hall. from the cancer research department , university of otago , dunedin , n.z. received for publication july 6 , 1948 . it has been realized for a long time that two processes might be involved in the pathogenesis of neoplasms , one which is concerned with the transformation of normal into neoplastic cells , and the other which promotes the growth of friedewald and rous ( 1944a , 1944b ) used neoplastic cells into a visible tumour . initiating " for the former , and " promoting " for the latter process . the term rous and kidd ( 1941 ) , and mackenzie and rous ( 1941 ) analyzing the effects of tar and carcinogenic hydrocarbons on the skin of rabbits , found that these agents " cause many more cells to become tumour cells than give rise to visible growths . " berenblum ( 1941a ) discovered that the yield of tumours of the skin induced in mice by sub - optimal doses of carcinogenic hydrocarbons could be increased by subsequent application of croton oil , and used the term " epi - carcinogenic action " to describe this effect . 
mottram ( 1944a ) refined berenblum 's technique ; he found that tumours could be obtained by a single application of benzpyrene if the painting with the carcinogen was followed by repeated application of croton oil.. 
they were seen first in a rat killed 10 weeks after the withdrawal of the carcinogen , whereas an animal of the same group sacrificed 3 weeks earlier , showed only the well - known picture of hyperplasia and loss of colloid . 
the number and size of the adenomata increased during the course of the experiment , but their histological pattern remained essentially unaltered there was up to the twenty - first week , when the experiment was terminated . no indication of beginning malignancy , the nodules remaining sharply defined apart from the multiple adenomata of the thyroid , and showing orderly growth . no other lesions were found which could be attributed to the action of a.a.f. even when the duration of the experiment is prolonged for 18 months , the incidence of tumours induced by 10 - 15 mg . 
the only neoplastic changes seen in this group were single adenomata , the first of which was found in a rat which had this was of minute size involving received methyl thiouracil for 21 weeks . in three of the four animals killed after 42 weeks of treatonly a few follicles . ment with methyl thiouracil , single adenomata were also found . 
bielschowsky has allowed me to include in this paper an experiment performed by him in 1945 which he has already mentioned ( bielschowsky , 1947 )  . twenty female rats received daily 6 mg . 
the neoplastic changes found were single adenomata of varying size . these benign neoplasms were indistinguishable from the ones which appear after prolonged stimulation with goitrogenic agents , and which persist after their withdrawal . only in one animal ( rat 3 ) two minute nodules were present in the same lobe . it is of interest that a.a.f. 
did not transform these benign structures into cancers . to test for the existence of latent neoplastic cells in the thyroid the following experiment was set up . fourteen rats received first 4 doses of 2 - 5 mg . 
the existence of such latent cells in mice was demonstrated by applying an unspecific irritant to the skin which had received a single dose of a carcinogenic hydrocarbon ( mottram , 1944a ; berenblum and shubik , 1947a )  . there is excellent agreement between the results of mottram , and of berenblum and shubik except in one point . 
berenblum ( 1941b ) , and berenblum and shubik ( 1947a ) could not find any evidence for a sensitizing action of croton oil applied previous to the carcinogen to.the skthe results obtained in this laboratory agree with those of berenblum and shubik . there was no evidence that pre - treatment of the thyroid with a goitrogenic agent sensitized the gland to the subsequent action of a.a.f. it could be shown that a small dose of a.a.f. , which alone is incapable of inducing visible tumours in any part of the body , must nevertheless transform many normal into neoplastic cells . 
in the doses used , acts on the thyroid in the same way as a single moderate does of a carcinogenic hydrocarbon . there exists , however , one difference between the action of croton oil and the effects obtained with prolonged hormonal croton oil , however long applied to the skin of mice , produces only stimulation . diffuse hyperplasia , but several examples are known where long continued stimulation by hormones leads to formation of benign and malignant tumours . for instance , treatment with oestrogens leads to cancer of the breast in rats ( geschickter , 1942 ; nelson , 1944 ) , and administration of goitrogenic compounds induces cancer of the thyroid after 20 or more months ( purves and griesbach , 1946 ) , benign tumours appearing earlier ( purves and griesbach , 1947 )  . 
similarly in spayed mice , tumours of the ovary can be obtained by transplantation of this organ into the spleen . here the gonadotropic hormones are the stimulating agents ( biskind and biskind , 1944 )  . 
the single adenomata which , as bielschowsky ( 1945 ) has already shown , develop after stimulation with thyrotropic hormone in absence of a chemical carcinogen , very rarely appear as quickly and never with the regularity of the multiple tumours initiated by a.a.f. 
they seem to appear nearly as quickly as the papillomata of the skin in the experiments of mottram ( 1944a ) and berenblum and shubik ( 1947a , 1947b )  . unfortunately it is necessary to kill the animals in order to demonstrate the presence of the adenomata of the thyroid , so that it is difficult to discover the very early lesions . it seems , therefore , justified to assume that , in the experiments reported in this paper , the thyrotropic hormone plays the same role in the pathogenesis of the multiple adenomata of the thyroid as the croton oil in the pathogenesis of the papillomata of the skin . the fact that only benign tumours are induced in both sets of experiments strengthen the analogy , and it seems legitimate to disregard the late effects of hormonal stimulation in the interpretation of the.results. is worth while mentioning that the choice of method is of utmost importance in experiments designed to demonstrate the role of initiating and promoting factors . for instance , when methylcholanthrene is used in high concentrations a single application is sufficient to induce benign or malignant tumours ( cramer and stowell , 1943 )  . also large doses of goitrogenic agents , as used by kuzell , tripi , gardner and laqueur ( 1948 ) , seem to hasten the appearance of multiple adenomata of the thyroid . the induction of multiple adenomata of the thyroid by 10 - 15 mg . 
the conceptions derived from the study of experimental cancer of the skin by rous and collaborators , and by berenblum and shubik can be successfully applied to an analysis of the pathogenesis of experimental neoplasms of the thyroid . i wish to thank t . 
according to these measurements very little difference was observed between the size of the tumours of the control and dibenzanthracene treated animals in the high protein group after 7 days , and the tumours of the treated animals appeared to be only slightly smaller than those of the controls after 10 days . in the low protein group , however , the measurements on the 7th and on the 10th days showed that there was considerable inhibition of tumour growth in the animals treated with dibenzanthracene , while the tumours of the control animals had grown to about the same size as those of the controls of the high after 11 days the animals were killed and the tumours dissected protein group . very little tumour inhibiout and weighed . 
as - there was some doubt as to the absolute validity of this control method , we computed the number of cancer cases which would be expected , based on the morbidity figures from the cancer registry and on the official mortality statistics . 
rather unusual for twin studies of this kind . griginally all hospital cancer cases from the danish population of 4 million through six years , or an annual - number between 5000 and 6000 cases , but this figure must be reduced by about 20 per cent in which the questio ' n about twin birth had been left unanswered , giving a total very near to 30 , 000 cases ( 29 , 458 )  . the system of notification involves a rather heavy toll of omissions , vet it has functioned satisfactorily . 
the special questions asked twins with cancerbesides such items as name , address , ' occupation and the like - were confinea to previous diseases of a more serious character , including diagnosis and the date , in order to identify whether the twins were molloand place of treatment . zygotic or dizygotic , questions were asked about the similarity and about mistakes made by parents or others , and similarly about type and colour of hair , colour of eyes , stature , height and weight on the whole it may be said that we demanded almost full congruity before accepting a pair as monozygotic . 
the final distribution of dizygotic twins on groups of same and opposite sex , and the proportion between monozygotic and dizygotic pairs seem to show that our measures have been justified . it should be stressed that we have not been in - a position to contact the patients or their twins personally . 
the official percentage of twin births in denmark for the years 1926 - 30 is 1 - 64 , and considering the increased mortality among twin babies we ' think this a satisfactory correspondence . another check on the result was obtained through computation of the number of deaths expected from all causes among twins for whom notifications were satisfactory . 
among dizygotics we expected 36 - 3 and found 26 . these differences are not statistically 'significant , and they may be partially due to the less efficient information about those pairs of which one partner has died . in denmark , as elsewhere , the girl - boy ratio at birth is 0 , 97 with a male excess , which in the course of a fev years changes to a slight female preponderance . however , we find among both monozygotic pairs and dizygotic pairs of opposite sex a female preponderance of 1 , 48 to 1 , and 1 , 64 among the same - sexed dizygotic pairs , making 1 ' 53 for the total . 
the explanation of this considerable female excess m our material no doubt must be ascribed to the higher cancer incidence among females than among males in denmark , combined with the earlier age - in which female cancers arise . 
and , if we calculate the percentage of opposite - sexed twin pairs in our material , a figure which should be uninfluenced by the difference in mortality among the two sexes , we find exactly the same value as in the corresponding official birth statistics - 36 , 2 per cent . in spite of these satisfactory results , it should be remembered that in dealing with twin - pairs , of which at least one is suffering from old - age disease like cancer , we must expect insufficient information from twins in cases where the partner died in childhood . therefore we have excluded the twin - pairs where one partner bas died before the age of 5 years . similarly we have lost sight of a number of cc second " twins through emigration and similar events , so that the number has shrunk ' from 336 to 185 pairs . 
3. given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . since 1944 we have taken a detailed family history from all patients reporting with carcinoma of the breast . 
we have 459 family records up to the end of 1947 which are reasonably complete . so far we have not succeeded in supplementing these histories , taken at the time of first visit to hospital , by later questions to the surviving patients or by arranging visits to their homes or relations . 
some attempt has been made to confirm the causes of death of relatives by letters to hospitals , doctors and the registrar - general 's department , but such confirmation has , as yet , been obtained in only a few cases . our figures , therefore , contain all those errors of inadequate information and faulty recollection that one would expect from data collected . 
many people die of cancer without their relations knowing that this was the cause of death . it is in fact surprising how successful a woman can be in concealing a cancer of the breast from her nearest relatives living in the same house with her . it is not , therefore , so surprising that more distant relatives , or even close relatives living away from home , may be unaware of the nature of the illness involved relations , even some of an older generation , who are still living at the time that the patient is first questioned may later develop malignant disease . 
the mixtures which had a ph of about 2 - 5 were polarographed as f - 611ows , : the test solution , into which dipped a dropping mercury cathode , was connected to a saturated calomel reference anode ( s.c.e. ) by salt - agar bridges ( saturated kci in 3 per cent agar - agar ) and the solution deoxygena - ted by passing a stream of water - washed oxygen - free nitrogen through it for 10 minutes . 
the percentage ttc reduced by serum was estimated with reference to the wave height of ttc in the blank reaction mixture . triphenylformazan 1 - 2 volts under the present conditions . gave no reduction wave in the range 0 to 200 to fig . 
2. - scatter diagram showing negative linear correlation between percentage ttc reduction regression lines have been constructed from by serum and percentage tumour weight . the regression equations : in the scatter diagram , fig . 
2 , from which it will be seen that there is a negative linear correlation between percentage ttc reduced and percentage tumour weight . the correlation coefficient ( r ) was calculated in the usual way ( moroney 1953 ) and found to be - 0 - 75 , t test = 5 - 63 ( n = number of animals ) highly significant at the 01 per cent level . reducing capacities of tumour and normal rat sera are show - n in fig . 
serum hastened colour development in iruminated mixtures , the colours being marked after i day . control solutions containing no serurn required 2 to 3 days to develop a pink colour whfle serum mixtures and controls kept in the dark exhibited no colour even after i week . after exposure to dayeght for 2 days tumour serum mixtures were coloured pink whereas normal serum mixtures , orange - pink after i day , were orange366 w . 
neish of 10 tumour sera , 9 ( tumour range , 3 - 4 to 22 - 8 per cent ) yellow in colour . showed pink colours and 1 serum ( 8.1 per cent ) gave the orange - yellow reaction . six normal sera each gave orange - yellow colours . in time , all colours faded to pale yellow and the solutions fluoresced blue in ultra - violet light . 
no difference was found with respect to ttc wave height between tumour and normal serum - ttc mixtures and the illuminated control but a new wave was observed in each solution which had been exposed to light . this wave was never observed in the ttc - alkali reaction mixtures described in sections ( 1 ) and ( 2 ) , or in control mixtures kept in the dark . 
and it was found to be due to another photochemical reaction product of ttc , namely the 2 , 3 , diphenylene - 5 - phenyl tetrazolium compound ( blue fluorescent in ultra - violet light ) described by hausser , jerchel and kuhn ( 1949a ) and by kuhn and jerchel ( 1952 )  . 
the tumour extended outwards for 1 - 5 cm . into the surrounding lung tissue , and in collar - fashion for 4 to 5 calong the bronchus , its branches and the contiguous blood vessels . ' the cut surface of the tumour was finely patterned by white striae , which separated softer , yellow or grey areas . 
the lymph nodes in the hilus of the left lung were replaced by a large mass of partly necrotic tumour tissue which , extended into the posterior mediastinum , compressing and invading the adventitia of the great vessels and of the oesophagus . 
numerous deposits of tumour , up to 3 cin diameter , were present in the left pleura , especially over the intercostal spaces , and the pleural sac contained approxiniately 300 ml . 
the mucosa was fixed to the tumour and slightly elevated ; superficial ulceration involved an area of 2 - 5 x 2 cthe lumen of the bowel was not obstructed , and the mesocolic lymph nodes appeared to be normal . the peritoneal cavity contained a small amount of straw - coloured fluid ; the serosa was sparsely studded with tumour deposits which measured up to i cin diameter . 
the surviving liver tissue was deeply bile - stained and congested . the lymph nodes around the coehac axis and head of the pancreas , in the porta hepatis and in the lesser omentum were enlarged , and their substance was replaced by tumour tissue . 
the para - aortic and iliac lymph nodes were involved to a less degree . there were no relevant abnormahties of the other abdominal and pelvic viscera . the body of the ilth thoracic vertebra was almost completely destroyed by tumour , and had collapsed , with consequent pressure upon the spinal cord . 
the appearances were characteristic of an anaplastic bronchial carcinoma " of the " oat - cell " type , and confirmed the macroscopic diagnosis of primary bronchial carcinoma . the greater part of the colonic tumour was . 
the mucosa overlying the mass , however , showed an abrupt transition at its periphery from the normal structure and cytology to a polypoid , hyperchfomatic columnar - cefl adenocarcinoma , irregular gland - hke extensions of which penetrated deeply into the tunica muscularis ; the structure and cytology were those ' of a primary colonic adenocarcinoma . 
the patient remainecl in seemingly good health for more than 18 months , and then sustained a fracture of the pelvis in an accident . nine weeks later an abscess developed deep in the inter - ischial region , necessitating incision ; its contents were not examined . during the next fortnight a papiroma , about 0 - 8 cin diameter and situated at the medial end of the left inguinal skin fold , began to grow rapidly ; it doubled its size within this period , after which it was excised . 
the patient then remained apparently well until 1949 , when she began to be dyspnoeic ; - examination showed a right - sided pleural effusion . clear , amber - coloured fluid was aspirated 5 times , at intervals of a few weeks , the quantities withdrawn ' ranging from 550 to 1200 ml . the fluid contained between 4 and 5 per cent of protein ; a few cehs were present , mostly lymphocytes , with a very small pro_portion of neutrophile polymorphonuclear leucocytes and normal serosal cells . aerobic and anaerobic cultivation on ordinary media yielded no growth , and , cultures for mycobacterium tuberculosis were also sterile . radiography showed no evidence of neoplasm in the chest , but the effusion persistently obscured the - greater part of the right lung field ; there was never any demonstrable effusion in the left pleural sac . as there was no evidence of recurrence or metastasis of the carcinoma , and as there was no demonstrable infective cause of the recurrent pleural effusion , the discovery of an adnexal tumour on pelvic examination suggested the possibifity that the con ' dition was an at pical variant of the meigs - culhngworth syndrome . 
at laparotomy , 6 months after the onset of dyspnoea , a cystic tumour of the left ovary was fou ' nd and removed ; there was no other abnormality in the pelvis or abdomen . 
the tumour of the left breast was a simple intracanaficular fibro - adenoma . macroscopically , the ovarian tumour was a unilocular cystic teratoma , i 1 cm . in diameter , filled with sebum - hke material and hair . 
the cyst had a smooth lining ; its war was i mor less in thickness , except near the pedicle , where there was an irregular , bone - hard eminence , approximately 2 cin diameter , projecting into the cavity . adjacent to the pediele the remnant of the ovary was identifiable on the external surface of the tumour as a flattened , ovoid area of firm , greyish - white tissue , which measured 3 - 5 x 2 - 5 csuperficially , and up j . 
symmers microscopically the cyst was lined by keratinizing epi - to 0 - 4 cin thickness . dermis , external to which was a narrow zone of fibro - fatty tissue . hair - follicles and large sebaceous glands were numerous in the skin covering the hard projection , which consisted of bone , bron ' chial structures and neuroglia . 
the third hypothesis seems to us to be the only one tenable . if the coexistence of two primary neoplasms is accepted , the significance of the presence of a metastatic deposit from the primary bronchial carcinoma . at the site of the primary colonic carcinoma requires to be considered . this association may have been fortuitous , or the presence of the colonic neoplasrn may have predisposed to the establishment there of the metastasis , or the development of the latter may have inducea cancerous change in the adjacent mucosa ; it seems to be impossible to say which suggestion is correct . 
the induction , by some effect of the existing neoplasm , of sarcomatous change in the stroma of carcinomata has at times been postulated in explanation of the genesis of so - called careinosarcomata : in view of the considerable doubt as to the origin of the sarcoma - like component of these tumours , such a hypothesis has httle practical value . 
the induction of one carcinoma by another was postulated by duboisferri ' ere ( 1939 ) , who suggested that hepatic metastases in his case of islet - cell pancreatic carcinoma had induced local development of bile - duct carcinomata . he was not able to exclude the possibihty that the adenocarcinomatous areas in the liver were metastases with an unusually well - developed tubular structure , such as is sometimes seen in islet - cell neoplasms . seecof ( 1924 ) reported a case which was in some respects similar to ours . 
7. received for publication june 9 , 1947 . the presence and activity of the milk - borne agent of mammary tumours of mice discovered by bittner ( 1936 ) are detectable only by the growth of a mammary tumour . 
found two nodules in one mouse out of nine of the n strain in which mammary tumours had never occurred . also when efforts have been made to exclude the milk - borne agent from high cancer strains by cross - suckling , nodules have nevertheless been found . 
thus bittner , huesby , visscher , ball and smith ( 1944 ) examined the mammae of fostered breeding females ( fostered by cancer - free maternal stock ) from high cancer strains a and c3h . 
all the females had given birth to at least three litters and ranged from 11 to 16 months old , thereby providing suitable conditions for pathogenic activity of the milk - borne agent . nodules were found occasionally , though never more than one to a gland , thus nodules were still present though in smaller numbers when efforts were made to exclude them than in mice which had been suckled on their own cancer - prone mothers . this evidence indicated that nodule incidence is not eliminated by cross suckling with the same regularity that is attainable in regard to tumour incidence . 
6. - regression of hyperplasia induced by 800 y oestradiol in spayed r3 female ( carrying the milk - borne agent ) , and persistence of areas of nodular hyperplasia ( adenomas ) at 6 months old . 
the former discrepant results ( bittner et al . , 1944 ; huesby and bittner , 1946 ) have to be remembered , although subsequent observations ( kirschbaum et al . , 1946 ) provide convincing evidence that hyperplastic mammary nodules do not occur in the absence of the milk - borne tumour agent . the second source of objection to accepting nodular hyperplasia as evidence of activity of the milk - borne agent acting alone is that certain observations , which will be referred to again later , suggest that similar cellular proliferations with acinus formation are stimulated by oestrogenic hormones alone . the problem of the exact origin of the hyperplastic nodules is of great these focal acinar proliferations precede maligimportance for several reasons . nant tumours in time of appearance and are often more numerous . they might thus provide an alternative and earlier means of detecting activity of the tumour they may also represent the earliest sign of tumour growth before it agent . can be described as malignant . if so they would provide material enabling one to determine which influences are causative and which are encouraging , in the sense in which the term is used by rous and kidd ( 1941 ) and mackenzie and rous ( 1941 ) in the development of malignant tumours . 
the discrepant results ( previously referred to ) concerning their incidence often suggest that they may be more sensitive criteria of the presence of the agent . if the nodular hyperplasias are to be used for any of the purposes suggested , it must be proved beyond question that they are in fact dependent for their origin and continued existence on the presence of the milk - borne tumour agent , and that the nodules , or some of them , are but an early stage of eventual malignant tumours . other possible causes of focal cell proliferation such as hormones must be excluded . the possibility has also to be considered that mice of high cancer strains carry more than one formative milk - borne stimulus for the mammary gland . one agent might be the cause of frankly malignant tumours and another the cause of nodular hyperplasias . appears more probable , however , that one and the same agent is responsible for both types of tumour , benign and malignant , but that its virulence varies . greater virulence would be understood as the capacity to stimulate the mammary gland cells to multiply and invade or metastasize within the life of the mouse ; less virulent variants would cause merely focal proliferations . 
whether the cell proliferations which it produces are benign or malignant depends upon the combination of its " virulence " with encouraging or deterrent forces . the experiments here recorded are concerned only with the origin , provocation and continued existence of the adenomatous hyperplastic nodules . was found possible to stimulate the appearance of nodules artificially with measured limited amounts of hormone at an earlier date than that at which they become detectable spontaneously . it was also possible to distinguish responses in the mammary gland due to hormone alone . responses to other formative stimuli were considered . mamnmae of female and rudimentary mammae of male mice respond to 180 b . 
the responses to single and repeated doses ' of ovarian hormones were examined at various intervals after application as described under experimental methods . the existence of a strain difference in response to oestrogens which was independent of the presence of milk - borne tumour agent was confirmed . 
a similar hormonal response was obtained in c3h mice giving rise to focal hyperplasias , but as this strain was not freed from the milk - borne tumour agent , it is uncertain , though probable , that the response to hormone alone would have given this atypical reaction . 
some were derived from pure lines , others from random breeding within the strathe incidence of spontaneous nodules of hyperplasia in the mammae in 26 virgin females segregated from males had previously been found to be 100 per cent after the age of 8 to 9 months . malignant tumour incidence in the same series was 69 per cent nodules in this strain are extremely numerous in both virgin females and breeders . r3x sublines free from the milk - borne tumour agent were bred by foster nursing an original family of 2 females and 1 male on a c57 ( black ) mother from the moment of birth . 
pullinger record was kept of the relationships of every mouse of these sublines so that , if evidence of the presence of milk - borne tumour agent subsequently reappeared , the progeny liable to be affected could be traced . 
from every litter containing more than one female , one or two were used for testing the hormone response this breeding provided further while the remainder were allowed to breed . mice for testing , and also controls to prove the absence of the milk - borne agent . the same breeding females also provided controls for all the male mice that altogether , 44 breeding females reached the average tumour were treated . age ( 81 months for this strain ) ; of these 24 were force bred owing to the circumstance that they failed to rear or destroyed their young , a habit to which many r3 females are prone . in three years no tumours were seen . 
the majority of strong a mice when two months old or over failed to survive the combination of this anaesthetic and ovariectomy . their survival could only be assured after they had reached the age of 2 months , if ether ' ere used . 
the ovaries of all mice were removed by the abdominal route ; they were excised of their oviducts ( uterine horns )  . together with about successful removal of all local oestrogen - producing tissue was judged at autopsy by complete atrophy of oviducts and uterus . vaginal smears were made from some of the females for 2 - 3 weeks before they were killed . it was necessary to examine the former site of uterus and oviducts in every mouse , because if the tissues were not excised as described , cysts containing clear fluid sometimes developed at the cut ends of oviducts after subsequent oestrogen treatment . 
when this was the case atrophy of uterus and oviducts was never complete , and the impression was gained as the result of much experience of mammary gland changes that these cysts were themselves secreting oestrogen . this difficulty was soon overcome at a time when oestrus records were not being made in spayed mice , so the matter was never settled . 
the oviducts became very slender tubes ( brownish in r3 and r3x mice ) and the uterus was greatly shrunken . oestrus cycles ceased in all those mice which were tested and did not reappear . 
any mice that had developed intraabdominal cysts or ligature abscesses , thereby possibly concealing cysts , at the cut ends of the oviducts , or whose oviducts had not undergone atrophy at the 16th to 20th weeks of experiment , were discarded . 
the purpose in using it was to give a limited measured amount of hormone within at most a few hours in order to obtain a limited response rather than a cumulative one due to prolonged irregular absorption as from oily solutions or pellets . 
the results indicate that responses in females vary quantitatively with dosage and qualitatively with strain and , within the strains , with ages younger than 49 to 56 days old . for the purpose of the present experiment most of the females received two doses of 400 microgrammes at 20 days ' interval . 
the response is visible owing to its atypical nature in respect of a milky secretion which renders ducts and clusters of acini visible . mice examined in vivo in early stages and all others were finally killed . all 10 mammary glands ( or fat pads in males ) were stained in bulk , cleared , inspected , and whole mounts made of representative mammae or those showing special features . the method of staining in bulk differed little from that described by gardner ( 1934 )  . after 4 days ' fixation in bouin 's fluid the mammae were dissected off from the skin , muscle and covering fascia with the aid of a dissecting microscope magnifying 7 and 14 times . nerve fibres were removed and some of the large blood vessels . these stripped mammae were then immersed overnight in 50 per cent alcohol , and next stained for about 4 hours in 1 part of ehrlich 's acid haematoxylin freshly diluted with 3 parts of a 2 per cent aqueous solution of after differentiating for about 10 minutes in acid alcohol ( 3 per acetic acid . cent hc1 in 50 per cent alcohol ) the stained glands were rendered blue or blueblack in several changes of 50 , then 70 per cent alcohol for as many hours or days as were required to develop a deep colour . they were next dehydrated and cleared in the usual manner . while in the first change of clearing agent ( xylol ) notes were made by the author after examining all 10 mammae or fat pads with the binocular dissecting microscope . 
the ducts were distended and filled with milky secretion , which rendered the main branches and many smaller ones visible to the naked eye in all 10 mammary glands . there was also a pseudolobular alveolar differentiation with great multiplication of acini arranged in clusters in all 10 mammary glands . 
a similar response was given by the maximum dose of 400 y of oc - oestradiol repeated at 20 days ' interval ( total 800 y ) in 15 out of 15 mice which were examined in ' ivo . 
pullinger limits of outgrowth attained during normal pregnancy . it is pathological also in that the degree of differentiation is suggestive of a 9th - 12th day pregnancy while the milky secretion is voluminous . male glands reacted to larger doses in a similar manner . 
some light on this problem was gained from experiments similar to those here described using the double dose of 400 microgrammes of oestradiol on spayed f.1 hybrid females of the c57 x r3x cross . the curious observation was made that a similar lobular - alveolar response was provokedin all the mammae , but it was localized in approximately half of each gland . 
no inflammatory or metaplastic nodules were encountered . in the course of these experiments the possibility had to be considered that in the females some other sources of oestrogens might be stimulated by ovariectomy and after cessation of the action of artificially applied hormone to produce oestrogens , as smith and bittner ( 1945 ) found in the c3h strain . that no such stimulation had occurred was proved by making vaginal smears during the last two to three weeks of the experimental period in 11 out of 20 mice , and by inspection of uterus and oviducts at autopsy . in no case was there a return of oestrus or failure of uterus and oviducts to atrophy . r3 virgin females deprived of their ovaries but containing the milk - borne tumouqr agent . early changes in the mammae in response to ovariectomy and oestrogen treatment ( ketohydroxyoestrin and oestradiol ) were similar to those described in the same strain deprived of the tumour agent ( 32 out of 32 mice )  . 
by the vaginal smear technique , oestrus in 30 cells were seen on one occasion in each of 2 mice out of 32 examined . mice oestrus cycles or cells did not recur . the contrast between the mammae in the two sets of mice at 16 to 20 weeks there was complete absence of adenomas in those mice which was striking . had been deprived of the milk - borne tumour agent , whereas in mice of the original r3 strains carrying milk agent adenomas were numerous in nearly all fig . 
a few imperfections due to incomplete regression did not cause confusion , and will be referred to in this connection again . the conclusions were drawn that the foci of hyperplasia ( adenomas ) in the r3 females carrying tumour agent , were due in respect of their origin and persistence to the presence of a milk - borne tumour agent , presumably identical with or a variant of bittner 's agent , and that this agent had been forced into activity by the large dose of - hormone . these nodules are considered to be experimentally produced counterparts of those that occur spontaneously in all r3 females after the age of 8 to 9 months . they are similar to those described in great detail , and finely illustrated by gardner ( 1942 ) in other strains . 
an average of 6 mammary glands per mouse developed from rudiments and all examined revealed the atypical response characteristic of females of this strain . irregular lobules were seen after cutaneous application of 8001200 microgrammes of oestradiol with or without 1500 microgrammes of proregression required 6 to 7 months to become complete , leaving gesterone . bare atrophic ducts ( table ii )  . r3 males containing milk - borne tumnour agent . when additional time had been allowed for regression of hormone response , results were similar , and almost as regular as in spayed females containing milkborne tumour agent . either oestrogen alone ( 1200 microgrammes ) or combined with one dose of progesterone ( 1 , 500 microgrammes ) was sufficient to stimulate the growth of adenomas ( table ii )  . 
gagliano. from the cancer research institute and the department of medicine , college of physicians and surgeons , columbia university , new york . received for publication january 30 , 1950 . tetra - sodium mitchell ( 1948 ) recently reported a clinical study on the use of parenterally administered 2 - methyl - i : 4 - naphthohydroquinone diphosphate ( synkayvite ) as an adjuvant to radiotherapy in the management of inoperable and far advanced malignant disease . in a small series he noted prolongation of the mean survival time of patients with inoperable carcinoma of the bronchus treated by the combination of chemical agent and irradiation when compared with that of patients who received x - ray therapy alone , which he found to be statistically significant . the rationale for mitchell 's ( 1948 ) selection of this drug for clinical trial in combination with radiotherapy depended upon his observation that the chemical compound produced mitotic inhibition of chick fibroblasts in tissue culture . although there have been many laboratory studies on synkayvite as a vitamin k substitute , no investigations have been published on the effect of this compound on experimental neoplasms . 
the growth of the tumours in control and treated animals was followed by serial mensuration of the outside diameters , but the conclusions reached in this study rest on the comparison of the wet weight of the tumours in the control and treated series determined at the 104 a . 
from the information included it is possible to estimate with accuracy the actual protocols for the individual experiments , even though the pertinent results are here summarized as averages ; the standard deviation has been calculated in each instance in order to describe the range and the distribution of the individual tumour weights about the mean tumour weight . 
the standard deviation of the mean which is necessary for the determination of statistical significance between two means is derived by dividing the standard deviation by the square root of the number of observations . in several of the experiments 5 - amino - 7 - hydroxy - 1 - h - v - triazolo [ d ] pyrimidine ( 8 - azaguanine ) was also administered to tumour - bearing animals for purposes of comparison with synkayvite . 
gagliano neoplastic disease and malignant tumours in experimental animals is an unsettled issue , it is important to note that , thus far , all of the chemotherapeutic agents which have a demonstrable palliative effect against neoplasms in man have also been shown to inhibit comparable tumours in laboratory animals . it is also appreciated that the observations which we have recorded do not duplicate in the laboratory the clinical experiments of mitchell ( 1948 ) , inasmuch as he studied the combination of radiotherapy and the drug whereas - we investigated the drug alone . evaluation of combination therapy , however , utilizing radiant energy plus a chemical compound , is not feasible in studies on experimental neoplasms due to the ease with which x rays alone can destroy subcutaneous tumours . therefore , in spite of negative experimental evidence of the type presented in this report , the possibility remains that synkayvitein combination with radiotherapy may produce a greater carcinolytic effect than x - ray therapy alone . 
pullinger. from the imperial cancer research fund laboratories and the research department , the glasgow royal cancer hospital , glasgow , c.3. received for publication february 7 , 1952 . the hyperplastic nodules here referred to comprise all varieties found in surveys of spontaneous nodules in previous publications ( pullinger , 1949 , 1952 )  . at the time these surveys were being made specimens of affected nipple regions were almost invariably mounted and kept . it gradually became obvious that one nipple region , the 2nd on either side , was more often the site of nodule formation than any other . 
when the surveys were complete , the 5 pairs of nipple regions were arranged together with the number of times they contained one or more hyperplastic nodules of the various sorts . only those nodules are now included of which whole mounts were kept . 
the period of time covered was continuous from 1945 to the end of 1950 . the number of mice with mounted nodule - containing nipple regions was 116 ; the number of the nipple regions 146 . 
no record had been kept of 13 from which serial sections were made in the earlier stages of the survey ; more were incomplete or have been mislaid . six examples of bilateral nodules in the same gland were counted as only one of the pair . 
belcher. from the wards and the bland - sutton institute of pathology , the middlesex hospital , london , w.1. received for publicatiod , may 16 , 1952 . adenocarcinoma in the oesophagus may arise in three ways : ( 1 ) as an upward extension of a carcinoma of the stomach , ( 2 ) as malignant change in the mucous glands that are normally found in the oesophageal submucosa , and ( 3 ) from ectopic gastric mucosa . the first is not uncommon ; the second is rare . the third , also rare , is the type that concerns us here . in 1950 carrie reported a case of adenocarcinoma of the oesophagus that had arisen in an area of ectopic gastric mucosa . 
he reviewed the literature and likened the lesion to the unicorn in that many authors had described it , but only one had ever seen it . although he makes no reference to the possibility of a hernia being present , the description of the specimen , coupled with the fact that the tumour was in the cricothyroid region ( where ectopic gastric mucous membrane is most frequently encountered - schridde ( 1904 ) ) , makes it certain that this was indeed a genuine example of this rare lesion . bosher and taylor ( 1951 ) describe a case in which ectopic gastric mucosa was present in the oesophagus . there was reflux oesophagitis and stricture formation at the level of the aortic arch . at first sight this would appear to be a case similar to the one about to be described , but it seems more likely that it is another example of hiatus hernia with extreme secondary shortening of the oesophagus , as the barium meal strongly suggests that only a small portion of the stomach is in the abdomen . although they state that at operation the hernia was small , it is notoriously difficult to distinguish stomach from gullet on external appearances alone . 
he had no difficulty with fluids . one week prior to admission food stuck in the same place and was regurgitated . since then solid food would not pass at all . and no glands were palpable . on examination the patient looked well . there was no wasting or dehydration on 14 . 
the oesophagus was removed from a point 2 inches above the tumour to the cardia and the free end implanted into the upper part of the stomach . post - operatively the patient had some fever and pylorospasm but was eventually discharged from hospital well on 4 . 
the mucous membrane above the tumour was entirely squamous in type and was normal for the oesophagus ; that below the growth was entirely glandular apart from a few islands of squamous epithelium about 2 inches above the lower limit of excision . 
the lower half of the oesophagus contains only smooth muscle in its muscular coat . in the case described , striated muscle was present down to and including the site of the adenocarcinoma . this represents a point about 5 inches above the junction of gullet and stomach . 
the normal gullet is about 10 inches long as meastired from the termination of the pharynx at the level of the cricoid cartilage to the cardiac orifice of the stomach . it would thus appear that the striated muscle in this case had a normal distribution . however , the circular muscle - fibres at the squamo - glandular junction appear to have thickened to form a sphincter . 
this constitutes a departure from normal , and it may have prevented regurgitation of acid secreted by the gastric mucosa lining the lower half of the gullet . this may well have prevented the development of oesophagitis earlier in the patient 's life . there was definite histological evidence in this case that the adenocarcinoma had arisen in the glandular mucous membrane immediately adjacent to the junction of the squamous and glandular epithelium . the emphasis is placed on " glandular " , for this showed varied degrees of chronic inflammatory and atrophic changes which obscured the normal picture of a gastric type of mucous membrane . these changes conform to those that may be seen in stomachs that are affected by chronic gastritis , including the atrophic type . 
thus we conclude that the lower half of the gullet in this case was lined by gastric mucous membrane that was the seat of chronic inflammatory and atrophic changes , which may well have been a factor in the development of carcinoma . the rare occurrence of adenocarcinoma in the oesophagus , other than those cases that have obviously spread from a gastric origin , has been put down in the 130 13 . 
mitchell. from the department of radiotherapeuties , university of cambridge . received for publication july 8 , 1953 . attempts to evaluate tetra - sodium 2 - methyl - i : 4 - naphthohydroquinone diphosphate ( compound i , synkavit ) as a radiosensitiser in the radiotherapy of malignant tumours have been in progress since november , 1946 . 
at first the compound was used alone and in conjunction with palliative x - ray therapy in some very it soon became evident that in general the compound alone had advanced cases . no therapeutic effect in malignant tumours . 
at the same time , all cases of inoperable carcinoma of the bronchus were treated , if possible , by the combination of x - ray therapy and compound i ; the results were assessed mainly by survival times from the first x - ray treatment and the first sympton and were compared with those which had been obtained previously in the same department with x - ray therapy only , and which were very similar to the depressing results obtained by most of the workers . slowly the difficulties of this type of clinical investigation were appreciated . moreover in 1950 erratic results were encountered both in the clinical trials and in animal experiments . it seems likely that these findings were attributable to the thermal instability of compound i in aqueous solution in the absence of oxygen ( mitchell and simonreuss , 1952 )  . 
much more consistent results have been obtained since the ampoules have been stored in a refrigerator at about 30 c . the evidence obtained by these preliminary studies was sufficiently suggestive to justify further work , but the methods used were clearly inadequate . it became essential to employ properly designed methods for the clinical evaluation of radiosensitisers . 
the importance of these methods was emphasised at the time by their use in clinical evaluation of chemotherapeutic agents in tuberculosis ( medical research council , 1948 , 1950 )  . investigations of this type in the study of radiosensitisers have been in progress since april 1951 ; as yet the only results available are for the treatment of inoperable carcinoma of the bronchus . the results of the earlier studies have been reported by mitchell ( 1948 , 1949a , 1949b , 1950 , 1951 )  . this work has been criticised by gellhorn and gagliano ( 1950 )  . otte ( 1949 ) reported briefly on the combination of x - ray therapy and some synthetic vitamin k substitutes in the treatment of 300 patients with advanced malignant tumours and claimed improved palliation . 
mitchell selection of types of malignant tumour for investigation . it is suggested that a practical minimum requirement for usefulness of a radiosensitising chemical agent is that its employment in combination with radiotherapy should produce a mean survival time after treatment double that after radiotherapy only , for the type of malignant tumour treated . 
hence taking into account the frequency distribution of the survival times , it is likely to be necessary to observe the cases treated by combined therapy for an interval of at least 6 times the mean survival after radiotherapy only . 
to this time must be added the time necessary to accumulate an adequate number of cases . this approach is limited to the study of types of malignant tumour in which the results of present methods of treatment are bad and in which the time of survival is short . inoperable carcinoma of the bronchus is an obvious choice for investigation it is the only common type of malignant disease with a very short natural history . despite advances , only a small proportion of all cases of carcinoma of the bronuntreated patients are often very miserable . 
the chus are curable by surgery . results of treatment of inoperable cases by present methods , including radical nevertheless x - ray therapy in general has sufficient x - ray therapy , are poor . palliative value apart from prolongation of life per se , to justify attempts to improve this . with x - ray therapy only , inoperable carcinoma ofthe bronchus appears to have a a rather uniform natural history . 
of these , histological evidence was obtained in 245 patients and their average survival from the first symptom was 14 - 3 months and from the beginning of x - ray treatment 4 - 5 months . 
7 of this paper , it can be deduced that of 729 patients , only 45 survived 8 months , 20 survived 12 months , 8 survived 18 months and none survived 3 years following in this series , the best survival rate - 4 - 7 months - was in a x - ray therapy . group of 80 patients who received a total dose as measured in air of 5000 - 6000 r ; higher and lower doses were associated with poorer results . 
the most important factor in determining survival is the extent of spread of the disease when treated . this evidence suggests that in representative series of cases of inoperable carcinoma of the bronchus receiving x - ray therapy , the mean survival from the beginning of treatment is about 4 - 5 months . 
to try to minimise its shortcomings , all the cases to which it is applied have been followed until death , or for at least 3 - 1 years and in assessing the results the proportion of cases showing unexpectedly good response has been compared in the case of patients treated by means of radiotherapy combined with intravenous compound with those treated by radiotherapy combined with intramuscular compound . the results of various types of treatment of patients with advanced malignant tumours classified as inoperable , stages iii and iv , and recurrent of all types except carcinoma of the bronchus using compound i in treatments from november , 1946 to july , 1909 inclusive , and assessed up to 31 december , 1952 , are summarised in table i for the cases verified histoan essentialy similar table has been prepared showing the rather logically . poorer results for 56 cases not confirmed histologically , but with reasonably the cases allocated to this preliminary survey were the great certain diagnosis . majority of the patients with advanced malignant tumours in which it was considered that present methods of treatment were not likely to give satisfactorily results . 
when the survey was started it was not realised that the use of the compound by intravenous injection was likely to be more effective than its use by intramuscular injection . the allocation of the patients to treatments involving the two mnethods of administration of the compound were certainly not a.t random , and the possibility of bias by the use of intramuscular injection in the more seriously ill patients cannot be excluded . however , there is no reason to suppose that such bias would influence the proportion of cases showing unexpectedly good clinical response . the resultsof the preliminary general survey summarised in table i suggests that the proportion of cases showing unexpectedly good clinical response is greater 316 j . 
one case of advanced carcinoma of the body of the uterus was treated by means of palliative x - ray therapy combined with intravenous compound , and one case of carcinoma of the tongue recurrent after previous x - ray therapy was treated successfully by radical x - ray therapy combined with intramuscular compound . of the 56 cases not confirmed histologically three survived more than 4 years after treatment . 
two of these showed an unexpectedly good response ; one was a woman aged 46 , who had a stage iv carcinoma of the breast with supraclavicular glands , and was treated by means of radical x - ray therapy combined with intramuscular compound , and the other was a case of a mixed parotid tumour which had failed to respond to further x - ray therapy , but appeared to be checked and rendered quiescent by intravenous compound onlv . 
the results are treated by statistical methods . it is suggested that estimation of the survival times , especially that from the beginning of x - ray therapy , is the most reliable criterion for objective assessment of the results of treatment . special attention has been paid to the influence of the extent of the disease , age and sex , the histology , the minimum tumour dose and overall time of the x - ray therapy and the details of administration of the compound . the general principles involved in the consideration of these factors are essentially the same in these preliminary studies as in the later clinical trials and except where relevant , will be discussed in this connection . 
the results of treatment were reviewed as from this group of cases of inoperable carcinoma of the bronchus december 31 , 1952 . comprises all those cases referred in which the diagnosis is accepted as proven according to the criteria given below , with the exclusion of patients not likely to benefit by palliative x - ray therapy . 
no technically operable cases and no postoperative cases are included . the control group consists of those cases of inoperable carcinoma of the bronchus selected according to the same criteria , which were treated by x - ray therapy only , using similar methods , in the same department between 1943 and may , 1947 . the difficulties of this method of providing a control group are recognised and include the possibility of introduction of serious errors of sampling . 
the use of alternate cases as controls was attempted but was abandoned as impractical . however , it has been shown that the relevant properties of the control and treated groups apart from the length of survival after treatment are substantially the same . it is found that the results of x - ray treatment in the present control group are substantially identical with those obtained in two large published series . 
mitchell ( b ) cases with positive histology on biopsy specimens of supraclavicular nodes , cutaneous or other metastases but in which there was no bronchoscopy or the bronchoscopic appearances were not definite ; this sub - group consists of 8 control cases and 8 treated cases ; ( c ) one case ( treated ) with typical bronchoscopic appearances together with metastases in the skin , confirmed histologically . these additional 15 control and 18 treated cases are usually more advanced and are in general less comparable than the " histologically verified " cases but must be considered with them to give a complete picture . 
of the combined series of " confirmed cases , " there are in all 34 in the control group , which was treated by x - ray therapy only , and 47 in the treated group , which received x - ray therapy together with the compound . 
as anticipated the results of treatment of the " confirmed cases " are poorer than those of the " histologically verified " cases . other groups of cases which cannot be included in the main part of this investigation may be summarised as follows : ( i ) cases with typical radiological appearances together with metastases at some stage but not verified histologically and in which there was no bronchoscopy or the bronchoscopic appearances were not definite . in these cases the diagnosis can only be regarded as probable . in the control group , there are 12 cases ; the mean time of survival is 8 - 50 months from the first symptom and 3 - 67 months from the first x - ray treatment . in the treated group , there are 13 cases ; the mean times of survival are 12 - 15 months from the first symptom and 6 * 31 months from the first x - ray treatment . ( ii ) cases rejected as unsuitable for palliative x - ray therapy . during the control period , there were 18 of these cases , of which 10 were histologically verified and during the period corresponding to the treated group , there were 7 cases of which only one was verified histologically . the enumeration of rejected cases is unsatisfactory because of selection by the physicians referring these advanced cases . hence the total number of cases with a reasonably certain or probable diagnosis of inoperable carcinoma of the bronchus is 131 . 
of the 7 cases of squamous carcinoma , two showed keratinisation . of the 29 verified treated cases , there are 17 cases of stratified carcinoma , of which 10 are squamous and 7 non - squamous , 3 cases of adenocarcinoma , 8 of anaplastic carcinoma and one an unusual poorly differentiated lesion . of the 10 cases of squamous carcinoma three cases show definite keratinisait is interesting tion ; in two further cases there is a suggestion of keratinisation . to note that all these cases responded well to treatment . the control group was treated by x - ray therapy only , from 1943 to may , 1947 . 
even if the cases which survived only one month from the first x - ray treatment are excluded , to meet the criticism of a possible difference in selection of the cases , the difference in survival after the first treatment between the treated group ( mean survival 9 - 68 months ) and the control group ( mean survival 5 - 23 months ) is still significant ( n = 39 , t 2 * 457 , p is slightly less than 0 - 02 )  . considering the histological classification , the only type providing adequate numbers is the stratified carcinoma . 
the basic principles involved are well understood as a result of the classical statistical studies of fisher ( 1925 , 1935 ) on the design of experiments , and on the work of hill ( 1952 ) on the design of clinical trials . 
in general , in considering therapeutic trials in the cancer field , the design must be capable of giving a completely convincing statistically significant quantitative result as efficiently as possible with a minimum number of patients and must be acceptable and above reproach from the moral and ethical points of view . 
the most important single feature of the design is random allocation of the patients to two or more alternative forms of treatment the value of which is being compared . for assessment of the result of treatment , it is necessary to select relevant criteria capable of objective measurement such as the survival time suitably specified . 
at the same time , it is absolutely essential to provide for each individual patient treatment which is the best possible according to present knowledge . accordingly , it may be , and probably often will be , necessary to plan to depart from what may be termed the theoretically ideal form of experiment with deliberate sacrifice of some information . in the present example of the attempted evaluation of tetra - sodium 2 - methyl1 : 4 - naphthohydroquinone diphosphate ( compound i , synkavit ) as a radiosensitiser in the radio therapy of inoperable carcinoma of the bronchus , cases were allocated at random to one of two alternative forms of treatment , x - ray therapy combined with compound i administered by intravenous injection ( x + i - vs ) and x - ray therapy combined with compound i administered by intramusculrzr injection ( x + i - ms )  . 
the latter is regarded as the control group . the preliminary clinical studies and animal experiments suggested that the results of x - ray therapy combined with intramuscular compound ( x + i - ms ) were slightly better than those of x - ray therapy only , and that with comparable doses of compound it was likely that x + i - vs would produce better results than x + i - ms . 
mitchell tests of heterogeneity must be made . clinical therapeutic trial must be justified a posteriori . it is necessary to - examine the possible importance of all the various factors which may be relevant including age , sex , extent of the disease at treatment , histology and / or cytology , the minimum tumour dose and overall time of radiotherapy , the total dose and overall time of administration of the compound and in particular the certainty of the diagnosis . it does not seem possible to estimate in advance the number of patients required . this will depend on the differences observed between the groups and subgroups . 
the results are likely to be of sufficient importance to necessitate the use of stringent criteria of significance . the randomisation was made on the basis of a provisional diagnosis of inoperable carcinoma of the bronchus , made when the patient was first examined by the staff of the department . 
some of the cases were referred with histological evidence from bronchial biopsy . in other cases , there had been no previous investigation and the provisional diagnosis was based on clinical evidence only . all cases were investigated critically , as necessary , and every effort was made to obtain histological and / or cytological verification of the diagnosis . almost all the sections have been reviewed by a . 
cruickshank , of the sims woodhead memorial laboratory , papworth , for most of the reports on specimens of bronchial aspirate . particular attention has been paid to the establishment of the diagnosis of carcinoma of the bronchus and the identification and exclusion of cases of bronchial adenoma and related tumours of low grade malignancy apparently arising in bronchial glands . 
barrett and may be summarised as follows : ( 1 ) stratified carcinoma , either squamous or non - squamous , the degree of keratinisation or differentiation being noted , ( 2 ) adenocarcinoma , ( 3 ) anaplastic carcinoma , including " oat - celled " carcinoma , and ( 4 ) others , including " alveolar " cell carcinoma and carcinoma not classifiable . 
the histological classification of carcinoma of the bronchus is often difficult because of the existence of intermediate types and is somewhat arbitrary in some cases . on the clinical side , a careful and full medical examination is made , including usually indirect laryngoscopy . it has been considered important to determine the extent of spread of the disease with special reference to the early detection of metastases in bones . the occasional cases originally considered inoperable and in which it has been found possible subsequently to carry out some type of surgery have been considered separately in the assessment of the results . 
and increased daily in steps of any undesirable reaction such as excessive coughing , nausea , faintness the chest is observed after intravenous injection , the dose which there is no such reaction and then cautiously increased again on the following days , sometimes by steps of for most patients , for intravenous injections the best maximum daily dose appears to be 100 mg . ; dose is increased to as high a level as is tolerated . dosage is started with or discomfort or pain for the purpose of + i - ms . administration i - v , is reduced many will mg . 
some cases are still surviving so that additional evidence concerning the diagnosis may be forthcoming in a few of these and the estimates of survival time are necessarily incomplete . it is reasonably certain that any such new evidence will increase the differences observed between the two series . the total numbers of cases are 46 in the x + i - vs series , of which one received compound only with no x - ray therapy and 45 in the x + i - ms series . the fate of every case is accounted for in the groups ( a ) to ( j ) of table ii . 
12 * 4 days ; for the 19 patients in the x + i - ms series , 4 received radical treatment and survived respectively 4 , 6 , 7 and 6 months , the mean m.t.d. 
mitchell by intravenous injection than with radiotherapy combined with the compound administered by intramuscular injection . preliminary clinical studies of the influence of the ancillary use of the compound on the survival times of inoperable cases of carcinoma of the bronchus treated by x - ray therapy are discussed in some detail and the end results summarised . the design of a clinical therapeutic trial of a radiosensitiser is discussed , with special reference to the evaluation of tetra - sodium 2 - methyl - i : 4 - naphthohydroquinone diphosphate m a radiosensitiser in the radiotherapy of inoperable cases of carcinoma of the bronchus . 
the results of this clinical trial are summarised to date . it is concluded that intravenous administration of this compound ( synkavit ) has a small but useful effect as a clinical radiosensitiser . in this work i have been helped by many colleagues at addenbrooke 's hospital . in particular i wish to thank a . 
7. received for publication june 19 , 1948 . the testing of substances for anticarcinogenic properties must proceed on purely empirical lines , or be based upon a hypothetical conception of the nature of some phase of the biochemical mechanism of chemical carcinogenesis . suggestive , but not conclusive , evidence has been obtained that s - metabolism is intimately connected with a primary stage in the interaction of chemical carcinogens with cellular constituents . 
crabtree in the groups receiving either the carcinogen alone or in conjunction with a substance which proved to be innocuous , the number of mice surviving the full all mice were epilated course of the experiment was always 90 per cent or over . over the scapular region once only , two days before the experiments began . the approximate amounts of carcinogen and tested substance used in any one experiment were as follows : 0 - 1l% 3 : 4 - benzpyrene 0 2% / methylcholanthrene 0 20 / 2.0% s - compound 1 : 2 : 5 : 6 - dibenzanthracene solutnused . 
a 0 1 per cent solution has been found most convenient , since with higher concentrations less obvious effects are produced by an inhibitor , and with lower concentrations the experiments are unduly prolonged , thus favouring any possible toxic action of the substance tested . 
with the strain of mice used , the average time for tumour induction with 0.1 per cent 3 : 4 - benzpyrene applied twice weekly is 16 - 0 i 0 1 weeks , a figure obtained repeatedly in many experiments . the substances tested were chosen for no other reason than that of convenience . 
when this occurred in the early part of an experiment and clearly reflected the toxicity of the substance tested , the difficulty was easily met by using smaller doses of the toxic agent . 
spicer. influence of bal on induction time . the results for bal have been analysed in two parts . those for bal and benzpyrene , where several percentages of bal were used , can be analysed using the technique of regression ( fisher , 1947 )  . that is to say a straight line is fitted to the mean induction times by the method of least squares ; if the slope of this line is significantly different from zero , then bal can be said to exert an inhibitory effect on the benzpyrene . the slope of the line is a measure of the efficacy of the bal . 
 " a lesser mass increment " of transplanted tumours was observed when the hosts were injected with diphenylsulphoxide or diphennylsulphone ( hammett , 1930 ) , and cystine disulphoxide proved inhibitory to the growth of spontaneous mouse tumours ( staff of the lankenau hospital , 1936 )  . conversely , compounds containing s in the reduced form , r.sh ( the nature of r appears to be of secondary importance ) , were shown to stimulate cell - division in a wide variety of plant and animal tissues ( hammett , 1931 )  . arising from these results it was anticipated that the increased proliferation of the cells in mouse skin induced by treatment with an sh - compound would render the tissue more susceptible to the action of a p - thiocresol was therefore applied in conjunction with a carcinogen , carcinogen . but the opposite effect was observed , i.e. 
the sh - compound caused a pronounced retardation in the rate of tumour induction ( reimann and hall , 1936 )  . reimann and hall performed a variety such inhibition stands in sharp contrast to the entirely innocuous behaviour towards carcinogenesis of the mono - thiol compounds used in the present work . the discrepancy can hardly be attributed to variations in the activities of the sh - compounds themselves , and must be referred to differences in experimental techniques . of experiments differing only in the amounts of carcinogen and p - thiocresol administered , and the timedistribution of their application . the actual doses of carcinogen varied from experiment to experiment , e.g.. 
the control group of mice received 2 - 4 times as much 1 : 2 : 5 : 6 - dibenzanthracene over the latent period as the groups treated with p - thiocresol , and this feature alone would suffice to account for the wide variations in average induction times , and the apparent inhibitory effect . moreover , the choice of lanoline as a solvent for p - thiocresol was unfortunate , since the work of twort and twort ( 1929 ) , rosicky andhatschek ( 1943 ) , simpson , carruthers and cramer ( 1945 ) , and berenblum and schoental ( 1947 ) , have shown that lanoline greatly retards the carcinogenic action of tar , 3 : 4 - benzpyrene , and methylcholanthrene . complicating factor augments the difficulty of accepting the experiments of reimann and hall as a demonstration of the anti - carcinogenic activity of sh - compounds . of the mono - sh - compounds used in the present work , together with the fact that bal , a di - sh - compound , can cause a moderate retardation of carcinogenic action , clearly signifies that the mere presentation of any sh - containing molecules ( as implied by the philadelphian workers ) is not in itself sufficient to produce a biological effect ascribable to the sh - group . experiences of peters , stocken and thompson ( 1945 ) in the search for a suitable sh - compound , which culminated in the discovery of bal , also emphasizes this . apart from the question of variable toxicity , which rules out a substance like the lack of activity this added 288 h . 
crabtree toluene - 3 : 4 - dithiol , it is evident that the total molecule , with sh - groups appropriately disposed , is a factor of importance . the analogy with the anti - vesicant activity of bal cannot be pushed too far , since experiments in vitro clarified the nature of the reaction between bal and lewisite , whereas any possible reaction between bal and a carcinogen , modified in an unknown way , cannot be attempted at present . lacassagne , buuii - hoi and rudali ( 1945 ) have ostensibly shown that competition between a potent carcinogen and a structurally related substance with their little or no carcinogenic activity can result in delayed tumour induction . work was an outcome of the conception that " the mutation which transforms a normal cell into a malignant cell is the result of the alteration of an organic substrate by the fixation to it of some toxic molecules ( in this case polycyclic chrysene , l : 2 : 5 : 6 - dibenzfluorene , five isomeric dimethyl - benzhydrocarbons )  . " acridines and a trimethyl - benzacridine were chosen as near relations of methylresemblance to cholanthrene , and 1 : 2 : 5 : 6 - dibenzacridine for its structural though they state in general terms that inhibitions 1 : 2 : 5 : 6 - dibenzanthracene . of carcinogenic action were demonstrated , the experimental details hardly justify so wide a conclusion , since only chrvsene and 1 : 2 : 5 : 6 - dibenzfiuorene caused some slight delay in tumour emergence . 
nordling. received for publication december 29 , 1952 . recent research in genetics and pathology has shown an amazing consistency between the agents causing mutations and those causing - or contributing to the one of the more prominent theories , which since the development of - cancer . 1920 's has been advocated by bauer ( 1949 ) , strong ( 1949 ) and others , claims that the original cancerous cell is nothing but an ordinary cell affected by genetic mutation of some kind . 
one of the main objections to this theory has been that it does not explain the age variation of the cancer frequency . in reply , bauer ( 1949 ) contends that the mutated cells apparently remain latent during a long period until the new qualities become evident and the phenomenon can be diagbauer has found this period of latency to average 9 years for nosed as cancer . x - ray cancer , 12 years for paraffin cancer , 18 years for aniline cancer and 40 years for seaman 's cancer ( caused by solar radiation )  . 
the early occurrence of sarcoma and of leukaemia , however , does not conform to the idea of a latent period . moreover , it appears somewhat unreasonable to suppose that the length of the latency period would depend upon whether the mutation is caused by sun - rays writh most forms of carcinoma , furthermore , the frequency at or by x - rays . different ages is such that wre are compelled to consider average latency periods of 70 years or more , in order to explain the actual age frequency curve of cancer these facts still make it difficult for many of the most commortality in man . petent authorities in the field to accept the mutation theory without reservations . dahlberg ( 1943 ) has advanced a completely different explanation concerning the relationship between age and cancer . 
he expressed the opinion that malignant tumours develop increasingly easily with rising age . this implies that , for the development of tumourous cells , it is necessary for a certain number of cellular divisions to have taken place , between each of which there has been a certain period of time . all experience concerning the cancerous influence of chronic irritations promoting cellular divisions seems strongly to support this theory . 
the number of mutations required for experimental cancer in mice may be less , as suggested by the investiobviously , we need not assume that any gations of iversen and arley ( 1950 )  . only mutations which increase the ratio seven mutations will cause cancer . between cellular divisions and cellular loss in a positive direction in the environaccording to fischer ment in question may be expected to have this effect . ( 1930 ) , the short average life - span of cancerous cells is their dominant feature , and that by which all their other qualities can be explained . their rapid propagation , which exceeds their high death - rate , their ability to ferment sugar on a large scale and to disintegrate heterogeneous proteins , constitute normal cellular responses to a high mortality among adjacent cells . it may be added that the frequent variability in the number of chromosomes among cells from the same tumour is also a " normal " feature in the sense that the same phenomenon also occurs in certain normal tissues , as shown by therman and timonen ( 1951 )  . thus , some or most of the mutations required to start an incessant self - stimulating propagation among a group of cells might consist of any of the forms of mutation that weaken the cell , and make it more liable to die from even minor disturbances . if cancer were caused by one mutation only , it might be expected to be equally common among persons of different ages after an age corresponding to the length of the latency period , if this period were interpreted as the time required by the first cancerous cell to multiply in such degree as to be diagnosed as cancer . 
nordling prevails in countries with a high percentage of deaths due to " senility " , " other and unknown causes " and the like , whereas the latter is the case in countries e.g. , the united states , new zealand , with detailed and reliable statistics , australia , great britain and other western european countries . it can be shown , as by nordling ( 1952 ) , that the cancer frequency curve of a population with undependable vital statistics will be restored to the same shape as that of the populations with accurate statistics if , as a rule , about one - fourth of the deaths due to such causes as " senility " are added to the registered cancer deaths . united states white population 1940 united kingdom 1939 france 1947 norway 1941 - 1945 000o = + = : + 14 at = ___x___ 200l asla42w 2 i - = 3 ___ _ - - _ 40 60 80 50 70 60 80 50 70 60 80 50 70 40 60 8u 50 70 fig . 
1. - diagram drawn to double logarithmic ( log / log ) scale showing the cancer death - rate ( in the case of the united kingdom , the carcinoma death - rate ) in males at different ages . deaths per 100 , 000 males are shown on the vertical scale , age figures on the horizontal scale . however , the very highest age - groups , which are always numerically small this is and certainly highly selected , can hardly be taken into consideration . because these individuals are usually already very frail and likely to die from any trivial cause , irrespective of whether or not they have cancer in a more or less developed stage . thus , it seems probable that , in reality , the age - frequency relationship for cancer follows the same general rule everywhere in the civilized world , although in these reliable examples can be given in only a limited number of cases . cases it is obvious , as is shown in fig . 
with regard to cancer among females , it is necessary to distinguish between cancer in the specificially female organs , of which the increase is fairly small above the age of 45 , and cancer at other sites , of which the frequency seems to increase according to the sixth power of age both before and after the forties , but not during the decade of the menopause , when the increase is smaller . it seems possible that altered hormonal conditions in connection with the menopause might play a part in determining the actual cancer frequency curve obviously , more slowly operating hormonal variations might among women . be present in both men and women . 
it is therefore by no means certain that the entire increase in the incidence of cancer with age is to be explained by means of the multiple mutation mechanism . it is possible that a small proportion of the increase is due to a lesser degree of hormonal inhibition of growth of potentially cancerous cells in an older organism than in a younger one . 
the writer is not , however , aware of any evidence definitely substantiating such a variability of natural cancer inhibition with age . during childhood and adolescence cancer is rare , but it occurs considerably in these cases it is more often than the sixth - power - of - age rule would allow . mainly a question of sarcoma , leukaemia and other non - epithelial forms of cancer . such a condition does not , however , imply any contradiction of the hypothesis since it is unlikely that mutaof successive mutations as the cause of cancer . genic noxae reach the bones and other internal tissues , it therefore seems more reasonable in the case of sarcoma to presume spontaneous mutations ( i.e. , mutations due to normal molecular collisions ) and radiation mutations as the such mutations may , of course , occur already in the foetal causative factor . in view of the extremely rapid growth during this period , it is not period . surprising that multiple mutations occasionally have time to occur , giving rise to infantile or even foetal sarcoma . 
the infrequency of malignant tumours in the striated muscles , despite their large volume , may have some connection with the fact that this kind of tissue is composed of multinuclear cells . according to the theory put forward in the present paper , cancer is caused by mutations multiplied and accumulated usually through large - scale proliferation it is easy to explain on this basis such facts as the ( sometimes inherited ) of cells . high susceptibility to cancer of certain organs , especially under experimental this is because every stimulant causing - or congenital capacity conditions . characterized by - a high proliferation rate also increases the number of mutated also the high susceptibility to cancer cells and thus the probability of cancer . of benign tumours is easy to understand in this way . the facts and theories advanced here demonstrate , among other matters , the importance of having reliable vital statistics in order to elucidate casual relationships in the pathogenesis of cancer . 
gutnz of untreated leukaemic cells observed in vitro . only the quantitative aspects of the subject will be dealt with here ; the cytological findings will be described in a separate paper . normal and leukaemic blood and bone marrow have been studied in tissue cultures by many workers since the publication of the first report on tissue culture of leukaemic blood by awrorow and timofejewskij ( 1914 )  . 
among other investigations carried out in recent years the following should be mentioned , as they deal wholly or in part with culture of leukaemic blood or marrow : papers by barnes and furth ( 1937 ) and bichel ( 1940 ) on mouse leukaemia ; doljanski and pikovski ( 1941 ) on fowl leukosis ; and fieschi and astaldi ( 1946 ) , israels ( 1940a , 1940b ) , osgood and brownlee ( 1936 , 1937 , as well as many later papers from the same laboratory ) , pierce ( 1932 , 1942 ) , schrek ( 1946a , 1946b ) , and wallbach ( 1936 ) , on human leukaemia . 
the vaccine caps are washed , and as rubber is toxic to living cells , they are then coated with a very thin layer of paraffin wax , by dipping them into a saturated solution of paraffin in petrol ether and wiping off excess after withdrawal . 
gunz been put into a conical flask , and the cells are now added to it , the aim being to give a final concentration of about 2000 leucocytes per c.msome practice is required in judging the correct volume of cells to be added . three consecutive counts are done on the cell suspension , and when the mean reveals a suitable cell concentration , a quantity of 2 ml . 
3. - mean daily counts of a sample culture of blood ( chronic myeloid leukaemia ) , expressed as per cent of initial count drawn on logarithmic scale . 6 days in the light of these two experiments , the following routine procedure has been thought justifiable : the mean of three counts of the original cell suspension is taken as the 100 per cent initial value for all tubes . 
on each subsequent occasion three separate counts are done on each of three fresh tubes , and the mean and standard error between tubes are calculated for all nine counts . 
means are calculated from the three individual counts and used for constructing the growth curve . in these differential counts a siniplified nomenclature of the myeloid series has been used , cells being divided into the three broad classes of myeloblasts , myelocytes and polymorphonuclears ( eosinophils and basophils being counted separately )  . 
the term " immature cell " comprises myeloblasts and myelocytes , the latter being arbitrarily defined as complying with two or all of the three following characteristics : total cell size exceeding that of a normal polymorphonuclear by 1 / 3 or more ; nucleus oval and only slightly indented ; cytoplasm basophilic . 
some of the patients with chronic myeloid leukaemia were untreated , while others had had various forms of therapy . cultures were either continued until all cells had died , or they were deliberately abandoned at an earlier period . 
when they were continued , there was always a gradual decrease in the total counts until death of the last cells occurred , usually between the sixth and the ninth day of culture . 
no significant increase in total counts has ever been observed . of especial interest is a group of nine cultures , selected because the cells lived for at least 7 days . 
4. - mean daily counts of a sample culture of blood ( chronic myeloid leukaemia ) , expressed as per cent of initial count drawn on linear scale . days log y = 2.0792 - * 0747x 7 days fig . 
6. - effect of 5 per cent rat embryo extract on culture of blood ( chronic myeloid leukaemia )  . total and differential counts expressed as per cent of initial count . 0 1 / 3 3 days of the total count in the two series are probably not significant , they certainly do not follow a straight line . 
of greater interest is the behaviour of the immature cells , in which a striking difference between the two series is apparent . while there is a gradual decrease of the number of immature cells in the control cultures , there is a significant rise in the e.e. 
cultures showing a peak of more than four times the height of that in the control cultures . results similar to these have been found in all cultures in which differential counts were done . 
6 ; the excess polymorphonuclears can have only been formed from immature cells , and the decrease in the number of the latter is explained by their proliferation failing to keep pace with maturation . after the second day , the process is less important and soon stops , mature and immature cells decaying approximately exponentially at the same rate , as shown in fig . 
may be a ribo - nucleoprotein , and experiments are now in progress designed to co - ordinate the growth curve with the nucleic acid metabolism of the cells . the action of ionizing radiations , as well as of many chemotherapeutic agents , is primarily on mitotic cells . in investigating these actions , every effort should therefore be made to provide the maximum number of mitoses in the test object . thus in fluid cultures the addition of e.e. 
de. from the chittaranjan cancer ho8pital , calcutta , india . received for publication january 4 , 1954 . the study of the effect of radiation on cancer cells presents problems of fundamental importance . it is still an open question in the field of radiobiology as to whether the ionising effect of radiation directly induces differentiation in cancer cers . 
he has also shown that radiosensitive and radio - resistant cancer cells react to radiation in a different way after a preliminary radiation . waren and dixon ( 1949 ) are of opinion that radiation does not induce differentiation of cancer cers . johes and koher ( 1950 ) remark that the apparent increase of differentiating cers after radiation on cancer cers , is only relative and is caused by destruction of other types of cells . glucksmann 's method of estimating the radio - sensitivity of cancer cells with prehminary radiation ' has been criticised by gricouroff ( 1952 ) who is of the opinion that radio - sensitivity and differentiation of cancer cells are related to stromal nutrition . thus it is evident from the literature that our knowledge of the mode of action on radiation is not decisive . 
our study was strictly confined to those cancerous areas which were characterised by anisocytosis , anisonucleosis , abundance of mitotic cells , loss of polarity of epithehal cells and just breakage of basement membrane . 
the induction of differentiation in cancer cells is one of such delayed effects . it is for this reason , that we have collected tissues , as mentioned previously , on the 7th day after first radiation with 7000 r , on the 21st day after the second 7000 r radiation and finally 3 months after a total radiation of 21 , 000 r . before coming to our problem proper , we made a comparative study of the cellular population of the differentiating phases of the stratified squamous epithefia of the normal cervix and of epidermoid carcinoma of the cervix . table i shows that the cell population of the differentiating phase of the normal cervix is 48 - 17 0 - 41 per cent compared with 3 - 57 + 0 - 14 per cent of the epidermoid carcinoma of the cervix . we find the incidence of the variation of standard error in post - radiation conditions is high . might be due to variation on the biology of cancer cells , and also to altered conditions of different patients . 
de the trend of distribution shows also significant changes after second and third 7000 r , but the ' t ' test could not be applied because the number of cancer positive cases decreased materially after the 2nd and 3rd radiation . our second problem is concemed with the possibihty of predicting radiosensitivity of epidermoid cancer of cervix after preliminary radiation with 7000 r . it has been shown previously ( table ii ) that after the first radiation with 7000 r , there was a uniform reduction of cancer cell population of both resting and mitotic phases , and similarly a uniform increase of cell population of the differentiating and degenerating phases . 
we have not found any differential variation in the four biological phases of cancer cells after preliminary radiation to distinguish a radio - sensitive case from a radio - resistant one , as has been found by glucksmann ( 1948 )  . in our present series of 91 cases , no cancer cers were found in the final biopsy after 21 , 000 r in 76 cases , which may be considered as radio - sensitive cases . cancer cers were persistent in the remaining 15 cases under similar conditions and they may be termed radio - resistant cases . on further analysis of our data , arranging them into final cancer - positive and cancer - negative groups after full radiation with 21 , 000 r , we do not find any significant variation of cell population in different phases after the preliminary radiation with 7000 r ( table iv )  . 
when the influence of irradiation on the number of cells in the different classes was examined separately after the first irradiation for radio - resistant and radio - sensitive groups of tumours , no significant difference was found between the two groups . we express our gratitude to the atomic energy commission under the government of india for a grant which has given us an opportunity to do this work , and also to the chittaranjan cancer hospital , calcutta , for facilities to work in the laboratories . we also express our sincere thanks to the staff of the chittaranjan cancer hospital , particularly to n . 
the animals were killed by cervical dislocation or by exsanguination under ether anaesthesia and the livers immediately perfused with 0 9 per cent sodium chloride solution before being removed , chilled and homogenized . 
nuclei were also prepared from the grch 15 tumour originally described by peacock ( 1933 )  . for the preparation of fowl erythrocyte nuclei the method of dounce and lan ( 1943 ) was used . in all cases the suspensions of clean nuclei were dried from the frozen state after small measured portions had been taken for dilution and counting in a haemocytometer . 
a weighed portion of dried nuclei acid - soluble 1 ( discarded ) nuclei 10% tca extraction residue lipid extraction phospholipid p residue n - naoh ab 370 insoluble 1 alkali - soluble 1 acidification acid soluble 2 precipitate dnap organic p inorganic p fig . 
2. scheme of separation of phosphorus compounds in nuclei ( modified from schmidt and thaunhauser , 1945 )  . was extracted three times with 10 per cent trichloracetic acid ( tca )  . 
the extracts were combined ( acid soluble 1 ) , but little attention was paid to this fraction since clearly much of the soluble p must already have been removed during the isolation of the nuclei . 
the extracted residue was treated with successive portions of acetone , ethanol , ethanol - chloroform ( 3 : 1 ) , warm ethanol - ether ( 3 : 1 ) and ether . these extracts were taken to dryness and the residue taken up in chloroform to form the phospholipid fraction . the dry nucleoprotein residue was incubated overnight at 37 with n naoh to hydrolyse rna to acid soluble nucleotides . 
the phosphorus which remained in solution was treated as organic phosphate ( fraction " organic p " )  . fractions " acid soluble 2 " and " organic p " should contain phosphorus derived from rna in the form of acid soluble nucleotides ( rntap )  . pentose was therefore estimated in " acid soluble 2 " by the orcinol method of mejbaum nuclei 10% tca extraction acid soluble 1 ( discarded ) residue lipid extraction phospholipid p residue 5% tca at 900 schneider extract schneider residue n nagh at 370 insoluble 2 alkali soluble 2 acidification acid soluble 3 precipitate ester phosphate inorganic p ester phosphate residue fig . 
3. - combined schneider and schmnidt - thannhauser procedure . ( 1939 ) and by the phloroglucinol method of euler and hahn ( 1946 ) , using calibration curves made from a purified sample of yeast rna , so that pentose could be read off directly in terms of ribonucleic acid phosphorus ( rnap )  . fraction " dnap " should contain phosphorus derived from dna only . deoxypentose was therefore estimated by the diphenylamine method ( dische , 1930 ) as employed by davidson and waymouth ( 1944b ) , using a calibration curve prepared from a purified specimen of thymus dna so that readings could be made directly in terms of deoxyribonucleic acid phosphorus ( dnap )  . phosphorus estimations were made on all samples by the method of allen ( 1940 )  . the optical densities of fractions " acid soluble 2 " and " dnap " were read in a beckman model du spectrophotometer at 260 m , u . 
and were read against a reagent blank . the radioactivity of each fraction was determined on a type m6 liquid counter ( 20th century electronics ) attached to a conventional scaling unit . ( ii ) the schneider ( 1945 ) technique . - a weighed portion of dried nuclei was extracted with tca and lipid solvents , as described above . 
the " schneider " residue clearly contained a mixture of phosphorus compounds , and it was therefore submitted to a schmidt - thannhauser separation by incubating in alkaline solution at 370 for 18 hours . 
to demonstrate them a separate run on a strip 57 cx 7 cwas carried out at a potential gradient of 13 - 6 volts / cfor 6 hours . after a run the paper was dried and the bands located by the ultra - violet light method of holiday and johnson ( 1949 ) and marked lightly in pencil . photographic records were made by the method of markham and smith ( 1949 ) , and occasional autoradiographs were made by leaving the paper in contact with kodak industrex type d film for about 18 days . the portions of the paper containing the bands were cut out and eluted according to consden , gordon and martin ( 1947 )  . 
davidson was determined by its position on the paper and its ultraviolet absorption spectrum . total phosphorus and radioactivity were also determined . the results of a series of analyses are shown in table i , in which the composition of bulk nuclei is given in terms of mg . 
although it might be expected that the schneider extract would contain all the phosphorus derived from rna and dna , the figure obtained for this fraction is invariably table ii . - mean values for the composition qf the single cell nucleus pg . 
at the same time the schneider residue , which might be expected to contain only phosphoprotein p , invariably shows a much higher phosphorus content than could be accounted for this discrepancy was observed by schneider ( 1945 , 1946 ) for by fraction p2 . whole tissue and has been commented on by davidson , frazer and hutchison that the schneider residue contains several different types of phosphorus ( 1951 )  . compound is made abundantly clear when it is submitted to a schmidt - thannhauser fractionation ( table i )  . the protein - bound inorganic fraction " p3 " obtained in this way corresponds roughly in amount to fraction " p2 "  . it therefore represents the true " phosphoprotein " phosphorus , and the other phosphorus compounds in the schneider residue are almost certainly derived from the nonnucleotide esters mentioned above , and from nucleic acid phosphorus which has failed to be removed in the schneider extraction although the portions of the nucleic acid molecules containing the reactive sugars have been split off from the this is clear from the fact that , in general , the figures for rnap protein . obtained by pentose estimation on the schneider extract agree with those obtained 206 w . 
davldson by pentose estimation on " acid soluble 2 " , while dnap obtained by the diphenylamine method on the schneider extract gives results which are comparable with those obtained from the schmidt - thannhauser dnap fraction . it is clear from table i that dry preparations of calf thymus and fowl erythrocyte nuclei have a much higher dna concentration and a lower rna concentration than have liver nuclei , but a quite different light is shed on the results when they are expressed as amounts of each component per nucleus ( table ii )  . 
4 , which is a photograph in ultraviolet light taken by the method of markham and smith ( 1949 )  . in the material from one sample of rat liver nuclei each nucleotide was submitted to hydrolysis with perchloric acid ( marshak and vogel , 1950 ) , and the bases so liberated examined by paper chromatography by the method of wyatt ( 1951 )  . in each nucleotide only the expected base and no other was found . it is clear therefore that nuclear rna is similar qualitatively to cytoplasmic rna . 
component b lies immediately behind component a , from which it cannot readily be separated . it is probable that component b consists essentially of the inorganic moiety associated with component a . 
component b should in fact correspond to fraction p2 derived from phosphoprotein . component d lies immediately in front of uridylic acid and component c in the space between b and d ; both c and d are organic in nature . it is clear therefore that fraction " acid soluble 2 " contains in addition to the expected ribonucleotides at least four other components of which three are organic phosphates . these components are clearly visible in the autoradiographs shown in fig . 
the incorporation of 32p into all fractions of fowl erythrocytes was so low as to make the results of the specific activity of the dnap in rabbit and rat liver is little significance . very low indeed as compared with the cytoplasmic fractions , but by contrast the specific activity of the organic p fraction which contains ribonucleotides is very in experiments in which we have compared nuclear rnap and high indeed . cytoplasmic rnap the former has always shown a much higher rate of incorporation of 32p than the latter ( davidson , mclndoe and smellie , 1951 )  . 
the high specific activity of nuclear rna is confirmed by isolation of the individual nucleotides . although there is no great difference between the activity of the nucleotides , adenylic acid tends to show the highest components c and d have activities of the same order as those of the activity . nucleotides , while the activities of components a and b together are considerably higher . 
the general pattern obtained from grch 15 tumour is similar to that for other tissues . the presence of components a , b , c and d is shown clearly in the autoradiograph in fig . 
5 , in which the areas of radioactivity are seen to correspond closely with the ultraviolet absorbing areas in the adjacent ultraviolet print . since the " dnap " fraction has a low specific activity and is precipitated from a solution of much greater specific activity , it is possible that this fraction may be contaminated with small amounts of phosphorus of high activity although it was therefore thought necessary to investigate it is washed several times . the effect of dissolving the " dnap " fraction in alkali and reprecipitating with one such reprecipitation reduced the activity by about 40 per cent , but acid . further reprecipitations proved to be unnecessary and indeed undesirable since in all experiments in which they tended to promote degradation of the material . ionophoresis was employed one reprecipitation of the dnap fraction was used . from table i it is clear that the specific activity of the dnap in rabbit and rat liver is very low indeed , and this is again evident in table iv . 
the dnap of the liver of the normal cock on the other hand has a much higher specific activity , while that of the dnap in the grch 15 tunmour , as might be expected in a rapidly growing tissue , is still higher and approaches the value for the riboit is of interest that the specific activity of the dnap in nucleotides ( table iv )  . the liver of the tumour - bearing bird is higher than that in the normal bird . 
on the other hand fairly convincing evidence for the loss of protein from the nucleus during the process of isolation from aqueous media has been reported by pollister and leuchtenberger ( 1949b ) and by dounce , tishkoff , barnett and frier ( 1950 ) , although this is contested by stedman and stedman ( 1951 )  . 
to what extent loss of rna and other phosphorus - containing constituents may occur during isolation in citric acid is quite unknown . it is clear from the results shown in table i that , as might be expected , the bulk of the phosphorus in the nucleus is present as dna , but the results of the schmidt and thannhauser procedure reveal considerable amounts of phosphorus in the " acid soluble 2 " fraction . that a large proportion of this fraction consists of the ribonucleotides produced by alkaline hydrolysis of rna is evident from the results of pentose estimations by the orcinol and phloroglucinol methods , and the results of the ionophoresis experiments have conclusively established the presence in nuclear rna of the four nucleotides which are found in rna 210 w . 
2. components a , c and .d are organic phosphates , the presence of which is responsible , in part at least , for the difference between the " organic p " fraction in table i and the rnap by the orcinol reaction . the presence of such esters has already been suggested by davidson and mclndoe ( 1949 )  . it is clear that in nuclear tissue , as in whole tissue ( davidson , frazer and hutchison , 1951 ; davidson and smellie , 1952 ) , the method of schmidt and thannhauser ( 1945 ) tends to give rather misleading results , since the rna fraction contains , in addition to ribonucleotides , considerable amounts of non - ribonucleotide phosphate . incorporation studies with 32p have revealed the rapid incorporation of the isotope into nuclear rna and its slow incorporation into dna in nongrowing tissues . although nuclear rna is much less abundant than cytoplasmic rna it is more active , as has been shown by marshak and calvet ( 1949 ) , barnum and huseby ( 1950 ) , jeener and szafarz ( 1950 ) and davidson , mclndoe and smellie ( 1951 ) using 32p and by potter , recknagel and hurlbert ( 1951 ) using labelled orotic acid . 
the present studies show that this more rapid rate of incorporation of 32p into nuclear rna holds for all four nucleotides , which become labeled to practically the same extent . the specific activities of components c and d are of the same order as those of the nucleotides 2 hours after administration of 32p , but that of the inorganic phosphate fraction is much higher ( table iv )  . this component corresponds to fraction p2 in table i and is derived mainly from " phosphoprotein , " although it may contain traces of inorganic phosphate originally present in the tissue . its presence is responsible for the fact that the activity of fraction " acid soluble 2 " is higher than that of " organic p . " the high activity of fraction p2 in whole tissue has already been commented on by davidson , frazer and hutchison ( 1951 )  . the results of the experiments on fowls confirm the observation of kelly and jones ( 1951 ) and kelly , payne , white and jones ( 1951 ) in rats that the presence of a rapidly growing tumour in the animal body leads to an increased incorporation of 32p into the liver dnap . 
this effect is still unexplained and obviously requires much further examination , since it is associated in our experiments with the rather high specific activity of normal fowl liver dna as compared with rat or rabbit liver dna . 
the high activity for the dna of the grch 15 tumour is in agreement with the results of other workers for rapidly growing tissues ( brues , tracey and cohn , 1944 ; davidson and raymond , 1948 )  . the results presented in table ii are of some interest in relation to the claims of vendrely and vendrely ( 1948 , 1949 ) and of mirsky and ris ( 1949 ) that the dna content of the cell nucleus is apparently constant for the cells of the different somatic tissues of any one species although there may be wide variations between one species and another . the implications of these observations have been discussed by davidson and leslie ( 1950a , b )  . 
as might be expected , no loss of dna from the rat liver nucleus too much stress however occurs on fasting , although the rna content falls . should not be laid on this latter observation , since the presence of minute amounts of cytoplasmic contamination could significantly alter the rna content of it has already been shown ( davidson , 1947 ) that fasting causes a the nucleus . marked fall in the total rna content of the rat liver , while the total dna content this would of course be expected if the dna content of the is unchanged . individual nuclei and the number of nuclei per liver were unaltered . in the grch 15 fowl tumour the dna content of the nucleus is approximately double that in the fowl erythrocyte or liver cell . 
the significance of this observation is as yet obscure , but a similar high value for tumour cells has been recorded by klein ( 1951 ) for several mouse tumours . 
the samples were frozen in cyhndrical tubes immersed in a quartz dewar vessel and were irradiated with filtered light from a high pressure mercury arc , either the 3100 a or the 3650 a group of hnes being used . under these conditions afl the molecules examined were strongly luminescent , showing both a short - lived fluorescence ( persisting for less than 10 - 8 seconds ) and longhved phosphorescence ( persisting for several seconds ) in different spectral regions . fluorescence spectra were traced photoelectrically using a hilger e2 spectrograph equipped with a scanning unit . phosphorescence spectra were photographed using a mechanical phosphorescope as described elsewhere ( lewis and kasha , 1944 ; moodie and reid , 1952 )  . 
the phosphorescence spectra are the result of excitation to the very lowest excited state of the carcinogen molecule , a " triplet " state resulting from the fact that there are two unpaired electrons . excitation of this state requires only about 45 k.cal. , much less energy than is necessary to break bonds in the molecule , and its formation may well be an intermediate step in the reaction with protein . in this connection it should be pointed out that the triplet levels , since they cannot be detected in absorption , the common method of observing spectra , have been much neglected by biologists in their considerations of low barrier reaction paths that may be involved in biochemical reactioins . ( 2 ) the second significant correlation comes from heterogeneous system experiments . 
we have found that ff a carcinogen is ' used as the microcrystalfne component and the dissolved component is naphthacene , the ( fluorescent ) emission of the naphthacene is shifted shghtly in wave length because of its interaction with the carcinogen . 
some of the results are it will be observed that the smallest shffts in the naphthacene show - n in table ii . bands occur when the strongest carcinogens are used as the host crystal . there is a moderately good correlation between these shifts and the self - polarizabihties at the position of the substituent calculated by greenwood ( 1951 ) , which values themselves correlate better with carcinogenic power than do an ' other physical constants . 
the technique for painting with the 03 per cent benzpyrene solution in - acetone was that described by calcutt and powell ( 1947 ) , and further treatment was as in earlier work ( weigert , calcutt and powell , 1946 )  . extraction and estimations of the metabolites were by the methods of weigert ( 1948 )  . the nutrient media used were as below : 1 . 
for a period of 8 hours . metabolism of the benzpyrene only occurred in the series on the four buffered in the case of the tap water and the normal saline the media were found media . to be turbid and the skins sodden and waterlogged . 
on the other hand , the variation in explanations of this based on the yields obtained is in itself of some interest . the detailed composition of the media used appear to be of doubtful significance . the outstanding point seems to be the ph of the medium . under the conditions of experiment it is reasonable to assume that the tissues of the skins concemed became adjusted in some degree to the environmental conditions , that is , that the internal state of the cells approximated more nearly to the external ph than would normally be the case . 
the question arises , therefore , as to whether such a state of affairs could influence the metabolic turnover . taking advantage of some recent findings , it is believed that an explanation of the results can be offered along the above lines . it has long been suspected that the process of carcinogenesis is intimately involved with sulphydryl groups . this view has recently been reinforced by crabtree ( 1948 ) , and the weight of evidence is now strongly in its favour . 
at the same time it has been suggested that the metabolism of benzpyrene is also mediated by - sh groups . this has received confirmation by the findings of 432 a . 
extremely active material capable of s " rdng fivsh t clours in less than two weeks has been obtained from both chemically induced and spontaneous sarcom firozen at - 790 c . 
since it involves the quesbon , first raised by ehrlich in 1907 , in connection with a possible bacterial source of cancer , of whether extreme cold can be used to destroy mammalian cells , and multaneously to preserve any posdble intraor extra - cellular agent capable of starting a t aour de novo in if the continued activity of such refiigerated tisme is cells of another host . aour produced in the due to new host is merely a transplant . if , however , it can be shown that the cers in the refrigerated tissue are dead , then the n6w tumour must be produced by an agent ( which would then be the " continuing cause " of cancer ) which is a separate .val of cells of the original anhml , then the t 260 w . 
craigie entity from the cells in which it lives , and which is capable of surviving under such transm , ission would be " cell - free , " certain conditions when they are dead . and would place any tumour so produced in the class of virus tumours , among the known virus chicken tumours , the shope papilloma of rabbits , bittner 's mammary carcinoma and lucke " s adenocarcinoma of the frog . the proof that prolongecl refrigeration kills mammalian tumour cells is difficult , and we are aware that in the past it has always been held , except by cramer ( 1930 ) , that the survival of only a few cells in the tumour mass accounts for the tumour in the new host . we have investigated the problem from a variety ofangles and have concluded , as will appear , that the cells are dead . jn the first place it must be realized that the sarcomas of mice which we have used are three well known to laboratory woikers , one a methylcholanthrene sarcoma ( c.48 in the inbred strain c57 black ) , and the other two arising as stromal transformations in transplants of sporadic mammary cancers investigated by r . 
none of these procedures affect the activity of the refrigerated tissue , which remains as great as or greater thirdly , we have made histological examinations than that of the fresh tissue . of frozen tissue implants at intervals and have examined the material itself , finding , - however , neither any evidence for survival of cells , nor conclusive proof of their total destruction , since one cannot be certain that every cell has been examined . finally , being well aware that to all these methods of approach might be opposed the objection of the remote possibility of the exceptional survival of a few cells , we have proceeded to dxy the refrigerated tissue completely to dust this is universally allowed to be lethal in vacuo at a temperature of - - 25 ' c . to both normal and tumour cells , yet we have obtained highly active dry material it therefore appears impossible to avoid from all the three tumours studied . the conclusion that from both the chemically induced and the sporadic sarcomas a cell - free agent can be recovered , which on injection into appropriate mice is capable of starting the tumour afresh . 
during this period attempts had been made again and again to propagate the tumour with cell - fi - ee filtrates and with dry tissue , and all had previously failed . ( 2 ) a sarcoma of the strain r3 . 
the sarcoma which formed from the stromal connective tissue was separated from the mamm ry cancer by ludford by early transplantations by which the slower growmg carcinoma was lost . ( 3 ) a similar sarcoma derived from the stroma of a carcinoma of the strain all three tumours are soft , rapidly growing sarcomas . 
the ' ampouilie - - s were then transferred to a storage cabinet kept at - 79 ' c . after an appropriate interv - al of hours , days or months , an ampoule was taken out , thawed to room temperature , opened , and 0 - 05 c.c. 
or less of the contents inoculated subcutaneously in the right flank of mice of the appropriate strawhen these ampoules were opened it was always noted that a physical change ha - d taken place in their contents , which had become more homogeneous , softer and slightly sticky after freezing . 
twe - four experiments were made with inoculations at varying intervals with uniform ] ' good results ( table 1 )  . it wiu be noted that in the last experiment on the time frozen makes no difference to the results . the list the material had been frozen 201 days , and was inoculated not only into its mouse of origin , but also into four other atains . 
refrigeration in van ; ow media . from experiments with mouse embryo tissue ( mann , 1949 ) we know that treatment with glucose ( without refrigeration ) reduces the activity of normal mamm lian cells , that storage in glycerol at 4 ' c . them , and that a combination of dextrose and cystein severely damages them , while fiwzing alone for one mour cells using glycerol , hour ik - ill them all . dextrose , eystein , and distifed water with and without fiwzing were therefore performed . table ii shows that these procedures , known to kill normal cells , have no effect on the activity of tumour tissue , dextrose indeed appearing definitely beneficial ( cmigie , 1949 )  . it wiff be noted that the results in table i and table 11 are very similar , and are condstent with the presence of a t nour agent other than a living mamm lian cell . 
as an example of the amount of man pulation which such t aour mince will stand we can cite the protocol of an experimentwith the c48 t ilour , carried various experiments with t 262 w . 
the mortar was then taken out of the c02 snow and solid frozen tissue and buffer pounded vigorously with the pestle , to break up as far as possible any remaining whole t thirty c.c. 
of cold distilled water was added , and when the mixture was finally hquid it was spun for 15 minutes at 10 , 000 revolutions a minute . ' the supernatant fluid was reddi - sh in colour and was of a ph 6 - 0 ; the deposit , firmly . 
of sahne ( - 85 per cent nacl in distffled water ) and the emulsion injected into six c57 mice . the mice developed ical c48 tumours , which were large on the 14th day . fibns of the emulsion were examined under the microscope and ' m none could a whole cell be found ; all that could be seen consisted of naked nuclei and separated masses of cytoplasm . experiments such as this do not appear to lend any aours started bv fi - ozen tissues are transplants , support t - o the belief that the t i.e. 
even there are even fewer apparentl - v intact bv the mincer . cells , while after treatment with glucose or with distified water profound changes appear affecting both nucleus and cytoplasa detailed studv of these changes is being made by one of us and wir be pubhshed later . a series of sections of implants of tumour tissue ( both sarcoma and carcinoma ) frozen to 79 ' c . 
by the fourth day much of this tissue is beiing absorbed and removed by the host , and on the fifth and sixth days and subsequently , the begi of a new sarcoma can be seen in the connective tissues surrounding the ne ; brotic mass . 
the appearances do not suggest survival of any of the implanted tissue , but rather a fresh sarcomatous reaction of the encapsulating in the case of frozen carcinoma also no living subcutaneous tissues of the host . tumour ceus were seen , and by the seventh day the decrotic m was encapsulated and shrunken . 
they were successful , as was also a similar experiment with the or tumour which wasaxied fresh by craigie . it has not so far been possible to obtain active dxied material from the c48 without preliminary storage at - 79 ' c . a brief account of the metbod of drying must be given , though for details of the apparatus used craigie 's paper ( 1949 ) should be consulted . 
the tissue to oule or , if freshly miinced , diluted be dried is either taken from the storage a v ' n ' th an eqltal volume of 5 - 3 per cent dextrose and is run into the drying flask . it sbould be distributed as evenly as possible over the bottom of the flask in a thin layer . 
ofm / 150 eystein ph added after cirying to zero , pumping is then continued for a further half or one hour to be absolutely certain of the removal of the last traces of wate ' r . 
of which is injected subcutaneously in each mouse . before this method of drying was evolved , many unsuccessful experiments with these tumours , using the knox method of drying , had been cam ' ed out . even now a successful res - ult - is not obtained in every case , and - much further experimentation will be required to determine the optimum conditions . 
raven. from the royal cancer hospital ( free ) and the gordon hospital for diseases of the rectum and colon . received for publication march 20 , 1948 . a study of the literature concerning malignant disease of the heart teaches that whilst primary tumours are rare , secondary deposits are not infrequently found . 
the following figures are illustrative . scott and garvin ( 1939 ) , in a series of 11 , 100 autopsies , including 1 , 082 performed in cases of malignant disease , reported secondary malignant disease as follows - heart , 79 cases ( 7 * 3 per cent ) ; pericardium , 61 cases ( 5 7 per cent ) ; heart and pericardium , 140 cases ( 12 * 9 per cent )  . willis reported an incidence of 6 - 2 per cent ; burke , 4 2 per cent ; helwig , 0 9 per cent ; pollia and gogol , 2 per cent ; lymburner , 0 6 per cent ; and symmers , 1 6 per cent . the subject is of more than academic interest , for with a better understanding it may be possible to establish a diagnosis during life in a greater number of patients , and the institution of certain forms of treatment , even though these are of a palliative nature . 
the symptomatology will therefore be reviewed , and attention drawn to the electrocardiographic findings in these patients . this paper is based on a series of 51 cases of secondary malignant disease of the heart which were collected at the royal cancer hospital from the autopsy records for the years 1930 to 1945 inclusive . 
the pericardium is usually involved and various types of disease are described . focal collections of carcinoma cells may occur in the epicardial fat , the cells being transported along the dilated lymphatics . in other cases the pericardium is studded with nodules of growth , whilst a third variety consists of diffuse pericardial infiltration , and this process may extend into the pericardial fat . there may be commencing infiltration near the commencement of the great vessels . another variety comprises flat plaques of growth embedded in the pericardium . in a number of cases there is combined involvement of the pericardium and heart muscle . 
tumour cells were seen in the lumen of a small arteriole ; obviously the disease in the heart was conveyed by the blood stream . in another case nodules of growth were found in the muscle of the right auricle , left ventricle and left auricle ; some of these were situated beneath the endocardium and growing into the auricle . 
the microscopic picture was similar to that of the primary skin tumour . in the third case an amelanotic nodule was present in the upper and posterior part of the left ventricle , from which more extensive spread had occurred into the heart muscle . moragues ( 1939 ) reviewed the subject of cardiac metastases from malignant melanoma and found reports of 23 cases in the literature , to which he added 4 in one of these cases there were signs of cardiac involvement ; personal cases . a loud systolic murmur was present in the pulmonary area , caused by a large tumour mass which almost occluded the pulmonary orifice . the spread of malignancy to the heart . this occurs by the usual four methods , namely , haematogenous , lymphatic , in this combined haematogenous and lymphatic , and by direct extension . series of cases there was definite evidence of all these modes . 
any subsequent abnormality which is noted can be compared with this initial investigation and inferences drawn . in cases with tumours of the heart , carnot and lambling ( 1928 ) have described a clinical syndrome which resembles that of subacute bacterial endoapart from this group of cases , attention is called to certain symptoms carditis . and signs which suggest cardiac involvement in patients known to be suffering from malignant diseases , especially of those organs which are recognized to give rise to secondary cardiac deposits . dyspnoea , tachycardia and cardiac irregularity are frequently outstanding symptoms , the irregularity being of the nature of either auricular fibrillation or auricular flutter . 
the symptoms may be correlated with the location of the tumour in the heart , causing heart block , or due to a pericardial or pleural effusion . it must not be assumed , however , that evidence of pericardial disease in a patient with malignancy is pathognomonic of involvement of the pericardium ; acute pericarditis may occur in the advanced phase from other causes . 
amongst important signs are those of cardiac enlargement and dysfunction , impaired resonance of the chest , the presence of abnormal breath sounds and added sounds . cyanosis may be present and the signs of cardiac failure . in the presence of this symptomatology certain investigations are carried out . 
when a pericardial effusion manifests itself , paracentesis is performed and cytological examination of the fluid is made . in a number of cases malignant tumour cells will be demonstrated . radiological examination of the heart , including tomography , is regarding the electrocardiographic out . findings , the case reports in the literature do not show uniformity ; the results vary according to the position of the tumour in the heart . siegel and young ( 1933 ) , dealing with this aspect of the subject , call attention to the work of lloyd ( 1929 ) , who published the first electrocardiogram in a proved case of tumour of carried r . 
the t waves in leads 1 and 2 were slightly diphasic . had been given before the patient was admitted to hospital , which may account siegel and young ( 1933 ) reported the for the abnormality of the t waves . findings in a case of metastatic sarcoma of the myocardiuthe t waves were inverted constantly in all leads , and there was no significant change daily . 
when the primary tumour is known to be radiosensitive , high - voltage x - irradiation may prove of value in the diagnosis in these cases clinical of metastases in the heart when enlargement is present . and radiological evidence may be forthcoming of a marked reduction in the size of the heart and the disappearance of the pericardial effusion . shelburne and aronson ( 1940 ) report the effects of high - voltage x - irradiation in a patient with metastases in the heart and pericardium from a primary myeloblastoma in the frontal bone . 
1. received for publication january 21 , 1948 . surgery in the form of the so - called radical operation is in general at the present time the principal weapon in the treatment of carcinoma of the breast . what it can achieve and its limitations are now fairly well established . 
thus it is known that if a patient with carcinoma of the breast has microscopical invasion of the axillary glands , the strong probabilities are that the disease has passed beyond the local area and that the patient will sooner or later succumb it is to the disease , although there will be a minority of fortunate exceptions . also known that if the axillary glands are not invaded the chances that the patient will be cured of the disease are appreciably increased . 
with a stroke of 6 cat a rate of 90 per minute , and melanin formation estimated at appropriate intervals by observing the extinction coefficients of the solution with an e.e.l. 
on 15 occasions there was acceleration averaging approximately 0 - 3 per cent as compared with the control . on the assumption that the errors inevitably present will tend to operate equally in either direction , the probability of obtaining 15 results out of 17 in one direction is ( approximately ) only i in 500 , so that the results are statisticany significant . the possibility of the acceleration being due to change in ph was reconsidered . the ph of the various solutions employed was estimated , electrometrically , using a glass electrode . 
1. - lung cancer in denmark , 1931 - 1945 . 1931 33 35 crude mortality rate per 100 , 000 in males 43 45 39 41 alterations in the age distribution of the population might be suggested as the cause of the rise in crude mortality from lung cancer , but if we compute the mortality rate according to age in the capital for periods of five years , and on the base of quinquennial age groups of dead and living persons , as in fig . 
2 , we find no confirmation of the suggestion mentioned . thus , we have found a very steep increase of mortality from lung cancer within a limited area , well furnished with modern medical facilities , available to all social classes . * the increase is found among both sexes , but is far more pronounced for males than for females , and it will be worth while further to analyse the population in question with regard to the incidence of lung cancer , as copenhagen seems to provide a good example of the changes in the mortality from lung cancer found elsewhere in europe . the central tuberculosis station of the city of copenhagen provides excellent opportunities for checking up the reliability of statistics given in the first part in its work to trace tuberculous infections in patients of the present paper . suffering from all sorts of respiratory diseases , this institution performs numerous thorough examinations on such patients referred from general practitioners . annual reports contain tables giving the number of patients , subdivided in decennial age groups for each sex separately . 
the group examinations under * for members of the public health insurance , which comprise 85 - 90 per cent of the danish population , no fees are charged in the municipal hospitals of copenhagen . 
3 , shows no steady rise , and hardly any irregularity is found in the curve for females , which , however , comprises very few individuals , as seen from the absolute figures . the very steep rise of the male curve about 1941 may have been caused by the fact that the efficiency of a central tuberculosis station may also have increased if the duration of the disease is one or two years in a disease like lung cancer . from its earliest possible detection to death , and this is , in fact , the opinion of the tuberculosis station , the steep rise in 1941 given in fig . 
even if we allow for the small absolute values of the figures , it can be said , as with regard to the corresponding mortality figures , that there is no increase of morbidity in the young , as would be expected if the inerease was due to an increase in the inhalation of tobacco smoke , if we are not to assume a latent period for lung cancer of about two decades . in our opinion the figures given illustrate that even a pronounced increase of the crude mortality rate for lung cancer among males , and almost only among males , does not necessarily mean an increase in incidence of that disease . presumably the more frequent detection of the disease is due to improvement of 2s~~~~~~~~~~~~~ __ _ 120 ___ __ 80 __ f - ~i 40 ' j years fig . 
if the results from copenhagen can be generalized , it seems that the apparent increase in lung cancer mortality is , to a very large extent , conditioned by improvements in diagnostic means , and it can be expected to continue until the sex ratio amounts to about 8 males to 1 female . our thanks are due to knud winge , m.d. , the chief physician of the central tuberculosis station , copenhagen , for permitting us to use the material of the station , and for his kind interest in our work , and to kontorchef miss m . 
1. received for publication december 1 , 1952 . it has for long been an accepted principle that the earlier the diagnosis of malignant disease is made the more likely it is that the growth , if in a region of the body accessible to the surgeon , will be in a stage which admits of radical resection and the higher will be the survival rate . 
however , balfour ( 1937 ) recorded that the 5 - year survival rate for 2112 patients after resection of the stomach for carcinoma was 25 per cent for those patients with histories of symptoms for less than 6 months and 35 per cent for those with histories of symptoms for more than one year . 
walters , gray and priestley ( 1942 ) in a later study recorded that 24 * 6 per cent of patients whose symptoms were of less than one year 's duration survived 5 years after resection of the stomach for carcinoma , whereas 32 - 6 per cent of patients the duration of whose symptoms was more than one year survived 5 years . 
the authors investigated the association between the length of history and the grade of malignancy as judged by broders ' classification , and give a table which shows that 39 of the 114 patients had growths which were classified as broders ' groups i and ii , while 75 had growths classified as broders ' groups iii and iv ; in each case the proportion of patients who gave histories of symptoms for more than 2 years was 23 per cent . eggers , de cholnoky and jessop ( 1941 ) reported that while the 5 - year survivals of 235 patients who had undergone radical .mastectomy for cancer of the breast fell steadily from 76 per cent to 20 per cent with delay in treatment up to 2 years , the survival rates rose to 25 per cent of 20 patients in whom the delay was over 2 years , and to 40 * 9 per cent of 22 patients in whose cases - there had been delay of 3 years or over . 
harnett tomies for cancer of the breast , found that 24 - 8 per cent of the 938 5 - year survivors were treated more than one year after recognition of the tumour ; he considered that the majority of these cases were the indolent , slowly - growing types of breast carcinoma , which metastasized late or occurred in hosts whose desmoplastic reaction to the tumour was intense . 
bloom ( 1950a ) in an analysis of 470 cases of cancer of the breast treated by surgery alone or with ancillary radiotherapy found , after classifying them into 3 groups according to histological criteria of degree of malignancy , that 79 per cent of 141 cases graded as of low malignancy survived 5 years , 42 per cent of 191 graded as of moderate malignancy and 25 per cent of 138 graded as of high malignancy ; when the histological grading was subdivided according to the presence or absence of invasion of the axillary lymph nodes , he found that with lymph nodes not invaded the 5 - year survival rates for gradesi , ii and iii were 94 , 61 and 53 per cent respectively , while for patients in whom the lymph nodes were demonstrated histologically to be invaded the survival rates for the three grades were 65 , 30 and 16 per cent respectively . 
as all types of treatment , surgery , radiotherapy and combined treatment , whether radical or palliative , were included , it is not surprising that few significant differences in survival rate were detected , though in most regions it appeared that the patients treated early showed little better survival rates than those who came late . in the present communication tabulations are presented from the same series of cases of the results of treatment of patients in stages i , ii or iii , who were treated by radical surgery alone or combined with radiotherapy , arranged according to duration of symptoms at the time of commencing treatment . 
by the elimination of all patients who were in stage iv , and of those in whose cases only operations of a palliative nature were performed , the series is restricted to those in whom there was a reasonable expectation of 5 - year cure . patients treated by radiotherapy alone have been excluded , because it is difficult to separate those in whose cases the treatment was intended to be curative from those in which it was palliative only , though some of the latter survived 5 years . the cases are grouped by site of the disease and by duration of symptoms at the time of commencing treatment into ( a ) , those in which the interval from first symptom to commencement of treatment was less than 6 months , ( b ) , those in which it was between 6 and 12 months , ( c ) , those in which it was more than 12 months , ( d ) , those in which it was unknown . 
the 5 - year survival rates for each of these groups is expressed as a percentage of the total in the group , and the standard errors of the differences have been calculated to test for statistical significance . in the more important sites the survivals are shown by stages : i . 
survd. over 12 , , not known the differences in survival rate are not statistically significant . for cases of known duration x2 = 1x77 , n = 2 , p < 50 > 30 . . 
among 383 patients treated by radical mastectomy alone , 35 - 5 per cent were in stage i and the best survival rate for all stages combined was 50 9 3 - 3 per cent for those treated during the first 6 months ; among 175 who were treated by radical mastectomy combined with radiotherapy only 21 * 1 per cent were in stage i and 43 * 4 per cent were in stage iii , and the best survival rate for all stages combined was 58 - 8 8 - 4 per cent for patients treated one year or more subsequent to the first symptom , who numbered 34 . 
the difference of 7 - 9 9 0 between these survival rates is not statistically significant . when the sites were subdivided into those in which the highest survival rates were among the patients who came under treatment in less than 3 months and those in which the highest rates were among those treated in the second 3 months , it was found that the former included squamous carcinoma of the skin , corpus uteri , penis and female breast with a survival rate for all groups of 54 - 9 per cent , while the latter included cervix uteri , kidney , .papillary carcinoma of the bladder and carcinoma of the pharynx ( treated by radical surgery or by combined methods ) with a 5 - year survival rate for all groups of 51x0 per cent . the age distribution of 702 patients with cancer of the breast who were . 
the group of 63 in whom the symptoms were of over 12 months ' standing at the time of operation had a survival rate of 14 3 per cent ; the difference of 9 9 7 0 between this figure and that for the group treated in the second 6 months is not statistically significant . if the patients are grouped into those of less than 6 months ' duration , with a survival rate of 11 - 2 per cent , and those of over 6 months ' duration , with a survival rate of 19 - 2 per cent , the difference of 8 - 0 4 - 7 is not significant . the age distribution of the patients with cancer of the stomach and colon were investigated by the x2 test , but in neither case were there any significant differences between the observed and expected survivals in the different age groups ; for the stomach cases p < * 20 > * 10 and for the colon cases p < - 70 > .50 , showing that the differences in survival rates were not due to differences in age distribution . 
the survival rate for cancer of the stomach was 20 - 4 per cent for 108 patients in the age groups 25 - 54 and 11.1 per cent for 133 patients of 55 and upwards , but the difference of 9.3 4 - 7 is not significant , though the prognosis was not so good in the older patients . 
as has been stated above this difference cannot be accounted for by differences in the age distribution of patients in either of the groups , so it must be presumed to be due to variations in the rate of growth of individual tumours all cases of patients with and in their infiltrating and metastatising powers . distant metastases have been eliminated from the present series , which was confined to those in which the tumour was local or had given rise to clinically recognisable metastases in lymph nodes ; they were selected as operable cases , no patient in an advanced stage or suitable only for palliative treatment being small differences were found in the proportion of patients in stage i included . among those with the highest survival rate in each of the three groups ; for group w . 
the mean duration of life in 153 untreated patients in group a was 23 - 1 months , of 176 in group b was 11 - 7 months and of 296 in group c was 17 - 6 months . 
the sites showing the longest survivals among the untreated patients are those in which treatment by radical surgery alone or with radiotherapy gives the best results , although some sites show a short duration of life , either because , as in the case of the lip , very few cases are left untreated , or because , as in the case of the colon and the intrinsic larynx , untreated patients often die of complications , such as intestinal w3w . 
group a included the skin ( squamous carcinoma ) , corpus uteri , penis , cervix uteri , female breast , kidney , bladder ( papillary carcinoma ) and pharynx . for this group of sites , comprising 1097 cases of known duration , the best survival rate was 51 1 per cent of 616 patients treated in the first 6 months against 42 - 0 per cent for the remainder . 
group b included salivary glands , tonsil , testis , colon , skin ( malignant melanoma ) , nasal sinuses , bladder ( infiltrating carcinoma ) and stomach . this group of sites , comprising 718 cases of known duration , the best survival rate was 30 - 6 per cent of 134 patients treated in the second 6 months against 27 1 per cent for the remainder . 
a blank estimation was carried out on the reagents and in the latter half of the investigation a weighed amount of the filter - paper surrounding the discoloured areas was included in the blank , but this addition makes no considerable difference . occasional very high blanks were discarded as due to some unusual contamination . 
3. - mean seasonal variations in arsenic content of air at eight stations . w = winter ( november to march ) ; s = summer ( may to september )  . establish any exact comparison between the seasonal changes in the individual richard doll has pointed out to us that , the average values for the towns . different stations would be more properlv comparable , in view of the seasonal variations , if ( 1 ) the means of two figures for the same month and town were taken to represent that month , and ( 2 ) the mean of the figures for two months which are separated by a gap of one month without data were taken to represent that month . 
one might suggest some such classification as the following of the not very abundant data available upon the types of sunmmation ( table ii ) ; no claim is made that this is in any way a complete summary of the literature . 
the summation of action of two chemical carcinogens is not easy to demonstrate , and we appear to have few indubitable instances of it . * in connection with the subject of cancer of the lung , the work of lynch ( 1935 ) and andervont ( 1937 ) upon summation in the lung of some strains of mice is of especial interest , although the neoplasms of the lung in this species differ from those in man . 
a few small arterioles present in the floor and edges of the ulcer showed no evidence of endarteritis . at one point the tumour had penetrated the periphery of the pancreas for a there was no involvement of the common distance of approximately 2 nun . 
5 , showing invasion of the submucosal connective - tissue strata by adenocarcinoma which has , on left - hand side , lost all resemblance to normal brunner 's gland acini . 
hence there can be no reasonable doubt that it is primarily duodenal . histological appearances clearly indicate that the initial neoplastic change has involved the epithelium throughout the whole thickness of the mucous membrane , including brunner 's glands . 
phillips. from the national cancer in8titute of canada , 800 bay street , toronto 5 , ontario . received for publication april 3 , 1954 . within recent years evidence has been brought forth on variations in the distribution of ' cancer in different parts of the world . cancer of the base of the tongue , for example , is relatively frequent in certain parts of india and primary cancer of the hver is relatively frequent in africa and indonesia . cancer of the stom - ach on the other hand , is relatively infrequent in african negroes , javanese and the indigenous people of french north africa . such observations have focused attention upon racial origin , environment and custom as i ' mportant factors in the study of cancer . in 1950 at a conference on the aeo - araphical pathology and demography of cancer ( clemmesen , 1950a ) it was agreed that a high degree of comparability is desirable in any study of geographical variation . 
phillips the origin of the north american indian remains uncertain , but anthropologists beheve that they came to america in successive migrations in prehistoric times from northern asia , probably by wa of the bering sea . 
the primary function of this branch is to administer the affairs of the indians of canada in a manner that will enable them to become inereasinglv self - supporting and independent members of the community . health services to indians date back to the early part of the seventeenth century when french armv doctors gave medical care to this group . 
the indian health service operates 18 hospitals and 29 nursing stations giving a capacity of approximately 2287 beds . across the country there are 65 full - time doctors caring for indians . there axe also 90 pubhc health nurses assisted by provincial public health nurses , red cross outpost nurses and the ceintres range in size from the 456 - bed charles victorian order of nurses . camser indian hospital at edmpnton , alberta , to small units of 16 to 20 beds . in addition the services of some 380 community ' and private hospitals are utihzed for the treatment of indians . the indian health service has been faced - with a number of problems of which tuberculosis , inadequate nutrition and high infant mortality are the most serious . 
phlllips when an indian receives medical care a record of his case is forwarded to the this record gives , among other data , national office of the indian health service . the patient 's name , band number , age , sex , diagnosis , and days of hospitahzation . with such information available the patient - records in forty - eight hospitals were reviewed for the years 1948 - 1952 inclusive and all cases of cancer were selected for analysis . 
the indian health service has estimated that over 90 per cent of indians with cancer would be referred to ' the hospitals included in this study . in the five years which were reviewed , 327 cases of cancer were re - ported , 125 in males and 202 in females . 
the finding that cancer is less frequent inindians over 30 years of age than in whites over 30 years of age is to be accepted with caution . " ir - defined causes " are reported in death certification more frequently ( table 11 ) for indians and it is possible that illness and deaths from cancer may he within this group and which , if properly reported , would raise the incidence rates for older indians . in other words , the observed difference in total cancer incidence rates between indians and whites may be more apparent than real . it is possible that skin pigmentation of indians acts as a protection against skhi cancer in the same way as for the black race . however , it is also possible that skin cancer cases did not come under medical care but we doubt this because the incidence of other sites , excepting cervix , was the same as in the white population . the most interesting finding is that relating to the high incidence of cancer of the cervix uteri . 
phillips over this age the incidence of cancer among indians is apparently less than among whites . cancer of the skin occurs less frequently among indians . the incidence of cancer of the cervix uteri is much higher among indians than that reported for the white population in canada and the disease tends to occur earlier in life . the incidence rates for all other sites of the disease show no difference between indians and whites . the authors wish to acknowledge the assistance of p . 
the rats were 4 weeks old when these operations were performed and 7 days later the litter - mates were joined in parabiosis . the surgical technique used was the one recommended by jacobsohn ( 1948 )  . in most pairs both partners were females except in those forming groups iii and vii , where a castrated male took the place of the spayed female . 
a total of 10 to 25 doses was given , when possible in a schedule of 3 doses per week . occasionally , this dosage had to be reduced to one or two administrations per week when the pair failed to show the expected gain in weight . twenty - six pairs of albinos ( groups i , ii and iii ) and 3 pairs of piebald rats 332 f . 
by stomach - tube during the first 8 weeks of the experiment . these rats , hke the majority of the parabiotic pairs , were 2 to 21 months old when the administration of the carcinogen was commenced , and served as controls for the assessment of the carcinogenic activity of the amounts of a.a.f. 
the parabiotic rats were sacrificed when declining health , in most instances due to the preserice of large pyometra , made it advisable or when the presence of a tumour was suspected . 
two of the " single " rats were killed when a palpable tumour was present , the remainder when the experiment was terminated at the 52nd week . the material taken for histological study was fixed in zenker , and the sections were stained with haematoxylin - eosin or according to van gieson . 
the tumours originated in gonads which were grossly hyperplastic . the histological changes occurring in the ovaries of rats joined in parabiosis to gonadectomized litter - mates have been well described by zeckwer ( 1944 ) , therefore our findings will be mentioned only briefly . 
the wall of these cysts was smooth , and when an epithelial lining could be recognized the cells were low cuboid or flat without any indication of cellular activity . such cysts occurred equafly in intact partners treated with a.a.f. 
the earliest neoplasms seen were generally round in sfiape and had a diameter of 3 to 4 mthey were found in wistar rats of groups i to iii after 16 to 20 weeks of parabiosis ; in piebalds they occurred even earlier . 
the largest gr ' anulosa cell tumour which had destroyed completely the ovary in which it originated measured 27 x 16 x 25 mand it was the only neoplasm of this kind to produce a metastasis , weighed 3 - 88 g . the secondary being situated in the adhesions linking the primary to neighbouring organs . the material at our disposal allows the study of the development of granulosa fig . 
2 shows a large haemorrhagic cyst cell tumours from their early stages . found in an ovary of rat 1 , group iv , sacrificed at the 13th week of the experiment . this cyst had a thin wall formed b fibrous connective tissue which in most places was poor in cells . in some areas the capsule was thickened , and here signs of previous haemorrhage such as pigment - loaded macrophages were present . into the cavity papillary projections protruded . 
they were of two kinds , some into the former , delicate strands with a narrow and others with a broad base . of spindle - shaped cers entered , forming their core . into the latter , capinaries penetrated surrounded by cers having ample eosinophihc cytoplasm , and a nucleous less rich in chromatin than the cells which covered and formed the bulk of the projections . these had a nucleus rich in chromatin and a scanty cytoplasthey were typical granulosa cells , while the ones having ample cytoplasm this was the earliest neopalstic lesion found in our resembled lutein cells . material , and shows that atypical growths of this kind were not necessarily permanent ones . 
and killed after more prolonged parabiosis hae ' morrhagic cysts , where only small nests of granulosa cells remained embedded in the dense connective tissue of the capsule while the cavity contained only inspissated blood and tissue debris . such chocolate cystlike lesions were absent from the ovaries of the control pairs not treated with a.a.f. another animal of the same group sacrificed 2 weeks , later was found to have in the ovary a macroscopically visible nodule formed almost entirely by granulosa cells . it was of about the same size as the early granulosa cell tumuor depicted in fig . 
3 shows a sharply limited spherical nodule situated in an ovary containing cystic follicles . it was surrounded by a thin fibrous capsule . between the capsule and the neighbouring cystic folhcles were large blood - fifed sinuses . 
5 shows the appearance of the granulosa cells forming the bulk of the nodule , and the tendency towards foci of liquefaction leading to the formation of cystic spaces within the tumour . 
the tumorous right ovary of rat 5 , group 111 , showed histologically an unusual picture . this ovary was also considerably enlarged ( 802 mg . ) and fairly solid with only a few blood - filled cysts only a small rim of ovarian tissue remained ; most of the near its surface . histologically this tumour was composed specimen was obviously neoplastic . mainly of spindle - shaped cells with scanty cytoplasm , and a nucleus which varied considerably from elongated dense to oval or spherical vesicular . 
among them small groups of cells were present having ample cytoplasm which stained well these elements had a larger vesicular nucleus with the chromatin with eosin . displaced towards the nuclear membrane . 
we have classified this neoplasm as a theca cell tumour because the granulosa contributed only little to its make - up . in the 36th week of the experiment the health of the intact partner suddenly declined and therefore in the region of the left ovary there was a large blackish the pair was sacrificed . cyst , on the posterior wall of which some ovarian tissue was recognizable . 
two types of neoplastic cells could be distinguished : bizarre cells of unusually large size having one or , rarely , their cytoplasm was several nuclei with deeply stained prominent nucleoli . intermi ' ngled with these elenients ample and stained only weakly with eosin . these were polyhedral in were nests of much smaller cells of epithelial character . shape and had well - marked cell borders , in cohtrast to the large elements which tended to form svnvctia . 
 ( groups v , vi and vii )  . the only lesion suspicious of atypical growth was found in one of the ovaries of an intact female which survived parabiosis for 42 weeks ( group v , rat 8 )  . 
we are unable to state with certainty that this lesion was of neoplastic nature . as already mentioned , no ovarian tumours were found in the 10 " single albino rats which received 24 doses of 4 mg . 
among many hundred female rats treated with this carcinogen we have found only one instance of a neoplastic lesion in the female gonads . this was discovered in a rat 171 months of age when sacrificed . 
by stomach - tube when 2 months old ; then the animal was kept without further treatment for 1 year , and for the last 16 weeks of her life she received methyl - thiouracil in the drinking water . 
at the post - mortem the left ovary was found to be converted into a large cyst measuring 20 x 15 x 10 mm . on histological examination septa subdividing the cyst in several compartments and covered with granulosa cells were seen . although macroscopicany this cyst resembled the clear cysts which we have frequently found in the ovaries of parabiotic females and also in rats treated with stilboestrol , we have never observed in such structures prohferation of granulosa cells exce ' t in this one instance . the morphological 8ign8of the endocrine imbalance exi8ting in the intact partner . all signs of hyperoestrinism were present in the intact partner ( zeckwer , 1944 )  . 
the vagina was lined by hyperplastic squamous keratinizing epithelium . in the few instances where the uterus was not heavily infected the epithelium lining the cavity was tar cyhndrical and areas of squamous metaplasia were also present , the wall of the organ being thickened . in the infected uteri most of the epithehum was destroyed . 
the breast glands were grossly hyperplastic , and in most animals macroscopicary visible cysts fired with a milky fluid were seen . histologically such glands showed a pronounced cystic hyperplasia of the ducts and periductal fibrosis . 
the thymus was atrophic , and the suprarenals enlarged in size due to a hyperplasia of the cortex . the pituitaries of the intact partners were invariably larger than those of the gonadectomized litter - mates , and already after 15 to 17 weeks of parabiosis had increased to an average of 8 mg . 
the largest observed ( rat 6 , group iii , and rat 8 , group v ) reached the extraordinary weight of 74 - 8 and 139 - 3 mg . 
the pituitaries of the intact partners were mostly solid and of whitish colour and haemorrhagic areas while the majority of these glands showed a symmetrical were not conspicuous . enlargement of the anterior lobe , in females surviving for more than 25 weeks of irregular shape . 
at the experiment the pituitaries assumed an ever - increasin first small whitish or sfightly yerowish nodules appeared which were single or multiple . later on the normal shape of the gland became more and more obscured by irregular growths , which compressed but never invaded the brain . the larger the tumour the greater was the tendency for brownish discoloration . these lesions occurred in intact partners independently of whether a.a.f. 
common to many of these elements and independent of the degree of acidophilic granulation was the pecuhar golgi apparatus which in papanicolaou preparations appeared as a ring - like structure , the negative golgi fig . 
17 , shows that the majority of the cells composing this structure were degranulated with only a few acidophils remaining . in the more advanced adenomata of the pituitary more atypical cens appeared but fundamentary they did not differ from the earlier lesions . in our material we have rarely seen adenomata completely free of acidophils . 
to conclude , we consider the nodular structures to be adenomata derived from cells of the acidophil series . tumour8of other organ8ob8erved in intact partner8and in " 8ingle " rat8of group viii treated with a.a.f. in the rats of group viii three adenocarcinomata of the breast and one squamous ketatinizing epithelioma of the extemal auditory meatus were found ( table iii )  . 
two of the cancers appeared after an interval of 51 to 52 weeks , only one of the i.e. , 9 weeks after the pair surviving longest had been sacrificed . intact partners treated with a.a.f. 
developed tumours of the breast ( rat 6 , group ii )  . in the 35th week of the experiment a mass was felt in the region of it was surgically removed , and was found to be the fifth left mammary gland . a well - encapsulated tumour measuring 20 x 12 x 9 mon cutting , milky histologically it was a fibroadenoma , in which fluid escaped under pressure . the epithelial elements were much more numerous than is common in such tumours except when occurring in pregnant or lactating females . 
the other was a small adenocareinoma of the breast which showed far less secretory activity than the fibroadenoma which had developed simultaneously . benign cystic cholangiomata were present in practically all rats treated with a.a.f. , but in the intact partners they were generally larger and more widespread than in the " single " animals , in which they were limited to a few cysts in lobus caudatus and left lobe . 
we are unable to state why such changes occurred only in isolated instances . another feature in which the spayed parabiont differed from a " single ovariectomized female was the cytology of the suprarenals . 
24 is included for comin animals killed after 15 to 25 weeks of parabiosis . it shows the distribution of lipoids in the cortex of the suprarenal of a parison rat spayed 6 months previously . 
a second experimental method ofobtaining such neoplasms was discovered by biskind and biskind ( 1944 ) , who obtained such tumours by transplanting ovaries into the spleen of gonadectomized rats . 
the gonads of the intact partners were composed of cystic follicles - proof of increased secretion of fouiclestimulating hormone ( f.s.h. ) by the pituitary of the irradiated parabiont . the liver of rodents inactivates ovarian steroids so efficiently that the secretions of a gonad grafted into the spleen do not enter the general circulation . in consequence the pituitaries of animals bearing such grafts are of the castrate type , and have an elevated gonadotropin content , as shown by greep and jones ( 1950 )  . fels ( 1949 ) discovered that a temporary hgature of the blood vessels supplying the ovaries led to an endocrine imbalance characterized by hyperoestrinism in the presence of castration changes in the pituitary . it seems therefore that one factor is common to at least 3 of the 4 methods quoted above ; they induce an endocrine imbalance characterized by pituitaries secreting elevated amounts of gonadotropins . it is therefore not astonishing that the neoplastic changes induced under these experimental conditions are all of the same kind . nearly all growths so obtained belong to the group of granulosa - theca - lutein cell tumours . 
moon , simpson , li and evans ( 1950 ) also regard the neoplastic changes observed in the ovaries of rats treated with growth hormone to be due to a pituitary imbalance . these authors mention a reduction of the acidophils and an increase of the chromophobes in the pituitaries of such rats , and noted that in 2 animals the histological picture of the anterior pituitary was of the castration type . it seems therefore that the basophils and especiary the f.s.h. secreting cells can increase in animals treated with growth hormone . however , more information is required before one can assume that ovarian .eoplasms obtained by treatment with growth hormone are due to the same mechanism as the other experimental tumours of the ovary , i.e. , to an excess of gonadotropins . in our case there can be no doubt that tumour development in the female gonad was the result of increased stimulation by gonadotropins and of the carcinogenic action of a.a.f. it is especially the foricle - stimulating hormone secreted in elevated amounts by the gonadectomized partner which determines the endoadmittedly during the first weeks of parabiosis there is good crine situation . evidence for the action of luteinizin hormone , as indicated b the presence of many healthy corpora lutea in the ovary of the intact litter - mate . later , when the increased secretion of oestrogens from the stimulated ovary has suppressed all the gonadotrophic activity of the intact partner 's pituitary and continuous oestrus has become established , the pituitary hormone dominating the picture is f.s.h. it is therefore not astonishing that granulosa cell tumours are so frequent in our material and that luteinization occurred to only a hmited extent . 
4 , 6 and 7 of their paper resemble closely the early lesions observed by us , and which we have seen to progress to tumours of considerable size . it seems unfortunate that drips and ford ( 1932 ) compared the atypical structures observed - by them in the irradiated ovaries of rats with carcinomatous ovarian cystadenomata of the 342 f . 
and luteinizing hormone ( l.h. ) in the ovarian cycle is greatly disturbed in the parabiotic female joined to a gonadectomized litter - mate . after 3 to 4 months of parabiosis the ripe follicle is not any more transformed into a corpus luteum nor does it involute , but is exposed to continued stimulation , which does not cease after the death of the ovuthis is in our opinion the decisive factor which leads to the development of the granulosa cell tumours . contrary to what is seen in spleen graftecl or irradiated ovaries of mice , in the rat there is not the shghtest evidence that these tumours " arise from proliferation and ingrowth of germinal epithehum " , as assumed by li and gardner ( 1947 )  . we have observed in some glands smar tufts of cells growing out from the surface ' germina of the ovary , but we have never seen tubular ingrowths from origin from embryonic nests seems a most unlikely hypothesis , epithehum "  . since many workers obtained ovarian tumours in 50 to 70 per cent of their experimental animals ( kaplan , 1950 ; furth and sobel , 1948 )  . . 
undoubtedly the stroma cell of the ovary can differentiate into theca or granulosa cells , and therefore one cannot still , we prefer origin from differentiated granulosa exclude this possibility . cers because of the morphology of the early lesions observed by us . 
12 and 13 one has not to fall back on the conception of disturbed embryogenesis . in preovulatory follicles invaginations of the theca accompanying tufts of capifaries are a common feature . the chorion epithelioma - like tumour presented some diagnostic difficulties . we consider it to be an anaplastic carcinoma . 
as pointed out by willis ( 1947 ) , anaplastic carcinoma can simulate chorion epithehoma and therefore more than morphological similarity is required to establish the diagnosis , in the absence of pregnancy . 
the lack of teratomatous elements and the lack of signs of functional activity such as corpus luteum cysts in the unaffected right ovary are in favour of the diagnosis of anaplastic carcinoma . 
was given simultaneously with or previously to the treatment with goitrogen . spontaneous ovarian tumours and especially granulosa cell tumours are exceedingly rare in rats ( iglesias , stemberg and segaloff , 1950 ) , and therefore do not complicate the interpretation of the experiments reported in this paper . finary an explanation has to be given why the incidence of granulosa cell tumours in group i is lower than in groups ii and iii . 
and most probably also our surgicaltechnique . group i represents our first parabiotic pairs , in which we did not succeed as well as later on to obtain wide junctions , measuring 6 to 10 cat the time the animals were sacrificed . the study of a number of organs of the intact partner showed clearly the effects of oestrogens secreted in excessive amounts by the stimulated ovaries . one of the sequels of this hyperoestrinism were the pituitary adenomata which occurred whether or not a.a.f. 
we beheve , however , that originary these benign neoplasms were acidophilic , just as in zondek 's case ( 1940 )  . this author observed an adenomatous lesion composed of acidophils in the pituitary of a woman treated with very high doses of oestradiol . whereas the increased secretion of oestrogens by the stimulated ovaries led to neoplastic changes in the pituitary , no mammary tumours were observed in the control pairs , contrary to the findings of zeckwer ( 1944 ) , and only one of the intact parabionts treated with a.a.f. 
developed tumours of the breast gland . the material at our disposal does not arow the conclusion that the high level of oestrogen in the circulation of the intact partner inhibited the carcinogenic action of a.a.f. 
in intact female rats joined in parabiosis to gonadectomized litter - mates . ovarian tumours developed in about 50 per cent of these animals . ( 2 ) a description of the histology of the ovarian neoplasms has been given and their histogenesis discussed . it has been found that most of them were of the granulosa cell type . 
secreted in excess by the pituitary of the gonadectomized litter - mate is regarded to be the factor essential for their development . ( 3 ) the pituitary tumouis observed in intact parabiotic females are considered to be due to the excess of oestrogens secreted by their stimulated ovaries . 
the gonadectomized partners were always found to be free of neoplastic lesions , whether or not their litter - mates received a.a.f. ( 5 ) the state of hyperoestrinism present in the intact parabiont did not enhance the carcinogenic action of a.a.f. 
were administered to " single " female rats two mammary cancers appeared during the first 40 weeks of the experiment , a period which corresponds to the maximum survival of our parabiotic pairs . ( 6 ) benign cystic cholangiomata were found in nearly all rats treated with in the intact parabionts they were more numerous and larger than in a.a.f. the " single " rats . we wish to thank professor r . 
hamer. from the cancer research laboratories , department of pathology , the medical school , birmingham 15 . received for publication january 13 , 1953 . results for the analysis of thymus histone presented from this laboratory ( hamer , 1950 , 1951 ) have been followed by similar results from other sources ( daly , mirsky and ris , 1951 ; eadie and leaf , 1952 )  . these results all show the same general characteristics in composition but the actual values obtained vary appreciably from worker to worker , suggesting that either the methods of isolation or the source of the material may be affecting the final product . analysis of other nucleo - proteins have been reported by brunish , fairley and luck ( 1951 ) , liver histone , and by khouvine and baron ( 1951 ) , rat epithelioma histone . the last - mentioned paper evidence was presented that different treatments during isolation could yield products of varying composition . 
stedman and stedman ( 1951 ) have also reported qualitative and partial quantitative analyses of a number of basic proteins from isolated nuclei . in the work reported here further analyses of thymus histone are presented along with other results for the non - histone or acid - insoluble protein of the nucleus . all the fractions examined were derived from the same batch of thymus nuclei , and consequently it was possible to study whether the methods of fractionation used caused changes in the amino - acid compositions . 
of defatted calf thymus by the following method : the tissue was homogenised in a blendor , suspended in a total of 2 litres of saline citric acid solution ( 0.14 m nacl , 0 * 025 m citric acid ) , and then centrifuged , discarding the supernatant . 
the sedimented material was washed by alternate suspension and centrifugation in another saline citric acid solution ( 0.14 m nacl , 0 * 01 m citric acid ) , six times in all , the preparation of isolated nuclei was then free of whole cells and had no appreciable cytoplasmic the nitrogen to phosphorus ratio of such a preparation was contamination . 4 - 5 : 1 . 
next a tenth of the volume of a 5 per cent solution of sodium dodecyl sulphate ( sulphonated lauryl alcohol - glover ) in 45 per cent alcohol was added and the ph brought to 5 - 5 . 
the residue from the acid extraction was washed two further times with 0 - 2 m hydrochloric acid , and the remaining insoluble fibrous material was suspended in water , dialysed for 48 hours and freeze - dried ( fraction nr )  . the remaining half of the solution of nuclei in 1 - 2 m saline was shaken with an equal volume of chloroform - butyl alcohol ( 4 : 1 ) to dissociate the nucleic acid and the protethe nucleic acid remains in the aqueous phase ( from which it may be precipitated with alcohol ) , while the protein forms a gel at the interface . this treatment was repeated twice , combining the gel layers obtained . 
the gel was washed three times with the buffered 1 - 2 m saline , agitating and centrifuging each time , and then the protein was thrown down by adding chilled alcohol . 
the precipitate was extracted overnight with 01 m hydrochloric acid , and the acid extract containing histone was worked up as above to give fraction sh , the second histone specimen . 
the residue was washed further with acid and then suspended in water , dialysed and freeze - dried ( fraction sr )  . these four main fractions and the " whole protein " ( dp ) were then analysed . there was insufficient material in fraction r to permit a full analysis , but it is hoped to study this further at a later stage . 
extract with hci whole protein complex ( dp ) nucleic acid histone ( nh ) residue ( nr ) insoluble residue ( r ) shake with chc13 - buoh protein nucleic acid fig . 
the specimens had slightly lower nitrogen contents than those previously examined and contained about 02 per cent phosphorus . the specimen sr of non - histone or acid - insoluble protein was slightly yellowish , and contained a little less nitrogen and more phosphorus than the histones . was insoluble in water , but would dissolve at ph 9 - 10 to give a pale yellow solution 154 d . 
hamer and then precipitated out when this solution was acidified to about ph 5 - 5 . the course of this treatment some unit in the protein is apparently destroyed as evidenced by the production of a strong unpleasant odour on acidification . 
the related specimen nr contains , of course , much nucleic acid in addition to proestimated from the phosphorus content and the absorption spectrum tein . there is approximately 56 per cent nucleic acid in this fraction . in dilute alkalis an opalescent viscous solution is obtained . finally , specimen dp precipitated from the solution of isolated nuclei by sodium dodecyl sulphate has a nitrogen content of about 9 - 8 per cent indicating that the ratio of protein to detergent is around 3 : 2 by weight . 
the act of separating the non - histone protein from the nucleic acid apparently damages the protein , and it does not seem possible to obtain it in other than an insoluble and denatured forthis would suggest that the non - histone protein may be chemioally bound to the nucleic acid while the histone is held by a predominantly ionic union . 
some support for such a structure has recently been presented by fleming and jordan ( 1952 ) , who have found that the results of eleotrophoretic studies on thymus nucleoprotein in solutions of varying ionic strength could be explained by the existence of an equilibrium np np + p ' ( where np is the original nucleoprotein , np a nucleoprotein fraction with a higher nucleic acid content , and p ' a dissociated protein )  . 
however another possibility is that in the cell the histone is loosely combined with the non - histone protein and that acid treatment breaks the compound open . this would be in accord with the close similarity of amino - acid composition , but would require that all the cystine and tryptophane remain with one fraction on fission . 
the first possibility considered seems on the whole to be more probable , as it is more in keeping with the variation in the amounts of histone and non - histone protein in the nucleus of different cell types ( hamer , 1951 ; stedman and stedman , 1951 ; mirsky and ris , 1951 )  . in the case of the thymus nuclei studied here the histone and non - histone proteins occurred in roughly 156 d . 
kreyberg. from the institutt for generell og eksperimentell patologi , universitetet i oslo . received for publication february 19 , 1952 . in many countries the statistical reports show a steady and remarkable increase in the number of deaths from " lung cancer . " the problem puzzles the cancer specialists and troubles the public and the medical profession . does this increase signify a real augmentation of cases of lung cancer , or does it simply mean an increasingly better diagnostic service ? this question will not be discussed in this paper . if we wish , however , to study , by statistical methods , the possible role of certain irritants in the genesis of lung cancer we have to make clear what we mean by the term " lung cancer . " according to kennaway and kennaway ( 1947 ) their statistics from england and wales comprise : " cancer , carcinoma , or sarcoma of lung , bronchus , pleura , root of lung , hilum of lung , lung and mediastinum , or jung and pleura . 
the norwegian " statistisk sentralbyra " has , since the first of january , 1951 , acted accordingly . it is a great step forward . in order to study a possible relationship between lung carcinoma and smoking habits , or industrial irritants , it may be of importance , not only to exclude all other lung tumours than primary lung carcinomas , but even to subdivide the latter into special sub - groups . from our general experience in the field of cancer research we are ever more impressed by the importance of the study of the geographical distribution of the different manifestations of malignant disease . this different geographical distribution examined on the background of the corresponding difference as to races , primary epithelial . 
this report deals with 100 consecutive cases ofprimary epithelial lung tumourb , received for diagnosis at the institute of pathology , at the university all , but also only those , tumours are included , where the piece of tissue of oslo . o 60 1929 1939 fig . 
1. - mortality statistics from norway , 1929 to 1949 ( " statistisk sentralbyroa " )  . was large enough to permit a definite histological classification . the main part of the material ( 97 cases ) was received from the surgical department a , at the university hospital , 2 cases came from the ear , nose and throat department , and 1 case from the roentgen - radium department . hereto are added 5 cases of secondary lung tumours , received within the same period , and clinically regarded as primary tumours , the histological examination , however , revealing their true character ( 2 cases of metastasizing thyroid adenoma , and 1 case each of hypernephroma , adenocarcinoma of uterus and malignant naevus tumour )  . the 100 tumours of the main series were classified according to traditional terminology as follows : 114 l . 
10 the number and the different types of tumours of our main series may be seen , as well as the occurrence in age - groups and the distribution between the two sexes . 
the individual tumours of groups g and f are tabulated in table ii . the groups e , f and g do not show any marked preponderance in the one further , these tumours are rather evenly distributed in the sex or the other . different age - groups , and they occur even in very young people , our youngest patient being a girl of 19 with a malignant adenoma . 
as to the microscopical classfication , he has : adenocarcinomas 4 - 6 per cent , squamous cell carcinoma 62 - 9 per cent , undifferentiated carcinoma 25 1 per cent and uncertain type 7 - 4 per cent . here again the similarity is greater when we examine the material on the basis of the more objective characteristic the distribution in age - groups than on the basis of the more subjectively influenced classification in histological types . it is evident that the surgical material cannot , without a closer examination , be taken as representative for the occurrence and the distribution of lung carcinomas and lung tumours in the population . firstly , cases occurring in old age 118 l . 
kreyberg will not be represented , as these patients are poor operative risks and seldom secondly , in old age the diagnosis may be more difficult and operated upon . possibly not pursued with the same enthusiasm as when the patient is a younger . it is not unlikely that the local thirdly , the sex distribution may be different . doctor , the surgeon and the patient himself will take a greater risk and show a somewhat more heroic attitude towards the question of operation when the patient is a male . 
the women in these age - groups may possibly show more resigfourthly , surgical material may show a greater nation to the blows of fate . number of benign and moderately malignant tumour types than the sum total . this is significant when the material examined includes all primary epithelial lung tumours , but less important when only true bronchogenic carcinomas are this underlines the importance of a careful classification when statisconcerned . tics are to be compared . 30 ~2021 - 30 31 - 40 41 - 50 51 - 60 61 - 70 71 - 80 81 - 90 age groups fig . 
the occurrence of a certain number of cases in the early age - groups indicates that a few adenomas are included also in this post - mortem series . i wish to emphasize that the present paper represents a preliminary orientation only , as to the occurrence of lung carcinomas in norway . 
mottram ( 1945 ) published the results of experiments designed to demonstrate a relationship between the tumour yield induced by benzpyrene and the number of epidermai mitoses present at the time of application of the carcinogen . painting the skin of rnice at midnight resulted in a higher yield ofpapillomata than did painting at midday . 
but not water , and 1 - 4 hours later they were given a single appheation of carcmogen , benzpyrene ( hoffinan - la roche ) in experiment i and methyleholanthrene ( eastman kodak & co in experiment 2 . in the 1 - - ) enzpyrene experiment each animal received 0 - 1 ml . 
of a 0 - 3 per cent solution in acetone apphed to the interseapular region of the skin , and ' m the methyleholanthrene experiments the dose wasalso 0i ml . 
the mice were starved for a total period of 64 hours , after which they three days after the application of the carcinogen painting were fed ad libitum . with croton oil ( 0 - aper cent in acetone ) was commenced , and this was repeated twice weekl for 20 weeks . 
these mice were treated in the same way as those in the group b , except that the period of starvation was omitted altogether . in experiment 3 , group a contained 25 male mice which were deprived of all food 36 hours before each was painted with 0 - 05 ml . 
most of the papillomata being discovered between the 1 : 21th this is in good agreement with the results obtained bv berenand 15th weeks . blum and shubik ( 1947 )  . 
ludford. from the laboratories of the imperial cancer research fund , london . received for publication january 30 , 1948 . in a review devoted to the discussion of colchicine as a possible chemotherapeutic agent for cancer ( ludford , 1945 ) , attention was directed to the dual action of this drug on tumours . it is the most potent of mitotic poisons , and as . 
at the time the experiment to be described was performed , sections exhibited large compact groups of carcinoma cells , surrounded by an abundant and highly cellular stroma , composed of enlarged and hyperchromatinic spindle - shaped and polymorphic cells , presenting the typical cytological appearance of sarcoma cells . 
an aqueous solution was employed in a concentration of 1 part in 10 , 000 of distilled water . this had been prepared six days previously , when it was maintained at the temperature of boiling water for ten minutes to reduce the possibility of infection , and was stored in the dark for use throughout the exp6risince the activity of colchicine is reduced by high temperatures and by ment . keeping , especially when exposed to light , the solution employed for this experiment was rather less potent than a freshly prepared solution . 
1 by comparing the size of the tumours of the controls and the treated mice on the 21st day . control 71141 211301 37 treated 7 14 3 43 10 01 234 fig . 
2. - regression of a sarcoma ( c ) in strong a strain mice after treatment with colchicine . such after the shortest possible interval consistent with survival of the mice . treatment is invariably accompanied by a high mortality . an experiment with a spindle - celled sarcoma in strong a mice demonstrates the possibility of completely inhibiting malignant growth . this sarcoma was one which originated by the sarcomatous transformation of the stroma of a mice into which it is transplanted do not usually survive mammary carcinoma . long , as it rapidly penetrates the skin and leads to considerable superficial ulceraof six young adults transplanted with this sarcoma three were treated tion . 11 and 20 days after transplantation . 
age. - since actively growing tissues are most sensitive to mitotic poisoning , it is to be expected that young animals would be more susceptible than older ones ries ( 1939 ) reported that a 42 - days - old mouse to the toxic action of the drug . will survive more than 17 times the dose of colchicine which is lethal to one 10 days old . the maximum inhibition of malignant growth occurs with the highest tolerated therefore , to obtain the greatest arrest of tumour growth it is doses of the drug . necessary to employ animals at the age when they are most resistant to the the best results general toxic action and the largest doses can be administered . old mice are less able to tolerate have been obtained with young adult mice . thus , 11 strong a mice varying in age from 18 months to 2 years the drug . and 12 young adults were each injected with 0 , 056 mg . 
3. - action of colchicine upon sarcoma 37 grown in strong a and c 57 strain mice . tumours in c 57 mice indicated by outline , tumours in a mice stippled . 
the size of the tumours in the c 57 mice is indicated it will be observed that in outline , and in the a mice by the stippled areas . actually there is little difference in the size of the tumours in the control animals . growth is slightly more rapid in the a mice , but there is a definite difference in the two strains of treated mice . 
a similar acquirement of tolerance by tumours to the haemorrhage - inducing action of bacterial polysaccharides has been reported by shear ( 1944 )  . application of the preceding results for obtaining the maximum " colchicinic effect . " discrepancies in the reports on the action of colchicine on neoplasms which have been published are explicable on the basis of the preceding findings . 
of colchicine over a period of 4hours . two other tumours regressed completely , but the - , remaining two continued to grow progressively . both received the same treatment on the 37th day . one died with a large tumour on the 45th day . 
the five mice which had been completely " cured " were kept under observation for a year and were then killed . post - mortem examination revealed no trace of carcinomas . the charting of all the tumours in these experiments was carried out independently by a . 
chapman , the senior technician in charge of this work . discusston9 with all the tumours which underwent regression in the preceding experiments there was extensive haemorrhage following treatment . this ' was most readily induced in the a strain mice . 
a few hours after the injection of the maximum sub - lethal doses of the drug the tumours appeared blue through the skin . subsequently superficial ulceration was of common occurrence . since boyland and boyland ( 1937 ) first drew attention to the similarity of action of colchicine and bacterial filtrates they have been shown to behave alike in most other respects . 
with both , complete regression of some transplantable and spontaneous tumours has been effected . ' the results acquire significance in that they indicate the limitation of haemorrhage - inducing agents in the treatment of malignant growths . that some form of damage to the capillary system of tumours might be ' the best way to inhibit malignant growth was suggested by woglom ( 1922 )  . 
a critical review of the evidence concerning tumour regression led him to raise the question whether " the receding tumor may not differ from the growing one only in the extent to which its blood vessels have been obliterated by thrombosis . " he pointed out that the blood vessels of many tumours are more subject to thrombosis than those of normal tissues , and he conceived the possibility of both chemical and mechanical factors being responsible . 
the former resulted from the abnormal metabolism of malignant cells , and the latter was described as " the mechanical pressure which the rapidly increasing parenchyma must often exert upon its vessels , with all the possibilities of injury to their walls which this would entail . " more recently algire ( 1945 ) has devised an adaptation of the transparent chamber technique which enables microscopic observations to be made of the development of the blood vessels of tumour transplants . 
he reports that although many vessels in growing tumours become very large , " differentiation in mammary cancers he observed into arterioles and venules was not evident . " the development of " blood - filled cul - de - sacs . " " these appeared to result from r . 
the usefulness of ultraviolet absorption in studying solutions of methylcholanthrene in different solvents and the physico - qhemical significance of spectroscopic data suggested an approach to the standardization problem . it has become necessary for us to discontinue work on the suspensions , and there is no likelihood of our returning to the matter . 
at the end of the exposure time the paste , which had been kept moist through the 42 - day period , was extracted for 24 hours with 35 ml . 
3. - ultraviolet absorption curves from a " protected " suspension of mnethylcholanthrene after 80 days ' exposure to diffuse davlight . curves a , b , c as in fig . 
4. - ultraviolet absorption curves from an " unprotected " suspension of methylcholanthrene after 80 days ' exposure to diffuse daylight . curves a , b , c as in fig . 
4 , a , the contribution of scatter predominates . it is evident that these solutions differ markedly in the type of suspended material , and this might well result in substantial differences in biological behaviour . in order to arrive at a representative selective absorption curve the scatter component must be subtracted from the observed data . 
5. - ultraviolet absorption curves of a saline extract of ground , moist methylcholanthrene crystals which had been exposed to diffuse daylight 42 days before the extract was prepared . curves a , b , c as in fig . 
the procedure for making these approximations is as follows : from an inspection of the curve plotted from the spectrophotometer data the contribution of scatter and turbidity is estimated and a smooth curve characteristic of scatter and turbidity is drawn to approximate this contribution . 
the ratio of the difference obtained as above and the density value at the same wave - length of a known concentration of the solute dissolved in a solvent in which scatter is absent is determined . 
the ratio so found is used as a multiplying factor which is applied to the density values of the reference curve ( known solute in true solution ) at several wave - lengths . this product is subtracted from the density values at corresponding wave - lengths of the mixed scatter - absorption curve to give a series of density values which are plotted - , and ' a smooth curve is fitted to the points so determined . 
the procedure as outlined gives a family of curves , with each member progressing towards a more accurate estimation and being uniquely related to the known absorption curve of the solute , and a mixed curve which is assumed to be composed of true absorption of the solute and a scatter - turbidity component . such a series of approximations can be made when one knows from other sources the true absorption spectrum of the solute , and can use this information as a standard of reference . the above procedure has been used to determine the scatter curve presented in the figures of this paper . 
5 shows the absorption of th3 extract from the ground methylcholanthrene there is a large scatter contribution , otherwise the curve bears little crystals . resemblance to the curves from the suspensions . 
bielschowsky. from the , hugh adam cancer research department of the medical school and the new zealand branch of the british empire cancer campaign , university of otago , dunedin . received for publication april 7 , 1953 . judging from the literature , adenomata occur more frequently in the pituitaries than in the thyroids of aged rats . 
at the routine autopsies of 154 albinos of the wistar strain , 41 of which were males , 86 intact and 27 spayed females , 24 cases of adenoma of the pituitary were discovered . seven of these occurred in the males , 16 in the intact females and only one in an ovariectomised animal . the average age of these rats was 2 years . 
adenomata of the thyroid were found in 5 animals , 4 times in combination with neoplastic lesions of the pituitary . post - mortem examinations performed on old rats of a more recently acquired hooded strain have furnished three additional cases of tumours of thyroid and pituitary . 
the diet consisted of a dry mixture of bran 30 per cent , pollard 35 per cent , meat meal 15 per cent , maize meal 15 per cent and bone flour 5 per cent , supplemented by wheat and kibbled maize , and once weekly by green vegetables and cod liver oil . drinking water was supplied in liberal amounts . 
the weight of the animals was recorded at fortnightly intervals and they wer6 sacrificed when loss of weight and general appearance indicated ill - health . at autopsy the pituitaries were immediately transferred into a pre - weighed bottle containing about 2 ml . 
when treated with gomori 's fuchsin aldehyde reagent , the cytoplasm of the angular cells and especially their granules stained purplish - violet . in other words , these cells strongly resembled and gave the staining reactions of those basophils which purves and griesbach ( 1951a ) named " thyrotrophs . " therefore the tumour is considered to be a basophil adenoma formed by thyrotrophs . in the part of the anterior lobe outside the basophil adenoma the basophils were considerably increased in numbers . angular types again predominated , but here vacuolated forms , extremely rare within the tumour , were numerous . these cells were identical with those seen after partial thyroidectomy . they gave a positive pas reaction of varying intensity , and with the gomori stain some were found to contain coarse violet - purple granules . the large round gomori 206 f . 
5 , the larger of the two protrudes above the anterior surface and is closely connected with the pars internmedia : the other , just appearing in the section , bridges the pituitary cleft and is situated laterally . 
the pituitary was of irregular shape with a small this was a well defined basophil adenoma , the haemorrhagic brownish area . tumour cells giving the same staining reactions as described above . 
the neoplastic changes found in the hypophysis and thyroid of the younger animal were of microscopic size . in the slightly abnormally shaped anterior lobe numerous thyroidectomy cells and also multiple nodules formed by atypical basophils were present , the pars intermedia being normal . 
normal anterior lobe tissue was recognisable in the periphery as a narrow rim surrounding approximately half of the circumference of the tumour . radiating from this rim compressed strands of predominantly acidophilic and chromophobic elements were seen between areas of tumour , an indication that the neoplasm had arisen from different foci . intermediate and posterior lobes appeared normal . 
the cells composing the tumour were large , showed great variation in size and shape , had sharply defined cell borders and vesicular nuclei with one or more large fuchsinophilic nucleoll . multi - nucleated and tumour giant cells were rather numerous and so were mitoses . 
when stained by the pas technique or with gomori 's aldehyde fuchsin after long search an occasional only in this respect , cell was found having pas or gomori positive granules . did the adenoma differ from those described above . in papanicolaou preparations the cytoplasm stained faintly with light green . the histology of the thyroid was that of an inactive gland . 
many mitoses were found in this nodule , considered to be a benign pheochromocytoma . rat 8 , a 26 months old male , was killed because of the presence of an abscess otherwise the animal was in an excellent in the subcutaneous tissue of the neck . state of health and weighed 460 g . 
the first question to be answered is : which cells produce the thyrotrophic hormone and the second , how many types of basophils occur in the anterior lobe of the hypophysis . 
as to the second , romeis ( 1940 ) described two types of basophils both stainable with aniline blue but distinguishable by their affinity to creso - fuschin or resorcinol - fuschthe type stained by these fuchsin dyes is the beta cell , the other is the delta cell of romeis . 
as shown by halmi ( 1950 ) another elastica stain , gomori 's fuchsin aldehyde reagent , also differentiates between two types of basophils , whereas most other techniques like pearse ( 1952a ) does not papanicolaou 's or gram 's method stain all basophils . seem to attach great significance to these different tinctorial qualities and adheres to a unitarian view . 
now the pathogenesis of the basophil tumours can be discussed . chronic iodine deficiency lowers the thyroxine level in time , to which the pituitary responds with an increase in thyrotrophic cells . this compensatory hyperplasia progresses towards the formation of tumours , in this connection it might be which in some instances reach considerable size . mentioned that proliferating normal thyrotrophs , as observed by guyer and claus ( 1937 ) , tend to aggregate in clusters , a mode of growth which might be favourable to nodular hyperplasia , the first stage in adenoma formation . 
the adenoma of this animal was functionally inactive as judged by the appearance of the thyroid which was that of a resting gland . also cells giving a positive reaction for glycoprotein were virtually absent in this tumour . the most convincing evidence for funttional activity is provided by rat 4 . the large pituitary tumour of this animal contained numerous pas and gomori positive elements and its thyroid showed the most pronounced signs of stimulation . in addition , in the pituitary of this animal , so little normal anterior lobe tissue was left that it seems most unlikely that this small rest could have secreted amounts of thyrotrophin large enough to induce a four - five fold enlargement of the thyroid . finally the pituitary lesion of rat 8 has to be considered . in this case the morphological evidence was more in favour of hyperplasia than of neoplasia . here an agglomeration of thyrotrophs had persisted in one area despite the fact that ki had been supplied for 7 months . in the rest of the anterior lobe these cells were found in normal numbers , as was to be expected , and the thyroid had undergone involution . rich glycoprotein content of the cells forming this aggregation was probably due to storage and not a sign of secretory activity . the anomalous behaviour of these cells suggests that they were no longer normal thyrotrophs . the thyroid tumours observed are , in the writer 's opinion , due to stimulation by elevated amounts of thyrotrophic hormone . the stimulus for the increased secretion by the pituitary was a deficiency of thyroxine due to impaired synthesis by an inadequate content of iodine in the diet . in six instances the thyroid tumours were found in activated and twice in resting glands . the latter occurred in animals which had received a supplement of ki for several months and are considered to be evidence of past stimulation . these neoplasms differed morphologically from those observed in stimulated thyroids in the same way as the thyroid adenomata found during administration of thiouracil differ from those seen after the treatment with the goitrogen has ceased . 
their epithelium was rather low , and cystic follicles filled with colloid were a prominent feature . to summarise the pathogenesis and structure of the thyroid adenomata observed is similar to that of the tumours induced by goitrogens which act by blocking the synthesis of thyroxine . the conception that thyroxine deficiency is the ultimate cause of the syndrome described is strengthened by the following observations . fischer ( 1926 ) , writing from bern , switzerland recorded two cases of pituitary tumours found in aged female rats . 
the thyroids of both animals contained multiple tubular adenomata , and in one an adenocarcinoma was also present in this gland . the rats belonged to wegelin 's colony in which goitre was endemic fischer 's paper was published long before the gonadotrophic and thyrotrophic hormones had been discovered . she stressed , however the similarity of the pituitary tumour cells with the ele212 f . 
bielschowsky ments which appear in the rat 's hypophyis after castration or thyroidectomy ; and considered the neoplasms to be carcinomata formed by " castration " cells fischer believed that although the ovaries of one of her animals were normal . the neoplasms originated from the pars intermedia or tuberalis . " spontaneous " tumour formation occurring simultaneously in thyroid and pituitary of rodents seems to have been observed only by fischer and by the writer , but one sees this syndrome under experimental conditions most frequently in animals t ' reated with so purves and griesbach ( 1951a ) mention goitrogens for prolonged periods . a basophil adenoma of a rat treated with methythiouracil for two years . basophil adenomata occur also in thyroidectomised rats treated with acetylaminofluorene into the same class belong also the pituitary tumours ( unpublished results )  . discovered by gorbman ( 1950 )  . 
they appear in mice exposed to high doses of radioactive iodine , but can be prevented by the administration of thyroxine ( goldberg and chaikoff , 1951 ; gorbman , 1952 )  . furth , gadsden and upton ( 1952 ) reported that transplants of such tumours contain large amounts of thyrotrophic hormone . 
of tissue was homogenised in a total volume of 50 ml . , more sucrose being added later to dilute the homogenate to this , as was shown by direct comparison , a final concentration of 10 per cent . had no effect on subsequent fractionation . it was found in preliminary experiments that maximal liberation of cytoplasmic proteins into the supernatant fluid was achieved by homogenisation lasting for 1 to 2 minutes . the separation of the cell components was carried out by means of differential centrifugation at a temperature of 20 to 40 c . 
in a " spinco " ( specialised instruments corporation , belmont , california ) model e ultracentrifuge , except for the preliminary removal of nuclei , unbroken cells , debris , etc . , which was carried out in an ordinary low - speed centrifuge . 
the centrifugal procedure with some modifications was based on those , originally described by claude ( 1943 , 1946 ) and developed by hogeboom , claude , and hotchkiss ( 1946 ) , hogeboom , schneider , and pallade ( 1948 ) , schneider ( 1946b )  . in some of the later experiments it was based on that of schneider and hogeboom ( 1950a )  . 
stickland oxidase activity of each fraction was determined by the method described by umbreit , burris and stauffer ( 1945 ) and the results expressed as q02 ( n )  . 
a concentration of the enzyme in this fraction was also found in normal lactating breast tissue of highand low - cancer - strain mice . while the microsomal fractions of rat and mouse liver showed only a small amount of the enzyme , the same fractions of breast tissue revealed an appreciable quantity of it . in order to establish that this activity was a true property of these fractions , on some occasions the activity was determined after washing and was found to be unaltered . these results expressed as specific activity of the enzyme in the respective fractions are shown in table iii . 
hogeboom and schneider ( 1950 ) observed partial inactivation of succinoxidase after sonic disintegration of mitochondria . the possibility of contamination with mitochondria could not be excluded by histological examination alone . mitochondria were invariably observed in smears of microsome fractions , but in considerably smaller numbers than in the mitochondrial fractions : it is , however , impossible to make such comparisons quantitative . 
the chief arguments against contamination with whole mitochondria are first , that in rat liver no succinoxidase was found in the microsomes ( or negligible quantity ) , and second , that in a number of experiments with mammary tumour tissues the same mitochondria were sedimented in two parallel ways , at 5000 times gravity and at 8000 times gravity , and in the latter case the activity of the microsomes subsequently obtained was only slightly lower than in the former . the possibility of contamination of microsome fractions by fragments of broken mitochondria cannot easily be disposed of . clearly such contamination was not observed in liver microsome fractions , obtained in similar manner as those from normal and malignant mammary tissues . 
the results showed clearly that mitochondria from normal and malignant mammary cells of mice are not more fragile than those from liver , and if anything rather less . it can therefore be deduced that mammary cell mitochondria are not appreciably fragmented during homogenisation , and that consequently the enzymic activity present in the microsome fractions from these cells is likely to be a true property of microsomes present in these fractions . 
the ready fragmentability of liver - cell mitochondria in the potter - elvehjen homogeniser after they have been separated from other cell components is at a first glance not easily reconciled with the fact that no damage appears to occur to these cellular components during the homogenisation of the tissue . this difference is presumably due to the protection of the mitochondria against friction and damage by the presence in the latter case of larger cell fragments . the enzyme activity of microsomal fractions of normal and malignant breast tissues remained practically unaltered in spite of washings in isotonic sucrose 258 l . 
stickland solution , which again points against the possibility of the enzyme being adsorbed on microsomes . from the experiments of price , miller and miller ( 1948 ) , price , miller , miller and weber ( 1949a , 1949b ) on rat hepatoma and of schneider and hogeboom ( 1950b ) on mouse hepatoma , it is now known that in both rat and mouse hepatoma , the protein content of the mitochondrial and microsomal fractions is much lower than that in similar fractions of normal rat and mouse liver . further , it has been shown in these studies that in rat and mouse hepatoma the succinoxidase content of the mitochondrial fraction is lower than that in normal rat and mouse liver , the total activity being 5 times lower and the specific activity 2 times lower , in spite of the same distribution of the enzyme in normal and malignant livers . in the present experiments no significant difference was observed between normal and malignant mammary cells , either in the total amount of succinoxidase or in its distribution between the various fractions of these cells . 
a curious point , so far unexplained , is that although in liver homogenates 100 per cent recovery of succinoxidase could be obtained in the fractions , in mammary tissues the recovery was much lower , amounting on the average to only 70 per cent . no difference was found between highand low - cancer - strain mice either in the protein and succinoxidase content or in the distribution of these in the various fractions , but the mammary tumour tissue in each case showed a reduced content of mitochondria , compared with the normal mammary tissue , which agrees with that found by schneider and hogeboom ( 1950b ) in mouse hepatomas . the reliability of the simplified centrifugal procedure used in the majority of the experiments has been tested by the use on three occasions of the more complicated procedure of schneider and hogeboom ( 1950a ) , which gave substanit may perhaps be of interest to mention that stern tially the same results . ( 1939 ) demonstrated the association of succinoxidase with particles of microsome size in beef heart muscle . a small point worthy of mention is that for greater convenience of making the enzyme assays , the samples of washed particles from rat and mouse liver and mammary tissues were kept overnight at - 79 c . 
korteweg. victorieplein 45 , awkrdam , netherlawi8 received for publication december 8 , 1953 . round about the end of the last war the total number of deaths from cancer recorded in the mortality statistics of the central bureau of statistics for the netherlands showed a conspicuous decrease . in females the decrease amounted to 6 per cent , in males to 9 per cent approximately . in the different age - groups it was about the same . this statistical decrease was very pronounced in lung cancer in males ( table i )  . in this paper the forowing tumours are expressed in terms of headings of the detailed intemational list of causes of death : " lung cancer " : no . 
231 ( revision of ( the figures for deaths from lung cancer in females are too small for a 1948 )  . statistical analysis and will be left out of consideration in this paper )  . 
with cancer of most other organs the decrease was less than with lung cancer , and in breast cancer and in some other cancers there was no decrease at all . in norway , according to kreyberg ( quoted by doll , 1953 ) , there was a similar dip in the mortahty curve for lung cancer in the same years , whereas in england and wales this curve continued without any interruption ( don , 1953 )  . in my report for the symposium on the endemiology of lung cancer in louvain , in 1952 ( korteweg , 1953 ) , i left the question undecided , whether the statistical decrease of mortahty from lung cancer resulted from mis - diagnoses due to war circumstances - non - functioning of the x - ray apparatuses for instance - or whether indeed in these years fewer people died from this disease . according to the central bureau of statistics , during the hunger winter of 1945 1784 males and 609 females died from starvation in amsterdam , a town of about in the first weeks after the liberation the number of persons 800 , 000 inhabitants . suffering from hunger oedema amounted to many tens of thousands . 
he pointed out heading 57 of the detailed intemational list of causes of death , revision of 1938 , under which ar tumours of undetermined nature - those tumours of which it was not reported whether they were mahgnant in one of its subgroups the figure for the tumours of undeor not - are recorded . termined nature of the respiratory organs is given . it appeared that in the same years that the decrease in lung cancer was greatest , those undetermined tumours of the respiratory organs , a very small group under normal circumstances , had strikingly increased . evidently in this group many cases of primary lung cancer were hidden . 
the length of the ordinate for a given age - group , therefore , gives the percentage pertaining to that age - group of the sum of the lengths of the ordinates of all age - groups together . unbroken line : lung cancer . broken line : tumours of undeterxnined nature of the respiratory organs . dotted line : cancer all sites . the vertical dashes at the top of the graph give the averages for the periods in question , i.e. 
the increase of lung cancer mortality in the last 40 years points to an increase of the sum total of cancer promoting influences . the older people of to - day hved a great part of their lives in a period when the menace from these influences was less than it is at present . 
as contrasted with the situation with younger people , therefore , mortality from lung cancer in the higher age - groups does not correspond to the sum total of cancer - promoting influences of to - day , but to this sum in an earlier period . it can be calculated that an inclusion in the group of undetermined tumours of the respiratory organs of even a small number of metastatic cancers possessing the normal age curve would have substantially altered the age curve proper to lung cancer . 
2 gives the crude death rates in males per million living in each year for this combination of recorded and probable ( though not as such recorded ) lung cancer deaths in the netherlands . ' 14t l\ i - i - - i 1938 - i . 
korteweg from the corrected curve . ( d ) the concavity in the curve for the years 1938 to 1941 has disappeared during discussions with officials of the central bureau of statistics on the reliability of the data on which the statistics of the causes of death are based , facts appeared which threw a new hght on our problem . in the netherlands the physician has to fill in two forms for each death . 
one in small vfllages where everyof these goes to the local civil registrar , a layman . body knows everybody the secrecy of this form is not absolutely guaranteed , and this leads , in cases of death from , for instance , venereal disease or cancer , to many physicians reporting meaningless diagnoses , such as heart failure . itnder normal circumstances the official netherlands statistics of causes of death are based on the second forms , which find their way , in a sealed envelope , to the medical official of the central bureau of statistics in the hague . the diagnosis mentioned on this form is incomplete , the medical official makes inquiries of the physician responsible for it as to the complete diagnosis and eventually corrects it . 
as the secrecy of these forms is ensured , there is no reason whatsoever for reserve . in 1944 and 1945 - when there was a general railway strike and other means of transport were extremely scarce and undependable and in 1946 , there was a lack of opportunities for making inquiries about incompletely fired in - forms . this reduces the rehability of the statistics for cancer for these years . 
the statistical decrease of cancer of the cervix uteri mentioned above , as well as the greater part of the statistical decrease of deaths from lung cancer find their explanation in this fact . the situation was by far the worst in 1945 , when the war front cut the netherlands in two . 
the mortality statistics for that year are based exclusively on the diagnoses given on the forms which were sent to the local civil registrars . it is clear that this was detrimental to the netherlands statistics for 1945 , and that to search for other explanations for the big statistical decrease of deaths from lung cancer in 1945 would be a mere waste of time . the only part of the dip for which no explanation can be given is the decrease this is the only indication that of i 0 per cent of lung cancer deaths in 1947 . the low level of tobacco consumption or the severe malnutrition in the foregoing years might have somewhat influenced mortahty from lung cancer . this decrease is rather small , however , and in 1947 eving conditions in the netherlands had not yet quite retumed to normal , so that it would not be wise to attach much importance to it . the cause of the great differences in the numbers of deaths recorded from undetermined tumours of the respiratory organs between the years before and after 1941 could not be discovered . 
maybe changes in the staff or the working methods of the central bureau of statistics or changing over from the revision of 1929 to the revision of 1938 could account for it . 
the straightening of the curve for the crude deathrrates for the years 1938 to 1941 , after correctio ' n for the undetermined tumours has been made , seems an argument in favour of the supposition that most of these tumours were in fact true lung cancers . 
1. received for publication january 21 , 1948 . surgery in the form of the so - called radical operation is in general at the present time the principal weapon in the treatment of carcinoma of the breast . what it can achieve and its limitations are now fairly well established . 
thus it is known that if a patient with carcinoma of the breast has microscopical invasion of the axillary glands , the strong probabilities are that the disease has passed beyond the local area and that the patient will sooner or later succumb it is to the disease , although there will be a minority of fortunate exceptions . also known that if the axillary glands are not invaded the chances that the patient will be cured of the disease are appreciably increased . 
the present article attempts to assess the comparative results of a personal series of cases in which various techniques of treatment were used . the technical surgical problem in carcinoma of the breast has been rendered clearer by modem work on lymphatic anatomy , and in particular by that of gray ( 1939 )  . this has shown , firstly , that the dermis is a plane rich in lvmphatics and hence a rich potential plane of spread of carcinoma , particularly if the growth has spread into or near the skin ; and secondly , that the deep fascia is a plane devoid of or very poor in lymphatics , and hence not an important potential plane of spread . the former fact suggests greater radicalism in removal of skin , and the latter removes the main pathological reason for the routine sacrifice of the pectoralis major muscle . accordingly , since the appearance of gray 's work we have modified our technique to remove more skin , in our more recent cases skin grafting in a high proportion , and we have gradually abandoned routine sacrifice of the pectoralis major , only removing it if actually invaded , which is rare and late . the argument is sometimes used that the removal of the pectoralis major is necessary for the adequate dissection of the axilla , and that in any case its nerve supply is bound to be cut . these technical arguments are with elevation of the arm , retraction of the pectoralis major and not valid . removal of the pectoralis minor it is easy to do a complete clearance of the axillary glands and fatty tissue right up to the apex of the axilla , and at the same time to preserve the lateral pectoral nerve , the main nerve supply to the pectoralis apart from this modified radical operation there are smaller series of major . cases which have been treated in other ways , e.g. 
the comparison between the figures of standard radical and the modified radical operation in this series is rendered more difficult in that the modified radical was evolved out of the standard radical , and hence has not been done for so long . 
survivals it would therefore seem fair to conclude that these figures bring no evidence to support the view that the addition of the removal of the pectoralis major muscle brings any increase in the survival figures , and to raise the question whether the routine removal of this muscle should remain an essential technical point . a further way in which the two operations can be compared is by the comparative incidence of recurrence in the operative area , i.e. 
skin , chest wall and out of 42 traced standard radical operations there were 10 cases with axilla . of these , 7 were recurrence in the operative area , chiefly skin recurrences . cases with original lymphatic glandular involvement and 3 without such involveout of 40 traced modified radical operations there were 7 local recurment . of these , 5 were cases with original lymphatic glandular involvement rences . while the incidence in both is too high , and and 2 without such involvement . approximates to the 22 per cent noted by truscott in the middlesex hospital series , the standard radical shows no lower incidence of local recurrence than the modified . the 3 other types of procedure which have been carried out were : ( 1 ) in the first place there were 10 cases in which partial mastectomy was combined with the usual full axillary dissection after the removal of the pectoralis minor . ( 2 ) secondly , there were 9 cases in which a simple removal of the breast was combined with irradiation to the axilla . ( 3 ) thirdly , there were 7 cases in which irradiation only of the breast was combined with axillary dissection . the last group comprised cases which were all advanced , the glands being invaded in all . 
one case died as a result of the operation ; the other 6 died of the disease at intervals varying from 6 months to 4 years after treatment . moreover , in a high proportion of cases - 4 out of 6 cases which survived operationthere was either failure of the irradiation to get rid of the original primary growth in the breast , or recurrence of the growth locally after apparent disappearance . in view of the advanced character of these cases , the ultimate fatal result was likely whatever form of treatment was adopted . 
of the 2 cases with invaded glands , 1 was alive with the disease at 5 years and 1 died of other causes at 2 of the 5 cases with glands not invaded , 3 were alive and well at 10 years , years . 9 years , and 5 years , 1 was alive with the disease at 8 years , and 1 had died of other causes 1 year after operation . there were also 3 cases in which no histological note was made of the condition of the axillary glands ; of these , 1 was alive and well at 6 years and 2 died of the disease . 
from the point of view of survival after operation , this group compares favourably with other groups . but the procedure has been abandoned because of the occasional further development of carcinoma in the portion of the breast remaining . this happened in 2 of the cases of this series , and it also happened in other similar cases in a private series , in spite of the fact that , as already noted , only small and apparently early cases were considered suitable for this procedure , that a wide area of breast tissue around the growth was removed , and that post - operative irradiation was it was concluded , therefore , that while in an occasional case given as a routine . partial mastectomy combined with a dissection of the axilla might be justifiable a conclusion supporting that of fitzwilliams ( 1940 ) and of mitchener , bailey and price ( 1937 ) - the danger of further development of carcinoma in the remaining breast tissue rendered the procedure an unwise routine . the last group was of 9 cases in which simple removal of the breast was the only surgery performed , the axilla being treated by irradiation . these cases wvere usually elderly patients with apparently early growths . 
the main routine removal is not necessary ? advantages of preserving the pectoralis major are three . firstly , there is the cosmetic consideration , mutilation being much less with the pectoralis major preserved as compared with the skeleton - like prominence of ribs and costal cartilages after - its removal . 
and if there is no curative advantage in removal of the muscle , cosmetic considerations , although secondary , are entitled to a place . secondly , there is less loss of blood if the muscle is not removed , and consequently less operative shock . while in most cases this does not amount to a point of much practical importance , in old or feeble patients it may . with preservation of the pectoralis major combined surgical treatment of the breast and axillary contents is , in our experience , much less upsetting than simple mastectomy combined with irradiation to the axilla , and we have as already stated for this reason largely abandoned the latter procedure . 
1. received for publication january 13 , 1948 . one of the implications underlying the work of huggins and hodges ( 1941 ) on the factors governing prostatic hypertrophy is that malignant prostatic cells are not fully , if at all , autonomous . that is , they are still controlled in some measure by the same factors that control normal prostatic cells . specifically , this is certainly true of their susceptibility to the influence of circulating androgens and oestrogens . carcinoma of the prostate is essentially a disease of old age . the possibility exists that the chief factor in deciding the individual 's susceptibility to this disease may be his androgenic state , that is , the level of circulating androgens in his blood , particularly during the later decades of life . the only practical method for ascertaining androgenic state is a determination of 17 - ketosteroids excreted in the urine of the subject . in the hands of many different workers ( barnett , henly , morris and warren , 1946 ) this method has revealed a very wide range of excretion of 17 - ketosteroids by normal men , at least in the lower age - groups . 
the hvbrid females of each litter , when four to six weeks of age . were mark - ed indi - vidually and di ' %ided into experimental and control n - lice . 
shown bv irregular movements of the indicator between 3 ' and these bursts last for a few seconds , and are separated bv shghtlv longer after the indicator has re - ached zero . 
grow and form large embrvomas which persist for months or indefinitely . the following series of experiments was , undertaken to gain knowledge of the beha - viour of such embrvo grafts under various conditions . 
the teratomas consisted of a me ' lange of normal tissues arranged - in an irregular manner skin , cartilage , bone , around cysts containing hair , skin and various secretions . marrow , muscle , fat , cubical and columnar epithelium , lymphoid tissue , blood vessels , glandular structures and pigment were all found . 
no necrotic patches were present , nor was there evidence of any reaction on the part of the host . in order to discover the best time to transplant such a primary teratoma for passaging mice were killed once a week , beginning a week after inoculation , the ' teratoma removed , lightly minced with scissors and a small portion ( approximately 0 - 03 - 0 - 05 c.c. ) iiioculated with a grafting needle into the right flank of in this generation increase in six cm mice . size of the graft occurred in 66 per cent of transplants done before the 4th week , in 33 per cent or less in those between the 4th and the 8th week , while after the 10th week practically no increase in size took place , the small masses either persisting in practically the same state as when implanted , or actually disappearing . several of those passaged at the first and second weeks were again divided and a portion transplanted . these only increased to between 12 x 6 mand 4 x 4 this is the 2ageneration . 
the e of 8toring findy min - ed embryo tiww in glycerol at 40 c . - the embryo tissue was passed through the craigie pressure mi ioer and then stored in ampoules at 4 ' c . 
extremely active material capable of s " rdng fivsh t clours in less than two weeks has been obtained from both chemically induced and spontaneous sarcom firozen at - 790 c . 
1. received for publication february 6 , 1947 . attempts to find some reliable basis for prognosis in carcinoma of the breast several factors have been thought valuable in have proved disappointing . formulating a prognosis , chief among which have been the presence or absence of secondary deposits in the axillary lymph nodes and the histological character but it has been found that , even in cases with no axillary involveof the growth . ment and carcinomata of low histological malignancy , there has been a mortality from recurrence of about 25 per cent in the first five years after operation . the axillary lymphatics were the only path by which carcinoma cells could escape from the breast , this mortality would be inexplicable . 
a biopsy specimen from one case in the first case the internal mammary gland was removed was also used . post - mortem in 1938 from a patient who died eleven days after a radical mastectomy . 
the internal mammary vessels also lie in this fat in a plane posterior to the glands and usually about half an inch lateral to the edge of the sternuthe glands may be either medial or lateral to the vessels . 
a thin but strong sheet of fascia , the costosternal fascia , intervenes between the glands and vessels and the pleura in the upper two spaces , and the transversus thoracis muscle in the lower spaces . 
the obliquely running the external intercostal membrane and the internal intercostal muscle are reflected as a somewhat ragged flap , either from lateral to medial and hinged on the inner end of the intercostal space : or from medial to lateral and hinged an inch lateral to the edge of the sternuwe prefer the ' former method , since bleeding from the perforating branch of the internal mammary artery seems easier fibres of the intercostal musculature are so loosely bound together that this flap cannot be neatly sutured back into once the intercostal flap has been reflected , position at the end of the operation . dissection should proceed with non - toothed dissecting forceps only . 
they might give rise to troublesome haemorrhage , but this should easily be controllable by packing while the main trunk was being ligated in the spaces above and below . closure of the intercostal space is done as neatly as possible but is seldom complete . 
cushing , my house - surgeon , has in three instances cleared out the anterior mediastinum on one side for recurrent cancer . it is very likely , i think , that we shall , in the near future , remove the mediastinal contents at some of our primary operations . " this idea does not seem to have been followed up . 
sampson handley ( 1922 ) explored the anterior mediastinum in six cases of carcinoma of the breast , finding glands in two , both of which were the seat of metastasis . 
he described in detail a case in which recurrences ' appeared in the inner ends of the intercostal spaces , one after another from above downwards , in a patient who finally succumbed to the disease twelve years after a radical mastectomy ; and he stated his belief that , by the time the axillary glands were enlarged , the internal mammary glands had frequently , and perhaps usually , been invaded . scarff and liandley ( 1938 ) investigated the ten - year results of radical mastectomy in 172 cases of carcinoma of the breast . 
they found that patients without evidence of axillary deposits ( the so - called stage 1 cases ) had a mortality of 25 per cent from recurrence in the first five years after operation , and that this mortality continued at about the same rate between the 5th and 10th years . 
the treatment of these glands must be by some form of radiotherapy . there seems much to commend sampson handley 's method of burying radium tubes in the intercostal spaces at the time of operation , thus securing a localized but intense irradiation of those points where intensity is most needed . it remains to discover whether , in a large series of cases , invasion of the internal mammary glands is as frequent as it would appear to be , what influence the site of a carcinoma in the breast has on internal mammary deposits , and what is the best method of treatment . 
microscopic examination of this gland might greatly increase the accuracy of prognosis , and prove of considerable assistance in post - operative treatment by irradiation . our thanks are due to the director , the bland sutton institute , the middlesex hospital , for permission to use the pathological reports ; to professor r . 
the frankly keratinizing members of our series we have taken as a standard with which to compare the behaviour of our remaining histological types . the morphological features of the more differentiated epitheliomata have been so completely evaluated that any further discussion would be superfluous . 
the mincer is shaken immediately to disperse the mince if the coarse plunger has been used the cap and operating in the suspending fluid . screw are detached and the fine plunger is inserted . tlle cap and screw are replaced and mincing is completmed . the suspension may contain coarse fragments of fibrous tissue or portions of iiiince which have clotted before dispersal in the suspending fluid . these may be removed either by l ' ow speed centrifugation , or by filtering the suspension througli a column of glass ballotini of suitable diameter . the mincer , which is illustrated in fig . 
1 , is the sixth of a series desigiied to all models have proved most satisfactory for operate with grooved plungers . the purpose for which they are intended , and it might be suggested that this tvpe of mincer will , for special purposes , be suitable for preparing suspensions of manimalian tissue or fowl embryos infected with certain viruses or bacteria . i wish toacknowledge my indebtedness to w . 
it is to ' be expected on theoretical grounds that temperatures below the fi - eezing points of the eutectic mixtures of the inorganic salts would favour survival of activitv . 
an equallv pending tumour mince in drying experiments . important reason for the use of dexlrose suspending fluid . tissue mince suspended in saline or ringer solution and frozen m a thin laver progressivelv consequentlv the dr , % - mg process becomes separates from glass during drying . greatlv impeded because of the low rate at which thermai energy is conducted across the intervening vacuuwhile dried fragments mav break off and mav be 22 ' c . 
the thermal conductivity of the dried material is adequate for the rapid drying of thin layers . water is removed from the tumour suspension by the low temperature con79 ' c . 
presents no difficulty , but there densation method . are technical problems in maintaining the drying tissue at a constant temperaif the lead from drying flask to condenser is of sufficient diameter ture level . and the vacuum is adequate , the problem is not one of cooling , but of supplying the maximum of thermal energy for rapid evaporation without heating the frozen it was considered undesirable mass above the chosen maximum t - i.imperature. to attempt to control the temperature of the drying mass on the basis of thermocouple readings . there is no guarantee that a thermocouple junction can be placed at that point in the frozen mass which will be the last to dry . 
the arm of the u - tube distal to the pump is extended horizontally and then downwards , to form the exit tube from the condenser flask . this exit tube is furnished with a ground glass taper which fits the neck of the flask . 
the stirrer rod is attached bv means of a slotted clamp which faeihtates assemblv with the thermos bath and drying flask . the rubber ring which drives the disc if the variable speed gear is mounted on a wheel which can be moved along the horizontal bar . this bar is mounted on two spring - loaded arms . 
a pliotographically reduced protractor scale is cemented to a piece of perspex 2 - 5 x 13 x 65 mand the pivot is centred at the origin of this scale . the vane is a piece of photographic dry mounting tissue 3 x 8 mm . , which is attached by shellac to a piece of fine copper wire 0 - 01 min diameter . 
the combined weight of vane and wire is 3 - 7 mg . , so that the vertical component of its weight at a displacement of v from its zero position is 0 - 065 mg . ( 4 ) vibration dampers . - owing to the design of the glass - drying system and the use of a sensitive vapour flow indicator , it is necessary to check the slight vibration arising from the electric motor driving the pump . 
the distribution of the frozen rnince is readily controlled if the level of ethyl cellosolve in the freezing bath is adjusted so that the flask will float with its neck resting on the rim of the thermos jar and can therefore be spun quickly by hand . the temperature of the freezing bath may it has not yet been determined whether a preliminary 30 ' c . 
shown bv irregular movements of the indicator between 3 ' and these bursts last for a few seconds , and are separated bv shghtlv longer after the indicator has re - ached zero . 
grow and form large embrvomas which persist for months or indefinitely . the following series of experiments was , undertaken to gain knowledge of the beha - viour of such embrvo grafts under various conditions . 
philps. from the department of clinical pathology , university college hospital , london , w.c.1. received for publication july 2 , 1954 . the examination of sputum for carcinoma cells can only be considered a diagnostic method of clinical value if false positive diagnoses be avoided and cases wrongly thought suggestive of carcinoma reduced to a minimuthe method cannot be used to exclude carcinoma as it is evident that malignant cells may not be found if they are present only in small numbers , or in the case of an early it must be accepted , therefore , that growth the sputum may contain none . 20 to 25 per cent of bronchial carcinomata will be missed by this method and the problem is to be sure that a positive report is as reliable as possible . 
1 , 2 and 3 contained a considerable amount of necrotic epithelial tissue , and in one small group of cells , two mitotic figures , one of which is shown in fig . 
4 , 5 , 6 and 7 . both cases the appearance suggested a clump of carcinoma cells but the ciliated border could in places be clearly seen , making the true nature of the cells evident . bronchial epithelial cells sometimes show vacuolation of the cytoplasm and may then give a disorderly appearance with may lead to confusion with carcinoma cells , , such an appearance is illustrated in fig . 
 - on close inspection of this clump , it was clear that the individual cells did not form part a fragment of tissue as there welre spaces between them , and they had more cytoplasm than do oat cells . 
the cells bear a strong resemblance to oat cells but can be distinguished from them because the cytoplasm is relatively abundant and the nuclei of adjacent cells show no tendency to moulld together . 
13. - part of the fragment under higher magnification . the pattern of the cells resembles that seen in oat cell carcinoma , adjacent nuclei showing a tendency to mould together . there is more cytoplasm separating the nuclei than is commonly seen in oat cells , and the chromatin pattern is nowhere visible whereas in oat cells it is usually clearly seen . this appearance was reported as being suggestive of carcinoma . 
17. - a corpus amylaceum enclosed within a cell which appears to be of epithelial origin . the nucleus of the enclosing cell was at the periphery of the enclosed body but is not well shown in the photograph . the corpus amylaceum was semitransparent and was devoid of any nuclear characteristics . 
the nuclei of the individual cells mould together rather as do those of oat cells , giving the whole clump an appearance resembling oat cell carcinoma . all the nuclei however , are dense and the cells possess more cytoplasm than is usually seen in oat cells . 
the specimen was reported as follows : " films show clumps of cells , the arrangement of which is suggestive of oat cell carcinoma though the individual cells are not sufficiently characteristic to indicate malignancy . " the diagnosis of bronchial adenoma was made at bronchoscopy and confirmed at post mortem nine months later following the patient 's death from coronary thrombosis . ( e ) appearances due to macrophages of unusual type . macrophages , when they are seen to contain dust particles , can be easily identified , but when devoid of such particles , they may sometimes be confused with carcinoma cells . 
the nuclei are central , multinucleate cells frequently occur in carcinoma but they and number about 12 . are in no way diagnostic of it , the commonest multinucleate cell seen in sputum films being the macrophage . this example is the largest that i have seen . 
 two recent investigations , both from the united states , upon the arsenic content of tobacco , and the volatilization of this arsenic when tobacco is smoked , have been reported . 
the work of these authors differs from our own in that they used artificial methods of combusting the tobacco , which may or may not repro duce the conditions present when smoking is carried out in the ordinary way , and they found no brands of tobacco containing only minimal quantities of arsenic . 
 ( 1 ) gross and nelson ( 1934 ) employed a method which consisted of digestion in nitric and sulphuric acids , precipitation of magnesium ammonium arsenate , solution in hydrochloric acid , and estimation by the gutzeit method . 
five such analytical groups were analysed for each brand studied . " they found the content of pooled groups of 4 cigarettes of 5 brands to range from 97 to 363 p.p. 
 ( 2 ) thomas and collier ( 1945 ) , using a modified cassil - wichmann method , found that " individual cigarettes and cigars of a given brand varied widely in arsenic content , " which ranged in pools of 2 to 4 cigarettes from 2 packs of 20 ( presumably of the same brand ) from 354 to 114 p.p.m. , while cigars ( 132 to 295 ) and pipe tobaccos ( 227 to 428 ) showed a lower range ( table i )  . 
gross and nelson ( 1934 ) attribute the rather narrower range found in cigarettes and in pipe tobacco , compared with cigars , to the mixing which the former receive , but this difference is not seen in the results for cigarettes and cigars of thom.as and collier ( 1945 )  . 
in american pipe and chewing tobaccos ; using suction by a water - pump , he concluded that " we can say roughly that half of the arsenic is evolved in the smoke gross and nelson ( 1934 ) used an apparatus drawing about 50 ml . 
 each : 207to256 211 , , 267 ' 253 , , 363 97 , , 130 229 , , 261 range in 5 single cigars from each of 5 brands : 229 241 332 116 247 83 to 484 range in 5samples from each of 4 brands : 260 to 500 116 to 266 311 to 451 1 - 5 1 - 4 thomas and collier : cigarettes " a single pack of 20 " " ali.other pack " 1 - 4 " groups of 2 to 4 . " 354 ; 400 ; 405 ; 472 ; 600 ; 61 - 4 * 614 ; 670 ; 714 ; 845 ; 1140 132 ; 225 ; 262 ; 295 cigars pipe tobacco cigars ( about 10%cutoffat ends ) pipe tobacco 1 - 5 396 ; 265 ; 227 ; 345 ; 428 * these figures represent the actual analyses in p.p.m. , on pooled groups of 2 to 4 cigarettes , and hence are not calculated means , though each figure represents the mean composition of the eigarettes in one pool . 
cigars and cigarettes were " smoked down to about 1 / 2 to 3 / 4 " ; the arsenic the " puffed " and " unpuffed " smoke was absorbed and estimated separately . 
 " the pipe smoker who smokes all the tobacco does not therefore have the protection afforded by the butts of cigars and cigarettes . " from the present point of view this question is not of great interest ; the important datum is the amount of arsenic inhaled , and in this country only about one smoker in ten smokes a pipe ( hansard , 1945 )  . 
in their first series ( table ii ) cigarettes of 7 c length were smoked down to 1 c ; in a later serjes only 2 / 3 was burned . 
 the arsenic found was compared with analyses of whole cigarettes from the same pack , " but in view of the large differences they later cut off about os c for analysis ; apparently they failed to discover that this method also can be falla cious . 
 our earlier results ( table iv ) were obtained by the gutzeit method , which depends upon the brown and yellow colours produced in paper impregnated with hgc12 ; it is fitted for the measurement of amounts of as20 3 between 10 and 1 g . , and shows differences most clearly in the range of 8 to 3 g . 
there may be con~ siderable differences in the matches made by different persons ; in these experi ments the mean was taken of the readings made independently by two persons unaware of the nature of the unknowns . 
the iodometric method of thomas and collier ( 1945 ) was adopted later ( tables iii , v and vi ) in view of the difficulty of determining the small amounts of arsenic lost in smoking . 
the method has the advantage that , whatever may be its errors in other respects , there is less disagreement over the very sharp end - point ( titration of iodine and starch ) , about which two observers usually do not differ by more than 005 c.c. 
 the estimations upon brands p and c were usually carried out upon amounts of 20 to 30 g . , as a method which is sufficiently accurate within this range 176 m . 
gross ( 1933 ) has drawn attention to the occurrence of such errors in the estimation of arsenic in tobacco , which are attributed to uncombusted residues of pyridine and nicotine ; we failed to obtain satisfactory results by the method which he devised to overcome this difficulty . 
 in the previous investigations summarized above artificial methods of smoking were employed , air being drawn through a pipe , cigar or cigarette by means of a water - pump . 
we have confined our experiments wholly to cigarettes smoked by one or other of three persons accustomed to this form of smoking , and they were asked to do this in their ordinary way ; the two brands used ( p and c ) are in common use in this country . 
the ash , and stump , were dropped into separate weighing bottles in our earlier experiments , but latterly the two have been analysed together ; the amount of arsenic found , if less than that in the cigarette , should indicate the amount volatilized in the smoke , of which a part must have been inspired . 
 before this width of range was realized we obtained many contradictory results , showing amounts in the ash and stump which were sometimes less , and sometimes more , than that thought to be present originally . 
 8 whole cigarettes 9 cigarettes ( 7 wholes and 2 halves ) 5 pieces from 3 cigarettes 1 piece from each of 4 cigarettes 6 successive pieces cut from 1 cigarette 13 estimations on mixed tobacco of 10 cigarettes e 10 range in 5 packages of brand p brand o . 
 678 823 307 496 461 275 10 pieces from 5 cigarettes 5 successive pieces cut from 1 cigarette a 20 a 20 11_ estimations on mixed tobacco of io cigarettes . 
but as the weight of most cigarettes does not differ very much from one gram the figures give a rough measure of the arsenic in one cigarette , which is of more obvious practical interest . 
the results were again contradictory , and we found that such suc cessive portions may show a range of 388 to 587 , or 100 : 151 in p , and of 306 to 542 , or 100 : 177 in c ( table iv )  . 
 in the hope of obtaining more uniform material , the papers were removed from the cigarettes of a package of 10 or 20 , and the tobacco mixed by hand and 178 m . 
but even this treatment does not give satisfactory results ; it is very difficult to take up samples of such material which will contain constant propor tions of the coarser and finer particles , as the latter tend to fall away from the . 
moreovar , the minced tobacco , even when moistened , is not easy to smoke in the same way as ordinary tobacco : adjacent cigarettes of brand p from a much larger package , containing 100 , were taken ; but these at first showed a wide range ( 495 to 766 , table iv )  . 
 that an average of 158 per cent of the arsenic is lost in the process of smoking and had presumably been volatilized ; this loss is statistically significant ( p = 0001 )  . 
the same method was applied to brand c , of which the largest boxes available contained 50 ; the first two rows showed in 18 cigarettes a loss of only 76 per cent , which was not statistically significant ( p = 02 )  . 
 580 527 623 558 603 418 456 458 568 556 617 } 681 mean 596 631 427 412 471 533 629 662 453 367 527 634 455 367 539 509 lower right row . 
kennaway the 4th row showed a loss of 182 per cent , which is just significant ( p = 005 ) , in spite of the small numbers ( 12 cigarettes ) involved . 
 the most likely source of the arsenic present in some tobaccos , which has been suggested by several authors , is the spraying of the adult plants with insecticides , and this particulate method of application would explain the difficulty in obtaining concordant analyses . 
 of the arsenic volatilized in smoking , a part must escape while the cigarette is not in the smoker 's mouth , and a part of what he inspires is expired again , hence the amount retained is no doubt very small . 
the concentration of arsenic in cigarettes containing the larger amounts is very \rariable ; this irregularity is perhaps due to a method by which the arsenic may have been introduced , namely , by the spraying of the plants with insecticides . 
an estimate was made of the amount of arsenic volatilized in smoking , by comparing the content of cigarettes , and of the ash and stumps derived from them , but the wide range of arsenic content makes it difficult to infer the amount present originally in a cigarette which is to be smoked . 
the results indicated that from 76 to 18 2 per cent of the arsenic present was lost in smoking ; this figure is of the same order as but somewhat lower than that obtained by some previous investigators who have used artificial methods of smoking . 
salaman. from the cancer research department , london hospital medical college , london , e.l. received for publication march 15 , 1952 . if a chemical carcinogen is applied to the skin of mice at a concentration just too low to produce tumours by itself and , after an interval , a co - carcinogen is repeatedly applied to the same site , tumours . 
weekly applications of 2 * 5 per cent croton oil in paraffin to both groups were begun 6 weeks after an initial treatment with 0 - 15 per cent dmba . 
croton oil treatment of group 5 was stopped after 8 applications , when the average tumour incidence in both groups was about 0 - 5 per mouse . incidence in the two groups increased for a further 2 to 3 weeks , after which incidence in group 4 continued to rise , following the curve usual in this type of experiment , while that in group 5 remained almost constant at about 2 tumours per mouse . after 9 weeks without treatment there had been no appreciable change in tumour number in this group , though the tumours already visible had continued to grow . 
tumour incidence in group 5 had , by then , reached about 11 tumours per mouse ; it continued to rise for a short time , as before , then fell a little , and again remained approximately . 
1. - comparison of the effects of continuous and intermittent weekly applications of croton oil to mouse skin , 6 weeks after a single application of a carcinogen . consequently individual points in fig . 
1 , which represent by others , is high . average numbers of tumours per mouse , have high standard errors , and the differences between corresponding points on the curves of groups , 4 and 5 are barely significant . it is easy to show , however , that the curves as a whole differ their slopes between the 15th and 21st week were compared as significantly . follows : the average increments .of tumour number of individual . 
one must suppose that there is a critical size , rather less than 1 mdiameter ; i.e. , that tumours smaller than this do not continue to grow without further stimulation . did these invisible tumours remain unchanged during the remission of treatment ? apparently not , for when the treatment was resumed there was no immediate outburst of newly - visible tumours . after 58 days the interrupted rise in numbers this latent period is not significantly different from that of the continued . response to the first course of croton oil treatment . 
the skin behaved as it would have done if it had had no previous co - carcinogenic stimulation . it is possible to conclude that the change produced by croton oil in mouse skin previously treated with a carcinogen is not sudden , or independently proit is a gradual change , requring repeated applications for its maingressive . tenance and progress , which is reversible during the greater part of its course , but becomes irreversible not long before tumours become visible . it has been previously noted ( shubik , 1950a , 1950b ; salaman and gwynn , 1951 ) that of the tumours produced in mouse skin by croton oil following a single treatment with a carcinogen most are benign , though some reveal or develop a malignant character later . 
the difference between these two latent periods is not significant . ( 3 ) these results are discussed . it is concluded that the change produced by croton oil in mouse skin previously treated with a carcinogen is a gradual one , requiring repeated treatments for progression towards tumour formation , that it is reversible during the greater part of its course , but becomes irreversible not long before tumours become visible . i am indebted to professor s . 
on the 4th day the males were removed from the boxes and 39 females which had shown plugs were placed in separate boxes , these constiforty - three unmated female mice of similar tuting the experimental group . average age , and wherever possible litter mates of the experimental mice , made the control group . on the day of separation , each of the mice received a subcutaneous graft , roughly 2 mx 2 mm . , in the right flank , from a 25 - day - old transplantable methylcholanthrene - induced spindle - cell sarcoma growing in cba mice . this tumour retained the original histological appearance and characters of steady and uniform growth through successive generations , and was chosen because its rapid growth was considered an advantage in view of the shortness of the pregnancy and lactation periods in mice . from the 10th day following grafting the tumours were measured every 4th or 5th day in 2 diameters ( length and breadth ) until the end of lactation , i.e. until 19 days following parturition . 
1 by curves obtained by plotting the average of the sums of 2 diameters ( i + b ) against time , as described by haddow ( 1938 )  . because of the difficulty in obtaining a large number of pregnant mice at one time , the experiment had to be performed on 6 batches of mice , 25 - day - old tumours of successive generations being used for grafting . 
leveaux. * from the westminster hospital , london , s.w.1. received for publication may 12 , 1954 . the earliest recorded description of carcinoma of the pancreas is attributed to mondiere in 1836 . 
da costa ( 1858 ) of philadelphia reviewed 37 cases and gave a comprehensive description of the clinical presentation of this disease with * nmphasis on pain as a prominent sympton in 32 of these patients . 
in not a few cases it is increased by the erect position and hence we find patients seeking relief by stooping and curving their body forward so as to relax the abdominal parietes . " physicians of the french school sustained their interest in this condition , and bard and pic in 1888 observed the common association of a palpable gall bladder with jaundice , and the frequent incidence of cachexia . 
from the descriptions given by these and other observers the concept of painless jaundice as the classical form of presentation of this disease spread widely . mirallie ( 1893 ) found glycosuria in 3 cases , and chauffard ( 1908 ) emphasized distinctive features of growths involving the body of the gland . speed ( 1920 ) , eusterman ( 1922 ) , eusterman and wilbur ( 1933 ) , kiefer ( 1927 ) and other observers have subsequently reported on series of cases , and berk ( 1941 ) has included these in his review of a total of 1449 cases . 
levy and lichtman ( 1940 ) , and duff ( 1939 ) have further clarified the picture of carcinoma of the body and tail of the pancreas , emphasizing early and severe pain , ascites , venous thrombosis , and widespread metastases to liver and peritoneum as important features . towards the end of the last century surgeons became interested in the pancreas , and finney ( 1910 ) quotes a case of total pancreatectomy for carcinoma by billroth in 1884 with recovery of the patient from the operation . gordon - taylor ( 1934 ) successfully removed a carcinoma of the body of the pancreas in 1927 , his patient surviving when the case was reported 7 years later . in spite of such isolated successes , however , attempts at surgical removal gave little promise until , in 1935 , whipple and his colleagues demonstrated the technical feasibility of resection of the head of the gland , and opened a more hopeful era ( whipple , parsons and mullins , 1935 ; whipple , 1938 )  . these and subsequent advances in surgery have greatly intensified the need for early diagnosis in a disease which has been estimated to comprise 1 to 2 per cent of all cancers , and which is by no means a clinical rarity . 
the head was spared in 14 cases ( 30.4 per cent ) , of which 4 cases involved the body alone , 4 cases the tail alone , and 6 cases both regions . 
one case had active thrombo - phlebitis , and 1 presented with paraplegia due to extradural metastases . in many cases the disease was well - advanced by the time that abnormal signs were clear cut . 
per cent in 20 of 40 cases ( 50 per of 8 cases examined by the glucose tolerance test , a diabetic type curve cent )  . was obtained in 6 cases ( 75 per cent )  . these latter cases included 2 of the known cases of diabetes of recent onset , but none of long standing . 
n / 20 sodium hydroxide as the upper limit of normality . johnson and bockus ( 1940 ) reported a raised value in 5 of 8 cases . secretin stimulation of the pancreas was performed in 3 cases , accentuating an already raised level in 2 cases , and producing an abnormal value in 1 . 
per cent in 27 of 33 cases investigated , of which 24 had clinical jaundice . the serum alkaline phosphatase was examined in 26 cases and was raised above 5 bodansky units in 13 , of which all had associated hyperbilirubinaemia . of 13 cases shown to have liver metastases , the alkaline phosphatase was raised in 7 and normal in 6 . the serum cholesterol was raised above 220 mg . 
a normal chloesterol level occurred in 5 cases with associated hyperbilirubinaemia . the cholesterolesters exceeded 50 per cent of the total cholesterol in 20 of 21 cases . it appears , therefore , that these latter three investigations reflect only the presence of biliary obstruction , and beyond this are not helpful in the present diagnostic problem . the plasma proteins were normal in 23 of 25 cases , there being some degree of hypoalbuminaemia in the remaining 2 cases . the cephalin , thymol and colloidal gold flocculation and turbidity tests were normal in all of 22 cases examined . in 3 cases the cephalin flocculations test became positive after cholecysto - enterostomy . the value of these tests in the present connection is that they facilitate exclusion of hepatitis in cases presenting with jaundice , as pointed out by maclagan ( 1947 ) of 46 cases examined , 31 ( 67 - 4 per cent ) had haemoglobin levels below 13 - 0 g . per cent , with an average of 12.13 ( 76 per cent hb . ) for the whole series . 
a relationship between the anatomical position of the tumour and the site of the pain complained of by the patient is suggested . a scheme of investigation is proposed which includes careful radiological studies , a glucose tolerance test , serum lipase and amylase determinations and a bromsulphalein retention test . surgical exploration is advocated where strong clinical grounds alone exist . i wish to express my warm thanks to h . 
bockus , professor of gastroenterology in the graduate hospital of the university of pennsylvania , for all his help and encouragement in this investigation . i am also grateful to a . 
3 received for publication january 11 , 1951 . it has long been known that the rous sarcoma may be transmitted by dried tumour tissue and it has been concluded , therefore , that the tumour agent can survive under such conditions ( rous and murphy , 1914 ; rous , 1911 ; and hoffstadt and tripi , 1946 )  . 
the ampoules were then connected to a manifold and the ice sublimed in vacuo . knox 's ( 1939 ) apparatus and conditions were later used by dmochowski ( 1948 ) for the freeze - drying of rous v - irus suspensions produced by fractional centrifugation and other methods . 
dmochowski ( 1948 ) claimed that similar virus suspensions treated with a drop of fowl or rabbit serum suffered no loss of activity under the same conditions , but that addition of salts , such as nacl , kc1 or caci2 , had no such preservative action . 
by gentle shaking for 35 minutes . if the shaking was carried out in the absence of gas space , albeit with glass beads in the tube , inactivation was negligible . 
gave complete protection for t5 phage for 14 minutes . the duration of the protective effect was found to be a function of the gelatin concentration , since the gelatin itself protection could also be obtained with gum arabic or with is " denatured . " serum albumin although 100 - fold and 10 - fold the gelatin concentration were required . this work may well provide the theory behind the observation that viruses are more stable when diluted in serum or broth than when the dilutions are made equally one might expect that small viruses would be with salt or water . inactivated more rapidly than larger , and that the rate of inactivation would be proportional to temperature , since the forces responsible for bringing the particles to an interface will be thermal forces . such conditions as these have frequently been realized empirically . rivers and vvard ( 1935 ) sought to add a material to vaccinia virus suspension which would ( a ) act as a protective agent , ( b ) add bulk to the final product and ( c ) go back into solution with ease , carrying the virus with it . 
this suspension was clarified on the sharples centrifuge and the virus deposited from the supernatant on to a cellophane bowl lining sheet by deposition at high speed ( carr and harris , 1951 )  . this virus - containing deposit was then resuspended in a ' volume of medium ( concentration medium ) equal v / w to the original weight of tumour tissue . ( 2 ) comentration media . ( a ) buffer - trypsin , b - t . - mcilvaine 's ( 1921 ) phosphate - citric acid buffer ( plff 7 - 5 to 8 - 0 ) prepared from 0 - 2 m na2hp104and 0 - 1 m citric acid and diluted 1 : 19 with water ( buffer ) and a few mg . 
the mccartney bottles were accommodated in drihed compartments in the centrifuge head of the drying chamber of the machine . each bottle was inclined towards the axis of rotation , so that when the head was spinning the contents of each bottle formed a wedge . the virus suspensions were snap - frozen by evaporative cooling , and the purpose for spinning the bottle was 2 - fold . ( a ) frothing was prevented and ( b ) the wedge of frozen material presented a greatly increased surface area with a consequent increase in the rate of drying . 
the rate of drying was high throughout the drying cycle and no evidence was found to suggest that , as the layer of dried virus material increased in thickness , the rate of evaporation of vapour fen off and the underlying frozen mass melted ( bauer and pickels , 1940 )  . the drying cycle occupied 40 to 44 hours . 
the bottles , which were either uncapped , or lightly capped with two or three layers of sterile surgical gauze during the drying , were then screw - capped and sealed with tape and stored at 2 ' c . 
the media used , and here abbreviated , included : ( a ) buffered - 8aline , b - s . - ten per cent sahne adjusted to ph 7 - 2 with 0 - 2 m sodium phosphate . ( b ) buffer , ph 5 - o . - mcilvaine 's phosphate - citric acid , diluted 1 : 19 with water . ( e ) water - trypsin , w - t . - - solution containing a few mg . 
a similar result appears from table vii if the result of 29jr.49 is compared with that of 5.vii.49 , and from table viii , 15ar.49 being compared with 29.iii.49 ; although activation was not found in the experiments with egg albumin or egg white . freeze - drying in salt solutions ( table ii )  . the sharples deposits were resuspended throughout in , 0 - 005 m phosphate buffer , ph 7 - 2 , containing a few mg . 
50 , where lemco is compared with io per cent lemco as a medium for freeze - drying , there is a reduction in the titre with the weaker broth . freeze - drying in carbohydrate media ( table vii )  . the sharples deposits were resuspended in buffer - trypsin and " purified " in the usual way . 
or 0 - 125 per cent neutrahzed cysteine hydrochloride gave protection , and the protection afforded by 2 - 5 per cent dextrose containing 0 - 05 per cent b.a.l. 
the method now adopted , that of freeze - drying virus concentrates in lemeo broth , fulfils the condition , but little hght has been thrown on the mode of action of the stabihzing material . virus concentrates dried in this way have retained their fur activity for minimum periods of 12 months . the experiments with water alone showed that dmochowski 's ( 1948 ) results are confirmed in so far as virus may be recovered after drying - and our preparations had all been treated with 1 : 10 , 000 hcn during the isolation procedurebut it was not possible under these conditions to recover as much as 60 to 80 per cent of the initial virus activity as he claimed . salt solutions had no preservative action , and broth - containing media showed immediate advantages , even where the suspensions had been " purified " by centrifugal fractionation before desiccation . 
the action of the broth appears to be ponfined to the freezing - and - drying cycle or subsequently , since nothing was gained by carrying out the concentration stages in broth or broth - containing media , for which buffer - trypsin is quite satisfactory . it is unhkely , therefore , that the effect is solely an example of the phenomenon described by adams ( 1948 )  . 
the conditions of freeze - drying , moreover , do not involve vigorous shaking of the material but , equally , there is as yet ' no knowledge of the surface conditions which exist at an ice surface which is gradually receding through a drying mass . 
the observation that weaker ( 10 , per cent ) lemco broth is a less effective protective agent is of interest in this respect . it is possible to suppose that the action of broth and similar material is complex , that one or a combination of such factors as the forowing are important : ( a ) the broth pro - vides optimum conditions during freezing - such as an optimum eutectic point ; ( b ) that protection is conferred against the deleterious effect of ' heavy metals or of oxidation systems ; ( c ) that , in some way , the tendenoy of the virus to aggregate is reduced ; or ( d ) that an optimum amount of water only is lost . 
bartholomew 's hospital , london . received for publication may 15 , 1951 the data given below have been collected in continuation of two earlier studies ( kennaway and kennaway , 1936 , 1947 )  . stocks ( 1936 , 1947 ) has compared the death rates from cancer of the lung in males during the years 1921 to 1930 in london , and in the county boroughs , other urban districts , and rural districts of england and wales , and has shown that the rate increased with increasing urban conditions . * the same method has now been applied to the data , for both sexes ( table ii ) , of a later period ( 1946 to 1949 ) , when a great increase in deaths attributed to cancer of the lung has taken place . 
as recently as 1929 the numbers of cancers of the larynx , and of the lung , in males , were about equal ( table i ) ; since then , deaths attributed to the latter have increased enormously . 
the crude death rate for males has been falling in recent years ( 1946 to 1949 ) and in view of the ageing population this indicates an actual decrease in the incidence ; the death rate for females has been remarkably constant since these considerations show that the pooling of data for the larynx and 1935 . lung under any such heading as " respiratory system " is very undesirable . the standardized death rates show no perceptible difference in either sex between the figures for the 14 years 1926 to 1939 immediately preceding the war , and the since 1942 standardized death rates have been means for the period 1921 to 1930 . superseded by comparative mortality indices , which compare the death rate in each year with that of 1938 . . 
22 - 5 = 1 - 0 100 ' 0 82 - 2 17 - 8 100.0 the data at present available on the social incidence of cancer of the larynx show a gradient which is steep in men and absent in women ( table vi )  . 
hence the increased consumption of tobacco in recent years has not affected this form of cancer . ( 5 ) thus cancer of the larynx in men , and in women , differs in geographical , anatomical and social distribution , and in changing prevalence at the present time , and should be regarded as constituting two separate diseases . ( 6 ) the sexual distribution of intrinsic and extrinsic cancer of the larynx appears to be changing . we are greatly indebted to w . 
phillips , of the general register office , for a large part of the material contained in this paper , for help in the preparation of it , and for advice upon many matters . 
campbelt. poultry research centre at the university of edinburgh . * received for publication december 30 , 1948 . the original purpose of this investigation was to study the effects of implanting various tumnours affecting the fowl into the fertile egg . a survey of the literature revealed the rather surprising fact that apart from the rous i sarcoma ( rous and murphy , 1911 ) , and a few leucosis cases ( pierce , 1942 ) , no attempt has been made to grow spontaneous neoplasms of the chicken in fertile eggs . there is a high incidence , relative to disease in general , of spontaneous neoplasia in the fowl . 
campbell ( 1945 ) , in a survey extending over five years , found the relative average incidence to be 18 ' 7 per cent in the breeds examined , the minimum and maximum figures for specific breeds being 10 - 3 per cent and nearly 39 per cent . during this survey a number of chicken tumours were studied which bore a close morphological resemblance to known virus - associated growths . in view ofclaims by various authors ( taylor , 1943 ; heilman and bittner , 1944 ; hungate , snider , taylor and thompson , 1945 ) that mammalian tumours can be easily cultivated in the yolk - sac of the chick embryo , and that a virus - like factor associated with mammary carcinoma of mice has been directly demonstrated by this method , it was thought desirable to apply similar methods to the study of spontaneous chicken tumours . the advantages of using fertile eggs for such cultivation experiments are many . 
the chick embryo , on the other hand , has not yet been reported to be a natural carrier of virus . it has been shown by grasset ( 1929 ) , who worked with diphtheria and tetanus toxoids as antigens , that the chick embryo does not produce antibody . polk , buddingh and goodpasture ( 1938 ) showed that no complement is present in embryonic serum , and murphy ( 1914 ) first demonstrated the ability of normal heteroplastic tissues and tumours to graft on to the chorioallantois without causing an inflammatory reaction until the 18th day of incubation . subsequently some reaction of the host tissues does occur , to the detriment of the graft . the culture of tumour tissues in fertile eggs therefore resembles much more closely tissue culture in vitro than it does in orthodox animal inoculation methods . at an early stage in this investigation the frequent occurrence of typical ectodermal lesions in the vicinity of chicken tumours implanted on the chorioallantois led to the conception that such tumours might contain a factor capable of stimulating cell division . such a factor , if it existed , might be a self - propagating agent within living malignant cells , or something in the nature of a mitotic activator similar to those growth - stimulating substances present in embryonic tissues . with this hypothesis in mind it was decided to study the effects of implanting embryonic tissues , certain viruses , and as wide a range of tumours as possible , derived from a variety of animals . about this time a series of cases of spontaneous liver carcinoma in ducks came under observation , and similar experiments were undertaken with the resultant material , the details of which are recorded in a separate paper . the first record of tumour cultivation in the fertile egg was by rous and murphy ( 1911 ) , who applied it to the newly discovered rous chicken sarcoma , which they succeeded in cultivating in various sites , including the yolk - sac , and on the chorioallantoic membrane . 
they make no mention of any reaction on the part of the chick embryo or its associated membranes , and their plates only illustrate the histology of the cultivated tumours ; the membranes themselves were apparently not examined . stevenson ( 1918 ) then tried various rat , mouse and guinea - pig tumours and had about 30 per cent takes . 
campbell keogh ( 1938 ) found that filtrates prepared from the rous i sarcoma gave rise to ectodermal proliferative lesions when inoculated on the chorioallantois . these focal lesions were fully developed about the 7th day after inoculation , and took the form of flattened pearly opacities varying in diameter from 0 - 5 mm . to 2 mdilute inocula produced these lesions ; when concentrated suspensions were inoculated a proportion of sarcomatous lesions developed . pierce ( 1942 ) transferred leucosis to chick embryos by seeding fragments of leucotic tissue , e.g. 
no lesions developed on the membrane , and inclusion bodhes were absent when filtrates were used , but leucotic tissue caused gross thickening and cloudiness of the membrane . taylor , thacker and penington ( 1942 ) described the growth of cancer tissue ( mammaryv carcinoma of mice ) in the yolk - sac of the chick embryo , and claimed it to be a new method . 
the presence of necrotic tissue in the tumours resulted in the death of the embryo . in a subsequent communication taylor ( 1943 ) described the cultivation of a spontaneous mammary tumour of dba strain mice in the yolk - sac of the fertile egg . 
the yolk from such eggs produced similar tumours in mice upon injection , and taylor found that berkefeld filtrates prepared from this yolk also gave rise to tumours upon injection into mice , thus showing the presence of a virus - like principle in this particular mammary carcinoma . at about the same time heilman and bittner ( 1944 ) injected a 40 per cent suspension of mouse carcinoma into the yolk - sac of the embryonic chick , using an inoculum of 0 - 2 ml . 
they extracted the tumours from the yolk - sac , and showed that fitrates prepared from these and from the yolk itself were capable of causing mammary cancer in mice , thus confirming the work of hungate , taylor and thompson ( 1944 ) , that a virus - like body was involved . following up this line of investigation bittner , evans and green ( 1945 ) showed that the " milk factor " was able to survive in the yolk - sac for 12 days in the absence of mouse mammary carcinoma cells . 
they did not know whether the factor had multiplied in the yolk - sac . twombly and meisel ( 1946 ) attempted to grow several mammalian tumours in the yolk - sacs of fertile eggs . 
the greatest number of takes occurred with the bagg 755 mouse mammary carcinoma , but they report a very high mortality rate ( 73 per cent ) by the 17th day of incubation in their embryos . 
numerous fitration experiments were done in an attempt to demonstrate a cancer virus , but with uniformly negative results . ( a ) the intra - vitelline techniqe . the method adopted for the cultivation of tumours in the yolk - sac was a modification of that described by taylor et al . 
they were then taken direct to 95 per cent alcohol , through absolute alcohol , equal parts absolute alcohol and cedarwood oil , cedarwood oil alone , and finally embedded in paraffin wax . other tissues were fixed in 10 per cent formol saline for 24 hours . 
the eggs were sealed with their own shell flap , using paraffin wax , and this was removed on the fifth day and a cover - glass substituted . tumours were seen growing in each , dependent from the chorioallantois . 
the eggs were opened 9 days later , and both contained large ( 9 mm . ) spherical , richly vascular tumours growing from the chorioallantois and hanging down into the allantoic cavity . 
of this filtrate was injected into each pectoral muscle of a brown leghorn cockerel aged 14 weeks . typical tumours subsequently grew in these sites . hi / to / og . the only histological findings to be given in any detail will be those associated with changes in the membranes in the vicinity of implanted tumours . 
a delicate argyrophil reticulum ramifies throughout the growth , and appears to be derived from the mesenchyme of the membrane . normally the epithelial surface of the chorioallantois consists of low cuboidal cells , and is only one cell thick . 
the tube was shaken in an automatic shaking machine for 1 hour , at the end of which the suspension was filtered through a " technico " filter , using a ford 's " sterimat " grade g.s. the fitrate was used as the inoculum , the amount inoculated on to each membrane varying between 0 - 02 to 0 - 06 ml . four 10 - day embryonated eggs were inoculated , using a graduated capillary pipette as a dropper . in order to secure a wide distribution of the virus over the membrane , it was placed direct on to the shell membrane , and a tear made through this with a glass needle . 
the virus was then drawn into the egg and on to the chorioallantois by applying negative pressure to the air - cell with the aid of a small rubber teat . 
the egg was then sealed in the normal way and incubated for 3 days.when opened and examined , small roughly circular opacities were found on the chorioallantois of 3 embryos . 
an occasional attempt at the formation of a " cell nest " may be found , but usually the cells occur in groups without any sign of a whorled appearance . 
carcinoma simplex , with large round and spindle - shaped cells . experiments 10 and 11 were chorioallantoic implants using methylcholanthrene induced transplantable mammary carcinomas of mice . five 10 - day embryonated eggs were implanted with fragments of tumour and examined 7 days later . all but one contained small tumours 3 - 5 mdiameter . 
of a suspension of mouse sarcoma s.37 in twenty - seven embryos subsequently died at periods varying normal saline . most of these showed congestion and petechial haemorbetween 1 and 8 days . rhages in the skno bacteria were isolated from these eggs . 
the dead embryos showed intense congestion and petechial haemorrhages . in 2 cases tumours were found tumour - bearing membranes were attached to the interior of the yolk - sac . ground up with sand and saline , and 0 - 25 ml . 
a haemorrhagic membrane was treated in the nine days later the mice were found dead , same way and injected into 5 mice . due to a heating failure during a cold spell . six of the mice injected with tumourbearing membranes were found to have small lymphoid turnours growing in the subcutis at the site of injection . 
the membranes appeared normal upon histological examination . ( e ) spontaneouvs chicken tunours . in experiments 19 , 20 and 21 the intra - vitelline method was again tried . these experiments may be briefly dismissed , as in each case contamination with bacteria killed all the eggs . 
coli was isolated from the eggs , although broths inoculated with tumour tissue from the original case remained sterile . experiments 20 and 21 consisted of the injection of a saline suspension prepared from lymphocytomata , involving the thigh and ovary respectively . the embryos died subsequent to injection , and bact . 
hen suffering from aleukaemic lymphoid leucosis . eight days later two of the embryos were found to be dead , namely those with liver and liver plus spleen implants . only the latter had a tumour in the membrane . 
the remaining spleen only implanted embryo was living , and the membrane bore a 4 mdiameter pink tumour . in the case of the dead embryos both were extremely congested , and the livers appeared swollen and leukaemic . histological examination of the membrane bearing the spleen implant shows a vascular growth of endothelial - like structure . all resemblance to normal or even leukaemic spleen has disappeared . 
the growth is composed of an irregular syncytium of calls with round , angular or elongated nuclei , the cytoplasm of which is drawn out into processes which appear to merge with those of adjacent cells . 
the vessels are formed of a single layer of flattened endothelium and are congested . at the periphery of this tumour large numbers of primitive blood cells appear to be wandering into the mesenchymal stroma of the chorioallantois . " cell nests " occur in this region . 
an examination of the heart blood from these two embryos shows in the case of the liver only implant a large number of primitive cells which appear to be differentiating into erythroblasts , i.e. 
the bird was destroyed and immediately opened , and the viscera were exposed to the air in the post - mortem room for about 2 hours before the case was seen , but the liver surface was seared with a hot spatula at the time of implantation , and fragments taken from within the organ with sterile knife and forceps . 
the actual implants were made about 21 hours after the fowl was destroyed . broths inoculated with tumour material at the same time were later seen to be sterile . nine days later two embryos were found to be dead . 
the second method of tissue culture is involved and requires an elaborate technique , and has the great drawback that frequently only one component of the original neoplasm grows , while the rest , e.g. 
more experiments involving sub - inoculation with tissue fitrates and extra - embryonic fluids from dead and haemorrhagic embryos should help to settle this point . the chorioallantoic method has been found to be most successful in the case of the cultivation of avian tumours associated with viruses . thus , the rous i sarcoma and the duran - reynals sarcoma give the biggest growths in the membrane . these are both rapidly growing tumours , and therefore would naturally tend to give better results in the short period ( never more than 14 days ) of cultivation . slow growing tumours usually give disappointingly small growths , whilst normal adult tissues may fail to grow and be absorbed . in the case of the rous and duran - reynals sarcomata , the virus stimulates the mesenchymal tissue of the chorioallantois to participate in the general malignancy , thus augmenting the size of the implant . 
of more interest , however , is the observation , originally by keogh ( 1938 ) , that the rous virus also appears to stimulate the ectodermal cells of the chorioallantois to proliferate in an apparently uncontrolled manner . 
he speculates on the possibility that the virus may be carcinogenic , not only for mesenchymal tissue , but also for epithelium ectodermal proliferation due to rous virus has been under certain conditions . confirmed in the present investigation , and the pathological changes in the membrane ectoderms produced by the rous and duran - reynals tumours have been compared with those produced by dermatrophic viruses such as those of fowl - pox and contagious papillomata of cattle , also with similar changes noted in the membrane adjacent to certain implanted spontaneous tumours of the chicken . as a check on these observations a number of experiments were performed with chemically induced tumours of the mouse , rat and chicken ; also with normal adult and embryonic chicken tissues . the significance of the " cell nests " or " epithelial pearls " is interesting , resembling as they do transverse sections of infiltration cores of epithelial tissue similar lesions were noted by which characterize squamous - cell carcinoma . huxley and murray ( 1924 ) adjacent to the fragments of chick embryos implanted on the chorioallantois . it is well known that embryonic tissue extracts contain growth - promoting substances , and for this reason are frequently added to tissue culture media . claude ( 1938 ) showed that a fraction could be isolated from chick embryos which j . 
campbell possessed the same physical and chemical properties as the purified active fraction despite these similarities , however , the embryo extract of the rous i sarcoma . failed to produce tumours in susceptible chickens . in this connection it is interesting to note that earle ( 1943 ) noticed an apparent malignant transformation of mouse fibroblasts grown on a fibrin clot and bathed in horse serum and chick embryo juice . these observations , together with the production of ectodermal proliferation and cell nest formation found to be associated with so many chorioallantoic implants of tumnours in the present investigation , gave rise to the conception that tumours and embryonic tissue might contain growth - promoting substances capable of causing the overgrowth of the ectodermal layer of cells in the embryonic membrane . if this proved to be the case it might be possible to demonstrate some relationship between the intensity of the membrane reaction and the type of tumour implanted , especially from the aspect of virus content . 
no mention of " epithelial pearls " is made by keogh ( 1938 ) , or by the numerous other workers who have studied ectodermal lesions of the chorioallantoic membrane induced by viruses . a number of experiments were devised in order to test this hypothesis , and especially to study the membrane reaction to a spontaneous liver carcinoma of the duck , which is described in a separate paper . table i shows that the ectodermal lesions do not appear to be as specific as in all cases where tumours known to contain virus , or fitrates of was hoped . such turnours , or dermatrophic viruses , were placed on the membrane , proliferation of the ectoderm took place . in some instances eosinophilic " inclusions " were observed , but the nature of these is not clear , except of course in the case in the main , virus alone caused simple proliferation without the of fowl pox . formation of " cell nests . " in general those tumours which failed to grow subsequent to implantation and were absorbed did not cause any detectable lesions in the membrane ; similar results were obtained for normal adult tissues . also in several cases , although not invariably , an accidental infection of the membrane with bacteria did not result in ectodermal proliferation . the spontaneous chicken tumours which grew successfully all caused proliferation and the formation of " cell nests . " it was thought possible that chemically induced tumours , being presumably free of virus , might give a different membrane reaction . 
the majority of spontaneous tunours give disappointingly small growths . it has been shown that the capacity for indutcing ectodermal proliferation in the chorioallantois is not confined to tumour viruses , or to fowl pox and other non - tumour associated viruses , but occurs in the membranes adjacent to the majority of implanted tumours , whether spontaneous , virus associated , or chemically induced ; or even occasionally in response to bacterial growth . attention has been drawn to the tendency of the proliferating ectoderm to form " cell nests " or " epithelial pearls , " resembling those occurring in squamous - cell carcinoma , and the significance of this has been discussed . the induction has been described of two distinct leukaemic conditions in chick embryos as the result of implanting tissues from a third type of spontaneous leukaemia in a fowl , and has been briefly discussed . i wish to express my gratitude to professor a . 
murray drennan , of the pathology department , university of edinburgh , for his interest in this work , and for the numerous suggestions as to the manner of development of the investigation . all the fertile eggs were obtained from a . 
7. received for publication february 3 , 1949 . one of the surprising elements in bittner 's discovery of the " milk factor " is the apparent entry of the virus into the bodies of the young mice via the it is , however , obviousthat during suckling a small amount alimentary canal . of milk may also enter the nostrils , and that the nasal mucosa may offer an alternative port of entry . it also seems possible that the milk factor might be destroyed by digestion in the stomach . if this were so it would be difficult to recover milk factor from the stomach contents of suckling mice . 
the unfortunately the experiresult was entirely negative in the 40 mice so treated ment was not adequately controlled , in that none of the mice were tested for susceptibility by means of extracts known to contain the virus . 
cohen free , will , in this paper , be designated as ffc , and the reciprocal factor - harbouring ( c3h x cba ) f1 as fhc . all parent strain and hybrid mice were housed in the same environment and maintained on a standard laboratory chow diet with tap water ad libituit was found expedient , in view of ' the temperamental breeding habits of both cba and cm females , to isolate routinely all pregnant mice until after the weaning of consequently , no f , bybrid was ever in contact with the father , which , the litters . as has recently been shown by peacock ( 1953 ) , reduces the probability of " infection " in the ffc with milk - factor from the cm male parent . the incidence of spontaneous mammary tumours in old factor - harbouring ( c3h x stock albino ) f , females , which were observed for over a year and inadvertently force - bred , was at least 70 per cent . 
no mammary tumours were noted in the corresponding , similarly treated , factor - free females , and it was considered that the presence of the milk - factor in the c3h niale parent exerted little or no influence on this group . 
the tumour , retracted from the body onto a wax backing , is fitted into the mouth of a 2 cdiameter open - end applicator , fsd = 25 cm . , and treated at 240 w . 
the mean - log of the volume in cubic millimeters of the fhc group is 2 - 12 ( 0 - 08 ) , while the mean - log - volume for the ffc group is 1 - 85 ( 0 - 08 ) , which is significantly smaller . while unequivocal comparisons between the c3h and hybrid groups could be made with confidence , it was considered possible that , as a result of the variations in growth rate within the hybrid hosts , smaller tumours might be more readily cured , and the ffc group consequently biased in favour of a higher curerate . 
2 , togeth ' er with comparative data previously determined for the parent this design is analogous to a six - point assay , in which both hnearity strain . and parallehsm of the regression hnes can be tested . 
the magnitude of the parameters and the significance of the inter - group differences were computed by finney 's ( i 952 ) methods . a third experiment was designed to determine , whether the increased radiosensitivity of the tuniour in f , hybrids was an inherent change in the tumour cel ' is per se , or a reflection of host - resistance . 
2. - probit diagram showing response of the cm carcinoma growing in various situations . ( a ) control series treated in homozygous cm mice in 8itu . ( d ) irradiated in 8itu in heterogeneous hybrid mice . ( f ) irradiated in factor - free ( ffc ) mice . 
the increased radiosensitivity of the tumour associated with genetic diversification in the host is evident . ( e ) irradiated in factor - harbouring ( fhc ) mice . 6000 7000 5000 cells growing in a relatively alien environment was suggested by barrett and deringer 's ( 1952 ) observation that a permanent adaptive change occurred in the oh mammary carcinoma following one - sub - passage through susceptible f , hybrids . since the object of this experiment was to demonstrate any inherent acquired radiosensitivity in the tumour , a smar homoplast ( first passa - ge from a oh mouse ) , growing slowly in an ffc host , which had attained a volume of only 30mm3 . 
the donor was also re - impladted with this tumour . takes " were 100 per cent in all groups . when each tumour had reached a standard size , about i cin its greatest diameter , it was irradiated in situ with a dose of 4200 r . 
the re - implanted tumour therefore , if the in the ffc donor was also irradiated at this dose , and cured . acquired radiosensitivity was a permanent adaptive change in the tumour cells capable of being carried over into the next transplant generation , it could be expected that the cure - rate of grafts originating from this tumgur at the dose givedwould be about 75 per cent in each genetiegyroup . 
2 , and the probit regression lines derived for the radiosensitivity of the tumour growing each reciprocal group are shown . in the genetically heterozygous environment of the ffc host , excluding the complicating influence of maternal factors , is shown by line f in fig . 
2. this line is virtually parallel to that previously obtained in the parent oh strain ( line a on the diagram ) , the coefficient of variation being 10 per cent . the median effective dose ( ld50 ) is found to be 3950 ( i 10 * ) r , compared to 5700 r previously reported in the oh . 
2. not only is the cure - rate , in the presence of the milk factor , considerably less than that of the factor - free mice , thougli still greater than that of the c3h parent , but the usual sharp response to increasing dosage has become much less sensitive , as evidenced by the considerably flatter slope of the regression line . this change test of the data reveals a is not due to fortuitous fluctuations in cure - rates , as a highly significant departure from parallelism with the other groups . 
the median , effective dose for the tumour growing in fhc mice appears to be 5100 ( + 400 * ) r with the unusually large coefficient of variation of 25 per cent . it must be assumed , therefore , that the maternal influence is not uniform and stochastically independent of other factors . 
was noted in the treatment of radiation - attenuated homoplasts growing in the parent strahi ( cohen and cohen , 1954 )  . at the ld50 level , the relative radiosensitivities , evidenced by the dosage ratio between the c3h and fhc groups is 1 - 13 ( + - 07 * ) , and that between the fhc and ffc groups is 1 - 29 ( - 08 * )  . 
the former ratio , compared with its standard eiror , indicates that the genetic effect per se , in spite of the complicating matemal influence , is probably significant ( p = 0 - 05 ) ; while the latter shows that the effect attributable to the milk factor alone withift the hybrid mice is highly significant ( p < 0 - 001 )  . 
the relative importance of these ratios , however , necessarily varies with the curative level t - ested , the maternal influence having the greater effect at doses above the median effective range . in order to eliminate any possible bias introduced by the greater average volume of the tumours in the fhc mice compared with those of the ffc group , a small number of animals bearing tumours of extreme size were discarded in the manner previously described , so as to equate the mean log - volumes of the two groups , and the probit analyses repeated on the remaining matched tumours . this correction , however , does not alter the magnitude of the parameters or affect materially the significance of the differences between them . further , comparison of the proportion of tumours cured within each class - interval of fig . 
i that within each genetic subgroup , the cured tumours tend to a smaller volume than the non - cures . these differences , however , are not signific ' ant , since the experiment was not designed to test the effect of tumour volume per se on radiosensitivity and contains insufficient data for this purpose . 
the question of the relative importance of genetic factors and of tumour size per se in determining radiosensitivity , is probably meaningless , since the smaller , more slowly - growing homoplast may itself be a manifestation of genetically - conditioned host - resistance ( eichwald , 1953 )  . 
cohen mal factors , therefore , materially affect the response of a tumour homoplast irradiated in situ . subsequent challenge with a second inoculum in those hybrids of both reciprocal groups , previously cured of the tumour , resulted in active growth in all it was also interesting to note , in the course of the experiment , that the cases . spontaneous mammary tumours in factor - harbouring f , females occurred regardless of whether the animal had previously been cured or not . third experiment table 11 shows the results of the third experiment , in which a " radiosensitive homoplast , growing in an ffc and later cured with 4200 r , was sub - passaged through mice of the three genetic categories and treated with the same dose . the cure - rates of these tumours in the ffc , fhc and parent c3h mice are respectesting the null - hypothesis that the radiosensitivity tively 67 , 35 and 0 per cent . of the sub - passaged homoplasts is the same as in the ffc hosts ( 76 per cent at 4200 r , table 1 ) , the probability of obtaining the results observed is shown in the last column of table ii . 
the susceptibility to tumour transplantation is a simple genetic - dominant , shown by the uniformly successful transfer of tlle inbred parent strain tumour to all f , hybrids . however , once such a graft is established , its rate of growth is no longer contingent on host genetics per se , but is dependent on the aternal extrachromosomal influence which , when present , exerts a significantl accelerating effect . likewise , a matemal influence , presumably the milk agent , is sufficient to induce spontaneous mammary tumours in f , hybrid females , the incidence approaching that in the inbred parent strain , in spite of genetic dilution . it has here been shown that the radiosensitivity of a tumour transplant , in this case the c3h mammary adencarcinoma , is dependent on both genetic and maternal ( extrachromosomal ) factors in the hybrid host . it appears , however , that the two factors are not necessarily independent . in the case of the factor - free f1 hybrid , a uniform and uncomphcated response is elicited which seems to be a - clear expression of immunogenetic differences between host and tumour . 
the differences between these groups are significant , although all three groups of mice were uniformly susceptible to the tumour and showed no overt manifestations of resistance . it appears , therefore , that the radiosensitivity of a tumour is a quantitative measure of subhminal host - resistance resulting from immunogenetic differences in the host - tumour relationship , including extrachromosomal factors . the mechanisni involved was further elucidated when a tumour growing in a factor - free f , hybrid , and known to be curable with 4200 r , was sub - passaged to mice of the three genetic groups . 
the homoplasts responded to treatment in the same manne ' r as the directly passaged parent strain tumour in the corresponding hosts , indicating that no inherent radiosensitisation of the tumour cells per se had occurred . all the facilities required for the maintenance of the animals used in this investigation were generously provided at the south african institute for medical 312 a . 
3. received for publication february 6 , 1947 . it has frequently been noted by the early investigators of tumour pathology that besides a high mitotic rate , tumour cells may also show great variation in the details of mitosis ( pianese , 1896 ; hansemann , 1904 )  . 
the abnormalities may concern the behaviour of the chromosomes or the cytoplasm or both , and most of them lead to degeneration and death of the cells . this is largely due to the deficient nuclei which usually result from abnormal mitosis . 
by repeated chromosome multiplication within the nuclear membrane ( biesele , poyner and painter , 1942 ; koller , 1943c )  . polyploid cells are frequent in tumour regions where .cell breakdown is in progress on a large scale . 
x - rays induce stickiness of chromosomes in plants and animals ( markquand , 1938 ; koller , 1943a ; darlington and la cour , 1945 )  . temperature changes and chemical treatment can lead to similar abnormalities ( barber and callan , 1943 ; ostergren , 1944b ) , and complete suppression of the spindle is brought about by low temperature and by specific compounds , such as colchicine . polyploid , binucleate and multinucleate cells , owing to their chromosome balance , survive and may undergo mitosis . their rate of mitosis , however , is always less than that of cells with a normal chromosome number . 
koller until recently it was believed that a nucleus with the diploid chromosome number was necessary for normal cell behaviour , and that cells with a deficient complement could function only under very specific conditions , the life of such cells always being short ( darlington , 1942 )  . 
the adenocarcinoma here described presents an example in which cells with less than the normal number of chromoit is not out of place to somes are still able to divide and to continue dividing . draw attention to recent literature on cytoplasmic control in micro - organisms ( sonneborn , 1943 ; spiegelman and kamen , 1946 ) , the relevance of which , for the origin of cancer , has been dealt with by many authors ( graffi , 1939 , 1940a , b ; darlington , 1944 ; haddow , 1944 ; potter , 1945 ; woods and du buy , 1945 , 1946 ) , who suggest that the permanent change which renders a cell malignant takes place in the cytoplasm . cell behaviour in this adenocarcinoma is a further indication that the nucleus can be so subordinated , and the cell remain active in spite of its deficient nucleus . u0 ' c unromosome numoer fig . 
i presents the absolute number of deatlis from lung cancer in norway in order to avoid the disturbance in comparability introfrom 1929 to 1952 . duced by the 1948 classification , the figures for 1951 and 1952 have been adjusted , according to the analysis of julie e . 
backer , head of the medical statistics division of " statistisk sentralby - rh , " so that they very approximately represent the figures that would have been found in group 47b , if the coding had taken place according to the 1938 classification . 
1 , showing the gradual and pararel rise ' lung cancer in both sexes up to the middle of the 1940 's , however , with a shght lead of the males . 
2 lead , h ' owever , to a more accurate pictureof the registered increase . in males this ' mcfease is from 0 - 11 per 10 , 000 living in 1930 to 0 - 77 in 1950 . 
figures for 1930 a - re given as the mean value of the and 0 - 34 in 1950 . instead of a tenfold increase in males we find a sevenfold , and years 1929 - 1931 . instead of a sixfold increase in females , w - e find a four - and - a - half - fold . in a recent paper kreyberg ( 1954 ) has described 466 primary epithehal lung tumours and typed the tumours in six main types , according to criteria previously stated ( kreyberg , 1952 )  . 
kreyberg these tumours are designated group i tumours . series ( christiansen ( 1953 ) , 134 cases , and jakobsen ( 1953 ) , 100 cases ) , as well as the authors own clinical material , embracing 232 cases . the examination of the histological types , as well as the sex and age occurrence , in the light of our present clinical and epidemiological kiiowledge lead to the following conclusions : ( i ) squamous cell , large - cefl and small - cell carcinomas represent a biological entity . these tumotirs occur with a very marked preponderance in males and they show an age - curve indicating that in the so - called western world potent carcinogenic factors of recent origin are of aetiologic signi ( ii ) adenocarcinomas ficance . occur in norway with the same frequedcyin males and females , and this tumour shows a steadily increasing occurrence with advancing years , indicating a stable and moderate carcinogenic influence . ( iii ) bronchiolar cell carcinomas are likewise evenly distributed among males and females , but there is no increase in the higher age - groups . 
udknown factors hitting at random are supposed responsible ( iv ) lung adenomas and salivary gland tumours of the for their development . lungs sbow an equal sex distribution and occur in all ages . these facts , together with the histological picture point in the direction of developmental factors being responsible for their occurrence . these last four tumour types have been , designated group 11 tuniours . if the three norwegian materials are examined and christiansen 's ( 1953 ) series is divided into two sub - series , according to two different time periods , we get the figures as shown in table ii . 
the consequence of this assumption should again be that an increase registered for group ii tumours would represent a measure of an increase in diagnostic efficacy . as regards the group i tumours , table ii again clearly reveals interesting in the four time periods , tfie two middle partly overlapping , one may facts . observe that females , in accord with clinical experience , constantly present a small number of group i tumours . 
no conclusion in the opposite direction is drawn from the rather declining frequency because of the smafl figures . it may therefore be correct to regard the lung cancer in females to - dav as an expression of what clemmesen , nielsen and jensen ( 1953 ) call " unavoidable lung cancer . this unavoidable lung cancer should include ar the group ii tumours , as well as a smar number of group i tumours . if these assumptions are correct , the increase in lung cancer in females should at least in norway today , be a fair index of the increased diagnostic efficacy . the twenty years ' period 1930 - 1950 this increase is approximately four - and - a - halffold . 
we have , however , probably not yet reached the limitation of our diagnostic although better diagnosis may in some cases lead to the discovery expansion . of a primary site outside the lung , and thereby exercise a depressive effect on the lung cancer mortahty registered , it seems more hkely that further improvements at the present time will mainly result in an increase in the mortahty figures . 
we ought , therefore , to accept even a furtlier increase in the lung cancer mortahty registered in females , without necessarily drawing the conclusion that more lung cancer is actually developing . 
from that period a marked increase in grou ' p i tumours can be observed in males , at the same time as a pronounced deviation in the mortality rates in the two sexes takes place . it seems that the marked additional rise in lung tumours in males is caused solely by the group i tumours . 
the group 11 tumours , on the other hand , closely follow the pattem it may be that in the latest series ( kreyberg 's ) in table ii , the of the females . difference between the group i and ii tumours is too marked to be whory representative , because that material is a clinical one with an underrepresentation of older people liable to develop adenocarcinomas . 
the tendency is clear , however , and the development continues to - day . at present it seems permissible to conclude that in norway , during the twenty years ' period 1930 - 1950 , the four - and - a - half - fold increase registered in lung cancer in females is entirely caused by greater diagnostic efficacy . 
as the development in males initiary closely followed that of the females , it seems reasonable to accept the recent deviation in the mortality rates , as well as in the representation of the histological types , as indicating a new situation , and to regard the added increase in lung cancer in males as an expression of a real increase . this should mean the difference between a sevenfold and a four - and - a - half - fold increase . the importance of this conclusion is not expressed by the magnitude of the real rise to - day , but it is indicated by the tendency and the sliort time it has been manifest . 
1. - lung cancer in denmark , 1931 - 1945 . 1931 33 35 crude mortality rate per 100 , 000 in males 43 45 39 41 alterations in the age distribution of the population might be suggested as the cause of the rise in crude mortality from lung cancer , but if we compute the mortality rate according to age in the capital for periods of five years , and on the base of quinquennial age groups of dead and living persons , as in fig . 
2 , we find no confirmation of the suggestion mentioned . thus , we have found a very steep increase of mortality from lung cancer within a limited area , well furnished with modern medical facilities , available to all social classes . * the increase is found among both sexes , but is far more pronounced for males than for females , and it will be worth while further to analyse the population in question with regard to the incidence of lung cancer , as copenhagen seems to provide a good example of the changes in the mortality from lung cancer found elsewhere in europe . the central tuberculosis station of the city of copenhagen provides excellent opportunities for checking up the reliability of statistics given in the first part in its work to trace tuberculous infections in patients of the present paper . suffering from all sorts of respiratory diseases , this institution performs numerous thorough examinations on such patients referred from general practitioners . annual reports contain tables giving the number of patients , subdivided in decennial age groups for each sex separately . 
the group examinations under * for members of the public health insurance , which comprise 85 - 90 per cent of the danish population , no fees are charged in the municipal hospitals of copenhagen . 
3 , shows no steady rise , and hardly any irregularity is found in the curve for females , which , however , comprises very few individuals , as seen from the absolute figures . the very steep rise of the male curve about 1941 may have been caused by the fact that the efficiency of a central tuberculosis station may also have increased if the duration of the disease is one or two years in a disease like lung cancer . from its earliest possible detection to death , and this is , in fact , the opinion of the tuberculosis station , the steep rise in 1941 given in fig . 
even if we allow for the small absolute values of the figures , it can be said , as with regard to the corresponding mortality figures , that there is no increase of morbidity in the young , as would be expected if the inerease was due to an increase in the inhalation of tobacco smoke , if we are not to assume a latent period for lung cancer of about two decades . in our opinion the figures given illustrate that even a pronounced increase of the crude mortality rate for lung cancer among males , and almost only among males , does not necessarily mean an increase in incidence of that disease . presumably the more frequent detection of the disease is due to improvement of 2s~~~~~~~~~~~~~ __ _ 120 ___ __ 80 __ f - ~i 40 ' j years fig . 
if the results from copenhagen can be generalized , it seems that the apparent increase in lung cancer mortality is , to a very large extent , conditioned by improvements in diagnostic means , and it can be expected to continue until the sex ratio amounts to about 8 males to 1 female . our thanks are due to knud winge , m.d. , the chief physician of the central tuberculosis station , copenhagen , for permitting us to use the material of the station , and for his kind interest in our work , and to kontorchef miss m . 
 the compilation of this paper was prompted by the idea that some investi gators of cancer as it occurs in man do not know the valuable material which is contained in the publications of the general register office , while even those who are acquainted with this literature may find some use for a list of the collec tions of data about cancer which it contains . 
 the material dealt with in these publications consists of the death certificates from england and wales , considered in association with the data on population , civil state , occupation and locality obtained at the census of 1911 , 1921 and 1931 , together with population estimates for intervening and subsequent years . 
the certificate does not state , and is not intended to state , how long the deceased had followed the occupation named , and had lived at the home address given ; this information could be obtained only by inquiry into individual cases . 
the sources of such errors have been discussed in two earlier papers ( henry , kenna way and kenna way , 1931 ; ~eimaway and kennaway , 1936 )  . 
 the _decennial supplements for 1921 and 1931 contain data collected at the census of those years , and were published in 1927 and 1938 respectively ( registrar general , 1927 , 1938 )  . 
_they contain a large amount of tabulated material for periods adjacent to the census , namely 1921 - 23 and 1930 - 32 ; the scope of those tables , in so far as they are concerned with cancer , is summarized in tables i and ii . 
the 240 , 726 deaths of all married women during 1930 - 32 were classified according to the husband 's occupation as stated on the death certificate , while 19 , 422 single women who died during the same period were classified according to their own occupations . 
the reasons for the association of the married woman with the occupation of her husband are that ( 1 ) " only about 10 per cent of married women were recorded as gainfully occupied at the census of 1931 , " and ( 2 ) some indication is obtained of the social , or occupational , nature of the mortality in the husbands ' occupation , "  . 
table ix shows a selection from the supplements for 1921 and 1931 of some very interesting - data for the incidence of cancer of various organs upon men and married women of the five social classes , and in the case of the men two periods ( 1921 - 23 and 1930 - 32 ) can be compared . 
a recent paper by swan ston ( 1950 ) on " the iron and steel industry " shows the use which can be made of the material in the decennial supplements . 
 the registrar - general publishes annually a " statistical review of england and wales for the year  . , " normally in two parts , namely , ( 1 ) text , ( 2 ) tables . 
the " text " now contains a section upon cancer consisting of a commentary upon the data which have been obtained during the year in question , and certain tables . 
this table provides material in answer to the question so often asked - " is cancer increasing ? " the comparative mortality index , which takes account of changes in the sex and age structure of the population , shows that the total mortality from cancer in england and wales has barely increased during the past twenty years . 
the distinction between the entry of " carcinoma " and " cancer " upon death certificates is probably of no value , but the separation of the two at any rate absolves the general register office from any responsibility for the distinction ( table lxxvi )  . 
 ( e ) by regions ( england and wales , greater london , rest of south - east , north , midland , east , south - west , wales ) , and by class of area ( county boroughs , other urban districts , rural districts ) ( table lxxvii )  . 
 such data for the total incidence of cancer must , of couj1se , be recorded , calculated and examined , but they cannot show the peculiar incidence of cancer upon the various organs , and in the two sexes , and in persons living in different areas , and various interesting changes may cancel one another and hence be lost in the totals . 
the great interest of these data is best made plain here by reproduction in table iii of a part of an example ( table lxxviiia , 1940 - 42 )  . 
 all sites lips tongue mouth tonsil pharynx jaw others total oesophagus stomach duodenum other small intestine caecum hepatic flexure , splenic flexure sigmoid flexure large intestine ( colon ) other and undefined intestine rectum ( not anus ) liver gall bladder and ducts pancreas peritoneum , mesentery , others other and unspecified digestive organs 89 , 902 606 2 , 254 703 534 1 , 008 748 529 6 , 382 4 , 498 20 , 778 129 155 860 418 2 , 157 8 , 801 228 10 , 365 2 , 581 703 3 , 267 4 , 053 147 232 199 250 females . 
 other female genital organs total total total total total breast scrotum prostate testis penis others kidney bladder , urethra , ureter : 163 155 6 , 055 339 457 7 , 009 409 3 , 360 3 , 769 147 174 606 623 593 667 219 312 755 2 , 877 202 3 , 834 5 , 482 721 6 , 416 12 , 619 4 , 952 1 , 281 6 , 248 20 , 049 107 184 173 183 107 265 386 162 510 705 499 550 1 , 114 312 1 , 557 1 , 869 452 458 185 the material contained in this table is very significant . 
the cancer problem in its simplest form is reduced to the question , why does a cell divide ? but no single universal " cause of cancer , " such as is announced from time to time , could , even if it were actually discovered , explain all the features of this table . 
the nature of cancer proceeds by means of the most refined cytological methods , there is scope for investigation of factors occurring in everyday life which may explain the 1rery peculiar sexand organ distribution of cancer . 
 breast total cancers of female reproduc tive organs other organs total cancers in females males exce811 in females 18 , 867 20 , 049 38 , 916 58 , 090 97 , 006 89 , 902 7 , 104 164 e . 
kennaway for instance ( table iv ) , the total deaths from carcinoma in males ( 89 , 902 ) and females ( 97 , 006 ) show a difference of only about 7 per cent , yet the latter total includes 38 , 916 deaths , or 40 .per cent of the whole , from carcinoma of organs peculiar to the female , among which organs the female breast , being capable o , f lactation , must for the present purpose be reckoned . 
this calculation illustrates the phenomenon of the " amount " of cancer in man , to which attention was drawn in an earlier paper ( kennaway and kennaway , 1937 )  . 
no better example has been given by later workers than that recorded by the dutch investigators snijders and straub ( 1924 ) in sumatra , who first described this numerical relation of total cancers in populations differing in habitat or in sex ( table v )  . 
 28 27 these figures show that in sumatran and european populations , in which the total incidence of cancer is about the same , the proportion of one form of cancer , in this case that of the liver , may be very different . 
 " there appears to be a general law that when in a given population the incidence of cancer in one particular organ is markedly increased as compared with another population , there is then a compensating decrease in the incidence of cancer in a number of the other organs " ( cramer , 1936 )  . 
 ( b ) the data shown in table lxxviiia and bare subdivided under 15 quin quennial or decennial age - groups from 0 - 5 to 85years ( tables lxxixa , b , e , d , e , f )  . 
thus in men aged 55 - 64 the mortality from cancer of the lip has fallen to 26 per cent of the initial figure , while that attributed to cancer of the lung has increased by more than 17 times . 
 1911 - 20 1921 - 30 1931 - 35 1936 - - 39 1940 - 44 1945 1911 - 20 1921 - 30 1931 - 35 1936 - - 39 1940 - 44 1945 1911 - 20 1921 - 30 1931 - 35 1936 - - 39 1940 - 44 1945 the exact comparison of the prevalence of cancer , or of any form of cancer , at different periods , requires standardized death rates owing to the continual increase in the numbers of older persons , who are of " cancer age . " such data are given at intervals in the statistical reviews ( text ) , and most recently in table lix in the review for 1938 and 1939 ( registrar - general , statistical review ) , which records the standardized rates per million population for cancer of 27 sites in men and women separately in the periods 1901 - 10 , 1911 - 20 , 19.21 - 30 , 1931 - 35 , 1936 , 1937 , 1938 and 1939 . 
these figures for each one of the four most recent years are of especial interest because they show the present state of increase or decrease of the various forms of cancer . 
 in the table in question the great majority of the 52 sex - site combinations show a decrease , or are stationary ; the only quite definite increase is in cahcer of the lung and bronchus in both sexes . 
since 1942 standardized death rates have been superseded by comparative mortality indices , which compare the death rate in each year with that of 1938 , after making allowance for changes in the proportion of the population at different ages . 
for a number of sites of cancer since 1933 have been published in the medical tables volume of the statistical review ( table viii ) for each year since 1942 . 
 ( d ) the deaths from cancer of certain sites ( mouth and oesophagus , stomach and duodenum , respiratory system , breast , uterus , other sites ) per 1000 for all sites in men and women at certain ages , in certain regions and classes of areas named above ( table lxxvii ) during 1940 - - : - 42 and 1943 - 45 ( table lxxxi ) are set forth . 
 the cancers of the respiratory system show the greater liability of urban populations ( stocks , 1936 ) ; this portion of the tabl~ is of such interest that it may be reproduced in extenso here ( table vii , section a )  . 
if one recalculates the figures for the various districts on the basis that " rural districts " = 100 , whereby the data for the two periods 1940 - 42 and 1943 - 45 become more comparable , one obtains the figures shown in section b of the above table , which show a very close similarity between the two series for women , with the single exception of the figures for the south - west region . 
of course this result has no bearing on the accuracy of death certificates , but it does show that two sets of such certificates , gathered in a number of districts during two consecutive periods , give results which have a considerable uniformity . 
 when the mortality from any form of cancer , such as that of the lung , is higher in urban than in rural districts , one must consider whether the difference is due , not to the conditions of life in towns , but to better facilities for diagnosis , and a further extract from table lxxxi is of interest in this respect ( table viii )  . 
 males , 45 - 65 mouth and oesophagus , 1940 - 42 1943 - 45 stomach and duodenum 1940 - 42 1943 - 45 males , all agesrespiratory system females , 45 - 65 breast uterus 1940 - 42 1943 - 45 1940 - 42 1943 - 45 1940 - 42 1943 - 45 238 225 156 183 236 231 165 157 205 187 216 249 261 254 150 137 100 254 235 103 126 236 244 148 144 the diagnosis of cancer of the oesophagus , stomach and duodenum , breast and uterus may be by no means easy , yet these forms of cancer do not show the difference seen in cancer of the respiratory syste this last must be made up largely of cancer of the lung , and hence these data provide further evidence of a carcinogenic factor in urban environment . 
 the annual statistical reviews do not deal with the social and occupational incidence of cancer , as the occupational distribution of the population is ascer tained only at census periods . 
 in this summary of the annual and decennial publications of the general register office in relation to cancer one cannot of course refer to the numerous passages which treat of the material tabulated . 
 the decennial supplement for 1921 ( registrar - general , 1927 ) contains the first detailed study of the social incidence of cancer upon the various organs in men , which study developed from an earlier investigation of the incidence of cancer as a whole ( stevenson , 1923 )  . 
so far as is possible from the material available , class i purports to represent the pro fessional and generally well - to - do section of the population , class iii , skilled artisans and analogous workers , and class v , labourers and other unskilled callings , while classes ii and iv are intermediate , comprising occupations of mixed types , or types not easily assignable to the classes on either side . " the parts of the body affected by cancer were divided into two classes , namely : exposed sites ( buccal cavity , pharynx , oesophagus , stomach , larynx , skin ) , and other sites . 
 the mortality from cancer of the exposed sites increases from social class i to class v , while cancer of the other sites shows no such relationship ( table ix )  . 
 the author of the decennial supplement , 1921 , comments upon these data : " it thus appears that a large proportion , at least , of cancer mortality is of a highly preventable nature , for we must suppose that if the conditions of life of all sections of society could be assimilated to those of its upper ranks , mortality from cancer of the exposed sites would fall for all classes to the class i level . 
 the paragraph made up by these two sentences should be regarded as one of the classics of cancer research , for it brings carcinogenesis in man into relation with factors in everyday life which can be investigated , while the most refined methods of physics and chemistry are applied to the problem of cancer in general . 
 the most extreme instance of a social factor in the incidence of cancer appears in the case of cancer of the scrotum ( kennaway and kennaway , 1946 ) , which could in all probability be eliminated altogether by cleanllness , as is cancer of the penis by circumcision in infancy . 
 the figures ( table ix ) for cancer of the upper alimentary canal in males show a significant reduction in the steepness of the social gradient from 58 , 80 , 99 , 102 , 140 , to 63 , 80 , 97 , 109 , 129 ten years later . 
this may be due in part to " earlier or more effective treatment than before of cancer of the more accessible sites " in men of the poorer classes , as is suggested in the text , but probably also to the improvement of social conditions in other ways . 
the change has been chiefly in the cancers of the buccal cavity ( tongue , tonsil , pharynx ) , for cancer of the oesophagus shows no , and that of the stomach very little , loss of gradient . 
 the steeply graded figures for the larynx , in contrast to those of the buccal cavity , show no change , while those for cancer of the skin show a flattening which one would associate with improved personal cleanliness . 
 figures for the socia ] distribution of cancer in women in 1921 - 23 are not available , but the comparisons of those for men , and women , in 1930 - 32 are 170 e . 
 " of gastric cancer mortality can have little to do with the effects of occupation , and must arise from factors of selection , economics or environment which affect the wives of the men in occupational groups as much as they affect the men themselves . " cancer of the skin also affects men , and married women , of the the employment of a different social classes in much the same way ; "  . 
 proportion , largest no doubt in classes iv and v of married women in textile occupations , may be partly responsible for the mortality gradient for skin cancer . " no attempt is made here to deal with all the indications for inquiry which may be drawn from this table ; the subject is dealt with , and illustrated by graphs , in pp . 
cancers of the buccal cavity , and of the larynx , show a high incidence upon occupations associated with alcohol ( kennaway and kennaway , 1936 ; wassink , 1930 ; registrar - general , 1927 , appendix d ) ; the change in gradient in the former only might suggest that this is due to another factor , namely , better oral hygiene . 
 the lack of influence of social class upon the liability to cancer of the lung , together with the very considerable effect of urban conditions ( stocks , 1936 ; registrar - general , 1947 , table vii ) , suggasts some carcinogenic factor to which all classes are exposed ; owing to the mixing action of the wind there is less difference in the outdoor air breathed by different classes than in other social conditions such 1 , 1 , s food and cleanliness ( kennaway and kennawa.y , 1947 ) , and all classes seem to share in the increased use of tobacco , largely in the form of cigarettes . 
 a good example of the unique value of such studies of social distribution is given by cancer of the uterus , which was examined in this way for the first time in 1930 - 32 . 
thus , at ages 35 - 65 the rate in married women of class v is twice that of class i , and single women in classes iv - v show a mortality 44 per cent greater than that of classes i and ii . 
 thus in 1921 the ratio of registered to 100 calculated births for married males in the five social classes was 85 , 85 , 97 , 109 , 128 , and the social distribution of uterine cancer in married women might be thought to be due to the difference in fertility . 
 the data on the mortality from cancer in the last twenty years should yield very valuable information when correlated with the results of the census in 1951 , the first made since 1931 , in view of the considerable social changes which have taken place . 
 ( 1 ) the british empire cancer campaign has published in its 13th annual report a very elaborate study by stocks ( 1936 ) , il1ustrated by 17 maps , of the distribution of cancer of eight sites ( oesophagus ; stomach ; intestines ; rectum ; liver , gall - bladder and pancreas ; skin ; lung ; breast ) in both sexes at various ages in the counties and county boroughs of england and wales . 
the 14th report of the campaign records an extension of this study ( stocks , 1937 ) , with 7 maps , to cancer of other sites ( tongue , mouth , jaw , larynx , bladder , prostate ) , and a final section ( stocks , 1939 ) , with 9 maps , deals with cancer of the uterus , vagina , ovaries and fallopian tubes , and of the skin , lung , rectum and bones in women . 
 no such study of cancer in relation to this , or any other , geographical area has ever been made , and no summary is attempted here of the results and suggestions for research which it contains . 
 ( 2 ) the changes in mortality from cancer of various organs in england and wales between 1911 and 1944 are described in a paper by stocks and mackay ( 1946 )  . 
 ( 3 ) the general register office has published a study by stocks ( registrar general , 1947 ) of cancer of the stomach , oesophagus , lung , larynx , breast , uterus , ovary and some other sites in relation to a number of localities and environmental factors ( urban and rural districts , counties , the 13 , largest cities in england , 30 large towns , metropolitan boroughs of london , social indices , number of persons per room , amount of sunshine , source of water supply ) during one or other or both of two periods , 1921 - 30 and 1940 - 44 . 
one may mention here two results which provide valuable indications for further research , namely ( a ) an inverse relationship between number of sunshine hours and deaths from cancer of the lung , and ( b ) a high incidence of cancer of the stomach in the northern and central counties of wales , especially in the former . 
the author says : " the purpose of this report is to present the statistical facts , and point out any peculiarities in distribution and correspondences with other measurable factors which appear , so that all possible clues may be followed up by further study . 
 a list has been compiled of the types of information about cancer in man in england and wales which are to be found in the publications of the general register office . 
peacock. froni the research department , glavotr royal cancer hospital . received for publication april 6 , 1949 . it is a remark - able fact that while carcinogenic hydrocarbons readily , induce sarcoma in the connective tissues of fowls , the same agents have not vet been shown to induce epithehal tumours in this species . indeed until recentlv all attempts to induce epithelial tumours in fowls by any means seem to have f.iled. recently gottschalk ( 1948 ) mentioned iin uccessful attempts to induce hepatoma in 89 fowls fed with " massive " doses of p - dimethylaminoazobenzene ( da - ab ) , and maintained for over a year on a diet deficient in protein and riboflavine or enriched with biothe also quoted similar iin uccessu attempts to induce hepatoma with butter yerow by kinosita ( i940 ) , and other failures to induce epithelial tumours in general with various carcinogens . 
one case of hepatoma was observed by ober , guerin and boic ( 1933 ) in a bird inoculated 9 months previously with a mtrate of 3fill hill 2 endothelioma . this hepatoma was not transmissible , but birds grafted with fragments of hepatoma developed leucosis which was transmissible . 
the aetiolo&y of this hepatoma therefore is uncertain.induced epithehal tumours were amongst the teratomas obtained by michalowsky ( i 929 ) following the injection of 5 per cent zinc chloride into the testicles of cocks . duran - reynals ( 1946 ) , while trying to transmit primitive renal tumours in fowls , obtained sarcomas but no epithelial tumours in the inoculated birds . it may be that other workers have made extensive negative tests without them , but it seenis advisable to describe our ow - n mainlv negative recor attempts , which have now extended over a period of about 17 years , and have 3ielded only two carcinomas , apparently caused by 2 - acetylaminofluorene ( 2 - a - a - f )  . in contrast with these negative results , bielchowsky and green ( i945 ) obtained an anaplastic renal carcinoma in i of 5 rhode island red cocks maintained on a mixed diet to which was added 2aaf , at the rate of 3 - 30 mg . 
149 , previously recorded as bearing a tumour , was found to have a necrobiotic lesion in the region of the eneysted tar and a large haematoma in the breast muscle , but no sarcoma . ( 2 ) twenty - seven bpr fowls ' were painted on the right side of the comb witli tar and injected in the right breast muscle with the same sample of tar . while these experiments were running the first recognition of a pure hydrocarbon , 1 : 2 : 5 : 6 - dibenzanthracene ( db ) , as a carcinogen was reported by kennaway and hieger ( i 930 ) , and thereafter when the substance became available these birds were painted with a saturated solution of db in chloroform instead of tar . in view of the lack of obvious reaction to the previous tar painting , light cautery of the comb with a hot platinum wire was applied to survivors immediately before painting with db . 
pellet of 3 : 4 : 5 : 6dibenzearbazole ( dbc ) implanted into the right preening gland , followed by twice - weekly painting of the preening gland area with 0 - 1 per cent solution of croton oil in acetone . 
no tumours occurred in other birds in this experiment . ( 8 ) in preliminary experiments , 7 bl fowls were injected into the preeiiing gland with solutions of dmb in arachis oil . 
the fluorescent solution was expelled through the duct of the preening gland and , as there was no evidence of retention in the gland cavity after a few days , this type of experiment was abandoned . implants into the preening glands . tllree groups of 6 bl hens had the following pellets iniplanted into the left preening gland : 15 - 30 mg . 
the other birds had ar been implanted with similar perets of methylcholanthrene , n : n - dimethylami ioswbene , or 1 : 2 : 5 : 6 - dibenzanthracene into the right preening gland , without obvious effect . of the remaining 6 survivors after 17 months , 2 had palpable nodules in the wah of the crop . 
one of these , a bl hen , was kffled because it was rapidly losing weight and was found to have several ulcers in the crop varying in diameter from about i to 8 mm . , and partly covered by tenaceous slough . there were also numerous oily cysts in the connective tissues around the crop and in the muscular and submucous tissues of the crop itself representing renmant - 8 of previous injections of 2aaf in arachis oil . 
the re ndaer of the alimentarv tract was thoroughly examined but no other lesions were found . the hver and spleen were smafl and paler than normal but showed no locahzed lesions . 
the ovary was in a resting stage and the oviduct was involuted . sections of the ulcers in the crop show that it was the seat of at least 3 apparently separate squamous carcinomass . 
the low incidence of carcinoma in fowls n - iight be explained on these grounds . on the other hand , mammals differ in their susceptibility to the actioli of carcinogens . 
a case of keratinizing squamous carcinoma of the buccal mucosa in a fowl was described and well ifustrated bv puente - duany ( 1932 )  . the orilv case of spontaneous squamous carcinoma se ' en by us in over 3000 post - mortem examinations of fowls , over a period of 20 years , occurred in a bpr fowl that had been unsuccessfully graftedwith fragments firom a chemicauyinduced sarcoma . 
the absence of sebaceous follicles in fowls and the concentration of the sebaceous glands in the paired preening gland prompted us to implant potent carcinogens into the cavity of these glands . 
campbell. from the poultry research centre at the university of edinburgh and from the royal ( dick ) veterinary college , edinburgh . received for publication february 17 , 1949 . in july , 1944 , during the course of a long - term investigation into avian neoplastic disease , a post - mortem examination of a duck showed it to have multiple liver tumours . unfortunately , this case was not seen personally and no record was kept of any details apart from the sex of the subject - a female . however , material was taken for histological examination and a diagnosis was later made of liver - cell carcinoma . primary cancer of the liver is known to occur in chickens , but is relatively uncommon . 
two of these sources provided 3 cases each , a third provided 4 cases ( one of which was not seen personally ) , and a fourth flock provided 8 cases from a flock of 12 ducks . 
one of the latter cases ( case 17 ) had 2 different simultaneous neoplastic conditions , namely a large thoracic histiocytic - sarcoma of undetermined origin , and a much smaller hepatoma . prior to the first observed case in 1944 a total of 21 ducks had been examined in 4 years , and no case of neoplastic disease was encountered . 
no information was obtained regarding the 2 rema several birds suffering from this condition have been examined alive , and in the later stages of the disease the symptoms are very characteristic . there is usuary a history of loss of appetite and of lethargy . 
as the disease progresses , general weakness brings about the loss of locomotory power , and death superv - enes either suddenly from an internal haemorrhage , or slowly from cachexia and exhaustion . if examined during this late stage , a dropsical condition of the abdomen is apparent , and careful palpation shows the prewnee of an enlarged nodular liver projecting wer beyond the caudal extremity of the stemum on the floor of the abdomen . 
usuary one lobe is mainly involved , but there is no definite predilection for right or left ical caw , the fiver tumours are nodular and bright green in colour lobe . 
ina and covered with a tense glistening membrane containing ramifying vessels . other tumours may take the form of firm , cream - coloured nodules , probably reprewnting more recent growths not yet stained with bile . haemorrhagic or necrotic nodules are not uncommon . 
these trabeculae may merge towards the centre of the tumourous lobe to form a broad , well - defined " tnmk " from which the trabeculae radiate outwards like branches wig . 
the liver cells forming these structur ' es - are cuboidal , columnar , or polyhydral with a faintly granular eosinophilic cytoplasm ; they contain a rather small , well defined nucleus , 3 - 4 [ l . 
the nuclei of those cells forming tubules are often situated ceiitrally or adjacent to the lumen . there may be attempts at the formation of a central vein and the cells immediately apposed to the endothelium are connective tissue divides the tumour into irregular usually bolumnar in form . lobules and contains numerous aberrant bile ducts . at the other extreme is the anaplastic type , which is characterized by an almost complete loss of differentiation towards a glandular structure . 
the cells are large and polymorphic with vesicular nuclei varying greatly in size and shape , some exhibiting hyper - chromatisand containing i to as many as 10 typical measurements for such cells are , prominent eosinophilic nucleoli . nucleus 13 - 6 [ l . 
the cells are fi - equently columnar and in such cases the nuclei are usuary situated mitotic figures are common and the proximary , or remote from the lumen . rumour appears to grow mainly by infiltration . 
24 hours old filtrate prepared by grinding up liver tumour tissue in a glass homogenizer , centrifuging , and filtering , using a seitz type filter and ford 's grade g.s. 
a liver fragment and some of the sahne in which it was minced , were placed into broth which - on the fohowing day was found t - o be sterile . on the 20th of the month 2 embrvos were found to be dead . 
of the 5 , 4 had small growths in the membrane - disappointingly smafl considering the cultivation period ( 12 days )  . three of these were removed , dissected awav from the membranes and reimplanted into two ' - d - day - old embrvonated eggs . 
fragments of tissue were immediately implanted into eggs , 4 containing 101 - dav - old embrvos , and i being 9 davs . the eggs were opened 9 davs later ; 4 contained tumours . 
the eggs containing the second passage implants were opened 10 davs later , and 3 contained small tumours between 2 - 3 mdiameter . later a further biopsy on case 20 provided material to implant into three 8 - dav embrvonated eggs . 
the bird was then 8 months old . fourteen we ' eks later it was observed to be weak , losing weight , and to have an enlarged abdomen . it was destroyed and examination showed a large liver tumour weig ' hing 280 g . 
the original tumour was from duck case 18 . on the 3rd day i chicken was found in a dying condition and was kired . the pectoral muscle contained a smar greenish - brown growth which was taken for this was approximately 66 hours subsequent to injection . 
10 shows the same tumour - bearing membrane photographed aaainst a white background , and the lesions are then barely perceptible . upon histological examination , an interesting picture is revealed . 
yolk - sac cultivation did not give satisfact - ory results , this also being the experience of twombly and meisel ( 1946 ) ; although taylor , thacker and p nini ( 1942 ) , and several other workers claimed a high perentage of intraviteuine growths with the particular tumours these were mainly mouse and rat mam iary carcinomata , and the poor used . results obtained by others , using different tumours , seems to indicate that the environ.ment provided by the chick embryo yolk - sac is pecuharly suitable for the metabolic requirements of mam lary cancer cells . on the other hand , most of the tumours implanted on the chorioallantois 208 j . 
the sudden occurrence of a number of cases of hitherto unrecorded primary carcinoma of the duck 's liver provided material for cultivation by various methods , with the main object of searching for a transmissible factor or virus . 
the chorioallantoic method of cultivation , therefore , seemed particularly suitable , and was extensively used . there appear to be two possible explanations of the etiology of this condition . firstly , the disease might be associated with a transmissible factor . 
 ' it is known that the mouse mammary cancer factor of bittner is transmitted from mother to offspring by the milk , and this is one of the very few known instances of a tumour of epithelial nature associated with a virus - like principle . it was felt that the duck liver carcinoma might also contain a factor transmissible probably via the egg , which might be capable of propagation in the same manner as the milk factor of mice . experiments designecl to test this theory , however , have given negative results as far as transmission by cell - free material is concerned . 
but the sui - vival of these heterologous grafts for at le - ast 6 davs in the muscle and peritoneum of chick - ens is rather remarkable . the second possible explanation of this apparent outbreak of liver cancer , is a genetic one . 
a complete circuit of the vascular svstem throu h the pulmonarv circulation and so to the spleen t - ia the splenic arterv . in the one case encountered in the duck , pulmonarv metastases occurred , and once the lungs are involved so this second hypothesis mav be the correct one . tumour cells or emboli could then the tumours there mav also metastasize reach the spleen without much diffieultv . 
a direct spread t - ia the lungs seems iinlikelv in view of the formidable barrier offered bv the pulmonarv capillaries . fox and bartels ( 1928 ) favour the niew that in the human subject the spleen and mesenteric veins mav be invacled bv retrogtade extension along the portal in case 6 , besides seros - al implantation on the wall of the int - estine , tumour vein . emboli were found within the veins of the gut wall . 
greenwood 's flock of brown - legliorns , and i have pleasure in recording niy appreciation of iiis co - operation iii this respect , and for much help in otlier directions . the histological preparations are the work of messrs . 
christiansen. from the institutt for generell og elcperimentell patologi , universitetet i oslo . received for publication february 2 , 1953 . it is a strange fact that in the voluminous literature on breast cancer the prognostic value of the size of the tumour is only cursorily dealt with , a fact mentioned by geschickter ( 1945 ) and underlined by bloom ( 1950 )  . 
the explanation probably is , that the view expressed by kaae ( 1948 ) , namely , " it is generally recognized that the size of the tumour is a very important factor in the prognosis , and that the latter is much more favourable for the small tumours than for the large , " seems so generally sound , even self evident , that the problem has not been considered worthy of a closer study . if we examine the pertinent literature , we find , however , that the findings are not unequivocal . dahl iversen ( 1930 ) states that breast cancers up to the size of plums are without recurrences after 3 years ' observation in 83 per cent of the cases , whereas tumours larger , up to the size of a hen 's egg , show only 13 per cent freedom from recurrences after 3 years . eggers , de cholnoky and jessup ( 1941 ) report upon a 5 - year survival of 73 per cent , if the mass is 2 cor less , and only 24 per cent haagensen and stout ( 1943 ) found a if the mass has reached a size of 3 to 6 cm . 5 - year clinical cure of 62 * 2 per cent if the tumour was under 3 cand only 19 - 8 per cent if the tumour had reached 6 cor more . 
they conclude that " the data indicate , as might be expected , that the prognosis becomes worse as the size of the tumour increases "  . bloom ( 1950 ) found 5 - year survivals in the following percentages : tumour less than 1 inch 59 per cent , 1 to 2 inches 45 per cent , and more than 2 inches 32 per cent , and he finds after grading of the tumours that : " of the tumours with a diameter of 1 inch or less , 37 per cent are classified as grade i and 23 per cent as grade iii . 
on the other hand , in the case of growths of more than 2 inches diameter only 8 per cent belong to grade i whilst 54 per cent are grade iii . when the diameter lies between 1 and 2 inches the incidence of these tumours is practically the same " , and he concludes that : " whether the tumours are small or large , the outlook is uniformly good in the former ( grade i ) and bad in the latter group ( grade iii )  . 
on the other hand , an intermediate result is obtained for the intermediate cases ( grade ii ) , the survival rate being practically halved in in other words , the metastasizing power the presence of the larger neoplasms . for growths for grade i and also grade iii cancers is independent of size . classified as grade ii this power bears a direct relationship to the diameter , the larger the tumour the greater the likelihood of spread having taken place "  . 
christiansen the time factors are so long or so short that their significance is obscured under the usual clinical conditions . when kunath ( 1940 ) says : " size and ma88 . - an analysis of this point failed to reveal that a larger tumour carries any more serious a prognosis than " no does a small one " , and hoopes and mcgraw ( 1942 ) likewise conclude : correlation was found between the post - operative duration of life and the size of the tumour removed " , these findings are not necessarily in contradiction to the opposite conclusions , mentioned above . 
the explanation may be a different composition of the groups of tumours , as regard number of representatives of the again we have to guard ourselves in transferring different grades of malignancy . conclusions from groups to individual cases . considering the importance of assessing the significance of a minimum size of tumour for the prognosis of breast cancer , we have examined breast cancer material consisting of a total of 974 cases . 
we planned to examine the ultimate development of breast cancers as small as practically diagnosable . in order to decide the upper limit of the size to include , theoretical and practical considerafirstly , we considered the smallest lump , tions have been taken into account . that size evidently depends upon the site distinguishable as a definite tumour . and upon the amount of adipose tissue . 
a tumour near the surface and in a shrunken atrophic breast will be more easily discovered than one deeply situated it seems that tumours smaller than those the size in a full and developed breast . of a pea cannot reasonably be distinguished from the many irregular nodosities in a cimacteric , or pre - cimacteric breast , and in most cases it is difficult to feel secondly , we wanted to examine tumours a lump smaller than a small hazel nut . of a size so small that the number of cases would represent a very small fraction of the total , whereby we would obtain a statistical claim to a designation " a very small breast tumour "  . 
the tumours are usually characterized by some object for comparison , usually : pea , bean , nut kernel , hazel nut , date - stone , date , wall nut , plum , etc . 
a tumour the size of a hazel nut will usually measure some 10 to 12 by 15 to 17 mone has to have in mind the small size of a norwegian hazel nut to appreciate the size . when we examined our total material we found that only 56 tumours out of 974 , i.e. , 5 - 7 per cent . 
the fate of the patients has been followed for from 10 to 20 years . the material was examined during the later half of 1952 . the clinical information is not always precise , or detailed , as some of the case histories are very short . 
nor is the pathological material always complete , as some of the surgeons do not submit adipose tissue from the axilla if no suspicious glands are found . in other cases a selection of glands only are sent to the laboratory , and finally , some of our paraffin blocks were destroyed during the war , with the result that for some cases a few slides only could be examined . this means that all the positive findings are minimum recordings . the clinical follow - up has been complete , all patients having been accounted for . reliable death certificates have been received for all the dead , and the patients alive have been personally examined by one of us , or by competent doctors as regards the patients living in remote parts of the country . as only the patients with a definite statement as to the size of the tumour have been included , the size is known in all cases . 
8 died from broncho - pneumonia one year and a half after operation , symptom - free . all the others succumbed to their tumours . this 5 - year oure rate corresponds very closely to the rate quoted by engelstad ( 1948 ) for his group of 768 cases , regarded as stage i and stage ii cases . this indicates that our " small " breast cancers do not present a particularly favourable clinical picture . in one aspect our table ii shows a remarkable deviation from the usual , namely , the small difference between the 5 - year and the 10 - year figures , only 1 out of 37 patients dying in the second 5 - year interval . as stated , the whole group of 56 patients has been followed for 10 years . a smaller group has , however , been followed for a longer period , and in table iii some of the results are summarized . 
even if we select the very smallest tumours present in our series , those the size of a pea or a bean , out of a total of 10 , we find only 5 patients alive after 10 years , or more , and 4 patients dead from metastases . in the present series the combined surgical and radiological treatment seems , in a number of cases , to have effected a considerable delay in a finally fatal this delay is of very great value from a therapeutic standpoint , even outcome . if the treatment fails to effect a complete cure . staging actually is an ambiguous process . the prolonged observation also helps to assess more accurately the real stage the simplest and least of the tumours . reliable staging is the immediate clinical , unreliable to a degree to make it practically useless . 
we have , however , to bear in mind that the value even of negative findings of tumour cells in lymph this grouping is rather limited . nodes removed may be the result of the pathologist not finding the cells in spite or , tumour cells may by - pass the usual lymphatic filters in of their presence . the axillary glands and proceed directly to the supraclavicular or the intrathoracic nodes , or the tumour cells may spread via the blood streathe discrepancy between the number of tumours anatomically staged as stage i and the number of cures effected after a proper local operation shows the degree of failure in the process of staging . 
on the other hand , if radiological treatment has been added to the surgical , even the delayed retrospective clinical staging may be incomplete , because a tumour , anatomically staged as stage i and actually being in stage ii , may be cured by radiological treatment and thereby escape its proper staging . in spite of the incomplete clinical and pathological information , it will be of some interest to examine the state of affairs , as regards stages recorded in this material . 
10 , 27 , 31 died symptom - free after more than 10 years ' observation . the large number of fatal outcomes with negative findings of tumour cells in the axillary lymph nodes confirm our assumption that our figures represent the considerable number of patients alive and symptom - free minimum findings . in spite of positive findings of tumour cells in the lymph nodes , actually 5 patients , further confirm our statement as to a considerable effect of the treatment , but l . 
christiansen also underlines the great number of patients already in stage ii ( or further ) at the moment of presenting a very small breast cancer . if we add these 5 patients with microscopical lymph - node metastases , but still symptom - free , to the group of the dead and those living with metastases , we find that two - thirds of all our patients with small tumours were in stage ii ( or further ) when the operation was performed . the value of bloom 's ( 1950 ) grading and analysis of his material made it natural to try his principles on our material . 
we deliberately use the word principles , because any grading is arbitrary , and the designation in each case is the result of a subjective estimate of a series of characteristics , which themselves are unprecise . 
the explanation may be that the number of cases is too small , that the treatment given may have influenced the final result because a number of very malignant tumours are comparatively radiosensitive , or it may be caused by our incompetency . 
the medium long histories , from a few months up to a year , show an increasingly gloomy picture . if we again deduct the grade i cases we conserve the pattem , and still find indications of a benefit for very quick reaction with immediate treatment after diagnosis , and with a still more pronounced bad prognosis in cases with delays from a few months up to a year . for the very long histories ( more than a year ) the comparatively better prognosis is preserved , and may partly be accounted for by a default in the process of grading , partly by combination of high malignancy and high grade radiosensitivity in certain cases , and partly by inclusion of tumours with a more moderate malignancy ( grade ii )  . besides , a perfect correspondence between morphological grading and biological development is evidently not obtainable . too many unknown factors are involved here . 
we have adopted the following staging , which is similar to that employed at the christie hospital and holt radium institute , manchester : stage i . - primary growth limited in extent to site of origno loss of mobility or function . 
lymph nodes fixed , matted or bilateral , or distant metastases present . table iv shows , as already mentioned , how many cases had already reached stages iii or 1v when first seeking treatment . 
warren and gates ( 1932 ) investigated the problem in considerable detail , and concluded that a patient with one cancer was statistically more likely to develop another cancer than a normal individual . 
watson ( 1939 ) calls attention to the fact that when a patient with carcinoma of the oesophagus has - a second growth this is nearly always situated in the mouth . 
it is therefore of interest to know how often this treatnment succeeds or fails in its objective , and in the latter case , when there is a recurrence , what are the chances of further arresting the disease . these facts cannot be determined with any real accuracy , since each case clearly has to be assessed on its clinical development and course . 
harmer in stage i and ii cancers of the lip , re - treatment is rarely successful . first planned treatment fails , the patient does not often have a second chance . if the response of primary and secondary to irradiation . glucksmann ( 1948 ) has stated that the response to irradiation of the primary and secondary manifestations of cancer of the mouth is about the same , and that those growths " with a tendency to lymph - node involvement differ in their biology and radio - curability from those without such a tendency . " the more generally held view is that while the primary may be " cured , " the secondary is often more resistant to treatment . only stage iii and iv cases can be analysed if the theory that an irradiated primary will recur as frequently as an irradiated secondary is to be examined . there were 248 patients with stage iii and iv growths arising from buccal sites in whom radiotherapy produced regression of both primary and secondary forty - five remained well , and 203 recurred : 61 in the primary only , growths . 69 in the secondary only , 73 in both . 
hartley has kindly done a significance test on these figures . the number of cases has been adjusted so that the proportion of stage iii and iv royal cancer hospital patients is the same as that of the holt radium institute series . 
the accessible growths of the for cervical mouth and lip , and teleradium for the oro - pharyngeal primaries . metastases block dissection hasbeen the method of choice , or radium therapy for the inoaperable cases . x - rays have&been used comparatively rarely . memorial hospital , new york ( martin , 1948 )  . - hayes martin states that surgical excision is the method of choice for cancer of the lip , gum , anterior for oro - pharyngeal portion of the tongue , cheek , floor of mouth or palate . growths a combination of roentgen therapy and interstitial radiation is indicated . cervical metastases are treated by dissection when operable and by x - rays when not . radiumhemmet , stockholm ( berven , 1937 )  . - for more than 20 years - the usual treatment for growths of the tongue and most other buccal sites has been teleradium , with diathermy coagulation of any residual mass . 
sixty - five per cent had symptoms for less than 6 months before treatment commenced , yet ( with the exception of carcinoma of the lip ) in 60 per cent of cases the disease had already metastasized to the cervical lymph nodes when first seen . 
the treatment of these 800 cases has been largely by radiotherapy . comparison of the results of treatment published by different authorities is table xv shows wide difficult because of lack of uniformity in criteria adopted . divergencies for instance in the survivals of patients with growths of the buccal this is largely due to mucosa , and to a lesser extent of the alveoli and palate . the small numbers of the cases . the last section of this paper shows that although very different methods of it is treatment may be employed , the results on the whole are much the same . therefore inadvisable to attempt definite conclusions from the analysis of the cases presented . 
the cases have been under the care of all members of the staff of the hospital , past and present , to whom grateful acknowledgment is made for permission to publish them . in the preparation of the paper much help was derived from copeland - chatterton punch cards , many of which had been completed by j . 
the carcinogen was then placed in contact with the surface of the epithelium , and ingerted into a bashford transplanting needle , care being taken to shield the carcinogen from the connective tissues of the host animal . in some instances as manv as tbxee subcutaneous primarv grafts were made on each side of the belly of a s ' mgle host mouse to give a series of prostatic tumours growing under identical hormonal conditions . 
the technique is similar in some essentials to that - previously employed bv greene ( 1945 ) , and rous and smith ( 1945 ) , except for the important difference that the present experiments involved tiimour production from adult , not embrvonic tissues . the influence of bilateral orchidectomv upon the growth rates of glandular and squamous cefl prostatic carcinomas was mvestigated in 6 - months - old mice , which had pre ' %iously been castrated before attaining pubertv . 
10 were of the squamous variety , and 2 were spindle - cell sarcomas . sixteen homologous grafts failed to gi - ow , and were foiind at autopsy not to have becoi - ne vasettlarized . in order to detern - iine the early phases of carcinogeiiesis , witliin the primary grafts a further 30 mice received prostati c iniplai - its , and , " , - ere sacrificed at intervals ranging from two weeks to five inonths after iniplantation . 
which are practicallv fused together with an anterior portion and an isthmus or middle lobe which , as in the rodent , surrounds the urethra . unlik - e the hu - man crland , the mouse prostate has no uterus masculinus or its equdvalent , nor is it encapsulated . 
thus in the human gladd there are as many as 32 ducts ( 31axiniow and bloom 1948 ) , whilst in the mouse them are onlv six . a fibromuscular stroma consisting of dense connective tissue is common to both ty - pes of gland . 
the cytoplasm of the glandular epithelium in both species contains numerous secretorv granules , the majority cytologically treated mouse maerial shows the secreticn of which are , of lipids . in both forms to consist ot protein w%ith fine lipoidal droplets in suspension . 
iiornixg to a failure in the release of the secretion , siiice the ducts ai - e iio lojitretpatent , and proliferation which might be due to the direct action of the carciilogeii . neoplastic change - s in graft8 implanted with the carcinogen . the carcinogen , which is placed in direct contact with the living tissuewithout solvent such as oil . 
or lard , induces verv little foreign body reaction , necrosis or residue within the graft which iiiight mask or conceal the actual areas where neoplastic changes fii - st arise . 
h perplastic alveolus froni which it has arisen . through a whole graft of dorsal lobe epitheliuni fixed 41 weeks after implantation . there is very little foreign bodv reaction , and it will be iioted how clearly the foci in which iiialignant changes arst arise may be detected . adjacent to alveoli lined with a , low colunuiar epithelium and distended with secretion colitaining epithelial debris and polyiiiorphs are collapsed alveoli in wliieb the epitheliuni has entered an exhaustion phase . 
the tongue - lik - e colony , of earlv malignant cells , of t3 - pe a was t3 - pical of those tumours which finally developed into secreting glandular carcinomas . l [ n the example ihustratc ; 1 the proliferation arose from a single alveolus and was the only fo - cus of later stages from other grafts showed malignant change in this part - icudar gr - aft . the onset of secretorv activitv . 
14 shows three ii - ialignant alveoh in the peripheral engaged in secretion . area of an invading new grom - th of this type from an eight weeks ' old graft.. several epithelial cefls are in process of abnormal cefl division . 
transplanted into n - lice of the s - ame age and sex as the host mouse , retained their histological charact - c - rs for 16 generations of serial transplants before finallv transforming into a squamous - cehed tumour . the type b lesion arose in the various grafts exaniined from a single alveolus . aild the example illustrated in fig . 
the area of the alveolar wafl malignant cells - , contain small nuclei with nunierous atypical mitotic figuxes . apart from the different morphology and staining reactions of the prohferating cells . 
it will be noted that they tak - e origin from an alveoluss in which secretory adjacent alveoli not shor% - ing these proliferative activitv has been inhibited . changes are distended with secretion . in older grafts the type b prohferation leads to the formation of pseudo - alveoli at the margins of the tumour and . although the glandular architecture of the epithelium is thus partly restored , there is no evidence of secretion . 
the secretory epithelium like that in the mouse gland is thrown into folds which project into the glandular lumina . note alveolar concretions , and compare with that of mouse in fig . 
4. - implant of portion of dorsal epithelium from a normal strong a mouse without carcinogen after surviving subcutaneously in a host male mouse of same age and strain for 12 weeks . note distension of alveoli with prostatic fluid which is far in excess of what is typical of the normal gland in 8itu , and frequently leads to cystic dilatation . 
9. - early hyperplastic changes in prostatic epithelium of a strong a mouse , after eight weeks ' subcutaneous implantation with carcinogen in a host mouse of same sex , age and stra ' the glandular epithelium contains patches which are 10 - 20 cells in depth . 
on palpation the tumours undergoing regression were hard and the two which failed to respond to orchidect.omv were soand sin - iilar nodular t.o those growing in the control mice . 
variable influence of orchidectomv on the behaviour and gro - wth of this alandular carcinoma was further demonsirated in another series of experiments which were repeated at a later date . in this instance two groups of mice , 10 in each , lik - ewise castrated before pubertv . 
received transplants of the same tumour . the gro , %th rate of three tuniours in the first group of io mice was entirelv four tumours in the second group also grew at approxitunaffected bv castration . iiiatelv the same rate as the transplants in the intact control mice . 
four tumours - , responded to this treatment bv showing an immediate increase in growth rate while the , remainder were una#ectedsquanwus - cd , l cwrcinonia.. a glandular cell carcinoma which had undergone spontaneous inetaplasia after its 10th generation of serial transplants in non - castrated normal male mice , was chosen to determine the possible influence of orchidectomv on a glandular tumour which was undergoing squamous transformation . microscopic exan - iination of this particular tuniour had sho - w - n that the metaplastic alveolar epithelium was columnar and much of it still retained secretorv activitv . 
a variable degree of keratinization associated with prickle cell transformation of the epithelium occurred in concentric nests of cells in the peripheral alveoli of the tumour . comparison of the grouth rates of this particular tumour transplanted inw intact control mice . 
the occasional slight inhibition of tumour growth in soiiie orchidectomized mice was within the limits of possible normal variation . the histological changes accompanying vaiiations in grawth and behaviours , in castrated and non - castrated mice . 
17 , were ha ' rder and tnore nodular on palpation than those growing in secretory activity as judged from sectioiis had beeil sitpcontrol intact mice . pressed and squamous metaplasia , of variable intensity in different areas of aiiy tumour , was always found . 
 ' portions of this tumour failed to grow when transplanted into normal ho ; t rnice . tumours inhibited bv castration but subsequentlv treated with testosterone . after which wth was renewed . 
the alveolar character of the growth had persisted , but.the epithelial cells were shorter than in the original untreated tumour . these results were confirmed in a second series of experiments involving the same number of castratm mice using the same dosages of testosterone . 
tumours found to be retarded in growtli during the fifth week of treatment were characterized by a decrease in the size of the majoritv of the alveoli , a reduction in the height of the epitheliuni , a coinplete disappearance of cell - divisioii , and an increase in the fibro - mtiscular stroiiia . 
the alveoli diminished in size when this rupture occurred , whereas adjacent alveoli with intact epithelial cells appeared to be so slightly affected by the oestrogen that little more than a reduction in the lieight of the cells could be obsei - ved . 
a detailed study of the hyperplastic ' changes in numerous grafts has shown concltisively that in no single instance has an actively secreting epithelium been the focus of malignant change . 
the technique used in the present without at the same time da experiments is pomibly supenor to that involving injection of carcinogens , dissolved in such solvents as lard , merely because it entails less damage and concentrates the carcinogen at the proper site . since the present technique also involves homologous grafting , however , the reaction between host and graft tissues may play some part in the successful induction of a tumour . in mice the survival of a homologous graft seems to depend on the use of a closely inbred stock mice of incleterminate ancestry will not often tolerate grafts for strain . periods sufficient for the establishment of tumours . recent experiments have indicated fwrthermore that the age of the mice providing the graft tissue , and the age of the host mice into which the grafts are implanted , have an important bearing on the problethus the survival rate of grafts of lung or prostatic epithelium without carcinogen was greater if host mice under eight weeks old were used , and was considerably reduced if the mice were over eight months this was invariably the case if the mice were of mixed or pure line origin , old . but only 12 per cent of the grafts in young mi ed stock mice survived as against in older mixed stock mice of 8 months 85 per cent in the young pure line mice . to one year no graft survivecl after three months ' implantation , whilst in inbred mice of a similar age 25 per cent of grafts survived after the same period . 
combining the carcinogen 20 - methylcholanthrene with grafts of lu or p - rostatic epithelium in 25 eight - weeks - old mice of mixed stock gave only one tumour , a spindle - miled sarcoma , twelve weeks after grafting ; the remaining 24 host mice failed to produce tumours , and at autopsy the grafts were found not to have price ( 1941 ) , using rats of different ages from an albino become vascularizedl strain which was not strictly pure hne , found that ventral lobe prostatic tissue grafted subcutaneousl in the abdominal wall beha - ved in much the same way , prostatic tissues from old rats being very limited in their capacity to survive as homologous grafts . 
many apparently viable grafts from old rats were found to be degenerate on histological examination , but when regrafted into younger hosu the implants underwent a rapid recovery and the pmstatic epithehum even regained its secretory activity . 
one of the most intere8ting features in successful grafting of prostatic epithehum is its ability to continue secreting while growing under the influence of foreign host reactiom and changed vascularity . 
ob - viously androgenic stimulation , as price ( 1941 ) maintains , must be important in this phenomenon . the dependence of prostatic epitheli - um upoii androgen smretion has long been realized and the experimental evidence need not be referred to here , except to mention that in recent years the elegant technique of transplantation of fmgments of prostate into the anterior chamber of the eye ba - s provided additional confirmation . and rosenblum ( 1937 ) , moore , rownblum , tolin and melchionrka ( 1937 ) , and moore and smith ( 1937 ) , grafted rabbit prostatic epithelium in this way and photographed the implants dailv . 
they were able to record fluctuations in size of the grafts which were abohshed by castration , and considerably increased by administration of testosterone propionate . heckel and kretwhmer ( 1935 ) made similar observations of the responses of prostatic grafts to anterior pituitary extracts . 
horning mice or rats will maintain the size and normal histological appearances of the hill and strong ( 1938 ) attribute the androgpnic prostate and seniinal vesicles . effect of the ovary to the lowered temperature of the ear , and deanesly ( 1938 ) has correlated this activit ' with extensive luteinization of the theca intema within the ovarian grafts . another potential source of androgens to be considered in relation to prostatic grafts and tumours is , of course , the adrenal cortex . 
the rare adrenal insufficiency in young children associated with adxenal hypertrophy leads to enlargement of the prostate and differentiation of its glandular tissues to a degree comparable with the adult gland ( dijkhuizen and behr , 1939 - 40 )  . prostatic enlargement also occurs in adults with adxenal cortical tumours . miller ( 1947 ) has found a relative increase in dehydroisoandxosterone , and a decrease in androsterone in the urine of patients with benign hypertrophy of the prostate . according to callow and callow ( 1940 ) the source of dehydroisoandxosterone is probably in the adxenal cortex . it remains in the urine after castration , but disappears in cases where there is destruction of the adrenal cortex . while it niight be assumed that grafts of prostate or transplantable prostatic tumours would have poor chances of survival in female hosts , under certain conditions they do in fact survive and this must be attributed to the influence of androgens produced either in the ovary or in the adxenal cortex . price ( i 941 ) grafted normal prostate into female host rats , and found that in some cases the grafts were similar in histological structure to the prostates of castrate males , whereas other - grafts flourished and underwent secretory activity . this result she maintained could be due to the development of androgenic foci in the ovaries of some , but not all , host animals . 
the grafts failed to differentiate in spayed rats , whereas they survived in a functional condition for prolonged periods if the hosts were over 80 days old . either virgin females or rats which had littered frequently would sustain functional grafts , provided they were not youngei than this apparently critical age . the opinion is often expressed that the prostate gland in rodents is not strictly homologous with the prostate in the human , and thus there can be rttle justification for comparing growth behaviour and endocrine responses in experimentally induced prostatic tumours or hyperplasias with the spontaneously occurr , ingconditionsinthehumangland . greenstein ( i - 947 ) maintainsforinstance , that because certain rodeint prostate tumours grow when transplanted into female mice , whereas human tumours are so sensitive to inhibition by oestrogens , the two types of neoplasm are not fundamentally the same . 
apart from the single case reported by deniing , jenkins and van wagenen ( i935 ) of a spontaneous nodular hyperplasia in the suburethral tissue of an albino rat , there is no record of spontaneous prostatic hyperplasia or cancer in rodents . if it can be shown , however , that the prostate tumou - ts induced by methylcholanthrene behave in essentially the same way to hormone administration or deprivation , the differences between rodent and human neoplasms will be less significant . the glandular carcinomas described in these experiments , when transplanted into rnice ca 'strated before puberty , show complete inhibition of secretion , later followed by squamous differentiation . 
subsequent traimplantation into castrated hosu is not followed by any appreciable inbibition . some glandular celled carcinomas am thus dependent for their sustained growth on an adequate androgen level ; the squamous growths would appear to flourish without testicular androgens and , if they are at all androgen - dependent , it must be concluded that adrenal cortical androgens are in these cases suflicient . and hodges ( 1941 ) buman prostatic cancer falls into two according to it is possible that groups , androgen dependent - and androgen independent . squamous - celled carcinomas in mice belong to the second category , although aours rarely occur in man ( willis , 1948 )  . such t a smah percentage of glandular mouse tumours failed to regress when transplanted into castrated hosts ; they even grew at approxim tely the saine rate m those transplanted into uncaamted mice . 
howard ( 1937 , 1938 ) has demonstrated that removal of the gonads in rats , provided these are sufficiently yoijn , increases the capacity of the adrenals to secrete androgens . 
as ar the mice in the present experiments were castrated before puberty , and an interval of several months elapsed before they received t aour transplants , it seems probable that androgenic foci had developed in the adrenals of those castrated mice in which unfortunately.biochemical assay the tumours showed no inbibition of growth . of androgens secreted from non - testicular sources cannot be undertaken in the mouse to confirm or refute these conjectures . on the chnical side the serum acid phosphatase and urinary 17 - ketosteroid levels can be used respectively as indicators of the activity of mahgnant prostate cells and of androgen smretion . 
thus mn4vs stevens and hodges ( 1941 ) studied cases in which a recurrence of prodatic cancer had fobowed an initial improvement in the condition obtained - by bilateral orchidectomy . there was a rapid reduction in the serum acid phosphatase , and a simil ri marked fall in the urinary 17 - ketosteroids after orchiclectomy . 
the development of androgenic foci in the adrenals was regarded by and swtt ( i945 ) as responsible for the recurrence of the disease . recently , following failure in four - selected cases to control growths by orchidectomy , these worken tried bilateral adrenalectomy ancl , although three of the patients died within a comparatively short fume after operation , the fourth survived for 116 clays . 
cox ( 1947 ) tried unilateral adrenalectomy on three patients with prostatic cancer , all of whom had temporarily responded to treatment with there was an immedi te drop in the 17 - ketosteroid level and a oestrogens . r tumours transplanted into normal male mice showed a varying retardation of growth after oeamgen treatment , but in no single instance did any undergo complete regression , as was the case following orchidectomy . 
horning inhibition of tumour growth with such relatively high doses was the result of non - specific toxic action . it was also found that the amount of stilboestrol tolerated depended upon the genetic constitution of the rnice . 
although in the present experiments the dose of stilboestrol was approximately half of that used by ludford and dmochowski ( 1947 ) , the average loss of weight of the tumourbearing rnice was approximately i ' to 2 g . 
during the total period of treatment . histological examination of regressing glandular tumours after stilboestrol gested that diminution in size of the tumours was primarily due to thera inhibition of secretion , later followed b ' degeneration and collapse of alveoli . schenken , burns and kahle ( 1942 ) and fergusson ( 1946 ) have exandned serial biopsies of human prostatic carcinoma under oestrogen treatment . 
the former authors described in detail such cytological changes as vacuolation of the alveolar epithelium , disintegration of the cell membranes , sometimes accompanied by stratification of the epithelium , and an increase in the stroma . these changes are very similar to those which occur in the glandular mouse tumours during oestrogen treatment . 
the squamous metaplassia , which some of the glandular mouse tumours undergo in response to oestrogen administration , is rarely found in the human gland after sirnilar treatment . recently , however , inglis ( 1948 ) described a pronounced squamous differentiation in a man treated with stilboestrol for prostatic cancer . it is tempting to regard the atrophy of prostatic tumours in the mouse as due to failure of optimum androgen secretion in the castrated hosts , or to a similar drop in gonadotrophin production when intact tumour - bearing mice are treated those tumours whieh fail to regress are possibly receiving with oestrogens . sufficient androgenic stimulation from the adrenal cortex . inhibition of secretion and degeneration of the epithelium in these tumours are so similar to the changes induced in the normal prostate following castration or oestrogen administration that any more complicated mechanism operating in the case of the tumourbearing mice seems unnecessary . 
it bas been possible in grafts , impregnated with the carcinogen , as soon as four to eight weeks following implantation , , to distinguish between three distinct types of early malignaint lesions . detailed swdy of the hyperplastic changes in prostatic alveoh in numerous grafts showed that in no single idstance has the actively secreting epithelium been the focus of mahgnant change . it tberefore appears that the non - secreting exhausted alveolar cells m the prostatic gland are more susceptible to the action of the carcinogen than those at the height of secretory activity . this supports the contention that chemical carcinogens act - more readily on cells following depression of cellular activity . the influence of sex hormones and orchidectomy was determined on the behaviour and growth of glandular and squamous - cell carcinomas of the prosute . a greater number of glandular carcinomas regress when transplanted into male mice cm - trated before puberty , and a small percentage of - the - e tumours resume growth when treated with testosterone propionate . 
tumours which at the time of their induction were diagnosed as squamous growths , or glandular carcinomas which had undergone spontaneous squamous differentiation during serial transplantation , exhibited no appreciable response to these fornvs of therapy . these results indicate that only glandular and not squamous carcinomas are dependent for their sustained growth on an adequate androgen level . glandular carcinomas when treated with dieth - vlstflboeaml respond more re - adily than squamous t aours . 
and bave given additional information on the factors responsible for tumour regremon . particular attention hm been paid to those glandular tumours which failed to respond to either orchidectomy or hormonal theraphy , and the possible endocrine factors inducing resmtance to treatment are discussed in the hght of recent experimental and clinical evidence . this investigation has been supported by grants to the royal cancer hospital , fi - om the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the u.s. 
at the time it was known that adenomas of this gland produced abnormalities in children and young adults ; it was therefore postulated that in later life , when gigantism and acromegaly were no longer possible , increased activity of the pituitary gland might be responsible for the production of tumours ( funk , 1917 )  . for a long time and for obvious reasons it was impossible to put this hypothesis to a test . 
thanks to the classical work of evans , li and simpson ( 1948 ) we now have the necessary tools for preliminary and systematic appraisal of the importance of various hormones of the anterior pituitary in tumour growth . the purpose of the work reported in this paper was to test the effect of various anterior pituitary and related hormones upon the growth of implanted tumours in hypophysectomized rats . 
as a supplement to this work we also dealt with the removal of certain organs ( mainly glands of internal secretion ) on the rate of growth of a transplanted rat tumour in otherwise intact animals . while there is no doubt that studies on this subject have already been made , it appears doubtful whether a systematic study was ever made of the effect of the removal of these organs upon the growth of one particular tumour . 
to check on the completeness of the surgical procedures used we have excised and weighed , at the time of sacrifice , those organs that are in a physiological relationship to the excised gland . for instance , in orchidectomy the seminal vesicles and the prostate were weighed . 
the diet was the same as in the hypoall animals received tap water , except the adrenaphysectomy experiments . lectomized animals , which received 1 per cent saline . in some experiments rats 282 c . 
no improvement in survival was noted . 1 of the controls 40 per cent had open vaginas , none of the castrates , at time of implant . a mortality was about 30 per cent of the animals operated upon . 8 mortality of 33 per cent of the operated animals , probably due to bartonella muria infection . 4 all animals received 60 mg . 
of alloxan from the time of tumour shaefer - hartman blood - sugar determinations were as implantation to the end of the experiment . follows : pre - implant 461 - 9 mg . 
using the enriched diet in our present work , we have attempted to restore tumour size by the administration of some anterior pituitary hormones and serum gonadotropin . growth hormone increased tumour weight of hypophysectomized animals so treated . however , this increase is directly proportional to the increase in body weight due to the hormone . thus , tumour weight difference per g . 
body weight difference is the same for both growth hormone treated and intact animals using untreated hypophysectomized animals as the base . it would appear that the influence of growth hormone on tumour growth is related to its effect upon the general metabolic condition of the animal . this is not true for acth and thyrotropic hormone . these two hormones cause a greater increase in tumour growth than could be expected from their effect upon body growth , using the same criterion . the ratio of tumour weight to body weight gain in adrenalectomized animals seems to confirm the fact that without adrenal hormones the tumour does not grow as well as in intact rats . this is the opposite of the effect ofacth treatment . 
the restorative effect of the latter hormone and the decreasing effect of the operation , greater than their respective actions upon body growth , show a clear effect on the tumour itself . 
our data are not as clear in the thyroidectomy experiments , however ; in one experiment the tumour - body weight ratio is indicative of the depressant effect of this operation upon the tumour . in the other experiment the administration of thyroxine to a thyroidectomized animal had the same effect as thyro286 c . 
ehrlich tropic hormone given to a hypophysectomized animal . increase in tumour size greater than could be expected from the body growth . this effect was an the effect of fsh and serum gonadotropin on hypophysectomized animals was not very marked either on absolute tumour weight or on tumour weight per g . 
body - weight gathe treatment of castrated males with testosterone may have stimulated tumour growth . splenectomy may have had some effect upon increasing tumour size by both criteria . while it is clear that diabetes per se reduces tumour growth , it is not so clear whether or not this reduction is related to body weight . it has been shown by mceuen and thomson ( 1933 ) that the reduced rate of tumour growth in hypophysectomized animals could not be solely attributable to the concomitant metabolic deficiency . in their studies on intact animals , evans , moon , simpson and li ( 1950 ) have found that only by long - continued treatment with growth hormone were they able to produce neoplasms , while shulman and greenberg ( 1949 ) in a shorter experiment , using intact mice , found no effect upon tumour growth with this hormone . 
daily with their diet ( bielschowsky , in experiment ii the ordinary stock diet ( hall , 1948 ) was 1944 ) for 25 weeks . given and the carcinogens , dissolved in peanut oil , were administered by stomachtube . 
the survivors of experiment i were killed in the 63rd and those of experiment ii in the 52nd week of the experinment . table i summarizes the results of experiment i . for comparison the tumours obtained by feeding 4 mg . 
the first tumour , a hepatoma , was examination . foumd in the 54th week , and the second , a cancer of the meatus acousticus externus , 3 weeks later . 
by the 24th week neoplasms of the breast gland were present also in cancers of the meatus acousticus externus made their the two other groups . appearance in rats treated with the methyl compounds from the 34th week palonwards , whereas in the a.a.f. 
group the first was seen in the 25th week . pable liver tumours , lowever , occurred only in the latter group after the 33rd week of the experiment . these consisted of a few minute cysts . the total yield of cancers induced by d.a. 
induced two hepatomas , definite signs of liver damage and fairly widespread cystic cholangiomata in 2 other males of this group , while 2 of the females showed a few minute cysts in the liver . 
four hepatomas were found in the males and one in the females , cystic cholangiomata being present in all . to summarize , the genetic background determined to a large degree the site of tumour development . 
thus breast tumours appeared in a much higher incidence in the wistar rats than in the piebalds , in which cancers of the small nevertheless in both strains a striking difference intestine were readily induced . in the response of the liver to the three compounds was apparent . in the first experiment 700 mg . 
were given , while in the second the total dose administered amounted to about half of the methyl compounds and to approximately a quarter in the case of a.a.f. yet in both experiments a.a.f. 
is readily split off in vivo and therefore can be only of minor importance for the carcinogenic activity has been substantiated by weisburger , weisburger and morris ( 1950 ) , who showed that after feeding w_ - c14 - 2 - acetylaminofluorene radioactivity appeared in the breath within 6 hours . ray and argus ( 1951 ) found the toluene - sulphonic ester of 2 - aminofluorene to be non - carcinogenic for the rat , only minute amounts of this ester being morris , dubnik , dunn and johnson ( 1947 ) , studying hydrolysed in the body . the action of 2 - nitro , 2 - amino , mono - acetyl and diacetyl - 2 - aminofluorene , reported that the acetyl compounds induced the majority of liver tumours observed , when the substances were given per os . why the acetylated aminofluorenes have such an affinity for the liver , whereas m.a. 
bartholomew 's hospital , london , e.c.1. received for publication january 12 , 1949 . thie carcinogenic activity of ethereal extracts of domestic soot was demonstrated by passey ( 1922 )  . domestic soot may contain as much as 40 per cent of tarry matter ( cohen and ruston , 1925 )  . 
the use of the fluorescence spectrum by mayneord and hieger led to the identification of 3 : 4 - benzpyrene in gas - works pitch ( cook , hewett and hieger , 1933 )  . this discovery suggests that this hydrocarbon might be one of the carcinogenic agents in domestic soot , although the conditions of pyrolysis in the domestic hearth , and in the gas - works retort , are different . berenblum and schoental ( 1947 ) found that carcinogens other than 3 : 4 - benzpyrene were present in coal tar . 
the first attempt to identify 3 : 4 benzpyrene as a contaminant of the atmosphere was made by hieger ( 1946 ) , who exposed non - fluorescing benzene to the air in london , and found that the fluid became fluorescent and showed spectral bands resembling those of benzpyrene . 
for the present purpose , samples showing a ph value of 10 - 0 - 10 - 3 were found to be most suitable . 3 : 4 - benzpyrene . - the commercial product contains a pale - blue - fluorescing impurity which is very strongly adsorbed on alumina . 
benzene. the first attempts to separate benzpyrene from soot were based on the method described by berenblum ( 1945 ) for the extraction of benzpyrene from coal tar . in the original method vacuum distillation of the suitable fraction of tar was followed by solution of the distillate in concentrated sulphuric acid . attempts at vacuum distillation of benzene extracts of soot showed , however , that the composition of the soot extract was very different from that of coal tar . 
evaporation of the benzene extract yielded a residue consisting mainly of non - volatile material , which appeared to decompose on distillation in vacuo with evolution of gas . direct sulphuric acid extraction of the crude tar extracted from soot was also unsuccessful , probably owing to considerable sulphonation . moreover , recovery experiments , with microgram quantities , of pure benzpyrene from icecold sulphuric acid showed that considerable loss of the hydrocarbon occurred , and that the method was useless as a quantitative one for such small amounts . chromatographic adsorption was next tried . 
when an extract of soot was submitted to chromatographic separation , the characteristic fluorescence spectrum experiments with various of benzpyrene was given by the appropriate eluate . samples of alumina showed that spence 's type h alumina , containing adsorbed benzpyrene , could be washed freely with a mixture of benzene - petroleum ether ( 1 : 10 ) without elution , and that the benzpyrene was eluted only when the proportion of benzene was increased ( 3 : 10 )  . 
the extract was given a preliminary purification by passing it through a short column of alumina ( 14 x 25 mm . ) and eluting with the same mixture of solvents . 
the lower band was easily eluted with benzene - petroleum ether ( 1 : 10 ) , while the upper could only be washed down when the benzene content of the eluting fluid was increased ( 3 : 10 )  . this latter fraction is shown in fig . 
cotton treated in a colloid mill . this was prepared from cotton velvet shearings suspended in water and passed through a colloid mill 6 times in succession . after each passage only the finer fraction was slected for further milling . 
5 shows the compact growth of mouse mammary carcinoma obtained in the presence of fibres of colloid milled cotton ; as a contrast the uneven growth of cells in the absence of fibres is shown in fig . 
for 5 minutes , washed with distilled water until free from ammonium ion ( tested by nessler 's reagent ) and sulphide ion ( tested by sodium nitro - prusside )  . they were then bleached 15 minutes at room temperature in sodium hypochlorite solution containing 0 - 1 per cent available chlorine , and finally washed with distilled water until free from chloride ion ( tested by silver nitrate )  . 
they were stored under distilled water . the films were autoclaved in distilled water at 18 lb . / square inch pressure , and before use were rinsed in sterile tyrode solution , excess moisture being removed with sterile filter - paper . cultures were placed directly on the coverslip , a drop of mixed serum and embryonic extract spread over them and the viscose film then applied . 
the culture usually adhered to the glass surface , and on washing or fixation the film floated off . the film is easily cut with a cataract knife when the tissue is subcultured . with a thickness of 30 , u the total thickness of the preparation was considerably less than can be achieved with the double coverslip method of maximow . 
they have found that perforated cellophane is an advantageous addition to flask cultures and hanging - drop preparations ( evans and earle , 1947 ; earle and evans , 1949 ; schilling , earle and evans , 1950 ; earle , evans and schilling , 1950 )  . in our hands perforated cellophane , kindly supplied by w . 
earle , was very siinilar in effect to viscose , but the outgrowth obtained with viscose seemed slightly greater . glass wool has been used for the same purpose by warner , hanawalt and bischoff ( 1949 ) , who used it with the roller tube method . 
viscose ifim , colloid milled cotton and durafil were technicauy suitable for use , and have been found advantageous in improvilg growth of malignant cells and of enabling growth of normal and malignant cells to take place in fluid media . we wish to thank professor astbury of leeds for his advice , and t . 
of the hydrocarbon suspended in arachis oil , by intraperitoneal injection , in no case , however , even with 100 mg . and the rats weighed daily as a group . average 1 : 2 : 5 : 6 - dibenzanthracene , after 9 days a second injection of growth rate of any group of rats observed . 1 : 2 : 5 : 6 - dibenzanthracene was given and again no the same amounts of constant effect was observed , but after several days considerable fluctuations in the growth rates occurred , and eventually 21 days after the first injection all the groups showed a lower average weight than the control group , which had although the average weight of the received injections of arachis oil alone . group which had received the two injections of 100 mg . 
1 : 2 : 5 : 6 - dibenzanthracene was slightly lower than that of the other group , there was no direct relation to the amount of hydrocarbon given , and the rats receiving 50 mg . had a higher average weight than the group which had been given 25 mg . 
of the other five left as controls . pituitary extract daily had practically no effect on the growth of the animals , but when the amount was increased to 1 c.c. 
1 : 2 : 5 : 6 - dibenzanthracene to rats maintained on a 20 per cent protein diet causes no immediate inhibition of growth , a delayed toxic effect occurs which ultimately results in death of all the animals . 
when the length of time survival of the dibenzanthracene - treated rats on the 20 per cent protein diet is compared with that of the similarly treated animals maintained on the 10 per cent protein diet , as shown in fig . 
6 , it is seen that although in the latter group there is an immediate growth inhibitory action , the animals survive for a longer period after treatment . ( mean survival time of 17 animals on the 20 per cent protein diet was 44 days after dibenzanthracene injection , whilst that of the same number of animals on the 10 per cent protein diet was 67 days . ) effect of 1 : 2 : 5 : 6 - dibenzanthracene on tail growth in rats maintained on a 20 per cent protein diet . an attempt was made to see if any growth - inhibiting action of 1 : 2 : 5 : 6 - dibenzanthracene could be demonstrated by measuring the increase in tail length of rats treated with this hydrocarbon . young male rats of about 50 g . 
the animals were lightly anaesthetized with ether , placed on x - ray film in the prone position , and skiagrams taken of the bones from the pelvic region to the tip of the tail . 
of stilboestrol was injected in all but two of the animals growth of the tail was markedly into each rat . inhibited , and in 3 rats tail growth practically ceased . 
the difference in the diets used is mainly of the protein content and , since the fat content of the diets is the same , their total it would thus appear that the procalorific values do not differ appreciably . tective action of the 20 per cent protein diet is directly attributable to its high this is confirmed by the protective action of the 25 per cent protein content . protein diet , which differs from the unprotective 10 per cent protein diet only in protein content . the growth - inhibitory action of the hydrocarbon does not appear to be the result of a direct action on the anterior lobe of the pituitary gland causing interadministration of growth hormone ference with growth hormone secretion . to rats maintained on the high protein diet and treated with dibenzanthracene does , in most cases , bring about some increase in growth , but appears at the same time to increase the toxic action of the hydrocarbon since this growth dibenzanthracene is increase is rapidly followed by the death of the animal . only very slightly soluble in body fluids , and when administered by intraperitoneal injection remains in the peritoneum for a considerable period of time . metabolism of the compound probably takes place by combination with since this combination is sulphydryl - containing substances as its first stage . not the direct cause of its growth - inhibiting action ( elson , goulden and warren , 1947 ) , it is probable that a later stage metabolic product is responsible for this effect . 
one of the effects of the growth hormone is to increase the total metabolism of the animal , and it seems likely that this results in increased absorption and metabolism of the dibenzanthracene from the peritoneum of the treated animal . 
of 1 : 2 : 5 : 6dibenzanthracene per rat usually results in very little growth inhibition for about 14 days , after which the animals , at varying intervals , lose weight rapidly and die . 
1. received for publication july 1 , 1948 . in the course of experiments on a transplantable mouse sarcoma it was observed that fresh saline extracts of tumour tissue agglutinated mouse and rabbit red cells . 
when extract and red cell suspension were mixed on a slide agglutination became visible to the naked eye within 30 seconds and appeared to be complete within 2 minutes . a number of different mouse and rat tumours , and a wide range of normal tissues , have been examined for haemagglutinating activity . 
when quantitative results were required a tube test based on that used by burnet and his co - workers ( burnet , beveridge , mcewin and boake , 1945 ) was adopted . serial two - fold dilutions of tissue extract were made in calcium - saline in round - bottomed tubes of approximately 0 - 8 cinternal diameter . 
of a 2 per cent suspension of washed red cells in calcium - saline ; the tubes were then shaken and allowed to stand at room temperature for 20 - 30 minutes . 
a preliminary reading of the end - point could then be made , if a quick answer was needed , which did not differ by more than one place from the final reading . calcium - saline , 0 - 3 c.c. , was then added , the tubes were shaken and allowed to stand a further 1 hours at room temperature , when the final reading was made . the type of agglutination , and also of the deposition of red cells in saline controls , varied with species . 
mouse cells seldom , and rabbit cells hardly ever , gave the compact button of deposit which is typical of unagglutinated fowl or human cells , and which workers with influenza virus haemagglutination take as negative . rabbit cells , in the absence of an agglutinating agent , settle in a round - bottomed tube as an ill - defined deposit surrounded by a slightly granular film , which would be regarded as evidence of agglutination of fowl cells . resembles closely the " shield pattern " which has been described ( burnet and stone , 1946 ) as typical of agglutination of fowl cells by lipoids . 
proved a it was effective in low concentration ( 0.005 m ) , very satisfactory preservative . and though it increased slightly the granularity of deposits of red cells in control tubes , it had no haemagglutinating action which could be confused with that of tumour extracts , even in concentrations much higher than this . it was slowly lytic for mouse red cells ( though this did not interfere with tests read after the usual period of two hours ) but not for those of other species . 
a final concentration of 0 01 m ( 0 12 per cent ) was generally used ; this was conveniently obtained by adding to a tumour extract 1 / 50th of its volume of a saturated aqueous solution of b.a.l. 
brought about regeneration of the activity of inactive extracts to their original titre . this regeneration was progressive : some activity was apparent in a previously inactive extract a few seconds after the addition of b.a.l. , but the full titre was not reached for about an hour , at room temperature . table i shows the preservation by b.a.l. 
fowl cells of each type , distinguished by a previous test against kahn antigen , were included in this test . it will be seen that rabbit cells were agglutinated by the tumour extract to lipoid agglutinable and far higher titre than those of any other species tried . lipoid non - agglutinable fowl cells were agglutinated to the same low titre . tumour extracts varied somewhat with regard to the ratio between titres for the titre for rabbit different red cells , but these variations were not constant . cells was always between 4 and 16 times the titre for mouse cells . extracts treated in various ways , to be described later , were tested in most cases against rabbit and mouse cells . 
red cells which were agglutinated to low titre by c57 were inagglutinable by s37 extracts . extracts of all the tumours tested lost their activity on standing , though at varying rates , e.g. 
extracts of c57 sarcoma took about 24 hours to become inactive , but extracts of c57 / lh1 , sarcoma , though initially often of similar titre , became inactive in one hour , or less . the loss could be prevented , or reversed , by the addition of b.a.l. occurrence and distribution of haemagglutinating agent in normal tissue . extracts of mouse liver , spleen , kidney , heart , lung , brain , voluntary muscle , lymph gland and thyroid , derived from both normal and tumour - bearing mice , were found not to agglutinate mouse red cells ; and for a time it was thought that the haemagglutinating agent was confined to tumours . examination of a wider range of normal tissues , using rabbit as well as mouse red cells , showed that this was not so . extracts of several tissues , notably adult mouse testicle , ovary , uterus and voluntary muscle , as well as whole mouse embryo and placenta , agglutinated the haemagglutinating rabbit red cells and sometimes mouse red cells also . titres of these extracts were , in general , low compared with those of extracts of mouse sarcomata , but comparable with those of extracts of some of the other table iv gives the range of haemagglutinating titres for tumours examined . rabbit , mouse and human red cells , of a number of normal tissue extracts . haemagglutinating power of these extracts declined on standing , and was preserved , or regenerated , by the addition of b.a.l. 
0 - 01 m added after standing 22 hours at room temperature figures represent reciprocals of haemagglutinating titres for rabbit red cells . some other properties of the haemagglutinating agents of tumrnours and normal tissues . action of normal serum on haemagglutination . - haemagglutination by lipoids is inhibited by normal serum in high dilution , while haemagglutination by viruses is unaffected by normal sera , but inhibited by specific antiviral sera ( burnet and stone , 1946 )  . the effect of normal horse serum on haemagglutination by tumour and normal tissue extracts was tested . extracts were mixed with equal volumes of a 1 in 100 dilution of horse serum , and the mixtures tested for haemagglutination in the usual way . 
an experiment similar to the last showed that addition of either of these sera had no effect on haema gglutination by either c57 or s37 sarcoma extracts . effect of temperature at which the test is performed on haemagglutination . 
than at room temperature ( stone , 1946 ; burnet and stone , 1946 ) , while haemagglutination by influenza virus is more active in the cold than at room temperature or 37 c . 
 ( salk , 1944 )  . haemagglutination by extracts of c57 and s37 sarcomata , and of normal mouse embryo and adult uterus , was tested at approximately 4 c . , at room temperature , and at 37c . 
overnight. neither rabbit nor mouse presence of complement had no detectable effect : cells were lysed and their agglutination by the tumour extract was unaffected . absorption of haemagglutinating agent by red cells . - - c57 sarcoma extracts were absorbed with rabbit , mouse , and fowl red cells , under various conditionts . the following is a representative experiment . samples of 20 per cent extracts of c57 sarcoma , ( i ) fresh , i.e. 
for three hours , and centrifuged ; the supernatant fluids were removed and the cells finally resuspended in the original volumes of saline , and examined for persistent agglutination and for agglutinability . 
fowl cells , which were only very slightly agglutinated , did not absorb appreciably . in all except one case red cells agglutinated during absorption were unsuitable for subsequent tests for agglutinability because they remained agglutinated . the exception was mouse cells used to absorb fresh extract . these , though agglutinated in the presence of the extract ( 30 minutes at room temperature ) redispersed during the subsequent incubation with saline . 
the difference is probably quantitative . gross ( 1947 ) has reported the presence of haemolytic agents in several tumours . haemolysis by such an agent , if of low titre , would be active only in the first one or two tubes of a haemagglutination test and , since these contain only 1 / 450th of their volume of packed red cells , haemolysis might be masked by the small amount of haemoglobin present in all crude tissue extracts . 
had been added before , and those to which it had been added after , heat treatment . a heavy precipitate formed in the heated extract , which was spun out before testing for haemagglutinating power , and it was thought possible that the haemagglutinating agent might be adsorbed on the precipitate . however , no agent could be recovered by extracting the precipitate with m / 15 na2hpo4 . the effect of digestion of tumour extracts by trypsin or papain depends on whether they contain b.a.l. in the absence of b.a.l. , extracts of c57 , or of c57 / lh1 , sarcoma incubated at 37 c . with trypsin or papain ( activated with kcn ) for an hour , were found to be irreversibly inactivated , i.e. 
0005 m 0 - 01 m + , , trypsin 0.5 per cent of commercial powder ( hopkins & williams )  . all mixtures buffered at ph 8 with m / 15 phosphate , 2 drops of chloroform added as baoteriostatic ; neutralized , and b.a.l. 
0.005 0 ' 01 m casein was " light , soluble " of british drug houses , dissolved in m / 15 na , hpo , by heating relevant conditions as in a . 1 hour on a water - bath . it will be noted that there was a considerable irreversible drop in titre of a control sample of sarcoma extract incubated without b.a.l. 
to such extracts gradually falls . it seems probable that this effect is due to the action of tissue proteases . the effect of tryptic digestion on extracts of normal mouse tissues was also tried . it is difficult to obtain such extracts with haemagglutinating titres high enough to make this test satisfactory . in an experiment in which a mouse embryo extract with a haemagglutinating titre for rabbit cells of 1 : 4 was digested with trypsin , with and without b.a.l. , activity appeared to be destroyed in 1 . 
on proteolysis was a 20 per cent extract of c57 sarcoma in m / 15 phosphate buffer ph8 was incubated ( a ) alone , ( b ) with trypsin , ( c ) with trypsin , and b.a.l. 
they show that , with casein as substrate , after 1 hour 's incubation there was no detectable inhibition of proteolysis by b.a.l. ; but with both casein and tumour extract as substrates , after 21 hours ' incubation there was definite inhibition : about 50 per cent by b.a.l. 
elliott , on the haemagglutinating power of a tumour extract , with and without b.a.l. , was essentially similar to that of commercial trypsin . the haemagglutinating agent does not become dialysable through cellophane after digestion of a b.a.l. - containing tumour extract with trypsin . lecithinase : it has been shown by stone ( 1946a ) that the haemagglutinating action of lipoids , and of vaccinia and ectromelia viruses , which probably owe their haemagglutinating action to lipoid components , is destroyed by cl . 
to 0 01 m was then added , and haemagglutinating in a similar experiment mouse embryo extract was treated with the results showed that incubation with lecithinase had no detectable effect on the ' ' haemagglutinating agents of c57 sarcoma or mouse embryo extracts . haemolysis by lecithinase present in the mixtures was not rapid enough , in the presence of b.a.l. , to interfere with haemagglutination . action of heavy metals and oxidizing agents , and its reversal by b.a.l. 
to samples of fresh , actively haemagglutinating , sarcoma extract , not containing b.a.l. , cus0o4 was added , to give final concentrations of m / 300 and m / 3000 . in both mixtures haemagglutinating activity disappeared within a few seconds ; there was a partial return of activity in the later , but none in the former , after addition of b.a.l. 
the haemagglutinating activity of these mixtures declined on standing at the same it thus appeared that the presence of heavy metals rate as that of a control . was not essential for natural inactivation . the addition of various oxidizing agents to a fresh sarcoma extract destroyed or reduced its haemagglutinating activity . 
the list includes serum antibodies ( naturally occurring , acquired , or experimentally induced ) , many viruses ( hirst , 1941 ; nagler , 1942 ; burnet , 1945 ; lush , 1943 ; burnet and stone , 1946 ; mills and dochez , 1944 ) , purified lipoids ( stone , 1946b ) , bacterial extracts ( keogh , north , and warburton , 1947 ) , the globulin fraction of egg - white ( commission on acute respiratory diseases , 1946 ) , some plant proteins such as ricin and abrin , basic proteins such as protamines and histones , inorganic colloidal acids and bases such as colloidal silicic acid , and many metallic salts ( landsteiner , 1945 )  . 
they are labile , while the latter are both fairly stable substances ; their red - cell species specificity is different from that of both lipoids and viruses ; they are unaffected by cl . 
welchii toxin , which destroys the haemaggluthinating power of lipoids and of vaccinia and ectromelia viruses ; their action is unaffected by normal serum , which inhibits that of lipoids but not that of viruses . in the manner in which temperature affects haemagglutinating titre they differ from lipoids . 
a sarcoma extract is absorbed by red cells which it agglutinates , but the cells , when they redisperse , as they do under certain conditions , are fully agglutinable by the same agent ; red cells agglutinated by a virus may also redisperse , but are then inagglutinable by that virus , and often by some others also ( burnet , beveridge , mcewin and boake , 1945 )  . egg - white is more like the tissue extracts in its haemagglutinating properties than are the other haemagglutinating substances referred to , particularly in respect of red cell species range , and effect of temperature on haemagglutinating titre , but it is not - reported to be labile . the general properties of the haemagglutinating agent of tumours suggest that it is a readily oxidizable substance which is active only in the reduced state . it may be a sulphydryl compound , but there is at present no positive evidence of this . neither inactivation by heavy metals , nor by oxidizing agents , is conclusive on this point . 
ascorbic acid , are ineffective , suggests that preservation is a specific effect of sulphydryl . natural inactivation does not appear to depend on the presence of heavy metals in an active state , and therefore it is unlikely that its prevention by b.a.l. 
has been stated not to inhibit the action of trypsin or papain ( webb and van heyningen , 1947 ) , but this work has been repeated here , with a it has been shown that b.a.l. 
protects it from the former . certain physical and chemical properties of the haemagglutinating agent of reasons are given for regarding it as an easily oxidizable it is destroyed by proteolytic b.a.l. 
was found to have definite inhibitory action on proteolysis by trypsin , the haemagglutinating agents of tumours and of normal tissues differ from and on digestion of egg - yolk by lecithinase . haemagglutinating viruses and lipoids in important respects . no qualitative differences have been found between the haemagglutinating agents of different tumours , or between those of tumours and normal tissues . the author gratefully acknowledges his debt to professor j . 
sterile vials , each containing 0 - 7 g . of a mixture of the sodium salts of the four nucleotides of yeast ribonucleic acid preserved with 0 - 3 per cent cresol . the mice used were the f1 cross of the a and c 57 lines . these were chosen because a mice have a relatively high spontaneous lung tumour incidence ( bittner , 1939 ; heston , 1940 ) , and it has been observed that such strains respond more readily to the carcinogenic effect of urethane ( cowen , 1947 )  . 
the hybrids would also tend to have a high spontaneous incidence , since the inheritance of spontaneous lung tumours in this cross seems to be due to a single dominant gene ( bittner and little , 1937 ; bittner , 1938 )  . seventeen a x c 57 males approximately two months old were injected with the pentose nucleotides solution subcutaneously at the flanks , daily at midmorning . 
of pentose nucleotides for a week the water . mice started to show ill effects . both treatments were discontinued ( after 2 weeks of pentose nucleotides and 1 week of urethane treatment ) for two days , on resuming treatments the dosage of pentose nucleotides to rest the mice . was decreased to 0 - 3 c.c. 
the figure clearly shows that a marked inhibition of the carcinogenicity of urethane was produced by the pentose nucleotides . the average number of lung tumours per mouse caused by urethane in controls 1 and 2 separately was 46 in each case , which was reduced to 26 in the p . 
strong. from the school of medicine , yale university , u.s.a. received for publication february 2 , 1949 . the idea of somatic mutation as an explanation for the origin of cancer has had a long and interesting history . its original use as an interpretation of cancer is usually associated with the names of murray and of boveri . these men arrived at the somatic mutation conclusion from different fields , murray from experimental cancer research , and boveri from his classical observations in experimental embryology . 
at that time he stated : " the existence of such tumours , the biological characters of which are retained through long periods of propagation , shows that the cellular transformation which initiates carcinomatous growth may take place in varying degrees . 
1 , the method of analysis employed compensates fully for difference in " size " of the pattern analysed , and the p values for grade and intergrade patterns can therefore be regarded as strictly comparable . if we regard p < .05 as evidence of abnormal patterning , then a glance at the table shows that abnormal patterns occur with considerable frequency . this is best seen by comparing the frequency distribution of the 224 grade and 192 intergrade p values of the table with the strictly equivalent frequency distribution of the 4000 random series ( cruickshank , 1940 )  . 
1. statistical maps often present data by the use of " grades . " the several counties in any one grade may be scattered " at random " over the map , or may be juxtaposed to form small or large these varying types of distribution are described briefly as " patterns . " the exact " groups . " type of pattern to be expected from random distributions has been determined experimentally ( 4000 patterns ) , and from these experiments the " expected frequency " of any specific type of rare types of patterns , i.e. 
patterns with low expected frequency , are observed pattern is known . described as " highly developed . " on cancer maps highly developed patterns occur with excessive frequency . indeed , " statistically significant " patterns , i.e. 
2 and 4 will show that p values across the gradings ( 1 - 12 - 1 - 23 7 ) give rise to curves with clearly defined trends , which include the develop114 d . 
2. the " intensity " of a regional influence can be expressed in terms of the " degree of development " of patterns found within its zone of action ; the more non - random the pattern the more powerful the influences at work . the analysis is best shown graphically ; the expected random frequency of the 7 grades and 6 inter - grades patterns of each map are plotted out on an i * erted logarithmic scale so that " peaks " show high degrees of pattern development - that is , powerful regional influences . the striking feature of the curves so formed is their essential simplicity . in fact they are almost e.g. 
that a significant " zone " is not always associated with a significant peak . in such cases the individual counties of the zone each show a deviation from the mean > 2 s.e. 
that curves of type 2 which develop a peak before the extreme grades and then fall off are usually associated with maps in which the highest ( or lowest ) grades do not form a single zone , but break up into two or more sub - zones , e.g. grade 7 may appear as three separate zones , unrelated to each other , but all related to grade 6 ,  . . 
the frequency of effects " increasing " and " decreasing " the rate are shown separately ; the frequency of effects " modifying " the rate ( significant ] y ) is the sum of these two . in the absence of regional influences we anticipate that a county will participate in " random " significant pattern formations in about 1 / 20 cases , i.e. 
 ( stocks ' data )  . now , if the distributions and trends in each of the 28 maps are unrelated , the result of combining these inter - random distributions should be to flatten out the whole pattern ( irregular multiple hillock picture )  . 
on the other hand , if they are related , their combination may be expected to result in some definite composite pattern or configuration ( hill and valley picture )  . from the entries of table vii three contour maps were prepared ( appendix 7 ) ; these are shown in fig . 
we may therefore conclude that county boundaries have no essential significance in relation to regional influences . in fact these influences behave in every way as continuous variables , and their variations in intensity are most appropriately depicted by means of contour - lines on the surface of the map . to depict these regional influences by contours may serve to drive home another of their characteristics as revealed by this study , viz . 
cornwall , somerset and dorset . while the majority of counties meet at a common county boundary , occasionally they meet only over a very narrow range , the so - called " point contacts " ( solid circles on map )  . 
where the county boundary is a river or an estuary the counties may fail to make a de facto cantact , and yet , it may be necessary to consider these as " touching " for the purpose of studying regional influences ( solid rectangles on map )  . note the distinctly higher values of the contact numbers of the inland counties as contrasted with those of the coastal counties . the mean contact number ( c ) works out at 5 - 12 . , , ~n this is an important constant in theoretical formulae , e.g. 
mark on the glass with grease pencil all " grade 1 " counties . remove glass template and place on white sheet . analyse arrangement of marked counties ; record ; clean off wax pencil mark with chloroform . replace on map and proceed similarly to work and analyse " grade 2 " counties , and so on . 
8 , in conjunction with appendix 4 , indicates the probable , simple explanation , viz . that estimates of the degree of pattern development of an organized pattern must generally fall below the true value when they are based on the examination of only part of the pattern - for the simple reason that the relation of one " piece " of the pattern to a neighbouring " piece " is thereby overlooked . 
the process of " intergrading " was evolved to deal with this contingency . thus , to explain the observed fact that the p grade greater than p intergrade we must assume that the mean " pattern " associated with regional influences covers an area greater than that of a mean grade , i.e. 
regional influences decreasing cancer exist alongside the " positive , " in fact these two types of influence , both of which are represented by peaks and zones , occur with equal negative effects must not be regarded as merely due frequency ( table vii )  . to the absence of positive effects , for the observed type of trend and degree of patterning associated with negative zones is of a much higher order than is to be expected from the mere absence of positive effect . it seems that there must be some general factor other than regional which operates to produce a definite incidence of cancer . regional influences are not themselves the cause of cancer , but merely impress their effect , positively or negatively , upon this general factor . i wish to express my thanks to n . 
the substance , usually dissolved in tyrode saline , is added to a culture after a dividing cell in mitosis therein has been selected fgr study , and the reaction of that cell to the agent is recorded for a period usually less than one hour . 
the cells in prophase then to be found in the outgrowth of the stained cultures were subsequently counted . the effects on mitosis of three phosphorylated naphthohydroquinones have been studied in this work . these are as follows : 1 . 
the di - methyl compound was found to be slightly less active than synkavit as a mitotic inhibitor in vitro . it again potentiates the effects of irradiation . further work on this substance is in progress , including clinical trials . normal mitosis in the chick osteoblast . osteoblasts were chosen for this work on the grounds that clear phase contrast pictures of them can be obtained during mitosis , and that they appear to be much less sensitive to light than are other fibroblast types of chick cells . in previous papers there has been described the normal course of cell division which can be observed under the phase - contrast microscope in living osteoblast cultures ( hughes and fell , 1949 ; hughes , 1949b )  . 
the nucleoli and nuclear membrane disappear remarkably rapidly at the end of prophase , but while the spindle is being formed several minutes pass before the chromosomes assume their equatorial position as a metaphase plate . it is convenient to speak of all this period after the loss of nuclear membrane and nucleoli as metaphase , and to separate an early from a late division of this phase of mitosis , respectively before and after establishment of the metaphase plate . the general cytological effects of compounds , i , ii , and xx viii . in the present work over fifty film records of the behaviour of dividing cells under the influence of these substances have been made . 
20. - cell from the outgrowth of a culture treated with 5 x 10 - 7 m synkavit ( i ) for 40 cell has undergone mitosis with the suppression of cleavage . 
nucleoli still present 5 mlater ditto , ditto , 10 mlater 3.5 x 10 - 6 m metaphase metaphase plate metaphase late prophase early metaphase 4 x 10 - 6 m prophase . 
the methylfree substance exerted this effect in late telophase over a range of dilutions of about one thousand - fold ( 27 , 3 x 10 - 9 m ; 36 , 1 x 10 - 6 m )  . 
at higher concentrations the substance rapidly kills both dividing and resting cells ( 38 , 1 x 1o - 5 m )  . it is noteworthy that although the effect of the methyl - free compound differs considerably from those of the methylated derivatives , both in the types of inhibition and the dilutions at which they are exerted , yet in the present data there are no significant differences in the maximum concentrations of each of the three substances at which a cell has been observed to undergo a normal mitosis ( synkavit , 17 , 18 , 19 ; di - methyl compound 25 , 26 ; non - methyl 36 , 42 )  . one point in the mitotic cycle on which these three substances do not appear to exert any immediate effect is the entry of cells into prophase . early prophases are still found in cultures treated with these substances at the highest concentrations which have been used in the course of this work . since synkavit and the di - methyl compound can interfere with the division of a cell in several ways , a culture which has been treated with these substances at appropriate dilutions for periods of an hour will show a variety of effects . these depend both on the individual sensitivity of the cells and the phase of mitosis which they had reached at the time of adding the substance . 
the fate of a particular cell selected for photography is , therefore , to some extent a matter of chance . it may be that the 55 instances which are recorded in table i do not exhaust these possibilities , though study of the whole cultures after fixation has not so far revealed any other types of inhibition . the variability of the behaviour of cells towards these substances , however , extends further than to inhibition at different stages of mitosis . treatment of a culture with a concentration sufficient to arrest and damage some dividing cells will leave unaffected others which continue a normal mitosis . this fact can best be illustrated by comparison of the effects of synkavit in a number of instances where it was applied to cells early in.prophase. 
at 1 x 10 - 6 m a normal mitosis ( 59 ) , an arrest in metaphase ( 60 ) and a clumping of chromosomes and cell oedema at this stage were recorded ( 52 )  . 
when the di - methyl compound at 4 x 10 - 6 m was added to cells in metaphase , there were seen both a normal mitosis ( 26 ) and an instance of clumping of the chromosomes ( 24 )  . this circumstance must be borne in mind in the search for any further generalisations from however , one other conclusion clearly emerges , namely , that the these data . effect of these substances on dividing cells is greater when they are applied at early stages of mitosis . 
with synkavit at 3 * 5 x 10 - 6 m addition to a cell early in metaphase resulted in clumping of chromosomes and oedema ( 15 ) , while later in metaphase in two instances this concentration was not found to be inhibitory ( 18 , 19 )  . 
it is probably true to say that phase specificity is most marked with substances to which the cell in division is much more sensitive than during the restthus , for instance , the action of colchicine on the dividing cell is ing stage . restricted to its effect on the mitotic spindle , and this is exerted at dilutions much greater than those necessary to affect intermitotic cells . 
the proportion of cells entering prophase thus , this substance appears to penetrate the cell memhas then decreased . brane so slowly that a concentration within the cell sufficient to provoke these effects is not reached for several hours . 
the secondary fusion of the daughter cells in late telophase which has been observed in the course of the present experiments may well be due to an alteration in the properties of the cell surface . 
a large number of binucleate cells were seen in stained cultures after treatment for 6 hours with this substance at concentrations of 1 x 10 - 9 m . this effect may be due either to secondary fusion of the daughter cells , or to an inhibition of cell cleavage in the first instance . finally , the value of the two general methods of investigations of the action of chemical substances on living cells in culture can be compared . in the one mainly used in the present work the effects of the agent on a single living cell in the culture is followed ; in the other a quantitative analysis of the whole culture is made after fixation and staining . 
where the effects of a given treatment often differ from cell to cell , it would be unwise to draw here the quantitative conclusions from the study of only a few examples . analysis of large numbers of cells is indispensable . 
cells may be inhibited at any point in mitosis , though their entry into prophase is apparently unaffected under the conditions of these experiments . arrest in metaphase and clumping of the chromosomes is the most common effect . individual cells vary greatly in their sensitivity to these substances . 
at sub - lethal concentrations the latter does not affect the course of mitosis until late in telophase , when to a varying extent the daughter cell re - unites . we wish to thank a . 
stern. from the general hospital , northampton . received for publication june 12 , 1954 . although a study of the morbid anatomy of carcinoma of the bronchus can have little bearing on the important problem of etiology , nevertheless any ascertainable facts about this increasingly common disease may contribute something to our knowledge of it . recent comprehensive surveys of the pathology of carcinoma of the bronchus have been made in this country by harrison ( 1950 ) , on 353 confirmed cases seen at st . 
the average age at which death occurred was 56.4 years , slightly higher in males ( 56 - 7 years ) than in females ( 54 - 7 years )  . 
on the other hand both willis and bryson and spencer found metastases in the adrenals much more often than they were discovered ( willis 40 per cent , bryson and spencer 23 per cent , present series in this series . 13 - 7 per cent )  . 
the frequency with which cerebral deposits have been recorded in carcinoma of the bronchus has varied widely with different observers . those who have investigated metastatic tumours in the brain have found that a very high proportion of these had their primary source in the lung . elkington ( 1935 ) , who analysed the records of the national hospital for the period 1918 - 1933 , found that of 72 metastatic cerebral tumours , 24 ( 33 per cent ) originated in the bronchus . 
the highest recorded figure is that of fried and buckley ( 1930 ) , who recognized secondary cerebral deposits in other observers have given much lower figures : reingold , ottoman 41 per cent . and konwaler ( 1950 ) 30 - 5 per cent , willis ( 1952 ) 21 per cent , bonser ( 1934 ) 16 per cent , harrison ( 1950 ) 20 per cent , bryson and spencer ( 1951 ) 17 per cent , simpson ( 1929 ) 13.5 per cent ( in a series of 139 cases ) , kilkuth ( 1925 ) 12 - 6 per cent ( in a series of 246 cases )  . few authors have differentiated between multiple cerebral deposits from carcinoma of the bronchus and large single masses except to say that the former are common and the latter rare , though kilkuth ( 1925 ) reported single masses in 13 of 31 cases with cerebral metastases . although the present series is small it is noteworthy that in 14 cases with cerebral metastases only 6 were multiple and 8 single . 
the multiple deposits were widely distributed and showed no predilection for any particular area of the in all except one of the cases with multiple cerebral metastases there were brain . also secondary deposits in the viscera . 
on examination there was a complete hemiplegia and a dubious hemianosevere neck rigidity was present , but examination of the cerebro - spinal fluid revealed pia . a normal fluid except for pressure , which was 190 mthe only abnormality disclosed by examination of the chest was diminished air entry in the upper zone of the left lung with deviation of the trachea to the lethe differential diagnosis made was betweenr tuberculous encephalitis and cerebral thrombosis . 
death took place 2 days after admission . at post mortem dense fibrous adhesions were found almost completely to obliterate the left pleural cavity . there were old fibrous adhesions at the right apex . 
the trachea and arising from , and producing main bronchi contained a considerable amount of muco - pus . almost complete obstruction of the left upper lobe bronchus was a hard , white tumour , distal to this tumour the lobe was collapsed and contained approximately 5 cacross . a number of irregular cavities filled with thick yellow pus . 
the left lower lobe was studded with a number of nodules of tumour up to 0 ' 5 cacross . in the upper half of the right upper lobe there was an irregular tuberculous focus 2 cacross consisting of a central caseous mass enclosed in dense fibrous tissue . 
her main complaint was loss of weight and a cough of 3 months ' duration , which had been accompanied by a blood - stained sputuon examintion the fundi could not be seen . 
an x - ray showed a mass extending from the left hilum and involving the mid and lower portions of the left upper lobe . the patient died 12 days after admission . at post mortem a large , white , firm tumour mass was found involving the whole of the medial portion of the upper lobe of the left lung . 
no mediastinal glands were infiltrated and no other deposits were found in the viscera . the skull was normal , but attached to the flax cerebri at the vertex of the brain , and pressing on the pre - rolandic portion of the left superior frontal gyrus there was a firm hard tumour the size of a cherry ( proved histologically to be a meningioma )  . the cerebral convolutions were somewhat flattened . 
onimmediate examination a weakness of the left face was noted and there was slow nystagmus on lateral and upward deviation of the eyes . the reflexes were all exaggerated but the plantar responses were flexor . a diagnosis of cerebral tumour was made tentatively , but before further investigations could be carried out the patient died suddenly the day after admission . at post mortem a fungating , cauliflower - like growth was found in the upper lobe of the left lung . 
no enlarged mediastinal glands were present . the pelvis showed no evidence of any local or secondary lymphatic involvement from the cervix . the brain was moderately congested and oedematous . the left half of the cerebellum was replaced by a degenerating , cystic tumour . histologically the growth in the lung and the secondary deposit in the cerebellum were found to be an unspecified type of carcinoma of the bronchus . ( sections were not available for personal study . ) chronic bronchitis " and convulsive attacks with loss of consciousness which began a fortnight before admission . six months previously , when he had attended hospital as an out - patient , an x - rayhad been suggestive of bronchial neoplasm , with displacement of the mediastinum to the right side . 
the cerebro - spinal fluid was normal apart from an increased pressure of 250 man x - ray of the chest gave evidence of neoplastic formation in the left hilar region with associated collapse at that base . death occurred 3 days after admission . at post mortem the left lung was found to be collapsed and the left pleural cavity contained about 500 c.c. 
the left main bronchus was compressed by a soft , buff - coloured tumour , about 8 cin diameter , which was covered by a layer of lung 2 cm . this layer of lung was relatively airless and thick yellow pus was expressed from the thick . the oesophagus and aorta were displaced posteriorly by the tumour . 
46 on account of frontal headaches , throbbing in character and especially severe in the mornings , which had been present for 3 weeks . just before admission much nausea and vomiting had developed . there had been no cough at any time . 
the arm and leg sides . reflexes were normal , but some past pointing was noted in the right arlumbar puncture gave a yellow fluid under 300 mof pressure . the protein was increased to 120 mg . 
the patient deteriorated rapidly and died 3 weeks after admission . at post mortem a hard , white tumour , 1 in diameter , was present at the apex of the right lung . 
no abnormalities were found in the abdomen . in the brain there was a secondary deposit , just over 1 in diameter , deep in the left temporo - parietal lobe . the mass impinged on the left lateral ventricle , which was slightly dilated . 
a mixed type of types of cells encountered in these tumours were : alveolar cells and oat cells , 4 cases ; alveolar cells and polygonal cells , 2 cases ; and one case each of spheroidal cells and squamous cells ; polygonal cells and oat cells ;  . 
the alveolar epithelium in this particular graft actually shows the various stages in the secretory cycle of the normal prostatic gland . it is interesting to compare the histology of these successfully vascularised grafts seen in fig . 
horning the prostatic it is relatively easy to detect by palpation non - vascularised grafts , as they are smaller and invariably softer when compared with successfully vascularised prostatic grafts , which are firmer on palpation , larger and invariably cystic in the earlier phases of growth , owing to active secretion of the glandular epithelium . non - vascularised graft fixed5fig . 
in this particular implant this was the only malignant focus within the entire graft . alveoli distended with secretion and with normal epithelium are seen adjacent to this exhausted alveolus from which this early malignant lesion arose . 
the proliferating epithelial components in all the early malignant foci break through the alveolar basement membrane , invariably forming tongue - like lesions which rapidly invade the fibromuscular stroma of the host as depicted in all prostatic grafts which have grown after treatment with 20in fig . 
10. methylcholanthrene , it was found possible to distinguish between three distinct types of early epithelial growth , all of which have been previously described in detail ( horning , 1949 )  . by studying the cytology and mode of growth in serial sections of these early invasive foci through later phases of development in other similar older grafts , it has been possible to predict the types of tumours which would have subsethere is one type which gives rise to a glandular carcinoma , quently arisen . both these types of and a second which develops into a squamous growth . lesions are easily recognised by their histological character , and both arise from the alveolar epithelium . the third type is the most uncommon variety , characterised by a stratified squamous metaplasia of the epithelium in sita , followed by a diffuse marginal growth into the stroma , which clearly arises from the duct occasionally some grafts show two or sometimes three types of epithelium . proliferating foci within the same implant . 
11. this shows a section of a graft treated with crystals of stilboestrol alone and fixed 4weeks after implantation . there is a complete inhibition of secretion after this period of grafting . every individual alveolus within the graft was entirely devoid of prostatic secretion , and the epithelial cells had undergone marked morphological changes . 
the prostatic epithelium at this period of treatment contrasts greatly with similar grafts treated with the female sex hormone after implantation in host mice for the same period of time . 
the alveolar epithelium not only maintains its glandular character , but in the majority of grafts testosterone propionate induces a pronounced stimulation of the prostatic secretions , invariably resulting in a cvstic dilatation of the alveoli . 
grafts combined with the carcinogen and sex hormones . 20 - methylcholanthrene and testosterone propionate . - three squamous - celled carcinomas developed from prostatic grafts impregnated with the carcinogen and the male sex hormone in strain a mice at intervals ranging from 7 to 9 weeks following implantation . one sarcoma arose in a c3h mouse after 8 weeks ( table i , group iii )  . 
the differences in histological structure between prostatic tumours derived from grafts treated with the carcinogen together with either the male or female sex hormone can best be appreciated by comparing fig . 
examination of pituitary and adrenal glands and gonads from host mice bearing grafts . examination of pituitaries from mice bearing grafts from all three groups of rodents treated either with the carcinogen alone or in combination with either of the sex hormones revealed no abnormal histological changes , with the exception of excessive amounts of colloid seen in the clefts of pituitaries from mice treated with stilboestrol and the carcinogen . there was no diminution of acidophiles or increase in chromophobe cells following implantation of the stilboestroltreated grafts . neither did the adrenal cortex reveal any histological abnormalities resulting from this treatment . 
horning of both lung and prostatic tissues have been previously described by the author in mice the survival of an homologous graft seems to be dependent ( 1949 , 1952 )  . upon the use of a closely inbred strain , since stock mice of indeterminate ancestry do not easily tolerate grafts of this kind . 
pan and gardner ( 1948 ) found an increased susceptibility to tumour formation from grafted uterine epithelium in pure line mice as compared with hybrids . recent experiments ( horning , 1952 ) have further indicated that the age of the donor providing the graft , and the age of the host mouse into which the grafts are implanted , also have an important bearing on the problem of graft other factors such as the reaction beween the graft and the host survival . mouse play an important role . it has been previously reported that more difficulty has been experienced in obtaining malignant tumours from lung grafts impregnated with 20 - methylcholanthrene than with similar grafts of other it was interesting to note that tissues which are normally under hormonal tissues . influence are much better tolerated as grafts in host mice of the same sex and strain than tissues which are to a greater extent ( such as the lung ) independent of hormone action ( horning , 1952 )  . nevertheless , a certain number of prostatic grafts , when implanted subcutaneously into host mice of the same strain as those of the donor , fail to survive irrespective as to whether the grafts were impregnated either with the carcinogen alone , or in combination with either the male or female sex hormone . 
the present experiments on the reaction between the implanted prostatic graft and the host bearing mouse have shown conclusively that the survival of the donor graft is dependent upon a rapid vascularisation within the subcutaneous tissues of the host mouse . 
the reason , however , why some grafts fail to become vascularised still remains obscure . the influence of steroid hormones on the behaviour and growth of prostatic cancer has been the subject of intensive investigation . 
1. - the skin of a c3h male mouse is cut and pinned back so as to expose an untreated homologous prostatic graft which had been growing subcutaneously for 6 weeks . 
6. - transverse section through an homologous prostatic graft which failed to become vascularised , fixed 6j weeks after subcutaneous implantation . the relationship of the grafted prostate to that of the skin of the host rodent is clearly shown . 
horning alveoli have completely broken down ; there is also evidence of lymphatic infiltration . the whole graft has been encapsulated and is slowly being absorbed by the tissues of the host mouse . 
meredith. from the christie hospital and holt radiumt institute , manhester . received for publication december 12 , 1948 . ix a series of papers ( dale , 1940 ; dale , meredith and tweedie , 1943 ) it has been shown that the action of x - rays on aqueous solutions of biologically active compounds was indirect , i.e. 
further , it has been shown that in consequence of this indirect action , if two solutes are present , the second solute ( the protector ) reduces the radiation effect on the first one ( the indicator ) ( dale , 1942 ; 1943 ) , by sharing the intermediate product formed from water by the radiation . 
meredith enon revealed certain unexpected quantitative relationships between the protective power of a substance and its concentration , which will be described and discussed in this paper , together with the closely linked ionic yield of the indicators used , the knowledge of which is the necessary basis for the quantitative treatment of the experimental results . 
the fact that these new results were derived from experiments with two indicators of very different molecular weight , for an extended range of protective substances added to both indicators , helps to build up a more complete picture than has been obtained hitherto . 
 ( average a 130xu ) from a 250 kv tube . whenever possible , the solutions , contained in pyrex glass tubes , were spaced at such distances from the target that each received the desired dose during the same overall treatment time , care being taken to avoid shielding of one tube by another . this ensures that the relative doses received by different tubes are not affected by unavoidable fluctuations in the tube output . 
the stock solution of enzyme and the solutions of protective substances were made up with water , glass re - distilled from alkaline potassium permanganate , and the ph adjusted so that a sample reacted pink to phenolphthalein . all necessary dilutions were carried out with glass re - distilled water adjusted to the same ph by the addition of 1 ml . 
were performed during this series of experiments , these arise because very high and some special difficulties were encountered . doses of radiation ( one to two million roentgens ) are required to achieve a reasonable degree of inactivation in solutions with concentrations of the order there is a strong tendenvcy of re - crystallization during of 10 per cent or more . the long exposure to radiation , which makes it almost impossible to keep the enzyme in solution at a ph compatible with its stability . however , it was found that a 6 per cent solution could be maintained for most of the time by stepwise addition of naoh . 
the concentration reached by this method was derived from the known concentration of the suspension by measuring the height of the coluimn of crystals after , and the height of the suspension before centrifugation . 
compound ( warburg and christian , 1938 )  . since various preparations ofthe specific protein of the amino acid oxidase differ in their activity , and even any one preparation gradually loses activity when kept for some weeks , the oxygen uptake with a known amount of d.n. 
1. these results may also be presented , as shown in a previous paper ( dale , gray and meredith , 1949 ) , by the formula : d5 - 2 x 107  . 
calculated by lea ( 1946 ) from earlier experiments by one of us is much lower than the value obtained in the horizontal part of the curve , and this is due to the fact that the concentration then used was of the order of ~~~i ~~~~~~~ii conc . 
for the sake of accuracy the degree of inactivation should be kept between the limits of 25 - 75 per cent . in a previous report ( dale , 1947 ) the value of q was found from the protection afforded by generally lo100 g . 
q was roughly constant , and it was concluded that the protective power per molecule is proportional to the molecular weight - perhaps not a surprising result , since all these substances have roughly the same average composition . it is only when low molecular weight substances of special chemical configuration are examined that remarkable differences are found . oxalic acid , which was earlier ( dale , 1942 ) found to be a poor protector of d.n. , also proved to be a poor protector in the case of c.p. , but if the c - c bond in oxalic acid is broken and the free valency of the carboxylic group linked to an h atom , thus forming formic acid , the protective power is raised about 200 times , and similarly , if w . 
our arguments , however , are not dependent upon its correctness , nor would they be invalidated by its disproof . lea , smith , holmes and markham ( 1944 ) pointed out that , in addition to reacting with solute molecules , radicals may also recombine with one another , having a mean life , as free radicals , of r sees . 
 ( 1944 ) also suggested a modification of equation ( 3 ) to cover the protection effect on the assumption that the indicator and protector molecules " share " the available radicals . 
thus although the protector molecule has removed a radical from the solution , it can " hand on " the effect of the radical to the indicator molecule , and thus fails to fulfil its since we have no clue to the nature of this change function as a protector . we will call it " activation , " and it might be thought of as a sort of meta - stable state . 
and the collision frequency between " activated " protector molecules and indicator molecules , 1 , m and pi have already been defined , whilst pa is the probability that a collision between a radical and a protector molecule destroys the former and activates the latter . 
ps is the probability of an indicator molecule being inactivated in a collision with an " activated " protector molecule . from equations ( 9 ) and ( 4 ) we findao + m rt [ ( ao + t ) pi ( ao + m ) pap . 
i ~~ ( ao + t ) p , + lp , apz~l ( 10 ) some of the constants appearing in equation ( 10 ) can be evaluated from results obtained with solutions of the indicator alone , whilst the others can be evaluated from any two experimental values of q for known protector concentrations . 
the values of ( p ) are indications of the protective power per molecule of each substance for the particular indicator , and the values given show the same tendency as was shown previously for protective power per unit weight by molecules with approximately the same atomic constitution have dale ( 1947 )  . approximately equal protective powers , whilst marked differences occur when special groupings are present . from the results it is also possible to calculate the relative values of pr for d.n. 
not only has the type of therapy most likely to achieve success been the subject of dispute , but also the same measures in the hands of well - known authorities have produced a wide variation in results . 
have we a classification which accomplishes this ? the outlook for a patient with cancer of the breast depends first and foremost upon the degree of malignancy of the tumour and upon its extent . 
it is a wide belief that the prognosis is also influenced by certain other features , but the value of these is open to que ! rtion and will form the subject of a separate inquiry . 
 suffice here to state that such factors as age of patient , site of tumour in the breast , size of primary growth and duration of symptoms were not found , per se , to influence the outlook materiallv . 
 _ - \ttempts have been made in the past to group patients with breast cancer according to histological criteria which , it has been claimed , give some indication as to the degree of malignancy of the tumour . 
 the other is based upon a system of grading , wbilst the results of the former have largely proved disappointing , conflicting views exist as to the value of the latter . 
 it is the prime object of this paper to investigate the significance of the grade of malignancy in mammary cancer in an attempt to establish a more accurate system of classifying patients with this disease . 
 there is great difficulty at the present time in deciding on the line of action to adopt in view of the widely different procedure . ; , advocated by different authorities . 
 , vhilst gordon - taylor ( 1948 ) and cade ( 1948 ) believe radical mastec tomy alone to be the most suitable treatment for these patients , riddell ( 1948 ) and also richards ( 1948 ) advocate ancillary radiotherapy . 
it is now over fifty , ears since : moore of london conceived and introduced the radica.l mastectom , ( rodman , 1904 ) , and still there is controversy in some quarters as to its valu ;  . 
 if we cannot solve the problems of mammary carcinoma , what hope is there for the surgery of malignant disease in less accessible sites ? pretw ' u , , 8 attempts at grading . 
 little attention was directed to the grading of tumours until broders ( 1920 ) applied , on hansemann 's theory to squamous cell carcinoma of the lip , and a year later to similar tumours of the skin ( broders , 1921 )  . 
 l\iaccarty and sistrunk ( 1922 ) and l\iaccarty ( 1922 , 1924 ) also studied the histology of breast tumours , and found the most important prognostic charac teristics to be the degree of cellular differentiation and the presence or absence of certain stromal features . 
 ' white ( 1927 ) was unable to agree with the views of : : \iaccarty , but in a series of 100 cases confirmed the results of greenough ( 1925 )  . 
 smith and bartlett ( 1929 ) , and lat.er simmons , wright , hartwell and greenough ( 1933 ) , also confirmed the value of the syst.em introduced by greenough ( 1925 )  . 
 the five - year survival rat.es for the three grades of malignancy obtained by these authors are comparable , and agree in the main with those of pat.ey and scarff ( 1928 )  . 
they therefore elaborated a " clinical index of malignancy " based upon age , presence of lactation , rat.e of growth of tumour , and extent ( stage ) of the disease . 
perry ( 1925 ) , lane - claypon ( 1928 ) , truscott ( 1947 ) and hamett ( 1948 ) were not able ti < > prove that the position of the growth had any bearing on outcome in breast cancer . 
 flothow ( 1928 ) , in a little over 200 cases of carcinoma of the breast , studied the facrors stated by llaccarty ( 1922 ) to represent a defensive mechanism by the body to a malignant tumour . 
it was shown that the malignancy increased with a rise in the " malignancy index . " for comparison a clinical classification was also elaborated by schmitz , but no att.empt was made to study the effect of correlating these histological and clinical syst.ems ( hueper and schmitz , 1929 )  . 
 opinions regarding the accuracy of hisrological grading have varied from huepe , r , who finds as many as twenty different features of prognostic value ( hueper and schmitz , 1929 ) , ti < > reimann ( 1929 ) , who is unable ti < > find one . 
he considers , however , the broad grouping methods based on general histological stucture - - presumably such as that of greenough ( 1925 ) - ro be of value . 
greenough ( 1925 ) , on the other hand , applying the principal of anaplasia , concentrated on tubule formation , variation in size of cells and nuclei , secretory activity and mitotic and hyperchromatic figures . 
 the principles laid down by greenough ( 1925 ) were closely followed by others , such as smith and bartlett ( 1929 ) , and simmons , wright , hartwell and greenough ( 1933 )  . 
patey and scarff ( 1928 ) and scarff and handley ( 1938 ) , however , attached chief importance to tubule formation , variation in size of nuclei , and mitotic and hyperchromatic figures . 
 delbet and mendaro ( 1927 ) in france , on the other hand , considered the presence or absence of mucous secretion to be the most important factor in ascer taining the outcome of patients with mammary carcinoma . 
leroux and perrot ( 1928 ) andmoureau and lambert ( 1932 ) support the views ofdelbet and mendaro ( 1927 ) , but betrand and de nagey ( 1931 ) consider muco - secretion to be of no value in determining clinical progress . 
 evans ( 1933 ) studied a number of parenchymal and stromal features , and con cluded that , although anaplasia indicates a poor prognosis , it is of no practical value in assessing the outcome for the individual case . 
he concluded that the grade of malignancy is the most important indication ot survival period , and this is more significant when considered together with the state of the axillary glands . 
 complicated , exact numerical systems , such as the " histological malignogram " introduced by hueper ( hueper and schmitz , 1929 ) , are time - consuming and of doubtful value . 
 the series taken for the present investigation consists of 565 cases of carcinoma of the breast treated at the middlesex hospital between the years 1936 and 1942 inclusive , and at the war sector units associated with it during the latter half of this period . 
in spite of the movement of population produced by the recent conflict , all but 11 of the c3888 were traced by the follow - up department of the hospital . 
 for the present study the five - year survival rate will be the chief prognostic yard - stick , though some attention will also be given to ten - year results . 
 " sur vival rate , " however , does not necessarily imply freedom from cancer ; it is in point of fact , merely an indication of the number of patients actually alive . 
this was based on the principles laid down by greenough ( 1925 ) , but chief importance was attached to tubule formation , regularity in size , shape and staining of nuclei and hyperchromatism and mitoses . 
this view is supported by the work of greenough ( 1925 ) , white ( 1927 ) , patey and scarff ( 1928 ) , smith and bartlett ( 1929 ) , sophian ( 1935 ) , and in fact , this is the only histological feature on which scarff and handley ( 1938 )  . 
certain authors , such as evans ( 1933 ) , greenough ( 1925 ) and haagensen ( 1933 ) , paid attention to variation in size of the cells , but the outlines of these are usually indistinct ; it is more reliable to consider the nuclei . 
evans ( 1933 ) was unable to support this view , and plaut ( 1927 ) considers the feature unreliable on the grounds that many cancer cells divide by amitosis . 
nevertheless , as haagensen ( 1933 ) points out , a considerab1 proportion of the cells in cancer of the breast divide by mitosis , and he found a close relationship between the number present and the outcome . 
this is also supported by the work of greenough ( 1925 ) , white ( 1927 ) , patey and scarff ( 1928 ) , smith and bartlett ( 1929 ) , sophian ( 1935 ) , and simmons , wright , hart well and greenough ( 1933 )  . 
 the cases were fairly evenly distributed , 30 per cent of the total being pla - oed in grade i , 41 per cent in grade ii , and 29 per cent in grade iii . 
 227 it is evident that a parallel exists between grading and prognosis , there being more than three times the number of patients alive with grade i than with grade iii tumours . 
it will be noted that they a . , , uree especially with the findings of pat.ey and scarff ( 1928 ) , and table ii . - - grade and prognosis by various authors . 
no grade iii cases remained alive in the series of greenough ( 1925 ) , and also of white ( 1927 ) , but this does not appear to be the general experience . 
 total 218 433 the five - year survival period is a convenient yard - stick with which to gauge prognosis in breast cancer , but as truscott ( 1947 ) and others have pointed out , a large number of fatalities from this disease occur from five to ten years after operation . 
 comparison of the fiveand ten - year results emphasizes the importance of the latter as a more accurate indicator of the control of mammary carcinoma , there being a striking fall in the numbers oi survivals for the corresponding grades of tumour , even with allowance for expected deaths from other causes . 
this is in keeping with the 26 per cent obtained by richards ( 1948 ) , and the 32 per cent by harring t - 0n ( 1946 )  . 
 ( i ) well - marked ( ii ) moderate ( iii ) slight or ml total ( i ) slight ( ii ) moderate ( iii ) marked y ariation in nuclei h : yperchromatic and mitotic  . 
the extent of the growth should also be taken into account , and the most important single factor indicating this is whether the axillary lymph nodes are histologically involved or not . 
it is particularly interesting to note that the prognosis in the lower grade of malignancy with glandular spread is better than for either the higher or intermediate grades without such metastases ( 65 per cent alfre at fi . , e years compared with 53 per cent and 61 per cent respectively )  . 
 these results agree in principle with those of most workers who have employed the system introduced by greenough ( 1925 ) , and are almost identical with the findings of simmons , wright , hartwell and greenough ( 1933 ) ( table viti )  . 
 patey and scarff ( 1928 ) and scarff and handley ( 1938 ) , on the other hand , found a uniformly good result in all three grades when the glands were not involved , and so concluded thatgrading is only of prognostic value in those cases with axillary metastases . 
the figures in table ix refer to the state of the cases at the time of operation , and the time factor involved here is the delay in seeking treatment . 
on the other hand , if for any reason the grade ill .cases tend to present for treatment after a longer interval of time than those belonging to grade i , then this may account for the greater incidence of axillary involvement in the former . 
in addition a higher percentage of the former present within six months of the onset of the disease and fewer after twelve months as compared with the grade i cases . 
thus , in spite of the shorter delay in seeking treatment , there is a greater incidence of axillary involvement among the high and intermediate grad~ of malignancy , consequently emphasizing the greater metastasizing power of these types of growth . 
ewing ( 1940 ) , however , prefers to employ the term " potential malignancy " for a neoplasm as determined by microscopic examination , because the clinical course may be modified by such features as site of tumour , surgical trauma and perhaps changes in rate of growth . 
 several authors , such as hueper and schmitz ( 1929 ) , and also lee and stiiben bord ( 1928 ) , have compared the results of grading and staging in breast cancer . 
 involvement of the skin directly over and in continuitv with the tumour does not affect staging provided that the area ~volved is small in relation to the size of the breast . 
as previously , when the cases were classified according to grade ( tables i , iv ) , a large number of deaths are seen to take place in the interval between the shorter and longer follow - up periods , thus once more emphasizing the importance of the latter in assessing the achievements of breast cancer therapy . 
 a study of grading and also staging indicates that both methods give com parable results ; the latter , however , has the slight advantage of revealing the outcome for the most advanced cases ( stage 4 )  . 
 we ha , e already drawn attention to the relationship in breast cancer between the histological architecture of the tumour and its tendency to involve the axillary glands ( table ix )  . 
exactly half of the grade i tumours have not yet extended beyond the first stage , whilst about a quarter are advanced , belonging to stages 3 or 4 taken together . 
 100 100 100 these results merely gi , e additional support to the view already expressed with regard to the relation between histology and axillary involvement , that the higher the grade of mammary carcinoma , the greater the tendency for early spread beyond the breast . 
the vast majority of workers in this field , however , have argued as to the relati , e merits of either syste but why should the grade and stage be considered only separately , and in the sense of competing with each other to form the basis of a reliable prognostic guide ? a combination of these features would result in a classification which gives information on not only the type of growth , but also its extent when first seen . 
would this not bring about a more accurate grouping of cases than could be produced by either system alone ? indeed , se , eral authors have taken the histological picture into consideration with the state of the axillary lymph nodes , and the value of this has been con firmed here ( table vii )  . 
the percentage of five - year survivors is seen to range from as high as 87 per cent for stage i , grade i cases down to as low as 6 per cent for those belonging to stage 4 , grade ill . 
it is also evident that whilst the prognosis in each stage deteriorates with the rise in histological malignancy , the cases with low grade tumours do not conform to the general trend . 
it reveals that all is by no means lost if a patient presents with a stage 2 or even a state 3 growth provided that it belongs to the lowest grade of malignancy ( grade 1 )  . 
 having revealed the value of combining histological grading with clinical staging for prognosis in mammary carcinoma , the suggestion is now put forward that the wide range in results produced by different authors for identical methods of treatment depends upon the comparison of incomparable groups of cases . 
 w ' hat evidence is there to support these views ? with reference to this question , two groups of cases will be taken for study , one treated by surgery alone , and the other by surgery with ancillary radio therapy . 
although it is not the purpose of this paper to discuss the merits of treatment in breast cancer , the results achieved by these two methods will be compared in order to illustrate the discussion . 
it must be pointed out that the treatment in each group was by no means uniform , there being considerable variation both from the surgical as well as the radiological aspect . 
 irradiation was predominantly in the form of deep x - rays , either pre - operati.e , post - operative , or both , a few cases being treated with radium alone or radium and deep x - rays . 
 according t - 0 grade . - let us first consider the results achieved for each group according to the grade of malignancy ( tables x " \ ' ~i , xviii )  . 
on the other hand , in the radio - surgical group , although this operation was performed in the majority , there were many instances of more conservative surgery , which included 37 simple mastectomies and 17 local excisions . 
 " ~ith this in view , the survivals of a more uniform type of therapy were taken for study , the comparison being made between patients treated by radical surgery alone and radical surgery with irradiation ( tables xxii , xxiit )  . 
 the greater achievement of surgery alone over the combined attack is again seen in harnett 's ( 1948 ) figures which are also for the radical operation and are classified by stages ( table xxi )  . 
 from these facts it is clear that the variation in treatment by surgery in the present material does not appear to interfere with the fair comparison of the 278 h . 
 in this instance a false impres sion may be given when the results of two series of cases are compared owing to the possible unequal distribution of clinical stages in corresponding histological grades . 
here there are small number of seen to be more low and fewer high grade tumours in each stage ot the surgical as compared with the radio - surgical cases . 
furthermore , of all the neoplasms of low grade malignancy ( grade i ) 57 per cent were in this surgical group in contrast to only 30 per cent of the highly malignant type ( grade ill ) ( table xxvi )  . 
what , then , may acco~t for this fact ? is it merely fortuitous chance , it is true , may play a part , but this is not the only possibility  . 
 .although two groups of patients are placed in the same clinical stage , there may be some difference in the extent of the growth for which no allowance is made in our present staging systems . 
in view of the parallel revealed between hist.glogical picture and extent of tumour ( tables ix , xiv ) , it is these unfavourable cases which also tend to be of high grade malig nancy , hence the distribution in fig . 
it i < ; , therefore , useless to compare results obtained by different authors if the cases are taken according to stage and no allowance is in this instance chance is probably the chief factor made for type of growth . 
however , cannot be ruled out , individual surgeons ha , ing , to some extent , personal criteria for deciding on the measures to be adopted for a given case  . 
.y egkcte , d , routes of extension . - reference will be made to avenues of extension of breast cancer which are largely neglected in both prognosis and also treatment . 
of these unfavourable grade iii cases nearly 70 per cent ( table xxvi ) were referred for irradiation , thus emphasizing the disadvantage placed on the radiotherapy group when it comes to the comparison of treatment results . 
 to sum up : it is postulated that in a given stage certain cases haw unfa rnur able clinical features , which influence the surgeon to refer them for radiotherapy . 
 the tumours of these patients tend to be of high grade histological malignancy , and h~ve probably also extended , ia routes , as yet , not given adequate considera tion in prognosis and treatment . 
this may account , at least to some extent , for the unfavourable results achieved here and elsewhere ( adair , 194& ; truscott , 1947 ; harnett , 1948 ) by ancillary radiotherapy . 
in these instances the achievement of radiotherapy is probably even greater than appears on first examination owing to the unfavourable features which tend to be present in cases referred for this treatment . 
 it has been pointed out that the problem of grouping also applies to series treated by identical methods , though here chance rather than selection is prob ably a more important factor accounting for the distribution of the patients . 
with this method it is hoped that further light may be thrown on some of the problems of breast cancer , and possibly the true merits of the various treatments of the disease assessed . 
 when this clinico - pathological system is applied here , will the results achieved by ancillary radiotherapy appear to be any better ? this question , unfortunately , 282 h . 
harries ( personal commanication ) , at the middlesex hospital , quotes 19 per cent for the five - year follow - up and 4 per cent for a period of ten years among some 220 cases . 
these figures are inferior to those obtained by treatment , which is universally accepted as being of definite , aloe in prolonging life , except perhaps in the very advanced cases . 
 once the cases are classified more accurately , such as on the lines indicated earlier in this paper , and only then , shall we be in a position to study the merits of , arious treatments . 
we may find , for example , that less radical surgery may be adequate for the control of certain cases such as those with grade i , stage 1 tumours , whilst radiotherapy may be an important ancillary measure for some cases , but on the other hand of little use for others . 
grace ( 1937 ) in america obtained a 56 per cent fi , e - year surrival rate among 40 cases treated by simple mastectomy and radio tht > rapy . 
this author considers that " the cellular structure of the tumour is the dominant factor in prognosis , and surgical technique , irrespecti.e of its radicalism , plays a definite secondary role . " some support tor this view is perhaps to be found in the paragraphs which follow . 
a group of 45 cases in his series were treated by local excision with implantation of radium , and 63 per cent were alive after a similar period of time . 
 what do these results mean ? can it be possible that more conservative surgical measures than the radical operation are sufficient for the control of mammary cancer ? such , indeed , is the view in this country of keynes ( 1937 ) , and more recently mcwhirter ( 1948a , 1948b )  . 
 we have already suggested that when cases are properly grouped accord.mg to both stage and grade it may be found that less radical surgery may be adequate for certain types of case . 
it is not even necessary to have numerous sections to appreciate this picture ; one or two portions of tissue of reasonable size taken from the periphery of the growth are adequate . 
 thus , patey and scarff ( 1929 ) , in a series of llo cases , found that the metatases in the axillary nodes were of the same grade as the primary in 82 per cent , of a lower grade in 16 per cent , and of a higher grade in only 2 per cent . 
comparable figures to these are also given by other writers , such as harrington ( 1935 ) , lach man ( 1944 ) , riddell ( 1948 ) and ledlie ( 1948 )  . 
little attention appears to have been given to this problem until scarff and handley ( 1938 ) suggest.ed that disappointing results in stage 1 cases may be explained by this mode of spread . 
this applies particularly to growths situated in the inner half of the breast ; of 17 such cases 12 had deposits in the internal mammary chain , in 2 of which the axilla was not also involved . 
 in spite of this , truscott ( 1947 ) and harnett ( 1948 ) were unable to show that the site of the growth plays an important part in prognosis . 
 in those cases where the axilla appears to be free from involvement at the time of operation and the prognosis subsequently turns out to be poor , invasion has probably occurred by routes such as the int.ernal mammary chain , and perhaps the supraclavicular glands . 
 after considering these facts it would appear , as handley and thackray ( 1949 ) point out , that there are but few growths which are really confined to the breast . 
chief success , from the point of accuracy and simplicity , appears to have been from histological grading , on the lines mdicated by pat.ey and scarff ( 1928 ) , combined with the state of the axillary glands . 
stage i ? this question has defeated explanation in the past , and will probably continue to do so until such time as the pathologist plays a part in establishing a prognostic system of the type indicated in this paper . 
 the controversy which exists as to the relative merits of the different methods of treatment for carcinoma of the breast has led to the present investigation , the prime object of which has been to establish a more accurate classification for this disease . 
 the gra < le of the tumour taken together with the state of the axillary lymph nodes gives a more accurate indication of outcome than either grading or staging alone . 
for example , 94 per cent of grade i cases without glandular involvement were ali , e at five years compared with 16 per cent of grade iii with this complication . 
it offers an explanation for disasters in early cases , and also for remarkably good results obtained in advanced in indicates that all is not necessarily lost if a patient presents with a stages . 
 lt has been shown that in a given clinical stage or histological grade the cases treated by surgery alone are not strictly comparable to those subjected to surgery and radiotherapy . 
in addition this has probably also played a major part in bringing about the present - day confusion as to the relative merits of the various measures advanced for the control of the disease . 
sambrook for assessing the clinical st.age of the cases ; to miss chambers of the follow - up department for tracing the patients , and to the photographic department for assistance with the microphotographs . 
a laparotomy was performed on each animal using ether anesthesia for rats and guinea - pigs and nembutal for mioe , and a loop of the intestine adjacent to the pylorus ligated . 
the abdominal cavity was closed with nylon sutures and each animal returned to its original cage . the animals were not treated further until 3 to 3hours following the laparotomy by which time all had emerged from the anesthesia . 
of body - weight of a 0.5 per cent aqueous solution of toluidine blue 0 . animals were anesthetized i an hour following the time of injection and a blood sample withdrawn either by heart puncture or from the aorta . 
the ph of the contents as well as of the gastric mucosa was obtained with hydrion the stomach contents were diluted 1 : 1 with acetone , stirred , and centripaper . fuged for 10 minutes at 2000 r.p.the supernatant was withdrawn and a 1 ml . aliquot diluted with acetone to 10 ml . this was stored at 50 to 100 c . 
overnight following which it was centrifuged 20 minutes at 2000 r.p.m. , and the supernatant removed for spectrophotometric analysis . in some rats the intestinal tract was removed and the contents collected . these as well as the blood samples were analyzed in the same manner as the stomach oontents . for the standard curve , 1 ml . 
an acetone blank was used for all determinations . in the case of gastric samples , the ph of the blank was adjusted to that of the sample using hc1 . the same acetone was used throughout the experiments and was redistilled prior to use . a beckman model du spectrophotometer was employed in making the measurements . 
inasmuch as the the guinea - pig , like the dog , is considered to be susceptible to histamine stimulation , an enhancement of gastric secretion following injection in this species was anticipated . the proportion of formed elements to plasma in the blood was determined for rats and guinea - pigs but not for mice in several of the groups . these results are listed in table i under hematocrit values . it will be observed that among the rats which received histamine ( groups i , ii , v , vi ) , an average value of 69 was obtained . 
whenthe ratswere not injected with histamine ( group iii ) , thehematoneither the ph of the stomach contents nor that of the crit value averaged 65 . gastrio glandular mucosa was altered significantly by the administration of histamine . in the rat a normal hematocrit value of 45 - 8 has been reported for males of the sprague - dawley strain ( gardner , 1947a )  . this value was confirmed in our laboratory . 
thus the histamine appeared to have no additional effect on the hemoconcentration observed in all operated animals . in untreated male guinea - pigs a hematocrit value of 42 has been reported ( gardner , 1947b )  . examination of the blood of treated guinea - pigs in our experiments disclosed a significantly higher hematocrit value in every animal . 
the control and 4 treated animals show no selective absorption in the region in question . similar analyses , using 5 guinea - pigs of group i and 1 guinea - pig corresponding to rat group ii , showed no definite peaks in the range between 375 and 400m , tt . although animals were fasted 48 hours prior to the start of operations no precautions were taken to prevent coprophagy , since it was our intention to duplicate the oonditions which prevailed in the experiments of ray and peters ( 1951 )  . when gastric contents were collected , it was observed that in addition to fluids although some of this may there also was present a varying amount of solids . have been due to residual food , it is more likely that ingestion of feces was responsible . 
18 - not included in any group - rat injected subcutaneously with histamine solution alone . solid lines represent animals given compound iii . analyses of blood from rats injected with compound iii revealed no compound by a method which was shown to detect 001 mg . 
on the other hand , the presence of toluidine blue o may be established by spectrophotometric analysis since intestinal contents give no peaks in the region of maximum absorption of this dye . it is of interest that such analysis from rats injected intraperitoneally with an aqueous solution of toluidine blue 0 failed to reveal this blue dye . ray and peters ( 1951 ) reported that gastric extracts from 3 out of 3 rats treated with compound iii showed substantial absorption at 400 mru . in the present experiments only 1 rat out of 15 showed similar results , while 2 fell in an intermediate , doubtful category . 
lipschutz. from departamento de medicina experimental , servicio nacional de salud , avenida irarrazaval 849 , santiago de chile . received for publication april 2 , 1953 . the tumours which appear in the intrasplenic ovarian graft in castrated rats , mice , guinea - pigs or rabbits apparently are due to the uncontrolled gonadotrophic activity of the prehypophysis , the ovarian steroid hormones which normally control hypophysial activity being inactivated during their passage through the liver before reaching the general circulation ( iglesias , mardones and lipschutz , 1953 )  . 
we shall be able to show ( 1 ) that this is not the case , and ( 2 ) that the hormonal imbalance from which ovarian tumourigenesis under the given experimental conditions derives can , and must , be expressed in quantitative terms . for the purpose of this study the secretory activity of 15 intrasplenic grafts , as listed in table i of our previous paper ( iglesias , mardones and lipschutz , 1953 ) has been checked by the histological examination of the vaginal mucosa . the uterus and the mammary glands . 
the presence of ovarian hormones in the general circulation at a level allowing for the transformation of the vaginal mucosa and of the uterine epithelium , even with the production of cystic glandular hyperplasia and metaplasia . 
rus. * pregnancy = several layers of clear vacuolized epithelia . * * transition = several layers of proliferated cells of the basal epithelium beneath the vacuolized layers as in fig . 
as evidenced by various new observations , we must drop the idea held originally both by biskind and by ourselves as to the gonadotrophic activity of the hypophysis in experiments with intrasplenic ovarian grafts in castrated females : contrary to what we thought before , the hypophysis is , under these experimental conditions , not identical to a castrate hypophysis . thus , the content of gonadotrophic hormones in the hypophysis of animals with grafts is considerably less than in the castrate hypophysis ( jungck , heller and nelson , 1947 )  . indeed this non - identity may be due to a difference , not of production , but only of release of gonadotrophins in castrated and grafted animals ( miller and pfeiffer , 1950 ) ; but non - identity seems to be a fact . castration cells are absent in the hypophysis of the grafted rat , in 224 2 . 
lipschutz any case in advanced stages of ovarian tumourigenesis ( lacour and guerin , 1951 )  . however , as compared to a normal hypophysis , that of a castrated animal with an intrasplenic ovarian graft is functionally impaired . differential tumourigenic thresholk concentrations of oestrogen . the problem of differential levels of oestrogen by which control of the vaginal or uterine mucosa and of the hypophysial gonadotrophic activity is achieved is intimately related to the problem of the differential tumourigenic threshold concentrations of oestrogen . 
how will the hypophysis behave when exposed to the action of these minute quantities of oestrogen in experiments lasting more than 2 years ? a group of 9 guinea - pigs was castrated and one ovary was grafted into the spleen ; sixteen days later a pellet of 23 to 30 mg . 
but the quantities absorbed were not sufficient for a complete control of this hypophysial activity : they were not able to reduce it to normality , as shown by the presence of haemorrhagic follicles in most of the animals of the group . there was in this group control of the vaginal mucosa and of uterine growth . in one animal the uterine weight was only 0o6 g . ; but in the remaining animals a weight of 0 - 8 to 1 - 2 g . 
with these 1 per cent pellets the incidence is not in another great ; new experiment lasting 757 to 875 days , without intrasplenic ovarian grafts , it occurred likewise but once in a group of 10 animals . 
one may raise the question whether some irreversible hypophysial change takes place during those 2 to 3 weeks which are needed for the vascularisation of the graft and for recuperation of hormone production . we have referred above to the three gonadotrophic hormones of the hypobut the possibility must be considered that also the somatotrophic or physis . some other hypophysial organotrophic hormone is partaking in establishing tumoural growth in the ovary ; this question has been discussed especially with reference to tumoural growth of wolffian structures ( iglesias , mardones , bruzzone and lipschutz , 1953 )  . the statement that ovarian tumourigenesis does not presuppose a complete suppression of the steroid control of the hypophysis but is the outcome of an irregular interplay of ovarian and hypophysial hormones may at the first sight however . 
the hormonal imbalance may last for as long as 3 years , and sometimes even more , without norwhereas it was evident , almost from the beginning mality being again attained . of this phase of our work , that the sequels of ovarian fragmentation , i.e. , reducing the mass of two ovaries to a small ovarian fragment , or remnant , in situ , were due to an overthrow of the normal ovarian - hypophysial relationship , we were unable to understand why this hormonal imbalance is in some cases irreversibly maintained . 
gutnz of untreated leukaemic cells observed in vitro . only the quantitative aspects of the subject will be dealt with here ; the cytological findings will be described in a separate paper . normal and leukaemic blood and bone marrow have been studied in tissue cultures by many workers since the publication of the first report on tissue culture of leukaemic blood by awrorow and timofejewskij ( 1914 )  . 
among other investigations carried out in recent years the following should be mentioned , as they deal wholly or in part with culture of leukaemic blood or marrow : papers by barnes and furth ( 1937 ) and bichel ( 1940 ) on mouse leukaemia ; doljanski and pikovski ( 1941 ) on fowl leukosis ; and fieschi and astaldi ( 1946 ) , israels ( 1940a , 1940b ) , osgood and brownlee ( 1936 , 1937 , as well as many later papers from the same laboratory ) , pierce ( 1932 , 1942 ) , schrek ( 1946a , 1946b ) , and wallbach ( 1936 ) , on human leukaemia . 
the vaccine caps are washed , and as rubber is toxic to living cells , they are then coated with a very thin layer of paraffin wax , by dipping them into a saturated solution of paraffin in petrol ether and wiping off excess after withdrawal . 
gunz been put into a conical flask , and the cells are now added to it , the aim being to give a final concentration of about 2000 leucocytes per c.msome practice is required in judging the correct volume of cells to be added . three consecutive counts are done on the cell suspension , and when the mean reveals a suitable cell concentration , a quantity of 2 ml . 
3. - mean daily counts of a sample culture of blood ( chronic myeloid leukaemia ) , expressed as per cent of initial count drawn on logarithmic scale . 6 days in the light of these two experiments , the following routine procedure has been thought justifiable : the mean of three counts of the original cell suspension is taken as the 100 per cent initial value for all tubes . 
on each subsequent occasion three separate counts are done on each of three fresh tubes , and the mean and standard error between tubes are calculated for all nine counts . 
means are calculated from the three individual counts and used for constructing the growth curve . in these differential counts a siniplified nomenclature of the myeloid series has been used , cells being divided into the three broad classes of myeloblasts , myelocytes and polymorphonuclears ( eosinophils and basophils being counted separately )  . 
the term " immature cell " comprises myeloblasts and myelocytes , the latter being arbitrarily defined as complying with two or all of the three following characteristics : total cell size exceeding that of a normal polymorphonuclear by 1 / 3 or more ; nucleus oval and only slightly indented ; cytoplasm basophilic . 
some of the patients with chronic myeloid leukaemia were untreated , while others had had various forms of therapy . cultures were either continued until all cells had died , or they were deliberately abandoned at an earlier period . 
when they were continued , there was always a gradual decrease in the total counts until death of the last cells occurred , usually between the sixth and the ninth day of culture . 
no significant increase in total counts has ever been observed . of especial interest is a group of nine cultures , selected because the cells lived for at least 7 days . 
4. - mean daily counts of a sample culture of blood ( chronic myeloid leukaemia ) , expressed as per cent of initial count drawn on linear scale . days log y = 2.0792 - * 0747x 7 days fig . 
6. - effect of 5 per cent rat embryo extract on culture of blood ( chronic myeloid leukaemia )  . total and differential counts expressed as per cent of initial count . 0 1 / 3 3 days of the total count in the two series are probably not significant , they certainly do not follow a straight line . 
of greater interest is the behaviour of the immature cells , in which a striking difference between the two series is apparent . while there is a gradual decrease of the number of immature cells in the control cultures , there is a significant rise in the e.e. 
cultures showing a peak of more than four times the height of that in the control cultures . results similar to these have been found in all cultures in which differential counts were done . 
6 ; the excess polymorphonuclears can have only been formed from immature cells , and the decrease in the number of the latter is explained by their proliferation failing to keep pace with maturation . after the second day , the process is less important and soon stops , mature and immature cells decaying approximately exponentially at the same rate , as shown in fig . 
may be a ribo - nucleoprotein , and experiments are now in progress designed to co - ordinate the growth curve with the nucleic acid metabolism of the cells . the action of ionizing radiations , as well as of many chemotherapeutic agents , is primarily on mitotic cells . in investigating these actions , every effort should therefore be made to provide the maximum number of mitoses in the test object . thus in fluid cultures the addition of e.e. 
jolles. from the radiotherapy department , general hospital , northampton . received for publication december 16 , 1948 . the focusing of attention on the malignant cell in the study of tumour tissue reactions to radiations and growth inhibitory substances has not brought us nearer the state of affairs where both practical and theoretical issues of oncology and treatment of tumours can be studied with a better understanding and fairer prospects of success . the importance of the stroma reaction to tumour and stromal reaction to radiation has been accepted for a long time , but only with generalizations on changes in " blood supply " and " tumour bed , " leaving the whole problem of connective tissue reaction in a hazy state . as regards tumour tissue reaction to radiation , much stress has been laid in the past on the changes following irradiation in the cells alone , but very little although recent attention has been paid to the intercellular tissue components . advances in cytology and genetics have enhanced the importance of the cellular nucleus , it must not be forgotten that evidence , both experimental and clinical , is available to show that the effect of ionizing radiations on cells alone " is not the whole story of the events leading to the destruction of proliferating tissues and that other factors come into play " ( muller , 1940 )  . the great importance of connective - tissue reactions to x - rays in radiotherapeutics has been raised by windeyer ( 1942 ) , ellis ( 1942 ) , windholz ( 1947 )  . 
the lesion is reproduced by means of a stent impression in a plaster cast , over which a tightly fitting stent or black - tray compound applicator is built in such a way as to be easily mounted over the part of the body , and fitting in such a way as not to allow even minimal shifts of the applicator , and so avoid the x - ray beam striking the alternate " opaque " squares of the lead chess which is recessed in the mould . the radiation has to be delivered at right angles with the x - ray tube head in order to avoid oblique penetration into areas applicator directed vertically . beneath the opaque squares the lead chess must be in direct touch with the tumour it is found in the course of treatment that owing to shrinkage of the surface . tumour the recess sleeve in the stent mould into which the " chess " is slipped has to be filed down from time to time during the course of treatment . the thickness of the lead , which is limited for practical considerations , permits 3 per cent of the radiation to pass through on to the protected areas . 
to that amount of radiation received by the not directly irradiated areas has to be added about 3 - 5 per cent of scatter radiation from the neighbouring exposed areas . this varies according to the size of the apertures , and decreases towards the centre of the " opaque ' , squares . 
the size of the squares has been chosen of not less than 1 cm . , so as to leave an adequate amount of tissue either almost completely non - irradiated or exposed for biopsy taking . sections are taken before treatment is commenced and then at varying intercuts are made into the exposed and protected sectors , and also one section vals . is made cutting across both the exposed and protected areas of tissue . accurate labelling of biopsy material must be insured , as no other way of recognizing the protected and exposed sectors on the histological slide is available . a working chart is found indispensable . prior to taking the biopsy the lead mask is applied and the exposed areas are mapped out by means of gentian violet paint . the biopsy material was fixed in sublimate - formol solution or sousa 's solution . following paraffin embedding , sections were cut at 7l and stained with ( 1 ) harris ' haematoxylin , eosin , ( 2 ) van gieson stain , ( 3 ) by gallego 's method , and ( 4 ) silver impregnation . the irradiation was taking place every day , 5 - 6 days per week . 
hard mass filling right breast , fixed to pectoralis and ulcerating skin in anterior axillary line over an area 8 x 5 cwith a sloughy crater and rolled - up edges . 
at this point " chess " technique abandoned and routine glancing technique reverted to . ( 4 ) section taken when tumour received apart from the 4000r with the chess technique 2500r on each glancing field in 14 days ; 10 treatments . ( 5 ) section taken at end of treatment ( 4000r to chess and 3500r on each glancing field in 5 weeks )  . she is remarkably when last seen , 15 . 
meredith. from the christie hospital and holt radiumt institute , manhester . received for publication december 12 , 1948 . ix a series of papers ( dale , 1940 ; dale , meredith and tweedie , 1943 ) it has been shown that the action of x - rays on aqueous solutions of biologically active compounds was indirect , i.e. 
further , it has been shown that in consequence of this indirect action , if two solutes are present , the second solute ( the protector ) reduces the radiation effect on the first one ( the indicator ) ( dale , 1942 ; 1943 ) , by sharing the intermediate product formed from water by the radiation . 
kennedy. from the endocrinology research department of the new zealand medical research council , medical school , dunedin , new zealand . received for publication july 30 , 1951 . previous communications from this laboratory ( griesbach , kennedy and purves , 1945 ; purves and griesbach , 1946 , 1947 ) described the induction of thyroid adenomata in rats by the long - term administration of goitrogens . bielschowsky , griesbach , hall , kennedy and purves ( 1949 ) showed that these thyroid tumours as well as those appearing under the combined influence of goitrogen and carcinogen could be transplante ' d into rats of the same strain . transplantation was only successful when the recipient animal was kept in a state of thyroxine deficiency produced either by treatment with goitrogen or thyroidectomy . 
from this failure of the transplanted tissue to grow in normal animals it was concluded that an excess of thyrotrophin was needed for the continued progressive growth of such tissue in a similar way as it had been necessary for the induction of the original tumour in the rat 's thyroid . therefore , these tumours were not considered to be " autonomous , " although they showed such signs of mahgnancy as a typical and progressive growth , invasion of surrounding tissues and formation of metastases . 
being injected subcutaneously in the flank of each the majority of rats were continuously supplied with a - 01 per cent rat . special mention is made in the solution of methylthiouracil as drinking water . text when no goitrogen was given . 
the thyroid was very large with a nodule protruding from the isthmus . part of this nodule was removed and two pieces were inoculated into two young rats which had been given 0 - 01 per cent methylthiouracil beginning 5 days previously . 
the acini varied in size , many of them being larger than the acini of the normal rat thyroid . in one line of transplantation this structure has been maintained up to the present day , and ' fig . 
6 shows the histology of a graft from the fourth generation of this fine . it will be noted that surrounding the larger acini there are numbers of small acini which suggest that new acini are being formed by budding from the larger ones . small cellular areas exist without well - defined acini , but these are considered to be areas of prohferation in which differentiation has not yet taken place . 
the acini are well filled with colloid , this colloid accumulation being always present even under conditions of strong thyrotrophic stimulation . this presence of colloid does not , however , indicate that the tumou ' rs are not influenced by thyrotrophic hormone , since when the thyrotrophic hormone production in the host is inhibited , these tumours undergo rapid regression . iodine , metaboli8ln of t , tumour . the iodine metabolism of the transplanted t , tumour was tested in rats bearing second generation grafts . table i shows the results of in vivo tests of the uptake of radioactive iodine in three rats after radioactive iodine had been injected . 
l. - chart of the first 6 generations ' grafting of the tbyroid tumour t , the treatment of the recipient animals is indicated on the cbart . solid black indicates animal bearing tumour . 
kennedy the evidence of secretory function in the t , tumour has been obtained from the results of transplants growing in totally thyroidectomized animals . these animals the ti tumour transplants do not grow continually , but appear to reach a maximum weight of about i g . 
of rats witb tumour growth . growth was obtained in the normal animals . this indicates the dependence on high thyrotrophic hormone levels , a dependence which is also displayed when animals bearing growing tumours during the administration of methylthiouracil have their medication stopped . 
the large irregularly - shaped acini which were prominent in the ti colloid was present in some of the acini but was less tumour were not seen . prominent than in the t , tumour . 
the nuclei were hyperchromatic and irregular in sha e . ( 2 ) embedded in this adenomatous tissue was a nodule of tiss ' ue distinctly different in staining properties . in this tissue , which had a well - developed acinar structure corresponding to a very hype ' rplastic normal rat thyroid , the cells were large with abundant cytoplasthe nuclei were round and did not contain excess chromatthe lesser numbers of nuclei and their weaker staining properties ' ' were responsible for the pafer appearance of these nodules in the 306 h . 
the fact that such tissue always forms microscopic nodules and has not ever formed a large part of the grafts in any of the inoculated animals suggests that this type of tissue is a slow - growing variant which arises spontaneously within the adenomatous tissue . 
the nodules of this type seen in the fourth generation appear to have arisen from the modified adenomatous tissue of these animals mentioned above which differs from that of the original tumour . ( 3 ) the third type of tissue is an anaplastic carcinomatous tissue without any in animal 253 , no . 
in weight being observed after 10 days . in the fourth week after transplantation animals with the rapidly growing tumours began to succumb . in a proportion of the animals , however , the growth was slower and the animals survived 3 or 4 months . 
the histology of ah these tumours was that of the anaplastic carcinoma described above as the third type of tissue seen in the fourth was successfury maintained by serial generation . transplantation , and - in later transplantations successful grafts were obtained in up to 80 per cent of those inoculated . 
the t22 tumour has now been transplanted through 7 consecutive generations and has not undergone any progressive change in either malignancy or histology . histology of tumour t22on the cut surface two regions cciuld be regularly seen , the outer with a shiny grey appearance , 5 to 8 mbroad , and the central one coloured a pale orange frequently a brown albuminuous fluid had replaced with a crumbled surface . mioroscopic examination revealed that , ' generally , the inner the central tissue . zone ofthe tumours consisted ofdegenerating cers or amorphous masses , infiltrated by round ceus , and isolated cers with strongly eosinophihe cytoplasm and pycnotic nucleus , lying , between the cell debris . the outer zone , microscopically , appeared simflar to that of the anaplastic nodule of the original tumour , and this description apphes to both tissues . 
unusuary large tumour cefls were present which had slightly basophilic cytoplasm and nuclei with ir - regulariy dispersed chromatin . giant cells were present with nuclei varying in number from 2 to ' 8 . 
the numbers of giant cers found varied somewhat in different animals and were relatively few they have , however , been a constant feature of in the first animal examined . the tumour ' and we consider that the tumour should , therefore , be classed as a giant cell carci ' noma of the thyroid . mitotic ftgures are frequent and many of them atypical . effe , ct of t22 tumour on the host . the striking feature of the t22 tumour is that it kirs its host in as short a period as 3 weeks . there is , however , a considerable variation in the rate of growth in different animals , some of them surviving for 2 months or more . those animals which died within 3 to 4 weeks after inoculation , the animals showed at autopsy an extreme state of emaciation with atrophic muscles and thin soft bones . 
was lower than ' its weight at the time of transplantation . it appears , therefore , that the rapid growth of these tumours withdraws nutrients from the host and leads to the state of emaciation described . effect of thyrotrophic hormone level on tumour t22 ' the t22 tumour has been found to grow equally wer when inoculated into normal animals or animals receiving methylthiouracil . moreover , in normal animals in which this tumour is growing , no inhibition of the growth rate has been observed when the an ' imals were treated with thyroxine injections . in some selected animals bearing this tumour in which the growth was relatively slow this treatment did not produce any marked some were treated with thiouracil . acceleration in the growth of these tumours . 
the t22tumour , therefore , does not show the dependence upon thyrotrophic stimulation which was shown by its parent tu ' mour . iodine , metabolimof the t22 tumour . rats bearing the t22 tumour were injected with radio - active iodine and 24 hours later were killed , and the radio - active iodine concentrations in the tumour tissue and in the blood plasma were measured . 
kennedy considered that both the action of the carcinogen plus the hyperplasia resulting from the goitrogen were necessary for the induction ofthyroid tumours . however , griesbach , kennedy and purves ( 1945 ) reported that the prolonged action of goitrogens alone led to the formation of tumours , which in a later publication ( bielschowsky , griesbach , hall , kennedy and purves , 1949 ) were shown to be similar in all respectsto those appearing after the carcinogen treatment . 
with goitrogen alone , however , tumours are later in appearing and are fewer in number . these tumours aredependent upon high thyrotrophic hormone level for their in normal animals such tumours , either in the thyroid or as grafted growth . - tumours , undergo rapid regression and eventually disappear , so that they cannot be induced to reappear by the subsequent administration of goitrogen . 
the simplest explanation , therefore , of the role of the goitrogen in the production of these tumours is that it induces the high thyrotrophic hormone production without in this view , the goitrogen would not have which such tumours cannot grow . any influence on the formation of neoplastic cells . it is , therefore , considered that neoplastic cells arl 'se spontaneously in the normal rat thyroid , and that when conditions are suitable for the growth of such cells , visible neoplasms result . 
in weight are commonly produced.. the continuous growth of such tumours 4nd the propagation of them by transplantation leads naturary to the selection of fast - growing types of tissue so that an increase in mahgnancy with transplantation is to be expected . however , modifications of the adenoma are not invariably in the direction of increased mahgnancy . 
we consider that the type of nodule described as the second type of tissue observed in the fourth generation transplants is a relatively slow - growing benig - n structure which reappears in successive generations , and which by virtue of its slow growth and lack ofmetastasizing power cannot be selectively propagated by transplantation . 
on the other hand , the truly malignant , invasive and metastasizing carcinoma will , when it once appears , invariably supplant entirely the benign structure in two , or three at the most , generations of grafting . evolution of malignancy in benign tumour8 . while it has been recognized that transplantable mammalian tumours show increases in mahgnancy on transplantation , it has been often assumed that such increase in mahgnancy results from a gradual adaptation to the host or a gradual modification of the original tumour . 
the thyroid adenomata appearing in - the rat thyroid are all dependent on thyrotrophic hormone for their ' existence , and in fact require higher levels of thyrotrophic hormone for their continued growth than does the normal thyroid tissue . investigation of human thyroid neoplasms with the aid of radio - active iodine have shown that many of these are in fact susceptible to the stimulating influence of thyrotrophic hormone , although neoplasms in human material have not been described which are so entirely dependent upon thyrotrophic hormones as are these primary rat thyroid tumours . 
the existence of undoubted stimulating effects of thyrotrophic hormone in human thyroid tumours supports the view that these rat thyroid tumours are not exceptional , although their high degree of dependence on thyrotrophic hormone sets them somewhat apart from the thyroid tumours encountered clinically . there seems no reason to hold the view , as some people have done , that these rat tumours should not be classed as neoplasms , since in their case the stimulating hormone or factor on which their 310 h . 
kennedy growth depends ' is well characterized and can be artificially manipulated so as to presumably as further knowledge is gained the control the tumour growth . stimulating influences which condition the growth of other tumours win be discovered , but this should in no way affect their classification as neoplasms . it is important to note here that from a tumour at first dependent upon a hormonal imbalance for its growth , there has been derived a mahgnant neoplasm which is no longer dependent upon the stimulating influences which condition the growth of the more benign original tumour . 
thus where mahgnant tumours are found which are not susceptible to any known hormonal influence , the effect of hormonal imbalance in the production of such tumours is not excluded . 
the work was undertaken as a collater ' al contribution to a wider scheme planned in 1952 by the cheshire and north wales branch of the british empire cancer campaign . for research into the pathogenesis of cancer the branch council required among many other things a laboratory analysis of soil taken from the vicinitv there was no precedent for the sort of analysls of the home of each patient . most suited to the project , previous workers in this field having been content with simple and often crude analyses or with the more detailed examination of too few specimens . it was clearly impossible to make a full physical and chemical examination of all the solid , fiquid and gaseous phases of every soil sample as several thousands were to be examined , so with some slight modification the analytical procedure of the soil survey of england and wales * was adopted - at first . it was felt , however , that an investigation of fatal cases of cancer in relation to soils as mapped by the late professor g . 
every case where cancer was mentioned on the death certificate , even when not the immediate cause of death , was included in the analysis , except that those occurring in the county of persons ordinarily resident in other areas were excluded . cancer was defined as any condition named in no . 
the differences between observed and expected values were subjected to the chi - squared test to determine the probabihty of such differences arising as a result of random these are the probabilities quoted in the tables that follow . 
that cancer of site a would be no more associated in an compariwith attribute b than would be the generality of cancer deaths . sons , unless the contrary is indicated , allowance was made for variations attributable to age and sex by calculating separately an expected number for six agesex groups and then adding . 
where it was desired to allow for a possible interaction between associations , expected values were adjusted . for example , if cancer of site a had shown an association with both attribute b and attribute c considered singly , and attributes b and c were known or suspected to be associated one with the other , adjusted distribution of expected values with respect to b were determined as follows . 
thus series having a common parent material geologically , are all indicated by the same capital letter , e.g. , all derived from non - calcareous shales of ordovician age are indicated p . 
the inclusion of many of this large group in social these considerations and our special class ii was therefore open to question . interest being in the association between cancer of the stomach and soil , suggested that it might be advisable to treat separately those occupations which bring the person into intimate connection with the land . 
griffith the public mains are supphed for the most part from surface water such as there is an exception where two small small lakes fed by streams and springs . ceintres get their water from deep bore holes but the populations are too smafl to be separated in the analysis . 
the in group l there social groups , however , show certain interesting differeinces . does not appear to be any association with fl soil . there is a relative excess of deaths in the other three groups although only in group iii is this undoubtedly siginificant in the statistical sense . soil and cancer of the breast . when corrections are applied for social group and water supply it is found that the association betweein cancer of the breast and a soil as compared with all other forms of caincer is stif present ( table x )  . 
0 - 20 > p > 0i i - ii * stomach all sites iii * stomach all sites iv - v * stomach ar sites stomach all sites all social groups : stomach males all sites females stomach ar sites 13 - 8  . 
w.7. received for publication march 14 , 1949 . previous observations ( foulds , 1947 , 1949b ) showed that the growth of some transplanted mammary tumours in hybrid mice depended on a hormonal stimulus which operated in normal female mice but not in normal males ; artificially - administered oestrogen supplied the necessary stimulus for growth in males . 
some of the tumours were independent of the hormonal stimulus at the first transplantation ; others lost their dependence after several transfers . dependence on hormones seemed to characterize one stage in the life - history of mammary tumours in hybrid mice . 
the majority of the mice were br hybrids , mostly of the f3 and f4 generations , and made up of 71 mice of strain br4 ( pink label ) , 90 of strain br4 ( blue label ) , and 69 of strain br6 . 
a preceding paper ( foulds , 1949a ) describes the source of these hybrids and the incidence of tumours in them . the mice were subjected to forced breeding and most of them had pregnancies in rapid succession throughout the period of observation , even when bearing multiple large tumours . 
tumours were recognized usually when about 0 5 cin diameter , and weekly thereafter two main diameters were measured with calipers . growth charts were made by plotting the sum of the two diameters against post - mortem measurements usually agreed time . satisfactorily with those made during life ; measurements on regressing tumours were the most difficult and subject to the largest errors . frequent , often daily , measurements were made on selected mice . litters were recorded each morning except on sundays and public holidays . the time of parturition as shown on the charts was usually later than the actual time by unknown periods of up to 24 hours on weekdays and 48 hours at weekends . 
the mice were examined post - mortem except for a few that were eaten ; the tumours were measured and pieces of them fixed for histological examination . in the charts the first tumour , or largest of contemporaneous tumours , is represented by a continuous line joining crosses which indicate the actual measurements ; the second tumour is represented by a broken line and circles , and the third by a dotted line and triangles . 
178. 8 9 10 weeks ( i ) left axilla ; ( ii ) right axilla . in most of the mice from 1 to 6 new tumours appeared during the course of the first . 
1 shows three different types of behaviour at the same time in one mouse . at least three major factors contributed to the wide diversity of behaviour amongst spontaneous tumours , and even amongst multiple tumours in the same mouse : first , the regulation of tumour growth by the environmental , and presumably hormonal , changes occurring during pregnancy and the puerperium ; second , the specific reactivities of particular tumours to the environmental 348 l . 
foulds changes ; and third the qualitative changes occurring in tumours during their manifest clinical course as evidenced in particular by altered responsiveness to in the remainder of this paper the terms " responsive " and reproduction . " unresponsive " are used in a special and restricted sense to describe tumours which , respectively , do and do not vary their growth in response to the physiological changes occurring in their ho * ts during pregnancy and the puerperium . the term " progression " is used , also in a special sense , to denote qualitative change in tumours as distinguished from mere advancement in size , and as evidenced in particular , but not exclusively , by altered responsiveness to pregnancy and parturition . subsequent paragraphs detail the analysis of the phenomena here outlined . for convenience of description the tumours are classified according to a few main types of behaviour , but transitional and indeterminate types are encountered and preclude a precise statement of the relative frequency of types . 
the peak size , however , was often considerable , as shown in some of the other charts representing type i tumours ( fig . some tumours maintained their 20 )  . course unchanged through several months of observation , whereas others after two or three cycles changed their behaviour , as described in a later section . the growth of responsive type i tumours was strictly conditional and dependent on pregnancy . if breeding stopped the tumours disappeared and , as a rule , did not recur until breeding was resumed . 
51. ( i ) right vulva ( ? recurrence of tumour excised 7 weeks previously ; earlier tumour not shown ) ; ( ii ) right axilla . with a small range of growth and regression at each pregnancy , and a slow but steady increase in average size . another tumour shown in the same diagram ( dotted line ) appeared 8 weeks after the first and then followed an almost parallel course . 
the peaks of growth , or the averages of the maximum and minimum sizes during successive pregnancies , fell close to a straight line . thus , the course of a tumour was represented by a curve which could be resolved into a straight line with superimposed waves ; the straight line indicated the rate of net growth or , for want of a better term , the intrinsic growth rate , and the waves indicated the response to pregnancy and parturition . 
the intrinsic growth rate and the degree of response , however , varied within wide limits and independently similar intrinsic growth rates were of each other from one mouse to another . responsive and linked with different degrees of responsiveness and vice versa . unresponsive tumours in the same mouse sometimes , as an exception to the general rule , had similar intrinsic growth rates as illustrated in fig . 
their differentiation from type i tumours was questionable , but they seemed to correspond with relatively frequent tumours in , nonbreeding mice whose course was represented by a horizontal straight line , and possibly differed essentially from type i tumours in the ability to persist without the stimulus of pregnancy . 
the great diversity of behaviour was attributable to two circumstances : first , the intrinsic growth rates and the responsiveness varied within wide limits and independently of each other as shown in the present section and , second , progression from one type to another occurred variously during the clinically manifest course of the tumour . 
the tumour itself had changed . the recognition of a similar change in responsive tumours was necessarily more difficult because the pregnancy waves obscured the intrinsic growth rate . probably an acceleration of growth often accompanied the loss of responsiveness 4m.3~ 0k 11 i / i i..#4 i 11 9 10 11 12 - 13 14 15 i\it - l 18 19 20 21 22 16 17 weeks fig . 
19 , however , the one that regressed completely between pregnancies ( broken line ) increased its peak size somewhat more steeply than the tumour that regressed incompletely ( continuous line )  . increasing peak size , therefore , was not attributable , in general , to summation . the regression of some tumours was slight and of short duration , being followed almost at once by progressive unresponsive growth . 
the regression was sometimes trivial and probably within the limits of error in measurements , and the tumours were then scarcely distinguishable from those already described which continued as unresponsive tumours from the peak of a pregnancy wave . possibly the two tumours illustrated in fig . 
29 proved unresponsive at a subsequent pregnancy . another tumour ( broken line ) shown in the same figure behaved similarly , except that it apparently began to grow earlier and was less certainly unresponsive at the subsequent pregnancy . some tumours regressed slightly or moderately after parturition and then maintained a constant size . 
the terminal course was represented by a straight line , but the intermediate course through the first and second pregnancies after the resumption of breeding was more fairly indicated by a curved line , suggesting a gradual accession of growth energy in an unresponsive ( or minimally responsive ) tumour . 5 0o d - t . 
more commonly the first tumour was solitary and further tumours developed consecutively . so far as could be seen the spacing of successive tumours and the sequence of types were irregular . 
tumours that remained solitary throughout the period of observation were sometimes unresponsive , but more frequently responsive . in the majority of the mice where two tumours appeared at about the same time both tumours were responsive ; in the minority both were unresponsive , or one was responsive and the other unresponsive . 
as a rule new tumours were registered first during pregnancy . different types of tumours developed independently of each other in the same mouse , and progression from one type to another occurred independently in the several tumours . 
13 , regressed completely within 7 days , but when another pregnancy followed without delay regression was only partial . possibly hormonal changes during the first 2 or 3 days of pregnancy sufficed to check regression , although growth was not apparent until a few days later . perhaps a few of the " recurrent " tumours were , in reality , new primary growths , but so nearly as could be determined the recurrent tumours occupied the same positions as those which had disappeared and were of similar shape . after partial regression the reality of true recurrent growth was not in doubt . some tumours were reduced to thin plaques not greatly different in superficial dimensions from the tumours at their peaks of growth ; recurrence was manifested by a thickening of the whole plaque . other tumours shrank to vague subcutaneous thickenings of doubtful , but probably considerable , extent ; recurrent growth was evidenced by sharpening of the outlines . it seemed that tumours recurred by the simultaneous grow ' th of all parts of a substantial area of previously altered mammary tissue rather than by centrifugal growth from a in consequence , recurrent tumours were often relatively small residual focus . large when first registered and the gradients of growth and regression remarkably steep . a few tumour - bearing mice nursed and weaned their litters . their tumours behaved during lactation like those in recently pregnant mice that did not at once become pregnant again although deprived of their young . 
some dubious tumours , registered once or twice on suspicion , were not seen again , but only 5 tumours , recorded on at least one occasion without query , disappeared permanently from mice that continued to breed . after interruption of breeding the tumours that had regressed recurred , with few fig . 
the recurrences corresponded as a rule with expected pregnancies in continuously breeding mice , and the recurrent tumours , unlike those in segregated females , were responsive ; almost certainly the recurrences were stimulated by unrecorded pregnancies . 
76. male removed at a ; injections three experiments were carried out with oestrogens . in the first , each of 8 mice received 4 daily applications to the skin of 0 - 2 c.c. 
36 shows regression checked and succeeded by growth at the time of the injections , but as similar events occurred without injections during intermissions of breeding the interpretation was doubtful . in other mice an action on tumours was trivial or lacking . in the third experiment cholesterol pellets containing 10 per cent of diethylstilboestrol and weighing on the average 8 - 2 mg . 
were implanted subcutaneously in 7 mice . nine tumours previously observed in these mice had disappeared before the pellets were implanted and none recurred promptly , but eventually each mouse developed a solitary tumour . in 3 mice the late tumours recorded 366 l . 
foulds 54 days , 145 days and 145 days respectively after implantation of the pellets were in the same region as earlier tumours which had regressed , and were possibly , but , in view of the long delays , not probably , recurrent tumours . in the other 4 mice the late tumours were remote from the sites of the earlier tumours and were undoubtedly new primary growths . 
the present section records the transplantation of tumours whose previous course was known and describes experiments with tumours removed surgically with three main objectives , namely to study autotransplantation , to compare successive primary tumours in the same host , and to compare primary tumours with the recurrent tumours which followed the operation . the experiments were few in number , the general plan of this investigation being to study the natural course of tumours with a minimum of experimental interference . tumours of similar size from the same mouse were used to compare the transplantabilities of responsive and unresponsive tumours . 
tumour in the first passage tumour b grew a grew in female hosts but not in males . equally in male and female hosts , although in the second passage the implants grew tardily in males . 
from these experiments it appeared that , in general , unresponsive tumours were transplantable into male and female hosts and responsive tumours only into female hosts , but that the correlation between type of growth in the primary tumour and behaviour after transplantation was not perfect . five tumours were excised and used for autotransplantation , implants being inoculated subcutaneously near the mid - line of the abdomen in order to minimize confusion with new primary tumours . three of the transplantations were unsuccessful . 
foulds each , so far as could be judged from the short period of observation , was " responsive . " two autotransplantations were successful . growth of the implant from a primary tumour measuring about 0 - 2 cin diameter and removed 6 days after detection was evident after 26 days , and continued steadily until the mouse was killed 22 days later . 
haddow , using in the main dealers ' mice of unknown ancestry , recorded frequent measurements during and after pregnancy , and concluded that " no evidence was found to suggest that gestation itself has any influence on the rate of growth of mammary cancer in the mouse , but in approximately half of the available cases it was observed that parturition was followed by a temporary decline in tumour growth rate . " haddow 's two figures illustrate , respectively , a substantial though incomplete regression after parturition and a halting of growth without regression ; they match some curves of mine . 
gardner ( 1941 ) described 5 hybrid ( 057 black x cba ) f1 mice which , repeatedly , had tumours attaining 1 - 2 cin 2 to 5 pregnancies ; the tumours regressed after parturition , but 3 of the mice eventually died with mammary adenocarcinomas . the responses of the tumours in the hybrid mice used in the present investigation are , possibly , exceptional in frequency and degree , but are not essentially different from those described by haddow and by gardner . notable response to pregnancy and parturition is here recorded in hybrids of varied genetic constitution derived from the inbred strains c57 black , riii and a ; it is not correlated with anomalous transmission of the milk - borne mammary tumour agent . the pregnancy effect usually becomes apparent during the second half of gestation , but probably begins during the first week and continues until the ' day before parturition . 
the abrupt regressions about the time of parturition suggest the sudden withdrawal of a stimulus which , though not yet identified , is presumably hormonal , affecting widely - distributed multiple tumours . 
the preliminary experiments with hormones are indecisive ; a simple oestrogenic action seems unlikely , and the possible effect of gonadotropic hormones , placental hormones , and the co - operative action of oestrogenic and luteal hormones require further investigation . lactation has no specific effect , and modifies the course of the tumours only in so far as it delays the next pregnancy . the pregnancy effect on mammary tumours is comparable with the " promoting " action of various procedures on chemically - induced tumours of the skin of rabbits and mice . 
rous and his colleagues ( rous and kidd , 1941 ; mackenzie and rous , 1941 ; friedewald and rous , 1944a , b ) studied promoting factors in rabbits , and berenblum , who has recently adopted rous 's nomenclature , in mice ( berenblum , 1944 ; berenblum and shubik , 1947 )  . 
foulds his colleagues describe the " promoting " action of trauma and irritants in eliciting and maintaining tumour - growth from latent tumour cells present in the skin as a result of the " initiating " action of a carcinogen . 
some " conditional " tumours grow only whilst the promoting factor operates ; they disappear when it is withdrawn , but recur from the irreversibly altered epithelum when the promoting factor is restored . 
rous and kidd discuss whether or not their argument the conditional growths of rabbits ' skin are " true tumours . " in essential applies equally to the conditional mammary tumours of mice . agreement with rous and kidd , i consider that their exclusion from the group of tumours by an arbitrary definition is unwarranted , and i describe as " tumours " all the mammary growths except a few palpable nodules which regress and do not recur , and those nodules , probably similar , that do not survive autotransplantation . they are accountable to a reversible change in mammary tissue , and perhaps to the exceptional persistence in gross nodules of the properties of the hyperplastic nodules or " adenomas " which are widely accepted as precursors of mammary tumours in mice although many of them are abortive ( gardner , 1941 )  . browning ( 1948 ) reported that nodules less than 02 cin diameter in c3h mice were not transplantable , and that about a third of them regressed , whereas nodules larger than 02 cin diameter never regressed . my observations differ from browning 's in revealing no correlation between behaviour and size ; autotransplantation of tumours more than 05 cin diameter was unsuccessful . the remaining mammary tumours develop from an irreversibly altered mammary tissue . 
the great diversity of behaviour is attributable to the interplay of factors which vary within wide limits and independently of each other . classification into types , though convenient for description , is arbitrary , and hampered by gradations from one type to another . 
the primary distinction , although not absolute , is between the " responsive " tumours whose course is notably influenced by pregnancy and parturition and the " unresponsive " tumours whose growth is unaffected by reproduction . the tumours assigned to responsive type i correspond with the " conditional " neoplasms of rabbits ' skthey grow during pregnancy , regress promptly after parturition , and recur , with rare exceptions , in the same place at each successive .pregnancy ; after several cycles of growth and regression they achieve no net increase in size or aggressiveness . 
the responsive type ii tumours are less strictly " conditional " ; they wax and wane at each gestation , but with a net increase of size at each cycle . 
the rate of net increase is steady and characteristic of the individual tumour , depending on a specific property described as the " intrinsic growth rate . " the term is provisional , to be discarded when elucidation of the property suggests a better name , and is used to denote the steady growth , represented by a straight line , upon which the waves of response to pregnancy are superimposed . 
the intrinsic growth rate , measured by the slope of the straight line and the responsiveness as indicated by the amplitude of the pregnancy waves , are constant , often for long periods , in a particular tumour , but vary within wide limits and independently of each other from one tumour to another . 
foulds of tumours , namely the capacity for progression , as above defined , and that general principles or rules of progression , deduced from the study of mammary tumours of mice , are widely applicable . the material for this analysis of progression consists of spontaneous tumours following their natural courses without experimental interference beyond temit is especially favourable on account of the porary interruption of breeding . abundance of multiple tumours , for the comparison of multiple tumours establishes beyond doubt that progression is a change in the individual tumour ; alteration in only one of several contemporaneous growths is not attributable to change in a hypothetical " general resistance . " the varied tumours encountered in this investigation may be arranged in a series having at one extreme the wholly conditional responsive tumours , at the other extreme the rapid - growing unresponsive tumours , and intermediately all indidegrees and combinations of responsiveness and intrinsic growth rate . vidual tumours , however , do not in general traverse this series ; they advance by abrupt steps , vaulting many possible transitional stages . 
at its first clinical manifestation a tumour may occupy any position in the series of types , irrespective of the time of its occurence or its position in a sequence of multiple tumours . 
tumours which develop simultaneously or consecutively in the same mouse conform sometimes to the same type and sometimes to as many types progression occurs independently and unpredictably as there are tumours . in multiple tumours in the same animal irrespective of their size or clinical progression may occur earliest in the first , second , or any subsequent duration . member of a sequence of multiple tumours . 
when two or three tumours , similar in size , duration , and type of behaviour are present , progression occurs in only one of them at a time . moreover , the progression of one tumour has no apparent effect on the course of the others . 
the present observations decisively controvert browning 's ( 1948 ) suggestion that a second tumour may " abrogate the autonomy " of the first . the several recognizable characters of individual tumours undergo progression often , no doubt , responsiveness and intrinsic growth rate independently . change simultaneously , but in some tumours progression in responsiveness occurs transplantation without progression in intrinsic growth rate and vice versa . experiments provide further evidence of independent progression of characters , namely the responsiveness of transplanted tumours to pregnancy and the gross milky secretion in response to oestrogenic stimulation ( foulds , 1949b )  . the development of a tumour does not always reach its end - point within the life - time of the host ; progression advances further during serial transplantation ( foulds , 1949b )  . 
the course of the growth elicited by pregnancy depends on specific properties which change , by progression , in latent tumour cells and in stationary tumours . the manifestation of progression in the mammary tumours is usually abrupt , as it is in the induced skin tumours of rabbits and mice , but progression itself is not necessarily abrupt ; it is possible that cumulative gradual changes reach a threshold level at which they are first manifest . 
some tumours evidence a gradual progression through a graded sequence of types . gradual , continuous progression seems uncommon , but it is less conspicuous than the abrupt type , and more accurate and more frequent measurements might reveal it more frealthough the observations are few and indecisive , it seems that slow quently . gradual progression is apt to result in sluggish , irregular , or dubiously unresponsive growth . 
the unequivocal rapid - growing unresponsive tumours , as a rule , are either primarily unresponsive or the result of abrupt progression from a fully responsive and , often , strictly conditional tumour . apparently two paths of progression are available . 
one path leads directly to unresponsive tumour ; the tumour acquires its definitive properties early without traversing the numerous intermediate stages which are possible , and which are observed on the other path or " responsive detour . " the detour leads ultimately to an unresponsive tumour , but progression along it may be slow and gradual and the end - point indeterminate , or reached only after transplantation . 
abrupt progression switches many tumours from the detour to the direct path ; jumping the intermediate stages , the tumours change from the fully responsive to the definitive unresponsive type . 
a few applications arehere briefly indicated . the behaviour of tumours is the resultant of multiple characters which vary , within wide limits , independently of each other and undergo independent progression . 
the - characters include growth energy , invasiveness , capacity for dissemination , and responsiveness to environmental stimuli , of which the hormones are the most easily recognized , but not necessarily the only , examples . " malignancy " is not a single character . 
independent progression of characters ( rule ii ) , however , results in disproportionate or " out - of - step " development , as for example in the " benign " tumours that metastasize and the " locally malignant " tumours that do not . 
the out - of - step development is especially important in carcinoma of the prostate , which , despite conspicuous growth , invasion and dissemination , willis ( 1948 ) criticizes the sharp division of tumours is responsive to hormones . into innocent and malignant groups , and deprecates the question , " is this tumour innocent or malignant ? " ; the appropriate question in his opinion is , " how it is even more important , i suggest , innocent or malignant is this tumour ? to ask , " in which characters , and to what degree in each of them , is the tumour innocent or malignant ? " errors in the prognosis of " early " tumours are explained by the observations that progression is independent of the size or duration of a tumour , and that progression occurs without manifest growth , as in latent or stationary tumours ( rule iii and corollaries )  . 
progression without manifest growth and independently of the size or duration of tumours probably accounts , too , for the otherwise mysterious but clinically important phenomena of long - delayed recurrence and secondary growth after apparent similarly the ultimate failure of several chemo " cure " of primary tumours . therapeutic methods after favourable early response is reasonably attributed to progression in the inhibited tumours . 
some tumours maintained the same type of behaviour throughout their clinical course ; others changed their course , often abruptly , as the result of an irreversible qualitative change in the tumours termed " progression . " the diversity of behaviour of the spontaneous tumours was attributable , in the main , to varied combinations of responsiveness and intrinsic growth rate , and to progression in one or both of these characters . following generalizations or rules of progression summarize the results of the analysis of the behaviour of tumours , especially multiple tumours , in breeding and non - breeding mice : ( 1 ) progression occurs independently in different ( independent progression of multiple tumours . ) tumours in the same animal . ( 2 ) progression occurs independently in different characters in the same tumour . ( independent progression of characters . ) ( 3 ) progression is independent of growth , occurring in latent tumour cells and in stationary tumours . ( 4 ) pro ( 5 ) progression follows one of altergression is continuous or discontinuous . ( 6 ) progression of a tumour does not always reach its end - point native paths . within the lifetime of the animal . these rules are probably widely applicable to the behaviour of varied tumours in animals and in man , and some applications are mentioned briefly . 
 " malignancy " is not a single character . disproportionate or " out - of - step " development of the various characters which determine malignant behaviour ( independent progression of characters ) accounts for many anomalieg in the behaviour of cancer in man , and progression in tumours whose growth is inhibited probably explains the ultimate failure of therapeutic measures which have a favourable immediate effect . i am grateful to l . 
8. - hormonally - induced hyperplasia on anterior edge of pectoral fin showing an early translucent appearance of tumour produced by my ' xomatous change in stroma . of the mucus - secreting epithelium and a myxomatous change in stroma . 
the present situation has been briefly restated by stocks ( 1953 ) at cardiff . there have been many endeavours to establish a racial factor to account for the known variations in cancer incidence . although they have been invariably inconclusive , as might be expected when consideration is given to the pronounced differences within individual countries , these surveys have shown that where racial types have migrated to other countries , e.g. , negroes to america , they appear to take over the incidence of malignant disease of the natural inhabitants among whom they have come to live . 
1. goitre distribution in holland ( amsterdam university )  . year , three further districts have been added to the list in the northern province of holland ( polak , 1954 ; personal communication )  . the lower incidence of goitre towards the belgian frontier is apparent and almost certainly significant . ( 2 ) united kingdom . variations of goitre and cancer within the united kingdom are striking . 
a recent survey ( stocks , 1950 ) of the incidence of carcinoma of the stomach in 83 county boroughs over a period of 18 years showed notable differences " which cannot be explained by chance variation or by differing accuracy of certification of cause of death "  . these variations were shown to correspond to variations in the hardness of the water supply : those with a moderate hardness tended to have 396 j . 
survey of goitre ( murray et this would be in keeping with the al . , 1948 ) to have a high goitre incidence . known clinical experience with regard to malignant disease in that county . comparing these two maps a striking correlation is at once apparent . outstanding are the heavy incidences of goitre and cancer in mid - wales , westmoreland fig . 
spencer and the fen district and neighbouring counties , and by contrast the light incidence in yorkshire , lincolnshire , herefordshire and pembrokeshire . gradations of correspondence on both maps are evident in comparing norfolk , suffolk and essex ; kent and sussex ; cornwall and devon ; glamorgan and carmarthen . a higher death rate from cancer was shown to exist in two swedish counties , kopparberg and gefieborg , than was found in the total rural areas of sweden ( stocks , 1925 )  . those two counties , as shown by examination of schoolchildren , recruits for the army and candidates for confirmation , were found to have a higher incidence of goitre as compared with the rest of the country . similarly , known goitrous counties in norway were compared by stocks ( 1924 ) with counties showing little goitre , and it was found that the goitrous counties showed a cancer rate for all organs of 113 - 7 as compared with 94.4 for the niiongoitrous counties . in iceland , the thyroid has been shown to contain one of the highest conlcentrations of iodine , and endemic goitre is non - existent ( rundle , 1951 )  . thyroids there weigh on an average 14 g . 
and carcinoma of the stomnach and oesophagus , when considering separate states . ( 10 ) australia and new zealand . australia is considerably more industrialised than new zealand and has many furthermore , rodent ulcer is large cities as compared with the latter country . infinitely more common in australia , where goitre does not obtrude as a major health problem , though there are certain areas where there are definite , if small , districts where goitre is found ( kelly , 1946 )  . 
the more rural and agricultural population of new zealand has here goitre is a major health problem and its a death rate from cancer of 14 - 56 . incidence in europeans , maoris and animals alike has been closely studied for years . 
as metabolic rate is in general a rough indication of thyroid activity , there would be appear to be some relationship between malignant disease and thyroid thus , the lowered metabolic rate often seen in diabetes mellitus dysfunction . ( joslin , 1946 ) may be considered with the increased liability of diabetics to develop carcinoma in any site or organ as compared with non - diabetics ( joslin , 1946 )  . in the same way , the lowered metabolic rate commonly found in patients with all types of peptic ulcers ( kolmer , 1949 ) may be considered with the incidence of carcinoma of the stomach - still one of the commonest neoplasms of man . ( 2 ) it has long been observed that puberty and pregnancy are periods when goitres may appear ( marine and lenhart , 1909 ; marine , 1935 ) , and may disappear when the period of excessive demand ceases or when iodine is given . these are also the periods when melanomata tend to increase in size and may , not infrequently , become malignant . 
at the beginning of this year rwas admitted to this hospital on account of malignant melanoma with spread to glands in the course of her third pregnancy . in her two previous pregnancies she also developed malignant melanoma on each occasion and was in this hospital in consequence . she has a moderate enlargement of the thyroid of the smooth " colloid " type seen commonly in pregnancy . 
the end of pregnancy is also the period when chorionic carcinoma and lactation carcinoma of the breast occur - perhaps the most rapidly growing class of cancer known . ( 3 ) administration of thyroid has been found to improve the action of oestrogens in the treatment of carcinoma of the prostate , permnitting the effective use of smaller doses of oestrogen and delaying the onset of insensibility to oestrogen ( winsbury white , 1948 )  . in support of this clinical experience a paper in endocrinological research is quoted ( chu and you , 1945 ) , but the final conclusions of these workers was that the simultaneous administration of oestrogen and thyroid was the same as that obtained by thyroid feeding alone . ( 4 ) reduction of keloid formation can often be brought about by administration of thyroid . 
the age for the start of the decline in iodine content of the thyroid coincides in general with the age at which malignant disease in mnan becomes a prominent feature . ( 7 ) in the second week of january of this year there were at least three patients in this hospital at the same time with gross goitre and cancer . m - - , carcinoma of breast and a large colloid goitre visible seven or eight beds away down the ward . e - , lymphosarcoma and a thyroid that weighed 80 g . 
the nodular goitre caused some difficulty ing involvement with growth . during resection of glands of neck . since january other patients have been seen in the wards of the hospital with coexistent carcinoma and goitre . it is relevant to note that the area from which this hospital draws its material , gloucester , somerset and cornwall , is not one in which goitre is frequent . ( 8 ) the association of goitre and malignant disease in the post - mortem room was strikingly illustrated by analysis of 1000 post mortems at the middlesex hospital ( stocks , 1924 ) , when anomalies of the thyroid were found in 13.3 per cent of males and 21.2 per cent of females of 500 persons dying of cancer ; whereas only 2 - 0 per cent of males and 6.5 per cent of females dying of non - cancerous conditions showed anomalies of the thyroid . professor barlow excluded from these anomalies secondary invasion of the thyroid by cancer , and the anomalies most frequently found were simple parenchymatous enlargement and adenomatosis , while calcified nodules , cystic changes , atrophy and fibrosis were frequent . 
of dba ( bather , 1952 )  . ( 3 ) rats bearing walker rat carcinoma 256 were treated with natural thyroof these 27 per cent showed complete remission and 12 per cent " favourxine . able " histological response , 68 per cent . 
showing no response at all . another group treated with synthetic hormone gave only 2 per cent of remissions and no response in 98 per cent of animals . 158 animals were involved ( herbut , kraemer , and jacksen , 1950 )  . regression of rat tumours may be induced by thyroxine the natural comment . hormone being superior to the synthetic . ( 4 ) feeding butter yellow ( p - dimethylaminobenzene ) to rats produced malignant neoplasms of the liver . 
the recent work of moon , simpson , li and evans ( 1950a , 1950b , 1952a , 1952b ) has convincingly confirmed the conclusions of earlier workers twenty years ago ( ball and samuels , 1932 ; bischoff , maxwell and ullmann , 1934 ) , that whereas extracts of the anterior pituitary cause tumours to arise in a variety of sites in laboratory 408 j . 
spencer iodine availability , traced by goitre incidence , appears to be one of such factors . closer scrutiny of some of these countries corroborates these conclusions . clinical findings and a review of some of the experimental work available lend further emphasis to these observations . the apparent relationship of thyroid insufficiency and the liability to develop cancer is discussed in connection with such other hormonal influences over cancer as are already known , particularly in respect of the pituitary . lines of investigation and clinical trials have been started , but results of any value cannot be expected for several years . a non - specific organ immunity or susceptibility seems to be the simplest explanation of the facts presented , and the possibilities , preventive and perhaps therapeutic , that are opened up by this line of research are briefly discussed . i am indebted to polak of amsterdam for fig . 
calcutt. from the department of cancer research , mount vernon hospital and the radium institute , northwood , middlesex . received for publication may 3 , 1952 . the staining of living tissues , either in vitro or in the form of freshly excised material , is a well recognised technique . normally it is restricted to the identification of specific morphologic entities such as mitochondria . attempts to determine intracellular biochemical features have been rather unsuccessful as far as living material is concerned , although successes have been achieved with fixed specimens . 
the availability of tetrazolium compounds now has rendered possible further attempts at the identification of intracellular sites of reduction . three compounds are generally available . in their normal state they form colourless solutions , but in the presence of suitable reducing groups they are converted to coloured formazans . 
 it has recently been demonstrated that the most critical factor determining the epidermal mitosis rate in the adult mouse is the carbohydrate supply to the cells , and the evidence at present available all points to the conclusion that the function of this carbohydrate is to supply the energy needed during cell division in extending this work the discovery has been ( bullough , 1949a , 1950a , b )  . 
 made that a restricted diet has a powerful effect in depressing mitotic actirity ( bullough , 1949b ) , and it has been suggested that this obserration may help towards an explanation of tannenbaum 's remarkable results on the effects of restricted diets on tumour genesis ( tannenbaum , 1940a , 1940b , 1942 , 1944 , 1945 , 1947 )  . 
this involved a study of the results obtained with a graded series of diets as regards body weight , blood sugar concentration , liver glycogen content , and epidermal mitotic activity . 
 the two experiments performed involved a total of 55 mice , which were all in the first experiment the 25 adult males of between 3 and 5 months of age . 
 these mice had been reared since weaning on a mixed diet of commercial rat cake with cod - liver oil , flaked maize , and dog biscuit , but during the experiments they were fed on commercial rat cake alone . 
this deter mined the form of their diurnal cycle of mitotic activity , and ensured that a high mitosis rate developed shortly after midday ( bullough , 1948 )  . 
it was unfortunate that the animals in the first experiment were considerably lighter than those in the second experiment , but it was remarkable how little this fact affected the results obtained . 
 on the day when each experiment began a piece of ear was removed from each animal at 14.00 hours , the normal time of maximum epidermal mitotic activity associated with the afternoon sleep period . 
the animals were killed at 1500 hours , it having been previously determined that for a period of about 5 hours after the injection of this weight of colchicine there is no great disturbance of the mitosis rate or of the blood - sugar level ( bullough , 1949c )  . 
the liver was removed , cut into two roughly equal parts , and the glycogen content was converted into glucose by the method of good , kramer and somogyi ( 1933 )  . 
 in estimating the epidermal mitotic activity the pieoos of ear , fixed in bouin 's alcoholic fluid and embedded in ester wax ( steedman , 194 7 ) , were cut into sections 7 thick . 
 255097 217096 200076 199 : : : ! : : 075 197078 100 , , - : 250097 261085 267075 25 - 1 + 092 279 ; 0 - 97 in the second experiment only strong 's cba males were used , and these , being 4 months old when the food restrictions began , were heavier than the mice of the first experiment . 
 252068 244 : : : ! : : 052 218043 21 4052 21206 . ' ; 90 0 ' .o 247150 257118 252130 253075 246070 table ii . - the average body weight ( in grammes ) in group& each of 5 adult male mice fed on restmtetl diets of rat cake . 
 306116 288 : : : : : 115 279075 283070 299094 the results obtained were much as could have been expected , the figures for the groups on the lower diets falling steadily as the weeks passed . 
by the end of the fourth week it is clear that the relationship between body weight and diet is a direct one which can be expressed by a straight line graph . 
 since it is evident that mitotic activity is closely associated with carbohydrate concentration , the carbohydrate reserves were estimated at the close of the experiments in terms of the liver glycogen content and the blood sugar concen tration . 
 233 12 l 214448 200045 183459 172323 240619 218 133 199422 187413 18001 - .~ 175108 superficial examination of table iv might suggest that the poorer the diet the higher the blood - sugar level . 
at that time the blood - sugar level must have been low ( bullough , 1949b ) , and with a coincidentally low secretion rate of insulin the effect of the meal must have been to raise the blood - sugar level to abnormal heights . 
it is thus logical that the poorer the diet the higher the blood - sugar level should be , and once again the relation is a direct one expressible as a straight line graph . 
 75029 36042 25017 23018 22024 one surprising conclusion that can be drawn from these figures is that the imposition of a restricted diet results in an extremely rapid fall in the mitosis in most groups there was a steady reduction throughout the whole experi rate . 
i these results are expressed graphically , the figures chosen for com parison being ~ose of the numbers of mitoses observed after 3 weeks ( without colchicine ) and after 4 weeks ( with colchicine )  . 
it appears that in general the mitosis rates of the lighter mice of the first experiment were lower than those of the second experiment , but the differences are remarkably slight and are of doumful significance . 
 the most significant point emerging from these graphs is the indication given both with and without colchicine that the relationship between resmcted diet and mitotic activity is not a direct one . 
 the present results confirm earlier observations that restricted diets cause a pronounced fall in mitotic activity , and indicate that when less than 70 per cent of the normal food intake is given the epidermal mitosis rate is reduced to about 35 per cent of the normal . 
on the basis of earlier work it can be safely suggested that this reduction is caused by a shortage of carbohydrate , in the form of glycogen or glucose , in the epidermal cells themselves ( bullough , 1949a , 1949b , 1949c , 1950a , 1950b ; bullough and eisa , 1950 )  . 
at this time the fall in the body weight is only just beginning , and it is therefore evident that a mouse is unable to maintain a high rat , e of cell division by means of the utilization of fat deposits . 
 in a fully - fed four - month - old mouse of about 35 g . , as in a fully - fed three - month - old mouse of about 25 g . , the epidermal mitosis rate reaches a sleep maximum of about 75 mitoses per c similarly in either case the food intake remains steady at about 36 g . 
 ' when fed on restricted diets the mice lost weight in a regular manner week by week , the speed of loss being in direct proportion to the degree of underfeeding . 
 in a similar manner the carbohydrate reserves , as indicated by the liver glycogen content , fell after 4 weeks to a level which was directly proportional to the amount of food given . 
2 , in which for comparison a graph of the present results is in both cases the form of the graph is sigmoid , and in both cases the included . 
this adds further support to the thesis put forward by bullough ( 1949b ) , and developed in the following review ( bullough , 1950c ) , that the rate of tumour genesis in a particular tissue or in the body as a whole may be directly related to the mitosis rate . 
the mitosis rate in turn is related to a tariety of factors , of which one of the most important is the carbohydrate , or calorie , content of the food . 
 groups of adult male mice were maintained for 4 weeks on diets varying from 55 per cent to 105 per cent of what they would eat if fed ad libitu weekly records were made of the body weights and epidermal mitosis rates , and at the end of the experiments the carbohydrate reserves were estimated in terms of liver glycogen content and blood - sugar concentration . 
die greatest mitosis depression accompanied a reduction from 80 per cent to 70 per cent of the normal diet , a result which compares closely with that of tannenbaum ( 194 7 ) regarding the effects of restricted diets on carcinogenesis . 
 ( karnofsky , burchenal , armistead , southam , benstein , craver and rhoads , 1951 ) , therefore , aroused much interest . human trials on the hazards of water contamination carried out by the american army medical centre indicated that aliphatic nitrogen mustards might be absorbed after oral administration : hn3 in a total dose of 15 to 18 mg . 
the walker tumours were passages of tumour cell suspension in dextrose , prepared by craigie 's mincer technique ( craigie , 1949 ) and preserved at - 70 ' c . 
the mouse sarcoma was treated daily for 7 days . in the tests against the walker tumour the total dose was given over 7 , 8 or 10 days , and ajso as a . 
single dose ( boyland , cleg , koller , rhoden and warwick , 1948 ; haddow , kon and ross , 1948 )  . eleven to fifteen animals were used for test . the water - soluble drugs were dissolved in distilled water immediately before administration and given orally or intraperitoneally . 
of distilled water was passed through the tube to ensu - re that the whole dose was washed into thl - , stomach . r 48 was given in a single oral dose in arachis oil . control animals received the solvent by stomach - tube or remained untreated . 
the walker tumours and sarcomata 37 were dissected 14 and 9 days respectively after transplantation , fixed in bouin 's fluid and 70 per cent alcohol , dried between filter - paper , and weighed . the difference in weight between control and treated tumours was analysed statisticafly . 
the maximum tolerated oral administered orall dose was about twice the maximum tolerated intraperitoneal dose . using these doses , both oral and parenteral treatment produced similar effects against the walker tumour ( table 11 )  . 
the oral activity seeme ' d to be influenced by the distribution of the total dose ; the weight ratio between control and hn2 - treated tumours became more significant when the total dose was divided over 7 instead of boyland , cleg , koller , rhoden and ' " tarwick ( 1948 ) found over io da - ily doses . that the parenteral activitv of nitrogen mustards increased when the total dose was given as a single injection . 
when given in a single oral do the effect of hn3 was negligible , whereas the activity of hn2 and nor hn2 seemed to be increased to a certain extent . 
the oral activity of nor hn2 seemed at least equal to that of hn2 , and more pronounced than that of hn3 , but even the highest weight ratios between control - tumours and those treated with the ahphatic compounds were only about one - quarter of the ratio recorded after treatment with r 48 ( table ii )  . 
the other aromatic nitrogen mustard tested , nn - bis ( 2 chloroethyl ) p - phenylene diamine hydrochloride , when given as a single oral dose of 4 mg . 
peczenik the adult group ; the ratio was about 3 times that recorded in the young animals - seven tests only were performed in duplicate , six of them against the walker in the three tests with the young rats the duplicat - e results agreed , tumour . whilst in the three tests carried out with the adult rats the duplicates agreed in two but disagreed in the other ( intraperitoneal treatment with hn3 )  . 
the maximum tolerated oral dose of nor hn2 was about 10 times larger than that of hn2 and 14 times larger than that of hn3 ( table 11 )  . 
the therapeutic ratio of hn2 and hn3 , whether the drugs were given intraperitoneally or orally , seemed as low as 2 , or even lower . as estimated from the death - rate , hn2 and hn3 were more toxic to tumourbearing than to normal rats . 
was toxic to adult but tolerated by young tumour - bearers . effect of nitrogen mustard8and triethylene melamine on body - weight . the tumour - inhibitory effect of the agents investigated was frequently assoin some instances , more frequent in ciated with inhibition of somatic growth . the adult than in the young rats . 
the experiment is described here because it has been suggested that urethane potentiates the effect of nitrogen mustards clinically . three groups of adult bearers of walker tumour received hn3 orally in a daily dose of 0 - 4 mg . 
of urethane daily , a dose of urethane whichper8e is known to be inactive against the walker tumour . another group received unstandardized adrenocortical extract ( eucortone ) intraperitoneally , i ml . 
peczenik from that of the controls during the first few days inhibition of the walker tumour became manffest during the second week , suggesting that the agents clid not influence the " take " of the transplants . the therapeutic ratios of hn2 and hn3 are probably not lar er after oral than after intraperitoneal administration . in non - tumour - bearing rats fed with hn3 , roberts ( 1952 , personal communication ) found changes in the intestine very similar to those described by several authors after injections of nitrogen mustards ( selye , 1950 )  . in view of this finding , it is worth noting that most of the tumour - inhibition shown in this paper was associated with significant suppression of somatic growth , whether the drugs that held true even when the net weight were given intraperitoneally or orally . ( body - weight minus tumour - weight ) was considered instead of the gross weight . thus the question arises to what extent the tumour - inhibition recorded after oral administration of the agents was due to a specific effect or to starvation . 
walpole ( 1951 ) has fo - und 40 per cent growth - inhibition of untreated walker tumours when ifthis 40 per cent ofthe observed somatic growth was prevented by underfeeding . tumour - inhibition is deducted from the figures in tables i to iv , the maximum .tolerated oral dose of hn3 would appear to be inactive in adult tumour - bearers ( table iv ) whilst the significance of the other results remains unchanged . it may be assumed , therefore , that the retardation of tumour - growth described above was this view is supported by the finding mainly due to other causes than starvation . that the suppression of tumour - growth after a single oral dose of r 48 or nor hn2 was not associated with suppression of somatic growth . moreover , - whilst effects , on tumour - growth were similar , effects ' on body - growth were more pronounced after intraperitoneal than after oral treatment . 
most of the animals on both diets lost weight during the treatment , and the ratio between the weight losses in rats with the 20 per cent and the 5 per cent protein diet was almost the same as the ratio of the degrees of tumour - inhibition . according to houck , crawford , bannon and smith ( 1947 ) , animals treated with nitrogen mustards lose body weight by loss of protein and water . 
the rats under these experiments , therefore , though fed with loss of protein may also intensify a high protein diet ( 19 - 2 per cent ) , lost protein . according to elson ( 1951 ) , the effect of inhibitors on tumourand body - growth . as an initially large dose of an inhibitor is gradually reduced , the animal will recover from the inhibitory action quicker than the tumour will , and the latter may completely regress under high protein diet . my experiments in which the drug was given in a single dose the loss of protein ceased in time to arow the animal to recover its growth - rate whilst tumour - growth remained retarded . it may well be that in those summary . administered intraperitoneally in about maximum tolerated doses , nor hn2 , hn2 and hn3 had approximately equal activity against the walker carcinosarcoma , although aaainst the sarcoma 37 , hn3 was more active than hn2 . the walker tumour was significantly more affected by triethylene melamine than by the aliphatic nitrogen mustards . 
r 48 was at least 4 times as active as the aliphatic bis ( 2 chloroethyl ) p - phenylenediamine was active after intraperitoneal amines . but inactive after oral administration . bromine substitution in hn2 and hn3 seemed to cause loss of activitv . triethylene melamine given orally was practically inactive in the non - fasting rat , whereas the same dose given to the fasting animal had marked activity but was toxic . tumour - bearing rats tolerated r 48 and nor hn2 in doses respectively 36 and 10 times the maximum tolerated dose of hn2 . 
the smith type is still , however , a relative rarity and less than a score of cases have been reported since the original description in 1934 . the forowing case , the second to be seen in south africa , closely resembles that originally described by smith ( i934 ) ; but it is unique in that the . 
he had suffered since 1942 from recurrent spontaneously heahng tumours of the left face , ear , neck , chest , shoulder and upper arno other member of his family was known to have suffered from any similar disease ; and he was not related to the other south african who suffers from the smith type of morusca pseudocar ' c ' momatosa . skin generally was normal for his age and was not hypersensitive to sunhght . his occupation as a contractor kept him mainly in the open . 
he had never been exposed to tars , mineral oils or arsenic . he stated that the tumours , of wbich he usually had several active , began like festering blackheads " , grew for 4 - 6 weeks , and then began to regress and disappeaxed , leaving scars , in 4 - - 6 months . 
on his first visit he had two active tumours on the back of the left ear and one over the left scapula and thirty depressed wbite scars on the left side of the nose , upper hp , cheek , ear , neck , chest and upper arthe scalp and buccal mucosa were unaffected . 
a month later the ear lesions were distinctly smaher and flatter and that over the scapula had flattened dow - n to a coin - like plaque with rolled edges and a central area of soft keratinous material . all the lesions were chnically indistinguishable from squamous epitheliomata . 
at this visit a fresh lesion , i mm . , was discovered iin the angle of the left ear lobe and cheek it closely resembled , as the patient had described , a festering blackhead . the patient , who b . - ilieved himself to be suffering from skin cancers , has on several occasions been subjected to biopsy or excision of tumours ; and a diagnosis of squamous epithlioma had generally been made . x - ray therapy had also been given niore than once with little impression on the rate of healing of the tumours ; but the scars left in such areas were more mutilating than those seen after spontaneous healing . a portion of one of the lesions on the ear was excised for histological examination and we examined several sections of lesions excised in the past by d . 
the stretched and atrophic epidermis covering the lesion is between the central mass of keratin and the covering epithelium are seen on the left . irregular and well - differentiated masses of epithelium and cell nests . 
the recently developed methods of detection and determination of polycyclic hydrocarbons in micro - gram quantities have provided a more sensitive way of analysis than has yet been employed ( cooper , 1951 , 1953 ; wedgwood and cooper , 1951 , 1953 )  . in view of the suggested connection between carcinoma of the lung and smoking ( menary , 1932 ; schrek , baker , ballard and dolgoff , 1950 ; mirs and porter , 1950 ; dor and hill , 1950 ; rigden and kirschoff , 1952 ; sadowsky , gilliam and cornfield , 1953 ; wynder , graham and croninger , 1953 ) and the estabhshed presence of carcinogenic hydrocarbons in combustion products , it was decided to use these methods to examine cigarette smoke . 
on the other hand several investigators have devised apparatus to collect smoke produced in conditions resembling closely those of normal smoking ( bradford , harlan and hanmer , 1936 ; wenusch and sch6ller , 1938 ; w , ynder , graham and croninger , 1953 )  . the apparatus we have employed . 
the tap c with a glass rod sealed on to it was turned on for the period necessary to simulate a " draw " made by a snioker by means of a cam attached to the periphery of a 3 inch pulley wheel , d . the glass rod was held in the groove of the puuey by means of a stretched rubber this wheel was driven by a gear train from a smar electric motor , the speed band . of which was variable by adjustment of a " variac " auto - transformer connected to the altemating current mains . other cams could be attached to the wheel and thus the length and frequency of the " draws " were adjusted . in the u - tubes suitable solvents were placed so that the smoke was made to bubble tbrough them and the condensable material separated from the gas . a packing of 10 cof pyrex glass wool in the second u - tube served to remove the both u - tubes could be surrounded by beakers last traces of condensable matter . full of solid carbon dioxide to assist in the condensation , but it was found that strong cooling was not always necessary to effect complete removal of the disperse phase . 
each , the average time of draw is about 2 seconds and the average time of smoking such a cigarette to a short butt ( about 1 - 5 clong ) is 12 minutes . these conditions are attained by oiir apparatus when adjusted to give a 2 second draw every 45 seconds with a negative pressure of 25 cwater . 
air. smoke obtained in this way is an aerosol with a viscous fiquid as the disperse phase and a gas , consisting of a mixture of unburnt air , carbon dioxide , carbon monoxide , water vapour and traces of other gases as the dispersing medium . the average amount of condensable material from 100 c ' igarettes weighs about 4 g . we have concemed ourselves only with the condensable disperse phase whicli in bulk , after the evaporation of the solvent ( acetone , chloroform or cyclobexane ) used to trap it , is a dark brown viscous fluid . preparation of apparatus and materials . the solvents ( cyclohexane , acetone , benzene and chloroform of reaaeint grade ) were distilled in an all - glass apparatus , rejecting the first and last tenths . this product was then distilled through a dufton column and corected over a range of - 9jo c . 
the residues were not fluorescent in ultra - violet hgbt . all the glass apparatus employed was cleaned bv immersing overnight in chromic - sulphuric acid mixture , washing and drying . 
500 ultra - violet spectrophotometer . graphy the eluates were examined at a few definite wavelengths only and hydrocarbons were identified by specific absorption peaks and the order in which they appeared in the eluates . 
the solvent was then removed by distillation , the residue boiled twice with cyclohexane ( 5 to 10 ml . ) and the solutions decanted off after cooling . the - united cyclohexane solutions were then shaken with three quantities of 2nsulphuric acid and then with three quantities of 2nsodium hydroxide . solution thus freed from basic and acidic substances was reduced to about 5 ml . 
the eluates from the colunm were examined by the method of wedgwood and cooper ( 1953 ) namely by searching for absorption peaks at wavelengths known to be specific for the various polycyclic hydrocarbons . 
usuahy the initial chromatography only revealed the hydrocarbon peakb as inflexions againbt considerable background absorption and the combined filtrates suspected of containing the compounds had to be passed through fresh columns in order to reveal their presence more satisfactorily . anthracene was recognised by its peak at 376 ma . 
and it was always followed closely by the appearance of a peak at 355 m / % , reveahng pyrene . the compounds were determined bv making the cyclohexane solutions up to known volumes and then measuring the height of the peaks by the base line technique . for this purpose two convenient points on either side of a given peak calibration of the peak heights above the base were used to construct a base line . line was effected by using standard curves of the authentic hydrocarbons prepared from solutions of known strength . the background absorption interfered considerably in these experiments and various attempts were made to reduce its effect . 
when hydrolysis was effected on the cyclohexane extract of the whole smoke , the background absorption was even greate ' r than before , indicating that some hydrolysis products of the smoke constituents were entering the hydrocarbon sections of the column . the presence of pyrene and anthracene indicated in these experients was confirmed by their chromatographic behaviour relative to added methyl ethers . relatively few compounds , absorbing hght in the region studied , are associated with the polycychc hydrocarbons on aluniina columns . 
the peaks used for recognition of the various compounds are labened with their wavelengths . it will be noted that a sequence of peaks of added calibration materials interspersed with the recognisable peaks of substances originary present , gives an infalfble method of identification and determination . 
the results of a number of analyses utilising in all 250 cigarettes of one popular brand showed quantities of anthracene and pyrene equal to 10 - 2 and 9 - 0 itg . 
and to paraffms which he states are present in t e original tobacco and are vaporised unchanged during smoking . acetylene has been determined in tobacco smoke by weighing it as cuprous acetyhde ( fishel and haskins , 1949 )  . its pyrplysis may give a ready explanation 300 b . 
was attained at the hottest part of the periphery . more satisfactory measurements were made by using a calibrated coppernichrome thermocouple which was threaded through the cigarette from one side to the other . after sealing the holes by means of small pieces of paper , the cigarette was smoked in the normal way and the temperature recorded from time to time . 
the temperature rose rapidly when the burning end advanced towards the couple and , when the glowing material was in contact with the couple , a temperature of about 650 c . 
each time air it thus appears that the highest temperatures during was being drawn in . suction are confined to the surface and that the main body of the hot end is always at a temperature between 650 and 700 c . similar temperatures were recorded when a cigarette with a thermocouple inserted was smoked in the mouth . these temperatures are sufficiently high for pyrolysis of simple compounds to polycyclic hydrocarbons . 
the temperatures recorded by us agree remarkably closely with those obtained independently by wynder , graham and croninger ( 1953 )  . our investigations upon the composition of tobacco smoke are being continued . the authors wish to acknowledge the helpful and kindly criticism given by professor sir e . 
legon. from the department of geography , the london school of economics and political science . received for publication april 20 , 1951 . in considering the heavy mortalities from gastric cancer that exist in the counties of northern and western wales ( stocks , 1936 ) , the writer wondered whether mortality was uniform over the area , or whether there were marked local variations within it . 
the low - mortality rural districts of eastern montgomery and of radnor ( 70 deaths ) are well drained , in contrast to the rural districts to the west , which lie on an ill - drained plateau with extensive tracts of bog . 
the impermeability of the rocks of anglesey ( 203 deaths ) , and the extreme flatness of much of the island , make for peat accumulation , despite the fact that rainfall is light compared with that of the highland parts of north wales . case involving the pennant grit . it may be stated , therefore , that the rural districts of low mortality are all on the sheltered east and south of the welsh massif and are well drained . 
legon huntingdon , ely , peterborough and the holland division of lincoln ( stocks , 1947 ) , since these four counties alone in england have proportionally large areas of peaty fen soils . apart from the typically high organic content of their soils , north wales and the fens have little in common . 
as further information ( marston , 1951 ) is made available , it may prove worth while to consider whether a carcinogenic substance exists in food - plants grown on these soils . the possibility of an association between soil organic matter and cancer mortality was expressed verbally to the author by g . 
orr. from the department of pathology , univer8ity of birmingham . received for publication may 7 , 1953 . when a carcinogenic agent is applied to the skin of a mouse epithelial hyperplasia follows in the course of a week or two . if the applications are then stopped , the epidermis reverts to a histologically normal appearance , but if hyperplasia is again induced by the co - carcinogen croton oil , tumours of the skin will in due course be elicited . it is clear that the apparently normal skin has been altered in some way by quite a short treatment with carcinogen ( a single application of a powerful carcinogen will suffice ) , so that further growth - stimulation by an agent not itself carcinogenic completes the process of tumour induction . attention was first drawn to this phenomenon by berenblum ( 1941 )  . 
mottram ( 1944 ) showed that a single application of 3 : 4 - benzpyrene would suffice to produce tumours if followed by a course of croton oil paintings . in a full analysis of the factors involved , berenblum and shubik ( 1947 ) adopted the terminology of friedewald and rous ( 1944 ) , the effect of the preliminary carcinogen being described as the " initiating " factor , and that of the croton oil ( co - carcinogen ) as the " promoting " factor . both these factors were conceived as causing changes in some of the epithelial cells themselves . there is evidence , however , that the effects of carcinogens are not attributable wholly to the direct changes brought about in the epidermis . various authors have drawn attention to the progressive changes that occur in the dermis during experimental carcinogenesis of the skwhen the technique of grafting different components of the skin became available ( billingham and medawar , 1951 ) , an attempt to evaluate the relative importance of epidermal and dermal changes in the evolution of cancer was undertaken by billingham , orr and woodhouse ( 1951 )  . they transferred the fully treated epidermis alone to an untreated site prepared on the opposite side of the mouse 's thorax . in these conditions this epithelium no longer gave rise to tumours , though the reciprocal transfer of untreated epidermis to a bed cut in the carcinogen - treated site gave a yield of tumours approximately equal to what might have been expected had no operative treatment been undertaken . in view of these findings there appears to be another possible explanation of the phenomenon of co - carcinogenesis , namely , that after short treatment with a carcinogen the dermis is sufficiently altered to permit tumour induction when further epidermal hyperplasia is evoked by croton oil . 
the cutting of these grafts was greatly facilitated by the hyperthe rectangular slices plasia of the epidermis due to the carcinogen treatment . were floated raw side down on 0 5 per cent commercial trypsin solution and incubated at 38c . 
i. - experiment j : each horizontal strip represents the survival of a mouse after the grafting operation ( life line )  . oblique shading represents a papilloma , solid black shading a malignant tumour . 
an oblique line cutting the life line indicates operative removal of a tumour . the rate of appearance of tumours on the original methylcholanthrene - treated area after removal of thin thiersch grafts is indicated by the shading in the life line . 
orr treated site after removal of thin thiersch grafts in 16 out of 37 animals . 10 cases these tumours were removed to prolong the life of the animal . in 7 of these further tumours occurred , but 3 of them later regressed . the time range from operation to the appearance of a first persisting tumour was from 0 to 420 days with a mean time of 48 27 - 6 days . 
the survival of these mice from first croton oil painting ranged from 173 to 330 days ; some are still alive and under observation . these times are not , of course , comparable with those for the experimental animals , where the datum line was placed at the time of grafting . the total incidence of tumours on the grafted site is thus not very different from that induced by croton oil alone . there is a qualitative difference in that one of the tumours on the grafted site became conventionally malignant . 
by comparison , the original treated site yielded tumours in 16 of the same animals , 8 of them clinically and histologically malignant , without co - carcinogenic treatment on that site . the results in general of this experiment do not support the view that the transplanted epidermis contained latent tumour cells . 
the result is not , of course , unequivocal , but the occurrence of a single carcinoma does not suggest that many irreversibly altered cells can have been present . an attempt is in progress to find the effect of preliminary grafting of normal skin , followed by treatment with croton oil , in order to see whether the operative treatment of the dermis modifies the effect of croton oil . it is technically difficult to prepare pure epidermal grafts of normal thoracic epidermis , but experiments are in progress with re - implanted thiersch grafts . experiment k : reimplantation of a pinch graft cut from carcinogen - treated skin . billingham , orr and woodhouse ( 1951 ) made a few observations on the effects of cutting pinch grafts from the carcinogen - treated area , and reimplanting them at the same site . these experiments were undertaken to control the results of transplantation and in particular to make certain that the detachment of the superficial skin was not in itself the reason for the paucity of tumours when it was transplanted . 
the grafts were then replaced and the surrounding gap , caused by retraction of the skin around the wound , was dusted with sterile animal charcoal to mark the graft position . 
2. of 17 grafted mice surviving beyond the time of first tumour appearance , 11 produced tumours , but these regressed on 5 animals so that only 6 mice had tumours present at death . 
the tumours appeared after 8 to 200 days ( mean 42 17 - 3 days ) from the time of grafting the experimental group of animals . eight tumours became malignant after 20 to 100 days . 
the mice survived after grafting for 38 to 230 days ( mean 98 11 days )  . it will be seen that 70 days after the reimplantation more tumours were present on experimental animals that controls , and it seemed that the tumour production was indeed being augmented by the grafting operation as in the previously reported experiment . however , after about 100 days several tumours on the experimental animals regressed - a much less frequent occurrence in control animals . the outcome was that the proportion of animals bearing tumours at their deaths was no greater in the grafted animals than in the controls . 
2. - experiment k : the rate of appearance of tumours in the bridge epithelium over the scar around the reimplanted pinch graft of carcinogen - treated skin is indicated by shading in the life line and persistent tumours by the letter s . 
tumours arising on grafts themselves are shown by shaded blocks above the life line and persistent ones by the letter g . tumours arising outside the grafts are shown by shaded blocks below the life line and persistent ones by the letter o . 
1. experiment l : reimplantation of thin thiersch grafts cut from carcinogen - treated skin . in this experiment thin thiersch grafts were removed from the carcinogentreated area as described in experiment j . 
as great an area of the carcinogentreated skin as possible was taken off and the pieces were then planted back again , in some cases after smearing the graft beds with animal charcoal to mark them . the results are shown in fig . 
the mice survived from 69 to 230 days ( mean 124 + 12 - 5 days )  . tumours appeared on 5 out of 18 control ungrafted mice after 16 , 20 , 23 , 24 all became malignant . 
the mice survived from 38 to 230 days and 200 days . ( mean 99 14 - 2 days )  . experimental animals control animals 4222 4223 4225 4246 4247 4248 4249 i 4250 4488 z 4493 4494 4498 4499 4500 4502 4206 4207 4208 4209 4210 4227 = r_ 4229 4230 4474 4475 4476 4477 4478 4479 4480 4481 4483 4495 z 77 days after thiersch graft operation fig . 
3. - experiment l : the rate of appearance on reimplanted thiersch grafts of carcinogenblocks of shading below the line indicate treated skin is indicated by shading in the lifeline . tumours outside the grafted area . 
some of them , such as age , sex and diet are fairly easy to control . others , such as range of temperature and amount of carcinogen administered , may be less easily controlled . 
orr of animals such as were used in the present experiments . may strike at any time . parasites and infections experiment m : the insertion of cotton threads into the dermis of carcinogen - treated skin and their removal after 2 weeks . orr ( 1934 and 1935 ) showed that preliminary alteratioii of the dermis , by the introduction of linen threads and their subsequent removal before treatment with a carcinogen led to a significantly earlier appearance of tumours . 
we thought it of interest to see what happened if the threads were introduced after the standard preliminary carcinogenic treatment of the present experiments . fine white cotton button - thread was threaded into the finest ordinary sewing needle which would take it and then sterilised . the needle was inserted into the skin of the anaesthetised mouse just outside the carcinogen - treated site . was passed through the dermis of the treated area as near to the surface as possible , endeavouring not to injure the treated epidermis itself , and out through the cotton was carefully pulled through and the surface beyond the treated area . the procedure repeated again under another part of the treated area . the thread was passed under the treated skin in both directions about half a dozen times in all and left in situ for 2 weeks . at the end of this time the projecting loops of cotton were cut and the threads carefully pulled out of the skin under anaesthesia . unfortunately the threaded area had not been covered over and many of the mice had scratched and tugged at the loops of thread , resulting in some damage to the carcinogen - treated epidermis itself '  . the results are shown in fig . 
5. persistent tumours appeared on 10 of 19 experimental animals in 9 to 92 days ( mean 35 7 * 9 days )  . eight tumours later showed malignant changes . 
orr croton oil , the tumour yield is only very slightly greater than that obtained by croton oil on otherwise untreated skin . of the few tumours so produced , all except one were papillomata , which appeared somewhat earlier than might have been expected with croton oil on previously untreated intact skthe single exceptional tumour was a carcinoma , an unusual occurrence with simple croton oil treatment , but it has to be remembered that grafting was delayed up to the time that tumours were already beginning to appear on the original methylcholanthreneexperimental animals control animals 77 , , / , , , , z , , 4358 4361 4369 4370 4372 4373 4374 ' .. 
the results of berenblum and shubik ( 1947 ) were explained on this basis by postulating a two - stage process , the first stage being the alteration by a sudden and irreversible process of a few normal epithelial cells into latent tumour cells , the second the conversion of these latent cells into visible tumours . the first stage ( " initiating process " ) requires a carcinogen ; the second ( " promoting process " ) can be brought about by various non - carcinogenic hyperplasia - inducing factors , of which croton oil is the most fully analysed . it appears to us that the facts elicited by berenblum and shubik are explicable without reference to the conception of latent tumour cells , and that an irreversible change inflicted on the carcinogen - treated site as a whole , and perhaps particularly on the supporting tissues , would explain the olbserved phenomena of co - carcinogenesis . in one respect the view we put forward offers a more satisfying basis for one of the berenblum and shubik findings . 
they showed that even after as long an interval as 20 weeks between the initial painting with carcinogen and the subsequent croton oil treatment , the total tumour incidence remained undiminished as compared with shorter intervals . if , therefore , latent tumour cells were there all the time , it would be necessary to assume that they did not participate in the normal processes of desquamation . it is also relevant to point out that blum ( 1944 ) has analysed the results of carcinogenesis by mathematical methods , and reaches the conclusion that the available data are not consistent with the hypothesis of a discontinuous two - stage process . if the dermal and subcuticular changes are of importance to carcinogenesis , the most obvious way in which they could act would be by interference with the nutrition and metabolism of the overlying epitheliuthe latter does not carry blood vessels , and is dependent on the functional effectiveness of the stromal tissues . it has previously been pointed out that the rate of evolution of the dermal changes ( in simple treatment with a carcinogen ) is of the same order as the potency of the carcinogen in terms of time taken to produce tumours . it may therefore be asked why a single application of a carcinogen followed by a co - carcinogen is effective at all in the induction of tumours . 
a possible explanation is that the hyperplastic epithelium following the co - carcinogen is susceptible to degrees of dermal change and vascular impairment which would not effect normal epithelium or epithelium in a less vigorous state of multiplication . 
orr the reimplantation studies of experiments k and l necessitate some modification of the conclusions drawn from the previous reimplantation of billingham , orr and woodhouse ( 1951 )  . it is now found that this treatment does not appreciably alter the ultimate tumour yield , because the apparent increase in the period immediately following the operation is offset by the regression of several of it was suggested that the previous result might be these " explosive " tumours . accounted for if the operative treatment accelerated the establishment of optimal it remains not impossible that this conditions for the evocation of tumours is so , and that subsequent regression of some of these tumours was dependent on the ischa3mic conditions in the dermis and subcutis developing further to a point at which the vascular conditions were inadequate to maintain the tumour . in experiments of the type recorded here , it is necessary to consider the effects experiments such as those of of mechanical trauma on the yield of tumours . lipschuiitz ( 1924 ) , mandl and stohr ( 1924 ) , doderlein ( 1926 ) and deelman ( 1927 ) indicated that trauma of a previously tarred area tended to provoke tumours closely related to the sites of the healed wounds . 
more recently pullinger ( 1943 ) obtained results similar to those of deelman using a pure chemical carcinogen . mackenzie and rous ( 1941 ) and friedewald and rous ( 1944 ) obtained a high incidence of tumours around healing wounds produced by punching holes in the it was on the basis of this work that ears of rabbits after carcinogen treatment . the conception of initiating and promoting factors , later adopted by berenblum and shubik ( 1947 ) was based . in almost all such work , attention has been almost exclusively directed to the epithelial cells , but linell ( 1947 ) showed that there was a difference between superficial and deep trauma . 
numerous tumours , including carcinomata , appeared on the original treated donor site . re - implantation of pinch grafts and thin thiersch grafts into the site from which they were cut in the carcinogen - treated skin did not result in an increased incidence of persistent tumours . there was an increase in regressing tumours . trauma to the treated dermis ( by temporary insertion of threads or by electrically heated wires ) did not increase the incidence of tumours . the present results , like those previously reported , suggest strongly that both the epidermis and dermis ( and possibly deeper structures ) are involved in the carcinogenic action of methylcholanthrene . in particular , they are difficult to reconcile with the two - stage epithelial hypothesis of berenblum and shubik ( 1947 )  . we are indebted to r . 
the column was developed with several litres of light petroleum , followed by mixtures of this with progressively increasing amounts of benzene , and the eluates were collected in separate lots of about 2 l each . these were examined spectrographically , and those possessing similar fluorescent spectra were combined , evaporated to a small bulk , and dissolved in small amounts of benzene , providing the following fractions for testing : pes - a : fractions before the appearance of anthracene bands ; pes - b : those with anthracene bands predominating ; pes - c : those after anthracene , but before benzypyrene ; pes - d : all fractions containing benzypyrene bands ; pes - e : subsequent fractions , with recognizable fluorescence bands at 412 and 430m , u . ; pes - f : later fractions with main fluorescence band at 391 m ,  . ; pes - g : still later fractions with fluorescence band at 385 m ,  . in rabbits , skin tumours were obtained with fractions pes - c , pes - d , pes - e , pes - f , and somewhat more slowly with pes - g , while in mice skin tumours appeared only with fractions pes - d and pes - e . two interesting points arise from these results : the first is the confirmation of the previous experiments , mentioned above , that fractions appearing before and after the benzpyrene - containing fraction , are highly carcinogenic . 
the second is that the one appearing before benzpyrene , is far more potent for the rabbit 's than for the mouse 's skin . in a second fractionation , starting with larger quantities of tar ( 4 l ) , the same procedure was adopted , except that the original petroleum extract was shaken 160 i . 
was somewhat more active , while the highest activity was obtained with the next fraction , coming over at 170 - 180 c . the combined fraction of 160 - 180 c . 
was then chromatographed from light petroleum , and collected into four fractions : ( a ) a very early fraction , containing naphthalene and most of the anthracene . ( b ) an intermediate fraction , containing in addition to the remainder of the anthracene , fluoranthene , a large amount of chrysene , and probably chrysene homologues ( see below )  . ( c ) a large third fraction , containing all the benzyprene , also some chrysene , ( d ) a late fraction , in which 1 : 2 - benzcarbazole was recognized . these four fractions were tested on rabbit skin ; fractions ( b ) and ( c ) ( referred to as pf and ph in table i ) was found to be highly carcinogenic , while ( d ) ( fraction pi ) was less so . these fractions , on concentration , deposited crystalline material , which was collected and recrystallized several times from different solvents . one of the components proved to be chrysene , crystallizing in the first crop . 
they are neither acids nor bases , since preliminary treatment with alkali and acid , respectively , does not remove theby fractional distillation , these carcinogens appear slightly earlier than 3 : 4 - benzpyrene . 
one of these , which appeared just before benzpyrene on the chromatography column , possessed the unusual property of high carcinogenic potency for rabbit skin and none for mouse skin . the final active material obtained by the above methods of fractionation , represented more than a two hundred - fold concentration of the original tar . still consisted , however , of a mixture of substances , and the active constituent has not yet been identified . we are indebted to the city of leeds gas department for a generous supply of horizontal retort tar . 
almost all cases of leukaemia in 2955 days . the aka line are lymphogenous or of a very ' immature type - the so - called stem - cell leukaemia . the low leukaemia line which we have used for the cross - breediilg is called b . this line is also inbred . 
among hundreds of b mice we have previously observed , only one case of lymphogenous leukaemia was found . in the fl there was found 43 per cent of deaths due to leukaemia ; the age distribution of these mice dying from leukaemia is shown in fig . 
the age distribution is somewhat wider than in aka mice and the peak is displaced about 300 days later , so that in th ' is case the average lifetime for mice dying from leukaemia is 59119 - 6 days . in the f2 we encountered 37 per cent cases of leukaemia , and the distribution of age appears to be very wide , as shown by fig . 
the curve may be regarded as a combination of two distributions , one corresponding to the aka mice and one corresponding to the fl . the backcross derived from the fl crossed with aka shows a rise in the frequency of leukaemia to 49 per cent , and the curve concerning the distribut ' ion of age shows , as is seen from fig . 
l. - the age distribution of mice dying from leukaemia within the aka line - - - - - and the a ' ckli ii i t 60days ] days age lunit = 60daysj fig . 
the curve for the f2 shows a tendency to a bimodal form . you will see that , in spite of the genotypical uniformity of the mice of the aka line and the fl , leukaemia only develops.in respectively 63 per cent and 43 per cent of the animals . 
the percentages mentioned as is the case with the figures from previous experiments - calculated by comparing the number of mice dying from leukaemia with the total number of day , ; fig . 
4. - age distribution of leukaemia in backeross of fl mice to b line . dead mice , the animals dying before the first case of leukaemia occurs not being included . it is quite evident that this mode of calculation is entirely inadequate , because deaths caused by other reasons than leukaemia ( such as intercurrent diseases ) , will influence the result to a very high degree . 
the frequency in the fl is not so great as in the aka line , but this can be in part due to the fact that the cases appear at an average age of 300 days later , so that the deaths from other causes will decrease the frequency of leukaemia . the figures found in ' this material , as seen from the following considerations , support the view that the inheritance may depend on one single dominant gene . if we suppose that this is the case , we can calculate the expected numbers of leukaemic animals in the f2 and backcrosses to the parent lines on the basis of the observations in the aka and the fl mice . these results are calculated in table 1 , taking into account the deaths from other causes . these figures agree very well with the observations , but in the calculated mortality curves the agreement was not so evident . 
the difference is not significant . if we assume the presence of two genes the calculated number will only be 8 - 2 '  . these data thus support the hypothesis of a single domi ' nant gene . the variation in the average lifetime of the leukaemic animals has previously been described by macdowell , potter and tayl ' or ( 1945 ) , macdowell and richter ( 1935 ) , furth and barnes ( 1941 ) , kirschbaum ( 1944 ) , and cole and furth ( 1941 ) in similar crossbreeding experiments . 
the phenomenon seems therefore to be independent of the character of the lines used , which fact seems to refute the previous supposition that casual changes in the average lifetime of all the mice may influence the result . i would sooner say that the discovery confirms the supposition that the immature leukaemic cells arise by a somatic mutation in cells which possess a labile 112 g . 
where and how this mutation arises could be a if the animals are homozygous with regard to the labile gene , matter of chance . the mutation will naturally arise earlierand more frequently than ' is the case if the animals are only heterozygous . 
we spent more than eight months working on one such incidental problem , which had to be solved before we could proceed with the main work . this effort was well rewarded , however . 
we not only improved our experimental approach , but also acquired information that will further our understanding of the intricate role played by biological factors in regulating the influence of external agencies on living cells . in view of all this , i should like to point out that our investigations of the genetic potencies of carcinogens are still in an early stage . 
koller these few instances are selected from many clinical and pathological findings to illustrate that the environment of tumours is of great importance , and must be taken into consideration when devising improvements in radiotherapeutic procedures . it may prove to be important not only in surgical and radiotherapeutic practice , but also as regards theoretical problems of oncology . 
the classical study of willis ( 1948 ) emphasizes the fact that potentially neoplastic tissue zone is much greater than the size of the initially appearing tumour would indicate , and brings forward evidence which lends support to the field - theory of the origin of cancer . 
thus the possibility that the " recurrence " of a tumour after surgical treatment may represent an entirely new cancerous change in a predisposed tissue , and is not due to the incomplete removal of the malignant growth , has to be considered . the aim of post - operative x - ray therapy is not only to destroy viable tumour cells which might have been left in situ , but also to reduce the chance of the occurrence of an entirely new malignant growth by producing gross alterations in the histological architecture of particular regions , showing a proneness to neoplasia , and to affect the substrate in which any malignant cell left in situ might progress and defeat the treatment . 
the importance of connective tissue and tumour - environment has also been stressed by vernoni ( 1948 ) , whose views on the connective - tissue role in carcinogenesis find support in recent research work . a better understanding of the behaviour of the connective tissue of the tumour - bed and stroma during and after radiation treatment leads to the revision of fundamental principles on which the rationale of treatment is based . 
the practical application of the latter in the radiotherapy of accessible tumours finds expression in a new technique , described as the " sieve or alternating chess - board method " ( jolles , 1949a )  . for the past two years this method has been tested on a small number of patients , yet the radiation response in these cases has shown characteristics which hitherto have not been seen in tumours irradiated by the usual conventional methods . 
the purpose of the present paper is to describe these phenomena , and to discuss their bearings on the destruction of malignant growth . the biological basis of radiation effects in tumours . the radiation - induced changes in the cellular and stromal part of the tumour may be summarized briefly as follows : the cellular injuries consist of diverse nuclear or chromosome injuries , as well as disturbances in cytoplasmic enzyme activity . 
the chromosome injuries manifest themselves during mitosis which follows treatment , and lead to cell death by the breakdown of the mitotic mechanisthe amount of chromosome injury and the number of injured radiation - induced enzyme disturcells show a direct dependence on the dose . bances , the extent of which also depends on the dose , either lead to reversible injuries , e.g. 
the recent investigations by bloom and jacobson ( 1948 ) , anderson ( 1949 ) , and warren and dixon ( 1949 ) , brought forward further evidence to show that radiation does not produce cell differentiation . in the stroma and tumour - bed two chief events can be distinguished : hypertrophy of the connective - tissue elements , and a reaction closely resembling inflammation . 
the first phenomenon mainly consists in an excessive deposition of intercellular collagen fibres ( fibrosis ) ; the second is represented by an invasion of lymphocytes , polymorphonuclear leucocytes and macrophages into the fine these changes network of connective tissue forming the stroma and tumour - bed . in the normal tissues naturally react on tumour cells and tissue ; the effects in the latter thus produced can be referred to , therefore , as " indirect radiation effects . " they must , however , be clearly distinguished from those " indirect " effects which are assumed to be brought about by injury to the blood supply ( desjardins , 1932 ; harvey , 1942 )  . failla , 1940 ; ellis , 1942 ; windeyer , 1942 ; the importance of the tumour - bed during treatment has been recognized by a great number of investigators ( russ , chambers and scott , 1921 ; kok and vorlaender , 1922 ; caspari , 1922 ; murphy , maisin and sturm , 1923 ; czepa , 1924 ; roussy , 1926 ; ewing , 1926 ; souttar , 1929 ; sugiura and cohen , 1939 ; jolles , 1946 , friedman , 1939 ; evidence was also obtained in various 1948 ; spear , 1946 ; windholz , 1947 )  . experiments which shows the influence of the tumour bed in the radiation response of tumours ( lasnitzki , 1947 ; elson and lamerton , 1949 ) , and it was found that by taking into consideration the " stroma - reaction " , treatment methods could be devised for individual tumours in which the total dose given did not exceed 2700 r ( koller and smithers , 1946 )  . 
in the interdependent tissue structures of tumour and tumour - bed , the different reactions ( cellular and intercellular , direct and indirect ) are knitted together and closely integrated . it was observed that the onset , degree and rate of these reactions vary greatly in different tumours . because the outcome of treatment depends on them , the total dose necessary for the destruction of tumours also varies within very wide limits ( 2700 r and this observation leads to the conclusion that on biological grounds the 9000 r )  . concept of a " standard tumour - lethal dose " is untenable . it is unnecessary , however , to stress that a minimal effective dose which is indispensable for the destruction of a tumour remains of paramount importance , and the enhancement of the effect of this minimal dose , by utilization of the indirect radiation effects , is here discussed . the various reactions induced by the radiation all contribute to the resolution and eventual disappearance of the tumour , therefore the reaction - system must be it is only by the analysis of all these factors and the study considered as a whole . of the behaviour of all tissue structures , that an explanation may be found either for the inadequate response , or for the recurrence of a particular tumour . 
the technique has been fully described in a previous communication ( jolles , 1949b )  . apart from the direct radiation transmitted through the " opaque " lead squares ( and which does not exceed 3 per cent with the thickness of lead used ) , the protected areas also receive a very small amount of scatter irradiation . latter is irregularly distributed , tailing off towards the centre of the protected this contingency must be taken into consideration when studying and areas . conmparing the radiation effects of the directly exposed and protected parts . biopsy specimens are taken simultaneously from the exposed and protected areas , preferably fronm the centre of these regions , and occasionally a third biopsy specimen is obtained by cutting across both the exposed and protected areas in order to follow the transitional stages of the histological changes due to radiation . the great variability of tumours in respect of the histological organization including the structure of stronia and tumour - bed , has to be kept in mind , and our observations were based only on biopsy material showing similarity in these respects . eighteen patients have been treated with the sieve technique , and the radiation reactions in the exposed and protected areas have been compared by the analysis of biopsy specimens . 
two sets of experiments were devised ; in the first instance only one sieve was used throughout the treatment . in the second set , two sieves a and b , were employed ; chess - board b differs from chess - board a in that the order of transparent and opaque squares is reversed . 
xi.48 : 4 days after start of treatment 28.xi.48 : 13 days after start of treatment 8.xii.48 : 23 days after start of treatment 16.xii.48 : 31 days after start of treatment 15 . 
the gland increased in size very slightly during treatment to the lesion on the temple . one month later the gland had grown to the size of a hazel - nut . 
lederman , the behaviour of over 450 accessible tumours has been analysed during and after treatment , and it was established that besides the injuries in dividing cells and the great increase in cytoplasmic volume of differentiating or maturing tumour cells , the most striking change occurs in the connective tissue of the stroma and tumour - bed , which may be described as tissue " fibrosis . " the connective tissue becomes more rigid in architecture , less flexible and adaptable for the development of the inflammatory reaction ( " coarse " tissue fibrosis )  . 
koller to state what is the primary cause of tissue changes in the protected areas ; i may be that the small amount of scatter radiation received in ten fractions o for that reasoi 40 r daily can produce such alterations in the connective tissue . further experiments are in progress to study the stromal effect of such a smal the experimental evidence so far available indicates that tissue reactioi dose . after a dose of this order is negligible ; if there is any , e.g. 
we are of the opinioi that the tissue changes in the protected regions are brought about by a complet mechanism in which , among others , a diffusible substance produced in the directli irradiated tissues might play a role . 
the absence of chromosome fragmentation is another proof that the alteration seen in the protected areas , such as the increase in the size of tumour cells , and the slight degree of fibrosis and inflammatory reaction , must be considered as an indirect reaction to radiation . our investigation has shown that the rate and degree of the indirect radiation reaction depends on the histological organization of stroma , and on the dose . on account of the differences in the histological architecture of tumours , the minimum effective dose varies from tumour to tumour . 
we found that in tumours in which the connective tissue is abundant the minimum effective dose is smaller than in tumours with scanty stroma . this is illustrated in case ii , in which the dosage used ( 2700 r actual dose in 35 days ) did not reach the critical minimum level necessary to produce a reaction of sufficient strength and efficiency in the scanty connective tissue of the " protected " tumour areas . 
on the other hand , the use of the sieve - technique has permitted the subsequent treatment of the residual tumour with a relatively high but adequate dose ( 4500 r actual dose in 18 days ) , because the histological texture of the skin , owing to the small size of the areas directly exposed to irradiation during the initial treatment has been left unimpaired , and could safely be subjected to such a high dose in the second treatment . the complexity of the various cellular and tissue interactions increases when further radiation is carried out through another " chess - board or sieve " in which the position of transparent and opaque areas is reversed . 
we found that while the connective tissue needs protection from excessive radiation , it requires a certain quantity of radiation and a specific distribution in time and space of this quantity in order to elaborate the radiationinduced reaction . 
the stroma and tumour - bed reactions , however , being too obvious to disregard completely , are referred to , but only as concomitant , " independent " events , which have no , or too little , bearing on the radiation response of the malignant growth itself . 
the most cursory histological study of tumours under radiation reveals the fact that the destruction of all malignant cells of the tumour parenchyma rarely , if ever , can it seems , therefore , be achieved by the " direct " action of a therapeutic dose . necessary and logical not only to admit the existence of an " indirect " effect , but to accept all the implications of the generic statement that the purpose of radiation is to kill a variable but significant proportion of active tumour cells , and at the same time to assist the local body defence system by inducing the various responses in the tumour - bed and stroma . it also follows that any view based on changes induced by radiation in some and not all tumour - tissue components is not comprehensive , and that the conclusions drawn from the study of cell behaviour alone are doubtful . 
on " cell count method " of glucksmann and co - workers that account the ( gluicksmann , 1941 , 1948 ; glucksmann and spear , 1945 ; gkicksmann and way , 1948 ) , which per se represents a contribution to radiobiological knowledge , is liable to be misleading when claims are being attached to it , such as that it provides an explanation for the variation of radiation response of tumours , predicts the outcome of treatment , and indicates the most appropriate treatment method , whether surgical or radiological , for a given case . the cell count method is biased by subjective selection and interpretation ; it disregards the great regional heterogeneity shown by tumours both in growth rate and histological organization , and the fact that a malignant growth is composed of tumour and stroma , which form one closely integrated unit . it is more than obvious that for that reason the application of the cell - count method to biopsy specimens taken after a " test dose " of radiation in order to decide whether a tumour be submitted for surgery or radiotherapy is of doubtful value ( glucksmann and way , 1948 )  . it has been stated by spear ( 1946 ) that " radiation affects any given cell of a complex tissue in at least two ways , first by direct action on the cell , and secondly by injuring neighbouring tissues , upon the healthy functioning of which the cell depends . " our investigation leads us to a similar conclusion that the direct cellular effects , e.g. 
fragmentation of chromosomes , represent only the initial phase , and that the most important factors responsible for the disorganization , regression and re - absorption of tumours during and after irradiation are the various , closely integrated and related reactions which are produced by the radiation in the connective tissue of tumour - bed and tumour stroma . the present investigation , in which the alternating chess - board method was employed , has shown the role of the connective - tissue reaction in the destruction of tumours and the way by which this reaction can be favourably influenced and modified . 
we have found that the fractionation of dose in time as well as in space , as carried out by the sieve , induces specific changes in cells and tissues . the intensity and rate of these changes affects the whole architecture of stroma and tumour - bed as well as that of the tumour . our investigation has also shown that when the sieve is used sufficient response can be produced in the local defence system of connective tissue , and can be maintained by a much smaller dose than usually employed . 
roller us in cases where the tumour is radio - resistant , either by its nature or by its environment , to deliver a higher total tumour - dose without the danger of destroyit is our intention to investigate the ing vital structures of the tumour - bed . potentialities of this new procedure by applying the sieve method for the treatment of radio - resistant and deep - seated tumours , especially metastatic deposits in lymph nodes . 
the tumour is divided into a number of " exposed " and " protected " areas , the former receiving direct , the latter receiving only a small amount of scatter and transmitted radiation . 
two chess - boards or sieves , which differ in the order of the transparent ( exposed ) and opaque ( protected ) squares , can be used during treatment . irradiation induces injuries in the tumour cells and alterations in the connective tissue of the tumour - bed and stroma . 
the radiation reaction in the connective tissue plays a very important role in the destruction and reabsorption of tumours . in tumours irradiated through the sieve it was observed that tissue - reaction is reduced in the directly " exposed " regions , but at the same time , fibrosis and inflammatory reactions are induced in the " protected " regions . 
no cellular injuries , due to direct radiation such as chromosome fragmentation , were seen in cells of the " protected " areas . by using two sieves which differ in the order of the " transparent " and " opaque " areas , the reaction of the tumour - bed and stroma in the presence of abundant connective tissue becomes uniform throughout the tumour , irrespective of the different doses which regions may have received during treatment . analysis of the radiation reaction in tumours treated by the sieve has shown that fractionation of dose in time as well as in space induces injuries and specific alterations in the irradiated area , the rate and type of which greatly enhances tumour destruction . the authors are indebted to the british empire cancer campaign for a grant for technical assistance , and thanks are also due to f . 
kirby. from the research department , glasgow royal cancer hospital . received for publication february 8 , 1947 . the exceptional interest of 2 - acetylaminofluorene ( aaf ) as a carcinogen was clearly revealed by wilson , deeds and cox ( 1941 ) , who fed it to inbred albino rats in which only benign mammary tumours had been observed , and found carcinomas of the liver , breast , bladder , ureter , renal pelvis , colon , pancreas , lung and skin , a myogenic sarcoma , and in two cases liver lesions resembling leukaemic infiltration . 
the results of bielschowsky ( 1944 a and b ) and other workers are summarized later in this paper . in cba mice , neoplasms of liver and uterus ( one a sarcoma ) and of the urinary bladder were found by armstrong and bonser ( 1944 )  . bielschowsky and green ( 1945 ) reported a carcinoma of the kidney in a rhode island red cock which had been fed aaf for 45 weeks . the widespread variety of organs affected by aaf led bielschowsky ( 1944b ) to try to induce tumours of the goitrous thyroid gland with this substance . solid , parenchymatous goitre was induced by allyl thiourea ; in conjunction with aaf , also orally administered , allyl - thiourea induced adenoma in 9 out of 10 rats , while malignancy was observed in 3 of these rats . griesbach , kennedy and purves ( 1945 ) claim that the goitrogenic agent in brassica seeds can cause adenoma of the thyroid if given orally for long enough , but only 1 of 8 wistar rats developed such a lesion . subsequently purves and griesbach ( 1946 ) obtained malignant changes in 2 out of 30 wistar rats given thiourea in their drinking water for nearly two years . purves and his co - workers consider that the effect of the goitrogens is indirect , operating by inducing hypersecretion of the thyrotropic pituitary hormone . 
aaf has no specific action even on adenomatous thyroid tissue . the success achieved by bielschowsky in at least accelerating malignant changes .in the thyroid of rats by feeding aaf suggested that other organs apparently untouched by aaf alone might undergo neoplastic changes when stimulated to proliferate by suitable means . 
the sex - organs of the rat can be caused to hypertrophy by the administration of the appropriate sex - hormone , and it was thought that these organs , thus caused to proliferate , might proceed to malignant changes when influenced by orally administered aaf . 
the basal diet for all groups was rat - cake made to the formula of thomson ( 1936 )  . 2 - aminofluorene was synthesized from fluorene by the method of diels ( 1901 ) , * and acetylated as follows . 
up to 1 per cent of concentrated sulphuric acid was added to 2 - aminofiuorene stirring in an excess of acetic anhydride which became very hot and dissolved the amine . after chilling thoroughly the acetylated amine was filtered on a sintered - glass sufficient water was added to cause funnel , and dissolved in hot ethanol . permanent turbidity and the solution well cooled . 
emmens pointed out that absorption during the second month would be much reduced , and recommended the use of 20 mg . therefore thin disc - shaped pellets weighing 20 mg . 
a spindle - cell sarcoma of the left seminal vesicle was found in rat 354 ( group iib ) , and a whorled , spindle - cell sarcoma was found lying above the liver of rat 339 ( group iia )  . 
the reason for this may well be that suggested by these workers , namely that " the hyperplasia of target organs of sex - hormones is a functioning hyperplasia , whereas that induced in the thyroid by goitrogenic agents is non - functionthus the type of hyperplasia induced by bielschowsky in the rat thyroid ing . " in which growth is accompanied by loss of differentiation would appear to have been a suitable basis for carcinogenesis , whereas the hyperplasia associated with increased differentiation induced in sex organs by over - stimulation with sexhormones is apparently unsuitable . 
illustrate a " carcinoma arising adjacent to the external auditory canal , " and discuss the histogenesis of this and other tumours in this locality included by them under " subcutaneous tumours . " bielschowsky first drew attention to tumours of the ductus acusticus externus as a separate entity . 
as wistar rats were also used by bielschowsky , who found these tumours in 18 / 93 rats given aaf orally up to 210 days , the influence of diet seems to have some importance . 
when allyl - thiourea was also given , the incidence of tumours rose to 6 / 10 . lopez ( 1945 ) also found external meatus tumours in 2 / 4 rats . 
hence the action of aaf on proliferating mammary tissue was only slight in our experiments . in the matter of liver tumours , our series has yielded results in full accordance in our series , a . 
the types of liver tumours seem to be essentially the same as in wistar rats . this is also true of the liver tumours obtained by bielschowsky in piebald rats , in which the sex - ratio is also maintained and the in the sherman strain , cantarow et al . 
found the incidence much the same . incidence of liver tumours in female rats raised when oestradiol dipropionate was injected intramuscularly ; but the complete absence of liver neoplasms in rats given thiouracil was much more striking . 
the latter group ate less of the aaf diet than did controls receiving no thiouracil , but more than the oestrogenized rats . the incidence of mammary tumours in piebald rats was very low compared with that in wistar rats on the same diet ( bielschowsky , 1946 )  . but the incidence of tumours of the ductus acousticus externus was much higher in the piebald rats , in which tumours of the small intestine were also much more frequent . moreover , lung tumours were found in this strain , but have not been reported in wistar rats given aaf and were not found in our series , although one control female ( group ia ) was found to have undifferentiated bronchial carcinoma . the albino rats of wilson et al . 
the latter have not been found in any other strain of rat , and tumours of the kidney and bladder only once each . it would seem that , if sufficient strains of rat were employed , possibly no site in the body would be found immune from the carcinogenic action of aaf . 
in the strains so far tested , only mammary tissue among the sex - organs seems to be susceptible , and this tissue is liable to develop carcinoma due to the action of sarcomas are rare , and are not induced by subcutaneous oestrogens alone . injection of aaf , at least in wistar rats . in our series , a whorled , spindle - cell sarcoma was found in the omentum covering the left lateral lobe of the liver in one rat , and a spindle - cell sarcoma was present in the left seminal vesicle of another . it remains to discuss a few other points of interest . toxic damage to kidneys was seen in some animals of all groups ; rats receiving oestradiol benzoate pellets , with or without aaf , tended to show degeneration of the epithelium of the first and second convoluted tubules with the presence of a dark yellow a . 
kirby pigment in these cells . there was no consistent evidence of toxic damage to the kidneys by aaf or its metabolites , nor were any tumours of this organ seen . no tumours of the uterus were found , but all females receiving oestradiol benzoate had pyometra , which often made it necessary to kill the animal ; the 2 females receiving the male sex - hormone had no pyometra . the spleens of the control groups , ia and ib , showed no abnormality . 1 female in group iia and 1 male and 2 females in group iib had enlarged spleens , due to lymphoid hyperplasia . there was no question , however , of the regular , early , gross enlargement of the spleen seen in rats ingesting azo - compounds it may be ( smith , lillie and stohlman , 1943 ; kirby and peacock , in press )  . concluded that no splenotoxic substance passes from the liver into the blood of rats fed aaf ; rats fed p - aminoazobenzene ( aab ) or its n - monomethylor n , n - dimethyl - derivatives ( mab and dab ) have aab circulating in the blood and affecting the spleen ( miller , miller and baumann , 1945 )  . the rats given aaf orally in the experiments described in this paper developed tumours of the liver predominantly in the right lobes ; tumours in the left side of the liver were usually smaller or absent . 
a similar predominance of tumours in the right side of the rat liver has been reported by opie ( 1944 ) in rats fed dab in diets not inducing cirrhosis . 
dmochowski. from the department of experimental pathology and cancer research , medical school , university of leeds . received for publication december 15 , 1952 . the test mice most commonly used for ascertaining the presence of the mammary tumour agent are susceptible hybrid female mice obtained by mating low - breast - cancer - strain females to high - breast - cancer - strain males . in these test mice a low incidence of spontaneous mammary tumours was frequently recorded ( bittner , 1939b ; murray and little , 1939 ; andervont , 1940 ; gardner , 1941 ; dmochowski , 1944a ) , and was frequently found to be higher than that of their maternal parents ( andervont , 1945a )  . 
of even greater interest was the high tumour incidence reported in the progeny of susceptible low - cancer - strain females mated to high - cancer - strain males which had been subjected to forced breeding - that is , bearing a number of litters in quick succession ( andervont , 1945b )  . 
a similar high incidence of breast cancer was also observed in forciblybred hybrid progeny of low - cancer - strain females of low susceptibility to breast tumours mated to high - cancer - strain males ( bagg and jacksen , 1937 ; strong , 1943 )  . attempts to discover the mammary tumour agent in mammary tumours of some of these hybrids proved unsuccessful ( andervont , 1945b )  . 
a subline of c57 black strain is now established in which this subline a number of mammary tumours has been recorded by the author . comes from one of the original threelitters brought from the laboratories of the the progeny of these litters has been kept imperial cancer research fund . separately , and no breast tumours have so far been recorded in the descendants the description of the subline in which tumours have of the other two litters . the riii strain mice appeared will be the subject of a separate communication . were also obtained from the same source and maintained since 1946 . the tumour incidence of 83 per cent at an average age of 8x5 months in breeding females ( dmochowski and gye , 1943 ) has with small variations remained approximately it was known that mice of high - cancer strains derived from the fourth the same . or later litters develop a higher incidence of breast cancer than those from the first two litters ( bittner , 1942 ) , and that the appearance of an active agent in mice deprived of it by foster nursing had been recorded in the progeny obtained from hybrid progeny of the c57 black strain the third or later litters ( bittner , 1943 )  . females was therefore taken only from the fourth or laterlitters for the experiment , mice from earlierlitters being used for various other purposes . 
the ( c57 x riii ) fl hybrid females which were litter mates were divided into two groups . only two hybrid females were taken from each of the c57 females mated to riii strain males , if possible from the same or foliowing litters . whenever two females were not available from the same litter , the mice from later litters were included in this way two groups , each comprising thirty ( c57 x in the control group . riii ) f1 hybrid females , were obtained . mice of the control group were allowed to breed in a normal way and mice of the experimental group were forcibly bred by removing their litters as soon as they were born . mice of one of the later litters from fifteen hybrid females in this group and of one litter of a female from the these mice in turn , control group were saved for brother to sister matings . after saving one litter , were forcibly bred and this procedure was followed for several generations . 
the progeny of six ( c57 x riii ) f1 hybrid females , which had been subjected to forced breeding , was maintained for six generations and the progeny of nine additional ( c57 x riii ) f1 hybrids , treated in a similar manner , for only three generations . 
dmochowski tumour which on histological examination was found to be a lymphosarcoma . the average number of litters bom to these hybrid females was three , and varied from two to seven . 
the number of breast tumours which developed in their litter mate ( c57 x riii ) f1 hybrid females , which had been forcibly bred , is shown in table ii . 
among these hybrids , the tumorous females had an average of 6 * 5 litters and the tumour - free females 6 - 4 litters . there was no difference therefore in the number of litters born to these two types of females which had been forcibly bred . none of the c57 black strain mothers , mated to riii strain males and bred in a normal way , developed mammary cancer , although they lived to an average twelve c57 black strain females , which were litter - mates age of 19 mouths . of some of the c57 females mated to riii strain males , were forcibly bred with their own litter - mate males , and none developed breast cancer , although they had an average of 5 * 2 litters and lived to an average age of 18 months . 
the observation that none of the c57 strain females developed mammary tumours after mating to c57 strain males and forced breeding points against the possibility of c57 black strain females harbouring a weak or attenuated mammary tumour it is now well known that various sublines of c57 black strain differ agent . considerably in their susceptibility to the agent . c57 strain mice of the subline of the present experiments , when foster nursed by riii strain females , developed an incidence of mammary cancer of only 11 per cent ( dmochowski , 1948 )  . this low susceptibility was probably responsible for the failure to induce mammary cancer in mature c57 mice of this subline even by a combined action of large doses of material containing the agent and forced breeding ( dmochowski , 1948 )  . again this low susceptibility may also have been responsible for c57 mice of this subline remaining tumour - free after mating to riii high - cancer - strain males as well as for their hybrid progeny , bred in a normal way , not developing mammary cancer . 
a further indication against the possibility of c57 black mice of this subline harbouring a weak agent or in small quantities was provided by the absence of the agent in mammary tumours induced in both virgin and breeding c57 females by treatment with methyloholanthrene ( dmochowski and orr , 1949 )  . 
the forcibly - bred progeny of four ( c57 x rhij ) f1 hybrid females which had died free from tumours , also continued in these figures , the number of for six generations , is presented in fig . 
3 to 6 that descendants of tumorous hybrid females . females can remain tumour - free for two , three or four successive generations before developing mammary cancer , and that descendants of a non - tumorous female , in spite of reaching tumour age , may show no mammary tumours for as many as five generations before developing breast cancer , in spite of inbreeding it may be of interest to point out that and intensive hormonal stimulation . andervont ( 1949a , 1949b ) found the agent to be transmitted through three or four successive generations of susceptible mice without inducing mammary further , the study of the distribution of mammary tumours in charts cancer . of the progeny of tumorous and non - tumorous hybrids , shown in fig . 
1 to 6 , indicates the possibility of the agent being involved in the development of these tumours . a comparison of the age of the earliest tumour appearance , tumour incidence , average tumour age and average age at death of the progeny of individual tumorous and four tumour - free ( c57 x rii1 ) f1 hybrid females is shown in table iii . as can be seen , there was little , if any , difference between the forcibly - bred progeny of the two ( c57 x riii ) f1 females which developed breast cancer and the forcibly - bred progeny of the four ( c57 x riii ) f1 hybrid females which died without tumours . table iv demonstrates the tumour incidence and tumour age in the forcibly - bred progeny of additional nine non - tumorous ( c57 x rii1 ) f1 females which was continued for three generations . 
the tumour incidence , although varied in the progeny of the individual hybrids , was lower and the age of breast tumour appearance higher than those in the progeny of the two tumorous and also of the four tumour - free ( c57 x r111 ) f1 hybrid females . 
number preceding letters t , n or l = number of female ; number following letters t , n or l = tumour age or life span in days . of the earliest tumour appearance , the appearance of mammary tumours according to months , the tumour incidence , and the average tumour age in six generations of combined forcibly - bred progeny of the thirteen non - tumorous ( c57 x riii ) f1 hybrid females . 
dmochowski generation of the progeny of this non - cancerous hybrid female may be seen in this figure as well as the consecutive number of litter to which the mice belonged which developed tumours . it would have been of interest to obtain the first litter of this female and its progeny and compare any mammary tumour incidence in this progeny with that of the progeny obtained from the sixth litter , but this could not be done owing to limitation of space . table vii shows the age of earliest tumour appearance , the tumour incidence , and the average tumour age in the normally - bred progeny of this non - tumorous ( c57 x riii ) f1 hybrid female . 
the breast tumour incidence in the forcibly - bred progeny of the non - cancerous ( c57 x riii ) f1 hybrid females was lower and the average tumour age considerably higher than those in the forcibly - bred progeny of cancerous ( c57 x riii ) f1 hybrid females , but this difference in tumour incidence and average tumour age gradually became smaller in successive generations of the progeny . 
the age of the earliest tumour appearance and the average tumour age in the progeny bred in a normal way of one cancer - free ( c57 x riii ) f1 hybrid female was distinctly higher than those in the forcibly - bred progeny of both tumorous and tumour - free ( c57 x riii ) f1 hybrids . 
the tumour incidence in the normally - bred progeny was , with one exception , lower than that in the forcibly - bred progeny of tumorous hybrid females and , again with one exception , approximated to that in the forcibly - bred progeny of non - tumorous hybrid females . it should be pointed out that the results of the comparison of the behaviour of normally - bred progeny of one non - tumorous female with that of the forcibly - bred progeny of thirteen non - tumorous hybrid females may not be the same as those which would have been obtained should this comparison have been extended to similarly maintained progeny of a number of other cancer - free hybrids which had been bred in a normal way . this point may be seen from the observations on the forcibly - bred progeny of four nontumorous ( c57 x rii1 ) f1 hybrids compared with those on similarly treated progeny of two tumorous ( c57 x riii ) f1 hybrid females . 
the difference in mammary tumour incidence and average tumour age between these two groups of hybrid females became pronounced only after including the observations on the progeny of nine additional non - tumorous ( c57 x riii ) f1 hybrid females . is therefore possible that the results of the comparison of normally with forciblybred progeny of non - cancerous hybrids would have been different as in the case of the comparison of forcibly - bred progeny of non - tumorous with that of tumorous it is not known whether the results of foulds ' ( 1949 ) comparison of hybrids . forcibly - bred progeny from tumorous and non - tumorous hybrid females would l . 
dmochowski not have been different had the progeny of a greater number of non - tumorous hybrid females been included in his study . from the study of the distribution of cancerous females in the forcibly - bred progeny of tumorous and tumour - free ( c57 x riii ) f1 hybrid females and in the normally - bred progeny of a cancer - free hybrid , shown in fig . 
among the forcibly - bred progeny of the four tumour - free ( c57 x riii ) f1 hybrids , tumorous mice had an average of 7 3 ( 1 to 13 ) and the mice without tumours an average of 8 - 3 ( 1 to 16 ) litters . 
the behaviour of mice in the progeny obtained after the tumour appeared in their mother may greatly vary even in the case of hybrid females of the same origin , probably as a result of variations in the genetic make - up of individual females infiuencing the presence or transmission of the agent . in conolusion it may be stated that both the genetic constitution and hormonal stimulation play an important part in the development of mammary cancer in the hybrid mice which were the subject of the present study , and that the mammary tumour agent also appears to take a part in the origin of these tumours . biological tests for the presence of the mammary tumour agent . as soon as the first mammary tumours appeared in the hybrid mice , biological altogether twenty - three tests for the presence of the agent were carried out . of the mammary tumours were tested and the results are shown in table xiii . four mammary tumours which developed in ( c57 x riii ) f1 hybrid females , two showed the presence of the agent and two others failed to reveal the agent under the conditions of the test . 
at first it appears surprising that the tumour which developed at the age of 10 months failed to show the agent , as the time of storage in desiccated state was equal to that of another breast tumour which appeared in the same generation and which , although injected in smaller quantity , induced tumours in the test mice but in distinctly smaller incidence compared with that induced by other dried agent - harbouring tissues in previous it must be stressed experiments ( dmochowski , 1945a , 1945b , 1946 , 1948 , 1949c )  . that the method of desiccation of these two as well as of all the other tumours was the same , and the age of the test mice used was in all cases approximately the same . the only varying factors were the amount of tissue injected and the time of storage . 
the longest period of storage in the ice - chest was that of a negative tumour in a ( c57 x riii ) f , hybrid female and amounted to 8 months . this should not have made an appreciable difference in the test , as it was previously shown that agent - harbouring tissue induced breast canoer in test mice after two years of storage ( dmochowski , 1946 )  . 
from the results of the tests of the four tumours in the first generation of hybrid females it may be concluded that two of them possessed the agent , and the two other negative tumours either did not contain the agent or harboured only small quantities or a weak agent which could not be shown under the conditions of the test . 
2 , from the study of parent - offspring correlation there was a definite tendency towards breast cancer development in daughters of tumorous as well as non - tumorous mothers . 
9 female had ten litters and her sister had seven litters . it may well be that the considerable hormonal stimulation was responsible for the appearance of breast cancer in these females , and more likely that the agent took part in the development of these tumours but in quantities too small to be detected by the ( c57 x riii ) f3 no . 
it may well be that had the test a : nimals , in which the latter tumour was tested , lived longer , the agent would probably have been detected . in the fourth generation of the progeny of no . 
20 ( c57 x riii ) f3 hybrid , were found to harbour the agent . the first tumour developed at the age of 8 months after the female had six litters , and the second at approximately 17 months after the female had thirteen litters . it is of interest that both tumours showed the agent , although the second developed comparatively late in life . in the fifth generation of the same line three tumours were tested , those of no . 
69 ( c57 x riii ) f1 tumorous hybrid female in whose tumour the agent was not detected , it may be seen how necessaiy it is to adopt a cautious attitude towards the results of biological tests . it appears probable that the agent may have increased gradually in quantity in successive generations of the descendants of this hybrid female , so that it eventually could be detected by the method applied in the present biological tests . it is possible that the treatment , such as desiccation , may have in part been responsible for the negative results when tumours with small quantities of the agent were tested . had the mammary tumour of no . 
69 ( c57 x riii ) f1 hybrid only been tested and the progeny of this female not raised , the conclusion would have been that increased hormonal stimulation of a susceptible genetic substrate was responsible for the appearance of this breast tumour . it may well be stated that hormonal and genetic factors combined with the mammary tumour agent were responsible for the development of the majority of the tested breast tumours in this line , and probably also a weak or attenuated agent in the tumours negative in the biological test . in the progeny of non - tumorous ( c57 x riii ) f1 no . 
33 female at the age of 17 months after she had eleven litters and one which arose in ( c57 x riii ) f4 no . 39 hybrid at the age of 10 - 5 months after she had given birth to six litters . 
21 , 47 , and 49 ( c57 x riii ) f3 hybrids , all of which developed after the eighth litter at the age of 9 , 12 , and 10 months respectively . all four tumours harboured the agent , yet , although they all arose comparatively early in life , the incidence of tumours induced in the test mice by the tumour of no . 
tumours developed in hybrid mice of all three coat colours without particular connection with any coat colour . foulds ( 1949 ) recorded a similar observation in his c57 x riii hybrids . neither the presence or absence of the agent , as shown in biological tests , was connected with any particular coat colour . foulds ( 1949 ) detected the agent in the tumour of a ( 057 x riii ) f1 hybrid muhlbock ( 1952 ) failed to discover the agent in tumours which had been tested . of five ( c57 x d ) hybrids which developed at ages varying from 20 to 30 months . these hybrids came from early litters . 
mammary tumours in hybrids from later litters of c57 females were not tested , but the presence of the agent in these tumours was assumed by muhlbock ( 1952 ) on the basis of a high tumour incidence in the litters , although the average tumour age was 18 months . 
a search for the agent in mammary tumours of hybrid progeny from another ( c ) low - cancer - strain but susceptible females and high - cancer - strain ( 03h ) males led to the detection of the agent in tumours which developed at an early age up to 12 months , although on two occasions even such tumours were negative ( andervont , 1945b ; andervont and dunn , 1950b ) , while mammary tumours arising at a late age , in spite of their high incidence , failed to reveal the agent ( andervont and dunn , 1949 , 1950b ; andervont , 1950a )  . yet , on one occasion a c strain female was found to harbour the agent , although she developed breast cancer at the age of 21 months ( andervont and dunn , 1950b )  . thus there may be exceptions in both early and late developing tumours , as shown in the present study with dried tumour tissue and in the experiments of andervont and dunn with fresh tumour tissues . biological tests of some tumours appearing at a late age , as shown in the present experiments , revealed the agent , although they failed in other . 
tumours of similar it is not known how far the recent observation of andervont ( 1950b ) late age . that small quantities of the agent may only be ascertained by observing at least one or even two generations of the descendants of the inoculated test mice would be helpful , but it is certainly worth trying in any future tests of mammary tumours appearing at a late age . in some mammary cancers which developed up to the age of 12 months , the agent could not be detected on several occasions in the present study . 
69 f1 hybrid were found to possess andervont ( 1945b , 1950a ) also failed to detect the agent in mice with the agent . tumours at 8 , 12 , 14 , 15 and 16 months . 
on the basis of the study of parentoffspring correlation shown in pedigree charts , it appears probable that the negative tumours also harboured the agent possibly in quantities too small to be detected by the tests applied . in conclusion it may be stated that the results of the biological tests for the presence of the agent in desiccated mammary tumours which developed in the hybrid mice indicate a gradual accumulation of factors responsible for the appearance of mammary cancer . it appears that there may be a certain threshold below which it is difficult or not possible to show the agent in some mammary tumours , at least by the methods so far employed , and only after combined influence of inbreeding and intensive hormonal stimulation the presence of the agent may become detectable . there is no reason to consider the biological tests as inadequate , in view of the previously reported constant positive results with dried agent - containing tissue , and also in view of the negative results occasionally recorded by other workers with fresh material even from tumours which developed early inlife . further , negative tests for the agent in dried tissue of an 86th transplant of a mammary tumour which originally harboured the agent ( dmochowski , 1952 ) have been confirmed with fresh tissue of a 101st serial passage of the same tumour . the negative findings may have been due either to small quantities of the agent present in some tumours or to the kind of relationship of the agent to other cell constituents in these tumours , such as close integration with these constituents , different from that in other tumours which were found positive in the biological tests . microscopical appearance of mammary tumours . in view of the availability of a large number of tumours of a comparatively uniform origin a microscopical study of these tumours was made , and also an attempt to correlate the morphological appearance of these tumours with the presence or absence of the agent . 
as can be seen the majority of tumours in this agentharbouring strain could be divided into roughly equal numbers of type a and type b tumours . the results of the study of 377 mammary tumours in 327 c57 x riii hybrid mice are shown in table xiv . 
among the 327 tumorous mice , 32 had two tumours and 9 had three tumours . as shown in table xiv , the majority of most of the tumours ( 70.6 per cent ) developed during tumours were of type b . the first 12 months , and among them 53 were of type a ( 19.7 per cent ) and 215 ( 79.9 per cent ) were type b tumours ; one unclassified mammary carcinoma also after the first 12 months , 21 tumours belonged to this group of early tumours . were of type a ( 19.4 per cent ) , 77 tumours belonged to type b ( 71.4 per cent ) , 9 tumours were of type d ( 8 - 3 per cent ) , and 1 tumour was unclassified . 
an analysis of the distribution of the different types of tumours in the progeny of tumorous and non - tumorous ( c57 x rii ) f1 hybrids revealed that the progeny of both types of females had a number of each type of tumour similar to that found in the total number of all tumours . 
among the 120 mammary tumours of the descendants of tumorous hybrid females , there were 19 ( 15.8 per cent ) of type a , 99 ( 82.5 per cent ) of type b , and 2 ( 1.7 per cent ) of type d . 
among the 225 tumours in the forcibly - bred progeny of non - tumorous hybrid females , 50 ( 22.2 per cent ) belonged to type a , 166 ( 73.8 per cent ) to type b , 7 ( 3.1 per cent ) to type d , and 2 ( 0.9 per cent ) were unclassified . there were 32 mammary tumours examined in the progeny of a non - tumorous hybrid female which had been bred in a normal way ; five ( 15 - 6 per cent ) were of type a and 27 ( 84.4 per cent ) belonged to type b . 
there was no difference in the distribution of types of tumours in the progeny of hybrids which had been subjected to hormonal stimulation of varying intensity . no correlation was observed between the type of tumour and its location or size or rate of growth or litter sequence of the tumour - bearing mice or age of the animal at which the tumour developed , except in the case of type d tumours , further , there was no all of which developed in mice older than 12 months . correlation between the types of tumours in litter mates or between tumours of mothers and offspring . similar observations were reported by andervont and dunn ( 1950b ) on ( c x c3h ) susceptible hybrids , in which they found 38 per cent of type a tumours , 44 per cent of type b , 9 per cent of type c , and 8 per cent of type d . 
they observed a correlation between the age at which mammary tumours appeared and the type encountered , as in mice of up to 19 months of age 63 per cent were type a tumours and 33 per cent type b tumours , and in older mice 31 per cent belonged to type a and 48 per cent to type b . in another study ( andervont , 1950a ) 38 per cent of tumours were of type a and 46 per cent type b , and in 106 l . 
they did not detect the agent in a c strain female with a squamous type mammary tumour at a late age , yet in her progeny there appeared a type a tumour with the agent and one squamous type cancer without the agent . another two females of the same strain , two tumours of type a and b respectively both harboured the agent ; in their progeny all tumours with the agent were of type a . 
the majority of tumours in old mice were similar to those of mice with the agent ( andervont , 1945b , andervont and dunn , 1949 )  . in hybrid mice obtained from crossings of agent - free low - cancer - strains the majority of mammary tumours were of types c and d , and in those obtained from one of the parents belonging to agent - free but high - cancer strain the majority of breast tumours were of types a and b ( andervont and dunn , 1948a )  . it appears that the genetic constitution of strains used for breeding hybrids influences at least the distribution of the various types of breast cancer . there was no correlation in c57 x riii hybrid females between the presence of the agent , as shown in biological tests , and the type of tumour encountered . of the seventeen tumours in which the agent was found , ten were of type b , six of type a , and one of type d , and among the mammary tumours in which the test failed to reveal the agent , four were type b and two type a , cancer ( table xiii )  . 
the finding of the agent in type d mammary tumour which developed at 17 months is of interest , as it appears to indicate that not all squamous type tumours which appear comparatively late need be agent - free tumours , or possibly tumours in which for some as yet unknown reason it is difficult to detect the agent . 
two agent - harbouring tumours of ( c57 x riii ) f1 hybrids were of type a ( 11 months ) and type b ( 16 months ) , and the two other tumours in which the agent was not detected were also of type a ( 10 months ) and type b ( 11 months )  . 
among the fifteen agent - harbouring tumours of c57 x riii hybrid progeny , five were type a and arose at the age of 9 to 13 months , nine were type b and developed at 7 to 17 months , and one type d at the age of 17 months . 
among the tumours in the hybrid progeny in which the agent was not detected , one was of type a ( 18 months ) and three of type b ( 8 to 10 months )  . in andervont and dunn 's experience ( 1950b ) the majority of tumours ( 84 per cent ) in hybrids developed at the age of 18 to 29 months and the rest during the first 17 months . 
they also found no correlation between the microscopical appearance of a tumour and the presence of the agent . some of the early appearing tumours in which the agent could not be detected were of type a or b ( andervont , 1945b , 1950a )  . foulds ( 1949 ) described the microscopical appearance of breast tumours in his c57 x riii hybrids as " unmiihlbock ( 1952 ) found the morphology of tumours in c57 x d remarkable "  . hybrids of little assistance in the study of the part played by the agent in the development of these tumours . 
he also noted more unusual features in tumours presumably free of the agent compared with those harbouring the agent , yet the tumours accumulated in later litters of c57 mice following mating to high - cancerstrain males , in which the agent was presumed to be present , had an appearance like that of agent - harbouring breast tumours , in spite of their late average age 108 l . 
dmochowski of development ( 20 months )  . there appears to be a greater variety in appearance of mammary tumours in mice of strains in which the agent could not be detected ( andervont and dunn , 1950a ; 1950b ; heston , deringer , dunn and levillain , in the present study all tumours of type d developed 1950 ; muhlbock , 1952 )  . after 12 months of age . similarly , andervont and dunn ( 1950b ) found this type of tumour to be very rare in younger hybrid mice in which the agent could be detected , although , as shown in this study , this type of tumour even at a late therefore the greater frequency of squamous age may harbour the agent . metaplasia in tumours of old hybrid mice , if the age of 17 months could be considered as a comparatively late age , need not indicate at least in every case their development without participation of the agent , contrary to the previous sugthere is no doubt , however , about the greater gestion of kirschbaum ( 1949 )  . frequency of squamous type tumours in agent - free high - cancer - strain or susceptible mice ( gardner , 1947 ; heston , 1948 ; heston , deringer , dunn and levillain , 1950 ) than in similar mice with the agent , but they do appear occasionally in agent - carrying strains of mice as observed by dunn ( 1945 ) , andervont and dunn ( 1950b ) , and in the present study . from these observations it may be concluded that no particular microscopical appearance of mammary cancer in hybrid mice can be correlated with the presence or absence of the agent , in spite of the difference in distribution of the particular types in various strains of mice . 
thus a variable but low tumour incidence was reported by andervont and dunn ( 1948a ) in hybrids from reciprocal crosses of low - cancer - strain ( c , i , c57 ) mice and a higher but still comparatively low tumour incidence in the hybrid progeny of low - cancer - strain ( c ) females and agent - free high - cancer - strain ( dba - ) males , in spite of increased hormonal stimulation . 
dmochowski showed a high incidence after mating to one ( c3h ) high - cancer - strain male developed a much lower incidence ( 30 per cent ) when mated to other ( a ) high - cancerstrain males . females of strains with low susceptibility may show similar differences . 
even after the 10th pregnancy of low - cancer - strain females mated to males with and without the agent , these two types of females when used as foster mothers induced a similar tumour incidence in the test mice . 
dmochowski tumour age ( 19 to 25 months ) in both types of hybrids is characteristic and hormonal stimulation was assumed to be the cause of these tumours ( muhlbock , 1952 )  . 
the development of mammary tumours in the descendants of both tumorous and the majority of non - tumorous hybrid progeny ofc57 females which remained tumour - free after mating to agent - carrying males in the present experiments as well as the detection of the agent in the majority of the tumours tested indicate the transfer of the agent by riii high - cancer - strain males . though not all ( 057 x riii ) f1 hybrids developed breast cancer , the transfer of similarly , the agent must have taken place in the majority of the females . bittner ( 1952a ) noted a high incidence of tumours and the presence of the agent in the descendants of cancerous and cancer - free hybrid progeny of certain strain females mated to agent - carrying males . 
the presence of the agent was assumed in mammary tumours which appeared in hybrid progeny of later litters of some c57 females mated to high - cancer - strain ( d ) males ( muhlbock , 1952 ) because of the high tumour incidence , in spite of the late age at which the tumours appeared . 
as a result of this transfer , only few tumours in the hybrid progeny develop early and harbour the agent , while the majority of transfer of the agent tumours develop late without participation of the agent . to embryos , however , appears to be doubtful , because of the absence of the agent in high - cancer - strain embryos ( dmochowski , 1949c ; hummel and little , 1949 )  . the passage of the agent from embryos , should they become infected in utero , is also questionable because of the reported neutralisation of the agent by placenta transmission of the agent in utero would ( hummel , little and eddy , 1949 )  . also contradict the basis of the discovery of the agent itself . 
the increase in tumour incidence in hybrid progeny of later litters ( andervont and dunn , 1949 ; bittner , 1952a ; muhlbock , 1952 ) and the high incidence of tumours observed in the descendants of later litters from hybrid females observed in the present experiments may indicate either a transfer of the agent to females repeatedly mated to agent - carrying males and / or gradual increase in the agent , transferred by mating , during its long latent period under the influence of hormonal stimulation ( repeated pregnancies )  . 
the low incidence of tumours observed in the hybrid progeny of some derivations need not necessarily be interpreted in the same way as the small number of tumours induced in mature mice which had been given the agent , as suggested by muhlbock ( 1952 )  . 
a high incidence of tumours obtained in mature mice of some strains after repeated injections of material containing the agent ( dmochowski , 1945a ; muhlbock , 1952 ) , and a small incidence in mature mice of other strains ( bittner , 1952b ) , indicate that the genetic constitution is the more likely explanation for the different tumour incidences in transmission of the agent by the sperm to lowhybrids of various derivations . cancer - strain females , followed by its transmission to their hybrid progeny in the mnilk of these females ( bittner , 1952a ) , appears to be the most likely way in which the agent gains access to hybrid females , although in females of some strains it may only occasionally take place ( miihlbock , 1952 )  . 
the observation of several generations of descendants of hybrid females can give a clear picture whether the transfer of the agent has taken place or not , as shown in the present study . 
under the same experimental conditions some hybrid females may develop mammary tumours while their litter - mates may fail to show tumours ; their descendants may show a similar variation in their behaviour . thus , the study of the behaviour of the hybrid progeny of low - cancer - strain females , especially of the descendants of later litters of the hybrid progeny , can only decide whether or not the agent has been transferred by the male parent . the observations on tumour development and the presence of the agent in 114 l . 
dmochowsk1 the descendants of the hybrid progeny obtained by mating c57 black straini females to agent - carrying riii strain males , made in the present experiments , appear to indicate an interesting possibility in the agent - host relationship which may be the outoome of gradual mcrease in the amount of the agent or its activation in some hybrid females , while in other hybrid females it appears in quantities large enough to be detected immediately with the development of breast cancer in the first generation of hybrid progeny . this may be on one hand the result of individual variations in the genetic constitution of hybrid females , and on the other hand the outcome of varying quantities of the agent which the hybrid females obtain from their low - cancer - strain mothers mated to high - cancer - strain within the framework of individual differences in the genetic make - up males . and / or quantities of the agent obtained , inbreeding combined with hormonal stimulation also exerts its influence . 
thus we have the situation , encountered in the present experiments , that under the same experimental conditions some hybrid females develop mammary cancer and others ( even their litter mates ) do not show breast cancer ; some of the tumorous females do and others do not reveal the agent ; some of the progeny of the cancerous hybrid females may develop mammary tumours which again may or may not reveal the agent , and other progeny of the same cancerous females do not develop tumours ; the progeny of non - cancerous hybrid females may develop tumours which contain the agent . 
the development of breast cancer in some of the ( c57 x riii ) f1 hybrids only after foroed breeding may be explained by the transmission of small quantities of the agent by at least some of the c57 black strain mothers after mating to riii agent - carrying males . 
the high , although varied , tumour incidence in the progefny of these hybrids may be explained by the origin of these females as well as of their progeny from late litters and therefore an increase or activation of the agent in these litters , enhanced by inbreeding and increased hormonal andervont and dunn ( 1950b ) also observed that under the same stimulation . conditions some low - cancer - strain females developed and others failed to develop breast cancer , and some females with tumours possessed and others lacked the there was also no correlation between the presenco of the agent in these agent . females and its presence in their hybrid progeny , cancerous females with or without the agent giving rise to hybrid progeny with only late tumours apparently without the agent , or to progeny with both early tumours with the agent and late tumours without the agent , although they were litter mates . therefore , again , the presence or absence of the tumour and / or the agent in the mother did not necessarily involve the presence or absence of the agent in her progeny . andervont and dunn ( 1950b ) noted on several occasions among the hybrid progeny with late tumours that their litter mates had early tumours with the agent , and on one occasion a hybrid female with an early tumour harbouring the agent had progeny with either no tumours or only late tumours without the agent , which suggested the disappearance of the agent ( andervont and dunn , 1949 )  . bittner ( 1952a ) also reported on the hybrid progeny of some derivations with low mammary tumour incidence that some of them gave rise to descendants with a high incidence of tumours harbouring the agent . 
thus the variable results appear to be due to variations in the genetic make - up of both the hybrid females and their progeny , which in turn leads to variations in the amount of the agent transmitted . a more favourable genetic make - up may account for an increased amount of the agent and its detection . 
the appearance of mammary tumours in some low - cancer - strain females ( c3hb x ax ) mated to agent - free ( c3hb ) males and the high incidence of tumours in their descendants , on the basis of which the presence of the agent was assumed although the tumours were not tested biologically ( bittner , 1952a ) , is one at the moment rather perplexing sudden " de novo " appearance of the agent was therefore also observation . considered as a possible explanation of some of the findings ( andervont and dunn , 1949 ; bittner , 1952a )  . this consideration was based on previous observations of bittner ( 1941 ) on the sudden appearance of the agent in some susceptible ( ax ) mice , deprived of the agent by foster nursing by low - cancer - strain mothers , which remained free of the agent for seven generations , and on similar observations made recently by bittner ( 1952a ) on susceptible mice of another strain ( c3hb ) which remained free of the agent for sixteen generations following foster nursing before the appearance of breast cancer in one of the females , which then gave rise to progeny with a high incidence of mammary tumours . according to the writer 's opinion , these observations of a sudden appearance of the agent may only show the length of time during which the agent may lie dormant or the time required before the agent , originally present in small amounts , increases in quantity sufficient to induce breast cancer in combination with other known and unknown factors . of the known factors , either a change in the genetic constitution of the animal concerned alone and / or increased hormonal stimulus may , at least in part , be responsible for the activation of the agent . bittner ( 1939a ) reported the appearance of some mammary tumours in mice without the agent , and strong ( 1943 ) stressed the influence of hormonal factors in such tumours . 
the difficulties encountered in the detection of the agent in breast tumours appearing late in the life of mice and the comparative ease with which it could be shown in tumours developing early ( andervont , 1950a ) , further the isolated tumours in hybrid progeny of early litters and the accumulation of tumours in hybrid mice of late litters ( miihlbock , 1952 ) , led to the conclusion that there may be two types of mammary tumours in mice . 
one type of tumour would be the result of all three factors taking part in its development , the other type would be the result of hormonal and genetic factors without participation 116 l . 
dmochowski of the agent ( andervont , 1950a ; muhlbock , 1952 )  . however , the possibility of the agent being involved in both types of tumours was not discounted by andervont ( 1950a )  . 
the genetic constitution and intensive hormonal stimulation were considered adequate by heston , deringer , dunn and levillain ( 1950 ) to give rise to mammary tumours in susceptible ( c3hb ) mice , originally derived from mice deprived of the agent by foster nursing , but they also stressed that absolute proof of the absence of the agent from such tumours was lacking . 
the appearance of only a few tumours in the hybrid progeny from reciprocal matings of these ( c3hb ) mice with low - cancer - strain ( c57 ) mice with no evidence of an increase in tumour incidence in the hybrid progeny of later litters , as originally reported by bittner ( 1944 ) in mice of agent - carrying strains or in hybrid progeny from low - cancer - strain females and agent - carrying males , again led heston and deringer ( 1952 ) to suggest that some mammary tumours develop in the absence yet , in hybrid progeny of similar mice of other strains , bittner of the agent . ( 1952a ) observed the appearance of tumours harbouring the agent . further , the agent has been detected in some mammary tumours appearing in comparatively old hybrids , as shown by bittner ( 1952a ) and in the present study . in other late tumours as well as occasionally also in early - developing breast cancers the agent could not be detected by any , so far , employed testing procedures as noted by andervont ( 1950a ) , andervont and dunn ( 1950b ) , and by the writer . thus , intensive hormonal stimulation combined with a suitable genetic background influence the origin of mammary tumours in hybrid mice , increase their there is no doubt that the mammary incidence , and accelerate their appearance . tumour agent takes a part in the development of breast tumours appearing up to a certain age , although not all tumours of early appearance in hybrid mice reveal its presence . 
 ( c57 x ri11 ) f1 hybrid females , obtained by mating agent - free c57 black strain females to agent - harbouring riii high - cancer - strain males , developed a 14 per cent incidence of mammary tumours at an average age of 13 months after bearing in quick succession an average number of 6 - 4 litters . their litter - mates , bred in a normal way , died free of tumours after rearing an average number of 3 litters . 
analysis of parent - offspring correlation in the distribution of tumours in the descendants of the hybrids revealed that the progeny of tumours and of the majority of non - tumorous hybrids had a greater chance to develop cancer if the parent developed cancer than if the parent died without a tumour . 
thus there was a strong indication of the presence of the agent in these hybrids and of its transmission to their progeny , which showed an increasing number of tumours following the combined influence of inbreeding and intensive hormonal stimulation . 
biological tests for the presence of the agent in twenty - three mammary tumours were positive in seventeen and negative in the remainder of tumours . the age of tumours in which the agent was detected varied from 7 to 17 months , and that of tumours in which the agent could not be detected from 8 to 18 months . these tests , combined with the observed distribution of tumours in the descendants of hybrid mice , showed that under the same experimental conditions some hybrids developed tumours which either harboured the agent or failed to reveal it , while other hybrids , even their litter mates , died without tumours . 
some of the progeny of tumorous hybrids failed to develop tumours and others of the same females developed cancer in which again the agent was either demonstrated or could not be shown . 
dmochowski which as a rule developed in older mice above the age of 12 months . there was also no correlation between the appearance of mammary tumours in parents and their offspring . 
with the advent breast cancer . of x - rays the same effect was brought about by ovarian irradiation ( foveau de courmelles , 1926 ; ahlbom , 1930 )  . on the experimental side , the work of lathrop and loeb ( 1916 ) , loeb ( 1919 ) and murray ( 1928 ) demonstrated the part played by the ovary in the production of mammary tumours , while lacassagne ( 1932 ) showed that , in certain circumstances , mammary carcinomata could be induced by the injection of oestrogenic substances . interest in the problem was further stimulated by the work of huggins and hodges ( 1941 ) on the treatment of carcinoma of the prostate by castration and stilboestrol . it was logical that the next step in the management of advanced breast testosterone propionate was cancer in women should be the use of androgens . tried with success by ulirich ( 1939 ) and by many later workers . the treatment of women suffering from breast cancer with one of the oestrogen preparations was apparently illogical , although zondek ( 1936 ) had put forward the suggestion in 1936 . 
they are rare , however , and in over 4000 cases of breast cancer observed in this department no spontaneous regression has so far been noted . the survival rate will be mentioned in the groups of cases to be considered and , although it seems that life can be prolonged with hormone treatment , no attempt is made to claim success on this account alone . the responses were graded as follows : a . 
good responses were seen in all types of metastases , skin nodules , glands , pulmonary and skeletal in 3 patients with osteolytic bone metastases there was radiological metastases . evidence of new bone formation . in 4 a pleural effusion disappeared and in 4 it diminished in amount . 
5 illustrates the findings on 9.x.46. patients treated by surgical castration and testosterone . in 1941 a small group of patients was treated by surgical castration , accompanied by the administration of testosterone . this was done in an attempt to find out why there were some failures with ovarian irradiation . it was thought that ovarian function might recover to some extent after irradiation and that the effect of o6phorectomy would be more lasting . nine patients with advanced breast carcinoma were treated in this manner by o6phorectomy , followed by daily intramuscular injections of 25 mg . 
testosterone propionate for periods up to 3 months . only one patient showed a slight response . she was a premenopausal woman of 40 with an inoperable breast carcinoma and bone metastases . 
the primary tumour became smaller and the glands disappeared temporarily , but no effect was noted on the skeletal metastases . patients treated by oestrogen therapy . in the latter part of 1942 it was decided to investigate the value of oestrogens in advanced breast carcinoma , and since that time the following oestrogens have been tried : stilboestrol dipropionate , dienoestrol , triphenylchlorethylene and ethinyl oestradiol . 
twice a day sometimes caused sufficient water retention to increase the pleural effusion and add to the patient 's dyspnoea . it was remarkable to find in a few such patients that doses as small as 0 ' 5 mg . 
the number of patients having no symptoms attributable to the hormone while taking stilboestrol was 122 , while many of the remainder had symptoms which did not inconvenience them greatly , the most common being nausea and vomiting at the commencement 36 maryidouglas of treatment . 
even pleural effusions dimished in amount , and in 3 cases disappeared altogether with no treatment other than stilboestrol dipropionate . it is also very interesting to note that in this series 13 patients with bone metastases experienced relief from pain , while in 6 , new bone formation was demonstrated radiologically in osteolytic lesions . 
no post - mortem was carried out , but this gastric tumour was probably metastatic in nature from the carcinoma breast . the following case illustrates the improvement which may take place in a patient with a pleural effusion : ca8e no . 
of testosterone propionate daily , given intramuscularly . treatment was continued for 3 to 4 weeks , and if the patient 's condition showed some improvement , further treatment was given either by means of an implant of 400 to 600 mg . 
one patient who was comatose with cerebral metastases improved sufficiently under treatment with testosterone to subsequent post - mortem examination confirmed attempt crossword puzzles . the presence of large intracerebral metastatic deposits , which presumably had regressed only temporarily under the influence of testosterone . in another patient a large pleural effusion did not cause any further respiratory embarrassment , and required aspiration only at increasingly longer intervals . this patient is still alive 25 months after the commencement of treatment . only one patient experienced relief of pain from skeletal metastases while another patient with metastases in bone stated she receiving testosterone . felt the pain easier when the drug was withdrawn . there was no radiological evidence of repair occurring in bone metastases . 
the series , although small , is in this respect at variance with the results so frequently reported in the literature ( adair et al . , 1949 ; kaae , 1949 ; report of the council on pharmacy and chemistry , 1949 )  . only one patient could not tolerate the drug . she was a woman of 43 with cerebral metastases , who developed very severe vomiting , and treatment had to be discontinued after she had received 150 mg . apart from this one patient no one was upset by treatment . 
treatment was also given to post - menopausal women to determine the effect . many of these patients had already failed to respond to other methods of hormone therapy , and they were beyond the aid of all other forms of treatment . the pituitary was irradiated by two opposed fields , each 6 x 8 cplaced in the temporal region , and a dose of 3000r was delivered in 3 weeks to the region of the sella turcica . a series of 37 patients was treated between october , 1949 , and october , 1950 , and the results are shown in table vi . as will be seen from table vi , only 2 patients showed a good response . 
the recurrence had become flatter for 3 months , but after that had spread again . following pituitary irradiation complete healing took place slowly , but new nodules appeared 10 months later . of the 2 women showing a fair response , the first was aged 46 and premenoshe had a skin recurrence on the chest wall within the irradiated area pausal . and was treated by pituitary irradiation in december , 1949 . slight regression of the recurrence was noted for 3 months , but then the disease became widespread and she died on 6 . 
none had shown any response to the other types of hormone treatment . it would seem from this that pituitary irradiation may be of value in the tylie of case suitable for ovarian irradiation , or in cases where ovarian irradiation has already been given with some good temporary effect . there is no doubt that pituitary irradiation was the least well tolerated of all fourteen patients were very upset by the treatment it is possible that a modification of technique forms of hormone therapy . before the course was completed . and dosage would overcome some of these difficulties . of the 37 patients , 21 have died within one year , the average survival being 2 to 9 months after the commencement of treatment . 
no good results were seen in bone lesions apart from relief of pain in 2 cases , although , of course , the series was small , and treatment may not have been continued over a long enough period . the reports in the literature on the efficacy of testosterone are very variable . farrow ( 1944 ) noted a deleterious effect in female patients , nathanson ( 1944 ) observed no effect at all , and various later workers ( adair , 1947 ; adair et al . , 1949 ; kaae , 1949 ) reported a proportion of good responses in skeletal and extra - skeletal all are agreed that testosterone may produce a beneficial effect metastases . on the general health but this is a non - specific effect , and due partly to the stimulating effect of the hormone on protein metabolism . it is , however , important not to assess improvement in general health as an anti - carcinogenic effect . with both oestrogen and androgen therapy some responses were noted here after the drug was stopped - a withdrawal response . farrow ( 1944 ) also noted this occasionally in the metastases after withdrawal of either oestrogens or androgens . consideration of the mode of action of hormone therapy . wvhile hormone therapy is widely employed , the basis of treatment remains largely empirical . the extension of our knowledge of the exact mode of action would be of great interest , and might result in further advances in this form of therapy.. 
the clinical results obtained , however , appear to be due to some modification of the endocrine status of the patient . for example , in a young patient who has not reached the menopause , oophorectomy or ovarian irradiation causes a sudden withdrawal of the natural ovarian hormones which influence the rate of growth of the cells of breast tissue whether these cells are normal or malignant . 
at this stage of our knowledge , however , it is doubtful if it would be justifiable to use a higher dosage . the administration of an artificial oestrogen again modifies the endocrine status . 
the oestrogens may produce a direct effect on the breast cancer cells , or the effect may be obtained indirectly through the anterior pituitary . if the action is a direct one , the best results would be expected in older women . tn an older patient , for example a woman who is 5 or more years past the nmenopause , there is little or no circulating oestradiol , and the addition of oestrogens produces a change . after the passage of time , however , the body , and in particular the breast cells , may become readjusted , and this might explain why the good effect passes off . the work of zondek suggests that the oestrogens may have an indirect effect through the anterior pituitary . 
zondek ( 1936 ) found that the administration of large doses of oestrin produced a chromophobe adenoma of the pituitary in male rats , that is , in rats not normally subject to the action of large amounts of oestrogen . zondek ( 1947 ) also reports a case in which he gave large doses of oestradiol benzoate to a woman of 216 with metastases from a carcinoma breast . 
the increase in size of the pituitary was due to an eosinophil adenoma . unless the production of an adenoma of the pituitaryr interferes with the output of other hormones the explanation is not very satisfactory in older patients . in a premenopausal patient , a drug such as stilboestrol may cause inhibition of the gonadotrophic hormones , so suppressing natural ovarian secretion , but castration could not be said to be complete not bringing about a true castration . consewhile an artificial oestrogenic substance is circulating in the blood . quently , there is not the same profound change in the endocrine status and no useful therapeutic effect is produced . the question of the administration of testosterone might now be considered . in a premenopausal patient this brings about an artificial menopause and , from this point of view , testosterone might be expected to produce similar results to ovarian irradiation or o6phorectomy . in addition to this , the administration of testosterone must disturb the normal oestrogen - androgen ratio . finally , testosterone , like the oestrogens , causes inhibition of the gonadotrophic hormones of the anterior pituitary ( moore and price , 1932 )  . it may , therefore , like the oestrogens , produce an indirect effect on the breast cells by a disturbance of pituitary function . an explanation must now be sought for the failures . 
how this would affect the response is not known exactly , but it is perhaps significant that few patients with clinical evidence of liver involvement showed any response to any of the methods of treatment mentioned . there may , however , be other factors modifying the response . 
haddow , watkinson and paterson ( 1944 ) suggested that the tumour called " carcinoma of the breast " might in reality comprise walpole and paterson ( 1949 ) also made the same suggestion , several categories . even going so far as to say that a tumour might produce an " anti - hormone " or inhibitory factor antagonising the action of the oestrogen . 
of advanced breast carcinoma treated by hormone therapy has been surveyed and the results obtained have been presented . the findings suggest that , in premenopausal wonmen , the treatment of choice is ovarian irradiation , which was found to produce beneficial results in 30 per cent of patients in this category . in women who are 5 or more years past the menopause , oestrogen therapy would appear to be the most satisfactory form of treatment . the drug found to be most generally useful was stilboestrol dipropionate 5 mg . 
jackson memorial laboratory , bar harbor , maine . received for publication april 20 , 1954 in a comparative study of alkaline phosphatase in tumors , greenstein ( 1942 ) noted that the mouse tumours studied possessed little or no alkahne phosphatase activity with the exception of spontaneous mammary tumors and lymphomas . comparative q values were calculated as the ratio of the percentage of disodiumphenyl phosphate hydrolyzed to milligrams of total n per cubic centimeters of several concentrations of n were taken and the q values remained tissue extract . remarkably constant in relation to nitrogen . 
the highest value for any tumor was the transplanted hepatoma 31 in rats with a q value of ' 542 . kabat and furth ( i 941 ) could not demonstrate alkahne phosphatase by means of gomori procedure in mammary adenocarcinoma spontaneously arising in c3h however , hard , pratt - thomas and belkin ( 1948 ) examined twenty - nine stock . spontaneous mammary carcinomas in c3h , a and dba mice and noted high alkaline phosphatase activity . 
the predominent picture in the mouse tumours examined was the high alkahne phosphatase activity shown by the cells of the acinar units while the stroma and vascular elements were free . 
descenden ' t of a mouse that was bom from a fertilized ovum transplanted into the uterug of a dba mouse this has gone through 320 transplant and was nursed by her dba mother . results from the jackson laboratory indicates 100 per cent transgenerations . plantability in c57bi , and their f , hybrids . 
the histological type is an adenocarcinoma ( sneh , cloudman and woodworth , 1948 )  . the tumor h2712 originated spontaneously in the mammarv gland of ' a c3h mouse in 1948 at the roscoe b . 
the histological type - is an adenocarcinoma . the tumor dbrb originated in the department of genetics , carnegie institute of wasliington in 1918 in the mammary gland of a dba / i mouse and has gone throuo ' h 845 transplant generations . refjults from the roscoe b . 
the histological type is an adenocarcinoma ( strong and little , 1920 ; ' little and strong , 1924 )  . the tumor 15091a originated in the laboratory of the university of a - fichigan in the mammary gland of an a albino mouse in 1928 ( cloudman , 1928 )  . this has gone through 341 transplant generations and shows 100 per cent transplantability in a albino and their f , hybrids . 
the histological type now is that of an anaplastic carcinoma . for the purposes of the experiment the animals were divided into four serieg . series 1 consisted of tumor e0771 transplanted into males and females of c57bl and their f , hybrids between c57bl and a / l . series ii consisted of tumor h2712 transplanted into c3h males and females . series iii consisted of tumor dbrb transplanted into dba male and female . series iv consisted of tumor 15091a transplanted into f , hybrids of c57bl and a / he male and female . the total number of animals of the four series were i 00 and 8 1 . all mice were transplanted with their respective tumor at the roscoe b . 
jackson memorial laboratory and sacrificed at intervals between 7 and 22 days or an average of 16 davs . the am - mals were kired by ether anesthesia and thin slices of the ever , spleen , adrenals , kidney , testes , ovary and the tumor were placed immediately into formoltissues placed in fo ' rmol - saline were stained saline and into ice - cold acetone . by the regular hemotoxyliin and eosin methods . tissues placed in ice - cold acetone were left for 24 hours with one change of acetone . 
they were then placed in cold absolute alcohol over night followed by two changes of benzol of 45 minutes e " ach . they were then imbedded and infiltrated in paraffin at 56 ' c . 
they were then dehydrated and mounted in permount . incubation times in the substrate were as follows : series 1 , ily ill : i minute , 5 miinutes , 15 minutes and 1 hour , and series iv : i.minute , 5 minutes , 15 minutes , i hour , ij hours , 2 hours and 21 hours . 
a total of 1124 shdes was prepared . the shdes were read and visually graded according to their intensities from i to 6 . in this way a relative assay could be arrived at which showed a distribution within each incubation time , and the earliest reaction or end point could be ascercontrols were run . 
at i minute incubation time 29 of the 39 reactions had a reaction intensity of one and hence this was considered as the " end point . " at 5 minutes there were no negati ' ve reactions , the majority of reactions being two or three . 
the distribution was , however , strikingly different from the other tumors and will be referred to in the subsequent section . series iii consisted of 48 transplanted dbrb mammary carcinomas . 
l. - tumor e0771 transplanted into c57bl and f , hydribs ( series i )  . alkaline phosphatase reaction at 15 minutes ' incubation tixne slides show irregular areas of activity . 
3. - tumor dbrb transplanted into dba ( series iii )  . alkaline phosphatase reaction at 15 minutes ' incubation tixne shows a tendency of the peripheral cells of islands to show more activity than central portion . 
7. - tumor h2712 transplanted into c3h ( series ii ) under high power magnification . note the peculiar and intense distribution at the borders of cells lining the lumens . in the center is also seen gomori positive acerular material in a very small lumen . 
4 , 5 , 6 at 60 minutes incubation period . it is quite evident that 1.5091 a exhibits no alkaline phosphatase activity and further extension of the incubation time to 2 - 1 hours showed no reaction except in the vessels . in series i tumor e0771 is composed of irregular islands of tumor tissue . these varv in size and shape . 
the islands are fairly solid with the exception of small areas where itimens can be seen . larger iiimens are lined by several rows and layers of cells . most of ' the lumen8 are very small . 
8 shows a photoreticular material with many large thin - walled vessels . micrograph of this tumor stained by hemotoxyl - in and eosin showing the islands of the interstitiat tumor tissue with an attempt at luminal and tubular forma - tion . tissue seen to the left is loose and reticular in nature . there seem to be attempts to form tubular structures . the phosphatase reaction began during the first minute of incubation time with a blackening or graying of the cytoplasm . this gave a gray appearance to the slide except in such areas where the blackening is much more pronounced . 
at this time enzyme activity large irregular can be demonstrated in many areas in the centres of the island . clefts can be distinguished and stand out prominently bv the activity of the enzyme of the cells lining the lumens . intraluminal material which is not apparent in the hemotoxylin and eosin preparation shows intense activity . small globules are present in the cytoplasm of many cells adjacent to lumens or attempted lumen formation . 
the connective tissue and vessels do not react . tumor dbrb iin series iii under hemotoxylin and eosin stain shows a more lobular distribution than either e0771 or h2712 and is shown in fig . 
the interstitial tissue is composed of loose connective tissue , connective tissue and large thin - walled vessels . with graded gomori stains the reaction has an " end point " at 15 minutes . here the areas of activity are irregular thoughout the tumor . 
some activity is there is a tendency for present in the small lumens but this is not marked . increased activity at the periphery of the lobule as shown in fig . 
the loose supporting connective tissue and vessels show no activity . in series iv tumor 15091a differs somewhat from the other 3 in that it is a fairly solid tumor not composed of islands or lobules . there are numerous mitosis and the cells vary more in size and shape . 
at i hour this showed rather marked activity . the cells of the peripheral portion of the nodules showed most intense activity . there is no essential difference between the various series . the liver shows , for the most part , two types of reaction . 
the ovary begins in most series with the 5 minute incubation time in the theca externa which shows progressive activity to i hour . ksmall stromal vessels also show activity . all the series were approximately the same . 
one difference that occurs in the e0771 is the presence of doubl - e layers of tumor cells in the attempt at acinar formation . in the 15091 a the tumor is solid with very few smar acini . the overall phosphatase reaction was very intense in e07 7 1 , very much less in this was evident in spite of the fact that h2712 and bdrb and none in 15091a . the rate of growth of the tumor was about the same in all the series . 
numerous hard , pratt - thoma 's and belkin ( 1948 ) mitoses were present in all the tumours . felt that there was a loss of alkahne phosphatase activity in the more anaplastic although it would seem in our series that the anaplastic tumor tumor cells . 15091a having no reaction would point toward such contention , the e0771 is a very rapidly growing tumor with numerous mitoses . 
we would prefer to delay our judgment on this issue until a larger variety and strains of tumors have been studied . an interesting and significant paper which has come to our attention as this work was completed was the observation of shelton ( 1952 )  . this investigator found a tumor in a 6 - month - old strain a female mouse that had been exposed to 400 r whole body x - radiation on the date of birth . 
lymphoma 1 was propagated in a mice from a large tumor mass located in the anterior mediastinum . lymphoma 2 was propagated by subcutaneous injection into strain a mice of fragments of lymph nodes from a mouse bearing the original tumor . strain i grew as a localized tumor with local invasion ' but no metastasis , but strain 2 reacted as an acute leukemia with rapid growth infiltration of the organs and high peripheral count . in determination of the alkahne phosphatase activity it was found the lymphoma 1 showed no reaction while lymphoma 2 showed a reaction as expressed by 5 mg . 
no detectable reaction could be seen by the gomori method in lymphoma i whereas lymphoma 2 was here we have a rapidly growing persumably anaplastic tumor strongly positive . showing an increase in alkahne phosphatase reaction . in our laboratory we have also determined the alkahne phosphatase activity as expressed in gamma of phosphorus per mflhgram of nitrogen at 30 minutes incubation time in a large series of these 4 mammary tumours . 
carr. from the poultry re8earch centre , edinburgh , 9 . recieved for publication january 19 , 1953 . most cancer investigations involve the use of small rodents , and it is now clear that many of the " generalisations " obtained from research on this material break down when other animals are considered . while the relevance of any result obtained with grafted tumours to the problem of spontanous cancer may be doubted , it seems desirable to report the results obtained by parallel work on non - rodent material in order to offer proof that similar results are , or are not obtained . the grch / 15 tumour is a non - filterable fibro - sarcoma originated by peacock in 1939 ( peacock , 1946 ) , and by his courtesy made available to other workers it is through the animal breeding unit of the british empire cancer campaign . readily distinguished from the virus - induced tumours by the absence of the mucoid material that they all produce , but unless the section is specially stained for this , microscopic differentiation is less easy . transplantation was always made into brown leghorns of greenwood 's flock ( in one of which the original was induced ) , either by implanting small pieces with a fine trocar and cannula , or injection by syringe of the suspended material left after shaking minced tumour or tumour ground with sand and saline . transplants were usually made into each pectoral muscle , and by the trocar and cannula method " one - sided " negatives occurred about 1 in 20 times , while the second gave less than 1 per 100 " one - sided " failures ; the incorrect negatives due to experimental errors would therefore be 1 in 400 and 1 in 10 , 000 respectively , which can be ignored . 
the material for this account is based upon 60 transplant generations involving some 600 birds over a period of 8 years . in most experiments the birds were 6 to 10 weeks old when the tumour was implanted . in the bird the tumour appears as a hard white lump , though after the alteration in the growth rate the texture was softer , and microscopically the cells appeared rather more compact . 
983 , from which all material for the 32nd and subsequent generations derived . it is interesting that the change coincides with a distinct alteration in the conditions of husbandry , for the facilities for keeping animals at the experiment station were at first not optimuno cages were available for birds , and the food comprised various ration - free products , which produced a series of deficiency diseases ranging from protein to multiple vitamin shortages . 
when the conditions were built up to those nearer first - class management the change in appearance and behaviour of the tumour remained . there is no direct evidence that the change in conditions caused the alteration of the tumour , and it remains possible that it was a coincidence . the most notable change in the tumour was in the rate of growth . 
by contrast , in only one bird out of many thousands has this organ been the site of a rous 1 metastasis . of 352 birds killed and examined with large growths in the breast muscle , 51 had metastic growths in one or more sites . 
nor is it due the conditions for tissue transto a failure of the bird to produce iso - antigens . plantation , however , seem to differ markedly from those of the lower rodents . for example , organ transplantation between fowl varieties is a normal experimental technique , used for example by greenwood ( 1928 ) to investigate the relation of the testis to henny feathering of males of some breeds ; yet transplantation of an adrenal is regarded as a novel event in the mammalian field similarly , the elaborate integumental decorations of birds early ( darcy , 1952 )  . attracted the attention of zoologists , and the results of skin transplant between different genera were being embodied into the general assembly of zoological theory before tissue iso - antigens were recognised . it is possible to suspect that a similar mechanism is indeed operative in the mammalian field , but the methods used are not refined enough to detect it . 
the domesticated rat and mouse have an oestrous cycle of only a few days in length , as compared with the sharply - defined annual cycle in the hen , and lesser cyclic variation of the cock . 
even the pregnancy of 3 weeks is rather short for observations in the rat and mouse , but it is significant that foulds ( 1949 ) found some evidence of a variation in tumour growth and structure in the mouse , and there are many reports of pregnancy influencing the course of tumours in the human . the appearance of many cancers at an age when the sexual functions are failing may be another aspect of this . this would seem to be a point of considerable importance , for it indicates that control of a malignant tumour would be possible within the limits of normal physiological variations ; similarly studies on the cancers induced by chemicals , and more especially by x - rays , indicate that the production of the malignant change and the appearance of a progressive tumour are distinct phenonema , a separation that is even more obvious with the mouse milk factor , where infection takes place soon after birth but the tumour appears months later , and only if the endocrine history of the host has been suitable . 
carr aries in the proventriculus in older birds carrying the " slow " tumour refers to a difference in the biochemical suitability of the organ in the older hosts is it is to be expected that the differences of tissue permeability with unknown . age ( duran - reynals , 1942 ) would also have some influence upon the metastatic growths . the absence of any neutralising action in the sera of fowls immunised against the grch / 15 sarcoma is in contrast to the findings of gottschalk ( 1943 ) for sarcoma 16 . but it is well known for commercial birds suffering from the related " leukosis complex " viruses to have death - rates of up to 40 per cent and carrier rates of nearly 100 per cent , so that such a finding is only of value if it can be stated that such carriers are not a complicating factor . 
a fast - growing mutant strain retained this property , and the mutation was not associated with an increased frequency of takes , though the distribution of secondaries was altered . 
clemmesen. from the danish cancer registry under the national anti - cancer league , copenhagen . received for publication december 10 , 1949 . developments in recent decades have made the term " cancer statistics " inadequate for the description of the ways in which statistics have contributed it is time that this term was reserved for statistical treatment to cancer research . of results , while statistical research into the occurrence of human cancer , be it from racial , genetical , geographical , occupational or other sociological points of view , should be included in the term " cancer demography . " this will be the case in the following . unlike many other branches of science joining in the research of cancer at some stage of its development , cancer sociology can point to a long , though most often neglected , history . 
when percivall pott , in 1775 , described the chimney sweep 's cancer , not only giving its clinical features , its treatment , and its social aetiology , but also taking active steps toward its prevention , in which we have finally succeeded , it was the first step in cancer sociology . pott 's observation of the latent period of scrotal cancer in chimney sweeps contained a very obvious clue to the experimental production of cancer , but experimental workers seem to have been too fascinated by experimental and pathological problems to take a lesson , not to speak of inspiration , from clinical or sociological observations , and 140 years passed before cancer was provoked experimentally by tar and soot . however , it seeins still more surprising that after this experience we have spent decades since young and russell 's demonstration in 1927 of a causal relationship between alcoholic consumption and cancer of the upper digestive tract in examining the carcinogenicity of numerous other compounds , while alcohol has been examnined only in a single experiment on a small scale ( krebs , 1928 )  . similarly it is well known that the first birth increases the possibility of a later cervical cancer , but where are experiments based on this and similar facts ? it would not seem unlikely that the slow progress in obtaining results of practical value in the fight against cancer is to a large extent due to our theoretical way of tackling problems . for instance , it is not unlikely that the future will reveal very interesting facts with regard to the influence of cosmic radiation on the incidence of cancer in heavily inbred animals of some kind , but there is considerable evidence that unless the energy released by such radiation shows a j . 
clemmesen different affinity to individuals of the various social classes , there must be social factors of a far more decisive character influencing the incidence of cancer in man . in order to bring about a closer contact between cancer research and problems of clinical importance , a more thorough investigation into the aetiology of cancer should be attempted by cancer demography through mass observations . 
to this we may add a frequent tendency among the former to take a more national and less universal point of view than is common so far in the medical world . 
an example of this is the variation in the proportion of gastric cancer in different countries , which has been discussed more often than the possible sources of error involved . for instance a first - class textbook of pathology states : " the incidence of gastric cancer in sweden and czechoslovakia apparently is about three times that of england . 
no satisfactory explanation has been offered for these interesting findings " ( anderson , 1948 ) as far as the present author has been able to establish , the reason for some of the differences may be that death certificates in the thinly populated areas of northern sweden for practical reasons are issued by parsons . furthermore , it will appear from the demands already mentioned that a direct comparison of percentages without a further analysis with regard to age distribution is unsatisfactory , especially in the case of a site such as the stomach , in which the establishment of a definite diagnosis is difficult . admittedly , death certificates have in the past rendered valuable information , especially in the hands of the english registrar - general , but this is no guarantee that death certificates from any country will produce similarly reliable details . it is vital to the use of death certificates that they are referred to the domicile of the patient , and not to the locality where death has occurred . 
and it must also be remembered that occupational statistics based on death certificates theoretically demand that the occupation of the deceased person should be stated from the same source as in the census , that is , some registration office , and not from the case - record or the statement of relatives , although tlis might not cause serious errors . comparisons of death certificates of different date are often made without the necessary regard to the dangers of this method . pedigrees of greater length may for instance be misleading because the frequency of cancers of various sites , whether apparent or real , will differ from one generation to the next . for sites of cancer where therapy is improving death certificates are decreasing in value as indicators of frequency , while other sites may show an apparent increase in frequency due to progress in diagnostic technique , and post - mortem figures will also be subject to this influence . 
heady and kennaway ( 1949 ) suggest that the proportional occurrence of lung cancer among the post - mortem total will serve as an indicator of changes in the incidence among the whole population . such figures are , however , influenced not only by the experience and information available to pathologists , but also through progress in the therapy of early complicating pneumonias and of lung cancer itself . * it is generally assumed that progress in diagnostic technique will cause an increase in the number of cancer cases registered , but according to the author 's experience gastric cancer tends to be overestimated , and will often decrease in frequency with improvements in medical facilities . consequently , comparisons between different countries or periods based on death certificates as well as on other sources of medical information demand additional knowledge of a more direct character . * readers of their review are recommended to compare the order of magnitude of the yearly totals criticized with those accepted as a basis for considerations , j . 
clemmesen for years hence , however , death certificates are bound to play an important part in demography of cancer , because they will be the best information available for the many cases not treated in hospital . 
even in the case of compulsory registration there will remain a number of notifications from general practitioners amounting in quality to little more than death certificates . it is also important to.the statistician to realize that the difference in quality of diagnosis between hospitals and general practice will cause a difference in the material , unless practically all cases are examined in hospitals , and this will be the case for only another difference between these groups will appear very few sites of cancer . in the age distribution curves , which must be based on the age at onset of the cancer , theoretically at the onset of symptomns . accurate statements on this item are unfortunately very difficult to obtain on death certificates , and for hospitals it is most practical to state the date of the first admission , which has the advantage of being an accurate reality . for all these reasons it will be evident that complete statistics on the incidence of cancer in a given area should contain figures for the number of cases treated in hospital for each site of cancer , and separate age distribution figures for this it is not uncommon for authors part of the material as well as for the total . dealing with a single site of cancer to leave out the total cancer incidence in the population concerned , but this is not permissible when we do not know the interrelations between cancers of different sites . 
the percentage of cases examined histologically or by autopsy should also be given for each site as an indicator of the basis of the diagnosis , and is particularly valuable in statistics giving figures for diagnoses of a histological character . 
at the moment such figures can only comprise a part of the cases really occurring , and it is most important to know the actual number of microscopical examinations from which they are collected , even in the case of a diagnosis such as " sarcoma , " which sometimes may be founded only on a macroscopical examination . unfortunately , many publications on cancer demography are inadequate with regard to statistics , and amount to little more than a summary of the author 's own conclusions , although they should contain all the basal figures for both the normal and the cancer populations , as well as the formulas applied , not only with regard to an independent judgment by contemporary workers , but also with a probably it is mostly view to retrospective work in the same field in future . editors and not authors who are to blame for such omissions , and the same applies to diagrams , which are as essential to such articles as are photomicrographs to histological or roentgenograms to radiological publications . cost will probably also be blamed for the fact that most of the valuable material on the occurrence of cancer is hidden away in statements from public health authorities . 
a unification of publications in this field , so that they could be collected in journals accessible to workers in experimental cancer research , would contribute far beyond its cost to the vital connection between experimental research and cancer demography . but it is most important in such publications that the author ascribes his findings to factors of some established certainty , and is reticent in advancing readers may find , even in new theories of his own on the aetiology of cancer . modern publications of some standing , that the well - established connection of alcoholic consumption with the incidence of certain cancers is paralleled by the influence of tinned or fried food . 
leveaux. * from the westminster hospital , london , s.w.1. received for publication may 12 , 1954 . the earliest recorded description of carcinoma of the pancreas is attributed to mondiere in 1836 . 
da costa ( 1858 ) of philadelphia reviewed 37 cases and gave a comprehensive description of the clinical presentation of this disease with * nmphasis on pain as a prominent sympton in 32 of these patients . 
in not a few cases it is increased by the erect position and hence we find patients seeking relief by stooping and curving their body forward so as to relax the abdominal parietes . " physicians of the french school sustained their interest in this condition , and bard and pic in 1888 observed the common association of a palpable gall bladder with jaundice , and the frequent incidence of cachexia . 
from the descriptions given by these and other observers the concept of painless jaundice as the classical form of presentation of this disease spread widely . mirallie ( 1893 ) found glycosuria in 3 cases , and chauffard ( 1908 ) emphasized distinctive features of growths involving the body of the gland . speed ( 1920 ) , eusterman ( 1922 ) , eusterman and wilbur ( 1933 ) , kiefer ( 1927 ) and other observers have subsequently reported on series of cases , and berk ( 1941 ) has included these in his review of a total of 1449 cases . 
levy and lichtman ( 1940 ) , and duff ( 1939 ) have further clarified the picture of carcinoma of the body and tail of the pancreas , emphasizing early and severe pain , ascites , venous thrombosis , and widespread metastases to liver and peritoneum as important features . towards the end of the last century surgeons became interested in the pancreas , and finney ( 1910 ) quotes a case of total pancreatectomy for carcinoma by billroth in 1884 with recovery of the patient from the operation . gordon - taylor ( 1934 ) successfully removed a carcinoma of the body of the pancreas in 1927 , his patient surviving when the case was reported 7 years later . in spite of such isolated successes , however , attempts at surgical removal gave little promise until , in 1935 , whipple and his colleagues demonstrated the technical feasibility of resection of the head of the gland , and opened a more hopeful era ( whipple , parsons and mullins , 1935 ; whipple , 1938 )  . these and subsequent advances in surgery have greatly intensified the need for early diagnosis in a disease which has been estimated to comprise 1 to 2 per cent of all cancers , and which is by no means a clinical rarity . 
the head was spared in 14 cases ( 30.4 per cent ) , of which 4 cases involved the body alone , 4 cases the tail alone , and 6 cases both regions . 
one case had active thrombo - phlebitis , and 1 presented with paraplegia due to extradural metastases . in many cases the disease was well - advanced by the time that abnormal signs were clear cut . 
per cent in 20 of 40 cases ( 50 per of 8 cases examined by the glucose tolerance test , a diabetic type curve cent )  . was obtained in 6 cases ( 75 per cent )  . these latter cases included 2 of the known cases of diabetes of recent onset , but none of long standing . 
n / 20 sodium hydroxide as the upper limit of normality . johnson and bockus ( 1940 ) reported a raised value in 5 of 8 cases . secretin stimulation of the pancreas was performed in 3 cases , accentuating an already raised level in 2 cases , and producing an abnormal value in 1 . 
per cent in 27 of 33 cases investigated , of which 24 had clinical jaundice . the serum alkaline phosphatase was examined in 26 cases and was raised above 5 bodansky units in 13 , of which all had associated hyperbilirubinaemia . of 13 cases shown to have liver metastases , the alkaline phosphatase was raised in 7 and normal in 6 . the serum cholesterol was raised above 220 mg . 
a normal chloesterol level occurred in 5 cases with associated hyperbilirubinaemia . the cholesterolesters exceeded 50 per cent of the total cholesterol in 20 of 21 cases . it appears , therefore , that these latter three investigations reflect only the presence of biliary obstruction , and beyond this are not helpful in the present diagnostic problem . the plasma proteins were normal in 23 of 25 cases , there being some degree of hypoalbuminaemia in the remaining 2 cases . the cephalin , thymol and colloidal gold flocculation and turbidity tests were normal in all of 22 cases examined . in 3 cases the cephalin flocculations test became positive after cholecysto - enterostomy . the value of these tests in the present connection is that they facilitate exclusion of hepatitis in cases presenting with jaundice , as pointed out by maclagan ( 1947 ) of 46 cases examined , 31 ( 67 - 4 per cent ) had haemoglobin levels below 13 - 0 g . per cent , with an average of 12.13 ( 76 per cent hb . ) for the whole series . 
a relationship between the anatomical position of the tumour and the site of the pain complained of by the patient is suggested . a scheme of investigation is proposed which includes careful radiological studies , a glucose tolerance test , serum lipase and amylase determinations and a bromsulphalein retention test . surgical exploration is advocated where strong clinical grounds alone exist . i wish to express my warm thanks to h . 
bockus , professor of gastroenterology in the graduate hospital of the university of pennsylvania , for all his help and encouragement in this investigation . i am also grateful to a . 
harnett. published for the clinical cancer research committee of the british empire cancer campaign . received for publication july 16 , 1948 . in 1938 - 39 the clinical cancer research committee of the british empire cancer campaign carried out a clinical survey of all cases of cancer seen in the hospitals , both voluntary and l.c.c. 
in the administrative county of london . this was done by means of questionnaires , one of which was filled in by the registrars in the various hospitals for each patient and returned to the clinical cancer research committee for record . 
the work was interrupted by the outbreak of war after it had been in progress for 17 months . by this time 15 , 200 cases of cancer had been registered , of which 2529 ( 16 * 6 per cent ) were cancer of the breast . these patients have now been followed up for five years or more and the records analysed . 
4 - 556 1 8 + 0 66 . the mean age is 5 - 6 years higher than those given by lane - claypon ( 1926 ) and wainwright ( 1931 ) , due to the fact that the two latter series include only cases coming to hospital for operation , whereas the b.e.c.c. 
the youngest patient in the series was aged 15 , and survived 5 years after enucleation of a tumour of 3 years ' standing , which proved on histological examination to be an early adenocarcinoma . 
expected actual per cent of expected possible x - rays alone or with interstitial radium . number of cases of known duration mean number of months lived j in 5 years from onset maximum  . 
expected lactual possible per cent of expected x - rays with local surgery . number of cases of known duration mean number of months lived in 5 years from onset maximum  . 
it was found that patients in stage iv who were not treated either by surgery or radiotherapy had a 5 - year expectation of life of 46 - 7 per cent of normal , which was not improved by palliative x - ray treatment . all these figures must be considered in the light of the fact that the mean duration of the disease is 38.3 months ( major greenwood , 1926 ) , so that these patients whose mean age was 57 years would have a 5 - year expectation of life of about 56 months ; a 5 - year follow - up is therefore insufficient for assessment of the results of treatment . 
the variations in mean age of the patients submitted to various types of treatment is shown below , and indicates that the more radical methods were used in the younger patients . radiotherapy mean age of 703 patients treated by radical mastectomy alone mean age of 133 patients treated by local mastectomy alone radiotherapy mean age of 174 patients treated by radium alone or with local surgery h.v. 
fodden. from the department of pathology , university of liverpool , and the liverpool cancer control organization . received for publication august 20 , 1948 . in his ' textbook of pathological anatomy ' rokitansky ( 1861 ) made his classical statement that pyloric cancer was exactly bounded by the pyloric ring , and that the growth never reached beyond into the duodenufrom this time it appears that the majority of observers , with the early exception of brinton ( 1864 ) , commented upon the integrity of the duodenum in cases of carcinoma of the stomach . 
many well - known surgical teachers spoke of the habitual immunity of the duodenum from invasion . kocher ( 1893 ) , mikulicz ( 1898 ) and most ( 1899 ) believed it to be always constant . kocher ventured that it was a problem of extreme interest to consider why gastric carcinoma grows in almost all cases towards the cardia , yet stops , on the contrary , at the duodenopyloric junction . it was brinton who first took especial exception to this proposition of rokitansky . 
meredith. from the christie hospital and holt radiumt institute , manhester . received for publication december 12 , 1948 . ix a series of papers ( dale , 1940 ; dale , meredith and tweedie , 1943 ) it has been shown that the action of x - rays on aqueous solutions of biologically active compounds was indirect , i.e. 
further , it has been shown that in consequence of this indirect action , if two solutes are present , the second solute ( the protector ) reduces the radiation effect on the first one ( the indicator ) ( dale , 1942 ; 1943 ) , by sharing the intermediate product formed from water by the radiation . 
meredith enon revealed certain unexpected quantitative relationships between the protective power of a substance and its concentration , which will be described and discussed in this paper , together with the closely linked ionic yield of the indicators used , the knowledge of which is the necessary basis for the quantitative treatment of the experimental results . 
the fact that these new results were derived from experiments with two indicators of very different molecular weight , for an extended range of protective substances added to both indicators , helps to build up a more complete picture than has been obtained hitherto . 
 ( average a 130xu ) from a 250 kv tube . whenever possible , the solutions , contained in pyrex glass tubes , were spaced at such distances from the target that each received the desired dose during the same overall treatment time , care being taken to avoid shielding of one tube by another . this ensures that the relative doses received by different tubes are not affected by unavoidable fluctuations in the tube output . 
the stock solution of enzyme and the solutions of protective substances were made up with water , glass re - distilled from alkaline potassium permanganate , and the ph adjusted so that a sample reacted pink to phenolphthalein . all necessary dilutions were carried out with glass re - distilled water adjusted to the same ph by the addition of 1 ml . 
were performed during this series of experiments , these arise because very high and some special difficulties were encountered . doses of radiation ( one to two million roentgens ) are required to achieve a reasonable degree of inactivation in solutions with concentrations of the order there is a strong tendenvcy of re - crystallization during of 10 per cent or more . the long exposure to radiation , which makes it almost impossible to keep the enzyme in solution at a ph compatible with its stability . however , it was found that a 6 per cent solution could be maintained for most of the time by stepwise addition of naoh . 
the concentration reached by this method was derived from the known concentration of the suspension by measuring the height of the coluimn of crystals after , and the height of the suspension before centrifugation . 
compound ( warburg and christian , 1938 )  . since various preparations ofthe specific protein of the amino acid oxidase differ in their activity , and even any one preparation gradually loses activity when kept for some weeks , the oxygen uptake with a known amount of d.n. 
1. these results may also be presented , as shown in a previous paper ( dale , gray and meredith , 1949 ) , by the formula : d5 - 2 x 107  . 
calculated by lea ( 1946 ) from earlier experiments by one of us is much lower than the value obtained in the horizontal part of the curve , and this is due to the fact that the concentration then used was of the order of ~~~i ~~~~~~~ii conc . 
for the sake of accuracy the degree of inactivation should be kept between the limits of 25 - 75 per cent . in a previous report ( dale , 1947 ) the value of q was found from the protection afforded by generally lo100 g . 
q was roughly constant , and it was concluded that the protective power per molecule is proportional to the molecular weight - perhaps not a surprising result , since all these substances have roughly the same average composition . it is only when low molecular weight substances of special chemical configuration are examined that remarkable differences are found . oxalic acid , which was earlier ( dale , 1942 ) found to be a poor protector of d.n. , also proved to be a poor protector in the case of c.p. , but if the c - c bond in oxalic acid is broken and the free valency of the carboxylic group linked to an h atom , thus forming formic acid , the protective power is raised about 200 times , and similarly , if w . 
our arguments , however , are not dependent upon its correctness , nor would they be invalidated by its disproof . lea , smith , holmes and markham ( 1944 ) pointed out that , in addition to reacting with solute molecules , radicals may also recombine with one another , having a mean life , as free radicals , of r sees . 
 ( 1944 ) also suggested a modification of equation ( 3 ) to cover the protection effect on the assumption that the indicator and protector molecules " share " the available radicals . 
thus although the protector molecule has removed a radical from the solution , it can " hand on " the effect of the radical to the indicator molecule , and thus fails to fulfil its since we have no clue to the nature of this change function as a protector . we will call it " activation , " and it might be thought of as a sort of meta - stable state . 
and the collision frequency between " activated " protector molecules and indicator molecules , 1 , m and pi have already been defined , whilst pa is the probability that a collision between a radical and a protector molecule destroys the former and activates the latter . 
ps is the probability of an indicator molecule being inactivated in a collision with an " activated " protector molecule . from equations ( 9 ) and ( 4 ) we findao + m rt [ ( ao + t ) pi ( ao + m ) pap . 
i ~~ ( ao + t ) p , + lp , apz~l ( 10 ) some of the constants appearing in equation ( 10 ) can be evaluated from results obtained with solutions of the indicator alone , whilst the others can be evaluated from any two experimental values of q for known protector concentrations . 
the values of ( p ) are indications of the protective power per molecule of each substance for the particular indicator , and the values given show the same tendency as was shown previously for protective power per unit weight by molecules with approximately the same atomic constitution have dale ( 1947 )  . approximately equal protective powers , whilst marked differences occur when special groupings are present . from the results it is also possible to calculate the relative values of pr for d.n. 
kerrich from the radiation therapy department , johannesburg general hospital , and the department of mathematics , u niversity of the witwatersrand . received for publication april 20 , 1951 . in a previous paper the writer ( cohen , 1949 ) proposed a biological dosage unit , the " roentgen equivalent clinical " ( rec ) based on an empirical formula d = e.a.tn.l - q , relating the physical dose in roentgens ( d ) to the biological dose in rec ( e ) , taking into account the relative biological efficiency of radiation of various qualities ( a ) , the over - all time in days ( t ) , and the field size in decimetres ( l )  . 
the physical and biological doses could be equated when the specific ion - density is minimal ( a = 1 ) , the treatment is completed in 1 day ( t = 1 ) , and the field diameter is 1 d ( l = 1 )  . 
cohen in diametercan the hypothesis of a " diffusible substance " ( grynkraut and sitkowski , 1936 ; jolles , 1950 ) , for diminishing the treated field by a given factor , or increasing the time interval by the same factor , would allow the same proportion of the " substance " to diffuse across the surface bounding the treated volume . 
the difference between the 220 kv and 180 kv ranges is statistically significant ( p 0 - 01 ) , but of minor importance clinically , so that for practical purposes the two high - voltage qualities may be grouped together taking a as 0 - 7 . 
2 illustrates the variation in biological efficacy with halfvalue layer , and shows the agreement between our estimates and similar data derived in a different manner by maccomb and quimby ( 1937 ) and by mackee and cipollaro ( 1940 )  . each point represents the median erythema dose ( a x 1000 ) estimated from table ii , the vertical lines delimit the 95 per cent confidence range , and the lettering refers to data by the authors quoted . in comparing these results with other published data , it is necessary to note inevitable differences in the definition of the erythema dose . 
from the method we have used the standard erythema dose is that which , delivered to a 10 cm . field in one sitting , produces a " moderate " erythema in 50 per cent of the treated cases . 
with the same dose , however , some slight reddening would be visible in considerably more than half ( probably 90 per cent ) of the treated cases . since this type of " barely perceptible reaction " is a convenient and objective end - point much favoured in erythema studies , there is obviously need for care in comparing such results . it is also necessary to distinguish the transient reddening ( fruiherythems ) appearing within 24 hours of the delivery of quite small doses ( helmke , 1949 ) from the main reaction ( haupterythems ) , which reaches its maximum about three weeks after treatment . for example , the threshold erythema dose ( ted ) is defined ( maccomb and quimby , 1937 ) as that quantity of radiation giving a faint reddening of the skin , visible in two to four weeks , in 80 per cent of treated cases . it would , therefore , differ little from our standard erythema ; hence the fair agreement between our results and the threshold erythema data in fig . 
the customary five - year - cure policy could not be applied since estimates of depth - doses from treatment records prior to 1945 are not sufficiently accurate it was decided instead to use , as a standard criterion , freedom for our purpose . from perceptible recrudescence for not less than three years . the records of 100 suitable cases treated between 1946 and 1948 , and followed with periodic examinations through 1950 , were abstracted and the data collected in table iii . the cases are arranged in order of increasing biological dosage ( rec )  . the dosage data shown are the true mimimum tumour doses , and differed , especially with superficial therapy , from the nominally given doses . in the case of very superficial tumours treated with lightly filtered radiation the significant point was taken to be 5 mbelow the edge of the treated field . with 2 ma1 filter this point receives about 85 per cent of the given dose ; and with the chaoul apparatus , only 67 per cent . with deeper growths treated at higher voltages , standard depth - dose tables were used to assess the tumour dose ; while with radium applicators and implants dosage was calculated on the paterson - parker system . since various qualities of radiation were used , it was necessary to correct the dosage by a factor ( rbe ) which , taking that for y - rays as unity , becomes 0.5 for superficial therapy , and0.7 for the 200 kv range ( tableii )  . in the case of deep - seated tumours treated with 200 kv radiation , the half - value layer ( and hence the rbe ) in the tissues differs from that of the incident beam on account of the increase in the average wave - length brought about by the compton recoil process . this effect is the more marked the harder the incident radiation . 
3 each 188 case site . face orbit neck node larynx back tongue pharynx neck nosoe alveolus neck face scalp larynx tongue , base pharynx orbit face temple post - cricoid  . 
0.5 , dose * ( r )  . 3200 2300 2250 3300 3150 2000 3800 3500 3000 1400 2000 3000 3150 3000 3300 4400 3600 5000 3750 2250 3300  . 
4 illustrates a method for determining the recovery exponent various values of n ranging from zero to 0.5 were ( n ) by a graphical solution . selected , and the resultant estimates of biological dose tabulated in a manner field diameter ( cm . ) therapeutic ratio skin tolerance dose 5000 median cancerocidal dose 4500 time days 1204 a% t% % - iuuut 9000 8000 - 7000 - 6000 - 5000 4000 - 3000 - 2000 1j4mi iolvv 40003500300025002000fig . 
a single line and volume factors . across the diagram gives all the relevant factors simultaneously . similar to table iii but regrouped accordingly . the cure rates so obtained were similarly charted in lognormal probability graphs , and the values of the standard deviation factor ( f ) corresponding to each value of n was determined . it is seen that f is a minimum as n approximates 0 - 25 . 
by means of the method of least squares , estimates of a and n for six different qualities of radiation were obtained , and shown to be in good agreement with previously established data . 
the uncertainty factor in dosage estimated on this basis ranged from 1.21 to 1 - 35 . a further 100 cases of epidermoid cancer were similarly analysed in order to determine the dependence of curability on the biological dose . 
the median lethal dose for this tumour ( 3000 rec ) and its uncertainty factor ( 1.3 ) were determined , and it was shown that , under optimal conditions of time and area , 95 per cent of tumours could be cured with a dose exceeding the median lethal dose by it has also been demonstrated that the prognosis is a mathematical 30 per cent . function of the therapeutic ratio . the author wishes to acknowledge the valuable advice given by j . 
kerrich. from the data in table iii cohen suggests that biological dose = dose / rbe x tn , or x = z / tn say , where xbiological dose , zdose / rbe , t = time in days . 
he goes on to show that if x is the exact dose necessary to effect a cure , then a reasonable assumption is that log x = log z n log t is normally distributed . writing x = log x , z = log z , t = log t this hypothesis becomes x = z nt is normally distributed with , say , mean oc and variance a2 . by a neat graphical method he proceeds to estimate ac , n and a . 
cohen the sizes of the estimated standard deviations show that none of the constants can claim to be very " well determined . " it must , however , be remembered that we are not dealing with a planned experiment , but that the author had to use the data that were to hand . 
as a suggestion to future workers in this field , more observations for small values of t ( say t 0 ) and large values of t ( say t - 1.5 ) would help greatly in fixing c and n more accurately . in more detail , the estimated covariance matrix is var . 
sylvin. fromn the department of radio - pathology , radiumnhemmet , stockholmi , swveden . received for publicationi february 11 , 1947 . our defective knowledge of the biological factors responsible for infiltrative growth is partly due to lack of sufficient information on the biology of the stroma connective tissue in malignant tumours . thus , growing carcinoma vegetations induce different complicated reactions on the part of the surrounding connective tissue , e.g. 
fibroblast proliferation and various inflammatory reactions . in the course of the stroma investigations by the writer , special attention has been paid to the transformation ( " dedifferentiation " ) of the connective tissue preceding the actual infiltration by cancer cells and to the simultaneous appearance of high molecular ester sulphates of unknown composition ( sylvan , 1938 , 1941 , 1945 and unpublished data . ) interpretation of the events taking place in the stroma is rendered almost impossible by the multiplicity of intermingling reactions . 
on this account it was decided to treat each problem separately . consequently , i thought it advisable to study these changes in cartilage , a tissue characterized by very slow reparative and reactive capacities . thus , the actual question was to investigate the morphology and the histochemical changes of normal cartilage when infiltrated by carcinoma cells . 
 - in this way comnparisons could be made with the stroma reactions of the different tissues , and with the alterations in the chondroitin - sulphate of cartilage and the unknown stroma ' ester sulphate mentioned above . 
by selecting suitable cases it was felt that the source of error caused by the connective tissue stroma reaction accompanying cancer vegetations growing from outside the perichondrium , could be avoided . for the sake of brevity , the readers are referred to current literature regarding the normal morphology of cartilage ( maximow and bloom , 1938 )  . 
the resulting newly formed , growing , connective tissue would then " penetrate " into the ground substance of cartilage , which was " dissolved " and replaced by the tissue mentioned above . after this , the cancer cells were believed to grow into this connective tissue , thereby seemingly infiltrating the cartilaginous tissue proper . ribbert emphatically denied that cancer cells ever could infiltrate cartilage directly , the process instead being mediated by connective tissue . 
as to the operating forces ribbert stated that "  . epithelien ( cancerous ) haben nicht die fdhigkeit anders als durch den wachstumsdruck auf ihn ( cartilage ) einzuwirken . " such a restricted mechanical interpretation involving pressure for the explanation of infiltrative growth , is nowadays of little value ( sylv6n , 1945 )  . oestreich ( 1910 ) suggested that the chemical composition of cartilage , mainly the chondroitin - sulphate , would be injurious to the cancer cells and consequently infiltrative growth would become impeded by this substance . since ribbert 's review in 1911 no special articles have been published regarding these questions . 
the statements of ribbert demand a survey of the cooperating factors active in the destruction of cartilage by carcinomatous tumours . the following possible factors have to be considered : 1 . 
the cancer cells might by direct action be destructive . in order to obtain a satisfactory understanding of the morphological factors unfortunately , they should be interpreted in terms of biochemical principles . for lack of complete data the chemical principles can only be touched upon . cartilage has a strongly acid intercellular matrix , due to the presence of large amounts of chondroitin - sulphuric acid . this substance is very sensitive to even slight changes in ph towards the alkaline side ( blix and snellman , 1945 )  . such ph variations cause a rapid depolymerization and disintegration of the long chain molecule . 
a shift in ph resulting in a disappearance of chondroitin - sulphate has recently been suggested to occur in inflammatory lesions of cartilage ( sylven , in press )  . 
when considering the complexity of the problem , i have to admit that no final conclusions regarding the biochemical nature of the operating factors can be drawn from the material presented here . 
some results , however , seem to be conclusive . some information concerning the mutual relationship between cancer cells and the perichondral connective tissue in the absence of any intervening inflammatory stroma reaction was obtained from case 2 , ii . 
the carcinoma strands in question were growing in the perichondrium , which was transformed into a loose metachromatic stroma connective tissue similar to the one met with in most carcinomas ( sylven , 1938 , 1945 and unpublished data . ) in the superficial part of the underlying cartilage a moderate decrease in the content of chondroitin - sulphate was demonstrated , the cartilage in other respects apparently being normal . 
sylvien actual cartilage destruction was seen to be effected either by the sole inflammatory stroma reaction ( case 1 ) or by the combined stroma and cancer strands ( case 2 )  . in the cases under consideration , that part of cartilage just being infiltrated was always devoid of the typical ester sulphate . remains of this substance might be found in the shape of thin pericellular halos . 
1. - the early changes in ear cartilage , previous to the actual infiltration , are demonstrated . at top of picture the perichondral connective tissue is swollen and slightly invaded by lympho - plasmocytes . the superficial part of cartilage appears unstained , indicating that metachromatic material is lacking . 
4. - the disappearance of chondroitin - sulphate precedes the growing tumour . in this picture the stroma reaction has reached the left top corner ; the lightly stained ametachromatic cartilage area contains very few inflammatory cells . 
when investigating the process more carefully , however , it was established that cancer cells really have the capacity of digesting cartilage by their own activities without any co - operating stroma reaction . further , the results indicate , that the first demonstrable alteration of cartilage just being infiltrated is an early disappearance of most of the preexisting ester sulphate . 
the cultures were grown by the hanging - drop technique in a medium consisting of equal parts of fowl plasma and 15 per cent chick embryo extract in ty - rode solution . 
the explants were subcultured every 48 hours for 4 passages to obtain as uniform growth as possible . fresh embryo extract was groups of cultures , each from the 4th passage , were selected and matched used . and used for experimental material and controls . 
agent were observed on the unfixed living cells in culture by cine - photomicrography . for most of the work we used apparatus modified from that described by willmer ( 1933 )  . recently , in collaboration with a . 
hughes of the department of anatomy , we have recorded the effects on the living cells by phase - contrast cine ' - photomicrography , using the techniques described by hugbes ( 1949 , 1952 )  . phase contrast microscopy has been used in a few cases to observe directly the effects of the chemicals on the living cells in culture . ( ii ) radiological details . the primary x - radiation used was of equivalent wave - length 0 - 221k , as deduced from the h.v.l. 
the nominal dose rate , which was always measured within + 2 per cent was in the reaion of 2oor per minute at distance 40 cfrom the focus , and was varied by altering the distance . 
the quality of the radiation was unchainged throughout these experiments , so that the probleof the exact value of the ionisation in the cells of the culture near the surface of the glass coverslip is not of importance here . in the cultures used most of the mitotic cells coudted lie between the glass surface and a distance 201i from it , so that the ionisation in the cells is increased by photo - electrons arising in the glass , probably by a factor in the region of 2 ( spiers , 1949 )  . 
3 , 4 , 5 . - effect of tetra - sodiuni 2 - mothyl - 1 : 4 - naphthohydroquinone cliphosphate ( compound i ) on a living resting cell of a chick fibroblast culture of the fourth passage , 24 hours old . phase - contrast c ' me ' - photomicrographs , taken by a . 
the doses were given in a fixed time , 2 - 00 minutes , except in the case of tlle three points marked , for which the radiation was delivered at 200 r per minute . the mitotic inhibition in probits is plotted against log dos - , ( finney , 1947 ; fisher and yates , 1948 ) there is no indication of departure from a linear relatiodbetween mitotic inhibition in probits and log dose . it is concluded that the relation between iiiitotic inhibition and the radiation dose plotted on a logarithmic scale is a sigmoid curve . 
the dose corresponding to 50 per cent mitot - ic inhibition after 6 hours is 315 the calculated regressiod line gives a sa - tisfactory fit . the calculation of the regression line is somewhat laborious . the mitotic inhibition produced by compound i in the chick fibroblast cultures has been studied in some detail after 24 hours ' application . 
the calculated regression line gives a satisfactory fit . there is no indication of departure from a linear relation between mitotic inhibition in probits and the logarithm of the concentration . thus there is a sigmoid relation between mitotic inhibition and the applied confor 50 per cent mitotic inhibition after 24 hours the concentration centration . of i is 3 - 81 0.15 x 10 - 6molar . for most of the compounds studied such accuracy is not necessary . tt is justifiable to deduce the approximate concentration required to give 50 per cent mitotic inhibition from the curve fitted by eye to relate the observed percentage mitotic inhibition to the molar concentration plotted on a log scale . in the case of compound i this method gave a value of 3 - 84 x 10 - 6m . the first experiments on the antimitotic effects of x - rays and i in chick fibroblast cultures ( mitcher and simon - reuss ' 1947 ) showed much greater mitotic inhibition with the combination of 3 x 10 - 6mcompound and 244 r of x - radiation delivered 18 hours later with fixation and counting after a further period of 6 hours , than with the same amounts of the two agents separately . to test for potentiation rigorously , it is essential to compare the effect of a combination of half amounts ( or other suitable mixtures ) of the two agents with the mean effect of the agents acting independently . this method , which may be termed the summation , method , is well recognised in pharmacology , and has already been applied in radiobiology by liechti and muller ( 1936 ) , gray and read ( 1944 ) , and mitchell ( 1947 )  . our original experiments showed a combined effect of 86 - 7 per cent mitotic inhibition , while the corresponding mean ' calculated for the two agents separately from the regression lines in fig . 
i and 2 , is 78 - 6 per cent . this result suggests that there is at least additivity of the effects , but it does not provide evidence for potentiation . in other experiments , the combined effect of 2 x 10 - 6mcompound followed 310 j . 
the combination of 2 x 10 - 6mcompound followed after 18 hours by 200 r of x - radiation produced 93 - 25 per cent mitotic inhibition after 24 hours . froni the number of mitoses in the individual cultures it is found that for 8 degrees of freedom student 's t is 15 - 71 , so that p is much less thlan - 001 . in this experiment , as in table 1 , the highest values of the mitotic inhibition were associated with no significant reduction of the area of the outgrowth . this finding confirms the unimportance of cell migration under the experimental conditions of the combined action of x - rays and the compound 1 . the possibility of differences in the behaviour of the outgrowth and of the central part of the culture has been , studied by means of the counts made in serial sections of 24 - hour cu - itures . 
 - the method is a laborious one ; by its use , fischer and parker ( 1929 . ) showed that in chick periosteal fibroblasts , the proportion of cells in mitosis was 0 - 79 per cent in the outgrowth , but only about 0 - 09 in our cultures - as in those of jacoby ( 19371 ) - the per ceiit in the central part . mitoses in the central part are limited to the " perichondxium " on its surfaces . studies of the topographical distribution of mitoses in our cultures by a . 
f. phillips showed no appreciable decrease in the number of cells in mitosis per unit the area of the central part is usually area as the central part is approached . not more than 20 per cent of the total area of the culture . in the serial sections of the cultures the central part is easily defined . 
the resting and mitotic cells were counted in the surface layers . in the sections of a control culture , out of 6205 cells counted there were 53 cells in mitosis , of which 13 were in prophase , 31 in metaphase , 3 in anaphase and 6 in telophase . 
at 24 hours after the application of 5 x 10 - 6mcompound 1 , out of 6220 ceus counted , there were 26 cells in mitosis ; of these i was in prophase , 19 were in metaphase , none were in anaphase and 6 were in telophase . 
simon - re ] utss cytological effects . tlio cytological changes produced by compound i in the chick fibi - oblast perhaps the most cultures differ in some ways from those produced by x - rays . fundamental difference is that anaphase bridges are only rarely produced by ' the compound , unlike x - rays . after the application of compound i to the hving cers , the first change observed is temporary cell enlargement , presumably due at least in part to hydration ( " cell oedema " )  . this does not occur with 5 x 10 - 7mconcentration , but has been observed in its early stages at 2 minutes after application of the compound in concentration 5 x 10 - 6m . 
the change is obvious after 5 minutes and probably affects the cytoplasm first . after 10 minutes the effects are still increasing ; ' there is bubbling of the enlarged cytoplasm and enlargement of the mitochondria , nucleus and nucloolus . 
the slight transient shrinkage of the cell immediately after addit - ion of the compound is observed consistently . at the maximum of the cell enlargemei - it the increase in transverse dimensions of the cells is often in the region of 50 per ' cent . mitotic inhibition is obvious after 80 minutes and persists after 24 and 36 counts show that there is no appreciable change in the distribution of hours . the phases of mitosis even in high concentrations such as 5 x 10 5m where mitotic inhibition is almost complete . example at 4 x 10 - 6mconcentration the abnormal mitoses increased slowly from about 5 per cent of the total mitotic count after 80 minutes to about 15 per cent after 24 hours . 
a typical count of the mitotic abnormalities is included in table il and photomicrographs of examples of the abnormal cells after fixation are enlargement of some of the dividing cells is shown in fig . 
2 x 10 - 6m  . compound i followed after 18 hr . by 150 r x - radiation * also 1 tripolar met - aphase . i and x - radiation shows potentiation of chromosome fragmentation . this finding is of particular interest in connection with possible radiotherapeutic applications . instability of compound i in solution . studies of the thermal instability of compound i in aqueous solution were made because of erratic results in animal experiments and clinical trials . 
for 7 days almost completely destroys the antimitotic activity and produces a rather toxic - solution . there is no significant mitotic inhibition , but the outgrowth is poor , many of the resting cells are vacuolated , disconnected and rounded and - a large number of the cells in metaphase show gross chromosome clumpiaig . there is progressive reduction of the mitotic ' hibition + 4 - 1 314 s . 
the outgrowth ig poor , many of the resting cells are rounded , there is some accumulation in metaphase and a number of exploded cells ; there is wide it seems likely that there are variation in the behaviour of different cultures . several unstable intermediate products involved in the process of inactivation of compound i by incubation at 39 ' c . 
experiments. tetra - sodium 2 - methyl - 1 : 4 - naphthohydroquinone diphosphate ( compound 1 ) it is found that there is no has been studied in detail as a reference substance . indication of departure from a linear relation be - tween mitotic inhibition in probits accordingly it is sugand the logarithm of the concentration of the compound . gested that the best estimate of the activity of the compound is the concentration which produces 50 per cent mitotic inhibition under the experimental conditions . this concentration may be termed mi 50 as a convenient abbreviation . 
for compound 1 , there is no indication of departure from a linear relation between the rnitotic inhibition in probits and the logarithm of the concentration . for 50 per cent mitotic inhibition after 24 hours , the concentration is 3 - 81 0 . 
legon. from the department of geography , the london school of economics and political science . received for publication april 20 , 1951 . in considering the heavy mortalities from gastric cancer that exist in the counties of northern and western wales ( stocks , 1936 ) , the writer wondered whether mortality was uniform over the area , or whether there were marked local variations within it . 
the low - mortality rural districts of eastern montgomery and of radnor ( 70 deaths ) are well drained , in contrast to the rural districts to the west , which lie on an ill - drained plateau with extensive tracts of bog . 
the impermeability of the rocks of anglesey ( 203 deaths ) , and the extreme flatness of much of the island , make for peat accumulation , despite the fact that rainfall is light compared with that of the highland parts of north wales . case involving the pennant grit . it may be stated , therefore , that the rural districts of low mortality are all on the sheltered east and south of the welsh massif and are well drained . 
legon huntingdon , ely , peterborough and the holland division of lincoln ( stocks , 1947 ) , since these four counties alone in england have proportionally large areas of peaty fen soils . apart from the typically high organic content of their soils , north wales and the fens have little in common . 
as further information ( marston , 1951 ) is made available , it may prove worth while to consider whether a carcinogenic substance exists in food - plants grown on these soils . the possibility of an association between soil organic matter and cancer mortality was expressed verbally to the author by g . 
daily with their diet ( bielschowsky , in experiment ii the ordinary stock diet ( hall , 1948 ) was 1944 ) for 25 weeks . given and the carcinogens , dissolved in peanut oil , were administered by stomachtube . 
the survivors of experiment i were killed in the 63rd and those of experiment ii in the 52nd week of the experinment . table i summarizes the results of experiment i . for comparison the tumours obtained by feeding 4 mg . 
the first tumour , a hepatoma , was examination . foumd in the 54th week , and the second , a cancer of the meatus acousticus externus , 3 weeks later . 
by the 24th week neoplasms of the breast gland were present also in cancers of the meatus acousticus externus made their the two other groups . appearance in rats treated with the methyl compounds from the 34th week palonwards , whereas in the a.a.f. 
group the first was seen in the 25th week . pable liver tumours , lowever , occurred only in the latter group after the 33rd week of the experiment . these consisted of a few minute cysts . the total yield of cancers induced by d.a. 
induced two hepatomas , definite signs of liver damage and fairly widespread cystic cholangiomata in 2 other males of this group , while 2 of the females showed a few minute cysts in the liver . 
four hepatomas were found in the males and one in the females , cystic cholangiomata being present in all . to summarize , the genetic background determined to a large degree the site of tumour development . 
thus breast tumours appeared in a much higher incidence in the wistar rats than in the piebalds , in which cancers of the small nevertheless in both strains a striking difference intestine were readily induced . in the response of the liver to the three compounds was apparent . in the first experiment 700 mg . 
were given , while in the second the total dose administered amounted to about half of the methyl compounds and to approximately a quarter in the case of a.a.f. yet in both experiments a.a.f. 
is readily split off in vivo and therefore can be only of minor importance for the carcinogenic activity has been substantiated by weisburger , weisburger and morris ( 1950 ) , who showed that after feeding w_ - c14 - 2 - acetylaminofluorene radioactivity appeared in the breath within 6 hours . ray and argus ( 1951 ) found the toluene - sulphonic ester of 2 - aminofluorene to be non - carcinogenic for the rat , only minute amounts of this ester being morris , dubnik , dunn and johnson ( 1947 ) , studying hydrolysed in the body . the action of 2 - nitro , 2 - amino , mono - acetyl and diacetyl - 2 - aminofluorene , reported that the acetyl compounds induced the majority of liver tumours observed , when the substances were given per os . why the acetylated aminofluorenes have such an affinity for the liver , whereas m.a. 
ungar. from the department of pathology , hadassah university hospital , jerusalem , israel . received for publication june 7 , 1949 . carcinoma of the duodenum has been observed in this laboratory at autopsy in three young siblings whose case reports form the subject of this paper . 
the examination revealed several histological aspects which may be regarded as representative of successive stages in the development of polyps . in the area of the prominence , the submucosa was widened and the muscularis mucosae showed a funnel - shaped protrusion in the direction of the intestinal lumen . 
the earlier history contained no fourteen months prior to admission he first began these occurred at irregular contributory information . to complain of bouts of cramp in the abdomen . intervals and were without clear localization . the patient was admitted to the hospital in june , 1939 , three months before his death . 
at admission his chief complaints were shortness of breath , attacks of tachycardia , lack of appetite and abdominal colic localized under the costal arch on either side . during the preceding year the patient had lost a great deal of weight . there were recurrent periods of diarrhoea . 
the duodenal mucosa choledochus as far as 1 cbehind the papilla of vater was without lesions . and pancreatic duct without abnormalities . beyond the papilla of vater , the lumen was considerably distended . there was a nearly circular , crateriform defect , which extended from the posterior wall , the lesion , which including almost the entire circumference of the duodenum . measured 7 to 8 cin diameter , showed a rugged floor ; it was entirely composed of tumour tissue and blended underneath with enlarged lymphatic glands of the peripancreatic group . 
the latter were glued together and had been sections through the floor of the ulceration completely replaced by tumour . revealed a firm and , in some places , a friable tissue which was of a pale greyishyellowish colour . 
the tumour was defined against the head of the pancreas by a thin layer of greyish - red connective tissue . the remaining portion of the duodenum was considerably distended and filled with greenish fluid . 
sections from the large ulcerated tumour revealed a carcinoma which grew in some areas in solid strands , while in others gland - like formations predominated . epithelia showed a considerable degree of pleomorphism and there were numerous typical and atypical mitotic figures . 
the main mass of the node was made up of glandular epithelium tissue with regular lumina which in places were slightly tortuous . was columnar with dark nuclei and oxyphilic cytoplasm . there was no pleomorphism or mitotic activity . 
an x - ray examination of the stomach and duodenum 2 months following the operation likewise failed to reveal pathologic changes . the three younger boys were kept under observation from birth by the infant welfare centres and the school hygiene departments of the hadassah medical organisation . 
nagel ( 1925 ) benign polyposis . duodenal polyp , polyposis recti et colon duodenum , jejunum , ileum duodenum , stomach , colon , duodenum , stomach , caerectum cum , colon adenomas in duodenum , multiple polyps in cae . cum , colon , rectum duodenum , jejunum , colon polyps in duodenum and jejunum duodenum , jejunum 9 . 
the disease is hereditary and affects patients since generalized polyposis is known to of all age groups , including the lowest . involve predominantly the large intestine , it is not infrequently mentioned in textbooks and articles under the name " polyposis or adenomatosis of the colon . " however , in rare cases , the disease was found to be prevalent in the small intestine . besides the instances mentioned in table iii , others of this variant have been described by lubarsch in 1888 ( dohring 1907 ) , schwytzer ( 1924 ) , roan ( 1932 ) , haggard and floyd ( 1935 ) , ravitch ( 1948 )  . some pathologists have taken the view that generalized polyposis is an entity which since it causes characteristic severe dysentery - like symptoms and malignant change in a high percentage of cases , should be separated from that represented by cases in which only few polyps are formed ( oberndoerfer , 1929 ; lockhart - mummery , 1934 ; hullsiek , 1928 )  . 
the designation of all three of our cases as generalized polyposis therefore seems to be justified . the observations reported in this article are relevant to the understanding of factors which govern the manifestation of malignancy in intestinal polyposis . several authors have assumed a casual relationship between the appearance of polyps and carcinoma in any given case . 
gunz. * from the department of radiotherapeutics , university of cambridqe . received for publication june 11 , 1949 . in previous publications ( gunz , 1948a ; b ) a technique of cultivating human leukaemic leucocytes in vitro was described , and the quantitative and cytological findings in untreated cultures made by it were analysed . 
jung. from the cancer research laboratory , university of florida , gainesville , florida . received for publication march 21 , 1951 . the experimental investigation of gastric cancer is seriously impeded by our present inability readily to produce this condition in animals . 
the difficulty and uncertainty of this method have progress in this field would be greatly facilitated if a precluded its general use . chemical compound capable of producing gastric cancer were discovered . that a carcinogen with such specificity is possible may be implied from the frequency with which butter yerow , for example , produces hepatomas ( kinosita , 1940 ) and beta - napthylamine , bladder tumors ( wiley , 1938 )  . 
when this is done it very seldom results in malignant growth in the stomach because of the protective if the carcinogen could be 8ecreted by the stomach it would action of the mucus . be in a much more favourable position to initiate cancer . the first step towards a solution of the problem is to ascertain just what properties of a substance influence its secretion by the glands of the stomach . the optimum properties might then be conferred on - a carcinogen by judicious substitution in the molecule . 
the resulting compound could be expected to initiate neoplastic growth in the stomach . several groups of workers during the past twenty - five years have studied , by means of gastric pouches in dogs , the secretion of intravenously injected dyes . dawson and ivy ( 1925 ) , kobayashi ( 1926 ) , ingraham and visscher ( 1935 ) , and varco and visseher ( 1941 ) , although working under varied conditions , are geneof some sixty dyes rally in agreement as to the dyes secreted by the stomach . studied ( ingraham and visscher , 1935 ) , afl those secreted are electropositive ( basic ) under some conditions . 
on the other hand , dyes not secreted by the gastric glands are acid or amphoteric with the possible exception of four basic triphenylmethane dyes . the basicity of these dyes seems to be the property most likely to determine their degree of gastric secretion . 
at a pkbof 11 - 3 , for instance , this equation yields a concentration ratio of 51 , at a pkb of 7 - 5 a ratio of 2 - 8 x 101 . ratios actuary obtained were 1 - 3 and 26 - 4 . although experimental results indicate a definite tendency for secretion to increase with increasing basicity . 
it is obvious that there is some opposing factor . this opposing factor increases with increasing basicity , so that at pkbof about 6 - 0 the tendency for the basic dve to concentrate in the stomach , due to distribution differences , might be completely overcome . this opposition to gastric secretion of dyes of increasing basicity is nicely explained in terms of the pore theory , or the concept of the ositively charged membrane ( ingraham and visscher , 1935 )  . acid dyes would be retained by chemical combination . basic dyes are assumed to pass through this membrane in the undissociated foras the ionization constants of these dyes increase it would become increasingly more difficult for them to pass through a positively charged membrane . it appears , therefore , that we are dealing with two main effects in the gastric secretion of dyes . 
bartholomew 's hospital , london , e.c.1. received for publication february 11 , 1952 . radium and thorium are widely distributed throughout the earth 's crust , although , as yet , no large deposits have been found ( it has been estimated that uranium and thorium exist in as much as 4 and 12 parts per million respectively )  . both these materials decay through a radioactive series , and in each case one ' these two radioactive gases escape into the member of the series is gaseous . atmosphere where their respective decay products will be formed and these prothere are other sources ducts will probably attach themselves to dust particles . of naturally occurring radioactive material ( actinium , which decays to gaseous actinon ; potassium ; rubidium and carbon 14 ) , but these are insignificant compared to members of the radium and thorium series . the presence of radioactive material in the atmosphere was first observed by their observations were confirmed by other workers elster and geitel ( 1901 )  . most of these early determinations were made by in various parts of the world . the charged wire method , which gave quite good qualitative results . 
the rate of air flow depended on the length of tubing connecting the pump and filter - holder , but was always between 30 and 35 litres a minute . it was measured by a u - tube manometer , and controlled by a screw clip . 
the collecting time was 20 minutes , which does not necessarily give the maximum measurable activity , but allows the experiment to be completed in an hour . the efficiency of the filter was examined in a series of experiments in which one , two or three filter - papers of different types were used in series as a backing for the whatman no . 
as it was not possible to obtain standard samples of each member of the radium and thorium series , we determined the efficiency of the counter for measuring the ft particles from three radioactive these efficiencies were plotted against energy , and the efficiency for the isotopes . , f emitting members of the radium and thorium series were read from this graph . the efficiency of the counter for measuring a particles cannot be determined in the same way as for f8 particles ; since an unknown number of a particles will be absorbed in the filter - paper . in order to calculate the ac efficiency , a dust sample was taken and counted in the usual way ; a piece of aluminium foil ( thick enough to absorb all the ac particles ) was then inserted between the filter - paper and the geiger counter , and the count was continued . this experiment was the proportion of ac to ft particles emitted by repeated for a series of samples . the dust was deduced theoretically , and the proportion of a particles which were counted was determined from the drop in counting rate caused by interposing the aluminium foil . 
dawson the data for kew were taken unless there was a significant difference between these two sites , in which case that day was ignored or mean values were taken . 
dawson than those taken in the morning . rothamsted is a third - order station of the meteorological office and more accurate correlation of weather phenomena and activity were possible ; the conclusions drawn from the hospital results were confirmed . the activity was greater if the ground was dry or drying . 
the floor of the cellar was only 4 below street level ; there was some ventilation from a window and the door leading to the main part of the house . 
the cellar had not been used for several in order to avoid disturbing the dust , the pump and filter - holder were weeks . kept outside the cellar ( table iii )  . 
the proportion of radon atoms that will decay whilst passing through the filter - paper is negligible , but when one considers the very large absorptive capacity of carbon for radon , it is rather surprising that no radon was found . we have not investigated the proportion of the other members of the radioactive series that will adhere to dust particles . carmichael and tunniciffe ( 1948 ) removed the dust from a closed room by fanning the air across a greasy plate and noted the diminution of activity in an air sample . 
on introducing smoke there was an immediate increase in activity , showing that in a small room there is never an appreciable quantity of free radioactive atoms - they either become attached to dust or migrate to the walls . 
shelter tolerance ( maximum concentration ) 11 , 800 100 , 000 the figure for droitwich spa was taken from a brochure issued by the local council . our inquiries as to who made the original measurements were not very successful , but it is believed that they were made by professor h . 
schrodinger , at seeham ; 8 - 9 x 10 - 12 curie / metre3 of air . simpsoin ( 1905 ) made a very exacting survey of the air - borne radioactive material in lapland in 1904 , using the charged wire method ( table vi )  . 
read and mottram ( 1939 ) have published the results of some determinations of the radon concentration in the radium laboratories at mount vernon hospital , at the radium institute , and in the radium workshops of messrs . 
 ( all in or near london )  . in the last case a concentration of 22 x 10 - 7 curie / metre3 of air was observed . evans ( 1950 ) has calculated the dose received by joachimstal ( jachymov ) miners in a working day through inhaling radon . 
bartholomew 's hospital , in the city of london ; rothamsted , a semi - rural area , thirty miles from london ; chiswick , geographically in middlesex but actually a semi - industrial part of london ; and in the centre of manchester . 
the results were similar to those of other observers in different parts ofthe world ( table v )  . large day - to - day variations in activity were observed , but these can be explained by variations in the weather - the more stationary the air , the greater the concentration of active material . 
the slight differences between the four sites mentioned above may be seasonal . the experimental procedure was not sufficiently accurate to show whether thoron or its decay products were present . radon , absorbed on dust particles , was not detected . 
no variation with height up to 100 above ground level was observed . the results obtained in rooms with varying degrees of ventilation are of in the laboratory there was usually twice the activity found at the interest . open - air site on the roof . 
at chiswick , ventilating the room lowered the activity by as much as one - half , whilst in the coal - cellar the activity was 14 times greater than at the site in the garden . in the post office air - raid shelter the ventilation was as restricted as any found in habitable buildings ; the activity was 120 times as high as at the open - air control site , i.e. , nearly one - eighth the tolerance concentration of radon . in every case the large day - to - day variations were similar to those at the control site . these large amounts are due to the greater emanating area in a room ( compared with the open air ) from which the parent radon can escape , and to the restricted ventilation which will allow the radon concentration to build up . 
the amounts show no considerable difference between urban and rural districts , but there are large day - to - day variations which in situations out of doors are affected chiefly by the wind ; the more stationary the air , the greater in closed places , e.g. , an air - raid shelter underground , the amount the activity . may be 100 or more times greater than those in the street outside , but even these are small in comparison with the lowest amounts considered harmful to man . i wish to thank professor j . 
fisk , of the general post office , london , for their kindness in providing facilities for this investigation , which has been supported by grants from the medical research council , the british empire cancer cami wish to express my indebtedness to t . 
usually the ventral prostates were explanted ; they were grown by the watch - glass technique , which is eminently suitable for organized gro - wth ( fell and robinson , 1930 )  . 
the medium was placed in a small watch - glass and allowed to clot ; the watch - glass rested on a layer of sterile cotton - wool soaked with sterile distilled water inside a small petri dish . 
but later this method was improved by explanting one lobe of each gland into medium containing methylcholanthrene while the other was kept as control . the explants were placed well flattened out on th ' e surface of the plasma clot , where they became firmly anchored . after a day or two the growing explants liquefied part of the plasma clot , and while still firmly attached to the surfa - ce of the clot were surrounded by a pool of liquefied mediuthe cultures were after the ninth day no transferred to fresh medium every second or third day . more methy1cholanthrene was added , and the cultures were maintained in normal medium for the rest of the culture period . the used glass - ware was decontaminated by keepino , it in concentrated sulphuric acid at room temperature for at least one week . 
the glands were fixed in 2 per cent acetic zenker after the following periods of growth : 5 days , io days , 14 days and 21 days . five to nine experimental and an equal number of control cultures were used for each point of observation . 
they were embedded in paraffin and seriary sectioned ; the sections were stained with ehrlich 's haematoxylin and eosin . to assess mitosis the number of dividing cells was counted in every second section , i.e. , in at least 20 sections of all single - lobe cultures . 
cultures treated with 20 - methylcholanthrene . cultures treated with methylcbolanthrene show a similar tvpe of growth at the beginning of the culture period : formation of new alveoh at the periphery and some central degeneration . 
the epithehum retains its glandular character and remains actively secreting in the treated explants for a longer time , but the stroma is usually verv poor and reduced in botb . 
one out of fi - ve treated cultures shows squamous metaplasia after the higher mitosis is stfll ' above that in the controls and has , in fact , risen after the dose . higher concentration while it has dropped after the lower . table ii gives th - e number of mitotic cells counted in 20 sections of controls and cultures treated for 9 days with 2 , y / cic . 
the number of dividing cells has fallen and nearly reached the control level . at the same time changes of a more anaplastic type can be observed in one batch of cultures treated with 2y of methylcholanthrene . 
squamous metaplasia develops more fully , particularly after the smaller dose , after the end of treatment . it is noteworthy that the d - ownward bend of the first wave coincides with the end of treatment . this may mean that the first peak is caused by a direct stimulating action of the carcinogen , whfle the second one is due to the increased growth - potential of the changed epitheliua rise in cell division has been reported by cooper and reller ( 1942 ) , who found a ten - fold increase hi the mitotic rate in the skin of mouse ears painted with methylcholanthrene , and by glucksmann ( 1945 ) , who observed a rise in mitosis a few hours after a single painting with benzpyrene . in contrast to the increase in mitosis and proliferation of the epithelial cells is the reduction of the stroma of the treated explants . 
of methylcholanthrene , which indicates that the dose for stimulation of fibroblasts is roughly twenty times lower than that for epithelium if the concentrations of 2 - 4y / / c.c. 
the cultures were grown in the presence of the agent for 9 days , then transferred to a normal medium and fixed at intervals after removal of the carcinogen . in both control and experimental cultures new alveoli were usually formed at the periphery of the explanted glands , while in the centre some of the al - veoli underwent degeneration . in the control cultures the epithelium quickly lost its glandular character , and the alveoli developed wide lumina lined by one layer of low epithelium in which mitosis was present though infrequent . 
of methylcholanthrene , the alveolar epithelium retained its glandular character for a longer time and showed a marked increase in mitosis , leading to hyperplasia and squamous metaplasia , while the stroma was considerably reduced in contrast to that of the controls . the first changes were recognizable 5 days after the beginning of treatment . they became more pronounced as the treatment continued and persisted after removal of the carcinogen . in the later stages partial or complete occlusion of the alveolar lumen with squamous metaplasia were observed . the rise in mitosis showed two distinct peaks , the downward bend of the first wave coinciding with the removal of the c ' arcinogen . 
fell for suggesting this problem and for her criticism in the preparation of the manuscript . i also wish to thank a . howard , radiotherapeutic research unit , hammersmith hospital , ' london , for the generous supply of cx males , c . 
we are probably all agreed that tumours , although usually , or perhaps always , preceded by abnormal local . this change consists in - an increase in conditions , arise by a sudden change . the rate of growth of a cell or a group of cells . in this way there arises a new cell - lineage distinct from its antecedents , and one which can propagate its new it has the character of a genetic property irreversibly and even indefinitelv . secondary changes may follow establishing subchange , a somatic mutation . sidiary cell - lineages , - some involving further increases of growth - rate and dedifferentiation , and all surviving and multiplying subject to natural selection . to these secondary changes i shall return later . the chemical conditions arising - in the changed tissue h4ve been examined bv santesson and caspersson ( 1942 ) , while the processes of its cell division have been described by koller ( 1947a ) for epithelial tumours and by la cour ( 1944 ) for pernicious anaemia , which is an analogous condition depending on the enhanced multiplication of the red blood precursor cells of the bone marrow . 
a single polymitotic gene in maize and extra heterochromatic chromosomes in millet both cause rapid and unwanted nuclear divisi ' ons in the pollen grain . in maize up to fou - r extra mitoses take place before the chromosomes have had time to divide immediately after meiosis . 
the nucleus is forced into division , and the unsplit chromosomes are scattered on a spindle which merely disperses them into a number of deficient nuclei , each of which is aga ' m compelled to divide before it is ready , and in this way the whole pollen grain is brought to ruin . in millet the mitoses ( also up to the nu ' mber of four ) do not occur before the chromosomes are split , but the whole pollen grain is none the i - ess consumed and killed in the end by the production of redundant nuclei . 
the pollen grain is thus , in , a sense , an encapsulated tumour ( darlington , 1947 )  . comparison of these cases of polymitosis in plants with animal tumours polyinitosis is not due to a somatic enables us to clear our minds on one point . it 4ffects every cell of a mutation . particular type in the body . 
the spontaneous tumour on the other hand arises at random both in time and space . it does not affect all cells of one type , but only one cell , nor is it the first cell of a particular normal type to arise which is affected . 
we are therefore confirmed in regarding the spontaneous tumour as due to a genetic change . this conclusion removes the contradiction between development on one side and heredity and infection on the other by withdrawing to a lower level ofanalysis . the organism is now seen from the cell point of view as a vegetatively propagating colony . 
how far does it enable us to distinguish between nucleus and cytoplasm as the seat of the mutation general the most efficient carcmogens ( such as the hydrocarbons ) and the most efficient agents of nuclear mutation ( such as mustard gas ) do not coincide . ' carcinogens do not damage the nucleus in proportion to their effect as carcinogens ( darlington and koller , 1947 )  . 
thus the nucleus again seems to beexcluded , just as it is by the direct evidence . but the evidence of xray effects is a more serious objection to a nuclear origin . x - ray damage leads to the development of cancer only when the dose has been so heavy as to damage the cytoplasm , and only then after prolonged delay . light doses which have a proportionate effect on the breakage of the chromosomes and the mutation of the 120 c . 
different conditions , in differeni tissues and in different stages of development . now plasmagenes , like all other such determinants , are susceptible to mutation . it is not possible certain of them control the formation of plastids in plant cells . to relate here ( as i have elsewhere ) the long detectiv - e story of investigations which have led in the course of 40 years to the revelation of the character and continuity of the plastid plasmagene . suffice it to say that , like the centromere and nucleolar organizer of the chromosomes , it its stock - in - trade on its back , which being a sac of green pigment marks or tags its owner and enables us to count its numbers in the cell and note its changes : it can mutate from green to white and vice versa , so that cells can occur with mixed green and white plasmagenes ; and , moreover , the same plastid may be starved white , as it were , by a stepmother nucleus , and recover its normal colour when it is put back with its own proper parent . prolonged coitus causes a paramecium to be infected by the kappa plasmagene of its mate . transplantation of an organ or of serum from a c02 - sensitive drosophila infects a nonsensitive fly , including its egg , with the sensitive plasmagene ( sonneborn , 1948 ; l ' he ' ritier ; 1948 )  . these infections , it will be seen , are artific ' ial , or at least unnatural . 
a number of aberrant conditions can be trans ' mitted from stock to scioii , and some even have arisen in a scion after it has been grafted on a healthy stock . these are artificial diseases ; they are not transmitted in nature , but only by grafting . 
we make a great mistake therefore in calling them viruses : they are proviruses ( darlington and mather , 1949 )  . conversely it has been know - n for 40 years that the . 
virus ricketmia is carried by the eggs of its vector dermatocentor . the terror of its infection for man has closed our eyes to the fact of its inheritance for the tick . 
what appears as a virus in one host is indistinguishable from a plasmagene in the other - and it may weh be that the plasmagene is the older ( l ' he ' ritier , 1948 )  . at the same time billingham and medawar ( 1948 ) have sh ' own that a selfpropagating particle.differentiated in development may by its diffusibility enjoy certain of the properties of infection - a situation which can come to our notice only when the particle is as innocuous , and the differentiation as trivial , as the black pigmentproducer of a ' piebald mammal . 
they have never been guilty of infection , and are therefore totally unadapted for or against it . the virus type may well have arisen likewise by mutation of a plasmagene , but it must have been a mutation followed by others adapting it to infection . moreover , this type falls into two groups by a most instructive distinction . 
the milk - agent , on the other hand , cannot be imagined as having arisen anywhere save in the moiise , itself , in whieb it is inherited by the milk instead of by the eggs . how accidental is the distinction between the infectious and the non - iilfectious particle is revealed most strikingly by one true virus . 
but in its new host it not only it even ceases to be inoculable . it loses the property ceases to be infectious ; of infection , and becomes transferable , if at all , only in whole cells . this is just the opposite transformation to the one by which proviruses arise or demonstrate their existence when two plants are grafted together . 
ob ection8and di ffil cultie8 . three grounds for suspicion of the plasmagene origin of cancer are now worth first , the cancer agents have one characteristic which will at once discussing . be noticed as marking ' them off from all previous plasmagenes . 
now the inheritance of lethal mutations out of the running . in the nucleus , when they are recessive in their lethality , is mendelian and can therefore be followed in experiment . 
a whole tissue can be destroyed by rendering its there is , however , no contradiction between nuclei unworkable in this way . the nucleus is the assumptions of a cytoplasmic cause and a nuclear cure . that is especially easy the only wheel in the cell that we can put a spoke in . to do in rapidly dividing cells ( darlington and la cour , 1945 )  . 
we are therefore merely attacking the malignant cell where it is weakest . incidentally the effect of irradiation in breaking the chromosomes and stopping the growth of the cells leaves no doubt that the remarkable deficient nuclei found in tumours by koller ( 1947b ) will have a limited life . 
the particle analysis : competitive propagation . the cancer miita - tion , as we saw , is often followed by other changes beyond these may be described under the the primafly one of change in growth rate . headings of dedifferentiation or the loss of tissue character , metastasis or migration , secondary mutation and various breakdowns of mitosis and of chromosome structure . 
what we now have to ask ourselves is how far these secondary changes require secondarv assumptions , and how far they are implied by the primary on.e. recent experiments equally with flies , infusoria and tomatoes liave revealed to us the conditions of normal development . 
thev have shown that it is iiot merely ebaracterized by adjusted between nucleus and cytoplasm , but between different self - propagating constithese adjustments can be broken down under experituents of the cytoplasm . in polymental conditions , with results which have ' been ace - lirately described . mitotic maize , as we saw , the cytoplasm runs away from the nucleus : in polyin paramecium , in mitotic millet the nucleus runs away from the cytoplasm . c02 - sensitive drosophila , and in rogue tomatoes , the whole system at a high temperature can be made to run away from a particular plasmagene . 
bv rapid growth the 250 kappa particles of one cell can be run down to one ( from which they can recover ) and then finally to zero ( from which thev cannot recover ) , so that the cell lineage has mutated . 
and in most virus diseases of course the virus runs away from the rest of the system or vice versa ; only occasionally is equievidently therefore the cell contains self - propagating elements librium reached . these limits are exposed in with different limits to their speeds of reproduction . a protozoan or a plant when the temperature is raised . 
these three classes of particle are conditional and interchangeable . cancerproducing particles fall into all three . the origin of cancer can therefore be ascribed to mutations in cytoplasmic determinants , indifferently infectious or non - infectious , which make themselves visible by causing the resumption of growth . further , the study of plasmagene and virus inheritance in relation to differentiation reveals a competitive propagation of cytoplasmic particles . this explains both the genetic control and the secondary development of cancer with its potential dedifferentiation and metastasis . the discovery of , not the cause , but the system of causation of cancer tells us nothing immediately about the cure that we do not already know . 
althougih biologists have for long been uneasily aware of the existence of a problem of cell heredity , its systematic analysis is the work of very recent cell heredity deals with the origin and maintenance of inherited character years . differences between cells ; more particularly , between cells that set up division its problems present themselves in their most acute , lineages by mitotic fission . if not most easily workable , form in metazoan development . the outcome of cellular differentiation in ( say ) mammalian development is the formation of a limited number of histologically definable cell genera , each one further subdivided into a variety of cellular genetic species . 
the genus " fibroblast , " as yet far from completely analysed , may be subdivided into cells which manufacture bone , cartilage , white connective - tissue fibres , and so on . genus " epidermis , " of which we have made a particular study ; includes the epidermal epithelium of the superficial skin , of the sole of the foot , the tongue , cells of each of these epidermal the claws or nails , the vagina and the cornea . species display a distinctive combination of structural or physiological properties . the epidermis of the sole of the foot , for example , has a characteristically high rate of cell division . 
but this has proved not to be the case . although plausible " phenocopies " of sole epithelium ( in the form of corns and callosities ) can be made by irritating the thin and relatively quiescent skin of the body surface , the difference between the division rates of sole and body epidermis is in fact " intrinsic " and inheritable . 
we have , for example , transplanted sole epidermis to positions in the body where it is protected by neighbouring hair and secure from mechanical irritation ; but even so , its characteristic growth rate has been maintained for at least two years , and thick pads of now functionless cuticle continue to form over it and may periodically be removed . claw epithelium tells the same story - more clearly , since the difference between claw and body epidermis is anatomically crude and obvious . 
hopkin and williams , who supplied the following information : " it is a distillers ' yeast , composed of one race of yeast only . it is not debittered , because it is not bitter in the first instance . the desiccated yeast is active and can be killed by temperabefore use the yeast was heated to6 60 c . 
bielschowsky table ii gives the results of an experiment ( f ) which has been chosen because it is typical of the response of wistar rats receiving 2 - acetyl - amino - fluorene and the original diet . 
two rats dying at an early date ( rats 3 and 6 , experiment b ) had to be omitted from the table . of the 28 rats left , 22 were still alive at the end of the 42nd week ; they seemed to be in excellent health and no tumours could be palpated ; 14 of these were females and 8 males . however , neoplasms were found in 11 at the post - mortem examination . the commonest tumours were small hepatomas , having a diameter of 3 - 6 mm . ; in one wistar rat a small flat intraductal papilloma of the breast was discovered . histological examination of these early neoplasms frequently failed to give proof of their malignancy . 
bielschowsky this difference was best seen when the average weights of fed the yeast diet . only such animals were the females of the piebald strain were compared . selected as were found to be free of hepatomas . 
any effects observed in the yeast series have , therefore , primarily to be attributed to the substitution of milk powder by dried yeast . experiment e is in good agreement with harris 's findings that an increase in milk proteins there exists now failed to protect against the action of 2 - acetyl - amino - fluorene . good evidence that a high casein - high riboflavin diet protects only against dimethyl - amino - azo - benzene . 
even related compounds ( giese , clayton , miller and baumann , 1946 ) are not inhibited to the same extent by such a diet . further , strong and figge ( 1946 ) , who reviewed the literature on this subject , did not succeed in inhibiting by a diet of liver supplemented by a combination of raw milk , riboflavin and xanthine the development of tumours induced by subharris 's failure to protect against cutaneous injection of methylcholanthrene . acetyl - amino - fluorene by a diet which inhibited the action of " butter yellow " has already been mentioned . the results obtained in the yeast experiment are not impressive , but they seem significant since the same trend of delayed tumour growth was found in three experiments involving various litters of two different strains of rats . it would probably have been an advantage to use a smaller dose of the carcinogen in the experiments reported in this paper . 
of acetyl - aminofluorene will still produce a high percentage of cancers . it seems possible that the relatively low incidence of cancers observed by cantarow , paschkis , stasney and rothenberg ( 1946 ) after prolonged treatment of rats with acetyl - amino - fluorene was partly due to a supplement of brewers ' yeast in the diet given . the problem whether certain dietary factors are true anti - carcinogens , or protect only the liver against a damage the reaction to which leads to the establishment of cancers , could not be answered by workers who studied the effect of it was hoped that working diet in rats receiving dimethyl - amino - azo - benzene . with a more versatile carcinogen would give a clue to this question . at first sight it seems that in experiments a , b and c the development of all types of there was , for instance , a significant reduction in the tumours was delayed . incidence of mammary cancers in females of the wistar strain . this finding , however , could be explained also by the assumption that a less damaged liver was better able to cope with an excess of endogenous oestrogen and so prevented the ' development of tumours of the breast . 
the frankly keratinizing members of our series we have taken as a standard with which to compare the behaviour of our remaining histological types . the morphological features of the more differentiated epitheliomata have been so completely evaluated that any further discussion would be superfluous . 
the primary lesion grows slowly and tends to be clinically latent for a considerable period of time , it appears as a especially if it is situated in a region such as the nasopharynx . smooth or finely granular , firm , globular tumour , at first a mere nodule , but later attaining considerable dimensions . infiltrative spread and superficial ulceration occur fairly late in the evolution of the growth . cervical lymph glandular metastases appear at an early date , while the final phase is frequently ushered in by distant visceral extension , osseous deposits being rather characteristic ( kienbock and selka , 1935 ; ch ' in and szutu , 1940 )  . 
the histological picture may be syncytia of large , palely staining cells appear as sheets , irregular quite typical . clumps , or columns , in a lymphocytic stroma of varying density . 
ewing was doubtful of the specificity of schmincke 's description , and found its distinction from other types of undifferentiated pharyngeal growth difficult or impossible . the term " transitional cell carcinoma " was first employed by quick and cutler ( 1927 ) to describe a group of highly radiosensitive buccopharyngeal tumours of uncertain histogenesis which lacked the classical features of epithelioma , but presented transitional epithelial characters . ewing 's writings ( 1929 , 1940 ) have done much to clarify the morphological features of this growth . the most frequently encountered sites are the tonsil , base of tongue , nasopharynx , laryngopharynx , nasal cavity , and accessory nasal sinuses . quick and cutler described the primary lesion as possessing " a finely granular , velvety surface , e . 
fairburn this description is , however , far from being specific . which looks like an erosion of the mucous membrane rather than a frank ulceragives the impression of having originated in the tion . 
the lesion deeper structures and adhered to and eroded the mucous membrane from the clinical beneath . " course resembles that of lympho - epithelioma - a small and often occult primary histologically , transitional focus , and early cervical lymph glandular metastasis . cell cancer is typified by the presence of broad , clearly demarcated , epithelial the cells are cylindrical , polygonal or spindlecolumns and alveolar formations . shaped , with a rather hazy cytoplasmic membrane . 
the oval or fusiform nucleus is more chromatic than that of lympho - epithelioma , while its nucleolus is less frequently the marginal cells appear regimented as though forming distinct . degeneration and necrosis of the central zones of some of the a basal layer . lymphocytic infiltration of the stroma epithelial formations may be observed . may be present , but is never marked . there is considerable divergence of opinion regarding the justification of the classification of lympho - epithelioma and transitional cell carcinoma as specific entities . 
each has been traced to death or for a minimum period of five years following the first examination . purposes of classification we have created the following groups according to the site of the primary lesion : 3 . 
the cells are distributed the cell body is spheroidal or polygonal in solid masses or diffuse infiltrations . in form with palely staining cytoplasm , and a relatively large , oval , hyperchromatic nucleus which frequently shows bizarre , atypical features and mitotic figures . these classifications have presented certain difficulties : 1 . 
compared with the figure for the frankly keratinizing group ( 61.5 years ) , the former two differences are statistically significant , while the latter is not . there is no significant difference between the mean ages of - our cases when distributed according to the site of the primary growth . 
fairburn we have adopted ebenius ' clinical criteria of metastasis . the frankly keratinizing cancers possess a statistically significant lower incidence of metastasis ( 36 per cent ) than the remainder of their fellows , with the exception of the undifferentiated group which only metastasized in 22 per cent of cases . this table also illustrates the influence of glandular metastasis upon the likelihood of death with active growth . 
frank , lev and blahd ( 1941 ) , in their study of transitional cell growths , report a 44 per cent incidence of metastasis . 52 per cent of our cases possessed evidence of glandular extension on first examination . inspection of our data discloses the relative insignificance of tumour histology as a prognostic factor in cases of cancer of the lympho - epithelial sites . 
maccarty ( 1922 ) and plaut ( 1927 ) have emphasized its limitations , stressing the far greater importance , in most instances , of clinical features , such as the age and general condition of the patient , the duration , location , and gross anatomy of the growth , and the presence , or absence , of metastasis . 
the enormous preponderance of the site factor over that of histology is borne out by this study . thus , frankly keratinizing neoplasms of the lip carry a relatively good prognosis , but when arising in a lympho - epithelial region their significance is as sinister as that of their ill - differentiated fellows . 
the presence of lymph - node metastasis on first examination is , in our experience , a factor of far greater prognostic value than tumour histology , although very appreciably influenced by the site of the parent growth and its accessibility to treatment . 
to take a specific example , metastasis in a case of lip cancer markedly decreases the likelihood of cure , whereas when a lympho - epithelial region is involved , death with active malignancy is likely to occur whether the cervical nodes are involved or not . the chance of invasion of the cervical lymph glands appears to be largely independent of the histological grouping , the site of origin of the tumour being of infinitely greater significance . it has been widely assumed that the main factor in dissemination is the inherent growth capacity of the neoplasbut this is not the only influence which has to be considered . 
 two recent investigations , both from the united states , upon the arsenic content of tobacco , and the volatilization of this arsenic when tobacco is smoked , have been reported . 
the work of these authors differs from our own in that they used artificial methods of combusting the tobacco , which may or may not repro duce the conditions present when smoking is carried out in the ordinary way , and they found no brands of tobacco containing only minimal quantities of arsenic . 
 ( 1 ) gross and nelson ( 1934 ) employed a method which consisted of digestion in nitric and sulphuric acids , precipitation of magnesium ammonium arsenate , solution in hydrochloric acid , and estimation by the gutzeit method . 
five such analytical groups were analysed for each brand studied . " they found the content of pooled groups of 4 cigarettes of 5 brands to range from 97 to 363 p.p. 
 ( 2 ) thomas and collier ( 1945 ) , using a modified cassil - wichmann method , found that " individual cigarettes and cigars of a given brand varied widely in arsenic content , " which ranged in pools of 2 to 4 cigarettes from 2 packs of 20 ( presumably of the same brand ) from 354 to 114 p.p.m. , while cigars ( 132 to 295 ) and pipe tobaccos ( 227 to 428 ) showed a lower range ( table i )  . 
gross and nelson ( 1934 ) attribute the rather narrower range found in cigarettes and in pipe tobacco , compared with cigars , to the mixing which the former receive , but this difference is not seen in the results for cigarettes and cigars of thom.as and collier ( 1945 )  . 
in american pipe and chewing tobaccos ; using suction by a water - pump , he concluded that " we can say roughly that half of the arsenic is evolved in the smoke gross and nelson ( 1934 ) used an apparatus drawing about 50 ml . 
 each : 207to256 211 , , 267 ' 253 , , 363 97 , , 130 229 , , 261 range in 5 single cigars from each of 5 brands : 229 241 332 116 247 83 to 484 range in 5samples from each of 4 brands : 260 to 500 116 to 266 311 to 451 1 - 5 1 - 4 thomas and collier : cigarettes " a single pack of 20 " " ali.other pack " 1 - 4 " groups of 2 to 4 . " 354 ; 400 ; 405 ; 472 ; 600 ; 61 - 4 * 614 ; 670 ; 714 ; 845 ; 1140 132 ; 225 ; 262 ; 295 cigars pipe tobacco cigars ( about 10%cutoffat ends ) pipe tobacco 1 - 5 396 ; 265 ; 227 ; 345 ; 428 * these figures represent the actual analyses in p.p.m. , on pooled groups of 2 to 4 cigarettes , and hence are not calculated means , though each figure represents the mean composition of the eigarettes in one pool . 
cigars and cigarettes were " smoked down to about 1 / 2 to 3 / 4 " ; the arsenic the " puffed " and " unpuffed " smoke was absorbed and estimated separately . 
 " the pipe smoker who smokes all the tobacco does not therefore have the protection afforded by the butts of cigars and cigarettes . " from the present point of view this question is not of great interest ; the important datum is the amount of arsenic inhaled , and in this country only about one smoker in ten smokes a pipe ( hansard , 1945 )  . 
in their first series ( table ii ) cigarettes of 7 c length were smoked down to 1 c ; in a later serjes only 2 / 3 was burned . 
 the arsenic found was compared with analyses of whole cigarettes from the same pack , " but in view of the large differences they later cut off about os c for analysis ; apparently they failed to discover that this method also can be falla cious . 
 our earlier results ( table iv ) were obtained by the gutzeit method , which depends upon the brown and yellow colours produced in paper impregnated with hgc12 ; it is fitted for the measurement of amounts of as20 3 between 10 and 1 g . , and shows differences most clearly in the range of 8 to 3 g . 
there may be con~ siderable differences in the matches made by different persons ; in these experi ments the mean was taken of the readings made independently by two persons unaware of the nature of the unknowns . 
the iodometric method of thomas and collier ( 1945 ) was adopted later ( tables iii , v and vi ) in view of the difficulty of determining the small amounts of arsenic lost in smoking . 
the method has the advantage that , whatever may be its errors in other respects , there is less disagreement over the very sharp end - point ( titration of iodine and starch ) , about which two observers usually do not differ by more than 005 c.c. 
 the estimations upon brands p and c were usually carried out upon amounts of 20 to 30 g . , as a method which is sufficiently accurate within this range 176 m . 
gross ( 1933 ) has drawn attention to the occurrence of such errors in the estimation of arsenic in tobacco , which are attributed to uncombusted residues of pyridine and nicotine ; we failed to obtain satisfactory results by the method which he devised to overcome this difficulty . 
 in the previous investigations summarized above artificial methods of smoking were employed , air being drawn through a pipe , cigar or cigarette by means of a water - pump . 
we have confined our experiments wholly to cigarettes smoked by one or other of three persons accustomed to this form of smoking , and they were asked to do this in their ordinary way ; the two brands used ( p and c ) are in common use in this country . 
the ash , and stump , were dropped into separate weighing bottles in our earlier experiments , but latterly the two have been analysed together ; the amount of arsenic found , if less than that in the cigarette , should indicate the amount volatilized in the smoke , of which a part must have been inspired . 
 before this width of range was realized we obtained many contradictory results , showing amounts in the ash and stump which were sometimes less , and sometimes more , than that thought to be present originally . 
 8 whole cigarettes 9 cigarettes ( 7 wholes and 2 halves ) 5 pieces from 3 cigarettes 1 piece from each of 4 cigarettes 6 successive pieces cut from 1 cigarette 13 estimations on mixed tobacco of 10 cigarettes e 10 range in 5 packages of brand p brand o . 
 678 823 307 496 461 275 10 pieces from 5 cigarettes 5 successive pieces cut from 1 cigarette a 20 a 20 11_ estimations on mixed tobacco of io cigarettes . 
but as the weight of most cigarettes does not differ very much from one gram the figures give a rough measure of the arsenic in one cigarette , which is of more obvious practical interest . 
the results were again contradictory , and we found that such suc cessive portions may show a range of 388 to 587 , or 100 : 151 in p , and of 306 to 542 , or 100 : 177 in c ( table iv )  . 
 in the hope of obtaining more uniform material , the papers were removed from the cigarettes of a package of 10 or 20 , and the tobacco mixed by hand and 178 m . 
but even this treatment does not give satisfactory results ; it is very difficult to take up samples of such material which will contain constant propor tions of the coarser and finer particles , as the latter tend to fall away from the . 
moreovar , the minced tobacco , even when moistened , is not easy to smoke in the same way as ordinary tobacco : adjacent cigarettes of brand p from a much larger package , containing 100 , were taken ; but these at first showed a wide range ( 495 to 766 , table iv )  . 
 that an average of 158 per cent of the arsenic is lost in the process of smoking and had presumably been volatilized ; this loss is statistically significant ( p = 0001 )  . 
the same method was applied to brand c , of which the largest boxes available contained 50 ; the first two rows showed in 18 cigarettes a loss of only 76 per cent , which was not statistically significant ( p = 02 )  . 
 580 527 623 558 603 418 456 458 568 556 617 } 681 mean 596 631 427 412 471 533 629 662 453 367 527 634 455 367 539 509 lower right row . 
kennaway the 4th row showed a loss of 182 per cent , which is just significant ( p = 005 ) , in spite of the small numbers ( 12 cigarettes ) involved . 
 the most likely source of the arsenic present in some tobaccos , which has been suggested by several authors , is the spraying of the adult plants with insecticides , and this particulate method of application would explain the difficulty in obtaining concordant analyses . 
 of the arsenic volatilized in smoking , a part must escape while the cigarette is not in the smoker 's mouth , and a part of what he inspires is expired again , hence the amount retained is no doubt very small . 
the concentration of arsenic in cigarettes containing the larger amounts is very \rariable ; this irregularity is perhaps due to a method by which the arsenic may have been introduced , namely , by the spraying of the plants with insecticides . 
an estimate was made of the amount of arsenic volatilized in smoking , by comparing the content of cigarettes , and of the ash and stumps derived from them , but the wide range of arsenic content makes it difficult to infer the amount present originally in a cigarette which is to be smoked . 
the results indicated that from 76 to 18 2 per cent of the arsenic present was lost in smoking ; this figure is of the same order as but somewhat lower than that obtained by some previous investigators who have used artificial methods of smoking . 
korteweg. victorieplein 45 , amskrdam , neturlands . received for publication february 12 , 1951 . most curves indicating the cancer death rates per million living in the different age - groups rise continuously with advancing age . 
the numbers of lung cancer deaths in the netherlands and in england and wales , 1125 and 5941 respectively , were large enough to exclude the possibility that these exceptions to the rule might be caused by chance only . is this decrease of the cancer death rate at a relatively early age a characteristic of lung cancer or is there some other explanation ? cia l%22 r . 
2 , which is derived from table l the age curves for males in all yeargroups given show the same early decline of the lung cancer death rate , with the .2 ^ ^ ^ 35 - 44 45 - 54 55 - 64 65 - 74 75 + years fig . 
3 , constructed from the numbers following one another vertically , show us , for each age - group separately , the increasing lung cancer mortahty in the course of years . 
3 we can derive , by interpolation , for each year and each age - group separately the approximate values of the cancer death rates . this has been done for the years 1915 , 1925 and 1935 . 
4 it is necessary to take the following points into consideration : cancer only develops after a long period of preparation , which in most cases can be counted in decades . those who at the age of 80 contract cancer , do so partly because of a tendency to cancer years before - let us say at the age of 70 . 
they are recruited from the group of the younger ones , whose tendency to cancer is also known , as it is given by the length of the ordinate belonging to that age in fig . 
4. it would be wrong , therefore , to compare in this respect persons who in ' 1945 were 80 years of age with persons surely this comparison should be who , in the same year , were 70 years of age . made with those who , ten years earlier , in 1935 , belonged to that age - group . 
we must presume , therefore , that it is not only the younger people who are endangered by these irritative factors . third : let us suppose that all males were exposed to these irritative factors to about the same degree , and that in each of the last 40 years the quantity of these factors had increased considerably . 
were this so , then really we would expect to find an " age curve " for lung cancer approximately such as we did if one fact proves the reality of the great increase of lung cancer in the find . last 40 years , it is the sbape of its " age curve , " now demoilstrated as being an illusion only . artificiary , with older age , the lung cancer age curve is pushed down . at this moment , the increase of lung cancer in the younger age - groups came to a halt , even then it would - progress in the older age - gr6ups up tir the moment when theillusionary age curve changed into the real one . 
we can ' ut it in another way : at this moment the lung cancer mortalitv is lower than corresponds mr - ith the tota - i amount of the causative irritative factors . the lung cancer " ceifing is lying at a far higher level than the mortality figures would suggest . up to the age - group 55 to 64 inclusive the shape of - the illusionarv age curve is about normal ; it is only after that , that the sharp dechne begins . in 1945 , in england and wales , in males less than 65 years of age , the number of deaths from lung cancer was 33 - 8 per cent of those from " all cancers with the exclusion of lung - cancer " ( registrar - general , 1947 )  . 
6 this also means that in this case the total number of cancer deaths in males would have ' been 30 , 835 + 10422 = 41 , 257 , and not 36 , 776 , which was the number given in the statistical review for 1945 ( registrar - general , 1947 )  . following the same reasoning it appears that in 1949 , in the netherlands , for males this " ceiling " was lying at a level of 1.710 , whereas the lung cancer deaths registered numbered 1125 only . it is clear that the " ceiling " will never be reached except after a long period of rest , with stationary lung cancer death rates in the younger age - groups . 
6. - balance of lung cancer mortality in males , england dnd wales , 1945 : - _ rears ..1 - - lung cancer deaths recorded deficit lung cancer risk lung cancer age curve after correction . ..... 
pseudo lung cancer age curve . 5941 4481 10 , 422 after having studied this table we no longer wonder that in england and wales . cancer in males is again on the increase . 
and still , if in 1948 the " ceiling " of lung cancer had been reached , the total number of cancer deaths would not have been 40 , 026 , but more than 46 , 000 ! in females lung cancer is also increasing . 
an analysis of its age curve , such as i have made in this paper for lung cancer in males , shows us that , just as formales , the real age curve for females closely resembles that for the " non - hormonal cancers " ( cancers other than those of breast and uterus ) in females . the problem which lung cancer presents to us is a very serious one , not only for england and wales , but also for the netherlands and many other countries . * in the review for 1948 ( registrar - general , 1950 ) the numbers for lung cancer are only given in combination with those for cancer of the mediastinum . during the last 40 years cancer of the mediastinum has not changed much in frequency . 
hopkin and williams , who supplied the following information : " it is a distillers ' yeast , composed of one race of yeast only . it is not debittered , because it is not bitter in the first instance . the desiccated yeast is active and can be killed by temperabefore use the yeast was heated to6 60 c . 
bielschowsky table ii gives the results of an experiment ( f ) which has been chosen because it is typical of the response of wistar rats receiving 2 - acetyl - amino - fluorene and the original diet . 
two rats dying at an early date ( rats 3 and 6 , experiment b ) had to be omitted from the table . of the 28 rats left , 22 were still alive at the end of the 42nd week ; they seemed to be in excellent health and no tumours could be palpated ; 14 of these were females and 8 males . however , neoplasms were found in 11 at the post - mortem examination . the commonest tumours were small hepatomas , having a diameter of 3 - 6 mm . ; in one wistar rat a small flat intraductal papilloma of the breast was discovered . histological examination of these early neoplasms frequently failed to give proof of their malignancy . 
bielschowsky this difference was best seen when the average weights of fed the yeast diet . only such animals were the females of the piebald strain were compared . selected as were found to be free of hepatomas . 
any effects observed in the yeast series have , therefore , primarily to be attributed to the substitution of milk powder by dried yeast . experiment e is in good agreement with harris 's findings that an increase in milk proteins there exists now failed to protect against the action of 2 - acetyl - amino - fluorene . good evidence that a high casein - high riboflavin diet protects only against dimethyl - amino - azo - benzene . 
even related compounds ( giese , clayton , miller and baumann , 1946 ) are not inhibited to the same extent by such a diet . further , strong and figge ( 1946 ) , who reviewed the literature on this subject , did not succeed in inhibiting by a diet of liver supplemented by a combination of raw milk , riboflavin and xanthine the development of tumours induced by subharris 's failure to protect against cutaneous injection of methylcholanthrene . acetyl - amino - fluorene by a diet which inhibited the action of " butter yellow " has already been mentioned . the results obtained in the yeast experiment are not impressive , but they seem significant since the same trend of delayed tumour growth was found in three experiments involving various litters of two different strains of rats . it would probably have been an advantage to use a smaller dose of the carcinogen in the experiments reported in this paper . 
of acetyl - aminofluorene will still produce a high percentage of cancers . it seems possible that the relatively low incidence of cancers observed by cantarow , paschkis , stasney and rothenberg ( 1946 ) after prolonged treatment of rats with acetyl - amino - fluorene was partly due to a supplement of brewers ' yeast in the diet given . the problem whether certain dietary factors are true anti - carcinogens , or protect only the liver against a damage the reaction to which leads to the establishment of cancers , could not be answered by workers who studied the effect of it was hoped that working diet in rats receiving dimethyl - amino - azo - benzene . with a more versatile carcinogen would give a clue to this question . at first sight it seems that in experiments a , b and c the development of all types of there was , for instance , a significant reduction in the tumours was delayed . incidence of mammary cancers in females of the wistar strain . this finding , however , could be explained also by the assumption that a less damaged liver was better able to cope with an excess of endogenous oestrogen and so prevented the ' development of tumours of the breast . 
doll. from the statistical research unit of the medical research council , london school of hygiene , keppel stred , kondon , w.c.i. received for publication november 28 , 1953 . attempts to derive theoretical laws from changes in the death rate with age have a long history . 
they have not , in general , been very fruitful and there has - been some hesitation in applying the technique to the study of cancer . recently , however , two hypotheses about the mechanism of carcinogenesis have been put forward , which have been derived from analysis of cancer mortahty fisher and horomon ( 1951 ) used statistics from the united states statistics . for cancer of the stomach in women , and nordling ( i953 ) , classing all sites together , used statistics for cancer in men from britain , france , norway and the u.s.a. both found that , within the age group 25 - 74 years , the logarithm of the death rate increased in direct proportion to the logarithm of the age , but about six times as rapidly ; in other words , the death rate increased proportionany with the sixth power of the age . 
death rates in some age groups under 24 years were . higher than would be expected had this basis been a general law throughout iffe . rates for the age groups above 75 years were considered unreliable and were excluded . in interpreting these observations , both assumed that mortahty gave a good indication of incidence and treated the data as if they referred to age specific incidence rates . 
they considered that cancer in youth might be affected by special factors which were unhkely to operate at later ages and they , therefore , felt justified in basing their hypotheses on the data recorded for adults . fisher and horomon ( 1951 ) pointed out that the observed relationship between age and mortahty could result if a colony of six or seven cancer cells was a critical size below which independent growth was not sustained . thig hypothesis , however , also leads to the conclusion that cancer incidence should be proportional to the fifth or sixth power of the concentration of the effective carcinogen whereas experimental data suggest that , in general , tumour incidence and concentration of the carcinogen vary ' in arithmetical proportion . 
the hypothesis in its simple form is , therefore , untenable . nordling ( 1 - 953 ) , on the other hand , suggested that the observed relationship would be explained if a cancer cell was the end - result of sev ' en successive mutations . this hypothesis does not lead to the observed result in all circumstances . does so only if the probability of occurrence of each mutation remaihs constant throughout hfe . in this case and so long as the occurrence of each mutation p . 
the logarithm of the incidence rate will then be directly proportional to the logarithm of the age and will increase six times as rapidly , ix , log rate 6 log t + a constant . in contrast to fisher and hollomon 's ( 1951 ) hypothesis this leads to the conclusion that the final rate of tumour formation wir be directly proportional to the concentration of an applied carcinogen , so long as the probability of occurrence of a mutation is proportional to the concentration of the carcinogenic factor and different factors are required to effect different mutations . in his analysis , nordling ( 1953 ) grouped all types of cancer in men together and considered them as a whole . 
he gave no detailed figures for cancer in women , but stated that for cancer of the sex organs the increase in mortahty was fairly small above the age of 4.5 and that for other sites the mortality seemed " to increase according to the sixth power of the age both before and after the forties but not during the decade of the menopause when the increase is smaller . " he considered that the entire increase with age in cancer incidence among adults was not wholly explicable by a mechanism of multiple mutations but that hormonal control of growth might play an independent part . 
1 - 4 show the logarithms of the male and female death rates from cancer of the commonest sites in england and wales in 1950 and 1.951 ( registrar general , 19521 1953 ) , plotted against the logarithms of the mid - points of the age groups . for each sex , all those sites are shown for which more than 1000 deaths were recorded in each of the two years . 
are less reliable than those for the subsequent ones since they are based on much smaller numbers , and both standard errors and ( to a lesser extent ) arithmetical errors are much larger . for example , the standard error of the death rate from gastric cancer in women is 18 per cent of the rate for the first age group ( 25 - 29 years ) and .2 per cent of the rate for the last ( 70 - 74 years )  . that is to say , the logarithms of the true rates for these age groups are likely to lie within a range of - .0 - 13 and - .0 - 02 respectively of those showm in fig . 
i. - change in mortality with age for cancer of the oesophagus , stomach and pancreas in men and for cancer of the stomach and pancreas in women shown on a double logarithmic scale , that is , the logarithm of the death rate per million persons plotted against the logarithm of the mid - point of the age group . 
the straight line through the points has been drawn arbitrarily to give the best fit , subject to the gradient being 6 to 1 . cancer of the stomach , colon , rectum and pancreas in women - the observations fall fairly close to the lines . in some , however ( cancer of the colon in men , cancer of the stomach , colon and rectum in women ) , the observations fall closer to lines with less steep gradients . 
the relatively high rates at the younger ages could , however , result if the population contained a group of subjects speciahy susceptible to cancer of these sites in early life - and so far as cancer of the p . 
doll colon and rectum is concerned , such a group is in fact found in subjects of polyposis coli . the actual regression coefficients for all the first group of cancers are shown in all the mortahty rates for this group , table i ; they vary from 4 - 97 to 6 - 48 . therefore , show the same sort of association with age as was reported by fisher andhoromon ( 1951 ) andbynordling ( 1953 )  . 
3. - change in mortality with age for cancer of the lung , bladder and prostate in men and for cancer of the lung in women , shown as in fig . 
1. i 0 - 1 - 6 consists of cancers for which there is already reason to believe that the strengths of some of the factors responsible for their development are variable . cancers of the prostate , breast , ovary , and cervix and corpus uteri are all believed to be influenced by endocrine secretions , which vary 1 ' n each individual in the course of his life ; a proportion of the cases of cancer of tho lung is believed to be related to cigarette smoking which has become more prevalent in the last 50 years and a proportion of the cases of cancer of the bladder is due to occupational hazards , to which men have been exposed for various periods at various ages . 
on the hypothesis that carcinogenesis is a multi - stage process , therefore , cancer at these sites would not be expected to show a uniform relationship between death rates and any power of the age . 
doll the sort of irregularities to be expected will depend on the periods when the carcinogenic factors are most active and on which of the stages in the process of carcinogenesis are affected . 
an increased rate of production for a short time during early life will provide a larger number of altered cells to be acted upon by other factors in the future , and wfll therefore appreciably affect the incidence at , say , age 60 . 
the weight depends both on the time of operation of the carcinogenic factor concemed and on the order of the cellular change which it affects . if t is the age at which the cancer incidence is observed , to the age at which the subjects are exposed to the factor , and s takes a value between i and 6 according as the change effected is the first , or sixth , then the weight is proportional to second , tos - i ( t - to ) 6 - 8 . hence it can be show - n that the weight by which a varying probability of the first mutation would be multiplied is highest at age 0 and decreases rapidly throughout life . 
the weight for the probabihty of the second change reaches its maximum one - fifth of the way through the exposure period ; that for the third change , for factors effecting the seventh change ' , two - fifths of the way ; and so on . the cancer incidence will be directly proportional to the rate of production of this change at the time of observation , and the previous behaviour of this rate will be irrelevant ( i.e. , will have zero weight )  . since the weighted mean of the varying probabihty will in general depend on the age , t , the overall incidence at age t is no longer proportional to the sixth power of t . 
doll old ages , can be attributed to the fact that the populations concerned belong to if mortality generations which smoked fewer cigarettes than subsequent ones . at different ages is examined for cohorts born in different five - year periods , the effect disappears . the concept of carcinogenesis as a multi - stage process also makes it easy to understand the mechanism of the latent period which occurs after exposure to a for example , kennaway carcinogenic agent before the appearance of a tumour . ( 1947 ) has demonstrated that circumcision deferred until the fourteenth year of life fails to give the complete protection against cancer of the penis that it provides when carried out on the eighth day ; in other words some change must take place within the first 14 years of life which eventually leads to the development of the disease after a latent period which may be as long as 70 years . 
on the hypothesis that penile cancer is the end - result of a series of seven successive cellular changes - the first of which occurs only in the presence of the prepuce , it can be shown that at age 53 ( the average age * of all the patients referred to in table ii ) the relative risks of developing the disease when circumcision is carried out at the mid - points of shrek and lenowitz 's ( 1947 ) age periods are 0 - 30 , 0 - 77 , 0 - 98 and 1 - 00 ( see mathematical appendix )  . children circumcised during the first six years of life are , however , most likely to have been operated on within the first few weeks , in which case the theoretical risk for this group would be of the order of 0 - 01 . 
on the other hand , u the present data were held to be equally accurate at all ages ( including the oldest ) it would be possible to obtain a quite different mathematical relationship . thirdly , other mechanisms than that of a multi - stage process can also be postulated to account for the observed relationship - and one has , in fact , been suggested by fisher and hollomon ( 1951 )  . moreover , some other diseases show similar types of increase with age ( e.g. , cerebral haemorrhage , coronary thrombosis and gastric ulcer ) and it is difficult to believe that they should all be dependent on the same type of mechanism . bereilblum and shubik ( 1949 ) , in summarizing the results of their experiments , have , however , stated that " whatever interpretation is adopted as a base line for research , the recognition that careinogenesis is at least a two - stage process , should invariably be bome in mind "  . it is , therefore , natural to see whether a twostage process - or even a more complex multi - stage one can account for the human data . 
from the analysis that has been made here , it would seem that a complex process of perhaps six or seven stages could account for : sites , and ( 1 ) the rapid increase in mortahty with age observed in cancer of some ( 2 ) the irregularity in the increase in cancer of some other sites ( 3 ) the long latent period observed after exposure to a carc ' mogen ( 4 ) clinical observation . 
doll the mortality rates for cancer of the lung , bladder and prostate in men and for cancer of the lung , breast , ovary and cervix and corpus uteri in women also accord with the theory , if it is postulated that the carcinogenic factors responsible have varied in strength . a formula has been obtained which can be used to weight the strengths of the carcinogenic factors at different periods and it is shown that the time when the strength of the factors responsible for the individual changes is of greatest importance varies according to which change in the series is affected . 
the conclusion provides a possible explanation for the observation that circumcision exerts an important protective effect against the development of cancer of the penis only if it be carried out early in life . we are most grateful to r . 
more precisely , we assume that the probability that the sth change occurs in the small interval i changes have already occurred , is p , ( to ) dto where ( tw to + dto ) , given that s all the other p 's are assumed to be constant . 
then p , ( to ) is a function of to . the probability that the sth change occurs in the interval ( to , to + dto ) , and the rth in the interval ( t , t + dt ) , is the product of ( i ) the probability that exactly s i changes occur in the interval  . 
we shall ignore the variation in age amongst the patients , and consider the expected incidence of penile cancer at t = 53 years ( the average age of all the patients referred to in table ii )  . 
w.3. received for publication march 1 , 1952 . some of the effects of ionising radiations are associated with formation of such effects are often reduced free hydroxyl radicals and possibly of peroxides . for these under anaerobic conditions and increased in the presence of oxygen . reasons it appeared possible that conditions which would increase the concentration of hydrogen peroxide in tissues might augment the biological effects of of the possible ways of increasing radiosensitivity by such a radiation . mechanism , two have been investigated . the first depends upon increasing the concentration of substrates , the metabolism of which is known to produce hydrogen peroxide . such substrates are those oxidised by flavine enzymes , including aldehydes , xanthine , hypoxanthine this method is being investigated by administration of and d - amino acids . suitable substrates and riboflavin , the latter in attempts to increase the concentration of flavin enzymes of the tumours . a second method of increasing hydrogen peroxide concentration of tissues depends upon the inhibition of the enzymes involved in hydrogen peroxide thus by inhibition of catalase and peroxidase of tissues this destrucdestruction . tion and utilisation of hydrogen peroxide might be prevented and its concentration in cells should increase . this was attempted without success in the present paper . many of the known catalase inhibitors including sodium azide and cyanide are also respiratory poisons . 
x 77 , 500 so , where ko = the reaction constant at zero time expressed in logarithms to base 10 and so = the h202 concentration at zero time . 
kat.f. qo21 - 29 x 10 - ' mxh20 activity of a tissue to the other metabolic processes expressed in q values . the tables of this catalase activity is expressed as qo21 29 x lothis expression makes it easier to relate the catalase the catalase activity is determined at 0 c . 
the testis probably oxidised primary carbohydrate . recent work has shown that ionising radiations ( taylor , greenstein and radiomimetic hollaender , smith , 1950 ) induce depolymerization of deoxyribonucleic acid . 
some of the biological effects of radiation may be due to such an action occurring in in the case of ionising radiations the effect is probably due to fr~e the cell . hydroxyl radicals which are produced in irradiated water . if increase in hydrogen peroxide concentration should increase sensitivity to x - rays , then addition of hydrogen peroxide to a solution of deoxyribonucleic acid should augment the depolymerising action of x - rays . such an effect has indeed been found by conway and butler ( 1952 )  . a large number of substances have been reported as catalase poisons , and some of these are listed in table i in order of potency . in the present work the activity of catalase poisons is compared with their toxicity to mice and an attempt made to measure the inhibition in vivo . 
the toxicities are also listed for some of the compounds , and the ratio of the concentrations causing inhibition of the enzyme to the toxicity expressed as the ld 50 ( calculated on a molar basis ) is given in table i . 
gallico the poisoning of catalase in vivo is difficult to estimate owing to the reversibility of the poisoning . blaschko ( 1935a ) showed that of a number of catalase poisons only potassium chlorate produced irreversible inhibition . 
the pretreatment with the catalase poisons tried did not modify the effect of radiation on the tumour . reduction of sensitivity of mice treated with sodium azide and hydroxylamine to x - radiation . groups of each stock of 10 mice were exposed to 700 r irradiation from an x - ray tube operated at 220 kvp . 
the result with azide is similar to that obtained by bacq ( 1951 ) , but the result with hydroxylamine appears to be a new finding in general agreement with bacq 's work . a4 [ 2 ' ' ' " 45 1 : contro . 2 : - inece wit 1.5per kg ; nan3 15m.bfoeradato. 
gallico the search for a poison more specific for catalase than is azide was also unsuccessful . sodium azide and hydroxylamine are much the most specific catalase poisons of the compounds examined . p - hydroxyphenylazide had only 1 / 50 of the activity of sodium azide ( calculated on a molar basis )  . this difference is exactiy the same as that found between hydroxylamine and phenylhydroxylamine . on the other hand , phenylhydrazine appears to be a more potent inhibitor than hydrazine ( blaschko , 1935a )  . 
the introduction of a methyl group into the hydroxylamine molecule ( o - methyl - hydroxylamine ) reduced the activity 400 fold . the inhibition produced by diethyl - p - phenylenediamine was of the same order as that described for dimethyl - p - phenylenediamine by homer and betzel ( 1950 )  . the figures on the ratio of catalase inhibiting concentration to lethal dose show that sodium azide is the most favourable catalase poison as well as the most active . 
the median lethal dose of sodium azide should give , a concentration of azide which is one thousand times that causing 50 per cent inhibition of catalase . thus , sodium azide is probably the safest catalase poison for use in vivo in spite of its high toxicity . the increase in poisoning activity of azide with decrease in the ph is similar to that found for the effect of formate and acetate by agner and theorell ( 1946 ) , who showed that anions in general combine with catalase and inactivate it to an extent increasing with decrease in ph . these authors explained this as due to the anion displacing the hydroxyl group of the catalase and it is possible that azide acts in the same way . 
the data of agner and theorell ( 1946 ) on poisoning of catalase with formate at different ph values are analogous to those found for azide ( table iv ) as shown in table xi . 
the replacement of a hydrogen of formic acid by ch3 as in acetic acid reduces the activity 800 fold ( agner and theorell , 1946 ) , which is the same order as that produced by the introduction of an o - methyl group in hydroxylamine . thus the poisons may combine readily with catalase , possibly replacing a hydroxyl group or hydrogen peroxide because of their shape and size . in testing this hypothesis , methylamine was found to be a poison ( of the same order as hydrazine ) , but ethyl formate and formamide , which it was hoped would be as effective as undissociated formic acid , were both found to be inactive . while the poisoning with hydrazoic acid and formic acid may depend upon the entire undissociated molecule , the poisoning with hydroxylamine and hlydrazine appeared to be independent of the ph . 
now in the cases of hydrazoic acid and formic acid , ionisation would result in loss of a hydrogen atom ( and gain of a charge ) , so that the ion would have less structural resemblance to hydrogen peroxide . 
gallico ( 3 ) poisoning of catalase of liver and tumour of rats was demonstrated after injection of azide . ( 4 ) injection of small doses of azide or hydroxylamine into rats immediately before x - irradiation did not increase the radiosensitivity of tumours . injection of large doses of azide or hydroxylamine into mice before irradiation reduced the mortality from x - irradiation of the whole body . ( 5 ) catalase activity could be expressed as a qo21 - 29 x 10h202 value in p11 . 
the investigation was supported by grants to the royal cancer hospital and chester beatty research institute from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the national cancer institute of the national institutes of health , u.s. 
i. received for publication january 4 , 1951 . recent work has provided evidence in favour of the supposition that tumours contain , and therefore probably release into circulation , a substance capable of depressing liver catalase activity . 
nakahara and fukuoka ( 1949 ) claimed to have produced a liver catalase depr ' ession in mice after the injection of alcoholprecipitated fractions obtained from human tumours . similar fractions from normal tissue were stated to be inactive . 
adams ( 1950a ) commenced a study of the effect of the injection of homogenized mouse tumours into mice , and showed that after an early ( 24 and 48 hours ) depression , the hver catalase level returned to normal approximately 4 days after injection , and fer once more as the new tumour grew . 
the results were interpreted as indicating that the initial depression is due to some substance or substances present in the , injected material , the second depression only being due to the new tumour . injection of homogenized normal tissues had no effect on catalase level . appleman , skavinski and stein ( i950 ) , in the course of an investigation of the variations in erythrocyte , kidney , and liver catalase activity in rats bearing the jensen sarcoma or the u.c.l.a. 
fibrosarcoma , found that normal rats kept on a protein - free diet showed a drop in liver catalase activity to approximately 50 per cent of normal within 7 to 10 days from the time thev were placed on the diet and this low level wa - s maintained for 53 davs or longer . 
the variatioils in liver catalase level following the subcutaneous injection of coarse suspensions of these tumours into albino mice results in both males and females were similar to those preappear in table 1 . viously obtained with s37 and carcinoma 63 . 
adams two general methods have been employed : the first involved the injection of s37 sarcoma , which had been treated so as to render it incapable of giving rise to tumour growth , and the second , the results of which are presented in the next section , the injection of pure line mouse tumours which do not grow in the strains of mice used . sarcoma 37 tissue was disintegrated by shaking for several minutes with glass beads in a " mickle " tissue disintegrator , made by messrs . 
is a plot of the subsequent variation in hver catalase level over a cers . period of 10 days , the crosses representing the arithmetic mean values of the groups . in the experiment represented iin the left - hand graph the tissue was disintegrated in normal saline ( ph 6 - 8 ) , and it wir be seen that a 24 - and 48 - hour depression was obtained , the level rising to normal at 4 days and remaining so at 7 and 10 days . however , this treatment was not completely succe 'ssful in pre ' venting tumour growth , in spite of failure to discover intact cells in the homogenate microscopicary . 
the experiment was repeated , using m / 100 citric acid as the suspending fluid ( ph 5 - 5 ) , and the results appear in the righthand graph . 
the catalase depressing effect is very similar , but in this case no tumours appeared in 18 mice kept for 3 months , when the experiment was terminated . a second method involved the partial centrifugation of a fine homogenate ofs37 tissue in normal saline , prepared originall with a tenbroeck grinder . 
n. abscissa : time in days . effect of in ' jection of tumours which do not grow in the 8train of mice u8ed . a number of pure line mouse tumours which do not grow , at any rate after the in ection of coarse homogenates , in the stock albinos used , were injected subcutaneously or intraperitoneally in 100 mg . 
the results appear in table il in every case a significant depression in catalase activity was observed 48 hours subsequently , with a return to normal by the 4th to 7th day . in one experiment of this series , not recorded in table 11 , a different result was obtained . 
the catalase level at 48 hours was very low , and remained low at 4 days ; at 10 days , of th - e 6 remaining mice , 3 in which the abscesses were healed had high levels and 3 120 d . 
the results are given in table il no significant variations in catalase level were observed , and with the rat tumours in particular the variations appear to be completely random . ..cb - r = 1 l -  . 
the points lie on a slightly curved line , showing a progressive deorease of catalase activity with dose . the depression is seen to be approximatelv proportional to dosage over the range 10 to 30 per cent . 
4. - liver catalase levels 48 hours after the intraperitoneal injection of varying quantities of coarse homogenate of sarcoma 37 into stock albino male mice . ordinate : catalase level in arbitrary units / mg . 
adams it is not claimed , however , that nutritive effects play no part in producing the depression of catalase activity , particiilarlv in animals bearing large tumours . miller ( 1950 ) has recently shown that although catalase level in animals which are maintained on low or non - protein diets parallels approximately the level of total liver protein , the enzyme soon begins to disappear more rapidly than the consequently , even if the only relevant effect of a large remaining protein . tumour on the nutritional status of an animal were a simple depletion of protein , however , the depression which occurs in a depression of catalase would result . the early stages of tumour growth may be expected to be due mainly to toxic material produced by the tumour , since the importance of purely nutritive factors , e.g. , protein depletion , must be small at this stage , though becoming progressively greater as the tumour size increases . 
the effectof large tumours on catalase is probably the resultant of separate nutritive and toxic actions , which could not be readilv distin uished . the effect of injecting infected c57 sarcoma is quoted as a possible source of error in investigations of this nature . it is not yet known whether catalase depression is a common result of bacterial infections , but this possibility must be reckoned with when using , for example , human intestinal tumours , which are greenstein ( 1947 ) states that infection of mice with certain often infected . strains of poliomyehtis virus , or with streptococci and staphylococei , has no . however , it has been observed in this laboratory effect on catalase activity . during epidemics of a sabnonella infection , and of ectromelia , that catalase level was low when the liver showed signs of involvement . 
dounce and shanewise ( 1950 ) i - lave recently shown that catalase activity is significantly depressed in rats suffering from advanced murine leprosy . apart from these isolated observaticjns , no detailed investigation has beeii made of the effect on liver catalase of infections of the liver , or of injections of infected normal or malignant tissue . although a depression of liver catalase may occur in conditions other than cancer , this does not detract from the importance of the effect as a property of maligiriant but not of nornial tissue , and work on the mechanisbv which the toxic substance exerts its effect may thrcw light on some fundamental difference recently reports of prehminary experibetweennormal and malignant tissue . ments have appeared , indicating the importance of hormones in maintaining a normal level of liver catalase ( begg and reynolds , 1950 ; adams , 1950b )  . present investigation is being follo - vved up by an endeavour to relate the tumourdepressing effect with the hormonal control mechanism . depression of liver catalase activity b - as been shown to follow the injection into mice of mouse tumours , but not of rat and human tumours in single doses of up to 100 mg . 
nakahara and fukuoka ( 1949 ) , on the other hand , observed a depression after the injection of alcohol - precipitated fractions of human tumours however , their dosage , referred to weight of original tissue , was into mice . probably very much bigher than that used here . all that is now claimed is that injection , in the dose used , of mouse tumours into mice produces a considerable depression of liver catalase , while injection of similar doses of tumours of other species produces no apparent change . 
the early variation in injection . females was not significant in one case . ( 2 ) injection into stock albino mice of sarcoma 37 tissue ( a ) disintegrated in m / 100 citric acid , or ( b ) partly centrifuged after coarse homogenization in 70 mg . 
doses , resulted in a depression of liver catalase without any obseirvable tumour growth . ( 3 ) six pure line mouse tumours , which do not grow in the stock mice used , also gave catalase depressions 48 hours after injection in 100 - mg . 
the work was undertaken as a collater ' al contribution to a wider scheme planned in 1952 by the cheshire and north wales branch of the british empire cancer campaign . for research into the pathogenesis of cancer the branch council required among many other things a laboratory analysis of soil taken from the vicinitv there was no precedent for the sort of analysls of the home of each patient . most suited to the project , previous workers in this field having been content with simple and often crude analyses or with the more detailed examination of too few specimens . it was clearly impossible to make a full physical and chemical examination of all the solid , fiquid and gaseous phases of every soil sample as several thousands were to be examined , so with some slight modification the analytical procedure of the soil survey of england and wales * was adopted - at first . it was felt , however , that an investigation of fatal cases of cancer in relation to soils as mapped by the late professor g . 
every case where cancer was mentioned on the death certificate , even when not the immediate cause of death , was included in the analysis , except that those occurring in the county of persons ordinarily resident in other areas were excluded . cancer was defined as any condition named in no . 
the differences between observed and expected values were subjected to the chi - squared test to determine the probabihty of such differences arising as a result of random these are the probabilities quoted in the tables that follow . 
that cancer of site a would be no more associated in an compariwith attribute b than would be the generality of cancer deaths . sons , unless the contrary is indicated , allowance was made for variations attributable to age and sex by calculating separately an expected number for six agesex groups and then adding . 
where it was desired to allow for a possible interaction between associations , expected values were adjusted . for example , if cancer of site a had shown an association with both attribute b and attribute c considered singly , and attributes b and c were known or suspected to be associated one with the other , adjusted distribution of expected values with respect to b were determined as follows . 
thus series having a common parent material geologically , are all indicated by the same capital letter , e.g. , all derived from non - calcareous shales of ordovician age are indicated p . 
the inclusion of many of this large group in social these considerations and our special class ii was therefore open to question . interest being in the association between cancer of the stomach and soil , suggested that it might be advisable to treat separately those occupations which bring the person into intimate connection with the land . 
griffith the public mains are supphed for the most part from surface water such as there is an exception where two small small lakes fed by streams and springs . ceintres get their water from deep bore holes but the populations are too smafl to be separated in the analysis . 
the in group l there social groups , however , show certain interesting differeinces . does not appear to be any association with fl soil . there is a relative excess of deaths in the other three groups although only in group iii is this undoubtedly siginificant in the statistical sense . soil and cancer of the breast . when corrections are applied for social group and water supply it is found that the association betweein cancer of the breast and a soil as compared with all other forms of caincer is stif present ( table x )  . 
0 - 20 > p > 0i i - ii * stomach all sites iii * stomach all sites iv - v * stomach ar sites stomach all sites all social groups : stomach males all sites females stomach ar sites 13 - 8  . 
bruzzone. from the department of experimental medicine , national health service of chile , santiago . received for publication june 9 , 1949 . abdominal fibroids induced in the guinea - pig by a - oestradiol ( nelson , 1937 ; lipschutz and iglesias , 1939 ) are prevented when progesterone or other 3 - ketosteroids are administered simultaneously with the oestrogen ( lipschutz and vargas , 1941 ; lipschutz , 1944 ; lipschutz , iglesias , bruzzone , fuenzalida and riesco , 1948 )  . 
 = fibrous tumoural effect ; units according to lipschutz and vargas ( 1939 ) t tablets of pure progesterone or part of a tablet . in the remaining groups - tablets from experiments of e . 
but these figures of active quantities of progesterone are not very distant from those obtained in our former work with the antifibromatogenic action of progesterone against o - oestradiol . there is also the fact that statements about absorption per day are stultified by its not being uniform throughout the experiment on account of the diminished surface , and by substances entering into the tablet from outside ; errors are 400 s . 
bruzzone this is why it would be daring to consequently considerable ( folley , 1944 )  . interpret the present results as indicative of a greater resistance of artificial oestrogens to the antifibromatogenic action of progesterone . 0o i1111j1 hexestrol hexestrol and progesterone fig . 
 lung tissue is unsuitable for direct injection of carcinogens , consequently pulmonary tumours in laboratory animals have hitherto been induced by applying the carcinogen at some remote site , by injecting it subcutaneously , intratracheally , intravascularly , intraperitoneally , or by including it in the diet . 
 recently the author ( horning , 1947 ) reported the induction of pulmonary tumours after relatively short periods of treatment by the direct application of carcinogens to adult lung tissue growing as subcutaneous homologous grafts in host animals . 
 the method of tumour induction consists in isolating small strips of lung from 6 - 12 weeks strain a mice , impregnating the grafts with crystals of a carcinogen ( 2 - acetylaminofluorene , 2 - aminofluorene , or 20 - methylcholanthrene ) prior to im planting them subcutaneously into host mice of similar age and strain in a manner which has been described elswhere ( horning , 1947 )  . 
small palpable tumours were obtained at intervals ranging from 6 - 12 weeks following grafting , but in order to examine the differences between the responses to individual carcinogens , grafts were fixed before tumours developed at intervals ranging from 1 - 5 weeks after implantation . 
 lung fragments from 6 weeks old strain a mice were grafted , in some instances without the carcinogen , into host mice of similar age , and also into mice of 15 months age which were selected from stock mice of undetermined ancestry . 
 this was done to find out if the survival of homologous grafts was dependent on employing a closely inbred strain , or whether it might be influenced by the age of the host . 
 in another series of experiments a number of lung grafts were treated with 20 - methylcholanthrene , half being implanted into the superficial fascia , and the remainder placed as usual between the skin and the abdominal wall . 
the host mice were again of the same age and strain , and it was thought that some infor mation might be obtained as to whether rapid vascularization played any role in successful survival of the grafts . 
 lung tissue was obtained from 30 strong a male mice aged 6 weeks , and implanted subcutaneously into host mice of the same strain and age , each indi vidual receiving 2 grafts on each side of its belly ( table i )  . 
when the same number of grafts from females were implanted into strong a male mice over 8 months of age , only 14 grafts had survived after 8 weeks and 4 of these contained areas of necrosis ( table i )  . 
grafting the same number of lung implants from strain a mice 6 weeks old into stock mice of indeterminate ancestry , all of which were over io months old , resulted in 58 becoming totally absorbed after the same interval of 8 weeks ' implantation ( table i )  . 
either the nuclei become pycnotic , or as in most grafts they lose their differential stain ing and the cytoplasm becomes homogenous , to be followed in later stages by fragmentation and dispersal . 
the nuclei of the collapsed lung alveoli undergo chromatolysis far more rapidly than those of the adjacent bronchiole epitheliu histological examination of these grafts suggests that their failure to survive in host tissues may be due to a partial failure of vascularization which induces necrosis . 
these results obtained with adult lung grafts indicate that successful survival and growth depends on age of both the donor and host animals , together with employment of a closely inbred strain in which homologous grafting is much better tolerated than in mixed strains . 
 in order to obtain a foreign body reaction fragments of lung from 6 - 7 weeks old donor strong a mice were treated with crystals of commercial cholesterol and subcutaneously implanted in 8 - weeks - old host mice ( table i )  . 
 in every instance in this series of experiments lung tissue was obtained from strong a mice of either sex , 7 - 8 weeks old , and impregnated with the carcinogen and implanted subcutaneously into host mice of the same strain and age ( table i )  . 
 the remaining 13 were no longer translucent , and it was found that eight of these opaque grafts had been accidentally transplanted into the superficial fascia instead of between the skin and the abdominal wall . 
 the histological characteristics of pulmonary tumours induced from sub cutaneous lung grafts treated with carcinogens differ in some respects from those of tumours arising in sitit in the intact lung of rodents under the influence of in pieces of isolated lung growing as . 
 a typical carcinoma of the lung in a graft impregnated with 20 - methylcholan threne fixed 11 weeks following subcutaneous implantation in a strong a host mouse is illustrated in fig . 
the lumen of the bronchiole is occluded by cellular debris , and the epithelium in some regions has become stratified , but in the malignant area the bronchiolar epithelium is ciliated._ the cells comprising this neoplastic focus possess all the histological characteristics of malignant cells . 
 the histological appearance of these carcinomas varies , however , according to the age of the primary gra those recovered from mice 9 - 12 weeks old consist of acini of cells with large oval nuclei . 
 all primary tumours induced by the several carcinogens were obviously bronchogenic carcinomas , with the exception of a squamous - celled growth in duced by 2aaf after 16 weeks ' implantation . 
one was a polymorphic and the other a spindle - celled sarcoma~ as both these tumours were too far advanced in their growth it was impossible to ascertain whether they were derived from the tissues of the implant or from the host , so they were discarded . 
in some which carried six or more graft1 it was frequently noticed that after 8 - 10 weeks the palpable grafts varied considerably in size , and that this variation often occurred irrespective of the particular carcinogen employed . 
those implants which failed to develop into tumours , and were hardly palpable in the living host , were found to contain large inflam matory foci or areas of foreign body reaction . 
in every instance the inflamed grafts were obtained from the same donor mouse grown in the same host and treated with the same carcinogen for a similar period of time as those which developed into tumours . 
 in the majority of grafts ( table i ) necrosis and fibrosis are absent , although these changes are so often associated with inflammation of the intact lung in situ . 
 bronchioles when present in these grafts tend to be obscured , since the lumen is filled with cellular exudate consisting mainly of lymphocytes , plasma cells , and a few macrophages or polymorphs . 
multinucleated giant cells frequently seen in tissues reacting to foreign bodies were absent in grafts treated with car cinogen , but were found in several implants impregnated with commercial choles terol . 
every lung graft was fixed in alcoholic bouin and stained by ehrlich 's haematoxylin and eos f1 . - a typical bronchogenic carcinoma , induced from a graft of adult normal lung impreg nated with crystals of 20 - methylcholanthrene , fixed 11 weeks following subcutaneous implan tation in a host ( strain a ) mouse . 
this is of special significance , as it indicates that the carcinogen has a selective action only for the bronchiolar epitheliu the adjoining alveolar cells remain quiescent to the local presence of the carcinogen . 
the lumen of the bronchiole is occluded with a cellular exudate , and in some regions the epithelium has became stratified , but in area of malignant focus the bronchiolar epithelium is ciliated . 
 since the induction of carcinoma of the prostate in mice , arising from fragments of adult glandular epithelium combined with the carcinogen growing as homologous subcutaneous grafts in host mice , was first reported ( horning , 1946 ) , this method of tumour induction has been successfully extended by other investigators to other tissues and organs . 
more recently hughes ( 1949 a , b ) , using the same technique , has succeeded in inducing transplant able carcinomas from fragments of adult bladder and uterine epithelium combined with methylcholanthrene , as well as tumours of adrenal cortex . 
 one of the several advantages arising from homologous subcutaneous grafting in the presence of a carcinogen is that the tumours growing under the skin are palpable , and can readily be obtained at the required stage of growth . 
the time taken for tumours to appear is shorter most likely because the carcinogen is more concentrated , and lies in close proximity to the bronchiolar epithelium of the gra with indirect methods of induction such as painting the carcinogen of the skin , by injecting it or including it in the diet , there may be changes in organs and tissues throughout the body , and not necessarily only in the region where a tumour arises . 
 thus dunlap and warren ( 1942 ) have reported that if swiss mice are injected subcutaneously with carcinogenic hydrocarbons , the incidence of primary pulmo nary tumours is higher in mice which have also developed tumours at the site of inoculation . 
 it must be admitted , however , that these two methods of induction differ fundamentally , because the changes which occur in the intact lung in situ following treatment at some remote site with a carcinogen are not necessarily the same as those which take place in homologous subcutaneous grafts of isolated , collapsed lung . 
these differences were discussed in a recent paper by orr ( 1947 ) , in which he rightly pointed out that it is difficult to compare results obtained by the two methods of induction . 
 recent eijeriments have shown conclusively that the survival of lung grafts either with or without the carcinogen is dependent upon the age and strain of the donor mouse , together with the age and strain of the host . 
examination of table i shows , however , that donor lung implants impregnated with a carcinogen survive more readily and in greater numbers in older hosts than would be the case if the grafts did not contain any carcinogen . 
it is of course possible that since the lung carcinomas arise from bronchiolar epithelium , some grafts may at the outset contain insufficient epithelium of this region to give a response . 
a separate series of experiments in progress show that pulmonary tumours are obtained more readily and in greater numbers from fragments of lung in which particular care has been taken to isolate portions of a bronchus , discarding the more peripheral parts of the organ . 
otherwise it is difficult to understand why prostatic epithelium should flourish as a graft despite the antagonism between graft and host tissues , and yet lung fragments implanted under the same conditions do not always survive so readily . 
pre liminary experiments reported elswhere ( horning , 1949 ) suggest that tissues which are normally under hormonal influence are much better tolerated as grafts in host mice of the same sex andstrain than tissues which are to a greater extent independent of hormone action . 
a higher incidence was not obtained in males , as seems to be the case in human lung cancer according to clemmensen and busk ( 1947 ) , and in strain a and strain c mice treated with urethane in the experiments of larson and heston ( 1945 )  . 
there is a slight difference between the potency of the three carcinogens used in the present experiments in that a greater number of tumours appeared in grafts treated with 20 - methylcholanthrene . 
 with regard to the histogenesis of the present lung tumours the method of grafting allows examination of the neoplastic changes in graded stages , leaving no doubt that the tumours arise from bronchiolar epitheliu it is curious that no response to the carcinogens is obtained from the walls of the lung alveoli . 
 an alveolar epithelium exists why should it remain entirely quiescent , whilst the closely adjacent epithelium of the bronchioles proliferates in so striking and so specific a manner ? controversy still exists concerning the nature of the lining of the lung alveoli . 
ross ( 1939 ) maintains that although an epithelial lining to the alveoli is not visible in ordinary histological preparations , it becomes appa rent in response to certain abnormal stimuli . 
grady and stewart ( 1940 ) not only affirmed the existence of an alveolar epithelium , but regarded it .as the source of lung tumours in mice treated with methylcholanthrene . 
 thus while they agreed that human tumours are bronchogenic in origin , they were convinced that mouse lung tumours arose from the alveolar epitheliu more recently herbut ( 1946 ) has reviewed the ev ' idence concerning the origin of human lung tumours , and concludes that all " alveolar cell tumours " come from the basal cells of the bronchi and bronchioles ; and that there is no justification for assuming that they arise from septal cells . 
it is unlikely that any fundamental difference exists between the rodent and human lung , and since there is such clear indication of the origin of malignant foci in early grafts combined with a carcinogen , it would appear that the case for bronchogenic origin of all lung carcinomas is strengthened . 
in the presence of chronic inflammation a proliferation of the epithelium in the respiratory bronchioles may extend to form a lining within the alveolar ducts and alveoli in much the same manner as bronchial epithelium will grow into an old abscess cavity . 
 the relationship of pulmonary cancer to inflammatory foci has been studied recently by grady and stewart ( 1940 ) , de eds and cox ( 1941 ) , nettleship , henshaw and meyer ( 1943 ) , orr ( 194 7 ) , orr and bielschowsky ( 194 7 ) , and selbie and thackray ( 1948 )  . 
the effects of urethane on the mouse lung in situ indicate according to nettleship , henshaw and meyer ( 1943 ) and orr ( 1947 ) that inflam mation and adenomas arise together . 
grady and stewart ( 1940 ) and selbie and thackray ( 1948 ) disagree , and the last authors believe that in orr 's series of 433 animals which were examined after they had died from natural causes , there was a susceptibility to terminal inflammatory involvement . 
here also the evidence obtained from grafting clearly supports the contention that there is no relationship between inflammation and lung neoplasia , since the grafts which failed to produce tumours contained large areas of inflammation and those in which tumours developed rapidly were comparatively free . 
 summary , bronchogenic carcinomas have been induced from homologous subcutaneous grafts of lung tissues growing in host mice , after impregnation with either 20methylcholanthrene , 2 - acetylaminofluorene , or 2 - aminofluorene . 
 the period of tumour induction in grafts of homologous lung is considerably reduced when compared with lung tumours which develop in situ , in rodents following treatment with the carcinogen at some remote site on the body . 
 the susceptibility to tumour formation in subcutaneous lung grafts treated with the carcinogen is found to be dependent upon the age and strain of the donor as well as that of the host mouse . 
additional experimental evidence supports the view that the pulmonary alveoli are not lined by a continuous epitheliu factors influencing the survival of lung grafts without using a carcinogen were also investigated ; these showed that the successful survival of subcutaneous grafts is dependent upon the age of both the donor and host mice , together 244 e . 
 this investigation has been supported by grants to the royal cancer hospital from the british empire cancer campaign , the jane coffin childs fund for medical research , the anna fuller fund , and the division of research grants of the u.s. 
hewitt. from the john burford carlill laboratories , westminster hospital , london . received for publication may 26 , 1953 . in a previous paper ( hewitt , 1953 ) a method for the preparation and titration of single - cell suspensions of sarcoma 37 was described . 
each mouse received 4 subcutaneous inoculations of the appropriate cell dose , one in each axilla and one in each grothe new - born mice were allowed to remain with their mothers throughout the experiments . 
1 the points plotted represent the percentage incidence of palpable tumours from inocula containing various numbers of viable tumour cells ( expressed logarithmically ) calculated from the cell count of a dense suspension and the dilution factor . the points shown were obtained from the data of various experiments . although the points are insufficient in number and accuracy to disclose the true character of the curve relating log . 
cell dose and tumour incidence , they serve to show the general trend of the relationship . litters born to mothers which had been rendered completely resistant to s37 by their having regressed a tumour before pregnancy ensued gave results which did not depart appreciably from those indicated in the graph . the td50 , read from the graph , is approximately 9 viable tumour cells . this figure is less than that obtained for the titration of c3h sarcoma in c3h mice over one year old , that is , 18 viable cells . certain technical difficulties have the effect of reducing the observed percentage of tumours obtained from specified cell doses below the maximum value . 
owing to the fact that the tumours which form in the suckling mice quickly reach a size which jeopardises health and movements , some animals die with tumours in 2 or 3 of the inoculated sites before all sites have been observed for a sufficiently long period to exclude tumour formation in thethe incidence of tumours recorded for any group thus tends to be submaximal . 
a further difficulty is that a proportion of each inoculum volume often exudes from the needle track after withdrawl of the needle . cell counts and volume measurements of the exuded fluid have shown that a quarter or more of the inoculated cells are lost in this way . if these known errors were to be eliminated , the points in the graph would be shifted slightly upward and to the left of their present positions , and the td50 would be rather lower than is obtained from the results as they stand . the effect of the diluent on the activity of sarcoma cells in dilute suspensions . craigie ( 1949 ) , discussing various technical requirements for the quantitative transplantation of tumour cells , drew attention to the inimical effects of various 386 h . 
hewitt in a later paper ( craigie , lind , diluents upon the viability of tumour cells . hayward , and begg , 1951 ) an account was given of certain atypical cells which composed about 5 per cent . 
the number of various mean doses of viable 837 cells . beside each point is the number of sites inoculated at that dose level . diluents in which inoculated cells were suspended : o tyrode solution . a , 0 5 per cent gelatine in tyrode solution . * 33 per cent mouse aacitic fluid in tyrode solution . a 10 per cent ascitic fluid in tyrode solution . the suspensions used to obtain the points shown in fig . 
the order of inoculation was so arranged that the interval elapsing between the time of preparation of the dilute suspension and the average time at which the mice of any litter were inoculated was equal for all the litters . 
hewitt quantitative transplantation of s37 in mature mice of different age - groups . a single - cell suspension of s37 was titrated in three series of mice , all from the same albino stock that provided the new - born mice and belonging to the following age - groups : 18 - 25 days ; 143 - 174 days ; 268 - 296 days . 
the incidence of palpable tumours in the inoculated sites was recorded for a period of 27 days following inoculation . in table i the td50 value given by each series is given together with its limits of error . 
the difference between the youngest and the oldest mice is not significant , but the td50 given by the oldest mice is considerably lower than that given by the mice of interthis last different , however , does not attain a significant level by mediate age . the irwin and cheeseman ( 1939 ) test . 
the systemic mechanisms by which resistance is manifested are cellular and humoral . in the case of resistance to tissue grafts , it appears that cells primarily are concerned in the resistance mnechanisms ( murphy , 1926 )  . 
young mice would therefore not be expected to possess resistance against a homologous tumour by virtue of maternal serum factors reaching them by the transplacental route before birth or by the colostrum after birth . in the course of the present studies it has been observed that a litter from a mother which was completely resistant to s37 , a tumour having regressed in her before pregnancy ensued , showed the gross developthe same high susceptibility as the litters of normal mothers . ment of the lymphatic system appears to be quite advanced in new - born animals as indicated by the presence of the thymus and by the existence of lymphocytes if it is assumed that the lymphocyte is responsible for tumour in the circulation . immunity , then the low resistance of new - born mice must be ascribed to functional immaturity of the lymphatic system . the td50 given by the titration of s37 in new - born mice , as will be seen fronm the trend of the points shown in the fig . 
1 , is about 9 viable sarcoma cells . graph suggests that the percentage of tumours to be expected from an average it is of interest to note that furth and inoculum of 1 viable cell is about 7 . kahn ( 1937 ) succeeded in transplanting leukaemia to about 5 per cent . 
kahn and furth ( 1938 ) obtained only about 20 per cent of tumours from subcutaneous sites inoculated with 50 - 100 viable sarcoma cells in circumstances where there was no genetic difference between the animal in which the tumour arose and those to which it was transplanted . 
a c3h sarcoma gave a td50 of 18 viable it is evident from tumour cells when titrated in old c3h mice ( hewitt , 1953 )  . these comparisons that the results of quantitative transplantation of s37 in newborn mice of a heterogeneous strain of which the adults exhibit some resistance to small inocula , are compared with those obtained for similar tumours within a genetically homogeneous tumour - host systethe use of new - born mice therefore provides a more uniform and more sensitive system for the detection or assay of viable tumour cells in circumstances where , owing to limited facilities or to the use of genetically unknown tumours , a genetically homogeneous system cannot be achieved . it will be seen from fig . 
2 , however , that quantitative resistance increases this being so , it is likely that very differperceptibly within the first week of life . ent quantitative results would be obtained from the titration in new - born mice of tumours with a slower growth rate than s37 . in these circumstances resistance factors could produce their effects before the tumours became palpable . 
a lymphoma which occurred spontaneously in a mouse of the albino strain used in these experiments gave a td50 of over 10 , 000 viable cells when titrated in newborn mice ; krebs ' carcinoma ascitic cells gave a td50 of over 2000 viable cells . it must be concluded from the results of titrating s37 in new - born mice that the high td50 levels obtained in adult mice of the same stock ( i.e. , about 1600 ) were due to immunity factors and not to intrinsic limitations of the proliferative power of the cells . an estimate can be made of the proportion of inoculated s37 cells which are capable of continued proliferation if it is assumed that such cells are not subject to any hazard affecting their proliferation once they have been successfully in these circumstances the dose - response curve deposited in the host tissues . would represent the chances of getting one or more " taking units " in random samples ( inocula ) taken from suspensions containing different mean densities of 390 h . 
1 , a suspension which gives 37 per cent of negative sites ( 63 per cent of takes ) contained a mean density of about 17 tumour cells per inoculum , and this evidently constitutes a single " taking unit . " thus , when it is assumed that there are no influences at the inoculated site which inhibit continued proliferation of a cell intrinsically capable of giving rise to a palpable tumour , then the results reported indicate that such cells are present in a proportion of about 1 : 17 ( 6 per cent ) of the population of cells designated as living s37 cells on the grounds of their resistance to staining with trypan blue the frequency with which abnormal mitoses and and their diameters ( > 9 , )  . cellular pleomorphy are found in rapidly growing tumours would seem to indicate that there may be a continuous production of cells which , though alive , are various observations have been intrinsically incapable of indefinite proliferation . fischer ( 1935 ) was unable to cultivate made which suggest that this is the case . solid s37 in vitro , and concluded that dying cells exceeded living cells in this lasnitzki ( 1952 ) found that the majority of s37 ascites cells failed to tumour . she found also that one - third to two - thirds of the mitoses seen divide in vitro . since it is unlikely that all mitotic in the ascitic cells in vivo were abnormal . abnormalities are visible , it is possible that the proportion of mitoses which are koller and smithers ( 1946 ) give experiabnormal in vivo may reach 50 per cent . mental proof that loss of chromosomes or of chromosome segments leads to the death of the cell . 
on the other hand , there is evidence that cells with a defective chromosome complement may survive and divide under conditions where contiguity between the cells is preserved , while being unable to do so when isolated these considerations favour the assumption from one another ( koller , 1947 )  . that a significant proportion of the s37 ascitic cells are unlikely to be capable of furthermore , if the cells should indefinite proliferation and tumour formation . be dependent upon one another for a stimulus to divide , dilution may reduce the proliferative power of an inoculum , not by damaging individual cells , but by abolishing essential mutual influences between the cells . 
quantitative transplantation of s37 in new - born mice of a heterogeneous strain gave results similar to those obtained for the transplantation of a c3h sarcoma in adult c3h mice . 
nielsen. from the danish cancer registry under the national anti - cancer league , copenhagen , denmark . received for publication april 30 , 1951 . in comparing mortality figures for cancer from various countries for the years around 1938 , clemmesen and busk ( 1947a , 1947b , 1948a , 1949a , 1949b ) found that while denmark ranked third for total mortality from cancer , her figures for females were highest among the countries investigated , surpassing even switzerland and england , for which countries the total mortality was higher . appeared that the high mortality figures for danish women were caused primarily by a high mortality from cancers of " accessible site . " from figures given in the series of articles quoted , it is seen that the incidence of cancer as expressed by the figures from the danish cancer registry for 1942 to 1944 was higher for copenhagen than for the provincial towns , which in their turn exceeded the incidence for rural areas . consequently , in the following paper the incidence of cancer in copenhagen will be studied separately , with particular reference to social conditions , social class being expressed in terms of annual house rent for various subdistricts of greater copenhagen . it is an established fact that expenditure on housing is a more reliable indicator of the social status of a family than the annual income of the breadwinner . 
the level of house rent in copenhagen was fixed during the period studied , and the wartime shortage of housing which prevailed during the entire period must have restricted the number of changes of residence . 
hence several factors working together tended to stabilize some of the variables which would be inclined to disturb a study such as this . the city of copenhagen , the capital of denmark , has one million inhabitants , another million live that is , about a quarter of the total for the whole country . in the provincial towns , and two millions in rural areas . medical facilities in copenhagen left very little to be desired during the period examined , in spite of current political and military events . 
nielsen the reference of cases of cancer to distinct geographical location has , however , inforin the present study been made without regard to the place of treatment . mation on cases was collected by the cancer registry , and each case was referred to the subdistrict corresponding to the address of the patient when first seen in hospital for cancer . 
the cancer registry collects notifications from hospitals all over denmark of all cases of cancer seen , and separately of all post - mortem examinations performed on cases of cancer . for patients not entering hospitals it is assumed that death certificates will give sufficient information , but it will appear that such cases amount to rather insignificant numbers in copenhagen . further details of the activities of the danish cancer registry have been given elsewhere by clemmesen and busk ( 1948b , 1948c ) clemmesen , busk and nielsen ( 1949 ) , and clemmesen ( 1950 , 1951 )  . the subdivision of the greater copenhagen area into 22 subdistricts used for the present study had originally been worked out for various administrative purposes , and proved useful because detailed figures for the distribution of the population by age were available for each subdistrict . 
the wealthy boroughs of frederiksberg and gentofte had , however , to be treated as separate entities because ot the absence of such information for their subdistricts . after a careful analysis of the figures for each site of cancer in each of the 22 subdistricts , it became possible to collect subdistricts within the same range of house rent into however , the average annual house rent of five major classes or " districts . " each subdistrict is given together with the relative values for cervical , mammary and pulmonary cancer in table v . in order to describe the material from a medical point of view table i has been worked out . 
we denote the observed number in subdistrict v comprising all age groups . by l we denote the total number of person - years of exposure , and by c the addition of the subscripts v computed number of persons developing cancer . and s to l and c has the same meaning as described for 0 . if the morbidity from cancer were identical for all subdistricts of the town , we would expect the number of cancer cases at a given age to be distributed on the subdistricts in the same manner as the number of person - years of exposure for a given age . consequently we obtain the computed number c , 8 from the equationlvs . and this number should be compared with the observed number ov.. now the number ov , , is usually small ; we therefore take this number for all age groups and make the comparison for all of them at the same time . 
nielsen pondingly the incidence of cervical , mammary and pulmonary cancer is given as a percentage of the values computed for each subdistrict , with full allowance for differences in age distribution of the population o.. 
nielsen between the social status of the various subdistricts and the incidence of cervical cancer demonstrated in table v is striking to anybody familiar with the city . the irregularity presented by district ii , which mainly consists of the borough of frederiksberg , showing an unexpectedly high frequency of cervical cancer , can by no means be ascribed to a particularly high birth rate in the borough , since this rate is lower than for gentofte , and also lower than the average for the - ~~~~~.... . 
from these areas patients with cervical cancer are centralized for treatment in the radiumstations of the anti - cancer league , situated in the towns of copenhagen , aarhus and odense . 
nielsen connection with the development of cancer , it should be pointed out that the cases have been puboccurrence of cervical cancer in virgins is questionable . lished of cervical cancer in children ( heckel , 1950 ) , but these have been adenocarcinomata , so that it may be desirable in statistical work to separate this group from squamous cell cancers of the cervix . 
the mincer is shaken immediately to disperse the mince if the coarse plunger has been used the cap and operating in the suspending fluid . screw are detached and the fine plunger is inserted . tlle cap and screw are replaced and mincing is completmed . the suspension may contain coarse fragments of fibrous tissue or portions of iiiince which have clotted before dispersal in the suspending fluid . these may be removed either by l ' ow speed centrifugation , or by filtering the suspension througli a column of glass ballotini of suitable diameter . the mincer , which is illustrated in fig . 
1 , is the sixth of a series desigiied to all models have proved most satisfactory for operate with grooved plungers . the purpose for which they are intended , and it might be suggested that this tvpe of mincer will , for special purposes , be suitable for preparing suspensions of manimalian tissue or fowl embryos infected with certain viruses or bacteria . i wish toacknowledge my indebtedness to w . 
it is to ' be expected on theoretical grounds that temperatures below the fi - eezing points of the eutectic mixtures of the inorganic salts would favour survival of activitv . 
an equallv pending tumour mince in drying experiments . important reason for the use of dexlrose suspending fluid . tissue mince suspended in saline or ringer solution and frozen m a thin laver progressivelv consequentlv the dr , % - mg process becomes separates from glass during drying . greatlv impeded because of the low rate at which thermai energy is conducted across the intervening vacuuwhile dried fragments mav break off and mav be 22 ' c . 
the thermal conductivity of the dried material is adequate for the rapid drying of thin layers . water is removed from the tumour suspension by the low temperature con79 ' c . 
presents no difficulty , but there densation method . are technical problems in maintaining the drying tissue at a constant temperaif the lead from drying flask to condenser is of sufficient diameter ture level . and the vacuum is adequate , the problem is not one of cooling , but of supplying the maximum of thermal energy for rapid evaporation without heating the frozen it was considered undesirable mass above the chosen maximum t - i.imperature. to attempt to control the temperature of the drying mass on the basis of thermocouple readings . there is no guarantee that a thermocouple junction can be placed at that point in the frozen mass which will be the last to dry . 
the arm of the u - tube distal to the pump is extended horizontally and then downwards , to form the exit tube from the condenser flask . this exit tube is furnished with a ground glass taper which fits the neck of the flask . 
the stirrer rod is attached bv means of a slotted clamp which faeihtates assemblv with the thermos bath and drying flask . the rubber ring which drives the disc if the variable speed gear is mounted on a wheel which can be moved along the horizontal bar . this bar is mounted on two spring - loaded arms . 
a pliotographically reduced protractor scale is cemented to a piece of perspex 2 - 5 x 13 x 65 mand the pivot is centred at the origin of this scale . the vane is a piece of photographic dry mounting tissue 3 x 8 mm . , which is attached by shellac to a piece of fine copper wire 0 - 01 min diameter . 
the combined weight of vane and wire is 3 - 7 mg . , so that the vertical component of its weight at a displacement of v from its zero position is 0 - 065 mg . ( 4 ) vibration dampers . - owing to the design of the glass - drying system and the use of a sensitive vapour flow indicator , it is necessary to check the slight vibration arising from the electric motor driving the pump . 
the distribution of the frozen rnince is readily controlled if the level of ethyl cellosolve in the freezing bath is adjusted so that the flask will float with its neck resting on the rim of the thermos jar and can therefore be spun quickly by hand . the temperature of the freezing bath may it has not yet been determined whether a preliminary 30 ' c . 
shown bv irregular movements of the indicator between 3 ' and these bursts last for a few seconds , and are separated bv shghtlv longer after the indicator has re - ached zero . 
grow and form large embrvomas which persist for months or indefinitely . the following series of experiments was , undertaken to gain knowledge of the beha - viour of such embrvo grafts under various conditions . 
cook. from the bland sutton institute of pathology and the barnato joel laboratories , middlesex hospital , london , w.1. received for publication april 5 , 1951 . the effects of high - frequency electric fields on living tissues , micro - organisms and viruses have been extensively investigated in the last fifty years . short - wave fields were first applied to animal tumours by schereschewsky ( 1928 ) using a transplantable mouse sarcoma , and by schereschewsky and andervont ( 1928 ) working with the rous fowl sarcoma ; these workers claimed to have produced complete regression of a number of the tumours following their results , together with those of subsesubjection to electric fields in vivo . quent workers who have reported investigations into the effects of short waves on animal tumour tissue in vivo and in vitro , were reviewed by dickens , evans and weil - malherbe ( 1936 )  . 
from a consideration of previous studies and as a result of their own extensive investigations performed with tumour tissue to which short - wave fields were applied both in vitro and in vivo , dickens , evans and weil - malherbe ( 1936 , 1937 ) concluded that , when heat effects were eliminated , ultra - short waves had no action on tumours or isolated tissues ; all the findings reported were , in their view , due to the action of heat . the many studies concerned with the effects of high - frequency electric fields on bacteria , bacterial toxins , viruses and unicellular protozoa which followed the original experiments of d ' arsonval and charrin ( 1896a , 1896b ) have been reviewed by burton ( 1949 )  . in commenting on the extreme variation of the results reported , burton ( 1949 ) emphasized that it still remained to be determined whether or not any action of the short waves existed apart from heating effects in the suspending medium . a recent claim was made by nyrop ( 1946 ) to have discovered a so - called specific effect distinct from heat effects , when pulsed fields at a frequency of 20 mc / s were applied to bacterium coli cultures in a fluid medium , the virus of foot and mouth disease , and unspecified tissue cultures . this claim was been criticized on the grounds that energy absorption by ionic and dipolar processes in the medium immediately surrounding the bacterium or virus might have resulted in a local temperature rise sufficiently high to destroy it , even though the general temperature of the test specimen were kept below the lethal level ( jackson , 1946 )  . 
they were between 8 and 14 weeks old when inoculated and belonged to two of the institute 's lines , which have been described by greenwood , blyth and carr ( 1948 ) , or crosses derived from them ( intensity , breeding , breeding hen x intensity cock , intensity hen x breeding cock )  . 
both the age at which the birds were inoculated and their distribution within the various line groups were determined by the exigencies of the supply . preparation of material for irradiation . for each experiment a bird with a large actively growing sarcoma of anything from 8 to 35 days ' growth from the date of inoculation was selected as a source of tumour material . 
the speed and the duration of the run of this machine was varied with each individual tumour , but was so arranged as to give homogenization of the resulting the tissue ; disintegrated material was placed in tubes and centrifuged very lightly ( in a horizontal centrifuge accelerated to 2000 - r.p.and at once decelerated ) , so as to bring all the contained air to the surface as a sharply demarcated layer of foam , which was then removed . 
the material obtained in this way , referred to in this paper as " disintegrated tumour , " was either mounted at once for irradiation , as described below , or was used in the preparation of other material for irradiation as follows : this was usually achieved in less than 1 minute . where a preparation of disintegrated tumour largely free of cells was to be irradiated , it was made by placing 4 c.c. 
the filings and tissue debris were separated off after the period of shaking by centrifuging in a horizontal centrifuge for 5 minutes at 2000 r.p.the supernatant fluid so obtained was drawn off and centrifuged again for 15 minutes at 6000 r.p.in order to throw down at least the greater part of any remaining cells . 
the supernatant fluid resulting from this final centrifugation , designated " virus suspension " , was drawn off ready for irradiation . water flow calorimeter c02 ice specimen standin wave icatoa from magnetron jacket for freezing mixture specimen at centre of waveguide ( maximum field strength ) 1 1 + 1 specimen at side of waveguide ( field of low intensity ) fig . 
with the experimental conditions used this peak field was given by1016v / a volts cm . - 1 , where a - average power in watts . where a section of the guide was filled with carbon dioxide ice the field at the central point of the section depended as well on the length of the section filled and on the dielectric constant of the carbon dioxide ice . this latter had been found ( in a separate experiment ) to be 1.6 at 3000 mc / s , and the length of the guide filled with the carbon dioxide ice was adjusted so as to be half the wave - length of the radiation in the ice . 
under suic ' h conditions the block of carbon dioxide ice was non - reflecting and the field strength at the central point was given bythe field in a frozen specimen at the central point of the carbon diqxide ice blbck differed from that in the ice in the absence of the specimen , since the dielectric constant of the frozen material differed from that of the ice . although the dielectric constant at 3000 mc / s of disintegrated tumour or virus suspension at room temperature is high ( between 40 and 80 ) , in the frozen state it drops to the region of 2 , not far removed from the dielectric constant of the carbon dioxide ice . 
the overall exposure time in each experiment was thirty minutes , corresponding to 9 x 105 pulses of 0.6 x 106 seconds ' duration each . the total time for which the field was operative was therefore 0.54 seconds in each thirty - minute exposure . 
cook surrounding the virus could take place ( experiment 1 , irradiation without cooling ) , and under conditions where precautions had been taken to prevent such energy absorption ( experiments 2 , 3 , 4 , 5 , irradiation with cooling )  . it is considered that the method of cooling employed was such as to keep the temperature of the material exposed to irradiation below 70 c . exposure to a temperature of below 70 c . 
on the other hand , absorption at a resonant frequency increases as the such absorption does not occur in water at microwave temperature falls . frequencies , but may possibly take place in large molecules or parts of them . thus , in the irradiation of frozen material , absorption by ionic conduction and dipolar orientation was avoided . 
at the frequency of 3000 mc / s . the results in table i can be attributed to energy absorption by ionic and dipolar processes in the medium surrounding the virus causing a general temperature rise well above the lethal level . thus the results of the present experiments show that any effects of the microwave field upon the rous no . 
where such heat production was eliminated , microwaves of a frequency of 3000 mc / s were found to have no demonstrable effect on the virus of the rous fowl sarcoma as judged by changes in its tumour - producing activity . 
where heat production was allowed to take place the tum6ur - producing activity was abolished . the expenses of this investigation were borne by the british empire cancer campaign . the authors wish to express their thanks to professor j . 
howatson. * from the cancer research department , royal beatson memorial hospital , glasgow . received for publication july 6 , 1953 . several attempts have been made to purify and isolate the particulate agent or virus associated with mammary carcinoma in certain strains of mice , with a view to its identification and the study of its morphology by electron microscopy . the conclusions reached by different observers , particularly about the average size of the particles identified with the active agent , have been considerably at variance . passey , dmochowski , reed and astbury ( 1950 ) and dmochowski , and passey ( 1952 ) have described an extensive investigation in which biological tests for the presence of the agent in extracts of tissues and milk from high and low cancer strain mice were correlated with the appearance of the same extracts in the electron microscope . 
they conclude that the tumour - inducing activity is associated with typical particles of diameter 200 - 300 a , preparations of high activity containing large numbers of these particles and inactive extracts containing none or very few . graff et al ( 1949 ) , using as starting material milk from riii and c57 mice , and c57 mice foster - nursed by riii mothers , claim to have isolated from infected milk , after treatment with chymotryspin and differential centrifugation , particles of diameter 750 - 1000 a which they regard as the mouse mammary carcinoma virus . 
 ( 1950 ) but this could hardly account for the large difference in size . porter and thompson ( 1948 ) carried out an electron microscope investigation of epithelial cells grown in tissue culture from spontaneous and transplanted adenocarcinoma in c3h mice . 
they found that in three out of six preparations spherical particles were present in the cytoplasm of the cells . these had a double structure - a dense centre portion of diameter about 750 a and a less dense outer zone of diameter approximately 1300 a . 
they conclude that their findings are consonant with the view that the particles represent the milk agent . huseby , barnum and bittner ( 1950 ) , on the other hand , observed particles of diameter 500 - 2500 a in extracts of milk and mammary gland tissue but were unable to distinguish in the active extracts any distinctive particles which could be identified with the virus . in view of the long period required to obtain results from biological tests for the agent , any method of assaying rapidly the activity would be of great value in experimental work . 
howatson it was thought that a new attack on the problem involving a direct comparison of extracts of tumours from agent - carrying and agent - free mice of the same strain might give a conclusive answer . for our experiments we were fortunate in having available , through the courtesy of b . 
a commercially produced atomiser or spray gun operated from the high - pressure air line was found to be satisfactory the specimen was deposited by directing a fine spray of droplets of the extract to be examined on to filmed specimen mounts . 
each droplet is a representative sample of the extract and most are small enough to be included in a single micrograph . thus to obtain information about a given extract it is necessary to photograph only a few droplet patterns instead of searching the whole field . 
as far as possible the treatment of agent - containing and agent - free tumours was identical . a weighed amount of tissue was homogenised for a few minutes in a glass homogeniser , the suspending fluid ( usually distilled water ) being added slowly to give a final tissue concentration of 2 per cent . 
both extracts contain much particulate material together with fragments of mitochondria , collagen fibres and other cellular debris . these larger fragments can be removed if desired by further centrifugation , leaving an array of macromolecular particles on a background composed of low molecular weight material , which is not generally resolved by the electron microscope . 
the particles are approximately spherical and , although covering a range of size , are predominantly of diameter 250 - 300 a , the size attributed to the milk agent by dmochowski and passey ( 1952 )  . the particle - size distribution based in each case on the measurement of 200 particles , is shown in histogram form in fig . 
the number of particles present in a given extract depends somewhat on the type of tumour , the efficiency of homogenisation and the centrifugal forces employed but provided the simple standard procedures outlined were adhered to , the variations were small . despite careful search , it was not found possible to detect any significant difference in the number , size or appearance of the particles present in the droplet patterns obtained from extracts of agent - containing and agent - free tumours . the failure to observe any difference in the tumour extracts is readily understood when similarly prepared extracts of normal organs are investigated . nearly every case examined , including spleen , liver , marrow , brain and lymph 396 a . 
14 ( c ) shows that diameter . in size - distribution , these presumably normal particles do not differ significantly from those derived from tumour tissue . it is apparent that simple fractionation procedures are not sufficient to effect a separation enabling the pathogenic particles to be distinguished from the numerous cell particulates of similar size and shape which are also present . 
14. - size distribution of particles in extracts of ( a ) agent - containing mouse m ary tumour , ( b ) agent - free mouse mammary tumour , and ( c ) normal mouse spleen . the field of the smaller animal viruses , where it has been satisfactorily overcome in only a few cases . 
an attempt was made to differentiate in this way between normal and infective particles by studying the action of the enzymes trypsin , chymotrypsin , ribonuclease and deoxyribonuclease on extracts of agent containing and agent - free tumours . 
the buffer salts , which crystallise on drying , can fairly readily be distinguished from organic material , but the latter shows a tendency to aggregate in the presence of electrolytes . this effect had previously 398 a . 
a comparison was made between extracts of the mill hill 2 endothelioma which has all the attributes of a " virus " tumour and the chemically - induced grch 16 tumour which in addition rous no . 
1 sarcoma and has no such " filterable " properties . biological tests for the infectivity normal chicken tissue extracts were examined . of the various preparations were carried out in many cases . the methods adopted were similar to those previously described , and need not fig . 
extracts of the first type regularly excite tamours on injection into susceptible birds , whereas the second type of extract , though apparently of similar particulate content , is these micrographs may be compared with fig . 
9 , which completely innocuous . shows an extract from a normal chicken spleen . it is again evident that the infective particles , if present , are masked by the large quantity of other particulate material which occurs in normal as well as tumour tissue extracts . 
the lower limit of size ( 600 a ) given by claude ( 1946 ) appears to be arbitrary . certainly most of the particles observed were smaller than this , though some shrinkage during desiccation may occur . 
the presence of still smaller cytoplasmic particles in cells fixed by osmium tetroxide has recently been demonstrated by high resolution electron micrographs of ultra - thin sections ( eaves , 1953 , private communication )  . there is no doubt that the particles observed in the present experiments are products of the disintegrated cells , the spraying method giving consistent and conclusive evidence of their presence in the extracts . 
the dissolving action of trypsin and chymotrypsin is a strong indication that they are protein in nature . the crystalline trypsin used was tested for the presence of particulate material by spraying on to coated specimen mounts a solution 100 times as strong as that used in the experiments . 
12 is shown a partially disintegrated mitochondrion with what appears to be an extrusion of particulate material . a group of mitochondrial membranes largely devoid of contents is illustrated in fig . 
it seems very probable that some of the particles observed in tissue extracts are derived from such disruptions . it is clear that the range of size of the normal cell particulates covers that of the smaller animal viruses . this is a major difficulty in the isolation of any presumed virus by purely physical methods such as differential centrifugation or in chemical composition also , the microsomes are found to be strikfiltration . ingly similar to certain known viruses , so that attempts at chemical or enzymatic separation may also fail . there remains the possibility of using the highly specific methods of serology , though even these may not distinguish normal from pathogenic particles unless the latter are of extraneous origin . the difficulty of identifying tumour - inciting particles , particularly the milk agent , by electron microscopy is enhanced by lack of independent data on size . estmates have been made by finding the centrifugal force required to clear the supernatant of infectious material . there have also been some attempts to deduce the approximate size of the milk agent by measurement of sedimentation rates in an ultracentrifuge ( kahler and bryan ( 1943 ) )  . 
the presence of normal particles and aggregates makes the interpretation of such experiments somewhat doubtful , but the evidence is in favour of the association of the infectivity with rather small particles of molecular weight 3 - 5 million , corresponding to a particle diameter of at most a few hundred angstroms . it is remarkable that no attempts appear to have been made to determine the approximate size of the milk factor particles by means of gradacol membranes , as has been done for example in the case of several fowl tumour viruses . 
by this method it should be possible to determine conclusively whether the infectivity is associated with particles in the large ( > 1000 a ) or small ( < 300 a ) size range . it is clear that further work is necessary to establish the elementary physical properties of the tumour viruses . 
the examination of tissue culture cells and of thin sections of fixed tissue may give valuable information , but is not likely to be conclusive because of the difficulty of relating the observations to biological tests . on the other hand , the method of extracting homogenised tissue , while convenient for biological testing , presents problems arising from the presence of much contaminating material which can only be satisfactorily solved by the discovery of some action highly specific to the virus , which can be used for its isolation . in conclusion it is emphasised that the presence in tumour extracts of particulate material in the size range of the smaller animal viruses is no indication that the particles are in any way related to virus activity , unless it can be conclusively 400 a . 
bartholomew 's hospital , london , e.c.l. received for publication february 11 , 1952 . the use of the fluorescence spectrum by mayneord and hieger led to the detection of 3 - 4 - benzpyrene in coal tar and to the isolation of this compound recently goulden and tipler from pitch ( cook , hewett and hieger , 1933 )  . ( 1949 ) identified it by the same means in domestic soot , which is carcinogenic ( passey , 1922 ) , and their method has been extended to samples of smoke drawn from the atmosphere . 
the apparatus is described fully in " atmospheric pollution in leicester " ( leicester , ' atmospheric pollution , ' 1945 ) , and generally consists of a small electric motor drawing air from outside a building through a filter - paper , upon which most of the suspended smoke is deposited , followed by a bottle containing h202 for the determination of so2 , and a gas meter to measure the volume of air . filter - papers are changed daily , and the " shade " of the resulting stain , as compared with a calibrated " scale of these data are collated shades " , is taken as a measure of the smoke collected . on monthly sheets showing the daily volume of air sampled , the shade number and smoke conceiltration deduced therefrom , with monthly summaries . 
vvaaller in the main experiment acetone extracted up to 50 per cent more benzpyrene . was used , and each extraction was continued until ( after about 4 hours ) no further fluorescent material could be extracted . 
the resultant golden - yellow solution was passed through a short column of activated alumina ( 3 x 1p4 cm . , spence type h ) , which removed any finely divided particles , traces of water , and certain after running more acetone through the column of the unwanted hydrocarbons . the resultant solution was evaporated , leaving a yellow oily droplet with a brilliant blue - violet fluorescence in ultra - violet light , which was dissolved as far as possible in several successive lots of boiling petroleum ether ( 60 - 80 ) ; the insoluble part was redissolved in acetone and retained separately to be checked for the absence of benzpyrene . 
the solution at this stage was pale straw - coloured , with a strong bluish fluorescence in ultra - violet light , and on passing through a column of alumina ( 8 x 1 - 4 cm . ) previously washed with petroleum ether , nmost of the fluorescent material was adsorbed as a narrow , blue - fluorescing band near the top of the column . development with petroleum ether , followed by a mixture of 30 per cent benzene in petroleum ether , produced a series of rather diffuse bands , distinguishable in ultra - violet light by their slightly differing fluorescence . 
 " osira " lamp with separate wood 's glass filter , and spectra were recorded on a hilger e.51.7 spectrograph , using a 0 1 mslit and 2 - mninute exposures with ilford " zenith " plates . all final solutions were prepared in petroleum ether , and no precautions were taken against oxygen quenching ( bowen and williams , 1939 ; miler and baumann , 1943 ; weilmalherbe , 1944 )  . schoental and scott ( 1949 ) give the fluorescence bands of benzpyrene in petroleum ether as a main system at a 4032 , 4272 and 4535 , with subsidiary systems at a 4082 , 4310 and 4149 , 4367 . 
with the weak solutions used here , only those at a 4032 , 4082 , and 4272 appeared in the negatives , and not all of these in reprothe group of hg lines around a 3650 appears in all photographs , and ductions . serves as a useful reference line . 
the position and intensity of the bands varies with the solvent ( chalmers , 1938 ; sambursky and wolfsohn , 1940 ) , but at this stage the difference between petroleum ether and its mixtures with benzene is in most cases , the spectrum of benzpyrene was visible in eluate unimportant . 30% b and not in the others . these former solutions still contained much material other than benzpyrene , some of which fluoresces in the same wave - length region as benzpyrene . 
3. - yearly cycle of benzpyrene at london ( county hall )  . the variations from month to month at any one station are greater than the difference between stations , so that a mean value over at least one year is required for any comparisons . table ii shows appreciable variations from one year to the next ; an average over something like 5 years would be required to give reliable figures . 
a general discussion on recent changes in pollution is included in the 26th report in this series ( ' atmospheric pollution , ' 1949 )  . at sheffield there is less variation during the year than at county hall , suggesting the influence of industrial smoke containing a lower proportion of benzpyrene than domestic smoke , coupled perhaps with a greater use of domestic the smloke at cannock is primarily from coal mines fires during the sumrmer . and domestic fires and shows the highest proportion of benzpyrene , with a range intermediate between that of county hall and sheffield . the seasonal values at the whole range of stations in the ntain confirm and winter concentrations exceed summer extend the conclusions drawn above . ones by a factor of three or four times on the average , and with one exception the proportion of benzpyrene in the smoke is also greater everywhere in the winter by a factor of just under two . the highest values throughout are shown by beckton , which should be regaided apart as a special case . here there is much local pollution from the adjoining gas works , which would appear to contain at least as niuch benzpyrene as domestic smoke since the proportion of benzpyrene in the smoke persists at a level above the average throughout the year . however , the effects of such abnormal conditions fall off rapidly as the distance from the source increases , for at crossness , only two miles a.way , the nmean annual concerntration is one of the lowest observed . these results serve also as a warning r . 
waller that large variations in betnzpyrene concentration can occur even within very short distances , so that to assess the mnean concentration within a town would require readings from a large nunmber of stations . hence the position of a town in the following list , arranged in descending order of concentration , indicates only the conditions close to each station , and not necessarily those in the town as a whole : london ( county hall )  . sheffield leicester bumley bilston cannock hiull bristol  . 
one nmight expect the concentration near the centre of a town to bear some relationi to the population , although many other local conditions play their part . fact , the first six towns are very nearly in descending order of population , and the low position of the large cities of hull and bristol is perhaps noteworthy . results from stations in many other towns not investigated might well be higher than most of those quoted . 
the limitation of an ordinary filter - paper is that it soon becomes blocked with smoke , and must be changed at intervals . the soxhlet thimble mentioned above , when used in series with a normal filterpaper , forms quite an efficient smoke collector , and will retain very much more smoke than a filter - paper alone . however , a more compact filter which serves the same purpose can be made from a pyrene filter disc ( type 2130 ) backed with an ordinary filter - paper . such filters required prolonged washing with acetone in a soxhlet apparatus before use for benzpyrene work . 
they can be used for collecting smoke at a low rate over a long period without being changed , but are not suitable where it is required to weigh the smoke collected , as fibres frequently drop out of the filter during use . 
the use of filter - papers of various kinds has been discussed by bourne and street ( 1950 ) , and silverman and viles ( 1948 ) have described an apparatus using pleated filter - papers . filters consisting of salicylic acid crystals lightly packed in a brass tube have also been used , but again difficulties arise in weighing the smoke , as the usual method of volatilising the acid at about 1050 c . 
a description of various air - sampling devices used in industry has been given by silverman ( 1948 )  . for rapid determinations over a short period some form of impactor is useful ( may , 1945 ; sonkin , 1946 ) , as the smoke can be collected free from all other material on glass slides . samples of smoke weighing a few milligrams were collected in a crude single - jet impactor , but as the smoke began to pile up , so the efficiency of the system dropped , thus limiting its capacity . 
waller air - conditioning plants in hospitals and public buildings , and filters on ment . air compressors in some industrial concerns , collect much " suspended impurity " from the air , which may be used for benzpyrene determinations , although it is often difficult to free the smoke from the filtering medium in order to weigh it , and in general the volume of air from which it has been drawn is unknown . 
a large sample was obtained from the compressed air plant at beckton , and has been used in pilot experiments to determine a suitable method of dealing with to extract the tarry matter without the very finely divided smoke bulk material . particles entering the solution , the sample was contained in a soxhlet thimble completely surrounded by filter - paper powder inside another thimble . since the smoke at beckton is not representative of normal conditions , no final results were obtained from it , as a more normal sample is now available from the royal festival hall , london . some suspended matter is removed from the air by a natural thermal precipitator action , in which warm air rising up the side of a building deposits some of its smoke on projections on the wall . 
a small deposit of soot often builds up near the end of exhaust pipes , and this is probably similar to the material dispersed into the atmosphere . samples taken from a motor cycle , two cars and two diesel compressors have all shown the presence of benzpyrene . uncertain , for the question of whether or not it is present in the fuel or lubricating oil used depends on their source and the treatments to which they have been subjected . 
no benzpyrene was found in particular samples of " pool " petrol , but , after the separation of large quantities of interfering substances , it was detected in a sample of lubricating oil . however , conditions in the combustion chamber may be suitable for the production of benzpyrene , so that it might be emitted in any case . 
as an attempt to identify it in domestic soot proved unsuccessful , this may indicate that a small proportion of smoke collected in towns comes from internal combustion it may also be of importance to note that whilst the particles in coal engines . smoke are distributed over a large range of sizes , those in the exhaust of internal combustion engines are concentrated in a limited range of small sizes , and that this may be quite near to the range which undergoes maximum retention in the lung ( wilson and lamer , 1948 ; landahl and herrmann , 1948 ; hatch and hemeon , 1948 ; davies , 1949 ; owens , 1923 ; boyland , gaddum and macdonald , 1947 )  . hence any further inquiry into this subject might benefit from the segregation of smoke into different size - ranges prior to the estimation of benzpyrene . for this purpose a large capacity cascade impactor would provide a suitable means of collecting the smoke . amongst miscellaneous substances tested for benzpyrene was a sample of the " coke " obtained as a by - product in the refining of petroleum . this showed a trace of benzpyrene which , if not present in the crude oil , may have arisen in a cracking process . the benzpyrene found in certain rubbers ( falk , steiner , goldfein , breslow and hykes , 1951 ) is attributed to the carbon black used as a filler . the literature on the carcinogenic action of tobacco tars and smoke contains somewhat conflicting reports , and has been summarised by flory ( 1941 )  . 
some of the apparent differences may be due to differing conditions of combustion and distillation ; only those simulating natural smoking are of any practical interest . in view of the influence of cigarette smoking upon the incidence of lung cancer ( wynder and graham , 1950 ; doll and hill , 1950 ) a few experiments were carried out on cigarette smoke , with negative results . however , one must emphasise that it was very difficult to free cigarette smoke extracts from relatively large amounts of a yellow substance soluble in petroleum ether and strongly absorbent to ultra - violet light , so that benzpyrene may possibly have been missed in these experiments , which were carried out partly on cigarette ends collected from several smokers who had avoided any contamination of them , and partly on smoke collected by a filter of salicylic acid crystals loosely packed between cotton - wool in a short glass cigarette holder . 
the former method represented normal smoking , and assumed that some of the smoke which had passed through the end would have been retained there ( mulinos and cockrill , 1938 )  . 
none has been found in cigarette smoke . this investigation has been rendered possible only by the enthusiastic cooperation of a number of individuals , including the following and their respective staffs : a . 
as this finding was of great importance not only to the general problem , but more particularly as a possible test of the validity of conclusions which were being formulated , it was decided to confirm their results . initial casual observation by nettleship and henshaw was made on female mice of the c3h strain , which normally shows a low incidence of pulmonary tumours , in an experiment in which urethane had been used as the anaesthetic . 
the urethane group in the first experiment consisted of 100 mice , the other three groups of 60 mice each , and 60 untreated mice were observed over the same period . 
the mice were examined post mortem as they died during the course of the experiment , or when the survivors were killed 185 days urethane 12 per cent ; 312 j . 
the second experiment was made on 100 mice similarly treated with urethane ; no other substances were used , in view of the negative results of the first experiment . in this experiment at the end of treatment the mice were allowed to survive until they died , with a view to assessing the persistence and growth of the adenomata . unfortunately enteritis and cannibalism reduced the amount of histological material below what was hoped for in both experiments , but not to such an extent as to make it inadequate . 
when the nodule projects above the pleural surface , is smooth and uniformly rounded , and greyish - white in colour or semi - translucent , it can be regarded with some confidence as a formed adenoma , but only a proportion of the fiat nodules will prove to be adenomata . 
at a later stage the lungs showed induration from chronic inflammation , more often than not accompanied by acute consolidation of one or more lobes . it was at this stage that subpleural nodules began to appear in numbers , and the pale miliary spots on a deep red background often presented in the latest stages , after treatment had been discontinued , a striking picture . the lungs were free from consolidation , but showed distortion of shape as a result of emphysema . 
not only is it possible to trace the stages of development of a tumour in the chronic foci of inflammation and collapse , but the striking difference in the incidence of pneumonia with urethane as compared with the other anaesthetic substances used is highly suggestive . since this work was done , larsen ( 1946 ) has also shown that urethane is so far unique amongst narcotic compounds tested ; he used a larger selection of such substances than was employed here , but without finding any other which produced a significant increase in pulmonary adenomata . in their original communication nettleship and henshaw ( 1943 ) did not appear to be impressed with the evidence of inflammation . 
they found that conditions such as bronchiectasis , purulent bronchitis and acute pneumonia were distributed alike among the experimental and control animals . they are emphatic that lung tumours and pneumonia were never seen together , it is possible that this difference though they occurred apart from each other . of interpretation may depend on what is meant by the term pneumonia . 
orr. from the department of experimental pathology and cancer research , university of leeds . received for publication july 19 , 1947 . attention was drawn to the frequency of spontaneous tumours in the lungs of mice by tyzzer ( 1907 - 8 , 1909 ) , whose description of their histology has required but little amendment . 
he has shown that bacterial growth can be understood in terms of certain simple mathematical relationships , in spite of the fact that the molecular mechanisms involved are extraordinarily complicated . in this paper an attempt is made to see if such an approacli may help to throw a little light on the problem of tumour formation and growth . 
a brief review of carcinogene8i , 3 . the various ways of producing cancer have been reviewed in a recent paper by boyland ( 1952 )  . but it will help for the purposes of the present communicatioii to provide a summary of the results . ( a ) chemical carcinogens . - the first chemical compound to be identified as a carcinogenic agent was 1 : 2 : 5 : 6 - dibenzanthracene ( cook , hieger , kennaway and mayneord , 1932 )  . since that time , the polycyclic hydrocarbons have been investigated systematically from this point of view . 
a certain degree of specificity has been observed and it has been correlated to some extent with the presence of a region of high electron density ( k region , schmidt , 1939 ) , within the molecule . some recent work has suggested , however , that the carcinogenic activity of the polycyclic hydrocarbons may be related in part to their ability to undergo autooxidation and liberate free radicals ( alexander , 1952 )  . the second class of carcinogenic compounds includes mustard gas ( heston , 1950 ) , nitrogen mustards ( boyland and horning , 1949 ) , epoxides , mesyl glycols ( haddow and timmis , 19051 ) , etc . 
these compounds are all known to act as alkylating or esterifying agents and probably prodtice their effects on the body by this type of reaction . certain inorganic salts of beryllium and zinc can produce tumours ( bagg , 1936 )  . there are also a number of other chemical compoiinds , showing little relationship 260 f . 
urethane it might , from the ( nettleship and henshaw , 1943 ) is an example of this kind . nature of its amide group be expected to attack the secondary forces of cohesion known as hydrogen bonds , which play a most important part in maintaining the structure of biological organeres such as chromosomes ( ambrose and gopalayengar , 1952 )  . ( b ) physical methods of producing cancer . - it appears that the simple process of implanting an inert object such as a disc of bakelite ( tumer , 1941 ) or sheets of cellophane ( oppenheimer , oppenheimer and stout , 1948 ) into a tissue can produce a tumour , while an extreme change of temperature produced by the application of carbon dioxide snow ( berenblum , 1929 ) can have a similar effect . although the ionising radiations can induce cancer , it is probable that their mode of action is indirect and is due to the formation of free radicals ( butler and conway , 1952 )  . ( c ) biological carcinogens . - the well - known rous sarcoma can be propagated by virus particles ( rous , 1936 )  . certain parasitic organisms are able to cause a malignant change to occur in the tissue ( e.g. , phytomonas tumefaciens in plants , smith , 1916 )  . 
the spontaneous tumours , whose origins are unknown should perhaps be considered to be due to the action of a biological carcinogen . it was pointed out by haddow in 1938 that there was a striking multiplicity of tumour - producing agents and , as can be seen from the summary given above , the number has greatly increased since that time ( hartwell , 1951 )  . 
the agents appear to have one feature in common ; they may be expected to lead to a more random configuration of the molecular structure within the cell , than is present in the normal tissue . 
we will try , at a later stage , to see ff the models may have any bearing on the behaviour of real biological systems . ( a ) classical treatment . ( 1 ) simple growth . - we will consider the very simple system shown in fig . 
is considered to contain a dilute solution of metabolite molecules ; the molecules could , for example , be molecules of amino acids . it will be assumed that the solution is ideal ; i.e. , that the molecules are quite independent of each other and do not interact with the solvent molecules . 
the work in thermodynamic which has to be done is generally known as osmotic work . nomenclature the work which must be done on the system is in this case expressed as a change ofentropy . 
1. in real systems the energy required for the decrease of entropy is in some cases balanced by a change in the potential energy , e.g. , the formation of a chemical precipitate is accompanied by a decrease of potential energy , because forces of attraction occur betw ' een the molecules forming the precipitate and a closer approach of the molecules leads to a decrease of potential energy . ( 2 ) growth with differentiation . - we will at this stage consider the problem of growth with differentiation since it has been the subject of a beautiful study by tyler ( 1939 ) , using sea urchin eggs , although the treatment is not in this case strictly thermodynamic . the cells at the two cell stage of embryonic development are isolated . 
2d. it is possible to compare the energy requirements for growth in the case of the normal and dwarf embryos by making use of the principle of dimensional analysis ( galmeo , rayleigh , tolman , buckingham )  . these principles tell us that there is a relationsfii . 
the war thickness is d / a / 2 units and fie , 2 . ( in d the longer line between arrows indicates r . ) suppose that an invaginot d - umits as in the real dwarf embryo shown in fig . 
3b the molecules are shown to be arranged in a hnear sequence , inert gas . in the form of a polymer chain . in this case the chain is coiled in an irregular in fig . 
3a there are very few regtrictions upon they are called , in the three figures . it is only necessary that one molethe arrangement of the metabohte molecules . cule should not coincide with another and that they should an be confined within in fig . 
3b we see that the number of possible ways of the sphere of radius r . arranging the units is greatly reduced , because each unit must be maintained at a 264 e . 
a statistical thermodynamic treatment makes it possible to express the entropy ( s ) of the systems in terms of the number of conformations with the most probable energy . if n is the number of conformations with this energy : k log n , where k is a constant . the logarithmic form occurs because the result is obtained by integration over a large number of terms . it wffl be seen that the simple process of polymerization must lead to a decrease in the entropy of the systems and that any process leading to a preferred orientation of the polymer molecules must lead to a further decrease . let us now consider a case in which we have a number of the spherical units of the kind shown in fig . 
4b is shown a similar corection of units which are now arranged another . if we now consider the configurational entropy in a definite sequence or pattem . of the polymer chlains in an individual spherical unit , we see that in the case of fig . 
4b the restriction in the configurations of the spheres , produced by arranging them in a definite pattern , wfll also restrict the number of configurations of the polymer chain 's inside the spheres . quantitatively , the actual energy difference . 
the building up of biological structures takes place by a complicated process of cefl division in which metabohte molecules are constantly being absorbed from the surroundings , while energy sources are broken down to carbon dioxide and water and subsequently discarded ; i.e. , we are dealing with an open system in which there is a constant flow of material . 
4 and let us suppose for a moment that they represent living cells containin ' g protein , nucleic acid , polysaccharide and lipid molecules . in fig 4a they are considered : to be unicellular organisms which do not interact in any way ; in fig . 
now we may be able to produce a series of reversible processes whereby we could bring metabolite niolecules in dilute solution first within the semi - permeable membrane of the cell by a process of isothermal compression , then into an orientated configuration by a series of compressions and extensions in the sohd state . because no process can be more efficient than a reversible process the energy changes involved would be the least that could possibly occur in the formation of these structures . in the actual biological process of synthesis , where events take place at a finite rate , the energy requirements for synthesis must be greater than they would be in our hypothetical models , we have also neglected for a reversib - le process . changes of internal energy in the systethe formation of polymers involves the synthesis of chemical bonds between the nionomer units . 
the synthesis of the peptide bond - co - nh - from the free amino acids h2n - c - - cooh is an endothermic reaction which requires a supply of energy , and the same is true for other biological polymers . 
the two factors of irreversibility and internal energy changes will require that all growth processes will involve a continuous supply of energy in excess of that which would be required for the entropy component in our hypothetical models . 
but these factors do not prevent us from calculating the entropy term in a real biological system . fowler and guggenheim ( 1939 ) point out that material which is not in an equihbirum state still has a definite entropy . 
ambrose the cell , the number of units of which they are composed is very large and although the number of configurations is restricted it is still very large . in the succeeding sections in the present paper , we shafl attempt to make some purely quahtative observations on what we might expect to be the differences in energy requirements for the growth of normal cells and tumour cells , in so far as the entropy component is concerned . 
m corresponds , as before , to b corresponds to the entropy state of the materials incormetabohte molecules . porated within the embryonic cell . this is represented as a lower entropy than the cell a . 
because the cell contains within itself a molecular structure which is capable of interacting with other cers . b ' + d represents the cell when differentiated and fulfilling its proper function . 
an attack upon the cer which leads to a more randoni condition of its parts can lead to an increase of - entropy . we might expect to find therefore that such an attack would lead to a reversal of the sequence shown in fig . 
a cell ' vh11 remain in an equirbrium state , or wir grow , depending upon whether the rate of synthesis is equal to or greater than the rate of degradation of the striictural components . 
5c the cell is considered to be in an equihbrium state , i.e. , in the condition of dynamic equilibrium in a polypbase system suggested by gowland hopkins ( quoted by baldwin , 1947 )  . 
5c represents the energy requirement for the carrying out of the proper function of the cefl in its differentiated foras for the autosynthetic system , the synthesis of extra - cellular material is also associated with a condition of dynamic equilibriumany of the extracellular proteins , for example , represent unstable svstenis . insuhn exhibts a spontaneous denaturation jaqueous solution which appears to be due to an autocatalytic mechanism ( waugb , 1946 ; ambrose and elliott , 1951 )  . in order that a steady concentration of materials can be present in the organism , continual synthesis must occur to make up for the loss . 
the regionrrepresents the reservoir of energy producing material in the cell , together with its associated system of enzymes . in the normal differentiated cell all the levelsof a , dandrare steady . 
we note that the present simple theory accounts for the existence of the steady state in in any system in which a large number of chemical differentiated organisms . reactions occur in a stepwise sequence , the products of one reaction being utihzed by the next , as occurs in a series of enzymatic reactions in a unicerular orgamsm , the growth curve should obey an exponential law ( hinshelwood , 1952 ) , i.e. , the rate of growth is proportioned to the number of cers present . various possible explanations for this difference have been suggested as for example by rashevsky ( 1945 ) who proposes that each cer prodiices some substance which inhibits the growth of other cells . 
chromosome breakage may therefore be a gross manifestation of the kind of change in the synthetic mechanism which can produce cancer cells . gopal - ayengar ( 1953 ) has made an extensive studv of the chromosome abnormalities which are found in normal cells and in tumour cells , particularly ascites tumour cells . 
the ducts can be seen in cross section ; it will be seen that they are arranged in the form of honow cylinders with the cefls forming a single layer round the wall . in a case of carc ' moma it is the duct cers which become mahgnant . 
6. as in the analysis given in section iib , it would be possible to calculate the energy differences for the three forms of growth , if a reversible process for changing from one form to the other could be visuahzed . 
the increase in surface area associated with the formation of the new surface requires that work must be done to provide the surface energy . in addition , a posit ' lve pressure must be apphed witbin the bubble . 
6 will require still more . were an elastic solid much more work would have to be done to form the hollow it would be similar to blowing up a rubber tube . 
the successive stages in the loss of differentiation , in this case of duct carcinoma , do therefore appear to represe ' nt states of increasing entropy , at least in so far as the observed changes of form are concemed . phenomena of this kind are again clearly irustrated in the very complete account of the genetic origin and morphology of the melanomata by dawson it is generally agreed that the naevi are derived from cefls which would , ( 1925 )  . in normal tissue , be engaged in building up a layer or sheet type of tissue . 
the transition from a layer structure to a warty form and finafly to the smooth malignant tumour represent successive stages in the reduction of surface area / unit mass for the hquid case . 
as in the previous example , the elastic case would require successively increasing amounts of energy for the formation of the structure corresponding to a departure from the uniformly spherical form . we will now examine some changes associated with tumour growth , which are taking place on a molecular scale , and can be considered in terms of the analysis in fig . 
this is because the refractive index of the fibres measured parallel to their length is different from the refractive hidex measured perpendicular to their length ; the brightness of the fibres , for a given thickness , is in these pictures a measure of the degree of molecular orientation which has been achieved during the synthesis , e.g. , the fibres of fig . 
the fibroblast cells are still laying dow - n fibrous material , but it is much more wavy in appearance , as was the case for the tumour derived from the uterine wall . 
the tissue was stained for coragen , using the technique of van gieson . the tumour showed a considerable reduction in the amount of collagen present as compared with the nornial tissue . 
20 still gives a considerable colour due to - collagen . it will be seen that there is practically no detectable birefringence m the tumour region which is on the right of the field . this result suggests that there is a relative decrease in the amount of orientated fibrous material deposited in the tumour region . in fig 9 is shown a section of normal breast tissue , ' hotographed under the polarizing microscope . 
a fibrous structure can be seen but there is a complete absence of any birefringence . the experimental evidence given above therefore appears to be in agreemedt with the general conclusion of section iv , that tumour growth corresponds to disordered states of high entropy and that in so far as the forms of growth and molecular orientation of fibrous protein are concerned the successive stages of malignancy do in fact appear to be associated with successive increases of entropy . it may be pointed out that a number of other instances could be quoted in favour of the general picture . 
the principle may help a httle in understanding the relationship between carcinogenesis and growth inhibition , as first described by haddow ( 1947 )  . if the carcinogens do in fact have a disorganising effect upon the synthetic system , it is more likely that in a given instance they wir disorganise the structure to such an extent that it can no longer function at all . 
 urethane ( ethylcarbamate ) has recently received much attention because of its use in the treatment of chronic myeloid leukaemia and other members of the group of diseases of doubtful nature at present called " reticuloses , " and also because of its action as a carcinogen . 
it was therefore thought to be of interest to study the action of urethane on the oxidation of tyrosine , by tyrosinase , to me1an tyrosine solution of concentration 0 - 02 per cent in buffer ph 7 4 was prepared , and ethyl carbamate solution of 10 per cent concentration in the same buffer . 
the upper limit of urethane concentration inveetigated was 5 per cent ; the lower limit at which inhibition could be detected by the method employed was 0 - 2 per cent . 
 from what is known of the chain of events in the oxidation of tyrosine to melanin ( raper , 1926 ) , it will be evident that this finding does not provide specific evidence for an action of the urethane on the enzyme . 
the further oxidation of dopa to melanin can occur without the aid of the enzyme , though the enzyme produces marked acceleration of the process , and the evidence so far given throws no light on which step in the oxidation is inhibited . 
 the method used was identical with that for tyrosine , with the exceptions that the final concentration of dopa was 0005 per cent , and the absence of the enzyme . 
 120 180 : ? 40 11 : ? 0 3692 - 6105 - 8377 095 : ? 3298 5510 7652 0901 3138 5152 7133 0893 3012 4873 6591 0860 - 2866 4639 6282 0809 2686 4257 5810 from this it appears probable that urethane affects the tyrosine - tyrosinase reaction in two ways : it inhibits the enzymatic conversion of tyrosine to dopa , and it accelerates the conversion of dopa to melan it seemed that further information might be obtained by in , estigating the effect of urethane on the enzymatic oxidation of dopa . 
on the assumption that the errors inevitably present are to be expected to operate equally in either direction , the probability of obtaining 8 results the same is only i in 128 . 
 120 180 240 lncremenu of ' ' e . ' ' 1496 2735 3714 4663 1427 2757 3768 4750 1367 2716 3768 4815 1405 2818 3957 4995 1427 2798 3925 5017 the inhibition of tyrosinase by urethane is , in view of the previously known action of this substance , not surprising . 
the autoxidative processes do not seem to have received the same attention as have the enzymatic ones , and the author has been unable to find any references in the literature to substances affecting their speeds , other than those producing marked changes in ph . 
h the urethane combines with the enzyme , and the ure thane and enzyme are present in such concentrations that they neutralize each other , there should be no difference between the reaction speeds of this solution and the control . 
the only suggestion which at present appears to cover these observations is that urethane has a greater attraction for the enzyme than has dopa , and that one or more of the first reaction products of their interaction acts as an inhibitor of the autoxidation of dopa later , when the enzyme has disposed of the urethane , and the intermediate metabolites have undergone further change to substances which presumably do not affect the progress of the oxidation of dopa , dopa is acted on by the enzyme , hence the acceleration of the reaction in its terminal stages . 
lea it must be emphasized that this explanation is purely hypothetical ; no direct evidence for the combination of tyrosinase with urethane , or of the presence of reaction product.s , either intermediate or final ( other than melanin ) , has been obtained . 
it is not suggested that the oxidation of tyrosine to melanin has any place in either the normal or abnormal metabolism of leucocytes , though there is the interesting fact that these cells do contain a polyphenolase capable of oxidizing dopa to melan but it did seem possible that other similar oxidations might be involved . 
methyl , propyl and butyl carbamates were prepared , the choice being limited to these as they are freely water - soluble , and their actions could be investigated by the method used for ethyl carbamate , and compared directly with that substance . 
it has been found advantageous to reduce these until the present level of 0001 per cent has been reached , as these lower concentrations prolong the period during which melanin formation can be esti mated by the colorimeter . 
the difference , however , is not great , an " d certainly does not seem to be of sufficient magnitude to allow of any explanation of the known action on leukaemia . 
it was thought possible that the effect of another water - soluble carcinogen and chemotherapeutic agent might throw further light on the proble the effect of di ( 2 - chloroethyl ) methylamine hydrochloride on the oxidation of tyrosine was investigated . 
it is of particular interest to compare the differences between these two solutions , when it will be noticed that the changes are , within the limits of accuracy of the method , yery regular . 
 - 0023 0071 0051 0029 - 0069 0172 - 0260 1155 1879 the suggested explanation in this case is that an intermediate metabolite of the interaction between nitrogen mustard and dopa gradually accumulates until it reaches such a concentration that it inhibits the reaction , thus masking the accelerating effect of the nitrogen mustard . 
 it therefore appears that there is a similarity of action between di ( 2 - chloro ethyl ) methylamine hydrochloride and the urethanes , and that this is in their action on autoxidation and not on enzymatic oxidation . 
it is obvious that it would be quite unjustifiable to attempt to explain the action of these substances in the leukaemias and other reticuloses on the grounds of their effects on melanin formation . 
in view of our present lack of knowledge of the reticuloses , and espe cially because of their almost inevitably fatal nature , it might be of ~nsiderable interest and possibly of value to investigate the effect on these diseases of other groups of substances which accelerate the progress of autoxidations . 
 methyl , propyl and butyl carbamat.es have the same effects , but to a lesser the water - soluble nitrogen mustard , di ( 2 - chloroethyl ) methylamine hydro chloride does not inhibit the enzymatic oxidation of tyrosine in a concentration of 0 - 2 per cent . 
pullinger. from the imperial cancer research fund laboratories and the research department , the glasgow royal cancer hospital , glasgow , c.3. received foi publication february 7 , 1952 . the suggestion was previously made that nodular adenomatous hyperplasia in mammary glands of mice of the riii ( paris ) strain , and possibly others , might provide a more sensitive and an earlier indication of the action of bittner 's milk agent than do actual tumours . evidence obtained under experimental conditions of forced activation of the glandular response to combined influence of hormone and agent was givren in support of this suggestion . it seemed probable also that spontaneously occurring nodules as well as those forcibly stimulated would afford reliable evidence of the action of the agent . 
the validity of such evidence would depend upon complete absence of spontaneous adenomatous nodules in the same strain deprived of agent . in sublines of the riiix strain ( renamed riib in accordance with international usage ) , which had been freed from agent by cross - suckling , no nodules had been found in the mammae of young unmated females forcibly stimulated , but two hyperplastic nodules were seen in 2 out of 44 females of the old breeding stock ( pullinger , 1947 )  . 
a survey of the mammae of all old females was in progress and was continued and combined with experiment in an endeavour to find an answer . the same problem , the stimulus for hyperplastic nodules in the zb strain ( c3h cross - suckled to deprive it of milk influence ) , was investigated by huseby and bittner ( 1946 ) , who came to the conclusion that all three factors , namely the milk tumour influence , ovarian hormone and susceptibiltiy that are responsible for the development of heritable mammary tumours in mice are also necessary for the development of these alveolar hyperplasias . 
the same authors gave an account of the morphology of nodules found in the mammae of mice in former high cancer strains and their hybrids after deliberate exclusion of the agent by cross - suckling . the strains examined were c3h and a , designated zb and ax . they compared the nodules with those in high cancer strains described by previous authors before knowledge of the milk agent existed . in the course of the present survey of old rilib ( formerly riiix ) breeders similar types of nodule were seen with the exception focal acinar proliferations were often but of those described as inflammatory . the squamous - celled nodules found in old not invariably discretely lobular . riiib females have been described and their origins discussed ( pullinger , 1949 )  . in relation to the problem of the presence and action of the milk agent these squamous - celled proliferations are not relevant , for it is generally agreed that tumours due to bittner 's agent are characteristically acinar formations and that b . 
the actual average number of litters was 4 to 5 . breeders were then segregated to allow the mammae to involute , thereby permitting detection of nodular hyperplasia of various sorts . under these conditions involution is completed in this straleaving main and a few branch ducts with tapered ends and no acinar structures . 
hybrids of less than i month old . extracts were made by grinding the tumours with sterile sand and distilled water , spinning at 2000 r.p.in a hearson centrifuge for 10 minutes , removing the supernatant fluid and spinning this in an ecco centrifuge at approximately 8000 g . 
the mammae of as many as possible of the rijib mice injected with test tumours were examined in bulk - stained preparations . will be seen from tables ii and iii that the f.i. 
pullinger dilute brown strain and their hybrids which bore more than 3 litters had a higher incidence of mammary tumours than those with less . the parous riiib females attained this average with 4 to 5 litters . of mice injected with riii tumour extracts 13 out of 23 developed mammary tumours . the mammary glands of all 7 which were examined , out of the remaining 10 , contained multiple adenomatous nodules , one as many as 30 . 
thus nodule incidence was increased in the riiib test mice by injection with riii tumour extracts . nodule incidence was not increased in the rilib mice which had been inoculated with extracts of the 2 tumours undergoing test for the agent . 
of 20 mice in the two experiments which were available for examination , the mammae of 3 contained acinar nodules ( 15 per cent ) , 8 contained nodules of other types , and 11 ( 55 per cent ) were free of all nodules . these figures are near the normal incidence . nodules in hvbrids are not recorded because there was no basis for comparison . thus neither from tumour incidence nor from nodule incidence was there any evidence of the presence of bittner 's milk agent in the 2 test tumours . the validity of results of tests in which grafts are used as suspected source of agent rather than primary tumours may be questioned . 
the majority of authors have been able to detect the milk agent in extracts of grafts derived from tumours which were known to have contained it in the first instance . jmochowski ( 1949 ) , who reviewed the various reports , has himself obtained evidence of the presence of agent after 42 serial transplantations . 
on that occasion he used multiple injections , but both he and others have succeeded with single injections of graft extracts . in a total of 69 test mice in the two experiments here recorded , not one tumour arose . these results are in accord with those of other workers who have tested extracts of primary spontaneous mammary adenocarcinomas in othier agent - free strains ( andervont and dunn , 1950 ; heston , deringer , dunn and levillian , 1950 ; dmochowski , 1951 )  . 
 ( personal communication ) were typical adenocarcinomas . assessment of the value of adenomatous nodules as indicators of the action of the milk agent . a comparison of the spontaneous incidence of adenomatous nodules in various groups of riii and ritib mice is given in table iv . it will be seen that among virgin females of the riii strain multiple nodules were present in 100 per cent at 9 months old . 
the relative reduction in number of nodules at 13 months after ovariectomy at 9 months is probably due in part to the difficulty of making accurate counts when the effect of ovarian hormone is still to be seen . among young virgin females of the riiib strain deprived of milk agent no adenomatous or other mammary nodules were found . 
pullinger when these nodules are present in mammae of young females of this strain of less than 12 months old , whether virgin or parous , they appear to provide reliable evidence of the action of the agent . 
this conclusion is more certain if oestrogen has been excluded by ovariectomy several months prior to examination of the mammae . breeders of the riiib strain deprived of agent , of 12 months of age or more , developed 1 to 3 adenomatous nodules in the 10 nipple regions . since these nodules were not associated with agent in the tests recorded , it is clear that they do not invariably provide evidence of the presence of agent in old breeders . they may be due to some other unknown cause . multiple adenomatous nodules in old breeders of this substrain would nevertheless provide presumptive evidence , requiring confirmation , of the presence of the agent . thus for purposes of detection of agent by inoculating suspected substances into susceptible test mice and using the adenomatous nodule as evidence of the action of agent , only young rijib virgins or breeders under 12 months old would be suitable as test animals . that is to say , they would have to be killed and examined at about 9 to 11 months old when positive results could be expected and before the nodules of unknown origin begin to appear . only if counts of nodules were required would ovariectomy have to be done because the naturally occurring hormone under normal conditions does not cause a confusing degree of focal acinar proliferation . 
nodules of purely adenomatous hyperplasia were found in about 19 per cent of parous females of 1 year old and over of the rijib strain deprived of bittner 's milk agent . 
no evidence was found that the nodules or tumours in the mammae of old parous females of the cross - suckled riiib strain owed their persistence to ovarian hormone ; neither could their origin or persistence be attributed to the milk agent . 
ludford , director of the research department , and to the board of management of the mount vernon hospital , northwood , continuity of observation was maintained to the end of these experiments . to the generosity of p . 
allsopp. from guy 's hospital medical school , london , s.e.1. received for publication march 5 , 1951 . in earlier papers ( allsopp and szigeti , 1946 ) an account was given of some of the properties of water - soluble substances which are produced from 3 : 4 - benzpyrene under the influence of monochromatic radiation of wavelength 2537a . aqueous ( bicarbonate ) extracts from the irradiated benzpyrene were found to be carcinogenic when painted on the skins of mice ( allsopp , 1946 )  . these biological tests , however , were very prolonged , four or five paintings weekly for some in an attempt twenty - six weeks being required before growths were obtained . to reduce this " latent period " experiments have been made in which croton oil was used as a co - carcinogen . observations on the effects of croton oil on the mice used in these experiments , when compared with those of p . 
of 0 - 5 per cent croton oil in acetone ( experiment la ) at first caused little superficial change . slight ulceration , as evidenced by patchy encrustation , was visible on the third day , after which epilation began . this was complete by about the tenth day . 
so soon as the encrustation sloughed hair began to grow again , and by the fourteenth day the animals appeared normal . day to day observations are set out in table ii . painting with 0 - 5 per cent croton oil at weekly intervals ( experiment lb ) caused a similar sequence of macroscopic changes , but restoration of hair growth was delayed until the third week , after which the epilation cycle repeated itself 276 c . 
no growths resulted , and histological examination of the painted skins revealed nothing more than a slight hyperplasia on any animal . co - carcinogenic effect of croton oil with 3 : 4 - benzpyrene . ( table i , experiment 3 . ) equal volumes ( 0 ' 1 ml . ) of 0 - 05 per cent benzpyrene in acetone and of 0.5 per cent croton oil in acetone were applied alternately at 3to 4 - day intervals , each animal thus receiving each agent once weekly . 
control animals were painted at the same times with benzpyrene , but with acetone instead of croton oil solution . papillomata were first seen on the experimental animals after 5 weeks ; all the survivors had malignant or " pre - cancerous " lesions by the fourteenth week , a precancerous lesion in this context being one exhibiting irregular epilation , hyperkeratosis , abnormal regeneration of hair follicles , ill - defined epidermal projections , a large increase in the number of mitotic cells , numerous abnormal mitotic figures , and leucocytic infiltration of the dermis ( allsopp , 1946 )  . 
when the experiment was discontinued in the twentieth week , 4 out of 8 surviving control animals had cancerous or pre - cancerous lesions ; the remainder showed marked hyperplasia only . 
the experiments described above , however , suggest that its action is more complicated than this simple description migth indicate . despite a marked difference in the response to croton oil of the mice now used when compared with that of strains used by other workers , berenblum 's findings ( berenblum , 1944 ) have been largely confirmed when 3 : 4 - benzpyrene was the carcinogen ; but when the hydrocarbon was replaced by the water - soluble substances which are obtained from it by the action of ultraviolet light croton oil appeared to exert a different effect since , while papillomata appeared on the mice at a very much earlier stage than they did with the carcinogenic solutions alone , a proportion of these papillomata did not develop into epitheliomata , whereas 278 c . 
the distinction in behaviour , however , was not entirely clear - cut , since the papillomata on 2 out of 9 animals did persist , growing very slowly , until they became malignant . the earlier experiments with the water - soluble substances ( allsopp , 1946 ) showed that with them the process of carcinogenesis was slow , but that it passed through the usual 3 phases of hyperplasia , papillomata , and finally carcinomata . the last stage required 6 to 10 weeks . 
the present experiments suggest that croton oil accelerates the transition from hyperplasia to papillomata - the first papilloma appeared after 13 instead of 26 weeks - but not the transition from papillomata to epitheliomata , which again took about 9 weeks . indeed it may even delay this change , or - in those cases where the papillomata were sloughedin contrast to this , benzpyrene itself appears to act rather more prevent it . quickly ; epitheliomata had developed in the animals recorded in experiment 3b of fig . 
gorer , of guy 's hospital medical school , and to m . salaman , of the london hospital , for comparing with mine the results of their experiments on the effects of croton oil on the skin of mice . 
the tumour incidence in the experimental group ( 9 / 22 , or 41 per cent ) is thus not significantly in fact , a slight falling off in the tumour lower than in the control groups . incidence might have been expected in mice that were 43 weeks older than their controls at the time of tumour development . 
campbell. from ae royal ( dick ) veterinary college , edinburgh , and the poultry re8earch centre , king ' 8buildinp , we8t main8road , edinburgh . received for publication february 5 , 1951 neoplasms involving the ovary are common in the fowl ( olson and bullis , 1942 ; campbell , 1945 )  . 
the great majority far into one or other of two categories , namely adenocareinomatous growths in various stages ofdifferentiation from the frankly anaplastic type to the sclerosing tumour , or , secondly , lymphomatous growths associated with the leucotic complex , e.g. , lymphocytoma , fowl paralysis tumour , aleukaemic lymphoid leucosis , etc . 
most of these lymphoid growths should not be classified as ovarian tumours , since in view of the generalized nature of the leucotic process it is usuary impossible to be certain whether they are primary in that organ or not . 
they are mentioned simply because of the frequent teference in avian pathological literature to " lymphoid ovarian tumours . " in human pathology , besid6s - the common adenocareinomatous types of , ovarian tumour , several other rarer forms are recognized as follows : brenner tumour ( o6phoroma folliculare ) : granulosa - cell , thecal , and luteal tumours arrhenoblastomas ; dysgerminomas . a survey of the hterature deahng with neoplastic disease of the fowl shows the apparent extreme rarity of such tumours . seifried ( 1923 ) recorded a brenner tumour of the fowl and compared it with its human counterpart , a ' nd friedgood and uotila ( i 941 ) detailed 5 cases of - ovarian " tumours " associated with virilism in two of these latter cases , tuberculosis of the ovary compheated in the fowl . the picture , and the remainder were cystic or contained smau growths which appeared to be tumours in various stages of degeneration . tentative diagnoses of arrhenoblastoma were made , but it was also suggested that they might be luteal - cell tumours or " hypernephromata . the only record of an ovarian teratoma in the fowl is by jackson ( 1936 )  . with regard to the male bird , there appear to be no reports of spontaneous seminoma or interstitial - cell tumour , but several cases of spontaneous teratoma testis have been recorded ( sheather , 1911 ; jackson , 1936 ; olson and bulhs , 1942 )  . it seemed reasonable to beheve that the absence of reports of the rarer forms of ovarian and testicular tumours was simply an indication of a lack of intensive study in this brartch of comparative pathology . it was therefore determined to examine as many tumours arising in these sites as possible . 
to date approximately 2000 cases have been submitted to a thorough post - mortem and histological scrutiny , and , as was anticipated , several hitherto unrecorded types of tumour of the fowl gonads have been encountered . it ' is desirable that an account of these should be put on record , not only because of their interest from the viewpoint of comparative oncology , but also j . 
at post - mortem a thorough search was made for metastases , and the possibihty that the gonadal tumour was not the primary growth was ruled out as far as possible . blocks of tissue were taken from many organs for histological examination , whether they showed visible abnormality or not . 
the growth offered some resistance to ' the knife , and its cut surface showed pale yellow fibrous areas containing numerous small cysts and islands of pinkish tissue . there were no implantations in the abdominal cavity and no metastases were found . histologically a large part of the tumour consists of a stroma of interlacing bands and whorls of fibrous tissue , mostly dense , but having a looser texture in there is a certain amount of plain muscle ( characteristic of the some places . avian ovary especially at the hilus ) in one part of a section . 
a comparable structure occurs in the human subject , and is well ifustrated by nicholson ( 1950 )  . ( 2 ) the next ovarian tumour to be considered is the granulosa - cell type , of which 4 cases have been studied in this series . 
on section , it was cream to yellowish in colour and displayed bands of tissue which had a tehdency to radiate from the centre of the growth . the vascularity appeared to be very poor . 
the rest of the ovary seemed normal , with a few atretic follicles , and the oviduct was that of a bird in full lay . histologl ' cally , this tumour is mainly composed of round oval or fusiform cefls , with a j . 
the periphery of the growth is largely necrotic . radiating bands of smooth muscle occur in the interior of the section . wilhs ( 1948 ) states that ovarian fibromata are probably the end result of a in that case , the rarity of the latter in fowls may account theca - cell tumour . for the equary rare occurrence of fibrous tissue tumours associated with this organ . 
as an instance of this the only case of ovarian fibroma encountered in this series is worth mentioning . it was found in a rhode island red hen in her third year , and weighed 570 g . 
maximow and bloom ( 1948 ) state that what are usually considered chromaffin cefls ( sympathicotrophic cells ) are to be found at the hilus of the human ovary . these apparently have much in common with the medullary cells of the adrenal , although they cautiously conclude that until these cells have been shown to elaborate epinephrin , their relationship to adrenal medulla must remain unproven . the chromaffin reaction of such ovarian cells is unrehable but this also applies to the adrenal medullary cells , where the staining by chrome salts may vary from practicary none to a very deep brown . as far as can be ascertained there is no record of chromaffin cells or heterotopic adrenal cortical tissue in the avian ovary . that such cells may in fact be occasionally present seems to be imphed by the following cases , and a thorough cytological examination of the region of the hilus should clear up this point . the first of these tumours to be described occurred in a brown leghorn hen which was brought for examination after developing signs of mascuhnization . the bird was said to have ceased laying , commenced crowing and to have endeavoured to copulate with other hens in the run . the comb was decidedly male in character , and plumage changes were evident especially in the neck and taff . upon post - mortem , a rounded soft yellow - brown tumour measuring 3 - 8 x 3 - 5 x 28 cwas found in the ovary , which was inactive . 
numerous irregular trabeculae containing vessels arise from this and pass into the interior of the growth . between these are sohd islands of large polyhedral epithehal cells which are in turn divided into small irregular groups by fine connective tissue staining as for reticuluthe cytoplasm is eosinophilic and faintly granular . in places it is vacuolated . 
the first view is favoured as being the more probable . ( 5 ) the next case , though not a mascuhnizing growth , is worth recording for its unusual nature , and because its interpretation could mean that besides adrenal cortical ceus , chromaffin cells resembhng those of the adrenal medura may occur in the fowl 's ovary and may undergo neoplasia in common with other heterotopic - tissues . during the examination of a crossbred fowl wbich was found dead , a large intra - abdominal blood clot was found proceeding from a rupture in the substance .of a smoothly lobulated brownish - yerow tumour of soft consistency , measuring 6 - 5 x 5 x 4 - 3 cand occupyi ' ng the site of the left ( functional ) ovary . it was - freelymovable , being only attached at the bilus , and was therefore easily dissected out . 
the healthy remainder is composed of connective tissue cells with spherical to spindle - shaped nuclei , and eosinophilic granular cytoplasm , surrounding aggregations of large polyhedral cells with abundant finely granular eosinophihe cytoplasm , large nuclei and very prominent nucleoli ( nuclear - nucleolar ratio . 1 : 3 to 1 : 5 )  . an abundant infiltration with eosinophils is present in many parts of the smau epithelial - cer moiety . a well - marked but thin layer of connective tissue separates this outer zone . from the inner , which is composed of small lobules of cens separated from each other by fine trabeculae of connective tissu ' e . 
the cefls composing these groups are large , with giant nucleoh similar to those mentioned above , and have a brownish - yerow cytoplasm in bichromate fixed haematoxyhn and eosin preparations . 
at the edge of one series of sections , the only indication of ovarian origin is the presence of a few folhcles . bands of smooth muscle are scattered throughout the section . the presence of such la ' e numbers of cers showing a distinct chromaffin reaction justifies ' a diagnosis of chromaffmoma or paraganghoma . 
the growth appears to have arisen within the adrenal capsule . another small ( 0 - 5 x 0 - 2 cm . ) tumour was found in the site of the rudimentary right goriad and closely adherent to the dorsal wall . this shows not only testiculoid elements , but also a considerable area composed of whorls and strands of rapidly dividing mesenchymatous cers , presumably a metastasis from the experimentary transplanted sarcoma . the histology of both gonadal rowths resembles ewing 's ( 1942 ) fig . 
the nests of cells below the germinal epithehum resemble the primitive sex cords of the indifferent embryonic gonad . this tumour iuustrates well the bisexuality of the embryonic fowl 's ovary . 
the rete ovarii formed from the primitive sex cords is a homologue of the testis and as is well known can develop into one following left ovariectomy of the hen , where the right gonad hypertrophies and differentiates even to the exteht of producing spermatozoa ( benoit , 1923 )  . another tumour of the ovary associated with masculinization in a light sussex hen is shown in fig . 
17. folfculoid formation and luteinization is apparent , and the structure is comparable to a granulosa - cell tumour . in fact , this diagnosis would be justifiable on histological grounds alone , but has to be modified in view of the androgenic effects on the host . it would appear that the rudimentary right ovary is not the only place where in theory at any rate , testiculoid structures could arise in the intact bird . 
champy , lavedan and marquez ( 1 939 ) state that the adrenals of either male or female castrates in the fowl frequently contain " regenerating gonadal cens . " birds ' adrenals constantly contain wolffian duct remnants in the capsule on the ventral these slowly hypertrophy following castration to form an internal aspect . epididymis - hke structure , whilst some form epithelial tubules similar to those found in the right ovarian rudiment subsequent to castration . 
spermatogenesis has not been seen in the adrenal capsule however . there does not seem to be any record of spontaneous arrhenoma arising in the adrenal capsule of the fowl , but it seems possible that the foregoing is a case in point . ( 7 ) the last of the tumours of the female gonad to be described was originally considered to be a teratoma . it is unfortunate that no comparison can be made of this case with the only comparable ovarian tumour of the fowl on record ( jackson , 1936 ) , since apart from stating its didermic character , no other details were given , and the single photograph is of the gross specimen . the present case occurred in a brown leghom hen aged about 3 years , at the poultry research centre . 
of which was withafter death 4 days later , an ovanan tumour was drawn from the abdomen . it was mottled pink , brownish and cream , of found measuring 5 x 4 x 4 cm . other growths , pinkish and soft , firm consistency and mucinous on section . were attached to the wall of the oviduct , and to the serous investment of the duodenum , pancreas and liver . histologically the ovarian tumour is the only one to show complexity of immediately below a thin capsule there are nests oflarge pale staining structure . epithehal cefls , spme of which have differentiated into cysts of varying size , lined with one or several layers of columnar epithehum . in many cases these cells are actively secreting mucus . 
at first sight two embryonic layers appear to be involved , namely mesoderm and ectoderm . the latter may be represented by the cyst epithelium forming mucinous glands , and possibly as the complex epithelial tubular structures . 
the remainder of the tumour is mesodermal in origin . ifthis is the case the presence of these derivatives of two germinal layers presumably puts it in the same category as jackson 's ( 1936 ) " didermic teratoma . " wiuis ( 1948 ) defines a teratoma as " a true tumour or neoplasm composed of multiple tissues of kinds foreign tothe part in which it arises . " the presence of cartilage can be explained by the conversion of connective tissue normary present in the ovary , to cartflage by mucoid degeneration and hyalinization . 
one of their cases exhibited metastases , but no details are given of the histology of this secondary growth or its site . several seminomas have been studied during the past 11 years and two of these are selected for description here . 
the right testis was normal both in size and microscopic structure , and no metastases were found . microscopically the left testis consists of poorly dehneated lobules of pale staining epithelial cells arranged in diffuse sheets and penetrated here and there by blood vessels . the cells are mainly spherical to polygonal through mutual pressure , but the faintness of cytoplasmic outfine often gives a syncytial appearance . 
a second testicular tumour - also involving the left organ - wa 's seen at autopsy in a buff rock cockerel . it measured 4 - 5 x 3 - 8 x 3 - 5 cm . , and on section showed an irregular yeflowish area near the caudal pole , compared with the rest of the tumour which was of a cream colour . 
the cream - coloured area , forming about two - thirds of the tumour . , is composed of typical seminoma cefls , showing in many places a marked acinar structure . luteinization of these cens is proceeding in small isolated areas . 
the question arises whether the interstitial - cell moiety represents a concommitant neoplasia of the stroma , as the acceptance of firket 's ( 1920 ) view on the connective tissue origin of interstitial cells would imply . in other words , is this an example of a " mixed tumour " - or alternatively is it an indication of the teratomatous nature of seminoma , as ewing ( 1942 ) beheves , but which willis ( 1948 ) , nicholson ( 1950 ) , and others dispute ? still another possibility exists , namely that the two cell types have arisen from a common ancestral totipotent germinal cell capable ofgiving rise to a variety of tissues , in accordance with the view put forward by innes , harvey , and dawson ( 1938 )  . a re - examination of fig . 
the last testicular tumour of special interest occurred in a cross - bred fowl , which showed during life a marked atrophy of the comb , and cessation of crowing and of other activities associated with the adult male bird . at post - mortem , a greatly enlarged ( 9 x 10 x 6 cm . ) left gonad was found , a flattened oval in shape and firm in consistency . 
at subsequent autopsy this bird had a small nodule at the site of the right gonad , whose histological structure , in the opinion of the present - writer , resembles that of a thecal - cell tumour . teilum 's ( 1946 ) case of " androma " of the testis in man may be ' another example of a feminizing tumour arising from a persistent remnant of the " ovarian " cortex , and the presence of arrhenomatoid tissue in a testicular teratoma of a .fbwl which lost certain of its male characters has already been described in the present paper . tuming to granulosa - cell and related tumours , the development of the ovary throws some light on the inter - relationship of these oestrogen - secreting growths . in the embryonic ovary it is commonly stated that the granulosa cells arise from coelomic epithehum derived from the genital ridge , whereas the thecal cens , being stromal in nature arise from the mesenchymal elements of the mesoderm . examination of the early ovary , however , shows primary folhcles composed of a central ovocyte surrounded by a ring of indifferent epithehal cens indistinguishable .from the stromal cells composing the rest of the organ . these indifferent cens appear to be the precursors of the granulosa cells , whereas the remainder of the it seems probable that this common ancestry is reflected - stroma forms the theca . in the behaviour of thecal and granulosal cees in the neoplastic state , where both secrete oestrogens as judged by the muscular and glandular hypertrophy of the , oviduct of the tumour - bearing bird , and both undergo the phenomenon of luteinization . granulosa - cell tumours in the fowl are not morphologicary identical to these in man in that they do not exhibit the characteristic " rosettes " which are often j . 
campbell a feature of human tumours , and which are considered to be identical to the bodies of call - exner occurring normally in the stratum granulosum of the human such bodies are not found in the granulosa layer of the ovarian follicle ovary . because this is usuary only one , or at the most two or three cers thick . callexner bodies are usuary considered to be due to cystic degeneration of granulosa , this does not occur in avian tumours where there is ample space for such cers . a change to take place , and it therefore seems possible that these structures may serve some specific purpose as for example a glandular function , in the ovaries of those animals in which they occur . with regard to thecal - luteal cells and the interstitial cells of the testis , it is interesting to note that they appear to have a common ancestory . fell ( 1924 ) states that the ovarian thecal - luteal cells of the fowl are derived from remnants of aborted medulla in the development of the ovary . thus they have the same histogenesis as seminiferous tissue . 
9. - structure of the above , showing vacuolated cells , due to removal of lipoids , to the left ( some nuclei are pyknotic ) and cells resembling fibrous tissue to the right of the figure . 
18. - - - - " mixed ? " ovarian tumour , consisting of areas of tortuous glands , mucinous cysts , cartilage , solid nests of epithelial cells and a myxomatous stroma . 
the medium is left unchanged throughout each experiment . films of concentrated cell suspensions made after gentle centrifugation were in the present series stained by a combined leishman - giemsa stain , and by feulgen 's method . 
about 500 - 600 leishman - giemsastained films were studied in the course of these experiments . the appearances described are those found in the basic culture medium . the addition of 5 per cent rat e.e. 
causes few differencem , apart from raising the number of mitoses . the only divergent feature is the appearance of increased numbers of degenerate polymorphonuclears , probably owing to the metabolic stimulant action of the e.e. from the cytological point of view , the life of each culture of leukaemic blood may be divided into two phases . 
the first , during which there is evidence of multiplication , and to a less extent of maturation , of the immature cells , reaches a climax during the first day , and comes to an end some time during the second 24 hours . 
from this , it does not follow that there is an increase in the total cell count of the cultures , for there is also a concomitant dying - off of mature cells . if , however , the mitotic index is high enough , as in cultures containing e.e. , there may be an increase in the absolute number of immature cells . this means that proliferation outstrips maturation . mitotic figures , very rare in the peripheral blood , are regularly found in cultures from the second hour onwards . 
they occur mainly in myelocytes , but are also seen in myeloblasts . differential counts have been done as a routine , but the total numbers of mitoses are too small to permit precise conclusions on the phase distribution ; further , owing to the technique necessary in making smears , the recognition of telophases is often difficult , and their number probably greater than is apparent in counts . no gross deviation from the ordinary phase distribution has , however , been found . in particular , there is no evidence of a metaphase arrest in untreated cultures . 
the mitotic index reaches a maximum of four to six mitoses per 1000 immature cells at about the eighth hour of culture in basic medium , or of up to 19 per 1000 immature cells at about 24 hours , if e.e. 
an extensive literature deals with tissue culture of normal and leukaemic blood and bone marrow , and has been reviewed by bloom ( 1938 ) , and more recently by fieschi and astaldi ( 1946 )  . it is not proposed to discuss this volume of work in detail , especially in view of the fact that much of it is not strictly comparable , as the methods of culturing and of examining the cells were often different from those employed in this series of experiments . thus most workers have used the cultivation of solid fragments rather than that of cell suspensions , and have described the appearances in sections instead of smears . 
comment will therefore be restricted to a few papers in which results have been obtained by related methods . there is general agreement that survival of human leukaemic cells is possible in cultures , and though the maximum times given vary considerably , no claims of indefinitely prolonged life in vitro have been advanced . 
many authors report the development of non - specific connective - tissue cell strains such as macrophages and fibroblasts from the highly specialized blood cells , but this appears to depend on the presence of a solid supporting framework , and does not occur in cultures made in a fluid medium . mitotic division of immature cells has been frequently observed and generally found normal . it is of interest to note that whereas mitoses are extremely rare in the circulating blood , they begin to appear almost as soon as blood is withdrawn from the body . the rapid change can scarcely be due to the effect of the culture medium alone , but may well be caused by the removal of an inhibitory factor operative in the body . the occurrence of maturation is a more controversial question , and the various answers which have been given appear to be mostly based on impressions . strict proof can only be obtained if total as well as differential counts are done with adequate methods , and this is only possible in fluid cultures . israels ( 1940a , 1940b ) , working along these lines , maintains that maturation occurs normally . fieschi and astaldi , on the strength of smears made from solid cultures , admit a certain degree of maturation , but state that this is always less pronounced than the proliferative processes . 
the findings cited here and in the previous report tend to support the latter view . while the normal maturative changes have not been very striking in this series of experiments , the development of new and abnormal cell types has been it is remarkable that this has not been commented upon by other of interest . workers , except by fieschi and astaldi , who , in their fig . 
7 and 14 it can be seen that the coarsening of abnormal erythropoiesis . the chromatin pattern is accompanied by its breaking up into discrete fragit is possible that ments , the nuclear membrane remaining meanwhile intact . these appearances signify an abnormal prophase , the first stage of endomitosis . the abnormality is conceived to consist in a premature separation of the daughter chromatids , which does not lead to metaphase or to a breakdown of the nuclear membrane . 
the consequence is an increased nuclear size , which may express itself by lobe formation and can , but need not , lead eventually to a more or less regular nuclear division , unaccompanied by division of the cytoplasm . in this connection the disappearance of the nucleolus is noteworthy : it is apparently a prelude to the accumulation in the nucleus of desoxyribose - nucleic acid , which is made evident by the deeper staining in leishman - giemsa and especially in feulgen - stained films . it may be objected that small numbers of polyploid cells occur normally in tissue cultures ( macklin , 1916 ) , and that their formation can be encouraged by manipulations such as the reduction of oxygen tension ( barta , 1926 ) or variations in the temperature of incubation ( stillwell , 1944 )  . 
8 with its double layer of cytoplasm has often been described and pictured as typical of the cells of " monocytic " leukaemia ( d ' antona , 1931 ) , while the resemblance of some of the polymorphs to those seen in pelger 's anomaly has already been remarked upon . it may be concluded that immature blood cells can , in vivo , undergo changes similar to those which are here reported for in vitro work . 
the special conditions prevailing in cultures made in the fluid medium , and - by the technique described , are evidently particularly suitable for encouraging this sequence of abnormal it is probable that at least events , but do not permit full normal maturation . some of the abnormalities in cultures are explained by lack of metabolic factors ordinarily present in the body , and possible that study of the metabolic processes in cultures and of variations in the composition of the medium may elucidate if successful , such a study might lead to the nature of some of these factors . a clearer understanding of the reasons responsible for the varied behaviour in culture of different bloods . 
1. received for publication february 23 , 1948 . in a previous communication we reported that a strain of the shope rabbit papilloma had been transmitted for 10 serial passages in the domestic rabbit ( selbie and robinson , 1947 )  . 
the adaptation of this tumour virus as a transmissible infection in domestic rabbits occurred during experiments in which the simultaneous inoculation of shope papilloma virus and sheep dermatitis virus in domestic rabbits produced papillomas that proved infective to other rabbits ( selbie , 1946 )  . 
the further passage of this virus in domestic rabbits was materially helped by continuing the procedure of mixing a second virus suspension with the infective inoculum of papilloma virus , and also by treating the skin with croton oil before inoculation , but there was no evidence of an increase in the virulence of the virus suspensions during passage . in the present communication we shall show that carcinomatous transformation has occurred regularly in this transmissible papillomatosis , and in a mamner similar to that found in the non - infective papillomatosis that is produced in domestic rabbits by the inoculation of extracts of papillomas from the cotton - tail rabbit , the original host of the shope papilloma virus . 
3. received for publication january 18 , 1949 . the investigation of carcinogenic substances which have been obtained from human tissues ( kleinenberg , neufach and shabad , 1940 ) and from other biological sources has been the subject of earlier publications from this institute ( hieger , 1940 , 1941 , 1946 , 1947 ) , reporting that : 1 . 
technique used in these experiments for testing for carcinogenic activity . unless otherwise stated , the substance is injected subeute ( 15 per cent solution in lard ) into mice of c57 strain or of mixed commercial stock . 
control experiment on reagents used in the saponification of tissue by potassium hydroxide and alcohol . since the great majority of the carcinogenic fractions had undergone saponification at least once , control experiments on the process itself acting on noncarcinogenic tissue components were made . 
distilled alcohol for 2 - 3 hours and then carcinogens might be formed during extracted several times with ether . saponification from precursors in the tissues or from the reagents themselves . in the earlier experiments the alcohol was industrial spirit ( the manufacturers state that it consists of ethyl and methyl alcohols in the ratio of 19 : 1 with 5 per cent water ) , which in separate experiments was found to darken rapidly on refluxing with koh owing to resinous condensation of aldehyde . acetaldehyde was therefore refluxed with koh and spirit under the same conditions as those of tissue saponification . 
 " n on - cancer liver " indicates the liver of a human subject who has died of any cause other than cancer . ( b ) fraction a from mixed cancer livers , partly the same as those used for the preparation in ( a ) , was crystallized from 80 per cent aqueous alcohol after adsorption from petrol ether on to a large column of a1203 eluted with petrol ether - benzene - meoh ( 80 - 20 - 20 )  . 
the possible reasons for the absence of tumours are discussed below . ( d ) a similar fractionation was made on another batch of cancer livers , and mice were injected with material from g , c , f , d , e and h . 
the test on f was repeated on a further 10 mice in which one tumour arose after 2 years . ( f ) the 10 fraction from human non - cancer lung - kidney - muscle ( fraction a ) had given 3 tumours in 25 mice , and was considered a potent it had been in the cold room for over carcinogen - containing fraction . 3 years and was then fractionated according to a simplified scheme ( flow sheet 2 )  . of 52 mice at the beginning of the tests , 43 survived 12 months and 26 , 18 months . 
four sarcomas appeared , 3 in fraction g and 1 in c . ( g ) the crude unsaponifiable fraction ( m ) of mixed livers which had been used in experiment ( d ) was fractionated and tested at j , k , l , g , a , c , f , m , i , using in all 110 mice , which lived well ; 92 survived 12 months and 40 , 18 months . 
a large batch of the crude unsaponifiable matter was worked up to stage a ; a part was kept for injection , and another part was acetylated and crystallized by careful seeding . 
the crystalline acetate was hydrolysed and the regenerated cholesterol tested . in the 12th month one sarcoma appeared in the a series , and in the 19th month one sarcoma developed in the cholesterol group . 20 mice were employed in each test . ( i ) cholesterol - rich fraction from cream ( cow 's milk )  . - kennaway ( unpublished communication ) had found that the unsaponifiable part of cow 's milk produced a sarcoma by injection into c3h mice . 
the experimental mice lived well ; after 29 months a mouse of the f series ( flow sheet i ) developed a sarcoma at the site of injection . ( k ) liver from a lymphosarcomatous human subject gave a highly carcinogenic unsaponifiable fraction in some of the earlier experiments ( hieger , 1940 ) , and the tissues of humans with this type of cancer may possibly be rich sources of carcinogen three livers from lymphosarcoma cases were saponified , fractionated into stages a , j , m , l , and injected into 6 , 5 , 11 and 6 mice of crossed c3h x c57 strain , which survived well , but no tumours developed . the 85 per cent cholesterol fraction ( a ) of cancer livers which had given 2 sarcomas in 10 stock mice was stored in the cold room for 2years , then tested on 10 c57 mice . 
one sarcoma appeared in the first series in the 14th month in a c57 female , and one sarcoma of fibrous type in the second in the 22nd month in a stock female ( experiment 7 , table i )  . when over 300 control tests had been carried out on lard alone without the production of a single tumour , a sarcoma arose at the site of injection in a c57 mouse first injected with lard when already 16 months old . 
fatty extract of walker rat tunmour . aptekman , king and lewis ( 1943 ) induced sarcoma in rats by injection of their results were confirmed here by the fatty fraction of walker rat tumours . tests where the tumours were dried by storing in distilled spirit and extracting with benzene . 
a after parallel group of 10 rats were injected subcutaneously with lard alone . two years one rat in each series developed a fibro - sarcoma , which grew with difficulty on transplantation . 
both tumours arose in the subcutaneous tissue at the same level as the injection site , but on the opposite side this effect has been observed several times in experiments where of the body . the injected substance is very fluid , and is probably pressed round the subcutaneous spaces by the movements of the animal 9 . 
10 stock in the 14th month in group b 2 mice developed sarcomas , and pre - neoplastic changes were seen at the site of injection in 4 other mice . thus in group b , 6 of 10 mice had either developed sarcoma or might have done so if they had lived longer . 
the two sarcomatous mice and two of the incipiently sarcomatous mice were from the same box of 5 mice . one cannot say why only group b responded so readily , but ( 1 ) in a fair number of experiments the saponification of tissue has been done in spirit but the products have produced no tumours , showing that spirit is not essential for carcinogenesis by the unsaponifiable product ; ( 2 ) the absorption spectra of the two final products ( cholesterol saponified in spirit and in alcohol ) are closely similar ; and ( 3 ) while the substance was strongly carcinogenic in group b ( stock mice ) , the same preparation was inactive in group a ( c57 )  . consequently it must be supposed that the b group of mice were either ( 1 ) peculiar genetically ; ( 2 ) peculiar congenitally ; ( 3 ) had become infected or ( 4 ) had become contaminated with carcinogen . ( 4 ) is , on the whole , not very probable , because the 1946 paper reported that in tests on 18 subfractions of the unsaponifiable fraction of human tissue , partly from cancerous , partly from non - cancerous 134 i . 
ieger subjects , of the total yield of 8 sarcomas , 7 were produced by fraction a made from 3 different sources and 1 from an m fraction ( flow sheet 1 )  . 
the concentration of 7 / 8ths of the sarcomas in one particular fraction strongly suggests that the fraction itself was responsible and not a chance contamination , for it would be highly improbable that contamination would occur only in the boxes , holding 5 mice each , containing those treated with the a fraction . the data in table mi are the results when a fraction was divided into 3 or more sub - fractions . 
pre - neoplastic changes at the site of injection of lipid . since the detection of only a few tumours could be important in deciding the technique of further fractionation , it was essential not to miss any tumours not visible macroscopically . 
30 non - cancer livers tested separately ( 6 in 30 were active ) tested separately ( 8 in 37 were active ) ratio : sarcoma mice total mice used . 12 / 56 = 21o 5 / 63 = 8o 44 / 120 = 370to0mean21 17 / 101 = 17o% 12 / 456 = 10 ' 440 = 2 30o thus the effect of testing a number of livers ( 67 ) separately was to reduce the sarcoma production by a factor of 9 , i.e. 
hieger ( 2 ) commercial cholesterol in lard gave sarcomas in about 5 per cent of 213 mice ( table ii )  . ( 3 ) the mixture formed when cholesterol is refluxed with koh and distilled spirit gave no tumnours when injected into 10 c57 mice , but in 10 stock mice there arose 2 sarcomas , and in 4 other mice of the same series changes were detected , post - mortem , suggestive of pre - neoplasia , at the site of injection . 
a total of 69 sarcomas has been obtained at the site of injection of lipoid substances in approximately 2000 mice of c57 and mrc strains and commercial mixed stock mice . 
7. received for publication june 9 , 1947 . the presence and activity of the milk - borne agent of mammary tumours of mice discovered by bittner ( 1936 ) are detectable only by the growth of a mammary tumour . 
found two nodules in one mouse out of nine of the n strain in which mammary tumours had never occurred . also when efforts have been made to exclude the milk - borne agent from high cancer strains by cross - suckling , nodules have nevertheless been found . 
thus bittner , huesby , visscher , ball and smith ( 1944 ) examined the mammae of fostered breeding females ( fostered by cancer - free maternal stock ) from high cancer strains a and c3h . 
all the females had given birth to at least three litters and ranged from 11 to 16 months old , thereby providing suitable conditions for pathogenic activity of the milk - borne agent . nodules were found occasionally , though never more than one to a gland , thus nodules were still present though in smaller numbers when efforts were made to exclude them than in mice which had been suckled on their own cancer - prone mothers . this evidence indicated that nodule incidence is not eliminated by cross suckling with the same regularity that is attainable in regard to tumour incidence . 
6. - regression of hyperplasia induced by 800 y oestradiol in spayed r3 female ( carrying the milk - borne agent ) , and persistence of areas of nodular hyperplasia ( adenomas ) at 6 months old . 
the former discrepant results ( bittner et al . , 1944 ; huesby and bittner , 1946 ) have to be remembered , although subsequent observations ( kirschbaum et al . , 1946 ) provide convincing evidence that hyperplastic mammary nodules do not occur in the absence of the milk - borne tumour agent . the second source of objection to accepting nodular hyperplasia as evidence of activity of the milk - borne agent acting alone is that certain observations , which will be referred to again later , suggest that similar cellular proliferations with acinus formation are stimulated by oestrogenic hormones alone . the problem of the exact origin of the hyperplastic nodules is of great these focal acinar proliferations precede maligimportance for several reasons . nant tumours in time of appearance and are often more numerous . they might thus provide an alternative and earlier means of detecting activity of the tumour they may also represent the earliest sign of tumour growth before it agent . can be described as malignant . if so they would provide material enabling one to determine which influences are causative and which are encouraging , in the sense in which the term is used by rous and kidd ( 1941 ) and mackenzie and rous ( 1941 ) in the development of malignant tumours . 
the discrepant results ( previously referred to ) concerning their incidence often suggest that they may be more sensitive criteria of the presence of the agent . if the nodular hyperplasias are to be used for any of the purposes suggested , it must be proved beyond question that they are in fact dependent for their origin and continued existence on the presence of the milk - borne tumour agent , and that the nodules , or some of them , are but an early stage of eventual malignant tumours . other possible causes of focal cell proliferation such as hormones must be excluded . the possibility has also to be considered that mice of high cancer strains carry more than one formative milk - borne stimulus for the mammary gland . one agent might be the cause of frankly malignant tumours and another the cause of nodular hyperplasias . appears more probable , however , that one and the same agent is responsible for both types of tumour , benign and malignant , but that its virulence varies . greater virulence would be understood as the capacity to stimulate the mammary gland cells to multiply and invade or metastasize within the life of the mouse ; less virulent variants would cause merely focal proliferations . 
whether the cell proliferations which it produces are benign or malignant depends upon the combination of its " virulence " with encouraging or deterrent forces . the experiments here recorded are concerned only with the origin , provocation and continued existence of the adenomatous hyperplastic nodules . was found possible to stimulate the appearance of nodules artificially with measured limited amounts of hormone at an earlier date than that at which they become detectable spontaneously . it was also possible to distinguish responses in the mammary gland due to hormone alone . responses to other formative stimuli were considered . mamnmae of female and rudimentary mammae of male mice respond to 180 b . 
the responses to single and repeated doses ' of ovarian hormones were examined at various intervals after application as described under experimental methods . the existence of a strain difference in response to oestrogens which was independent of the presence of milk - borne tumour agent was confirmed . 
a similar hormonal response was obtained in c3h mice giving rise to focal hyperplasias , but as this strain was not freed from the milk - borne tumour agent , it is uncertain , though probable , that the response to hormone alone would have given this atypical reaction . 
some were derived from pure lines , others from random breeding within the strathe incidence of spontaneous nodules of hyperplasia in the mammae in 26 virgin females segregated from males had previously been found to be 100 per cent after the age of 8 to 9 months . malignant tumour incidence in the same series was 69 per cent nodules in this strain are extremely numerous in both virgin females and breeders . r3x sublines free from the milk - borne tumour agent were bred by foster nursing an original family of 2 females and 1 male on a c57 ( black ) mother from the moment of birth . 
pullinger record was kept of the relationships of every mouse of these sublines so that , if evidence of the presence of milk - borne tumour agent subsequently reappeared , the progeny liable to be affected could be traced . 
from every litter containing more than one female , one or two were used for testing the hormone response this breeding provided further while the remainder were allowed to breed . mice for testing , and also controls to prove the absence of the milk - borne agent . the same breeding females also provided controls for all the male mice that altogether , 44 breeding females reached the average tumour were treated . age ( 81 months for this strain ) ; of these 24 were force bred owing to the circumstance that they failed to rear or destroyed their young , a habit to which many r3 females are prone . in three years no tumours were seen . 
the majority of strong a mice when two months old or over failed to survive the combination of this anaesthetic and ovariectomy . their survival could only be assured after they had reached the age of 2 months , if ether ' ere used . 
the ovaries of all mice were removed by the abdominal route ; they were excised of their oviducts ( uterine horns )  . together with about successful removal of all local oestrogen - producing tissue was judged at autopsy by complete atrophy of oviducts and uterus . vaginal smears were made from some of the females for 2 - 3 weeks before they were killed . it was necessary to examine the former site of uterus and oviducts in every mouse , because if the tissues were not excised as described , cysts containing clear fluid sometimes developed at the cut ends of oviducts after subsequent oestrogen treatment . 
when this was the case atrophy of uterus and oviducts was never complete , and the impression was gained as the result of much experience of mammary gland changes that these cysts were themselves secreting oestrogen . this difficulty was soon overcome at a time when oestrus records were not being made in spayed mice , so the matter was never settled . 
the oviducts became very slender tubes ( brownish in r3 and r3x mice ) and the uterus was greatly shrunken . oestrus cycles ceased in all those mice which were tested and did not reappear . 
any mice that had developed intraabdominal cysts or ligature abscesses , thereby possibly concealing cysts , at the cut ends of the oviducts , or whose oviducts had not undergone atrophy at the 16th to 20th weeks of experiment , were discarded . 
the purpose in using it was to give a limited measured amount of hormone within at most a few hours in order to obtain a limited response rather than a cumulative one due to prolonged irregular absorption as from oily solutions or pellets . 
the results indicate that responses in females vary quantitatively with dosage and qualitatively with strain and , within the strains , with ages younger than 49 to 56 days old . for the purpose of the present experiment most of the females received two doses of 400 microgrammes at 20 days ' interval . 
the response is visible owing to its atypical nature in respect of a milky secretion which renders ducts and clusters of acini visible . mice examined in vivo in early stages and all others were finally killed . all 10 mammary glands ( or fat pads in males ) were stained in bulk , cleared , inspected , and whole mounts made of representative mammae or those showing special features . the method of staining in bulk differed little from that described by gardner ( 1934 )  . after 4 days ' fixation in bouin 's fluid the mammae were dissected off from the skin , muscle and covering fascia with the aid of a dissecting microscope magnifying 7 and 14 times . nerve fibres were removed and some of the large blood vessels . these stripped mammae were then immersed overnight in 50 per cent alcohol , and next stained for about 4 hours in 1 part of ehrlich 's acid haematoxylin freshly diluted with 3 parts of a 2 per cent aqueous solution of after differentiating for about 10 minutes in acid alcohol ( 3 per acetic acid . cent hc1 in 50 per cent alcohol ) the stained glands were rendered blue or blueblack in several changes of 50 , then 70 per cent alcohol for as many hours or days as were required to develop a deep colour . they were next dehydrated and cleared in the usual manner . while in the first change of clearing agent ( xylol ) notes were made by the author after examining all 10 mammae or fat pads with the binocular dissecting microscope . 
the ducts were distended and filled with milky secretion , which rendered the main branches and many smaller ones visible to the naked eye in all 10 mammary glands . there was also a pseudolobular alveolar differentiation with great multiplication of acini arranged in clusters in all 10 mammary glands . 
a similar response was given by the maximum dose of 400 y of oc - oestradiol repeated at 20 days ' interval ( total 800 y ) in 15 out of 15 mice which were examined in ' ivo . 
pullinger limits of outgrowth attained during normal pregnancy . it is pathological also in that the degree of differentiation is suggestive of a 9th - 12th day pregnancy while the milky secretion is voluminous . male glands reacted to larger doses in a similar manner . 
some light on this problem was gained from experiments similar to those here described using the double dose of 400 microgrammes of oestradiol on spayed f.1 hybrid females of the c57 x r3x cross . the curious observation was made that a similar lobular - alveolar response was provokedin all the mammae , but it was localized in approximately half of each gland . 
no inflammatory or metaplastic nodules were encountered . in the course of these experiments the possibility had to be considered that in the females some other sources of oestrogens might be stimulated by ovariectomy and after cessation of the action of artificially applied hormone to produce oestrogens , as smith and bittner ( 1945 ) found in the c3h strain . that no such stimulation had occurred was proved by making vaginal smears during the last two to three weeks of the experimental period in 11 out of 20 mice , and by inspection of uterus and oviducts at autopsy . in no case was there a return of oestrus or failure of uterus and oviducts to atrophy . r3 virgin females deprived of their ovaries but containing the milk - borne tumouqr agent . early changes in the mammae in response to ovariectomy and oestrogen treatment ( ketohydroxyoestrin and oestradiol ) were similar to those described in the same strain deprived of the tumour agent ( 32 out of 32 mice )  . 
by the vaginal smear technique , oestrus in 30 cells were seen on one occasion in each of 2 mice out of 32 examined . mice oestrus cycles or cells did not recur . the contrast between the mammae in the two sets of mice at 16 to 20 weeks there was complete absence of adenomas in those mice which was striking . had been deprived of the milk - borne tumour agent , whereas in mice of the original r3 strains carrying milk agent adenomas were numerous in nearly all fig . 
a few imperfections due to incomplete regression did not cause confusion , and will be referred to in this connection again . the conclusions were drawn that the foci of hyperplasia ( adenomas ) in the r3 females carrying tumour agent , were due in respect of their origin and persistence to the presence of a milk - borne tumour agent , presumably identical with or a variant of bittner 's agent , and that this agent had been forced into activity by the large dose of - hormone . these nodules are considered to be experimentally produced counterparts of those that occur spontaneously in all r3 females after the age of 8 to 9 months . they are similar to those described in great detail , and finely illustrated by gardner ( 1942 ) in other strains . 
an average of 6 mammary glands per mouse developed from rudiments and all examined revealed the atypical response characteristic of females of this strain . irregular lobules were seen after cutaneous application of 8001200 microgrammes of oestradiol with or without 1500 microgrammes of proregression required 6 to 7 months to become complete , leaving gesterone . bare atrophic ducts ( table ii )  . r3 males containing milk - borne tumnour agent . when additional time had been allowed for regression of hormone response , results were similar , and almost as regular as in spayed females containing milkborne tumour agent . either oestrogen alone ( 1200 microgrammes ) or combined with one dose of progesterone ( 1 , 500 microgrammes ) was sufficient to stimulate the growth of adenomas ( table ii )  . 
tumours in the other line of descent behaved similarly as far as the fourth passage . three tumours of the implants of two of the tumours grew in fourth generation were transplanted . female mice but not in males . 
the two lines thus converged , without abrupt changes m beha - viour . one other br tumour ( br4 ) grew onlv in females in the first three pa& - - , ages and in the fourth grew equallv in males and females . 
thev oozed milk - v fluid when cut some discharged similar fluid through ulcerated evsts with milk - v or creamv fluid patches of skin . aahen slices of tumours were fixed in formol sahne the secretorv tumours were evident to cursorv inspection bv reason of the milkiness of th.e histological examination showed aceumulations of secretion , patchv fixative . tumour acini ' distended with secretion were contiguous with in dlistribution small . 
tumours from 12 out of 14 mice were milk - v in greater or less degree : in one of the two mice with non - milkv tumours tl ; e stilboestrol pellet was ' not found post mortem and e ' vidence of oestrogenic action on the sex organs was lacking . secretion was thus dependent on hormonal stimulation . 
the new observations support that conclusion by demonstrating two responses of establisbed transplants to hormonal variations in the host . pregnanev in females and artificiarv administered oestrogen in males elicits gross milky secretion in some transplanted eisen 's observations ( 1941 ) show similarly a pronounced though tumours . patchy secretion , in transplantable mammary carcinoma in rats . 
in response to oestrogenic stimulation above physiological levels , although transplantation was equahy successful in male and female hosts . ' " ithdrawal of oestmgen from male mice stops the secretion but growth continues after only a temporary secretion in response to hormones is a properkv independent of . 
the acceleration of growth in two transplantable stra ' during pregnancv is another specific response ; the growth of transplantable tumours in general is either unchanged or inhibited during pregnancv . 
the two responses , by secretion and by accelerated growth , are independent of each other , and each is manifest in only a minoritv of those transplantable tumours whose growth is inhibited in male hosts . the inbibition of implants in male hosts is sometimes partial or doubtful at the first transplantation or after several transfers . 
wider search would probably " close stih greater variety in the type and degree of response to hormones , and many different combinations of the relatively independent responses exempfified in the establishment of implants and in the growth and secretory activity of established tumours . 
tumour bri , whose growth at first was consistently inbibited in male hosts , lost this characteristic and grew equally in male and female hosts ; concurrently its growth accelerated . 
two other tumouir strains changed similarly under obser there is an evident tendency for hormone - responsive tumours to lose their distinctive quahties ; if suflicient opportunity is provided by repeated transplantations they attain the unresponsive state which characterizes the generahty of transplantable mamm ry carcinomata in mice . 
the hormonedependence was not correlated with lack of milk agent . pm - gnancy in females and an artificial oestrogen in males ehcited gross milky secretion in mammary tumours of some transplantable strains . 
rinaldini. from the strangeways research laboratories , cambridge . received for publication april 25 , 1952 . the nitrogen mustards have been shown to have a marked inhibitory action upon cell division , a property that warrants their inclusion in the miscellaneous group of the " mitotic poisons " ( loveless and revel , 1949 ) and their use as chemotherapeutic agents in certain forms of malignant growth ( haddow , 1947 )  . some of the 2 - chloroethylamines are mutagenic in drosophila ( auerbach and robson , 1947 ) and in neurospora ( tatum , 1947 ) , and more recently both the alkyl ( boyland and horning , 1949 ) and the aryl ( haddow , kon and ross , 1948 ) derivatives have been shown to exhibit tumour - inducing properties . the present work deals primarily with the effects of p - amino n - n - di - ( 2 - chloroethyl ) aniline hydrochloride on the number , duration and distribution of mitoses in tissue cultures during the first 1 to 3 days after exposure . 
though not very adequate for detailed cytological work because of the smallness and large number of the chick chromosomes , this material was found particularly suitable for quantitative treatment as regards variations in mitotic number and duration of the mitotic cycle . 
mitotic counts in fixed and stained cultures . this method furnishes data on the total number of mitoses and on the number of cells undergoing each phase of division at a given moment , and therefore an indirect estimation of the delay or arrest at any stage of the cycle . 
the number of abnormalities can also be ascertained . the cultures that showed the most abundant growth after two transplantations were selected , and the explants were cut in halves as closely similar in size as possible , under the dissecting microscope . 
all the solutions used here were made up in tyrode fluid . the cultures were stained with ehrlich 's haematoxylin after hydrolysis in n hydrochloric acid for 8 to 10 minutes at 600 c . 
 ( hughes and fell , 1949 )  . total mitotic counts were made in every culture . in order to facilitate counting the whole of the mitotic cycle was considered to be comprised within the period between the disappearance and the reappearance of the nucleoli . exception was made , however , for those cells in which the nucleolus persisted in advanced prophase and , conversely , for telophases in which the nucleus was fully reconstructed before completion of cytokinesis . 
low power phase - contrast cinemicrography . this method permits a direct , though only approximate , measurement of the rate of division and duration of each phase in a group of cells . for film recording the cultures were mounted in an air - tight chamber made with a metal frame between two coverslips and sealed with paraffin wax ( hughes and swann , 1948 )  . 
rinaldini the apparatus , devised by canti and lately improved by hughes , consists of a phase - contrast microscope encased in a thermostatically controlled chamber and attached to a 35 mcine camera . 
the chromosome movements can be seen in detail , and it is possible to measure accurately the duration of each mitotic phase . the technical arrangements were similar to those for the low - power film recording , except that critical focusing and phase adjustment required constant observation , and the time interval between frames was much shorter . 
rinaldini less concentrated solutions of the order of 1 : 50 , 000 to 1 : 100 , 000 - 74 x 10 - 6 and 37 x 10 - 6 molar - allowed indefinite survival and successful suboultivation , although the outgrowth was smaller than in normal cultures . 
at this stage the treated cultures showed no sign of recovery , but on the contrary there was a visible difference in the area of the outgrowth as compared with the controls . this was measured with the aid of a camera lucida as shown in fig . 
lindley using test " t " for p = 005 , the x2 analysis of contingency tables and the analysis of the variance on the square root of the counts . 
the percentage of abnormal proand metaphases taken together was approximately 35 per cent after 24 hours and 20 per cent after 48 hours , while the number of abnormal anaand telophases was only 4 per cent after 24 hours and reached 12 per cent after 48 hours . in spite of the normal appearance of the resting cells , all the evidence obtained from the counts points to the fact that almost 100 per cent of the inhibitory action was exerted during interphase . 
rinaldini no difference was found between the duration of 10 normal mitoses photographed during the first 5 hours and the last 5 hours of an experiment , nor between peripheral and central cells . 
a similar case was recorded under high magnification ( see below )  . six cells could be followed from one division to another in the control cultures . the intermitotic period varied from 5 to 20 hours , with an average of 10 - 6 hours . cells in the middle had a longer resting stage than cells in the periphery of the outgrowth . in the treated cultures no cell could be found to divide twice in one film ( 20 to 24 hours ) , but due to the scarcity of cell divisions it was not possible to decide whether the resting stage was prolonged or whether cells were prevented from dividing again . high power phase - contrast cinemicrography . the results have been reported elsewhere by hughes ( 1950 ) , and i shall only briefly summarize them here . 
with dilute solutions a large proportion of cells are prevented from entering mitosis , but no pycnosis or vacuolation appears . proand metaphase abnormalities this effect is exerted mainly during interphase . are conspicuous and anaand telophase abnormalities rare during the first 24 hours , anaphase abnormalities increasing after this period . 
the duration of the first two phases is significantly prolonged in some cells . cultures recover from these effects when transplanted into a fresh medium after 48 hours and hardly any residual effect can be detected . 
on the 4th day the males were removed from the boxes and 39 females which had shown plugs were placed in separate boxes , these constiforty - three unmated female mice of similar tuting the experimental group . average age , and wherever possible litter mates of the experimental mice , made the control group . on the day of separation , each of the mice received a subcutaneous graft , roughly 2 mx 2 mm . , in the right flank , from a 25 - day - old transplantable methylcholanthrene - induced spindle - cell sarcoma growing in cba mice . this tumour retained the original histological appearance and characters of steady and uniform growth through successive generations , and was chosen because its rapid growth was considered an advantage in view of the shortness of the pregnancy and lactation periods in mice . from the 10th day following grafting the tumours were measured every 4th or 5th day in 2 diameters ( length and breadth ) until the end of lactation , i.e. until 19 days following parturition . 
1 by curves obtained by plotting the average of the sums of 2 diameters ( i + b ) against time , as described by haddow ( 1938 )  . because of the difficulty in obtaining a large number of pregnant mice at one time , the experiment had to be performed on 6 batches of mice , 25 - day - old tumours of successive generations being used for grafting . 
and the mice were kept on a balanced diet of commercial food pellets and water ad libidum . eventually the hybrids formed the following groups . group i consists of the offspring of males no . 
1. of the original 2 sisters , the segregated one died after her first litter , and was replaced by a third sister which was also segregated for birth and rearing of her first four litters . she was left with the male for the birth of her fifth litter ( table i . ) group iii consists of the offspring of 2 females , each permanently in the cage the paired segregated sisters of each died with males no . 
two sets of unrelated sisters were mated to male no 11 . ( table ii ) ideally all the segregated females should have been sisters of the female left with the male , but this was not always possible . the result of the experiment is summarised below : c3h . 
 ( mothers kept with male ) cba.c3h 11 mammary tumours out of 82 hybrids . ( mothers segregated from male ) , , 84 the incidence is expressed as the number of mice bearing mammary tumours as numerators over the number of survivors aged 450 days ( age of youngest tumour - bearing mouse in this series ) as denominators . all these mammary tumours appearing in the hybrids were confirmed histologically by p . 
2b , segregated from the male , developcd a mammary tumour at 538 days and 387 days respectively . these tumours could be attributed to transmission of virus in the mothers ' milk , or to infection from the c3h male in each case , or they may be unrelated to the in the case of female no . 
no definite conclusion can be drawn from the occurrence of such sporadic tumours . ( b ) andervont and dunn ( 1948 ) have shown that c3h males can carry the mammary tumour virus in their vesicular glands and secretion , and have suggested that the mother may be infected during copulation . foulds ( 1949 ) has shown a similar transfer of virus by riii males to their fl hybrids with c57 black females . bittner ( 1952 ) has studied similar crosses between high and low mammary cancer strains , with and without the agent , and has reached essentially the same conclusion about the role of the male in transmitting the agent . 
iversen. * from the institute of pathological anatomy , university of copenhagen , denmark . received for publication june 11 , 1948 . earlier investigations by weigert and mottram ( 1946 ) have shown that 3 : 4benzpyrene after administration to the animal organism is metabolized to at least four different derivatives , labelled by weigert and mottram as bpx1 , bpx2 , bpf bpf . 
the diameter of the particles of the emulsion was between 6 to 15k . immediately after the emulsion was prepared it was injected intravenously in patients suffering from myeloid or lymphatic leukaemia . 
emulsion. blood samples ( one part 3 - 8 per cent sodium - citrate solution plus 9 parts blood ) were taken from a cubital vein immediately before , immediately after and at various times after the injection . 
2. - absorption curves of plasma extracted with ethanol before and after intravenous injection of 3 : 4 - benzpyrene . in order to make sure that the emulsifier ( postonal ) itself had no effect on the amount of nitrogen in plasma , 8 g . 
2 shows that the maxima of absorption characteristic of 3 : 4 - benzpyrene are , little by little , altered to maxima of absorption characteristic of the metabolites labelled as bpx1 . 
iversen the results of kjeldahl analysis on the precipitates showed that there was no noticeable difference between the percentage of nitrogen in the different samples of precipitate , which may mean that the composition of protein in plasma does not alter considerably in relation to an intravenous injection of 3 : 4 - benzpyrene , or that it varies so little that it has been impossible , with the technique used , to determine the difference . it would be possible to obtain a quantitative estimation of the proportion between the amount of unchanged benzpyrene and changed benzpyrene , and thus get an expression for the speed with which the metabolism ( or detoxication ? ) of 3 : 4 - benzpyrene takes place by determining the proportions between the extinction at 380 m , u . 
the same quotient for the x1 derivative is unknown and could not be determined , as it was not possible to obtain the x1 derivative in a pure form , but the quotient must be higher than 1 00 , as the absorption of the xl derivative is more intense at 380 m ,  . 
the curves further show that the time at which the rate of conversion is highest nearly coincides with the time at which the decrease in nitrogen - ( protein - ) conadditionally the curves indicate that tent of the plasma is most conspicuous . after the maximum concentration of changed hydrocarbon has been reached , elimination takes place at a constant speed . that the conversion may take place in the liver after an intravenous injection is an obvious consideration , and the following experiment would indicate that this is the case in rabbits : blood is transfused through a living rabbit liver ( nielsen , 1933 ) , and to the circulating blood is added 10 mg . 
3 samples of blood are taken before and at various times after the injection . shows , as in the case of human beings , that the absorption maxima of 3 : 4benzpyrene are altered gradually to the maxima of absorption characteristic of that these curves appear higher and higher on the ordinate the x1 derivatives . axis may be accounted for by the fact that it is not possible for the system to the variations in the quotient 380 / 385 m , u . 
iversen perhaps to be mentioned in this connection that the patients during , or immediately after , but never later than half an hour after the injection , sometimes got slight attacks of pulmonary infarcts . whether one considers the changes in the amount of nitrogen ( protein ) in plasma as attached to the metabolism of 3 : 4 - benzpyrene or as bearing no relation fig . 
 ( left ordinate axis )  . c and d give the corresponding relative amounts of x2 derivative calculated in the way described ( right ordinate axis )  . 1n 135150 us5 so o9 ? 0 150nt240 552t70 from fig . 
no sarcomata were found , however , and the local trauma to the squamous epithelium of the crop apparently favoured the local action of the oily solution of carcinogen . further experiments designed to assess the possible action of 2 - aaf in arachis oil eneysted in the submucous tissues of the crop have been in progress for about 4 years , so far with negative results . 
of 2 - aaf was injected repeatedly into the crop of each bird . sixteen white leghom cockerels of our inbred flock , aged 5 months at the start of the experiment were injected twice weekly for 4 months , then once weekly for a further year , and then at less frequent intervals , determined by their gene ' ral state of health . they were kept on open grass range with access to unheated fowl houses and fed twice daily with commercial poultry mash and pehets . 
no foreign body was present in the ulcer or underlying tissues . halfway along the oesophagus between the buccal ulcer and the crop , a small pedunculated translucent polyp 3 min diameter projected from the posterior wall . 
both kidneys were very mottled with white spots and small retention cysts ; the left kidney also contained a firm white tumour pressing on the sacral plexus ( cause of paralysis )  . 
3412. this bird had repeated i ' ections of a 0 - 5 per cent solution of methylcholanthrene ( mc ) in arachis oil into the wan of the crop with a total dose of 30 mg . 
for 3 months past it had had a palpable tumour in the neck and this had grow - n to a mass about 10 cin diameter when the bird was kined . 
a biopsy taken when the tumour was first noted showed a solid cehular tu ' mour with little differentiation and with a dehcate stroma with little or no intercellular substance . 
the tumour was considered to be an anaplastic carcinoma . cell suspensions from biopsy material were injected into 12 birds with negative results . material taken post - mortem showed a fleshy , spindle - cened tumour very similar histologicary to the chemically - induced sarcomata that are the usual response in fowls to injections of carcinogenic hydrocarbons . grafts of fresh tumour tissue were made into 13 birds with negative results . these 2 tumours contrast with those induced with 2 - aaf in which the diagnosis of carcinoma was in no doubt . n : n - dimethylamino8tilbene ( dmas )  . - as this siibstance has been shown by haddow and his co - workers to be a versatile carcinogen for rats it was thought that it might also prove an epitheliotropic carcinogen for the fowl . thirteen white leghorn cocks aged about 5 months were injected periodically into the pectoral muscles with 0 - 4 per cent solution of dmas in arachis oil with a total dose of from 0 - 5 g . 
to 0 - 8 g . these birds died or were killed between 78 and 208 weeks from the start of the experiment but no tumours were observed in any organ . 
the present experiment shows that 2 - aaf is similarly active against a variety of epithelial tissues ih the fowl and confirms the earlier report by bielschowsky and green ( 1945 ) that it is carcinogenic for the kidney of this species . in contrast with 2 - aaf , n : n - dimethylaminostilbene , which is also a versatile carcinogen for rats ( haddow and kon , 1947 ) , caused no tumours in fowls in our experiments . thus it seems that the epithehal tissues of the fowl are much more resistant to the action of many carcinogenic hydrocarbons than are those of rodents . however , monkeys also seem to be relatively resistant to the action of carcinogenic hydrocarbons ( pfeiffer and allen , 1948 ) , and it may be that we should rather regard the small rodents as being unusually susceptible to these agents . it is unfortunate that all attempts to transmit the 2 - aaf induced carcinomata have failed so far . 
 evidence offered by calcutt ( 1949 ) showed that 3 : 4 - benzpyrene is effective in inducing the oxidation of the - sh groups of a variety of compounds , the benzpyrene itself also undergoing oxidation during this process . 
on the basis of physical properties and fluorescence spectra it was suggested that the benzpyrene derivatives obtained in this fashion were comparable to those obtained as a result of the metabolism of the hydrocarbon by mice . 
this suggestion is important in view of crabtree 's ( 1947 ) conclusions as to the involvement of - sh groups in the carcinogenic process , and also in relation to powell and calcutt 's ( 1949 ) conclusion that the availability of sulphydryl influences the metabolism of benzpyrene . 
 studies by weigert and mottram ( 1946a , 1946b ) showed that the initial step in the metabolism of benzpyrene is conversion to either 8 : 9 - dihydro 8 : 0r1 - 9.0h benzpyrene ( bpx1 ) or 8 : 9 - dihydro 8 : 0r1 - 90r2 benzpyrene ( bpx2 ) , r 1 and r 2 being unidentified radicals . 
at the same time it was shown that these compounds were convertible by simple chemical methods , which have their counterpart in the animal body , to the final excretion products - 8.0h benzpyrene and the 5 : 8 quinone . 
 it was suggested by quick ( 1937 ) that the primary step in the metabolic oxidation of hydrocarbons is a union of cysteine with the unsubstituted aromatic ring , replacement of the mercapturic acid by a hydroxyl group occurring later . 
 there is no direct evidence for this view , but the recognized involvement between carcinogenesis and sulphur metabolism ( crabtree , 1947 ; calcutt , 1949 ) is in its favour . 
it is , however , severely criticized by boyland and weigert ( 1947 ) , who point out that phenylcysteine is excreted as phenylmercapturic acid - - - evidence which suggests that the linkage between cysteine and an aromatic compound is not easily broken in the body . 
it is apparent that such a scheme could apply equally well in the case of the chemically related benzpyrene , bpx1 or bpx2 arising from the substitution of the hydrogen of one or other of the hydroxyl groups of the primarily formed dialcohol . 
an alternative possibility in line with the perhydroxylation view is feasible since autoxidizing thiols are known to give rise to hydrogen peroxide ( schober ! , 1932 ; holtz and triem , 1937 ; schales , 1938 )  . 
 if a perhydroxylation process is the initial step in both the in vivo and in vitro oxidation of benzpyrene it appears that it should be possible - under suitable conditions - to oxidize the hydrocarbon directly with hydrogen peroxide . 
 the addition of 6 per cent hydrogen peroxide to a colloidal suspension of benzpyrene in distilled water had no effect at room temperature even when the two compounds were maintained together for long periods . 
since hydrogen peroxide contains acid as a stabi lizing agent , any derivative of the bpx1 type formed in the reaction would be expected to break down to the phenol and thence to the quinone - a sequence of events which superficially would resemble those found . 
 as an attempt to counteract any influence due to the acid the experiment was repeated using the benzpyrene colloid suspended in a clark and lubbs buffer solution at a ph of 75 . 
this time the hydrogen peroxide was added tilowly ; whilst at intervals the ph was checked , and when necessary was restored to 75 by the further addition of 02m . 
examination of the fluorescent spectra of the solution derived from the three portions gave results as below : surface : - two diffuse maxima at 420 and 440 able from fluorescence spectrum of bpx1 derived from mice . 
the likelihood of it actually being 8.oh benzpyrene is enhanced by the fact that after transfer to petroleum ether and standing for a few days it lost its blue fluorescence and achieved a barely perceptible yellowish tinge , behaviour which would be in keeping with the known autoxidation of 8.oh benzpyrene to benzpyrene 5 : 8 quinone . 
the passage of a weak solution of an authentic sample of 3 : 4 - benzpyrene 5 : 8 - quinone through the same column resulted in concentration over the previous zone , and , although the zone slowly passed down the column , no further elution or variation in solvent allowed any separation of the two zones . 
the similarity of fluorescence spectra , physical pro perties and behaviour suggests then that the material separated from the reaction mixture is similar to , even if not identical with , the bpx1 from mice and the bpx1 - like material formed in the presence of autoxidizing thiols . 
 further examination of the substances extracted from the other two portions of the original chromatograph column produced little of interest other than that the material was water - soluble in both cases . 
attempts to utilize the benzpyrene in solution in organic solvents have so far failed , the only results being the formation of small amounts of apparent 8.oh benzpyrene and quantities of various unidenti fiable products . 
furthermore , the evidence suggests that the primary reaction product is a diol closely resembling that found as the initial product of benzpyrene metabolis at the same time this primary product shows a remarkable resemblance to that found as the result of oxidation of benzpyrene in the presence of autoxidizing thiols . 
 in view of the known forma tion of hydrogen peroxide during the autoxidation of - sh groups , it seems prob able that the primary mechanism of oxidation in both cases consists of the addition of hydrogen peroxide to the hydrocarbon . 
equally , since the formation of peroxide is a phenomenon known to occur during biological oxidations ( oppen heimer and stern , 1939 ) , it seems that such a mechanism could account for the initial steps of the in vivo oxidation of benzpyrene . 
 the oxidation of 3 : 4 - benzpyrene with hydrogen peroxide and the isolation of a product similar to the benzpyrene oxidation products obtained during metabolism and during oxidation in the presence of autoxidizing thiols is de scribed . 
kennaway also of those following each one of the recognized occupations , at the time of the census . the number of deaths attributed to cancer of the lung and larynx occurring in the whole male population in each of these age groups during the years in question was obtained from material at the general register office . the comparison of the various occupations with the general population is then a sum in proportion , which gives the ratio of the number of deaths in any given occupation to those , reckoned as 100 , which occurred in the same number of males in ' the same age groups in the whole population . 
an example of this calculation is given in the earlier paper . sources of error in statistical work on death certificates . these were examined in the earlier paper ( kennaway and kennaway ; 1936 )  . the use of death certificates for statistical purposes is liable to errors which are inherent in the nature of the material and cannot be wholly eliminated . 
one must either recognize and admit these errors and correct them in any way possible , or abandon any attempt to obtain information from these data . ( 1 ) correction for period between census . - in order to compare the incidence of cancer upon different occupations one must know the number of persons following each occupation . this is learned from the census returns . 
the figures for populations used for the earlier period ( 1921 - 32 ) were those of the 1921 and the 1931 census , which were combined by means of a formula described in the earlier paper ( kennaway and kennaway , 1936 ) ; those in the present paper are from the 1931 census , which is the last taken . 
kennaway when large numbers are concerned . the immense amount of labour involved in such enquiries can be seen in the monograph on cancer of the scrotum by henry ( 1946 )  . but as none of the occupations included in the present study , with one exception , shows a very high incidence of cancer of the lung , comparable to that seen in the occupational cancers of ' the skin and bladder , this source of error is not a very serious one . ( 4 ) incorrect diagnos8is is of course a source of error in these , as in all other , in the case of death certificates received in bulk , perhaps some medical data . years after the dates of the deaths recorded , one can do nothing but exclude any certificate of which the wording suggests ( 1 ) that the cause of death did not come within the category under examination , or ( 2 ) that the diagnosis was uncertain or ill - founded ( see next section ; such certificates are made the subject of individual inquiry by the general register office )  . when such exclusions have been made , one must treat the remaining certificates as correct if any use is to be made of the material . death certificates taken for examination . the material utilized in this paper has been restricted as far as possible to cases of primary malignant growth of the lung , and of the larynx . 
when the individual occupations are examined considerable variations are found . in the earlier paper attention was drawn to the high ratio for cancer of the lung in judges , stipendiary magistrates and barristers ( 173 ) and in stockbrokers and stockjobbers ( 187 ) ; in the later period ( 1933 - 38 ) the former fell to 112 and the latter rose to 253 . the stockbrokers and jobbers also have the highest ratio among the professional workers for cancer of the larynx . the figures for roman catholic priests and monks are too small to be significant . the ratio for ministers of other religious bodies has risen ( table xx )  . 
no attempt is made here to deal with all the data on the carcinogenic action of arsenic , as this subject is under investigation by a committee of the industrial health board , but the following quotations from recent annual reports of the senior medical inspector of factories show the possible importance of arsenic in relation to cancer of the lung . 
kennaway there was a special surgical clinic dealing with lung cases , and where full x - ray and bronchoscopic investigation was practised , 42 per cent of the clinical diagnoses were wrong ( table xxiv )  . 
hence the diagnosis of cancer of the lung appears to be still very incomplete , even under favourable conditions , in spite of the great improvements which are generally stated to have been made . 
some possible causes of a real increase are considered in the next section . in the earlier paper ( kennaway and kennaway , 1936 ) we drew attention to the evidence afforded by cases of cancer of the lung in which an erroneous diagnosis was made based on nervous or mental symptoms due to metastases . 
18. ( 2 ) one must look , therefore , for some other factor to explain the increase , if there is a real increase , in cancer of the lung in recent years . 
a similar argumnent might be applied in tile case of cancer of the lung , which is not known to be prevalent in any of the lower animals . the adenoma of the lung of the mouse , and certain affections of the lung of sheep in south africa and iceland , are neoplasms of which the exact nature is uncertain . we know one instance at any rate of the susceptibility of the lung of an animal to a carcinogenic agent , namely the lung of the cat in relation to 2 - acetylaminofluorene given by the mouth ( harding , 1946 ) ; hence there is no reason to think that animals are immune to any such one obvious factor , possibly carcinogenic , to which the lung of mnan agents . alone is exposed is tobacco smoke . during the present century very considerable changes have taken place in this country in the social distribution of the various methods of smoking . there were , of course , exceptions to any rule , but roughly one might say that in the earlier part of this period men of the richer classes smoked pipes , cigarettes and cigars , and men of the poorer classes smoked pipes ; cigarette smoking was increasing among the richer women , while women of the poorer classes did not smoke . one never saw a woman scrubbing her front door - step , or hanging out the washing , with a cigarette in her mouth . the great change which has taken * a . 
of course no claim is made here that the simultaneous increases in the consumption of tobacco , and in cancer of the lung , proves any etiological connection between the two . other changes which have taken place in the same period , which no one proposes to associate with cancer of the lung , e.g. 
kennaway to summarize the evidence brought together in this section on the incidence of cancer of the lung : the higher mortality in towns , the low mortality in agricultural occupations , and the absence of social gradient , are compatible with a factor in the air , such as coal smoke . in any such comparison of urban and rural areas , the question of facilities for diagnosis must be considered . coal smoke , which is probably a decreasing contaminant of the air , does not account well for the increase of cancer of the lung . 
among various possible factors is tobacco smoke ; the consumption of tobacco has risen , and so has the percentage of it smoked in the form of cigarettes , of which the smoke is often inhaled . 
among various possible factors which have been suggested to account for the increase is tobacco smoke ; the consumption of tobacco has risen , and so has the percentage of it smoked in the form of cigarettes , of which the smoke is often inhaled ; such an effect of tobacco would accord well with the absence of social gradient . we are indebted to the registrar - general for the data considered in this paper , and also for kindly permitting us to use some figures which have not yet been made public officially . 
we have received much assistance in the classification of occupations , and on various other questions , from some members of the staff of the general register office , to whom we wish to express our gratitude . we wish to thank e . 
w.3. received for publication july 16 , 1949 . in an investigation of the body growthand tumour growth - inhibiting action of carcinogenic substances , it was found that the nature of the inhibition is profoundly influenced by the protein content of the diet ( elson and warren , 1947 ; elson and haddow , 1947 ; elson , 1949 )  . in rats maintained on a 20 per cent protein diet injection of the carcinogen usually has little immediate effect on body growth although a delayed action , resulting in rapid loss of weight followed by death , may occur later . 
carcinogenic hydrocarbon 1 : 2 : 5 : 6 - dibenzanthracene 24 hours after implantation of walker carcinoma 256 in rats maintained on a 20 per cent protein diet results in very little difference in size and weight of the tumours from those of controls . if , however , the animals are fed a 5 per cent protein diet the tumours of those similarly treated with dibenzanthracene were found to be only one - quarter the weight of those of controls when the rats were killed 13 days after implantation ( elson and haddow , 1947 )  . 
lamerton for the studies involving the localized irradiation of the tumour , it was necessary first to develop .a method whereby the rat could be held firmly in anaesthesia reasonable comfort and the tumour alone irradiated with precision . was contra - indicated , since it may affect the response of the animal to radiation . the device eventually developed is shown in fig . 
a length of transparent plastic " cloth " is held by means of two clamping bars on an aluminium base . the rat is placed under the plastic material , which is then stretched under the clamping bars . 
the edge of the plastic cloth near the rat 's head must be reinforced with a strip of cellophane one to two inches wide , which serves to hold fig . 
1. - photograph of rat in holder designed for x - ray treatment of tumour . the rat 's head down and prevents him biting his way out . the tumour itself projects through a hole in the plastic material , and can be treated by crossfire techniques without irradiation of the rest of the body . a victor kx1o plant was used , run at 140 kvp . 
lamerton direct irradiation of e8tablished tumours . for these experiments the tumours were allowed to grow untreated for 6 days after implantation . daily estimates of the size of the tumour were then made by - measurement with calipers along two axes at right angles . 
2. from the results obtained with more than 20 control animals there appeared to be no very marked difference in rate of growth of the tumour in animals maintained either on 5 per cent or on 20 per cent protein diets . 
the group maintained on the 5 per cent protein diet , however , showed considerable inhibition of tumour growth , and the tumours after the first 7 days of treatment ceased to grow and remained fairly constant in size for a considerable time . 
3. - growth of walker rat carcinoma 256 treated with x - radiation ; 250 r per day , total dose 4000 r . * rats fed on 20 per cent protein diet . rats fed on 5 per cent protein diet . gradually developed areas of necrosis , which usually become infected , and in some cases the tumour had resumed growth shortly before the death of the animal . 
lamerton for the first four days after treatment the tumours of the 5 animals comprising the 20 per cent protein diet group grew more rapidly than those of the 5 per cent protein group , and reached an average size of about one and a half times that of the low protein group . after this period the tumours of the 20 per cent protein diet animals began to decrease in size , and eventually two of them regressed completely by a " shelling - out " process and a third remained very small over a long period . 
the other two , after a considerable period of regression , eventually grew again rapidly and the animals died of the tumour about 45 days after implantation . in the 5 per cent protein group one tumour regressed completely but the others grew fairly steadily at a much reduced rate for a considerable period , eventually resuming a more rapid growth rate before the death of the animal , which occurred on the average 36 days after implantation . died 2400 s 2000 3 1600 z 1200 en 800 perioi fig . 
no cures were obtained in animals of either group . it appeared therefore that regular control of the established walker tumour could not be effected by a daily dose of 400 r , and in the next experiment the effect of a daily dose of 600 r was studied , together with the effect of changing the diet of the low protein group of animals to the high protein content at the completion of the course of radiation . x - radiation , 600 r per treatment ( total 4000 r )  . in these experiments a dose of 600 r was given daily on six days , the seventh dose being reduced to 400 r to maintain the total dose at 4000 r . in the first experiment the animals of the 20 per cent protein diet group responded well at first , and nearly all the tumours began to decrease in size after the fourth dose of radiation . although the tumours then remained small for a considerable time no complete regressions occurred , and all eventually grew again fairly rapidly , leading to the death of the animals . the tumours of the animals maintained on the 5 per cent protein diet again at first responded to the treatment by growing rather more - slowly than those of the 20 per cent protein group . 
the day following the last radiation treatment the 5 per cent protein group animals were changed over to the 20 per cent protein diet and maintained thereafter on this high protein diet . 
5. - growth of walker rat carcinoma 256 treated with x - radiation ; extended treatment with initial high dose ( 1000 r ) ; total dose 4000 r . . 
under these conditions therefore the large initial dose of radiation appears to have such a strong inhibiting effect on the tumours that a marked difference is no longer observed between the initial response of low and high protein diet animals . 
the greatest degree of tumour inhibition was obtained when the animals were maintained on a low protein diet . it has now been shown that the response of rats implanted with walker carcinoma 256 to whole body x - radiation under conditions approaching those of the " walker tumour test " is also greater in those animals maintained on the low protein diet . 
with x - ray treatment , however , it is possible to apply direct to the tumour a sufficiently large dose of radiation to bring about an adequate initial growth - inhibitory response , even in animals maintained on a high protein diet , so that the subsequent outcome of the treatment then depends almost entirely on process ( b ) , and a favourable result is thus to a very large extent dependent on a high protein content of the diet . though the results obtained may be related to some extent to the particular characteristics of the tumour used , it is very interesting to note how closely the two processes distinguished in the radiation response of the tumour follow the concepts of " intra - cellular response " and " inter - cellular response " put forward by koller and smithers ( 1946 ) from studies in clinical radiotherapy . . 
tumour regression as the result of koller and smithers suggest that "  . irradiation is initiated by an intra - cellular response , but is carried on by an inter - cellular response which follows and plays an important part in the success of any treatment . 
the inter - cellular reaction is manifested through the repair processes , and depends on the construction of the tumour tissue as a whole . this reaction is conditioned and influenced by the intra - cellular response ; in this sense it is an indirect effect of radiation it seems likely that this " inter - cellular " response may constitute an important part of what we have described as process ( b ) , and have shown to be favourably if the " inter - cellular response " is related to influenced by a high protein diet . the repair processes , then it is very reasonable to suppose that nutritional factors can affect the elimination of the tumour in radiation treatment , and indeed proteins would be of special importance in view of their known value in the healing of burns and wounds . clearly the present work can only be regarded as a preliminary study . 
lamerton implantation , inhibition of tumour growth was greatest in those animals maintained on the low protein diet , but no complete regressions of the tumour were obtained . with localized irradiation of the tumour , when the total dose of 4000 r was applied in larger daily doses , complete regression of some tumours was observed , and the most favourable results were obtained by application of an initial dose of 1000 r with extended time intervals between successive smaller doses . 
complete regression of the tumours was then obtained in about 90 per cent of the animals maintained on the high protein diet , but in only about 15 per cent of these maintained on the low protein diet . it is suggested that two effects are concerned in the response of tumours to radiation , ( a ) the initial inhibition of tumour growth , ( b ) the elimination of process ( a ) is favoured by a low the inhibited tumour and cure of the animal . protein diet , and process ( b ) by a high protein diet . we would like to express our appreciation of the interest taken in this work and the encouragement given by professor a . 
we also wish to express our thanks for grants supporting this investigation from the british empire cancer - campaign , the anna fuller fund , the jane coffin childs memorial fund for medical research and the u.s. 
powell. from the department of experimental biology , mount vernon hospital , and the radium institute , northwood , middlesex . received for publication july 29 , 1947 . preparatory to commencing some detailed work on the metabolism of 3 : 4 - benzpyrene in the skin of the mouse consideration was given to a number of experimental factors which appeared likely to affect the reproducibility of the results . 
for quantitative work some standardization of the area to be treated was the method finally adopted was to apply the solution of benzpyrene required . through a stencil cut from sheet aluminium ( 16 gauge ) , with a hole of the desired size and shape . 
as it was desired to use a volatile solvent , acetone or benzene , for the application , the question of how much solvent to use in order to apply any given standard amount of the benzpyrene was examined . 
the use of a small volume of solvent , 005 c.c. , resuited in rapid drying and the deposition of the benzpyrene as a crust of crystals over 324 g . 
bearing in mind the points raised above , a series of determinations of the amounts of benzpyrene left in the skin at various time intervals after painting the results are shown diagrammatically in fig . 
on the other hand examination of the dissected animals showed the presence of benzpyrene distributed throughout the length of the digestive tract . this suggested that the benzpvrene was being licked from the skin by the animals . confirmation of this conclusion came from watching the behaviour of the almost immediately after painting and return to the boxes furthermore , when there is more than one painted animals . they start to clean themselves . mouse in a box they lick , not only themselves , but each other . further confirmation was obtained by painting mice and fixing them to a board with adhesive tape . 
 3 : 4 : 5 : 6 - dibenzcarbazole has been tested on numerous occasions and has been shown to be a potent carcinogen in mice . ( boyland and brues , 1937 ; strong , smith and gardner , 1937 ; boyland and mawson , 1938 ; andervont , 1939 ; andervont and edwards , 1941 )  . 
 in the latter organ the changes were very severe and comprised cirrhosis and bile - duct proliferation , which proceeded to the formation of cholangiomas , as well as hepatomas . 
 as boyland and brues ( 1937 ) had suggested that naphthylamine workers might come in contact with dibenzcarbazoles during the course of their work , it was decided to re - investigate 3 : 4 : 5 : 6 - dibenzcarbazole as a potential bladder carcinogen . 
mice of the oba strain were chosen , as this strain had previously given a higher yield of bladder tumours when 2 - acetyl aminofluoi : ene was fed by stomach tube than four other strains tested ( armstrong and bonser , 1947 )  . 
as the mortality in oba mice in the first few weeks was very high , successive groups were tested at different dosage until a reasonable survival was obtained ( table ii )  . 
the oba mice were treated until death ; in strong a mice , when it was evident from the swollen state of the abdomen that much liver damage had taken place , treatment was continued for as long as the mice seemed able to support it and was then withheld until death , the interval in some cases being over 20 weeks ( table iii )  . 
the dose was not found which would permit the females to live for more than 20 weeks , although 27 out of 60 oba males survived from 20 to 49 weeks . 
 in experiment v , strong a female mice showed only a slight tendency to die early from the effects of the chemical with the dose given , 5 out of 18 dying in the first few weeks , but when once tolerance had been established the females survived rather longer than the males ( table ii )  . 
several showed such a degree of cellular irregularity in the basal layers as to be consistent with a diagnosis of early malignancy , but this diagnosis was not made unless there was invasion and destruction of the muscular coat of the stomach of such degree as to leave no doubt as to the invasiveness of the process . 
the livers were on the whole larger in strong a than in cba mice , but it was thought that some reduction in liver size occurred in the mice of the former .strain when the treatment was with drawn . 
no attempt was made to count or measure these tumours , but the impression was gained that they were , on the whole , of larger size in those mice which were treated until death than in those in which a long interval elapsed between the cessation of treatment and death . 
there was focal lymphocytic infiltration of the interstitial - tissue , proceeding to fibrosis , and after 20 weeks of treatment there was usually calcifi cation of some of the cortical tubules and of the adjacent glomerular vessels . 
it is to be noted , however , that no cba mouse survived longer than 49 weeks , while all but one strong a mouse survived into the period 40 to 59 weeks . 
at 49 weeks only one of 18 cba mice treated with the potent bladder carcinogen 2 - acetylaminofluorene was known to have developed a tumour ( armstrong and bonser , 1947 ) , whereas 5 out of 10 strong a mice were known to have hyperplasia or a benign papilloma when dying between 40 and 59 weeks . 
thus , while it cannot be stated with certainty that 3 : 4 : 5 : 6 - dibenzcarbazole administered orally is not a bladder car cinogen , no indication has been obtained which would suggest that it has any action on the bladder epithelium , although from previous experience with these strains of mice evidence of hyperplasia or papillomatosis might be expected to be forthcoming within the experimental period available . 
more strong a than cba mice had tumours at death , but the difference is not statistically significant , and may be due to the greater dose of chemical and the longer survival period in strong a than in cba mice ( table iv )  . 
when it is taken into account that the incidence of carcinomas was identical in the two strains , despite the shorter survival period and smaller dose in cba mice , it would appear probable that cba is the more susceptible stra from table iii it is seen that these tumours of the forestomach are not dependent upon the continued administration of the carcinogen for the main tenance of their growth , as the chemical was discontinued for an average of 10 l weeks before the death of strong a mice , the range being o to 22 weeks . 
 it is rather surprising that papillomas of the forestomach were so rarely observed when tar was applied to the skin of mice , twort and twort ( 1932 ) having observed only occasional papillomas in 60 , 000 mice so treated . 
it seems clear that 20 - methylcholanthrene , 3 : 4 - benzpyrene and 1 : 2 : 5 : 6dibenzanthracene are carcinogenic in this sense , the latter having produced one benign tumour ( beck , 1946 ) and several malignant ones ( lorenz and stewart , 1948 )  . 
from the observations so far reported it is necessary to administer the chemical by the oral route , as no similar tumours were found after skin painting or subcutaneous injection . 
the reasons given by beck ( 1946 ) may account for this : the presence of the mucus barrier , the mucus flow tending to remove the carcinogen from contact with the cells , the possibility that contact between a carcinogen and a resting cell may not be sufficient to induce neoplasia , and finally the possibility that glandular epithelium is essen tially less susceptible than squamous epithelium to the type of carcinogen under discussion . 
there seems to be little support for the latter suggestion when the recent work ( horning , 1946 ; pan and gardner , 1948 ) on the induction of tumours by carcinogens in glandular epithelia in implants is considered . 
carcinomas of the intestine were not observed , in contrast with the results of lorenz and stewart ( 1946 ) , who noted such tumours in strain a and other mice which received aqueous emulsions of 20 - methylcholanthrene and 1 : 2 : 5 : 6 - dibenzanthracene . 
 amines are not without a similar action on the epithelium of the forestomach , papillomas having been observed in one riii , one oba and 2 strong a mice at 77 , 74 , 69 and 65 weeks respectively of treatment with 2 - acetylamhi.ofluorene in addition , otsuka ( 1935 ) described papilloma ( armstrong and bonser , 1947 )  . 
bonser seems possible that perforation of the stomach might have occurred during intu bation , resulting in a false passage of the tube into the muscles of the posterior abdominal wall and consequent injection of . 
in the course of observation of the cba strain for 17 years ( unpublished observation ) , one spontaneous spindle - cell sarcoma has been found and , therefore , the possi bility of a spontaneous origin of the tumour in mouse 10 cannot be completely excluded . 
contrary to the experience of andervont and edwards ( 1941 ) , this sex difference was observed only in the early weeks of the present experiment in strain a mice ( table iii )  . 
 in comparing the degree of liver damage in the two strains , it is evident that both suffered severely , but that the incidence of hepatomas was greater in strain a mice than in cba , the proportion of histologically malignant tumours being also greater . 
not only were hepatomas more abundant and more malignant in strong a mice than in cba with the latter chemical , but cirrhosis and bile - duct proliferation were a marked feature in both strains . 
although a high incidence of hepatomas was observed in cba mice ( but not in strong a mice ) when treated with 2 - acetylaminofluorene ( armstrong and bonser , 1947 ) , cirrhosis was absent and bile duct changes were minimal . 
it would appear possible that the chief action of 2 - acetylaminofluorene is to enhance the tendency to hepatoma already hereditarily present in cba mice , whereas 3 : 4 : 5 : 6 - dibenzcarbazole damages the liver parenchyma in such a way that changes are set in train which eventually lead to tumour formation ( orr , 1940 )  . 
 an experiment is described in which mice of the strong a and cba strains received by stomach tube , twice weekly , an oily solution of 3 : 4 : 5 : 6 - dibenzcar bazole , with a view to testing this substance as a bladder carcinogen . 
 no bladder epithelial changes were observed during an experimental period which would have sufficed to show , in these strains , hyperplasia and early tumour formation had 2 - acetylaminofluorene been the carcinogen . 
3. received for publication april 21 , 1951 . studies of the electrophoretic behaviour of sera from patients bearing malignant and non - malignant tumours have been carried out by various workers with the view to their utilization as diagnostic or prognostic tests for cancer . 
polarography has also been investigated as a possible clinical tool for diagnosis or prognosis following brdicka 's ( 1933 ) discovery that proteins give a characteristic " catalytic double wave " in ammoniacal cobalt salt solutions . applications of this method to the study of sera have shown differences between specimens obtained from normal and pathological cases , and the results of an examination of over 100 sera from cancer subjects has been published by one of us ( butler , although good correlation between the wave height and the pathological 1951 )  . condition was obtained , a number of false positive and false negative results were included , the latter particularly in cases of cancer of the buccal cavity and skin . the electrophoretic behaviour of sera has been discussed by a number of workers ( seibert , seibert , atno and campbell , 1947 ; petermann and hogness , 1948a , 1948b ) , and the most consistent changes found in pathological conditions were increases in the c1and a2 - globulin levels . however , no specific changes have been found for any particular clinical conditions ( mides , alling and morton , 1950 )  . the work of winzler and his colleagues ( winzler , devor and mehl , 1947 ; winzler , devor , mehl and smyth , 1948 ; winzler and smyth , 1948 ; mehl , humphrey and winzler , 1949 ; mehl , golden and winzler , 1949 ; weimer , mehl and winzler , 1950 ) , has shown that a mucoprotein , isolated from normal plasma , appears to be responsible for the polarographic filtrate wave . this mucoprotein migrates in the al - globulin fraction , when examined electrophoretically at ph 8 ' 4 in barbiturate buffer . it has an isoelectric point at ph 1 ' 8 and still has a negative charge at ph 4 ' 5 . 
the acidic protein fraction demonstrated in cases of gastric cancers by petermann and hogness ( 1948b ) has been shown to be a similar mucoprotemayer ( 1942 ) had previously isolated a " mucoid - like substance " from horse serum which he claimed was the polarographically active seibert et al . 
 ( 1947 ) showed that increases in a2 - globulin were paralsubstance . leled by increases in the polysaccharide content of the serum . these results suggest that the polarographic and electrophoretic patterns of cancer sera may be due to mucoproteins which migrate in the a - globulin group . 
the results were expressed either as the height of the filtrate wave , or as the protein index of muller and davis ( 1947 ) or as the blood index ( butler , 1951 )  . the results of the electrophoretic measurements were expressed in terms of the areas ( measured by means of a planimeter ) under each of the peaks of the descending differential patterns ( longsworth and macinnes , 1940 ; svensson , 1943 )  . 
the relative composition was expressed by computing the percentage contribution of the area under any one peak with respect to the area under the whole pattern , excluding the boundary anomaly . 
a statistical evaluation of the results was therefore necessary in order for this an estimation of the change in per cent to draw any valid conclusions . and absolute composition from the normal to the pathological condition was made . 
no such increase in this fraction was observed in the two lymphosarcoma cases investigated here , nor in any of the three cases investigated by petermann , karnofsky and hogness ( 1948 )  . calculation of correlation coefficients between the component peak areas and the polarographic fitrate wave heights ( f ) and blood indices ( bi ) indicate significant relationships between the ocl - globulin area and the filtrate wave heights and blood indices factors in the pathological group . it is of interest and importance that no correlation between the ocl - globulin content and the polarographic factors was found in the normal group , and similarly none of significance if the normal and pathological groups are considered as one population . this is demonstrated in the correlation diagram shown in fig . 
3. correlations between the oq - globulin content and the polarographic indices were not found when percentage composition was considered , indicating that complications by other variable factors may occur . calculations of the correlation coefficients and inspection of the correlation diagrams shown in fig . 
correlations between the serum composition and polarographic factors are discussed , and their relation to the suggested anomalous mucoprotein content in the ocl - globulin fraction is indicated . we wish to thank d . 
the investigation has been supported by grants from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund and the u.s. 
kreyberg. from the institutt for generell og eksperimentell patologi , universitetet i oslo . received for publication february 19 , 1952 . in many countries the statistical reports show a steady and remarkable increase in the number of deaths from " lung cancer . " the problem puzzles the cancer specialists and troubles the public and the medical profession . does this increase signify a real augmentation of cases of lung cancer , or does it simply mean an increasingly better diagnostic service ? this question will not be discussed in this paper . if we wish , however , to study , by statistical methods , the possible role of certain irritants in the genesis of lung cancer we have to make clear what we mean by the term " lung cancer . " according to kennaway and kennaway ( 1947 ) their statistics from england and wales comprise : " cancer , carcinoma , or sarcoma of lung , bronchus , pleura , root of lung , hilum of lung , lung and mediastinum , or jung and pleura . 
the norwegian " statistisk sentralbyra " has , since the first of january , 1951 , acted accordingly . it is a great step forward . in order to study a possible relationship between lung carcinoma and smoking habits , or industrial irritants , it may be of importance , not only to exclude all other lung tumours than primary lung carcinomas , but even to subdivide the latter into special sub - groups . from our general experience in the field of cancer research we are ever more impressed by the importance of the study of the geographical distribution of the different manifestations of malignant disease . this different geographical distribution examined on the background of the corresponding difference as to races , primary epithelial . 
this report deals with 100 consecutive cases ofprimary epithelial lung tumourb , received for diagnosis at the institute of pathology , at the university all , but also only those , tumours are included , where the piece of tissue of oslo . o 60 1929 1939 fig . 
1. - mortality statistics from norway , 1929 to 1949 ( " statistisk sentralbyroa " )  . was large enough to permit a definite histological classification . the main part of the material ( 97 cases ) was received from the surgical department a , at the university hospital , 2 cases came from the ear , nose and throat department , and 1 case from the roentgen - radium department . hereto are added 5 cases of secondary lung tumours , received within the same period , and clinically regarded as primary tumours , the histological examination , however , revealing their true character ( 2 cases of metastasizing thyroid adenoma , and 1 case each of hypernephroma , adenocarcinoma of uterus and malignant naevus tumour )  . the 100 tumours of the main series were classified according to traditional terminology as follows : 114 l . 
10 the number and the different types of tumours of our main series may be seen , as well as the occurrence in age - groups and the distribution between the two sexes . 
the individual tumours of groups g and f are tabulated in table ii . the groups e , f and g do not show any marked preponderance in the one further , these tumours are rather evenly distributed in the sex or the other . different age - groups , and they occur even in very young people , our youngest patient being a girl of 19 with a malignant adenoma . 
as to the microscopical classfication , he has : adenocarcinomas 4 - 6 per cent , squamous cell carcinoma 62 - 9 per cent , undifferentiated carcinoma 25 1 per cent and uncertain type 7 - 4 per cent . here again the similarity is greater when we examine the material on the basis of the more objective characteristic the distribution in age - groups than on the basis of the more subjectively influenced classification in histological types . it is evident that the surgical material cannot , without a closer examination , be taken as representative for the occurrence and the distribution of lung carcinomas and lung tumours in the population . firstly , cases occurring in old age 118 l . 
kreyberg will not be represented , as these patients are poor operative risks and seldom secondly , in old age the diagnosis may be more difficult and operated upon . possibly not pursued with the same enthusiasm as when the patient is a younger . it is not unlikely that the local thirdly , the sex distribution may be different . doctor , the surgeon and the patient himself will take a greater risk and show a somewhat more heroic attitude towards the question of operation when the patient is a male . 
the women in these age - groups may possibly show more resigfourthly , surgical material may show a greater nation to the blows of fate . number of benign and moderately malignant tumour types than the sum total . this is significant when the material examined includes all primary epithelial lung tumours , but less important when only true bronchogenic carcinomas are this underlines the importance of a careful classification when statisconcerned . tics are to be compared . 30 ~2021 - 30 31 - 40 41 - 50 51 - 60 61 - 70 71 - 80 81 - 90 age groups fig . 
the occurrence of a certain number of cases in the early age - groups indicates that a few adenomas are included also in this post - mortem series . i wish to emphasize that the present paper represents a preliminary orientation only , as to the occurrence of lung carcinomas in norway . 
parsons. from the department of chemistry , the university , manchester , 13 , and the royal eye hospital , southwark , london . received for publication august 15 , 1949 . the effects of injection of the four nucleotides obtained from ribonucleic acid on the tissues of normal and tumour - bearing mice have been described ( barakan , barker , gulland and parsons , 1948 ; parsons , gulland and barker , further experiments have now been carried out to note the action 1947 )  . of purine and pyrimidine bases on sarcoma growth , and to correlate if possible the biological activities of the compounds with their chemical structure . these experiments fall into two groups : ( a ) those relating to the amino and hydroxy purines , ( b ) those relating to uracil and its derivatives . both pure - line and stock mice were grafted with homologous or heterologous sarcomas , including c57 and s37 and the crocker sarcoma , the latter known to be very refractory to inhibitory action ( badger , elson , haddow , hewett and robinsoir , 1942 )  . 
the technique for treatment of the grafted mice was similar to that previously described , but the standard dose ( 0025 g . ) was reduced in proportion to the toxicity of any particular compound , or where the condition of the mouse necessitated this . insoluble or relatively insoluble compounds such as xanthine , guanine , adenine or hypoxanthine were administered as fine suspensions in the same media as used for the soluble compounds . examination of the tissues at varying intervals showed that all compounds injected as suspensions were rapidly removed within 24 hours with the exception of guanine , the relative inactivity of which on tumour growth seems to be due to its marked insolubility . deposits of the injected guanine were found at the site of injection long after the last dose . table i summarizes the results obtained . 
the total number of control mice was in all cases the same as the total number of treated mice . the amino and hydroxy purines . it had been noted that adenylic acid or adenosine produced shock when injected into mice , and it seems probable that this effect was due to the adenine radical , of which the pyrimidine ring is in a lower state of oxidation than those of the other compounds used which do not induce shock . injection of adenine in doses comparable with those used for adenosine or adenylic acid has been found to cause immediate and profound shock with heavy mortality , the minimum sublethal dose being 0005 g . 
parsons radical , but may be connected with the presence of the amino group in position 6 in the adenine radical . xanthine injected in tumour - bearing mice was removed from the tissues injected into in 24 hours , but no inhibition of sarcoma growth was observed . normal mice in doses of from 0 - 02 - 0 * 025 g . 
kirby. from the research department , glasgow royal cancer hospital . received for publication february 8 , 1947 . the exceptional interest of 2 - acetylaminofluorene ( aaf ) as a carcinogen was clearly revealed by wilson , deeds and cox ( 1941 ) , who fed it to inbred albino rats in which only benign mammary tumours had been observed , and found carcinomas of the liver , breast , bladder , ureter , renal pelvis , colon , pancreas , lung and skin , a myogenic sarcoma , and in two cases liver lesions resembling leukaemic infiltration . 
the results of bielschowsky ( 1944 a and b ) and other workers are summarized later in this paper . in cba mice , neoplasms of liver and uterus ( one a sarcoma ) and of the urinary bladder were found by armstrong and bonser ( 1944 )  . bielschowsky and green ( 1945 ) reported a carcinoma of the kidney in a rhode island red cock which had been fed aaf for 45 weeks . the widespread variety of organs affected by aaf led bielschowsky ( 1944b ) to try to induce tumours of the goitrous thyroid gland with this substance . solid , parenchymatous goitre was induced by allyl thiourea ; in conjunction with aaf , also orally administered , allyl - thiourea induced adenoma in 9 out of 10 rats , while malignancy was observed in 3 of these rats . griesbach , kennedy and purves ( 1945 ) claim that the goitrogenic agent in brassica seeds can cause adenoma of the thyroid if given orally for long enough , but only 1 of 8 wistar rats developed such a lesion . subsequently purves and griesbach ( 1946 ) obtained malignant changes in 2 out of 30 wistar rats given thiourea in their drinking water for nearly two years . purves and his co - workers consider that the effect of the goitrogens is indirect , operating by inducing hypersecretion of the thyrotropic pituitary hormone . 
aaf has no specific action even on adenomatous thyroid tissue . the success achieved by bielschowsky in at least accelerating malignant changes .in the thyroid of rats by feeding aaf suggested that other organs apparently untouched by aaf alone might undergo neoplastic changes when stimulated to proliferate by suitable means . 
the sex - organs of the rat can be caused to hypertrophy by the administration of the appropriate sex - hormone , and it was thought that these organs , thus caused to proliferate , might proceed to malignant changes when influenced by orally administered aaf . 
the basal diet for all groups was rat - cake made to the formula of thomson ( 1936 )  . 2 - aminofluorene was synthesized from fluorene by the method of diels ( 1901 ) , * and acetylated as follows . 
up to 1 per cent of concentrated sulphuric acid was added to 2 - aminofiuorene stirring in an excess of acetic anhydride which became very hot and dissolved the amine . after chilling thoroughly the acetylated amine was filtered on a sintered - glass sufficient water was added to cause funnel , and dissolved in hot ethanol . permanent turbidity and the solution well cooled . 
emmens pointed out that absorption during the second month would be much reduced , and recommended the use of 20 mg . therefore thin disc - shaped pellets weighing 20 mg . 
a spindle - cell sarcoma of the left seminal vesicle was found in rat 354 ( group iib ) , and a whorled , spindle - cell sarcoma was found lying above the liver of rat 339 ( group iia )  . 
the reason for this may well be that suggested by these workers , namely that " the hyperplasia of target organs of sex - hormones is a functioning hyperplasia , whereas that induced in the thyroid by goitrogenic agents is non - functionthus the type of hyperplasia induced by bielschowsky in the rat thyroid ing . " in which growth is accompanied by loss of differentiation would appear to have been a suitable basis for carcinogenesis , whereas the hyperplasia associated with increased differentiation induced in sex organs by over - stimulation with sexhormones is apparently unsuitable . 
illustrate a " carcinoma arising adjacent to the external auditory canal , " and discuss the histogenesis of this and other tumours in this locality included by them under " subcutaneous tumours . " bielschowsky first drew attention to tumours of the ductus acusticus externus as a separate entity . 
as wistar rats were also used by bielschowsky , who found these tumours in 18 / 93 rats given aaf orally up to 210 days , the influence of diet seems to have some importance . 
when allyl - thiourea was also given , the incidence of tumours rose to 6 / 10 . lopez ( 1945 ) also found external meatus tumours in 2 / 4 rats . 
hence the action of aaf on proliferating mammary tissue was only slight in our experiments . in the matter of liver tumours , our series has yielded results in full accordance in our series , a . 
the types of liver tumours seem to be essentially the same as in wistar rats . this is also true of the liver tumours obtained by bielschowsky in piebald rats , in which the sex - ratio is also maintained and the in the sherman strain , cantarow et al . 
found the incidence much the same . incidence of liver tumours in female rats raised when oestradiol dipropionate was injected intramuscularly ; but the complete absence of liver neoplasms in rats given thiouracil was much more striking . 
the latter group ate less of the aaf diet than did controls receiving no thiouracil , but more than the oestrogenized rats . the incidence of mammary tumours in piebald rats was very low compared with that in wistar rats on the same diet ( bielschowsky , 1946 )  . but the incidence of tumours of the ductus acousticus externus was much higher in the piebald rats , in which tumours of the small intestine were also much more frequent . moreover , lung tumours were found in this strain , but have not been reported in wistar rats given aaf and were not found in our series , although one control female ( group ia ) was found to have undifferentiated bronchial carcinoma . the albino rats of wilson et al . 
the latter have not been found in any other strain of rat , and tumours of the kidney and bladder only once each . it would seem that , if sufficient strains of rat were employed , possibly no site in the body would be found immune from the carcinogenic action of aaf . 
in the strains so far tested , only mammary tissue among the sex - organs seems to be susceptible , and this tissue is liable to develop carcinoma due to the action of sarcomas are rare , and are not induced by subcutaneous oestrogens alone . injection of aaf , at least in wistar rats . in our series , a whorled , spindle - cell sarcoma was found in the omentum covering the left lateral lobe of the liver in one rat , and a spindle - cell sarcoma was present in the left seminal vesicle of another . it remains to discuss a few other points of interest . toxic damage to kidneys was seen in some animals of all groups ; rats receiving oestradiol benzoate pellets , with or without aaf , tended to show degeneration of the epithelium of the first and second convoluted tubules with the presence of a dark yellow a . 
kirby pigment in these cells . there was no consistent evidence of toxic damage to the kidneys by aaf or its metabolites , nor were any tumours of this organ seen . no tumours of the uterus were found , but all females receiving oestradiol benzoate had pyometra , which often made it necessary to kill the animal ; the 2 females receiving the male sex - hormone had no pyometra . the spleens of the control groups , ia and ib , showed no abnormality . 1 female in group iia and 1 male and 2 females in group iib had enlarged spleens , due to lymphoid hyperplasia . there was no question , however , of the regular , early , gross enlargement of the spleen seen in rats ingesting azo - compounds it may be ( smith , lillie and stohlman , 1943 ; kirby and peacock , in press )  . concluded that no splenotoxic substance passes from the liver into the blood of rats fed aaf ; rats fed p - aminoazobenzene ( aab ) or its n - monomethylor n , n - dimethyl - derivatives ( mab and dab ) have aab circulating in the blood and affecting the spleen ( miller , miller and baumann , 1945 )  . the rats given aaf orally in the experiments described in this paper developed tumours of the liver predominantly in the right lobes ; tumours in the left side of the liver were usually smaller or absent . 
a similar predominance of tumours in the right side of the rat liver has been reported by opie ( 1944 ) in rats fed dab in diets not inducing cirrhosis . 
 3 : 4 : 5 : 6 - dibenzcarbazole has been tested on numerous occasions and has been shown to be a potent carcinogen in mice . ( boyland and brues , 1937 ; strong , smith and gardner , 1937 ; boyland and mawson , 1938 ; andervont , 1939 ; andervont and edwards , 1941 )  . 
 in the latter organ the changes were very severe and comprised cirrhosis and bile - duct proliferation , which proceeded to the formation of cholangiomas , as well as hepatomas . 
 as boyland and brues ( 1937 ) had suggested that naphthylamine workers might come in contact with dibenzcarbazoles during the course of their work , it was decided to re - investigate 3 : 4 : 5 : 6 - dibenzcarbazole as a potential bladder carcinogen . 
mice of the oba strain were chosen , as this strain had previously given a higher yield of bladder tumours when 2 - acetyl aminofluoi : ene was fed by stomach tube than four other strains tested ( armstrong and bonser , 1947 )  . 
as the mortality in oba mice in the first few weeks was very high , successive groups were tested at different dosage until a reasonable survival was obtained ( table ii )  . 
the oba mice were treated until death ; in strong a mice , when it was evident from the swollen state of the abdomen that much liver damage had taken place , treatment was continued for as long as the mice seemed able to support it and was then withheld until death , the interval in some cases being over 20 weeks ( table iii )  . 
the dose was not found which would permit the females to live for more than 20 weeks , although 27 out of 60 oba males survived from 20 to 49 weeks . 
 in experiment v , strong a female mice showed only a slight tendency to die early from the effects of the chemical with the dose given , 5 out of 18 dying in the first few weeks , but when once tolerance had been established the females survived rather longer than the males ( table ii )  . 
several showed such a degree of cellular irregularity in the basal layers as to be consistent with a diagnosis of early malignancy , but this diagnosis was not made unless there was invasion and destruction of the muscular coat of the stomach of such degree as to leave no doubt as to the invasiveness of the process . 
the livers were on the whole larger in strong a than in cba mice , but it was thought that some reduction in liver size occurred in the mice of the former .strain when the treatment was with drawn . 
no attempt was made to count or measure these tumours , but the impression was gained that they were , on the whole , of larger size in those mice which were treated until death than in those in which a long interval elapsed between the cessation of treatment and death . 
there was focal lymphocytic infiltration of the interstitial - tissue , proceeding to fibrosis , and after 20 weeks of treatment there was usually calcifi cation of some of the cortical tubules and of the adjacent glomerular vessels . 
it is to be noted , however , that no cba mouse survived longer than 49 weeks , while all but one strong a mouse survived into the period 40 to 59 weeks . 
at 49 weeks only one of 18 cba mice treated with the potent bladder carcinogen 2 - acetylaminofluorene was known to have developed a tumour ( armstrong and bonser , 1947 ) , whereas 5 out of 10 strong a mice were known to have hyperplasia or a benign papilloma when dying between 40 and 59 weeks . 
thus , while it cannot be stated with certainty that 3 : 4 : 5 : 6 - dibenzcarbazole administered orally is not a bladder car cinogen , no indication has been obtained which would suggest that it has any action on the bladder epithelium , although from previous experience with these strains of mice evidence of hyperplasia or papillomatosis might be expected to be forthcoming within the experimental period available . 
more strong a than cba mice had tumours at death , but the difference is not statistically significant , and may be due to the greater dose of chemical and the longer survival period in strong a than in cba mice ( table iv )  . 
when it is taken into account that the incidence of carcinomas was identical in the two strains , despite the shorter survival period and smaller dose in cba mice , it would appear probable that cba is the more susceptible stra from table iii it is seen that these tumours of the forestomach are not dependent upon the continued administration of the carcinogen for the main tenance of their growth , as the chemical was discontinued for an average of 10 l weeks before the death of strong a mice , the range being o to 22 weeks . 
 it is rather surprising that papillomas of the forestomach were so rarely observed when tar was applied to the skin of mice , twort and twort ( 1932 ) having observed only occasional papillomas in 60 , 000 mice so treated . 
it seems clear that 20 - methylcholanthrene , 3 : 4 - benzpyrene and 1 : 2 : 5 : 6dibenzanthracene are carcinogenic in this sense , the latter having produced one benign tumour ( beck , 1946 ) and several malignant ones ( lorenz and stewart , 1948 )  . 
from the observations so far reported it is necessary to administer the chemical by the oral route , as no similar tumours were found after skin painting or subcutaneous injection . 
the reasons given by beck ( 1946 ) may account for this : the presence of the mucus barrier , the mucus flow tending to remove the carcinogen from contact with the cells , the possibility that contact between a carcinogen and a resting cell may not be sufficient to induce neoplasia , and finally the possibility that glandular epithelium is essen tially less susceptible than squamous epithelium to the type of carcinogen under discussion . 
there seems to be little support for the latter suggestion when the recent work ( horning , 1946 ; pan and gardner , 1948 ) on the induction of tumours by carcinogens in glandular epithelia in implants is considered . 
carcinomas of the intestine were not observed , in contrast with the results of lorenz and stewart ( 1946 ) , who noted such tumours in strain a and other mice which received aqueous emulsions of 20 - methylcholanthrene and 1 : 2 : 5 : 6 - dibenzanthracene . 
 amines are not without a similar action on the epithelium of the forestomach , papillomas having been observed in one riii , one oba and 2 strong a mice at 77 , 74 , 69 and 65 weeks respectively of treatment with 2 - acetylamhi.ofluorene in addition , otsuka ( 1935 ) described papilloma ( armstrong and bonser , 1947 )  . 
bonser seems possible that perforation of the stomach might have occurred during intu bation , resulting in a false passage of the tube into the muscles of the posterior abdominal wall and consequent injection of . 
in the course of observation of the cba strain for 17 years ( unpublished observation ) , one spontaneous spindle - cell sarcoma has been found and , therefore , the possi bility of a spontaneous origin of the tumour in mouse 10 cannot be completely excluded . 
contrary to the experience of andervont and edwards ( 1941 ) , this sex difference was observed only in the early weeks of the present experiment in strain a mice ( table iii )  . 
 in comparing the degree of liver damage in the two strains , it is evident that both suffered severely , but that the incidence of hepatomas was greater in strain a mice than in cba , the proportion of histologically malignant tumours being also greater . 
not only were hepatomas more abundant and more malignant in strong a mice than in cba with the latter chemical , but cirrhosis and bile - duct proliferation were a marked feature in both strains . 
although a high incidence of hepatomas was observed in cba mice ( but not in strong a mice ) when treated with 2 - acetylaminofluorene ( armstrong and bonser , 1947 ) , cirrhosis was absent and bile duct changes were minimal . 
it would appear possible that the chief action of 2 - acetylaminofluorene is to enhance the tendency to hepatoma already hereditarily present in cba mice , whereas 3 : 4 : 5 : 6 - dibenzcarbazole damages the liver parenchyma in such a way that changes are set in train which eventually lead to tumour formation ( orr , 1940 )  . 
 an experiment is described in which mice of the strong a and cba strains received by stomach tube , twice weekly , an oily solution of 3 : 4 : 5 : 6 - dibenzcar bazole , with a view to testing this substance as a bladder carcinogen . 
 no bladder epithelial changes were observed during an experimental period which would have sufficed to show , in these strains , hyperplasia and early tumour formation had 2 - acetylaminofluorene been the carcinogen . 
as - there was some doubt as to the absolute validity of this control method , we computed the number of cancer cases which would be expected , based on the morbidity figures from the cancer registry and on the official mortality statistics . 
rather unusual for twin studies of this kind . griginally all hospital cancer cases from the danish population of 4 million through six years , or an annual - number between 5000 and 6000 cases , but this figure must be reduced by about 20 per cent in which the questio ' n about twin birth had been left unanswered , giving a total very near to 30 , 000 cases ( 29 , 458 )  . the system of notification involves a rather heavy toll of omissions , vet it has functioned satisfactorily . 
the special questions asked twins with cancerbesides such items as name , address , ' occupation and the like - were confinea to previous diseases of a more serious character , including diagnosis and the date , in order to identify whether the twins were molloand place of treatment . zygotic or dizygotic , questions were asked about the similarity and about mistakes made by parents or others , and similarly about type and colour of hair , colour of eyes , stature , height and weight on the whole it may be said that we demanded almost full congruity before accepting a pair as monozygotic . 
the final distribution of dizygotic twins on groups of same and opposite sex , and the proportion between monozygotic and dizygotic pairs seem to show that our measures have been justified . it should be stressed that we have not been in - a position to contact the patients or their twins personally . 
the official percentage of twin births in denmark for the years 1926 - 30 is 1 - 64 , and considering the increased mortality among twin babies we ' think this a satisfactory correspondence . another check on the result was obtained through computation of the number of deaths expected from all causes among twins for whom notifications were satisfactory . 
among dizygotics we expected 36 - 3 and found 26 . these differences are not statistically 'significant , and they may be partially due to the less efficient information about those pairs of which one partner has died . in denmark , as elsewhere , the girl - boy ratio at birth is 0 , 97 with a male excess , which in the course of a fev years changes to a slight female preponderance . however , we find among both monozygotic pairs and dizygotic pairs of opposite sex a female preponderance of 1 , 48 to 1 , and 1 , 64 among the same - sexed dizygotic pairs , making 1 ' 53 for the total . 
the explanation of this considerable female excess m our material no doubt must be ascribed to the higher cancer incidence among females than among males in denmark , combined with the earlier age - in which female cancers arise . 
and , if we calculate the percentage of opposite - sexed twin pairs in our material , a figure which should be uninfluenced by the difference in mortality among the two sexes , we find exactly the same value as in the corresponding official birth statistics - 36 , 2 per cent . in spite of these satisfactory results , it should be remembered that in dealing with twin - pairs , of which at least one is suffering from old - age disease like cancer , we must expect insufficient information from twins in cases where the partner died in childhood . therefore we have excluded the twin - pairs where one partner bas died before the age of 5 years . similarly we have lost sight of a number of cc second " twins through emigration and similar events , so that the number has shrunk ' from 336 to 185 pairs . 
3. given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . since 1944 we have taken a detailed family history from all patients reporting with carcinoma of the breast . 
we have 459 family records up to the end of 1947 which are reasonably complete . so far we have not succeeded in supplementing these histories , taken at the time of first visit to hospital , by later questions to the surviving patients or by arranging visits to their homes or relations . 
some attempt has been made to confirm the causes of death of relatives by letters to hospitals , doctors and the registrar - general 's department , but such confirmation has , as yet , been obtained in only a few cases . our figures , therefore , contain all those errors of inadequate information and faulty recollection that one would expect from data collected . 
many people die of cancer without their relations knowing that this was the cause of death . it is in fact surprising how successful a woman can be in concealing a cancer of the breast from her nearest relatives living in the same house with her . it is not , therefore , so surprising that more distant relatives , or even close relatives living away from home , may be unaware of the nature of the illness involved relations , even some of an older generation , who are still living at the time that the patient is first questioned may later develop malignant disease . 
orr. from the department of pathology , univer8ity of birmingham . received for publication may 7 , 1953 . when a carcinogenic agent is applied to the skin of a mouse epithelial hyperplasia follows in the course of a week or two . if the applications are then stopped , the epidermis reverts to a histologically normal appearance , but if hyperplasia is again induced by the co - carcinogen croton oil , tumours of the skin will in due course be elicited . it is clear that the apparently normal skin has been altered in some way by quite a short treatment with carcinogen ( a single application of a powerful carcinogen will suffice ) , so that further growth - stimulation by an agent not itself carcinogenic completes the process of tumour induction . attention was first drawn to this phenomenon by berenblum ( 1941 )  . 
mottram ( 1944 ) showed that a single application of 3 : 4 - benzpyrene would suffice to produce tumours if followed by a course of croton oil paintings . in a full analysis of the factors involved , berenblum and shubik ( 1947 ) adopted the terminology of friedewald and rous ( 1944 ) , the effect of the preliminary carcinogen being described as the " initiating " factor , and that of the croton oil ( co - carcinogen ) as the " promoting " factor . both these factors were conceived as causing changes in some of the epithelial cells themselves . there is evidence , however , that the effects of carcinogens are not attributable wholly to the direct changes brought about in the epidermis . various authors have drawn attention to the progressive changes that occur in the dermis during experimental carcinogenesis of the skwhen the technique of grafting different components of the skin became available ( billingham and medawar , 1951 ) , an attempt to evaluate the relative importance of epidermal and dermal changes in the evolution of cancer was undertaken by billingham , orr and woodhouse ( 1951 )  . they transferred the fully treated epidermis alone to an untreated site prepared on the opposite side of the mouse 's thorax . in these conditions this epithelium no longer gave rise to tumours , though the reciprocal transfer of untreated epidermis to a bed cut in the carcinogen - treated site gave a yield of tumours approximately equal to what might have been expected had no operative treatment been undertaken . in view of these findings there appears to be another possible explanation of the phenomenon of co - carcinogenesis , namely , that after short treatment with a carcinogen the dermis is sufficiently altered to permit tumour induction when further epidermal hyperplasia is evoked by croton oil . 
the cutting of these grafts was greatly facilitated by the hyperthe rectangular slices plasia of the epidermis due to the carcinogen treatment . were floated raw side down on 0 5 per cent commercial trypsin solution and incubated at 38c . 
i. - experiment j : each horizontal strip represents the survival of a mouse after the grafting operation ( life line )  . oblique shading represents a papilloma , solid black shading a malignant tumour . 
an oblique line cutting the life line indicates operative removal of a tumour . the rate of appearance of tumours on the original methylcholanthrene - treated area after removal of thin thiersch grafts is indicated by the shading in the life line . 
orr treated site after removal of thin thiersch grafts in 16 out of 37 animals . 10 cases these tumours were removed to prolong the life of the animal . in 7 of these further tumours occurred , but 3 of them later regressed . the time range from operation to the appearance of a first persisting tumour was from 0 to 420 days with a mean time of 48 27 - 6 days . 
the survival of these mice from first croton oil painting ranged from 173 to 330 days ; some are still alive and under observation . these times are not , of course , comparable with those for the experimental animals , where the datum line was placed at the time of grafting . the total incidence of tumours on the grafted site is thus not very different from that induced by croton oil alone . there is a qualitative difference in that one of the tumours on the grafted site became conventionally malignant . 
by comparison , the original treated site yielded tumours in 16 of the same animals , 8 of them clinically and histologically malignant , without co - carcinogenic treatment on that site . the results in general of this experiment do not support the view that the transplanted epidermis contained latent tumour cells . 
the result is not , of course , unequivocal , but the occurrence of a single carcinoma does not suggest that many irreversibly altered cells can have been present . an attempt is in progress to find the effect of preliminary grafting of normal skin , followed by treatment with croton oil , in order to see whether the operative treatment of the dermis modifies the effect of croton oil . it is technically difficult to prepare pure epidermal grafts of normal thoracic epidermis , but experiments are in progress with re - implanted thiersch grafts . experiment k : reimplantation of a pinch graft cut from carcinogen - treated skin . billingham , orr and woodhouse ( 1951 ) made a few observations on the effects of cutting pinch grafts from the carcinogen - treated area , and reimplanting them at the same site . these experiments were undertaken to control the results of transplantation and in particular to make certain that the detachment of the superficial skin was not in itself the reason for the paucity of tumours when it was transplanted . 
the grafts were then replaced and the surrounding gap , caused by retraction of the skin around the wound , was dusted with sterile animal charcoal to mark the graft position . 
2. of 17 grafted mice surviving beyond the time of first tumour appearance , 11 produced tumours , but these regressed on 5 animals so that only 6 mice had tumours present at death . 
the tumours appeared after 8 to 200 days ( mean 42 17 - 3 days ) from the time of grafting the experimental group of animals . eight tumours became malignant after 20 to 100 days . 
the mice survived after grafting for 38 to 230 days ( mean 98 11 days )  . it will be seen that 70 days after the reimplantation more tumours were present on experimental animals that controls , and it seemed that the tumour production was indeed being augmented by the grafting operation as in the previously reported experiment . however , after about 100 days several tumours on the experimental animals regressed - a much less frequent occurrence in control animals . the outcome was that the proportion of animals bearing tumours at their deaths was no greater in the grafted animals than in the controls . 
2. - experiment k : the rate of appearance of tumours in the bridge epithelium over the scar around the reimplanted pinch graft of carcinogen - treated skin is indicated by shading in the life line and persistent tumours by the letter s . 
tumours arising on grafts themselves are shown by shaded blocks above the life line and persistent ones by the letter g . tumours arising outside the grafts are shown by shaded blocks below the life line and persistent ones by the letter o . 
1. experiment l : reimplantation of thin thiersch grafts cut from carcinogen - treated skin . in this experiment thin thiersch grafts were removed from the carcinogentreated area as described in experiment j . 
as great an area of the carcinogentreated skin as possible was taken off and the pieces were then planted back again , in some cases after smearing the graft beds with animal charcoal to mark them . the results are shown in fig . 
the mice survived from 69 to 230 days ( mean 124 + 12 - 5 days )  . tumours appeared on 5 out of 18 control ungrafted mice after 16 , 20 , 23 , 24 all became malignant . 
the mice survived from 38 to 230 days and 200 days . ( mean 99 14 - 2 days )  . experimental animals control animals 4222 4223 4225 4246 4247 4248 4249 i 4250 4488 z 4493 4494 4498 4499 4500 4502 4206 4207 4208 4209 4210 4227 = r_ 4229 4230 4474 4475 4476 4477 4478 4479 4480 4481 4483 4495 z 77 days after thiersch graft operation fig . 
3. - experiment l : the rate of appearance on reimplanted thiersch grafts of carcinogenblocks of shading below the line indicate treated skin is indicated by shading in the lifeline . tumours outside the grafted area . 
some of them , such as age , sex and diet are fairly easy to control . others , such as range of temperature and amount of carcinogen administered , may be less easily controlled . 
orr of animals such as were used in the present experiments . may strike at any time . parasites and infections experiment m : the insertion of cotton threads into the dermis of carcinogen - treated skin and their removal after 2 weeks . orr ( 1934 and 1935 ) showed that preliminary alteratioii of the dermis , by the introduction of linen threads and their subsequent removal before treatment with a carcinogen led to a significantly earlier appearance of tumours . 
we thought it of interest to see what happened if the threads were introduced after the standard preliminary carcinogenic treatment of the present experiments . fine white cotton button - thread was threaded into the finest ordinary sewing needle which would take it and then sterilised . the needle was inserted into the skin of the anaesthetised mouse just outside the carcinogen - treated site . was passed through the dermis of the treated area as near to the surface as possible , endeavouring not to injure the treated epidermis itself , and out through the cotton was carefully pulled through and the surface beyond the treated area . the procedure repeated again under another part of the treated area . the thread was passed under the treated skin in both directions about half a dozen times in all and left in situ for 2 weeks . at the end of this time the projecting loops of cotton were cut and the threads carefully pulled out of the skin under anaesthesia . unfortunately the threaded area had not been covered over and many of the mice had scratched and tugged at the loops of thread , resulting in some damage to the carcinogen - treated epidermis itself '  . the results are shown in fig . 
5. persistent tumours appeared on 10 of 19 experimental animals in 9 to 92 days ( mean 35 7 * 9 days )  . eight tumours later showed malignant changes . 
orr croton oil , the tumour yield is only very slightly greater than that obtained by croton oil on otherwise untreated skin . of the few tumours so produced , all except one were papillomata , which appeared somewhat earlier than might have been expected with croton oil on previously untreated intact skthe single exceptional tumour was a carcinoma , an unusual occurrence with simple croton oil treatment , but it has to be remembered that grafting was delayed up to the time that tumours were already beginning to appear on the original methylcholanthreneexperimental animals control animals 77 , , / , , , , z , , 4358 4361 4369 4370 4372 4373 4374 ' .. 
the results of berenblum and shubik ( 1947 ) were explained on this basis by postulating a two - stage process , the first stage being the alteration by a sudden and irreversible process of a few normal epithelial cells into latent tumour cells , the second the conversion of these latent cells into visible tumours . the first stage ( " initiating process " ) requires a carcinogen ; the second ( " promoting process " ) can be brought about by various non - carcinogenic hyperplasia - inducing factors , of which croton oil is the most fully analysed . it appears to us that the facts elicited by berenblum and shubik are explicable without reference to the conception of latent tumour cells , and that an irreversible change inflicted on the carcinogen - treated site as a whole , and perhaps particularly on the supporting tissues , would explain the olbserved phenomena of co - carcinogenesis . in one respect the view we put forward offers a more satisfying basis for one of the berenblum and shubik findings . 
they showed that even after as long an interval as 20 weeks between the initial painting with carcinogen and the subsequent croton oil treatment , the total tumour incidence remained undiminished as compared with shorter intervals . if , therefore , latent tumour cells were there all the time , it would be necessary to assume that they did not participate in the normal processes of desquamation . it is also relevant to point out that blum ( 1944 ) has analysed the results of carcinogenesis by mathematical methods , and reaches the conclusion that the available data are not consistent with the hypothesis of a discontinuous two - stage process . if the dermal and subcuticular changes are of importance to carcinogenesis , the most obvious way in which they could act would be by interference with the nutrition and metabolism of the overlying epitheliuthe latter does not carry blood vessels , and is dependent on the functional effectiveness of the stromal tissues . it has previously been pointed out that the rate of evolution of the dermal changes ( in simple treatment with a carcinogen ) is of the same order as the potency of the carcinogen in terms of time taken to produce tumours . it may therefore be asked why a single application of a carcinogen followed by a co - carcinogen is effective at all in the induction of tumours . 
a possible explanation is that the hyperplastic epithelium following the co - carcinogen is susceptible to degrees of dermal change and vascular impairment which would not effect normal epithelium or epithelium in a less vigorous state of multiplication . 
orr the reimplantation studies of experiments k and l necessitate some modification of the conclusions drawn from the previous reimplantation of billingham , orr and woodhouse ( 1951 )  . it is now found that this treatment does not appreciably alter the ultimate tumour yield , because the apparent increase in the period immediately following the operation is offset by the regression of several of it was suggested that the previous result might be these " explosive " tumours . accounted for if the operative treatment accelerated the establishment of optimal it remains not impossible that this conditions for the evocation of tumours is so , and that subsequent regression of some of these tumours was dependent on the ischa3mic conditions in the dermis and subcutis developing further to a point at which the vascular conditions were inadequate to maintain the tumour . in experiments of the type recorded here , it is necessary to consider the effects experiments such as those of of mechanical trauma on the yield of tumours . lipschuiitz ( 1924 ) , mandl and stohr ( 1924 ) , doderlein ( 1926 ) and deelman ( 1927 ) indicated that trauma of a previously tarred area tended to provoke tumours closely related to the sites of the healed wounds . 
more recently pullinger ( 1943 ) obtained results similar to those of deelman using a pure chemical carcinogen . mackenzie and rous ( 1941 ) and friedewald and rous ( 1944 ) obtained a high incidence of tumours around healing wounds produced by punching holes in the it was on the basis of this work that ears of rabbits after carcinogen treatment . the conception of initiating and promoting factors , later adopted by berenblum and shubik ( 1947 ) was based . in almost all such work , attention has been almost exclusively directed to the epithelial cells , but linell ( 1947 ) showed that there was a difference between superficial and deep trauma . 
numerous tumours , including carcinomata , appeared on the original treated donor site . re - implantation of pinch grafts and thin thiersch grafts into the site from which they were cut in the carcinogen - treated skin did not result in an increased incidence of persistent tumours . there was an increase in regressing tumours . trauma to the treated dermis ( by temporary insertion of threads or by electrically heated wires ) did not increase the incidence of tumours . the present results , like those previously reported , suggest strongly that both the epidermis and dermis ( and possibly deeper structures ) are involved in the carcinogenic action of methylcholanthrene . in particular , they are difficult to reconcile with the two - stage epithelial hypothesis of berenblum and shubik ( 1947 )  . we are indebted to r . 
salaman. from the cancer research department , london hospital medical college , london , e.l. received for publication march 15 , 1952 . if a chemical carcinogen is applied to the skin of mice at a concentration just too low to produce tumours by itself and , after an interval , a co - carcinogen is repeatedly applied to the same site , tumours . 
weekly applications of 2 * 5 per cent croton oil in paraffin to both groups were begun 6 weeks after an initial treatment with 0 - 15 per cent dmba . 
croton oil treatment of group 5 was stopped after 8 applications , when the average tumour incidence in both groups was about 0 - 5 per mouse . incidence in the two groups increased for a further 2 to 3 weeks , after which incidence in group 4 continued to rise , following the curve usual in this type of experiment , while that in group 5 remained almost constant at about 2 tumours per mouse . after 9 weeks without treatment there had been no appreciable change in tumour number in this group , though the tumours already visible had continued to grow . 
tumour incidence in group 5 had , by then , reached about 11 tumours per mouse ; it continued to rise for a short time , as before , then fell a little , and again remained approximately . 
1. - comparison of the effects of continuous and intermittent weekly applications of croton oil to mouse skin , 6 weeks after a single application of a carcinogen . consequently individual points in fig . 
1 , which represent by others , is high . average numbers of tumours per mouse , have high standard errors , and the differences between corresponding points on the curves of groups , 4 and 5 are barely significant . it is easy to show , however , that the curves as a whole differ their slopes between the 15th and 21st week were compared as significantly . follows : the average increments .of tumour number of individual . 
one must suppose that there is a critical size , rather less than 1 mdiameter ; i.e. , that tumours smaller than this do not continue to grow without further stimulation . did these invisible tumours remain unchanged during the remission of treatment ? apparently not , for when the treatment was resumed there was no immediate outburst of newly - visible tumours . after 58 days the interrupted rise in numbers this latent period is not significantly different from that of the continued . response to the first course of croton oil treatment . 
the skin behaved as it would have done if it had had no previous co - carcinogenic stimulation . it is possible to conclude that the change produced by croton oil in mouse skin previously treated with a carcinogen is not sudden , or independently proit is a gradual change , requring repeated applications for its maingressive . tenance and progress , which is reversible during the greater part of its course , but becomes irreversible not long before tumours become visible . it has been previously noted ( shubik , 1950a , 1950b ; salaman and gwynn , 1951 ) that of the tumours produced in mouse skin by croton oil following a single treatment with a carcinogen most are benign , though some reveal or develop a malignant character later . 
the difference between these two latent periods is not significant . ( 3 ) these results are discussed . it is concluded that the change produced by croton oil in mouse skin previously treated with a carcinogen is a gradual one , requiring repeated treatments for progression towards tumour formation , that it is reversible during the greater part of its course , but becomes irreversible not long before tumours become visible . i am indebted to professor s . 
the carcinogen was then placed in contact with the surface of the epithelium , and ingerted into a bashford transplanting needle , care being taken to shield the carcinogen from the connective tissues of the host animal . in some instances as manv as tbxee subcutaneous primarv grafts were made on each side of the belly of a s ' mgle host mouse to give a series of prostatic tumours growing under identical hormonal conditions . 
the technique is similar in some essentials to that - previously employed bv greene ( 1945 ) , and rous and smith ( 1945 ) , except for the important difference that the present experiments involved tiimour production from adult , not embrvonic tissues . the influence of bilateral orchidectomv upon the growth rates of glandular and squamous cefl prostatic carcinomas was mvestigated in 6 - months - old mice , which had pre ' %iously been castrated before attaining pubertv . 
10 were of the squamous variety , and 2 were spindle - cell sarcomas . sixteen homologous grafts failed to gi - ow , and were foiind at autopsy not to have becoi - ne vasettlarized . in order to detern - iine the early phases of carcinogeiiesis , witliin the primary grafts a further 30 mice received prostati c iniplai - its , and , " , - ere sacrificed at intervals ranging from two weeks to five inonths after iniplantation . 
which are practicallv fused together with an anterior portion and an isthmus or middle lobe which , as in the rodent , surrounds the urethra . unlik - e the hu - man crland , the mouse prostate has no uterus masculinus or its equdvalent , nor is it encapsulated . 
thus in the human gladd there are as many as 32 ducts ( 31axiniow and bloom 1948 ) , whilst in the mouse them are onlv six . a fibromuscular stroma consisting of dense connective tissue is common to both ty - pes of gland . 
the cytoplasm of the glandular epithelium in both species contains numerous secretorv granules , the majority cytologically treated mouse maerial shows the secreticn of which are , of lipids . in both forms to consist ot protein w%ith fine lipoidal droplets in suspension . 
iiornixg to a failure in the release of the secretion , siiice the ducts ai - e iio lojitretpatent , and proliferation which might be due to the direct action of the carciilogeii . neoplastic change - s in graft8 implanted with the carcinogen . the carcinogen , which is placed in direct contact with the living tissuewithout solvent such as oil . 
or lard , induces verv little foreign body reaction , necrosis or residue within the graft which iiiight mask or conceal the actual areas where neoplastic changes fii - st arise . 
h perplastic alveolus froni which it has arisen . through a whole graft of dorsal lobe epitheliuni fixed 41 weeks after implantation . there is very little foreign bodv reaction , and it will be iioted how clearly the foci in which iiialignant changes arst arise may be detected . adjacent to alveoli lined with a , low colunuiar epithelium and distended with secretion colitaining epithelial debris and polyiiiorphs are collapsed alveoli in wliieb the epitheliuni has entered an exhaustion phase . 
the tongue - lik - e colony , of earlv malignant cells , of t3 - pe a was t3 - pical of those tumours which finally developed into secreting glandular carcinomas . l [ n the example ihustratc ; 1 the proliferation arose from a single alveolus and was the only fo - cus of later stages from other grafts showed malignant change in this part - icudar gr - aft . the onset of secretorv activitv . 
14 shows three ii - ialignant alveoh in the peripheral engaged in secretion . area of an invading new grom - th of this type from an eight weeks ' old graft.. several epithelial cefls are in process of abnormal cefl division . 
transplanted into n - lice of the s - ame age and sex as the host mouse , retained their histological charact - c - rs for 16 generations of serial transplants before finallv transforming into a squamous - cehed tumour . the type b lesion arose in the various grafts exaniined from a single alveolus . aild the example illustrated in fig . 
the area of the alveolar wafl malignant cells - , contain small nuclei with nunierous atypical mitotic figuxes . apart from the different morphology and staining reactions of the prohferating cells . 
it will be noted that they tak - e origin from an alveoluss in which secretory adjacent alveoli not shor% - ing these proliferative activitv has been inhibited . changes are distended with secretion . in older grafts the type b prohferation leads to the formation of pseudo - alveoli at the margins of the tumour and . although the glandular architecture of the epithelium is thus partly restored , there is no evidence of secretion . 
the secretory epithelium like that in the mouse gland is thrown into folds which project into the glandular lumina . note alveolar concretions , and compare with that of mouse in fig . 
4. - implant of portion of dorsal epithelium from a normal strong a mouse without carcinogen after surviving subcutaneously in a host male mouse of same age and strain for 12 weeks . note distension of alveoli with prostatic fluid which is far in excess of what is typical of the normal gland in 8itu , and frequently leads to cystic dilatation . 
9. - early hyperplastic changes in prostatic epithelium of a strong a mouse , after eight weeks ' subcutaneous implantation with carcinogen in a host mouse of same sex , age and stra ' the glandular epithelium contains patches which are 10 - 20 cells in depth . 
on palpation the tumours undergoing regression were hard and the two which failed to respond to orchidect.omv were soand sin - iilar nodular t.o those growing in the control mice . 
variable influence of orchidectomv on the behaviour and gro - wth of this alandular carcinoma was further demonsirated in another series of experiments which were repeated at a later date . in this instance two groups of mice , 10 in each , lik - ewise castrated before pubertv . 
received transplants of the same tumour . the gro , %th rate of three tuniours in the first group of io mice was entirelv four tumours in the second group also grew at approxitunaffected bv castration . iiiatelv the same rate as the transplants in the intact control mice . 
four tumours - , responded to this treatment bv showing an immediate increase in growth rate while the , remainder were una#ectedsquanwus - cd , l cwrcinonia.. a glandular cell carcinoma which had undergone spontaneous inetaplasia after its 10th generation of serial transplants in non - castrated normal male mice , was chosen to determine the possible influence of orchidectomv on a glandular tumour which was undergoing squamous transformation . microscopic exan - iination of this particular tuniour had sho - w - n that the metaplastic alveolar epithelium was columnar and much of it still retained secretorv activitv . 
a variable degree of keratinization associated with prickle cell transformation of the epithelium occurred in concentric nests of cells in the peripheral alveoli of the tumour . comparison of the grouth rates of this particular tumour transplanted inw intact control mice . 
the occasional slight inhibition of tumour growth in soiiie orchidectomized mice was within the limits of possible normal variation . the histological changes accompanying vaiiations in grawth and behaviours , in castrated and non - castrated mice . 
17 , were ha ' rder and tnore nodular on palpation than those growing in secretory activity as judged from sectioiis had beeil sitpcontrol intact mice . pressed and squamous metaplasia , of variable intensity in different areas of aiiy tumour , was always found . 
 ' portions of this tumour failed to grow when transplanted into normal ho ; t rnice . tumours inhibited bv castration but subsequentlv treated with testosterone . after which wth was renewed . 
the alveolar character of the growth had persisted , but.the epithelial cells were shorter than in the original untreated tumour . these results were confirmed in a second series of experiments involving the same number of castratm mice using the same dosages of testosterone . 
tumours found to be retarded in growtli during the fifth week of treatment were characterized by a decrease in the size of the majoritv of the alveoli , a reduction in the height of the epitheliuni , a coinplete disappearance of cell - divisioii , and an increase in the fibro - mtiscular stroiiia . 
the alveoli diminished in size when this rupture occurred , whereas adjacent alveoli with intact epithelial cells appeared to be so slightly affected by the oestrogen that little more than a reduction in the lieight of the cells could be obsei - ved . 
a detailed study of the hyperplastic ' changes in numerous grafts has shown concltisively that in no single instance has an actively secreting epithelium been the focus of malignant change . 
the technique used in the present without at the same time da experiments is pomibly supenor to that involving injection of carcinogens , dissolved in such solvents as lard , merely because it entails less damage and concentrates the carcinogen at the proper site . since the present technique also involves homologous grafting , however , the reaction between host and graft tissues may play some part in the successful induction of a tumour . in mice the survival of a homologous graft seems to depend on the use of a closely inbred stock mice of incleterminate ancestry will not often tolerate grafts for strain . periods sufficient for the establishment of tumours . recent experiments have indicated fwrthermore that the age of the mice providing the graft tissue , and the age of the host mice into which the grafts are implanted , have an important bearing on the problethus the survival rate of grafts of lung or prostatic epithelium without carcinogen was greater if host mice under eight weeks old were used , and was considerably reduced if the mice were over eight months this was invariably the case if the mice were of mixed or pure line origin , old . but only 12 per cent of the grafts in young mi ed stock mice survived as against in older mixed stock mice of 8 months 85 per cent in the young pure line mice . to one year no graft survivecl after three months ' implantation , whilst in inbred mice of a similar age 25 per cent of grafts survived after the same period . 
combining the carcinogen 20 - methylcholanthrene with grafts of lu or p - rostatic epithelium in 25 eight - weeks - old mice of mixed stock gave only one tumour , a spindle - miled sarcoma , twelve weeks after grafting ; the remaining 24 host mice failed to produce tumours , and at autopsy the grafts were found not to have price ( 1941 ) , using rats of different ages from an albino become vascularizedl strain which was not strictly pure hne , found that ventral lobe prostatic tissue grafted subcutaneousl in the abdominal wall beha - ved in much the same way , prostatic tissues from old rats being very limited in their capacity to survive as homologous grafts . 
many apparently viable grafts from old rats were found to be degenerate on histological examination , but when regrafted into younger hosu the implants underwent a rapid recovery and the pmstatic epithehum even regained its secretory activity . 
one of the most intere8ting features in successful grafting of prostatic epithehum is its ability to continue secreting while growing under the influence of foreign host reactiom and changed vascularity . 
ob - viously androgenic stimulation , as price ( 1941 ) maintains , must be important in this phenomenon . the dependence of prostatic epitheli - um upoii androgen smretion has long been realized and the experimental evidence need not be referred to here , except to mention that in recent years the elegant technique of transplantation of fmgments of prostate into the anterior chamber of the eye ba - s provided additional confirmation . and rosenblum ( 1937 ) , moore , rownblum , tolin and melchionrka ( 1937 ) , and moore and smith ( 1937 ) , grafted rabbit prostatic epithelium in this way and photographed the implants dailv . 
they were able to record fluctuations in size of the grafts which were abohshed by castration , and considerably increased by administration of testosterone propionate . heckel and kretwhmer ( 1935 ) made similar observations of the responses of prostatic grafts to anterior pituitary extracts . 
horning mice or rats will maintain the size and normal histological appearances of the hill and strong ( 1938 ) attribute the androgpnic prostate and seniinal vesicles . effect of the ovary to the lowered temperature of the ear , and deanesly ( 1938 ) has correlated this activit ' with extensive luteinization of the theca intema within the ovarian grafts . another potential source of androgens to be considered in relation to prostatic grafts and tumours is , of course , the adrenal cortex . 
the rare adrenal insufficiency in young children associated with adxenal hypertrophy leads to enlargement of the prostate and differentiation of its glandular tissues to a degree comparable with the adult gland ( dijkhuizen and behr , 1939 - 40 )  . prostatic enlargement also occurs in adults with adxenal cortical tumours . miller ( 1947 ) has found a relative increase in dehydroisoandxosterone , and a decrease in androsterone in the urine of patients with benign hypertrophy of the prostate . according to callow and callow ( 1940 ) the source of dehydroisoandxosterone is probably in the adxenal cortex . it remains in the urine after castration , but disappears in cases where there is destruction of the adrenal cortex . while it niight be assumed that grafts of prostate or transplantable prostatic tumours would have poor chances of survival in female hosts , under certain conditions they do in fact survive and this must be attributed to the influence of androgens produced either in the ovary or in the adxenal cortex . price ( i 941 ) grafted normal prostate into female host rats , and found that in some cases the grafts were similar in histological structure to the prostates of castrate males , whereas other - grafts flourished and underwent secretory activity . this result she maintained could be due to the development of androgenic foci in the ovaries of some , but not all , host animals . 
the grafts failed to differentiate in spayed rats , whereas they survived in a functional condition for prolonged periods if the hosts were over 80 days old . either virgin females or rats which had littered frequently would sustain functional grafts , provided they were not youngei than this apparently critical age . the opinion is often expressed that the prostate gland in rodents is not strictly homologous with the prostate in the human , and thus there can be rttle justification for comparing growth behaviour and endocrine responses in experimentally induced prostatic tumours or hyperplasias with the spontaneously occurr , ingconditionsinthehumangland . greenstein ( i - 947 ) maintainsforinstance , that because certain rodeint prostate tumours grow when transplanted into female mice , whereas human tumours are so sensitive to inhibition by oestrogens , the two types of neoplasm are not fundamentally the same . 
apart from the single case reported by deniing , jenkins and van wagenen ( i935 ) of a spontaneous nodular hyperplasia in the suburethral tissue of an albino rat , there is no record of spontaneous prostatic hyperplasia or cancer in rodents . if it can be shown , however , that the prostate tumou - ts induced by methylcholanthrene behave in essentially the same way to hormone administration or deprivation , the differences between rodent and human neoplasms will be less significant . the glandular carcinomas described in these experiments , when transplanted into rnice ca 'strated before puberty , show complete inhibition of secretion , later followed by squamous differentiation . 
subsequent traimplantation into castrated hosu is not followed by any appreciable inbibition . some glandular celled carcinomas am thus dependent for their sustained growth on an adequate androgen level ; the squamous growths would appear to flourish without testicular androgens and , if they are at all androgen - dependent , it must be concluded that adrenal cortical androgens are in these cases suflicient . and hodges ( 1941 ) buman prostatic cancer falls into two according to it is possible that groups , androgen dependent - and androgen independent . squamous - celled carcinomas in mice belong to the second category , although aours rarely occur in man ( willis , 1948 )  . such t a smah percentage of glandular mouse tumours failed to regress when transplanted into castrated hosts ; they even grew at approxim tely the saine rate m those transplanted into uncaamted mice . 
howard ( 1937 , 1938 ) has demonstrated that removal of the gonads in rats , provided these are sufficiently yoijn , increases the capacity of the adrenals to secrete androgens . 
as ar the mice in the present experiments were castrated before puberty , and an interval of several months elapsed before they received t aour transplants , it seems probable that androgenic foci had developed in the adrenals of those castrated mice in which unfortunately.biochemical assay the tumours showed no inbibition of growth . of androgens secreted from non - testicular sources cannot be undertaken in the mouse to confirm or refute these conjectures . on the chnical side the serum acid phosphatase and urinary 17 - ketosteroid levels can be used respectively as indicators of the activity of mahgnant prostate cells and of androgen smretion . 
thus mn4vs stevens and hodges ( 1941 ) studied cases in which a recurrence of prodatic cancer had fobowed an initial improvement in the condition obtained - by bilateral orchidectomy . there was a rapid reduction in the serum acid phosphatase , and a simil ri marked fall in the urinary 17 - ketosteroids after orchiclectomy . 
the development of androgenic foci in the adrenals was regarded by and swtt ( i945 ) as responsible for the recurrence of the disease . recently , following failure in four - selected cases to control growths by orchidectomy , these worken tried bilateral adrenalectomy ancl , although three of the patients died within a comparatively short fume after operation , the fourth survived for 116 clays . 
cox ( 1947 ) tried unilateral adrenalectomy on three patients with prostatic cancer , all of whom had temporarily responded to treatment with there was an immedi te drop in the 17 - ketosteroid level and a oestrogens . r tumours transplanted into normal male mice showed a varying retardation of growth after oeamgen treatment , but in no single instance did any undergo complete regression , as was the case following orchidectomy . 
horning inhibition of tumour growth with such relatively high doses was the result of non - specific toxic action . it was also found that the amount of stilboestrol tolerated depended upon the genetic constitution of the rnice . 
although in the present experiments the dose of stilboestrol was approximately half of that used by ludford and dmochowski ( 1947 ) , the average loss of weight of the tumourbearing rnice was approximately i ' to 2 g . 
during the total period of treatment . histological examination of regressing glandular tumours after stilboestrol gested that diminution in size of the tumours was primarily due to thera inhibition of secretion , later followed b ' degeneration and collapse of alveoli . schenken , burns and kahle ( 1942 ) and fergusson ( 1946 ) have exandned serial biopsies of human prostatic carcinoma under oestrogen treatment . 
the former authors described in detail such cytological changes as vacuolation of the alveolar epithelium , disintegration of the cell membranes , sometimes accompanied by stratification of the epithelium , and an increase in the stroma . these changes are very similar to those which occur in the glandular mouse tumours during oestrogen treatment . 
the squamous metaplassia , which some of the glandular mouse tumours undergo in response to oestrogen administration , is rarely found in the human gland after sirnilar treatment . recently , however , inglis ( 1948 ) described a pronounced squamous differentiation in a man treated with stilboestrol for prostatic cancer . it is tempting to regard the atrophy of prostatic tumours in the mouse as due to failure of optimum androgen secretion in the castrated hosts , or to a similar drop in gonadotrophin production when intact tumour - bearing mice are treated those tumours whieh fail to regress are possibly receiving with oestrogens . sufficient androgenic stimulation from the adrenal cortex . inhibition of secretion and degeneration of the epithelium in these tumours are so similar to the changes induced in the normal prostate following castration or oestrogen administration that any more complicated mechanism operating in the case of the tumourbearing mice seems unnecessary . 
it bas been possible in grafts , impregnated with the carcinogen , as soon as four to eight weeks following implantation , , to distinguish between three distinct types of early malignaint lesions . detailed swdy of the hyperplastic changes in prostatic alveoh in numerous grafts showed that in no single idstance has the actively secreting epithelium been the focus of mahgnant change . it tberefore appears that the non - secreting exhausted alveolar cells m the prostatic gland are more susceptible to the action of the carcinogen than those at the height of secretory activity . this supports the contention that chemical carcinogens act - more readily on cells following depression of cellular activity . the influence of sex hormones and orchidectomy was determined on the behaviour and growth of glandular and squamous - cell carcinomas of the prosute . a greater number of glandular carcinomas regress when transplanted into male mice cm - trated before puberty , and a small percentage of - the - e tumours resume growth when treated with testosterone propionate . 
tumours which at the time of their induction were diagnosed as squamous growths , or glandular carcinomas which had undergone spontaneous squamous differentiation during serial transplantation , exhibited no appreciable response to these fornvs of therapy . these results indicate that only glandular and not squamous carcinomas are dependent for their sustained growth on an adequate androgen level . glandular carcinomas when treated with dieth - vlstflboeaml respond more re - adily than squamous t aours . 
and bave given additional information on the factors responsible for tumour regremon . particular attention hm been paid to those glandular tumours which failed to respond to either orchidectomy or hormonal theraphy , and the possible endocrine factors inducing resmtance to treatment are discussed in the hght of recent experimental and clinical evidence . this investigation has been supported by grants to the royal cancer hospital , fi - om the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the u.s. 
on the other hand the quantity necessary to induce abdominal fibroids is not much above the mentioned hysterotrophic dose ; abdominal fibroids can be induced by three injections per week of 5 lg . 
of oc - oestradiol , or even less , when administered as the 17 - caprylic ester of a - oestradiol , which is absorbed so slowly that a continuous oestrogenic action is made possible ( lipschutz , bellolio , chaume and vargas , 1941 )  . similarly a few micrograms of free oc - oestradiol or oestrone absorbed from a subcutaneously implanted tablet also are sufficient to induce fibroids ( lipschutz , thibaut and vargas , 1942 )  . 
on the contrary , quantities about a hundred times greater are necessary to elicit the same tumorigenic abdominal reaction if administered by subcutaneous injections of the free hormone ( lipschutz et al . , 1939 , 1942 )  . in the present work we shall deal with abdominal fibroids induced by extremely small quantities of estrogens and with the neoplastic action of these quantities on the uterine glands in experiments of long duration . fibromatogenic action of very small quantities of x - oestradiol and of oestradioldipropionate . tablets weighed 33 to 35 mg . 
each. tablets consisting of one part of the oestrogen and 19 parts of cholesterol merck were prepared in the usual way by mixing , dissolving in ether , drying and after drying in vacuo they mixing again . were implanted beneath the skin into castrated female guinea - pigs weighing 380 to 480 g . uterine and other abdominal fibroids were elicited under these experimental conditions ( riesco , 1942 ) , though the incidence was less than with the injection of great quantities of oestradiol administered as the benzoic ester , as in the experiments of iglesias ( 1938 )  . necropsy was made 112 to 118 days later . during necropsy , cleaned and dried subsequently . absorption was calculated from the loss of weight of the tablets recovered calculation was made under * this work has been aided by a grant from the jane coffin childs memorial fund for medical research , grant administered by a . 
the result of these experiments is given in table i . as seen from table i , tablets containing originally 5 per cent of the free cx - oestradiol and remaining for about 4 months in the body of a guinea - pig produce anew oestrogenic and fibromatogenic actions when reimplanted into another guinea - pig . the same result was observed when 4 months afterwards the tablet was implanted for a third time and a fourth time . there was in all these experiments opening of the vagina , growth of the nipples and uterine bleeding . 
should there have been selective absorption , oestrogenic hysterotrophic and fibromatogenic actions or uterine bleeding would have been impossible , in any case , in the third and fourth implantation . 
were obtained for the first 4 months . it is remarkable that in successive implantation smaller figures were obtained . allowance must be made for entering of substances into the tablet as has been shown by different authors ( bishop and folley , 1944 ; deanesly and parkes , 1943 )  . absorption was most probably greater than indicated by figures in our table i . 
but it can easily be demonstrated that daily absorption of oestradiol was certainly less than about 3 to 4 , g . in these experiments the total quantity of oestradiol in the tablet was never more than 1750 , g . , and the tablet remained beneath the skin during 470 days without exhaustion of the oestrogen . 
but in the next paragraph we shall mention experiments in which similar tablets were active for a total of 675 days without the oestrogen being exhausted . histological examination of the uterus in the mentioned animals revealed pronounced cystic glandular hyperplasia of the endometrium , polypous proliferation of the latter , thickening of the vaginal wall and proliferation of mammary these statements coincide with what has been formerly observed with tissue . the prolonged action of estrogens in this department . neoplastic action of small quantities of oestrogens on the uterine glands in experiments of long duration . in the above - mentioned preliminary experiments evidence was given that by continuous absorption of very small quantities of oestrogen , certainly less than 3 to 4 ug . 
fibromatogenic action was rather less pronounced than with the free hormones . but with the fibromatogenic action of oestrogens due allowance has to be made for variation . in the second series in which tablets already used in the first one were again implanted and left in the body for no less than one and a half years , uterine growth was considerable . uterine fibroids were also induced . microscopical examination of the uterus revealed in the series of long duration a condition fundamentally different from that seen at four months ; there was besides cystic glandular hyperplasia of the endometrium also proliferation of glands infiltrating the myometrium , reaching the serosa and even perforating it . the lumen of the proliferating and infiltrating glands was sometimes cystic , sometimes small or absent . 
the neoplastic and infiltrative growth of the glands was , in lipschutz ' experiments with ovarian fragmentation , coincident with those we have described in the last paragraph , with the exception that with ovarian fragmentation the invading glands did not reach the serosa and did not perforate it , as was the case in one of our animals . 
a guinea - pig having been injected for 8 months with oestradiol benzoate was found , 4 months later , to have a " precancerous " transformation of the endometrium in the upper third of the uterine horn . this latter observation of lipschutz and others is so far the only one which may be quoted in favour of irreversible atypical proliferation of the uteririe mucosa elicited in the guinea - pig by oestrogens and persisting after the withdrawal of the hormone . neoplastic malignant growth seems to be more easily elicited in the cervix of the uterus in the mouse , as shown by the work of gardner and others ( gardner , allen , smith and strong , 1938 ) and allen and gardner ( 1941 )  . in the work of these authors the oestrogens - - the benzoic ester of oestrone and oestradiol were given by injection . 
the quantities injected were , when calculated per gram of body weight in the work of the american authors with mice , probably 20 times greater than in our work with guinea - pigs . another interesting aspect of our work may be mentioned here . 
minutes. this degree ' of hydrolysis was found to remove ar non - dna phosphorus as wer as all non - dna adenine from the cells , while leaving dna phosphorus and dna adenine in situ , thus obviating the necessity for the use of the einzyme ribonuclease ( lajtha , 1954b )  . adenine 14c administered to cells appears both as labelled adenine and labelled guanine in the dna ( hamilton , 1953 )  . no attempts to separate labelled adenine from labehed guanine have been made in the experiments ; the activity of the dna has been measured as a whole . the autoradiographs were exposed for 10 - 14 days . 
ar autoradiographs belonging to the same experiment were coated with the same batch of stripping film , exposed the same length of time at the same temperature ( 3 - 4 ' c . ) , and developed in one batch of developer simultaneously , and , finally , were stained simul368 l . 
on each slide 100 - 200 nuclei were counted , and grains were counted over - 5 - 10 showing the strongest autoradiographs . this was to obtain the values for the maximum degree of dna synthesis and was done after surveying repeated counts at different times were performed to tes - t the over 500 nuclei . reprodiicibihty of the counts , and it was found that with the above technique the same observer showed ain error not greater than 10 - 15 per cent . for the calculations on the quantity of isotope i ' ricorporated into the cell , it was assumed ( 1 ) that the geometry of the autoradiographs was such that only 50 per cent of the electrons emitted frothe disintegrations reached the photograpbic emulsion , and ( 2 ) that the 32p electrons produced 0 - 7 grains per incident electron , and the 14c electrons 2 gfai - ns per incident electron ( lamerton , 1950 )  . if the exposure tiine and the half life of the isotope in question as well as the grain count per nueleus and the grain yield per electron of the isotope are known , then the number of the atoms of the isotope withiii the nucleus can be calculated . the technique is sensitive enough to detect 20 - 30 32p atoms per cen . because of the very long half - hfe of 14c ( and because exposure times were limited to the relatively short period of 14 - 30 days ) the minimum necessary number of 14c atoms per nucleus to show an autoradiograph is of the order of 106 . in preliminary experiments the maximum dna 32p uptake per nucleus was found to be the order of 600 atoms ( > i 00 grains in 14 days ' exposure 07 grains / electron )  . 
the labelling obtained in vitro of the dna is therefore of the order of i : 3 x 107 . if the cehs cannot differentiate between 31p and 32p then the total phosphorus pool available for the cens must also have been labered in the ratio of the order of i : 3 x 107 . thus for 5 , ac . 
in seruthe addition of adeniine 14c into the culture medium does not represent the labelling of a pool , but the provision of adenine to the cers which would otherwise have to synthesise it . 
the marked ability of the cellsto take up adenine from the cultur - e medium is shown by the fact that the average maximum uptake per nucleus was of the order of 1 - 2 x 107 atoms dna 14c ( 50 grains in 10 , days ' expostire , 2 grains / electron )  . 
i ' he cell cycle . if the cells svnthesised dna throughout the entire intermitotic period , then , after a few hours of culture in the presence of the isotope all the cers should contain labelled dna . 
ellis fore the cells within a hours of the end of the period of dna synthesis at the start of the culture in isotope wif not be labered , and , similarly , cers enterina the period of dna synthesis during the culture time ( t ) and spending less than a hours 11111hours fig . 
the length of the s period is also indicat - ed by the gradual increase of the grain count / nuclei up to about 15 hours , then reaching the maximum average value for a given concentration of the isotope in the culture mediuthe length of the total cen cycle can also be calculated in a different way . 
3 illustrates the timing this timing , in of the cell cycle obtained with the methods outhned above . principle agrees well with that found in the bean root by howard and pelc ( 1951 )  . it can be seen from tables i and ii and fig . 
the reason for this difference is , firstly the differences betweein eilergy of the beta particles emitted by 14c and the higher energy32p electrons result in a greater scatter and , consequently , in a higher background , thus interfering with the accuracy of the c ' secondly , while the half hfe of 14c is a neghgible problem when the isotope dilutions are added to the culture medium , variations in volume to allow for the decay are a also , diie to the decay of 32p and to the fact that32p is so - lirce of error with32p  . supplied in3lpphosphate buffer , the ratioof 31 to 32pwill not be constant : the degree of labelling of the phosphorus pool will be variable . these factors all contribute to the lesser accuracy of the counts in cultures with 32plabelling as compared with the 14c labelling . 25 - 30hours 12 - 15 hours 3 - 4hours g2 m fig . 
rate , of dna synthe , 8i8 in different type8 of bone marrow cei18 . in these experiments only those types of cells were found to synthesise dna which are known to be capable of mitosis . 
3 represents the average values for the majority of the dividing cells of the bone marrow , i.e. , promyelocytes , myelocytes , pronormoblasts , basophihc normoblasts and early polychromatic normoblasts . in a few experiments , however , where it was found to be possible to count early normoblasts and early myeloid cells separately , a shorter cycle than in fig . 
the affect of x - ray irradiation on dna synthesis large doses of x - rays ( 5000 r in 15 minutes , 140 kv , i . / mal filter ) exerted a marked inhibition on dna synthesis . 
14. - post - irradiation dna synthesis . was not a recovery in the sense of ability to synthesise normal amounts of dna , but the entry of some 0 , cers into the s period for a hmited time . it appears that ar 01 cehs are damaged by a dose of 5000 r . the effect of irradiation on theg2 period is indicated by the fa ' ct that no mitoses were observed in any of the irradiated cultures . a dose of 5000 r produced a marked degeneration of the cers in the cultures , but over 6 hour culture times were needed to show the first morphological signs 378 l . 
in a sense this could be better defined , as the assembly of the dna experiments with the synthesis , of the purines and pyrimidines from molecule . labeued one carbon compound precursors ( e.g. , formate 14c ) are in progress . the timing of the cer cycle is , in principle , in good agreement with that it is expected that described in the bean root cell by howard and pelc ( 1951 )  . the timing of the cer cycle in different . 
the total cycle time was found to be of the order of 40 - 48 hours for the average dividing bone marrow cers ( promyelocytes , myelocytes , pronormoblasts , basophihc and polychromatic normoblasts )  . 
a phenomenon , involving the abnormal growth of two kinds of pigmented cers , was recently found in spontaneous tumours experimentary produced by genetic methods in platyfish - swordtail hybrids . the tumorous hybrids were produced by mating a male spot - sided and rub throated platyfish ( platypoecilw maculatus ) to an albino swordtail ( xiphophoru& hellerii )  . 
the ruby - throated pattern is composed of xantho - erythrophores , which are red pig ' ment cers containing erythropterin in granular form and lutein gordon ( 1950 ) and gordon and nigrelli ( 1950 ) and zeaxanthin in solution . indicated that these colour patterns are inherited and referable to two platyfish sex - linked genes : sp for the black and bt for the red pigment cers . 
the genetic analysis revealed that the pigmented tumours were produced in platyfish - swordtail hybrids containing the hnked genes , sp and bt from the platyfish and a number of sp and bt gene modifiers from the swordtail . some of these pigmented tum ' ours were diagnosed as erythromelanomas in an earher report by gordon ( 1950 ) and nigrelh , jakowska and gordon ( 1950 )  . more extensive study of additional specimens revealed that there were two kinds of pigmented tumours involved , first , a red tumour , a xantho - erythrophoroma of the head and , second , a black tumour , a melanoma of the body . in some of the hybrids , cers of the melanoma reached , penetrated and replaced the tissues of the red pigmented tumour . 
only a few macrophages , however , are evident in these tumours . the relatively few dendritic and rounded cells are similar to those described in the simple xantho - erythrophoroma . 
the various stages in the development of the melanoma within the xantho - erythrophoroma can be demonstrated and traced in one of these fishes ( 243 - 11 )  . 
33. - melanotic area of the tumour ( 243 - 1 1 )  . 1 - n this region one or two cells from the original xantho - erythrophoroma can still be distinguished . in other areas , however , a , region just below the epidermis - note the melanotic they are completely absent . cell ( melanoblast ) in metaphase ; b , typical melanotic cell of this region associated with a cell of the xantho - erythrophoroma ; c . 
the melanotic cells ( melanoblast 's ) are smaller and less dendritic than the typical macromelanophores ; they are usuany rounded , sometimes fusiform , varying from 10 to 40 tl at their widest dimensions . 
the present studies , however , show that two distinct tumours are involved : a xantho - erythrophoroma in the head region and a melanoma of the trunk and caudal peduncle . in some of the hybrids the more actively proliferating cers of the melanoma invade and replace the red pigmented tumours of the head , producing an erythromelanoma . the red and yerow pigment cell characteristic of the xantho - erythrophoroma was first described by kosswig ( 1928 ) from normal fish as an erythro - xanthophore . according to goodrich , hill and arrick ( 1941 ) , the cell ; which they caued a xantho - erythrophore , is a xanthophore in which erythropterin is laid down in addition to lutein and zeaxanthin . in fixed and stained tumorous material the xantho - erythrophores are either non - pigmented dendritic , rounded or fusiform cers . in both normal and tumorous tissues the nuclei of these cers ' are weak in chromatin ; nevertheless , mitotic figures are frequently found . 
the degeneration of the xantho - erythrophoroma probably results from the growth - pressure of the apparently more actively reproducing melanotic cers which infiltrate and penetrate the interstices between the xantho - erythrophores . 
whether or not the metastasizing tissue would have comalthough complete pletely replaced the invaded tumour was not determined . replacement of a xantho - erythrophoroma by melanoma has never been observed in our fishes , the evidence seems to indicate that this would have occurred had the specimens lived longer . an interpretation of the nature of the genic action that modifies pigment cell growth and the physiological effects of the interaction of such genes in platyfish - swordtail hybrids was outhned by gordon ( 1948 , 1950 )  . 
the effect of the various genes for pigment cells upon the development of the red , the black and the red - black pigment cell tumours may now be suggested . in the normal platyfish gordon ( 1928 ) showed that the dominant , sex - finked , spot - sided gene , sp , manifests itself in the development of large black pigment cells or macromelanophores ; the large melanophores first appear in postembryonic platyfish in the posterior region of the body , specifically , in the caudal peduncle . 
the number of macro melanophores produced by the sp gene in the normal , spotted platyfish is influenced strongly by the action of the stippled gene , st , a dominant , autosomal factor for the - presence of many micromelanophores . 
when sp is associated with the dominant gene st ( that is , sp st ) , more macromelanophores develop than when the sp gene is associated with the recessive gene st ( that is sp st )  . furthermore , in both the sp 8t post - embryonic and adult platyfish the macromelanophores are restricted for the most part to the caudal peduncle . 
315. - - below , a platyfish - swordtail hybrid of the genetic constitiition rts , 206 - 15 , showing the early stage of the development of the xantho - erythrophoroma . this shows up as a red patch on the left operculum surrounding the lower half of the eye . 
241 , produced by mating a platyfish - swordtail rtsp hybrid , 206 - 12 , exhibiting an erythromelanoma , back to an albino swordtail , 1822 - 6 ; upper left , an albino with an amelanotic melanoma at the tip of a caudal fin ; lower left , a sibling showing the " ghost " pattern of macromelanophores ; right , typical melanotic hybrid showing the ear ' lv sta - ae of melanosis in the posterior region of the body . 
the minimu ' m requirement for the production of the erythromelanoma in platyfish - swordtail hybrids is the presence of the linked genes rtsp . gordon ( 1950 ) showed that a platyfish parent of the genetic constitution of rtsbidrsp would not , while a rtspidrsb would produce some hybrids with erythromelanomas when mated with an albino swordtail . 
in the tumorous animals the xantho - erythrophoroma develops rapidly in the head region , and at the same time a condition of melanosis develops in the posterior region of the body . in some individuals the melanotic cens show great reproductive activity and produce a melanoma . 
in those animals that develop a melanoma the cells of the melanoma may invade the xantho - erythrophoroma and destroy and replace the cells of the red pigmented tumour . in other cases the melanin - bearing cers are restricted to the posterior part of the body , aflowing the red tumours to develop on the head without the involvement of the black pigment cers . 
the sequence of events in the invasion of one kind of neoplastic tissue by another type is discussed from the points of view of histology and developmental genetics . this work has been aided by a grant to the new york zoological society from the national cancer institute , national institutes of health , united states public health service in support of the project : " genetic and correlated studies of normal and atypical pigment cer growth . " some details in this paper were presented by myron gordon before a meeting , of the royal academy of medicine , london , july 4 , 1950 . we are deeply indebted to ' the american museum of natural history for .laboratory facilities , to j . 
this process is one of the most fundamental of cell mechanisms , so fundamental indeed that , except in minor details , it has never been influenced by evolutionary change . 
obviously the physiology of such a process is particularly fascinating , and in addition it is becoming clear that its study may shed important light on a variety of practical problems . 
 however , the greater part of this work has been from the viewpoint of pathology , and has resulted on the one hand in the mass of observations on the effects of carcinogenic substances , and on the other with the discovery of the so - called mitotic poisons ( loveless and revell , 1949 )  . 
by comparison , the direct study of the physiology of normal mitosis has been surprisingly neglected , presumably because of the difficulty of the techniques involved , and becaube the practical value of such knowledge has not been fully appreciated . 
 the present discussion starts with a consideration of the physiology of normal mitosis in mammalian tissues , and continues with an examination of its relation to modern work on carcinogenesis . 
 in recent years a considerable amount of attention has been paid to the problem of mitotic activity in the epidermis of the mouse ( bullough , 1948a , 1948b , 1949a , 1949b , 1949c , 1949d , 1950a , 1950b , 1950c ) and of the general biology of the skin ( medawar , 1947 , 1948 , 1949 )  . 
the work on the mouse epidermis began with an analysis of the diurnal cycle of mitotic activity , which was found to be a simple rhythm directly determined by the waking and sleeping habits of the animals . 
factors determining the form of the diurnal cycle are the accustomed times of feeding , the quantity and quality of the food given , and the age and sex of the animals . 
it was found that by means of subcutaneous injections of glucose or starch the mitosis rate can be raised in both active and sleeping mice to a level considerably higher than normal . 
 further studies have indicated that the epidermal mitosis rate is related , not to the blood - sugar concentration , which is high during hours of activity and low during hours of sleep , but to the concentration of intracellular glycogen . 
 bullough and eisa ( 1950 ) have shown that the diurnal cycle of glycogen concen tration in the skin is exactly similar to the diurnal cycle of epidermal mitotic activity . 
it is well known that glucose is deposited from the blood during sleep , and , while most of it is stored as glycogen in the liver , it is now evident that significant quantities are also deposited elsewhere . 
the most obvious alternatives were either that carbohydrate is incorporated , for instance as ribose , in the new nucleo plasm or cytoplasm as it is formed , or that it is destroyed to provide energy . 
the second was strengthened when it was found that the stimulus obtained from extra starch can be augmented by coincident injections of phosphate , and that , conversely , mitosis can be almost eliminated by injections of phloridzin , a substance known to inhibit phosphorylation ( bullough , 1949b )  . 
the conclusion that mitotic activity may involve the expenditure of a significant amount of energy also receives support from the results of experiments made with dividing eggs by such men as brachet ( 1932 ) , runnstr5m ( 1933 ) , and zeuthen ( 1946 , 1947 , 1948 )  . 
 in mammalian epidermis the importance of oxygen has been stressed by medawar ( 1947 ) in the rabbit , and by bullough and johnson ( bullough , 1950c ) in the mouse . 
when this tissue is kept in vitro anaerobic conditions inhibit cell division , and it is now clear that glycogen , phosphate and oxygen are all involved at the onset of an epidermal mitosis . 
however , since in a normal body it seems unlikely that either phosphate or oxygen are ever in such short supply as to become limiting factors in cell division , further elaboration of this point is not necessary here . 
 summarizing what has been said above it is evident that , in a normal mouse , carbohydrate in the form of glycogen or glucose is a most important substance determining mitotic activity , and that its apparent function is to supply the energy requirements of cell division . 
as one outcome of these conclusions it was to be expected that diet would be found to have an important effect on the mitosis rate , and this has now been confirmed ( bullough , 1949c )  . 
 it was later confirmed that a restricted diet results in a lowered body weight , a reduced glycogen reserve , and hence a reduced mitosis rate ( bullough and eisa , 1950 )  . 
however , while the body weights and carbohydrate reserves were found to vary in direct proportion to the degree of underfeeding , the rate of epidermal mitosis varied in a complex manner expressible in terms c , f a sigmoid graph . 
 it must be added that while the results primarily concerned the epidermis , other observations showed that similar conditions develop in other tissues , and it can b6 safely concluded that the reduction of mitotic activity by diet is a general effect visible throughout the body . 
 the striking thing about these observations is that they parallel so closely the results of recent work by tannenbaum ( 1940a , 1940b , 1942a , 1942b , 1944a , 19441 > , 1945 , 1947 ) and tannenbaum and silverstone ( 1949a , 1949b ) , who have in introducing this studied the effects of restricted diets on carcinogenesis . 
 subject it is vitally important to emphasize that it is indeed the genesis of tumours that is being considered , and not the growth of tumours once they have been formed . 
the growth of a visible tumour is only influenced in slight degree by variations in diet , and it is only in the process of tumour genesis that diet has any pronounced effect . 
the greater part of the earlier evidence was reviewed by hoffman ( 1937 ) , who came to the conclusion that " ovemutrition is common in the case of cancer patients to a remarkable and exceptional degree . " this statement can be justified by figures such as those of dublin ( 1929 ) , who showed statistically that persons who are overweight during middle age have a higher expectation of death from cancer than those who remain underweight . 
his first experiments involved a simple restriction of diet , and led to the surprising discovery that animals maintained on a 66 per cent diet are more active , develop fewer tumours and fewer diseases , and so live longer on the average than do the fully fed controls . 
 in later experiments all groups were provided with a basic diet of protein , fat , vitamins , and minerals , and the only differences lay in the amount of carbohydrate which they received . 
of male dba mice painted 19 times with 3 : 4 - benzpyrene , one group of 50 fed ad libitum developed 32 tumours , while another group of 50 fed on a carbohydrate restricted diet developed only 11 . 
as a general principle it can be said that the most striking results are obtained with spontaneous tumours , which are often prevented altogether , and it is evident that with induced tumours the modifying effect of the diet can be at least partly masked if sufficiently heavy doses of carcinogens are given . 
 in both cases this relation is expressible by means of a sigmoid curve , and the great.est fall in both the mitosis rate and the tumour yield accompanies a reduction of from 80 per cent to io per cent of the full diet . 
thus with an average daily intake of about 14 calories the latent period in one experiment had an average length of about 18 weeks , while with an intake of 8 c9.lories the latent period was 39 weeks . 
are that carbohydrate , or calorie , shortage causes reduced body weight , a strongly depressed mitosis rate , the restriction or prevention of a wide variety of spon taneous and induced tumours , a considerable delay in the time of appearance of those few tumours which do develop , fewer dise.ases of all kinds , and consequently a healthier and a longer life . 
tannenbaum ( 1947 ) himself has no explanation to offer , but he has rightly emphasized one crucial point that , like the depression of mitotic activity , the prevention of tumour genesis by calorie restriction is the result of a general effect operating throughout the whole body . 
 at this point it is evident that a prima jooie case can be bmlt up to indicate a connexion between the three factors carbohydrate lack , mitosis depression , and reduced tumour incidence . 
further , it appears possible that these factors may be related to each other in this sequence , carbohydrate lack limiting mitotic activity , and low mitotic activity limiting carcinogenesis . 
however , before attempting this analysis it is important to consider at what possible point in the sequence of events leading to the formation of a tumour the mitosis rate may be able to exert an effect . 
 in the first , whether through the action of a carcinogen , a virus , or some unknown factor , a normal cell is transformed into a cancerous cell , which then lies dormant . 
 of these two steps , the first need not be considered further because , although it was once suggested that the mitosis rate at the time of application of a carcinogen has an effect on the number of resulting tumours ( mottram , 1945 ) , this theory has now been abandoned ( bilsechowsky and bullough , 1949 )  . 
they must compete with the healthy cells for the nutrients in the fluids of the tissue spaces . " some of them may even succumb , and it seems highly probable that those which do survive do not begin to multiply actively until they are stimulated to do so . 
the theory developed below is that the stimulus to multiplication may he any one of the several factors that are known to promote cell division in normal cells , and there fore that a close and direct connexion may well exist between normal mitotic activity and carcinogenesis . 
it is well known , for instance , that carcinomas , derived from mitotically active epithelia , are of much commoner occurrence than sarcomas , derived from mitotically inert connective tissues . 
on the one hand , the only extensive study of normal mitosis rates in a wide varietv of tissues concerns the female mome ( bullough , 1946 ) , while on the other the only extensive analysis of the natural tumour yield tissue by tissue concerns man ( annual statistical reviews of the registrar - general )  . 
first , it is evident that epithelia such as those of the vagina , uterus , and : rectum , which are naturally most highly active mito tically , are also most liable to develop tumours , while such mitotically inert tissues as striped muscle and brain do so ra : re ] y if at all . 
one such exception is the duo denal mucosa , which , though it has a normal mitosis rate as high or higher than that of the : rectal mucosa , shows a relatively low tumour yield . 
the mammary gland , which , though it shows far less mitotic activity than the lining epithelium of the vagina , has a tumour yield which is : relatively extremely high . 
willis ( 1948 ) emphasu , ed this strongly when he noted that " in the breast , fibro - adenomas are almost always situated in a bed of hyperplastic tissue , and persistent cystic hyperplasia is an important pre - cancerous state . 
 persist , eventually evoke progressive neoplasia as well . ' ' incidentally this seems to he the explanation of the action of croton oil , which , after the application of a carcinogen , greatly increases the tumour yield in mice . 
 it is a substance which has been shown to cause a local increase of as much as six - fold in the epidermal mitosis rate ( bullough , unpublished )  . 
 h now it is admitt.ed that some connexion may be traceable between local mitotic activity and local tumour genesis , it is reasonable to consider that some connexion may also be found between the general mitosis rat.e of the body as a whole , and the chance that somewhere within that body a tumour may develop . 
 as for the suppression of mitosis and of carcinogenesis , it is evident that both can be achieved by means of a restricted diet , and in view of the apparent role of carbohydrat.e during cell division , it may be expected that anything which limits the production of energy in the tissues will have a similar effect . 
one such substance is phloridzin , which inhibits phosphorylation , and another is dinitro phenol , which is said to uncouple the processes of phosphorylation and oxidation ( loomis and lipmann , 1948 )  . 
as regards phloridzin , bullough ( 1949b ) has described its effect in depressing the mitosis rat.e , and he has also obtained results showing a lowered yield of spontaneous mamma " " y tumours . 
as regards dinitro phenol , clowes and krahl ( 1936 ) first noticed its power to inhibit.mitosis , and tannenbaum and stlverstone ( 1949b ) have recently shown that it , too , reduces the yield of spontaneous mammary tumours  . 
environmental cold and muscular exercise are also known to depress mitotic activity , apparently by di , erting t - 0 other uses the energy produced from carbo hydrat.e ( bullough , 1949a )  . 
tannenbaum and silverstone ( 1949b ) have now shown that cold has a similar depressing effect on carcinogenesis , but the effect of prolonged muscular exercise has apparently not yet been determined . 
thus the explanation of the connection between hyperplasia and cancer may rest quite simply with the fact that with a higher mitosis rat.e there is a correspondingly higher chance that some lat.ant tumour cell will be stimulated to multiply , an effect which will become evident both in the earlier development of tumours , and in the appearance of many which would otherwise never have formed . 
conversely , hypoplasia may be expected to reduce the chances of multiplication , and so , as tannenbaum 's ( 1947 ) results show , to delay the development of those few tumours which do form and to prevent the appearance of many which otherwise would have formed . 
it appears possible that the average length of the period of dormancy , which every newly - formed tum.our cell appears to experience , is determined by the mitosis rate of the tissue in which the cell lies . 
 the mitosis rate itself is determined by a variety of factors , local and general , normal and abnormal , of which one is the carbohydrate , or calorie , supply . 
 this conclusion is in agreement with a suggestion that the practical problem of cancer can be divided into two distinct parts : the formation of the latent tumour cell , and the breaking of its period of dormancy . 
already it is known that the period of dormancy can be lengthened simply by means of a restricted diet , and with a more detailed understanding of those factors which control normal mitotic activity other practical methods may be devised . 
 already it is known that the incidence of human cancer varies in direct proportion to body weight , and therefore presumably to food intake , and it does not seem impossible that the idea of strict dieting to maintain the body weight of the middle - aged at an optimum level may some day be an accepted and normal practice . 
 as a postscript , attention may be drawn once more to tannenbaum 's ( 194 : 7 ) observation that with restricted diets disease incidence as well as tum.our incidence is markedly lowered . 
in considering this further question it seems possible that parasites penetrating into a tissue may , like the latent tumour cells , have to compete with the normal cells for the available nutrients . 
already it is known that in conditions of hypoglycaemia canaries are less liable to contract malaria ( hegner , 1937 ) and rats are less liable to contract tuberculosis ( steinbach and duca , 194 : 2 )  . 
 it now appears that the whole subject of competition between cells , and perhaps also between tissues , is worthy of the most serious consideration for the practical results which it may yield . 
this process is one of the most fundamental of cell mechanisms , so fundamental indeed that , except in minor details , it has never been influenced by evolutionary change . 
obviously the physiology of such a process is particularly fascinating , and in addition it is becoming clear that its study may shed important light on a variety of practical problems . 
 however , the greater part of this work has been from the viewpoint of pathology , and has resulted on the one hand in the mass of observations on the effects of carcinogenic substances , and on the other with the discovery of the so - called mitotic poisons ( loveless and revell , 1949 )  . 
by comparison , the direct study of the physiology of normal mitosis has been surprisingly neglected , presumably because of the difficulty of the techniques involved , and becaube the practical value of such knowledge has not been fully appreciated . 
 the present discussion starts with a consideration of the physiology of normal mitosis in mammalian tissues , and continues with an examination of its relation to modern work on carcinogenesis . 
 in recent years a considerable amount of attention has been paid to the problem of mitotic activity in the epidermis of the mouse ( bullough , 1948a , 1948b , 1949a , 1949b , 1949c , 1949d , 1950a , 1950b , 1950c ) and of the general biology of the skin ( medawar , 1947 , 1948 , 1949 )  . 
the work on the mouse epidermis began with an analysis of the diurnal cycle of mitotic activity , which was found to be a simple rhythm directly determined by the waking and sleeping habits of the animals . 
factors determining the form of the diurnal cycle are the accustomed times of feeding , the quantity and quality of the food given , and the age and sex of the animals . 
it was found that by means of subcutaneous injections of glucose or starch the mitosis rate can be raised in both active and sleeping mice to a level considerably higher than normal . 
 further studies have indicated that the epidermal mitosis rate is related , not to the blood - sugar concentration , which is high during hours of activity and low during hours of sleep , but to the concentration of intracellular glycogen . 
 bullough and eisa ( 1950 ) have shown that the diurnal cycle of glycogen concen tration in the skin is exactly similar to the diurnal cycle of epidermal mitotic activity . 
it is well known that glucose is deposited from the blood during sleep , and , while most of it is stored as glycogen in the liver , it is now evident that significant quantities are also deposited elsewhere . 
the most obvious alternatives were either that carbohydrate is incorporated , for instance as ribose , in the new nucleo plasm or cytoplasm as it is formed , or that it is destroyed to provide energy . 
the second was strengthened when it was found that the stimulus obtained from extra starch can be augmented by coincident injections of phosphate , and that , conversely , mitosis can be almost eliminated by injections of phloridzin , a substance known to inhibit phosphorylation ( bullough , 1949b )  . 
the conclusion that mitotic activity may involve the expenditure of a significant amount of energy also receives support from the results of experiments made with dividing eggs by such men as brachet ( 1932 ) , runnstr5m ( 1933 ) , and zeuthen ( 1946 , 1947 , 1948 )  . 
 in mammalian epidermis the importance of oxygen has been stressed by medawar ( 1947 ) in the rabbit , and by bullough and johnson ( bullough , 1950c ) in the mouse . 
when this tissue is kept in vitro anaerobic conditions inhibit cell division , and it is now clear that glycogen , phosphate and oxygen are all involved at the onset of an epidermal mitosis . 
however , since in a normal body it seems unlikely that either phosphate or oxygen are ever in such short supply as to become limiting factors in cell division , further elaboration of this point is not necessary here . 
 summarizing what has been said above it is evident that , in a normal mouse , carbohydrate in the form of glycogen or glucose is a most important substance determining mitotic activity , and that its apparent function is to supply the energy requirements of cell division . 
as one outcome of these conclusions it was to be expected that diet would be found to have an important effect on the mitosis rate , and this has now been confirmed ( bullough , 1949c )  . 
 it was later confirmed that a restricted diet results in a lowered body weight , a reduced glycogen reserve , and hence a reduced mitosis rate ( bullough and eisa , 1950 )  . 
however , while the body weights and carbohydrate reserves were found to vary in direct proportion to the degree of underfeeding , the rate of epidermal mitosis varied in a complex manner expressible in terms c , f a sigmoid graph . 
 it must be added that while the results primarily concerned the epidermis , other observations showed that similar conditions develop in other tissues , and it can b6 safely concluded that the reduction of mitotic activity by diet is a general effect visible throughout the body . 
 the striking thing about these observations is that they parallel so closely the results of recent work by tannenbaum ( 1940a , 1940b , 1942a , 1942b , 1944a , 19441 > , 1945 , 1947 ) and tannenbaum and silverstone ( 1949a , 1949b ) , who have in introducing this studied the effects of restricted diets on carcinogenesis . 
 subject it is vitally important to emphasize that it is indeed the genesis of tumours that is being considered , and not the growth of tumours once they have been formed . 
the growth of a visible tumour is only influenced in slight degree by variations in diet , and it is only in the process of tumour genesis that diet has any pronounced effect . 
the greater part of the earlier evidence was reviewed by hoffman ( 1937 ) , who came to the conclusion that " ovemutrition is common in the case of cancer patients to a remarkable and exceptional degree . " this statement can be justified by figures such as those of dublin ( 1929 ) , who showed statistically that persons who are overweight during middle age have a higher expectation of death from cancer than those who remain underweight . 
his first experiments involved a simple restriction of diet , and led to the surprising discovery that animals maintained on a 66 per cent diet are more active , develop fewer tumours and fewer diseases , and so live longer on the average than do the fully fed controls . 
 in later experiments all groups were provided with a basic diet of protein , fat , vitamins , and minerals , and the only differences lay in the amount of carbohydrate which they received . 
of male dba mice painted 19 times with 3 : 4 - benzpyrene , one group of 50 fed ad libitum developed 32 tumours , while another group of 50 fed on a carbohydrate restricted diet developed only 11 . 
as a general principle it can be said that the most striking results are obtained with spontaneous tumours , which are often prevented altogether , and it is evident that with induced tumours the modifying effect of the diet can be at least partly masked if sufficiently heavy doses of carcinogens are given . 
 in both cases this relation is expressible by means of a sigmoid curve , and the great.est fall in both the mitosis rate and the tumour yield accompanies a reduction of from 80 per cent to io per cent of the full diet . 
thus with an average daily intake of about 14 calories the latent period in one experiment had an average length of about 18 weeks , while with an intake of 8 c9.lories the latent period was 39 weeks . 
are that carbohydrate , or calorie , shortage causes reduced body weight , a strongly depressed mitosis rate , the restriction or prevention of a wide variety of spon taneous and induced tumours , a considerable delay in the time of appearance of those few tumours which do develop , fewer dise.ases of all kinds , and consequently a healthier and a longer life . 
tannenbaum ( 1947 ) himself has no explanation to offer , but he has rightly emphasized one crucial point that , like the depression of mitotic activity , the prevention of tumour genesis by calorie restriction is the result of a general effect operating throughout the whole body . 
 at this point it is evident that a prima jooie case can be bmlt up to indicate a connexion between the three factors carbohydrate lack , mitosis depression , and reduced tumour incidence . 
further , it appears possible that these factors may be related to each other in this sequence , carbohydrate lack limiting mitotic activity , and low mitotic activity limiting carcinogenesis . 
however , before attempting this analysis it is important to consider at what possible point in the sequence of events leading to the formation of a tumour the mitosis rate may be able to exert an effect . 
 in the first , whether through the action of a carcinogen , a virus , or some unknown factor , a normal cell is transformed into a cancerous cell , which then lies dormant . 
 of these two steps , the first need not be considered further because , although it was once suggested that the mitosis rate at the time of application of a carcinogen has an effect on the number of resulting tumours ( mottram , 1945 ) , this theory has now been abandoned ( bilsechowsky and bullough , 1949 )  . 
they must compete with the healthy cells for the nutrients in the fluids of the tissue spaces . " some of them may even succumb , and it seems highly probable that those which do survive do not begin to multiply actively until they are stimulated to do so . 
the theory developed below is that the stimulus to multiplication may he any one of the several factors that are known to promote cell division in normal cells , and there fore that a close and direct connexion may well exist between normal mitotic activity and carcinogenesis . 
it is well known , for instance , that carcinomas , derived from mitotically active epithelia , are of much commoner occurrence than sarcomas , derived from mitotically inert connective tissues . 
on the one hand , the only extensive study of normal mitosis rates in a wide varietv of tissues concerns the female mome ( bullough , 1946 ) , while on the other the only extensive analysis of the natural tumour yield tissue by tissue concerns man ( annual statistical reviews of the registrar - general )  . 
first , it is evident that epithelia such as those of the vagina , uterus , and : rectum , which are naturally most highly active mito tically , are also most liable to develop tumours , while such mitotically inert tissues as striped muscle and brain do so ra : re ] y if at all . 
one such exception is the duo denal mucosa , which , though it has a normal mitosis rate as high or higher than that of the : rectal mucosa , shows a relatively low tumour yield . 
the mammary gland , which , though it shows far less mitotic activity than the lining epithelium of the vagina , has a tumour yield which is : relatively extremely high . 
willis ( 1948 ) emphasu , ed this strongly when he noted that " in the breast , fibro - adenomas are almost always situated in a bed of hyperplastic tissue , and persistent cystic hyperplasia is an important pre - cancerous state . 
 persist , eventually evoke progressive neoplasia as well . ' ' incidentally this seems to he the explanation of the action of croton oil , which , after the application of a carcinogen , greatly increases the tumour yield in mice . 
 it is a substance which has been shown to cause a local increase of as much as six - fold in the epidermal mitosis rate ( bullough , unpublished )  . 
 h now it is admitt.ed that some connexion may be traceable between local mitotic activity and local tumour genesis , it is reasonable to consider that some connexion may also be found between the general mitosis rat.e of the body as a whole , and the chance that somewhere within that body a tumour may develop . 
 as for the suppression of mitosis and of carcinogenesis , it is evident that both can be achieved by means of a restricted diet , and in view of the apparent role of carbohydrat.e during cell division , it may be expected that anything which limits the production of energy in the tissues will have a similar effect . 
one such substance is phloridzin , which inhibits phosphorylation , and another is dinitro phenol , which is said to uncouple the processes of phosphorylation and oxidation ( loomis and lipmann , 1948 )  . 
as regards phloridzin , bullough ( 1949b ) has described its effect in depressing the mitosis rat.e , and he has also obtained results showing a lowered yield of spontaneous mamma " " y tumours . 
as regards dinitro phenol , clowes and krahl ( 1936 ) first noticed its power to inhibit.mitosis , and tannenbaum and stlverstone ( 1949b ) have recently shown that it , too , reduces the yield of spontaneous mammary tumours  . 
environmental cold and muscular exercise are also known to depress mitotic activity , apparently by di , erting t - 0 other uses the energy produced from carbo hydrat.e ( bullough , 1949a )  . 
tannenbaum and silverstone ( 1949b ) have now shown that cold has a similar depressing effect on carcinogenesis , but the effect of prolonged muscular exercise has apparently not yet been determined . 
thus the explanation of the connection between hyperplasia and cancer may rest quite simply with the fact that with a higher mitosis rat.e there is a correspondingly higher chance that some lat.ant tumour cell will be stimulated to multiply , an effect which will become evident both in the earlier development of tumours , and in the appearance of many which would otherwise never have formed . 
conversely , hypoplasia may be expected to reduce the chances of multiplication , and so , as tannenbaum 's ( 1947 ) results show , to delay the development of those few tumours which do form and to prevent the appearance of many which otherwise would have formed . 
it appears possible that the average length of the period of dormancy , which every newly - formed tum.our cell appears to experience , is determined by the mitosis rate of the tissue in which the cell lies . 
 the mitosis rate itself is determined by a variety of factors , local and general , normal and abnormal , of which one is the carbohydrate , or calorie , supply . 
 this conclusion is in agreement with a suggestion that the practical problem of cancer can be divided into two distinct parts : the formation of the latent tumour cell , and the breaking of its period of dormancy . 
already it is known that the period of dormancy can be lengthened simply by means of a restricted diet , and with a more detailed understanding of those factors which control normal mitotic activity other practical methods may be devised . 
 already it is known that the incidence of human cancer varies in direct proportion to body weight , and therefore presumably to food intake , and it does not seem impossible that the idea of strict dieting to maintain the body weight of the middle - aged at an optimum level may some day be an accepted and normal practice . 
 as a postscript , attention may be drawn once more to tannenbaum 's ( 194 : 7 ) observation that with restricted diets disease incidence as well as tum.our incidence is markedly lowered . 
in considering this further question it seems possible that parasites penetrating into a tissue may , like the latent tumour cells , have to compete with the normal cells for the available nutrients . 
already it is known that in conditions of hypoglycaemia canaries are less liable to contract malaria ( hegner , 1937 ) and rats are less liable to contract tuberculosis ( steinbach and duca , 194 : 2 )  . 
 it now appears that the whole subject of competition between cells , and perhaps also between tissues , is worthy of the most serious consideration for the practical results which it may yield . 
woodyatt. * from the meyerstein institute of radiotherapy and the bland sutton institute of pathology , middlesex hospital , london , w.1. received for publication february 15 , 1950 . failure in the treatment of malignant disease is most often due to the occurthere rence of metastasis before treatment of the primary lesion is instituted . are , however , a number of cases in which the tumour remains localized for a considerable time , but cannot be removed surgically on account of its size and anatomical situation , and cannot be destroyed by radiotherapy without irreit is the aim of the radioparable damage to neighbouring normal tissues . therapist to exploit the differences in sensitivity between normal and neoplastic tissues , and it is the object of this research to see whether the effects of radiotherapy on certain tumours can be enhanced by modification of the techniques of therapy in common use at present . a course of x - ray treatment involves a number of variable factors . 
the segments , usually 2 or 4 in number , and as nearly as possible of equal size , were then treated by one or more experimental techniques , while one segment was treated by a control technique . segments not being treated were protected by lead shields while neighbouring segments were irradiated , and care was taken to avoid overlap of adjacent segments or an untreated gap * b.m.a. 
woodyatt between them by careful skin markings and " setting up . " the question of side - scattering of x - rays from one segment into adjacent ones was investigated by physical measurements with micro - ionization chambers in a wax " phantom . " the amount of scattered radiation was found to be less than 5 per cent at 1 cm . from the edge of a treated segment , and this was considered small enough to be ignored . in this way erroneous conclusions resulting from unpredictable individual variations in response are largely eliminated , and each case constitutes a complete separate experiment . 
the results of individual experiments can later be compared to see whether the experimental technique in question regularly produces a particular effect . the tumours and surrounding skin were examined at frequent intervals to follow progress , and to detect and note differences in response between the areas . in addition , biopsies were taken from all areas before , during and after treatment . at first , weekly biopsies were taken , but it soon became obvious that in the earlier stages more frequent examinations were necessary , while after completion of the course of treatment intervals of a month or more might elapse . 
the sections were examined by a pathologist who not only had no preconceived views about the various techniques of irradiation employed , but was kept in ignorance of the area from which each specimen had been taken . biopsies from each area before treatment were studied carefully to provide a base line , and also to give an idea of the degree of variation between different this variability was often found to be marked , and areas of the same tumour . differences in biopsies subsequently taken from the several segments had often to be discounted as representing no more than possible chance variations . 
fractionation is , however , usually by equal daily doses given on 5 or 6 days each week , and this fractionation technique is applied with little discrimination to widely different sorts of tumour . certain theoretical considerations , mentioned below , suggested that a different method of fractionation , leaving longer intervals between the fractions , might be more effective . 
an important direct effect of a dose of irradiation is temporary suppression of mitotic activity . koller ( 1948 ) found that in squamousand basal - cell carcinomas of the skin the number of dividing cells was considerably reduced 6 hours after 200r , and that after doses of 400r and 500r mitotic suppression might last for several days . 
the susceptibility of cells to irradiation damage varies at different periods of their life cycle , being greatest in early prophase ( lea , 1947 ) , and irradiation given spear and during the period of mitotic suppression is relatively ineffective . glucksmann ( 1938 , 1939 ) have demonstrated by experiments on irradiation of tissue cultures and animal tissues in vivo that a greatly enhanced lethal effect is obtained if fractions are spaced so as to coincide with the recovery of mitotic activity following the suppressive effect of the previous dose . information concerning the duration of mitotic suppression in human tumours it probably varies in different tumours , but will after different doses is scanty . depend largely on the size of the dose . 
a clinical investigation indicating advantages from a wider spacing of fractions has been reported by koller and smithers ( 1946 )  . koller ( 1948 ) considers that the nature of the tumour bed and the indirect effects of irradiation on the stromal reaction in the surrounding normal tissue exercises an important influence on the response of the tumour itself . 
a further limitation was , of course , imposed by consideration for the patient 's welfare , and no case was undertaken where it was felt that there would be less chance of effecting a cure by the method . tumours of three types were treated - large rodent ulcers ( 2 cases ) , carcinomas of the skin ( 5 cases ) , and carcinomas of the breast involving the skin ( 4 cases )  . most tumours of the first two types are radio - sensitive , and a successful result could normally be expected from the use of an orthodox technique . these tumours were treated in order to assess the relative efficiency of the experimental techniques , and to determine any differences in the reaction of normal tissue at the edge of the tumour . the cases of carcinoma of the breast were of special interest , for , as is well known , a considerable proportion are markedly radio - resistant . 
the usual erythematous reaction developed , and proceeded to moist desquamation over the tumour and surrounding skthe area of skin at the periphery which was only covered by the original 71 x 15 cfields showed pigmentation , but no desquamation . 
the dose to this skin area had only been about 2000r when the smaller fields were substituted . no difference in reaction or tumour response in the two areas was apparent at this stage . on october 6 , as viable tumour was still feared to be present , further treatment was given as described . three weeks after the conclusion of treatment a marked difference was apparent between the two areas . 
the area treated by the control technique ( area 1 ) was completely healed over by healthy new epithelium except for a small ulcer at the site of the first surgical attack . 
the remaining tumour consisted of some firm pink papillary processes , almost flush with the surface . in area 2 much of the tumour and surrounding skin covered by the treatment applicator was still raw and denuded of epitheliuthe remaining tumour was a little flatter than in the control area . eight weeks after treatment further flattening was apparent . area 1 was healed except for the remains of the ulcer . area 2 showed very little progress of healing , although a few islands of epithelium had appeared in the raw skin area ; there was some discharge from a fissure between two sessile processes . four months after treatment a striking difference between the two areas was apparent . 
the control area was healed and showed marked pigmentation , all that remained of the tumour being some fibrotic nodularity beneath the surface . area 2 showed up as a sharply outlined , completely unpigmented square , corresponding to the treatment applicator . there was still an indurated fissure at the site of the tumour , and an area of skin below the tumour remained unhealed and had clearly undergone necrosis . five and a half months after treatment the patient complained of burning pain in the lower part ( area 2 ) , and an increase in discharge from the fissure which was still present . 
a month later ( april , 1948 ) radionecrosis was obviously developing in area 2 ; the fissure had deepened , its edges were grey and necrotic , and the surrounding tissues were pale and avascular , and as hard as cartilage . by may a large necrotic ulcer corresponding to area 2 had developed . local treatment failed to bring about healing , so in november , 1948 , the whole treated area was excised , after a preliminary colostomy . this was done partly because residual foci of active growth were suspected . 
woodyatt there was a moderate degree of associated inflammatory mitotic activity . biopsies taken from both areas during and after treatment showed reaction . progressive differentiation of the tumour cells with reduction in the percentage of viable cells and their final disappearance . 
no sign of tumour could be seen in the biopsies taken at 6months , and no significant differences between the series of sections from areas 1 and 2 were detected . 
a small nodule of recurrent growth ( 1.25 cdiameter ) had appeared , adjacent to the mastectomy scar , in february , 1945 . superficial x - ray treatment was given ( 4 daily doses of 800r ) and the nodule regressed , being quite healed by september , 1945 . 
3. - carcinoma of breast ( case 3 ) divided into four areas . 11111 11111 11111 total 3000r . in 27days area area area area total 4000 r in 26 days total 3000r in 27 days total 3680r in 24 days 11111 11111 11111 days i = biopsies taken from all areas , and on day 50 fig . 
the control technique was modified in this case , 150r being given daily instead of the usual 200r . this was done to bring it more into line with the average daily tumour dose administered in this clinic for carcinoma of the breast . 
by the end of treatment , february 18th , the greater part of the surface was covered by smooth granulation tissue . there was still a considerable amount of tumour present , with a subcutaneous shelf of induration palpable all round the edge . there was severe erythema of the surrounding skin , with much pain and discharge , and for these reasons treatment was curtailed . it is probable that the unusual severity of the reaction was due to infection of the raw surface , as the patient had fever up to 1010 f . 
the tumour had shrunk to 10 - 5 x 6 - 5 cm . the ulcer floor was covered by necrotic slough and its edges were still firm , but were softer and less raised in areas 1 and 3 . seven weeks after treatment the skin had begun to heal in area 3 . 
the skin in area 1 showed well - marked pigmentation , but was perfectly healed . well - marked differences were now apparent in the different areas of the tumour , which had shrunk further to 9 x 6 cboth areas treated by the control technique showed clinical evidence of active residual tumour , the ulcer in these areas having a hard raised edge with much adjacent subcutaneous induration . area 1 showed some suspicious induration , but less than in the areas treated by the control technique . area 3 was soft and nearly flat , with no definite sign of residual growth . 
6 at the end of treatment . the tumour cell mass in the upper part of the field shows extensive hyalinization , and there is heavy lymphocytic infiltration of the stroma . note that the magnification is the same as in fig . 
8 , 9 and 10 . - squamous - cell carcinoma of the ear ( case 8 )  . biopsies taken before , at about the middle of , and at the end of the course of treatment . 
the upper half was treated by technique i ( 500r twice weekly ) to a total of 3500r in 24 days , and the lower half by the control technique ( 200r daily ) to a total of 3600r in 24 days ; 95 k.v. 
x - rays clinically there was rapid regression of the lesion in both areas , were used . and the tumour had disintegrated completely before the course was finished . the serial biopsies showed a very satisfactory response in both areas , no viable cells remaining within two weeks of starting treatment . 
any conclusions we may draw from this small series of cases must be purely tentative ; the final evaluation of these techniques may require the elapse of a considerable interval of time , and in view of the possibility of variation in different parts of the same growth many cases must be studied before definite conclusions can be reached . complete equality of total dose and protraction were seldom obtained , and this introduces another variation from strict experimental conditions . 
with these facts in mind the following conclusions are cautiously presented . technique i ( 500r twice a week ) was used in 9 cases ; 3 squamous - cell carcinomas , 4 carcinomas of the breast , and 2 rodent ulcers . 
the clinical result in the 3 cases of epithelioma was uniformly good , and in one case this technique gave slightly quicker results than the control . in 2 cases of carcinoma of the breast this technique gave a better response , judged clinically and histologically , than the control ; in the other 2 cases the results were equally good . 
the cases of basal cell carcinoma responded better both clinically and histologically to the control technique ( daily fractions of 200r )  . technique ii ( looor once a week ) was tried in 4 cases ; 2 squamous - cell carcinomas of the skin , one carcinoma of the breast , and one rodent ulcer . 
he was considered too old for successful operative treatment so he was kept under observation and in february , 1954 , was readmitted to hospital with evidence of bone metastasis . 
apart from this , there is little irregularity of nuclear shape , size or staining density . these cells clearly form part of a fragment of tissue in the sputum , and because of the vacuolation of the cytoplasm , were considered to be diagnostic of adenocarcinoma . 
they are of adenocarcinomatous type and do not resemble cells usually seen in primary bronchial carcinomata . " an enlarged cervical gland was later removed for histological examination and was reported as showing a mucus - secreting adenocarcinoma , probably of colonic origin . the patient died , and post mortem examination was refused . it will be noted that the cells shown in the clump in fig . 
4 appear to surround a number of vacuoles , but gross vacuolation is not evident in the cells themselves . the larger mass is hollow , the wall being formed of a single layer of cells . i make it a practice only to report adenocarcinoma from sputum examination it cannot be too strongly emphawhen clumps of the types described are seen . sised that single cells containing vacuoles as shown in fig . 
the tracheo - bronchial glands may occasionally arow small amounts of the carbon to pass through into the thoracic duct or into lymphatic efferents from the glands which communicate directly with the great veins within the thorax , and thus the carbon reaches the such carbon in the blood stream is taken up by the cells of the blood stream . reticulo - endothehal system in organs hke the spleen and hver , which very occasionally at autopsy may show shght stippling with carbon , though in six spleens examined chemically we have found no weighable carbon in our residues . the amount of carbon deposited in a lifetime in the lungs and tracheo - bronchial glands depends on many variable factors such as age and occupation . 
where the degree of atmospheric pollution is great the excessive amount of carbon inhaled clogs the ciha of the respiratory mucous membrane and a large amount is not expelled even in the normal subject . in the subject who suffers from chronic catarrhal inflammation of the respiratory mucosa , there occurs ' a progressive destruction of the normal ciliated epithelium which is partially replaced by a non - cifiated type of a lower order , such as cuboidal or even squamous cens , which are unable to expel carbon particles . 
the scarring so caused is usuary the seat of dense areas of diffuse fibrosis resulting from bronchiectasis accumulation of carbon . or from the imperfect resolutions of acute pneumonias are often relatively free thus the only from carbon . 
why this should be so is not altogether clear . accurate means of assessing the total amount of carbon in the lungs and tracheobronchial glands as a whole is by estimating chemically all the carbon in these structures , and it is from this angle that we have approached the problethe amount found in these organs at autopsy thus represents what has been retained during a hfetime . 
the carbon itself may be innocuous , but from our studies of atmospheric pollution ( goulden and tipler , 1949 ; warer , 1952 ; goulden , kennaway and urquhart , 1952 ) , one can form some idea of the amounts of the carcinogens , 3 : 4 benzpyrene and arsenic , which would accompany it , and may possibly have some effect , either in association with , or apart from , that of tobacco . the black coloration of the lungs and bronchial glands must have become increasingly famihar to british pathologists since the industrial revolution which in the earlier part of the nineteenth century converted britain , by the utilisation of coal and iron , from an agricultural to a largely industrial country . although abundant material has been available in britain during the last 150 years , no one has , so far as we know , attempted to estimate the amount of carbon in human lungs , except in the special case of coal - miners ( king and gilchrist , 1945 )  . 
a questionnaire on the following points was circulated : sex ; age ; diagnosis and post - mortem findings ; places of residence for more than three years and the period lived in each ; occupations followed for more than three years ; the smoking history as regards the use of a pipe or cigarettes ; the age at which smoking was begun and stopped ; the maximum and average amounts smoked per day , and whether inhalation was practised always , occasionally or never . considerable difficulties were encountered in obtaining lungs from persons without bronchial carcinoma for controls ; those were needed from whom an accurate history could be obtained , but who were not likely to live long . 
joules of the central middlesex hospital , london , for the supply of material ; also to professor neils dungal of reykjavik for the lungs of eight persons who had always lived in iceland . 
the pulmonary glands in the lung substance were separated as far as possible from lung tissue ; no claim is made that this division , was carried out very accurately , but the much lower concentration of carbon in the lung makes some contamination with it unimportant . 
the separation oflymph glands is of course still more difficult when a large invasive mass of bronchial carcinoma is present ; the practice has been to regard as lymph glands any deep black stippled areas of simflar size and shape , and to class the remainder as lung . 
histology. - the lungs submitted to us had been fixed whole in formalin and thus the fixation from a histological point of view was not perfect . blocks of lung tissue were nearly always taken from the pleural region and from deep in the lung substance , and occasionally from the tracheo - bronchial glands . these blocks were subsequently refixed in formol - corrosive and the paraffin sections were stained by haemotoxylin , by carmalum or neutral red , by van gieson or mallory , and , in a certain number of cases referred to later , by potassium ferrocyanide to demonstrate any iron . 
the cases from hospitals in london ( tables ii and iii )  . - the places of residence and occupations given are those of longest duration only . in the case of persons hving in london , the part of london in which they hved is stated in brackets after a capital l ; for those living in other towns , the county is given i " cigarettes " expresses tobacco consumption in this form even where brackets . cigars or a pipe were smoked . 
tobacco is equivalent to 28 cigarettes . the small number of cases prevents any firm conclusions about differences in the amounts of carbon in the lungs ofpersons with and without bronchial carcinoma . these differences are not statistically significant , but are nevertheless of interest . the average amount of carb ' on in the lungs of females with bronchial carcinoma was greater than that in the controls ( table iii ) , although the carbon content of the glands did not differ appreciably between the two groups of women ; one might expect this result if some carcinogen such as 3 : 4 benzpyrene adsorbed on to the carbon particles in soot is concemed in the aetiology of lung cancer . 
the again , the carbon in two groups of men , however , showed the opposite result . the glands was approximately the same for the two groups , but the control group had the higher carbon content in the lungs . there was no apparent reason why men and women should differ in this way . the total carbon content of a lung must vary according to three chief factors , ( a ) age , ( b ) the size of the lung ( since a larger person will ' mspire more air and hence more carbon ) , and ( c ) the environment in which a person lived . allowance for the first of these variables is easily made . 
when the weight of carbon in the lungs and glands was divided by the age ( table iv ) the differences between the four groups remained and were still of the same order . 
the cases from iceland ( table v . ) - since these , specimens did not include the whole trachea , some of the bronchial glands may not have been present ; the figures in table v therefore represent the carbon and ash content of the lungs and glands together . the content of both carbon and ash in the women - 's lungs was considerably greater than that in the men 's , apart from the exceptional value for the man no . 
carbon in lungs / age in years . 25 - 1 ( 12 - 6 ) 13 - 8 15 - 4 11.9 bracketed averages include the abnormal figures for no . 
50. tthis very high value for a - sh was omitted from the average . microscopicary , no silica was found in sections of the lung . those obtained in london , shows that the lungs of icelandic men had a lower average carbon content , while those of the icelandic women had a much larger amount . 
the same differences obtained on correction of these figures for variation in age distributio ' n . the presence of such amounts of carbon in these lungs from iceland seemed at first sight surprising , for in iceland general atmospheric pollution as understood in this country is very small . there is no native coal or oil , and these are costly to import . 
was a non - smoker . in the group of women with bronchial carcinoma , i out of 5 did not smoke , and in the control group , 9 out these figures , especiary for the women , show a higher proportion of nonof 1 1 . smokers among persons without bronchial carcinoma . 
the total carbon content of the lungs varied over a wide range all the points indicating a total consumption of more than for non - smokers ; 200 , 000 cigarettes refer to men and women with bronchial carcinoma . 
the average daily consumptions were : males with bronchial carcinoma , 24 / day ( 16 cases ) ; males without bron ' chial carcinoma , 12 / day ( 5 cases ) ; females with j . 
urquhart bronchial carcinoma , 19 / day ( 5 cases ) ; and females without bronchial carcinoma , 2 / day ( 10 cases )  . ash content of the lungs and bronchial glands . the nature of the ash deposited from the hydrolysates of these lungs has not although about 10 per cent of the total carbon was contained been determined . in the glands , the fraction of the total ash present in them was about 20 per cent . this suggested that the bronchial glands were even more efficient in concentrating particles of mineral matter than they were in accumulating carbon particles . 
for comparison with the histological findings the chemical results were divided into three groups , namely , those with a carbon content of ( a ) 0 - 49 g . 
the carbon in the sections showed the normal distribution , being heavier under the pleura , around the bronchi and blood vessels and in the fibrous septa , than in the vesicular portions of the lung . the rocks of iceland are of volcanic origin and the roads are metaned with such material which , due to weathering , quickly breaks down so that with the passing probably road dust has become considerable of traffic much dust is created . in iceland , where there are now 11 , 000 motor vehicles , only since the acquisition in view of this the icelandic lungs were of american cars after the last war . submitted to a more intense microscopic study for the presence of sihca and of iron . 
no evidence of silicosis was noted in any and doubly refractile granules of in only one case was iron silica were very scanty or absent in all the sections . found , apart from occasional heart - failure cells in the others . in this case the iron was present chiefly in the fibrous tissue of the septa and around the bronchi and blood - vessels in close association with carbon particles which the iron pigment appeared to surround . 
is retained ; this gives some measure of the efficiency of the nasal filter and of the mechanism by which particles which have reached the deeper respiratory passages are swept upwards again by ciliary action and expectorated or swallowed . 
when the floor of a room is swept towards the door , the part adjacent to the door is exposed to dirt from a much larger area . similarly , when particles of dust are arrested on the walls of the smaller bronchi and bronchioles , they are swept upwards by ciliary action through the main bronchi ( the door ) into the trachea , and carcinogens might diffuse from the particles into the layer of mucus covering the bronchial mucous membrane during transit . 
some such mechanism would be in accord with the statement about the site quoted above ; but some recent investigators ( westermark , 1938 ; raebum , 1951 ; raebum and spencer , 1953 ) think that tumours arise - with about equal frequency in any part of the lung . the estimations of arsenic and of 3 : 4 benzpyrene in the air of large towns given in table viii are those of goulden , kennaway and urquhart ( 1952 ) and table viii . - concentrations of arsenic and of 3 : 4 benzpyrene in town air . london ( becton ) bilston manchester liverpool . sheffield london ( county hall ) hull bristol mean concentrations , pg . 
a8203per cigarette ( daff and kennaway , 1950 )  . ini ' mum amount of a strong carcinogen such as i : 2 : 5 : 6 ' dibenzanthracene which will produce * our earlier results , which were confirmed subsequently , were demonstrated at a meeting of the pathology section of the royal society of medicine held at this hospital on january 15 , 1952 . shear ( 1936 ) found that the j . 
of 3 : 4 benzpyrene which may be inspired in ' a lifetime , but in view of the vastly greater area over which this may be spread and the different time relations , one may doubt whether this comparison has any value . the size and arrest of smoke particlm . the available data about the arrest of smoke particles in the air passages are very defective because we have not , to begin with , any adequate information about the size of these particles . 
the passages quoted verbatim below contain all the information that we have found on this subject . the leicester report says : " the size distribution of smoke is a subject which still requires investigation . green ( 1936 ) gives estimates for five industrial dusts from which it can be inferred that 50 per cent by weight of such dusts is less than 3 to 10 microns , and 80 per cent is less than 5 to 15 microns in mean diameter . atmospheric smoke may be similar in size distribution but a direct investigation is  . 
some of the properties of smoke depend on the area it can cover ; half the surface or sectional area of the smoke was in particles larger than about 0 - 35 micron . there is a distinct tendency for smoke particles to stick together in chains , perhaps one micron long . " the comparison of such results obtained by different methods of arrest is not e . 
are in the range of size where there is minimum retention in the lung , 80 per cent of them being exhaled and 20 per cent arrested in the alveoli . ( b ) the mean diameter of smoke particles and the range of particle size of carbon black which shows the greatest adsorption of 3 : 4 benzpyrene from benzene ( falk and steiner , 1952 )  . 
though the material was not statisticary adequate , the smoking histories of the cases examined showed a higher consumption of tobacco among both men and women with bronchial carcinoma compared with the controls . 
if the carbon in the lungs and bronchial glands does not leave the body by any channel the amount found post - mortem represents what is retained out of the intake of a lifetime . 
the data now available for atmospheric poflution in some english towns arows an estimate to be made of the amount inspired during a hfetime in them ; this might be of the order of i 00 g . , while the quantity found in the lungs and bronchial glands was approximately 0 - 5 to i - 0 g . 
estimations of 3 : 4 benzpyrene and of arsenic in the suspended matter of the air of various english towns enable one to calculate the amounts of these compounds which would accompany the carbon inspired , and retained , in a lifetime . we wish to express our gratitude for the materials and case histories which have been the subject of this investi ation to professor niels dungal of revkiavik ; to horace joules of the central middlesex hospital , london , and to two members of his staff , a . 
a fuller account will be found in appendix i . it is sufficient to note here that it is a slightly modified form of the ordinary death rate which would be calculated as 2 l ( x ) m ( x ) l ( z ) ' the reasons for introducing such a modification are twofold : firstly , it makes allowance for the fact that the specific death rate considered is underestimated owing to deaths from other causes , and secondly , it measures the rate at which animals are dying out from the cause under investigation at the moment , x , not the bulk death rate over a month . the latter property allows a continuous curve to be drawn through the calculated values whose ordinates measure the rate of mortality at any moment of life . 
the monthly death rates on the other hand are strictly discontinuous , being , as is shown in appendix i , functions of the area under the , ( x ) curve over the month in question . using the method of haldane given in appendix i , the values of , ( x ) for cancer were calculated for a number of strains . those for three strains whose life tables were given by murray and hoffman ( 1941 ) are graphed in fig . 
1. the three curves bear out the conclusion of maurray and hoffman that the dba mice were the most susceptible , then the bittner albinos , and finally the marsh time in months fig . 
spicer albinos - a result which is the reverse of that indicated by the percentages dying the method of approach used here indicates that the cause of the of tumour . discrepancy is the difference that exists between the non - tumour death rates of the three strains . for if , using the methods outlined below , we calculate the percentage of cancer deaths that would be expected if eachl strain had the same non - cancer death rate as the marsh albinos , we find the following values : bittnera marsh a  . 
~. corrected to marsh - a . 90 5 per cent 87 - 7 76 - 6 uncorrected . 67 7 per cent 73.7 76 - 6 the process of calculating the p ( x ) 's has involved some smoothing of the data , and in the graphs no attempt has been made to draw a smooth curve ; the points have merely been joined by straight lines . 
the irregularities in the curves are mostly due to random errors , though the flattening of the , u ( x ) curve for dba mice from the 12th to the 15th month is repeated in the curve for another group of the same strain , and is therefore probably due to some real interruption of the steady increase in the tumour mortality . a further series of , l ( x ) curves are given in fig . 
3. allowing for this by subjecting the a - ro mice to the a - fc non - cancer , ( x ) , it is found that they would have almost the same percentage of cancer deaths . the percentage of cancer expected in the a - ro mice at the a - fc death rate is in fact 86 , while the percentage found in the a - fc is 88 . it appears then that almost the whole 302 c . 
the most obvious method of comparison is to compare the numbers or proportion of cancer deaths in any strain with those of a strain having a standard non - tumour death rate . alternatively the number of deaths over a similar period of time may be calculated when all non - tumour mortality has been eliminated . both of these indices can be calculated using the , ( x ) values . the difficulty of this approach is to find a standard which is equally useful for all strains , since there are wide variations in life span and in o 15 iii 0 ' 30 0.25 0 20 - o * i 0.10 time in months fig . 
murray and hoffman ( 1941 ) have attempted to overcome the first difficulty by using a life span as a unit and expressing time in percentiles of this value . this method seems to be unsatisfactory in that the determination of the length of span is to some extent arbitrary . 
murray and hoffman use the time at which 1 per cent of animals are surviving , adding that it would be possible to use the 0.1 per cent point if larger numbers of animals were available . 
each of these two cut - off points would give a different system furthermore these authors make no direct allowance for differences of time units . in non - tumour mortality , though they discuss the merits of a number of arbitrary weighting factors for calculating averages of the monthly cancer death rates . to avoid the use of arbitrary systems of weights it seemed best to calculate indices of susceptibility after the non - tumour death rate has been eliminated . this was done using a method due to dublin and lotka ( 1920 , 1921 ) , which has also been discussed by karn ( 1933 ) and irwin ( 1935 )  . 
spicer quently pointed out that the estimates might be improved by using the method of maximum likelihood , which gives results having a smaller standard error . the full calculations are rather more laborious than in the case of dublin and lotka 's method . 
6. it will be seen that the process of summation has resulted in a considerable smoothing of the data , and though the original , u ( x ) curves are not all similar in form , the integrated curves approach more closely to this ideal which is essential if strict comparisons of tumour susceptibility are to be made . after some initial confusion the curves spread out from left to right in order of decreasing susceptibility . 
any horizontal line drawn across the figures will give , by its intersections with the curves , the times of equal proportional mortality . vertical lines will give the proportional mortality corresponding to equal times of life . 
they are : 25 6 for the cross with a dba mother , and 37 8 for the reciprocal . from a study of the , ( x ) graphs it is obvious that the differences in the form of the curves from strain to strain make strict comparisons of tumour susceptibility , of the same kind as are made in biological assay , impossible . future work will probably reveal some of the factors which determine the shape of the curves , but in the meantime it should be emphasized that susceptibility to mammary tumour is determined in a different way in each strain , though the similarity of the , u ( x ) curves of different groups of mice of the same pure line does enable more exact comparisons to be made in this case . 
haldane , who first suggested that the , t ( x ) curves could be used for the investigation of tumour susceptibility , and who provided me with the method of calculation given in appendix i . 
 ( - ) = log.e 2 = 0 693 gives the half life . ( 4 ) modified expectation of life . the number obtained by taking the reciprocal of the sum x log . 
 ( 1 / px ) for the whole table is of interest since it gives an estimate of the expectation of life . suppose the table extends over ages from o t so that the sum of probabilities is then we can twrite the reciprocal of this sum t1 log . 
 ( 1 / p ) = t , j ( x ) dx ' ( x ) 1 ( x ) dx if there is no cause of death but cancer . so that the reciprocal is a weighted mean of the [ ( x ) 's . multiplying this by t , the interval over which the table extends , gives an estimate of the expectation of life . this estimate is rather lower than that given by the correct method of calculation since the values of 1 ( x ) are weighted in favour of the low values at the higher ages where the , u ( x ) 's are large . it might be preferable to use this modified life expectation instead of the half - life as it takes into account all the data and can be given a standard error . 
 ( p ) and the variance of the sum is equal to the sum of the variances since the p 's are independent . if we call this sum 2 then the variance of the half life will be given by and since and the standard error of x is var . 
levvis. from the chemi8try department , university of adelaide . received for publication may 23 , 1952 . soon after the discovery of the carcinogenic activity of 1 : 2 : 5 : 6 - dibenzanthracene by cook , kennaway and colleagues , yoshida ( 1932 , 1933 , 1934 ) and sasaki and yoshida ( 1935 ) reported that the addition of o - aminoazotoluene to the food leads to the production of malignant liver tumours in rats . during the past two decades scores of other azocompounds have been tested for carcinogenic activity of this type and many have been shown to be active . for reviews see shear ( 1937 ) , kinosita ( 1937 ) , cook ( 1939 , 1943 , 1948 ) , cook and kennaway ( 1938 )  . these carcinogenic azocompounds form a very interesting group . 
unhke the polycyclic aromatic hydrocarbons , they do not , as a rule , produce tumours at the site of injection , but mostly affect the liver . furthermore , the induction of liver tumours with azocompounds is markedl influenced bv the dieb , and if a cc protective " diet is supplied , the production of tumours can be strongly inhibited or even entirely prevented . all the azocompounds are , of course , artificial synthetic substances ; and they are highly coloured ( mainly orange to red )  . 
some are used as textile dyestuffs , and certain members of the group are used for colouring foodstuffs . the most part such compounds are probably harmless ( cook , 1948 )  . 
most of the food - colouring matters which have been tested have failed to induce liver tumours in rats ; and in any case it is most unlikely that anyone could ever consume enough of an azocompound in food to have any deleterious effect . 
to some extent the compound is also carcinogenic towards the bladder ( yoshida , 1935 ) , and it is interesting that the deaminated compound , namely 2 : 3 ' - azotoluene ( iii ) , was found to be non - carcinogenic to the liver of the rat , but produced numerous papillomas in the bladder ( otsuka and nagao , 1936 )  . many derivatives of azobenzene , containing substituent aminoand methylgroups , were tested for carcinogenic activity by kinosita ( 1937 )  . 
none of these produced cancer of the liver except o - aminoazotoluene , its mono - acetyland diacetylderivatives , and an isomer of o - aminoazotoluene , namely 4 - dimethylaminoazobenzene ( iv )  . 
the latter compound , which is also known as p - dimethylaminoazobenzene , and as n , n - dimethyl - p - aminoazobenzene , was formerly used as a food - colouring matter under the name of " butter yellow "  . 
the effects of such structural alterations are described in a following section . most of the known carcinogenic azocompounds are derivatives of 4 - dimethylnevertheless , a 4 - aminoaminoazobenzene , or at least of 4 - aminoazobenzene . this was shown for example , by group is not essential for activity of this type . cook , hewett , kennaway and kennaway ( 1940 ) , who examined the action of azonaphthalenes on mice . 
manv liver tumours , mostly of the type of cholangioma , were obtained with 2 : 2 ' - azonaphthalene ( vi ) , and a few tumours were obtained with 1 : 1 ' - azonaphthalene ( vii )  . 
lewis the same relative potencies do not always apply in other laborat - ory animals . it is well known , for example , that 4 - dimethylaminoazobenzene is much less active in producing ' hver tumours in mice than it is in rats . 
agents with therapeutic possibilities such as radio - phosphorus and the radio - iodines , and probably much better , suitable organic compounds containing radio - active isotopes , whose action depends on selective concentration of the radio - activity in particular cells . the separation on the industrial scale of non - radio - active isotopes and the practical development of the mass spectrometer open new possibilities of isotopic tracer research where radio - active effects are undesirable , as in many clinical investigations , or where , as in the case of nitrogen and oxygen , no suitable radioactive isotopes exist . the cyclotron still remains an essential instrument both for the production of small amounts of certain isotopes and as a source of fast neutrons for therait is by no means certain that the peutic trials in cancer and related diseases . frequency modulated cyclotron will be useful as a therapeutic source of fast j . 
mitchell neutrons , on account of the possibility of reduced neutron output and of the undesirability of a pulsed output . a promising field for radiotherapeutic investigation appears to be the study of high energy , 20 - 50 mev . 
prove more suitable than the synchrotron . the electron beam can now be extracted from these machines , the therapeutic possibilities of the high energy beta particles are rather uncertain and must be investigated with caution . the development of high energy generators opens the interesting possibility of the radiotherapeutic application of fast protons of energy in the region of 140 mev . 
 ( wilson , 1946 )  . the results of selected investigations are best summarized in the discussion of these newer agents . properties and production of isotopes , radio - active and stable . the properties of selected isotopes of especial interest are summarized in recent information on isotopes , which may be useful as radio - active table i . tracers , and which are produced in the pile , is summarized in table ii . 
a list of recent references on isotopes is also given . the pile is without a rival for producing isotopes in the very large number of cases where , during irradiation in the pile , a simple slow neutron capture process occurs , e.g. 
and for s35 10 millicuries per g . there is one slow neutron ( np ) reaction of especial importance : n14 + it is of interest that this process is probably responsible for n - > c14 + p . 50 - 80 per cent of the biological effects of thermal neutrons , the remainder of the effects being due almost entirely to the n - y reaction in hydrogen ( mitchell , however , the n , p reaction in nitrogen is of extreme importance for 1947 )  . isotopic tracer research as the basis for the preparation of c14 , the long - lived it has been shown by yankwich , rollefson and radio - active isotope of carbon . norris ( 1946 ) that the c14 is produced by slow neutron irradiation of compounds such as ammonium nitrate and urea in the form of very simple compounds such as c02 , co , ch3oh , h.cooih , and of especial importance as a starting - point for organic syntheses , hcn . in addition to the preparation of materials by direct irradiation , a very considerable number of radio - active isotopes are found as fission products in the uranium rods in a pile . 
a most valuable detailed list of these has been given by the plutonium project ( 1946 )  . in general , for the preparation of isotopes the yields with the cyclotron are very much smaller than those with the pile . 
the oxygen isotopes have been concentrated by distillation of water and by exchange reactions . sulphur has been separated by chemical exchange between so2 and the bisulphite ion . potassium has been also separated by chemical exchange methods . the development of the mass - spectrometer as a practical instrument and its routine use for hydrocarbon analyses by industrial laboratories in u.s.a. show clearly the possibility in medicine and biology of non - radio - active isotopic tracer investigations . 
an interesting possible diagnostic application of measurements of p32 in breast tumours in situ has been reported by low - beer , bell , mccorkle , stone , steinbach and hill ( 1946 )  . * the application of p32 as a tracer in metabolic investigations exemplifies the in order to avoid short - term problems raised by this method of investigation . effects , it is essential to calculate the dose of radiation received by the tissues for example , with p32 , one microcurie per g . from the radio - active isotope . * one line of metabolic tracer investigation insufficiently well known is the use of radio - active brominated compounds , e.g. 
of animal with times of observation of the order of 6 hours . of especial interest is the work of abels , kenney , craver , marinelli and rhoads ( 1941 ) , who accidentally found significant metabolic changes in the leucocytes in chronic leukaemias after total body x - radiation with doses as small as 3 r . , as a result of the radiation given by sub - therapeutic doses of p32 . of much greater importance in the clinical applications of isotopic tracer research is the avoidance of all possible risk of carcinogenesis as a long - term in a recent report on the result of the radio - active material introduced . " health protection activities of the plutonium project , " robert s . 
stone ( 1946 ) states that " it is now well established that ( radio ) strontium given to mice and rats in amounts insufficient to kill them for many months can cause bone and lymphatic tissue tumours to develop in significant numbers of animals . over long periods of time , plutonium has been shown to cause atrophy of the bone and bone sarcomas . " it is evident that great caution is necessary however , before introducing any radio - active materials into human subjects . it is likely that for many isotopes safe conditions for tracer work will be established after dosimetric studies and prolonged animal experiments . 
mayneord ( march 1 , 1946 - unpublished ) that the dose rate at 1 cfrom a point source of 1 millicurie of co60 enclosed in a platinum envelope of thickness 0 5 mis 11 - 1 r . 
however , it may prove more convenient to measure co60 sources in terms of equivalent radium . the production of large amounts of these isotopes by means of the pile raises the practical possibility of the therapeutic application of large gamma ray sources - " mass radiation units " equivalent to 50 - 100 g . 
mitchell in the form of na2hpo4 solution soaked in blotting - paper and dried . in addition to therapeutic applications , these beta - ray sources may be useful in experimental cancer research , e.g. 
stone ( 1946 ) states that " it has been established that single large doses of beta rays and multiple small doses can cause cancers in the skin without the animal being killed by the effect of the beta rays . " therapeutic possibilities of selectively concentrated radio - active agents . radio - active isotope therapy has as yet been limited to inorganic compounds . radio - phosphorus ( p32 ) , and to a much smaller extent the radio - iodines ( 1130 andi1131 ) , are the only isotopes with which limited clinical trials appear justified without further preliminary animal experiments . in general it seems unlikely that inorganic radio - active isotope therapy will stand the test of time . it seems much more hopeful to study the selective concentration by malignant cells of suitable organic compounds carrying radio - active isotopes of many elements ( rhoads , 1946 )  . the usual therapeutic applications of p32 in the form of na2hpo4 appear to depend upon its synthesis into nucleic acids by the multiplying cells . one other method of therapeutic application ofp32 reported ( jones , wrobel and lyons , see low - beer , lawrence and stone , 1942 ) depends on the selective concentration of colloidal anhydrous chromic phosphate by the cells of the reticulo - endothelial system . it is easy to understand the concentration of the radio - iodines by the thyroid in hyperthyroidism and in the rare cases of carcinoma of the thyroid , where the primary and sometimes also the metastases retain the function of secretion . 
one must be sceptical of the therapeutic possibilities in bone sarcoma of sr89 or ca45 ; it is interesting to note that stone ( 1946 ) reports that radio " strontium , barium , zirconium , yttrium and others locate quite selectively in the bones , and many of them stay for long periods of time . " radio - phosphorus , p32 , has been used since 1936 mainly in u.s.a. , in the treatment of patients with chronic myeloid and lymphatic leukaemia , polycythemia vera , lymphosarcoma and various related ( low - beer , lawrence and stone , 1942 ; reinhard , moore , bierbaum , kenney , 1942 ; lindgren ( 1944 ) showed thatp32 , which is selectively moore and kamen , 1946 )  . concentrated , gave better results than na24 , which is not selectively concentrated . the therapeutic possibilities and dosage of radio - phosphorus has been reviewed recently ( mitchell , 1947b )  . it is considered that the present position with regard to its therapeutic applications may be summarized as follows : diseases 1 . 
in the treatment of chronic myeloid and chronic lymphatic leukaemia , p32 is probably as satisfactory as , but no better than x - radiait is important to investigate the possibility of development of tion . methods of routine treatment of these diseases by means ofp32 . the average , each case is likely to require 10 to 15 millicuries ofp32 given , preferably intravenously , in the form of a solution of na2hpo4 in fractions in an over - all time of 10 - 12 weeks . it is desirable to correlate the dose with roentgen units ( marinelli , 1942 ) , and to measure the differential absorption ratio in different tissues ( kenney , marinelli and woodard , 1941 )  . 
phillips. * from the department of radiotherapeutics , university of cambridge . received for publication june 3 , 1952 . for the development of quantitative methods of study of mitotic inhibition by x - rays and chemical a ents , it has been necessary to examine the distribution of mitoseg in tissue cultures ' of chick fibroblasts . 
a statistical analysis of the distribution of , the mitoses has been made . previous quantitative work on tissue culture colonies in vitro has been reviewed by mayer ( 1939 )  . afitoses in fibroblast colonies were mapped by fischer and parker ( 1929 ) , by ' gairard ( 1935 ) , by jacoby ( 1937 ) , and in epithelial colonies by ephrussi and litvae ( 1934 )  . 
the colony had been grow - n for 24 hours in the usual ' mixture of one drop of fowl plasma and one drop of 15 per cent chick embryo extract ' then fixed in susa , stained with heidenhain 's haematoxyhn , and mounted whole . it was selected from a number of " control colonies of another experiment , asbeing of average growth and mitot - ic activity , and free from any obvious abnormahty . the colony was mapped using the 1 / 6 inch ( dry ) objective and an eye - piece micrometer which divided the field of view into 16 squares each of 901l side . 
the number of ceus in each square was counted , and at the same time a record was made of cers in mitosis , and of the phase of mitosis . 
4 by which the colony is divided into five arbitrary zones according to the cer density . the area of the uncounted central part is 22 per cent of the total area of the colony . 
the proportions of the phases of mitosis over the whole area are : prophase 17 per cent , metaphase 34 per cent , anaphase 7 per cent , telophase 42 per cent , and within the hmits of statistical variation they are the same in each of the five zones . in order to detect any departure from random distr ' lbution of mitoses within any one zone , the numbers of squares containing 0 , 1 , 2 , 3 , etc . 
mitoses were c ' ompared with the numbers expected on the poisson distribution , and were there was a suggestion found to agree within the limits of statistical significance . that the number of squares containing more than two mitoses wag shghtly greater than expected , but the total numbers were too small to establish that this was more than random variation . 
the total value of " chi squared " is 16 - 5 , which , for 7 degrees of freedom , gives a probabihty p this strongly suggests a factor other than chance causing non - uniform distribution . 
the number of mitoses per unit area can be seen in the map of his colony 27646 to be lower in the zone nearest the central part than the average value by at least a factor of 2 , which again is in marked contrast with the present work . the map published by jacoby ( 1937 ) can be compared as regards the relative number of mitoses per unit area in the different parts of the colony , and shows a similar trend to that found in the present work . it is interesting to note that the fairly constant level reached outside the central zone is maintained in jacoby 's colony across the central zone itsell if this was also the case in the present colony , there would have been about 120 mitoses in the central part which was not counted . willmer ( 1933 ) found that the frequency of mitosis was great - est in regions of moderate cell density , as is the case in the present colony . the distribution of cells and of mitoses in the outgrowth of a typical fibroblast colony is presented in the form of a map . 
the maximum mitotic index is in the region of moderate cell density , and the number of mitoses per unit area rises from the periphery to a steady value near the central part . 
the distribution of mitoses within the regions of constant average mitotic frequency agrees in general with a random distribution , which suggests that chance is the main factor controlling it . 
some of the authors misrepresent their own data , misquote those of others , are defective in arithmetic and make the task of anyone who wishes to examine their conclusions difficult . some authors , when giving data for the incidence of cancer other than uterine , do not say whether the figures refer to one or both sexes ; and in statistics based on admissions to a hospital they do not say whether this is a women 's hospital or a general hospital , or where the hospital is situated , data which are not always easy to obtain in another country . 
the age distribution of these 7 cases was as follows : 30 - 40 , 1 ; 40 - 50 , 2 ; 50 - 60 , 2 ; 60 - 70 , 2 . the seven cases of uterine cancer in jewesses which appear in table ii appear to be identical with those in table iii . * this is a very high percentage , for which theilhaber shows no detailed evidence . deaths of women from all forms of malignant disease deaths from malignant disease of the uterus the registrargeneral 's statistical review ( 1935 - 1939 ) gives the following figures for england and wales for the five years 1935 - 1939 :  . 
sanders ( 1916 ) gives data from rotterdam ( table x ) which show a low incidence of cancer of the uterus in jews , and a still lower incidence upon members of two of the protestant churches ( christian reformed and reformed )  . 
about one per thousand of the population . the radiumhemmet serves a well - defined area of the country which covers about half of the population . since 1914 practically all cases of cancer of the cervix occurring within that area are referred to the radiumhemmet for treatment . from 1914 to 1947 inclusive i have seen about 7000 cases of cervical cancer . among those were three jewish women . 
he considered that this was almost certainly an hereditary factor and not likely to be due to special observances of the jewish law , the same facts being noted in unorthodox jews . * unfortunately karplus gave no figures in support of this statement . 
data showing an equally low incidence of cancer of the uterus , which is more difficult to demonstrate than a high incidence , in populations known to consist of orthodox , and of unorthodox jews must have been difficult to obtain and would be of great interest . * i am indebted to d . 
100 table xi shows that cancer of the uterus , reckoned as a percentage of all cancers ( fishberg does not make clear whether the figures refer to females only ) is less than one - half as common among jewish women as among other races , while cancer of the breast shows a smaller difference in the same direction . smith ( 1941 ) studied the racial incidence of 3106 cases of cancer of the cervix observed at the memorial hospital , new york , from 1916 to 1937 . 
he says : " in an attempt to compare the nationality incidence in cervical cancer in this series with that of patients suffering from other gynecological lesions , consecutive records as filed have been studied , but the numbers used in each classification are not the entire number of patients filed under that diagnosis ; i.e. , this is a cross section of the clinic in the years studied rather than the total number of cases in the clinic . " i have been unable to learn from the memorial hospital the system upon which the cases making up this " cross section " were selected . apparently a number of cases of other gynaecological conditions roughly equal in number ( 3062 ) to those of cancer of the cervix ( 3106 ) were taken . 
the results are summarized by smith in tables xii and xiii ( his tables iv and iva )  . the significance of these figures is affected by the very high proportion of benign tumours , hence in table xiv and xiva smith 's figures have been recalculated for the malignant tumours only . in table xiv the result of the whole investigation , which for some reason smith does not give , namely , the ratio of cervix cancers to other conditions , is calculated from his figures . 
3106 6168 3062 vineberg ( 1919 ) gives data for the incidence of cancer of the cervix based upon material from 80 , 000 female patients at the mount sinai dispensary and hospital , table xv represents an attempt to reduce his rather confused statenew york . ment to a clearer forthe higher proportion of cancer in the hospital cases as against those of the dispensary is attributed to better conditions for examination . vineberg ( 1919 ) points out that jewesses of the poorer classes , to which most of those dealt with in his paper belong , are most likely to be orthodox in religious matters . 
the authors suggest the possibility that this difference certainly the age at which some forms of cancer depends upon racial factors . occur is affected by genetic differences ; examples have been given in detail in another paper ( kennaway and kennaway , 1944 )  . but there is nothing in these data for age distribution to indicate whether the liability to uterine cancer , which is the chief subject considered here , is affected by racial or by extrinsic factors . 
cancer of the uterus in hindu , moslem , parsee and indian christian women . statistics based upon attendance at hospitals are notoriously liable to error , more especially when they refer to people differing in race and religion . however , the following figures ( table xxi1 ) should at any rate encourage further investigation . 
they are taken from the valuable collection of data on cancer in india obtained by nath and grewal ( 1935 ) from the records of in - patients of 13 hospitals in punjab , delhi , united provinces , and bihar and orissa , comprising 6395 cases of cancer in all . 
cancer of the uterus in china . maxwell ( 1929 ) in his book " the diseases of china " says : " it is probable that uterine cancer ranks highest of all in the malignant growths in this country . 
the women are classified according to the husbands ' occupation into four main classes , with 14 numbered and 35 named sub - divisions . in table xxvii , only the four main classes are quoted . theilhaber does not state the populations of these various groups , and makes figures for the age distribution no comment upon this very serious deficiency . of the populations of these classes were not available . 
the object of the preliminary bath was not cleanliness per se , but the removal of anything which would intervene between the skin and the water during the total immersion , and thus deprive this ritual of its efficacy.t some medical writers have emphasized , in rather vague terms , the importance of the cleanliness enforced by the mosaic law , hence it is important to note exactly what the law requires . 
the washing , in a normal woman , at the beginning and end of the seven days , adds two baths a month to whatever other ablutions she may carry out . * this account of jewish ritual immersion is taken from various articles in the jewish encyclopedia ( 1891 ) , from ploss , bartels and bartels ( 1927 ) and from preuss ( 1923 )  . 
one might form some estimate in london from the number of public ritual baths available , which are said to be not more than half a dozen ; there are also some private ones . 
but it seems probable that many women who do not go to the ritual bath may conform to the law in other respects , namely , the first and second bath , and abstention from intercourse , which are matters of purely private conduct . the mosaic law ( leviticus xii , 2 , 5 ) relating to child - birth is important in view of the association of cancer of the cervix with parity . 
 " if a woman conceive seed , and bear a man child , then she shall be unclean seven days ; as in the days of the impurity of her sickness shall she be unclean . . 
but if she bear a maid child , then shall she be unclean two weeks as in her impurity : and she shall continue in the blood of her impurity three score and six days . " thus the whole period of impurity was either 7 + 33 = 40 , or 14 + 66 = 80 days . 
the practice in this country at the present time is said to be , to observe rather longer periods , of two and three months respectively . ( b ) moslem law . the koran ( sura 2 ) gives directions for the purification of women which are much less precise than those of the jewish law . 
a flow of blood lasting more than nine nights is the work of evil spirits . modi ( 1922 ) , a parsee , quotes these laws and says : " at present also , most of the parsee women generally observe the above practices . there are no separate dastanistans or houses for menses in parsee towns or streets , but generally a sequestered part of one 's own house is chosen for the purpose . the downfloor of the house was thought to be the proper place . 
but nowadays , in a crowded city like bombay , the down - floor , instead of being a quiet and healthy place such as that contemplated by the early injunctions of the vendidad , is so , most women in menses pass the period of generally quite the contrary . menstruation on their upper floors , but in an isolated way . 
in the matter of taking food , very few use spoons now , though up to about 25 years ago , that was generally the case . in the matter of purification , they observe the bath enjoined by the early books , but the vendidad injunction of bathing over the three " magas " is not observed at all . 
a separate place of bathing and for purposes of nature for women in this condition is generally provided in parsee houses . " ( d ) hindu ritual . khanolkar ( personal communication ) says that the parsee laws regarding menstruation are almost identical with those practised by orthodox hindus and probably both of them are derived from early aryan ritual . 
the abbe dubois ( beauchamp , 1906 ) , writing about the beginning of the nineteenth century , quotes from the book padma - purama , reputed to be the work of the hermit vasishta , a rule for a 3 - day p3riod of isolation for the menstruating woman , followed by a day of ceremonies and ablutions , including 36 total immersions in a river . 
during the three days "  . the mere wish to cohabit with her husband would be a serious sin . " elsewhere he says , " the mother of the newly - born child lives entirely apart for a whole month or more , during which time she may touch neither the vessels nor the furniture of the house , nor any clothes , and still less any person whatsoever . the time of her seclusion being over , she is immersed in a bath , or else a great quantity of water is poured over her head and body . women are similarly isolated during the time of their periodical uncleanness . in all decent houses there is a sort of small gynaeceum set apart for them ; but amongst the poor , in whose huts there is no such accommodation , the women are turned into the street , under a sort of shed or outhouse , or else they are allowed a corner of the cowshed . . 
when the time of uncleanness is passed , all the garments that the woman has worn are given to the washerwoman . her clothes are not allowed inside the house ; in fact , no one would even dare to look on them . " jhaveri ( 1910 ) says that in all hindu religious books minute directions for during the first four days of the first baths on very many occasions are given . menstrual period everything which the girl touches must be washed and " 202 e . 
nor do married women abstain procreation is almost a matter of religious observance with from child - bearing . uterine cancer ought to be , if anything , more the mass of jewesses . common among jewish women than among non - jewish . " various talmudic writers ( epstein , 1936 , 29b - 30a ) laid down that a father should cause his sons to marry at 16 to 24 , or 18 to 24 , and that a daughter should " be dowered , clothed and adorned , that men should eagerly desire her " ; no age is stated at which a woman should marry . 
a modern compiler ( abramowitz , 1900 ) states the law of israel on this matter thus : " after a man has arrived at the age of 18 it is his duty to take unto himself a wife in order that he may be fruitful and multiply , at any rate he should not pass his 20th year without having taken a wife . having begotten a son and a daughter who are also generative , one has fulfilled  . 
the command " to the commandment " to be fruitful and multiply . " be fruitful and multiply " is not obligatory upon women ; nevertheless a it is woman should not remain single lest she be liable to suspicion . one of the mandates of the sages that a man shall give his sons and daughters in marriage immediately they approach maturity . these jewish practices thus laid down in the law , and described by sorsby as prevailing at the present day , should encourage early marriage . the abb6 dubois ( beauchamp , 1906 ) says that "  . . 
thus 45 per cent of women with cancer of the cervix , and only 16 per cent of those with cancer of the breast , were married before that age . " variables which might be considered are : earlier childbirth , multiple children , poor obstetrical service , longer duration of married life , syphilis , immaturity of tissues at time of marriage , and excessive hormonal stimulation . " of these factors , longer married life could be eliminated by comparison with other groups . 
circumcision. some authors ( handley , 1936 , 1947 ) consider that no explanation of the lower incidence of cervical cancer upon jewesses need be sought beyond the ( assumed ) difference in the bacteriali flora of the female genital tract brought about by this factor , a matter which it would be possible to investigate . more data from moslem populations who practise circumcision , and from parsees , who do not , are obviously very desirable . handley ( 1936 ) has emphasized the value of statistics from fiji , where the natives practise circumcision , in contrast to the hindu immigrants , in whose native country phimosis and cancer of the penis are very common ( kennaway , 1947 ) ; certainly if these two races could receive equal medical attention interesting results might be obtained.t circumcision might act in another way , not dependent upon bacterial action . phimosis , cancer of the penis and cancer of the cervix appear to be common in * see " the racial origins of jewish types , " by radcliffe n . 
we have no data which give directly the respective social incidence of cancer of the cervix , and of the corpus , but information should be available from hospitals which have separate accommodation for paying and other patients . 
2. - age at death from oanoer of uterus in bamberg , augsburg , wuirzburg , erlangen , niirnberg and the provinoe of unterfranken , 1908 , and in munioh , 1906 - 7 - 8 ( theilhaber , 1910 )  . 
the jewish ritual has some unique features . more or less complete isolation of menstruating women is practised by many other peoples and is laid downi in the religious literature of some of these ( koran , zend - avesta , dharmasindhu )  . some quite primitive peoples ( aleuts ; natives of the congo and of australia ; for references see ploss , bartels and bartels ( 1927 ) ) are stated to enforce isolation at the menstrual period for as long as 6 to 7 days . 
one might make the following suggestions for further investigations : ( a ) an inquiry into the incidence of cancer of the cervix in jewish women who observe the 12 - day period , the ritual immersion being disregarded . 
all of the twenty collections of data which have been found in the literature show an incidence of uterine cancer which is greater on non - jewish than on jewish women . 
these data are calculated upon several different bases and hence are not all comparable . seven authors express the figures for cancer of the uterus as a percentage of all cancers in women , which percentage ranges from 28 to 14 in non - jews , and from 10 to 4 in jews , the mean values being 20 and 7 . 
the very scanty data available ( 25 cases only ) show a much lower incidence of cancer of the cervix on parsees . this might signify that so short a post - menstrual period does not affect the matter one way or the other , anid this difference in liability to cancer must then be due to other factors . 
cancer of the uterus appears to be prevalent in some peoples ( hindus , chinese ) among whom phimosis and cancer of the penis are also common , while the moslem women of india show a lower incidence . 
but any attribution of this difference to the practice of circumcision by moslems is very doubtful in view of the similar low incidence on peoples ( parsees , indian christians , possibly some dutch ) in whom this factor is absent . 
the only numerical data on the social incidence of cancer of the uterus appear to be those from bavaria 40 years ago , and from england and wales , after the last census , in 1930 - 32 . 
the unavoidable mixture , in large - scale statistics , of cancers of the cervix and of the corpus uteri , is unfortunate , as these two forms probably differ in etiology . 
harnett. published for the clinical cancer research committee of the british empire cancer campaign . received for publication july 16 , 1948 . in 1938 - 39 the clinical cancer research committee of the british empire cancer campaign carried out a clinical survey of all cases of cancer seen in the hospitals , both voluntary and l.c.c. 
in the administrative county of london . this was done by means of questionnaires , one of which was filled in by the registrars in the various hospitals for each patient and returned to the clinical cancer research committee for record . 
the work was interrupted by the outbreak of war after it had been in progress for 17 months . by this time 15 , 200 cases of cancer had been registered , of which 2529 ( 16 * 6 per cent ) were cancer of the breast . these patients have now been followed up for five years or more and the records analysed . 
a laparotomy was performed on each animal using ether anesthesia for rats and guinea - pigs and nembutal for mioe , and a loop of the intestine adjacent to the pylorus ligated . 
the abdominal cavity was closed with nylon sutures and each animal returned to its original cage . the animals were not treated further until 3 to 3hours following the laparotomy by which time all had emerged from the anesthesia . 
of body - weight of a 0.5 per cent aqueous solution of toluidine blue 0 . animals were anesthetized i an hour following the time of injection and a blood sample withdrawn either by heart puncture or from the aorta . 
the ph of the contents as well as of the gastric mucosa was obtained with hydrion the stomach contents were diluted 1 : 1 with acetone , stirred , and centripaper . fuged for 10 minutes at 2000 r.p.the supernatant was withdrawn and a 1 ml . aliquot diluted with acetone to 10 ml . this was stored at 50 to 100 c . 
overnight following which it was centrifuged 20 minutes at 2000 r.p.m. , and the supernatant removed for spectrophotometric analysis . in some rats the intestinal tract was removed and the contents collected . these as well as the blood samples were analyzed in the same manner as the stomach oontents . for the standard curve , 1 ml . 
an acetone blank was used for all determinations . in the case of gastric samples , the ph of the blank was adjusted to that of the sample using hc1 . the same acetone was used throughout the experiments and was redistilled prior to use . a beckman model du spectrophotometer was employed in making the measurements . 
inasmuch as the the guinea - pig , like the dog , is considered to be susceptible to histamine stimulation , an enhancement of gastric secretion following injection in this species was anticipated . the proportion of formed elements to plasma in the blood was determined for rats and guinea - pigs but not for mice in several of the groups . these results are listed in table i under hematocrit values . it will be observed that among the rats which received histamine ( groups i , ii , v , vi ) , an average value of 69 was obtained . 
whenthe ratswere not injected with histamine ( group iii ) , thehematoneither the ph of the stomach contents nor that of the crit value averaged 65 . gastrio glandular mucosa was altered significantly by the administration of histamine . in the rat a normal hematocrit value of 45 - 8 has been reported for males of the sprague - dawley strain ( gardner , 1947a )  . this value was confirmed in our laboratory . 
thus the histamine appeared to have no additional effect on the hemoconcentration observed in all operated animals . in untreated male guinea - pigs a hematocrit value of 42 has been reported ( gardner , 1947b )  . examination of the blood of treated guinea - pigs in our experiments disclosed a significantly higher hematocrit value in every animal . 
the control and 4 treated animals show no selective absorption in the region in question . similar analyses , using 5 guinea - pigs of group i and 1 guinea - pig corresponding to rat group ii , showed no definite peaks in the range between 375 and 400m , tt . although animals were fasted 48 hours prior to the start of operations no precautions were taken to prevent coprophagy , since it was our intention to duplicate the oonditions which prevailed in the experiments of ray and peters ( 1951 )  . when gastric contents were collected , it was observed that in addition to fluids although some of this may there also was present a varying amount of solids . have been due to residual food , it is more likely that ingestion of feces was responsible . 
18 - not included in any group - rat injected subcutaneously with histamine solution alone . solid lines represent animals given compound iii . analyses of blood from rats injected with compound iii revealed no compound by a method which was shown to detect 001 mg . 
on the other hand , the presence of toluidine blue o may be established by spectrophotometric analysis since intestinal contents give no peaks in the region of maximum absorption of this dye . it is of interest that such analysis from rats injected intraperitoneally with an aqueous solution of toluidine blue 0 failed to reveal this blue dye . ray and peters ( 1951 ) reported that gastric extracts from 3 out of 3 rats treated with compound iii showed substantial absorption at 400 mru . in the present experiments only 1 rat out of 15 showed similar results , while 2 fell in an intermediate , doubtful category . 
de. from the chittaranjan cancer ho8pital , calcutta , india . received for publication january 4 , 1954 . the study of the effect of radiation on cancer cells presents problems of fundamental importance . it is still an open question in the field of radiobiology as to whether the ionising effect of radiation directly induces differentiation in cancer cers . 
he has also shown that radiosensitive and radio - resistant cancer cells react to radiation in a different way after a preliminary radiation . waren and dixon ( 1949 ) are of opinion that radiation does not induce differentiation of cancer cers . johes and koher ( 1950 ) remark that the apparent increase of differentiating cers after radiation on cancer cers , is only relative and is caused by destruction of other types of cells . glucksmann 's method of estimating the radio - sensitivity of cancer cells with prehminary radiation ' has been criticised by gricouroff ( 1952 ) who is of the opinion that radio - sensitivity and differentiation of cancer cells are related to stromal nutrition . thus it is evident from the literature that our knowledge of the mode of action on radiation is not decisive . 
our study was strictly confined to those cancerous areas which were characterised by anisocytosis , anisonucleosis , abundance of mitotic cells , loss of polarity of epithehal cells and just breakage of basement membrane . 
the induction of differentiation in cancer cells is one of such delayed effects . it is for this reason , that we have collected tissues , as mentioned previously , on the 7th day after first radiation with 7000 r , on the 21st day after the second 7000 r radiation and finally 3 months after a total radiation of 21 , 000 r . before coming to our problem proper , we made a comparative study of the cellular population of the differentiating phases of the stratified squamous epithefia of the normal cervix and of epidermoid carcinoma of the cervix . table i shows that the cell population of the differentiating phase of the normal cervix is 48 - 17 0 - 41 per cent compared with 3 - 57 + 0 - 14 per cent of the epidermoid carcinoma of the cervix . we find the incidence of the variation of standard error in post - radiation conditions is high . might be due to variation on the biology of cancer cells , and also to altered conditions of different patients . 
de the trend of distribution shows also significant changes after second and third 7000 r , but the ' t ' test could not be applied because the number of cancer positive cases decreased materially after the 2nd and 3rd radiation . our second problem is concemed with the possibihty of predicting radiosensitivity of epidermoid cancer of cervix after preliminary radiation with 7000 r . it has been shown previously ( table ii ) that after the first radiation with 7000 r , there was a uniform reduction of cancer cell population of both resting and mitotic phases , and similarly a uniform increase of cell population of the differentiating and degenerating phases . 
we have not found any differential variation in the four biological phases of cancer cells after preliminary radiation to distinguish a radio - sensitive case from a radio - resistant one , as has been found by glucksmann ( 1948 )  . in our present series of 91 cases , no cancer cers were found in the final biopsy after 21 , 000 r in 76 cases , which may be considered as radio - sensitive cases . cancer cers were persistent in the remaining 15 cases under similar conditions and they may be termed radio - resistant cases . on further analysis of our data , arranging them into final cancer - positive and cancer - negative groups after full radiation with 21 , 000 r , we do not find any significant variation of cell population in different phases after the preliminary radiation with 7000 r ( table iv )  . 
when the influence of irradiation on the number of cells in the different classes was examined separately after the first irradiation for radio - resistant and radio - sensitive groups of tumours , no significant difference was found between the two groups . we express our gratitude to the atomic energy commission under the government of india for a grant which has given us an opportunity to do this work , and also to the chittaranjan cancer hospital , calcutta , for facilities to work in the laboratories . we also express our sincere thanks to the staff of the chittaranjan cancer hospital , particularly to n . 
 although urethane has been mentioned as carcinogenic for mouse ( nettleship and henshaw , 1943 ) and rat lung ( jaffe , 1947 ) this action has not yet been reported in other animals . 
since the inherited susceptibility to most known cancers is due to dominant genes this was anticipated here , and con sequently a large number of the c57 backcross mice were bred in order to note segregation , which should be manifest in the group on this assumption . 
preliminary experiments indicated that the various strains and crosses of mice used did not differ in their fluid intake , and consequently strain differences due to this treatment were not due to a different intake of the carcinogen . 
they were from another experiment and were only given 7 weeks ' urethane treatment , though they were killed 7 months from the beginning of treatment , the same as the rest . 
 when the mice were sacrificed their lungs were removed and fixed in 10 per cent formol - saline for 24 hours , which preserved the material and made handling easy . 
since nearly all lung tumours in mice tend to occur on the periphery of the lobes ( grady and stewart , 1940 ) the lobes were separated and the number of nodules on their surface visible to the naked eye were counted . 
in a previous paper ( cowen , 194 7 ) it was noted that strains of mice which gave a low number oflung tumours had tumours of a smaller size . 
 since the tumours in a lobe varied in size from microscopic dimensions to nodules about 4 m in diameter , it was not feasible to use the average size of all these tumours . 
the best way of gauging the response on a basis of tumour size was considered to be that of determining the size attained by the largest tumour in the total lungs of a mouse . 
this was tested statistically using the formula v ' ; ; ; 2 on the other hand , the fl hybrids were slightly but significantly lower than both of these classes . 
the polygon for the 057 backcross mice is obviously bimodal , and roughly consists of a combination of the figures for the 057 and fl hybrid mice in approximately equal proportions . 
 it may be mentioned that the a backcross mice which segregated for colour giving three phenotypes , albino , non - agouti and non - agouti brown , showed no apparent linkage of susceptibility with colour . 
 - ~ number of tumours f 3 . - - scatter diagram showing the relationship between the 2 groups of c57 backcross mice with respect to number and size of tumours . 
 thus , of all the chickens and guinea - pigs treated with urethane , only one chicken developed a neoplasm which was lymphoid in orig this type of tumour is not uncommon in chickens normally , and is not considered to be due to treatment with urethane . 
the first ( number of tumours ) gave more obvious results than the second ( size of the largest tumour per mouse ) , though both results closely paralleled each other . 
 these results point most significantly to the existence of a single dominant gene in a mice which is responsible for urethane - induced lung tumour suscepti bility , the c57 mice carrying the recessive . 
this does not entirely explain the results , for if a single dominant gene only were responsible , then a , fl , a back cross and the high group of the c57 backcross mice would all have exactly the same tumour incidence , which is not the case . 
firstly , the tumour susceptibility was genetically ina.ependent of mortality , and secondly , as the mortality was considerable only in the a and a backcross mice , a higher tumour susceptibility in the dead mice would merely have emphasized the line differences . 
 heston ( 1940 , 1942a , 1942b ) reported somewhat similar results using spon taneous and hydrocarbon - induced lung tumours in a and l mice ( high and low strains respectively )  . 
a possible reason for this is that the incidence of lung tumours in these mice was much lower than in the urethane - treated mice of the c57 backcross as reported here . 
 from the results of these workers , it appears that certain carcinogenic chemicals cause different lung tumour incidences in different strains of mice depending on the incidence of spontaneous lung tumours in these strains . 
that is , a strain of mice which develops few spontaneous lung tumours does not respond so well to a carcinogen as a strain which has a high spontaneous incidence . 
from this , it seems that environmental factors ( certain carcinogens ) do not simply cause tumours , but increase the incidence of them in mice depending on the inherited tendency of mice to develop the this argument can most probably be applied to other animals as well as mice . 
 it seems rather significant that no reports have been found in the literature of spontaneous ( or induced ) lung tumours in guinea - pigs , and out of the many neoplasms that arise in chickens , only one report exists of a spontaneous lung tumour in these animals ( apperly , 1935 )  . 
for example , guinea - pigs , which have a relatively frequent incidence of spontaneous liposarcomas ( warren and gates , 1941 ) , develop these tumours on treatment with hydrocarbons ( shimkin and mider , 1941 )  . 
it was considered that the resistance of mice to infections in general was lowered , and at the same time a specific carcinogenic virus was responsible for the lung tumours . 
if a single recessive gene is assumed to be the cause of the different mortalities , then the a backcross would be the segregating group , and should have a survival rate equal to the average of those for the a and c57 mice . 
from table i it is seen to be 45 , which agrees reasonably with the theoretical figure considering the small number of mice involved ( x2 = 317 , p > 005 )  . 
 it can thus be safely concluded that the mechanism whereby strain a mice are genetically susceptible to lung tumours is not the same as the one responsible for their susceptibility to general infections . 
correlation between leucopaenicity causing susceptibility to infection on one hand and a carcinogenic virus causing lung tumours on the other is therefore considered most unlikely in mice given urethane treatment . 
 two criteria which parallel each other closely are used as an index of response of mice to the carcinogenic action of urethane - the number of tumours per mouse and the size attained by the largest tumour in total lungs . 
of 9 : 10dimethyl - 1 : 2 - benzanthracene into the lungs of mice of strain street formed a part of a comprehensive study ( rask - nielsen , 1948 ) carried out in an endeavour to confirin or repudiate the hypothesis that tumours can be induced only in tissues that produce tumours spontaneously , whereas tissues that do not produce tumours spontaneously are unable to develop tumours even following very powerful carcinogenic action . the experiments showed that direct application of 0 - 5 mg . 
to this end , 3 : 4 - benzpyrene , 1 : 2 : 5 : 6 dibenzanthracene , or 20 - methylcholanthrene , all in doses of 0 5 mg . , were introduced directly into the lungs of street mice . since application of 9 : 10 - dimethyl - 1 : 2 - benzanthracene to the lung had previously induced thymic tumours ( rask - nielsen , 1948 ) , the present experiments were presumed to afford information also about the tumours which the three hydrocarbons would be capable of inducing in the thymus . these experiments will be reported in the present paper , which also includes the previous experiments with 9 : 10 - dimethyl - 1 : 2 - benzanthracene for comparison . benzpyrene , dibenzanthracene , or methylcholanthrene , 0 5 mg . , was injected , suspended in 0 01 c.c. 
the technique was as follows : in order to make the path of the needle in the lung tissue as long as possible , the needlewas inserted through the abdominal wall , immediately below the right costal border , and plunged through the diaphragm and longitudinally upwards through about two - thirds of the chest , before the suspension was injected . the mice used were litter mates of strain street , aged 5 to 7 weeks , divided into four lots . one lot was left untreated as controls , whereas the other three were injected with the respective hydrocarbons . 
as far as possible , the litters were divided equally in all four lots , an equal number of males and females in each in the corresponding experiments carried out with 9 : 10 - dimethyl - 1 : 2lot . benzanthracene ( rask - nielsen , 1948 ) litters of street mice were divided into lots of equal number , one of which was set aside as a control group . 
the effective total is the number of mice living to be as old as the youngest tumour - bearing mouse , namely , 12 months . in the sections prepared for the study of the spindle - cell sarcomas and thymic tumours , small adenomas were observed in a few mice . 
as shown in table ii , this phenomenon ' occurred following injection of dibenzanthracene in 4 out of 21 mice aged 5 - 7 months , following injection of methylcholanthrene in 2 out of 29 mice aged 6 and 7 months , and following injection of 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 1 out of 9 mice aged 5 months . these figures apply only to the adenomas , one , or at most two or three , in each mouse , observed in one section through the lungs . nothing is known about microscopically visible adenomas in the remaining part of the lungs '  . neither is it known whether a corresponding production of adenomas had taken place in the mice showing no grossly visible it is worth mentioning that untreated tumours , but it is considered probable . street mice do not usually exhibit microscopic adenomas . serial sections from 48 mice , ranging in age from four to twelve months ( rask - nielsen , 1948 ) , showed one adenoma , only microscopically visible , in a mouse aged 12 months . 
the present experiments , therefore , appear to indicate that 9 : 10 - dimethyl - 1 : 2 - benzanthracene , methylcholanthrene , and dibenzanthracene , and presumably also benzpyrene , have induced pulmonary adenomas . 
the explanation why these growths were in most cases visible only upon microscopic examination is probably afforded by the short survival time of the mice ( table i )  . although the experiments allow of but an estimate of the development of pulmonary adenoma , they appear to indicate that injection of dibenzanthracene has induced a more marked increase in the development of adenoma than did injection of benzpyrene , methylcholanthracene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene . the macroscopic adenomas as well as those visible only upon microscopic examination were of the ordinary , typical sub - pleural variety . in addition to the adenomas of the right lung , adenomas were also present in the left lung of a 7 - month - old mouse injected with dibenzanthracene and in the two 12 - month - old mice injected with 9 : 10 - dimethyl - 1 : 2 - benzanthracene . 
1rask - nielsen sarcomas of varying differentiation . associated with lymphosarcomatous thymic tumours . in two mice the spindle - cell sarcomas were table ii shows that spindle - cell sarcomas were observed following injection of benzpyrene in 2 out of 81 ( 2 - 5 per cent ) , following injection of dibenzanthracene in 14 out of 73 ( 19 per cent ) , and following injection of methylcholanthrene in 19 out of 59 mice ( 32 per cent ) , the effective total of experimental mice being the number of mice living to be as old as the youngest tumour - bearing mouse of all 4 groups , namely four months . 
the effective total of experimental mice was calculated on the basis of the number of mice living to be as old as the youngest mouse exhibiting a thymic tumour within all four groups , namely three months . with the exception of one spindle - cell sarcoma of the thymus , observed in a mouse injected with methylcholanthrene , all the growths were typical lymphosarcomas , made up of stem cells and accompanied by a frequently highly pronounced perivascular infiltration , particularly in the central areas of the lungs . 
one mouse injected with 9 : 10 - dimethyl - 1 : 2benzanthracene exhibited such violent infiltration without actual thymic tumour . the latent period of thymic tumours is given in table iii , which shows that the average latent period following injection of benzpyrene , dibenzanthracene , methylcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene was 20 , 16 , 10 and 16 weeks respectively . the experiments revealed that the carcinogenicity of the hydrocarbons used , in doses of 0 - 5 mg . 
none of the six cases of generalized leukaemia was affected with thymic tumour . on the whole , the experiments showed that the order of carcinogenicity of the four hydrocarbons , as estimated from the incidence of tumours induced , varied , when 0 5 mg . 
of the same four hydrocarbons ( rask - nielsen , 1950a ) which showed that the lung tissue of street mice was susceptible to this dose of dibenzanthracene , less so to this dose of 9 : 10 - dimethyl - 1 : 2 - benzanthracene , but failed to respond to benzpyrene and iiethylcholanthrene . these recent experiments also showed that the thymus was particularly susceptible to direct application of 0 - 02 mg . 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene and methylcholanthrene , less to the same dose of dibenzanthracene and least to the same dose of benzpyrene . the incidence of thymic tumours induced by the four hydrocarbons was therefore decreasing in the same order following injection of a small dose into the thymus ( rask - nielsen , 1950a ) and a large dose into the lung . the results cannot be compared with earlier experiments , since thymic tumours following a direct carcinogenic action on the lung or thymus have not been reported before , with the exception of a few instances of thymic lymuphosarcoma observed after injection of methylcholanthrene into the lung ( esmarch , 1940b )  . but such remote effect was not observed . it is evident that the carcinogenicity of 9 : 10 - dimethyl - 1 : 2 - benzanthracene for the interstitial connective tissue of the lungs differed from that of the other three hydrocarbons . 9 : 1 0 - dimethyl1 : 2 - benzanthracene proved to be non - carcinogenic for this tissue , whereas the carcinogenicity of the other three hydrocarbons increased in the same order as their carcinogenicity for the subcutaneous connective tissue following application of the same dose into this tissue ( rask - nielsen , 19501 ) , i.e. 
they take advantage of the spontaneous adhesion on plastic membranes of the free cells present in physiological fluids such as blood , cerebro - spinal fluid , peritoneal and pleural effusions . in brief : glass slides coated with formvar are placed in contact with the fluid ( with addition of heparin if necessary ) in an incubator at 37 ' c . 
for 15 to 60 minutes . the slides are then rinsed with tyrode solution at 37 ' , fixed 10 minutes to several hours in acid osmic vapour and washed thoroughly in distined water . the formvar is stripped from the slide , mounted on grids and anowed to dry at room temperature for at least 24 hours . photographs were taken with a triib - taiiber electron microscope at 60 kv . we adopted stringent criteria for purposes of comparison and considered only undamaged cells , that is to say cers having clear and well defined chondriosomes and with a satisfactory cytoplasmic transparency . 
as the appearance of a cell may vary from one area to another ( because of differences in spreading , lipid constituents , etc . ) we only considered the best portions . counts were made in each cell of osmiophihe bodies less than 150 mp . 
at least a few such bodies are to be found in every cell , but to consider them as true ultrachondrioma we adopted as a minimum 10 such particles 354 j . 
oberling showing a certain degree of polymorphism ( to distinguish them from merely lipidic granules ) per i oo #2  . for each preparation at least 1000 cells were counted . 
the same submicroscopic corpuscles as in leukocytes are encountered , but frequently they appear as bent or twisted filaments which may have swelhngs or a beaded structure . sometimes these filaments are extremely long . their thickness may vary from 30 mlt . 
they may aggregate in groups of two , three or more , or may appear to arise from an ordinary chondriocont . the statistical analysis shows that those submicroscopic bodies are not a ebaracteristic only of nialignant effusions but are seen in various inflammatory or circulatory disturbances . 
but when those figures are an almost constant finding , when it becomes impossible to estabhsh a distinction between chondrioconts and those structures on any other basis than the rather arbitrary one of size and thickness , then it seems difficult to deny the mitochondrial nature of the described structure . they have the same characteristics and the same polymorphism as certain types of mitochondria ( especially in plant cells )  . 
even the specifity of janus green stain depends on certain criteria ( showacre , 1953 )  . furthermore there is a question of principle involved in the discussion about the significance of these structures . if we require for the identification of ultramicroscopic structures the same characteristics as those used in classical cytology , ff certain mitochondria can no ion er be considered as such because their size prevents the use of janus green and the apphcation of more or less debatable functional tests , then we shau have two cytologies : orie optical and one electronit is highly improbable that cytoplasmic conical , which is not satisfactory . stituents are of a different nature simply because they are too smar to be seen with the ordinary microscope . on the contrary it should be our aim to show the links between microscopic and - ultramicroscopic structures . this has been done with great benefit with basophihc structures , ergastoplasm and intracytoplasmic network . it would be curious if the same did not hold true for the mitochondrial structures . furthermore the concept of mitochondria which are invisible witli the optical microscope is not new and it can account for certain results . many cytologists consider the chondrioma as fixed both in amount and morphology . 
but this stabihty is dependant upon the material studied , and it is in fact true of speciahzed tissues observed under standard conditions . botanists have long noted the morphological variations of the chondrioma in active cens ( guilhermond , 1934 ; gautheret , 1950 )  . no6l ( 1924 ) and many others bave made similar observations with animal cells . the researches of levi ( 1934 ) , lewis and 1 - jewis ( 1915 ) , etc . , seemed in favour of the de novo appearance of mitochondrioma in cells of tissue cultures . recently chevremont and frederic ( 1952 ) observing tissue culture cells during mitosis with the phase contrast - microscope , noted the transformation of chondrioconts into very minute rods and granules which resemble the structures described here . ' these formations sometimes disappeared and appeared again in daughter - cehs and then growing thicker and longer , reconstituted ordinary chondriosomes . the existence of the ultrachondrioma may well explain the apparent appear - ance de novo of mitochondrioma as a result of their regeneration from the ultra.chondrioma. it is not impossible that the absence of the ultrachondrioma in many cers may be more apparent than real -  . 
the degree to which ordinary mitochondriaare susceptible to variations of physicochemical conditions such as ph , osmotic afinor variations of conditions that are uncontrollable pressure , is well known . by present methods might cause a cavitation of the ultrachondrioma that would make it impossible to distinguish from the surrounding endoplasm . actually we never observed ultrachondrioma in cells where swelling of the ordinary chondrioma occurred . furthermore we sometimes found ultrachondrioma in the perinuclear region wben very favourable conditions permit observation in this area . but usually the thickness and high rpid content of this area in spread cens pre - ntent its study with the electron microscope . 
oberling there are two fields in which the existence of the ultrachondrioma raises special problems . in cytology , the presence of corpuscles resembling viruses in normal ( or presumably normal ) cells should be a warning against mistaken interpretations and will complicate the task of those workers who are engaged on the problem of the interaction of cell and virus . in biochemistry it introduces a new factor into the study of cytoplasmic it seems obvious that a large part of fractions isolated by ultracentrifugation . the ultrachondrioma will be deposited in the so - called microsomal fraction and would therefore lead the erroneous conclusions concerning the homogeneity of this fraction . the concept of the ultrachondrioma limited though it appears should entail a critical revision of some of the present data of cytology . we wish to thank madame dontcheff for the tissue cultures , and madame arnoult and martin for technical assistance . 
ungar. from the department of pathology , hadassah university hospital , jerusalem , israel . received for publication june 7 , 1949 . carcinoma of the duodenum has been observed in this laboratory at autopsy in three young siblings whose case reports form the subject of this paper . 
the examination revealed several histological aspects which may be regarded as representative of successive stages in the development of polyps . in the area of the prominence , the submucosa was widened and the muscularis mucosae showed a funnel - shaped protrusion in the direction of the intestinal lumen . 
the earlier history contained no fourteen months prior to admission he first began these occurred at irregular contributory information . to complain of bouts of cramp in the abdomen . intervals and were without clear localization . the patient was admitted to the hospital in june , 1939 , three months before his death . 
at admission his chief complaints were shortness of breath , attacks of tachycardia , lack of appetite and abdominal colic localized under the costal arch on either side . during the preceding year the patient had lost a great deal of weight . there were recurrent periods of diarrhoea . 
the duodenal mucosa choledochus as far as 1 cbehind the papilla of vater was without lesions . and pancreatic duct without abnormalities . beyond the papilla of vater , the lumen was considerably distended . there was a nearly circular , crateriform defect , which extended from the posterior wall , the lesion , which including almost the entire circumference of the duodenum . measured 7 to 8 cin diameter , showed a rugged floor ; it was entirely composed of tumour tissue and blended underneath with enlarged lymphatic glands of the peripancreatic group . 
the latter were glued together and had been sections through the floor of the ulceration completely replaced by tumour . revealed a firm and , in some places , a friable tissue which was of a pale greyishyellowish colour . 
the tumour was defined against the head of the pancreas by a thin layer of greyish - red connective tissue . the remaining portion of the duodenum was considerably distended and filled with greenish fluid . 
sections from the large ulcerated tumour revealed a carcinoma which grew in some areas in solid strands , while in others gland - like formations predominated . epithelia showed a considerable degree of pleomorphism and there were numerous typical and atypical mitotic figures . 
the main mass of the node was made up of glandular epithelium tissue with regular lumina which in places were slightly tortuous . was columnar with dark nuclei and oxyphilic cytoplasm . there was no pleomorphism or mitotic activity . 
an x - ray examination of the stomach and duodenum 2 months following the operation likewise failed to reveal pathologic changes . the three younger boys were kept under observation from birth by the infant welfare centres and the school hygiene departments of the hadassah medical organisation . 
nagel ( 1925 ) benign polyposis . duodenal polyp , polyposis recti et colon duodenum , jejunum , ileum duodenum , stomach , colon , duodenum , stomach , caerectum cum , colon adenomas in duodenum , multiple polyps in cae . cum , colon , rectum duodenum , jejunum , colon polyps in duodenum and jejunum duodenum , jejunum 9 . 
the disease is hereditary and affects patients since generalized polyposis is known to of all age groups , including the lowest . involve predominantly the large intestine , it is not infrequently mentioned in textbooks and articles under the name " polyposis or adenomatosis of the colon . " however , in rare cases , the disease was found to be prevalent in the small intestine . besides the instances mentioned in table iii , others of this variant have been described by lubarsch in 1888 ( dohring 1907 ) , schwytzer ( 1924 ) , roan ( 1932 ) , haggard and floyd ( 1935 ) , ravitch ( 1948 )  . some pathologists have taken the view that generalized polyposis is an entity which since it causes characteristic severe dysentery - like symptoms and malignant change in a high percentage of cases , should be separated from that represented by cases in which only few polyps are formed ( oberndoerfer , 1929 ; lockhart - mummery , 1934 ; hullsiek , 1928 )  . 
the designation of all three of our cases as generalized polyposis therefore seems to be justified . the observations reported in this article are relevant to the understanding of factors which govern the manifestation of malignancy in intestinal polyposis . several authors have assumed a casual relationship between the appearance of polyps and carcinoma in any given case . 
gunz. * from the department of radiotherapeutics , university of cambridqe . received for publication june 11 , 1949 . in previous publications ( gunz , 1948a ; b ) a technique of cultivating human leukaemic leucocytes in vitro was described , and the quantitative and cytological findings in untreated cultures made by it were analysed . 
the mice which survived to tumour age , though not themselves used for experiment , were not certainly representative of the whole colony and , owing to the concentration of tumours in famihes , the inclusion or omission of a single litter could greatly alter the tumour incidence calculated on the small nurabers available . 
the " effective total " ' is the number of mice which surv - ived to the age at which the earfiest tumour was detected in any of the groups , namely i 10 days in an f4 mouse of strain br4 ( blue label )  . 
many of the mice recorded as dead without tumour succumbed to epidemic infection about a year after the beginning of the experiment . tables 1 - 111 show that the incidence of tumours in the strains br4 ( pink label ) , br4 ( blue label ) , and br6 was unequivocally " high . " the three strains were substantially alike . 
tumours developed , indiscriminately as it seemed , in 11 wild , " 11 white , " and " black " mice in the f . - f4generations and continue to develop in " white " and " black " sublines up to the f6 generation . 
the later age - incidence of tumours in the f2 females was probably attributable to the breeding history ; the f2 females , in contrast with later generations , were not subjected to forced breeding . the incidence of tumours in the br16 strain ( table iv ) so far is extremely low . 
the great majority of the mice survive and more tumours may yet develop , but the average age is already higher than th ' e average age of tumour development in the other three strains . 
tumours were ground in - a mortar with sand and saline to make suspensions which ranged in strength , in different experiments , from 13 to 20 per cent w / v . 
the debris was removed by spinning in an ordinary centrifuge , and the supematant fluid was injected , at weekly intervals , into the dorsal subcutaneous tissues , each dose being 1 - 0 c.c. sixteen mice reeeived each 4 injections of extracts of bri tumours of the first or third transplanted generations , five received 3 injections and two received 2 injections . twelve mice received each i injection of an extract of a primary spontaneous c3h tumour and 3 injections of primary spontaneous r3 tumours , and seven mice received 3 injections of the r3 extracts only . all the extracts were similarly prepared . the females were caged with males and subjected to forced breeding , litters being removed within 48 hours ( usually within 24 hours ) of birth . table v summarizes the results at 89 weeks from the beginning of the experiment . 
the " effective totals " comprise the mice which survived to the age when the first tumour was detected ( 180 days in a mouse injected with bri extract )  . 
the average number of tumours per mouse was 2 - 5 , 24 mice having from 2 to 6 t aours each . aour was 25 weeks ; the earhest the average age at the first detection of a t tumour wa - s recorded at the age of 17 weeks , and the latest at 54 weeks . the 3 mice without tumours are alive at ages of 81 , 81 and 85 weeks respecit is noteworthy that although continuously with males they have had tively . no litters for about a year ; previoxwly litters were not recorded . 
no observations were made on virgin mice . incidence of tumours in ( c57 black ? x agew - free r3 ct ) f ] l hybri& . remale mice taken at random from the laboratorystock of c57 black were mated with males : firom a colony of r3 mice free from milk agent . i am indebted for the male mice to my coreague b . 
the f , , hybrids were subjected to forced breeding throughout their reproductive lives . one hundred female hybrids were reared ; 21 died without tumours at an average age of 21 weeks and 79 are alive at an average age of 57 weeks . 
the diversity of genetic constitution in the f2 and subsequent generations did not noticeably affect the incidence of tumours which developed indiscriminately in " black , " " white " and " wild " mice 4 ' white " and " w - fld " subhnes estabhshed by and in each of the " black , ly 31 selective breeding . 
the patemal contribution was not probably genetic for , as shown in this paper and in previous reports from this laboratory ( dmochowski , 1944 , 1945 ) , the c57 black x a hybrids developed tumours abundantly when tumour agent was supphed to them artificiafly . 
the uncompleted observ - ations on hybrids having fathers belonging to a subline of r3 mice deprived of tumour agent accorded with similar observations bv anderv - ont and dinnn ( 1948a , b , c ) in showing a substantial reduction in the incidence of tumours comparison with similar hybrids whose fathers derived from a line carrying the tumour agent . 
the experiment was open to the criticism , which anderv - ont and dunn apphed to their ow - n experiment , that the agent - fiee and agentbearing malet ; were separated by several generations of inbreeding and possibly differed geneticary . 
tumour agent was not demonstrable in the hybrids or in their tumours , and the offspring of tumour - bearing mice , whether obtained by back - crossing or by brother - sister matings , rarely developed tumours . 
two litters of - ( c x c3h ) f , were exceptional in that tumours developed in sisters at unusually early ages ( 4 - 10 months )  . the backcross offspring of two tumour - bearing females of one litter all developed tumours at average ages of 7 and 9 months respectively . 
the progeny of two tumour - bearing ( c57 black y x r3 ct ) - p . , females had a high incidence of mammary tuinours ( about 70 per cent ) through at least 5 generations . 
5 ( peacock , 1946 )  . since our last publication on this subject we have successfully propagated three new induced sarcomata , grch 16 , 17 and 18 . these three tumours occurred in the course of attempts to induce epithelial tumours by injecting into adult white leghorn fowls a mixture of tissues from 10 to 14 - day chick embryos of the same flock , with methylcholanthrene and sudan iv dissolved in olive oil , following the technique used by rous and smith ( 1945 ) for inducing epithelial tumours in mammalian embryo tissues . 
we used a variety of embryonic epithelia , but the only tumours that resulted from these procedures were spindle cell sarcomata of precisely the same familiar pattern as when the carcinogens were inoculated directly into the adult breast muscles . 
they are made up of fleshy spindle cells arranged in whorls and interlacing bundles , the individual cells being elongated , sometimes with branched ends , with finely granular acidophil cytoplasm , and with an oval nucleus containing generally one small sometimes the cells are multinucleate , in which case the nuclei are nucleolus . in line one behind another , never in the form of giant cells of the foreign body mitoses occur very frequently , and are often somewhat irregular with type . bridging and incomplete separation of the chromosomes ; but many apparently occasionally longitudinal fibrillation of the normal mitoses are also to be seen . cytoplasm can be made out , but cross - striation has never been observed in metastases in viscera free from striated muscle such as the liver . 
48 : ( a ) liver and ( b ) squamous epithelium from the crop of a 10 - dayold chick embryo were mixed with 1 per cent methylcholanthrene dissolved in a saturated solution of sudan iv in olive oil . 
3086 was killed in moribund condition . there was an oval tumour 5 cin greatest diameter in the left pectoral muscles . there was no tumour in the right pectoral muscles , and no residual fluorescence was detected at either site of injection . there was a chronic plastic peritonitis , probably from a healed perforation of the gut , which was bound down with adhesions . the gall bladder was greatly distended . 
of fresh tumour was ground smooth in a sterile mortar , and 10 ml . of 5 per cent dextrose saline were added and well stirred to give a turbid cell suspension . ten 6 - week - old white leghorn chicks were inoculated with doses of 0 - 2 ml . to 1 * 0 ml . 
a 1 in 10 fresh cell suspension in 5 per cent dextrose saline was injected into the breast muscles of 6 white leghorns , 9 to 12 months old , in 2 of which tumours were palpable in about 4 weeks . subsequently the tumour was maintained through 3 serial passages , by cell suspension inoculation . 
the lowest 1 cwas cut off and discarded , and the remainder of the paper was laid on a sterile agar plate and flooded with melted agar at 460 c . 
prodigiosus was present only in the lower 3 cm . all levels of wet paper , however , were infective in the case of of the wet strip . the mh2 tumour , but in the case of the grch 16 tumour no level above the meniscus of the tumour extract was infective . as in the case of ea ' rlier chemically induced sarcomata in which the test was made by similar technique , using paper at levels above the first centimetre from the free fluid , grch 16 and 17 homogenates yielded only negative results . this observation is completely in keeping with the results of the more conventional filtrations through gradacol membranes or seitz clarifying pads . 
on the other hand , the tumour itself might be supposed to contain such an agent , which for some reason or other was adsorbed strongly by the filter . in the case of paper chromatography the whole paper can be injected either intact or homogenised in saline , and this might be thought to favour the demonstration of viruses where filtrates yield negative results . 
as there are many variable factors in such exposures , it is convenient to express dosage as time related to sterilising effect on bacteria . under our conditions suspensions of b . 
for 5 to 10 minutes were exposed in plastic tubes to a focused beam of ultrasonic waves with a frequency of one megacycle per second transmitted through a cooling water bath . 
the plastic tube was transparent to the waves , and was so placed that maximum disturbance occurred in the centre of the tube . in order to concentrate the effect of the waves as much as possible 2 to 5 ml . of 1 / 10 homogenate of fresh tumour in normal saline were used . 
1 in the resulting proliferative reaction tissue . we have previously reported the localisation of virus - induced fowl sarcomata at remote sites of x - ray or radium burns ( peacock , 1946 )  . cauterisation with a red hot platinum wire or with fuming nitric acid applied to the skin with a glass rod ( 2 to 3 mdiameter ) has more recently been found to localise the virus in birds bearing rous sarcoma no . 
a sterile cotton thread was inserted in the left pectoral muscles of each chick and also ( a ) in 5 the left wing was injected with 0 - 1 ml . 
50 : ( a ) four out of 5 chicks had tumours in the right breast but no ( b ) all 5 chicks had tumours in the right breast . 
50 : the 9 chicks with large tumours at the site of rous sarcoma three chicks out of 6 had localisation at site of cautery , inoculation were killed . and 1 of them had localisation at site of control thread . none of the remaining 3 tumour - bearing chicks had localisation either at the site of sudan iv injection or at the site of the control thread . 
on the other hand , occasionally local inflammatory reaction occurs around the metal wing tabs used for numbering the birds , and we have seen 2 cases of localisation of rous sarcoma no . 
1 , and had 1 feather plucked from the leading edge of the wing on the day of injection and on the 4th , 6th , 13th and 15th days thereafter . 
no localisation occurred at the sites of trauma . it was thought that histamine - like action following cautery might cause local blood stasis and so favour the metastatic growth of blood - borne emboli from the tumour histamine was therefore injected into the left wing web at the damaged site . of 6 white leghorn chicks 4 weeks old bearing rous sarcoma no . 
50 : a large tumour was present in the right breast and the bird was there was direct spread from the grch 17 tumour injection site to the killed . liver , but no tumour at the site of rous no . 
3312 , 3316 and 3317 , which had not grown tumours at the site of injection of the seitz filtrate ( see above )  . typical grch 17 sarcoma grew in no . 
on the other hand , no such localisation has been observed in the case of the grch series of tumours . it seemed that the electron microscope , which can undoubtedly reveal particles of the size of viruses , might afford conclusive evidence of their presence or absence in our limited experience of this technique , however , there are in tumour cells . even less differences to be seen between infective and non - infective tumours and even normal tissues and in homogenates and filtrates prepared from them than can be seen by ordinary visual microscopy or even by direct visual observafurther work may overcome this initial difficulty of recognising viruses tion . from normal cell constituents ; but in the meantime circumstantial evidence points to essential differences between certain induced and spontaneous tumours . the occasional occurrence of a chemically - induced tumour which on propagation yields a virus does not in our opinion justify the assumption that all indeed , the existence of spontaneous filterable tumours contain such viruses . tumours would suggest that ultimately one is likely to encounter such agents in duran - reynals ( 1952 ) has recently suggested , birds injected with carcinogens . however , that viruses not usually associated with tumours may become adapted to cells conditioned by chemical carcinogens , and so play a part in the aetiology of cancer . 
our failure to induce any epidermoid cancers in the skin of fowls after repeated painting with chemical carcinogens may be due , as he suggests , to the absence of fowl pox in our flock ; but we have had no difficulty in inducing upwards of 60 sarcomata at the sites of injection of chemical carcinogens , and have seen a few carcinomata of the crop following exposure to 2 - acetylaminofluorene ( peacock and peacock , 1949 )  . 
though we failed in attempts to transmit the carcinomata and therefore cannot assess their possible viral content , we saw no inclusions of the kind described and illustrated by duran - reynals ( 1952 ) in his fowl pox methylcholanthrene carcinomata . the study of a wider range of chemically - induced fowl tumours , preferably including carcinomata of recognisable patterns , seems to offer the best prospects for obtaining more information about the aetiological factors concerned . 
1 , mill hill 2 endothelioma and the grch 16 , 17 , 18 sarcomata show that the two former tumours are readily transmissible by filtrates and by other extracts in which cells are probably destroyed or excluded , whereas the grch tumours are only transmissible by extracts containing cells . at the time of writing the authors were unaware that loewenthal ( 1931 ) had used capillary ascent on strips of filter paper of extracts of rous sarcoma no . 
w.3. received for publication july 16 , 1949 . in an investigation of the body growthand tumour growth - inhibiting action of carcinogenic substances , it was found that the nature of the inhibition is profoundly influenced by the protein content of the diet ( elson and warren , 1947 ; elson and haddow , 1947 ; elson , 1949 )  . in rats maintained on a 20 per cent protein diet injection of the carcinogen usually has little immediate effect on body growth although a delayed action , resulting in rapid loss of weight followed by death , may occur later . 
carcinogenic hydrocarbon 1 : 2 : 5 : 6 - dibenzanthracene 24 hours after implantation of walker carcinoma 256 in rats maintained on a 20 per cent protein diet results in very little difference in size and weight of the tumours from those of controls . if , however , the animals are fed a 5 per cent protein diet the tumours of those similarly treated with dibenzanthracene were found to be only one - quarter the weight of those of controls when the rats were killed 13 days after implantation ( elson and haddow , 1947 )  . 
lamerton for the studies involving the localized irradiation of the tumour , it was necessary first to develop .a method whereby the rat could be held firmly in anaesthesia reasonable comfort and the tumour alone irradiated with precision . was contra - indicated , since it may affect the response of the animal to radiation . the device eventually developed is shown in fig . 
a length of transparent plastic " cloth " is held by means of two clamping bars on an aluminium base . the rat is placed under the plastic material , which is then stretched under the clamping bars . 
the edge of the plastic cloth near the rat 's head must be reinforced with a strip of cellophane one to two inches wide , which serves to hold fig . 
1. - photograph of rat in holder designed for x - ray treatment of tumour . the rat 's head down and prevents him biting his way out . the tumour itself projects through a hole in the plastic material , and can be treated by crossfire techniques without irradiation of the rest of the body . a victor kx1o plant was used , run at 140 kvp . 
lamerton direct irradiation of e8tablished tumours . for these experiments the tumours were allowed to grow untreated for 6 days after implantation . daily estimates of the size of the tumour were then made by - measurement with calipers along two axes at right angles . 
2. from the results obtained with more than 20 control animals there appeared to be no very marked difference in rate of growth of the tumour in animals maintained either on 5 per cent or on 20 per cent protein diets . 
the group maintained on the 5 per cent protein diet , however , showed considerable inhibition of tumour growth , and the tumours after the first 7 days of treatment ceased to grow and remained fairly constant in size for a considerable time . 
3. - growth of walker rat carcinoma 256 treated with x - radiation ; 250 r per day , total dose 4000 r . * rats fed on 20 per cent protein diet . rats fed on 5 per cent protein diet . gradually developed areas of necrosis , which usually become infected , and in some cases the tumour had resumed growth shortly before the death of the animal . 
lamerton for the first four days after treatment the tumours of the 5 animals comprising the 20 per cent protein diet group grew more rapidly than those of the 5 per cent protein group , and reached an average size of about one and a half times that of the low protein group . after this period the tumours of the 20 per cent protein diet animals began to decrease in size , and eventually two of them regressed completely by a " shelling - out " process and a third remained very small over a long period . 
the other two , after a considerable period of regression , eventually grew again rapidly and the animals died of the tumour about 45 days after implantation . in the 5 per cent protein group one tumour regressed completely but the others grew fairly steadily at a much reduced rate for a considerable period , eventually resuming a more rapid growth rate before the death of the animal , which occurred on the average 36 days after implantation . died 2400 s 2000 3 1600 z 1200 en 800 perioi fig . 
no cures were obtained in animals of either group . it appeared therefore that regular control of the established walker tumour could not be effected by a daily dose of 400 r , and in the next experiment the effect of a daily dose of 600 r was studied , together with the effect of changing the diet of the low protein group of animals to the high protein content at the completion of the course of radiation . x - radiation , 600 r per treatment ( total 4000 r )  . in these experiments a dose of 600 r was given daily on six days , the seventh dose being reduced to 400 r to maintain the total dose at 4000 r . in the first experiment the animals of the 20 per cent protein diet group responded well at first , and nearly all the tumours began to decrease in size after the fourth dose of radiation . although the tumours then remained small for a considerable time no complete regressions occurred , and all eventually grew again fairly rapidly , leading to the death of the animals . the tumours of the animals maintained on the 5 per cent protein diet again at first responded to the treatment by growing rather more - slowly than those of the 20 per cent protein group . 
the day following the last radiation treatment the 5 per cent protein group animals were changed over to the 20 per cent protein diet and maintained thereafter on this high protein diet . 
5. - growth of walker rat carcinoma 256 treated with x - radiation ; extended treatment with initial high dose ( 1000 r ) ; total dose 4000 r . . 
under these conditions therefore the large initial dose of radiation appears to have such a strong inhibiting effect on the tumours that a marked difference is no longer observed between the initial response of low and high protein diet animals . 
the greatest degree of tumour inhibition was obtained when the animals were maintained on a low protein diet . it has now been shown that the response of rats implanted with walker carcinoma 256 to whole body x - radiation under conditions approaching those of the " walker tumour test " is also greater in those animals maintained on the low protein diet . 
with x - ray treatment , however , it is possible to apply direct to the tumour a sufficiently large dose of radiation to bring about an adequate initial growth - inhibitory response , even in animals maintained on a high protein diet , so that the subsequent outcome of the treatment then depends almost entirely on process ( b ) , and a favourable result is thus to a very large extent dependent on a high protein content of the diet . though the results obtained may be related to some extent to the particular characteristics of the tumour used , it is very interesting to note how closely the two processes distinguished in the radiation response of the tumour follow the concepts of " intra - cellular response " and " inter - cellular response " put forward by koller and smithers ( 1946 ) from studies in clinical radiotherapy . . 
tumour regression as the result of koller and smithers suggest that "  . irradiation is initiated by an intra - cellular response , but is carried on by an inter - cellular response which follows and plays an important part in the success of any treatment . 
the inter - cellular reaction is manifested through the repair processes , and depends on the construction of the tumour tissue as a whole . this reaction is conditioned and influenced by the intra - cellular response ; in this sense it is an indirect effect of radiation it seems likely that this " inter - cellular " response may constitute an important part of what we have described as process ( b ) , and have shown to be favourably if the " inter - cellular response " is related to influenced by a high protein diet . the repair processes , then it is very reasonable to suppose that nutritional factors can affect the elimination of the tumour in radiation treatment , and indeed proteins would be of special importance in view of their known value in the healing of burns and wounds . clearly the present work can only be regarded as a preliminary study . 
lamerton implantation , inhibition of tumour growth was greatest in those animals maintained on the low protein diet , but no complete regressions of the tumour were obtained . with localized irradiation of the tumour , when the total dose of 4000 r was applied in larger daily doses , complete regression of some tumours was observed , and the most favourable results were obtained by application of an initial dose of 1000 r with extended time intervals between successive smaller doses . 
complete regression of the tumours was then obtained in about 90 per cent of the animals maintained on the high protein diet , but in only about 15 per cent of these maintained on the low protein diet . it is suggested that two effects are concerned in the response of tumours to radiation , ( a ) the initial inhibition of tumour growth , ( b ) the elimination of process ( a ) is favoured by a low the inhibited tumour and cure of the animal . protein diet , and process ( b ) by a high protein diet . we would like to express our appreciation of the interest taken in this work and the encouragement given by professor a . 
we also wish to express our thanks for grants supporting this investigation from the british empire cancer - campaign , the anna fuller fund , the jane coffin childs memorial fund for medical research and the u.s. 
the hvbrid females of each litter , when four to six weeks of age . were mark - ed indi - vidually and di ' %ided into experimental and control n - lice . 
the largest part has been obtained from the rikshospital , which receives patients from approximately one - sixth of the material has been placed at the whole country . ' cal depaxtment iii and by proniy disposal by professor c . 
a few cases onl come from - other hospitals . in addition to the two clinical , two post - mortem series have been used in this analysis , namely , t6 material of jacobsen ( 1953 ) from wo city hos itals , covering the years 1937 to 1946 , and the material of christiansen ( 1953 ) from the rikshospital , covering the years 1925 to 1952 / 1 . all the tumours of these post - mortem materials have been typed by kreyberg with no knowledge ofthe clinical data . 
figures of each series are comparatively small , but a few feature - s seem to be significant , and possibly important . the main differences between the chnical and the post - mortem series are ( 1 ) the relatively much higher number of adenocareinomas , 30 per cent of an cases in the latter against less than 10 per cent in the former , and ( 2 ) the lower number of squamous cell carcinomas in the post mortem series . 
a study of the two papers dealing with the post - mortem series reveals a greater number of old persona i these materials , as compared to the clinical group . 
the significance of these differences will be discussed later . in kreyberg 's ( 1952 ) first paper a comparison was made between the occurrence of the different histological types in the norwegian material and a sipailar recent material from the mayo clinic . 
kreyberg mainly as a result of differences in criteria for typing . in the present table 1 , three series from foot ( 1952 ) have been included in order to stress this point . 
the distribution of histological types in this american material is remarkably similar to the norwegian clinical series , with one exception , the group adenomas and salivary gland tumours . these tumours occur more than ten times as frequeiltly in all the norwegian series . 
the cause of the relatively greater number of these suffice it to mention at this tumours may be manifold and will be discussed later . point that even in america certain investigators have found these tumours ratheifrequently . in table ii is presented the distribution of the different histological types as regards age and sex . 
t. uncertain group ii : 17 in table iii the findings regarding the sex distribution have been summarized . it will be seen that the different histological types in this chnical material form two main groups with markedly different sex ratio . 
the fact that the tumour material has been collected during the years 1948 to 1953 , while the population figures refer females 3 4567891 4 5 67 891 i1 1 3 456789 figa . 
1. - age distribution at the time of diagnosis of all lung tumours ( l ) and the mortality figures for stomach carcinomas ( v ) in males and females separately . 
1 curves have been drawn on double logarithmic paper , representing the whole material of the clinical series for males and females separately . for comparison one other curve for each sex has been drawn , namely , the corresponding curves for stomach carcinomas , based upon the mortality figures for norway , 1950 . 
2 two curves have been plotted in the traditional manner , namely , the curves for the relative age frequency of squamous cell carcinomas and for large cell lo~ ~ ~ fig . 
the figures are given in table iv the two curves are nearly identical and they indicate that the group i tumours biologically actually represent a uniform group , in spite of unquestionable histoit will further be seen that these group i tumours mainly are logical differences . responsible for the characteristic features of the lung " cancer " curve in general . the other lung tumour types have been examined in a similar manner . 
the adenocarcinomas and the sub - group lung adenomas and salivary gland tumours are , however , comparatively few in number in each of all the series , and accordingly subject to considerable chance fluctuations . in table v the figures for these tumours in all the three norwegian materials the basic figures are given for each material separately . 
the unusual fall in the higher age groups is taken to indicate a new carcinogenic situation in development , and the future stages are forecast by the direction of the curve for the age groups 30 - 39 and 50 - 59 . the adenocarcinomas , according to our diagnostic criteria : malignant tumours coniposed of more or less atypical , secreting or non - secreting , columnar cefls , with their nearly equal sex distribution and their increasing frequency with the advancing age , indicate that they are caused bv comparatively weak carcinogenic agents , well established in the society , and acting with equal strength in both sexes , at least in large parts of the country . the small group of bronchiolar cell carcinomas occur in all age groups and with no definite sex preference . 
they may be caused by unknown agents , hitting at random . the histological pictures , the equal sex incidence , as well as the appearance with no preference for any age group , together indicate that lung adenomas , benign and malignant , and sahvary gland tumours are caused by accidental factors , presumably of developmental origin . at this stage a few more words about the latter tumours may be justified . 
some surprise has been voiced as to the considerable number of adenomas and sahvary gland tumours in norwegian materials . firstly , a survey of the lung tumour problem i : ft general in norway shows that the total number of lung tumours is very moderate , as compared to the figures for england and wales , the netherlands , the united states , and even denmark . if , as assumed and actually found , the recent increase in norway is caused mainly by the ever larger number of group i tumours , it follows that the other histological this development has been types must show a proportionate decrease in number . observed in the ordinary columnar cer carcinomas . 
a decrease in the number of lung adenomas and sahvary gland tumours in relation to the sum total is predicted , but it may for a while be less marked in chnical and especiary surgical materials , because these tumours represent comparatively favourable clinical cases and are therefore selected . secondly , the tumours in question are , actually , observed in considerable numbers also in other materials . fried ( 1948 ) in the massachusetts general hospital found 17 adenomas out of 175 cases of bronchogenic neoplasms , and carlens ( 1952 ) reported 8 - 10 per cent in a swedish material . tbirdly , these tumours are most probably present in many other materials without beino , recognized as such . true columnar cen careindmas and group i tumours very rarely occur before the age of 35 years . in most 1 - ung cancer statistics some tumours are registered in younger and verv young persons . 
some of them have been diagnosed as adenocareinomas , others as sman cer carcinomas , especially if unfavourable preparations have been the base for diagnosis , or if the tumours are infiltrating . 
any academic discussion as to the propriety of the designation cc mahgnant adenoma " ought to be silenced by the very important fact , that if the proper criteria are observed and the material typed without clinical information , a grou ' of tumours will emerge , wit - h a sex ratio 1 : 1 , with no accumulation in anv a - ae aro - ud . 
each histological type has been analysed , especiany as to distribution according to age and sex , and the findings correlated to our additional present knowledge regarding the development of these tumours . 
they do very seldom occur before the age of 35 years and they present a very characteristic and , for human carcinomas , singular age distribution . this age curve as wer as the vital statistical evidence indicate that the main part of these tumours are caused by a recently estabhshed carcinogenic situation in certain ' parts of the world , notably the united states of america and westem europe . columnar cell adenocarcinomas appear with httle sex difference and they show a steadily increasing ffequ - ency with advancing age , a development in conformity these tumours are probably caused by with a great many human carcinomas . comparatively weak carcinogenic influences , evenly distributed over large areas , well established in the society and striking both sexes with equal force . bronchiolar cell carcinomas occur with equal frequency in both sexes and strike individuals in ar ages . 
hewitt. from the john burford carlill laboratories , westminster hospital , london . received for publication may 26 , 1953 . from the fact that certain mouse tumours could be transplanted using freezedried tumour tissue , gye , begg , mann and craigie ( 1949 ) concluded that they had evidence of virus transmission of their tumours . subsequently , it was shown ( passey , dmochowski , lasnitzki and milard , 1950 ) that a small proportion of the cells in these tumours were able to withstand freeze - drying as indicated by the proliferation in vitro of tumour tissue so treated . these findings focused attention on the quantitative aspects of tumour transplantation , and various observations were made which suggested that the malignant cell population in sarcomacraigie , lind , hayward and begg , ( 1951 ) tous ascitic fluids is heterogeneous . reported that a small proportion of the sarcoma cells in certain ascites tumours could be distinguished from the modal cells by their peculiar appearance under phase - contrast microscopy , and by their relative resistance to freezing and to the inimical effects of exposure to isotonic glucose . lasnitzki ( 1952 ) showed that a high proportion of the cells of sarcoma 37 ( hereafter referred to as " s37 " ) ascitic fluid undergo morphological transformation in tissue - culture and do not subsequently divide ; she found that this change was accompanied by a reduction in the power of the cells to give rise to a tumour on transplantation , and considered her observations to be evidence of bimorphism of the s37 cells . histological studies of the fate of implants of tumour tissue have not given conclusive evidence that the cells of the new tumour are direct descendants of the cells in the implant . 
 ( 1949 ) stated that the appearance of implants which had been frozen previous to inoculation , although they subsequently would give rise to tumours , " did not suggest survival of any of the implanted tissue . " zahl and drasher ( 1947 ) drew similar conclusions from their observations of the fate of implants of sarcoma 180 in mice . these authors state that there is no increase in the size of the implant and that it undergoes immediate cytological degeneration . several previous workers have studied the variation of tumour incidence with the number of cells inoculated . 
de gaetani and blothner ( 1936 ) found that over 100 , 000 cells were generally required for the successful transplantation of mouse carcinoma and sarcoma . furth and kahn ( 1937 ) , working with an inbred strain of mouse and a spontaneous leukaemia derived from that strain succeeded in transplanting leukaemia to about 5 per cent of their mice by the intravenous inoculation of a single leukamic cellw kahn and furth ( 1938 ) , using the trypan 368 h . 
hewitt a reaction usually regarded as being incompatible with cell viability ( schrek , 1936b ; pappenheimer , 1917 )  . counts of suspensions prepared from solid tumours were tberefore made after mixing equal volumes of the suspension and 0 5 per cent trypan blue ( b.d.h. , biologically tested ) in m / 15 sorensen buffer at ph 7 - 2 . no ascitic cell suspension has been found to contain more than 3 per cent of stained cells , and counts of these suspensions were made in the absence of trypan blue . trypan blue was preferred to eosin for the differentiation of non - viable cells because counts were made in a fuchsit gave more definite staining at non - toxic levels . rosenthal haemocytometer using phase - contrast microscopy . the absence of any reliable morphological criterion by which to identity a viable tumour cell makes it impossible to signify with certainty whether a given cell is a malignant cell or a normal cell contributed by the cellular reaction of the host . it has been found convenient to make an arbitrary distinction between normal tissue cells and sarcoma cells in fresh single - cell preparations of the tumours used in this study , on the basis of cell diameter . it was noted that 90 per cent of the nucleated single cells in sedimented preparations of minces of normal mouse lymph gland , thymus and spleen , and 70 per cent of the cells in saline washings of normal mouse peritoneum had diameters of 9 , t or less . 
on the other hand , a relatively small proportion ( 10 - 20 per cent ) of the cells in many single cell preparations of the solid sarcomas or in some s37 ascitic fluids , had diameters of less than 9 , u . 
the density of viable cells in a suspension has therefore been taken as equivalent to the density of cells having a diameter of over 9 , t and failing to stain with after considerable experience had been gained of the measurement trypan blue . of the cells in fresh preparations , actual measurement of the cells was abandoned and the larger cells were selectively counted by estimation of their size . frequency distribution curves of the diameters of the single cells of sarcoma preparations showed a modal diameter in the region 14 - 16 , t . 
a smaller , second peak was sometimes seen at about 7 , u , and this was considered to represent the mode of the inflammnatory cell population in the suspension . the effect of elimination from the cell count of all cells of diameter less than 9 , u was to exclude from the count the great majority of the non - tumour cells . 
on the other hand , a count of tumour cells made using this criterion might represent only 80 per cent , but no less , of the actual number of tumour cells present . titration of sarcoma cell suspensions . if necessary , the counted s37 cell suspensions were diluted to contain about 20 , 000 tumour cells in 0q1 ln . 
 ( the inoculum volume )  . of this suspension , five 3 - fold dilutions were made in the gelatine - tyrode medium , giving a series of six suspensions with cell densities varying from about 20 , 000 / 0 1 ml . 
to facilitate accurate placing of the inocula , all inoculations were given under ether anaesthesia . throughout all manipulations from the time of setting up the second phase of the sedimentation procedure until inoculation , the suspensions were kept at 2 - 5 c . full aseptic technique was employed throughout and special precautions were taken to keep the suspended celis in homogeneous distribution . recording of tumour incidence and calculation of end - points . inoculated mice were examined for palpable tumours at 2 - 3 day intervals from the 6th till the 30th day after inoculation in the case of s37 and from the 6th to the 40th day after inoculation in the case of the c3h sarcoma . it was found that , with very few exceptions , the smallest detectable mass in an inoculated site would become a definite tumour within a few days of its presentation . regression occurred in a fairly high proportion of the s37 tumours derived from the smaller inocula , but was unusual except in tumours which had attained moderate size . 
the proportion of sites in which a palpable tumour formed was recorded for each of the 6 different tumour cell in an ideal titration , all sites inoculated with the highest dose doses inoculated . of cells gave tumours and all those inoculated with the lowest dose failed to give tumours . 
from these data , the number of tumour cells which would have given tumours in 50 per cent of the inoculated sites ( hereafter referred to as " td50 " ) was calculated by the method of reed and muench ( 1938 )  . 
variation in td50 values obtained in ( i ) separate titrations of different s37 cell suspensions and ( ii ) parallel titrations qf the same suspension . in 16 titrations of different s37 cell suspensions performed in the manner described and using 4 - 6 mice per group , the td50 values ranged from 603 to 3162 cells , with a mean of 1641 and a coefficient of variation of 51 per cent . 
the ratio of the highest to the lowest value obtained in this series was 5 - 2 . it has not been possible to correlate this variability with any one factor known to vary from one experiment to another . suspensions prepared from tumours during their early growth phase and those prepared from older tumours gave results which were not consistently different . it is clear , however , that the variability in results from one experiment to another is contributed to both by unspecified differences between the suspensions and by random differences in the batches of mice used for the titrations . in order to assess the order of variability in results which may be expected in parallel titrations of the same suspension , a number of paired titrations were performed using 2 series each of 6 groups of 2 - 3 mice . in these experiments the mice were of comparable age but the members of corresponding groups were not litter mates . 
the values 2 sd and 3sd corresponded to ratios respectively of 2 - 0 and 2 - 82 , so that a significant difference between the td50s obtained for parallel titrations in control and treated animals should be considered when this figure was used as a guide ; the following further their ratio exceeds 2 - 0 . test of significance being applied when the ratio of the results exceeded 2 - 0 : the td50 and its standard error were calculated from the results of each titration by the approximate method of irwin and cheeseman ( 1939 ) ; the limits of error of each td50 were defined from a value 3 x s.e. , and a significant difference was inferred when the limits of error of the td50 with the greatest s.e. 
did not include this criterion of significance was the td50 value given by the other titration . used by the authors of the method to compare ld50s in certain toxicity tests . the adequacy of the test in the present context appears to be justified by the the multiple difference of td50 values obtained in following considerations : 8 pairs of titrations using only 2 - 3 mice per group , and with only random pairing of mice between the two series , did not exceed 2 * 0 ; in the parallel titrations to the results of which the test was applied , however , there were 4 - 6 mice per group , and each mouse of one series was carefully paired with a mouse in the corresponding group of the other series , the members of a pair being usually litter mates but occasionally mice from two litters born on the same day . 
each mouse received four equal inocula in the following sites : subcutaneously in the right axilla and right groin ; intramuscularly in the medial muscles of the proximal segment of the left forelimb and in the adductor muscles of the left leg . 
the inter - actions of multiple inocula in a single mouse . no normal mouse of the age and stock used has failed to develop a palpable tumour from the inoculation of undiluted s37 mince or of single - cell suspensions nevertheless , the behaviour of s37 transplants in of over 100 , 000 viable cells . the mice used displays the immunological phenomena characteristic of most strain - heterologus transplantations : regression occurs in a high percentage of tumours , and solid immunity to a second transplant usually follows upon the regression . 
from the fact that growth of s37 in the mice used results in the induction of resistance it must be assumed that each of several simultaneous inoculations into the same animal , whether of equal or of graduated doses , may be subject to influences of a constitutional nature induced by the others . to investigate this possibility a suspension of s37 cells was titrated in two series of mice . 
each series consisted of 6 groups of 5 mice each , and corresponding groups of the two series received the same dilution of the suspension and the same cell dose per inoculueach mouse of a group in one series ( s ) received a single inoculum of the appropriate dilution subcutaneously in the right axilla . 
each mouse of a group in the other series ( m ) received 6 subcutaneous inocula , all of the same size , one of these being in the right axilla . 
when the td50s were calculated from the right axilla results alone for each series their ratio was 1 - 6 , the difference it was concluded that the practice of giving four equal being not significant inoculations per mouse , in order to increase the number of sites used in the calcula374 h . 
hewitt tions , was probably not associated with results peculiar to the multiple inoculation procedure itself provided that the several inocula in each mouse were of equal sizes . a further experiment was designed to show whether the resistance induced by a large inoculum was capable of preventing a smaller inoculum of cells , placed simultaneously elsewhere in the same animal , from becoming a palpable tumour . a number of 3 - 5 - week - old albino mice were randomised to give one series ( c ) of 6 groups of 5 mice each and a second series ( m ) of 20 mice . 
the dilutions were inoculated into the mice of the successive groups of the c series in the usual way , 4 equal inocula being given to each mouse subcutaneously in the groin and axillary sites . 
the mean latent periods of all tumours arising from inocula of 247 , 741 and 2222 cells ( i.e. , in the region of the td50 ) in the s series and in the m series were respectively 13 - 7 days and 11 - 4 days . 
the 30 per cent incidence of tumours from 82 cells in the s series is fortuitously high , as may be seen from the trend of inoidence in this series . it is clear that the relatively high total inocula per animal with which the 247 , 741 and 2222 cell inocula were associated in the m series ( see last horizontal column of table ii ) has not significantly diminished the incidence or extended the latent periods of the tumours produced by these inocula . 
the effect of " hyalase " of the tumour incidence from small inocula of s37 cells . a single - cell suspension of s37 was titrated in two parallel series of mice . 
the influence of dead s37 cells upon the fate of small inocula of viable cells . in the following two experiments the effect of dead tumour tissue upon the fate of minimal inocula s37 cells has been studied under two conditions : ( i ) where the dead tissue was inoculated intraperitoneally previous to the inoculation of viable tumour cells subcutaneously , and ( ii ) where the dead tissue was incorporated in the inocula of viable cells . a s37 single - cell suspension was titrated in a control series of mice and in a parallel series each mouse of which had been inoculated intraperitoneally with 0 5 ml . 
of 20 per cent s37 mince freshly killed by repeated freezing and thawing . the inoculation with dead tumour tissue was made 48 hours before titration of the viable cell suspension . 
no significant difference between the td50s was obtained in the two titrations , their ratio being 1 - 07 . the second experiment was designed to show whether tumour production from minimal inocula is depressed or enhanced by the presence in the inoculum of a large preponderance of dead cells . 
hewitt the td50 values obtained in the two series were as follows : dilutions in gelatine - tyrode diluent dilutions in dead cell suspension 2818 although the difference ( ratio 4.3 ) was considerable , it did not quite attain significance by the irwin and cheeseman ( 1939 ) test . 
an experiment was therefore designed to compare under more carefully controlled conditions the activities on transplantation of two suspensions prepared respectively from these two sources . malignant ascitic fluid and four moderate sized subcutaneous tumours of s37 - were harvested from a single mouse inoculated intraperitoneally and subcutaneously with s37 mince 15 days previously . 
215 it will be seen from table iv that correlation between the td50 values in the two series is highest when the cell - determining tumour incidence is taken to be the larger unstained cell . 
1 shows the relationship between viable tumour cell dose and the proportion of inoculated sites giving tumours , for the c3h sarcoma and for s37 . the case of each tumour the points shown were obtained from two separate titraaverage tumour cells per inoculum ( loglo ) fig . 
the accuracy of the points is not sufficient to reveal the true character of the curves relating cell dose and tumour incidence but it will be seen that the rate of change of tumours incidence with log . 
white and loeb ( 1910 ) have described the successful transplantation of regressing tumours , and schrek ( 1936a ) has found no effect of immunity on the growth capicity of the tumour cells . these findings do not suggest the presence of humoral factors in regressing tumours which are active against the tumour cells themselves and encourage the view that regression is the result of primary breakdown of the stroma . the significantly lower td50 values given by intramuscular sites of inoculation compared with subcutaneous sites , for s37 , might ascribed to the greater vascularity of muscle . 
on the other hand , this site difference was not demonstrable for the c3h sarcoma , and a more likely explanation of the site difference found for s37 would appear to be that local resistance mechanisms are less readily manifested in the intramuscular sites . from the results of the experiments recorded in section 3 , it is clear that a small inoculum of cells is not suppressed , in the period before it forms a palpable tumour , by multiple and larger inocula of the same tumour placed simultaneously elsewhere in the same animal . this being the case , it seems probable that the failure to give rise to palpable tumours which is displayed by half the inocula of about 2000 cells of s37 , is not due to induction of systemic immunity by these 380 h . 
methods are described of preparing single - cell suspensions of mouse sarcomata from solid and ascitic tumours , of finding the viable tumour cell density in the suspensions , and of " titrating " them for tumour producing activity on inoculation . 
the implication of this finding for the problem of cell - free transfer is discussed . i wish to express my gratitude to miss catherine fysh , b.sc. , for skilled technical assistance , and to professor r . 
1. received for publication january 13 , 1948 . one of the implications underlying the work of huggins and hodges ( 1941 ) on the factors governing prostatic hypertrophy is that malignant prostatic cells are not fully , if at all , autonomous . that is , they are still controlled in some measure by the same factors that control normal prostatic cells . specifically , this is certainly true of their susceptibility to the influence of circulating androgens and oestrogens . carcinoma of the prostate is essentially a disease of old age . the possibility exists that the chief factor in deciding the individual 's susceptibility to this disease may be his androgenic state , that is , the level of circulating androgens in his blood , particularly during the later decades of life . the only practical method for ascertaining androgenic state is a determination of 17 - ketosteroids excreted in the urine of the subject . in the hands of many different workers ( barnett , henly , morris and warren , 1946 ) this method has revealed a very wide range of excretion of 17 - ketosteroids by normal men , at least in the lower age - groups . 
robinson the prostates of individuals who excrete at the higher or lower end of this scale will be subjected to grossly different amounts of androgenic stimulation . most of the available data on the excretion of 17 - ketosteroids is confined to results obtained in studies of men under the age of 30 - years . although there is a general impression that the excretion of these substances decreases with advancing age of the individual , there is a paucity of data on the range of excretion in the higher age - groups . the ideal method of study would be to make repeated determinations of the 17 - ketosteroid output in a large number of individuals over a period of m%ny years , until , in fact , the subjects did or did not develop prostatic cancer . 
the colorimetric measurements - were made on a hilger spekker photoelectric absorptiometer using a green ( ilford spectrum 604 ) and a violet ( ilford spectrum 601 ) light filter . 
1 clearly shows the distribution of excretion of 17 - ketosteroids with age . the output in childhood is low , rising rapidly at or about the age of puberty and reaching a maximum in middle age . 
2 , in which are plotted the as men between 30 and 40 . mean excretions for the third to the eighth decade , together with the upper and the ranges are computed lower limits of the ranges encountered at those ages . as the mean values + 2a . the fact that men continue to show comparatively wide individual variations in their outputs of 1 7 - ketosteroids and hence , probably , in the degree of androgenic stimulation to which their prostates are subjected , until very advanced age , must obviously be taken into account in any consideration of the aetiology of prostatic it will clearly be of importance to know whether known sufferers from cancer . this disease are characterized by excretions at the upper or lower ranges of their appropriate age - groups , or whether they are not significantly distinguishable a . 
clemmesen. from the danish cancer registry under the national anti - cancer league , copenhagen . received for publication december 10 , 1949 . developments in recent decades have made the term " cancer statistics " inadequate for the description of the ways in which statistics have contributed it is time that this term was reserved for statistical treatment to cancer research . of results , while statistical research into the occurrence of human cancer , be it from racial , genetical , geographical , occupational or other sociological points of view , should be included in the term " cancer demography . " this will be the case in the following . unlike many other branches of science joining in the research of cancer at some stage of its development , cancer sociology can point to a long , though most often neglected , history . 
when percivall pott , in 1775 , described the chimney sweep 's cancer , not only giving its clinical features , its treatment , and its social aetiology , but also taking active steps toward its prevention , in which we have finally succeeded , it was the first step in cancer sociology . pott 's observation of the latent period of scrotal cancer in chimney sweeps contained a very obvious clue to the experimental production of cancer , but experimental workers seem to have been too fascinated by experimental and pathological problems to take a lesson , not to speak of inspiration , from clinical or sociological observations , and 140 years passed before cancer was provoked experimentally by tar and soot . however , it seeins still more surprising that after this experience we have spent decades since young and russell 's demonstration in 1927 of a causal relationship between alcoholic consumption and cancer of the upper digestive tract in examining the carcinogenicity of numerous other compounds , while alcohol has been examnined only in a single experiment on a small scale ( krebs , 1928 )  . similarly it is well known that the first birth increases the possibility of a later cervical cancer , but where are experiments based on this and similar facts ? it would not seem unlikely that the slow progress in obtaining results of practical value in the fight against cancer is to a large extent due to our theoretical way of tackling problems . for instance , it is not unlikely that the future will reveal very interesting facts with regard to the influence of cosmic radiation on the incidence of cancer in heavily inbred animals of some kind , but there is considerable evidence that unless the energy released by such radiation shows a j . 
clemmesen different affinity to individuals of the various social classes , there must be social factors of a far more decisive character influencing the incidence of cancer in man . in order to bring about a closer contact between cancer research and problems of clinical importance , a more thorough investigation into the aetiology of cancer should be attempted by cancer demography through mass observations . 
to this we may add a frequent tendency among the former to take a more national and less universal point of view than is common so far in the medical world . 
an example of this is the variation in the proportion of gastric cancer in different countries , which has been discussed more often than the possible sources of error involved . for instance a first - class textbook of pathology states : " the incidence of gastric cancer in sweden and czechoslovakia apparently is about three times that of england . 
no satisfactory explanation has been offered for these interesting findings " ( anderson , 1948 ) as far as the present author has been able to establish , the reason for some of the differences may be that death certificates in the thinly populated areas of northern sweden for practical reasons are issued by parsons . furthermore , it will appear from the demands already mentioned that a direct comparison of percentages without a further analysis with regard to age distribution is unsatisfactory , especially in the case of a site such as the stomach , in which the establishment of a definite diagnosis is difficult . admittedly , death certificates have in the past rendered valuable information , especially in the hands of the english registrar - general , but this is no guarantee that death certificates from any country will produce similarly reliable details . it is vital to the use of death certificates that they are referred to the domicile of the patient , and not to the locality where death has occurred . 
and it must also be remembered that occupational statistics based on death certificates theoretically demand that the occupation of the deceased person should be stated from the same source as in the census , that is , some registration office , and not from the case - record or the statement of relatives , although tlis might not cause serious errors . comparisons of death certificates of different date are often made without the necessary regard to the dangers of this method . pedigrees of greater length may for instance be misleading because the frequency of cancers of various sites , whether apparent or real , will differ from one generation to the next . for sites of cancer where therapy is improving death certificates are decreasing in value as indicators of frequency , while other sites may show an apparent increase in frequency due to progress in diagnostic technique , and post - mortem figures will also be subject to this influence . 
heady and kennaway ( 1949 ) suggest that the proportional occurrence of lung cancer among the post - mortem total will serve as an indicator of changes in the incidence among the whole population . such figures are , however , influenced not only by the experience and information available to pathologists , but also through progress in the therapy of early complicating pneumonias and of lung cancer itself . * it is generally assumed that progress in diagnostic technique will cause an increase in the number of cancer cases registered , but according to the author 's experience gastric cancer tends to be overestimated , and will often decrease in frequency with improvements in medical facilities . consequently , comparisons between different countries or periods based on death certificates as well as on other sources of medical information demand additional knowledge of a more direct character . * readers of their review are recommended to compare the order of magnitude of the yearly totals criticized with those accepted as a basis for considerations , j . 
clemmesen for years hence , however , death certificates are bound to play an important part in demography of cancer , because they will be the best information available for the many cases not treated in hospital . 
even in the case of compulsory registration there will remain a number of notifications from general practitioners amounting in quality to little more than death certificates . it is also important to.the statistician to realize that the difference in quality of diagnosis between hospitals and general practice will cause a difference in the material , unless practically all cases are examined in hospitals , and this will be the case for only another difference between these groups will appear very few sites of cancer . in the age distribution curves , which must be based on the age at onset of the cancer , theoretically at the onset of symptomns . accurate statements on this item are unfortunately very difficult to obtain on death certificates , and for hospitals it is most practical to state the date of the first admission , which has the advantage of being an accurate reality . for all these reasons it will be evident that complete statistics on the incidence of cancer in a given area should contain figures for the number of cases treated in hospital for each site of cancer , and separate age distribution figures for this it is not uncommon for authors part of the material as well as for the total . dealing with a single site of cancer to leave out the total cancer incidence in the population concerned , but this is not permissible when we do not know the interrelations between cancers of different sites . 
the percentage of cases examined histologically or by autopsy should also be given for each site as an indicator of the basis of the diagnosis , and is particularly valuable in statistics giving figures for diagnoses of a histological character . 
at the moment such figures can only comprise a part of the cases really occurring , and it is most important to know the actual number of microscopical examinations from which they are collected , even in the case of a diagnosis such as " sarcoma , " which sometimes may be founded only on a macroscopical examination . unfortunately , many publications on cancer demography are inadequate with regard to statistics , and amount to little more than a summary of the author 's own conclusions , although they should contain all the basal figures for both the normal and the cancer populations , as well as the formulas applied , not only with regard to an independent judgment by contemporary workers , but also with a probably it is mostly view to retrospective work in the same field in future . editors and not authors who are to blame for such omissions , and the same applies to diagrams , which are as essential to such articles as are photomicrographs to histological or roentgenograms to radiological publications . cost will probably also be blamed for the fact that most of the valuable material on the occurrence of cancer is hidden away in statements from public health authorities . 
a unification of publications in this field , so that they could be collected in journals accessible to workers in experimental cancer research , would contribute far beyond its cost to the vital connection between experimental research and cancer demography . but it is most important in such publications that the author ascribes his findings to factors of some established certainty , and is reticent in advancing readers may find , even in new theories of his own on the aetiology of cancer . modern publications of some standing , that the well - established connection of alcoholic consumption with the incidence of certain cancers is paralleled by the influence of tinned or fried food . 
and storing at that temperature and after drying following freezing to from the frozen state ( gye , begg , mann and craigie , 1949 )  . in addition , mouse breast carcinoma which had been frozen to - 79 ' c . 
from these results it was concluded that since the physical treatments kired the normal embryo cells , they must also have killed the tumour cers , and that the tumours which arose from tho inoculations of treated m ' aterial must have been caused by a viius liberated from the dead cells . the claims of gye and his co - workers have been much criticized ; hirschberg and rusch ( 1950 ) , passey and dmochowski ( 1950 ) , passey , dmochowski , lasnitzki and millard ( 1950 ) and wamer and gostfing ( 1950 ) have all pointed out the great weakness of the assumption that since embryonic cells failed to grow after exposure these recent authors to low temperature , such treatment is lethal to ar cells . have each reviewed some of the ' extensive work reported in the last forty years , which shows that of both normal and neoplastic tissues in many species , some will and some will not survive exposure to extreme cold . in view of this great variation in response to cold shown by different tissues , it was felt that an investigation into the effects of freezing and drying upon a tumour affecting a non - mammalian host would be of value ; the rous no . 
i since it is a tumour from which a virus is easily fowl sarcoma was selected . separable , it was considered that the effects of cold and desiccation should be investigated upon the virus and the cers separately . that the virus was able to survive freezing and drying has been estabhshed for some time ( knox , 1939a ; hoffstadt and tripi , 1946 ; dmochowski , 1948 ; carr and harris , 1951 ) , and it has also been know - n to retain its tumour - producing activity after the ap ' plication of cold by repeated freezing and thawing ( cramer and foulds , 1930 ; selbie and mcintosh , 1939 )  . however , the response of the cells of the rous sarcoma to freezing and desiccation has not hitherto been ascertained . 
nakahara and yaoi ( 1930 ) found that rous sarcoma material which had been subjected to repeated freezing and thawing was less active when injected than similar untreated material , whidst selbie and mcintosh ( 1939 ) were able to prepare from rous tumour treated in this way filtrates with a greater tumour - producing activity than those made from untreated samples . selbie and mcintosh ( 1939 ) considered that repeated freezing and thawing broke up the cers and allowed a greater liberation of virus than would otherwise occur , and the method has been used for obtaining good yields of rous virus in various investigations ( knox , 1939b ; porard , 1939 )  . the work reported here consists ofexperiments upon the effects oftemperatures ' 70 ' c . 
they were between eight and nineteen weeks old when inoculated , apart from four exceptions which were slightly older , and belonged to three susceptible inbred lines developed at edinburgh , or crosses derived from thethe fines and crosses used were intensity , breeding , non - moult , breeding hen x intensity ' cock , and intensity hen x breeding cock , and have been described by greenwood , blyth and carr ( i948 ) ; both the age at which the birds were inoculated and the line or cross to which they belonged were determined by the exigencies of supply . preparation and treatment of tumour material . for each experiment a bird with a large actively growing sarcoma of anything from 15 to 27 days ' growth from the date of inoculation was selected as a source of tumour material and kired by wringing of the neck . 
when prepared , the disintegrated tumour was loaded into a record syringe for easy manipulation . where disintegrated tumour was to be subjected to cold or desiccation , the treatment was apphed as follows : freezing and storing . - amounts of i c.c. 
by starting the motor and setting the ampoule rapidly spinning on its longitudinal axis , a thin even film of disintegrated tumour was obtained on the inside of the bulb of the ampoule . 
the forceps w ' ere then released , causing a rapid rise of pressure within the apparatus ; this fell within five minutes to the original level , which was then maintained until the end of the period of drying , which lasted for 3 to 5 hours . 
epstein were separated off by centrifuging in an angle centrifuge at 3500 r.p.for 15 minutes , decanting the supernatant fluid obtained , and recentrifuging it aga ' in in a horizontal centrifuge at 6000 r.p.for a further 15 minutes . 
of saline and centrifuging in a horizontal centrifuge at 6000 r.p.for 15 minutes , resuspending the deposit in fresh saline , and performing the procedure either three ( experiment 1 ) or six - ( experiment 4 ) times . 
one sample of each preparation was mixed and incubated with an equal volume of saline and the other with an equal volume of serum ( diluted i in i 0 with sahne )  . 
the serum used ( e ) was from a fowl whose rous tumour had regressed and was one which had been shown to have strong anti - rous virus neutralizing powers in experiments 2 and 3 . that part of the experiment in which the virus and cer preparations were made from disintegrated tumour subjected to freezing and storing ( experiment 4c ) , samples of the preparations were mixed with an equal volume of pooled normal serum ( diluted 1 in io with saline ) , as well as with safine and neutrahzing serum e . all the mixtures were incubated in a water - bath at 37 ' c . 
in volume , and four inoculations of each preparation or dilution of a preparation were made . when inoculating preparations whose tumour - producing potencies were to be compared with one another , the injections of material from each preparation were made into separate groups of birds ; the scheme for the distribution of the injections of the various dilutions of each preparation amongst the birds in a group was the same in every case . 
the method of ' calculation used was that of reed and muench ( 1938 ) , and the figure obtained has been called by warner and gostling ( i950 ) the tpd 50 ; it is show - n in the tables comparison of this by its negative logarithm , designated the " tpd 50 index . " tpd 50 index of various preparations offers a comparison of their tumourproducing activities . strict aseptic technique was maintained throughout all the experimental procedures . all the experimental procedures were timed . 
where the virus suspension was made from disintegrated tumour which had been frozen and stored , the tumour - producing activity was in one case greater ( experiment id ) and in the other case less than that made from untreated material ( experiment 4d )  . it will be seen from table ii that washed cells of the rous sarcoma which had been exposed to any of the three physical treatments employed had less tumour322 m . 
on the other hand , in the case of washed cells which had been subjected to repeated freezing and thawing or freezing and storing ( experiments 4b and 4d ) , incubation with neutralizing serum , in contrast with incubation with saline or normal serum , totally deprived them of their tumour - producing activity . 
at the very least the centrifugation employed must be allowed to have separated off the overwhelming majority of the cefls , and the great tumour - producing activity remaining with the virus suspensions cannot be attributed to occasional cells left in them . accepting therefore that the virus suspensions were almost entirely if not wholly cell - free , the ability of the rous virus to retain some of its tumour - producing activity after exposure to cold has been demonstrated , thus confirming the work of cramer and foulds ( 1930 ) and selbie and mcintosh ( 1939 ) , who were able to prepare active filtrates from rous tumour material subjected to repeated confirmation has also been obtained of the ability of the freezing and thawing . virus to survive freezing and drp ' ng , which has been demonstrated by a number of previous investigators ( knox , 1939a ; hoffstadt and tripi , 1946 ; dmochowski , 1948 ; carr and harris , 1951 )  . 
as in the work of knox ( 1939a ) , so here the activity of virus preparations obtained from frozen and dried tumour material was considerably less than those made from untreated material ( table i , experiments ic and 4c )  . 
the contention , however , that preparations of rous virus made from repeatedly frozen and thawed sarcoma had a greater tumour - producing activity than those made from untreated material on account of the treatment breaking up.the tissue fragments and hberating the virus ( selbie and mcintosh , 1939 ) has not been borne out . 
the failure of the neutralizing ' serum to abolish the tumour - pro - ducing activity of washed cells which had been left untreated ( table iv , experiment 4a ) is considered to be evidence of the presence of live cells in the preparation . the slight reduction in the tumour - producing activity of the untreated washed cells which was brought about by incubation with neutralizing serum is considered to be due to the action of the serum on free virus liberated from or attached to cells damaged during the disintegration of the tumour material . the washed tumour cells subjected to freezing and drying were deprived of most of their tumour - producing activity after incubation with neutralizing serum ( table iv , experiment 4c ) ; out of the inoculations made with all the various dilutions of the frozen and dried washed cells , only one gave rise to a tumour . this was from one of the inocula of the 10 - 1 dilution of the mixture of cells and antiserunow , it has long been known that viruses can be recovered from neutral mixtures with antiserum simply by dilution of the mixture with sahne ; such reactivation has been demonstrated with vaccinia ( andrewes , 1928 ) and fowl plague ( todd , 1928 ) , and although this " dilution phenomenon " is harder to obtain in the case of the rous virus , andrewes ( 1932 ) was able to show it conclusively . 
japha. received for publication february 2 , 1949 . martn and reese ( 1936 , 1942 , 1945 ) were the first to describe an extensive series of cases of retinal glioma treated by deep x - ray therapy . in their latest paper they report 75 per cent 5 - year cures in 8 cases of bilateral disease , one eye having previously been removed by surgery . 
at the middlesex hospital 19 cases of glioma retinae were seen between 1929 and january , 1946 . all cases were treated , 4 by surgery alone ; in the others radiotherapy of one type or another played a major part in the treatment . 
the numbers are too small to allow comparisons to be made between different types of treatment , but as regards deep x - ray therapy certain conclusions have emerged , and a technique has been evolved which differs in some respects from that advocated by the workers of the new york memorial hospital . the results of surgery have greatly improved in the last 30 years according to ray and mcclean ( 1943 )  . collecting their figures from the literature they estimate that between 1868 and 1941 , 18 per cent cures were obtained by enucleation in 677 cases , whereas 50 per cent cures are claimed for the 105 cases so treated between 1911 and 1941 . this progress is ascribed to the more radical and improved technique , often with partial excision of the optic nerve , used in later years . 
the number of bilateral cases included , if any , is , however , not stated . the authors themselves advocate a combined intracranial and orbital operation in view of reese 's ( 1931 ) statement that 52 per cent of 119 cases showed invasion of the optic nerve beyond the lamina cribrosa . duke - elder ( 1940 ) also states that 50 - 57 per cent of unilateral cases may expect to be cured . reese ( 1940 ) cites statistics of 95 cases collected by the division of ophthalmic pathology of the american registry at the army medical museum , 26 of which had bilateral disease . 
at the time of review 21 cases were untraced , 39 had died , 13 had lived 5 years , 2 had lived 3 - 4 years , 10 between 1 and 3 years , and another 10 just 1 year . besides x - ray therapy , which is historically reviewed by martin and reese ( 1936 , 1942 , 1945 ) , attempts have been made at treatment of the second eye m bilateral cases by radon - seeds . these are usually introduced either into the growth itself or sown on to the sclera over the neoplasm . stalhard , in his gifford edmond prize essay ( 1933 ) , reports 5 cases treated primarily by these methods . one of his cases - first reported on by moore ( 1930 , 1935 ) , was treated in 1929 ( twice by the insertion of a seed into the growth and also by episcleral seeds ) , is still alive , but has a cataract . three other cases , including an advanced case treated only experimentally and intended for subsequent histological investigation , came to excision . in a further report stallard ( 1948 ) gives the result of 15 cases so treated . 
deep x - ray therapy . - as long as radium moulds were being used it was inevitable that the whole of the globe was being irradiated to a high dose , but with the change - over to and use of small beams that were developed in deep x - ray therapy it became possible to limit the volume ofhigh dose to a certain extent . 
our technique has been directed at eradicating the focus of disease present rather than treating the whole of the posterior half of the retina ( where the majority of the growths are situated )  . 
a recent case , however ( not included in this survey ) , showed us that a certain risk isrun thereby in that shortly after the treatment and subsequent disappearance of a small lesion below the equator by fields of 2 and 3 cdiameter a further nodule appeared in the upper half of the retina . in an endeavour to treat as small a part of the eye as possible we have used circular fields of 2 and 3 cdiameter by means of special tubular applicators primarily intended for intrabuccal lesions as described by roberts and quick these are used in connection with our deep x - ray tubes , treatment ( 1943 )  . being carried out at 190 - 220 kv . 
lateral ( temporal ) , medial ( tansnasal ) , superior and inferior orbitals . abandoned as soon as it became apparent that the cornea was the most vulnerable structure of the eye , and disintegration of the eye had occurred in 2 or 3 cases in which this approach had been used . the lens , too , will receive a relatively large dose of irradiation when the anterior field is used and the lens dose should be kept at aminimuwe endeavour to ensure this by our technique of " by - passing " the lens as much as possible , which can be achieved in all the other fields mentioned . the anterior field was fields used so that accuracy ofalignment positioning . - special problems ofset - up arise because of the age of the patients and the small is of much greater importance . most of the children under the age of 4 need steadying during each treatment , and the older ones atleast during the first 2 or 3 sessions . we have in a few cases tried to make individual plaster casts into which the child is put during treatment , the cast including a headpiece with a frontal process to obviate any possibility of head movement . in practice , however , even the smallestchildren have been found to wriggle around in these casts human hands have had to help . the casts are usefuil , nevertheless , for steadying at least the trunk , and one escapes the otherwise necessary manoeuvre of binding the child on to the couch . children this can be done best by first wrapping the child tightly into a blanket , arms included . all cases - - and at each treatment - are set up by a medical officer , and during treatment , if necessary , the head steadied either by himself , by a radiographer , or by a nurse - or , if available , one of the parents . 
and by treatments lasting 16 or 57 days , but the number of cases observed is too small to confirm the impression that neither dose rate nor the total time are of critical importance within a wide range . 
irrespective of whether radium - moulds or deep x - rays were used , including one case in whom radium - moulds of increasing strengths were applied at short intervals within 5 months , the highest single dose being 3800 r . two main treatment schemes have been used : either a single " radical " course or repeated courses of deep x - rays , in each one of which a dose was given just sufficient to make the tumour disappear . this was usually achieved by doses of 2000 - 3000 r . , to be repeated as soon as there was renewed activity . the latter scheme is somewhat similar to that recommended by martin and reese ( 1936 , 1942 , 1945 ) , but in our hands it has never been successful , whereas the single radical course of treatment has given us outright cures . we have only once had the opportunity of treating a unilateral case ab initio . this was a girl , aged 3 years and 9 months , who came with a history of over 2 years but still only a comparatively small growth . 
ten months later , however , there was a large recurrence and the eye was excised . histology confirmed the presence of active growth . sometimes it has been necessary to continue the first course up to a much higher tumour dose . there was one case in our series where even the second eye carried a growth covering almost the whole of the retina - he had come to us with simultaneous affection of both eyes . after the excision of the first eye , which was completely filled by growth , a tumour dose of 5730 r . 
japha in this part of the body as anywhere else - but perhaps even with greater force - is one struck by the confirmation of the hypothesis most prevalent for the explanation of failures through over - dosage . 
we have not as yet given postoperative treatment to the orbit of the removed eye in bilateral cases . this may be advisable as a general policy in view of the ultimate fate of some of them , i.e. 
local recurrence even where no apparent extra - ocular extension was originally present , unless one regards these deposits as due to retrograde extension from the second eye , which by that time has got completely out of control . 
one should also remember , as duke - elder ( 1940 ) points out , citing meighan and michaelson ( 1938 ) , that there may be discontinuous spread in the nerve , so that the excised specimen ( even if part of the nerve is included ) need not necessarily show the extra - ocular extension which has in fact already taken place . carrying out this suggestion the contribution that the lateral fields will make to the retained retina or the enucleated orbit respectively and which will amount to a depth dose of about 20 per cent must be taken into account . this technique has been used in a recent case which had a recurrence in the excised orbit as well as growth in the second eye , and is also applicable in the " prophylactic " irradiation of a case in which bilateral enucleation has been performed . when we first collected these cases it appeared as if the unilateral cases treated post - operatively by irradiation would not be of very great interest because surgery alone might have been responsible for the good results . 
we have , however , in our series one case of recurrence within 6 / 12 of the operation ( this was treated by a combination of deep x - rays and implantation of radon - seeds , but recurred again and proved rapidly fatal ) , and the above - mentioned case , which may be regarded as having been inadequately treated in the post - operative period . this case had a remarkably long latent period of 5 years , and a very large dose of irradiation was necessary to arrest the growth . 
no growth was found on histological examination . one case of massive recurrence in the orbit with bone involvement after enucleation of the only affected eye failed to respond to combined irradiation by deep x - rays and implantation of radon needles ; another case , successfually treated , is of considerable interest . it is the case already mentioned which received a post - operative prophylactic dose of 660 r . 
by deep x - rays in 16 days for a recurrence after treatment by radon - seeds elsewhere ( tumnour dose estimated at 2000 r . ) , was complicated by chronic iritis and needed extraction of this the remaining eye 4 months later ( now 52 years ago ) - no growth was found on histological examination , as already mentioned . 
 ( in 57 days ) ; this was extracted 4 years ago and vision is only partial another cataract that was removed was obvious already 9 months after now . a dose of 3000 r . 
hfirst came under observation at the middlesex hospital in july , 1945 , at the age of 9 / 12 , having had his left eye excised elsewhere 3 months before ( histology showed retinoblastoma without involvement of the optic nerve ) , and at the same time a focus the size of a disc in the periphery of the right retina had been isolated by diathermy barrage . 
about a fortnight after this examination the boy began to vomit ( apparently in a rather projectile manner ) and became drowsy . lvhen examined again on 20.xi.46 there were signs of brain - stem involvement , and a course of deep x - rays directed there was some temporary improvement , but the at this region was started . child died within 3 months of the onset of the final stage . 
lumbar puncture during this time showed the presence of peculiar mononuclear cells in the cerebrospinal fluid , which in the light of the later post - mortemn findigs must be regarded as retinoblasts . 
m - 1 , a boy , 5 years of age , was sent to the middlesex hospital in 1929 from jersey , where 5 months previously his right eye had been removed for glioma retinae . 
a radium mould was applied as a " delayed post - operative measure , " but the surface dose when recalculated recently was found to have been only 660 r . 
 ( in 36 hours )  . nearly 5 years later there was a large swelling in the orbit whiceh was treated by x - rays in jersey ( details unknown ) and the swelling disappeared . 
a few months later a further course of x - rays was given for a " small hard bean - shaped swelling " in the lower half of the orbit . seven months after this the mass was again thought to be larger and the boy referred back to the middlesex hospital in september , 1936 . 
the boy was lost sight of during the war , but reported again as a young man in october , 1946 , that is , 10 years later , when he presented with marked telangiectases on the right cheek around the orbit and a small sinus over the zygomatic arch . 
the results of radiotherapy are summarized in table vii . ( a ) post - operative irradiation has been successful in the two cases where adequate treatment was given irrespective of whether a radium mould or deep x - rays were applied . in the one case described at length above , the first treatment , where 660 r . 
only were given , must be regarded as quite inadequate , but the recurrence which developed 5 years later responded well to a radical course . ( b ) primary irradiation . - the two cases treated by radium moulds and two of the three cases treated by deep x - rays more than 5 years ago are alive and e . 
cotton treated in a colloid mill . this was prepared from cotton velvet shearings suspended in water and passed through a colloid mill 6 times in succession . after each passage only the finer fraction was slected for further milling . 
5 shows the compact growth of mouse mammary carcinoma obtained in the presence of fibres of colloid milled cotton ; as a contrast the uneven growth of cells in the absence of fibres is shown in fig . 
for 5 minutes , washed with distilled water until free from ammonium ion ( tested by nessler 's reagent ) and sulphide ion ( tested by sodium nitro - prusside )  . they were then bleached 15 minutes at room temperature in sodium hypochlorite solution containing 0 - 1 per cent available chlorine , and finally washed with distilled water until free from chloride ion ( tested by silver nitrate )  . 
they were stored under distilled water . the films were autoclaved in distilled water at 18 lb . / square inch pressure , and before use were rinsed in sterile tyrode solution , excess moisture being removed with sterile filter - paper . cultures were placed directly on the coverslip , a drop of mixed serum and embryonic extract spread over them and the viscose film then applied . 
the culture usually adhered to the glass surface , and on washing or fixation the film floated off . the film is easily cut with a cataract knife when the tissue is subcultured . with a thickness of 30 , u the total thickness of the preparation was considerably less than can be achieved with the double coverslip method of maximow . 
they have found that perforated cellophane is an advantageous addition to flask cultures and hanging - drop preparations ( evans and earle , 1947 ; earle and evans , 1949 ; schilling , earle and evans , 1950 ; earle , evans and schilling , 1950 )  . in our hands perforated cellophane , kindly supplied by w . 
earle , was very siinilar in effect to viscose , but the outgrowth obtained with viscose seemed slightly greater . glass wool has been used for the same purpose by warner , hanawalt and bischoff ( 1949 ) , who used it with the roller tube method . 
viscose ifim , colloid milled cotton and durafil were technicauy suitable for use , and have been found advantageous in improvilg growth of malignant cells and of enabling growth of normal and malignant cells to take place in fluid media . we wish to thank professor astbury of leeds for his advice , and t . 
dmochowski. from the department of experimental pathology and cancer research , medical school , university of leeds . received for publication december 15 , 1952 . the test mice most commonly used for ascertaining the presence of the mammary tumour agent are susceptible hybrid female mice obtained by mating low - breast - cancer - strain females to high - breast - cancer - strain males . in these test mice a low incidence of spontaneous mammary tumours was frequently recorded ( bittner , 1939b ; murray and little , 1939 ; andervont , 1940 ; gardner , 1941 ; dmochowski , 1944a ) , and was frequently found to be higher than that of their maternal parents ( andervont , 1945a )  . 
of even greater interest was the high tumour incidence reported in the progeny of susceptible low - cancer - strain females mated to high - cancer - strain males which had been subjected to forced breeding - that is , bearing a number of litters in quick succession ( andervont , 1945b )  . 
a similar high incidence of breast cancer was also observed in forciblybred hybrid progeny of low - cancer - strain females of low susceptibility to breast tumours mated to high - cancer - strain males ( bagg and jacksen , 1937 ; strong , 1943 )  . attempts to discover the mammary tumour agent in mammary tumours of some of these hybrids proved unsuccessful ( andervont , 1945b )  . 
a subline of c57 black strain is now established in which this subline a number of mammary tumours has been recorded by the author . comes from one of the original threelitters brought from the laboratories of the the progeny of these litters has been kept imperial cancer research fund . separately , and no breast tumours have so far been recorded in the descendants the description of the subline in which tumours have of the other two litters . the riii strain mice appeared will be the subject of a separate communication . were also obtained from the same source and maintained since 1946 . the tumour incidence of 83 per cent at an average age of 8x5 months in breeding females ( dmochowski and gye , 1943 ) has with small variations remained approximately it was known that mice of high - cancer strains derived from the fourth the same . or later litters develop a higher incidence of breast cancer than those from the first two litters ( bittner , 1942 ) , and that the appearance of an active agent in mice deprived of it by foster nursing had been recorded in the progeny obtained from hybrid progeny of the c57 black strain the third or later litters ( bittner , 1943 )  . females was therefore taken only from the fourth or laterlitters for the experiment , mice from earlierlitters being used for various other purposes . 
the ( c57 x riii ) fl hybrid females which were litter mates were divided into two groups . only two hybrid females were taken from each of the c57 females mated to riii strain males , if possible from the same or foliowing litters . whenever two females were not available from the same litter , the mice from later litters were included in this way two groups , each comprising thirty ( c57 x in the control group . riii ) f1 hybrid females , were obtained . mice of the control group were allowed to breed in a normal way and mice of the experimental group were forcibly bred by removing their litters as soon as they were born . mice of one of the later litters from fifteen hybrid females in this group and of one litter of a female from the these mice in turn , control group were saved for brother to sister matings . after saving one litter , were forcibly bred and this procedure was followed for several generations . 
the progeny of six ( c57 x riii ) f1 hybrid females , which had been subjected to forced breeding , was maintained for six generations and the progeny of nine additional ( c57 x riii ) f1 hybrids , treated in a similar manner , for only three generations . 
dmochowski tumour which on histological examination was found to be a lymphosarcoma . the average number of litters bom to these hybrid females was three , and varied from two to seven . 
the number of breast tumours which developed in their litter mate ( c57 x riii ) f1 hybrid females , which had been forcibly bred , is shown in table ii . 
among these hybrids , the tumorous females had an average of 6 * 5 litters and the tumour - free females 6 - 4 litters . there was no difference therefore in the number of litters born to these two types of females which had been forcibly bred . none of the c57 black strain mothers , mated to riii strain males and bred in a normal way , developed mammary cancer , although they lived to an average twelve c57 black strain females , which were litter - mates age of 19 mouths . of some of the c57 females mated to riii strain males , were forcibly bred with their own litter - mate males , and none developed breast cancer , although they had an average of 5 * 2 litters and lived to an average age of 18 months . 
the observation that none of the c57 strain females developed mammary tumours after mating to c57 strain males and forced breeding points against the possibility of c57 black strain females harbouring a weak or attenuated mammary tumour it is now well known that various sublines of c57 black strain differ agent . considerably in their susceptibility to the agent . c57 strain mice of the subline of the present experiments , when foster nursed by riii strain females , developed an incidence of mammary cancer of only 11 per cent ( dmochowski , 1948 )  . this low susceptibility was probably responsible for the failure to induce mammary cancer in mature c57 mice of this subline even by a combined action of large doses of material containing the agent and forced breeding ( dmochowski , 1948 )  . again this low susceptibility may also have been responsible for c57 mice of this subline remaining tumour - free after mating to riii high - cancer - strain males as well as for their hybrid progeny , bred in a normal way , not developing mammary cancer . 
a further indication against the possibility of c57 black mice of this subline harbouring a weak agent or in small quantities was provided by the absence of the agent in mammary tumours induced in both virgin and breeding c57 females by treatment with methyloholanthrene ( dmochowski and orr , 1949 )  . 
the forcibly - bred progeny of four ( c57 x rhij ) f1 hybrid females which had died free from tumours , also continued in these figures , the number of for six generations , is presented in fig . 
3 to 6 that descendants of tumorous hybrid females . females can remain tumour - free for two , three or four successive generations before developing mammary cancer , and that descendants of a non - tumorous female , in spite of reaching tumour age , may show no mammary tumours for as many as five generations before developing breast cancer , in spite of inbreeding it may be of interest to point out that and intensive hormonal stimulation . andervont ( 1949a , 1949b ) found the agent to be transmitted through three or four successive generations of susceptible mice without inducing mammary further , the study of the distribution of mammary tumours in charts cancer . of the progeny of tumorous and non - tumorous hybrids , shown in fig . 
1 to 6 , indicates the possibility of the agent being involved in the development of these tumours . a comparison of the age of the earliest tumour appearance , tumour incidence , average tumour age and average age at death of the progeny of individual tumorous and four tumour - free ( c57 x rii1 ) f1 hybrid females is shown in table iii . as can be seen , there was little , if any , difference between the forcibly - bred progeny of the two ( c57 x riii ) f1 females which developed breast cancer and the forcibly - bred progeny of the four ( c57 x riii ) f1 hybrid females which died without tumours . table iv demonstrates the tumour incidence and tumour age in the forcibly - bred progeny of additional nine non - tumorous ( c57 x rii1 ) f1 females which was continued for three generations . 
the tumour incidence , although varied in the progeny of the individual hybrids , was lower and the age of breast tumour appearance higher than those in the progeny of the two tumorous and also of the four tumour - free ( c57 x r111 ) f1 hybrid females . 
number preceding letters t , n or l = number of female ; number following letters t , n or l = tumour age or life span in days . of the earliest tumour appearance , the appearance of mammary tumours according to months , the tumour incidence , and the average tumour age in six generations of combined forcibly - bred progeny of the thirteen non - tumorous ( c57 x riii ) f1 hybrid females . 
dmochowski generation of the progeny of this non - cancerous hybrid female may be seen in this figure as well as the consecutive number of litter to which the mice belonged which developed tumours . it would have been of interest to obtain the first litter of this female and its progeny and compare any mammary tumour incidence in this progeny with that of the progeny obtained from the sixth litter , but this could not be done owing to limitation of space . table vii shows the age of earliest tumour appearance , the tumour incidence , and the average tumour age in the normally - bred progeny of this non - tumorous ( c57 x riii ) f1 hybrid female . 
the breast tumour incidence in the forcibly - bred progeny of the non - cancerous ( c57 x riii ) f1 hybrid females was lower and the average tumour age considerably higher than those in the forcibly - bred progeny of cancerous ( c57 x riii ) f1 hybrid females , but this difference in tumour incidence and average tumour age gradually became smaller in successive generations of the progeny . 
the age of the earliest tumour appearance and the average tumour age in the progeny bred in a normal way of one cancer - free ( c57 x riii ) f1 hybrid female was distinctly higher than those in the forcibly - bred progeny of both tumorous and tumour - free ( c57 x riii ) f1 hybrids . 
the tumour incidence in the normally - bred progeny was , with one exception , lower than that in the forcibly - bred progeny of tumorous hybrid females and , again with one exception , approximated to that in the forcibly - bred progeny of non - tumorous hybrid females . it should be pointed out that the results of the comparison of the behaviour of normally - bred progeny of one non - tumorous female with that of the forcibly - bred progeny of thirteen non - tumorous hybrid females may not be the same as those which would have been obtained should this comparison have been extended to similarly maintained progeny of a number of other cancer - free hybrids which had been bred in a normal way . this point may be seen from the observations on the forcibly - bred progeny of four nontumorous ( c57 x rii1 ) f1 hybrids compared with those on similarly treated progeny of two tumorous ( c57 x riii ) f1 hybrid females . 
the difference in mammary tumour incidence and average tumour age between these two groups of hybrid females became pronounced only after including the observations on the progeny of nine additional non - tumorous ( c57 x riii ) f1 hybrid females . is therefore possible that the results of the comparison of normally with forciblybred progeny of non - cancerous hybrids would have been different as in the case of the comparison of forcibly - bred progeny of non - tumorous with that of tumorous it is not known whether the results of foulds ' ( 1949 ) comparison of hybrids . forcibly - bred progeny from tumorous and non - tumorous hybrid females would l . 
dmochowski not have been different had the progeny of a greater number of non - tumorous hybrid females been included in his study . from the study of the distribution of cancerous females in the forcibly - bred progeny of tumorous and tumour - free ( c57 x riii ) f1 hybrid females and in the normally - bred progeny of a cancer - free hybrid , shown in fig . 
among the forcibly - bred progeny of the four tumour - free ( c57 x riii ) f1 hybrids , tumorous mice had an average of 7 3 ( 1 to 13 ) and the mice without tumours an average of 8 - 3 ( 1 to 16 ) litters . 
the behaviour of mice in the progeny obtained after the tumour appeared in their mother may greatly vary even in the case of hybrid females of the same origin , probably as a result of variations in the genetic make - up of individual females infiuencing the presence or transmission of the agent . in conolusion it may be stated that both the genetic constitution and hormonal stimulation play an important part in the development of mammary cancer in the hybrid mice which were the subject of the present study , and that the mammary tumour agent also appears to take a part in the origin of these tumours . biological tests for the presence of the mammary tumour agent . as soon as the first mammary tumours appeared in the hybrid mice , biological altogether twenty - three tests for the presence of the agent were carried out . of the mammary tumours were tested and the results are shown in table xiii . four mammary tumours which developed in ( c57 x riii ) f1 hybrid females , two showed the presence of the agent and two others failed to reveal the agent under the conditions of the test . 
at first it appears surprising that the tumour which developed at the age of 10 months failed to show the agent , as the time of storage in desiccated state was equal to that of another breast tumour which appeared in the same generation and which , although injected in smaller quantity , induced tumours in the test mice but in distinctly smaller incidence compared with that induced by other dried agent - harbouring tissues in previous it must be stressed experiments ( dmochowski , 1945a , 1945b , 1946 , 1948 , 1949c )  . that the method of desiccation of these two as well as of all the other tumours was the same , and the age of the test mice used was in all cases approximately the same . the only varying factors were the amount of tissue injected and the time of storage . 
the longest period of storage in the ice - chest was that of a negative tumour in a ( c57 x riii ) f , hybrid female and amounted to 8 months . this should not have made an appreciable difference in the test , as it was previously shown that agent - harbouring tissue induced breast canoer in test mice after two years of storage ( dmochowski , 1946 )  . 
from the results of the tests of the four tumours in the first generation of hybrid females it may be concluded that two of them possessed the agent , and the two other negative tumours either did not contain the agent or harboured only small quantities or a weak agent which could not be shown under the conditions of the test . 
2 , from the study of parent - offspring correlation there was a definite tendency towards breast cancer development in daughters of tumorous as well as non - tumorous mothers . 
9 female had ten litters and her sister had seven litters . it may well be that the considerable hormonal stimulation was responsible for the appearance of breast cancer in these females , and more likely that the agent took part in the development of these tumours but in quantities too small to be detected by the ( c57 x riii ) f3 no . 
it may well be that had the test a : nimals , in which the latter tumour was tested , lived longer , the agent would probably have been detected . in the fourth generation of the progeny of no . 
20 ( c57 x riii ) f3 hybrid , were found to harbour the agent . the first tumour developed at the age of 8 months after the female had six litters , and the second at approximately 17 months after the female had thirteen litters . it is of interest that both tumours showed the agent , although the second developed comparatively late in life . in the fifth generation of the same line three tumours were tested , those of no . 
69 ( c57 x riii ) f1 tumorous hybrid female in whose tumour the agent was not detected , it may be seen how necessaiy it is to adopt a cautious attitude towards the results of biological tests . it appears probable that the agent may have increased gradually in quantity in successive generations of the descendants of this hybrid female , so that it eventually could be detected by the method applied in the present biological tests . it is possible that the treatment , such as desiccation , may have in part been responsible for the negative results when tumours with small quantities of the agent were tested . had the mammary tumour of no . 
69 ( c57 x riii ) f1 hybrid only been tested and the progeny of this female not raised , the conclusion would have been that increased hormonal stimulation of a susceptible genetic substrate was responsible for the appearance of this breast tumour . it may well be stated that hormonal and genetic factors combined with the mammary tumour agent were responsible for the development of the majority of the tested breast tumours in this line , and probably also a weak or attenuated agent in the tumours negative in the biological test . in the progeny of non - tumorous ( c57 x riii ) f1 no . 
33 female at the age of 17 months after she had eleven litters and one which arose in ( c57 x riii ) f4 no . 39 hybrid at the age of 10 - 5 months after she had given birth to six litters . 
21 , 47 , and 49 ( c57 x riii ) f3 hybrids , all of which developed after the eighth litter at the age of 9 , 12 , and 10 months respectively . all four tumours harboured the agent , yet , although they all arose comparatively early in life , the incidence of tumours induced in the test mice by the tumour of no . 
tumours developed in hybrid mice of all three coat colours without particular connection with any coat colour . foulds ( 1949 ) recorded a similar observation in his c57 x riii hybrids . neither the presence or absence of the agent , as shown in biological tests , was connected with any particular coat colour . foulds ( 1949 ) detected the agent in the tumour of a ( 057 x riii ) f1 hybrid muhlbock ( 1952 ) failed to discover the agent in tumours which had been tested . of five ( c57 x d ) hybrids which developed at ages varying from 20 to 30 months . these hybrids came from early litters . 
mammary tumours in hybrids from later litters of c57 females were not tested , but the presence of the agent in these tumours was assumed by muhlbock ( 1952 ) on the basis of a high tumour incidence in the litters , although the average tumour age was 18 months . 
a search for the agent in mammary tumours of hybrid progeny from another ( c ) low - cancer - strain but susceptible females and high - cancer - strain ( 03h ) males led to the detection of the agent in tumours which developed at an early age up to 12 months , although on two occasions even such tumours were negative ( andervont , 1945b ; andervont and dunn , 1950b ) , while mammary tumours arising at a late age , in spite of their high incidence , failed to reveal the agent ( andervont and dunn , 1949 , 1950b ; andervont , 1950a )  . yet , on one occasion a c strain female was found to harbour the agent , although she developed breast cancer at the age of 21 months ( andervont and dunn , 1950b )  . thus there may be exceptions in both early and late developing tumours , as shown in the present study with dried tumour tissue and in the experiments of andervont and dunn with fresh tumour tissues . biological tests of some tumours appearing at a late age , as shown in the present experiments , revealed the agent , although they failed in other . 
tumours of similar it is not known how far the recent observation of andervont ( 1950b ) late age . that small quantities of the agent may only be ascertained by observing at least one or even two generations of the descendants of the inoculated test mice would be helpful , but it is certainly worth trying in any future tests of mammary tumours appearing at a late age . in some mammary cancers which developed up to the age of 12 months , the agent could not be detected on several occasions in the present study . 
69 f1 hybrid were found to possess andervont ( 1945b , 1950a ) also failed to detect the agent in mice with the agent . tumours at 8 , 12 , 14 , 15 and 16 months . 
on the basis of the study of parentoffspring correlation shown in pedigree charts , it appears probable that the negative tumours also harboured the agent possibly in quantities too small to be detected by the tests applied . in conclusion it may be stated that the results of the biological tests for the presence of the agent in desiccated mammary tumours which developed in the hybrid mice indicate a gradual accumulation of factors responsible for the appearance of mammary cancer . it appears that there may be a certain threshold below which it is difficult or not possible to show the agent in some mammary tumours , at least by the methods so far employed , and only after combined influence of inbreeding and intensive hormonal stimulation the presence of the agent may become detectable . there is no reason to consider the biological tests as inadequate , in view of the previously reported constant positive results with dried agent - containing tissue , and also in view of the negative results occasionally recorded by other workers with fresh material even from tumours which developed early inlife . further , negative tests for the agent in dried tissue of an 86th transplant of a mammary tumour which originally harboured the agent ( dmochowski , 1952 ) have been confirmed with fresh tissue of a 101st serial passage of the same tumour . the negative findings may have been due either to small quantities of the agent present in some tumours or to the kind of relationship of the agent to other cell constituents in these tumours , such as close integration with these constituents , different from that in other tumours which were found positive in the biological tests . microscopical appearance of mammary tumours . in view of the availability of a large number of tumours of a comparatively uniform origin a microscopical study of these tumours was made , and also an attempt to correlate the morphological appearance of these tumours with the presence or absence of the agent . 
as can be seen the majority of tumours in this agentharbouring strain could be divided into roughly equal numbers of type a and type b tumours . the results of the study of 377 mammary tumours in 327 c57 x riii hybrid mice are shown in table xiv . 
among the 327 tumorous mice , 32 had two tumours and 9 had three tumours . as shown in table xiv , the majority of most of the tumours ( 70.6 per cent ) developed during tumours were of type b . the first 12 months , and among them 53 were of type a ( 19.7 per cent ) and 215 ( 79.9 per cent ) were type b tumours ; one unclassified mammary carcinoma also after the first 12 months , 21 tumours belonged to this group of early tumours . were of type a ( 19.4 per cent ) , 77 tumours belonged to type b ( 71.4 per cent ) , 9 tumours were of type d ( 8 - 3 per cent ) , and 1 tumour was unclassified . 
an analysis of the distribution of the different types of tumours in the progeny of tumorous and non - tumorous ( c57 x rii ) f1 hybrids revealed that the progeny of both types of females had a number of each type of tumour similar to that found in the total number of all tumours . 
among the 120 mammary tumours of the descendants of tumorous hybrid females , there were 19 ( 15.8 per cent ) of type a , 99 ( 82.5 per cent ) of type b , and 2 ( 1.7 per cent ) of type d . 
among the 225 tumours in the forcibly - bred progeny of non - tumorous hybrid females , 50 ( 22.2 per cent ) belonged to type a , 166 ( 73.8 per cent ) to type b , 7 ( 3.1 per cent ) to type d , and 2 ( 0.9 per cent ) were unclassified . there were 32 mammary tumours examined in the progeny of a non - tumorous hybrid female which had been bred in a normal way ; five ( 15 - 6 per cent ) were of type a and 27 ( 84.4 per cent ) belonged to type b . 
there was no difference in the distribution of types of tumours in the progeny of hybrids which had been subjected to hormonal stimulation of varying intensity . no correlation was observed between the type of tumour and its location or size or rate of growth or litter sequence of the tumour - bearing mice or age of the animal at which the tumour developed , except in the case of type d tumours , further , there was no all of which developed in mice older than 12 months . correlation between the types of tumours in litter mates or between tumours of mothers and offspring . similar observations were reported by andervont and dunn ( 1950b ) on ( c x c3h ) susceptible hybrids , in which they found 38 per cent of type a tumours , 44 per cent of type b , 9 per cent of type c , and 8 per cent of type d . 
they observed a correlation between the age at which mammary tumours appeared and the type encountered , as in mice of up to 19 months of age 63 per cent were type a tumours and 33 per cent type b tumours , and in older mice 31 per cent belonged to type a and 48 per cent to type b . in another study ( andervont , 1950a ) 38 per cent of tumours were of type a and 46 per cent type b , and in 106 l . 
they did not detect the agent in a c strain female with a squamous type mammary tumour at a late age , yet in her progeny there appeared a type a tumour with the agent and one squamous type cancer without the agent . another two females of the same strain , two tumours of type a and b respectively both harboured the agent ; in their progeny all tumours with the agent were of type a . 
the majority of tumours in old mice were similar to those of mice with the agent ( andervont , 1945b , andervont and dunn , 1949 )  . in hybrid mice obtained from crossings of agent - free low - cancer - strains the majority of mammary tumours were of types c and d , and in those obtained from one of the parents belonging to agent - free but high - cancer strain the majority of breast tumours were of types a and b ( andervont and dunn , 1948a )  . it appears that the genetic constitution of strains used for breeding hybrids influences at least the distribution of the various types of breast cancer . there was no correlation in c57 x riii hybrid females between the presence of the agent , as shown in biological tests , and the type of tumour encountered . of the seventeen tumours in which the agent was found , ten were of type b , six of type a , and one of type d , and among the mammary tumours in which the test failed to reveal the agent , four were type b and two type a , cancer ( table xiii )  . 
the finding of the agent in type d mammary tumour which developed at 17 months is of interest , as it appears to indicate that not all squamous type tumours which appear comparatively late need be agent - free tumours , or possibly tumours in which for some as yet unknown reason it is difficult to detect the agent . 
two agent - harbouring tumours of ( c57 x riii ) f1 hybrids were of type a ( 11 months ) and type b ( 16 months ) , and the two other tumours in which the agent was not detected were also of type a ( 10 months ) and type b ( 11 months )  . 
among the fifteen agent - harbouring tumours of c57 x riii hybrid progeny , five were type a and arose at the age of 9 to 13 months , nine were type b and developed at 7 to 17 months , and one type d at the age of 17 months . 
among the tumours in the hybrid progeny in which the agent was not detected , one was of type a ( 18 months ) and three of type b ( 8 to 10 months )  . in andervont and dunn 's experience ( 1950b ) the majority of tumours ( 84 per cent ) in hybrids developed at the age of 18 to 29 months and the rest during the first 17 months . 
they also found no correlation between the microscopical appearance of a tumour and the presence of the agent . some of the early appearing tumours in which the agent could not be detected were of type a or b ( andervont , 1945b , 1950a )  . foulds ( 1949 ) described the microscopical appearance of breast tumours in his c57 x riii hybrids as " unmiihlbock ( 1952 ) found the morphology of tumours in c57 x d remarkable "  . hybrids of little assistance in the study of the part played by the agent in the development of these tumours . 
he also noted more unusual features in tumours presumably free of the agent compared with those harbouring the agent , yet the tumours accumulated in later litters of c57 mice following mating to high - cancerstrain males , in which the agent was presumed to be present , had an appearance like that of agent - harbouring breast tumours , in spite of their late average age 108 l . 
dmochowski of development ( 20 months )  . there appears to be a greater variety in appearance of mammary tumours in mice of strains in which the agent could not be detected ( andervont and dunn , 1950a ; 1950b ; heston , deringer , dunn and levillain , in the present study all tumours of type d developed 1950 ; muhlbock , 1952 )  . after 12 months of age . similarly , andervont and dunn ( 1950b ) found this type of tumour to be very rare in younger hybrid mice in which the agent could be detected , although , as shown in this study , this type of tumour even at a late therefore the greater frequency of squamous age may harbour the agent . metaplasia in tumours of old hybrid mice , if the age of 17 months could be considered as a comparatively late age , need not indicate at least in every case their development without participation of the agent , contrary to the previous sugthere is no doubt , however , about the greater gestion of kirschbaum ( 1949 )  . frequency of squamous type tumours in agent - free high - cancer - strain or susceptible mice ( gardner , 1947 ; heston , 1948 ; heston , deringer , dunn and levillain , 1950 ) than in similar mice with the agent , but they do appear occasionally in agent - carrying strains of mice as observed by dunn ( 1945 ) , andervont and dunn ( 1950b ) , and in the present study . from these observations it may be concluded that no particular microscopical appearance of mammary cancer in hybrid mice can be correlated with the presence or absence of the agent , in spite of the difference in distribution of the particular types in various strains of mice . 
thus a variable but low tumour incidence was reported by andervont and dunn ( 1948a ) in hybrids from reciprocal crosses of low - cancer - strain ( c , i , c57 ) mice and a higher but still comparatively low tumour incidence in the hybrid progeny of low - cancer - strain ( c ) females and agent - free high - cancer - strain ( dba - ) males , in spite of increased hormonal stimulation . 
dmochowski showed a high incidence after mating to one ( c3h ) high - cancer - strain male developed a much lower incidence ( 30 per cent ) when mated to other ( a ) high - cancerstrain males . females of strains with low susceptibility may show similar differences . 
even after the 10th pregnancy of low - cancer - strain females mated to males with and without the agent , these two types of females when used as foster mothers induced a similar tumour incidence in the test mice . 
dmochowski tumour age ( 19 to 25 months ) in both types of hybrids is characteristic and hormonal stimulation was assumed to be the cause of these tumours ( muhlbock , 1952 )  . 
the development of mammary tumours in the descendants of both tumorous and the majority of non - tumorous hybrid progeny ofc57 females which remained tumour - free after mating to agent - carrying males in the present experiments as well as the detection of the agent in the majority of the tumours tested indicate the transfer of the agent by riii high - cancer - strain males . though not all ( 057 x riii ) f1 hybrids developed breast cancer , the transfer of similarly , the agent must have taken place in the majority of the females . bittner ( 1952a ) noted a high incidence of tumours and the presence of the agent in the descendants of cancerous and cancer - free hybrid progeny of certain strain females mated to agent - carrying males . 
the presence of the agent was assumed in mammary tumours which appeared in hybrid progeny of later litters of some c57 females mated to high - cancer - strain ( d ) males ( muhlbock , 1952 ) because of the high tumour incidence , in spite of the late age at which the tumours appeared . 
as a result of this transfer , only few tumours in the hybrid progeny develop early and harbour the agent , while the majority of transfer of the agent tumours develop late without participation of the agent . to embryos , however , appears to be doubtful , because of the absence of the agent in high - cancer - strain embryos ( dmochowski , 1949c ; hummel and little , 1949 )  . the passage of the agent from embryos , should they become infected in utero , is also questionable because of the reported neutralisation of the agent by placenta transmission of the agent in utero would ( hummel , little and eddy , 1949 )  . also contradict the basis of the discovery of the agent itself . 
the increase in tumour incidence in hybrid progeny of later litters ( andervont and dunn , 1949 ; bittner , 1952a ; muhlbock , 1952 ) and the high incidence of tumours observed in the descendants of later litters from hybrid females observed in the present experiments may indicate either a transfer of the agent to females repeatedly mated to agent - carrying males and / or gradual increase in the agent , transferred by mating , during its long latent period under the influence of hormonal stimulation ( repeated pregnancies )  . 
the low incidence of tumours observed in the hybrid progeny of some derivations need not necessarily be interpreted in the same way as the small number of tumours induced in mature mice which had been given the agent , as suggested by muhlbock ( 1952 )  . 
a high incidence of tumours obtained in mature mice of some strains after repeated injections of material containing the agent ( dmochowski , 1945a ; muhlbock , 1952 ) , and a small incidence in mature mice of other strains ( bittner , 1952b ) , indicate that the genetic constitution is the more likely explanation for the different tumour incidences in transmission of the agent by the sperm to lowhybrids of various derivations . cancer - strain females , followed by its transmission to their hybrid progeny in the mnilk of these females ( bittner , 1952a ) , appears to be the most likely way in which the agent gains access to hybrid females , although in females of some strains it may only occasionally take place ( miihlbock , 1952 )  . 
the observation of several generations of descendants of hybrid females can give a clear picture whether the transfer of the agent has taken place or not , as shown in the present study . 
under the same experimental conditions some hybrid females may develop mammary tumours while their litter - mates may fail to show tumours ; their descendants may show a similar variation in their behaviour . thus , the study of the behaviour of the hybrid progeny of low - cancer - strain females , especially of the descendants of later litters of the hybrid progeny , can only decide whether or not the agent has been transferred by the male parent . the observations on tumour development and the presence of the agent in 114 l . 
dmochowsk1 the descendants of the hybrid progeny obtained by mating c57 black straini females to agent - carrying riii strain males , made in the present experiments , appear to indicate an interesting possibility in the agent - host relationship which may be the outoome of gradual mcrease in the amount of the agent or its activation in some hybrid females , while in other hybrid females it appears in quantities large enough to be detected immediately with the development of breast cancer in the first generation of hybrid progeny . this may be on one hand the result of individual variations in the genetic constitution of hybrid females , and on the other hand the outcome of varying quantities of the agent which the hybrid females obtain from their low - cancer - strain mothers mated to high - cancer - strain within the framework of individual differences in the genetic make - up males . and / or quantities of the agent obtained , inbreeding combined with hormonal stimulation also exerts its influence . 
thus we have the situation , encountered in the present experiments , that under the same experimental conditions some hybrid females develop mammary cancer and others ( even their litter mates ) do not show breast cancer ; some of the tumorous females do and others do not reveal the agent ; some of the progeny of the cancerous hybrid females may develop mammary tumours which again may or may not reveal the agent , and other progeny of the same cancerous females do not develop tumours ; the progeny of non - cancerous hybrid females may develop tumours which contain the agent . 
the development of breast cancer in some of the ( c57 x riii ) f1 hybrids only after foroed breeding may be explained by the transmission of small quantities of the agent by at least some of the c57 black strain mothers after mating to riii agent - carrying males . 
the high , although varied , tumour incidence in the progefny of these hybrids may be explained by the origin of these females as well as of their progeny from late litters and therefore an increase or activation of the agent in these litters , enhanced by inbreeding and increased hormonal andervont and dunn ( 1950b ) also observed that under the same stimulation . conditions some low - cancer - strain females developed and others failed to develop breast cancer , and some females with tumours possessed and others lacked the there was also no correlation between the presenco of the agent in these agent . females and its presence in their hybrid progeny , cancerous females with or without the agent giving rise to hybrid progeny with only late tumours apparently without the agent , or to progeny with both early tumours with the agent and late tumours without the agent , although they were litter mates . therefore , again , the presence or absence of the tumour and / or the agent in the mother did not necessarily involve the presence or absence of the agent in her progeny . andervont and dunn ( 1950b ) noted on several occasions among the hybrid progeny with late tumours that their litter mates had early tumours with the agent , and on one occasion a hybrid female with an early tumour harbouring the agent had progeny with either no tumours or only late tumours without the agent , which suggested the disappearance of the agent ( andervont and dunn , 1949 )  . bittner ( 1952a ) also reported on the hybrid progeny of some derivations with low mammary tumour incidence that some of them gave rise to descendants with a high incidence of tumours harbouring the agent . 
thus the variable results appear to be due to variations in the genetic make - up of both the hybrid females and their progeny , which in turn leads to variations in the amount of the agent transmitted . a more favourable genetic make - up may account for an increased amount of the agent and its detection . 
the appearance of mammary tumours in some low - cancer - strain females ( c3hb x ax ) mated to agent - free ( c3hb ) males and the high incidence of tumours in their descendants , on the basis of which the presence of the agent was assumed although the tumours were not tested biologically ( bittner , 1952a ) , is one at the moment rather perplexing sudden " de novo " appearance of the agent was therefore also observation . considered as a possible explanation of some of the findings ( andervont and dunn , 1949 ; bittner , 1952a )  . this consideration was based on previous observations of bittner ( 1941 ) on the sudden appearance of the agent in some susceptible ( ax ) mice , deprived of the agent by foster nursing by low - cancer - strain mothers , which remained free of the agent for seven generations , and on similar observations made recently by bittner ( 1952a ) on susceptible mice of another strain ( c3hb ) which remained free of the agent for sixteen generations following foster nursing before the appearance of breast cancer in one of the females , which then gave rise to progeny with a high incidence of mammary tumours . according to the writer 's opinion , these observations of a sudden appearance of the agent may only show the length of time during which the agent may lie dormant or the time required before the agent , originally present in small amounts , increases in quantity sufficient to induce breast cancer in combination with other known and unknown factors . of the known factors , either a change in the genetic constitution of the animal concerned alone and / or increased hormonal stimulus may , at least in part , be responsible for the activation of the agent . bittner ( 1939a ) reported the appearance of some mammary tumours in mice without the agent , and strong ( 1943 ) stressed the influence of hormonal factors in such tumours . 
the difficulties encountered in the detection of the agent in breast tumours appearing late in the life of mice and the comparative ease with which it could be shown in tumours developing early ( andervont , 1950a ) , further the isolated tumours in hybrid progeny of early litters and the accumulation of tumours in hybrid mice of late litters ( miihlbock , 1952 ) , led to the conclusion that there may be two types of mammary tumours in mice . 
one type of tumour would be the result of all three factors taking part in its development , the other type would be the result of hormonal and genetic factors without participation 116 l . 
dmochowski of the agent ( andervont , 1950a ; muhlbock , 1952 )  . however , the possibility of the agent being involved in both types of tumours was not discounted by andervont ( 1950a )  . 
the genetic constitution and intensive hormonal stimulation were considered adequate by heston , deringer , dunn and levillain ( 1950 ) to give rise to mammary tumours in susceptible ( c3hb ) mice , originally derived from mice deprived of the agent by foster nursing , but they also stressed that absolute proof of the absence of the agent from such tumours was lacking . 
the appearance of only a few tumours in the hybrid progeny from reciprocal matings of these ( c3hb ) mice with low - cancer - strain ( c57 ) mice with no evidence of an increase in tumour incidence in the hybrid progeny of later litters , as originally reported by bittner ( 1944 ) in mice of agent - carrying strains or in hybrid progeny from low - cancer - strain females and agent - carrying males , again led heston and deringer ( 1952 ) to suggest that some mammary tumours develop in the absence yet , in hybrid progeny of similar mice of other strains , bittner of the agent . ( 1952a ) observed the appearance of tumours harbouring the agent . further , the agent has been detected in some mammary tumours appearing in comparatively old hybrids , as shown by bittner ( 1952a ) and in the present study . in other late tumours as well as occasionally also in early - developing breast cancers the agent could not be detected by any , so far , employed testing procedures as noted by andervont ( 1950a ) , andervont and dunn ( 1950b ) , and by the writer . thus , intensive hormonal stimulation combined with a suitable genetic background influence the origin of mammary tumours in hybrid mice , increase their there is no doubt that the mammary incidence , and accelerate their appearance . tumour agent takes a part in the development of breast tumours appearing up to a certain age , although not all tumours of early appearance in hybrid mice reveal its presence . 
 ( c57 x ri11 ) f1 hybrid females , obtained by mating agent - free c57 black strain females to agent - harbouring riii high - cancer - strain males , developed a 14 per cent incidence of mammary tumours at an average age of 13 months after bearing in quick succession an average number of 6 - 4 litters . their litter - mates , bred in a normal way , died free of tumours after rearing an average number of 3 litters . 
analysis of parent - offspring correlation in the distribution of tumours in the descendants of the hybrids revealed that the progeny of tumours and of the majority of non - tumorous hybrids had a greater chance to develop cancer if the parent developed cancer than if the parent died without a tumour . 
thus there was a strong indication of the presence of the agent in these hybrids and of its transmission to their progeny , which showed an increasing number of tumours following the combined influence of inbreeding and intensive hormonal stimulation . 
biological tests for the presence of the agent in twenty - three mammary tumours were positive in seventeen and negative in the remainder of tumours . the age of tumours in which the agent was detected varied from 7 to 17 months , and that of tumours in which the agent could not be detected from 8 to 18 months . these tests , combined with the observed distribution of tumours in the descendants of hybrid mice , showed that under the same experimental conditions some hybrids developed tumours which either harboured the agent or failed to reveal it , while other hybrids , even their litter mates , died without tumours . 
some of the progeny of tumorous hybrids failed to develop tumours and others of the same females developed cancer in which again the agent was either demonstrated or could not be shown . 
dmochowski which as a rule developed in older mice above the age of 12 months . there was also no correlation between the appearance of mammary tumours in parents and their offspring . 
calcutt. from the department of cancer research , mount vernon hospital , and the radium institute , northwood , middlesex . received for publication april 16 , 194 ' the question of the involvement of the polycyclic hydrocarbons with sulphydryl groups during the process of carcinogenesis has been under discussion for a ceitain indirect evidence exists and has been reviewed by crabtree long time . ( 1947 ) , who concludes that the available evidence does not warrant any decision as to whether the involvement is direct or not . in other directions mueller and rusch ( 194t3 ) could obtain no effect upon the activity of urease - - this being dependent upon the integrity of the - sh groups - with benzpyrene solution . 
on the other hand rondoni and bassi ( 1948 ) have found benzpyrene to inhibit the papainaise digestion of gelatin and also the cathepsins of rat sarcoma and horse liver . 
the non - carcinogenic hydrocarbons , phenanthrene , anthracene and pyrene , had no action . calcutt and newhouse ( 1948 ) also found that the photodynamic action of benzpyrene was inhibited by cysteine hydrochloride . further work ( calcutt , 1948 ) showed that certain other - sh - containing compounds were also effective as inhibitors of photodynamic action . in the attempt to find the mechanism of this action it was found that after incubation of a colloidal suspension of benzpyrene in a solution of cysteine hydrochloride the characteristic yellow - green fluorescence colour of the benzpyrene changed to preliminary attempts to isolate this blue fluorescing compound were pale blue . unsuccessful , but it was found that the mixture no longer gave a positive test this implied the inhibition of the - sh group of the with sodium nitroprusside . cysteine and formed the starting - point for further work . the inhibition of - sh groups . using colloidal benzpyrene in distilled water , tests were carried out with a in each case the technique was the same . equal aniounts series of compounds . of a solution of the sulphydryl - containing compound were placed in each of two tubes . 
with slightly alkahne nlixtures , however , a small amount of blue fluorescing compound was obtained in solution . for all the cases mentioned above incubation has to be continued for upwards of 11 hours at a temperature of 65 ' c . 
before any inhibition became apparent . at lower temperatures the action was very slow , and at room temperature - 25 ' c . - there appeared to be no effect whatever . prelim ' mary trials having indicated that caffeine solutions had fittle effect upon - sh as detected by nitroprusside , some of the previous experiments were repeated , using a solution of benzpyrene in a 3 per cent caffeine solution . 
inhibition of - sh was achieved as before , but this time inuch more rapidly - 30 nlinutes at 650 c . isolation of the reaction products . under the conditions so far investigated the yield of the pale blue fluorescing product of the reactions has only been very small . nevertheless it has been found possible to isolate products from both the alkahne and acid reaction rmxtures . 
from the alkahne reaction raixture a water soluble compound was derived . this is soluble in organic reagents , strongly adsorb6d to silica , strongly adsorbed to alurnina , fluoresces a whitish - blue colour in ultra - violet light . 
on addition of dilute acid it changes to a blue fluorescing compound which is soluble in organic reagents insoluble in water but soluble in dilute alkali . from the acid reaction mixture a com ound has been separated wliich is soluble in organic reagents , soluble in dilute alka ' li , insoluble in water , adsorbed strongly to alumina and is weakly adsorbed to silica , moving down slowly as elution is continued . thus in their physical properties these compounds show a remarkable similarity to those separated from aninials and designated by weigert and mottrani ( 1946 ) as bpx . , , bpfj aind bpf21 this latter apparently being identical with the compound characterized by berenblum , crowfoot , holiday and schoental ( 1943 ) as 8 . 
furthermore the evidence suggests a considerable parallelism , even if not identity , with the course of events after the introduction of benzpyrene into the animal body . whilst the apparent identity of the fluorescence spectra does not - imply strict cheniical identity , it does mean the very close relationship of the substances concerned . from this it is reasonable to suggest that the interaction of benzpyrene with a - sh containing compound gives rise to a substance of the bpxj type . this , bowever , is in the presence of acid successively broken to compounds of bpfj and bpf2 type . it has already been suggested by crabtree ( 1947 ) that the detoxication of benzpyrene is by way of - sh compounds . in view of the evidence presented above this must now be regarded as being most probable . crabtree ( 1940 , 1944 , 1945 ) has as a result of his work with - sh inhibitors suggested the involvement of sulphur in carcinogenesis caused by the polycyclic hydrocarbons . this is further reinforced by the recent work of lusky , braun and woodard ( 1947 ) , who inhibited the carcinogenic action - of the benzpyrene by application of b.a.l. 
 ( 2 : 3 - dimercaptopropanol )  . additionally , evidence has been put forward by weigert , calcutt and powell ( 1947 ) to the effect that detoxication occurs at the site of careinogenesis . 
modem technique - 3 of microscopy , particularly phase - contrast , by greatly facilitating the study of fiving cells have resulted in greater use being made of tissue cultures for morphological studies . 
when cells migrate from an explant in vitro , they tend to spread out so that around the periphery of an outgrowth they are considerably flattened . this is most obvious in fluid culture media where the cells furthest away from the explant may be reduced to little such cells are ideal for the study of cytoplasmic structure , more than a fine film . as many investigators have realised . 
the necessity of rapid fixation , in order to obtain perfect preservation of chromosome structure has also resulted in the common practice of using squash preparations and smears for the study of nuclear strucsuch procedures possess the further merit of eliminating the possibihty tures . of slight morphological alterations being brought about by the prolonged dehydrating , clearing and imbedding necessary for the preparation of sections . nevertheless ah these methods have the common disadvantage of rendering difficult the correct appreciation of the spatial arrangement of intranuclear structures . in this respect the older method of studying stained sections of fixed tissues presents definite advantages . 
by cutting sections of approximately the same thickness as the average diameter of the cell nuclei , one obtains preparations with whole nuclei and shces of nuclei of varying thickness . 
yet with all fixed preparations of cers there arise doubts as to the validity of the finest structural details which are detectable , especially when they approach the limits of mic ' roscopic resolution . so the results of the study of fixed and stained cells have been correlated with observations made by other techniques , which have included the microscopical examination of living cers immediately after their removal from the animal body . structural organization of the nucleus seen in sections . the ideal type of cell with which to commence an investigation of this kind would be one with a large nucleus , single nucleolus and well - defined chromatin granules . 
most nearly fulfilling these requirements were the cells of a mouse adenocareinoma ( t27 )  . its selection was further influenced by the fact that it had been employed in several previous researches ( ludford , 1924 , 1930 , 1932 a , 1932 b , 1933 , 1934 ) so that the structure of its cells , and their behaviour under a variety of experimental conditions , as well as their growth characteristics , both in vivo and in vitro , were already well known . the same methods of fixation and staining were adopted as were formerly used for the study of chromosomes ( ludford , 1930 ) , except that after iron - alumhaematoxylin staining the differentiation was not carried so far as is usual in making chromos ' ome preparations . frozen sections stained by the feulgen technique were also found most useful . for demonstrating the smallest structural details it is doubtful whether any method can excel the results obtained by flemming fixation followed by intense staining with iron - alum - haematox.ylin when the surface of a nucleus from such a preparation is examined there are to be seen numerous minute granules varying in size . 
4 depicts a slice through the membranes in the process of section cutting . here are seen the same peripheral granules , and also the centre of a nucleus . strands connecting the two nucleoli with the membrane . 
3 , which is another slice from in this one , some well - defined strings of granules are the surface of a nucleus . discernible , while in the adjacent fig . 
the latter obviously represent an early stage in the formation of the prophase ch - romosomes . actually in a section of a rapidly growing tumour it is impo - ssible to determine ex ' actly when the prophase does . 
8 they appear as single threads , and granules are perceptible on some of them . it thus seems that the nucleoli are connected with the periphery of the nucleus by chromosomes , and also by threads of a different nature . frequently the latter appear to be attached distally to a chromosome . examination of prophases at the stage when the nuclear membrane is undergoing dissolution will sometime reveal chromosomes connected with remnants of nucleoli . 
13 represents part of a cell of the same carcinoma on the edge of a 2 - days - old culture , which had been fixed in flemming 's fluid , and intensely stained with iron - alum - haematoxylthe fine peripheral granules beneath the nuclear membrane which are shown in fig . 
16 and 17 , these are projection drawings ( indicated by " p " in the legends )  . there are included in the plane of each drawing bodies distributed throughout the whole thus each drawing constitutes a diagrammatic representation of the nucleus . structures as if they were projected on to the equatorial plane . 
this does not mean none is present , because extremely thin threads might only be visible when coated with dyestuff , and this may have beeil removed in the early stage of differentiating with the iron - aluthe nucleus seen in fig . 
each of the nucleoli is surrounded by particles which appear to have been emitted froin its surface . if observation is now extended to feulgen - stained cultures it becomes evident that the nucleolus is of a dual nature . 
the latter constitutes what caspersson ( 1947 ) has termed " the nucleolar associated chromat - in " and to which he attributes a special role in it can be distinguished from the material of which the bulk protein synthesis . of the nucleolus is composed in the living condition , and in fixed preparations after a variety of staining methods . 
on the basis of the reaction of the two nucleolar components to staining by the feulgen and the pyronine - methyl - green techniques it is concluded that the chromatin is composed of appreciable amounts of deoxyribose nucleotides , and the remainder of the nucleolus of ribose nucleotides . there is considerable variation in the amount of nucleolar chromatin in different cers , as is demonstrated by fig . 
20. in one form of cellular degeneration as has previously been mentioned , particles are discharged from the surface of the nucleolus . comparison of cells stained by the iron - alum - haematoxylin technique , such as that show - n in fig . 
the latter are stained by haematoxylin , but are invisible in feulgen preparations . there are also distinguishable in nucleoli varying numbers of argentophile bodies . page , regan and maccarty ( i 938 ) found that both types of inclusions were more numerous in malignant than in non - malignant cells , and that " the more ma - lignant the neoplasm , the greater the number of intra - nucleolar bodies . " examination of nucleoh with the electron microscope has suggested the existence of a more comphcated structure . 
the hmit of resolution attained with the ultra - violet this is the best resolution represented in microscope is only about 0 - 1 micron . the figures ' illustrating this paper . occasionaby when a nucleolus is highly vacuolated its appearance is rather deceptive , and might erroneously be interpreted as being reticulate . 
one wonders whether the coniphcated internal structure which has been described may be the result of a slight distortion induced by the procedures involved in preparing sections for examination by the electron microscope . 
the vacuolated appearance is not an artefact of fixation as it is visible in hving cells . distribution of nucleic acids in the nucleus . as a matter of convenience , for the purpose of description , it is proposed to refer to the material of which the nucleolus is mainly composed as " plasmosomin "  . 
the nucleolar chromatin contains sufficient deoxyribose nucleotides to stain intensely by the feulgen techiiique , while plasmosomin this does not ehminate the possibility that in the latter deoxyribose does not . nucleotides may be present in such small quantities as to be below the limit of sensitivity of the feulgen techn ' ique , upon the vahdity of which as a tes t for deoxyribonucleic acid this only definitely known chemical difference between nucleolar chromatin and plasmosomin depends . cytogeneticists find it convenient to use the terms " euchromatin " and their usage is based upon the conclusion that at the heterochromatin "  . end of mitosis as the chromosomes uncoil deoxyribonucleic acid remains attached at certain loci ( heterochromatin ) , and is discharged from the rest of since it has been impossible to see whether the chromosome ( euchromatin )  . this actually happens in the cells employed in this investigation no attempt has been made to distinguish between two types of chromatthe term " chromatin " is used in this paper to describe nuclear material which gives a positive reaction with the feulgen test , and which is not visibly connected with the nucleolus . whether one studies fixed and stained feulgen preparations , or ultra - violet micrographs of living cells , it becomes obvious that there must be an increase of deoxyribonucleic acid at prophase , and a corresponding decrease during the evidence has already been adduced that the reconstruction phase of mitosis . chromosomes are represented in the " resting " nucleus by the fine granules at its surface , and on strands connecting the nucleolus with the nuclear membrane . these granules appear to be faintly stained by the feulgen technique . 
but it is doubtful whether any definite conclusion can be justifiably drawn from pale staining , as it has been pointed out , most of these minute particles are just ifthey fail to stain that does above , or below , the liniits ofmicroscopic resolution . not necessarily mean that they contain no deoxyribonucleic acid . it might well be that the amounts present in such small particles would be undetectable by the techni ' que . also very faint staining could result from absorption of traces of diffuse dyestuff . 
the latter usually appears to be very faintly coloured in feulgen preparations , and the nuclear periphery is always most clearly defined there is by comparison an even in the absence of cytoplasmic counterstaining . intense staining of larger peripheral particles , and of others on the filaments connecting the nucleoli with one another and with the nuclear membrane . 
30 is an ultra - violet micrograph of some flattened coagulated nuclei from another mouse carcinoma ( af )  . it will be noticed that the superficial structure is very similar to that draw - n in fig . 
they have been regarded as the chromosomes , or fragments of chromosomes , of the interphase nucleus , but this interpretation of their nature has been disputed by lamb ( 1950 )  . it is highly probable that they are identical with the strands of material exhibiting strong absorption of ultra - violet radiations of 2570 a wave - length , which are seen in fig . 
the absorbing material presumably comprises the fine granules , which for reasons already stated are regarded as representing the chromosomes of the interphase probably their volume is augmented at the time of nuclear coagulation nucleus . as the result of the accretion of additionaldeoxyribonucleic acid from the nuclear sap , by a piocess analogous to that which occurs at the prophase of mitosis . relationship between nucleolar chromatin and plasmosomin . on the basis of the preceding considerations it is concluded that the highest concentration of deoxyribonucleic acid is in the nucleolar chromatin and ' bodies deoxyribonucleic acid is also present in the minute granules derived from it . which represent the interphase chromosomes and in the nuclear sap . considerable evidence has been adduced by other investigators to prove that the plasmosome is particularly rich in oxyribonucleic acid . the functional relationship between nucleolar chromatin and plasmosomin requires furtber investigation . 
the observations that are reported in this paper are consistent with two possibifities . either nucleolar chromatin and plasmosomin are built up from the same simple precursors , and there are altemate pathways of metabolism the 122 r . 
ludford course of which can be deflected so as to lead to the formation of either oiie or or , there are contained in plasmosomin enzynie systems the other substance . responsible for the synthesis of the substances comprising nucleolar chromatin from certain of its chemicary simpler constituents ; or perhaps for breaking dow - n plasmosomin and converting it into nucleolar chromatthe latter notion finds support from the behaviour of the nucleolus during the formation of the chromofig . 
36 and 37 are ultra - violet micrographs of hving prophase somes at prophase . nuclei of a sarcoma ( rb )  . in the former the surface of the nucleus is in focus and the peripheral chromosomes are seen in process of formation . in the latter the nucleoli in the interior of the nucleus are in focus . 
the darker nucleolar chromatin is distinguishable from the lighter plasmosomthe nucleoli are in process of disintegration , and there is a considerable production of nucleolar after the chromosomes are fully formed , small spherical masses of chromatin . plasmosomin are often distinguishable devoid of any chromatat this stage all the feulgen positive material has been deposited on the chromosomes . 
the fonner was photograpbed from a 3 - days - old primary culture of mammary carcinoma ( ad ) in a strain mice ; the latter from a 5 - days - old primary culture of mammary gland from a low - cancerstrain mouse ( c57 )  . 
38 exhibited the greatest degree of polymorphisnote also in this figure the derangement of mitosis which has resulted in two daughter nuclei with numerous karyomeres instead of nuclei . despite the similaritv of the nuclear structure of the cers of fig . 
38 and 39 explants of carcinomata give rise to sheet their behaviour in vitro differs . growths of cells with greater reg - ularity and rapidity than do those of mammary glands . 
the cehs of other mammary cancers induced by carcinogenic compounds , independently of the milk factor , exhibit greater abnormalities , which distinguish them from normal mammary gland cells . there is corresponding variation in the extent to which sarcoma cells differ from fibroblasts with respect to nuclear structure . 
the former is a photomicrograph of a 7 - days - old primary culture of mouse - embryo - heart fibroblasts , and the latter of a 3 - days - old culture of a sarcoma ( aa ) which originated fig . 
34 and 35 mosomin and nucleolar chromatin are included in the drawing . are ultra - violet micrographs of a cell of the same sarcoma , which was the most rapidly growing of the tumours which have been studied in the course of this since all the fig . 
ludford of these the " simplest and rarest type " involved the formation reconstruction . of chromosomal vesicles , or karyomeres . this was " long ago described by biitschli and fol in the blastomeres of segmenting eggs and since observed in embryonic cells of many species.. in this process each chromosome is converted into a small vesicle exactly hke a minature nucleus , the whole group then fusing together progressively so as to form first an irregular , chambered structure and finally a smgyle nucleus . 
from the outer wall of this , apparently , arises the nuclear menibrane , while the inner walls of the vesicles break down irregularly to form the nuclear network "  . 
he considers that the interphase nucleus " probably consists of closely packed , firmly adherent , swollen chromosomes ( chromosomal vesicles or karyomeres )  . " this condition is brought about by the telophase chromosomes swelling to form vesicles whicli adhere to one another . 
each vesicle retains its identity throughout the interphase . " during prophase each chromosome sinks into a dense gel which is separated from its neighbours by the fluid which collects between them . " lewis ( 1947 ) points out that amitosis and nuclear fragmentation would be readily explicable as resulting from the loss of adhesion between chromosomal vesicles . since nuclear formation by the fusion of chromosomal vesicles is said to be speciary characteristic of embryonic cells , it would not be surprising to find the same process occurring in malignant cells which they resemble in many respects . karyomeres are often clearly distinguishable in dividing cancer cells . attention has already been directed to the example in the middle of fig . 
28 and 29 could originate from the cohesion of karyomeres , formed , not as lewis ( 1947 ) suggested , by the swelhng of chromosomes , but by their spreading out over the surface of after coalescence of the latter , the chromosomes would adhere to the vesicles . internal surface of the external walls of the vesicles , which form the nuclear membrane . 
instead of the inner walls of the vesicles breaking down irregularly to form a nuclear network as wilson ( 1925 ) suggested , they would constitute the strands which extend between the nucleoli and the cell membrane . 
to bring ' about such an arrangement it would be necessary to postulate the existence of some mutually repellant force between the chromosomes and the nucleolus at this stage , so that the latter was forced into the centre of the coherent vesicles . from a cursory examination which has been made of different tissues of a number of mammals , including man , it appears that their nuclear structure is essentially the same as that which has been described , but no comparable study has been made of the nuclei of lower animals , or plants . apparently there is a fundamental difference between the nuclear structure of the higher animals and the higher plants . according to the recent work of chayen , davies and miles ( 1953 ) the interphase nucleus of plants ( vicia , allium , zea , tradescantia ) consists of a peripheral zone containing the chromosomes , a middle zone with a protein content , the width of which varies with the state of mitotic activity , and an inner zone occupied by the nucleoli . 
the most striking morphological feature is the manner in which most of the chromosomes are spread out over a spherical area , therebv brinain - a about maximum exposure to the cytoplasm on the outside , and to subsiances emitted from the nucleolus on the inside . 
some of the mitochondria and other granules are applied to the surface of the nucleus , and only clearly , the thickness of its membrane separates them from the chromosomes . substances which penetrate the plasma membrane must pass through the cordon of mitochondria before reaching the nucleus , and between the chromosomes if they are to get to the nucleolar system . in pioneer studies on living cells in tissue cultures , lewis and lewis ( 1915 ) followed the movements of mitochondria backwards and forwards between the nucleus and the cell periphery , and recently pomerat ( 1953 ) has observed rotary movements of the nucleus in epithelial cells growing in vitro . reasons have already been adduced for believing that the mitochondria are involved in protein synthesis ( ludford , smiles and welch , 1948a , 1948b . ) , and attention has been directed to the correlation between . 
hypertrophy of the nucleolar system , proliferation of mitochondria and increased nucleotide content of the cytoplasm ( ludford , 1951 )  . such observations as these tend to emphasise that the cell as a whole is a unified functional system . it is reasonable to suppose that the performance of its fundamental vital processes necessitates intimate correlation of the functional activities of all its organerae . recently brenner ( 1953 ) has deduced from the appearance presented by the nucleus in phase - contrast photomicrographs and ultra - violet micrographs ( ludford and smiles , 1950a , 1950b . ) , and from the results of ultra - centrifugation experiments carried out by himself and others ( beams , 1948 ; claude , 1943 ) that segments of chromosomes are attached to the inner surface of the nuclear mem " these segments maintain their continuity with the remaining parts of brane . the chromosomes which , as uncoiled threads , occupy the inside of the interphase nucleus . " on the basis of caspersson 's ( 1950 ) hypothesis that heterochromatic regions of the chromosomes control protein synthesis brenner ( 1953 ) has proposed that " the nuclear membrane heterochromatin with its specific genes controls the synthesis of equally specific microsomes , each desoxyribonucleic acid directing the synthesis of a characteristic type of ribonucleoprotein "  . " protein synthesis is a two phase reaction " , according to haurowitz and crampton ( 1952 )  . in its first phase , an expanded peptide film acts as a template on which a layer of amino acids is absorbed . 
the peptide film is maintained in the expanded state , its only efficient form , by combining with nucleic acids to form a nucleoin the second phase of protein synthesis , the peptide chain is folded protein . to form ' a three - dimensional globular molecule . haurowitz and crampton ( 1952 ) suggest that the highly specific peptide chains are probably first formed in the nucleus , and that they pass out into the cytoplasm where they are specifically since antigens are deposited mainly in cytoplasmic granules in liver folded . cells it is concluded that the folding of the peptide chains takes place in these granules . 
as haurowitz and crampton ( 1952 ) admit , their evidence that the first phase occurs inside the nucleus is equivocal , while certain of their experimental results indicate that it takes place in the cytoplasmic granules . 
the peptide ffim which haurowitz and crampton ( i952 ) suggest acts as a template in protein synthesis might be locahsed on the surface of the occasionally fibroblasts migrating from explants in tissue cultures mitochondria . leave behind them small pieces of cytoplasm which contain mitochondria and other granules . 
one possible reason for this is that the function of mitochondria is controlled by substances produced by the chromosomes . certain observations also suggest that the latter are dependent upon substances supphed by the nucleolar system . in conclusion , it should be pointed out that cells may undergo malignant transformation without any alteration occurring in their nuclear structure that can be detected by the present methods of microscopy . this is understandable if as has been suggested ( lufford , 1952 ) the cytological basis of malignancy ie ; an imbalance in the genes brought about by processes which result in ( 1 ) the loss of some chromosomes , or parts of chromosomes , and ( 2 ) the intranuclear duphhcation of others . 
this implies that with improvements in microscopical technique it should be possible to distinguish differences between the chromosomes which are spread out on the inner surface of the nuclear membranes of malignant cells and their non - mahgnant prototypes . 
accorcling to caspersson and santesson ( 1942 ) the heterochromatin system of malignant cers is stimulated to abnormal activity . this leads to disturbances in the formation of cytoplasmic proteins and in the reproduction of gene protein , which result in abnormal growth . 
it would be more compatible with the results of the present study if hypertrophy of the nucleolar system and a hyperchromatinic condition of the nucleus were the morphological expression of an increased growth rate rather than being indicative of malignant growth . it has not been possible to identify the nucleolar organizer on the chromosomes of the cells examined during the course of this work . so it remains to be deter ' mined whether increase in size of the nucleolar system is the result of duplication of chromosomes bearing nucleolar orgadizers . there is , however , indirect evidence that this may be the case ( biesele , poyner and painter , 1942 )  . the studies with ultra - violet microscopy described in this paper were carried out in the national institute for medical research and constitute part of a wider 130 r . 
korteweg. from ae antoni vanleeuwenhoek - hui8 , am8terdam . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . it was shown by little et al . 
korteweg ( 1936a , b ) predicted that chromosomal factors must also be active . this prediction was based on the fact that differences in susceptibility to cancer exist between dba females and the fl hybrids of the dba x c57 black cross . 
the present paper concems these chromosomal factors . the fact that chromosomal factors exist is important , but the way they act , their mechanism , is of still greater inter ' est . 
a number of investigators have considered the role of the follicular hormone , and checked the possibility of differences between the oestrus cycles of the high - cancer and low - cancer strains of mice . 
as no differences were found this form of experiment was discontinued . yet i was not convinced . i spayed females of different strains , and afterwards determined the sensitivity of the vaginal epithelium to oestrone by means of the vaginal smear method . i found - that , to cause oestrus , it was necessary to inject three times as much oestrone into females of the high - cancer strain dba as in those of the low - cancer c57 black . 
the ovaries of our high - cancer strain greatly sur ass those of our low - cancer ammals this is partly caused by the somewhat greater num ' ber of graafian in volume . follicles , partly by the much greater number of corpora lutea , and partly by the r . 
hooker ( 1945 ) recorded that the effect of progesterone can be demonstrated in ' the structure of .the endometrial stroma just as well as the effect of i have found that the epithelium of the uterus of the virginal mouse oestrone . also shows a response to progesterone . 
as in the endometrium of the human female , in which on the 17th day of the cycle , shortly after the bursti ' ng of the follicle when the luteinizing process is beginning , a vacuole becomes visible in the basal pait of the epithelial cells , so also this phenomenon occurs in the virginal it is the ' refore necessary to be aware always of the possibilitythat mouse . progesterone too may influence susceptibility to cancer ( by its synergistic ' action with oestrone )  . if the mammary glands ' also of high - cancer strain mice should be relatively insensitive to oestrone , as is the vaginal epithelium of high - cancer strain animals , then the excess of oestrone produced would probably be harmless to the mammary glands . if , on the contrary , the sensitivity of the mammary glands of highand low - cancer strain animals should be the same , the excess of oestrone produced in high - cancer strain animals might be injurious to the mammary glands . it therefore became necessary to determine the 'sensitivity to oestrone of the mammary glands . 
of oestrone into 21 - months - old spayed females of different str ' ains , it seemed evident to van gulik and myself that our high - cancer strain females dba reacted to a lesser degree to oestrone than our low - cancer strain animals when judged by the extent of development of the glands . in 21 - m ' onths - old castrated males injected with 13 i.u. 
of oestrone , we found more growth also in the low - cancer than in the high - cancer miihlbock then drew our attention to the fact that in our experiments strains . we had injected large doses . if one wishes to determine the sensitivit ' y of an organ it is preferable to determine the threshold dose '  . 
as the first visible sign of an effect of oestrone , miihlbock ( 1948a ) took the beginning of budding of the end of the milk ducts ( swelling of the end bulbs )  . 
firstly in the males of the three strains c57 black , dba and 020 , the sensitivity of the mammary gland is about the same according to the threshold test . secondly , the minimal dose causing budding ( swelling of end bulbs ) in castrated males is approximately five times less than in non - castrated males . obviously in non - castrated males the testosterone largely counteracts the oestrone . this supposition proved to be right , as in castrated males which were injected both with oestrone and testosterone , the presence of the latter suppressed the action of the former . in noncastrated males three times as much oestrone is needed to cause budding ( swelling of end bulbs ) in the glands of high - cancer strain dba mice than in those of lowcancer strain mice ; in castrated males the sensitivity is the same . 
anderson. from the research department , glasgow royal cancer hospital . received for publication february 22 , 1949 . the need for controlling the influence of solvents used as vehicles for carcinogenic hydrocarbons was recognized by burrows , hieger and kennaway ( 1932 ) , who reported experiments designed to test the fat solvents then in use for this pui - pose , for possible carcinogenic action on the connective tissues of rats and subsequent work showed that in fact lard , which had been previously mice . heated to 140 ' c . , was a potential carcinogen for the connective tissues of fowls ( peacock , 1933 ) , and that lard alone could give rise to spindle - cell tumours in rats ( barry and cook , 1934 ) ; and later that lard , olive oil ' and other fatty materials could induce connective - tissue tumours , some of which appeared to be malignant in rats , but not in mice , in the experience of burrows , hieger and kennaway ( 1936 )  . the first instance of undoubted sarconia induction at the site of the injection of lard in fowls cited above was complicated by the fact that the same birds had been injected with a solution of 1 : 2 : 5 : 6 - dibenzanthracene in lard in the right breast and with lard alone in the left breast . 
of incidentally these tumours in a susceptible bird cannot be excluded . experiments suggest that the quantity of dibenzanthracene actually required to initiate sarcomatous growth must be remarkably small , since the bulk of the the injection appears to remain encapsulated throughout the expei - inient " ( peacock , 1933 )  . 
the latter assumption subsequently proved to be wrong . to test this point , chalmers ( 1934 ) analysed the contents of encapsulated niatter from the site of dibenzanthracene lard injection in one of peacock 's sarcoiiia - bearing fowls , which died 7 months after the last injectioii . 
dibenzanmoreover , in this group no tissue reaction thracene in 0 - 4 per cent solution . could be found at the site of injection after a few months , indicating that the homologous fat had caused httle disturbance . however , with egg yolk fat as vehicle for dibenzanthmmne m 0 - 4 per cent solution , 2 metastasising sarcomas occurred among 4 birds that s ' urvived 9 months or more after injection . birds inject - ed with yolkfat showed fibrous cysts at the site of injection , sinular t - 0 those observed in the lard experiment , and in contrast with the absence of such local reaction in birds injected with chicken - fat . there seemed , therefore , to be some aetiological connection bet - w - een the " foreignness " of the solvent used as vehicle and the local tissue reaction and the ultimate carcinogenic response t - o dibenzantli - racene . owing to the costlv and time - consuming nature of long - term experinients on fowls work was begun on similar lines on mice . while these experiments were in progress berenblum ( 1938 ) reported the co - carcinogenic action of croton oil . he had previouslv shown ( 1929 ) that mustard gas in dilute solution and ( 1935 ) cantharidin had anticarcinogenic properties for the skin of mice , and in the interim had found that no simple relationship between irritant and coor anticarcinogenic action was demonstrable . 
olive oil , tended to retain the dissolved benzp - % - rene as judged by the persistence of violet fluorescence , where - as in the case of those that were rapidlv absorbed , e.g. 
mouse fat or ether , fluorescence could not , be detected after a few weeks ( peacock and beck , 1938 )  . moreover , in the fornier group the incidence of sarcomas was high , and in the latter group it was low . this suggested that there mav be an optimal period for the retention of a carcinogen at the site of injection for the induction of a tumour , and that in mice this period was about a months . dickens and weil - malherbe ( 1942 ) at first confirmed our observation with mouse fat ' , but later ( 1946a ) , as a result of intensive experiments , found that the effect was not constant and was related to the phospho - lipid content of the 298 p . 
the mice were killed after different periods ( table 1 ) , the subcutaneous tissues exposed and examined for ultra - violet sixteen of 20 mice killed at various times over a period of 7 months fluorescence . had fluorescent material located at the original site of injection ; ulceration and sepsis at the site of injection killed 4 mice early in the experiment . in 3 of these mice no sign of the injected material was found , probably due to sloughing and leakage from the site of injection . 
the fourth had a small spot of fluorescence . these mice were not examined further ; in the remainder the fluorescent material was extracted with benzene , with the exception of 2 mice , which died after 412 - and 51 months , both showing persistent fluorescence and tumours at the site of injection . after the third month of experiinent tumours began to be clinically recognized at the sites of injection . as most of these tumours were similar to many such induced sarcomas in mice , not a 11 were histologically examined . 
one tumour in the abdominal cavity associated with intraperitoneal deposits of fluorescent material was probably induced by benzpyrene injected accidentally through the abdominal w , - , 11 . another tumour occurred in an ulcerated area at the site of injection . this proved to be a squamous carcinoma . 
benzene , and the benzene extract dried over anhydrous sodium sulphate . since the main object of these experiments was to demonstrate the pre - sence vne after various periods , the experiments were not conor absence of benz ducted quantitatively . however , the limit of sensitivity of the method of detection provides some indication of the quantities involved ( vi& infra )  . 
to eliminate the possibihty of a false positive reswt due to traces of benzpvrene adhering to the apparatus used in the experiments , benzene washings of each piece of chemical apparatus or other instrument used , were examined under the ultraviolet lamp imniediately before its use . attention was drawn to the necessity for such precautions ri_ - , cently ( anderson , 1947a )  . 
owing t - o the difficulty of eliminating minute traces of material from apparatus , such traces may be recorded by the fluorescence method of detection , and lead to a false positi ' ve result . 
the absenee of benzpyrene from extracts of two tumour - bearing mice killed - 4 months after a siiigle injection of benzpyrene does not preclude the possibilitv that the uneliaiiored hvdrocarbon was still present at the inception of the tuiiiour process as it was in tfie other tumour - bearing animals killed after shorter periodss . thus the results of this experiment accord well  . , a - ith otir previous observations ( peacock and beck , 1938 ) that when fluorescence remained at the site of injectioii in iiiiee for 5 months or more there was a hiah incidence of sarcoma . 
on this basis dickens ( 1947 ) states that " the surprising result was obtained that the more rapid elimination of benzpyrene was associated witli the higher carcinogenic activity , and slower elimination mith lower acti - 6ty . " fact the graphs published bv dickens and weil - ' - nlalherbe ( 1946b ) show . 
in the case of tricaprylin alone , and of tricaprylin plus phospholipids as solvents for benzpyrene , a consistent rate of elimination of the hvdrocarbon from the sit ' e of injection , but not to the point of extinction within s5 davs and 10 - 10 davs extrapolation of the tricaprvlin graph would in&ate total etim " lrespectively . nation in the region of 26 weeks . as w out of 26 mice had tumours bv the 20th week , it seems reasonable to , suppose , that some benzpyrene was present in these mice throughout the latent period of careinogenesis . this would correspond closely with our own experience . in the graph illustrating the course of events following injection of benzpyrene dissolved in tricaprylin plus 3 per cent choleste , rol , dickens and weil - malherbe ( 1946b ) show a considerable variation in the persistence of benzpyrene in different mice . 
as no t - umours were recorded before about the 19th week of their experiment , there is no positive evidence about the persistence or absence of benzpyrene at the site of injeetion in their tumourbearing mice . ou - r own repetition of their experiment . 
anderson mice , and must therefore have been present throughout the latent period of carcinogenesis . while it seems certain that partition of benzpyrene between the solvent used - is vehicle and the body fluids must be largely responsible for the rate of elimination of benzpyrene , the local tissue reaction to different solvents may also help to determine the local response . 
they established that for benzpyrene the partition coefficient between human sera and various lipoid solvents was directly related to the carcinogenic response of mice injected with benzpyrene dissolved in those solvents that readily parted with benzpyrene in vitro gave fewer solvents . ttimours when used as vehicles for injection of benzpyrene in mice . their conclusions support the conception that there is a significant relationship between the retention at the site of injection of benzpyrene and the ultimate carcinogenic response . whatever may be the essential mechanism of conversion of a normal cell to a malignant one , it seems certain that some local consumption of energy by some part of the cell must be involved in the transformation . it may well be that the liberation of energy at the optimum time in the life - cycle of a stisceptible cell is the essential carcinogenic stimulus , and this may be provided by the metabolism of a carcinogen . in this event neither the parent hydrocarbon nor its metabolites , but the transition from one to the other , may provide the essential carcinogenic stimulus . 
kreyberg spondence is established between the patient group and the control material with regard to such factors as age and sex composition , distribution of broad occupational groups and place of residence , which may influence smoking habits and / or lung cancer frequency , and a large number of factors clearly may be considered irrelevant , a field of uncertainty of considerable extent still remains . two points of practical importance emerge from the above discussion . 
the first is that control material consistin - g of non lung cancer cases among patients in a chest department , or even among hospital patients generary , may introduce a bias if , for instance , the factor " visiting a chest department for reasons other than lung cancer " - present in a control material but not among the lung cancer patients - is associated with the level of tobacco smoking . there may thus be a tendency towards excessive smoking in such a control material , or patients in chest departments may on the contrary tend to be persons whose reaction even to mild forms of chest trouble is a visit to the hospital , and who are careful if both these tendencies not to expose themselves to irritants sucli as tobacco . are present among the patients , they may neutralize each other , but the net result will obviously depend on their relative occurrence in the control material . similar objections may be brought against the use of hospital patients generally this point has been stressed by mirs and porter ( 1953 ) as control material . who believe that the bias probably wfll obscure an excess of smoking among lung cancer cases . 
at least , it is not established that hospital patients do not differ systematically from the general population with regard to smoking habits . the second point to be made is that a careful survey of all possible cancer producing factors must precede the instigation of a control study , and that prehminary surveys are needed to estabhsh the relationships between these factors and the level of tobacco smoking . there is thus a priori reason to consider the need for relevant definitions and differentiation of occupational groups among the cancer patients as well as in the control material , in view of the frequently indicated possibilities of specific occupational hazards with respect to lung cancer . assume , for instance , that a particular type of industrial occupation has a definite but unrecognized excess incidence of lung cancer , and that the carcinogenic agent is connected with the nature of the work . 
assume further that this particular occupation also is associated with an excess of tabocco smoking , because of higher pay , better opportunities of smoking during working hours , psychological stress or other causes . if the occupational selection criteria are such that this occupation does not exphcitly constitute a stratum in the control material it may be under - represented in a control material with random selection within each stratum , and the controls may , for the separate occupational groups and in toto , show a lower smoking level than the cancer such a difference will clearly be misleading for an evaluation of patient group . the carcinogenic effect of tobacco smoking . if , on the other hand , the particular occupation in our example is associated with an exceptionally low smoking level , a possibly significant excess smoking in the cancer patient group may be obscured . 
kreyberg composition of tobacco consumption are available only after 1927 . since then , tobacco smoked , i.e. , cigars , cigarettes and pipe tobacco , has accounted for a steadily increasing proportion of the total tobacco consumption at the expense of chewing tobacco and snuff , as shown in fig . 
the amount smoked is here calculated as production plus imports minus exports of cigars , cigarettes and pipe tobacco . these changes will year to year inventory changes have not been corrected for . be small , however , and without influence on the trend even if the vearlv figures may contain erratic deviations from the true consumption level . it should be permissible to assume that chewing tobacco and snuff played a greater r ' ole before 1927 . 
even if some of the chewing tobacco in fact has been smoked in pipe , it is reasonable to assu ' me that the amount of tobacco smoked , per person 15 years and older , has increased to some extent during the whole period from 1901 to 1940 . 1800 1600 1400 1200 1000 11 1% in600 1928 year fig . 
2. - consumption of smoking tobacco in granis per person 15 years and older . 38 39 after the last world war the yearly amount of tobacco smoked , i.e. , cigars , cigarettes and pipe tobacco , has reached a level of approximately 1650 g . 
3 for 1928 - 29 , 193 7 - 39 and the post - war years . the black parts of the columns represent the proportion of ready made cigarettes , which was 34 - 7 per cent in 1928 , rose to 42 - 9 per cent in 1947 and has since declined to 35 - 8 per cent in 1951 . 
patients , ear - nose - throat department , the rikshospital ( whole country ) kongsberg is a smar industrial town in central southem nor - way , s smar industrial and mining commuiiity ( iron - ore ) in the extreme north . varanger ( kirkenes ) a in the groups 1 , 3 , 4 and 5 among the males and 1 , 2 and 3 among the females the number of returned questionnaires falls substantially short of the total number of individuals in the groups selected . 
the age distribution of the separate groups is given appendix tables iii and iv . incidence of each of the forowing were computed . each of the above - mentioned groups were divided into age - classes with a for each group and age - class the percentage for males : 1 . 
4 is shown the range of variation found for the frequency of smokers in each age - class among the groups investigated . it will be noted that this range is fairly narrow , especially in the age - class 45 - 54 years in which the lowest percentage smokers ( found among the visitors at the oslo first aid station ) is 83 - 5 and the highest ( among industrial workers , oslo ) is 91 - 9 . 
the latter group , on the other hand , reaches its highest frequency at a i ' ater age than most of the other groups . generally the percentage smokers is lower among industrial workers in kongsberg , than in the other groups . per cent pure cigarette smokers . 
5 we find a very wide range of variation for the occurrence of pure cigarette smokers in the material , especially in the lower age - classes . among the industrial workers in kongsberg in the age - class 25 - 34 years only 28 - 4 per cent smoke cigarettes exclusively , whereas 75 - 9 per cent of their colleagues in s6r - varanger do so . 
6 is similar to that found for the percentage pure cigarette smokers , but the level has been shifted upwards and the range is a little less wide , corresponding to the tendency for the cigarette - pipe smoker combination to be more frequent in groups with relatively few pure cigarette smokers than in those with a high pure cigarette smoker percentage . 
8 the range of variation in the percentage medium and heavy smokers is large in all age classes , but the frequency does in no case exceed 50 per cent . 
12 is very rare among women , occuriing only among physicians and the patients and followers at the oslo first aid station , in the age - classes 35 - 54 years , with frequencies ranging from 1 - 4 per cent to 2 - 3 . per cent heavy and medium smokers . 
how much of this variation is real , i.e. , caused by actual differences in smoking habits in the groups under consideration , and how much may be caused by a systematic bias in those groups whose degree of co - operation in retur ' n ' mg questionnaires was low , cannot be decided on the basis of available inforrnation . 
the question is of considerable interest however , since for most of the smoking habit criteria , the range of variation among males would narrow considerably if the figures for the industrial workers in kongsberg are left out . this group comprises questionnaires from only a part of the total number of workers in the arms factory selected for analysis , and ff it could be shown that the degree of co - operation in this group is systematically related to smoking habits , the deviations shown would not reflect a true difference in smoking habits between these factory workers and the other groups . there are , however , certain indications that part of the difference at least between the kongsberg workers and the other male groups is real . first of all the percentage smokers in this group ( appendix table v ) are not substantially below those of the other groups . 
even if there is a tendency for smokers to be under - represented among those workers who answered the questionnaire , such a bias can not account for the very low percentages pure and pure and mixed cigarette rsmokers found in the kongsberg group , and is not likely to expla ' entirely the low percentages found for the quantitative criteria ( per cent heavy and per cent heavy and medium smokers )  . secondly , groups other than the kongsberg workers have failed to co - operate fully , without any resulting systematic deviation from the complete groups . 
an explanation of the result for the kongsberg group in terms of a systematic bias , would thus imply that this bias was a characteristic of the kongsberg workers but not of the others . thirdly , the material from the male physicians seems to indicate that there is no strong tendency that individuals who fail to fir a questionaire deviate appreciably i their smoking habits from those who co - operate readily . 
a new questionnaire was sent out approximately a year later with an appeal to those who had not answered previously this appeal resulted in 601 new questionnaires which were to do so now . analysed separately , however , the two groups showed added to the old material . the following figures for the separate smoking habit criteria . there is thus cause to believe that the range of variation found in the material largely reflects real differences in smoking habits . special menti ' on may be made of the male group of patients at the rikshospital ear - nose - throat department which displays exceptionally low percentages heavy and heavy and medium smokers ( both generally and cigarette ) in the lower age - classes and rather high percentages in the higher age - classes . the material is , however , too small to permit any conclusion as to whether or not this reflects a characteristic pattem in this group . conclusion as was pointed out initiahy , the present study has been undertaken in order to provide background information on factors which must be taken into conh . 
the present study may serve as a basis of comparison with the smoking habits of lung cancer patients , in the sense that findings generally outside the range of variation exhibited by the present material would be indicative of real deviations in the smoking habits of lung cancer patients , but quantitative statements about differences found cannot be inferred . the low frequency of smokers in the higher age - classes among most groups of women may indicate that the increasing trend in total tobacco consumption h . 
fibroid with advanced sclerosis ; patch of oedematous tissue ' probably smooth muscle fibres ; proliferation of vascular endothelium ; invasion diahypertrophic endophragm ; thelium on the surface of the tumour . . 
the peripheral belt of fibroblasts originating most probably from subendothelial cells of the serosa and so characteristic of the oestrogeninduced abdominal fibroid ( lipschutz , 1942 ) was present in a diaphragmatic tumour belonging to the animal of fig . 
as with the abdominal fibroids we have described formerly , there were in thoracic tumours also some cells resembling there was a proliferation of the cells of the wall of vascular smooth muscle fibres . spaces ; there was an hypertrophy of the endothelium at some places on the there was invasion of the muscular tissue of the diasurface of the tumour . phragm , or the thoracic wall , by the tumours . 
but there were in this tumour also accumulations of cells resembling fibroblasts which seemed to originate from the proliferation of the subendothelial cells of the wall of vascular spaces , or the endothelium proper . 
the tumour was covered by various layers of flattened cells . there were besides the animals described , 4 females and 2 males in which small nodules just visible to the naked eye were found on the surface of the only 2 animals of this group have been examined lung or on the parietal pleura . microscopically ( table i ) and in one of these a tiny fibrous nodule was found on the surface of the lung ; the structure of this nodule was identical with that of similar oestrogen - induced nodules of the abdominal serosa . 
note thickened border of opening in the diaphragm , prolapsed liver and intestine . fibrous reaction also on the right though the opening is on the left . small nodules on the pericardium in lxiii . 
the tablet occupied in some cases a retrosternal or mediastinal position ; it was surrounded by a thin capsule and in other cases the capsule adhered to the costal serosa , thin fibrous strands . where the fibrous reaction around the oestradiol tablet was more conspicuous . but there was not a single animal with thoracic tumours in this group . 
lipschutz oestrogen - induced thoracic fibroids increased very considerably ; thoracic fibroids in 7 out of 18 animals with such a communication . there were in most of these animals part of the liver and of the intestine prolapsed to but the mechanical stimulus due to this accident was the thoracic cavity . seemingly not responsible for the increase of the incidence of oestrogen - induced this was shown by the fact that in 24 animals without an thoracic fibroids . abdominal - thoracic communication the capsule enveloping a foreign body introduced in the thoracic cavity ( metallic tablet or a tablet of oc - oestradiol ) did not , or only exceptionally , become surrounded , under the influence of the oestrogen , by a fibroid as was the case with a similar foreign body ( metallic tablet ) introduced in the abdominal cavity of these animals . the above experimental results suggest that the oestrogen - induced fibrous tumoral reaction of the peritoneum in the guinea - pig is mediated by an internal ambiental factor normally present in the abdominal serosal fluid , or a factor originating under the influence of the oestrogen and given up to the abdominal it is seemingly the absence of this mediating factor which protects the cavity . animals against production of fibroids in the thoracic cavity . aided by grants from the the jane coffin childs memorial fund for medical research . 
lipschutz. from departmento de medicina experimental , servicio nacional de salud , avenida irarrdzaval 849 , santiago de chile . received for publication february 2 , 1953 . the behaviour of the intrasplenic ovarian graft in the castrated guinea - pig has been studied in this department since 1942 . the graft shows two particularities : blood follicles which may appear as early as 3 weeks after transplantation and at 2 months are frequently cystically enlarged ; and small nodules and cords of luteal cells , i.e. , of eells whieh resemble those of corpora lutea , scattered in the ovarian stroma . 
later gn , at say 10 months , the graft consists , predominantly , of very large corpora lutea embedded in irregularly shaped masses of cells similar to those of corpora lutea ( ponce de leon , 1944 ; woywood , 1944 ; lipschutz , 1946 ; lipschutz , ponce de leon , woywood and gay , 1946 ; iglesias , lipschutz and mardones , 1950 )  . 
the condition has been termed by us as luteomatous . the luteal cells originate partly from small follicles whose theca - in some cases , but in a minor degree , possibly also the granulosa - undergoes precocious luteinization , and partly , according to our evidence , from cells of the stroma . blood follicles and graafian follicles were still present at 10 and even 20 months . on the contrary , blood follioles fail to appear in the intrasplenic graft when the seoond ovary is left in situ ( gay , 1944 ) or grafted into the kidney ( ramirez , 1950 )  . 
they appear only exceptionally when a minute ovarian fragment is left in situ ( gay , 1944 ; niedmann , 1947 ; bruzzone , lipschutz and niedman.n , 1952 ) , whereas they invariably appear when both ovaries are grafted into the spleen ( ramirez , 1950 ; ramirez , iglesias , mardones and lipschutz , 1952 )  . there is thus full evidence that the whole gamut of atypical changes , including tumourigenesis , is due to the hypophysial gonadotrophic activity not duly controlled by ovarian hormones , the latter having been inactivated to a considerable degree in the liver . the luteomatous or tumoural structure described in the guinea - pig is different from that in other laboratory animals . granulosa - cell tumours and luteomata appear in the intrasplenic graft in castrated rats ( biskind and biskind , 1944 , 1949 ; van lancker and maisin , 1950 ; lacour , oberling and guerin , 1951 )  . mice granulosa - cell tumours are more prevalent than luteoma ( li and gardner , 1947a , 1947b ; li , 1948 ; furth and sobel , 1947 )  . metastases may occur in mice and the tumour is transplantable ( li , 1948 )  . 
in there but haeinorrhagic follicles were present in all the growth of nipples and uterine growth . one of these animals there was a luteoma . t in the animals of this group tiny pellets containinig 40 per cent . 
15 - the graft divided into two halves - could be due to proliferation of capsular endothelium ? in several cases we found a zone of necrotio appearance between the fibrous capsule of the graft and the splenic tissue , possibly due to luteal tissue invading the spleen and undergoing necrosis after a period of more or less abundant proliferation . rupture of the capsule is possibly not the only route by which invasion is in fig . 
23 what seems to be splenic tissue was found in the loose part of the ovarian stroma which corresponds to the hilus of the ovary . we have not seen metastases in our work in the guinea - pig . 
bartholomew 's hospital , london , e.c.1. received for publication january 12 , 1949 . thie carcinogenic activity of ethereal extracts of domestic soot was demonstrated by passey ( 1922 )  . domestic soot may contain as much as 40 per cent of tarry matter ( cohen and ruston , 1925 )  . 
the use of the fluorescence spectrum by mayneord and hieger led to the identification of 3 : 4 - benzpyrene in gas - works pitch ( cook , hewett and hieger , 1933 )  . this discovery suggests that this hydrocarbon might be one of the carcinogenic agents in domestic soot , although the conditions of pyrolysis in the domestic hearth , and in the gas - works retort , are different . berenblum and schoental ( 1947 ) found that carcinogens other than 3 : 4 - benzpyrene were present in coal tar . 
the first attempt to identify 3 : 4 benzpyrene as a contaminant of the atmosphere was made by hieger ( 1946 ) , who exposed non - fluorescing benzene to the air in london , and found that the fluid became fluorescent and showed spectral bands resembling those of benzpyrene . 
for the present purpose , samples showing a ph value of 10 - 0 - 10 - 3 were found to be most suitable . 3 : 4 - benzpyrene . - the commercial product contains a pale - blue - fluorescing impurity which is very strongly adsorbed on alumina . 
benzene. the first attempts to separate benzpyrene from soot were based on the method described by berenblum ( 1945 ) for the extraction of benzpyrene from coal tar . in the original method vacuum distillation of the suitable fraction of tar was followed by solution of the distillate in concentrated sulphuric acid . attempts at vacuum distillation of benzene extracts of soot showed , however , that the composition of the soot extract was very different from that of coal tar . 
evaporation of the benzene extract yielded a residue consisting mainly of non - volatile material , which appeared to decompose on distillation in vacuo with evolution of gas . direct sulphuric acid extraction of the crude tar extracted from soot was also unsuccessful , probably owing to considerable sulphonation . moreover , recovery experiments , with microgram quantities , of pure benzpyrene from icecold sulphuric acid showed that considerable loss of the hydrocarbon occurred , and that the method was useless as a quantitative one for such small amounts . chromatographic adsorption was next tried . 
when an extract of soot was submitted to chromatographic separation , the characteristic fluorescence spectrum experiments with various of benzpyrene was given by the appropriate eluate . samples of alumina showed that spence 's type h alumina , containing adsorbed benzpyrene , could be washed freely with a mixture of benzene - petroleum ether ( 1 : 10 ) without elution , and that the benzpyrene was eluted only when the proportion of benzene was increased ( 3 : 10 )  . 
the extract was given a preliminary purification by passing it through a short column of alumina ( 14 x 25 mm . ) and eluting with the same mixture of solvents . 
the lower band was easily eluted with benzene - petroleum ether ( 1 : 10 ) , while the upper could only be washed down when the benzene content of the eluting fluid was increased ( 3 : 10 )  . this latter fraction is shown in fig . 
lane. from the department of pathology , royal cancer ho8pital , london . received for publication june 7 , 1952 . scepticism is a healthy response to diagnosis of any tumour as angiosarcoin ' - 11 . to dispel all doubts , full necropsy and thorough histological exaniination of all lesions with indisputable evidence of the vasoformative natuire of the tumour and proof of metastasis are essential . 
many lymph nodes in the cervical regions , supraclavicular fossae and posterior triangles were enlarged ( up to 2 - 0 cmain diameter ) , soft , dark red and cystic . 
on the surface and in the substance of both lungs were numerous discrete , firm , red , spherical nodules ( up to 3 - 0 cdiameter ) whose cut surfaces resembled blood clot . other parts the paratracheal and mediastinal lymph nodes of the lungs were oedematous . were greyish - black and slightly enlarged . 
the common bile - duct was dilated and contained several small pigment calculi . the spleen was small , and on its surface was a cyst ( 1 - 2 cdiameter ) containing clear fluid.. 
the nuclei are pale - staining , vesicular and variable in size : in shape 's.pherical , ovoid or indented . mitotic figures are few , but within such aggregations capillary channels are forming by separation of the cells . 
he interpreted his case as a benign angioma producing metastases , and separated it sharply from a case described by theile ( 1904 ) in which all the lesions showed sarcomatous areas . his interpretation is not acceptable in pathology , and the histology of the lesions in shennan 's ( 1914 ) case was no less benign , yet penetration of a pulmonary vein shennan suggested that our criteria of malignancy were at fault in was found . regarding such lesions as histologically benign . 
livingstone and klemperer ( i 926 ) concluded that the lesions in these cases were not as benign histolozicallv as the authors believed , and they thought that all showed atypical areas suggestive of malignancy . stout ( i 943 ) confirmed this , and considered the same applied to the original lesion in robinson and castleman 's ( 1936 ) case . however , in this connection it is well know - n that other malignant tumours and their metastases sometimes show deceptively benign histological appearances ( e.g. , chondrosarcoma and carcinoma of prostate , thyroid or kidney )  . the present case seems to be of the same nature as these and , in addition , has fe ' atiires similar to some others in which the histological structure was more malignant . kettle ( 1918 ) described an angioblastic tumour of the leg with metastases in the inguinal lymph nodes , ulrich ( 1921 ) a similar tumour of the lumbar muscles with metastases in the lungs , and downing and manory ( 1930 ) multiple angiomatoid lesions appearing in successive crops over an area which had been bumt some months previously . in the last two cases intravascular extensions were present , which strongly suggests that the lesions other than the primary mallory ( 1 914 ) , however , states that some caverwere blood - bome metastases . nous haema - ngiomas - not only arise in veins but permeate their wa ' ils and , at various placeg , rupture them , infiltrate the tissues and produce lesions which , while simulating metastases , are , in reality , in contiguity . this must be unusual , and would clearly be an incorrect interpretation of some of the cases cited where the lesions are far apart and particularly where peripheral lesions are associated with pulmonary ones . 
on the other hand , if benign angiomatous lesions extend into the lumina of veins , it cannot be concluded from observing intravascular extension alone that multiple lesions are metastatic rather than multifocal . in the present case , however , tumour tissue , not in cont ' lguity with large masses , is demonstrable within pulmonary vessels and , of special interest , witbin perivascular lymphatics and afferents to cervical lymph nodes . 
the only acceptable explanation of such findings is that the lesions in the cervical lymph nodes and lungs are embolic metastases . this case does not appear to shed any new light on those angiomatous conditions having a " system " distrib - ution described by theile ( 1904 ) , jores ( 1908 ) , wright ( 1928 ) and de nava , squez ( 1936 )  . in all these the authors described primary angioblastic tumours of the spleen with metastases in the liver . in theile 's case there were additional lesions in the lungs and stomach . willis ( 1948 ) , while c ' onceding these authors ' interpretations may have been correct , points out the possibility of the lesions in their cases being multifocal in origin . evidence suggestive of such cases being malignant metastasizing neoplasms ( local infiltration , poor differentiation , mitoses and intravascular extensions ) is not sufficient to classify them , witb certainty , as such . 
tumour tissue was found within perineural lymphatics of the scalp , in the afferent lymphatics of cervical lymph nodes ' and within pulmonary blood - vessels . i am indebted to j . 
a. - ( 1934 ) ' the spread of tumours in the human body , ' london ( chiirchill ) , p 148 . - ( 1948 ) ' the pathology of tumours , ' london ( biitterworth ) , p . 
at that time research into their pharmacological and toxicological properties showed that certain of their effects were strikingly similar to those of ionizing radiation ( gilman and philips , 1946 ; kamofsky , graef and smith , 1948 ; philips , 1950 )  . this led to further investigations of their action as mutagenic agents and as growth inhibitors and their importance in these connections quickly became apparent . 
tumours were selected for treatment on the 6th or 7th day after implantation . the standard dose level adapted as the basis for comparison of chemical and x - ray effects was 1 mg . 
casarini analyses showed that 200 r might be considered to be an " equivalent " dose , i.e. , it produced in tumour and bone marrow the same amount and the same type of cellular injuries up to 24 hours after administration ( koller , unpublished )  . 
body weight throughout the experiments . for cytological analysis small pieces of tumours were fixed in acetic alcohol mixture ( 1 : 3 ) , and squash preparations were made and stained with feulgen 's for histological study fragments were fixed in bouin 's solution , basic fuchsin . embedded in paraffin wax , and sections cut at 5 . 
were stained with haematoxylin and orange - g . cytological effects : method of analysis . the method used for estimating cellular injuries is the same as was employed by devik , elson , koller and lamerton ( 1950 )  . cells in post - metaphase stages were selected . 
the importance of some biological variables ( age , sex , diet , etc . ) has already been discussed ; devil and coworkers ( 1950 ) demonstrated by analysis that the data , obtained by the same method as used in the present study , do in fact provide a valid basis for comparison . but as will be seen , the effects observed 72 hours after treatment by x ray and hn2 were in any case qualitatively so different that they could not be compared on a quantitative basis . x - ray effects : localised treatment ( 200 r )  . the tumours only were irradiated and cytological effects were analysed at 6 , 12 , 24 , 48 , 72 , 96 , 120 , 144 and 168 hours after treatment . 
date when the animal was killed . this is also the sample in which the number of chromosome fragments per cell is at a maximuthe damage is less 24 hours after irradiation , and it diminishes further in the 48 and 72 - hour samples . in tumours 4 to 6 days after treatment the number of dividing tumour cells with abnormalities is very small . our observations indicate that 200 r is insufficient to inhibit the growth of the walker carcinoma ; the growth rate of treated tumours 6 days after irradiation was found this finding is in close agreement with that to be the same as that of the controls . of devik and co - workers ( 1950 )  . hn2 - induced cytological effects . it has already been reported by the senior author that a dose of 1 mg . 
by including such cells in the analysis , the true number of injured cells is reduced ( compare the 144 and 168 hour samples , table iib )  . ' 0060 - / time after treatment in hours fig . 
they are particularly evident in young tumour implants and are found in large numbers at the periphery of growalthough these cells are normally present in the walker carcinoma , ing tumours . they play a small part in the histological organisation of the tumour . 
the great and rapid increase in histiocytes after hn2 administration , which takes place in the cellular tumour parenchyma , has important consequences . table iib shows the drastic change which occurs in the cell composition of the tumour . 
the proliferation of those tumours cells which may recover from nuclear or cytoplasmic disturbances was found to be seriously hindered by the altered environmental conditions . establishment of a solid tumour parenchyma does occur occasionally in the region of the connective - tissue capsule . 
the histological structure of this particular region is known to differ greatly from that of the tumour , and the different type of reaction to hn2 is presumably correlated with this . in conclusion we wish to emphasize the important fact that 72 hours after hn2 administration a series of changes takes place which result in the complete transformation of the histological structure of the walker carcinoma . 
the effect is , however , temporary ; the animals were already gaining weight again 7 days after treatment . in this respect the effect of hn2 is much more drastic than was observed after  . 
body weight ( intraperitoneal injection )  . while the cellular injury in the femoral bone marrow induced by 500 r was much more drastic than that produced by the hn2 " ld50 - equivalent " this x - ray dose was found to be still insufficient to bring about by way of the systemic effects the same amount of cellular and the same kind of histological changes which have been observed after hn2 administration . 
the delay in the developmental cycle may last 12 hours . this is indicated by the fact that in the 12 - hour sample 6 cells with chromosome injuries were observed out of 27 in which the chromosome abnormality suggested that they were already the frequency distribution of the injured cells in mitosis during irradiation . observed in the various samples is a further indication that cell development has been retarded . while the highest proportion of injured cells is seen 12 hours after exposure to 300 r , the maximum damage was in the 48 - hour tumour sample 182 p . 
the true significance of this observation lies in the relationship which it has to the primary reactions induced by the two ' agents . the view is now widely accepted that during irradiation ionisation takes place in the cell , followed immediately by the formation of free radicals of the water molecules ( lea , 1946 )  . this event represents the first step in the complex similarly reaction - chain which in time leads to a definite biological phenomenon . there is no substantial delay between administration of hn2 and its primary reaction in the organisthe rate of hydrolysis of nitrogen mustard is extremely high in a biological system , and it has been shown recently by batemann , klopp and cromer ( 1951 ) that it remains " active " only for a few minutes after intravenous injection . this is the main reason which allows us to compare the cellular effects of x ray and hn2 in tumour samples taken at the same time after treatment and to determine the relative sensitivity of the various stages of the mitotic cycle . the measure of sensitivity of a cell is the frequency of chromosome injuries observed at a given time . 
the interval between treatment and fixing the cell for analysis indicates the cell stage during treatment . using this criterion the radiation sensitivity of the mitotic cycle has been determined in pollen grains of tradescantia ( koller , 1946 )  . if our present data are interpreted on the same criterion , then we must draw the conclusion that tumour cells of the walker carcinoma are most sensitive to x rays at the end ofthe resting stage or beginning of prophase , while they are least sensitive to hn2 at this stage . 
revell ( 1952 ) employed a new and critical method in the study of chromosome effects of several substances ( mustards , epoxides , etc . ) and came to the same conclusion . 
the fact that x ray ' and hn2 initiate their effects at different stages strongly suggests that their mode of action is different . thus , for instance , we may assume that x rays act directly on definite linkages of the already synthesized polypeptide structure of the prophase chromosome thread , while a chemical agent affects the ' resting stage chromosome - filament either before or during the process of synthesis . this aspect of the chemical effects is discussed in more detail by revell ( 1952 )  . the higher sensitivity of the resting stage to the chemical agents has another implication . 
the non - dividing ( intermitotic or " resting " ) cells are ' believed to be functionally the most active cells , and often referred to as cells in the " metait is not unlikely that the degeneration of many bolic phase " ( hughes , 1952 )  . non - dividing tumour cells which we observed after hn2 administration is due to a gross disturbance in this metabolic phase . if it is found that chemical agents act preferentially on cells in the resting stage , a new approach may possibly be opened to the chemotherapy of cancer . because the functional or morphological characteristics of cells are determined 184 p . 
our experiment demonstrated such difference between tumour cells and histiocytes . the study of the cytological behaviour of the walker carcinoma under x ray and hn2 treatment has accordingly led to the conclusion that the mode of action of these agents differs , and there is other experimental evidence of different kinds to support this conclusion . 
no such reduction was observed when nitrogen mustard in barley , mutations of particular genes was used ( auerbach and moser , 1951 )  . were induced with a higher frequency by hn2 than was expected , indicating some specificity of action ( gustafsson and mackey , 1948 )  . 
cytological analysis of the femoral bone marrow and implanted walker carcinoma of the rat has shown that up to 24 hours after treatment , 200 roentgens produce the same amount of chromosome injuries as 1 mg . 
the difference in behaviour shown by the walker carcinoma after irradiation and after nitrogen mustard treatment indicates that the primary basic reactions initiated by these agents are fundamentally different . this investigation has been supported by grants to the royal cancer hospital and chester beatty research institute from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the national cancer institute of the national institutes of health , u.s. 
harris , coal tar research association , who had purified it by chromatography and checked it by ultra - violet spectroscopy for impurities . these were below the level of detection . fluorewene mea8urement& the fluorescence values for solutions of the various hydrocarbons were determined by constructing curves using a hilger " spekker " photoelectric fluorimeter with cers of capacity approximately 11 ml . , and with filter chance 0 x 7 348 d . 
mouse protein after 6 days ' benzpyrene treatment appear to be of the same order as that recovered by mller ( 1951 ) although it is not possible to assess gravimetricallv the data given by this worker since her figures are relative and apply to the instrument and filters employed . berenblum and schoental ( 1942 ) found that 24 hours after one intraperitoneal injection of 10 mg . 
woodhouse benzpyrene was added to denatured , fat - free , normal skin - protein and refluxed with alkah , toluene and zinc , it could be completely and quantitatively removed from the alkahne solution by benzene extraction . 
the extra - cellular bound ilydrocarbon might consist of metabohtes " excreted " from the cells - or it might be derived from dead or damaged cells . although the fluorescence technique was not sufficiently sensitive for accurate estimations with the small amounts of protein available , the occurence of bound hydrocarbon in cellular constituents has been confirmed by extracting the dna and rna skin proteins from a batch of benzpyrene - treated mice . 
of " fixed " benzpyrene was extracted and a trace was found in the dna protein sample which , however , weighed only 2 mg . a corroborative experiment was also carried out based on the observations of calcutt aind payne ( 1953 ) who showed that nuclei and mitochondria isolated from the livers of mice which had been given a single intraperitoneal injection of benzpyrene in finely dispersed eiuspension , contained fluorescent hydrocarbon 2 hours to 21 weeks after the injection . 
the believed , therefore , that benzpvrene injected in this way is rapidly transported to the mitochondria and nuclei and is held there in an unchanged state for prolonged periods . 
they did not examine the effect of alkahne hydrolysis on alcohol - extracted nuclei . the experiment was repeated in this laboratory but the prelinu ' nary extractions were made as described previously for the skin tissues and continued with alkaline hydrolysis . 
a small amount of fluorescent material was extracted from the hydrolysate but nuclei froni control mice did not yield comparable fluorescent extracts at any stage . this experiment showed that at least a portion of the benzpyrene can be it was repeated , therefore , employing fixed in vivo by nuclear components . perylene , and , after alkaline hvdrolysis an extract with fluorescence characteristic of perylene was obtained from the separated , alcohol - treated nuclei . 
the free hydrocarbon was thoroughly removed and the " bound hydrocarbon " was extracted after hydrolysing the protein with koh and measured fluorimetrically . although these species of animals vary considerably in their response to this hydrocarbon as a carcinogenic agent the amounts of bound hydrocarbon obtained from 25 mg . 
samples of extracted and dried tissue were very similar in all instances . other polycyclic hydrocarbons which are less carcinogenic to mice , e.g. , 2 ' 6 - dimethyl - benzanthracene , and perylene which is non - carcinogenic , have also been tested , and in all instances comparable amounts of bound hydrocarbon could be extracted from the alkahne bydrolysate . using similar extraction techniques a smar amount of fluorescent , bound hydrocarbon could be removed from the nuclei isolated from hvers of mice 24 hours after a single intraperitoneal injection of either 3 4 - benzpyrene or perylene . it is concluded that further evidence is needed to substantiate the view that 352 d . 
harris. * from the chester beatty research in.3titute , royal cancer hospital , london , s.w.3. received for publication january 11 , 1951 . themajor requirement for the investigation of the physical and chemical properties of the rous no . 
i sarcoma agent is a source of " purified " agent of a uniformly high infectivity , and which may be stored without loss of this activity , since it is not always convenient to compress the investigation to within the relatively short period in which the purified agent is stable in vitro . this paper describes a method for the production of concentrates of the vir ' us in a form suitable for storage , and the storage problem itself is considered in the following paper . a variety of chemical and physical methods have hitherto been used for separating and concentrating the agent from biologically - inactive tumour protein and nucleoproteins . claude ( 1935a ) found that such contaminants could be removed by adsorption , on to freshlv prepared aluminium bvdroxide gel , and the carbohydrate contaminant by precipitation with gelatthe agent was not directly affected , and a - combined chemical fractionation and dialysis gave a 25 - fold concentration in - terms of dry weight ( claude , 1935b )  . this method was also investigated by dmochowski ( 1948b ) , who recorded a 50 per cent increase in the activity of the agent compared with the startino , c5 filtrate . shemin , sproul and jobling ( 1940 ) , and shemin and sproul ( 1942 ) precipitated the agent from filtrates by addition of papain or of histone . 
nitrogen ( the range was 1 - 3 x 10 - 3 mg . to 7 x 10 - 7 mg . ) were found to be infective . concentration of the agent by centrifugation was first described by ledingham and gye in 1935 and fractional centrifugation methods have since been widely used ( mcintosh , 1935 ; amies , 1937 ; claude , 1937 , 1938 , 1939 , 1940 ; claude and rothen , 1940 ; pollard , 1938 , 1939 ; stern and duran - reynals , 1939 ; dmochowski , 1948a )  . claude ( 1938 , 1939 ) isolated a fraction corresponding to less than 3 - 5 per cent of the dry weight of the original extract which , in amounts corresponding to 4 - 0 x 10 - 10 mg . 
harris pollard ( 1939 ) and amies and carr ( 1939 ) were able to overcome the first difficulty by precipitat - ing the agent from a clarified extract by adjusting the ph to 5.0 to 5 - 5 . 
the isoelectric point of the purified agent is 3 - 5 , but tumour extracts deposit a mucoprotein at ph 5 - 0 , which takes down the agent with it . the aggregated agent , etc . , was then further concentrated by a low - speed centrithe aggregates were.broken down by tryptic digestion at fugation procedure . ph 8 - 8 to 9 - 0 and the released agent further " purified " by fractional centrifugation . alternatively , the ' mucoprotein may be hydrolysed by incubation of the extract - with hyaluronidase , which has no deleterious effect upon the agent ( siturm , and duran - reynals , 1932 ; shemin and sproul , 1942 )  . 
the agent may then be deposited directly from the non - viscous extract . bryan , riley , deihl and voorhees ( 1947 ) have avoided this difficulty by the simple , but uneconomical , procedure of rejecting the first , viscous extract . a further method which has been claimed to apply to the purification of small arrlounts of agent is that of chromatography on celite ( riley , 1948 )  . 
the agent is strongly adsorbed to celite from physiological salt solution , but may be eluted intermsoftheratio , biologicalactivity : withverydilute ( o - 001m ) saltsolution . nitrogen content , a 3to 7 - fold enrichment was obtained from a partially ' - purified three of the above methods , papain precipitation , fractional tumour extract . centrifugation after precipitation at ph 5 - 0 and direct deposition after treatment of the initial extract with hyaluronidase , have been reinvestigated from the point of view of the preparation of large quantities of agent in a form suitable for storage . 
a further method , methanol precipitation , hitherto applied to a number of other animal viruses , has also been investigated . cox , van der scheer , aiston and bohnel ( 1947 ) found that influenza virus ( from arantoic fluid ) could be precipitated in active form from suspensions in phosphate buffer at ph 7 - 0 to 8 - 0 by addition of methanol to a final concentration of 15 to 30 per cent . 
sharples air - driven supercentrifuge , stainles - 3 the rous agent becomes progressively more thermolabile as purification centrifuge b was used in a cold - room at o ' c . , and c was adjusted to the sharples centrifuge ( a ) was cooled with the centrifugal procedures used are listed below and steel bowls . - ( i ) clarifica ( ii ) deposition at ( iii ) deposition at ph 7 - 0 . 
the bulk of the tumour was extracted in the waring " blendor " with 10 volumes of water containing 1 : 10 , 000 hcn , and the small sample " minced with scissors " and extracted into a similar medium . suitable dilutions of these extracts were injected into fowls . 
0.005 m buffer at ph 7 - 2 containing hyaluronidase and 1 : 10 , 000 ticn . the tissue suspension was clarified ( b , i ) and the agent deposited from the supernatant ( b , ii )  . 
the control suspension ( a ) was ' assayed comparatively against ( b ) - resuspended papain - agent complex , etc . , ( b ) - supematant and ( c )  . 
and methanolic buffer solutions prepared , and cooled to these buffers contained ( a ) 40 per cent methancil , ( b ) 50 per cent methanol and ( c ) 60 per cent . methanol respectively in 0 - 005 m buffer . equal volumes of ( a ) , ( b ) , ( c ) or buffer ( d ) - control , were added to volumes of the supernatant . 
an equal volume of 50 per cent methanolic buffer was added under the same conditions as method 1 and the resuspended deposit assayed against the extract . the assay showed that the alcohol - deposited agent had only i per cent of the activity of the control suspension . ( 3 ) a similar clarified extract was prepared , cooled to o ' c . 
the deposit was resuspended in 0 - 005 m buffer at ph 7 - 2 , clarified ( b , i ) and the agent in the supernatant deposited ( b , ii )  . the pellet was finary resuspended in 0 - 005 m buffer , ph 7 - 2 , adjusted in concentration to the equivalent of i g . 
de osition after precipitation at ph 5 - 0 . a 10 per cent fresh tumour tissue suspension was prepared in the usual way , but with the omission of hyaluronidase . 
the air - driven sharples supereentrifuge with a maximum speed of rotation of 50 , 000 r.p. ( 62 , 000 g . ) was used by stanley in 1945 for the concentration of influenza virus for vaccine production . 
for deposition of the virus the stainlesssteel centrifuge bowl was invariably lined with cell ' ophane ( 7 / 1000 in . ) which may ( a ) be readily withdrawn and which ( b ) minimizes contact of the virus with metals . when unrolled this " liner " invariably showed a boundary , the distance of which from the bottom of the bowl , varied with the rate of flow of the virus in terms of total nitrogen distribution , the suspension through the centrifuge . deposit was uniformly distributed above and below the boundary , although the virus content of the top and bottom fractions differed considerably . 
the " liner was therefore divided at the boundary and the deposits removed and separately resuspended in 0 - 01 m buffer at ph 7 - 2 ( dband dt )  . 
per cent crystalline trypsin was added to each , the suspensions incubated at room temperature for 40 minutes and the virus re - deposited ( a , iii ) ( sb , st - supernatants and dbj , dt , - deposits )  . 
fresh tumour tissue was disintegrated with 10 volumes of 0 - 005 m phosphate buffer at ph 7 - 2 containing 1 : 10 , 000 hcn - but without hyaluronidase - and the suspension clarified ( a , i )  . 
88. the " liner " was removed and the total deposit ( d . , ) resuspended in 375 ml . 0 - 005 m phosphate buffer at ph 7 - 5 to 8 - 0 containing a few mg . 
harris constant standard could be obtained or that the subsequent comparison would be unaffected by such factors as the season of the year or the nature of the medium in which the virus was suspended . 
the first group ( " limiting dilution " methods ) had , also , the advantage of giving some degree of absolute measure corresponding to the actual number of tumour - producing particles . two injection routines have been favoured by prev - ious workers ; either the intradermal or the intramuscular . 
the former allows several different dilutions to be tested in the same bird , but accurate localization of the injection is rendered difficult by the paper - thin structure of the avian skin . moreover , the frequent occurrence of resistant fowls necessitates replication of the tests . intramuscular injections involve a more readily standardized reaction site , but 6 - week - old birds frequently show a variable and unpredictable resistance to the virus . such resistant birds may not react to 1000 times the virus dose which will produce tumours in susceptible birds , and if the end - point , ( m.i.d. ) is dependent , as may be shown , upon a poisson distribution of virus particles , then a large number of 6 - week - old fowls would be required for an accurate assay . it is inconvenient to use large numbers of birds of this age for a single assay and for such reasons the use of embryos or of day - old chicks , which may readily be obtained in large numbers , was investigated . 
the survivors are killed and examined at 28 - days . sudden deaths in the young birds as a result of the " haemorrhagic disease " described by milford and duranreynals ( 1943 ) did not occur when the inoculum was given into the leg muscle . irregular results were obtained in the assay when the . 
harris trypsin ( which removes more than 60 per cent of the non - virus proteins ) gives a product containing only 2 per cent of the nitrogen of the clarified tumour extracts , but possessing almost ar the virus activity . 
a biological assay method using very young chicks has beerr developed . these chicks are found to be more sensitive to the virus than older birds and are obviously more convenient to handle and maintain . the authors wish to express their thanks to professor a . 
the tumour extended outwards for 1 - 5 cm . into the surrounding lung tissue , and in collar - fashion for 4 to 5 calong the bronchus , its branches and the contiguous blood vessels . ' the cut surface of the tumour was finely patterned by white striae , which separated softer , yellow or grey areas . 
the lymph nodes in the hilus of the left lung were replaced by a large mass of partly necrotic tumour tissue which , extended into the posterior mediastinum , compressing and invading the adventitia of the great vessels and of the oesophagus . 
numerous deposits of tumour , up to 3 cin diameter , were present in the left pleura , especially over the intercostal spaces , and the pleural sac contained approxiniately 300 ml . 
the mucosa was fixed to the tumour and slightly elevated ; superficial ulceration involved an area of 2 - 5 x 2 cthe lumen of the bowel was not obstructed , and the mesocolic lymph nodes appeared to be normal . the peritoneal cavity contained a small amount of straw - coloured fluid ; the serosa was sparsely studded with tumour deposits which measured up to i cin diameter . 
the surviving liver tissue was deeply bile - stained and congested . the lymph nodes around the coehac axis and head of the pancreas , in the porta hepatis and in the lesser omentum were enlarged , and their substance was replaced by tumour tissue . 
the para - aortic and iliac lymph nodes were involved to a less degree . there were no relevant abnormahties of the other abdominal and pelvic viscera . the body of the ilth thoracic vertebra was almost completely destroyed by tumour , and had collapsed , with consequent pressure upon the spinal cord . 
the appearances were characteristic of an anaplastic bronchial carcinoma " of the " oat - cell " type , and confirmed the macroscopic diagnosis of primary bronchial carcinoma . the greater part of the colonic tumour was . 
the mucosa overlying the mass , however , showed an abrupt transition at its periphery from the normal structure and cytology to a polypoid , hyperchfomatic columnar - cefl adenocarcinoma , irregular gland - hke extensions of which penetrated deeply into the tunica muscularis ; the structure and cytology were those ' of a primary colonic adenocarcinoma . 
the patient remainecl in seemingly good health for more than 18 months , and then sustained a fracture of the pelvis in an accident . nine weeks later an abscess developed deep in the inter - ischial region , necessitating incision ; its contents were not examined . during the next fortnight a papiroma , about 0 - 8 cin diameter and situated at the medial end of the left inguinal skin fold , began to grow rapidly ; it doubled its size within this period , after which it was excised . 
the patient then remained apparently well until 1949 , when she began to be dyspnoeic ; - examination showed a right - sided pleural effusion . clear , amber - coloured fluid was aspirated 5 times , at intervals of a few weeks , the quantities withdrawn ' ranging from 550 to 1200 ml . the fluid contained between 4 and 5 per cent of protein ; a few cehs were present , mostly lymphocytes , with a very small pro_portion of neutrophile polymorphonuclear leucocytes and normal serosal cells . aerobic and anaerobic cultivation on ordinary media yielded no growth , and , cultures for mycobacterium tuberculosis were also sterile . radiography showed no evidence of neoplasm in the chest , but the effusion persistently obscured the - greater part of the right lung field ; there was never any demonstrable effusion in the left pleural sac . as there was no evidence of recurrence or metastasis of the carcinoma , and as there was no demonstrable infective cause of the recurrent pleural effusion , the discovery of an adnexal tumour on pelvic examination suggested the possibifity that the con ' dition was an at pical variant of the meigs - culhngworth syndrome . 
at laparotomy , 6 months after the onset of dyspnoea , a cystic tumour of the left ovary was fou ' nd and removed ; there was no other abnormality in the pelvis or abdomen . 
the tumour of the left breast was a simple intracanaficular fibro - adenoma . macroscopically , the ovarian tumour was a unilocular cystic teratoma , i 1 cm . in diameter , filled with sebum - hke material and hair . 
the cyst had a smooth lining ; its war was i mor less in thickness , except near the pedicle , where there was an irregular , bone - hard eminence , approximately 2 cin diameter , projecting into the cavity . adjacent to the pediele the remnant of the ovary was identifiable on the external surface of the tumour as a flattened , ovoid area of firm , greyish - white tissue , which measured 3 - 5 x 2 - 5 csuperficially , and up j . 
symmers microscopically the cyst was lined by keratinizing epi - to 0 - 4 cin thickness . dermis , external to which was a narrow zone of fibro - fatty tissue . hair - follicles and large sebaceous glands were numerous in the skin covering the hard projection , which consisted of bone , bron ' chial structures and neuroglia . 
the third hypothesis seems to us to be the only one tenable . if the coexistence of two primary neoplasms is accepted , the significance of the presence of a metastatic deposit from the primary bronchial carcinoma . at the site of the primary colonic carcinoma requires to be considered . this association may have been fortuitous , or the presence of the colonic neoplasrn may have predisposed to the establishment there of the metastasis , or the development of the latter may have inducea cancerous change in the adjacent mucosa ; it seems to be impossible to say which suggestion is correct . 
the induction , by some effect of the existing neoplasm , of sarcomatous change in the stroma of carcinomata has at times been postulated in explanation of the genesis of so - called careinosarcomata : in view of the considerable doubt as to the origin of the sarcoma - like component of these tumours , such a hypothesis has httle practical value . 
the induction of one carcinoma by another was postulated by duboisferri ' ere ( 1939 ) , who suggested that hepatic metastases in his case of islet - cell pancreatic carcinoma had induced local development of bile - duct carcinomata . he was not able to exclude the possibihty that the adenocarcinomatous areas in the liver were metastases with an unusually well - developed tubular structure , such as is sometimes seen in islet - cell neoplasms . seecof ( 1924 ) reported a case which was in some respects similar to ours . 
the tumour incidence in the experimental group ( 9 / 22 , or 41 per cent ) is thus not significantly in fact , a slight falling off in the tumour lower than in the control groups . incidence might have been expected in mice that were 43 weeks older than their controls at the time of tumour development . 
some important records of pedigrees , showing apparent . transmission from mother to daughter , were published nearly a century ago . the most remarkable was recorded by broca ( 1866 ) , in which four generations of females had the disease . in spite of evidence brought forward by a great many observers that mammary cancer can frequently be found affecting several of the female members of a family group , doubt , still remains as to whether heredity plays any significant ' aetiological part . this doubt arises because of the great prevalence of the disease in the general population , where it is responsible for nearly 3 per cent of all female deaths . 
with so comm ' on a condition , it is difficult to demonstrate convincingly that the occas ' lonal familial conoentration is not merely the result of a random distribution of cases . to obviate this uncertainty , most investigators in recent years have collected a series of cases , noted the incidence of similar disease among their relatives , and compared it with the corresponding incidence among a control group of cases free from the disease , selected so far as possible at random . in spite of elaborate precautions , - the difficulties , involved in obtaining a satigfactory control group of family histories to match those of the propositae , have repeatedly proved almost insuperable . 
the result is that many workers ( hanhart , 1943 ; passey , 1942 ) still ' consider that there is , insufficient evidence to prove the reality of familial transmission of mammary cancer or of aay type of human ma " lignant disease . stocks and karn ( 1933 ) found no evidence that a history of cancer in relatives increased the risk of cancer to anymeasurable extent . several extensive surveys have been published , all of which give some evidence for believing that mammary cancer is unusually prevalent amon the mothers and sisters of affected cases . 
the patients were attending either university college ilospital or the london hospital , and they were personally interviewed . all possible hospital records and reports were searched or checked by correspondence . this procedure applied b6th to the propositae and to any of their relatives who were reported to have suffered from malignant disease . unfortunately , in a number ' of instances , records had been destroyed by enemy action during the war . ideally , the death certifica ' te of every relative believed to have died of malignant disease should have been obtained , as corroborative evidence , but th ' is we have not been able to do . 
the distribution of these 116 " familial " cases and the mean age of onset of their illness ( 5 1 0 years ) was extremely similar to that of the this finding does not support jacobsen 's remaining " non - familial " cases . assertion that familial cases have an earlier onset than others . 
the infertility ratio , 91 out of 408 , or 22 - 3 per cent , significantly exceeds the value of 17 - 3 per cent for married women of the same mean age given by the registrargeneral ( 1938 ) , and supports the view that nulliparity is an etiological factor . the mean age of the patients when first interviewed for purposes of this this indicates that they had , on the average , lived survey was 55 - 2 years . undoubtedly three - and - a - half years since first gigns of the disease had appeared . the survival of the patient was a property , which determined her inclusion in the investigation , and the longer the survival , the more probably would she be selected as a proposita . 
the date of death and the age at the time were recorded in a few instances the dates were approximate , but could hardly for each case . be more than a few years in error . 
the expected proportion of deaths due to mammary cancer and other types of malignancy in each year and at each age can be obtained on the basis of the general population statistics . 
the distribution of deaths by year and age is shown in table iii . from ' this table the number of deaths due to mammary cancer if the women had been subject to the mortality in the general population was estimated at 11 - 17 , a figure significantly less than the observed 25 . 
51 observed as compared with 48 - 76 expected . there were 102 mothers still living at the time of investigation a ' nd , of these , six were know - n to be under treatment for mammary cancer while four had some other type of malignant disease . 
hence any likeness of onset age of mammary cancer in sisters is not peculiar to this type of malignancy . another interesting correlation concerns the sites affected in pairs of sisters and other relatives . 
the tracheo - bronchial glands may occasionally arow small amounts of the carbon to pass through into the thoracic duct or into lymphatic efferents from the glands which communicate directly with the great veins within the thorax , and thus the carbon reaches the such carbon in the blood stream is taken up by the cells of the blood stream . reticulo - endothehal system in organs hke the spleen and hver , which very occasionally at autopsy may show shght stippling with carbon , though in six spleens examined chemically we have found no weighable carbon in our residues . the amount of carbon deposited in a lifetime in the lungs and tracheo - bronchial glands depends on many variable factors such as age and occupation . 
where the degree of atmospheric pollution is great the excessive amount of carbon inhaled clogs the ciha of the respiratory mucous membrane and a large amount is not expelled even in the normal subject . in the subject who suffers from chronic catarrhal inflammation of the respiratory mucosa , there occurs ' a progressive destruction of the normal ciliated epithelium which is partially replaced by a non - cifiated type of a lower order , such as cuboidal or even squamous cens , which are unable to expel carbon particles . 
the scarring so caused is usuary the seat of dense areas of diffuse fibrosis resulting from bronchiectasis accumulation of carbon . or from the imperfect resolutions of acute pneumonias are often relatively free thus the only from carbon . 
why this should be so is not altogether clear . accurate means of assessing the total amount of carbon in the lungs and tracheobronchial glands as a whole is by estimating chemically all the carbon in these structures , and it is from this angle that we have approached the problethe amount found in these organs at autopsy thus represents what has been retained during a hfetime . 
the carbon itself may be innocuous , but from our studies of atmospheric pollution ( goulden and tipler , 1949 ; warer , 1952 ; goulden , kennaway and urquhart , 1952 ) , one can form some idea of the amounts of the carcinogens , 3 : 4 benzpyrene and arsenic , which would accompany it , and may possibly have some effect , either in association with , or apart from , that of tobacco . the black coloration of the lungs and bronchial glands must have become increasingly famihar to british pathologists since the industrial revolution which in the earlier part of the nineteenth century converted britain , by the utilisation of coal and iron , from an agricultural to a largely industrial country . although abundant material has been available in britain during the last 150 years , no one has , so far as we know , attempted to estimate the amount of carbon in human lungs , except in the special case of coal - miners ( king and gilchrist , 1945 )  . 
a questionnaire on the following points was circulated : sex ; age ; diagnosis and post - mortem findings ; places of residence for more than three years and the period lived in each ; occupations followed for more than three years ; the smoking history as regards the use of a pipe or cigarettes ; the age at which smoking was begun and stopped ; the maximum and average amounts smoked per day , and whether inhalation was practised always , occasionally or never . considerable difficulties were encountered in obtaining lungs from persons without bronchial carcinoma for controls ; those were needed from whom an accurate history could be obtained , but who were not likely to live long . 
joules of the central middlesex hospital , london , for the supply of material ; also to professor neils dungal of reykjavik for the lungs of eight persons who had always lived in iceland . 
the pulmonary glands in the lung substance were separated as far as possible from lung tissue ; no claim is made that this division , was carried out very accurately , but the much lower concentration of carbon in the lung makes some contamination with it unimportant . 
the separation oflymph glands is of course still more difficult when a large invasive mass of bronchial carcinoma is present ; the practice has been to regard as lymph glands any deep black stippled areas of simflar size and shape , and to class the remainder as lung . 
histology. - the lungs submitted to us had been fixed whole in formalin and thus the fixation from a histological point of view was not perfect . blocks of lung tissue were nearly always taken from the pleural region and from deep in the lung substance , and occasionally from the tracheo - bronchial glands . these blocks were subsequently refixed in formol - corrosive and the paraffin sections were stained by haemotoxylin , by carmalum or neutral red , by van gieson or mallory , and , in a certain number of cases referred to later , by potassium ferrocyanide to demonstrate any iron . 
the cases from hospitals in london ( tables ii and iii )  . - the places of residence and occupations given are those of longest duration only . in the case of persons hving in london , the part of london in which they hved is stated in brackets after a capital l ; for those living in other towns , the county is given i " cigarettes " expresses tobacco consumption in this form even where brackets . cigars or a pipe were smoked . 
tobacco is equivalent to 28 cigarettes . the small number of cases prevents any firm conclusions about differences in the amounts of carbon in the lungs ofpersons with and without bronchial carcinoma . these differences are not statistically significant , but are nevertheless of interest . the average amount of carb ' on in the lungs of females with bronchial carcinoma was greater than that in the controls ( table iii ) , although the carbon content of the glands did not differ appreciably between the two groups of women ; one might expect this result if some carcinogen such as 3 : 4 benzpyrene adsorbed on to the carbon particles in soot is concemed in the aetiology of lung cancer . 
the again , the carbon in two groups of men , however , showed the opposite result . the glands was approximately the same for the two groups , but the control group had the higher carbon content in the lungs . there was no apparent reason why men and women should differ in this way . the total carbon content of a lung must vary according to three chief factors , ( a ) age , ( b ) the size of the lung ( since a larger person will ' mspire more air and hence more carbon ) , and ( c ) the environment in which a person lived . allowance for the first of these variables is easily made . 
when the weight of carbon in the lungs and glands was divided by the age ( table iv ) the differences between the four groups remained and were still of the same order . 
the cases from iceland ( table v . ) - since these , specimens did not include the whole trachea , some of the bronchial glands may not have been present ; the figures in table v therefore represent the carbon and ash content of the lungs and glands together . the content of both carbon and ash in the women - 's lungs was considerably greater than that in the men 's , apart from the exceptional value for the man no . 
carbon in lungs / age in years . 25 - 1 ( 12 - 6 ) 13 - 8 15 - 4 11.9 bracketed averages include the abnormal figures for no . 
50. tthis very high value for a - sh was omitted from the average . microscopicary , no silica was found in sections of the lung . those obtained in london , shows that the lungs of icelandic men had a lower average carbon content , while those of the icelandic women had a much larger amount . 
the same differences obtained on correction of these figures for variation in age distributio ' n . the presence of such amounts of carbon in these lungs from iceland seemed at first sight surprising , for in iceland general atmospheric pollution as understood in this country is very small . there is no native coal or oil , and these are costly to import . 
was a non - smoker . in the group of women with bronchial carcinoma , i out of 5 did not smoke , and in the control group , 9 out these figures , especiary for the women , show a higher proportion of nonof 1 1 . smokers among persons without bronchial carcinoma . 
the total carbon content of the lungs varied over a wide range all the points indicating a total consumption of more than for non - smokers ; 200 , 000 cigarettes refer to men and women with bronchial carcinoma . 
the average daily consumptions were : males with bronchial carcinoma , 24 / day ( 16 cases ) ; males without bron ' chial carcinoma , 12 / day ( 5 cases ) ; females with j . 
urquhart bronchial carcinoma , 19 / day ( 5 cases ) ; and females without bronchial carcinoma , 2 / day ( 10 cases )  . ash content of the lungs and bronchial glands . the nature of the ash deposited from the hydrolysates of these lungs has not although about 10 per cent of the total carbon was contained been determined . in the glands , the fraction of the total ash present in them was about 20 per cent . this suggested that the bronchial glands were even more efficient in concentrating particles of mineral matter than they were in accumulating carbon particles . 
for comparison with the histological findings the chemical results were divided into three groups , namely , those with a carbon content of ( a ) 0 - 49 g . 
the carbon in the sections showed the normal distribution , being heavier under the pleura , around the bronchi and blood vessels and in the fibrous septa , than in the vesicular portions of the lung . the rocks of iceland are of volcanic origin and the roads are metaned with such material which , due to weathering , quickly breaks down so that with the passing probably road dust has become considerable of traffic much dust is created . in iceland , where there are now 11 , 000 motor vehicles , only since the acquisition in view of this the icelandic lungs were of american cars after the last war . submitted to a more intense microscopic study for the presence of sihca and of iron . 
no evidence of silicosis was noted in any and doubly refractile granules of in only one case was iron silica were very scanty or absent in all the sections . found , apart from occasional heart - failure cells in the others . in this case the iron was present chiefly in the fibrous tissue of the septa and around the bronchi and blood - vessels in close association with carbon particles which the iron pigment appeared to surround . 
is retained ; this gives some measure of the efficiency of the nasal filter and of the mechanism by which particles which have reached the deeper respiratory passages are swept upwards again by ciliary action and expectorated or swallowed . 
when the floor of a room is swept towards the door , the part adjacent to the door is exposed to dirt from a much larger area . similarly , when particles of dust are arrested on the walls of the smaller bronchi and bronchioles , they are swept upwards by ciliary action through the main bronchi ( the door ) into the trachea , and carcinogens might diffuse from the particles into the layer of mucus covering the bronchial mucous membrane during transit . 
some such mechanism would be in accord with the statement about the site quoted above ; but some recent investigators ( westermark , 1938 ; raebum , 1951 ; raebum and spencer , 1953 ) think that tumours arise - with about equal frequency in any part of the lung . the estimations of arsenic and of 3 : 4 benzpyrene in the air of large towns given in table viii are those of goulden , kennaway and urquhart ( 1952 ) and table viii . - concentrations of arsenic and of 3 : 4 benzpyrene in town air . london ( becton ) bilston manchester liverpool . sheffield london ( county hall ) hull bristol mean concentrations , pg . 
a8203per cigarette ( daff and kennaway , 1950 )  . ini ' mum amount of a strong carcinogen such as i : 2 : 5 : 6 ' dibenzanthracene which will produce * our earlier results , which were confirmed subsequently , were demonstrated at a meeting of the pathology section of the royal society of medicine held at this hospital on january 15 , 1952 . shear ( 1936 ) found that the j . 
of 3 : 4 benzpyrene which may be inspired in ' a lifetime , but in view of the vastly greater area over which this may be spread and the different time relations , one may doubt whether this comparison has any value . the size and arrest of smoke particlm . the available data about the arrest of smoke particles in the air passages are very defective because we have not , to begin with , any adequate information about the size of these particles . 
the passages quoted verbatim below contain all the information that we have found on this subject . the leicester report says : " the size distribution of smoke is a subject which still requires investigation . green ( 1936 ) gives estimates for five industrial dusts from which it can be inferred that 50 per cent by weight of such dusts is less than 3 to 10 microns , and 80 per cent is less than 5 to 15 microns in mean diameter . atmospheric smoke may be similar in size distribution but a direct investigation is  . 
some of the properties of smoke depend on the area it can cover ; half the surface or sectional area of the smoke was in particles larger than about 0 - 35 micron . there is a distinct tendency for smoke particles to stick together in chains , perhaps one micron long . " the comparison of such results obtained by different methods of arrest is not e . 
are in the range of size where there is minimum retention in the lung , 80 per cent of them being exhaled and 20 per cent arrested in the alveoli . ( b ) the mean diameter of smoke particles and the range of particle size of carbon black which shows the greatest adsorption of 3 : 4 benzpyrene from benzene ( falk and steiner , 1952 )  . 
though the material was not statisticary adequate , the smoking histories of the cases examined showed a higher consumption of tobacco among both men and women with bronchial carcinoma compared with the controls . 
if the carbon in the lungs and bronchial glands does not leave the body by any channel the amount found post - mortem represents what is retained out of the intake of a lifetime . 
the data now available for atmospheric poflution in some english towns arows an estimate to be made of the amount inspired during a hfetime in them ; this might be of the order of i 00 g . , while the quantity found in the lungs and bronchial glands was approximately 0 - 5 to i - 0 g . 
estimations of 3 : 4 benzpyrene and of arsenic in the suspended matter of the air of various english towns enable one to calculate the amounts of these compounds which would accompany the carbon inspired , and retained , in a lifetime . we wish to express our gratitude for the materials and case histories which have been the subject of this investi ation to professor niels dungal of revkiavik ; to horace joules of the central middlesex hospital , london , and to two members of his staff , a . 
althougih biologists have for long been uneasily aware of the existence of a problem of cell heredity , its systematic analysis is the work of very recent cell heredity deals with the origin and maintenance of inherited character years . differences between cells ; more particularly , between cells that set up division its problems present themselves in their most acute , lineages by mitotic fission . if not most easily workable , form in metazoan development . the outcome of cellular differentiation in ( say ) mammalian development is the formation of a limited number of histologically definable cell genera , each one further subdivided into a variety of cellular genetic species . 
the genus " fibroblast , " as yet far from completely analysed , may be subdivided into cells which manufacture bone , cartilage , white connective - tissue fibres , and so on . genus " epidermis , " of which we have made a particular study ; includes the epidermal epithelium of the superficial skin , of the sole of the foot , the tongue , cells of each of these epidermal the claws or nails , the vagina and the cornea . species display a distinctive combination of structural or physiological properties . the epidermis of the sole of the foot , for example , has a characteristically high rate of cell division . 
but this has proved not to be the case . although plausible " phenocopies " of sole epithelium ( in the form of corns and callosities ) can be made by irritating the thin and relatively quiescent skin of the body surface , the difference between the division rates of sole and body epidermis is in fact " intrinsic " and inheritable . 
we have , for example , transplanted sole epidermis to positions in the body where it is protected by neighbouring hair and secure from mechanical irritation ; but even so , its characteristic growth rate has been maintained for at least two years , and thick pads of now functionless cuticle continue to form over it and may periodically be removed . claw epithelium tells the same story - more clearly , since the difference between claw and body epidermis is anatomically crude and obvious . 
comeal epithelium is very transparent , and its mode of cell - packing and cuticle formation is characteristic . these properties might well be the outcome of the peculiar situation in which it lives - lying taut over the unvascularized comeal dermis , relatively low in temperature , and nourished under conditions of ' ow 02 tension by the aqueous humour , and perhaps to some extent through its outer ( cuticular ) surface as well . if the difference between comeal and body epidermis were merely a difference of " nurture , " then the heter6topic transplantation of the comeal epidermis to ( say ) the chest wall should bring about its reversion to the cell type characthis does not happen . 
expand its substance and area fifty - fold by cell division and outward spread ; but it still retains its characteristic cell packing , mode of cuticle formation and exquisite transparency , so that fine regenerating dermal blood - vessels corneal grafts have are to be seen through it as clearly as through a window . proved to form a rather unstable epithelium , which never seems to achieve the firm union with the underlying corium characteristic of body skin . for this reason we have not yet been able to " ' cultivate ' " corneal epithelium as a heterotopic graft long enough to be quite sure that ' it represents a distinct epidermal species . 
we can only say that it has given no hint of reversion after fiv ' e weeks of cultivation . in general , the technique of tissue culture confirms the results of heterotopic transplantation ; but it is far less critical in its discrimination between cells of different species , because cultivation in vitro has a tendency to make different ciiltivation in vitro is not known to bring about any cells look rather alike . inherited change in differentiated cells , unless we take into account the fact that prolonged and rapid growth may perhaps cause individual cells to lose specific properties in the " growth rate dilution process " recently reported on by preer ( 1946 )  . 
the " antigenic simplification " ( gorer , 1938 , 1942 ) and anaplastic tendencies of long established and ra idly growing transplanted tumours may conceivably represent a phenomenon of similar origiia . it will be clear from the foregoing examples that the techniques we have so far used to discriminate between the several true - breeding species of epidermal cells are , in their use of heterotopic transplantation , formally identical with those used in classical experimental embryology to distinguish between cell systems undergo ' ing " self " and " dependent " differentiation . 
the study of cell heredity is likewise , in effect , the study of cellular transformation - that is , of the origin of inherited differences between the phenotypes of cells . from our point of view , the most important of the several different types of cell transformation is that which , in a rough preliminary classification , has been called infective ( medawar , 1947 )  . 
the second , a corollary of the first , is that infective transformations can be serially propagated - a cell once transformed can in its ttirn transform another . the special importance of infective transformations is that they provide clear direct evidence of the particulate nature of cell heredity , and so , indirectly , of the fact that the differences between cell species are combinatorial in nature and not smoothly blended . 
 ' the authors ' work on the inheritance of colour differences in spotted guinea - pigs ( as , in the cells of guinea - pigs ' skin is relevant here . apparently , in spotted pigs and friesian cattle ) the - pigmentation of the black skin areas can be seen during life to encroach upon the white . 
the spread is even in density and snioothly progressive , but it notmally leaves untouched the liairs of the white area that are being encroached upon , so - that - the transitional zone of black skin that was formerly white is distinguished by bearing white liairs on a black skin background . 
our interpretation of the phenomenon ( billingham and medawar , 1948 ) is , in outline , as follows : the origin and seat of pigmentary function in black or other coloured skins is the pigmentary dendritic cell , a branching cell which lives in the lower reaches of the epidermis and which in some unexplained manner " feeds " - or , as masson ( 1948 ) puts it , " injects " - rnelanin granules into the malpighian layer cells on which its branches end . pigmentary dendritic cells form a facultatively syncytial system , since the branches of neighbouring cells are sometimes confluent , and a branch from one dendritic cell , instead of ending on a malpighian cell , may sometimes apply itself to the cell body of another . in the white areas a dendritic cell system is present which is similar in every respect save one : the cells lack both melanin granules and the enzyme apparatus required for making it , and no form of merelv physical stimulus will cause them to acquire pigmentary ftinction . we have shown , not yet with final precision , that the phenomenon of pigment encroachment or spread at the pigmentation boundaries of spotted guinea - pigs is due to the transformation of white ( non - pigmentary ) dendritic cells into melaninforming cells by contact with their pigmentary neighbours . 
the transformation , once achieved , is permanent in the transformed cell and its division lineage and a white cell transformed to pigmentary function can in its tum tramform its neighbours . 
we - have now to ask whether the pigment - spread phenomenon we have analysed is a mere curiosity of nature , or whether it exemplifies a principle of general importance . the experimental system we bave been using is a very unusual one indeed , for the following reasons : most cells liberate their secretory products externally or into the general circulation . dendritic cells pass their secretory product , melanin , into the cells around them - " cytocrine " activity , as masson calls it . their neighbours are norinally the malpighian cells of the epidermis ; but , as inlasson lias pointed out , dendritic cells may also inject melanin granules into cells of quite different origin - into the cells of gut epithelium for example , if a tumour metastasis happens to bring them within reach of its branches . 
the casual leakage of enzymes from one cell into another would make nonsense of embryo ] ogical de - velopment ; no organ could exist under these conditions , with its great variety of cells of different types in intimate physical contact . 
an infective transformation can only be secured by taking advantage of peculiar cell properties , like the cytocrine properties of dendritic cells and their transiently syncytial lay - o - ut ; of peculiar animals , like spotted guinea - pigs ; or of technical tricks , like grafting claw epithelium to the skin of the chest , or - to choose an example from the illuminating pioneer work of sonneborn ( 1943a , b ) - by delaying the conjugation process of paramecium so that the conjugant pairs may 130 r . 
the relevance of these ideas of cellular heredity to cancer etiology has been dealt with by other speakers , so that only special aspects of the problem need be considered here . the centre of gravity of modern speculat - ion about tumours has altogether shifted from - the idea of the malignant cell as one which proliferates faster than its neighbours , towards the simpler and more general fact that it has acquired their rapid rate an inherited character difference from its normal homologues . of growth and their invasiveness may be the most important clinical facts about tumours , but they are not necessarily the most important biological facts . suppose , now , that we accept one variant or another of the view , that malignant cells differ from their normal homologues by the multiplication within them of an exogenous or proprietary virus or mutant plasmagene . if that view is correct , the infective propagation of tumours should be the rule rather than the ( for if we disregard the intervention of virus - like particles in rare exception . the initiation of mammary tumours in mice and in the propagation of the brownpearce carcinoma ( kidd , 1946 ) , the list of tumours or tumour - like growths initiated by viruses seems to be exhausted by the shope papilloma and a variety of chicken sarcomas . ) but what has been said above about the inherent difficulty of demonstrating infective transformationsin normal cells applies without any qualification to those which happen to be mahgnant . 
the limiting factor must be supposed to be , not the actual ' rarity of tumours rendered malignant by the propagation within them of specific virus - like particles , but our technical facilities for extracting them from malignant cells and introducing them into normal cells of a type in which they are competent to flourish ' ; in other words , not the material existence of such particles , but thoir reluctance to display infective behaviour . luckily , infection techniques are not the only ones . 
at our " disposal ; kidd 's ( 1946 , 1948 ) subtle serological analysis of the brow - n - pearce carcinoma has the great theoretical merit of overcoming their almost crippling defects , though it has certain limitations of its own . the interpretation we have put upon the phenomenon of pigment spread in guinea - pigs ' skin was said earlier to have been incompletely demonstrated for this vory reason ; altho - ligh we have the strongest circumstantial and anatomically factual evidence for supposing that the transformation we have been studying is infective in character , we have not yet been able to produce a cell - fiee extract ofpigmentary dendritic cells which will convert white dendritic cells to pigmentary function . 
of extraction are formidable enough ; we may be dealing with a small battery of oxidases , and the existence of at least two , a tyrosinase and a dopa - oxidase , is likely . 
to reproduce its action artificially cannot be technically easy ; we may be obliged in the end to resort to the crude solution offered by microinjection methods . in spite of the rarity of overt cases of infective propagation of tumours , it may nevertheless occur under circumstances in which , being clinically of trivial if the so - called melanotic carcinoma of significance , it has been overlooked . skin is in reality a tumour of dendritic cells , then it is at least conceivable that some melanomas spread infectively by the transformation of their non - malignant neighbours . such spread would be so slow as to be wholly outweighed in clinical importance by infiltrative growth and metastasis , but clinicians may know of certain peculiarities of melanotic growths which such a concept would help to it would be a mistake here , of course , to suppose that the melanotic interpret . character of such growths was itself of anything but secondary importance : some melanomas are recognizable histologically which are barely melanotic . epidermal dendritic cells of human beings , barring albinos , can be provoked into manufacturing melanin ; and an irreversible malignant or pre - malignant change might be initiated in normal dendritic cells by the cytocrine activities of their malignant neighbours before their rapid growth , and rapid elaboration of melanin , gave outward evidence of the fact . since this is a privileged occasion , speculation may be allowed to become wilder still . 
the ordinary literature of tumour transplantation is unhelpful on this point , since stock epidermal carcinomas are normally propagated by subcutaneous ( or some other form of heterotopic ) transplantation from mouse to mouse . 
my reasonsfor considering that the risk is a real one , and of importance , are perhaps best discussed in relation to my own experiments , as i am naturally most familiar with this material . i was iniectin - a dibenzanthracene into some dominant ( lethal ) yellow mice of mainly inbred type , and intercrossing for up to four generations , in order to study the type . 
the tests were on 400 - 800 f . , these results , though consistent , are not significant , males in each group . statistically tinless all three treatments are combined into one group . 
of some interest was the incidental finding of two visible mutants found in the casual inspection of cib c - liltures , which would be an extraordinary occurrence bv rhe drosophila work , too , indicated that the mutants were mere chance . appearing in sperm after removal from the mutagen . 
carr which tends to mutate only those loci that require a relatively small energy this would also imply that these comchange to give a new stable mutation . pounds will tend especially to mutate genes that have already mutated sponthus , although not really specific for any given gene , their effects taneously . may be normally limited to only a small fraction of the genes on the chromosome . but i think that there is a risk with chemicals not encountered with radiation , and this is that a given chemical can react with all , or at any rate a major part of the genes of one type in the animal exposed , as this is merely a repetition of a possible chemical reaction . 
then they might also react with the same genes in another exposed individual equally well , and thus the offspring of two people exposed to carcinogenic mutagens could immediately show an induced recessive . this gives a new problem in human genetics - inbreeding with an occupation . and i have suggested that mutant sperm may be produced long after exposure i don ' t know whether any data on this could be accuto the mutagen ceases . mulated - all i can recall in the literature is the so - called " industrial melanism " of insects described by harrison ( 1920 ) , but i think we should be aware of the risk . 
jackson memorial laboratory , bar harbor , me . received for publication december 16 , 1948 . it is known from the work of andervont and bryan ( 1944 ) and green , moosey and bittner ( 1946 ) that the milk agent is antigenic for the rabbit and the rat . if , as is probable , the agent , is a virus one would expect it to be antigenic for the susceptible species . 
for 30 minutes and then cooled prior to incubation . in experiments 4 and 5 serum from hyper - immunized blacks was used . c57 black mice were injected at weekly intervals as follows : 0 - 1 ml . , 0 - 2 ml . , 0 - 4 ml . , 0 - 8 ml . , 0 - 8 ml . , 0 - 8 ml . 
a few papillomata also occurred . there is a suggestion of neutralization in experiment 2 . however , the probability of obtaining such a result by chance alone is of the order of 10 per it is specially regrettable that this experiment was terminated , as a higher cent . degree of significance might well have been obtained . on the other hand , there is no suggestion of any neutralization in experiments 4 and 5 , where hyper - immune serum was used together with a relatively weak tumour fitrate . 
of special pertinence to experiments with serum from hyper - immunized blacks may be the observations of webster ( 1938 ) and hodes and webster ( 1938 ) with the virus of st . 
louis here a high degree of immunity developed about 6 weeks after encephalitis . vaccination , and had waned before antibodies appeared some 20 weeks after injection . it may be that we bled our mice too soon . possibly our technique was entirely inadequate to show any neutralization . however , identical techniques were used by andervont and bryan ( 1944 ) and green , moosey and bittner ( 1946 )  . 
a strain it may be that this very mice are being constantly immunized since birth . prolonged stimulation is needed for the production of protective antibodies . the fact that the agent can be demonstrated in serum may be due to dilution if this is . 
hamer. from the cancer research laboratories , department of pathology , the medical school , birmingham 15 . received for publication january 13 , 1953 . results for the analysis of thymus histone presented from this laboratory ( hamer , 1950 , 1951 ) have been followed by similar results from other sources ( daly , mirsky and ris , 1951 ; eadie and leaf , 1952 )  . these results all show the same general characteristics in composition but the actual values obtained vary appreciably from worker to worker , suggesting that either the methods of isolation or the source of the material may be affecting the final product . analysis of other nucleo - proteins have been reported by brunish , fairley and luck ( 1951 ) , liver histone , and by khouvine and baron ( 1951 ) , rat epithelioma histone . the last - mentioned paper evidence was presented that different treatments during isolation could yield products of varying composition . 
stedman and stedman ( 1951 ) have also reported qualitative and partial quantitative analyses of a number of basic proteins from isolated nuclei . in the work reported here further analyses of thymus histone are presented along with other results for the non - histone or acid - insoluble protein of the nucleus . all the fractions examined were derived from the same batch of thymus nuclei , and consequently it was possible to study whether the methods of fractionation used caused changes in the amino - acid compositions . 
of defatted calf thymus by the following method : the tissue was homogenised in a blendor , suspended in a total of 2 litres of saline citric acid solution ( 0.14 m nacl , 0 * 025 m citric acid ) , and then centrifuged , discarding the supernatant . 
the sedimented material was washed by alternate suspension and centrifugation in another saline citric acid solution ( 0.14 m nacl , 0 * 01 m citric acid ) , six times in all , the preparation of isolated nuclei was then free of whole cells and had no appreciable cytoplasmic the nitrogen to phosphorus ratio of such a preparation was contamination . 4 - 5 : 1 . 
next a tenth of the volume of a 5 per cent solution of sodium dodecyl sulphate ( sulphonated lauryl alcohol - glover ) in 45 per cent alcohol was added and the ph brought to 5 - 5 . 
the residue from the acid extraction was washed two further times with 0 - 2 m hydrochloric acid , and the remaining insoluble fibrous material was suspended in water , dialysed for 48 hours and freeze - dried ( fraction nr )  . the remaining half of the solution of nuclei in 1 - 2 m saline was shaken with an equal volume of chloroform - butyl alcohol ( 4 : 1 ) to dissociate the nucleic acid and the protethe nucleic acid remains in the aqueous phase ( from which it may be precipitated with alcohol ) , while the protein forms a gel at the interface . this treatment was repeated twice , combining the gel layers obtained . 
the gel was washed three times with the buffered 1 - 2 m saline , agitating and centrifuging each time , and then the protein was thrown down by adding chilled alcohol . 
the precipitate was extracted overnight with 01 m hydrochloric acid , and the acid extract containing histone was worked up as above to give fraction sh , the second histone specimen . 
the residue was washed further with acid and then suspended in water , dialysed and freeze - dried ( fraction sr )  . these four main fractions and the " whole protein " ( dp ) were then analysed . there was insufficient material in fraction r to permit a full analysis , but it is hoped to study this further at a later stage . 
extract with hci whole protein complex ( dp ) nucleic acid histone ( nh ) residue ( nr ) insoluble residue ( r ) shake with chc13 - buoh protein nucleic acid fig . 
the specimens had slightly lower nitrogen contents than those previously examined and contained about 02 per cent phosphorus . the specimen sr of non - histone or acid - insoluble protein was slightly yellowish , and contained a little less nitrogen and more phosphorus than the histones . was insoluble in water , but would dissolve at ph 9 - 10 to give a pale yellow solution 154 d . 
hamer and then precipitated out when this solution was acidified to about ph 5 - 5 . the course of this treatment some unit in the protein is apparently destroyed as evidenced by the production of a strong unpleasant odour on acidification . 
the related specimen nr contains , of course , much nucleic acid in addition to proestimated from the phosphorus content and the absorption spectrum tein . there is approximately 56 per cent nucleic acid in this fraction . in dilute alkalis an opalescent viscous solution is obtained . finally , specimen dp precipitated from the solution of isolated nuclei by sodium dodecyl sulphate has a nitrogen content of about 9 - 8 per cent indicating that the ratio of protein to detergent is around 3 : 2 by weight . 
the act of separating the non - histone protein from the nucleic acid apparently damages the protein , and it does not seem possible to obtain it in other than an insoluble and denatured forthis would suggest that the non - histone protein may be chemioally bound to the nucleic acid while the histone is held by a predominantly ionic union . 
some support for such a structure has recently been presented by fleming and jordan ( 1952 ) , who have found that the results of eleotrophoretic studies on thymus nucleoprotein in solutions of varying ionic strength could be explained by the existence of an equilibrium np np + p ' ( where np is the original nucleoprotein , np a nucleoprotein fraction with a higher nucleic acid content , and p ' a dissociated protein )  . 
however another possibility is that in the cell the histone is loosely combined with the non - histone protein and that acid treatment breaks the compound open . this would be in accord with the close similarity of amino - acid composition , but would require that all the cystine and tryptophane remain with one fraction on fission . 
the first possibility considered seems on the whole to be more probable , as it is more in keeping with the variation in the amounts of histone and non - histone protein in the nucleus of different cell types ( hamer , 1951 ; stedman and stedman , 1951 ; mirsky and ris , 1951 )  . in the case of the thymus nuclei studied here the histone and non - histone proteins occurred in roughly 156 d . 
it seemed likely that 1131 would prove so since it is specifically concentrated in the thyroid , whose cells are thereby submitted to a course of ~ - ray irradiation . 
the problem is important , sirice we do not yet know the carcinogenic hazard of 1131 in clinical medicine , where it is being increasingly used both tracer and therapeutic doses . 
hyperplasia and adenomas of the thyroid have been produced by goitro gens ( griesbach , kennedy and purves , 1945 ) , and by goitrogens together with the carcinogen acetylaminofluorene ( a.a.f. ) ( bielschowsky , 1944 )  . 
when the following work was started in february , 1948 , there were discrepancies in the literature as to the incidence of thyroid tumours in untreated rats and the carcinogenic potencies of goitrogens , which were due to the different rat strains , ages and living conditions , times of application of the in view of the discrepancies and in order drugs and criteria of malignancy used . 
the rats were killed by coal gas_ at an average age of 15 months , having had treatment for an average of 13 months ( including the rest period )  . 
the trachea and thyroid attached was fixed in helly 's fluid ; the thyroid was then dissected off the trachea and weighed to the nearest milligra the thyroids were embedded in wax , serially cut at 5 and mounted on to slides as ribbons of 8 to 14 sections , including both lobes . 
the number of rats used was 98 to obtain data for the main experiment , at the end of which the remaining 15 from various groups were put aside for study of the thyroid ! 131 uptake by direct measurement and autoradiography . 
 the indication of adenomas by plus signs in tables i , ii , iii , iv and v is not devised to be any more than a crude indication of tumour incidence ; the object was to seek for major rather than minor differences resulting from the various treatments of these small numbers of rats . 
 i have not given a detailed description of the histology and histogenesis of the adenomas , because in addition to the references cited in the introduction , there have appeared further detailed illustrated descriptions by purves and griesbach ( 1947 ) , money and rawson ( 1947 ) , laqueur ( 1949 ) , and hall and bielschowsky ( 1949 )  . 
 nil + + + + + + + + + nil female * number of months before the rats were killed when they received the first of their two injections + represents i adenoma per gland ; + + , 2 or 3 adenomas ; + + + , multiple adenomas . 
in many areas it was difficult to differentiate the adenomas , and the number of plus signs awarded in the thyroid adenoma column of table ii is probably an underestimate . 
however , the cells of these extra and intracapsular and juxta - venous follicles were quite innocent in appear ance , and in no way different from those constituting the main mass of the glands . 
the effect of the 1131 was such that every one of the glands in this admittedly small group showed a most striking increase in adenoma formation as compared with the rats treated with methylthiouracil alone . 
 female male 10 14 14 14 14 17 11 11 14 14 14 15 14 14 14 11 12 12 11 11 died killed died killed died kiiied di~d killed di~ died killed died killed 229 thyroid adenomas . 
 100 168 100 129 136 116 120 160 125 130 110 125 130 155 110 120 130 125 140 130 175 117 119 125 120 108 124 107 acetylaminofluorene + methylthi , ouracil + radioactive iodine . 
 the adenomas were larger in size as well as increased in number , and showed evidence of malignancy by a gross increase in size and by dissemination outside the thyroid in two instances . 
secondly , as shown by autoradiography ( leblond and gross , 1948 ; doniach and pelc , 1949 ) , there is a wide variation in concentration from follic ] e to follicle ; the peripheral follicles in the rat take up considerably less iodine than the central ones . 
the radiation effect~ are due mostly to radiation , since most of the y rays , which are much more penetrating , will not be absorbed in the small thyroid of the rat . 
they found that this radiation did not interfere at all with the ability of the thyroids to take up further iodine , produced no histological changes , and showed no alteration of thyroid function as gauged by various physiological tests . 
their rats averaged 40 per cent maximal uptake of psi , ours was nearer 20 per cent , and our total psi injected was 32 , theirs was 30 c . , therefore our dosage was roughly 15 , 000 roentgen equivalents physical . 
from the long - term view in our experiments this dosage proved damaging , as shown in table vi , where it can be seen that the thyroid weights of all psi treated rats in all groups was one - half to one - third of their respective controls . 
clearly though , enough thyroid had survived to maintain normal growth of the rats , since the body - weights did not differ from their respective controls in spite of the fact that the first dose of psi was administered at an average age of 2 months . 
methylthiouracil rat killed 12 days after cessation of 13 months ' treatment , showing intense blackening over t , he colloid of the normal follicles and less intense but definite blackening over the colloid secreted by the adenoma lying in the centre of the photomicrograph . 
this is the accepted mechanism for the goitrogenic action of anti thyroid " drugs , such as thiouracil ( astwood , sullivan , bissell and tyslowitz , 1943 ; mackenzie and mackenzie , 1943 )  . 
nevertheless , this nodular hyperplasia must be regarded as a definite deviation from the normal , akin to tumour production both on morphology , and on the grounds that it may lead to malignant change as shown by previous and the present work . 
this may well be due to the fact that the dosage of pat used was destructive enough to the thyroid temporarily to diminish thyroxine formation , and thus step up thyrotrophic hormone production . 
it is interesting to note in this connection that the same number of rats showed adenomas in the pat group ( table ii ) as in the methyl thiouracil group ( table iii ) , and that the number of adenomas was greater in the former group . 
 the problem remains as to why the controls show an occasional deviation from the normal in the formation of adenomata , and how does prolonged excessive thyroid stimulation by the pituitary intensify this deviation , and by what means additional carcinogen leads to a further increase in adenomas . 
experimentally , gorb man ( 1947 ) found hyperplastic thyroid tissue within the lumens of pulmonary vessels of chronically thiouracil treated mice as well as parenchymatous pul monary deposits considered to be probably thyroid in orig yet a return to normal diet after prolonged goitrogen treatment was followed by involution of the supposedly cancerous thyroids . 
one may assume , therefore , that two types of metastatic thyroid tissue exist , one , possibly resulting from a mechanical breakaway , still dependent upon thyrotrophic hormone for its survival , the other independent . 
neverthe less , from the host 's point of view the first type of metastasis may prove just as embarrassing as the second , so long as thyrotrophic hormone stimulation is main tained . 
prolonged thyroxine treatment , used in clinical medicine in the therapy of nodular goitre , may , by inhibiting thyrotrophic hormone production , not only shrink the goitre , but lessen the likelihood of mechanical production of thyroid metastases and of their survival . 
the radioactive iodine was found to significantly increase the formation of thyroid adenomas as compared with non ! 1 31 treated controls in the following groups : those treated with ! 131 alone , those treated with methylthiouracil and those treated with methylthiouracil plus acetylaminofl.uorene. 
some of the authors misrepresent their own data , misquote those of others , are defective in arithmetic and make the task of anyone who wishes to examine their conclusions difficult . some authors , when giving data for the incidence of cancer other than uterine , do not say whether the figures refer to one or both sexes ; and in statistics based on admissions to a hospital they do not say whether this is a women 's hospital or a general hospital , or where the hospital is situated , data which are not always easy to obtain in another country . 
the age distribution of these 7 cases was as follows : 30 - 40 , 1 ; 40 - 50 , 2 ; 50 - 60 , 2 ; 60 - 70 , 2 . the seven cases of uterine cancer in jewesses which appear in table ii appear to be identical with those in table iii . * this is a very high percentage , for which theilhaber shows no detailed evidence . deaths of women from all forms of malignant disease deaths from malignant disease of the uterus the registrargeneral 's statistical review ( 1935 - 1939 ) gives the following figures for england and wales for the five years 1935 - 1939 :  . 
sanders ( 1916 ) gives data from rotterdam ( table x ) which show a low incidence of cancer of the uterus in jews , and a still lower incidence upon members of two of the protestant churches ( christian reformed and reformed )  . 
about one per thousand of the population . the radiumhemmet serves a well - defined area of the country which covers about half of the population . since 1914 practically all cases of cancer of the cervix occurring within that area are referred to the radiumhemmet for treatment . from 1914 to 1947 inclusive i have seen about 7000 cases of cervical cancer . among those were three jewish women . 
he considered that this was almost certainly an hereditary factor and not likely to be due to special observances of the jewish law , the same facts being noted in unorthodox jews . * unfortunately karplus gave no figures in support of this statement . 
data showing an equally low incidence of cancer of the uterus , which is more difficult to demonstrate than a high incidence , in populations known to consist of orthodox , and of unorthodox jews must have been difficult to obtain and would be of great interest . * i am indebted to d . 
100 table xi shows that cancer of the uterus , reckoned as a percentage of all cancers ( fishberg does not make clear whether the figures refer to females only ) is less than one - half as common among jewish women as among other races , while cancer of the breast shows a smaller difference in the same direction . smith ( 1941 ) studied the racial incidence of 3106 cases of cancer of the cervix observed at the memorial hospital , new york , from 1916 to 1937 . 
he says : " in an attempt to compare the nationality incidence in cervical cancer in this series with that of patients suffering from other gynecological lesions , consecutive records as filed have been studied , but the numbers used in each classification are not the entire number of patients filed under that diagnosis ; i.e. , this is a cross section of the clinic in the years studied rather than the total number of cases in the clinic . " i have been unable to learn from the memorial hospital the system upon which the cases making up this " cross section " were selected . apparently a number of cases of other gynaecological conditions roughly equal in number ( 3062 ) to those of cancer of the cervix ( 3106 ) were taken . 
the results are summarized by smith in tables xii and xiii ( his tables iv and iva )  . the significance of these figures is affected by the very high proportion of benign tumours , hence in table xiv and xiva smith 's figures have been recalculated for the malignant tumours only . in table xiv the result of the whole investigation , which for some reason smith does not give , namely , the ratio of cervix cancers to other conditions , is calculated from his figures . 
3106 6168 3062 vineberg ( 1919 ) gives data for the incidence of cancer of the cervix based upon material from 80 , 000 female patients at the mount sinai dispensary and hospital , table xv represents an attempt to reduce his rather confused statenew york . ment to a clearer forthe higher proportion of cancer in the hospital cases as against those of the dispensary is attributed to better conditions for examination . vineberg ( 1919 ) points out that jewesses of the poorer classes , to which most of those dealt with in his paper belong , are most likely to be orthodox in religious matters . 
the authors suggest the possibility that this difference certainly the age at which some forms of cancer depends upon racial factors . occur is affected by genetic differences ; examples have been given in detail in another paper ( kennaway and kennaway , 1944 )  . but there is nothing in these data for age distribution to indicate whether the liability to uterine cancer , which is the chief subject considered here , is affected by racial or by extrinsic factors . 
cancer of the uterus in hindu , moslem , parsee and indian christian women . statistics based upon attendance at hospitals are notoriously liable to error , more especially when they refer to people differing in race and religion . however , the following figures ( table xxi1 ) should at any rate encourage further investigation . 
they are taken from the valuable collection of data on cancer in india obtained by nath and grewal ( 1935 ) from the records of in - patients of 13 hospitals in punjab , delhi , united provinces , and bihar and orissa , comprising 6395 cases of cancer in all . 
cancer of the uterus in china . maxwell ( 1929 ) in his book " the diseases of china " says : " it is probable that uterine cancer ranks highest of all in the malignant growths in this country . 
the women are classified according to the husbands ' occupation into four main classes , with 14 numbered and 35 named sub - divisions . in table xxvii , only the four main classes are quoted . theilhaber does not state the populations of these various groups , and makes figures for the age distribution no comment upon this very serious deficiency . of the populations of these classes were not available . 
the object of the preliminary bath was not cleanliness per se , but the removal of anything which would intervene between the skin and the water during the total immersion , and thus deprive this ritual of its efficacy.t some medical writers have emphasized , in rather vague terms , the importance of the cleanliness enforced by the mosaic law , hence it is important to note exactly what the law requires . 
the washing , in a normal woman , at the beginning and end of the seven days , adds two baths a month to whatever other ablutions she may carry out . * this account of jewish ritual immersion is taken from various articles in the jewish encyclopedia ( 1891 ) , from ploss , bartels and bartels ( 1927 ) and from preuss ( 1923 )  . 
one might form some estimate in london from the number of public ritual baths available , which are said to be not more than half a dozen ; there are also some private ones . 
but it seems probable that many women who do not go to the ritual bath may conform to the law in other respects , namely , the first and second bath , and abstention from intercourse , which are matters of purely private conduct . the mosaic law ( leviticus xii , 2 , 5 ) relating to child - birth is important in view of the association of cancer of the cervix with parity . 
 " if a woman conceive seed , and bear a man child , then she shall be unclean seven days ; as in the days of the impurity of her sickness shall she be unclean . . 
but if she bear a maid child , then shall she be unclean two weeks as in her impurity : and she shall continue in the blood of her impurity three score and six days . " thus the whole period of impurity was either 7 + 33 = 40 , or 14 + 66 = 80 days . 
the practice in this country at the present time is said to be , to observe rather longer periods , of two and three months respectively . ( b ) moslem law . the koran ( sura 2 ) gives directions for the purification of women which are much less precise than those of the jewish law . 
a flow of blood lasting more than nine nights is the work of evil spirits . modi ( 1922 ) , a parsee , quotes these laws and says : " at present also , most of the parsee women generally observe the above practices . there are no separate dastanistans or houses for menses in parsee towns or streets , but generally a sequestered part of one 's own house is chosen for the purpose . the downfloor of the house was thought to be the proper place . 
but nowadays , in a crowded city like bombay , the down - floor , instead of being a quiet and healthy place such as that contemplated by the early injunctions of the vendidad , is so , most women in menses pass the period of generally quite the contrary . menstruation on their upper floors , but in an isolated way . 
in the matter of taking food , very few use spoons now , though up to about 25 years ago , that was generally the case . in the matter of purification , they observe the bath enjoined by the early books , but the vendidad injunction of bathing over the three " magas " is not observed at all . 
a separate place of bathing and for purposes of nature for women in this condition is generally provided in parsee houses . " ( d ) hindu ritual . khanolkar ( personal communication ) says that the parsee laws regarding menstruation are almost identical with those practised by orthodox hindus and probably both of them are derived from early aryan ritual . 
the abbe dubois ( beauchamp , 1906 ) , writing about the beginning of the nineteenth century , quotes from the book padma - purama , reputed to be the work of the hermit vasishta , a rule for a 3 - day p3riod of isolation for the menstruating woman , followed by a day of ceremonies and ablutions , including 36 total immersions in a river . 
during the three days "  . the mere wish to cohabit with her husband would be a serious sin . " elsewhere he says , " the mother of the newly - born child lives entirely apart for a whole month or more , during which time she may touch neither the vessels nor the furniture of the house , nor any clothes , and still less any person whatsoever . the time of her seclusion being over , she is immersed in a bath , or else a great quantity of water is poured over her head and body . women are similarly isolated during the time of their periodical uncleanness . in all decent houses there is a sort of small gynaeceum set apart for them ; but amongst the poor , in whose huts there is no such accommodation , the women are turned into the street , under a sort of shed or outhouse , or else they are allowed a corner of the cowshed . . 
when the time of uncleanness is passed , all the garments that the woman has worn are given to the washerwoman . her clothes are not allowed inside the house ; in fact , no one would even dare to look on them . " jhaveri ( 1910 ) says that in all hindu religious books minute directions for during the first four days of the first baths on very many occasions are given . menstrual period everything which the girl touches must be washed and " 202 e . 
nor do married women abstain procreation is almost a matter of religious observance with from child - bearing . uterine cancer ought to be , if anything , more the mass of jewesses . common among jewish women than among non - jewish . " various talmudic writers ( epstein , 1936 , 29b - 30a ) laid down that a father should cause his sons to marry at 16 to 24 , or 18 to 24 , and that a daughter should " be dowered , clothed and adorned , that men should eagerly desire her " ; no age is stated at which a woman should marry . 
a modern compiler ( abramowitz , 1900 ) states the law of israel on this matter thus : " after a man has arrived at the age of 18 it is his duty to take unto himself a wife in order that he may be fruitful and multiply , at any rate he should not pass his 20th year without having taken a wife . having begotten a son and a daughter who are also generative , one has fulfilled  . 
the command " to the commandment " to be fruitful and multiply . " be fruitful and multiply " is not obligatory upon women ; nevertheless a it is woman should not remain single lest she be liable to suspicion . one of the mandates of the sages that a man shall give his sons and daughters in marriage immediately they approach maturity . these jewish practices thus laid down in the law , and described by sorsby as prevailing at the present day , should encourage early marriage . the abb6 dubois ( beauchamp , 1906 ) says that "  . . 
thus 45 per cent of women with cancer of the cervix , and only 16 per cent of those with cancer of the breast , were married before that age . " variables which might be considered are : earlier childbirth , multiple children , poor obstetrical service , longer duration of married life , syphilis , immaturity of tissues at time of marriage , and excessive hormonal stimulation . " of these factors , longer married life could be eliminated by comparison with other groups . 
circumcision. some authors ( handley , 1936 , 1947 ) consider that no explanation of the lower incidence of cervical cancer upon jewesses need be sought beyond the ( assumed ) difference in the bacteriali flora of the female genital tract brought about by this factor , a matter which it would be possible to investigate . more data from moslem populations who practise circumcision , and from parsees , who do not , are obviously very desirable . handley ( 1936 ) has emphasized the value of statistics from fiji , where the natives practise circumcision , in contrast to the hindu immigrants , in whose native country phimosis and cancer of the penis are very common ( kennaway , 1947 ) ; certainly if these two races could receive equal medical attention interesting results might be obtained.t circumcision might act in another way , not dependent upon bacterial action . phimosis , cancer of the penis and cancer of the cervix appear to be common in * see " the racial origins of jewish types , " by radcliffe n . 
we have no data which give directly the respective social incidence of cancer of the cervix , and of the corpus , but information should be available from hospitals which have separate accommodation for paying and other patients . 
2. - age at death from oanoer of uterus in bamberg , augsburg , wuirzburg , erlangen , niirnberg and the provinoe of unterfranken , 1908 , and in munioh , 1906 - 7 - 8 ( theilhaber , 1910 )  . 
the jewish ritual has some unique features . more or less complete isolation of menstruating women is practised by many other peoples and is laid downi in the religious literature of some of these ( koran , zend - avesta , dharmasindhu )  . some quite primitive peoples ( aleuts ; natives of the congo and of australia ; for references see ploss , bartels and bartels ( 1927 ) ) are stated to enforce isolation at the menstrual period for as long as 6 to 7 days . 
one might make the following suggestions for further investigations : ( a ) an inquiry into the incidence of cancer of the cervix in jewish women who observe the 12 - day period , the ritual immersion being disregarded . 
all of the twenty collections of data which have been found in the literature show an incidence of uterine cancer which is greater on non - jewish than on jewish women . 
these data are calculated upon several different bases and hence are not all comparable . seven authors express the figures for cancer of the uterus as a percentage of all cancers in women , which percentage ranges from 28 to 14 in non - jews , and from 10 to 4 in jews , the mean values being 20 and 7 . 
the very scanty data available ( 25 cases only ) show a much lower incidence of cancer of the cervix on parsees . this might signify that so short a post - menstrual period does not affect the matter one way or the other , anid this difference in liability to cancer must then be due to other factors . 
cancer of the uterus appears to be prevalent in some peoples ( hindus , chinese ) among whom phimosis and cancer of the penis are also common , while the moslem women of india show a lower incidence . 
but any attribution of this difference to the practice of circumcision by moslems is very doubtful in view of the similar low incidence on peoples ( parsees , indian christians , possibly some dutch ) in whom this factor is absent . 
the only numerical data on the social incidence of cancer of the uterus appear to be those from bavaria 40 years ago , and from england and wales , after the last census , in 1930 - 32 . 
the unavoidable mixture , in large - scale statistics , of cancers of the cervix and of the corpus uteri , is unfortunate , as these two forms probably differ in etiology . 
harnett. published for the clinical cancer research committee of the british empire cancer campaign . received for publication july 16 , 1948 . in 1938 - 39 the clinical cancer research committee of the british empire cancer campaign carried out a clinical survey of all cases of cancer seen in the hospitals , both voluntary and l.c.c. 
in the administrative county of london . this was done by means of questionnaires , one of which was filled in by the registrars in the various hospitals for each patient and returned to the clinical cancer research committee for record . 
the work was interrupted by the outbreak of war after it had been in progress for 17 months . by this time 15 , 200 cases of cancer had been registered , of which 2529 ( 16 * 6 per cent ) were cancer of the breast . these patients have now been followed up for five years or more and the records analysed . 
 * from the department of experimental pathology and cancer research , school of medicine , leeds , 2 . received for publication august 11 , 1951 . ' thf , need for devising a technique for testing the carcinogenic properties of chemical compounds by direct application to the bladder epithelium has been felt for some time . 
yamazaki and sato ( 1937 ) described a method of introduction of oily solutions of chemicals into the rabbit bladder by catheterization . interpretation of the true nature of the one acceptable tumour described by these authors after the introduction of o - aminoazotoluol is complicated by the presence in an extensive series of of lipoid in phagocytes in the subepithehal tissues . experiments , hughes ( 1949 ) , by means of epithelial grafts wrapped around 20methylcholanthrene crystals , obtained 14 transplantable carcinomas from 120 attempts . 
by this method an even distribution of the carcinogen was difficult to obtain , and so considerable variation in concentration may have occurred . under ether anaesthesia the bladder was exposed by a small incision through the skin and abdominal wall about i cabove the urethral opening . 
the bladder was drawn out of the abdomen and supported on a small pad of gauze ; an incision was then made through the dome of the bladder and the edges held apart by small metal retractors . 
the suture passed through all the layers of the bladder wall , and the edges were drawn together so that the two epithelial surfaces were bound closely to one another ; thus a continuous epithelial layer only and no muscle nor connective tissue was exposed to the direct action of the carcinogen in the pellet . 
the abdominal wall and skin were closed separately by sutures of cotton or thick silk . the operative mortality was negligible , but a number ' of animals died within a few weeks of the operation due to the pellets blocking the urethra . 
the latter concentration had been found previously to be effective in inducing subcutaneou 's tumours , both sarcomas and breast adenocarcinomas ( bonser , personal communication )  . in the present experiment pellets containing 2 per cent of the carcinogen induced bladder epithelial h erplasia but not tumours , whereas a pellet containing 30 per cent induced an infiltrating cancer . 
no doubt lower concentrations would be equally effective . this technique has the advantage that an ' substance so apphed to th ' e bladder is subject only to the action of the urine be ' fore coming in contact with the bladder epithelium ; thus metabohc changes in chemical structure subsequent to feeding or injection are obviated . 
a reasonably high i ' ncidence of tumours should be obtained with an active substance without incidental induction of sarcomas . it should now be possible to determine whether metabolites of bladder carcinogens such as 2 - naphthylamine are ' tho active agents in inducing bladder cancer . economy in time , animals and material can be effected , and this is important when investigating the carcinogenicity of small quantities of metabolites isolated from urine . 
bartholomew 's hospital , and the statistical research unit of the me - dical research council , london school of hygiene and tropical medicine . received for publication february 20 , 1951 further data on the arsenic content of cigarette - 3 . in an earher paper ( daff and kennaway , 1950 ) data were given for the arsenic content of 5 brands of cigarettes of british and american types , of 8 brands of turkish type , and of two - others ( french , rhodesian ) , and also for the amount of arsenic volatilized in smoking . 
and germany are those of saglam ( 1944 ) from turkey and of dungal ( 1950 ) from iceland . ( 4 ) population by aores . ( 2 ) number of autopsies showing cancer . the data which one would like to obtain from any given country are : a . 
from univer8ity clinic8 ( for men and women separatelv - preferably by ages )  . - ( i ) number of autopsies . number of autopsies showing cancer of lung . in the countries where a ( 5 ) is not available one must rely on b . 
le hastaliklari klinigi in 23 months ( among 2084 patients , 53 in a thousand )  . " cc all these statistics show that in our country , within the last 30 years , pulmonary carcinoma has increased in a great proportion . " saglam rejects cigarette - smoking as a factor in the incidence of bronchial " some authors believe that there exists a relationship between carcinoma . smoking tobacco and inhahng the smoke and pulmonary carcinoma . 
we do not hold for a long time , at least since 50 years , almost only cigarettes the same view . in spite of this the increase in pulmonary ca . 
kennaway data for 1934 and have removed 3 cases , all in men , described as benign tumours , from the total of primary lung tumours ( a chondroma in 1935 , another in 1939 , and a polyp in 1937 )  . 
the official figures for tobacco consumption ( hutson , 1937 ) and for population ( statesman 's year book , 1931 ) indicate an annual consumption of about 17 lb . 
he writes that the kinds of tobacco smoked in yugoslavia ( b ) type hercegovina ( cigarettes ) ; and are : " ( a ) type makedonija ( cigarettes ) ; ( c ) type vojcodina ( pipe and cigars )  . " these are of the oriental type , i.e. , they have a natural ' bouquet ' which gives the tobacco type makedonija . " only in the north - western part of yugoslavia there are smoked cigars and pipe . 
use of tobacco for snuffing is quite insignificant . before the last war the only import was some dutch tobacco for cigars - ; during the war some bulgarian and after it some american tobacco ( through u.n.r.r.a. ) was imported , but all these amounts were very small . we are also indebted to kosir and to f . 
among 20 , 681 autopsies , there were 3584 cases of cancer and 276 cases of cancer of the lung . these figures are compared with those from other countries in table ix . ( 3 ) it is , however , not necessary to be dependent on hospital statistics for an estimate of the incidence of cancer of the lung in switzerland , as vital statistics are available for - the whole country . 
the calculated death rates from cancer of the lung are shown in table x . the national figures are reasonably reliable ' as , according to jakobsen , " the doctor who has treated the deceased during his last illness is required to which must be fill in an official certificate stating the cause of death stated in medical terms as precisel.v as possible , and it is not permitted to use general diagnoses such as " disease of the heart " or " disease of the lungs . " the 16fl ravii i 12 . 
kennaway clearl no exact proportionaht however , reasonably close to the difference in cigarette consumption . in switzerland tobacco consumption was much the same as in england and wales , but death rates were only half as high . differences in cigarette consumption again agree with the differences in death rates better than do differences in total tobacco conthis is because a much smaher proportion of the tobacco is consumed sumption . in the form of cigarettes in switzerland than in england . has been found in the data so far available between the amount of tobacco smoked and the prevalence of cancer of the lung cancer of the lung appears to in different countries and at different periods . increase more rapidly than does the use of tobacco ; such a change in effect may occur at a certain level in the dosage of a drug . 
the figures from a single hospital in yugoslavia suggest an incidence of cancer of the lung comparable to the british figures of 30 years ago . we have no figures for the incidence of cancer of the lung upon the whole population of any east european country . 
the e - vidence available at the moment is against the direct carcinogenic importance of tobacco smoke , because it tends to exclude the two most obvious carcinogens , arsenic and benzpyrene , which one might expect to be present . 
known carcinogens is now so wide that one must consider other possibilities . ( 3 ) all the older data about cancer of the lung must be reviewed in the light of this connection with smoking ; one must reconsider the inverse relationship with sunhght ( stocks , 1947 ) and the very low incidence upon a rather curious - assortment of occupations , namely , agriculture , coal - niining , and mule - spinning ( kennaway and kennaway , 1947 )  . 
one cannot answer this question at present , but it is especiary important in countries where smokers buy the cheaper pipe tobacco to make their own cigarettes . norway one obtains in this way nearly twice as many cigarettes for a given sum ( jakobsen , personal communication )  . 
the incidence of cancer of the lung upon the two sexes is not very different ( death rate , male to female , i : 07 ) ; it is greater in urban than in rural districts , and this difference is greater in men than in women . 
the increase in mortality in the last 20 years has been greater in men than in women , and greater in the towns than in the country . ( 5 ) in sweden , snuff makes up a much larger fraction ( one - third in 1949 ) of the total tobacco products consumed than is recorded in other countries . ( 6 ) a comparison is made of the data available for the increases since 1931 in ( a ) deaths attributed to cancer of the lung , and ( b ) in the consumption of tobacco , in england and wales , norway and switzerland . 
the consumption of tobacco per head has been for the last 10 years rather higher in switzerland than in the united kingdom , and in norway has been about one - half that in the other two countries , while the crude death rates at the beginning and end of the period were m . 
kennaway rou - ahlv in the proportion of i 0 ( england and wales ) to 5 ( switzerland ) , and 2 cigarette consumption was approximately in the proportion of 4 ( norway )  . ( england and wales ) to 2 ( switzerland ) and i ( norway ) and was more in accord with the relative death rates . 
the increase in the number of deaths has been about the same ( twofold ) in all three countries , but the increase in consumption oftobacco and cigarettes has , been ' less . 
the differences in the incidence of cancer of the lung are therefore quite different in extent from those in the quantity of tobacco consumed ; they are m ' ore hke ( though stir different from ) those in the quantity of cigarettes consumed . 
the study of the relation between the national consumption of tobacco and the national incidence of cancer of , the lung has scarcely begun . we wish to thank saglam and prol p . 
westlake avenue , l08angele8 , california . received for publication january 19 , 1951 . huggins , miller and jensen ( 1949 ) studied the thermocoagulability of the serum protein in health and disease in the presence of an extrinsic inhibitortheir results , however , while showing an abnormal behaviour iodoacetic acid . fo ' r mahgnant and certain non - mahgnant diseases , tend to establish a seeming relationship between cancer and tuberculosis . 
serum m micromoles of sodium iodoacetate in the nearest where 05 tube containing a firm clot preceding a tube in which the coagulum is a " shapeless viscous mass , .. 
or in the ori inal state before boiling . the serum protein determinations were carried out by the semi - micro kjeldahl procedure recommended by huggins , miller and jensen ( 1949 )  . every fifth determination was duplicated with an average agreement of 0 - 5 per cent . procedure was frequently checked for accuracy for the recovery of 5 - 0 mg . quantities of nitrogen by carrying out a complete determination with 23 - 6 mg . quantities of anhydrous ammonium sulfate with recovery in duplicate being 0 - 02 to 0 , 03 mg . 
the two myelomas were r - eceiving nitrogen mustards ; the leucaemias , x - rays and / or transfusions ; some of the advanced cases , polysaccharides or chymotrypsin ; eight of the breast cancer cases , testosterone . 
none of the patients in groups i and ii received any special diet , except that the most advanced , uncontrolled cases were getting either plasma transfusions or protein hydrolysates of one kind or another . all of them received an iron - vitamin preparation . 
for the series of cases in group iv merely reflects the ratio of concentration of iodoacetate as an inhibitor of coagulation for decreasing quantities of serum protein . there is no evidence that age distribution of the group tested played any significant role in the ratios obtained for the i.i. discussion analysis of the factors involved in the procedure showed that the coagulability of 52 per cent of the group i sera is abnormal for entirely different reasons from the sera ofgroups 11 and iii . 
evidence for this lack ofhomogeneity between the protein values and the degree of positive h.m.j. , obtained for tubercular sera and the sera from new untreated cancer soon became apparent , i.e. 
to the group i patients . in some the " positive " was altered to " negative , " andin there was good agreeothers the positive results became more or less positive . ment , however , for the i.i. 
values established by both kjeldahl and falhng - drop methods of protein estimations , for the remah - iing groups of cases . this led us to consider an " aberrant " or " combined - protein " as being responsible for the striking disagreement with the h.m.j. 
for the two types of disease . the possibihty that we were deahng with an increase in one of the normal fractions of the serum , the alpha globulins , reported to be increased in mahgnancy , led us to carry out the test on a sample of mucoprotein from cancerous serum , generously supphed by richard winzler , of the department of biochemistry , of the university of southem califomia , and a " bence jones " protein , isolated from the urine of one of the two myeloma cases in this series . 
neither ofthese substances yielded a positive i.i. if , as others have observed , the degree of increase of alpha globuhn is proportional to the severity of active tissue destruction , then apparently the alpha globulin plays no part in the huggins test , either for advanced tuberculosis , which certainly involves active tissue destruction , or in the early and new untreated cancer cases in our study . the question of the existence of modified serum protein molecules in various disease states , including mahgnancy , has been discussed recently by one of those whose published data estabhshed a close correlation between plasma viscosity , and the severity of the organic changes ( harkness , 1949 )  . 
added emphasis that we may be dealing with an altered protein in malignant tumours is given by the experimental observations ofhellwig ( 1949 ) , who found that as a rule the size ofspherical bodies in the form ofclusters , short - chains and aggregates from tumour extracts when examined by electron microscope was exceeffingly larger than that in benign or normal tissue . 
he concludes that these globules are not virus - like causative agents of cancer , but rather globular proteins , probable aggregates of the cytoplasmic globules due to an alteration in the cohoidal state of the cancer it is quite possible that this cytoplasmic material may be introduced into cell . the blood serum and may play a role in accounting for the positive i.i. 
duboff subjective element in the estiniation of the coaguluthe task for the future is the elimination of this factor , perhaps , by measuring the degree of coagulation by an appropriate electronic procedure characterized by the electrical resistance or potential of the coagulum . can one explain the paradox of the 22 negative h.m.j. 
tests have a pattern of deformation in one direction , it is not inconceivable that the former 22 cases have - a pattern of deformation in another direction that is not manifested in the test through the present combination ofreagents . 
furthermore , if the mechanism of action of this method is due to the increase of net negative charges on the protein molecule by the addition of sodium iodoacetate , then our results strongly suggest variations in the polar character of the proteiii molecule in the serum of certain phases of tumour development . the magnitude of relationship between absolute protein per cent and the ll demonstrated by group iii serum does not reflect the magnitude of the effect , when apphed to group i . 
the term " false positive " cannot be apphed ' there - t fore , to such tuberculosis sera , in the same sense as the term " positive " is applied to that of early cancerous sera , since the term " positive " itself is not tenableon the same basis . 
the serum of individuals undergoing some type of degenerative process , appears to possess an admixture of some elements , the source of which we do not yet comprehend , but the presence of which has been demonstrated by measurable function of the thermocoagulation of protein in the presence of an extrinsic inhibitor , iodoacetate . tentatively , we are inclined toward the conclusiozi that abnormality in the blood serum of some cancer patients , unhke that of some tuberculosis blood with a corresponding i.i. 
it is suggested that the use of the expression " false positive " or " pseudo positive " be elimiiaated from the terminology of cancer tests . the ' author wishes to tender his sincere thanks to clyde k . 
lipschutz. from departamento de medicina experimental , servicio nacional de salud , avenida irarrazaval 849 , santiago de chile . received for publication april 2 , 1953 . the tumours which appear in the intrasplenic ovarian graft in castrated rats , mice , guinea - pigs or rabbits apparently are due to the uncontrolled gonadotrophic activity of the prehypophysis , the ovarian steroid hormones which normally control hypophysial activity being inactivated during their passage through the liver before reaching the general circulation ( iglesias , mardones and lipschutz , 1953 )  . 
we shall be able to show ( 1 ) that this is not the case , and ( 2 ) that the hormonal imbalance from which ovarian tumourigenesis under the given experimental conditions derives can , and must , be expressed in quantitative terms . for the purpose of this study the secretory activity of 15 intrasplenic grafts , as listed in table i of our previous paper ( iglesias , mardones and lipschutz , 1953 ) has been checked by the histological examination of the vaginal mucosa . the uterus and the mammary glands . 
the presence of ovarian hormones in the general circulation at a level allowing for the transformation of the vaginal mucosa and of the uterine epithelium , even with the production of cystic glandular hyperplasia and metaplasia . 
rus. * pregnancy = several layers of clear vacuolized epithelia . * * transition = several layers of proliferated cells of the basal epithelium beneath the vacuolized layers as in fig . 
as evidenced by various new observations , we must drop the idea held originally both by biskind and by ourselves as to the gonadotrophic activity of the hypophysis in experiments with intrasplenic ovarian grafts in castrated females : contrary to what we thought before , the hypophysis is , under these experimental conditions , not identical to a castrate hypophysis . thus , the content of gonadotrophic hormones in the hypophysis of animals with grafts is considerably less than in the castrate hypophysis ( jungck , heller and nelson , 1947 )  . indeed this non - identity may be due to a difference , not of production , but only of release of gonadotrophins in castrated and grafted animals ( miller and pfeiffer , 1950 ) ; but non - identity seems to be a fact . castration cells are absent in the hypophysis of the grafted rat , in 224 2 . 
lipschutz any case in advanced stages of ovarian tumourigenesis ( lacour and guerin , 1951 )  . however , as compared to a normal hypophysis , that of a castrated animal with an intrasplenic ovarian graft is functionally impaired . differential tumourigenic thresholk concentrations of oestrogen . the problem of differential levels of oestrogen by which control of the vaginal or uterine mucosa and of the hypophysial gonadotrophic activity is achieved is intimately related to the problem of the differential tumourigenic threshold concentrations of oestrogen . 
how will the hypophysis behave when exposed to the action of these minute quantities of oestrogen in experiments lasting more than 2 years ? a group of 9 guinea - pigs was castrated and one ovary was grafted into the spleen ; sixteen days later a pellet of 23 to 30 mg . 
but the quantities absorbed were not sufficient for a complete control of this hypophysial activity : they were not able to reduce it to normality , as shown by the presence of haemorrhagic follicles in most of the animals of the group . there was in this group control of the vaginal mucosa and of uterine growth . in one animal the uterine weight was only 0o6 g . ; but in the remaining animals a weight of 0 - 8 to 1 - 2 g . 
with these 1 per cent pellets the incidence is not in another great ; new experiment lasting 757 to 875 days , without intrasplenic ovarian grafts , it occurred likewise but once in a group of 10 animals . 
one may raise the question whether some irreversible hypophysial change takes place during those 2 to 3 weeks which are needed for the vascularisation of the graft and for recuperation of hormone production . we have referred above to the three gonadotrophic hormones of the hypobut the possibility must be considered that also the somatotrophic or physis . some other hypophysial organotrophic hormone is partaking in establishing tumoural growth in the ovary ; this question has been discussed especially with reference to tumoural growth of wolffian structures ( iglesias , mardones , bruzzone and lipschutz , 1953 )  . the statement that ovarian tumourigenesis does not presuppose a complete suppression of the steroid control of the hypophysis but is the outcome of an irregular interplay of ovarian and hypophysial hormones may at the first sight however . 
the hormonal imbalance may last for as long as 3 years , and sometimes even more , without norwhereas it was evident , almost from the beginning mality being again attained . of this phase of our work , that the sequels of ovarian fragmentation , i.e. , reducing the mass of two ovaries to a small ovarian fragment , or remnant , in situ , were due to an overthrow of the normal ovarian - hypophysial relationship , we were unable to understand why this hormonal imbalance is in some cases irreversibly maintained . 
laws. from the department of pathology , guy 's hospital medical school . received for publication august 8 , 1952 . in a previous paper laws and wright ( 1952 ) have shown that - the growth of an implanted sarcoma in the bagg albino strain of mouse is associated with a reduction in the mitotic activity of the normal epidermis of the pinna . this fall was apparent when the tumour reached about 10 per cent of the body weight of the host . 
the tumour was the sarcoma 37 of the imperial epidermal samples were obtained from the pinna , and cancer research fund . after their separation from the underlying connective tissues they were staiiied by feulgen 's method . 
aetotic activity was estimated by counting the division figures seen in 100 microscopic fields uiider a magnification of 540 diameters . blood - sugar determinations were made on tail vein blood bv the method of haslewood and strookman ( 1939 )  . 
blood - sugar values in control and tumour - bearing mice . in experiments previouslv recorded ( laws and wright , 1952 ) , a significant difference was observed between the mitotic activities in the epidermis of the pinna in contiol and tumour - bearing mice . in order to compare the bloodsugar values in these two groups of animals , samples of blood were obtained at the same time of day ( 10 a.m. ) as the skin biopsies . 
correlatiom between tumour size , mitotic activity and blood - 8ugar value . since the growth of the tumour seemed to affect detrimentally the n - iitotic activity of the epidermis , coefficients of correlation were calculated between proportionate tumour size , niitotic activity and - blood - sugar value for a group 244 j . 
black. from the postgraduate medical school of london . received for publication march 25 , 1952 . from perusal of the literature available it appears that chronic ulceration associated with varicose veins is the most rare cause of malignant disease of the skin of the lower limb . 
we therefore wish to present 6 cases which undoubtedly occurred in conjunction with a varicose ulcer or eczema which had been present for many years . cutaneous neoplasia of the leg is rare , and study of the literature demonstrates that such skin cancers as do occur very rarely arise de novo , but usually in connection with chronic inflammation following injury , in old scars and sinuses , or after some chronic skin infections such as lupus vulgaris as well as in the varicose conditions mentioned . since the latter are without question the most commonly found benign lesions of the leg the excessive rarity of malignant degeneration is surprising and interesting . in recent years papers on this subject have been few . 
on examination she was a wasted , frail old woman not well orientated . there were no large nodes in the groin , the general examination showed senile but several small soft nodes could be palpated . changes but no obvious disease . biopsy of the tumour revealed a well - differentiated squamous carcinoma with cell - nests . 
b - , aged 71 years , was referred to us for treatment of a very large varicose ulcer of 20 years ' duration . four months before his admission to hospital the lower edge had begun to hypertrophy and the ulcer to spread on to the dorsum of the foot . 
h - , a widow of 67 years , was referred to us for treatment to secondary neoplastic nodes in the right inguinal region . she had been treated by mid - thigh amputation , at another hospital , for a 30 - year - old decubitus ulcer which , at the time of amputation , extended from the dorsum of the right foot to one - third of the distance up the tibial shaft and involved the bone . there had been no recent change in the ulcer prior to amputation but it had steadily increased in size during about 7 years before admission to hospital . amputation had been advised for pain , and because of the large size and failure to heal with support and dressings . on examination her right leg had been removed through the thigh . 
hard mobile nodes were present in both groins and in the right axilla . the left leg showed marked varicose veins and the scar of a healed ulcer above the left internal malleolus . her heart was fibrillating ( she had been receiving treatment for this for about 6 years ) , but there were no signs of cardiac failure . a report on sections taken from the ulcer after amputation showed a well - differentiated keratinising squamous - celled carcinoma . a biopsy excision of nodes palpable in the axilla was performed . 
no other radiological evidence of malignancy was found . biopsy of the tumour showed a general structure like granulation tissue , with wellformed capillaries and abundant reticulin . cytologically it was definitely sarcomatous , with large , pleomorphic , usually spindle - shaped cells with large irregular often multiple nuclei and numerous mitoses . although the size and histology of the growth and the necrosis of bone underlying made primary mid - thigh amputation the treatment of choice , his general condition was so bad that it was decided to attempt more by radiotherapy . 
lateral and medial fields were used and skin doses of 3300 and 3000 r respectively given using 220 kv . however , only slight response to this therapy couldbe found on serial biopsy , the tumour cells and stroma remaining as in the first biopsy , but mitoses became less frequent and some collagen was deposited . his blood urea , reduced by diet and conservative measures , again rose above 200 mg . 
he remained well for one year , when he was readmitted for treatment of a mass in the posterior flap of the stump . this mass was excised locally , a wide wedge of tissue being removed down to the bone . this local operation was again performed at the patient 's insistence . section of the tumour contained in this block of tissue revealed the identical histological picture presented by the original tumour and the nodule found in the inguinal lymph node . healing was by first intention . 
black this will prevent loss of time , decrease the period of pain for the treatment . patient , and allow the patient to acclimatize himself to the loss of his leg without radiotherapy should be the disappointment of failed conservative treatment . held in reserve for those patients whose general condition does not permit of operation , and these must be very few now . the treatment ofthe inguinal nodes depends upon the age and general condition extensive block dissection is a formidable undertaking in the of the patient . very old , and in these cases irradiation should be advised . 
where the patient will bear the operation this represents the safest method of eradicating growth . sarcoma , largely owing to its extreme rarity is difficult to recognise both clinically and histologically . it appears to occur more towards the centre of an ulcer than at the edge , to produce a florid fungating cauliflower growth and to these bleed readily . 
as with the squamous growths , sarcomata in varicose ulcers appear less ready to metathis may be due stasise than similar tumours elsewhere or in younger patients . to the fibrosis and scarring present after years of ulceration . 
 from the department of experimental , pathology and ganeer research , university of leeds , and department of pharmacology , guy 's hospital , medical school , university of london . 
greenblatt and kupper man ( 1947 ) , also using the rat , observed squamous metaplasia of the horn and a doubtful precancerous lesion in the cervix uteri , but no tumours , when a similar dose of methylcholanthrene was introduced . 
pan and gardner ( 1948 ) reported the development of numerous carcinomas and sarcomas in mice of several strains , when subcutaneous implants of cervical and uterine epithelium - were made together with small crystals of methylcholanthrene . 
 in the experiments described here uterine tumours were induced by the intro duction of methylcholanthrene directly into the uterine horn in two types of mice and the effects of various hormonal factors were studied . 
 the experiments were performed on two types of mice : inbred cba mice , maintained by brother - sister mating in the department of cancer research at leeds , and white mice obtained from dealers . 
the gun was intro duced through the incision , a fine silk ligature placed around it a short distance below the incision , and the carcinogen pushed out into the lumen of the horn . 
the amount of material introduced in solution in lard varied considerably , depending on the size of the uterus , but there is no doubt that the weight of methylcholanthrene introduced with method ( 2 ) was less , and sometimes considerably less , than that introduced into the uterus with method ( 1 )  . 
 ( 3 ) this method was similar to ( 1 ) and ( 2 ) , except that the upper part of the horn through which the material was introduced was removed . 
the upper part of the vagina was then exposed and dissected free from surrounding tissue and partly separated from the rectu a stout ligature was loosely placed around the vagina just above the symphysis pubis . 
the needle was introduced into the vagina and pushed up above the level of the ligature , which was then tied ( with one knot ) around the needle and held tied by an assistant . 
the ligature around the lower end of the left horn was tied , the ligature around the vagina rele : ased and removed , and the needle with syringe withdrawn . 
 the abdominal organs were carefully palpated at regular intervals to deter mine the first appearance of uterine tumours , but the mice were not killed until they appeared to be ill or until there was no doubt about the presence of an abdominal tumour . 
 of 15 immature oba mice , 12 developed tumours of the uterus , as follows : 4 had carcinomas , 6 sarcomas , and 2 both types of tumour ( table i )  . 
 the tumours presented a homogeneous translucent appearance , sometimes with haemorrhagic and necrotic areas , except in the case of the squamous cancers , table 1 . - 0oourrenoe of tumours in immature oba mice . 
 the object of the experiment was to find out whether the direct introduction of a carc~ogen into the uterine horn would be effective in inducing carcinoma of the endometrium in mice , and if so , whether the incidence of tumours could in 109 mice be influenced by hormonal factors , or by differences in technique . 
 effect of stra a higher incidence of both carcinoma and sarcoma occurred in oba than in laboratory white mice ( tables i , ii ) , in spite of the fact that all the oba mice were immature at the time of implantation . 
the difference in carcinoma incidence ( oba 40 per cent , white 149 per cent 134 ) is nearly but not quite statistically significant ( table iii ) ; that in sarcoma incidence ( oba 533 per cent , white 74 per cent 134 ) exceeds the conventional level of statistical significance . 
but when immature oba mice are compared with immature white mice ( table iii ) , then the difference in carcinoma incidence becomes significant ( oba 40 per cent , white 83 per cent 134 )  . 
above and to the right are the rectal glands and submucosa invaded by loose sarcoma tissue ; passing obliquely across the figure is the muscle of the rectal wall ; below is the main mass of sarcoma . 
 it was rather surprising that carcinoma could be induced by this means in immature mice , spayed at the time of implantation , when they weighed ll - 15 g . 
it is evident , however , that maturity at the start tended to improve the tumour yield , though it did not lower the period of induction in white mice ( table iv )  . 
 spaying had no apparent effect on the incidence of all tumours either in oba mice ( table i ) , where the numbers were very small , or in white mice ( table iv )  . 
 16 85 27 85 14 8 l 26 8 l 86 113 114 25 81 13 81 the yield of sarcomas was , however , greater in intact than in spayed white mice , though the difference was not statistically significant . 
mice which received the larger dose of carcinogen , are considered ( table v ) , it is noteworthy that the lowest incidence of tumours occurred in spayed immature mice . 
even though the numbers are small , the agreement between the three other groups in table v suggests that the lower incidence of tumours in spayed immature mice is of significance . 
it is probably comparable with the dose used by pan and gardner ( 1948 ) for the induction of tumours in subcutaneous implants ( " small crystals " )  . 
price. from the medical research laboratory , department of pathology , university of bristol . received for publication december 8 , 1951 . during the past thirty years much useful progress has been made in the this work , of histological grading of malignant tumours of epithelial origin . which one practical application has been the attempted correlation of prognosis with histological structure of a tumour , has had many valuable results ; and although there may be not infrequent discrepancies between the histological appreciation and the outcome of treatment in any given type of neoplasm , the results have at any rate led to some attempt being made by the histo - pathologist to guide the clinician at least in qualitative terms of high or low malignancy ; and to more precise premises for the comnparison of differing methods of treatment in series of comparable cases . the starting point of this present analysis was the observation that irrespective of the mode of treatment applied , the overall five year survival rates in most published dissections of groups of cases of osteogenic sarcomata were approxinmately of a similar order . 
some of these features can , it is true , be visualised by x - ray plates . however , the interpretation of these is mainly the proper province of the radiologist , and they are seldom to be seen in theroutine pathological laboratory . for the fortunate histo - pathologist who may be granted access to such aids , the position is onlyinmproved to such an extent as the experience which he may have in the interpretation of skiagrams , which is a field with c . 
the ideal state no doubt is the close liaison between surgeon , radiodiagnostician , radiotherapist and histologist with personal conference in each and every case . such states of collaboration seldom exist under conditions of normal routine work . the histological specimens from the present series of cases have been considered under the following headings : 1 . 
to anyone working in this field the fallacies of diagnosis are only too well known , and the cases included have all been subjected to free discussion and unanimous acceptance as osteogenic sarcoma by the group of radiologists , radiotherapists , surgeons and pathologists which forms the working panel of the register . in each case the diagnosis has been based upon consideration of the full history , clinical examination , adequate skiagrams and histological sections . in some instances the histological material is derived from biopsy , in others from surgical or autopsy specimens . this has been indicated in table i , also the time relationship of the histological specimen to any pre - operative x - radiation . for histological purposes the specimens were fixed , cut and stained by the usual routine methods . 
owing to the presence in sonle sections of many multinucleated tumour giant cells , and the indistinct outlines of a large proportion of the polyhedral cells , the nucleus was taken as the unit rather than the cell . in each case a minimum of 2500 neoplastic cell nuclei were examined in each section , using a ruled internal screen in one ocular of a binocular microscope . 
as there are also 8 cases included in the series that are still alive and when last reported were well , but for periods less than 5 years , the 5 - year survival rate is best expressed as 6 in 28 cases - i.e. , 21 - 4 per cent . two of these cases died at respectively 77 and 96 months with multiple pulmonary metastases , and the writer fully supports the view that 5 years is too short a period on which to base estimates of rate of cure in patients with osteogenic sarcoma . these brief data may be compared with those published on larger series by the following : christensen ( 1925 ) , coley and pool ( 1940 ) , the results of the new york memorial hospital series mentioned by coley ( 1949 ) , geschickter and copeland ( 1949 ) , the series reported by the british empire cancer campaign ( 1949 ) , and platt ( 1951 )  . as may be expected with a relatively small group of cases , there are some differences from the larger published series , e.g. , an unduly high incidence of femoral tumtours , but the broad agreement would suggest that this group may be regarded as a fair sample from which certain conclusions may tentatively be reached . clinical grading of the tumours . the data on which the clinical assessment of degree of malignancy has been based has been considered from the following points of view : 1 . 
from observations on these tumours and other bony conditions , the writer has acquired the view that one of the essential functions of the osteoblast is the formation of osteoid tissue - the precursor of bone , from which under suitable conditions of substrate the formation of bone may occur , possibly with no further part being taken in the process by the osteoblast . 
price callus and in paget 's disease . both normal and neoplastic , may produce phosphatase . it is also generally accepted that the osteoblast , from the grounds that this cell therefore is actively concerned in the laying down of osteoid arises the essential stromal feature of this histological sub - type of osteogenic sarcoma , i.e. , the characteristic osteoid stroma , which mav also be accompanied by considerable amounts of collagen and ill - formed cartilage . however , the osteoid is the essential feature . this stromal material may , however , sometimes occur in considerable amount in a tumour which is predominantly spindle - celled , but is then usually less evident than the collagenous fibrous matrix produced by the spindle cells . 
under suitable conditions the osteoid matrix may either calcify or ossify , more often the latter , and then produce the appearance of the osteoblastic or sclerotic type of tumour . it is thus possible to subdivide this group further into i . 
from the viewpoint of the histologist the essential histological structure of any neoplasmn occurring in a bone is more characteristically shown in an area of active growth , the radiological manifestations of which are more frequently lytic than blastic . hence this feature of the amount of bony matrix is not always readily appreciable from even a large biopsy . for this reason this subdivision will not be pursued further in the present analysis ; but it should be added , however , that a markedly bony stroma is often indicative of a tumour of relatively low malignancy , and this point should receive due consideration by the person who may attempt to correlate the histological , radiological and clinical findings in any particular case . from inspection of table iv the following points are evident : 1 . 
in an approximately quantitative assessment of the amount of osteoid stroma present in these sarcomata it is seen that there is usually a rich matrix in tumours of lower grade malignancv , and conversely a relatively smaller amount in the high - grade group . there are noteworthy exceptions , and the specimens showing perhaps this stromal feature in the greatest degree were those from btr / 66 , r . 
66 , 213 , 221 and 226 , but generally this feature was less evident in the more actively growing tumours . it is emphasized that a change in ph of the substrate is only one of a number of factors concerned it is also wise to bear in mind a fallacy that may in this biochemical change . arise in sampling a bony tumour , as the more easily sectioned and hence less bony areas are frequently selected for routine diagnostic examination . quite a nuimber of these sarcomata also show chondroid stromal areas which may either calcify or ossify , both changes often being seen in adjacent areas and largely governed by two factors : 1 . 
the iimean mitotic ratio of these sarcomata decreases as one passes from this is mluch more evident in the separation of clinical grade i to grade iii , clinical grade i from the tumours of grades ii and iii . it may be noted here that based upon clinical data case btr / 136 , y . 
price by the american registry of bone sarcoma in their 1939 ( revised ) classification , and they continued to regard intrinsic fibro - sarcoma as a variant of the osteogenic group ( ewing , 1939 )  . jaffe ( 1947 ) , on the other hand , commenting upon this adheres to the stricter view and classifies fibro - sarcoma as a separate entity . from consideration of the small group of cases here reported it would seem that this differentiation is indistinct and serves no useful purpose . table v gives details of these 7 cases . this grouip is far too small to be the basis for any definite conclusions , but the following tentative points emerge : 1 . 
in the spindle - celled group there were no tumours which appeared to merit a clinical or histological grading of i on comparison with those of the larger polyhedral - celled series . this appears to be confirmed on considering the figures obtained for the mitotic ratio in these growths . .5. 
one may perhaps from this draw the conclusion that there is some evidence to suggest that in a series of these two histological types of osteogenic sarconma if composed of tumours of average or more than average malignancy that the tinme of survival is rather longer in favour of the spindle - celled type . in this small series of cases , one obvious difficulty that has arisen has been the determination of mean survival time of the sub - groups , and it is fully appreciated that the figures shown are only minimal inasmuch as cases have been included which are still living . 
on reference to table iii again it will be seen that 7 of the 9 tuiyours showed a mitotic ratio considerably greater than the average for their appropriate clinical grade . 
g - , and it is strongly suggested that the aoverning factor in the survival of any case of osteogenic sarcoma is the combination of site of origin and histological grading of the tumour . table vi shows the 36 cases of osteogenic sarcoma arranged in ascending order according to the mitotic ratio , i.e. , in order of diminishing mitotic activity . this has been subdivided into three purely histological grades of malignancy , c . 
price into those cases with a mitotic ratio less than 100 : 1 , from 100 : 1 to 400 : 1 , and greater than 400 : 1 . this may be taken as approximnating to those of greater , average and lesser degrees of nuclear activity . reference back to tables iv and v will show that all the cases there clinically graded as iii appear again as grade iii ( histological ) plus one case , btr / 157 , d . 
a - : probably favourable result of treatment has led ta unduly low clinical grading ; tumour in lower end of femur . group based on range of mitotic ratio of less than 100 . mean survival period of grade iii ( 11 ) 114 + months . 
g - , aged 14 , mitotic ratio 83 : 1 , sarcoma of lower end of femur , who survived for a total period of 18 months . another case supporting this view was btr / 157 , d . 
mean survival 11 4 months . the marked difference in the prognosis in these separated groups of cases can it would be of the greatest value to subject many again be well seen from fig . 
2. further cases to this type of analysis , to confirm if possible the significance of the mitotic ratio and to find its mean value based upon the examination of a much larger series of tumours . 
the mean mitotic ratio for this series is 238 resting nuclei to one nucleus in mitosis . analysis of the group gives the following ranges : grade i : grade ii : grade iii : m.r. 
the mean mitotic ratio for this group of sarcomata is markedly different from that which has been found in the examination of presumably related cells in non - neoplastic conditions . the author wishes to record his great indebtedness to the late s . 
much thanks are also justly due to the members of the committee of the register for their co - operation in the collection and discussion of all the cases included in this series . material has been derived from the sourceindicated below , and to the surgeons , radiotherapists , radiologists and pathologists who have referred cases to the register , due recognition and thanks for their assistance are here rendered : 1 . 
we have adopted the following staging , which is similar to that employed at the christie hospital and holt radium institute , manchester : stage i . - primary growth limited in extent to site of origno loss of mobility or function . 
lymph nodes fixed , matted or bilateral , or distant metastases present . table iv shows , as already mentioned , how many cases had already reached stages iii or 1v when first seeking treatment . 
warren and gates ( 1932 ) investigated the problem in considerable detail , and concluded that a patient with one cancer was statistically more likely to develop another cancer than a normal individual . 
watson ( 1939 ) calls attention to the fact that when a patient with carcinoma of the oesophagus has - a second growth this is nearly always situated in the mouth . 
it is therefore of interest to know how often this treatnment succeeds or fails in its objective , and in the latter case , when there is a recurrence , what are the chances of further arresting the disease . these facts cannot be determined with any real accuracy , since each case clearly has to be assessed on its clinical development and course . 
harmer in stage i and ii cancers of the lip , re - treatment is rarely successful . first planned treatment fails , the patient does not often have a second chance . if the response of primary and secondary to irradiation . glucksmann ( 1948 ) has stated that the response to irradiation of the primary and secondary manifestations of cancer of the mouth is about the same , and that those growths " with a tendency to lymph - node involvement differ in their biology and radio - curability from those without such a tendency . " the more generally held view is that while the primary may be " cured , " the secondary is often more resistant to treatment . only stage iii and iv cases can be analysed if the theory that an irradiated primary will recur as frequently as an irradiated secondary is to be examined . there were 248 patients with stage iii and iv growths arising from buccal sites in whom radiotherapy produced regression of both primary and secondary forty - five remained well , and 203 recurred : 61 in the primary only , growths . 69 in the secondary only , 73 in both . 
hartley has kindly done a significance test on these figures . the number of cases has been adjusted so that the proportion of stage iii and iv royal cancer hospital patients is the same as that of the holt radium institute series . 
the accessible growths of the for cervical mouth and lip , and teleradium for the oro - pharyngeal primaries . metastases block dissection hasbeen the method of choice , or radium therapy for the inoaperable cases . x - rays have&been used comparatively rarely . memorial hospital , new york ( martin , 1948 )  . - hayes martin states that surgical excision is the method of choice for cancer of the lip , gum , anterior for oro - pharyngeal portion of the tongue , cheek , floor of mouth or palate . growths a combination of roentgen therapy and interstitial radiation is indicated . cervical metastases are treated by dissection when operable and by x - rays when not . radiumhemmet , stockholm ( berven , 1937 )  . - for more than 20 years - the usual treatment for growths of the tongue and most other buccal sites has been teleradium , with diathermy coagulation of any residual mass . 
sixty - five per cent had symptoms for less than 6 months before treatment commenced , yet ( with the exception of carcinoma of the lip ) in 60 per cent of cases the disease had already metastasized to the cervical lymph nodes when first seen . 
the treatment of these 800 cases has been largely by radiotherapy . comparison of the results of treatment published by different authorities is table xv shows wide difficult because of lack of uniformity in criteria adopted . divergencies for instance in the survivals of patients with growths of the buccal this is largely due to mucosa , and to a lesser extent of the alveoli and palate . the small numbers of the cases . the last section of this paper shows that although very different methods of it is treatment may be employed , the results on the whole are much the same . therefore inadvisable to attempt definite conclusions from the analysis of the cases presented . 
the cases have been under the care of all members of the staff of the hospital , past and present , to whom grateful acknowledgment is made for permission to publish them . in the preparation of the paper much help was derived from copeland - chatterton punch cards , many of which had been completed by j . 
iversen. * from the institute of pathological anatomy , university of copenhagen , denmark . received for publication june 11 , 1948 . earlier investigations by weigert and mottram ( 1946 ) have shown that 3 : 4benzpyrene after administration to the animal organism is metabolized to at least four different derivatives , labelled by weigert and mottram as bpx1 , bpx2 , bpf bpf . 
the diameter of the particles of the emulsion was between 6 to 15k . immediately after the emulsion was prepared it was injected intravenously in patients suffering from myeloid or lymphatic leukaemia . 
emulsion. blood samples ( one part 3 - 8 per cent sodium - citrate solution plus 9 parts blood ) were taken from a cubital vein immediately before , immediately after and at various times after the injection . 
2. - absorption curves of plasma extracted with ethanol before and after intravenous injection of 3 : 4 - benzpyrene . in order to make sure that the emulsifier ( postonal ) itself had no effect on the amount of nitrogen in plasma , 8 g . 
2 shows that the maxima of absorption characteristic of 3 : 4 - benzpyrene are , little by little , altered to maxima of absorption characteristic of the metabolites labelled as bpx1 . 
iversen the results of kjeldahl analysis on the precipitates showed that there was no noticeable difference between the percentage of nitrogen in the different samples of precipitate , which may mean that the composition of protein in plasma does not alter considerably in relation to an intravenous injection of 3 : 4 - benzpyrene , or that it varies so little that it has been impossible , with the technique used , to determine the difference . it would be possible to obtain a quantitative estimation of the proportion between the amount of unchanged benzpyrene and changed benzpyrene , and thus get an expression for the speed with which the metabolism ( or detoxication ? ) of 3 : 4 - benzpyrene takes place by determining the proportions between the extinction at 380 m , u . 
the same quotient for the x1 derivative is unknown and could not be determined , as it was not possible to obtain the x1 derivative in a pure form , but the quotient must be higher than 1 00 , as the absorption of the xl derivative is more intense at 380 m ,  . 
the curves further show that the time at which the rate of conversion is highest nearly coincides with the time at which the decrease in nitrogen - ( protein - ) conadditionally the curves indicate that tent of the plasma is most conspicuous . after the maximum concentration of changed hydrocarbon has been reached , elimination takes place at a constant speed . that the conversion may take place in the liver after an intravenous injection is an obvious consideration , and the following experiment would indicate that this is the case in rabbits : blood is transfused through a living rabbit liver ( nielsen , 1933 ) , and to the circulating blood is added 10 mg . 
3 samples of blood are taken before and at various times after the injection . shows , as in the case of human beings , that the absorption maxima of 3 : 4benzpyrene are altered gradually to the maxima of absorption characteristic of that these curves appear higher and higher on the ordinate the x1 derivatives . axis may be accounted for by the fact that it is not possible for the system to the variations in the quotient 380 / 385 m , u . 
iversen perhaps to be mentioned in this connection that the patients during , or immediately after , but never later than half an hour after the injection , sometimes got slight attacks of pulmonary infarcts . whether one considers the changes in the amount of nitrogen ( protein ) in plasma as attached to the metabolism of 3 : 4 - benzpyrene or as bearing no relation fig . 
 ( left ordinate axis )  . c and d give the corresponding relative amounts of x2 derivative calculated in the way described ( right ordinate axis )  . 1n 135150 us5 so o9 ? 0 150nt240 552t70 from fig . 
and the mice were kept on a balanced diet of commercial food pellets and water ad libidum . eventually the hybrids formed the following groups . group i consists of the offspring of males no . 
1. of the original 2 sisters , the segregated one died after her first litter , and was replaced by a third sister which was also segregated for birth and rearing of her first four litters . she was left with the male for the birth of her fifth litter ( table i . ) group iii consists of the offspring of 2 females , each permanently in the cage the paired segregated sisters of each died with males no . 
two sets of unrelated sisters were mated to male no 11 . ( table ii ) ideally all the segregated females should have been sisters of the female left with the male , but this was not always possible . the result of the experiment is summarised below : c3h . 
 ( mothers kept with male ) cba.c3h 11 mammary tumours out of 82 hybrids . ( mothers segregated from male ) , , 84 the incidence is expressed as the number of mice bearing mammary tumours as numerators over the number of survivors aged 450 days ( age of youngest tumour - bearing mouse in this series ) as denominators . all these mammary tumours appearing in the hybrids were confirmed histologically by p . 
2b , segregated from the male , developcd a mammary tumour at 538 days and 387 days respectively . these tumours could be attributed to transmission of virus in the mothers ' milk , or to infection from the c3h male in each case , or they may be unrelated to the in the case of female no . 
no definite conclusion can be drawn from the occurrence of such sporadic tumours . ( b ) andervont and dunn ( 1948 ) have shown that c3h males can carry the mammary tumour virus in their vesicular glands and secretion , and have suggested that the mother may be infected during copulation . foulds ( 1949 ) has shown a similar transfer of virus by riii males to their fl hybrids with c57 black females . bittner ( 1952 ) has studied similar crosses between high and low mammary cancer strains , with and without the agent , and has reached essentially the same conclusion about the role of the male in transmitting the agent . 
laws. from the department of pathology , guy 's hospital medical school . received for publication august 8 , 1952 . in a previous paper laws and wright ( 1952 ) have shown that - the growth of an implanted sarcoma in the bagg albino strain of mouse is associated with a reduction in the mitotic activity of the normal epidermis of the pinna . this fall was apparent when the tumour reached about 10 per cent of the body weight of the host . 
the tumour was the sarcoma 37 of the imperial epidermal samples were obtained from the pinna , and cancer research fund . after their separation from the underlying connective tissues they were staiiied by feulgen 's method . 
aetotic activity was estimated by counting the division figures seen in 100 microscopic fields uiider a magnification of 540 diameters . blood - sugar determinations were made on tail vein blood bv the method of haslewood and strookman ( 1939 )  . 
blood - sugar values in control and tumour - bearing mice . in experiments previouslv recorded ( laws and wright , 1952 ) , a significant difference was observed between the mitotic activities in the epidermis of the pinna in contiol and tumour - bearing mice . in order to compare the bloodsugar values in these two groups of animals , samples of blood were obtained at the same time of day ( 10 a.m. ) as the skin biopsies . 
correlatiom between tumour size , mitotic activity and blood - 8ugar value . since the growth of the tumour seemed to affect detrimentally the n - iitotic activity of the epidermis , coefficients of correlation were calculated between proportionate tumour size , niitotic activity and - blood - sugar value for a group 244 j . 
the original premise on which the present study was built was that if these three groups have any real existence it should be possible to demonstrate some differences in their natural history . a diagnosis that does not imply a prognosis is traditionally worthless ; not only is it of no practical value , but the difficulty of testing it leaves every opportunity it was proposed therefore to collect a series of rodent ulcers , classify for error . them according to foot 's ( 1947 ) criteria , and then to apply to them all available touchstones of clinical behaviour in the hope of being able to separate them . some such differences as those demonstrated by schrek and gates ( 1941 ) and schrek ( 1941a , 1941b ) between rodent ulcer and squamous carcinoma were sought . the attempt to do this , however , broke down unexpectedly early , for after our series had been collected it proved impossible to classify it on the lines proposed by foot ( 1947 )  . 
wells lesions with which foot ( 1947 ) dealt , it became clear that the great majority of tumours at the stage at which they are usually received by the pathologist are typical examples too various in appearance to admit of such simple treatment . of each class could be found easily enough , but there were so many mixed and intermediate and aberrant forms that no progress was possible . 
no modification of the classification could be devised that would avoid them . during a long interval in which the matter was left in this discouraging state , interest was deflected into a study of the pigmentation of rodent ulcers and of epithelial skin tumours generally which has already been reported ( lennox , 1949 )  . there emerged from this one possible way of classifying rodent ulcers , namely , into the pigmented and the non - pigmented . such a classification is almost wholly objective ; there either is or is not melanin in the tumour . contrast with the process of matching a tumour against a series of idealized types in the hope of being able to recognize a greater or less resemblance to one of them is very marked . it is true that the matching technique is reliable enough in the ordinary process of histological diagnosis , but where the types themselves are of doubtful existence it becomes open to great error . 
they are a large proportion of those received in this department in the years 1936 to 1948 . most have come from the radio - therapeutic research unit which was established in 1942 ; without its very full record system this study would have been impossible . cases have been rejected if the biopsy specimen was inadequate or if the history was deficient in any important detail , but an effort was made to include as many of the cases found as possible , partly because the available material was small , partly because any form of selection may profoundly and unpredictably influence the results of any study of this type . it was not possible to insist on more than a year 's follow - up , though most cases have had considerably longer ; the recurrence rate is therefore falsely low , though sufficient to provide some useful data for comparative purposes . surgical excision supplied 26 specimens ; diagnostic biopsies , multiple in 30 cases , were provided by 124 cases . most of the material was fixed in plain formalin - saline ; recent biopsies have been fixed in halfsaturated mercuric chloride in 15 per cent formalin - saline ( fss )  . 
the typical examples of this group seem distinct enough , yet it soon became obvious that transitional forms are numerous . wte therefore provisionally included the sub - group , and found later no reason to regret it ; we believe that these are merely the most benign and well - differentiated end of the rodent ulcer series ( the multiple and often familial tumours of brooke ( 1892 ) and fordyce ( 1892 ) we believe also to be of the same nature , though here we are extrapolating beyond our personal experience )  . in the second place , at the other end of the scale we find 11 tumours of the type illustrated in fig . 
we believe the evidence against the squamous nature of this sub - group is strong . within the typically squamous tumours a close parallel between histological dedifferentiation and clinical malignancy can be the most malignant epithelial skin tumour seen in this hospital demonstrated . in the last 4 years is that illustrated in fig . 
3 ; it grew very rapidly under observation and killed its host within 18 months of first appearance . less well differentiated squamous carcinomata should be even more malignant ; but all the tumours we have seen of the type of fig . 
2 have been relatively benign , and can be shown only by careful statistical analysis to differ in behaviour from the general run of rodent ulcers . inclusion of these two sub - groups harmonizes with the view of the rodent ulcer group developed later in this paper , as a series in which a gradation of differentiation can be recognized , with a definite though not very striking parallel gradation in behaviour . 
removal of these two sub - groups would not affect the general conclusions drawn , though it would reduce the level of significance of some of our figures . forms of differentiation chosen for analysis . only four common histological forms of differentiation in rodent ulcers could be defined well enough for analysis . 
some obvious features , especially those based on cell size and shape and on tumour cell group size and shape , had to be rejected because of the difficulty of establishing exact descriptive criteria and , more important , their great variability within any one tumour . 
some very interesting features were too infrequent in our series to justify detailed separate analysis : these were ( a ) keratin formation ( 11 cases , 7 ' 3 per cent ) , ( b ) hyaline stroma ( 11 cases , 7 ' 3 per cent ) , ( c ) squamous differentiation ( 4 cases , 2 ' 7 per cent ) , ( d ) " sebaceous " differentiation ( 4 cases , 2 - 7 per cent ; lipoid was not identified , and the recognition of these occasional foamy cell groups as sebaceous remains doubtful ) , ( e ) duct formation ( 1 case , 0 ' 67 per cent )  . the four forms of differentiation finally chosen were , in order of frequency , palisading , fluid formation , whorls and pigmentation . 
these presented the following advantages : ( a ) they were all common , so that sufficient cases were available for analysis , ( b ) their presence or absence could be readily determined , ( c ) between them they were responsible for a large part of the variation in appearance assumed by rodent ulcers , and ( d ) they were constant throughout the same tumour , varying 198 b . 
what form of degeneration of the stroma it can be we fail to see ; it is not myxomatous , it is only occasionally hyaline , and it is curiously localized if it is oedema . if one believes it to be stromal in origin one is driven to the proposition that it is an active secretion of the stroma - an unprecedented occurrence in an epithelial tumour , and one that in any case does not explain cysts within the epithelial masses . massive fluid production such as that of fig . 
by whorls we mean small spherical groups of concentrically arranged flattened cells , more eosinophilic than the bulk of the tumour and centred on an even more eosinophilic core ; this core often appears to be converted into a laminated plug of keratwe have counted nothing that did not have at least a trace of central eosinophilia , but think it possible to recognize even earlier stages of which the giant - cell - like structure seen above left centre in fig . 
9 may be an example . at least three interpretations of these structures have been offered : ( a ) they are cell nests ( parakeratotic pearls ) of basically the same nature as those of squamous carcinoma ( darier and ferrand , 1922 ; montgomery , 1928 )  . 
they differ from these in their smaller size , sharper demarcation , more concentric structure and lack of prickle cells , and usually also in the smaller amount of central keratin . ( b ) they are abortive hair follicles ( haythorn , 1931 ; warren , gates and butterfield , 1936 )  . 
the term " abortive " here is a convenient one ; it conceals the fact that the structures resemble no part of the follicle in any respect which will bear analysis . 
1. - a nodular tumour of the epithelioma adenoides cysticum type , only slightly cystic . note the position immediately deep to the epidermis , unrelated to hair matrices , and also the focus of abnormal epithelium , similar to that seen in early rodent ulcers , to the right of case 219 : from the scalp of a man of 33 , duration 22 years . 
14. - colonization of hair follicles by homologous epidermis in the rabbit . the epidermis and the epithelium of the hair follicles of the graft have died , but the stroma survives . 
and post - auricular area from pinna postauricular , 2 . is justified by the obvious difference in exposure , and by a difference in behaviour well marked even in the small number of cases involved . 
a preliminary test by standard error of the differences of the percentages in the 0 and 9 - 15 columns for each other and from the mean figures for the whole series gave in the event results differing little from those of more elaborate methods . 
wells it casts some doubt on the opinion earlier histological diagnosis is most difficult . it would , however , be statisexpressed that these tumours are all rodent ulcers . tically equally suspicious to find no such tumours . perhaps the group does include some spurious cases , but we have found no satisfactory way of determining which they are , and at least two alternative explanations , apart from chance numerical variation , offer themselves . 
boag , to whom we submitted the figures , pointed out that from nition . the statistical point of view they could equally be explained by a slight tendency to aggregation of the separate differentiations ; he was able to show that three of the differentiations ( melanin being the exception ) were rather more frequent in the presence of one than in the presence of no other differentiation , and a little more frequent still in the presence of two others . 
our four main differentiations are seen to associate in what appears to be an entirely random manner . put the case that there exists any histologically separable sub - group of rodent it is exceedingly improbable that ulcers , and that it is of any substantial size . any significant definition of such a group could be devised that would not involve at least one of our four main features . 
then infallibly the random grouping only if it is extremely small , or if it depends on criteria would be disturbed . which have so far escaped definition , can any such sub - group exist . of such possible sub - groups the most important , because the most widely accepted , is the " type intermediare mixte " of darier and ferrand ( 1922 ) which is the " baso - squamous " form of montgomery ( 1928 )  . 
we can find no real criterion of the diagnosis of this type of rodent ulcer except the presence of the " pearls , " and these do not appear to be anything except our whorls in their higher grades . montgomery ( 1928 ) states that his cases are more malignant and radio - resistant than other rodent ulcers . 
he gives no statistical evidence for this , basing it as far as one can tell from his original article on impressions of a small number of it will be clear that our series gives no support for the idea either of the cases . separate existence of such a group , or of the abnormal behaviour of tumours showing whorls . 
of our 54 cases showing whorls , 4 recurred ( 7 ' 4 per cent , compared to a general recurrence rate of 11 ' 3 per cent ) and 3 responded poorly to irradiation ( 5 - 6 per cent compared to a general rate of 9 ' 7 per cent )  . 
an analogy which seems justifiable is that of the parathyroids and the thymus ( the liver and the pancreas , or the enamel organ and the sublingual glands , or several other pairs might be used ) , which are equally closely related in their manner of origin , but yet , being histologically totally distinct structures , produce totally distinct tumours . foot 's ( 1947 ) manner of using the term primordium for the conical downgrowth of epidermal cells in which both begin obscures the fact that such primordia are not usually multipotential ; except in the few areas where sweat glands open into the mouths of hair follicles the two structures arise quite independently , and in most places at different times . we are impressed with the lack of truly organized structure in these tumours . we have already expressed our doubts about the so - called abortive hair follicles . one solitary tumour in this series ( unique so far in an experience of roughly twice the number of cases here reported ) showed reasonably convincing duct - like structures . 
wells hair matrix origin of rodent ulcers . mallory ( 1910 ) suggested that the rodent ulcer might arise from the hair matrix , and haythorn ( 1931 ) asserted that all rodent ulcers are simply hair matrix subsequent authors ( except wallace and halpert , 1950 ) have not tumours . accepted this completely , but no detailed refutation of his arguments has been attempted . 
they may , however , be shown to include several major flaws . ( a ) haythorn ( 1931 ) regards the connection of the tumour with the epidermis as purely accidental . 
we are not very impressed with the fibrils which we have been able to demonstrate ; in any case it seems probable that they are homologues of the tonofibrils of the rete malpighii , and that such fibrils form readily in any epidermal derivative , forming intercellular bridges which will be demonstrable as prickles wherever the cells are sufficiently separated . ( c ) haythorn 's ( 1931 ) identification of hair shafts we have already discussed . ( d ) we have been unable to confirm haythorn 's ( 1931 ) observations on the resemblance of the silver - stained basement membrane of rodent ulcers to that indeed it would be surprising if a hair matrix tumour of the hair follicle . developed a basement membrane like the " membrana vitrea " of the root sheath . we have not examined the neurofibril content of our tumours , but willis ( 1948 ) has indicated the unreliability of the evidence they provide . ( e ) haythorn ( 1931 ) describes atypical proliferations of hair follicles producing appearances which he interprets as the early stages of rodent ulcer formation . but nearly all these changes occurred in hairs surrounded by squamous carcinotheir occurrence is therefore rather to be taken as evidence that hair mata . follicles react in this sort of way ( it may be merely a disturbance of ordinary cyclical regeneration ) to any injury , and to be a warning that apparent transitional changes in hair follicles even within a rodent ulcer may be quite meaningless . ( f ) an argument which haythorn ( 1931 ) does not consider is that based on the site of origin of the tumours . 
where we find it necessary to disagree with them is in the assumption that this necessarily involves a specifically basal - cell origin . as von hansemann ( 1907 ) was first to point out , the surface epithelium and squamous carcinoma arise equally from the basal layer of the epidermis . seems , however , to be generally believed that if squamous carcinoma and rodent ulcer are different tumours they must have separate cells of origin . this is not necessarily so . 
at the time of first formation of hair follicles the epidermis possesses only a rudimentary " peritrichous " outer layer , and all the capacity for growth in either of its two main directions resides in one layer of cells . 
the stimulus to active keratin - ward proliferation ( whatever its proximate mechanism ) must be found in some contact with the external world - though there must be a basal level of activity of the degree seen in implantation cysts . 
the stimulus to the adnexa - ward proliferation almost certainly comes from some form of direct evidence for this in mammals is organizer - like action of the mesoderm . lacking , studies of hair genesis so far available ( danneel , 1931 ; trotter , 1932 ) being purely anatomical . 
but in birds , where the large size of the feather papilla makes transplantation experiments possible , the work of lillie and his school has produced a great deal of evidence on the process of morphogenesis ( lillie , 1942 ) , and it is known that the original stimulus to feather growth arises in the dermis ( wang , 1943 ) , though the type of epithelium responding to the stimulus partly determines the type of feather to be formed . in the absence of evidence to the contrary it seems reasonable to assume that in mammals hairs and sweat glands are evoked from the epidermis by similar stimuli derived from the dermis . thus we have two stimuli , two responses , and two very different forms of correspondingly we have two forms tissue formed from the same layer of cells . it is simplest ( though perhaps not entirely necessary ) to state the of tumour . resultant hypothesis in terms of pullinger 's ( 1949 ) theory of tumour origin in general . according to this , squamous carcinoma would be the result of the acquirement by epidermal cells of the ability to produce within themselves some stimulating substance which is normally only derived by external irritation , and rodent ulcer is the result of the acquirement by the same cells of the ability to produce an altogether different substance - a substance which is the normal stimulus to growth of the adnexae and which is normally derived only from the dermis . why then , if it results from the application of the same stimulus to the same tissue , is the rodent ulcer so poor a copy of hair follicle or sweat gland ? a possible answer may lie in the importance of the connective - tissue framework in the differentiation of adnexae , a matter concerning which there is some experimental evidence . 
a hypothesis is proposed ascribing the rodent ulcer to the autogenous production by the epidermis of a stimulus to proliferation normally supplied by the foetal dermis . our thanks are due to professor j . 
mark 's hospital , london . received for publication december 29 , 1949 . it is well known that different histological types of cancer vary in their rate of growth and liability to metastasise , but this relationship between histology cancer and spread is easier to study in some organs of the body than in others . of the intestine provides exceptionally good material for investigating this question becauise ; surgical operations are planned to remove a good stretch of bowel above and below the tumour as well as a wide field of lymphatic drainage in the mesentery . 
it happens , therefore , that the pathologist is presented not only with the tumour , but ' also with its surroundings , so he can first classify the tumour according to ' its histology , then measure the extent ' qf local spread by direct continuity , and finally record the number and position - of lymphatic metastases . when the histology and spread are compared in ' this way it soon becomes obvious that different histological ' varieties often behave differently , but a fairly big series of cases must be examined in order to express these differences quantiit takes a long time tatively and give them anything like precise significance . to collect many cases of cancer of one organ of the body such as the bowel at a general hospital admitting patients of all sorts , ' but this is done much more quickly in a special hospital like st . 
mark 's , which is intended primarily for in the last 21 years ( 1928 - 1948 inclusive ) diseases of the rectum and colon . 3 , 220 operation specimens of intestinal cancer were examined and dissected in the laboratory of st . 
mark 's hospital , the general distribution being as follows : 2 , 642 cases of cancer of the rectum , 429 of the colon , 51 of the anal canal , and 98 cases of multiple malignancy . in each case the records describe the extent of local spread and the n ' umber and position of all lymphatic metastases . preparation for this paper i ' have re - examined the sections of all these tumours and compared their histology ' and their local and lymphatic spread . since rectal cancer is much the largest of these groups , forming 82 per cent ' of all cases , it will be convenient to start with this . histological varieties of rectal cancer . the three main histological varieties of rectal cancer are adenocarcinoma , colloid ( or mucinous ) carcinoma and an undifferentiated variety which i shall call " anaplastic carcinoma simplex . " aden ? ocarcinoma is much the commonest variety , constituting 85 per cent its histological characteristics are well known , and it is sufficient of all cases . to point out that though the growth usually shows a tubular or acinar pattern there is as a rule very little evidence of mucous secretion , either in the cells or 60cuthbert e . 
the last two varieties were too few in number for analysis , but comparisons between adenocarcimoma and colloid showed once more that mucus thus , secreting or colloid tumours spread more rapidly than adenocarcinoma . at the time of operation , only 5 per cent of the colloid carcinomas were still stage 1 , i.e. 
dukes such relationship between histology and spread can only be established if the histological varieties are clearly distinct : as definitely different , let us say , as adenocarcinoma , colloid carcinoma and carcinoma simplex of the intestine . this is seldom the case . another handicap arises from the fact that in some organs of the body the injury caused by a malignant growth is much more attributable to its anatomical position than to any niceties of histology . this is particularly true of tumours of the kidney , ureter and bladder . 
jackson memorial laboratory , bar harbor , me . received for publication december 16 , 1948 . it is known from the work of andervont and bryan ( 1944 ) and green , moosey and bittner ( 1946 ) that the milk agent is antigenic for the rabbit and the rat . if , as is probable , the agent , is a virus one would expect it to be antigenic for the susceptible species . 
for 30 minutes and then cooled prior to incubation . in experiments 4 and 5 serum from hyper - immunized blacks was used . c57 black mice were injected at weekly intervals as follows : 0 - 1 ml . , 0 - 2 ml . , 0 - 4 ml . , 0 - 8 ml . , 0 - 8 ml . , 0 - 8 ml . 
a few papillomata also occurred . there is a suggestion of neutralization in experiment 2 . however , the probability of obtaining such a result by chance alone is of the order of 10 per it is specially regrettable that this experiment was terminated , as a higher cent . degree of significance might well have been obtained . on the other hand , there is no suggestion of any neutralization in experiments 4 and 5 , where hyper - immune serum was used together with a relatively weak tumour fitrate . 
of special pertinence to experiments with serum from hyper - immunized blacks may be the observations of webster ( 1938 ) and hodes and webster ( 1938 ) with the virus of st . 
louis here a high degree of immunity developed about 6 weeks after encephalitis . vaccination , and had waned before antibodies appeared some 20 weeks after injection . it may be that we bled our mice too soon . possibly our technique was entirely inadequate to show any neutralization . however , identical techniques were used by andervont and bryan ( 1944 ) and green , moosey and bittner ( 1946 )  . 
a strain it may be that this very mice are being constantly immunized since birth . prolonged stimulation is needed for the production of protective antibodies . the fact that the agent can be demonstrated in serum may be due to dilution if this is . 
sionally. 197 3 67 0 364 - 0 102 - 6 . 41 - 0 used purgatives ; 1 - 7 x 34 or 63 to have used purgatives occasionary in a hke manner the " expected 34 or 6 - 1 to have taken purgatives often . f7 - 7 x purgative consumption was calculated separately for each age - group in each sex . 
the differences in the senna rates - while showing tlle same trendwere not so marked or consistent , and though the age - specific rates of beecham 's pffls ' usage were without exception higher amongst gastro - intestinal cancer patient 's , the individual differences were , on the whole , small . direct comparison between the gastro - intestinal cancer and non - gastrointestinal groups was carried out for each of the three purgatives , making appropriate adjustment as before for the differing age and sex structures of the two populations ( table vi )  . 
the comparisons relating to the use of senna and beecham 's pills show similar , but less marked , trends towards heavier usage by the gastro - intestinal cancer patients . 
the excess of senna in the gastrointestinal cancer group just reached the level of technical significance and while a similar picture was presented by the separate consideration of cancer of the large bowel ( x2 - 7.21 , n - 2 , p = 0 03 ) , - there was no significant difference between the experience of patients with cancer of the stomach and those suffering from a non - gastro - intestinal complaint . 
my reasonsfor considering that the risk is a real one , and of importance , are perhaps best discussed in relation to my own experiments , as i am naturally most familiar with this material . i was iniectin - a dibenzanthracene into some dominant ( lethal ) yellow mice of mainly inbred type , and intercrossing for up to four generations , in order to study the type . 
the tests were on 400 - 800 f . , these results , though consistent , are not significant , males in each group . statistically tinless all three treatments are combined into one group . 
of some interest was the incidental finding of two visible mutants found in the casual inspection of cib c - liltures , which would be an extraordinary occurrence bv rhe drosophila work , too , indicated that the mutants were mere chance . appearing in sperm after removal from the mutagen . 
carr which tends to mutate only those loci that require a relatively small energy this would also imply that these comchange to give a new stable mutation . pounds will tend especially to mutate genes that have already mutated sponthus , although not really specific for any given gene , their effects taneously . may be normally limited to only a small fraction of the genes on the chromosome . but i think that there is a risk with chemicals not encountered with radiation , and this is that a given chemical can react with all , or at any rate a major part of the genes of one type in the animal exposed , as this is merely a repetition of a possible chemical reaction . 
then they might also react with the same genes in another exposed individual equally well , and thus the offspring of two people exposed to carcinogenic mutagens could immediately show an induced recessive . this gives a new problem in human genetics - inbreeding with an occupation . and i have suggested that mutant sperm may be produced long after exposure i don ' t know whether any data on this could be accuto the mutagen ceases . mulated - all i can recall in the literature is the so - called " industrial melanism " of insects described by harrison ( 1920 ) , but i think we should be aware of the risk . 
h there had been equal nijmbers of men and women , and equaltiijmbers in the age - groups , on an average the male mortahty would have amounted to 24 , 855 . 
environment and occupation may , therefore , be expected to exert a greater influence in men . bt say that , ta average age at death from carcinoma of each site . for each organ we can assess not only the fi - equency with which it is attacked , but also the average ao , , e at which this occurs . 
among jewesses we find a low incidence for carcinomas of the stomach , bile pwmges and cerv and a high incidence for carcinomas of the breast , ovary , intestines and kidneys . it would be more conrect to compare the jews , not with the average population , but with that of the big towns , for 80 - 4 per cent and 80 - 7 per cent of jews and jewesses respectively live in the big towns . if we do so , we find an increased incidence for carcinomas of the liver , gall - bladder , intestines , rectum , lung , ovary and breast , and a decrease for the mouth , oesophagus , stomach , uterus and skin . from the age - group distribution of jews and jewesses we should expect 228 and 296 cases of carcinoma respectively . 
versluys carcinoma and trade or profe , 88ion . we now come to the real object of this research - to trace the influence of trade or profession on the origin and the localization of carcinoma . 
our research covers a wider field than that of the so - called occupational cancers , and all that has gone before is necessary to enable us to interpret what follows . before we can proceed , we shall have to examine some problems a little more this will be facihtated by taking a specific occupation as an example , closely . and i have chosen coal - mining . the mortality cards show usa . 
how many people who had formerly been miners died of carcinoma from 1931 to 1935 , their ages , and the sites of their carcinomas . the census of 1930 ( there was no census in 1940 on account of the german occupation , consequently - an interpolation is - impossible for the years between 1930 and 1940 ) shows us ilow many miners there were in the netherlands and their ages , but ' thin ' about ex - miners . now if we take groups a and b together we include all miners who got carcinoma while still working or aftei . 
leaving the trade , with their ages , but t , leir distribution over the various age - classes cannot be compared with the census of 1930 , which gives no information about ex - miners . 
then the average error is when y i - s small this is practically equal to - % / .. this average error has always been taken into account in this research , and a difference is cared real only when the percentages found and those to be expected differ by at least 3 times the average error . fi - equency of carcinoma of the stomach and a low prostate fi - equency . 9 and 50 - 59 we find a total mortality of 50 cases , whereas we should expect 32 , so that the total carcinoma mortality of coal miners is very high . 
the fi - equency of carcinoma of the stomach is greatly increased , for we find 33 cases instead of the 12 we should expect . the number of cases of carcinoma of the prostate in these age - classes is too small to reach a conclusion . the question now arises , is this high stomach fi - equency amongst miners bound up with their trade or with their environment ; is it an " occupational or a " smial cancer " ? ( cramer )  . 
to answer this question we must caiieer study wives of miners " ( from the mortality cards of those married women where the trade of the head of the - fanifly is given as " coal miner . the manded woman practically always lodges with her husband )  . the percentage distribution of carcinoma over the various organs in " wives of miners " compared with the distribution in married women amongst the general population is shown in table xi . taking the " average error " into account , we see from table xi that only 172 j . 
the smaller the unit in our research the more chance we have of getting results of value . if we gather the trades into groups their typical characteristics will become less and less obvious until at last the ratios obtaining among the average population are reached . i have tried taking some trades together , but the typical characteristics of a certain trade always get lost , and the whole group misses what individual component parts show as typical . it is , however , worth while compari ' ng any one trade with another of the same kind , and i have therefore tried to arrange the order of the trad - es - discussed so that trades 6f a kind come near tog ' ether . table xii compares the actual deaths of men of different occupations with the numbers expected if the total carcinoma deaths had in each instance been distributed over the various sites in the same way as amongst all m - ales - that is to say , according to the percentages shown in table 1 . table xllla gives a similar comparison , for wives of men in different occupations , with the deaths expected if the total carcl ' no ' ma deaths had been distributed in the same way as amongst all married women . 
cervix uteri lung prostate lung prostate oil vender8 are only a small group but have an excessi - % , , ely high stomach frequency ' ( 26 carcinomas )  . . 
faxmers. baxmen butch ' ers soldiers - cigax makers soldiers university men tobacconists dock labourers shoemakers office - staff .iall porters officestaffs car men barinen teachers soldiers fisherinen plumbers greengrocers barinen plumbers commer . 
froiii the figures in this paper , but that would take up too much space . besides , in mv opinion conclusions will only be justifiable when we have sufficient international material at our disposal for comparison . this material will have to consist of the results of research on manv , relativelv small , areas during a period shortlv before the second world war , with due observance of the nece , - , sarv precautions . 
with larger areas racial , geographical and economic differences in the same trade plkv a prominent part . , and a trade during and after the war may be quite different in one countrv from another . there was too much changing of occupation . i wish to express mv gratitude to w . 
in 1940 , however , an important change was made in the method of selecting the main cause when more than one was mentioned , a disease certified as merely contributory and not in the direct line of causation being ignored if another well - defined condition was stated as the direct cause of death . 
for breast cancer in women , for example , the factor to be applied to a rate at all ages prior to 1935 was * 941 , signifying that the new procedure resulted in about 6 per cent of deaths which would previously have been credited to breast cancer being classified from 1940 onwards to some other cause . when it is desired to study the trend of mortality at particular ages it is not safe to assume that the correction to be applied to rates before 1940 is the same at every age , until that has been tested , as may be done by examining the ratios at different age groups between the deaths in 1939 based upon the old and new methods , tabulated for that purpose in table 21 and appendix bl of the statistical review for that year . 
for certain diseases where it was important , such as diabetes , more exact correction factors based on the dual classification carried out during the four years 1936 - 1939 were used in the registrar - general 's analyses of past death rates at separate age - groups , and on page 135 of the text volume of the review for 1938 - 1939 it was shown that for cancer of all sites combined the conversion ratios for each sex were slightly above unity at ages before 45 and below unity at ages after , diminishing regularly from 1 - 17 at 5 - 14 to * 95 at 75 and over for males . 
for cancer of the breast in females it can be deduced from the tables in the review for 1939 referred to above that the correcting factor diminishes progressively from * 997 at ages 25 - 29 to * 970 at 55 - 59 and * 810 at ages 85 and over . this is easy to understand because of the increasing frequency of the presence of breast cancer , in its primary or secondary manifestations , as age advances , coupled with increasing liability to die of some intercurrent disease which is certified as the direct cause of death . throughout these studies of the trend of death rates according to age , correction of the rates in years prior to 1940 has been carried out by means of factors derived jointly from the age - by - age comparison of the deaths in 1939 and the conversion ratio forall ages combined obtained from the dual tabulations of 19361939 . 
in 1950 - 51 it was possible for the first time to distinguish mortality from cancer of the cervix and corpus uteri as a result of the inquiries by the general register office concerning the large number of deaths certified as cancer of " uterus " without further definition , and the rates for cervix uteri show still lower proportions of single women and greater contrasts with cancer of the breast and other causes of death . amongst women who died of cancer of the cervix in 1950 - 51 at ages under 55 the proportions who had never married were about one - third of the corresponding proportions amongst women who died of all causes . 
at ages 55 - 74 the proportion was about two - fifths , and after 75 it was about three - fifths . in the registrar - general 's statistical review for 1940 - 45 ( registrar - general , 1951 ) deaths of married women from various causes were analysed by age groups according to whether the deceased women had borne any children or not , and the resulting proportions stated at death registration not to have had a child are shown in table iv for cancer of the uterus , breast and ovary , non - genital cancer and all causes . 
2 , in sharp contrast with those for uterine cancer , show on the whole very little change through 25 10 o > 9a t > 7 - id 5 - s = ~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~i 1921 - 26 1926 - 30 1931 - 35 1936 - 40 1941 - 45 1946 - 50 40 period when death occurred age when death occurred fig . 
at ages over 65 the rates increased up to 1940 and then fell back slightly , and between ages 30 and 45 the rates have increased since 1940 . this may be seen by expressing the rates in 1936 - 40 as percentages of those in 1926 - 30 , and the rates in 1946 - 50 as percentages of those in 1936 - 40 ( table x )  . in the right - hand part of fig . 
the increase in breast cancer mortality of married women to be expected at ages over 45 in the last 20 years would be , therefore , about 2 per cent of the rate . information as to the numbers of pregnancies experienced by women who later develop breast cancer at various ages is scanty , and the only data found suitable for the purpose of this study were in a tabulation by smithers et al . 
at ages under 45 the effect seems to be even greater , but the numbers on which the ratios are based are small , and there might be other reasons contributing to the low frequency of women with four or more children amongst patients seen during the period of childbearing . it is desirable that this inverse correlation with number of children should be confirmed by other and larger data , and such information is in process of collection in the liverpool hospital region and north wales by the british empire cancer campaign . assuming it to be correct , what effect would the decline in family size since 1905 be expected to have upon the incidence of breast cancer amongst all married women ? this can be calculated by applying the ratios for women over 45 to the successive distributions in table via and aggregating the products , as was done for uterine cancer . 
lung cancer death rates and also those from other forms of cancer tend to increase steadily with advancing age , so movements of the ratio will give no indication of that part of the upward progression which lung cancer shares with other cancer . 
the years of birth of the cohorts attaining these ages in 1901 would be 1882 - 1886 , centred at 1884 as the table indicates ; in 1931 the men of this cohort would be aged 45 - 49 , in 1933 their ages would be in calculating the ratio for the 1884 cohort in 1933 , three times 47 - 51 , and so on . the deaths at 45 - 49 were added to twice the deaths at 50 - 54 in 1933 , both for lung cancer and all other cancer , and the first total divided by the second . 
the " nil " increases in table xvi from 1937 to 1940 mean that in the cohorts bom before 1875 the lung cancer death rate was then rising with advancing age after 65 at about the same gradient as the death rate for all other cancer , and the actual gradient at that age and time period has been shown to be about 33 per cent increase in 5 years or 20 per cent in a trienniuthe preceding explanation for what occurred between 1925 and 1937 is far more probable , but the hypothesis of influenza as a contributory factor cannot be excluded as a possibility . from 1937 onwards sulphonamides began to be used in increasing amount , and pneumonia deaths soon began to fall . could this have affected lung cancer rates appreciably by keeping alive longer many persons who without sulphonamides would have died of a complicating pneumonia before the cancer could be recognised ? pneumonia death rates of males fell between 1937 and 1942 from 477 to 255 per nillion at ages 35 - 44 , from 950 to 457 at 45 - 54 and from 1535 to 1024 at 55 - 64 , and the fall continued till 1946 . during that period the lung cancer ratio continued to rise steadily in men born about 1880 , the gradient being steeper amongst men at ages around 40 and 50 than around 60 , and only slight after 65 . 
the distribution according to number of children born for hospital patients with breast cancer , in such data as are available , differs from what would be expected , and it is estimated tentatively that the bearing of 2 or 3 children reduces the likelihood of this form of cancer developing after 45 by about onefifth and that 4 or more children reduces it by about two - fifths . 
from 1937 to 1946 the lung cancer ratio continued to rise by about 7 per cent of the ratio annually in men born since 1890 , more slowly in men born between 1875 and 1890 , and inappreciably in cohorts born before that ; but after 1946 the increase again spread to all ages . sulphonamides , and later penicillin , must have contributed something to this by preventing some men from dying from penumonia without cancer having been diagnosed and allowing them to die a year or so later of recognised lung cancer . 
one of these paths is through the physiology of hormone production , a second is through the physiology of the propagation and transmission of the milk agent , and a third possible path is through the physiology within the mammary tissue cell governing its reaction to the hormonal stimulation or the milk agent . other paths may exist , and it is probable that these three are interwoven . proof of the effect of genic action in relation to the hormonal stimulation resulted from crosses between strain a in which the incidence in the virgin females is low althougb that of the breeders is high , and strain ch , in which the incidence in the virgin females as well as the breeders is high . results of such crosses were reported by bittner , h ' useby , visscber , ball and smith ( 1944 ) , heston and andervont ( i 944 ) , and bittner and huseby ( i 946 )  . 
heston incidence occurred among the virgin f , females resulting from mating strain a females to ' ch males as well as in the reciprocal f , virgins , together with evidence of segregation in the f2 generation , indicated that the difference between the strains was primarily a genetic difference . such a difference was to be regarded as either a difference in horinone metabolism , or a difference in the reaction of the mammary gland cell to horinone such evidence as the fact that added oestrogen stimulation yielded stimulation . tumours ' m ' strain a virgins , ' and the relationship of number of litters to tumour incidence in strain a reported by jones ( 1940 ) , strongly indicated a difference studies of the oestrus cycles of virgin females of strains in hormone stimulation . a and ch and their reciprocal f , hybrids reported by deringer , heston and andervont ( 1945 ) , however , failed to show any difference in the cycles , except that in the low - tumout group of virgin strain a females the onset of oestrus was these observations , therefore , suggested later than in the high - tubiour groups . that at least a part of the genetic difference could be manifested through the physiology within the mammary gland cell . in an attempt to determine the physiological mechanisms through which the genetic differences are manifest , huseby and bittner ( 1947 ) also have carried out a number of studies , including ovarian transplantation to f , hybrid mice , ovariectomy , vaginal smearing , and histologic examination of the genital tissues . these studies have indicated that more than ' one endocrine organ is affected . we have become more interested in the second path of gene action - that it has concemed with the propagation and transmission of the milk agent . been observed by a number of investigators that certain strains will propagate all the . 
high - mammary tumour strains the agent , whereas others will not . normally transmit the agent from generation to generation , and even low - tumour strains may have the same innate capacity as andervont ( 1945 ) has reported for strain c . 
on the other hand , bittner ( 1948 ) has found tumours in his descendants of strain c57 black females into which the agent was introduced , and fekete and little ( 1942 ) bave reported mammary tumours in descendants of c , , 7 black females that had developed in strain dba uteri from transferred ova . 
thus the situat ' lon m regard to the capacities of the various strains to propagate the agent is not clear . by crossing high - tumour strain c , h females with low tumour strain c57 black males , and comparing the two . 
types of backeross females produced by backcrossmg the f , females to both the ch and c.7black males , definite evidence of genetic differences in the ability to propagate and transmit the agent was revealed ( heston , deringer and andervont , 1945 )  . 
the possibility of an intracellular origin of the agent also enters into consideration . in some respects the picture is comparable to the gene - kappa relationship stuclied by sonneborn ( 1945 ) and co - workers in parameciuthe picture is not as , simple , however , in that there is . 
our attention has been directed toward tumours that arise in females in which the agent cannot be demonstrated ( heston , deringer and levillain , unpublished data )  . in order to obtain a line of strain ch friae of the milk agent a litter of 3 females and 3 males were removed from their c3h mother by cesarean section and fostered upon c57 black female . 
these females were later mated to their male littermates , and subsequently the line has been maintained by brother x sister matings , the young being nursed upon their own mothers . in this line ; designated as c3hb , mammary tumours are arising . in 194 of the females of this line 14 months of age and older and extending through the first 5 generations to date , 47 , or 24 per cent , have developed mammary tumours at an average age of 18 - 9 months ; seventy - eight have died without mammary tumours at an average age of 16 months , and 69 are still living at an average age of 18 months . study of the histologic section of 37 of these tumours has not revealed mucli dissimilarity between these and the usual ch mammary tumours . nine , however , ' have show - n areas of squamous metaplasia with pearl formation similar to that described by kirschbaum , williams and bittner ( 1946 ) in mammary tumours induced by methylcholanthrene in the absence of the milk agent such areas also occasionally occur in normal strain ch females of older age , suggesting that the occurrence of squamous areas may be characteristic of older age rather than specifically owing to the possible absence of the milk agent . three of the tumours arising in these c3hb females have been transplanted into other c3hb females , and in each case the transplant has grown . we have no evidence , however , of a milk agent in the etiology of these tumours . distribution of the tumour - bearing females in the pedigree chart does not show segregation of tumour families , as ' would be expected if the agent were present . furthermore , we have found no evidence of the agent in cell - free extracts of these these extracts varied from 2 to 5 per cent , and were prepared in 0 - 005 m tumours . .phosphate buffer ph 7 - 0 with a waring blendor ; cleared in a multispeed centrifuge at 18 , 000 g.. 
heston extracts premonths of age and older , and none has yet developed a tumour . pared with the same technique from tumours from c3h females produce tumours in c3hb test females in approximately 8 to 10 months . this is not presented as absolute proof that the agent is not present . if it is , however , it is not comparable to that in c3h females , nor is there any evidence of its being built up comparable to that of c3h . if the agent is not present we have proof that the accumulation of genetic factors and of non - genetic factors other than the milk agent can cause the tumour threshold to be surpassed . this light the milk agent would be comparable to the carcinogens in the induction of lung tumours , where the presence of the carcinogen appears to merely increase the probability that the tumour will appear and at an earlier age ( heston , 1942a , b )  . while all of these factors have been shown to alter the probability that the normal mammary tissue cell may be transformed into a malignant cell , these investigations have not answered the question as to what constitutes this change to malignancy . 
the largest part has been obtained from the rikshospital , which receives patients from approximately one - sixth of the material has been placed at the whole country . ' cal depaxtment iii and by proniy disposal by professor c . 
a few cases onl come from - other hospitals . in addition to the two clinical , two post - mortem series have been used in this analysis , namely , t6 material of jacobsen ( 1953 ) from wo city hos itals , covering the years 1937 to 1946 , and the material of christiansen ( 1953 ) from the rikshospital , covering the years 1925 to 1952 / 1 . all the tumours of these post - mortem materials have been typed by kreyberg with no knowledge ofthe clinical data . 
figures of each series are comparatively small , but a few feature - s seem to be significant , and possibly important . the main differences between the chnical and the post - mortem series are ( 1 ) the relatively much higher number of adenocareinomas , 30 per cent of an cases in the latter against less than 10 per cent in the former , and ( 2 ) the lower number of squamous cell carcinomas in the post mortem series . 
a study of the two papers dealing with the post - mortem series reveals a greater number of old persona i these materials , as compared to the clinical group . 
the significance of these differences will be discussed later . in kreyberg 's ( 1952 ) first paper a comparison was made between the occurrence of the different histological types in the norwegian material and a sipailar recent material from the mayo clinic . 
kreyberg mainly as a result of differences in criteria for typing . in the present table 1 , three series from foot ( 1952 ) have been included in order to stress this point . 
the distribution of histological types in this american material is remarkably similar to the norwegian clinical series , with one exception , the group adenomas and salivary gland tumours . these tumours occur more than ten times as frequeiltly in all the norwegian series . 
the cause of the relatively greater number of these suffice it to mention at this tumours may be manifold and will be discussed later . point that even in america certain investigators have found these tumours ratheifrequently . in table ii is presented the distribution of the different histological types as regards age and sex . 
t. uncertain group ii : 17 in table iii the findings regarding the sex distribution have been summarized . it will be seen that the different histological types in this chnical material form two main groups with markedly different sex ratio . 
the fact that the tumour material has been collected during the years 1948 to 1953 , while the population figures refer females 3 4567891 4 5 67 891 i1 1 3 456789 figa . 
1. - age distribution at the time of diagnosis of all lung tumours ( l ) and the mortality figures for stomach carcinomas ( v ) in males and females separately . 
1 curves have been drawn on double logarithmic paper , representing the whole material of the clinical series for males and females separately . for comparison one other curve for each sex has been drawn , namely , the corresponding curves for stomach carcinomas , based upon the mortality figures for norway , 1950 . 
2 two curves have been plotted in the traditional manner , namely , the curves for the relative age frequency of squamous cell carcinomas and for large cell lo~ ~ ~ fig . 
the figures are given in table iv the two curves are nearly identical and they indicate that the group i tumours biologically actually represent a uniform group , in spite of unquestionable histoit will further be seen that these group i tumours mainly are logical differences . responsible for the characteristic features of the lung " cancer " curve in general . the other lung tumour types have been examined in a similar manner . 
the adenocarcinomas and the sub - group lung adenomas and salivary gland tumours are , however , comparatively few in number in each of all the series , and accordingly subject to considerable chance fluctuations . in table v the figures for these tumours in all the three norwegian materials the basic figures are given for each material separately . 
the unusual fall in the higher age groups is taken to indicate a new carcinogenic situation in development , and the future stages are forecast by the direction of the curve for the age groups 30 - 39 and 50 - 59 . the adenocarcinomas , according to our diagnostic criteria : malignant tumours coniposed of more or less atypical , secreting or non - secreting , columnar cefls , with their nearly equal sex distribution and their increasing frequency with the advancing age , indicate that they are caused bv comparatively weak carcinogenic agents , well established in the society , and acting with equal strength in both sexes , at least in large parts of the country . the small group of bronchiolar cell carcinomas occur in all age groups and with no definite sex preference . 
they may be caused by unknown agents , hitting at random . the histological pictures , the equal sex incidence , as well as the appearance with no preference for any age group , together indicate that lung adenomas , benign and malignant , and sahvary gland tumours are caused by accidental factors , presumably of developmental origin . at this stage a few more words about the latter tumours may be justified . 
some surprise has been voiced as to the considerable number of adenomas and sahvary gland tumours in norwegian materials . firstly , a survey of the lung tumour problem i : ft general in norway shows that the total number of lung tumours is very moderate , as compared to the figures for england and wales , the netherlands , the united states , and even denmark . if , as assumed and actually found , the recent increase in norway is caused mainly by the ever larger number of group i tumours , it follows that the other histological this development has been types must show a proportionate decrease in number . observed in the ordinary columnar cer carcinomas . 
a decrease in the number of lung adenomas and sahvary gland tumours in relation to the sum total is predicted , but it may for a while be less marked in chnical and especiary surgical materials , because these tumours represent comparatively favourable clinical cases and are therefore selected . secondly , the tumours in question are , actually , observed in considerable numbers also in other materials . fried ( 1948 ) in the massachusetts general hospital found 17 adenomas out of 175 cases of bronchogenic neoplasms , and carlens ( 1952 ) reported 8 - 10 per cent in a swedish material . tbirdly , these tumours are most probably present in many other materials without beino , recognized as such . true columnar cen careindmas and group i tumours very rarely occur before the age of 35 years . in most 1 - ung cancer statistics some tumours are registered in younger and verv young persons . 
some of them have been diagnosed as adenocareinomas , others as sman cer carcinomas , especially if unfavourable preparations have been the base for diagnosis , or if the tumours are infiltrating . 
any academic discussion as to the propriety of the designation cc mahgnant adenoma " ought to be silenced by the very important fact , that if the proper criteria are observed and the material typed without clinical information , a grou ' of tumours will emerge , wit - h a sex ratio 1 : 1 , with no accumulation in anv a - ae aro - ud . 
each histological type has been analysed , especiany as to distribution according to age and sex , and the findings correlated to our additional present knowledge regarding the development of these tumours . 
they do very seldom occur before the age of 35 years and they present a very characteristic and , for human carcinomas , singular age distribution . this age curve as wer as the vital statistical evidence indicate that the main part of these tumours are caused by a recently estabhshed carcinogenic situation in certain ' parts of the world , notably the united states of america and westem europe . columnar cell adenocarcinomas appear with httle sex difference and they show a steadily increasing ffequ - ency with advancing age , a development in conformity these tumours are probably caused by with a great many human carcinomas . comparatively weak carcinogenic influences , evenly distributed over large areas , well established in the society and striking both sexes with equal force . bronchiolar cell carcinomas occur with equal frequency in both sexes and strike individuals in ar ages . 
the present work was undertaken to determine whether any such action would affect the process of malignant transformation as brought about by painting a carcinogenic hydrocarbon on mouse sk material .and me ' l ' hods . 
 a drop of the solution was applied interscapularly on the skin of the mice , by paint - brush , once a week , for one year till the mice died or were sacrificed . 
at the end of the experiment one mouse group3 urethane group2 } : 2 = 5 = 6 - dibem : anthracene groupl 1 : 2 : 5 : 6 - dibenxanthracene and urethane 3 - .... 
it was found that all mice in groups 1 and 3 after six or more months ' treatment , had developed multiple pulmonary adenomas which appeared to be typically urethane - induced . 
 the results show that , under the experimental conditions described here , urethane ca~ no obvious change in the frequency or time of appearance of papillomas or epitheliomas induced by 1 : 2 : 5 : 6 - dibenzanthracene . 
consequently a better test to detect a weak inhibiting activity of urethane might have consisted of treating mouse skin with one application of the hydrocarbon , and thereafter more frequent urethane applications . 
no studies were made of the histological effects of urethane on either normal skin or skin under going malignant transformation , since the experiments suggest that any such effects have little action on the production of cancer . 
 it is most interesting to note that those mice which received urethane treat ment ( groups 1 and 3 ) had multiple lung tumours , whereas those receiving 1 : 2 : 5 : 6 - dibenzanthracene alone ( group 2 ) had none . 
 when urethane was administered to mice in their drinking water in previous experiments , a reduced fluid consumption was noted for the first few days , showing their aversion to it . 
an estimate was made of amount of urethane in a paint - brush full of the solution ( as painted on the mice ) by applying it to a cover slip and weighing after the acetone had evaporated . 
for previous studies ( cowen , 1947 ) , lung tumours in comparable numbers to those obtained here were induced in various inbred jines of mice by injecting 025 c.c. 
since total dosage was not the same , and since there are marked strain differences with respect to lung tumour response by different lines of mice , no accurate comparison can be made . 
it would be safe to say , however , that a large part of the urethane applied to the skin was absorbed by the mice in this experiment , judging by their tumour response . 
 it is not unreasonable to suppose that urethane is absorbed at least as readily from human as from mouse sk since urethane causes leucopenia in man ( moeschlin and melli , 1947 ) and lung cancer in mice ( nettleship and henshaw , 1943 ) and rats ( jaffe , 1947 ) , it would be well for those who handle this substance frequently in the laboratory or commercially to consider it a possible risk to health and consequently take effective precautions . 
 three groups of mice were painted interscapularly with an acetone solution of 1 : 2 : 5 : 6 - dibenzanthracene , urethane and a mixture of both each week . 
 this points out that most of the urethane applied to the skin was absorbed .all expenses in connection with this work were home by the british empire by it  . 
according to these measurements very little difference was observed between the size of the tumours of the control and dibenzanthracene treated animals in the high protein group after 7 days , and the tumours of the treated animals appeared to be only slightly smaller than those of the controls after 10 days . in the low protein group , however , the measurements on the 7th and on the 10th days showed that there was considerable inhibition of tumour growth in the animals treated with dibenzanthracene , while the tumours of the control animals had grown to about the same size as those of the controls of the high after 11 days the animals were killed and the tumours dissected protein group . very little tumour inhibiout and weighed . 
strong. from the school of medicine , yale university , u.s.a. received for publication february 2 , 1949 . the idea of somatic mutation as an explanation for the origin of cancer has had a long and interesting history . its original use as an interpretation of cancer is usually associated with the names of murray and of boveri . these men arrived at the somatic mutation conclusion from different fields , murray from experimental cancer research , and boveri from his classical observations in experimental embryology . 
at that time he stated : " the existence of such tumours , the biological characters of which are retained through long periods of propagation , shows that the cellular transformation which initiates carcinomatous growth may take place in varying degrees . 
strong this biological alteration colours permanently their whole biological behaviour . is of such a kind that the cells are able to take up nourishment , increase in size and multiply indefinitely . 
they acquire an individuality and powers of resistance to injurious agencies superior to those of normal tissue elements . " boveri 's idea on the nature of the origin of cancer stemmed from his observations on atypical mitoses . 
he had suggested the possibility that by this means an unequal distribution of the chromosomes would ensue and thus lead to unconhe was loath to expand upon this concept until aichel trolled growth . ( 1911 ) , using boveri 's own observations on the development of the sea urchin egg , arrived at the conclusion that a malignant tumour was caused by a fusion boveri 's concept has not received wide recogof a tissue cell with a leucocyte . the essential feature of the idea is expressed in his own words ( boveri , nition . 1929 ) : " the essence of my theory is not abnormal mitosis , but in general , a however this may arise , the result definite abnormal chromosome - complex . beside the multipolar mitoses , which might would always be a definite tumour . depend either on a simultaneous multidivision of the centrosome or on distorting the parallelism between the division of the centrosome and the cell - division , asymmetrical mitosis should be chiefly considered for the origin of tumours . indeed , according to analogy with certain occurrences in sea urchins , these would depend on a lack in certain chromosomes of the power to divide ; this would result far more surely in tumour than would multipolar mitoses , which depend agencies which would act on chance for the distribution of their chromatin . most directly would be those that have the power of destroying definite chromoboveri , therefore , saw quite somes.of a cell , while leaving the others uninjured . " distinctly that irrespective of the mechanism of origin , the disturbed chromatin content is the essential feature in cellular physiology , including the abnormal condition of a tumorous growth . 
the pleomorphism of cancer cells and the irregular atypical mitoses so characteristic of their nuclei had been observed and carefully studied , however , since the middle of the nineteenth century . whitman ( 1919 ) wrote a critical review of von hansemann 's theory of aiiatyzzer ( 1916 ) expressed plasia in the origin of cancer in terms of modern genetics . the opinion that a somatic mutation may be involved in the origin of cancer . tyzzer stated , " there are marked differences in the behaviour of various tumours on transplantation in given classes of mice . 
even tumours arising in homogeneous races show such differences , and this may be attributed to the acquisition of new characteristics by the soma which are manifested in the development of the tumour . 
as a matter of fact some investigators express the opinion that tb.e two genetic phenomena are entirely antagonistic to each other . for example , a very recent article by bauer ( 1948 ) of heidelberg discusses at length that susceptibility to cancer in the human population is not inherited , and at the same time elaborates on the development of the concept that cancer arises as a somatic mutation . 
that a tendency to undergo somatic mutation may have a definite genetic basis in normal tissues has been discussed by east ( 1917 )  . this phenomenon has been encountered especially in plants , but also has been reported in the higher animals . an early example of a genetic influence on somatic mutations is discussed by whitman ( 1919 )  . 
a yellow chrysanthemum carrying white flowers on one branch . it is obvious that , since the colour of the flower is known to depend on definite factors , the development of a branch carrying flowers of a colour different from that of the flowers on the other branches could only arise through the failure of the factors to pass over , during mitosis , into the cell from which that branch developed . the branch , in other words , represents a somatic mutation due to asymmetrical mitosis . " many tumours have been described in a variety of genetic material . 
many of these tumnours are pigmented and occur especially in the early development of the individual , and some are associated with or are identical to lethal mutathese have been recorded by stark and bridges ( 1926 ) , wilson ( 1924 ) tions . and others in drosophila , by federly ( 1936 ) in lepidopterous larvae , and by many other investigators . most of these tumours are inherited by a multiple factor complex and , in the opinion of t . 
morgan , expressed to the author many years ago , at least one of the drosophila tumours arose as a mutation . time alone prevents the further discussion of this interesting genetic material and its bearing on the somatic mutation hypothesis . the next advance in the somatic mutation idea in relation to neoplastic lesions was undertaken by the present author , in 1918 . 
from that time onward until 1930 , a considerable amount of evidence was accumulated from the study of the transplantation of adenocarcinomata of the mammary gland in mice that eventually provided the first experimental evdence that a somatic mutation may be involved in the origin of cancer ( strong , 1926a , b )  . 
some of these data have been published , but a considerable amount has not . the development of this experimental approach to the nature of the origin of cancer was as follows : tyzzer and little investigated the transplantation of a sarcoma that originally arose in a japanese waltzing mouse . 
they found that the progressive growth of this transplantable tumour was dependent upon thesimultaneous presence of multiple mendelizing units strong and little , in 1920 , and later in 1924 , determined that two transplantable adenocarcinomata of the mammary gland in mice were dependent upon different genetic complexes for their continued the dbrb tumour was dependent upon the simultaneous presence of growth . two genes , whereas the dbra tumour was dependent upon the simultaneous presence of these same two genes , but required the presence , in the host , of a third gene . 
the presence of the third gene had no detectable influence on the growth of the dbrb tumnour . this geneticsimilarity and difference was obtained in the same series of mice in spite of the fact that the two tumours were histologically indistinguishable ( strong andlittle , 1920 ; little and strong , 1924 )  . the opinion of identical diagnosis was given by the late james ewing , as well as by francis carter wood . 
a third spontaneous tumour that arose in a dilute brown mouse ( given symbol dbrc ) provided evidence that six genes were involved originally in the growth of this tumour when transplanted into a series of suitable f2 individuals derived from a cross between mice of the dilute brown stock and mice of a totally unrelated stock , the well - known a stock . 
growth rates on the various transplantable tumours derived from the dbrc tumrour were determined . after several transplant generations a tumour was obtained that grew so rapidly that it was considered out of the normal range of growth for the original transplantable tumour . 
when the derived transplant was tested it was found that now its growth was dependent upon the simultaneous presence of only two genes . this sudden acquirement of growth capacity also resulted consequently in a new transplantability characteristic . 
a second sudden change subsequently took place , and a new derived ( mutant ) type of tumour would now grow in 75 per cent of all inoculated f2 mice ( observation 75 - 00 + : 23 - 002 - 79 )  . 
theprobable error difference between this newratio and the actual observation for the original dbrc tumour was 5813 per cent 3 ' 67 or 15 - 84 x p.e. this new derived transplantable tumnour continued to give a 3 : 1 ratio in a series of f2 mice for several transplant generations . eventually a new sudden change took place at which time the - new mutant type grew in practically all f2 mice ( observation 243 ' 00 + : 2 - 004 0 ' 94 )  . these new data in the f2 deviated from the ratio obtained with the original dbrc tumour as follows : 80 - 78 per cent 2 - 48 or 32 - 57 x p.e. there can be no doubt that sudden genetic changes are taking place somewhere in the relationship between the host and the transplanted tumour . since the mutant types and the original transplantable tumour were being compared in the same series of f2 mice , these sudden changes could not be taking place in the host but must be taking place within the tumour cell ( strong , 1926a , 1926b )  . another point that should also be emphasized is the fact that when the derived mutant transplantable tumour would grow in all f2 mice derived from a cross between the dilute brown and the a stocks , then , and not till then , would it grow in all mice irrespective of genetic relationship . in other words , it had lost all characteristics of tissue specificity . the transplanted tumour would grow invasively at a tremendous rate and would metastasize extensively . 
thus evidence was obtained that a highly specific , relatively benign , slow - growing transplantable tumour had progressively and suddenly acquired periodically new biological characteristics until finally it had been converted over into a carcinoma . 
toward the end of the series , however , especially at the terminal non - specific state , the tumour had become more cellular and had lost most of its original adenocarcinomatous arrangement . another series of investigations was performed on the transplantation of the 13 spontaneous tumours that mouse f1 79 gave rise to . this mouse was not only the common ancestor of the well known c , c3h , cba , c121 and chi strains of inbred mice , but also gave rise to a wealth of neoplastic tissue as follows : all 13 of her spontaneous tumours of mammary origin were tested out by trans102 l . 
and if one tumour tissue has deviated from the genetic constitution of the somatic tissue from which it arose , then possibly all tumours undergo the same process in their origin . the above phenomena especially of sudden changes taking place during the transplantability of spontaneous adenocarcinomas of the mammary gland in mice has been amply verified , not only by the investigation of the 11 other tumours derived from female f179 referred to previously , but also by many other all the phenomena of tumours derived from other mice in my laboratory . transplantation consistent with the genetic theory of transplantation were also verified by the independent work of bittner ( 1931 ) and by cloudman ( 1932a , b )  . eight years later little ( 1934 ) wrote a review on the genetic work on the transplanted tumour in mice in which he included a discussion of the somatic mutation in this paper little points out that he had outlined the genetic basis for idea . susceptibility and nonsusceptibility to transplanted tumours in 1914 ( little , 1914 )  . 
he states again in 1934 that " the bit of tumnour tissue to be transplanted has a genetic composition , which is determined by that of the animal in which it if this idea was exclusively true , then it is obvious that a somatic arises . " mutation could not have been involved in its origin since any mutational process it is indeed true that in the should alter or change the original genetic state . early transfer generations , the transplanted tumour derived originally from a spontaneous source does retain the characteristic of tissue specificity determined by the genetic constitution of the mouse , inthat it will grow only in individuals which are genetically related to the mouse that gave rise to the tumour . 
but it has now been definitely proven that this phenomenon of tissue specificity is periodically and progressively lost by sudden changes resulting in simpler and simpler mendelian ratios , until eventually the tumour retains no or very little tissue specificity which it originally had . these sudden or mutational changes have always produced more and more malignancy , as determined by percentage of takes , growth rate and eventual invasive and metastatic characteristics . has also been indicated that no two tumours , even though they be derived from the same mouse and present the same histological appearance , ever showed the same mendelian ratio when transplanted into a series of appropriate f2 individuals . 
when two transplantable tumours were derived from - the same mouse , some of the genetic complex involved in their successful transplantation is common to both tumours , whereas some are unique to either the one or the similarity of genetic transplantability complex indicates genetic other tumour . in this particular little 's concept of 1914 is relationship of origin for tumours . it is also evident that the more recently chemicallytherefore partially correct . induced tumours show , from their very origin , on an average , more malignancy , and thus less tissue specificity than do the spontaneous tumours that arise in it is probably true , although at present the same series of inbred or hybrid mice . impossible of proof , that there is some genetic mechanism within cells that determines to some extent normal cell relationship , but that under certain conditions this controlling genetic mechanism alters or changes , and by so doing permits an uncontrolled or cancerouscondition to arise somewhere in the biological this phenomenon of break of co - ordinating influence of system ( the organism )  . a definitive part is , i believe , the essential feature in the origin of cancer . 
strong following the experimental evidence reported by strong ( 1926a , b ) , and verified later by bittner ( 1931 ) and by cloudman ( 1932a , b )  . little ( 1941 ) stated the problem in different terms from those he used in 1914 . he now states : " in accepting as a working hypothesis the statement that cancer ilfils the requirements of a somatic mutation , namely , a sudden change which is perpetuated in succeeding cell generations , it must be noted that there are already on record two distinct general types of somatic mutation , either of which might be involved in the appearance of cancer . 
the other has a sporadic etiology dependent on various influences which affect individual cells or groups in the first category belong such cases as mutations in colour of cells directly . genes in rodents described by castle , pincus , bittner and others . 
one of castle 's cases is particularly interesting in that it shows several cases of mutations occurring in several generations of a single family of rabbits , thus indicating a definite cases of the second type have been recorded as the result of genetic basis . lockhart - mummery ( 1934 ) has published a exposure to radio - active agents . " book on mutations and cancer , and there have been several other articles dealing with this problem . these cannot be discussed at this time . the disovery that carcinogenic compounds can induce mutations when injected into suitable experimental animals has not originated the idea that cancer may arise by a process of somatic mutation , but rather has reopened interest in an old concept . 
some experimental evidence , although of an indirect nature , has been obtained , and it is clear that there is no evidence contrary to such a somatic mutation concept . 
on the other hand , the somatic - mutation theory hardly explains the embryonic features of malignant tumours ; and it does not explain why growths are more frequent in older than in younger individuals , because it has not been observed that mutations in cells of the gonads are more frequent in older than in younger persons . 
by this means he has reported many mutations ( notably sex - linked lethals ) with the carcinogenic hydrocarbons , and has stated that he has obtained a few chromosome breaks in his experimental material . it is an established fact that the term mutagenic is not an absolute characteristic for any physical or chemical agent . for example , it may be said that x - rays are a powerful mutagen . they are very effective in inducing mutations in drosophila and in neurospora , and to acertain extent in maize , but do so very poorly in mice . 
on the other hand , ultra - violet light appears to be more effective in inducing mutations in maize than in drosophila . again it must be taken into consideration that the different physical and chemical agentsbring about mutations in various ways . x - rays break chromosomes , thus leading to rearrangements of parts , transpositions and inversions , to deletions , etc . ultra - violet light , however , seems more effective in inducing point mutations in both corn and drosophila , possibly by a specific wave - length , 2600 , that is selectively absorbed by the nucleoproviding proteins of the chromosomes . 
strong sex ratios and in distorted mendelian ratios which may be later proven to be chromosomal , but so far all mutations induced by methylancholthrene in mice finally , the which have been tested have been proven to be point mutations . mustard gas derivatives , the fourth group of powerful mutagens seem very effective in breaking chromosomes , producing embryonic disturbances very similar to the effects of x - rays , but apparently may have another action on mutagenesis , since they appear to affect cells even before there be any evidence of cell division ( action therefore similar , but possibly different from that obtained with x - rays )  . carcinogenesis again is a relative rather than an absolute property . 
on the other hand , other species are extremely liable to great resistance to experimentally for example , the rhesus monkeys in new haven have been induced tumours . injected with methylcholanthrene for 15 years without producing a single neoone must conclude , therefore , that for this species methylplastic tumour . cholanthrene is not a carcinogen , or at least , if it is , the evidence for such a conclusion is still not available . 
the problem is even more complex than this , as will be indicated in the following discussion . not all of the biological variants obtained in mice with methylcholanthrene are genetic . 
the somatic mosaic may be due to a chromosomal aberration rather than a point mutation in somatic differentiation , although the actual mechanism involved in their origin cannot be determined . we have obtained , therefore , a multiplicity of biological effects when methylcholanthrene has been injected into a series of mice over many generations . whether all these phenomena are due to the original methylcholanthrene or to one or many of the derived metabolites is still not known . 
some of these effects are definite point mutations , some are non - genetic , some are non - genetic produced possibly by inhibitions of embryonic morphogenesis at critical periods , and other biological effects may have other mechanisms in their origin , such as abnormal distribution of chromosomes during morphogenesis . but these mice whose ancestry has been injected with methylcholanthrene for many generations are not only giving rise to a wealth of biological effects , but also to a great variety of cancers . 
the first genetic result was the production of germinal mutations which changed the rate at which fibrosarcomas appeared at the site of injection of methylcholanthrene ( a decreased latent period )  . 
the second genetic effect was the production of spontaneous lesions involving the mucus - secreting cells of the gastric mucosa following the induction of this same gastric lesion from the subcutaneous injection of methylcholanthrene . 
the appearance of this specific type of pathological lesion was brought about by a mutation on the " brown tagged " chromosome . several new sudden changes have appeared in the gastric lesion subline changing the latent period for the appearance of the lesion - a phenomenon that was obtained in the transplantation of adenocarcinomata of the mammary gland in mice and discussed in this same paper . 
1. received for publication march 25 , 1947 . tins investigation was undertaken to bring up to date the records of the middlesex hospital , and to attempt to discover whether there was any statistical evidence to support commonly held views on factors affecting prognosis and methods of treatment . 836 cases of carcinoma of the female breast treated during the years 1926 - 35 were analysed and a smaller group of 265 cases , treated during the years 1936 - 40 , were the subject of a further investigation to discover the effect of more modern methods of treatment . the hopes held at the start of this work have not been completely fulfilled . for such an investigation to give a clear cut statistical answer to all of the controversial questions , careful planning and equal distribution of cases , according to the extent of the disease and type of treatment used , would be necessary . this was not so in this series of cases . 
as a result the evidence on some points is too inconclusive to give an answer . careful analysis of results would seem to be essential if methods of treatment are to be guided by fact rather than by impressions . if , in the future , reliable figures on a large scale are to be obtained , co - ordination of policy in treatment and planning ahead in large medical formations will be necessary . whether this is acceptable or desirable may be open to argument , for it must inevitably mean some acceptance by each individual surgeon of the combined opinion of his colleagues . only thus , however , can the successful analysis of large series be substituted for the analysis of smaller series for individual surgeons . despite the difficulties that have arisen owing to the many variations in technique during the years covering this investigation , certain facts that may be of interest and value have emerged . 
some previously held views have been supported ; others appear to be incorrect . the histological findings in this series have been omitted owing to the impracticability of examining over 1000 sections in the time available . this in itself would make the basis of a separate inquiry . from the statistical point of view therefore it has been assumed that any variations in the histological grouping of the growths have been spread evenly throughout the series . the presentation of results of an investigation such as this is difficult . while the actual detailed figures and tables by which conclusions have been reached are of importance , their inclusion in the text would make reading wearisome . therefore simplified tables only have been included . * late surgical registrar ( demobilized )  . 
a case dying of other causes or of unknown causes cannot really be called a success or a failure . two ways of expressing the result seem to be possible - the survival rate or the mortality rate . 
the former has the advantage that it allows easier comparison with previous series that are almost universally expressed in terms of survival it would appear , however , that results expressed in terms of ( or cure ) rates . those actually dying of carcinoma of the breast will give a more accurate picture of effects of various factors influencing the prognosis . for these reasons the " mortality rate " has been used as a routine in this it has been expressed as the percentage of those cases dead from carcinoma paper . of the breast of all traced cases . 
when both ulceration and axillary gland involvement are present as in stage iiib cases the outlook is gloomy in the extreme . the survival rate for stage i cases is 51 - 4 per cent . this appears poor when compared with other series , but it should be remembered that this figure includes only those cases alive . 
any case dying of unknown cause or other cause in this method of calculating the survival rate would be counted as a failure . if such cases are excluded from the total the figure would be very close to 60 per cent . a point that is striking is the number of cases that die from a carcinoma of the breast during the 5 - 10 - year period . there is a consistent increase in mortality rates . 
a further subdivision was made of cases with slight attachment into those with attachment to the skin and those with attachment to deeper tissues . the mortality rate for these sub - groups was : deep attachment skin attachment percentage ~~~~~stage . 
when a growth lay between two quadrants it was described as lying in a " mid " position . thus there were the " mid - medial , " the " mid - inferior , " the " mid - lateral " and thbe " mid - superior " positions . 
the average age for stage i growths was 55 years , for stage ii growths 54 years , and for stage iii growths 59 years . the incidence of growths in decades was : decade . 0 - 39 40 - 49 50 - 59 60 - 69 70 - 79 80 - 89  . 
when associated with surgery the radiotherapy was either the implantation of radium into the wound at the time of operation according to the method described by sampson handley ( 1922 ) or prophylactic deep x - ray therapy . the latter was given in multiple intermittent sub - erythemal doses with medium voltage . 
as would be expected , this interval was increased with the stages of the disease . thus stage i cases had an average delay of 7 months , stage ii cases of 10 months and stage iii cases of 18 months . one can therefore reason that an average case has between 7 and 10 months ' unforgrace before the catastrophe of axillary gland involvement takes place . tunately there is too much variance in individual growths for this figure to be of anly real value . 
they should probably be called " insufficiently treated , " but have those under the heading " breast , been included in this analysis for convenience . contralateral " are those in which the evidence strongly suggests a true recurrence rather than a second primary . the low incidence of mediastinal recurrences is probably due to the fact that practitioners were likely to call any intrathoracic recurrences " pulmonary metathese figures , however , do not lend support to rowlands and turner stasis . " ( 1936 ) , who state that the mediastinum is the commonest site for a recurrence . this investigation has cleared up one point that has been debated in the past . there is a direct path of spread from the breast to the supraclavicular glands . of 91 cases that developed recurrences in those glands 17 were stage i cases , treated by radical mastectomy , and with axillary glands proved to be free from in view of the fact that the axillary glands were removed growth histologically . at operation and that path of spread permanently closed , the subsequent invasion of the supraclavicular glands must have been through a more direct path . relation of site of primary growth to site of recurrence . some quadrants of the breast have been considered to be more likely to metathus , inner quadrant growths have been held to give stasize in certain areas . secondaries in the chest more frequently . 
the ten to fifteen year period . no surgeon who has followed cases of carcinoma of the breast can have failed to see cases of recurrence occurring at long intervals after operation . these are often regarded as interesting rarities . 
the actual number that do develop these late recurrences is small owing to the cases that die early , and this has given the false impression that survival to five years means that the chance of recurrence is negligible . 
a few small arterioles present in the floor and edges of the ulcer showed no evidence of endarteritis . at one point the tumour had penetrated the periphery of the pancreas for a there was no involvement of the common distance of approximately 2 nun . 
5 , showing invasion of the submucosal connective - tissue strata by adenocarcinoma which has , on left - hand side , lost all resemblance to normal brunner 's gland acini . 
hence there can be no reasonable doubt that it is primarily duodenal . histological appearances clearly indicate that the initial neoplastic change has involved the epithelium throughout the whole thickness of the mucous membrane , including brunner 's glands . 
burn re8earch laboratory , royal victoria infirmary , newcastle - upon - tyne . received for publication january 30 , 1954 . this is the first of a series of reports on an experiment suggested by the work strong hybridised three strains of mice , and after 3 of , strong ( 1940 , 1945 )  . inbred generations he injected subcutaneously i mg . 
to f12 injections were continued but there was selection towards resistance to tumours at the site of injection ; five sublines were then spht off and the mice injected for a further 4 generations , after which one group was set aside and bred from without further treatment . the experiment to be reported here differs in several respects from that of strong ( 1940 , 1945 )  . 
towards the ' end of 1945 two inbred strains of mice , the nbt ( newcastle bone tumour ) and the cba ( one of the ancestral strains used by strong ) were crossed in both directions . half the mice in each f , htter were injected subcutaneously in the right flank at the age of 2 months with i mg . methylcholanthrene in 0 - 1 c.c. 
sesame oil ( one inject ' lon only ) ; the other half were not treated and were bred from ( brother - sister matings only ) for 12 generations , ar untreated . 
the untreated reciprocal - hybrid strains were known as the cba / nbt and nbt / cba strains , or cn and nc for short , the maternal strain being given first . the injected f , mice were also bred from , their inbred descendants likewise being injected and subsequently bred from for a total of 10 generations . 
from the beginning an attempt was made to breed selectively for resistance to local tumours , but entirely without success ; offspring of apparently resistant inice appeared to be just as susceptible as those of susceptible mice . 
onwards etters from mice which early developed local tumours were neither injected nor bred from . finauy , as the failure to produce resistant lines seemed likely to spoil the purpose of the experiment , 2 final generations ( f , , and f.2 ) were raised , in which no mice were injected . the injected reciprocal hybrids together with their untreated descendants formed the m / cba / nbt and m / nbt , / cba strains , or mcn and amc for short . mice were fed on " rat cake " compounded to the formula of the rowett institute by an aberdeen firm , supplemented with cabbage and carrot , with drinking water ad lib . the purpose of the experiment was , like strong 's ( i 940 , 1945 ) , the development of lines of mice resistant to tumours at the place of injection , so that the mice would live long enough to produce tunio ' urs at ' remote sites . 
the origin of the strain has been described ( pybus and mffler , 1938 ) and the various types of bone tumours have been described and illustrated ( pybus and mfller , 1940a , 1940b )  . afice of inbred generations 28 and 29 , coming from i pair of mice of generation 22 , were used as parents of the hybrid stra ' ms ; 131 mice ( 59 females and 72 males ) of generations 28 to 30 were treated with methylcholanthrene . 
one generation of 81 females and 94 males , an untreated , was raised from the treated mice ; 28 p , , .irs , belonging to 9 famihes , were successfuey bred from , a further 17 pairs proving sterfle . the last bone sarcomata to be seen in this strain were 4 which occurred in f27 prior to these there were 3 in f22and i in f24 . 
the purpose of the experiment was not to investigate the occurrence of local t ' umours , but ( as already stated ) to try to develop strains of mice that would be resistant to the local action of the carcinogen and would therefore live long enough to produce neoplasms at places remote from the site of injection . 
ar mice were therefore allowed to live as long as possible , and those with local tumours were killed only when the tumour grew large or showed signs of ulceration . there was a certain amount of variation in size of tumours at death , those close to the skin or in a position to rub against the box having a tendency to ulcerate 166 e . 
at first the mice were charted regularly , outhne drawings of tumours being made when they appeared and their growth followed week by week , but as the numbers of injected animals increased this became impossible and tumour sizes at death only were charted . it was observed from the initial weekly chartings that there was great variation in the , rate of growth of different tumours , but it cannot be stated whether this variation depended to any extent on the sex of the h ' ost ; it did not appear to do so . 
the males might be more susceptible than the females to the local action of the carcinogen ; i.e. , tumours might appear after a shorter latent period in males , and , even if tumour growth - rate was the same in both sexes , the males would be killed at an earlier age . 
with a very few exceptions in certain generations , many non - tumour males died prematurely and usuahy earlier than non - tumour females ( i.e. , mean age at death was less for males in ar cases except m / cba , mcn fl , and mnc f9 and flo ) , due mainly to wounds received in fighting . in some generations some of the non - tumour males which died prematurely might have developed tumours had they lived longer . this would have raised the tumour incidence and would proba - bly also have raised the mean tumour age at death in these instances . although causes i and 2 cannot be completely dismissed , there is evidence for the fourth possibihty in a comparison between the two pure strains . 
the local response o methylcholanthrene . two inbred strains to one subcutaneous injection of nbt strain . - as shown in table 1 , 59 females and 72 males were treated at local tumours appeared in 27 females ( 45 - 8 per cent ) and the age of 2 months . in 25 males ( 34 - 7 per cent )  . 
the non - tumour males in this strain died young from various causes , the principal bein - a filrhting ( 17 mice ) , while diarrhoea diarrhoea was responsible for the death of a number ( 7 ) of accounted for 8 . other causes of death in both sexes were kidney diseases , young females . pneumonia and pseudo - tubercle , and there were a few cases of neoplasms ( leukaemia , lung adenoma , mammary carcinoma and skin papillomata )  . there was no significant difference between the ages at death of tumour and non - tumour males ; from this it may be concluded that more of the males might have developed tumours had they lived longer . 
f6was a small generation of only 25 mi ' ce and 8 of th ' e io non - tumour males were dead by 6 months ; this could account partly for the lo ' w incidence . 
but f2was a very large generation with 134 females and 120 males , there being 96 tumour females ( 71 - 6 per cent ) and 94 tumour males ( 78 - 3 per cent ) , the combined incidence being 74 - 8 per cent . 
why this generation should be so susceptible is not clear at the moment . age at death : the result of inbreeding on the survival age of injected mice was evident in this experiment . in generations i to 5 , 74 mice died at 21 months and over , the oldest at 28 months ; in generations 6 to 10 only 3 mice ( non - tumour ) except for fl , to be discussed later , the ages at lived over the age of 17 months . death in each generation were not analysed separately . 
 - minbticba8train ( table iii )  . - each generation was analysed to find out whether the sexes were equally susceptible to the development oflocal tumours . with the exception of the first and third generations , the differences in each generation between the tumour incidences i ' n males and females were not significant . in fl , more than half the non - tumour males died at ages up to 7 months ( mainly due to fighting ) and the tumour incidence in the males was probably too low ; f , , was a smar generation and the early death of a number of non - tumour males had a disproportionate influence on the result . 
was a smah generation of 36 males 66 - 4 per cent ( 511 tumours in 770 males )  . and many of the non - tumour males died young , while in f4 half the non - tumour males were dead by 8 months . 
the incidences for these two generations of males were very probably too low , as some of the non - tumour mice would certainly have developed tumours had they eved longer . although it is therefore probable that the sex - difference in incidence was due to a lack of fur opportunity for the development of tumours in the males owing to a disproportionate number of the latter dying young , this cannot be presumed to be certain . a comparison of the reciprocal crosses regarding their susceptibility to local tumours was thus a comparison between an incidence of 62 - 8 per cent in the 538 mcn females and 73 - 4 per cent in the 669 mnc females ; and between 59 - 6 per cent in the 542 mcn males and 66 - 4 per cent in the 770 mnc males . 
the tumours seen were of the various types described by bonser and orr ( 1939 ) ; the greatest number were subcutaneous fibrosarcomata , of varying degrees of fibrosis ; there were a few pure fibromata , and many spindle and polymorphous - celled sarcomata . giant cells were frequently present . 
persons. 0 - 020 0 090 0 219 the difference between any pair of rates for subjects of the same age group men . 0 031 0 070 0 - 509 0 - 018 0091 0 203 is , in no instance , as great as twice the standard error of the difference . * between 0 000 and 0 - 017 , depending on the proportion of the 14 female patients dying of lung cancer who were non - smokers . all areas , england and wales . a____ - __ an opportunity to test the first assumption is provided through the courtesy of the government social survey by the use of figures for the proportions of nonsmokers in the population , obtained in the course of an independent inquiry . the subjects were interviewed in september 1951 and were a random sample of the whole population ; the definition of a " non - smoker " was the same as that used by doll and hill ( 1952 )  . 
the total number of subjects interviewed between the ages of 21 and 74 was 2 , 268 ; the numbers in each age and sex group were proportional to the numbers in the whole population and the numbers of men interviewed - particularly in the older age groupswere considerably smaller than the numbers used for the previous calculations . the results obtained by the use of the government social survey figures for the estimation of the numbers of non - smokers living at june 30 , 1950 , are shown in table v . 
1 it is seen that the estimated rates for non - smokers are ( with one exception ) slightly less than the rates for women in rural districts - that is , the lowest recorded by the registrar - general . 
the exception , the rate for non - smokers aged 25 to 44 , is derived from the experience of the smallest number of bronchial carcinoma patients and is likely to be the least reliable ; this rate lies between the lowest and the lowest but one of the registrar - general 's rates . the estimated rates are , therefore , of the order which could be expected if they represented the basic minima independent of variable environmental factors . proportion of deaths due to causes other than smoking . if the estimated rates for non - smokers are accepted as appoximately accurate , it is possible to calculate the number of deaths from lung cancer in persons between the ages of 25 and 74 which would have been expected , in the absence of smoking , by multiplying the populations given in table i by the rates for all persons given in table iv and adding the results for each age group . the number expected in 1950 would have been 1 , 875 ; the number which actually occurred was 11 , 189 . it must be presumed that the other causes of lung cancer continued to operate irrespective of the use of tobacco , and it is , therefore , concluded that about one in five of the lung cancer deaths in persons aged 25 to 74 in 1950 , were attributable to causes other than smoking . sex ratio among non - smokers . table iv shows no consistent difference between the estimated rates for men and for women ; and in the age - group 45 to 64 , for which the rates must be presumed to be the most reliable because derived from interviews with the greatest number of patients , the rates are most nearly equal . 
the data are , therefore , not grossly inconsistent with the hypothesis that in the absence of smoking there is no appreciable sex difference in the incidence of lung cancer . the closeness with which the data fit the hypothesis can be seen more readily if the rates for women ( derived from greater numbers of non - smokers than the rates for men ) are used to calculate the number of non - smokers among men with bronchial carcinoma who would have been expected to have been interviewed , if men and women suffered the same mortality . for example , the mortality rate for women aged 45 to 64 , and resident in greater london , is estimated to be 60.6 / 673 , 000 ( table iii ) ; the estimated number of male non - smokers in the same age and area of residence sub - group is 38 , 100 ( table iii ) , so that the expected number of male non - smokers dying of lung cancer in 1950 is ( 60.6 / 673 , 000 ) x 38 , 100 = 3 * 43 . altogether 1 , 473 men in this sub - group died of lung cancer , 308 r . 
the expected numbers are calculated similarly for each sub - group when , by addition , the total number of male non - smokers expected to have been interviewed is found to be 6 - 1 . 
the number actually observed was 7 . the conclusion that in the absence of smoking there is no appreciable sex difference in the incidence of lung cancer appears to be contrary to the observations reported earlier that the mortality among women in greater london was lower than that among men at each level of tobacco consumption ( doll and hill , 1952 , table xii )  . 
the observations recorded among smokers are , therefore , not incompatible with the findings among non - smokers . mortality among non - smokers in different areas . from table iv it appears that there are no consistent differences in mortality among persons resident in areas of different density of population . moreover , the rates for greater london , other urban areas and rural districts are most nearly equal in the age - group 45 to 64 in which they are likely to be subject to the least error . the essential similarity of the rates , in the absence of smoking , can be seen more readily by a method similar to that used for comparing the mortality in men and in women . 
since there is no reason to presume that any one set of rates is more reliable than another , it is preferable to calculate the number of nonsmokers with bronchial carcinoma , resident in each type of area , who would have been expected to have been interviewed , if the estimated rates for men and 310 r . 
the data are not accurate enough for an aetiological relationship to be postulated . " no difference was found in the incidence of past attacks of asthma , chronic nasal catarrh , pleural effusion and pulmonary tuberculosis between the patients with lung carcinoma and those with other forms of cancer . 
the data did not suggest that the effect of smoking was through the intermediary of other respiratory diseases . should , however , pneumonia and chronic bronchitis really predispose to the development of bronchial carcinoma independently of any association they may have with smoking , it might be expected that their effect would be seen more clearly among non - smokers than among the whole population , in whom another cause can frequently be implicated . 
the past history of respiratory illnesses has , therefore , been analysed in the 47 patients who were non - smokers and the incidence of each disease compared with the incidence which would have been expected from the experience of all patients with bronchial carcinoma of the same sex and age groups ( table viii )  . it is clear that the data provide no evidence 312 r . 
pected. 5 * 2 62 summary . a " non - smoker " is defined as a person who has never consistently smoked for as long as one year at the rate of as much as one cigarette or one gramme of tobacco a day . estimates of the mortality rates from lung cancer among non - smokers are obtained from the registrar - general 's figures for the number of deaths attributed to lung cancer and for the total population ; and from the data , obtained in a clinical inquiry into the proportion of non - smokers among patients with bronchial carcinoma and among patients with other diseases ( excluding cancer of the oral cavity , respiratory tract or intrathoracic organs )  . the assump - tions required to enable the estimates to be made are bold and the number of cases of bronchial carcinoma among non - smokers is small . the rates obtained are , therefore , highly speculative , but it is thought that they are likely to be reasonably reliable since they are consistent with other experience . it is concluded : 1 . 
that occupational hazards and the previous occurrence of certain respiratory diseases are unlikely to be of frequent aetiological importance . i am most grateful to the officers of the government social survey for permission to make use of data collected during one of their inquiries and to trade sources for data of tobacco consumption , summarised in table vi . i am deeply indebted to professor a . 
the present work was undertaken to determine whether any such action would affect the process of malignant transformation as brought about by painting a carcinogenic hydrocarbon on mouse sk material .and me ' l ' hods . 
 a drop of the solution was applied interscapularly on the skin of the mice , by paint - brush , once a week , for one year till the mice died or were sacrificed . 
at the end of the experiment one mouse group3 urethane group2 } : 2 = 5 = 6 - dibem : anthracene groupl 1 : 2 : 5 : 6 - dibenxanthracene and urethane 3 - .... 
it was found that all mice in groups 1 and 3 after six or more months ' treatment , had developed multiple pulmonary adenomas which appeared to be typically urethane - induced . 
 the results show that , under the experimental conditions described here , urethane ca~ no obvious change in the frequency or time of appearance of papillomas or epitheliomas induced by 1 : 2 : 5 : 6 - dibenzanthracene . 
consequently a better test to detect a weak inhibiting activity of urethane might have consisted of treating mouse skin with one application of the hydrocarbon , and thereafter more frequent urethane applications . 
no studies were made of the histological effects of urethane on either normal skin or skin under going malignant transformation , since the experiments suggest that any such effects have little action on the production of cancer . 
 it is most interesting to note that those mice which received urethane treat ment ( groups 1 and 3 ) had multiple lung tumours , whereas those receiving 1 : 2 : 5 : 6 - dibenzanthracene alone ( group 2 ) had none . 
 when urethane was administered to mice in their drinking water in previous experiments , a reduced fluid consumption was noted for the first few days , showing their aversion to it . 
an estimate was made of amount of urethane in a paint - brush full of the solution ( as painted on the mice ) by applying it to a cover slip and weighing after the acetone had evaporated . 
for previous studies ( cowen , 1947 ) , lung tumours in comparable numbers to those obtained here were induced in various inbred jines of mice by injecting 025 c.c. 
since total dosage was not the same , and since there are marked strain differences with respect to lung tumour response by different lines of mice , no accurate comparison can be made . 
it would be safe to say , however , that a large part of the urethane applied to the skin was absorbed by the mice in this experiment , judging by their tumour response . 
 it is not unreasonable to suppose that urethane is absorbed at least as readily from human as from mouse sk since urethane causes leucopenia in man ( moeschlin and melli , 1947 ) and lung cancer in mice ( nettleship and henshaw , 1943 ) and rats ( jaffe , 1947 ) , it would be well for those who handle this substance frequently in the laboratory or commercially to consider it a possible risk to health and consequently take effective precautions . 
 three groups of mice were painted interscapularly with an acetone solution of 1 : 2 : 5 : 6 - dibenzanthracene , urethane and a mixture of both each week . 
 this points out that most of the urethane applied to the skin was absorbed .all expenses in connection with this work were home by the british empire by it  . 
cohen. from the experimental oncology laboratory , radiation therapy department , johannesburg general hospital . received for publication february 7 , 1953 . an apparent discrepancy exists between the multiplicity of experimental cancer cures which have appeared in the literature since homologous transmission of tumours was first demonstrated , and the difficulties encountered in the therapy of human cancer . 
among the basic reasons for this are differences in the hosttumour relationship which presents a range of characteristics , from the completely unstable heterologous relationship , where the host and tumour are of different strains , or even species , to the relatively stable situation , as with human between these two extremes are the many , now or other autogenous tumours . widely used , homologous tumours displaying varying degrees of stability . 
the facile experimental cure , or spontaneous regression of a tumour followed by absolute immunity to further implants , is invariably a feature of the relatively unstable host - tumour relationship , and the less stable this relationship the more since this effective the " cure , " be it mechanical , chemical or radiological . propitious situation rarely , if ever , occurs in humans bearing autogenous tumours , experimental investigation of an animal tumour can have at best only remote application to clinical cancer therapy unless it applies in the first instance to a stable host - tumour relationship . 
as a prerequisite to any such investigation , therefore , the following criteria for stability of the host - tumour relationship are considered indispensable : ( 1 ) there shall be unequivocal evidence of malignancy , characterised by progressive growth , invasion or metastasis , and death of the host . ( 2 ) the tumour shall be genetically compatible with the host , either having arisen spontaneously or been induced in the tissues of the animal being investigated , or be transmitted by implantation into a homologous animal closely related by inbreeding to the host in which the tumour first arose . ( 3 ) the tumour shall " take " in practically 100 per cent of recipients on irnplantation , and there shall be neither spontaneous regression nor regression induced by non - specific trauma or intoxication of the host . ( 4 ) on irradiation of the tumour in situ , the curative dose shall be of the same order of magnitude as that of human tumours ( 103 to 104 r )  . ( 5 ) removal or destruction of the tumour in situ shall not evoke absolute resistanoe to further implants of the same tumour . since both human and experimental arlimal tumours can be made to regress following exposure to ionising radiations , one of the more promising avenues of 232 a . 
cohen research would appear to be the investigation of all factors affecting the radioalthough earlier work in this field has formulated certain sensitivity of tumours . fundamental principles ( krebs , 1929 ; cramer , 1932 ; crabtree and cramer , 1934 ; sugiura , 1937 ; sugiura and cohen , 1939 ; goldfeder , 1942 ) , it has been largely limited by inaccurate dosage estimation or lack of suitable biologic it is now possible for the radiobiologist to combine precise quantitamaterials . tive radiotherapy with a judicious choice of experimental hosts and tumours ; and it was with this in mind that a study of the radiobiology of the c3h mouse mammary adenocarcinoma was undertaken . 
with no added filters ( the inherent filtration of the tube - head consisting of approximately 3 moil and 1 mbakelite in addition to the glass envelope ) , giving a half - value layer of 0 34 mcu . 
of 25 cthe dose rate was 500 r / m ( 3 per cent ) measured in air . dose rates were measured in air with a secondary standard ( victoreen ) dosemeter , and corrected for atmospheric density . 
when completely filled with tissue fragments this arrangement provides full back - scatter for the field used , and avoids any heterogeneity due to variations in density or atomic number such as would be encountered with a glass slide . 
the tumour is relatively radioresistant , requiring doses of the order of 6000 r in one treatment to produce a significant number of this is essentially similar to goldfeder 's findings ( 1951 )  . 
the discrepancy isprobably due to ionisation contributed by the glass slide in which her tumour fragments were irradiated , instead of the plastic used in this experiment . it is of interest to note that the effective dosage for some other strains of mouse mammary carcinomas irradiated prior to implantation are of a similar magnitude ( lawrence , horn and strong , 1937 ; reinhard , goltz and warner , 1952 )  . considering that their more heavily filtered radiation ( hvl 1 mcu . ) has a relative biological efficiency of about four - fifths of that used in this experiment , the reported effective dosage of 3600 r is virtually identical with our findings . the results of both types of irradiation are analysed graphically in fig . 
2 using the " probit " method , from which it can be deduced that , in the case of treatment in situ ( line a ) the ld50 is 5700 ( + 140 * ) r , and for attenuation prior to implantation ( line b ) the ld50 is 2850 ( i 50 * ) r . it will be noted that the two dosage - response lines are apparently parallel , their slopes corresponding in both cases to a coefficient of variation of about 9 per cent . attenuation of tumour homoplasts by x rays prior to implantation into animals was described as early as 1909 by haaland . 
on occasion , this procedure was shown to induce a state in which the recipient became resistant to challenge with unirradiated implants of the same tumour , although rarely were adequately inbred strains immunised against homologous carcinoma ( hauschka , 1952 )  . 
 urethane ( ethylcarbamate ) has recently received much attention because of its use in the treatment of chronic myeloid leukaemia and other members of the group of diseases of doubtful nature at present called " reticuloses , " and also because of its action as a carcinogen . 
it was therefore thought to be of interest to study the action of urethane on the oxidation of tyrosine , by tyrosinase , to me1an tyrosine solution of concentration 0 - 02 per cent in buffer ph 7 4 was prepared , and ethyl carbamate solution of 10 per cent concentration in the same buffer . 
the upper limit of urethane concentration inveetigated was 5 per cent ; the lower limit at which inhibition could be detected by the method employed was 0 - 2 per cent . 
 from what is known of the chain of events in the oxidation of tyrosine to melanin ( raper , 1926 ) , it will be evident that this finding does not provide specific evidence for an action of the urethane on the enzyme . 
the further oxidation of dopa to melanin can occur without the aid of the enzyme , though the enzyme produces marked acceleration of the process , and the evidence so far given throws no light on which step in the oxidation is inhibited . 
 the method used was identical with that for tyrosine , with the exceptions that the final concentration of dopa was 0005 per cent , and the absence of the enzyme . 
 120 180 : ? 40 11 : ? 0 3692 - 6105 - 8377 095 : ? 3298 5510 7652 0901 3138 5152 7133 0893 3012 4873 6591 0860 - 2866 4639 6282 0809 2686 4257 5810 from this it appears probable that urethane affects the tyrosine - tyrosinase reaction in two ways : it inhibits the enzymatic conversion of tyrosine to dopa , and it accelerates the conversion of dopa to melan it seemed that further information might be obtained by in , estigating the effect of urethane on the enzymatic oxidation of dopa . 
on the assumption that the errors inevitably present are to be expected to operate equally in either direction , the probability of obtaining 8 results the same is only i in 128 . 
 120 180 240 lncremenu of ' ' e . ' ' 1496 2735 3714 4663 1427 2757 3768 4750 1367 2716 3768 4815 1405 2818 3957 4995 1427 2798 3925 5017 the inhibition of tyrosinase by urethane is , in view of the previously known action of this substance , not surprising . 
the autoxidative processes do not seem to have received the same attention as have the enzymatic ones , and the author has been unable to find any references in the literature to substances affecting their speeds , other than those producing marked changes in ph . 
h the urethane combines with the enzyme , and the ure thane and enzyme are present in such concentrations that they neutralize each other , there should be no difference between the reaction speeds of this solution and the control . 
the only suggestion which at present appears to cover these observations is that urethane has a greater attraction for the enzyme than has dopa , and that one or more of the first reaction products of their interaction acts as an inhibitor of the autoxidation of dopa later , when the enzyme has disposed of the urethane , and the intermediate metabolites have undergone further change to substances which presumably do not affect the progress of the oxidation of dopa , dopa is acted on by the enzyme , hence the acceleration of the reaction in its terminal stages . 
lea it must be emphasized that this explanation is purely hypothetical ; no direct evidence for the combination of tyrosinase with urethane , or of the presence of reaction product.s , either intermediate or final ( other than melanin ) , has been obtained . 
it is not suggested that the oxidation of tyrosine to melanin has any place in either the normal or abnormal metabolism of leucocytes , though there is the interesting fact that these cells do contain a polyphenolase capable of oxidizing dopa to melan but it did seem possible that other similar oxidations might be involved . 
methyl , propyl and butyl carbamates were prepared , the choice being limited to these as they are freely water - soluble , and their actions could be investigated by the method used for ethyl carbamate , and compared directly with that substance . 
it has been found advantageous to reduce these until the present level of 0001 per cent has been reached , as these lower concentrations prolong the period during which melanin formation can be esti mated by the colorimeter . 
the difference , however , is not great , an " d certainly does not seem to be of sufficient magnitude to allow of any explanation of the known action on leukaemia . 
it was thought possible that the effect of another water - soluble carcinogen and chemotherapeutic agent might throw further light on the proble the effect of di ( 2 - chloroethyl ) methylamine hydrochloride on the oxidation of tyrosine was investigated . 
it is of particular interest to compare the differences between these two solutions , when it will be noticed that the changes are , within the limits of accuracy of the method , yery regular . 
 - 0023 0071 0051 0029 - 0069 0172 - 0260 1155 1879 the suggested explanation in this case is that an intermediate metabolite of the interaction between nitrogen mustard and dopa gradually accumulates until it reaches such a concentration that it inhibits the reaction , thus masking the accelerating effect of the nitrogen mustard . 
 it therefore appears that there is a similarity of action between di ( 2 - chloro ethyl ) methylamine hydrochloride and the urethanes , and that this is in their action on autoxidation and not on enzymatic oxidation . 
it is obvious that it would be quite unjustifiable to attempt to explain the action of these substances in the leukaemias and other reticuloses on the grounds of their effects on melanin formation . 
in view of our present lack of knowledge of the reticuloses , and espe cially because of their almost inevitably fatal nature , it might be of ~nsiderable interest and possibly of value to investigate the effect on these diseases of other groups of substances which accelerate the progress of autoxidations . 
 methyl , propyl and butyl carbamat.es have the same effects , but to a lesser the water - soluble nitrogen mustard , di ( 2 - chloroethyl ) methylamine hydro chloride does not inhibit the enzymatic oxidation of tyrosine in a concentration of 0 - 2 per cent . 
they are of twofold character : ( 1 ) mortality statistics and post - mortem examinations ; ( 2 ) systematic bloodpressure examinations among people of various ages . relying on mortality statistics of the united states , fahr ( 1928 ) estimates essential hypertension to be the cause of death of 23 per cent of the population aged over 50 years , a figure which is held by volhard ( 1931 ) as being too small . bell and clawson ( 1928 ) , on the strength of exact anatomical examinations , came to the conclusion that in all cases of mortality about 7 per cent in the 40 to 49 agegroup and 13 per cent of people over 50 years are dying from hypertension . 
zondek the attempt to come to a definite estimation of the incidence of essential hypertension based on the numerous blood - pressure examinations among various classes of a certain population undoubtedly encounters certain difficulties ; one of the main difficulties lies , in my opinion , in the precise definition of essential not every rise in blood pressure , even a permanent one , is , of hypertension . it is rather easy to exclude course , connected with true essential hypertension . cases of secondary hypertension , such as those caused by bright 's disease , aortic valvular disease and hyperthyroidism ; moreover , from a statistical point of view , these cases do not play a major part , at least not in the age - group which is of particular interest to us . 
a person was not classified as suffering from essential hypertension unless , constantly , or at least in most of the exaniinations carried out , a blood pressure of more than 160 / 90 mhg was detected , i.e. , 165 / 90 or 160 / 95 and more . though a permanent diastolic pressure of 95 mhg may be regarded as a very reliable proof of the existence of essential hypertension , if diseases such as bright 's disease can be excluded , we based our examination nevertheless on a somewhat lower pressure , i.e. , 90 mhg ; we did so because people suffering from hypertension in the course of their illness may not infrequently display a lowering of their diastolic pressure , probably as a result of developing arteriosclerosis ( fishberg , 1939 )  . 
the decrease of diastolic pressure from 95 to 90 mhg as a minimum value for essential hypertension will , of course , increase the figure for the morbidity of hypertension ; but , apparently , a compensation has been created - at least in men - by relating the diastolic pressure to a minimal systolic 134 s . 
zondek pressure of 165 mhg . ( blood - pressure has always been taken while there is no statistical method , based on blood - pressure patient was sitting . ) examinations alone , which will include every case of essential hypertension , or will , with certainty , exclude every other type of hypertension ; but this is not of paramount importance , since in view of the high incidence of essential hypertension , small degrees of error will probably not be significant . it may reasonably be assumed that the figures contained in our statistics , and especially in that of master , marks and dack ( 1943 ) , indicate fairly accurately the incidence of essential hypertension in the various age - groups ; confirmation of this assumption may be noted by the figures contained in the mortality statistics ; nor do the anatomical examinations quoted above contradict this . what , in comparison , is the incidence of essential hypertension in cancer patients ? we shall not attach any importance to anything but a great deviation from the normal rate . 
the number of cancer patients referred to in this paper is 1490 ; a certain proportion of the cases has been observed by us ; as to the remainder , we obtained the necessary data from the cards of the cases put at our disposal by various hospitals of the country . 
the number of other types of carcinoma , such as carcinoma of the gall - bladder , pancreas , liver , kidneys and respiratory tract , was not great enough to be used for separate statistical elaboration . for the same reason , in men , only the cases of carcinoma of the digestive tract were statistically elaborated . essential hypertension proved to be a rather infrequent occurrence in all it is more or less the age - groups , but especially between the ages of 40 to 59 . same picture as that reproduced in the general statistics ( table i )  . though the number of cases of carcinoma of the respiratory tract examined by us was relatively small , we tended to find the same relationship to hypertension as in table i . 
we examined 37 cases in the age - group 40 to 59 , of whom only one showed hypertension . two factors may be held responsible for the rare occurrence of a combination of carcinoma and essential hypertension : ( 1 ) carcinoma may have a depressing influence on a previously existing hypertension ; ( 2 ) a person suffering from essential hypertension may have smaller tendency to develop carcinoma . the possibility of a depressing action of carcinoma cannot be denied . 
in this connection we may quote the investigations of rosenfeld ( 1929 ) , feldweg ( 1929 ) and fortunati ( 1936 ) , who were among the few who carried out systematic blood - pressure investigations in cases of cancer ; in the course of the illness a fall in blood pressure could be detected , though the fall , if present , was in most cases only moderate . 
the number of cases examined by fortunati ( 1936 ) was very small ; yet it occurred to him that high blood pressure is more often met with in cases of cancer of breast and female genitals than in cases of cancer of the digestive tract ; he failed , however , to take into consideration the normal incidence of hypertension ; therefore , he could not even try to answer the decisive question as to whether the frequent occurrence of hypertension in carcinoma of the breast and female genitals or its rare occurrence in carcinoma of the digestive tract are to be considered as extraordinary . 
ritchie. from the division of oncology , the chicago medical school , 2755 west 15th street , chicago 8 , illinois . received for publication july 31 , 1953 . by studying the life of various kinds of spontaneous and induced tumors in animals , it has been found that they sometimes undergo irreversible changes in character . for example , a papilloma induced in mouse skin by applications of carcinogen , may become a carcinoma , so changing its character ; or a spontaneous tumor of the mouse breast responding to pregnancy by an increase in growth rate may change its character and no longer respond to this stimulus . foulds ( 1949 , 1950 , 1951 ) made a special study of these changes in character , calling them " progressions " , and defining " progression " as an " irreversible , qualitative change " in a tumor . foulds then went further , claiming that different characters of the same tumor could progress independently of one another . for example , he found that in spontaneous mammary tumours in mice one character , the growth rate , might progress , and the tumor grow faster , while another , the responsiveness to pregnancy remained unchanged . foulds ( 1949 ) studied not only the spontaneous mammary tumors of mice , but also bladder tumors induced by feeding 2 - acetylaminofluorene to mice ( foulds , 1950 ) and transplantable mammary fibroadenomata in rats ( foulds , 1951 )  . in each case he found that the tumors did sometimes progress , and that progression could occur independently in different characters of the same tumor . these findings seemed so interesting as to make desirable further confirmation , and this paper records an investigation of the life of tumors induced in mouse skin by repeated applications of 9 , 10 - dimethyl - 1 , 2 - benzanthracene . 
ritchie the second type of sessile papilloma consisted mainly of epithelial tissue . the architectural pattern of the normal human epidermis was imitated , the epidermis being thickened from four to six times . 
the surface of the tumor was often hyperkeratotic . in a few cases a tumor of this type arose in a pedunculated papilloma . sheets of closely packed cells invaded the dermis and muscularis . 
most of the tumors grew at a steady rate throughout , in so far as the growth rate could be determined by the crude method used . however , definite changes in growth rate did occur . 
8 to 11 , and will be described individually , each mouse having tumors with differing behaviors demonstrating the validity of one or other of fould 's proposals . all charts illustrate the validity of rule 1 : namely , that progression occurs independently in different tumors in the same animal . 
9 also confirms fould 's rule 2 , showing three tumors , a , b and c progressing from one morphological type to another while growing at a constant rate . this type of progression , from one morphological type to another , without progression in growth rate , was much more common than progression in growth rate alone , as seen in this chart in tumor d . 
10 , and confirms the validity of fould 's rule 3 , that progression is independent of growth . in the same chart , in tumors a and b may be seen again a change in growth rate without a corresponding change in morphological type . * n 5 31_ * - - __ + * - - + b ..od / , ' / ___ _ , / " ... 
11. - showing independent progression of multiple tumors . tulmor a was malignant at its first clinical appearance , showing that at this period of its development a tumor can be all other tumors began as sessile papillomata . 
a well - known example of progression affecting only part of a tumor is the carcinomatous change which sometimes affects the tip of an adenomatous polyp of the colon in man . foulds ( 1949 ) remarked that progression could occur by gradual change or by abrupt steps . in general , the changes seen in the tumors of this experiment occurred abruptly . 
a step - wise transformation of different characters in these tumors was observed throughout their existence . this investigation was supported by a cancer control grant from the national cancer institute of the national institutes of health , u.s. 
price. from the medical research laboratory , department of pathology , university of bristol . received for publication december 8 , 1951 . during the past thirty years much useful progress has been made in the this work , of histological grading of malignant tumours of epithelial origin . which one practical application has been the attempted correlation of prognosis with histological structure of a tumour , has had many valuable results ; and although there may be not infrequent discrepancies between the histological appreciation and the outcome of treatment in any given type of neoplasm , the results have at any rate led to some attempt being made by the histo - pathologist to guide the clinician at least in qualitative terms of high or low malignancy ; and to more precise premises for the comnparison of differing methods of treatment in series of comparable cases . the starting point of this present analysis was the observation that irrespective of the mode of treatment applied , the overall five year survival rates in most published dissections of groups of cases of osteogenic sarcomata were approxinmately of a similar order . 
some of these features can , it is true , be visualised by x - ray plates . however , the interpretation of these is mainly the proper province of the radiologist , and they are seldom to be seen in theroutine pathological laboratory . for the fortunate histo - pathologist who may be granted access to such aids , the position is onlyinmproved to such an extent as the experience which he may have in the interpretation of skiagrams , which is a field with c . 
the ideal state no doubt is the close liaison between surgeon , radiodiagnostician , radiotherapist and histologist with personal conference in each and every case . such states of collaboration seldom exist under conditions of normal routine work . the histological specimens from the present series of cases have been considered under the following headings : 1 . 
to anyone working in this field the fallacies of diagnosis are only too well known , and the cases included have all been subjected to free discussion and unanimous acceptance as osteogenic sarcoma by the group of radiologists , radiotherapists , surgeons and pathologists which forms the working panel of the register . in each case the diagnosis has been based upon consideration of the full history , clinical examination , adequate skiagrams and histological sections . in some instances the histological material is derived from biopsy , in others from surgical or autopsy specimens . this has been indicated in table i , also the time relationship of the histological specimen to any pre - operative x - radiation . for histological purposes the specimens were fixed , cut and stained by the usual routine methods . 
owing to the presence in sonle sections of many multinucleated tumour giant cells , and the indistinct outlines of a large proportion of the polyhedral cells , the nucleus was taken as the unit rather than the cell . in each case a minimum of 2500 neoplastic cell nuclei were examined in each section , using a ruled internal screen in one ocular of a binocular microscope . 
as there are also 8 cases included in the series that are still alive and when last reported were well , but for periods less than 5 years , the 5 - year survival rate is best expressed as 6 in 28 cases - i.e. , 21 - 4 per cent . two of these cases died at respectively 77 and 96 months with multiple pulmonary metastases , and the writer fully supports the view that 5 years is too short a period on which to base estimates of rate of cure in patients with osteogenic sarcoma . these brief data may be compared with those published on larger series by the following : christensen ( 1925 ) , coley and pool ( 1940 ) , the results of the new york memorial hospital series mentioned by coley ( 1949 ) , geschickter and copeland ( 1949 ) , the series reported by the british empire cancer campaign ( 1949 ) , and platt ( 1951 )  . as may be expected with a relatively small group of cases , there are some differences from the larger published series , e.g. , an unduly high incidence of femoral tumtours , but the broad agreement would suggest that this group may be regarded as a fair sample from which certain conclusions may tentatively be reached . clinical grading of the tumours . the data on which the clinical assessment of degree of malignancy has been based has been considered from the following points of view : 1 . 
from observations on these tumours and other bony conditions , the writer has acquired the view that one of the essential functions of the osteoblast is the formation of osteoid tissue - the precursor of bone , from which under suitable conditions of substrate the formation of bone may occur , possibly with no further part being taken in the process by the osteoblast . 
price callus and in paget 's disease . both normal and neoplastic , may produce phosphatase . it is also generally accepted that the osteoblast , from the grounds that this cell therefore is actively concerned in the laying down of osteoid arises the essential stromal feature of this histological sub - type of osteogenic sarcoma , i.e. , the characteristic osteoid stroma , which mav also be accompanied by considerable amounts of collagen and ill - formed cartilage . however , the osteoid is the essential feature . this stromal material may , however , sometimes occur in considerable amount in a tumour which is predominantly spindle - celled , but is then usually less evident than the collagenous fibrous matrix produced by the spindle cells . 
under suitable conditions the osteoid matrix may either calcify or ossify , more often the latter , and then produce the appearance of the osteoblastic or sclerotic type of tumour . it is thus possible to subdivide this group further into i . 
from the viewpoint of the histologist the essential histological structure of any neoplasmn occurring in a bone is more characteristically shown in an area of active growth , the radiological manifestations of which are more frequently lytic than blastic . hence this feature of the amount of bony matrix is not always readily appreciable from even a large biopsy . for this reason this subdivision will not be pursued further in the present analysis ; but it should be added , however , that a markedly bony stroma is often indicative of a tumour of relatively low malignancy , and this point should receive due consideration by the person who may attempt to correlate the histological , radiological and clinical findings in any particular case . from inspection of table iv the following points are evident : 1 . 
in an approximately quantitative assessment of the amount of osteoid stroma present in these sarcomata it is seen that there is usually a rich matrix in tumours of lower grade malignancv , and conversely a relatively smaller amount in the high - grade group . there are noteworthy exceptions , and the specimens showing perhaps this stromal feature in the greatest degree were those from btr / 66 , r . 
66 , 213 , 221 and 226 , but generally this feature was less evident in the more actively growing tumours . it is emphasized that a change in ph of the substrate is only one of a number of factors concerned it is also wise to bear in mind a fallacy that may in this biochemical change . arise in sampling a bony tumour , as the more easily sectioned and hence less bony areas are frequently selected for routine diagnostic examination . quite a nuimber of these sarcomata also show chondroid stromal areas which may either calcify or ossify , both changes often being seen in adjacent areas and largely governed by two factors : 1 . 
the iimean mitotic ratio of these sarcomata decreases as one passes from this is mluch more evident in the separation of clinical grade i to grade iii , clinical grade i from the tumours of grades ii and iii . it may be noted here that based upon clinical data case btr / 136 , y . 
price by the american registry of bone sarcoma in their 1939 ( revised ) classification , and they continued to regard intrinsic fibro - sarcoma as a variant of the osteogenic group ( ewing , 1939 )  . jaffe ( 1947 ) , on the other hand , commenting upon this adheres to the stricter view and classifies fibro - sarcoma as a separate entity . from consideration of the small group of cases here reported it would seem that this differentiation is indistinct and serves no useful purpose . table v gives details of these 7 cases . this grouip is far too small to be the basis for any definite conclusions , but the following tentative points emerge : 1 . 
in the spindle - celled group there were no tumours which appeared to merit a clinical or histological grading of i on comparison with those of the larger polyhedral - celled series . this appears to be confirmed on considering the figures obtained for the mitotic ratio in these growths . .5. 
one may perhaps from this draw the conclusion that there is some evidence to suggest that in a series of these two histological types of osteogenic sarconma if composed of tumours of average or more than average malignancy that the tinme of survival is rather longer in favour of the spindle - celled type . in this small series of cases , one obvious difficulty that has arisen has been the determination of mean survival time of the sub - groups , and it is fully appreciated that the figures shown are only minimal inasmuch as cases have been included which are still living . 
on reference to table iii again it will be seen that 7 of the 9 tuiyours showed a mitotic ratio considerably greater than the average for their appropriate clinical grade . 
g - , and it is strongly suggested that the aoverning factor in the survival of any case of osteogenic sarcoma is the combination of site of origin and histological grading of the tumour . table vi shows the 36 cases of osteogenic sarcoma arranged in ascending order according to the mitotic ratio , i.e. , in order of diminishing mitotic activity . this has been subdivided into three purely histological grades of malignancy , c . 
price into those cases with a mitotic ratio less than 100 : 1 , from 100 : 1 to 400 : 1 , and greater than 400 : 1 . this may be taken as approximnating to those of greater , average and lesser degrees of nuclear activity . reference back to tables iv and v will show that all the cases there clinically graded as iii appear again as grade iii ( histological ) plus one case , btr / 157 , d . 
a - : probably favourable result of treatment has led ta unduly low clinical grading ; tumour in lower end of femur . group based on range of mitotic ratio of less than 100 . mean survival period of grade iii ( 11 ) 114 + months . 
g - , aged 14 , mitotic ratio 83 : 1 , sarcoma of lower end of femur , who survived for a total period of 18 months . another case supporting this view was btr / 157 , d . 
mean survival 11 4 months . the marked difference in the prognosis in these separated groups of cases can it would be of the greatest value to subject many again be well seen from fig . 
2. further cases to this type of analysis , to confirm if possible the significance of the mitotic ratio and to find its mean value based upon the examination of a much larger series of tumours . 
the mean mitotic ratio for this series is 238 resting nuclei to one nucleus in mitosis . analysis of the group gives the following ranges : grade i : grade ii : grade iii : m.r. 
the mean mitotic ratio for this group of sarcomata is markedly different from that which has been found in the examination of presumably related cells in non - neoplastic conditions . the author wishes to record his great indebtedness to the late s . 
much thanks are also justly due to the members of the committee of the register for their co - operation in the collection and discussion of all the cases included in this series . material has been derived from the sourceindicated below , and to the surgeons , radiotherapists , radiologists and pathologists who have referred cases to the register , due recognition and thanks for their assistance are here rendered : 1 . 
the animals were killed by cervical dislocation or by exsanguination under ether anaesthesia and the livers immediately perfused with 0 9 per cent sodium chloride solution before being removed , chilled and homogenized . 
nuclei were also prepared from the grch 15 tumour originally described by peacock ( 1933 )  . for the preparation of fowl erythrocyte nuclei the method of dounce and lan ( 1943 ) was used . in all cases the suspensions of clean nuclei were dried from the frozen state after small measured portions had been taken for dilution and counting in a haemocytometer . 
a weighed portion of dried nuclei acid - soluble 1 ( discarded ) nuclei 10% tca extraction residue lipid extraction phospholipid p residue n - naoh ab 370 insoluble 1 alkali - soluble 1 acidification acid soluble 2 precipitate dnap organic p inorganic p fig . 
2. scheme of separation of phosphorus compounds in nuclei ( modified from schmidt and thaunhauser , 1945 )  . was extracted three times with 10 per cent trichloracetic acid ( tca )  . 
the extracts were combined ( acid soluble 1 ) , but little attention was paid to this fraction since clearly much of the soluble p must already have been removed during the isolation of the nuclei . 
the extracted residue was treated with successive portions of acetone , ethanol , ethanol - chloroform ( 3 : 1 ) , warm ethanol - ether ( 3 : 1 ) and ether . these extracts were taken to dryness and the residue taken up in chloroform to form the phospholipid fraction . the dry nucleoprotein residue was incubated overnight at 37 with n naoh to hydrolyse rna to acid soluble nucleotides . 
the phosphorus which remained in solution was treated as organic phosphate ( fraction " organic p " )  . fractions " acid soluble 2 " and " organic p " should contain phosphorus derived from rna in the form of acid soluble nucleotides ( rntap )  . pentose was therefore estimated in " acid soluble 2 " by the orcinol method of mejbaum nuclei 10% tca extraction acid soluble 1 ( discarded ) residue lipid extraction phospholipid p residue 5% tca at 900 schneider extract schneider residue n nagh at 370 insoluble 2 alkali soluble 2 acidification acid soluble 3 precipitate ester phosphate inorganic p ester phosphate residue fig . 
3. - combined schneider and schmnidt - thannhauser procedure . ( 1939 ) and by the phloroglucinol method of euler and hahn ( 1946 ) , using calibration curves made from a purified sample of yeast rna , so that pentose could be read off directly in terms of ribonucleic acid phosphorus ( rnap )  . fraction " dnap " should contain phosphorus derived from dna only . deoxypentose was therefore estimated by the diphenylamine method ( dische , 1930 ) as employed by davidson and waymouth ( 1944b ) , using a calibration curve prepared from a purified specimen of thymus dna so that readings could be made directly in terms of deoxyribonucleic acid phosphorus ( dnap )  . phosphorus estimations were made on all samples by the method of allen ( 1940 )  . the optical densities of fractions " acid soluble 2 " and " dnap " were read in a beckman model du spectrophotometer at 260 m , u . 
and were read against a reagent blank . the radioactivity of each fraction was determined on a type m6 liquid counter ( 20th century electronics ) attached to a conventional scaling unit . ( ii ) the schneider ( 1945 ) technique . - a weighed portion of dried nuclei was extracted with tca and lipid solvents , as described above . 
the " schneider " residue clearly contained a mixture of phosphorus compounds , and it was therefore submitted to a schmidt - thannhauser separation by incubating in alkaline solution at 370 for 18 hours . 
to demonstrate them a separate run on a strip 57 cx 7 cwas carried out at a potential gradient of 13 - 6 volts / cfor 6 hours . after a run the paper was dried and the bands located by the ultra - violet light method of holiday and johnson ( 1949 ) and marked lightly in pencil . photographic records were made by the method of markham and smith ( 1949 ) , and occasional autoradiographs were made by leaving the paper in contact with kodak industrex type d film for about 18 days . the portions of the paper containing the bands were cut out and eluted according to consden , gordon and martin ( 1947 )  . 
davidson was determined by its position on the paper and its ultraviolet absorption spectrum . total phosphorus and radioactivity were also determined . the results of a series of analyses are shown in table i , in which the composition of bulk nuclei is given in terms of mg . 
although it might be expected that the schneider extract would contain all the phosphorus derived from rna and dna , the figure obtained for this fraction is invariably table ii . - mean values for the composition qf the single cell nucleus pg . 
at the same time the schneider residue , which might be expected to contain only phosphoprotein p , invariably shows a much higher phosphorus content than could be accounted for this discrepancy was observed by schneider ( 1945 , 1946 ) for by fraction p2 . whole tissue and has been commented on by davidson , frazer and hutchison that the schneider residue contains several different types of phosphorus ( 1951 )  . compound is made abundantly clear when it is submitted to a schmidt - thannhauser fractionation ( table i )  . the protein - bound inorganic fraction " p3 " obtained in this way corresponds roughly in amount to fraction " p2 "  . it therefore represents the true " phosphoprotein " phosphorus , and the other phosphorus compounds in the schneider residue are almost certainly derived from the nonnucleotide esters mentioned above , and from nucleic acid phosphorus which has failed to be removed in the schneider extraction although the portions of the nucleic acid molecules containing the reactive sugars have been split off from the this is clear from the fact that , in general , the figures for rnap protein . obtained by pentose estimation on the schneider extract agree with those obtained 206 w . 
davldson by pentose estimation on " acid soluble 2 " , while dnap obtained by the diphenylamine method on the schneider extract gives results which are comparable with those obtained from the schmidt - thannhauser dnap fraction . it is clear from table i that dry preparations of calf thymus and fowl erythrocyte nuclei have a much higher dna concentration and a lower rna concentration than have liver nuclei , but a quite different light is shed on the results when they are expressed as amounts of each component per nucleus ( table ii )  . 
4 , which is a photograph in ultraviolet light taken by the method of markham and smith ( 1949 )  . in the material from one sample of rat liver nuclei each nucleotide was submitted to hydrolysis with perchloric acid ( marshak and vogel , 1950 ) , and the bases so liberated examined by paper chromatography by the method of wyatt ( 1951 )  . in each nucleotide only the expected base and no other was found . it is clear therefore that nuclear rna is similar qualitatively to cytoplasmic rna . 
component b lies immediately behind component a , from which it cannot readily be separated . it is probable that component b consists essentially of the inorganic moiety associated with component a . 
component b should in fact correspond to fraction p2 derived from phosphoprotein . component d lies immediately in front of uridylic acid and component c in the space between b and d ; both c and d are organic in nature . it is clear therefore that fraction " acid soluble 2 " contains in addition to the expected ribonucleotides at least four other components of which three are organic phosphates . these components are clearly visible in the autoradiographs shown in fig . 
the incorporation of 32p into all fractions of fowl erythrocytes was so low as to make the results of the specific activity of the dnap in rabbit and rat liver is little significance . very low indeed as compared with the cytoplasmic fractions , but by contrast the specific activity of the organic p fraction which contains ribonucleotides is very in experiments in which we have compared nuclear rnap and high indeed . cytoplasmic rnap the former has always shown a much higher rate of incorporation of 32p than the latter ( davidson , mclndoe and smellie , 1951 )  . 
the high specific activity of nuclear rna is confirmed by isolation of the individual nucleotides . although there is no great difference between the activity of the nucleotides , adenylic acid tends to show the highest components c and d have activities of the same order as those of the activity . nucleotides , while the activities of components a and b together are considerably higher . 
the general pattern obtained from grch 15 tumour is similar to that for other tissues . the presence of components a , b , c and d is shown clearly in the autoradiograph in fig . 
5 , in which the areas of radioactivity are seen to correspond closely with the ultraviolet absorbing areas in the adjacent ultraviolet print . since the " dnap " fraction has a low specific activity and is precipitated from a solution of much greater specific activity , it is possible that this fraction may be contaminated with small amounts of phosphorus of high activity although it was therefore thought necessary to investigate it is washed several times . the effect of dissolving the " dnap " fraction in alkali and reprecipitating with one such reprecipitation reduced the activity by about 40 per cent , but acid . further reprecipitations proved to be unnecessary and indeed undesirable since in all experiments in which they tended to promote degradation of the material . ionophoresis was employed one reprecipitation of the dnap fraction was used . from table i it is clear that the specific activity of the dnap in rabbit and rat liver is very low indeed , and this is again evident in table iv . 
the dnap of the liver of the normal cock on the other hand has a much higher specific activity , while that of the dnap in the grch 15 tunmour , as might be expected in a rapidly growing tissue , is still higher and approaches the value for the riboit is of interest that the specific activity of the dnap in nucleotides ( table iv )  . the liver of the tumour - bearing bird is higher than that in the normal bird . 
on the other hand fairly convincing evidence for the loss of protein from the nucleus during the process of isolation from aqueous media has been reported by pollister and leuchtenberger ( 1949b ) and by dounce , tishkoff , barnett and frier ( 1950 ) , although this is contested by stedman and stedman ( 1951 )  . 
to what extent loss of rna and other phosphorus - containing constituents may occur during isolation in citric acid is quite unknown . it is clear from the results shown in table i that , as might be expected , the bulk of the phosphorus in the nucleus is present as dna , but the results of the schmidt and thannhauser procedure reveal considerable amounts of phosphorus in the " acid soluble 2 " fraction . that a large proportion of this fraction consists of the ribonucleotides produced by alkaline hydrolysis of rna is evident from the results of pentose estimations by the orcinol and phloroglucinol methods , and the results of the ionophoresis experiments have conclusively established the presence in nuclear rna of the four nucleotides which are found in rna 210 w . 
2. components a , c and .d are organic phosphates , the presence of which is responsible , in part at least , for the difference between the " organic p " fraction in table i and the rnap by the orcinol reaction . the presence of such esters has already been suggested by davidson and mclndoe ( 1949 )  . it is clear that in nuclear tissue , as in whole tissue ( davidson , frazer and hutchison , 1951 ; davidson and smellie , 1952 ) , the method of schmidt and thannhauser ( 1945 ) tends to give rather misleading results , since the rna fraction contains , in addition to ribonucleotides , considerable amounts of non - ribonucleotide phosphate . incorporation studies with 32p have revealed the rapid incorporation of the isotope into nuclear rna and its slow incorporation into dna in nongrowing tissues . although nuclear rna is much less abundant than cytoplasmic rna it is more active , as has been shown by marshak and calvet ( 1949 ) , barnum and huseby ( 1950 ) , jeener and szafarz ( 1950 ) and davidson , mclndoe and smellie ( 1951 ) using 32p and by potter , recknagel and hurlbert ( 1951 ) using labelled orotic acid . 
the present studies show that this more rapid rate of incorporation of 32p into nuclear rna holds for all four nucleotides , which become labeled to practically the same extent . the specific activities of components c and d are of the same order as those of the nucleotides 2 hours after administration of 32p , but that of the inorganic phosphate fraction is much higher ( table iv )  . this component corresponds to fraction p2 in table i and is derived mainly from " phosphoprotein , " although it may contain traces of inorganic phosphate originally present in the tissue . its presence is responsible for the fact that the activity of fraction " acid soluble 2 " is higher than that of " organic p . " the high activity of fraction p2 in whole tissue has already been commented on by davidson , frazer and hutchison ( 1951 )  . the results of the experiments on fowls confirm the observation of kelly and jones ( 1951 ) and kelly , payne , white and jones ( 1951 ) in rats that the presence of a rapidly growing tumour in the animal body leads to an increased incorporation of 32p into the liver dnap . 
this effect is still unexplained and obviously requires much further examination , since it is associated in our experiments with the rather high specific activity of normal fowl liver dna as compared with rat or rabbit liver dna . 
the high activity for the dna of the grch 15 tumour is in agreement with the results of other workers for rapidly growing tissues ( brues , tracey and cohn , 1944 ; davidson and raymond , 1948 )  . the results presented in table ii are of some interest in relation to the claims of vendrely and vendrely ( 1948 , 1949 ) and of mirsky and ris ( 1949 ) that the dna content of the cell nucleus is apparently constant for the cells of the different somatic tissues of any one species although there may be wide variations between one species and another . the implications of these observations have been discussed by davidson and leslie ( 1950a , b )  . 
as might be expected , no loss of dna from the rat liver nucleus too much stress however occurs on fasting , although the rna content falls . should not be laid on this latter observation , since the presence of minute amounts of cytoplasmic contamination could significantly alter the rna content of it has already been shown ( davidson , 1947 ) that fasting causes a the nucleus . marked fall in the total rna content of the rat liver , while the total dna content this would of course be expected if the dna content of the is unchanged . individual nuclei and the number of nuclei per liver were unaltered . in the grch 15 fowl tumour the dna content of the nucleus is approximately double that in the fowl erythrocyte or liver cell . 
the significance of this observation is as yet obscure , but a similar high value for tumour cells has been recorded by klein ( 1951 ) for several mouse tumours . 
payne. from the department of cancer research , mount vernon hospital and the radium institute , northwood , middx . received for publication may 2 , 1953 . in the course of their original work on the metabolism of 3 : 4 benzpyrene weigert and mottram ( 1946 ) noted that once the hydrocarbon had been introduced into a tissue it could only be extracted with difficulty . repeated and prolonged washing of the finely minced tissue was found necessary to remove the hydrocarbon and its metabolites . in view of this " binding " of the carcinogen and its derivatives within the cell an attempt has been made to fractionate mouse liver after treatment with 3 : 4 benzpyrene . 
the liver was chosen for detailed work as being easily handled , of adequate bulk , and as a site where metabolism of 3 : 4 benzpyrene is known to occur . 
the hydrocarbon was introduced as a colloidal susthis method was deliberately chosen as pension by intraperitoneal injection . offering the best chance of avoiding the presence of undissolved particles of hydrocarbon in the blood vessels as occurs after intravenous injection . all mice received one intraperitoneal injection of 1 c.c. 
the best known method for isolation of intact mitochondria is that devised by hogeboom , schneider and pallade this involves maceration of the tissue in 0 - 88 m sucrose solution , removal ( 1948 )  . of nuclei by low speed centrifugation and then isolation of the mitochondria by further differential centrifugation . 
payne as they caused agglutination of the mitochondria and their consequent sedimentation with the nuclear fraction . methods , such as the modified behrens technique used by mayer and gulick ( 1942 ) , where fractionation is done in organic solvents , were considered impracticable on the grounds of being liable to remove any bound benzpyrene attention was then turned to the standard methods for isofrom the tissues . these involve maceration in citric acid solutions lation of nuclear fractions . since it is generally accepted that mitochondria followed by centrifugation . however , it was found are destroyed by acids these did not appear hopeful . that using ice - cold 1 per cent citric acid as advocated by mirsky and pollister ( 1946 ) it was possible to remove a clean nuclear fraction , and then by further centrifugation at higher speed to obtain a mitochondrial fraction . 
the mitochondria obtained in this fashion were a bit swollen and distorted , but still stained readily in very dilute janus green b solutions . in bulk the fraction obtained in this fashion compared favourably with similar fractions obtained using sucrose this result was rendered less surprising , however , when it was found solutions . that the literature references to the solubility of mitochondria in acid only refer to acetic acid . on the basis of the above findings a technique using citric acid was developed . at selected intervals after injection the mice were killed by a blow on the head , this was examined under a u.v. 
lamp opened , and the entire liver removed . with wood 's glass filter , and any particles of benzpyrene detected - their fluorescence shows very distinctly against the background dull blue fluorescence of the liver - were washed off with normal saline . 
the 70 per cent acetone was selected , as previous experience had shown this to be the best solvent for benzpyrene in tissues . all fractions were spun down again to clear them , and fluorescence spectrograms were made according to the method devised by doniach , mottram and weigert ( 1943 )  . 
payne an acid mediuat ph values below about 7 - 1 both these compounds lose water to form 8 - 0 h benzpyrene . this latter has a rather indistinct spectrum , and may easily have been missed against the background fluoresence due to the tissue equally it may have been oxidised still further to the residues themselves . 5 - 8 quinone during the violent agitation associated with the maceration process . in any event it was considered that the experimental conditions employed were not suited to the quest for benzpyrene metabolites . the significance of the results obtained is difficult to assess . 
althougih biologists have for long been uneasily aware of the existence of a problem of cell heredity , its systematic analysis is the work of very recent cell heredity deals with the origin and maintenance of inherited character years . differences between cells ; more particularly , between cells that set up division its problems present themselves in their most acute , lineages by mitotic fission . if not most easily workable , form in metazoan development . the outcome of cellular differentiation in ( say ) mammalian development is the formation of a limited number of histologically definable cell genera , each one further subdivided into a variety of cellular genetic species . 
the genus " fibroblast , " as yet far from completely analysed , may be subdivided into cells which manufacture bone , cartilage , white connective - tissue fibres , and so on . genus " epidermis , " of which we have made a particular study ; includes the epidermal epithelium of the superficial skin , of the sole of the foot , the tongue , cells of each of these epidermal the claws or nails , the vagina and the cornea . species display a distinctive combination of structural or physiological properties . the epidermis of the sole of the foot , for example , has a characteristically high rate of cell division . 
but this has proved not to be the case . although plausible " phenocopies " of sole epithelium ( in the form of corns and callosities ) can be made by irritating the thin and relatively quiescent skin of the body surface , the difference between the division rates of sole and body epidermis is in fact " intrinsic " and inheritable . 
we have , for example , transplanted sole epidermis to positions in the body where it is protected by neighbouring hair and secure from mechanical irritation ; but even so , its characteristic growth rate has been maintained for at least two years , and thick pads of now functionless cuticle continue to form over it and may periodically be removed . claw epithelium tells the same story - more clearly , since the difference between claw and body epidermis is anatomically crude and obvious . 
comeal epithelium is very transparent , and its mode of cell - packing and cuticle formation is characteristic . these properties might well be the outcome of the peculiar situation in which it lives - lying taut over the unvascularized comeal dermis , relatively low in temperature , and nourished under conditions of ' ow 02 tension by the aqueous humour , and perhaps to some extent through its outer ( cuticular ) surface as well . if the difference between comeal and body epidermis were merely a difference of " nurture , " then the heter6topic transplantation of the comeal epidermis to ( say ) the chest wall should bring about its reversion to the cell type characthis does not happen . 
expand its substance and area fifty - fold by cell division and outward spread ; but it still retains its characteristic cell packing , mode of cuticle formation and exquisite transparency , so that fine regenerating dermal blood - vessels corneal grafts have are to be seen through it as clearly as through a window . proved to form a rather unstable epithelium , which never seems to achieve the firm union with the underlying corium characteristic of body skin . for this reason we have not yet been able to " ' cultivate ' " corneal epithelium as a heterotopic graft long enough to be quite sure that ' it represents a distinct epidermal species . 
we can only say that it has given no hint of reversion after fiv ' e weeks of cultivation . in general , the technique of tissue culture confirms the results of heterotopic transplantation ; but it is far less critical in its discrimination between cells of different species , because cultivation in vitro has a tendency to make different ciiltivation in vitro is not known to bring about any cells look rather alike . inherited change in differentiated cells , unless we take into account the fact that prolonged and rapid growth may perhaps cause individual cells to lose specific properties in the " growth rate dilution process " recently reported on by preer ( 1946 )  . 
the " antigenic simplification " ( gorer , 1938 , 1942 ) and anaplastic tendencies of long established and ra idly growing transplanted tumours may conceivably represent a phenomenon of similar origiia . it will be clear from the foregoing examples that the techniques we have so far used to discriminate between the several true - breeding species of epidermal cells are , in their use of heterotopic transplantation , formally identical with those used in classical experimental embryology to distinguish between cell systems undergo ' ing " self " and " dependent " differentiation . 
the study of cell heredity is likewise , in effect , the study of cellular transformation - that is , of the origin of inherited differences between the phenotypes of cells . from our point of view , the most important of the several different types of cell transformation is that which , in a rough preliminary classification , has been called infective ( medawar , 1947 )  . 
the second , a corollary of the first , is that infective transformations can be serially propagated - a cell once transformed can in its ttirn transform another . the special importance of infective transformations is that they provide clear direct evidence of the particulate nature of cell heredity , and so , indirectly , of the fact that the differences between cell species are combinatorial in nature and not smoothly blended . 
 ' the authors ' work on the inheritance of colour differences in spotted guinea - pigs ( as , in the cells of guinea - pigs ' skin is relevant here . apparently , in spotted pigs and friesian cattle ) the - pigmentation of the black skin areas can be seen during life to encroach upon the white . 
the spread is even in density and snioothly progressive , but it notmally leaves untouched the liairs of the white area that are being encroached upon , so - that - the transitional zone of black skin that was formerly white is distinguished by bearing white liairs on a black skin background . 
our interpretation of the phenomenon ( billingham and medawar , 1948 ) is , in outline , as follows : the origin and seat of pigmentary function in black or other coloured skins is the pigmentary dendritic cell , a branching cell which lives in the lower reaches of the epidermis and which in some unexplained manner " feeds " - or , as masson ( 1948 ) puts it , " injects " - rnelanin granules into the malpighian layer cells on which its branches end . pigmentary dendritic cells form a facultatively syncytial system , since the branches of neighbouring cells are sometimes confluent , and a branch from one dendritic cell , instead of ending on a malpighian cell , may sometimes apply itself to the cell body of another . in the white areas a dendritic cell system is present which is similar in every respect save one : the cells lack both melanin granules and the enzyme apparatus required for making it , and no form of merelv physical stimulus will cause them to acquire pigmentary ftinction . we have shown , not yet with final precision , that the phenomenon of pigment encroachment or spread at the pigmentation boundaries of spotted guinea - pigs is due to the transformation of white ( non - pigmentary ) dendritic cells into melaninforming cells by contact with their pigmentary neighbours . 
the transformation , once achieved , is permanent in the transformed cell and its division lineage and a white cell transformed to pigmentary function can in its tum tramform its neighbours . 
we - have now to ask whether the pigment - spread phenomenon we have analysed is a mere curiosity of nature , or whether it exemplifies a principle of general importance . the experimental system we bave been using is a very unusual one indeed , for the following reasons : most cells liberate their secretory products externally or into the general circulation . dendritic cells pass their secretory product , melanin , into the cells around them - " cytocrine " activity , as masson calls it . their neighbours are norinally the malpighian cells of the epidermis ; but , as inlasson lias pointed out , dendritic cells may also inject melanin granules into cells of quite different origin - into the cells of gut epithelium for example , if a tumour metastasis happens to bring them within reach of its branches . 
the casual leakage of enzymes from one cell into another would make nonsense of embryo ] ogical de - velopment ; no organ could exist under these conditions , with its great variety of cells of different types in intimate physical contact . 
an infective transformation can only be secured by taking advantage of peculiar cell properties , like the cytocrine properties of dendritic cells and their transiently syncytial lay - o - ut ; of peculiar animals , like spotted guinea - pigs ; or of technical tricks , like grafting claw epithelium to the skin of the chest , or - to choose an example from the illuminating pioneer work of sonneborn ( 1943a , b ) - by delaying the conjugation process of paramecium so that the conjugant pairs may 130 r . 
the relevance of these ideas of cellular heredity to cancer etiology has been dealt with by other speakers , so that only special aspects of the problem need be considered here . the centre of gravity of modern speculat - ion about tumours has altogether shifted from - the idea of the malignant cell as one which proliferates faster than its neighbours , towards the simpler and more general fact that it has acquired their rapid rate an inherited character difference from its normal homologues . of growth and their invasiveness may be the most important clinical facts about tumours , but they are not necessarily the most important biological facts . suppose , now , that we accept one variant or another of the view , that malignant cells differ from their normal homologues by the multiplication within them of an exogenous or proprietary virus or mutant plasmagene . if that view is correct , the infective propagation of tumours should be the rule rather than the ( for if we disregard the intervention of virus - like particles in rare exception . the initiation of mammary tumours in mice and in the propagation of the brownpearce carcinoma ( kidd , 1946 ) , the list of tumours or tumour - like growths initiated by viruses seems to be exhausted by the shope papilloma and a variety of chicken sarcomas . ) but what has been said above about the inherent difficulty of demonstrating infective transformationsin normal cells applies without any qualification to those which happen to be mahgnant . 
the limiting factor must be supposed to be , not the actual ' rarity of tumours rendered malignant by the propagation within them of specific virus - like particles , but our technical facilities for extracting them from malignant cells and introducing them into normal cells of a type in which they are competent to flourish ' ; in other words , not the material existence of such particles , but thoir reluctance to display infective behaviour . luckily , infection techniques are not the only ones . 
at our " disposal ; kidd 's ( 1946 , 1948 ) subtle serological analysis of the brow - n - pearce carcinoma has the great theoretical merit of overcoming their almost crippling defects , though it has certain limitations of its own . the interpretation we have put upon the phenomenon of pigment spread in guinea - pigs ' skin was said earlier to have been incompletely demonstrated for this vory reason ; altho - ligh we have the strongest circumstantial and anatomically factual evidence for supposing that the transformation we have been studying is infective in character , we have not yet been able to produce a cell - fiee extract ofpigmentary dendritic cells which will convert white dendritic cells to pigmentary function . 
of extraction are formidable enough ; we may be dealing with a small battery of oxidases , and the existence of at least two , a tyrosinase and a dopa - oxidase , is likely . 
to reproduce its action artificially cannot be technically easy ; we may be obliged in the end to resort to the crude solution offered by microinjection methods . in spite of the rarity of overt cases of infective propagation of tumours , it may nevertheless occur under circumstances in which , being clinically of trivial if the so - called melanotic carcinoma of significance , it has been overlooked . skin is in reality a tumour of dendritic cells , then it is at least conceivable that some melanomas spread infectively by the transformation of their non - malignant neighbours . such spread would be so slow as to be wholly outweighed in clinical importance by infiltrative growth and metastasis , but clinicians may know of certain peculiarities of melanotic growths which such a concept would help to it would be a mistake here , of course , to suppose that the melanotic interpret . character of such growths was itself of anything but secondary importance : some melanomas are recognizable histologically which are barely melanotic . epidermal dendritic cells of human beings , barring albinos , can be provoked into manufacturing melanin ; and an irreversible malignant or pre - malignant change might be initiated in normal dendritic cells by the cytocrine activities of their malignant neighbours before their rapid growth , and rapid elaboration of melanin , gave outward evidence of the fact . since this is a privileged occasion , speculation may be allowed to become wilder still . 
the ordinary literature of tumour transplantation is unhelpful on this point , since stock epidermal carcinomas are normally propagated by subcutaneous ( or some other form of heterotopic ) transplantation from mouse to mouse . 
the purely acinar foci found in rlllb females were shown to ' persist in the absence of milk factor in this cross - suckled substrain and in the absence of ovarian hormone . 
they were referred to as benign adenomas rather than nodular hyperplasias on account of their eventual independence of ovarian in addition some small invasive tumours were found by microscopic hormone . examination that appeared to represent intermediate stages in progression from benign to malignant growth ( pulhnger , 1952 )  . afitoses were found in both types of growth with the exception of the keratinised foci . all the morphological varieties persisted after ovariectomy in old animals . ' in order to ' test the capacity of the benign growths for progression to malignancy , transplantation of as many as could be found in the fresh state was attempted . grafts were transferred to young unmated females and to others of the same strain breeding rapidly . 
the nipple area on cork was searched under a glass cover using a dissecting microscope magnifying 7 and 14 times and with sterile forceps for the presence of benign tumours . ( these are seldom all adjacent surfaces of dissecting visible to the naked eye unless stained . ) microscope and glass cover were thoroughly wiped with absolute alcohol . the event no trouble arose from sepsis . 
as each benign growth was found it was cut out with fine scissors and placed in a sterile embryo dish with a drop of sterile water on the inside of the cover glass to provide a moist atmosphere . 
the next nipple area was then excised and similarly grafting was done either under anaesthesia through an incision or by treated . injection with needle and trocar into subcutaneous tissue or peritoneal cavity . the inoculated hosts were unmated females about 2 months old or breeding females that had already bome one litter . all were of the same strain bred by brother and sister matings . 
they were left in the latter from 12 - 18 months , with 15 as the average . fourteen subcutaneous grafts of bem ' gn growths minced with scissors were made from 8 donors into 9 rapidly breeding females . 
shujbik. from the oxford university reseach centre of tje british empire cancer campaign , sir william dunn scoo of pathology , unirersity of oxford . received for publication november 20 , 1948 . though non - carcinogenic to normal skin , croton oil elicits tumours in skin previously treated with a carcinogen for an inadequate period ( berenblum , 1941 )  . this procedure , with the modification of mottram ( 1944 ) , using only one single application of carcinogen prior to the croton oil treatment , served as the basis of a quantitative analysis of carcinogenic response ( berenblum and shubik , 1947b )  . 
the results led to the establishment of the essential difference in mechanism between the preliminary " initiating process " and the subsequent " promoting process " of carcinogenesis . for reviews of the literature dealing with earlier work on the stages of carcinogenesis , and with the previous terminologies used , see berenblum , 1944 , 1947 ; rusch , 1944 ; berenblum and shubik , 1947a and b . from this analysis ( berenblum and shubik , 1947b ) , it was concluded that the initiating process represents a sudden and irreversible change in a small minority of the cells of the treated area , giving rise to isolated " latent tumour cells , " apparently mdtinguishable morphologically from the surrounding non - neoplastic cells . 
the presence of these latent tumour cells is only demonstrable by subsequent promoting action , which converts them into morphological tumours . this promoting action is less specific than the initiating action , in that it can as readily be induced by croton oil as by continued applications of a true carcinogen . the irreversible nature of the initiating process was demonstrated by the fact that the number of tumours elicited by croton oil was as great after an interval of 20 weeks ( between the carcinogen application and the commencement of croton oil treatment ) as after an interval of only 3 days . according to this new concept , the latent period of carcinogenesis is dependent on the efficacy ' of the promoting action , while the actual turnour yield is prethis was borne out by comparative tests , determined by the initiating action . using 3 : 4 - benzpyrene , and 9 : 10 - dimethyl - 1 : 2 - benzit was found , as anthracene , as initiators , followed by croton oil treatment . expected , that whereas the percentage of tumour - bearing animals differed in the three series , the latent periods were approximately the same . 1 : 2 : 5 : 6 - dibenzanthracene , unfortunately , owing to considerations of solubilities , it was necessary , in these comparisons , to use a different concentration for each carcinogen . consequently , more than one variable was involved in the experiment . 
while the results obtained provided an adequate basis for the general conclusions referred to above , it was felt , nevertheless , that unequivocal evidence could best be 110 i . 
shubik provided by studying the effects of a series of graded concentrations of one and for this investigation , described below , the same carcinogen as initiator . 9 : 10 - dimethyl - 1 : 2 - benzanthracene was chosen as initiator . an additional purpose of this investigation was that the quantitative data thus obtained could , at the same time , serve as indirect evidence for or against the possibility of a " mutation - like change " for the initiating stage of carcinohowever , for a re - assessment of the validity of the " somatic cell genesis . mutation theory of cancer " in the light of the dual - stage mechanism of carcinogenesis , a more direct experimental approach was required . such an approach seemed possible from the following considerations . mustard gas is known to possess mutagenic properties when tested on drosophila ( auerbach and robson , 1946 , 1947 ) , and on neurospora and e . 
coli ( tatum , 1947 ) , so that , according to the somatic cell mutation theory , this compound admittedly , mustard gas is a potent should act as a carcinogenic initiator . anti - carcinogenic agent ( berenblum , 1929 ) , but this effect was shown to be confined to the later stages of carcinogenesis ( berenblum , 1929 , 1931 ) , and could thus , mustard gas should , thus be attributed to an anti - promoting action ; theoretically , still be capable of initiating action . 
the experimental areas of skin , in the inter - scapular regions , were clipped periodically all test solutions were applied with a with fine scissors for removal of hair . glass rod , and colourless , non - fluorescent , liquid paraffin ( " liquid petrolatum " ) was used as solvent throughout , for standardization of response ( berenblum and schoental , 1947 ; berenblum and shubik , 1947a )  . the main departure from the technique of the previous experiments was that instead of merely noting the numbers of tumour - bearing mice , the individual tumours were also recorded . 
from these results , and from other evidence brought forward , it was concluded that the ultimate tumour yield in carcinogenesis is pre - determined by an irreversible initiating process , while the latent period of carcinogenesis , i.e. 
the speed with which the induced " latent tumnour cells " are converted into morphological tumours , is a function of the subsequent promoting process . the idea of the possible existence of " latent tumour cells " requiring additional stimulation , i.e. 
the results suggest that the acetylaminofluorene acted as initiator , and the goitrogenic agent as promoter , in an analogous fashion to the carcinogen and the croton oil , respectivelv.y , in the case of skin experiments . in the present investigation , one and the same carcinogen was applied to the mouse 's skonce only in different ( graded ) concentrations , to serve as initiator , and then followed by repeated applications of croton oil . expressed in ratios , the concentrations of initiator ( 9 : 10 - dimethvl - l : 2 - benzanthracene in liquid paraffin ) in the four experimental groups were 1 : 3 : 9 : 27 , and the total yields of tumours for the corresponding groups were in the ratio of 1 : 6 - 6 : 12 - 4 : 26 - 5 ( table yet the average latent periods for these 4 groups were closely similar , ii )  . namely , 14 - 4 , 12 - 1 , 10 - 6 , and 11 - 8 weeks , respectively . 
not only was there a progressive increase in the total number of tumours , with increase in concentration of initiator , and also in the number of tumour - bearing animals . 
many different experimental approaches have , however , been devised in recent years to obtain , at least , indirect evidence in support of the theory , and these may conveniently be considered under the following headings : 1 . 
induction , by knonn carcinogenic agents , of mutations in louer organisms . the early studies in this field were concerned with x - ravs and ultraviolet although radiation , the literature of which is well reviewed by muller ( 1941 )  . most of this work was not directly concerned with correlating carcinogenicity 114 i . 
genetic analysis of tumour transplantation phenomena in pure strain mice . the genetic control of tumour transplantation in pure strain mice has been investigated in some detail , and the earlier work in this field is well smmarized it has been shown that a number of genes control the behaviour by little ( 1941 )  . of certain tumours , and this approach has been extended further by gorer ( 1937 , 1947 ) , showing that these genes probably determine their antigenic proalso , according to strong ( 1926 ) , bittner ( 1931 ) and others , the observed perties . sudden change in the transplantation properties of tumnours could be explained on the basis of the occurrence of mutations . 
quantitative interpretation of carcinogenic experiment . several attempts have been made to evaluate quantitatively some of the more reliable carcinogenic data , to determine whether or not such data would be in keeping with a sudden irrev%ersible change of a mutation - like nature . in the investigation of dunning , curtis and wood ( 1940 ) , the production of sarcomas in rats , by subcutaneous injection of 3 : 4 - benzpyrene , was submitted to quantitative analysis . 
the concentration of carcinogen and the volume of fluid injected , both of which were variables , were correlated with the number of tumours induced and with the latent period of tumour induction . it was found that increasing the number of foci injected did increase the number of tumours induced , whereas increasing the volume of fluid injected in one locus did not . in view of the variables involved , and for other reasons to be discussed later , these results do not lend themselves to an exact interpretation of a single response to a single stimulus . charles and luce - clausen ( 1942 ) analysed data of a mouse skin carcinogenesis experiment , using continued painting with 3 : 4 - benzpyrene , to determine whether or not this was in keeping with the concept of the somatic cell mutation theory . in their introduction , they make the primary assumption that if a mutation were the basis of carcinogenesis , it must , of necessity , be of a recessive nature , thus postulating two successive mutations to bring to light an actual tumour . there is , however , no valid reason for this assumption , which is , in fact , at variance with the theory of dominancy , as proposed by fisher ( 1930 )  . in all these previous attempts at analysing carcinogenic experiments , in which the carcinogen is allowed to act continuously , there is the inevitable complication arising from the fact that , of the two stages of carcinogenesis , only one - the initiating stage - could possibly be ascribed to a mutation , since this is the stage which involves a sudden and irreversible change , possibly affecting one cell only . 
shlbik in the present investigation , the correlation of concentration of carcinogen , as initiator , with the total number of turnours induced , has revealed approximately a direct 1 : 1 ratio . this could be taken as being in keeping with the somatic cell mutation theory . however , the other investigation , described above , does not lend support to as already mentioned , mustard gas is a potent mutagenic agent this theory . on drosophila ( auerbach and robson , 1946 , 1947 )  . since its anti - carcinogenic properties ( berenblum , 1929 , 1931 ) can undoubtedly be attributed to antipromoting action , it was to be expected , according to the somatic cell mutation theory , that when allowed to act once only on mouse 's skin , followed by repeated croton oil treatment , tumours should have arisen , the mustard gas acting as an initiator by virtue of its mutagenic properties . 
when tested , this was found not to be the case . in view of this negative finding , and in the light of the highly conflicting evidence of recent experiment in an attempt to adduce more indirect support of the theory , it becomes necessary to re - assess the validity of the theory . basically , neither proof nor disproof of the somatic cell mutation theorv of cancer is possible ( haldane , 1934 ) , as referred to above . the accumulating indirect evidence would seem to run counter to the theorinstead of supporting of the evidence presented in the present communicationi , the first experiment is consistent with the theory , while the second is strongly against it . the force of past reasoning in support of the theory has rested largely on the assumption that , given an irreversible change as the basis of carcinogenesis , the only known biological phenomenon to explain this would be a mutation . however , a closer examination of other common biological phenomena instantly reveals that this is not so . for example , in the course of the development of the embryo , the divergent differentiation that ultimately results in the irreversible cell types , e.g. 
horning. from the chester beally research institute of the royal cancer hospital , london , s.w.3. received for publication december 12 , 1948 . recfnt experience has shown that many of the growth - inhibiting agents used in the palliative treatment of cancer are carcinogenic . 
they also cause specific damage to cell nuclei and chromosomes and are able to induce mutations . the association of these biological effects of ( 1 ) growth inhibition , ( 2 ) chromosome damage , ( 3 ) production of mutations and ( 4 ) induction of cancer suggests if the that they may have a common fimundamental biochemical mechanism . induction of cancer is indeed a somatic mutation , then cancer induction might be included as a special mutation . 
the fact that x - rays can produce cancer in man was published in 1902 ( frieben , 1902 ) , seven years after rontgen 's discovery muiiller ( 1928 ) found that x - rays are mutagenic , and later mather of x - rays . and stone ( 1933 ) and koller ( 1934 ) described the chromosome damage following irradiation . 
the idea that cancer arises as a somatic mutation was supported by the demonstration of an increased incidence of mutations occurring in mice this was shown with methylcholanthrene treated with chemical carcinogens . by strong ( 1945 ) and with 1 : 2 : 5 : 6 - dibenzanthracene by carr ( 1947 )  . carcinogenic hydrocarbons inhibit the growth of animals and the establishment and growth of transplanted tumours ( haddow , scott and scott , 1937 )  . 
niicleoprotein , are believed to play an important part in cell reproduction , but their basic functions have recently developed analytical techniques , particularly not been elucidated . chromatographic analysis and the use of the ultra - violet spectrophotoilieter , have produced considerable fresh data on the composition of the nucleic acids , but much less research has been done on the protein fractions . this paper collects some information on this topic and some analytical results obtained in our laboratory are presented . the proteins found in the nucleus . mirsky and pollister ( 1946 ) were able to dissolve nuclear nucleoprotein in 1 m sodium chloride , after first removing the cytoplasniic material with 014 m saline , and to isolate this nucleoprotein by diluting the solution to a salt concentration of 014 m , when it precipitates in fibrous form . similar material could be obtained from isolated nuclei ( dounce , 1943 ) confirming that these nucleoproteins were of this extracted material was found to consist of deoxyribonuclear origin . nucleic acid and two protein fractions , one of which was classified as a histone , being readily soluble in acid and precipitated out of solution by ammonia . 
from isolated nuclei , apparently failed to do so from the chromosomes , and therefore claims respecting the identity of tr.pr. and the residual chronlosomes must await analytical confirmation . 1 - t is of special interest that cells which could be considered metabolically active ( liver , kid ' ney ) contain as mucb . 
as 50 per cent of the total isolated chromosome material in the form of residual chromosome . stedman and stedman ( 1943 , 1947 ) also isolated an acid - insoliible protein from the nucleus which they termed " chromosomin , " believing that it was the structural protein of the chromosome and that in the nucleus it was embedded in a support of nucleo - bistone . 
the work of both mirsky ( 1947 ) and stedman and stedman ( 1943 , 1947 ) seems to indicate that a protein forms the basic structure of the ebromosomes though the part played by the nucleic acid and the histone this is an important aspect but cannot be discussed here . 
from this material they isolated nucleic acid and histone , and in addition a fraction with isoelectric point between 5 - 8 and 6 - 15 , which coiistituted an appreciable proportion of the nuclear proteins . 
the evidence suggested that the fraction contained a sulphur - containing protein with an acidic isoelectric point and a protein of globulin typeif this material was , indeed , of nuclear origin , then this fraction appears to correspond in properties with the " chromosomin " ' of8tedmanandstedman ( 1943 , 1947 )  . 
the nuclei and chromosomes were fi - rst extracted with i m sodi - um chloride and then the residue was extracted with dilute sodium hydroxide . acidification cf this extract precipitated a protein which contained about 6 per cent arginine and since the nucleoprotein extracted from the nuclei has been no nucleic acid . shown to contain nucleic acid histone and tr.pr. , the alkali soluble protein here must be of different character and this is more likely to be the protein of the finally , two russian workers residual chromosomes than the tr.pr. 
fraction. ( zbarskii and debov , 1948 ) have reported that the protein remaining after the extraction of the nucleoprotein consists of two fractions , one of which is weakly acidic in character , being soluble in dilute alh - ah and having an isoelectric point 132 d . 
da - vidson and lawrie ( 1948 ) , using paper chromatography , carried out qualitative analyses of specimens of histone and non - histone ( acid - insoluble ) proteins from nuclei of calf thymus , rat liver and fowl erythrocytes . the histones contained alanine , arginine , aspartic acid , glutamic acid , isoleucine , leucine , ivsine , phenylalanine , proline , serine , tyrosine , valine and one unidentified constituent . in addition to the above amino - acids the acid - insoluble portein contained i per cent tryptophane , glycine but no lysine , and a further unidentified component . in silnilar studies khouvine and gregoire ( 1949 ) have analysed nuclear nucleoprotein from rat epithelioma and compared it with that foiind in the surrounding nectrotic the acid - extractable proteins nn - ere compared , using paper chromatotissues . graphy and found to be qualitatively the same . very recently stedman and stedman ( 1950 ) have reported arginine contents of histones from various tissues and found they all contained about 28 to 30 per cent arginine ( as per cent of total nitrogen )  . in addition these workers claim to have isolated sub - fractions of the histone of different composition , but no details of the n - iethod of extraction or fractionation are given . importance has often been attached to the tryptopbane content of the nuclear generally speaking , histone specimens have been found to contain proteins . 0 - 0 per cent to 0 - 1 per cent , while the acid - insoluble proteins have about 1 - 0 per cent tryptophane . stedman and stedman ( 1 - 947 ) believe that the presence of tryptopbane in histone is an indication of impurity . mirsky and pollister ( 1946 ) found very small amounts of tryptophane in histone , but about 0 - 8 per cent in the tr.pr. 
of the other histochemical studies reference will only be made to the recent work of thomas and steinitz ( 1950 ) using a method which will stain proteins of high arginine content in paraffin sections . 
the application of this method has indicated that the ratio of arginine - containing protein ( histone type ) to total possibly a combination of this technique protein , is greater in normal epidermis . with spectrophotometric methods will give further data on the localization of the basic proteins in the nucleus . extracted histone has been tested for bactericidal action ( nnleissman and graf , 1947 ) and the pharmacological properties of histone from avian erythrocytes bave also been studied . 
the nitrogen content of histone from both the above materials was 18 - 2 per cent . the acid - insoluble protein was prepared from the whole protein of the nucleoprotein , separated from the nucleic acid by the method of sevag , lackman and smollens ( 1938 )  . 
the solvent n - bu ' tanol - acetic acid - water ( 4 : 1 : 5 ) was used , followed bv either collidine - lutidine - water ( 1 : 1 : 4 ) or phenol - water . the papers were sprayed with 0 - 2 per cent ninhydrin and heated for 6 minutes at 100 ' c . 
to develop the characteristic ninhydrin - amino - acid colours . reference mixtures , " , , ere alwavs run at the same time . in the acid - hydrolysates of three specimens , histone and the acid - insoluble protein from thymus gland and histone from rat sarcoma , exactly the same comindeed , by this qualitative method it was not possible to ponents were found . detect any differences in composition in three fractions . all contained the following aniino - acids : alanine , arginine , aspartic acid , glutamic acid , glycine , bistidine , isoleucine and leucine , lysine , phenylalanine , proline , serine , threonine , tyrosine , were detected . 
for each analysis except in the case of the solvent ( c ) , wben half this amount was used to avoid excess of water on the coluinn . columns of potato stai - ch i cdiameter and 30 clong were used in conjunction with the following solvents : ( a ) n - butanol - n - propanol - 0 . 
moore and stein ( i 949 ) studied the recovery of individual amino - acids from mixtures and found that the chromatographic procedure on starch columns is capable of yielding recoveries of 100 3 per cent . their average recoveries were well within this rang - e and the sum of the aminoacids was almost invariably accurate to i per cent . 
by separate analysis no appreciable amount of trytophane could be found in the histone specimens . less than 0 - 04 per cent was found using the colorimetric method described by spies and chambers ( 1948 )  . 
protein was indicated in the rat sarcoma histone . the thymus histone specimen was quite negative in this test . comparing the two specimens analysed , there are no striking differences in composition . 
stedman and stedman ( 1943 ) believed that their acidinsoluble material ( chromosomin ) , despite a high content of the basic amino - acids must also contain a relatively large amount of glutamic acid . 
the present analyses do not support this claim . since the two proteins , histone and the acid - insoluble ty ] pe are so similar and are extracted together , it seems possible that they may be bonded together in the cell and are subsequently split by the extraction techniques to give basic soluble histone and a denatured " sulphurhistone " product . no considerable differences have as vet been found in the nuclear proteins of normal and neoplastic tissues . there are some small differences in the aminoacid compositions and there is evidence of ' variation in the proportions of the this may be connected with mirsky 's protein fractions in different tissues . ( 1947 ) observation on the variation of the proportion of " residual chromosomes " in the cell in relation to its metabolic acti - vity . 
complete amino - acid analyses of histone from calf thymus and from rat only small quantitative differences v - ere found , but there is sarcoma are given . evidence of a difference in the ] proportion of the protein components in different materials . this work is part of the research programme of the birmingham branch of the british empire cancer campaign . 
they reported an increase of urinary cholesterol in 19 out of 92 cancer patients . later , bruger and ehrlich ( 1943 ) , using a similar method of estimation , found a higher incidence of hypercholeshowever , the teroluria , 11 of their 32 cases giving results above normal limits . actual concentration of cholesterol reported by bruger and ehrlich in normal urine was approximately twice as great as that found by sobotka , bloch and rosenbloom . it appeared , therefore , that the methods used in these two studies must have been significantly different , and we felt that further work on the technique of estimation was needed . while admitting the possible non - specificity of the liebermann - burchard reaction , we felt that this type of method was the only one likely to find immediate clinical application , and it does appear to have given results consistent with the original work of bloch and sobotka . 
an attempt was made to correct for this error by the introduction of a blank reading , which was obtained by adding to half the urinary extract in 5 ml . 
the general procedure was to filter the urine slowly through a 3 - inch wide column of adsorbent from 1 to 3 inches in length , and after washing the column with water , to elute with 40 ml . 
maclagan treated with the liebermann - burchard reagent as described below under aluminthe final chloroform solution was invariably colourless , ium tungstate method . and gave negligible blank values when treated with 09 ml . 
the large tarry residue after alcohol - ether extraction was difficult to extract with petroleum ether and recovery of added cholesterol was poor , ranging from 30 to 70 per cent in various experiments . in this method a gross excess of sulphuric acid is used which is difficult to wash out of the precipitate and results in charring . 
for 20 minutes , and the green colour compared in the photoelectric absorptiometer ( king - gallenkamp ) with the ilford spectrum red filter ( maximum transmission 660mi . ) a preliminary calibration curve showed that beer 's law was well obeyed up to optical densities of 0 - 5 . 
proteose. the results given above under adsorption methods indicate a definite association between urinary cholesterol and protein when present , and suggest a possible association between cholesterol and proteose in normal urine . further evidence of the latter association was sought by estimating the nitrogen content of the aluminium tungstate precipitate obtained ( a ) after washing the precipitate with water as above , and ( b ) after dialysis of the original urine before precipitation . it was assumed that any nitrogen remaining in the precipitate after these procedures was attributable to urinary proteose . ( a ) washing of aluminium tungstate precipitate . - the relationship between cholesterol and proteose was investigated by serial washing of the aluminium in this experiment four identical samples of 100 ml . 
some support for this assumption was obtained by treating the washed precipitate with biuret reagent ( hiller , 1927 ) and also with the phenol reagent of folin and ciocalteu ( 1927 ) as follows : the precipitate from 5 ml . 
of normal urine with added cholesterol ( 0 - 5 mg . ) were duplicate dialysed in a collodion sac against running tap - water for 16 hours . samples were similarly dialysed for 40 and 64 hours . 
of the dialysed urine were precipitated with aluminium tungstate , and the nitrogen content of the precipitate determined by the kjeldahl method as above , without further washing . from the result of this experiment , as shown in table x , it can be seen that the m . 
the precipitated protein was removed by centrifugation , washed once with 0 - 5 per cent acetic acid and extracted three times with boiling acetone , the acetone extract evaporated to dryness and the residue extracted with petroleum ether for cholesterol determination as above . 
the experiments reported give some support to the hypothesis that the urinary cholesterol is normally associated with a urinary proteose fraction , and also with heat - coagulable protein if present . removal of heat coagulable protein does not , however , carry down the whole of the native cholesterol . urine is not a homogeneous substance , and the varying distribution of cholesterol between the deposit and supernatant urine which we have demonstrated is obviously relevant to clinical studies . this factor has been recognized previously , e.g. 
bruger in 1935 reported up to 40 per cent of the cholesterol in the urinary deposit in cases of nephritis . however , most authors have not recognized its importance , and have included the deposit even though pathological in certain cases ( sobotka , bloch and rosenbloom , 1940 ; bruger and ehrlich , 1943 )  . 
much or all of the urinary cholesterol may at times be found in the urinary deposit , or associated with heat - coagulable protein when present . this work was aided by a grant from the british empire cancer campaign to westminster hospital . 
the diet was supplemented with cod liver oil , and greens once weekly , and 2 - 3 g . bread ( 80 - 85 per cent extraction ) daily . thirty - four female and 12 male control rats received the same diet without pda or a mixed diet of rat cubes , bread , and once weekly greens . 
the value for total proteins obtained in the present experiments , in which only mature animals were employed , are higher than those found by lippman for mature animals , but lower than the values of metcoff and favour . 
the deviations of the values obtained by the specific gravity method were within + 6 - 5 and 3 - 5 per cent in 10 cases . the sera were fractionated by electrophoresis in the tiselius apparatus with the cylindrical lens schlieren optical system ( thovert , 1914 ; philpot , 1938 ; the buffer solution svensson , 1939 )  . 
the final patterns and the base lines were traced under magnification , superposed in such a way that those parts which did not show any elevation of the base line coincided . both the ascending and descending patterns were analysed . 
the aand the r - globulins appear frequently as broad regions ( moore , 1945 ) , which by overlapping with the 5 - globulin peak , made the separation of the globulins into individual groups uncertathe uncertainty in the values given for the x - , por - - globulins was + 15 per cent or less . wherever the uncertainty was greater , the combined areas of pand y - globulin were measured . 
of ascites was found together with high serum protein . the sera from 6 treated and 10 control animals were analysed by electrophoresis , and the results are given in table ii and fig . 
no difference in the patterns was found between the normal albino and blackhooded rats , on the semisynthetic diet , or on the mixed laboratory diet . all these patterns showed a double albumin peak , the components of which were separated to varying extent . ~~~~~~~~~~~~~~~i ~~01o0 ~~~~~~~~~~~~~~~~~~~~~i c0 - 3 5 - 0 - o ' - o ! a very ~asmiil fig . 
1. 20 b 30 50 gtc 5o.tu.g in the descending pattern the peak of the slower albumin component was in some cases higher than the corresponding peak in the ascending pattern , and in some cases this region in the descending side indicated gravitational instability , reminisin contrast cent of the , - anomaly , which is often seen with normal human sera . the patterns of sera from rats which developed hepatic tumours due to the ingesin no . 
the gravitational disturbance on the descending side was seen in cases 15 and 16 , and to a smaller extent in cases 13 and 14 . the concentration of the total globnlins was significantly increased in the group fed pda , while the concentration of the albumin remained unchanged . the increase occurred mainly in the [ and y - globulins with the exception of case 12 . 
3. - - e : lectrophoretic patterns of rat sera~ 1 - 10 , cotrol rats , 11 - 16 , rate fed pda._ left : = a~ - ~ling , rit = descenamig patterns . cending , right = descendig patterns . threpeaks in the ascending limb , remaining single in the descending limb - and convectional disturbances were observed near the m - globulin region of the ascending limb , but not in the descending or any other part of the ascending limb . ( similar disturbances near the 4 - globulin region have been observed with some human sera in more concentrated solution in the same buffer . ) these disturbances were not due to heat effects caused by the electric current , but probably to the formation of a gravitationally unstable region . 
the figures in brackets are percentages of the total protein . the remarkable sudden increase in the serum proteins at the time of the development of a tumour and the fact that the increase is independent of the size of the tumour seem to exclude the possibility that the increased serum protein has its source in the disintegration of tumour tissue : this sudden increase in the serum proteins has an analogy with the reaction of the body to foreign protein , where the amount of antibody produced is largely independent of the amount of antigen present . 
the results would suggest that , at least in hepatic tumours , the first pathological change in the serum proteins is an increase in the globulins , and a decrease is only the expression of the general deterioration of the diseased individual . the general impression that the serum protein of patients suffering from malignant diseases is decreased may be erroneously gained from reports ( a ) giving 146 c . 
the increase of the yand p - globulins of these rats might be due to an increase in immune bodies frequently associated with these fractions ( tiselius this explanation would be in accordance with the concept and kabat , 1939 )  . that the increase of the total serum protein in rats developing hepatic tumours is an immunological phenomenon . 
powell. from the department of experimental biology , mount vernon hospital , and the radium institute , northwood , middlesex . received for publication july 29 , 1947 . preparatory to commencing some detailed work on the metabolism of 3 : 4 - benzpyrene in the skin of the mouse consideration was given to a number of experimental factors which appeared likely to affect the reproducibility of the results . 
for quantitative work some standardization of the area to be treated was the method finally adopted was to apply the solution of benzpyrene required . through a stencil cut from sheet aluminium ( 16 gauge ) , with a hole of the desired size and shape . 
as it was desired to use a volatile solvent , acetone or benzene , for the application , the question of how much solvent to use in order to apply any given standard amount of the benzpyrene was examined . 
the use of a small volume of solvent , 005 c.c. , resuited in rapid drying and the deposition of the benzpyrene as a crust of crystals over 324 g . 
bearing in mind the points raised above , a series of determinations of the amounts of benzpyrene left in the skin at various time intervals after painting the results are shown diagrammatically in fig . 
on the other hand examination of the dissected animals showed the presence of benzpyrene distributed throughout the length of the digestive tract . this suggested that the benzpvrene was being licked from the skin by the animals . confirmation of this conclusion came from watching the behaviour of the almost immediately after painting and return to the boxes furthermore , when there is more than one painted animals . they start to clean themselves . mouse in a box they lick , not only themselves , but each other . further confirmation was obtained by painting mice and fixing them to a board with adhesive tape . 
pyrene per animal and the same procedure followed . 1 : 2 : 5 : 6 - dibenzanthracene . for the determination of lipid and nucleic acid phosphorus the animal was weighed and then killed by dislocation of the neck . the liver was removed immediately , weighed , and a sample of about 500 mg . 
from each of two lobes was analysed for lipid , " pentosenucleic acid " ( p.n.a.p. ) and " desoxypentosenucleic acid " ( d.n.a.p. ) phosphorus by a modification of the method of schmidt and thannhauser ( 1945 )  . in this modification the whole of the separation is carried out in a single centrifuge tube and transfer of material is thereby avoided . the tubes have a ground neck to which may be fitted a condenser for refiuxing the solvent in the lipid extraction stage . the dry weight of the liver was determined by drying a weighed sample of the organ in an air oven at 110 c . 
has occurred , and the decrease is due solely to an increase in the concentration of d.n.a.p. there was no significant difference in the liver weight : body weight ratio between the groups of animals on 5 per cent and 20 per cent protein diets . influence of 1 : 2 : 5 : 6 - dibenzanthracene . administration diet on either l : 2 : 5 : 6 - dibenzanthracene produced a marked increase in the p.n.a.p. 
1 , which shows the growth curves of six animals , three of which were killed before any very marked growth inhibitory effect of the carcinogen was observed , and three after considerable loss in weight had the p.n.a.p. 
concentration , and a decrease in p.n.a.p. concentration was also found in the low protein group . administration of the non - carcinogenic hydrocarbon pyrene to rats maintained on the 5 per cent protein diet produced no significant change in the nucleic acid balance . the increase which was found in the liver weight : body weight ratio in the carcinogen - treated rats did not appear to be a result of any increase in the water or neutral fat content of the livers . kennaway , kennaway and warren ( 1944 ) have observed a similarly - increased ratio in mice treated with carcinogenic hydrocarbons . non - carcinogenic substances gave only irregular results . 
no explanation of this increase in liver weight was advanced . the possibility that the increase is related to a differential inhibitory action of the carcinogen on the growth of the animal body as a whole compared with the growth of the liver is being investigated . in considering the possible relationship of the decrease in the d.n.a.p ; concentration in the livers of the carcinogen - treated rats to growth inhibition and carcinogenesis , it is of interest that gopal - ayengar ( 1947 ) has shown that in epidermal carcinogenesis , induced experimentally in mice by application of 20 - methylcholanthrene , the initial effect of the compound was to produce a decrease in the desoxyribosenucleic content of chromosome threads isolated from the epidermal cells . the low desoxyribosenucleic acid content persisted during.the precancerous ( hyperplastic ) stage and was then followed by an increase when malignancy ensued . stowell ( 1945 ) found that x - irradiation of transplanted mouse mammary carcinoma brought about an initial decrease in cellular desoxyribosenucleic acid content , and mitchell ( 1942 ) found a small increase in cytoplasmic pentose nucleotides in biopsied specimens of x - irradiated human tumours . 
she complained of cough , haemoptyses and loss of weight for about four months , but since october , 1944 , she had been feelmg listless and noticing palpitations and dyspnoea on exertion . 
a little lymphatic permeation was traced to the base of this lobe and involved the diaphragthe lower part of the lower lobe showed a fairly marked collapse together with a slight fibrosis . the left upper lobe was well aerated , but showed a sharply defined , firm area of congestion ( suggesting venous infarction )  . 
adjacent broncho - pulmonary lymph nodes are almost completely infiltrated . section of a main pulmonary vein shows neoplastic cells infiltrating the wall of the vessel ; in places these have reached the lumen and lined the wall with a thin layer of squamous carcinoma . 
ante - mortem thrombi have resulted , and some regions show early organization of the thrombus , which itself contains typical neoplastic cells . section of the left lower lobe shows lymphatic permeation by neoplasm , marked collapse and areas of oedema and haemorrhage . 
intra - alveolar phagocytes containing iron and carbon are numerous , and foreign body giant cells are seen in relation to the typical golden - yellow asbestos bodies lying in the alveoli and the finer lung trabeculae . there is marked subpleural fibrosis not related to neoplastic infiltration , but a consequence of the asbestosis . 
one section of this lobe shows that the neoplastic cells , although preserving most of the features of squamous carcinoma , nevertheless show a definite tendency to acinus formation , and here there is much secretion of mucus into the intercellular 252 r . 
the period of exposure also was long ( seven years ) , and although this is usual , cases have been reported of a neop ] asm developing after considerably shorter exposures . 
1. received for publication july 1 , 1948 . in the course of experiments on a transplantable mouse sarcoma it was observed that fresh saline extracts of tumour tissue agglutinated mouse and rabbit red cells . 
when extract and red cell suspension were mixed on a slide agglutination became visible to the naked eye within 30 seconds and appeared to be complete within 2 minutes . a number of different mouse and rat tumours , and a wide range of normal tissues , have been examined for haemagglutinating activity . 
the column was developed with several litres of light petroleum , followed by mixtures of this with progressively increasing amounts of benzene , and the eluates were collected in separate lots of about 2 l each . these were examined spectrographically , and those possessing similar fluorescent spectra were combined , evaporated to a small bulk , and dissolved in small amounts of benzene , providing the following fractions for testing : pes - a : fractions before the appearance of anthracene bands ; pes - b : those with anthracene bands predominating ; pes - c : those after anthracene , but before benzypyrene ; pes - d : all fractions containing benzypyrene bands ; pes - e : subsequent fractions , with recognizable fluorescence bands at 412 and 430m , u . ; pes - f : later fractions with main fluorescence band at 391 m ,  . ; pes - g : still later fractions with fluorescence band at 385 m ,  . in rabbits , skin tumours were obtained with fractions pes - c , pes - d , pes - e , pes - f , and somewhat more slowly with pes - g , while in mice skin tumours appeared only with fractions pes - d and pes - e . two interesting points arise from these results : the first is the confirmation of the previous experiments , mentioned above , that fractions appearing before and after the benzpyrene - containing fraction , are highly carcinogenic . 
the second is that the one appearing before benzpyrene , is far more potent for the rabbit 's than for the mouse 's skin . in a second fractionation , starting with larger quantities of tar ( 4 l ) , the same procedure was adopted , except that the original petroleum extract was shaken 160 i . 
was somewhat more active , while the highest activity was obtained with the next fraction , coming over at 170 - 180 c . the combined fraction of 160 - 180 c . 
was then chromatographed from light petroleum , and collected into four fractions : ( a ) a very early fraction , containing naphthalene and most of the anthracene . ( b ) an intermediate fraction , containing in addition to the remainder of the anthracene , fluoranthene , a large amount of chrysene , and probably chrysene homologues ( see below )  . ( c ) a large third fraction , containing all the benzyprene , also some chrysene , ( d ) a late fraction , in which 1 : 2 - benzcarbazole was recognized . these four fractions were tested on rabbit skin ; fractions ( b ) and ( c ) ( referred to as pf and ph in table i ) was found to be highly carcinogenic , while ( d ) ( fraction pi ) was less so . these fractions , on concentration , deposited crystalline material , which was collected and recrystallized several times from different solvents . one of the components proved to be chrysene , crystallizing in the first crop . 
they are neither acids nor bases , since preliminary treatment with alkali and acid , respectively , does not remove theby fractional distillation , these carcinogens appear slightly earlier than 3 : 4 - benzpyrene . 
one of these , which appeared just before benzpyrene on the chromatography column , possessed the unusual property of high carcinogenic potency for rabbit skin and none for mouse skin . the final active material obtained by the above methods of fractionation , represented more than a two hundred - fold concentration of the original tar . still consisted , however , of a mixture of substances , and the active constituent has not yet been identified . we are indebted to the city of leeds gas department for a generous supply of horizontal retort tar . 
keyser. from the department of pathology and bacteriology , wel - sh national school qf medicine , cardiff . receivecl for publication march 13 , 1954 . many observations have been published on the effect of disease or injury on the concentration of protein - bound carbohydrate ( polysaccharide , protein sugar ) or various carbohydrate - rich protein fractions in the blood serum , both in human beings and in animals . 
a study of the level of serum polysaccharide in various diseases led seibert , seibert , atno and campbell ( 1947 ) to suggest that a raised however , shetlar , bryan , concentration is associated with tissue destruction . foster , shetlar and everett ( 1949 ) put forward an apparently opposing view , namely , that such increases are a reflection of tissue proliferation or repair rather than of destruction . this paper deals with an investigation undertaken to find out what effect nitrogen mustard ( the bis compound , di ( 2 - chloroethyl ) methylamine hydrochloride , was used throughout ) or irradiation treatment might have on the serum polysaccharide level in patients with various neoplastic and allied diseases . ( in such patients raised values are usually found . ) it was hoped that sonie light might be thrown on any relationship between the polysaccharide level and tissue proliferation or destruction , since the nitrogen mustards and x - irradiation are known to cause tissue destruction or at least to inhibit actively growing tissues . another ob ' ect was to find out how much of any increase was contributed by the mucoprotein fraction . 
p - , a man , aged 50 , suffering from hodgkin 's disease , was admitted to bospital on 30.iii.50 for bis second coursfof nitrogen mustard . since the first course of - treatment a few months previously there had been an increase in essential case notes are as fohows 240 j . 
keyser dailv injections resulted in improvement correspoindidg the size of the glands . with a fall in the total white cell count and total polysaccharide , which was down nearly to normal a week after the beginning of treatment ( see table i )  . 
no significant fall in the polycourse . saccharide level occuited during the course of injections , but within 3 weeks after the end of the course it had faren by 40 mg . 
on examination it was found that the whole of the left breast was involved by growth , and biopsy showed there was no radiological evidence of secondary deposits squamous carcinoma . in chest , thorax or pelvis but there was body destruction of the radicles and laminae of vertebra u . 
at the end of 2 months , however , the total polysaccharide had fallen considerably and the mucoprotefn fraction to a lesser extent . healing of the medial half of the right breast area was progressing satisfactorily . 
on examination ( about september , 1950 ) the patient had a large mass of glands involving the whole left side of the neck , and the left tonsil was enlarged and fleshy - looking . biopsy of the neck glands showed the presence of hodgkin 's disease . 
the polysaccharide ( total and mueoprotein ) soon began to increase again , though the patient appeared to be in good health . after several months , however , she began to complain of tiredness and aching associated with a feeling of pyrexia in the evenings , for several clays at a time . these symptoms were apparently unconnected with the menstrual cycle . 
a temperature chart kept by the patient from january to may , 1952 , showed that on these days there was in fact a rise of temperature idthe evenings , usually to 100 - 101 ' f . 
normal figures found ' m this laboratory for the distribution of polysaccharide betweedthese fractions are given in table il the polysaccharide soon began to increase again and the patient 's condition deteriorated . 
 ( 1947 ) found a correlation between the levels of serum a - globulin and polysaccharide in their series of cases . using the tryptophan - perchloric acid test ( cohen , 1944 ; seibert et al . , 1948 ) we obtained evidence of a rise in the level of a serum constituent , that was believed 248 j . 
keyser to be probably polysaccharide in nature , after buming ( keyser , p949 , 1950 )  . the reaction has since been shown to be due to a polyhydroxylic acid of unknown structure ( " sialic acid " ) occurring in the proteins ( werner and odin , 1952 )  . more recently we have employed the orcinol method : both in burns and in fractitre cases pronounced rises in the level of serum polysaccharide ( total and mucoprotein ) were found ( keyser , 1952b )  . this is consistent with the tissue destruction hypothesis , but the increase might equary wer bave been connected with healing processes . that increases in the serum polysaccharide concentration occur in adimals after experimental injury was shown by shetlar , bryan et al . 
the response was a delayed one , with a maximal elevation in 3 to 6 days after the increases in polysaccharide were produced by ( among other methods ) injury . injection of talc suspensions or intrapleural injection of turpentine , causing conditions in which little tissue destructions was thought to occur ; fever was not essential for the elevation ; and the length of time that elapsed before the polysaccharide level returned to normal seemed to be correlated with the extent of repair taking place . 
they give no details , however , except in one case in which a small temporary rise is attributed this patient had previously undergone surgical removal of to inflammation . increases in the level of blood " polypeptides " as a result of the carcinoma . radium and x - ray treatment were reported by cristol and puech in 1930 . 
effect due to inhibition of a breakdown process in and around the tumour and depending on tumour growth . such a break - down process might be expected to be greatest when the tumour is growmg rapidly , and to be retarded when the tumour is subjected to an inhibitory influence such as that of the nitrogen mustards or irradiation . 
working with mice , catchpole ( 1950 ) found that connective tissue bordering on tumours contained increased amounts of water - soluble mueoproteins ; and histochemical studies suggest that in the region of tumours a process of depolymerization is taking place , whereby the components of the ground substance may become water - soluble and enter the general circulation as mucoproteins ( catchpole , 1950 ; gersh and catchpole , 1949 )  . 
the existence of such a mechanism would go far tciwards reconciling the " tissue destruction " and " tissue proliferation " hypotheses , since the two processes - growth of the tumour and consequent depolymerizait remains to be determined what tion - would be associated with one another . bearing the depolymerization hypothesis has on the rises in the level of serum this and other aspects of the problem are mucoprotein observed after in ' now being studied . in four of our cases urinary total nitrogen and nitrogenous constituents were measured in the hope that they might provide an indication of any tissue destruction taking place . that no consistent changes were found was perhaps to be expected , in view of the results of danowski et al . 
wood of the radiotherapy department for calculating the estimnated integral doses referred to in table i ; to dodwell of whitchurch hospital for much help in obtaining specimens of blood ; to our haematology laboratory for blood counts ; to a . 
philps. from the department of clinical pathology , univer8ity college , ho8pital . received for publication december 5 , 1953 . owing to recent improvements in surgical technique the chances of successful intervention in bronchial carcinoma have much improved , and the need for early diagnosis has correspondingly increased . 
the early recognition of mahgnancy , however , may be very difficult and it is hoped that the method described it does not replace histological in this paper may be a help towards diagnosis . examination of material removed at bronchoscopy , but when no tumour can be seen through the bronchoscope , or when histological examination reveals no tumour tissue it can be of great value . when there is some contra - indication to bronchoseopy , the demonstration of carcinoma cells in the sputum may be the sole means of estabhshing a diagnosis . the demonstration of atypical epithehal cers in the sputum of a patient suffering from bronchial carcinoma is not new . 
a positive result was obtained in 13 of the 25 cases . in 1935 dudgeon and wrigley pubfished details of a simple staining method that could be used on sputum films , in which they employed haemalum and eosin . they also described some varieties of neoplastic cell found in the sputum . subsequent papers ( dudgeon , 1936 ; barrett , 1938 ) enlarged upon the original work . at about the same time , gloyne ( 1937 ) described the cytology of sputum with special reference to neoplastic cells . since then , papers on the subject have been pubhshed in a number ofcountries , including britain ( gowar , 1943 ; bamforth , 1946 ; schuster , 1947 ; perrin and littlejohn , 1950 ) , america ( herbut and clerf , 1946 ; mckay , ware , atwood and harken , ' i948 ; liebow , lindskog and bloomer , 1948 ; papanicolaou , 1949 ; foot , 1952 ) , germany ( schmidtmann and sauer , 1952 ) , russia ( altgauzen , 1939 ) and denmark ( wandall 1943 , 1944 )  . 
the lastmentioned paper is quite outstanding and forms a valuable work of reference on this subject . it has a full bibliography , particularly of the continental literature . the proportion of cases of bronchial carcinoma that can be discovered by for example , sputum examination has varied in the hands of different workers . perrin and littlejohn ( 1950 ) obtained a positive result in 60 per cent whereas wandall ( 1944 ) discovered 84 per cent in this way . all of the reports to which i have had access have shown that occasionary a false positive diagnosis is made by sputum examination . while it is clear f . 
philps that such mistakes are more fikely to be made by an inexperienced worker , there remains the risk that even when the pathologist has considerable experience , errors may still occur . 
herbut and clerf ( 1946 ) point out that patients with early bronchial carcinoma frequently have no sputum and advocate the examination of bronchial secretion . in my hands the examination of sputum has been more successful and has sometimes been positive when examination of bronchial secretion has yielded a negative result . 
the routine is simple for patients who are in hospital . a specimen coughed up in the early morning , before any food or drink is taken , and before the teeth are cleaned , is sent to the laboratory . 
very often , although the specimen is produced before breakfast , it is found to contain particles of food material unless the patient has been warned to eat nothing on waking . specimens that contain particles of food visible to the naked eye should usually be rejected , but when a patient has very rttle sputum , any specimen that can be obtained should be examined . out - patients can be given containers and instructed to bring their sputum in them , but it is important that specimens so produced reach the laboratory as soon as possible , and certainly within 24 hours of being coughed up , otherwise infection and autolysis may destroy the cytological picture . specimens sent through the post , particularly in the winter ,  . 
are occasionally satisfactory , but if long delayed they are useless . the whole success of sputum examination for carcinoma cells depends in the first instance upon the selection of a suitable piece of the specimen for microscopical examination . in order that it may be clearly seen , the specimen is transferred to a petri dish and examined against a dark background . 
a mucopurulent piece that is slightly tinged should be taken if it can be found . if the specimen be frankly and uniformly purulent , then there is no alternative but to take a piece of it at randounder these circumstances the chance of finding neoplastic cells is not good , but on occasion they may be found , and are often of squamous type . it has been found that sputum produced during the first few days after the patient has had a bronchoscopy is unsuitable for examination for carcinoma cells . it contains a great deal of cellular material shed from the tracheal lining and the chance of finding neoplastic cells is therefore reduced . i have made it a practice not to examine sputum until a week has elapsed after bronchoscopy . the most suitable instrument with which to handle sputum is a pair of dissecting forceps that have been sharpened to a point on a grindstone . after a little practice , minute pieces of the specimen can be cut out and manipulated with ease . the piece of sputum removed from the gross specimen is placed on a slide , thoroughly mixed with the help of the forceps , and half of it transferred to a second slide . 
one of these is stained with methylene blue ( see below ) , and the other smeared carefully into as even and thin a layer as possible , and placed while still wet into fixative preparatory to staining with haemalum and eosin . it is essential that precautions be taken to avoid disseminating infection from tuberculous sputa . 
philps group has the advantage that films may be stored and re - examined in the light of subsequent findings , or compared with histological preparations made from a tumour . 
the precise technique used differs only in minor detail from that described by schuster ( 1947 )  . it was taught to me at the london chest hospital , and is as follows : a 0 - 5 per cent aqueous solution of methylene blue is used . 
the shde is then warmed by holding it about 8 above a bunsen flame , and at the same time the two are rapidly mixed with the forceps , until the excess moisture contributed by the stain has evaporated . 
the stained sputum is then heaped into a ridge along the middle of the slide , and a cover glass of suitable length immediately put on it and pressed down so that an even thin film is formed . such films tend to fade after an hour or so , the precise time apparently depending upon the amount of infection present in the specimen , but if it is desired that they last longer , this can sometimes be achieved by sealing round the edge of the cover glass with paraffin wax . schuster ( 1947 ) recommends the addition of glycerine to the stain in order that the preparation may keep longer . all sputa sent for examination are stained first by this technique , which is quick . 
a few crystals of mercuric chloride are allowed to remain in the bottom of the vessel containing the mixture to saturate any moisture that may be absorbed by the alcohol . 
the stain is ready for use in 24 hours and can be used repeatedly for 3 or 4 months . it should be filtered if it shows a deposit . it is essential that the film be fixed immediately after it has been spread and while it is still wet , nor at any subsequent stage must it be abowed to dry . it sometimes happens that a specially characteristic cer or clump of cers is seen in the mothylene blue film , and it is desired to make a permanent preparathis can frequently be done in the following way . 
the cover glass is slid off in a direction exactly at right angles to the long axis of the shde , an operation which occasionally destroys the preparation but more frequently leaves the film in place though somewhat smeared in a transverse direction . the slide is immediately dropped into ' the fixative , where it is left for 5 min . the methylene blue becomes purple during fixation . 
undoubtedly this is desirable , but it ' has been found in the present series that between 20 and 30 minutes are required for the preparation and complete examination of a film and it has been impracticable to examine six films from each specimen . 
the writer has found it more profitable to look at it with the naked - eye first so that any parts of it that show a streaky appearance may be especially selected for it has been found that carcinoma cells tend to occur in minute examination . streaks and when these are seen they should be searched throughout their entire length and depth . normally , films are examined with the 1 - inch objective , the i - inch objective being used only when likely cers are seen with the low power . there is little - inch objective in this work , though it is occasionany useful for demand for the examining the chromatin pattem , especiary in oat cells . 
a rather powerful lamp should be used ( a 200 watt bulb is satisfactory ) so that the condenser of the microscope may be lowered shghtly in order to obtain maximum resolution and contrast . 
the nuclear border is smooth and devoid of wrinkhng or irregularity . sometimes , particularly in infected sputum that has stood on the bench for some time , squamous cells are seen which are infiltrated with neutrophil leucocytes . 
39 shows such a carcinoma cells and can ' be a serious source of confusion . cell from a patient in whom there was no evidence of carcinoma . less commonly , a smaller type of squamous cell is seen , which stains more deeply than that just described . it is about 20 microns in diameter , and usually occurs as part of a small sheet of epithelium in the spututhe cytoplasm stains pure b ' lue ( as opposed to green ) with methylene blue , or fairly deep pink with eosthe outline of the cefl is frequently angular - a feature that is evident when such cells are seen lying singly . 
normal epithelial cells tend to be regular in shape , whereas carcinoma cells , particularly those of squamous type , show an irregularity which is best appreciated when many are seen together in the low - power field . 
macrophages. macrophages are constantly found in the sputum in large or small numbers , and are sometimes rather difficult to distinguish from carcinoma cens . many macrophages contain dust particles , which appear as black or brown granules in the haemalum and eosin - stained preparation , and as black , greenish , or purple granules in a film stained with methylene blue . sometimes in a film stained by the latter method , the macrophages are seen to contain a large number of highly refractile fat droplets . 
the presence of dust particles in a cell enables it to be identified as a macrophage , but confusion may arise through the presence of free dust particles overlying a cell and giving the impression of being contained within it . normally they are from 10 to 50 microns in diameter , but , exceptionally , large forms occur . 
as a general rule , they are more or less circular in outline , but this feature is bv no means constant and they assume a variety of shapes . spindle shaped and crescentic forms are not uncommon , and occasionally they may assume a tadpole - fike shape , and may thus be confused with some types of carcinoma cell if shape alone be relied usually the cytoplasm is eosinophilic when stained upon for identification . with haemalum and eosin , but ' it may stain somewhat brownish owing to the presence of ingested particles . 
with methylene blue , it is usuall ' stained blue but when there is a large amount of ingested material the colour may be anything from green to pinkish purple . 
the cytoplasm stains blue with methylene blue , and pink with eosin . the nucleus stains rather deeply and may show some unevenness in the distriit is circular in shape and the nuclei of neighbouring bution of the chromatin . cells in a clump maintain their shape and do not indent each other . cells from oat cell carcinomata , when seen in the sputum , are similar in size to lymphocytes , but differ from them in the following ways : ( a ) the nucleus of an oat cell is larger in relation to the cell area than that of a lymphocyte . 
the cytoplasm of an oat cer appears as only a thin rim round the nucleus , or it may not be visible at all . ( b ) the chromatin of an oat cell sometimes stains more deeply than that of a lymphocyte , and when seen under the - inch objective , shows as a reticulum as opposed to the rather lumpy chromatin of the lymphocyte . ( c ) oat cells nearly always appear in clumps ; lymphocytes seldom do . frequently , oat cers are so closely opposed to each other that they appear t - 0 form a syncytiuthe individual cer borders of lymphocytes are always seen . ( d ) the individual nuclei of oat cers , though usually fairly constant in size , vary considerably in shape . it will be seen that neighbouring nuclei compress and indent each other . 
the only normal cell found in the sputum which occasionally shows this compression effect is the macrophage , which is unhkely to be confused with an oat cell . lymphocytes are shown in fig . 
they are circular bodies , from 10 to 20 microns in diameter . they stain deep blue with methylene blue , and pink , yellowish or - brown with eosalmost always their non - cellular nature is clear : they may show concentric rings , - radial streaking or fissures , or they may be structureless . 
43. - a drawing of a cell seen in a methylene blue filthe cell " body " is a macrophage , and the " nucleus " is a corpus amylaceum which has been taken up . this appearance should not lead to difficulty , a - s the lack of any nuclear details and the concentric rings in the corpus amylaceum make its nature obvious . 
26. - two cell bodies united by a filamentous cytoplasmic bridge . this appearance is not commonly seen , but when present it is considered by the writer to be diagnostic of squamous cell carcinoma . carcinoma whenever considerable pleomorphism is seen in epithelial cells , it should be stressed that a moderate degree may be seen in conditions unassociated fig . 
35 shows an appearance which was mistakenly thought with carcinoma . to be due to carcinoma in a patient who showed no other evidence of a tumour at the time , who has been followed for a year and has developed no sign of the disease . the staining reaction of the cytoplasm is somewhat variable , but may be of some help in identification . 
with methylene blue , it frequently stains greener than that of normal cells , but this property is shared by any degenerate epithelial cell , be it from a carcinoma or from a non - malignant condition , so it is in no way diagnostic . 
the cytoplasm of many squamous carcinoma cells is peculiar in that it appears to be more refractile than that of normal epithelial cells . the methylene blue preparation , this property shows itself by the presence of a dark , rather emerald green outline to the cell and sometimes also to the nucleus within it . 
the cytoplasm itself appears lighter and slightly luminous compared with that of the surrounding normal cells . when stained with haemalum and eosin , the cytoplasm as a general rule stains bright pink , occasionally with a tinge of orange . frequently , as in the methylene blue film , the cell appears brighter than those round it , and if it is put slightly out of focus it may shine up quite brilliantly . cells of this type have been named " bright cells " and are in my opinion diagnostic of squamous cen carcinoma . 
25. - cells from squamous cell carcinomata that give the appearance of wrinkling often , squamous carcinoma cells show a series of irregular concentric lines in the cytothese may be seen most commonly at the periphery , although they are seen to the best advantage in the methylene blue film , they show in of the cytoplasm . plasm , which appear to be minute folds . but they may also occur round the nucleus . the permanent film as well . the nuclei of squamous carcinoma cers have few constant features . another feature frequently seen in the methylene blue film is a mass of minute refractile bodies which are usually disposed in a circular manner round the nucleus . on close inspection , the individual particles sometimes appear to be angular in outhne rather than circular . 
24. - cells showing collections of minute refractile particles in the cytoplasm . these particles are transparent and tend to occur most commonly in a circular arrangement round the nucleus , but they may be seen in any part of the cell . 
normal squamous epithelial cells not uncommonly show sirnilar particles in the neighbourhood of the nucleus , but in the writer 's experience , these are not seen in such large numbers as in carcinoma cells , nor are they concentrated so definitely in one portion of the cell . these particles must be clearly distinguished from the larger , usually black , dust particles and from the large circular fat droplets that are commonly seen in macropltages . dust particles usually present no difficulty owing to their larger size , dark colour and the fact that they are evenly distributed throughout the cell . fat droplets are usually evenly distributed , and appear globular . the six drawings , and those in fig . 
the presence of mitoses in epithehal cells does not imply malignancy , as it may occur in any condition in which there is a considerable amount of epithelial regeneration . in addition to the features mentioned above , a nuihber of other characteristics may be seen which are of considera - ble help in the diagnosis of carcinoma of squamous cell type . 
a particular type of clump has been found to occur in both squamous cer and adenocarcinoma , and though not absolutely diagnostic of mahgnancv appears to be nearly always associated with it . 
the cells all appear to spring from a central point and the clump gives the impression that it may have formed part of a polypoid mass that has broken off into the sputum . if this is correct then any condition associated with papilliferous projections into a bronchus could give rise to such clumps and they might be expected in the sputum in bronchiectasis . i have not seen such clumps in bronchiectatic sputum , but a clump of this type has , nevertheless , led to a mistake . 
philps in the presence of such a change , cells from the metaplastic area would probably be seen in the sputum , but their morphology is not clearlv known . occasionary , round cells of squamous type which have the pecuhar glistening cytoplasm that one associates with keratinisation are seen in the methylene blue preparation . these cells differ from carcinoma cells in that their nuclei are regular in size and shape , though they are often somewhat large in relation to the size of the cell . 
they do not suggest carcinoma in the latter preparation , though they may give rise to suspicion in the methylene blue film . it appears that cells of this type are young squamous cells which may have been derived from the mouth or pharynx or may possibly have come from a metaplastic area in a bronchus . 
the cvtoplasm is geanty , forming at the most a thin rim round the nucleus , which nearly fills the cell . in niany cells , no cytoplasm at all is seen : in others , when the clump is examinedlinder the - j - - inch objective , cell borders cannot be defined , the ceus appearmg to form a svncvtiiithe cytoplasm when seen stains pink with eosin . the nucleus stains deeply with haemalum , and is seldom circular as the nuclei of neighbouring cells indent each other , giving the appearance of having been pressed together . this feature is of great importance in the identification of these cells , and in conjunction with the clumpiing and relatively large nuclear size , appears to be diagnostic and makes the cers easy to recognise . 
the nuclear chromatin is usually clearly defined when thecell is seen under the - ! - - inch objective , and is reminiscent of the appearance of the , reticulum of a stained reticulocyte . less commonly , particularly in degenerate cells , the nucleus may be denser and the chromatin network difficult to define . oat cells are shown in fig . 
the round cers were about twice the size of an pat cell , that is , from 20 to 25 microns in diameter , and they showed greater variation in some , the nucleus was vesicular and nearly fined the cell : than do oat cells . in others , it appeared somewhat contracted and stained more deeply , while in the third and commonest type the nucleus was quite smah and stained nearly spindle cells were seen in clumps amona the streaks of round cens . 
typically , the cells appear in clumps and show vacuolation ' of the cytoplasm , the vacuoles firequently filling the cell and pushing the nucleus to one side , often flatten ' mg ' it against the cell wall . the appearance shown in fig . 
31 , which is from the sputum of a patient diagnosed histoloyicallv as suffering from alveolar cell carcinoma , is very si ' milar to that described by the above - mentioned writers in adenocarcinoma . the presence of cells showing vacuolation is not in itself evidence of carcinoma . the cells shown in fig . 
38 were from the sputum of a patient who showed n ' o evidence of carcinoma , and who , because of th.e presence of these and similar cells has been followed for a - year and has ' developed no tumour . therefore , unless the ceus showing vacuolation occur in clumps and show other characteristics associated with malignancy , they must be considered to be unreliable as evidence of carcinoma . quite frequently , in sputa showing ample evidence of carcinoma of squamous cell type , clumps of cells are seen which surround a single vacuole . 
cers seen which constitute clear evidence of carcinoma . can be g ' iven . categories 1 , 3 and 4 appear from the results to be valuable as an indication of whether the patient has carcinoma , but the value of category 2 , judging from the analysis of results which follows , appears open to question . it will be seen that of the . 
untraced. no cells suggestive of carcinoma seen category 1 . in sputum catego , ry 2 . atypical epithelial cells seen upon which no certain opinion can be given category 3 . cells seen which are highly suggestive of carcinoma category 4 . cells seen which constitute clear evidence of carcinoma of the 9 patients untraced , 8 were out - patients in whose sputum no cells suggestive of carcinoma were found , and who did not return to the hospital . 
he left the hospital soon afterwards and the final diagnosis is not at present known to the writer . of the 8 cases recorded as not yet diagnosed , 3 had no cells suggestive of carcinoma in their sputum , 3 showed epithelial cells which were considered to be f . 
philps atypical but were not thought to constitute evidence of carcinoma , i showed cells that were highly suggestive of carcinoma and 1 , cells that were held to constitute clear evidence of it . 
the 2 patients who were diagnosed as sputum positive are both elderly men in one of whom there is strongly suggestive radiological evidence of carcinoma with persistent collapse of the right lower lobe but no tumour demonstrable on bronchoscopy . 
the other has a shadow persisting in the left mid - zone but has acid - fast bacilli in his sputuit is thought quite probable by those in clinical charge of him that he has carcinoma as well as tuberculosis . 
no bronchoscopy has been performed . * of the 123 patients , there are 106 in whom a final diagnosis has been reached . the results of sputum examination on these 106 will be considered in the analysis which follows . for the purpose of analysis , it is considered that categories 1 and 2 constitute a negative , and 3 and 4 a positive sputum diagnosis , and the terms " sputum negative " and " sputum positive " are used in this sense . it wfll be seen from table i that in two cases , cells that were highly suggestive of carcinoma were seen in the sputum of patients who were finally diagnosed as not having suffered from the condition . one of these patients has now come to post - mortem at which a diagnosis of haemorrhagic bronchitis was made : the other , who was admitted complaining of haemoptysis , is now well , with no evidence of any pulmonary lesion . 
the films ofthe sputa of both these patients have been reviewed and a single clump of cells in the former would still be held to be highly suggestive of carcinoma . in the case of the latter patient , there was a large amoudt ofrather eosinophilic epithelial debris , in the film , the appearance being one which would not now be thought by the writer to be suggestive of carcinoma unless some indication of the mahgnant nature of the cells were also present . 
of the two errors described here , the first must be held to be due to a limitation of the method , whereas the second was caused by lack of experience . of the 106 patients under review , , 39 were finally diagnosed as suffering from bronchial carcinoma , and 67 from other conditions . 
41. total cases in the series cases finally diagnosed as positive cases finally diagnosed as negative total positive diagnoses made by sputum examination correct positive diagnoses false positive diagnoses percentage of negative cases incorrectlydiagnosed as positive 30 false positive diagnoses expressed as a percentage of the total series positive cases in which carcinoma cells were not found in the sputum 9 percentage of positive cases in which carcinoma cells were not found 23percentage of positive cases correctly diagnosed by sputum examination addendum - at the time of going to press , these two patients a - re still udder observation . 
the one whose sputum contained cells that were considered clear evidence of carcinoma has now been readmitted to hospital a year after the cells were first found with clear clinical evidence of carcinoma with multiple bone metatases . 
b is sputum now contains cells similar to , but more pleomorphic than those first found . the other , whose sputum contained cells that were thought highly suggestive of carcinoma has been treated for a year for pulmonary tuberculosis and has improved , ' though the radiological picture is little changed . 
patient8 correctly diagno8ed a8 8putum negative . total patients one speciinen only examined two speciinens examined three four five total number of specimens examlined from these 65 patients mean of number of specimens examined in sputum negative patients j . 
of those who had carcinomata , 30 ( 76 - 9 per cent ) showed carcinoma cells in the sputum . sputum specimens from two patients in the series were wrongly reported as positive . 
one of these patients complained of haemoptysis but recovered rapidly and subsequently showed no evidence of any lung lesion . his sputum contained a great deal of eosinophihc cell debris which was thought to be the remains of necrotic carcinoma cells . 
he died and at post - mortem examination was diagnosed as having suffered from haemorrhagic bronchitis , no evidence of carcinoma being found . those from the first would not now be considered suggestive of carcinoma as the cells showed no other appearance associated with mahgnancy . 
the clump of cells from the second patient would still be held to be suggestive of carcinoma if seen again , which indicates that the method has limitations . further investigation is required into the significance of clumps of cells of this type . it ha - s been my experience that when a confident diagnosis of carcinoma can be made from sputum examination ' , it is usually possible to tell the predominant cell type in the tumour , and so far , when there has been an opportunity for histological confirmation , this has been show ' n to be correct . it has been stressed that in a series of this type , it is possible that misdiagnoses of carcinoma may go undiscovered because the proportion of positive cases is high . it is not certain that there are no such mistakes in the present series but since only about one third of the patients were in fact suffering from bronchial carcinoma , the chances are in favour of such errors being discovered . it is necessary that the limitation of a diagnostic technique of this type be clearly understood . 
a negative finding is of no significance in the exclusion of carcinoma , and may be due simply to the fact that the miinute portion of the specimen chosen for examination contains no cells that can be recognised as malignant . this is likely to be the commonest cause of failure . 
of these , a final diagnosis had been reached at the time of writing in 106 , 39 being shown to suffer from bronchial carcinoma . cells which were either highly suggestive of carcinoma or were considered to be clear evidence of it were seen in the sputum of 30 ( 76 - 9 per cent ) of these . 
an attempt is made to analyse the effect of the number of specimens examined upon the accuracy of diagnosis . where possible , it has been the writer 's practice to state the predominant cell type when a positive report is made . this was done in 23 of the 30 cases so reported . 
an opportun ' ity for histological confirmation has occurred in 10 of these , and there has been agreement . two sputa were erroneously thought to contain cells which were highly suggestive of carcinoma . 
the reasons for these two misdiagnoses are critically examined and it is concluded that one could have been avoided and one could not . further research is necessary to eliminate false positive diagnoses . my thanks are due to professor m . 
3. - normal bronchial epithelial cells obtained by aspiration at bronchoscopy . characteristically these cells are elongated with a ciliated free border and a filiform point of attachment to the ba - sement membrane . 
the nucleus , which ir , regular in size and oval in shape , is nearer to the attached end than to the free border of the cell and tends to make a small expansion in the cell body . 
on close inspection , however , it will be seen that a number of cells in the clump have the general shape of bronchial epithelial cells , showing a wide free border and a filiform point of attachment , and the nuclear distortion is mainly due to the presence of it is possible to discern gradations from those which appear vacuoles in the cytoplasm . nearly normal to those which seem grossly abnormal . 
the strongly eosinophilic cytoplasm is also suggestive of carcinoma , but may occasionally be seen in other degenerate epithelial cells . it should be noted that the appearance suggestive of inclusions seen in this cell differs from that shown in fig . 
the nucleus shows no unusual characteristics and is situated in the wider " body " of the cell . sometimes , chromatin masses are seen in the tail , and on occasion , two cell bodies , each containing a nucleus , are united by a long filamentous bridge . 
the writer has seen them only in cases of squamous cell carcinoma , and nothing resembling them has been seen in any sputum specimen from a non - malignant condition . they appear considerably more refractile than do normal cells , and by virtue of this property , look bright when compared with the cells that surround thewhen put slightly out of focus they shine brilliantly . the high refractility of these cells is possibly associated with keratinisation , and may be related to the appearance shown in fig . 
and the cell itself is surrounded by a greenish coloured band which is probably due to some optical property of the cytoplasm . its brilliance is enhanced compared with the cells in the surrounding field . 
the coloured band which surrounds the cell stands out clearly . in addition to the cell described , there is a considerable amount of eosinophilic debris shown , similar to that seen in fig . 
34 , which is from the sputum of a patient diagnosed clinically as suffering from bronchial carcinoma , but which is considered by the writer to constitute insufficient evidence to enable a diagnosis of carcinoma to be made . 
the present writer now shows considerable caution in the interpretation of the significance of such clumps as two mistakes have been made . before this it was thought that clumps of epithelial cells of this type constituted strong evidence of carcinoma . 
41 and 42 , which were both thought to be strongly suggestive of carcinoma , were from patients who had no other evidence of carcinoma at the tiirne , and in one of whom there wa - s later no post - mortem evidence . 
they have the following chaxacteristics which , taken together , distinguish them clearly from any other cell that is seen in the sputum : the cytopla - sm may be visible as a thin nvhere neighbouring cells are closely applied to each other , riirn , or it may not be seen at all . as is often the case , cell borders are not seen , the appearance being that of a syncytium . ( 2 ) the nuclei of all the cells in a clump are of approxiinately the same size , but they vary considerably in shape , many of them tending to be rectangular . 
the reason for this is that the nuclei of neighbouring cells indent each other . this is the most important single feature in the identification of oat cells . ( 3 ) the nucleus usually stains deeply , but the chromatin pattern can nearly alway 's be distinguished . 
29. - ( 2 ) spheroidal and 8pindle cell carcinonw . a field showing a group of cells similar tov but larger than , oat cells and a small bundle of spindle cells . 
34. - a clump of cells , the individual members of which have no definite characteristics of malignancy though one of the cells seems to possess large nucleoh - an appearance which may be due to the superimposition of pus cells . 
at one time , clumps of this type were thought by the writer to be diagnostic of carcinoma , but a clump of rather similar appearance led to a false positive diagnosis in a patient who was found at postmortem examination not to be suffering from carcinoma . for clumps of cells that are considered to be diagnostic of carcinoma , see fig . 
35. - a group of epithelial cells showing a considerable degree of pleomorphism and nuclear degeneration . this is the most confusing appearance that has been seen in the whole series . 
the cells resemble carcinoma cells closely , but in no case is the nucleus large . this field , and the three that follow , were from the sputum of a single patient , in whom a positive diagnosis was made as a ' result . 
41. - a clump of cells which appear to surround a vacuole from the sputum of a patient who , on the strength of this evidence , was thought by the writer to be suffering from bronchial carcinoma . 
eye hospital , southwark , london . received for publication december 15 , 1950 . in a previous communication ( barker , dhar and parsons , 1949 ) the effects on sarcoma growth in mice produced by treatment with some derivatives of purine and pyrimidine compounds were recorded . further experiments described below have extended the range of pyrimidine compounds studied , and an attempt has been made to correlate molecular structure with biological activity . 
the compounds employed fall into the forowing groups : ( 1 ) cytidyfic acid and alhed compounds . ( 2 ) barbituric acid , its imino derivatives and related compounds . ( 3 ) acyclic analogues of some of the above compounds . pure line or stock mice were grafted with the homologous c57 or the heterologous 837 or crocker sarcomas . 
the technique for treatment was similar to that previously described ( barakan , barker , guband and parsons , 1948 ) , the standard dose ( 0 - 025 g . ) being reclueed in proportion to the toxicity of the particular compound . 
table i summarizes the statistical analysis has shown that the differences in tumour results obtained . weights for treated and untreated grafted mice are significant for groups 2 , 10 , ii and 12 . 
cytosine and uracil , on the other hand , are not utilized in nucleic acid synthesis . this suggested that examination should be made of the action of cytosine when injected into grafted mice . 
the behaviour of 4 - aminouracil appears to be specifically associated with its chemical structure , since the introduction of the sulphur atom at position 2 to give 2 - thio - 4 - amino - 6oxypyrimidine is sufficient to abohsh its inhibitory action . it is considered possible that the marked difference in activity between 4 - aminouracil and 5aminouracil is due to the difference in the electron - availability at the free positions of the two molecules ( positions 4 and 5 respectively ) , which would influence the abihty of the tissues to metabohze the compounds by oxidation . since 4 - aminouracil may also be regarded in its tautomeric form as 4 - iminobarbituric acid , a systematic study was made of barbituric acid and its derivatives , all of which are characterized by high chemical reactivity at position 5 . 
parsons ( 3 ) the 8pecificity of the heterocyclic ring . in the above discussio ' n of the biological act ' ivity of the varl ' ous constituent groups in the pyrimidine derivati - ves the structures were considered only as part of the heterocychc system . in order to determi e whether the ring structure of the compounds is essential to the activities observed three acychc compounds in the first , carbamido - acetamidine , the whole of the structure have been tested . of 4 - aniinouracil is present except for the carbon atom at position 2 . in the second , acetyl urea , the configurations at positions 1 , 2 , 3 and 6 of 4 - aminouracil the third , acetamidine , possesses a similar grouping of atoms to are inaitated . that at position 4 of 4 - aminouracil . 
hall. from the cancer research laboratories of the new zealand branch of the british empire cancer campaign , medical school , university of otago , dunedin . received for publication january 1 , 1951 . kseveralmethods are available for studying the effect of prolonged stimu ( 1 ) repeated implanlation of the sex organs by gonadotropic hormones : tation of pituitaries obtained from castrates , ( 2 ) implantation of testis or ovary into the spleen of a castrated animal ( biskind and biskind , 1944 , 1945 ) and ( 3 ) parabiotic junction of a normal animal to a gonadectomized litter - mate . the first method is not very effective owing to the generally short survival of the grafted pituitaries . 
the ingenious method of the biskinds ( 1944 , 1945 ) , however , does not allow one to study how the increased hormonal output of the stimulated gonads affects the accessory sex organs , whereas in parabiotic animals this effect can be observed . 
we have fouiid in the literature only one reference to an investigation in which a similar experimental procedure has been used . strombeck and ekman ( 1949 ) fed a diet containing a.a.f. 
a breakdown of the junction is a rare event . operative mortality was practically nil , but in the second or third week after the operation a great number of pairs died due to incompatibility of the partners no pair sbowing signs of " parabiotic intoxication " survived longer than 5 weeks . the use of more closely inbred rats ( three generations of brother - sister mating ) did not lower the rate of mortality at this critical period . in most experiments acetylaminofluorene - vvas given by stomach tube to the normal partner , who received the carcinogen in doses of 4 mg . 
the treatment with the carcinogen was started 3 to 4 weeks after parabiosis had been established , when consistent gain in weight and the good condition of the animals showed that the operation had been successful . 
were given on 6 consecutive days by stomach tube and in another the carcinogen was given to the twins with their diet ( 4 mg . dailv to each rat for a period of 4 weeks )  . all the rats which received a.a.f. by stomach tube were fed the ordinary stock diet , consisting of meat meal , pollard , bran , maize meal , bone flour and whole wheat supplemented by cabbage . 
was administered with their food were kept for 4 w - eeks on a diet consisting of skimmed milk and whole meal flour supplemented by codliver oil and cabbage . subsequently they received the same food as the other pairs . the twins were killed when a tumour was suspected or when loss of weight indicated that they were in a precarious state of health . pituitary , testis , accessory sex organs , breast , suprarenal and liver of most pairs were studied histologically . 
the pituitaries were fixed in mercury - saline ( 6 per cent ) , the other organs in zenker or neutralized formol - saline . for staining of the pituitaries a modified papanicolau tecbnique was used ' the other organs were stained with ha , matoxylin - eosin or according to weigert - vail cxieson . the material presented consists of 20 r . , airs of parabiotic rats treated with a.a.f. 
the remaining 2 pairs consisted of litter - mates , none of which had been castrated . of the 6 pairs not treated with a.a.f. , 4 were combinations of a normal male joined to a castrated brother , while in the other 2 the male was joined to a spayed female . in addition , cc single " ' rats were treated with a.a.f. 
 - in a similar manner as the normal partners of parabiotic pairs . five young males received by stomach tube 15 doses of the carcinogen and to a group of 10 , 24 doses ofa.a.f. 
only benign lesions of the liver were seen when the animals were killed in the 52nd week of the experiment . in the group treated with 24 dosos malignant hepatomas were also found from the 37th week onwards . 
was seen in any of the rats joined to a partner to whom the carcinogen had been administered . these livers were macroscopically and histologically normal . in the pair of rats who had received a.a.f. 
the hyperplastic seminal vesicles contained macroscopically visible iiodules which were situated near the cephalad margin of the organ ; in addition a fifth neoplasm of microscopic size was found . in all 5 instances the fundamental histological change was the invasion of the muscular coat of the seminal vesicle by atypical glandular epithelium and therefore the lesion must be considered an adenocarcinoma . 
11 and 12 illustrate the appearance of the only tumour of the seminal vesicle found previously in our material . this large anaplastic carcinoma arose in a seminal vesicle of an albino rat of the " sheffield " strain which had received a diet containing a.a.f. 
and para - amino benzoic acid . in another case both seminal vesicles and prostates formed one large mass containing multiple cysts filled with yellowish creamy material . adhesions connected this mass with loops of the bowel . this - lesion was of inflammatory origin and no neoplastic changes were found in it although many sections were studied . as already mentioned not a single neoplastic lesion was found in the castrates joined to brothers treated with a.a.f. in the pair where both received the carcinogen with their food , the kidnev of the castrate showed a lesion of microscopic size which we have not found so far in rats treated with a.a.f. 
the whole picture resembled that of a benign tubular a4enoma of the kidney . morphological sign8 of increa8ed androgen secretion in the normal parabiotic male partner . the changes to be described were found in most cases and were i ' ndependent of the administration of a.a.f. 
the testes were frequently increased in size . their tubules were normal ; the leydig cers were large , having ample cytoplasm and in some animals their numbers h ' ad increased . 
the hyperplasia of prostate and in tlle latter the glandular part of seminal vesicle has already been mentioned . the organ was more stimulated than the outer mesenchyma ' l layer . this disproportionate growth led to compression of the epithehal folds lined by high cylindrical cells . 
the suprarenals of the intact partner differed histologically from those of the castrated twthe glomerulo 'sa of the former was denser and consisted mainly of cells the cytoplasm of which stained wen with eosin . however , thev - were not as frequent the fascicularis contained signet - ring cells . as in the example ifustrated by selye ( 1947 ) on p . 
133 of his text - book of endoin the castrate the glomerulosa was formed by large pale cells , the crinology . fascicularis was free of signet - ring cells and the reticularis was hyperaemic and better developed than in the normal twthe kidneys of the normal partner their surfa ' e was more granular and were larger than the ones of the castrate . histologically the tubular apparatus showed slight degenerative changes , the , connective tissue being more prominent , especially in the outer layer of the cortex . the pituitaries of the norma - i litter - mates were consistently smaher than in the castrates and were sometimes even ' below the weights normally found in our in these pituitaries the numbers of acidophils were increased rats of similar size . with a corresponding decrease in chromophobes . 
griesbach with faintl the periodate - feulgen technique , the cells gave a slight schiff reaction . this agglomeration of basophils was probably not a - permanent structure . zahler ( 1950 ) has described the appearance of nests of basophils in the pituitaries of rats treated with testosterone . the state of parabiosis did not seem to influence the growth of the rats , nor to increase their suseeptibihty tor a.a.f. in the two pairs where two normal males had been joined together , the animals treated with 24 doses of a.a.f. reached the same size as " single " rats , which had received the same dosage of the carcinogen . 
amounts as used in this investigation are administered . in this respect the carcinogen behaves like the steroid hormones which ass only from one to the other partner when extremely high concentrations are reached in the eirculat ' ion of one of them ( zeckwer , 1946 )  . the liver tumours obtained appeared after approximately the same interval as in " single " rats treated with similar amounts of a.a.f. metastases occurred in two instances , proving the malignant character of these hepatomas . 
although the hepatomatous liver was situated in the same peritoneal cavity as the hver of the untreated partner , the latter remained perfectly normal . there was not the slightest indication for an agent derived from the malignant hepatoma affecting the liver of the litter - mate . as mentioned in the introduction a constant flow of gonadotropins passes from the castrate to the normal partner stimulating its gonads . however , no tumours in this respect our experiments failed where of the testicles have been found . those of biskind and bisldnd ( 1945 ) and of twombly , meisel and stout ( 1949 ) these authors obtained tumours in testes which had been grafted succeeded . into the splee ' n . 
two further points should be considered . spermatogenesis is inhibited in testes situated in the abdomen and consequently the morphology of such gonads is considerably altered ; in additionil transplantation of a testis into the spleen involves traumatic injury . these two factors further studies seem are not present in the experimental procedure used by us . to be required to elucidate the conditions essential for tumour induction in the male gonad , a problem which has been recently reviewed by lipschutz ( 1950 )  . the androgens secreted by a testis transplanted into the spleen do not reach the general circulation and therefore the accessory sex organs of rats bearing such the normal parabiotic male joined to a gonadecgrafts are not stimulated . tomized litter - mate shows the effects of increased androgen secretion . in the pairs not treated with a.a.f. 
this stimulation did not lead to tumour formation in any of the target organs , but in the group treated with the carcinogen five tumours appeared in the seminal vesicles of normal partners . 
we have never found this type of tumour occurring spontaneously in the new zealand strain , nor have we seen it in " single " rats only once a carcinoma of the seminal vesicle was observed treated with a.a.f. in an albino rat of the " sheffield " strain treated with a.a.f. our combined material represents the post - mortem findings of nearly a thousand male rats treated with a.a.f. in the rat spontaneous tumours of the seminal vesicle are extremely rare and we have found in the literature only the case reported by flexner and jobling ( 1907 )  . in men , tumours of this organ are also of very lazarus ( 1946 ) has critically reviewed the cases reported , infrequent occurrence . and since then only a few additional observations have been recorded ( mccree , ] 1948 ; gee , 1948 )  . in the case of the thyroid , the carcinogenic action of a.a.f. 
the liyperplasia induced by increased amounts of androgens secreted by the stimulated testis enhances tlle susceptibflity of the seminal vesicle to the carcinogenic action of ' a.a.f. the ' fact that tumours of macroscopic size were found only in rats treated with 24 or more doses of 4 mg . 
and not in animals receiving less suggests that considerably more of the carcinogen is required to bring about tumour development in the stimulated seminal vesicle than was needed for the induction of adenomata in the hyperplastic thyroid ( hall , 1948 )  . that only one minute tumour of the seminal vesicle was found in an intact male joined to a spayed female is probably due to the lower dosage of a.a.f. given to this group and not to the nature of the gonadotropins of the spayed female . only 17 to 20 doses of the carcinogen were administered because great difficulties were encountered in keeping alive pairs of opposite sex for periods necessary for tumour development . however , our material is not large enough to decide this question . to summarize , we consider the tumours of the seminal vesicle to be due to a hormonal imbalance created by gonadotropins in the normal partner . these hormones , by stimulating the gonads of the ' normal partner , increase the androgen production of its testes and therefore are responsible for the hyperplasia of the although unable to promote tumour growth in the testes they , seminal vesicles . bring about conditions in which an accessory sex organ becomes susceptible to the . 
the possibility cannot be excluded that stin more prolonged androgenic stimulation may ultimately bring about tumour formation in the seminal vesicle without the aid of a.a.f. addend - um ( received for publication february 7 , 1951 )  . after the above paper had been submitted an additional pair of parabiotic rats had to be sacrificed . in this pair a normal male was joined in parabiosis to a castrate , the former having received 20 doses of a.a.f. 
left seminal vesicle with loops of small intestine and a hard small nodule was found embedded in these adhesions at approximately 3 mdistance from the upper margin of the fig . 
in normal male rats joined in parabiosis neoplasms were only to castrated or spayed litter - mates have been described . obtained in animals receiving the carcinogen and never in their untreated littermates . ( 2 ) benign or malignant tumours of the liver were found depending on the amounts of the carcinogen given and on the duration of the experiment . 
the mahgnant hepatomas metastasized to the lungs of the animal bearing the cancer of the liver , but never " infected " the other partner . these neoplasms are considered to be due to two factors ; tlle carcinogenic action of a.a.f. 
agents with therapeutic possibilities such as radio - phosphorus and the radio - iodines , and probably much better , suitable organic compounds containing radio - active isotopes , whose action depends on selective concentration of the radio - activity in particular cells . the separation on the industrial scale of non - radio - active isotopes and the practical development of the mass spectrometer open new possibilities of isotopic tracer research where radio - active effects are undesirable , as in many clinical investigations , or where , as in the case of nitrogen and oxygen , no suitable radioactive isotopes exist . the cyclotron still remains an essential instrument both for the production of small amounts of certain isotopes and as a source of fast neutrons for therait is by no means certain that the peutic trials in cancer and related diseases . frequency modulated cyclotron will be useful as a therapeutic source of fast j . 
mitchell neutrons , on account of the possibility of reduced neutron output and of the undesirability of a pulsed output . a promising field for radiotherapeutic investigation appears to be the study of high energy , 20 - 50 mev . 
prove more suitable than the synchrotron . the electron beam can now be extracted from these machines , the therapeutic possibilities of the high energy beta particles are rather uncertain and must be investigated with caution . the development of high energy generators opens the interesting possibility of the radiotherapeutic application of fast protons of energy in the region of 140 mev . 
 ( wilson , 1946 )  . the results of selected investigations are best summarized in the discussion of these newer agents . properties and production of isotopes , radio - active and stable . the properties of selected isotopes of especial interest are summarized in recent information on isotopes , which may be useful as radio - active table i . tracers , and which are produced in the pile , is summarized in table ii . 
a list of recent references on isotopes is also given . the pile is without a rival for producing isotopes in the very large number of cases where , during irradiation in the pile , a simple slow neutron capture process occurs , e.g. 
and for s35 10 millicuries per g . there is one slow neutron ( np ) reaction of especial importance : n14 + it is of interest that this process is probably responsible for n - > c14 + p . 50 - 80 per cent of the biological effects of thermal neutrons , the remainder of the effects being due almost entirely to the n - y reaction in hydrogen ( mitchell , however , the n , p reaction in nitrogen is of extreme importance for 1947 )  . isotopic tracer research as the basis for the preparation of c14 , the long - lived it has been shown by yankwich , rollefson and radio - active isotope of carbon . norris ( 1946 ) that the c14 is produced by slow neutron irradiation of compounds such as ammonium nitrate and urea in the form of very simple compounds such as c02 , co , ch3oh , h.cooih , and of especial importance as a starting - point for organic syntheses , hcn . in addition to the preparation of materials by direct irradiation , a very considerable number of radio - active isotopes are found as fission products in the uranium rods in a pile . 
a most valuable detailed list of these has been given by the plutonium project ( 1946 )  . in general , for the preparation of isotopes the yields with the cyclotron are very much smaller than those with the pile . 
the oxygen isotopes have been concentrated by distillation of water and by exchange reactions . sulphur has been separated by chemical exchange between so2 and the bisulphite ion . potassium has been also separated by chemical exchange methods . the development of the mass - spectrometer as a practical instrument and its routine use for hydrocarbon analyses by industrial laboratories in u.s.a. show clearly the possibility in medicine and biology of non - radio - active isotopic tracer investigations . 
an interesting possible diagnostic application of measurements of p32 in breast tumours in situ has been reported by low - beer , bell , mccorkle , stone , steinbach and hill ( 1946 )  . * the application of p32 as a tracer in metabolic investigations exemplifies the in order to avoid short - term problems raised by this method of investigation . effects , it is essential to calculate the dose of radiation received by the tissues for example , with p32 , one microcurie per g . from the radio - active isotope . * one line of metabolic tracer investigation insufficiently well known is the use of radio - active brominated compounds , e.g. 
of animal with times of observation of the order of 6 hours . of especial interest is the work of abels , kenney , craver , marinelli and rhoads ( 1941 ) , who accidentally found significant metabolic changes in the leucocytes in chronic leukaemias after total body x - radiation with doses as small as 3 r . , as a result of the radiation given by sub - therapeutic doses of p32 . of much greater importance in the clinical applications of isotopic tracer research is the avoidance of all possible risk of carcinogenesis as a long - term in a recent report on the result of the radio - active material introduced . " health protection activities of the plutonium project , " robert s . 
stone ( 1946 ) states that " it is now well established that ( radio ) strontium given to mice and rats in amounts insufficient to kill them for many months can cause bone and lymphatic tissue tumours to develop in significant numbers of animals . over long periods of time , plutonium has been shown to cause atrophy of the bone and bone sarcomas . " it is evident that great caution is necessary however , before introducing any radio - active materials into human subjects . it is likely that for many isotopes safe conditions for tracer work will be established after dosimetric studies and prolonged animal experiments . 
mayneord ( march 1 , 1946 - unpublished ) that the dose rate at 1 cfrom a point source of 1 millicurie of co60 enclosed in a platinum envelope of thickness 0 5 mis 11 - 1 r . 
however , it may prove more convenient to measure co60 sources in terms of equivalent radium . the production of large amounts of these isotopes by means of the pile raises the practical possibility of the therapeutic application of large gamma ray sources - " mass radiation units " equivalent to 50 - 100 g . 
mitchell in the form of na2hpo4 solution soaked in blotting - paper and dried . in addition to therapeutic applications , these beta - ray sources may be useful in experimental cancer research , e.g. 
stone ( 1946 ) states that " it has been established that single large doses of beta rays and multiple small doses can cause cancers in the skin without the animal being killed by the effect of the beta rays . " therapeutic possibilities of selectively concentrated radio - active agents . radio - active isotope therapy has as yet been limited to inorganic compounds . radio - phosphorus ( p32 ) , and to a much smaller extent the radio - iodines ( 1130 andi1131 ) , are the only isotopes with which limited clinical trials appear justified without further preliminary animal experiments . in general it seems unlikely that inorganic radio - active isotope therapy will stand the test of time . it seems much more hopeful to study the selective concentration by malignant cells of suitable organic compounds carrying radio - active isotopes of many elements ( rhoads , 1946 )  . the usual therapeutic applications of p32 in the form of na2hpo4 appear to depend upon its synthesis into nucleic acids by the multiplying cells . one other method of therapeutic application ofp32 reported ( jones , wrobel and lyons , see low - beer , lawrence and stone , 1942 ) depends on the selective concentration of colloidal anhydrous chromic phosphate by the cells of the reticulo - endothelial system . it is easy to understand the concentration of the radio - iodines by the thyroid in hyperthyroidism and in the rare cases of carcinoma of the thyroid , where the primary and sometimes also the metastases retain the function of secretion . 
one must be sceptical of the therapeutic possibilities in bone sarcoma of sr89 or ca45 ; it is interesting to note that stone ( 1946 ) reports that radio " strontium , barium , zirconium , yttrium and others locate quite selectively in the bones , and many of them stay for long periods of time . " radio - phosphorus , p32 , has been used since 1936 mainly in u.s.a. , in the treatment of patients with chronic myeloid and lymphatic leukaemia , polycythemia vera , lymphosarcoma and various related ( low - beer , lawrence and stone , 1942 ; reinhard , moore , bierbaum , kenney , 1942 ; lindgren ( 1944 ) showed thatp32 , which is selectively moore and kamen , 1946 )  . concentrated , gave better results than na24 , which is not selectively concentrated . the therapeutic possibilities and dosage of radio - phosphorus has been reviewed recently ( mitchell , 1947b )  . it is considered that the present position with regard to its therapeutic applications may be summarized as follows : diseases 1 . 
in the treatment of chronic myeloid and chronic lymphatic leukaemia , p32 is probably as satisfactory as , but no better than x - radiait is important to investigate the possibility of development of tion . methods of routine treatment of these diseases by means ofp32 . the average , each case is likely to require 10 to 15 millicuries ofp32 given , preferably intravenously , in the form of a solution of na2hpo4 in fractions in an over - all time of 10 - 12 weeks . it is desirable to correlate the dose with roentgen units ( marinelli , 1942 ) , and to measure the differential absorption ratio in different tissues ( kenney , marinelli and woodard , 1941 )  . 
3. given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . since 1944 we have taken a detailed family history from all patients reporting with carcinoma of the breast . 
we have 459 family records up to the end of 1947 which are reasonably complete . so far we have not succeeded in supplementing these histories , taken at the time of first visit to hospital , by later questions to the surviving patients or by arranging visits to their homes or relations . 
some attempt has been made to confirm the causes of death of relatives by letters to hospitals , doctors and the registrar - general 's department , but such confirmation has , as yet , been obtained in only a few cases . our figures , therefore , contain all those errors of inadequate information and faulty recollection that one would expect from data collected . 
many people die of cancer without their relations knowing that this was the cause of death . it is in fact surprising how successful a woman can be in concealing a cancer of the breast from her nearest relatives living in the same house with her . it is not , therefore , so surprising that more distant relatives , or even close relatives living away from home , may be unaware of the nature of the illness involved relations , even some of an older generation , who are still living at the time that the patient is first questioned may later develop malignant disease . 
many patients with cancer of the breast survive for long periods following treatment , and may ultimately die from some other cause ; we are , however , unable to include patients living who either have , or have had , cancer in our figures for comparison with expected incidence in the general population because no adequate morbidity statistics are available . in our series , for instance , there are the same number of sisters alive following treatment for cancer of the breast as there are sisters who died of the disease . ' comparisons must be made on a basis of mor164 d . 
3 shows a family where the mother of the patient died of cancer of the uterus aged 67 - she had two sisters , one who died of " internal cancer , " and one 166 d . 
smithers this sister had a daughter of cancer of the breast ' the latter aged about 60 . who had her breast amputated for cancer aged 45 , and who died aged 60 of lymphatic leukaemia . 
we find no evidence that cancer of the breast tends to develop earlier in patients whose relations are known to have suffered from the disease . the greater part of the work presented in this paper was done by p . rigby - jones and h . 
hartley , whose valuable assistance made this contribution to the symposium possible . i am also indebted to my colleagues on the staff of the royal cancer hospital whose patients were interrogated during this investigation , and particutlarly to r . 
the centrifugary - cleared extract was adjusted to i per cent with 20 per cent saline and the crude mucoprotein , etc . , precipitated by addition of two volumes of alcohol . 
the washed deposit was redissolved in 1 per cent saline , adjusted to ph 7 - 5 , and digested for 24 hours at room temperature with commercial trypsthe mixture was then filtered with the aid of hyflo super - cel and reprecipitated with 2 volumes of alcohol . 
the yield of protein - free , crude polysaccharide was about 2 per cent of the acetone - dried tumour tissue . the material contained polysaccharide and pentosenucleic acid , and the analytical data were : nitrogen ( kjeldahl ) varying between 5 - 2 and 6 - 3 per cent ; phosphorus ( fiske and subbarow ) 1 - 7 to 1 - 8 per cent ; and sulphur ( paulson ) 0 - 6 per cent . 
the ninhydrin reaction was negative . metachromatic sta ' m ' mg with azure a ( sylv6n and malmgren , 1952 ) revealed the presence of one orthochromatic component and another presenting alcohol - resistant metachromatic precipitates . 
d was also degraded by testis hyaluronidase at a similar rate to other such hyaluronates . glucose ( glucosamine ) could be demonstrated by following acid hvdrolvsis onl paper electrophoresis in borate buffer ( consden and stanier , 1952 )  . in addition , infra - red spectral measurements kindly performed by s . 
the two spectra were identical in the region 680 - 980 cm . - ' , showing the two materials to have the same molecular skeleton ( orr , 1954 )  . 
the only difference lay in the relative intensities of the bands due to the acid and amide carbonyl groups . however , the acid : amide ratio in sample d cannot be more than 5 per cent greater than that in the purified umbilical hyaluronate . nature of the_8uiphur - containing material . the metachromatic precipitate formed by azure a treatment of sample b was almost insoluble and further information about its composition could not be obtained . 
attempts were therefore made to remove the nucleic acid and the hyaluronate from the starting material by successive ribonuclease and hyaluroafter removal of the hydrolysis products by dialysis it was nidase treatments . thought possible to obtain the s - bearing material in a purified and soluble state . however , this latter material exhibited a powerful inhibitory effect on hyaluroin one experiment , when 30 mg . 
the s content of the remaining non - digested material was 0 - 49 per in the course of this long digestion , however , a small precipitate was cent . formed , which had a n content of 10 - 0 per cent and s content of 4 - 8 per cent . these figures suggested that a new product had been formed between the protein hyaluronidase and a s - containing polysaccharide . if the polysaccharide is assumed to contain 3 per cent nitrogen , the nitrogen value of the precipitate would fit a protein content of about 55 per cent , and hence a polybaccharide content of about 45 per cent . 
the intermediate protein - free material ( sample a ) contained about 70 per cent hyaluronate , 25 per cent nucleic acid , and about 5 per cent of a sulphur - be ' aring polysaccharide presenting some biological characteristics of heparthe largest part of the polysaccharide material present is thus beyond doubt hyaluronic acid with identical molar characteristics with that obtained from mammahan sources . 
the rous hyaluronate has probably a lower particle size than the hyaluronate from normal tissues , and the high viscosity of the intercellular rous material seems partly due to the protein components . the identification of heparin in the sulphur - bearing polysaccharide has not been fury established . 
a single male introduced the ay gene into all three lines , and the yellow mice in the offspring were crossed again to the respective pure line , and this process carried on indefinitely . 
were he responsible , he would have had to be heterozygous for these 7 genes in addition to his own ayat make - up , which would be rather an admirable genetic achievement , even if deliberately attempted . ( 3 ) contamination by stray mice : the whole experiment was carried out in a small room of the mousery , in which only this " yellow experiment " and inbred mice are maintained . 
none of the mutants was of this type , but all of the contamination by strays does not therefore appear to be usual " inbred " size . a satisfactory explanation , and true genetic mutation . 
though considerable discussion has been given to the question of mutations produced by atomic bomb explosions , it is possible that a much more frequent cause of these disturbances may have been unsuspectedly in action for many years on persons exposed to the influences of carcinogenic hydrocarbons . while mutations analogous to some described in this paper , e.g. 
reduction of hair and eye pigments , may be unimportant in humans , other types of mutants , some not detectable by the hydrocephalus , found methods used , would be a serious factor in public health . in this work , certainly would be . dominant lethals , leading to sterility or miscarriages , may also be produced , unimportant in mice where a large litter size is found , but of serious concern in man . it is possible that some mutants , such as the brain hernia found as an embryo , would normally be missed by the scheme used above , as mice usually eat abnormal and inviable young . the same unconcerned and easy solution of such difficulties is not the case in humans . there are possible also dominant mutations , which would appear in the first generation . though none was found in the series above , several were reported by strong it is obviously desirable that this additional ( 1945 ) using methylcholanthrene . hazard of exposure to these carcinogens should be evaluated . that this need is urgent is also suggested by the following line of argument : radiation mutations are almost entirely random , i.e. 
if a certain gene is mutated by an ionization in one sperm , the chance that the same gene will mutate in another sperm in the same or another individual is not increased . 
the efficiency of but this is not mutation with regard to any given gene is thus almost zero . if a chemical distributed via the blood necessarily the case with chemicals . stream reacts with a given locus to produce a mutation in one sperm , it is bbviously liable to do the same with all other similar loci in other sperms ( or ova )  . 
an efficiency of mutation at a given locus at 100 per cent can thus be imagined , and then all offspring of an exposed individual will carry the abnormal gene . a mating of any two exposed individuals would then give all f1 of the mutated type , a state which does not arise until the f4 of close inbreeding with radiation156 j . 
they could therefore have a high efficiency at certain loci resulting in a high frequency of abnormal offspring without causing death of the cell , as happens when concentrated doses of irradiation are given to increase mutation rate . combination with genetic material is thus likely . it is obviously tempting to ascribe the ability of the carcinogenic hydrocarbons to produce mutations to their complex system of conjugated double bonds . this system would readily pick up energy from the surroundings , and liberate it with destructive effect at one point . 
the hydrocarbons are possibly even less energetic , and thus may only be able to produce mutations in genes that are of less stability than most . this would produce some degree of specificity as required above , and it is significant that most of the mutations produced both here and by strong are already known , i.e. 
no sarcomata were found , however , and the local trauma to the squamous epithelium of the crop apparently favoured the local action of the oily solution of carcinogen . further experiments designed to assess the possible action of 2 - aaf in arachis oil eneysted in the submucous tissues of the crop have been in progress for about 4 years , so far with negative results . 
of 2 - aaf was injected repeatedly into the crop of each bird . sixteen white leghom cockerels of our inbred flock , aged 5 months at the start of the experiment were injected twice weekly for 4 months , then once weekly for a further year , and then at less frequent intervals , determined by their gene ' ral state of health . they were kept on open grass range with access to unheated fowl houses and fed twice daily with commercial poultry mash and pehets . 
no foreign body was present in the ulcer or underlying tissues . halfway along the oesophagus between the buccal ulcer and the crop , a small pedunculated translucent polyp 3 min diameter projected from the posterior wall . 
both kidneys were very mottled with white spots and small retention cysts ; the left kidney also contained a firm white tumour pressing on the sacral plexus ( cause of paralysis )  . 
3412. this bird had repeated i ' ections of a 0 - 5 per cent solution of methylcholanthrene ( mc ) in arachis oil into the wan of the crop with a total dose of 30 mg . 
for 3 months past it had had a palpable tumour in the neck and this had grow - n to a mass about 10 cin diameter when the bird was kined . 
a biopsy taken when the tumour was first noted showed a solid cehular tu ' mour with little differentiation and with a dehcate stroma with little or no intercellular substance . 
the tumour was considered to be an anaplastic carcinoma . cell suspensions from biopsy material were injected into 12 birds with negative results . material taken post - mortem showed a fleshy , spindle - cened tumour very similar histologicary to the chemically - induced sarcomata that are the usual response in fowls to injections of carcinogenic hydrocarbons . grafts of fresh tumour tissue were made into 13 birds with negative results . these 2 tumours contrast with those induced with 2 - aaf in which the diagnosis of carcinoma was in no doubt . n : n - dimethylamino8tilbene ( dmas )  . - as this siibstance has been shown by haddow and his co - workers to be a versatile carcinogen for rats it was thought that it might also prove an epitheliotropic carcinogen for the fowl . thirteen white leghorn cocks aged about 5 months were injected periodically into the pectoral muscles with 0 - 4 per cent solution of dmas in arachis oil with a total dose of from 0 - 5 g . 
to 0 - 8 g . these birds died or were killed between 78 and 208 weeks from the start of the experiment but no tumours were observed in any organ . 
the present experiment shows that 2 - aaf is similarly active against a variety of epithelial tissues ih the fowl and confirms the earlier report by bielschowsky and green ( 1945 ) that it is carcinogenic for the kidney of this species . in contrast with 2 - aaf , n : n - dimethylaminostilbene , which is also a versatile carcinogen for rats ( haddow and kon , 1947 ) , caused no tumours in fowls in our experiments . thus it seems that the epithehal tissues of the fowl are much more resistant to the action of many carcinogenic hydrocarbons than are those of rodents . however , monkeys also seem to be relatively resistant to the action of carcinogenic hydrocarbons ( pfeiffer and allen , 1948 ) , and it may be that we should rather regard the small rodents as being unusually susceptible to these agents . it is unfortunate that all attempts to transmit the 2 - aaf induced carcinomata have failed so far . 
the technique for painting with the 03 per cent benzpyrene solution in - acetone was that described by calcutt and powell ( 1947 ) , and further treatment was as in earlier work ( weigert , calcutt and powell , 1946 )  . extraction and estimations of the metabolites were by the methods of weigert ( 1948 )  . the nutrient media used were as below : 1 . 
for a period of 8 hours . metabolism of the benzpyrene only occurred in the series on the four buffered in the case of the tap water and the normal saline the media were found media . to be turbid and the skins sodden and waterlogged . 
on the other hand , the variation in explanations of this based on the yields obtained is in itself of some interest . the detailed composition of the media used appear to be of doubtful significance . the outstanding point seems to be the ph of the medium . under the conditions of experiment it is reasonable to assume that the tissues of the skins concemed became adjusted in some degree to the environmental conditions , that is , that the internal state of the cells approximated more nearly to the external ph than would normally be the case . 
the question arises , therefore , as to whether such a state of affairs could influence the metabolic turnover . taking advantage of some recent findings , it is believed that an explanation of the results can be offered along the above lines . it has long been suspected that the process of carcinogenesis is intimately involved with sulphydryl groups . this view has recently been reinforced by crabtree ( 1948 ) , and the weight of evidence is now strongly in its favour . 
at the same time it has been suggested that the metabolism of benzpyrene is also mediated by - sh groups . this has received confirmation by the findings of 432 a . 
nordling. received for publication december 29 , 1952 . recent research in genetics and pathology has shown an amazing consistency between the agents causing mutations and those causing - or contributing to the one of the more prominent theories , which since the development of - cancer . 1920 's has been advocated by bauer ( 1949 ) , strong ( 1949 ) and others , claims that the original cancerous cell is nothing but an ordinary cell affected by genetic mutation of some kind . 
one of the main objections to this theory has been that it does not explain the age variation of the cancer frequency . in reply , bauer ( 1949 ) contends that the mutated cells apparently remain latent during a long period until the new qualities become evident and the phenomenon can be diagbauer has found this period of latency to average 9 years for nosed as cancer . x - ray cancer , 12 years for paraffin cancer , 18 years for aniline cancer and 40 years for seaman 's cancer ( caused by solar radiation )  . 
the early occurrence of sarcoma and of leukaemia , however , does not conform to the idea of a latent period . moreover , it appears somewhat unreasonable to suppose that the length of the latency period would depend upon whether the mutation is caused by sun - rays writh most forms of carcinoma , furthermore , the frequency at or by x - rays . different ages is such that wre are compelled to consider average latency periods of 70 years or more , in order to explain the actual age frequency curve of cancer these facts still make it difficult for many of the most commortality in man . petent authorities in the field to accept the mutation theory without reservations . dahlberg ( 1943 ) has advanced a completely different explanation concerning the relationship between age and cancer . 
he expressed the opinion that malignant tumours develop increasingly easily with rising age . this implies that , for the development of tumourous cells , it is necessary for a certain number of cellular divisions to have taken place , between each of which there has been a certain period of time . all experience concerning the cancerous influence of chronic irritations promoting cellular divisions seems strongly to support this theory . 
the number of mutations required for experimental cancer in mice may be less , as suggested by the investiobviously , we need not assume that any gations of iversen and arley ( 1950 )  . only mutations which increase the ratio seven mutations will cause cancer . between cellular divisions and cellular loss in a positive direction in the environaccording to fischer ment in question may be expected to have this effect . ( 1930 ) , the short average life - span of cancerous cells is their dominant feature , and that by which all their other qualities can be explained . their rapid propagation , which exceeds their high death - rate , their ability to ferment sugar on a large scale and to disintegrate heterogeneous proteins , constitute normal cellular responses to a high mortality among adjacent cells . it may be added that the frequent variability in the number of chromosomes among cells from the same tumour is also a " normal " feature in the sense that the same phenomenon also occurs in certain normal tissues , as shown by therman and timonen ( 1951 )  . thus , some or most of the mutations required to start an incessant self - stimulating propagation among a group of cells might consist of any of the forms of mutation that weaken the cell , and make it more liable to die from even minor disturbances . if cancer were caused by one mutation only , it might be expected to be equally common among persons of different ages after an age corresponding to the length of the latency period , if this period were interpreted as the time required by the first cancerous cell to multiply in such degree as to be diagnosed as cancer . 
nordling prevails in countries with a high percentage of deaths due to " senility " , " other and unknown causes " and the like , whereas the latter is the case in countries e.g. , the united states , new zealand , with detailed and reliable statistics , australia , great britain and other western european countries . it can be shown , as by nordling ( 1952 ) , that the cancer frequency curve of a population with undependable vital statistics will be restored to the same shape as that of the populations with accurate statistics if , as a rule , about one - fourth of the deaths due to such causes as " senility " are added to the registered cancer deaths . united states white population 1940 united kingdom 1939 france 1947 norway 1941 - 1945 000o = + = : + 14 at = ___x___ 200l asla42w 2 i - = 3 ___ _ - - _ 40 60 80 50 70 60 80 50 70 60 80 50 70 40 60 8u 50 70 fig . 
1. - diagram drawn to double logarithmic ( log / log ) scale showing the cancer death - rate ( in the case of the united kingdom , the carcinoma death - rate ) in males at different ages . deaths per 100 , 000 males are shown on the vertical scale , age figures on the horizontal scale . however , the very highest age - groups , which are always numerically small this is and certainly highly selected , can hardly be taken into consideration . because these individuals are usually already very frail and likely to die from any trivial cause , irrespective of whether or not they have cancer in a more or less developed stage . thus , it seems probable that , in reality , the age - frequency relationship for cancer follows the same general rule everywhere in the civilized world , although in these reliable examples can be given in only a limited number of cases . cases it is obvious , as is shown in fig . 
with regard to cancer among females , it is necessary to distinguish between cancer in the specificially female organs , of which the increase is fairly small above the age of 45 , and cancer at other sites , of which the frequency seems to increase according to the sixth power of age both before and after the forties , but not during the decade of the menopause , when the increase is smaller . it seems possible that altered hormonal conditions in connection with the menopause might play a part in determining the actual cancer frequency curve obviously , more slowly operating hormonal variations might among women . be present in both men and women . 
it is therefore by no means certain that the entire increase in the incidence of cancer with age is to be explained by means of the multiple mutation mechanism . it is possible that a small proportion of the increase is due to a lesser degree of hormonal inhibition of growth of potentially cancerous cells in an older organism than in a younger one . 
the writer is not , however , aware of any evidence definitely substantiating such a variability of natural cancer inhibition with age . during childhood and adolescence cancer is rare , but it occurs considerably in these cases it is more often than the sixth - power - of - age rule would allow . mainly a question of sarcoma , leukaemia and other non - epithelial forms of cancer . such a condition does not , however , imply any contradiction of the hypothesis since it is unlikely that mutaof successive mutations as the cause of cancer . genic noxae reach the bones and other internal tissues , it therefore seems more reasonable in the case of sarcoma to presume spontaneous mutations ( i.e. , mutations due to normal molecular collisions ) and radiation mutations as the such mutations may , of course , occur already in the foetal causative factor . in view of the extremely rapid growth during this period , it is not period . surprising that multiple mutations occasionally have time to occur , giving rise to infantile or even foetal sarcoma . 
the infrequency of malignant tumours in the striated muscles , despite their large volume , may have some connection with the fact that this kind of tissue is composed of multinuclear cells . according to the theory put forward in the present paper , cancer is caused by mutations multiplied and accumulated usually through large - scale proliferation it is easy to explain on this basis such facts as the ( sometimes inherited ) of cells . high susceptibility to cancer of certain organs , especially under experimental this is because every stimulant causing - or congenital capacity conditions . characterized by - a high proliferation rate also increases the number of mutated also the high susceptibility to cancer cells and thus the probability of cancer . of benign tumours is easy to understand in this way . the facts and theories advanced here demonstrate , among other matters , the importance of having reliable vital statistics in order to elucidate casual relationships in the pathogenesis of cancer . 
bielschowsky. from the hugh adam cancer research department of the , medical school and the , new zealand branch of the british empire cancer campaign , university of otago , dunedin . received for publication december 5 , 1953 . chromophmic tumours of the pituitary are more frequent in the rat than in man . 
thus chronic thyroxine deficiency can lead to the formation of basophihc adenomata and the morphological signs of hyperoestrinism are found often in conjunction with acidophilic adenomata . when the normal level of oestrogen in the body of the female rat is raised for prolonged periods , vagina , uterus and mammary glands undergo a series of changes one of which is cystic hyperplasia of the breast . 
growth had taken place mainly in direction of the cerebellum with which the tumour was in close contact without invading uterus ( 125 mg . ) and vagina were atrophic , it . 
the kidneys had a granulated surface and the adrenals were of a slightly darker colour than normally . large fat deposits were present in subcutaneous and retroperitoneal tissues , as well as in the abdomen . 
respectively , when killed after 10 months of parabiosis . smears taken from the spayed female indicated persistent anoestrous , whereas those of the intact littermate showed the picture of continuous oestrous . 
at the post mortem the pituitary of the intact parabiont ( rat 2 ) was found to be considerably enlarged ( 139 - 3 mg )  . nodular structures protruded above the surface which showed haemorrhagic discoloration . 
the ovaries were large and cystic , of a yerowish colour and apparently free of corpora lutea . there was after removal of the capsule fluid between the capsule and the ovarian tissue . the combined weight of the ovaries was 299 mg . 
the breast glands were remarkably hyperplastic and contained large milk cysts . in sections of the pituitary normal anterior lobe tissue was not recognisable and the presence of basophihc cells could not be demonstrated by any method . the cleft separating intermediate and anterior lobes was enlarged ' and filled with 156 f . 
the great majority of the tumour cells appeared to be larger than normal chromophobes or acidophils and most of them had a very prominent golgi apparatus the negative image of which was alreadv recogni 'sable at low power . 
the frequency of mitoses varied in different parts of the tumour , but rarely more than two were seen in one field at low magnification . blood - filled sinuses and areas of haemorrhage were present in all sections and so were strands of dense connective tissue , originating from the capsule or from larger blood vessels . 
the vagina was lined by layers of stratified , squamous , keratinising epithehuthe outstanding feature of the greatly hyperplastic mammary glands were cysts filled with eosinophilic material which apparently exercised pressure on the lining epithehum , flattening it . smaller cysts were surrounded by cuboid epithelium containing secretion droplets . 
the histological examination of the breast confirmed that the changes seen at autopsy were of a similar kind in both partners as far as their secretory activity was coneemed . to recapitulate , a remarkable secretory activity was found in the breast of the ovariectomised parabiont , the uterus and vagina of which showed the typical castration atrophy . in this case the stimulus responsible for " lactation " is oestrogenic stimulation can be assumed to have come from the intact partner . excluded because of the state of pituitary , vagina and uterus of the spayed animal . at the time this observation was published we were unable to explain whv such changes in the breast were seen only occasionally in spayedanimals joined in parabiosis to an intact female . revision of the material has shown that there exists a good parahelism between the presence of a pituitary tumour in the intact partner and stimulation of the breast of the ovariectomised parabiont . 
a fortnight later vaginal smears revealed the presence of cornified unfortunately cells which remained the predominant cell type for 13 months . no smears were taken during the following 3 months , but during the week preceding death the vaginal smears were those of anoestrous . 
ar other organs appeared normal except the lungs which contained small areas of consolidation . histological investigation showed that little non - neoplastic tissue remained in the pituitary . this consisted of chromophobes and acidophils of fairly normal appearance , but the presence of basophils could not be demonstrated in the compressed rim of normal anterior lobe . 
the tumour itself consisted of atypical large acidophils which in some regions were nearly as numerous as non - granulated cells , whereas in others the latter predominated . bizarre cells with giant nuclei were a common occurrence and one or more mitoses could be found in nearly an fields . 
the glands contained follicles in various stages of development groups of pale vacuolated cells , separated by with healthy appearing ova . strands of spindle - shaped elements predominated in the stroma . in frozen section the pale cells were found to contain ample sudanophilic material . 
of the target organs of the adenohypophysis only the breast glands were found to be stimulated and of the known pituitary hormones only prolactin can cause secretion in the breasts of ovariectomised adult rats ( desclin , 1952 )  . the functional activity of the pituitary tumours of the rat is at variance with that of the acidophilic adenomata of human pathology . 
two types of acidophils can be easily distinguished in the pituitaries of several species as for instance the rabbit ( friedgood and dawson , 1938 )  . here cells with a strong affinity for carmine are found besides others which do not retain this dye . 
the former increase in numbers after coitus , towards the end of pregnancy and during the first days of lactation . in man , romeis ( 1940 ) demonstrated the presence of one type of acidophils staining red , and of a second staining yerow in azan preparations , his a and e cefls . in addition he recognised a third variety of acidophils , the q or pregnancy cers of erdheiin the rat the histological methods with which the writer is familiar unfortunately do not allow differential staining of two types of acidophils . 
why in man the growth hormone producing cells undergo neoplastic changes and in rodents the prolactin secreting acidophils , i am unable to explain . the interrelation between pituitary tumours and secretory activity of the mammary glands has been studied by lacour ( 1950 ) in the rat . in a series of 37 oestrogen induced adenomata she found in 23 granulated as well as " chromophobic " cells with a hypertrophic golgi apparatus . 
whenever the granulated elements were present , the breast had the aspect of a " lactating " gland . used romeis ' kresazan technique which stained the granulated tumour cells according to lacour a few cells , having the same tinctorial qualities orange . occur in the pituitary of the normal female rat . 
they become more numerous early in pregnancy and increase considerably in numbers 3 days ante partum . from this date onwards until weaning these ora ' ngeophil acidophils outnumber the other type . 
the close correlation between the presence of orangeophilic cells in the normal and tumourous pituitary and lactation changes in the breast suggested to lacour that these elements were the sourc ' e of prolactin . the hterature on experimental and spontaneous pituitary adenomata in rodents has been recently reviewed by horning ( 1952 ) and by gardner ( 1953 )  . in contrast to the opinion of the writer , gardner considers the oestrogen induced pituitary tumours as chromophobic adenomata , a view still shared by most admittedly , degranulated elements are more numerous in many authorities . of these tumours than granulated forms , but can - one classify all cells without granula as chromophobes ? the difficulty lies in the morphological resemblance of degranulated acidophils to chromophobes . 
the oestrogen induced pituitary growths with functional activity cannot be chromophobic tumours because the acidophils and not the chromophobes are the source of lactogenic hormone . another point of controversy is the nature of these pituitary growths . 
they are considered by some authors to be true neoplasms and conditioned growths by others , because they have been seen to regress when stimulation ceased ( nelson , 1944 )  . 
the " spontaneous " tumour described in this paper did not differ histologically or functionary from the two oestrogen mduced growths . this adenoma certainly was not dependant on oestrogen since it showed no sign of regression 51 months after ovariectomy . 
one occurred in an ovariectomised rat , the second in an intact female joined in parabiosis to a spayed partner and the third in a female treated with stilboestrol , in which , however , the histology of the vagina indicated a very low oestrogen level at the end of the experiment . the pituitary growths were found in animals having secreting mammary 160 f . 
pullinger. from the imperial cancer research fund laboratories and the research department , the glasgow royal cancer hospital , glasgow , c.3. received foi publication february 7 , 1952 . the suggestion was previously made that nodular adenomatous hyperplasia in mammary glands of mice of the riii ( paris ) strain , and possibly others , might provide a more sensitive and an earlier indication of the action of bittner 's milk agent than do actual tumours . evidence obtained under experimental conditions of forced activation of the glandular response to combined influence of hormone and agent was givren in support of this suggestion . it seemed probable also that spontaneously occurring nodules as well as those forcibly stimulated would afford reliable evidence of the action of the agent . 
the validity of such evidence would depend upon complete absence of spontaneous adenomatous nodules in the same strain deprived of agent . in sublines of the riiix strain ( renamed riib in accordance with international usage ) , which had been freed from agent by cross - suckling , no nodules had been found in the mammae of young unmated females forcibly stimulated , but two hyperplastic nodules were seen in 2 out of 44 females of the old breeding stock ( pullinger , 1947 )  . 
a survey of the mammae of all old females was in progress and was continued and combined with experiment in an endeavour to find an answer . the same problem , the stimulus for hyperplastic nodules in the zb strain ( c3h cross - suckled to deprive it of milk influence ) , was investigated by huseby and bittner ( 1946 ) , who came to the conclusion that all three factors , namely the milk tumour influence , ovarian hormone and susceptibiltiy that are responsible for the development of heritable mammary tumours in mice are also necessary for the development of these alveolar hyperplasias . 
the same authors gave an account of the morphology of nodules found in the mammae of mice in former high cancer strains and their hybrids after deliberate exclusion of the agent by cross - suckling . the strains examined were c3h and a , designated zb and ax . they compared the nodules with those in high cancer strains described by previous authors before knowledge of the milk agent existed . in the course of the present survey of old rilib ( formerly riiix ) breeders similar types of nodule were seen with the exception focal acinar proliferations were often but of those described as inflammatory . the squamous - celled nodules found in old not invariably discretely lobular . riiib females have been described and their origins discussed ( pullinger , 1949 )  . in relation to the problem of the presence and action of the milk agent these squamous - celled proliferations are not relevant , for it is generally agreed that tumours due to bittner 's agent are characteristically acinar formations and that b . 
the actual average number of litters was 4 to 5 . breeders were then segregated to allow the mammae to involute , thereby permitting detection of nodular hyperplasia of various sorts . under these conditions involution is completed in this straleaving main and a few branch ducts with tapered ends and no acinar structures . 
hybrids of less than i month old . extracts were made by grinding the tumours with sterile sand and distilled water , spinning at 2000 r.p.in a hearson centrifuge for 10 minutes , removing the supernatant fluid and spinning this in an ecco centrifuge at approximately 8000 g . 
the mammae of as many as possible of the rijib mice injected with test tumours were examined in bulk - stained preparations . will be seen from tables ii and iii that the f.i. 
pullinger dilute brown strain and their hybrids which bore more than 3 litters had a higher incidence of mammary tumours than those with less . the parous riiib females attained this average with 4 to 5 litters . of mice injected with riii tumour extracts 13 out of 23 developed mammary tumours . the mammary glands of all 7 which were examined , out of the remaining 10 , contained multiple adenomatous nodules , one as many as 30 . 
thus nodule incidence was increased in the riiib test mice by injection with riii tumour extracts . nodule incidence was not increased in the rilib mice which had been inoculated with extracts of the 2 tumours undergoing test for the agent . 
of 20 mice in the two experiments which were available for examination , the mammae of 3 contained acinar nodules ( 15 per cent ) , 8 contained nodules of other types , and 11 ( 55 per cent ) were free of all nodules . these figures are near the normal incidence . nodules in hvbrids are not recorded because there was no basis for comparison . thus neither from tumour incidence nor from nodule incidence was there any evidence of the presence of bittner 's milk agent in the 2 test tumours . the validity of results of tests in which grafts are used as suspected source of agent rather than primary tumours may be questioned . 
the majority of authors have been able to detect the milk agent in extracts of grafts derived from tumours which were known to have contained it in the first instance . jmochowski ( 1949 ) , who reviewed the various reports , has himself obtained evidence of the presence of agent after 42 serial transplantations . 
on that occasion he used multiple injections , but both he and others have succeeded with single injections of graft extracts . in a total of 69 test mice in the two experiments here recorded , not one tumour arose . these results are in accord with those of other workers who have tested extracts of primary spontaneous mammary adenocarcinomas in othier agent - free strains ( andervont and dunn , 1950 ; heston , deringer , dunn and levillian , 1950 ; dmochowski , 1951 )  . 
 ( personal communication ) were typical adenocarcinomas . assessment of the value of adenomatous nodules as indicators of the action of the milk agent . a comparison of the spontaneous incidence of adenomatous nodules in various groups of riii and ritib mice is given in table iv . it will be seen that among virgin females of the riii strain multiple nodules were present in 100 per cent at 9 months old . 
the relative reduction in number of nodules at 13 months after ovariectomy at 9 months is probably due in part to the difficulty of making accurate counts when the effect of ovarian hormone is still to be seen . among young virgin females of the riiib strain deprived of milk agent no adenomatous or other mammary nodules were found . 
pullinger when these nodules are present in mammae of young females of this strain of less than 12 months old , whether virgin or parous , they appear to provide reliable evidence of the action of the agent . 
this conclusion is more certain if oestrogen has been excluded by ovariectomy several months prior to examination of the mammae . breeders of the riiib strain deprived of agent , of 12 months of age or more , developed 1 to 3 adenomatous nodules in the 10 nipple regions . since these nodules were not associated with agent in the tests recorded , it is clear that they do not invariably provide evidence of the presence of agent in old breeders . they may be due to some other unknown cause . multiple adenomatous nodules in old breeders of this substrain would nevertheless provide presumptive evidence , requiring confirmation , of the presence of the agent . thus for purposes of detection of agent by inoculating suspected substances into susceptible test mice and using the adenomatous nodule as evidence of the action of agent , only young rijib virgins or breeders under 12 months old would be suitable as test animals . that is to say , they would have to be killed and examined at about 9 to 11 months old when positive results could be expected and before the nodules of unknown origin begin to appear . only if counts of nodules were required would ovariectomy have to be done because the naturally occurring hormone under normal conditions does not cause a confusing degree of focal acinar proliferation . 
nodules of purely adenomatous hyperplasia were found in about 19 per cent of parous females of 1 year old and over of the rijib strain deprived of bittner 's milk agent . 
no evidence was found that the nodules or tumours in the mammae of old parous females of the cross - suckled riiib strain owed their persistence to ovarian hormone ; neither could their origin or persistence be attributed to the milk agent . 
ludford , director of the research department , and to the board of management of the mount vernon hospital , northwood , continuity of observation was maintained to the end of these experiments . to the generosity of p . 
malowan ( 1932 ) - also found blood changes of the same low order , though becher and herrmann ( 1932 ) stated that they were unable to find any significant change that could be attributed to the presence of the tumour . all the above workers used danielson 's modification of folin 's well - known colorimetric method for blood amino acids . 
2. these observations show that the growth of the transplantable carcinoma ' m 2146 is accompanied by an elevation in the blood ac - amino nitrogen . while the mean value in normal mice was 4 76 mg . 
the corresponding regression equation between these variables is : oc - amino nitrogen values = 0 - 1213 tumour percentage size + 5 - 63 . these changes in the level of the blood ac - amino nitrogen probably account for the increase in the blood non - protein nitrogen in tumour - bearing animals found by other authors ( greenstein , 1947 )  . blood ac - amino nitrogen in mice with regressing tumours . in about 10 per cent of the mice used in these experiments the tumour , after having grown and reached a definite size , regressed completely . it seemed of interest to estimate the blood amino acid concentrations in these animals . 
the animals consumed this food freely for the first two days , but seemed to lose appetite during the remainder of the experimental five - day period . the loss of weight , which had become severe by the fifth day , together with the blood ac - amino nitrogen values , are shown in table iv . with the introduction of the deficient diet there was a marked loss of weight in both groups of mice ; the tumours , however , continued to increase in size even at the expense of the host , which was clearly in negative nitrogen balance . 
per cent throughout most of the experiment seems to show that this represents the basal level for this group of substances , below which further in the tumour - bearing group , on the other hand , the concentrafall is resisted . tion of the ac - amino nitrogen fell rapidly to between 4 and 5 mg . 
the similarity of the fall to that found for the control group would seem to show that whatever metabolic change was responsible for the characteristically elevated blood oc - amino nitrogen level was independent of the state of alimentation , 100 m . 
there is little evidence that the free ac - amino acids are increased in tumorous animals , but observations on rats with a transplantable hepatoma have shown that the second fraction may on average be raised seven or eight fold ( winzler and burk , 1944 )  . 
the elevation continues almost unabated when the animals are placed on a diet wholly deficient in protein . it seems , therefore , that the increase in oc - amino nitrogen must be attributable to one or other of the following factors : a local increase in the production of amino acids or of polypeptides by the tumour itself , either through the degeneration of its cells or the hydrolysis of normal body proteins brought to it by the circulation ; or to some hepatic dysfunction that is present in tumour - bearing animals which interferes with the normal disposal of these substances , and thus permits them to accumulate in the blood . this latter possibility will be considered first . fujiwara ( 1929 ) , weil ( 1935 ) , greenstein , jenrette , mider and white ( 1941 ) , and el mehairy ( 1949 ) found little inhibition of liver arginase in tumorous animals . greenstein ( 1947 ) also noted no dimunition in cystine , desulphurase activity in the same organ . arginase and cystine desulphurase are two of the main liver enzymes concerned with the intermediary metabolism of amino acids , and the study of their behaviour provides valuable information upon disturbances in the hepatic enzyme pattern generally . robertson and kahler ( 1942 ) and lan ( 1944 ) have also failed to observe any decrease in the enzymic activity of livers in animals bearing tumours . 
tumours of less than 5 per cent of the total body weight were not accompanied by any significant change in the oc - amino nitrogen concentration in the blood . the tumour tissue itself is believed to be the source of extra a - amino nitrogen in the blood . i wish to record my indebtedness to professor g . 
kirby , research department , glasgow royal cancer hospital . received for publication march 4 , 1948 . althoulgh the claims of roffo ( 1938 , 1939a , 1939b , 1941 ) to have induced adenocarcinoma of the stomach in rats given orally fats or cholesterol which had been heated to 3500 c . 
for half - an - hour have not been confirmed ( beck and peacock , 1941 ; kirby , 1943 , 1944 , 1945 ; morris , larsen and lippincott , 1943 ) , the positive results obtained by other routes in mice by other workers make a good case for regarding the products of such pyrolyses as carcinogenic . thus beck ( 1941 ) found sarcomas in 2 of 12 mice at the site of injection of cottonseed oil , previously heated to 340 - 360 c . 
for 1 hour , and steiner , steele and koch ( 1943 ) reported sarcomas in 3 of 9 mice injected with sesame oil heated to 3500 c . these latter workers found no tumours in similar mice injected with cholesterol that had been heated to 2000 c . 
for half - an - hour , and another sarcoma in 1 of 9 mice surviving more than 340 days after subcutaneous injection with a residue left after removing dicholesteryl ether and a4cholestenone from cholesterol heated in the same way ; these tumours were closely associated with the sites of injection . negative results were obtained by these workers when mice were injected subcutaneously with cholesterol that had been heated to 4300 c . 
of the remaining 14 , 5 died or were killed between 400 and 500 days , 1 was killed at 533 days , 1 died and 2 were killed between 500 and 600 days and 3 were killed at 735 days . bronchiectatic abscesses were found in most animals surviving 400 days ; there was no other frequent lesion . 
the stomachs were all normal , save for that of a rat dying after 616 days which had the haemorrhagic erosions of the glandular zone commonly found in rats in a state of inanition . 
shortly after the paintings had been commenced , 0 5 per cent of croton oil was added to the benzene solution in the hope of speeding up or enhancing the action of any carcinogen present in the c.o.h. after 258 days ' experimentation , a 15 per cent benzene solution of c.o.h , containing 0 5 per cent croton oil , replaced the original 10 per cent solution ; 2 males and 5 females survived long enough to be treated with the stronger three other male mice were painted with the 10 per cent - solution solution . for 168 days and then with the 15 per cent solution . atrophic changes at the site of painting were seen in mice dying at 80 days after the beginning of the experiment , but even in 2 females painted 258 days with the 10 per cent solution and then 374 days with the 15 per cent solution , and surviving totals of 640 and 656 days respectively , no further lesion was found . fourteen mice showed fatty changes in the liver , sometimes with extensive necrosis , but no hyperplastic changes were seen in this organ . 
the first mouse to die survived 80 days after the first injection ; 2 others died before 100 days , 10 survived 100 to 200 days , 2 from 200 to 300 days , 2 from 300 to 400 days , 5 from 400 to 500 days , and 1 survived 518 days . a mild histiocytic reaction was seen around sites of injection , but no sign of fatty changes in the liver were rare , but in mice any tumour was ever found . dying at 126 , 130 and 384 days after the first injection there were leukemic changes involving the liver and spleen in the first , the liver in the second , and the liver , spleen , kidney and lungs in the third mouse . ( c ) cholesteryl linoleate ( heated ) in mice . linoleic acid was prepared from cottonseed oil ( organic syntheses , 1942 ) and converted to the acid chloride by refluxing with oxalyl chloride . purified cholesterol was heated with linoleyl chloride on the water - bath for 3 hours , and purified as for the oleate . 
in the left flank , 31 days after the injection in the other flank . eight mice survived 100 to 200 days after the first injection , 1 for 247 days , 1 for 357 days , 2 for 470 days , 1 for 509 days , 1 for 558 days and 1 for 653 days . at the site of injection nothing beyond a mild histiocytic reaction was found in any mouse . 
and the time was 2 hours . as the esters were prepared by a non - pyrolytic method and were subsequently purified till non - fluorescent , any polycyclic hydrocarbon present in the residue after heating would have arisen as a direct result of the heating . 
no chemical experiments have been made to determine the nature of the components of the but the biological tests reported here gave no evidence of carcinoresidue . genicity in these residues for the skin or subcutaneous tissues of stock mice . such tumours as did arise in the mice used were almost certainly spontaneous . damage to the liver and the spleen was frequent , and the occurrence of leukemic infiltration was significant and probably attributable to the injections . it now seems that cholesterol and its naturally occurring esters may not be an important source of carcinogens in heated food . 
the results of the experiments described in this paper lend no support to the results reported by beck , kirby and peacock ( 1945 ) , who administered cholesterol heated to 3000 c . 
for the same period , as recorded by those authors , also of the negative findings of steiner , steele and koch ( 1943 ) with cholesterol heated to 2000 and to 300 c . 
it is concluded from this work and from other reports in the literature that cholesterol and its esters heated to reasonable dfooking temperatures for a reasonable cooking period have not been proved to yield carcinogenic residues . the author is indebted to p . 
i. - cancer of the lung and of the larynx . males , england and wales , 1921 - 1951 . ascribed to lung cancer , for cancer of the larynx there has been little change over the past twenty years . the preceding papers in this series ( kennaway and kennaway , 1951 ; kennaway and waller , 1953 ) compared the incidence during the period 1946 - 1949 . 
kennaway cancer of the lung and larynx as shown by death certificates in four classes of area ( london , county boroughs , other urban ' districts , rural districts ) in england and wales . 
for a particular sub - division of the country expresses the mortality in that area as a percentage of that for the whole of england and wales , allowance being made for any differences in the age - distribution . 
given as an indication of the relative importance of the two causes of death ; these measures of mortality will not be used in this analysis . the most striking feature of table 11 is the behaviour of the figures for the female larynx as previously described . whereas for cancer of the lung the male and female figures show similar trends the corresponding figures for the larynx show no such similarity . 
the next step is to see whether the geographical or the urbanization factor is the more important ; this can be done by a study of table iv and fig . 
3 and table iv that urbanization is the predominating factor : in each region , the mortality due to lung cancer increases from the rural to the urban areas and although the same is true of the male larynx , when we look at the figures foi the female larynx we find the exact contrary ; in every case the highest mortahty is in the fural districts . 
the comparison is particularly striking when we look at the s.m.r.s for the county of london ( the most densely populat - ed of all our areas ) and then at those for the sparsely populated rural districts inv.i ' ales ancl the north . for the purposes of this comparison the differences between the c.m.r. 
we cannot say whether the extremely high figures for the female larynx in wales ( where the population at risk is in any case small ) are more than an extreme manifestation of the reverse urbanization gradient or whether they m , ight be due , for instance , to some ethnographical factor . further study of eancer of the lung . another feature that emerges from the diagram is , that for cancer of the lung the urbanization gradient is consistently steeper in the men thad . 
of 160 for the county of london . it would be interesting to make a similar analysis with the urban districts ( or better with the county boroughs and urban districts combined ) but the labour would be prohibitive . it may be mentioned in this connection that since 1950 the registrar general has adopted a more realistic classification , which wfll considerably simphfy the study of many problems . 
with its large dormitory areas , the male s.m.r.s for cancer of the lung are all higher than in the sparsely populated s.w. , wales ii and north il in females the absence of such a clear association is partly a reflexion of the lesser gradient already noticed for women and partly due to the larger sampling errors to which these s.m.r.s are subject ; on the other hand the remarkably low female s.m.r. 
a possible explanation is that there are two aetiological factors at work , the one positively correlated with urbanization ( a ) and the other negatively ( b )  . 
the mortahty ratio for the larynx ranged from 60 for males of class i to 143 for males of class v , but it is significant that married wo ' men showed no significant social class gradient , thus suggesting that the factors responsible for the excess of cancee of this site amongst unskflled males are directly associated with occupation . " on the other hand there was in 1931 no marked social gradient for cancer of the lung . what connection is there between the occupational factor and urbanization ? we cannot answef that question in the absence of mortality rates analysed by urbanization simultaneously with occupation . 
if the figures in table viii are representative , they may be said to show ( a ) cancer of the larynx is four times as common in men as in women ; in men , intrinsic cancers are nearly twice as common as extrinsic , whereas in women extrinsic are four times as common as intrinsic ; as a consequence of ( a ) and ( b ) , intrinsic cancers appear nearly thirteen times as often in men as in women * and the extrinsic twice as often in men as in women . the conventional inclusion of cancers of the retro - cricoid region among laryngeal tumours is very unfortunate . " the term ( cancer of the larynx ) should be restricted to the so - called ' intrinsic ' group of cancers . 
kennaway mouth , tongue , and pharynx , angular stomatitis , hypochromic anaemia , achlorhydria , splenomegaly , and spoon nails , in which carcinoma ofthe post - cricoid region this condition was first described independedtly by may develop in later years . paterson from cardiff ( 1919 ) and by brown kery from the westem infirmary , glasgow ( 1919 ) and has become know - n by the names of two latee investigators as the " plummer - vinson " syndrome . neitherpaterson ( 1919 , 1937 ) nor brown kelly ( 1919 , 1931 ) suggest , either in their earher or later papers , that this affectioin . is especiafly common in their own districts , though any such frequency would have this syndrome is of qu ' ite especial interest in cancer research assisted recognition . because the features present during the earlier years may indicate a precancerous metabolic state , which may be treated succes - sfury by improved feeding and administration of iron ( see for instance hare ' n , 1938 ; waldenstrom , 1938 , and elkelesg 1942 )  . 
the forowing section represents an attempt to collect the literature on the paterson - kery syndrome in relation to cancer ; no attempt has been made to introduce any uniformity into the anatomical classificatioin adopted by the various authors . ahlbom ( 1937 ) records , from the radiumhemmet , stockholm ( 1931 - 1936 ) , the incidence of carcinoma of the post - cricoid region . ( a ) cancers of the hypopharynx are more frequent in women , in whom also a mucb higher proportion ( 90 per cent ) of these tumours affect the post - cricoid area , than in men . 
was in der diiit der drmeren schwedischen bevblkerung fehlt , sind vor allem eisenhaltige vegetabilien , obst und fleisch . " bingham and logan ( 1953 ) say " the incidence of hypochromic anaemia in northern ireland is considerable and . 
these trends apply equally when the figures are analysed according to the separate regions , but there are differences between the regions , which may or may not be due to differences in degrees of urbanization undetected by the classiin particular the s.m.r.s for wales are very low for the fication we have used . lung and male larynx but very high for the female larynx . 
the literature upon the relation of the paterson - kelly syndrome to cancer , and upon possible dietetic and social factors in this condition , is summarized . we are greatly indebted to w . 
calcutt. from the department of cancer research , mount vernon hospital and the radium institute , northwood , middlesex . received for publication may 3 , 1952 . the staining of living tissues , either in vitro or in the form of freshly excised material , is a well recognised technique . normally it is restricted to the identification of specific morphologic entities such as mitochondria . attempts to determine intracellular biochemical features have been rather unsuccessful as far as living material is concerned , although successes have been achieved with fixed specimens . 
the availability of tetrazolium compounds now has rendered possible further attempts at the identification of intracellular sites of reduction . three compounds are generally available . in their normal state they form colourless solutions , but in the presence of suitable reducing groups they are converted to coloured formazans . 
orr. from the department of experimental pathology and cancer research , university of leeds . received for publication july 19 , 1947 . attention was drawn to the frequency of spontaneous tumours in the lungs of mice by tyzzer ( 1907 - 8 , 1909 ) , whose description of their histology has required but little amendment . 
a small group of stock mice was treated intranasally with 1 : 2 : 5 : 6 - dibenzanthracene in almond oil , but owing to intercurrent disease these had all died before adenomata were present in any except one . 
the present communication is based on the histological investigation of the lungs of a representative sample of these mice , together with the urethanetreated mice of the previous paper ( orr , 1947 ) , and a number of mice showing spontaneous pulmonary adenomata . 
the outline of the whole tumour is usually more or less circumscribed , though there is no definite capsule ; sometimes it is irregular , but the appearance is not that of true infiltration . 
the two types of tumour have also been noted by grady and stewart ( 1940 )  . occasionally , both types of structure have been seen in the same nodule , and there appear to be adequate grounds for regarding them as morphological variants of an identical process . it is not uncommon to find alveolar macrophages of the " dust cell " type in the adenomata . 
they are often so heavily loaded with carbon as to obscure all nuclear and cytoplasmic detail . less often other evidence of inflammation in the form of lymphocytic or leucocytic infiltration is seen . but in addition a very large number of lesions show appearances which make the impression inescapable that they are stages in the development of adenomata within inflammatory foci . this evidence is more striking where the tubulo - papillary structure is being evolved , in view of its highly characteristic and easily recognized pattern . 
the inflammatory changes resulting from urethane are relatively chronic , and take a considerable time to clear up on withdrawal of treatment . moreover , the proportionate share played by polymorphs in the reaction even in its early stages seemed smaller than average : it may be that urethane exerts some depressant effect on them , and thus necessitates greater activity by the so - called fixed tissues . the source of the epithelium in the tumours has not been determined with certainty . indeed , in many instances even the simple statement that it is epithelium involves a measure of assumption ; the most that can be said with 320 j . 
the actual existence in the fully developed lung of such a tissue is denied by many authorities , and some of those who claim to find it describe morphological appearances very different from those found in the tumour cells . if the alveolar epithelium is implicated , it can only be by reversion to the embryonic type , and if this occurs , such epithelium might owe its genesis , as it does in the embryo , to the bronchial epithelium . it appears to the present author that some workers have been inclined to regard as alveolar epithelium any lepidic tissue in the lung which could not be . 
shown directly to be bronchial in origin . the present results are therefore in agreement with those of magnus ( 1939 ) in respect of the tissue of origin , without accepting his view regarding the intrabronchial papillomata . 
orr does not suggest that it is malignant ; the rate of growth is slow once the characbut there can be little doubt that a malignant teristic size has been attained . " variant " occasionally turns up . the role of antecedent inflammation . slye , holmes and wells ( 1914 ) thought that adenomata arise from areas of lung tissue in which inflammatory hyperplasia has occurred . grady and stewart ( 1940 ) consider that they are not associated with inflammation . 
the present author 's observations have convinced him that these tumours invariably originate in foci of chronic collapse inflammation , which become invaded by bronrchial epithelium , and that it is the extent of the original inflammatory focus which this would explain the paradox of its determines that of the formed adenoma . comparatively rapid appearance and slow subsequent growth . 
ludford. from the laboratories of the imperial cancer research fund , london . received for publication january 30 , 1948 . in a review devoted to the discussion of colchicine as a possible chemotherapeutic agent for cancer ( ludford , 1945 ) , attention was directed to the dual action of this drug on tumours . it is the most potent of mitotic poisons , and as . 
at the time the experiment to be described was performed , sections exhibited large compact groups of carcinoma cells , surrounded by an abundant and highly cellular stroma , composed of enlarged and hyperchromatinic spindle - shaped and polymorphic cells , presenting the typical cytological appearance of sarcoma cells . 
an aqueous solution was employed in a concentration of 1 part in 10 , 000 of distilled water . this had been prepared six days previously , when it was maintained at the temperature of boiling water for ten minutes to reduce the possibility of infection , and was stored in the dark for use throughout the exp6risince the activity of colchicine is reduced by high temperatures and by ment . keeping , especially when exposed to light , the solution employed for this experiment was rather less potent than a freshly prepared solution . 
1 by comparing the size of the tumours of the controls and the treated mice on the 21st day . control 71141 211301 37 treated 7 14 3 43 10 01 234 fig . 
2. - regression of a sarcoma ( c ) in strong a strain mice after treatment with colchicine . such after the shortest possible interval consistent with survival of the mice . treatment is invariably accompanied by a high mortality . an experiment with a spindle - celled sarcoma in strong a mice demonstrates the possibility of completely inhibiting malignant growth . this sarcoma was one which originated by the sarcomatous transformation of the stroma of a mice into which it is transplanted do not usually survive mammary carcinoma . long , as it rapidly penetrates the skin and leads to considerable superficial ulceraof six young adults transplanted with this sarcoma three were treated tion . 11 and 20 days after transplantation . 
age. - since actively growing tissues are most sensitive to mitotic poisoning , it is to be expected that young animals would be more susceptible than older ones ries ( 1939 ) reported that a 42 - days - old mouse to the toxic action of the drug . will survive more than 17 times the dose of colchicine which is lethal to one 10 days old . the maximum inhibition of malignant growth occurs with the highest tolerated therefore , to obtain the greatest arrest of tumour growth it is doses of the drug . necessary to employ animals at the age when they are most resistant to the the best results general toxic action and the largest doses can be administered . old mice are less able to tolerate have been obtained with young adult mice . thus , 11 strong a mice varying in age from 18 months to 2 years the drug . and 12 young adults were each injected with 0 , 056 mg . 
3. - action of colchicine upon sarcoma 37 grown in strong a and c 57 strain mice . tumours in c 57 mice indicated by outline , tumours in a mice stippled . 
the size of the tumours in the c 57 mice is indicated it will be observed that in outline , and in the a mice by the stippled areas . actually there is little difference in the size of the tumours in the control animals . growth is slightly more rapid in the a mice , but there is a definite difference in the two strains of treated mice . 
a similar acquirement of tolerance by tumours to the haemorrhage - inducing action of bacterial polysaccharides has been reported by shear ( 1944 )  . application of the preceding results for obtaining the maximum " colchicinic effect . " discrepancies in the reports on the action of colchicine on neoplasms which have been published are explicable on the basis of the preceding findings . 
of colchicine over a period of 4hours . two other tumours regressed completely , but the - , remaining two continued to grow progressively . both received the same treatment on the 37th day . one died with a large tumour on the 45th day . 
the five mice which had been completely " cured " were kept under observation for a year and were then killed . post - mortem examination revealed no trace of carcinomas . the charting of all the tumours in these experiments was carried out independently by a . 
chapman , the senior technician in charge of this work . discusston9 with all the tumours which underwent regression in the preceding experiments there was extensive haemorrhage following treatment . this ' was most readily induced in the a strain mice . 
a few hours after the injection of the maximum sub - lethal doses of the drug the tumours appeared blue through the skin . subsequently superficial ulceration was of common occurrence . since boyland and boyland ( 1937 ) first drew attention to the similarity of action of colchicine and bacterial filtrates they have been shown to behave alike in most other respects . 
with both , complete regression of some transplantable and spontaneous tumours has been effected . ' the results acquire significance in that they indicate the limitation of haemorrhage - inducing agents in the treatment of malignant growths . that some form of damage to the capillary system of tumours might be ' the best way to inhibit malignant growth was suggested by woglom ( 1922 )  . 
a critical review of the evidence concerning tumour regression led him to raise the question whether " the receding tumor may not differ from the growing one only in the extent to which its blood vessels have been obliterated by thrombosis . " he pointed out that the blood vessels of many tumours are more subject to thrombosis than those of normal tissues , and he conceived the possibility of both chemical and mechanical factors being responsible . 
the former resulted from the abnormal metabolism of malignant cells , and the latter was described as " the mechanical pressure which the rapidly increasing parenchyma must often exert upon its vessels , with all the possibilities of injury to their walls which this would entail . " more recently algire ( 1945 ) has devised an adaptation of the transparent chamber technique which enables microscopic observations to be made of the development of the blood vessels of tumour transplants . 
he reports that although many vessels in growing tumours become very large , " differentiation in mammary cancers he observed into arterioles and venules was not evident . " the development of " blood - filled cul - de - sacs . " " these appeared to result from r . 
cravetz. from the lawall memorial laboratory of pharmacology and biochemi8try , philadelphia college of pharmacy and science , philadelphia , penn8ylvania . received for publication june 15 , 1951 . caspersson and his associates advanced a hypothesis on the ' role of nucleic acids in the biological synthesis of proteins ( caspersson , 1947 )  . several other results suggested the role of nucleotides in the metabolism of tumors as well , as a result of which many structural analogues of pyrimidine and purine derivatives were synthesized and tested for anti - cancer and growth - inhibiting activity ( roblin , lampen , english , cole and vaughan , 1945 ; kidder and dewey , 1949 ; kidder , dewey , parks and woodside , 1949 ; sugiura , hitchings , cavalieri and stock , 1950 ; burchenal , bendich , brown , clian , hitchings , rhoads and stock , 1949 ; skipper , bennet , edwards , bryan , hutchison , chapman and bell , 1950 ; law , 1950 ; lewis and crossley , 1950 . ) however , little is known about the effect of the naturally occurring nucleotides on tumor growth . parsons , gulland and barker ( 1946 , 1947 ) described that in c57 mice the growth of homologous methylcholanthrene sarcoma grafts was inhibited by ( yeast ) ad ' enylic acid or guanylic acid ; uridyhc acid showed a growth - promoting effect , whereas cytidylic acid had no effect . 
tumor cells are free in the ascitic ascitic fluid was harvested by fluid , usuar abdominal puncture under aseptic conditions , and the number of cells present in the ascitic fluid counted in a hemacytometer . 
cravetz the method used in this study offers the forowing advantages : ' ( a ) cancer cells of known number and equal virulence are inoculated into the control , as ( b ) upon intraperitoneal inoculation similar well as the experimental animals ; ascitic tumors are produced , while subcutaneous inoculation results in the development of solid tumors ; ( c ) in case of intraperitoneal inoculation the action . 
the error in thi 's method is that there is always some microscopic infiltration of sohd tissues in the peritoneal cavity ( klein , 1950 ; klein and klein 1951 )  . cells are , of course , not included in our cell counts . these infiltratin ' swiss mice , bred in our colony , were used for these studies . these mice were maintained o ' n rockland complete rat diet and water , ad libitum , and kept in air - conditioned quarte ' rs at 2 p c . 
the strain aspecificity of this tumor was discussed by klein ( 1950 ) and klein and klein ( 1951 )  . subcutaneous inoculations were twenty - one days after inoculation the made into the caudal third of the back . groups animals were sacrificed , and their tumors dissected and weighed . receiving intraperitoneal injections of cancer cehs were observed for mortailty animals dying were autopsied , their ascitic fluid harvested and measured , rate . and the number of cancer cehs per cubic mihimetre estabhshed as previously descr ' lbed . nucleotides were administered by daily subcutaneous injection , alternating adenosine - 3 - phosphoric acid was injected in between the right and left flank . solution in 3 - 2 per cent disodium phosphate , adenosine triphosphate and adenosine - 5 - phosphoric acid in normal saline warmed to about 37 ' c . 
mean tumor weight8 in gram8 . serim i ( 2 , 000 , 000 cells ) meem mean mean mean serim 11 ( 2 , 000 , 000 cells ) : serim ih ( 2 , 000 , 000 cells ) seriew .1 v ( 200 , 000 cells ) : adenosine - 3adenosine - 5adenosine phosphoric acid phosphoric acid triphosphate i 00 mg . 
the number of cancer cers , however , was smaher in the ascitic fluid of the nucleotide - treated mice than in the control animals . we are greatly indebted to margaret r . 
anderson. from the research department , glasgow royal cancer hospital . received for publication february 22 , 1949 . the need for controlling the influence of solvents used as vehicles for carcinogenic hydrocarbons was recognized by burrows , hieger and kennaway ( 1932 ) , who reported experiments designed to test the fat solvents then in use for this pui - pose , for possible carcinogenic action on the connective tissues of rats and subsequent work showed that in fact lard , which had been previously mice . heated to 140 ' c . , was a potential carcinogen for the connective tissues of fowls ( peacock , 1933 ) , and that lard alone could give rise to spindle - cell tumours in rats ( barry and cook , 1934 ) ; and later that lard , olive oil ' and other fatty materials could induce connective - tissue tumours , some of which appeared to be malignant in rats , but not in mice , in the experience of burrows , hieger and kennaway ( 1936 )  . the first instance of undoubted sarconia induction at the site of the injection of lard in fowls cited above was complicated by the fact that the same birds had been injected with a solution of 1 : 2 : 5 : 6 - dibenzanthracene in lard in the right breast and with lard alone in the left breast . 
of incidentally these tumours in a susceptible bird cannot be excluded . experiments suggest that the quantity of dibenzanthracene actually required to initiate sarcomatous growth must be remarkably small , since the bulk of the the injection appears to remain encapsulated throughout the expei - inient " ( peacock , 1933 )  . 
the latter assumption subsequently proved to be wrong . to test this point , chalmers ( 1934 ) analysed the contents of encapsulated niatter from the site of dibenzanthracene lard injection in one of peacock 's sarcoiiia - bearing fowls , which died 7 months after the last injectioii . 
dibenzanmoreover , in this group no tissue reaction thracene in 0 - 4 per cent solution . could be found at the site of injection after a few months , indicating that the homologous fat had caused httle disturbance . however , with egg yolk fat as vehicle for dibenzanthmmne m 0 - 4 per cent solution , 2 metastasising sarcomas occurred among 4 birds that s ' urvived 9 months or more after injection . birds inject - ed with yolkfat showed fibrous cysts at the site of injection , sinular t - 0 those observed in the lard experiment , and in contrast with the absence of such local reaction in birds injected with chicken - fat . there seemed , therefore , to be some aetiological connection bet - w - een the " foreignness " of the solvent used as vehicle and the local tissue reaction and the ultimate carcinogenic response t - o dibenzantli - racene . owing to the costlv and time - consuming nature of long - term experinients on fowls work was begun on similar lines on mice . while these experiments were in progress berenblum ( 1938 ) reported the co - carcinogenic action of croton oil . he had previouslv shown ( 1929 ) that mustard gas in dilute solution and ( 1935 ) cantharidin had anticarcinogenic properties for the skin of mice , and in the interim had found that no simple relationship between irritant and coor anticarcinogenic action was demonstrable . 
olive oil , tended to retain the dissolved benzp - % - rene as judged by the persistence of violet fluorescence , where - as in the case of those that were rapidlv absorbed , e.g. 
mouse fat or ether , fluorescence could not , be detected after a few weeks ( peacock and beck , 1938 )  . moreover , in the fornier group the incidence of sarcomas was high , and in the latter group it was low . this suggested that there mav be an optimal period for the retention of a carcinogen at the site of injection for the induction of a tumour , and that in mice this period was about a months . dickens and weil - malherbe ( 1942 ) at first confirmed our observation with mouse fat ' , but later ( 1946a ) , as a result of intensive experiments , found that the effect was not constant and was related to the phospho - lipid content of the 298 p . 
the mice were killed after different periods ( table 1 ) , the subcutaneous tissues exposed and examined for ultra - violet sixteen of 20 mice killed at various times over a period of 7 months fluorescence . had fluorescent material located at the original site of injection ; ulceration and sepsis at the site of injection killed 4 mice early in the experiment . in 3 of these mice no sign of the injected material was found , probably due to sloughing and leakage from the site of injection . 
the fourth had a small spot of fluorescence . these mice were not examined further ; in the remainder the fluorescent material was extracted with benzene , with the exception of 2 mice , which died after 412 - and 51 months , both showing persistent fluorescence and tumours at the site of injection . after the third month of experiinent tumours began to be clinically recognized at the sites of injection . as most of these tumours were similar to many such induced sarcomas in mice , not a 11 were histologically examined . 
one tumour in the abdominal cavity associated with intraperitoneal deposits of fluorescent material was probably induced by benzpyrene injected accidentally through the abdominal w , - , 11 . another tumour occurred in an ulcerated area at the site of injection . this proved to be a squamous carcinoma . 
benzene , and the benzene extract dried over anhydrous sodium sulphate . since the main object of these experiments was to demonstrate the pre - sence vne after various periods , the experiments were not conor absence of benz ducted quantitatively . however , the limit of sensitivity of the method of detection provides some indication of the quantities involved ( vi& infra )  . 
to eliminate the possibihty of a false positive reswt due to traces of benzpvrene adhering to the apparatus used in the experiments , benzene washings of each piece of chemical apparatus or other instrument used , were examined under the ultraviolet lamp imniediately before its use . attention was drawn to the necessity for such precautions ri_ - , cently ( anderson , 1947a )  . 
owing t - o the difficulty of eliminating minute traces of material from apparatus , such traces may be recorded by the fluorescence method of detection , and lead to a false positi ' ve result . 
the absenee of benzpyrene from extracts of two tumour - bearing mice killed - 4 months after a siiigle injection of benzpyrene does not preclude the possibilitv that the uneliaiiored hvdrocarbon was still present at the inception of the tuiiiour process as it was in tfie other tumour - bearing animals killed after shorter periodss . thus the results of this experiment accord well  . , a - ith otir previous observations ( peacock and beck , 1938 ) that when fluorescence remained at the site of injectioii in iiiiee for 5 months or more there was a hiah incidence of sarcoma . 
on this basis dickens ( 1947 ) states that " the surprising result was obtained that the more rapid elimination of benzpyrene was associated witli the higher carcinogenic activity , and slower elimination mith lower acti - 6ty . " fact the graphs published bv dickens and weil - ' - nlalherbe ( 1946b ) show . 
in the case of tricaprylin alone , and of tricaprylin plus phospholipids as solvents for benzpyrene , a consistent rate of elimination of the hvdrocarbon from the sit ' e of injection , but not to the point of extinction within s5 davs and 10 - 10 davs extrapolation of the tricaprvlin graph would in&ate total etim " lrespectively . nation in the region of 26 weeks . as w out of 26 mice had tumours bv the 20th week , it seems reasonable to , suppose , that some benzpyrene was present in these mice throughout the latent period of careinogenesis . this would correspond closely with our own experience . in the graph illustrating the course of events following injection of benzpyrene dissolved in tricaprylin plus 3 per cent choleste , rol , dickens and weil - malherbe ( 1946b ) show a considerable variation in the persistence of benzpyrene in different mice . 
as no t - umours were recorded before about the 19th week of their experiment , there is no positive evidence about the persistence or absence of benzpyrene at the site of injeetion in their tumourbearing mice . ou - r own repetition of their experiment . 
anderson mice , and must therefore have been present throughout the latent period of carcinogenesis . while it seems certain that partition of benzpyrene between the solvent used - is vehicle and the body fluids must be largely responsible for the rate of elimination of benzpyrene , the local tissue reaction to different solvents may also help to determine the local response . 
they established that for benzpyrene the partition coefficient between human sera and various lipoid solvents was directly related to the carcinogenic response of mice injected with benzpyrene dissolved in those solvents that readily parted with benzpyrene in vitro gave fewer solvents . ttimours when used as vehicles for injection of benzpyrene in mice . their conclusions support the conception that there is a significant relationship between the retention at the site of injection of benzpyrene and the ultimate carcinogenic response . whatever may be the essential mechanism of conversion of a normal cell to a malignant one , it seems certain that some local consumption of energy by some part of the cell must be involved in the transformation . it may well be that the liberation of energy at the optimum time in the life - cycle of a stisceptible cell is the essential carcinogenic stimulus , and this may be provided by the metabolism of a carcinogen . in this event neither the parent hydrocarbon nor its metabolites , but the transition from one to the other , may provide the essential carcinogenic stimulus . 
as this finding was of great importance not only to the general problem , but more particularly as a possible test of the validity of conclusions which were being formulated , it was decided to confirm their results . initial casual observation by nettleship and henshaw was made on female mice of the c3h strain , which normally shows a low incidence of pulmonary tumours , in an experiment in which urethane had been used as the anaesthetic . 
the urethane group in the first experiment consisted of 100 mice , the other three groups of 60 mice each , and 60 untreated mice were observed over the same period . 
the mice were examined post mortem as they died during the course of the experiment , or when the survivors were killed 185 days urethane 12 per cent ; 312 j . 
the second experiment was made on 100 mice similarly treated with urethane ; no other substances were used , in view of the negative results of the first experiment . in this experiment at the end of treatment the mice were allowed to survive until they died , with a view to assessing the persistence and growth of the adenomata . unfortunately enteritis and cannibalism reduced the amount of histological material below what was hoped for in both experiments , but not to such an extent as to make it inadequate . 
when the nodule projects above the pleural surface , is smooth and uniformly rounded , and greyish - white in colour or semi - translucent , it can be regarded with some confidence as a formed adenoma , but only a proportion of the fiat nodules will prove to be adenomata . 
at a later stage the lungs showed induration from chronic inflammation , more often than not accompanied by acute consolidation of one or more lobes . it was at this stage that subpleural nodules began to appear in numbers , and the pale miliary spots on a deep red background often presented in the latest stages , after treatment had been discontinued , a striking picture . the lungs were free from consolidation , but showed distortion of shape as a result of emphysema . 
not only is it possible to trace the stages of development of a tumour in the chronic foci of inflammation and collapse , but the striking difference in the incidence of pneumonia with urethane as compared with the other anaesthetic substances used is highly suggestive . since this work was done , larsen ( 1946 ) has also shown that urethane is so far unique amongst narcotic compounds tested ; he used a larger selection of such substances than was employed here , but without finding any other which produced a significant increase in pulmonary adenomata . in their original communication nettleship and henshaw ( 1943 ) did not appear to be impressed with the evidence of inflammation . 
they found that conditions such as bronchiectasis , purulent bronchitis and acute pneumonia were distributed alike among the experimental and control animals . they are emphatic that lung tumours and pneumonia were never seen together , it is possible that this difference though they occurred apart from each other . of interpretation may depend on what is meant by the term pneumonia . 
orr. from the department of experimental pathology and cancer research , university of leeds . received for publication july 19 , 1947 . attention was drawn to the frequency of spontaneous tumours in the lungs of mice by tyzzer ( 1907 - 8 , 1909 ) , whose description of their histology has required but little amendment . 
bruzzone. from the department of experimental medicine , national health service of chile , santiago . received for publication june 9 , 1949 . abdominal fibroids induced in the guinea - pig by a - oestradiol ( nelson , 1937 ; lipschutz and iglesias , 1939 ) are prevented when progesterone or other 3 - ketosteroids are administered simultaneously with the oestrogen ( lipschutz and vargas , 1941 ; lipschutz , 1944 ; lipschutz , iglesias , bruzzone , fuenzalida and riesco , 1948 )  . 
 = fibrous tumoural effect ; units according to lipschutz and vargas ( 1939 ) t tablets of pure progesterone or part of a tablet . in the remaining groups - tablets from experiments of e . 
but these figures of active quantities of progesterone are not very distant from those obtained in our former work with the antifibromatogenic action of progesterone against o - oestradiol . there is also the fact that statements about absorption per day are stultified by its not being uniform throughout the experiment on account of the diminished surface , and by substances entering into the tablet from outside ; errors are 400 s . 
bruzzone this is why it would be daring to consequently considerable ( folley , 1944 )  . interpret the present results as indicative of a greater resistance of artificial oestrogens to the antifibromatogenic action of progesterone . 0o i1111j1 hexestrol hexestrol and progesterone fig . 
5. continued immersion in the agent gave rise to a more intense staining in this region , with the formation of dense , highly coloured figures . these are shown in fig . 
7 , and are strictly comparable with the golgi bodies of cells of the same tumour ( sarcoma 37s ) illustrated by ludford ( 1932 )  . it was found that the golgi body of cells of the two fast - growing tumours , i.e. , beta and 37s , was 262 g . 
the intense , and rapid staining may also be associated with lipoid constituents in the mitochondrial structure , since fatty substances within the cells very rapidly absorb and reduce the tetrazolium salts . consideration of the staining reactions of nuclei suggests that the nuclear membrane is in two distinct layers . 
the outer is a continuous hyaline sheath , whilst the inner is a structure of irregular thickness . it is this inner structure which so readily stains with the tetrazoliuthe appearance of the nuclear membrane under these conditions corresponds with that described by ludford and smiles ( 1950 )  . these authors ascribed the granular material on the inner side of the nuclear membrane to chromatthe present technique indicates by virtue of the differential staining intensities that it is chemically different from whatever material comprises the chromonemata , and more nearly resembles the nucleolar material in the distribution of reducing groups . 
the method does not , however , offer any indications as to exact chemical nature of the stained substrate . the falling off in staining intensity exhibited by the chromosomes as division proceeds is interesting in that tumour cells are known to be more sensitive to irradiation during the early stages of mitosis . it appears possible that this is associated with the greater number of reducing groups available at this stage , since radiation effects are known to include oxidation of such groups as - sh . since the evidence on this point can only be regarded as equivocal this issue will be the subject of further experiment . the uptake of tetrazolium by the golgi region of these cells is perhaps not surprising , since the classical techniques for demonstration of the golgi apparatus rely on the reduction of metallic compounds to insoluble derivatives . 
the very slow but continuous manner in which the staining takes place suggests that there is no great array of reducing groups available at any one time , but that as a result of metabolic processes these are steadily being rendered accessible . 
lucasanda.c.thackray. from the , department of pathology , the royal dental hospital of london school of dental surgery and the bland - sutton institute of pathology , the , middlesex hospital , london , w . 
the tumour occurs in the lower jaw much more frequently than in the upper ( i 7 cases and 3 cases respectively in this series ) , is usually a central lesion and gradually enlarges , in the majonty of cases without pain . in the course of time the bone becomes absorbed , and if a cystic loculus is opened infection and discharge forow . local recurrence iscommon fohowing inadequate treatment , but metastases are very rare . 
a case of pulmonary metastases has been reported by waterworth and purar ( 1948 ) , who review previous reports . the natural history of the disease is long ; it is not always easy therefore to assess the efficacy of various methods of treatment . most authorities consider radical excision of the tumour to be the treatment of choice . 
thus the least evolved type of tumour consists of strands of more or less undifferentiated epithehal cers growing in a fibrous stroma , while a tumour which has undergone a greater degree of entiation consists of folhclea 290 r . 
the epithelial follicles in such cases consist of an outer layer of columnar cells resembling the similarly situated cells of the enamel organ , while towards the centre the cells become stellate in appearance and cyst formation may occur . on the other hand , the trend of differentiation may be towards a more highly developed type of squamous epithelium , in which case the tumour consists of sheets of squamous cells showing a tendency to cornification , or a basal cell type of growth may be produced . these tumours may thus present a variety of appearances , from case to case , or in different areas of the same growth , and while attempts at classification on a histological basis are helpful in so far as they indicate the varying degrees of differentiation whicli can be observed , they are seldom entirely applicable to any given specimen . 
tboma ( 1950 ) has proposed one such classification , as follows , though he notes that pure types are but infrequently seen : ( 1 ) primitive type , composed of strands of epithelial cells showing little tendency to differentiation , growing in a loose fibrous stroma . 
a very rare type of tumour in which haemangiomatous characters are present . ( 8 ) melano - amelobla , 3toma . also a very rare tumour , in which the epithelial cells contain pigment . in our series 4 cases were of the primitive type , whilst the remainder were fig . 
2 ( case 5 ) shows an largely follicular or showed mixed appearances . example of the primitive type of tumour , cords of epithelial cells growing in a fibrous stroma . 
6 ( case 5 ) , in which the growth is composed of follicles or nests of epithelial cells with outer columnar layer and inner stellate area . microcyst formation , a common occurrence in adamantinoma , was present in typically , these cysts occur in the area of stellate cells towards the 14 cases . centres of the follicles , but they also form in the stroma . 
the occurrence of stromal cysts is a point to which very little previous consideration appears to siegmund ( 1929 ) noted their occurrence in 2 of his cases , but bave been given . apart from this instance , and a passing reference by kronfeld ( 1930 ) to the same fig . 
8 ( case 1 )  . in the latter case , however , it will be seen that though there is some breakdown within the follicles , the majority of the cysts have formed on the side of the columnar cell layer opposite to that on which fig . 
even in the 6 cases showing epithelial cysts only , evidence could be found in 3 cases of incipient degenerative changes in the stroma . the cause of cyst formation is a matter of conjecture . it is believed to be the result of progressive degeneration in originally solid growths . the solid tumour closely resembles the developing tooth up to the point at which differentiation of adjacent connective - tissue cells into odontoblasts , and subsequently amelogenesis , would occur in the case of the tooth , but at this stage the tumour cannot develop further . degeneration therefore takes place ( kronfeld , 1930 ; robinson , the ensuing accumulation of fluid of relatively high osmotic tension is 1937a )  . probably a factor in the progressive enlargement of the microcysts , a mechanism investigated by toller ( 1948 ) in the case of simple dental cysts , and quite possibly a factor also in the case of cyst formation in these tumours . with regard to cyst formation in the stroma , it appears that again a process of degeneration is at work , and all stages of breakdown can be seen from a slight loosening of the stroma to mucinous - like degeneration and the formation of completely clear cystic spaces . 
the inner enamel epithelium is that which lines the concavity of the enamel organ , a single layer of tan columnar cells which will produce enamel , while the outer enamel epithelium consists of cuboidal cells covering the convexity of the organ . 
on the other hand , bland - sutton ( 1922 ) thought that the enamel organ could not be the origin of these growths , since the majority of patients were well into adult life when their tumours first appeared . however , robinso ' n ( 1937b ) in his survey of 379 cases found that the tumour was first noticed between the tenth and thirty - fifth years in 70 per cent of cases . considered together with the fact that these tumours are very slow growmg and have a long natural history , it is evident that the majority of growths originate at quite an early age . robinson ( 1937b ) also found that the tumour occurred most frequently in the premolar and molar regions , where supernumerary tooth germs most often occur , kegel ( 1932 ) and and that many cases were associated with a missing tooth . geschickter ( 1935 ) also support the view that the tumour arises from the enamel byers and sarnat ( 1945 ) believe that the tumour originates from that organ . structure during the first few years of life , though active growth may not become manifest till later . if these tumours , or at least the majority of them , originated directly from the enamel organ , it might be expected that on occasion enamel would be formed . this is never the case , though thoma ( i 950 ) considers that the homogeneous zone sometimes to be seen between the basal membrane of the columnar cells in the follicular type of adamantinoma and the stroma , which appears yellow with van gieson 's stain , must be considered as abortive enamel formation , though it is possible that precystic changes in the stroma could account for such appearances . 
thackray these tumours resemble rodent ulcers in several respects . tumour without involvement of the oral epithelium , is , however , evidence against an origin from the oral mucosa . both are related to derivatives of the covering ectoderm , the one to teeth and the other to hair follicles , though discussion continues as to the stage of development of the appendage at which they arise . 
they are composed of relatively undifferentiated cells which can give rise to any of the appearances found in these tumours , and moreover will produce a central growth . it is not necessary to postulate tumour formation from these rests in early life , with a subsequent interval of dormancy to account for those cases in which the tumour first appears at a comparatively late age . being present from the formative phase of the dental tissues onwards they can proliferate at any time , and this seems a more satisfactory hypothesis than the dormancy theory . the rests of serre , those left by the dental lamina , are situated quite superficially . 
here the cells tend to take on a sterate appearance towarcls the centres of the cords and become elongated and columnar at the periphery . there is some cystic degeneration in the stellate areas and also in the stroma . case 4 : - 11 . 
1893. - 1910 : dentigerous cyst of one year 's duration 1928 : swelling had gradually increased in removed . size till there was now a hard tumour of the right mandible . this was excised and the cavity of a multilocular cyst exposed . 
radium tubes forced up through harcl palate . october , 1925 : no improvement . tubes left in 18 hours . december , 1925 : left side of face swollen over superior maxilla . severe paon left side of hard palate is an irregular swelling extending from mid - line to , and including alveolar margjanuary , 1926 : alveolar part of superior maxilla and the palatal tumour excised . 
1892. - 1926 : noticed a lump in the right upper jaw which she thought to be due to ill - fitting dentures . this was treated with " caustic and disappeared , but recurred within 4 months . it was again similarly treated . 
1928 on admission to hospital an oval area of enlargement of the right maxina was noted , situatecl between the alveolar margin of the maxilla and the inner surface of the cheek , the long axis clirected antero - posteriorly for about an inch . 
1899. - 1928 : operated on for " abscess of j aw . 1937 : painful swelling appeared at site of previous operation . x - ray examination showed a multflocular cyst in the 3 - / - 6 region . 
1887. - 1929 : the patient complained of a lump on the right side of the jaw of 10 years ' duration , which had been operated on 3 times , 10 , 6 and 3 years previously . it had increased in size , painlessly , but rather rapidly since the last operation . 
1881. - 1937 : three years ' history of swelling of the right lower jaw after extraction of 3 teeth . this was considered to be due to a dental cyst , and the jaw was scraped on two occasions . after the first operation the swelling disappeared . 
thackra ' y examination showed a large swelling on the lingual and buccal aspects of the pain . x - ray showed expansion of the jaw by a loculated , premolar and molar regions . 1950 : died from other causes . 
1883. - 1937 : admitted to hospital for a fracture of the this appeared elbow - joint , when a large swelling of the right mandible was noticed . to have started some 5 years previously , and had been gradually increasing in size . x - ray examination showed the typical appearances of adamantinoma , and local excision of the cyst was undertaken . 
3. given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . since 1944 we have taken a detailed family history from all patients reporting with carcinoma of the breast . 
we have 459 family records up to the end of 1947 which are reasonably complete . so far we have not succeeded in supplementing these histories , taken at the time of first visit to hospital , by later questions to the surviving patients or by arranging visits to their homes or relations . 
some attempt has been made to confirm the causes of death of relatives by letters to hospitals , doctors and the registrar - general 's department , but such confirmation has , as yet , been obtained in only a few cases . our figures , therefore , contain all those errors of inadequate information and faulty recollection that one would expect from data collected . 
many people die of cancer without their relations knowing that this was the cause of death . it is in fact surprising how successful a woman can be in concealing a cancer of the breast from her nearest relatives living in the same house with her . it is not , therefore , so surprising that more distant relatives , or even close relatives living away from home , may be unaware of the nature of the illness involved relations , even some of an older generation , who are still living at the time that the patient is first questioned may later develop malignant disease . 
many patients with cancer of the breast survive for long periods following treatment , and may ultimately die from some other cause ; we are , however , unable to include patients living who either have , or have had , cancer in our figures for comparison with expected incidence in the general population because no adequate morbidity statistics are available . in our series , for instance , there are the same number of sisters alive following treatment for cancer of the breast as there are sisters who died of the disease . ' comparisons must be made on a basis of mor164 d . 
3 shows a family where the mother of the patient died of cancer of the uterus aged 67 - she had two sisters , one who died of " internal cancer , " and one 166 d . 
smithers this sister had a daughter of cancer of the breast ' the latter aged about 60 . who had her breast amputated for cancer aged 45 , and who died aged 60 of lymphatic leukaemia . 
we find no evidence that cancer of the breast tends to develop earlier in patients whose relations are known to have suffered from the disease . the greater part of the work presented in this paper was done by p . rigby - jones and h . 
hartley , whose valuable assistance made this contribution to the symposium possible . i am also indebted to my colleagues on the staff of the royal cancer hospital whose patients were interrogated during this investigation , and particutlarly to r . 
5. continued immersion in the agent gave rise to a more intense staining in this region , with the formation of dense , highly coloured figures . these are shown in fig . 
7 , and are strictly comparable with the golgi bodies of cells of the same tumour ( sarcoma 37s ) illustrated by ludford ( 1932 )  . it was found that the golgi body of cells of the two fast - growing tumours , i.e. , beta and 37s , was 262 g . 
the intense , and rapid staining may also be associated with lipoid constituents in the mitochondrial structure , since fatty substances within the cells very rapidly absorb and reduce the tetrazolium salts . consideration of the staining reactions of nuclei suggests that the nuclear membrane is in two distinct layers . 
the outer is a continuous hyaline sheath , whilst the inner is a structure of irregular thickness . it is this inner structure which so readily stains with the tetrazoliuthe appearance of the nuclear membrane under these conditions corresponds with that described by ludford and smiles ( 1950 )  . these authors ascribed the granular material on the inner side of the nuclear membrane to chromatthe present technique indicates by virtue of the differential staining intensities that it is chemically different from whatever material comprises the chromonemata , and more nearly resembles the nucleolar material in the distribution of reducing groups . 
the method does not , however , offer any indications as to exact chemical nature of the stained substrate . the falling off in staining intensity exhibited by the chromosomes as division proceeds is interesting in that tumour cells are known to be more sensitive to irradiation during the early stages of mitosis . it appears possible that this is associated with the greater number of reducing groups available at this stage , since radiation effects are known to include oxidation of such groups as - sh . since the evidence on this point can only be regarded as equivocal this issue will be the subject of further experiment . the uptake of tetrazolium by the golgi region of these cells is perhaps not surprising , since the classical techniques for demonstration of the golgi apparatus rely on the reduction of metallic compounds to insoluble derivatives . 
the very slow but continuous manner in which the staining takes place suggests that there is no great array of reducing groups available at any one time , but that as a result of metabolic processes these are steadily being rendered accessible . 
the coal miners form an interesting group for comparison with the professional classes , for the miner 's daily bath , often obtained under very adverse conditions , secures cleanliness for about two - thirds qf the time , while in other respects his skin receives very rough treatment . 
the census returne ( registrar - general , 1938 ) give the age distribution , in 5and 10 - yearly periods , of the whole population of males , and also of those following each one of the recognized occupations , at the time of the census . the number of deaths attributed to cancer of the skin and lip occurring in the whole male population in each of these age groups during the years in question was obtained from the statistical reviews of the registrar - general . 
 " cancer of the thigh , " " cancer of the neck and face , " " cancer of the face and antrum . " certificates of persons under 14 years of age were excluded . 
1 shows the percentages , arranged in ascending order from left to right , for 41 occupations in which more than 5 deaths from cancer of the skin occurred in the 34 - year period ; this quite arbitrary limit in number of deaths is drawn to lessen sampling error . 
the percentage in 15 out of 16 professional occupations selected thus is below 100 , while that in 9 out of 13 agricultural occupations is above 100 , and in 5 is above 150 . 
the occupations of mining engineers , and mechanical and electrical engineers , show no deaths from cancer of the lip , and low percentages for cancer of the skin , but the numbers of deaths ( 5 and 2 respectively ) are small . the high standard of cleanliness maintained by the coal miner at the end of his day 's work , and his lack of exposure to sunlight , perhaps compensate for the various injurious factors , of which an account has been given by knowles ( 1944 ) , first - hand descriptions of the coal - miner 's life to which his skin is exposed . are given in two recent books ( shaw , 1946 ; agnew , 1947 )  . 
the mortality in the hewers and getters , who carry out much of the most severe work of the mine , is , if anything , lower ( 97 - 7 per cent ) than it is in the general population . the percentage is below 100 in 5 coal - mining occupations , comprising 828 , 246 out of the 939 , 378 men , or 88 per cent of those engaged in the 7 divisions of the industry . 
six out of 17 occupations , with a population of nearly 700 , 000 , have percentages from 131 to 249 ; this last figure ( gardeners ) is the highest of all those recorded in this paper . 
fingers , hand , forearm , and so on , might seem to give more information , but the sampling errors would be increased , and in such material the assignment to the smaller sites has not been carried out on any uniform system ; e.g. 
there would be no certainty that some cancers of the fingers had not been classed as of the hand . the numbers of cancers at these sites in the three groups of occupations , and their percentage distribution , are given in table iv and fig . 
1 provides a comparison of the percentages for cancer of the skin , and of the lip , selected and arranged in the same way , except that all cancers of the lip are included and not only those shown by occupation yielding more than 5 deaths . 
the number of fatal cases of cancer of the lip in the professional classes is so small ( 27 in 34 years in about 400 , 000 men ) that these have been pooled m . 
2. - occupational distrnbution of cancers of the skin according to site . show that no one of the seven groups of coal and shale miners gives a percentage above 100 ; the figures are low ( 38 - 3 to 56 - 0 per cent ) except in one large group which is the most exposed to light ( other workers above ground , population 106 , 549 ) , in which the incidence ( 97 - 5 per cent ) is approximately the same as in the general population . 
1 shows that the incidence of fatal cancer of the skin is high upon agricultural workers , and very low upon the professional classes , while the miners take an intermediate position not far removed from that of the general population . 
the especial liability of the out - door workers is generally supposed to be due to exposure to sunlight ( blum , 1948 )  . the results given in table iv and fig . 
2 show that the cancers of the whole region of neck , head , and face together , selected on the basis described above , make up from 70 to 78 per cent of cancers of the skin in all three occupational groups . 
the face is the only part of the body which is never clothed , and those parts which are shaved receive more thorough cleansing than do any others ; these characters are common to all social classes . 
the most notable result of this tabulation is the lack of any great difference between the three groups . another factor which may be of considerable importance is that the cosmetic effect of cancer of exposed portions of the skin and of the lip may attract attention sooner in richer subjects . ingram ( 1947 ) , in a comment on the paper by ryle and russell ( 1947 ) , says : " prognosis in skin cancer depends largely upon the size of the lesion , and negligence is probably an important factor in relation to death from this cause . i should , in the ordinary course of events , expect neglect of a symptomless lesion to be higher in unskilled workers and labourers ( iv and v of the registrar - general 's social classes ) than in the other groups . " obviously one cannot assess the quantitative importance of this difference . data in equal detail for the distribution of skin cancer in married women whose husbands follow these occupations would be of great interest . 
the great preponderance of tumours of the lower lip is explained as due to direct exposure of its mucocutaneous junction to sunlight , while the corresponding part of the upper lip is relatively shaded . " some factor in addition to exposure to sunlight is required smoking , and especially pipe to explain the differences shown in table vii . smoking , is , of course , regarded as another possible factor in the production of cancer of the lip . during the earlier part of the period ( 1911 to 1944 ) cigarette smoking was practically restricted to the richer classes , which produce fewest cancers of the lip ; data on the change in this matter in recent years have been given elsewhere ( kennaway and kennaway , 1947 )  . 
the data collected by lane - claypon ( 1930 ) from the literature , summarized in table vii , show the great preponderance of cancers of the lower lip , especially in males . 
 ( lanecilaypon , 1930 )  . all occupied and retired males agricultural labourers farmers deaths . death rate per million per annul . 212 798 55 - 0 comparison of cancer of the skin and of the lip . the data given in fig . 
of the 14 agricultural occupations which produce any cancers of the lip , 11 show agreement in regard to cancer of the skin and of the lip in that both percentages are either below , or above , 100 . this suggests that the aetiological factors are to some extent the same in some occupations . 
the incidence upon the coal miner is of especial interest in view of the cleanliness secured by his daily bath , and of his minimal exposure to sunlight . in occupations in which 88 per cent of the coal - mining population are engaged the liability to cancer of the skin is less than it is in the general population . only one occupation of social class i ( civil engineers and surveyors ) shows a mortality from cancer of the skin higher than that in the whole population ; hence these results illustrate the social distribution of cancer of exposed sites discovered by stevenson . 
the comparative distribution of cancer upon the various parts of the skin does not show any great differences in the three groups ; from 70 to 80 per cent of these cancers are situated on the head and neck . 
campbell. from ae royal ( dick ) veterinary college , edinburgh , and the poultry re8earch centre , king ' 8buildinp , we8t main8road , edinburgh . received for publication february 5 , 1951 neoplasms involving the ovary are common in the fowl ( olson and bullis , 1942 ; campbell , 1945 )  . 
the great majority far into one or other of two categories , namely adenocareinomatous growths in various stages ofdifferentiation from the frankly anaplastic type to the sclerosing tumour , or , secondly , lymphomatous growths associated with the leucotic complex , e.g. , lymphocytoma , fowl paralysis tumour , aleukaemic lymphoid leucosis , etc . 
most of these lymphoid growths should not be classified as ovarian tumours , since in view of the generalized nature of the leucotic process it is usuary impossible to be certain whether they are primary in that organ or not . 
they are mentioned simply because of the frequent teference in avian pathological literature to " lymphoid ovarian tumours . " in human pathology , besid6s - the common adenocareinomatous types of , ovarian tumour , several other rarer forms are recognized as follows : brenner tumour ( o6phoroma folliculare ) : granulosa - cell , thecal , and luteal tumours arrhenoblastomas ; dysgerminomas . a survey of the hterature deahng with neoplastic disease of the fowl shows the apparent extreme rarity of such tumours . seifried ( 1923 ) recorded a brenner tumour of the fowl and compared it with its human counterpart , a ' nd friedgood and uotila ( i 941 ) detailed 5 cases of - ovarian " tumours " associated with virilism in two of these latter cases , tuberculosis of the ovary compheated in the fowl . the picture , and the remainder were cystic or contained smau growths which appeared to be tumours in various stages of degeneration . tentative diagnoses of arrhenoblastoma were made , but it was also suggested that they might be luteal - cell tumours or " hypernephromata . the only record of an ovarian teratoma in the fowl is by jackson ( 1936 )  . with regard to the male bird , there appear to be no reports of spontaneous seminoma or interstitial - cell tumour , but several cases of spontaneous teratoma testis have been recorded ( sheather , 1911 ; jackson , 1936 ; olson and bulhs , 1942 )  . it seemed reasonable to beheve that the absence of reports of the rarer forms of ovarian and testicular tumours was simply an indication of a lack of intensive study in this brartch of comparative pathology . it was therefore determined to examine as many tumours arising in these sites as possible . 
to date approximately 2000 cases have been submitted to a thorough post - mortem and histological scrutiny , and , as was anticipated , several hitherto unrecorded types of tumour of the fowl gonads have been encountered . it ' is desirable that an account of these should be put on record , not only because of their interest from the viewpoint of comparative oncology , but also j . 
at post - mortem a thorough search was made for metastases , and the possibihty that the gonadal tumour was not the primary growth was ruled out as far as possible . blocks of tissue were taken from many organs for histological examination , whether they showed visible abnormality or not . 
the growth offered some resistance to ' the knife , and its cut surface showed pale yellow fibrous areas containing numerous small cysts and islands of pinkish tissue . there were no implantations in the abdominal cavity and no metastases were found . histologically a large part of the tumour consists of a stroma of interlacing bands and whorls of fibrous tissue , mostly dense , but having a looser texture in there is a certain amount of plain muscle ( characteristic of the some places . avian ovary especially at the hilus ) in one part of a section . 
a comparable structure occurs in the human subject , and is well ifustrated by nicholson ( 1950 )  . ( 2 ) the next ovarian tumour to be considered is the granulosa - cell type , of which 4 cases have been studied in this series . 
on section , it was cream to yellowish in colour and displayed bands of tissue which had a tehdency to radiate from the centre of the growth . the vascularity appeared to be very poor . 
the rest of the ovary seemed normal , with a few atretic follicles , and the oviduct was that of a bird in full lay . histologl ' cally , this tumour is mainly composed of round oval or fusiform cefls , with a j . 
the periphery of the growth is largely necrotic . radiating bands of smooth muscle occur in the interior of the section . wilhs ( 1948 ) states that ovarian fibromata are probably the end result of a in that case , the rarity of the latter in fowls may account theca - cell tumour . for the equary rare occurrence of fibrous tissue tumours associated with this organ . 
as an instance of this the only case of ovarian fibroma encountered in this series is worth mentioning . it was found in a rhode island red hen in her third year , and weighed 570 g . 
maximow and bloom ( 1948 ) state that what are usually considered chromaffin cefls ( sympathicotrophic cells ) are to be found at the hilus of the human ovary . these apparently have much in common with the medullary cells of the adrenal , although they cautiously conclude that until these cells have been shown to elaborate epinephrin , their relationship to adrenal medulla must remain unproven . the chromaffin reaction of such ovarian cells is unrehable but this also applies to the adrenal medullary cells , where the staining by chrome salts may vary from practicary none to a very deep brown . as far as can be ascertained there is no record of chromaffin cells or heterotopic adrenal cortical tissue in the avian ovary . that such cells may in fact be occasionally present seems to be imphed by the following cases , and a thorough cytological examination of the region of the hilus should clear up this point . the first of these tumours to be described occurred in a brown leghorn hen which was brought for examination after developing signs of mascuhnization . the bird was said to have ceased laying , commenced crowing and to have endeavoured to copulate with other hens in the run . the comb was decidedly male in character , and plumage changes were evident especially in the neck and taff . upon post - mortem , a rounded soft yellow - brown tumour measuring 3 - 8 x 3 - 5 x 28 cwas found in the ovary , which was inactive . 
numerous irregular trabeculae containing vessels arise from this and pass into the interior of the growth . between these are sohd islands of large polyhedral epithehal cells which are in turn divided into small irregular groups by fine connective tissue staining as for reticuluthe cytoplasm is eosinophilic and faintly granular . in places it is vacuolated . 
the first view is favoured as being the more probable . ( 5 ) the next case , though not a mascuhnizing growth , is worth recording for its unusual nature , and because its interpretation could mean that besides adrenal cortical ceus , chromaffin cells resembhng those of the adrenal medura may occur in the fowl 's ovary and may undergo neoplasia in common with other heterotopic - tissues . during the examination of a crossbred fowl wbich was found dead , a large intra - abdominal blood clot was found proceeding from a rupture in the substance .of a smoothly lobulated brownish - yerow tumour of soft consistency , measuring 6 - 5 x 5 x 4 - 3 cand occupyi ' ng the site of the left ( functional ) ovary . it was - freelymovable , being only attached at the bilus , and was therefore easily dissected out . 
the healthy remainder is composed of connective tissue cells with spherical to spindle - shaped nuclei , and eosinophilic granular cytoplasm , surrounding aggregations of large polyhedral cells with abundant finely granular eosinophihe cytoplasm , large nuclei and very prominent nucleoli ( nuclear - nucleolar ratio . 1 : 3 to 1 : 5 )  . an abundant infiltration with eosinophils is present in many parts of the smau epithelial - cer moiety . a well - marked but thin layer of connective tissue separates this outer zone . from the inner , which is composed of small lobules of cens separated from each other by fine trabeculae of connective tissu ' e . 
the cefls composing these groups are large , with giant nucleoh similar to those mentioned above , and have a brownish - yerow cytoplasm in bichromate fixed haematoxyhn and eosin preparations . 
at the edge of one series of sections , the only indication of ovarian origin is the presence of a few folhcles . bands of smooth muscle are scattered throughout the section . the presence of such la ' e numbers of cers showing a distinct chromaffin reaction justifies ' a diagnosis of chromaffmoma or paraganghoma . 
the growth appears to have arisen within the adrenal capsule . another small ( 0 - 5 x 0 - 2 cm . ) tumour was found in the site of the rudimentary right goriad and closely adherent to the dorsal wall . this shows not only testiculoid elements , but also a considerable area composed of whorls and strands of rapidly dividing mesenchymatous cers , presumably a metastasis from the experimentary transplanted sarcoma . the histology of both gonadal rowths resembles ewing 's ( 1942 ) fig . 
the nests of cells below the germinal epithehum resemble the primitive sex cords of the indifferent embryonic gonad . this tumour iuustrates well the bisexuality of the embryonic fowl 's ovary . 
the rete ovarii formed from the primitive sex cords is a homologue of the testis and as is well known can develop into one following left ovariectomy of the hen , where the right gonad hypertrophies and differentiates even to the exteht of producing spermatozoa ( benoit , 1923 )  . another tumour of the ovary associated with masculinization in a light sussex hen is shown in fig . 
17. folfculoid formation and luteinization is apparent , and the structure is comparable to a granulosa - cell tumour . in fact , this diagnosis would be justifiable on histological grounds alone , but has to be modified in view of the androgenic effects on the host . it would appear that the rudimentary right ovary is not the only place where in theory at any rate , testiculoid structures could arise in the intact bird . 
champy , lavedan and marquez ( 1 939 ) state that the adrenals of either male or female castrates in the fowl frequently contain " regenerating gonadal cens . " birds ' adrenals constantly contain wolffian duct remnants in the capsule on the ventral these slowly hypertrophy following castration to form an internal aspect . epididymis - hke structure , whilst some form epithelial tubules similar to those found in the right ovarian rudiment subsequent to castration . 
spermatogenesis has not been seen in the adrenal capsule however . there does not seem to be any record of spontaneous arrhenoma arising in the adrenal capsule of the fowl , but it seems possible that the foregoing is a case in point . ( 7 ) the last of the tumours of the female gonad to be described was originally considered to be a teratoma . it is unfortunate that no comparison can be made of this case with the only comparable ovarian tumour of the fowl on record ( jackson , 1936 ) , since apart from stating its didermic character , no other details were given , and the single photograph is of the gross specimen . the present case occurred in a brown leghom hen aged about 3 years , at the poultry research centre . 
of which was withafter death 4 days later , an ovanan tumour was drawn from the abdomen . it was mottled pink , brownish and cream , of found measuring 5 x 4 x 4 cm . other growths , pinkish and soft , firm consistency and mucinous on section . were attached to the wall of the oviduct , and to the serous investment of the duodenum , pancreas and liver . histologically the ovarian tumour is the only one to show complexity of immediately below a thin capsule there are nests oflarge pale staining structure . epithehal cefls , spme of which have differentiated into cysts of varying size , lined with one or several layers of columnar epithehum . in many cases these cells are actively secreting mucus . 
at first sight two embryonic layers appear to be involved , namely mesoderm and ectoderm . the latter may be represented by the cyst epithelium forming mucinous glands , and possibly as the complex epithelial tubular structures . 
the remainder of the tumour is mesodermal in origin . ifthis is the case the presence of these derivatives of two germinal layers presumably puts it in the same category as jackson 's ( 1936 ) " didermic teratoma . " wiuis ( 1948 ) defines a teratoma as " a true tumour or neoplasm composed of multiple tissues of kinds foreign tothe part in which it arises . " the presence of cartilage can be explained by the conversion of connective tissue normary present in the ovary , to cartflage by mucoid degeneration and hyalinization . 
one of their cases exhibited metastases , but no details are given of the histology of this secondary growth or its site . several seminomas have been studied during the past 11 years and two of these are selected for description here . 
the right testis was normal both in size and microscopic structure , and no metastases were found . microscopically the left testis consists of poorly dehneated lobules of pale staining epithelial cells arranged in diffuse sheets and penetrated here and there by blood vessels . the cells are mainly spherical to polygonal through mutual pressure , but the faintness of cytoplasmic outfine often gives a syncytial appearance . 
a second testicular tumour - also involving the left organ - wa 's seen at autopsy in a buff rock cockerel . it measured 4 - 5 x 3 - 8 x 3 - 5 cm . , and on section showed an irregular yeflowish area near the caudal pole , compared with the rest of the tumour which was of a cream colour . 
the cream - coloured area , forming about two - thirds of the tumour . , is composed of typical seminoma cefls , showing in many places a marked acinar structure . luteinization of these cens is proceeding in small isolated areas . 
the question arises whether the interstitial - cell moiety represents a concommitant neoplasia of the stroma , as the acceptance of firket 's ( 1920 ) view on the connective tissue origin of interstitial cells would imply . in other words , is this an example of a " mixed tumour " - or alternatively is it an indication of the teratomatous nature of seminoma , as ewing ( 1942 ) beheves , but which willis ( 1948 ) , nicholson ( 1950 ) , and others dispute ? still another possibility exists , namely that the two cell types have arisen from a common ancestral totipotent germinal cell capable ofgiving rise to a variety of tissues , in accordance with the view put forward by innes , harvey , and dawson ( 1938 )  . a re - examination of fig . 
the last testicular tumour of special interest occurred in a cross - bred fowl , which showed during life a marked atrophy of the comb , and cessation of crowing and of other activities associated with the adult male bird . at post - mortem , a greatly enlarged ( 9 x 10 x 6 cm . ) left gonad was found , a flattened oval in shape and firm in consistency . 
at subsequent autopsy this bird had a small nodule at the site of the right gonad , whose histological structure , in the opinion of the present - writer , resembles that of a thecal - cell tumour . teilum 's ( 1946 ) case of " androma " of the testis in man may be ' another example of a feminizing tumour arising from a persistent remnant of the " ovarian " cortex , and the presence of arrhenomatoid tissue in a testicular teratoma of a .fbwl which lost certain of its male characters has already been described in the present paper . tuming to granulosa - cell and related tumours , the development of the ovary throws some light on the inter - relationship of these oestrogen - secreting growths . in the embryonic ovary it is commonly stated that the granulosa cells arise from coelomic epithehum derived from the genital ridge , whereas the thecal cens , being stromal in nature arise from the mesenchymal elements of the mesoderm . examination of the early ovary , however , shows primary folhcles composed of a central ovocyte surrounded by a ring of indifferent epithehal cens indistinguishable .from the stromal cells composing the rest of the organ . these indifferent cens appear to be the precursors of the granulosa cells , whereas the remainder of the it seems probable that this common ancestry is reflected - stroma forms the theca . in the behaviour of thecal and granulosal cees in the neoplastic state , where both secrete oestrogens as judged by the muscular and glandular hypertrophy of the , oviduct of the tumour - bearing bird , and both undergo the phenomenon of luteinization . granulosa - cell tumours in the fowl are not morphologicary identical to these in man in that they do not exhibit the characteristic " rosettes " which are often j . 
campbell a feature of human tumours , and which are considered to be identical to the bodies of call - exner occurring normally in the stratum granulosum of the human such bodies are not found in the granulosa layer of the ovarian follicle ovary . because this is usuary only one , or at the most two or three cers thick . callexner bodies are usuary considered to be due to cystic degeneration of granulosa , this does not occur in avian tumours where there is ample space for such cers . a change to take place , and it therefore seems possible that these structures may serve some specific purpose as for example a glandular function , in the ovaries of those animals in which they occur . with regard to thecal - luteal cells and the interstitial cells of the testis , it is interesting to note that they appear to have a common ancestory . fell ( 1924 ) states that the ovarian thecal - luteal cells of the fowl are derived from remnants of aborted medulla in the development of the ovary . thus they have the same histogenesis as seminiferous tissue . 
9. - structure of the above , showing vacuolated cells , due to removal of lipoids , to the left ( some nuclei are pyknotic ) and cells resembling fibrous tissue to the right of the figure . 
18. - - - - " mixed ? " ovarian tumour , consisting of areas of tortuous glands , mucinous cysts , cartilage , solid nests of epithelial cells and a myxomatous stroma . 
moroney. from the leicester general h08pital and the colleges qf technology and commerce , leicester . received for publication juno 3 , 1952 . does chronic g " tric ulcer tend to undergo malignant change ? the importance of this question is beyond doubt , both because of the high incidence of gastric ulcer , and because many patients suffering from it are still treated medically over long periods before reference to a surgeon . 
the answer to it is also of considerable importance to the surgeon , owing to the great difficulty of assessing at laparotomy whether early malignant change may have already if the development of secondary carcinoma supervened on chronic ulceration . is really as common as some pathologists ' figures would appear to indicate , there might be a strong case for an e ' ven more radical gastrectomy than is usually carried out for such lesions . conflicting clinical and pathological evidence . the consensus of opinion in the medical literature is that gastric ulcer is a definite predisposing cause of carcinoma , but there is profound disagreement among pathologists about the percentage of cases ' which undergo such malignant change . 
udaondo ( 1939 ) , in an extensive survey of the world literatu ' re , found estimat - es of the incidence of " ulcer - cancer " which ranged frotn 0 to 100 per obviously , some statistical cent , with most intermediate values represented . uncertainty must be present in the majority of these assessmeints , yet there is usually quite inadequate evidence in the published data to lead to its detection . the only general conclusion that can be drawn from a study of these papers is that the authors ' confidence in the more extraordinary estimates seems to vary inversely with the amount of evidence at their disposal . since , according to the registrar - general 's returns , s ' omething like 14 , 000 people die each year from cancer of the stomach , it is not surprising that the heavy incidence of gastric ulcer in the population should have suggested that there was some connection between the two conditions . 
moroney as regards the stomach , and suggests that the incidence of mahgnant change must be very considerably lower than is suggested by most pathologists ' figures . livingstone and pack ( 1939 ) assess the average survival of patients admitted to hospital with inoperable cancer of the stomach at under 4 months , whilst the total duration of untreated primary gastric carcinoma is often under a year , from the onset of the first chnical symptoms until death supervenes . chronic gastric ulcer , on the other hand , appears to be relatively benign . 
the importance of this is amply justified in view of the gravity of the problem at issue ; particularly so since the ultimate verdict of malignancy must so frequently depend on a but , apart ' from the fact that no two histologists will microscopical opinion . whollv agree on the evidence which justifies such an opinion , the same pathologist not infrequently changes his criteria on reviewing the same series of specimens after a lapse of years . this , of course , is bound to occur as the result of increasing experience ; yet it means that the findings of an individual pathologist over a lengthy series of cases are only likely to be sufficiently homogeneous for statistical purposes if the time i - nvolved in the assessment of his data is not too lengthy , in terms of his tendency to change his pathological criteria . equally , it means that there is grave statistical objection to " averaging " blindly the data of until pathologists in general are able to come to an different pathologists . agreement to assess their findings on common criteria as to what constitutes malignant change in an ulcer and what differentiates this from a cancer arising de novo , each set of figures must be judged independently on internal statistical criteria , 1 4 . 
the only statistical task then remaining would be that of estimating the frequency of its occurrence . but no such agreement on the microscopical findings and their histological interpretation appears probable as ven amongst the most experienced workers . 
on the contrary , the conflicting evidence and extreme variations in the published pathological data make any attempt at mathematical analysis of them futile . as has already been suggested , the chnical evidence of malignant change in pre - existing gastric ulcer is a relative rarity in the collective experience of both thus , as soon as doubts are cast on the infauibility surgeons ' and pathologists . of histological diagnosis , it would seem that the only logical basis for continued belief in " ulcer - cancer " as a comparatively common entity is the analogy of the causative influence of chronic inflammation on subsequent development of carcinoma elsewhere in the body . such arguments by analogy may , however , be most fallacious , and can directly contravene the famous principle first enunciated by william of occam several centuries ago - " entia non sunt multiplicanda praeter nece88itatem . " the importance of this principle in scientific thought , of which it forms one of the main pillars , arises from the fact that it is impossible in practice to prove a universal negative by inductive processes . 
an example will make this clear . our ancestors , influenced by superstition rather than by scientific method , were constantly inventing ad hoc explanations for things in terms of witches , goblins , evil eyes , fairies and leprechauns which the whole weight of philosophy and christianity has not yet succeeded in completely eradicating . 
the survival of such hypotheses is understandable on the grounds that they are easy to conceive , better than no explanation at all and , once accepted , virtually impossible to disprove . 
and then we shall always be countered by the fellow who is positive he saw several the other night such hypotheses are by their very nature invulnerable . in contrast , the opposite scientific hypothesis that the genu8 leprechaun does not exist , except possibly as a freak of natural development in isolated instancesis extremely vulnerable . indisputable evidence of widespread loprechaun activity will entirely refute it , even if no actual leprechaun can be produced for examination . it is essential that this characteristic be present in any scientific hypothesis , so that the collection of sufficient opposition evidence can establish its falsity . adoption o the null hypothesi8 . applying these basic principles to the problem of " ulcer - cancer , " can it be said that this conception has really been adequately demonstrated clinically , 218 a . 
moroney or have we or even that it forms an essential entity in morbid anatomy perhaps accepted its existence with little more justification than our ancestors had in welcoming the leprechaun ? the very phraseology of the relevant literature - " the incidence of ulcer - cancer probably does not exceed x per cent suggests that this ma be the case , and that pathologists are themselves engaged in an attempt to depreciate its frequency of occurrence . it would seem , therefore , that a more profitable approach to the problem will be to attack it from the opposite direction , by the assumption of a " nufl hypothesis "  . in other words , to investigate the situation on the postulate that ulcer and cancer always occur independently in the stomach , in the aetiological sense , and that their occasional intimate association is entirply a matter of pure chance . failing the demonstration of " ulcer - cancer " as a necessary and unmistakable microscopical entity , such a null hypothesis could still be chanenged by statistical evidence that the relative frequency of occurrence of associated ulcer if the frequency and cancer is significantlv areater than the hypothesis predicts . of such associated lesions is so high that it is unlikely to have arisen by chance , the aetiological connection would be estabhshed , but even then this might only indicate that ulcer is a favoured site for the development of a carcinoma destined however , since it is on the relative frequencies of these to arise ' m any case . lesions that the null hypothesis must stand or fall , it is now important to survey the position statistically . 
and this is best carried out ' m general terms in order to avoid errors present in the conflicting pathological figures , and any profitless mathematical resolution of them . in - such an investigation , general figures of cancer incidence are obviously valueless . 
the only data worthy of consideration are thos ' e which have been verified pathologically , and the analysis must therefore be carried from the population at large up to the point where gastric specimens arrive at the patholoin the statistical model of the situation about to be constructed , it is gist . assumed that the specimens eventually arriving at the pathologist are drawn from a population ' whose characteristics with respect to both gastric ulcer and carcinoma may be regarded as stable over a period of time covered by any particular analysis ; and that , by virtue both of its size and its autogenerative properties , the composition of this population remains substantially unaffected by the withdrawal of the specimens . it will also be assumed that u1cer and cancer occur quite independently . development of the statistical model . in the population postulated therewill . 
i with the frequencies stated , the left - hand compartments of the diagrams representing the pyloric zone and the right - hand ones the lesser curvature ; the two lower sections showing the position with respect to the relative frequencies of double lesions occurring in the same region , compared with double lesions which are sited in separate regions of the stomach . 
we shall refer to such double lesions occurring in the same region of the stomacb as " amalgamated lesions " throughout the remainder of this paper , even if they are actually separate . within this limited selection of the whole data evidence might be found of a tendency for co - existing ulcer and cancer lesions to become amalgamated in this sense more frequently thad predicted by the null hypothesis , on wbicb basis the expected value of the ratio of amalgamat - ed lesions to non - amalgamated lesions is seen from fig . 
moroney the developmaint of a cancer , if not an actual aetiolooical factor in its developit will be - seen that this ratio has the statistical advantage that it does ment . not include the imponderable quantities u and c , but depends only on the site it wfll . 
i gives the expected distribution of an cases of if the null hypothesis is true , ulcer and carcinoma into the various categories . we should expect that a randoni collection of pathological specimens from the population at large would agree with the predicted ratios within the linlits of sampling error . but , of course , pathological specimens are not collected at random , and it is therefore essential to consider in some detail the effect of the selection chain along which patients have to pass before their stomachs become pathological specimens . the first group illustrated in the model shown in fig . 
1 , those cases which have neither ulcer nor cancer , will , of course , be entirely missing from the pathologist 's data . is it likely that ulcer of consider next the two categories of simple ulcer . the pyloric canal will have the same probability of pass ' mg along the reference chain to the pathologist as ulcer at the lesser curve ? prepyloric ulcer , in its uncomplicated form , is notoriously difficult to demonstrate radiologicany but , once diagnosed with certainty , is usually operated on without delay , since so many of these lesions prove eventually to have been malignant since their benign ulcers at this site tend to give rise to early symptoms from the onset . secondary pylorospasm which they cause ; yet they are often undetected until pyloric obstruction supervenes later , as the result of gradual stenosis , or unless acute perforation occurs . 
moroney hand , it is more often inoperable at laparotomy , and therefore is less hkely to reach the pathologist as a specimen . there is thus a complex selection mechanism operating along the whole of the reference chain , from the differential symptomatology in the patient through only after all the medical practitioner or consulting physician to the surgeon . this does the stomach become a potential pathological specimen , the likehhood of which is again govemed by the surgeon 's technical skill , and the influence of this on his decision whether to operate and finally to resect . moreover , still other factors may influence this selection of specimens , which will be different for each pathologist . 
the number of patients with gastric ulcer under observation by the medical side of the hospital wif be one of these , for associated " ulcercancer " lesions will have a better chance of being diagnosed early if the chronic ulcer lesions are kept under continual scrutiny by the consultant physician rather than being referred back to their own farnily doctors for routine treatment . further , the alteration in symptomatology resulting from the development of a secondary cancer in these cases is often relatively smah in the early stages . much depends on the vigilance and diagnostic skill of the physician concerned . the almost universal tendency among reporters is to ignore these very important weightings of their figures , and to hope that in the end they win cancel each other out over a large series . comparison of one series with another - or even the first and second part of the same observer 's series - soon demonstrates that this does not happen . 
the fact is that each pathologist 's series must be considered a unique set , not only because of his particular pathological criteria for " ulcer - cancer " but , perhaps even more , because his experience will include a unique set of weights in the data . introduction of the weighting factors . it is now evident that the simple model shown in fig . 
2 appropriate weighting factors have been introduced , which will take unique values for each individual pathologist in accordance with the varying nature of the particular selection chain along which his specimens have passed . 
the group of the population having neither ulcer nor cancer will be completely absent from such specimens and so will have weight zero . this is the only weight that the data of all pathologists will . 
and w6 , are the weightings for referability of associated ulcer and cancer losions in separate compartments of the same stomach - the pathological data for the frequency of wbich is scanty and its clinical recognition difficult . 
moroney if the individual pathologist could be given this ratio of the phcit values . weiahts concerned , and the values for u and c , he could then calculate the expected values for a and d3 , against which the observed values for these ratios in his own series could be tested . the evaluation of u and c from existin - a fi - aures is , however , rendered impossible by the effect of the reference chain and the different criteria adopted for the boundaries of the various stomach zones , nearly all the pubhshed work on stomach pathology conflicting in this respect . minor differences on the latter score between different series - may be partially taken up in the weights w7 and w8 , since all comparisons wif be intemal ones within each set of individual data , but the question is of academic interest only so long as marked reference chain separate independent research , deliberately designed to eliminate effects persist . moreover , the effect of reference chains , would be necessary for their estimation . even if the individual pathologist was supplied with values for u and c , he would still be unable to determine whether his observed values for a and a differed from the null hypothesis expectation for these ratios . 
the ratio w7 is inherently a property of his own series , representing the effect of the reference chain operating in his particular case . it can thorefore only be determined by using his own observed frequencies for u and c and checking them against those established manifestly , he cannot use his own data through such an independent survey . both to establish the expected value of the expressions d2 and d3 , and then to see if his observed values differ from expectation . 
the position , from the point of view of the individual pathologist , is that significant departures in this respect from the null hyporthesis predictions are inextricably confused with the effect of the reference chain ; and the same applies , even mo ' re , to the ratios a2 and a 35 which are under the influence of the reference chain to a greater extent . its implication is that no pathologist , however competent , and no consensus of opinion among pathologists , however widespread , can refute the null hypothesis on the basis of existing figures . it follows inevitably that the solution to this problem of the incidence of cc ulcer - cancer " must await a research project specifically designed to remove the insuperable obstacle facino , the individual pathologist - the effect of the reference chain represented by the weights w in our analysis . 
the results of such an investigation could then be evaluated by means of the ratios al and dl , which only involve the site ' distribution factors u and c . it would be essential for this purpose to establish some sufficiently accurate convention defining the admittedly , these are not boundaries between the various stomach zones . always easy to demarcate in practice , but the contrivance ot ' some effective standard in this respect ought not to present insuperable difficulties . the most hopeful way of establishing reliable values for u and c would appear to be by planned , clinical research at a number of large centres . the assiduous co - operation of all the local general practitioners surrounding these centres would be an essential , so that every case of a suspected stomach lesion reaches them at the earliest possible moment . 
the research would have to be based on several centres , whose respective findings could finally be checked for statistical homogeneity , and these cent - res ought to be carefully select ' ed . 
they should be situated at large - population centres which are growing , to minimise loss of patients during prolonged observation from drift to other areas ; and in provincial towns rather than in very large cities , where it might be difficult to trace their admission to , or treatment at , a large number of alternative hospitals for a gastric emergency or some intercurrent disease . if the establishment of such centres were practicable , it might be possible to eliminate the reference chain weigbts w for all practical purposes , and thus - trrive at reliable values for the site distribution factors u and c . there are , of course , dangers of leakage in the procedure outlined . in addition to the inevitable loss of some patients during the prolonged observation necessary , there is the certainty that some cases would not reach autopsy . moreover , there will be a fraction of the population who will not seek any medical advice until the disease has progressed too far for any statistical value to be elicited regarding the site diagnosis . this is not the place to discuss the details of such an investigation , but the essential problem regarding such losses is not so much their magnitude as whether they are likely to introduce bias in the determination of u and c . .if unbiased estimates of u and c could be ob - tained in this way , the data collected would suffice to test the null hypothesis expectations . cases with single lesions could be used to provide values for these quantities , and thus for the expected values of al and dl , of a high degree of accuracy deriving from the large number of observations on which they would be based . cases with double lesions would then give an adequate check on such results , using the incidence figures of ulcer and cancer in different stomach zones for this purpose in addition to those of amalgamated lesions in the sa - me zone . 
butler. from the chester beatty research institute , the royal cancer hospital , london , s.w.3. received for publication april 21 , 1951 . the observation of brdicka ( 1933 ) that proteins gave catalytic double waves when added to an ammoniacal cobalt buffer and examined polarographically was soon applied to an examination of the serum proteins , and brdicka ( 1937 ) himself was the first to show that differences could be found in this way between normal and cancerous sera . 
there is no need to relate in detail here the earlier studies on the protein reaction as these have already been adequately reported ( brdicka , 1939 , 1947 ; brdicka , novak and klumpar , 1939 ) , but it will suffice to state briefly that pathological sera after hydrolysis with potassium hydroxide and polarographed in cobaltous buffer show a decreased wave height as compared with normal sera , but after deproteination with sulphosalicylic acid and the filtrates polarographed in cobaltic buffer show an increased wave height . 
brdicka ( 1939 ) found that the latter test , known as the " filtrate test , " was more reliable , but the readings from both tests are dependent on the temperature , and on the characteristics of the dropping mercury electrode . muiller and davis ( 1947 ) introduced an index , known as the " protein index , " derived from the ratio of the two tests multiplied by a constant , which was found to be independent of the temperature and of the capillary characteristics , and also of the age and sex of the subjects . the fact that the polarographic test is not specific for malignancy has been well established and it is therefore of no use diagnostically , but more recent results robinson ( 1948 ) , using the indicate that it may be of value as a prognostic tool . filtrate test , has studied its application in the prognosis of prostate cancers , and has obtained results which are superior to those obtained with the acid phosphatase test normally used for this type of cancer . 
the purpose of the work to be reported below was to gain further information concerning the usefulness of the method , and to compare it with other methods which might be more applicable in general routine . over 100 sera have been examined polarographically , and a smaller number examined by means of the " huggins test " and by the tryptophane - perchloric acid reaction . since the publication by huggins , miller and jensen ( 1949 ) of the " huggins test , " depending on the relative ease of the thermal clotting of serum in the presence of various concentrations of iodoacetate , many workers have investigated its application ( bodansky and mcinnes , 1950 ; homburger , pfeiffer , page , rizzone and benotti , 1950 )  . 
the original authors stated that the " iodoacetate index , " obtained by dividing the highest concentration of iodoacetate in which clotting could still occur by the total protein content of the serum , was lower in 226 l . 
the results obtained from an examination of a limited number of sera by means of the modified method ( huggins , miller and jensen , 1949 , private communication ) are reported below . increases in the polysaccharide content of sera have been observed by a number ofworkers in cases ofmalignancy , tuberculosis , nephrosis , hepatic cirrhosis andpneumonia ( shetlar , foster , kelly , shetlar , bryan and everett , 1949 )  . using the carbazole method seibert , pfaff and seibert ( 1948 ) showed that the globulins ( particularly the a2 - globulin ) contained the most of the protein bound polysaccharide . in an attempt to determine the nature of the polysaccharide seibert and her co - workers ( 1948 ) found that the tryptophane - perchloric acid ( tpa ) test of cohen ( 1944 ) was more useful . using this reaction the authors claimed a correlation between increases in the polysaccharide and increases in the o2 - globulin in cases of tuberculosis and malignancy . moreover , changes in the tpa readings were found in minimal tuberculosis when no change was observed with the carbazole reaction , and it was suggested that this was probably due to the former reaction being more specific although the latter reaction is probably more sensitive . the identity of the polysaccharide involved in the tpa reaction is not known , but only negligible colour formation is obtained with glucose , mannose , galactose and glucosamine , while a positive reaction is obtained with desoxyribose - nucleic acid and fructose . 
a new index was then formulated derived from dividing the value of the filtrate test ( test ii ) by the difference between tests iii and iv and multiplying by ten to bring it to a round number , i.e. , blood index ( b.i. ) = test ( ii ) test ( iii ) test ( iv ) huggins reaction . the modified method ( huggins , miller and jensen , 1949 , private communication ) was used . the iodoacetic acid was recrystallized from a mixture of equal volumes of benzene and 80 - 100 c . 
the contents of the tubes were gently mixed , the tubes covered and heated in a boiling water - bath for 10 minutes . alter cooling quickly they were allowed to stand for 40 minutes and then filtered through a no . 
the upper limit for normal values was fixed at an arbitrary level below which the majority of the normals were grouped ( 21 table i is divided into two groups , and considering the negative , 3 positive )  . cases placed in group ( a ) , it can be seen that 93 per cent gave a positive reaction . 
the former were ( i ) a patient with a 5 years ' history who had been successfully treated by surgery and by androgen , and who was clinically normal at the time the blood sample was taken ; ( ii ) a male case who gave a positive reading 2 weeks later ; and ( iii ) a patient with an advanced tumour who gave a negative reading again 2 weeks later . 
the negative prostate case had already been receiving stilboestrol treatment . these cases show a high correlation with the clinical observations , but group ( b ) of table i gives figures for two malignant groups which appear to give an even chance of positive results . classified in " buccal cavity " are carcinomas of the fauces , palate , tonsil , tongue , mouth , larynx and pharynx , and in " skin " are classified carcinomas of nose and scalp . 
great improvement was observed clinically while under androgen treatment ( after radiotherapy followed by radical mastectomy ) , and the polarographic however , the last five readings , taken readings altered from positive to normal . over a period of eight months , gave positive reactions , although it was only at the time of the last reading that a relapse was clinically observed . in this case , therefore , the relapse was forecast by the polarographic readings . 
youden ( 1950 ) has suggested the use of an index for the comparison of so - called diagnostic methods , which has a value of unity if there are no false positives or false negatives , and a value of zero when the test gives equal proportions of positives for the condition under investigation and the controls . 
the polarographic method gives a value for the index of 0 - 219 , the huggins reaction , 0 - 250 , and the tryptophane - perchloric acid method , 0 - 253 . 
the end - point as described by huggins was not easily determinable , as it was not always obvious what constituted a " well - defined mass . " this difficulty was also noted by bodansky and mcinnes ( 1950 )  . also , the end - point often did not occur within the limits of the recommended iodoacetate concentrations - a problem which presumably would have been overcome by using a larger range of concentrations , making the test much more tedious . 
the results obtained support the conclusions of bodansky and mcinnes ( 1950 ) and of homburger , pfeiffer , page , rizzone and benotti ( 1950 ) , which were reached after a much more intensive study of the reaction than has been attempted here , and it can be stated further that the test is too unreliable to be used in prognosis . the results given in table iii showed that the polarographic readings followed to a very large degree the clinical findings , and it can be stated that within certain limitations this method is useful as a prognostic agent . it can be seen from table i that apart from the two groups of cancers , a high correlation was obtained and the proportion of false negatives was low . there was , in fact , only one case in the negatives shown in table i ( a ) , which remains unexplained , since the prostate case was being treated with stilboestrol , and of the breast patients , one was clinically normal and the other case gave a positive reading two weeks later . this last case supports the view that the serial examination of serum gives far greater information than a single test , a view also supported by brdicka both positive and negative cases should be followed . ( 1947 ) and robinson ( 1948 )  . a persistently positive test or a negative test becoming positive would indicate that the patient requires investigation , a positive test becoming negative indicates that the patient has improved , while a persistently negative test may be misleading ; this last fact is the main weakness of the method . 
excluding tumours of the buccal cavity and skin , which gave an equal chance of giving positive or negative readings , polarographic examination gave a 93 per cent correlation with the clinical diagnosis of malignancy . 
a high correlation with the clinical diagnosis of malignancy was obtained with the tryptophane - perchloric acid test , although it is considered too unspecific to be of use in prognosis . i wish to thank professor e . 
the concentration of aaf in the food was 0.03 per cent for 5 weeks and then 0 - 05 per cent for 20 weeks , the total period of administration extending over 25 weeks from october , 1945 , to april , 1946 . thereafter the mice received the standard diet of rat cubes for the rest of their lives and the control mice received that diet throughout . all mice had an the experiment was terminated in unrestricted - supply of food and water . the eighty - fourth week by killing the mice then surviving , namely 2 males which had eaten aaf and 3 control males . several attempts to control the localization of tumours were made on small during the third to sixth weeks of experiment 5 females of groups of mice . the aaf group and 5 control females were mated with vasectomized males and silk threads were tied in the pseudo - pregnant uterine horns to elicit deciduomata . in the twenty - second week of experiment , pellets containing 25 per cent of diethylstilboestrol ( b.d.h. ) in cholesterol and weighing 5 or 6 mg . 
the stilboestrol pellets shortened life , the testosterone tablets were harmless ; especially by causing pyometra . their possible effect on the induction of bladder tumours is mentioned below . granulation tissue , fibrosis and abscess were found in uterine horns where silk threads were tied but tumours were not recognized there . " spontaneous " tumours were found in 3 male control mice as follows : osteogenic sarcoma of the thigh , with secondary deposits in liver and lungs , in the forty - eighth week ; hepatoma in the sixty - third week ; and lymphoma in the sixty - eighth week . 
the average time was 50.7 weeks , but 8 of the tumours only 1 tumour occurred were found from the thirty - ninth to forty - sixth weeks . in an effective total of 8 mice carrying testosterone tablets ; 6 of the mice survived from 58 to 64 weeks without tumours . 
the incidence as a percentage of the effective total was 12.5 for aaf males with testosterone tablets , 73 - 3 for aaf males without testosterone , and 52 - 2 for all aaf males . most of the tumours were intravesical , pedunculated or sessile papilliferous tumours of transitionalor squamous - cell types , and conformed with the descriptions of armstrong and bonser ( 1944 ) , who distinguished benign and malignant forms but observed no extra - vesical extension . 
the distribution of tumours amongst these and less common sites depends on the species and on the strain of the animals used ( bielschowsky , 1946 , 1947 ; armstrong and bonser , 1947 ; dunning , curtis and madsen , 1947 ; harris , 1947 )  . harris concludes that " the site at which tumours may be induced by fluorene compounds is probably determined by the genetic constitution of the rat employed . " this statement , though true , is not a definitive explanation . 
the genetic constitution determines how particular cells react to particular stimuli ; remains to determine what reactions are iminportant in the production of tumours by acetylaminofluorene and how the reactions are variable in kind or degree . the importance of the genotype is accepted ; the urgent task is to elucidate its phenotypic expression . carcinogenic hydrocarbons affect tissues remote from the site of application and increase the incidence of certain tumours , notably tumours of the breast , long adenomas and leukaemia . 
many observations , summarized recently by enge ] breth - holm and rask - nielsen ( 1947 ) , suggest that the action is , essentially , an acceleration of spontaneous tumour development . 
some actions of acetylaminofluorene may be attributable to acceleration of a spontaneous disease as , for examnple , the increase of mammary tumours recorded by armstrong and in my experiment the evidence for an increase in the naturally high bonser . incidence of breast tumours in r3 mice was not decisive , and acetylaminofluorene did not accelerate or increase the incidence of lymphoma or sarcoma which occur , uncommonly , in normal r3 mice . 
the unequivocal effect of aminofluorene was the growth of tumours of the bladder which are not found in normal controls and which , as yet , have not been induced in mice by other carcinogens ( bonser , 1947 )  . in some strains of rats , acetylaminofluorene notably induces carcinoma of the external auditory canal , previously unrecorded . these and other comparable observations show that tumours induced by acetylaminofluorene do not grow preferentially in tissues prone to develop " spontaneous " tumours and are not accelerated " spontaneous " tumours . 
foulds hepatoma is much less frequent and , as my observations show , develops later than tumours of the bladder by about 20 weeks - a substantial fraction of the life of a mouse . consequently , intercurrent diseases , mammary tumours in females or bladder tumours in males kill most r3 mice before the response of the liver to aminofluorene is manifested by the growth of hepatoma . 
some geneticists maintain that the processes directed by allelomorphic genes differ only in speed . speed of reaction is probably one of the most important expressions of the genetic factors which govern the distribution of the tumours induced by acetylaminofluorene . 
the high and relatively early incidence of mammary tumours in female r3 mice presumably reduces the opportunities for other tumours to become evident , but it does not account for the complete absence of bladder tumours from the females in my experiment , or for the lower incidence in females compared with males in the 5 strains studied by armstrong and bonser . 
tumours of the bladder grew in about half the male mice which survived 9 months or longer from the beginning of the experiment . testosterone seemed to inhibit the induction of bladder tumours in males and none grew in females . 
stern. from the general hospital , northampton . received for publication june 12 , 1954 . although a study of the morbid anatomy of carcinoma of the bronchus can have little bearing on the important problem of etiology , nevertheless any ascertainable facts about this increasingly common disease may contribute something to our knowledge of it . recent comprehensive surveys of the pathology of carcinoma of the bronchus have been made in this country by harrison ( 1950 ) , on 353 confirmed cases seen at st . 
the average age at which death occurred was 56.4 years , slightly higher in males ( 56 - 7 years ) than in females ( 54 - 7 years )  . 
on the other hand both willis and bryson and spencer found metastases in the adrenals much more often than they were discovered ( willis 40 per cent , bryson and spencer 23 per cent , present series in this series . 13 - 7 per cent )  . 
the frequency with which cerebral deposits have been recorded in carcinoma of the bronchus has varied widely with different observers . those who have investigated metastatic tumours in the brain have found that a very high proportion of these had their primary source in the lung . elkington ( 1935 ) , who analysed the records of the national hospital for the period 1918 - 1933 , found that of 72 metastatic cerebral tumours , 24 ( 33 per cent ) originated in the bronchus . 
the highest recorded figure is that of fried and buckley ( 1930 ) , who recognized secondary cerebral deposits in other observers have given much lower figures : reingold , ottoman 41 per cent . and konwaler ( 1950 ) 30 - 5 per cent , willis ( 1952 ) 21 per cent , bonser ( 1934 ) 16 per cent , harrison ( 1950 ) 20 per cent , bryson and spencer ( 1951 ) 17 per cent , simpson ( 1929 ) 13.5 per cent ( in a series of 139 cases ) , kilkuth ( 1925 ) 12 - 6 per cent ( in a series of 246 cases )  . few authors have differentiated between multiple cerebral deposits from carcinoma of the bronchus and large single masses except to say that the former are common and the latter rare , though kilkuth ( 1925 ) reported single masses in 13 of 31 cases with cerebral metastases . although the present series is small it is noteworthy that in 14 cases with cerebral metastases only 6 were multiple and 8 single . 
the multiple deposits were widely distributed and showed no predilection for any particular area of the in all except one of the cases with multiple cerebral metastases there were brain . also secondary deposits in the viscera . 
on examination there was a complete hemiplegia and a dubious hemianosevere neck rigidity was present , but examination of the cerebro - spinal fluid revealed pia . a normal fluid except for pressure , which was 190 mthe only abnormality disclosed by examination of the chest was diminished air entry in the upper zone of the left lung with deviation of the trachea to the lethe differential diagnosis made was betweenr tuberculous encephalitis and cerebral thrombosis . 
death took place 2 days after admission . at post mortem dense fibrous adhesions were found almost completely to obliterate the left pleural cavity . there were old fibrous adhesions at the right apex . 
the trachea and arising from , and producing main bronchi contained a considerable amount of muco - pus . almost complete obstruction of the left upper lobe bronchus was a hard , white tumour , distal to this tumour the lobe was collapsed and contained approximately 5 cacross . a number of irregular cavities filled with thick yellow pus . 
the left lower lobe was studded with a number of nodules of tumour up to 0 ' 5 cacross . in the upper half of the right upper lobe there was an irregular tuberculous focus 2 cacross consisting of a central caseous mass enclosed in dense fibrous tissue . 
her main complaint was loss of weight and a cough of 3 months ' duration , which had been accompanied by a blood - stained sputuon examintion the fundi could not be seen . 
an x - ray showed a mass extending from the left hilum and involving the mid and lower portions of the left upper lobe . the patient died 12 days after admission . at post mortem a large , white , firm tumour mass was found involving the whole of the medial portion of the upper lobe of the left lung . 
no mediastinal glands were infiltrated and no other deposits were found in the viscera . the skull was normal , but attached to the flax cerebri at the vertex of the brain , and pressing on the pre - rolandic portion of the left superior frontal gyrus there was a firm hard tumour the size of a cherry ( proved histologically to be a meningioma )  . the cerebral convolutions were somewhat flattened . 
onimmediate examination a weakness of the left face was noted and there was slow nystagmus on lateral and upward deviation of the eyes . the reflexes were all exaggerated but the plantar responses were flexor . a diagnosis of cerebral tumour was made tentatively , but before further investigations could be carried out the patient died suddenly the day after admission . at post mortem a fungating , cauliflower - like growth was found in the upper lobe of the left lung . 
no enlarged mediastinal glands were present . the pelvis showed no evidence of any local or secondary lymphatic involvement from the cervix . the brain was moderately congested and oedematous . the left half of the cerebellum was replaced by a degenerating , cystic tumour . histologically the growth in the lung and the secondary deposit in the cerebellum were found to be an unspecified type of carcinoma of the bronchus . ( sections were not available for personal study . ) chronic bronchitis " and convulsive attacks with loss of consciousness which began a fortnight before admission . six months previously , when he had attended hospital as an out - patient , an x - rayhad been suggestive of bronchial neoplasm , with displacement of the mediastinum to the right side . 
the cerebro - spinal fluid was normal apart from an increased pressure of 250 man x - ray of the chest gave evidence of neoplastic formation in the left hilar region with associated collapse at that base . death occurred 3 days after admission . at post mortem the left lung was found to be collapsed and the left pleural cavity contained about 500 c.c. 
the left main bronchus was compressed by a soft , buff - coloured tumour , about 8 cin diameter , which was covered by a layer of lung 2 cm . this layer of lung was relatively airless and thick yellow pus was expressed from the thick . the oesophagus and aorta were displaced posteriorly by the tumour . 
46 on account of frontal headaches , throbbing in character and especially severe in the mornings , which had been present for 3 weeks . just before admission much nausea and vomiting had developed . there had been no cough at any time . 
the arm and leg sides . reflexes were normal , but some past pointing was noted in the right arlumbar puncture gave a yellow fluid under 300 mof pressure . the protein was increased to 120 mg . 
the patient deteriorated rapidly and died 3 weeks after admission . at post mortem a hard , white tumour , 1 in diameter , was present at the apex of the right lung . 
no abnormalities were found in the abdomen . in the brain there was a secondary deposit , just over 1 in diameter , deep in the left temporo - parietal lobe . the mass impinged on the left lateral ventricle , which was slightly dilated . 
a mixed type of types of cells encountered in these tumours were : alveolar cells and oat cells , 4 cases ; alveolar cells and polygonal cells , 2 cases ; and one case each of spheroidal cells and squamous cells ; polygonal cells and oat cells ;  . 
it seemed likely that 1131 would prove so since it is specifically concentrated in the thyroid , whose cells are thereby submitted to a course of ~ - ray irradiation . 
the problem is important , sirice we do not yet know the carcinogenic hazard of 1131 in clinical medicine , where it is being increasingly used both tracer and therapeutic doses . 
hyperplasia and adenomas of the thyroid have been produced by goitro gens ( griesbach , kennedy and purves , 1945 ) , and by goitrogens together with the carcinogen acetylaminofluorene ( a.a.f. ) ( bielschowsky , 1944 )  . 
when the following work was started in february , 1948 , there were discrepancies in the literature as to the incidence of thyroid tumours in untreated rats and the carcinogenic potencies of goitrogens , which were due to the different rat strains , ages and living conditions , times of application of the in view of the discrepancies and in order drugs and criteria of malignancy used . 
the rats were killed by coal gas_ at an average age of 15 months , having had treatment for an average of 13 months ( including the rest period )  . 
the trachea and thyroid attached was fixed in helly 's fluid ; the thyroid was then dissected off the trachea and weighed to the nearest milligra the thyroids were embedded in wax , serially cut at 5 and mounted on to slides as ribbons of 8 to 14 sections , including both lobes . 
the number of rats used was 98 to obtain data for the main experiment , at the end of which the remaining 15 from various groups were put aside for study of the thyroid ! 131 uptake by direct measurement and autoradiography . 
 the indication of adenomas by plus signs in tables i , ii , iii , iv and v is not devised to be any more than a crude indication of tumour incidence ; the object was to seek for major rather than minor differences resulting from the various treatments of these small numbers of rats . 
 i have not given a detailed description of the histology and histogenesis of the adenomas , because in addition to the references cited in the introduction , there have appeared further detailed illustrated descriptions by purves and griesbach ( 1947 ) , money and rawson ( 1947 ) , laqueur ( 1949 ) , and hall and bielschowsky ( 1949 )  . 
 nil + + + + + + + + + nil female * number of months before the rats were killed when they received the first of their two injections + represents i adenoma per gland ; + + , 2 or 3 adenomas ; + + + , multiple adenomas . 
in many areas it was difficult to differentiate the adenomas , and the number of plus signs awarded in the thyroid adenoma column of table ii is probably an underestimate . 
however , the cells of these extra and intracapsular and juxta - venous follicles were quite innocent in appear ance , and in no way different from those constituting the main mass of the glands . 
the effect of the 1131 was such that every one of the glands in this admittedly small group showed a most striking increase in adenoma formation as compared with the rats treated with methylthiouracil alone . 
 female male 10 14 14 14 14 17 11 11 14 14 14 15 14 14 14 11 12 12 11 11 died killed died killed died kiiied di~d killed di~ died killed died killed 229 thyroid adenomas . 
 100 168 100 129 136 116 120 160 125 130 110 125 130 155 110 120 130 125 140 130 175 117 119 125 120 108 124 107 acetylaminofluorene + methylthi , ouracil + radioactive iodine . 
 the adenomas were larger in size as well as increased in number , and showed evidence of malignancy by a gross increase in size and by dissemination outside the thyroid in two instances . 
secondly , as shown by autoradiography ( leblond and gross , 1948 ; doniach and pelc , 1949 ) , there is a wide variation in concentration from follic ] e to follicle ; the peripheral follicles in the rat take up considerably less iodine than the central ones . 
the radiation effect~ are due mostly to radiation , since most of the y rays , which are much more penetrating , will not be absorbed in the small thyroid of the rat . 
they found that this radiation did not interfere at all with the ability of the thyroids to take up further iodine , produced no histological changes , and showed no alteration of thyroid function as gauged by various physiological tests . 
their rats averaged 40 per cent maximal uptake of psi , ours was nearer 20 per cent , and our total psi injected was 32 , theirs was 30 c . , therefore our dosage was roughly 15 , 000 roentgen equivalents physical . 
from the long - term view in our experiments this dosage proved damaging , as shown in table vi , where it can be seen that the thyroid weights of all psi treated rats in all groups was one - half to one - third of their respective controls . 
clearly though , enough thyroid had survived to maintain normal growth of the rats , since the body - weights did not differ from their respective controls in spite of the fact that the first dose of psi was administered at an average age of 2 months . 
methylthiouracil rat killed 12 days after cessation of 13 months ' treatment , showing intense blackening over t , he colloid of the normal follicles and less intense but definite blackening over the colloid secreted by the adenoma lying in the centre of the photomicrograph . 
this is the accepted mechanism for the goitrogenic action of anti thyroid " drugs , such as thiouracil ( astwood , sullivan , bissell and tyslowitz , 1943 ; mackenzie and mackenzie , 1943 )  . 
nevertheless , this nodular hyperplasia must be regarded as a definite deviation from the normal , akin to tumour production both on morphology , and on the grounds that it may lead to malignant change as shown by previous and the present work . 
this may well be due to the fact that the dosage of pat used was destructive enough to the thyroid temporarily to diminish thyroxine formation , and thus step up thyrotrophic hormone production . 
it is interesting to note in this connection that the same number of rats showed adenomas in the pat group ( table ii ) as in the methyl thiouracil group ( table iii ) , and that the number of adenomas was greater in the former group . 
 the problem remains as to why the controls show an occasional deviation from the normal in the formation of adenomata , and how does prolonged excessive thyroid stimulation by the pituitary intensify this deviation , and by what means additional carcinogen leads to a further increase in adenomas . 
experimentally , gorb man ( 1947 ) found hyperplastic thyroid tissue within the lumens of pulmonary vessels of chronically thiouracil treated mice as well as parenchymatous pul monary deposits considered to be probably thyroid in orig yet a return to normal diet after prolonged goitrogen treatment was followed by involution of the supposedly cancerous thyroids . 
one may assume , therefore , that two types of metastatic thyroid tissue exist , one , possibly resulting from a mechanical breakaway , still dependent upon thyrotrophic hormone for its survival , the other independent . 
neverthe less , from the host 's point of view the first type of metastasis may prove just as embarrassing as the second , so long as thyrotrophic hormone stimulation is main tained . 
prolonged thyroxine treatment , used in clinical medicine in the therapy of nodular goitre , may , by inhibiting thyrotrophic hormone production , not only shrink the goitre , but lessen the likelihood of mechanical production of thyroid metastases and of their survival . 
the radioactive iodine was found to significantly increase the formation of thyroid adenomas as compared with non ! 1 31 treated controls in the following groups : those treated with ! 131 alone , those treated with methylthiouracil and those treated with methylthiouracil plus acetylaminofl.uorene. 
3 , and the cancer re8earch laboratories , department cf pathology , the medical sclwol , birmingham , 15 . received for publication may 28 , 1952 . the experiments recorded in this article were carried out in the course of investigations on behalf of the medical research council , a sub - committee having been set up in 1949 to inquire into the careinogeiuc properties of mineral oils and allied products . 
the arrangements for co - ordinating the research have been briefly described by auld ( 1950 )  . the entire series of tests have been made in duphcate at the cancer research laboratories , department of pathology , university of birmingham , and at , the chester beatty research institute , the royal cancer hospital , london . 
at each centre the activity of 3 selected crude oils 4 fractions derived from each crude by methods of distiration specially designed to avoid high temperature cracking , and the final residues , have been tested on groups of 50 mice for each sample and also on a total of 105 rabbits . 
he had already shown ( berenblum , 1945a ) that tumours were readily elicited on the rabbit by 9 : 10 - dimethyl - i : 2 - benzanthraceiie , which was found to be more potent to rabbits than to rats or guinea - pigs , in which positive results were , however , obtained ( berenblum , 1945b )  . 
he also subsequently observed ( 1947 ) that this hyd - r - ocarbon when injected subcutaneously did not induce rabbit tumours , tbough rats and guinea - pigs responded by this method . 
much earlier , oberling , sannie ' , guerin and guerin ( 1937 ) had shown that a i per cent solution of 3 : 4 - benzpyrene in benzene was active on rabbits ' skins , and berenblum ( 1945a ) observed that 9 : 10 - dimethyl - i : 2 - benzanthracene was much more active than benzpyrene at a similar ( o 5 per cent ) concentration . experiments using a high boiling fraction of mineral oil from an experimental catalytic cracking operatiori have recently been carried out by smith , sunderland and sugiura ( 1951 ) , testing the residue after removing the lower boiling naphtha and li - aht aas oil cuts , upon mice , rats , guinea - pigs , rabbits and rhesus monkeys . the rats and guinea - pigs were found to be refractory to skin applications but papillomata were elicited in all of the 6 monkeys , 2 being proved cancerous by papillomata were produced on biopsy 4 years after the start of the experiment . the inner surface of the ears of the 21 rabbits within 100 days . 
the number and size of such growths tended to increase during the 2 years in which painting was continued , and in 3 of the 6 surviving animals cancerous changes in the growths for tests on the type of material which they intended to study , were observed . namely , samples containing oils which had been subjected to a process of fluid catalysis up to 950 ' f . 
at birminorham they were selected , 25 of each sex froni an outbred laboratory albino strain previously employed in grading a series of oil fractions ( woodhouse and irwin , 1950 )  . in london the mice used were from laboratory stocks randomised so that each group of 50 contained some of each colour and genetic constitution . 
they were housed in fairly small cages of usual type and fed on greens alternated with crushed oats and a little bran . applications of the oils to patches of skin about 3 csquare from which the hair had been removed by electric clippers were made twice weekly . six areas on each of 30 animals were used for testing the 3 crudes , and 75 animals were used for the 15 derived fractions employing 7 areas on each animal . 
the 6 areas comprised the 2 ears , left and right thoracic , and the left and right lateral abdominal . the seventh area was the inter - scapular reorion . these sites are shown in fig . 
irwin ( medical research council 's statistical research unit , university of london ) , so that a statistical evaluation of the effects of site variation and differences in response by the individual animals might be possible . it will be apparent that each crude was applied to 60 sites and each of the other fractions to 35 sites . appheations were made twice weekly using approximately 0 3 ml . 
woodhouse in contrast , there was a total of 61 tumour - bearing rabbit sites in the birmingham series and 39 in the london series out of a possible 705 sites in each case , or , excluding the crudes and residues , which altogether yielded only 4 tumours ( london series ) , the remaining 12 fractions produced 61 and 35 tumours in the birmingham and london sen ' es respectively on a possible 420 sites . 
the addition of methionine to the basal diet affords good protection against fatty cystine is not as livers and the health of the animals was much improved . reliable as methionine in this respect , probably on account of its toxic action ( curtis and newburgh , 1927 ) , and the growth rates of the animals in the cystinesupplemented diet show considerably more variation than those of the animals on the basal and methionine - supplemented diets . in experiments on the growth - inhibitory action of 1 : 2 : 5 : 6 - dibenzanthracene in rats maintained on a 5 per cent protein diet it was noticed that the treated animals had fatty livers . this 5 per cent protein diet ( for composition see table ii ) contained considerably less fat than the white basal diet , and the control animals maintained on it did not develop fatty livers during the course of the experiment ( up to 56 days )  . although combination of the hydrocarbon with essential sulphur - containing amino acids has been shown not to be a direct cause of its growth - inhibitory action , it was considered possible that on the very low ( 5 per cent ) protein diet such a combination might be sufficient to prevent the lipotropic action of these amino - acids , and thus result in the development of fatty livers . 
 - in the present investigation it has been found that the addition of cystine or methionine to the basal diet without incorporation of the growth inhibitory hydrocarbon brings about an increase in growth rate of the animal ; hence if the effect of this addition is also to negative the growth - inhibiting action of added hydrocarbon , the resultant growth rate should be greater than that produced by the basal diet alone , which , on white 's results , is not the case . the white basal diet is a very poor diet for maintaining the health of the animals , and a number of deaths occurred after a few weeks . 
campbell. from the poultry research centre at the university of edinburgh and from the royal ( dick ) veterinary college , edinburgh . received for publication february 17 , 1949 . in july , 1944 , during the course of a long - term investigation into avian neoplastic disease , a post - mortem examination of a duck showed it to have multiple liver tumours . unfortunately , this case was not seen personally and no record was kept of any details apart from the sex of the subject - a female . however , material was taken for histological examination and a diagnosis was later made of liver - cell carcinoma . primary cancer of the liver is known to occur in chickens , but is relatively uncommon . 
two of these sources provided 3 cases each , a third provided 4 cases ( one of which was not seen personally ) , and a fourth flock provided 8 cases from a flock of 12 ducks . 
one of the latter cases ( case 17 ) had 2 different simultaneous neoplastic conditions , namely a large thoracic histiocytic - sarcoma of undetermined origin , and a much smaller hepatoma . prior to the first observed case in 1944 a total of 21 ducks had been examined in 4 years , and no case of neoplastic disease was encountered . 
no information was obtained regarding the 2 rema several birds suffering from this condition have been examined alive , and in the later stages of the disease the symptoms are very characteristic . there is usuary a history of loss of appetite and of lethargy . 
as the disease progresses , general weakness brings about the loss of locomotory power , and death superv - enes either suddenly from an internal haemorrhage , or slowly from cachexia and exhaustion . if examined during this late stage , a dropsical condition of the abdomen is apparent , and careful palpation shows the prewnee of an enlarged nodular liver projecting wer beyond the caudal extremity of the stemum on the floor of the abdomen . 
usuary one lobe is mainly involved , but there is no definite predilection for right or left ical caw , the fiver tumours are nodular and bright green in colour lobe . 
ina and covered with a tense glistening membrane containing ramifying vessels . other tumours may take the form of firm , cream - coloured nodules , probably reprewnting more recent growths not yet stained with bile . haemorrhagic or necrotic nodules are not uncommon . 
these trabeculae may merge towards the centre of the tumourous lobe to form a broad , well - defined " tnmk " from which the trabeculae radiate outwards like branches wig . 
the liver cells forming these structur ' es - are cuboidal , columnar , or polyhydral with a faintly granular eosinophilic cytoplasm ; they contain a rather small , well defined nucleus , 3 - 4 [ l . 
the nuclei of those cells forming tubules are often situated ceiitrally or adjacent to the lumen . there may be attempts at the formation of a central vein and the cells immediately apposed to the endothelium are connective tissue divides the tumour into irregular usually bolumnar in form . lobules and contains numerous aberrant bile ducts . at the other extreme is the anaplastic type , which is characterized by an almost complete loss of differentiation towards a glandular structure . 
the cells are large and polymorphic with vesicular nuclei varying greatly in size and shape , some exhibiting hyper - chromatisand containing i to as many as 10 typical measurements for such cells are , prominent eosinophilic nucleoli . nucleus 13 - 6 [ l . 
the cells are fi - equently columnar and in such cases the nuclei are usuary situated mitotic figures are common and the proximary , or remote from the lumen . rumour appears to grow mainly by infiltration . 
24 hours old filtrate prepared by grinding up liver tumour tissue in a glass homogenizer , centrifuging , and filtering , using a seitz type filter and ford 's grade g.s. 
a liver fragment and some of the sahne in which it was minced , were placed into broth which - on the fohowing day was found t - o be sterile . on the 20th of the month 2 embrvos were found to be dead . 
of the 5 , 4 had small growths in the membrane - disappointingly smafl considering the cultivation period ( 12 days )  . three of these were removed , dissected awav from the membranes and reimplanted into two ' - d - day - old embrvonated eggs . 
fragments of tissue were immediately implanted into eggs , 4 containing 101 - dav - old embrvos , and i being 9 davs . the eggs were opened 9 davs later ; 4 contained tumours . 
the eggs containing the second passage implants were opened 10 davs later , and 3 contained small tumours between 2 - 3 mdiameter . later a further biopsy on case 20 provided material to implant into three 8 - dav embrvonated eggs . 
the bird was then 8 months old . fourteen we ' eks later it was observed to be weak , losing weight , and to have an enlarged abdomen . it was destroyed and examination showed a large liver tumour weig ' hing 280 g . 
the original tumour was from duck case 18 . on the 3rd day i chicken was found in a dying condition and was kired . the pectoral muscle contained a smar greenish - brown growth which was taken for this was approximately 66 hours subsequent to injection . 
10 shows the same tumour - bearing membrane photographed aaainst a white background , and the lesions are then barely perceptible . upon histological examination , an interesting picture is revealed . 
yolk - sac cultivation did not give satisfact - ory results , this also being the experience of twombly and meisel ( 1946 ) ; although taylor , thacker and p nini ( 1942 ) , and several other workers claimed a high perentage of intraviteuine growths with the particular tumours these were mainly mouse and rat mam iary carcinomata , and the poor used . results obtained by others , using different tumours , seems to indicate that the environ.ment provided by the chick embryo yolk - sac is pecuharly suitable for the metabolic requirements of mam lary cancer cells . on the other hand , most of the tumours implanted on the chorioallantois 208 j . 
the sudden occurrence of a number of cases of hitherto unrecorded primary carcinoma of the duck 's liver provided material for cultivation by various methods , with the main object of searching for a transmissible factor or virus . 
the chorioallantoic method of cultivation , therefore , seemed particularly suitable , and was extensively used . there appear to be two possible explanations of the etiology of this condition . firstly , the disease might be associated with a transmissible factor . 
 ' it is known that the mouse mammary cancer factor of bittner is transmitted from mother to offspring by the milk , and this is one of the very few known instances of a tumour of epithelial nature associated with a virus - like principle . it was felt that the duck liver carcinoma might also contain a factor transmissible probably via the egg , which might be capable of propagation in the same manner as the milk factor of mice . experiments designecl to test this theory , however , have given negative results as far as transmission by cell - free material is concerned . 
but the sui - vival of these heterologous grafts for at le - ast 6 davs in the muscle and peritoneum of chick - ens is rather remarkable . the second possible explanation of this apparent outbreak of liver cancer , is a genetic one . 
a complete circuit of the vascular svstem throu h the pulmonarv circulation and so to the spleen t - ia the splenic arterv . in the one case encountered in the duck , pulmonarv metastases occurred , and once the lungs are involved so this second hypothesis mav be the correct one . tumour cells or emboli could then the tumours there mav also metastasize reach the spleen without much diffieultv . 
a direct spread t - ia the lungs seems iinlikelv in view of the formidable barrier offered bv the pulmonarv capillaries . fox and bartels ( 1928 ) favour the niew that in the human subject the spleen and mesenteric veins mav be invacled bv retrogtade extension along the portal in case 6 , besides seros - al implantation on the wall of the int - estine , tumour vein . emboli were found within the veins of the gut wall . 
greenwood 's flock of brown - legliorns , and i have pleasure in recording niy appreciation of iiis co - operation iii this respect , and for much help in otlier directions . the histological preparations are the work of messrs . 
whitfield jarcho ( i936 ) also states : has often biased the clinician in favour of a purely haematological diagnosis . despite the frequent difficulties in chnical diagnosis the primary growth and / or its metastases were always readily visible at autopsy . jarcho ( 1936 ) stated that many patients dying from mahgnant thrombocytopenic purpura also showed lymphangitic carcinomatosis of the lungs althou - ah histological examination was often necessary to demonstrate its presence . 
he adopted the term " diffusely infiltrating carcinoma " to cover both mahgnant purpura and lymphangitic carcinomatosis of the lungs , suggesting that they were manifestations of the same disease process . 
on boxing day , 1952 , she noticed profuse painless haematuria which lasted for 19 days . investigation showed no casts in the urine , a normal blood urea and normal intravenous and retrograde pyelograms . 
the urine contained a few red cells , polymorphs and cohform bacilli . hess 's test was negative , the bleeding and clotting times were normal and the prothrombin was 100 per cent . there were 2 , 180 , 000 red cells , 46 per cent haemo lobin , 5 , 000 white cells and a again there was normal differential count . 
no cause for the purpura had been found during life . po - st - mortem finding8 . there were many skin ecchymoses over the legs , thighs and arms , some of which extended deeply into the underlying tissues . there were petechial haemorrhages on the posterior third of the tongue and soft palate . 
the left breast and axilla were normal . the pleural surfaces of the lung8 were normal . their cut surfaces were unusually bloodless , firm in texture and grey in colour . these gross appearances suggested diffuse pulmonary fibrosis . there was no evidence of carcinomatous infiltration . 
the hilar lymph node8 were enlarged and firm and their cut surfaces in view of the previous history showed several tiny grey homogeneous areas . of breast carcinoma a frozen section was prepared from one of these glands . it showed secondary polyhedral - celled carcinoma consistent with a primary origin in the breast . these nodes were not adherent to the hilar blood vessels which were normal in all respects . 
two similar para - tracheal lymph nodes were found i cinferior to the thyroid gland . the upper 12 cof both femoral shafts contained pink marrow which sank in water and which on close inspection was flecked with several pale homogeneous foci measuriaig 1 - 2 min diameter . there was absorption ofthe bony trabeculae . a smear prepared from this marrow showed irregular clumps of malignant cells . the rest of the marrow was fatty . immediately inferior to the left lesser trochanter was a smooth walled cyst 2 x i cdiameter . 
the femoral marrow would have been accepted as showing hyperplasia and a simple cyst resulting from previous haemorrhage if carcinomatous deposits in the pulmonary lymph nodes had not been confirmed histologically earlier in the course of the autopsy . the 8ternum showed hyperplasia of red marrow and absorption of tlle bony trabeculae . the brain showed symmetrical swelling of both frontal lobes and bilateral sectioning revealed extensive tentorial hemiations . iiitracerebral haemorrhages involving the white matter dorsal ancl anterior to the genu of the bilateral 100 w . 
whitfield corpus callosuthe haemorrhages extended backwards on both sides as far as the post - central gyrus , becoming continuous at this level by involvement of the body of the corpus callosuboth lateral ventricles contained recent bloodclot . 
the basal gangha , brain - stem , cerebellum , venous sinuses and pituitary showed no macroseopical changes apart from occasional petechial haemorrhages . the vessels of the circle of wilhs and their major branches showed no evidence of embolism or thrombosis . the thyroid was small , hard , had an irregularly scarred outer surface and showed several brownish areas - each 1 - 2 min diameter - on its cut surface . these areas resembled old areas of haemorrhage . 
the gall bladder was normal . several para - aortic lymph nodes felt firm , their cut surfaces were a uniform pinkish - grey colour and were devoid of definite metastatic deposits . the pericardium , heart , skmmch , intestines , spleen , pancreas , suprarenals , urinary bladder , fallopian tubes and ovaries all appeared normal macroscopically . the uterus contained several small intra - mural fibroids . although there had been histological confirmation of secondary deposits in the pulmonary lymph nodes and bone - marrow during the autopsy , it should be emphasised that there was no other definite evidence of gross metastases , despite extensive examination of all viscera . 
the axillary lymph nodes were extensively infiltrated with similar carcinoma . ( 2 ) tissues taken at autopsy . - the pulmonary and right axillary lymph nodes and femoral marrow contained microscopical metastases which resembled the primary tumour morphologically . the abdominal lymph nodes , thyroid and posterior lobe of pituitary showed scanty microscopical metastases nevertheless still identifiable with the primary growth . 
the above tissues also showed intra - vascular carcinomatous einboli , which had not effected extra - vasc - ular extension . all other post - mortem material examined showed numerous intra - vascular , micro - emboli composed of compact clumps of polyhedral carcinoma cells devoid of stroma . 
the cells were cytologically identical with those which constituted the primary tumour , but because of the minute size of the emboli the general pattem of the primary was lacking . 
the renal tubules contained red blood cells or occasional clumps of tumour cells - " tumour casts . " intracapillary carcinoma plugs were seen in the dermi8and8ub - cutaneousfat in sections prepared from areas of skin ecchymoses . 
the post - operative history of the case may be explained in two ways . either ( 1 ) viable carcinoma cells survived in unextirpated glands or other sites of pre - operative metastasis during the major part of the long period of apparent surgical cure , and only later - perhaps related in time to the onset of purpura 6 months before deathgained access to the general circulation by venous invasion , or ( 2 ) a degree of intra - vascular dissemination was also present since the original operation , but for 71 years had not resu - ited in manifest embolic phenomena . 
the lung was the main exception to this statewidespread intra - vascular deposits , in places apparently resulting in ment . complete occlusion , had not given r ' ise to obvious symptoms or signs during life , even though cardio - respiratory manifestations arising on this basis are well recognised ( jarcho 1936 , storstein 1951 )  . neither did the lung show histological evidence of embolic phenomena . carcinoma cells had undoubtedly passed through the pulmonary vascular bed and into the systemic circulation without interruption or the formation of metastases . thik ; is a rare phenomenon and is discussed in detail by wilhs ( i 952 , page 45 )  . 
the experimental evidence of zeidman and buss ( i952 ) suggests that the transpulmonary passage of tumour emboli may occur more commonly than was previously supposed . the reason for the absence of the usual type of gross metastases in this patient is unknown . 
the fact that all organs examined showed tumour emboli , often in large numbers , does not support the view of coman ( 1953 ) that the distribution of metastases i 's dependant upon the number of embohc cells reaching the various factors other than the frequency - distribution of tumour cells appear to organs . have played a part in our case . 
the ancestral neoplastic cells constituting the primary growth clearly possessed infiltrative propensities . unless the intra - vascular descendants of these cehs had lost these inherent aggressive characteristics - and the presence of mitoses , lack of degenerative changes and the scanty but nevertheless definite microscopical foci of extravascular infiltration that were found does not support this view - one is left to assume that the unusual behaviour of this neoplasm resulted from a lack of the host stromal response which is such an essential factor in successful metastasisation . 
the possibility that " stroma - inducing " properties of the tumour cells were lacking , cannot of course be excluded by histological criteria . it is repolted ( willis , 1952 , page 272 ) that carcinoma of the breast produces intra - thyroid metastases in about 20 per cent of cases . it has also been show - n ( wilhs , 1931b ) that pre - existing abnormahties in the gland were prominent in these findings favour the cases of carcinoma showing intra - thyroid deposits . view that the associated chronic non - specific thyroiditis in our case , preceded the secondary deposits . in a recent paper describing four cases of sub - acute cerebellar degeneration occurring in association with carcinoma elsewhere in the body , brain , daniel and greenfield ( 1951 ) recorded non - specific thyroid changes in one of their patients , similar to those found in our patient . 
the status of the thyroid gland in carcinomatosis seems to merit further investigation . it will depend upon the results of such studies as to whether relationship can be seen between the thyroid changes and the unusual features of our case . the presenting symptoms of haematuria and skin purpura were related to the presence of tumour emboli in the skin and glomerular capillaries . 
haematological investigations during the life failed to elucidate any other aetiological vascular changes in the skin in malignant disease have recently been factors . described ( forman 1952 ) and may have contributed to the skin lesions shown by our p ' atient . the terminal acute massive cerebral haemorrhage may have resulted from the rupture of a small degenerative blood vessel traversing a pre - haemorrhagic focus of softening , a mechanism postulated by globus ( 1937 ) and further substantiated by globus and epstein ( 1953 )  . 
the presence of embohc phenomena elsewhere in the body , the unusual distribution of the effused blood , and the absence of cerebro - vascular disease excluded the possibility that this wa - s a coincident haemorrhage of the classical spontaneous variety . 
madow and alpers ( 1952 ) have described a case of cerebral softening due to multiple cerebral carcinomatous emboli , the primary tumour being a squamous carcinoma of bronchus . as in our case there were no macroseopical cerebral deposits but other visceral metastases were however abundant . 
the above authors also refer to three previously recorded cases of cerebral softening resulting from blood - bome cerebral lesions due to massive neoplastic embohsm carcinomatous emboli . are reviewed by till and fairbum ( 1947 )  . 
the petechial haemorrhages , microscopical softeiiings and focal demylination in the cerebral white matter of our patient resembled experimental lesions produced by the injection of calibrated paraffin emboli ( swank and hain , 1952 ) and sterile cod - liver oil ( lumsden , 1950 ) into the cerebral circulation . cerebellar degeneration ( brain et al . , 1951 ) and peripheral neuritis ( dennybrown , 1948 ) occurring in association with carcinoma elsewhere in the body have been described . 
the changes in the cerebellum and peripheral nerves of our case bear only a superficial resemblance to the lesions described in the above reports as they were focal , associated with carcinomatous emboli and did not include systematised tract degeneration as furthermore , in our case - apart from the terminal far as we could ascertain . apoplexy - the neurological lesions gave rise to no definite symptoms or signs . the platelet thrombosis syndrome ( " thrombotic microangiopathic haemolytic anaemia " ) has recently been reviewed by symmers ( 1952 ) , who states that this condition was first described by moschowitz ( 1924 )  . 
the neurohistological lesions in this syndrome were described by adams , cammermeyer and fitzgerald ( 1948 ) and are easily differentiated from those noted in our case by the presence of platelet thrombi , endothelial and probably adventitial hyperplasia in the walls of the involved vessels and less severe damage to the neural thrombocytopenia is usually present both in previously recorded cases tissue . of malignant purpura and in the platelet thrombosis syndrome . 
at autopsy gross metastases were not present and yet histology revealed intravascular carcinoma in the liver , lungs , one suprarenal , lymph nodes , bone - marrow and dura - mater . 
the degree of intra - vascular spread noted both in oertel 's and our own cases leads us to suggest that a search for carcinoma cells in marrow , skin or muscle biopsies and perhaps in urine , sputum or even blood specimens may be of diagnostic value in suspected cases of intra - vascular carcinomatosis either associated with an occult primary growth or occurring after radical excision such investigations may also help in differentiating the of a known primary . condition from the platelet thrombosis syndrome . 
we feel that even though features such as thrombocytopenia were present , tumour emboli may have been a factor in the mechanism of the purpura in these cases . the evidence that we have presented shows that our patient finauy died from the mechanical effects of tumour emboli that had not resulted in macroscopical metastases , and also that carcinoma cers may have existed " commensary " i the blood stream for many years . 
the patient died from massive intracerebral detailed histological examination estabhshed that the purpura haemorrhage . it is suggested that resulted from the effects of blood - bome carcinoma emboli . carcinoma cells may have existed in the blood stream since the original operation and that similar embohsation may also play some part in the mechanism of malignant purpura . 
the clinical picture of this case is compared with that of the platelet thrombosis syndrome . neurological lesions were present and are discussed in relation to previously recorded cases that show points of similarity . we wish to express our gratitude to professor w . 
whittick. from the department of pathology , royal cancer hospital , london . received for publication december 13 , 1952 . there is an astonishing neglect in the literature of the benign cutaneous condition described by maccormac and scarff in 1936 , and named by them molluscum sebaceuan alternative name , kerato - acanthoma , has since been applied , and this has the merit of preventing confusion with molluscum contagiosum , an unrelated condition . it has been the subject of only 4 papers , all by british authors , maccormac and scarff ( 1936 ) , musso and gordon ( 1950 ) , rook and whimster ( 1950 ) and beare ( 1953 ) , and does not yet appear to have reached text - books of dermatology or pathology . that this in no way reflects the incidence of molluscum sebaceum is certain . indeed , it is not an uncommon condition , and is still very frequently misdiagnosed as squamous - cell carcinoma by both dermatologist and pathologist . smith , in 1934 , described the occurrence in a young man of multiple primary squamous - cell carcinomas of the skin which healed spontaneously and he was unable to find any comparable case in the literature . since that time there have been eight papers on the subject ( table ii ) with descriptions of similar lesions in 11 patients . comparison of the clinical and pathological descriptions of these cases with the natural history and the structure of molluscum sebaceum at once suggests the probability that all the recorded cases of spontaneously healing epithelioma of the skin are in fact instances of molluscum sebaceum . the following account is based on a series of 7 cases of molluscum sebaceum which after biopsy diagnosis were untreated and allowed to run their natural course to spontaneous regression . 
whittick that the lesion of molluscum sebaceum closely simulates highly differentiated squamous carcinoma will be apparent from the histological description and illustrations . there is no single feature which will allow differentiation . 
about this central plug of keratin is a broad , dull red , convex and smooth - surfaced epidermal riwith regression there is gradual flattening of the lesion , and finally the keratin plug falls off to leave a clean , slightly depressed scar . ordinary squamous carcinoma usually has a much slower rate of growth with progressive increase in size for several months . although rapid growth may occur , it is usually accompanied by early involvement of the regional lymph that rapidity of growth has not been accompanied by metastasis to the glands . local lymph nodes in the spontaneously regressing cases has indeed been stressed by some of the authors . 
whittick local and lymphatic spread . were the alleged cases of spontaneously healing epithelioma true instances of squamous carcinoma there should be good evidence of local destructive invasion and lymphatic extension , but this is lacking . in over half the recorded cases the regional glands are not mentioned and , in view of the long survival period in these cases , it may reasonably be presumed that they were not involved . example in smith 's ( 1948 ) case 1 there is a history of lesions for 21 years and in his case 2 for 29 years . 
lack of lymphatic involvement was mentioned by dunn and smith ( 1934 ) , and grzybowski ( 1950 ) comments on " the lack of involvement of lymph nodes in spite of the 9 years ' duration of in only one case , charteris ' second ( charteris , 1951 ) , is enlargethe disease . " ment of lymphatic glands mentioned , and these were found , histologically , to be tumour - free . local invasion , too , appears to have been very limited in the spontaneously healing cases , being restricted to local penetration into the dermis . thus , dunn and smith ( 1934 ) , " the invasive process at its height never appears to transgress this feature applies equally well to molluscum the limits of the true skin . " description by two authors of local tissue destruction in sponsebaceum . taneously healing epithelioma requires comment . smith ( 1948 ) , when recording the subsequent history of his case 1 , states that he was an irregular attender and " permitted much further destruction of the soft tissues of his face , ' and that he now wore a prosthesis to cover extensive destruction of his nose . this on first reading seems proof of an infiltrating and destructive malignant growth , but it must be pointed out that in the previous paragraph we are told that following treatment of a lesion of the right leg by radium , the same patient had to undergo amputation of his leg because of necrosis of the tibia . lesions of his face had been treated by contact x - ray therapy . if this extensive destruction of the nose , requiring a prosthesis , was indeed due to squamous carcinoma , then the lack of lymphatic extension and the ultimate spontaneous healing ( sic ) make this case even more remarkable . 
chadwin. since completion of this paper two other relevant communications have currie and smith ( 1952 ) , under the title " multiple primary sponappeared . taneous - healing squamous - cell carcinomata of the skin " , describe 2 new cases . they maintain that the lesions they describe are unrelated to molluscum sebaceum . whittle and lyell ( 1952 ) , in commenting on a case of molluscum 'sebaceum which f . 
powell. from the department of experimental pathology , mount vernon hospital , northwood , middlesex . received for publication april 30 , 1951 . in previous communications ( powell , 1944 , 1946a , 1946b , 1947 ) it has been suggested that many of the typical properties of tumour cells can be explained by the occurrence of a derangement of the submicroscopic protein framework it was also suggested that the growth of malignant cells of their protoplasm . might be inhibited by chemical compounds able to link together the ultrastructural protein fibrils of tumour cells , and thus simulate the arrangement of comparable fibrils in normal cells . disulphide bridges constitute one of the more important classes of interconnections between the fibrils of native proteins . 
the quinone was recovered from the fitered bisulphite solution by precipitation with sodium carbonate or sulphuric acid . further purification was carried out by repeated formation of the additive bisulphite compound and subsequent precipitation as above . 
the following transplantable tumours were used : carcinoma 63 , a fibrosarcoma ( ac ) of strong a mice , a spindle cell tumour and a squamous cell carcinoma of cba mice , a rapidly growing undifferentiated sarcoma ( rb ) and a mammary adenocarcinoma of riii mice . the tumours were grafted subcutaneously in the right flanks of the mice , in each experiment the implants being portions taken from one tumour . in each experiment mice with actively growing tumours were divided into groups , control and experimental . 
1. - effect of 1 per cent phenanthraquinone upon the growth of carcinoma 63 in a strain in all the text - figures the horizontally placed numbers indicate days after inoculation , mice . and the concentration of phenanthraquinone in the food is given as a percentage of the combined weights of flour and rat cake powder . the quinone used in this experiment possibly contained a trace of the hot tasting impurity , but treated mice showed no harmful effects from it . 
2 and 3 demonstrate the similarity of the results obtained in different experiments with a particular strain of tumour when the rate of tumour growth is approximately the same , and the concentration of the drug is constant . 
1 , in which the growth of the control tumours is appreciably faster . here , with a higher concentration of the drug , smaller initial sizes and slower intrinsic growth rates of the tumours , the inhibitory effects of the treatment are greater than in c ontrol a . 
the inhibition of several spontaneous mammary tumours of a and riii strains of mice by the quinone was comparable with that of the transplanted tumours . also , the growth of a transplantable mammary adeno . carcinoma of riii mice and a transplantable squamous cell carcinoma of cba mice was strongly inhibited . thus the growth of a variety of different tumours can be inhibited by phenanthraquinone under the conditions described . unpalatable cause loss of weight of the treated animals . samples of phenanthraquinone containing sufficient impurity to make it gastro - enteritis some270 a . 
the latter causes prepared food to be unpalatable , and can give rise , if present in sufficient amount , to gastrobut , by comparing the effects of samples of quinone of varying degrees enteritis . of palatability , it has been established that the purest samples are the least toxic this greater inhibition to mice and inhibit tumour growth to the greatest extent . of tumour growth may be due in part to a greater intake of food , and therefore detailed investigation of the effects of phenanthraquinone upon of quinone . tumours and of its possible value in tumour chemotherapy is dependent upon the preparation of the drug in a pure state . its further purification and alternative methods of synthesis are under investigation . the additive compound of phenanthraquinone with sodium metabisulphite is serial intraperitoneal very readily hydrolyzed in vivo to yield the free quinone . injections in mice of aqueous solutions of the quinone - bisulphite compound in sub - lethal doses at frequent intervals indicate that the liberated quinone is very rapidly metabolized in the body . in view of the rapid destruction of phenanthraquinone in vivo and of the rapid growth rates of many tumours , it is essential that continuous administration of the drug be maintained in order to expose the tumour cells to an effective concentration of the drug for sufficiently long periods . failure to achieve this could permit a proportion of the tumour cells to grow and in the early stages of an experiment cessation of treatment with the divide . quinone may result , in some instances , in stationary tumours recommencing growth . 
on the other hand , similar tumours continually subjected to the action of the quinone fail to grow and often regress completely . in these preliminary experiments the simplest method of ensuring an adequate and continual supply of the quinone , namely , by adding it to the food , was adopted . however , this method is not entirely satisfactory . adequately controlled experiments in which individual mice receive known amounts of quinone at definite times are necessary for detailed studies of the action of the drug . very little of the quinone in a concentration of 1 to 2 per cent in the food ingested by a mouse can be available for action on substrates in tumour cells , since there is a very great disparity between this amount and the lethal dose given as the bisulphite derivative by injection . 
much of the fed quinone may not be absorbed from the food , and the greater part of that reaching the body fluids may be metabolized . sodium salts of the phosphoric and sulphuric acid esters of 9 : 10 - phenanthrahydroquinone have been synthesized and tested for possible inhibitory effects on tumour growth , but they have been found to be unsuitable for the treatment of tumour - bearing mice . 
the former very readily hydrolyzes to give the hydroquinone , which readily oxidizes to the quinone , and the latter is extremely resistant to hydrolysis . preliminary experiments upon the administration of thiol compounds concurrently with phenanthraquinone to tumour - bearing mice appear to indicate that its inhibitory action on tumour the latter reacts with thiol groups in vivo . growth may be due , at least in part , to this effect . 
powell may enable phenanthraquinone to function as an oxidation - reduction catalyst and so disturb the natural oxidation - reduction balance of tumour cells , possibly to a greater extent than that of most normal cells . in view of its considerable chemical reactivity , as well as of its affinity for proteins , phenanthraquinone despite the possibility that would be expected to have multiple effects on cells . phenanthraquinone has in vivo the mode of action postulated earlier , that is , of forming cross - linkages between ultra - structural protein fibrils , it is emphasized that its actual mode of action remains a completely open question . 
the available evidence favours the view that over a certain range of concentration tumour cells are more sensitive than normal cells to the effects of phenanthraquinone . it has been reported by mitchell ( 1948 ) that the combined antimitotic effect of " synkavit " and x - rays is greater than the additive effects of both agents used singly . 
kreyberg. from the institutt for generell og eksperimentell patologi , universitetet i oslo . received for publication april 24 , 1952 . the importance of using pure , inbred strains in cancer research is now generally accepted . strong ( 1942 ) , emphasizing this point , gave a survey of the origin of some of the best known strains , originating from his laboratory . 
the new informal document , mouse news letter , acts as a most valuable source of information as to a great many strains used all over the world . the characteristics of the different strains as to susceptibility to development of spontaneous tumours , reaction to carcingenic agents , as well as susceptibility to transplantation and other biological responses may be very marked and very different . it is therefore of great importance to have a great number of different strains with marked characteristics , in order to supply research workers with the best material possible for their special needs . the purpose of the present paper is to describe the origin , development and some of the features of our strain " white label "  . the first animals were obtained from a commercial dealer in oslo , a young man who used to supply a number of laboratories with albino mice , and who , from time to time , added animals of different origin to his stock . 
the figure shows , however , very clearly how two lines were developing with extreme differences as to the formation of spontaneous mammary carcinomas . " line 27 " produced a high , and an increasingly higher percentage of mammary tumours . 
from f2 and up to and including f14 , when this line became extinct , mammary tumours occurred in every generation , and from fg until f14 16 out of 18 females developed such tumours . from the sister of no . 
2 indicated by an arrow . in the 11 generations ( f5 - f15 ) in which there were 102 females , not a single instance of mammary carcinoma was observed . such was the situation in 1935 . in the following years the brother - to - sister matings were continued and many sidelines died out , or were not continued , but " line 426 " was kept until the war interrupted the experiment at f37 . in table i is given a complete record of the females of all the generations descending from pair ( 2 + 3 ) up to f37 . in the first column is indicated the generation . 
in the second column is given the total number of females in each generation . in the third column is given the number of females belonging to " line 426 " ; from f15 all the females belong to this line , as this is the only line surviving . in the fourth column is given the total number of mammary carcinomas occurring in each generation . finally the 24 columns show the number of animals dying in each month after birth , as well as the occurrence of mammary carcinomas , the figures in brackets . at the bottom of the table the sum total is recorded , as well as the reversed figures , indicating the number of females alive at the end of each month . table i gives a clear picture of the great number of mammary tumours occurring in the first heterozygous generations . 
from f12 it is only " line 27 " which still contributes to the presentation of mammary tumours , and from f14 when this line becomes extinct , only one single mammary tumour occurs ( that is in " line 426 " )  . 
an exception , indicated by a cross , will be mentioned later . this means that " line 426 " , during 34 generations , comprising 1595 females , presents one single case of mammary carcinoma . 
bonser , university of leeds , wrote me in august , 1949 , regarding this question as follows : " i still keep ' white label ' mice in this laboratory . 
by suckling ' white label ' babies on riii mothers i showed that they were susceptible to the riii milk factor , which i regard as a potent factor . never published these experiments , and they were only done on small numbers of mice , but they point strongly to the fact that ' white label ' mice in leeds have the milk factor , and are susceptible to it . " bonser wrote me a further letter in february , 1951 , stating that " mammary cancers still occur in our line and we regard the incidence as being about 30 per cent in mice which live to be 12 months of age or more , but i have not any recent accurate estimate of the mammary cancer incidence , because we have been very short of accommodation lately . addition : " now , in 1952 , we find that 7 of 33 females over 10 months of age have developed mammary cancer , usually rather late in life . but we make no attempt to assess the mammary cancer incidence accurately as we usually dispose of breeding females when they reach the age of one year . " i also had the following information , dated january , 1951 , from w . 
s. bullough : " my experienoe with these mice falls into two periods . first when i was working in the zoology department in leeds and when i obtained the mice from bonser . then mammary carcinoma was common in females of from 11 months of age onwards . i have no figures now , but my recollection is that it developed in not less than 40 per cent of the older females . also there was the odd occurrence in a male , though this was of course rare . " further : " this colony was allowed to die out in 1944 , but in 1946 i obtained two females and a male from bonser and started a new colony in the university of sheffield . since then a colony of some 200 - 300 mice has been maintained . . 
kreyberg further , in 1952 : " the final chapter in the story starts in 1949 when , in the autumn , i took the milk factor out by fostering one family with a strong 's cba female . 
my present colony is entirely derived from this one family , and now mammary cancer is exceedingly rare . so my present stock of your mice indeed i cannot remember when i last had a case . is without the milk factor , and i suppose it is no use for your own present purposes . " i regret very much that i cannot definitely state so , but i have strong reasons to believe that the animals sent to leeds in may , 1934 , were descendants from the pair ( 4 + 5 ) ofmy " white label "  . 
at present one " white label " strain ( leeds ) carries the milk factor and produces about 30 per cent of mammary carcinomas in females reaching the age of 12 months or more . this strain has the characteristics of the branch ( 4 + 5 ) of the original material . 
another " white label " strain ( oslo ) is devoid of the milk factor and produces practically no mammary carcinomas spontaneously . this strain is probably one of the lowest mammary for future references it is therefore of great imcancer strains in existence . therefore portance to distinguish between these two " white label " strains ; the leeds strain will be designated wll and the oslo strain wlo . 
the two strains most probably have only a heterozygous founding mother in common . this experiment has been carried out for more than twenty years . it would not have been possible without the assistance of my collaborator miss hj . 
aasland , who continued the experiment during the first years of the war , until illness and an untimely death ended her devoted and loyal partnership . during the remaining years of the war the strain was maintained at a reduced scale through the initiative and faithful service of e . 
orr. from the department of experimental pathology and cancer research , medical school , university of leeds , and the de7partment of pathology , university of birmingham.. received for publication , april 23 , 1949 . the discovery of the milk factor or mammary tumour agent ( bittner , 1936 ) and the demonstration that three factors , namely , the genetic factor , the hormonal factor , and the milk factor , are essential for the development of spontaneous breast cancer in certain inbred strains of mice ( bittner , 1939 ) , was followed by investigations of the part played by the agent in the induction of breast cancer by oestrogenic hormone . 
lacassagne ( 1939a ) , lacassagne and danysz ( 1939 ) , twombly ( 1939 , 1940 ) , and later bittner ( 1940 , 1941 ) , gardner ( 1941a ) , shimnkin and andervont ( 1941 , 1942 ) , dmochowski and gye ( 19.44 ) , found that fosternursing of low - breast - cancer strain mice by high - breast - cancer strain females increases the incidence of breast cancer in the low - breast - cancer strain mice treated with oestrogenic hormones . 
tlhus male mice do not develop breast cancer , even if they are susceptible and have the mammary tumour agent , unless the hormonal or oestrogenic factor is supplied , and only few or no breast tumours are induced in low - breast - cancer strain mice , i.e. 
it is probable that a quantitative deficiency of any one factor can be overcome by a relative quantitative increase in the other two factors ( shimkin , 1945 )  . the accelerating influence of carcinogenic hydrocarbons on the appearance of breast cancer in mice of unmknow - n genetic constitution was first observed by maisin and coolen ( 1936 ) and perry and ginzton ( 1937 ) , while dobrovolskaiazavadskala and adamova ( 1938 , 1939 ) , were unable to observe a similar effect on inbred mice employed by theexperiments carried out by mider and morton ( 1939 ) , bonser and orr ( 1939 ) , strong and smith ( 1939 ) , bonser ( 1940 ) , strong and williams ( 1941 ) , engelbreth - holm ( 1941 ) , engelbreth - holm and lefevre ( 1941 ) , orr ( 1943 ) , kirschbaum , lawrason , kaplan and bittner ( 1944 ) , kirschbaum , williams and bittner ( 1946 ) , shimkin and bryan ( 1943 ) , strong ( 1945 ) , orr ( 1946 ) , demonstrated that carcinogenic hydrocarbons induce the appearance of breast cancer in females of low - cancer strains or accelerate the development of breast tumours in female mice of high - cancer strains . 
in these experiments it was also shown that oestrogenic influence is important in the induction of breast cancer by carcinogenic hydrocarbons , since mice developing these tumours in the absence of treatment with oestrogens were females , with one exception , a cba male ( orr , 1943 )  . 
the male mice of both strains , when 60 - 70 days old , were divided into three groups : mice of the first group received oestrone and methylcholanthrene , mice of the second group methylcholanthrene alone , and mice of the third group oestrone alone . 
c57 strain females , when 6 weeks old , were divided into two groups : mice of the first group were forcibly bred , mice of the second group were maintained as virgins ; both groups were treated with methylcholanthrene alone . oestrone was applied as a 0.02 per cent solution of keto - hydroxy - oestrone in alcohol , by painting the mice twice weekly for a period of 12 months . 
methylcholanthrene was administered according to the method described by orr ( 1946 )  . sixteen drops of 0 - 5 per cent solution in sweet almond oil were applied , at fortnightly intervals , to the skin of mice , four on each side of the dorsal and ventral surfaces of each animal . the c57 females of both groups received fortnightly applications of methylcholanthrene from the age of 6 weeks till death or the appearance of a tumour . in male mice the mammary gland is in a rudimentary state and they do not have nipples ( lacassagne , 1936 )  . 
administration of oestrogenic hormones leads to the progressive development of the mammary glands described in detail by turner and gomez ( 1934 ) , burrows ( 1935 , 1936 ) , gardner ( 1935 , 1939 , 1941b ) , lacassagne ( 1939b ) , loeb ( 1940 ) , loeb and suntzeff ( 1941 )  . 
because of these observations and the findings that breast cancer can be induced by methylcholanthrene in males treated simultaneously with oestrogens ( orr , 1943 ) , the c57 and c3h strain males were painted for 3 months with oestrone before the treatment with methylcholanthrene . 
after 3 months of painting with oestrone both the 057 and c3h males received their first application of methylcholanthrene which was then continued at fortnightly intervals until death or appearance of a tumour , except in the group of c3h males painted with oestrone which received only 14 applications of methylcholanthrene . 
two 057 males and one c57 female , which were treated with methylcholanthrene , developed general enlargement of lymphoid tissue , and in the c57 male which developed breast cancer a lymphosarcoma was found in the abdominal cavity . 
one c57 virgin female developed a spindle - celled sarcoma in the subcutaneous tissue . skin tumours were found in 10 out of 18 c57 males treated with methylcholanthrene alone and in 10 out of 35 c57 males treated with oestrone and methylcholanthrene . 
squamous metaplasia was observed in two tumours induced in 03h males by oestrone and .methylcholanthrene. the breast tumours induced in c57 mice , both male and female mice , showed a much greater degree of squamous metaplasia than the breast tumours induced in some of the induced tumours , as in the case of spontaneous in c3h male mice . tumours , variations in structure between different parts of the same tumour were found . 
sometimes the tumour cells were packed in solid sheets while elsewhere they occurred singly or - in small groups surrounded by an abundant stroma ; in some parts acinar structure could be clearly seen while in other parts it was lost entirely ; in places elongated cords of spindle - shaped tumour cells were found . 
thus the observations recorded by previous workers in this field were confirmed and the influence of hormonal factors on the development of carcinogen - induced breast cancer in mice shown . mammary tumours were also induced in c57 low - breast - cancer strain females , both breeding and non - breeding . 
orr results of other investigators . in mice , both males and females , which lack the mammary tumour agent . it is , therefore , possible to induce breast cancer in the present experiments breast cancer was induced in mice of a sub - line of c57 black low - breast - cancer strain which has a low susceptibility to spontaneous breast cancer . 
breast tumours developed in c57 black strain females , both breeding and non - breeding , after treatment with methylcholanthrene , and a c57 black strain male after combined treatment with oestrone and methylcholanthrene . it is not known whether the failure of kirschbaum , williams and bittner ( 1946 ) to induce breast cancer in breeding c57 black strain females with methylcholanthrene was due to the different method of application of methylcholanthrene or to differences in susceptibility of the two sub - lines of the c57 strano tumours were observed in either c3h or c57 black strain males treated with methylcholanthrene alone . this supports the findings of other workers that hormonal factors play a part in the development of tumours induced by methylcholanthrene . orr ( 1943 ) , however , reported the induction of breast cancer in one out of 16 cba low - breast - cancer strain males after intranasal administration of methylcholanthrene in the absence of treatment with oestrogen . 
he also obtained breast cancer in virgin mice of two low - breast - cancer strains ( if and cba ) after treatment with methylcholanthrene . in the present experiments tumours developed in two non - breeding c57 females treated with methylcholanthrene . mider and morton ( 1939 ) failed to induce breast cancer in non - breeding dba high - breast - cancer strain mice , while strong and smith ( 1939 ) , strong and williams ( 1941 ) and strong ( 1945 ) in their successful experiments on the induction of breast cancer in jk , nh and nho low - breast - cancer strain mice employed breeding females only . the present experiments confirm the findings of other workers that breast tumours can be induped in male mice of susceptible strains after treatment with oestrogenic hormones ( shimkin and andervont , 1941 , 1942 ; bittner , 1941 ; dmochowski and gye , 1944 ; bonser , 1944a , 1944b )  . the present findings also confirm the observation that mammary tumours develop in mice of resistant strains following treatment with methylcholanthrene . 
the c57 low - breastcancer strain mice of the sub - line used , when foster - nursed soon after their birth by riii high - breast - cancer strain females , develop an incidence of 11 per cent of breast tumours , but fail to develop breast cancer when given the tumour agent at the age of 4 - 6 weeks , even after large quantities of the agent and in spite of increased hormonal stimulation by repeated pregnancies ( dmochowski , thus mature mice of this strain though resistant to the mammary 1948 )  . tumour agent are susceptible to a different agent , i.e. 
methylcholanthrene. the treatment with oestrogenic hormones failed to induce breast cancer in c57 low - cancer strain males . this again confirms the previous findings ( twombly , 1939 , 1940 ; bittner , 1940 , 1941 ; shimkin and andervont , 1941 , 1942 ; dmochowski and gye , 1944 ) that an increased oestrogenic stimulation overcomes the threshold of lowor non - susceptibility and results in the development of breast tumours only in the presence of the mammary tumour agent . treatment with methylcholanthrene induced in c57 black low - cancer strain females , breast tumours which , although similar in their structure to spontaneous breast cancer of highand of low - breast - cancer strain mice , show an increased incidence of squamous metaplasia . 
the samples were frozen in cyhndrical tubes immersed in a quartz dewar vessel and were irradiated with filtered light from a high pressure mercury arc , either the 3100 a or the 3650 a group of hnes being used . under these conditions afl the molecules examined were strongly luminescent , showing both a short - lived fluorescence ( persisting for less than 10 - 8 seconds ) and longhved phosphorescence ( persisting for several seconds ) in different spectral regions . fluorescence spectra were traced photoelectrically using a hilger e2 spectrograph equipped with a scanning unit . phosphorescence spectra were photographed using a mechanical phosphorescope as described elsewhere ( lewis and kasha , 1944 ; moodie and reid , 1952 )  . 
the phosphorescence spectra are the result of excitation to the very lowest excited state of the carcinogen molecule , a " triplet " state resulting from the fact that there are two unpaired electrons . excitation of this state requires only about 45 k.cal. , much less energy than is necessary to break bonds in the molecule , and its formation may well be an intermediate step in the reaction with protein . in this connection it should be pointed out that the triplet levels , since they cannot be detected in absorption , the common method of observing spectra , have been much neglected by biologists in their considerations of low barrier reaction paths that may be involved in biochemical reactioins . ( 2 ) the second significant correlation comes from heterogeneous system experiments . 
we have found that ff a carcinogen is ' used as the microcrystalfne component and the dissolved component is naphthacene , the ( fluorescent ) emission of the naphthacene is shifted shghtly in wave length because of its interaction with the carcinogen . 
some of the results are it will be observed that the smallest shffts in the naphthacene show - n in table ii . bands occur when the strongest carcinogens are used as the host crystal . there is a moderately good correlation between these shifts and the self - polarizabihties at the position of the substituent calculated by greenwood ( 1951 ) , which values themselves correlate better with carcinogenic power than do an ' other physical constants . 
harnett. published for the clinical cancer research committee of the british empire cancer campaign . received for publication july 16 , 1948 . in 1938 - 39 the clinical cancer research committee of the british empire cancer campaign carried out a clinical survey of all cases of cancer seen in the hospitals , both voluntary and l.c.c. 
in the administrative county of london . this was done by means of questionnaires , one of which was filled in by the registrars in the various hospitals for each patient and returned to the clinical cancer research committee for record . 
the work was interrupted by the outbreak of war after it had been in progress for 17 months . by this time 15 , 200 cases of cancer had been registered , of which 2529 ( 16 * 6 per cent ) were cancer of the breast . these patients have now been followed up for five years or more and the records analysed . 
4 - 556 1 8 + 0 66 . the mean age is 5 - 6 years higher than those given by lane - claypon ( 1926 ) and wainwright ( 1931 ) , due to the fact that the two latter series include only cases coming to hospital for operation , whereas the b.e.c.c. 
the youngest patient in the series was aged 15 , and survived 5 years after enucleation of a tumour of 3 years ' standing , which proved on histological examination to be an early adenocarcinoma . 
expected actual per cent of expected possible x - rays alone or with interstitial radium . number of cases of known duration mean number of months lived j in 5 years from onset maximum  . 
expected lactual possible per cent of expected x - rays with local surgery . number of cases of known duration mean number of months lived in 5 years from onset maximum  . 
it was found that patients in stage iv who were not treated either by surgery or radiotherapy had a 5 - year expectation of life of 46 - 7 per cent of normal , which was not improved by palliative x - ray treatment . all these figures must be considered in the light of the fact that the mean duration of the disease is 38.3 months ( major greenwood , 1926 ) , so that these patients whose mean age was 57 years would have a 5 - year expectation of life of about 56 months ; a 5 - year follow - up is therefore insufficient for assessment of the results of treatment . 
the variations in mean age of the patients submitted to various types of treatment is shown below , and indicates that the more radical methods were used in the younger patients . radiotherapy mean age of 703 patients treated by radical mastectomy alone mean age of 133 patients treated by local mastectomy alone radiotherapy mean age of 174 patients treated by radium alone or with local surgery h.v. 
fodden. from the department of pathology , university of liverpool , and the liverpool cancer control organization . received for publication august 20 , 1948 . in his ' textbook of pathological anatomy ' rokitansky ( 1861 ) made his classical statement that pyloric cancer was exactly bounded by the pyloric ring , and that the growth never reached beyond into the duodenufrom this time it appears that the majority of observers , with the early exception of brinton ( 1864 ) , commented upon the integrity of the duodenum in cases of carcinoma of the stomach . 
many well - known surgical teachers spoke of the habitual immunity of the duodenum from invasion . kocher ( 1893 ) , mikulicz ( 1898 ) and most ( 1899 ) believed it to be always constant . kocher ventured that it was a problem of extreme interest to consider why gastric carcinoma grows in almost all cases towards the cardia , yet stops , on the contrary , at the duodenopyloric junction . it was brinton who first took especial exception to this proposition of rokitansky . 
1. received for publication may 10 , 1951 . there is still some disagreement on the question whether the early changes produced in epidermis by chemical carcinogens are specific , i.e. , whether they can be distinguished from the effects of non - carcinogenic irritants . the chemical evidence is inconclusive . 
cowdry and his school have been able to show that the chemical constituents of mouse epidermis made hyperplastic by several applications of 20 methylcholanthrene differ quantitatively from those of normal epidermis ( carruthers , 1950 ) , but it does not appear to have been proved that these changes are produced only by carcinogenic substances . histological evidence is more definite . 
the only significant way in which such skin has hitherto been found to differ from untreated skin is in its ability to produce tumours when treated with a co - carcinogen such as croton oil . 
the " latent tumour cells , " if present , must be so few that they are very unlikely to be detected in sections , or perhaps they may not be recognizable if seen . 
the skin has passed through a state known to be produced only by carcinogenic agents ; this state has apparently passed away , yet the skin will then react to treatment with a non - carcinogenic substance in a manner quite different from normal skin . the early reaction of normal mouse skin to croton oil is similar in general type to its reaction to other non - carcinogenic irritants , and differs in important respects from the reaction to carcinogenic substances . 
the chief criteria on which this distinction is based have been fully described by pullinger ( 1940 ) and by gluiicksmann ( 1945 ) , and only a summary will be given here . 
gwynn the epidermis is stratified . in the normal skin of the body of the mouse there are no strata , and the various types of cell are arranged apparently at random in a layer one cell , or in places two cells , thick . of the nucleated cells in the epidermis of the back of a normal adult mouse , about 14 per cent are resting , 80 per cent differentiating , and the rest are mitotic or degenerating . this classification was used because it gives definite information about the state of the epidermis which is not obtainable by any other method known to this information is not dependent on any hypothesis about the function or potentialities of the different classes of cells . 
for the purpose of this work they are simply types of cells which can be distinguished , the absolute and relative numbers of which vary in different states of the skin . one of the most striking features of the hyperplasia produced by chemical carcinogens in mouse epidermis is the rise in absolute and relative numbers of the resting cells . non - carcinogenic irritants , on the other hand , produce a hyperplasia in which the absolute number of all epidermal cells is increased but their relative numbers remain approximately the same as in normal skin ( gliicksmann , 1945 )  . 
the percentage of resting cells in the epidermis was chosen as a criterion for comparison of the hyperplasia produced by the different treatments used in the following experiments . it provides a measure , which can be handled statistically , of the specificity of the reaction of the epidermis , i.e. , of its resemblance to the characteristic reaction to carcinogenic substances . in the work now reported the effect of croton oil on normal mouse skin has been compared histologically with its effect on skin after the reaction to previous treatment with a chemical carcinogen has apparently disappeared . three strains of mice and two different carcinogens were used . 
 " t " and " s " mice were purchased from dealers . " p " mice were of an institute - bred strain originally obtained from the national institute for medical research ; they had been used before for studies on skin carcinogenesis by gluiicksmann ( 1945 ) and salaman ( 1943 )  . 
the standard errors of means were of the same order in this experiment as in the other two . the mice were examined weekly for the appearance of tumours , for periods of 200 to 250 days . 
gwynn high level and remained well above normal . in group 2 there was a parallel but smaller increase . in group 3 application of croton oil without previous treatment was followed by an initial slight rise in resting cell percentage , which then these results are listed in table i and charted in fig . 
the first tumour appeared on the further trials have 63rd day in group 1 , but not till the 170th day in group 2 . confirmed the superiority of acetone over paraffin as a solvent for the carcinogen comparisons of various concentrations of croton used as the primary treatment . oil in acetone and paraffin have shown that a 0.5 per cent solution in the former is almost as powerful a co - carcinogen as a 2.5 per cent solution in the latter . 
13. - experiment 2 : 0 group 2 : 10 mice at beginning of experiment , 8 survivors at 217th day . e group 4 : 12 mice at beginning of experiment , 11 survivors at 217th day . weekly croton oil applications without previous treatment ( group 3 ) caused only a transient rise to 21 per cent on the 3rd day , and thereafter the level declined gradually to 16 per cent on the 115th day . 
13. since no tumour it will be seen that tumour appeared in the other groups , they are omitted . production in group 4 began earlier than in group 2 , but later proceeded more this suggests a possible parallelism between the early rise of resting rapidly . cell percentage and the tumour production which follows about 50 days later . ( 3 ) in a third experiment , four groups , each of 8 male and 8 female mice of group 1 , in this experiment , the " s " strain , were treated as shown in table iii . has the same function as in the last : a test of the carcinogenicity of the primary treatment with the carcinogen . 
14. as in the last two experiments , the difference between the effects of croton oil treatment with and without a previous carcinogenic stimulus is clear ( groups 2 and 3 )  . in group 4 , resting cell percentages were at first lower than , but later rose above , those of group 2 . 
15 shows the rate of tumour production in these groups . dimethyl - 1 : 2 - benzanthracene in paraffin oil appears to have been less effective than 1 per cent benzpyrene in acetone ( group 4 of experiment 2 , but note that different strains of mice were used )  . tumours appeared earlier in group 2 than in group 4 ; thus , as in the former experiment , there appears to be a parallelism between resting cell percentage and subsequent tumour production . 
gwynn except one in which early malignant change was probably present . during a considerable experience of the application to mouse skin of croton oil alone , a very few small tumours have been seen , but never as many as in this experiment . precautions against contamination of cages , etc . , with carcinogenic substances are taken , but the possibility that such a technical mistake occurred cannot , of course , be entirely excluded . it is perhaps significant that the resting cell percentage in this group , after falling to 16.6 per cent on the 132nd day , rose again to 20 per cent on the 216th day . tumours produced by the application of substances generally regarded as non - carcinogenic have been occasionally reported . 
9 and 10 are high - power views of regions of the epidermis consisting predominantly of resting cells and differentiating cells , respectively , taken from the same specimen as fig . 
many substances are as powerful hyperplastic agents as croton oil , without being co - carcinogenic . croton oil is much the most powerful co - carcinogen for the mouse 's skin yet discovered . its action appears to be highly specific with respect to animal species , and perhaps also with respect to the carcinogen with which it acts . it may be that it combines very weak carcinogenic with powerful co - carcinogenic power . 
a number of tumours subsequently appear . this number varies widely according to strain of mouse and strength of initial carcinogenic stimulus ; there may be an average of only 2 or 3 , or as many as 20 , per mouse . 
but even if the higher figure is taken , and it is assumed that each tumour was represented before croton oil treatment began by a single " latent tumour cell , " or a small group of such cells , these cannot be responsible for the generalized rise in restingcell percentage which is observed throughout the epidermis . in fact the chance of finding such a cell or group in a section is small . 
it appears that mouse epidermis which has been treated with a carcinogen , though it returns to a state closely resembling the normal , has suffered a general change which does not consist merely in the presence of a few latent tumour cells . we are indebted to professor s . 
w.3. received for publication april 3 , 1954 . the development of the search for endogenic carcinogens has been reported in earher publications from this institute , ( see hieger ( 1949 ) for references to previous papers )  . it has been shown that the cholesterol - rich fraction of ' tissues from human subjects who had died of cancer or of other causes , and even commercial cholesterol . 
the first tumour in table i was carried through 93 generations and the first tumour in table iv ( highly purified cholesterol ) has been growing vigorously in its 25th generation . 
the control tests on solvents are described further on in this paper . purification of the cholesterol was next undertaken , as a first step using the simplest technique . table ii gives the results of tests on fractions of commercial cholesterol obtained by crystalhsation from acetone . 
the method involved several stages . these were : ( 1 ) acetylation . this step provided several advantages , nameiy ( a ) the oh group was protected during bromination ; ( b ) the acetate can be differentially eluted from a1203by mild eluents the unacetylated sterol when absorbed on a1203 requires more powerful eluents . ( 2 ) bromination , filtration and debromination . ( 3 ) adsorption on a1203colunin and elution with benzene - pet . 
orr there was , of course , no guarantee that contamination could have been completely avoided in the " carcinogen - free " room ; for example , 'sawdust from a box - containing benzpyrene - treated mice might accidentally be carried in to the noncarcinogen room on the shoes of anyone who had walked through the carcinogen however , the technicians who serviced the mice in the . 
consequently the controls had more injections than the sterol injected mice in order to maintain a stationary nodule . is the carcinogenic activity of commercial cholesterol due ( a ) to the sterol itself , or ( b ) to highly active impurities ? the evidence presented in tables iv and v provides support for ( a ) , i.e. , cholesterol per se is the true carcinogen in the commercial product . if the incidence of sarcomas be expressed as the ratio ( percentage ) of tumour mice to injmted mice which survived to a minimal latent period level , say i year , then the result can be stated thus : ( a ) purified cholesterol gives rise to 4 per cent sarcomas in q ,  . 
the mice did not survive well , and in fact the single sarcoma appeared at the 27th month in the sole survivor of the 34 mice initioy injected with purified cholesterol . twenty - seven months is near the outsidei limit of the range of latent periods found with the carcinogens of the cholesterol categpyy , , in an experiment with commercial cholesterol ( table ii , section a ) 3 of the 4 280 1 . 
orr in 1947 ( unpubhshed ) , would provide an attractive theory of the mode of action of cholesterol as carcinogen . however , it would be necessary to postulate that the carcinogen is held by adsorption on the cholesterol 292 1 . 
op.p. although stif in a - n active stage , and that in sucha condition it is not roadily eluted , for clearly if it were a case of simple solubility there would be no more reason for ' the factor dissolving in the cholesterol than for it to be dissolved out secondly i ' ected cholesterol after a year or so in the body should be again . thirdly , if such an assumption were accepted , there rich in absorbed carcinogen . would be httle necessity to proceed with the question of whether pure or impure fourthly , if the carcinogen ' which is concencholesterol is the true carcinogen . trated in the cholesterol originated in the environment , it should be easy to test the hypothesis by purposely arowing the mice injected with the cholesterol to hve an atmosphere rich in carcinogen . this test has been put into operation , and constitutes a secoind stage to the investigation on atmospheric carcinogens as a factor in sarcoma induction ( see above )  . one hundred stock mice were injected with ohve oil solution of commercial cholesterol and kept in a carcinogen - rich atmosphere as described above . 
the control mice ( 135 ) were kept in the room free from carcinogen . the results are shown in table v . control te8t8 on the 801vent8 . lard was employed as solvent from 1936 to 1949 . during this time a total of over 360 mice was tested with the solvent , lard ' alone . these mice did not survive remarkably well ; they gave no positive result until the series had been almost completed , when among the last few batches a single sarcoma developed . 
when in 1950 , a change was made from lard to olive oil ( hospital dispensary grade ) , a control series of 134 mice was set up for injection with the oil alone . 
the old c " mice were 12 ( and upwards ) months of age at the start of the experiments ; their effective number should therefore be raised by a factor of the order of 2 since the initial number , 19 , would represent the survivors at 12 months . 
the siingle sarcoma occurred in an oldc57moim at the unexpectedly low latent period of 6 months . * however , s ' mce this mouse was 16 months of age at the start of the experiment some ageing factor for tumour induction is obviously operating . 
this preparation gave 2 sarcomas in 20 mice initiary . other work on carcinogenic activity of chole8terol . truhaut ( 1947 ) could find no activity in his sample of purified cholesterol . truhaut injected 20 mice , of unnamed genetic origin , with cholesterol " purifie ' , " 20 mice with cholesterol irradiated with 10 , 000 r , and 20 with solvent alone , namelv ohve oil . 
 " " si la susceptibilite ' individuelle des animaux n ' est pas en cause , cela tendrait ' a d6monter la pre 'sence , dans le choleste ' rol commercial , d ' impurete 's fortement cance ' rig ' enes qm se rapprochent vraisemblablement des substancek ; responsables de i ' activite ' cance ' rig ' ene de la fraction des ste ' rols precipitables par le digitonoside dans l ' insaponifiable du foie de sujets cancereux . steiner ( 1951 ) has also reported that no carcinogenic activity could be detected in a sample of cholesterol . 
from the carbonyl absorption found in cholesterol fractions , therefore , the type of impurity and its approximate amount can be deduced . cholesterol preparation numbers , 3 , 4 , 6 , 7 and 9 ( for key , vide supra ) showed no appreciable carbonyl absorption ( less than 0 - 25 per cent )  . 
number 8 ( glaxo sample 5989 ) had a band at 1744 cm . - ' , assigned to a 17 - ketone , equivalent to about 1 per cent of such an impurity . 
number 11 ( glaxo sample 1201 ) had three bands at 1744 , 1710 and 1674 cm - ' ; these indicate about 9 per cent of a 17 - ketone , 4 per cent of a 20 - ketone ( or possibly in a 6 - membered ring ) and 3 per cent of an ac , unsaturated ketone , probably a a4 : 3 - ketone . number 5 , which was the least soluble fraction obtained by fractional crystallisation of this latter commer290 i . 
the most soluble fraction in this crystallisation and used for the test in section d , table ii ( number 13 ) contained the impurities concentrated about five - fold . 
1. received for publication january 21 , 1949 . kennaway , kennaway and warren ( 1944 ) found that injection of certain carcinogenic substances , including 1 : 2 : 5 : 6 - dibenzanthracene , caused an increase in the concentration of ascorbic acid in the liver of mice , whilst some noncareinogenic , chemically related substances ( naphthalene , anthracene , phenanthrene ) did not show this effect . in an investigation of the growth - inhibitory action of the carcinogenic hydrocarbon 1 : 2 : 5 : 6 - dibenzanthracene ( elson and warren , 1947 ) it was found that the inhibition of rat body growth and of the growth of walker rat carcinoma 256 ( elson and haddow , 1947 ) by this substance is dependent on the protein content of the diet of the animals . 
1 : 2 : 5 : 6 - dibenzanthracene in the rat usually results in little growth inhibition for about the first 14 days , after which the animals at varying intervals lose weight and die . 
on a 10 per cent protein diet after the same dose of the carcinogen , immediate inhibition of growth occurs and persists for a prolonged period , usually until the death of the animal . in considering the cause of the rise in liver ascorbic acid brought about by 1 : 2 : 5 : 6 - dibenzanthracene , it appeared possible that this was a result of the growthinhibitory action of the compound . 
there was some evidence ( elson , unpublished communication ) that the growth inhibition was accompanied by a fall in the succinic dehydrogenase component of the succinoxidase enzyme system of since the cytochrome oxidase component of this enzyme system is the liver . capable of rapid oxidation of ascorbic acid , it seemed possible that the rise in ascorbic acid after 1 : 2 : 5 : 6 - dibenzanthracene might be the result of less destruction by such oxidation occurring owing to the decreased content of the oxidizing enzyme . 
they were weighed every 2 or 3 days . high and low protein tabls . in later experiments it was found necessary to estimate the amount of food consumed by each rat , and in order to facilitate this 25 per cent and 5 per cent protein diets were made up in 5 g . 
tablets in the shape of cylinders of approximately 3 cdiameter and 0 - 5 chigh . this necessitated replacement of some of the starch in the original diets by cane sugar and glucose in order to obtain a firm tablet . 
from the control experiments , in which only arachis oil was injected , .it is seen that the variation of the protein content of the diet itself has practically no influence on the level of ascorbic acid in the liver . 
the animals fed the 5 per cent protein diet grow only very slowly , but the effect of dibenzanthracene on them is not to make them lose weight , as would be expected if the magnitude of the growth inhibition was proportionate to that observed in animals this smaller effect is presumably maintained on the 10 per cent protein diet . related to the lower total metabolism of the 5 per cent protein diet animals , and 152 l . 
5 , although complete inhibition of growth occurred , and at one time actual loss of weight , the food intake , after the initial drop , rose steadily to a value higher than the level before administration of dibenzanthracene at the time the animals were killed for determination of liver ascorbic acid the actual degree of growth inhibition was greater than the maximum previously obtained with the 10 per cent protein diet animals . 
the degree of growth inhibition is dependent on an equilibrium being established between the rate at which the animal is metabo - _wa% growth rate fooie ratn ? j final liver wt ascorbic acid o * + |~~ 1i 135 6 - 14 ( 1 * 1 [ oo llll , , illlllllllllll , lll ( 134 1i111 . , g14 3 ) o3 ) _ t .%1 5 days 20 25 7 - 02 ' 10 - ~ _ ~3124 8 - 17 7 - 63 fig . 
in animals fed 20 per cent protein diet liver ascorbic acid increases before any marked growth - inhibition is observed , and the increase is thus not an indirect consequence of the inhibition of growth . the growth - inhibition is not merely the result of a lowered intake of food . the animals may react to treatment with dibenzanthracene by maintaining or even increasing their daily food consumption , although growth is completely inhibited . this suggests that a profound change in basal metabolism must have taken place , and the rise in liver ascorbic acid may be associated with this change . we wish to express our thanks for generous grants supporting this investigation , from the british empire cancer campaign , the anna fuller fund , the jane coffin childs memorial fund for medical research , and the u.s. 
carr. from the poultry re8earch centre , edinburgh , 9 . recieved for publication january 19 , 1953 . most cancer investigations involve the use of small rodents , and it is now clear that many of the " generalisations " obtained from research on this material break down when other animals are considered . while the relevance of any result obtained with grafted tumours to the problem of spontanous cancer may be doubted , it seems desirable to report the results obtained by parallel work on non - rodent material in order to offer proof that similar results are , or are not obtained . the grch / 15 tumour is a non - filterable fibro - sarcoma originated by peacock in 1939 ( peacock , 1946 ) , and by his courtesy made available to other workers it is through the animal breeding unit of the british empire cancer campaign . readily distinguished from the virus - induced tumours by the absence of the mucoid material that they all produce , but unless the section is specially stained for this , microscopic differentiation is less easy . transplantation was always made into brown leghorns of greenwood 's flock ( in one of which the original was induced ) , either by implanting small pieces with a fine trocar and cannula , or injection by syringe of the suspended material left after shaking minced tumour or tumour ground with sand and saline . transplants were usually made into each pectoral muscle , and by the trocar and cannula method " one - sided " negatives occurred about 1 in 20 times , while the second gave less than 1 per 100 " one - sided " failures ; the incorrect negatives due to experimental errors would therefore be 1 in 400 and 1 in 10 , 000 respectively , which can be ignored . 
the material for this account is based upon 60 transplant generations involving some 600 birds over a period of 8 years . in most experiments the birds were 6 to 10 weeks old when the tumour was implanted . in the bird the tumour appears as a hard white lump , though after the alteration in the growth rate the texture was softer , and microscopically the cells appeared rather more compact . 
983 , from which all material for the 32nd and subsequent generations derived . it is interesting that the change coincides with a distinct alteration in the conditions of husbandry , for the facilities for keeping animals at the experiment station were at first not optimuno cages were available for birds , and the food comprised various ration - free products , which produced a series of deficiency diseases ranging from protein to multiple vitamin shortages . 
when the conditions were built up to those nearer first - class management the change in appearance and behaviour of the tumour remained . there is no direct evidence that the change in conditions caused the alteration of the tumour , and it remains possible that it was a coincidence . the most notable change in the tumour was in the rate of growth . 
by contrast , in only one bird out of many thousands has this organ been the site of a rous 1 metastasis . of 352 birds killed and examined with large growths in the breast muscle , 51 had metastic growths in one or more sites . 
nor is it due the conditions for tissue transto a failure of the bird to produce iso - antigens . plantation , however , seem to differ markedly from those of the lower rodents . for example , organ transplantation between fowl varieties is a normal experimental technique , used for example by greenwood ( 1928 ) to investigate the relation of the testis to henny feathering of males of some breeds ; yet transplantation of an adrenal is regarded as a novel event in the mammalian field similarly , the elaborate integumental decorations of birds early ( darcy , 1952 )  . attracted the attention of zoologists , and the results of skin transplant between different genera were being embodied into the general assembly of zoological theory before tissue iso - antigens were recognised . it is possible to suspect that a similar mechanism is indeed operative in the mammalian field , but the methods used are not refined enough to detect it . 
the domesticated rat and mouse have an oestrous cycle of only a few days in length , as compared with the sharply - defined annual cycle in the hen , and lesser cyclic variation of the cock . 
even the pregnancy of 3 weeks is rather short for observations in the rat and mouse , but it is significant that foulds ( 1949 ) found some evidence of a variation in tumour growth and structure in the mouse , and there are many reports of pregnancy influencing the course of tumours in the human . the appearance of many cancers at an age when the sexual functions are failing may be another aspect of this . this would seem to be a point of considerable importance , for it indicates that control of a malignant tumour would be possible within the limits of normal physiological variations ; similarly studies on the cancers induced by chemicals , and more especially by x - rays , indicate that the production of the malignant change and the appearance of a progressive tumour are distinct phenonema , a separation that is even more obvious with the mouse milk factor , where infection takes place soon after birth but the tumour appears months later , and only if the endocrine history of the host has been suitable . 
carr aries in the proventriculus in older birds carrying the " slow " tumour refers to a difference in the biochemical suitability of the organ in the older hosts is it is to be expected that the differences of tissue permeability with unknown . age ( duran - reynals , 1942 ) would also have some influence upon the metastatic growths . the absence of any neutralising action in the sera of fowls immunised against the grch / 15 sarcoma is in contrast to the findings of gottschalk ( 1943 ) for sarcoma 16 . but it is well known for commercial birds suffering from the related " leukosis complex " viruses to have death - rates of up to 40 per cent and carrier rates of nearly 100 per cent , so that such a finding is only of value if it can be stated that such carriers are not a complicating factor . 
a fast - growing mutant strain retained this property , and the mutation was not associated with an increased frequency of takes , though the distribution of secondaries was altered . 
koller. from the chester beatty research institute , the royal cancer hospital , london . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . xeroderma pigmentosum ( hence referred to as x.p. ) , is marked by rougheniing , dryness , pigmentation and ulceration of the skthe condition is attributed to hypersensitivity of the skin , particularly that of the basal cell layer , to sunlight . the disease was first described adequately by kaposi in 1874 ( hebra and kaposi , 1874 )  . 
occurs in the first year of life , often within a few , months after birth . first , erythema develops on the skin , on those regions which are exposed to light , followed by freckling and frequently by telangiectasis . from these regions epithelioma or basal - cell carcinoma develops . 
the malignant change may take place not only in the skin , but also in the cornea and conjunctiva the genetical and chromosomal basis of x.p. the hereditary basis of x.p. 
was first investigated by siemens and kohn ( 1925 )  . they analysed 76 families , and cockayne ( 1933 ) brought this more up - to - date with a further 43 family histories . in both groups of data the incidence of consanguineous marriages was very high : 24 out of 76 and 16 out of 43 respectively , were first - cousin marriages . 
is one of those which is borne in that particular region of the sex chromosome , common to x and y . it may not be superfluous to describe the cytological mechanism which underlies incomplete sex - linkage . the genetical basis of incomplete sex - linkage is clear , and is already described 150 p . 
they found thait during the first meiotic d ' ivi ' lsion of the male rat , one or two chiasmata are forined between the x and y chromosomes , and that the shape of the sex bivalent is determined by the position of chiasmata in relation to the centromere and differential segment . 
the structure of the bivalent is determined by the position of the chiasmata ; the frequencies of the various bivalents are shown by the number of percentages beside the figures . similar chromosome behaviour wak ; observed in man . 
the fact that the heteromorphic pair present in the chromosome set of the human male , forms a very easily observable unequal or asymmetrical bivalent during meiosis , is - well known from the - works of painter ( 1923 ) , evans and swezy ( 1929 )  . 
when a ' man inherits such incompletely sex - linked gene from his mother , it will be in his x chromosome , but occasionally it may cross - o ' ver to the y consequently the man will transmit the gene to most of his daughters and to a similarly , if he inherits it from his . 
father , he , will transmit it few of his sons . to most of his sons and to a few of his daughters . human genetics is greatly indebted to j . 
he analysed 82 family histories collected from various sources , and by using ingemoug statistical methods drew the conclusion thatthe incomplete sex - linkage of the g ' ene x.p. 
he made the suggestion tha ' t one of the 82 families on which analysis was based should be excluded on intemal evidence , which would further loosen linkage , and in this case the true position of x.p. 
the data obtained from these cases has given further information on the hereditary basis of this morbid condition , and has shown the 'significance of the pathological symptoms , including the degree of manifestation and the time of onset of the disease . 
of one year the whole skin of the left 'side of her face came up in red blisters after being exposed to the sun . she was treated with calomel lotion . 
the condition it was treated by " caustic pencl ' l , " and six months later , was diagnosed as x.p. in 1943 another lesion developed on the right when it recurred , by radium . cheek , which was similarly treated by radiuthe patient 's skin of the exposed both the pathological skin conparts ( face , hands , legs ) shows some scarring . ditions and the histological analysis of the lesions indicated x.p. 
the parents are unrelated ; father is of a dark complexion , mother has some slight freckling search through family histories on the cheek , which is of the common type . of near relatives and sibs did not reveal any similar conditions . 
at that time some of the freckles developed into small ulcers , which healed slowly . she found out , by experience , that strong sunlight accentuates the lesions , and since the age of 40 she has taken care not to expose herself to direct sunli.ght. 
the matemal and patemal grandfathers were brothers.. the eldest brother , frank , hischildren and grandchildren are all normal . isabel , the patient concemed , was the second child , but before her birth one ' miscarriage took place . 
her sister , dorothy , is one year younger ; she is afflicted with the dorothy shows freckling on the face disease in the same mild manner as isabel . and forearm , which is somewhat less severe than that of - her elder sister '  . a younger brother , thomas , was born after isabel . 
the high number of miscarriages and the death of the sixth child , a girl , on the day following birth , may , not unlikely , find its sidney died at the age of 25 explanation in the consanguineous marr ' lage . up to his death he appeared to be normal . there are two unusual features in the history of the hfamily which require explanation . 
in the hfamily does not conform closely to expectations ; the number of cross - overs is higher than could be expected . in order to explain the exceptional pathological features and the unexpected segregation of x.p. 
in the sexe - s in this particular family , the followina possibilities may be considered : ( a ) this condition - may be due to an independent autosomal gene , or ( b ) the gene x.p. 
the increased distance of the gene from the differential segment would loosen linkage with sex , and its altered position may also lead to a lower degree of malignancy . the data at our disposal from this one family , however , is too meagre to draw definite conclusions , whether we are dealing here with a distinct autosomal gene or with position effect . 
gunz. * from the department of radiotherapeutics , university of cambridqe . received for publication june 11 , 1949 . in previous publications ( gunz , 1948a ; b ) a technique of cultivating human leukaemic leucocytes in vitro was described , and the quantitative and cytological findings in untreated cultures made by it were analysed . 
he did not , however , determine the mitotic rates in his cultures , because of the small number of dividing cells present . osgood 's findings may be compared with those of schrek ( 1946a , b ) , who irradiated suspensions of thymus and spleen lymphocytes , and of bone marrow cells ( rabbit ) , and of normal and leukaemic human blood cells in " phosphate ringer solution " with and without homologous serum , with doses of x - rays of using as a criterion of survival a failure of cells to stain with a 20 - 4000 r . 1 : 1000 solution of eosin in tyrode solution , schrek found exposure to x - rays to cause a decreased survival time vitro in lymphocytes from the thymus , normal blood and four of five bloods from patients with chronic lymphatic leukaemia . such an effect was noted after a dose of 50 r , and increased with an increase in the dose up to 1000 r , remaining approximately constant at higher doses . 
the author , discussing possible reasons for this lack of effect , attributes it to an absence of dividing myeloid cells in his preparations , x - rays leaving resting myeloid cells unaffected . interference with mitosis , as a result of x - irradiation , was definitely demonstrated by rachmilewitz , rosin , goldhaber and doljanski ( 1945 , 1947 ) in experiments with fragments of explanted rabbit bone marrow . following the application of 250 - 1000 r there was a depression of mitosis lasting for two to four hours , with subsequent recovery . 
many mitotic abnormalities were caused , and the marrow became hypocelhular , or almost completely aplastic , according to the size of the dose given . the observations in the literature may be summarized by stating that x - rays have been found to damage blood and haemopoietic cells , especially lymphocytes and all classes of immature cells , when applied directly in vitro , and that disturbances of mitosis appear to be among the earliest signs of injury in cells so exposed . 
two patients had not received any x - ray treatment when first seen ; the others had had various amounts of treatment in the past . the technique of culture was that previously described ( gunz , 1948a )  . brief , it consisted of the distribution of small equal quantities of leukaemic leucocytes , suspended in the culture medium , over a series of culture tubes , and the withdrawal of some of the tubes for counting after varying periods of incubaat these times total and differential counts were made , and the total tion . number and phase distribution of mitoses determined . the culture medium used consisted either of 50 per cent dried , reconstituted human plasma , with the addition of 5 per cent rat embryo extract , or of 50 per cent fresh homologous human serum , both diluted in ringer solution . the duration of experiments was two days , and counts were done at 8 , 24 and 48 hours , unless otherwise stated . the technique of irradiation was as follows : after the cultures had been set up , they were incubated at 370 for about 15 minutes , to give them time to reach body temperature . in some experiments some of the tubes were also incubated for longer periods before irradiation . 
the tubes were exposed at two fixed distances ( approximately 21 and 81 cfrom the target ) , the dose rates , measured in air , at these points being 622 and 62r / nirespectively . 
the actual dose rate to which cells were exposed depended on three factors : the dose rate in air , the absorption and scatter due to the glass , and the absorption and scatter due to the fluid . 
the dose rate in air was measured by means of a victoreen dose meter in the normal way ; it was found that when the chamber of the dose meter was inserted into empty culture tubes , the average decrease in the dose rate was 6 - 5 per cent . this enabled a correction to be made for the glass of the tubes . 
the volume of the liquid being only of the order of 1 or 2 ml . , the correction for the absorption and scatter due to it would be less than 5 per cent , and was ignored in estimating the dose rate . 
the results of irradiation with 100 , 1000 , and 10 , 000 r are set out in tables i - vi . if the contents of tables i - vi be summarized and analysed , we obtain the following findings : immature cell8 . with a dose of 100 r the ratio , at 8 hours , of immature cells in irradiated to in five experiments it those in control cultures varied from 65 - 113 per cent . was greater , and in seven experiments less than 100 per cent . 
a significance in the analyses of immature cell counts test ( student 's t - test ) was employed . percentages were first converted to logarithms , in order to obtain a more normal distribution of the series . 
the actual formula used was t - s - - = where x is the arithmetic mean of the series , 8x its standard error , and m = log10100 = 2 . this gave a value of t = 0 * 97 , which is not significant . at 24 hours the ratio varied from 71 to 111 per cent . in four experiments it was greater , in one equal to , and in seven less than 100 per cent . 
the difference is not significant . at 48 hours the ratio varied from 48 to 112 per cent . in one experiment it was greater , and in ten experiments less than 100 per cent . 
from this t = 5 - 25 , and p is less than 0 * 001 . there was , therefore , a highly significant reduction in the number of immature cells in cultures 48 hours after irradiation with 100 r . with a dose of 1000 r the ratio , at 8 hours , of immature cells in irradiated to those in control cultures varied from 76 to 111 per cent . in three experiments it was greater , and in three experiments less than 100 per cent . 
no analysis was carried out for the 48 - hour values . with a dose of 1000 r the ratio was less than 100 per cent in all experiments , and at all times . 
no mitoses were present in irradiated cultures in 4 out of 7 experiments at 8 hours , in 5 out of 8 experiments at 24 hours , and in 4 out of 6 experiments at 48 hours . 
the results with 10 , 000 r were similar . it must be emphasized that these experiments were performed with varying culture media , and that the cells in some of them came from untreated , and in others from previously treated patients . this explains many of the numerical differences between individual experiments , particularly in the mitotic counts . however , in spite of the non - homogeneity of the material , the results show clearly the following points : irradiation of cultures of leucocytes from chronic myeloid leukaemias with 100 r produced a significant reduction in the number of dividing cells for at mitosis then recovered , and did not differ significantly from least 8 hours . controls at 24 hours or later . 
1. - in vitro irradiation of leucocytes ( chronic myeloid leukaemia )  . irradiation with 1000 and 10 , 000 r produced a more marked depression of mitosis at 8 hours , and this did not recover subsequently . 
at that stage there were practically no dividing cells present , and the vast majority of all immature leucocytes in the cultures were truly " resting . " only after the lapse of several hours could any considerable numbers of them be expected to be approaching or entering it is , however , well known that chromosomes are particularly liable mitosis . to damage from radiation in the late pre - mitotic or early mitotic stages ( lea , 1946 )  . 
the following experiments were made in an attempt to irradiate cells at such a moment of increased sensitivity to x - rays , and to determine whether chromosome abnormalities could thereby be induced . - ~~~~ _ ~~~ ~ ~~~~1 ' ~~~~~~~~~~~~~~~~~~~~~ 338 f . 
gunz effect of varying the time of irradiation . in two experiments different groups of tubes were irradiated with 100 r at 0 , 2 and 4 hours from the time of setting up the cultures . 
3 , from which it is clear that no significant difference in the mitotic rate or the number of immature cells was produced as a result of varying the time at which the cultures were irradiated by up to 4 hours ; neither was the number of mitotic abnormalities in stained films altered . in another group of three experiments cultures were irradiated with 100 or 1000 r 7 hours after they had been set up , and counts and filmns were made at it was known that at 7 hours , appreciable frequent intervals after irradiation . numbers of cells would be entering mitosis . 
4. - effect of x - rays on leukaemic leucoeytes in vitro . irradiation 7 hours after explanta ' tion . that they only appeared when cultures were irradiated at a time when many mitoses were present , suggests that they arose from dividing cells , and it is likely that they originated in early prophase . 
15. it would seem that the findings at 8 and 24 hours are most likely to reflect the character of the cells themselves ; later on , artefacts due to the composition of the medium become superadded . taking only the 8 - hour counts into consideration , there was a good correlation between the patient 's blood count and the number of mitoses in cultures . 
 ( 1945 ) for normal rabbit bone marrow , but these authors worked with a different culture technique . no evidence was found that 100 r produced different results when given at this is in agreement with the finding of lasnitzki ( 1946 ) different dose rates . that in cultures of chick fibroblasts the initial inhibition of mitosis was independent of the dose rate ( 9.3 - 103 r / min . ) for doses up to 100 r . 
the explanation in the present experiments is probably that with both the dose rates used ( 62 and 622 r / min . ) , the time of irradiation - 10 or 97 seconds - was short compared to the overall time required for mitosis ( 35 - 60 minutes )  . no significant increase in the number of mitotic abnormalities was found to follow irradiation of cultures . 
the explanation for this is not clear ; it is , however , possible that technical difficulties prevented the recognition of finer structural alterations , like chromosome breaks . when cultures were irradiated 7 hours after their start , it was found that many cells in mitosis at the moment of irradiation completed their division . this agrees with the observations of many other workers , such as strangeways and oakley ( 1923 ) , canti and donaldson ( 1926 ) , kemp and juul ( 1930 ) , and furthermore , with 1000 r , a new kind of breaking - down cell love ( 1931 )  . appeared 3 hours after irradiation , and rapidly increased in numbers . 
assuming , for instance , that a similar process took place in the irradiated spleen , we should expect a definite diminution in the number of new leukaemic cells produced in that organ ; moreover , any further similar treatments would repeat , and possibly augment the effect . 
one could therefore picture the manner in which x - rays cause the enlarged spleen to involute . it is , however , more difficult to account by this means for the fall in circulating leucocytes which is such a prominent feature of the response to local radiotherapy in leukaemia , or for the involution of distant leukaemic lesions which had not been directly irradiated ( for examples , see piney and riach , 1932 )  . 
some light may be thrown on the latter problem by the findings in section b of the experimental part . here it was seen that leukaemic leucocytes , taken from the peripheral blood , showed a dininished power of proliferation in vitro after therapeutic irradiation of the patient , and that this effect was reversed as the clinical effects of treatment began to wear off . it thus seemed as if the biological make - up of the cells had been changed by the treatment . 
pullinger. from the imperial cancer research fund laboratories and the research department , the glasgow royal cancer hospital , glasgow , c.3. received for publication february 7 , 1952 . the hyperplastic nodules here referred to comprise all varieties found in surveys of spontaneous nodules in previous publications ( pullinger , 1949 , 1952 )  . at the time these surveys were being made specimens of affected nipple regions were almost invariably mounted and kept . it gradually became obvious that one nipple region , the 2nd on either side , was more often the site of nodule formation than any other . 
when the surveys were complete , the 5 pairs of nipple regions were arranged together with the number of times they contained one or more hyperplastic nodules of the various sorts . only those nodules are now included of which whole mounts were kept . 
the period of time covered was continuous from 1945 to the end of 1950 . the number of mice with mounted nodule - containing nipple regions was 116 ; the number of the nipple regions 146 . 
no record had been kept of 13 from which serial sections were made in the earlier stages of the survey ; more were incomplete or have been mislaid . six examples of bilateral nodules in the same gland were counted as only one of the pair . 
but for the extremes prognosis is definitelv affected in group statistics by the age at time of operation . in our e - xperience below the age of fortv vears axillary metastasis is much more apt to be present at the time of operation than bevond that age . in the s - ame , wav postoperative survivals . 
and the average postoperative hfe is shorter ( 16 - 7 months ) than in similar cases in the adult . " duk - es ( 1940 ) found that patients under the age of 40 vears had a higher incidence of lymphatic metastases than those in the age gmup 40 - 59 vears . 
they gave their opinion that the most malignant forms , both chnically and histologically , tended to occur at the younger ages . frissell and knox ( 1937 ) gave details of 46 cases of primarv lung cancer which on examining included - the age , and the duration of the - disease for each patient . these data we have found that there is no relation at all between age and the duration of the disease . 
he divided them into a carcinoma  . " group of 89 patients and an " epithelioma " group of 23 patients . he had no doubt that the clinical mahgnanev of the tumoiirs in the carcinoma group was greater in these patients than in older patients . 
undifferentiated tissue , often with manv mitotic figures in each field . " he found that h - valinization was never present that 1.ymphocytic infilltration and fibrosis were present to a moderate degree and only in the less mahgnant and that cellular differentiation was present mainlv in ovarian and tumours th - vroid carcinomas where . 
carried on through the cards and chose the first carcinoma recorded in the same organ and of the same sex in an individual in age group 46 - - 55 and again in a high age group . 
rectum ; and 61 vears and over for lung ( where the middle age group was 41 - 50 )  . for each tumour type we thus had three randomlv chosen groups of slides . 
the middle - aged and the old . ' the slides were then taken out of their holders and shuffled . this made identification of the sections impossible without reference to the laboratorv register of the numbers etched on the slides . 
ceu polymorphim and degree of fibrost - 3 ( scirrhous reaction ) the principle adopt . - d was to allocate grades i and iv to cases which were strikinglv low and strikinglv high respectivelv in these features . grades 11 and iii formed intermediate groups of " low moderate " and " high moderate respectivelv . for epidern " d differentiation the scale . 
 ' after completing the ' experiment , we were qiiite convinced that there was no such gross systematic change in type of material or standards of diagnosis over the years . 
we have , therefore , not considered that the difference between blocks arranged by date of diagnosis would appreciably reduce the residual error on which the significance of inter - age differences would be estimated . the experiment was therefore designed to allow for an analysis of variance . for example , in the sub - experiment " degree of glanduliform differentiation in rectal carcinoma " there was a total of 42 units or slides divided into 3 groups of 14 each for patients of 30 ygars or less , 46 to 55 years , and 70 years or more respectively , and divisible also into 14 groups of 3 each , i in each age group , diagnosed in an analysis of the variance in this balanced design in the same calendar year . there would then have been a total of 41 " degrees of freedom " comprising 2 for age , 13 for date of diagnosis , and 26 for residual error . 
of the 2 degrees of freedom for age , one could have been used to test the linearity of the difference in fact there was no need for this since a relatively coarse by age if necessary . analysis of the data indicated that the figures might we ] i have occurred by chance - on the hypothesis that there was no correlation between age and any of the factors we estimated . colloid ' formation " and " cell polymorphism , " using the total figures of each factor for for example , in the case of " epidermoid differentiation " there each age group . was a contingency table of the formthe x2 test was carried out for each factor , with the exception of the results for the various factors were epidermoid differentiation : 6 x2 4 - 95 p 0 - 7 - 0 - 5 . glanduliform differentiation ( consolidating grades iii and iv ) : 4 x2 = 4 - 55 p = c . 
at the begin9of the experiment , however , we laid down the hypothesis that we had no reason to expect significant results from one tumour type or characteristic more than another . it foflows that there is , so far as our results per se are coneemed , no rea - son to regard this as indicating a real correlation between age and increas ' epidermoid differentiation in bronchogenic carcinoma . it is notable , however , that in our reading of the literature the tumour in which the correlation between increasing differentiation and increa - sing age ha - s been most strikingly demonstrated ( geschickter and denison , 1934 ) is also bronchogenic carcinoma . consequently our figures , in so far as they are confirmatory , are also suggestive . we did , in fact , although we have not given the table , estimate , using the method of analysis of variance , the probabihty with which the figures for epidermoid differentiation and age could have occurred by chance for epidermoid differentiation of ( a ) bronchogeiiic carcinoma , ( b ) carcinoma of the cervix , ( c ) carcinoma oflip . 
a blank estimation was carried out on the reagents and in the latter half of the investigation a weighed amount of the filter - paper surrounding the discoloured areas was included in the blank , but this addition makes no considerable difference . occasional very high blanks were discarded as due to some unusual contamination . 
3. - mean seasonal variations in arsenic content of air at eight stations . w = winter ( november to march ) ; s = summer ( may to september )  . establish any exact comparison between the seasonal changes in the individual richard doll has pointed out to us that , the average values for the towns . different stations would be more properlv comparable , in view of the seasonal variations , if ( 1 ) the means of two figures for the same month and town were taken to represent that month , and ( 2 ) the mean of the figures for two months which are separated by a gap of one month without data were taken to represent that month . 
one might suggest some such classification as the following of the not very abundant data available upon the types of sunmmation ( table ii ) ; no claim is made that this is in any way a complete summary of the literature . 
the summation of action of two chemical carcinogens is not easy to demonstrate , and we appear to have few indubitable instances of it . * in connection with the subject of cancer of the lung , the work of lynch ( 1935 ) and andervont ( 1937 ) upon summation in the lung of some strains of mice is of especial interest , although the neoplasms of the lung in this species differ from those in man . 
3. received for publication january 21 , 1948 . during the war the pharmacology of the nitrogen mustards or chloroethylamines was studied intensively ( gilman and philips , 1946 )  . in the course of these investigations it was observed that tissues with a high proportion of dividing cells were particularly injured . this discovery led to the application of these substances in the treatment of malignant growth . 
of dimethyl - , - chloroethylamine hydrochloride by subcutaneous injection . such treatment when given repeatedly caused inhibition of some spontaneous mammary tumours ( table i ) , but had very little effect in prolonging the life of mice with transplanted lymphosarcoma . this compound given in single doses of 100 mg . 
the effect is similar to that induced by radioactive substances ; it is identical with the phenomenon of depigmentation in mice caused by subcutaneous implantation of plutonium ( brues , 19 , 47 , personal thus " bleaching of hair - colour " is another example of the communication )  . radiomimetic actions of the bis - chloroethylamines . the metabolism of walker carcinoma tissue from rats dosed with 1 mg . 
a variant of this compound , dimethyl - ] 3 - chloroethylamine hydrochloride , was used in 3 other cases , reported here because of the favourable response in 1 case . 
on two consecutive days in 30 cases , in 10 of which treatment was repeated once or several times at 3 - week or longer intervals depending upon the length of remission from symptoms . 
the majority of patients with advanced bronchogenic carcinoma have white cell counts above 10 , 000 per c.mm. , and such patients do not develop the moderate to severe leucopenia observed in cases of hodgkin 's disease ( apthomas and cullumbine , 1947 )  . in only 2 of our patients has the white cell count fallen below 4000 per c.mm. , in these cases to 1000 and 1800 with restoration to normal counts in 3 weeks ' time . the first of these cases had had previous radiation therapy , and at the commencement of treatment had a white blood cell count of 4000 per c.mhaemorrhagic nianifestations have not been observed in this group , nor has any significant change in haemoglobin dosages of 0 - 2 mg . 
at 10 - day intervals can be tolerated for been noted . periods of at least 10 weeks , as judged by the 4 cases we have treated over such a period . 
the presence of fever , pleural exudation or jaundice are not , in our experience , contraindications to the use of the drug . the adverse effects of the dimethyl compound were observed in 3 patients , 2 of whom are not included in this group as their diagnosis was not histologically proven . 
one patient was carried on for a period of 5 months with marked relief of pain , cough and dyspnoea and decrease of sputum for 18 to 21 days following each course of injections . 
a patient with remission of symptoms for 6 to 8 weeks after each treatment is still being observed one patient receiving dimethyl - , 3 - chloroethylamine is still in after 9 months . remission 7 months after treatment and leading a normal life . 
the relief of dyspnoea in some cases is almost complete - an observation very difficult to explain , for in such cases there may not be corresponding observable changes in the lungs . relief of general malaise and anorexia is also noted in over half the cases following the initial 1 - or 2 - day period of adverse effects . 
warwick sputum usually increases in amount for several days , and is said " to come up more easily . " the amount may then fall off rapidly , in some cases from 90 - 120 ml . 
the sputum may also change in character from purulent to colourless . reabsorption of pleural exudate or decreased rate of formation has been these observations are of interest in that most radioseen in 5 of 13 cases . ' therapists hesitate to give treatment to cases with pleural exudation because of the tendency to increase the amount of exudate . superficial metastases of measurable size decreased in 3 of 10 cases . 
a larger total number for such observations wouild have been obtained had not metastatic nodules been removed for microscopic study at various intervals following injection in 8 cases . twenty - two patients who had weight loss were weighed weekly following in 9 of these cases weight loss continued for approximately 1 week , treatment . following which a gain in weight occurred amounting uisually to 2 to 8 lb . four patients gained 10 to 15 lb . 
in 2 months , and 1 patient who lost 40 lb . in the 18 months prior to treatment with dimethyl - 3 - chloroethylamine has in 7 months regained all her lost weight . radiological evidence of decrease in size of pulmonary metastases and re - aeration of segments or lobes was observed in 8 of 35 cases . 
hb , 55 per cent . 3 , 800 , 000 . heart , mediastinum and trachea displaced to the right ; appearance of atelectasis with probable cavitation near 2nd right carina broadened rib . and invaded on the right by a large nodular friable mass completely occluding the right main bronchus . bronchoscopy report from harefield in april , 1946 . pathological report : adenocarcinoma with numerous mitotic figures . treatment : dimethyl - chloroethylamine 2 mg . 
a corresponding effect in a tumour of the breast might reasonably be expected not to be noticed in support of such a suggestion is the fact that a similar relief by the patient . of respiratory symptoms following chloroethylamine without radiological evidence of changes in the lungs has been observed in a case of carcinoma of the breast with pulmonary metastases . 
by repeating the treatment at suitable intervals the life of animals with tumours can be prolonged , but cessation of treatment leads to recurrence of tumour growth . forty - one cases of histologically proven carcinoma of the bronchus unsuitable for other forms of therapy have been treated with the chloroethylamines . 
the original premise on which the present study was built was that if these three groups have any real existence it should be possible to demonstrate some differences in their natural history . a diagnosis that does not imply a prognosis is traditionally worthless ; not only is it of no practical value , but the difficulty of testing it leaves every opportunity it was proposed therefore to collect a series of rodent ulcers , classify for error . them according to foot 's ( 1947 ) criteria , and then to apply to them all available touchstones of clinical behaviour in the hope of being able to separate them . some such differences as those demonstrated by schrek and gates ( 1941 ) and schrek ( 1941a , 1941b ) between rodent ulcer and squamous carcinoma were sought . the attempt to do this , however , broke down unexpectedly early , for after our series had been collected it proved impossible to classify it on the lines proposed by foot ( 1947 )  . 
wells lesions with which foot ( 1947 ) dealt , it became clear that the great majority of tumours at the stage at which they are usually received by the pathologist are typical examples too various in appearance to admit of such simple treatment . of each class could be found easily enough , but there were so many mixed and intermediate and aberrant forms that no progress was possible . 
no modification of the classification could be devised that would avoid them . during a long interval in which the matter was left in this discouraging state , interest was deflected into a study of the pigmentation of rodent ulcers and of epithelial skin tumours generally which has already been reported ( lennox , 1949 )  . there emerged from this one possible way of classifying rodent ulcers , namely , into the pigmented and the non - pigmented . such a classification is almost wholly objective ; there either is or is not melanin in the tumour . contrast with the process of matching a tumour against a series of idealized types in the hope of being able to recognize a greater or less resemblance to one of them is very marked . it is true that the matching technique is reliable enough in the ordinary process of histological diagnosis , but where the types themselves are of doubtful existence it becomes open to great error . 
they are a large proportion of those received in this department in the years 1936 to 1948 . most have come from the radio - therapeutic research unit which was established in 1942 ; without its very full record system this study would have been impossible . cases have been rejected if the biopsy specimen was inadequate or if the history was deficient in any important detail , but an effort was made to include as many of the cases found as possible , partly because the available material was small , partly because any form of selection may profoundly and unpredictably influence the results of any study of this type . it was not possible to insist on more than a year 's follow - up , though most cases have had considerably longer ; the recurrence rate is therefore falsely low , though sufficient to provide some useful data for comparative purposes . surgical excision supplied 26 specimens ; diagnostic biopsies , multiple in 30 cases , were provided by 124 cases . most of the material was fixed in plain formalin - saline ; recent biopsies have been fixed in halfsaturated mercuric chloride in 15 per cent formalin - saline ( fss )  . 
the typical examples of this group seem distinct enough , yet it soon became obvious that transitional forms are numerous . wte therefore provisionally included the sub - group , and found later no reason to regret it ; we believe that these are merely the most benign and well - differentiated end of the rodent ulcer series ( the multiple and often familial tumours of brooke ( 1892 ) and fordyce ( 1892 ) we believe also to be of the same nature , though here we are extrapolating beyond our personal experience )  . in the second place , at the other end of the scale we find 11 tumours of the type illustrated in fig . 
we believe the evidence against the squamous nature of this sub - group is strong . within the typically squamous tumours a close parallel between histological dedifferentiation and clinical malignancy can be the most malignant epithelial skin tumour seen in this hospital demonstrated . in the last 4 years is that illustrated in fig . 
3 ; it grew very rapidly under observation and killed its host within 18 months of first appearance . less well differentiated squamous carcinomata should be even more malignant ; but all the tumours we have seen of the type of fig . 
2 have been relatively benign , and can be shown only by careful statistical analysis to differ in behaviour from the general run of rodent ulcers . inclusion of these two sub - groups harmonizes with the view of the rodent ulcer group developed later in this paper , as a series in which a gradation of differentiation can be recognized , with a definite though not very striking parallel gradation in behaviour . 
removal of these two sub - groups would not affect the general conclusions drawn , though it would reduce the level of significance of some of our figures . forms of differentiation chosen for analysis . only four common histological forms of differentiation in rodent ulcers could be defined well enough for analysis . 
some obvious features , especially those based on cell size and shape and on tumour cell group size and shape , had to be rejected because of the difficulty of establishing exact descriptive criteria and , more important , their great variability within any one tumour . 
some very interesting features were too infrequent in our series to justify detailed separate analysis : these were ( a ) keratin formation ( 11 cases , 7 ' 3 per cent ) , ( b ) hyaline stroma ( 11 cases , 7 ' 3 per cent ) , ( c ) squamous differentiation ( 4 cases , 2 ' 7 per cent ) , ( d ) " sebaceous " differentiation ( 4 cases , 2 - 7 per cent ; lipoid was not identified , and the recognition of these occasional foamy cell groups as sebaceous remains doubtful ) , ( e ) duct formation ( 1 case , 0 ' 67 per cent )  . the four forms of differentiation finally chosen were , in order of frequency , palisading , fluid formation , whorls and pigmentation . 
these presented the following advantages : ( a ) they were all common , so that sufficient cases were available for analysis , ( b ) their presence or absence could be readily determined , ( c ) between them they were responsible for a large part of the variation in appearance assumed by rodent ulcers , and ( d ) they were constant throughout the same tumour , varying 198 b . 
what form of degeneration of the stroma it can be we fail to see ; it is not myxomatous , it is only occasionally hyaline , and it is curiously localized if it is oedema . if one believes it to be stromal in origin one is driven to the proposition that it is an active secretion of the stroma - an unprecedented occurrence in an epithelial tumour , and one that in any case does not explain cysts within the epithelial masses . massive fluid production such as that of fig . 
by whorls we mean small spherical groups of concentrically arranged flattened cells , more eosinophilic than the bulk of the tumour and centred on an even more eosinophilic core ; this core often appears to be converted into a laminated plug of keratwe have counted nothing that did not have at least a trace of central eosinophilia , but think it possible to recognize even earlier stages of which the giant - cell - like structure seen above left centre in fig . 
9 may be an example . at least three interpretations of these structures have been offered : ( a ) they are cell nests ( parakeratotic pearls ) of basically the same nature as those of squamous carcinoma ( darier and ferrand , 1922 ; montgomery , 1928 )  . 
they differ from these in their smaller size , sharper demarcation , more concentric structure and lack of prickle cells , and usually also in the smaller amount of central keratin . ( b ) they are abortive hair follicles ( haythorn , 1931 ; warren , gates and butterfield , 1936 )  . 
the term " abortive " here is a convenient one ; it conceals the fact that the structures resemble no part of the follicle in any respect which will bear analysis . 
1. - a nodular tumour of the epithelioma adenoides cysticum type , only slightly cystic . note the position immediately deep to the epidermis , unrelated to hair matrices , and also the focus of abnormal epithelium , similar to that seen in early rodent ulcers , to the right of case 219 : from the scalp of a man of 33 , duration 22 years . 
14. - colonization of hair follicles by homologous epidermis in the rabbit . the epidermis and the epithelium of the hair follicles of the graft have died , but the stroma survives . 
and post - auricular area from pinna postauricular , 2 . is justified by the obvious difference in exposure , and by a difference in behaviour well marked even in the small number of cases involved . 
a preliminary test by standard error of the differences of the percentages in the 0 and 9 - 15 columns for each other and from the mean figures for the whole series gave in the event results differing little from those of more elaborate methods . 
wells it casts some doubt on the opinion earlier histological diagnosis is most difficult . it would , however , be statisexpressed that these tumours are all rodent ulcers . tically equally suspicious to find no such tumours . perhaps the group does include some spurious cases , but we have found no satisfactory way of determining which they are , and at least two alternative explanations , apart from chance numerical variation , offer themselves . 
boag , to whom we submitted the figures , pointed out that from nition . the statistical point of view they could equally be explained by a slight tendency to aggregation of the separate differentiations ; he was able to show that three of the differentiations ( melanin being the exception ) were rather more frequent in the presence of one than in the presence of no other differentiation , and a little more frequent still in the presence of two others . 
our four main differentiations are seen to associate in what appears to be an entirely random manner . put the case that there exists any histologically separable sub - group of rodent it is exceedingly improbable that ulcers , and that it is of any substantial size . any significant definition of such a group could be devised that would not involve at least one of our four main features . 
then infallibly the random grouping only if it is extremely small , or if it depends on criteria would be disturbed . which have so far escaped definition , can any such sub - group exist . of such possible sub - groups the most important , because the most widely accepted , is the " type intermediare mixte " of darier and ferrand ( 1922 ) which is the " baso - squamous " form of montgomery ( 1928 )  . 
we can find no real criterion of the diagnosis of this type of rodent ulcer except the presence of the " pearls , " and these do not appear to be anything except our whorls in their higher grades . montgomery ( 1928 ) states that his cases are more malignant and radio - resistant than other rodent ulcers . 
he gives no statistical evidence for this , basing it as far as one can tell from his original article on impressions of a small number of it will be clear that our series gives no support for the idea either of the cases . separate existence of such a group , or of the abnormal behaviour of tumours showing whorls . 
of our 54 cases showing whorls , 4 recurred ( 7 ' 4 per cent , compared to a general recurrence rate of 11 ' 3 per cent ) and 3 responded poorly to irradiation ( 5 - 6 per cent compared to a general rate of 9 ' 7 per cent )  . 
an analogy which seems justifiable is that of the parathyroids and the thymus ( the liver and the pancreas , or the enamel organ and the sublingual glands , or several other pairs might be used ) , which are equally closely related in their manner of origin , but yet , being histologically totally distinct structures , produce totally distinct tumours . foot 's ( 1947 ) manner of using the term primordium for the conical downgrowth of epidermal cells in which both begin obscures the fact that such primordia are not usually multipotential ; except in the few areas where sweat glands open into the mouths of hair follicles the two structures arise quite independently , and in most places at different times . we are impressed with the lack of truly organized structure in these tumours . we have already expressed our doubts about the so - called abortive hair follicles . one solitary tumour in this series ( unique so far in an experience of roughly twice the number of cases here reported ) showed reasonably convincing duct - like structures . 
wells hair matrix origin of rodent ulcers . mallory ( 1910 ) suggested that the rodent ulcer might arise from the hair matrix , and haythorn ( 1931 ) asserted that all rodent ulcers are simply hair matrix subsequent authors ( except wallace and halpert , 1950 ) have not tumours . accepted this completely , but no detailed refutation of his arguments has been attempted . 
they may , however , be shown to include several major flaws . ( a ) haythorn ( 1931 ) regards the connection of the tumour with the epidermis as purely accidental . 
we are not very impressed with the fibrils which we have been able to demonstrate ; in any case it seems probable that they are homologues of the tonofibrils of the rete malpighii , and that such fibrils form readily in any epidermal derivative , forming intercellular bridges which will be demonstrable as prickles wherever the cells are sufficiently separated . ( c ) haythorn 's ( 1931 ) identification of hair shafts we have already discussed . ( d ) we have been unable to confirm haythorn 's ( 1931 ) observations on the resemblance of the silver - stained basement membrane of rodent ulcers to that indeed it would be surprising if a hair matrix tumour of the hair follicle . developed a basement membrane like the " membrana vitrea " of the root sheath . we have not examined the neurofibril content of our tumours , but willis ( 1948 ) has indicated the unreliability of the evidence they provide . ( e ) haythorn ( 1931 ) describes atypical proliferations of hair follicles producing appearances which he interprets as the early stages of rodent ulcer formation . but nearly all these changes occurred in hairs surrounded by squamous carcinotheir occurrence is therefore rather to be taken as evidence that hair mata . follicles react in this sort of way ( it may be merely a disturbance of ordinary cyclical regeneration ) to any injury , and to be a warning that apparent transitional changes in hair follicles even within a rodent ulcer may be quite meaningless . ( f ) an argument which haythorn ( 1931 ) does not consider is that based on the site of origin of the tumours . 
where we find it necessary to disagree with them is in the assumption that this necessarily involves a specifically basal - cell origin . as von hansemann ( 1907 ) was first to point out , the surface epithelium and squamous carcinoma arise equally from the basal layer of the epidermis . seems , however , to be generally believed that if squamous carcinoma and rodent ulcer are different tumours they must have separate cells of origin . this is not necessarily so . 
at the time of first formation of hair follicles the epidermis possesses only a rudimentary " peritrichous " outer layer , and all the capacity for growth in either of its two main directions resides in one layer of cells . 
the stimulus to active keratin - ward proliferation ( whatever its proximate mechanism ) must be found in some contact with the external world - though there must be a basal level of activity of the degree seen in implantation cysts . 
the stimulus to the adnexa - ward proliferation almost certainly comes from some form of direct evidence for this in mammals is organizer - like action of the mesoderm . lacking , studies of hair genesis so far available ( danneel , 1931 ; trotter , 1932 ) being purely anatomical . 
but in birds , where the large size of the feather papilla makes transplantation experiments possible , the work of lillie and his school has produced a great deal of evidence on the process of morphogenesis ( lillie , 1942 ) , and it is known that the original stimulus to feather growth arises in the dermis ( wang , 1943 ) , though the type of epithelium responding to the stimulus partly determines the type of feather to be formed . in the absence of evidence to the contrary it seems reasonable to assume that in mammals hairs and sweat glands are evoked from the epidermis by similar stimuli derived from the dermis . thus we have two stimuli , two responses , and two very different forms of correspondingly we have two forms tissue formed from the same layer of cells . it is simplest ( though perhaps not entirely necessary ) to state the of tumour . resultant hypothesis in terms of pullinger 's ( 1949 ) theory of tumour origin in general . according to this , squamous carcinoma would be the result of the acquirement by epidermal cells of the ability to produce within themselves some stimulating substance which is normally only derived by external irritation , and rodent ulcer is the result of the acquirement by the same cells of the ability to produce an altogether different substance - a substance which is the normal stimulus to growth of the adnexae and which is normally derived only from the dermis . why then , if it results from the application of the same stimulus to the same tissue , is the rodent ulcer so poor a copy of hair follicle or sweat gland ? a possible answer may lie in the importance of the connective - tissue framework in the differentiation of adnexae , a matter concerning which there is some experimental evidence . 
a hypothesis is proposed ascribing the rodent ulcer to the autogenous production by the epidermis of a stimulus to proliferation normally supplied by the foetal dermis . our thanks are due to professor j . 
but for the extremes prognosis is definitelv affected in group statistics by the age at time of operation . in our e - xperience below the age of fortv vears axillary metastasis is much more apt to be present at the time of operation than bevond that age . in the s - ame , wav postoperative survivals . 
and the average postoperative hfe is shorter ( 16 - 7 months ) than in similar cases in the adult . " duk - es ( 1940 ) found that patients under the age of 40 vears had a higher incidence of lymphatic metastases than those in the age gmup 40 - 59 vears . 
they gave their opinion that the most malignant forms , both chnically and histologically , tended to occur at the younger ages . frissell and knox ( 1937 ) gave details of 46 cases of primarv lung cancer which on examining included - the age , and the duration of the - disease for each patient . these data we have found that there is no relation at all between age and the duration of the disease . 
he divided them into a carcinoma  . " group of 89 patients and an " epithelioma " group of 23 patients . he had no doubt that the clinical mahgnanev of the tumoiirs in the carcinoma group was greater in these patients than in older patients . 
undifferentiated tissue , often with manv mitotic figures in each field . " he found that h - valinization was never present that 1.ymphocytic infilltration and fibrosis were present to a moderate degree and only in the less mahgnant and that cellular differentiation was present mainlv in ovarian and tumours th - vroid carcinomas where . 
carried on through the cards and chose the first carcinoma recorded in the same organ and of the same sex in an individual in age group 46 - - 55 and again in a high age group . 
rectum ; and 61 vears and over for lung ( where the middle age group was 41 - 50 )  . for each tumour type we thus had three randomlv chosen groups of slides . 
the middle - aged and the old . ' the slides were then taken out of their holders and shuffled . this made identification of the sections impossible without reference to the laboratorv register of the numbers etched on the slides . 
ceu polymorphim and degree of fibrost - 3 ( scirrhous reaction ) the principle adopt . - d was to allocate grades i and iv to cases which were strikinglv low and strikinglv high respectivelv in these features . grades 11 and iii formed intermediate groups of " low moderate " and " high moderate respectivelv . for epidern " d differentiation the scale . 
 ' after completing the ' experiment , we were qiiite convinced that there was no such gross systematic change in type of material or standards of diagnosis over the years . 
we have , therefore , not considered that the difference between blocks arranged by date of diagnosis would appreciably reduce the residual error on which the significance of inter - age differences would be estimated . the experiment was therefore designed to allow for an analysis of variance . for example , in the sub - experiment " degree of glanduliform differentiation in rectal carcinoma " there was a total of 42 units or slides divided into 3 groups of 14 each for patients of 30 ygars or less , 46 to 55 years , and 70 years or more respectively , and divisible also into 14 groups of 3 each , i in each age group , diagnosed in an analysis of the variance in this balanced design in the same calendar year . there would then have been a total of 41 " degrees of freedom " comprising 2 for age , 13 for date of diagnosis , and 26 for residual error . 
of the 2 degrees of freedom for age , one could have been used to test the linearity of the difference in fact there was no need for this since a relatively coarse by age if necessary . analysis of the data indicated that the figures might we ] i have occurred by chance - on the hypothesis that there was no correlation between age and any of the factors we estimated . colloid ' formation " and " cell polymorphism , " using the total figures of each factor for for example , in the case of " epidermoid differentiation " there each age group . was a contingency table of the formthe x2 test was carried out for each factor , with the exception of the results for the various factors were epidermoid differentiation : 6 x2 4 - 95 p 0 - 7 - 0 - 5 . glanduliform differentiation ( consolidating grades iii and iv ) : 4 x2 = 4 - 55 p = c . 
at the begin9of the experiment , however , we laid down the hypothesis that we had no reason to expect significant results from one tumour type or characteristic more than another . it foflows that there is , so far as our results per se are coneemed , no rea - son to regard this as indicating a real correlation between age and increas ' epidermoid differentiation in bronchogenic carcinoma . it is notable , however , that in our reading of the literature the tumour in which the correlation between increasing differentiation and increa - sing age ha - s been most strikingly demonstrated ( geschickter and denison , 1934 ) is also bronchogenic carcinoma . consequently our figures , in so far as they are confirmatory , are also suggestive . we did , in fact , although we have not given the table , estimate , using the method of analysis of variance , the probabihty with which the figures for epidermoid differentiation and age could have occurred by chance for epidermoid differentiation of ( a ) bronchogeiiic carcinoma , ( b ) carcinoma of the cervix , ( c ) carcinoma oflip . 
causes an almost complete cessation ofepidermal mitotic activity , and the same effect is caused by phloridzin , which interferes with the phosphorylation of sugar . since insulin and phloridzin both exert their mitosis depressing effect bv reducing the availabifity of sugar , it appeared probable that a similar depression would also be induced bv starvation . 
12 hours of starvation the blood sugar level remained fairlv high , but the drop in the mitosis rate was pronounced . however , during the afternoon sleep period there was a marked rise in mitotic activitv at 14.00 hours to a figure of 4 - 1 0 - 35 , which is about half the figum reachc ; l by the well - fed controls . - after 24 hours ' starvation the blood sugar level had faren seriously , and mitotic .1gain , however , there was a slight activitv had reached a very low level . response to the period of rest , so that at 14.00 hours a figure of 2.0 0 - 21 was this is about a quarter of the figure for the control animals obtained . ..a&r 36 hours the blood sugar concentration had dropped to 100 mg . 
observations were next made on the effects of such diets on epidermal mitotic acti - %ity . in prehminary experiments determinati ' ons were made of the dailv food intake of threeor four - monthold strong cba males which were allowe ; 1 to feed ad libitum on a diet of rat cake . 
13ttllo ' ug14 66 per cent diet remaitied active aiid in excelleiit health , btit those which received a 50 per cent diet showed sigiis of ill - health , and it is dotibtftil whether they could have stirvived the treatnieiit for i - iiore tliaii another few ' weeks , at the end of the experiment at 20.00 hours all the niice wei - e killed and blood sugaiestimations were made . 
that middle age is characterized bv a generallv raised mitosis rate which must itself assist in the development of any latent tumour cells which may be present . ll ' hfle the reason for the increased initotic activitv is still obscure . 
this observation mav afford some explanation of the fact that middle age is characteristically the cancer age . since the development of latent tumour cells is assisted bv conditions of hyperplasia , it is reasonable to suppose that conditions of hypoplasia wih have the hyperplasia increases the chances that the latent tumour cells opposite effect . will be stimulated to multiplv . 
and so delavs the development of those tumours which do forand prevents altogether the appearance of manv which otherwise would forthus it is possible to provide a logical explanation of tannenbaum 's re - sults . 
and the fact that carbohvdrate - supply is the critical factor in both cell division and tumour genesis can be taken as corroborative evidence . at last it iis becoming possible to split the cancer problem into two separate parts : that which is coneemed with the formation of latent tumour cells . 
but it now appears possible that a practical control of cancer mav be developed from a thorough understanding of those factors which govern normal cell division . if hypoplasia can be maintained without damage to health . 
and reveal fewer pathological changes in the tissues . " this mav well be related to , the fact that hypoglyeaemia not onlv reduces the rate of cell division of a host . but also that of a parasite . 
a sin - iilar effect is produeed bv restricted diets . - kninials rationed to 66 per cent of what thev would eat if fed .4 , libitunt have an epidermal mitosis rate which is less than 40 per cent of that of well fed controls . if rationed to 50 per cent . 
the mitosis rate dxops to about 15 per cent of that of the controls . it is suggested that these observations provide an explanation of tannenbaum 's results on the prevention of tumour genesis bv diet restriction . 
mottram ( 1945 ) published the results of experiments designed to demonstrate a relationship between the tumour yield induced by benzpyrene and the number of epidermai mitoses present at the time of application of the carcinogen . painting the skin of rnice at midnight resulted in a higher yield ofpapillomata than did painting at midday . 
of 9 : 10 : dimethyl - 1 : 2 - benzanthracene ; specific tumours of the thymus and lung , which are prone to spontaneous tulour developmnent in this strain , were induced by this treatment , whereas the mammary and subcutaneous tissues which are also prone to spontaneous tumour developmnent did not respond . the testis and kidney , in which spontaneous tumours have never been observed , and the spleen , lymph nodes and bone marrow , inl which tumours are not presumed to develop spontaneously , also proved insusceptible to this slight carcinogenic influence , and did not respond to a very powerful direct carcinogeniic influence . 
paraffin of the same batch as that used for analogous experiments performed with 9 : 10 - dimethyl - 1 : 2 - benzanthracene ( engelbreth - holm and rask - nielsen , 1947 ; rask - nielsen , 1948 )  . the technique of application was the same as that used in earlier experiments . 
rask - nielsen zanthracene - induced specific tumours , lymphosarcomatous hyperplasia of the thymic gland in 1i7 per cent , 6.7 per cent , 10 4 per cent and 13 per cent , the effective total being the number of mice whose survival time was at least that of the youngest tumour - bearing animal within all four groups , namely , three months . in addition a thymic spindle - cell sarcoma was found in one animal injected with methylcholanthrene . injections of three of the hydrocarbons into the lung induced thymic tumours in 2 , 2 and 4 per cent following the injection of benzpyrene , dibenzanthracene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene respectively . 
the average latent period , the interval between injection and the death of the animal , following injections into the thymus of benzpyrene , dibenzanthracene , methylcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene was 15 , 14 , 16 and 21 weeks , respectively ; the minimum latent period of the three latter hydrocarbons was 11 , 14 and 10 weeks , respectively . 
analogous negative results were observed by others , using mice from various strains ( esmarch , 1940 ; strong and smith , 1939 )  . experiments including the nho strain of mice , however , exhibit positive results ( strong and smith , 1939 ; strong and williams , 1941 ; strong , 1945 )  . 
from these experiments it is rather difficult to form an estimate of the susceptibility of the mammary tissue to carcinogenic hydrocarbons , since susceptibility is dependent on simultaneous hormonal stimulation as well as on the presence of the milk agent . since the present experinments included only non - breeding mice . 
the hormonal stimulation was at least not maximal . street mice have been used in all the experiments recorded here and the deductions made apply only to mice of that strain . the susceptibility to carcinogenic action of various tissues being genetically determined ( lefevre , 1945 ) it is necessary , in order to elucidate the susceptibility to a direct carcinogenic action of a particular tissue , to examine animals from different strains under identical experinmental conditions . such investigations , for the time being with application of 9 : 10 - dimethyl - 1 : 2 - benzanthracene to the thymus , lung and subcutaneous 116 r . 
fodden. from the department of pathology , university of liverpool , and the liverpool cancer control organization . received for publication august 20 , 1948 . in his ' textbook of pathological anatomy ' rokitansky ( 1861 ) made his classical statement that pyloric cancer was exactly bounded by the pyloric ring , and that the growth never reached beyond into the duodenufrom this time it appears that the majority of observers , with the early exception of brinton ( 1864 ) , commented upon the integrity of the duodenum in cases of carcinoma of the stomach . 
many well - known surgical teachers spoke of the habitual immunity of the duodenum from invasion . kocher ( 1893 ) , mikulicz ( 1898 ) and most ( 1899 ) believed it to be always constant . kocher ventured that it was a problem of extreme interest to consider why gastric carcinoma grows in almost all cases towards the cardia , yet stops , on the contrary , at the duodenopyloric junction . it was brinton who first took especial exception to this proposition of rokitansky . 
he brought against it criticisms founded upon numerous personal caseobservations : " we may justifiably apply to it a criticism of unusual severitya criticism which , even if it weigh every word , will scarcely do more than the author 's ( rokitansky 's ) terse and weighty proposition really deserves . " from 125 cancers of the pylorus studied by brinton , there were no less than ten cases in which the disease was not bounded by the valve , but passed beyond it for a variable distance , often an inch or two inches , into the duodenuhe gave no information concerning the method of this spread . brinton concluded by saying the rules which rokitansky had the merit of laying down were , in this respect , like many others in pathology , of general though not of universal importance ; their value was not much affected by occasional exceptions . this question of duodenal invasion by pyloric cancer seemed to present a surgical problem of out of a large series of gastric carcinoma cun6o ( 1903 ) took 11 j . 
fodden some magnitude , and the frequency and degree of its occurrence has been the object of several subsequent researches . carle and fantino ( 1898 ) , discussing the pathology and treatment of carcinoma of the stomach , expressed disagreement with kocher . they mention three cases out of fourteen gastric resections in which neoplastic infiltration had spread under brunner 's glands for a distance of one to three centimetres . in addition , these authors stated that such a progression of the growth towards the duodenum necessitates an extension of the surgical resection as far as the second part of the duodenum . other later surgical authors , notably borrmann ( 1901 ) and cuneo ( 1903 ) , attached considerable importance to brinton 's " occasional exceptions " with reference to the spread of cancer into the duodenum . cuneo ( 1900 ) , during his classical work on the lymphatic propagation of pyloric cancer , was already investigating the accepted state of immunity of the duodenuhe remarked on the disaccord between the macroscopic aspect - the abrupt termination of a gastric cancer at the level of the pylorus and the results of the histological examination . this examination systematically diminished , he said , the percentage of the duodenal integrity . cancers of the pylorus , and subjected their distal extension to a critical macroscopic and microscopic examination . 
but , he goes on to say , it is impossible to ignore the fact that such a wide resection complicates the operation , and necessitates a dissection of the duodenum from the pancreas . the researches of fenwick and fenwick ( 1902 ) do not lend support to brinton 's findings , as they discovered out of a series of 87 pyloric cancers only 2 cases which demonstrated lymphatic spread into the duodenum . these authors remarked that though malignant growths of the pylorus may project into the lumen of the duodenum , they rarely implicated its walls . however , it is open to question whether their histological investigations were sufficiently careful to give reliable evidence , and the conclusions they advanced could scarcely have been founded upon their own results . moynihan ( 1926 ) was very familiar with the possibility of duodenal permeation in gastric cancer , and stressed that the duodenal integrity was more apparent than real . 
he quoted several of the authors already mentioned , and advocated the removal in all cases of pyloric cancer of the whole of the first portion of the duodenum . sherren ( 1932 ) , describing the methods of spread of gastric cancer , mentioned his own surgical familiarity with duodenal infiltration by carcinoma . 
a study of the microscopical anatomy of this region , in relation to the morbid process in situ , may help to clear up some components of each problem . to cun6o ( 1900 ) the apparent arrest of a cancer at the pylorus was due , for him it depended upon an absence of conabove all , to a mechanical cause . tinuity between the gastric and duodenal submucous spaces - a continuity broken by the annular muscle of the pylorus , and by a condensation of cellular tissue within the submucosa to form a dividing septum . his gelatine injections into the gastric submucosa near the pylorus met with an " invincible obstacle . " at the same time he admitted that though it would be ludicrous to consider such barriers as absolute in opposing gastric cancer , they still played the principal role in the protection of the duodenum against neoplastic invasion . for brinton ( 1864 ) and for fenwick and fenwick ( 1902 ) the reason was again anatomical . 
the muscular coats of the two viscera along the line of fusion were so distinct from one another that a direct continuity could scarcely be said to these authors made the analogy between the duodenal attachment to exist . the stomach and the manner in which the vagina embraces the neck of the uterus . to them a growth of the pylorus was more apt to infiltrate the contiguous walls of . 
in their opinion it was obvious that the duodenum may possibly be invaded from the pylorus by the in addition , extension of cancer along the submucous and subserous channels . both jamieson and dobson and cun6o emphasized the final possibility of retrograde lymphatic spread . 
as these nodes also receive vessels from the that this may be of some duodenum , an indirect communication also exists . importance was stressed by moynihan ( 1926 ) when he says that the implication of a single gland may so sufficiently disturb the direction of the lymph current that cancer cells from a primary growth may pursue an erratic course . horton ( 1928 ) working upon stomachs removed from young subjects one to three hours after death , injected 35 with coloured gelatine or indian ink . 
two of the present surgical specimens were small cancer - ulcers upon the lesser curvature of the pyloric antrum , and cancer had invaded on the gastric side only the submucosa , with extension in one case into the pyloric sphincter muscle . 
yet both these specimens showed cancer islands within duodenal lymphatics at a distance of almost 1 ' 5 cfrom the pyloro - duodenal junction . this was also instanced by a cabot case no . 
25472 ( 1939 ) of the massachusetts general hospital , in which specimen a small malignant ulcer of the pylorus was limited to the mucosa except for a small extension below the muscularis mucosae . 
the only structure apparently offering any kind of barrier action was the gland layer of brunner . it has been the experience of the majority of authors that the layer of brunner glands remains free , in spite of many , and long , extensions of gastric cancer beyond the pylorus . in addition , whatever the method of propagation , it is exceptional that the mucosal epithelium of the 246 j . 
a resection of almost 3 cof the duodenum was made . microscopically the duodenal growth was so proliferative in the muscular and serous layers that one could not avoid an impression that an even greater length of duodenal resection would have been advisable . 
davie for his help with the plan of this research during its initial stages , and those pathologists and surgeons of the liverpool regional hospitals who have so kindly supplied me with specimens and helpful data . 
as none of these other cell types are seen in the typical rodent ulcer , the lesion must be considered as being completely undifferentiated . but such a tumour should be highly malignant , more so at any rate than the ordinary keratinizing squamous cell carcinoma . this difficulty is resolved by the more recent view , apparently a revival of krompecher 's first thoughts on the matter , which relates these tumour , not to the basal layer of the epidermis , but 214 a . 
thackray to those accessory structures of the skin derived from the surface epithelium , the haythorn ( 1931 ) for example , relates the tumours hair follicles and sweat glands . in nearly every case to existing hair follicles and matrix , regarding any connection between epidermis and tumour tissue as secondary and fortuitous . 
some workers find it difficult to reconcile an origin in the hair matrix , which is comparatively deeply situated , with the superficial situation of early tumours . but hairs have a definite life span , at the end of which they atrophy , are shed and replaced . 
the pilar type , which included about threequarters of the tumours in his series , he further subdivided into a pilar type proper , a primordial type , a cylindrical celled or " ribbon " type , and a cystic type . 
from this large number 200 cases were finally selected to form the basis of the present investigation . the selected cases were all those that fulfilled the following conditions : 1 . 
the sections available did not always include the whole lesion , but where this was so a note was made as to whether excision appeared to be complete , incomplete or doubtful . 
of the 12 cases which recurred , 8 were obviously incompletely excised , one appeared to have been completely removed from the section studied , and 3 were doubtful . of the 51 successful excisions , 42 had been removed with an adequate margin of healthy tissue , one tumour reached to the limit of excision , and 3 came so near to the edge that the outcome seemed doubtful . in the remainder the sections available did not cover the whole lesion and no opinion as to completeness of removal could be given . of the 12 failures with surgery , one was cured by further excision , and 4 more by irradiation . three of the remaining 7 died as a result of the disease , unchecked by further surgery or irradiation , 2 patients are still alive with the ulcer active , and the other 2 died of other causes with the ulcer uncured . 
of these 39 ulcers , 19 were soon cured by further treatment , leaving 20 which proved radio - resistant . it is proposed to compare the incidence of various histological features in the biopsies from the 82 lesions cured by a single course of radiotherapy with their these figures incidentally introduced incidence in the 20 radio - resistant ulcers . must not be considered as representative of the results of radiotherapy by modern methods , for it must be remembered that these cases were all followed for 10 years , the most recent treatment being therefore in 1938 . influence of size of lesion on prognosis . before considering the histological analysis of these cases it is interesting to note the influence of the size of the lesion on the prognosis . 
the greatest measurement of the ulcer in inches was noted on the cards , and these sizes were then divided into two groups , large and small , taking one inch or more as the criterion of largeness . this boundary between large and small was placed quite arbitrarily and in fact there proved to be about twice as many small lesions as large . of the surgically excised lesions , the size had been noted in 51 cases , and of these 16 were large and 35 small . 
thackray influence of type of lesion on prognosis . as has been described already , the lesions were classed on their histological appearance as being circumscribed ( group i ) , predominantly circumscribed , but with early infiltration present ( group ii ) , or infiltrative ( group iii ) in their type of growth . it was hoped that this classification might give an indication of the malignancy of the tumours without introducing controversial problems concerning their origin . it may be suggested that the infiltrative lesions are the large and advanced ones , and that any correlation we may note between type of growth and prognosis will merely be a repetition of what we saw in the preceding section . 
the whole series of surgical cases , including also those in which surgical excision was combined with radiotherapy in the first instance , was therefore grouped as to size of lesion and type of growth . 
the great majority of the lesions with no palisade formation apparent on section were of the infiltrative variety , whereas in the group with well - marked palisades 30 were circumscribed ( group i ) and 19 infiltrative ( group iii )  . 
the question of metastasis does not arise , and it is only necessary to be sure that the margin of the excised tissue is free from growth . this can be done by cutting serial sections of the excised tissue , which is well worth while if there is any doubt . if serial sections are not prepared , then the nature of the growth itself gives a fair indication , for tumours of the circumscribed type , as we have called it , are relatively compact and their extent is apparent from the surface , whereas infiltrative growths extend beyond their apparent limits . when considering the results of radiotherapy it is important to distinguish clearly between radio - sensitivity and radio - curability . 
a tumour which melts away when irradiated may often recur , whereas the tumour which can be destroyed curing the patient , may show no dramatic immediate response . in this investigation the ten - year cure is the criterion of successful treatment , so that radiocurability is all we are concerned with . it is well known that the histological grade of malignancy as applied to carcinomas of the skin , say , or breast , has some bearing on the outcome of radiotherapy - those of low - grade malignancy often being curable , those of high malignancy usually being sensitive , but recurring . in carcinomas of the breast such features as the degree of tubule formation , variability in size and staining of the nuclei and the frequency of mitoses are all significant , and are taken into account in determining the grade . 
the results of the present investigation have been largely negative , for most of the histological features of rodent ulcers considered have been shown to be without significance in assessing the probable outcome of treatment . 
thackray the presence of cysts , pigmentation , nor even the number of mitoses seem to have any bearing on the question . the only method of dividing up the tumours which seemed to bear any relation to the prognosis was that based on the habit of growth , into circumscribed or infiltrative , and the fact that an intermediate group was necessary indicates grading as practised in connection the difficulty in making this distinction . with carcinomas of the breast and elsewhere is an indication of the degree of malignancy of malignant tumours ; the term " group " has been used here rather than " grade " in view of the suspicion that many of the group i tumours are probably in actual fact benign . 
of the other histological features studied , only the extent to which growth is infiltrative seemed to have a direct bearing on the prognosis and prospect of cure by radiotherapy . my thanks are due to the surgeons of the middlesex hospital and to professor b . 
korteweg. from ae antoni vanleeuwenhoek - hui8 , am8terdam . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . it was shown by little et al . 
korteweg ( 1936a , b ) predicted that chromosomal factors must also be active . this prediction was based on the fact that differences in susceptibility to cancer exist between dba females and the fl hybrids of the dba x c57 black cross . 
the present paper concems these chromosomal factors . the fact that chromosomal factors exist is important , but the way they act , their mechanism , is of still greater inter ' est . 
a number of investigators have considered the role of the follicular hormone , and checked the possibility of differences between the oestrus cycles of the high - cancer and low - cancer strains of mice . 
as no differences were found this form of experiment was discontinued . yet i was not convinced . i spayed females of different strains , and afterwards determined the sensitivity of the vaginal epithelium to oestrone by means of the vaginal smear method . i found - that , to cause oestrus , it was necessary to inject three times as much oestrone into females of the high - cancer strain dba as in those of the low - cancer c57 black . 
the ovaries of our high - cancer strain greatly sur ass those of our low - cancer ammals this is partly caused by the somewhat greater num ' ber of graafian in volume . follicles , partly by the much greater number of corpora lutea , and partly by the r . 
hooker ( 1945 ) recorded that the effect of progesterone can be demonstrated in ' the structure of .the endometrial stroma just as well as the effect of i have found that the epithelium of the uterus of the virginal mouse oestrone . also shows a response to progesterone . 
as in the endometrium of the human female , in which on the 17th day of the cycle , shortly after the bursti ' ng of the follicle when the luteinizing process is beginning , a vacuole becomes visible in the basal pait of the epithelial cells , so also this phenomenon occurs in the virginal it is the ' refore necessary to be aware always of the possibilitythat mouse . progesterone too may influence susceptibility to cancer ( by its synergistic ' action with oestrone )  . if the mammary glands ' also of high - cancer strain mice should be relatively insensitive to oestrone , as is the vaginal epithelium of high - cancer strain animals , then the excess of oestrone produced would probably be harmless to the mammary glands . if , on the contrary , the sensitivity of the mammary glands of highand low - cancer strain animals should be the same , the excess of oestrone produced in high - cancer strain animals might be injurious to the mammary glands . it therefore became necessary to determine the 'sensitivity to oestrone of the mammary glands . 
of oestrone into 21 - months - old spayed females of different str ' ains , it seemed evident to van gulik and myself that our high - cancer strain females dba reacted to a lesser degree to oestrone than our low - cancer strain animals when judged by the extent of development of the glands . in 21 - m ' onths - old castrated males injected with 13 i.u. 
of oestrone , we found more growth also in the low - cancer than in the high - cancer miihlbock then drew our attention to the fact that in our experiments strains . we had injected large doses . if one wishes to determine the sensitivit ' y of an organ it is preferable to determine the threshold dose '  . 
as the first visible sign of an effect of oestrone , miihlbock ( 1948a ) took the beginning of budding of the end of the milk ducts ( swelling of the end bulbs )  . 
firstly in the males of the three strains c57 black , dba and 020 , the sensitivity of the mammary gland is about the same according to the threshold test . secondly , the minimal dose causing budding ( swelling of end bulbs ) in castrated males is approximately five times less than in non - castrated males . obviously in non - castrated males the testosterone largely counteracts the oestrone . this supposition proved to be right , as in castrated males which were injected both with oestrone and testosterone , the presence of the latter suppressed the action of the former . in noncastrated males three times as much oestrone is needed to cause budding ( swelling of end bulbs ) in the glands of high - cancer strain dba mice than in those of lowcancer strain mice ; in castrated males the sensitivity is the same . 
the substance , usually dissolved in tyrode saline , is added to a culture after a dividing cell in mitosis therein has been selected fgr study , and the reaction of that cell to the agent is recorded for a period usually less than one hour . 
the cells in prophase then to be found in the outgrowth of the stained cultures were subsequently counted . the effects on mitosis of three phosphorylated naphthohydroquinones have been studied in this work . these are as follows : 1 . 
the di - methyl compound was found to be slightly less active than synkavit as a mitotic inhibitor in vitro . it again potentiates the effects of irradiation . further work on this substance is in progress , including clinical trials . normal mitosis in the chick osteoblast . osteoblasts were chosen for this work on the grounds that clear phase contrast pictures of them can be obtained during mitosis , and that they appear to be much less sensitive to light than are other fibroblast types of chick cells . in previous papers there has been described the normal course of cell division which can be observed under the phase - contrast microscope in living osteoblast cultures ( hughes and fell , 1949 ; hughes , 1949b )  . 
the nucleoli and nuclear membrane disappear remarkably rapidly at the end of prophase , but while the spindle is being formed several minutes pass before the chromosomes assume their equatorial position as a metaphase plate . it is convenient to speak of all this period after the loss of nuclear membrane and nucleoli as metaphase , and to separate an early from a late division of this phase of mitosis , respectively before and after establishment of the metaphase plate . the general cytological effects of compounds , i , ii , and xx viii . in the present work over fifty film records of the behaviour of dividing cells under the influence of these substances have been made . 
20. - cell from the outgrowth of a culture treated with 5 x 10 - 7 m synkavit ( i ) for 40 cell has undergone mitosis with the suppression of cleavage . 
nucleoli still present 5 mlater ditto , ditto , 10 mlater 3.5 x 10 - 6 m metaphase metaphase plate metaphase late prophase early metaphase 4 x 10 - 6 m prophase . 
the methylfree substance exerted this effect in late telophase over a range of dilutions of about one thousand - fold ( 27 , 3 x 10 - 9 m ; 36 , 1 x 10 - 6 m )  . 
at higher concentrations the substance rapidly kills both dividing and resting cells ( 38 , 1 x 1o - 5 m )  . it is noteworthy that although the effect of the methyl - free compound differs considerably from those of the methylated derivatives , both in the types of inhibition and the dilutions at which they are exerted , yet in the present data there are no significant differences in the maximum concentrations of each of the three substances at which a cell has been observed to undergo a normal mitosis ( synkavit , 17 , 18 , 19 ; di - methyl compound 25 , 26 ; non - methyl 36 , 42 )  . one point in the mitotic cycle on which these three substances do not appear to exert any immediate effect is the entry of cells into prophase . early prophases are still found in cultures treated with these substances at the highest concentrations which have been used in the course of this work . since synkavit and the di - methyl compound can interfere with the division of a cell in several ways , a culture which has been treated with these substances at appropriate dilutions for periods of an hour will show a variety of effects . these depend both on the individual sensitivity of the cells and the phase of mitosis which they had reached at the time of adding the substance . 
the fate of a particular cell selected for photography is , therefore , to some extent a matter of chance . it may be that the 55 instances which are recorded in table i do not exhaust these possibilities , though study of the whole cultures after fixation has not so far revealed any other types of inhibition . the variability of the behaviour of cells towards these substances , however , extends further than to inhibition at different stages of mitosis . treatment of a culture with a concentration sufficient to arrest and damage some dividing cells will leave unaffected others which continue a normal mitosis . this fact can best be illustrated by comparison of the effects of synkavit in a number of instances where it was applied to cells early in.prophase. 
at 1 x 10 - 6 m a normal mitosis ( 59 ) , an arrest in metaphase ( 60 ) and a clumping of chromosomes and cell oedema at this stage were recorded ( 52 )  . 
when the di - methyl compound at 4 x 10 - 6 m was added to cells in metaphase , there were seen both a normal mitosis ( 26 ) and an instance of clumping of the chromosomes ( 24 )  . this circumstance must be borne in mind in the search for any further generalisations from however , one other conclusion clearly emerges , namely , that the these data . effect of these substances on dividing cells is greater when they are applied at early stages of mitosis . 
with synkavit at 3 * 5 x 10 - 6 m addition to a cell early in metaphase resulted in clumping of chromosomes and oedema ( 15 ) , while later in metaphase in two instances this concentration was not found to be inhibitory ( 18 , 19 )  . 
it is probably true to say that phase specificity is most marked with substances to which the cell in division is much more sensitive than during the restthus , for instance , the action of colchicine on the dividing cell is ing stage . restricted to its effect on the mitotic spindle , and this is exerted at dilutions much greater than those necessary to affect intermitotic cells . 
the proportion of cells entering prophase thus , this substance appears to penetrate the cell memhas then decreased . brane so slowly that a concentration within the cell sufficient to provoke these effects is not reached for several hours . 
the secondary fusion of the daughter cells in late telophase which has been observed in the course of the present experiments may well be due to an alteration in the properties of the cell surface . 
a large number of binucleate cells were seen in stained cultures after treatment for 6 hours with this substance at concentrations of 1 x 10 - 9 m . this effect may be due either to secondary fusion of the daughter cells , or to an inhibition of cell cleavage in the first instance . finally , the value of the two general methods of investigations of the action of chemical substances on living cells in culture can be compared . in the one mainly used in the present work the effects of the agent on a single living cell in the culture is followed ; in the other a quantitative analysis of the whole culture is made after fixation and staining . 
where the effects of a given treatment often differ from cell to cell , it would be unwise to draw here the quantitative conclusions from the study of only a few examples . analysis of large numbers of cells is indispensable . 
cells may be inhibited at any point in mitosis , though their entry into prophase is apparently unaffected under the conditions of these experiments . arrest in metaphase and clumping of the chromosomes is the most common effect . individual cells vary greatly in their sensitivity to these substances . 
at sub - lethal concentrations the latter does not affect the course of mitosis until late in telophase , when to a varying extent the daughter cell re - unites . we wish to thank a . 
niicleoprotein , are believed to play an important part in cell reproduction , but their basic functions have recently developed analytical techniques , particularly not been elucidated . chromatographic analysis and the use of the ultra - violet spectrophotoilieter , have produced considerable fresh data on the composition of the nucleic acids , but much less research has been done on the protein fractions . this paper collects some information on this topic and some analytical results obtained in our laboratory are presented . the proteins found in the nucleus . mirsky and pollister ( 1946 ) were able to dissolve nuclear nucleoprotein in 1 m sodium chloride , after first removing the cytoplasniic material with 014 m saline , and to isolate this nucleoprotein by diluting the solution to a salt concentration of 014 m , when it precipitates in fibrous form . similar material could be obtained from isolated nuclei ( dounce , 1943 ) confirming that these nucleoproteins were of this extracted material was found to consist of deoxyribonuclear origin . nucleic acid and two protein fractions , one of which was classified as a histone , being readily soluble in acid and precipitated out of solution by ammonia . 
from isolated nuclei , apparently failed to do so from the chromosomes , and therefore claims respecting the identity of tr.pr. and the residual chronlosomes must await analytical confirmation . 1 - t is of special interest that cells which could be considered metabolically active ( liver , kid ' ney ) contain as mucb . 
as 50 per cent of the total isolated chromosome material in the form of residual chromosome . stedman and stedman ( 1943 , 1947 ) also isolated an acid - insoliible protein from the nucleus which they termed " chromosomin , " believing that it was the structural protein of the chromosome and that in the nucleus it was embedded in a support of nucleo - bistone . 
the work of both mirsky ( 1947 ) and stedman and stedman ( 1943 , 1947 ) seems to indicate that a protein forms the basic structure of the ebromosomes though the part played by the nucleic acid and the histone this is an important aspect but cannot be discussed here . 
from this material they isolated nucleic acid and histone , and in addition a fraction with isoelectric point between 5 - 8 and 6 - 15 , which coiistituted an appreciable proportion of the nuclear proteins . 
the evidence suggested that the fraction contained a sulphur - containing protein with an acidic isoelectric point and a protein of globulin typeif this material was , indeed , of nuclear origin , then this fraction appears to correspond in properties with the " chromosomin " ' of8tedmanandstedman ( 1943 , 1947 )  . 
the nuclei and chromosomes were fi - rst extracted with i m sodi - um chloride and then the residue was extracted with dilute sodium hydroxide . acidification cf this extract precipitated a protein which contained about 6 per cent arginine and since the nucleoprotein extracted from the nuclei has been no nucleic acid . shown to contain nucleic acid histone and tr.pr. , the alkali soluble protein here must be of different character and this is more likely to be the protein of the finally , two russian workers residual chromosomes than the tr.pr. 
fraction. ( zbarskii and debov , 1948 ) have reported that the protein remaining after the extraction of the nucleoprotein consists of two fractions , one of which is weakly acidic in character , being soluble in dilute alh - ah and having an isoelectric point 132 d . 
da - vidson and lawrie ( 1948 ) , using paper chromatography , carried out qualitative analyses of specimens of histone and non - histone ( acid - insoluble ) proteins from nuclei of calf thymus , rat liver and fowl erythrocytes . the histones contained alanine , arginine , aspartic acid , glutamic acid , isoleucine , leucine , ivsine , phenylalanine , proline , serine , tyrosine , valine and one unidentified constituent . in addition to the above amino - acids the acid - insoluble portein contained i per cent tryptophane , glycine but no lysine , and a further unidentified component . in silnilar studies khouvine and gregoire ( 1949 ) have analysed nuclear nucleoprotein from rat epithelioma and compared it with that foiind in the surrounding nectrotic the acid - extractable proteins nn - ere compared , using paper chromatotissues . graphy and found to be qualitatively the same . very recently stedman and stedman ( 1950 ) have reported arginine contents of histones from various tissues and found they all contained about 28 to 30 per cent arginine ( as per cent of total nitrogen )  . in addition these workers claim to have isolated sub - fractions of the histone of different composition , but no details of the n - iethod of extraction or fractionation are given . importance has often been attached to the tryptopbane content of the nuclear generally speaking , histone specimens have been found to contain proteins . 0 - 0 per cent to 0 - 1 per cent , while the acid - insoluble proteins have about 1 - 0 per cent tryptophane . stedman and stedman ( 1 - 947 ) believe that the presence of tryptopbane in histone is an indication of impurity . mirsky and pollister ( 1946 ) found very small amounts of tryptophane in histone , but about 0 - 8 per cent in the tr.pr. 
of the other histochemical studies reference will only be made to the recent work of thomas and steinitz ( 1950 ) using a method which will stain proteins of high arginine content in paraffin sections . 
the application of this method has indicated that the ratio of arginine - containing protein ( histone type ) to total possibly a combination of this technique protein , is greater in normal epidermis . with spectrophotometric methods will give further data on the localization of the basic proteins in the nucleus . extracted histone has been tested for bactericidal action ( nnleissman and graf , 1947 ) and the pharmacological properties of histone from avian erythrocytes bave also been studied . 
the nitrogen content of histone from both the above materials was 18 - 2 per cent . the acid - insoluble protein was prepared from the whole protein of the nucleoprotein , separated from the nucleic acid by the method of sevag , lackman and smollens ( 1938 )  . 
the solvent n - bu ' tanol - acetic acid - water ( 4 : 1 : 5 ) was used , followed bv either collidine - lutidine - water ( 1 : 1 : 4 ) or phenol - water . the papers were sprayed with 0 - 2 per cent ninhydrin and heated for 6 minutes at 100 ' c . 
to develop the characteristic ninhydrin - amino - acid colours . reference mixtures , " , , ere alwavs run at the same time . in the acid - hydrolysates of three specimens , histone and the acid - insoluble protein from thymus gland and histone from rat sarcoma , exactly the same comindeed , by this qualitative method it was not possible to ponents were found . detect any differences in composition in three fractions . all contained the following aniino - acids : alanine , arginine , aspartic acid , glutamic acid , glycine , bistidine , isoleucine and leucine , lysine , phenylalanine , proline , serine , threonine , tyrosine , were detected . 
for each analysis except in the case of the solvent ( c ) , wben half this amount was used to avoid excess of water on the coluinn . columns of potato stai - ch i cdiameter and 30 clong were used in conjunction with the following solvents : ( a ) n - butanol - n - propanol - 0 . 
moore and stein ( i 949 ) studied the recovery of individual amino - acids from mixtures and found that the chromatographic procedure on starch columns is capable of yielding recoveries of 100 3 per cent . their average recoveries were well within this rang - e and the sum of the aminoacids was almost invariably accurate to i per cent . 
by separate analysis no appreciable amount of trytophane could be found in the histone specimens . less than 0 - 04 per cent was found using the colorimetric method described by spies and chambers ( 1948 )  . 
protein was indicated in the rat sarcoma histone . the thymus histone specimen was quite negative in this test . comparing the two specimens analysed , there are no striking differences in composition . 
stedman and stedman ( 1943 ) believed that their acidinsoluble material ( chromosomin ) , despite a high content of the basic amino - acids must also contain a relatively large amount of glutamic acid . 
the present analyses do not support this claim . since the two proteins , histone and the acid - insoluble ty ] pe are so similar and are extracted together , it seems possible that they may be bonded together in the cell and are subsequently split by the extraction techniques to give basic soluble histone and a denatured " sulphurhistone " product . no considerable differences have as vet been found in the nuclear proteins of normal and neoplastic tissues . there are some small differences in the aminoacid compositions and there is evidence of ' variation in the proportions of the this may be connected with mirsky 's protein fractions in different tissues . ( 1947 ) observation on the variation of the proportion of " residual chromosomes " in the cell in relation to its metabolic acti - vity . 
complete amino - acid analyses of histone from calf thymus and from rat only small quantitative differences v - ere found , but there is sarcoma are given . evidence of a difference in the ] proportion of the protein components in different materials . this work is part of the research programme of the birmingham branch of the british empire cancer campaign . 
3. received for publication february 6 , 1947 . it has frequently been noted by the early investigators of tumour pathology that besides a high mitotic rate , tumour cells may also show great variation in the details of mitosis ( pianese , 1896 ; hansemann , 1904 )  . 
the abnormalities may concern the behaviour of the chromosomes or the cytoplasm or both , and most of them lead to degeneration and death of the cells . this is largely due to the deficient nuclei which usually result from abnormal mitosis . 
by repeated chromosome multiplication within the nuclear membrane ( biesele , poyner and painter , 1942 ; koller , 1943c )  . polyploid cells are frequent in tumour regions where .cell breakdown is in progress on a large scale . 
x - rays induce stickiness of chromosomes in plants and animals ( markquand , 1938 ; koller , 1943a ; darlington and la cour , 1945 )  . temperature changes and chemical treatment can lead to similar abnormalities ( barber and callan , 1943 ; ostergren , 1944b ) , and complete suppression of the spindle is brought about by low temperature and by specific compounds , such as colchicine . polyploid , binucleate and multinucleate cells , owing to their chromosome balance , survive and may undergo mitosis . their rate of mitosis , however , is always less than that of cells with a normal chromosome number . 
koller until recently it was believed that a nucleus with the diploid chromosome number was necessary for normal cell behaviour , and that cells with a deficient complement could function only under very specific conditions , the life of such cells always being short ( darlington , 1942 )  . 
the adenocarcinoma here described presents an example in which cells with less than the normal number of chromoit is not out of place to somes are still able to divide and to continue dividing . draw attention to recent literature on cytoplasmic control in micro - organisms ( sonneborn , 1943 ; spiegelman and kamen , 1946 ) , the relevance of which , for the origin of cancer , has been dealt with by many authors ( graffi , 1939 , 1940a , b ; darlington , 1944 ; haddow , 1944 ; potter , 1945 ; woods and du buy , 1945 , 1946 ) , who suggest that the permanent change which renders a cell malignant takes place in the cytoplasm . cell behaviour in this adenocarcinoma is a further indication that the nucleus can be so subordinated , and the cell remain active in spite of its deficient nucleus . u0 ' c unromosome numoer fig . 
1. given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . most people would agree that studies with transplanted tumours have given information concerning the autonomy of malignant tumours and concerning their histogenesis . however , there is a tendency to regard such studie8 as somewhat old - fashioned and this field of study more or less closed . in this paper it is hoped to show that there is still valuable information to be gathered of significance for general biology as well as oncology . general biology and tumour transplantation . the genetical laws governing the transplantation of normal and malignant tissues are now generally accepted . in both cases a complex of dominant genes is concerned which snell ( 1948 ) has called histocompatibility genes . there have always been two schools of thought conceming the nature of these genes , gne that the genes determine iso - antigenic differences , the other that they deterinine " individual differentials " - substances with somewhat mysterious and ill - defined properties . it is not easy to study these questions with normal tissues for technical reasons , one of which is that the number of factors is always high . 
with tumours the number varies , but may be low , and in addition tumours stimulate a better antibody response . iso - immune reactions are most easily studied in the erythrocytes , and it so happens that certain important iso - antigens in strong 's a strain of mice are shared by the erythrocytes and fixed tissues . 
four tumours from this strain have been studied genetically and serologically . the first two were studied in england ; in both it appeared that two histocompatibility genes were concerned , one of which was identical with a gene for an antigen known as antigen ii . 
by serological means it was shown that the occasionally iso - antibodies tumours contained another antigen in addition to 11 . were formed against it , but too irregularly 4nd at too low a titre to be of value for genetical work ( gorer , 1937 , 1938 , 1942 )  . those studied in america were both found to give single gene ratios in backcrosses . 
furthermore , in conjunction with snell and lyman ( gorer , snell and lyman , 1948 ) it was possible to show close linkage between antigen 11 and the locus for " fused " ( a tail anomaly )  . full information is to be published elsewhere , but it can be seen from table 11 that the linkage is close . 
the sera were produced by inoculation of c57 blacks . the similarity is not shown to the same degree by all sera . provisionally called h2 and h2d ( table 111 )  . closely related antigens occur in strains cba and - cm , so perhaps , there is a long series of alleles at this locus . animals carrying the we are not certain how many cross - overs there were . gene for fused may have norm ' al tails , and there are other difficulties associated with tumour transplantation that will be discussed later on . in backerosses involving 257 animals the recombinations were between 0 and 5 per cent . previous to these studies strong ( 1929 ) had used tumour transplantation to show sex linkage of a histocompatibility gene , and bittner ( 1933 ) found loose linkage with " dilution . " the location of h2 was first found by snell and lyman using tumour . 
inoculation without serological testing , and i hope i am betraying no confidences by saying that they have other instances of linkage as well . will be seen that tumour inoculation is - a most useful weapon in mapping chromoit is best to use serological tests as well . 
without going into details it may be said that they were not serologically unifortumour transplantation indicates that this polymorphism may be maintained by a high pure strains unless kept on a very small scale automatically mutation rate . it was shown by bittner ( 1935 ) that a dba crystallize into various sub - strains . tumour would not take in all sub - strains , and this has been found to be a common finding , having been seen with various tumours arising in strains c57 black ( law , gorer , unpublished ) and cm ( gross , 1947 )  . 
we have as yet no ' evidence that liability to disease is influenced bv antigemc constitution , or indeed very little knowledge of the antigens ' perhaps the polymorphism is connected with the risk of functions in the cell . iso - i ' mmunization during pregnancy ; this must be great where foetal absorption is common . 
if a species were completely uniform the risk would vanish , but it is unlikely that any species would be completely so over the whole of its rangle . on the other hand , if it were sufficiently polymorphic , the danger may be minimized . 
if a male has a rare antigen he would probably be heterozygous , and only half the litter would perish if iso - immunization took place . further , in matings with different males , a female would be unlikely to receive successive doses of lastly , it is possible that if a mixture of a large - number of the same antigen . antigens is received , dangerous titres of antibodies are not formed against any antigen ii does not appear to be very mutable , but here mice one of them . also seem very ' polymorphic . eight pure strains have been examined ; all are somewhat different . 
both the tumours tested in bar harbor gave such a ratio , but it was shown conclusively that they both contained at least two antigens . this is easily explained immunologically . antigens differ greatly in potency . 
gorer it is now well known that tumours may " mutate . " strain , we would get about 50 per cent susceptible progeny ( macdowell and richter , 1932 )  . errors of the above t - vpe are counterbalanced by precisely the opposite effect . some tumours may grow and kill the host in spite of iso - antigenic differences . there is considerable indirect evidence of this , but recently it has been possible to show that an animal succumbing to a tumour derived from any other strain may form high titres of antibodies ( gorer , 1947 )  . 
when first tested a tumour may appear to have upwards of 7 factors ; later on , only one or two . differences of this order cannot be accounted for by errors of the type just mentioned . there this might be due to mutations of domimust be some real antigenic alteration . this is extremely improbable ; one would have to nants to recessive alleles . have 6 or 7 homozygous mutations . 
what may happen is that one or more antigens crowd the others if for the sake of argument we assume that antigen 11 occupies 10 per cent out . of the surface of a normal cell , in a malignant one it may occupy 90 per cent . these experiments have the disadvantage that we have no really satisfactory for example , we can show that the cells of a myeloblastic normal control.. leukaemia contain increased amounts of antigen 11 , but we cannot get enough there is evidence that analogous antigenic normal myeloblasts for comparison . alterations may occur in human tumours . 
it is believed that all mammals ( and perhaps many other forms ) are highly polymorphic for histocompatibility genes . there is evidence that some of these genes have a high mutation rate in mice . 
sylvin. fromn the department of radio - pathology , radiumnhemmet , stockholmi , swveden . received for publicationi february 11 , 1947 . our defective knowledge of the biological factors responsible for infiltrative growth is partly due to lack of sufficient information on the biology of the stroma connective tissue in malignant tumours . thus , growing carcinoma vegetations induce different complicated reactions on the part of the surrounding connective tissue , e.g. 
fibroblast proliferation and various inflammatory reactions . in the course of the stroma investigations by the writer , special attention has been paid to the transformation ( " dedifferentiation " ) of the connective tissue preceding the actual infiltration by cancer cells and to the simultaneous appearance of high molecular ester sulphates of unknown composition ( sylvan , 1938 , 1941 , 1945 and unpublished data . ) interpretation of the events taking place in the stroma is rendered almost impossible by the multiplicity of intermingling reactions . 
on this account it was decided to treat each problem separately . consequently , i thought it advisable to study these changes in cartilage , a tissue characterized by very slow reparative and reactive capacities . thus , the actual question was to investigate the morphology and the histochemical changes of normal cartilage when infiltrated by carcinoma cells . 
 - in this way comnparisons could be made with the stroma reactions of the different tissues , and with the alterations in the chondroitin - sulphate of cartilage and the unknown stroma ' ester sulphate mentioned above . 
by selecting suitable cases it was felt that the source of error caused by the connective tissue stroma reaction accompanying cancer vegetations growing from outside the perichondrium , could be avoided . for the sake of brevity , the readers are referred to current literature regarding the normal morphology of cartilage ( maximow and bloom , 1938 )  . 
the resulting newly formed , growing , connective tissue would then " penetrate " into the ground substance of cartilage , which was " dissolved " and replaced by the tissue mentioned above . after this , the cancer cells were believed to grow into this connective tissue , thereby seemingly infiltrating the cartilaginous tissue proper . ribbert emphatically denied that cancer cells ever could infiltrate cartilage directly , the process instead being mediated by connective tissue . 
as to the operating forces ribbert stated that "  . epithelien ( cancerous ) haben nicht die fdhigkeit anders als durch den wachstumsdruck auf ihn ( cartilage ) einzuwirken . " such a restricted mechanical interpretation involving pressure for the explanation of infiltrative growth , is nowadays of little value ( sylv6n , 1945 )  . oestreich ( 1910 ) suggested that the chemical composition of cartilage , mainly the chondroitin - sulphate , would be injurious to the cancer cells and consequently infiltrative growth would become impeded by this substance . since ribbert 's review in 1911 no special articles have been published regarding these questions . 
the statements of ribbert demand a survey of the cooperating factors active in the destruction of cartilage by carcinomatous tumours . the following possible factors have to be considered : 1 . 
the cancer cells might by direct action be destructive . in order to obtain a satisfactory understanding of the morphological factors unfortunately , they should be interpreted in terms of biochemical principles . for lack of complete data the chemical principles can only be touched upon . cartilage has a strongly acid intercellular matrix , due to the presence of large amounts of chondroitin - sulphuric acid . this substance is very sensitive to even slight changes in ph towards the alkaline side ( blix and snellman , 1945 )  . such ph variations cause a rapid depolymerization and disintegration of the long chain molecule . 
a shift in ph resulting in a disappearance of chondroitin - sulphate has recently been suggested to occur in inflammatory lesions of cartilage ( sylven , in press )  . 
when considering the complexity of the problem , i have to admit that no final conclusions regarding the biochemical nature of the operating factors can be drawn from the material presented here . 
some results , however , seem to be conclusive . some information concerning the mutual relationship between cancer cells and the perichondral connective tissue in the absence of any intervening inflammatory stroma reaction was obtained from case 2 , ii . 
the carcinoma strands in question were growing in the perichondrium , which was transformed into a loose metachromatic stroma connective tissue similar to the one met with in most carcinomas ( sylven , 1938 , 1945 and unpublished data . ) in the superficial part of the underlying cartilage a moderate decrease in the content of chondroitin - sulphate was demonstrated , the cartilage in other respects apparently being normal . 
sylvien actual cartilage destruction was seen to be effected either by the sole inflammatory stroma reaction ( case 1 ) or by the combined stroma and cancer strands ( case 2 )  . in the cases under consideration , that part of cartilage just being infiltrated was always devoid of the typical ester sulphate . remains of this substance might be found in the shape of thin pericellular halos . 
1. - the early changes in ear cartilage , previous to the actual infiltration , are demonstrated . at top of picture the perichondral connective tissue is swollen and slightly invaded by lympho - plasmocytes . the superficial part of cartilage appears unstained , indicating that metachromatic material is lacking . 
4. - the disappearance of chondroitin - sulphate precedes the growing tumour . in this picture the stroma reaction has reached the left top corner ; the lightly stained ametachromatic cartilage area contains very few inflammatory cells . 
when investigating the process more carefully , however , it was established that cancer cells really have the capacity of digesting cartilage by their own activities without any co - operating stroma reaction . further , the results indicate , that the first demonstrable alteration of cartilage just being infiltrated is an early disappearance of most of the preexisting ester sulphate . 
the smith type is still , however , a relative rarity and less than a score of cases have been reported since the original description in 1934 . the forowing case , the second to be seen in south africa , closely resembles that originally described by smith ( i934 ) ; but it is unique in that the . 
he had suffered since 1942 from recurrent spontaneously heahng tumours of the left face , ear , neck , chest , shoulder and upper arno other member of his family was known to have suffered from any similar disease ; and he was not related to the other south african who suffers from the smith type of morusca pseudocar ' c ' momatosa . skin generally was normal for his age and was not hypersensitive to sunhght . his occupation as a contractor kept him mainly in the open . 
he had never been exposed to tars , mineral oils or arsenic . he stated that the tumours , of wbich he usually had several active , began like festering blackheads " , grew for 4 - 6 weeks , and then began to regress and disappeaxed , leaving scars , in 4 - - 6 months . 
on his first visit he had two active tumours on the back of the left ear and one over the left scapula and thirty depressed wbite scars on the left side of the nose , upper hp , cheek , ear , neck , chest and upper arthe scalp and buccal mucosa were unaffected . 
a month later the ear lesions were distinctly smaher and flatter and that over the scapula had flattened dow - n to a coin - like plaque with rolled edges and a central area of soft keratinous material . all the lesions were chnically indistinguishable from squamous epitheliomata . 
at this visit a fresh lesion , i mm . , was discovered iin the angle of the left ear lobe and cheek it closely resembled , as the patient had described , a festering blackhead . the patient , who b . - ilieved himself to be suffering from skin cancers , has on several occasions been subjected to biopsy or excision of tumours ; and a diagnosis of squamous epithlioma had generally been made . x - ray therapy had also been given niore than once with little impression on the rate of healing of the tumours ; but the scars left in such areas were more mutilating than those seen after spontaneous healing . a portion of one of the lesions on the ear was excised for histological examination and we examined several sections of lesions excised in the past by d . 
the stretched and atrophic epidermis covering the lesion is between the central mass of keratin and the covering epithelium are seen on the left . irregular and well - differentiated masses of epithelium and cell nests . 
1. received for publication may 10 , 1951 . there is still some disagreement on the question whether the early changes produced in epidermis by chemical carcinogens are specific , i.e. , whether they can be distinguished from the effects of non - carcinogenic irritants . the chemical evidence is inconclusive . 
cowdry and his school have been able to show that the chemical constituents of mouse epidermis made hyperplastic by several applications of 20 methylcholanthrene differ quantitatively from those of normal epidermis ( carruthers , 1950 ) , but it does not appear to have been proved that these changes are produced only by carcinogenic substances . histological evidence is more definite . 
the only significant way in which such skin has hitherto been found to differ from untreated skin is in its ability to produce tumours when treated with a co - carcinogen such as croton oil . 
the " latent tumour cells , " if present , must be so few that they are very unlikely to be detected in sections , or perhaps they may not be recognizable if seen . 
the skin has passed through a state known to be produced only by carcinogenic agents ; this state has apparently passed away , yet the skin will then react to treatment with a non - carcinogenic substance in a manner quite different from normal skin . the early reaction of normal mouse skin to croton oil is similar in general type to its reaction to other non - carcinogenic irritants , and differs in important respects from the reaction to carcinogenic substances . 
the chief criteria on which this distinction is based have been fully described by pullinger ( 1940 ) and by gluiicksmann ( 1945 ) , and only a summary will be given here . 
gwynn the epidermis is stratified . in the normal skin of the body of the mouse there are no strata , and the various types of cell are arranged apparently at random in a layer one cell , or in places two cells , thick . of the nucleated cells in the epidermis of the back of a normal adult mouse , about 14 per cent are resting , 80 per cent differentiating , and the rest are mitotic or degenerating . this classification was used because it gives definite information about the state of the epidermis which is not obtainable by any other method known to this information is not dependent on any hypothesis about the function or potentialities of the different classes of cells . 
for the purpose of this work they are simply types of cells which can be distinguished , the absolute and relative numbers of which vary in different states of the skin . one of the most striking features of the hyperplasia produced by chemical carcinogens in mouse epidermis is the rise in absolute and relative numbers of the resting cells . non - carcinogenic irritants , on the other hand , produce a hyperplasia in which the absolute number of all epidermal cells is increased but their relative numbers remain approximately the same as in normal skin ( gliicksmann , 1945 )  . 
the percentage of resting cells in the epidermis was chosen as a criterion for comparison of the hyperplasia produced by the different treatments used in the following experiments . it provides a measure , which can be handled statistically , of the specificity of the reaction of the epidermis , i.e. , of its resemblance to the characteristic reaction to carcinogenic substances . in the work now reported the effect of croton oil on normal mouse skin has been compared histologically with its effect on skin after the reaction to previous treatment with a chemical carcinogen has apparently disappeared . three strains of mice and two different carcinogens were used . 
 " t " and " s " mice were purchased from dealers . " p " mice were of an institute - bred strain originally obtained from the national institute for medical research ; they had been used before for studies on skin carcinogenesis by gluiicksmann ( 1945 ) and salaman ( 1943 )  . 
the standard errors of means were of the same order in this experiment as in the other two . the mice were examined weekly for the appearance of tumours , for periods of 200 to 250 days . 
gwynn high level and remained well above normal . in group 2 there was a parallel but smaller increase . in group 3 application of croton oil without previous treatment was followed by an initial slight rise in resting cell percentage , which then these results are listed in table i and charted in fig . 
the first tumour appeared on the further trials have 63rd day in group 1 , but not till the 170th day in group 2 . confirmed the superiority of acetone over paraffin as a solvent for the carcinogen comparisons of various concentrations of croton used as the primary treatment . oil in acetone and paraffin have shown that a 0.5 per cent solution in the former is almost as powerful a co - carcinogen as a 2.5 per cent solution in the latter . 
13. - experiment 2 : 0 group 2 : 10 mice at beginning of experiment , 8 survivors at 217th day . e group 4 : 12 mice at beginning of experiment , 11 survivors at 217th day . weekly croton oil applications without previous treatment ( group 3 ) caused only a transient rise to 21 per cent on the 3rd day , and thereafter the level declined gradually to 16 per cent on the 115th day . 
13. since no tumour it will be seen that tumour appeared in the other groups , they are omitted . production in group 4 began earlier than in group 2 , but later proceeded more this suggests a possible parallelism between the early rise of resting rapidly . cell percentage and the tumour production which follows about 50 days later . ( 3 ) in a third experiment , four groups , each of 8 male and 8 female mice of group 1 , in this experiment , the " s " strain , were treated as shown in table iii . has the same function as in the last : a test of the carcinogenicity of the primary treatment with the carcinogen . 
14. as in the last two experiments , the difference between the effects of croton oil treatment with and without a previous carcinogenic stimulus is clear ( groups 2 and 3 )  . in group 4 , resting cell percentages were at first lower than , but later rose above , those of group 2 . 
15 shows the rate of tumour production in these groups . dimethyl - 1 : 2 - benzanthracene in paraffin oil appears to have been less effective than 1 per cent benzpyrene in acetone ( group 4 of experiment 2 , but note that different strains of mice were used )  . tumours appeared earlier in group 2 than in group 4 ; thus , as in the former experiment , there appears to be a parallelism between resting cell percentage and subsequent tumour production . 
gwynn except one in which early malignant change was probably present . during a considerable experience of the application to mouse skin of croton oil alone , a very few small tumours have been seen , but never as many as in this experiment . precautions against contamination of cages , etc . , with carcinogenic substances are taken , but the possibility that such a technical mistake occurred cannot , of course , be entirely excluded . it is perhaps significant that the resting cell percentage in this group , after falling to 16.6 per cent on the 132nd day , rose again to 20 per cent on the 216th day . tumours produced by the application of substances generally regarded as non - carcinogenic have been occasionally reported . 
9 and 10 are high - power views of regions of the epidermis consisting predominantly of resting cells and differentiating cells , respectively , taken from the same specimen as fig . 
many substances are as powerful hyperplastic agents as croton oil , without being co - carcinogenic . croton oil is much the most powerful co - carcinogen for the mouse 's skin yet discovered . its action appears to be highly specific with respect to animal species , and perhaps also with respect to the carcinogen with which it acts . it may be that it combines very weak carcinogenic with powerful co - carcinogenic power . 
a number of tumours subsequently appear . this number varies widely according to strain of mouse and strength of initial carcinogenic stimulus ; there may be an average of only 2 or 3 , or as many as 20 , per mouse . 
but even if the higher figure is taken , and it is assumed that each tumour was represented before croton oil treatment began by a single " latent tumour cell , " or a small group of such cells , these cannot be responsible for the generalized rise in restingcell percentage which is observed throughout the epidermis . in fact the chance of finding such a cell or group in a section is small . 
it appears that mouse epidermis which has been treated with a carcinogen , though it returns to a state closely resembling the normal , has suffered a general change which does not consist merely in the presence of a few latent tumour cells . we are indebted to professor s . 
woodyatt. * from the meyerstein institute of radiotherapy and the bland sutton institute of pathology , middlesex hospital , london , w.1. received for publication february 15 , 1950 . failure in the treatment of malignant disease is most often due to the occurthere rence of metastasis before treatment of the primary lesion is instituted . are , however , a number of cases in which the tumour remains localized for a considerable time , but cannot be removed surgically on account of its size and anatomical situation , and cannot be destroyed by radiotherapy without irreit is the aim of the radioparable damage to neighbouring normal tissues . therapist to exploit the differences in sensitivity between normal and neoplastic tissues , and it is the object of this research to see whether the effects of radiotherapy on certain tumours can be enhanced by modification of the techniques of therapy in common use at present . a course of x - ray treatment involves a number of variable factors . 
the segments , usually 2 or 4 in number , and as nearly as possible of equal size , were then treated by one or more experimental techniques , while one segment was treated by a control technique . segments not being treated were protected by lead shields while neighbouring segments were irradiated , and care was taken to avoid overlap of adjacent segments or an untreated gap * b.m.a. 
woodyatt between them by careful skin markings and " setting up . " the question of side - scattering of x - rays from one segment into adjacent ones was investigated by physical measurements with micro - ionization chambers in a wax " phantom . " the amount of scattered radiation was found to be less than 5 per cent at 1 cm . from the edge of a treated segment , and this was considered small enough to be ignored . in this way erroneous conclusions resulting from unpredictable individual variations in response are largely eliminated , and each case constitutes a complete separate experiment . 
the results of individual experiments can later be compared to see whether the experimental technique in question regularly produces a particular effect . the tumours and surrounding skin were examined at frequent intervals to follow progress , and to detect and note differences in response between the areas . in addition , biopsies were taken from all areas before , during and after treatment . at first , weekly biopsies were taken , but it soon became obvious that in the earlier stages more frequent examinations were necessary , while after completion of the course of treatment intervals of a month or more might elapse . 
the sections were examined by a pathologist who not only had no preconceived views about the various techniques of irradiation employed , but was kept in ignorance of the area from which each specimen had been taken . biopsies from each area before treatment were studied carefully to provide a base line , and also to give an idea of the degree of variation between different this variability was often found to be marked , and areas of the same tumour . differences in biopsies subsequently taken from the several segments had often to be discounted as representing no more than possible chance variations . 
fractionation is , however , usually by equal daily doses given on 5 or 6 days each week , and this fractionation technique is applied with little discrimination to widely different sorts of tumour . certain theoretical considerations , mentioned below , suggested that a different method of fractionation , leaving longer intervals between the fractions , might be more effective . 
an important direct effect of a dose of irradiation is temporary suppression of mitotic activity . koller ( 1948 ) found that in squamousand basal - cell carcinomas of the skin the number of dividing cells was considerably reduced 6 hours after 200r , and that after doses of 400r and 500r mitotic suppression might last for several days . 
the susceptibility of cells to irradiation damage varies at different periods of their life cycle , being greatest in early prophase ( lea , 1947 ) , and irradiation given spear and during the period of mitotic suppression is relatively ineffective . glucksmann ( 1938 , 1939 ) have demonstrated by experiments on irradiation of tissue cultures and animal tissues in vivo that a greatly enhanced lethal effect is obtained if fractions are spaced so as to coincide with the recovery of mitotic activity following the suppressive effect of the previous dose . information concerning the duration of mitotic suppression in human tumours it probably varies in different tumours , but will after different doses is scanty . depend largely on the size of the dose . 
a clinical investigation indicating advantages from a wider spacing of fractions has been reported by koller and smithers ( 1946 )  . koller ( 1948 ) considers that the nature of the tumour bed and the indirect effects of irradiation on the stromal reaction in the surrounding normal tissue exercises an important influence on the response of the tumour itself . 
a further limitation was , of course , imposed by consideration for the patient 's welfare , and no case was undertaken where it was felt that there would be less chance of effecting a cure by the method . tumours of three types were treated - large rodent ulcers ( 2 cases ) , carcinomas of the skin ( 5 cases ) , and carcinomas of the breast involving the skin ( 4 cases )  . most tumours of the first two types are radio - sensitive , and a successful result could normally be expected from the use of an orthodox technique . these tumours were treated in order to assess the relative efficiency of the experimental techniques , and to determine any differences in the reaction of normal tissue at the edge of the tumour . the cases of carcinoma of the breast were of special interest , for , as is well known , a considerable proportion are markedly radio - resistant . 
the usual erythematous reaction developed , and proceeded to moist desquamation over the tumour and surrounding skthe area of skin at the periphery which was only covered by the original 71 x 15 cfields showed pigmentation , but no desquamation . 
the dose to this skin area had only been about 2000r when the smaller fields were substituted . no difference in reaction or tumour response in the two areas was apparent at this stage . on october 6 , as viable tumour was still feared to be present , further treatment was given as described . three weeks after the conclusion of treatment a marked difference was apparent between the two areas . 
the area treated by the control technique ( area 1 ) was completely healed over by healthy new epithelium except for a small ulcer at the site of the first surgical attack . 
the remaining tumour consisted of some firm pink papillary processes , almost flush with the surface . in area 2 much of the tumour and surrounding skin covered by the treatment applicator was still raw and denuded of epitheliuthe remaining tumour was a little flatter than in the control area . eight weeks after treatment further flattening was apparent . area 1 was healed except for the remains of the ulcer . area 2 showed very little progress of healing , although a few islands of epithelium had appeared in the raw skin area ; there was some discharge from a fissure between two sessile processes . four months after treatment a striking difference between the two areas was apparent . 
the control area was healed and showed marked pigmentation , all that remained of the tumour being some fibrotic nodularity beneath the surface . area 2 showed up as a sharply outlined , completely unpigmented square , corresponding to the treatment applicator . there was still an indurated fissure at the site of the tumour , and an area of skin below the tumour remained unhealed and had clearly undergone necrosis . five and a half months after treatment the patient complained of burning pain in the lower part ( area 2 ) , and an increase in discharge from the fissure which was still present . 
a month later ( april , 1948 ) radionecrosis was obviously developing in area 2 ; the fissure had deepened , its edges were grey and necrotic , and the surrounding tissues were pale and avascular , and as hard as cartilage . by may a large necrotic ulcer corresponding to area 2 had developed . local treatment failed to bring about healing , so in november , 1948 , the whole treated area was excised , after a preliminary colostomy . this was done partly because residual foci of active growth were suspected . 
woodyatt there was a moderate degree of associated inflammatory mitotic activity . biopsies taken from both areas during and after treatment showed reaction . progressive differentiation of the tumour cells with reduction in the percentage of viable cells and their final disappearance . 
no sign of tumour could be seen in the biopsies taken at 6months , and no significant differences between the series of sections from areas 1 and 2 were detected . 
a small nodule of recurrent growth ( 1.25 cdiameter ) had appeared , adjacent to the mastectomy scar , in february , 1945 . superficial x - ray treatment was given ( 4 daily doses of 800r ) and the nodule regressed , being quite healed by september , 1945 . 
3. - carcinoma of breast ( case 3 ) divided into four areas . 11111 11111 11111 total 3000r . in 27days area area area area total 4000 r in 26 days total 3000r in 27 days total 3680r in 24 days 11111 11111 11111 days i = biopsies taken from all areas , and on day 50 fig . 
the control technique was modified in this case , 150r being given daily instead of the usual 200r . this was done to bring it more into line with the average daily tumour dose administered in this clinic for carcinoma of the breast . 
by the end of treatment , february 18th , the greater part of the surface was covered by smooth granulation tissue . there was still a considerable amount of tumour present , with a subcutaneous shelf of induration palpable all round the edge . there was severe erythema of the surrounding skin , with much pain and discharge , and for these reasons treatment was curtailed . it is probable that the unusual severity of the reaction was due to infection of the raw surface , as the patient had fever up to 1010 f . 
the tumour had shrunk to 10 - 5 x 6 - 5 cm . the ulcer floor was covered by necrotic slough and its edges were still firm , but were softer and less raised in areas 1 and 3 . seven weeks after treatment the skin had begun to heal in area 3 . 
the skin in area 1 showed well - marked pigmentation , but was perfectly healed . well - marked differences were now apparent in the different areas of the tumour , which had shrunk further to 9 x 6 cboth areas treated by the control technique showed clinical evidence of active residual tumour , the ulcer in these areas having a hard raised edge with much adjacent subcutaneous induration . area 1 showed some suspicious induration , but less than in the areas treated by the control technique . area 3 was soft and nearly flat , with no definite sign of residual growth . 
6 at the end of treatment . the tumour cell mass in the upper part of the field shows extensive hyalinization , and there is heavy lymphocytic infiltration of the stroma . note that the magnification is the same as in fig . 
8 , 9 and 10 . - squamous - cell carcinoma of the ear ( case 8 )  . biopsies taken before , at about the middle of , and at the end of the course of treatment . 
the upper half was treated by technique i ( 500r twice weekly ) to a total of 3500r in 24 days , and the lower half by the control technique ( 200r daily ) to a total of 3600r in 24 days ; 95 k.v. 
x - rays clinically there was rapid regression of the lesion in both areas , were used . and the tumour had disintegrated completely before the course was finished . the serial biopsies showed a very satisfactory response in both areas , no viable cells remaining within two weeks of starting treatment . 
any conclusions we may draw from this small series of cases must be purely tentative ; the final evaluation of these techniques may require the elapse of a considerable interval of time , and in view of the possibility of variation in different parts of the same growth many cases must be studied before definite conclusions can be reached . complete equality of total dose and protraction were seldom obtained , and this introduces another variation from strict experimental conditions . 
with these facts in mind the following conclusions are cautiously presented . technique i ( 500r twice a week ) was used in 9 cases ; 3 squamous - cell carcinomas , 4 carcinomas of the breast , and 2 rodent ulcers . 
the clinical result in the 3 cases of epithelioma was uniformly good , and in one case this technique gave slightly quicker results than the control . in 2 cases of carcinoma of the breast this technique gave a better response , judged clinically and histologically , than the control ; in the other 2 cases the results were equally good . 
the cases of basal cell carcinoma responded better both clinically and histologically to the control technique ( daily fractions of 200r )  . technique ii ( looor once a week ) was tried in 4 cases ; 2 squamous - cell carcinomas of the skin , one carcinoma of the breast , and one rodent ulcer . 
w.7. received for publication march 14 , 1949 . previous observations ( foulds , 1947 , 1949b ) showed that the growth of some transplanted mammary tumours in hybrid mice depended on a hormonal stimulus which operated in normal female mice but not in normal males ; artificially - administered oestrogen supplied the necessary stimulus for growth in males . 
some of the tumours were independent of the hormonal stimulus at the first transplantation ; others lost their dependence after several transfers . dependence on hormones seemed to characterize one stage in the life - history of mammary tumours in hybrid mice . 
the majority of the mice were br hybrids , mostly of the f3 and f4 generations , and made up of 71 mice of strain br4 ( pink label ) , 90 of strain br4 ( blue label ) , and 69 of strain br6 . 
a preceding paper ( foulds , 1949a ) describes the source of these hybrids and the incidence of tumours in them . the mice were subjected to forced breeding and most of them had pregnancies in rapid succession throughout the period of observation , even when bearing multiple large tumours . 
tumours were recognized usually when about 0 5 cin diameter , and weekly thereafter two main diameters were measured with calipers . growth charts were made by plotting the sum of the two diameters against post - mortem measurements usually agreed time . satisfactorily with those made during life ; measurements on regressing tumours were the most difficult and subject to the largest errors . frequent , often daily , measurements were made on selected mice . litters were recorded each morning except on sundays and public holidays . the time of parturition as shown on the charts was usually later than the actual time by unknown periods of up to 24 hours on weekdays and 48 hours at weekends . 
the mice were examined post - mortem except for a few that were eaten ; the tumours were measured and pieces of them fixed for histological examination . in the charts the first tumour , or largest of contemporaneous tumours , is represented by a continuous line joining crosses which indicate the actual measurements ; the second tumour is represented by a broken line and circles , and the third by a dotted line and triangles . 
178. 8 9 10 weeks ( i ) left axilla ; ( ii ) right axilla . in most of the mice from 1 to 6 new tumours appeared during the course of the first . 
1 shows three different types of behaviour at the same time in one mouse . at least three major factors contributed to the wide diversity of behaviour amongst spontaneous tumours , and even amongst multiple tumours in the same mouse : first , the regulation of tumour growth by the environmental , and presumably hormonal , changes occurring during pregnancy and the puerperium ; second , the specific reactivities of particular tumours to the environmental 348 l . 
foulds changes ; and third the qualitative changes occurring in tumours during their manifest clinical course as evidenced in particular by altered responsiveness to in the remainder of this paper the terms " responsive " and reproduction . " unresponsive " are used in a special and restricted sense to describe tumours which , respectively , do and do not vary their growth in response to the physiological changes occurring in their ho * ts during pregnancy and the puerperium . the term " progression " is used , also in a special sense , to denote qualitative change in tumours as distinguished from mere advancement in size , and as evidenced in particular , but not exclusively , by altered responsiveness to pregnancy and parturition . subsequent paragraphs detail the analysis of the phenomena here outlined . for convenience of description the tumours are classified according to a few main types of behaviour , but transitional and indeterminate types are encountered and preclude a precise statement of the relative frequency of types . 
the peak size , however , was often considerable , as shown in some of the other charts representing type i tumours ( fig . some tumours maintained their 20 )  . course unchanged through several months of observation , whereas others after two or three cycles changed their behaviour , as described in a later section . the growth of responsive type i tumours was strictly conditional and dependent on pregnancy . if breeding stopped the tumours disappeared and , as a rule , did not recur until breeding was resumed . 
51. ( i ) right vulva ( ? recurrence of tumour excised 7 weeks previously ; earlier tumour not shown ) ; ( ii ) right axilla . with a small range of growth and regression at each pregnancy , and a slow but steady increase in average size . another tumour shown in the same diagram ( dotted line ) appeared 8 weeks after the first and then followed an almost parallel course . 
the peaks of growth , or the averages of the maximum and minimum sizes during successive pregnancies , fell close to a straight line . thus , the course of a tumour was represented by a curve which could be resolved into a straight line with superimposed waves ; the straight line indicated the rate of net growth or , for want of a better term , the intrinsic growth rate , and the waves indicated the response to pregnancy and parturition . 
the intrinsic growth rate and the degree of response , however , varied within wide limits and independently similar intrinsic growth rates were of each other from one mouse to another . responsive and linked with different degrees of responsiveness and vice versa . unresponsive tumours in the same mouse sometimes , as an exception to the general rule , had similar intrinsic growth rates as illustrated in fig . 
their differentiation from type i tumours was questionable , but they seemed to correspond with relatively frequent tumours in , nonbreeding mice whose course was represented by a horizontal straight line , and possibly differed essentially from type i tumours in the ability to persist without the stimulus of pregnancy . 
the great diversity of behaviour was attributable to two circumstances : first , the intrinsic growth rates and the responsiveness varied within wide limits and independently of each other as shown in the present section and , second , progression from one type to another occurred variously during the clinically manifest course of the tumour . 
the tumour itself had changed . the recognition of a similar change in responsive tumours was necessarily more difficult because the pregnancy waves obscured the intrinsic growth rate . probably an acceleration of growth often accompanied the loss of responsiveness 4m.3~ 0k 11 i / i i..#4 i 11 9 10 11 12 - 13 14 15 i\it - l 18 19 20 21 22 16 17 weeks fig . 
19 , however , the one that regressed completely between pregnancies ( broken line ) increased its peak size somewhat more steeply than the tumour that regressed incompletely ( continuous line )  . increasing peak size , therefore , was not attributable , in general , to summation . the regression of some tumours was slight and of short duration , being followed almost at once by progressive unresponsive growth . 
the regression was sometimes trivial and probably within the limits of error in measurements , and the tumours were then scarcely distinguishable from those already described which continued as unresponsive tumours from the peak of a pregnancy wave . possibly the two tumours illustrated in fig . 
29 proved unresponsive at a subsequent pregnancy . another tumour ( broken line ) shown in the same figure behaved similarly , except that it apparently began to grow earlier and was less certainly unresponsive at the subsequent pregnancy . some tumours regressed slightly or moderately after parturition and then maintained a constant size . 
the terminal course was represented by a straight line , but the intermediate course through the first and second pregnancies after the resumption of breeding was more fairly indicated by a curved line , suggesting a gradual accession of growth energy in an unresponsive ( or minimally responsive ) tumour . 5 0o d - t . 
more commonly the first tumour was solitary and further tumours developed consecutively . so far as could be seen the spacing of successive tumours and the sequence of types were irregular . 
tumours that remained solitary throughout the period of observation were sometimes unresponsive , but more frequently responsive . in the majority of the mice where two tumours appeared at about the same time both tumours were responsive ; in the minority both were unresponsive , or one was responsive and the other unresponsive . 
as a rule new tumours were registered first during pregnancy . different types of tumours developed independently of each other in the same mouse , and progression from one type to another occurred independently in the several tumours . 
13 , regressed completely within 7 days , but when another pregnancy followed without delay regression was only partial . possibly hormonal changes during the first 2 or 3 days of pregnancy sufficed to check regression , although growth was not apparent until a few days later . perhaps a few of the " recurrent " tumours were , in reality , new primary growths , but so nearly as could be determined the recurrent tumours occupied the same positions as those which had disappeared and were of similar shape . after partial regression the reality of true recurrent growth was not in doubt . some tumours were reduced to thin plaques not greatly different in superficial dimensions from the tumours at their peaks of growth ; recurrence was manifested by a thickening of the whole plaque . other tumours shrank to vague subcutaneous thickenings of doubtful , but probably considerable , extent ; recurrent growth was evidenced by sharpening of the outlines . it seemed that tumours recurred by the simultaneous grow ' th of all parts of a substantial area of previously altered mammary tissue rather than by centrifugal growth from a in consequence , recurrent tumours were often relatively small residual focus . large when first registered and the gradients of growth and regression remarkably steep . a few tumour - bearing mice nursed and weaned their litters . their tumours behaved during lactation like those in recently pregnant mice that did not at once become pregnant again although deprived of their young . 
some dubious tumours , registered once or twice on suspicion , were not seen again , but only 5 tumours , recorded on at least one occasion without query , disappeared permanently from mice that continued to breed . after interruption of breeding the tumours that had regressed recurred , with few fig . 
the recurrences corresponded as a rule with expected pregnancies in continuously breeding mice , and the recurrent tumours , unlike those in segregated females , were responsive ; almost certainly the recurrences were stimulated by unrecorded pregnancies . 
76. male removed at a ; injections three experiments were carried out with oestrogens . in the first , each of 8 mice received 4 daily applications to the skin of 0 - 2 c.c. 
36 shows regression checked and succeeded by growth at the time of the injections , but as similar events occurred without injections during intermissions of breeding the interpretation was doubtful . in other mice an action on tumours was trivial or lacking . in the third experiment cholesterol pellets containing 10 per cent of diethylstilboestrol and weighing on the average 8 - 2 mg . 
were implanted subcutaneously in 7 mice . nine tumours previously observed in these mice had disappeared before the pellets were implanted and none recurred promptly , but eventually each mouse developed a solitary tumour . in 3 mice the late tumours recorded 366 l . 
foulds 54 days , 145 days and 145 days respectively after implantation of the pellets were in the same region as earlier tumours which had regressed , and were possibly , but , in view of the long delays , not probably , recurrent tumours . in the other 4 mice the late tumours were remote from the sites of the earlier tumours and were undoubtedly new primary growths . 
the present section records the transplantation of tumours whose previous course was known and describes experiments with tumours removed surgically with three main objectives , namely to study autotransplantation , to compare successive primary tumours in the same host , and to compare primary tumours with the recurrent tumours which followed the operation . the experiments were few in number , the general plan of this investigation being to study the natural course of tumours with a minimum of experimental interference . tumours of similar size from the same mouse were used to compare the transplantabilities of responsive and unresponsive tumours . 
tumour in the first passage tumour b grew a grew in female hosts but not in males . equally in male and female hosts , although in the second passage the implants grew tardily in males . 
from these experiments it appeared that , in general , unresponsive tumours were transplantable into male and female hosts and responsive tumours only into female hosts , but that the correlation between type of growth in the primary tumour and behaviour after transplantation was not perfect . five tumours were excised and used for autotransplantation , implants being inoculated subcutaneously near the mid - line of the abdomen in order to minimize confusion with new primary tumours . three of the transplantations were unsuccessful . 
foulds each , so far as could be judged from the short period of observation , was " responsive . " two autotransplantations were successful . growth of the implant from a primary tumour measuring about 0 - 2 cin diameter and removed 6 days after detection was evident after 26 days , and continued steadily until the mouse was killed 22 days later . 
haddow , using in the main dealers ' mice of unknown ancestry , recorded frequent measurements during and after pregnancy , and concluded that " no evidence was found to suggest that gestation itself has any influence on the rate of growth of mammary cancer in the mouse , but in approximately half of the available cases it was observed that parturition was followed by a temporary decline in tumour growth rate . " haddow 's two figures illustrate , respectively , a substantial though incomplete regression after parturition and a halting of growth without regression ; they match some curves of mine . 
gardner ( 1941 ) described 5 hybrid ( 057 black x cba ) f1 mice which , repeatedly , had tumours attaining 1 - 2 cin 2 to 5 pregnancies ; the tumours regressed after parturition , but 3 of the mice eventually died with mammary adenocarcinomas . the responses of the tumours in the hybrid mice used in the present investigation are , possibly , exceptional in frequency and degree , but are not essentially different from those described by haddow and by gardner . notable response to pregnancy and parturition is here recorded in hybrids of varied genetic constitution derived from the inbred strains c57 black , riii and a ; it is not correlated with anomalous transmission of the milk - borne mammary tumour agent . the pregnancy effect usually becomes apparent during the second half of gestation , but probably begins during the first week and continues until the ' day before parturition . 
the abrupt regressions about the time of parturition suggest the sudden withdrawal of a stimulus which , though not yet identified , is presumably hormonal , affecting widely - distributed multiple tumours . 
the preliminary experiments with hormones are indecisive ; a simple oestrogenic action seems unlikely , and the possible effect of gonadotropic hormones , placental hormones , and the co - operative action of oestrogenic and luteal hormones require further investigation . lactation has no specific effect , and modifies the course of the tumours only in so far as it delays the next pregnancy . the pregnancy effect on mammary tumours is comparable with the " promoting " action of various procedures on chemically - induced tumours of the skin of rabbits and mice . 
rous and his colleagues ( rous and kidd , 1941 ; mackenzie and rous , 1941 ; friedewald and rous , 1944a , b ) studied promoting factors in rabbits , and berenblum , who has recently adopted rous 's nomenclature , in mice ( berenblum , 1944 ; berenblum and shubik , 1947 )  . 
foulds his colleagues describe the " promoting " action of trauma and irritants in eliciting and maintaining tumour - growth from latent tumour cells present in the skin as a result of the " initiating " action of a carcinogen . 
some " conditional " tumours grow only whilst the promoting factor operates ; they disappear when it is withdrawn , but recur from the irreversibly altered epithelum when the promoting factor is restored . 
rous and kidd discuss whether or not their argument the conditional growths of rabbits ' skin are " true tumours . " in essential applies equally to the conditional mammary tumours of mice . agreement with rous and kidd , i consider that their exclusion from the group of tumours by an arbitrary definition is unwarranted , and i describe as " tumours " all the mammary growths except a few palpable nodules which regress and do not recur , and those nodules , probably similar , that do not survive autotransplantation . they are accountable to a reversible change in mammary tissue , and perhaps to the exceptional persistence in gross nodules of the properties of the hyperplastic nodules or " adenomas " which are widely accepted as precursors of mammary tumours in mice although many of them are abortive ( gardner , 1941 )  . browning ( 1948 ) reported that nodules less than 02 cin diameter in c3h mice were not transplantable , and that about a third of them regressed , whereas nodules larger than 02 cin diameter never regressed . my observations differ from browning 's in revealing no correlation between behaviour and size ; autotransplantation of tumours more than 05 cin diameter was unsuccessful . the remaining mammary tumours develop from an irreversibly altered mammary tissue . 
the great diversity of behaviour is attributable to the interplay of factors which vary within wide limits and independently of each other . classification into types , though convenient for description , is arbitrary , and hampered by gradations from one type to another . 
the primary distinction , although not absolute , is between the " responsive " tumours whose course is notably influenced by pregnancy and parturition and the " unresponsive " tumours whose growth is unaffected by reproduction . the tumours assigned to responsive type i correspond with the " conditional " neoplasms of rabbits ' skthey grow during pregnancy , regress promptly after parturition , and recur , with rare exceptions , in the same place at each successive .pregnancy ; after several cycles of growth and regression they achieve no net increase in size or aggressiveness . 
the responsive type ii tumours are less strictly " conditional " ; they wax and wane at each gestation , but with a net increase of size at each cycle . 
the rate of net increase is steady and characteristic of the individual tumour , depending on a specific property described as the " intrinsic growth rate . " the term is provisional , to be discarded when elucidation of the property suggests a better name , and is used to denote the steady growth , represented by a straight line , upon which the waves of response to pregnancy are superimposed . 
the intrinsic growth rate , measured by the slope of the straight line and the responsiveness as indicated by the amplitude of the pregnancy waves , are constant , often for long periods , in a particular tumour , but vary within wide limits and independently of each other from one tumour to another . 
foulds of tumours , namely the capacity for progression , as above defined , and that general principles or rules of progression , deduced from the study of mammary tumours of mice , are widely applicable . the material for this analysis of progression consists of spontaneous tumours following their natural courses without experimental interference beyond temit is especially favourable on account of the porary interruption of breeding . abundance of multiple tumours , for the comparison of multiple tumours establishes beyond doubt that progression is a change in the individual tumour ; alteration in only one of several contemporaneous growths is not attributable to change in a hypothetical " general resistance . " the varied tumours encountered in this investigation may be arranged in a series having at one extreme the wholly conditional responsive tumours , at the other extreme the rapid - growing unresponsive tumours , and intermediately all indidegrees and combinations of responsiveness and intrinsic growth rate . vidual tumours , however , do not in general traverse this series ; they advance by abrupt steps , vaulting many possible transitional stages . 
at its first clinical manifestation a tumour may occupy any position in the series of types , irrespective of the time of its occurence or its position in a sequence of multiple tumours . 
tumours which develop simultaneously or consecutively in the same mouse conform sometimes to the same type and sometimes to as many types progression occurs independently and unpredictably as there are tumours . in multiple tumours in the same animal irrespective of their size or clinical progression may occur earliest in the first , second , or any subsequent duration . member of a sequence of multiple tumours . 
when two or three tumours , similar in size , duration , and type of behaviour are present , progression occurs in only one of them at a time . moreover , the progression of one tumour has no apparent effect on the course of the others . 
the present observations decisively controvert browning 's ( 1948 ) suggestion that a second tumour may " abrogate the autonomy " of the first . the several recognizable characters of individual tumours undergo progression often , no doubt , responsiveness and intrinsic growth rate independently . change simultaneously , but in some tumours progression in responsiveness occurs transplantation without progression in intrinsic growth rate and vice versa . experiments provide further evidence of independent progression of characters , namely the responsiveness of transplanted tumours to pregnancy and the gross milky secretion in response to oestrogenic stimulation ( foulds , 1949b )  . the development of a tumour does not always reach its end - point within the life - time of the host ; progression advances further during serial transplantation ( foulds , 1949b )  . 
the course of the growth elicited by pregnancy depends on specific properties which change , by progression , in latent tumour cells and in stationary tumours . the manifestation of progression in the mammary tumours is usually abrupt , as it is in the induced skin tumours of rabbits and mice , but progression itself is not necessarily abrupt ; it is possible that cumulative gradual changes reach a threshold level at which they are first manifest . 
some tumours evidence a gradual progression through a graded sequence of types . gradual , continuous progression seems uncommon , but it is less conspicuous than the abrupt type , and more accurate and more frequent measurements might reveal it more frealthough the observations are few and indecisive , it seems that slow quently . gradual progression is apt to result in sluggish , irregular , or dubiously unresponsive growth . 
the unequivocal rapid - growing unresponsive tumours , as a rule , are either primarily unresponsive or the result of abrupt progression from a fully responsive and , often , strictly conditional tumour . apparently two paths of progression are available . 
one path leads directly to unresponsive tumour ; the tumour acquires its definitive properties early without traversing the numerous intermediate stages which are possible , and which are observed on the other path or " responsive detour . " the detour leads ultimately to an unresponsive tumour , but progression along it may be slow and gradual and the end - point indeterminate , or reached only after transplantation . 
abrupt progression switches many tumours from the detour to the direct path ; jumping the intermediate stages , the tumours change from the fully responsive to the definitive unresponsive type . 
a few applications arehere briefly indicated . the behaviour of tumours is the resultant of multiple characters which vary , within wide limits , independently of each other and undergo independent progression . 
the - characters include growth energy , invasiveness , capacity for dissemination , and responsiveness to environmental stimuli , of which the hormones are the most easily recognized , but not necessarily the only , examples . " malignancy " is not a single character . 
independent progression of characters ( rule ii ) , however , results in disproportionate or " out - of - step " development , as for example in the " benign " tumours that metastasize and the " locally malignant " tumours that do not . 
the out - of - step development is especially important in carcinoma of the prostate , which , despite conspicuous growth , invasion and dissemination , willis ( 1948 ) criticizes the sharp division of tumours is responsive to hormones . into innocent and malignant groups , and deprecates the question , " is this tumour innocent or malignant ? " ; the appropriate question in his opinion is , " how it is even more important , i suggest , innocent or malignant is this tumour ? to ask , " in which characters , and to what degree in each of them , is the tumour innocent or malignant ? " errors in the prognosis of " early " tumours are explained by the observations that progression is independent of the size or duration of a tumour , and that progression occurs without manifest growth , as in latent or stationary tumours ( rule iii and corollaries )  . 
progression without manifest growth and independently of the size or duration of tumours probably accounts , too , for the otherwise mysterious but clinically important phenomena of long - delayed recurrence and secondary growth after apparent similarly the ultimate failure of several chemo " cure " of primary tumours . therapeutic methods after favourable early response is reasonably attributed to progression in the inhibited tumours . 
some tumours maintained the same type of behaviour throughout their clinical course ; others changed their course , often abruptly , as the result of an irreversible qualitative change in the tumours termed " progression . " the diversity of behaviour of the spontaneous tumours was attributable , in the main , to varied combinations of responsiveness and intrinsic growth rate , and to progression in one or both of these characters . following generalizations or rules of progression summarize the results of the analysis of the behaviour of tumours , especially multiple tumours , in breeding and non - breeding mice : ( 1 ) progression occurs independently in different ( independent progression of multiple tumours . ) tumours in the same animal . ( 2 ) progression occurs independently in different characters in the same tumour . ( independent progression of characters . ) ( 3 ) progression is independent of growth , occurring in latent tumour cells and in stationary tumours . ( 4 ) pro ( 5 ) progression follows one of altergression is continuous or discontinuous . ( 6 ) progression of a tumour does not always reach its end - point native paths . within the lifetime of the animal . these rules are probably widely applicable to the behaviour of varied tumours in animals and in man , and some applications are mentioned briefly . 
 " malignancy " is not a single character . disproportionate or " out - of - step " development of the various characters which determine malignant behaviour ( independent progression of characters ) accounts for many anomalieg in the behaviour of cancer in man , and progression in tumours whose growth is inhibited probably explains the ultimate failure of therapeutic measures which have a favourable immediate effect . i am grateful to l . 
we spent more than eight months working on one such incidental problem , which had to be solved before we could proceed with the main work . this effort was well rewarded , however . 
we not only improved our experimental approach , but also acquired information that will further our understanding of the intricate role played by biological factors in regulating the influence of external agencies on living cells . in view of all this , i should like to point out that our investigations of the genetic potencies of carcinogens are still in an early stage . 
when i learned , therefore , that vapours could reach the sperm of drosophila i was confident that it would be possible to produce fine aerosols of chemical solutions it was evident tbat , if we could develop an aerosol that could do the same thing . method of inducing mutations , we could work with a wide selection of chemicals that are soluble in solvents not injurious to the ' flies , and would not be limited to chemicals that can be vaporized at temperatures not lethal to the flies . after much experimentation we finally succeeded in developing an aerosol technique that is effective in inducing mutations in drosophila males . males are kept for several hours ( from 6 to 200 ) in an atmosphere containing an aerosol of the desired solution ; and after this treatment their sperm is tested for induced genetic changes ' by standard genetical methods . 
the flies are treated in a milk bottle , and the aerosol is generated intermittently , for 30 seconds every 30 minutes , by a de vilbiss nebulizer . in our work with chemicals we have concentrated on carcinogens , because there is a feeling.among geneticists that these coffipounds should also be mutagenic . 
what classifies them as carcinogens is their ability to change normal cells into cancerous cells - that is , to produce permanent changes in living cells , which this definition can also be applied are transmitted to the progeny of those cells . to mutagens , which cause permanent and heritable changes , or mutations , in cells . this series of experiments with carcinogens also included chemically related tests were made with nine polycyclic hydrocarbons ( four non - carcinogens . carcinogens and five ' non - carcinogens ) and with seven azo compounds ( three of them carcinogenic )  . 
the observations were made on induction of x - chromosome .onclusions lethals and of chromosomal aberrations coincident with lethals . reached on the basis of the experimental results are summarized in table i . from table t a definite correlation between mutagenicity and carcinogenicity is evident . 
of the seven carcinogens tested , six were found to be mutagenic ; and of the nine non - carcinogens onlv two were found to be mutagens , and one is still classified as doubtful . the evidence now available suggests that some chemicals ( dibenzanthracene , benzpyrene , and hydroxyazobenzene ) induce both gene changes - le . 
lethals and chromosomal aberrations , whereas some others ( benzanthracene , dimethylaminoazobenzene , and 2 - amino - 5 - azobenzene ) are more effective in inducing chromosomal aberrations . during our experiinentation it was observed that different males treated at the sametime quite frequently showed different results ; that is , genetic changes could be induced in some males m ' ore readily than in others . table ti gives the 116 m . 
at present the most likely solution seems to be that a gene is responsible for the observed variability of effect between different males and between different , experiments . i shall conclude this presentation by quoting freely the conclusions given in a paper presented at the meeting of the fourth intemational cancer research congress in st . 
from these results it seems reasonable to infer a common causative mechanism relating mutagenicity this inference is further strengthened by the behaviour and carcinogenicity . of all known non - chemical carcinogens , such as x - rays and related radiations . ultraviolet rays , and heat - all of which are also mutagenic . 
the most obvious and probable relation ' between mutagenicity and carcinogenicity is the one suggested by the hypothesis that cancer may originate through a gene mutation occurring in a somatic cell . 
such a cell , and the cells derived from it by division , would have their properties changed so that they would behave as cancerous . this would mean that higher organisms possess a gene - - or , more likely , a number of genes - whose mutations can initiate a cancer - type cell . it may be assumed that such mutations , like a great majority of mutations in other genes , would occur spontaneously with a very low frequency . 
the human body has a tremendously large num ' ber of cells , however , so that - it is probable that a cancertype mutation would occur a number of times among the cells of an individual . not all of these need give rise to cancer , since a large proportion of the cancertype cells might be prevented by normal cells from dividing , or might be eliminated in some other way . if gene mutation is responsible for the origin of cancer , then all mutagenic agents may be expected to increase the frequency with which such mutation occurs , and consequently to act as carcinogens . in our fight against cancer , therefore , precautions should be taken to avoid exposure to ' all mutagens chemicals as well as radiations . such precautions , however , even if rigorously enforced , would only lower the incidence of cancer ; they could not entirely prevent its occurrence . there would still be a chance left for cancer - type mutations to occur among the billion 's of cells that constitute the human body , and a mutated cell that continued to divide would give rise to cancerous growth . 
we know that mutations do occur with great regularity , caused by some force not yet explained , and that we have no means of stopping or controlling their occurconsequently , if cancer originates through a genetic change , our chances of finding ways to prevent it are very , very slight . 
a phenomenon , involving the abnormal growth of two kinds of pigmented cers , was recently found in spontaneous tumours experimentary produced by genetic methods in platyfish - swordtail hybrids . the tumorous hybrids were produced by mating a male spot - sided and rub throated platyfish ( platypoecilw maculatus ) to an albino swordtail ( xiphophoru& hellerii )  . 
the ruby - throated pattern is composed of xantho - erythrophores , which are red pig ' ment cers containing erythropterin in granular form and lutein gordon ( 1950 ) and gordon and nigrelli ( 1950 ) and zeaxanthin in solution . indicated that these colour patterns are inherited and referable to two platyfish sex - linked genes : sp for the black and bt for the red pigment cers . 
the genetic analysis revealed that the pigmented tumours were produced in platyfish - swordtail hybrids containing the hnked genes , sp and bt from the platyfish and a number of sp and bt gene modifiers from the swordtail . some of these pigmented tum ' ours were diagnosed as erythromelanomas in an earher report by gordon ( 1950 ) and nigrelh , jakowska and gordon ( 1950 )  . more extensive study of additional specimens revealed that there were two kinds of pigmented tumours involved , first , a red tumour , a xantho - erythrophoroma of the head and , second , a black tumour , a melanoma of the body . in some of the hybrids , cers of the melanoma reached , penetrated and replaced the tissues of the red pigmented tumour . 
only a few macrophages , however , are evident in these tumours . the relatively few dendritic and rounded cells are similar to those described in the simple xantho - erythrophoroma . 
the various stages in the development of the melanoma within the xantho - erythrophoroma can be demonstrated and traced in one of these fishes ( 243 - 11 )  . 
33. - melanotic area of the tumour ( 243 - 1 1 )  . 1 - n this region one or two cells from the original xantho - erythrophoroma can still be distinguished . in other areas , however , a , region just below the epidermis - note the melanotic they are completely absent . cell ( melanoblast ) in metaphase ; b , typical melanotic cell of this region associated with a cell of the xantho - erythrophoroma ; c . 
the melanotic cells ( melanoblast 's ) are smaller and less dendritic than the typical macromelanophores ; they are usuany rounded , sometimes fusiform , varying from 10 to 40 tl at their widest dimensions . 
the present studies , however , show that two distinct tumours are involved : a xantho - erythrophoroma in the head region and a melanoma of the trunk and caudal peduncle . in some of the hybrids the more actively proliferating cers of the melanoma invade and replace the red pigmented tumours of the head , producing an erythromelanoma . the red and yerow pigment cell characteristic of the xantho - erythrophoroma was first described by kosswig ( 1928 ) from normal fish as an erythro - xanthophore . according to goodrich , hill and arrick ( 1941 ) , the cell ; which they caued a xantho - erythrophore , is a xanthophore in which erythropterin is laid down in addition to lutein and zeaxanthin . in fixed and stained tumorous material the xantho - erythrophores are either non - pigmented dendritic , rounded or fusiform cers . in both normal and tumorous tissues the nuclei of these cers ' are weak in chromatin ; nevertheless , mitotic figures are frequently found . 
the degeneration of the xantho - erythrophoroma probably results from the growth - pressure of the apparently more actively reproducing melanotic cers which infiltrate and penetrate the interstices between the xantho - erythrophores . 
whether or not the metastasizing tissue would have comalthough complete pletely replaced the invaded tumour was not determined . replacement of a xantho - erythrophoroma by melanoma has never been observed in our fishes , the evidence seems to indicate that this would have occurred had the specimens lived longer . an interpretation of the nature of the genic action that modifies pigment cell growth and the physiological effects of the interaction of such genes in platyfish - swordtail hybrids was outhned by gordon ( 1948 , 1950 )  . 
the effect of the various genes for pigment cells upon the development of the red , the black and the red - black pigment cell tumours may now be suggested . in the normal platyfish gordon ( 1928 ) showed that the dominant , sex - finked , spot - sided gene , sp , manifests itself in the development of large black pigment cells or macromelanophores ; the large melanophores first appear in postembryonic platyfish in the posterior region of the body , specifically , in the caudal peduncle . 
the number of macro melanophores produced by the sp gene in the normal , spotted platyfish is influenced strongly by the action of the stippled gene , st , a dominant , autosomal factor for the - presence of many micromelanophores . 
when sp is associated with the dominant gene st ( that is , sp st ) , more macromelanophores develop than when the sp gene is associated with the recessive gene st ( that is sp st )  . furthermore , in both the sp 8t post - embryonic and adult platyfish the macromelanophores are restricted for the most part to the caudal peduncle . 
315. - - below , a platyfish - swordtail hybrid of the genetic constitiition rts , 206 - 15 , showing the early stage of the development of the xantho - erythrophoroma . this shows up as a red patch on the left operculum surrounding the lower half of the eye . 
241 , produced by mating a platyfish - swordtail rtsp hybrid , 206 - 12 , exhibiting an erythromelanoma , back to an albino swordtail , 1822 - 6 ; upper left , an albino with an amelanotic melanoma at the tip of a caudal fin ; lower left , a sibling showing the " ghost " pattern of macromelanophores ; right , typical melanotic hybrid showing the ear ' lv sta - ae of melanosis in the posterior region of the body . 
the minimu ' m requirement for the production of the erythromelanoma in platyfish - swordtail hybrids is the presence of the linked genes rtsp . gordon ( 1950 ) showed that a platyfish parent of the genetic constitution of rtsbidrsp would not , while a rtspidrsb would produce some hybrids with erythromelanomas when mated with an albino swordtail . 
in the tumorous animals the xantho - erythrophoroma develops rapidly in the head region , and at the same time a condition of melanosis develops in the posterior region of the body . in some individuals the melanotic cens show great reproductive activity and produce a melanoma . 
in those animals that develop a melanoma the cells of the melanoma may invade the xantho - erythrophoroma and destroy and replace the cells of the red pigmented tumour . in other cases the melanin - bearing cers are restricted to the posterior part of the body , aflowing the red tumours to develop on the head without the involvement of the black pigment cers . 
the sequence of events in the invasion of one kind of neoplastic tissue by another type is discussed from the points of view of histology and developmental genetics . this work has been aided by a grant to the new york zoological society from the national cancer institute , national institutes of health , united states public health service in support of the project : " genetic and correlated studies of normal and atypical pigment cer growth . " some details in this paper were presented by myron gordon before a meeting , of the royal academy of medicine , london , july 4 , 1950 . we are deeply indebted to ' the american museum of natural history for .laboratory facilities , to j . 
oliver. from the radiotherapy and cancer research departments , london ho8piw , london , e.i. received for publication january 25 , 1951 . the distribution of radioactive phosphorus can be investigated in vivo using a thin - walled g.m. 
the maximum range for beta paitioles of p32 in soft tissue is 8 mm . , but the half - value thickness is only of the order of 0 - 6 to 0 - 8 mconsequently , measurements on the skin can only indicate the amount of phosphorus in the superficial layers of the body ( effectively some 3 mdeep )  . however , under favourable conditions , such measurements can be used to demonstrate the increased phosphorus up - take by malignant tumours . low - beer , glenn - bell , mccorkle and stone ( 1946 ) have used this method with some success , as a diagnostic procedure , but its value is reduced by the low penetration of the beta rays and by the increased up - take also found in inflammatory conditions . 
phosphate buffer at ph 7 - 35 . it has been found advisable to check , by counter measurements , that the radioactive material has actuary left the site of injection , as , even after taking more than ordinary care , some unsatisfactory injections have been detected . this is particularly important , of course , when giving the isotope therapeutically , as dose calculations assume that the whole of the material enters the blood streano side effects of the injection were observed . 
the tumour may have received 4 to 8 times the dose calculated above , a total which is in excess of the generally agreed " tolerance " level . this was , however , of no consequence as the site was to re ' ceive an x - ray dose of 3000 to 4000 r . a number of sites over the tumour , on the diseased breast , and at corresponding points on the normal breast , were marked with gentian violet , and measurements of the activities were made with a counter tube applied directly f . 
the background rate was in each case the complete set of measurechecked before and after the series . ments was repeated and a mean value for each site was used . it was not feasible to prolong the counting time at any site ab ' ove about 3 minutes . 
as the count rates with this tracer dose were rather low , the measurements were usually limited to 1000 counts ( 3 per cent standard deviation ) or , after several days and over normal tissue , to only 100 counts ( 10 per cent standard deviation )  . consequently , the ratios of count rates over tumour and normal skin were not obtained very accurately , but the results sufficed to demonstrate large changes . series of measurements were made before , during , and 4 to 6 weeks after the treatment , at which time the x - ray erythema had subsided but the skin of the irradiated breast remained highly pigmented . observations were made on altemate days during 2 to 3 weeks . after intravenous injection , the radioactive phosphorus could be demonstrated immediately ( 5 to 8 seconds ) in the tissues of the breast , but the concentrations continued to increase in both healthy and dis6ased breasts for 10 to considerably lower count rates were observed when the next series 15 minutes . of measurements were made after an interval of 2 days , a change probably due to the excretion of p32 ' thereafter the fall was found to follow a roughly exponential form , corresponding to a " biological half - hfe " of between 7 and 9 typical cases are ifustrated in fig . 
i. and over both axillae are also included . it is of interest to note that the readings , over the forehead ( indicating thep . , 2 content of the frontal bone ) increased to the level found over the tumour and then decreased more slowly than the latter . values of the ratio of count rates over the diseased breast to those over the healthy breast are presented in fig . 
a sudden drop in the ratio occurred after the third irradiation . four weeks after the end of the treatment a second tracer dose was given , and the results obtained are shown in fig . 
for the first three readings the skin was still very red . by the time the erythema had subsided the count rates were rather low , but they appeared to be higher than normal over the whole of the diseased breast , without any locahzed . 
at a later date the authors hope to continue the investigation , although working at different institutions . the countrate due to p..2 was fodnd to be very much higher ( between 3 and 8 times ) over malignant mammary tumours attached to the skin , than over the corresponding parts of the healthy breast . 
no such , change occurred during after erythema stilboestrol treatment in a case which did not respond clinically . had subsided the ratios of measurements over the two breasts were found to be similar to those before treatmentbut the primary growth was still present in all these cases . the authors wish to thank sykes , the chief pharmacist at the hos ital , for preparing the material for intravenous injections , and k . 
argus. from the cancer research laboratory , university of florida , gainesville , florida . received for publication april 7 , 1953 . it has been observed that when certain sulfonic acid dyes , such as trypan blue , are injected into animals with tumors , the neoplasms become more highly unfortunately these dyes concentrate in colored than the surrounding tissue . some vital organs to a much greater extent . 
an investigation by moore , tobin and aub ( 1943 ) of br82 derivatives of evans blue and trypan blue in tumorbearing mice showed that the tumor took up considerably more dye than the surrounding tissue . 
the liver , however , took up about three times as much stevens , lee , stewart , quinlin and gilson ( 1949 ) radioactivity as the tumor . studied the distribution of radioactive iodinated trypan blue , one of the compounds first prepared by bloch and ray ( 1946 )  . 
the concentration of radioactivity in tumor tissue was several times greater than that in skeletal muscle or skin , but considerably less than in the liver , spleen and kidneys . the purpose of the present study was to deternine if such localization in vital organs is a necessary concomitant to tumor localization by aromatic sulfonic acids . because radioactivity offers a ready means of detection , the need of a colored derivative no longer exists and sulfonic acids other than dyes may be employed . since certain derivatives of fluorene are known to produce tumors in various sites in the animal body ( bielschowsky , 1944 , 1947 ; morris , dubnik and johnson , 1950 ; wilson , deeds and cox , 1941 ) , it is possible that other derivatives of this molecule might be directed to tumors already present . 
the 2 , 7 - disulfonic acid of fluorene was selected and this compound was prepared labelled with s35 . benzene sulfonic acid injected into dogs can be recovered unchanged in the urine ( williams , 1947 )  . 
sammons , shelswell and williams ( 1941 ) report that p - hydroxybenzenesulfonic acid is excreted unchanged from rabbits . it does not even form an ethereal sulfate despite the fact that it possesses a phenolic hydroxy zehender ( 1943 ) found that the amino group of sulfanilic acid ( p - aminogroup . benzenesulfonic acid ) is acetylated to the extent of 75 per cent in the guinea - pig , but that no cleavage of the sulfonic acid group from the ring occurs . 
a study of various aminophenolsulfonic acids by sammons , shelswell and williams ( 1941 ) also indicates that these compounds are eliminated unchanged . it is , therefore , apparent that aromatic sulfonic acids are stable compounds . since there is no evidence to indicate that the sulfonic acid groups of fluorene2 , 7 - disulfonic acid would be removed from the molecule , the distribution of radioactivity following administration of the compound labelled with s35 should 274 mary f . 
2 , 7 - fds35 having a specific activity of 39 , 660 counts per minute base experiments in which the animals received twice this concentraper mg . tion of the compound failed to reveal any toxicity symptoms . the animals were sacrificed at 2 - , 8and 32 - hour intervals following treatment , and pooled samples from 2 animals were used for each determination . 
samples of blood were plated directly on planchets . radioactivity measurements were made in an internal - type counter ( q - gas chamber and nuclear instrument and chemical corporation scaler , unit model 162 ) with an efficiency of 45 per cent . 
the concentration of 2 , 7 - fds35 in the tumor was over three and one - half times that in the spleen and two and onehalf times that in the liver . 
with this same compound the kidneys and spleen concentrated over three times as much of the dye as did the tumor . a much more favorable situation is found in the distribution of 2 , 7 - fds35 . at 8 and 32 hours only the kidneys had a slightly higher concentration of this compound than did the tumor . 
at no time was the localization of the fluorene derivative greater in the liver than in the tumor , and after 32 hours the concentration was two and one - half times greater in the tumor tissue than in the liver . 
by comparison with similar ratios for 1131 - labelled trypan blue , the fluorene compound has increased the ratio of localization in tumor tissue compared to liver , kidneys , spleen , blood and muscle . this investigation showed that the localization of a sulfonic acid in the liver and spleen of tumor - bearing mice 278 mary f . 
ray for his valuable suggestions and to hilda banks for technical assistance . this work was supported by a research grant from the national cancer institute of the national institutes of health , u.s. 
ritchie. from the division of oncology , the chicago medical school , 2755 west 15th street , chicago 8 , illinois . received for publication july 31 , 1953 . by studying the life of various kinds of spontaneous and induced tumors in animals , it has been found that they sometimes undergo irreversible changes in character . for example , a papilloma induced in mouse skin by applications of carcinogen , may become a carcinoma , so changing its character ; or a spontaneous tumor of the mouse breast responding to pregnancy by an increase in growth rate may change its character and no longer respond to this stimulus . foulds ( 1949 , 1950 , 1951 ) made a special study of these changes in character , calling them " progressions " , and defining " progression " as an " irreversible , qualitative change " in a tumor . foulds then went further , claiming that different characters of the same tumor could progress independently of one another . for example , he found that in spontaneous mammary tumours in mice one character , the growth rate , might progress , and the tumor grow faster , while another , the responsiveness to pregnancy remained unchanged . foulds ( 1949 ) studied not only the spontaneous mammary tumors of mice , but also bladder tumors induced by feeding 2 - acetylaminofluorene to mice ( foulds , 1950 ) and transplantable mammary fibroadenomata in rats ( foulds , 1951 )  . in each case he found that the tumors did sometimes progress , and that progression could occur independently in different characters of the same tumor . these findings seemed so interesting as to make desirable further confirmation , and this paper records an investigation of the life of tumors induced in mouse skin by repeated applications of 9 , 10 - dimethyl - 1 , 2 - benzanthracene . 
ritchie the second type of sessile papilloma consisted mainly of epithelial tissue . the architectural pattern of the normal human epidermis was imitated , the epidermis being thickened from four to six times . 
the surface of the tumor was often hyperkeratotic . in a few cases a tumor of this type arose in a pedunculated papilloma . sheets of closely packed cells invaded the dermis and muscularis . 
most of the tumors grew at a steady rate throughout , in so far as the growth rate could be determined by the crude method used . however , definite changes in growth rate did occur . 
8 to 11 , and will be described individually , each mouse having tumors with differing behaviors demonstrating the validity of one or other of fould 's proposals . all charts illustrate the validity of rule 1 : namely , that progression occurs independently in different tumors in the same animal . 
9 also confirms fould 's rule 2 , showing three tumors , a , b and c progressing from one morphological type to another while growing at a constant rate . this type of progression , from one morphological type to another , without progression in growth rate , was much more common than progression in growth rate alone , as seen in this chart in tumor d . 
10 , and confirms the validity of fould 's rule 3 , that progression is independent of growth . in the same chart , in tumors a and b may be seen again a change in growth rate without a corresponding change in morphological type . * n 5 31_ * - - __ + * - - + b ..od / , ' / ___ _ , / " ... 
11. - showing independent progression of multiple tumors . tulmor a was malignant at its first clinical appearance , showing that at this period of its development a tumor can be all other tumors began as sessile papillomata . 
a well - known example of progression affecting only part of a tumor is the carcinomatous change which sometimes affects the tip of an adenomatous polyp of the colon in man . foulds ( 1949 ) remarked that progression could occur by gradual change or by abrupt steps . in general , the changes seen in the tumors of this experiment occurred abruptly . 
a step - wise transformation of different characters in these tumors was observed throughout their existence . this investigation was supported by a cancer control grant from the national cancer institute of the national institutes of health , u.s. 
murray. from the radiation therapy department , johannesburg general hospital , the non - european hospital , and the south african institute for medical research , johannesburg . received for publication january 10 , 1953 . skin cancer is relatively infrequent in the african . in the three - year period 1949 to 1951 , during which time 590 cases of malignant disease in africans were referred to the radiation therapy department , only 50 cases of skin cancer were encountered . 
the pigmented skin of the african would , of course , be largely protected from this effect , and indeed when skin cancer does make its appearance , it is almost invariably in areas exposed , not to sunlight , but to other types of chronic irritation . we have also observed distinct differences in pathogenesis , and the rate of growth and dissemination of skin tumours in the african , as compared with the m . 
murray classical description of the disease in europeans . these factors have compelled us to adopt a different approach to the management of skin tumours in the two races , and to revise our views on the surgical and radiological curability of skin cancers of various histopathological types . since these racial differences might be of some interest in the study of the demography , endemiology , and management of cancer in africa , it was considered worth while putting our experiences on record at this stage . the population from which this material is drawn consists of approximately 2 , 000 , 000 africans of the bantu race inhabiting the southern half of the transvaal , and originating for the most part from the sotho and zulu tribes . 
about onequarter of this population is urbanised and resident on the witwatersrand , but a much larger fraction of the hospital population gives an urban address . this is due , in part , to many rural patients living with relatives in the urban area prior to entering the hospital and witholding their true addresses , and also to the greater tendency among rural natives to receive treatment from indigenous herbalists in the absence of suitable vital statistics it is impossible rather than in hospitals . to state the age distribution of the bantu population , although it is safe to assume that the average age is somewhat lower than that of the european group . 
the ratio of males to females at the time of the 1946 census was 1 - 33 , the predominance of males presumably reflecting the migratory labouring class . from the genetic point of view it is important to bear in mind that the bantu inhabitants of south africa originate from central and east african tribes , who have , at least within historic memory , had no admixture of european blood . 
by comparison , the negro of the united states originates from west african ancestry and is largely a product of prolonged hybridisation . although environmental conditions in the southern states of the u.s.a. 
are not dissimilar to those encountered by the bantu in the transvaal , the two groups generally show a very different incidence and distribution of malignant disease ( higginson , 1951 ; and robinson , 1951 )  . 
the cells are arranged in the form of distorted , branching tubules or of alveolar masses . in some areas the cells are separated from the surrounding stroma by a well - defined basement membrane while in other areas the cells appear to infiltrate into the stroma . 
as the cells approach the lumen they become larger , the cytoplasm becomes faintly eosinophilio and sometimes vacuolated . the nucleus becomes smaller , more dense , and shows a well - defined nuclear membrane . the nucleus in these cells lies centrally , and their whole appearance is that of lipoid containing cells resembling those of the sebaceous glands . 
he was admitted from an outside hospital with a history of having had a tumour of the right upper arm excised 10 months previously , and that the lesion has subsequently recurred . there was a massive tumour present on the right upper arm and shoulder region , surrounding a vertical scar of the old excision . 
he became very ill , and was transferred home after further palliative x - ray therapy to the lumbar spine . the 2 cases of " sebaceous gland carcinoma " , although showing advanced disease , clearly illustrate the extreme radiosensitivity of these tumours , with conventional large field x - ray therapy . 
one patient is free from disease , while the second has extensive and incurable tumour . albinism and cancer of the skin . it is remarkable that there were 12 albinos among the 50 cases of skin cancer reviewed , although the albino trait is rare in the african . 
the exact incidence of albinism in the bantu is not known , but a cursory review of recent hospital records suggests that it cannot be greater than 1 in 5000 , and is possible less than consequently the 12 patients seen , representing the appearance of 1 in 10 , 000 . 4 new new cases annually ( and probably several more who do not attend hospital ) , implies that a large proportion , if not all of the albinos among the transvaal bantu necessarily develop skin cancer in early adult life . this observation is in agreement with the experimental findings of findlay ( 1928 ) , beard , boggess and von haam , ( 1936 ) and the recent precise quantitative investigations of blum ( 1950 ) , who have demonstrated that albino animals exposed to daily insolation or ultraviolet irradiation for a significant fraction of their life - spans invariably develop malignant skin tumours . all 12 patients showed complete albinism of the whole skin surface including the hair and eyes . 
we did not encounter any cases of partial albinism , such as those described by gelfand ( 1944 ) and shown to have the same propensity for skin cancer as the true albino . however , there was one case of xeroderma pigmentosum ( not included in table i ) occurring in a 4 - year - old bantu child in whom the whole skin surface showed the characteristic regular mottling caused by depigmented patches alternating with areas of increased pigmentation . 
murray pigment - free zones , especially those of the head and neck , possessed the characteristic hypersensitivity to light and were the origin of several histologically proved squamous carcinomas . there were 8 males and 4 females in the series . the age distribution of skin cancer in albinos shows a distinct tendency for the disease to occur in younger age - groups than in normally pigmented persons . there was 1 patient in the second decade , 3 in the third , 5 in the fourth and 3 in the fifth decade . 
we have not had the opportunity of observing the subsequent history of skin areas cleared of all macroscopic keratoses by podophyllin , and , in consequence , are not able to assert that the onset of skin cancer is , in fact , prevented . however , berenblum 's ( 1951 ) observations on the definite anticarcinogenic effect of podophyllin , even in the presence of actively carcinogenic hydrocarbons , suggests that this material may have a true prophylactic action . 
two to 3 weeks before admission black lumps appeared on the skin in the elbow region . on admission the patient had a typical malignant melanoma over the thenar eminence of the right hand . 
the primary growth and axillary glands were given 250 r daily to a total of 5500 r , other areas were treated with 1500 r and 1000 r daily to totals of 4000 r , 4500 r , and 6000 r , and six small areas were treated with three daily doses of 2000 r . all treated areas responded clinically by regression of the tumours and some necrosis of the tumour surface , but histological examination after the radiation showed minimal changes , a few lesions treated with 1000 r daily for 6 days disappeared completely . weeks after admission it was noted that the supraclavicular glands were enlarged and painful , but the intervening skin appeared normal . ten days later small black nodules were visible in this skin area . 
in 1940 , however , an important change was made in the method of selecting the main cause when more than one was mentioned , a disease certified as merely contributory and not in the direct line of causation being ignored if another well - defined condition was stated as the direct cause of death . 
for breast cancer in women , for example , the factor to be applied to a rate at all ages prior to 1935 was * 941 , signifying that the new procedure resulted in about 6 per cent of deaths which would previously have been credited to breast cancer being classified from 1940 onwards to some other cause . when it is desired to study the trend of mortality at particular ages it is not safe to assume that the correction to be applied to rates before 1940 is the same at every age , until that has been tested , as may be done by examining the ratios at different age groups between the deaths in 1939 based upon the old and new methods , tabulated for that purpose in table 21 and appendix bl of the statistical review for that year . 
for certain diseases where it was important , such as diabetes , more exact correction factors based on the dual classification carried out during the four years 1936 - 1939 were used in the registrar - general 's analyses of past death rates at separate age - groups , and on page 135 of the text volume of the review for 1938 - 1939 it was shown that for cancer of all sites combined the conversion ratios for each sex were slightly above unity at ages before 45 and below unity at ages after , diminishing regularly from 1 - 17 at 5 - 14 to * 95 at 75 and over for males . 
for cancer of the breast in females it can be deduced from the tables in the review for 1939 referred to above that the correcting factor diminishes progressively from * 997 at ages 25 - 29 to * 970 at 55 - 59 and * 810 at ages 85 and over . this is easy to understand because of the increasing frequency of the presence of breast cancer , in its primary or secondary manifestations , as age advances , coupled with increasing liability to die of some intercurrent disease which is certified as the direct cause of death . throughout these studies of the trend of death rates according to age , correction of the rates in years prior to 1940 has been carried out by means of factors derived jointly from the age - by - age comparison of the deaths in 1939 and the conversion ratio forall ages combined obtained from the dual tabulations of 19361939 . 
in 1950 - 51 it was possible for the first time to distinguish mortality from cancer of the cervix and corpus uteri as a result of the inquiries by the general register office concerning the large number of deaths certified as cancer of " uterus " without further definition , and the rates for cervix uteri show still lower proportions of single women and greater contrasts with cancer of the breast and other causes of death . amongst women who died of cancer of the cervix in 1950 - 51 at ages under 55 the proportions who had never married were about one - third of the corresponding proportions amongst women who died of all causes . 
at ages 55 - 74 the proportion was about two - fifths , and after 75 it was about three - fifths . in the registrar - general 's statistical review for 1940 - 45 ( registrar - general , 1951 ) deaths of married women from various causes were analysed by age groups according to whether the deceased women had borne any children or not , and the resulting proportions stated at death registration not to have had a child are shown in table iv for cancer of the uterus , breast and ovary , non - genital cancer and all causes . 
2 , in sharp contrast with those for uterine cancer , show on the whole very little change through 25 10 o > 9a t > 7 - id 5 - s = ~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~i 1921 - 26 1926 - 30 1931 - 35 1936 - 40 1941 - 45 1946 - 50 40 period when death occurred age when death occurred fig . 
at ages over 65 the rates increased up to 1940 and then fell back slightly , and between ages 30 and 45 the rates have increased since 1940 . this may be seen by expressing the rates in 1936 - 40 as percentages of those in 1926 - 30 , and the rates in 1946 - 50 as percentages of those in 1936 - 40 ( table x )  . in the right - hand part of fig . 
the increase in breast cancer mortality of married women to be expected at ages over 45 in the last 20 years would be , therefore , about 2 per cent of the rate . information as to the numbers of pregnancies experienced by women who later develop breast cancer at various ages is scanty , and the only data found suitable for the purpose of this study were in a tabulation by smithers et al . 
at ages under 45 the effect seems to be even greater , but the numbers on which the ratios are based are small , and there might be other reasons contributing to the low frequency of women with four or more children amongst patients seen during the period of childbearing . it is desirable that this inverse correlation with number of children should be confirmed by other and larger data , and such information is in process of collection in the liverpool hospital region and north wales by the british empire cancer campaign . assuming it to be correct , what effect would the decline in family size since 1905 be expected to have upon the incidence of breast cancer amongst all married women ? this can be calculated by applying the ratios for women over 45 to the successive distributions in table via and aggregating the products , as was done for uterine cancer . 
lung cancer death rates and also those from other forms of cancer tend to increase steadily with advancing age , so movements of the ratio will give no indication of that part of the upward progression which lung cancer shares with other cancer . 
the years of birth of the cohorts attaining these ages in 1901 would be 1882 - 1886 , centred at 1884 as the table indicates ; in 1931 the men of this cohort would be aged 45 - 49 , in 1933 their ages would be in calculating the ratio for the 1884 cohort in 1933 , three times 47 - 51 , and so on . the deaths at 45 - 49 were added to twice the deaths at 50 - 54 in 1933 , both for lung cancer and all other cancer , and the first total divided by the second . 
the " nil " increases in table xvi from 1937 to 1940 mean that in the cohorts bom before 1875 the lung cancer death rate was then rising with advancing age after 65 at about the same gradient as the death rate for all other cancer , and the actual gradient at that age and time period has been shown to be about 33 per cent increase in 5 years or 20 per cent in a trienniuthe preceding explanation for what occurred between 1925 and 1937 is far more probable , but the hypothesis of influenza as a contributory factor cannot be excluded as a possibility . from 1937 onwards sulphonamides began to be used in increasing amount , and pneumonia deaths soon began to fall . could this have affected lung cancer rates appreciably by keeping alive longer many persons who without sulphonamides would have died of a complicating pneumonia before the cancer could be recognised ? pneumonia death rates of males fell between 1937 and 1942 from 477 to 255 per nillion at ages 35 - 44 , from 950 to 457 at 45 - 54 and from 1535 to 1024 at 55 - 64 , and the fall continued till 1946 . during that period the lung cancer ratio continued to rise steadily in men born about 1880 , the gradient being steeper amongst men at ages around 40 and 50 than around 60 , and only slight after 65 . 
the distribution according to number of children born for hospital patients with breast cancer , in such data as are available , differs from what would be expected , and it is estimated tentatively that the bearing of 2 or 3 children reduces the likelihood of this form of cancer developing after 45 by about onefifth and that 4 or more children reduces it by about two - fifths . 
from 1937 to 1946 the lung cancer ratio continued to rise by about 7 per cent of the ratio annually in men born since 1890 , more slowly in men born between 1875 and 1890 , and inappreciably in cohorts born before that ; but after 1946 the increase again spread to all ages . sulphonamides , and later penicillin , must have contributed something to this by preventing some men from dying from penumonia without cancer having been diagnosed and allowing them to die a year or so later of recognised lung cancer . 
ghadially. from the department of pathology , the univemity of sheffleld . received for publication may 18 , 1951 . havingobserved that regeneration of hair in a clipped area on the back of a rabbit did not occur uniformly over the entire area , and occurred after varying intervals of time in different animals , it was decided to investigate the mode of hence , a band of hair , approximately regeneration of hair on the rabbit trunk . 4 inches wide , completely encircling the trunk , was removed from a few rabbits , and it was observed that the depilated skin was not uniformly pink , but that there were roughly linear bluish - black bilaterally symmetrical zones . besides these major dark zones , there were , in some animals , a few small irregular patches of a similar colour . 
the skin in these dark zones felt thicker than the rest of the after two days , when the animals were inspected , it was found that there skin . was prohfic hair growth in the dark zones , which continued until the hair reached its normal length , but during all this time no hair growth was observed in the pink zones . 
for a further period of 12 weeks with 2 per cent w / w , 9 : 10 - dimethyl - 1 : 2 - benzanthracene in lanohne , which was warmed to melting - point to facihtate apphcation . 
the animals were photographed at the beginning ofthe experiment and on numerous subsequent occasions . skin biopsies were taken at intervals from 3 experimental and 2 control animals . these were fixed in alcoholic bouin and sections were stained with haematoxylin 354 h . 
with the appearance of the papillomata changes began to occur in the surrounding skin ; the hair on the painted side now failed to show the vigorous growth it had shown so far . 
as already stated , by this time the whole of the skin on the painted side had attained a uniform appearance , and no distinction between active and quiescent zones was seen . 
the epidermis was much thicker than either the this change appeared to extend down active or quiescent skin before painting . into the folhcles , which were more prominent and deeply seated and showed the usual arrangement in groups . 
mottram ( 1944a , 1944b ) showed that the skin of mice can be sensitized by painting with croton oil , so that a subsequent single application of 3 : 4 - benzpyrene leads to an abundant production of tumours and a single application of carcinogen followed by repeated applications of croton oil also procluces tumours . 
hence mottram ( 1944b ) concluded that carcinogenesis was composed of three phases : ( 1 ) a " sensitizing factor " which could be brought about by preliminary treatment with croton oil , acting presumably in a non - specific manner by causina hyperplasia , on the supposition that proliferating cells were more responsive than resting cells to the specific ( 2 ) a " specific cellular reaction " induced carcinogenic action which followed . by the specific action ( even of a single application ) of a carcinogen , this representing the essential neoplastic change . ( 3 ) a " developing factor " responsible for the actual appearance of a visible wart , and produced by croton oil of by a carberenblum and shubik ( 1947a , 1947b ) confirmed the latter part of his cilnogen . observations , but found no evidence to suggest that a prelimi - nary croton oil hyperplasia had an augmenting influence on tumour production , which would 356 h . 
the depilated skin showed bila ' terally symmetrical dark zones which showed prolific hair growth within a few days , the rest of the skin remaining 9 : 10 - dimethyl - i : 2 - benzanthracene.in lanoline was painted on the left bald . half of 6 animals ; the remaining 4 were painted with lanoline . 
the following changes were observed : ( 1 ) within 30 days the painted area in the experimental animals became dark and showed prolific hair growth , while on the opposite side there was suppression of hair growth , the skin becoming bald . ( 2 ) in all animals initial papiromata appeared at the site of an originary active zone . 
the first papilloma appeared after 53 days . ( 3 ) after the appearance of papillomata hair growth ceased and zones of activity appeared on the opposite side . ( 4 ) the first carcinoma appeared after 81 days at the site of an originary active zone . it was concluded that ( a ) the naturally occurring zones of increased mitotic activity which continued for some time after the first painting must have acted as a promoting agent ; ( b ) it seems more probable that the tumours arose from hair folfcles , and not the epidermis , as the former are the site of increased mitotic activity during hair growth . it gives us great pleasure to express our thanks to professor h . 
keyser. from the department of pathology and bacteriology , wel - sh national school qf medicine , cardiff . receivecl for publication march 13 , 1954 . many observations have been published on the effect of disease or injury on the concentration of protein - bound carbohydrate ( polysaccharide , protein sugar ) or various carbohydrate - rich protein fractions in the blood serum , both in human beings and in animals . 
a study of the level of serum polysaccharide in various diseases led seibert , seibert , atno and campbell ( 1947 ) to suggest that a raised however , shetlar , bryan , concentration is associated with tissue destruction . foster , shetlar and everett ( 1949 ) put forward an apparently opposing view , namely , that such increases are a reflection of tissue proliferation or repair rather than of destruction . this paper deals with an investigation undertaken to find out what effect nitrogen mustard ( the bis compound , di ( 2 - chloroethyl ) methylamine hydrochloride , was used throughout ) or irradiation treatment might have on the serum polysaccharide level in patients with various neoplastic and allied diseases . ( in such patients raised values are usually found . ) it was hoped that sonie light might be thrown on any relationship between the polysaccharide level and tissue proliferation or destruction , since the nitrogen mustards and x - irradiation are known to cause tissue destruction or at least to inhibit actively growing tissues . another ob ' ect was to find out how much of any increase was contributed by the mucoprotein fraction . 
p - , a man , aged 50 , suffering from hodgkin 's disease , was admitted to bospital on 30.iii.50 for bis second coursfof nitrogen mustard . since the first course of - treatment a few months previously there had been an increase in essential case notes are as fohows 240 j . 
keyser dailv injections resulted in improvement correspoindidg the size of the glands . with a fall in the total white cell count and total polysaccharide , which was down nearly to normal a week after the beginning of treatment ( see table i )  . 
no significant fall in the polycourse . saccharide level occuited during the course of injections , but within 3 weeks after the end of the course it had faren by 40 mg . 
on examination it was found that the whole of the left breast was involved by growth , and biopsy showed there was no radiological evidence of secondary deposits squamous carcinoma . in chest , thorax or pelvis but there was body destruction of the radicles and laminae of vertebra u . 
at the end of 2 months , however , the total polysaccharide had fallen considerably and the mucoprotefn fraction to a lesser extent . healing of the medial half of the right breast area was progressing satisfactorily . 
on examination ( about september , 1950 ) the patient had a large mass of glands involving the whole left side of the neck , and the left tonsil was enlarged and fleshy - looking . biopsy of the neck glands showed the presence of hodgkin 's disease . 
the polysaccharide ( total and mueoprotein ) soon began to increase again , though the patient appeared to be in good health . after several months , however , she began to complain of tiredness and aching associated with a feeling of pyrexia in the evenings , for several clays at a time . these symptoms were apparently unconnected with the menstrual cycle . 
a temperature chart kept by the patient from january to may , 1952 , showed that on these days there was in fact a rise of temperature idthe evenings , usually to 100 - 101 ' f . 
normal figures found ' m this laboratory for the distribution of polysaccharide betweedthese fractions are given in table il the polysaccharide soon began to increase again and the patient 's condition deteriorated . 
 ( 1947 ) found a correlation between the levels of serum a - globulin and polysaccharide in their series of cases . using the tryptophan - perchloric acid test ( cohen , 1944 ; seibert et al . , 1948 ) we obtained evidence of a rise in the level of a serum constituent , that was believed 248 j . 
keyser to be probably polysaccharide in nature , after buming ( keyser , p949 , 1950 )  . the reaction has since been shown to be due to a polyhydroxylic acid of unknown structure ( " sialic acid " ) occurring in the proteins ( werner and odin , 1952 )  . more recently we have employed the orcinol method : both in burns and in fractitre cases pronounced rises in the level of serum polysaccharide ( total and mucoprotein ) were found ( keyser , 1952b )  . this is consistent with the tissue destruction hypothesis , but the increase might equary wer bave been connected with healing processes . that increases in the serum polysaccharide concentration occur in adimals after experimental injury was shown by shetlar , bryan et al . 
the response was a delayed one , with a maximal elevation in 3 to 6 days after the increases in polysaccharide were produced by ( among other methods ) injury . injection of talc suspensions or intrapleural injection of turpentine , causing conditions in which little tissue destructions was thought to occur ; fever was not essential for the elevation ; and the length of time that elapsed before the polysaccharide level returned to normal seemed to be correlated with the extent of repair taking place . 
they give no details , however , except in one case in which a small temporary rise is attributed this patient had previously undergone surgical removal of to inflammation . increases in the level of blood " polypeptides " as a result of the carcinoma . radium and x - ray treatment were reported by cristol and puech in 1930 . 
effect due to inhibition of a breakdown process in and around the tumour and depending on tumour growth . such a break - down process might be expected to be greatest when the tumour is growmg rapidly , and to be retarded when the tumour is subjected to an inhibitory influence such as that of the nitrogen mustards or irradiation . 
working with mice , catchpole ( 1950 ) found that connective tissue bordering on tumours contained increased amounts of water - soluble mueoproteins ; and histochemical studies suggest that in the region of tumours a process of depolymerization is taking place , whereby the components of the ground substance may become water - soluble and enter the general circulation as mucoproteins ( catchpole , 1950 ; gersh and catchpole , 1949 )  . 
the existence of such a mechanism would go far tciwards reconciling the " tissue destruction " and " tissue proliferation " hypotheses , since the two processes - growth of the tumour and consequent depolymerizait remains to be determined what tion - would be associated with one another . bearing the depolymerization hypothesis has on the rises in the level of serum this and other aspects of the problem are mucoprotein observed after in ' now being studied . in four of our cases urinary total nitrogen and nitrogenous constituents were measured in the hope that they might provide an indication of any tissue destruction taking place . that no consistent changes were found was perhaps to be expected , in view of the results of danowski et al . 
wood of the radiotherapy department for calculating the estimnated integral doses referred to in table i ; to dodwell of whitchurch hospital for much help in obtaining specimens of blood ; to our haematology laboratory for blood counts ; to a . 
cohen. from the experimental oncology laboratory , radiation therapy department , johannesburg general ho8pital . received for publication february 11 , 1954 . there are many reported examples of animals having been rendered immune or resistant , by various procedures , to subsequent inoculations of a tumour to which they are normally susceptible . 
with an adequately inbred strain eke the c3h mouse , however , and using homologous mammary tumour which has not lost its genetic specificity by repeated serial transplantation , absolute resistance to further implants of the same tumour cannot be evoked . it was previously shown that the radiosensitivity of a homologously - transmitted tumour is a function of the state of resistance of the host . 
when the tumours had reached the standard size of about i cin the largest diameter ( overall average volume 250 481 mm.3 ) , thev were irradiated in situ with our standardised techni.qu ' e as previously reported in detail . all mice were individually numbered and examined at regular intervals for at least 3 months after treatment . with the doses used in this series , the tumoiir has , within this observation period , either disappeared completely or bas resumed active growth , ulcerating the skin and killing the mouse by exsanguination or infection . in order to detect any acquired increase in radiosensitivity , tumours arising from each attenuation - dosage group were treated at three dose levels : 3500 , 4200 and 5000 r , making a total of six categories tested . 
1 - 27 ( 0 - 07 * )  . since this ratio exceeds unit the ld , for the attenuated homoplasts is found to be 4500 ( 200 * ) r , compared with 5700 r previously determined in the controls , and the coefficient of variation is 26 per cent compared to 9 per cent in the controls . 
the relative radiosensitivity of attenuated tumours with reference to the controls , that is the ratio of the ld50 's is four times its standard error , the result is highly significant ( p < 0 - 0001 ) , indicating a definite acquired radiosensitivity of the tumour arising from an attenuated implant . as has been previously shown , a changed radiosensitivity generally reflects an underlying change in host - resistance to the tumour . 
it would appear , therefore . , that the attenuation procedure , while not producing any absolute immunity to further implants of the same tumour , nevertheless induces within the host , albeit the strain of origin of the tumour , a subliminal resistant state . 
of the 22 " recipients " ( 2 to each donor ) , 1 1 were similarly treated in situ with 4200 r in order to detect persistent acquired radiosensitivity in the tumour transplants , and the remaining ii were treated with 7500 r in8ituto exclude the possibihty of an acquired radioresistance . 
the added disadvantage of bilateral treatments , even when the immediate mortahty could be reduced , was the possibility that the increased body dose would lower the expected percentage of cures , as previously demonstrated ( cohen and cohen , 1953b )  . 
the results of ' treatment of the attenuated homoplasts in the four experimental categories are shown in table ii , and the proportion of cures in each group plotted in fig . 
1 it can be seen that the proportion of cures to be expecied at this dosage with unattenuated homoplasts ( line a ) is exceedingly small , while in animals bearing attenuated implants ( line g ) it is 40 per cent , from which this result . 
the attenuation procedure , therefore , seems to induce a degree of resistance , presumably a similar antigenic difference between host and tumotir , at least as great as that engendered by the tumour growing in f , ilybrids harbouring the milk factor . the following facts conceming the nature of this phenomenon have been elucidated : ( 1 ) while not excluding the possibihty that the tumour cells have been inherently changed by this procedure , it is obvious that any such change is not , in itself " sufficient to affect the radiosensitivity of the transplanted attenuated conversely , there is no evidence of " takes " in the environment of a new host . acqiiired radioresistance in the tumour as a result of previous irradiation , in conformity with montgomery and warren 's findings ( 1953 )  . ( 2 ) it is unlikely that any local change in the tumour bed contributes to the changed radiosensitivity since no cures were obtained when recurrences followina the local excision at the original site were treated . it can probably be assumed , too , that damage to the tumour bed by the rsurgical excision was sufficient to abrogate the effect of systemic resistance . ( 3 ) since the increased radiosensitivity persists even where the tumour has 318 a . 
cohen been transplanted to another site in the original donor , it must be concluded that the effect is due to a systemic , generalised resistance mecbanism . the phenomenon of induced resistance to experimentalfy transmitted . 
cancer has been extensively investigated . in the past , results in this field were often contradictory and confusing ( woglom , 1929 ) , due to the use of heterogeneous strains of animals and gentically alien tumours . 
the long transplantation history of these and other commonly used tumours , maintained solely by serial transmission , is surveyed by dunham and it is generally realised that such procedures may perrnit antistewart ( 1953 )  . genic diversification or mutation in the tumour , which , in effect , results in a relatively unstable host - tumour relationship . consequently , many of these findings are largely invalidated in so far as their applicability to human cancer therapy is concemed . it would appear that only when a supply of spontaneous tumours is constantly availdble within a given strain , and is routinely transplanted through no more than a few subpassages to experimental animals of the same strain , can the hosttuniour relationship be considered adequately stabilised . 
where such stringent conditions prevail , absolute immunity to a tumour cannot be evoked ( bittner , 1936 ; barrett , 1940 ; lewis , 1940 ; fardon and prince , 1953 ; foley , 1953 )  . 
a recent review by hauschka ( 1952 ) contains an extensive analysis of the immunogenetic complexities of host - tumour relationships used in experimental cancer reseal - ch . with respect to the cm mammary carcinoma , the authors have shown that , even where some degree of immunogenetic difference existed between the tumour and the host , as in the case of f , hybrids bearing the parent strain tumour , no overt - immunity could be elicited by curing the comparatively radiosensitive tumour in8itu ( coben and coben , 1954 ) , or by previouslv inoculating the animals with radiation - attenuated fragments ( unpubhshed data )  . when one correlates these facts with the findings of the foregoing experiment , it become 's evident that resistance to tumour is by no means an " all - or - none " pbenomenon . it seems likely that partial or subliminal states of resistance can be induced in the stable host - tumour relationship which , while not obviously detectable by conventional methods , nevertheless yield significant results in the form of a perceptible increase in radiosensivity . in this connection , it is significant that gorer ( 1947 ) demonstrated high titres of circulating anti - tumour iso - antibodies in mice dying of foreign strain tumour transplants , which grew progressively in spite of antigenic differences with the hosts . 
when the previously attenuated homoplasts were transplanted from the original hosts to new hosts , however , the curative dose reverted to that of unattenuated tumour . it is considered probable that the inoculation of a viable tumour fragment , attenuated by sublethal doses of radiation prior to implantation , induces a state of subliminal resistance in the host which enhances the radiosensitivity of the resultant tumour . facilities for the maintenance of our experimental animals were generously provided at the south african institute for medical research by j . 
3. received for publication january 18 , 1949 . the investigation of carcinogenic substances which have been obtained from human tissues ( kleinenberg , neufach and shabad , 1940 ) and from other biological sources has been the subject of earlier publications from this institute ( hieger , 1940 , 1941 , 1946 , 1947 ) , reporting that : 1 . 
technique used in these experiments for testing for carcinogenic activity . unless otherwise stated , the substance is injected subeute ( 15 per cent solution in lard ) into mice of c57 strain or of mixed commercial stock . 
control experiment on reagents used in the saponification of tissue by potassium hydroxide and alcohol . since the great majority of the carcinogenic fractions had undergone saponification at least once , control experiments on the process itself acting on noncarcinogenic tissue components were made . 
distilled alcohol for 2 - 3 hours and then carcinogens might be formed during extracted several times with ether . saponification from precursors in the tissues or from the reagents themselves . in the earlier experiments the alcohol was industrial spirit ( the manufacturers state that it consists of ethyl and methyl alcohols in the ratio of 19 : 1 with 5 per cent water ) , which in separate experiments was found to darken rapidly on refluxing with koh owing to resinous condensation of aldehyde . acetaldehyde was therefore refluxed with koh and spirit under the same conditions as those of tissue saponification . 
 " n on - cancer liver " indicates the liver of a human subject who has died of any cause other than cancer . ( b ) fraction a from mixed cancer livers , partly the same as those used for the preparation in ( a ) , was crystallized from 80 per cent aqueous alcohol after adsorption from petrol ether on to a large column of a1203 eluted with petrol ether - benzene - meoh ( 80 - 20 - 20 )  . 
the possible reasons for the absence of tumours are discussed below . ( d ) a similar fractionation was made on another batch of cancer livers , and mice were injected with material from g , c , f , d , e and h . 
the test on f was repeated on a further 10 mice in which one tumour arose after 2 years . ( f ) the 10 fraction from human non - cancer lung - kidney - muscle ( fraction a ) had given 3 tumours in 25 mice , and was considered a potent it had been in the cold room for over carcinogen - containing fraction . 3 years and was then fractionated according to a simplified scheme ( flow sheet 2 )  . of 52 mice at the beginning of the tests , 43 survived 12 months and 26 , 18 months . 
four sarcomas appeared , 3 in fraction g and 1 in c . ( g ) the crude unsaponifiable fraction ( m ) of mixed livers which had been used in experiment ( d ) was fractionated and tested at j , k , l , g , a , c , f , m , i , using in all 110 mice , which lived well ; 92 survived 12 months and 40 , 18 months . 
a large batch of the crude unsaponifiable matter was worked up to stage a ; a part was kept for injection , and another part was acetylated and crystallized by careful seeding . 
the crystalline acetate was hydrolysed and the regenerated cholesterol tested . in the 12th month one sarcoma appeared in the a series , and in the 19th month one sarcoma developed in the cholesterol group . 20 mice were employed in each test . ( i ) cholesterol - rich fraction from cream ( cow 's milk )  . - kennaway ( unpublished communication ) had found that the unsaponifiable part of cow 's milk produced a sarcoma by injection into c3h mice . 
the experimental mice lived well ; after 29 months a mouse of the f series ( flow sheet i ) developed a sarcoma at the site of injection . ( k ) liver from a lymphosarcomatous human subject gave a highly carcinogenic unsaponifiable fraction in some of the earlier experiments ( hieger , 1940 ) , and the tissues of humans with this type of cancer may possibly be rich sources of carcinogen three livers from lymphosarcoma cases were saponified , fractionated into stages a , j , m , l , and injected into 6 , 5 , 11 and 6 mice of crossed c3h x c57 strain , which survived well , but no tumours developed . the 85 per cent cholesterol fraction ( a ) of cancer livers which had given 2 sarcomas in 10 stock mice was stored in the cold room for 2years , then tested on 10 c57 mice . 
one sarcoma appeared in the first series in the 14th month in a c57 female , and one sarcoma of fibrous type in the second in the 22nd month in a stock female ( experiment 7 , table i )  . when over 300 control tests had been carried out on lard alone without the production of a single tumour , a sarcoma arose at the site of injection in a c57 mouse first injected with lard when already 16 months old . 
fatty extract of walker rat tunmour . aptekman , king and lewis ( 1943 ) induced sarcoma in rats by injection of their results were confirmed here by the fatty fraction of walker rat tumours . tests where the tumours were dried by storing in distilled spirit and extracting with benzene . 
a after parallel group of 10 rats were injected subcutaneously with lard alone . two years one rat in each series developed a fibro - sarcoma , which grew with difficulty on transplantation . 
both tumours arose in the subcutaneous tissue at the same level as the injection site , but on the opposite side this effect has been observed several times in experiments where of the body . the injected substance is very fluid , and is probably pressed round the subcutaneous spaces by the movements of the animal 9 . 
10 stock in the 14th month in group b 2 mice developed sarcomas , and pre - neoplastic changes were seen at the site of injection in 4 other mice . thus in group b , 6 of 10 mice had either developed sarcoma or might have done so if they had lived longer . 
the two sarcomatous mice and two of the incipiently sarcomatous mice were from the same box of 5 mice . one cannot say why only group b responded so readily , but ( 1 ) in a fair number of experiments the saponification of tissue has been done in spirit but the products have produced no tumours , showing that spirit is not essential for carcinogenesis by the unsaponifiable product ; ( 2 ) the absorption spectra of the two final products ( cholesterol saponified in spirit and in alcohol ) are closely similar ; and ( 3 ) while the substance was strongly carcinogenic in group b ( stock mice ) , the same preparation was inactive in group a ( c57 )  . consequently it must be supposed that the b group of mice were either ( 1 ) peculiar genetically ; ( 2 ) peculiar congenitally ; ( 3 ) had become infected or ( 4 ) had become contaminated with carcinogen . ( 4 ) is , on the whole , not very probable , because the 1946 paper reported that in tests on 18 subfractions of the unsaponifiable fraction of human tissue , partly from cancerous , partly from non - cancerous 134 i . 
ieger subjects , of the total yield of 8 sarcomas , 7 were produced by fraction a made from 3 different sources and 1 from an m fraction ( flow sheet 1 )  . 
the concentration of 7 / 8ths of the sarcomas in one particular fraction strongly suggests that the fraction itself was responsible and not a chance contamination , for it would be highly improbable that contamination would occur only in the boxes , holding 5 mice each , containing those treated with the a fraction . the data in table mi are the results when a fraction was divided into 3 or more sub - fractions . 
pre - neoplastic changes at the site of injection of lipid . since the detection of only a few tumours could be important in deciding the technique of further fractionation , it was essential not to miss any tumours not visible macroscopically . 
30 non - cancer livers tested separately ( 6 in 30 were active ) tested separately ( 8 in 37 were active ) ratio : sarcoma mice total mice used . 12 / 56 = 21o 5 / 63 = 8o 44 / 120 = 370to0mean21 17 / 101 = 17o% 12 / 456 = 10 ' 440 = 2 30o thus the effect of testing a number of livers ( 67 ) separately was to reduce the sarcoma production by a factor of 9 , i.e. 
hieger ( 2 ) commercial cholesterol in lard gave sarcomas in about 5 per cent of 213 mice ( table ii )  . ( 3 ) the mixture formed when cholesterol is refluxed with koh and distilled spirit gave no tumnours when injected into 10 c57 mice , but in 10 stock mice there arose 2 sarcomas , and in 4 other mice of the same series changes were detected , post - mortem , suggestive of pre - neoplasia , at the site of injection . 
a total of 69 sarcomas has been obtained at the site of injection of lipoid substances in approximately 2000 mice of c57 and mrc strains and commercial mixed stock mice . 
kreyberg. from the institutt for generell og ek8perimentell patologi , universitetet i oslo . received for publication march 9 , 1953 . the clinical problems of breast carcinoma have been under intensive discussion for decades . 
a great deal of detailed information has been accumulated , but still widely different views are entertained as to diagnosis , treatment and theraour present knowledge was amply illustrated during the panel peutic results . discussion on treatment and results in cancer of the breast at the thirtieth annual meeting of the american radium society , chicago ( 1948 ) , and at the twenty - fifth meeting of the northern surgical association , copenhagen ( 1951 ) , to which readers may be referred . a few points seem to be universally acknowledged , as regards treatment . firstly , a careful and extensive surgical intervention will , in a number of cases , be life saving , or life prolonging . 
on the other hand , if the surgeon operates in a field where cancerous cells are present and the operation is incomplete , the surgeon may by his intervention precipitate an outburst of metastases and shorten the it may further be agreed that the development of the special life of the patient . surgical technique since the days of halstead and meyer is comparatively small , and that the advances , as manifested by a higher cure rate , are modest and mostly caused by improvements of surgery in general , for instance the introduction of penicillin and a better postoperative regime , thereby reducing the immediate it was this state of affairs that caused mcwhirter ( 1949 ) operative dangers . to state : " when radical mastectomy is the only method of treatment available and when all cases coming to a large general hospital are taken into account , the five - year survival rate is unlikely to exceed 25 per cent "  . secondly , it seems generally accepted that radiological treatment in a certain , restricted number of cases and under certain conditions , is able to effect a complete destruction of the tumour cells and thereby be life - saving . it further seems generally accepted that radiological treatment in other cases may , for a shorter or longer period , retard the development and the spread of the tumour cells , and that radiological treatment thereby may be life prolonging . kreyberg ( 1938 ) microscopically examined breast carcinomas and axillary metastases which had been submitted to pre - operative irradiation . 
the material came from three different hospitals , using different radiological techniques and different doses . the conclusions were that - : a pre - operative treatment , with the doses used , may 158 l . 
kreyberg in a series of cases damage the tumour cells to a degree , histologically visible , and in rare cases lead to complete disappearance of the tumour cells . this effect is dependent upon the dose , the effect being more pronounced after stronger doses . also the axillary metastases are damaged , but in a considerably lower degree than the primary tumour . but , even after the strongest doses ( with tele - radium ) , a great number of tumours show such small changes that we must conclude that the cells are growing during and in spite of the treatment . these observations have been generally confirmed . 
kaae ( 1952 ) stated that only 15 per cent of all breast carcinomas are really radiosensitive . baclesse ( 1949 ) had greater effects , but he used very heavy doses . 
an observation period of 5 years only is , however , too brief , since one of the radiological effects is fibrosis and scarring , after which cancer cells , retarded in growth , may regain their vitality and proliferative possibilities at a later date . haagensen ( 1949 ) stated " our reliance upon irradiation for the cure of the disease ( breast carcinoma ) has faltered until we have come to the point where we reserve irradiation for cases in which palliation is all that can be hoped for . " an attempt has been made to combine surgical and radiological treatment , in the hope of obtaining better results . 
the absolute or over - all cure rate is the number of patients alive and symptom - free out of the total number of patients received in the hospital and suffering from the disease under investigation . all dead are counted as victims of said disease , regardless of the real cause of death . 
even if this strict attitude is adopted , we meet , however , with factors which influence the statistics . firstly , the general cancer consciousness of the society , which to a certain degree will influence the relative number of early and late cases . secondly , social and racial factors , which may influence the soil of the cancer cells , and thirdly , the relative number of cases with moderate and with high malignancy , as shown by bloom ( 1950 )  . kreyberg ( 1952 ) in a survey of lung cancer in norway attempted to show that the difference in the sex distribution of this form of cancer in norway , as compared to england and wales , may be explained by the difference in the relative number of the different histological types . 
a similar situation may hold it is probable , therefore , that besides a plea good for breast carcinoma as well . for the use of absolute cure rates and tumour stages already in use , also a correction for tumour types and grades should be attempted . nielsen ( 1951 ) gave as reasonable the following figures as the average chances for a breast carcinoma patient in scandinavia : 5 - year survival rate , symptom free ( operable cases ) , 35 - 50 per cent . 5 - year survival rate , symptom free ( absolute ) , 20 - 30 per cent . these figures are valid for a population with a generally fair cancer consciousness and with a rather high standard of the doctors and the hospitals . individual surgeons and special clinics may present better results , but such material is more or less selected . the cause of the depressingly low cure rate in breast carcinoma is two - fold : ( 1 ) the tumour cells have spread beyond surgical control before the operation is performed and even before the diagnosis is made , and / or ( 2 ) the tumour cells are not sufficiently radiosensitive . this state of affairs has naturally led to a quest for other means of improving the therapeutic results , and as one of those , the importance of " early diagnosis " has been universally stressed and accepted . it may be useful therefore to examine the meaning of the designation " early diagnosis "  . 
in the present paper it is intended to examine different definitions of the term " early diagnosis " commonly used in order to ascertain our position today as regards the criteria for the immediate recognition of a breast carcinoma in a stage where a complete cure is possible , if a proper treatment actually at our disposal is used . especially will be examined the foundation of a propoganda promising great hopes of cure if the patient arrives for treatment on the basis of an " early diagnosis "  . when a breast carcinoma develops morbid changes have usually been present in the tissue for a shorter or a longer period . 
even if the essential change is considered to be a somatic mutation in a single cell , this mutation has its local further , the tissue is not clinically cancerous before the proliferation cause . has reached a certain extent . 
from a therapeutic standpoint to - day the breast carcinoma is in its early phase as long as the tumour is localized to a degree that makes a complete cure possible by such a relatively simple local operation as this is the background for the designation " stage i " , and in the mastectomy . absolute sense mastectomy should by definition in such cases result in 100 per 160 l . 
the discrepancy between the number of tumours histologically classified as stage i and the number of cures effected in this group , after a proper local operation , shows the degree of failure in the process of staging . this failure is approximately 20 - 30 per cent . in spite of this serious inaccuracy the histological staging is the method used for grouping of tumours for comparing different therapeutic interventions . the most accurate staging is the retrospective clinical , taking into consideration the final development of the cancerous process in each individual . even this staging is not perfect . it has been mentioned that patients supposed to be stage i eventually are shown to be in stageii or further . 
on the other hand , patients believed to be stagei , though actually in stage ii , may never be recognized as such if radiological treatment cures the patient . this brief survey shows that the decisive determination of the stage of a certain tumour is neither a direct nor an immediate process . 
kreyberg this table shows that even in these groups , where the time lag between diagnosis and commencement of treatment is reduced to the practical minimum , only half of the average patients can count upon a 5 years ' survival symptom free . it seems , therefore , that the definition p2 is of rather limited usefulness because a great number of the tumours are not any longer curable and the definition has not contained the criteria necessary to obtain this goal . 
a limited usefulness of p2 is demonstrated by the fact that some patients , an unknown number , have benefited from the shorter time lag - a question which will be discussed later . if we analyse the usual symptoms , some of them ( a feeling of heaviness , pains , stinging sensation and similar ) are rather vague and strictly subjective and little fitted for attempts at earlier detection . 
but among the symptoms analysed , a lump in the breast is the first in at least three - fourths of all cases , and this symptom is more material , more objective and more fitted for diagnostic research . 
here a regular and systematic palpation may facilitate the discovery of comparatively small nodules , but there evidently is a certain lower size limit . kaae ( 1948 ) voiced the traditional opinion when he stated that : another attempt at a useful definition may accordingly be : a diagnosis of a very small tumour ( p3 ) , in the hope that all such tumours actually are curable . " it is generally recognized that the size of the tumour is a very important factor in the prognosis , and that the latter is much more favourable for the small tumours than for the large . " if we , however , examine the pertinent literature , we shall discover that the students of this problem are not at all unanimous . 
the fate of the patients was followed and the long range survey , ten to twenty year 's observation , showed that nearly two - thirds of the patients had metastases when arriving for treatment . 
even the very smallest carcinomas , those the size of a pea or a bean , had a fatal outcome in four out of ten cases . these facts show that our attempt to define " early diagnosis " as a diagnosis of a very small tumour ( p3 ) , actually a tumour as small as practically diagnosable , also fails miserably . taking into consideration the three commonly used or accepted definitions of " early diagnosis " , pi fails , because the criteria are not immediately available , and p2 and p3 fail , because the criteria do not enable a patient to recognize a tumour still in a curable stage . 
nor is any other definition known , which makes such a recognition possible to - day . what p2 and p3 give are indications for obtaining the earliest possible diagnosis with our present diagnostic means . 
an examination of the actual degree of earliness shows that only half of the tumours occurring in a population can , under the best possible conditions , be diagnosed early enough to be cured with our present therapeutic means . 
the high percentage of cures is the result of a very strict selection of cases . first all cases proved to belong to stage ii , or further , are excluded . this would leave a curability of approximately 75 per cent for the remaining . next , larger tumours , and finally especially malignant - looking tumours , are excluded . 
a further improvement in the statistics may be obtained by a still greater efficiency in the process of selection , not necessarily being an expression of increased chances for the patient at large to survive . it is not correct and not fair to publish such statistics in a manner that makes 164 l . 
kreyberg the public believe that if the women examine themselves regularly and carefully , and pay a visit to a competent doctor at the first suspicion of a symptom from the breast , their chances of a complete cure is in the vicinity of 90 per cent . 
kaae ( 1948 ) arrived at the same standpoint , and wrote : " it is indicated by these investigations that a 5 - year symptom - free survival rate of about 40 per cent is obtainable in denmark to - day , and that these results may be improved from 40 to 50 per cent , if all patients see a doctor as soon as they notice the first symptom , and if the doctor makes the correct diagnosis and institutes adequate treatment without delay "  . the present study seems to show that a diagnosis as early as possible is of great importance to a certain , yet unknown , number of individual breast carcinoma patients . 
as we do not beforehand know who will benefit and who will not , a general plea for " early diagnosis " is fully substantiated , as every individual salvaged is important . 
we must , however , always have in mind that the benefit is statistically moderate , and we ought to be modest in our claims as to the possibility of materially altering the situation for the breast carcinoma patients by this approach to the problem . it has finally to be added that the present conclusion is based upon the use of the word " early " as an expression of curability seen on the background of our present diagnostic and therapeutic means . 
the earliness is , term is not used in the sense of a more or less absolute time unit . actually , here synonymous with curability to - day , and this again , in most cases , means a carcinoma in stage i . if we examine the means to diagnose a carcinoma still in stage i , we will discover that such a diagnosis can with a reasonable certainty be made only after a retrospective clinical survey , lasting some 15 to 20 years . the analysis further shows that we have no criteria enabling an immediate " eary diagnosis " , in the sense required . 
1949. although convenient and entirely suitable for the purposes for which they are employed , the u8ual methods of maintaining and utilizing transplantable tumours are not well adapted to special needs in experimental oncology , particularly when quantitative refinements and the desirability of repeating experiments with aliquot portions of the same tumour suspension are important considerations . the basis of any method which might meet such requirements must necessarily be one in which a number of separate and sin - iilar portions of a tumour can be preserved with some assurance that different portions tested at different - times will exhibit sirnilar activities . this means that the tumour tissue must be reduced to a fine state of division and homogeneous suspension and subjected to a method of preservation whereby its capacity to induce tumours remains constant for a long time . it is well known that growth may be obtained on transplantation of frozen and thawed tu ' mour tissue . although breedis and furth ( 1938 ) demonstrated the feasibility of preserving neoplastic cells in the frozen state for periods up to 400 days , this useful method does not seem to have been adopted to the extent that might have been expected . 
most of the observations have been made using the c3h sarcoma referred to by gye , begg , mann and craigie ( 1949 )  . pr " ration of tumour mmpennow . - the tumours were reduced to the necessary - state of subdivision by means of the pressure mincer described by craigie ( 1949 ) and the mince dispersed immediately in diluting fluid . 
the diluting fluids were freshly prepared from reboiled sterile distilled water and concentrated preparations of the required solutes . in experiments in which different diluting fluids were compared , a low primary dilution was first made in fluid of suitable composition and from this the secondary dilutions in the other fluids were prepared . 
were given subcutaneously in the approexcept in limited experiments , four sites in the anterior priate strain of mice . abdominal wall were used , these being approximately the centres of the upper and lower right and left quadrants . the " rtival of tumour 8uspen8iow in sau 8olulion& when a solution of sodium chloride is frozen at a temperature above 21t . ice crystalhzes out and the salt is concentrated as a strong solution ( 30 per cent ) between the cryistals . if a cer suspension in 34 volumes of 0 - 85 per cent nacl 20 ' c . 
in the strong salt solutions , in others the material was held in the frozen state for several hours at selected temperatures above and below that of the eutectic of nacl ; the results showed that although complete inactivation might require several hours , the initial rate of inactivation referable to electrolyte concentration was undesirably high . survival of tumour 8u8pen8ion8 in dextro8e solutiom . in view of the difficulties that might be expected to arise in attempts to obtain adequate preservation of activity in tumour suspensions frozen in inorganic salt solutions , the possibihty of substituting a suitable non - electrolyte was considered . of water - soluble organic materials , accordingly it was planned to test a variet but dextrose , the first of these selected for test , was found to have such a favourabl . 
effect that no attempt has yet been made to find substances more suitable for the purpose . because of the varied nature of the comparative tests which have been carried out and the introduction of a number of improvements in technique , it is not possible to present a synopsis of the results on a quantitative basis . table i provides a brief summary which , at best , merely shows that there is no contraindication to the use of - dextrose solution as a suspending fluid . 
16 - 25 m / 150cysteinehcim / 15onaohm / l5ona2hpoi , s = 0 - 85pereentn&o ; r four compamtive injections were msule in each mouse and the figure given in the cohnnn headed mouse group " ] indicates the arrangement of injections , eg . 
1 : 300 n&c1 the tumour mince was first thoroughly mixed with an equal volume of 0 - 85 per cent nacl and the mi iture was diluted i in 15 in the stated diluents . 
the first test was made after the suspensions had been kept frozen for 4 days . the lag periods observed in this test are not comparable w ' ith those in the later tests because of changes in technique of thawing , diluting and injecting , and also because of the use of a eysteine - phosphate.saline mixture in the later tests . however , it would appear legitimate to compare the activity of the material frozen for 253 days in the mixture of dextrose and 40 per cent glycerol withthe average activity of fresh c3h sarcoma suspension in ringer . 
further investigation is desirable not onlv with a view to improvements that might facifitate studies in which the tise of preserved tumour material is preferable , but also with the object of dete - riiiining the mecha i ms of surv - ival of activity . 
the varietv of pkvsical and physico - chemical factors which may he involved and the potential coniplexitv of their interplav need not be detailed , but some of the points which require investigation from the practical point of view mav be mentioned . thev are as follows : 1 . 
the development of a suitable fluid for dilution of thawed material . tumour ' suspensions which have been frozen may show a definite drop in activitv in 15 to 30 minutes after thawing . 
on the degree to which the material is diluted . it will have been noted from tables 11 and iii that cysteine phosphate buffer mixtures have been used as diluting fluids . 
the experimental evidence for the use of dilutina fluid of this composition is contradictorv and suggests a different approach to this problem . another matter which merits further investigation is the effect of dextrose on the nuclei of tumour c , - - ils as viewed with the phase contrast microscope . 
after preservation in the frozen state , sarcoma and c#rcinoma suspensions in dextrose solution show a greater and more consistent retention of activity than suspensions prepared with saline and ringer.. 
malowan ( 1932 ) - also found blood changes of the same low order , though becher and herrmann ( 1932 ) stated that they were unable to find any significant change that could be attributed to the presence of the tumour . all the above workers used danielson 's modification of folin 's well - known colorimetric method for blood amino acids . 
2. these observations show that the growth of the transplantable carcinoma ' m 2146 is accompanied by an elevation in the blood ac - amino nitrogen . while the mean value in normal mice was 4 76 mg . 
the corresponding regression equation between these variables is : oc - amino nitrogen values = 0 - 1213 tumour percentage size + 5 - 63 . these changes in the level of the blood ac - amino nitrogen probably account for the increase in the blood non - protein nitrogen in tumour - bearing animals found by other authors ( greenstein , 1947 )  . blood ac - amino nitrogen in mice with regressing tumours . in about 10 per cent of the mice used in these experiments the tumour , after having grown and reached a definite size , regressed completely . it seemed of interest to estimate the blood amino acid concentrations in these animals . 
the animals consumed this food freely for the first two days , but seemed to lose appetite during the remainder of the experimental five - day period . the loss of weight , which had become severe by the fifth day , together with the blood ac - amino nitrogen values , are shown in table iv . with the introduction of the deficient diet there was a marked loss of weight in both groups of mice ; the tumours , however , continued to increase in size even at the expense of the host , which was clearly in negative nitrogen balance . 
per cent throughout most of the experiment seems to show that this represents the basal level for this group of substances , below which further in the tumour - bearing group , on the other hand , the concentrafall is resisted . tion of the ac - amino nitrogen fell rapidly to between 4 and 5 mg . 
the similarity of the fall to that found for the control group would seem to show that whatever metabolic change was responsible for the characteristically elevated blood oc - amino nitrogen level was independent of the state of alimentation , 100 m . 
there is little evidence that the free ac - amino acids are increased in tumorous animals , but observations on rats with a transplantable hepatoma have shown that the second fraction may on average be raised seven or eight fold ( winzler and burk , 1944 )  . 
the elevation continues almost unabated when the animals are placed on a diet wholly deficient in protein . it seems , therefore , that the increase in oc - amino nitrogen must be attributable to one or other of the following factors : a local increase in the production of amino acids or of polypeptides by the tumour itself , either through the degeneration of its cells or the hydrolysis of normal body proteins brought to it by the circulation ; or to some hepatic dysfunction that is present in tumour - bearing animals which interferes with the normal disposal of these substances , and thus permits them to accumulate in the blood . this latter possibility will be considered first . fujiwara ( 1929 ) , weil ( 1935 ) , greenstein , jenrette , mider and white ( 1941 ) , and el mehairy ( 1949 ) found little inhibition of liver arginase in tumorous animals . greenstein ( 1947 ) also noted no dimunition in cystine , desulphurase activity in the same organ . arginase and cystine desulphurase are two of the main liver enzymes concerned with the intermediary metabolism of amino acids , and the study of their behaviour provides valuable information upon disturbances in the hepatic enzyme pattern generally . robertson and kahler ( 1942 ) and lan ( 1944 ) have also failed to observe any decrease in the enzymic activity of livers in animals bearing tumours . 
tumours of less than 5 per cent of the total body weight were not accompanied by any significant change in the oc - amino nitrogen concentration in the blood . the tumour tissue itself is believed to be the source of extra a - amino nitrogen in the blood . i wish to record my indebtedness to professor g . 
 lung tissue is unsuitable for direct injection of carcinogens , consequently pulmonary tumours in laboratory animals have hitherto been induced by applying the carcinogen at some remote site , by injecting it subcutaneously , intratracheally , intravascularly , intraperitoneally , or by including it in the diet . 
 recently the author ( horning , 1947 ) reported the induction of pulmonary tumours after relatively short periods of treatment by the direct application of carcinogens to adult lung tissue growing as subcutaneous homologous grafts in host animals . 
 the method of tumour induction consists in isolating small strips of lung from 6 - 12 weeks strain a mice , impregnating the grafts with crystals of a carcinogen ( 2 - acetylaminofluorene , 2 - aminofluorene , or 20 - methylcholanthrene ) prior to im planting them subcutaneously into host mice of similar age and strain in a manner which has been described elswhere ( horning , 1947 )  . 
small palpable tumours were obtained at intervals ranging from 6 - 12 weeks following grafting , but in order to examine the differences between the responses to individual carcinogens , grafts were fixed before tumours developed at intervals ranging from 1 - 5 weeks after implantation . 
 lung fragments from 6 weeks old strain a mice were grafted , in some instances without the carcinogen , into host mice of similar age , and also into mice of 15 months age which were selected from stock mice of undetermined ancestry . 
 this was done to find out if the survival of homologous grafts was dependent on employing a closely inbred strain , or whether it might be influenced by the age of the host . 
 in another series of experiments a number of lung grafts were treated with 20 - methylcholanthrene , half being implanted into the superficial fascia , and the remainder placed as usual between the skin and the abdominal wall . 
the host mice were again of the same age and strain , and it was thought that some infor mation might be obtained as to whether rapid vascularization played any role in successful survival of the grafts . 
 lung tissue was obtained from 30 strong a male mice aged 6 weeks , and implanted subcutaneously into host mice of the same strain and age , each indi vidual receiving 2 grafts on each side of its belly ( table i )  . 
when the same number of grafts from females were implanted into strong a male mice over 8 months of age , only 14 grafts had survived after 8 weeks and 4 of these contained areas of necrosis ( table i )  . 
grafting the same number of lung implants from strain a mice 6 weeks old into stock mice of indeterminate ancestry , all of which were over io months old , resulted in 58 becoming totally absorbed after the same interval of 8 weeks ' implantation ( table i )  . 
either the nuclei become pycnotic , or as in most grafts they lose their differential stain ing and the cytoplasm becomes homogenous , to be followed in later stages by fragmentation and dispersal . 
the nuclei of the collapsed lung alveoli undergo chromatolysis far more rapidly than those of the adjacent bronchiole epitheliu histological examination of these grafts suggests that their failure to survive in host tissues may be due to a partial failure of vascularization which induces necrosis . 
these results obtained with adult lung grafts indicate that successful survival and growth depends on age of both the donor and host animals , together with employment of a closely inbred strain in which homologous grafting is much better tolerated than in mixed strains . 
 in order to obtain a foreign body reaction fragments of lung from 6 - 7 weeks old donor strong a mice were treated with crystals of commercial cholesterol and subcutaneously implanted in 8 - weeks - old host mice ( table i )  . 
 in every instance in this series of experiments lung tissue was obtained from strong a mice of either sex , 7 - 8 weeks old , and impregnated with the carcinogen and implanted subcutaneously into host mice of the same strain and age ( table i )  . 
 the remaining 13 were no longer translucent , and it was found that eight of these opaque grafts had been accidentally transplanted into the superficial fascia instead of between the skin and the abdominal wall . 
 the histological characteristics of pulmonary tumours induced from sub cutaneous lung grafts treated with carcinogens differ in some respects from those of tumours arising in sitit in the intact lung of rodents under the influence of in pieces of isolated lung growing as . 
 a typical carcinoma of the lung in a graft impregnated with 20 - methylcholan threne fixed 11 weeks following subcutaneous implantation in a strong a host mouse is illustrated in fig . 
the lumen of the bronchiole is occluded by cellular debris , and the epithelium in some regions has become stratified , but in the malignant area the bronchiolar epithelium is ciliated._ the cells comprising this neoplastic focus possess all the histological characteristics of malignant cells . 
 the histological appearance of these carcinomas varies , however , according to the age of the primary gra those recovered from mice 9 - 12 weeks old consist of acini of cells with large oval nuclei . 
 all primary tumours induced by the several carcinogens were obviously bronchogenic carcinomas , with the exception of a squamous - celled growth in duced by 2aaf after 16 weeks ' implantation . 
one was a polymorphic and the other a spindle - celled sarcoma~ as both these tumours were too far advanced in their growth it was impossible to ascertain whether they were derived from the tissues of the implant or from the host , so they were discarded . 
in some which carried six or more graft1 it was frequently noticed that after 8 - 10 weeks the palpable grafts varied considerably in size , and that this variation often occurred irrespective of the particular carcinogen employed . 
those implants which failed to develop into tumours , and were hardly palpable in the living host , were found to contain large inflam matory foci or areas of foreign body reaction . 
in every instance the inflamed grafts were obtained from the same donor mouse grown in the same host and treated with the same carcinogen for a similar period of time as those which developed into tumours . 
 in the majority of grafts ( table i ) necrosis and fibrosis are absent , although these changes are so often associated with inflammation of the intact lung in situ . 
 bronchioles when present in these grafts tend to be obscured , since the lumen is filled with cellular exudate consisting mainly of lymphocytes , plasma cells , and a few macrophages or polymorphs . 
multinucleated giant cells frequently seen in tissues reacting to foreign bodies were absent in grafts treated with car cinogen , but were found in several implants impregnated with commercial choles terol . 
every lung graft was fixed in alcoholic bouin and stained by ehrlich 's haematoxylin and eos f1 . - a typical bronchogenic carcinoma , induced from a graft of adult normal lung impreg nated with crystals of 20 - methylcholanthrene , fixed 11 weeks following subcutaneous implan tation in a host ( strain a ) mouse . 
this is of special significance , as it indicates that the carcinogen has a selective action only for the bronchiolar epitheliu the adjoining alveolar cells remain quiescent to the local presence of the carcinogen . 
the lumen of the bronchiole is occluded with a cellular exudate , and in some regions the epithelium has became stratified , but in area of malignant focus the bronchiolar epithelium is ciliated . 
 since the induction of carcinoma of the prostate in mice , arising from fragments of adult glandular epithelium combined with the carcinogen growing as homologous subcutaneous grafts in host mice , was first reported ( horning , 1946 ) , this method of tumour induction has been successfully extended by other investigators to other tissues and organs . 
more recently hughes ( 1949 a , b ) , using the same technique , has succeeded in inducing transplant able carcinomas from fragments of adult bladder and uterine epithelium combined with methylcholanthrene , as well as tumours of adrenal cortex . 
 one of the several advantages arising from homologous subcutaneous grafting in the presence of a carcinogen is that the tumours growing under the skin are palpable , and can readily be obtained at the required stage of growth . 
the time taken for tumours to appear is shorter most likely because the carcinogen is more concentrated , and lies in close proximity to the bronchiolar epithelium of the gra with indirect methods of induction such as painting the carcinogen of the skin , by injecting it or including it in the diet , there may be changes in organs and tissues throughout the body , and not necessarily only in the region where a tumour arises . 
 thus dunlap and warren ( 1942 ) have reported that if swiss mice are injected subcutaneously with carcinogenic hydrocarbons , the incidence of primary pulmo nary tumours is higher in mice which have also developed tumours at the site of inoculation . 
 it must be admitted , however , that these two methods of induction differ fundamentally , because the changes which occur in the intact lung in situ following treatment at some remote site with a carcinogen are not necessarily the same as those which take place in homologous subcutaneous grafts of isolated , collapsed lung . 
these differences were discussed in a recent paper by orr ( 1947 ) , in which he rightly pointed out that it is difficult to compare results obtained by the two methods of induction . 
 recent eijeriments have shown conclusively that the survival of lung grafts either with or without the carcinogen is dependent upon the age and strain of the donor mouse , together with the age and strain of the host . 
examination of table i shows , however , that donor lung implants impregnated with a carcinogen survive more readily and in greater numbers in older hosts than would be the case if the grafts did not contain any carcinogen . 
it is of course possible that since the lung carcinomas arise from bronchiolar epithelium , some grafts may at the outset contain insufficient epithelium of this region to give a response . 
a separate series of experiments in progress show that pulmonary tumours are obtained more readily and in greater numbers from fragments of lung in which particular care has been taken to isolate portions of a bronchus , discarding the more peripheral parts of the organ . 
otherwise it is difficult to understand why prostatic epithelium should flourish as a graft despite the antagonism between graft and host tissues , and yet lung fragments implanted under the same conditions do not always survive so readily . 
pre liminary experiments reported elswhere ( horning , 1949 ) suggest that tissues which are normally under hormonal influence are much better tolerated as grafts in host mice of the same sex andstrain than tissues which are to a greater extent independent of hormone action . 
a higher incidence was not obtained in males , as seems to be the case in human lung cancer according to clemmensen and busk ( 1947 ) , and in strain a and strain c mice treated with urethane in the experiments of larson and heston ( 1945 )  . 
there is a slight difference between the potency of the three carcinogens used in the present experiments in that a greater number of tumours appeared in grafts treated with 20 - methylcholanthrene . 
 with regard to the histogenesis of the present lung tumours the method of grafting allows examination of the neoplastic changes in graded stages , leaving no doubt that the tumours arise from bronchiolar epitheliu it is curious that no response to the carcinogens is obtained from the walls of the lung alveoli . 
 an alveolar epithelium exists why should it remain entirely quiescent , whilst the closely adjacent epithelium of the bronchioles proliferates in so striking and so specific a manner ? controversy still exists concerning the nature of the lining of the lung alveoli . 
ross ( 1939 ) maintains that although an epithelial lining to the alveoli is not visible in ordinary histological preparations , it becomes appa rent in response to certain abnormal stimuli . 
grady and stewart ( 1940 ) not only affirmed the existence of an alveolar epithelium , but regarded it .as the source of lung tumours in mice treated with methylcholanthrene . 
 thus while they agreed that human tumours are bronchogenic in origin , they were convinced that mouse lung tumours arose from the alveolar epitheliu more recently herbut ( 1946 ) has reviewed the ev ' idence concerning the origin of human lung tumours , and concludes that all " alveolar cell tumours " come from the basal cells of the bronchi and bronchioles ; and that there is no justification for assuming that they arise from septal cells . 
it is unlikely that any fundamental difference exists between the rodent and human lung , and since there is such clear indication of the origin of malignant foci in early grafts combined with a carcinogen , it would appear that the case for bronchogenic origin of all lung carcinomas is strengthened . 
in the presence of chronic inflammation a proliferation of the epithelium in the respiratory bronchioles may extend to form a lining within the alveolar ducts and alveoli in much the same manner as bronchial epithelium will grow into an old abscess cavity . 
 the relationship of pulmonary cancer to inflammatory foci has been studied recently by grady and stewart ( 1940 ) , de eds and cox ( 1941 ) , nettleship , henshaw and meyer ( 1943 ) , orr ( 194 7 ) , orr and bielschowsky ( 194 7 ) , and selbie and thackray ( 1948 )  . 
the effects of urethane on the mouse lung in situ indicate according to nettleship , henshaw and meyer ( 1943 ) and orr ( 1947 ) that inflam mation and adenomas arise together . 
grady and stewart ( 1940 ) and selbie and thackray ( 1948 ) disagree , and the last authors believe that in orr 's series of 433 animals which were examined after they had died from natural causes , there was a susceptibility to terminal inflammatory involvement . 
here also the evidence obtained from grafting clearly supports the contention that there is no relationship between inflammation and lung neoplasia , since the grafts which failed to produce tumours contained large areas of inflammation and those in which tumours developed rapidly were comparatively free . 
 summary , bronchogenic carcinomas have been induced from homologous subcutaneous grafts of lung tissues growing in host mice , after impregnation with either 20methylcholanthrene , 2 - acetylaminofluorene , or 2 - aminofluorene . 
 the period of tumour induction in grafts of homologous lung is considerably reduced when compared with lung tumours which develop in situ , in rodents following treatment with the carcinogen at some remote site on the body . 
 the susceptibility to tumour formation in subcutaneous lung grafts treated with the carcinogen is found to be dependent upon the age and strain of the donor as well as that of the host mouse . 
additional experimental evidence supports the view that the pulmonary alveoli are not lined by a continuous epitheliu factors influencing the survival of lung grafts without using a carcinogen were also investigated ; these showed that the successful survival of subcutaneous grafts is dependent upon the age of both the donor and host mice , together 244 e . 
 this investigation has been supported by grants to the royal cancer hospital from the british empire cancer campaign , the jane coffin childs fund for medical research , the anna fuller fund , and the division of research grants of the u.s. 
cohen. from the experimental oncology laboratory , radiation therapy department , johannesburg general ho8pital . received for publication february 11 , 1954 . there are many reported examples of animals having been rendered immune or resistant , by various procedures , to subsequent inoculations of a tumour to which they are normally susceptible . 
with an adequately inbred strain eke the c3h mouse , however , and using homologous mammary tumour which has not lost its genetic specificity by repeated serial transplantation , absolute resistance to further implants of the same tumour cannot be evoked . it was previously shown that the radiosensitivity of a homologously - transmitted tumour is a function of the state of resistance of the host . 
when the tumours had reached the standard size of about i cin the largest diameter ( overall average volume 250 481 mm.3 ) , thev were irradiated in situ with our standardised techni.qu ' e as previously reported in detail . all mice were individually numbered and examined at regular intervals for at least 3 months after treatment . with the doses used in this series , the tumoiir has , within this observation period , either disappeared completely or bas resumed active growth , ulcerating the skin and killing the mouse by exsanguination or infection . in order to detect any acquired increase in radiosensitivity , tumours arising from each attenuation - dosage group were treated at three dose levels : 3500 , 4200 and 5000 r , making a total of six categories tested . 
1 - 27 ( 0 - 07 * )  . since this ratio exceeds unit the ld , for the attenuated homoplasts is found to be 4500 ( 200 * ) r , compared with 5700 r previously determined in the controls , and the coefficient of variation is 26 per cent compared to 9 per cent in the controls . 
the relative radiosensitivity of attenuated tumours with reference to the controls , that is the ratio of the ld50 's is four times its standard error , the result is highly significant ( p < 0 - 0001 ) , indicating a definite acquired radiosensitivity of the tumour arising from an attenuated implant . as has been previously shown , a changed radiosensitivity generally reflects an underlying change in host - resistance to the tumour . 
it would appear , therefore . , that the attenuation procedure , while not producing any absolute immunity to further implants of the same tumour , nevertheless induces within the host , albeit the strain of origin of the tumour , a subliminal resistant state . 
of the 22 " recipients " ( 2 to each donor ) , 1 1 were similarly treated in situ with 4200 r in order to detect persistent acquired radiosensitivity in the tumour transplants , and the remaining ii were treated with 7500 r in8ituto exclude the possibihty of an acquired radioresistance . 
the added disadvantage of bilateral treatments , even when the immediate mortahty could be reduced , was the possibility that the increased body dose would lower the expected percentage of cures , as previously demonstrated ( cohen and cohen , 1953b )  . 
the results of ' treatment of the attenuated homoplasts in the four experimental categories are shown in table ii , and the proportion of cures in each group plotted in fig . 
1 it can be seen that the proportion of cures to be expecied at this dosage with unattenuated homoplasts ( line a ) is exceedingly small , while in animals bearing attenuated implants ( line g ) it is 40 per cent , from which this result . 
the attenuation procedure , therefore , seems to induce a degree of resistance , presumably a similar antigenic difference between host and tumotir , at least as great as that engendered by the tumour growing in f , ilybrids harbouring the milk factor . the following facts conceming the nature of this phenomenon have been elucidated : ( 1 ) while not excluding the possibihty that the tumour cells have been inherently changed by this procedure , it is obvious that any such change is not , in itself " sufficient to affect the radiosensitivity of the transplanted attenuated conversely , there is no evidence of " takes " in the environment of a new host . acqiiired radioresistance in the tumour as a result of previous irradiation , in conformity with montgomery and warren 's findings ( 1953 )  . ( 2 ) it is unlikely that any local change in the tumour bed contributes to the changed radiosensitivity since no cures were obtained when recurrences followina the local excision at the original site were treated . it can probably be assumed , too , that damage to the tumour bed by the rsurgical excision was sufficient to abrogate the effect of systemic resistance . ( 3 ) since the increased radiosensitivity persists even where the tumour has 318 a . 
cohen been transplanted to another site in the original donor , it must be concluded that the effect is due to a systemic , generalised resistance mecbanism . the phenomenon of induced resistance to experimentalfy transmitted . 
cancer has been extensively investigated . in the past , results in this field were often contradictory and confusing ( woglom , 1929 ) , due to the use of heterogeneous strains of animals and gentically alien tumours . 
the long transplantation history of these and other commonly used tumours , maintained solely by serial transmission , is surveyed by dunham and it is generally realised that such procedures may perrnit antistewart ( 1953 )  . genic diversification or mutation in the tumour , which , in effect , results in a relatively unstable host - tumour relationship . consequently , many of these findings are largely invalidated in so far as their applicability to human cancer therapy is concemed . it would appear that only when a supply of spontaneous tumours is constantly availdble within a given strain , and is routinely transplanted through no more than a few subpassages to experimental animals of the same strain , can the hosttuniour relationship be considered adequately stabilised . 
where such stringent conditions prevail , absolute immunity to a tumour cannot be evoked ( bittner , 1936 ; barrett , 1940 ; lewis , 1940 ; fardon and prince , 1953 ; foley , 1953 )  . 
a recent review by hauschka ( 1952 ) contains an extensive analysis of the immunogenetic complexities of host - tumour relationships used in experimental cancer reseal - ch . with respect to the cm mammary carcinoma , the authors have shown that , even where some degree of immunogenetic difference existed between the tumour and the host , as in the case of f , hybrids bearing the parent strain tumour , no overt - immunity could be elicited by curing the comparatively radiosensitive tumour in8itu ( coben and coben , 1954 ) , or by previouslv inoculating the animals with radiation - attenuated fragments ( unpubhshed data )  . when one correlates these facts with the findings of the foregoing experiment , it become 's evident that resistance to tumour is by no means an " all - or - none " pbenomenon . it seems likely that partial or subliminal states of resistance can be induced in the stable host - tumour relationship which , while not obviously detectable by conventional methods , nevertheless yield significant results in the form of a perceptible increase in radiosensivity . in this connection , it is significant that gorer ( 1947 ) demonstrated high titres of circulating anti - tumour iso - antibodies in mice dying of foreign strain tumour transplants , which grew progressively in spite of antigenic differences with the hosts . 
when the previously attenuated homoplasts were transplanted from the original hosts to new hosts , however , the curative dose reverted to that of unattenuated tumour . it is considered probable that the inoculation of a viable tumour fragment , attenuated by sublethal doses of radiation prior to implantation , induces a state of subliminal resistance in the host which enhances the radiosensitivity of the resultant tumour . facilities for the maintenance of our experimental animals were generously provided at the south african institute for medical research by j . 
hewitt. from the john burford carlill laboratories , westminster hospital , london . received for publication may 26 , 1953 . from the fact that certain mouse tumours could be transplanted using freezedried tumour tissue , gye , begg , mann and craigie ( 1949 ) concluded that they had evidence of virus transmission of their tumours . subsequently , it was shown ( passey , dmochowski , lasnitzki and milard , 1950 ) that a small proportion of the cells in these tumours were able to withstand freeze - drying as indicated by the proliferation in vitro of tumour tissue so treated . these findings focused attention on the quantitative aspects of tumour transplantation , and various observations were made which suggested that the malignant cell population in sarcomacraigie , lind , hayward and begg , ( 1951 ) tous ascitic fluids is heterogeneous . reported that a small proportion of the sarcoma cells in certain ascites tumours could be distinguished from the modal cells by their peculiar appearance under phase - contrast microscopy , and by their relative resistance to freezing and to the inimical effects of exposure to isotonic glucose . lasnitzki ( 1952 ) showed that a high proportion of the cells of sarcoma 37 ( hereafter referred to as " s37 " ) ascitic fluid undergo morphological transformation in tissue - culture and do not subsequently divide ; she found that this change was accompanied by a reduction in the power of the cells to give rise to a tumour on transplantation , and considered her observations to be evidence of bimorphism of the s37 cells . histological studies of the fate of implants of tumour tissue have not given conclusive evidence that the cells of the new tumour are direct descendants of the cells in the implant . 
 ( 1949 ) stated that the appearance of implants which had been frozen previous to inoculation , although they subsequently would give rise to tumours , " did not suggest survival of any of the implanted tissue . " zahl and drasher ( 1947 ) drew similar conclusions from their observations of the fate of implants of sarcoma 180 in mice . these authors state that there is no increase in the size of the implant and that it undergoes immediate cytological degeneration . several previous workers have studied the variation of tumour incidence with the number of cells inoculated . 
de gaetani and blothner ( 1936 ) found that over 100 , 000 cells were generally required for the successful transplantation of mouse carcinoma and sarcoma . furth and kahn ( 1937 ) , working with an inbred strain of mouse and a spontaneous leukaemia derived from that strain succeeded in transplanting leukaemia to about 5 per cent of their mice by the intravenous inoculation of a single leukamic cellw kahn and furth ( 1938 ) , using the trypan 368 h . 
hewitt a reaction usually regarded as being incompatible with cell viability ( schrek , 1936b ; pappenheimer , 1917 )  . counts of suspensions prepared from solid tumours were tberefore made after mixing equal volumes of the suspension and 0 5 per cent trypan blue ( b.d.h. , biologically tested ) in m / 15 sorensen buffer at ph 7 - 2 . no ascitic cell suspension has been found to contain more than 3 per cent of stained cells , and counts of these suspensions were made in the absence of trypan blue . trypan blue was preferred to eosin for the differentiation of non - viable cells because counts were made in a fuchsit gave more definite staining at non - toxic levels . rosenthal haemocytometer using phase - contrast microscopy . the absence of any reliable morphological criterion by which to identity a viable tumour cell makes it impossible to signify with certainty whether a given cell is a malignant cell or a normal cell contributed by the cellular reaction of the host . it has been found convenient to make an arbitrary distinction between normal tissue cells and sarcoma cells in fresh single - cell preparations of the tumours used in this study , on the basis of cell diameter . it was noted that 90 per cent of the nucleated single cells in sedimented preparations of minces of normal mouse lymph gland , thymus and spleen , and 70 per cent of the cells in saline washings of normal mouse peritoneum had diameters of 9 , t or less . 
on the other hand , a relatively small proportion ( 10 - 20 per cent ) of the cells in many single cell preparations of the solid sarcomas or in some s37 ascitic fluids , had diameters of less than 9 , u . 
the density of viable cells in a suspension has therefore been taken as equivalent to the density of cells having a diameter of over 9 , t and failing to stain with after considerable experience had been gained of the measurement trypan blue . of the cells in fresh preparations , actual measurement of the cells was abandoned and the larger cells were selectively counted by estimation of their size . frequency distribution curves of the diameters of the single cells of sarcoma preparations showed a modal diameter in the region 14 - 16 , t . 
a smaller , second peak was sometimes seen at about 7 , u , and this was considered to represent the mode of the inflammnatory cell population in the suspension . the effect of elimination from the cell count of all cells of diameter less than 9 , u was to exclude from the count the great majority of the non - tumour cells . 
on the other hand , a count of tumour cells made using this criterion might represent only 80 per cent , but no less , of the actual number of tumour cells present . titration of sarcoma cell suspensions . if necessary , the counted s37 cell suspensions were diluted to contain about 20 , 000 tumour cells in 0q1 ln . 
 ( the inoculum volume )  . of this suspension , five 3 - fold dilutions were made in the gelatine - tyrode medium , giving a series of six suspensions with cell densities varying from about 20 , 000 / 0 1 ml . 
to facilitate accurate placing of the inocula , all inoculations were given under ether anaesthesia . throughout all manipulations from the time of setting up the second phase of the sedimentation procedure until inoculation , the suspensions were kept at 2 - 5 c . full aseptic technique was employed throughout and special precautions were taken to keep the suspended celis in homogeneous distribution . recording of tumour incidence and calculation of end - points . inoculated mice were examined for palpable tumours at 2 - 3 day intervals from the 6th till the 30th day after inoculation in the case of s37 and from the 6th to the 40th day after inoculation in the case of the c3h sarcoma . it was found that , with very few exceptions , the smallest detectable mass in an inoculated site would become a definite tumour within a few days of its presentation . regression occurred in a fairly high proportion of the s37 tumours derived from the smaller inocula , but was unusual except in tumours which had attained moderate size . 
the proportion of sites in which a palpable tumour formed was recorded for each of the 6 different tumour cell in an ideal titration , all sites inoculated with the highest dose doses inoculated . of cells gave tumours and all those inoculated with the lowest dose failed to give tumours . 
from these data , the number of tumour cells which would have given tumours in 50 per cent of the inoculated sites ( hereafter referred to as " td50 " ) was calculated by the method of reed and muench ( 1938 )  . 
variation in td50 values obtained in ( i ) separate titrations of different s37 cell suspensions and ( ii ) parallel titrations qf the same suspension . in 16 titrations of different s37 cell suspensions performed in the manner described and using 4 - 6 mice per group , the td50 values ranged from 603 to 3162 cells , with a mean of 1641 and a coefficient of variation of 51 per cent . 
the ratio of the highest to the lowest value obtained in this series was 5 - 2 . it has not been possible to correlate this variability with any one factor known to vary from one experiment to another . suspensions prepared from tumours during their early growth phase and those prepared from older tumours gave results which were not consistently different . it is clear , however , that the variability in results from one experiment to another is contributed to both by unspecified differences between the suspensions and by random differences in the batches of mice used for the titrations . in order to assess the order of variability in results which may be expected in parallel titrations of the same suspension , a number of paired titrations were performed using 2 series each of 6 groups of 2 - 3 mice . in these experiments the mice were of comparable age but the members of corresponding groups were not litter mates . 
the values 2 sd and 3sd corresponded to ratios respectively of 2 - 0 and 2 - 82 , so that a significant difference between the td50s obtained for parallel titrations in control and treated animals should be considered when this figure was used as a guide ; the following further their ratio exceeds 2 - 0 . test of significance being applied when the ratio of the results exceeded 2 - 0 : the td50 and its standard error were calculated from the results of each titration by the approximate method of irwin and cheeseman ( 1939 ) ; the limits of error of each td50 were defined from a value 3 x s.e. , and a significant difference was inferred when the limits of error of the td50 with the greatest s.e. 
did not include this criterion of significance was the td50 value given by the other titration . used by the authors of the method to compare ld50s in certain toxicity tests . the adequacy of the test in the present context appears to be justified by the the multiple difference of td50 values obtained in following considerations : 8 pairs of titrations using only 2 - 3 mice per group , and with only random pairing of mice between the two series , did not exceed 2 * 0 ; in the parallel titrations to the results of which the test was applied , however , there were 4 - 6 mice per group , and each mouse of one series was carefully paired with a mouse in the corresponding group of the other series , the members of a pair being usually litter mates but occasionally mice from two litters born on the same day . 
each mouse received four equal inocula in the following sites : subcutaneously in the right axilla and right groin ; intramuscularly in the medial muscles of the proximal segment of the left forelimb and in the adductor muscles of the left leg . 
the inter - actions of multiple inocula in a single mouse . no normal mouse of the age and stock used has failed to develop a palpable tumour from the inoculation of undiluted s37 mince or of single - cell suspensions nevertheless , the behaviour of s37 transplants in of over 100 , 000 viable cells . the mice used displays the immunological phenomena characteristic of most strain - heterologus transplantations : regression occurs in a high percentage of tumours , and solid immunity to a second transplant usually follows upon the regression . 
from the fact that growth of s37 in the mice used results in the induction of resistance it must be assumed that each of several simultaneous inoculations into the same animal , whether of equal or of graduated doses , may be subject to influences of a constitutional nature induced by the others . to investigate this possibility a suspension of s37 cells was titrated in two series of mice . 
each series consisted of 6 groups of 5 mice each , and corresponding groups of the two series received the same dilution of the suspension and the same cell dose per inoculueach mouse of a group in one series ( s ) received a single inoculum of the appropriate dilution subcutaneously in the right axilla . 
each mouse of a group in the other series ( m ) received 6 subcutaneous inocula , all of the same size , one of these being in the right axilla . 
when the td50s were calculated from the right axilla results alone for each series their ratio was 1 - 6 , the difference it was concluded that the practice of giving four equal being not significant inoculations per mouse , in order to increase the number of sites used in the calcula374 h . 
hewitt tions , was probably not associated with results peculiar to the multiple inoculation procedure itself provided that the several inocula in each mouse were of equal sizes . a further experiment was designed to show whether the resistance induced by a large inoculum was capable of preventing a smaller inoculum of cells , placed simultaneously elsewhere in the same animal , from becoming a palpable tumour . a number of 3 - 5 - week - old albino mice were randomised to give one series ( c ) of 6 groups of 5 mice each and a second series ( m ) of 20 mice . 
the dilutions were inoculated into the mice of the successive groups of the c series in the usual way , 4 equal inocula being given to each mouse subcutaneously in the groin and axillary sites . 
the mean latent periods of all tumours arising from inocula of 247 , 741 and 2222 cells ( i.e. , in the region of the td50 ) in the s series and in the m series were respectively 13 - 7 days and 11 - 4 days . 
the 30 per cent incidence of tumours from 82 cells in the s series is fortuitously high , as may be seen from the trend of inoidence in this series . it is clear that the relatively high total inocula per animal with which the 247 , 741 and 2222 cell inocula were associated in the m series ( see last horizontal column of table ii ) has not significantly diminished the incidence or extended the latent periods of the tumours produced by these inocula . 
the effect of " hyalase " of the tumour incidence from small inocula of s37 cells . a single - cell suspension of s37 was titrated in two parallel series of mice . 
the influence of dead s37 cells upon the fate of small inocula of viable cells . in the following two experiments the effect of dead tumour tissue upon the fate of minimal inocula s37 cells has been studied under two conditions : ( i ) where the dead tissue was inoculated intraperitoneally previous to the inoculation of viable tumour cells subcutaneously , and ( ii ) where the dead tissue was incorporated in the inocula of viable cells . a s37 single - cell suspension was titrated in a control series of mice and in a parallel series each mouse of which had been inoculated intraperitoneally with 0 5 ml . 
of 20 per cent s37 mince freshly killed by repeated freezing and thawing . the inoculation with dead tumour tissue was made 48 hours before titration of the viable cell suspension . 
no significant difference between the td50s was obtained in the two titrations , their ratio being 1 - 07 . the second experiment was designed to show whether tumour production from minimal inocula is depressed or enhanced by the presence in the inoculum of a large preponderance of dead cells . 
hewitt the td50 values obtained in the two series were as follows : dilutions in gelatine - tyrode diluent dilutions in dead cell suspension 2818 although the difference ( ratio 4.3 ) was considerable , it did not quite attain significance by the irwin and cheeseman ( 1939 ) test . 
an experiment was therefore designed to compare under more carefully controlled conditions the activities on transplantation of two suspensions prepared respectively from these two sources . malignant ascitic fluid and four moderate sized subcutaneous tumours of s37 - were harvested from a single mouse inoculated intraperitoneally and subcutaneously with s37 mince 15 days previously . 
215 it will be seen from table iv that correlation between the td50 values in the two series is highest when the cell - determining tumour incidence is taken to be the larger unstained cell . 
1 shows the relationship between viable tumour cell dose and the proportion of inoculated sites giving tumours , for the c3h sarcoma and for s37 . the case of each tumour the points shown were obtained from two separate titraaverage tumour cells per inoculum ( loglo ) fig . 
the accuracy of the points is not sufficient to reveal the true character of the curves relating cell dose and tumour incidence but it will be seen that the rate of change of tumours incidence with log . 
white and loeb ( 1910 ) have described the successful transplantation of regressing tumours , and schrek ( 1936a ) has found no effect of immunity on the growth capicity of the tumour cells . these findings do not suggest the presence of humoral factors in regressing tumours which are active against the tumour cells themselves and encourage the view that regression is the result of primary breakdown of the stroma . the significantly lower td50 values given by intramuscular sites of inoculation compared with subcutaneous sites , for s37 , might ascribed to the greater vascularity of muscle . 
on the other hand , this site difference was not demonstrable for the c3h sarcoma , and a more likely explanation of the site difference found for s37 would appear to be that local resistance mechanisms are less readily manifested in the intramuscular sites . from the results of the experiments recorded in section 3 , it is clear that a small inoculum of cells is not suppressed , in the period before it forms a palpable tumour , by multiple and larger inocula of the same tumour placed simultaneously elsewhere in the same animal . this being the case , it seems probable that the failure to give rise to palpable tumours which is displayed by half the inocula of about 2000 cells of s37 , is not due to induction of systemic immunity by these 380 h . 
methods are described of preparing single - cell suspensions of mouse sarcomata from solid and ascitic tumours , of finding the viable tumour cell density in the suspensions , and of " titrating " them for tumour producing activity on inoculation . 
the implication of this finding for the problem of cell - free transfer is discussed . i wish to express my gratitude to miss catherine fysh , b.sc. , for skilled technical assistance , and to professor r . 
korteweg. victorieplein 45 , awkrdam , netherlawi8 received for publication december 8 , 1953 . round about the end of the last war the total number of deaths from cancer recorded in the mortality statistics of the central bureau of statistics for the netherlands showed a conspicuous decrease . in females the decrease amounted to 6 per cent , in males to 9 per cent approximately . in the different age - groups it was about the same . this statistical decrease was very pronounced in lung cancer in males ( table i )  . in this paper the forowing tumours are expressed in terms of headings of the detailed intemational list of causes of death : " lung cancer " : no . 
231 ( revision of ( the figures for deaths from lung cancer in females are too small for a 1948 )  . statistical analysis and will be left out of consideration in this paper )  . 
with cancer of most other organs the decrease was less than with lung cancer , and in breast cancer and in some other cancers there was no decrease at all . in norway , according to kreyberg ( quoted by doll , 1953 ) , there was a similar dip in the mortahty curve for lung cancer in the same years , whereas in england and wales this curve continued without any interruption ( don , 1953 )  . in my report for the symposium on the endemiology of lung cancer in louvain , in 1952 ( korteweg , 1953 ) , i left the question undecided , whether the statistical decrease of mortahty from lung cancer resulted from mis - diagnoses due to war circumstances - non - functioning of the x - ray apparatuses for instance - or whether indeed in these years fewer people died from this disease . according to the central bureau of statistics , during the hunger winter of 1945 1784 males and 609 females died from starvation in amsterdam , a town of about in the first weeks after the liberation the number of persons 800 , 000 inhabitants . suffering from hunger oedema amounted to many tens of thousands . 
he pointed out heading 57 of the detailed intemational list of causes of death , revision of 1938 , under which ar tumours of undetermined nature - those tumours of which it was not reported whether they were mahgnant in one of its subgroups the figure for the tumours of undeor not - are recorded . termined nature of the respiratory organs is given . it appeared that in the same years that the decrease in lung cancer was greatest , those undetermined tumours of the respiratory organs , a very small group under normal circumstances , had strikingly increased . evidently in this group many cases of primary lung cancer were hidden . 
the length of the ordinate for a given age - group , therefore , gives the percentage pertaining to that age - group of the sum of the lengths of the ordinates of all age - groups together . unbroken line : lung cancer . broken line : tumours of undeterxnined nature of the respiratory organs . dotted line : cancer all sites . the vertical dashes at the top of the graph give the averages for the periods in question , i.e. 
the increase of lung cancer mortality in the last 40 years points to an increase of the sum total of cancer promoting influences . the older people of to - day hved a great part of their lives in a period when the menace from these influences was less than it is at present . 
as contrasted with the situation with younger people , therefore , mortality from lung cancer in the higher age - groups does not correspond to the sum total of cancer - promoting influences of to - day , but to this sum in an earlier period . it can be calculated that an inclusion in the group of undetermined tumours of the respiratory organs of even a small number of metastatic cancers possessing the normal age curve would have substantially altered the age curve proper to lung cancer . 
2 gives the crude death rates in males per million living in each year for this combination of recorded and probable ( though not as such recorded ) lung cancer deaths in the netherlands . ' 14t l\ i - i - - i 1938 - i . 
korteweg from the corrected curve . ( d ) the concavity in the curve for the years 1938 to 1941 has disappeared during discussions with officials of the central bureau of statistics on the reliability of the data on which the statistics of the causes of death are based , facts appeared which threw a new hght on our problem . in the netherlands the physician has to fill in two forms for each death . 
one in small vfllages where everyof these goes to the local civil registrar , a layman . body knows everybody the secrecy of this form is not absolutely guaranteed , and this leads , in cases of death from , for instance , venereal disease or cancer , to many physicians reporting meaningless diagnoses , such as heart failure . itnder normal circumstances the official netherlands statistics of causes of death are based on the second forms , which find their way , in a sealed envelope , to the medical official of the central bureau of statistics in the hague . the diagnosis mentioned on this form is incomplete , the medical official makes inquiries of the physician responsible for it as to the complete diagnosis and eventually corrects it . 
as the secrecy of these forms is ensured , there is no reason whatsoever for reserve . in 1944 and 1945 - when there was a general railway strike and other means of transport were extremely scarce and undependable and in 1946 , there was a lack of opportunities for making inquiries about incompletely fired in - forms . this reduces the rehability of the statistics for cancer for these years . 
the statistical decrease of cancer of the cervix uteri mentioned above , as well as the greater part of the statistical decrease of deaths from lung cancer find their explanation in this fact . the situation was by far the worst in 1945 , when the war front cut the netherlands in two . 
the mortality statistics for that year are based exclusively on the diagnoses given on the forms which were sent to the local civil registrars . it is clear that this was detrimental to the netherlands statistics for 1945 , and that to search for other explanations for the big statistical decrease of deaths from lung cancer in 1945 would be a mere waste of time . the only part of the dip for which no explanation can be given is the decrease this is the only indication that of i 0 per cent of lung cancer deaths in 1947 . the low level of tobacco consumption or the severe malnutrition in the foregoing years might have somewhat influenced mortahty from lung cancer . this decrease is rather small , however , and in 1947 eving conditions in the netherlands had not yet quite retumed to normal , so that it would not be wise to attach much importance to it . the cause of the great differences in the numbers of deaths recorded from undetermined tumours of the respiratory organs between the years before and after 1941 could not be discovered . 
maybe changes in the staff or the working methods of the central bureau of statistics or changing over from the revision of 1929 to the revision of 1938 could account for it . 
the straightening of the curve for the crude deathrrates for the years 1938 to 1941 , after correctio ' n for the undetermined tumours has been made , seems an argument in favour of the supposition that most of these tumours were in fact true lung cancers . 
the same study indicated that an excessive output of ethanolamine frequently occurred in the urine of patients with severe parenchymal liver disease , but that in such cases it was always accompanied by an excess of many other amino - acids . 
the presence in the urine of large quantities of ethanolamine , as an isolated abnormality , in the patient with primary carcinoma of the liver was therefore of some interest . its excretion might have resulted from a disorder of metabolism consequent on non - specific liver damage or from some peculiar form of neoplastic cell metabolism ; or it might even have represented a hitherto unrecognised error of metabolism which preceded and led to the development of a primary carcinoma in the liver . it has for some years been recognised , as a result mainly of animal experiment , that ethanolamine plays an important role as an intermediary in the metabolism of phospholipids and amino - acids . 
1. - some metabolic inter - relationships involving ethanolamine and other compounds . experimental dietary deficiency of choline has also been extensively studied . in rats it has been shown to lead to the production of fatty livers , followed after some time by cirrhosis . 
more recent work has shown that this may be followed eventually by the development of hepatoma - like tumours ( copeland and salmon , 1946 ; staub , viollier and werthemann , 1948 )  . furthermore , choline deficiency of a severity not sufficient to produce cirrhosis predisposes the liver to the carcinogenic action of butter yellow ( opie , 1944 ; buckley , buckley and snipes , 1951 )  . in the human hepatomata that occur in tropical countries there is ample evidence that dietary factors are concerned ( berman , 1951 )  . 
il - , a housewife , was aged 45 years at the time of her death in 1950 . apart from an attack of jaundice at the age of 7 she was in good health until april , 1939 , when , at the age of 34 , she had a febrile illness with delirium and a she had a second similar attack in october that year , and productive cough . this , like the first , lasted about 3 weeks . she suffered from similar attacks each in that year her illness was more severe and was associated winter until 1942 . with generalised aches and pains and vomiting . since that time she suffered from morning vomiting and also a burning pain , relieved by alkalis , behind the despite these regular winter illnesses and an increasing lower end of her sternum . sense of tiredness she continued with her work in a munitions factory until 1945 . from then until her death in 1950 she worked as a housewife . in january , 1947 , she first noticed a painless lump in her abdomen . in march of that year , following an illness with fever and malaise , she noticed that her abdomen was becoming tender to touch , her appetite was failing and the morning vomiting was becoming more severe . it was at this time that she was first seen and admitted for investigation at university college hospital . both parents and her 4 siblings were all alive and well . examination revealed a pale , slightly cyanosed , nonicteric woman of 8 st . 
the pulse was regular at 90 and the blood - pressure was 110 / 60 mhg . there were rhonchi over both lung fields and bilateral basal rales . in the nervous system the pupils were normal , the kneeand ankle - jerks were absent and the plantar responses were flexor . 
was normal , the circulation time was 17 seconds from arm to lung and 35 seconds from arm to tongue . the cyanosis was rapidly and completely relieved by breathing oxygen . whilst in hospital she ran a continuous low - grade fever . 
the metabolic studies carried out during this period are described later . opportunity was also taken at this time to examine chromatographically the urines of both parents and the other 4 siblings ; all showed a normal concentration and pattern of amino - acids . at the conclusion of the metabolic studies the patient went home much improved for her fortnight 's rest and largely pain - free for the first time for 2 years . she was instructed to take methionine 1 g . 
ethanolamine labelled with 50 per cent atom excess of 15n . on june 21 , 1950 , she was readmitted to hospital with an attack of bronchopneumonia . apart from her chest infection and gross oedema of the legs her general condition was unchanged . she volunteered the information that since taking choline her abdomen had felt looser and had been less painful . pneumonia was successfully treated with penicillin , and whilst on this her fever was . 
cameron reported on the histological sections of the liver as follows : " the tumour is undoubtedly a hepatoma ; it has not changed in character between 1947 , when the biopsy was taken , and 1950 . the most notable 170 c . 
each 24 - hour urine was analysed chromatographically for amino - acids and chemically for in addition blood specimens were drawn soon after the last dose ethanolamine . of each supplement had been taken and were analysed for amino - acids . further 24 - hour urine specimens were collected from her as an outpatient after she had been for 4 weeks on 10 g . 
7. apart from the very strong spot given by ethanolamine the remaining spots are of similar strength and pattern to those found in many normal urines . there was , however , an increase to a slightly abnormal level of the strength of the cystine spot during the patient 's last few months of life , and the unidentified weak " under proline " is not commonly found in urine whether normal or pathological . 
the only clearly identified gross abnormality was , nevertheless , the increased excretion of ethanolamine . these results clearly suggested that the ethanolamine was not the result of variable extrinsic factors ( such as diet ) , but was more likely to be due to a continuing metabolic abnormality . the plasma chromatograms were quite normal , except for a faint trace of ethanolamine . this indicated a definite , if slight , increase in the ethanolamine concentration of the plasma since the quantity ( 625 ' , d . ) of desalted plasma ultrafiltrate analysed was not sufficient to reveal the ethanolamine present in the plasma of a normal person . 
the urine to be analysed was placed at the right - hand bottom comer of the paper . phenol was run as the first solvent in the direction from right to left , followed by collidine - lutidine in an upward direction as the second solvent . 
8. - section of rat hepatoma kindly provided by copeland . hepatocellular type of tumour produced by prolonged feeding on a choline deficient diet ; ( no carcinogens added )  . note the difference from the histology shown in the illustrations of the tumour of c . 
9. it is seen that the output of " apparent ethanolamine " increased most on the day after the ethanolamine had been given and was probably still increased on the second day . 
the " increase " after serine was almost certainly due entirely to serine and not to additional ethanolamine , since the chromatograms showed a greatly increased serine output on this day and serine also gives rise , in the assay method , to its equivalent of " apparent ethanolamine " ( see above )  . 
walshe it has been involved were very small and the " spots " only just detectable . shown that many of the known amino - acidurias result mainly , if not entirely , from a raised renal clearance ( low threshold ) for amino - acids ( dent , 1951b )  . is not necessary to invoke this mechanism as a cause for the ethanolamine excretion here , since the normal subject who took ethanolamine by mouth produced a comparable urinary output at an induced blood level roughly similar to that of the patient . 
we suggest that it can best be understood in terms of an increased membrane permeability , on the part of the tumour cells , for ethanolamine . if such abnormnal permeability existed , a larger percentage of the loading dose of ethanolamine would pass from the extra - cellular fluid to the cells of the patient than it would in the case of the normal control . 
the urine from 7 cases of extensive secondary carcinoma of the liver ( appendix b ) was also investigated with negative results . it is not clear from the evidence at present available whether there is a specific , though rare , type of hepatic neoplasm characterised by an increased urinary excretion of ethanolamine or whether any tumour , if large enough , would give rise to a similar finding . 
ch3 + ch3 ch20h ( c . ) ch2n ( ch3 ) 2 + ch3 ch20h ( d . ) ch2n ( ch3 ) 3 ch20h ( choline )  . but , as has been mentioned already , we now prefer the theory of an increased membrane permeability for ethanolamine . 
the principal objection , perhaps , to the theory of a metabolic block is that if it were appreciable im extent it should have resulted in some degree of choline deficiency as well as in the accumulation of unmetabolisable ethanolamine . in experimental animals choline deficiency leads to fatty infiltration of the liver followed by fibrosis and , if sufficiently 176 c . 
we are , therefore , unable to accept the possibility that the large urinary excretion of ethanolamine resulted from a disturbance of the known metabolism of choline or one of its important intermediate metabolites . 
we prefer to believe that it was caused by some other property of this particular type of heptoma , such as a disturbance of " cell membrane permeability . " a further problem has been posed by the complete failure to increase the excretion of ethanolamine in the experiments in which large doses of its known biochemical precursors ( glycine and serine ) were given by mouth . this fact appears to underline further the difficulties encountered in attempting to interpret the results of this type of " classical " experiment . presumably the compounds failed to reach the cellular site where they would have been converted into ethanolamine and , therefore , that our patient did not provide a suitable opportunity to study normal ethanolamine metabolism by the rather crude methods at out disposal . 
the prospect of success would have been much greater using isotopically labelled precursors , since isolation from urine of pure samples of ethanolamine for isotype analysis presents no great difficulty . in conclusion we wish to thank sir harold himsworth for permission to publish this case , professor m . 
copeland for his very great kindness in lending us his original blocks of rat hepatoma tissue ; also the following for permission to investigate the cases referrred to in the appendices : a . 
a chemical method of analysis suggested that the output of ethanolamine this was confirmed by a rough quantitative was of the order of 0 - 5 to 1 - 0 g . 
as this substance is probably not readily taken up even in normals from the extracellular fluids by the tissue cells or from the glomerular filtrate by the renal tubule cells , it was therefore readily excreted into the urine . 
the presumed source of the ethanolamine was the neoplastic liver cell , and the enormous mass of these cells ( about a quarter of her body weight ) in the patient was probably sufficient to account for a greatly excessive production of this compound . 
he had a cholecystectomy for gall in 1950 he had an attack of renal colic and a ureteric calculus was stones in 1942 . in 1951 he was admitted to hospital with severe upper abdominal and demonstrated . laparotomy revealed a moderate enlargement of the liver , with left shoulder pain . very numerous white opaque nodules scattered throughout the liver substance . 
h - , aged 53 years . apart from a cholecysfectomy in 1950 he was in good health until shortly before admission to hospital when he was seized with a severe low back pain , greatly aggravated by movement . 
a diagnosis was made of carcinoma of the bronchus with secondaries in the lumbar spine and liver . his course was marked by very rapid enlargement of the liver and progressive cachexia . 
the medium is left unchanged throughout each experiment . films of concentrated cell suspensions made after gentle centrifugation were in the present series stained by a combined leishman - giemsa stain , and by feulgen 's method . 
about 500 - 600 leishman - giemsastained films were studied in the course of these experiments . the appearances described are those found in the basic culture medium . the addition of 5 per cent rat e.e. 
causes few differencem , apart from raising the number of mitoses . the only divergent feature is the appearance of increased numbers of degenerate polymorphonuclears , probably owing to the metabolic stimulant action of the e.e. from the cytological point of view , the life of each culture of leukaemic blood may be divided into two phases . 
the first , during which there is evidence of multiplication , and to a less extent of maturation , of the immature cells , reaches a climax during the first day , and comes to an end some time during the second 24 hours . 
from this , it does not follow that there is an increase in the total cell count of the cultures , for there is also a concomitant dying - off of mature cells . if , however , the mitotic index is high enough , as in cultures containing e.e. , there may be an increase in the absolute number of immature cells . this means that proliferation outstrips maturation . mitotic figures , very rare in the peripheral blood , are regularly found in cultures from the second hour onwards . 
they occur mainly in myelocytes , but are also seen in myeloblasts . differential counts have been done as a routine , but the total numbers of mitoses are too small to permit precise conclusions on the phase distribution ; further , owing to the technique necessary in making smears , the recognition of telophases is often difficult , and their number probably greater than is apparent in counts . no gross deviation from the ordinary phase distribution has , however , been found . in particular , there is no evidence of a metaphase arrest in untreated cultures . 
the mitotic index reaches a maximum of four to six mitoses per 1000 immature cells at about the eighth hour of culture in basic medium , or of up to 19 per 1000 immature cells at about 24 hours , if e.e. 
an extensive literature deals with tissue culture of normal and leukaemic blood and bone marrow , and has been reviewed by bloom ( 1938 ) , and more recently by fieschi and astaldi ( 1946 )  . it is not proposed to discuss this volume of work in detail , especially in view of the fact that much of it is not strictly comparable , as the methods of culturing and of examining the cells were often different from those employed in this series of experiments . thus most workers have used the cultivation of solid fragments rather than that of cell suspensions , and have described the appearances in sections instead of smears . 
comment will therefore be restricted to a few papers in which results have been obtained by related methods . there is general agreement that survival of human leukaemic cells is possible in cultures , and though the maximum times given vary considerably , no claims of indefinitely prolonged life in vitro have been advanced . 
many authors report the development of non - specific connective - tissue cell strains such as macrophages and fibroblasts from the highly specialized blood cells , but this appears to depend on the presence of a solid supporting framework , and does not occur in cultures made in a fluid medium . mitotic division of immature cells has been frequently observed and generally found normal . it is of interest to note that whereas mitoses are extremely rare in the circulating blood , they begin to appear almost as soon as blood is withdrawn from the body . the rapid change can scarcely be due to the effect of the culture medium alone , but may well be caused by the removal of an inhibitory factor operative in the body . the occurrence of maturation is a more controversial question , and the various answers which have been given appear to be mostly based on impressions . strict proof can only be obtained if total as well as differential counts are done with adequate methods , and this is only possible in fluid cultures . israels ( 1940a , 1940b ) , working along these lines , maintains that maturation occurs normally . fieschi and astaldi , on the strength of smears made from solid cultures , admit a certain degree of maturation , but state that this is always less pronounced than the proliferative processes . 
the findings cited here and in the previous report tend to support the latter view . while the normal maturative changes have not been very striking in this series of experiments , the development of new and abnormal cell types has been it is remarkable that this has not been commented upon by other of interest . workers , except by fieschi and astaldi , who , in their fig . 
7 and 14 it can be seen that the coarsening of abnormal erythropoiesis . the chromatin pattern is accompanied by its breaking up into discrete fragit is possible that ments , the nuclear membrane remaining meanwhile intact . these appearances signify an abnormal prophase , the first stage of endomitosis . the abnormality is conceived to consist in a premature separation of the daughter chromatids , which does not lead to metaphase or to a breakdown of the nuclear membrane . 
the consequence is an increased nuclear size , which may express itself by lobe formation and can , but need not , lead eventually to a more or less regular nuclear division , unaccompanied by division of the cytoplasm . in this connection the disappearance of the nucleolus is noteworthy : it is apparently a prelude to the accumulation in the nucleus of desoxyribose - nucleic acid , which is made evident by the deeper staining in leishman - giemsa and especially in feulgen - stained films . it may be objected that small numbers of polyploid cells occur normally in tissue cultures ( macklin , 1916 ) , and that their formation can be encouraged by manipulations such as the reduction of oxygen tension ( barta , 1926 ) or variations in the temperature of incubation ( stillwell , 1944 )  . 
8 with its double layer of cytoplasm has often been described and pictured as typical of the cells of " monocytic " leukaemia ( d ' antona , 1931 ) , while the resemblance of some of the polymorphs to those seen in pelger 's anomaly has already been remarked upon . it may be concluded that immature blood cells can , in vivo , undergo changes similar to those which are here reported for in vitro work . 
the special conditions prevailing in cultures made in the fluid medium , and - by the technique described , are evidently particularly suitable for encouraging this sequence of abnormal it is probable that at least events , but do not permit full normal maturation . some of the abnormalities in cultures are explained by lack of metabolic factors ordinarily present in the body , and possible that study of the metabolic processes in cultures and of variations in the composition of the medium may elucidate if successful , such a study might lead to the nature of some of these factors . a clearer understanding of the reasons responsible for the varied behaviour in culture of different bloods . 
1. received for publication february 23 , 1948 . in a previous communication we reported that a strain of the shope rabbit papilloma had been transmitted for 10 serial passages in the domestic rabbit ( selbie and robinson , 1947 )  . 
the adaptation of this tumour virus as a transmissible infection in domestic rabbits occurred during experiments in which the simultaneous inoculation of shope papilloma virus and sheep dermatitis virus in domestic rabbits produced papillomas that proved infective to other rabbits ( selbie , 1946 )  . 
the further passage of this virus in domestic rabbits was materially helped by continuing the procedure of mixing a second virus suspension with the infective inoculum of papilloma virus , and also by treating the skin with croton oil before inoculation , but there was no evidence of an increase in the virulence of the virus suspensions during passage . in the present communication we shall show that carcinomatous transformation has occurred regularly in this transmissible papillomatosis , and in a mamner similar to that found in the non - infective papillomatosis that is produced in domestic rabbits by the inoculation of extracts of papillomas from the cotton - tail rabbit , the original host of the shope papilloma virus . 
2 , where it wir be seen that the addition to the medium of the drug in a concentration of 60 mg . / litre reduces mitosis to less than one half . 
the drug was given intraperitoneary in doses of 5 y twice daily over a 5 - day period . there was no difference between treated and untreated mice in the time of disposal . ar experimental animals have shown a temporary loss of weight after being given the drug . effed , 8 on human malignant di8ea8e . this report , which is prehminary in nature , describes the testing of the compound in 17 patients suffering from leukaemia , polycvthaemia vera , lymphadenoma , multiple myeloma and three types of carcinoma . cases were chosen because they were unfavourable or too advanced for other forms of treatment . this choice of the least favourable cases - makes it harder to compare the effects ofthe drug with effects obtained with other forms oftherapy . it is , however , of value to compare in any individual patient the effects of the drug against those of any other type of appropriate treatment given either prior or subsequent to 9500 . the drug was given intravenously in doses ranging from 0 - 09 mg . 
probably represents a working range within which toxic effects on the bone marrow are not serious . side effects were slight ; half the patients had anorexia or nausea , generary very shght . 
the dose used in this case resulted in a temporary fan in haemoglobin and a fall in the white blood count to 1000 per c.mm. , at which time she was given a simple blood transfusion . 
at the end of this remission she was suffering from lassitude and following treatment with abdominal discomfort , and a rising white blood , count . 9500 her well - being improved ; her white cell count fell and the haemoglobin , which was 86 per cent , rose slightlv . primitive cells fell from 26 per cent to 14 per cent within 4 davs . 
the siibsequent historyof this patient was complicated , 2 months - after treatment , by , ' hepatogenous jaundice with leukopenia . four months after treatment the ' haemoglobin began to fall and the white cell count commenced to rise , and sore throat appeared , primitive cells rising above the she was re - treated a month later with 9500 , no beneficial pre - treatment level . effects being observed in the week that elapsed between treatment and death . post - mortem examination showed a massive leukaemic infiltration of liver , kidneys and spleen . 
the bone - marrow from femur and sternum appeared active . multiple capillary haemorrhages were present in the myocardium and brain . is difficult to assess the effect of treatment in this case owing to the complicating factors . 
the i - emission , however , was not as satisfactory as that previously obtained with x - rays . myeloblastic leukaemia of naegeli type . - this was a terminal case which had been treated previously only with transfusions . within 7 days after treatment the haemoglobin rose and the white cell count fell from 145 , 000 to within normal limits . primitive cells fell from a pre - treatment level of 76 per cent to 37 per cent and the myeloblasts and premyelocytes disappeared completely . however , this remission , although dramatic , was short . 
an improvement in the leukaemic condition was prompt . five days after the first treatment the total white cell count was within normal limits and immature cells had been reduced from 40 per cent to ' 6 per cent of the total . 
a good remission was noted 20 davs after treatment , which compared well with her first and best remission fohowing splenic irradiation . the patient felt better within a few days . 
the remission as far as the blood count was concerned after 9500 a similar reduction in red cells and haemoglobin lasted one month . this las ' ted 4 months , after which the symptoms recurred . 
none ( transfusion ) ( bleeding from tumour ) ca8e ix . generalized lymphadenoma ( section proved )  . - this patient was nevertheless the enlarged nodes decreased given a rather low dose of 9500 . very temporarily and the skin itching from which he suffered disappeared for - about a week . 
a drill - biopsy of the mass did not yield conclusive proof of lymphadenoma , which was nevertheless following treatment the itching was reduced and probable on clinical grounds . the skin , which was dry and iethyotic , became more normal in texture . 
the relief of symptoms this patient showed an interesting initial rise in the lasted less than 3 months . polymorphonuclear count at 4 days , prior to the onset of leukopenia . 
on both these occasions improvement in well - being occurred and some reduction took place in the size of his enlarged liver , - the improvement after the second course of nitrogen mustard being much less . on admission for treatment with 9500 , the liver was enlarged and oedema of the legs was present . 
none of them responded to the drug . case xv was later given a second course of treatment simultaneously with x - ray therapy , both agents being given as weekly treatments for growth - restraint . 
a leukopenia is generary seen , especiary at higher dose levels . this is due to a fall in both granular and lymphocyte series . the fafl in the granular cells may be preceded by a transitory rise over 3 to 4 days , not seen unless blood counts are repeated soon after treatment . 
effect of 9500 on peripheral blood count in a non - leukaemic case . no initial rise has been seen in the lymphocyte count , which reaches the lowest level 1 to 7 days after the end of treatment . complete recovery is slow and would seem to take about 2 months . 
for these two reasons we have waited for several weeks before instituting a second course of treatment in any patient . an extended clinical trial of 9500 would , however , seem to be justified on several grounds : first because it may be found effective in diseases other than those quoted ; even among the cases described there would seem to be a place for secondly , it could be regarded as a it in the treatment of polycythaemia . pleasanter alternative to nitrogen mustard , since , unlike nitrogen mustard , 9500 does not produce gastric effects and there is no fear of local thrombosis . 
thirdly , the drug is active ifgiven by mouth ; we have so far not tried its clinical effectiveness by this method , since , animal experiments have demonstrated that by this route the haematological response was less predictable . there is one disadvantage to an easily given drug of such potency . it is possible that it might be used without the constant supervision and check of blood counts which is necessary . 
as with all cytotoxic agents , its use should be contemplated only by those with facilities for adequate laboratory examinations . the tissue culture work has been carried out by m . 
the purely acinar foci found in rlllb females were shown to ' persist in the absence of milk factor in this cross - suckled substrain and in the absence of ovarian hormone . 
they were referred to as benign adenomas rather than nodular hyperplasias on account of their eventual independence of ovarian in addition some small invasive tumours were found by microscopic hormone . examination that appeared to represent intermediate stages in progression from benign to malignant growth ( pulhnger , 1952 )  . afitoses were found in both types of growth with the exception of the keratinised foci . all the morphological varieties persisted after ovariectomy in old animals . ' in order to ' test the capacity of the benign growths for progression to malignancy , transplantation of as many as could be found in the fresh state was attempted . grafts were transferred to young unmated females and to others of the same strain breeding rapidly . 
the nipple area on cork was searched under a glass cover using a dissecting microscope magnifying 7 and 14 times and with sterile forceps for the presence of benign tumours . ( these are seldom all adjacent surfaces of dissecting visible to the naked eye unless stained . ) microscope and glass cover were thoroughly wiped with absolute alcohol . the event no trouble arose from sepsis . 
as each benign growth was found it was cut out with fine scissors and placed in a sterile embryo dish with a drop of sterile water on the inside of the cover glass to provide a moist atmosphere . 
the next nipple area was then excised and similarly grafting was done either under anaesthesia through an incision or by treated . injection with needle and trocar into subcutaneous tissue or peritoneal cavity . the inoculated hosts were unmated females about 2 months old or breeding females that had already bome one litter . all were of the same strain bred by brother and sister matings . 
they were left in the latter from 12 - 18 months , with 15 as the average . fourteen subcutaneous grafts of bem ' gn growths minced with scissors were made from 8 donors into 9 rapidly breeding females . 
we spent more than eight months working on one such incidental problem , which had to be solved before we could proceed with the main work . this effort was well rewarded , however . 
we not only improved our experimental approach , but also acquired information that will further our understanding of the intricate role played by biological factors in regulating the influence of external agencies on living cells . in view of all this , i should like to point out that our investigations of the genetic potencies of carcinogens are still in an early stage . 
when i learned , therefore , that vapours could reach the sperm of drosophila i was confident that it would be possible to produce fine aerosols of chemical solutions it was evident tbat , if we could develop an aerosol that could do the same thing . method of inducing mutations , we could work with a wide selection of chemicals that are soluble in solvents not injurious to the ' flies , and would not be limited to chemicals that can be vaporized at temperatures not lethal to the flies . after much experimentation we finally succeeded in developing an aerosol technique that is effective in inducing mutations in drosophila males . males are kept for several hours ( from 6 to 200 ) in an atmosphere containing an aerosol of the desired solution ; and after this treatment their sperm is tested for induced genetic changes ' by standard genetical methods . 
the flies are treated in a milk bottle , and the aerosol is generated intermittently , for 30 seconds every 30 minutes , by a de vilbiss nebulizer . in our work with chemicals we have concentrated on carcinogens , because there is a feeling.among geneticists that these coffipounds should also be mutagenic . 
what classifies them as carcinogens is their ability to change normal cells into cancerous cells - that is , to produce permanent changes in living cells , which this definition can also be applied are transmitted to the progeny of those cells . to mutagens , which cause permanent and heritable changes , or mutations , in cells . this series of experiments with carcinogens also included chemically related tests were made with nine polycyclic hydrocarbons ( four non - carcinogens . carcinogens and five ' non - carcinogens ) and with seven azo compounds ( three of them carcinogenic )  . 
the observations were made on induction of x - chromosome .onclusions lethals and of chromosomal aberrations coincident with lethals . reached on the basis of the experimental results are summarized in table i . from table t a definite correlation between mutagenicity and carcinogenicity is evident . 
of the seven carcinogens tested , six were found to be mutagenic ; and of the nine non - carcinogens onlv two were found to be mutagens , and one is still classified as doubtful . the evidence now available suggests that some chemicals ( dibenzanthracene , benzpyrene , and hydroxyazobenzene ) induce both gene changes - le . 
lethals and chromosomal aberrations , whereas some others ( benzanthracene , dimethylaminoazobenzene , and 2 - amino - 5 - azobenzene ) are more effective in inducing chromosomal aberrations . during our experiinentation it was observed that different males treated at the sametime quite frequently showed different results ; that is , genetic changes could be induced in some males m ' ore readily than in others . table ti gives the 116 m . 
at present the most likely solution seems to be that a gene is responsible for the observed variability of effect between different males and between different , experiments . i shall conclude this presentation by quoting freely the conclusions given in a paper presented at the meeting of the fourth intemational cancer research congress in st . 
from these results it seems reasonable to infer a common causative mechanism relating mutagenicity this inference is further strengthened by the behaviour and carcinogenicity . of all known non - chemical carcinogens , such as x - rays and related radiations . ultraviolet rays , and heat - all of which are also mutagenic . 
the most obvious and probable relation ' between mutagenicity and carcinogenicity is the one suggested by the hypothesis that cancer may originate through a gene mutation occurring in a somatic cell . 
such a cell , and the cells derived from it by division , would have their properties changed so that they would behave as cancerous . this would mean that higher organisms possess a gene - - or , more likely , a number of genes - whose mutations can initiate a cancer - type cell . it may be assumed that such mutations , like a great majority of mutations in other genes , would occur spontaneously with a very low frequency . 
the human body has a tremendously large num ' ber of cells , however , so that - it is probable that a cancertype mutation would occur a number of times among the cells of an individual . not all of these need give rise to cancer , since a large proportion of the cancertype cells might be prevented by normal cells from dividing , or might be eliminated in some other way . if gene mutation is responsible for the origin of cancer , then all mutagenic agents may be expected to increase the frequency with which such mutation occurs , and consequently to act as carcinogens . in our fight against cancer , therefore , precautions should be taken to avoid exposure to ' all mutagens chemicals as well as radiations . such precautions , however , even if rigorously enforced , would only lower the incidence of cancer ; they could not entirely prevent its occurrence . there would still be a chance left for cancer - type mutations to occur among the billion 's of cells that constitute the human body , and a mutated cell that continued to divide would give rise to cancerous growth . 
we know that mutations do occur with great regularity , caused by some force not yet explained , and that we have no means of stopping or controlling their occurconsequently , if cancer originates through a genetic change , our chances of finding ways to prevent it are very , very slight . 
the addition of methionine to the basal diet affords good protection against fatty cystine is not as livers and the health of the animals was much improved . reliable as methionine in this respect , probably on account of its toxic action ( curtis and newburgh , 1927 ) , and the growth rates of the animals in the cystinesupplemented diet show considerably more variation than those of the animals on the basal and methionine - supplemented diets . in experiments on the growth - inhibitory action of 1 : 2 : 5 : 6 - dibenzanthracene in rats maintained on a 5 per cent protein diet it was noticed that the treated animals had fatty livers . this 5 per cent protein diet ( for composition see table ii ) contained considerably less fat than the white basal diet , and the control animals maintained on it did not develop fatty livers during the course of the experiment ( up to 56 days )  . although combination of the hydrocarbon with essential sulphur - containing amino acids has been shown not to be a direct cause of its growth - inhibitory action , it was considered possible that on the very low ( 5 per cent ) protein diet such a combination might be sufficient to prevent the lipotropic action of these amino - acids , and thus result in the development of fatty livers . 
 - in the present investigation it has been found that the addition of cystine or methionine to the basal diet without incorporation of the growth inhibitory hydrocarbon brings about an increase in growth rate of the animal ; hence if the effect of this addition is also to negative the growth - inhibiting action of added hydrocarbon , the resultant growth rate should be greater than that produced by the basal diet alone , which , on white 's results , is not the case . the white basal diet is a very poor diet for maintaining the health of the animals , and a number of deaths occurred after a few weeks . 
they are of twofold character : ( 1 ) mortality statistics and post - mortem examinations ; ( 2 ) systematic bloodpressure examinations among people of various ages . relying on mortality statistics of the united states , fahr ( 1928 ) estimates essential hypertension to be the cause of death of 23 per cent of the population aged over 50 years , a figure which is held by volhard ( 1931 ) as being too small . bell and clawson ( 1928 ) , on the strength of exact anatomical examinations , came to the conclusion that in all cases of mortality about 7 per cent in the 40 to 49 agegroup and 13 per cent of people over 50 years are dying from hypertension . 
zondek the attempt to come to a definite estimation of the incidence of essential hypertension based on the numerous blood - pressure examinations among various classes of a certain population undoubtedly encounters certain difficulties ; one of the main difficulties lies , in my opinion , in the precise definition of essential not every rise in blood pressure , even a permanent one , is , of hypertension . it is rather easy to exclude course , connected with true essential hypertension . cases of secondary hypertension , such as those caused by bright 's disease , aortic valvular disease and hyperthyroidism ; moreover , from a statistical point of view , these cases do not play a major part , at least not in the age - group which is of particular interest to us . 
a person was not classified as suffering from essential hypertension unless , constantly , or at least in most of the exaniinations carried out , a blood pressure of more than 160 / 90 mhg was detected , i.e. , 165 / 90 or 160 / 95 and more . though a permanent diastolic pressure of 95 mhg may be regarded as a very reliable proof of the existence of essential hypertension , if diseases such as bright 's disease can be excluded , we based our examination nevertheless on a somewhat lower pressure , i.e. , 90 mhg ; we did so because people suffering from hypertension in the course of their illness may not infrequently display a lowering of their diastolic pressure , probably as a result of developing arteriosclerosis ( fishberg , 1939 )  . 
the decrease of diastolic pressure from 95 to 90 mhg as a minimum value for essential hypertension will , of course , increase the figure for the morbidity of hypertension ; but , apparently , a compensation has been created - at least in men - by relating the diastolic pressure to a minimal systolic 134 s . 
zondek pressure of 165 mhg . ( blood - pressure has always been taken while there is no statistical method , based on blood - pressure patient was sitting . ) examinations alone , which will include every case of essential hypertension , or will , with certainty , exclude every other type of hypertension ; but this is not of paramount importance , since in view of the high incidence of essential hypertension , small degrees of error will probably not be significant . it may reasonably be assumed that the figures contained in our statistics , and especially in that of master , marks and dack ( 1943 ) , indicate fairly accurately the incidence of essential hypertension in the various age - groups ; confirmation of this assumption may be noted by the figures contained in the mortality statistics ; nor do the anatomical examinations quoted above contradict this . what , in comparison , is the incidence of essential hypertension in cancer patients ? we shall not attach any importance to anything but a great deviation from the normal rate . 
the number of cancer patients referred to in this paper is 1490 ; a certain proportion of the cases has been observed by us ; as to the remainder , we obtained the necessary data from the cards of the cases put at our disposal by various hospitals of the country . 
the number of other types of carcinoma , such as carcinoma of the gall - bladder , pancreas , liver , kidneys and respiratory tract , was not great enough to be used for separate statistical elaboration . for the same reason , in men , only the cases of carcinoma of the digestive tract were statistically elaborated . essential hypertension proved to be a rather infrequent occurrence in all it is more or less the age - groups , but especially between the ages of 40 to 59 . same picture as that reproduced in the general statistics ( table i )  . though the number of cases of carcinoma of the respiratory tract examined by us was relatively small , we tended to find the same relationship to hypertension as in table i . 
we examined 37 cases in the age - group 40 to 59 , of whom only one showed hypertension . two factors may be held responsible for the rare occurrence of a combination of carcinoma and essential hypertension : ( 1 ) carcinoma may have a depressing influence on a previously existing hypertension ; ( 2 ) a person suffering from essential hypertension may have smaller tendency to develop carcinoma . the possibility of a depressing action of carcinoma cannot be denied . 
in this connection we may quote the investigations of rosenfeld ( 1929 ) , feldweg ( 1929 ) and fortunati ( 1936 ) , who were among the few who carried out systematic blood - pressure investigations in cases of cancer ; in the course of the illness a fall in blood pressure could be detected , though the fall , if present , was in most cases only moderate . 
the number of cases examined by fortunati ( 1936 ) was very small ; yet it occurred to him that high blood pressure is more often met with in cases of cancer of breast and female genitals than in cases of cancer of the digestive tract ; he failed , however , to take into consideration the normal incidence of hypertension ; therefore , he could not even try to answer the decisive question as to whether the frequent occurrence of hypertension in carcinoma of the breast and female genitals or its rare occurrence in carcinoma of the digestive tract are to be considered as extraordinary . 
sterile vials , each containing 0 - 7 g . of a mixture of the sodium salts of the four nucleotides of yeast ribonucleic acid preserved with 0 - 3 per cent cresol . the mice used were the f1 cross of the a and c 57 lines . these were chosen because a mice have a relatively high spontaneous lung tumour incidence ( bittner , 1939 ; heston , 1940 ) , and it has been observed that such strains respond more readily to the carcinogenic effect of urethane ( cowen , 1947 )  . 
the hybrids would also tend to have a high spontaneous incidence , since the inheritance of spontaneous lung tumours in this cross seems to be due to a single dominant gene ( bittner and little , 1937 ; bittner , 1938 )  . seventeen a x c 57 males approximately two months old were injected with the pentose nucleotides solution subcutaneously at the flanks , daily at midmorning . 
of pentose nucleotides for a week the water . mice started to show ill effects . both treatments were discontinued ( after 2 weeks of pentose nucleotides and 1 week of urethane treatment ) for two days , on resuming treatments the dosage of pentose nucleotides to rest the mice . was decreased to 0 - 3 c.c. 
the figure clearly shows that a marked inhibition of the carcinogenicity of urethane was produced by the pentose nucleotides . the average number of lung tumours per mouse caused by urethane in controls 1 and 2 separately was 46 in each case , which was reduced to 26 in the p . 
strong. from the school of medicine , yale university , u.s.a. received for publication february 2 , 1949 . the idea of somatic mutation as an explanation for the origin of cancer has had a long and interesting history . its original use as an interpretation of cancer is usually associated with the names of murray and of boveri . these men arrived at the somatic mutation conclusion from different fields , murray from experimental cancer research , and boveri from his classical observations in experimental embryology . 
at that time he stated : " the existence of such tumours , the biological characters of which are retained through long periods of propagation , shows that the cellular transformation which initiates carcinomatous growth may take place in varying degrees . 
the ratio of the concentration of the compounds in the stomach to that in the blood in this range was about 20 : 1 or greater . by selecting carcinogens that have a pk , , falhng in this range it should be possible to circumvent the mucus barrier and expose the glandular stomach to attack . 
the animals had been fasted for 48 hours preceding the operation to simultaneously with the injecavoid contamination of the secretions with food . tion of the compounds to be tested 0 - 2 mg . 
with acetone and this extract allowed to stand overnight it was then centrifuged for 20 minutes at 2000 r.p.and the superat 5 - 10 ' c . natant used for spectrographic analysis . measurements were made on a beckman model du spectrophotometer against acetone - hci standard having the same ph as the gastric extracts . standard curves were obtained which essentially followed beer 's law . 
the 2 , 5 - isomer is soluble , whereas the 2 , 7 - isomer is not ( morgan and thomason , 1926 )  . yields of 55 to 60 per cent were obtained of 2 , 7 - dinitrofluorene decomposing at 293 - 4 '  . the 2 , 7 - dinitrofluorene was reduced with tin and hydrochloric acid by the method of schulman ( 1949 )  . 
the pure compound melts at 165 ' after recrystalthis was then converted to the dihydrochloride and lization from benzene . 2 - acetylamino - 7 - aminomono - acetylated in aqueous solution ( schulman , 1949 )  . fluorene hydrochloride was then slurried in 500 ml . 
the almost clear solution was filtered hot and a cream - white product precipitated from the cooled three recrystallizations from 50 per cent acetic acid resulted in a filtrate . goulden and kon ( 1945 ) reported that 2 - hydroxy - 7compound melting at 232 '  . acetylaminofluorene melts at 232 '  . the dyes of this series were prepared by coupling the components in acid buffered , or basic aqueous solution , neutralization and filtration . 
the yields ranged from 70 to 90 per cent . products could be recrystallized from dilute cellosolve , but highest purity was obtained from aniline , or benzyl alcohol . these compounds have not been previously reported . constants and analyses are given in table il 368 f . 
compound iv seems to be secreted to a slightly lesser extent , but this may not be significant . this was entirely unexpected , because it has a pkb ( 8 - 5 ) which hes in the optimum secretion range ( ray and jung , 1951 )  . this indicates that the pkbof maximum secretion in the fluorene series is much higher than it is in the benz ' ene series . because the serosa was colored , it was thought that this dye might have been reduced in the stomach at the azo link . 
an examination of the stomach contents for aminofluorene by the method of westfall and morris ( 1947 ) by miss mary f . argus failed to show the presence of this substance , either free or coniulyated . while , successful in leading us to potential carcinogens that are secreted in large amounts by the stomach , it is obvious that some factor ( or factors ) are involved other than the pkbit is true that the stomach of the rat may be less acidic than that of the dog , but this should only reduce the total concentration and not the relative order of absorption . the use of a tricyclic molecule hke fluorene in place of benzene leads to compounds with greatly reduced solubilities in dilute acid . 
the introduction of a third ( insoluble ) phase might well cause the stomach barrier to operate to exclude compounds of lower pkb ( greater basicity )  . the demonstration that some of these compounds are secreted in rather large amounts in the stomach has encouraged us to set up long - time experiments for testing their carcinogenicity . 
 data have been published which indicate that the average latent period for all methylcholanthrene - induced fibrosarcomas ( strong , 1948 ) and the survival time ( strong , 1950 ) of mice developing such tumours are both influenced by litter seriation . 
the latent period ( time between the subcutaneous injection of the carcinogen and the initiation or the initial growth of the ensuing fibrosarcoma ) was variouslv affected in the different strains bv the litter to which the mouse in mice of some strains ( prunt and f : of c67 x brs ) the latent period belonged . 
 ( strong , 1948 ) for the appearance of fibrosarcomas decreased in the successirn litters of the same pair of mice , while in other strains susceptibility to fibro sarcomas was relatively constant . 
the sunival time ( strong , 1950 ) of mice growing a chemically - induced fibrosarcoma ( time between the initial growth of the malig nancy and the death of the individual ) is also affected by litter seriation . 
 ' \\nen a mouse developed a fibrosarcoma in less than 100 days following the subcutaneous injection of methylcholanthrene it sunived an average of 52 days with the progressive growth of the tumour ifit belonged to a first litter . 
in the succeeding litters mice of the same age and latent i : eriod survived longer and longer with growing fibrosarcomas until , if they belonged to an eighth litter , they lived on an average of 130 days . 
these genes were derived from mice of the ancestral stocks jk and n which were used in the origin of the : xho stra the first three generations ( cba... " x jk ) were used for breeding purposes only . 
at the time of the separation of prunt from pbr descent , the average latent period for the appearance of methylcholanthrene - induced fibrosarcomas of the direct in the f 20 generation of the experimental maternal ancestry was 3695 days . 
these two untreated descents , prunt and 2prunt , should possess genetic similarity , and any biological differences that they have may be due either to divergent segregation from a residuum of genetic heterozygosity ( probably very small after 17 generations of brother - to - sistier matings ) or to new biological variability which has appeared in one or both untreated deseents following their separation from a common ancestry . 
the mice were fed a standard diet of nurishmix pellets ( pratt food company ) and water ad libitu a supplement of mixed grains ( oats , wheat and sunflower seeds ) and calf meal pellets were given to the mice once a week . 
the mice were examined periodically for tumoun ; , and the latent period taken to be the time at which a firm nodule at the site of the injection of the carcinogen began to increase progressively in si mice which developed tumours at sites other than the one at which the carcinogen had been injected were tabulated separately . 
 table i gives the percentage incidence of tumours in mice which developed in less than 100 days ( column e ) , together with the data obtained on all tumours at the site of injection of the carcinogen irrespective of latent period ( column d )  . 
 data on the total number of mice injected with methylcholanthrene ( column a ) , the number of mice which died without developing any tumour ( column b ) , and the total number of mice showing tumours irrespective of latent period and site are also given ( column c )  . 
since the two separate descents disclose similar genetic origin and show similar trends by which the females are consistently more susceptible to fibrosarcomas than the males , the data for both series may be added together . 
however , the present analysis of trends of susceptibility in s1icoessi.e litters discloses differences , and therefore the two strains , the prunt and the 2prunt , should be kept distinct . 
thus 27 2 pe : r cent of the females developed fi.brosa : rcomas within less than 100 days of latent period , whereas only 92 pe : r cent of the males developed similar tumou : rs during the same period , a difference of 180 pe : r cent in tumour susceptibility  . 
the trend for the percentage incidence of tumours developing in less than 100 days among females of successive litters was found to be y = 85 + 5 lz , with a standard deviation of the slope of 0 - 741 . 
comparison of this value with a no - trend or 0 - slope value by t test reveals that the observed trend is statistically significant ( since p = < 001 )  . 
 similarly the trend for the percentage incidence of tum.ours developing in less than 100 days among males of successive litters was found to be y = 132 - 12x , with a standard deviation of the slope c , f 0968 . 
 the analysis of the data thus discloses that there is an increasing sex differential in relation to chemically induced : fi.brosarcomas in successive litters in mice of the prunt descent . 
the difference between the mice of the two descents must , therefore , be associated with a mechanism which in the 2prunt descent changes in litter seriation at least in some strains of mice . 
 the maximal sexual differential is found in mice of the second litters ( 302 per cent ) , and this sex differential fluctuates in the succeeding litters and thus shows no significant trend . 
however , the data of the 2prunt descent are complicated by a high value for females of the second litter ( 382 per cent ) and a high value for males of the sixth litter ( 143 per cent )  . 
in one strain ( the chi ) males were more susceptible to chemically induced fibrosarcomas than were the females , whereas in the 15th inbred strain ( the cul ) the females were more susceptible to tumours than were the males . 
 the mechanism involved in the development of this new sexual differential in relation to chemically - induced fibrosarcomas in mice of the prunt descent gives a slight sex difference in mice belonging to the early litters of a breeding female , and apparently gradually increases in the succeeding litters . 
h the sex pattern of an individual is the reflection of the genetic constitution of the individua1 , then it is not clear whether mice of the early litters or mice of the later litters are to be considered the pattern for the species . 
but sex physiology is also under the influence of several hormones , and the sex pattern can be influenced significantly when a hormone is administered at an early age , preferably before birth . 
 the present investigation with methylcholanthrene has disclosed that several aspects of malignancy ( the average latent period , the survival time and the per centage susceptibility of tumours in mice of latent periods of less than 100 days ) are influenced by litter seriation . 
do hormones fluctuate in the female body with advancing litter frequency , pass the placental barrier and influence the subsequent physiology of the offspring at least in relation to malignancy and perhaps to other characteristics as well ? or are we to conclude that maturation phenomena in cytoplasm ( perhaps the mito chondria or other constituents ) are responsible for this transmission from mother to offspring which apparently is not through the genes ? perhaps another biological reason may eventually be found for the data at hand . 
these mice belonged to two separate descents derived from a common genetic orig in one descent , the prunt , there was an increasing sexual differential in relation to chemically - induced fibrosarcoma.s in the succeed320 l . 
cravetz. from the lawall memorial laboratory of pharmacology and biochemi8try , philadelphia college of pharmacy and science , philadelphia , penn8ylvania . received for publication june 15 , 1951 . caspersson and his associates advanced a hypothesis on the ' role of nucleic acids in the biological synthesis of proteins ( caspersson , 1947 )  . several other results suggested the role of nucleotides in the metabolism of tumors as well , as a result of which many structural analogues of pyrimidine and purine derivatives were synthesized and tested for anti - cancer and growth - inhibiting activity ( roblin , lampen , english , cole and vaughan , 1945 ; kidder and dewey , 1949 ; kidder , dewey , parks and woodside , 1949 ; sugiura , hitchings , cavalieri and stock , 1950 ; burchenal , bendich , brown , clian , hitchings , rhoads and stock , 1949 ; skipper , bennet , edwards , bryan , hutchison , chapman and bell , 1950 ; law , 1950 ; lewis and crossley , 1950 . ) however , little is known about the effect of the naturally occurring nucleotides on tumor growth . parsons , gulland and barker ( 1946 , 1947 ) described that in c57 mice the growth of homologous methylcholanthrene sarcoma grafts was inhibited by ( yeast ) ad ' enylic acid or guanylic acid ; uridyhc acid showed a growth - promoting effect , whereas cytidylic acid had no effect . 
tumor cells are free in the ascitic ascitic fluid was harvested by fluid , usuar abdominal puncture under aseptic conditions , and the number of cells present in the ascitic fluid counted in a hemacytometer . 
cravetz the method used in this study offers the forowing advantages : ' ( a ) cancer cells of known number and equal virulence are inoculated into the control , as ( b ) upon intraperitoneal inoculation similar well as the experimental animals ; ascitic tumors are produced , while subcutaneous inoculation results in the development of solid tumors ; ( c ) in case of intraperitoneal inoculation the action . 
the error in thi 's method is that there is always some microscopic infiltration of sohd tissues in the peritoneal cavity ( klein , 1950 ; klein and klein 1951 )  . cells are , of course , not included in our cell counts . these infiltratin ' swiss mice , bred in our colony , were used for these studies . these mice were maintained o ' n rockland complete rat diet and water , ad libitum , and kept in air - conditioned quarte ' rs at 2 p c . 
the strain aspecificity of this tumor was discussed by klein ( 1950 ) and klein and klein ( 1951 )  . subcutaneous inoculations were twenty - one days after inoculation the made into the caudal third of the back . groups animals were sacrificed , and their tumors dissected and weighed . receiving intraperitoneal injections of cancer cehs were observed for mortailty animals dying were autopsied , their ascitic fluid harvested and measured , rate . and the number of cancer cehs per cubic mihimetre estabhshed as previously descr ' lbed . nucleotides were administered by daily subcutaneous injection , alternating adenosine - 3 - phosphoric acid was injected in between the right and left flank . solution in 3 - 2 per cent disodium phosphate , adenosine triphosphate and adenosine - 5 - phosphoric acid in normal saline warmed to about 37 ' c . 
mean tumor weight8 in gram8 . serim i ( 2 , 000 , 000 cells ) meem mean mean mean serim 11 ( 2 , 000 , 000 cells ) : serim ih ( 2 , 000 , 000 cells ) seriew .1 v ( 200 , 000 cells ) : adenosine - 3adenosine - 5adenosine phosphoric acid phosphoric acid triphosphate i 00 mg . 
the number of cancer cers , however , was smaher in the ascitic fluid of the nucleotide - treated mice than in the control animals . we are greatly indebted to margaret r . 
7. received for publication june 19 , 1948 . the testing of substances for anticarcinogenic properties must proceed on purely empirical lines , or be based upon a hypothetical conception of the nature of some phase of the biochemical mechanism of chemical carcinogenesis . suggestive , but not conclusive , evidence has been obtained that s - metabolism is intimately connected with a primary stage in the interaction of chemical carcinogens with cellular constituents . 
crabtree in the groups receiving either the carcinogen alone or in conjunction with a substance which proved to be innocuous , the number of mice surviving the full all mice were epilated course of the experiment was always 90 per cent or over . over the scapular region once only , two days before the experiments began . the approximate amounts of carcinogen and tested substance used in any one experiment were as follows : 0 - 1l% 3 : 4 - benzpyrene 0 2% / methylcholanthrene 0 20 / 2.0% s - compound 1 : 2 : 5 : 6 - dibenzanthracene solutnused . 
a 0 1 per cent solution has been found most convenient , since with higher concentrations less obvious effects are produced by an inhibitor , and with lower concentrations the experiments are unduly prolonged , thus favouring any possible toxic action of the substance tested . 
with the strain of mice used , the average time for tumour induction with 0.1 per cent 3 : 4 - benzpyrene applied twice weekly is 16 - 0 i 0 1 weeks , a figure obtained repeatedly in many experiments . the substances tested were chosen for no other reason than that of convenience . 
when this occurred in the early part of an experiment and clearly reflected the toxicity of the substance tested , the difficulty was easily met by using smaller doses of the toxic agent . 
spicer. influence of bal on induction time . the results for bal have been analysed in two parts . those for bal and benzpyrene , where several percentages of bal were used , can be analysed using the technique of regression ( fisher , 1947 )  . that is to say a straight line is fitted to the mean induction times by the method of least squares ; if the slope of this line is significantly different from zero , then bal can be said to exert an inhibitory effect on the benzpyrene . the slope of the line is a measure of the efficacy of the bal . 
 " a lesser mass increment " of transplanted tumours was observed when the hosts were injected with diphenylsulphoxide or diphennylsulphone ( hammett , 1930 ) , and cystine disulphoxide proved inhibitory to the growth of spontaneous mouse tumours ( staff of the lankenau hospital , 1936 )  . conversely , compounds containing s in the reduced form , r.sh ( the nature of r appears to be of secondary importance ) , were shown to stimulate cell - division in a wide variety of plant and animal tissues ( hammett , 1931 )  . arising from these results it was anticipated that the increased proliferation of the cells in mouse skin induced by treatment with an sh - compound would render the tissue more susceptible to the action of a p - thiocresol was therefore applied in conjunction with a carcinogen , carcinogen . but the opposite effect was observed , i.e. 
the sh - compound caused a pronounced retardation in the rate of tumour induction ( reimann and hall , 1936 )  . reimann and hall performed a variety such inhibition stands in sharp contrast to the entirely innocuous behaviour towards carcinogenesis of the mono - thiol compounds used in the present work . the discrepancy can hardly be attributed to variations in the activities of the sh - compounds themselves , and must be referred to differences in experimental techniques . of experiments differing only in the amounts of carcinogen and p - thiocresol administered , and the timedistribution of their application . the actual doses of carcinogen varied from experiment to experiment , e.g.. 
the control group of mice received 2 - 4 times as much 1 : 2 : 5 : 6 - dibenzanthracene over the latent period as the groups treated with p - thiocresol , and this feature alone would suffice to account for the wide variations in average induction times , and the apparent inhibitory effect . moreover , the choice of lanoline as a solvent for p - thiocresol was unfortunate , since the work of twort and twort ( 1929 ) , rosicky andhatschek ( 1943 ) , simpson , carruthers and cramer ( 1945 ) , and berenblum and schoental ( 1947 ) , have shown that lanoline greatly retards the carcinogenic action of tar , 3 : 4 - benzpyrene , and methylcholanthrene . complicating factor augments the difficulty of accepting the experiments of reimann and hall as a demonstration of the anti - carcinogenic activity of sh - compounds . of the mono - sh - compounds used in the present work , together with the fact that bal , a di - sh - compound , can cause a moderate retardation of carcinogenic action , clearly signifies that the mere presentation of any sh - containing molecules ( as implied by the philadelphian workers ) is not in itself sufficient to produce a biological effect ascribable to the sh - group . experiences of peters , stocken and thompson ( 1945 ) in the search for a suitable sh - compound , which culminated in the discovery of bal , also emphasizes this . apart from the question of variable toxicity , which rules out a substance like the lack of activity this added 288 h . 
crabtree toluene - 3 : 4 - dithiol , it is evident that the total molecule , with sh - groups appropriately disposed , is a factor of importance . the analogy with the anti - vesicant activity of bal cannot be pushed too far , since experiments in vitro clarified the nature of the reaction between bal and lewisite , whereas any possible reaction between bal and a carcinogen , modified in an unknown way , cannot be attempted at present . lacassagne , buuii - hoi and rudali ( 1945 ) have ostensibly shown that competition between a potent carcinogen and a structurally related substance with their little or no carcinogenic activity can result in delayed tumour induction . work was an outcome of the conception that " the mutation which transforms a normal cell into a malignant cell is the result of the alteration of an organic substrate by the fixation to it of some toxic molecules ( in this case polycyclic chrysene , l : 2 : 5 : 6 - dibenzfluorene , five isomeric dimethyl - benzhydrocarbons )  . " acridines and a trimethyl - benzacridine were chosen as near relations of methylresemblance to cholanthrene , and 1 : 2 : 5 : 6 - dibenzacridine for its structural though they state in general terms that inhibitions 1 : 2 : 5 : 6 - dibenzanthracene . of carcinogenic action were demonstrated , the experimental details hardly justify so wide a conclusion , since only chrvsene and 1 : 2 : 5 : 6 - dibenzfiuorene caused some slight delay in tumour emergence . 
 from the department of experimental , pathology and ganeer research , university of leeds , and department of pharmacology , guy 's hospital , medical school , university of london . 
greenblatt and kupper man ( 1947 ) , also using the rat , observed squamous metaplasia of the horn and a doubtful precancerous lesion in the cervix uteri , but no tumours , when a similar dose of methylcholanthrene was introduced . 
pan and gardner ( 1948 ) reported the development of numerous carcinomas and sarcomas in mice of several strains , when subcutaneous implants of cervical and uterine epithelium - were made together with small crystals of methylcholanthrene . 
 in the experiments described here uterine tumours were induced by the intro duction of methylcholanthrene directly into the uterine horn in two types of mice and the effects of various hormonal factors were studied . 
 the experiments were performed on two types of mice : inbred cba mice , maintained by brother - sister mating in the department of cancer research at leeds , and white mice obtained from dealers . 
the gun was intro duced through the incision , a fine silk ligature placed around it a short distance below the incision , and the carcinogen pushed out into the lumen of the horn . 
the amount of material introduced in solution in lard varied considerably , depending on the size of the uterus , but there is no doubt that the weight of methylcholanthrene introduced with method ( 2 ) was less , and sometimes considerably less , than that introduced into the uterus with method ( 1 )  . 
 ( 3 ) this method was similar to ( 1 ) and ( 2 ) , except that the upper part of the horn through which the material was introduced was removed . 
the upper part of the vagina was then exposed and dissected free from surrounding tissue and partly separated from the rectu a stout ligature was loosely placed around the vagina just above the symphysis pubis . 
the needle was introduced into the vagina and pushed up above the level of the ligature , which was then tied ( with one knot ) around the needle and held tied by an assistant . 
the ligature around the lower end of the left horn was tied , the ligature around the vagina rele : ased and removed , and the needle with syringe withdrawn . 
 the abdominal organs were carefully palpated at regular intervals to deter mine the first appearance of uterine tumours , but the mice were not killed until they appeared to be ill or until there was no doubt about the presence of an abdominal tumour . 
 of 15 immature oba mice , 12 developed tumours of the uterus , as follows : 4 had carcinomas , 6 sarcomas , and 2 both types of tumour ( table i )  . 
 the tumours presented a homogeneous translucent appearance , sometimes with haemorrhagic and necrotic areas , except in the case of the squamous cancers , table 1 . - 0oourrenoe of tumours in immature oba mice . 
 the object of the experiment was to find out whether the direct introduction of a carc~ogen into the uterine horn would be effective in inducing carcinoma of the endometrium in mice , and if so , whether the incidence of tumours could in 109 mice be influenced by hormonal factors , or by differences in technique . 
 effect of stra a higher incidence of both carcinoma and sarcoma occurred in oba than in laboratory white mice ( tables i , ii ) , in spite of the fact that all the oba mice were immature at the time of implantation . 
the difference in carcinoma incidence ( oba 40 per cent , white 149 per cent 134 ) is nearly but not quite statistically significant ( table iii ) ; that in sarcoma incidence ( oba 533 per cent , white 74 per cent 134 ) exceeds the conventional level of statistical significance . 
but when immature oba mice are compared with immature white mice ( table iii ) , then the difference in carcinoma incidence becomes significant ( oba 40 per cent , white 83 per cent 134 )  . 
above and to the right are the rectal glands and submucosa invaded by loose sarcoma tissue ; passing obliquely across the figure is the muscle of the rectal wall ; below is the main mass of sarcoma . 
 it was rather surprising that carcinoma could be induced by this means in immature mice , spayed at the time of implantation , when they weighed ll - 15 g . 
it is evident , however , that maturity at the start tended to improve the tumour yield , though it did not lower the period of induction in white mice ( table iv )  . 
 spaying had no apparent effect on the incidence of all tumours either in oba mice ( table i ) , where the numbers were very small , or in white mice ( table iv )  . 
 16 85 27 85 14 8 l 26 8 l 86 113 114 25 81 13 81 the yield of sarcomas was , however , greater in intact than in spayed white mice , though the difference was not statistically significant . 
mice which received the larger dose of carcinogen , are considered ( table v ) , it is noteworthy that the lowest incidence of tumours occurred in spayed immature mice . 
even though the numbers are small , the agreement between the three other groups in table v suggests that the lower incidence of tumours in spayed immature mice is of significance . 
it is probably comparable with the dose used by pan and gardner ( 1948 ) for the induction of tumours in subcutaneous implants ( " small crystals " )  . 
as none of these other cell types are seen in the typical rodent ulcer , the lesion must be considered as being completely undifferentiated . but such a tumour should be highly malignant , more so at any rate than the ordinary keratinizing squamous cell carcinoma . this difficulty is resolved by the more recent view , apparently a revival of krompecher 's first thoughts on the matter , which relates these tumour , not to the basal layer of the epidermis , but 214 a . 
thackray to those accessory structures of the skin derived from the surface epithelium , the haythorn ( 1931 ) for example , relates the tumours hair follicles and sweat glands . in nearly every case to existing hair follicles and matrix , regarding any connection between epidermis and tumour tissue as secondary and fortuitous . 
some workers find it difficult to reconcile an origin in the hair matrix , which is comparatively deeply situated , with the superficial situation of early tumours . but hairs have a definite life span , at the end of which they atrophy , are shed and replaced . 
the pilar type , which included about threequarters of the tumours in his series , he further subdivided into a pilar type proper , a primordial type , a cylindrical celled or " ribbon " type , and a cystic type . 
from this large number 200 cases were finally selected to form the basis of the present investigation . the selected cases were all those that fulfilled the following conditions : 1 . 
the sections available did not always include the whole lesion , but where this was so a note was made as to whether excision appeared to be complete , incomplete or doubtful . 
of the 12 cases which recurred , 8 were obviously incompletely excised , one appeared to have been completely removed from the section studied , and 3 were doubtful . of the 51 successful excisions , 42 had been removed with an adequate margin of healthy tissue , one tumour reached to the limit of excision , and 3 came so near to the edge that the outcome seemed doubtful . in the remainder the sections available did not cover the whole lesion and no opinion as to completeness of removal could be given . of the 12 failures with surgery , one was cured by further excision , and 4 more by irradiation . three of the remaining 7 died as a result of the disease , unchecked by further surgery or irradiation , 2 patients are still alive with the ulcer active , and the other 2 died of other causes with the ulcer uncured . 
of these 39 ulcers , 19 were soon cured by further treatment , leaving 20 which proved radio - resistant . it is proposed to compare the incidence of various histological features in the biopsies from the 82 lesions cured by a single course of radiotherapy with their these figures incidentally introduced incidence in the 20 radio - resistant ulcers . must not be considered as representative of the results of radiotherapy by modern methods , for it must be remembered that these cases were all followed for 10 years , the most recent treatment being therefore in 1938 . influence of size of lesion on prognosis . before considering the histological analysis of these cases it is interesting to note the influence of the size of the lesion on the prognosis . 
the greatest measurement of the ulcer in inches was noted on the cards , and these sizes were then divided into two groups , large and small , taking one inch or more as the criterion of largeness . this boundary between large and small was placed quite arbitrarily and in fact there proved to be about twice as many small lesions as large . of the surgically excised lesions , the size had been noted in 51 cases , and of these 16 were large and 35 small . 
thackray influence of type of lesion on prognosis . as has been described already , the lesions were classed on their histological appearance as being circumscribed ( group i ) , predominantly circumscribed , but with early infiltration present ( group ii ) , or infiltrative ( group iii ) in their type of growth . it was hoped that this classification might give an indication of the malignancy of the tumours without introducing controversial problems concerning their origin . it may be suggested that the infiltrative lesions are the large and advanced ones , and that any correlation we may note between type of growth and prognosis will merely be a repetition of what we saw in the preceding section . 
the whole series of surgical cases , including also those in which surgical excision was combined with radiotherapy in the first instance , was therefore grouped as to size of lesion and type of growth . 
the great majority of the lesions with no palisade formation apparent on section were of the infiltrative variety , whereas in the group with well - marked palisades 30 were circumscribed ( group i ) and 19 infiltrative ( group iii )  . 
the question of metastasis does not arise , and it is only necessary to be sure that the margin of the excised tissue is free from growth . this can be done by cutting serial sections of the excised tissue , which is well worth while if there is any doubt . if serial sections are not prepared , then the nature of the growth itself gives a fair indication , for tumours of the circumscribed type , as we have called it , are relatively compact and their extent is apparent from the surface , whereas infiltrative growths extend beyond their apparent limits . when considering the results of radiotherapy it is important to distinguish clearly between radio - sensitivity and radio - curability . 
a tumour which melts away when irradiated may often recur , whereas the tumour which can be destroyed curing the patient , may show no dramatic immediate response . in this investigation the ten - year cure is the criterion of successful treatment , so that radiocurability is all we are concerned with . it is well known that the histological grade of malignancy as applied to carcinomas of the skin , say , or breast , has some bearing on the outcome of radiotherapy - those of low - grade malignancy often being curable , those of high malignancy usually being sensitive , but recurring . in carcinomas of the breast such features as the degree of tubule formation , variability in size and staining of the nuclei and the frequency of mitoses are all significant , and are taken into account in determining the grade . 
the results of the present investigation have been largely negative , for most of the histological features of rodent ulcers considered have been shown to be without significance in assessing the probable outcome of treatment . 
thackray the presence of cysts , pigmentation , nor even the number of mitoses seem to have any bearing on the question . the only method of dividing up the tumours which seemed to bear any relation to the prognosis was that based on the habit of growth , into circumscribed or infiltrative , and the fact that an intermediate group was necessary indicates grading as practised in connection the difficulty in making this distinction . with carcinomas of the breast and elsewhere is an indication of the degree of malignancy of malignant tumours ; the term " group " has been used here rather than " grade " in view of the suspicion that many of the group i tumours are probably in actual fact benign . 
of the other histological features studied , only the extent to which growth is infiltrative seemed to have a direct bearing on the prognosis and prospect of cure by radiotherapy . my thanks are due to the surgeons of the middlesex hospital and to professor b . 
this proportion insured chrom - atograms of satisfactory color intensity . ethanol was used for the extraction because it is believed to be a solvent which causes minimum proteolysis during denaturation of protea 78 per cent , solution has been found to be optimal for solubility of the amino - acids and for the extraction of non - protein nitrogen only . a two - dimensional chromatogram on whatman no . 
new amino - acids appeared at varying intervals in each of the four tissues 'studied , and - the changes were consistent fot each tissue in ar of the rabbits studied . 
they found that muscle temperature and ph decreased with isch - aemia . proteolysis found during ischaemia may be.caused by accelerated enzyjnic degradation in a more acid medium as the optimum h of tissue cathepsins hes between 4 and 5 ( willstiitter and bamann , 1929 )  . , in any event ischaemia m , 4y alter the chemical characteristics of a tissue . 8ummaim ' the number of free amino - acids extractable from clinical cancers of similar histogenesis - varied widely , due apparently to deliberate occlusion of the arterial supply in the , course . 
bielschowsky. from the hugh adam cancer research department of the , medical school and the , new zealand branch of the british empire cancer campaign , university of otago , dunedin . received for publication december 5 , 1953 . chromophmic tumours of the pituitary are more frequent in the rat than in man . 
thus chronic thyroxine deficiency can lead to the formation of basophihc adenomata and the morphological signs of hyperoestrinism are found often in conjunction with acidophilic adenomata . when the normal level of oestrogen in the body of the female rat is raised for prolonged periods , vagina , uterus and mammary glands undergo a series of changes one of which is cystic hyperplasia of the breast . 
growth had taken place mainly in direction of the cerebellum with which the tumour was in close contact without invading uterus ( 125 mg . ) and vagina were atrophic , it . 
the kidneys had a granulated surface and the adrenals were of a slightly darker colour than normally . large fat deposits were present in subcutaneous and retroperitoneal tissues , as well as in the abdomen . 
respectively , when killed after 10 months of parabiosis . smears taken from the spayed female indicated persistent anoestrous , whereas those of the intact littermate showed the picture of continuous oestrous . 
at the post mortem the pituitary of the intact parabiont ( rat 2 ) was found to be considerably enlarged ( 139 - 3 mg )  . nodular structures protruded above the surface which showed haemorrhagic discoloration . 
the ovaries were large and cystic , of a yerowish colour and apparently free of corpora lutea . there was after removal of the capsule fluid between the capsule and the ovarian tissue . the combined weight of the ovaries was 299 mg . 
the breast glands were remarkably hyperplastic and contained large milk cysts . in sections of the pituitary normal anterior lobe tissue was not recognisable and the presence of basophihc cells could not be demonstrated by any method . the cleft separating intermediate and anterior lobes was enlarged ' and filled with 156 f . 
the great majority of the tumour cells appeared to be larger than normal chromophobes or acidophils and most of them had a very prominent golgi apparatus the negative image of which was alreadv recogni 'sable at low power . 
the frequency of mitoses varied in different parts of the tumour , but rarely more than two were seen in one field at low magnification . blood - filled sinuses and areas of haemorrhage were present in all sections and so were strands of dense connective tissue , originating from the capsule or from larger blood vessels . 
the vagina was lined by layers of stratified , squamous , keratinising epithehuthe outstanding feature of the greatly hyperplastic mammary glands were cysts filled with eosinophilic material which apparently exercised pressure on the lining epithehum , flattening it . smaller cysts were surrounded by cuboid epithelium containing secretion droplets . 
the histological examination of the breast confirmed that the changes seen at autopsy were of a similar kind in both partners as far as their secretory activity was coneemed . to recapitulate , a remarkable secretory activity was found in the breast of the ovariectomised parabiont , the uterus and vagina of which showed the typical castration atrophy . in this case the stimulus responsible for " lactation " is oestrogenic stimulation can be assumed to have come from the intact partner . excluded because of the state of pituitary , vagina and uterus of the spayed animal . at the time this observation was published we were unable to explain whv such changes in the breast were seen only occasionally in spayedanimals joined in parabiosis to an intact female . revision of the material has shown that there exists a good parahelism between the presence of a pituitary tumour in the intact partner and stimulation of the breast of the ovariectomised parabiont . 
a fortnight later vaginal smears revealed the presence of cornified unfortunately cells which remained the predominant cell type for 13 months . no smears were taken during the following 3 months , but during the week preceding death the vaginal smears were those of anoestrous . 
ar other organs appeared normal except the lungs which contained small areas of consolidation . histological investigation showed that little non - neoplastic tissue remained in the pituitary . this consisted of chromophobes and acidophils of fairly normal appearance , but the presence of basophils could not be demonstrated in the compressed rim of normal anterior lobe . 
the tumour itself consisted of atypical large acidophils which in some regions were nearly as numerous as non - granulated cells , whereas in others the latter predominated . bizarre cells with giant nuclei were a common occurrence and one or more mitoses could be found in nearly an fields . 
the glands contained follicles in various stages of development groups of pale vacuolated cells , separated by with healthy appearing ova . strands of spindle - shaped elements predominated in the stroma . in frozen section the pale cells were found to contain ample sudanophilic material . 
of the target organs of the adenohypophysis only the breast glands were found to be stimulated and of the known pituitary hormones only prolactin can cause secretion in the breasts of ovariectomised adult rats ( desclin , 1952 )  . the functional activity of the pituitary tumours of the rat is at variance with that of the acidophilic adenomata of human pathology . 
two types of acidophils can be easily distinguished in the pituitaries of several species as for instance the rabbit ( friedgood and dawson , 1938 )  . here cells with a strong affinity for carmine are found besides others which do not retain this dye . 
the former increase in numbers after coitus , towards the end of pregnancy and during the first days of lactation . in man , romeis ( 1940 ) demonstrated the presence of one type of acidophils staining red , and of a second staining yerow in azan preparations , his a and e cefls . in addition he recognised a third variety of acidophils , the q or pregnancy cers of erdheiin the rat the histological methods with which the writer is familiar unfortunately do not allow differential staining of two types of acidophils . 
why in man the growth hormone producing cells undergo neoplastic changes and in rodents the prolactin secreting acidophils , i am unable to explain . the interrelation between pituitary tumours and secretory activity of the mammary glands has been studied by lacour ( 1950 ) in the rat . in a series of 37 oestrogen induced adenomata she found in 23 granulated as well as " chromophobic " cells with a hypertrophic golgi apparatus . 
whenever the granulated elements were present , the breast had the aspect of a " lactating " gland . used romeis ' kresazan technique which stained the granulated tumour cells according to lacour a few cells , having the same tinctorial qualities orange . occur in the pituitary of the normal female rat . 
they become more numerous early in pregnancy and increase considerably in numbers 3 days ante partum . from this date onwards until weaning these ora ' ngeophil acidophils outnumber the other type . 
the close correlation between the presence of orangeophilic cells in the normal and tumourous pituitary and lactation changes in the breast suggested to lacour that these elements were the sourc ' e of prolactin . the hterature on experimental and spontaneous pituitary adenomata in rodents has been recently reviewed by horning ( 1952 ) and by gardner ( 1953 )  . in contrast to the opinion of the writer , gardner considers the oestrogen induced pituitary tumours as chromophobic adenomata , a view still shared by most admittedly , degranulated elements are more numerous in many authorities . of these tumours than granulated forms , but can - one classify all cells without granula as chromophobes ? the difficulty lies in the morphological resemblance of degranulated acidophils to chromophobes . 
the oestrogen induced pituitary growths with functional activity cannot be chromophobic tumours because the acidophils and not the chromophobes are the source of lactogenic hormone . another point of controversy is the nature of these pituitary growths . 
they are considered by some authors to be true neoplasms and conditioned growths by others , because they have been seen to regress when stimulation ceased ( nelson , 1944 )  . 
the " spontaneous " tumour described in this paper did not differ histologically or functionary from the two oestrogen mduced growths . this adenoma certainly was not dependant on oestrogen since it showed no sign of regression 51 months after ovariectomy . 
one occurred in an ovariectomised rat , the second in an intact female joined in parabiosis to a spayed partner and the third in a female treated with stilboestrol , in which , however , the histology of the vagina indicated a very low oestrogen level at the end of the experiment . the pituitary growths were found in animals having secreting mammary 160 f . 
steiner. from the university of chicago , chicago 37 , illinois , u.s.a. received for publication april 15 , 1954 . in an aae of high specialization there is a tendency to achieve understanding in oncology this by the study of progressively smaller and stif smaher units . has taken the form of going fiom caincer as a whole to its various sites and types , and from tissues to cells to intracellular components and , finaffy , to molecules . much progress has been made in this way in an understanding of the disease . this dissective analytical approach has , however , tended to divert attention from some of the larger units within individuals and in societv which are still capable of teaching much about the natural history of the disease , including its etiology . 
the endemiological approach to etiology in cancer , wbich makes use of groups of cases , appears to be neglected . the present purpose is to show by a statistical study of large bodily units , namely , organ systems , an endemiological pattem in the natural frequency of cancers that appears to have etiological impfications . 
each major body system shows a harmonious pattem in its principal tumours , different from other systems , suggesting that they have similar etiological factors . in a recent statistical study , it was found that the curves fof cancer to autopsy ratios by age were similar for all major sites in an organ system and different from those of other organ systems . 
the study was then extended to the mortality statistics of the united states , which corroborated the previous observations . it is believed that this behaviour pattern has etiological significance . necropsy data , the basic data from which the curves in fig . 
1 , and the number of cancers at each site can be found in the principal table of tlle appropriate chapters of another publication ( steiner , 1954 )  . in that material of 35 , 293 necropsies , there were 6 , 072 malignant neoplasms . 
the twenty commonest cancers comprised 91 - 3 per cent of the total . sixteen of the twenty ( omitting carcinomas of the prostate , skin , pancreas , andthe intracranial tumors because they are lone representatives of systems ) far into six organ systems . 
they form the basis for the present study . if the curves of ratios of necropsies for cancer to total necropsies in the twenty tumors are plotted together , as in fig . 
the relationships of the can ' cers appear haphazard and disorderly . however , if now the curves for each organ system are withdrawn from this melange and plotted separately , as in fig . 
an attractive order emerges from chaos . thus , the tumors of the four principal sites in the ahmentary tract which give carcinomas of the mouth , esophagus , rise to carcinomas are plotted in fig . 
2. stomach and large intestine had low mortahties early in life but they increased to a maximum in the seventh decade , after which their importance dechned in relation to other causes of death . 
the mortahty from carcinomas of the mammary glands , uterus and ovaries began in the third decade , increased quickly as cancer to necropsy ratios to a maximum in the fifth decade , and then fell . 
the peaks and general configuration of the three curves are the same , differing only in amplitude . the mortafity began soon after puberty , increased to the time of the menopause , and then fell off relative to other causes of death - more in the uterus and ovary than in breast . 
steiner peak was at least four decades later than in the feinale generative tract . mortality began in the prostate when in the female generative organs it had already reached its peak . 
the curve for the prostate shows an inverse relationship to the period of most active sexual iffe , but a direct relationship is found in the female generative system . the two principal tumours of the respira ' tory tract , free from the confusion of fig . 
except for the sman peak m renal cancers in the first decade , caused by the wilm 's tumors , the configuration of the curves is the same . there was a gradual increase with age in these cancer necropsy ratios . 
7. although mortahtv from carcinoma of the hver began earlier than from the gafl - bladder , in both it mcreased with age , and there is a similarity in the curves which is not obvious in the apparent anarchy in fig . 
the cancers of the stomach intestine ( including rectum ) , esophagus and the buccal cavity ( including the pbarynx ) had totals of 24 , 258 , 33 , 383 , 3 , 866 if cancer death to ar death ratios are made by and 5 , 138 cases respectively . decenniums or bv quinquenniums , the configurations of the curves are the same for all four - tumours and they resemble those in fig . 
cavity show a virtual plateau in the two decades 50 - 59 and 60 - 69 . in the respiratory tract , 18 , 277 cancers were reported in the ' trachea , bronchi and lung ( some unspecified as primary or secondary ) and 1 , 852 in the larynx . the cancer to death ratios show peaks in the deca - de 50 - 59 as in fig . 
4. these peaks , also , lie between those found in the alimentary tract and the female gellefative organs . similarly , the three principal cancers of the female generative organs _ ( mammary glands , uterus and ovary plus fallopian tube and broad hgament ) show curves which are similar in configuration to each other and to - those in fig . 
3 , there were reported in 1950 18 , 973 cases of with peaks in the decade 40 - 49 . cancer of the breast , 16 085 of the uterus , and 5 , 652 of the ovary , faropian tube and broad ligament combined . ln the mesoblastic series of mahgnant tumours , those of bone ( 2 , 180 cases ) showed a curve resembling that in fig . 
5 with a peak in the decade 10 - 19 , a sman depression in the decade 30 - 39 ' and a small secondary rise followed by a gradual dechne . 
the mahgnant lymphatic diseases ( code numbers 200 - 205 ; total of 16 , 756 cases ) showed a peak in the first decade forowed by a gradual decline . the ratios to all deaths were higher during the first three decades than in the los angeles material . 
the sarcomas of ar soft tissues are not combined in the u.s. vital statistics , so this category cannot be stuclied . in the ul - inary tract , kidney tuiriiors ( 3 , 643 cases ) had a maximum in the decade 50 - 59 while bladder tumors ( 6 , 401 cases ) had a peak a decade later . neither curve showed the persistent rise of fig . 
6 in the older age groups . because all tumors of the hver and biliary passages are combined in the u.s. vital statistics , comparisons cannot be made between individual sites or with fig . 
mortality figures for 1950 conform to , with minor exceptions , the same endemiological pattems as the los angeles necropsies , showing that the latter were not exceptional in this regard . it should be noted that cancer to au ' topsy ratios were used in one set of data thus , autopsies for all causes and an and cancer to death ratios in the other . deaths were used , respectively , as the points of reference . cancer to autopsy ratios may be ofhmited . 
value in expressing total quantity but they are excenent for contrasting one site with another within a material because the point of reference however , essentially the same endemiowithin each age group is the same for all . logical facts are revealed by other methods ofanalysis , altbough less clearly . thus , the age distribution figures ( steiner , 1954 ) for the cases in the los angeles necropsies show - similarities within organ systems . 
figures gave sinfflar results in so far as they were compared . thus , if the data of clemmesen and nielsen ( 1952 ) from the danish cancer registry are used , the incidence curves for cancers of the stomach , esophagus and large intestine ( who code 153.0 - 3 , 153.9 plus 154 ) are similar in configuration , as are those of the uterus and ovary but not of the mammary gland . the question arises as to wbat , if anything , these statistical findings indicate regarding etiology . are they explained by chance ? that they probably are not is shown by the absence of exception in sixteen tumor sites representing six systems in the los angeles necropsy series , a ; nd an essential concordance by most such a high degree of thirteen tumors in five systems in the u.s. 
2 to 7 that the organs in some systems develop a greater proportion of their it is not known whether this earlier cancers at an earlier age than in others . occurrence represents an earher exposure to etiological factors or a shorter tumor induction time after the beginning of the exposure . induction time isthe resultant of many factors including type , potency and amount of carcinogen , number of ca - rcinogens , conditions of exposure and susceptibifity of the cens . that differences in induction time exist in man is indicated by the exposures - to ionizing radiation in japan ( hiroshima and nagasaki ) where to date only leukemias have occurred although ionizing radiations are known to induce tumors of other types . it is also apparent from the figures that the tumor yield by sites within systems varies greatly although the induction time appears to be the same . 
tumor yield is govemed , in general , by the same factors as the induction time just mentioned . in addition the number of cells being exposed is important in deter number of tumors obtained . 
steiner organ system can , in theory , be correlated in part with the number of cells at thus , in the alimentary tract each site exposed to hypothetical carcinogens . there would appear to be , on the basis of the gross and microscopical anatomy , approximately equal numbers of epithelial cells available for neoplastic conversion in the mouth and esophagus , many more in the stomach , and still more in the this is roughly parallel to the numbers of cancers that occur large intestine . in these locations ( in 1950 5 , 138 , 3 , 866 , 24 , 258 and 33 , 383 respectively in the united states )  . similar agreements between the relative numbers of epithelial cells and tumors are found in the larynx and lung , in the female generative organs ( if one assumes that most mammary carcinomas are ductal ) , and in the mesoblastic tissues if nuclei rather than total volume are considered . 
the curves of cancer to total mortality ratios by age in thirteen common tumors found in five systems showed a harmonious behavior within each system , which differed from that of other systems . some case distribution and some incidence data show the same statistical facts although less clearly . the etiological significance of these endemiological observations is unknown . however , it is suggested that they could be interpreted as signifying common etiological factors within each system with the differences in quantity in tumor by sites accounted for in part by the unequal numbers of cell populations at risk . comments are made about the interpretation of the quantitative differences in tumors between organ systems and in their age distribution . the author is grateful to the research committee of the los angeles county hospital staff for permission to study their material and to e . 
8. - hormonally - induced hyperplasia on anterior edge of pectoral fin showing an early translucent appearance of tumour produced by my ' xomatous change in stroma . of the mucus - secreting epithelium and a myxomatous change in stroma . 
pda was all rats received greens once ' %eekly . added in a concentration of 0 - 06 per cent . the diet and water were given ad libitum . twenty of 50 rats r ' eceiving this diet served as controls , whilst the remaining 30 rats each received - a daily addition of 10 ml . 
in two of the tumours ( rat ca 801 on the pda control diet and rat cl 917 receiving fresh milk ) pancreatic tissue was recognized and the origin of the tuniours . 
he describes these extraas being similar to reticulo - sarcomas or " composed of spindleordinarv tiimours shaped cells and multi - nucleated giant cells . as another deviiation some tumour cells . 
grouped in bulbous masses , show an evident tendenev to concentiric arrangement of cells which are more or less keratinized towards the centre sin - tilar to ordinarv squamous cell epithelionias . " the hver of rat cl 912 was infiltrated , %ith tumour cells . over the two - vear period in which the semi - synthetic diet was used , some 150 rats receivmg this diet without the addition of pda have been dissected . during this period carcinomas of the no pancreatic tumour was encountered . small intestine were found in three piebald and in one albino rat . in the present series of 50 rats fed pda one gimilar intestinal carcinoma was found . 
tumours not localized in the liver have not been observed previously , partly because of the preference of the compound for the liver and partly because experiments in which the liver has been protected ' were terminated too early for ttimours to develop elsewhere . whether or not the substances in the diet which defer or prevent tlle produetion of hepatic tun ' iours by feeding pda are really anticarcinogenic or only protect the liver has been questioned . it seems that in the case of milk at any rate only the liver is protected from the carcinogenic activity of pda , and that tumour development generally is not prevented . it is remarkable that the extra - hepatic tumours should arise in an intestinal gland , and this seems to siiggest that organs which might be connected with the metabolism of pda are attacked . the conception that milk has a protective action on the liver only is interesting in ' view of the general plan of these experiments , the object of which was to find , if possible , an explanation of the prevalence of hepatic tumours in the natives in it might be assumed that the effect of a careinocertain parts of africa and asia . - genic factor which produces hepatic tumours , given a certain set of dietary habits and environmental conditions can be modified when the conditions differ . 
as a differerit method of approach , studies are in progress on the antagonisation of the antimitotic action of tetra - sodium 2 - methyl - 1 : 4 - naphthohyd - roquinone diphosphate ( compound 1 ) by nucleotides , nucleosides , purines and pyrimidines and some other compounds ( mitchell , 1950 , 1951 )  . this paper is an account of the cytological effects of a series of 29 selectect 318 j . 
marrian. details of preparations have been published as follows : compounds 11 and iv ( friedmann , marrian and simon - reuss , 1948a ) , compounds xx - xxiii ( friedmann , marrian and simon - reuss , 1948b ) , compounds viii , ix and xxiv ( friedmann , marrian and simon - reuss 1952a )  . we are indebted to f . 
the cytological effects are considered in relation to those of compound 1 . of especial interest from the point of view of the selection of compounds as possible therapeutic radiosensitisers is the appearance of mitotic abnormalities in concentrations which produce mitotic inhibition without gross toxic effects on the resting cells . 
the most important abnormalities studied are chromosome fragmentation , anaphase bridges , metaphase chromosomes with regions of impaired stainabihty and with irregular and beaded structure , metaphases with clumping of the chromosomes , arrested metaphases and other spindle abnormalities , of which many of the types described by barber and callan ( 1943 ) have been noted . 
as already discussed ( mitchell and simonreuss ' 1952 ) , it seems likely that the most relevant cytological abnormalities are chromosome fragmentation , anaphase bridges and chromosome aberrations in examples of the various types of cytological effects observed with this general . series of compounds are show - n in lb ' ig . 
on the basis of the concentration required to procluce 50 per cent mitotic inhibition , hydroquinone diphosphate ( xvi ) is about twice as active as hydroquinone ( xv ) , but the increase of mitotic inhibition with concentration is much more rapid in the case of the former than with the latter . 
somewhat sirnilarly , for 50 per cent mitotic inhibition , phenyl phosphate ( xviii ) is more active than phenol ( xvii ) by a factor of about 20 , but the increase of mitotic inhibition with concentration is much less rapid in the case of phenyl phosphate than for phenol . the only exception so far to the finding of increased antimitotic activity on phosphorylation is in the case of resorcinol . friedmann and simonreuss found that 50 per cent mitotic inhibition is produced by resorcinol at 6 x 10 - 8m concentration but by resoreinol diphosphate at about 5 x 10 - 7m . - kt these concentrations both compounds showed few abnormal mitoses . the usual increase in antimitotic activity on phosphorylation is not associated with any change in character of the cytological effects . 
the frequency of cytological abnormalities appears to be of the same order for the phospborylated and non - phosphorylated compound at concentrations which produce the same mitotic inhibition . ( 2 ) methyl group . the methyl group plays an important part in modifying the biological action , especially from the point of view of practical applications . moreover , among methyl derivatives , the limitations of the use of mitotic inhibition as a sorting test are emphasised . in the chick fibroblast cultures , compound 11 is more active than compound i as a mitotic inhibitor by a factor of about 1000 , and it also shows potentiation of mitotic inhibition in combination with x - rays . however , compound ii appears to be ineffective as a radiosensitiser for the jensen rat sarcoma , and did not produce a focal reaction in the tumour after intravenous injection in a few it may be mentioned that its use in man in high doses may be cases in man . undesirable because of the possibility of induction of cataract , analogous to the experimental naphthalene cataract in rabbits ( boume , 1937 )  . it is of interest to compare the methyl free compound 11 , tetra - sodium 1 : 4 - naphthohydroquinone diphosphate , with the 2 - methyl derivative , compound 1 , and with the 2 : 3 - dimethyl derivative , compound xxviii . 
no other compound examined showed this behaviour . compound 11 showed an increase in the number of metaphases by a factor of about 2 - 5 on increasing the concentration for 50 per cent mitotic inhibition by a factor of io . it bas been show - n in the preceding paper ( mitcher and simon - reuss , 1952 ) that compound i is somewhat unstable in aqileous solution in the absence of oxygen at 39 ' c . 
one may speculate and suggest the possibihty of combination of the phosphates with arginine side cha ' ms of histones the chromosome structure . biological action of 2 : 3 - dimethyl - 1 : 4 - naphthohydroquinone diphosphate , tetrasodium salt ( compound xxviii )  . - the biological action of compound xxviii differs considerably from that of ar the other c ' , ompounds . 
even in concentration 2 x 10 - 6m ( though not at 5 x 10 - 7m ) , which produces no detectable mitotic inhibition , there is metaphase accumulation by about 50 per cent above the fraction of metaphases in the controls , together with spindle abnormalities . as an example of the frequency of relevant chromosome aberrations , it will be seen from table iii that after application in concentration 4 x 10 - 6mfor 24 hours , out of 534 cells in mitosis , there were 74 cells in metaphase showing chromosome fragmentation and 17 anaphase bridges . it appears that with compound xxviii there is more rejoining of chromosome breaks than with moreover , compound xxviii only any of the other compounds examined . starts to show effects on resting cells in high con ' entrations associated with almost complete mitot - ic inhibition ; this behaviour suggests low toxicity . detailed studies of the combination of the effects of compound xxviii and x - radiation on the chick fibroblast cultures have been made by the summation method . 
the results of one experiment are given in table iii . it is concluded that under the experimental conditions , the combination of the action of compound xxviii and of x - radiation shows potentiation of mitotic inhibition and that the mechanism of action of the two agents is different . ( 3 ) carboxyl group . the compound most closely resembling compound xxviii in biological action is compound xi , the hexasodium salt of 1 : 4 - dihydroxy - 2 : 3 - naphthalene dicarboxylic acid diphosphate . replacement of the methyl groups in the 2 and 3 positions in compound xxviii by carboxyl groups slightly reduces the activity as measured by mitotic inhibition and considerably reduces the metaphase effects , so that at 50 per cent mitotic inhibition there is metaphase accumulation by about 25 per cent and sphadle abnormalities are much less frequent . 
compound vi produces clumped metaphases with some chromosome fragmentation and many undivided telophases , but practically no anaphase bridges . metaphase accumulation appears at a concentration which produces about 70 per cent mitotic inhibition ; this is associated with negligible effect on resting ceus . the weak metaphase arrest with compound vi is perhaps associated . 
simon - reuss 5 - methyl - 4 : 7 - thionaphthene quinone ( xxvii ) is active when tested in solution in cerosolve and gum ghatti , and produces 50 per cent rnitotic inhibiti ' on m approximately 5 x 10 - 6m concentration . 
mitotic inhibitor than compound ( xiv ) by a factor of 2 , but produces metaphase accumulation and abnormal mitoses , mainly clumped metaphases , chromosome fragmentation and multipolar cells , at all concentrations showing mitotic inhibition . the tetra - sodium salt of hydroquinone diphosphate ( xvi ) is a very active compound , and produces 50 per cent mitotic inhibition at almost exactly the same concentrat - ion , 3 x 10 - 9m , as does compound il in this region of concentratioin it also produces few abnormal mitoses . 
simon - reuss variably increased by phosphorylation , often by a factor of 5 or more . these results and those with dinitrophenol suggest that blockage of the entry of cells into mitosis depends upon inhibition of synthetic processes mvolving phosit is interesting that from the non - protein moiety of a phosphorylation . phorylase has been isolated a yellow pigment tentatively identified as 2 - methylit seems unlikely that at the concentrations 1 : 4 - naphthoquinone ( buell , 1952 )  . used there is interference with glycolysis ( gemmill , 1949 )  . the comparison of the cytological effects of different compounds of closely related chemical constitution and also of ionising radiations makes it possible to separate some of the main types of mechanism of action of these agents on proliferating cells as follows : ( a ) blockage of the entry of ceus into mitosis , without specification of the exact time of the action and presumably including pre - prophase and antephase this is the characteristic action of compound 1 , and in this case is inhibition . other less clearly associated with relatively few chromosomal abnormalities . defined examples are compounds x and xv . ( b ) metapbase arrest and disturbances of the spindle mechanism apparent - ly examples of this type of action in association similar to the effects of coichicine . with ( a ) are compounds 11 , vi , viii , xi , xxvii and xxx at the higher concentrations , compound ix at low concentrations and compound xxviii iso - naphthazarin produces metaphase over a wide range of concentrations . arrest with little or no inhibition of the entry of cells into mitosis . ( c ) chromosome , including chromatid , brea - kage - with varyina degrees of rejoinability of the broken ends . 
these experiments suggest that the tetra - godium salt of 2 : 3 - dimethyl - 1 : 4naphthohydroquinone diphosphate , compound xxviii , is the most suitable compound for further investigation as a possible therapeutic radiosensitiser . in addition to the help acknowledged in the text , e . 
wiltshire. from the biochemical liaboratory , university of cambridge . received for publication january 22 , 1953 . in 1939 k6gl and erxleben ( 1939a ) published the first of a series of papers it was on the optical configuration of amino - acids in proteins from tumours . found that the optical rotations of some amino - acids , which had been isolated by the classical methods and purified by recrystallisation , did not correspond with it was concluded that the preparations contained the values in the literature . the " unnatural " d - isomer in addition to the " natural " or l - isomer . 
the calculated proportion of d - isomer was largest in serine and glutamic acid . authors considered that serine had probably been partly racemised during hydroglutamic acid on the lysis of the proteins or during subsequent purification . glutamic other hand was considered resistant to racemisation in acid solution . acid from normal tissues and benign tumours had the specific rotation [ a ] 200d + attention was directed to this apparent difference in the optical form 31 - 60 . of glutamic acid from malignant and non - malignant tissues , which promised to be a lead to the long - sought chemical difference between normal and neoplastic tissue , and one that could be used for diagnostic purposes . 
a theory of malignity was proposed ( kogl , 1939 ) depending on the inability of most peptidases to hydrolyse peptides of d - amino - acids . the experiments of kogl and collaborators were repeated in many other laboratories with variable results , which on the whole showed smaller amounts of d - isomer than had been found by kogl . 
the considerable controversy which developed between different schools was suspended by the recent war , but dodds and dickens ( 1940 ) had already concluded from a review of the results then available that the appearance of the d - isomer of glutamic acid was not characteristic of since the war further work by kogl , barendregt and klein tumour tissues . ( 1948 ) and kogl ( 1949 , 1950 ) has renewed discussion of this problem . indirect evidence was produced in support of the original hypothesis . it was decided to limit the present study to the problem of whether or not the d - isomer is found in protein hydrolysates , and if so whether it exists as such in the proteins or is an artifact . 
a similar study using different methods ( boulanger and osteux , 1950 ) has appeared since the experimental work was completed . preliminary experiments ( wiltshire , 1953 ) showed that glutainic acid is racemised to the extent of about 5 per cent in the preparation of protein hydrolysates . 
found for calf lung protein total glutamic - n equivalent to 5 59 per cent and the l - isomer to 554 per cent of the protein - n compared with the present 5 69 per cent and 5 49 per cent respectively . for the carcinoma of the bronchus they found 6 * 40 per cent and 6 29 per cent both methods compared with the present 6 * 23 per cent and 6 29 per cent . therefore would appear to account for all the glutamic acid ofthe proteins . this is of some importance , since in much of the earlier work involving purification of the amino - acid for polarimetry a very small proportion of the total glutamic acid was finally isolated and analysed . 
the same criticism may be made ofthe aluminachromatographic methods of wieland ( 1942 ) and boulanger and osteux ( 1950 ) , where only 70 to 80 per cent of the original glutamic was recovered . 
the isolation of a small and unrepresentative sample may account for the discrepancy between the results of experiments by graff , rittenberg and foster ( 1940 ) and wieland and paul ( 1944 ) , who , using n15 - labelled glutamic acid , could find only 2 to 5 per cent d - isomer in the glutamio acid from tumours , and by k6gl , erxleben and van veersen ( 1943 ) , who with deuterium - labelled glutamic found over 20 per cent . 
the latter experiments have been criticised on other grounds by rittenberg and shemin ( 1946 )  . soon after the discovery of d - amino - acids in tumours several workers tested the activity of d - amino - acid oxidase from kidney on hydrolysates of tumour and other tissue proteins . 
among others k6gl , herken and erxleben ( 1940 ) ; lipmann , behrens , kabat and burk ( 1940 ) ; lipmann , hotchkiss and dubos ( 1941 ) ; arnow and opsahl ( 1940a , 1940b ) and boulanger ( 1944 ) could find no d - amino - acid in whole hydrolysates by this means . 
the percentage of d - glutamic acid found was in all cases very small , and not more than would be formed by inversion of the l - isomer during hydrolysis . i wish to thank b . 
holmes for the jensen sarcomata , the bland - sutton institute of pathology , middlesex hospital , london , for the liver metastases from a case of carcinoma of the colon , and professor f . 
with the advent breast cancer . of x - rays the same effect was brought about by ovarian irradiation ( foveau de courmelles , 1926 ; ahlbom , 1930 )  . on the experimental side , the work of lathrop and loeb ( 1916 ) , loeb ( 1919 ) and murray ( 1928 ) demonstrated the part played by the ovary in the production of mammary tumours , while lacassagne ( 1932 ) showed that , in certain circumstances , mammary carcinomata could be induced by the injection of oestrogenic substances . interest in the problem was further stimulated by the work of huggins and hodges ( 1941 ) on the treatment of carcinoma of the prostate by castration and stilboestrol . it was logical that the next step in the management of advanced breast testosterone propionate was cancer in women should be the use of androgens . tried with success by ulirich ( 1939 ) and by many later workers . the treatment of women suffering from breast cancer with one of the oestrogen preparations was apparently illogical , although zondek ( 1936 ) had put forward the suggestion in 1936 . 
they are rare , however , and in over 4000 cases of breast cancer observed in this department no spontaneous regression has so far been noted . the survival rate will be mentioned in the groups of cases to be considered and , although it seems that life can be prolonged with hormone treatment , no attempt is made to claim success on this account alone . the responses were graded as follows : a . 
good responses were seen in all types of metastases , skin nodules , glands , pulmonary and skeletal in 3 patients with osteolytic bone metastases there was radiological metastases . evidence of new bone formation . in 4 a pleural effusion disappeared and in 4 it diminished in amount . 
5 illustrates the findings on 9.x.46. patients treated by surgical castration and testosterone . in 1941 a small group of patients was treated by surgical castration , accompanied by the administration of testosterone . this was done in an attempt to find out why there were some failures with ovarian irradiation . it was thought that ovarian function might recover to some extent after irradiation and that the effect of o6phorectomy would be more lasting . nine patients with advanced breast carcinoma were treated in this manner by o6phorectomy , followed by daily intramuscular injections of 25 mg . 
testosterone propionate for periods up to 3 months . only one patient showed a slight response . she was a premenopausal woman of 40 with an inoperable breast carcinoma and bone metastases . 
the primary tumour became smaller and the glands disappeared temporarily , but no effect was noted on the skeletal metastases . patients treated by oestrogen therapy . in the latter part of 1942 it was decided to investigate the value of oestrogens in advanced breast carcinoma , and since that time the following oestrogens have been tried : stilboestrol dipropionate , dienoestrol , triphenylchlorethylene and ethinyl oestradiol . 
twice a day sometimes caused sufficient water retention to increase the pleural effusion and add to the patient 's dyspnoea . it was remarkable to find in a few such patients that doses as small as 0 ' 5 mg . 
the number of patients having no symptoms attributable to the hormone while taking stilboestrol was 122 , while many of the remainder had symptoms which did not inconvenience them greatly , the most common being nausea and vomiting at the commencement 36 maryidouglas of treatment . 
even pleural effusions dimished in amount , and in 3 cases disappeared altogether with no treatment other than stilboestrol dipropionate . it is also very interesting to note that in this series 13 patients with bone metastases experienced relief from pain , while in 6 , new bone formation was demonstrated radiologically in osteolytic lesions . 
no post - mortem was carried out , but this gastric tumour was probably metastatic in nature from the carcinoma breast . the following case illustrates the improvement which may take place in a patient with a pleural effusion : ca8e no . 
of testosterone propionate daily , given intramuscularly . treatment was continued for 3 to 4 weeks , and if the patient 's condition showed some improvement , further treatment was given either by means of an implant of 400 to 600 mg . 
one patient who was comatose with cerebral metastases improved sufficiently under treatment with testosterone to subsequent post - mortem examination confirmed attempt crossword puzzles . the presence of large intracerebral metastatic deposits , which presumably had regressed only temporarily under the influence of testosterone . in another patient a large pleural effusion did not cause any further respiratory embarrassment , and required aspiration only at increasingly longer intervals . this patient is still alive 25 months after the commencement of treatment . only one patient experienced relief of pain from skeletal metastases while another patient with metastases in bone stated she receiving testosterone . felt the pain easier when the drug was withdrawn . there was no radiological evidence of repair occurring in bone metastases . 
the series , although small , is in this respect at variance with the results so frequently reported in the literature ( adair et al . , 1949 ; kaae , 1949 ; report of the council on pharmacy and chemistry , 1949 )  . only one patient could not tolerate the drug . she was a woman of 43 with cerebral metastases , who developed very severe vomiting , and treatment had to be discontinued after she had received 150 mg . apart from this one patient no one was upset by treatment . 
treatment was also given to post - menopausal women to determine the effect . many of these patients had already failed to respond to other methods of hormone therapy , and they were beyond the aid of all other forms of treatment . the pituitary was irradiated by two opposed fields , each 6 x 8 cplaced in the temporal region , and a dose of 3000r was delivered in 3 weeks to the region of the sella turcica . a series of 37 patients was treated between october , 1949 , and october , 1950 , and the results are shown in table vi . as will be seen from table vi , only 2 patients showed a good response . 
the recurrence had become flatter for 3 months , but after that had spread again . following pituitary irradiation complete healing took place slowly , but new nodules appeared 10 months later . of the 2 women showing a fair response , the first was aged 46 and premenoshe had a skin recurrence on the chest wall within the irradiated area pausal . and was treated by pituitary irradiation in december , 1949 . slight regression of the recurrence was noted for 3 months , but then the disease became widespread and she died on 6 . 
none had shown any response to the other types of hormone treatment . it would seem from this that pituitary irradiation may be of value in the tylie of case suitable for ovarian irradiation , or in cases where ovarian irradiation has already been given with some good temporary effect . there is no doubt that pituitary irradiation was the least well tolerated of all fourteen patients were very upset by the treatment it is possible that a modification of technique forms of hormone therapy . before the course was completed . and dosage would overcome some of these difficulties . of the 37 patients , 21 have died within one year , the average survival being 2 to 9 months after the commencement of treatment . 
no good results were seen in bone lesions apart from relief of pain in 2 cases , although , of course , the series was small , and treatment may not have been continued over a long enough period . the reports in the literature on the efficacy of testosterone are very variable . farrow ( 1944 ) noted a deleterious effect in female patients , nathanson ( 1944 ) observed no effect at all , and various later workers ( adair , 1947 ; adair et al . , 1949 ; kaae , 1949 ) reported a proportion of good responses in skeletal and extra - skeletal all are agreed that testosterone may produce a beneficial effect metastases . on the general health but this is a non - specific effect , and due partly to the stimulating effect of the hormone on protein metabolism . it is , however , important not to assess improvement in general health as an anti - carcinogenic effect . with both oestrogen and androgen therapy some responses were noted here after the drug was stopped - a withdrawal response . farrow ( 1944 ) also noted this occasionally in the metastases after withdrawal of either oestrogens or androgens . consideration of the mode of action of hormone therapy . wvhile hormone therapy is widely employed , the basis of treatment remains largely empirical . the extension of our knowledge of the exact mode of action would be of great interest , and might result in further advances in this form of therapy.. 
the clinical results obtained , however , appear to be due to some modification of the endocrine status of the patient . for example , in a young patient who has not reached the menopause , oophorectomy or ovarian irradiation causes a sudden withdrawal of the natural ovarian hormones which influence the rate of growth of the cells of breast tissue whether these cells are normal or malignant . 
at this stage of our knowledge , however , it is doubtful if it would be justifiable to use a higher dosage . the administration of an artificial oestrogen again modifies the endocrine status . 
the oestrogens may produce a direct effect on the breast cancer cells , or the effect may be obtained indirectly through the anterior pituitary . if the action is a direct one , the best results would be expected in older women . tn an older patient , for example a woman who is 5 or more years past the nmenopause , there is little or no circulating oestradiol , and the addition of oestrogens produces a change . after the passage of time , however , the body , and in particular the breast cells , may become readjusted , and this might explain why the good effect passes off . the work of zondek suggests that the oestrogens may have an indirect effect through the anterior pituitary . 
zondek ( 1936 ) found that the administration of large doses of oestrin produced a chromophobe adenoma of the pituitary in male rats , that is , in rats not normally subject to the action of large amounts of oestrogen . zondek ( 1947 ) also reports a case in which he gave large doses of oestradiol benzoate to a woman of 216 with metastases from a carcinoma breast . 
the increase in size of the pituitary was due to an eosinophil adenoma . unless the production of an adenoma of the pituitaryr interferes with the output of other hormones the explanation is not very satisfactory in older patients . in a premenopausal patient , a drug such as stilboestrol may cause inhibition of the gonadotrophic hormones , so suppressing natural ovarian secretion , but castration could not be said to be complete not bringing about a true castration . consewhile an artificial oestrogenic substance is circulating in the blood . quently , there is not the same profound change in the endocrine status and no useful therapeutic effect is produced . the question of the administration of testosterone might now be considered . in a premenopausal patient this brings about an artificial menopause and , from this point of view , testosterone might be expected to produce similar results to ovarian irradiation or o6phorectomy . in addition to this , the administration of testosterone must disturb the normal oestrogen - androgen ratio . finally , testosterone , like the oestrogens , causes inhibition of the gonadotrophic hormones of the anterior pituitary ( moore and price , 1932 )  . it may , therefore , like the oestrogens , produce an indirect effect on the breast cells by a disturbance of pituitary function . an explanation must now be sought for the failures . 
how this would affect the response is not known exactly , but it is perhaps significant that few patients with clinical evidence of liver involvement showed any response to any of the methods of treatment mentioned . there may , however , be other factors modifying the response . 
haddow , watkinson and paterson ( 1944 ) suggested that the tumour called " carcinoma of the breast " might in reality comprise walpole and paterson ( 1949 ) also made the same suggestion , several categories . even going so far as to say that a tumour might produce an " anti - hormone " or inhibitory factor antagonising the action of the oestrogen . 
of advanced breast carcinoma treated by hormone therapy has been surveyed and the results obtained have been presented . the findings suggest that , in premenopausal wonmen , the treatment of choice is ovarian irradiation , which was found to produce beneficial results in 30 per cent of patients in this category . in women who are 5 or more years past the menopause , oestrogen therapy would appear to be the most satisfactory form of treatment . the drug found to be most generally useful was stilboestrol dipropionate 5 mg . 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene into the flank and below a nipple in strain street mice ( rask - nielsen , 1948 )  . in both sites the injection induced only spindle - cell sarcomas and , in a few instances , squamous - cell carcinomas , but no mammary carcinomas . 
the ratio of cases of isolated thymic tumours to cases of generalized leukaemia was found to be 1 : 1 following injection into the flank and 1 : 5 following injection into the mammary region . 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene were performed . the leukaemic manifestations induced have been described in detail in a recent publication ( rask - nielsen , 1949 ) and the local tumours will be dealt with in the present paper . for the purpose of ascertaining whether the failing development of mammary carcinoma might be a phenomenon specific for injection of 9 : 10 - dimethyl - 1 : 2benzanthracene , mice of strain street were injected with 05 mg . 
of a mixture of the same hard and liquid paraffin as used in the analogous experiments with 9 : 10 - dimethyl - 1 : 2 - benzanthracene ( rask - nielsen , 1948 , 1949 )  . 
an equal number of females and males were injected into the flank , but only female mice were injected into the mammary region , except in a few 9 : 10 - dimethyl - 1 : 2benzanthracene experiments , where an equal number of each sex was used . more than half the experiments were carried out with litter mates , one half of each litter being left untreated as a control group . 
rask - nielsen sarcomas of a varying degree of differentiation ; a few were polymorphocellular , and a few rhabdomvosarcomas occurred . in the squamous - cell carcinomas marked cornification was a frequent finding ; no microscopic changes indicated that the growths might have originated in mammary tissue . 
however , the growths were considered to be most probably spontaneous and were , therefore , not included in table iii . following injection in the flank , spindle - cell sarcomas were induced by benzpyrene , dibenzanthracene , methylcholanthrene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 27 per cent , 50 per cent , 39 per cent and 12 per cent of the effective total of mice respectively . squamous - cell carcinomas were observed in the same experiment in 6 per cent , 7 per cent and 0 - 8 per cent following the injection of benzpyrene , methylcholanthrene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene respectivelv . 
as regards the application into the mammary region , spindle - cell sarcomas were observed following injection of benzpvrene , dibenzanthracene , methvlcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 4 per cent , 22 per cent , in this experiment , squamous - cell 37 per cent and 8 - 3 per cent respectively . carcinoma was observed in 2 per cent , 2 per cent , 22 per cent and 2 - 4 per cent respectively . the effective total of experimental mice is the number of mice living to be as old as the youngest tumour - bearing mouse , namely 4 months . the minimum , maximum and average latent period , the interval from the injection until death , is presented in table iv . 
the higher carcinogenicity of methylcholanthrene than of the other hydrocarbons apparent from the present experiments accords with previous findings ( greenstein , it accords also with the recent observation ( rask - nielsen , 1950a ) that 1947 )  . subcutaneous application of 0 - 02 mg . 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene was followed by leukaemic manifestations in 20 - 4 per cent with an average latent period of 20 to 25 weeks ( rask - nielsen , 1949 ) , injection of dibenzanthracene and methylocholanthrene had no accelerating effect on the development of leukamia , and the doubtful , extremely faint acceleration observed following injection of benzpyrene affected at any rate only the incidence ; not the latent period . the absence of leukaemic lesions following injection of the three last - mentioned hydrocarbons is all the more remarkable , as the development of leukaemia has been found to be accelerated following painting with benzyprene in dilute brown mice ( morton and mider , 1941 ) and in strain f mice ( kirschbaum and strong , 1942 ) following painting with dibenzanthracene , without , however , decreasing the latent period in strain f mice and with methylcholanthrene in strain f mice ( kirschbaum and strong , 1942 ) , in dilute brown mice ( mider and morton , 1939b ; morton and mider , 1941 ; lefevre , 1945 ) , in strains rf , and rf / ak ( mcendy , boon and furth , 1942 ) , in c3h mice ( kirschbaum , strong and gardner , 1940 ; morton and mider , 1941 ) , and in old and new buffalo mice painting with 9 : 10 - dimethyl - 1 : 2 - benzanthracene ( morton and mider , 1941 )  . also accelerated the development of leukaemia in aka mice ( engelbreth - holm and lefevre , 1941 ; lefevre , 1945 ) , in dilute brown mice ( engelbreth - holm and lefevre , 1941 ; law , 1941 ) , and in swiss mice ( law , 1941 )  . 
into the lung ( rask - nielsen , 1950a ) , and by the induction of only microscopically visible adenomas in mice , 4 - 11 months of age , injected with 05 mg . 
of benzpyrene , dibenzanthracene , methylcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene into the flank of strain street mice induced local spindle - cell sarcoma in 27 per cent , 50 per cent , 39 per cent and 12 per cent ; and squamous - cell carcinoma in 6 per cent , 0 per cent , 7 per cent and 0 - 8 per cent respectively . injection of the same hydrocarbons into the mammary region induced spindle - cell sarcoma in 4 per cent , 22 per cent , 37 per cent and 8 ' 3 per cent and squamous - cell carcinoma in 2 per cent , 2 per cent , 22 per cent and 2 - 4 per cent respectively . local mammary carcinoma was not induced . leukaemia developed following subcutaneous injection into the flank and into 132 r . 
rask - nielsen the mammary region of benzpyrene , dibenzanthracene , methylcholanthrene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 6 - 7 per cent , 1 - 2 per cent , 0 per cent and 20a4 per cent respectively . 
on the other hand the quantity necessary to induce abdominal fibroids is not much above the mentioned hysterotrophic dose ; abdominal fibroids can be induced by three injections per week of 5 lg . 
of oc - oestradiol , or even less , when administered as the 17 - caprylic ester of a - oestradiol , which is absorbed so slowly that a continuous oestrogenic action is made possible ( lipschutz , bellolio , chaume and vargas , 1941 )  . similarly a few micrograms of free oc - oestradiol or oestrone absorbed from a subcutaneously implanted tablet also are sufficient to induce fibroids ( lipschutz , thibaut and vargas , 1942 )  . 
on the contrary , quantities about a hundred times greater are necessary to elicit the same tumorigenic abdominal reaction if administered by subcutaneous injections of the free hormone ( lipschutz et al . , 1939 , 1942 )  . in the present work we shall deal with abdominal fibroids induced by extremely small quantities of estrogens and with the neoplastic action of these quantities on the uterine glands in experiments of long duration . fibromatogenic action of very small quantities of x - oestradiol and of oestradioldipropionate . tablets weighed 33 to 35 mg . 
each. tablets consisting of one part of the oestrogen and 19 parts of cholesterol merck were prepared in the usual way by mixing , dissolving in ether , drying and after drying in vacuo they mixing again . were implanted beneath the skin into castrated female guinea - pigs weighing 380 to 480 g . uterine and other abdominal fibroids were elicited under these experimental conditions ( riesco , 1942 ) , though the incidence was less than with the injection of great quantities of oestradiol administered as the benzoic ester , as in the experiments of iglesias ( 1938 )  . necropsy was made 112 to 118 days later . during necropsy , cleaned and dried subsequently . absorption was calculated from the loss of weight of the tablets recovered calculation was made under * this work has been aided by a grant from the jane coffin childs memorial fund for medical research , grant administered by a . 
the result of these experiments is given in table i . as seen from table i , tablets containing originally 5 per cent of the free cx - oestradiol and remaining for about 4 months in the body of a guinea - pig produce anew oestrogenic and fibromatogenic actions when reimplanted into another guinea - pig . the same result was observed when 4 months afterwards the tablet was implanted for a third time and a fourth time . there was in all these experiments opening of the vagina , growth of the nipples and uterine bleeding . 
should there have been selective absorption , oestrogenic hysterotrophic and fibromatogenic actions or uterine bleeding would have been impossible , in any case , in the third and fourth implantation . 
were obtained for the first 4 months . it is remarkable that in successive implantation smaller figures were obtained . allowance must be made for entering of substances into the tablet as has been shown by different authors ( bishop and folley , 1944 ; deanesly and parkes , 1943 )  . absorption was most probably greater than indicated by figures in our table i . 
but it can easily be demonstrated that daily absorption of oestradiol was certainly less than about 3 to 4 , g . in these experiments the total quantity of oestradiol in the tablet was never more than 1750 , g . , and the tablet remained beneath the skin during 470 days without exhaustion of the oestrogen . 
but in the next paragraph we shall mention experiments in which similar tablets were active for a total of 675 days without the oestrogen being exhausted . histological examination of the uterus in the mentioned animals revealed pronounced cystic glandular hyperplasia of the endometrium , polypous proliferation of the latter , thickening of the vaginal wall and proliferation of mammary these statements coincide with what has been formerly observed with tissue . the prolonged action of estrogens in this department . neoplastic action of small quantities of oestrogens on the uterine glands in experiments of long duration . in the above - mentioned preliminary experiments evidence was given that by continuous absorption of very small quantities of oestrogen , certainly less than 3 to 4 ug . 
fibromatogenic action was rather less pronounced than with the free hormones . but with the fibromatogenic action of oestrogens due allowance has to be made for variation . in the second series in which tablets already used in the first one were again implanted and left in the body for no less than one and a half years , uterine growth was considerable . uterine fibroids were also induced . microscopical examination of the uterus revealed in the series of long duration a condition fundamentally different from that seen at four months ; there was besides cystic glandular hyperplasia of the endometrium also proliferation of glands infiltrating the myometrium , reaching the serosa and even perforating it . the lumen of the proliferating and infiltrating glands was sometimes cystic , sometimes small or absent . 
the neoplastic and infiltrative growth of the glands was , in lipschutz ' experiments with ovarian fragmentation , coincident with those we have described in the last paragraph , with the exception that with ovarian fragmentation the invading glands did not reach the serosa and did not perforate it , as was the case in one of our animals . 
a guinea - pig having been injected for 8 months with oestradiol benzoate was found , 4 months later , to have a " precancerous " transformation of the endometrium in the upper third of the uterine horn . this latter observation of lipschutz and others is so far the only one which may be quoted in favour of irreversible atypical proliferation of the uteririe mucosa elicited in the guinea - pig by oestrogens and persisting after the withdrawal of the hormone . neoplastic malignant growth seems to be more easily elicited in the cervix of the uterus in the mouse , as shown by the work of gardner and others ( gardner , allen , smith and strong , 1938 ) and allen and gardner ( 1941 )  . in the work of these authors the oestrogens - - the benzoic ester of oestrone and oestradiol were given by injection . 
the quantities injected were , when calculated per gram of body weight in the work of the american authors with mice , probably 20 times greater than in our work with guinea - pigs . another interesting aspect of our work may be mentioned here . 
daily , add the remainder received twice this dose . table i shows the result of this experiment on the group receiving the lower dose level ; the treated tumours were completely inhibited . 
smar nodules persisted in the majority of these animals without change for about 2 weeks , after whicb tumours began to grow ; they were well developed in 70 per cent of the group 1 month after cessation of treatment . 
i and it seems reasonable to suppose that the same applies to all such tumours developing from inhibited nodules . when drug treatment was commenced 3 - 5 days after transplantation , both the sensitive walker tumour and its refractory derivative were always actively growing . 
the growth of the derived tumour was affected to a reasonably consistent extent by triethylene melamine , comparable to that observed with the lymphosarcoma . the subsequent development of inhibited walker tumour nodules has been surprisingly , growth was found to occur after a similar repeatedly confirmed . latent period in the majority of animals even though drug treatment was continued 340 h . 
ad example of this is shown id table iv , from wbich it is evident that tumours developed in 8 - 10 animals following the usual inbibitory period of nearly 3 weeks . it proceeded rapidly and then slowed quite markedly . in spite of the prolonged treatment in which 31 doses were given , there were no deaths which could be directly attributed to the effect of the drug . this faflure of continued treatment to maintain the state of inhibition id the tumour has also been confirmecl in other experiments . the contrast in susceptibihty between the original and derived walker tumours to the triazine , has also been found . 
as was mentioned earlier , the development of mouse leukaemia resistant to fohc acid analogues is wen known and there has been a recent report that the mouse sarcoma 180 , whicb is moderately inbibited by 6 - mercaptopurine , rapidly develops some resistance to this compound ( clarke , philips , stemberg , stock , elion and hitchings , 1953 )  . on the - whole , solid rat and mouse tumours appear to be relatively resistant to chemical inhibitors , although the response of different tumours to the same drug varies widely . 
not often does the arrest of growth extend to all tumours in an adequate group of experimental animals , in spite of the administration of dose levels of near lethal magnitude ( suguira and , stock , 1952a , 1952b )  . appears that rat tumours are more susceptible than those of the mouse to trie - thylene melamine , for complete regression has been obtained in nearly 100 per cent , of animals with the jensen rat sarcoma , sarcoma r39 and the flexner joblidg it is generally agreed that the longer carcinoma ( suguira and stock , 1952b )  . initiation of treatment is delayed , the less chance thei - e is of total regression . - the action of triethylene melamine on the walker carcinosarcoma is striking - even when treatment is delayed for as long as 5 days after implantation , by which time the tumour is actively growing . in the present series of experiments regression occurrecl in every animal and usuary little or no palpable material this confirms the work of hendry , homer , - remained at the site of the implant . rose and walpole ( 1951 ) and peczenik ( 1952 ) , who however , commenced treatment curiously , 24 hr . 
after transplantation of the walker tumour into wistar rats . suguira and stock ( 1952b ) were less successful with this tumour in wistar rats , .obtaining inhibition of growth in 70 per cent of animals with day old implants and regression in only 20 per cent when treatment was delayed for 7 days . 
the results clearly show that in effectively 4h animals the inhibitory effect is only temporary and that growth subsequently occurred irrespective of the duration of treatment , even though this may be continued for several weeks instead of the usual 7 - 10 in either case the suppression of growth continued for upwards of 2 weeks days . before renewal of activity could be detected . 
the derived tumour on which most of the work has been carried out , was selected at random from a group of tumours growing subsequent to one short course of treatment applied to the original walker tumour . 
the resistance is thus considered to be a stable and permanent change . another member of a group of tumours similarly derived from the original walker carcinosarcoma has also been shown to possess comparable resistance to further treatment . it is reasonable to suppose that the same will apply to all such tumours . 
a noticeable difference between the original walker and the derived tumours is the more rapid growth of the latter in untreated animals . the growth of tumours after a latent period followino , a short course of treatment with triethylene melamine , must be due to the survival of a small number of cells which are naturally resistant to the drug . 
the fact that this sequence of events is not changed by the continued administration of triethylene melamine to animals bearing implants of the original walker tumour , suggests that the resistance of the residual cells is maximal at the outset . additional support for this view emerges from the failure to enhance the resistance by further exposure to the drug . 
how far mutagenic effects of the ethyleneimine may be concerned remains to be investigated , but the fact that such a bigli proportiod of inhibited tumours ultimately grow seems to make this factor less likely . 
the resistant tumour has also been shown to be refractory to two other ethyleneimines ( compounds ii and iii ) at dose levels which completely inhibit the original walker thus resistance to triethylene melamine confers resistance to carcinosarcoma . a diethyleneimine , and this may be true of active ethyleneimines in general . how far the same statement may apply to other kinds of chemical inhibitors active against the ordinary walker tumour is being investigated . it is interesting that the walker tumour should be so sensitive to triethylene melamine , whilst two other tumours which have been tested in the same strain of animal ( a mammary adenocarcinoma and the lymphosarcoma referred to in the crossley , allison , wainio text ) were only little affected by the same treatment . and muenzen ( 1951 ) studied the effect of triethylene melamine on a sarcoma ( 231 ) in the king a rat . 
of the triazine without undue toxic treatment of 7 - day old transplants of the flexner jobhng careinomaeffects . with this dose rate for 7 days produced regressions in 90 per cent of animals in there was no reappearance of tumours during the next 3 months , 1 to 2 weeks . which was taken to indicate complete cure . 
not only different kinds of tumour but various strains of rat vary in their susceptibihty to triethylene melamine ; the growth of an occasional tumour in animals bearino , a neoplasm susceptible to the drug , may be connected with some unsuspected ability of the host animal to dispose of the administered compound . it appears reasonable to suppose that ethyleneimino - compounds as a whole owe their anti - tumour activity to these highly reactive groups , so that it is difficult to conceive a protective mechanism possessed by some cefls but not by the great majority it is equally difficult to imagine a high degree of susceptibility in a tumour . in one variety of neoplasm and indifference in another kind to chemical inhibitors hke triethyleneimino - phospboramide ( iii ) , which is highly soluble in water and hkely to diffuse with ease into cells . 
then too , there is the fact which has been estabhshed on many occasions , that the susceptibility of sensitive tumours to these drugs diminishes markedly with the age ( i.e. , size ) of the tumour . it is hoped that a study of the mechanism by which the resistant walker tumour is derived from the original variety and an investigation of the reason for the insusceptibihty of the formee tumour may throw light on these interesting and important phenomena . inhibited nodules from the walker carcinosarcoma treated with triethylene melamine , 24 hr . 
after the conclusion of a course of treatment show intact tumour cells . no mitotic figures were seen . estimation of the mitotic index of the original and derived forms , 48 hr . 
after the administration of the last of 2 doses of the same drug reveals that the growth rates of the two tumours are similarly depressed . the drug would therefore , appear to be exerting a cytotoxic effect on the resistant form , although the overall growth of this tumour is not much hindered by such treatment . 
steiner. from the university of chicago , chicago 37 , illinois , u.s.a. received for publication april 15 , 1954 . in an aae of high specialization there is a tendency to achieve understanding in oncology this by the study of progressively smaller and stif smaher units . has taken the form of going fiom caincer as a whole to its various sites and types , and from tissues to cells to intracellular components and , finaffy , to molecules . much progress has been made in this way in an understanding of the disease . this dissective analytical approach has , however , tended to divert attention from some of the larger units within individuals and in societv which are still capable of teaching much about the natural history of the disease , including its etiology . 
the endemiological approach to etiology in cancer , wbich makes use of groups of cases , appears to be neglected . the present purpose is to show by a statistical study of large bodily units , namely , organ systems , an endemiological pattem in the natural frequency of cancers that appears to have etiological impfications . 
each major body system shows a harmonious pattem in its principal tumours , different from other systems , suggesting that they have similar etiological factors . in a recent statistical study , it was found that the curves fof cancer to autopsy ratios by age were similar for all major sites in an organ system and different from those of other organ systems . 
the study was then extended to the mortality statistics of the united states , which corroborated the previous observations . it is believed that this behaviour pattern has etiological significance . necropsy data , the basic data from which the curves in fig . 
1 , and the number of cancers at each site can be found in the principal table of tlle appropriate chapters of another publication ( steiner , 1954 )  . in that material of 35 , 293 necropsies , there were 6 , 072 malignant neoplasms . 
the twenty commonest cancers comprised 91 - 3 per cent of the total . sixteen of the twenty ( omitting carcinomas of the prostate , skin , pancreas , andthe intracranial tumors because they are lone representatives of systems ) far into six organ systems . 
they form the basis for the present study . if the curves of ratios of necropsies for cancer to total necropsies in the twenty tumors are plotted together , as in fig . 
the relationships of the can ' cers appear haphazard and disorderly . however , if now the curves for each organ system are withdrawn from this melange and plotted separately , as in fig . 
an attractive order emerges from chaos . thus , the tumors of the four principal sites in the ahmentary tract which give carcinomas of the mouth , esophagus , rise to carcinomas are plotted in fig . 
2. stomach and large intestine had low mortahties early in life but they increased to a maximum in the seventh decade , after which their importance dechned in relation to other causes of death . 
the mortahty from carcinomas of the mammary glands , uterus and ovaries began in the third decade , increased quickly as cancer to necropsy ratios to a maximum in the fifth decade , and then fell . 
the peaks and general configuration of the three curves are the same , differing only in amplitude . the mortafity began soon after puberty , increased to the time of the menopause , and then fell off relative to other causes of death - more in the uterus and ovary than in breast . 
steiner peak was at least four decades later than in the feinale generative tract . mortality began in the prostate when in the female generative organs it had already reached its peak . 
the curve for the prostate shows an inverse relationship to the period of most active sexual iffe , but a direct relationship is found in the female generative system . the two principal tumours of the respira ' tory tract , free from the confusion of fig . 
except for the sman peak m renal cancers in the first decade , caused by the wilm 's tumors , the configuration of the curves is the same . there was a gradual increase with age in these cancer necropsy ratios . 
7. although mortahtv from carcinoma of the hver began earlier than from the gafl - bladder , in both it mcreased with age , and there is a similarity in the curves which is not obvious in the apparent anarchy in fig . 
the cancers of the stomach intestine ( including rectum ) , esophagus and the buccal cavity ( including the pbarynx ) had totals of 24 , 258 , 33 , 383 , 3 , 866 if cancer death to ar death ratios are made by and 5 , 138 cases respectively . decenniums or bv quinquenniums , the configurations of the curves are the same for all four - tumours and they resemble those in fig . 
cavity show a virtual plateau in the two decades 50 - 59 and 60 - 69 . in the respiratory tract , 18 , 277 cancers were reported in the ' trachea , bronchi and lung ( some unspecified as primary or secondary ) and 1 , 852 in the larynx . the cancer to death ratios show peaks in the deca - de 50 - 59 as in fig . 
4. these peaks , also , lie between those found in the alimentary tract and the female gellefative organs . similarly , the three principal cancers of the female generative organs _ ( mammary glands , uterus and ovary plus fallopian tube and broad hgament ) show curves which are similar in configuration to each other and to - those in fig . 
3 , there were reported in 1950 18 , 973 cases of with peaks in the decade 40 - 49 . cancer of the breast , 16 085 of the uterus , and 5 , 652 of the ovary , faropian tube and broad ligament combined . ln the mesoblastic series of mahgnant tumours , those of bone ( 2 , 180 cases ) showed a curve resembling that in fig . 
5 with a peak in the decade 10 - 19 , a sman depression in the decade 30 - 39 ' and a small secondary rise followed by a gradual dechne . 
the mahgnant lymphatic diseases ( code numbers 200 - 205 ; total of 16 , 756 cases ) showed a peak in the first decade forowed by a gradual decline . the ratios to all deaths were higher during the first three decades than in the los angeles material . 
the sarcomas of ar soft tissues are not combined in the u.s. vital statistics , so this category cannot be stuclied . in the ul - inary tract , kidney tuiriiors ( 3 , 643 cases ) had a maximum in the decade 50 - 59 while bladder tumors ( 6 , 401 cases ) had a peak a decade later . neither curve showed the persistent rise of fig . 
6 in the older age groups . because all tumors of the hver and biliary passages are combined in the u.s. vital statistics , comparisons cannot be made between individual sites or with fig . 
mortality figures for 1950 conform to , with minor exceptions , the same endemiological pattems as the los angeles necropsies , showing that the latter were not exceptional in this regard . it should be noted that cancer to au ' topsy ratios were used in one set of data thus , autopsies for all causes and an and cancer to death ratios in the other . deaths were used , respectively , as the points of reference . cancer to autopsy ratios may be ofhmited . 
value in expressing total quantity but they are excenent for contrasting one site with another within a material because the point of reference however , essentially the same endemiowithin each age group is the same for all . logical facts are revealed by other methods ofanalysis , altbough less clearly . thus , the age distribution figures ( steiner , 1954 ) for the cases in the los angeles necropsies show - similarities within organ systems . 
figures gave sinfflar results in so far as they were compared . thus , if the data of clemmesen and nielsen ( 1952 ) from the danish cancer registry are used , the incidence curves for cancers of the stomach , esophagus and large intestine ( who code 153.0 - 3 , 153.9 plus 154 ) are similar in configuration , as are those of the uterus and ovary but not of the mammary gland . the question arises as to wbat , if anything , these statistical findings indicate regarding etiology . are they explained by chance ? that they probably are not is shown by the absence of exception in sixteen tumor sites representing six systems in the los angeles necropsy series , a ; nd an essential concordance by most such a high degree of thirteen tumors in five systems in the u.s. 
2 to 7 that the organs in some systems develop a greater proportion of their it is not known whether this earlier cancers at an earlier age than in others . occurrence represents an earher exposure to etiological factors or a shorter tumor induction time after the beginning of the exposure . induction time isthe resultant of many factors including type , potency and amount of carcinogen , number of ca - rcinogens , conditions of exposure and susceptibifity of the cens . that differences in induction time exist in man is indicated by the exposures - to ionizing radiation in japan ( hiroshima and nagasaki ) where to date only leukemias have occurred although ionizing radiations are known to induce tumors of other types . it is also apparent from the figures that the tumor yield by sites within systems varies greatly although the induction time appears to be the same . 
tumor yield is govemed , in general , by the same factors as the induction time just mentioned . in addition the number of cells being exposed is important in deter number of tumors obtained . 
steiner organ system can , in theory , be correlated in part with the number of cells at thus , in the alimentary tract each site exposed to hypothetical carcinogens . there would appear to be , on the basis of the gross and microscopical anatomy , approximately equal numbers of epithelial cells available for neoplastic conversion in the mouth and esophagus , many more in the stomach , and still more in the this is roughly parallel to the numbers of cancers that occur large intestine . in these locations ( in 1950 5 , 138 , 3 , 866 , 24 , 258 and 33 , 383 respectively in the united states )  . similar agreements between the relative numbers of epithelial cells and tumors are found in the larynx and lung , in the female generative organs ( if one assumes that most mammary carcinomas are ductal ) , and in the mesoblastic tissues if nuclei rather than total volume are considered . 
the curves of cancer to total mortality ratios by age in thirteen common tumors found in five systems showed a harmonious behavior within each system , which differed from that of other systems . some case distribution and some incidence data show the same statistical facts although less clearly . the etiological significance of these endemiological observations is unknown . however , it is suggested that they could be interpreted as signifying common etiological factors within each system with the differences in quantity in tumor by sites accounted for in part by the unequal numbers of cell populations at risk . comments are made about the interpretation of the quantitative differences in tumors between organ systems and in their age distribution . the author is grateful to the research committee of the los angeles county hospital staff for permission to study their material and to e . 
 ( karnofsky , burchenal , armistead , southam , benstein , craver and rhoads , 1951 ) , therefore , aroused much interest . human trials on the hazards of water contamination carried out by the american army medical centre indicated that aliphatic nitrogen mustards might be absorbed after oral administration : hn3 in a total dose of 15 to 18 mg . 
the walker tumours were passages of tumour cell suspension in dextrose , prepared by craigie 's mincer technique ( craigie , 1949 ) and preserved at - 70 ' c . 
the mouse sarcoma was treated daily for 7 days . in the tests against the walker tumour the total dose was given over 7 , 8 or 10 days , and ajso as a . 
single dose ( boyland , cleg , koller , rhoden and warwick , 1948 ; haddow , kon and ross , 1948 )  . eleven to fifteen animals were used for test . the water - soluble drugs were dissolved in distilled water immediately before administration and given orally or intraperitoneally . 
of distilled water was passed through the tube to ensu - re that the whole dose was washed into thl - , stomach . r 48 was given in a single oral dose in arachis oil . control animals received the solvent by stomach - tube or remained untreated . 
the walker tumours and sarcomata 37 were dissected 14 and 9 days respectively after transplantation , fixed in bouin 's fluid and 70 per cent alcohol , dried between filter - paper , and weighed . the difference in weight between control and treated tumours was analysed statisticafly . 
the maximum tolerated oral administered orall dose was about twice the maximum tolerated intraperitoneal dose . using these doses , both oral and parenteral treatment produced similar effects against the walker tumour ( table 11 )  . 
the oral activity seeme ' d to be influenced by the distribution of the total dose ; the weight ratio between control and hn2 - treated tumours became more significant when the total dose was divided over 7 instead of boyland , cleg , koller , rhoden and ' " tarwick ( 1948 ) found over io da - ily doses . that the parenteral activitv of nitrogen mustards increased when the total dose was given as a single injection . 
when given in a single oral do the effect of hn3 was negligible , whereas the activity of hn2 and nor hn2 seemed to be increased to a certain extent . 
the oral activity of nor hn2 seemed at least equal to that of hn2 , and more pronounced than that of hn3 , but even the highest weight ratios between control - tumours and those treated with the ahphatic compounds were only about one - quarter of the ratio recorded after treatment with r 48 ( table ii )  . 
the other aromatic nitrogen mustard tested , nn - bis ( 2 chloroethyl ) p - phenylene diamine hydrochloride , when given as a single oral dose of 4 mg . 
peczenik the adult group ; the ratio was about 3 times that recorded in the young animals - seven tests only were performed in duplicate , six of them against the walker in the three tests with the young rats the duplicat - e results agreed , tumour . whilst in the three tests carried out with the adult rats the duplicates agreed in two but disagreed in the other ( intraperitoneal treatment with hn3 )  . 
the maximum tolerated oral dose of nor hn2 was about 10 times larger than that of hn2 and 14 times larger than that of hn3 ( table 11 )  . 
the therapeutic ratio of hn2 and hn3 , whether the drugs were given intraperitoneally or orally , seemed as low as 2 , or even lower . as estimated from the death - rate , hn2 and hn3 were more toxic to tumourbearing than to normal rats . 
was toxic to adult but tolerated by young tumour - bearers . effect of nitrogen mustard8and triethylene melamine on body - weight . the tumour - inhibitory effect of the agents investigated was frequently assoin some instances , more frequent in ciated with inhibition of somatic growth . the adult than in the young rats . 
the experiment is described here because it has been suggested that urethane potentiates the effect of nitrogen mustards clinically . three groups of adult bearers of walker tumour received hn3 orally in a daily dose of 0 - 4 mg . 
of urethane daily , a dose of urethane whichper8e is known to be inactive against the walker tumour . another group received unstandardized adrenocortical extract ( eucortone ) intraperitoneally , i ml . 
peczenik from that of the controls during the first few days inhibition of the walker tumour became manffest during the second week , suggesting that the agents clid not influence the " take " of the transplants . the therapeutic ratios of hn2 and hn3 are probably not lar er after oral than after intraperitoneal administration . in non - tumour - bearing rats fed with hn3 , roberts ( 1952 , personal communication ) found changes in the intestine very similar to those described by several authors after injections of nitrogen mustards ( selye , 1950 )  . in view of this finding , it is worth noting that most of the tumour - inhibition shown in this paper was associated with significant suppression of somatic growth , whether the drugs that held true even when the net weight were given intraperitoneally or orally . ( body - weight minus tumour - weight ) was considered instead of the gross weight . thus the question arises to what extent the tumour - inhibition recorded after oral administration of the agents was due to a specific effect or to starvation . 
walpole ( 1951 ) has fo - und 40 per cent growth - inhibition of untreated walker tumours when ifthis 40 per cent ofthe observed somatic growth was prevented by underfeeding . tumour - inhibition is deducted from the figures in tables i to iv , the maximum .tolerated oral dose of hn3 would appear to be inactive in adult tumour - bearers ( table iv ) whilst the significance of the other results remains unchanged . it may be assumed , therefore , that the retardation of tumour - growth described above was this view is supported by the finding mainly due to other causes than starvation . that the suppression of tumour - growth after a single oral dose of r 48 or nor hn2 was not associated with suppression of somatic growth . moreover , - whilst effects , on tumour - growth were similar , effects ' on body - growth were more pronounced after intraperitoneal than after oral treatment . 
most of the animals on both diets lost weight during the treatment , and the ratio between the weight losses in rats with the 20 per cent and the 5 per cent protein diet was almost the same as the ratio of the degrees of tumour - inhibition . according to houck , crawford , bannon and smith ( 1947 ) , animals treated with nitrogen mustards lose body weight by loss of protein and water . 
the rats under these experiments , therefore , though fed with loss of protein may also intensify a high protein diet ( 19 - 2 per cent ) , lost protein . according to elson ( 1951 ) , the effect of inhibitors on tumourand body - growth . as an initially large dose of an inhibitor is gradually reduced , the animal will recover from the inhibitory action quicker than the tumour will , and the latter may completely regress under high protein diet . my experiments in which the drug was given in a single dose the loss of protein ceased in time to arow the animal to recover its growth - rate whilst tumour - growth remained retarded . it may well be that in those summary . administered intraperitoneally in about maximum tolerated doses , nor hn2 , hn2 and hn3 had approximately equal activity against the walker carcinosarcoma , although aaainst the sarcoma 37 , hn3 was more active than hn2 . the walker tumour was significantly more affected by triethylene melamine than by the aliphatic nitrogen mustards . 
r 48 was at least 4 times as active as the aliphatic bis ( 2 chloroethyl ) p - phenylenediamine was active after intraperitoneal amines . but inactive after oral administration . bromine substitution in hn2 and hn3 seemed to cause loss of activitv . triethylene melamine given orally was practically inactive in the non - fasting rat , whereas the same dose given to the fasting animal had marked activity but was toxic . tumour - bearing rats tolerated r 48 and nor hn2 in doses respectively 36 and 10 times the maximum tolerated dose of hn2 . 
wiltshire. from the biochemical liaboratory , university of cambridge . received for publication january 22 , 1953 . in 1939 k6gl and erxleben ( 1939a ) published the first of a series of papers it was on the optical configuration of amino - acids in proteins from tumours . found that the optical rotations of some amino - acids , which had been isolated by the classical methods and purified by recrystallisation , did not correspond with it was concluded that the preparations contained the values in the literature . the " unnatural " d - isomer in addition to the " natural " or l - isomer . 
the calculated proportion of d - isomer was largest in serine and glutamic acid . authors considered that serine had probably been partly racemised during hydroglutamic acid on the lysis of the proteins or during subsequent purification . glutamic other hand was considered resistant to racemisation in acid solution . acid from normal tissues and benign tumours had the specific rotation [ a ] 200d + attention was directed to this apparent difference in the optical form 31 - 60 . of glutamic acid from malignant and non - malignant tissues , which promised to be a lead to the long - sought chemical difference between normal and neoplastic tissue , and one that could be used for diagnostic purposes . 
a theory of malignity was proposed ( kogl , 1939 ) depending on the inability of most peptidases to hydrolyse peptides of d - amino - acids . the experiments of kogl and collaborators were repeated in many other laboratories with variable results , which on the whole showed smaller amounts of d - isomer than had been found by kogl . 
the considerable controversy which developed between different schools was suspended by the recent war , but dodds and dickens ( 1940 ) had already concluded from a review of the results then available that the appearance of the d - isomer of glutamic acid was not characteristic of since the war further work by kogl , barendregt and klein tumour tissues . ( 1948 ) and kogl ( 1949 , 1950 ) has renewed discussion of this problem . indirect evidence was produced in support of the original hypothesis . it was decided to limit the present study to the problem of whether or not the d - isomer is found in protein hydrolysates , and if so whether it exists as such in the proteins or is an artifact . 
a similar study using different methods ( boulanger and osteux , 1950 ) has appeared since the experimental work was completed . preliminary experiments ( wiltshire , 1953 ) showed that glutainic acid is racemised to the extent of about 5 per cent in the preparation of protein hydrolysates . 
found for calf lung protein total glutamic - n equivalent to 5 59 per cent and the l - isomer to 554 per cent of the protein - n compared with the present 5 69 per cent and 5 49 per cent respectively . for the carcinoma of the bronchus they found 6 * 40 per cent and 6 29 per cent both methods compared with the present 6 * 23 per cent and 6 29 per cent . therefore would appear to account for all the glutamic acid ofthe proteins . this is of some importance , since in much of the earlier work involving purification of the amino - acid for polarimetry a very small proportion of the total glutamic acid was finally isolated and analysed . 
the same criticism may be made ofthe aluminachromatographic methods of wieland ( 1942 ) and boulanger and osteux ( 1950 ) , where only 70 to 80 per cent of the original glutamic was recovered . 
the isolation of a small and unrepresentative sample may account for the discrepancy between the results of experiments by graff , rittenberg and foster ( 1940 ) and wieland and paul ( 1944 ) , who , using n15 - labelled glutamic acid , could find only 2 to 5 per cent d - isomer in the glutamio acid from tumours , and by k6gl , erxleben and van veersen ( 1943 ) , who with deuterium - labelled glutamic found over 20 per cent . 
the latter experiments have been criticised on other grounds by rittenberg and shemin ( 1946 )  . soon after the discovery of d - amino - acids in tumours several workers tested the activity of d - amino - acid oxidase from kidney on hydrolysates of tumour and other tissue proteins . 
among others k6gl , herken and erxleben ( 1940 ) ; lipmann , behrens , kabat and burk ( 1940 ) ; lipmann , hotchkiss and dubos ( 1941 ) ; arnow and opsahl ( 1940a , 1940b ) and boulanger ( 1944 ) could find no d - amino - acid in whole hydrolysates by this means . 
the percentage of d - glutamic acid found was in all cases very small , and not more than would be formed by inversion of the l - isomer during hydrolysis . i wish to thank b . 
holmes for the jensen sarcomata , the bland - sutton institute of pathology , middlesex hospital , london , for the liver metastases from a case of carcinoma of the colon , and professor f . 
bather. from the poultry research centre , edinburgh , 9 . received for publication november 18 , 1953 . considerable interest has been centred lately on the use of ascites tumours in rats and mice for biological research . 
such tumours include , in mice , the ebrlich and krebs - 2 carcinomata ( loewenthal and jahn , 1932 ; klein and klein , 1951 ) and s - 37 and malignant lymphoma ( goldie and felix , 1951 ) and , in rats , the yoshida sarcoma , the mtk sarcomata i and 11 ( tanaka and kan ' o , 1951 ) and the hirosaki sarcoma ( makino and kano ' , 1953 )  . 
the growth of these tumours is characterized by the formation of large numbers of discrete tumour cers , living in a compatible medium ( peritoneal fluid ) which lend themselves admirably to various biochemical studies . during the course ofinvestigations into the nature of the virus of rous sarcoma , an ascitic variant of the tumour was estabhshed early in 1953 in order to see if infective virus could be obtained in a more pure forthe fact that rous no . 
of the suspension was no evidence of necrosis . inoculated into the abdominal cavity of each of 2 6 - week old chickens from a known rous susceptible strain maintained at this centre . 
most of the negative results can be attributed to failure of the inoculum to enter the abdomen and , usually , subcutaneous tumours grew at the site of entry of the needle . the rapid growth of the rous tissue and its invasion of the intemal organs has been observed in all subsequent passages . 
smar nodules of tumour tissue attach themselves to the surface of the organs and then proceed to infiltrate the membrane and musculature , often penetrating to the interior of the organ itsell of 30 birds from the ist to the 12th passages autopsied 9 - 19 days after the inoculation of the tumour , the following tissues showed invasion microscopically and grossly : gizzard ( 30 ) , pancreas ( 27 ) , duodenum ( 27 ) , spleen ( 25 ) , ovary ( 17 out of 20 ) , testis ( 5 out of 10 ) , liver ( 12 ) , heart ( 10 ) , adrenal ( 10 ) , kidney ( 7 ) , and lungs in the cases of the ovary and pancreas , invasion has frequently pr ' ogressed ( 1 )  . to such an extent that only a few fragments of normal tissue remain , almost the whole organ having been replaced by tumour tissue . 
pale yellow , viscous fluid present in a 6 - week - old bird after 10 - 1 2 days ' incubation , and , on occasion , as much as 60 ml . 
the cells account for approximately 10 per cent of the fluid volume . counts of the cells made from stained smears ( giemsa ) at variou 's times during the passaging of the tumour show that of over 2000 cells counted approximately 50 per cent are round tumour cehs , and the remainder leukocytes , lymphocytes and connective tissue cehs . this proportion has remained unchanged throughout the 18 passages so far maintained . 
on various occasions , virus or whole cells from ascitic fluid have been inoculated into the muscles of birds and , again , there is an immediate return to the normal histological picture of a solid rous no . 
1 shows the typical appearance of the fluid using iron haematoxylin stathe cytoplasmic and nuclear changes in rous sarcoma cells cultivated in vitro have been described ( tenenbaum and doljanski , 1941 ; doljanski and tenenbaum , 1943 ) and many of the descriptions apply to the appearance of the cells grown intraperitoneahy . 
the blue staining granule and thread network in the peripheral cytoplasm ( giemsa stain ) and the dense central zone can be seen , as well as the large cytoplasmic vacuoles and clubshaped pseudopodia . 
bather scattered at random and sometimes arranged round the periphery of the nucleus . the gathering of this granular material into the centre of the nucleus , leaving a clear zone between it and the nuclear membrane as described by tenenbaum and doljanski ( 1941 ) , is only rarely seen in these preparations . large round or rod - shaped , densely staining nucleoh are common and irregularly shaped ones are frequently found . multinucleate cells are present and many contain fragmented nuclei with as many as 15 - 20 fragments . measurement of the frequency of multinucleate cells is given in a later section . ascitic fluid examined microscopically by dark field illumination on the warm stage provides an excellent opportunity to observe the living cells for long periods of time . 
the lace - edge appearance of the .cells is typical of fresh preparations and the cell membrane tends to become more regular after a few hours . in the peripheral area of the cytoplasm , and in the pseudopodia , a very fine " mist " of minute particles can sometimes be seen , although this does not occur in every cell . 
the club - shaped pseudopodia described by doljanski and te ' nenbaum ( 1943 ) are a common feature and sometimes become detached , forming free spherical " bubbles " of protoplasm , usuary shimmering with the rapid brownian movement of very fine particles . similar vesicles are seen , especially in the clumps of aggregated cells in which either particles or an interwoven mass of fine filaments appears . 
they have been show - n to be present not only in pathological blood conditions , b ' ut also in normal blood after it has been kept for several hours under sterile conditions . in the rous ascitic tumour and in erythroleukaemic blood ( campbell , 1952 ) filamentous structures are present i fresh preparations and may be associated with the high rate of c ' ell degeneration . the possibility that they may represent a method of virus release from infected cells must be borne in mind . similar structures have been observed associated with cells infected with influenza virus by hoyle ( 1950 ) and wyckoff ( 1951 )  . a peculiar filamentous structure encountered , only occasionauy , is represented by the spear - shaped process shown in fig . 
the outer part of the thread becomes an external , free floating filament and the inner part withdraws to the cell , forming a small protrusion on the cell membrane . 
this type of structure usually occurs in cells having a poorly defined nucleas under conditions of dark - ground inumination . the fluid surrounding the cers also contains numerous tiny rapidly moving particles which scatter light . multinucleate cells show up very well and , occaascitic rous no . 
the samples were taken between the 10th and only cers containing morphologically 14th days after inoculation of the tumour . such cells arise because normal nuclei are included in the multinucleate forms . of failure of cell cleavage after nuclear division . 
the incidences of karyorrhexis and mitosis after 10 - 1 4 days ' tumour growth have not altered to any significant extent . number of nuclei per cell . karyorrhexis mitosis infective viru8 in ascite8 and 8olid rou8 8arcomata . the amounts of infective virus contained in either the cytoplasm of the washed cells or in the cell - free fluid have been determined by means of the day - old chick titration method first described by carr and harris ( 1951 )  . 
bather table ii shows the results for the first i 0 passages , along with two sets of figures obtained for solid rous sarcoma tissue and cell - free exudate . 
the virus titres of fluid and cell contents follow each other fairly closely . in 4 of the 7 pairs of results , however , the intracellular virus shows a higher titre by one logio dose . in this respect the ascitic tumour behaves in the same way as the sohd sarcoma and its exudate . edimation of total 4cpurified " viru8 material in cell8 and cell - free fluid of the rou8 in view of the differences encountered in the infectivity titres of the fluid and cehs , estimates have been made of the amounts of virus material obtainable from both sources . 
the " purified " virus was isolated by the fractional centrifugation method of carr and harris ( 1951 )  . ascites fluid was first treated with hyaluronidase to reduce the viscosity . 
the cells were then centrifuged off , washed in 0 - 85 per cent saline , lysed in distilled water and the cell debris discarded . both the cell extract and the fluid were then deposited in the servall s.s. 
the resulting pellets were treated with trypsin in m / 5 phosphate solution , clarified and deposited agathe amounts of virus material obtained in this way were estimated by the biuret method described in a previous pubhcation ( bather , 1953 )  . virus content is expressed as ml . 
dry weight per unit of tissue or fluid . during the washing of the cers , a cell count was done in a haemacytometer . table iii summarizes the results and includes an estimate of the virus per cell in solid rous sarcoma tissue . 
the figure is based on the average virus yields , as reported elsewhere ( bather , 1953 ) and an approximate cer count using the method of afizen and petermann ( 1952 )  . this method utifizes controlled homogenization in sucrose and acetic acid solutions containhag calcium chloride , ( 0 - 0023 m cac12 is used here )  . after suitable dilution , a count can be made of the whole cells and nuclei in a haemacytometer . 
an average figure for rous sarcoma , based on five different tumours was found to be 32 - 2 x 107 cells per g . with a standard deviation of + 2 - 8 . 
bather peritoneal fluid containing suspended round cehs . it seems probable that this type of conversion does not depend on the selection of round cells since when the tumour invades the abdominal organs , the secondary growth reverts to the normal spindle - cell form immediately . moreover , virus or whole fluids , from the ascites tumour , when inoculated intramuscularly , produces a typical solid rous doljanski and tenenbaum ( 1941 ) have described the reversible transsarcoma . formation of the one type olf rous cell to the other in tissue culture . 
thus the rous sarcoma , in chickens , closely resembles s37 sarcoma and t2146 tumour in mice , both of which have been shown to form ascites tumours by reversible adaptation ( lasnitzki , 1953 )  . results from the first ten passages of the ascites tumour indicate that the cell - free ascitic fluid contains infective virus to an extent , roughly , of that contained in a 10 per cent extract of the cehs . similar observations have been made on the liquid exudate from sohd rous sarcomata . there are various ways in the first place , of course , in which the virus may be released from the cells . virus might be released upon necrosis and disintegration of the cell . secondly , there is the possibihty that the filaments , which are abundant even in fresh preparations of rous ascites fluid , may represent a method of eiectinlr virus particles . 
of the sohd tumour growing in birds of the same age . in terms of dry weight of virus material , this infective titre was given by 0 - 30 m.g " purified " virus for the ascites tumour and 0 - 46 mg . 
the ascites produced is made up of cells ( 10 per cent ) and a pale yellow viscous fluid ( 90 per cent ) both of which contain infective virus . 
the cells are mostly dispersed singly but some are aggregated into small clumps . approximately 50 per cent of them are round tumour cells , the remainder lymphocytes , leucocytes and connective tissue cehs . 
after 10 - 14 days ' growth , 10 - 5 per cent of the tumour cells are multinucleate ( with 2 - 4 nuclei ) 1 - 8 per cent contain pyknotic , fragmentary nuclei ( karyorrhexis ) and 1 - 1 per cent are undergoing mitosis . 
no improvement in the yields of infective virus , as detectable by the day - old chick titration method , has been obtained from either washed cehs or cell - free fluid of the rous ascites tumour when compared with the sohd rous no . 
86 x 10 9 mg fluid exhibits the same , or more often , all expenses in connection with this work were borne by the british empire cancer campaign . i should fike to thank j . 
5 ( peacock , 1946 )  . since our last publication on this subject we have successfully propagated three new induced sarcomata , grch 16 , 17 and 18 . these three tumours occurred in the course of attempts to induce epithelial tumours by injecting into adult white leghorn fowls a mixture of tissues from 10 to 14 - day chick embryos of the same flock , with methylcholanthrene and sudan iv dissolved in olive oil , following the technique used by rous and smith ( 1945 ) for inducing epithelial tumours in mammalian embryo tissues . 
we used a variety of embryonic epithelia , but the only tumours that resulted from these procedures were spindle cell sarcomata of precisely the same familiar pattern as when the carcinogens were inoculated directly into the adult breast muscles . 
they are made up of fleshy spindle cells arranged in whorls and interlacing bundles , the individual cells being elongated , sometimes with branched ends , with finely granular acidophil cytoplasm , and with an oval nucleus containing generally one small sometimes the cells are multinucleate , in which case the nuclei are nucleolus . in line one behind another , never in the form of giant cells of the foreign body mitoses occur very frequently , and are often somewhat irregular with type . bridging and incomplete separation of the chromosomes ; but many apparently occasionally longitudinal fibrillation of the normal mitoses are also to be seen . cytoplasm can be made out , but cross - striation has never been observed in metastases in viscera free from striated muscle such as the liver . 
48 : ( a ) liver and ( b ) squamous epithelium from the crop of a 10 - dayold chick embryo were mixed with 1 per cent methylcholanthrene dissolved in a saturated solution of sudan iv in olive oil . 
3086 was killed in moribund condition . there was an oval tumour 5 cin greatest diameter in the left pectoral muscles . there was no tumour in the right pectoral muscles , and no residual fluorescence was detected at either site of injection . there was a chronic plastic peritonitis , probably from a healed perforation of the gut , which was bound down with adhesions . the gall bladder was greatly distended . 
of fresh tumour was ground smooth in a sterile mortar , and 10 ml . of 5 per cent dextrose saline were added and well stirred to give a turbid cell suspension . ten 6 - week - old white leghorn chicks were inoculated with doses of 0 - 2 ml . to 1 * 0 ml . 
a 1 in 10 fresh cell suspension in 5 per cent dextrose saline was injected into the breast muscles of 6 white leghorns , 9 to 12 months old , in 2 of which tumours were palpable in about 4 weeks . subsequently the tumour was maintained through 3 serial passages , by cell suspension inoculation . 
the lowest 1 cwas cut off and discarded , and the remainder of the paper was laid on a sterile agar plate and flooded with melted agar at 460 c . 
prodigiosus was present only in the lower 3 cm . all levels of wet paper , however , were infective in the case of of the wet strip . the mh2 tumour , but in the case of the grch 16 tumour no level above the meniscus of the tumour extract was infective . as in the case of ea ' rlier chemically induced sarcomata in which the test was made by similar technique , using paper at levels above the first centimetre from the free fluid , grch 16 and 17 homogenates yielded only negative results . this observation is completely in keeping with the results of the more conventional filtrations through gradacol membranes or seitz clarifying pads . 
on the other hand , the tumour itself might be supposed to contain such an agent , which for some reason or other was adsorbed strongly by the filter . in the case of paper chromatography the whole paper can be injected either intact or homogenised in saline , and this might be thought to favour the demonstration of viruses where filtrates yield negative results . 
as there are many variable factors in such exposures , it is convenient to express dosage as time related to sterilising effect on bacteria . under our conditions suspensions of b . 
for 5 to 10 minutes were exposed in plastic tubes to a focused beam of ultrasonic waves with a frequency of one megacycle per second transmitted through a cooling water bath . 
the plastic tube was transparent to the waves , and was so placed that maximum disturbance occurred in the centre of the tube . in order to concentrate the effect of the waves as much as possible 2 to 5 ml . of 1 / 10 homogenate of fresh tumour in normal saline were used . 
1 in the resulting proliferative reaction tissue . we have previously reported the localisation of virus - induced fowl sarcomata at remote sites of x - ray or radium burns ( peacock , 1946 )  . cauterisation with a red hot platinum wire or with fuming nitric acid applied to the skin with a glass rod ( 2 to 3 mdiameter ) has more recently been found to localise the virus in birds bearing rous sarcoma no . 
a sterile cotton thread was inserted in the left pectoral muscles of each chick and also ( a ) in 5 the left wing was injected with 0 - 1 ml . 
50 : ( a ) four out of 5 chicks had tumours in the right breast but no ( b ) all 5 chicks had tumours in the right breast . 
50 : the 9 chicks with large tumours at the site of rous sarcoma three chicks out of 6 had localisation at site of cautery , inoculation were killed . and 1 of them had localisation at site of control thread . none of the remaining 3 tumour - bearing chicks had localisation either at the site of sudan iv injection or at the site of the control thread . 
on the other hand , occasionally local inflammatory reaction occurs around the metal wing tabs used for numbering the birds , and we have seen 2 cases of localisation of rous sarcoma no . 
1 , and had 1 feather plucked from the leading edge of the wing on the day of injection and on the 4th , 6th , 13th and 15th days thereafter . 
no localisation occurred at the sites of trauma . it was thought that histamine - like action following cautery might cause local blood stasis and so favour the metastatic growth of blood - borne emboli from the tumour histamine was therefore injected into the left wing web at the damaged site . of 6 white leghorn chicks 4 weeks old bearing rous sarcoma no . 
50 : a large tumour was present in the right breast and the bird was there was direct spread from the grch 17 tumour injection site to the killed . liver , but no tumour at the site of rous no . 
3312 , 3316 and 3317 , which had not grown tumours at the site of injection of the seitz filtrate ( see above )  . typical grch 17 sarcoma grew in no . 
on the other hand , no such localisation has been observed in the case of the grch series of tumours . it seemed that the electron microscope , which can undoubtedly reveal particles of the size of viruses , might afford conclusive evidence of their presence or absence in our limited experience of this technique , however , there are in tumour cells . even less differences to be seen between infective and non - infective tumours and even normal tissues and in homogenates and filtrates prepared from them than can be seen by ordinary visual microscopy or even by direct visual observafurther work may overcome this initial difficulty of recognising viruses tion . from normal cell constituents ; but in the meantime circumstantial evidence points to essential differences between certain induced and spontaneous tumours . the occasional occurrence of a chemically - induced tumour which on propagation yields a virus does not in our opinion justify the assumption that all indeed , the existence of spontaneous filterable tumours contain such viruses . tumours would suggest that ultimately one is likely to encounter such agents in duran - reynals ( 1952 ) has recently suggested , birds injected with carcinogens . however , that viruses not usually associated with tumours may become adapted to cells conditioned by chemical carcinogens , and so play a part in the aetiology of cancer . 
our failure to induce any epidermoid cancers in the skin of fowls after repeated painting with chemical carcinogens may be due , as he suggests , to the absence of fowl pox in our flock ; but we have had no difficulty in inducing upwards of 60 sarcomata at the sites of injection of chemical carcinogens , and have seen a few carcinomata of the crop following exposure to 2 - acetylaminofluorene ( peacock and peacock , 1949 )  . 
though we failed in attempts to transmit the carcinomata and therefore cannot assess their possible viral content , we saw no inclusions of the kind described and illustrated by duran - reynals ( 1952 ) in his fowl pox methylcholanthrene carcinomata . the study of a wider range of chemically - induced fowl tumours , preferably including carcinomata of recognisable patterns , seems to offer the best prospects for obtaining more information about the aetiological factors concerned . 
1 , mill hill 2 endothelioma and the grch 16 , 17 , 18 sarcomata show that the two former tumours are readily transmissible by filtrates and by other extracts in which cells are probably destroyed or excluded , whereas the grch tumours are only transmissible by extracts containing cells . at the time of writing the authors were unaware that loewenthal ( 1931 ) had used capillary ascent on strips of filter paper of extracts of rous sarcoma no . 
some authors ( willis , 1948 ) believe that the association is mainly indirect , and that the nutritional features result chiefly from anorexia , ulceration and infection , to which , with cancers of the alimentary tract especially , are added disordered digestion and absorption of food . 
others consider that the connection may be morp , direct , perhaps through metabolic competition for circulating nutrients , and in - recent years animal experiments have lent some support for this hypothesis . a reduction in plasma albumin concentration has been noted both in cancer patients and in tumour - bearing animals ( abols , rekers , binkley , pack and rhoads , 1942 ; siebert , siebert , atno and campbell , i 947 ; huggins , 1949 )  . 
a - n early fall in the blood haemoglobin level ( greenstein , andervont and thompson , 11942 taylor and pollack , 1942 ; el mahairy , 1950 ) and marked reductions in tissue enzyme activity , e.g. , in liver catalase , in organs far d - istant from the growth have been similarly recorded ( greenstein , 1947 )  . while tb - ere is no doubt that a growing cancer often exerts widespread effects on general metabolism , no study has yet been made of any process common to both normal and tumour cells in whicb any such metabolic competition might be expected to disclose itself . 
with this in mind , therefore , it seemed profitable to niake a comparative study in normal and tumour - bearing animals of the occurrence of mitosis - a phase of the growth process which to the best of our present knowledge presents similar features in botb types of cell . 
in some experiments the protein content was doubled at the expense of the carbohydrate ; this " high - protein " diet contained 40 per cent of casewith the aid of a little water all the ingredients were mixed into a stiff paste which the mice ate readily . 
present work , bullough ( 1949b ) stated that changes in temperature within the range normally found indoors in this country had no noticeable effect on mitotic activitv in the skin of the ear . 
this anaplastic tumour grows readily in the strain of mouse used ; it has a high percentage of " takes , " and shows very little tendency to regress when once established . 
immediately after its removal the piece was trimmed all round in order to expose a raw edge which facilitated the penetration of the cold i per cent acetic acid solution in which it was at once immersed . 
after i to 2 hours in this solution ( the time depending on the size of the piece ) , it w ' as possible to slide the epithelium from both sides of the underlying connective tissues . 
after it had been covered with a similar piece of filter - paper the whole was moistened with fixative , compressed lightly between two coverslips held together with an elastic band , and immersed in fixative for at least an hour . the fixative used was a mixture of one part of glacial acetic acid with two parts of absolute alcohol ; exposure to this solul . - jon for several days did not greatly harm the cells , biit a period of not more than 24 hours gave optimal results . 
the " sandwich " was therefore removed intact from the coverslips , washed free from fixative in 33 per cent alcohol followed by water , and then soaked for a short time inn / 1 hci before it was replaced between the coverslipa and their rubber band . 
after about i hour the maximum degree of staining was reached , and a subsequent washing for a similar period in s02 water was needed to remove unchanged stain which would otherwise have become re - oxidized in the later treatment . 
changes in the mitotic activit qf ear epithelium in tumour - bearing m - ice . the results of three similar experiments which show the general effect of the growth of the tumour on the mitotic activity of the epidermal cells of the pinna are given in table i . 
the relation of the reduction in the mitotic activity of epidermal ce118 in tumoursince it is possible , as some authors have suggested , that systemic effects in persons or animals bearing tumours may be due more to depression of appetite and lowered food intake than to the direct competitive effect of the tumour itself , some experiments were performed to determine how far such indirect factors may be - the cause of the reduction in mitotic activity . 
since the tumours had reached about 10 per cent of the animal 's body weight at the time of death , the neoplastic tissue was resected before the final carcass weight was determined . from table ii it can be seen that even wlien the tumours had reached this lai - ge proportion of the body weight , the average carcass weight had not fallen from the time of implantation . 
although there was no sign of wasting in these tumour - bearing mice , and their behaviour continued to be typically active , the frequency of mitosis in the epidermal cells had fallen significantly . a further test of the inanition theory of reduction of mitosis lay in determining whetlier there was any correlation between the change in the weiglit of the mouse in the ' final 24 hours and the frequency of mitosis . 
since the mouse has a very higil food intake - 15 to 20 per cent of its body weight daily - any abst ' inence from eating is quickly revealed by a . 
in table iii the control and tumourbearing mic - e have been subdivided into two aroups on the basis of change of weight in the preceding 24 hours , and the mean number of mitoses per i 00 fields of the ear epidermis recorded . 
these general findings are in conformity with those of sherman , morton and mider ( i 9 , 50 ) , who observed that in tumour - bearing rats the nitrogen required for the nutrition of the tumour was derived from the diet until the growth reached about 10 per cent of the liost 's body weight , and that it was only after this proportion had been exceeded that this requirement was obtained at the expense of wasting of the body tissues . 
it is difficult , consequently , to attribute the decreased rate of multiplication of the epidermal cells in our mi - ce to any change ' comparable with ihe intoxication and cachexia often present in the later stages of neoplastic disease in man . an alternative explanatioii for our observations is that during the growth of such implanted . 
tumours nutrient substances essentia ' l for cell division may be diverted from normal to neoplastic cells to the detriment of the former . during periods of nutritional stress , such as severe malnutrition or pregnancy ( barcroft , 1946 ) , it is nowbelieved that a competition for circulating anabolites develops between cells , which be ' ars unequally on those of different types . 
should a coniparable contest for nutrients develop in neoplasia , the processes associated with the multiplication of ' normal cells might be amongst the first to reflect a deterioration in the metabolic state of the host . 
further , as cortisone fails to produce this effect when it is applied in the " pre - induction " and " induction " phase of carcinogenesis , no support is given to mottram 's hypothesis , that the inducing action of a carcinogen is exerted on a dividing cell . 
the number of cells in mitosis in the cortisone pre - treated animals during the period of " induction " would be few or none and on this hypothesis far less papillomata should have appeared whereas the numbers equalled that of the controls . baserga and shubik ( 1954 ) have obtained essentially siniilar results . 
the findings of green and savigear ( 1951 ) may bear on this point . they showed that after 4 applications of dmb , over 14 days , the epidermal cells of the mouse ear became relatively refractory to the antimitotic action of cortisone given systematically . this was confirmed by an in vitro technique ( green , 1952 )  . it might be expected therefore that chemical carcinogenesis would not be delayed or prevented by cortisone , whereas in fact the present results show that it was . 
a possible explanation of this apparent discrepancy is that the time of appearance of resistance to cortisone depends directly on the rate of mitosis . if this rate is strongly diminished ( by cortisone ) from the outset of carcinogen treatment resistance would then appear much more slowly . 
at the time of its appearing however the treated area of epidermis would be rich in cells in the " induction " phase of carcinogenesis since cortisone does not affect this process . such a mass of cells , after a long exposure to the carcinogen , could be envisaged , when finally they had become completely resistant to cortisone , as emerging as a frank carcinoma . 
a single male introduced the ay gene into all three lines , and the yellow mice in the offspring were crossed again to the respective pure line , and this process carried on indefinitely . 
were he responsible , he would have had to be heterozygous for these 7 genes in addition to his own ayat make - up , which would be rather an admirable genetic achievement , even if deliberately attempted . ( 3 ) contamination by stray mice : the whole experiment was carried out in a small room of the mousery , in which only this " yellow experiment " and inbred mice are maintained . 
none of the mutants was of this type , but all of the contamination by strays does not therefore appear to be usual " inbred " size . a satisfactory explanation , and true genetic mutation . 
though considerable discussion has been given to the question of mutations produced by atomic bomb explosions , it is possible that a much more frequent cause of these disturbances may have been unsuspectedly in action for many years on persons exposed to the influences of carcinogenic hydrocarbons . while mutations analogous to some described in this paper , e.g. 
reduction of hair and eye pigments , may be unimportant in humans , other types of mutants , some not detectable by the hydrocephalus , found methods used , would be a serious factor in public health . in this work , certainly would be . dominant lethals , leading to sterility or miscarriages , may also be produced , unimportant in mice where a large litter size is found , but of serious concern in man . it is possible that some mutants , such as the brain hernia found as an embryo , would normally be missed by the scheme used above , as mice usually eat abnormal and inviable young . the same unconcerned and easy solution of such difficulties is not the case in humans . there are possible also dominant mutations , which would appear in the first generation . though none was found in the series above , several were reported by strong it is obviously desirable that this additional ( 1945 ) using methylcholanthrene . hazard of exposure to these carcinogens should be evaluated . that this need is urgent is also suggested by the following line of argument : radiation mutations are almost entirely random , i.e. 
if a certain gene is mutated by an ionization in one sperm , the chance that the same gene will mutate in another sperm in the same or another individual is not increased . 
the efficiency of but this is not mutation with regard to any given gene is thus almost zero . if a chemical distributed via the blood necessarily the case with chemicals . stream reacts with a given locus to produce a mutation in one sperm , it is bbviously liable to do the same with all other similar loci in other sperms ( or ova )  . 
an efficiency of mutation at a given locus at 100 per cent can thus be imagined , and then all offspring of an exposed individual will carry the abnormal gene . a mating of any two exposed individuals would then give all f1 of the mutated type , a state which does not arise until the f4 of close inbreeding with radiation156 j . 
they could therefore have a high efficiency at certain loci resulting in a high frequency of abnormal offspring without causing death of the cell , as happens when concentrated doses of irradiation are given to increase mutation rate . combination with genetic material is thus likely . it is obviously tempting to ascribe the ability of the carcinogenic hydrocarbons to produce mutations to their complex system of conjugated double bonds . this system would readily pick up energy from the surroundings , and liberate it with destructive effect at one point . 
the hydrocarbons are possibly even less energetic , and thus may only be able to produce mutations in genes that are of less stability than most . this would produce some degree of specificity as required above , and it is significant that most of the mutations produced both here and by strong are already known , i.e. 
the mice used for transplantation undoubtedly came from therefore , additional experiments were different sublines of these two strains . carried , out in an attempt to elucidate the forowing questions : 1 . 
does the regression of a well - developed transplanted tumour forowing irradiation in vivo render the animal resistant to the development of spontaneous tumours ? this study was made possible by the use of the irradiation technique ( goldfeder , 1950a ) which facihtates the exposure of the tumour and protects the rest of the body of the animal from secondary scattered radiation , thus permitting the treated animals to eve their life span . previous work on the irradiation of tumours has been summarized by the writer ( 1945a )  . there is no doubt that results obtained with tumours heterogenous to the animal bosts - that is , tumours which have a different genetic constitution from that of the host , are not comparable with those obtained with tumours autogenous to the animal hosts - that is with tumours having the same genetic constitution as that of the host , or with , those in patients suffering from cancer . 
memorial laboratory on julv 5 , 1933 , and they were designated at that these mice have been inbred since : they behave time as inbred strain ' d '  . immunologicary like dba / 212 , and have an incidence of over 85 pe ' r cent of spontaneous mammary tumours among breeding females . 
a tumour of about 5 min diameter usuauy develops from an implant within a period of 12 to 14 days , and grows progressively . a spontaneous mammary tumour of an i 1 - month - old female mouse of the dba this tumour was : firmer in consistency than that strain was excised asepticary . fragments of about 2 mdissected removed from the c3h mouse described . from the edges of the tumour were implanted subcutaneously into 10 dba mice ( 8 males and 2 females )  . 
1 round coverslip 7 inch in diameter , wbich had been previously attached by a drop of sterile water to a mica sheet and covered with a maximow depression slide , in the concavity of wl - lich moist filter paper had been placed to maintain the water content of the tissue . 
the absorption of radiation by the cover glass , mica sheet and maximow slide was about io per cent , which was taken into consideration in calculating the x - ray dose delivered to the tumour tissue . immediately after irradiation the tumour fragments were implanted into about 2 - 3 - month - old mice , most in two additional experiments the mice were injected of which were litter mates . intradermally with aliquots of irradiated . 
tumour cells , suspended in physiological this was done because , according to observations made by several investisaline . gators , the intradermal route of immunization appears to produce more effective and lasting results ( besredka , magat , laval and besnard , 1936 ; kolmar and tuft , for the latter experiments the tumour fragments following irradiation 1941 )  . were cut with sharp curved scissors until an almost homogeneous mass was obtained . 
doses by mea ' ns of a tuberculiin syringe and .25 gauge needle in two or three sites of the abdominal wall of each mouse . the latent period and the number of " takes " produced by tumciur grafts irradiated in vitro served as criteria of the effect of a given dose of x - radiation . the procedure of irradiation of the estabhshed tumours in v& ' vo was as follows actively growing tumours ranging in size from 1 - 0 to 1 - 5 cin diameter were exposed to filtered x - radiation while the rest of the animal orgamsm was shielded bv a lead chamber ( goldfeder , 1950a )  . during the early experiments the tumours were irradiated in vivo under the same physical conditions as the tumour grafts during the later experiments , the following physical factors were in vitro . employed : the radiation was generated by a westinghouse " quadrocondex " constant potential unit at 200 kv , 15 ma ; the incident beam was filtered by 05 mcu plus i 0 mal ; hvl equalled i 0 mcu ; fsd , 20 . 
the dose rate measured in air bv a thimble ionization chamber during the coiirse of the investigations varied from 395 r / mto 402 r / min . special measurements were made with and without the lead ( 5 per cent )  . shield , the ionizatioil chamber being placed in the same position . 
observations on c3hb transplantable mammary tumour . the results obtained on implantation of the irradiated c3hb tumour - grafts a - re recorded in table i are presented graphically in fig . 
the first ' retardation of tumour growth , as indicated by a slight increase in the latent period of tumour appearance , was prodiiced by a dose of 2000 r . 
ii , an implant irradiated with 5000 r developed a tumour after a latent period of 117 days . in this , as wer as in other similar instances , the question arises whether the tumour cells had been attenuated by x - radiation to such an extent that they remained dormant for this comparatively long ' time , or whether only a few cers had escaped injury and took , therefore , a much longer time to develop a palpable tumour . this question cannot be answered with any certainty . it is certain , however , that the tumour grew on the site of grafting and that the rate of growth and the histologic ' al pattem were similar to those of a tumour developed by a non - irradiated implant . in no instance did a tumour , developed by an irradiated implant , regress spontaneously , contrary to observations frequently made when the tumoiir implant and the host are not of the same genetic origin . search for induced re8i8tance the mice in which the irradiated tumour grafts failed to produce tumours ( experiments 7 - 14 , table i ) were reimplanted with fresh , viable tumour grafts . due to the long latent period , the second implantation into mice of this series was performed 3 to 4 months after the implantation of the irradiated tumour grafts . 
a dose of 12 , 000 r completely destroyed all the treated tumours . sections of the tumours removed within 10 to 12 days after irradiation showed only necrotic tissue . it appears , therefore , that a dose within the range of i 1 , 000 r to 12 , 000 r is lethal for the c3hb tumour of 1 - 0 to 1 - 5 cni . 
the irradiated tumours which resumed their growth after initial decrease in size , grew steadily and in no instance did a tumour regress once it began to grow again . occasionary secondary tumours developed in the treated mice either in the inguinal or axillary reg - ions within 2 or 3 weeks after the regression of the irradiated in some instances , new growth developed on the periphery of the tuniours . irradiated tumour , probably from tumour cells which bad not been included in the exposed area . 
the histological appearance of these secondary tumours resembled that of the primary , non - irradiated c3hb tumour . epilation and regrowth of gray hair appeared in the exposed areas 3 to 6 weeks after regression of the irradiated tumours . 
no ulceration of the skin in the irradiated area was ever noted in the c3h mice once gray hair appeared . a significant number of c3h mice hved about i year after regression of the tumours and spontaneous tumours appeared in some of the c3h females . 
observation8on dbah transplantable mammary titmour . this tumour had been carried for 8 generations of serial transplants in the dba mice from which it originated before it was used for irradiation . although loo per cent " takes " resulted in most instances , occasionany , however , an iniplant failed to produce a tumour in a dba mouse which later proved to be resistant to further viable tumour grafts . according to hauschka , this may be the result of a mutant histocompatibility factor present in the dba strain ; in other words , an outcome of genetic incompatibihty between the bost and the transplanted tumour . 
to secure a better statistical evaluation of the results , a number of mice were grafted with viable , non - irradiated dbah tumour fragments to serve as controls to those grafted with irradiated dbah tumour implants . 
the delay in the latent period is probably a more rehable criterion than the tumour " take " for re - evaluation of the radiation effects in this case , because it could be argued that the 2 mice in which the irradiated tumourcells failed to produce tumours possessed the mutant - histocompatibility factor . in one experinient , a dose of 4500 r resulted in 22 - 9 per cent of " takes " , while a dose of 4800 r resulted in 13 - 0 per cent of " takes " and a dose of 5000 r gave only 5 - 1 per cent of " takes however , in two additional experiments , after doses of 5000 r and 5200 r no " takes ocetirred . 
none of these 7 produced tumours fohowing implantations of viable tumour grafts . in the experimental - mice , the number which failed to develop tumours was 150 out of a total of 341 mice which had been implanted with irradiated tumour grafts . 
none of these eighteen dayis later these - mice were reimplanted 25 niiee developed tumours . subcutaneously with fiesh , viable tumour grafts . palpable tumours , whicb , grew progressively , appeared within 9 to 13 days in 14 out of the 15 reimplanted male and in 9 out of 10 re - implanted female mice . two mice , one male and one female , in which the irradiated tumour cells failed to produce tumours in the first place , remained refractory to twice repeated implantations of viable tumour grafts . this result may also be ascribed to the mutant histocompatibihty factor present in these 2 mice . re8u1t8qf x - radiation o dbah tumour8in vivo . table v records the observations made on a total of 227 mice ( 164 males and 63 females )  . 
a rather sudden increase in the number of tumours which showed regression was noted forowing the application of doses higher than 6000 r . thus , 60 per cent of the tumours regressed after a dose of 7000 r . 
while a dose of 6000 r destroyed only 25 per cent of the treated tumours . the larger percentage of the regressed tumours which had been treated with a dose of 10 , 000 r indicates that this is the destructive dose for the dbah transplantable tiimours , ranging in size.from 1 - 0 to 1 - 5 cin cliameter . 
as in the case of the c3hb tumour , this dose is twice as large as the dose necessary for the attenuation of grafts of this tumour in vitro . the majority of the mice . ' m which tumours had regressed eved in apparent good health for i year or longer , and the young female ' mice produced apparently normal litters . 
the ulceration - s persisted iintil the death of the - ani ' mals . these two instances may parallel radiation necrosis occasionally noted in human patients treated with x - rays . 
the turnours in the remaining 7 mice grew steadily . fourteen tumours decreased considerably in size within 10 days after irradiation increased tumours grew steadily after exposure . five tumours regressed within 3 to 4 weeks following exposure . 
two females developed spontaneous months after regression of the treated tumours . in 27 mice ( 20 males and 7 females ) the tumours regressed completely within 3 weeks after irradiation . 
microscopic sections of the regressing tumours consisted mainly of fibrous tissue . the tumours regressed completely in 30 treated mice ( 21 males and 9 females )  . five fexnales developed spontaneous tumours 6 - 7 months after regression of the treated tumours . the treated m1ce lived for as long as i year and more after treatment . 
the mice lived in apparent good health up to 1 year and more . of ar treated mice only in two - instances did ulceration of the skin in the irradiated area occur 11 months after regression of the tumour . should be noted that in the experiments cited above , geneticary impure ammals and tumours geneticary different from the hosts were used . 
the writer 's interest in the problem of induced resistance arose from investigations on mouse sarcoma 180 grown in white mice of the swiss strain ( golffeder , 1942 )  . 
the writer explored the possibihty of inducing a resistant state in inbred animals by implanting into these animals irradiated grafts of a tumour which originary developpd in an animal of the same inbred line . these expenments were carried out hi an attempt to ascertain whether ionizing radiation induces genetic and antigeriie changes in the tiimour cells which make them foreign to the host . 
the irradiation of tumour cells in the present experiments did not make them foreign or antigenic to the host in which they originahy developed . an analysis of the results recorded in table i and in table iii reveals a difference in the radiosensitivity between the c3hb and dbah tumours . for example , a dose of 3500 r gave 92 per cent " takes " of the c3hb tumour grafts and only 57 1 . 
determined for implants of other mammary adenocarcinomas in inbred strains of mice ( lawrence , horn , strong , 1937 ; goldfeder , 1945a ) and for a mammary adenocarcinoma of an inbred line of rats ( eisen , 1940 )  . 
on the other hand , the c3hb mammary adenocarcinoma used in t - he present studies proved to be more resistant to irradiation than the cm mammary adenocarcinoma used in previous experiments ( goldfeder , 1947 ) , the latter requiring only 2700 r to prevent its grafts from " takes "  . 
the difference in the radiosensitivity between the c3hb and c3h mammary adenocarcinomas may be explained by ( a ) a difference in degree of differentiation : the c3hb mammary adenocarcinoma in the present experiments is a more anaplastic type of tumour consisting of fiheets and bands of closely packed cells , with relatively little fibrous connective tissue , while the cm mammary adenocarcinoma previously reported ( goldfeder 1947 ) consisted of acini , uniformly distributed and separated by connective tissue ; ( b ) by a difference in genetic make - up between the tumours and their hosts : the c3hb niammary tumour was carried by serial transplants in pure inbred cm mice from which it originated , while the mammary tumour , used in previous studies ( 1947.1950 ) , was carried in c3h mice of different sublines and thus the tumoiir and the hosts were not of the same genetic origin . failure of the tumour to " tak - e " in about 10 per cent of the hosts indicated that some of the cm mice used in the experiments of 1947 - 1950 had a different genetic constitution than that of the .mouse in which the tumour developed . 
the skewed curve illustrated in that publication ( goldfeder , 1947 ) in contrast to the typical s - shaped curve obtained in the present experiment may also be the result of the difference in the genetic make - up between the hosts and the tumour . 
the radiosensitivity of tumours depends to a large extent on whether they are growing in hosts of the same strain from which they originated , or in foreign hosts as shown by aughterson , tennant , irradiation of a transplantable mammary carcinoma in and lawrence ( 1940 )  . strain a mice in which the tumour originated induced regression only in i per cent of the treated mice when 2500 r were apphed and in 48 per cent of mice forowing the application of 5000 r . 
the antigenic reaction of ' the foreign host is thus a contributing f ' actor in rendering the tumour more vulnerable to ' regression after irradiation . the more anaplastic c3hb tumour proved to be more resistant to radiatioii than the relatively more differentiated dbah tumour . this corroborates the observations made by the writer on another mouse mammary adenocarcinonia ( goldfeder , 1950a ) and those noted on human tumours . for example , cathie ( 1939 ) , lenz ( 1942 ) and gliicksmann ( 1948 ) found that well differentiated cancers regressed more readily and offered a better prognosis than the less differentiated tumours . the r ' ole of connective tissue in the response of animal tumours to irradiation and its relationship to the host was brought forth by cramer ( 1932 ) aind by aughterson , tennant and lawrence ( 1940 )  . 
the relatively more pronounced proliferation of the connective tissue in the dbah tiiniour thanin the c3hb tumour may also be regarded as a contributing factor rendering the dbah tumour more vulnerable to irradiation . 
the observation of secondary tumours occurring in the treated mice also seems to parallel observations made on human mammary this observatioin indicates the failure of the disintegrated irradiated cancers . tumour tissue to induce resistance in the hosts to new cancerous growths . it has been noted that untreated metastatic tumours often regress after x - ravv treatment of primary tumours ( sugiura , 1937 ; aughterson , tennant and lawthis observation has been attribiited to a supposed indirect effect rence , 1940 )  . of irradiation ( sugiura , 1937 )  . these observations could probably be explained by the fact that the tumours were grown in genetically foreign mice . 
the present experiments on mice of geneticafly pure strains and their autogenous tumours indicate that the indirect effect of irradiation is not sufficient to affect secondary growths . regression of the secondary tumours in x - ray treated heterozygous mice may be attributed to an antigenic effect ' ehcited by the genetically differing tumour tissue . 
the inability of the irradiated tumour tissue to induce " immunity " in hosts from which it originated may indicate that no quahtative change of a genetic or antigenic character occurred in the irradiated tumour cells which would render them foreign to the hosts . inbred hnes of mice and their tumours offer far more suitable material for investigations of this type than heterozygous mice . 
the observations made from such studies seem to pararel those noted on human mammary cancers . in earlier publications ( goldfeder 1950b , 1952 ) , the writer showed that a fast growing , less differentiated mouse mammary adenocarcinoma also possessed a more vigorous metabolic rate and suggested that this propertv may have been one of the factors influencing the radiosensitivity of the mammary adenocarcinomas then used . 
a smaller irradiation dose was found to prevent the irradiated dbah tumour grafts from growing in vivo than was required to produce a similar effect on c3hb tumour similarly , for treatment of established tumours in vivo , the dose of irragrafts . diation which produced regression of the dbah tumour was found to be smaller than that which had a similar effect on the c3hb tumour . 
some factors which are involved in the difference in the radiosensitivity of these two tumours are the state of differentiation of the tumour cells and the amount of stroma . in both instances about half of the radiation dose , producing destruction of the established tumours grown in their respective hosts , was required to obtain the attenuation of the grafts of both c3hb and dbah tumours . the c3h mice in which the irradiated in vitro c3hb tumour grafts failed to " take " or in which a well developed transplanted c3hb tumour regressed after irradiation in vivo remained susceptible to reimplanted viable c3hb tumour grafts . 
a small number of the dba mice in which the viable dbah tumour grafts failed to " take " in vivo remained resistant to viable tumour grafts . similarly , a small number of the dba mice in which the irradiated in vitro tumour grafts failed to " take " was found resistant to re - implantation of fresh viable tumour implants . this is explained by a difference between the genetic make - up of some of the dba mice and the dbah tumour . a significant number of mice of both strains lived in apparent good health for 1 year and longer after regression of the in vivo irradiated tumours ; among these survivors the young females produced apparently normal litters . spontaneous tumours also occurred among these female survivors on reaching cancer age . thus , under the experimental conditions described , the question about the possibility of inducing immunity in homozygous hosts to endogenous tumours by irradiation of these tumours appears to have been answered in the negative.. the part played by the genetic relationship between the tumour and host in the induction of resistance to the appearance of tumours was brought forth . 
butler. from the chester beatty research institute , the royal cancer hospital , london , s.w.3. received for publication april 21 , 1951 . the observation of brdicka ( 1933 ) that proteins gave catalytic double waves when added to an ammoniacal cobalt buffer and examined polarographically was soon applied to an examination of the serum proteins , and brdicka ( 1937 ) himself was the first to show that differences could be found in this way between normal and cancerous sera . 
there is no need to relate in detail here the earlier studies on the protein reaction as these have already been adequately reported ( brdicka , 1939 , 1947 ; brdicka , novak and klumpar , 1939 ) , but it will suffice to state briefly that pathological sera after hydrolysis with potassium hydroxide and polarographed in cobaltous buffer show a decreased wave height as compared with normal sera , but after deproteination with sulphosalicylic acid and the filtrates polarographed in cobaltic buffer show an increased wave height . 
brdicka ( 1939 ) found that the latter test , known as the " filtrate test , " was more reliable , but the readings from both tests are dependent on the temperature , and on the characteristics of the dropping mercury electrode . muiller and davis ( 1947 ) introduced an index , known as the " protein index , " derived from the ratio of the two tests multiplied by a constant , which was found to be independent of the temperature and of the capillary characteristics , and also of the age and sex of the subjects . the fact that the polarographic test is not specific for malignancy has been well established and it is therefore of no use diagnostically , but more recent results robinson ( 1948 ) , using the indicate that it may be of value as a prognostic tool . filtrate test , has studied its application in the prognosis of prostate cancers , and has obtained results which are superior to those obtained with the acid phosphatase test normally used for this type of cancer . 
the purpose of the work to be reported below was to gain further information concerning the usefulness of the method , and to compare it with other methods which might be more applicable in general routine . over 100 sera have been examined polarographically , and a smaller number examined by means of the " huggins test " and by the tryptophane - perchloric acid reaction . since the publication by huggins , miller and jensen ( 1949 ) of the " huggins test , " depending on the relative ease of the thermal clotting of serum in the presence of various concentrations of iodoacetate , many workers have investigated its application ( bodansky and mcinnes , 1950 ; homburger , pfeiffer , page , rizzone and benotti , 1950 )  . 
the original authors stated that the " iodoacetate index , " obtained by dividing the highest concentration of iodoacetate in which clotting could still occur by the total protein content of the serum , was lower in 226 l . 
the results obtained from an examination of a limited number of sera by means of the modified method ( huggins , miller and jensen , 1949 , private communication ) are reported below . increases in the polysaccharide content of sera have been observed by a number ofworkers in cases ofmalignancy , tuberculosis , nephrosis , hepatic cirrhosis andpneumonia ( shetlar , foster , kelly , shetlar , bryan and everett , 1949 )  . using the carbazole method seibert , pfaff and seibert ( 1948 ) showed that the globulins ( particularly the a2 - globulin ) contained the most of the protein bound polysaccharide . in an attempt to determine the nature of the polysaccharide seibert and her co - workers ( 1948 ) found that the tryptophane - perchloric acid ( tpa ) test of cohen ( 1944 ) was more useful . using this reaction the authors claimed a correlation between increases in the polysaccharide and increases in the o2 - globulin in cases of tuberculosis and malignancy . moreover , changes in the tpa readings were found in minimal tuberculosis when no change was observed with the carbazole reaction , and it was suggested that this was probably due to the former reaction being more specific although the latter reaction is probably more sensitive . the identity of the polysaccharide involved in the tpa reaction is not known , but only negligible colour formation is obtained with glucose , mannose , galactose and glucosamine , while a positive reaction is obtained with desoxyribose - nucleic acid and fructose . 
a new index was then formulated derived from dividing the value of the filtrate test ( test ii ) by the difference between tests iii and iv and multiplying by ten to bring it to a round number , i.e. , blood index ( b.i. ) = test ( ii ) test ( iii ) test ( iv ) huggins reaction . the modified method ( huggins , miller and jensen , 1949 , private communication ) was used . the iodoacetic acid was recrystallized from a mixture of equal volumes of benzene and 80 - 100 c . 
the contents of the tubes were gently mixed , the tubes covered and heated in a boiling water - bath for 10 minutes . alter cooling quickly they were allowed to stand for 40 minutes and then filtered through a no . 
the upper limit for normal values was fixed at an arbitrary level below which the majority of the normals were grouped ( 21 table i is divided into two groups , and considering the negative , 3 positive )  . cases placed in group ( a ) , it can be seen that 93 per cent gave a positive reaction . 
the former were ( i ) a patient with a 5 years ' history who had been successfully treated by surgery and by androgen , and who was clinically normal at the time the blood sample was taken ; ( ii ) a male case who gave a positive reading 2 weeks later ; and ( iii ) a patient with an advanced tumour who gave a negative reading again 2 weeks later . 
the negative prostate case had already been receiving stilboestrol treatment . these cases show a high correlation with the clinical observations , but group ( b ) of table i gives figures for two malignant groups which appear to give an even chance of positive results . classified in " buccal cavity " are carcinomas of the fauces , palate , tonsil , tongue , mouth , larynx and pharynx , and in " skin " are classified carcinomas of nose and scalp . 
great improvement was observed clinically while under androgen treatment ( after radiotherapy followed by radical mastectomy ) , and the polarographic however , the last five readings , taken readings altered from positive to normal . over a period of eight months , gave positive reactions , although it was only at the time of the last reading that a relapse was clinically observed . in this case , therefore , the relapse was forecast by the polarographic readings . 
youden ( 1950 ) has suggested the use of an index for the comparison of so - called diagnostic methods , which has a value of unity if there are no false positives or false negatives , and a value of zero when the test gives equal proportions of positives for the condition under investigation and the controls . 
the polarographic method gives a value for the index of 0 - 219 , the huggins reaction , 0 - 250 , and the tryptophane - perchloric acid method , 0 - 253 . 
the end - point as described by huggins was not easily determinable , as it was not always obvious what constituted a " well - defined mass . " this difficulty was also noted by bodansky and mcinnes ( 1950 )  . also , the end - point often did not occur within the limits of the recommended iodoacetate concentrations - a problem which presumably would have been overcome by using a larger range of concentrations , making the test much more tedious . 
the results obtained support the conclusions of bodansky and mcinnes ( 1950 ) and of homburger , pfeiffer , page , rizzone and benotti ( 1950 ) , which were reached after a much more intensive study of the reaction than has been attempted here , and it can be stated further that the test is too unreliable to be used in prognosis . the results given in table iii showed that the polarographic readings followed to a very large degree the clinical findings , and it can be stated that within certain limitations this method is useful as a prognostic agent . it can be seen from table i that apart from the two groups of cancers , a high correlation was obtained and the proportion of false negatives was low . there was , in fact , only one case in the negatives shown in table i ( a ) , which remains unexplained , since the prostate case was being treated with stilboestrol , and of the breast patients , one was clinically normal and the other case gave a positive reading two weeks later . this last case supports the view that the serial examination of serum gives far greater information than a single test , a view also supported by brdicka both positive and negative cases should be followed . ( 1947 ) and robinson ( 1948 )  . a persistently positive test or a negative test becoming positive would indicate that the patient requires investigation , a positive test becoming negative indicates that the patient has improved , while a persistently negative test may be misleading ; this last fact is the main weakness of the method . 
excluding tumours of the buccal cavity and skin , which gave an equal chance of giving positive or negative readings , polarographic examination gave a 93 per cent correlation with the clinical diagnosis of malignancy . 
a high correlation with the clinical diagnosis of malignancy was obtained with the tryptophane - perchloric acid test , although it is considered too unspecific to be of use in prognosis . i wish to thank professor e . 
1. received for publication july 1 , 1948 . in the course of experiments on a transplantable mouse sarcoma it was observed that fresh saline extracts of tumour tissue agglutinated mouse and rabbit red cells . 
when extract and red cell suspension were mixed on a slide agglutination became visible to the naked eye within 30 seconds and appeared to be complete within 2 minutes . a number of different mouse and rat tumours , and a wide range of normal tissues , have been examined for haemagglutinating activity . 
when quantitative results were required a tube test based on that used by burnet and his co - workers ( burnet , beveridge , mcewin and boake , 1945 ) was adopted . serial two - fold dilutions of tissue extract were made in calcium - saline in round - bottomed tubes of approximately 0 - 8 cinternal diameter . 
of a 2 per cent suspension of washed red cells in calcium - saline ; the tubes were then shaken and allowed to stand at room temperature for 20 - 30 minutes . 
a preliminary reading of the end - point could then be made , if a quick answer was needed , which did not differ by more than one place from the final reading . calcium - saline , 0 - 3 c.c. , was then added , the tubes were shaken and allowed to stand a further 1 hours at room temperature , when the final reading was made . the type of agglutination , and also of the deposition of red cells in saline controls , varied with species . 
mouse cells seldom , and rabbit cells hardly ever , gave the compact button of deposit which is typical of unagglutinated fowl or human cells , and which workers with influenza virus haemagglutination take as negative . rabbit cells , in the absence of an agglutinating agent , settle in a round - bottomed tube as an ill - defined deposit surrounded by a slightly granular film , which would be regarded as evidence of agglutination of fowl cells . resembles closely the " shield pattern " which has been described ( burnet and stone , 1946 ) as typical of agglutination of fowl cells by lipoids . 
proved a it was effective in low concentration ( 0.005 m ) , very satisfactory preservative . and though it increased slightly the granularity of deposits of red cells in control tubes , it had no haemagglutinating action which could be confused with that of tumour extracts , even in concentrations much higher than this . it was slowly lytic for mouse red cells ( though this did not interfere with tests read after the usual period of two hours ) but not for those of other species . 
a final concentration of 0 01 m ( 0 12 per cent ) was generally used ; this was conveniently obtained by adding to a tumour extract 1 / 50th of its volume of a saturated aqueous solution of b.a.l. 
brought about regeneration of the activity of inactive extracts to their original titre . this regeneration was progressive : some activity was apparent in a previously inactive extract a few seconds after the addition of b.a.l. , but the full titre was not reached for about an hour , at room temperature . table i shows the preservation by b.a.l. 
fowl cells of each type , distinguished by a previous test against kahn antigen , were included in this test . it will be seen that rabbit cells were agglutinated by the tumour extract to lipoid agglutinable and far higher titre than those of any other species tried . lipoid non - agglutinable fowl cells were agglutinated to the same low titre . tumour extracts varied somewhat with regard to the ratio between titres for the titre for rabbit different red cells , but these variations were not constant . cells was always between 4 and 16 times the titre for mouse cells . extracts treated in various ways , to be described later , were tested in most cases against rabbit and mouse cells . 
red cells which were agglutinated to low titre by c57 were inagglutinable by s37 extracts . extracts of all the tumours tested lost their activity on standing , though at varying rates , e.g. 
extracts of c57 sarcoma took about 24 hours to become inactive , but extracts of c57 / lh1 , sarcoma , though initially often of similar titre , became inactive in one hour , or less . the loss could be prevented , or reversed , by the addition of b.a.l. occurrence and distribution of haemagglutinating agent in normal tissue . extracts of mouse liver , spleen , kidney , heart , lung , brain , voluntary muscle , lymph gland and thyroid , derived from both normal and tumour - bearing mice , were found not to agglutinate mouse red cells ; and for a time it was thought that the haemagglutinating agent was confined to tumours . examination of a wider range of normal tissues , using rabbit as well as mouse red cells , showed that this was not so . extracts of several tissues , notably adult mouse testicle , ovary , uterus and voluntary muscle , as well as whole mouse embryo and placenta , agglutinated the haemagglutinating rabbit red cells and sometimes mouse red cells also . titres of these extracts were , in general , low compared with those of extracts of mouse sarcomata , but comparable with those of extracts of some of the other table iv gives the range of haemagglutinating titres for tumours examined . rabbit , mouse and human red cells , of a number of normal tissue extracts . haemagglutinating power of these extracts declined on standing , and was preserved , or regenerated , by the addition of b.a.l. 
0 - 01 m added after standing 22 hours at room temperature figures represent reciprocals of haemagglutinating titres for rabbit red cells . some other properties of the haemagglutinating agents of tumrnours and normal tissues . action of normal serum on haemagglutination . - haemagglutination by lipoids is inhibited by normal serum in high dilution , while haemagglutination by viruses is unaffected by normal sera , but inhibited by specific antiviral sera ( burnet and stone , 1946 )  . the effect of normal horse serum on haemagglutination by tumour and normal tissue extracts was tested . extracts were mixed with equal volumes of a 1 in 100 dilution of horse serum , and the mixtures tested for haemagglutination in the usual way . 
an experiment similar to the last showed that addition of either of these sera had no effect on haema gglutination by either c57 or s37 sarcoma extracts . effect of temperature at which the test is performed on haemagglutination . 
than at room temperature ( stone , 1946 ; burnet and stone , 1946 ) , while haemagglutination by influenza virus is more active in the cold than at room temperature or 37 c . 
 ( salk , 1944 )  . haemagglutination by extracts of c57 and s37 sarcomata , and of normal mouse embryo and adult uterus , was tested at approximately 4 c . , at room temperature , and at 37c . 
overnight. neither rabbit nor mouse presence of complement had no detectable effect : cells were lysed and their agglutination by the tumour extract was unaffected . absorption of haemagglutinating agent by red cells . - - c57 sarcoma extracts were absorbed with rabbit , mouse , and fowl red cells , under various conditionts . the following is a representative experiment . samples of 20 per cent extracts of c57 sarcoma , ( i ) fresh , i.e. 
for three hours , and centrifuged ; the supernatant fluids were removed and the cells finally resuspended in the original volumes of saline , and examined for persistent agglutination and for agglutinability . 
fowl cells , which were only very slightly agglutinated , did not absorb appreciably . in all except one case red cells agglutinated during absorption were unsuitable for subsequent tests for agglutinability because they remained agglutinated . the exception was mouse cells used to absorb fresh extract . these , though agglutinated in the presence of the extract ( 30 minutes at room temperature ) redispersed during the subsequent incubation with saline . 
the difference is probably quantitative . gross ( 1947 ) has reported the presence of haemolytic agents in several tumours . haemolysis by such an agent , if of low titre , would be active only in the first one or two tubes of a haemagglutination test and , since these contain only 1 / 450th of their volume of packed red cells , haemolysis might be masked by the small amount of haemoglobin present in all crude tissue extracts . 
had been added before , and those to which it had been added after , heat treatment . a heavy precipitate formed in the heated extract , which was spun out before testing for haemagglutinating power , and it was thought possible that the haemagglutinating agent might be adsorbed on the precipitate . however , no agent could be recovered by extracting the precipitate with m / 15 na2hpo4 . the effect of digestion of tumour extracts by trypsin or papain depends on whether they contain b.a.l. in the absence of b.a.l. , extracts of c57 , or of c57 / lh1 , sarcoma incubated at 37 c . with trypsin or papain ( activated with kcn ) for an hour , were found to be irreversibly inactivated , i.e. 
0005 m 0 - 01 m + , , trypsin 0.5 per cent of commercial powder ( hopkins & williams )  . all mixtures buffered at ph 8 with m / 15 phosphate , 2 drops of chloroform added as baoteriostatic ; neutralized , and b.a.l. 
0.005 0 ' 01 m casein was " light , soluble " of british drug houses , dissolved in m / 15 na , hpo , by heating relevant conditions as in a . 1 hour on a water - bath . it will be noted that there was a considerable irreversible drop in titre of a control sample of sarcoma extract incubated without b.a.l. 
to such extracts gradually falls . it seems probable that this effect is due to the action of tissue proteases . the effect of tryptic digestion on extracts of normal mouse tissues was also tried . it is difficult to obtain such extracts with haemagglutinating titres high enough to make this test satisfactory . in an experiment in which a mouse embryo extract with a haemagglutinating titre for rabbit cells of 1 : 4 was digested with trypsin , with and without b.a.l. , activity appeared to be destroyed in 1 . 
on proteolysis was a 20 per cent extract of c57 sarcoma in m / 15 phosphate buffer ph8 was incubated ( a ) alone , ( b ) with trypsin , ( c ) with trypsin , and b.a.l. 
they show that , with casein as substrate , after 1 hour 's incubation there was no detectable inhibition of proteolysis by b.a.l. ; but with both casein and tumour extract as substrates , after 21 hours ' incubation there was definite inhibition : about 50 per cent by b.a.l. 
elliott , on the haemagglutinating power of a tumour extract , with and without b.a.l. , was essentially similar to that of commercial trypsin . the haemagglutinating agent does not become dialysable through cellophane after digestion of a b.a.l. - containing tumour extract with trypsin . lecithinase : it has been shown by stone ( 1946a ) that the haemagglutinating action of lipoids , and of vaccinia and ectromelia viruses , which probably owe their haemagglutinating action to lipoid components , is destroyed by cl . 
to 0 01 m was then added , and haemagglutinating in a similar experiment mouse embryo extract was treated with the results showed that incubation with lecithinase had no detectable effect on the ' ' haemagglutinating agents of c57 sarcoma or mouse embryo extracts . haemolysis by lecithinase present in the mixtures was not rapid enough , in the presence of b.a.l. , to interfere with haemagglutination . action of heavy metals and oxidizing agents , and its reversal by b.a.l. 
to samples of fresh , actively haemagglutinating , sarcoma extract , not containing b.a.l. , cus0o4 was added , to give final concentrations of m / 300 and m / 3000 . in both mixtures haemagglutinating activity disappeared within a few seconds ; there was a partial return of activity in the later , but none in the former , after addition of b.a.l. 
the haemagglutinating activity of these mixtures declined on standing at the same it thus appeared that the presence of heavy metals rate as that of a control . was not essential for natural inactivation . the addition of various oxidizing agents to a fresh sarcoma extract destroyed or reduced its haemagglutinating activity . 
the list includes serum antibodies ( naturally occurring , acquired , or experimentally induced ) , many viruses ( hirst , 1941 ; nagler , 1942 ; burnet , 1945 ; lush , 1943 ; burnet and stone , 1946 ; mills and dochez , 1944 ) , purified lipoids ( stone , 1946b ) , bacterial extracts ( keogh , north , and warburton , 1947 ) , the globulin fraction of egg - white ( commission on acute respiratory diseases , 1946 ) , some plant proteins such as ricin and abrin , basic proteins such as protamines and histones , inorganic colloidal acids and bases such as colloidal silicic acid , and many metallic salts ( landsteiner , 1945 )  . 
they are labile , while the latter are both fairly stable substances ; their red - cell species specificity is different from that of both lipoids and viruses ; they are unaffected by cl . 
welchii toxin , which destroys the haemaggluthinating power of lipoids and of vaccinia and ectromelia viruses ; their action is unaffected by normal serum , which inhibits that of lipoids but not that of viruses . in the manner in which temperature affects haemagglutinating titre they differ from lipoids . 
a sarcoma extract is absorbed by red cells which it agglutinates , but the cells , when they redisperse , as they do under certain conditions , are fully agglutinable by the same agent ; red cells agglutinated by a virus may also redisperse , but are then inagglutinable by that virus , and often by some others also ( burnet , beveridge , mcewin and boake , 1945 )  . egg - white is more like the tissue extracts in its haemagglutinating properties than are the other haemagglutinating substances referred to , particularly in respect of red cell species range , and effect of temperature on haemagglutinating titre , but it is not - reported to be labile . the general properties of the haemagglutinating agent of tumours suggest that it is a readily oxidizable substance which is active only in the reduced state . it may be a sulphydryl compound , but there is at present no positive evidence of this . neither inactivation by heavy metals , nor by oxidizing agents , is conclusive on this point . 
ascorbic acid , are ineffective , suggests that preservation is a specific effect of sulphydryl . natural inactivation does not appear to depend on the presence of heavy metals in an active state , and therefore it is unlikely that its prevention by b.a.l. 
has been stated not to inhibit the action of trypsin or papain ( webb and van heyningen , 1947 ) , but this work has been repeated here , with a it has been shown that b.a.l. 
protects it from the former . certain physical and chemical properties of the haemagglutinating agent of reasons are given for regarding it as an easily oxidizable it is destroyed by proteolytic b.a.l. 
was found to have definite inhibitory action on proteolysis by trypsin , the haemagglutinating agents of tumours and of normal tissues differ from and on digestion of egg - yolk by lecithinase . haemagglutinating viruses and lipoids in important respects . no qualitative differences have been found between the haemagglutinating agents of different tumours , or between those of tumours and normal tissues . the author gratefully acknowledges his debt to professor j . 
the possibility then had to be considered whether the hereditary condition acted through genetically transmitted differences in ovarian functional activity , or through an unequal response of mammary glands or genital tract to ovarian hormone . 
numerous and extensive observations were made with somewhat conflicting results , both on the nature of the oestrous cycle and on variations in organ sensitivity to hormonal stimulation , in strains of mice with differing mammary cancer incidence . when the existence of the third factor , i.e. 
as the number of determinations was so small , no statistical analysis of the figures was made , but there appears to be no real difference between the strains themselves , nor could the changes produced by foster - nursing be correlated with the presence or absence of the milk factor . 
armstrong ( b ) the character of the oestrous cycle . ( i ) virgin mice . - daily vaginal smearing of virgin mice of all groups was continued for periods ranging from 56 - 137 days immediately following canalization or weaning . 
the number of complete cycles during the observation period in addition , the average length of the whole cycle and of the was recorded . comparison actual period of heat for each mouse was calculated ( table ii )  . was then made between the fostered and non - fostered groups ( table iii )  . all cases comparisons show no significant difference . 
the p factor being of the order of o 1 - 0 5 . a second series of estimations was then made , in which two types of atypical cycle were excluded , in view , of the fact that such cycles might have been caused in the one type , a prolonged dioestrous by the repeated smearing technique . interval is observed , a state termed pseudo - pregnaney . this occurs naturally following sterile copulation and artificially following a great variety of stimuli . parkes ( 1926 ) regarded 7 days as the shortest duration of natural pseudo - pregtherefore all cycles with dioestrus greater than 7 days have been nancy . in the other type there is prolonged cornification or regarded as atypical . heat , a condition which has been produced experimentally by repeated vaginal smearing . 
the death of so many mice while still showing oestrous cycles detracts from the value of the results , but there was some indication that the range of age at which the menoe . 
from table i it is seen that vaginal canalization occurred later in group 3 ( free from milk factor ) than in group 1 ( having natural milk factor ) , but that the effect of foster - nursing was to increase the age in both cases , so that this cannot be correlated with the administration or withholding of milk factor . 
no undue importance has been attached to this as it occurs in the riii groups , in which foster - nursing is an unsatisfactory procedure , due to the possibility of the offspring receiving milk factor from their mothers during the interval between birth and transference to foster - parent ; also the difference is not statisticllay significant when all cycles are included and the samples are small . on comparing the two strains ( table iii ) there is some indication that the nature of the cycle shows a strain difference , which is unaffected by foster - nursing . comparing these results with the features of the oestrous cycle as described by other workers , there are , in general , appreciable strain differences in this respect ( table vi )  . it may be noted that the average duration of the cycle in young cba mice as observed by bonser ( 1935 ) is closely comparable with that obtained in the present experiment - 5 - 8 and 5 - 3 days respectively . foster - nursing as a means of administering the milk factor appears to be an entirely satisfactory procedure . thus the fact that no significant change in the character of the oestrous cycle was induced by this means , would seem to indicate that the factor does not influence the cycle . it is possible , however , that some adjustment to the new conditions created by the foster - mother 's milk is made during the period of suckling . the milk factor effect might be counteracted by the time puberty is reached and the hereditary condition alone revealed in the characteristics of the sexual cycle . the distribution and extent of two forms of atypical cycle were stuidied , as it was thought that , if they were caused by smearing technique , their incidence might vary in the different groups of mice . should , however , such cycles occur spontaneously , any observed strain difference in the duration of the cycle or e . 
bonser for her guidance and interest in the planning of this work and for her co - operation in the experimental procedure , which made consecutive daily observations over such a long period possible . i also wish to thank j . 
jv.7. reeeived for publication march 5 , 1949 . the pressure mincer described in this article was designed to facilitate the preparation of tumour suspensions for a quantitative studv of the survival of tumours in the frozen state . 
the choice of principle and design was determined by the foflowing requirements : ( a ) rapid reduction of tumour tissue to a suspension of fine fragments and separated ceus , ( b ) ease of aseptic manipulation , ( c ) mechanical simpficitv and ( d ) ease of cleaning . the essential feature of this instrument is a grooved plunger which operates in a closed eyfinder . 
the tissue is placed below ' the plunger , and on the application of pressure is forced through the grooves to the upper face . the niincer and its component parts are shown in fig . 
1. all parts are machined from brass and are chromium plated . * it is important to have the plungers ( c and d ) fitted to the body tube ( a ) with the minimum clearance consistent with smooth working . 
the nose of each plunger fits accumtely into the recess in the base plate ( b )  . similarlv the nose of the fine pliiin er fits accurately into the base of the coarse plunger . 
the diameter of the bodv tube is 1 - 6 cm . thus i mof displacement of the plung - er corresponds to a volume of 0 - 2 ml . cleaning is facilitated and design of the plungers is simplified bv the prov - ision of a detachable base plate . the operating screw ( f ) is of sufficient length to extrude the plungers from the lower end of the body tube . the various parts of the mincer are sterilized separately in glass tubes . 
the mincer is shaken immediately to disperse the mince if the coarse plunger has been used the cap and operating in the suspending fluid . screw are detached and the fine plunger is inserted . tlle cap and screw are replaced and mincing is completmed . the suspension may contain coarse fragments of fibrous tissue or portions of iiiince which have clotted before dispersal in the suspending fluid . these may be removed either by l ' ow speed centrifugation , or by filtering the suspension througli a column of glass ballotini of suitable diameter . the mincer , which is illustrated in fig . 
1 , is the sixth of a series desigiied to all models have proved most satisfactory for operate with grooved plungers . the purpose for which they are intended , and it might be suggested that this tvpe of mincer will , for special purposes , be suitable for preparing suspensions of manimalian tissue or fowl embryos infected with certain viruses or bacteria . i wish toacknowledge my indebtedness to w . 
at the time it was known that adenomas of this gland produced abnormalities in children and young adults ; it was therefore postulated that in later life , when gigantism and acromegaly were no longer possible , increased activity of the pituitary gland might be responsible for the production of tumours ( funk , 1917 )  . for a long time and for obvious reasons it was impossible to put this hypothesis to a test . 
thanks to the classical work of evans , li and simpson ( 1948 ) we now have the necessary tools for preliminary and systematic appraisal of the importance of various hormones of the anterior pituitary in tumour growth . the purpose of the work reported in this paper was to test the effect of various anterior pituitary and related hormones upon the growth of implanted tumours in hypophysectomized rats . 
as a supplement to this work we also dealt with the removal of certain organs ( mainly glands of internal secretion ) on the rate of growth of a transplanted rat tumour in otherwise intact animals . while there is no doubt that studies on this subject have already been made , it appears doubtful whether a systematic study was ever made of the effect of the removal of these organs upon the growth of one particular tumour . 
to check on the completeness of the surgical procedures used we have excised and weighed , at the time of sacrifice , those organs that are in a physiological relationship to the excised gland . for instance , in orchidectomy the seminal vesicles and the prostate were weighed . 
the diet was the same as in the hypoall animals received tap water , except the adrenaphysectomy experiments . lectomized animals , which received 1 per cent saline . in some experiments rats 282 c . 
no improvement in survival was noted . 1 of the controls 40 per cent had open vaginas , none of the castrates , at time of implant . a mortality was about 30 per cent of the animals operated upon . 8 mortality of 33 per cent of the operated animals , probably due to bartonella muria infection . 4 all animals received 60 mg . 
of alloxan from the time of tumour shaefer - hartman blood - sugar determinations were as implantation to the end of the experiment . follows : pre - implant 461 - 9 mg . 
using the enriched diet in our present work , we have attempted to restore tumour size by the administration of some anterior pituitary hormones and serum gonadotropin . growth hormone increased tumour weight of hypophysectomized animals so treated . however , this increase is directly proportional to the increase in body weight due to the hormone . thus , tumour weight difference per g . 
body weight difference is the same for both growth hormone treated and intact animals using untreated hypophysectomized animals as the base . it would appear that the influence of growth hormone on tumour growth is related to its effect upon the general metabolic condition of the animal . this is not true for acth and thyrotropic hormone . these two hormones cause a greater increase in tumour growth than could be expected from their effect upon body growth , using the same criterion . the ratio of tumour weight to body weight gain in adrenalectomized animals seems to confirm the fact that without adrenal hormones the tumour does not grow as well as in intact rats . this is the opposite of the effect ofacth treatment . 
the restorative effect of the latter hormone and the decreasing effect of the operation , greater than their respective actions upon body growth , show a clear effect on the tumour itself . 
our data are not as clear in the thyroidectomy experiments , however ; in one experiment the tumour - body weight ratio is indicative of the depressant effect of this operation upon the tumour . in the other experiment the administration of thyroxine to a thyroidectomized animal had the same effect as thyro286 c . 
ehrlich tropic hormone given to a hypophysectomized animal . increase in tumour size greater than could be expected from the body growth . this effect was an the effect of fsh and serum gonadotropin on hypophysectomized animals was not very marked either on absolute tumour weight or on tumour weight per g . 
body - weight gathe treatment of castrated males with testosterone may have stimulated tumour growth . splenectomy may have had some effect upon increasing tumour size by both criteria . while it is clear that diabetes per se reduces tumour growth , it is not so clear whether or not this reduction is related to body weight . it has been shown by mceuen and thomson ( 1933 ) that the reduced rate of tumour growth in hypophysectomized animals could not be solely attributable to the concomitant metabolic deficiency . in their studies on intact animals , evans , moon , simpson and li ( 1950 ) have found that only by long - continued treatment with growth hormone were they able to produce neoplasms , while shulman and greenberg ( 1949 ) in a shorter experiment , using intact mice , found no effect upon tumour growth with this hormone . 
persons. 0 - 020 0 090 0 219 the difference between any pair of rates for subjects of the same age group men . 0 031 0 070 0 - 509 0 - 018 0091 0 203 is , in no instance , as great as twice the standard error of the difference . * between 0 000 and 0 - 017 , depending on the proportion of the 14 female patients dying of lung cancer who were non - smokers . all areas , england and wales . a____ - __ an opportunity to test the first assumption is provided through the courtesy of the government social survey by the use of figures for the proportions of nonsmokers in the population , obtained in the course of an independent inquiry . the subjects were interviewed in september 1951 and were a random sample of the whole population ; the definition of a " non - smoker " was the same as that used by doll and hill ( 1952 )  . 
the total number of subjects interviewed between the ages of 21 and 74 was 2 , 268 ; the numbers in each age and sex group were proportional to the numbers in the whole population and the numbers of men interviewed - particularly in the older age groupswere considerably smaller than the numbers used for the previous calculations . the results obtained by the use of the government social survey figures for the estimation of the numbers of non - smokers living at june 30 , 1950 , are shown in table v . 
1 it is seen that the estimated rates for non - smokers are ( with one exception ) slightly less than the rates for women in rural districts - that is , the lowest recorded by the registrar - general . 
the exception , the rate for non - smokers aged 25 to 44 , is derived from the experience of the smallest number of bronchial carcinoma patients and is likely to be the least reliable ; this rate lies between the lowest and the lowest but one of the registrar - general 's rates . the estimated rates are , therefore , of the order which could be expected if they represented the basic minima independent of variable environmental factors . proportion of deaths due to causes other than smoking . if the estimated rates for non - smokers are accepted as appoximately accurate , it is possible to calculate the number of deaths from lung cancer in persons between the ages of 25 and 74 which would have been expected , in the absence of smoking , by multiplying the populations given in table i by the rates for all persons given in table iv and adding the results for each age group . the number expected in 1950 would have been 1 , 875 ; the number which actually occurred was 11 , 189 . it must be presumed that the other causes of lung cancer continued to operate irrespective of the use of tobacco , and it is , therefore , concluded that about one in five of the lung cancer deaths in persons aged 25 to 74 in 1950 , were attributable to causes other than smoking . sex ratio among non - smokers . table iv shows no consistent difference between the estimated rates for men and for women ; and in the age - group 45 to 64 , for which the rates must be presumed to be the most reliable because derived from interviews with the greatest number of patients , the rates are most nearly equal . 
the data are , therefore , not grossly inconsistent with the hypothesis that in the absence of smoking there is no appreciable sex difference in the incidence of lung cancer . the closeness with which the data fit the hypothesis can be seen more readily if the rates for women ( derived from greater numbers of non - smokers than the rates for men ) are used to calculate the number of non - smokers among men with bronchial carcinoma who would have been expected to have been interviewed , if men and women suffered the same mortality . for example , the mortality rate for women aged 45 to 64 , and resident in greater london , is estimated to be 60.6 / 673 , 000 ( table iii ) ; the estimated number of male non - smokers in the same age and area of residence sub - group is 38 , 100 ( table iii ) , so that the expected number of male non - smokers dying of lung cancer in 1950 is ( 60.6 / 673 , 000 ) x 38 , 100 = 3 * 43 . altogether 1 , 473 men in this sub - group died of lung cancer , 308 r . 
the expected numbers are calculated similarly for each sub - group when , by addition , the total number of male non - smokers expected to have been interviewed is found to be 6 - 1 . 
the number actually observed was 7 . the conclusion that in the absence of smoking there is no appreciable sex difference in the incidence of lung cancer appears to be contrary to the observations reported earlier that the mortality among women in greater london was lower than that among men at each level of tobacco consumption ( doll and hill , 1952 , table xii )  . 
the observations recorded among smokers are , therefore , not incompatible with the findings among non - smokers . mortality among non - smokers in different areas . from table iv it appears that there are no consistent differences in mortality among persons resident in areas of different density of population . moreover , the rates for greater london , other urban areas and rural districts are most nearly equal in the age - group 45 to 64 in which they are likely to be subject to the least error . the essential similarity of the rates , in the absence of smoking , can be seen more readily by a method similar to that used for comparing the mortality in men and in women . 
since there is no reason to presume that any one set of rates is more reliable than another , it is preferable to calculate the number of nonsmokers with bronchial carcinoma , resident in each type of area , who would have been expected to have been interviewed , if the estimated rates for men and 310 r . 
the data are not accurate enough for an aetiological relationship to be postulated . " no difference was found in the incidence of past attacks of asthma , chronic nasal catarrh , pleural effusion and pulmonary tuberculosis between the patients with lung carcinoma and those with other forms of cancer . 
the data did not suggest that the effect of smoking was through the intermediary of other respiratory diseases . should , however , pneumonia and chronic bronchitis really predispose to the development of bronchial carcinoma independently of any association they may have with smoking , it might be expected that their effect would be seen more clearly among non - smokers than among the whole population , in whom another cause can frequently be implicated . 
the past history of respiratory illnesses has , therefore , been analysed in the 47 patients who were non - smokers and the incidence of each disease compared with the incidence which would have been expected from the experience of all patients with bronchial carcinoma of the same sex and age groups ( table viii )  . it is clear that the data provide no evidence 312 r . 
pected. 5 * 2 62 summary . a " non - smoker " is defined as a person who has never consistently smoked for as long as one year at the rate of as much as one cigarette or one gramme of tobacco a day . estimates of the mortality rates from lung cancer among non - smokers are obtained from the registrar - general 's figures for the number of deaths attributed to lung cancer and for the total population ; and from the data , obtained in a clinical inquiry into the proportion of non - smokers among patients with bronchial carcinoma and among patients with other diseases ( excluding cancer of the oral cavity , respiratory tract or intrathoracic organs )  . the assump - tions required to enable the estimates to be made are bold and the number of cases of bronchial carcinoma among non - smokers is small . the rates obtained are , therefore , highly speculative , but it is thought that they are likely to be reasonably reliable since they are consistent with other experience . it is concluded : 1 . 
that occupational hazards and the previous occurrence of certain respiratory diseases are unlikely to be of frequent aetiological importance . i am most grateful to the officers of the government social survey for permission to make use of data collected during one of their inquiries and to trade sources for data of tobacco consumption , summarised in table vi . i am deeply indebted to professor a . 
of particles of 3 diameter or less during a 6 - weeks period : seven rabbits survived the injections for 7 months or more , and all developed malignant osteosarcomas , often with multiple primary sites . 
 we have repeated these experiments , using zinc beryllium silicate and beryl lium silicate and confirm the findings of gardner and heslington ( 1946 ) , although the proportion of survivors developing tumours is less in our series . 
x - ray analysis has shown that zinc beryllium silicate is really a solid solution of z11iisio4 and be2sio4 an analysis of the zinc beryllium silicate used in experimental groups b and c ( table i ) gave a composition zno 67 per cent , sio2 31 per cent , beo 2 per cent . 
the complex injected in experimental group a ( table i ) contained manganese , and had a composition zno 67 per cent , sio2 28 per cent , beo 2 per cent , mno 3 per cent . 
 examination of the tissues of animals dying immediately after injection and between 14 and 83 weeks after the injection of the silicates has shown the presence of silicate particles in the lungs , spleen and liver of all injected animals . 
the macro phages of the spleen first form giant cells of the foreign body type and even of the langhans type , but later the particles are contained in large syncytial masses , which show up to 100 nuclei in a single section . 
for some months the particles are present in isolated kupffer cells , but 3 to 4 months after injection the kupffer cells have increased in size and number to form cellular masses that fill and often distend the sinusoids . 
 the nodules are present in all injected animals whose bones have been searched for them , and in many cases are not associated with any other abnormality , either histological or radiological . 
these : findings correspond closely with those for rabbit 4 , where consideration of histological material in conjunction with radiographs leads to the conclusion that the radiographic appearances result from occupation of the marrow cavity by ossifying tumour tissue . 
histological examination of the femoral shaft shows a complete replacement of the normal marrow by tumour tissue , quite comparable to that seen in more advanced lesions in other animals , but not yet expanding the periosteum or causing erosion of the cortical bone of the sha part of the tumour is bony , part cartilaginous , while some areas consist merely of anaplastic spindle - celled tissue . 
numerous fat cells are scattered through the area , and the tissue varies from an almost acellular mass of fibres to a tissue composed largely of rounded and elongated fibroblasts . 
5 shows such an area , where a network of recently - formed bone - trabeculae is present , and where the osteoblastic cells covering the surfaces of the trabeculae are linked to the intervening fibroblasts by numerous intermediate forms . 
on the left side of the bone a few areas show a similar pattern , but there is also some more diffuse aggregation of radio - opaque material , corresponding to the formation of calcified cartilage by the tumourtissue . 
 in the lower part of each femur the marrow is completely replaced by a mass of bone - forming tumour tissue , which has begun to extend into the haversian canals of the dense cortical bone . 
some areas consist entirely of cartilaginous tissue , others show extensive osteoid and bony differentiation , while in some places the two tissues merge into a composite " osteochondroid " pattern . 
in several situations this was beginning to invade the dense cortex of the bone concerned , and to expand the covering periosteu in this animal the body of one lumbar vertebra contained a small rounded area of calcifying spindl~ - celled tumour tissue , 2 m in diameter , sharply demarcated from the surrounding normal marrow . 
this suggests that a continuous process is concerned in the development of frankly malignant tissue from the earlier pre - invasive lesion seen , for example , in the humerus of rabbit 4 . 
of soluble berylliu treatment of the refractory beryijium silicates with n , 100 hydrochloric acid produces a 10 to 20 - fold increase in the proportion of soluble beryllium in the aqueous suspension . 
 when stained by the method developed by denz ( 1949 ) for the histochemical detec tion of beryllium these sections showed that some soluble beryllium had left the necrotic area and stained the surrounding fibrous tissue faintly an_d diffusely . 
while the fully _developed tumours present a very different appearance from the medul lary bone formation that has been described as an early stage of malignancy , all stages of transition between the two can be traced . 
it is suggested that these indicate a continuous process of transformation from the early medullary : fibrosis to the later obviously malignant lesions , but this is only the interpretation of a number of morbid anatomical observations . 
 the relationship between the small nodules which are the first change seen within the bone marrow and the subsequent : fibrosis and malignant change is uncerta the nodules produced by the silicates containing beryllium and those produced by the zinc silicate are indistinguishable by the usual histological methods . 
it seems clear , however , that it is the presence ofthe beryllium within the nodule that is in some way responsible for the progressive changes that lead eventually to malignancy . 
although the beryllium silicates are considered to be insoluble , the observations on material injected intradermally into a rabbit showed that beryllium can be liberated from the particles and can diffuse into the surrounding tissues . 
 _therefore , if beryllium is to be held directly responsible for the tumours , it is much more likely that this beryllium is liberated from deposits in the marrow rather than derived from more distant deposits . 
the possibility that the silicate may play some part in the development of the tumours is excluded by the fact that gardner and heslington ( 1946 ) produced tumours with beryllium oxide , and more recently barnes ( 1950 ) has reported that two rabbits that received intravenous injections of a suspension of beryllium metal particles have developed characteristic sarcomas . 
 it is also apparent that the tissues themselves must contribute a factor , because similar nodules in the liver and lungs arouse very little : fibrous tissue reaction , while in the spleen : fibrosis and atrophy may go to extreme lengths without showing evidence of malignant change . 
 since this paper was submitted one further rabbit has died with a sarcoma of the pelvis 30 months after the last of a series of injections of zinc beryllium silicate . 
 the materials used in these experiments were supplied to us by the research laboratories of the general electric company , wembley , to whom we would like to express our thanks . 
1. given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . most people would agree that studies with transplanted tumours have given information concerning the autonomy of malignant tumours and concerning their histogenesis . however , there is a tendency to regard such studie8 as somewhat old - fashioned and this field of study more or less closed . in this paper it is hoped to show that there is still valuable information to be gathered of significance for general biology as well as oncology . general biology and tumour transplantation . the genetical laws governing the transplantation of normal and malignant tissues are now generally accepted . in both cases a complex of dominant genes is concerned which snell ( 1948 ) has called histocompatibility genes . there have always been two schools of thought conceming the nature of these genes , gne that the genes determine iso - antigenic differences , the other that they deterinine " individual differentials " - substances with somewhat mysterious and ill - defined properties . it is not easy to study these questions with normal tissues for technical reasons , one of which is that the number of factors is always high . 
with tumours the number varies , but may be low , and in addition tumours stimulate a better antibody response . iso - immune reactions are most easily studied in the erythrocytes , and it so happens that certain important iso - antigens in strong 's a strain of mice are shared by the erythrocytes and fixed tissues . 
four tumours from this strain have been studied genetically and serologically . the first two were studied in england ; in both it appeared that two histocompatibility genes were concerned , one of which was identical with a gene for an antigen known as antigen ii . 
by serological means it was shown that the occasionally iso - antibodies tumours contained another antigen in addition to 11 . were formed against it , but too irregularly 4nd at too low a titre to be of value for genetical work ( gorer , 1937 , 1938 , 1942 )  . those studied in america were both found to give single gene ratios in backcrosses . 
furthermore , in conjunction with snell and lyman ( gorer , snell and lyman , 1948 ) it was possible to show close linkage between antigen 11 and the locus for " fused " ( a tail anomaly )  . full information is to be published elsewhere , but it can be seen from table 11 that the linkage is close . 
the sera were produced by inoculation of c57 blacks . the similarity is not shown to the same degree by all sera . provisionally called h2 and h2d ( table 111 )  . closely related antigens occur in strains cba and - cm , so perhaps , there is a long series of alleles at this locus . animals carrying the we are not certain how many cross - overs there were . gene for fused may have norm ' al tails , and there are other difficulties associated with tumour transplantation that will be discussed later on . in backerosses involving 257 animals the recombinations were between 0 and 5 per cent . previous to these studies strong ( 1929 ) had used tumour transplantation to show sex linkage of a histocompatibility gene , and bittner ( 1933 ) found loose linkage with " dilution . " the location of h2 was first found by snell and lyman using tumour . 
inoculation without serological testing , and i hope i am betraying no confidences by saying that they have other instances of linkage as well . will be seen that tumour inoculation is - a most useful weapon in mapping chromoit is best to use serological tests as well . 
without going into details it may be said that they were not serologically unifortumour transplantation indicates that this polymorphism may be maintained by a high pure strains unless kept on a very small scale automatically mutation rate . it was shown by bittner ( 1935 ) that a dba crystallize into various sub - strains . tumour would not take in all sub - strains , and this has been found to be a common finding , having been seen with various tumours arising in strains c57 black ( law , gorer , unpublished ) and cm ( gross , 1947 )  . 
we have as yet no ' evidence that liability to disease is influenced bv antigemc constitution , or indeed very little knowledge of the antigens ' perhaps the polymorphism is connected with the risk of functions in the cell . iso - i ' mmunization during pregnancy ; this must be great where foetal absorption is common . 
if a species were completely uniform the risk would vanish , but it is unlikely that any species would be completely so over the whole of its rangle . on the other hand , if it were sufficiently polymorphic , the danger may be minimized . 
if a male has a rare antigen he would probably be heterozygous , and only half the litter would perish if iso - immunization took place . further , in matings with different males , a female would be unlikely to receive successive doses of lastly , it is possible that if a mixture of a large - number of the same antigen . antigens is received , dangerous titres of antibodies are not formed against any antigen ii does not appear to be very mutable , but here mice one of them . also seem very ' polymorphic . eight pure strains have been examined ; all are somewhat different . 
both the tumours tested in bar harbor gave such a ratio , but it was shown conclusively that they both contained at least two antigens . this is easily explained immunologically . antigens differ greatly in potency . 
gorer it is now well known that tumours may " mutate . " strain , we would get about 50 per cent susceptible progeny ( macdowell and richter , 1932 )  . errors of the above t - vpe are counterbalanced by precisely the opposite effect . some tumours may grow and kill the host in spite of iso - antigenic differences . there is considerable indirect evidence of this , but recently it has been possible to show that an animal succumbing to a tumour derived from any other strain may form high titres of antibodies ( gorer , 1947 )  . 
when first tested a tumour may appear to have upwards of 7 factors ; later on , only one or two . differences of this order cannot be accounted for by errors of the type just mentioned . there this might be due to mutations of domimust be some real antigenic alteration . this is extremely improbable ; one would have to nants to recessive alleles . have 6 or 7 homozygous mutations . 
what may happen is that one or more antigens crowd the others if for the sake of argument we assume that antigen 11 occupies 10 per cent out . of the surface of a normal cell , in a malignant one it may occupy 90 per cent . these experiments have the disadvantage that we have no really satisfactory for example , we can show that the cells of a myeloblastic normal control.. leukaemia contain increased amounts of antigen 11 , but we cannot get enough there is evidence that analogous antigenic normal myeloblasts for comparison . alterations may occur in human tumours . 
it is believed that all mammals ( and perhaps many other forms ) are highly polymorphic for histocompatibility genes . there is evidence that some of these genes have a high mutation rate in mice . 
we are probably all agreed that tumours , although usually , or perhaps always , preceded by abnormal local . this change consists in - an increase in conditions , arise by a sudden change . the rate of growth of a cell or a group of cells . in this way there arises a new cell - lineage distinct from its antecedents , and one which can propagate its new it has the character of a genetic property irreversibly and even indefinitelv . secondary changes may follow establishing subchange , a somatic mutation . sidiary cell - lineages , - some involving further increases of growth - rate and dedifferentiation , and all surviving and multiplying subject to natural selection . to these secondary changes i shall return later . the chemical conditions arising - in the changed tissue h4ve been examined bv santesson and caspersson ( 1942 ) , while the processes of its cell division have been described by koller ( 1947a ) for epithelial tumours and by la cour ( 1944 ) for pernicious anaemia , which is an analogous condition depending on the enhanced multiplication of the red blood precursor cells of the bone marrow . 
a single polymitotic gene in maize and extra heterochromatic chromosomes in millet both cause rapid and unwanted nuclear divisi ' ons in the pollen grain . in maize up to fou - r extra mitoses take place before the chromosomes have had time to divide immediately after meiosis . 
the nucleus is forced into division , and the unsplit chromosomes are scattered on a spindle which merely disperses them into a number of deficient nuclei , each of which is aga ' m compelled to divide before it is ready , and in this way the whole pollen grain is brought to ruin . in millet the mitoses ( also up to the nu ' mber of four ) do not occur before the chromosomes are split , but the whole pollen grain is none the i - ess consumed and killed in the end by the production of redundant nuclei . 
the pollen grain is thus , in , a sense , an encapsulated tumour ( darlington , 1947 )  . comparison of these cases of polymitosis in plants with animal tumours polyinitosis is not due to a somatic enables us to clear our minds on one point . it 4ffects every cell of a mutation . particular type in the body . 
the spontaneous tumour on the other hand arises at random both in time and space . it does not affect all cells of one type , but only one cell , nor is it the first cell of a particular normal type to arise which is affected . 
we are therefore confirmed in regarding the spontaneous tumour as due to a genetic change . this conclusion removes the contradiction between development on one side and heredity and infection on the other by withdrawing to a lower level ofanalysis . the organism is now seen from the cell point of view as a vegetatively propagating colony . 
how far does it enable us to distinguish between nucleus and cytoplasm as the seat of the mutation general the most efficient carcmogens ( such as the hydrocarbons ) and the most efficient agents of nuclear mutation ( such as mustard gas ) do not coincide . ' carcinogens do not damage the nucleus in proportion to their effect as carcinogens ( darlington and koller , 1947 )  . 
thus the nucleus again seems to beexcluded , just as it is by the direct evidence . but the evidence of xray effects is a more serious objection to a nuclear origin . x - ray damage leads to the development of cancer only when the dose has been so heavy as to damage the cytoplasm , and only then after prolonged delay . light doses which have a proportionate effect on the breakage of the chromosomes and the mutation of the 120 c . 
different conditions , in differeni tissues and in different stages of development . now plasmagenes , like all other such determinants , are susceptible to mutation . it is not possible certain of them control the formation of plastids in plant cells . to relate here ( as i have elsewhere ) the long detectiv - e story of investigations which have led in the course of 40 years to the revelation of the character and continuity of the plastid plasmagene . suffice it to say that , like the centromere and nucleolar organizer of the chromosomes , it its stock - in - trade on its back , which being a sac of green pigment marks or tags its owner and enables us to count its numbers in the cell and note its changes : it can mutate from green to white and vice versa , so that cells can occur with mixed green and white plasmagenes ; and , moreover , the same plastid may be starved white , as it were , by a stepmother nucleus , and recover its normal colour when it is put back with its own proper parent . prolonged coitus causes a paramecium to be infected by the kappa plasmagene of its mate . transplantation of an organ or of serum from a c02 - sensitive drosophila infects a nonsensitive fly , including its egg , with the sensitive plasmagene ( sonneborn , 1948 ; l ' he ' ritier ; 1948 )  . these infections , it will be seen , are artific ' ial , or at least unnatural . 
a number of aberrant conditions can be trans ' mitted from stock to scioii , and some even have arisen in a scion after it has been grafted on a healthy stock . these are artificial diseases ; they are not transmitted in nature , but only by grafting . 
we make a great mistake therefore in calling them viruses : they are proviruses ( darlington and mather , 1949 )  . conversely it has been know - n for 40 years that the . 
virus ricketmia is carried by the eggs of its vector dermatocentor . the terror of its infection for man has closed our eyes to the fact of its inheritance for the tick . 
what appears as a virus in one host is indistinguishable from a plasmagene in the other - and it may weh be that the plasmagene is the older ( l ' he ' ritier , 1948 )  . at the same time billingham and medawar ( 1948 ) have sh ' own that a selfpropagating particle.differentiated in development may by its diffusibility enjoy certain of the properties of infection - a situation which can come to our notice only when the particle is as innocuous , and the differentiation as trivial , as the black pigmentproducer of a ' piebald mammal . 
they have never been guilty of infection , and are therefore totally unadapted for or against it . the virus type may well have arisen likewise by mutation of a plasmagene , but it must have been a mutation followed by others adapting it to infection . moreover , this type falls into two groups by a most instructive distinction . 
the milk - agent , on the other hand , cannot be imagined as having arisen anywhere save in the moiise , itself , in whieb it is inherited by the milk instead of by the eggs . how accidental is the distinction between the infectious and the non - iilfectious particle is revealed most strikingly by one true virus . 
but in its new host it not only it even ceases to be inoculable . it loses the property ceases to be infectious ; of infection , and becomes transferable , if at all , only in whole cells . this is just the opposite transformation to the one by which proviruses arise or demonstrate their existence when two plants are grafted together . 
ob ection8and di ffil cultie8 . three grounds for suspicion of the plasmagene origin of cancer are now worth first , the cancer agents have one characteristic which will at once discussing . be noticed as marking ' them off from all previous plasmagenes . 
now the inheritance of lethal mutations out of the running . in the nucleus , when they are recessive in their lethality , is mendelian and can therefore be followed in experiment . 
a whole tissue can be destroyed by rendering its there is , however , no contradiction between nuclei unworkable in this way . the nucleus is the assumptions of a cytoplasmic cause and a nuclear cure . that is especially easy the only wheel in the cell that we can put a spoke in . to do in rapidly dividing cells ( darlington and la cour , 1945 )  . 
we are therefore merely attacking the malignant cell where it is weakest . incidentally the effect of irradiation in breaking the chromosomes and stopping the growth of the cells leaves no doubt that the remarkable deficient nuclei found in tumours by koller ( 1947b ) will have a limited life . 
the particle analysis : competitive propagation . the cancer miita - tion , as we saw , is often followed by other changes beyond these may be described under the the primafly one of change in growth rate . headings of dedifferentiation or the loss of tissue character , metastasis or migration , secondary mutation and various breakdowns of mitosis and of chromosome structure . 
what we now have to ask ourselves is how far these secondary changes require secondarv assumptions , and how far they are implied by the primary on.e. recent experiments equally with flies , infusoria and tomatoes liave revealed to us the conditions of normal development . 
thev have shown that it is iiot merely ebaracterized by adjusted between nucleus and cytoplasm , but between different self - propagating constithese adjustments can be broken down under experituents of the cytoplasm . in polymental conditions , with results which have ' been ace - lirately described . mitotic maize , as we saw , the cytoplasm runs away from the nucleus : in polyin paramecium , in mitotic millet the nucleus runs away from the cytoplasm . c02 - sensitive drosophila , and in rogue tomatoes , the whole system at a high temperature can be made to run away from a particular plasmagene . 
bv rapid growth the 250 kappa particles of one cell can be run down to one ( from which they can recover ) and then finally to zero ( from which thev cannot recover ) , so that the cell lineage has mutated . 
and in most virus diseases of course the virus runs away from the rest of the system or vice versa ; only occasionally is equievidently therefore the cell contains self - propagating elements librium reached . these limits are exposed in with different limits to their speeds of reproduction . a protozoan or a plant when the temperature is raised . 
these three classes of particle are conditional and interchangeable . cancerproducing particles fall into all three . the origin of cancer can therefore be ascribed to mutations in cytoplasmic determinants , indifferently infectious or non - infectious , which make themselves visible by causing the resumption of growth . further , the study of plasmagene and virus inheritance in relation to differentiation reveals a competitive propagation of cytoplasmic particles . this explains both the genetic control and the secondary development of cancer with its potential dedifferentiation and metastasis . the discovery of , not the cause , but the system of causation of cancer tells us nothing immediately about the cure that we do not already know . 
althougih biologists have for long been uneasily aware of the existence of a problem of cell heredity , its systematic analysis is the work of very recent cell heredity deals with the origin and maintenance of inherited character years . differences between cells ; more particularly , between cells that set up division its problems present themselves in their most acute , lineages by mitotic fission . if not most easily workable , form in metazoan development . the outcome of cellular differentiation in ( say ) mammalian development is the formation of a limited number of histologically definable cell genera , each one further subdivided into a variety of cellular genetic species . 
the genus " fibroblast , " as yet far from completely analysed , may be subdivided into cells which manufacture bone , cartilage , white connective - tissue fibres , and so on . genus " epidermis , " of which we have made a particular study ; includes the epidermal epithelium of the superficial skin , of the sole of the foot , the tongue , cells of each of these epidermal the claws or nails , the vagina and the cornea . species display a distinctive combination of structural or physiological properties . the epidermis of the sole of the foot , for example , has a characteristically high rate of cell division . 
but this has proved not to be the case . although plausible " phenocopies " of sole epithelium ( in the form of corns and callosities ) can be made by irritating the thin and relatively quiescent skin of the body surface , the difference between the division rates of sole and body epidermis is in fact " intrinsic " and inheritable . 
we have , for example , transplanted sole epidermis to positions in the body where it is protected by neighbouring hair and secure from mechanical irritation ; but even so , its characteristic growth rate has been maintained for at least two years , and thick pads of now functionless cuticle continue to form over it and may periodically be removed . claw epithelium tells the same story - more clearly , since the difference between claw and body epidermis is anatomically crude and obvious . 
bartholomew 's hospital , london , e.c.1. received for publication december 22 , 1948 . in an earlier publication ( robinson , 1948 ) the results obtained in a study of 17 - ketosteroid excretion in men of different age - groups were reported . special attention was paid to quantitative dlifferences in total ketosteroid excretion during the later decades of life . 
the method involves adsorption of the 17 - ketosteroids on a column of alumina from benzene solution followed by fractional elution with benzene of increasing ethanol content . the amount of 17 - ketosteroid present in each eluate is determined by the zimmerpreliminary experiments with the method described by these mann reaction . authors showed that separation and estimation of the steroid components could be achieved , but that reproducible results depended on careful standardization of the alumina and of the conditions of elution . 
of total 17 - ketosteroid was found to be the most suitable amount , and sufficient urine from a 24 or 48 - hour collection was hydrolysed and extracted to furnish a quantity in excess of 5 mg . 
was evaporated to dryness , and two successive portions of pure benzene ( 5 ml . ) added and distilled off to remove the last traces of alcohol prior to solution in benzene for adsorption on alumina . ( 2 ) stamndardization of alumina and adsorption columns . since merck 's alumina was not available , many samples of alumina were examined in order to obtain a product with the desired activity . spence " type h " alumina was finally selected for this purpose . 
when samples of this alumina are exposed to air ( by spreading the material in thin layers and exposing it to the moist air of the laboratory ) they gradually lose their adsorptive activity . this loss of activity is accompanied by a decrease in ph of aqueous suspensions of the alumina . suspensions prepared by mixing alumina with distilled water ( 1 part a1203 with 2 parts distilled water , by weight ) show an initial ph of 105 before deactivation and a gradual decrease to ph 9 - 3 after 2 to 3 days ' deactivation . the adsorptive power of the alumina was checked at intervals during the deactivating process by employing brockman 's method of standardization , using mixtures of dyes ( brockmann and schodder , 1941 )  . 
gurr , and further purified by solution in benzene and filtration through alumina followed by crystallization from benzene ( sudan red ) or alcohol ( sudan yellow )  . for standardization , 1 ml . of this dye solution is adsorbed on a column ( 50 x 14 mm . ) prepared from a suspension of alumina ( 7 g . ) in benzene - petroleum ether ( 1 : 4 ) and eluted with 30 ml . 
the alumina is considered to have suitable adsorptive power when the yellow band reaches the bottom of the column , while the red band moves down about 10 mm . the alumina columns for adsorption of the urine extracts are contained in glass tubes of 14 minternal diameter fitted with glass taps at the lower end . above the tap a plug of cotton - wool is inserted and the alnmina filling is added above the plug . 
fractions. these fractions are numbered successively 1 - 43 . ( 4 ) assay of eluted fractions . the solvent is removed from each fractional eluate and the residue dissolved in 2 ml . 
the observed colorimetric values are corrected when necessary for interfering chromogens ( robinson , 1948 )  . ( 5 ) recording of chronatograms and identification of con8tituents . the amount of 17 - ketosteroid in each eluate is plotted as the ordinate against an abscissa corresponding to the serial number of the eluate . 
with normal urine as many as nine peaks may occur , but in no case was the number less than seven . dingemanse , huis in ' t veld and de laat ( 1946 ) adopted a system of numbering in which successive peaks on the curve were indicated by roman numerals i - vi , the lowest numeral corresponding to the peak with the lowest eluate serial numbers . this system was used in the present work to facilitate comparison with the results of these authors . in some urines , however , small quantities of a component occurred which appeared to be different from any of the 8 main fractions , and this component was allocated to a sub - group hia . 
the substance originarlly referred to as " 17 - ketosteroid hi " ( dingemanse , huis in ' t veld and de laat , 1946 ; dingemanse , huis in ' t veld and hartogh - katz , 1948a ) was later shown to be i - androsten - 6 - ol - 17 - one ( dingemanse , huis in ' t veld and hartoghkatz , 1948b ; barton and klyne , 1948 )  . the dutch workers isolated this substance from the urine of a two - year - old girl with an adrenal tumour , but found only small quantities in the urine of normal persons . in the presence of hydrochloric acid this substance gives rise to chlorodehydroisoandrrone and dehydroisoandrosterone , and such a conversion may occur durijg the preliminary hydrolysis of the urine . in the present investigation confirmation of these identities for peaks mn , rv and v was obtained ( a ) by the isolation of the constituents of peaks rv and v and the preparation of crystalline acetates and benzoates therefrom , ( b ) by the urinary 17 - ketosteroids application of a colour reaction ( patterson , 1947 ) to the constituents of peak ni , ( c ) by identification of the peaks formed by authentic specimens of dehydroi&oandrosterone , androsterone and aetiocholan - 3 - ( x ) - ol - 17 - one . in order to study the reproducibility of the method and the type of curves to be expected , known amounts of dehydroisoandrosterone , androsterone and aetiocholan - 3 - ( x ) - ol - 17 - one were chromstographed alone and in mixtures containing varying proportions of these three steroids . 
the curves obtained in these experiments revealed immediately a problem that has to be faced in determining the amount of ketosteroid represented by any one peak . this is the complication introduced by the fact that the minimum values in the depressions between peaks are not always zero . 
the question therefore arises as to how the amount of ketosteroid corresponding to such minimum values should be partitioned between two peaks on either side of the minimuthree treatments were considered : ( i ) half of the minimum value might be allotted to each of the adjacent peaks ; ( ii ) the whole of the mimmum value might be added to the preceding peak ; ( iii ) the descending curve of the preceding peak might be projected down to the abscissa axis , and the additional values thus formed added to the preceding peak while corresponding deductions are made from the succeeding peak . these three methods were tested by their application to the model chromatograms obtained with the known mixtures of the three steroids menin general it was found that the projection method ( iii ) gave a tioned above . closer approximation to the actual amounts of the individual steroids than did either method ( i ) or method ( ii )  . this method was therefore adopted as standard for computing the amounts of 17 - ketosteroids represented by different peaks . a striking example of the reproducibility of the method has recently been encountered . 
1. the curve of case 0 was obtained on an extract from a 10 - day collection of urine from a boy aged three . in cases 1 and 2 it was necessary to collect urine for 2 to 3 days in order to obtain sufficient ketosteroid for analysis . 
the percentage distribution of the total ketosteroids among the different peaks is given in table i for all the normal males investigated with the exception of case 0 , in which the peaks normally present in adult curves could not be differentiated . urines from 2 cases of benign hyperplasia of the prostate and from 6 cases of carcinoma of this gland were also examined , and the corresponding curves and percentage compositions of these extracts are shown in fig . 
1. - 17 - ketosteroid content of eluates from chromatograms of urines from normal males case 0 ( not included in table i )  . three - year - old boy . incomplete differentiation into cases 1 , 8 , 17 represent the predominant type in which androsterone exceeds aetiocases 2 and 5 are unusual types in which aetiocholanolone exceeds androsterone . case 13 is a man , aged 50 ; 17 - ketosteroid output 20 mg . 
per day ; dehydroi / androcholanolone . sterone 34 per cent of total ketosteroid . .420 urinary 17 - ktogsrerrds case 20 case 19 ly~~~~~~~~~~~l case21 case22 case 23 case 24 case 25 case 26 eluate number fio . 
peak ii , average value 11 - 7 per cent , ranges from 2 to 34 per cent of the total , peak iv averages 30 per cent , with a range from 8 - 4 to 49 per cent , and peak v has a mean it will be seen that the of 24 - 2 per cent , with a range from 11 to 38 per cent . average output of androsterone exceeds that of actiocholanolone in the ratio only in three of the 18 cases shown in table i does the output of 1 - 25 : 1 - 0 . aetiocholanolone notably exceed that of androsterone ( cases 2 , 3 and 5 ) ; in the other 15 cases the amount of the former ketosteroid is either approximately equal to or less than the amount of androsterone . luriary 17 - ketosteroimds a comparison of the data shown in table ii with those of table i shows , however , what appears to be a significant change in pattern . in the urines from the cases of prostatic disease there is a consistent preponderance of peak v over peak iv . this is illustrated in fig . 
3. - relative excretions of dehydroisoandrosterone , androsterone and aetiocholanolone in normal males and in males with prostatic disease . cases 13 - 18 , normal . cases 19 - 20 , prostatic hyperplasia . cases 21 - 26 , prostatic carcinoma . amounts of dehydroisoandrosterone and aetiocholanolone are shown relative to the same amount ( 100ug . ) of androsterone in all cases . three major peaks are shown for extracts prepared from urines of six normal males over 50 years of age ( cases 13 - 18 ) , and from the urines of two subjects with prostatic hyperplasia ( cases 19 and 20 ) , and six patients with carcinoma of the prostate ( cases 21 - 26 )  . utrines from the carcinoma cases were obtained before oestrogen therapy was begun , and those from the benign hyperplasias before operation . 
for convenience of comparison , the amounts of peaks in and v are shown relative to the same amount ( 100lg . ) of peak rv ( androsterone ) in it will be seen that the most striking feature is the relative increase in all cases . peak v in the cases suffering from prostatic disease . in the normal males over 50 years of age the amount of this peak is equal to or less than the amount of androsterone , but in the 8 cases of prostatic disease it is present in considerable excess . as mentioned earlier , the preliminary experiments with known mixtures of 17 - ketosteroids showed that peak v normally indicates the presence of aetiocholanolone , and the total amount represented by this peak is a measure of the quantity of this steroid in the original mixture . it may be provisionally assumed , therefore , that the increased size of this peak in prostatic disease indicates a a . 
goulden relative increase in the output of aetiocholan - 3 - ( x ) - ol - 17 - one , although the possibility is not excluded that the incrased peak size is caused by the inclusion of a second substance ( of at present unknown nature ) which is eluted with the aetiocholanolone . 
a decision on this question can be made only when sufficient of the material present in this peak has been accumulated to allow of its identification , and experiments are in progress with this object in view . if it is assumed that aetiocholanolone is the substance that is increased in relative amount in prostatic disease , the cause of this increase is at the moment obscure . this ketosteroid has been recognized as a transformation product of more than one other steroid . callow ( 1939 ) isolated aetiocholanolone and androsterone in approximately equ%l amounts from the urine of normal men , and also much larger , but still approximately equal , amounts from the urine of a man treated with testosterone . these two isomers appear to be end - products of testosterone metabolism , and to be formed in about equal amounts from this hormone . 
an explanation of increased testosterone metabolism does.not appear to fit the present observations , however , since they show an increase in aetiocholanolone relative to androsterone . in this connection it may be remarked that callow 's finding of approximately equal amounts of these two ketosteroids in normal male urine was based on experiments with a pooled sample of urine , and an examination of table i shows that in individual urines the ratio between the amounts of androsterone and aetiocholanolone is not constant , although the average values are approximately equal . aetiocholan - 3 - ( c ) - ol - 17 - one has also been shown to be a metabolite of dehydrosoandrosterone . 
mason and kepler ( 1945 , 1947 ) found that administration of dehydroandsterone acetate by intramuscular injection in oil to patients with very low outputs of 17 - ketosteroids ( a man with anterior pituitary deficiency and a man and a woman with addison 's disease ) led to greatly increased excretion of both aetiocholanolone and androsterone . in the two male subjects the amount of androsterone excreted exceeded that of aetiocholanolone by approximately 75 per cent , while in the female patient the aetiocholanolone was about 4 - 5 times as much as the androsterone . the observed increase in the ratio of aetiocholanolone to androsterone in the cases of prostatic disease might be produced by an increase in the absolute amount of aetiocholanolone , or by a decrease in the absolute amount of androsterone excreted , or by both simultaneously . the amounts of 3 - ( , ) - hydroxyketosteroids , androsterone and aetiocholanolone excreted in 24 - hours were calculated for the cases illustrated in fig . 
3. normal males in the later decades have been examined . such a comparison will be possible when further in a study of z - ketosteroid excretion in patients with neoplastic disease dobriner , rhoads , lieberman , hill and fieser ( 1944 ) found abnormal patterns in in the one case of prostatic cancer reported in several cancerous conditions . their paper there was a great excess of aetiocholanolone as compared with androthey found a similar relation in a case of carcinoma of the larynx and sterone . a case of carcinoma of the breast . 
kennedy. from the endocrinology research department of the new zealand medical research council , medical school , dunedin , new zealand . received for publication july 30 , 1951 . previous communications from this laboratory ( griesbach , kennedy and purves , 1945 ; purves and griesbach , 1946 , 1947 ) described the induction of thyroid adenomata in rats by the long - term administration of goitrogens . bielschowsky , griesbach , hall , kennedy and purves ( 1949 ) showed that these thyroid tumours as well as those appearing under the combined influence of goitrogen and carcinogen could be transplante ' d into rats of the same strain . transplantation was only successful when the recipient animal was kept in a state of thyroxine deficiency produced either by treatment with goitrogen or thyroidectomy . 
from this failure of the transplanted tissue to grow in normal animals it was concluded that an excess of thyrotrophin was needed for the continued progressive growth of such tissue in a similar way as it had been necessary for the induction of the original tumour in the rat 's thyroid . therefore , these tumours were not considered to be " autonomous , " although they showed such signs of mahgnancy as a typical and progressive growth , invasion of surrounding tissues and formation of metastases . 
being injected subcutaneously in the flank of each the majority of rats were continuously supplied with a - 01 per cent rat . special mention is made in the solution of methylthiouracil as drinking water . text when no goitrogen was given . 
the thyroid was very large with a nodule protruding from the isthmus . part of this nodule was removed and two pieces were inoculated into two young rats which had been given 0 - 01 per cent methylthiouracil beginning 5 days previously . 
the acini varied in size , many of them being larger than the acini of the normal rat thyroid . in one line of transplantation this structure has been maintained up to the present day , and ' fig . 
6 shows the histology of a graft from the fourth generation of this fine . it will be noted that surrounding the larger acini there are numbers of small acini which suggest that new acini are being formed by budding from the larger ones . small cellular areas exist without well - defined acini , but these are considered to be areas of prohferation in which differentiation has not yet taken place . 
the acini are well filled with colloid , this colloid accumulation being always present even under conditions of strong thyrotrophic stimulation . this presence of colloid does not , however , indicate that the tumou ' rs are not influenced by thyrotrophic hormone , since when the thyrotrophic hormone production in the host is inhibited , these tumours undergo rapid regression . iodine , metaboli8ln of t , tumour . the iodine metabolism of the transplanted t , tumour was tested in rats bearing second generation grafts . table i shows the results of in vivo tests of the uptake of radioactive iodine in three rats after radioactive iodine had been injected . 
l. - chart of the first 6 generations ' grafting of the tbyroid tumour t , the treatment of the recipient animals is indicated on the cbart . solid black indicates animal bearing tumour . 
kennedy the evidence of secretory function in the t , tumour has been obtained from the results of transplants growing in totally thyroidectomized animals . these animals the ti tumour transplants do not grow continually , but appear to reach a maximum weight of about i g . 
of rats witb tumour growth . growth was obtained in the normal animals . this indicates the dependence on high thyrotrophic hormone levels , a dependence which is also displayed when animals bearing growing tumours during the administration of methylthiouracil have their medication stopped . 
the large irregularly - shaped acini which were prominent in the ti colloid was present in some of the acini but was less tumour were not seen . prominent than in the t , tumour . 
the nuclei were hyperchromatic and irregular in sha e . ( 2 ) embedded in this adenomatous tissue was a nodule of tiss ' ue distinctly different in staining properties . in this tissue , which had a well - developed acinar structure corresponding to a very hype ' rplastic normal rat thyroid , the cells were large with abundant cytoplasthe nuclei were round and did not contain excess chromatthe lesser numbers of nuclei and their weaker staining properties ' ' were responsible for the pafer appearance of these nodules in the 306 h . 
the fact that such tissue always forms microscopic nodules and has not ever formed a large part of the grafts in any of the inoculated animals suggests that this type of tissue is a slow - growing variant which arises spontaneously within the adenomatous tissue . 
the nodules of this type seen in the fourth generation appear to have arisen from the modified adenomatous tissue of these animals mentioned above which differs from that of the original tumour . ( 3 ) the third type of tissue is an anaplastic carcinomatous tissue without any in animal 253 , no . 
in weight being observed after 10 days . in the fourth week after transplantation animals with the rapidly growing tumours began to succumb . in a proportion of the animals , however , the growth was slower and the animals survived 3 or 4 months . 
the histology of ah these tumours was that of the anaplastic carcinoma described above as the third type of tissue seen in the fourth was successfury maintained by serial generation . transplantation , and - in later transplantations successful grafts were obtained in up to 80 per cent of those inoculated . 
the t22 tumour has now been transplanted through 7 consecutive generations and has not undergone any progressive change in either malignancy or histology . histology of tumour t22on the cut surface two regions cciuld be regularly seen , the outer with a shiny grey appearance , 5 to 8 mbroad , and the central one coloured a pale orange frequently a brown albuminuous fluid had replaced with a crumbled surface . mioroscopic examination revealed that , ' generally , the inner the central tissue . zone ofthe tumours consisted ofdegenerating cers or amorphous masses , infiltrated by round ceus , and isolated cers with strongly eosinophihe cytoplasm and pycnotic nucleus , lying , between the cell debris . the outer zone , microscopically , appeared simflar to that of the anaplastic nodule of the original tumour , and this description apphes to both tissues . 
unusuary large tumour cefls were present which had slightly basophilic cytoplasm and nuclei with ir - regulariy dispersed chromatin . giant cells were present with nuclei varying in number from 2 to ' 8 . 
the numbers of giant cers found varied somewhat in different animals and were relatively few they have , however , been a constant feature of in the first animal examined . the tumour ' and we consider that the tumour should , therefore , be classed as a giant cell carci ' noma of the thyroid . mitotic ftgures are frequent and many of them atypical . effe , ct of t22 tumour on the host . the striking feature of the t22 tumour is that it kirs its host in as short a period as 3 weeks . there is , however , a considerable variation in the rate of growth in different animals , some of them surviving for 2 months or more . those animals which died within 3 to 4 weeks after inoculation , the animals showed at autopsy an extreme state of emaciation with atrophic muscles and thin soft bones . 
was lower than ' its weight at the time of transplantation . it appears , therefore , that the rapid growth of these tumours withdraws nutrients from the host and leads to the state of emaciation described . effect of thyrotrophic hormone level on tumour t22 ' the t22 tumour has been found to grow equally wer when inoculated into normal animals or animals receiving methylthiouracil . moreover , in normal animals in which this tumour is growing , no inhibition of the growth rate has been observed when the an ' imals were treated with thyroxine injections . in some selected animals bearing this tumour in which the growth was relatively slow this treatment did not produce any marked some were treated with thiouracil . acceleration in the growth of these tumours . 
the t22tumour , therefore , does not show the dependence upon thyrotrophic stimulation which was shown by its parent tu ' mour . iodine , metabolimof the t22 tumour . rats bearing the t22 tumour were injected with radio - active iodine and 24 hours later were killed , and the radio - active iodine concentrations in the tumour tissue and in the blood plasma were measured . 
kennedy considered that both the action of the carcinogen plus the hyperplasia resulting from the goitrogen were necessary for the induction ofthyroid tumours . however , griesbach , kennedy and purves ( 1945 ) reported that the prolonged action of goitrogens alone led to the formation of tumours , which in a later publication ( bielschowsky , griesbach , hall , kennedy and purves , 1949 ) were shown to be similar in all respectsto those appearing after the carcinogen treatment . 
with goitrogen alone , however , tumours are later in appearing and are fewer in number . these tumours aredependent upon high thyrotrophic hormone level for their in normal animals such tumours , either in the thyroid or as grafted growth . - tumours , undergo rapid regression and eventually disappear , so that they cannot be induced to reappear by the subsequent administration of goitrogen . 
the simplest explanation , therefore , of the role of the goitrogen in the production of these tumours is that it induces the high thyrotrophic hormone production without in this view , the goitrogen would not have which such tumours cannot grow . any influence on the formation of neoplastic cells . it is , therefore , considered that neoplastic cells arl 'se spontaneously in the normal rat thyroid , and that when conditions are suitable for the growth of such cells , visible neoplasms result . 
in weight are commonly produced.. the continuous growth of such tumours 4nd the propagation of them by transplantation leads naturary to the selection of fast - growing types of tissue so that an increase in mahgnancy with transplantation is to be expected . however , modifications of the adenoma are not invariably in the direction of increased mahgnancy . 
we consider that the type of nodule described as the second type of tissue observed in the fourth generation transplants is a relatively slow - growing benig - n structure which reappears in successive generations , and which by virtue of its slow growth and lack ofmetastasizing power cannot be selectively propagated by transplantation . 
on the other hand , the truly malignant , invasive and metastasizing carcinoma will , when it once appears , invariably supplant entirely the benign structure in two , or three at the most , generations of grafting . evolution of malignancy in benign tumour8 . while it has been recognized that transplantable mammalian tumours show increases in mahgnancy on transplantation , it has been often assumed that such increase in mahgnancy results from a gradual adaptation to the host or a gradual modification of the original tumour . 
the thyroid adenomata appearing in - the rat thyroid are all dependent on thyrotrophic hormone for their ' existence , and in fact require higher levels of thyrotrophic hormone for their continued growth than does the normal thyroid tissue . investigation of human thyroid neoplasms with the aid of radio - active iodine have shown that many of these are in fact susceptible to the stimulating influence of thyrotrophic hormone , although neoplasms in human material have not been described which are so entirely dependent upon thyrotrophic hormones as are these primary rat thyroid tumours . 
the existence of undoubted stimulating effects of thyrotrophic hormone in human thyroid tumours supports the view that these rat thyroid tumours are not exceptional , although their high degree of dependence on thyrotrophic hormone sets them somewhat apart from the thyroid tumours encountered clinically . there seems no reason to hold the view , as some people have done , that these rat tumours should not be classed as neoplasms , since in their case the stimulating hormone or factor on which their 310 h . 
kennedy growth depends ' is well characterized and can be artificially manipulated so as to presumably as further knowledge is gained the control the tumour growth . stimulating influences which condition the growth of other tumours win be discovered , but this should in no way affect their classification as neoplasms . it is important to note here that from a tumour at first dependent upon a hormonal imbalance for its growth , there has been derived a mahgnant neoplasm which is no longer dependent upon the stimulating influences which condition the growth of the more benign original tumour . 
thus where mahgnant tumours are found which are not susceptible to any known hormonal influence , the effect of hormonal imbalance in the production of such tumours is not excluded . 
1. received for publication january 21 , 1949 . kennaway , kennaway and warren ( 1944 ) found that injection of certain carcinogenic substances , including 1 : 2 : 5 : 6 - dibenzanthracene , caused an increase in the concentration of ascorbic acid in the liver of mice , whilst some noncareinogenic , chemically related substances ( naphthalene , anthracene , phenanthrene ) did not show this effect . in an investigation of the growth - inhibitory action of the carcinogenic hydrocarbon 1 : 2 : 5 : 6 - dibenzanthracene ( elson and warren , 1947 ) it was found that the inhibition of rat body growth and of the growth of walker rat carcinoma 256 ( elson and haddow , 1947 ) by this substance is dependent on the protein content of the diet of the animals . 
1 : 2 : 5 : 6 - dibenzanthracene in the rat usually results in little growth inhibition for about the first 14 days , after which the animals at varying intervals lose weight and die . 
on a 10 per cent protein diet after the same dose of the carcinogen , immediate inhibition of growth occurs and persists for a prolonged period , usually until the death of the animal . in considering the cause of the rise in liver ascorbic acid brought about by 1 : 2 : 5 : 6 - dibenzanthracene , it appeared possible that this was a result of the growthinhibitory action of the compound . 
there was some evidence ( elson , unpublished communication ) that the growth inhibition was accompanied by a fall in the succinic dehydrogenase component of the succinoxidase enzyme system of since the cytochrome oxidase component of this enzyme system is the liver . capable of rapid oxidation of ascorbic acid , it seemed possible that the rise in ascorbic acid after 1 : 2 : 5 : 6 - dibenzanthracene might be the result of less destruction by such oxidation occurring owing to the decreased content of the oxidizing enzyme . 
they were weighed every 2 or 3 days . high and low protein tabls . in later experiments it was found necessary to estimate the amount of food consumed by each rat , and in order to facilitate this 25 per cent and 5 per cent protein diets were made up in 5 g . 
tablets in the shape of cylinders of approximately 3 cdiameter and 0 - 5 chigh . this necessitated replacement of some of the starch in the original diets by cane sugar and glucose in order to obtain a firm tablet . 
from the control experiments , in which only arachis oil was injected , .it is seen that the variation of the protein content of the diet itself has practically no influence on the level of ascorbic acid in the liver . 
the animals fed the 5 per cent protein diet grow only very slowly , but the effect of dibenzanthracene on them is not to make them lose weight , as would be expected if the magnitude of the growth inhibition was proportionate to that observed in animals this smaller effect is presumably maintained on the 10 per cent protein diet . related to the lower total metabolism of the 5 per cent protein diet animals , and 152 l . 
5 , although complete inhibition of growth occurred , and at one time actual loss of weight , the food intake , after the initial drop , rose steadily to a value higher than the level before administration of dibenzanthracene at the time the animals were killed for determination of liver ascorbic acid the actual degree of growth inhibition was greater than the maximum previously obtained with the 10 per cent protein diet animals . 
the degree of growth inhibition is dependent on an equilibrium being established between the rate at which the animal is metabo - _wa% growth rate fooie ratn ? j final liver wt ascorbic acid o * + |~~ 1i 135 6 - 14 ( 1 * 1 [ oo llll , , illlllllllllll , lll ( 134 1i111 . , g14 3 ) o3 ) _ t .%1 5 days 20 25 7 - 02 ' 10 - ~ _ ~3124 8 - 17 7 - 63 fig . 
in animals fed 20 per cent protein diet liver ascorbic acid increases before any marked growth - inhibition is observed , and the increase is thus not an indirect consequence of the inhibition of growth . the growth - inhibition is not merely the result of a lowered intake of food . the animals may react to treatment with dibenzanthracene by maintaining or even increasing their daily food consumption , although growth is completely inhibited . this suggests that a profound change in basal metabolism must have taken place , and the rise in liver ascorbic acid may be associated with this change . we wish to express our thanks for generous grants supporting this investigation , from the british empire cancer campaign , the anna fuller fund , the jane coffin childs memorial fund for medical research , and the u.s. 
this proportion insured chrom - atograms of satisfactory color intensity . ethanol was used for the extraction because it is believed to be a solvent which causes minimum proteolysis during denaturation of protea 78 per cent , solution has been found to be optimal for solubility of the amino - acids and for the extraction of non - protein nitrogen only . a two - dimensional chromatogram on whatman no . 
new amino - acids appeared at varying intervals in each of the four tissues 'studied , and - the changes were consistent fot each tissue in ar of the rabbits studied . 
they found that muscle temperature and ph decreased with isch - aemia . proteolysis found during ischaemia may be.caused by accelerated enzyjnic degradation in a more acid medium as the optimum h of tissue cathepsins hes between 4 and 5 ( willstiitter and bamann , 1929 )  . , in any event ischaemia m , 4y alter the chemical characteristics of a tissue . 8ummaim ' the number of free amino - acids extractable from clinical cancers of similar histogenesis - varied widely , due apparently to deliberate occlusion of the arterial supply in the , course . 
mitchell. from the department of radiotherapeuties , university of cambridge . received for publication july 8 , 1953 . attempts to evaluate tetra - sodium 2 - methyl - i : 4 - naphthohydroquinone diphosphate ( compound i , synkavit ) as a radiosensitiser in the radiotherapy of malignant tumours have been in progress since november , 1946 . 
at first the compound was used alone and in conjunction with palliative x - ray therapy in some very it soon became evident that in general the compound alone had advanced cases . no therapeutic effect in malignant tumours . 
at the same time , all cases of inoperable carcinoma of the bronchus were treated , if possible , by the combination of x - ray therapy and compound i ; the results were assessed mainly by survival times from the first x - ray treatment and the first sympton and were compared with those which had been obtained previously in the same department with x - ray therapy only , and which were very similar to the depressing results obtained by most of the workers . slowly the difficulties of this type of clinical investigation were appreciated . moreover in 1950 erratic results were encountered both in the clinical trials and in animal experiments . it seems likely that these findings were attributable to the thermal instability of compound i in aqueous solution in the absence of oxygen ( mitchell and simonreuss , 1952 )  . 
much more consistent results have been obtained since the ampoules have been stored in a refrigerator at about 30 c . the evidence obtained by these preliminary studies was sufficiently suggestive to justify further work , but the methods used were clearly inadequate . it became essential to employ properly designed methods for the clinical evaluation of radiosensitisers . 
the importance of these methods was emphasised at the time by their use in clinical evaluation of chemotherapeutic agents in tuberculosis ( medical research council , 1948 , 1950 )  . investigations of this type in the study of radiosensitisers have been in progress since april 1951 ; as yet the only results available are for the treatment of inoperable carcinoma of the bronchus . the results of the earlier studies have been reported by mitchell ( 1948 , 1949a , 1949b , 1950 , 1951 )  . this work has been criticised by gellhorn and gagliano ( 1950 )  . otte ( 1949 ) reported briefly on the combination of x - ray therapy and some synthetic vitamin k substitutes in the treatment of 300 patients with advanced malignant tumours and claimed improved palliation . 
mitchell selection of types of malignant tumour for investigation . it is suggested that a practical minimum requirement for usefulness of a radiosensitising chemical agent is that its employment in combination with radiotherapy should produce a mean survival time after treatment double that after radiotherapy only , for the type of malignant tumour treated . 
hence taking into account the frequency distribution of the survival times , it is likely to be necessary to observe the cases treated by combined therapy for an interval of at least 6 times the mean survival after radiotherapy only . 
to this time must be added the time necessary to accumulate an adequate number of cases . this approach is limited to the study of types of malignant tumour in which the results of present methods of treatment are bad and in which the time of survival is short . inoperable carcinoma of the bronchus is an obvious choice for investigation it is the only common type of malignant disease with a very short natural history . despite advances , only a small proportion of all cases of carcinoma of the bronuntreated patients are often very miserable . 
the chus are curable by surgery . results of treatment of inoperable cases by present methods , including radical nevertheless x - ray therapy in general has sufficient x - ray therapy , are poor . palliative value apart from prolongation of life per se , to justify attempts to improve this . with x - ray therapy only , inoperable carcinoma ofthe bronchus appears to have a a rather uniform natural history . 
of these , histological evidence was obtained in 245 patients and their average survival from the first symptom was 14 - 3 months and from the beginning of x - ray treatment 4 - 5 months . 
7 of this paper , it can be deduced that of 729 patients , only 45 survived 8 months , 20 survived 12 months , 8 survived 18 months and none survived 3 years following in this series , the best survival rate - 4 - 7 months - was in a x - ray therapy . group of 80 patients who received a total dose as measured in air of 5000 - 6000 r ; higher and lower doses were associated with poorer results . 
the most important factor in determining survival is the extent of spread of the disease when treated . this evidence suggests that in representative series of cases of inoperable carcinoma of the bronchus receiving x - ray therapy , the mean survival from the beginning of treatment is about 4 - 5 months . 
to try to minimise its shortcomings , all the cases to which it is applied have been followed until death , or for at least 3 - 1 years and in assessing the results the proportion of cases showing unexpectedly good response has been compared in the case of patients treated by means of radiotherapy combined with intravenous compound with those treated by radiotherapy combined with intramuscular compound . the results of various types of treatment of patients with advanced malignant tumours classified as inoperable , stages iii and iv , and recurrent of all types except carcinoma of the bronchus using compound i in treatments from november , 1946 to july , 1909 inclusive , and assessed up to 31 december , 1952 , are summarised in table i for the cases verified histoan essentialy similar table has been prepared showing the rather logically . poorer results for 56 cases not confirmed histologically , but with reasonably the cases allocated to this preliminary survey were the great certain diagnosis . majority of the patients with advanced malignant tumours in which it was considered that present methods of treatment were not likely to give satisfactorily results . 
when the survey was started it was not realised that the use of the compound by intravenous injection was likely to be more effective than its use by intramuscular injection . the allocation of the patients to treatments involving the two mnethods of administration of the compound were certainly not a.t random , and the possibility of bias by the use of intramuscular injection in the more seriously ill patients cannot be excluded . however , there is no reason to suppose that such bias would influence the proportion of cases showing unexpectedly good clinical response . the resultsof the preliminary general survey summarised in table i suggests that the proportion of cases showing unexpectedly good clinical response is greater 316 j . 
one case of advanced carcinoma of the body of the uterus was treated by means of palliative x - ray therapy combined with intravenous compound , and one case of carcinoma of the tongue recurrent after previous x - ray therapy was treated successfully by radical x - ray therapy combined with intramuscular compound . of the 56 cases not confirmed histologically three survived more than 4 years after treatment . 
two of these showed an unexpectedly good response ; one was a woman aged 46 , who had a stage iv carcinoma of the breast with supraclavicular glands , and was treated by means of radical x - ray therapy combined with intramuscular compound , and the other was a case of a mixed parotid tumour which had failed to respond to further x - ray therapy , but appeared to be checked and rendered quiescent by intravenous compound onlv . 
the results are treated by statistical methods . it is suggested that estimation of the survival times , especially that from the beginning of x - ray therapy , is the most reliable criterion for objective assessment of the results of treatment . special attention has been paid to the influence of the extent of the disease , age and sex , the histology , the minimum tumour dose and overall time of the x - ray therapy and the details of administration of the compound . the general principles involved in the consideration of these factors are essentially the same in these preliminary studies as in the later clinical trials and except where relevant , will be discussed in this connection . 
the results of treatment were reviewed as from this group of cases of inoperable carcinoma of the bronchus december 31 , 1952 . comprises all those cases referred in which the diagnosis is accepted as proven according to the criteria given below , with the exclusion of patients not likely to benefit by palliative x - ray therapy . 
no technically operable cases and no postoperative cases are included . the control group consists of those cases of inoperable carcinoma of the bronchus selected according to the same criteria , which were treated by x - ray therapy only , using similar methods , in the same department between 1943 and may , 1947 . the difficulties of this method of providing a control group are recognised and include the possibility of introduction of serious errors of sampling . 
the use of alternate cases as controls was attempted but was abandoned as impractical . however , it has been shown that the relevant properties of the control and treated groups apart from the length of survival after treatment are substantially the same . it is found that the results of x - ray treatment in the present control group are substantially identical with those obtained in two large published series . 
mitchell ( b ) cases with positive histology on biopsy specimens of supraclavicular nodes , cutaneous or other metastases but in which there was no bronchoscopy or the bronchoscopic appearances were not definite ; this sub - group consists of 8 control cases and 8 treated cases ; ( c ) one case ( treated ) with typical bronchoscopic appearances together with metastases in the skin , confirmed histologically . these additional 15 control and 18 treated cases are usually more advanced and are in general less comparable than the " histologically verified " cases but must be considered with them to give a complete picture . 
of the combined series of " confirmed cases , " there are in all 34 in the control group , which was treated by x - ray therapy only , and 47 in the treated group , which received x - ray therapy together with the compound . 
as anticipated the results of treatment of the " confirmed cases " are poorer than those of the " histologically verified " cases . other groups of cases which cannot be included in the main part of this investigation may be summarised as follows : ( i ) cases with typical radiological appearances together with metastases at some stage but not verified histologically and in which there was no bronchoscopy or the bronchoscopic appearances were not definite . in these cases the diagnosis can only be regarded as probable . in the control group , there are 12 cases ; the mean time of survival is 8 - 50 months from the first symptom and 3 - 67 months from the first x - ray treatment . in the treated group , there are 13 cases ; the mean times of survival are 12 - 15 months from the first symptom and 6 * 31 months from the first x - ray treatment . ( ii ) cases rejected as unsuitable for palliative x - ray therapy . during the control period , there were 18 of these cases , of which 10 were histologically verified and during the period corresponding to the treated group , there were 7 cases of which only one was verified histologically . the enumeration of rejected cases is unsatisfactory because of selection by the physicians referring these advanced cases . hence the total number of cases with a reasonably certain or probable diagnosis of inoperable carcinoma of the bronchus is 131 . 
of the 7 cases of squamous carcinoma , two showed keratinisation . of the 29 verified treated cases , there are 17 cases of stratified carcinoma , of which 10 are squamous and 7 non - squamous , 3 cases of adenocarcinoma , 8 of anaplastic carcinoma and one an unusual poorly differentiated lesion . of the 10 cases of squamous carcinoma three cases show definite keratinisait is interesting tion ; in two further cases there is a suggestion of keratinisation . to note that all these cases responded well to treatment . the control group was treated by x - ray therapy only , from 1943 to may , 1947 . 
even if the cases which survived only one month from the first x - ray treatment are excluded , to meet the criticism of a possible difference in selection of the cases , the difference in survival after the first treatment between the treated group ( mean survival 9 - 68 months ) and the control group ( mean survival 5 - 23 months ) is still significant ( n = 39 , t 2 * 457 , p is slightly less than 0 - 02 )  . considering the histological classification , the only type providing adequate numbers is the stratified carcinoma . 
the basic principles involved are well understood as a result of the classical statistical studies of fisher ( 1925 , 1935 ) on the design of experiments , and on the work of hill ( 1952 ) on the design of clinical trials . 
in general , in considering therapeutic trials in the cancer field , the design must be capable of giving a completely convincing statistically significant quantitative result as efficiently as possible with a minimum number of patients and must be acceptable and above reproach from the moral and ethical points of view . 
the most important single feature of the design is random allocation of the patients to two or more alternative forms of treatment the value of which is being compared . for assessment of the result of treatment , it is necessary to select relevant criteria capable of objective measurement such as the survival time suitably specified . 
at the same time , it is absolutely essential to provide for each individual patient treatment which is the best possible according to present knowledge . accordingly , it may be , and probably often will be , necessary to plan to depart from what may be termed the theoretically ideal form of experiment with deliberate sacrifice of some information . in the present example of the attempted evaluation of tetra - sodium 2 - methyl1 : 4 - naphthohydroquinone diphosphate ( compound i , synkavit ) as a radiosensitiser in the radio therapy of inoperable carcinoma of the bronchus , cases were allocated at random to one of two alternative forms of treatment , x - ray therapy combined with compound i administered by intravenous injection ( x + i - vs ) and x - ray therapy combined with compound i administered by intramusculrzr injection ( x + i - ms )  . 
the latter is regarded as the control group . the preliminary clinical studies and animal experiments suggested that the results of x - ray therapy combined with intramuscular compound ( x + i - ms ) were slightly better than those of x - ray therapy only , and that with comparable doses of compound it was likely that x + i - vs would produce better results than x + i - ms . 
mitchell tests of heterogeneity must be made . clinical therapeutic trial must be justified a posteriori . it is necessary to - examine the possible importance of all the various factors which may be relevant including age , sex , extent of the disease at treatment , histology and / or cytology , the minimum tumour dose and overall time of radiotherapy , the total dose and overall time of administration of the compound and in particular the certainty of the diagnosis . it does not seem possible to estimate in advance the number of patients required . this will depend on the differences observed between the groups and subgroups . 
the results are likely to be of sufficient importance to necessitate the use of stringent criteria of significance . the randomisation was made on the basis of a provisional diagnosis of inoperable carcinoma of the bronchus , made when the patient was first examined by the staff of the department . 
some of the cases were referred with histological evidence from bronchial biopsy . in other cases , there had been no previous investigation and the provisional diagnosis was based on clinical evidence only . all cases were investigated critically , as necessary , and every effort was made to obtain histological and / or cytological verification of the diagnosis . almost all the sections have been reviewed by a . 
cruickshank , of the sims woodhead memorial laboratory , papworth , for most of the reports on specimens of bronchial aspirate . particular attention has been paid to the establishment of the diagnosis of carcinoma of the bronchus and the identification and exclusion of cases of bronchial adenoma and related tumours of low grade malignancy apparently arising in bronchial glands . 
barrett and may be summarised as follows : ( 1 ) stratified carcinoma , either squamous or non - squamous , the degree of keratinisation or differentiation being noted , ( 2 ) adenocarcinoma , ( 3 ) anaplastic carcinoma , including " oat - celled " carcinoma , and ( 4 ) others , including " alveolar " cell carcinoma and carcinoma not classifiable . 
the histological classification of carcinoma of the bronchus is often difficult because of the existence of intermediate types and is somewhat arbitrary in some cases . on the clinical side , a careful and full medical examination is made , including usually indirect laryngoscopy . it has been considered important to determine the extent of spread of the disease with special reference to the early detection of metastases in bones . the occasional cases originally considered inoperable and in which it has been found possible subsequently to carry out some type of surgery have been considered separately in the assessment of the results . 
and increased daily in steps of any undesirable reaction such as excessive coughing , nausea , faintness the chest is observed after intravenous injection , the dose which there is no such reaction and then cautiously increased again on the following days , sometimes by steps of for most patients , for intravenous injections the best maximum daily dose appears to be 100 mg . ; dose is increased to as high a level as is tolerated . dosage is started with or discomfort or pain for the purpose of + i - ms . administration i - v , is reduced many will mg . 
some cases are still surviving so that additional evidence concerning the diagnosis may be forthcoming in a few of these and the estimates of survival time are necessarily incomplete . it is reasonably certain that any such new evidence will increase the differences observed between the two series . the total numbers of cases are 46 in the x + i - vs series , of which one received compound only with no x - ray therapy and 45 in the x + i - ms series . the fate of every case is accounted for in the groups ( a ) to ( j ) of table ii . 
12 * 4 days ; for the 19 patients in the x + i - ms series , 4 received radical treatment and survived respectively 4 , 6 , 7 and 6 months , the mean m.t.d. 
mitchell by intravenous injection than with radiotherapy combined with the compound administered by intramuscular injection . preliminary clinical studies of the influence of the ancillary use of the compound on the survival times of inoperable cases of carcinoma of the bronchus treated by x - ray therapy are discussed in some detail and the end results summarised . the design of a clinical therapeutic trial of a radiosensitiser is discussed , with special reference to the evaluation of tetra - sodium 2 - methyl - i : 4 - naphthohydroquinone diphosphate m a radiosensitiser in the radiotherapy of inoperable cases of carcinoma of the bronchus . 
the results of this clinical trial are summarised to date . it is concluded that intravenous administration of this compound ( synkavit ) has a small but useful effect as a clinical radiosensitiser . in this work i have been helped by many colleagues at addenbrooke 's hospital . in particular i wish to thank a . 
campbelt. poultry research centre at the university of edinburgh . * received for publication december 30 , 1948 . the original purpose of this investigation was to study the effects of implanting various tumnours affecting the fowl into the fertile egg . a survey of the literature revealed the rather surprising fact that apart from the rous i sarcoma ( rous and murphy , 1911 ) , and a few leucosis cases ( pierce , 1942 ) , no attempt has been made to grow spontaneous neoplasms of the chicken in fertile eggs . there is a high incidence , relative to disease in general , of spontaneous neoplasia in the fowl . 
campbell ( 1945 ) , in a survey extending over five years , found the relative average incidence to be 18 ' 7 per cent in the breeds examined , the minimum and maximum figures for specific breeds being 10 - 3 per cent and nearly 39 per cent . during this survey a number of chicken tumours were studied which bore a close morphological resemblance to known virus - associated growths . in view ofclaims by various authors ( taylor , 1943 ; heilman and bittner , 1944 ; hungate , snider , taylor and thompson , 1945 ) that mammalian tumours can be easily cultivated in the yolk - sac of the chick embryo , and that a virus - like factor associated with mammary carcinoma of mice has been directly demonstrated by this method , it was thought desirable to apply similar methods to the study of spontaneous chicken tumours . the advantages of using fertile eggs for such cultivation experiments are many . 
the chick embryo , on the other hand , has not yet been reported to be a natural carrier of virus . it has been shown by grasset ( 1929 ) , who worked with diphtheria and tetanus toxoids as antigens , that the chick embryo does not produce antibody . polk , buddingh and goodpasture ( 1938 ) showed that no complement is present in embryonic serum , and murphy ( 1914 ) first demonstrated the ability of normal heteroplastic tissues and tumours to graft on to the chorioallantois without causing an inflammatory reaction until the 18th day of incubation . subsequently some reaction of the host tissues does occur , to the detriment of the graft . the culture of tumour tissues in fertile eggs therefore resembles much more closely tissue culture in vitro than it does in orthodox animal inoculation methods . at an early stage in this investigation the frequent occurrence of typical ectodermal lesions in the vicinity of chicken tumours implanted on the chorioallantois led to the conception that such tumours might contain a factor capable of stimulating cell division . such a factor , if it existed , might be a self - propagating agent within living malignant cells , or something in the nature of a mitotic activator similar to those growth - stimulating substances present in embryonic tissues . with this hypothesis in mind it was decided to study the effects of implanting embryonic tissues , certain viruses , and as wide a range of tumours as possible , derived from a variety of animals . about this time a series of cases of spontaneous liver carcinoma in ducks came under observation , and similar experiments were undertaken with the resultant material , the details of which are recorded in a separate paper . the first record of tumour cultivation in the fertile egg was by rous and murphy ( 1911 ) , who applied it to the newly discovered rous chicken sarcoma , which they succeeded in cultivating in various sites , including the yolk - sac , and on the chorioallantoic membrane . 
they make no mention of any reaction on the part of the chick embryo or its associated membranes , and their plates only illustrate the histology of the cultivated tumours ; the membranes themselves were apparently not examined . stevenson ( 1918 ) then tried various rat , mouse and guinea - pig tumours and had about 30 per cent takes . 
campbell keogh ( 1938 ) found that filtrates prepared from the rous i sarcoma gave rise to ectodermal proliferative lesions when inoculated on the chorioallantois . these focal lesions were fully developed about the 7th day after inoculation , and took the form of flattened pearly opacities varying in diameter from 0 - 5 mm . to 2 mdilute inocula produced these lesions ; when concentrated suspensions were inoculated a proportion of sarcomatous lesions developed . pierce ( 1942 ) transferred leucosis to chick embryos by seeding fragments of leucotic tissue , e.g. 
no lesions developed on the membrane , and inclusion bodhes were absent when filtrates were used , but leucotic tissue caused gross thickening and cloudiness of the membrane . taylor , thacker and penington ( 1942 ) described the growth of cancer tissue ( mammaryv carcinoma of mice ) in the yolk - sac of the chick embryo , and claimed it to be a new method . 
the presence of necrotic tissue in the tumours resulted in the death of the embryo . in a subsequent communication taylor ( 1943 ) described the cultivation of a spontaneous mammary tumour of dba strain mice in the yolk - sac of the fertile egg . 
the yolk from such eggs produced similar tumours in mice upon injection , and taylor found that berkefeld filtrates prepared from this yolk also gave rise to tumours upon injection into mice , thus showing the presence of a virus - like principle in this particular mammary carcinoma . at about the same time heilman and bittner ( 1944 ) injected a 40 per cent suspension of mouse carcinoma into the yolk - sac of the embryonic chick , using an inoculum of 0 - 2 ml . 
they extracted the tumours from the yolk - sac , and showed that fitrates prepared from these and from the yolk itself were capable of causing mammary cancer in mice , thus confirming the work of hungate , taylor and thompson ( 1944 ) , that a virus - like body was involved . following up this line of investigation bittner , evans and green ( 1945 ) showed that the " milk factor " was able to survive in the yolk - sac for 12 days in the absence of mouse mammary carcinoma cells . 
they did not know whether the factor had multiplied in the yolk - sac . twombly and meisel ( 1946 ) attempted to grow several mammalian tumours in the yolk - sacs of fertile eggs . 
the greatest number of takes occurred with the bagg 755 mouse mammary carcinoma , but they report a very high mortality rate ( 73 per cent ) by the 17th day of incubation in their embryos . 
numerous fitration experiments were done in an attempt to demonstrate a cancer virus , but with uniformly negative results . ( a ) the intra - vitelline techniqe . the method adopted for the cultivation of tumours in the yolk - sac was a modification of that described by taylor et al . 
they were then taken direct to 95 per cent alcohol , through absolute alcohol , equal parts absolute alcohol and cedarwood oil , cedarwood oil alone , and finally embedded in paraffin wax . other tissues were fixed in 10 per cent formol saline for 24 hours . 
the eggs were sealed with their own shell flap , using paraffin wax , and this was removed on the fifth day and a cover - glass substituted . tumours were seen growing in each , dependent from the chorioallantois . 
the eggs were opened 9 days later , and both contained large ( 9 mm . ) spherical , richly vascular tumours growing from the chorioallantois and hanging down into the allantoic cavity . 
of this filtrate was injected into each pectoral muscle of a brown leghorn cockerel aged 14 weeks . typical tumours subsequently grew in these sites . hi / to / og . the only histological findings to be given in any detail will be those associated with changes in the membranes in the vicinity of implanted tumours . 
a delicate argyrophil reticulum ramifies throughout the growth , and appears to be derived from the mesenchyme of the membrane . normally the epithelial surface of the chorioallantois consists of low cuboidal cells , and is only one cell thick . 
the tube was shaken in an automatic shaking machine for 1 hour , at the end of which the suspension was filtered through a " technico " filter , using a ford 's " sterimat " grade g.s. the fitrate was used as the inoculum , the amount inoculated on to each membrane varying between 0 - 02 to 0 - 06 ml . four 10 - day embryonated eggs were inoculated , using a graduated capillary pipette as a dropper . in order to secure a wide distribution of the virus over the membrane , it was placed direct on to the shell membrane , and a tear made through this with a glass needle . 
the virus was then drawn into the egg and on to the chorioallantois by applying negative pressure to the air - cell with the aid of a small rubber teat . 
the egg was then sealed in the normal way and incubated for 3 days.when opened and examined , small roughly circular opacities were found on the chorioallantois of 3 embryos . 
an occasional attempt at the formation of a " cell nest " may be found , but usually the cells occur in groups without any sign of a whorled appearance . 
carcinoma simplex , with large round and spindle - shaped cells . experiments 10 and 11 were chorioallantoic implants using methylcholanthrene induced transplantable mammary carcinomas of mice . five 10 - day embryonated eggs were implanted with fragments of tumour and examined 7 days later . all but one contained small tumours 3 - 5 mdiameter . 
of a suspension of mouse sarcoma s.37 in twenty - seven embryos subsequently died at periods varying normal saline . most of these showed congestion and petechial haemorbetween 1 and 8 days . rhages in the skno bacteria were isolated from these eggs . 
the dead embryos showed intense congestion and petechial haemorrhages . in 2 cases tumours were found tumour - bearing membranes were attached to the interior of the yolk - sac . ground up with sand and saline , and 0 - 25 ml . 
a haemorrhagic membrane was treated in the nine days later the mice were found dead , same way and injected into 5 mice . due to a heating failure during a cold spell . six of the mice injected with tumourbearing membranes were found to have small lymphoid turnours growing in the subcutis at the site of injection . 
the membranes appeared normal upon histological examination . ( e ) spontaneouvs chicken tunours . in experiments 19 , 20 and 21 the intra - vitelline method was again tried . these experiments may be briefly dismissed , as in each case contamination with bacteria killed all the eggs . 
coli was isolated from the eggs , although broths inoculated with tumour tissue from the original case remained sterile . experiments 20 and 21 consisted of the injection of a saline suspension prepared from lymphocytomata , involving the thigh and ovary respectively . the embryos died subsequent to injection , and bact . 
hen suffering from aleukaemic lymphoid leucosis . eight days later two of the embryos were found to be dead , namely those with liver and liver plus spleen implants . only the latter had a tumour in the membrane . 
the remaining spleen only implanted embryo was living , and the membrane bore a 4 mdiameter pink tumour . in the case of the dead embryos both were extremely congested , and the livers appeared swollen and leukaemic . histological examination of the membrane bearing the spleen implant shows a vascular growth of endothelial - like structure . all resemblance to normal or even leukaemic spleen has disappeared . 
the growth is composed of an irregular syncytium of calls with round , angular or elongated nuclei , the cytoplasm of which is drawn out into processes which appear to merge with those of adjacent cells . 
the vessels are formed of a single layer of flattened endothelium and are congested . at the periphery of this tumour large numbers of primitive blood cells appear to be wandering into the mesenchymal stroma of the chorioallantois . " cell nests " occur in this region . 
an examination of the heart blood from these two embryos shows in the case of the liver only implant a large number of primitive cells which appear to be differentiating into erythroblasts , i.e. 
the bird was destroyed and immediately opened , and the viscera were exposed to the air in the post - mortem room for about 2 hours before the case was seen , but the liver surface was seared with a hot spatula at the time of implantation , and fragments taken from within the organ with sterile knife and forceps . 
the actual implants were made about 21 hours after the fowl was destroyed . broths inoculated with tumour material at the same time were later seen to be sterile . nine days later two embryos were found to be dead . 
the second method of tissue culture is involved and requires an elaborate technique , and has the great drawback that frequently only one component of the original neoplasm grows , while the rest , e.g. 
more experiments involving sub - inoculation with tissue fitrates and extra - embryonic fluids from dead and haemorrhagic embryos should help to settle this point . the chorioallantoic method has been found to be most successful in the case of the cultivation of avian tumours associated with viruses . thus , the rous i sarcoma and the duran - reynals sarcoma give the biggest growths in the membrane . these are both rapidly growing tumours , and therefore would naturally tend to give better results in the short period ( never more than 14 days ) of cultivation . slow growing tumours usually give disappointingly small growths , whilst normal adult tissues may fail to grow and be absorbed . in the case of the rous and duran - reynals sarcomata , the virus stimulates the mesenchymal tissue of the chorioallantois to participate in the general malignancy , thus augmenting the size of the implant . 
of more interest , however , is the observation , originally by keogh ( 1938 ) , that the rous virus also appears to stimulate the ectodermal cells of the chorioallantois to proliferate in an apparently uncontrolled manner . 
he speculates on the possibility that the virus may be carcinogenic , not only for mesenchymal tissue , but also for epithelium ectodermal proliferation due to rous virus has been under certain conditions . confirmed in the present investigation , and the pathological changes in the membrane ectoderms produced by the rous and duran - reynals tumours have been compared with those produced by dermatrophic viruses such as those of fowl - pox and contagious papillomata of cattle , also with similar changes noted in the membrane adjacent to certain implanted spontaneous tumours of the chicken . as a check on these observations a number of experiments were performed with chemically induced tumours of the mouse , rat and chicken ; also with normal adult and embryonic chicken tissues . the significance of the " cell nests " or " epithelial pearls " is interesting , resembling as they do transverse sections of infiltration cores of epithelial tissue similar lesions were noted by which characterize squamous - cell carcinoma . huxley and murray ( 1924 ) adjacent to the fragments of chick embryos implanted on the chorioallantois . it is well known that embryonic tissue extracts contain growth - promoting substances , and for this reason are frequently added to tissue culture media . claude ( 1938 ) showed that a fraction could be isolated from chick embryos which j . 
campbell possessed the same physical and chemical properties as the purified active fraction despite these similarities , however , the embryo extract of the rous i sarcoma . failed to produce tumours in susceptible chickens . in this connection it is interesting to note that earle ( 1943 ) noticed an apparent malignant transformation of mouse fibroblasts grown on a fibrin clot and bathed in horse serum and chick embryo juice . these observations , together with the production of ectodermal proliferation and cell nest formation found to be associated with so many chorioallantoic implants of tumnours in the present investigation , gave rise to the conception that tumours and embryonic tissue might contain growth - promoting substances capable of causing the overgrowth of the ectodermal layer of cells in the embryonic membrane . if this proved to be the case it might be possible to demonstrate some relationship between the intensity of the membrane reaction and the type of tumour implanted , especially from the aspect of virus content . 
no mention of " epithelial pearls " is made by keogh ( 1938 ) , or by the numerous other workers who have studied ectodermal lesions of the chorioallantoic membrane induced by viruses . a number of experiments were devised in order to test this hypothesis , and especially to study the membrane reaction to a spontaneous liver carcinoma of the duck , which is described in a separate paper . table i shows that the ectodermal lesions do not appear to be as specific as in all cases where tumours known to contain virus , or fitrates of was hoped . such turnours , or dermatrophic viruses , were placed on the membrane , proliferation of the ectoderm took place . in some instances eosinophilic " inclusions " were observed , but the nature of these is not clear , except of course in the case in the main , virus alone caused simple proliferation without the of fowl pox . formation of " cell nests . " in general those tumours which failed to grow subsequent to implantation and were absorbed did not cause any detectable lesions in the membrane ; similar results were obtained for normal adult tissues . also in several cases , although not invariably , an accidental infection of the membrane with bacteria did not result in ectodermal proliferation . the spontaneous chicken tumours which grew successfully all caused proliferation and the formation of " cell nests . " it was thought possible that chemically induced tumours , being presumably free of virus , might give a different membrane reaction . 
the majority of spontaneous tunours give disappointingly small growths . it has been shown that the capacity for indutcing ectodermal proliferation in the chorioallantois is not confined to tumour viruses , or to fowl pox and other non - tumour associated viruses , but occurs in the membranes adjacent to the majority of implanted tumours , whether spontaneous , virus associated , or chemically induced ; or even occasionally in response to bacterial growth . attention has been drawn to the tendency of the proliferating ectoderm to form " cell nests " or " epithelial pearls , " resembling those occurring in squamous - cell carcinoma , and the significance of this has been discussed . the induction has been described of two distinct leukaemic conditions in chick embryos as the result of implanting tissues from a third type of spontaneous leukaemia in a fowl , and has been briefly discussed . i wish to express my gratitude to professor a . 
murray drennan , of the pathology department , university of edinburgh , for his interest in this work , and for the numerous suggestions as to the manner of development of the investigation . all the fertile eggs were obtained from a . 
7. received for publication february 3 , 1949 . one of the surprising elements in bittner 's discovery of the " milk factor " is the apparent entry of the virus into the bodies of the young mice via the it is , however , obviousthat during suckling a small amount alimentary canal . of milk may also enter the nostrils , and that the nasal mucosa may offer an alternative port of entry . it also seems possible that the milk factor might be destroyed by digestion in the stomach . if this were so it would be difficult to recover milk factor from the stomach contents of suckling mice . 
the unfortunately the experiresult was entirely negative in the 40 mice so treated ment was not adequately controlled , in that none of the mice were tested for susceptibility by means of extracts known to contain the virus . 
he was considered too old for successful operative treatment so he was kept under observation and in february , 1954 , was readmitted to hospital with evidence of bone metastasis . 
apart from this , there is little irregularity of nuclear shape , size or staining density . these cells clearly form part of a fragment of tissue in the sputum , and because of the vacuolation of the cytoplasm , were considered to be diagnostic of adenocarcinoma . 
they are of adenocarcinomatous type and do not resemble cells usually seen in primary bronchial carcinomata . " an enlarged cervical gland was later removed for histological examination and was reported as showing a mucus - secreting adenocarcinoma , probably of colonic origin . the patient died , and post mortem examination was refused . it will be noted that the cells shown in the clump in fig . 
4 appear to surround a number of vacuoles , but gross vacuolation is not evident in the cells themselves . the larger mass is hollow , the wall being formed of a single layer of cells . i make it a practice only to report adenocarcinoma from sputum examination it cannot be too strongly emphawhen clumps of the types described are seen . sised that single cells containing vacuoles as shown in fig . 
shujbik. from the oxford university reseach centre of tje british empire cancer campaign , sir william dunn scoo of pathology , unirersity of oxford . received for publication november 20 , 1948 . though non - carcinogenic to normal skin , croton oil elicits tumours in skin previously treated with a carcinogen for an inadequate period ( berenblum , 1941 )  . this procedure , with the modification of mottram ( 1944 ) , using only one single application of carcinogen prior to the croton oil treatment , served as the basis of a quantitative analysis of carcinogenic response ( berenblum and shubik , 1947b )  . 
the results led to the establishment of the essential difference in mechanism between the preliminary " initiating process " and the subsequent " promoting process " of carcinogenesis . for reviews of the literature dealing with earlier work on the stages of carcinogenesis , and with the previous terminologies used , see berenblum , 1944 , 1947 ; rusch , 1944 ; berenblum and shubik , 1947a and b . from this analysis ( berenblum and shubik , 1947b ) , it was concluded that the initiating process represents a sudden and irreversible change in a small minority of the cells of the treated area , giving rise to isolated " latent tumour cells , " apparently mdtinguishable morphologically from the surrounding non - neoplastic cells . 
the presence of these latent tumour cells is only demonstrable by subsequent promoting action , which converts them into morphological tumours . this promoting action is less specific than the initiating action , in that it can as readily be induced by croton oil as by continued applications of a true carcinogen . the irreversible nature of the initiating process was demonstrated by the fact that the number of tumours elicited by croton oil was as great after an interval of 20 weeks ( between the carcinogen application and the commencement of croton oil treatment ) as after an interval of only 3 days . according to this new concept , the latent period of carcinogenesis is dependent on the efficacy ' of the promoting action , while the actual turnour yield is prethis was borne out by comparative tests , determined by the initiating action . using 3 : 4 - benzpyrene , and 9 : 10 - dimethyl - 1 : 2 - benzit was found , as anthracene , as initiators , followed by croton oil treatment . expected , that whereas the percentage of tumour - bearing animals differed in the three series , the latent periods were approximately the same . 1 : 2 : 5 : 6 - dibenzanthracene , unfortunately , owing to considerations of solubilities , it was necessary , in these comparisons , to use a different concentration for each carcinogen . consequently , more than one variable was involved in the experiment . 
while the results obtained provided an adequate basis for the general conclusions referred to above , it was felt , nevertheless , that unequivocal evidence could best be 110 i . 
shubik provided by studying the effects of a series of graded concentrations of one and for this investigation , described below , the same carcinogen as initiator . 9 : 10 - dimethyl - 1 : 2 - benzanthracene was chosen as initiator . an additional purpose of this investigation was that the quantitative data thus obtained could , at the same time , serve as indirect evidence for or against the possibility of a " mutation - like change " for the initiating stage of carcinohowever , for a re - assessment of the validity of the " somatic cell genesis . mutation theory of cancer " in the light of the dual - stage mechanism of carcinogenesis , a more direct experimental approach was required . such an approach seemed possible from the following considerations . mustard gas is known to possess mutagenic properties when tested on drosophila ( auerbach and robson , 1946 , 1947 ) , and on neurospora and e . 
coli ( tatum , 1947 ) , so that , according to the somatic cell mutation theory , this compound admittedly , mustard gas is a potent should act as a carcinogenic initiator . anti - carcinogenic agent ( berenblum , 1929 ) , but this effect was shown to be confined to the later stages of carcinogenesis ( berenblum , 1929 , 1931 ) , and could thus , mustard gas should , thus be attributed to an anti - promoting action ; theoretically , still be capable of initiating action . 
the experimental areas of skin , in the inter - scapular regions , were clipped periodically all test solutions were applied with a with fine scissors for removal of hair . glass rod , and colourless , non - fluorescent , liquid paraffin ( " liquid petrolatum " ) was used as solvent throughout , for standardization of response ( berenblum and schoental , 1947 ; berenblum and shubik , 1947a )  . the main departure from the technique of the previous experiments was that instead of merely noting the numbers of tumour - bearing mice , the individual tumours were also recorded . 
from these results , and from other evidence brought forward , it was concluded that the ultimate tumour yield in carcinogenesis is pre - determined by an irreversible initiating process , while the latent period of carcinogenesis , i.e. 
the speed with which the induced " latent tumnour cells " are converted into morphological tumours , is a function of the subsequent promoting process . the idea of the possible existence of " latent tumour cells " requiring additional stimulation , i.e. 
the results suggest that the acetylaminofluorene acted as initiator , and the goitrogenic agent as promoter , in an analogous fashion to the carcinogen and the croton oil , respectivelv.y , in the case of skin experiments . in the present investigation , one and the same carcinogen was applied to the mouse 's skonce only in different ( graded ) concentrations , to serve as initiator , and then followed by repeated applications of croton oil . expressed in ratios , the concentrations of initiator ( 9 : 10 - dimethvl - l : 2 - benzanthracene in liquid paraffin ) in the four experimental groups were 1 : 3 : 9 : 27 , and the total yields of tumours for the corresponding groups were in the ratio of 1 : 6 - 6 : 12 - 4 : 26 - 5 ( table yet the average latent periods for these 4 groups were closely similar , ii )  . namely , 14 - 4 , 12 - 1 , 10 - 6 , and 11 - 8 weeks , respectively . 
not only was there a progressive increase in the total number of tumours , with increase in concentration of initiator , and also in the number of tumour - bearing animals . 
many different experimental approaches have , however , been devised in recent years to obtain , at least , indirect evidence in support of the theory , and these may conveniently be considered under the following headings : 1 . 
induction , by knonn carcinogenic agents , of mutations in louer organisms . the early studies in this field were concerned with x - ravs and ultraviolet although radiation , the literature of which is well reviewed by muller ( 1941 )  . most of this work was not directly concerned with correlating carcinogenicity 114 i . 
genetic analysis of tumour transplantation phenomena in pure strain mice . the genetic control of tumour transplantation in pure strain mice has been investigated in some detail , and the earlier work in this field is well smmarized it has been shown that a number of genes control the behaviour by little ( 1941 )  . of certain tumours , and this approach has been extended further by gorer ( 1937 , 1947 ) , showing that these genes probably determine their antigenic proalso , according to strong ( 1926 ) , bittner ( 1931 ) and others , the observed perties . sudden change in the transplantation properties of tumnours could be explained on the basis of the occurrence of mutations . 
quantitative interpretation of carcinogenic experiment . several attempts have been made to evaluate quantitatively some of the more reliable carcinogenic data , to determine whether or not such data would be in keeping with a sudden irrev%ersible change of a mutation - like nature . in the investigation of dunning , curtis and wood ( 1940 ) , the production of sarcomas in rats , by subcutaneous injection of 3 : 4 - benzpyrene , was submitted to quantitative analysis . 
the concentration of carcinogen and the volume of fluid injected , both of which were variables , were correlated with the number of tumours induced and with the latent period of tumour induction . it was found that increasing the number of foci injected did increase the number of tumours induced , whereas increasing the volume of fluid injected in one locus did not . in view of the variables involved , and for other reasons to be discussed later , these results do not lend themselves to an exact interpretation of a single response to a single stimulus . charles and luce - clausen ( 1942 ) analysed data of a mouse skin carcinogenesis experiment , using continued painting with 3 : 4 - benzpyrene , to determine whether or not this was in keeping with the concept of the somatic cell mutation theory . in their introduction , they make the primary assumption that if a mutation were the basis of carcinogenesis , it must , of necessity , be of a recessive nature , thus postulating two successive mutations to bring to light an actual tumour . there is , however , no valid reason for this assumption , which is , in fact , at variance with the theory of dominancy , as proposed by fisher ( 1930 )  . in all these previous attempts at analysing carcinogenic experiments , in which the carcinogen is allowed to act continuously , there is the inevitable complication arising from the fact that , of the two stages of carcinogenesis , only one - the initiating stage - could possibly be ascribed to a mutation , since this is the stage which involves a sudden and irreversible change , possibly affecting one cell only . 
shlbik in the present investigation , the correlation of concentration of carcinogen , as initiator , with the total number of turnours induced , has revealed approximately a direct 1 : 1 ratio . this could be taken as being in keeping with the somatic cell mutation theory . however , the other investigation , described above , does not lend support to as already mentioned , mustard gas is a potent mutagenic agent this theory . on drosophila ( auerbach and robson , 1946 , 1947 )  . since its anti - carcinogenic properties ( berenblum , 1929 , 1931 ) can undoubtedly be attributed to antipromoting action , it was to be expected , according to the somatic cell mutation theory , that when allowed to act once only on mouse 's skin , followed by repeated croton oil treatment , tumours should have arisen , the mustard gas acting as an initiator by virtue of its mutagenic properties . 
when tested , this was found not to be the case . in view of this negative finding , and in the light of the highly conflicting evidence of recent experiment in an attempt to adduce more indirect support of the theory , it becomes necessary to re - assess the validity of the theory . basically , neither proof nor disproof of the somatic cell mutation theorv of cancer is possible ( haldane , 1934 ) , as referred to above . the accumulating indirect evidence would seem to run counter to the theorinstead of supporting of the evidence presented in the present communicationi , the first experiment is consistent with the theory , while the second is strongly against it . the force of past reasoning in support of the theory has rested largely on the assumption that , given an irreversible change as the basis of carcinogenesis , the only known biological phenomenon to explain this would be a mutation . however , a closer examination of other common biological phenomena instantly reveals that this is not so . for example , in the course of the development of the embryo , the divergent differentiation that ultimately results in the irreversible cell types , e.g. 
horning. from the chester beally research institute of the royal cancer hospital , london , s.w.3. received for publication december 12 , 1948 . recfnt experience has shown that many of the growth - inhibiting agents used in the palliative treatment of cancer are carcinogenic . 
they also cause specific damage to cell nuclei and chromosomes and are able to induce mutations . the association of these biological effects of ( 1 ) growth inhibition , ( 2 ) chromosome damage , ( 3 ) production of mutations and ( 4 ) induction of cancer suggests if the that they may have a common fimundamental biochemical mechanism . induction of cancer is indeed a somatic mutation , then cancer induction might be included as a special mutation . 
the fact that x - rays can produce cancer in man was published in 1902 ( frieben , 1902 ) , seven years after rontgen 's discovery muiiller ( 1928 ) found that x - rays are mutagenic , and later mather of x - rays . and stone ( 1933 ) and koller ( 1934 ) described the chromosome damage following irradiation . 
the idea that cancer arises as a somatic mutation was supported by the demonstration of an increased incidence of mutations occurring in mice this was shown with methylcholanthrene treated with chemical carcinogens . by strong ( 1945 ) and with 1 : 2 : 5 : 6 - dibenzanthracene by carr ( 1947 )  . carcinogenic hydrocarbons inhibit the growth of animals and the establishment and growth of transplanted tumours ( haddow , scott and scott , 1937 )  . 
it would be wrong to give the impression that undesirable sequelae are common , yet such complications as wound sepsis , necrosis of the skin edges and a poor functional result are still seen with greater frequency than one would expect following an operation which has been abundantly practised by innumerable surgeons all over the world for over half a century . 
these particular sequelae are essentially a reflection on the judgment or the executive skill of the operator and not upon the operation itself , because with care they need not happen . 
furthermore , such indifferent results become known , and because they lose nothing in the telling may have a serious deterrent effect upon patients contemplating advice about a newly acquired lump in the breast . 
it is to be remembered that we are operating under almost ideal conditions - the patients are constitutionally well and often near the prime of life , the anatomy of the area is normal and not distorted as it might be , and there are none of the embarrassments associated with operations within a body cavity . 
a very high degree of technical excellence should therefore be our aim , both in regard to the thoroughness of the dissection which has as its objective the extirpation of the disease , and in regard to the care with which this is carried out , which can so much determine the degree of ultimate functionaf disability . 
 there are three features of the " skin short " case which need some explana i will call them ( i ) anticipating the gap , ( ii ) siting the gap , ( iii ) covering tion . 
riddell surgery - may be influenced ; second , the surgeon is forewarned , and so can avoid being surprised into an awkward situation at the end of a long operation . 
 an assessment - an estimate - should be made in all new cases of cancer of the breast of the amount of skin that will be left for closing the wound after the breast and tumour have been removed . 
it will be found that patients fall into two categories : ( 1 ) a larger group in whom it is judged that it will be possible to approximate the skin edges in the usual way without tension . 
h we remove too little skin , secondary nodules will appear for certain and quickly ; if we remove a more generous amount - - as we must - we shall have to be prepared to deal with a gap . 
 in these patients two alternatives are open to us : either we can proceed to radical mastectomy , skin graft the resulting gap , and hope that the skin covering it will heal in a reasonable time and so allow early post - operative irradiation , or we can anticipate the probable delay in healing by giving the x - ray treatment before the operation . 
 personally in this small group i prefer to give the x - ray treatment first , because in practice unfortunately every skin graft does not take uniformly , so that a proportion of cases are left to heal - at least in part - by granulation , and this takes time ; indeed , sometimes so much time that post - operative x - ray treat ment may be delayed to a point where its usefulness is open to question . 
for this reason it is suggested that if by careful pre - operative clinical assessment we can anticipate and so forecast such a defect arising , we should consider giving the x - ray treatment before the operation . 
the use of pre - operative irradiation does not in any way absolve the operator subsequently from still adhering to the principle of excising a wide area clear of the growth . 
this patient was treated by pre - operatilre irradiation followed by radical mastectomy with an immediate skin - gra the satisfactory functional result can be attributed to ( i ) adoption of the " arm raised " position before approximation of the skin flaps , ( ii ) the early recognition of the inevitability of " a gap " in this type of case and of the need for a skin - gra fro . 
2. - full range of movement : the " arm raised " position is the most delicate test of function at the shoulder following mastectomy ; six months should be allowed after the termination of all treatment for the skin to regain its suppleness beforp 8 - ing function ; inability to raise the arm vertically after such an interval must be regarded as an imperfect functional result . 
3. - llarginal flap necrosis : the illustration shows an area of skin loss as a result of damage to the blood supply of the lateral flap during its elevation . 
at the same time it is not vital to graft ; what is vital is that a gap should be left in a skin short case ; whether a dressing of skin is put on that gap or not is almost a secondary consideration , although skin is very clearly to be preferred to scar tissue if the gap is a large one . 
 the time lo gra the decision as to whether the graft is applied at the time of the mastectomy or not depends solely on the condition of the patient at the end of the operation . 
 h this is unsatisfactory , as it may be in an elderly patient , no harm is done by leaving a raw area and grafting early in convalescence , usually at the time of the first major dressing . 
 if , in addition , we have made our pre - operative reconnaissance , the procedure is robbed of its only disagreeable feature , the element of surprise , since a donor area will have been chosen and prepared and the few special instruments and dressings will be immediately available . 
this accident most commonly occurs as the dissection approaches the anterior border oflatissimus dorsi , which corresponds with the deepest and darkest part of the wound ; it is usually due to hurrying this part of the reflection in a field obscured by haemorrhage ; the blood 811pply may also be cut off from a portion of the flap by the use of tension sutures and with the same result . 
riddell displacement of sk in the second category the skin is not lost in the sense that it is destroyed , but is lost by displacement , because skin is borrowed from the axilla and upper arm to close the axillary part of the wound . 
 ( 2 ) slide the skin of the lateral flap well up into the axilla ; by making use of the longer contour of the lateral flap in this way an adequate supply of skin in in suturing the flaps together exactly opposite points on the axilla is assured . 
 in other words , lend skin from the lateral flap to the axilla ; do not borrow it from the axilla and upper arm by bringing the arm down to a right angle or less . 
 i should perhaps add that in my experience functional disability at the shoulder is not related to loss of the pectoral muscles ; indeed , it can be quite severe following a local mast.ectomy , and is not related t - 0 failure to employ early fig . 
the drawing shows the correct position of the upper limb before closing the wound ; the skin of the lateral flap should be pushed well up into the axilla before suturing ( arrow )  . 
in a series of cases examined in which the subscapular nerve had been divided , no functional disability could be found by comparison with control cases and with the opposite side , although , of course , there was a positive r.d. 
the aim is to display the anterior border of the latissimus dorsi muscle , and in " skin short " cases to mobilize the lateral flap still further by carrying the dissection backwards for two or three inches beyond this point , keeping on a plane buperficial to the muscle . 
the aim is to raise a flap of even thinness , but if by a careless stroke of the knife the flap is cut too thin , the blood supply will be damaged and the whole course of convalescence unnecessarily prolonged . 
h too thick a flap is raised the dissection may in error proceed on the deep face of latissimus dorsi into the space between this muscle and the serratus anterior , a space which is filled with large veins . 
h , on admission , the patient is severely anaemic , blood should be given , but let the transfusion be given before the operation ; it can be supplemented by plasma or other blood substitute during the operation if necessary . 
this is a partial contradiction of views ex pressed earlier in my experience ( riddell , 1948 ) , and is based on the fact that blood transfusion to an unconscious patient carries with it an extra hazard - slight though it may be - for the patient cannot proclaim against the blood if it is incom patible , as would be possible if she were conscious . 
the towelling of the operation area should be so arranged , by placing a towel behind the patient 's back , that there is no unprotected area on the flank from which the main wound might be contaminated ; hot wet packs , which so quickly become cold wet packs and chill the patient , should only be used for haemostatic purposes at the end of the operation ; dry hot packs 296 v . 
 drainage should never be employed through any part of the original incision , because it can so easily lead to cross infection of the main length of the wound ; it is best carried out through a separate stab incision in the lateral flap , pre ferably well clear of the hair and sweat - bearing skin of the axilla . 
lastly , let us banish for all time the use of tension sutures , and above all the expression f 10 . - the composite dra ' lring illustrates ( a ) the position of the leg for cutting an imme it is a sound precaution to towel up all " skin - short " cases with the diate skin - gra donor area prepared and &ec8111111 > le . 
functional disability usually takes the form of restricted movement at the shoulder and is doubly undesirable , since it not only seriously reduces the range of w ! efo1ness of the limb concerned , but aggravates by constant reminder the psychological trauma resulting from the operation . 
3. received for publication january 21 , 1948 . during the war the pharmacology of the nitrogen mustards or chloroethylamines was studied intensively ( gilman and philips , 1946 )  . in the course of these investigations it was observed that tissues with a high proportion of dividing cells were particularly injured . this discovery led to the application of these substances in the treatment of malignant growth . 
of dimethyl - , - chloroethylamine hydrochloride by subcutaneous injection . such treatment when given repeatedly caused inhibition of some spontaneous mammary tumours ( table i ) , but had very little effect in prolonging the life of mice with transplanted lymphosarcoma . this compound given in single doses of 100 mg . 
the effect is similar to that induced by radioactive substances ; it is identical with the phenomenon of depigmentation in mice caused by subcutaneous implantation of plutonium ( brues , 19 , 47 , personal thus " bleaching of hair - colour " is another example of the communication )  . radiomimetic actions of the bis - chloroethylamines . the metabolism of walker carcinoma tissue from rats dosed with 1 mg . 
a variant of this compound , dimethyl - ] 3 - chloroethylamine hydrochloride , was used in 3 other cases , reported here because of the favourable response in 1 case . 
on two consecutive days in 30 cases , in 10 of which treatment was repeated once or several times at 3 - week or longer intervals depending upon the length of remission from symptoms . 
the majority of patients with advanced bronchogenic carcinoma have white cell counts above 10 , 000 per c.mm. , and such patients do not develop the moderate to severe leucopenia observed in cases of hodgkin 's disease ( apthomas and cullumbine , 1947 )  . in only 2 of our patients has the white cell count fallen below 4000 per c.mm. , in these cases to 1000 and 1800 with restoration to normal counts in 3 weeks ' time . the first of these cases had had previous radiation therapy , and at the commencement of treatment had a white blood cell count of 4000 per c.mhaemorrhagic nianifestations have not been observed in this group , nor has any significant change in haemoglobin dosages of 0 - 2 mg . 
at 10 - day intervals can be tolerated for been noted . periods of at least 10 weeks , as judged by the 4 cases we have treated over such a period . 
the presence of fever , pleural exudation or jaundice are not , in our experience , contraindications to the use of the drug . the adverse effects of the dimethyl compound were observed in 3 patients , 2 of whom are not included in this group as their diagnosis was not histologically proven . 
one patient was carried on for a period of 5 months with marked relief of pain , cough and dyspnoea and decrease of sputum for 18 to 21 days following each course of injections . 
a patient with remission of symptoms for 6 to 8 weeks after each treatment is still being observed one patient receiving dimethyl - , 3 - chloroethylamine is still in after 9 months . remission 7 months after treatment and leading a normal life . 
the relief of dyspnoea in some cases is almost complete - an observation very difficult to explain , for in such cases there may not be corresponding observable changes in the lungs . relief of general malaise and anorexia is also noted in over half the cases following the initial 1 - or 2 - day period of adverse effects . 
warwick sputum usually increases in amount for several days , and is said " to come up more easily . " the amount may then fall off rapidly , in some cases from 90 - 120 ml . 
the sputum may also change in character from purulent to colourless . reabsorption of pleural exudate or decreased rate of formation has been these observations are of interest in that most radioseen in 5 of 13 cases . ' therapists hesitate to give treatment to cases with pleural exudation because of the tendency to increase the amount of exudate . superficial metastases of measurable size decreased in 3 of 10 cases . 
a larger total number for such observations wouild have been obtained had not metastatic nodules been removed for microscopic study at various intervals following injection in 8 cases . twenty - two patients who had weight loss were weighed weekly following in 9 of these cases weight loss continued for approximately 1 week , treatment . following which a gain in weight occurred amounting uisually to 2 to 8 lb . four patients gained 10 to 15 lb . 
in 2 months , and 1 patient who lost 40 lb . in the 18 months prior to treatment with dimethyl - 3 - chloroethylamine has in 7 months regained all her lost weight . radiological evidence of decrease in size of pulmonary metastases and re - aeration of segments or lobes was observed in 8 of 35 cases . 
hb , 55 per cent . 3 , 800 , 000 . heart , mediastinum and trachea displaced to the right ; appearance of atelectasis with probable cavitation near 2nd right carina broadened rib . and invaded on the right by a large nodular friable mass completely occluding the right main bronchus . bronchoscopy report from harefield in april , 1946 . pathological report : adenocarcinoma with numerous mitotic figures . treatment : dimethyl - chloroethylamine 2 mg . 
a corresponding effect in a tumour of the breast might reasonably be expected not to be noticed in support of such a suggestion is the fact that a similar relief by the patient . of respiratory symptoms following chloroethylamine without radiological evidence of changes in the lungs has been observed in a case of carcinoma of the breast with pulmonary metastases . 
by repeating the treatment at suitable intervals the life of animals with tumours can be prolonged , but cessation of treatment leads to recurrence of tumour growth . forty - one cases of histologically proven carcinoma of the bronchus unsuitable for other forms of therapy have been treated with the chloroethylamines . 
3. received for publication february 6 , 1947 . following the discovery by haddow and sexton ( 1946 ) of the effects of ethylcarbamate ( urethane ) on the growth and differentiation of the walker rat carcinoma , the action of this substance in human leukaemia was described by paterson , apthomas , haddow and watkinson ( 1946 )  . since the early experiments of warburg in 1910 , ethylphenylcarbamate ( phenylurethane ) had been known to arrest the division of the sea - urchin egg at metaphase . 
a similar effect in plant cells , closely resembling that of colchicine , was discovered in 1939 by lefevre and by simonet and guinochet ( 1939 ) , and was further studied by gavaudan ( 1943 ) and deysson ( 1944 )  . ludford ( 1936 ) treated tissue cultures with a 2 per cent solution of ethylcarbamate and noted abnormal metaphases and a considerable amount of nuclear and cellular degeneration . similar results were obtained by geiersbach ( 1939 ) , and ostergren ( 1944 ) also claimed that ethylcarbamate arrested mitosis at metaphase in alliutempleman and sexton ( 1945 ) , investigating the growth - inhibiting properties of numerous carbamic esters in plants , found , however , that ethylcarbamate was inactive in this respect , although marked activity was shown by ethyl phenylcarbamate and it was this work which led haddow and sexton isopropyl phenylcarbamate . to investigate the action of carbamic esters on tumour growth , and to the discovery that in this case ethylcarbamate itself is effective . these authors suggested that this substance might belong to the group of caryoclastic ( nuclear ) poisons studied by a . 
described by gorer ( 1946 ) was utilized , in which large stem - cells produced a diffuse infiltration of lymph nodes , spleen , liver and kidneys , leading to death of the mice in from 14 to 22 days after subcutaneous grafting of leukaemic tissue . enumeration of reticulocytes was made from dry blood smears , following postvital staining with * associe du fonds national belge de la recherche scientifique . 
the nucleus then disintegrates , the thymonucleic acid material forming shell - like structures covering an acidophil sphere , which also contains some ribonucleic acid ( by the further destruction ribonuclease method ) and the remnant of the nucleolus . leads to irregular fragments , with a positive or negative feulgen reaction . 
52 and within 3 days the number of reticulocytes was close to the initial value . no significant change in the numbers of red blood cells , or in the leucocytes , was observed . these results may be compared with those following the injection of colchicine , when the reticulocyte fall is marked and the minimum is also reached in 48 hours . 
the erythroblastic mitoses are arrested in metaphase by colchicine during the first hours following its injection , and the delayed decrease of the number of reticulocytes is a consequence of the time needed for the maturation of the erythroblasts . 
by comparing the histological pictures found in these last two groups it is possible to appreciate the specific effects of ethylcarbamate . ( ii ) blood - picture . - the principal changes were an increase in the percentage of granulocytes and a decrease in the numbers of reticulocytes . 
no evident atrophy of the mucosa , nor ulceration . leukaemic infiltrations : no evidence of increased cell - destruction nor mitotic abnormalities . in animals losing weight during the experiment , splenic and lymphoid atrophy is more pronounced . 
the bone - marrow remains very cellular , with a there is no evidence of aplasia . high proportion of immature granulocytes . in the thymus the atrophy of the cortical region is complete , the epithelial cells this picture of " inverted thymus " is found after the pycnotic only remaining . destruction of thymus cells by mitotic poisons ( dustin , 1929 ) or non - specific in this case it is probable that the stimuli ( selye , 1937 ) , and in inanition . ethylcarbamate injections and the loss of body weight have additive effects . no marked changes are found in other organs . * rosin and doljanski ( 1944 ) have described inclusions in liver cells of rats treated with urethane , which they believe are red blood cells engulfed in cytoplasm and even in the nucleus . 
for 5 days , there was an increase in leucocytes from 9200 to 22 , 800 , and in granulocytes from 33 to 58 per cent . the bone - marrow showed very active granulopoiesis . bring about any aplasia of the bone - marrow in the rabbit . these preliminary results indicate that large doses of ethylcarbamate do not 2 . 
the possible relations between mitotic poisoning and the therapeutic action of ethylcarbamate in human leukaemia are discussed . this work has been supported by grants to the royal cancer hospital ( free ) from the british empire cancer campaign , the anna fuller fund , and the jane coffin childs memorial fund . 
bartholomew 's hospital , london . received for publication february 3 , 1953 . this investigation was planned at a meeting on august 29 , 1949 , at the baggeridge colliery , staffordshire , ' arranged by a . 
some small series of cases suggest that silicosis may predispose to cancer of the ' lung , but the general indication of the literature is that silicosis is not active in this respect . 
hence the area where there is most pneumokoniosis shows a low incidence of lung cancer . the prevalence of pneumokoniosis in any area is indicated by the number of compensation cases arising under the workmen 's compensation acts and the industrial injuries scheme . 
4. - numbers of deaths from cancer of the lung in coal miners , and of wage - earners on colliery books , from 1921 . 1930 1940 face may be included , but this criterion must be difficult to apply to non - stationary however , in practice , the doubtful cases may not be very numerous , workers . and one must match the entry on the death certificate as nearly as possible with one of the official occupations . the increase in deaths from cancer of the lung . the increase in deaths per annum attributed to cancer of the lung from 1921 to 1950 is shown in tables iii and ix and in fig . 
some possible reasons for these differences are discussed . ( 2 ) in the last 30 years the mortality from cancer of the lung has increased in coal miners in the same way as in the general population ; in view of the peculiarities of the miner 's life , this fact calls for further inquiry . ( 3 ) the incidence of cancer of the lung differs ( a ) in face - workers and in other it is low coal miners , and ( b ) in the various coalfields of england and wales . in the south wales coalfield , where pneumokoniosis is most prevalent . we are indebted to the officers of the national coal board named at the begining of this paper for the suggestions which initiated this inquiry . 
of these large towns other than london 42 are located in the northern region of england and 41 in the remainder of england and wales , these groups being designated as " north " and " south " in this paper . 
the total deaths in all county boroughs , numbering 70 , 110 , were divided by the census population at the centre of the period , 1931 , and " expected ratios " of deaths to population obtained for each of the 16 sex - age groups . 
the census population of each town at each sex - age group was then multiplied by the corresponding " expected ratio , " giving the " expected " deaths in that group in 1921 - 39 . 
the actual deaths in a particular age group , or at all ages , divided by the expected deaths at the corresponding ages , or by the summation of them in all the age groups , and multiplied by 100 , gave for each sex comparative mortality ratios ( c.m.r. ) at each age group and at all ages . 
these are only approximate indices , since no correction has been made for irregular population trends in some of the towns ; but in no instance would the error from that cause exceed 5 per cent , and for only a few towns would it exceed 2 per cent . 
the values range from 130 to 55 , those which are greater than 100 by at least twice the standard deviation being denoted by a + sign , and those less than 100 by twice the standard deviation are denoted by a sign . 
stocks as a percentage of the expected deaths , giving a series of group c.m.r. 's , indi cating how the relative excess or deficiency of mortality characterizing the towns within the group changed according to age . 
 other digestive indices : similar ratios for deaths from cancer of the liver and causes included in the international groups for diseases of the diges tive system except appendicitis and peptic ulcer . 
 in table i 23 of the towns had c.m.r. 's exceeding 100 by twice their standard deviation or more , and 30 had c.m.r. 's less than 100 by that amount . 
no more than 4 out of the 83 would be expected to give values differing from 100 by as much as this on account of random variations due to a small number of deaths , so it is evident that the deviations for 49 of the towns cannot be so accounted for . 
was from 142 to 61 , with 27 towns showing significant excess over 100 and 27 a significant deficiency , so the deviations for 50 of the towns cannot be accollnted for by random variation . 
 and the social class index on the one hand and the age index on the other have been calculated separately for the 42 northern towns and 41 other towns , and also for the 83 together . 
the values given in table iii show that cancer of stomach mortality is positively correlated with the proportion of unskilled workers in the populapion , more so in south than north ; and in england and wales as a whole the coefficients are about + 5 for each sex . 
there is , however , a strong negative correlation between the social class index and age index , mean ing that towns with larger proportions of unskilled labour tend to have smaller proportions of their adult populations with ages over 55 . 
when the age index is kept constant cancer of stomach is still positively correlated with social class index to the extent of + 3 to + 4 , and this agrees with a similar result for the metropolitan boroughs of london in 1921 - 30 ( registrar - general , 1948 )  . 
 it is now seen that there is also a small negative correlation between cancer of stomach and the proportion of people of the same sex alive at ages 55 and over , and that this does not disappear when the social class index is made constant . 
 this is important , because it shows that the great variation in cancer of stomach rates in the towns is not due to mere differences in the correctness of certification of this cause of death by doctors . 
it has been suggested that the notable differences between cancer of stomach rates recorded in britain , denmark and switzerland may be due to excessive statement of this as cause of death in parts of those countries . 
if that were so it would be expected that the over - state ment would be greater amongst old than amongst young people , since the care devoted to diagnosis and correct statement of cause of death inevitably diminishes after about age 55 . 
consequently , if the great differences in standardized death rates in different towns , and in social grades , were due to excessive statement of cancer of stomach in certain of them , those with high rates would tend to have larger proportions of old people . 
for males the contrast is greatest at ages between 35 and 55 , when the death rates in the aggregate of 20 towns forming group ( a ) were just double those in the 18 towns forming group ( d ) ; and after 55 the relative excess diminishes to only 35 per cent at ages 75 and over . 
for females the excess in group ( a ) compared with group ( d ) was around 90 per cent up to age 65 , and then diminished to 45 per cent at 75 and over . 
 a pronounced decrease in the dispersion of death rates as age advances after 45 in males and after 55 in females is to be seen in table v , where rates for cancer of the stomach in the different social classes of the population of england and wales in 1930 - 32 are compared in the same way . 
for males the excess mor tality in class v , unskilled labourers , compared with that in classes i - ii , pro fessional and higher graded occupations , was as great as 86 per cent at 35 - 45 , and diminished progressively to only 8 per cent at 70 and over . 
for the wives of men in class v and single women in unskilled occupations the excess was 80 per cent at 45 - 55 , and fell to 37 per cent at 70 and over . 
 these relations with age are the reverse of what would be expected if the large differences in causes of stomach mortality between various large towns and between social classes arose from differing accuracy of death certification . 
 it will be seen from table 13 of that publication that the dispersion of rates according to a housing density grouping were much smaller at ages over 65 than at 45 - 65 . 
if the differences between cancer rates in groups ( a ) and ( d ) of table iv were due to more complete diagnosis , or excessive diagnosis , of stomach cancer in ( a ) than ( d ) , there must have been corresponding deficiencies in causes of death other than cancer in the towns of group ( a )  . 
the total deaths in all the county boroughs during 1931 - 39 from the various groups of causes concerned , and from cancer of the stomach , at ages 45 - 65 and at 65 and over were as shown in table vii . 
10 , 568 at the age - groups 45 - 65 , 65 and over , the totals of cancer of stomach deaths were not much different from the totals of digestive diseases excluding peptic ulcer and appendicitis , and since the great bulk of any transfer of deaths into or out of the cancer group by wrong certification must pass out of or into the " other digestive " group , this means that a strong negative correlation must exist between death rates attributed to the two groups if the large variation in stomach cancer rates arises from diagnostic differences amongst the towns . 
 indeed , if this were the main cause , doubling the stomach cancer rate ( as in group ( a ) compared with group ( d ) towns ) would involve almost abolishing the rate for other digestive diseases . 
transfer might also occur between stomach cancer and peptic ulcer as a result of mis taken diagnosis , but the numbers of deaths attributed to the latter group were small in comparison with those attributed to the former , except amongst males aged 45 - 65 . 
it follows that the transfer of the whole of them to cancer , if that were possible , in certain towns would fail to account for the excess of certified cancer in those towns ; and even large negative correlations between the two causes could not account for the variation in stomach cancer amongst males over 65 or amongst females of either age group . 
 table vi shows that for males of both age groups cancer of stomach death rates had no appreciable correlation with either peptic ulcer or other digestive diseases ; for females of both age groups there was a small but statistically insig nificant negative correlation with peptic ulcer , and a small just significant positive correlation with other digestive diseases in the country as a whole . 
 since none of the factors tested above can account for the differences in tables i and ii , the remaining explanation is that some extrinsic irritant factor is concerned which differed in intensity in the various towns . 
the curious contrasts in cancer of stomach mortality in london boroughs when grouped according to their source of water supply ( registrar - general , 1947 ) , correlation coefficients were calculated between the c.m.r. 
for cancer of the stomach during 1921 - 39 and the estimated total hardness of thewater supply of the 83 towns during 1911 - 31 , as shown in tables i and ii . 
it has to be remembered that the location of certain industries has been influenced to some extent in the past by the need for a soft water supply , and that in the north of england much of the industrial population is served by soft water . 
of the 42 northern towns 23 had water supplies with less than 7 degrees , or 10 parts per 100 , 000 of total hardness ; their average social class index was about 37 per cent unskilled and partly skilled workers . 
the 9 northern towns with water supplies of 20 or more parts per 100 , 000 total hardness had an average social class ' lildex about 42 per cent ; and the correlation between hardness and social index was in the 41 towns elsewhere there was no correlation between significantly positive . 
 the coefficients of correlation in table iii between cancer of stomach mor tality and hardness were positive in the north for males and negative in the south for each sex ; and when all the towns are grouped according to an ascending scale of water hardness , it appears that the c.m.r. 
no expla nation is offered for this , but the : figures are placed on record because they might at some future time fit in with other facts ( table viii )  . 
 102 100 llo 100 100 whatever irritant may be concerned in the production of gastric cancer , the effect of greater intensity of the irritant in one environment than in another might be ( 1 ) to increase the proportion of people developing cancer at each age without changing the latent period of develop : ment ; ( 2 ) to shorten the average latent period before cancer appears without changing the proportions of people affected , or ( 3 ) to increase the proportion affected and also shorten the latent period . 
if it is a long - continued mechanical or chemical injury to cells the predominant effect to be expected from increased intensity of action would be a shortening of the latent period , without necessarily increasing the proportion of people affected , although that might also occur . 
the ratios between death rates in groups of towns and between social groups would not be expected to fall with advancing age after 50 or 60 as in tables iv and v , and this suggests that the irritant is not an infective organis assuming some form of chemical or mechanical irritant is concerned , the latent period before cancer appears will vary rather widely about a mean value in the manner characteristic of most measurable vital factors ; and if the latent periods of gastric cancers in residents of all towns could be measured they would form a distribution approximating to the " normal " type . 
 it would be possible to reproduce the observed age - incidence of deaths from gastric cancer on the supposition that the irritant begins to affect a certain pro portion , p , of people who are susceptible to it at about 15 years of age , and th.at at each year of age thereafter an additional proportion p / k become susceptible to it and begin to be affected . 
 if , for example , the mean latent period before death were 20 years , with a standard deviation of 5 and normal distribution , k being a suitable constant , the numbers of deaths at successive quinquennial age periods from 25 - 29 to 65 - 69 would give a reasonably good fit to the deaths registered in england and wales in 194 7 . 
a shortening of the latent period in the towns where the irritant was most intense and a lengthening of it in those towns where it was least intense would then result in the ratio between the respective death rates diminishing with advancing age after about 40 , as in table iv . 
the observed facts appear to be consistent with such an explanation , but a careful study of the mathematics of the assumptions outlined above is needed before definite conclusions can be reached . 
 the death rates from cancer of the stomach in the 83 county boroughs of england and wales in the period 1921 - 39 show great differences , which cannot be explained either by chance variations , or by differing accuracy of certification of the cause of death . 
standardized mortality tends to be greater in the northern towns , in towns with a low proportion of people of advanced age and in towns with a high proportion of men in unskilled and partly skilled occupations . 
 cancer of the stomach death rates of men were unrelated with those for peptic ulcer or other digestive diseases ; but amongst women there was a small negative correlation with peptic ulcer and a positive correlation with other digestive diseases . 
the present situation has been briefly restated by stocks ( 1953 ) at cardiff . there have been many endeavours to establish a racial factor to account for the known variations in cancer incidence . although they have been invariably inconclusive , as might be expected when consideration is given to the pronounced differences within individual countries , these surveys have shown that where racial types have migrated to other countries , e.g. , negroes to america , they appear to take over the incidence of malignant disease of the natural inhabitants among whom they have come to live . 
1. goitre distribution in holland ( amsterdam university )  . year , three further districts have been added to the list in the northern province of holland ( polak , 1954 ; personal communication )  . the lower incidence of goitre towards the belgian frontier is apparent and almost certainly significant . ( 2 ) united kingdom . variations of goitre and cancer within the united kingdom are striking . 
a recent survey ( stocks , 1950 ) of the incidence of carcinoma of the stomach in 83 county boroughs over a period of 18 years showed notable differences " which cannot be explained by chance variation or by differing accuracy of certification of cause of death "  . these variations were shown to correspond to variations in the hardness of the water supply : those with a moderate hardness tended to have 396 j . 
survey of goitre ( murray et this would be in keeping with the al . , 1948 ) to have a high goitre incidence . known clinical experience with regard to malignant disease in that county . comparing these two maps a striking correlation is at once apparent . outstanding are the heavy incidences of goitre and cancer in mid - wales , westmoreland fig . 
spencer and the fen district and neighbouring counties , and by contrast the light incidence in yorkshire , lincolnshire , herefordshire and pembrokeshire . gradations of correspondence on both maps are evident in comparing norfolk , suffolk and essex ; kent and sussex ; cornwall and devon ; glamorgan and carmarthen . a higher death rate from cancer was shown to exist in two swedish counties , kopparberg and gefieborg , than was found in the total rural areas of sweden ( stocks , 1925 )  . those two counties , as shown by examination of schoolchildren , recruits for the army and candidates for confirmation , were found to have a higher incidence of goitre as compared with the rest of the country . similarly , known goitrous counties in norway were compared by stocks ( 1924 ) with counties showing little goitre , and it was found that the goitrous counties showed a cancer rate for all organs of 113 - 7 as compared with 94.4 for the niiongoitrous counties . in iceland , the thyroid has been shown to contain one of the highest conlcentrations of iodine , and endemic goitre is non - existent ( rundle , 1951 )  . thyroids there weigh on an average 14 g . 
and carcinoma of the stomnach and oesophagus , when considering separate states . ( 10 ) australia and new zealand . australia is considerably more industrialised than new zealand and has many furthermore , rodent ulcer is large cities as compared with the latter country . infinitely more common in australia , where goitre does not obtrude as a major health problem , though there are certain areas where there are definite , if small , districts where goitre is found ( kelly , 1946 )  . 
the more rural and agricultural population of new zealand has here goitre is a major health problem and its a death rate from cancer of 14 - 56 . incidence in europeans , maoris and animals alike has been closely studied for years . 
as metabolic rate is in general a rough indication of thyroid activity , there would be appear to be some relationship between malignant disease and thyroid thus , the lowered metabolic rate often seen in diabetes mellitus dysfunction . ( joslin , 1946 ) may be considered with the increased liability of diabetics to develop carcinoma in any site or organ as compared with non - diabetics ( joslin , 1946 )  . in the same way , the lowered metabolic rate commonly found in patients with all types of peptic ulcers ( kolmer , 1949 ) may be considered with the incidence of carcinoma of the stomach - still one of the commonest neoplasms of man . ( 2 ) it has long been observed that puberty and pregnancy are periods when goitres may appear ( marine and lenhart , 1909 ; marine , 1935 ) , and may disappear when the period of excessive demand ceases or when iodine is given . these are also the periods when melanomata tend to increase in size and may , not infrequently , become malignant . 
at the beginning of this year rwas admitted to this hospital on account of malignant melanoma with spread to glands in the course of her third pregnancy . in her two previous pregnancies she also developed malignant melanoma on each occasion and was in this hospital in consequence . she has a moderate enlargement of the thyroid of the smooth " colloid " type seen commonly in pregnancy . 
the end of pregnancy is also the period when chorionic carcinoma and lactation carcinoma of the breast occur - perhaps the most rapidly growing class of cancer known . ( 3 ) administration of thyroid has been found to improve the action of oestrogens in the treatment of carcinoma of the prostate , permnitting the effective use of smaller doses of oestrogen and delaying the onset of insensibility to oestrogen ( winsbury white , 1948 )  . in support of this clinical experience a paper in endocrinological research is quoted ( chu and you , 1945 ) , but the final conclusions of these workers was that the simultaneous administration of oestrogen and thyroid was the same as that obtained by thyroid feeding alone . ( 4 ) reduction of keloid formation can often be brought about by administration of thyroid . 
the age for the start of the decline in iodine content of the thyroid coincides in general with the age at which malignant disease in mnan becomes a prominent feature . ( 7 ) in the second week of january of this year there were at least three patients in this hospital at the same time with gross goitre and cancer . m - - , carcinoma of breast and a large colloid goitre visible seven or eight beds away down the ward . e - , lymphosarcoma and a thyroid that weighed 80 g . 
the nodular goitre caused some difficulty ing involvement with growth . during resection of glands of neck . since january other patients have been seen in the wards of the hospital with coexistent carcinoma and goitre . it is relevant to note that the area from which this hospital draws its material , gloucester , somerset and cornwall , is not one in which goitre is frequent . ( 8 ) the association of goitre and malignant disease in the post - mortem room was strikingly illustrated by analysis of 1000 post mortems at the middlesex hospital ( stocks , 1924 ) , when anomalies of the thyroid were found in 13.3 per cent of males and 21.2 per cent of females of 500 persons dying of cancer ; whereas only 2 - 0 per cent of males and 6.5 per cent of females dying of non - cancerous conditions showed anomalies of the thyroid . professor barlow excluded from these anomalies secondary invasion of the thyroid by cancer , and the anomalies most frequently found were simple parenchymatous enlargement and adenomatosis , while calcified nodules , cystic changes , atrophy and fibrosis were frequent . 
of dba ( bather , 1952 )  . ( 3 ) rats bearing walker rat carcinoma 256 were treated with natural thyroof these 27 per cent showed complete remission and 12 per cent " favourxine . able " histological response , 68 per cent . 
showing no response at all . another group treated with synthetic hormone gave only 2 per cent of remissions and no response in 98 per cent of animals . 158 animals were involved ( herbut , kraemer , and jacksen , 1950 )  . regression of rat tumours may be induced by thyroxine the natural comment . hormone being superior to the synthetic . ( 4 ) feeding butter yellow ( p - dimethylaminobenzene ) to rats produced malignant neoplasms of the liver . 
the recent work of moon , simpson , li and evans ( 1950a , 1950b , 1952a , 1952b ) has convincingly confirmed the conclusions of earlier workers twenty years ago ( ball and samuels , 1932 ; bischoff , maxwell and ullmann , 1934 ) , that whereas extracts of the anterior pituitary cause tumours to arise in a variety of sites in laboratory 408 j . 
spencer iodine availability , traced by goitre incidence , appears to be one of such factors . closer scrutiny of some of these countries corroborates these conclusions . clinical findings and a review of some of the experimental work available lend further emphasis to these observations . the apparent relationship of thyroid insufficiency and the liability to develop cancer is discussed in connection with such other hormonal influences over cancer as are already known , particularly in respect of the pituitary . lines of investigation and clinical trials have been started , but results of any value cannot be expected for several years . a non - specific organ immunity or susceptibility seems to be the simplest explanation of the facts presented , and the possibilities , preventive and perhaps therapeutic , that are opened up by this line of research are briefly discussed . i am indebted to polak of amsterdam for fig . 
allsopp. from guy 's hospital medical school , london , s.e.1. received for publication march 5 , 1951 . in earlier papers ( allsopp and szigeti , 1946 ) an account was given of some of the properties of water - soluble substances which are produced from 3 : 4 - benzpyrene under the influence of monochromatic radiation of wavelength 2537a . aqueous ( bicarbonate ) extracts from the irradiated benzpyrene were found to be carcinogenic when painted on the skins of mice ( allsopp , 1946 )  . these biological tests , however , were very prolonged , four or five paintings weekly for some in an attempt twenty - six weeks being required before growths were obtained . to reduce this " latent period " experiments have been made in which croton oil was used as a co - carcinogen . observations on the effects of croton oil on the mice used in these experiments , when compared with those of p . 
of 0 - 5 per cent croton oil in acetone ( experiment la ) at first caused little superficial change . slight ulceration , as evidenced by patchy encrustation , was visible on the third day , after which epilation began . this was complete by about the tenth day . 
so soon as the encrustation sloughed hair began to grow again , and by the fourteenth day the animals appeared normal . day to day observations are set out in table ii . painting with 0 - 5 per cent croton oil at weekly intervals ( experiment lb ) caused a similar sequence of macroscopic changes , but restoration of hair growth was delayed until the third week , after which the epilation cycle repeated itself 276 c . 
no growths resulted , and histological examination of the painted skins revealed nothing more than a slight hyperplasia on any animal . co - carcinogenic effect of croton oil with 3 : 4 - benzpyrene . ( table i , experiment 3 . ) equal volumes ( 0 ' 1 ml . ) of 0 - 05 per cent benzpyrene in acetone and of 0.5 per cent croton oil in acetone were applied alternately at 3to 4 - day intervals , each animal thus receiving each agent once weekly . 
control animals were painted at the same times with benzpyrene , but with acetone instead of croton oil solution . papillomata were first seen on the experimental animals after 5 weeks ; all the survivors had malignant or " pre - cancerous " lesions by the fourteenth week , a precancerous lesion in this context being one exhibiting irregular epilation , hyperkeratosis , abnormal regeneration of hair follicles , ill - defined epidermal projections , a large increase in the number of mitotic cells , numerous abnormal mitotic figures , and leucocytic infiltration of the dermis ( allsopp , 1946 )  . 
when the experiment was discontinued in the twentieth week , 4 out of 8 surviving control animals had cancerous or pre - cancerous lesions ; the remainder showed marked hyperplasia only . 
the experiments described above , however , suggest that its action is more complicated than this simple description migth indicate . despite a marked difference in the response to croton oil of the mice now used when compared with that of strains used by other workers , berenblum 's findings ( berenblum , 1944 ) have been largely confirmed when 3 : 4 - benzpyrene was the carcinogen ; but when the hydrocarbon was replaced by the water - soluble substances which are obtained from it by the action of ultraviolet light croton oil appeared to exert a different effect since , while papillomata appeared on the mice at a very much earlier stage than they did with the carcinogenic solutions alone , a proportion of these papillomata did not develop into epitheliomata , whereas 278 c . 
the distinction in behaviour , however , was not entirely clear - cut , since the papillomata on 2 out of 9 animals did persist , growing very slowly , until they became malignant . the earlier experiments with the water - soluble substances ( allsopp , 1946 ) showed that with them the process of carcinogenesis was slow , but that it passed through the usual 3 phases of hyperplasia , papillomata , and finally carcinomata . the last stage required 6 to 10 weeks . 
the present experiments suggest that croton oil accelerates the transition from hyperplasia to papillomata - the first papilloma appeared after 13 instead of 26 weeks - but not the transition from papillomata to epitheliomata , which again took about 9 weeks . indeed it may even delay this change , or - in those cases where the papillomata were sloughedin contrast to this , benzpyrene itself appears to act rather more prevent it . quickly ; epitheliomata had developed in the animals recorded in experiment 3b of fig . 
gorer , of guy 's hospital medical school , and to m . salaman , of the london hospital , for comparing with mine the results of their experiments on the effects of croton oil on the skin of mice . 
 data have been published which indicate that the average latent period for all methylcholanthrene - induced fibrosarcomas ( strong , 1948 ) and the survival time ( strong , 1950 ) of mice developing such tumours are both influenced by litter seriation . 
the latent period ( time between the subcutaneous injection of the carcinogen and the initiation or the initial growth of the ensuing fibrosarcoma ) was variouslv affected in the different strains bv the litter to which the mouse in mice of some strains ( prunt and f : of c67 x brs ) the latent period belonged . 
 ( strong , 1948 ) for the appearance of fibrosarcomas decreased in the successirn litters of the same pair of mice , while in other strains susceptibility to fibro sarcomas was relatively constant . 
the sunival time ( strong , 1950 ) of mice growing a chemically - induced fibrosarcoma ( time between the initial growth of the malig nancy and the death of the individual ) is also affected by litter seriation . 
 ' \\nen a mouse developed a fibrosarcoma in less than 100 days following the subcutaneous injection of methylcholanthrene it sunived an average of 52 days with the progressive growth of the tumour ifit belonged to a first litter . 
in the succeeding litters mice of the same age and latent i : eriod survived longer and longer with growing fibrosarcomas until , if they belonged to an eighth litter , they lived on an average of 130 days . 
these genes were derived from mice of the ancestral stocks jk and n which were used in the origin of the : xho stra the first three generations ( cba... " x jk ) were used for breeding purposes only . 
at the time of the separation of prunt from pbr descent , the average latent period for the appearance of methylcholanthrene - induced fibrosarcomas of the direct in the f 20 generation of the experimental maternal ancestry was 3695 days . 
these two untreated descents , prunt and 2prunt , should possess genetic similarity , and any biological differences that they have may be due either to divergent segregation from a residuum of genetic heterozygosity ( probably very small after 17 generations of brother - to - sistier matings ) or to new biological variability which has appeared in one or both untreated deseents following their separation from a common ancestry . 
the mice were fed a standard diet of nurishmix pellets ( pratt food company ) and water ad libitu a supplement of mixed grains ( oats , wheat and sunflower seeds ) and calf meal pellets were given to the mice once a week . 
the mice were examined periodically for tumoun ; , and the latent period taken to be the time at which a firm nodule at the site of the injection of the carcinogen began to increase progressively in si mice which developed tumours at sites other than the one at which the carcinogen had been injected were tabulated separately . 
 table i gives the percentage incidence of tumours in mice which developed in less than 100 days ( column e ) , together with the data obtained on all tumours at the site of injection of the carcinogen irrespective of latent period ( column d )  . 
 data on the total number of mice injected with methylcholanthrene ( column a ) , the number of mice which died without developing any tumour ( column b ) , and the total number of mice showing tumours irrespective of latent period and site are also given ( column c )  . 
since the two separate descents disclose similar genetic origin and show similar trends by which the females are consistently more susceptible to fibrosarcomas than the males , the data for both series may be added together . 
however , the present analysis of trends of susceptibility in s1icoessi.e litters discloses differences , and therefore the two strains , the prunt and the 2prunt , should be kept distinct . 
thus 27 2 pe : r cent of the females developed fi.brosa : rcomas within less than 100 days of latent period , whereas only 92 pe : r cent of the males developed similar tumou : rs during the same period , a difference of 180 pe : r cent in tumour susceptibility  . 
the trend for the percentage incidence of tumours developing in less than 100 days among females of successive litters was found to be y = 85 + 5 lz , with a standard deviation of the slope of 0 - 741 . 
comparison of this value with a no - trend or 0 - slope value by t test reveals that the observed trend is statistically significant ( since p = < 001 )  . 
 similarly the trend for the percentage incidence of tum.ours developing in less than 100 days among males of successive litters was found to be y = 132 - 12x , with a standard deviation of the slope c , f 0968 . 
 the analysis of the data thus discloses that there is an increasing sex differential in relation to chemically induced : fi.brosarcomas in successive litters in mice of the prunt descent . 
the difference between the mice of the two descents must , therefore , be associated with a mechanism which in the 2prunt descent changes in litter seriation at least in some strains of mice . 
 the maximal sexual differential is found in mice of the second litters ( 302 per cent ) , and this sex differential fluctuates in the succeeding litters and thus shows no significant trend . 
however , the data of the 2prunt descent are complicated by a high value for females of the second litter ( 382 per cent ) and a high value for males of the sixth litter ( 143 per cent )  . 
in one strain ( the chi ) males were more susceptible to chemically induced fibrosarcomas than were the females , whereas in the 15th inbred strain ( the cul ) the females were more susceptible to tumours than were the males . 
 the mechanism involved in the development of this new sexual differential in relation to chemically - induced fibrosarcomas in mice of the prunt descent gives a slight sex difference in mice belonging to the early litters of a breeding female , and apparently gradually increases in the succeeding litters . 
h the sex pattern of an individual is the reflection of the genetic constitution of the individua1 , then it is not clear whether mice of the early litters or mice of the later litters are to be considered the pattern for the species . 
but sex physiology is also under the influence of several hormones , and the sex pattern can be influenced significantly when a hormone is administered at an early age , preferably before birth . 
 the present investigation with methylcholanthrene has disclosed that several aspects of malignancy ( the average latent period , the survival time and the per centage susceptibility of tumours in mice of latent periods of less than 100 days ) are influenced by litter seriation . 
do hormones fluctuate in the female body with advancing litter frequency , pass the placental barrier and influence the subsequent physiology of the offspring at least in relation to malignancy and perhaps to other characteristics as well ? or are we to conclude that maturation phenomena in cytoplasm ( perhaps the mito chondria or other constituents ) are responsible for this transmission from mother to offspring which apparently is not through the genes ? perhaps another biological reason may eventually be found for the data at hand . 
these mice belonged to two separate descents derived from a common genetic orig in one descent , the prunt , there was an increasing sexual differential in relation to chemically - induced fibrosarcoma.s in the succeed320 l . 
 evidence offered by calcutt ( 1949 ) showed that 3 : 4 - benzpyrene is effective in inducing the oxidation of the - sh groups of a variety of compounds , the benzpyrene itself also undergoing oxidation during this process . 
on the basis of physical properties and fluorescence spectra it was suggested that the benzpyrene derivatives obtained in this fashion were comparable to those obtained as a result of the metabolism of the hydrocarbon by mice . 
this suggestion is important in view of crabtree 's ( 1947 ) conclusions as to the involvement of - sh groups in the carcinogenic process , and also in relation to powell and calcutt 's ( 1949 ) conclusion that the availability of sulphydryl influences the metabolism of benzpyrene . 
 studies by weigert and mottram ( 1946a , 1946b ) showed that the initial step in the metabolism of benzpyrene is conversion to either 8 : 9 - dihydro 8 : 0r1 - 9.0h benzpyrene ( bpx1 ) or 8 : 9 - dihydro 8 : 0r1 - 90r2 benzpyrene ( bpx2 ) , r 1 and r 2 being unidentified radicals . 
at the same time it was shown that these compounds were convertible by simple chemical methods , which have their counterpart in the animal body , to the final excretion products - 8.0h benzpyrene and the 5 : 8 quinone . 
 it was suggested by quick ( 1937 ) that the primary step in the metabolic oxidation of hydrocarbons is a union of cysteine with the unsubstituted aromatic ring , replacement of the mercapturic acid by a hydroxyl group occurring later . 
 there is no direct evidence for this view , but the recognized involvement between carcinogenesis and sulphur metabolism ( crabtree , 1947 ; calcutt , 1949 ) is in its favour . 
it is , however , severely criticized by boyland and weigert ( 1947 ) , who point out that phenylcysteine is excreted as phenylmercapturic acid - - - evidence which suggests that the linkage between cysteine and an aromatic compound is not easily broken in the body . 
it is apparent that such a scheme could apply equally well in the case of the chemically related benzpyrene , bpx1 or bpx2 arising from the substitution of the hydrogen of one or other of the hydroxyl groups of the primarily formed dialcohol . 
an alternative possibility in line with the perhydroxylation view is feasible since autoxidizing thiols are known to give rise to hydrogen peroxide ( schober ! , 1932 ; holtz and triem , 1937 ; schales , 1938 )  . 
 if a perhydroxylation process is the initial step in both the in vivo and in vitro oxidation of benzpyrene it appears that it should be possible - under suitable conditions - to oxidize the hydrocarbon directly with hydrogen peroxide . 
 the addition of 6 per cent hydrogen peroxide to a colloidal suspension of benzpyrene in distilled water had no effect at room temperature even when the two compounds were maintained together for long periods . 
since hydrogen peroxide contains acid as a stabi lizing agent , any derivative of the bpx1 type formed in the reaction would be expected to break down to the phenol and thence to the quinone - a sequence of events which superficially would resemble those found . 
 as an attempt to counteract any influence due to the acid the experiment was repeated using the benzpyrene colloid suspended in a clark and lubbs buffer solution at a ph of 75 . 
this time the hydrogen peroxide was added tilowly ; whilst at intervals the ph was checked , and when necessary was restored to 75 by the further addition of 02m . 
examination of the fluorescent spectra of the solution derived from the three portions gave results as below : surface : - two diffuse maxima at 420 and 440 able from fluorescence spectrum of bpx1 derived from mice . 
the likelihood of it actually being 8.oh benzpyrene is enhanced by the fact that after transfer to petroleum ether and standing for a few days it lost its blue fluorescence and achieved a barely perceptible yellowish tinge , behaviour which would be in keeping with the known autoxidation of 8.oh benzpyrene to benzpyrene 5 : 8 quinone . 
the passage of a weak solution of an authentic sample of 3 : 4 - benzpyrene 5 : 8 - quinone through the same column resulted in concentration over the previous zone , and , although the zone slowly passed down the column , no further elution or variation in solvent allowed any separation of the two zones . 
the similarity of fluorescence spectra , physical pro perties and behaviour suggests then that the material separated from the reaction mixture is similar to , even if not identical with , the bpx1 from mice and the bpx1 - like material formed in the presence of autoxidizing thiols . 
 further examination of the substances extracted from the other two portions of the original chromatograph column produced little of interest other than that the material was water - soluble in both cases . 
attempts to utilize the benzpyrene in solution in organic solvents have so far failed , the only results being the formation of small amounts of apparent 8.oh benzpyrene and quantities of various unidenti fiable products . 
furthermore , the evidence suggests that the primary reaction product is a diol closely resembling that found as the initial product of benzpyrene metabolis at the same time this primary product shows a remarkable resemblance to that found as the result of oxidation of benzpyrene in the presence of autoxidizing thiols . 
 in view of the known forma tion of hydrogen peroxide during the autoxidation of - sh groups , it seems prob able that the primary mechanism of oxidation in both cases consists of the addition of hydrogen peroxide to the hydrocarbon . 
equally , since the formation of peroxide is a phenomenon known to occur during biological oxidations ( oppen heimer and stern , 1939 ) , it seems that such a mechanism could account for the initial steps of the in vivo oxidation of benzpyrene . 
 the oxidation of 3 : 4 - benzpyrene with hydrogen peroxide and the isolation of a product similar to the benzpyrene oxidation products obtained during metabolism and during oxidation in the presence of autoxidizing thiols is de scribed . 
the frankly keratinizing members of our series we have taken as a standard with which to compare the behaviour of our remaining histological types . the morphological features of the more differentiated epitheliomata have been so completely evaluated that any further discussion would be superfluous . 
the primary lesion grows slowly and tends to be clinically latent for a considerable period of time , it appears as a especially if it is situated in a region such as the nasopharynx . smooth or finely granular , firm , globular tumour , at first a mere nodule , but later attaining considerable dimensions . infiltrative spread and superficial ulceration occur fairly late in the evolution of the growth . cervical lymph glandular metastases appear at an early date , while the final phase is frequently ushered in by distant visceral extension , osseous deposits being rather characteristic ( kienbock and selka , 1935 ; ch ' in and szutu , 1940 )  . 
the histological picture may be syncytia of large , palely staining cells appear as sheets , irregular quite typical . clumps , or columns , in a lymphocytic stroma of varying density . 
ewing was doubtful of the specificity of schmincke 's description , and found its distinction from other types of undifferentiated pharyngeal growth difficult or impossible . the term " transitional cell carcinoma " was first employed by quick and cutler ( 1927 ) to describe a group of highly radiosensitive buccopharyngeal tumours of uncertain histogenesis which lacked the classical features of epithelioma , but presented transitional epithelial characters . ewing 's writings ( 1929 , 1940 ) have done much to clarify the morphological features of this growth . the most frequently encountered sites are the tonsil , base of tongue , nasopharynx , laryngopharynx , nasal cavity , and accessory nasal sinuses . quick and cutler described the primary lesion as possessing " a finely granular , velvety surface , e . 
fairburn this description is , however , far from being specific . which looks like an erosion of the mucous membrane rather than a frank ulceragives the impression of having originated in the tion . 
the lesion deeper structures and adhered to and eroded the mucous membrane from the clinical beneath . " course resembles that of lympho - epithelioma - a small and often occult primary histologically , transitional focus , and early cervical lymph glandular metastasis . cell cancer is typified by the presence of broad , clearly demarcated , epithelial the cells are cylindrical , polygonal or spindlecolumns and alveolar formations . shaped , with a rather hazy cytoplasmic membrane . 
the oval or fusiform nucleus is more chromatic than that of lympho - epithelioma , while its nucleolus is less frequently the marginal cells appear regimented as though forming distinct . degeneration and necrosis of the central zones of some of the a basal layer . lymphocytic infiltration of the stroma epithelial formations may be observed . may be present , but is never marked . there is considerable divergence of opinion regarding the justification of the classification of lympho - epithelioma and transitional cell carcinoma as specific entities . 
each has been traced to death or for a minimum period of five years following the first examination . purposes of classification we have created the following groups according to the site of the primary lesion : 3 . 
the cells are distributed the cell body is spheroidal or polygonal in solid masses or diffuse infiltrations . in form with palely staining cytoplasm , and a relatively large , oval , hyperchromatic nucleus which frequently shows bizarre , atypical features and mitotic figures . these classifications have presented certain difficulties : 1 . 
compared with the figure for the frankly keratinizing group ( 61.5 years ) , the former two differences are statistically significant , while the latter is not . there is no significant difference between the mean ages of - our cases when distributed according to the site of the primary growth . 
fairburn we have adopted ebenius ' clinical criteria of metastasis . the frankly keratinizing cancers possess a statistically significant lower incidence of metastasis ( 36 per cent ) than the remainder of their fellows , with the exception of the undifferentiated group which only metastasized in 22 per cent of cases . this table also illustrates the influence of glandular metastasis upon the likelihood of death with active growth . 
frank , lev and blahd ( 1941 ) , in their study of transitional cell growths , report a 44 per cent incidence of metastasis . 52 per cent of our cases possessed evidence of glandular extension on first examination . inspection of our data discloses the relative insignificance of tumour histology as a prognostic factor in cases of cancer of the lympho - epithelial sites . 
maccarty ( 1922 ) and plaut ( 1927 ) have emphasized its limitations , stressing the far greater importance , in most instances , of clinical features , such as the age and general condition of the patient , the duration , location , and gross anatomy of the growth , and the presence , or absence , of metastasis . 
the enormous preponderance of the site factor over that of histology is borne out by this study . thus , frankly keratinizing neoplasms of the lip carry a relatively good prognosis , but when arising in a lympho - epithelial region their significance is as sinister as that of their ill - differentiated fellows . 
the presence of lymph - node metastasis on first examination is , in our experience , a factor of far greater prognostic value than tumour histology , although very appreciably influenced by the site of the parent growth and its accessibility to treatment . 
to take a specific example , metastasis in a case of lip cancer markedly decreases the likelihood of cure , whereas when a lympho - epithelial region is involved , death with active malignancy is likely to occur whether the cervical nodes are involved or not . the chance of invasion of the cervical lymph glands appears to be largely independent of the histological grouping , the site of origin of the tumour being of infinitely greater significance . it has been widely assumed that the main factor in dissemination is the inherent growth capacity of the neoplasbut this is not the only influence which has to be considered . 
 * from the department of experimental pathology and cancer research , school of medicine , leeds , 2 . received for publication august 11 , 1951 . ' thf , need for devising a technique for testing the carcinogenic properties of chemical compounds by direct application to the bladder epithelium has been felt for some time . 
yamazaki and sato ( 1937 ) described a method of introduction of oily solutions of chemicals into the rabbit bladder by catheterization . interpretation of the true nature of the one acceptable tumour described by these authors after the introduction of o - aminoazotoluol is complicated by the presence in an extensive series of of lipoid in phagocytes in the subepithehal tissues . experiments , hughes ( 1949 ) , by means of epithelial grafts wrapped around 20methylcholanthrene crystals , obtained 14 transplantable carcinomas from 120 attempts . 
by this method an even distribution of the carcinogen was difficult to obtain , and so considerable variation in concentration may have occurred . under ether anaesthesia the bladder was exposed by a small incision through the skin and abdominal wall about i cabove the urethral opening . 
the bladder was drawn out of the abdomen and supported on a small pad of gauze ; an incision was then made through the dome of the bladder and the edges held apart by small metal retractors . 
the suture passed through all the layers of the bladder wall , and the edges were drawn together so that the two epithelial surfaces were bound closely to one another ; thus a continuous epithelial layer only and no muscle nor connective tissue was exposed to the direct action of the carcinogen in the pellet . 
the abdominal wall and skin were closed separately by sutures of cotton or thick silk . the operative mortality was negligible , but a number ' of animals died within a few weeks of the operation due to the pellets blocking the urethra . 
the latter concentration had been found previously to be effective in inducing subcutaneou 's tumours , both sarcomas and breast adenocarcinomas ( bonser , personal communication )  . in the present experiment pellets containing 2 per cent of the carcinogen induced bladder epithelial h erplasia but not tumours , whereas a pellet containing 30 per cent induced an infiltrating cancer . 
no doubt lower concentrations would be equally effective . this technique has the advantage that an ' substance so apphed to th ' e bladder is subject only to the action of the urine be ' fore coming in contact with the bladder epithelium ; thus metabohc changes in chemical structure subsequent to feeding or injection are obviated . 
a reasonably high i ' ncidence of tumours should be obtained with an active substance without incidental induction of sarcomas . it should now be possible to determine whether metabolites of bladder carcinogens such as 2 - naphthylamine are ' tho active agents in inducing bladder cancer . economy in time , animals and material can be effected , and this is important when investigating the carcinogenicity of small quantities of metabolites isolated from urine . 
payne. from the department of cancer research , mount vernon hospital and the radium institute , northwood , middx . received for publication may 2 , 1953 . in the course of their original work on the metabolism of 3 : 4 benzpyrene weigert and mottram ( 1946 ) noted that once the hydrocarbon had been introduced into a tissue it could only be extracted with difficulty . repeated and prolonged washing of the finely minced tissue was found necessary to remove the hydrocarbon and its metabolites . in view of this " binding " of the carcinogen and its derivatives within the cell an attempt has been made to fractionate mouse liver after treatment with 3 : 4 benzpyrene . 
the liver was chosen for detailed work as being easily handled , of adequate bulk , and as a site where metabolism of 3 : 4 benzpyrene is known to occur . 
the hydrocarbon was introduced as a colloidal susthis method was deliberately chosen as pension by intraperitoneal injection . offering the best chance of avoiding the presence of undissolved particles of hydrocarbon in the blood vessels as occurs after intravenous injection . all mice received one intraperitoneal injection of 1 c.c. 
the best known method for isolation of intact mitochondria is that devised by hogeboom , schneider and pallade this involves maceration of the tissue in 0 - 88 m sucrose solution , removal ( 1948 )  . of nuclei by low speed centrifugation and then isolation of the mitochondria by further differential centrifugation . 
payne as they caused agglutination of the mitochondria and their consequent sedimentation with the nuclear fraction . methods , such as the modified behrens technique used by mayer and gulick ( 1942 ) , where fractionation is done in organic solvents , were considered impracticable on the grounds of being liable to remove any bound benzpyrene attention was then turned to the standard methods for isofrom the tissues . these involve maceration in citric acid solutions lation of nuclear fractions . since it is generally accepted that mitochondria followed by centrifugation . however , it was found are destroyed by acids these did not appear hopeful . that using ice - cold 1 per cent citric acid as advocated by mirsky and pollister ( 1946 ) it was possible to remove a clean nuclear fraction , and then by further centrifugation at higher speed to obtain a mitochondrial fraction . 
the mitochondria obtained in this fashion were a bit swollen and distorted , but still stained readily in very dilute janus green b solutions . in bulk the fraction obtained in this fashion compared favourably with similar fractions obtained using sucrose this result was rendered less surprising , however , when it was found solutions . that the literature references to the solubility of mitochondria in acid only refer to acetic acid . on the basis of the above findings a technique using citric acid was developed . at selected intervals after injection the mice were killed by a blow on the head , this was examined under a u.v. 
lamp opened , and the entire liver removed . with wood 's glass filter , and any particles of benzpyrene detected - their fluorescence shows very distinctly against the background dull blue fluorescence of the liver - were washed off with normal saline . 
the 70 per cent acetone was selected , as previous experience had shown this to be the best solvent for benzpyrene in tissues . all fractions were spun down again to clear them , and fluorescence spectrograms were made according to the method devised by doniach , mottram and weigert ( 1943 )  . 
payne an acid mediuat ph values below about 7 - 1 both these compounds lose water to form 8 - 0 h benzpyrene . this latter has a rather indistinct spectrum , and may easily have been missed against the background fluoresence due to the tissue equally it may have been oxidised still further to the residues themselves . 5 - 8 quinone during the violent agitation associated with the maceration process . in any event it was considered that the experimental conditions employed were not suited to the quest for benzpyrene metabolites . the significance of the results obtained is difficult to assess . 
horning. from the chester beally research institute of the royal cancer hospital , london , s.w.3. received for publication december 12 , 1948 . recfnt experience has shown that many of the growth - inhibiting agents used in the palliative treatment of cancer are carcinogenic . 
they also cause specific damage to cell nuclei and chromosomes and are able to induce mutations . the association of these biological effects of ( 1 ) growth inhibition , ( 2 ) chromosome damage , ( 3 ) production of mutations and ( 4 ) induction of cancer suggests if the that they may have a common fimundamental biochemical mechanism . induction of cancer is indeed a somatic mutation , then cancer induction might be included as a special mutation . 
the fact that x - rays can produce cancer in man was published in 1902 ( frieben , 1902 ) , seven years after rontgen 's discovery muiiller ( 1928 ) found that x - rays are mutagenic , and later mather of x - rays . and stone ( 1933 ) and koller ( 1934 ) described the chromosome damage following irradiation . 
the idea that cancer arises as a somatic mutation was supported by the demonstration of an increased incidence of mutations occurring in mice this was shown with methylcholanthrene treated with chemical carcinogens . by strong ( 1945 ) and with 1 : 2 : 5 : 6 - dibenzanthracene by carr ( 1947 )  . carcinogenic hydrocarbons inhibit the growth of animals and the establishment and growth of transplanted tumours ( haddow , scott and scott , 1937 )  . 
body - weight of freshly made aqueous solutions of nitrogen the first group was given methyl di ( 2 - chloroethyl ) amine hydromustard . chloride ( hn2 ) in a concentration of 1 mg . 
the second group received the same dose of tri ( 2 - chloroethyl ) amine hydrochloride ( hn3 ) for 10 weeks , after which time only 4 mice remained alive and injections were stopped . post - mortem findings of the mice which died within a week of an injection usually showed congestion of the alimentary tract or lungs . 
with the doses used all the coloured mice showed the effect of no nervous symptoms were seen . greying of hair ( boyland et al . , 1948 ) similar to that produced by x - rays ( hance and murphy , 1926 ) or by subcutaneously implanted plutonium ( prosser , painter , lisco , brues , jacobson and swift , 1947 )  . 
hornin - g occur spontaneously , and the tumours were larger and more malignant than those generally encountered in untreated mice . the carcinogenic action of the nitrogen mustards is very slow , the earliest lung tumour and lymphosarcoma being seen at 284 and 347 days respectively . berenblum and shubik ( 1947 ) have shown that carcinogenesis can be divided into an initial stage in which cells are irreversibly changed into latent tumrnour cells , and a development stage which can be brought about by cocarcinogens such as croton oil . 
the incidence of tumours expressed as quantal response is probably dependent on the initiating action , but the rate of appearance of the tumours depends upon cocarcinogenic action . the present authors consider that the initial irreversible conversion to latent tumour cells is the change which is associated with chromosome damage and mutations . 
the nitrogen mustards are possibly active in initiating the carcinoin order to test this hypothesis genic change but poor in developing action . experiments are in hand in which mice are being treated with nitrogen mustard and croton oil . a possible explanation of the association between inhibition of growth and carcinogenic power is that the inhibition is due to interference with cell division in growing tissues . 
the drugs under discussion reduce the rate of growth by impeding mitosis . this interference with mitosis is likely to increase the chances of a somatic mutation from normal to malignant cells occurring . 
of 14 mice which survived more than 250 days , 10 had tumours including lung tumours ( 8 ) , lymphosarcomas ( 2 ) , a uterine fibromyoma and a spindle - celled sarcoma at site of injection . this investigation has been supported by grants to the royal cancer hospital from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the u.s. 
3. received for publication january 18 , 1949 . the investigation of carcinogenic substances which have been obtained from human tissues ( kleinenberg , neufach and shabad , 1940 ) and from other biological sources has been the subject of earlier publications from this institute ( hieger , 1940 , 1941 , 1946 , 1947 ) , reporting that : 1 . 
a fuller account will be found in appendix i . it is sufficient to note here that it is a slightly modified form of the ordinary death rate which would be calculated as 2 l ( x ) m ( x ) l ( z ) ' the reasons for introducing such a modification are twofold : firstly , it makes allowance for the fact that the specific death rate considered is underestimated owing to deaths from other causes , and secondly , it measures the rate at which animals are dying out from the cause under investigation at the moment , x , not the bulk death rate over a month . the latter property allows a continuous curve to be drawn through the calculated values whose ordinates measure the rate of mortality at any moment of life . 
the monthly death rates on the other hand are strictly discontinuous , being , as is shown in appendix i , functions of the area under the , ( x ) curve over the month in question . using the method of haldane given in appendix i , the values of , ( x ) for cancer were calculated for a number of strains . those for three strains whose life tables were given by murray and hoffman ( 1941 ) are graphed in fig . 
1. the three curves bear out the conclusion of maurray and hoffman that the dba mice were the most susceptible , then the bittner albinos , and finally the marsh time in months fig . 
spicer albinos - a result which is the reverse of that indicated by the percentages dying the method of approach used here indicates that the cause of the of tumour . discrepancy is the difference that exists between the non - tumour death rates of the three strains . for if , using the methods outlined below , we calculate the percentage of cancer deaths that would be expected if eachl strain had the same non - cancer death rate as the marsh albinos , we find the following values : bittnera marsh a  . 
~. corrected to marsh - a . 90 5 per cent 87 - 7 76 - 6 uncorrected . 67 7 per cent 73.7 76 - 6 the process of calculating the p ( x ) 's has involved some smoothing of the data , and in the graphs no attempt has been made to draw a smooth curve ; the points have merely been joined by straight lines . 
the irregularities in the curves are mostly due to random errors , though the flattening of the , u ( x ) curve for dba mice from the 12th to the 15th month is repeated in the curve for another group of the same strain , and is therefore probably due to some real interruption of the steady increase in the tumour mortality . a further series of , l ( x ) curves are given in fig . 
3. allowing for this by subjecting the a - ro mice to the a - fc non - cancer , ( x ) , it is found that they would have almost the same percentage of cancer deaths . the percentage of cancer expected in the a - ro mice at the a - fc death rate is in fact 86 , while the percentage found in the a - fc is 88 . it appears then that almost the whole 302 c . 
the most obvious method of comparison is to compare the numbers or proportion of cancer deaths in any strain with those of a strain having a standard non - tumour death rate . alternatively the number of deaths over a similar period of time may be calculated when all non - tumour mortality has been eliminated . both of these indices can be calculated using the , ( x ) values . the difficulty of this approach is to find a standard which is equally useful for all strains , since there are wide variations in life span and in o 15 iii 0 ' 30 0.25 0 20 - o * i 0.10 time in months fig . 
murray and hoffman ( 1941 ) have attempted to overcome the first difficulty by using a life span as a unit and expressing time in percentiles of this value . this method seems to be unsatisfactory in that the determination of the length of span is to some extent arbitrary . 
murray and hoffman use the time at which 1 per cent of animals are surviving , adding that it would be possible to use the 0.1 per cent point if larger numbers of animals were available . 
each of these two cut - off points would give a different system furthermore these authors make no direct allowance for differences of time units . in non - tumour mortality , though they discuss the merits of a number of arbitrary weighting factors for calculating averages of the monthly cancer death rates . to avoid the use of arbitrary systems of weights it seemed best to calculate indices of susceptibility after the non - tumour death rate has been eliminated . this was done using a method due to dublin and lotka ( 1920 , 1921 ) , which has also been discussed by karn ( 1933 ) and irwin ( 1935 )  . 
spicer quently pointed out that the estimates might be improved by using the method of maximum likelihood , which gives results having a smaller standard error . the full calculations are rather more laborious than in the case of dublin and lotka 's method . 
6. it will be seen that the process of summation has resulted in a considerable smoothing of the data , and though the original , u ( x ) curves are not all similar in form , the integrated curves approach more closely to this ideal which is essential if strict comparisons of tumour susceptibility are to be made . after some initial confusion the curves spread out from left to right in order of decreasing susceptibility . 
any horizontal line drawn across the figures will give , by its intersections with the curves , the times of equal proportional mortality . vertical lines will give the proportional mortality corresponding to equal times of life . 
they are : 25 6 for the cross with a dba mother , and 37 8 for the reciprocal . from a study of the , ( x ) graphs it is obvious that the differences in the form of the curves from strain to strain make strict comparisons of tumour susceptibility , of the same kind as are made in biological assay , impossible . future work will probably reveal some of the factors which determine the shape of the curves , but in the meantime it should be emphasized that susceptibility to mammary tumour is determined in a different way in each strain , though the similarity of the , u ( x ) curves of different groups of mice of the same pure line does enable more exact comparisons to be made in this case . 
haldane , who first suggested that the , t ( x ) curves could be used for the investigation of tumour susceptibility , and who provided me with the method of calculation given in appendix i . 
 ( - ) = log.e 2 = 0 693 gives the half life . ( 4 ) modified expectation of life . the number obtained by taking the reciprocal of the sum x log . 
 ( 1 / px ) for the whole table is of interest since it gives an estimate of the expectation of life . suppose the table extends over ages from o t so that the sum of probabilities is then we can twrite the reciprocal of this sum t1 log . 
 ( 1 / p ) = t , j ( x ) dx ' ( x ) 1 ( x ) dx if there is no cause of death but cancer . so that the reciprocal is a weighted mean of the [ ( x ) 's . multiplying this by t , the interval over which the table extends , gives an estimate of the expectation of life . this estimate is rather lower than that given by the correct method of calculation since the values of 1 ( x ) are weighted in favour of the low values at the higher ages where the , u ( x ) 's are large . it might be preferable to use this modified life expectation instead of the half - life as it takes into account all the data and can be given a standard error . 
 ( p ) and the variance of the sum is equal to the sum of the variances since the p 's are independent . if we call this sum 2 then the variance of the half life will be given by and since and the standard error of x is var . 
1. received for publication january 13 , 1948 . one of the implications underlying the work of huggins and hodges ( 1941 ) on the factors governing prostatic hypertrophy is that malignant prostatic cells are not fully , if at all , autonomous . that is , they are still controlled in some measure by the same factors that control normal prostatic cells . specifically , this is certainly true of their susceptibility to the influence of circulating androgens and oestrogens . carcinoma of the prostate is essentially a disease of old age . the possibility exists that the chief factor in deciding the individual 's susceptibility to this disease may be his androgenic state , that is , the level of circulating androgens in his blood , particularly during the later decades of life . the only practical method for ascertaining androgenic state is a determination of 17 - ketosteroids excreted in the urine of the subject . in the hands of many different workers ( barnett , henly , morris and warren , 1946 ) this method has revealed a very wide range of excretion of 17 - ketosteroids by normal men , at least in the lower age - groups . 
robinson the prostates of individuals who excrete at the higher or lower end of this scale will be subjected to grossly different amounts of androgenic stimulation . most of the available data on the excretion of 17 - ketosteroids is confined to results obtained in studies of men under the age of 30 - years . although there is a general impression that the excretion of these substances decreases with advancing age of the individual , there is a paucity of data on the range of excretion in the higher age - groups . the ideal method of study would be to make repeated determinations of the 17 - ketosteroid output in a large number of individuals over a period of m%ny years , until , in fact , the subjects did or did not develop prostatic cancer . 
the colorimetric measurements - were made on a hilger spekker photoelectric absorptiometer using a green ( ilford spectrum 604 ) and a violet ( ilford spectrum 601 ) light filter . 
1 clearly shows the distribution of excretion of 17 - ketosteroids with age . the output in childhood is low , rising rapidly at or about the age of puberty and reaching a maximum in middle age . 
2 , in which are plotted the as men between 30 and 40 . mean excretions for the third to the eighth decade , together with the upper and the ranges are computed lower limits of the ranges encountered at those ages . as the mean values + 2a . the fact that men continue to show comparatively wide individual variations in their outputs of 1 7 - ketosteroids and hence , probably , in the degree of androgenic stimulation to which their prostates are subjected , until very advanced age , must obviously be taken into account in any consideration of the aetiology of prostatic it will clearly be of importance to know whether known sufferers from cancer . this disease are characterized by excretions at the upper or lower ranges of their appropriate age - groups , or whether they are not significantly distinguishable a . 
jolles. from the radiotherapy department , general hospital , northampton . received for publication december 16 , 1948 . the focusing of attention on the malignant cell in the study of tumour tissue reactions to radiations and growth inhibitory substances has not brought us nearer the state of affairs where both practical and theoretical issues of oncology and treatment of tumours can be studied with a better understanding and fairer prospects of success . the importance of the stroma reaction to tumour and stromal reaction to radiation has been accepted for a long time , but only with generalizations on changes in " blood supply " and " tumour bed , " leaving the whole problem of connective tissue reaction in a hazy state . as regards tumour tissue reaction to radiation , much stress has been laid in the past on the changes following irradiation in the cells alone , but very little although recent attention has been paid to the intercellular tissue components . advances in cytology and genetics have enhanced the importance of the cellular nucleus , it must not be forgotten that evidence , both experimental and clinical , is available to show that the effect of ionizing radiations on cells alone " is not the whole story of the events leading to the destruction of proliferating tissues and that other factors come into play " ( muller , 1940 )  . the great importance of connective - tissue reactions to x - rays in radiotherapeutics has been raised by windeyer ( 1942 ) , ellis ( 1942 ) , windholz ( 1947 )  . 
the lesion is reproduced by means of a stent impression in a plaster cast , over which a tightly fitting stent or black - tray compound applicator is built in such a way as to be easily mounted over the part of the body , and fitting in such a way as not to allow even minimal shifts of the applicator , and so avoid the x - ray beam striking the alternate " opaque " squares of the lead chess which is recessed in the mould . the radiation has to be delivered at right angles with the x - ray tube head in order to avoid oblique penetration into areas applicator directed vertically . beneath the opaque squares the lead chess must be in direct touch with the tumour it is found in the course of treatment that owing to shrinkage of the surface . tumour the recess sleeve in the stent mould into which the " chess " is slipped has to be filed down from time to time during the course of treatment . the thickness of the lead , which is limited for practical considerations , permits 3 per cent of the radiation to pass through on to the protected areas . 
to that amount of radiation received by the not directly irradiated areas has to be added about 3 - 5 per cent of scatter radiation from the neighbouring exposed areas . this varies according to the size of the apertures , and decreases towards the centre of the " opaque ' , squares . 
the size of the squares has been chosen of not less than 1 cm . , so as to leave an adequate amount of tissue either almost completely non - irradiated or exposed for biopsy taking . sections are taken before treatment is commenced and then at varying intercuts are made into the exposed and protected sectors , and also one section vals . is made cutting across both the exposed and protected areas of tissue . accurate labelling of biopsy material must be insured , as no other way of recognizing the protected and exposed sectors on the histological slide is available . a working chart is found indispensable . prior to taking the biopsy the lead mask is applied and the exposed areas are mapped out by means of gentian violet paint . the biopsy material was fixed in sublimate - formol solution or sousa 's solution . following paraffin embedding , sections were cut at 7l and stained with ( 1 ) harris ' haematoxylin , eosin , ( 2 ) van gieson stain , ( 3 ) by gallego 's method , and ( 4 ) silver impregnation . the irradiation was taking place every day , 5 - 6 days per week . 
hard mass filling right breast , fixed to pectoralis and ulcerating skin in anterior axillary line over an area 8 x 5 cwith a sloughy crater and rolled - up edges . 
at this point " chess " technique abandoned and routine glancing technique reverted to . ( 4 ) section taken when tumour received apart from the 4000r with the chess technique 2500r on each glancing field in 14 days ; 10 treatments . ( 5 ) section taken at end of treatment ( 4000r to chess and 3500r on each glancing field in 5 weeks )  . she is remarkably when last seen , 15 . 
meredith. from the christie hospital and holt radiumt institute , manhester . received for publication december 12 , 1948 . ix a series of papers ( dale , 1940 ; dale , meredith and tweedie , 1943 ) it has been shown that the action of x - rays on aqueous solutions of biologically active compounds was indirect , i.e. 
further , it has been shown that in consequence of this indirect action , if two solutes are present , the second solute ( the protector ) reduces the radiation effect on the first one ( the indicator ) ( dale , 1942 ; 1943 ) , by sharing the intermediate product formed from water by the radiation . 
sionally. 197 3 67 0 364 - 0 102 - 6 . 41 - 0 used purgatives ; 1 - 7 x 34 or 63 to have used purgatives occasionary in a hke manner the " expected 34 or 6 - 1 to have taken purgatives often . f7 - 7 x purgative consumption was calculated separately for each age - group in each sex . 
the differences in the senna rates - while showing tlle same trendwere not so marked or consistent , and though the age - specific rates of beecham 's pffls ' usage were without exception higher amongst gastro - intestinal cancer patient 's , the individual differences were , on the whole , small . direct comparison between the gastro - intestinal cancer and non - gastrointestinal groups was carried out for each of the three purgatives , making appropriate adjustment as before for the differing age and sex structures of the two populations ( table vi )  . 
the comparisons relating to the use of senna and beecham 's pills show similar , but less marked , trends towards heavier usage by the gastro - intestinal cancer patients . 
the excess of senna in the gastrointestinal cancer group just reached the level of technical significance and while a similar picture was presented by the separate consideration of cancer of the large bowel ( x2 - 7.21 , n - 2 , p = 0 03 ) , - there was no significant difference between the experience of patients with cancer of the stomach and those suffering from a non - gastro - intestinal complaint . 
kerrich from the radiation therapy department , johannesburg general hospital , and the department of mathematics , u niversity of the witwatersrand . received for publication april 20 , 1951 . in a previous paper the writer ( cohen , 1949 ) proposed a biological dosage unit , the " roentgen equivalent clinical " ( rec ) based on an empirical formula d = e.a.tn.l - q , relating the physical dose in roentgens ( d ) to the biological dose in rec ( e ) , taking into account the relative biological efficiency of radiation of various qualities ( a ) , the over - all time in days ( t ) , and the field size in decimetres ( l )  . 
the physical and biological doses could be equated when the specific ion - density is minimal ( a = 1 ) , the treatment is completed in 1 day ( t = 1 ) , and the field diameter is 1 d ( l = 1 )  . 
cohen in diametercan the hypothesis of a " diffusible substance " ( grynkraut and sitkowski , 1936 ; jolles , 1950 ) , for diminishing the treated field by a given factor , or increasing the time interval by the same factor , would allow the same proportion of the " substance " to diffuse across the surface bounding the treated volume . 
the difference between the 220 kv and 180 kv ranges is statistically significant ( p 0 - 01 ) , but of minor importance clinically , so that for practical purposes the two high - voltage qualities may be grouped together taking a as 0 - 7 . 
2 illustrates the variation in biological efficacy with halfvalue layer , and shows the agreement between our estimates and similar data derived in a different manner by maccomb and quimby ( 1937 ) and by mackee and cipollaro ( 1940 )  . each point represents the median erythema dose ( a x 1000 ) estimated from table ii , the vertical lines delimit the 95 per cent confidence range , and the lettering refers to data by the authors quoted . in comparing these results with other published data , it is necessary to note inevitable differences in the definition of the erythema dose . 
from the method we have used the standard erythema dose is that which , delivered to a 10 cm . field in one sitting , produces a " moderate " erythema in 50 per cent of the treated cases . 
with the same dose , however , some slight reddening would be visible in considerably more than half ( probably 90 per cent ) of the treated cases . since this type of " barely perceptible reaction " is a convenient and objective end - point much favoured in erythema studies , there is obviously need for care in comparing such results . it is also necessary to distinguish the transient reddening ( fruiherythems ) appearing within 24 hours of the delivery of quite small doses ( helmke , 1949 ) from the main reaction ( haupterythems ) , which reaches its maximum about three weeks after treatment . for example , the threshold erythema dose ( ted ) is defined ( maccomb and quimby , 1937 ) as that quantity of radiation giving a faint reddening of the skin , visible in two to four weeks , in 80 per cent of treated cases . it would , therefore , differ little from our standard erythema ; hence the fair agreement between our results and the threshold erythema data in fig . 
the customary five - year - cure policy could not be applied since estimates of depth - doses from treatment records prior to 1945 are not sufficiently accurate it was decided instead to use , as a standard criterion , freedom for our purpose . from perceptible recrudescence for not less than three years . the records of 100 suitable cases treated between 1946 and 1948 , and followed with periodic examinations through 1950 , were abstracted and the data collected in table iii . the cases are arranged in order of increasing biological dosage ( rec )  . the dosage data shown are the true mimimum tumour doses , and differed , especially with superficial therapy , from the nominally given doses . in the case of very superficial tumours treated with lightly filtered radiation the significant point was taken to be 5 mbelow the edge of the treated field . with 2 ma1 filter this point receives about 85 per cent of the given dose ; and with the chaoul apparatus , only 67 per cent . with deeper growths treated at higher voltages , standard depth - dose tables were used to assess the tumour dose ; while with radium applicators and implants dosage was calculated on the paterson - parker system . since various qualities of radiation were used , it was necessary to correct the dosage by a factor ( rbe ) which , taking that for y - rays as unity , becomes 0.5 for superficial therapy , and0.7 for the 200 kv range ( tableii )  . in the case of deep - seated tumours treated with 200 kv radiation , the half - value layer ( and hence the rbe ) in the tissues differs from that of the incident beam on account of the increase in the average wave - length brought about by the compton recoil process . this effect is the more marked the harder the incident radiation . 
3 each 188 case site . face orbit neck node larynx back tongue pharynx neck nosoe alveolus neck face scalp larynx tongue , base pharynx orbit face temple post - cricoid  . 
0.5 , dose * ( r )  . 3200 2300 2250 3300 3150 2000 3800 3500 3000 1400 2000 3000 3150 3000 3300 4400 3600 5000 3750 2250 3300  . 
4 illustrates a method for determining the recovery exponent various values of n ranging from zero to 0.5 were ( n ) by a graphical solution . selected , and the resultant estimates of biological dose tabulated in a manner field diameter ( cm . ) therapeutic ratio skin tolerance dose 5000 median cancerocidal dose 4500 time days 1204 a% t% % - iuuut 9000 8000 - 7000 - 6000 - 5000 4000 - 3000 - 2000 1j4mi iolvv 40003500300025002000fig . 
a single line and volume factors . across the diagram gives all the relevant factors simultaneously . similar to table iii but regrouped accordingly . the cure rates so obtained were similarly charted in lognormal probability graphs , and the values of the standard deviation factor ( f ) corresponding to each value of n was determined . it is seen that f is a minimum as n approximates 0 - 25 . 
by means of the method of least squares , estimates of a and n for six different qualities of radiation were obtained , and shown to be in good agreement with previously established data . 
the uncertainty factor in dosage estimated on this basis ranged from 1.21 to 1 - 35 . a further 100 cases of epidermoid cancer were similarly analysed in order to determine the dependence of curability on the biological dose . 
the median lethal dose for this tumour ( 3000 rec ) and its uncertainty factor ( 1.3 ) were determined , and it was shown that , under optimal conditions of time and area , 95 per cent of tumours could be cured with a dose exceeding the median lethal dose by it has also been demonstrated that the prognosis is a mathematical 30 per cent . function of the therapeutic ratio . the author wishes to acknowledge the valuable advice given by j . 
kerrich. from the data in table iii cohen suggests that biological dose = dose / rbe x tn , or x = z / tn say , where xbiological dose , zdose / rbe , t = time in days . 
he goes on to show that if x is the exact dose necessary to effect a cure , then a reasonable assumption is that log x = log z n log t is normally distributed . writing x = log x , z = log z , t = log t this hypothesis becomes x = z nt is normally distributed with , say , mean oc and variance a2 . by a neat graphical method he proceeds to estimate ac , n and a . 
cohen the sizes of the estimated standard deviations show that none of the constants can claim to be very " well determined . " it must , however , be remembered that we are not dealing with a planned experiment , but that the author had to use the data that were to hand . 
as a suggestion to future workers in this field , more observations for small values of t ( say t 0 ) and large values of t ( say t - 1.5 ) would help greatly in fixing c and n more accurately . in more detail , the estimated covariance matrix is var . 
cohen free , will , in this paper , be designated as ffc , and the reciprocal factor - harbouring ( c3h x cba ) f1 as fhc . all parent strain and hybrid mice were housed in the same environment and maintained on a standard laboratory chow diet with tap water ad libituit was found expedient , in view of ' the temperamental breeding habits of both cba and cm females , to isolate routinely all pregnant mice until after the weaning of consequently , no f , bybrid was ever in contact with the father , which , the litters . as has recently been shown by peacock ( 1953 ) , reduces the probability of " infection " in the ffc with milk - factor from the cm male parent . the incidence of spontaneous mammary tumours in old factor - harbouring ( c3h x stock albino ) f , females , which were observed for over a year and inadvertently force - bred , was at least 70 per cent . 
no mammary tumours were noted in the corresponding , similarly treated , factor - free females , and it was considered that the presence of the milk - factor in the c3h niale parent exerted little or no influence on this group . 
the tumour , retracted from the body onto a wax backing , is fitted into the mouth of a 2 cdiameter open - end applicator , fsd = 25 cm . , and treated at 240 w . 
the mean - log of the volume in cubic millimeters of the fhc group is 2 - 12 ( 0 - 08 ) , while the mean - log - volume for the ffc group is 1 - 85 ( 0 - 08 ) , which is significantly smaller . while unequivocal comparisons between the c3h and hybrid groups could be made with confidence , it was considered possible that , as a result of the variations in growth rate within the hybrid hosts , smaller tumours might be more readily cured , and the ffc group consequently biased in favour of a higher curerate . 
2 , togeth ' er with comparative data previously determined for the parent this design is analogous to a six - point assay , in which both hnearity strain . and parallehsm of the regression hnes can be tested . 
the magnitude of the parameters and the significance of the inter - group differences were computed by finney 's ( i 952 ) methods . a third experiment was designed to determine , whether the increased radiosensitivity of the tuniour in f , hybrids was an inherent change in the tumour cel ' is per se , or a reflection of host - resistance . 
2. - probit diagram showing response of the cm carcinoma growing in various situations . ( a ) control series treated in homozygous cm mice in 8itu . ( d ) irradiated in 8itu in heterogeneous hybrid mice . ( f ) irradiated in factor - free ( ffc ) mice . 
the increased radiosensitivity of the tumour associated with genetic diversification in the host is evident . ( e ) irradiated in factor - harbouring ( fhc ) mice . 6000 7000 5000 cells growing in a relatively alien environment was suggested by barrett and deringer 's ( 1952 ) observation that a permanent adaptive change occurred in the oh mammary carcinoma following one - sub - passage through susceptible f , hybrids . since the object of this experiment was to demonstrate any inherent acquired radiosensitivity in the tumour , a smar homoplast ( first passa - ge from a oh mouse ) , growing slowly in an ffc host , which had attained a volume of only 30mm3 . 
the donor was also re - impladted with this tumour . takes " were 100 per cent in all groups . when each tumour had reached a standard size , about i cin its greatest diameter , it was irradiated in situ with a dose of 4200 r . 
the re - implanted tumour therefore , if the in the ffc donor was also irradiated at this dose , and cured . acquired radiosensitivity was a permanent adaptive change in the tumour cells capable of being carried over into the next transplant generation , it could be expected that the cure - rate of grafts originating from this tumgur at the dose givedwould be about 75 per cent in each genetiegyroup . 
2 , and the probit regression lines derived for the radiosensitivity of the tumour growing each reciprocal group are shown . in the genetically heterozygous environment of the ffc host , excluding the complicating influence of maternal factors , is shown by line f in fig . 
2. this line is virtually parallel to that previously obtained in the parent oh strain ( line a on the diagram ) , the coefficient of variation being 10 per cent . the median effective dose ( ld50 ) is found to be 3950 ( i 10 * ) r , compared to 5700 r previously reported in the oh . 
2. not only is the cure - rate , in the presence of the milk factor , considerably less than that of the factor - free mice , thougli still greater than that of the c3h parent , but the usual sharp response to increasing dosage has become much less sensitive , as evidenced by the considerably flatter slope of the regression line . this change test of the data reveals a is not due to fortuitous fluctuations in cure - rates , as a highly significant departure from parallelism with the other groups . 
the median , effective dose for the tumour growing in fhc mice appears to be 5100 ( + 400 * ) r with the unusually large coefficient of variation of 25 per cent . it must be assumed , therefore , that the maternal influence is not uniform and stochastically independent of other factors . 
was noted in the treatment of radiation - attenuated homoplasts growing in the parent strahi ( cohen and cohen , 1954 )  . at the ld50 level , the relative radiosensitivities , evidenced by the dosage ratio between the c3h and fhc groups is 1 - 13 ( + - 07 * ) , and that between the fhc and ffc groups is 1 - 29 ( - 08 * )  . 
the former ratio , compared with its standard eiror , indicates that the genetic effect per se , in spite of the complicating matemal influence , is probably significant ( p = 0 - 05 ) ; while the latter shows that the effect attributable to the milk factor alone withift the hybrid mice is highly significant ( p < 0 - 001 )  . 
the relative importance of these ratios , however , necessarily varies with the curative level t - ested , the maternal influence having the greater effect at doses above the median effective range . in order to eliminate any possible bias introduced by the greater average volume of the tumours in the fhc mice compared with those of the ffc group , a small number of animals bearing tumours of extreme size were discarded in the manner previously described , so as to equate the mean log - volumes of the two groups , and the probit analyses repeated on the remaining matched tumours . this correction , however , does not alter the magnitude of the parameters or affect materially the significance of the differences between them . further , comparison of the proportion of tumours cured within each class - interval of fig . 
i that within each genetic subgroup , the cured tumours tend to a smaller volume than the non - cures . these differences , however , are not signific ' ant , since the experiment was not designed to test the effect of tumour volume per se on radiosensitivity and contains insufficient data for this purpose . 
the question of the relative importance of genetic factors and of tumour size per se in determining radiosensitivity , is probably meaningless , since the smaller , more slowly - growing homoplast may itself be a manifestation of genetically - conditioned host - resistance ( eichwald , 1953 )  . 
cohen mal factors , therefore , materially affect the response of a tumour homoplast irradiated in situ . subsequent challenge with a second inoculum in those hybrids of both reciprocal groups , previously cured of the tumour , resulted in active growth in all it was also interesting to note , in the course of the experiment , that the cases . spontaneous mammary tumours in factor - harbouring f , females occurred regardless of whether the animal had previously been cured or not . third experiment table 11 shows the results of the third experiment , in which a " radiosensitive homoplast , growing in an ffc and later cured with 4200 r , was sub - passaged through mice of the three genetic categories and treated with the same dose . the cure - rates of these tumours in the ffc , fhc and parent c3h mice are respectesting the null - hypothesis that the radiosensitivity tively 67 , 35 and 0 per cent . of the sub - passaged homoplasts is the same as in the ffc hosts ( 76 per cent at 4200 r , table 1 ) , the probability of obtaining the results observed is shown in the last column of table ii . 
the susceptibility to tumour transplantation is a simple genetic - dominant , shown by the uniformly successful transfer of tlle inbred parent strain tumour to all f , hybrids . however , once such a graft is established , its rate of growth is no longer contingent on host genetics per se , but is dependent on the aternal extrachromosomal influence which , when present , exerts a significantl accelerating effect . likewise , a matemal influence , presumably the milk agent , is sufficient to induce spontaneous mammary tumours in f , hybrid females , the incidence approaching that in the inbred parent strain , in spite of genetic dilution . it has here been shown that the radiosensitivity of a tumour transplant , in this case the c3h mammary adencarcinoma , is dependent on both genetic and maternal ( extrachromosomal ) factors in the hybrid host . it appears , however , that the two factors are not necessarily independent . in the case of the factor - free f1 hybrid , a uniform and uncomphcated response is elicited which seems to be a - clear expression of immunogenetic differences between host and tumour . 
the differences between these groups are significant , although all three groups of mice were uniformly susceptible to the tumour and showed no overt manifestations of resistance . it appears , therefore , that the radiosensitivity of a tumour is a quantitative measure of subhminal host - resistance resulting from immunogenetic differences in the host - tumour relationship , including extrachromosomal factors . the mechanisni involved was further elucidated when a tumour growing in a factor - free f , hybrid , and known to be curable with 4200 r , was sub - passaged to mice of the three genetic groups . 
the homoplasts responded to treatment in the same manne ' r as the directly passaged parent strain tumour in the corresponding hosts , indicating that no inherent radiosensitisation of the tumour cells per se had occurred . all the facilities required for the maintenance of the animals used in this investigation were generously provided at the south african institute for medical 312 a . 
3 received for publication january 11 , 1951 . it has long been known that the rous sarcoma may be transmitted by dried tumour tissue and it has been concluded , therefore , that the tumour agent can survive under such conditions ( rous and murphy , 1914 ; rous , 1911 ; and hoffstadt and tripi , 1946 )  . 
the ampoules were then connected to a manifold and the ice sublimed in vacuo . knox 's ( 1939 ) apparatus and conditions were later used by dmochowski ( 1948 ) for the freeze - drying of rous v - irus suspensions produced by fractional centrifugation and other methods . 
dmochowski ( 1948 ) claimed that similar virus suspensions treated with a drop of fowl or rabbit serum suffered no loss of activity under the same conditions , but that addition of salts , such as nacl , kc1 or caci2 , had no such preservative action . 
by gentle shaking for 35 minutes . if the shaking was carried out in the absence of gas space , albeit with glass beads in the tube , inactivation was negligible . 
gave complete protection for t5 phage for 14 minutes . the duration of the protective effect was found to be a function of the gelatin concentration , since the gelatin itself protection could also be obtained with gum arabic or with is " denatured . " serum albumin although 100 - fold and 10 - fold the gelatin concentration were required . this work may well provide the theory behind the observation that viruses are more stable when diluted in serum or broth than when the dilutions are made equally one might expect that small viruses would be with salt or water . inactivated more rapidly than larger , and that the rate of inactivation would be proportional to temperature , since the forces responsible for bringing the particles to an interface will be thermal forces . such conditions as these have frequently been realized empirically . rivers and vvard ( 1935 ) sought to add a material to vaccinia virus suspension which would ( a ) act as a protective agent , ( b ) add bulk to the final product and ( c ) go back into solution with ease , carrying the virus with it . 
this suspension was clarified on the sharples centrifuge and the virus deposited from the supernatant on to a cellophane bowl lining sheet by deposition at high speed ( carr and harris , 1951 )  . this virus - containing deposit was then resuspended in a ' volume of medium ( concentration medium ) equal v / w to the original weight of tumour tissue . ( 2 ) comentration media . ( a ) buffer - trypsin , b - t . - mcilvaine 's ( 1921 ) phosphate - citric acid buffer ( plff 7 - 5 to 8 - 0 ) prepared from 0 - 2 m na2hp104and 0 - 1 m citric acid and diluted 1 : 19 with water ( buffer ) and a few mg . 
the mccartney bottles were accommodated in drihed compartments in the centrifuge head of the drying chamber of the machine . each bottle was inclined towards the axis of rotation , so that when the head was spinning the contents of each bottle formed a wedge . the virus suspensions were snap - frozen by evaporative cooling , and the purpose for spinning the bottle was 2 - fold . ( a ) frothing was prevented and ( b ) the wedge of frozen material presented a greatly increased surface area with a consequent increase in the rate of drying . 
the rate of drying was high throughout the drying cycle and no evidence was found to suggest that , as the layer of dried virus material increased in thickness , the rate of evaporation of vapour fen off and the underlying frozen mass melted ( bauer and pickels , 1940 )  . the drying cycle occupied 40 to 44 hours . 
the bottles , which were either uncapped , or lightly capped with two or three layers of sterile surgical gauze during the drying , were then screw - capped and sealed with tape and stored at 2 ' c . 
the media used , and here abbreviated , included : ( a ) buffered - 8aline , b - s . - ten per cent sahne adjusted to ph 7 - 2 with 0 - 2 m sodium phosphate . ( b ) buffer , ph 5 - o . - mcilvaine 's phosphate - citric acid , diluted 1 : 19 with water . ( e ) water - trypsin , w - t . - - solution containing a few mg . 
a similar result appears from table vii if the result of 29jr.49 is compared with that of 5.vii.49 , and from table viii , 15ar.49 being compared with 29.iii.49 ; although activation was not found in the experiments with egg albumin or egg white . freeze - drying in salt solutions ( table ii )  . the sharples deposits were resuspended throughout in , 0 - 005 m phosphate buffer , ph 7 - 2 , containing a few mg . 
50 , where lemco is compared with io per cent lemco as a medium for freeze - drying , there is a reduction in the titre with the weaker broth . freeze - drying in carbohydrate media ( table vii )  . the sharples deposits were resuspended in buffer - trypsin and " purified " in the usual way . 
or 0 - 125 per cent neutrahzed cysteine hydrochloride gave protection , and the protection afforded by 2 - 5 per cent dextrose containing 0 - 05 per cent b.a.l. 
the method now adopted , that of freeze - drying virus concentrates in lemeo broth , fulfils the condition , but little hght has been thrown on the mode of action of the stabihzing material . virus concentrates dried in this way have retained their fur activity for minimum periods of 12 months . the experiments with water alone showed that dmochowski 's ( 1948 ) results are confirmed in so far as virus may be recovered after drying - and our preparations had all been treated with 1 : 10 , 000 hcn during the isolation procedurebut it was not possible under these conditions to recover as much as 60 to 80 per cent of the initial virus activity as he claimed . salt solutions had no preservative action , and broth - containing media showed immediate advantages , even where the suspensions had been " purified " by centrifugal fractionation before desiccation . 
the action of the broth appears to be ponfined to the freezing - and - drying cycle or subsequently , since nothing was gained by carrying out the concentration stages in broth or broth - containing media , for which buffer - trypsin is quite satisfactory . it is unhkely , therefore , that the effect is solely an example of the phenomenon described by adams ( 1948 )  . 
the conditions of freeze - drying , moreover , do not involve vigorous shaking of the material but , equally , there is as yet ' no knowledge of the surface conditions which exist at an ice surface which is gradually receding through a drying mass . 
the observation that weaker ( 10 , per cent ) lemco broth is a less effective protective agent is of interest in this respect . it is possible to suppose that the action of broth and similar material is complex , that one or a combination of such factors as the forowing are important : ( a ) the broth pro - vides optimum conditions during freezing - such as an optimum eutectic point ; ( b ) that protection is conferred against the deleterious effect of ' heavy metals or of oxidation systems ; ( c ) that , in some way , the tendenoy of the virus to aggregate is reduced ; or ( d ) that an optimum amount of water only is lost . 
the rats were 4 weeks old when these operations were performed and 7 days later the litter - mates were joined in parabiosis . the surgical technique used was the one recommended by jacobsohn ( 1948 )  . in most pairs both partners were females except in those forming groups iii and vii , where a castrated male took the place of the spayed female . 
a total of 10 to 25 doses was given , when possible in a schedule of 3 doses per week . occasionally , this dosage had to be reduced to one or two administrations per week when the pair failed to show the expected gain in weight . twenty - six pairs of albinos ( groups i , ii and iii ) and 3 pairs of piebald rats 332 f . 
by stomach - tube during the first 8 weeks of the experiment . these rats , hke the majority of the parabiotic pairs , were 2 to 21 months old when the administration of the carcinogen was commenced , and served as controls for the assessment of the carcinogenic activity of the amounts of a.a.f. 
the parabiotic rats were sacrificed when declining health , in most instances due to the preserice of large pyometra , made it advisable or when the presence of a tumour was suspected . 
two of the " single " rats were killed when a palpable tumour was present , the remainder when the experiment was terminated at the 52nd week . the material taken for histological study was fixed in zenker , and the sections were stained with haematoxylin - eosin or according to van gieson . 
the tumours originated in gonads which were grossly hyperplastic . the histological changes occurring in the ovaries of rats joined in parabiosis to gonadectomized litter - mates have been well described by zeckwer ( 1944 ) , therefore our findings will be mentioned only briefly . 
the wall of these cysts was smooth , and when an epithelial lining could be recognized the cells were low cuboid or flat without any indication of cellular activity . such cysts occurred equafly in intact partners treated with a.a.f. 
the earliest neoplasms seen were generally round in sfiape and had a diameter of 3 to 4 mthey were found in wistar rats of groups i to iii after 16 to 20 weeks of parabiosis ; in piebalds they occurred even earlier . 
the largest gr ' anulosa cell tumour which had destroyed completely the ovary in which it originated measured 27 x 16 x 25 mand it was the only neoplasm of this kind to produce a metastasis , weighed 3 - 88 g . the secondary being situated in the adhesions linking the primary to neighbouring organs . the material at our disposal allows the study of the development of granulosa fig . 
2 shows a large haemorrhagic cyst cell tumours from their early stages . found in an ovary of rat 1 , group iv , sacrificed at the 13th week of the experiment . this cyst had a thin wall formed b fibrous connective tissue which in most places was poor in cells . in some areas the capsule was thickened , and here signs of previous haemorrhage such as pigment - loaded macrophages were present . into the cavity papillary projections protruded . 
they were of two kinds , some into the former , delicate strands with a narrow and others with a broad base . of spindle - shaped cers entered , forming their core . into the latter , capinaries penetrated surrounded by cers having ample eosinophihc cytoplasm , and a nucleous less rich in chromatin than the cells which covered and formed the bulk of the projections . these had a nucleus rich in chromatin and a scanty cytoplasthey were typical granulosa cells , while the ones having ample cytoplasm this was the earliest neopalstic lesion found in our resembled lutein cells . material , and shows that atypical growths of this kind were not necessarily permanent ones . 
and killed after more prolonged parabiosis hae ' morrhagic cysts , where only small nests of granulosa cells remained embedded in the dense connective tissue of the capsule while the cavity contained only inspissated blood and tissue debris . such chocolate cystlike lesions were absent from the ovaries of the control pairs not treated with a.a.f. another animal of the same group sacrificed 2 weeks , later was found to have in the ovary a macroscopically visible nodule formed almost entirely by granulosa cells . it was of about the same size as the early granulosa cell tumuor depicted in fig . 
3 shows a sharply limited spherical nodule situated in an ovary containing cystic follicles . it was surrounded by a thin fibrous capsule . between the capsule and the neighbouring cystic folhcles were large blood - fifed sinuses . 
5 shows the appearance of the granulosa cells forming the bulk of the nodule , and the tendency towards foci of liquefaction leading to the formation of cystic spaces within the tumour . 
the tumorous right ovary of rat 5 , group 111 , showed histologically an unusual picture . this ovary was also considerably enlarged ( 802 mg . ) and fairly solid with only a few blood - filled cysts only a small rim of ovarian tissue remained ; most of the near its surface . histologically this tumour was composed specimen was obviously neoplastic . mainly of spindle - shaped cells with scanty cytoplasm , and a nucleus which varied considerably from elongated dense to oval or spherical vesicular . 
among them small groups of cells were present having ample cytoplasm which stained well these elements had a larger vesicular nucleus with the chromatin with eosin . displaced towards the nuclear membrane . 
we have classified this neoplasm as a theca cell tumour because the granulosa contributed only little to its make - up . in the 36th week of the experiment the health of the intact partner suddenly declined and therefore in the region of the left ovary there was a large blackish the pair was sacrificed . cyst , on the posterior wall of which some ovarian tissue was recognizable . 
two types of neoplastic cells could be distinguished : bizarre cells of unusually large size having one or , rarely , their cytoplasm was several nuclei with deeply stained prominent nucleoli . intermi ' ngled with these elenients ample and stained only weakly with eosin . these were polyhedral in were nests of much smaller cells of epithelial character . shape and had well - marked cell borders , in cohtrast to the large elements which tended to form svnvctia . 
 ( groups v , vi and vii )  . the only lesion suspicious of atypical growth was found in one of the ovaries of an intact female which survived parabiosis for 42 weeks ( group v , rat 8 )  . 
we are unable to state with certainty that this lesion was of neoplastic nature . as already mentioned , no ovarian tumours were found in the 10 " single albino rats which received 24 doses of 4 mg . 
among many hundred female rats treated with this carcinogen we have found only one instance of a neoplastic lesion in the female gonads . this was discovered in a rat 171 months of age when sacrificed . 
by stomach - tube when 2 months old ; then the animal was kept without further treatment for 1 year , and for the last 16 weeks of her life she received methyl - thiouracil in the drinking water . 
at the post - mortem the left ovary was found to be converted into a large cyst measuring 20 x 15 x 10 mm . on histological examination septa subdividing the cyst in several compartments and covered with granulosa cells were seen . although macroscopicany this cyst resembled the clear cysts which we have frequently found in the ovaries of parabiotic females and also in rats treated with stilboestrol , we have never observed in such structures prohferation of granulosa cells exce ' t in this one instance . the morphological 8ign8of the endocrine imbalance exi8ting in the intact partner . all signs of hyperoestrinism were present in the intact partner ( zeckwer , 1944 )  . 
the vagina was lined by hyperplastic squamous keratinizing epithelium . in the few instances where the uterus was not heavily infected the epithelium lining the cavity was tar cyhndrical and areas of squamous metaplasia were also present , the wall of the organ being thickened . in the infected uteri most of the epithehum was destroyed . 
the breast glands were grossly hyperplastic , and in most animals macroscopicary visible cysts fired with a milky fluid were seen . histologically such glands showed a pronounced cystic hyperplasia of the ducts and periductal fibrosis . 
the thymus was atrophic , and the suprarenals enlarged in size due to a hyperplasia of the cortex . the pituitaries of the intact partners were invariably larger than those of the gonadectomized litter - mates , and already after 15 to 17 weeks of parabiosis had increased to an average of 8 mg . 
the largest observed ( rat 6 , group iii , and rat 8 , group v ) reached the extraordinary weight of 74 - 8 and 139 - 3 mg . 
the pituitaries of the intact partners were mostly solid and of whitish colour and haemorrhagic areas while the majority of these glands showed a symmetrical were not conspicuous . enlargement of the anterior lobe , in females surviving for more than 25 weeks of irregular shape . 
at the experiment the pituitaries assumed an ever - increasin first small whitish or sfightly yerowish nodules appeared which were single or multiple . later on the normal shape of the gland became more and more obscured by irregular growths , which compressed but never invaded the brain . the larger the tumour the greater was the tendency for brownish discoloration . these lesions occurred in intact partners independently of whether a.a.f. 
common to many of these elements and independent of the degree of acidophilic granulation was the pecuhar golgi apparatus which in papanicolaou preparations appeared as a ring - like structure , the negative golgi fig . 
17 , shows that the majority of the cells composing this structure were degranulated with only a few acidophils remaining . in the more advanced adenomata of the pituitary more atypical cens appeared but fundamentary they did not differ from the earlier lesions . in our material we have rarely seen adenomata completely free of acidophils . 
to conclude , we consider the nodular structures to be adenomata derived from cells of the acidophil series . tumour8of other organ8ob8erved in intact partner8and in " 8ingle " rat8of group viii treated with a.a.f. in the rats of group viii three adenocarcinomata of the breast and one squamous ketatinizing epithelioma of the extemal auditory meatus were found ( table iii )  . 
two of the cancers appeared after an interval of 51 to 52 weeks , only one of the i.e. , 9 weeks after the pair surviving longest had been sacrificed . intact partners treated with a.a.f. 
developed tumours of the breast ( rat 6 , group ii )  . in the 35th week of the experiment a mass was felt in the region of it was surgically removed , and was found to be the fifth left mammary gland . a well - encapsulated tumour measuring 20 x 12 x 9 mon cutting , milky histologically it was a fibroadenoma , in which fluid escaped under pressure . the epithelial elements were much more numerous than is common in such tumours except when occurring in pregnant or lactating females . 
the other was a small adenocareinoma of the breast which showed far less secretory activity than the fibroadenoma which had developed simultaneously . benign cystic cholangiomata were present in practically all rats treated with a.a.f. , but in the intact partners they were generally larger and more widespread than in the " single " animals , in which they were limited to a few cysts in lobus caudatus and left lobe . 
we are unable to state why such changes occurred only in isolated instances . another feature in which the spayed parabiont differed from a " single ovariectomized female was the cytology of the suprarenals . 
24 is included for comin animals killed after 15 to 25 weeks of parabiosis . it shows the distribution of lipoids in the cortex of the suprarenal of a parison rat spayed 6 months previously . 
a second experimental method ofobtaining such neoplasms was discovered by biskind and biskind ( 1944 ) , who obtained such tumours by transplanting ovaries into the spleen of gonadectomized rats . 
the gonads of the intact partners were composed of cystic follicles - proof of increased secretion of fouiclestimulating hormone ( f.s.h. ) by the pituitary of the irradiated parabiont . the liver of rodents inactivates ovarian steroids so efficiently that the secretions of a gonad grafted into the spleen do not enter the general circulation . in consequence the pituitaries of animals bearing such grafts are of the castrate type , and have an elevated gonadotropin content , as shown by greep and jones ( 1950 )  . fels ( 1949 ) discovered that a temporary hgature of the blood vessels supplying the ovaries led to an endocrine imbalance characterized by hyperoestrinism in the presence of castration changes in the pituitary . it seems therefore that one factor is common to at least 3 of the 4 methods quoted above ; they induce an endocrine imbalance characterized by pituitaries secreting elevated amounts of gonadotropins . it is therefore not astonishing that the neoplastic changes induced under these experimental conditions are all of the same kind . nearly all growths so obtained belong to the group of granulosa - theca - lutein cell tumours . 
moon , simpson , li and evans ( 1950 ) also regard the neoplastic changes observed in the ovaries of rats treated with growth hormone to be due to a pituitary imbalance . these authors mention a reduction of the acidophils and an increase of the chromophobes in the pituitaries of such rats , and noted that in 2 animals the histological picture of the anterior pituitary was of the castration type . it seems therefore that the basophils and especiary the f.s.h. secreting cells can increase in animals treated with growth hormone . however , more information is required before one can assume that ovarian .eoplasms obtained by treatment with growth hormone are due to the same mechanism as the other experimental tumours of the ovary , i.e. , to an excess of gonadotropins . in our case there can be no doubt that tumour development in the female gonad was the result of increased stimulation by gonadotropins and of the carcinogenic action of a.a.f. it is especially the foricle - stimulating hormone secreted in elevated amounts by the gonadectomized partner which determines the endoadmittedly during the first weeks of parabiosis there is good crine situation . evidence for the action of luteinizin hormone , as indicated b the presence of many healthy corpora lutea in the ovary of the intact litter - mate . later , when the increased secretion of oestrogens from the stimulated ovary has suppressed all the gonadotrophic activity of the intact partner 's pituitary and continuous oestrus has become established , the pituitary hormone dominating the picture is f.s.h. it is therefore not astonishing that granulosa cell tumours are so frequent in our material and that luteinization occurred to only a hmited extent . 
4 , 6 and 7 of their paper resemble closely the early lesions observed by us , and which we have seen to progress to tumours of considerable size . it seems unfortunate that drips and ford ( 1932 ) compared the atypical structures observed - by them in the irradiated ovaries of rats with carcinomatous ovarian cystadenomata of the 342 f . 
and luteinizing hormone ( l.h. ) in the ovarian cycle is greatly disturbed in the parabiotic female joined to a gonadectomized litter - mate . after 3 to 4 months of parabiosis the ripe follicle is not any more transformed into a corpus luteum nor does it involute , but is exposed to continued stimulation , which does not cease after the death of the ovuthis is in our opinion the decisive factor which leads to the development of the granulosa cell tumours . contrary to what is seen in spleen graftecl or irradiated ovaries of mice , in the rat there is not the shghtest evidence that these tumours " arise from proliferation and ingrowth of germinal epithehum " , as assumed by li and gardner ( 1947 )  . we have observed in some glands smar tufts of cells growing out from the surface ' germina of the ovary , but we have never seen tubular ingrowths from origin from embryonic nests seems a most unlikely hypothesis , epithehum "  . since many workers obtained ovarian tumours in 50 to 70 per cent of their experimental animals ( kaplan , 1950 ; furth and sobel , 1948 )  . . 
undoubtedly the stroma cell of the ovary can differentiate into theca or granulosa cells , and therefore one cannot still , we prefer origin from differentiated granulosa exclude this possibility . cers because of the morphology of the early lesions observed by us . 
12 and 13 one has not to fall back on the conception of disturbed embryogenesis . in preovulatory follicles invaginations of the theca accompanying tufts of capifaries are a common feature . the chorion epithelioma - like tumour presented some diagnostic difficulties . we consider it to be an anaplastic carcinoma . 
as pointed out by willis ( 1947 ) , anaplastic carcinoma can simulate chorion epithehoma and therefore more than morphological similarity is required to establish the diagnosis , in the absence of pregnancy . 
the lack of teratomatous elements and the lack of signs of functional activity such as corpus luteum cysts in the unaffected right ovary are in favour of the diagnosis of anaplastic carcinoma . 
was given simultaneously with or previously to the treatment with goitrogen . spontaneous ovarian tumours and especially granulosa cell tumours are exceedingly rare in rats ( iglesias , stemberg and segaloff , 1950 ) , and therefore do not complicate the interpretation of the experiments reported in this paper . finary an explanation has to be given why the incidence of granulosa cell tumours in group i is lower than in groups ii and iii . 
and most probably also our surgicaltechnique . group i represents our first parabiotic pairs , in which we did not succeed as well as later on to obtain wide junctions , measuring 6 to 10 cat the time the animals were sacrificed . the study of a number of organs of the intact partner showed clearly the effects of oestrogens secreted in excessive amounts by the stimulated ovaries . one of the sequels of this hyperoestrinism were the pituitary adenomata which occurred whether or not a.a.f. 
we beheve , however , that originary these benign neoplasms were acidophilic , just as in zondek 's case ( 1940 )  . this author observed an adenomatous lesion composed of acidophils in the pituitary of a woman treated with very high doses of oestradiol . whereas the increased secretion of oestrogens by the stimulated ovaries led to neoplastic changes in the pituitary , no mammary tumours were observed in the control pairs , contrary to the findings of zeckwer ( 1944 ) , and only one of the intact parabionts treated with a.a.f. 
developed tumours of the breast gland . the material at our disposal does not arow the conclusion that the high level of oestrogen in the circulation of the intact partner inhibited the carcinogenic action of a.a.f. 
in intact female rats joined in parabiosis to gonadectomized litter - mates . ovarian tumours developed in about 50 per cent of these animals . ( 2 ) a description of the histology of the ovarian neoplasms has been given and their histogenesis discussed . it has been found that most of them were of the granulosa cell type . 
secreted in excess by the pituitary of the gonadectomized litter - mate is regarded to be the factor essential for their development . ( 3 ) the pituitary tumouis observed in intact parabiotic females are considered to be due to the excess of oestrogens secreted by their stimulated ovaries . 
the gonadectomized partners were always found to be free of neoplastic lesions , whether or not their litter - mates received a.a.f. ( 5 ) the state of hyperoestrinism present in the intact parabiont did not enhance the carcinogenic action of a.a.f. 
were administered to " single " female rats two mammary cancers appeared during the first 40 weeks of the experiment , a period which corresponds to the maximum survival of our parabiotic pairs . ( 6 ) benign cystic cholangiomata were found in nearly all rats treated with in the intact parabionts they were more numerous and larger than in a.a.f. the " single " rats . we wish to thank professor r . 
philps. from the department of clinical pathology , university college hospital , london , w.c.1. received for publication july 2 , 1954 . the examination of sputum for carcinoma cells can only be considered a diagnostic method of clinical value if false positive diagnoses be avoided and cases wrongly thought suggestive of carcinoma reduced to a minimuthe method cannot be used to exclude carcinoma as it is evident that malignant cells may not be found if they are present only in small numbers , or in the case of an early it must be accepted , therefore , that growth the sputum may contain none . 20 to 25 per cent of bronchial carcinomata will be missed by this method and the problem is to be sure that a positive report is as reliable as possible . 
1 , 2 and 3 contained a considerable amount of necrotic epithelial tissue , and in one small group of cells , two mitotic figures , one of which is shown in fig . 
4 , 5 , 6 and 7 . both cases the appearance suggested a clump of carcinoma cells but the ciliated border could in places be clearly seen , making the true nature of the cells evident . bronchial epithelial cells sometimes show vacuolation of the cytoplasm and may then give a disorderly appearance with may lead to confusion with carcinoma cells , , such an appearance is illustrated in fig . 
 - on close inspection of this clump , it was clear that the individual cells did not form part a fragment of tissue as there welre spaces between them , and they had more cytoplasm than do oat cells . 
the cells bear a strong resemblance to oat cells but can be distinguished from them because the cytoplasm is relatively abundant and the nuclei of adjacent cells show no tendency to moulld together . 
13. - part of the fragment under higher magnification . the pattern of the cells resembles that seen in oat cell carcinoma , adjacent nuclei showing a tendency to mould together . there is more cytoplasm separating the nuclei than is commonly seen in oat cells , and the chromatin pattern is nowhere visible whereas in oat cells it is usually clearly seen . this appearance was reported as being suggestive of carcinoma . 
17. - a corpus amylaceum enclosed within a cell which appears to be of epithelial origin . the nucleus of the enclosing cell was at the periphery of the enclosed body but is not well shown in the photograph . the corpus amylaceum was semitransparent and was devoid of any nuclear characteristics . 
the nuclei of the individual cells mould together rather as do those of oat cells , giving the whole clump an appearance resembling oat cell carcinoma . all the nuclei however , are dense and the cells possess more cytoplasm than is usually seen in oat cells . 
the specimen was reported as follows : " films show clumps of cells , the arrangement of which is suggestive of oat cell carcinoma though the individual cells are not sufficiently characteristic to indicate malignancy . " the diagnosis of bronchial adenoma was made at bronchoscopy and confirmed at post mortem nine months later following the patient 's death from coronary thrombosis . ( e ) appearances due to macrophages of unusual type . macrophages , when they are seen to contain dust particles , can be easily identified , but when devoid of such particles , they may sometimes be confused with carcinoma cells . 
the nuclei are central , multinucleate cells frequently occur in carcinoma but they and number about 12 . are in no way diagnostic of it , the commonest multinucleate cell seen in sputum films being the macrophage . this example is the largest that i have seen . 
they received a diet consisting of whole meal flour ( 7 parts ) and skimmed milk powder ( 3 parts ) , supplemented by cod - liver oil and cabbage once weekly . for each animal 12 g . of food were provided daily . 
the dose of methylthiouracil given to the males was doubled during the last 10 days before they were sacrificed . four males and two females received methylthiouracil only ; two males and two females methylthiouracil plus a.a.f. , and four females a.a.f. 
only. thyroxine injections were started when the animals had stopped growing . this occurred in the females after three weeks of methylthiouracil treatment , in the case of the males , after four weeks . dl - thyroxine was dissolved in saline with na2co3 to ' give a solution containing 10 , ug . 
griesbach during the period of thyroxine treatment the rats were weighed were killed . twice weekly and the injected amounts adjusted to the weights . five female rats , 7 to 8 weeks old , were thyroidectomized . three weeks after operation , when the constant weight of the animals suggested completeness of thyroid ablation , these rats were started on the milk - flour diet containing 0 02 per this concentration of a.a.f. 
are badly tolerated the carcinogen to each rat per day . after eight weeks of this regime , thyroxine treatment by thyroidectomized rats . was started , each animal receiving one daily injection of 2 - 5 , ug . 
body weight completely compensated for the thyroxine deficiency produced by methylthiouracil , independent of the presence of a.a.f. twenty - two rats ( 6 males and 16 females ) were treated with 2 - 5 , ug . 
nor the controls reacted as uniformly as the animals injected with the higher dose of thyroxine ( table iii )  . in the males , the thyroid weights did not show any significant differences , the values being slightly above normal in both groups . 
with the exception of two animals , all showed an increase in cell all pituitaries were normal , showing heights far above the normal values . basophil counts of the same order as the controls . comparison of the values obtained in the animals with and without a.a.f. statistical shows that the greatest differences were found for the cell heights . analysis of these values proved that the difference between the means was highly the difference found for the means of the thyroid weights significant ( p < 0 0 1 )  . of the two groups , however , was of doubtful significance ( p > 0 05 )  . the pituitaries of the five thyroidectomized females treated with a.a.f. 
the weight increase of the thyroid induced by goitrogens is a complex phenomenon . it is due to increased numbers and size of the epithelial cells , and may be partially offset by the loss of colloid . 
when the supply of thyrotropin is reduced either by withdrawal of the goitrogen , or by administration of thyroxine , cell size decreases within a short time , whereas , the number of cells remains high over prolonged periods and colloid reappears . 
the latter factor must introduce uncontrollable errors when the thyroid weight is used as a criterion of thyrotropic action . in our experience , as in that of rawson and starr ( 1938 ) , the estimation of the mean acinar cell height has been found to give more reproducible results in assaying the degree of thyroid stimulation than the weight method . since a close correlation exists between the size of thyroid cells and the number of pituitary basophil cells , the percentage count of basophils has been used for assaying states of thyroxine deficiency in combination with the measurement of epithelial cell heights ( griesbach and purves , 1945 )  . in the state of fully developed thyroxine deficiency the percentage of basophils reaches values of 30 to 45 per cent . 
by excluding from the count masses of basophilic colloid free from cellular structures , we believe to have eliminated this possible source of error . all rats injected with 5 - 0 yig . 
griesbach the goitrogen - treated rat enlargement of thyroid cells is linked with an increase in numbers of pituitary basophil cells , indicating elevated thyrotropic activity . this correlation breaks down under the influence of a.a.f. 
one half of the animals still had large goitres and , histologically , in all but one the epithelium was almost as high as in the rats which did not receive thyroxine . no evidence for an increased demand for thyroxine or for higher sensitivity to thyrotropin was found in the animals treated with a.a.f. 
when a thyroxine deficiency was induced in a.a.f. treated animals by surgical or chemical means , their pituitaries responded in the similarly , the growth same way to thyroxine as did the animals without a.a.f. response of the female rats to thyroxine was independent of the presence of a.a.f. in the males , the pronounced liver damage prevented normal growth . these facts show that the action of thyroxine on the pituitary was not inhibited by a.a.f. 
the problem can therefore be reduced to that of an anomalous behaviour of the thyroid epithelium . in the hands of paschkis , cantarow and stasney ( 1948 ) l - thyroxine did not prevent the change from normal to high epithelium . in our experiments , physiological amounts of dlthyroxine did not reduce a high cylindrical epithelium to normal . it must , however , be remembered that the hyperplastic thyroid epithelium of the a.a.f. treated animals was not completely refractory to thyroxine . 
and storing at that temperature and after drying following freezing to from the frozen state ( gye , begg , mann and craigie , 1949 )  . in addition , mouse breast carcinoma which had been frozen to - 79 ' c . 
from these results it was concluded that since the physical treatments kired the normal embryo cells , they must also have killed the tumour cers , and that the tumours which arose from tho inoculations of treated m ' aterial must have been caused by a viius liberated from the dead cells . the claims of gye and his co - workers have been much criticized ; hirschberg and rusch ( 1950 ) , passey and dmochowski ( 1950 ) , passey , dmochowski , lasnitzki and millard ( 1950 ) and wamer and gostfing ( 1950 ) have all pointed out the great weakness of the assumption that since embryonic cells failed to grow after exposure these recent authors to low temperature , such treatment is lethal to ar cells . have each reviewed some of the ' extensive work reported in the last forty years , which shows that of both normal and neoplastic tissues in many species , some will and some will not survive exposure to extreme cold . in view of this great variation in response to cold shown by different tissues , it was felt that an investigation into the effects of freezing and drying upon a tumour affecting a non - mammalian host would be of value ; the rous no . 
i since it is a tumour from which a virus is easily fowl sarcoma was selected . separable , it was considered that the effects of cold and desiccation should be investigated upon the virus and the cers separately . that the virus was able to survive freezing and drying has been estabhshed for some time ( knox , 1939a ; hoffstadt and tripi , 1946 ; dmochowski , 1948 ; carr and harris , 1951 ) , and it has also been know - n to retain its tumour - producing activity after the ap ' plication of cold by repeated freezing and thawing ( cramer and foulds , 1930 ; selbie and mcintosh , 1939 )  . however , the response of the cells of the rous sarcoma to freezing and desiccation has not hitherto been ascertained . 
nakahara and yaoi ( 1930 ) found that rous sarcoma material which had been subjected to repeated freezing and thawing was less active when injected than similar untreated material , whidst selbie and mcintosh ( 1939 ) were able to prepare from rous tumour treated in this way filtrates with a greater tumour - producing activity than those made from untreated samples . selbie and mcintosh ( 1939 ) considered that repeated freezing and thawing broke up the cers and allowed a greater liberation of virus than would otherwise occur , and the method has been used for obtaining good yields of rous virus in various investigations ( knox , 1939b ; porard , 1939 )  . the work reported here consists ofexperiments upon the effects oftemperatures ' 70 ' c . 
they were between eight and nineteen weeks old when inoculated , apart from four exceptions which were slightly older , and belonged to three susceptible inbred lines developed at edinburgh , or crosses derived from thethe fines and crosses used were intensity , breeding , non - moult , breeding hen x intensity ' cock , and intensity hen x breeding cock , and have been described by greenwood , blyth and carr ( i948 ) ; both the age at which the birds were inoculated and the line or cross to which they belonged were determined by the exigencies of supply . preparation and treatment of tumour material . for each experiment a bird with a large actively growing sarcoma of anything from 15 to 27 days ' growth from the date of inoculation was selected as a source of tumour material and kired by wringing of the neck . 
when prepared , the disintegrated tumour was loaded into a record syringe for easy manipulation . where disintegrated tumour was to be subjected to cold or desiccation , the treatment was apphed as follows : freezing and storing . - amounts of i c.c. 
by starting the motor and setting the ampoule rapidly spinning on its longitudinal axis , a thin even film of disintegrated tumour was obtained on the inside of the bulb of the ampoule . 
the forceps w ' ere then released , causing a rapid rise of pressure within the apparatus ; this fell within five minutes to the original level , which was then maintained until the end of the period of drying , which lasted for 3 to 5 hours . 
epstein were separated off by centrifuging in an angle centrifuge at 3500 r.p.for 15 minutes , decanting the supernatant fluid obtained , and recentrifuging it aga ' in in a horizontal centrifuge at 6000 r.p.for a further 15 minutes . 
of saline and centrifuging in a horizontal centrifuge at 6000 r.p.for 15 minutes , resuspending the deposit in fresh saline , and performing the procedure either three ( experiment 1 ) or six - ( experiment 4 ) times . 
one sample of each preparation was mixed and incubated with an equal volume of saline and the other with an equal volume of serum ( diluted i in i 0 with sahne )  . 
the serum used ( e ) was from a fowl whose rous tumour had regressed and was one which had been shown to have strong anti - rous virus neutralizing powers in experiments 2 and 3 . that part of the experiment in which the virus and cer preparations were made from disintegrated tumour subjected to freezing and storing ( experiment 4c ) , samples of the preparations were mixed with an equal volume of pooled normal serum ( diluted 1 in io with saline ) , as well as with safine and neutrahzing serum e . all the mixtures were incubated in a water - bath at 37 ' c . 
in volume , and four inoculations of each preparation or dilution of a preparation were made . when inoculating preparations whose tumour - producing potencies were to be compared with one another , the injections of material from each preparation were made into separate groups of birds ; the scheme for the distribution of the injections of the various dilutions of each preparation amongst the birds in a group was the same in every case . 
the method of ' calculation used was that of reed and muench ( 1938 ) , and the figure obtained has been called by warner and gostling ( i950 ) the tpd 50 ; it is show - n in the tables comparison of this by its negative logarithm , designated the " tpd 50 index . " tpd 50 index of various preparations offers a comparison of their tumourproducing activities . strict aseptic technique was maintained throughout all the experimental procedures . all the experimental procedures were timed . 
where the virus suspension was made from disintegrated tumour which had been frozen and stored , the tumour - producing activity was in one case greater ( experiment id ) and in the other case less than that made from untreated material ( experiment 4d )  . it will be seen from table ii that washed cells of the rous sarcoma which had been exposed to any of the three physical treatments employed had less tumour322 m . 
on the other hand , in the case of washed cells which had been subjected to repeated freezing and thawing or freezing and storing ( experiments 4b and 4d ) , incubation with neutralizing serum , in contrast with incubation with saline or normal serum , totally deprived them of their tumour - producing activity . 
at the very least the centrifugation employed must be allowed to have separated off the overwhelming majority of the cefls , and the great tumour - producing activity remaining with the virus suspensions cannot be attributed to occasional cells left in them . accepting therefore that the virus suspensions were almost entirely if not wholly cell - free , the ability of the rous virus to retain some of its tumour - producing activity after exposure to cold has been demonstrated , thus confirming the work of cramer and foulds ( 1930 ) and selbie and mcintosh ( 1939 ) , who were able to prepare active filtrates from rous tumour material subjected to repeated confirmation has also been obtained of the ability of the freezing and thawing . virus to survive freezing and drp ' ng , which has been demonstrated by a number of previous investigators ( knox , 1939a ; hoffstadt and tripi , 1946 ; dmochowski , 1948 ; carr and harris , 1951 )  . 
as in the work of knox ( 1939a ) , so here the activity of virus preparations obtained from frozen and dried tumour material was considerably less than those made from untreated material ( table i , experiments ic and 4c )  . 
the contention , however , that preparations of rous virus made from repeatedly frozen and thawed sarcoma had a greater tumour - producing activity than those made from untreated material on account of the treatment breaking up.the tissue fragments and hberating the virus ( selbie and mcintosh , 1939 ) has not been borne out . 
the failure of the neutralizing ' serum to abolish the tumour - pro - ducing activity of washed cells which had been left untreated ( table iv , experiment 4a ) is considered to be evidence of the presence of live cells in the preparation . the slight reduction in the tumour - producing activity of the untreated washed cells which was brought about by incubation with neutralizing serum is considered to be due to the action of the serum on free virus liberated from or attached to cells damaged during the disintegration of the tumour material . the washed tumour cells subjected to freezing and drying were deprived of most of their tumour - producing activity after incubation with neutralizing serum ( table iv , experiment 4c ) ; out of the inoculations made with all the various dilutions of the frozen and dried washed cells , only one gave rise to a tumour . this was from one of the inocula of the 10 - 1 dilution of the mixture of cells and antiserunow , it has long been known that viruses can be recovered from neutral mixtures with antiserum simply by dilution of the mixture with sahne ; such reactivation has been demonstrated with vaccinia ( andrewes , 1928 ) and fowl plague ( todd , 1928 ) , and although this " dilution phenomenon " is harder to obtain in the case of the rous virus , andrewes ( 1932 ) was able to show it conclusively . 
christiansen. from the institutt for generell og elcperimentell patologi , universitetet i oslo . received for publication february 2 , 1953 . it is a strange fact that in the voluminous literature on breast cancer the prognostic value of the size of the tumour is only cursorily dealt with , a fact mentioned by geschickter ( 1945 ) and underlined by bloom ( 1950 )  . 
the explanation probably is , that the view expressed by kaae ( 1948 ) , namely , " it is generally recognized that the size of the tumour is a very important factor in the prognosis , and that the latter is much more favourable for the small tumours than for the large , " seems so generally sound , even self evident , that the problem has not been considered worthy of a closer study . if we examine the pertinent literature , we find , however , that the findings are not unequivocal . dahl iversen ( 1930 ) states that breast cancers up to the size of plums are without recurrences after 3 years ' observation in 83 per cent of the cases , whereas tumours larger , up to the size of a hen 's egg , show only 13 per cent freedom from recurrences after 3 years . eggers , de cholnoky and jessup ( 1941 ) report upon a 5 - year survival of 73 per cent , if the mass is 2 cor less , and only 24 per cent haagensen and stout ( 1943 ) found a if the mass has reached a size of 3 to 6 cm . 5 - year clinical cure of 62 * 2 per cent if the tumour was under 3 cand only 19 - 8 per cent if the tumour had reached 6 cor more . 
they conclude that " the data indicate , as might be expected , that the prognosis becomes worse as the size of the tumour increases "  . bloom ( 1950 ) found 5 - year survivals in the following percentages : tumour less than 1 inch 59 per cent , 1 to 2 inches 45 per cent , and more than 2 inches 32 per cent , and he finds after grading of the tumours that : " of the tumours with a diameter of 1 inch or less , 37 per cent are classified as grade i and 23 per cent as grade iii . 
on the other hand , in the case of growths of more than 2 inches diameter only 8 per cent belong to grade i whilst 54 per cent are grade iii . when the diameter lies between 1 and 2 inches the incidence of these tumours is practically the same " , and he concludes that : " whether the tumours are small or large , the outlook is uniformly good in the former ( grade i ) and bad in the latter group ( grade iii )  . 
on the other hand , an intermediate result is obtained for the intermediate cases ( grade ii ) , the survival rate being practically halved in in other words , the metastasizing power the presence of the larger neoplasms . for growths for grade i and also grade iii cancers is independent of size . classified as grade ii this power bears a direct relationship to the diameter , the larger the tumour the greater the likelihood of spread having taken place "  . 
christiansen the time factors are so long or so short that their significance is obscured under the usual clinical conditions . when kunath ( 1940 ) says : " size and ma88 . - an analysis of this point failed to reveal that a larger tumour carries any more serious a prognosis than " no does a small one " , and hoopes and mcgraw ( 1942 ) likewise conclude : correlation was found between the post - operative duration of life and the size of the tumour removed " , these findings are not necessarily in contradiction to the opposite conclusions , mentioned above . 
the explanation may be a different composition of the groups of tumours , as regard number of representatives of the again we have to guard ourselves in transferring different grades of malignancy . conclusions from groups to individual cases . considering the importance of assessing the significance of a minimum size of tumour for the prognosis of breast cancer , we have examined breast cancer material consisting of a total of 974 cases . 
we planned to examine the ultimate development of breast cancers as small as practically diagnosable . in order to decide the upper limit of the size to include , theoretical and practical considerafirstly , we considered the smallest lump , tions have been taken into account . that size evidently depends upon the site distinguishable as a definite tumour . and upon the amount of adipose tissue . 
a tumour near the surface and in a shrunken atrophic breast will be more easily discovered than one deeply situated it seems that tumours smaller than those the size in a full and developed breast . of a pea cannot reasonably be distinguished from the many irregular nodosities in a cimacteric , or pre - cimacteric breast , and in most cases it is difficult to feel secondly , we wanted to examine tumours a lump smaller than a small hazel nut . of a size so small that the number of cases would represent a very small fraction of the total , whereby we would obtain a statistical claim to a designation " a very small breast tumour "  . 
the tumours are usually characterized by some object for comparison , usually : pea , bean , nut kernel , hazel nut , date - stone , date , wall nut , plum , etc . 
a tumour the size of a hazel nut will usually measure some 10 to 12 by 15 to 17 mone has to have in mind the small size of a norwegian hazel nut to appreciate the size . when we examined our total material we found that only 56 tumours out of 974 , i.e. , 5 - 7 per cent . 
the fate of the patients has been followed for from 10 to 20 years . the material was examined during the later half of 1952 . the clinical information is not always precise , or detailed , as some of the case histories are very short . 
nor is the pathological material always complete , as some of the surgeons do not submit adipose tissue from the axilla if no suspicious glands are found . in other cases a selection of glands only are sent to the laboratory , and finally , some of our paraffin blocks were destroyed during the war , with the result that for some cases a few slides only could be examined . this means that all the positive findings are minimum recordings . the clinical follow - up has been complete , all patients having been accounted for . reliable death certificates have been received for all the dead , and the patients alive have been personally examined by one of us , or by competent doctors as regards the patients living in remote parts of the country . as only the patients with a definite statement as to the size of the tumour have been included , the size is known in all cases . 
8 died from broncho - pneumonia one year and a half after operation , symptom - free . all the others succumbed to their tumours . this 5 - year oure rate corresponds very closely to the rate quoted by engelstad ( 1948 ) for his group of 768 cases , regarded as stage i and stage ii cases . this indicates that our " small " breast cancers do not present a particularly favourable clinical picture . in one aspect our table ii shows a remarkable deviation from the usual , namely , the small difference between the 5 - year and the 10 - year figures , only 1 out of 37 patients dying in the second 5 - year interval . as stated , the whole group of 56 patients has been followed for 10 years . a smaller group has , however , been followed for a longer period , and in table iii some of the results are summarized . 
even if we select the very smallest tumours present in our series , those the size of a pea or a bean , out of a total of 10 , we find only 5 patients alive after 10 years , or more , and 4 patients dead from metastases . in the present series the combined surgical and radiological treatment seems , in a number of cases , to have effected a considerable delay in a finally fatal this delay is of very great value from a therapeutic standpoint , even outcome . if the treatment fails to effect a complete cure . staging actually is an ambiguous process . the prolonged observation also helps to assess more accurately the real stage the simplest and least of the tumours . reliable staging is the immediate clinical , unreliable to a degree to make it practically useless . 
we have , however , to bear in mind that the value even of negative findings of tumour cells in lymph this grouping is rather limited . nodes removed may be the result of the pathologist not finding the cells in spite or , tumour cells may by - pass the usual lymphatic filters in of their presence . the axillary glands and proceed directly to the supraclavicular or the intrathoracic nodes , or the tumour cells may spread via the blood streathe discrepancy between the number of tumours anatomically staged as stage i and the number of cures effected after a proper local operation shows the degree of failure in the process of staging . 
on the other hand , if radiological treatment has been added to the surgical , even the delayed retrospective clinical staging may be incomplete , because a tumour , anatomically staged as stage i and actually being in stage ii , may be cured by radiological treatment and thereby escape its proper staging . in spite of the incomplete clinical and pathological information , it will be of some interest to examine the state of affairs , as regards stages recorded in this material . 
10 , 27 , 31 died symptom - free after more than 10 years ' observation . the large number of fatal outcomes with negative findings of tumour cells in the axillary lymph nodes confirm our assumption that our figures represent the considerable number of patients alive and symptom - free minimum findings . in spite of positive findings of tumour cells in the lymph nodes , actually 5 patients , further confirm our statement as to a considerable effect of the treatment , but l . 
christiansen also underlines the great number of patients already in stage ii ( or further ) at the moment of presenting a very small breast cancer . if we add these 5 patients with microscopical lymph - node metastases , but still symptom - free , to the group of the dead and those living with metastases , we find that two - thirds of all our patients with small tumours were in stage ii ( or further ) when the operation was performed . the value of bloom 's ( 1950 ) grading and analysis of his material made it natural to try his principles on our material . 
we deliberately use the word principles , because any grading is arbitrary , and the designation in each case is the result of a subjective estimate of a series of characteristics , which themselves are unprecise . 
the explanation may be that the number of cases is too small , that the treatment given may have influenced the final result because a number of very malignant tumours are comparatively radiosensitive , or it may be caused by our incompetency . 
the medium long histories , from a few months up to a year , show an increasingly gloomy picture . if we again deduct the grade i cases we conserve the pattem , and still find indications of a benefit for very quick reaction with immediate treatment after diagnosis , and with a still more pronounced bad prognosis in cases with delays from a few months up to a year . for the very long histories ( more than a year ) the comparatively better prognosis is preserved , and may partly be accounted for by a default in the process of grading , partly by combination of high malignancy and high grade radiosensitivity in certain cases , and partly by inclusion of tumours with a more moderate malignancy ( grade ii )  . besides , a perfect correspondence between morphological grading and biological development is evidently not obtainable . too many unknown factors are involved here . 
usually the ventral prostates were explanted ; they were grown by the watch - glass technique , which is eminently suitable for organized gro - wth ( fell and robinson , 1930 )  . 
the medium was placed in a small watch - glass and allowed to clot ; the watch - glass rested on a layer of sterile cotton - wool soaked with sterile distilled water inside a small petri dish . 
but later this method was improved by explanting one lobe of each gland into medium containing methylcholanthrene while the other was kept as control . the explants were placed well flattened out on th ' e surface of the plasma clot , where they became firmly anchored . after a day or two the growing explants liquefied part of the plasma clot , and while still firmly attached to the surfa - ce of the clot were surrounded by a pool of liquefied mediuthe cultures were after the ninth day no transferred to fresh medium every second or third day . more methy1cholanthrene was added , and the cultures were maintained in normal medium for the rest of the culture period . the used glass - ware was decontaminated by keepino , it in concentrated sulphuric acid at room temperature for at least one week . 
the glands were fixed in 2 per cent acetic zenker after the following periods of growth : 5 days , io days , 14 days and 21 days . five to nine experimental and an equal number of control cultures were used for each point of observation . 
they were embedded in paraffin and seriary sectioned ; the sections were stained with ehrlich 's haematoxylin and eosin . to assess mitosis the number of dividing cells was counted in every second section , i.e. , in at least 20 sections of all single - lobe cultures . 
cultures treated with 20 - methylcholanthrene . cultures treated with methylcbolanthrene show a similar tvpe of growth at the beginning of the culture period : formation of new alveoh at the periphery and some central degeneration . 
the epithehum retains its glandular character and remains actively secreting in the treated explants for a longer time , but the stroma is usually verv poor and reduced in botb . 
one out of fi - ve treated cultures shows squamous metaplasia after the higher mitosis is stfll ' above that in the controls and has , in fact , risen after the dose . higher concentration while it has dropped after the lower . table ii gives th - e number of mitotic cells counted in 20 sections of controls and cultures treated for 9 days with 2 , y / cic . 
the number of dividing cells has fallen and nearly reached the control level . at the same time changes of a more anaplastic type can be observed in one batch of cultures treated with 2y of methylcholanthrene . 
squamous metaplasia develops more fully , particularly after the smaller dose , after the end of treatment . it is noteworthy that the d - ownward bend of the first wave coincides with the end of treatment . this may mean that the first peak is caused by a direct stimulating action of the carcinogen , whfle the second one is due to the increased growth - potential of the changed epitheliua rise in cell division has been reported by cooper and reller ( 1942 ) , who found a ten - fold increase hi the mitotic rate in the skin of mouse ears painted with methylcholanthrene , and by glucksmann ( 1945 ) , who observed a rise in mitosis a few hours after a single painting with benzpyrene . in contrast to the increase in mitosis and proliferation of the epithelial cells is the reduction of the stroma of the treated explants . 
of methylcholanthrene , which indicates that the dose for stimulation of fibroblasts is roughly twenty times lower than that for epithelium if the concentrations of 2 - 4y / / c.c. 
the cultures were grown in the presence of the agent for 9 days , then transferred to a normal medium and fixed at intervals after removal of the carcinogen . in both control and experimental cultures new alveoli were usually formed at the periphery of the explanted glands , while in the centre some of the al - veoli underwent degeneration . in the control cultures the epithelium quickly lost its glandular character , and the alveoli developed wide lumina lined by one layer of low epithelium in which mitosis was present though infrequent . 
of methylcholanthrene , the alveolar epithelium retained its glandular character for a longer time and showed a marked increase in mitosis , leading to hyperplasia and squamous metaplasia , while the stroma was considerably reduced in contrast to that of the controls . the first changes were recognizable 5 days after the beginning of treatment . they became more pronounced as the treatment continued and persisted after removal of the carcinogen . in the later stages partial or complete occlusion of the alveolar lumen with squamous metaplasia were observed . the rise in mitosis showed two distinct peaks , the downward bend of the first wave coinciding with the removal of the c ' arcinogen . 
fell for suggesting this problem and for her criticism in the preparation of the manuscript . i also wish to thank a . howard , radiotherapeutic research unit , hammersmith hospital , ' london , for the generous supply of cx males , c . 
w.3. received for publication april 3 , 1954 . the development of the search for endogenic carcinogens has been reported in earher publications from this institute , ( see hieger ( 1949 ) for references to previous papers )  . it has been shown that the cholesterol - rich fraction of ' tissues from human subjects who had died of cancer or of other causes , and even commercial cholesterol . 
the first tumour in table i was carried through 93 generations and the first tumour in table iv ( highly purified cholesterol ) has been growing vigorously in its 25th generation . 
the control tests on solvents are described further on in this paper . purification of the cholesterol was next undertaken , as a first step using the simplest technique . table ii gives the results of tests on fractions of commercial cholesterol obtained by crystalhsation from acetone . 
the method involved several stages . these were : ( 1 ) acetylation . this step provided several advantages , nameiy ( a ) the oh group was protected during bromination ; ( b ) the acetate can be differentially eluted from a1203by mild eluents the unacetylated sterol when absorbed on a1203 requires more powerful eluents . ( 2 ) bromination , filtration and debromination . ( 3 ) adsorption on a1203colunin and elution with benzene - pet . 
orr there was , of course , no guarantee that contamination could have been completely avoided in the " carcinogen - free " room ; for example , 'sawdust from a box - containing benzpyrene - treated mice might accidentally be carried in to the noncarcinogen room on the shoes of anyone who had walked through the carcinogen however , the technicians who serviced the mice in the . 
consequently the controls had more injections than the sterol injected mice in order to maintain a stationary nodule . is the carcinogenic activity of commercial cholesterol due ( a ) to the sterol itself , or ( b ) to highly active impurities ? the evidence presented in tables iv and v provides support for ( a ) , i.e. , cholesterol per se is the true carcinogen in the commercial product . if the incidence of sarcomas be expressed as the ratio ( percentage ) of tumour mice to injmted mice which survived to a minimal latent period level , say i year , then the result can be stated thus : ( a ) purified cholesterol gives rise to 4 per cent sarcomas in q ,  . 
the mice did not survive well , and in fact the single sarcoma appeared at the 27th month in the sole survivor of the 34 mice initioy injected with purified cholesterol . twenty - seven months is near the outsidei limit of the range of latent periods found with the carcinogens of the cholesterol categpyy , , in an experiment with commercial cholesterol ( table ii , section a ) 3 of the 4 280 1 . 
orr in 1947 ( unpubhshed ) , would provide an attractive theory of the mode of action of cholesterol as carcinogen . however , it would be necessary to postulate that the carcinogen is held by adsorption on the cholesterol 292 1 . 
op.p. although stif in a - n active stage , and that in sucha condition it is not roadily eluted , for clearly if it were a case of simple solubility there would be no more reason for ' the factor dissolving in the cholesterol than for it to be dissolved out secondly i ' ected cholesterol after a year or so in the body should be again . thirdly , if such an assumption were accepted , there rich in absorbed carcinogen . would be httle necessity to proceed with the question of whether pure or impure fourthly , if the carcinogen ' which is concencholesterol is the true carcinogen . trated in the cholesterol originated in the environment , it should be easy to test the hypothesis by purposely arowing the mice injected with the cholesterol to hve an atmosphere rich in carcinogen . this test has been put into operation , and constitutes a secoind stage to the investigation on atmospheric carcinogens as a factor in sarcoma induction ( see above )  . one hundred stock mice were injected with ohve oil solution of commercial cholesterol and kept in a carcinogen - rich atmosphere as described above . 
the control mice ( 135 ) were kept in the room free from carcinogen . the results are shown in table v . control te8t8 on the 801vent8 . lard was employed as solvent from 1936 to 1949 . during this time a total of over 360 mice was tested with the solvent , lard ' alone . these mice did not survive remarkably well ; they gave no positive result until the series had been almost completed , when among the last few batches a single sarcoma developed . 
when in 1950 , a change was made from lard to olive oil ( hospital dispensary grade ) , a control series of 134 mice was set up for injection with the oil alone . 
the old c " mice were 12 ( and upwards ) months of age at the start of the experiments ; their effective number should therefore be raised by a factor of the order of 2 since the initial number , 19 , would represent the survivors at 12 months . 
the siingle sarcoma occurred in an oldc57moim at the unexpectedly low latent period of 6 months . * however , s ' mce this mouse was 16 months of age at the start of the experiment some ageing factor for tumour induction is obviously operating . 
this preparation gave 2 sarcomas in 20 mice initiary . other work on carcinogenic activity of chole8terol . truhaut ( 1947 ) could find no activity in his sample of purified cholesterol . truhaut injected 20 mice , of unnamed genetic origin , with cholesterol " purifie ' , " 20 mice with cholesterol irradiated with 10 , 000 r , and 20 with solvent alone , namelv ohve oil . 
 " " si la susceptibilite ' individuelle des animaux n ' est pas en cause , cela tendrait ' a d6monter la pre 'sence , dans le choleste ' rol commercial , d ' impurete 's fortement cance ' rig ' enes qm se rapprochent vraisemblablement des substancek ; responsables de i ' activite ' cance ' rig ' ene de la fraction des ste ' rols precipitables par le digitonoside dans l ' insaponifiable du foie de sujets cancereux . steiner ( 1951 ) has also reported that no carcinogenic activity could be detected in a sample of cholesterol . 
from the carbonyl absorption found in cholesterol fractions , therefore , the type of impurity and its approximate amount can be deduced . cholesterol preparation numbers , 3 , 4 , 6 , 7 and 9 ( for key , vide supra ) showed no appreciable carbonyl absorption ( less than 0 - 25 per cent )  . 
number 8 ( glaxo sample 5989 ) had a band at 1744 cm . - ' , assigned to a 17 - ketone , equivalent to about 1 per cent of such an impurity . 
number 11 ( glaxo sample 1201 ) had three bands at 1744 , 1710 and 1674 cm - ' ; these indicate about 9 per cent of a 17 - ketone , 4 per cent of a 20 - ketone ( or possibly in a 6 - membered ring ) and 3 per cent of an ac , unsaturated ketone , probably a a4 : 3 - ketone . number 5 , which was the least soluble fraction obtained by fractional crystallisation of this latter commer290 i . 
the most soluble fraction in this crystallisation and used for the test in section d , table ii ( number 13 ) contained the impurities concentrated about five - fold . 
lucasanda.c.thackray. from the , department of pathology , the royal dental hospital of london school of dental surgery and the bland - sutton institute of pathology , the , middlesex hospital , london , w . 
the tumour occurs in the lower jaw much more frequently than in the upper ( i 7 cases and 3 cases respectively in this series ) , is usually a central lesion and gradually enlarges , in the majonty of cases without pain . in the course of time the bone becomes absorbed , and if a cystic loculus is opened infection and discharge forow . local recurrence iscommon fohowing inadequate treatment , but metastases are very rare . 
a case of pulmonary metastases has been reported by waterworth and purar ( 1948 ) , who review previous reports . the natural history of the disease is long ; it is not always easy therefore to assess the efficacy of various methods of treatment . most authorities consider radical excision of the tumour to be the treatment of choice . 
thus the least evolved type of tumour consists of strands of more or less undifferentiated epithehal cers growing in a fibrous stroma , while a tumour which has undergone a greater degree of entiation consists of folhclea 290 r . 
the epithelial follicles in such cases consist of an outer layer of columnar cells resembling the similarly situated cells of the enamel organ , while towards the centre the cells become stellate in appearance and cyst formation may occur . on the other hand , the trend of differentiation may be towards a more highly developed type of squamous epithelium , in which case the tumour consists of sheets of squamous cells showing a tendency to cornification , or a basal cell type of growth may be produced . these tumours may thus present a variety of appearances , from case to case , or in different areas of the same growth , and while attempts at classification on a histological basis are helpful in so far as they indicate the varying degrees of differentiation whicli can be observed , they are seldom entirely applicable to any given specimen . 
tboma ( 1950 ) has proposed one such classification , as follows , though he notes that pure types are but infrequently seen : ( 1 ) primitive type , composed of strands of epithelial cells showing little tendency to differentiation , growing in a loose fibrous stroma . 
a very rare type of tumour in which haemangiomatous characters are present . ( 8 ) melano - amelobla , 3toma . also a very rare tumour , in which the epithelial cells contain pigment . in our series 4 cases were of the primitive type , whilst the remainder were fig . 
2 ( case 5 ) shows an largely follicular or showed mixed appearances . example of the primitive type of tumour , cords of epithelial cells growing in a fibrous stroma . 
6 ( case 5 ) , in which the growth is composed of follicles or nests of epithelial cells with outer columnar layer and inner stellate area . microcyst formation , a common occurrence in adamantinoma , was present in typically , these cysts occur in the area of stellate cells towards the 14 cases . centres of the follicles , but they also form in the stroma . 
the occurrence of stromal cysts is a point to which very little previous consideration appears to siegmund ( 1929 ) noted their occurrence in 2 of his cases , but bave been given . apart from this instance , and a passing reference by kronfeld ( 1930 ) to the same fig . 
8 ( case 1 )  . in the latter case , however , it will be seen that though there is some breakdown within the follicles , the majority of the cysts have formed on the side of the columnar cell layer opposite to that on which fig . 
even in the 6 cases showing epithelial cysts only , evidence could be found in 3 cases of incipient degenerative changes in the stroma . the cause of cyst formation is a matter of conjecture . it is believed to be the result of progressive degeneration in originally solid growths . the solid tumour closely resembles the developing tooth up to the point at which differentiation of adjacent connective - tissue cells into odontoblasts , and subsequently amelogenesis , would occur in the case of the tooth , but at this stage the tumour cannot develop further . degeneration therefore takes place ( kronfeld , 1930 ; robinson , the ensuing accumulation of fluid of relatively high osmotic tension is 1937a )  . probably a factor in the progressive enlargement of the microcysts , a mechanism investigated by toller ( 1948 ) in the case of simple dental cysts , and quite possibly a factor also in the case of cyst formation in these tumours . with regard to cyst formation in the stroma , it appears that again a process of degeneration is at work , and all stages of breakdown can be seen from a slight loosening of the stroma to mucinous - like degeneration and the formation of completely clear cystic spaces . 
the inner enamel epithelium is that which lines the concavity of the enamel organ , a single layer of tan columnar cells which will produce enamel , while the outer enamel epithelium consists of cuboidal cells covering the convexity of the organ . 
on the other hand , bland - sutton ( 1922 ) thought that the enamel organ could not be the origin of these growths , since the majority of patients were well into adult life when their tumours first appeared . however , robinso ' n ( 1937b ) in his survey of 379 cases found that the tumour was first noticed between the tenth and thirty - fifth years in 70 per cent of cases . considered together with the fact that these tumours are very slow growmg and have a long natural history , it is evident that the majority of growths originate at quite an early age . robinson ( 1937b ) also found that the tumour occurred most frequently in the premolar and molar regions , where supernumerary tooth germs most often occur , kegel ( 1932 ) and and that many cases were associated with a missing tooth . geschickter ( 1935 ) also support the view that the tumour arises from the enamel byers and sarnat ( 1945 ) believe that the tumour originates from that organ . structure during the first few years of life , though active growth may not become manifest till later . if these tumours , or at least the majority of them , originated directly from the enamel organ , it might be expected that on occasion enamel would be formed . this is never the case , though thoma ( i 950 ) considers that the homogeneous zone sometimes to be seen between the basal membrane of the columnar cells in the follicular type of adamantinoma and the stroma , which appears yellow with van gieson 's stain , must be considered as abortive enamel formation , though it is possible that precystic changes in the stroma could account for such appearances . 
thackray these tumours resemble rodent ulcers in several respects . tumour without involvement of the oral epithelium , is , however , evidence against an origin from the oral mucosa . both are related to derivatives of the covering ectoderm , the one to teeth and the other to hair follicles , though discussion continues as to the stage of development of the appendage at which they arise . 
they are composed of relatively undifferentiated cells which can give rise to any of the appearances found in these tumours , and moreover will produce a central growth . it is not necessary to postulate tumour formation from these rests in early life , with a subsequent interval of dormancy to account for those cases in which the tumour first appears at a comparatively late age . being present from the formative phase of the dental tissues onwards they can proliferate at any time , and this seems a more satisfactory hypothesis than the dormancy theory . the rests of serre , those left by the dental lamina , are situated quite superficially . 
here the cells tend to take on a sterate appearance towarcls the centres of the cords and become elongated and columnar at the periphery . there is some cystic degeneration in the stellate areas and also in the stroma . case 4 : - 11 . 
1893. - 1910 : dentigerous cyst of one year 's duration 1928 : swelling had gradually increased in removed . size till there was now a hard tumour of the right mandible . this was excised and the cavity of a multilocular cyst exposed . 
radium tubes forced up through harcl palate . october , 1925 : no improvement . tubes left in 18 hours . december , 1925 : left side of face swollen over superior maxilla . severe paon left side of hard palate is an irregular swelling extending from mid - line to , and including alveolar margjanuary , 1926 : alveolar part of superior maxilla and the palatal tumour excised . 
1892. - 1926 : noticed a lump in the right upper jaw which she thought to be due to ill - fitting dentures . this was treated with " caustic and disappeared , but recurred within 4 months . it was again similarly treated . 
1928 on admission to hospital an oval area of enlargement of the right maxina was noted , situatecl between the alveolar margin of the maxilla and the inner surface of the cheek , the long axis clirected antero - posteriorly for about an inch . 
1899. - 1928 : operated on for " abscess of j aw . 1937 : painful swelling appeared at site of previous operation . x - ray examination showed a multflocular cyst in the 3 - / - 6 region . 
1887. - 1929 : the patient complained of a lump on the right side of the jaw of 10 years ' duration , which had been operated on 3 times , 10 , 6 and 3 years previously . it had increased in size , painlessly , but rather rapidly since the last operation . 
1881. - 1937 : three years ' history of swelling of the right lower jaw after extraction of 3 teeth . this was considered to be due to a dental cyst , and the jaw was scraped on two occasions . after the first operation the swelling disappeared . 
thackra ' y examination showed a large swelling on the lingual and buccal aspects of the pain . x - ray showed expansion of the jaw by a loculated , premolar and molar regions . 1950 : died from other causes . 
1883. - 1937 : admitted to hospital for a fracture of the this appeared elbow - joint , when a large swelling of the right mandible was noticed . to have started some 5 years previously , and had been gradually increasing in size . x - ray examination showed the typical appearances of adamantinoma , and local excision of the cyst was undertaken . 
orr. from the department of experimental pathology and cancer research , university of leeds . received for publication july 19 , 1947 . attention was drawn to the frequency of spontaneous tumours in the lungs of mice by tyzzer ( 1907 - 8 , 1909 ) , whose description of their histology has required but little amendment . 
a small group of stock mice was treated intranasally with 1 : 2 : 5 : 6 - dibenzanthracene in almond oil , but owing to intercurrent disease these had all died before adenomata were present in any except one . 
the present communication is based on the histological investigation of the lungs of a representative sample of these mice , together with the urethanetreated mice of the previous paper ( orr , 1947 ) , and a number of mice showing spontaneous pulmonary adenomata . 
the outline of the whole tumour is usually more or less circumscribed , though there is no definite capsule ; sometimes it is irregular , but the appearance is not that of true infiltration . 
the two types of tumour have also been noted by grady and stewart ( 1940 )  . occasionally , both types of structure have been seen in the same nodule , and there appear to be adequate grounds for regarding them as morphological variants of an identical process . it is not uncommon to find alveolar macrophages of the " dust cell " type in the adenomata . 
they are often so heavily loaded with carbon as to obscure all nuclear and cytoplasmic detail . less often other evidence of inflammation in the form of lymphocytic or leucocytic infiltration is seen . but in addition a very large number of lesions show appearances which make the impression inescapable that they are stages in the development of adenomata within inflammatory foci . this evidence is more striking where the tubulo - papillary structure is being evolved , in view of its highly characteristic and easily recognized pattern . 
the inflammatory changes resulting from urethane are relatively chronic , and take a considerable time to clear up on withdrawal of treatment . moreover , the proportionate share played by polymorphs in the reaction even in its early stages seemed smaller than average : it may be that urethane exerts some depressant effect on them , and thus necessitates greater activity by the so - called fixed tissues . the source of the epithelium in the tumours has not been determined with certainty . indeed , in many instances even the simple statement that it is epithelium involves a measure of assumption ; the most that can be said with 320 j . 
the actual existence in the fully developed lung of such a tissue is denied by many authorities , and some of those who claim to find it describe morphological appearances very different from those found in the tumour cells . if the alveolar epithelium is implicated , it can only be by reversion to the embryonic type , and if this occurs , such epithelium might owe its genesis , as it does in the embryo , to the bronchial epithelium . it appears to the present author that some workers have been inclined to regard as alveolar epithelium any lepidic tissue in the lung which could not be . 
shown directly to be bronchial in origin . the present results are therefore in agreement with those of magnus ( 1939 ) in respect of the tissue of origin , without accepting his view regarding the intrabronchial papillomata . 
orr does not suggest that it is malignant ; the rate of growth is slow once the characbut there can be little doubt that a malignant teristic size has been attained . " variant " occasionally turns up . the role of antecedent inflammation . slye , holmes and wells ( 1914 ) thought that adenomata arise from areas of lung tissue in which inflammatory hyperplasia has occurred . grady and stewart ( 1940 ) consider that they are not associated with inflammation . 
the present author 's observations have convinced him that these tumours invariably originate in foci of chronic collapse inflammation , which become invaded by bronrchial epithelium , and that it is the extent of the original inflammatory focus which this would explain the paradox of its determines that of the formed adenoma . comparatively rapid appearance and slow subsequent growth . 
7. received for publication february 7 , 1947 . it is a widespread doctrine among students of cancer that any tissue or organ capable of cell division may be the site of a malignant neoplasm , but it is well known to clinicians that certain tumours , theoretically possible , do not in fact occur . 
the most striking example of an organ which never gives rise to a neonotwithstanding the fact that mitoses occur in the lens plasm is the lens . throughout life , having been seen even in the lenses of patients 80 years old , no tumour of the lens has ever been discovered . the lens is an entirely epithelial structure embryologically derived from the surface ectoderm , devoid of blood supply and enclosed in a semi - permeable although mammalian lenses are enclosed membrane , the hyaline lens capsule . during embryonic life in a capillary net ( the vascular lens capsule ) this does not constitute a blood supply , since the vessels do not come in contact with the lens in the majority of vertebrates cells , being always outside the hyaline capsule . the lens can therefore be looked even this embryonic vascular capsule is absent . on as a segregated group of specialized epithelial cells growing and differentiating in a closed system , separated alike from the blood - stream and from the surface of the body . 
by carefill dissection of the eyes it is possible to get the lenses in their hyaline capsules completely free from vascular capsule or uveal tissue . these lenses were inserted under the skin of the flank of mice of the same inbred strain together with methylcholanthrene . in some cases the hyaline capsules were ruptured and the lenses mixed with a few crystals of methylcholanin others the unruptured lenses coated with a solution of the threne . in others again teased lenses were mixed carcinogen in oil were used . with methylcholanthrene in solution in equal parts of soft and liquid the exact method employed did not appear to be important , paraffin . two of the tumours being obtained with a solution of 1 mg . 
the tumours appeared between two and three months after implantation . characteristics of tumrnours of lens epithelium . the tumours are anaplastic carcinomas possessing certain characteristics suggestive of their origin from the subcapsular epithelium of the lens . 
a brief consideration of the normal structure and behaviour of this in mice is a necessary preliminary to the study of the tumours . the normal lens and its epithelium is seen in fig . 
the first stage of this differentiation is the lengthening of the cell and the displacement of the once this has occurred the cell cannot divide again , but nucleus to one end . proceeds to complete differentiation into a lens fibre , the nucleus of which evenfig . 
4 and 5 show results at three and at two days . thle ruptured capsule is in culture of the whole lens of a late mouse embryo . the centre of the explant and is surrounded by degenerating lens fibres . 
the cells are large , with voluminous spherical or oval nuclei , showing one or more nucleoli and a prominent reticular chromatin in the young cells the nucleus is central , in structure . the older cells it moves to the edge of the cell just before becoming pyknotic . metastases occurring in the inguinal lymph nodes show the same structure , but with less necrosis . 
6 and 7 is apparent . extending edge showed fibrillar outgrowths somewhat similar to those described this by kirby in tissue cultures of chick lenses . fixed and stained preparation of a 5 - day tissue culture of the same tumour also these are seen in fig . 
1. received for publication february 23 , 1948 . in a previous communication we reported that a strain of the shope rabbit papilloma had been transmitted for 10 serial passages in the domestic rabbit ( selbie and robinson , 1947 )  . 
the adaptation of this tumour virus as a transmissible infection in domestic rabbits occurred during experiments in which the simultaneous inoculation of shope papilloma virus and sheep dermatitis virus in domestic rabbits produced papillomas that proved infective to other rabbits ( selbie , 1946 )  . 
the further passage of this virus in domestic rabbits was materially helped by continuing the procedure of mixing a second virus suspension with the infective inoculum of papilloma virus , and also by treating the skin with croton oil before inoculation , but there was no evidence of an increase in the virulence of the virus suspensions during passage . in the present communication we shall show that carcinomatous transformation has occurred regularly in this transmissible papillomatosis , and in a mamner similar to that found in the non - infective papillomatosis that is produced in domestic rabbits by the inoculation of extracts of papillomas from the cotton - tail rabbit , the original host of the shope papilloma virus . 
thus in all rabbits frqm passage 4 in table i , area 1 represents normal skin inoculated with a 10 per cent extract of papillomas , area 2 , normal skin inoculated with a mixed extract of papillomas and sheep dermatitis lesions , area 3 , skin pre - treated with croton oil and inoculated with a 10 per cent extract of papillomas , and area 4 , skin pre - treated with croton oil and inoculated with the mixed virus suspensions . rabbit 2 , passage 2 was inoculated with papilloma extract on normal skin only , and in rabbit 4 , passage 3 , the procedures for areas 1 and 3 were omitted . the rabbits were examined at weekly intervals from the 7th week onwards . the tumours were charted and their size was measured by callipers at regular intervals . 
as was noted in the earlier communication ( selbie and robinson , 1947 ) , there was a tendency for individual papillomas to unite during development , and in some instances papillomas regressed completely . 
hence in this communication only those papillomas that were recognizable as single entities at 6 months in areas with confluent or semi - confluent papillomatosis will be considered . only a few papillomas could be distinguished as independent entities at 6 months , and no accurate count could be made , so that a fair estimate was given of 30 papillomas for confluent papillomatosis and 20 for semi - confluent papillomatosis . it became apparent early in this investigation that if the development of individual papillomas was to be studied over a prolonged period , cancers which arose in adjoining papillomas should be removed . 
1 are shown the times at which carcinomatous growths were first detected in passages 2 to 7 , passage 9 being omitted because the surviving rabbits have been observed for only 40 weeks after inoculation . it will be seen that the passage rabbit 2 __ to ~~ * : 6s weeks after inoculation fig . 
1. - times of observations of carcinomas in all rabbits from the 2nd to the 7th passage . each rabbit is represented by a line indicating the period of observation from the 40th week blocked circles indicate carcinomas arising from papillomas on skin treated onwards . with croton oil before inoculation , and open circles indicate carcinomas arising from papillomas on untreated skin . x = removal by operation of all remaining papillomas . 
the time at which glandular metastases were observed varied with the time at which the primary carcinomatous growth occurred , the limits being 33 weeks after inoculation in rabbit 2 , passage 9 , and 89 weeks in rabbit 2 , passage 2 , while the average time was 67 weeks for all the rabbits in the series . 
to draw any definite conclusions from this series concerning the incidence of glandular metastases as many of the primary growths were removed , and in consequence the opportunity for metastases to occur was reduced . 
2 , area 2 , the central papilloma with a concurrent thickening of the base . had slowly enlarged from the time of its original appearance to attain a diameter nine weeks later it measured 1 * 8 cin diameter and of 1 - 4 cat 53 weeks . the base had now thickened and was fleshy in appearance and consistency , in three weeks later , at 65 contras , t to the dry horny surface shown in fig . 
19. the secondary deposits in glands and lungs have all proved to be of the in many of squamous cell type showing varying degrees of differentiation . the lung metastases it can be seen that the infiltrating carcinoma cells form nodules within the alveolar spaces , so that the stroma of the deposit retains the architectural structure of the lung tissue . 
the time at which this change first occurs has tended to become shorter in successive passages , and has been reduced to 45 and 28 weeks in single rabbits of the 7th and 9th passages respecthis may indicate an increase in the virulence of the virus , but it is more tively . likely to be due to variations in the sensitivity of the rabbits . it has also been shown that the first occurrence of carcinomatous transformation in a rabbit is usually followed by others up to at least 5 in number and up to 85 weeks after indeed carcinomatous transformation occurs so regularly in this inoculation . transmissible infection that it would appear that all papillomas would show this change , provided that their evolution was not interrupted by the death of the host or by other factors such as spontaneous regression , infiltration from nearbv carcinomatous growth , or operative removal . carcinomatous transformation should then be regarded as a natural stage in the development of infective papillomatosis , and attributable only to the activity of the virus which initiates the infection . it is also clear from the work of kidd and rous ( 1938a , 1938b ) and mcintosh and selbie ( 1940 ) , who observed rapid transformation to malignancy in tar - induced papillomas infected with shope papilloma virus , that this virus is capable of causing immediate carcinomatous change . it is not therefore necessary to postulate an extraneous precipitating factor such as bacterial infection or an alteration in the virus itself to account for the change to malignancy , as suggested by rous , beard and kidd ( 1936 )  . although carcinomatous transformation would appear to be a natural stage in the development of this infection , it presents such a radical change in behaviour that it is difficult to see how it could be part of a continuous process . 
robinson cidence of tar tumours in mouse skin was increased at the site of injury by deep incision , numerous investigators have demonstrated the enhancing effect of unspecific irritation on the tumour - producing activity of carcinogenic substances . that chemical agents can also have this stimulating effect was shown by twort and twort ( 1928 ) , who accelerated the production of tar tumours in mice by pretreatment with oleic acid , and by berenblum ( 1941a , 1941b ) , who obtained a higher proportion of mice with tumours after painting with a dilute solution of benzpyrene by concurrent treatment with croton oil or by applying croton oil after a limited course of benzpyrene treatment . 
the possibility then had to be considered whether the hereditary condition acted through genetically transmitted differences in ovarian functional activity , or through an unequal response of mammary glands or genital tract to ovarian hormone . 
numerous and extensive observations were made with somewhat conflicting results , both on the nature of the oestrous cycle and on variations in organ sensitivity to hormonal stimulation , in strains of mice with differing mammary cancer incidence . when the existence of the third factor , i.e. 
 it has been found ( elson and lamerton , 1949 ) that the protein content of the diet has a profound influence on the response of the , valk.er rat carcinoma 256 to x - radiation . 
two effects were considered to be concerned in this response : ( a ) the initial inhibition of tumour growth and ( b ) the elimination of the inhibited tumour and cure of the animal . 
 although variations occur within a group of animals maintained on a standard diet of fixed composition , the general type of response to a suitably fractionated in animals maintained on the 5 per x - ray treatment is illustrated in fig . 
growth may be nearly stopped for a consider able time , but the tumour usually begins to grow again , at first slowly in animals maintained on a 20 and then more rapidly , finally causing death . 
the rate at which it decreases in size is at first fairly rapid , but gradually becomes slower , and in many cases the animal is then able to rid itself entirely of the tumour by a " shelling out " process or sometimes by the gradual complete regression of the tumour . 
 a detailed histological and c : ytological examination of tumours , particularly under conditions presented by a and b , was therefore undertaken in an attempt to elucidate the part played by diet in influencing the ultimate response of these tumours to radiation . 
they were kept in individual cages , and maintained on the 20 per cent or the 5 per cent protein diet for at lea.st 7 * r - arch fellow of the xorwegian defence research establishment . 
15 c under these conditions the dosage rate at the centre of the tumour is about 140 r / m h~ tuhnique . - - cross sections of the implanted tumours were made by means of a special cutter with parallel kni , es giving a section of about 5 m thickness . 
 the conventional method of propagation of the walker carcinoma consists of the insertion of small pieces of tumour ( approximately 7 x 5 x 5 mm . ) under the skin of rats . 
although factors such as age , sex , weight , etc . , and general condition may account for some of this variation , it is probably mainly an expression of genotypic differences present in the colony from which the rats used in these experiments were drawn . 
 with our present routine for breeding and selection of animals for tumour implantation , when the tumours of a group of ten rats are measured 8 days after implantation the measurements show a distribution of i or 2 large tumours , about 5 medium - sized tumours and the rest considerably smaller . 
that this is largely the result of genetical variation is shown by comparison of the growth rates of tumours in litter mates and by implantation of similar sized pieces of tumour in both flanks of the same animal . 
the animals were divided into 4 groups , each group consisting of 4 litter mates , 2 male and 2 female ; they were killed 14 days after implantation and the weights of their tumours recorded . 
it is seen that the 3 most rapidly growing and largest tumours ( over 35 g . ) all occurred in group 1 , whilst in group 3 none of the tumours grew well . 
the growth rates of both tum , ours were remarkably similar , and if a tumour implant in one flank failed to grow the corresponding tumour in the opposite flank also failed . 
the average daily weight increase of rat.s maintained on our 20 per cent protein diet is about 3 to 4 : g . , whilst that of those maintained on our 5 per cent protein diet is less than 05 g . 
 weight of tumours 14 : days after implantation taken from 85 animals maintained on the 20 per cent protein diet was 24 : g . , whilst that of 86 animals maintained on the 5 per cent protein diet was 20 g . 
thus the ratio between the tumour weight.s on 20 and on 5 per cent protein diet is 12 , and the average growth rate of tumours is only about 20 per cent higher in anima1s maintained on high prot.ein than in those receiving a low protein diet . 
la.merton for comparison of the histology of tumour grafts in animals maintained on high and low protiein diets transverse sections were made through the tumour implants and their surrounding tissue 4 , 7 , 8 , 10 and 15 days after implantation . 
 it was found that 4 days after grafting the int , ensity of the inflammatory reaction as estimated by the number of cells of the reticulo - endothelium accumulated around the graft was great.er in rats maintained on the 5 per cent than in those on the 20 per cent prot , ein diet . 
on the other hand , the capsule of connective tissue was much more distinct in rats on the 20 per cent than on the 5 per cent prot , ein diet . 
the boundary of the tumour is well defined in rats on the 20 per cent prot , ein diei , the migration of tumour cells is negligible and the tumour grows by the very high rat.a of cell proliferation at the periphery of the tumour parenchyma . 
on the 5 per cent prot , ein diet , how ever , there is no definit , e tumour boundary and many isolated tumour cells can be seen scatt , ered amongst the loose , primitive network of connective tissue , which included in this " incomplet , e " capsule are also many surrounds the tumour . 
 during the early stages of the " take " and growth of the implanted tumours the reactions of the surrounding tissues may be very complex and int , erpretation of the exact course of events is difficult , but in older tumours the histological features of the process are much more clearly defined . 
the cell - elements ofthe capsule undergo progressive : fibrous differentiation , which can be clearly seen in high prot , ein diet rats with 10 to 15 - days - old tumours . 
the : fibrous nature of the capsule is much less obvious in animals maintained on a low prot , ein diet , and its clear demarcation is obscured by the migrating tumour cells . 
 it should be emphasized that on both diets there may be a considerable variation in the " take " of the graft and in the spread of the implanted tumour in the " host , and instances have occasionally been encount , ered in which the tumour graft took and grew more rapidly in animals maintained on low than in those fed on high prot , ein diet . 
such cases were , however , rare , and the effect of the diet is so marked that the differences in capsule - formation and organization between animals maintained on high and low prot , eins diets can easily be det , ected in most cases . 
 in the study of the reaction of the host rat to the implantation of tumour grafts the fact that , the tumour graft is itself growing may very often obscure the observations of the organization of the newly formed connective tissue capsule . 
 it was felt that the introduction into the subcutaneous tissues of a " passive " non - growing hetierologous tissue fragment such as muscle inst , ead of the " active " tumour fragment , would make it easier to analyse the influence of environmental factors , etc . , on the host reaction . 
 pieces of muscle of about the sam~ size as the usual tumour implants , taken from the leg of a second rat were implanted under the skin of the host animal . 
 305 in the mbsequent reaction to this muscle implant two phases could be clearly distinguished : ( a ) the inflammatory tissue response , ( b ) the formation of a capsule around the implant . 
 the in : oammatory reaction ( a ) is intense 3 days after implantation in rats receiving either the 20 per cent or 5 per cent protein diet , but in those main tained on the 20 per cent protein diet it rapidly subsides and has almost dis appeared 5 days after grafting . 
 the 5 per cent protein diet rats , however , still show persistence of the inflam matory reaction at a time when the capsule is already well developed in 20 per cent protein diet animals . 
it appears that the prolonged persistence of the inflammatory reaction around the implant is related to the absence of the connective tissue capsu1e , the development of which is impaired or delayed in animals maintained on a diet deficient in prote the evidence derived from the histological investigation of muscle implants thus supports the conclusion reached from the tumour implant experiments that while maintenence of th~ animals on a low protein diet has no deleterious influence on the inflammatory reaction to the implant , it does interfere to a very large extent with the organization and development of the connective tissue capsule . 
 a quantitative analysis of radiation - induced injuries in cells of the walker carcinoma is difficult owing to the large number of chromosomes ( 2n = 40 ) in the relatively small tumour cell . 
 injuries to the chromosomes can be detected only in ana - telc : , phase during which the lagging of ' " acentric " chromosome fragments ( segments without the centromere ) can be seen . 
13. - dividing tumour cell in late anaphase with three acentric fragments , one lying out of focus , 6 hours after 300 r , 5 per cent protein diet . 
27. - the same tumour ( l . ) , showing the active tumour cell island which lies beyond the periphery of the tumour which occupies the bottom right hand corner . 
28. - the same tumour ( l . ) at a higher magnification to show that tumour cells which were scattered in the loose connective tissue capsule form foci of renewed activity after irradiation . 
 a comparison has been made of the frequency of tumour cells with various cytological abnormalities , such as chromosome fragments , bridges and micro nuclei at different times after irradiation of a six - day old walker tumour in rats kept on high and low protein diets . 
the data obtained ( table i ) do not represent the full extent of the radiation injury resulting from any particular treat ment , since an unknown proportion of injuries undergo restitution before the cytological examination is made and are thus lost for analysis . 
moreover , the acentric chromosome fragments can only be seen when they lie freely in the cytoplasm , and consequently those fragments which are mixed up with the normal chromosomes and moved to the pole escape detection . 
a similar difficulty arises when we attempt to estimate the true extent of the radiation injury to cells by the number of micro nuclei , since some of the chromosome fragments may be included in the daughter nuclei and some of the micronuclei can contain more than one fragment . 
on the assumption , however , that the chance for such events is the same in all the samples , it is justifiable to use the quantitative differences shown by the data as a basis for comparing differences in cell behaviour which may be induced by maintaining the animals on different diets . 
 the data of table i shows that the greatest amount of injury was found in tumour samples taken 12 hours after irradiation , suggesting that these samples contained cells which were , at the time of irradiation in the most sensitive period of the mitotic cycje . 
it is inferred on experimental evidence , derived from x - rayed pollen grains and root - tips cells ( darlington and lacour , 1945 ) that the most sensitive period coincides with the duplication of the chromosome filament , which process marks the beginning of prophase . 
since the injury in the cells is at a maximum at 12 hours after both 100 and 300 r , we may conclude that the duration of mitotic suppression does not differ over this range of dosage . 
 the number of cells with chromosome injuries and with micronuclei was found to be already quite high in the 6 hours ' sample , suggesting that the time interval between treatment and the first appearance of chromosome fragments may be shorter than 6 hours . 
therefore some rats were killed 4 hours after treatment , but although both chromosome fragments and bridges were observed in this early sample , their frequency could not be estimated because the so - called " physiological " effects of radiation grossly interfered with the analysis ( mar quardt , 1938 ; koller , 1943 )  . 
l. - uierton the number of resting cells with micronuclei increases up to 24 hours after treatment , but at 72 hours such cells have almost disappeared from the tumour . 
 comparison of the results obtained at different times after irradiation with both 100 rand 300 r ( table i ) , in all samples except those taken after 12 hours , shows no significant difference in the number of cells injured or the number of chromosome fragments per cell , between animals maintained on high or low protein diets . 
 the inconsistent behaviour observed in the 12 - hour samples may be related to the fact that all the mitotic cells in this sample represent those cells which were in their most sensitive stat , e when irradiated . 
it was , therefore , felt that the results obtained with the 12 - hour samples could not be relied upon and should be disregarded in view of the consistent results obtained with all the other samples . 
it is thus possible to compare the length of the inter - mitotic period on the two diets in order to find whether the duration of the mitotic cvcle is altered bv the diet or not . 
 the greatest amount of injury are those which at the time of irradiation were at in the x - rayed \\ ' alker carcinoma the the beginning of prophase of mitosis . 
 greatest amount of injury is found in the - 12 - hour sample and consequently the duration of mitosis from prophase to the end of telophase cannot be longer than 12 hours ; the cycle of the second division ( from prophase to telophase ) would occupy another 12 hours , thus lea , ing 20 hours for the duration of the inter mitotic period , if an allowance of 4 hours is made for the time lost by the radiation induced mitotic suppression . 
thus we may conclude that the active cells in the \\ ' alker carcinoma have a mitotic cycle of the order of 32 hours ( 20 hours spent in resting and 12 hours in mit - 0sis ) : this agrees with data obtained in similar experi ments in which irradiation is replaced by radiomimetic chemicals , such as the nitrogen mustards ( koller , unpublished communication )  . 
 from the observations of the frequency of cells in second mitosis 48 and 72 hours after irradiation with 100 or 300 r there was no indication that diet affects the duration of the mitotic cycle . 
at 6 days after the radiation treatment tissue fibrosis was much more developed , and the connective tissue capsule could be clearly distinguished from the actual tumour , since no tumour cells were present in this capsule zone . 
 it does , however , contain islands of active tumour cells , which , since the growth - inhibiting effect of a single dose of 1000 r is usually only temporary , no doubt represent centres from which the renewed growth of the tumour develops . 
 in the animals receiving the 5 per cent protein diet , the loosely organized con nective tissue capsule , 3 days after 1000 r , was not undergoing fibrosis to the same extent as the capsule in the 20 per cent protein diet animals . 
 six days after irradiation the tumour boundary which was previously very ill defi.ned , becomes more distinct , presumably owing to the fact that some of those tumour cells which were scattered in the connective tissue network and have survived the radiation treatment , have now undergone proliferation and brought about the formation of a new continuous tumour parenchyma . 
 w ' hile a single dose of 1000 r may cause considerable inhibition of growth of the walker rat carcinoma , and the inhibition may last for several days , complete regression of the tumour rarely occurs . 
the experiments with the single dose have shown , however , that at least in the 20 per cent protein diet animals , whilst the extent and rate of histological changes induced in the capsule or tumour bed is very favourable , it is insufficient to enable the animal to effect a cure . 
it is obvious , therefore , that the amount of radiation injury in the tumour cells must be increased without at the same time adversely affecting the favourable tissue response . 
it was therefore decided to increase the dose to 4000 r , which is of the order employed in the radiotherapy of human cancer , and a suitable method of fractionation for applying this dose was devised based on observations of the response of tumour capsule and tumour bed obtained in the single dose experi ments . 
the method employed can be illustrated as follows : 1000 r 500 r , 500 r 500 r , 500 r 500 r 250 r 250 r , in which represents two consecutive days on which no treatment was given . 
lamerton for the histological investigations 15 rats were treated with this fractionated dose , 7 of them being maintained on the 20 per cent and 8 on the 5 per cent protein diet . 
 two rats of each diet group h 1 , h ! ( high protein ) and l 1 , l 2 ( low protein ) were selected for histological examination ; of the remaining rats 4 out of the 5 maindied " 's e .. 
h 1 and h , indicate animals maintained on high protein diet and li and l , animals maintained on low protein diet at the time they were killed for histological examination . 
from similar results obtained in previous experiments ( elson and lamerton , 1949 ) and from a com parison of the growth curves of the tumours selected for histological investigation with those of the remainder of the groups shown in fig . 
22 it is reasonable to suppose that animals h 1 and h 2 on the high protein diet would have been cured , whereas li and l 2 maintained on the low protein diet would not . 
those of the high protein diet animals ( h1 and hz ) , however , had grown to a considerable maximum size and were then regressing , whilst those of the low protein diet animals ( l1 and lz ) had shown earlier retardation of growth , but were beginning to assume a more rapid growth rate . 
the animals h 1 and li had received a total dose of 3000 r ( in 5 fractions ) , whereas hz and lz had received the foll total dose of 4000 r ( in 8 fractions )  . 
 in assessing the response of tumours to radiation two effects must be con sidered : ( i ) the initial inhibition of tumour growth and ( 2 ) the elimination of the inhibited tumour and cure of the animal . 
in work with the walker rat carcinoma 256 it has previously been shown that the diet of the animal has a definite influence on each of these processes ( elson and lamerton , 1949 )  . 
 dealing first with process ( i ) , it has been shown that maintenance of the animal on a low protein diet favours the immediate growth inhibitory response of the implanted walker rat carcinoma 256 to radiation . 
it might be thought that this diet effect is related to an increased sensitivity of dividing tumour ce ] ls to radiation induced in some manner by the poor protein diet . 
furthermore , we do not feel that such differences as have been revealed in the course of the histological investigation of the tumour bed reported here offer any very satisfactory explanation of the greater immediat.e tumour response in the low protein diet animals , and we are inclined to believe that some more fundamental biochemical relation is involved . 
lamerton investigations with carcinogenic chemicals have suggest , ed that these sub stances may inhibit cellular growth by interfering with the normal processes of protein synthesis ( elson and warren , 1947 ; elson , 1949 )  . 
h this is the case it might be expected that animals in which the full capacity for protein synthesis is already restricted by a deficient protein diet would probably show an immediate growth inhibitory response of both animal and tumour to treatment . 
with ample protein to furnish more than suffi cient amino acid " building blocks ' for the full efficiency of protein synthesis would not be expected to show such an immediate reaction . 
it is not unlikely that x - radiation may act in a similar way and in order to throw more light on this problem the protein metabolism of irradiated animals maintained . 
 of the walker rat carcinoma a high protein diet has been shown to be of great assistance to the animal in the process of elimination of the inhibited tumour and the replacement of the tumour area by healthy tissue . 
that in the case of the implanted walker rat carcinoma 256 the main effect of the high protein diet is to ensure the development of a well organized . , extensive capsule of connective tissue around the growing tumour . 
response to radiation treat ment the ill - defined tissue capsule zone does not undergo fibrosis in the same way as does the firm capsule of the high protein diet animals . 
altho~h its main mass usually becomes necrotic , new tumour growth often develops in the incomplete capsule zone , from cells which have escaped the lethal action of the radiation . 
on a diet deficient in prote the effect of addition to the low protein diet of substances such as amino acids , particularly cystine and methionine , amino sugars , etc . , which may conceivably be involved . 
 313 taking into consideration the connective tissue reaction , devised treatment methods for epitheliomata , in which the total dose is of the order of 3000 r , far below the so - called " standard tumour lethal dose . " also it has been shown by jolles and koller ( 1950 ) that the tumour bed reaction can be influenced by a method of fractionation of the dose in space as well as time to give favourable therapeutic resu.jts. 
 the present animal experiments have shown that the character and organization of the tumour bed can be influenced by nutritional factors , and suggest that suitable regulation of nutritional conditions , such as , for instance , supplying a high protein diet , or supplementing the diet by protein hydrolysates , etc . , and by increasing protein anabolism by hormone administration , etc . , may jead to improvements in clinical response . 
 the effect of the protein content of the diet on the establishment and growth of implants of the walker rat carcinoma 256 , and on the response of this tumour to x - radiation , has been investigated . 
 the nature and extent of the inflammatory reaction has been found to be similar in animals maintained on both high ( 20 per cent ) and low ( 5 per cent ) protein diets , but in the low protein diet animals it persists for a longer period after implantation owing to slower and less complete development of the connec tive tissue capsule . 
 in assessing the response of the tumour to radiation two effects have been considered , ( a ) the initial inhibition of tumour growth , which is favoured by a low protein diet , and ( b ) the elimination of the inhibited tumour which is favoured by a high protein diet . 
 histological investigation has suggested that the favourable effect of a high protein diet on the elimination of the tumour is related to the development of the well organized capsule of connective tissue around the growing tumour . 
radia tion treatment , besides inhibiting division of the tumour cells , also increases the fibrosis in this capsu.je , which aids in the eventual elimination of the damaged tumour . 
 we wish to express our thanks for grants supporting this investigation from the british empire cancer campaign , the anna fuller fund , the jane coffin childs memorial fund for medical research and the u.s. 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene into the flank and below a nipple in strain street mice ( rask - nielsen , 1948 )  . in both sites the injection induced only spindle - cell sarcomas and , in a few instances , squamous - cell carcinomas , but no mammary carcinomas . 
the ratio of cases of isolated thymic tumours to cases of generalized leukaemia was found to be 1 : 1 following injection into the flank and 1 : 5 following injection into the mammary region . 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene were performed . the leukaemic manifestations induced have been described in detail in a recent publication ( rask - nielsen , 1949 ) and the local tumours will be dealt with in the present paper . for the purpose of ascertaining whether the failing development of mammary carcinoma might be a phenomenon specific for injection of 9 : 10 - dimethyl - 1 : 2benzanthracene , mice of strain street were injected with 05 mg . 
of a mixture of the same hard and liquid paraffin as used in the analogous experiments with 9 : 10 - dimethyl - 1 : 2 - benzanthracene ( rask - nielsen , 1948 , 1949 )  . 
an equal number of females and males were injected into the flank , but only female mice were injected into the mammary region , except in a few 9 : 10 - dimethyl - 1 : 2benzanthracene experiments , where an equal number of each sex was used . more than half the experiments were carried out with litter mates , one half of each litter being left untreated as a control group . 
rask - nielsen sarcomas of a varying degree of differentiation ; a few were polymorphocellular , and a few rhabdomvosarcomas occurred . in the squamous - cell carcinomas marked cornification was a frequent finding ; no microscopic changes indicated that the growths might have originated in mammary tissue . 
however , the growths were considered to be most probably spontaneous and were , therefore , not included in table iii . following injection in the flank , spindle - cell sarcomas were induced by benzpyrene , dibenzanthracene , methylcholanthrene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 27 per cent , 50 per cent , 39 per cent and 12 per cent of the effective total of mice respectively . squamous - cell carcinomas were observed in the same experiment in 6 per cent , 7 per cent and 0 - 8 per cent following the injection of benzpyrene , methylcholanthrene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene respectivelv . 
as regards the application into the mammary region , spindle - cell sarcomas were observed following injection of benzpvrene , dibenzanthracene , methvlcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 4 per cent , 22 per cent , in this experiment , squamous - cell 37 per cent and 8 - 3 per cent respectively . carcinoma was observed in 2 per cent , 2 per cent , 22 per cent and 2 - 4 per cent respectively . the effective total of experimental mice is the number of mice living to be as old as the youngest tumour - bearing mouse , namely 4 months . the minimum , maximum and average latent period , the interval from the injection until death , is presented in table iv . 
the higher carcinogenicity of methylcholanthrene than of the other hydrocarbons apparent from the present experiments accords with previous findings ( greenstein , it accords also with the recent observation ( rask - nielsen , 1950a ) that 1947 )  . subcutaneous application of 0 - 02 mg . 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene was followed by leukaemic manifestations in 20 - 4 per cent with an average latent period of 20 to 25 weeks ( rask - nielsen , 1949 ) , injection of dibenzanthracene and methylocholanthrene had no accelerating effect on the development of leukamia , and the doubtful , extremely faint acceleration observed following injection of benzpyrene affected at any rate only the incidence ; not the latent period . the absence of leukaemic lesions following injection of the three last - mentioned hydrocarbons is all the more remarkable , as the development of leukaemia has been found to be accelerated following painting with benzyprene in dilute brown mice ( morton and mider , 1941 ) and in strain f mice ( kirschbaum and strong , 1942 ) following painting with dibenzanthracene , without , however , decreasing the latent period in strain f mice and with methylcholanthrene in strain f mice ( kirschbaum and strong , 1942 ) , in dilute brown mice ( mider and morton , 1939b ; morton and mider , 1941 ; lefevre , 1945 ) , in strains rf , and rf / ak ( mcendy , boon and furth , 1942 ) , in c3h mice ( kirschbaum , strong and gardner , 1940 ; morton and mider , 1941 ) , and in old and new buffalo mice painting with 9 : 10 - dimethyl - 1 : 2 - benzanthracene ( morton and mider , 1941 )  . also accelerated the development of leukaemia in aka mice ( engelbreth - holm and lefevre , 1941 ; lefevre , 1945 ) , in dilute brown mice ( engelbreth - holm and lefevre , 1941 ; law , 1941 ) , and in swiss mice ( law , 1941 )  . 
into the lung ( rask - nielsen , 1950a ) , and by the induction of only microscopically visible adenomas in mice , 4 - 11 months of age , injected with 05 mg . 
of benzpyrene , dibenzanthracene , methylcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene into the flank of strain street mice induced local spindle - cell sarcoma in 27 per cent , 50 per cent , 39 per cent and 12 per cent ; and squamous - cell carcinoma in 6 per cent , 0 per cent , 7 per cent and 0 - 8 per cent respectively . injection of the same hydrocarbons into the mammary region induced spindle - cell sarcoma in 4 per cent , 22 per cent , 37 per cent and 8 ' 3 per cent and squamous - cell carcinoma in 2 per cent , 2 per cent , 22 per cent and 2 - 4 per cent respectively . local mammary carcinoma was not induced . leukaemia developed following subcutaneous injection into the flank and into 132 r . 
rask - nielsen the mammary region of benzpyrene , dibenzanthracene , methylcholanthrene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 6 - 7 per cent , 1 - 2 per cent , 0 per cent and 20a4 per cent respectively . 
gunz. * from the department of radiotherapeutics , university of cambridqe . received for publication june 11 , 1949 . in previous publications ( gunz , 1948a ; b ) a technique of cultivating human leukaemic leucocytes in vitro was described , and the quantitative and cytological findings in untreated cultures made by it were analysed . 
he did not , however , determine the mitotic rates in his cultures , because of the small number of dividing cells present . osgood 's findings may be compared with those of schrek ( 1946a , b ) , who irradiated suspensions of thymus and spleen lymphocytes , and of bone marrow cells ( rabbit ) , and of normal and leukaemic human blood cells in " phosphate ringer solution " with and without homologous serum , with doses of x - rays of using as a criterion of survival a failure of cells to stain with a 20 - 4000 r . 1 : 1000 solution of eosin in tyrode solution , schrek found exposure to x - rays to cause a decreased survival time vitro in lymphocytes from the thymus , normal blood and four of five bloods from patients with chronic lymphatic leukaemia . such an effect was noted after a dose of 50 r , and increased with an increase in the dose up to 1000 r , remaining approximately constant at higher doses . 
the author , discussing possible reasons for this lack of effect , attributes it to an absence of dividing myeloid cells in his preparations , x - rays leaving resting myeloid cells unaffected . interference with mitosis , as a result of x - irradiation , was definitely demonstrated by rachmilewitz , rosin , goldhaber and doljanski ( 1945 , 1947 ) in experiments with fragments of explanted rabbit bone marrow . following the application of 250 - 1000 r there was a depression of mitosis lasting for two to four hours , with subsequent recovery . 
many mitotic abnormalities were caused , and the marrow became hypocelhular , or almost completely aplastic , according to the size of the dose given . the observations in the literature may be summarized by stating that x - rays have been found to damage blood and haemopoietic cells , especially lymphocytes and all classes of immature cells , when applied directly in vitro , and that disturbances of mitosis appear to be among the earliest signs of injury in cells so exposed . 
two patients had not received any x - ray treatment when first seen ; the others had had various amounts of treatment in the past . the technique of culture was that previously described ( gunz , 1948a )  . brief , it consisted of the distribution of small equal quantities of leukaemic leucocytes , suspended in the culture medium , over a series of culture tubes , and the withdrawal of some of the tubes for counting after varying periods of incubaat these times total and differential counts were made , and the total tion . number and phase distribution of mitoses determined . the culture medium used consisted either of 50 per cent dried , reconstituted human plasma , with the addition of 5 per cent rat embryo extract , or of 50 per cent fresh homologous human serum , both diluted in ringer solution . the duration of experiments was two days , and counts were done at 8 , 24 and 48 hours , unless otherwise stated . the technique of irradiation was as follows : after the cultures had been set up , they were incubated at 370 for about 15 minutes , to give them time to reach body temperature . in some experiments some of the tubes were also incubated for longer periods before irradiation . 
the tubes were exposed at two fixed distances ( approximately 21 and 81 cfrom the target ) , the dose rates , measured in air , at these points being 622 and 62r / nirespectively . 
the actual dose rate to which cells were exposed depended on three factors : the dose rate in air , the absorption and scatter due to the glass , and the absorption and scatter due to the fluid . 
the dose rate in air was measured by means of a victoreen dose meter in the normal way ; it was found that when the chamber of the dose meter was inserted into empty culture tubes , the average decrease in the dose rate was 6 - 5 per cent . this enabled a correction to be made for the glass of the tubes . 
the volume of the liquid being only of the order of 1 or 2 ml . , the correction for the absorption and scatter due to it would be less than 5 per cent , and was ignored in estimating the dose rate . 
the results of irradiation with 100 , 1000 , and 10 , 000 r are set out in tables i - vi . if the contents of tables i - vi be summarized and analysed , we obtain the following findings : immature cell8 . with a dose of 100 r the ratio , at 8 hours , of immature cells in irradiated to in five experiments it those in control cultures varied from 65 - 113 per cent . was greater , and in seven experiments less than 100 per cent . 
a significance in the analyses of immature cell counts test ( student 's t - test ) was employed . percentages were first converted to logarithms , in order to obtain a more normal distribution of the series . 
the actual formula used was t - s - - = where x is the arithmetic mean of the series , 8x its standard error , and m = log10100 = 2 . this gave a value of t = 0 * 97 , which is not significant . at 24 hours the ratio varied from 71 to 111 per cent . in four experiments it was greater , in one equal to , and in seven less than 100 per cent . 
the difference is not significant . at 48 hours the ratio varied from 48 to 112 per cent . in one experiment it was greater , and in ten experiments less than 100 per cent . 
from this t = 5 - 25 , and p is less than 0 * 001 . there was , therefore , a highly significant reduction in the number of immature cells in cultures 48 hours after irradiation with 100 r . with a dose of 1000 r the ratio , at 8 hours , of immature cells in irradiated to those in control cultures varied from 76 to 111 per cent . in three experiments it was greater , and in three experiments less than 100 per cent . 
no analysis was carried out for the 48 - hour values . with a dose of 1000 r the ratio was less than 100 per cent in all experiments , and at all times . 
no mitoses were present in irradiated cultures in 4 out of 7 experiments at 8 hours , in 5 out of 8 experiments at 24 hours , and in 4 out of 6 experiments at 48 hours . 
the results with 10 , 000 r were similar . it must be emphasized that these experiments were performed with varying culture media , and that the cells in some of them came from untreated , and in others from previously treated patients . this explains many of the numerical differences between individual experiments , particularly in the mitotic counts . however , in spite of the non - homogeneity of the material , the results show clearly the following points : irradiation of cultures of leucocytes from chronic myeloid leukaemias with 100 r produced a significant reduction in the number of dividing cells for at mitosis then recovered , and did not differ significantly from least 8 hours . controls at 24 hours or later . 
1. - in vitro irradiation of leucocytes ( chronic myeloid leukaemia )  . irradiation with 1000 and 10 , 000 r produced a more marked depression of mitosis at 8 hours , and this did not recover subsequently . 
at that stage there were practically no dividing cells present , and the vast majority of all immature leucocytes in the cultures were truly " resting . " only after the lapse of several hours could any considerable numbers of them be expected to be approaching or entering it is , however , well known that chromosomes are particularly liable mitosis . to damage from radiation in the late pre - mitotic or early mitotic stages ( lea , 1946 )  . 
the following experiments were made in an attempt to irradiate cells at such a moment of increased sensitivity to x - rays , and to determine whether chromosome abnormalities could thereby be induced . - ~~~~ _ ~~~ ~ ~~~~1 ' ~~~~~~~~~~~~~~~~~~~~~ 338 f . 
gunz effect of varying the time of irradiation . in two experiments different groups of tubes were irradiated with 100 r at 0 , 2 and 4 hours from the time of setting up the cultures . 
3 , from which it is clear that no significant difference in the mitotic rate or the number of immature cells was produced as a result of varying the time at which the cultures were irradiated by up to 4 hours ; neither was the number of mitotic abnormalities in stained films altered . in another group of three experiments cultures were irradiated with 100 or 1000 r 7 hours after they had been set up , and counts and filmns were made at it was known that at 7 hours , appreciable frequent intervals after irradiation . numbers of cells would be entering mitosis . 
4. - effect of x - rays on leukaemic leucoeytes in vitro . irradiation 7 hours after explanta ' tion . that they only appeared when cultures were irradiated at a time when many mitoses were present , suggests that they arose from dividing cells , and it is likely that they originated in early prophase . 
15. it would seem that the findings at 8 and 24 hours are most likely to reflect the character of the cells themselves ; later on , artefacts due to the composition of the medium become superadded . taking only the 8 - hour counts into consideration , there was a good correlation between the patient 's blood count and the number of mitoses in cultures . 
 ( 1945 ) for normal rabbit bone marrow , but these authors worked with a different culture technique . no evidence was found that 100 r produced different results when given at this is in agreement with the finding of lasnitzki ( 1946 ) different dose rates . that in cultures of chick fibroblasts the initial inhibition of mitosis was independent of the dose rate ( 9.3 - 103 r / min . ) for doses up to 100 r . 
the explanation in the present experiments is probably that with both the dose rates used ( 62 and 622 r / min . ) , the time of irradiation - 10 or 97 seconds - was short compared to the overall time required for mitosis ( 35 - 60 minutes )  . no significant increase in the number of mitotic abnormalities was found to follow irradiation of cultures . 
the explanation for this is not clear ; it is , however , possible that technical difficulties prevented the recognition of finer structural alterations , like chromosome breaks . when cultures were irradiated 7 hours after their start , it was found that many cells in mitosis at the moment of irradiation completed their division . this agrees with the observations of many other workers , such as strangeways and oakley ( 1923 ) , canti and donaldson ( 1926 ) , kemp and juul ( 1930 ) , and furthermore , with 1000 r , a new kind of breaking - down cell love ( 1931 )  . appeared 3 hours after irradiation , and rapidly increased in numbers . 
assuming , for instance , that a similar process took place in the irradiated spleen , we should expect a definite diminution in the number of new leukaemic cells produced in that organ ; moreover , any further similar treatments would repeat , and possibly augment the effect . 
one could therefore picture the manner in which x - rays cause the enlarged spleen to involute . it is , however , more difficult to account by this means for the fall in circulating leucocytes which is such a prominent feature of the response to local radiotherapy in leukaemia , or for the involution of distant leukaemic lesions which had not been directly irradiated ( for examples , see piney and riach , 1932 )  . 
some light may be thrown on the latter problem by the findings in section b of the experimental part . here it was seen that leukaemic leucocytes , taken from the peripheral blood , showed a dininished power of proliferation in vitro after therapeutic irradiation of the patient , and that this effect was reversed as the clinical effects of treatment began to wear off . it thus seemed as if the biological make - up of the cells had been changed by the treatment . 
koller these few instances are selected from many clinical and pathological findings to illustrate that the environment of tumours is of great importance , and must be taken into consideration when devising improvements in radiotherapeutic procedures . it may prove to be important not only in surgical and radiotherapeutic practice , but also as regards theoretical problems of oncology . 
the classical study of willis ( 1948 ) emphasizes the fact that potentially neoplastic tissue zone is much greater than the size of the initially appearing tumour would indicate , and brings forward evidence which lends support to the field - theory of the origin of cancer . 
thus the possibility that the " recurrence " of a tumour after surgical treatment may represent an entirely new cancerous change in a predisposed tissue , and is not due to the incomplete removal of the malignant growth , has to be considered . the aim of post - operative x - ray therapy is not only to destroy viable tumour cells which might have been left in situ , but also to reduce the chance of the occurrence of an entirely new malignant growth by producing gross alterations in the histological architecture of particular regions , showing a proneness to neoplasia , and to affect the substrate in which any malignant cell left in situ might progress and defeat the treatment . 
the importance of connective tissue and tumour - environment has also been stressed by vernoni ( 1948 ) , whose views on the connective - tissue role in carcinogenesis find support in recent research work . a better understanding of the behaviour of the connective tissue of the tumour - bed and stroma during and after radiation treatment leads to the revision of fundamental principles on which the rationale of treatment is based . 
the practical application of the latter in the radiotherapy of accessible tumours finds expression in a new technique , described as the " sieve or alternating chess - board method " ( jolles , 1949a )  . for the past two years this method has been tested on a small number of patients , yet the radiation response in these cases has shown characteristics which hitherto have not been seen in tumours irradiated by the usual conventional methods . 
the purpose of the present paper is to describe these phenomena , and to discuss their bearings on the destruction of malignant growth . the biological basis of radiation effects in tumours . the radiation - induced changes in the cellular and stromal part of the tumour may be summarized briefly as follows : the cellular injuries consist of diverse nuclear or chromosome injuries , as well as disturbances in cytoplasmic enzyme activity . 
the chromosome injuries manifest themselves during mitosis which follows treatment , and lead to cell death by the breakdown of the mitotic mechanisthe amount of chromosome injury and the number of injured radiation - induced enzyme disturcells show a direct dependence on the dose . bances , the extent of which also depends on the dose , either lead to reversible injuries , e.g. 
the recent investigations by bloom and jacobson ( 1948 ) , anderson ( 1949 ) , and warren and dixon ( 1949 ) , brought forward further evidence to show that radiation does not produce cell differentiation . in the stroma and tumour - bed two chief events can be distinguished : hypertrophy of the connective - tissue elements , and a reaction closely resembling inflammation . 
the first phenomenon mainly consists in an excessive deposition of intercellular collagen fibres ( fibrosis ) ; the second is represented by an invasion of lymphocytes , polymorphonuclear leucocytes and macrophages into the fine these changes network of connective tissue forming the stroma and tumour - bed . in the normal tissues naturally react on tumour cells and tissue ; the effects in the latter thus produced can be referred to , therefore , as " indirect radiation effects . " they must , however , be clearly distinguished from those " indirect " effects which are assumed to be brought about by injury to the blood supply ( desjardins , 1932 ; harvey , 1942 )  . failla , 1940 ; ellis , 1942 ; windeyer , 1942 ; the importance of the tumour - bed during treatment has been recognized by a great number of investigators ( russ , chambers and scott , 1921 ; kok and vorlaender , 1922 ; caspari , 1922 ; murphy , maisin and sturm , 1923 ; czepa , 1924 ; roussy , 1926 ; ewing , 1926 ; souttar , 1929 ; sugiura and cohen , 1939 ; jolles , 1946 , friedman , 1939 ; evidence was also obtained in various 1948 ; spear , 1946 ; windholz , 1947 )  . experiments which shows the influence of the tumour bed in the radiation response of tumours ( lasnitzki , 1947 ; elson and lamerton , 1949 ) , and it was found that by taking into consideration the " stroma - reaction " , treatment methods could be devised for individual tumours in which the total dose given did not exceed 2700 r ( koller and smithers , 1946 )  . 
in the interdependent tissue structures of tumour and tumour - bed , the different reactions ( cellular and intercellular , direct and indirect ) are knitted together and closely integrated . it was observed that the onset , degree and rate of these reactions vary greatly in different tumours . because the outcome of treatment depends on them , the total dose necessary for the destruction of tumours also varies within very wide limits ( 2700 r and this observation leads to the conclusion that on biological grounds the 9000 r )  . concept of a " standard tumour - lethal dose " is untenable . it is unnecessary , however , to stress that a minimal effective dose which is indispensable for the destruction of a tumour remains of paramount importance , and the enhancement of the effect of this minimal dose , by utilization of the indirect radiation effects , is here discussed . the various reactions induced by the radiation all contribute to the resolution and eventual disappearance of the tumour , therefore the reaction - system must be it is only by the analysis of all these factors and the study considered as a whole . of the behaviour of all tissue structures , that an explanation may be found either for the inadequate response , or for the recurrence of a particular tumour . 
the technique has been fully described in a previous communication ( jolles , 1949b )  . apart from the direct radiation transmitted through the " opaque " lead squares ( and which does not exceed 3 per cent with the thickness of lead used ) , the protected areas also receive a very small amount of scatter irradiation . latter is irregularly distributed , tailing off towards the centre of the protected this contingency must be taken into consideration when studying and areas . conmparing the radiation effects of the directly exposed and protected parts . biopsy specimens are taken simultaneously from the exposed and protected areas , preferably fronm the centre of these regions , and occasionally a third biopsy specimen is obtained by cutting across both the exposed and protected areas in order to follow the transitional stages of the histological changes due to radiation . the great variability of tumours in respect of the histological organization including the structure of stronia and tumour - bed , has to be kept in mind , and our observations were based only on biopsy material showing similarity in these respects . eighteen patients have been treated with the sieve technique , and the radiation reactions in the exposed and protected areas have been compared by the analysis of biopsy specimens . 
two sets of experiments were devised ; in the first instance only one sieve was used throughout the treatment . in the second set , two sieves a and b , were employed ; chess - board b differs from chess - board a in that the order of transparent and opaque squares is reversed . 
xi.48 : 4 days after start of treatment 28.xi.48 : 13 days after start of treatment 8.xii.48 : 23 days after start of treatment 16.xii.48 : 31 days after start of treatment 15 . 
the gland increased in size very slightly during treatment to the lesion on the temple . one month later the gland had grown to the size of a hazel - nut . 
lederman , the behaviour of over 450 accessible tumours has been analysed during and after treatment , and it was established that besides the injuries in dividing cells and the great increase in cytoplasmic volume of differentiating or maturing tumour cells , the most striking change occurs in the connective tissue of the stroma and tumour - bed , which may be described as tissue " fibrosis . " the connective tissue becomes more rigid in architecture , less flexible and adaptable for the development of the inflammatory reaction ( " coarse " tissue fibrosis )  . 
koller to state what is the primary cause of tissue changes in the protected areas ; i may be that the small amount of scatter radiation received in ten fractions o for that reasoi 40 r daily can produce such alterations in the connective tissue . further experiments are in progress to study the stromal effect of such a smal the experimental evidence so far available indicates that tissue reactioi dose . after a dose of this order is negligible ; if there is any , e.g. 
we are of the opinioi that the tissue changes in the protected regions are brought about by a complet mechanism in which , among others , a diffusible substance produced in the directli irradiated tissues might play a role . 
the absence of chromosome fragmentation is another proof that the alteration seen in the protected areas , such as the increase in the size of tumour cells , and the slight degree of fibrosis and inflammatory reaction , must be considered as an indirect reaction to radiation . our investigation has shown that the rate and degree of the indirect radiation reaction depends on the histological organization of stroma , and on the dose . on account of the differences in the histological architecture of tumours , the minimum effective dose varies from tumour to tumour . 
we found that in tumours in which the connective tissue is abundant the minimum effective dose is smaller than in tumours with scanty stroma . this is illustrated in case ii , in which the dosage used ( 2700 r actual dose in 35 days ) did not reach the critical minimum level necessary to produce a reaction of sufficient strength and efficiency in the scanty connective tissue of the " protected " tumour areas . 
on the other hand , the use of the sieve - technique has permitted the subsequent treatment of the residual tumour with a relatively high but adequate dose ( 4500 r actual dose in 18 days ) , because the histological texture of the skin , owing to the small size of the areas directly exposed to irradiation during the initial treatment has been left unimpaired , and could safely be subjected to such a high dose in the second treatment . the complexity of the various cellular and tissue interactions increases when further radiation is carried out through another " chess - board or sieve " in which the position of transparent and opaque areas is reversed . 
we found that while the connective tissue needs protection from excessive radiation , it requires a certain quantity of radiation and a specific distribution in time and space of this quantity in order to elaborate the radiationinduced reaction . 
the stroma and tumour - bed reactions , however , being too obvious to disregard completely , are referred to , but only as concomitant , " independent " events , which have no , or too little , bearing on the radiation response of the malignant growth itself . 
the most cursory histological study of tumours under radiation reveals the fact that the destruction of all malignant cells of the tumour parenchyma rarely , if ever , can it seems , therefore , be achieved by the " direct " action of a therapeutic dose . necessary and logical not only to admit the existence of an " indirect " effect , but to accept all the implications of the generic statement that the purpose of radiation is to kill a variable but significant proportion of active tumour cells , and at the same time to assist the local body defence system by inducing the various responses in the tumour - bed and stroma . it also follows that any view based on changes induced by radiation in some and not all tumour - tissue components is not comprehensive , and that the conclusions drawn from the study of cell behaviour alone are doubtful . 
on " cell count method " of glucksmann and co - workers that account the ( gluicksmann , 1941 , 1948 ; glucksmann and spear , 1945 ; gkicksmann and way , 1948 ) , which per se represents a contribution to radiobiological knowledge , is liable to be misleading when claims are being attached to it , such as that it provides an explanation for the variation of radiation response of tumours , predicts the outcome of treatment , and indicates the most appropriate treatment method , whether surgical or radiological , for a given case . the cell count method is biased by subjective selection and interpretation ; it disregards the great regional heterogeneity shown by tumours both in growth rate and histological organization , and the fact that a malignant growth is composed of tumour and stroma , which form one closely integrated unit . it is more than obvious that for that reason the application of the cell - count method to biopsy specimens taken after a " test dose " of radiation in order to decide whether a tumour be submitted for surgery or radiotherapy is of doubtful value ( glucksmann and way , 1948 )  . it has been stated by spear ( 1946 ) that " radiation affects any given cell of a complex tissue in at least two ways , first by direct action on the cell , and secondly by injuring neighbouring tissues , upon the healthy functioning of which the cell depends . " our investigation leads us to a similar conclusion that the direct cellular effects , e.g. 
fragmentation of chromosomes , represent only the initial phase , and that the most important factors responsible for the disorganization , regression and re - absorption of tumours during and after irradiation are the various , closely integrated and related reactions which are produced by the radiation in the connective tissue of tumour - bed and tumour stroma . the present investigation , in which the alternating chess - board method was employed , has shown the role of the connective - tissue reaction in the destruction of tumours and the way by which this reaction can be favourably influenced and modified . 
we have found that the fractionation of dose in time as well as in space , as carried out by the sieve , induces specific changes in cells and tissues . the intensity and rate of these changes affects the whole architecture of stroma and tumour - bed as well as that of the tumour . our investigation has also shown that when the sieve is used sufficient response can be produced in the local defence system of connective tissue , and can be maintained by a much smaller dose than usually employed . 
roller us in cases where the tumour is radio - resistant , either by its nature or by its environment , to deliver a higher total tumour - dose without the danger of destroyit is our intention to investigate the ing vital structures of the tumour - bed . potentialities of this new procedure by applying the sieve method for the treatment of radio - resistant and deep - seated tumours , especially metastatic deposits in lymph nodes . 
the tumour is divided into a number of " exposed " and " protected " areas , the former receiving direct , the latter receiving only a small amount of scatter and transmitted radiation . 
two chess - boards or sieves , which differ in the order of the transparent ( exposed ) and opaque ( protected ) squares , can be used during treatment . irradiation induces injuries in the tumour cells and alterations in the connective tissue of the tumour - bed and stroma . 
the radiation reaction in the connective tissue plays a very important role in the destruction and reabsorption of tumours . in tumours irradiated through the sieve it was observed that tissue - reaction is reduced in the directly " exposed " regions , but at the same time , fibrosis and inflammatory reactions are induced in the " protected " regions . 
no cellular injuries , due to direct radiation such as chromosome fragmentation , were seen in cells of the " protected " areas . by using two sieves which differ in the order of the " transparent " and " opaque " areas , the reaction of the tumour - bed and stroma in the presence of abundant connective tissue becomes uniform throughout the tumour , irrespective of the different doses which regions may have received during treatment . analysis of the radiation reaction in tumours treated by the sieve has shown that fractionation of dose in time as well as in space induces injuries and specific alterations in the irradiated area , the rate and type of which greatly enhances tumour destruction . the authors are indebted to the british empire cancer campaign for a grant for technical assistance , and thanks are also due to f . 
levvis. from the chemi8try department , university of adelaide . received for publication may 23 , 1952 . soon after the discovery of the carcinogenic activity of 1 : 2 : 5 : 6 - dibenzanthracene by cook , kennaway and colleagues , yoshida ( 1932 , 1933 , 1934 ) and sasaki and yoshida ( 1935 ) reported that the addition of o - aminoazotoluene to the food leads to the production of malignant liver tumours in rats . during the past two decades scores of other azocompounds have been tested for carcinogenic activity of this type and many have been shown to be active . for reviews see shear ( 1937 ) , kinosita ( 1937 ) , cook ( 1939 , 1943 , 1948 ) , cook and kennaway ( 1938 )  . these carcinogenic azocompounds form a very interesting group . 
unhke the polycyclic aromatic hydrocarbons , they do not , as a rule , produce tumours at the site of injection , but mostly affect the liver . furthermore , the induction of liver tumours with azocompounds is markedl influenced bv the dieb , and if a cc protective " diet is supplied , the production of tumours can be strongly inhibited or even entirely prevented . all the azocompounds are , of course , artificial synthetic substances ; and they are highly coloured ( mainly orange to red )  . 
some are used as textile dyestuffs , and certain members of the group are used for colouring foodstuffs . the most part such compounds are probably harmless ( cook , 1948 )  . 
most of the food - colouring matters which have been tested have failed to induce liver tumours in rats ; and in any case it is most unlikely that anyone could ever consume enough of an azocompound in food to have any deleterious effect . 
to some extent the compound is also carcinogenic towards the bladder ( yoshida , 1935 ) , and it is interesting that the deaminated compound , namely 2 : 3 ' - azotoluene ( iii ) , was found to be non - carcinogenic to the liver of the rat , but produced numerous papillomas in the bladder ( otsuka and nagao , 1936 )  . many derivatives of azobenzene , containing substituent aminoand methylgroups , were tested for carcinogenic activity by kinosita ( 1937 )  . 
none of these produced cancer of the liver except o - aminoazotoluene , its mono - acetyland diacetylderivatives , and an isomer of o - aminoazotoluene , namely 4 - dimethylaminoazobenzene ( iv )  . 
the latter compound , which is also known as p - dimethylaminoazobenzene , and as n , n - dimethyl - p - aminoazobenzene , was formerly used as a food - colouring matter under the name of " butter yellow "  . 
the effects of such structural alterations are described in a following section . most of the known carcinogenic azocompounds are derivatives of 4 - dimethylnevertheless , a 4 - aminoaminoazobenzene , or at least of 4 - aminoazobenzene . this was shown for example , by group is not essential for activity of this type . cook , hewett , kennaway and kennaway ( 1940 ) , who examined the action of azonaphthalenes on mice . 
manv liver tumours , mostly of the type of cholangioma , were obtained with 2 : 2 ' - azonaphthalene ( vi ) , and a few tumours were obtained with 1 : 1 ' - azonaphthalene ( vii )  . 
lewis the same relative potencies do not always apply in other laborat - ory animals . it is well known , for example , that 4 - dimethylaminoazobenzene is much less active in producing ' hver tumours in mice than it is in rats . 
cohen. from the experimental oncology laboratory , radiation therapy department , johannesburg general hospital . received for publication february 7 , 1953 . an apparent discrepancy exists between the multiplicity of experimental cancer cures which have appeared in the literature since homologous transmission of tumours was first demonstrated , and the difficulties encountered in the therapy of human cancer . 
among the basic reasons for this are differences in the hosttumour relationship which presents a range of characteristics , from the completely unstable heterologous relationship , where the host and tumour are of different strains , or even species , to the relatively stable situation , as with human between these two extremes are the many , now or other autogenous tumours . widely used , homologous tumours displaying varying degrees of stability . 
the facile experimental cure , or spontaneous regression of a tumour followed by absolute immunity to further implants , is invariably a feature of the relatively unstable host - tumour relationship , and the less stable this relationship the more since this effective the " cure , " be it mechanical , chemical or radiological . propitious situation rarely , if ever , occurs in humans bearing autogenous tumours , experimental investigation of an animal tumour can have at best only remote application to clinical cancer therapy unless it applies in the first instance to a stable host - tumour relationship . 
as a prerequisite to any such investigation , therefore , the following criteria for stability of the host - tumour relationship are considered indispensable : ( 1 ) there shall be unequivocal evidence of malignancy , characterised by progressive growth , invasion or metastasis , and death of the host . ( 2 ) the tumour shall be genetically compatible with the host , either having arisen spontaneously or been induced in the tissues of the animal being investigated , or be transmitted by implantation into a homologous animal closely related by inbreeding to the host in which the tumour first arose . ( 3 ) the tumour shall " take " in practically 100 per cent of recipients on irnplantation , and there shall be neither spontaneous regression nor regression induced by non - specific trauma or intoxication of the host . ( 4 ) on irradiation of the tumour in situ , the curative dose shall be of the same order of magnitude as that of human tumours ( 103 to 104 r )  . ( 5 ) removal or destruction of the tumour in situ shall not evoke absolute resistanoe to further implants of the same tumour . since both human and experimental arlimal tumours can be made to regress following exposure to ionising radiations , one of the more promising avenues of 232 a . 
cohen research would appear to be the investigation of all factors affecting the radioalthough earlier work in this field has formulated certain sensitivity of tumours . fundamental principles ( krebs , 1929 ; cramer , 1932 ; crabtree and cramer , 1934 ; sugiura , 1937 ; sugiura and cohen , 1939 ; goldfeder , 1942 ) , it has been largely limited by inaccurate dosage estimation or lack of suitable biologic it is now possible for the radiobiologist to combine precise quantitamaterials . tive radiotherapy with a judicious choice of experimental hosts and tumours ; and it was with this in mind that a study of the radiobiology of the c3h mouse mammary adenocarcinoma was undertaken . 
with no added filters ( the inherent filtration of the tube - head consisting of approximately 3 moil and 1 mbakelite in addition to the glass envelope ) , giving a half - value layer of 0 34 mcu . 
of 25 cthe dose rate was 500 r / m ( 3 per cent ) measured in air . dose rates were measured in air with a secondary standard ( victoreen ) dosemeter , and corrected for atmospheric density . 
when completely filled with tissue fragments this arrangement provides full back - scatter for the field used , and avoids any heterogeneity due to variations in density or atomic number such as would be encountered with a glass slide . 
the tumour is relatively radioresistant , requiring doses of the order of 6000 r in one treatment to produce a significant number of this is essentially similar to goldfeder 's findings ( 1951 )  . 
the discrepancy isprobably due to ionisation contributed by the glass slide in which her tumour fragments were irradiated , instead of the plastic used in this experiment . it is of interest to note that the effective dosage for some other strains of mouse mammary carcinomas irradiated prior to implantation are of a similar magnitude ( lawrence , horn and strong , 1937 ; reinhard , goltz and warner , 1952 )  . considering that their more heavily filtered radiation ( hvl 1 mcu . ) has a relative biological efficiency of about four - fifths of that used in this experiment , the reported effective dosage of 3600 r is virtually identical with our findings . the results of both types of irradiation are analysed graphically in fig . 
2 using the " probit " method , from which it can be deduced that , in the case of treatment in situ ( line a ) the ld50 is 5700 ( + 140 * ) r , and for attenuation prior to implantation ( line b ) the ld50 is 2850 ( i 50 * ) r . it will be noted that the two dosage - response lines are apparently parallel , their slopes corresponding in both cases to a coefficient of variation of about 9 per cent . attenuation of tumour homoplasts by x rays prior to implantation into animals was described as early as 1909 by haaland . 
on occasion , this procedure was shown to induce a state in which the recipient became resistant to challenge with unirradiated implants of the same tumour , although rarely were adequately inbred strains immunised against homologous carcinoma ( hauschka , 1952 )  . 
the conversion of the cohesive subcutaneous tumour forms into a homogenous suspension of free cells may be due either to a selective proliferation of a few round cells present in the solid tumour or to a gradual adaptation to their new environment of the original spindle or polymorphous cells typical of sarcomas . 
two mouse ascites tumours were used for the experiments , the s 37 sarcoma and the t 2146 tumour which originated as a benzpyrene induced epithelioma but has both these tumours were developed since undergone sarcomatous transformation . from the subcutaneous form by craigie at the imperial cancer research fund laboratories . the paper is divided into three parts : i . 
no tumour smears of cell suspensions were nodules were present in the abdominal cavity . obtained by withdrawing peritoneal fluid at daily intervals from 24 inoculated mice and staining either by the feulgen method or that of papanicolaou . 
the whole of the ascites fluid was withdrawn and centrifuged at low speed for 3 minutes , which caused the heavier tumour cells to sink down while leucocytes and erythrocytes , if present , formed a top layer which could easily be removed with the supernatant fluid . 
the culture medium consisted of equal parts of fowl plasma , ascites fluid and chick embryo extract to which one drop of either s 37 or t 2146 tumour cell suspension was added . 
the undulating movements of the peripheral cytoplasmic area become more rapid , spikes and blunt processes are pushed out and withdrawn in quick succession . finally the cells elongate and assume pear and then spindle shape . for several hours after incubation the process may be reversed and spindle cells are seen to return to the round shape . examination of the fixed and stained specimens confirms the observations made on the living cells and shows that the process of transformation continues for 24 hours after incubation . 
the latter may represent a differentiated form which can no longer proliferate actively in contrast to the free round elements from which they are derived . to decide this question cultures of ascites tumour cells were inoculated subcutaneously into mice before and after 24 hours ' incubation , i.e. , before and after establishment of the spindle forms . 
the clots were cut into strips 2 x 4 min size containing approximately 2000 cells , and these were inoculated subcutaneously into the flank of c3h mice 2 - 3 months old . 
and that mitosis is only a third of that found in round cell grafts . after 24 hours the elongated cells revert to the round form but mitosis remains low until the fourth day ( fig . 31 , dotted line )  . 
the development of the implants can be followed from an early stage , and is described from 5 hours after inoculation until the fourth grafts derived from spindle cells showed a lower mitotic rate day of growth . after 5 hours in vivo , a significant delay in the appearance of tumours , and were of smaller size as compared with tumours obtained from round cells . 
3 , and the cancer re8earch laboratories , department cf pathology , the medical sclwol , birmingham , 15 . received for publication may 28 , 1952 . the experiments recorded in this article were carried out in the course of investigations on behalf of the medical research council , a sub - committee having been set up in 1949 to inquire into the careinogeiuc properties of mineral oils and allied products . 
the arrangements for co - ordinating the research have been briefly described by auld ( 1950 )  . the entire series of tests have been made in duphcate at the cancer research laboratories , department of pathology , university of birmingham , and at , the chester beatty research institute , the royal cancer hospital , london . 
at each centre the activity of 3 selected crude oils 4 fractions derived from each crude by methods of distiration specially designed to avoid high temperature cracking , and the final residues , have been tested on groups of 50 mice for each sample and also on a total of 105 rabbits . 
he had already shown ( berenblum , 1945a ) that tumours were readily elicited on the rabbit by 9 : 10 - dimethyl - i : 2 - benzanthraceiie , which was found to be more potent to rabbits than to rats or guinea - pigs , in which positive results were , however , obtained ( berenblum , 1945b )  . 
he also subsequently observed ( 1947 ) that this hyd - r - ocarbon when injected subcutaneously did not induce rabbit tumours , tbough rats and guinea - pigs responded by this method . 
much earlier , oberling , sannie ' , guerin and guerin ( 1937 ) had shown that a i per cent solution of 3 : 4 - benzpyrene in benzene was active on rabbits ' skins , and berenblum ( 1945a ) observed that 9 : 10 - dimethyl - i : 2 - benzanthracene was much more active than benzpyrene at a similar ( o 5 per cent ) concentration . experiments using a high boiling fraction of mineral oil from an experimental catalytic cracking operatiori have recently been carried out by smith , sunderland and sugiura ( 1951 ) , testing the residue after removing the lower boiling naphtha and li - aht aas oil cuts , upon mice , rats , guinea - pigs , rabbits and rhesus monkeys . the rats and guinea - pigs were found to be refractory to skin applications but papillomata were elicited in all of the 6 monkeys , 2 being proved cancerous by papillomata were produced on biopsy 4 years after the start of the experiment . the inner surface of the ears of the 21 rabbits within 100 days . 
the number and size of such growths tended to increase during the 2 years in which painting was continued , and in 3 of the 6 surviving animals cancerous changes in the growths for tests on the type of material which they intended to study , were observed . namely , samples containing oils which had been subjected to a process of fluid catalysis up to 950 ' f . 
at birminorham they were selected , 25 of each sex froni an outbred laboratory albino strain previously employed in grading a series of oil fractions ( woodhouse and irwin , 1950 )  . in london the mice used were from laboratory stocks randomised so that each group of 50 contained some of each colour and genetic constitution . 
they were housed in fairly small cages of usual type and fed on greens alternated with crushed oats and a little bran . applications of the oils to patches of skin about 3 csquare from which the hair had been removed by electric clippers were made twice weekly . six areas on each of 30 animals were used for testing the 3 crudes , and 75 animals were used for the 15 derived fractions employing 7 areas on each animal . 
the 6 areas comprised the 2 ears , left and right thoracic , and the left and right lateral abdominal . the seventh area was the inter - scapular reorion . these sites are shown in fig . 
irwin ( medical research council 's statistical research unit , university of london ) , so that a statistical evaluation of the effects of site variation and differences in response by the individual animals might be possible . it will be apparent that each crude was applied to 60 sites and each of the other fractions to 35 sites . appheations were made twice weekly using approximately 0 3 ml . 
woodhouse in contrast , there was a total of 61 tumour - bearing rabbit sites in the birmingham series and 39 in the london series out of a possible 705 sites in each case , or , excluding the crudes and residues , which altogether yielded only 4 tumours ( london series ) , the remaining 12 fractions produced 61 and 35 tumours in the birmingham and london sen ' es respectively on a possible 420 sites . 
the cultures were grown by the hanging - drop technique in a medium consisting of equal parts of fowl plasma and 15 per cent chick embryo extract in ty - rode solution . 
the explants were subcultured every 48 hours for 4 passages to obtain as uniform growth as possible . fresh embryo extract was groups of cultures , each from the 4th passage , were selected and matched used . and used for experimental material and controls . 
agent were observed on the unfixed living cells in culture by cine - photomicrography . for most of the work we used apparatus modified from that described by willmer ( 1933 )  . recently , in collaboration with a . 
hughes of the department of anatomy , we have recorded the effects on the living cells by phase - contrast cine ' - photomicrography , using the techniques described by hugbes ( 1949 , 1952 )  . phase contrast microscopy has been used in a few cases to observe directly the effects of the chemicals on the living cells in culture . ( ii ) radiological details . the primary x - radiation used was of equivalent wave - length 0 - 221k , as deduced from the h.v.l. 
the nominal dose rate , which was always measured within + 2 per cent was in the reaion of 2oor per minute at distance 40 cfrom the focus , and was varied by altering the distance . 
the quality of the radiation was unchainged throughout these experiments , so that the probleof the exact value of the ionisation in the cells of the culture near the surface of the glass coverslip is not of importance here . in the cultures used most of the mitotic cells coudted lie between the glass surface and a distance 201i from it , so that the ionisation in the cells is increased by photo - electrons arising in the glass , probably by a factor in the region of 2 ( spiers , 1949 )  . 
3 , 4 , 5 . - effect of tetra - sodiuni 2 - mothyl - 1 : 4 - naphthohydroquinone cliphosphate ( compound i ) on a living resting cell of a chick fibroblast culture of the fourth passage , 24 hours old . phase - contrast c ' me ' - photomicrographs , taken by a . 
the doses were given in a fixed time , 2 - 00 minutes , except in the case of tlle three points marked , for which the radiation was delivered at 200 r per minute . the mitotic inhibition in probits is plotted against log dos - , ( finney , 1947 ; fisher and yates , 1948 ) there is no indication of departure from a linear relatiodbetween mitotic inhibition in probits and log dose . it is concluded that the relation between iiiitotic inhibition and the radiation dose plotted on a logarithmic scale is a sigmoid curve . 
the dose corresponding to 50 per cent mitot - ic inhibition after 6 hours is 315 the calculated regressiod line gives a sa - tisfactory fit . the calculation of the regression line is somewhat laborious . the mitotic inhibition produced by compound i in the chick fibroblast cultures has been studied in some detail after 24 hours ' application . 
the calculated regression line gives a satisfactory fit . there is no indication of departure from a linear relation between mitotic inhibition in probits and the logarithm of the concentration . thus there is a sigmoid relation between mitotic inhibition and the applied confor 50 per cent mitotic inhibition after 24 hours the concentration centration . of i is 3 - 81 0.15 x 10 - 6molar . for most of the compounds studied such accuracy is not necessary . tt is justifiable to deduce the approximate concentration required to give 50 per cent mitotic inhibition from the curve fitted by eye to relate the observed percentage mitotic inhibition to the molar concentration plotted on a log scale . in the case of compound i this method gave a value of 3 - 84 x 10 - 6m . the first experiments on the antimitotic effects of x - rays and i in chick fibroblast cultures ( mitcher and simon - reuss ' 1947 ) showed much greater mitotic inhibition with the combination of 3 x 10 - 6mcompound and 244 r of x - radiation delivered 18 hours later with fixation and counting after a further period of 6 hours , than with the same amounts of the two agents separately . to test for potentiation rigorously , it is essential to compare the effect of a combination of half amounts ( or other suitable mixtures ) of the two agents with the mean effect of the agents acting independently . this method , which may be termed the summation , method , is well recognised in pharmacology , and has already been applied in radiobiology by liechti and muller ( 1936 ) , gray and read ( 1944 ) , and mitchell ( 1947 )  . our original experiments showed a combined effect of 86 - 7 per cent mitotic inhibition , while the corresponding mean ' calculated for the two agents separately from the regression lines in fig . 
i and 2 , is 78 - 6 per cent . this result suggests that there is at least additivity of the effects , but it does not provide evidence for potentiation . in other experiments , the combined effect of 2 x 10 - 6mcompound followed 310 j . 
the combination of 2 x 10 - 6mcompound followed after 18 hours by 200 r of x - radiation produced 93 - 25 per cent mitotic inhibition after 24 hours . froni the number of mitoses in the individual cultures it is found that for 8 degrees of freedom student 's t is 15 - 71 , so that p is much less thlan - 001 . in this experiment , as in table 1 , the highest values of the mitotic inhibition were associated with no significant reduction of the area of the outgrowth . this finding confirms the unimportance of cell migration under the experimental conditions of the combined action of x - rays and the compound 1 . the possibility of differences in the behaviour of the outgrowth and of the central part of the culture has been , studied by means of the counts made in serial sections of 24 - hour cu - itures . 
 - the method is a laborious one ; by its use , fischer and parker ( 1929 . ) showed that in chick periosteal fibroblasts , the proportion of cells in mitosis was 0 - 79 per cent in the outgrowth , but only about 0 - 09 in our cultures - as in those of jacoby ( 19371 ) - the per ceiit in the central part . mitoses in the central part are limited to the " perichondxium " on its surfaces . studies of the topographical distribution of mitoses in our cultures by a . 
f. phillips showed no appreciable decrease in the number of cells in mitosis per unit the area of the central part is usually area as the central part is approached . not more than 20 per cent of the total area of the culture . in the serial sections of the cultures the central part is easily defined . 
the resting and mitotic cells were counted in the surface layers . in the sections of a control culture , out of 6205 cells counted there were 53 cells in mitosis , of which 13 were in prophase , 31 in metaphase , 3 in anaphase and 6 in telophase . 
at 24 hours after the application of 5 x 10 - 6mcompound 1 , out of 6220 ceus counted , there were 26 cells in mitosis ; of these i was in prophase , 19 were in metaphase , none were in anaphase and 6 were in telophase . 
simon - re ] utss cytological effects . tlio cytological changes produced by compound i in the chick fibi - oblast perhaps the most cultures differ in some ways from those produced by x - rays . fundamental difference is that anaphase bridges are only rarely produced by ' the compound , unlike x - rays . after the application of compound i to the hving cers , the first change observed is temporary cell enlargement , presumably due at least in part to hydration ( " cell oedema " )  . this does not occur with 5 x 10 - 7mconcentration , but has been observed in its early stages at 2 minutes after application of the compound in concentration 5 x 10 - 6m . 
the change is obvious after 5 minutes and probably affects the cytoplasm first . after 10 minutes the effects are still increasing ; ' there is bubbling of the enlarged cytoplasm and enlargement of the mitochondria , nucleus and nucloolus . 
the slight transient shrinkage of the cell immediately after addit - ion of the compound is observed consistently . at the maximum of the cell enlargemei - it the increase in transverse dimensions of the cells is often in the region of 50 per ' cent . mitotic inhibition is obvious after 80 minutes and persists after 24 and 36 counts show that there is no appreciable change in the distribution of hours . the phases of mitosis even in high concentrations such as 5 x 10 5m where mitotic inhibition is almost complete . example at 4 x 10 - 6mconcentration the abnormal mitoses increased slowly from about 5 per cent of the total mitotic count after 80 minutes to about 15 per cent after 24 hours . 
a typical count of the mitotic abnormalities is included in table il and photomicrographs of examples of the abnormal cells after fixation are enlargement of some of the dividing cells is shown in fig . 
2 x 10 - 6m  . compound i followed after 18 hr . by 150 r x - radiation * also 1 tripolar met - aphase . i and x - radiation shows potentiation of chromosome fragmentation . this finding is of particular interest in connection with possible radiotherapeutic applications . instability of compound i in solution . studies of the thermal instability of compound i in aqueous solution were made because of erratic results in animal experiments and clinical trials . 
for 7 days almost completely destroys the antimitotic activity and produces a rather toxic - solution . there is no significant mitotic inhibition , but the outgrowth is poor , many of the resting cells are vacuolated , disconnected and rounded and - a large number of the cells in metaphase show gross chromosome clumpiaig . there is progressive reduction of the mitotic ' hibition + 4 - 1 314 s . 
the outgrowth ig poor , many of the resting cells are rounded , there is some accumulation in metaphase and a number of exploded cells ; there is wide it seems likely that there are variation in the behaviour of different cultures . several unstable intermediate products involved in the process of inactivation of compound i by incubation at 39 ' c . 
experiments. tetra - sodium 2 - methyl - 1 : 4 - naphthohydroquinone diphosphate ( compound 1 ) it is found that there is no has been studied in detail as a reference substance . indication of departure from a linear relation be - tween mitotic inhibition in probits accordingly it is sugand the logarithm of the concentration of the compound . gested that the best estimate of the activity of the compound is the concentration which produces 50 per cent mitotic inhibition under the experimental conditions . this concentration may be termed mi 50 as a convenient abbreviation . 
for compound 1 , there is no indication of departure from a linear relation between the rnitotic inhibition in probits and the logarithm of the concentration . for 50 per cent mitotic inhibition after 24 hours , the concentration is 3 - 81 0 . 
not only has the type of therapy most likely to achieve success been the subject of dispute , but also the same measures in the hands of well - known authorities have produced a wide variation in results . 
have we a classification which accomplishes this ? the outlook for a patient with cancer of the breast depends first and foremost upon the degree of malignancy of the tumour and upon its extent . 
it is a wide belief that the prognosis is also influenced by certain other features , but the value of these is open to que ! rtion and will form the subject of a separate inquiry . 
 suffice here to state that such factors as age of patient , site of tumour in the breast , size of primary growth and duration of symptoms were not found , per se , to influence the outlook materiallv . 
 _ - \ttempts have been made in the past to group patients with breast cancer according to histological criteria which , it has been claimed , give some indication as to the degree of malignancy of the tumour . 
 the other is based upon a system of grading , wbilst the results of the former have largely proved disappointing , conflicting views exist as to the value of the latter . 
 it is the prime object of this paper to investigate the significance of the grade of malignancy in mammary cancer in an attempt to establish a more accurate system of classifying patients with this disease . 
 there is great difficulty at the present time in deciding on the line of action to adopt in view of the widely different procedure . ; , advocated by different authorities . 
 , vhilst gordon - taylor ( 1948 ) and cade ( 1948 ) believe radical mastec tomy alone to be the most suitable treatment for these patients , riddell ( 1948 ) and also richards ( 1948 ) advocate ancillary radiotherapy . 
it is now over fifty , ears since : moore of london conceived and introduced the radica.l mastectom , ( rodman , 1904 ) , and still there is controversy in some quarters as to its valu ;  . 
 if we cannot solve the problems of mammary carcinoma , what hope is there for the surgery of malignant disease in less accessible sites ? pretw ' u , , 8 attempts at grading . 
 little attention was directed to the grading of tumours until broders ( 1920 ) applied , on hansemann 's theory to squamous cell carcinoma of the lip , and a year later to similar tumours of the skin ( broders , 1921 )  . 
 l\iaccarty and sistrunk ( 1922 ) and l\iaccarty ( 1922 , 1924 ) also studied the histology of breast tumours , and found the most important prognostic charac teristics to be the degree of cellular differentiation and the presence or absence of certain stromal features . 
 ' white ( 1927 ) was unable to agree with the views of : : \iaccarty , but in a series of 100 cases confirmed the results of greenough ( 1925 )  . 
 smith and bartlett ( 1929 ) , and lat.er simmons , wright , hartwell and greenough ( 1933 ) , also confirmed the value of the syst.em introduced by greenough ( 1925 )  . 
 the five - year survival rat.es for the three grades of malignancy obtained by these authors are comparable , and agree in the main with those of pat.ey and scarff ( 1928 )  . 
they therefore elaborated a " clinical index of malignancy " based upon age , presence of lactation , rat.e of growth of tumour , and extent ( stage ) of the disease . 
perry ( 1925 ) , lane - claypon ( 1928 ) , truscott ( 1947 ) and hamett ( 1948 ) were not able ti < > prove that the position of the growth had any bearing on outcome in breast cancer . 
 flothow ( 1928 ) , in a little over 200 cases of carcinoma of the breast , studied the facrors stated by llaccarty ( 1922 ) to represent a defensive mechanism by the body to a malignant tumour . 
it was shown that the malignancy increased with a rise in the " malignancy index . " for comparison a clinical classification was also elaborated by schmitz , but no att.empt was made to study the effect of correlating these histological and clinical syst.ems ( hueper and schmitz , 1929 )  . 
 opinions regarding the accuracy of hisrological grading have varied from huepe , r , who finds as many as twenty different features of prognostic value ( hueper and schmitz , 1929 ) , ti < > reimann ( 1929 ) , who is unable ti < > find one . 
he considers , however , the broad grouping methods based on general histological stucture - - presumably such as that of greenough ( 1925 ) - ro be of value . 
greenough ( 1925 ) , on the other hand , applying the principal of anaplasia , concentrated on tubule formation , variation in size of cells and nuclei , secretory activity and mitotic and hyperchromatic figures . 
 the principles laid down by greenough ( 1925 ) were closely followed by others , such as smith and bartlett ( 1929 ) , and simmons , wright , hartwell and greenough ( 1933 )  . 
patey and scarff ( 1928 ) and scarff and handley ( 1938 ) , however , attached chief importance to tubule formation , variation in size of nuclei , and mitotic and hyperchromatic figures . 
 delbet and mendaro ( 1927 ) in france , on the other hand , considered the presence or absence of mucous secretion to be the most important factor in ascer taining the outcome of patients with mammary carcinoma . 
leroux and perrot ( 1928 ) andmoureau and lambert ( 1932 ) support the views ofdelbet and mendaro ( 1927 ) , but betrand and de nagey ( 1931 ) consider muco - secretion to be of no value in determining clinical progress . 
 evans ( 1933 ) studied a number of parenchymal and stromal features , and con cluded that , although anaplasia indicates a poor prognosis , it is of no practical value in assessing the outcome for the individual case . 
he concluded that the grade of malignancy is the most important indication ot survival period , and this is more significant when considered together with the state of the axillary glands . 
 complicated , exact numerical systems , such as the " histological malignogram " introduced by hueper ( hueper and schmitz , 1929 ) , are time - consuming and of doubtful value . 
 the series taken for the present investigation consists of 565 cases of carcinoma of the breast treated at the middlesex hospital between the years 1936 and 1942 inclusive , and at the war sector units associated with it during the latter half of this period . 
in spite of the movement of population produced by the recent conflict , all but 11 of the c3888 were traced by the follow - up department of the hospital . 
 for the present study the five - year survival rate will be the chief prognostic yard - stick , though some attention will also be given to ten - year results . 
 " sur vival rate , " however , does not necessarily imply freedom from cancer ; it is in point of fact , merely an indication of the number of patients actually alive . 
this was based on the principles laid down by greenough ( 1925 ) , but chief importance was attached to tubule formation , regularity in size , shape and staining of nuclei and hyperchromatism and mitoses . 
this view is supported by the work of greenough ( 1925 ) , white ( 1927 ) , patey and scarff ( 1928 ) , smith and bartlett ( 1929 ) , sophian ( 1935 ) , and in fact , this is the only histological feature on which scarff and handley ( 1938 )  . 
certain authors , such as evans ( 1933 ) , greenough ( 1925 ) and haagensen ( 1933 ) , paid attention to variation in size of the cells , but the outlines of these are usually indistinct ; it is more reliable to consider the nuclei . 
evans ( 1933 ) was unable to support this view , and plaut ( 1927 ) considers the feature unreliable on the grounds that many cancer cells divide by amitosis . 
nevertheless , as haagensen ( 1933 ) points out , a considerab1 proportion of the cells in cancer of the breast divide by mitosis , and he found a close relationship between the number present and the outcome . 
this is also supported by the work of greenough ( 1925 ) , white ( 1927 ) , patey and scarff ( 1928 ) , smith and bartlett ( 1929 ) , sophian ( 1935 ) , and simmons , wright , hart well and greenough ( 1933 )  . 
 the cases were fairly evenly distributed , 30 per cent of the total being pla - oed in grade i , 41 per cent in grade ii , and 29 per cent in grade iii . 
 227 it is evident that a parallel exists between grading and prognosis , there being more than three times the number of patients alive with grade i than with grade iii tumours . 
it will be noted that they a . , , uree especially with the findings of pat.ey and scarff ( 1928 ) , and table ii . - - grade and prognosis by various authors . 
no grade iii cases remained alive in the series of greenough ( 1925 ) , and also of white ( 1927 ) , but this does not appear to be the general experience . 
 total 218 433 the five - year survival period is a convenient yard - stick with which to gauge prognosis in breast cancer , but as truscott ( 1947 ) and others have pointed out , a large number of fatalities from this disease occur from five to ten years after operation . 
 comparison of the fiveand ten - year results emphasizes the importance of the latter as a more accurate indicator of the control of mammary carcinoma , there being a striking fall in the numbers oi survivals for the corresponding grades of tumour , even with allowance for expected deaths from other causes . 
this is in keeping with the 26 per cent obtained by richards ( 1948 ) , and the 32 per cent by harring t - 0n ( 1946 )  . 
 ( i ) well - marked ( ii ) moderate ( iii ) slight or ml total ( i ) slight ( ii ) moderate ( iii ) marked y ariation in nuclei h : yperchromatic and mitotic  . 
the extent of the growth should also be taken into account , and the most important single factor indicating this is whether the axillary lymph nodes are histologically involved or not . 
it is particularly interesting to note that the prognosis in the lower grade of malignancy with glandular spread is better than for either the higher or intermediate grades without such metastases ( 65 per cent alfre at fi . , e years compared with 53 per cent and 61 per cent respectively )  . 
 these results agree in principle with those of most workers who have employed the system introduced by greenough ( 1925 ) , and are almost identical with the findings of simmons , wright , hartwell and greenough ( 1933 ) ( table viti )  . 
 patey and scarff ( 1928 ) and scarff and handley ( 1938 ) , on the other hand , found a uniformly good result in all three grades when the glands were not involved , and so concluded thatgrading is only of prognostic value in those cases with axillary metastases . 
the figures in table ix refer to the state of the cases at the time of operation , and the time factor involved here is the delay in seeking treatment . 
on the other hand , if for any reason the grade ill .cases tend to present for treatment after a longer interval of time than those belonging to grade i , then this may account for the greater incidence of axillary involvement in the former . 
in addition a higher percentage of the former present within six months of the onset of the disease and fewer after twelve months as compared with the grade i cases . 
thus , in spite of the shorter delay in seeking treatment , there is a greater incidence of axillary involvement among the high and intermediate grad~ of malignancy , consequently emphasizing the greater metastasizing power of these types of growth . 
ewing ( 1940 ) , however , prefers to employ the term " potential malignancy " for a neoplasm as determined by microscopic examination , because the clinical course may be modified by such features as site of tumour , surgical trauma and perhaps changes in rate of growth . 
 several authors , such as hueper and schmitz ( 1929 ) , and also lee and stiiben bord ( 1928 ) , have compared the results of grading and staging in breast cancer . 
 involvement of the skin directly over and in continuitv with the tumour does not affect staging provided that the area ~volved is small in relation to the size of the breast . 
as previously , when the cases were classified according to grade ( tables i , iv ) , a large number of deaths are seen to take place in the interval between the shorter and longer follow - up periods , thus once more emphasizing the importance of the latter in assessing the achievements of breast cancer therapy . 
 a study of grading and also staging indicates that both methods give com parable results ; the latter , however , has the slight advantage of revealing the outcome for the most advanced cases ( stage 4 )  . 
 we ha , e already drawn attention to the relationship in breast cancer between the histological architecture of the tumour and its tendency to involve the axillary glands ( table ix )  . 
exactly half of the grade i tumours have not yet extended beyond the first stage , whilst about a quarter are advanced , belonging to stages 3 or 4 taken together . 
 100 100 100 these results merely gi , e additional support to the view already expressed with regard to the relation between histology and axillary involvement , that the higher the grade of mammary carcinoma , the greater the tendency for early spread beyond the breast . 
the vast majority of workers in this field , however , have argued as to the relati , e merits of either syste but why should the grade and stage be considered only separately , and in the sense of competing with each other to form the basis of a reliable prognostic guide ? a combination of these features would result in a classification which gives information on not only the type of growth , but also its extent when first seen . 
would this not bring about a more accurate grouping of cases than could be produced by either system alone ? indeed , se , eral authors have taken the histological picture into consideration with the state of the axillary lymph nodes , and the value of this has been con firmed here ( table vii )  . 
the percentage of five - year survivors is seen to range from as high as 87 per cent for stage i , grade i cases down to as low as 6 per cent for those belonging to stage 4 , grade ill . 
it is also evident that whilst the prognosis in each stage deteriorates with the rise in histological malignancy , the cases with low grade tumours do not conform to the general trend . 
it reveals that all is by no means lost if a patient presents with a stage 2 or even a state 3 growth provided that it belongs to the lowest grade of malignancy ( grade 1 )  . 
 having revealed the value of combining histological grading with clinical staging for prognosis in mammary carcinoma , the suggestion is now put forward that the wide range in results produced by different authors for identical methods of treatment depends upon the comparison of incomparable groups of cases . 
 w ' hat evidence is there to support these views ? with reference to this question , two groups of cases will be taken for study , one treated by surgery alone , and the other by surgery with ancillary radio therapy . 
although it is not the purpose of this paper to discuss the merits of treatment in breast cancer , the results achieved by these two methods will be compared in order to illustrate the discussion . 
it must be pointed out that the treatment in each group was by no means uniform , there being considerable variation both from the surgical as well as the radiological aspect . 
 irradiation was predominantly in the form of deep x - rays , either pre - operati.e , post - operative , or both , a few cases being treated with radium alone or radium and deep x - rays . 
 according t - 0 grade . - let us first consider the results achieved for each group according to the grade of malignancy ( tables x " \ ' ~i , xviii )  . 
on the other hand , in the radio - surgical group , although this operation was performed in the majority , there were many instances of more conservative surgery , which included 37 simple mastectomies and 17 local excisions . 
 " ~ith this in view , the survivals of a more uniform type of therapy were taken for study , the comparison being made between patients treated by radical surgery alone and radical surgery with irradiation ( tables xxii , xxiit )  . 
 the greater achievement of surgery alone over the combined attack is again seen in harnett 's ( 1948 ) figures which are also for the radical operation and are classified by stages ( table xxi )  . 
 from these facts it is clear that the variation in treatment by surgery in the present material does not appear to interfere with the fair comparison of the 278 h . 
 in this instance a false impres sion may be given when the results of two series of cases are compared owing to the possible unequal distribution of clinical stages in corresponding histological grades . 
here there are small number of seen to be more low and fewer high grade tumours in each stage ot the surgical as compared with the radio - surgical cases . 
furthermore , of all the neoplasms of low grade malignancy ( grade i ) 57 per cent were in this surgical group in contrast to only 30 per cent of the highly malignant type ( grade ill ) ( table xxvi )  . 
what , then , may acco~t for this fact ? is it merely fortuitous chance , it is true , may play a part , but this is not the only possibility  . 
 .although two groups of patients are placed in the same clinical stage , there may be some difference in the extent of the growth for which no allowance is made in our present staging systems . 
in view of the parallel revealed between hist.glogical picture and extent of tumour ( tables ix , xiv ) , it is these unfavourable cases which also tend to be of high grade malig nancy , hence the distribution in fig . 
it i < ; , therefore , useless to compare results obtained by different authors if the cases are taken according to stage and no allowance is in this instance chance is probably the chief factor made for type of growth . 
however , cannot be ruled out , individual surgeons ha , ing , to some extent , personal criteria for deciding on the measures to be adopted for a given case  . 
.y egkcte , d , routes of extension . - reference will be made to avenues of extension of breast cancer which are largely neglected in both prognosis and also treatment . 
of these unfavourable grade iii cases nearly 70 per cent ( table xxvi ) were referred for irradiation , thus emphasizing the disadvantage placed on the radiotherapy group when it comes to the comparison of treatment results . 
 to sum up : it is postulated that in a given stage certain cases haw unfa rnur able clinical features , which influence the surgeon to refer them for radiotherapy . 
 the tumours of these patients tend to be of high grade histological malignancy , and h~ve probably also extended , ia routes , as yet , not given adequate considera tion in prognosis and treatment . 
this may account , at least to some extent , for the unfavourable results achieved here and elsewhere ( adair , 194& ; truscott , 1947 ; harnett , 1948 ) by ancillary radiotherapy . 
in these instances the achievement of radiotherapy is probably even greater than appears on first examination owing to the unfavourable features which tend to be present in cases referred for this treatment . 
 it has been pointed out that the problem of grouping also applies to series treated by identical methods , though here chance rather than selection is prob ably a more important factor accounting for the distribution of the patients . 
with this method it is hoped that further light may be thrown on some of the problems of breast cancer , and possibly the true merits of the various treatments of the disease assessed . 
 when this clinico - pathological system is applied here , will the results achieved by ancillary radiotherapy appear to be any better ? this question , unfortunately , 282 h . 
harries ( personal commanication ) , at the middlesex hospital , quotes 19 per cent for the five - year follow - up and 4 per cent for a period of ten years among some 220 cases . 
these figures are inferior to those obtained by treatment , which is universally accepted as being of definite , aloe in prolonging life , except perhaps in the very advanced cases . 
 once the cases are classified more accurately , such as on the lines indicated earlier in this paper , and only then , shall we be in a position to study the merits of , arious treatments . 
we may find , for example , that less radical surgery may be adequate for the control of certain cases such as those with grade i , stage 1 tumours , whilst radiotherapy may be an important ancillary measure for some cases , but on the other hand of little use for others . 
grace ( 1937 ) in america obtained a 56 per cent fi , e - year surrival rate among 40 cases treated by simple mastectomy and radio tht > rapy . 
this author considers that " the cellular structure of the tumour is the dominant factor in prognosis , and surgical technique , irrespecti.e of its radicalism , plays a definite secondary role . " some support tor this view is perhaps to be found in the paragraphs which follow . 
a group of 45 cases in his series were treated by local excision with implantation of radium , and 63 per cent were alive after a similar period of time . 
 what do these results mean ? can it be possible that more conservative surgical measures than the radical operation are sufficient for the control of mammary cancer ? such , indeed , is the view in this country of keynes ( 1937 ) , and more recently mcwhirter ( 1948a , 1948b )  . 
 we have already suggested that when cases are properly grouped accord.mg to both stage and grade it may be found that less radical surgery may be adequate for certain types of case . 
it is not even necessary to have numerous sections to appreciate this picture ; one or two portions of tissue of reasonable size taken from the periphery of the growth are adequate . 
 thus , patey and scarff ( 1929 ) , in a series of llo cases , found that the metatases in the axillary nodes were of the same grade as the primary in 82 per cent , of a lower grade in 16 per cent , and of a higher grade in only 2 per cent . 
comparable figures to these are also given by other writers , such as harrington ( 1935 ) , lach man ( 1944 ) , riddell ( 1948 ) and ledlie ( 1948 )  . 
little attention appears to have been given to this problem until scarff and handley ( 1938 ) suggest.ed that disappointing results in stage 1 cases may be explained by this mode of spread . 
this applies particularly to growths situated in the inner half of the breast ; of 17 such cases 12 had deposits in the internal mammary chain , in 2 of which the axilla was not also involved . 
 in spite of this , truscott ( 1947 ) and harnett ( 1948 ) were unable to show that the site of the growth plays an important part in prognosis . 
 in those cases where the axilla appears to be free from involvement at the time of operation and the prognosis subsequently turns out to be poor , invasion has probably occurred by routes such as the int.ernal mammary chain , and perhaps the supraclavicular glands . 
 after considering these facts it would appear , as handley and thackray ( 1949 ) point out , that there are but few growths which are really confined to the breast . 
chief success , from the point of accuracy and simplicity , appears to have been from histological grading , on the lines mdicated by pat.ey and scarff ( 1928 ) , combined with the state of the axillary glands . 
stage i ? this question has defeated explanation in the past , and will probably continue to do so until such time as the pathologist plays a part in establishing a prognostic system of the type indicated in this paper . 
 the controversy which exists as to the relative merits of the different methods of treatment for carcinoma of the breast has led to the present investigation , the prime object of which has been to establish a more accurate classification for this disease . 
 the gra < le of the tumour taken together with the state of the axillary lymph nodes gives a more accurate indication of outcome than either grading or staging alone . 
for example , 94 per cent of grade i cases without glandular involvement were ali , e at five years compared with 16 per cent of grade iii with this complication . 
it offers an explanation for disasters in early cases , and also for remarkably good results obtained in advanced in indicates that all is not necessarily lost if a patient presents with a stages . 
 lt has been shown that in a given clinical stage or histological grade the cases treated by surgery alone are not strictly comparable to those subjected to surgery and radiotherapy . 
in addition this has probably also played a major part in bringing about the present - day confusion as to the relative merits of the various measures advanced for the control of the disease . 
sambrook for assessing the clinical st.age of the cases ; to miss chambers of the follow - up department for tracing the patients , and to the photographic department for assistance with the microphotographs . 
mottram ( 1945 ) published the results of experiments designed to demonstrate a relationship between the tumour yield induced by benzpyrene and the number of epidermai mitoses present at the time of application of the carcinogen . painting the skin of rnice at midnight resulted in a higher yield ofpapillomata than did painting at midday . 
but not water , and 1 - 4 hours later they were given a single appheation of carcmogen , benzpyrene ( hoffinan - la roche ) in experiment i and methyleholanthrene ( eastman kodak & co in experiment 2 . in the 1 - - ) enzpyrene experiment each animal received 0 - 1 ml . 
of a 0 - 3 per cent solution in acetone apphed to the interseapular region of the skin , and ' m the methyleholanthrene experiments the dose wasalso 0i ml . 
the mice were starved for a total period of 64 hours , after which they three days after the application of the carcinogen painting were fed ad libitum . with croton oil ( 0 - aper cent in acetone ) was commenced , and this was repeated twice weekl for 20 weeks . 
these mice were treated in the same way as those in the group b , except that the period of starvation was omitted altogether . in experiment 3 , group a contained 25 male mice which were deprived of all food 36 hours before each was painted with 0 - 05 ml . 
most of the papillomata being discovered between the 1 : 21th this is in good agreement with the results obtained bv berenand 15th weeks . blum and shubik ( 1947 )  . 
the methylcholanthrene was introduced into average age of the mice was 6 months . the prostate gland in the following manner : under general anaesthesia , a median abdominal incision was made , exposing the prostate lobes . 
8. - the same after 3 weeks ' time . 10 or more layers deep , keratin pearl formation still absent . cells acquiring more pronounced squamous metaplasia . development of stratified squamous epithelium , h . 
they varied between i to 3 of an inch in diameter and frequently more than a single prostate lobe was involved . a tumour of average size is shown in fig . 
7. received for publication february 7 , 1947 . it is a widespread doctrine among students of cancer that any tissue or organ capable of cell division may be the site of a malignant neoplasm , but it is well known to clinicians that certain tumours , theoretically possible , do not in fact occur . 
the most striking example of an organ which never gives rise to a neonotwithstanding the fact that mitoses occur in the lens plasm is the lens . throughout life , having been seen even in the lenses of patients 80 years old , no tumour of the lens has ever been discovered . the lens is an entirely epithelial structure embryologically derived from the surface ectoderm , devoid of blood supply and enclosed in a semi - permeable although mammalian lenses are enclosed membrane , the hyaline lens capsule . during embryonic life in a capillary net ( the vascular lens capsule ) this does not constitute a blood supply , since the vessels do not come in contact with the lens in the majority of vertebrates cells , being always outside the hyaline capsule . the lens can therefore be looked even this embryonic vascular capsule is absent . on as a segregated group of specialized epithelial cells growing and differentiating in a closed system , separated alike from the blood - stream and from the surface of the body . 
may be important factors in the pathogenesis of cancer of deeply seated as well as of superficial organs indeed , early in the 19th century a careful local study of is hardly a new one . cancer deaths in verona was made by stern ( 1842 ) , the notion of cancer houses was looked into and fragmentary studies of cancer endemiology were made in the concept of cancer as a unitary disease switzerland , america and elsewhere . affecting organs rather at random has tended to discourage detailed research on site distributions . the general register office in london worked patiently upon the occupational aspects at successive census periods with increasing detail as death certification recently the danish cancer registry , initially of primary cancer sites improved . rather sceptical of some of the conclusions reached , has admitted that danish data tend to confirm them ( clemmesen , 1951 ) , and similar data have been pubin 1950 and 1951 the council for lished from the netherlands ( versluys , 1949 )  . co - ordination of international congresses of medical sciences arranged conferences on what was at first called " geographical pathology " , but has now become " endemiology " of cancer . very little has been written , however , on lung cancer from this aspect except with respect to tobacco , although it came under discussion at the first of the above - mentioned conferences ( c.c.i.c.m.s. , 1951 ; daff , doll and kennaway , 1951 )  . in the present paper the short term " lung cancer " is used to mean carcinoma and other malignant neoplasm of the bronchus , lung and pleura ; and when " mortality " is mentioned it is understood that whatever rate or index is used has been standardized for age . * the substance of this paper was communicated to the metropolitan brench of the society of medical officers of health on may 9 , 1952 , 100 p . 
at that time i still had to work upon the rates for 1921 - 30 , and failed to find any significant correlation either in the large towns or in the metropolitan boroughs between lung cancer mortality and the social class or overcrowding indices . recent research on correlation with tobacco smoking . between 1930 and 1946 the recorded rates in england and wales as a whole had been rising steadily , and to a surprising extent even when increasing use of x rays was considered . consequently the medical research council called a conference to advise whether any useful research could be undertaken to throw light on the causes . 
the result of that study was published in september , 1950 ( doll and hill , 1950 ) , and in my view it proved beyond doubt , in conjunction with american evidence of the same kind ( wynder and graham , 1950 ) that 102 p . 
stocks tobacco smoking is a very important factor in the causation of lung cancer . did not prove , however , that tobacco smoking is the only important factor in it has been suggested that the figures could mean that 90 per cent causation . of the lung cancer occurring in greater london is caused by tobacco ; but they do not necessarily mean that , and there are reasons for thinking that the proportion is - much lower , and that atmospheric pollution may be an additional factor . these reasons derive from some statistical facts not hitherto published . mortality in london in 1946 to 1949 . in the four years 1946 to 1949 the deaths of males attributed to lung cancer in in 1950 england and wales averaged 8183 annually , and of females 1774 . deaths of males exceeded 10 , 250 and those of females were just short of 2000 , and in 1951 the total reached 13 , 000 . 
the national rates at different ages are compared in table iv , which shows that at ages 35 - 45 the increase was 6 - fold , and at 55 - 75 it was more than 11 - fold . how much of this enormous increase has been due to more complete detection of the disease and how much to increased incidence we can only surmise . london county as a whole , allowing for age changes , male mortality increased about 8 - fold between the two periods ; and it is now about 60 per cent greater than in the country as a whole , and 21 times the rate for rural districts . 
1 shows the mortality distribution in 1946 - 49 . for 1921 - 30 there were two areas of specially high certified mortality , one in bermondsey , stepney , bethnal green , hackney and stoke newington , the other in hampstead , st . 
stocks wind direction as a possible factor . returning now to greater london , clark ( 1951 ) has shown that the logarithm of the population density per acre in successive zones diminishes in arithmetic progression on passing outwards from the business centre , and the same is true supposing domestic smoke to be an important factor in of other large cities . producing lung cancer , if there was no wind at all one would expect to find the highest incidence at the centre , diminishing in all directions outwards . if there is wind and it comes from all directions equally , a more diffused but still symmetrical distribution would be expected , with less contrast near the centre and more near the periphery . however , wind does not blow equally from all directions , and greenwich records over 12 - hour periods throughout the year 1950 show that the wind direction , when analysed into 8 sectors , was s.w. 
jensen. frm the danish cancer regi8try under the national anti - cancer league , kobenhavn 0 . received for publication january 31 , 1953 . in 1947 clemmesen and busk reviewed the material of the danish death certificates with a diagnosis of cancer of the lung from the years 1931 to 1945 ( clemmesen and busk , 1947 )  . 
they found an increase in the numbers for males , particularly pronounced in copenhagen , the capital , less striking in provincial towns , and somewhat smaller for rural areas . however , the incidence of cancer of the lung among persons subject to routine examination in the central tuberculosis station for the city of copenhagen did not reflect the heavy increase in mortality found in the city as a whole . 
diagnose a number of cases of cancer of the lung , so that the graph illustrating the incidence rates in its material should be changed , as shown in fig . 
1. during the years up to 1950 the increase in mortality rates for cancer of the lung among men in the various areas of denmark continued , and from fig . 
women. of the disease , and only to a small extent attributable to improvements of diagnosis , which can be expected to cause a proportional increase for both sexes in the number of cases diagnosed . 
the possibility that the deciding factor might be an increase in medical attention for all categories of diagnosis can be excluded because the patients from the tuberculosis station were unselected and referred directly for diagnosis with a view primarily to a disease different from bronchial carcinoma , and finally were examined in a uniform way . further analysis of the material from the danish cancer registry confirm the results from mortality statistics ( clemmesen and busk , 1947 ) that the increase in incidence of cancer of the lung among men is particularly strong for the relatively younger age classes ( clemmesen and nielsen , 1952a , 1952b )  . this seems to speak against the assumption that atmospheric pollution is a causative factor of primary importance to cancer of the lung as far as denmark is concerned . if this were the case we would expect an increase in incidence for all age classes . it might also be expected that the windy climate of copenhagen could cause regional differences in incidence of the disease within the city analogous to the findings of stocks ( 1952 ) for london , but in fact it appears that the distribution of cancer of the lung among men in copenhagen varies with the social level expressed in terms of annual house rent , much like cervical cancer of the uterus being most frequent in the classes of subdistricts with the lowest level of house rent , although the single subdistricts show no such parallelism . however , there is no tendency for leeward areas to exceed the weatherside with regard to incidence rates for carcinoma of the lung ( clemmesen and nielsen , 1951 )  . thus , it would seem that the main reason for assuming atmospheric pollution to be causative to cancer of the lung in denmark would be the excess of cases in towns , particularly in copenhagen . 
5 represents mortality rates at various ages for lung cancer among men in copenhagen arranged in quinquennial cohorts born in the period about the years given in the diagram . it would seem reasonable to assume that the carcinogenic influences determining the incidence of cancer of the lung , whether they be of customary , occupational or hormonal character , will not begin before the age of 15 or perhaps a few years later . it appears from the tables that the cohorts of highest mortality at an conearly age do not show an increase in rates until after the 35th year of age . sequently it will be justifiable to assume a minimal period of about 20 years from the beginning of the influence to the death of the patient from cancer of the lung under the conditions usual in copenhagen . it follows logically that if we assume a later or earlier beginning of the carcinogenic influence we must respectively shorten or prolong the assumed period with a corresponding number of years . it should also be remembered that we must allow for wide variations either way . under these assumptions and from the observations illustrated in fig . 
5 that the graphs for the quinquennial cohorts do not coincide as they would for most other sites of cancer , but are moving to the left , although now at a decreasing pace . this would not be explained by assuming that all cohorts were from a certain age subject to some carcinogenic influence unless we add that the influence was strengthened at some point of time , or during a limited period of years . now it is seen that the result of the carcinogenic influence increased particularly for men born between 1875 and 1885 , while the effect on the following cohorts progressed at a slower rate . 
2 , it will be seen that the differences in the level of the graphs indicating crude mortality rates for cancer of the lung between capital , provincial towns and rural areas can be ascribed to a later beginning of the rise in the latter categories , i.e. , 8 years for provincial towns and 10 for the rural areas , which is in full conformity with the result of the cohort analysis . hence it appears that the assumption of atmospheric pollution as a cause of cancer of the lung in denmark in order to explain the differences between towns and country is unnecessary , if we suppose that the carcinogenic influence began a few years later in the provincial towns and a few years later still in the country . quite apart from the etiological implications of our cohort study it is in the field of practical hygiene we find the widest consequences of the diagram of fig . 
calcutt oestrogens : oestrone and diethystilboestrol . a group of arsenicals chosen in view of neubauer 's ( i947 ) implication of arsenicals as carcinogem ' c agents . three unrelated compounds : nitrogen mustard ( shown to be carcinogenic by boyland and homing , 1949 ) , urethane ( shown to be carcinogenic by jaff6 , 1947 ) and light green f.s. 
numbers represent duration of exposure in minutes to filtered ultraviolet radiatioxi required to cause death of 90 per cent of the cultures . with the exception of the oestrogens none of the agents tested compare in comparisons among the compounds tested effectiveness with 3 : 4 benzpyrene . suggest a certain degree of correlation with carcinogenicity . 
whether the effects achieved are a true photodynamic response as occurs with fluorescein and other dye stuffs , or ate a consequence of intracellular action by the radiation leading to increased susceptibility to a toxic agent , as calcutt ( i 950 ) has show - n to occur in the case of certain - sh inhibitors must remain in doubt . 
on the other hand , it appears possible that the radiation has brought about such an intracenular change that the chemical carcinogen is now able to attack a much greater amount of substrate than is normary the case . 
thus complete disruption of the intracellular functioning and death occurs , rather than ' a partial disruption which manifests itself as the carcinogenic change . certain evidence supporting such a view exists calcutt ( 1950 ) showed that irradiation with wave - lengths in the literature . greater than 3300 a increased the availabihty of intracellular - sh groups . such treatment prior to the addition of a photosensitising agent was show - n by calcutt ( 1951 ) to enhance the photodynamic response . 
jung. from the cancer research laboratory , university of florida , gainesville , florida . received for publication march 21 , 1951 . the experimental investigation of gastric cancer is seriously impeded by our present inability readily to produce this condition in animals . 
the difficulty and uncertainty of this method have progress in this field would be greatly facilitated if a precluded its general use . chemical compound capable of producing gastric cancer were discovered . that a carcinogen with such specificity is possible may be implied from the frequency with which butter yerow , for example , produces hepatomas ( kinosita , 1940 ) and beta - napthylamine , bladder tumors ( wiley , 1938 )  . 
when this is done it very seldom results in malignant growth in the stomach because of the protective if the carcinogen could be 8ecreted by the stomach it would action of the mucus . be in a much more favourable position to initiate cancer . the first step towards a solution of the problem is to ascertain just what properties of a substance influence its secretion by the glands of the stomach . the optimum properties might then be conferred on - a carcinogen by judicious substitution in the molecule . 
the resulting compound could be expected to initiate neoplastic growth in the stomach . several groups of workers during the past twenty - five years have studied , by means of gastric pouches in dogs , the secretion of intravenously injected dyes . dawson and ivy ( 1925 ) , kobayashi ( 1926 ) , ingraham and visscher ( 1935 ) , and varco and visseher ( 1941 ) , although working under varied conditions , are geneof some sixty dyes rally in agreement as to the dyes secreted by the stomach . studied ( ingraham and visscher , 1935 ) , afl those secreted are electropositive ( basic ) under some conditions . 
on the other hand , dyes not secreted by the gastric glands are acid or amphoteric with the possible exception of four basic triphenylmethane dyes . the basicity of these dyes seems to be the property most likely to determine their degree of gastric secretion . 
at a pkbof 11 - 3 , for instance , this equation yields a concentration ratio of 51 , at a pkb of 7 - 5 a ratio of 2 - 8 x 101 . ratios actuary obtained were 1 - 3 and 26 - 4 . although experimental results indicate a definite tendency for secretion to increase with increasing basicity . 
it is obvious that there is some opposing factor . this opposing factor increases with increasing basicity , so that at pkbof about 6 - 0 the tendency for the basic dve to concentrate in the stomach , due to distribution differences , might be completely overcome . this opposition to gastric secretion of dyes of increasing basicity is nicely explained in terms of the pore theory , or the concept of the ositively charged membrane ( ingraham and visscher , 1935 )  . acid dyes would be retained by chemical combination . basic dyes are assumed to pass through this membrane in the undissociated foras the ionization constants of these dyes increase it would become increasingly more difficult for them to pass through a positively charged membrane . it appears , therefore , that we are dealing with two main effects in the gastric secretion of dyes . 
kennaway also of those following each one of the recognized occupations , at the time of the census . the number of deaths attributed to cancer of the lung and larynx occurring in the whole male population in each of these age groups during the years in question was obtained from material at the general register office . the comparison of the various occupations with the general population is then a sum in proportion , which gives the ratio of the number of deaths in any given occupation to those , reckoned as 100 , which occurred in the same number of males in ' the same age groups in the whole population . 
an example of this calculation is given in the earlier paper . sources of error in statistical work on death certificates . these were examined in the earlier paper ( kennaway and kennaway ; 1936 )  . the use of death certificates for statistical purposes is liable to errors which are inherent in the nature of the material and cannot be wholly eliminated . 
one must either recognize and admit these errors and correct them in any way possible , or abandon any attempt to obtain information from these data . ( 1 ) correction for period between census . - in order to compare the incidence of cancer upon different occupations one must know the number of persons following each occupation . this is learned from the census returns . 
the figures for populations used for the earlier period ( 1921 - 32 ) were those of the 1921 and the 1931 census , which were combined by means of a formula described in the earlier paper ( kennaway and kennaway , 1936 ) ; those in the present paper are from the 1931 census , which is the last taken . 
kennaway when large numbers are concerned . the immense amount of labour involved in such enquiries can be seen in the monograph on cancer of the scrotum by henry ( 1946 )  . but as none of the occupations included in the present study , with one exception , shows a very high incidence of cancer of the lung , comparable to that seen in the occupational cancers of ' the skin and bladder , this source of error is not a very serious one . ( 4 ) incorrect diagnos8is is of course a source of error in these , as in all other , in the case of death certificates received in bulk , perhaps some medical data . years after the dates of the deaths recorded , one can do nothing but exclude any certificate of which the wording suggests ( 1 ) that the cause of death did not come within the category under examination , or ( 2 ) that the diagnosis was uncertain or ill - founded ( see next section ; such certificates are made the subject of individual inquiry by the general register office )  . when such exclusions have been made , one must treat the remaining certificates as correct if any use is to be made of the material . death certificates taken for examination . the material utilized in this paper has been restricted as far as possible to cases of primary malignant growth of the lung , and of the larynx . 
when the individual occupations are examined considerable variations are found . in the earlier paper attention was drawn to the high ratio for cancer of the lung in judges , stipendiary magistrates and barristers ( 173 ) and in stockbrokers and stockjobbers ( 187 ) ; in the later period ( 1933 - 38 ) the former fell to 112 and the latter rose to 253 . the stockbrokers and jobbers also have the highest ratio among the professional workers for cancer of the larynx . the figures for roman catholic priests and monks are too small to be significant . the ratio for ministers of other religious bodies has risen ( table xx )  . 
no attempt is made here to deal with all the data on the carcinogenic action of arsenic , as this subject is under investigation by a committee of the industrial health board , but the following quotations from recent annual reports of the senior medical inspector of factories show the possible importance of arsenic in relation to cancer of the lung . 
kennaway there was a special surgical clinic dealing with lung cases , and where full x - ray and bronchoscopic investigation was practised , 42 per cent of the clinical diagnoses were wrong ( table xxiv )  . 
hence the diagnosis of cancer of the lung appears to be still very incomplete , even under favourable conditions , in spite of the great improvements which are generally stated to have been made . 
some possible causes of a real increase are considered in the next section . in the earlier paper ( kennaway and kennaway , 1936 ) we drew attention to the evidence afforded by cases of cancer of the lung in which an erroneous diagnosis was made based on nervous or mental symptoms due to metastases . 
18. ( 2 ) one must look , therefore , for some other factor to explain the increase , if there is a real increase , in cancer of the lung in recent years . 
a similar argumnent might be applied in tile case of cancer of the lung , which is not known to be prevalent in any of the lower animals . the adenoma of the lung of the mouse , and certain affections of the lung of sheep in south africa and iceland , are neoplasms of which the exact nature is uncertain . we know one instance at any rate of the susceptibility of the lung of an animal to a carcinogenic agent , namely the lung of the cat in relation to 2 - acetylaminofluorene given by the mouth ( harding , 1946 ) ; hence there is no reason to think that animals are immune to any such one obvious factor , possibly carcinogenic , to which the lung of mnan agents . alone is exposed is tobacco smoke . during the present century very considerable changes have taken place in this country in the social distribution of the various methods of smoking . there were , of course , exceptions to any rule , but roughly one might say that in the earlier part of this period men of the richer classes smoked pipes , cigarettes and cigars , and men of the poorer classes smoked pipes ; cigarette smoking was increasing among the richer women , while women of the poorer classes did not smoke . one never saw a woman scrubbing her front door - step , or hanging out the washing , with a cigarette in her mouth . the great change which has taken * a . 
of course no claim is made here that the simultaneous increases in the consumption of tobacco , and in cancer of the lung , proves any etiological connection between the two . other changes which have taken place in the same period , which no one proposes to associate with cancer of the lung , e.g. 
kennaway to summarize the evidence brought together in this section on the incidence of cancer of the lung : the higher mortality in towns , the low mortality in agricultural occupations , and the absence of social gradient , are compatible with a factor in the air , such as coal smoke . in any such comparison of urban and rural areas , the question of facilities for diagnosis must be considered . coal smoke , which is probably a decreasing contaminant of the air , does not account well for the increase of cancer of the lung . 
among various possible factors is tobacco smoke ; the consumption of tobacco has risen , and so has the percentage of it smoked in the form of cigarettes , of which the smoke is often inhaled . 
among various possible factors which have been suggested to account for the increase is tobacco smoke ; the consumption of tobacco has risen , and so has the percentage of it smoked in the form of cigarettes , of which the smoke is often inhaled ; such an effect of tobacco would accord well with the absence of social gradient . we are indebted to the registrar - general for the data considered in this paper , and also for kindly permitting us to use some figures which have not yet been made public officially . 
we have received much assistance in the classification of occupations , and on various other questions , from some members of the staff of the general register office , to whom we wish to express our gratitude . we wish to thank e . 
1. received for publication december 1 , 1952 . it has for long been an accepted principle that the earlier the diagnosis of malignant disease is made the more likely it is that the growth , if in a region of the body accessible to the surgeon , will be in a stage which admits of radical resection and the higher will be the survival rate . 
however , balfour ( 1937 ) recorded that the 5 - year survival rate for 2112 patients after resection of the stomach for carcinoma was 25 per cent for those patients with histories of symptoms for less than 6 months and 35 per cent for those with histories of symptoms for more than one year . 
walters , gray and priestley ( 1942 ) in a later study recorded that 24 * 6 per cent of patients whose symptoms were of less than one year 's duration survived 5 years after resection of the stomach for carcinoma , whereas 32 - 6 per cent of patients the duration of whose symptoms was more than one year survived 5 years . 
the authors investigated the association between the length of history and the grade of malignancy as judged by broders ' classification , and give a table which shows that 39 of the 114 patients had growths which were classified as broders ' groups i and ii , while 75 had growths classified as broders ' groups iii and iv ; in each case the proportion of patients who gave histories of symptoms for more than 2 years was 23 per cent . eggers , de cholnoky and jessop ( 1941 ) reported that while the 5 - year survivals of 235 patients who had undergone radical .mastectomy for cancer of the breast fell steadily from 76 per cent to 20 per cent with delay in treatment up to 2 years , the survival rates rose to 25 per cent of 20 patients in whom the delay was over 2 years , and to 40 * 9 per cent of 22 patients in whose cases - there had been delay of 3 years or over . 
harnett tomies for cancer of the breast , found that 24 - 8 per cent of the 938 5 - year survivors were treated more than one year after recognition of the tumour ; he considered that the majority of these cases were the indolent , slowly - growing types of breast carcinoma , which metastasized late or occurred in hosts whose desmoplastic reaction to the tumour was intense . 
bloom ( 1950a ) in an analysis of 470 cases of cancer of the breast treated by surgery alone or with ancillary radiotherapy found , after classifying them into 3 groups according to histological criteria of degree of malignancy , that 79 per cent of 141 cases graded as of low malignancy survived 5 years , 42 per cent of 191 graded as of moderate malignancy and 25 per cent of 138 graded as of high malignancy ; when the histological grading was subdivided according to the presence or absence of invasion of the axillary lymph nodes , he found that with lymph nodes not invaded the 5 - year survival rates for gradesi , ii and iii were 94 , 61 and 53 per cent respectively , while for patients in whom the lymph nodes were demonstrated histologically to be invaded the survival rates for the three grades were 65 , 30 and 16 per cent respectively . 
as all types of treatment , surgery , radiotherapy and combined treatment , whether radical or palliative , were included , it is not surprising that few significant differences in survival rate were detected , though in most regions it appeared that the patients treated early showed little better survival rates than those who came late . in the present communication tabulations are presented from the same series of cases of the results of treatment of patients in stages i , ii or iii , who were treated by radical surgery alone or combined with radiotherapy , arranged according to duration of symptoms at the time of commencing treatment . 
by the elimination of all patients who were in stage iv , and of those in whose cases only operations of a palliative nature were performed , the series is restricted to those in whom there was a reasonable expectation of 5 - year cure . patients treated by radiotherapy alone have been excluded , because it is difficult to separate those in whose cases the treatment was intended to be curative from those in which it was palliative only , though some of the latter survived 5 years . the cases are grouped by site of the disease and by duration of symptoms at the time of commencing treatment into ( a ) , those in which the interval from first symptom to commencement of treatment was less than 6 months , ( b ) , those in which it was between 6 and 12 months , ( c ) , those in which it was more than 12 months , ( d ) , those in which it was unknown . 
the 5 - year survival rates for each of these groups is expressed as a percentage of the total in the group , and the standard errors of the differences have been calculated to test for statistical significance . in the more important sites the survivals are shown by stages : i . 
survd. over 12 , , not known the differences in survival rate are not statistically significant . for cases of known duration x2 = 1x77 , n = 2 , p < 50 > 30 . . 
among 383 patients treated by radical mastectomy alone , 35 - 5 per cent were in stage i and the best survival rate for all stages combined was 50 9 3 - 3 per cent for those treated during the first 6 months ; among 175 who were treated by radical mastectomy combined with radiotherapy only 21 * 1 per cent were in stage i and 43 * 4 per cent were in stage iii , and the best survival rate for all stages combined was 58 - 8 8 - 4 per cent for patients treated one year or more subsequent to the first symptom , who numbered 34 . 
the difference of 7 - 9 9 0 between these survival rates is not statistically significant . when the sites were subdivided into those in which the highest survival rates were among the patients who came under treatment in less than 3 months and those in which the highest rates were among those treated in the second 3 months , it was found that the former included squamous carcinoma of the skin , corpus uteri , penis and female breast with a survival rate for all groups of 54 - 9 per cent , while the latter included cervix uteri , kidney , .papillary carcinoma of the bladder and carcinoma of the pharynx ( treated by radical surgery or by combined methods ) with a 5 - year survival rate for all groups of 51x0 per cent . the age distribution of 702 patients with cancer of the breast who were . 
the group of 63 in whom the symptoms were of over 12 months ' standing at the time of operation had a survival rate of 14 3 per cent ; the difference of 9 9 7 0 between this figure and that for the group treated in the second 6 months is not statistically significant . if the patients are grouped into those of less than 6 months ' duration , with a survival rate of 11 - 2 per cent , and those of over 6 months ' duration , with a survival rate of 19 - 2 per cent , the difference of 8 - 0 4 - 7 is not significant . the age distribution of the patients with cancer of the stomach and colon were investigated by the x2 test , but in neither case were there any significant differences between the observed and expected survivals in the different age groups ; for the stomach cases p < * 20 > * 10 and for the colon cases p < - 70 > .50 , showing that the differences in survival rates were not due to differences in age distribution . 
the survival rate for cancer of the stomach was 20 - 4 per cent for 108 patients in the age groups 25 - 54 and 11.1 per cent for 133 patients of 55 and upwards , but the difference of 9.3 4 - 7 is not significant , though the prognosis was not so good in the older patients . 
as has been stated above this difference cannot be accounted for by differences in the age distribution of patients in either of the groups , so it must be presumed to be due to variations in the rate of growth of individual tumours all cases of patients with and in their infiltrating and metastatising powers . distant metastases have been eliminated from the present series , which was confined to those in which the tumour was local or had given rise to clinically recognisable metastases in lymph nodes ; they were selected as operable cases , no patient in an advanced stage or suitable only for palliative treatment being small differences were found in the proportion of patients in stage i included . among those with the highest survival rate in each of the three groups ; for group w . 
the mean duration of life in 153 untreated patients in group a was 23 - 1 months , of 176 in group b was 11 - 7 months and of 296 in group c was 17 - 6 months . 
the sites showing the longest survivals among the untreated patients are those in which treatment by radical surgery alone or with radiotherapy gives the best results , although some sites show a short duration of life , either because , as in the case of the lip , very few cases are left untreated , or because , as in the case of the colon and the intrinsic larynx , untreated patients often die of complications , such as intestinal w3w . 
group a included the skin ( squamous carcinoma ) , corpus uteri , penis , cervix uteri , female breast , kidney , bladder ( papillary carcinoma ) and pharynx . for this group of sites , comprising 1097 cases of known duration , the best survival rate was 51 1 per cent of 616 patients treated in the first 6 months against 42 - 0 per cent for the remainder . 
group b included salivary glands , tonsil , testis , colon , skin ( malignant melanoma ) , nasal sinuses , bladder ( infiltrating carcinoma ) and stomach . this group of sites , comprising 718 cases of known duration , the best survival rate was 30 - 6 per cent of 134 patients treated in the second 6 months against 27 1 per cent for the remainder . 
japha. received for publication february 2 , 1949 . martn and reese ( 1936 , 1942 , 1945 ) were the first to describe an extensive series of cases of retinal glioma treated by deep x - ray therapy . in their latest paper they report 75 per cent 5 - year cures in 8 cases of bilateral disease , one eye having previously been removed by surgery . 
at the middlesex hospital 19 cases of glioma retinae were seen between 1929 and january , 1946 . all cases were treated , 4 by surgery alone ; in the others radiotherapy of one type or another played a major part in the treatment . 
the numbers are too small to allow comparisons to be made between different types of treatment , but as regards deep x - ray therapy certain conclusions have emerged , and a technique has been evolved which differs in some respects from that advocated by the workers of the new york memorial hospital . the results of surgery have greatly improved in the last 30 years according to ray and mcclean ( 1943 )  . collecting their figures from the literature they estimate that between 1868 and 1941 , 18 per cent cures were obtained by enucleation in 677 cases , whereas 50 per cent cures are claimed for the 105 cases so treated between 1911 and 1941 . this progress is ascribed to the more radical and improved technique , often with partial excision of the optic nerve , used in later years . 
the number of bilateral cases included , if any , is , however , not stated . the authors themselves advocate a combined intracranial and orbital operation in view of reese 's ( 1931 ) statement that 52 per cent of 119 cases showed invasion of the optic nerve beyond the lamina cribrosa . duke - elder ( 1940 ) also states that 50 - 57 per cent of unilateral cases may expect to be cured . reese ( 1940 ) cites statistics of 95 cases collected by the division of ophthalmic pathology of the american registry at the army medical museum , 26 of which had bilateral disease . 
at the time of review 21 cases were untraced , 39 had died , 13 had lived 5 years , 2 had lived 3 - 4 years , 10 between 1 and 3 years , and another 10 just 1 year . besides x - ray therapy , which is historically reviewed by martin and reese ( 1936 , 1942 , 1945 ) , attempts have been made at treatment of the second eye m bilateral cases by radon - seeds . these are usually introduced either into the growth itself or sown on to the sclera over the neoplasm . stalhard , in his gifford edmond prize essay ( 1933 ) , reports 5 cases treated primarily by these methods . one of his cases - first reported on by moore ( 1930 , 1935 ) , was treated in 1929 ( twice by the insertion of a seed into the growth and also by episcleral seeds ) , is still alive , but has a cataract . three other cases , including an advanced case treated only experimentally and intended for subsequent histological investigation , came to excision . in a further report stallard ( 1948 ) gives the result of 15 cases so treated . 
deep x - ray therapy . - as long as radium moulds were being used it was inevitable that the whole of the globe was being irradiated to a high dose , but with the change - over to and use of small beams that were developed in deep x - ray therapy it became possible to limit the volume ofhigh dose to a certain extent . 
our technique has been directed at eradicating the focus of disease present rather than treating the whole of the posterior half of the retina ( where the majority of the growths are situated )  . 
a recent case , however ( not included in this survey ) , showed us that a certain risk isrun thereby in that shortly after the treatment and subsequent disappearance of a small lesion below the equator by fields of 2 and 3 cdiameter a further nodule appeared in the upper half of the retina . in an endeavour to treat as small a part of the eye as possible we have used circular fields of 2 and 3 cdiameter by means of special tubular applicators primarily intended for intrabuccal lesions as described by roberts and quick these are used in connection with our deep x - ray tubes , treatment ( 1943 )  . being carried out at 190 - 220 kv . 
lateral ( temporal ) , medial ( tansnasal ) , superior and inferior orbitals . abandoned as soon as it became apparent that the cornea was the most vulnerable structure of the eye , and disintegration of the eye had occurred in 2 or 3 cases in which this approach had been used . the lens , too , will receive a relatively large dose of irradiation when the anterior field is used and the lens dose should be kept at aminimuwe endeavour to ensure this by our technique of " by - passing " the lens as much as possible , which can be achieved in all the other fields mentioned . the anterior field was fields used so that accuracy ofalignment positioning . - special problems ofset - up arise because of the age of the patients and the small is of much greater importance . most of the children under the age of 4 need steadying during each treatment , and the older ones atleast during the first 2 or 3 sessions . we have in a few cases tried to make individual plaster casts into which the child is put during treatment , the cast including a headpiece with a frontal process to obviate any possibility of head movement . in practice , however , even the smallestchildren have been found to wriggle around in these casts human hands have had to help . the casts are usefuil , nevertheless , for steadying at least the trunk , and one escapes the otherwise necessary manoeuvre of binding the child on to the couch . children this can be done best by first wrapping the child tightly into a blanket , arms included . all cases - - and at each treatment - are set up by a medical officer , and during treatment , if necessary , the head steadied either by himself , by a radiographer , or by a nurse - or , if available , one of the parents . 
and by treatments lasting 16 or 57 days , but the number of cases observed is too small to confirm the impression that neither dose rate nor the total time are of critical importance within a wide range . 
irrespective of whether radium - moulds or deep x - rays were used , including one case in whom radium - moulds of increasing strengths were applied at short intervals within 5 months , the highest single dose being 3800 r . two main treatment schemes have been used : either a single " radical " course or repeated courses of deep x - rays , in each one of which a dose was given just sufficient to make the tumour disappear . this was usually achieved by doses of 2000 - 3000 r . , to be repeated as soon as there was renewed activity . the latter scheme is somewhat similar to that recommended by martin and reese ( 1936 , 1942 , 1945 ) , but in our hands it has never been successful , whereas the single radical course of treatment has given us outright cures . we have only once had the opportunity of treating a unilateral case ab initio . this was a girl , aged 3 years and 9 months , who came with a history of over 2 years but still only a comparatively small growth . 
ten months later , however , there was a large recurrence and the eye was excised . histology confirmed the presence of active growth . sometimes it has been necessary to continue the first course up to a much higher tumour dose . there was one case in our series where even the second eye carried a growth covering almost the whole of the retina - he had come to us with simultaneous affection of both eyes . after the excision of the first eye , which was completely filled by growth , a tumour dose of 5730 r . 
japha in this part of the body as anywhere else - but perhaps even with greater force - is one struck by the confirmation of the hypothesis most prevalent for the explanation of failures through over - dosage . 
we have not as yet given postoperative treatment to the orbit of the removed eye in bilateral cases . this may be advisable as a general policy in view of the ultimate fate of some of them , i.e. 
local recurrence even where no apparent extra - ocular extension was originally present , unless one regards these deposits as due to retrograde extension from the second eye , which by that time has got completely out of control . 
one should also remember , as duke - elder ( 1940 ) points out , citing meighan and michaelson ( 1938 ) , that there may be discontinuous spread in the nerve , so that the excised specimen ( even if part of the nerve is included ) need not necessarily show the extra - ocular extension which has in fact already taken place . carrying out this suggestion the contribution that the lateral fields will make to the retained retina or the enucleated orbit respectively and which will amount to a depth dose of about 20 per cent must be taken into account . this technique has been used in a recent case which had a recurrence in the excised orbit as well as growth in the second eye , and is also applicable in the " prophylactic " irradiation of a case in which bilateral enucleation has been performed . when we first collected these cases it appeared as if the unilateral cases treated post - operatively by irradiation would not be of very great interest because surgery alone might have been responsible for the good results . 
we have , however , in our series one case of recurrence within 6 / 12 of the operation ( this was treated by a combination of deep x - rays and implantation of radon - seeds , but recurred again and proved rapidly fatal ) , and the above - mentioned case , which may be regarded as having been inadequately treated in the post - operative period . this case had a remarkably long latent period of 5 years , and a very large dose of irradiation was necessary to arrest the growth . 
no growth was found on histological examination . one case of massive recurrence in the orbit with bone involvement after enucleation of the only affected eye failed to respond to combined irradiation by deep x - rays and implantation of radon needles ; another case , successfually treated , is of considerable interest . it is the case already mentioned which received a post - operative prophylactic dose of 660 r . 
by deep x - rays in 16 days for a recurrence after treatment by radon - seeds elsewhere ( tumnour dose estimated at 2000 r . ) , was complicated by chronic iritis and needed extraction of this the remaining eye 4 months later ( now 52 years ago ) - no growth was found on histological examination , as already mentioned . 
 ( in 57 days ) ; this was extracted 4 years ago and vision is only partial another cataract that was removed was obvious already 9 months after now . a dose of 3000 r . 
hfirst came under observation at the middlesex hospital in july , 1945 , at the age of 9 / 12 , having had his left eye excised elsewhere 3 months before ( histology showed retinoblastoma without involvement of the optic nerve ) , and at the same time a focus the size of a disc in the periphery of the right retina had been isolated by diathermy barrage . 
about a fortnight after this examination the boy began to vomit ( apparently in a rather projectile manner ) and became drowsy . lvhen examined again on 20.xi.46 there were signs of brain - stem involvement , and a course of deep x - rays directed there was some temporary improvement , but the at this region was started . child died within 3 months of the onset of the final stage . 
lumbar puncture during this time showed the presence of peculiar mononuclear cells in the cerebrospinal fluid , which in the light of the later post - mortemn findigs must be regarded as retinoblasts . 
m - 1 , a boy , 5 years of age , was sent to the middlesex hospital in 1929 from jersey , where 5 months previously his right eye had been removed for glioma retinae . 
a radium mould was applied as a " delayed post - operative measure , " but the surface dose when recalculated recently was found to have been only 660 r . 
 ( in 36 hours )  . nearly 5 years later there was a large swelling in the orbit whiceh was treated by x - rays in jersey ( details unknown ) and the swelling disappeared . 
a few months later a further course of x - rays was given for a " small hard bean - shaped swelling " in the lower half of the orbit . seven months after this the mass was again thought to be larger and the boy referred back to the middlesex hospital in september , 1936 . 
the boy was lost sight of during the war , but reported again as a young man in october , 1946 , that is , 10 years later , when he presented with marked telangiectases on the right cheek around the orbit and a small sinus over the zygomatic arch . 
the results of radiotherapy are summarized in table vii . ( a ) post - operative irradiation has been successful in the two cases where adequate treatment was given irrespective of whether a radium mould or deep x - rays were applied . in the one case described at length above , the first treatment , where 660 r . 
only were given , must be regarded as quite inadequate , but the recurrence which developed 5 years later responded well to a radical course . ( b ) primary irradiation . - the two cases treated by radium moulds and two of the three cases treated by deep x - rays more than 5 years ago are alive and e . 
for example , greenstein and his associates have shown that the activity of certain liver enzyme systems is affected to a considerable extent by the presence of a distant tumour , and of those investigated , liver catalase appeared to be the most sensitive . 
in fact a marked decrease in the activity of this enzyme has been observed in rats and mice bearing a variety of spontaneous , transplanted , and chemically induced tumours ( greenstein and andervont , 1942 )  . 
the evidence connecting the liver catalase depression with the presence of a tumour has recently been reviewed , both by greenstein ( 1947 ) and by weil - malherbe and schade ( 1948 )  . 
either the tumour may release some toxic material into the circulation , or its excessive nutritive demands may abstract from the circulation some substance essential for the maintenance of a normal liver catalase level . 
 consequently , quantities of tissue breakdown products are likely to be released into the circulation , and any toxic material associated with tumour growth may be due to such relatively non - specific processes . 
there is in fact evidence ( winzler and burk , 1944 ) that abnormally large quantities of circulating protein break down products such as proteoses and polypeptides are found in tumour - bearing animals , and these authors did tentatively suggest that liver catalase depression might be due to this cause . 
excessive nutritive demands of the tumour , greenstein and andervont ( 1943 ) showed that the depression was not simply due to the presence of growing tissue within the host , since catalase activity remained normal both in pregnant mice , and in mice bearing progres sively growing , subcutaneously implanted , embryonic tissue mash . 
 greenstein ( 1943 ) looked for a direct inhibitor of catalase in tumours , arul in the livers of tumour - bearing animals , but the results were all negative . 
greenstein interpreted his experiments as indicating that the affected livers simply contained less catalase than normal , rather than the same ' amount of catalase plus an inhibitor , and_put forwal ' _d the interesting l ' ! lj.ggestion that the decrease in activity was due to an interference with the _synthesis of the enzyme . 
however , no depression of liver catalase activity was observed even after long periods of administration of commercial peptone or sheep seru sheep serum in fact resulted in a rise in activity , the significance of which is unknown . 
further , these authors in vestigated the possibility that the depression might be due to the exaggerated protein requirements oi the tumour , by maintaining two series of tumour - bearing rats on high and low protein diets respectively , but no significant differential effect on the course of the process was observed . 
 most previous work appears to have been carried out with relatively massive tumours ( roughly within the range of 5 per cent to 50 per cent of body weight )  . 
 it is true , however , that while miller ( 1947 ) found that starvation up to about 7 days caused a marked depression in liver catalase level , he also showed that total liver protein fell in an approximately parallel manner . 
there appears to be a possibility that the effect is of a relatively specific nature , given only by malignant tissue , but the evidence presented in the literature does not ; enable a decision to be made on this queetion . 
so far as the results go they are in support of the supposition that tumours contain a substance not present , or - present in much lower concentration , in normal tissue , which is capable of depressing catalase activity~ animals . 
during the period of the experiment the diet of the animals consisted of " rat cubes " ( north - eastern agricultural co - operative society , aberdeen ) and water ad libitu as a routine the mice were starved for 12 hours before catalase determination  . 
 most of the work has been carried out with the transplanted tumour sarcoma 37 ( obtained from the chester beatty research institute ) , which grows rapidly in both strains of mice after subcutaneous inoculation . 
since , however , the non - protein nitrogen amounts to less than io per cent of the protein nitrogen and appears relatively constant , total nitrogen has been employed as a standard in this investigation . 
f measurement , but to construct a standard curve of enzyme concentration in arbitrary units ( using different volumes of the same liver homogenate ) against hydrogen peroxide decomposed in 4 minutes . 
since the rate of hydrogen peroxide decomposition falls off rapidly with increasing enzyme concentration , it was found necessary to construct a curve covering a relatively wide range of concentra tions . 
of 15 per cent w / v potassium iodide and 3 drops of 5 per cent w / v ammonium molybdate were then added , and the liberated iodine titrated with n / 20 sodium thiosulphate . 
all enzyme determinations have been made in duplicate , and , for routine estimations , the quantity of enzyme taken has normally decomposed between 1 / 3 and 2 / 3 of the substrate during the course of the reaction . 
adams determinations , catalase activity in arbitrary units has been calculated by sub stituting the quantity of hydrogen peroxide decomposed in the equation to this line , and the result divided by the nitrogen content in mg . 
this was obtained by dissecting out tumours previously inoculated into ff mice , removing any necrotic areas , and homogenizing the actively growing tissue in a loose - fitting ten broeck grinder just sufficiently to give a coarse suspension . 
it may be seen that at 24 and 48 hours after injection the level is considerably depressed , that it rises approximately to normal at 4 days , and then falls progressively until 14 days , when the experiment was terminated . 
 because af this , and also since the amount of the initial ( 24and 48 - hour ) depression is not approached again until the new tumours are of a considerable size , it seems not unreasonable to suggest that the initial drop is due to some material contained in the injected tumour homogenate , that this effect is rapidly exhausted ( 4 days ) and that only the second depression ( > 4 days ) is due to the presence of the new tumour . 
although the treated groups become very small when split up , the initial ( 24and 48 - hour ) percentage depression in catalase activity appears to be considerably greater in the males . 
the experiment was repeated with schofield albinos , using s37 taken from the same strain , and larger treated groups to enable the sex difference in initial effect to be examined further . 
3 , where it will be seen that there is an early depression in enzyme level , a rise approximately to normal in 4 days , and a subsequent progressive fall . 
each point represents 6 tumour - bearing animals , and has been obtained from the arithmetic mean of the catalase level for the treated animals , and the arithmetic mean of the appropriate control group . 
this method of presenting the experimental data is by no means ideal , but the individual results would be very difficult to obtain , since no informa tion is available regarding the original oatalase level of a tumour - bearing animal . 
according to the graph , these authors obtained a rapid fall in 2 days , after which the level remained approximately constant until 4 days , and then fell once more . 
the salient point is that their results cannot be separated into " early " and " late " effects in the absence of the 4 - day rise to normal . 
their tumour must have grown extremely rapidly since they obtained a 90 per cent depression in 7 days , and greenstein and ander vont ( 1942 ) probably employed the usual technique of grafting small pieces of tumour subcutaneously rather than injecting a homogenate . 
it is fairly obvious , from the results already given ; that if the onset of tumour growth is sufficiently rapid to affect the catalase level at 4 days , the rise to normal after the initial drop will be obscured , or perhaps entirely obliterated . 
 a number of normal tissues have been coarsely homogenized ; and injected subcutaneously into male mice , which , as has been already pointed out , are more sensitive than females . 
 since the initial ( 24 and 48 hour ) depression is of primary interest , the effects on catalase level have been followed over a period of 4 days , the results appearing in table ii . 
the results in table ii show that a 24and 48 - hour depres sion was observed , although an appreciably smaller one than with s37 , and that the catalase level rose to normal at 4 days . 
 because of the much delayed onset of tumour growth , and because " takes " only occurred in a.bout half the animals it is not possible to state definitely whether the females showed a greater resistance to tumour growth , although there appeared to be a tendency in this direction . 
140 25 carcinoma 63 105 21 101 16 113 14 123 22 131 34 101 13 75 19 145 28 125 22 108 26 113 17 123 29 127 19 95 13 79 13 92 33 113 33 116 14 114 19 128 17 131 27 125 20 95 11 117 6 an experiment with coarsely homogenized necrotic s37 tissue yielded the following result : no significant depression was observed at 24 hours , but by 48 hours the level was considerably below normal , beginning to rise at 4 days . 
 since attention does not appear to have been drawn to a sex_ difference in normal mouse catalase levels , some results for males and females drawn from the same batches are given in table ill . 
 80 21 123 18 90 14 as pointed out in the introduction , the alternative mechanisms by which tumours may cause a catalase depression can be given thus : discussion . 
it is hardly possible that this early depression can be a result of any nutritive demands on the organism , and can only be due to some substance or substances present in the injected tumour tissue . 
assuming that the early and late depres sions are not entirely unconnected , it is suggested that the tumour is exerting its effect on catalase by continuously releasing this material into the circulation . 
of homogenized tumour tissue ( administered by the relatively inefficient method of subcutaneous injection ) is sufficiently active to depress the catalase level very considerably for approximately 2 days , it is probable that only a comparatively small continuous production would be required to account for the observed results . 
further , the point at which the graph flattens corresponds approximately to the tumour weight at which necrosis commences , and , for example , a tumour weighing 2 to ; 3 g . 
also , after subcutaneous injection , these tumours grow in the subcutaneous space and do not , as a rule , perforate the abdominal wall until they weigh 4 to 5 g . 
consequently little or no normal tissue can be destroyed by the growth of the tumour ; and even if this process were occurring to some small extent , the flattening of the curve at a given point would be unexplained . 
schultz and kuiken ( 1941 ) briefly mention that normal male rats have higher liver and kidney levels than females , and serfaty ( 1946 ) , working with the erythrocytes of fowls , found the level to be higher in cocks than in hens . 
 it seems reasonable to suppose that the maintenance of a normal catalase level is to some extent under hormonal control , and the different initial response of males and females to tumour tissue may indicate that the primary effect is not on the liver . 
these graphs make it clear that not only does homogenization enhance the initial depression ( as might be expected if the effect is due to some substance contained in the tumour cells ) but that such a procedure 194 d . 
their results show only a progressive fall in catalase level after the tumour implantation , and provide no evidence which could suggest that tumour tissue contains a toxic product capable of depressing liver catalsea activity . 
in some experiments the arithmetic mean of the results for the treated animals have been slightly lower than the arithmetic mean values for the controls , in others , slightly higher . 
it is impossible at present , therefore , to say whether tissues are capable of causing a slight depression , or whether normal the effect is wholly specific to tumours . 
after this process the material could be compared with similar fractions from normal tissue , and a sufficiently large dose given to show whether the cata ] ase depressing material is present at all in normal tissue . 
 it is already known ( greenstein and andervont , 1942 ) that , in general , the greatest falls in liver catalase level are produced by rapidly growing tumours , and , in fact , certain s ] ow - growing tumours produced little or no effect . 
 in the present investigation it appears that s37 tissue , which grows readily , gave a greater 24 and 48 - hour depression than carcinoma 63 , which does not . 
 following the subcutaneous injection of homogenized sarcoma 37 tissue into two strains of mice , the liver catalase activity fell significantly at 24 and 48 hours , subsequently rose to normal by the 4th day , and diminished again during the growth of the new tumours . 
there was also a sex difference in the initial response to the injection of tumour material , the males , which have the higher normal level , being more sensitive . 
bielschowsky. from the , hugh adam cancer research department of the medical school and the new zealand branch of the british empire cancer campaign , university of otago , dunedin . received for publication april 7 , 1953 . judging from the literature , adenomata occur more frequently in the pituitaries than in the thyroids of aged rats . 
at the routine autopsies of 154 albinos of the wistar strain , 41 of which were males , 86 intact and 27 spayed females , 24 cases of adenoma of the pituitary were discovered . seven of these occurred in the males , 16 in the intact females and only one in an ovariectomised animal . the average age of these rats was 2 years . 
adenomata of the thyroid were found in 5 animals , 4 times in combination with neoplastic lesions of the pituitary . post - mortem examinations performed on old rats of a more recently acquired hooded strain have furnished three additional cases of tumours of thyroid and pituitary . 
the diet consisted of a dry mixture of bran 30 per cent , pollard 35 per cent , meat meal 15 per cent , maize meal 15 per cent and bone flour 5 per cent , supplemented by wheat and kibbled maize , and once weekly by green vegetables and cod liver oil . drinking water was supplied in liberal amounts . 
the weight of the animals was recorded at fortnightly intervals and they wer6 sacrificed when loss of weight and general appearance indicated ill - health . at autopsy the pituitaries were immediately transferred into a pre - weighed bottle containing about 2 ml . 
when treated with gomori 's fuchsin aldehyde reagent , the cytoplasm of the angular cells and especially their granules stained purplish - violet . in other words , these cells strongly resembled and gave the staining reactions of those basophils which purves and griesbach ( 1951a ) named " thyrotrophs . " therefore the tumour is considered to be a basophil adenoma formed by thyrotrophs . in the part of the anterior lobe outside the basophil adenoma the basophils were considerably increased in numbers . angular types again predominated , but here vacuolated forms , extremely rare within the tumour , were numerous . these cells were identical with those seen after partial thyroidectomy . they gave a positive pas reaction of varying intensity , and with the gomori stain some were found to contain coarse violet - purple granules . the large round gomori 206 f . 
5 , the larger of the two protrudes above the anterior surface and is closely connected with the pars internmedia : the other , just appearing in the section , bridges the pituitary cleft and is situated laterally . 
the pituitary was of irregular shape with a small this was a well defined basophil adenoma , the haemorrhagic brownish area . tumour cells giving the same staining reactions as described above . 
the neoplastic changes found in the hypophysis and thyroid of the younger animal were of microscopic size . in the slightly abnormally shaped anterior lobe numerous thyroidectomy cells and also multiple nodules formed by atypical basophils were present , the pars intermedia being normal . 
normal anterior lobe tissue was recognisable in the periphery as a narrow rim surrounding approximately half of the circumference of the tumour . radiating from this rim compressed strands of predominantly acidophilic and chromophobic elements were seen between areas of tumour , an indication that the neoplasm had arisen from different foci . intermediate and posterior lobes appeared normal . 
the cells composing the tumour were large , showed great variation in size and shape , had sharply defined cell borders and vesicular nuclei with one or more large fuchsinophilic nucleoll . multi - nucleated and tumour giant cells were rather numerous and so were mitoses . 
when stained by the pas technique or with gomori 's aldehyde fuchsin after long search an occasional only in this respect , cell was found having pas or gomori positive granules . did the adenoma differ from those described above . in papanicolaou preparations the cytoplasm stained faintly with light green . the histology of the thyroid was that of an inactive gland . 
many mitoses were found in this nodule , considered to be a benign pheochromocytoma . rat 8 , a 26 months old male , was killed because of the presence of an abscess otherwise the animal was in an excellent in the subcutaneous tissue of the neck . state of health and weighed 460 g . 
the first question to be answered is : which cells produce the thyrotrophic hormone and the second , how many types of basophils occur in the anterior lobe of the hypophysis . 
as to the second , romeis ( 1940 ) described two types of basophils both stainable with aniline blue but distinguishable by their affinity to creso - fuschin or resorcinol - fuschthe type stained by these fuchsin dyes is the beta cell , the other is the delta cell of romeis . 
as shown by halmi ( 1950 ) another elastica stain , gomori 's fuchsin aldehyde reagent , also differentiates between two types of basophils , whereas most other techniques like pearse ( 1952a ) does not papanicolaou 's or gram 's method stain all basophils . seem to attach great significance to these different tinctorial qualities and adheres to a unitarian view . 
now the pathogenesis of the basophil tumours can be discussed . chronic iodine deficiency lowers the thyroxine level in time , to which the pituitary responds with an increase in thyrotrophic cells . this compensatory hyperplasia progresses towards the formation of tumours , in this connection it might be which in some instances reach considerable size . mentioned that proliferating normal thyrotrophs , as observed by guyer and claus ( 1937 ) , tend to aggregate in clusters , a mode of growth which might be favourable to nodular hyperplasia , the first stage in adenoma formation . 
the adenoma of this animal was functionally inactive as judged by the appearance of the thyroid which was that of a resting gland . also cells giving a positive reaction for glycoprotein were virtually absent in this tumour . the most convincing evidence for funttional activity is provided by rat 4 . the large pituitary tumour of this animal contained numerous pas and gomori positive elements and its thyroid showed the most pronounced signs of stimulation . in addition , in the pituitary of this animal , so little normal anterior lobe tissue was left that it seems most unlikely that this small rest could have secreted amounts of thyrotrophin large enough to induce a four - five fold enlargement of the thyroid . finally the pituitary lesion of rat 8 has to be considered . in this case the morphological evidence was more in favour of hyperplasia than of neoplasia . here an agglomeration of thyrotrophs had persisted in one area despite the fact that ki had been supplied for 7 months . in the rest of the anterior lobe these cells were found in normal numbers , as was to be expected , and the thyroid had undergone involution . rich glycoprotein content of the cells forming this aggregation was probably due to storage and not a sign of secretory activity . the anomalous behaviour of these cells suggests that they were no longer normal thyrotrophs . the thyroid tumours observed are , in the writer 's opinion , due to stimulation by elevated amounts of thyrotrophic hormone . the stimulus for the increased secretion by the pituitary was a deficiency of thyroxine due to impaired synthesis by an inadequate content of iodine in the diet . in six instances the thyroid tumours were found in activated and twice in resting glands . the latter occurred in animals which had received a supplement of ki for several months and are considered to be evidence of past stimulation . these neoplasms differed morphologically from those observed in stimulated thyroids in the same way as the thyroid adenomata found during administration of thiouracil differ from those seen after the treatment with the goitrogen has ceased . 
their epithelium was rather low , and cystic follicles filled with colloid were a prominent feature . to summarise the pathogenesis and structure of the thyroid adenomata observed is similar to that of the tumours induced by goitrogens which act by blocking the synthesis of thyroxine . the conception that thyroxine deficiency is the ultimate cause of the syndrome described is strengthened by the following observations . fischer ( 1926 ) , writing from bern , switzerland recorded two cases of pituitary tumours found in aged female rats . 
the thyroids of both animals contained multiple tubular adenomata , and in one an adenocarcinoma was also present in this gland . the rats belonged to wegelin 's colony in which goitre was endemic fischer 's paper was published long before the gonadotrophic and thyrotrophic hormones had been discovered . she stressed , however the similarity of the pituitary tumour cells with the ele212 f . 
bielschowsky ments which appear in the rat 's hypophyis after castration or thyroidectomy ; and considered the neoplasms to be carcinomata formed by " castration " cells fischer believed that although the ovaries of one of her animals were normal . the neoplasms originated from the pars intermedia or tuberalis . " spontaneous " tumour formation occurring simultaneously in thyroid and pituitary of rodents seems to have been observed only by fischer and by the writer , but one sees this syndrome under experimental conditions most frequently in animals t ' reated with so purves and griesbach ( 1951a ) mention goitrogens for prolonged periods . a basophil adenoma of a rat treated with methythiouracil for two years . basophil adenomata occur also in thyroidectomised rats treated with acetylaminofluorene into the same class belong also the pituitary tumours ( unpublished results )  . discovered by gorbman ( 1950 )  . 
they appear in mice exposed to high doses of radioactive iodine , but can be prevented by the administration of thyroxine ( goldberg and chaikoff , 1951 ; gorbman , 1952 )  . furth , gadsden and upton ( 1952 ) reported that transplants of such tumours contain large amounts of thyrotrophic hormone . 
1 , the method of analysis employed compensates fully for difference in " size " of the pattern analysed , and the p values for grade and intergrade patterns can therefore be regarded as strictly comparable . if we regard p < .05 as evidence of abnormal patterning , then a glance at the table shows that abnormal patterns occur with considerable frequency . this is best seen by comparing the frequency distribution of the 224 grade and 192 intergrade p values of the table with the strictly equivalent frequency distribution of the 4000 random series ( cruickshank , 1940 )  . 
1. statistical maps often present data by the use of " grades . " the several counties in any one grade may be scattered " at random " over the map , or may be juxtaposed to form small or large these varying types of distribution are described briefly as " patterns . " the exact " groups . " type of pattern to be expected from random distributions has been determined experimentally ( 4000 patterns ) , and from these experiments the " expected frequency " of any specific type of rare types of patterns , i.e. 
patterns with low expected frequency , are observed pattern is known . described as " highly developed . " on cancer maps highly developed patterns occur with excessive frequency . indeed , " statistically significant " patterns , i.e. 
2 and 4 will show that p values across the gradings ( 1 - 12 - 1 - 23 7 ) give rise to curves with clearly defined trends , which include the develop114 d . 
2. the " intensity " of a regional influence can be expressed in terms of the " degree of development " of patterns found within its zone of action ; the more non - random the pattern the more powerful the influences at work . the analysis is best shown graphically ; the expected random frequency of the 7 grades and 6 inter - grades patterns of each map are plotted out on an i * erted logarithmic scale so that " peaks " show high degrees of pattern development - that is , powerful regional influences . the striking feature of the curves so formed is their essential simplicity . in fact they are almost e.g. 
that a significant " zone " is not always associated with a significant peak . in such cases the individual counties of the zone each show a deviation from the mean > 2 s.e. 
that curves of type 2 which develop a peak before the extreme grades and then fall off are usually associated with maps in which the highest ( or lowest ) grades do not form a single zone , but break up into two or more sub - zones , e.g. grade 7 may appear as three separate zones , unrelated to each other , but all related to grade 6 ,  . . 
the frequency of effects " increasing " and " decreasing " the rate are shown separately ; the frequency of effects " modifying " the rate ( significant ] y ) is the sum of these two . in the absence of regional influences we anticipate that a county will participate in " random " significant pattern formations in about 1 / 20 cases , i.e. 
 ( stocks ' data )  . now , if the distributions and trends in each of the 28 maps are unrelated , the result of combining these inter - random distributions should be to flatten out the whole pattern ( irregular multiple hillock picture )  . 
on the other hand , if they are related , their combination may be expected to result in some definite composite pattern or configuration ( hill and valley picture )  . from the entries of table vii three contour maps were prepared ( appendix 7 ) ; these are shown in fig . 
we may therefore conclude that county boundaries have no essential significance in relation to regional influences . in fact these influences behave in every way as continuous variables , and their variations in intensity are most appropriately depicted by means of contour - lines on the surface of the map . to depict these regional influences by contours may serve to drive home another of their characteristics as revealed by this study , viz . 
cornwall , somerset and dorset . while the majority of counties meet at a common county boundary , occasionally they meet only over a very narrow range , the so - called " point contacts " ( solid circles on map )  . 
where the county boundary is a river or an estuary the counties may fail to make a de facto cantact , and yet , it may be necessary to consider these as " touching " for the purpose of studying regional influences ( solid rectangles on map )  . note the distinctly higher values of the contact numbers of the inland counties as contrasted with those of the coastal counties . the mean contact number ( c ) works out at 5 - 12 . , , ~n this is an important constant in theoretical formulae , e.g. 
mark on the glass with grease pencil all " grade 1 " counties . remove glass template and place on white sheet . analyse arrangement of marked counties ; record ; clean off wax pencil mark with chloroform . replace on map and proceed similarly to work and analyse " grade 2 " counties , and so on . 
8 , in conjunction with appendix 4 , indicates the probable , simple explanation , viz . that estimates of the degree of pattern development of an organized pattern must generally fall below the true value when they are based on the examination of only part of the pattern - for the simple reason that the relation of one " piece " of the pattern to a neighbouring " piece " is thereby overlooked . 
the process of " intergrading " was evolved to deal with this contingency . thus , to explain the observed fact that the p grade greater than p intergrade we must assume that the mean " pattern " associated with regional influences covers an area greater than that of a mean grade , i.e. 
regional influences decreasing cancer exist alongside the " positive , " in fact these two types of influence , both of which are represented by peaks and zones , occur with equal negative effects must not be regarded as merely due frequency ( table vii )  . to the absence of positive effects , for the observed type of trend and degree of patterning associated with negative zones is of a much higher order than is to be expected from the mere absence of positive effect . it seems that there must be some general factor other than regional which operates to produce a definite incidence of cancer . regional influences are not themselves the cause of cancer , but merely impress their effect , positively or negatively , upon this general factor . i wish to express my thanks to n . 
jensen. frm the danish cancer regi8try under the national anti - cancer league , kobenhavn 0 . received for publication january 31 , 1953 . in 1947 clemmesen and busk reviewed the material of the danish death certificates with a diagnosis of cancer of the lung from the years 1931 to 1945 ( clemmesen and busk , 1947 )  . 
they found an increase in the numbers for males , particularly pronounced in copenhagen , the capital , less striking in provincial towns , and somewhat smaller for rural areas . however , the incidence of cancer of the lung among persons subject to routine examination in the central tuberculosis station for the city of copenhagen did not reflect the heavy increase in mortality found in the city as a whole . 
diagnose a number of cases of cancer of the lung , so that the graph illustrating the incidence rates in its material should be changed , as shown in fig . 
1. during the years up to 1950 the increase in mortality rates for cancer of the lung among men in the various areas of denmark continued , and from fig . 
women. of the disease , and only to a small extent attributable to improvements of diagnosis , which can be expected to cause a proportional increase for both sexes in the number of cases diagnosed . 
the possibility that the deciding factor might be an increase in medical attention for all categories of diagnosis can be excluded because the patients from the tuberculosis station were unselected and referred directly for diagnosis with a view primarily to a disease different from bronchial carcinoma , and finally were examined in a uniform way . further analysis of the material from the danish cancer registry confirm the results from mortality statistics ( clemmesen and busk , 1947 ) that the increase in incidence of cancer of the lung among men is particularly strong for the relatively younger age classes ( clemmesen and nielsen , 1952a , 1952b )  . this seems to speak against the assumption that atmospheric pollution is a causative factor of primary importance to cancer of the lung as far as denmark is concerned . if this were the case we would expect an increase in incidence for all age classes . it might also be expected that the windy climate of copenhagen could cause regional differences in incidence of the disease within the city analogous to the findings of stocks ( 1952 ) for london , but in fact it appears that the distribution of cancer of the lung among men in copenhagen varies with the social level expressed in terms of annual house rent , much like cervical cancer of the uterus being most frequent in the classes of subdistricts with the lowest level of house rent , although the single subdistricts show no such parallelism . however , there is no tendency for leeward areas to exceed the weatherside with regard to incidence rates for carcinoma of the lung ( clemmesen and nielsen , 1951 )  . thus , it would seem that the main reason for assuming atmospheric pollution to be causative to cancer of the lung in denmark would be the excess of cases in towns , particularly in copenhagen . 
5 represents mortality rates at various ages for lung cancer among men in copenhagen arranged in quinquennial cohorts born in the period about the years given in the diagram . it would seem reasonable to assume that the carcinogenic influences determining the incidence of cancer of the lung , whether they be of customary , occupational or hormonal character , will not begin before the age of 15 or perhaps a few years later . it appears from the tables that the cohorts of highest mortality at an conearly age do not show an increase in rates until after the 35th year of age . sequently it will be justifiable to assume a minimal period of about 20 years from the beginning of the influence to the death of the patient from cancer of the lung under the conditions usual in copenhagen . it follows logically that if we assume a later or earlier beginning of the carcinogenic influence we must respectively shorten or prolong the assumed period with a corresponding number of years . it should also be remembered that we must allow for wide variations either way . under these assumptions and from the observations illustrated in fig . 
5 that the graphs for the quinquennial cohorts do not coincide as they would for most other sites of cancer , but are moving to the left , although now at a decreasing pace . this would not be explained by assuming that all cohorts were from a certain age subject to some carcinogenic influence unless we add that the influence was strengthened at some point of time , or during a limited period of years . now it is seen that the result of the carcinogenic influence increased particularly for men born between 1875 and 1885 , while the effect on the following cohorts progressed at a slower rate . 
2 , it will be seen that the differences in the level of the graphs indicating crude mortality rates for cancer of the lung between capital , provincial towns and rural areas can be ascribed to a later beginning of the rise in the latter categories , i.e. , 8 years for provincial towns and 10 for the rural areas , which is in full conformity with the result of the cohort analysis . hence it appears that the assumption of atmospheric pollution as a cause of cancer of the lung in denmark in order to explain the differences between towns and country is unnecessary , if we suppose that the carcinogenic influence began a few years later in the provincial towns and a few years later still in the country . quite apart from the etiological implications of our cohort study it is in the field of practical hygiene we find the widest consequences of the diagram of fig . 
some important records of pedigrees , showing apparent . transmission from mother to daughter , were published nearly a century ago . the most remarkable was recorded by broca ( 1866 ) , in which four generations of females had the disease . in spite of evidence brought forward by a great many observers that mammary cancer can frequently be found affecting several of the female members of a family group , doubt , still remains as to whether heredity plays any significant ' aetiological part . this doubt arises because of the great prevalence of the disease in the general population , where it is responsible for nearly 3 per cent of all female deaths . 
with so comm ' on a condition , it is difficult to demonstrate convincingly that the occas ' lonal familial conoentration is not merely the result of a random distribution of cases . to obviate this uncertainty , most investigators in recent years have collected a series of cases , noted the incidence of similar disease among their relatives , and compared it with the corresponding incidence among a control group of cases free from the disease , selected so far as possible at random . in spite of elaborate precautions , - the difficulties , involved in obtaining a satigfactory control group of family histories to match those of the propositae , have repeatedly proved almost insuperable . 
the result is that many workers ( hanhart , 1943 ; passey , 1942 ) still ' consider that there is , insufficient evidence to prove the reality of familial transmission of mammary cancer or of aay type of human ma " lignant disease . stocks and karn ( 1933 ) found no evidence that a history of cancer in relatives increased the risk of cancer to anymeasurable extent . several extensive surveys have been published , all of which give some evidence for believing that mammary cancer is unusually prevalent amon the mothers and sisters of affected cases . 
the patients were attending either university college ilospital or the london hospital , and they were personally interviewed . all possible hospital records and reports were searched or checked by correspondence . this procedure applied b6th to the propositae and to any of their relatives who were reported to have suffered from malignant disease . unfortunately , in a number ' of instances , records had been destroyed by enemy action during the war . ideally , the death certifica ' te of every relative believed to have died of malignant disease should have been obtained , as corroborative evidence , but th ' is we have not been able to do . 
the distribution of these 116 " familial " cases and the mean age of onset of their illness ( 5 1 0 years ) was extremely similar to that of the this finding does not support jacobsen 's remaining " non - familial " cases . assertion that familial cases have an earlier onset than others . 
the infertility ratio , 91 out of 408 , or 22 - 3 per cent , significantly exceeds the value of 17 - 3 per cent for married women of the same mean age given by the registrargeneral ( 1938 ) , and supports the view that nulliparity is an etiological factor . the mean age of the patients when first interviewed for purposes of this this indicates that they had , on the average , lived survey was 55 - 2 years . undoubtedly three - and - a - half years since first gigns of the disease had appeared . the survival of the patient was a property , which determined her inclusion in the investigation , and the longer the survival , the more probably would she be selected as a proposita . 
the date of death and the age at the time were recorded in a few instances the dates were approximate , but could hardly for each case . be more than a few years in error . 
the expected proportion of deaths due to mammary cancer and other types of malignancy in each year and at each age can be obtained on the basis of the general population statistics . 
the distribution of deaths by year and age is shown in table iii . from ' this table the number of deaths due to mammary cancer if the women had been subject to the mortality in the general population was estimated at 11 - 17 , a figure significantly less than the observed 25 . 
51 observed as compared with 48 - 76 expected . there were 102 mothers still living at the time of investigation a ' nd , of these , six were know - n to be under treatment for mammary cancer while four had some other type of malignant disease . 
hence any likeness of onset age of mammary cancer in sisters is not peculiar to this type of malignancy . another interesting correlation concerns the sites affected in pairs of sisters and other relatives . 
the conversion of the cohesive subcutaneous tumour forms into a homogenous suspension of free cells may be due either to a selective proliferation of a few round cells present in the solid tumour or to a gradual adaptation to their new environment of the original spindle or polymorphous cells typical of sarcomas . 
two mouse ascites tumours were used for the experiments , the s 37 sarcoma and the t 2146 tumour which originated as a benzpyrene induced epithelioma but has both these tumours were developed since undergone sarcomatous transformation . from the subcutaneous form by craigie at the imperial cancer research fund laboratories . the paper is divided into three parts : i . 
no tumour smears of cell suspensions were nodules were present in the abdominal cavity . obtained by withdrawing peritoneal fluid at daily intervals from 24 inoculated mice and staining either by the feulgen method or that of papanicolaou . 
the whole of the ascites fluid was withdrawn and centrifuged at low speed for 3 minutes , which caused the heavier tumour cells to sink down while leucocytes and erythrocytes , if present , formed a top layer which could easily be removed with the supernatant fluid . 
the culture medium consisted of equal parts of fowl plasma , ascites fluid and chick embryo extract to which one drop of either s 37 or t 2146 tumour cell suspension was added . 
the undulating movements of the peripheral cytoplasmic area become more rapid , spikes and blunt processes are pushed out and withdrawn in quick succession . finally the cells elongate and assume pear and then spindle shape . for several hours after incubation the process may be reversed and spindle cells are seen to return to the round shape . examination of the fixed and stained specimens confirms the observations made on the living cells and shows that the process of transformation continues for 24 hours after incubation . 
the latter may represent a differentiated form which can no longer proliferate actively in contrast to the free round elements from which they are derived . to decide this question cultures of ascites tumour cells were inoculated subcutaneously into mice before and after 24 hours ' incubation , i.e. , before and after establishment of the spindle forms . 
the clots were cut into strips 2 x 4 min size containing approximately 2000 cells , and these were inoculated subcutaneously into the flank of c3h mice 2 - 3 months old . 
and that mitosis is only a third of that found in round cell grafts . after 24 hours the elongated cells revert to the round form but mitosis remains low until the fourth day ( fig . 31 , dotted line )  . 
the development of the implants can be followed from an early stage , and is described from 5 hours after inoculation until the fourth grafts derived from spindle cells showed a lower mitotic rate day of growth . after 5 hours in vivo , a significant delay in the appearance of tumours , and were of smaller size as compared with tumours obtained from round cells . 
the recently developed methods of detection and determination of polycyclic hydrocarbons in micro - gram quantities have provided a more sensitive way of analysis than has yet been employed ( cooper , 1951 , 1953 ; wedgwood and cooper , 1951 , 1953 )  . in view of the suggested connection between carcinoma of the lung and smoking ( menary , 1932 ; schrek , baker , ballard and dolgoff , 1950 ; mirs and porter , 1950 ; dor and hill , 1950 ; rigden and kirschoff , 1952 ; sadowsky , gilliam and cornfield , 1953 ; wynder , graham and croninger , 1953 ) and the estabhshed presence of carcinogenic hydrocarbons in combustion products , it was decided to use these methods to examine cigarette smoke . 
on the other hand several investigators have devised apparatus to collect smoke produced in conditions resembling closely those of normal smoking ( bradford , harlan and hanmer , 1936 ; wenusch and sch6ller , 1938 ; w , ynder , graham and croninger , 1953 )  . the apparatus we have employed . 
the tap c with a glass rod sealed on to it was turned on for the period necessary to simulate a " draw " made by a snioker by means of a cam attached to the periphery of a 3 inch pulley wheel , d . the glass rod was held in the groove of the puuey by means of a stretched rubber this wheel was driven by a gear train from a smar electric motor , the speed band . of which was variable by adjustment of a " variac " auto - transformer connected to the altemating current mains . other cams could be attached to the wheel and thus the length and frequency of the " draws " were adjusted . in the u - tubes suitable solvents were placed so that the smoke was made to bubble tbrough them and the condensable material separated from the gas . a packing of 10 cof pyrex glass wool in the second u - tube served to remove the both u - tubes could be surrounded by beakers last traces of condensable matter . full of solid carbon dioxide to assist in the condensation , but it was found that strong cooling was not always necessary to effect complete removal of the disperse phase . 
each , the average time of draw is about 2 seconds and the average time of smoking such a cigarette to a short butt ( about 1 - 5 clong ) is 12 minutes . these conditions are attained by oiir apparatus when adjusted to give a 2 second draw every 45 seconds with a negative pressure of 25 cwater . 
air. smoke obtained in this way is an aerosol with a viscous fiquid as the disperse phase and a gas , consisting of a mixture of unburnt air , carbon dioxide , carbon monoxide , water vapour and traces of other gases as the dispersing medium . the average amount of condensable material from 100 c ' igarettes weighs about 4 g . we have concemed ourselves only with the condensable disperse phase whicli in bulk , after the evaporation of the solvent ( acetone , chloroform or cyclobexane ) used to trap it , is a dark brown viscous fluid . preparation of apparatus and materials . the solvents ( cyclohexane , acetone , benzene and chloroform of reaaeint grade ) were distilled in an all - glass apparatus , rejecting the first and last tenths . this product was then distilled through a dufton column and corected over a range of - 9jo c . 
the residues were not fluorescent in ultra - violet hgbt . all the glass apparatus employed was cleaned bv immersing overnight in chromic - sulphuric acid mixture , washing and drying . 
500 ultra - violet spectrophotometer . graphy the eluates were examined at a few definite wavelengths only and hydrocarbons were identified by specific absorption peaks and the order in which they appeared in the eluates . 
the solvent was then removed by distillation , the residue boiled twice with cyclohexane ( 5 to 10 ml . ) and the solutions decanted off after cooling . the - united cyclohexane solutions were then shaken with three quantities of 2nsulphuric acid and then with three quantities of 2nsodium hydroxide . solution thus freed from basic and acidic substances was reduced to about 5 ml . 
the eluates from the colunm were examined by the method of wedgwood and cooper ( 1953 ) namely by searching for absorption peaks at wavelengths known to be specific for the various polycyclic hydrocarbons . 
usuahy the initial chromatography only revealed the hydrocarbon peakb as inflexions againbt considerable background absorption and the combined filtrates suspected of containing the compounds had to be passed through fresh columns in order to reveal their presence more satisfactorily . anthracene was recognised by its peak at 376 ma . 
and it was always followed closely by the appearance of a peak at 355 m / % , reveahng pyrene . the compounds were determined bv making the cyclohexane solutions up to known volumes and then measuring the height of the peaks by the base line technique . for this purpose two convenient points on either side of a given peak calibration of the peak heights above the base were used to construct a base line . line was effected by using standard curves of the authentic hydrocarbons prepared from solutions of known strength . the background absorption interfered considerably in these experiments and various attempts were made to reduce its effect . 
when hydrolysis was effected on the cyclohexane extract of the whole smoke , the background absorption was even greate ' r than before , indicating that some hydrolysis products of the smoke constituents were entering the hydrocarbon sections of the column . the presence of pyrene and anthracene indicated in these experients was confirmed by their chromatographic behaviour relative to added methyl ethers . relatively few compounds , absorbing hght in the region studied , are associated with the polycychc hydrocarbons on aluniina columns . 
the peaks used for recognition of the various compounds are labened with their wavelengths . it will be noted that a sequence of peaks of added calibration materials interspersed with the recognisable peaks of substances originary present , gives an infalfble method of identification and determination . 
the results of a number of analyses utilising in all 250 cigarettes of one popular brand showed quantities of anthracene and pyrene equal to 10 - 2 and 9 - 0 itg . 
and to paraffms which he states are present in t e original tobacco and are vaporised unchanged during smoking . acetylene has been determined in tobacco smoke by weighing it as cuprous acetyhde ( fishel and haskins , 1949 )  . its pyrplysis may give a ready explanation 300 b . 
was attained at the hottest part of the periphery . more satisfactory measurements were made by using a calibrated coppernichrome thermocouple which was threaded through the cigarette from one side to the other . after sealing the holes by means of small pieces of paper , the cigarette was smoked in the normal way and the temperature recorded from time to time . 
the temperature rose rapidly when the burning end advanced towards the couple and , when the glowing material was in contact with the couple , a temperature of about 650 c . 
each time air it thus appears that the highest temperatures during was being drawn in . suction are confined to the surface and that the main body of the hot end is always at a temperature between 650 and 700 c . similar temperatures were recorded when a cigarette with a thermocouple inserted was smoked in the mouth . these temperatures are sufficiently high for pyrolysis of simple compounds to polycyclic hydrocarbons . 
the temperatures recorded by us agree remarkably closely with those obtained independently by wynder , graham and croninger ( 1953 )  . our investigations upon the composition of tobacco smoke are being continued . the authors wish to acknowledge the helpful and kindly criticism given by professor sir e . 
for example , greenstein and his associates have shown that the activity of certain liver enzyme systems is affected to a considerable extent by the presence of a distant tumour , and of those investigated , liver catalase appeared to be the most sensitive . 
in fact a marked decrease in the activity of this enzyme has been observed in rats and mice bearing a variety of spontaneous , transplanted , and chemically induced tumours ( greenstein and andervont , 1942 )  . 
the evidence connecting the liver catalase depression with the presence of a tumour has recently been reviewed , both by greenstein ( 1947 ) and by weil - malherbe and schade ( 1948 )  . 
either the tumour may release some toxic material into the circulation , or its excessive nutritive demands may abstract from the circulation some substance essential for the maintenance of a normal liver catalase level . 
 consequently , quantities of tissue breakdown products are likely to be released into the circulation , and any toxic material associated with tumour growth may be due to such relatively non - specific processes . 
there is in fact evidence ( winzler and burk , 1944 ) that abnormally large quantities of circulating protein break down products such as proteoses and polypeptides are found in tumour - bearing animals , and these authors did tentatively suggest that liver catalase depression might be due to this cause . 
excessive nutritive demands of the tumour , greenstein and andervont ( 1943 ) showed that the depression was not simply due to the presence of growing tissue within the host , since catalase activity remained normal both in pregnant mice , and in mice bearing progres sively growing , subcutaneously implanted , embryonic tissue mash . 
 greenstein ( 1943 ) looked for a direct inhibitor of catalase in tumours , arul in the livers of tumour - bearing animals , but the results were all negative . 
greenstein interpreted his experiments as indicating that the affected livers simply contained less catalase than normal , rather than the same ' amount of catalase plus an inhibitor , and_put forwal ' _d the interesting l ' ! lj.ggestion that the decrease in activity was due to an interference with the _synthesis of the enzyme . 
however , no depression of liver catalase activity was observed even after long periods of administration of commercial peptone or sheep seru sheep serum in fact resulted in a rise in activity , the significance of which is unknown . 
further , these authors in vestigated the possibility that the depression might be due to the exaggerated protein requirements oi the tumour , by maintaining two series of tumour - bearing rats on high and low protein diets respectively , but no significant differential effect on the course of the process was observed . 
 most previous work appears to have been carried out with relatively massive tumours ( roughly within the range of 5 per cent to 50 per cent of body weight )  . 
 it is true , however , that while miller ( 1947 ) found that starvation up to about 7 days caused a marked depression in liver catalase level , he also showed that total liver protein fell in an approximately parallel manner . 
there appears to be a possibility that the effect is of a relatively specific nature , given only by malignant tissue , but the evidence presented in the literature does not ; enable a decision to be made on this queetion . 
so far as the results go they are in support of the supposition that tumours contain a substance not present , or - present in much lower concentration , in normal tissue , which is capable of depressing catalase activity~ animals . 
during the period of the experiment the diet of the animals consisted of " rat cubes " ( north - eastern agricultural co - operative society , aberdeen ) and water ad libitu as a routine the mice were starved for 12 hours before catalase determination  . 
 most of the work has been carried out with the transplanted tumour sarcoma 37 ( obtained from the chester beatty research institute ) , which grows rapidly in both strains of mice after subcutaneous inoculation . 
since , however , the non - protein nitrogen amounts to less than io per cent of the protein nitrogen and appears relatively constant , total nitrogen has been employed as a standard in this investigation . 
f measurement , but to construct a standard curve of enzyme concentration in arbitrary units ( using different volumes of the same liver homogenate ) against hydrogen peroxide decomposed in 4 minutes . 
since the rate of hydrogen peroxide decomposition falls off rapidly with increasing enzyme concentration , it was found necessary to construct a curve covering a relatively wide range of concentra tions . 
of 15 per cent w / v potassium iodide and 3 drops of 5 per cent w / v ammonium molybdate were then added , and the liberated iodine titrated with n / 20 sodium thiosulphate . 
all enzyme determinations have been made in duplicate , and , for routine estimations , the quantity of enzyme taken has normally decomposed between 1 / 3 and 2 / 3 of the substrate during the course of the reaction . 
adams determinations , catalase activity in arbitrary units has been calculated by sub stituting the quantity of hydrogen peroxide decomposed in the equation to this line , and the result divided by the nitrogen content in mg . 
this was obtained by dissecting out tumours previously inoculated into ff mice , removing any necrotic areas , and homogenizing the actively growing tissue in a loose - fitting ten broeck grinder just sufficiently to give a coarse suspension . 
it may be seen that at 24 and 48 hours after injection the level is considerably depressed , that it rises approximately to normal at 4 days , and then falls progressively until 14 days , when the experiment was terminated . 
 because af this , and also since the amount of the initial ( 24and 48 - hour ) depression is not approached again until the new tumours are of a considerable size , it seems not unreasonable to suggest that the initial drop is due to some material contained in the injected tumour homogenate , that this effect is rapidly exhausted ( 4 days ) and that only the second depression ( > 4 days ) is due to the presence of the new tumour . 
although the treated groups become very small when split up , the initial ( 24and 48 - hour ) percentage depression in catalase activity appears to be considerably greater in the males . 
the experiment was repeated with schofield albinos , using s37 taken from the same strain , and larger treated groups to enable the sex difference in initial effect to be examined further . 
3 , where it will be seen that there is an early depression in enzyme level , a rise approximately to normal in 4 days , and a subsequent progressive fall . 
each point represents 6 tumour - bearing animals , and has been obtained from the arithmetic mean of the catalase level for the treated animals , and the arithmetic mean of the appropriate control group . 
this method of presenting the experimental data is by no means ideal , but the individual results would be very difficult to obtain , since no informa tion is available regarding the original oatalase level of a tumour - bearing animal . 
according to the graph , these authors obtained a rapid fall in 2 days , after which the level remained approximately constant until 4 days , and then fell once more . 
the salient point is that their results cannot be separated into " early " and " late " effects in the absence of the 4 - day rise to normal . 
their tumour must have grown extremely rapidly since they obtained a 90 per cent depression in 7 days , and greenstein and ander vont ( 1942 ) probably employed the usual technique of grafting small pieces of tumour subcutaneously rather than injecting a homogenate . 
it is fairly obvious , from the results already given ; that if the onset of tumour growth is sufficiently rapid to affect the catalase level at 4 days , the rise to normal after the initial drop will be obscured , or perhaps entirely obliterated . 
 a number of normal tissues have been coarsely homogenized ; and injected subcutaneously into male mice , which , as has been already pointed out , are more sensitive than females . 
 since the initial ( 24 and 48 hour ) depression is of primary interest , the effects on catalase level have been followed over a period of 4 days , the results appearing in table ii . 
the results in table ii show that a 24and 48 - hour depres sion was observed , although an appreciably smaller one than with s37 , and that the catalase level rose to normal at 4 days . 
 because of the much delayed onset of tumour growth , and because " takes " only occurred in a.bout half the animals it is not possible to state definitely whether the females showed a greater resistance to tumour growth , although there appeared to be a tendency in this direction . 
140 25 carcinoma 63 105 21 101 16 113 14 123 22 131 34 101 13 75 19 145 28 125 22 108 26 113 17 123 29 127 19 95 13 79 13 92 33 113 33 116 14 114 19 128 17 131 27 125 20 95 11 117 6 an experiment with coarsely homogenized necrotic s37 tissue yielded the following result : no significant depression was observed at 24 hours , but by 48 hours the level was considerably below normal , beginning to rise at 4 days . 
 since attention does not appear to have been drawn to a sex_ difference in normal mouse catalase levels , some results for males and females drawn from the same batches are given in table ill . 
 80 21 123 18 90 14 as pointed out in the introduction , the alternative mechanisms by which tumours may cause a catalase depression can be given thus : discussion . 
it is hardly possible that this early depression can be a result of any nutritive demands on the organism , and can only be due to some substance or substances present in the injected tumour tissue . 
assuming that the early and late depres sions are not entirely unconnected , it is suggested that the tumour is exerting its effect on catalase by continuously releasing this material into the circulation . 
of homogenized tumour tissue ( administered by the relatively inefficient method of subcutaneous injection ) is sufficiently active to depress the catalase level very considerably for approximately 2 days , it is probable that only a comparatively small continuous production would be required to account for the observed results . 
further , the point at which the graph flattens corresponds approximately to the tumour weight at which necrosis commences , and , for example , a tumour weighing 2 to ; 3 g . 
also , after subcutaneous injection , these tumours grow in the subcutaneous space and do not , as a rule , perforate the abdominal wall until they weigh 4 to 5 g . 
consequently little or no normal tissue can be destroyed by the growth of the tumour ; and even if this process were occurring to some small extent , the flattening of the curve at a given point would be unexplained . 
schultz and kuiken ( 1941 ) briefly mention that normal male rats have higher liver and kidney levels than females , and serfaty ( 1946 ) , working with the erythrocytes of fowls , found the level to be higher in cocks than in hens . 
 it seems reasonable to suppose that the maintenance of a normal catalase level is to some extent under hormonal control , and the different initial response of males and females to tumour tissue may indicate that the primary effect is not on the liver . 
these graphs make it clear that not only does homogenization enhance the initial depression ( as might be expected if the effect is due to some substance contained in the tumour cells ) but that such a procedure 194 d . 
their results show only a progressive fall in catalase level after the tumour implantation , and provide no evidence which could suggest that tumour tissue contains a toxic product capable of depressing liver catalsea activity . 
in some experiments the arithmetic mean of the results for the treated animals have been slightly lower than the arithmetic mean values for the controls , in others , slightly higher . 
it is impossible at present , therefore , to say whether tissues are capable of causing a slight depression , or whether normal the effect is wholly specific to tumours . 
after this process the material could be compared with similar fractions from normal tissue , and a sufficiently large dose given to show whether the cata ] ase depressing material is present at all in normal tissue . 
 it is already known ( greenstein and andervont , 1942 ) that , in general , the greatest falls in liver catalase level are produced by rapidly growing tumours , and , in fact , certain s ] ow - growing tumours produced little or no effect . 
 in the present investigation it appears that s37 tissue , which grows readily , gave a greater 24 and 48 - hour depression than carcinoma 63 , which does not . 
 following the subcutaneous injection of homogenized sarcoma 37 tissue into two strains of mice , the liver catalase activity fell significantly at 24 and 48 hours , subsequently rose to normal by the 4th day , and diminished again during the growth of the new tumours . 
there was also a sex difference in the initial response to the injection of tumour material , the males , which have the higher normal level , being more sensitive . 
the coal miners form an interesting group for comparison with the professional classes , for the miner 's daily bath , often obtained under very adverse conditions , secures cleanliness for about two - thirds qf the time , while in other respects his skin receives very rough treatment . 
the census returne ( registrar - general , 1938 ) give the age distribution , in 5and 10 - yearly periods , of the whole population of males , and also of those following each one of the recognized occupations , at the time of the census . the number of deaths attributed to cancer of the skin and lip occurring in the whole male population in each of these age groups during the years in question was obtained from the statistical reviews of the registrar - general . 
 " cancer of the thigh , " " cancer of the neck and face , " " cancer of the face and antrum . " certificates of persons under 14 years of age were excluded . 
1 shows the percentages , arranged in ascending order from left to right , for 41 occupations in which more than 5 deaths from cancer of the skin occurred in the 34 - year period ; this quite arbitrary limit in number of deaths is drawn to lessen sampling error . 
the percentage in 15 out of 16 professional occupations selected thus is below 100 , while that in 9 out of 13 agricultural occupations is above 100 , and in 5 is above 150 . 
the occupations of mining engineers , and mechanical and electrical engineers , show no deaths from cancer of the lip , and low percentages for cancer of the skin , but the numbers of deaths ( 5 and 2 respectively ) are small . the high standard of cleanliness maintained by the coal miner at the end of his day 's work , and his lack of exposure to sunlight , perhaps compensate for the various injurious factors , of which an account has been given by knowles ( 1944 ) , first - hand descriptions of the coal - miner 's life to which his skin is exposed . are given in two recent books ( shaw , 1946 ; agnew , 1947 )  . 
the mortality in the hewers and getters , who carry out much of the most severe work of the mine , is , if anything , lower ( 97 - 7 per cent ) than it is in the general population . the percentage is below 100 in 5 coal - mining occupations , comprising 828 , 246 out of the 939 , 378 men , or 88 per cent of those engaged in the 7 divisions of the industry . 
six out of 17 occupations , with a population of nearly 700 , 000 , have percentages from 131 to 249 ; this last figure ( gardeners ) is the highest of all those recorded in this paper . 
fingers , hand , forearm , and so on , might seem to give more information , but the sampling errors would be increased , and in such material the assignment to the smaller sites has not been carried out on any uniform system ; e.g. 
there would be no certainty that some cancers of the fingers had not been classed as of the hand . the numbers of cancers at these sites in the three groups of occupations , and their percentage distribution , are given in table iv and fig . 
1 provides a comparison of the percentages for cancer of the skin , and of the lip , selected and arranged in the same way , except that all cancers of the lip are included and not only those shown by occupation yielding more than 5 deaths . 
the number of fatal cases of cancer of the lip in the professional classes is so small ( 27 in 34 years in about 400 , 000 men ) that these have been pooled m . 
2. - occupational distrnbution of cancers of the skin according to site . show that no one of the seven groups of coal and shale miners gives a percentage above 100 ; the figures are low ( 38 - 3 to 56 - 0 per cent ) except in one large group which is the most exposed to light ( other workers above ground , population 106 , 549 ) , in which the incidence ( 97 - 5 per cent ) is approximately the same as in the general population . 
1 shows that the incidence of fatal cancer of the skin is high upon agricultural workers , and very low upon the professional classes , while the miners take an intermediate position not far removed from that of the general population . 
the especial liability of the out - door workers is generally supposed to be due to exposure to sunlight ( blum , 1948 )  . the results given in table iv and fig . 
2 show that the cancers of the whole region of neck , head , and face together , selected on the basis described above , make up from 70 to 78 per cent of cancers of the skin in all three occupational groups . 
the face is the only part of the body which is never clothed , and those parts which are shaved receive more thorough cleansing than do any others ; these characters are common to all social classes . 
the most notable result of this tabulation is the lack of any great difference between the three groups . another factor which may be of considerable importance is that the cosmetic effect of cancer of exposed portions of the skin and of the lip may attract attention sooner in richer subjects . ingram ( 1947 ) , in a comment on the paper by ryle and russell ( 1947 ) , says : " prognosis in skin cancer depends largely upon the size of the lesion , and negligence is probably an important factor in relation to death from this cause . i should , in the ordinary course of events , expect neglect of a symptomless lesion to be higher in unskilled workers and labourers ( iv and v of the registrar - general 's social classes ) than in the other groups . " obviously one cannot assess the quantitative importance of this difference . data in equal detail for the distribution of skin cancer in married women whose husbands follow these occupations would be of great interest . 
the great preponderance of tumours of the lower lip is explained as due to direct exposure of its mucocutaneous junction to sunlight , while the corresponding part of the upper lip is relatively shaded . " some factor in addition to exposure to sunlight is required smoking , and especially pipe to explain the differences shown in table vii . smoking , is , of course , regarded as another possible factor in the production of cancer of the lip . during the earlier part of the period ( 1911 to 1944 ) cigarette smoking was practically restricted to the richer classes , which produce fewest cancers of the lip ; data on the change in this matter in recent years have been given elsewhere ( kennaway and kennaway , 1947 )  . 
the data collected by lane - claypon ( 1930 ) from the literature , summarized in table vii , show the great preponderance of cancers of the lower lip , especially in males . 
 ( lanecilaypon , 1930 )  . all occupied and retired males agricultural labourers farmers deaths . death rate per million per annul . 212 798 55 - 0 comparison of cancer of the skin and of the lip . the data given in fig . 
of the 14 agricultural occupations which produce any cancers of the lip , 11 show agreement in regard to cancer of the skin and of the lip in that both percentages are either below , or above , 100 . this suggests that the aetiological factors are to some extent the same in some occupations . 
the incidence upon the coal miner is of especial interest in view of the cleanliness secured by his daily bath , and of his minimal exposure to sunlight . in occupations in which 88 per cent of the coal - mining population are engaged the liability to cancer of the skin is less than it is in the general population . only one occupation of social class i ( civil engineers and surveyors ) shows a mortality from cancer of the skin higher than that in the whole population ; hence these results illustrate the social distribution of cancer of exposed sites discovered by stevenson . 
the comparative distribution of cancer upon the various parts of the skin does not show any great differences in the three groups ; from 70 to 80 per cent of these cancers are situated on the head and neck . 
the mice used for transplantation undoubtedly came from therefore , additional experiments were different sublines of these two strains . carried , out in an attempt to elucidate the forowing questions : 1 . 
does the regression of a well - developed transplanted tumour forowing irradiation in vivo render the animal resistant to the development of spontaneous tumours ? this study was made possible by the use of the irradiation technique ( goldfeder , 1950a ) which facihtates the exposure of the tumour and protects the rest of the body of the animal from secondary scattered radiation , thus permitting the treated animals to eve their life span . previous work on the irradiation of tumours has been summarized by the writer ( 1945a )  . there is no doubt that results obtained with tumours heterogenous to the animal bosts - that is , tumours which have a different genetic constitution from that of the host , are not comparable with those obtained with tumours autogenous to the animal hosts - that is with tumours having the same genetic constitution as that of the host , or with , those in patients suffering from cancer . 
memorial laboratory on julv 5 , 1933 , and they were designated at that these mice have been inbred since : they behave time as inbred strain ' d '  . immunologicary like dba / 212 , and have an incidence of over 85 pe ' r cent of spontaneous mammary tumours among breeding females . 
a tumour of about 5 min diameter usuauy develops from an implant within a period of 12 to 14 days , and grows progressively . a spontaneous mammary tumour of an i 1 - month - old female mouse of the dba this tumour was : firmer in consistency than that strain was excised asepticary . fragments of about 2 mdissected removed from the c3h mouse described . from the edges of the tumour were implanted subcutaneously into 10 dba mice ( 8 males and 2 females )  . 
1 round coverslip 7 inch in diameter , wbich had been previously attached by a drop of sterile water to a mica sheet and covered with a maximow depression slide , in the concavity of wl - lich moist filter paper had been placed to maintain the water content of the tissue . 
the absorption of radiation by the cover glass , mica sheet and maximow slide was about io per cent , which was taken into consideration in calculating the x - ray dose delivered to the tumour tissue . immediately after irradiation the tumour fragments were implanted into about 2 - 3 - month - old mice , most in two additional experiments the mice were injected of which were litter mates . intradermally with aliquots of irradiated . 
tumour cells , suspended in physiological this was done because , according to observations made by several investisaline . gators , the intradermal route of immunization appears to produce more effective and lasting results ( besredka , magat , laval and besnard , 1936 ; kolmar and tuft , for the latter experiments the tumour fragments following irradiation 1941 )  . were cut with sharp curved scissors until an almost homogeneous mass was obtained . 
doses by mea ' ns of a tuberculiin syringe and .25 gauge needle in two or three sites of the abdominal wall of each mouse . the latent period and the number of " takes " produced by tumciur grafts irradiated in vitro served as criteria of the effect of a given dose of x - radiation . the procedure of irradiation of the estabhshed tumours in v& ' vo was as follows actively growing tumours ranging in size from 1 - 0 to 1 - 5 cin diameter were exposed to filtered x - radiation while the rest of the animal orgamsm was shielded bv a lead chamber ( goldfeder , 1950a )  . during the early experiments the tumours were irradiated in vivo under the same physical conditions as the tumour grafts during the later experiments , the following physical factors were in vitro . employed : the radiation was generated by a westinghouse " quadrocondex " constant potential unit at 200 kv , 15 ma ; the incident beam was filtered by 05 mcu plus i 0 mal ; hvl equalled i 0 mcu ; fsd , 20 . 
the dose rate measured in air bv a thimble ionization chamber during the coiirse of the investigations varied from 395 r / mto 402 r / min . special measurements were made with and without the lead ( 5 per cent )  . shield , the ionizatioil chamber being placed in the same position . 
observations on c3hb transplantable mammary tumour . the results obtained on implantation of the irradiated c3hb tumour - grafts a - re recorded in table i are presented graphically in fig . 
the first ' retardation of tumour growth , as indicated by a slight increase in the latent period of tumour appearance , was prodiiced by a dose of 2000 r . 
ii , an implant irradiated with 5000 r developed a tumour after a latent period of 117 days . in this , as wer as in other similar instances , the question arises whether the tumour cells had been attenuated by x - radiation to such an extent that they remained dormant for this comparatively long ' time , or whether only a few cers had escaped injury and took , therefore , a much longer time to develop a palpable tumour . this question cannot be answered with any certainty . it is certain , however , that the tumour grew on the site of grafting and that the rate of growth and the histologic ' al pattem were similar to those of a tumour developed by a non - irradiated implant . in no instance did a tumour , developed by an irradiated implant , regress spontaneously , contrary to observations frequently made when the tumoiir implant and the host are not of the same genetic origin . search for induced re8i8tance the mice in which the irradiated tumour grafts failed to produce tumours ( experiments 7 - 14 , table i ) were reimplanted with fresh , viable tumour grafts . due to the long latent period , the second implantation into mice of this series was performed 3 to 4 months after the implantation of the irradiated tumour grafts . 
a dose of 12 , 000 r completely destroyed all the treated tumours . sections of the tumours removed within 10 to 12 days after irradiation showed only necrotic tissue . it appears , therefore , that a dose within the range of i 1 , 000 r to 12 , 000 r is lethal for the c3hb tumour of 1 - 0 to 1 - 5 cni . 
the irradiated tumours which resumed their growth after initial decrease in size , grew steadily and in no instance did a tumour regress once it began to grow again . occasionary secondary tumours developed in the treated mice either in the inguinal or axillary reg - ions within 2 or 3 weeks after the regression of the irradiated in some instances , new growth developed on the periphery of the tuniours . irradiated tumour , probably from tumour cells which bad not been included in the exposed area . 
the histological appearance of these secondary tumours resembled that of the primary , non - irradiated c3hb tumour . epilation and regrowth of gray hair appeared in the exposed areas 3 to 6 weeks after regression of the irradiated tumours . 
no ulceration of the skin in the irradiated area was ever noted in the c3h mice once gray hair appeared . a significant number of c3h mice hved about i year after regression of the tumours and spontaneous tumours appeared in some of the c3h females . 
observation8on dbah transplantable mammary titmour . this tumour had been carried for 8 generations of serial transplants in the dba mice from which it originated before it was used for irradiation . although loo per cent " takes " resulted in most instances , occasionany , however , an iniplant failed to produce a tumour in a dba mouse which later proved to be resistant to further viable tumour grafts . according to hauschka , this may be the result of a mutant histocompatibility factor present in the dba strain ; in other words , an outcome of genetic incompatibihty between the bost and the transplanted tumour . 
to secure a better statistical evaluation of the results , a number of mice were grafted with viable , non - irradiated dbah tumour fragments to serve as controls to those grafted with irradiated dbah tumour implants . 
the delay in the latent period is probably a more rehable criterion than the tumour " take " for re - evaluation of the radiation effects in this case , because it could be argued that the 2 mice in which the irradiated tumourcells failed to produce tumours possessed the mutant - histocompatibility factor . in one experinient , a dose of 4500 r resulted in 22 - 9 per cent of " takes " , while a dose of 4800 r resulted in 13 - 0 per cent of " takes " and a dose of 5000 r gave only 5 - 1 per cent of " takes however , in two additional experiments , after doses of 5000 r and 5200 r no " takes ocetirred . 
none of these 7 produced tumours fohowing implantations of viable tumour grafts . in the experimental - mice , the number which failed to develop tumours was 150 out of a total of 341 mice which had been implanted with irradiated tumour grafts . 
none of these eighteen dayis later these - mice were reimplanted 25 niiee developed tumours . subcutaneously with fiesh , viable tumour grafts . palpable tumours , whicb , grew progressively , appeared within 9 to 13 days in 14 out of the 15 reimplanted male and in 9 out of 10 re - implanted female mice . two mice , one male and one female , in which the irradiated tumour cells failed to produce tumours in the first place , remained refractory to twice repeated implantations of viable tumour grafts . this result may also be ascribed to the mutant histocompatibihty factor present in these 2 mice . re8u1t8qf x - radiation o dbah tumour8in vivo . table v records the observations made on a total of 227 mice ( 164 males and 63 females )  . 
a rather sudden increase in the number of tumours which showed regression was noted forowing the application of doses higher than 6000 r . thus , 60 per cent of the tumours regressed after a dose of 7000 r . 
while a dose of 6000 r destroyed only 25 per cent of the treated tumours . the larger percentage of the regressed tumours which had been treated with a dose of 10 , 000 r indicates that this is the destructive dose for the dbah transplantable tiimours , ranging in size.from 1 - 0 to 1 - 5 cin cliameter . 
as in the case of the c3hb tumour , this dose is twice as large as the dose necessary for the attenuation of grafts of this tumour in vitro . the majority of the mice . ' m which tumours had regressed eved in apparent good health for i year or longer , and the young female ' mice produced apparently normal litters . 
the ulceration - s persisted iintil the death of the - ani ' mals . these two instances may parallel radiation necrosis occasionally noted in human patients treated with x - rays . 
the turnours in the remaining 7 mice grew steadily . fourteen tumours decreased considerably in size within 10 days after irradiation increased tumours grew steadily after exposure . five tumours regressed within 3 to 4 weeks following exposure . 
two females developed spontaneous months after regression of the treated tumours . in 27 mice ( 20 males and 7 females ) the tumours regressed completely within 3 weeks after irradiation . 
microscopic sections of the regressing tumours consisted mainly of fibrous tissue . the tumours regressed completely in 30 treated mice ( 21 males and 9 females )  . five fexnales developed spontaneous tumours 6 - 7 months after regression of the treated tumours . the treated m1ce lived for as long as i year and more after treatment . 
the mice lived in apparent good health up to 1 year and more . of ar treated mice only in two - instances did ulceration of the skin in the irradiated area occur 11 months after regression of the tumour . should be noted that in the experiments cited above , geneticary impure ammals and tumours geneticary different from the hosts were used . 
the writer 's interest in the problem of induced resistance arose from investigations on mouse sarcoma 180 grown in white mice of the swiss strain ( golffeder , 1942 )  . 
the writer explored the possibihty of inducing a resistant state in inbred animals by implanting into these animals irradiated grafts of a tumour which originary developpd in an animal of the same inbred line . these expenments were carried out hi an attempt to ascertain whether ionizing radiation induces genetic and antigeriie changes in the tiimour cells which make them foreign to the host . 
the irradiation of tumour cells in the present experiments did not make them foreign or antigenic to the host in which they originahy developed . an analysis of the results recorded in table i and in table iii reveals a difference in the radiosensitivity between the c3hb and dbah tumours . for example , a dose of 3500 r gave 92 per cent " takes " of the c3hb tumour grafts and only 57 1 . 
determined for implants of other mammary adenocarcinomas in inbred strains of mice ( lawrence , horn , strong , 1937 ; goldfeder , 1945a ) and for a mammary adenocarcinoma of an inbred line of rats ( eisen , 1940 )  . 
on the other hand , the c3hb mammary adenocarcinoma used in t - he present studies proved to be more resistant to irradiation than the cm mammary adenocarcinoma used in previous experiments ( goldfeder , 1947 ) , the latter requiring only 2700 r to prevent its grafts from " takes "  . 
the difference in the radiosensitivity between the c3hb and c3h mammary adenocarcinomas may be explained by ( a ) a difference in degree of differentiation : the c3hb mammary adenocarcinoma in the present experiments is a more anaplastic type of tumour consisting of fiheets and bands of closely packed cells , with relatively little fibrous connective tissue , while the cm mammary adenocarcinoma previously reported ( goldfeder 1947 ) consisted of acini , uniformly distributed and separated by connective tissue ; ( b ) by a difference in genetic make - up between the tumours and their hosts : the c3hb niammary tumour was carried by serial transplants in pure inbred cm mice from which it originated , while the mammary tumour , used in previous studies ( 1947.1950 ) , was carried in c3h mice of different sublines and thus the tumoiir and the hosts were not of the same genetic origin . failure of the tumour to " tak - e " in about 10 per cent of the hosts indicated that some of the cm mice used in the experiments of 1947 - 1950 had a different genetic constitution than that of the .mouse in which the tumour developed . 
the skewed curve illustrated in that publication ( goldfeder , 1947 ) in contrast to the typical s - shaped curve obtained in the present experiment may also be the result of the difference in the genetic make - up between the hosts and the tumour . 
the radiosensitivity of tumours depends to a large extent on whether they are growing in hosts of the same strain from which they originated , or in foreign hosts as shown by aughterson , tennant , irradiation of a transplantable mammary carcinoma in and lawrence ( 1940 )  . strain a mice in which the tumour originated induced regression only in i per cent of the treated mice when 2500 r were apphed and in 48 per cent of mice forowing the application of 5000 r . 
the antigenic reaction of ' the foreign host is thus a contributing f ' actor in rendering the tumour more vulnerable to ' regression after irradiation . the more anaplastic c3hb tumour proved to be more resistant to radiatioii than the relatively more differentiated dbah tumour . this corroborates the observations made by the writer on another mouse mammary adenocarcinonia ( goldfeder , 1950a ) and those noted on human tumours . for example , cathie ( 1939 ) , lenz ( 1942 ) and gliicksmann ( 1948 ) found that well differentiated cancers regressed more readily and offered a better prognosis than the less differentiated tumours . the r ' ole of connective tissue in the response of animal tumours to irradiation and its relationship to the host was brought forth by cramer ( 1932 ) aind by aughterson , tennant and lawrence ( 1940 )  . 
the relatively more pronounced proliferation of the connective tissue in the dbah tiiniour thanin the c3hb tumour may also be regarded as a contributing factor rendering the dbah tumour more vulnerable to irradiation . 
the observation of secondary tumours occurring in the treated mice also seems to parallel observations made on human mammary this observatioin indicates the failure of the disintegrated irradiated cancers . tumour tissue to induce resistance in the hosts to new cancerous growths . it has been noted that untreated metastatic tumours often regress after x - ravv treatment of primary tumours ( sugiura , 1937 ; aughterson , tennant and lawthis observation has been attribiited to a supposed indirect effect rence , 1940 )  . of irradiation ( sugiura , 1937 )  . these observations could probably be explained by the fact that the tumours were grown in genetically foreign mice . 
the present experiments on mice of geneticafly pure strains and their autogenous tumours indicate that the indirect effect of irradiation is not sufficient to affect secondary growths . regression of the secondary tumours in x - ray treated heterozygous mice may be attributed to an antigenic effect ' ehcited by the genetically differing tumour tissue . 
the inability of the irradiated tumour tissue to induce " immunity " in hosts from which it originated may indicate that no quahtative change of a genetic or antigenic character occurred in the irradiated tumour cells which would render them foreign to the hosts . inbred hnes of mice and their tumours offer far more suitable material for investigations of this type than heterozygous mice . 
the observations made from such studies seem to pararel those noted on human mammary cancers . in earlier publications ( goldfeder 1950b , 1952 ) , the writer showed that a fast growing , less differentiated mouse mammary adenocarcinoma also possessed a more vigorous metabolic rate and suggested that this propertv may have been one of the factors influencing the radiosensitivity of the mammary adenocarcinomas then used . 
a smaller irradiation dose was found to prevent the irradiated dbah tumour grafts from growing in vivo than was required to produce a similar effect on c3hb tumour similarly , for treatment of established tumours in vivo , the dose of irragrafts . diation which produced regression of the dbah tumour was found to be smaller than that which had a similar effect on the c3hb tumour . 
some factors which are involved in the difference in the radiosensitivity of these two tumours are the state of differentiation of the tumour cells and the amount of stroma . in both instances about half of the radiation dose , producing destruction of the established tumours grown in their respective hosts , was required to obtain the attenuation of the grafts of both c3hb and dbah tumours . the c3h mice in which the irradiated in vitro c3hb tumour grafts failed to " take " or in which a well developed transplanted c3hb tumour regressed after irradiation in vivo remained susceptible to reimplanted viable c3hb tumour grafts . 
a small number of the dba mice in which the viable dbah tumour grafts failed to " take " in vivo remained resistant to viable tumour grafts . similarly , a small number of the dba mice in which the irradiated in vitro tumour grafts failed to " take " was found resistant to re - implantation of fresh viable tumour implants . this is explained by a difference between the genetic make - up of some of the dba mice and the dbah tumour . a significant number of mice of both strains lived in apparent good health for 1 year and longer after regression of the in vivo irradiated tumours ; among these survivors the young females produced apparently normal litters . spontaneous tumours also occurred among these female survivors on reaching cancer age . thus , under the experimental conditions described , the question about the possibility of inducing immunity in homozygous hosts to endogenous tumours by irradiation of these tumours appears to have been answered in the negative.. the part played by the genetic relationship between the tumour and host in the induction of resistance to the appearance of tumours was brought forth . 
burn re8earch laboratory , royal victoria infirmary , newcastle - upon - tyne . received for publication january 30 , 1954 . this is the first of a series of reports on an experiment suggested by the work strong hybridised three strains of mice , and after 3 of , strong ( 1940 , 1945 )  . inbred generations he injected subcutaneously i mg . 
to f12 injections were continued but there was selection towards resistance to tumours at the site of injection ; five sublines were then spht off and the mice injected for a further 4 generations , after which one group was set aside and bred from without further treatment . the experiment to be reported here differs in several respects from that of strong ( 1940 , 1945 )  . 
towards the ' end of 1945 two inbred strains of mice , the nbt ( newcastle bone tumour ) and the cba ( one of the ancestral strains used by strong ) were crossed in both directions . half the mice in each f , htter were injected subcutaneously in the right flank at the age of 2 months with i mg . methylcholanthrene in 0 - 1 c.c. 
sesame oil ( one inject ' lon only ) ; the other half were not treated and were bred from ( brother - sister matings only ) for 12 generations , ar untreated . 
the untreated reciprocal - hybrid strains were known as the cba / nbt and nbt / cba strains , or cn and nc for short , the maternal strain being given first . the injected f , mice were also bred from , their inbred descendants likewise being injected and subsequently bred from for a total of 10 generations . 
from the beginning an attempt was made to breed selectively for resistance to local tumours , but entirely without success ; offspring of apparently resistant inice appeared to be just as susceptible as those of susceptible mice . 
onwards etters from mice which early developed local tumours were neither injected nor bred from . finauy , as the failure to produce resistant lines seemed likely to spoil the purpose of the experiment , 2 final generations ( f , , and f.2 ) were raised , in which no mice were injected . the injected reciprocal hybrids together with their untreated descendants formed the m / cba / nbt and m / nbt , / cba strains , or mcn and amc for short . mice were fed on " rat cake " compounded to the formula of the rowett institute by an aberdeen firm , supplemented with cabbage and carrot , with drinking water ad lib . the purpose of the experiment was , like strong 's ( i 940 , 1945 ) , the development of lines of mice resistant to tumours at the place of injection , so that the mice would live long enough to produce tunio ' urs at ' remote sites . 
the origin of the strain has been described ( pybus and mffler , 1938 ) and the various types of bone tumours have been described and illustrated ( pybus and mfller , 1940a , 1940b )  . afice of inbred generations 28 and 29 , coming from i pair of mice of generation 22 , were used as parents of the hybrid stra ' ms ; 131 mice ( 59 females and 72 males ) of generations 28 to 30 were treated with methylcholanthrene . 
one generation of 81 females and 94 males , an untreated , was raised from the treated mice ; 28 p , , .irs , belonging to 9 famihes , were successfuey bred from , a further 17 pairs proving sterfle . the last bone sarcomata to be seen in this strain were 4 which occurred in f27 prior to these there were 3 in f22and i in f24 . 
the purpose of the experiment was not to investigate the occurrence of local t ' umours , but ( as already stated ) to try to develop strains of mice that would be resistant to the local action of the carcinogen and would therefore live long enough to produce neoplasms at places remote from the site of injection . 
ar mice were therefore allowed to live as long as possible , and those with local tumours were killed only when the tumour grew large or showed signs of ulceration . there was a certain amount of variation in size of tumours at death , those close to the skin or in a position to rub against the box having a tendency to ulcerate 166 e . 
at first the mice were charted regularly , outhne drawings of tumours being made when they appeared and their growth followed week by week , but as the numbers of injected animals increased this became impossible and tumour sizes at death only were charted . it was observed from the initial weekly chartings that there was great variation in the , rate of growth of different tumours , but it cannot be stated whether this variation depended to any extent on the sex of the h ' ost ; it did not appear to do so . 
the males might be more susceptible than the females to the local action of the carcinogen ; i.e. , tumours might appear after a shorter latent period in males , and , even if tumour growth - rate was the same in both sexes , the males would be killed at an earlier age . 
with a very few exceptions in certain generations , many non - tumour males died prematurely and usuahy earlier than non - tumour females ( i.e. , mean age at death was less for males in ar cases except m / cba , mcn fl , and mnc f9 and flo ) , due mainly to wounds received in fighting . in some generations some of the non - tumour males which died prematurely might have developed tumours had they lived longer . this would have raised the tumour incidence and would proba - bly also have raised the mean tumour age at death in these instances . although causes i and 2 cannot be completely dismissed , there is evidence for the fourth possibihty in a comparison between the two pure strains . 
the local response o methylcholanthrene . two inbred strains to one subcutaneous injection of nbt strain . - as shown in table 1 , 59 females and 72 males were treated at local tumours appeared in 27 females ( 45 - 8 per cent ) and the age of 2 months . in 25 males ( 34 - 7 per cent )  . 
the non - tumour males in this strain died young from various causes , the principal bein - a filrhting ( 17 mice ) , while diarrhoea diarrhoea was responsible for the death of a number ( 7 ) of accounted for 8 . other causes of death in both sexes were kidney diseases , young females . pneumonia and pseudo - tubercle , and there were a few cases of neoplasms ( leukaemia , lung adenoma , mammary carcinoma and skin papillomata )  . there was no significant difference between the ages at death of tumour and non - tumour males ; from this it may be concluded that more of the males might have developed tumours had they lived longer . 
f6was a small generation of only 25 mi ' ce and 8 of th ' e io non - tumour males were dead by 6 months ; this could account partly for the lo ' w incidence . 
but f2was a very large generation with 134 females and 120 males , there being 96 tumour females ( 71 - 6 per cent ) and 94 tumour males ( 78 - 3 per cent ) , the combined incidence being 74 - 8 per cent . 
why this generation should be so susceptible is not clear at the moment . age at death : the result of inbreeding on the survival age of injected mice was evident in this experiment . in generations i to 5 , 74 mice died at 21 months and over , the oldest at 28 months ; in generations 6 to 10 only 3 mice ( non - tumour ) except for fl , to be discussed later , the ages at lived over the age of 17 months . death in each generation were not analysed separately . 
 - minbticba8train ( table iii )  . - each generation was analysed to find out whether the sexes were equally susceptible to the development oflocal tumours . with the exception of the first and third generations , the differences in each generation between the tumour incidences i ' n males and females were not significant . in fl , more than half the non - tumour males died at ages up to 7 months ( mainly due to fighting ) and the tumour incidence in the males was probably too low ; f , , was a smar generation and the early death of a number of non - tumour males had a disproportionate influence on the result . 
was a smah generation of 36 males 66 - 4 per cent ( 511 tumours in 770 males )  . and many of the non - tumour males died young , while in f4 half the non - tumour males were dead by 8 months . 
the incidences for these two generations of males were very probably too low , as some of the non - tumour mice would certainly have developed tumours had they eved longer . although it is therefore probable that the sex - difference in incidence was due to a lack of fur opportunity for the development of tumours in the males owing to a disproportionate number of the latter dying young , this cannot be presumed to be certain . a comparison of the reciprocal crosses regarding their susceptibility to local tumours was thus a comparison between an incidence of 62 - 8 per cent in the 538 mcn females and 73 - 4 per cent in the 669 mnc females ; and between 59 - 6 per cent in the 542 mcn males and 66 - 4 per cent in the 770 mnc males . 
the tumours seen were of the various types described by bonser and orr ( 1939 ) ; the greatest number were subcutaneous fibrosarcomata , of varying degrees of fibrosis ; there were a few pure fibromata , and many spindle and polymorphous - celled sarcomata . giant cells were frequently present . 
the possibility then had to be considered whether the hereditary condition acted through genetically transmitted differences in ovarian functional activity , or through an unequal response of mammary glands or genital tract to ovarian hormone . 
numerous and extensive observations were made with somewhat conflicting results , both on the nature of the oestrous cycle and on variations in organ sensitivity to hormonal stimulation , in strains of mice with differing mammary cancer incidence . when the existence of the third factor , i.e. 
as the number of determinations was so small , no statistical analysis of the figures was made , but there appears to be no real difference between the strains themselves , nor could the changes produced by foster - nursing be correlated with the presence or absence of the milk factor . 
armstrong ( b ) the character of the oestrous cycle . ( i ) virgin mice . - daily vaginal smearing of virgin mice of all groups was continued for periods ranging from 56 - 137 days immediately following canalization or weaning . 
the number of complete cycles during the observation period in addition , the average length of the whole cycle and of the was recorded . comparison actual period of heat for each mouse was calculated ( table ii )  . was then made between the fostered and non - fostered groups ( table iii )  . all cases comparisons show no significant difference . 
the p factor being of the order of o 1 - 0 5 . a second series of estimations was then made , in which two types of atypical cycle were excluded , in view , of the fact that such cycles might have been caused in the one type , a prolonged dioestrous by the repeated smearing technique . interval is observed , a state termed pseudo - pregnaney . this occurs naturally following sterile copulation and artificially following a great variety of stimuli . parkes ( 1926 ) regarded 7 days as the shortest duration of natural pseudo - pregtherefore all cycles with dioestrus greater than 7 days have been nancy . in the other type there is prolonged cornification or regarded as atypical . heat , a condition which has been produced experimentally by repeated vaginal smearing . 
the death of so many mice while still showing oestrous cycles detracts from the value of the results , but there was some indication that the range of age at which the menoe . 
from table i it is seen that vaginal canalization occurred later in group 3 ( free from milk factor ) than in group 1 ( having natural milk factor ) , but that the effect of foster - nursing was to increase the age in both cases , so that this cannot be correlated with the administration or withholding of milk factor . 
no undue importance has been attached to this as it occurs in the riii groups , in which foster - nursing is an unsatisfactory procedure , due to the possibility of the offspring receiving milk factor from their mothers during the interval between birth and transference to foster - parent ; also the difference is not statisticllay significant when all cycles are included and the samples are small . on comparing the two strains ( table iii ) there is some indication that the nature of the cycle shows a strain difference , which is unaffected by foster - nursing . comparing these results with the features of the oestrous cycle as described by other workers , there are , in general , appreciable strain differences in this respect ( table vi )  . it may be noted that the average duration of the cycle in young cba mice as observed by bonser ( 1935 ) is closely comparable with that obtained in the present experiment - 5 - 8 and 5 - 3 days respectively . foster - nursing as a means of administering the milk factor appears to be an entirely satisfactory procedure . thus the fact that no significant change in the character of the oestrous cycle was induced by this means , would seem to indicate that the factor does not influence the cycle . it is possible , however , that some adjustment to the new conditions created by the foster - mother 's milk is made during the period of suckling . the milk factor effect might be counteracted by the time puberty is reached and the hereditary condition alone revealed in the characteristics of the sexual cycle . the distribution and extent of two forms of atypical cycle were stuidied , as it was thought that , if they were caused by smearing technique , their incidence might vary in the different groups of mice . should , however , such cycles occur spontaneously , any observed strain difference in the duration of the cycle or e . 
bonser for her guidance and interest in the planning of this work and for her co - operation in the experimental procedure , which made consecutive daily observations over such a long period possible . i also wish to thank j . 
thus , administration of the milk factor from two different highbreast - cancer strains to the same susceptible hybrid mice , kept under controlled conditions , has shown differences in either quantity and / or quality of the factor present in these two high - breast - cancer strains . l , dmocrowski bittner and huseby ( 1946 ) reported similar findings by a different experimental procedure ,  . 
namely , by reciprocal crossings of two high - breast - cancer strains ( c3h and strong a ) , and by recording the tumour incidence and tumour age in virgin hybrids obtained from these strains . 
they described the recorded d ' ifferences in the tumour incidence and in the tumour age in these hybrids as a result of different concentration and / or activity of the milk factor present in these heston and andervont ( 1944 ) in a similarly two high - breast - cancer strains . conducted experiment on sublines of the same strains found no conclusive andervont and eviden ' ce of a difference in the milk factor of these strains . mceleney ( 1941 ) pointed out , however , that his high - breast - cancer strain - ( c3h ) must be regarded as a separate line , and the results obtained with it cannot be controlled by data procured from other lines of this strawamer , reinhard and goltz ( 1945 ) in experiments on virgin hybrids of two other high - breastcancer strains ( m and a ) obtained similar results ' and concluded that the milk factor was more concentrated in one of these stra ' ms than in the other . bittner and huseby ( 1946 ) found , however , the same incidence of breast cancer in breeding hybrids of the two strains tested . 
but they rightly pointed out that the ultimate result of the changes in the structure of breast tissue acted upon by the milk factor of another strain is determined also by the genetic constitution and responsiveness of the breast tissue to the particular milk factor . heston , deringer and andervont ( 1945 ) , b ' y employing susceptible hybrid mice obtained from high - breast - cancer strain mothers and low - breast - cancer strain fathers , and by backcrossing them to highand low - breast - cancer strain males , showed that differences in the milk factor were produced by differences in the genetic constitution of the mice from which the milk factor originated . 
3. as possible into three groups . mice of the first group , when 4r - 5 months old , received one subcutaneous injection of a distilled water suspension of dried riii breast tumour tissue corresponding to 0125 g . 
of fresh breast tumour tissue ; mice of the second group , when of the same age , received one subcutaneous injection ' of a distilled water suspension of dried 63 ca transplantable breast tumour tissue ( from a 428th transplant of the tumour obtained from the imperial cancer research fund ) corresponding to 0125 g . 
no tumours developed in any of the s low - breast - cancer strain females , whether injected with riii or 63 ca dried breast tumour tissue . in the fl generation of s strain females injected with 63 ca tissue and of the control females , no tumours were observed in any of the females , or in any of the males painted with oestrone . in the fl generation of s strain females injected with riii dried tumour tissue , 7 out of 16 females developed breast cancer , and 5 out of 15 males , which were painted , also developed breast tumours . in s x riii hybrid females obtained from daughters of s strain females injected with dried riii breast tumour tissue , 27 out of 32 females showed breast tumours , while s x riii hybrid males of the same origin , painted with oestrone , gave tumours in 10 out of 16 mice . 
observed by the method ' employed in the present experiment . it is impossible to state , however , whether the milk factor was originally absent in the primary tumour or whether it was lost during the course of so many transplantations . .in conclusion , it can be stated that only an analysis of the action and interaction of all know - n factors with allowance for other possible factors can make 102 l . 
the diet was supplemented with cod liver oil , and greens once weekly , and 2 - 3 g . bread ( 80 - 85 per cent extraction ) daily . thirty - four female and 12 male control rats received the same diet without pda or a mixed diet of rat cubes , bread , and once weekly greens . 
the value for total proteins obtained in the present experiments , in which only mature animals were employed , are higher than those found by lippman for mature animals , but lower than the values of metcoff and favour . 
the deviations of the values obtained by the specific gravity method were within + 6 - 5 and 3 - 5 per cent in 10 cases . the sera were fractionated by electrophoresis in the tiselius apparatus with the cylindrical lens schlieren optical system ( thovert , 1914 ; philpot , 1938 ; the buffer solution svensson , 1939 )  . 
the final patterns and the base lines were traced under magnification , superposed in such a way that those parts which did not show any elevation of the base line coincided . both the ascending and descending patterns were analysed . 
the aand the r - globulins appear frequently as broad regions ( moore , 1945 ) , which by overlapping with the 5 - globulin peak , made the separation of the globulins into individual groups uncertathe uncertainty in the values given for the x - , por - - globulins was + 15 per cent or less . wherever the uncertainty was greater , the combined areas of pand y - globulin were measured . 
of ascites was found together with high serum protein . the sera from 6 treated and 10 control animals were analysed by electrophoresis , and the results are given in table ii and fig . 
no difference in the patterns was found between the normal albino and blackhooded rats , on the semisynthetic diet , or on the mixed laboratory diet . all these patterns showed a double albumin peak , the components of which were separated to varying extent . ~~~~~~~~~~~~~~~i ~~01o0 ~~~~~~~~~~~~~~~~~~~~~i c0 - 3 5 - 0 - o ' - o ! a very ~asmiil fig . 
1. 20 b 30 50 gtc 5o.tu.g in the descending pattern the peak of the slower albumin component was in some cases higher than the corresponding peak in the ascending pattern , and in some cases this region in the descending side indicated gravitational instability , reminisin contrast cent of the , - anomaly , which is often seen with normal human sera . the patterns of sera from rats which developed hepatic tumours due to the ingesin no . 
the gravitational disturbance on the descending side was seen in cases 15 and 16 , and to a smaller extent in cases 13 and 14 . the concentration of the total globnlins was significantly increased in the group fed pda , while the concentration of the albumin remained unchanged . the increase occurred mainly in the [ and y - globulins with the exception of case 12 . 
3. - - e : lectrophoretic patterns of rat sera~ 1 - 10 , cotrol rats , 11 - 16 , rate fed pda._ left : = a~ - ~ling , rit = descenamig patterns . cending , right = descendig patterns . threpeaks in the ascending limb , remaining single in the descending limb - and convectional disturbances were observed near the m - globulin region of the ascending limb , but not in the descending or any other part of the ascending limb . ( similar disturbances near the 4 - globulin region have been observed with some human sera in more concentrated solution in the same buffer . ) these disturbances were not due to heat effects caused by the electric current , but probably to the formation of a gravitationally unstable region . 
the figures in brackets are percentages of the total protein . the remarkable sudden increase in the serum proteins at the time of the development of a tumour and the fact that the increase is independent of the size of the tumour seem to exclude the possibility that the increased serum protein has its source in the disintegration of tumour tissue : this sudden increase in the serum proteins has an analogy with the reaction of the body to foreign protein , where the amount of antibody produced is largely independent of the amount of antigen present . 
the results would suggest that , at least in hepatic tumours , the first pathological change in the serum proteins is an increase in the globulins , and a decrease is only the expression of the general deterioration of the diseased individual . the general impression that the serum protein of patients suffering from malignant diseases is decreased may be erroneously gained from reports ( a ) giving 146 c . 
the increase of the yand p - globulins of these rats might be due to an increase in immune bodies frequently associated with these fractions ( tiselius this explanation would be in accordance with the concept and kabat , 1939 )  . that the increase of the total serum protein in rats developing hepatic tumours is an immunological phenomenon . 
black. from the postgraduate medical school of london . received for publication march 25 , 1952 . from perusal of the literature available it appears that chronic ulceration associated with varicose veins is the most rare cause of malignant disease of the skin of the lower limb . 
we therefore wish to present 6 cases which undoubtedly occurred in conjunction with a varicose ulcer or eczema which had been present for many years . cutaneous neoplasia of the leg is rare , and study of the literature demonstrates that such skin cancers as do occur very rarely arise de novo , but usually in connection with chronic inflammation following injury , in old scars and sinuses , or after some chronic skin infections such as lupus vulgaris as well as in the varicose conditions mentioned . since the latter are without question the most commonly found benign lesions of the leg the excessive rarity of malignant degeneration is surprising and interesting . in recent years papers on this subject have been few . 
on examination she was a wasted , frail old woman not well orientated . there were no large nodes in the groin , the general examination showed senile but several small soft nodes could be palpated . changes but no obvious disease . biopsy of the tumour revealed a well - differentiated squamous carcinoma with cell - nests . 
b - , aged 71 years , was referred to us for treatment of a very large varicose ulcer of 20 years ' duration . four months before his admission to hospital the lower edge had begun to hypertrophy and the ulcer to spread on to the dorsum of the foot . 
h - , a widow of 67 years , was referred to us for treatment to secondary neoplastic nodes in the right inguinal region . she had been treated by mid - thigh amputation , at another hospital , for a 30 - year - old decubitus ulcer which , at the time of amputation , extended from the dorsum of the right foot to one - third of the distance up the tibial shaft and involved the bone . there had been no recent change in the ulcer prior to amputation but it had steadily increased in size during about 7 years before admission to hospital . amputation had been advised for pain , and because of the large size and failure to heal with support and dressings . on examination her right leg had been removed through the thigh . 
hard mobile nodes were present in both groins and in the right axilla . the left leg showed marked varicose veins and the scar of a healed ulcer above the left internal malleolus . her heart was fibrillating ( she had been receiving treatment for this for about 6 years ) , but there were no signs of cardiac failure . a report on sections taken from the ulcer after amputation showed a well - differentiated keratinising squamous - celled carcinoma . a biopsy excision of nodes palpable in the axilla was performed . 
no other radiological evidence of malignancy was found . biopsy of the tumour showed a general structure like granulation tissue , with wellformed capillaries and abundant reticulin . cytologically it was definitely sarcomatous , with large , pleomorphic , usually spindle - shaped cells with large irregular often multiple nuclei and numerous mitoses . although the size and histology of the growth and the necrosis of bone underlying made primary mid - thigh amputation the treatment of choice , his general condition was so bad that it was decided to attempt more by radiotherapy . 
lateral and medial fields were used and skin doses of 3300 and 3000 r respectively given using 220 kv . however , only slight response to this therapy couldbe found on serial biopsy , the tumour cells and stroma remaining as in the first biopsy , but mitoses became less frequent and some collagen was deposited . his blood urea , reduced by diet and conservative measures , again rose above 200 mg . 
he remained well for one year , when he was readmitted for treatment of a mass in the posterior flap of the stump . this mass was excised locally , a wide wedge of tissue being removed down to the bone . this local operation was again performed at the patient 's insistence . section of the tumour contained in this block of tissue revealed the identical histological picture presented by the original tumour and the nodule found in the inguinal lymph node . healing was by first intention . 
black this will prevent loss of time , decrease the period of pain for the treatment . patient , and allow the patient to acclimatize himself to the loss of his leg without radiotherapy should be the disappointment of failed conservative treatment . held in reserve for those patients whose general condition does not permit of operation , and these must be very few now . the treatment ofthe inguinal nodes depends upon the age and general condition extensive block dissection is a formidable undertaking in the of the patient . very old , and in these cases irradiation should be advised . 
where the patient will bear the operation this represents the safest method of eradicating growth . sarcoma , largely owing to its extreme rarity is difficult to recognise both clinically and histologically . it appears to occur more towards the centre of an ulcer than at the edge , to produce a florid fungating cauliflower growth and to these bleed readily . 
as with the squamous growths , sarcomata in varicose ulcers appear less ready to metathis may be due stasise than similar tumours elsewhere or in younger patients . to the fibrosis and scarring present after years of ulceration . 
1. received for publication february 6 , 1947 . attempts to find some reliable basis for prognosis in carcinoma of the breast several factors have been thought valuable in have proved disappointing . formulating a prognosis , chief among which have been the presence or absence of secondary deposits in the axillary lymph nodes and the histological character but it has been found that , even in cases with no axillary involveof the growth . ment and carcinomata of low histological malignancy , there has been a mortality from recurrence of about 25 per cent in the first five years after operation . the axillary lymphatics were the only path by which carcinoma cells could escape from the breast , this mortality would be inexplicable . 
a biopsy specimen from one case in the first case the internal mammary gland was removed was also used . post - mortem in 1938 from a patient who died eleven days after a radical mastectomy . 
the internal mammary vessels also lie in this fat in a plane posterior to the glands and usually about half an inch lateral to the edge of the sternuthe glands may be either medial or lateral to the vessels . 
a thin but strong sheet of fascia , the costosternal fascia , intervenes between the glands and vessels and the pleura in the upper two spaces , and the transversus thoracis muscle in the lower spaces . 
the obliquely running the external intercostal membrane and the internal intercostal muscle are reflected as a somewhat ragged flap , either from lateral to medial and hinged on the inner end of the intercostal space : or from medial to lateral and hinged an inch lateral to the edge of the sternuwe prefer the ' former method , since bleeding from the perforating branch of the internal mammary artery seems easier fibres of the intercostal musculature are so loosely bound together that this flap cannot be neatly sutured back into once the intercostal flap has been reflected , position at the end of the operation . dissection should proceed with non - toothed dissecting forceps only . 
they might give rise to troublesome haemorrhage , but this should easily be controllable by packing while the main trunk was being ligated in the spaces above and below . closure of the intercostal space is done as neatly as possible but is seldom complete . 
cushing , my house - surgeon , has in three instances cleared out the anterior mediastinum on one side for recurrent cancer . it is very likely , i think , that we shall , in the near future , remove the mediastinal contents at some of our primary operations . " this idea does not seem to have been followed up . 
sampson handley ( 1922 ) explored the anterior mediastinum in six cases of carcinoma of the breast , finding glands in two , both of which were the seat of metastasis . 
he described in detail a case in which recurrences ' appeared in the inner ends of the intercostal spaces , one after another from above downwards , in a patient who finally succumbed to the disease twelve years after a radical mastectomy ; and he stated his belief that , by the time the axillary glands were enlarged , the internal mammary glands had frequently , and perhaps usually , been invaded . scarff and liandley ( 1938 ) investigated the ten - year results of radical mastectomy in 172 cases of carcinoma of the breast . 
they found that patients without evidence of axillary deposits ( the so - called stage 1 cases ) had a mortality of 25 per cent from recurrence in the first five years after operation , and that this mortality continued at about the same rate between the 5th and 10th years . 
the treatment of these glands must be by some form of radiotherapy . there seems much to commend sampson handley 's method of burying radium tubes in the intercostal spaces at the time of operation , thus securing a localized but intense irradiation of those points where intensity is most needed . it remains to discover whether , in a large series of cases , invasion of the internal mammary glands is as frequent as it would appear to be , what influence the site of a carcinoma in the breast has on internal mammary deposits , and what is the best method of treatment . 
microscopic examination of this gland might greatly increase the accuracy of prognosis , and prove of considerable assistance in post - operative treatment by irradiation . our thanks are due to the director , the bland sutton institute , the middlesex hospital , for permission to use the pathological reports ; to professor r . 
the frankly keratinizing members of our series we have taken as a standard with which to compare the behaviour of our remaining histological types . the morphological features of the more differentiated epitheliomata have been so completely evaluated that any further discussion would be superfluous . 
philps. from the department of clinical pathology , univer8ity college , ho8pital . received for publication december 5 , 1953 . owing to recent improvements in surgical technique the chances of successful intervention in bronchial carcinoma have much improved , and the need for early diagnosis has correspondingly increased . 
the early recognition of mahgnancy , however , may be very difficult and it is hoped that the method described it does not replace histological in this paper may be a help towards diagnosis . examination of material removed at bronchoscopy , but when no tumour can be seen through the bronchoscope , or when histological examination reveals no tumour tissue it can be of great value . when there is some contra - indication to bronchoseopy , the demonstration of carcinoma cells in the sputum may be the sole means of estabhshing a diagnosis . the demonstration of atypical epithehal cers in the sputum of a patient suffering from bronchial carcinoma is not new . 
a positive result was obtained in 13 of the 25 cases . in 1935 dudgeon and wrigley pubfished details of a simple staining method that could be used on sputum films , in which they employed haemalum and eosin . they also described some varieties of neoplastic cell found in the sputum . subsequent papers ( dudgeon , 1936 ; barrett , 1938 ) enlarged upon the original work . at about the same time , gloyne ( 1937 ) described the cytology of sputum with special reference to neoplastic cells . since then , papers on the subject have been pubhshed in a number ofcountries , including britain ( gowar , 1943 ; bamforth , 1946 ; schuster , 1947 ; perrin and littlejohn , 1950 ) , america ( herbut and clerf , 1946 ; mckay , ware , atwood and harken , ' i948 ; liebow , lindskog and bloomer , 1948 ; papanicolaou , 1949 ; foot , 1952 ) , germany ( schmidtmann and sauer , 1952 ) , russia ( altgauzen , 1939 ) and denmark ( wandall 1943 , 1944 )  . 
the lastmentioned paper is quite outstanding and forms a valuable work of reference on this subject . it has a full bibliography , particularly of the continental literature . the proportion of cases of bronchial carcinoma that can be discovered by for example , sputum examination has varied in the hands of different workers . perrin and littlejohn ( 1950 ) obtained a positive result in 60 per cent whereas wandall ( 1944 ) discovered 84 per cent in this way . all of the reports to which i have had access have shown that occasionary a false positive diagnosis is made by sputum examination . while it is clear f . 
philps that such mistakes are more fikely to be made by an inexperienced worker , there remains the risk that even when the pathologist has considerable experience , errors may still occur . 
herbut and clerf ( 1946 ) point out that patients with early bronchial carcinoma frequently have no sputum and advocate the examination of bronchial secretion . in my hands the examination of sputum has been more successful and has sometimes been positive when examination of bronchial secretion has yielded a negative result . 
the routine is simple for patients who are in hospital . a specimen coughed up in the early morning , before any food or drink is taken , and before the teeth are cleaned , is sent to the laboratory . 
very often , although the specimen is produced before breakfast , it is found to contain particles of food material unless the patient has been warned to eat nothing on waking . specimens that contain particles of food visible to the naked eye should usually be rejected , but when a patient has very rttle sputum , any specimen that can be obtained should be examined . out - patients can be given containers and instructed to bring their sputum in them , but it is important that specimens so produced reach the laboratory as soon as possible , and certainly within 24 hours of being coughed up , otherwise infection and autolysis may destroy the cytological picture . specimens sent through the post , particularly in the winter ,  . 
are occasionally satisfactory , but if long delayed they are useless . the whole success of sputum examination for carcinoma cells depends in the first instance upon the selection of a suitable piece of the specimen for microscopical examination . in order that it may be clearly seen , the specimen is transferred to a petri dish and examined against a dark background . 
a mucopurulent piece that is slightly tinged should be taken if it can be found . if the specimen be frankly and uniformly purulent , then there is no alternative but to take a piece of it at randounder these circumstances the chance of finding neoplastic cells is not good , but on occasion they may be found , and are often of squamous type . it has been found that sputum produced during the first few days after the patient has had a bronchoscopy is unsuitable for examination for carcinoma cells . it contains a great deal of cellular material shed from the tracheal lining and the chance of finding neoplastic cells is therefore reduced . i have made it a practice not to examine sputum until a week has elapsed after bronchoscopy . the most suitable instrument with which to handle sputum is a pair of dissecting forceps that have been sharpened to a point on a grindstone . after a little practice , minute pieces of the specimen can be cut out and manipulated with ease . the piece of sputum removed from the gross specimen is placed on a slide , thoroughly mixed with the help of the forceps , and half of it transferred to a second slide . 
one of these is stained with methylene blue ( see below ) , and the other smeared carefully into as even and thin a layer as possible , and placed while still wet into fixative preparatory to staining with haemalum and eosin . it is essential that precautions be taken to avoid disseminating infection from tuberculous sputa . 
philps group has the advantage that films may be stored and re - examined in the light of subsequent findings , or compared with histological preparations made from a tumour . 
the precise technique used differs only in minor detail from that described by schuster ( 1947 )  . it was taught to me at the london chest hospital , and is as follows : a 0 - 5 per cent aqueous solution of methylene blue is used . 
the shde is then warmed by holding it about 8 above a bunsen flame , and at the same time the two are rapidly mixed with the forceps , until the excess moisture contributed by the stain has evaporated . 
the stained sputum is then heaped into a ridge along the middle of the slide , and a cover glass of suitable length immediately put on it and pressed down so that an even thin film is formed . such films tend to fade after an hour or so , the precise time apparently depending upon the amount of infection present in the specimen , but if it is desired that they last longer , this can sometimes be achieved by sealing round the edge of the cover glass with paraffin wax . schuster ( 1947 ) recommends the addition of glycerine to the stain in order that the preparation may keep longer . all sputa sent for examination are stained first by this technique , which is quick . 
a few crystals of mercuric chloride are allowed to remain in the bottom of the vessel containing the mixture to saturate any moisture that may be absorbed by the alcohol . 
the stain is ready for use in 24 hours and can be used repeatedly for 3 or 4 months . it should be filtered if it shows a deposit . it is essential that the film be fixed immediately after it has been spread and while it is still wet , nor at any subsequent stage must it be abowed to dry . it sometimes happens that a specially characteristic cer or clump of cers is seen in the mothylene blue film , and it is desired to make a permanent preparathis can frequently be done in the following way . 
the cover glass is slid off in a direction exactly at right angles to the long axis of the shde , an operation which occasionally destroys the preparation but more frequently leaves the film in place though somewhat smeared in a transverse direction . the slide is immediately dropped into ' the fixative , where it is left for 5 min . the methylene blue becomes purple during fixation . 
undoubtedly this is desirable , but it ' has been found in the present series that between 20 and 30 minutes are required for the preparation and complete examination of a film and it has been impracticable to examine six films from each specimen . 
the writer has found it more profitable to look at it with the naked - eye first so that any parts of it that show a streaky appearance may be especially selected for it has been found that carcinoma cells tend to occur in minute examination . streaks and when these are seen they should be searched throughout their entire length and depth . normally , films are examined with the 1 - inch objective , the i - inch objective being used only when likely cers are seen with the low power . there is little - inch objective in this work , though it is occasionany useful for demand for the examining the chromatin pattem , especiary in oat cells . 
a rather powerful lamp should be used ( a 200 watt bulb is satisfactory ) so that the condenser of the microscope may be lowered shghtly in order to obtain maximum resolution and contrast . 
the nuclear border is smooth and devoid of wrinkhng or irregularity . sometimes , particularly in infected sputum that has stood on the bench for some time , squamous cells are seen which are infiltrated with neutrophil leucocytes . 
39 shows such a carcinoma cells and can ' be a serious source of confusion . cell from a patient in whom there was no evidence of carcinoma . less commonly , a smaller type of squamous cell is seen , which stains more deeply than that just described . it is about 20 microns in diameter , and usually occurs as part of a small sheet of epithelium in the spututhe cytoplasm stains pure b ' lue ( as opposed to green ) with methylene blue , or fairly deep pink with eosthe outline of the cefl is frequently angular - a feature that is evident when such cells are seen lying singly . 
normal epithelial cells tend to be regular in shape , whereas carcinoma cells , particularly those of squamous type , show an irregularity which is best appreciated when many are seen together in the low - power field . 
macrophages. macrophages are constantly found in the sputum in large or small numbers , and are sometimes rather difficult to distinguish from carcinoma cens . many macrophages contain dust particles , which appear as black or brown granules in the haemalum and eosin - stained preparation , and as black , greenish , or purple granules in a film stained with methylene blue . sometimes in a film stained by the latter method , the macrophages are seen to contain a large number of highly refractile fat droplets . 
the presence of dust particles in a cell enables it to be identified as a macrophage , but confusion may arise through the presence of free dust particles overlying a cell and giving the impression of being contained within it . normally they are from 10 to 50 microns in diameter , but , exceptionally , large forms occur . 
as a general rule , they are more or less circular in outline , but this feature is bv no means constant and they assume a variety of shapes . spindle shaped and crescentic forms are not uncommon , and occasionally they may assume a tadpole - fike shape , and may thus be confused with some types of carcinoma cell if shape alone be relied usually the cytoplasm is eosinophilic when stained upon for identification . with haemalum and eosin , but ' it may stain somewhat brownish owing to the presence of ingested particles . 
with methylene blue , it is usuall ' stained blue but when there is a large amount of ingested material the colour may be anything from green to pinkish purple . 
the cytoplasm stains blue with methylene blue , and pink with eosin . the nucleus stains rather deeply and may show some unevenness in the distriit is circular in shape and the nuclei of neighbouring bution of the chromatin . cells in a clump maintain their shape and do not indent each other . cells from oat cell carcinomata , when seen in the sputum , are similar in size to lymphocytes , but differ from them in the following ways : ( a ) the nucleus of an oat cell is larger in relation to the cell area than that of a lymphocyte . 
the cytoplasm of an oat cer appears as only a thin rim round the nucleus , or it may not be visible at all . ( b ) the chromatin of an oat cell sometimes stains more deeply than that of a lymphocyte , and when seen under the - inch objective , shows as a reticulum as opposed to the rather lumpy chromatin of the lymphocyte . ( c ) oat cells nearly always appear in clumps ; lymphocytes seldom do . frequently , oat cers are so closely opposed to each other that they appear t - 0 form a syncytiuthe individual cer borders of lymphocytes are always seen . ( d ) the individual nuclei of oat cers , though usually fairly constant in size , vary considerably in shape . it will be seen that neighbouring nuclei compress and indent each other . 
the only normal cell found in the sputum which occasionally shows this compression effect is the macrophage , which is unhkely to be confused with an oat cell . lymphocytes are shown in fig . 
they are circular bodies , from 10 to 20 microns in diameter . they stain deep blue with methylene blue , and pink , yellowish or - brown with eosalmost always their non - cellular nature is clear : they may show concentric rings , - radial streaking or fissures , or they may be structureless . 
43. - a drawing of a cell seen in a methylene blue filthe cell " body " is a macrophage , and the " nucleus " is a corpus amylaceum which has been taken up . this appearance should not lead to difficulty , a - s the lack of any nuclear details and the concentric rings in the corpus amylaceum make its nature obvious . 
26. - two cell bodies united by a filamentous cytoplasmic bridge . this appearance is not commonly seen , but when present it is considered by the writer to be diagnostic of squamous cell carcinoma . carcinoma whenever considerable pleomorphism is seen in epithelial cells , it should be stressed that a moderate degree may be seen in conditions unassociated fig . 
35 shows an appearance which was mistakenly thought with carcinoma . to be due to carcinoma in a patient who showed no other evidence of a tumour at the time , who has been followed for a year and has developed no sign of the disease . the staining reaction of the cytoplasm is somewhat variable , but may be of some help in identification . 
with methylene blue , it frequently stains greener than that of normal cells , but this property is shared by any degenerate epithelial cell , be it from a carcinoma or from a non - malignant condition , so it is in no way diagnostic . 
the cytoplasm of many squamous carcinoma cells is peculiar in that it appears to be more refractile than that of normal epithelial cells . the methylene blue preparation , this property shows itself by the presence of a dark , rather emerald green outline to the cell and sometimes also to the nucleus within it . 
the cytoplasm itself appears lighter and slightly luminous compared with that of the surrounding normal cells . when stained with haemalum and eosin , the cytoplasm as a general rule stains bright pink , occasionally with a tinge of orange . frequently , as in the methylene blue film , the cell appears brighter than those round it , and if it is put slightly out of focus it may shine up quite brilliantly . cells of this type have been named " bright cells " and are in my opinion diagnostic of squamous cen carcinoma . 
25. - cells from squamous cell carcinomata that give the appearance of wrinkling often , squamous carcinoma cells show a series of irregular concentric lines in the cytothese may be seen most commonly at the periphery , although they are seen to the best advantage in the methylene blue film , they show in of the cytoplasm . plasm , which appear to be minute folds . but they may also occur round the nucleus . the permanent film as well . the nuclei of squamous carcinoma cers have few constant features . another feature frequently seen in the methylene blue film is a mass of minute refractile bodies which are usually disposed in a circular manner round the nucleus . on close inspection , the individual particles sometimes appear to be angular in outhne rather than circular . 
24. - cells showing collections of minute refractile particles in the cytoplasm . these particles are transparent and tend to occur most commonly in a circular arrangement round the nucleus , but they may be seen in any part of the cell . 
normal squamous epithelial cells not uncommonly show sirnilar particles in the neighbourhood of the nucleus , but in the writer 's experience , these are not seen in such large numbers as in carcinoma cells , nor are they concentrated so definitely in one portion of the cell . these particles must be clearly distinguished from the larger , usually black , dust particles and from the large circular fat droplets that are commonly seen in macropltages . dust particles usually present no difficulty owing to their larger size , dark colour and the fact that they are evenly distributed throughout the cell . fat droplets are usually evenly distributed , and appear globular . the six drawings , and those in fig . 
the presence of mitoses in epithehal cells does not imply malignancy , as it may occur in any condition in which there is a considerable amount of epithelial regeneration . in addition to the features mentioned above , a nuihber of other characteristics may be seen which are of considera - ble help in the diagnosis of carcinoma of squamous cell type . 
a particular type of clump has been found to occur in both squamous cer and adenocarcinoma , and though not absolutely diagnostic of mahgnancv appears to be nearly always associated with it . 
the cells all appear to spring from a central point and the clump gives the impression that it may have formed part of a polypoid mass that has broken off into the sputum . if this is correct then any condition associated with papilliferous projections into a bronchus could give rise to such clumps and they might be expected in the sputum in bronchiectasis . i have not seen such clumps in bronchiectatic sputum , but a clump of this type has , nevertheless , led to a mistake . 
philps in the presence of such a change , cells from the metaplastic area would probably be seen in the sputum , but their morphology is not clearlv known . occasionary , round cells of squamous type which have the pecuhar glistening cytoplasm that one associates with keratinisation are seen in the methylene blue preparation . these cells differ from carcinoma cells in that their nuclei are regular in size and shape , though they are often somewhat large in relation to the size of the cell . 
they do not suggest carcinoma in the latter preparation , though they may give rise to suspicion in the methylene blue film . it appears that cells of this type are young squamous cells which may have been derived from the mouth or pharynx or may possibly have come from a metaplastic area in a bronchus . 
the cvtoplasm is geanty , forming at the most a thin rim round the nucleus , which nearly fills the cell . in niany cells , no cytoplasm at all is seen : in others , when the clump is examinedlinder the - j - - inch objective , cell borders cannot be defined , the ceus appearmg to form a svncvtiiithe cytoplasm when seen stains pink with eosin . the nucleus stains deeply with haemalum , and is seldom circular as the nuclei of neighbouring cells indent each other , giving the appearance of having been pressed together . this feature is of great importance in the identification of these cells , and in conjunction with the clumpiing and relatively large nuclear size , appears to be diagnostic and makes the cers easy to recognise . 
the nuclear chromatin is usually clearly defined when thecell is seen under the - ! - - inch objective , and is reminiscent of the appearance of the , reticulum of a stained reticulocyte . less commonly , particularly in degenerate cells , the nucleus may be denser and the chromatin network difficult to define . oat cells are shown in fig . 
the round cers were about twice the size of an pat cell , that is , from 20 to 25 microns in diameter , and they showed greater variation in some , the nucleus was vesicular and nearly fined the cell : than do oat cells . in others , it appeared somewhat contracted and stained more deeply , while in the third and commonest type the nucleus was quite smah and stained nearly spindle cells were seen in clumps amona the streaks of round cens . 
typically , the cells appear in clumps and show vacuolation ' of the cytoplasm , the vacuoles firequently filling the cell and pushing the nucleus to one side , often flatten ' mg ' it against the cell wall . the appearance shown in fig . 
31 , which is from the sputum of a patient diagnosed histoloyicallv as suffering from alveolar cell carcinoma , is very si ' milar to that described by the above - mentioned writers in adenocarcinoma . the presence of cells showing vacuolation is not in itself evidence of carcinoma . the cells shown in fig . 
38 were from the sputum of a patient who showed n ' o evidence of carcinoma , and who , because of th.e presence of these and similar cells has been followed for a - year and has ' developed no tumour . therefore , unless the ceus showing vacuolation occur in clumps and show other characteristics associated with malignancy , they must be considered to be unreliable as evidence of carcinoma . quite frequently , in sputa showing ample evidence of carcinoma of squamous cell type , clumps of cells are seen which surround a single vacuole . 
cers seen which constitute clear evidence of carcinoma . can be g ' iven . categories 1 , 3 and 4 appear from the results to be valuable as an indication of whether the patient has carcinoma , but the value of category 2 , judging from the analysis of results which follows , appears open to question . it will be seen that of the . 
untraced. no cells suggestive of carcinoma seen category 1 . in sputum catego , ry 2 . atypical epithelial cells seen upon which no certain opinion can be given category 3 . cells seen which are highly suggestive of carcinoma category 4 . cells seen which constitute clear evidence of carcinoma of the 9 patients untraced , 8 were out - patients in whose sputum no cells suggestive of carcinoma were found , and who did not return to the hospital . 
he left the hospital soon afterwards and the final diagnosis is not at present known to the writer . of the 8 cases recorded as not yet diagnosed , 3 had no cells suggestive of carcinoma in their sputum , 3 showed epithelial cells which were considered to be f . 
philps atypical but were not thought to constitute evidence of carcinoma , i showed cells that were highly suggestive of carcinoma and 1 , cells that were held to constitute clear evidence of it . 
the 2 patients who were diagnosed as sputum positive are both elderly men in one of whom there is strongly suggestive radiological evidence of carcinoma with persistent collapse of the right lower lobe but no tumour demonstrable on bronchoscopy . 
the other has a shadow persisting in the left mid - zone but has acid - fast bacilli in his sputuit is thought quite probable by those in clinical charge of him that he has carcinoma as well as tuberculosis . 
no bronchoscopy has been performed . * of the 123 patients , there are 106 in whom a final diagnosis has been reached . the results of sputum examination on these 106 will be considered in the analysis which follows . for the purpose of analysis , it is considered that categories 1 and 2 constitute a negative , and 3 and 4 a positive sputum diagnosis , and the terms " sputum negative " and " sputum positive " are used in this sense . it wfll be seen from table i that in two cases , cells that were highly suggestive of carcinoma were seen in the sputum of patients who were finally diagnosed as not having suffered from the condition . one of these patients has now come to post - mortem at which a diagnosis of haemorrhagic bronchitis was made : the other , who was admitted complaining of haemoptysis , is now well , with no evidence of any pulmonary lesion . 
the films ofthe sputa of both these patients have been reviewed and a single clump of cells in the former would still be held to be highly suggestive of carcinoma . in the case of the latter patient , there was a large amoudt ofrather eosinophilic epithelial debris , in the film , the appearance being one which would not now be thought by the writer to be suggestive of carcinoma unless some indication of the mahgnant nature of the cells were also present . 
of the two errors described here , the first must be held to be due to a limitation of the method , whereas the second was caused by lack of experience . of the 106 patients under review , , 39 were finally diagnosed as suffering from bronchial carcinoma , and 67 from other conditions . 
41. total cases in the series cases finally diagnosed as positive cases finally diagnosed as negative total positive diagnoses made by sputum examination correct positive diagnoses false positive diagnoses percentage of negative cases incorrectlydiagnosed as positive 30 false positive diagnoses expressed as a percentage of the total series positive cases in which carcinoma cells were not found in the sputum 9 percentage of positive cases in which carcinoma cells were not found 23percentage of positive cases correctly diagnosed by sputum examination addendum - at the time of going to press , these two patients a - re still udder observation . 
the one whose sputum contained cells that were considered clear evidence of carcinoma has now been readmitted to hospital a year after the cells were first found with clear clinical evidence of carcinoma with multiple bone metatases . 
b is sputum now contains cells similar to , but more pleomorphic than those first found . the other , whose sputum contained cells that were thought highly suggestive of carcinoma has been treated for a year for pulmonary tuberculosis and has improved , ' though the radiological picture is little changed . 
patient8 correctly diagno8ed a8 8putum negative . total patients one speciinen only examined two speciinens examined three four five total number of specimens examlined from these 65 patients mean of number of specimens examined in sputum negative patients j . 
of those who had carcinomata , 30 ( 76 - 9 per cent ) showed carcinoma cells in the sputum . sputum specimens from two patients in the series were wrongly reported as positive . 
one of these patients complained of haemoptysis but recovered rapidly and subsequently showed no evidence of any lung lesion . his sputum contained a great deal of eosinophihc cell debris which was thought to be the remains of necrotic carcinoma cells . 
he died and at post - mortem examination was diagnosed as having suffered from haemorrhagic bronchitis , no evidence of carcinoma being found . those from the first would not now be considered suggestive of carcinoma as the cells showed no other appearance associated with mahgnancy . 
the clump of cells from the second patient would still be held to be suggestive of carcinoma if seen again , which indicates that the method has limitations . further investigation is required into the significance of clumps of cells of this type . it ha - s been my experience that when a confident diagnosis of carcinoma can be made from sputum examination ' , it is usually possible to tell the predominant cell type in the tumour , and so far , when there has been an opportunity for histological confirmation , this has been show ' n to be correct . it has been stressed that in a series of this type , it is possible that misdiagnoses of carcinoma may go undiscovered because the proportion of positive cases is high . it is not certain that there are no such mistakes in the present series but since only about one third of the patients were in fact suffering from bronchial carcinoma , the chances are in favour of such errors being discovered . it is necessary that the limitation of a diagnostic technique of this type be clearly understood . 
a negative finding is of no significance in the exclusion of carcinoma , and may be due simply to the fact that the miinute portion of the specimen chosen for examination contains no cells that can be recognised as malignant . this is likely to be the commonest cause of failure . 
of these , a final diagnosis had been reached at the time of writing in 106 , 39 being shown to suffer from bronchial carcinoma . cells which were either highly suggestive of carcinoma or were considered to be clear evidence of it were seen in the sputum of 30 ( 76 - 9 per cent ) of these . 
an attempt is made to analyse the effect of the number of specimens examined upon the accuracy of diagnosis . where possible , it has been the writer 's practice to state the predominant cell type when a positive report is made . this was done in 23 of the 30 cases so reported . 
an opportun ' ity for histological confirmation has occurred in 10 of these , and there has been agreement . two sputa were erroneously thought to contain cells which were highly suggestive of carcinoma . 
the reasons for these two misdiagnoses are critically examined and it is concluded that one could have been avoided and one could not . further research is necessary to eliminate false positive diagnoses . my thanks are due to professor m . 
3. - normal bronchial epithelial cells obtained by aspiration at bronchoscopy . characteristically these cells are elongated with a ciliated free border and a filiform point of attachment to the ba - sement membrane . 
the nucleus , which ir , regular in size and oval in shape , is nearer to the attached end than to the free border of the cell and tends to make a small expansion in the cell body . 
on close inspection , however , it will be seen that a number of cells in the clump have the general shape of bronchial epithelial cells , showing a wide free border and a filiform point of attachment , and the nuclear distortion is mainly due to the presence of it is possible to discern gradations from those which appear vacuoles in the cytoplasm . nearly normal to those which seem grossly abnormal . 
the strongly eosinophilic cytoplasm is also suggestive of carcinoma , but may occasionally be seen in other degenerate epithelial cells . it should be noted that the appearance suggestive of inclusions seen in this cell differs from that shown in fig . 
the nucleus shows no unusual characteristics and is situated in the wider " body " of the cell . sometimes , chromatin masses are seen in the tail , and on occasion , two cell bodies , each containing a nucleus , are united by a long filamentous bridge . 
the writer has seen them only in cases of squamous cell carcinoma , and nothing resembling them has been seen in any sputum specimen from a non - malignant condition . they appear considerably more refractile than do normal cells , and by virtue of this property , look bright when compared with the cells that surround thewhen put slightly out of focus they shine brilliantly . the high refractility of these cells is possibly associated with keratinisation , and may be related to the appearance shown in fig . 
and the cell itself is surrounded by a greenish coloured band which is probably due to some optical property of the cytoplasm . its brilliance is enhanced compared with the cells in the surrounding field . 
the coloured band which surrounds the cell stands out clearly . in addition to the cell described , there is a considerable amount of eosinophilic debris shown , similar to that seen in fig . 
34 , which is from the sputum of a patient diagnosed clinically as suffering from bronchial carcinoma , but which is considered by the writer to constitute insufficient evidence to enable a diagnosis of carcinoma to be made . 
the present writer now shows considerable caution in the interpretation of the significance of such clumps as two mistakes have been made . before this it was thought that clumps of epithelial cells of this type constituted strong evidence of carcinoma . 
41 and 42 , which were both thought to be strongly suggestive of carcinoma , were from patients who had no other evidence of carcinoma at the tiirne , and in one of whom there wa - s later no post - mortem evidence . 
they have the following chaxacteristics which , taken together , distinguish them clearly from any other cell that is seen in the sputum : the cytopla - sm may be visible as a thin nvhere neighbouring cells are closely applied to each other , riirn , or it may not be seen at all . as is often the case , cell borders are not seen , the appearance being that of a syncytium . ( 2 ) the nuclei of all the cells in a clump are of approxiinately the same size , but they vary considerably in shape , many of them tending to be rectangular . 
the reason for this is that the nuclei of neighbouring cells indent each other . this is the most important single feature in the identification of oat cells . ( 3 ) the nucleus usually stains deeply , but the chromatin pattern can nearly alway 's be distinguished . 
29. - ( 2 ) spheroidal and 8pindle cell carcinonw . a field showing a group of cells similar tov but larger than , oat cells and a small bundle of spindle cells . 
34. - a clump of cells , the individual members of which have no definite characteristics of malignancy though one of the cells seems to possess large nucleoh - an appearance which may be due to the superimposition of pus cells . 
at one time , clumps of this type were thought by the writer to be diagnostic of carcinoma , but a clump of rather similar appearance led to a false positive diagnosis in a patient who was found at postmortem examination not to be suffering from carcinoma . for clumps of cells that are considered to be diagnostic of carcinoma , see fig . 
35. - a group of epithelial cells showing a considerable degree of pleomorphism and nuclear degeneration . this is the most confusing appearance that has been seen in the whole series . 
the cells resemble carcinoma cells closely , but in no case is the nucleus large . this field , and the three that follow , were from the sputum of a single patient , in whom a positive diagnosis was made as a ' result . 
41. - a clump of cells which appear to surround a vacuole from the sputum of a patient who , on the strength of this evidence , was thought by the writer to be suffering from bronchial carcinoma . 
daily , add the remainder received twice this dose . table i shows the result of this experiment on the group receiving the lower dose level ; the treated tumours were completely inhibited . 
smar nodules persisted in the majority of these animals without change for about 2 weeks , after whicb tumours began to grow ; they were well developed in 70 per cent of the group 1 month after cessation of treatment . 
i and it seems reasonable to suppose that the same applies to all such tumours developing from inhibited nodules . when drug treatment was commenced 3 - 5 days after transplantation , both the sensitive walker tumour and its refractory derivative were always actively growing . 
the growth of the derived tumour was affected to a reasonably consistent extent by triethylene melamine , comparable to that observed with the lymphosarcoma . the subsequent development of inhibited walker tumour nodules has been surprisingly , growth was found to occur after a similar repeatedly confirmed . latent period in the majority of animals even though drug treatment was continued 340 h . 
ad example of this is shown id table iv , from wbich it is evident that tumours developed in 8 - 10 animals following the usual inbibitory period of nearly 3 weeks . it proceeded rapidly and then slowed quite markedly . in spite of the prolonged treatment in which 31 doses were given , there were no deaths which could be directly attributed to the effect of the drug . this faflure of continued treatment to maintain the state of inhibition id the tumour has also been confirmecl in other experiments . the contrast in susceptibihty between the original and derived walker tumours to the triazine , has also been found . 
as was mentioned earlier , the development of mouse leukaemia resistant to fohc acid analogues is wen known and there has been a recent report that the mouse sarcoma 180 , whicb is moderately inbibited by 6 - mercaptopurine , rapidly develops some resistance to this compound ( clarke , philips , stemberg , stock , elion and hitchings , 1953 )  . on the - whole , solid rat and mouse tumours appear to be relatively resistant to chemical inhibitors , although the response of different tumours to the same drug varies widely . 
not often does the arrest of growth extend to all tumours in an adequate group of experimental animals , in spite of the administration of dose levels of near lethal magnitude ( suguira and , stock , 1952a , 1952b )  . appears that rat tumours are more susceptible than those of the mouse to trie - thylene melamine , for complete regression has been obtained in nearly 100 per cent , of animals with the jensen rat sarcoma , sarcoma r39 and the flexner joblidg it is generally agreed that the longer carcinoma ( suguira and stock , 1952b )  . initiation of treatment is delayed , the less chance thei - e is of total regression . - the action of triethylene melamine on the walker carcinosarcoma is striking - even when treatment is delayed for as long as 5 days after implantation , by which time the tumour is actively growing . in the present series of experiments regression occurrecl in every animal and usuary little or no palpable material this confirms the work of hendry , homer , - remained at the site of the implant . rose and walpole ( 1951 ) and peczenik ( 1952 ) , who however , commenced treatment curiously , 24 hr . 
after transplantation of the walker tumour into wistar rats . suguira and stock ( 1952b ) were less successful with this tumour in wistar rats , .obtaining inhibition of growth in 70 per cent of animals with day old implants and regression in only 20 per cent when treatment was delayed for 7 days . 
the results clearly show that in effectively 4h animals the inhibitory effect is only temporary and that growth subsequently occurred irrespective of the duration of treatment , even though this may be continued for several weeks instead of the usual 7 - 10 in either case the suppression of growth continued for upwards of 2 weeks days . before renewal of activity could be detected . 
the derived tumour on which most of the work has been carried out , was selected at random from a group of tumours growing subsequent to one short course of treatment applied to the original walker tumour . 
the resistance is thus considered to be a stable and permanent change . another member of a group of tumours similarly derived from the original walker carcinosarcoma has also been shown to possess comparable resistance to further treatment . it is reasonable to suppose that the same will apply to all such tumours . 
a noticeable difference between the original walker and the derived tumours is the more rapid growth of the latter in untreated animals . the growth of tumours after a latent period followino , a short course of treatment with triethylene melamine , must be due to the survival of a small number of cells which are naturally resistant to the drug . 
the fact that this sequence of events is not changed by the continued administration of triethylene melamine to animals bearing implants of the original walker tumour , suggests that the resistance of the residual cells is maximal at the outset . additional support for this view emerges from the failure to enhance the resistance by further exposure to the drug . 
how far mutagenic effects of the ethyleneimine may be concerned remains to be investigated , but the fact that such a bigli proportiod of inhibited tumours ultimately grow seems to make this factor less likely . 
the resistant tumour has also been shown to be refractory to two other ethyleneimines ( compounds ii and iii ) at dose levels which completely inhibit the original walker thus resistance to triethylene melamine confers resistance to carcinosarcoma . a diethyleneimine , and this may be true of active ethyleneimines in general . how far the same statement may apply to other kinds of chemical inhibitors active against the ordinary walker tumour is being investigated . it is interesting that the walker tumour should be so sensitive to triethylene melamine , whilst two other tumours which have been tested in the same strain of animal ( a mammary adenocarcinoma and the lymphosarcoma referred to in the crossley , allison , wainio text ) were only little affected by the same treatment . and muenzen ( 1951 ) studied the effect of triethylene melamine on a sarcoma ( 231 ) in the king a rat . 
of the triazine without undue toxic treatment of 7 - day old transplants of the flexner jobhng careinomaeffects . with this dose rate for 7 days produced regressions in 90 per cent of animals in there was no reappearance of tumours during the next 3 months , 1 to 2 weeks . which was taken to indicate complete cure . 
not only different kinds of tumour but various strains of rat vary in their susceptibihty to triethylene melamine ; the growth of an occasional tumour in animals bearino , a neoplasm susceptible to the drug , may be connected with some unsuspected ability of the host animal to dispose of the administered compound . it appears reasonable to suppose that ethyleneimino - compounds as a whole owe their anti - tumour activity to these highly reactive groups , so that it is difficult to conceive a protective mechanism possessed by some cefls but not by the great majority it is equally difficult to imagine a high degree of susceptibility in a tumour . in one variety of neoplasm and indifference in another kind to chemical inhibitors hke triethyleneimino - phospboramide ( iii ) , which is highly soluble in water and hkely to diffuse with ease into cells . 
then too , there is the fact which has been estabhshed on many occasions , that the susceptibility of sensitive tumours to these drugs diminishes markedly with the age ( i.e. , size ) of the tumour . it is hoped that a study of the mechanism by which the resistant walker tumour is derived from the original variety and an investigation of the reason for the insusceptibihty of the formee tumour may throw light on these interesting and important phenomena . inhibited nodules from the walker carcinosarcoma treated with triethylene melamine , 24 hr . 
after the conclusion of a course of treatment show intact tumour cells . no mitotic figures were seen . estimation of the mitotic index of the original and derived forms , 48 hr . 
after the administration of the last of 2 doses of the same drug reveals that the growth rates of the two tumours are similarly depressed . the drug would therefore , appear to be exerting a cytotoxic effect on the resistant form , although the overall growth of this tumour is not much hindered by such treatment . 
 although urethane has been mentioned as carcinogenic for mouse ( nettleship and henshaw , 1943 ) and rat lung ( jaffe , 1947 ) this action has not yet been reported in other animals . 
since the inherited susceptibility to most known cancers is due to dominant genes this was anticipated here , and con sequently a large number of the c57 backcross mice were bred in order to note segregation , which should be manifest in the group on this assumption . 
preliminary experiments indicated that the various strains and crosses of mice used did not differ in their fluid intake , and consequently strain differences due to this treatment were not due to a different intake of the carcinogen . 
they were from another experiment and were only given 7 weeks ' urethane treatment , though they were killed 7 months from the beginning of treatment , the same as the rest . 
 when the mice were sacrificed their lungs were removed and fixed in 10 per cent formol - saline for 24 hours , which preserved the material and made handling easy . 
since nearly all lung tumours in mice tend to occur on the periphery of the lobes ( grady and stewart , 1940 ) the lobes were separated and the number of nodules on their surface visible to the naked eye were counted . 
in a previous paper ( cowen , 194 7 ) it was noted that strains of mice which gave a low number oflung tumours had tumours of a smaller size . 
 since the tumours in a lobe varied in size from microscopic dimensions to nodules about 4 m in diameter , it was not feasible to use the average size of all these tumours . 
the best way of gauging the response on a basis of tumour size was considered to be that of determining the size attained by the largest tumour in the total lungs of a mouse . 
this was tested statistically using the formula v ' ; ; ; 2 on the other hand , the fl hybrids were slightly but significantly lower than both of these classes . 
the polygon for the 057 backcross mice is obviously bimodal , and roughly consists of a combination of the figures for the 057 and fl hybrid mice in approximately equal proportions . 
 it may be mentioned that the a backcross mice which segregated for colour giving three phenotypes , albino , non - agouti and non - agouti brown , showed no apparent linkage of susceptibility with colour . 
 - ~ number of tumours f 3 . - - scatter diagram showing the relationship between the 2 groups of c57 backcross mice with respect to number and size of tumours . 
 thus , of all the chickens and guinea - pigs treated with urethane , only one chicken developed a neoplasm which was lymphoid in orig this type of tumour is not uncommon in chickens normally , and is not considered to be due to treatment with urethane . 
the first ( number of tumours ) gave more obvious results than the second ( size of the largest tumour per mouse ) , though both results closely paralleled each other . 
 these results point most significantly to the existence of a single dominant gene in a mice which is responsible for urethane - induced lung tumour suscepti bility , the c57 mice carrying the recessive . 
this does not entirely explain the results , for if a single dominant gene only were responsible , then a , fl , a back cross and the high group of the c57 backcross mice would all have exactly the same tumour incidence , which is not the case . 
firstly , the tumour susceptibility was genetically ina.ependent of mortality , and secondly , as the mortality was considerable only in the a and a backcross mice , a higher tumour susceptibility in the dead mice would merely have emphasized the line differences . 
 heston ( 1940 , 1942a , 1942b ) reported somewhat similar results using spon taneous and hydrocarbon - induced lung tumours in a and l mice ( high and low strains respectively )  . 
a possible reason for this is that the incidence of lung tumours in these mice was much lower than in the urethane - treated mice of the c57 backcross as reported here . 
 from the results of these workers , it appears that certain carcinogenic chemicals cause different lung tumour incidences in different strains of mice depending on the incidence of spontaneous lung tumours in these strains . 
that is , a strain of mice which develops few spontaneous lung tumours does not respond so well to a carcinogen as a strain which has a high spontaneous incidence . 
from this , it seems that environmental factors ( certain carcinogens ) do not simply cause tumours , but increase the incidence of them in mice depending on the inherited tendency of mice to develop the this argument can most probably be applied to other animals as well as mice . 
 it seems rather significant that no reports have been found in the literature of spontaneous ( or induced ) lung tumours in guinea - pigs , and out of the many neoplasms that arise in chickens , only one report exists of a spontaneous lung tumour in these animals ( apperly , 1935 )  . 
for example , guinea - pigs , which have a relatively frequent incidence of spontaneous liposarcomas ( warren and gates , 1941 ) , develop these tumours on treatment with hydrocarbons ( shimkin and mider , 1941 )  . 
it was considered that the resistance of mice to infections in general was lowered , and at the same time a specific carcinogenic virus was responsible for the lung tumours . 
if a single recessive gene is assumed to be the cause of the different mortalities , then the a backcross would be the segregating group , and should have a survival rate equal to the average of those for the a and c57 mice . 
from table i it is seen to be 45 , which agrees reasonably with the theoretical figure considering the small number of mice involved ( x2 = 317 , p > 005 )  . 
 it can thus be safely concluded that the mechanism whereby strain a mice are genetically susceptible to lung tumours is not the same as the one responsible for their susceptibility to general infections . 
correlation between leucopaenicity causing susceptibility to infection on one hand and a carcinogenic virus causing lung tumours on the other is therefore considered most unlikely in mice given urethane treatment . 
 two criteria which parallel each other closely are used as an index of response of mice to the carcinogenic action of urethane - the number of tumours per mouse and the size attained by the largest tumour in total lungs . 
kemp. from ae university institute , for human genetics , copenhagen . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . from ancient times it has been observed that cancer often occurs familially the inheritance of tumour 's in human beings has been studied and discussed for centuries , and it has especiallv been the object of extensive systematic investigations during the last decade , , about 6 years ago , a group of collaborators at the university institute for human genetics - in copenhagen decided to make an attempt to investigate the the ' investigation has partlybeen carried genetics of various aspects of cancer . out in co - operation with the danish cancer registry , under the direction of j . 
clemmesen , the university institute of pathological anatomy , and the radium centre in copenhagen and numerous danish hospitals and clinics . the work was supported by kong christian x 's fond , landsforenigen til kraeftens bekaempelse and anders hasselbalchs fond . these investigations include genetic experiments ' in mice and studies in man . twin examinations were also initiated in co - operation with the cancer registry . the statistical - genealogical investigations have been performecl as a series of surveys each concerning a considerable number , usually sevetal hundreds , of probands or propositi with cancer of a ce - rtain - type , e.g. 
canc - er mammae , cancer uteri , cancer oesophagi , multiple cancer or leukaemia , picked at random from the population . these investigations were made by a number of physicians , each being a ecialist in the field his study coneems . 
the families have been studied thoroughly , and every case of cancer in the relatives has , so far as possible , been verified ; in that respeot these investigations differ from earlier , more compre hensive statistical studies in the heredity of cancer . 
cancer of the breast , uterus , stomach and rectum , their occasionally familial occurrence has been know - n for in order to elucidate the etiologic significance of hered ' itary many years . factors in these tumours , proband investigation has been carried out . jacobsen 's ( 1946 ) study on the heredity in breast cancer includes ' 200 probands , ( 197 women and 3 men ) with cancer of the breast . 
the investigations of the probands ' families comprise the following categories of relationsi : parents , brothers and sisters , grandparents and brothers and sisters of the parents . videbaek ( 1947 ) has investigated ' edigrees of 20 ' 9 patients with leukaemia and 200 control probands , using the same methods as jacobsen . the propositi - method of investigation is , of course , rather complicated and leaves room for several sources of error . it must be realized that the diagnoses and the information on the whole as regards the older or more distant groups of relations are rather unreliable . 
some of the grandparents , for instance , died more than 50 years ago , and at that time , diaanostic skill was more limited and hospital records and death certificates were more insufficient than to - day . furthermore , it is difficult to procure a comparable control , material , because the probands are normally more interested in the occurrence of cancer in the family than normal control probands are ; probably that is the reason why the information conceming the distant groups of relations in jacobsen 's control material is insufficient . also it must be considered that during recent years many cancer patients , e.g. 
suffering from skin cancer , get cured without knowing they have had cancer , and thus escapenotice by the investigator . it should also be pointed out that the calculation of the morbidity risk is a complicated method , and cannot always be relied on . 
lip and skin cancer , are not represented in the families of the probands , but cancer of most other forms , sites and types occurs in the relatives in about the same proportion as among the r ' elations of the control probands , and is comprised under the collect ' lve term " endogenous cancer as a whole . " according to jacobsen ( 1946 ) , a study of the case histories of the probands gives no basis for supposing that extemal factors play any important role in the development of breast cancer . 
an excess incidence of breast cancer among the female relatives of the probands and likewise a significant excess incidence of " endogenous cancer as a whole " in all the categories of relatives , both male and female , were found . this indicates hereditary predisposition as the chief factor in the development of breast cancer . breast cancer is dependent o ' n hereditary factors , and the tendency to this particular form of the diseas.e is bound up with an inherited predisposition to endogenous cancers endogenous cancer in general . 
the localization of the tumour is determined either by hereditary or extemal factors . in many pedigrees the general hereditary predisposition appears to be inherited as a dominant character . in the leukaemia proband material , the familial incidence of the disease was found to be at least 8 per cent . several types of leukaemia ( acute or chronic lymphoge ' neous or myelogenous , monocytic or stem - cell leukaemia ) may occur in the same family -  . 
the multiple occurrence of leukaemia in an individual family is usually not confined to some particular type , which indicates that leukal - imia is probably genetically a morbid - entity . among members of a family there seems to be an age correlation as regards the onset of leukaemia.. 
according to videbaek ( 1947 ) leukaemia , as such , is not simple domininherited ; it is a question of inherited disposition to the disease . ance or recessivity may possibly be excluded ; it may have a genetical - basis with incomplete dominance or polymeria ( homologous polymeric factors )  . hereditary predisposition to disease is generally regarded as polymeric . 
the expression of the character is furthermore dependent on the interaction between the genotype and environment . the incidence of pemicious anaemia is significantly higher among the relatives of patients with leukaemia than among the relatives of the control probands . the relation is probably due . 
among the relatives of the leukaemia patients there is a significantly excessive incidence cancer , of cancer as a whole , due to a high incidence of all forms of cancer . including leukaemia , is piobably a disease entity genetically dependent on a dominant gene common for all the different forms of " endogenous cancer . " according to videbaek 's oplinlon the - development of leukaemia seems to depend on various conditions , among others , on a non - specific hereditary predisposition to cancer , which is believed to be present in at least 20 per cent of thepopulation in general , and partly on one or several genes , the activity of which plays a role for the localization of the cancer to the leukon ; leukaemia seems to constitute an entity genetically and environmental changes influence the type of the disease . there is evidence that extemal factors also ' play a role in the development of leukaemia . 
of several cases of leukaemia in the same family is rather slight ; but the risk of getting cancer in near relatives of a patient with leukaemia is as high as almost 50 per cent . table iii shows some of the data from the breast cancer and leuka6mia material in relation to cancer risk . 
among the relatives of probands with cancer of the body of the uterus the incidence of " endogenous cancer " was high , and the relatives of probands with cancer of the cervix show the same frequency as the relations in the families of the patients with cancor of the cervix , of control probands . on the other hand , a relatively increased frequency of cancer of the oesophagus in this connection it is worth while to draw attention to the simiwas present . larity of the histological structure of cancer of the cervix and cancer of the in the families of probands suffering from cancer of the oesophagus oesophagus . investigated by mogensen ( unpublished data ) , cancer of the oesophagus was often found in a close male relative , the father or a brother of the proband . in these families , both the proband and the relative with cancer of the oesophagus 148 t . 
the differences could , however , not be significantly proved , owing to the insufficiency of the material , and the differences may be due to the fact that - the old propositi generally have less detailed and exact information about their relatives in earlier generations than the young propositi have . still the accordance of the experimental results and the clinical observations makes the significance of the latter probable . our investigations into the heredity of various aspects of cancer , have show - n that hereditary disposition is an important tumour - causing factor . it was found that it is the chief factor in the development of breast cancer , and many other tumours are more or less dependent on hereditary factors . 
the general cancer - tendency " ( likely not a general blastoma tendency ) occurs with considerable frequency in the population ( it is probablv higher than 20 per cent ) , and is possibly inherited as a character showing incomplete dominance . 
our investigations have shown that the tendency of tumour - localization has also a hereditary basis . the development of leu ' kaemia and cancer is probably due to a common hereditary . 
koller. from the chester beatty research institute , the royal cancer hospital , london . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . xeroderma pigmentosum ( hence referred to as x.p. ) , is marked by rougheniing , dryness , pigmentation and ulceration of the skthe condition is attributed to hypersensitivity of the skin , particularly that of the basal cell layer , to sunlight . the disease was first described adequately by kaposi in 1874 ( hebra and kaposi , 1874 )  . 
occurs in the first year of life , often within a few , months after birth . first , erythema develops on the skin , on those regions which are exposed to light , followed by freckling and frequently by telangiectasis . from these regions epithelioma or basal - cell carcinoma develops . 
the malignant change may take place not only in the skin , but also in the cornea and conjunctiva the genetical and chromosomal basis of x.p. the hereditary basis of x.p. 
was first investigated by siemens and kohn ( 1925 )  . they analysed 76 families , and cockayne ( 1933 ) brought this more up - to - date with a further 43 family histories . in both groups of data the incidence of consanguineous marriages was very high : 24 out of 76 and 16 out of 43 respectively , were first - cousin marriages . 
i. received for publication january 4 , 1951 . recent work has provided evidence in favour of the supposition that tumours contain , and therefore probably release into circulation , a substance capable of depressing liver catalase activity . 
nakahara and fukuoka ( 1949 ) claimed to have produced a liver catalase depr ' ession in mice after the injection of alcoholprecipitated fractions obtained from human tumours . similar fractions from normal tissue were stated to be inactive . 
adams ( 1950a ) commenced a study of the effect of the injection of homogenized mouse tumours into mice , and showed that after an early ( 24 and 48 hours ) depression , the hver catalase level returned to normal approximately 4 days after injection , and fer once more as the new tumour grew . 
the results were interpreted as indicating that the initial depression is due to some substance or substances present in the , injected material , the second depression only being due to the new tumour . injection of homogenized normal tissues had no effect on catalase level . appleman , skavinski and stein ( i950 ) , in the course of an investigation of the variations in erythrocyte , kidney , and liver catalase activity in rats bearing the jensen sarcoma or the u.c.l.a. 
fibrosarcoma , found that normal rats kept on a protein - free diet showed a drop in liver catalase activity to approximately 50 per cent of normal within 7 to 10 days from the time thev were placed on the diet and this low level wa - s maintained for 53 davs or longer . 
the variatioils in liver catalase level following the subcutaneous injection of coarse suspensions of these tumours into albino mice results in both males and females were similar to those preappear in table 1 . viously obtained with s37 and carcinoma 63 . 
adams two general methods have been employed : the first involved the injection of s37 sarcoma , which had been treated so as to render it incapable of giving rise to tumour growth , and the second , the results of which are presented in the next section , the injection of pure line mouse tumours which do not grow in the strains of mice used . sarcoma 37 tissue was disintegrated by shaking for several minutes with glass beads in a " mickle " tissue disintegrator , made by messrs . 
is a plot of the subsequent variation in hver catalase level over a cers . period of 10 days , the crosses representing the arithmetic mean values of the groups . in the experiment represented iin the left - hand graph the tissue was disintegrated in normal saline ( ph 6 - 8 ) , and it wir be seen that a 24 - and 48 - hour depression was obtained , the level rising to normal at 4 days and remaining so at 7 and 10 days . however , this treatment was not completely succe 'ssful in pre ' venting tumour growth , in spite of failure to discover intact cells in the homogenate microscopicary . 
the experiment was repeated , using m / 100 citric acid as the suspending fluid ( ph 5 - 5 ) , and the results appear in the righthand graph . 
the catalase depressing effect is very similar , but in this case no tumours appeared in 18 mice kept for 3 months , when the experiment was terminated . a second method involved the partial centrifugation of a fine homogenate ofs37 tissue in normal saline , prepared originall with a tenbroeck grinder . 
n. abscissa : time in days . effect of in ' jection of tumours which do not grow in the 8train of mice u8ed . a number of pure line mouse tumours which do not grow , at any rate after the in ection of coarse homogenates , in the stock albinos used , were injected subcutaneously or intraperitoneally in 100 mg . 
the results appear in table il in every case a significant depression in catalase activity was observed 48 hours subsequently , with a return to normal by the 4th to 7th day . in one experiment of this series , not recorded in table 11 , a different result was obtained . 
the catalase level at 48 hours was very low , and remained low at 4 days ; at 10 days , of th - e 6 remaining mice , 3 in which the abscesses were healed had high levels and 3 120 d . 
the results are given in table il no significant variations in catalase level were observed , and with the rat tumours in particular the variations appear to be completely random . ..cb - r = 1 l -  . 
the points lie on a slightly curved line , showing a progressive deorease of catalase activity with dose . the depression is seen to be approximatelv proportional to dosage over the range 10 to 30 per cent . 
4. - liver catalase levels 48 hours after the intraperitoneal injection of varying quantities of coarse homogenate of sarcoma 37 into stock albino male mice . ordinate : catalase level in arbitrary units / mg . 
adams it is not claimed , however , that nutritive effects play no part in producing the depression of catalase activity , particiilarlv in animals bearing large tumours . miller ( 1950 ) has recently shown that although catalase level in animals which are maintained on low or non - protein diets parallels approximately the level of total liver protein , the enzyme soon begins to disappear more rapidly than the consequently , even if the only relevant effect of a large remaining protein . tumour on the nutritional status of an animal were a simple depletion of protein , however , the depression which occurs in a depression of catalase would result . the early stages of tumour growth may be expected to be due mainly to toxic material produced by the tumour , since the importance of purely nutritive factors , e.g. , protein depletion , must be small at this stage , though becoming progressively greater as the tumour size increases . 
the effectof large tumours on catalase is probably the resultant of separate nutritive and toxic actions , which could not be readilv distin uished . the effect of injecting infected c57 sarcoma is quoted as a possible source of error in investigations of this nature . it is not yet known whether catalase depression is a common result of bacterial infections , but this possibility must be reckoned with when using , for example , human intestinal tumours , which are greenstein ( 1947 ) states that infection of mice with certain often infected . strains of poliomyehtis virus , or with streptococci and staphylococei , has no . however , it has been observed in this laboratory effect on catalase activity . during epidemics of a sabnonella infection , and of ectromelia , that catalase level was low when the liver showed signs of involvement . 
dounce and shanewise ( 1950 ) i - lave recently shown that catalase activity is significantly depressed in rats suffering from advanced murine leprosy . apart from these isolated observaticjns , no detailed investigation has beeii made of the effect on liver catalase of infections of the liver , or of injections of infected normal or malignant tissue . although a depression of liver catalase may occur in conditions other than cancer , this does not detract from the importance of the effect as a property of maligiriant but not of nornial tissue , and work on the mechanisbv which the toxic substance exerts its effect may thrcw light on some fundamental difference recently reports of prehminary experibetweennormal and malignant tissue . ments have appeared , indicating the importance of hormones in maintaining a normal level of liver catalase ( begg and reynolds , 1950 ; adams , 1950b )  . present investigation is being follo - vved up by an endeavour to relate the tumourdepressing effect with the hormonal control mechanism . depression of liver catalase activity b - as been shown to follow the injection into mice of mouse tumours , but not of rat and human tumours in single doses of up to 100 mg . 
nakahara and fukuoka ( 1949 ) , on the other hand , observed a depression after the injection of alcohol - precipitated fractions of human tumours however , their dosage , referred to weight of original tissue , was into mice . probably very much bigher than that used here . all that is now claimed is that injection , in the dose used , of mouse tumours into mice produces a considerable depression of liver catalase , while injection of similar doses of tumours of other species produces no apparent change . 
the early variation in injection . females was not significant in one case . ( 2 ) injection into stock albino mice of sarcoma 37 tissue ( a ) disintegrated in m / 100 citric acid , or ( b ) partly centrifuged after coarse homogenization in 70 mg . 
doses , resulted in a depression of liver catalase without any obseirvable tumour growth . ( 3 ) six pure line mouse tumours , which do not grow in the stock mice used , also gave catalase depressions 48 hours after injection in 100 - mg . 
fibroid with advanced sclerosis ; patch of oedematous tissue ' probably smooth muscle fibres ; proliferation of vascular endothelium ; invasion diahypertrophic endophragm ; thelium on the surface of the tumour . . 
the peripheral belt of fibroblasts originating most probably from subendothelial cells of the serosa and so characteristic of the oestrogeninduced abdominal fibroid ( lipschutz , 1942 ) was present in a diaphragmatic tumour belonging to the animal of fig . 
as with the abdominal fibroids we have described formerly , there were in thoracic tumours also some cells resembling there was a proliferation of the cells of the wall of vascular smooth muscle fibres . spaces ; there was an hypertrophy of the endothelium at some places on the there was invasion of the muscular tissue of the diasurface of the tumour . phragm , or the thoracic wall , by the tumours . 
but there were in this tumour also accumulations of cells resembling fibroblasts which seemed to originate from the proliferation of the subendothelial cells of the wall of vascular spaces , or the endothelium proper . 
the tumour was covered by various layers of flattened cells . there were besides the animals described , 4 females and 2 males in which small nodules just visible to the naked eye were found on the surface of the only 2 animals of this group have been examined lung or on the parietal pleura . microscopically ( table i ) and in one of these a tiny fibrous nodule was found on the surface of the lung ; the structure of this nodule was identical with that of similar oestrogen - induced nodules of the abdominal serosa . 
note thickened border of opening in the diaphragm , prolapsed liver and intestine . fibrous reaction also on the right though the opening is on the left . small nodules on the pericardium in lxiii . 
the tablet occupied in some cases a retrosternal or mediastinal position ; it was surrounded by a thin capsule and in other cases the capsule adhered to the costal serosa , thin fibrous strands . where the fibrous reaction around the oestradiol tablet was more conspicuous . but there was not a single animal with thoracic tumours in this group . 
lipschutz oestrogen - induced thoracic fibroids increased very considerably ; thoracic fibroids in 7 out of 18 animals with such a communication . there were in most of these animals part of the liver and of the intestine prolapsed to but the mechanical stimulus due to this accident was the thoracic cavity . seemingly not responsible for the increase of the incidence of oestrogen - induced this was shown by the fact that in 24 animals without an thoracic fibroids . abdominal - thoracic communication the capsule enveloping a foreign body introduced in the thoracic cavity ( metallic tablet or a tablet of oc - oestradiol ) did not , or only exceptionally , become surrounded , under the influence of the oestrogen , by a fibroid as was the case with a similar foreign body ( metallic tablet ) introduced in the abdominal cavity of these animals . the above experimental results suggest that the oestrogen - induced fibrous tumoral reaction of the peritoneum in the guinea - pig is mediated by an internal ambiental factor normally present in the abdominal serosal fluid , or a factor originating under the influence of the oestrogen and given up to the abdominal it is seemingly the absence of this mediating factor which protects the cavity . animals against production of fibroids in the thoracic cavity . aided by grants from the the jane coffin childs memorial fund for medical research . 
harris , coal tar research association , who had purified it by chromatography and checked it by ultra - violet spectroscopy for impurities . these were below the level of detection . fluorewene mea8urement& the fluorescence values for solutions of the various hydrocarbons were determined by constructing curves using a hilger " spekker " photoelectric fluorimeter with cers of capacity approximately 11 ml . , and with filter chance 0 x 7 348 d . 
mouse protein after 6 days ' benzpyrene treatment appear to be of the same order as that recovered by mller ( 1951 ) although it is not possible to assess gravimetricallv the data given by this worker since her figures are relative and apply to the instrument and filters employed . berenblum and schoental ( 1942 ) found that 24 hours after one intraperitoneal injection of 10 mg . 
woodhouse benzpyrene was added to denatured , fat - free , normal skin - protein and refluxed with alkah , toluene and zinc , it could be completely and quantitatively removed from the alkahne solution by benzene extraction . 
the extra - cellular bound ilydrocarbon might consist of metabohtes " excreted " from the cells - or it might be derived from dead or damaged cells . although the fluorescence technique was not sufficiently sensitive for accurate estimations with the small amounts of protein available , the occurence of bound hydrocarbon in cellular constituents has been confirmed by extracting the dna and rna skin proteins from a batch of benzpyrene - treated mice . 
of " fixed " benzpyrene was extracted and a trace was found in the dna protein sample which , however , weighed only 2 mg . a corroborative experiment was also carried out based on the observations of calcutt aind payne ( 1953 ) who showed that nuclei and mitochondria isolated from the livers of mice which had been given a single intraperitoneal injection of benzpyrene in finely dispersed eiuspension , contained fluorescent hydrocarbon 2 hours to 21 weeks after the injection . 
the believed , therefore , that benzpvrene injected in this way is rapidly transported to the mitochondria and nuclei and is held there in an unchanged state for prolonged periods . 
they did not examine the effect of alkahne hydrolysis on alcohol - extracted nuclei . the experiment was repeated in this laboratory but the prelinu ' nary extractions were made as described previously for the skin tissues and continued with alkaline hydrolysis . 
a small amount of fluorescent material was extracted from the hydrolysate but nuclei froni control mice did not yield comparable fluorescent extracts at any stage . this experiment showed that at least a portion of the benzpyrene can be it was repeated , therefore , employing fixed in vivo by nuclear components . perylene , and , after alkaline hvdrolysis an extract with fluorescence characteristic of perylene was obtained from the separated , alcohol - treated nuclei . 
the free hydrocarbon was thoroughly removed and the " bound hydrocarbon " was extracted after hydrolysing the protein with koh and measured fluorimetrically . although these species of animals vary considerably in their response to this hydrocarbon as a carcinogenic agent the amounts of bound hydrocarbon obtained from 25 mg . 
samples of extracted and dried tissue were very similar in all instances . other polycyclic hydrocarbons which are less carcinogenic to mice , e.g. , 2 ' 6 - dimethyl - benzanthracene , and perylene which is non - carcinogenic , have also been tested , and in all instances comparable amounts of bound hydrocarbon could be extracted from the alkahne bydrolysate . using similar extraction techniques a smar amount of fluorescent , bound hydrocarbon could be removed from the nuclei isolated from hvers of mice 24 hours after a single intraperitoneal injection of either 3 4 - benzpyrene or perylene . it is concluded that further evidence is needed to substantiate the view that 352 d . 
whitfield jarcho ( i936 ) also states : has often biased the clinician in favour of a purely haematological diagnosis . despite the frequent difficulties in chnical diagnosis the primary growth and / or its metastases were always readily visible at autopsy . jarcho ( 1936 ) stated that many patients dying from mahgnant thrombocytopenic purpura also showed lymphangitic carcinomatosis of the lungs althou - ah histological examination was often necessary to demonstrate its presence . 
he adopted the term " diffusely infiltrating carcinoma " to cover both mahgnant purpura and lymphangitic carcinomatosis of the lungs , suggesting that they were manifestations of the same disease process . 
on boxing day , 1952 , she noticed profuse painless haematuria which lasted for 19 days . investigation showed no casts in the urine , a normal blood urea and normal intravenous and retrograde pyelograms . 
the urine contained a few red cells , polymorphs and cohform bacilli . hess 's test was negative , the bleeding and clotting times were normal and the prothrombin was 100 per cent . there were 2 , 180 , 000 red cells , 46 per cent haemo lobin , 5 , 000 white cells and a again there was normal differential count . 
no cause for the purpura had been found during life . po - st - mortem finding8 . there were many skin ecchymoses over the legs , thighs and arms , some of which extended deeply into the underlying tissues . there were petechial haemorrhages on the posterior third of the tongue and soft palate . 
the left breast and axilla were normal . the pleural surfaces of the lung8 were normal . their cut surfaces were unusually bloodless , firm in texture and grey in colour . these gross appearances suggested diffuse pulmonary fibrosis . there was no evidence of carcinomatous infiltration . 
the hilar lymph node8 were enlarged and firm and their cut surfaces in view of the previous history showed several tiny grey homogeneous areas . of breast carcinoma a frozen section was prepared from one of these glands . it showed secondary polyhedral - celled carcinoma consistent with a primary origin in the breast . these nodes were not adherent to the hilar blood vessels which were normal in all respects . 
two similar para - tracheal lymph nodes were found i cinferior to the thyroid gland . the upper 12 cof both femoral shafts contained pink marrow which sank in water and which on close inspection was flecked with several pale homogeneous foci measuriaig 1 - 2 min diameter . there was absorption ofthe bony trabeculae . a smear prepared from this marrow showed irregular clumps of malignant cells . the rest of the marrow was fatty . immediately inferior to the left lesser trochanter was a smooth walled cyst 2 x i cdiameter . 
the femoral marrow would have been accepted as showing hyperplasia and a simple cyst resulting from previous haemorrhage if carcinomatous deposits in the pulmonary lymph nodes had not been confirmed histologically earlier in the course of the autopsy . the 8ternum showed hyperplasia of red marrow and absorption of tlle bony trabeculae . the brain showed symmetrical swelling of both frontal lobes and bilateral sectioning revealed extensive tentorial hemiations . iiitracerebral haemorrhages involving the white matter dorsal ancl anterior to the genu of the bilateral 100 w . 
whitfield corpus callosuthe haemorrhages extended backwards on both sides as far as the post - central gyrus , becoming continuous at this level by involvement of the body of the corpus callosuboth lateral ventricles contained recent bloodclot . 
the basal gangha , brain - stem , cerebellum , venous sinuses and pituitary showed no macroseopical changes apart from occasional petechial haemorrhages . the vessels of the circle of wilhs and their major branches showed no evidence of embolism or thrombosis . the thyroid was small , hard , had an irregularly scarred outer surface and showed several brownish areas - each 1 - 2 min diameter - on its cut surface . these areas resembled old areas of haemorrhage . 
the gall bladder was normal . several para - aortic lymph nodes felt firm , their cut surfaces were a uniform pinkish - grey colour and were devoid of definite metastatic deposits . the pericardium , heart , skmmch , intestines , spleen , pancreas , suprarenals , urinary bladder , fallopian tubes and ovaries all appeared normal macroscopically . the uterus contained several small intra - mural fibroids . although there had been histological confirmation of secondary deposits in the pulmonary lymph nodes and bone - marrow during the autopsy , it should be emphasised that there was no other definite evidence of gross metastases , despite extensive examination of all viscera . 
the axillary lymph nodes were extensively infiltrated with similar carcinoma . ( 2 ) tissues taken at autopsy . - the pulmonary and right axillary lymph nodes and femoral marrow contained microscopical metastases which resembled the primary tumour morphologically . the abdominal lymph nodes , thyroid and posterior lobe of pituitary showed scanty microscopical metastases nevertheless still identifiable with the primary growth . 
the above tissues also showed intra - vascular carcinomatous einboli , which had not effected extra - vasc - ular extension . all other post - mortem material examined showed numerous intra - vascular , micro - emboli composed of compact clumps of polyhedral carcinoma cells devoid of stroma . 
the cells were cytologically identical with those which constituted the primary tumour , but because of the minute size of the emboli the general pattem of the primary was lacking . 
the renal tubules contained red blood cells or occasional clumps of tumour cells - " tumour casts . " intracapillary carcinoma plugs were seen in the dermi8and8ub - cutaneousfat in sections prepared from areas of skin ecchymoses . 
the post - operative history of the case may be explained in two ways . either ( 1 ) viable carcinoma cells survived in unextirpated glands or other sites of pre - operative metastasis during the major part of the long period of apparent surgical cure , and only later - perhaps related in time to the onset of purpura 6 months before deathgained access to the general circulation by venous invasion , or ( 2 ) a degree of intra - vascular dissemination was also present since the original operation , but for 71 years had not resu - ited in manifest embolic phenomena . 
the lung was the main exception to this statewidespread intra - vascular deposits , in places apparently resulting in ment . complete occlusion , had not given r ' ise to obvious symptoms or signs during life , even though cardio - respiratory manifestations arising on this basis are well recognised ( jarcho 1936 , storstein 1951 )  . neither did the lung show histological evidence of embolic phenomena . carcinoma cells had undoubtedly passed through the pulmonary vascular bed and into the systemic circulation without interruption or the formation of metastases . thik ; is a rare phenomenon and is discussed in detail by wilhs ( i 952 , page 45 )  . 
the experimental evidence of zeidman and buss ( i952 ) suggests that the transpulmonary passage of tumour emboli may occur more commonly than was previously supposed . the reason for the absence of the usual type of gross metastases in this patient is unknown . 
the fact that all organs examined showed tumour emboli , often in large numbers , does not support the view of coman ( 1953 ) that the distribution of metastases i 's dependant upon the number of embohc cells reaching the various factors other than the frequency - distribution of tumour cells appear to organs . have played a part in our case . 
the ancestral neoplastic cells constituting the primary growth clearly possessed infiltrative propensities . unless the intra - vascular descendants of these cehs had lost these inherent aggressive characteristics - and the presence of mitoses , lack of degenerative changes and the scanty but nevertheless definite microscopical foci of extravascular infiltration that were found does not support this view - one is left to assume that the unusual behaviour of this neoplasm resulted from a lack of the host stromal response which is such an essential factor in successful metastasisation . 
the possibility that " stroma - inducing " properties of the tumour cells were lacking , cannot of course be excluded by histological criteria . it is repolted ( willis , 1952 , page 272 ) that carcinoma of the breast produces intra - thyroid metastases in about 20 per cent of cases . it has also been show - n ( wilhs , 1931b ) that pre - existing abnormahties in the gland were prominent in these findings favour the cases of carcinoma showing intra - thyroid deposits . view that the associated chronic non - specific thyroiditis in our case , preceded the secondary deposits . in a recent paper describing four cases of sub - acute cerebellar degeneration occurring in association with carcinoma elsewhere in the body , brain , daniel and greenfield ( 1951 ) recorded non - specific thyroid changes in one of their patients , similar to those found in our patient . 
the status of the thyroid gland in carcinomatosis seems to merit further investigation . it will depend upon the results of such studies as to whether relationship can be seen between the thyroid changes and the unusual features of our case . the presenting symptoms of haematuria and skin purpura were related to the presence of tumour emboli in the skin and glomerular capillaries . 
haematological investigations during the life failed to elucidate any other aetiological vascular changes in the skin in malignant disease have recently been factors . described ( forman 1952 ) and may have contributed to the skin lesions shown by our p ' atient . the terminal acute massive cerebral haemorrhage may have resulted from the rupture of a small degenerative blood vessel traversing a pre - haemorrhagic focus of softening , a mechanism postulated by globus ( 1937 ) and further substantiated by globus and epstein ( 1953 )  . 
the presence of embohc phenomena elsewhere in the body , the unusual distribution of the effused blood , and the absence of cerebro - vascular disease excluded the possibility that this wa - s a coincident haemorrhage of the classical spontaneous variety . 
madow and alpers ( 1952 ) have described a case of cerebral softening due to multiple cerebral carcinomatous emboli , the primary tumour being a squamous carcinoma of bronchus . as in our case there were no macroseopical cerebral deposits but other visceral metastases were however abundant . 
the above authors also refer to three previously recorded cases of cerebral softening resulting from blood - bome cerebral lesions due to massive neoplastic embohsm carcinomatous emboli . are reviewed by till and fairbum ( 1947 )  . 
the petechial haemorrhages , microscopical softeiiings and focal demylination in the cerebral white matter of our patient resembled experimental lesions produced by the injection of calibrated paraffin emboli ( swank and hain , 1952 ) and sterile cod - liver oil ( lumsden , 1950 ) into the cerebral circulation . cerebellar degeneration ( brain et al . , 1951 ) and peripheral neuritis ( dennybrown , 1948 ) occurring in association with carcinoma elsewhere in the body have been described . 
the changes in the cerebellum and peripheral nerves of our case bear only a superficial resemblance to the lesions described in the above reports as they were focal , associated with carcinomatous emboli and did not include systematised tract degeneration as furthermore , in our case - apart from the terminal far as we could ascertain . apoplexy - the neurological lesions gave rise to no definite symptoms or signs . the platelet thrombosis syndrome ( " thrombotic microangiopathic haemolytic anaemia " ) has recently been reviewed by symmers ( 1952 ) , who states that this condition was first described by moschowitz ( 1924 )  . 
the neurohistological lesions in this syndrome were described by adams , cammermeyer and fitzgerald ( 1948 ) and are easily differentiated from those noted in our case by the presence of platelet thrombi , endothelial and probably adventitial hyperplasia in the walls of the involved vessels and less severe damage to the neural thrombocytopenia is usually present both in previously recorded cases tissue . of malignant purpura and in the platelet thrombosis syndrome . 
at autopsy gross metastases were not present and yet histology revealed intravascular carcinoma in the liver , lungs , one suprarenal , lymph nodes , bone - marrow and dura - mater . 
the degree of intra - vascular spread noted both in oertel 's and our own cases leads us to suggest that a search for carcinoma cells in marrow , skin or muscle biopsies and perhaps in urine , sputum or even blood specimens may be of diagnostic value in suspected cases of intra - vascular carcinomatosis either associated with an occult primary growth or occurring after radical excision such investigations may also help in differentiating the of a known primary . condition from the platelet thrombosis syndrome . 
we feel that even though features such as thrombocytopenia were present , tumour emboli may have been a factor in the mechanism of the purpura in these cases . the evidence that we have presented shows that our patient finauy died from the mechanical effects of tumour emboli that had not resulted in macroscopical metastases , and also that carcinoma cers may have existed " commensary " i the blood stream for many years . 
the patient died from massive intracerebral detailed histological examination estabhshed that the purpura haemorrhage . it is suggested that resulted from the effects of blood - bome carcinoma emboli . carcinoma cells may have existed in the blood stream since the original operation and that similar embohsation may also play some part in the mechanism of malignant purpura . 
the clinical picture of this case is compared with that of the platelet thrombosis syndrome . neurological lesions were present and are discussed in relation to previously recorded cases that show points of similarity . we wish to express our gratitude to professor w . 
gagliano. from the cancer research institute and the department of medicine , college of physicians and surgeons , columbia university , new york . received for publication january 30 , 1950 . tetra - sodium mitchell ( 1948 ) recently reported a clinical study on the use of parenterally administered 2 - methyl - i : 4 - naphthohydroquinone diphosphate ( synkayvite ) as an adjuvant to radiotherapy in the management of inoperable and far advanced malignant disease . in a small series he noted prolongation of the mean survival time of patients with inoperable carcinoma of the bronchus treated by the combination of chemical agent and irradiation when compared with that of patients who received x - ray therapy alone , which he found to be statistically significant . the rationale for mitchell 's ( 1948 ) selection of this drug for clinical trial in combination with radiotherapy depended upon his observation that the chemical compound produced mitotic inhibition of chick fibroblasts in tissue culture . although there have been many laboratory studies on synkayvite as a vitamin k substitute , no investigations have been published on the effect of this compound on experimental neoplasms . 
the growth of the tumours in control and treated animals was followed by serial mensuration of the outside diameters , but the conclusions reached in this study rest on the comparison of the wet weight of the tumours in the control and treated series determined at the 104 a . 
from the information included it is possible to estimate with accuracy the actual protocols for the individual experiments , even though the pertinent results are here summarized as averages ; the standard deviation has been calculated in each instance in order to describe the range and the distribution of the individual tumour weights about the mean tumour weight . 
the standard deviation of the mean which is necessary for the determination of statistical significance between two means is derived by dividing the standard deviation by the square root of the number of observations . in several of the experiments 5 - amino - 7 - hydroxy - 1 - h - v - triazolo [ d ] pyrimidine ( 8 - azaguanine ) was also administered to tumour - bearing animals for purposes of comparison with synkayvite . 
gagliano neoplastic disease and malignant tumours in experimental animals is an unsettled issue , it is important to note that , thus far , all of the chemotherapeutic agents which have a demonstrable palliative effect against neoplasms in man have also been shown to inhibit comparable tumours in laboratory animals . it is also appreciated that the observations which we have recorded do not duplicate in the laboratory the clinical experiments of mitchell ( 1948 ) , inasmuch as he studied the combination of radiotherapy and the drug whereas - we investigated the drug alone . evaluation of combination therapy , however , utilizing radiant energy plus a chemical compound , is not feasible in studies on experimental neoplasms due to the ease with which x rays alone can destroy subcutaneous tumours . therefore , in spite of negative experimental evidence of the type presented in this report , the possibility remains that synkayvitein combination with radiotherapy may produce a greater carcinolytic effect than x - ray therapy alone . 
the presence of the agent in mammary tumour cells after 42 transplantations in c57 black low - cancer - strain mice cbaracterised by low susceptibility to mammary cancer and lack of the agent again raised the question what part is played by the mammary tumour inducing agent im the propagation of the transplanted breast tumour cells , and whether bho cells will continue to multiply in the same way should the agent disappear from the bittner , evans and green ( 1945 ) reported the presence of the agent after cells . 10 serial passages of high - cancer - strain tumour cells in ag - ent - free but susceptible mice , and concluded that the agent is continuously produced in the transplanted tumour cells . in an attempt to ascertain whether the presence of the agent is a permanent feature of the transplanted cells , the c57 x transplantable mammary tumour was again tested for the presence of the agent after 86 serial transplant 's in c57 black low - cancer - strain mice . 
the method of preparation of the tissue for testing and the test itself were the same as those employed for the 42nd transplant of the tumour in whicb the agent was found to be present . 
 ' they succeeded in the recovery of small amounts of papilloma v ' irus from the first and second transplant of carcinoma cells in now - bom rabbits , but failed to recover the virus from tumours of the third and fourth passage . 
the same authors reported positive neutralisation and complement - fixation test - s between papiroma vi ' lrug iand sera of adult rabbits in which a carcinoma originally derived from a v ' irus papilloma was transplanted for 22 the 46th and 50th tumour transsuccessive passages . plants failed to give a positi - ve compl - e ' ment - fixation test . 
they concluded that the " virus was - no longer present in the attempts tumour , although the morphology of - the tumour , remained unaltered . to reinfect the tumours by placing them in a v ' l ' r - us s - aspension or mjecting papiltransplants of the carcinoma loma virus int - ravenously into rabbits be - ar ' m ' yielded dubious results . serological tests m mice similar to those carried out in rabbits by smith , kidd ancl rous ( 1947 ) in order to ascertain the . 
presence of a lat - ent or masked mammary tumour induc ' mg agent in cells of the , 86th transplant could not be of any help in this respect . 
no atte - mpts were made to test the nells of the 86th transplant c57 xmanimar tumou ' r by grafting the tumour tisgue into susceptible mice in view of , the previous observations by various authors . 
thus transplantation of mammary tumour tissue with the agent into susceptible mice has either failed to transfer the agent ( andervont , 1949 ) , or has induced only a low incidence of tumours ( humniel and little , 1949 )  . it has also been found to be a poor source of the a ' gent ( barnum , ball and bittner , 1947 )  . it was therefore considered an unsatisfactory method for testing the transplantreinfection of the tumour able c57 x tumour for the presence of the agent . tissue wit - h the mammary tumour agent was not carried out because of the observations of smith , kidd and rous ( 1947 ) , although it is quite posgible that it would in connection with the negative result obtained have yielded unequivocal results . with the 86th transplant , another test for the presence of the agent in cells of the so far no tumours have been observed 101st tumour transplant was carried out . in an of the test mice , but it is too early to draw a conclusion , as all the mice bittner ( 1952 , personal comare still alive , havi ' n ' g lived now for 11 months . munication ) has found the agent present in the 15th transplant of a c3h mammary tumour in agent - free cm mice , while in t - he cells , of the 7th transplant , of the same tumour it was apparently difficult to detect . it is not known whether a similar situation may arise with the c57 x transplant ' able mammary tumour , although the agent could not be detected in the 86th s ' en ' al passage by the same means which revealed its presence in the 42nd transplant . 
the agent or bittner virus , as it is described by some authors , may have been altered in some unknown way , possibly by mutation . it may have become closely associated with one of the particulate this close integration of the agent with the tumour elements of the tumour cells . cers may have produced a state in which it was unable to survive the death of the tumour cells during extraction procedures preparatory to the test . 
in giemsa preparations feulgen staining was the membrane appeared as a faintly stained pink line . completely ineffective , whilst after iron haematoxylin the membrane lost its stain early in the decolorising process . 
the mercuric bromphenol blue staining technique of mazia , brewer and alfert ( 1953 ) was tried and found to stain the membrane feebly . this method , however , proved useful for determining the relationship of the membrane to the spindle structure . examinat - ion of a large number of preparations has allowed the following description to be pieced together : 1 . 
telopha8e. - as the cytoplasm constricts to form two daughter cells , the membrane also constricts and finally , after fusion at the centre , separates into two complete membranes - - one to each daughter cell . 
7. examination of fresh smears of the tumour by phase contrast microscopy demonstrates the occurrence of this membrane within the living cell and dispels ' any possibility of its origin being that of a fixation artefact . 
the membrane , under these conditions , appears as a thin clear zone form ' mg a sharp line of demarcation between the karyoplasm and the cytoplasm . because of the overlying cytoplasm it is difficult to focus and photograph . in this particular tumour mitosis within a persistent membrane appears to be the standard type of division . 
3. other than that it was taken from a section of a hepatic metastasis of a carcinoma of the tonsil no further comment or information is it appears then that the phenomenon as described is not a completely given . isolated case but does occur occasionally in other material , but not with the regularity shown in this instance . it would not appear to be a fixation ar - tefact since it can be determined by phase contrast microscopy in living cells . further , the fact that such a wide variety of fixatives will preserve it is against such a view . 
on the basis of the evidence available it seems unhkely that such an event has taken place , and if so , takes no cogmsance of the fact that similar appearances do occur irregularly in other tumours . although no evidence can be adduced to show that this membrane arises de novo within each dividing cell it is possible to offer a fairly plausible explanation it has been demonstrated by chambers and of its appearance in this fashion . ludford ( 1932 ) that the cytoplasm of malignant cells has a ph value lying between 6 - 4 and 7 - 0 whilst the intranuclear ph is in excess of 7 - 2 . 
under such conditions a gradient of ph would occur . it is suggested that at some point on this gradi ' ent the isoelectric point of neighbouring cytoplasmic structural protein is reached . this would involve the localised precipitation of protein and the ensuing membrane appearance . if such an event does occur it suggests that intracytoplasmic disturbance during mitosis is minimal , otherwise one would expect distortion and breakage of the membrane . a mechanism of origin as suggested above would account for the isolated examples of similar appearances in other tumours . 
thus , administration of the milk factor from two different highbreast - cancer strains to the same susceptible hybrid mice , kept under controlled conditions , has shown differences in either quantity and / or quality of the factor present in these two high - breast - cancer strains . l , dmocrowski bittner and huseby ( 1946 ) reported similar findings by a different experimental procedure ,  . 
namely , by reciprocal crossings of two high - breast - cancer strains ( c3h and strong a ) , and by recording the tumour incidence and tumour age in virgin hybrids obtained from these strains . 
they described the recorded d ' ifferences in the tumour incidence and in the tumour age in these hybrids as a result of different concentration and / or activity of the milk factor present in these heston and andervont ( 1944 ) in a similarly two high - breast - cancer strains . conducted experiment on sublines of the same strains found no conclusive andervont and eviden ' ce of a difference in the milk factor of these strains . mceleney ( 1941 ) pointed out , however , that his high - breast - cancer strain - ( c3h ) must be regarded as a separate line , and the results obtained with it cannot be controlled by data procured from other lines of this strawamer , reinhard and goltz ( 1945 ) in experiments on virgin hybrids of two other high - breastcancer strains ( m and a ) obtained similar results ' and concluded that the milk factor was more concentrated in one of these stra ' ms than in the other . bittner and huseby ( 1946 ) found , however , the same incidence of breast cancer in breeding hybrids of the two strains tested . 
but they rightly pointed out that the ultimate result of the changes in the structure of breast tissue acted upon by the milk factor of another strain is determined also by the genetic constitution and responsiveness of the breast tissue to the particular milk factor . heston , deringer and andervont ( 1945 ) , b ' y employing susceptible hybrid mice obtained from high - breast - cancer strain mothers and low - breast - cancer strain fathers , and by backcrossing them to highand low - breast - cancer strain males , showed that differences in the milk factor were produced by differences in the genetic constitution of the mice from which the milk factor originated . 
3. as possible into three groups . mice of the first group , when 4r - 5 months old , received one subcutaneous injection of a distilled water suspension of dried riii breast tumour tissue corresponding to 0125 g . 
of fresh breast tumour tissue ; mice of the second group , when of the same age , received one subcutaneous injection ' of a distilled water suspension of dried 63 ca transplantable breast tumour tissue ( from a 428th transplant of the tumour obtained from the imperial cancer research fund ) corresponding to 0125 g . 
no tumours developed in any of the s low - breast - cancer strain females , whether injected with riii or 63 ca dried breast tumour tissue . in the fl generation of s strain females injected with 63 ca tissue and of the control females , no tumours were observed in any of the females , or in any of the males painted with oestrone . in the fl generation of s strain females injected with riii dried tumour tissue , 7 out of 16 females developed breast cancer , and 5 out of 15 males , which were painted , also developed breast tumours . in s x riii hybrid females obtained from daughters of s strain females injected with dried riii breast tumour tissue , 27 out of 32 females showed breast tumours , while s x riii hybrid males of the same origin , painted with oestrone , gave tumours in 10 out of 16 mice . 
observed by the method ' employed in the present experiment . it is impossible to state , however , whether the milk factor was originally absent in the primary tumour or whether it was lost during the course of so many transplantations . .in conclusion , it can be stated that only an analysis of the action and interaction of all know - n factors with allowance for other possible factors can make 102 l . 
murray. from the radiation therapy department , johannesburg general hospital , the non - european hospital , and the south african institute for medical research , johannesburg . received for publication january 10 , 1953 . skin cancer is relatively infrequent in the african . in the three - year period 1949 to 1951 , during which time 590 cases of malignant disease in africans were referred to the radiation therapy department , only 50 cases of skin cancer were encountered . 
the pigmented skin of the african would , of course , be largely protected from this effect , and indeed when skin cancer does make its appearance , it is almost invariably in areas exposed , not to sunlight , but to other types of chronic irritation . we have also observed distinct differences in pathogenesis , and the rate of growth and dissemination of skin tumours in the african , as compared with the m . 
murray classical description of the disease in europeans . these factors have compelled us to adopt a different approach to the management of skin tumours in the two races , and to revise our views on the surgical and radiological curability of skin cancers of various histopathological types . since these racial differences might be of some interest in the study of the demography , endemiology , and management of cancer in africa , it was considered worth while putting our experiences on record at this stage . the population from which this material is drawn consists of approximately 2 , 000 , 000 africans of the bantu race inhabiting the southern half of the transvaal , and originating for the most part from the sotho and zulu tribes . 
about onequarter of this population is urbanised and resident on the witwatersrand , but a much larger fraction of the hospital population gives an urban address . this is due , in part , to many rural patients living with relatives in the urban area prior to entering the hospital and witholding their true addresses , and also to the greater tendency among rural natives to receive treatment from indigenous herbalists in the absence of suitable vital statistics it is impossible rather than in hospitals . to state the age distribution of the bantu population , although it is safe to assume that the average age is somewhat lower than that of the european group . 
the ratio of males to females at the time of the 1946 census was 1 - 33 , the predominance of males presumably reflecting the migratory labouring class . from the genetic point of view it is important to bear in mind that the bantu inhabitants of south africa originate from central and east african tribes , who have , at least within historic memory , had no admixture of european blood . 
by comparison , the negro of the united states originates from west african ancestry and is largely a product of prolonged hybridisation . although environmental conditions in the southern states of the u.s.a. 
are not dissimilar to those encountered by the bantu in the transvaal , the two groups generally show a very different incidence and distribution of malignant disease ( higginson , 1951 ; and robinson , 1951 )  . 
the cells are arranged in the form of distorted , branching tubules or of alveolar masses . in some areas the cells are separated from the surrounding stroma by a well - defined basement membrane while in other areas the cells appear to infiltrate into the stroma . 
as the cells approach the lumen they become larger , the cytoplasm becomes faintly eosinophilio and sometimes vacuolated . the nucleus becomes smaller , more dense , and shows a well - defined nuclear membrane . the nucleus in these cells lies centrally , and their whole appearance is that of lipoid containing cells resembling those of the sebaceous glands . 
he was admitted from an outside hospital with a history of having had a tumour of the right upper arm excised 10 months previously , and that the lesion has subsequently recurred . there was a massive tumour present on the right upper arm and shoulder region , surrounding a vertical scar of the old excision . 
he became very ill , and was transferred home after further palliative x - ray therapy to the lumbar spine . the 2 cases of " sebaceous gland carcinoma " , although showing advanced disease , clearly illustrate the extreme radiosensitivity of these tumours , with conventional large field x - ray therapy . 
one patient is free from disease , while the second has extensive and incurable tumour . albinism and cancer of the skin . it is remarkable that there were 12 albinos among the 50 cases of skin cancer reviewed , although the albino trait is rare in the african . 
the exact incidence of albinism in the bantu is not known , but a cursory review of recent hospital records suggests that it cannot be greater than 1 in 5000 , and is possible less than consequently the 12 patients seen , representing the appearance of 1 in 10 , 000 . 4 new new cases annually ( and probably several more who do not attend hospital ) , implies that a large proportion , if not all of the albinos among the transvaal bantu necessarily develop skin cancer in early adult life . this observation is in agreement with the experimental findings of findlay ( 1928 ) , beard , boggess and von haam , ( 1936 ) and the recent precise quantitative investigations of blum ( 1950 ) , who have demonstrated that albino animals exposed to daily insolation or ultraviolet irradiation for a significant fraction of their life - spans invariably develop malignant skin tumours . all 12 patients showed complete albinism of the whole skin surface including the hair and eyes . 
we did not encounter any cases of partial albinism , such as those described by gelfand ( 1944 ) and shown to have the same propensity for skin cancer as the true albino . however , there was one case of xeroderma pigmentosum ( not included in table i ) occurring in a 4 - year - old bantu child in whom the whole skin surface showed the characteristic regular mottling caused by depigmented patches alternating with areas of increased pigmentation . 
murray pigment - free zones , especially those of the head and neck , possessed the characteristic hypersensitivity to light and were the origin of several histologically proved squamous carcinomas . there were 8 males and 4 females in the series . the age distribution of skin cancer in albinos shows a distinct tendency for the disease to occur in younger age - groups than in normally pigmented persons . there was 1 patient in the second decade , 3 in the third , 5 in the fourth and 3 in the fifth decade . 
we have not had the opportunity of observing the subsequent history of skin areas cleared of all macroscopic keratoses by podophyllin , and , in consequence , are not able to assert that the onset of skin cancer is , in fact , prevented . however , berenblum 's ( 1951 ) observations on the definite anticarcinogenic effect of podophyllin , even in the presence of actively carcinogenic hydrocarbons , suggests that this material may have a true prophylactic action . 
two to 3 weeks before admission black lumps appeared on the skin in the elbow region . on admission the patient had a typical malignant melanoma over the thenar eminence of the right hand . 
the primary growth and axillary glands were given 250 r daily to a total of 5500 r , other areas were treated with 1500 r and 1000 r daily to totals of 4000 r , 4500 r , and 6000 r , and six small areas were treated with three daily doses of 2000 r . all treated areas responded clinically by regression of the tumours and some necrosis of the tumour surface , but histological examination after the radiation showed minimal changes , a few lesions treated with 1000 r daily for 6 days disappeared completely . weeks after admission it was noted that the supraclavicular glands were enlarged and painful , but the intervening skin appeared normal . ten days later small black nodules were visible in this skin area . 
carr it is considered that the same proportion of the reproductive life of a - human female would bring her to 21 years of age , and that of a mouse to 41 moiiths , this emphasizes the very restricted nature of the sample usually studied . most of the data on spontaneous tumours comes from reports from poultry pathology laboratories , and is given as a percentage of all cases of deaths sent in for examination . this causes a serious under - estimate for several reasons for example , many of the deaths are due to s . 
pullorum and coccidial infections which strike the immature chick long before cancer age ; further , pathological investigations are usually only requested when a si - idden rise in mortality suggests an epizootic is beginning , while isolated deaths , which would include those due to cancer , are not always submitted for investigation post mortem . thirdly , there is little agreement among poultry pathologists upon the classification of cancer . 
the data available are thus no guide to " cancer incidence " in fowls , in the sense that this can be defined for mice and man , and are , for the reasons suggested above , usually a gross underestimate . 
although many such figures are available from various parts of the world it will perhaps be sufficient to compare the tumour incidence in the edinburgh flock , where all birds dying are examinedpodmortem , with data given bv goss ( 1940 ) , where a similar analysis has been made with flocks totalling 24 , 900 birds . 
out of 675 female birds dying since 1932 in the edinburgh flock at ages ranging from i to 9 years , only 50 , or 7 - 4per cent of the total adult mortality , gave evidence of neoplastic or allied conditions . 
the edinburgh flock in general is thus a " low cancer " line of considerable ' interest . at present it is sufficient to indicate that complications due to spontaneous cancer can be neglected in considering the resiilts which follow a preliminary 8tudy0f 8u8ceptibility . the first analysis was made upon a series of 429 birds inoculated with cell - free rous no . 
the susceptibility of each bird was graded a ' ceording to the following scheme : negative result ( 0 ) , regression of tumours ( r ) , tumour response to i to 4 , for increasing lasses in all . 
the largest size and malignancy of the induced sarcoma at death or after 28 days was used as an indicator of the susceptibility of the bird . the grading was ' done by inspection . weighing the tumour is unlikely to be more accurate because of the difficulty of clean dissection , and the neglect of such factors as the size and condition of the host , the invasiveness of the tumour , and the presence of large blood - clots and mucoid fluids within its substance . in addition to differences in susceptibility of the host other possible causes of variation were considered , such as sex , season , site of inoculation , number of inoculations , dose of virus , and presence of other factors , such as antibodies injected with the virus . 
no consistent sex difference in susceptibility was noted during the work , and , as was later seen in the analysis , sex does not seem to affect the susceptibility to any detectable extent . 
teratoma testis ( michaelowsky , 1928 ; falin and gromzewa , 1939 ; bagg , 1936 ) ; transplantable sarcoma ( peacock , 1935 ) ; chemical induction ( murphy and sturm , 1941 ) , an analysis of the susceptibility of these young chicks to the rous no . 
i sarcoma showed no seasonal trend ( carr , 1942 )  . that the site of inocul - ation is of little importance in influencing tumour growth was shown by gye and purdy ( 1 931 ) ; it was claimed by them that the resistance depends upon the dose of virus inoculation . no support for this claim could be found by carr ( 1942 , 1943a and b ) , and the results described below indicate that any such variation is inconsiderable . that the other factors mentioned , viz . 
number of inoculations - and presence of other materials , were probably of sl ' l ' ght importance was concluded from several experiments in which only one of these factors varied in an otherwise identically treated g ' roup . 
a large number of the experiinents found in the literature illustrate this point , which is seen to be confirmed in the analyses that follow . the birds comprising the first group of tested animals were from most - of the " all the year round " hatching had been necessary to maintain institute lines . an even supply of experimental chicks , but not many matingswere represented by more than a few tested chicks . in fact , the 429 birds were descended from 33 sires and 147 dams , and many matings had but one tested offspring . 
carr the various institute lines ; these were all selected for physiological characters associated with egg production . dividing each line into two clear classes , negatives and non - negatives , the difference between the breeding line ( with the largest number ) and non - moult line was examined . 
a similar test on the most conspicuous of the other negative tumour groups , intensity , gave a value of chisquare 1 - 23 , which is of no significance , being the variation that would occur in i out of 4 random samples . it was therefore unnecessary to test the rest of the since the regressio ' ns ( r ) are equal to the negatives in the breeding line , groups . but more frequent than the negatives in the non - moult line , the frequency of regressions in the non - moult line is therefore even more significantly disproportionate than the number of negatives , so that this line has an obviously high resistance to the production of fatal cancer by the rous no . 
at about the close of the period when the first analy 'sis was made , the breeding programme at edinburgh resulted in a large proportion of chicks provided for experimental inoculations being derived from a single pen of the breeding line . these chicks were all offspring of a single sire , f651 , and dams fairly closely related to him . .the annual population of the breeding line is larger than that in any of the other groups constituting the flock , and the method of selection used is such that they are also less inbred . in table iv the responses of the groups of progeny from 14 females mated to f651 are illustrated . it is obvious that there is considerably variation among the groups ; in the first three the responses are mainly restricted to the two highest types , and in the fourth the same tendency is only slightly less marked . in the next six progenies ( g196 - g866 ) they are distributed fairly evenly over all the classifications except the completely negative one . 
carr this tendency for the susceptibility of chicks from certain individual matings to fall into a rather narrow range has been encountered in other pens of birds , and knowledge of its existence has been made use of both in providing susceptible chicks for experimentation 4nd avo - iding the progeny of dams whose offspring were known to give a poor response . 
it had been noted that when the non - moult chicks included in the original analysis were grouped according to sires , one of the latter , h573 , stood out as producing particularly resistant progeny ( table v )  . fact , when the data from his chicks were omitted the difference between the responses of chicks from the breeding and non - moult lines were no longer signifiit seemed probable then that the disproportionate number of regressions cant . and negatives produced by h573 was not due to the character non - moult as such , but to some mechanism which can . 
on the other hand , to have carried out an experiment on a large number of birds in the hope that one of the rare resistant class was included would require labour and accommodation far beyond the facilities of any place engaged in fowl tumour work at this time.. the dams of the offspring of h573 analysed in table v were all fairly close relatives of the cock himself , and the way was thus opened for breeding a line of birds which would include a large proportion of resistant animals . it was arranged to carry out a small series of tests on the progeny of h573 , and almost all the birds tested gave either very ismall tumours , or more often , complete regressions . 
the slight shift towards greater resistance in the first 1941 test in both halves ofthe table suggests that some environmental factor leading t ' o a greater inhibitive effect on tumour growth may have been operative then . when the line had been thus established , a number of females , which had been tested and found to produce resistant offspring with a male of their own line , were then outcrossed to a non - moult cock , a descendant of the group from which the non - susceptible ( n - s ) line had been extracted . 
1 sarcoma virus varies from 40 per cent ( fischer , 1927 ) to 4 = 5 per cent ( gye and purdy , these figures may be complicated , however , by different rates of spon1931 )  . taneous sarcoma occurring in the population , either causing " natural " - or this complication is " induced " antibodies to be formed in the tested animal . probably absent at 6 weeks ( the age used here ) as no antibodies are present at this stage ( amies , 1937 ; andrewes , 1939 ; carr , 1943b ) , though they occur in resistance also varies with the age of the bird ( duranyounger and older chicks . reynals , 1940 ; rous and murphy , 1914 ; carr , 1943b ) , so a standard of age for testing is requisite for comparison . in the selection experiment for high and low susceptibility to jungherr sarcoma , carried out by cole ( 1941 ) for example , a resistant line with only 12 und impossible to raise the per cent susceptibility was obtained , but it was high incidence line much above the . 
original 70 per cent ; the cause of this may have been acquired r ' ather than a genetic immunity , since transmission from the immune female to the chick via the egg - yolk ( andrewes , 1939 ; carr , 1944 ) cannot be excluded , for progeny were tested at 7 - 18 days ,  . 
a time when yolk antibody is possibly still present in the chick . acquired immunity was ruled out as a cause of resistance of the n - s line . perhaps the most useful comparison which can be ' made is that between the present analysis of responses of the edinburgh flock to the filtrable tumour rous no . 
1 , and those of birds from the same stock to chemical tumour inducing material as demonstrated in the work of peacock , a report on which has been published ( greenwood and peacock , 1945 )  . 
the data , which cover the behaviour of 4 lines for the 10 - year period from 1935 - 1944 , are interesting both in their points of si ' milarity and dissimilarity to the material already discussed : they were classified only into positive and negative groups , but the non - moult line again showed itself the most resistant to cbemically induced tumours with a susceptibility of about 30 per cent , while breeding and large egg gave a figure close to 40 per cent and intensity had the highest susceptibility with 60 per cent since the early analysis of rous data places breeding ' as highest in posit ' lves . order of susceptibility , this difference in rank order might reflect inconsistency in the relative responses of the two lines to the different types of tumou ' r , but it appears more likely that with continued inbreeding the intensity line has chanced to become more susceptible . 
when most of the inbred lines were tested it was found that one in particular showed an obviously high resistance to the production of fatal cancer by the rous no . 
h there had been equal nijmbers of men and women , and equaltiijmbers in the age - groups , on an average the male mortahty would have amounted to 24 , 855 . 
environment and occupation may , therefore , be expected to exert a greater influence in men . bt say that , ta average age at death from carcinoma of each site . for each organ we can assess not only the fi - equency with which it is attacked , but also the average ao , , e at which this occurs . 
among jewesses we find a low incidence for carcinomas of the stomach , bile pwmges and cerv and a high incidence for carcinomas of the breast , ovary , intestines and kidneys . it would be more conrect to compare the jews , not with the average population , but with that of the big towns , for 80 - 4 per cent and 80 - 7 per cent of jews and jewesses respectively live in the big towns . if we do so , we find an increased incidence for carcinomas of the liver , gall - bladder , intestines , rectum , lung , ovary and breast , and a decrease for the mouth , oesophagus , stomach , uterus and skin . from the age - group distribution of jews and jewesses we should expect 228 and 296 cases of carcinoma respectively . 
versluys carcinoma and trade or profe , 88ion . we now come to the real object of this research - to trace the influence of trade or profession on the origin and the localization of carcinoma . 
our research covers a wider field than that of the so - called occupational cancers , and all that has gone before is necessary to enable us to interpret what follows . before we can proceed , we shall have to examine some problems a little more this will be facihtated by taking a specific occupation as an example , closely . and i have chosen coal - mining . the mortality cards show usa . 
how many people who had formerly been miners died of carcinoma from 1931 to 1935 , their ages , and the sites of their carcinomas . the census of 1930 ( there was no census in 1940 on account of the german occupation , consequently - an interpolation is - impossible for the years between 1930 and 1940 ) shows us ilow many miners there were in the netherlands and their ages , but ' thin ' about ex - miners . now if we take groups a and b together we include all miners who got carcinoma while still working or aftei . 
leaving the trade , with their ages , but t , leir distribution over the various age - classes cannot be compared with the census of 1930 , which gives no information about ex - miners . 
then the average error is when y i - s small this is practically equal to - % / .. this average error has always been taken into account in this research , and a difference is cared real only when the percentages found and those to be expected differ by at least 3 times the average error . fi - equency of carcinoma of the stomach and a low prostate fi - equency . 9 and 50 - 59 we find a total mortality of 50 cases , whereas we should expect 32 , so that the total carcinoma mortality of coal miners is very high . 
the fi - equency of carcinoma of the stomach is greatly increased , for we find 33 cases instead of the 12 we should expect . the number of cases of carcinoma of the prostate in these age - classes is too small to reach a conclusion . the question now arises , is this high stomach fi - equency amongst miners bound up with their trade or with their environment ; is it an " occupational or a " smial cancer " ? ( cramer )  . 
to answer this question we must caiieer study wives of miners " ( from the mortality cards of those married women where the trade of the head of the - fanifly is given as " coal miner . the manded woman practically always lodges with her husband )  . the percentage distribution of carcinoma over the various organs in " wives of miners " compared with the distribution in married women amongst the general population is shown in table xi . taking the " average error " into account , we see from table xi that only 172 j . 
the smaller the unit in our research the more chance we have of getting results of value . if we gather the trades into groups their typical characteristics will become less and less obvious until at last the ratios obtaining among the average population are reached . i have tried taking some trades together , but the typical characteristics of a certain trade always get lost , and the whole group misses what individual component parts show as typical . it is , however , worth while compari ' ng any one trade with another of the same kind , and i have therefore tried to arrange the order of the trad - es - discussed so that trades 6f a kind come near tog ' ether . table xii compares the actual deaths of men of different occupations with the numbers expected if the total carcinoma deaths had in each instance been distributed over the various sites in the same way as amongst all m - ales - that is to say , according to the percentages shown in table 1 . table xllla gives a similar comparison , for wives of men in different occupations , with the deaths expected if the total carcl ' no ' ma deaths had been distributed in the same way as amongst all married women . 
cervix uteri lung prostate lung prostate oil vender8 are only a small group but have an excessi - % , , ely high stomach frequency ' ( 26 carcinomas )  . . 
faxmers. baxmen butch ' ers soldiers - cigax makers soldiers university men tobacconists dock labourers shoemakers office - staff .iall porters officestaffs car men barinen teachers soldiers fisherinen plumbers greengrocers barinen plumbers commer . 
froiii the figures in this paper , but that would take up too much space . besides , in mv opinion conclusions will only be justifiable when we have sufficient international material at our disposal for comparison . this material will have to consist of the results of research on manv , relativelv small , areas during a period shortlv before the second world war , with due observance of the nece , - , sarv precautions . 
with larger areas racial , geographical and economic differences in the same trade plkv a prominent part . , and a trade during and after the war may be quite different in one countrv from another . there was too much changing of occupation . i wish to express mv gratitude to w . 
daab seemed to interfere with vitamin - a storage and hence to cut down food consumption , leading to a deficiency of some other kind , such as that suggested by zucker , berg and zucker ( 1945 ) , which was the immediate cause of the forestomach lesions . the present author ( 1947 ) was , however , unable to elicit such lesions in the stomachs of stock mice given daab orally , even up to 294 days , in either a balanced or one type of unbalanced diet . 
he concluded that otsuka 's diet ( which was grossly deficient in several essentials ) allowed a deficiency not existing in his own diets but necessary for eliciting such forestomach lesions in mice . he also found no tumours in similar mice injected subcutaneously with daab in arachis oil , on three occasions , up to 329 days after the first injection . 
daab thus appears not to be a carcinogen for the subcutaneous tissues of mice . hiowever , in another experiment which apparently broke fresh ground , the present author applied daab in acetone , in increasing strengths , to the nape of the neck of stock mice , and obtained two squamous carcinomas , one with spindlecell metaplasia , in 2 of 8 mice surviving 346 days or more . this seemed to be sufficient grounds for classing daab as a carcinogen for the skin of mice . a further series of experiments has now been carried out to check the previous findings with daab painted in acetone ; at the same time , the effect , if any , of added croton oil was investigated . 
at the commencement , all mice were painted with the solution containing croton oil ; after 15 days , the croton oil was withdrawn . croton oil was re - introduced for one - third of the mice after a further 167 days , and the experiments therefore fall into two groups : ( a ) initial croton oil , and ( b ) initial - plus - subsequent croton oil . applications were made to the nape of the neck , after clipping away hair , thrice weekly for a total period of 545 days . the basal diet throughout was rat - cake ( thomson , 1936 )  . ( a ) initial croton oil series . - the survival rates of mice surviving more than 200 days are shown in fig . 
kirby the commencement of painting ; of these , two showed acute yellow atrophy of hyperthe liver and one showed slight hyperkeratosis at the site of painting . keratosis , with or without necrosis or ulceration , was common after 200 days , but the first papilloma was found in a mouse killed after 320 days ' painting ; this papilloma grew as a coxcomb - shaped wart . 
the other mouse had a similar , though smaller , lesion which also proved to be a squamous carcinomna of low - grade malignancy . although a mouse dying after 435 days showed no gross abnormality at the site of painting , another dying after 449 days had two tumours in the painted area ; one of these was found to be a squamous carcinoma with invasion down to the depth of the muscle . 
a necrotic , warty outgrowth , showing parakeratosis beneath , and a multiple papillary growth , were found at the site of painting in mice painted for 495 and 545 days respectively , the latter dying at mice dying at 524 , 528 and 588 days , i.e. 
33 days after painting was stopped . 549 days respectively showed nothing more than a little hyperkeratosis at the the last survivor and one of the mice from group ( b ) unfortusites of painting . nately died at the same time ( 611 days ) and were examined post - mortem in the absence of the author . 
one of these mice showed early squamous carcinoma , and the other simple infected ulceration ; as there is no way of deciding which histological report belongs to which mouse , they will be excluded from consideration in comparing the results in the two groups . 
a mouse dying at 623 days showed no lesion at the site of injection . thus in 16 mice surviving more than 300 days ' painting with 5 per cent daab in acetone , 3 developed simple papilloma , and 3 others developed squamous hyperkeratosis and / or ulceration was found carcinoma , at the site of painting . in nearly all the rest . abdominal organs were only examined histologically when gross damage was visible , but the male dying at 449 days and one of the mice dying at 611 days showed amyloid changes in spleen , liver and kidney similar to those referred to in the previous paper ( kirby , 1947 )  . 
the mouse dying at 623 days showed pulmonary adenoma . ( b ) initial - plus - subsequent croton oil series . - survival rates , beyond 200 days , only slight are shown in fig . 
1. hyperkeratosis was found at the site of painting in 4 mice dying at 215 days and in 1 dying at 305 days . of 3 mice dying at 435 , 442 and 443 days respectively , all had papillomas , keratinized and partly necrotic , at the site of painting . 
of 17 mice painted for more than 400 days , 5 developed squamous carcinoma , and 5 others squamous papiiloma , at the site of painting , a tumour incidence of 60 per cent . 
the malignancy appears to have been low - grade in all cases , and metastases were never found . no evidence of spindle - cell metaplasia was seen in this series . 
as this substance is an intermediate in the manufacture of p - aminoazobenzene , the possible danger to workers handling it , especially in organic solvents , must not be overlooked . induction by daab of tumours at sites remote from that of application seems to be confined to the lung . 
no tumours were found in the liver of any mouse . co - carcinogen tests : neither the incidence of skin carcinomas - 3 / 11 ( surviving 400 days ) in group ( a ) and 1 / 5 in group ( b ) - nor the time of appearanceabout 400 days in either group - lends any weight to the view that croton oil acted as a co - carcinogen when applied concurrently with daab in group ( b )  . on the contrary , it would seem that croton oil had no effect either way on the induction of skin tumours . this suggests that the mechanism involved in carcinogenesis by daab differs from that of the polycyclic hydrocarbons . 
croton oil painted concurrently caused no increase in the incidence of the significance of the skin tumours , nor did it decrease the latent period ; absence of co - carcinogenic action of croton oil is discussed . the author is greatly indebted to p . 
kirby. from the research department , glasgow royal cancer hospital . received for publication , june 28 , 1984 . activity the carcinogenic of orally - administered 2 - acetylaminofluorene , aaf , for a number of tissues , mainly epithelial , was first demonstrated by wilson , deeds and cox ( 1941 ) for the rat , and subsequently confirmed for this species by bielschowsky ( 1944 , 1946 ) and others , for mice of various strains ( armstrong and bonser , 1944 , 1947 ; foulds , 1947 ) , for the fowl ( bielschowsky and green , 1945 ) and for the cat ( harding , quoted by bielschowsky , 1947 )  . recently wilson , deeds and cox ( 1947a ) have reported their own findings in mice of three pure strains . 
aaf has now been shown to be a carcinogen ( when given per os ) in eight strains of mice : cba , if , riii , white label , strong a , c57 black , c3h , and bagg albino . 
of the first five strains mentioned , cba were most prone to both liver and bladder tumours ; strong a were the least susceptible ( armstrong and bonser , 1947 )  . 
they received a diet consisting of whole meal flour ( 7 parts ) and skimmed milk powder ( 3 parts ) , supplemented by cod - liver oil and cabbage once weekly . for each animal 12 g . of food were provided daily . 
the dose of methylthiouracil given to the males was doubled during the last 10 days before they were sacrificed . four males and two females received methylthiouracil only ; two males and two females methylthiouracil plus a.a.f. , and four females a.a.f. 
only. thyroxine injections were started when the animals had stopped growing . this occurred in the females after three weeks of methylthiouracil treatment , in the case of the males , after four weeks . dl - thyroxine was dissolved in saline with na2co3 to ' give a solution containing 10 , ug . 
griesbach during the period of thyroxine treatment the rats were weighed were killed . twice weekly and the injected amounts adjusted to the weights . five female rats , 7 to 8 weeks old , were thyroidectomized . three weeks after operation , when the constant weight of the animals suggested completeness of thyroid ablation , these rats were started on the milk - flour diet containing 0 02 per this concentration of a.a.f. 
are badly tolerated the carcinogen to each rat per day . after eight weeks of this regime , thyroxine treatment by thyroidectomized rats . was started , each animal receiving one daily injection of 2 - 5 , ug . 
body weight completely compensated for the thyroxine deficiency produced by methylthiouracil , independent of the presence of a.a.f. twenty - two rats ( 6 males and 16 females ) were treated with 2 - 5 , ug . 
nor the controls reacted as uniformly as the animals injected with the higher dose of thyroxine ( table iii )  . in the males , the thyroid weights did not show any significant differences , the values being slightly above normal in both groups . 
with the exception of two animals , all showed an increase in cell all pituitaries were normal , showing heights far above the normal values . basophil counts of the same order as the controls . comparison of the values obtained in the animals with and without a.a.f. statistical shows that the greatest differences were found for the cell heights . analysis of these values proved that the difference between the means was highly the difference found for the means of the thyroid weights significant ( p < 0 0 1 )  . of the two groups , however , was of doubtful significance ( p > 0 05 )  . the pituitaries of the five thyroidectomized females treated with a.a.f. 
the weight increase of the thyroid induced by goitrogens is a complex phenomenon . it is due to increased numbers and size of the epithelial cells , and may be partially offset by the loss of colloid . 
when the supply of thyrotropin is reduced either by withdrawal of the goitrogen , or by administration of thyroxine , cell size decreases within a short time , whereas , the number of cells remains high over prolonged periods and colloid reappears . 
the latter factor must introduce uncontrollable errors when the thyroid weight is used as a criterion of thyrotropic action . in our experience , as in that of rawson and starr ( 1938 ) , the estimation of the mean acinar cell height has been found to give more reproducible results in assaying the degree of thyroid stimulation than the weight method . since a close correlation exists between the size of thyroid cells and the number of pituitary basophil cells , the percentage count of basophils has been used for assaying states of thyroxine deficiency in combination with the measurement of epithelial cell heights ( griesbach and purves , 1945 )  . in the state of fully developed thyroxine deficiency the percentage of basophils reaches values of 30 to 45 per cent . 
by excluding from the count masses of basophilic colloid free from cellular structures , we believe to have eliminated this possible source of error . all rats injected with 5 - 0 yig . 
griesbach the goitrogen - treated rat enlargement of thyroid cells is linked with an increase in numbers of pituitary basophil cells , indicating elevated thyrotropic activity . this correlation breaks down under the influence of a.a.f. 
one half of the animals still had large goitres and , histologically , in all but one the epithelium was almost as high as in the rats which did not receive thyroxine . no evidence for an increased demand for thyroxine or for higher sensitivity to thyrotropin was found in the animals treated with a.a.f. 
when a thyroxine deficiency was induced in a.a.f. treated animals by surgical or chemical means , their pituitaries responded in the similarly , the growth same way to thyroxine as did the animals without a.a.f. response of the female rats to thyroxine was independent of the presence of a.a.f. in the males , the pronounced liver damage prevented normal growth . these facts show that the action of thyroxine on the pituitary was not inhibited by a.a.f. 
the problem can therefore be reduced to that of an anomalous behaviour of the thyroid epithelium . in the hands of paschkis , cantarow and stasney ( 1948 ) l - thyroxine did not prevent the change from normal to high epithelium . in our experiments , physiological amounts of dlthyroxine did not reduce a high cylindrical epithelium to normal . it must , however , be remembered that the hyperplastic thyroid epithelium of the a.a.f. treated animals was not completely refractory to thyroxine . 
 it has recently been demonstrated that the most critical factor determining the epidermal mitosis rate in the adult mouse is the carbohydrate supply to the cells , and the evidence at present available all points to the conclusion that the function of this carbohydrate is to supply the energy needed during cell division in extending this work the discovery has been ( bullough , 1949a , 1950a , b )  . 
 made that a restricted diet has a powerful effect in depressing mitotic actirity ( bullough , 1949b ) , and it has been suggested that this obserration may help towards an explanation of tannenbaum 's remarkable results on the effects of restricted diets on tumour genesis ( tannenbaum , 1940a , 1940b , 1942 , 1944 , 1945 , 1947 )  . 
this involved a study of the results obtained with a graded series of diets as regards body weight , blood sugar concentration , liver glycogen content , and epidermal mitotic activity . 
 the two experiments performed involved a total of 55 mice , which were all in the first experiment the 25 adult males of between 3 and 5 months of age . 
 these mice had been reared since weaning on a mixed diet of commercial rat cake with cod - liver oil , flaked maize , and dog biscuit , but during the experiments they were fed on commercial rat cake alone . 
this deter mined the form of their diurnal cycle of mitotic activity , and ensured that a high mitosis rate developed shortly after midday ( bullough , 1948 )  . 
it was unfortunate that the animals in the first experiment were considerably lighter than those in the second experiment , but it was remarkable how little this fact affected the results obtained . 
 on the day when each experiment began a piece of ear was removed from each animal at 14.00 hours , the normal time of maximum epidermal mitotic activity associated with the afternoon sleep period . 
the animals were killed at 1500 hours , it having been previously determined that for a period of about 5 hours after the injection of this weight of colchicine there is no great disturbance of the mitosis rate or of the blood - sugar level ( bullough , 1949c )  . 
the liver was removed , cut into two roughly equal parts , and the glycogen content was converted into glucose by the method of good , kramer and somogyi ( 1933 )  . 
 in estimating the epidermal mitotic activity the pieoos of ear , fixed in bouin 's alcoholic fluid and embedded in ester wax ( steedman , 194 7 ) , were cut into sections 7 thick . 
 255097 217096 200076 199 : : : ! : : 075 197078 100 , , - : 250097 261085 267075 25 - 1 + 092 279 ; 0 - 97 in the second experiment only strong 's cba males were used , and these , being 4 months old when the food restrictions began , were heavier than the mice of the first experiment . 
 252068 244 : : : ! : : 052 218043 21 4052 21206 . ' ; 90 0 ' .o 247150 257118 252130 253075 246070 table ii . - the average body weight ( in grammes ) in group& each of 5 adult male mice fed on restmtetl diets of rat cake . 
 306116 288 : : : : : 115 279075 283070 299094 the results obtained were much as could have been expected , the figures for the groups on the lower diets falling steadily as the weeks passed . 
by the end of the fourth week it is clear that the relationship between body weight and diet is a direct one which can be expressed by a straight line graph . 
 since it is evident that mitotic activity is closely associated with carbohydrate concentration , the carbohydrate reserves were estimated at the close of the experiments in terms of the liver glycogen content and the blood sugar concen tration . 
 233 12 l 214448 200045 183459 172323 240619 218 133 199422 187413 18001 - .~ 175108 superficial examination of table iv might suggest that the poorer the diet the higher the blood - sugar level . 
at that time the blood - sugar level must have been low ( bullough , 1949b ) , and with a coincidentally low secretion rate of insulin the effect of the meal must have been to raise the blood - sugar level to abnormal heights . 
it is thus logical that the poorer the diet the higher the blood - sugar level should be , and once again the relation is a direct one expressible as a straight line graph . 
 75029 36042 25017 23018 22024 one surprising conclusion that can be drawn from these figures is that the imposition of a restricted diet results in an extremely rapid fall in the mitosis in most groups there was a steady reduction throughout the whole experi rate . 
i these results are expressed graphically , the figures chosen for com parison being ~ose of the numbers of mitoses observed after 3 weeks ( without colchicine ) and after 4 weeks ( with colchicine )  . 
it appears that in general the mitosis rates of the lighter mice of the first experiment were lower than those of the second experiment , but the differences are remarkably slight and are of doumful significance . 
 the most significant point emerging from these graphs is the indication given both with and without colchicine that the relationship between resmcted diet and mitotic activity is not a direct one . 
 the present results confirm earlier observations that restricted diets cause a pronounced fall in mitotic activity , and indicate that when less than 70 per cent of the normal food intake is given the epidermal mitosis rate is reduced to about 35 per cent of the normal . 
on the basis of earlier work it can be safely suggested that this reduction is caused by a shortage of carbohydrate , in the form of glycogen or glucose , in the epidermal cells themselves ( bullough , 1949a , 1949b , 1949c , 1950a , 1950b ; bullough and eisa , 1950 )  . 
at this time the fall in the body weight is only just beginning , and it is therefore evident that a mouse is unable to maintain a high rat , e of cell division by means of the utilization of fat deposits . 
 in a fully - fed four - month - old mouse of about 35 g . , as in a fully - fed three - month - old mouse of about 25 g . , the epidermal mitosis rate reaches a sleep maximum of about 75 mitoses per c similarly in either case the food intake remains steady at about 36 g . 
 ' when fed on restricted diets the mice lost weight in a regular manner week by week , the speed of loss being in direct proportion to the degree of underfeeding . 
 in a similar manner the carbohydrate reserves , as indicated by the liver glycogen content , fell after 4 weeks to a level which was directly proportional to the amount of food given . 
2 , in which for comparison a graph of the present results is in both cases the form of the graph is sigmoid , and in both cases the included . 
this adds further support to the thesis put forward by bullough ( 1949b ) , and developed in the following review ( bullough , 1950c ) , that the rate of tumour genesis in a particular tissue or in the body as a whole may be directly related to the mitosis rate . 
the mitosis rate in turn is related to a tariety of factors , of which one of the most important is the carbohydrate , or calorie , content of the food . 
 groups of adult male mice were maintained for 4 weeks on diets varying from 55 per cent to 105 per cent of what they would eat if fed ad libitu weekly records were made of the body weights and epidermal mitosis rates , and at the end of the experiments the carbohydrate reserves were estimated in terms of liver glycogen content and blood - sugar concentration . 
die greatest mitosis depression accompanied a reduction from 80 per cent to 70 per cent of the normal diet , a result which compares closely with that of tannenbaum ( 194 7 ) regarding the effects of restricted diets on carcinogenesis . 
kreyberg. from the institutt for generell og ek8perimentell patologi , universitetet i oslo . received for publication march 9 , 1953 . the clinical problems of breast carcinoma have been under intensive discussion for decades . 
a great deal of detailed information has been accumulated , but still widely different views are entertained as to diagnosis , treatment and theraour present knowledge was amply illustrated during the panel peutic results . discussion on treatment and results in cancer of the breast at the thirtieth annual meeting of the american radium society , chicago ( 1948 ) , and at the twenty - fifth meeting of the northern surgical association , copenhagen ( 1951 ) , to which readers may be referred . a few points seem to be universally acknowledged , as regards treatment . firstly , a careful and extensive surgical intervention will , in a number of cases , be life saving , or life prolonging . 
on the other hand , if the surgeon operates in a field where cancerous cells are present and the operation is incomplete , the surgeon may by his intervention precipitate an outburst of metastases and shorten the it may further be agreed that the development of the special life of the patient . surgical technique since the days of halstead and meyer is comparatively small , and that the advances , as manifested by a higher cure rate , are modest and mostly caused by improvements of surgery in general , for instance the introduction of penicillin and a better postoperative regime , thereby reducing the immediate it was this state of affairs that caused mcwhirter ( 1949 ) operative dangers . to state : " when radical mastectomy is the only method of treatment available and when all cases coming to a large general hospital are taken into account , the five - year survival rate is unlikely to exceed 25 per cent "  . secondly , it seems generally accepted that radiological treatment in a certain , restricted number of cases and under certain conditions , is able to effect a complete destruction of the tumour cells and thereby be life - saving . it further seems generally accepted that radiological treatment in other cases may , for a shorter or longer period , retard the development and the spread of the tumour cells , and that radiological treatment thereby may be life prolonging . kreyberg ( 1938 ) microscopically examined breast carcinomas and axillary metastases which had been submitted to pre - operative irradiation . 
the material came from three different hospitals , using different radiological techniques and different doses . the conclusions were that - : a pre - operative treatment , with the doses used , may 158 l . 
kreyberg in a series of cases damage the tumour cells to a degree , histologically visible , and in rare cases lead to complete disappearance of the tumour cells . this effect is dependent upon the dose , the effect being more pronounced after stronger doses . also the axillary metastases are damaged , but in a considerably lower degree than the primary tumour . but , even after the strongest doses ( with tele - radium ) , a great number of tumours show such small changes that we must conclude that the cells are growing during and in spite of the treatment . these observations have been generally confirmed . 
kaae ( 1952 ) stated that only 15 per cent of all breast carcinomas are really radiosensitive . baclesse ( 1949 ) had greater effects , but he used very heavy doses . 
an observation period of 5 years only is , however , too brief , since one of the radiological effects is fibrosis and scarring , after which cancer cells , retarded in growth , may regain their vitality and proliferative possibilities at a later date . haagensen ( 1949 ) stated " our reliance upon irradiation for the cure of the disease ( breast carcinoma ) has faltered until we have come to the point where we reserve irradiation for cases in which palliation is all that can be hoped for . " an attempt has been made to combine surgical and radiological treatment , in the hope of obtaining better results . 
the absolute or over - all cure rate is the number of patients alive and symptom - free out of the total number of patients received in the hospital and suffering from the disease under investigation . all dead are counted as victims of said disease , regardless of the real cause of death . 
even if this strict attitude is adopted , we meet , however , with factors which influence the statistics . firstly , the general cancer consciousness of the society , which to a certain degree will influence the relative number of early and late cases . secondly , social and racial factors , which may influence the soil of the cancer cells , and thirdly , the relative number of cases with moderate and with high malignancy , as shown by bloom ( 1950 )  . kreyberg ( 1952 ) in a survey of lung cancer in norway attempted to show that the difference in the sex distribution of this form of cancer in norway , as compared to england and wales , may be explained by the difference in the relative number of the different histological types . 
a similar situation may hold it is probable , therefore , that besides a plea good for breast carcinoma as well . for the use of absolute cure rates and tumour stages already in use , also a correction for tumour types and grades should be attempted . nielsen ( 1951 ) gave as reasonable the following figures as the average chances for a breast carcinoma patient in scandinavia : 5 - year survival rate , symptom free ( operable cases ) , 35 - 50 per cent . 5 - year survival rate , symptom free ( absolute ) , 20 - 30 per cent . these figures are valid for a population with a generally fair cancer consciousness and with a rather high standard of the doctors and the hospitals . individual surgeons and special clinics may present better results , but such material is more or less selected . the cause of the depressingly low cure rate in breast carcinoma is two - fold : ( 1 ) the tumour cells have spread beyond surgical control before the operation is performed and even before the diagnosis is made , and / or ( 2 ) the tumour cells are not sufficiently radiosensitive . this state of affairs has naturally led to a quest for other means of improving the therapeutic results , and as one of those , the importance of " early diagnosis " has been universally stressed and accepted . it may be useful therefore to examine the meaning of the designation " early diagnosis "  . 
in the present paper it is intended to examine different definitions of the term " early diagnosis " commonly used in order to ascertain our position today as regards the criteria for the immediate recognition of a breast carcinoma in a stage where a complete cure is possible , if a proper treatment actually at our disposal is used . especially will be examined the foundation of a propoganda promising great hopes of cure if the patient arrives for treatment on the basis of an " early diagnosis "  . when a breast carcinoma develops morbid changes have usually been present in the tissue for a shorter or a longer period . 
even if the essential change is considered to be a somatic mutation in a single cell , this mutation has its local further , the tissue is not clinically cancerous before the proliferation cause . has reached a certain extent . 
from a therapeutic standpoint to - day the breast carcinoma is in its early phase as long as the tumour is localized to a degree that makes a complete cure possible by such a relatively simple local operation as this is the background for the designation " stage i " , and in the mastectomy . absolute sense mastectomy should by definition in such cases result in 100 per 160 l . 
the discrepancy between the number of tumours histologically classified as stage i and the number of cures effected in this group , after a proper local operation , shows the degree of failure in the process of staging . this failure is approximately 20 - 30 per cent . in spite of this serious inaccuracy the histological staging is the method used for grouping of tumours for comparing different therapeutic interventions . the most accurate staging is the retrospective clinical , taking into consideration the final development of the cancerous process in each individual . even this staging is not perfect . it has been mentioned that patients supposed to be stage i eventually are shown to be in stageii or further . 
on the other hand , patients believed to be stagei , though actually in stage ii , may never be recognized as such if radiological treatment cures the patient . this brief survey shows that the decisive determination of the stage of a certain tumour is neither a direct nor an immediate process . 
kreyberg this table shows that even in these groups , where the time lag between diagnosis and commencement of treatment is reduced to the practical minimum , only half of the average patients can count upon a 5 years ' survival symptom free . it seems , therefore , that the definition p2 is of rather limited usefulness because a great number of the tumours are not any longer curable and the definition has not contained the criteria necessary to obtain this goal . 
a limited usefulness of p2 is demonstrated by the fact that some patients , an unknown number , have benefited from the shorter time lag - a question which will be discussed later . if we analyse the usual symptoms , some of them ( a feeling of heaviness , pains , stinging sensation and similar ) are rather vague and strictly subjective and little fitted for attempts at earlier detection . 
but among the symptoms analysed , a lump in the breast is the first in at least three - fourths of all cases , and this symptom is more material , more objective and more fitted for diagnostic research . 
here a regular and systematic palpation may facilitate the discovery of comparatively small nodules , but there evidently is a certain lower size limit . kaae ( 1948 ) voiced the traditional opinion when he stated that : another attempt at a useful definition may accordingly be : a diagnosis of a very small tumour ( p3 ) , in the hope that all such tumours actually are curable . " it is generally recognized that the size of the tumour is a very important factor in the prognosis , and that the latter is much more favourable for the small tumours than for the large . " if we , however , examine the pertinent literature , we shall discover that the students of this problem are not at all unanimous . 
the fate of the patients was followed and the long range survey , ten to twenty year 's observation , showed that nearly two - thirds of the patients had metastases when arriving for treatment . 
even the very smallest carcinomas , those the size of a pea or a bean , had a fatal outcome in four out of ten cases . these facts show that our attempt to define " early diagnosis " as a diagnosis of a very small tumour ( p3 ) , actually a tumour as small as practically diagnosable , also fails miserably . taking into consideration the three commonly used or accepted definitions of " early diagnosis " , pi fails , because the criteria are not immediately available , and p2 and p3 fail , because the criteria do not enable a patient to recognize a tumour still in a curable stage . 
nor is any other definition known , which makes such a recognition possible to - day . what p2 and p3 give are indications for obtaining the earliest possible diagnosis with our present diagnostic means . 
an examination of the actual degree of earliness shows that only half of the tumours occurring in a population can , under the best possible conditions , be diagnosed early enough to be cured with our present therapeutic means . 
the high percentage of cures is the result of a very strict selection of cases . first all cases proved to belong to stage ii , or further , are excluded . this would leave a curability of approximately 75 per cent for the remaining . next , larger tumours , and finally especially malignant - looking tumours , are excluded . 
a further improvement in the statistics may be obtained by a still greater efficiency in the process of selection , not necessarily being an expression of increased chances for the patient at large to survive . it is not correct and not fair to publish such statistics in a manner that makes 164 l . 
kreyberg the public believe that if the women examine themselves regularly and carefully , and pay a visit to a competent doctor at the first suspicion of a symptom from the breast , their chances of a complete cure is in the vicinity of 90 per cent . 
kaae ( 1948 ) arrived at the same standpoint , and wrote : " it is indicated by these investigations that a 5 - year symptom - free survival rate of about 40 per cent is obtainable in denmark to - day , and that these results may be improved from 40 to 50 per cent , if all patients see a doctor as soon as they notice the first symptom , and if the doctor makes the correct diagnosis and institutes adequate treatment without delay "  . the present study seems to show that a diagnosis as early as possible is of great importance to a certain , yet unknown , number of individual breast carcinoma patients . 
as we do not beforehand know who will benefit and who will not , a general plea for " early diagnosis " is fully substantiated , as every individual salvaged is important . 
we must , however , always have in mind that the benefit is statistically moderate , and we ought to be modest in our claims as to the possibility of materially altering the situation for the breast carcinoma patients by this approach to the problem . it has finally to be added that the present conclusion is based upon the use of the word " early " as an expression of curability seen on the background of our present diagnostic and therapeutic means . 
the earliness is , term is not used in the sense of a more or less absolute time unit . actually , here synonymous with curability to - day , and this again , in most cases , means a carcinoma in stage i . if we examine the means to diagnose a carcinoma still in stage i , we will discover that such a diagnosis can with a reasonable certainty be made only after a retrospective clinical survey , lasting some 15 to 20 years . the analysis further shows that we have no criteria enabling an immediate " eary diagnosis " , in the sense required . 
the mixtures which had a ph of about 2 - 5 were polarographed as f - 611ows , : the test solution , into which dipped a dropping mercury cathode , was connected to a saturated calomel reference anode ( s.c.e. ) by salt - agar bridges ( saturated kci in 3 per cent agar - agar ) and the solution deoxygena - ted by passing a stream of water - washed oxygen - free nitrogen through it for 10 minutes . 
the percentage ttc reduced by serum was estimated with reference to the wave height of ttc in the blank reaction mixture . triphenylformazan 1 - 2 volts under the present conditions . gave no reduction wave in the range 0 to 200 to fig . 
2. - scatter diagram showing negative linear correlation between percentage ttc reduction regression lines have been constructed from by serum and percentage tumour weight . the regression equations : in the scatter diagram , fig . 
2 , from which it will be seen that there is a negative linear correlation between percentage ttc reduced and percentage tumour weight . the correlation coefficient ( r ) was calculated in the usual way ( moroney 1953 ) and found to be - 0 - 75 , t test = 5 - 63 ( n = number of animals ) highly significant at the 01 per cent level . reducing capacities of tumour and normal rat sera are show - n in fig . 
serum hastened colour development in iruminated mixtures , the colours being marked after i day . control solutions containing no serurn required 2 to 3 days to develop a pink colour whfle serum mixtures and controls kept in the dark exhibited no colour even after i week . after exposure to dayeght for 2 days tumour serum mixtures were coloured pink whereas normal serum mixtures , orange - pink after i day , were orange366 w . 
neish of 10 tumour sera , 9 ( tumour range , 3 - 4 to 22 - 8 per cent ) yellow in colour . showed pink colours and 1 serum ( 8.1 per cent ) gave the orange - yellow reaction . six normal sera each gave orange - yellow colours . in time , all colours faded to pale yellow and the solutions fluoresced blue in ultra - violet light . 
no difference was found with respect to ttc wave height between tumour and normal serum - ttc mixtures and the illuminated control but a new wave was observed in each solution which had been exposed to light . this wave was never observed in the ttc - alkali reaction mixtures described in sections ( 1 ) and ( 2 ) , or in control mixtures kept in the dark . 
and it was found to be due to another photochemical reaction product of ttc , namely the 2 , 3 , diphenylene - 5 - phenyl tetrazolium compound ( blue fluorescent in ultra - violet light ) described by hausser , jerchel and kuhn ( 1949a ) and by kuhn and jerchel ( 1952 )  . 
they take advantage of the spontaneous adhesion on plastic membranes of the free cells present in physiological fluids such as blood , cerebro - spinal fluid , peritoneal and pleural effusions . in brief : glass slides coated with formvar are placed in contact with the fluid ( with addition of heparin if necessary ) in an incubator at 37 ' c . 
for 15 to 60 minutes . the slides are then rinsed with tyrode solution at 37 ' , fixed 10 minutes to several hours in acid osmic vapour and washed thoroughly in distined water . the formvar is stripped from the slide , mounted on grids and anowed to dry at room temperature for at least 24 hours . photographs were taken with a triib - taiiber electron microscope at 60 kv . we adopted stringent criteria for purposes of comparison and considered only undamaged cells , that is to say cers having clear and well defined chondriosomes and with a satisfactory cytoplasmic transparency . 
as the appearance of a cell may vary from one area to another ( because of differences in spreading , lipid constituents , etc . ) we only considered the best portions . counts were made in each cell of osmiophihe bodies less than 150 mp . 
at least a few such bodies are to be found in every cell , but to consider them as true ultrachondrioma we adopted as a minimum 10 such particles 354 j . 
oberling showing a certain degree of polymorphism ( to distinguish them from merely lipidic granules ) per i oo #2  . for each preparation at least 1000 cells were counted . 
the same submicroscopic corpuscles as in leukocytes are encountered , but frequently they appear as bent or twisted filaments which may have swelhngs or a beaded structure . sometimes these filaments are extremely long . their thickness may vary from 30 mlt . 
they may aggregate in groups of two , three or more , or may appear to arise from an ordinary chondriocont . the statistical analysis shows that those submicroscopic bodies are not a ebaracteristic only of nialignant effusions but are seen in various inflammatory or circulatory disturbances . 
but when those figures are an almost constant finding , when it becomes impossible to estabhsh a distinction between chondrioconts and those structures on any other basis than the rather arbitrary one of size and thickness , then it seems difficult to deny the mitochondrial nature of the described structure . they have the same characteristics and the same polymorphism as certain types of mitochondria ( especially in plant cells )  . 
even the specifity of janus green stain depends on certain criteria ( showacre , 1953 )  . furthermore there is a question of principle involved in the discussion about the significance of these structures . if we require for the identification of ultramicroscopic structures the same characteristics as those used in classical cytology , ff certain mitochondria can no ion er be considered as such because their size prevents the use of janus green and the apphcation of more or less debatable functional tests , then we shau have two cytologies : orie optical and one electronit is highly improbable that cytoplasmic conical , which is not satisfactory . stituents are of a different nature simply because they are too smar to be seen with the ordinary microscope . on the contrary it should be our aim to show the links between microscopic and - ultramicroscopic structures . this has been done with great benefit with basophihc structures , ergastoplasm and intracytoplasmic network . it would be curious if the same did not hold true for the mitochondrial structures . furthermore the concept of mitochondria which are invisible witli the optical microscope is not new and it can account for certain results . many cytologists consider the chondrioma as fixed both in amount and morphology . 
but this stabihty is dependant upon the material studied , and it is in fact true of speciahzed tissues observed under standard conditions . botanists have long noted the morphological variations of the chondrioma in active cens ( guilhermond , 1934 ; gautheret , 1950 )  . no6l ( 1924 ) and many others bave made similar observations with animal cells . the researches of levi ( 1934 ) , lewis and 1 - jewis ( 1915 ) , etc . , seemed in favour of the de novo appearance of mitochondrioma in cells of tissue cultures . recently chevremont and frederic ( 1952 ) observing tissue culture cells during mitosis with the phase contrast - microscope , noted the transformation of chondrioconts into very minute rods and granules which resemble the structures described here . ' these formations sometimes disappeared and appeared again in daughter - cehs and then growing thicker and longer , reconstituted ordinary chondriosomes . the existence of the ultrachondrioma may well explain the apparent appear - ance de novo of mitochondrioma as a result of their regeneration from the ultra.chondrioma. it is not impossible that the absence of the ultrachondrioma in many cers may be more apparent than real -  . 
the degree to which ordinary mitochondriaare susceptible to variations of physicochemical conditions such as ph , osmotic afinor variations of conditions that are uncontrollable pressure , is well known . by present methods might cause a cavitation of the ultrachondrioma that would make it impossible to distinguish from the surrounding endoplasm . actually we never observed ultrachondrioma in cells where swelling of the ordinary chondrioma occurred . furthermore we sometimes found ultrachondrioma in the perinuclear region wben very favourable conditions permit observation in this area . but usually the thickness and high rpid content of this area in spread cens pre - ntent its study with the electron microscope . 
oberling there are two fields in which the existence of the ultrachondrioma raises special problems . in cytology , the presence of corpuscles resembling viruses in normal ( or presumably normal ) cells should be a warning against mistaken interpretations and will complicate the task of those workers who are engaged on the problem of the interaction of cell and virus . in biochemistry it introduces a new factor into the study of cytoplasmic it seems obvious that a large part of fractions isolated by ultracentrifugation . the ultrachondrioma will be deposited in the so - called microsomal fraction and would therefore lead the erroneous conclusions concerning the homogeneity of this fraction . the concept of the ultrachondrioma limited though it appears should entail a critical revision of some of the present data of cytology . we wish to thank madame dontcheff for the tissue cultures , and madame arnoult and martin for technical assistance . 
the ratio of the concentration of the compounds in the stomach to that in the blood in this range was about 20 : 1 or greater . by selecting carcinogens that have a pk , , falhng in this range it should be possible to circumvent the mucus barrier and expose the glandular stomach to attack . 
the animals had been fasted for 48 hours preceding the operation to simultaneously with the injecavoid contamination of the secretions with food . tion of the compounds to be tested 0 - 2 mg . 
with acetone and this extract allowed to stand overnight it was then centrifuged for 20 minutes at 2000 r.p.and the superat 5 - 10 ' c . natant used for spectrographic analysis . measurements were made on a beckman model du spectrophotometer against acetone - hci standard having the same ph as the gastric extracts . standard curves were obtained which essentially followed beer 's law . 
the 2 , 5 - isomer is soluble , whereas the 2 , 7 - isomer is not ( morgan and thomason , 1926 )  . yields of 55 to 60 per cent were obtained of 2 , 7 - dinitrofluorene decomposing at 293 - 4 '  . the 2 , 7 - dinitrofluorene was reduced with tin and hydrochloric acid by the method of schulman ( 1949 )  . 
the pure compound melts at 165 ' after recrystalthis was then converted to the dihydrochloride and lization from benzene . 2 - acetylamino - 7 - aminomono - acetylated in aqueous solution ( schulman , 1949 )  . fluorene hydrochloride was then slurried in 500 ml . 
the almost clear solution was filtered hot and a cream - white product precipitated from the cooled three recrystallizations from 50 per cent acetic acid resulted in a filtrate . goulden and kon ( 1945 ) reported that 2 - hydroxy - 7compound melting at 232 '  . acetylaminofluorene melts at 232 '  . the dyes of this series were prepared by coupling the components in acid buffered , or basic aqueous solution , neutralization and filtration . 
the yields ranged from 70 to 90 per cent . products could be recrystallized from dilute cellosolve , but highest purity was obtained from aniline , or benzyl alcohol . these compounds have not been previously reported . constants and analyses are given in table il 368 f . 
compound iv seems to be secreted to a slightly lesser extent , but this may not be significant . this was entirely unexpected , because it has a pkb ( 8 - 5 ) which hes in the optimum secretion range ( ray and jung , 1951 )  . this indicates that the pkbof maximum secretion in the fluorene series is much higher than it is in the benz ' ene series . because the serosa was colored , it was thought that this dye might have been reduced in the stomach at the azo link . 
an examination of the stomach contents for aminofluorene by the method of westfall and morris ( 1947 ) by miss mary f . argus failed to show the presence of this substance , either free or coniulyated . while , successful in leading us to potential carcinogens that are secreted in large amounts by the stomach , it is obvious that some factor ( or factors ) are involved other than the pkbit is true that the stomach of the rat may be less acidic than that of the dog , but this should only reduce the total concentration and not the relative order of absorption . the use of a tricyclic molecule hke fluorene in place of benzene leads to compounds with greatly reduced solubilities in dilute acid . 
the introduction of a third ( insoluble ) phase might well cause the stomach barrier to operate to exclude compounds of lower pkb ( greater basicity )  . the demonstration that some of these compounds are secreted in rather large amounts in the stomach has encouraged us to set up long - time experiments for testing their carcinogenicity . 
the histology was typical of lymphosarcoma , the cells being chiefly of the " lymphoblastic " type . local spread had occurred upwards in the submucosa for a short distance , and there was infiltration of adjacent rectal muscle but no noticeable spread in perirectal fat . 
the tumour was softer in consistence than most carcinomas and the base of the ulcer was covered by a greyish slough . both " lymphoblastic " and " lymphocytic " cells present . extensive spread in rectal muscle and commencing invasion of perirectal fat . 
the adenocarcinoma had infiltrated more deeply , but there was no sign of venous spread and the lymphatic glands were all free from metastases . we have given careful consideration to the possibility that this might actually be only one tumour , exhibiting an undifferentiated pattern in one part and a differentiated glandular pattern in another , as was suggested by gr . 
tumour b is a melanoma with four lymphatic metastases containing melantumour a is an adenocarcinoma with two lymphatic metastases free from pigment . section of tumour a showing adenocarcinoma , fig . 
1945 , and found to have a fibrous nodular tumour on posterior quadrant of lower third of rectum . biopsy showed spindle cell sarcoma apparently of low grade malignancy . seven years previously patient had had the coccyx removed in another hospital , and three years later a small tumour had been found in the rectum which was reported as a mass of fibrous tissue . synchronous combined excision of rectum by o . 
more than 4 inches of healthy bowel both tumours had given separated the melanoma from the adenocarcinoma . rise to lymphatic metastases , those from the melanoma being pigmented , whereas those from the adenocarcinoma contained no melana unique pathological specimen . 
twenty years ago weeks ( 1927 ) found reference to 100 cases of rectal sarcoma , but he regarded many as of doubtful validity and remarked - " if the questionable cases were discarded it is certain that the number would be reduced by one half . " we agree with this comment and have formed the impression that many of the cases which until recent years were recorded in the literature as " sarcomas " were probably examples of anaplastic carcinoma . this criticism does not apply to the cases reported in the last 15 to 20 years . most authors who have written about this subject seeinm to take the view that all varieties of sarcoma tend to run a rapidly fatal course , but we think that each of the four varieties of malignancy has this attitude needs qualification . to some extent its own characteristics and peculiarities and the prognosis differs considerably in each . lymphosarcoma is the commonest form of sarcoma of the rectum . it may manifest itself either as a single localized tumour or give rise to a crop of tumours bensaude ( 1929 ) was one of the first to spread over a long stretch of the bowel . draw attention to the diffuse or generalized variety of lymphosarcoma . in one of our cases ( case 3 ) the disease affected the whole rectum and distal end of the pelvic colon , so that in describing the primary focus we could not speak of a particular site of origin , but only of a region of involvement . 
the largest tumour was in the lower third of the rectum , but the other smaller tumours at a higher level were certainly not secondary growths resulting from the transportation of tumour cells , but were obviously new foci of lymphosarcoma developing indein spite of this unfavourable feature of lymphosarcoma the prognosis pendently . after surgical treatment would seem to be fairly good on the whole . 
at present there is insufficient evidence on which to base a comparison because it is only within recent years that these tumours interest in the subject have been separated out from other varieties of sarcoma . of reticulosis , stimulated by the writings of robb - smith ( 1938 ) , has had considerreticulum cell sarcoma is certainly a rarer tumour able influence in this respect . in the rectum than lymphosarcoma , and we think that it will probably be found to have a worse prognosis . spindle cell sarcoma is also a rare form of malignancy in the rectum . it is the one most easy to distinguish clinically from carcinoma because it obviously arises from the tissues of the bowel wall and not from the surface mucous membrane . the firm solid structure and covering of intact mucosa are of special significance . it has already been mentioned that in their histology these tumours give the impression of being of a relatively benign character . all who have written about melanoma speak of it as the most malignant of all the tumours now being considered . 
we agree with the view expressed by linder and wood ( 1936 ) that melanomas arise from the skin of the anal canal and tend to grow up into the rectum and that they metastasize early . 
the lymphatic glands may contain more pigment than the primary tumour , but it is worth mentioning that the haemorrhoidal and paracolic lymphatic glands may contain melanin apart altogether from the presence of a melanotic tumour . 
bussey although the cases we have examined personally are only ten in number they do provide material for comparison with the much commoner tumour , carcinoma of the rectum . in the end , of course , these rarer forms of malignancy can only be identified by detailed study of their histology , but there are some features in their gross characters which would make an experienced surgeon suspect that he was dealing with something " out of the ordinary . " we have summarized these by setting them out in tabular form ( table i )  . finally we have left to the end what we consider to be the most interesting feature of these rare tumours , namely , the frequency of multiple foci of malignancy . in four of our ten cases more than one tumour was found in the rectum , and in two cases the second tumour was of a completely different histological type . 
this raises the question both of multiple malignancy and dissimilar primary tumours . multiple malignancy is commoner in the rectum than is usually supposed . it so happens that we are in a position to give facts about this question because for many years we have been making observations on the frequency of the occurrence of multiple primary carcinoma and have found that in operation specimens of rectal cancer removed by a combined operation more than one primary rectal carcinoma is present in 4 per cent of cases ( over 2 , 000 examined )  . moreover we have records of many additional cases in which a second carcinoma was present in the colon in association with rectal cancer , so we were not surprised to find multiple tumours in our cases of lymphosarcomas ; in fact , we expected this to be the case . the occurrence of dissimilar primary tumours was , however , a complete surprise , and as far as we have been able to find out has not been previously recorded as a characteristic of these rarer forms of malignancy . in any organ of the body the existence of two tumours of a different histological type is a rare phenomenon . it is indeed remarkable that this unusual combination should have occurred twice in a series of only ten cases . 
we have searched through the literature but found no reference to the simultaneous occurrence of carcinoma and sarcoma in the rectum , though kreibig ( 1929 ) mentions a case of carcinoma plus lymphosarcoma in the ileo - caecal region . as far as the general relationship between carcinoma and sarcoma is concerned we note that warren and gates ( 1932 ) in a study of this subject were only able to collect from the literature 25 instances of the co - occurrence of carcinoma and sarcoma as separate tumours in the same organ . three were cases of sarcoma and carcinoma of the breast , twelve were of the uterus , and ten were in miscellaneous organs , including four cases of the combination of carcinoma and 1ynphosarcoma of the stomach . they found no recorded case of carcinoma and sarcoma of the rectum or indeed of carcinoma of the rectum associated with sarcoma of any other part of the intestine . 
melanoma arises always from the ano - rectal region and spreads upwards into the rectum . it metastasizes early and runs a rapid course . in four of the ten cases we are reporting more than one malignant tumour was present in the rectuone of these was an example of multiple lymphosarcoma and another of multiple reticulum cell sarcoma . in these cases tlhe associated tumours were of the same histological type , but in two other cases the associated tumours were of completely different histological type . 
rinaldini. from the strangeways research laboratories , cambridge . received for publication april 25 , 1952 . the nitrogen mustards have been shown to have a marked inhibitory action upon cell division , a property that warrants their inclusion in the miscellaneous group of the " mitotic poisons " ( loveless and revel , 1949 ) and their use as chemotherapeutic agents in certain forms of malignant growth ( haddow , 1947 )  . some of the 2 - chloroethylamines are mutagenic in drosophila ( auerbach and robson , 1947 ) and in neurospora ( tatum , 1947 ) , and more recently both the alkyl ( boyland and horning , 1949 ) and the aryl ( haddow , kon and ross , 1948 ) derivatives have been shown to exhibit tumour - inducing properties . the present work deals primarily with the effects of p - amino n - n - di - ( 2 - chloroethyl ) aniline hydrochloride on the number , duration and distribution of mitoses in tissue cultures during the first 1 to 3 days after exposure . 
though not very adequate for detailed cytological work because of the smallness and large number of the chick chromosomes , this material was found particularly suitable for quantitative treatment as regards variations in mitotic number and duration of the mitotic cycle . 
mitotic counts in fixed and stained cultures . this method furnishes data on the total number of mitoses and on the number of cells undergoing each phase of division at a given moment , and therefore an indirect estimation of the delay or arrest at any stage of the cycle . 
the number of abnormalities can also be ascertained . the cultures that showed the most abundant growth after two transplantations were selected , and the explants were cut in halves as closely similar in size as possible , under the dissecting microscope . 
all the solutions used here were made up in tyrode fluid . the cultures were stained with ehrlich 's haematoxylin after hydrolysis in n hydrochloric acid for 8 to 10 minutes at 600 c . 
 ( hughes and fell , 1949 )  . total mitotic counts were made in every culture . in order to facilitate counting the whole of the mitotic cycle was considered to be comprised within the period between the disappearance and the reappearance of the nucleoli . exception was made , however , for those cells in which the nucleolus persisted in advanced prophase and , conversely , for telophases in which the nucleus was fully reconstructed before completion of cytokinesis . 
low power phase - contrast cinemicrography . this method permits a direct , though only approximate , measurement of the rate of division and duration of each phase in a group of cells . for film recording the cultures were mounted in an air - tight chamber made with a metal frame between two coverslips and sealed with paraffin wax ( hughes and swann , 1948 )  . 
rinaldini the apparatus , devised by canti and lately improved by hughes , consists of a phase - contrast microscope encased in a thermostatically controlled chamber and attached to a 35 mcine camera . 
the chromosome movements can be seen in detail , and it is possible to measure accurately the duration of each mitotic phase . the technical arrangements were similar to those for the low - power film recording , except that critical focusing and phase adjustment required constant observation , and the time interval between frames was much shorter . 
rinaldini less concentrated solutions of the order of 1 : 50 , 000 to 1 : 100 , 000 - 74 x 10 - 6 and 37 x 10 - 6 molar - allowed indefinite survival and successful suboultivation , although the outgrowth was smaller than in normal cultures . 
at this stage the treated cultures showed no sign of recovery , but on the contrary there was a visible difference in the area of the outgrowth as compared with the controls . this was measured with the aid of a camera lucida as shown in fig . 
lindley using test " t " for p = 005 , the x2 analysis of contingency tables and the analysis of the variance on the square root of the counts . 
the percentage of abnormal proand metaphases taken together was approximately 35 per cent after 24 hours and 20 per cent after 48 hours , while the number of abnormal anaand telophases was only 4 per cent after 24 hours and reached 12 per cent after 48 hours . in spite of the normal appearance of the resting cells , all the evidence obtained from the counts points to the fact that almost 100 per cent of the inhibitory action was exerted during interphase . 
rinaldini no difference was found between the duration of 10 normal mitoses photographed during the first 5 hours and the last 5 hours of an experiment , nor between peripheral and central cells . 
a similar case was recorded under high magnification ( see below )  . six cells could be followed from one division to another in the control cultures . the intermitotic period varied from 5 to 20 hours , with an average of 10 - 6 hours . cells in the middle had a longer resting stage than cells in the periphery of the outgrowth . in the treated cultures no cell could be found to divide twice in one film ( 20 to 24 hours ) , but due to the scarcity of cell divisions it was not possible to decide whether the resting stage was prolonged or whether cells were prevented from dividing again . high power phase - contrast cinemicrography . the results have been reported elsewhere by hughes ( 1950 ) , and i shall only briefly summarize them here . 
with dilute solutions a large proportion of cells are prevented from entering mitosis , but no pycnosis or vacuolation appears . proand metaphase abnormalities this effect is exerted mainly during interphase . are conspicuous and anaand telophase abnormalities rare during the first 24 hours , anaphase abnormalities increasing after this period . 
the duration of the first two phases is significantly prolonged in some cells . cultures recover from these effects when transplanted into a fresh medium after 48 hours and hardly any residual effect can be detected . 
the nature of the s35 substance . the presence of s35 in the cytoplasm of myeloid cells after culture in s35 sulphate was all the more interesting since most mammalian cells will not utilise experiments were designed to obtain information on the nature of sulphate . the s25 substance in the myeloid cells . 
the summarised findings are presented in table i . ( 1 ) since 2 - 3 hours ' washing of the slides in running water , or 1 hours ' incubation at 370 c . 
a search was therefore made for a sulphate compound in these cells . although most sulphates form an insoluble precipitate with barium , it has been reported that the barium salt of chondroitin sulphate is soluble in water it was thought that the s35 in the cells might ( bray , gregory and stacey , 1944 )  . be in a form related to the chondroitin sulphates , therefore experiments were carried out to test the barium solubility of the su compound in the cells . both 1 m and 0 - 1 m ba ( oh ) 2 removed all the cells from the slides , but this could be prevented by m.aking up the ba ( oh ) 2 solutions in 10 per cent formalin . the morphology of the cells on the slides thus treated was unaltered , and it was found that 15 minutes ' treatment with 1 m or 0 - 1 m ba ( oh ) 2 formalin at 20 c . removed all isotope from the cells . formalin alone did not appear to remove any s35 . it had to be ascertained whether the effect of ba ( oh ) 2 was a specific ba effect slides subjected to distilled water alkalinised with or due to the alkaline ph . nh3 to ph 9 - 10 for 15 minutes at 200 c . 
for one hour or longer . that the s35 substance is not closely related to hyaluronic acids . ( 6 ) no parallelism could be detected between the behaviour of the s35 substance and those polysaccharides and other substances which give a positive hotchkiss reaction ( periodic acid schiff reagent )  . 
for 1 hour , the s3 substance was not . all hotchkiss - positive substances ( fresh human saliva , 1 hour at 370 c . ) , but it did not affect the isotope content of the cells . 
the uptake of methionine s35 . at the beginning of the experiments it was considered to be unlikely that s35 administered as sulphate to the culture medium would be transformed by the cells to sh groups . 
oliver s35 sulphate administered in vivo to rats has been shown to be taken up into the chondroitin sulphate of the growing cartilage ( dziewiatkowsky , benesch and benesch , 1949 ; dziewiatkowsky , 1949 ; 1951a , 1951b , 1952 )  . irrespective of whether sulphate or sulphite s35 compounds were given to rats in vivo , activity this finding has was found in the bone marrow by singher and marinelli ( 1945 )  . been confirmed by dziewiatkowsky ( 1949 , 1952 ) using whole bone autoradiographs and it was thought not to be chondroitin sulphate , but to be inorganic sulphate this sulphur after the first 30 minutes sulphur which is precipitated by ba ( oh ) 2 . of administration , is incorporated into a more complex compound from which the sulphur is slowly removed . the s35 substance in the myeloid cells of the bone marrow cultured in vitro it is possible that the dose of s35 sulphate given is removed by barium salts . to the rats by dziewiatkowsky was too small to be detectable in whole bone autoradiographs in the acid formalin fixed bones ( 5 / tc . / 7 - day - old rat in one series and 1 - 25 , tc . / 7 - day - old - rat in the other series of experiments )  . at this stage of the work it is probably too speculative to attempt to correlate the specific s35 sulphate uptake of the myeloid cells with the specific action of myleran ( 1 - 4 dimethanesulphonyloxybutane ) on the myeloid cells . 
raven. from the royal cancer hospital ( free ) and the gordon hospital for diseases of the rectum and colon . received for publication march 20 , 1948 . a study of the literature concerning malignant disease of the heart teaches that whilst primary tumours are rare , secondary deposits are not infrequently found . 
the following figures are illustrative . scott and garvin ( 1939 ) , in a series of 11 , 100 autopsies , including 1 , 082 performed in cases of malignant disease , reported secondary malignant disease as follows - heart , 79 cases ( 7 * 3 per cent ) ; pericardium , 61 cases ( 5 7 per cent ) ; heart and pericardium , 140 cases ( 12 * 9 per cent )  . willis reported an incidence of 6 - 2 per cent ; burke , 4 2 per cent ; helwig , 0 9 per cent ; pollia and gogol , 2 per cent ; lymburner , 0 6 per cent ; and symmers , 1 6 per cent . the subject is of more than academic interest , for with a better understanding it may be possible to establish a diagnosis during life in a greater number of patients , and the institution of certain forms of treatment , even though these are of a palliative nature . 
the symptomatology will therefore be reviewed , and attention drawn to the electrocardiographic findings in these patients . this paper is based on a series of 51 cases of secondary malignant disease of the heart which were collected at the royal cancer hospital from the autopsy records for the years 1930 to 1945 inclusive . 
the pericardium is usually involved and various types of disease are described . focal collections of carcinoma cells may occur in the epicardial fat , the cells being transported along the dilated lymphatics . in other cases the pericardium is studded with nodules of growth , whilst a third variety consists of diffuse pericardial infiltration , and this process may extend into the pericardial fat . there may be commencing infiltration near the commencement of the great vessels . another variety comprises flat plaques of growth embedded in the pericardium . in a number of cases there is combined involvement of the pericardium and heart muscle . 
tumour cells were seen in the lumen of a small arteriole ; obviously the disease in the heart was conveyed by the blood stream . in another case nodules of growth were found in the muscle of the right auricle , left ventricle and left auricle ; some of these were situated beneath the endocardium and growing into the auricle . 
the microscopic picture was similar to that of the primary skin tumour . in the third case an amelanotic nodule was present in the upper and posterior part of the left ventricle , from which more extensive spread had occurred into the heart muscle . moragues ( 1939 ) reviewed the subject of cardiac metastases from malignant melanoma and found reports of 23 cases in the literature , to which he added 4 in one of these cases there were signs of cardiac involvement ; personal cases . a loud systolic murmur was present in the pulmonary area , caused by a large tumour mass which almost occluded the pulmonary orifice . the spread of malignancy to the heart . this occurs by the usual four methods , namely , haematogenous , lymphatic , in this combined haematogenous and lymphatic , and by direct extension . series of cases there was definite evidence of all these modes . 
any subsequent abnormality which is noted can be compared with this initial investigation and inferences drawn . in cases with tumours of the heart , carnot and lambling ( 1928 ) have described a clinical syndrome which resembles that of subacute bacterial endoapart from this group of cases , attention is called to certain symptoms carditis . and signs which suggest cardiac involvement in patients known to be suffering from malignant diseases , especially of those organs which are recognized to give rise to secondary cardiac deposits . dyspnoea , tachycardia and cardiac irregularity are frequently outstanding symptoms , the irregularity being of the nature of either auricular fibrillation or auricular flutter . 
the symptoms may be correlated with the location of the tumour in the heart , causing heart block , or due to a pericardial or pleural effusion . it must not be assumed , however , that evidence of pericardial disease in a patient with malignancy is pathognomonic of involvement of the pericardium ; acute pericarditis may occur in the advanced phase from other causes . 
amongst important signs are those of cardiac enlargement and dysfunction , impaired resonance of the chest , the presence of abnormal breath sounds and added sounds . cyanosis may be present and the signs of cardiac failure . in the presence of this symptomatology certain investigations are carried out . 
when a pericardial effusion manifests itself , paracentesis is performed and cytological examination of the fluid is made . in a number of cases malignant tumour cells will be demonstrated . radiological examination of the heart , including tomography , is regarding the electrocardiographic out . findings , the case reports in the literature do not show uniformity ; the results vary according to the position of the tumour in the heart . siegel and young ( 1933 ) , dealing with this aspect of the subject , call attention to the work of lloyd ( 1929 ) , who published the first electrocardiogram in a proved case of tumour of carried r . 
the t waves in leads 1 and 2 were slightly diphasic . had been given before the patient was admitted to hospital , which may account siegel and young ( 1933 ) reported the for the abnormality of the t waves . findings in a case of metastatic sarcoma of the myocardiuthe t waves were inverted constantly in all leads , and there was no significant change daily . 
when the primary tumour is known to be radiosensitive , high - voltage x - irradiation may prove of value in the diagnosis in these cases clinical of metastases in the heart when enlargement is present . and radiological evidence may be forthcoming of a marked reduction in the size of the heart and the disappearance of the pericardial effusion . shelburne and aronson ( 1940 ) report the effects of high - voltage x - irradiation in a patient with metastases in the heart and pericardium from a primary myeloblastoma in the frontal bone . 
1. received for publication january 21 , 1948 . surgery in the form of the so - called radical operation is in general at the present time the principal weapon in the treatment of carcinoma of the breast . what it can achieve and its limitations are now fairly well established . 
thus it is known that if a patient with carcinoma of the breast has microscopical invasion of the axillary glands , the strong probabilities are that the disease has passed beyond the local area and that the patient will sooner or later succumb it is to the disease , although there will be a minority of fortunate exceptions . also known that if the axillary glands are not invaded the chances that the patient will be cured of the disease are appreciably increased . 
of particles of 3 diameter or less during a 6 - weeks period : seven rabbits survived the injections for 7 months or more , and all developed malignant osteosarcomas , often with multiple primary sites . 
 we have repeated these experiments , using zinc beryllium silicate and beryl lium silicate and confirm the findings of gardner and heslington ( 1946 ) , although the proportion of survivors developing tumours is less in our series . 
x - ray analysis has shown that zinc beryllium silicate is really a solid solution of z11iisio4 and be2sio4 an analysis of the zinc beryllium silicate used in experimental groups b and c ( table i ) gave a composition zno 67 per cent , sio2 31 per cent , beo 2 per cent . 
the complex injected in experimental group a ( table i ) contained manganese , and had a composition zno 67 per cent , sio2 28 per cent , beo 2 per cent , mno 3 per cent . 
 examination of the tissues of animals dying immediately after injection and between 14 and 83 weeks after the injection of the silicates has shown the presence of silicate particles in the lungs , spleen and liver of all injected animals . 
the macro phages of the spleen first form giant cells of the foreign body type and even of the langhans type , but later the particles are contained in large syncytial masses , which show up to 100 nuclei in a single section . 
for some months the particles are present in isolated kupffer cells , but 3 to 4 months after injection the kupffer cells have increased in size and number to form cellular masses that fill and often distend the sinusoids . 
 the nodules are present in all injected animals whose bones have been searched for them , and in many cases are not associated with any other abnormality , either histological or radiological . 
these : findings correspond closely with those for rabbit 4 , where consideration of histological material in conjunction with radiographs leads to the conclusion that the radiographic appearances result from occupation of the marrow cavity by ossifying tumour tissue . 
histological examination of the femoral shaft shows a complete replacement of the normal marrow by tumour tissue , quite comparable to that seen in more advanced lesions in other animals , but not yet expanding the periosteum or causing erosion of the cortical bone of the sha part of the tumour is bony , part cartilaginous , while some areas consist merely of anaplastic spindle - celled tissue . 
numerous fat cells are scattered through the area , and the tissue varies from an almost acellular mass of fibres to a tissue composed largely of rounded and elongated fibroblasts . 
5 shows such an area , where a network of recently - formed bone - trabeculae is present , and where the osteoblastic cells covering the surfaces of the trabeculae are linked to the intervening fibroblasts by numerous intermediate forms . 
on the left side of the bone a few areas show a similar pattern , but there is also some more diffuse aggregation of radio - opaque material , corresponding to the formation of calcified cartilage by the tumourtissue . 
 in the lower part of each femur the marrow is completely replaced by a mass of bone - forming tumour tissue , which has begun to extend into the haversian canals of the dense cortical bone . 
some areas consist entirely of cartilaginous tissue , others show extensive osteoid and bony differentiation , while in some places the two tissues merge into a composite " osteochondroid " pattern . 
in several situations this was beginning to invade the dense cortex of the bone concerned , and to expand the covering periosteu in this animal the body of one lumbar vertebra contained a small rounded area of calcifying spindl~ - celled tumour tissue , 2 m in diameter , sharply demarcated from the surrounding normal marrow . 
this suggests that a continuous process is concerned in the development of frankly malignant tissue from the earlier pre - invasive lesion seen , for example , in the humerus of rabbit 4 . 
of soluble berylliu treatment of the refractory beryijium silicates with n , 100 hydrochloric acid produces a 10 to 20 - fold increase in the proportion of soluble beryllium in the aqueous suspension . 
 when stained by the method developed by denz ( 1949 ) for the histochemical detec tion of beryllium these sections showed that some soluble beryllium had left the necrotic area and stained the surrounding fibrous tissue faintly an_d diffusely . 
while the fully _developed tumours present a very different appearance from the medul lary bone formation that has been described as an early stage of malignancy , all stages of transition between the two can be traced . 
it is suggested that these indicate a continuous process of transformation from the early medullary : fibrosis to the later obviously malignant lesions , but this is only the interpretation of a number of morbid anatomical observations . 
 the relationship between the small nodules which are the first change seen within the bone marrow and the subsequent : fibrosis and malignant change is uncerta the nodules produced by the silicates containing beryllium and those produced by the zinc silicate are indistinguishable by the usual histological methods . 
it seems clear , however , that it is the presence ofthe beryllium within the nodule that is in some way responsible for the progressive changes that lead eventually to malignancy . 
although the beryllium silicates are considered to be insoluble , the observations on material injected intradermally into a rabbit showed that beryllium can be liberated from the particles and can diffuse into the surrounding tissues . 
 _therefore , if beryllium is to be held directly responsible for the tumours , it is much more likely that this beryllium is liberated from deposits in the marrow rather than derived from more distant deposits . 
the possibility that the silicate may play some part in the development of the tumours is excluded by the fact that gardner and heslington ( 1946 ) produced tumours with beryllium oxide , and more recently barnes ( 1950 ) has reported that two rabbits that received intravenous injections of a suspension of beryllium metal particles have developed characteristic sarcomas . 
 it is also apparent that the tissues themselves must contribute a factor , because similar nodules in the liver and lungs arouse very little : fibrous tissue reaction , while in the spleen : fibrosis and atrophy may go to extreme lengths without showing evidence of malignant change . 
 since this paper was submitted one further rabbit has died with a sarcoma of the pelvis 30 months after the last of a series of injections of zinc beryllium silicate . 
 the materials used in these experiments were supplied to us by the research laboratories of the general electric company , wembley , to whom we would like to express our thanks . 
kreyberg spondence is established between the patient group and the control material with regard to such factors as age and sex composition , distribution of broad occupational groups and place of residence , which may influence smoking habits and / or lung cancer frequency , and a large number of factors clearly may be considered irrelevant , a field of uncertainty of considerable extent still remains . two points of practical importance emerge from the above discussion . 
the first is that control material consistin - g of non lung cancer cases among patients in a chest department , or even among hospital patients generary , may introduce a bias if , for instance , the factor " visiting a chest department for reasons other than lung cancer " - present in a control material but not among the lung cancer patients - is associated with the level of tobacco smoking . there may thus be a tendency towards excessive smoking in such a control material , or patients in chest departments may on the contrary tend to be persons whose reaction even to mild forms of chest trouble is a visit to the hospital , and who are careful if both these tendencies not to expose themselves to irritants sucli as tobacco . are present among the patients , they may neutralize each other , but the net result will obviously depend on their relative occurrence in the control material . similar objections may be brought against the use of hospital patients generally this point has been stressed by mirs and porter ( 1953 ) as control material . who believe that the bias probably wfll obscure an excess of smoking among lung cancer cases . 
at least , it is not established that hospital patients do not differ systematically from the general population with regard to smoking habits . the second point to be made is that a careful survey of all possible cancer producing factors must precede the instigation of a control study , and that prehminary surveys are needed to estabhsh the relationships between these factors and the level of tobacco smoking . there is thus a priori reason to consider the need for relevant definitions and differentiation of occupational groups among the cancer patients as well as in the control material , in view of the frequently indicated possibilities of specific occupational hazards with respect to lung cancer . assume , for instance , that a particular type of industrial occupation has a definite but unrecognized excess incidence of lung cancer , and that the carcinogenic agent is connected with the nature of the work . 
assume further that this particular occupation also is associated with an excess of tabocco smoking , because of higher pay , better opportunities of smoking during working hours , psychological stress or other causes . if the occupational selection criteria are such that this occupation does not exphcitly constitute a stratum in the control material it may be under - represented in a control material with random selection within each stratum , and the controls may , for the separate occupational groups and in toto , show a lower smoking level than the cancer such a difference will clearly be misleading for an evaluation of patient group . the carcinogenic effect of tobacco smoking . if , on the other hand , the particular occupation in our example is associated with an exceptionally low smoking level , a possibly significant excess smoking in the cancer patient group may be obscured . 
kreyberg composition of tobacco consumption are available only after 1927 . since then , tobacco smoked , i.e. , cigars , cigarettes and pipe tobacco , has accounted for a steadily increasing proportion of the total tobacco consumption at the expense of chewing tobacco and snuff , as shown in fig . 
the amount smoked is here calculated as production plus imports minus exports of cigars , cigarettes and pipe tobacco . these changes will year to year inventory changes have not been corrected for . be small , however , and without influence on the trend even if the vearlv figures may contain erratic deviations from the true consumption level . it should be permissible to assume that chewing tobacco and snuff played a greater r ' ole before 1927 . 
even if some of the chewing tobacco in fact has been smoked in pipe , it is reasonable to assu ' me that the amount of tobacco smoked , per person 15 years and older , has increased to some extent during the whole period from 1901 to 1940 . 1800 1600 1400 1200 1000 11 1% in600 1928 year fig . 
2. - consumption of smoking tobacco in granis per person 15 years and older . 38 39 after the last world war the yearly amount of tobacco smoked , i.e. , cigars , cigarettes and pipe tobacco , has reached a level of approximately 1650 g . 
3 for 1928 - 29 , 193 7 - 39 and the post - war years . the black parts of the columns represent the proportion of ready made cigarettes , which was 34 - 7 per cent in 1928 , rose to 42 - 9 per cent in 1947 and has since declined to 35 - 8 per cent in 1951 . 
patients , ear - nose - throat department , the rikshospital ( whole country ) kongsberg is a smar industrial town in central southem nor - way , s smar industrial and mining commuiiity ( iron - ore ) in the extreme north . varanger ( kirkenes ) a in the groups 1 , 3 , 4 and 5 among the males and 1 , 2 and 3 among the females the number of returned questionnaires falls substantially short of the total number of individuals in the groups selected . 
the age distribution of the separate groups is given appendix tables iii and iv . incidence of each of the forowing were computed . each of the above - mentioned groups were divided into age - classes with a for each group and age - class the percentage for males : 1 . 
4 is shown the range of variation found for the frequency of smokers in each age - class among the groups investigated . it will be noted that this range is fairly narrow , especially in the age - class 45 - 54 years in which the lowest percentage smokers ( found among the visitors at the oslo first aid station ) is 83 - 5 and the highest ( among industrial workers , oslo ) is 91 - 9 . 
the latter group , on the other hand , reaches its highest frequency at a i ' ater age than most of the other groups . generally the percentage smokers is lower among industrial workers in kongsberg , than in the other groups . per cent pure cigarette smokers . 
5 we find a very wide range of variation for the occurrence of pure cigarette smokers in the material , especially in the lower age - classes . among the industrial workers in kongsberg in the age - class 25 - 34 years only 28 - 4 per cent smoke cigarettes exclusively , whereas 75 - 9 per cent of their colleagues in s6r - varanger do so . 
6 is similar to that found for the percentage pure cigarette smokers , but the level has been shifted upwards and the range is a little less wide , corresponding to the tendency for the cigarette - pipe smoker combination to be more frequent in groups with relatively few pure cigarette smokers than in those with a high pure cigarette smoker percentage . 
8 the range of variation in the percentage medium and heavy smokers is large in all age classes , but the frequency does in no case exceed 50 per cent . 
12 is very rare among women , occuriing only among physicians and the patients and followers at the oslo first aid station , in the age - classes 35 - 54 years , with frequencies ranging from 1 - 4 per cent to 2 - 3 . per cent heavy and medium smokers . 
how much of this variation is real , i.e. , caused by actual differences in smoking habits in the groups under consideration , and how much may be caused by a systematic bias in those groups whose degree of co - operation in retur ' n ' mg questionnaires was low , cannot be decided on the basis of available inforrnation . 
the question is of considerable interest however , since for most of the smoking habit criteria , the range of variation among males would narrow considerably if the figures for the industrial workers in kongsberg are left out . this group comprises questionnaires from only a part of the total number of workers in the arms factory selected for analysis , and ff it could be shown that the degree of co - operation in this group is systematically related to smoking habits , the deviations shown would not reflect a true difference in smoking habits between these factory workers and the other groups . there are , however , certain indications that part of the difference at least between the kongsberg workers and the other male groups is real . first of all the percentage smokers in this group ( appendix table v ) are not substantially below those of the other groups . 
even if there is a tendency for smokers to be under - represented among those workers who answered the questionnaire , such a bias can not account for the very low percentages pure and pure and mixed cigarette rsmokers found in the kongsberg group , and is not likely to expla ' entirely the low percentages found for the quantitative criteria ( per cent heavy and per cent heavy and medium smokers )  . secondly , groups other than the kongsberg workers have failed to co - operate fully , without any resulting systematic deviation from the complete groups . 
an explanation of the result for the kongsberg group in terms of a systematic bias , would thus imply that this bias was a characteristic of the kongsberg workers but not of the others . thirdly , the material from the male physicians seems to indicate that there is no strong tendency that individuals who fail to fir a questionaire deviate appreciably i their smoking habits from those who co - operate readily . 
a new questionnaire was sent out approximately a year later with an appeal to those who had not answered previously this appeal resulted in 601 new questionnaires which were to do so now . analysed separately , however , the two groups showed added to the old material . the following figures for the separate smoking habit criteria . there is thus cause to believe that the range of variation found in the material largely reflects real differences in smoking habits . special menti ' on may be made of the male group of patients at the rikshospital ear - nose - throat department which displays exceptionally low percentages heavy and heavy and medium smokers ( both generally and cigarette ) in the lower age - classes and rather high percentages in the higher age - classes . the material is , however , too small to permit any conclusion as to whether or not this reflects a characteristic pattem in this group . conclusion as was pointed out initiahy , the present study has been undertaken in order to provide background information on factors which must be taken into conh . 
the present study may serve as a basis of comparison with the smoking habits of lung cancer patients , in the sense that findings generally outside the range of variation exhibited by the present material would be indicative of real deviations in the smoking habits of lung cancer patients , but quantitative statements about differences found cannot be inferred . the low frequency of smokers in the higher age - classes among most groups of women may indicate that the increasing trend in total tobacco consumption h . 
it would be wrong to give the impression that undesirable sequelae are common , yet such complications as wound sepsis , necrosis of the skin edges and a poor functional result are still seen with greater frequency than one would expect following an operation which has been abundantly practised by innumerable surgeons all over the world for over half a century . 
these particular sequelae are essentially a reflection on the judgment or the executive skill of the operator and not upon the operation itself , because with care they need not happen . 
furthermore , such indifferent results become known , and because they lose nothing in the telling may have a serious deterrent effect upon patients contemplating advice about a newly acquired lump in the breast . 
it is to be remembered that we are operating under almost ideal conditions - the patients are constitutionally well and often near the prime of life , the anatomy of the area is normal and not distorted as it might be , and there are none of the embarrassments associated with operations within a body cavity . 
a very high degree of technical excellence should therefore be our aim , both in regard to the thoroughness of the dissection which has as its objective the extirpation of the disease , and in regard to the care with which this is carried out , which can so much determine the degree of ultimate functionaf disability . 
 there are three features of the " skin short " case which need some explana i will call them ( i ) anticipating the gap , ( ii ) siting the gap , ( iii ) covering tion . 
riddell surgery - may be influenced ; second , the surgeon is forewarned , and so can avoid being surprised into an awkward situation at the end of a long operation . 
 an assessment - an estimate - should be made in all new cases of cancer of the breast of the amount of skin that will be left for closing the wound after the breast and tumour have been removed . 
it will be found that patients fall into two categories : ( 1 ) a larger group in whom it is judged that it will be possible to approximate the skin edges in the usual way without tension . 
h we remove too little skin , secondary nodules will appear for certain and quickly ; if we remove a more generous amount - - as we must - we shall have to be prepared to deal with a gap . 
 in these patients two alternatives are open to us : either we can proceed to radical mastectomy , skin graft the resulting gap , and hope that the skin covering it will heal in a reasonable time and so allow early post - operative irradiation , or we can anticipate the probable delay in healing by giving the x - ray treatment before the operation . 
 personally in this small group i prefer to give the x - ray treatment first , because in practice unfortunately every skin graft does not take uniformly , so that a proportion of cases are left to heal - at least in part - by granulation , and this takes time ; indeed , sometimes so much time that post - operative x - ray treat ment may be delayed to a point where its usefulness is open to question . 
for this reason it is suggested that if by careful pre - operative clinical assessment we can anticipate and so forecast such a defect arising , we should consider giving the x - ray treatment before the operation . 
the use of pre - operative irradiation does not in any way absolve the operator subsequently from still adhering to the principle of excising a wide area clear of the growth . 
this patient was treated by pre - operatilre irradiation followed by radical mastectomy with an immediate skin - gra the satisfactory functional result can be attributed to ( i ) adoption of the " arm raised " position before approximation of the skin flaps , ( ii ) the early recognition of the inevitability of " a gap " in this type of case and of the need for a skin - gra fro . 
2. - full range of movement : the " arm raised " position is the most delicate test of function at the shoulder following mastectomy ; six months should be allowed after the termination of all treatment for the skin to regain its suppleness beforp 8 - ing function ; inability to raise the arm vertically after such an interval must be regarded as an imperfect functional result . 
3. - llarginal flap necrosis : the illustration shows an area of skin loss as a result of damage to the blood supply of the lateral flap during its elevation . 
at the same time it is not vital to graft ; what is vital is that a gap should be left in a skin short case ; whether a dressing of skin is put on that gap or not is almost a secondary consideration , although skin is very clearly to be preferred to scar tissue if the gap is a large one . 
 the time lo gra the decision as to whether the graft is applied at the time of the mastectomy or not depends solely on the condition of the patient at the end of the operation . 
 h this is unsatisfactory , as it may be in an elderly patient , no harm is done by leaving a raw area and grafting early in convalescence , usually at the time of the first major dressing . 
 if , in addition , we have made our pre - operative reconnaissance , the procedure is robbed of its only disagreeable feature , the element of surprise , since a donor area will have been chosen and prepared and the few special instruments and dressings will be immediately available . 
this accident most commonly occurs as the dissection approaches the anterior border oflatissimus dorsi , which corresponds with the deepest and darkest part of the wound ; it is usually due to hurrying this part of the reflection in a field obscured by haemorrhage ; the blood 811pply may also be cut off from a portion of the flap by the use of tension sutures and with the same result . 
riddell displacement of sk in the second category the skin is not lost in the sense that it is destroyed , but is lost by displacement , because skin is borrowed from the axilla and upper arm to close the axillary part of the wound . 
 ( 2 ) slide the skin of the lateral flap well up into the axilla ; by making use of the longer contour of the lateral flap in this way an adequate supply of skin in in suturing the flaps together exactly opposite points on the axilla is assured . 
 in other words , lend skin from the lateral flap to the axilla ; do not borrow it from the axilla and upper arm by bringing the arm down to a right angle or less . 
 i should perhaps add that in my experience functional disability at the shoulder is not related to loss of the pectoral muscles ; indeed , it can be quite severe following a local mast.ectomy , and is not related t - 0 failure to employ early fig . 
the drawing shows the correct position of the upper limb before closing the wound ; the skin of the lateral flap should be pushed well up into the axilla before suturing ( arrow )  . 
in a series of cases examined in which the subscapular nerve had been divided , no functional disability could be found by comparison with control cases and with the opposite side , although , of course , there was a positive r.d. 
the aim is to display the anterior border of the latissimus dorsi muscle , and in " skin short " cases to mobilize the lateral flap still further by carrying the dissection backwards for two or three inches beyond this point , keeping on a plane buperficial to the muscle . 
the aim is to raise a flap of even thinness , but if by a careless stroke of the knife the flap is cut too thin , the blood supply will be damaged and the whole course of convalescence unnecessarily prolonged . 
h too thick a flap is raised the dissection may in error proceed on the deep face of latissimus dorsi into the space between this muscle and the serratus anterior , a space which is filled with large veins . 
h , on admission , the patient is severely anaemic , blood should be given , but let the transfusion be given before the operation ; it can be supplemented by plasma or other blood substitute during the operation if necessary . 
this is a partial contradiction of views ex pressed earlier in my experience ( riddell , 1948 ) , and is based on the fact that blood transfusion to an unconscious patient carries with it an extra hazard - slight though it may be - for the patient cannot proclaim against the blood if it is incom patible , as would be possible if she were conscious . 
the towelling of the operation area should be so arranged , by placing a towel behind the patient 's back , that there is no unprotected area on the flank from which the main wound might be contaminated ; hot wet packs , which so quickly become cold wet packs and chill the patient , should only be used for haemostatic purposes at the end of the operation ; dry hot packs 296 v . 
 drainage should never be employed through any part of the original incision , because it can so easily lead to cross infection of the main length of the wound ; it is best carried out through a separate stab incision in the lateral flap , pre ferably well clear of the hair and sweat - bearing skin of the axilla . 
lastly , let us banish for all time the use of tension sutures , and above all the expression f 10 . - the composite dra ' lring illustrates ( a ) the position of the leg for cutting an imme it is a sound precaution to towel up all " skin - short " cases with the diate skin - gra donor area prepared and &ec8111111 > le . 
functional disability usually takes the form of restricted movement at the shoulder and is doubly undesirable , since it not only seriously reduces the range of w ! efo1ness of the limb concerned , but aggravates by constant reminder the psychological trauma resulting from the operation . 
the methylcholanthrene was introduced into average age of the mice was 6 months . the prostate gland in the following manner : under general anaesthesia , a median abdominal incision was made , exposing the prostate lobes . 
8. - the same after 3 weeks ' time . 10 or more layers deep , keratin pearl formation still absent . cells acquiring more pronounced squamous metaplasia . development of stratified squamous epithelium , h . 
they varied between i to 3 of an inch in diameter and frequently more than a single prostate lobe was involved . a tumour of average size is shown in fig . 
7. received for publication february 7 , 1947 . it is a widespread doctrine among students of cancer that any tissue or organ capable of cell division may be the site of a malignant neoplasm , but it is well known to clinicians that certain tumours , theoretically possible , do not in fact occur . 
the most striking example of an organ which never gives rise to a neonotwithstanding the fact that mitoses occur in the lens plasm is the lens . throughout life , having been seen even in the lenses of patients 80 years old , no tumour of the lens has ever been discovered . the lens is an entirely epithelial structure embryologically derived from the surface ectoderm , devoid of blood supply and enclosed in a semi - permeable although mammalian lenses are enclosed membrane , the hyaline lens capsule . during embryonic life in a capillary net ( the vascular lens capsule ) this does not constitute a blood supply , since the vessels do not come in contact with the lens in the majority of vertebrates cells , being always outside the hyaline capsule . the lens can therefore be looked even this embryonic vascular capsule is absent . on as a segregated group of specialized epithelial cells growing and differentiating in a closed system , separated alike from the blood - stream and from the surface of the body . 
7. received for publication february 7 , 1947 . it is a widespread doctrine among students of cancer that any tissue or organ capable of cell division may be the site of a malignant neoplasm , but it is well known to clinicians that certain tumours , theoretically possible , do not in fact occur . 
the most striking example of an organ which never gives rise to a neonotwithstanding the fact that mitoses occur in the lens plasm is the lens . throughout life , having been seen even in the lenses of patients 80 years old , no tumour of the lens has ever been discovered . the lens is an entirely epithelial structure embryologically derived from the surface ectoderm , devoid of blood supply and enclosed in a semi - permeable although mammalian lenses are enclosed membrane , the hyaline lens capsule . during embryonic life in a capillary net ( the vascular lens capsule ) this does not constitute a blood supply , since the vessels do not come in contact with the lens in the majority of vertebrates cells , being always outside the hyaline capsule . the lens can therefore be looked even this embryonic vascular capsule is absent . on as a segregated group of specialized epithelial cells growing and differentiating in a closed system , separated alike from the blood - stream and from the surface of the body . 
by carefill dissection of the eyes it is possible to get the lenses in their hyaline capsules completely free from vascular capsule or uveal tissue . these lenses were inserted under the skin of the flank of mice of the same inbred strain together with methylcholanthrene . in some cases the hyaline capsules were ruptured and the lenses mixed with a few crystals of methylcholanin others the unruptured lenses coated with a solution of the threne . in others again teased lenses were mixed carcinogen in oil were used . with methylcholanthrene in solution in equal parts of soft and liquid the exact method employed did not appear to be important , paraffin . two of the tumours being obtained with a solution of 1 mg . 
the tumours appeared between two and three months after implantation . characteristics of tumrnours of lens epithelium . the tumours are anaplastic carcinomas possessing certain characteristics suggestive of their origin from the subcapsular epithelium of the lens . 
a brief consideration of the normal structure and behaviour of this in mice is a necessary preliminary to the study of the tumours . the normal lens and its epithelium is seen in fig . 
the first stage of this differentiation is the lengthening of the cell and the displacement of the once this has occurred the cell cannot divide again , but nucleus to one end . proceeds to complete differentiation into a lens fibre , the nucleus of which evenfig . 
4 and 5 show results at three and at two days . thle ruptured capsule is in culture of the whole lens of a late mouse embryo . the centre of the explant and is surrounded by degenerating lens fibres . 
the cells are large , with voluminous spherical or oval nuclei , showing one or more nucleoli and a prominent reticular chromatin in the young cells the nucleus is central , in structure . the older cells it moves to the edge of the cell just before becoming pyknotic . metastases occurring in the inguinal lymph nodes show the same structure , but with less necrosis . 
6 and 7 is apparent . extending edge showed fibrillar outgrowths somewhat similar to those described this by kirby in tissue cultures of chick lenses . fixed and stained preparation of a 5 - day tissue culture of the same tumour also these are seen in fig . 
 the compilation of this paper was prompted by the idea that some investi gators of cancer as it occurs in man do not know the valuable material which is contained in the publications of the general register office , while even those who are acquainted with this literature may find some use for a list of the collec tions of data about cancer which it contains . 
 the material dealt with in these publications consists of the death certificates from england and wales , considered in association with the data on population , civil state , occupation and locality obtained at the census of 1911 , 1921 and 1931 , together with population estimates for intervening and subsequent years . 
the certificate does not state , and is not intended to state , how long the deceased had followed the occupation named , and had lived at the home address given ; this information could be obtained only by inquiry into individual cases . 
the sources of such errors have been discussed in two earlier papers ( henry , kenna way and kenna way , 1931 ; ~eimaway and kennaway , 1936 )  . 
 the _decennial supplements for 1921 and 1931 contain data collected at the census of those years , and were published in 1927 and 1938 respectively ( registrar general , 1927 , 1938 )  . 
_they contain a large amount of tabulated material for periods adjacent to the census , namely 1921 - 23 and 1930 - 32 ; the scope of those tables , in so far as they are concerned with cancer , is summarized in tables i and ii . 
the 240 , 726 deaths of all married women during 1930 - 32 were classified according to the husband 's occupation as stated on the death certificate , while 19 , 422 single women who died during the same period were classified according to their own occupations . 
the reasons for the association of the married woman with the occupation of her husband are that ( 1 ) " only about 10 per cent of married women were recorded as gainfully occupied at the census of 1931 , " and ( 2 ) some indication is obtained of the social , or occupational , nature of the mortality in the husbands ' occupation , "  . 
table ix shows a selection from the supplements for 1921 and 1931 of some very interesting - data for the incidence of cancer of various organs upon men and married women of the five social classes , and in the case of the men two periods ( 1921 - 23 and 1930 - 32 ) can be compared . 
a recent paper by swan ston ( 1950 ) on " the iron and steel industry " shows the use which can be made of the material in the decennial supplements . 
 the registrar - general publishes annually a " statistical review of england and wales for the year  . , " normally in two parts , namely , ( 1 ) text , ( 2 ) tables . 
the " text " now contains a section upon cancer consisting of a commentary upon the data which have been obtained during the year in question , and certain tables . 
this table provides material in answer to the question so often asked - " is cancer increasing ? " the comparative mortality index , which takes account of changes in the sex and age structure of the population , shows that the total mortality from cancer in england and wales has barely increased during the past twenty years . 
the distinction between the entry of " carcinoma " and " cancer " upon death certificates is probably of no value , but the separation of the two at any rate absolves the general register office from any responsibility for the distinction ( table lxxvi )  . 
 ( e ) by regions ( england and wales , greater london , rest of south - east , north , midland , east , south - west , wales ) , and by class of area ( county boroughs , other urban districts , rural districts ) ( table lxxvii )  . 
 such data for the total incidence of cancer must , of couj1se , be recorded , calculated and examined , but they cannot show the peculiar incidence of cancer upon the various organs , and in the two sexes , and in persons living in different areas , and various interesting changes may cancel one another and hence be lost in the totals . 
the great interest of these data is best made plain here by reproduction in table iii of a part of an example ( table lxxviiia , 1940 - 42 )  . 
 all sites lips tongue mouth tonsil pharynx jaw others total oesophagus stomach duodenum other small intestine caecum hepatic flexure , splenic flexure sigmoid flexure large intestine ( colon ) other and undefined intestine rectum ( not anus ) liver gall bladder and ducts pancreas peritoneum , mesentery , others other and unspecified digestive organs 89 , 902 606 2 , 254 703 534 1 , 008 748 529 6 , 382 4 , 498 20 , 778 129 155 860 418 2 , 157 8 , 801 228 10 , 365 2 , 581 703 3 , 267 4 , 053 147 232 199 250 females . 
 other female genital organs total total total total total breast scrotum prostate testis penis others kidney bladder , urethra , ureter : 163 155 6 , 055 339 457 7 , 009 409 3 , 360 3 , 769 147 174 606 623 593 667 219 312 755 2 , 877 202 3 , 834 5 , 482 721 6 , 416 12 , 619 4 , 952 1 , 281 6 , 248 20 , 049 107 184 173 183 107 265 386 162 510 705 499 550 1 , 114 312 1 , 557 1 , 869 452 458 185 the material contained in this table is very significant . 
the cancer problem in its simplest form is reduced to the question , why does a cell divide ? but no single universal " cause of cancer , " such as is announced from time to time , could , even if it were actually discovered , explain all the features of this table . 
the nature of cancer proceeds by means of the most refined cytological methods , there is scope for investigation of factors occurring in everyday life which may explain the 1rery peculiar sexand organ distribution of cancer . 
 breast total cancers of female reproduc tive organs other organs total cancers in females males exce811 in females 18 , 867 20 , 049 38 , 916 58 , 090 97 , 006 89 , 902 7 , 104 164 e . 
kennaway for instance ( table iv ) , the total deaths from carcinoma in males ( 89 , 902 ) and females ( 97 , 006 ) show a difference of only about 7 per cent , yet the latter total includes 38 , 916 deaths , or 40 .per cent of the whole , from carcinoma of organs peculiar to the female , among which organs the female breast , being capable o , f lactation , must for the present purpose be reckoned . 
this calculation illustrates the phenomenon of the " amount " of cancer in man , to which attention was drawn in an earlier paper ( kennaway and kennaway , 1937 )  . 
no better example has been given by later workers than that recorded by the dutch investigators snijders and straub ( 1924 ) in sumatra , who first described this numerical relation of total cancers in populations differing in habitat or in sex ( table v )  . 
 28 27 these figures show that in sumatran and european populations , in which the total incidence of cancer is about the same , the proportion of one form of cancer , in this case that of the liver , may be very different . 
 " there appears to be a general law that when in a given population the incidence of cancer in one particular organ is markedly increased as compared with another population , there is then a compensating decrease in the incidence of cancer in a number of the other organs " ( cramer , 1936 )  . 
 ( b ) the data shown in table lxxviiia and bare subdivided under 15 quin quennial or decennial age - groups from 0 - 5 to 85years ( tables lxxixa , b , e , d , e , f )  . 
thus in men aged 55 - 64 the mortality from cancer of the lip has fallen to 26 per cent of the initial figure , while that attributed to cancer of the lung has increased by more than 17 times . 
 1911 - 20 1921 - 30 1931 - 35 1936 - - 39 1940 - 44 1945 1911 - 20 1921 - 30 1931 - 35 1936 - - 39 1940 - 44 1945 1911 - 20 1921 - 30 1931 - 35 1936 - - 39 1940 - 44 1945 the exact comparison of the prevalence of cancer , or of any form of cancer , at different periods , requires standardized death rates owing to the continual increase in the numbers of older persons , who are of " cancer age . " such data are given at intervals in the statistical reviews ( text ) , and most recently in table lix in the review for 1938 and 1939 ( registrar - general , statistical review ) , which records the standardized rates per million population for cancer of 27 sites in men and women separately in the periods 1901 - 10 , 1911 - 20 , 19.21 - 30 , 1931 - 35 , 1936 , 1937 , 1938 and 1939 . 
these figures for each one of the four most recent years are of especial interest because they show the present state of increase or decrease of the various forms of cancer . 
 in the table in question the great majority of the 52 sex - site combinations show a decrease , or are stationary ; the only quite definite increase is in cahcer of the lung and bronchus in both sexes . 
since 1942 standardized death rates have been superseded by comparative mortality indices , which compare the death rate in each year with that of 1938 , after making allowance for changes in the proportion of the population at different ages . 
for a number of sites of cancer since 1933 have been published in the medical tables volume of the statistical review ( table viii ) for each year since 1942 . 
 ( d ) the deaths from cancer of certain sites ( mouth and oesophagus , stomach and duodenum , respiratory system , breast , uterus , other sites ) per 1000 for all sites in men and women at certain ages , in certain regions and classes of areas named above ( table lxxvii ) during 1940 - - : - 42 and 1943 - 45 ( table lxxxi ) are set forth . 
 the cancers of the respiratory system show the greater liability of urban populations ( stocks , 1936 ) ; this portion of the tabl~ is of such interest that it may be reproduced in extenso here ( table vii , section a )  . 
if one recalculates the figures for the various districts on the basis that " rural districts " = 100 , whereby the data for the two periods 1940 - 42 and 1943 - 45 become more comparable , one obtains the figures shown in section b of the above table , which show a very close similarity between the two series for women , with the single exception of the figures for the south - west region . 
of course this result has no bearing on the accuracy of death certificates , but it does show that two sets of such certificates , gathered in a number of districts during two consecutive periods , give results which have a considerable uniformity . 
 when the mortality from any form of cancer , such as that of the lung , is higher in urban than in rural districts , one must consider whether the difference is due , not to the conditions of life in towns , but to better facilities for diagnosis , and a further extract from table lxxxi is of interest in this respect ( table viii )  . 
 males , 45 - 65 mouth and oesophagus , 1940 - 42 1943 - 45 stomach and duodenum 1940 - 42 1943 - 45 males , all agesrespiratory system females , 45 - 65 breast uterus 1940 - 42 1943 - 45 1940 - 42 1943 - 45 1940 - 42 1943 - 45 238 225 156 183 236 231 165 157 205 187 216 249 261 254 150 137 100 254 235 103 126 236 244 148 144 the diagnosis of cancer of the oesophagus , stomach and duodenum , breast and uterus may be by no means easy , yet these forms of cancer do not show the difference seen in cancer of the respiratory syste this last must be made up largely of cancer of the lung , and hence these data provide further evidence of a carcinogenic factor in urban environment . 
 the annual statistical reviews do not deal with the social and occupational incidence of cancer , as the occupational distribution of the population is ascer tained only at census periods . 
 in this summary of the annual and decennial publications of the general register office in relation to cancer one cannot of course refer to the numerous passages which treat of the material tabulated . 
 the decennial supplement for 1921 ( registrar - general , 1927 ) contains the first detailed study of the social incidence of cancer upon the various organs in men , which study developed from an earlier investigation of the incidence of cancer as a whole ( stevenson , 1923 )  . 
so far as is possible from the material available , class i purports to represent the pro fessional and generally well - to - do section of the population , class iii , skilled artisans and analogous workers , and class v , labourers and other unskilled callings , while classes ii and iv are intermediate , comprising occupations of mixed types , or types not easily assignable to the classes on either side . " the parts of the body affected by cancer were divided into two classes , namely : exposed sites ( buccal cavity , pharynx , oesophagus , stomach , larynx , skin ) , and other sites . 
 the mortality from cancer of the exposed sites increases from social class i to class v , while cancer of the other sites shows no such relationship ( table ix )  . 
 the author of the decennial supplement , 1921 , comments upon these data : " it thus appears that a large proportion , at least , of cancer mortality is of a highly preventable nature , for we must suppose that if the conditions of life of all sections of society could be assimilated to those of its upper ranks , mortality from cancer of the exposed sites would fall for all classes to the class i level . 
 the paragraph made up by these two sentences should be regarded as one of the classics of cancer research , for it brings carcinogenesis in man into relation with factors in everyday life which can be investigated , while the most refined methods of physics and chemistry are applied to the problem of cancer in general . 
 the most extreme instance of a social factor in the incidence of cancer appears in the case of cancer of the scrotum ( kennaway and kennaway , 1946 ) , which could in all probability be eliminated altogether by cleanllness , as is cancer of the penis by circumcision in infancy . 
 the figures ( table ix ) for cancer of the upper alimentary canal in males show a significant reduction in the steepness of the social gradient from 58 , 80 , 99 , 102 , 140 , to 63 , 80 , 97 , 109 , 129 ten years later . 
this may be due in part to " earlier or more effective treatment than before of cancer of the more accessible sites " in men of the poorer classes , as is suggested in the text , but probably also to the improvement of social conditions in other ways . 
the change has been chiefly in the cancers of the buccal cavity ( tongue , tonsil , pharynx ) , for cancer of the oesophagus shows no , and that of the stomach very little , loss of gradient . 
 the steeply graded figures for the larynx , in contrast to those of the buccal cavity , show no change , while those for cancer of the skin show a flattening which one would associate with improved personal cleanliness . 
 figures for the socia ] distribution of cancer in women in 1921 - 23 are not available , but the comparisons of those for men , and women , in 1930 - 32 are 170 e . 
 " of gastric cancer mortality can have little to do with the effects of occupation , and must arise from factors of selection , economics or environment which affect the wives of the men in occupational groups as much as they affect the men themselves . " cancer of the skin also affects men , and married women , of the the employment of a different social classes in much the same way ; "  . 
 proportion , largest no doubt in classes iv and v of married women in textile occupations , may be partly responsible for the mortality gradient for skin cancer . " no attempt is made here to deal with all the indications for inquiry which may be drawn from this table ; the subject is dealt with , and illustrated by graphs , in pp . 
cancers of the buccal cavity , and of the larynx , show a high incidence upon occupations associated with alcohol ( kennaway and kennaway , 1936 ; wassink , 1930 ; registrar - general , 1927 , appendix d ) ; the change in gradient in the former only might suggest that this is due to another factor , namely , better oral hygiene . 
 the lack of influence of social class upon the liability to cancer of the lung , together with the very considerable effect of urban conditions ( stocks , 1936 ; registrar - general , 1947 , table vii ) , suggasts some carcinogenic factor to which all classes are exposed ; owing to the mixing action of the wind there is less difference in the outdoor air breathed by different classes than in other social conditions such 1 , 1 , s food and cleanliness ( kennaway and kennawa.y , 1947 ) , and all classes seem to share in the increased use of tobacco , largely in the form of cigarettes . 
 a good example of the unique value of such studies of social distribution is given by cancer of the uterus , which was examined in this way for the first time in 1930 - 32 . 
thus , at ages 35 - 65 the rate in married women of class v is twice that of class i , and single women in classes iv - v show a mortality 44 per cent greater than that of classes i and ii . 
 thus in 1921 the ratio of registered to 100 calculated births for married males in the five social classes was 85 , 85 , 97 , 109 , 128 , and the social distribution of uterine cancer in married women might be thought to be due to the difference in fertility . 
 the data on the mortality from cancer in the last twenty years should yield very valuable information when correlated with the results of the census in 1951 , the first made since 1931 , in view of the considerable social changes which have taken place . 
 ( 1 ) the british empire cancer campaign has published in its 13th annual report a very elaborate study by stocks ( 1936 ) , il1ustrated by 17 maps , of the distribution of cancer of eight sites ( oesophagus ; stomach ; intestines ; rectum ; liver , gall - bladder and pancreas ; skin ; lung ; breast ) in both sexes at various ages in the counties and county boroughs of england and wales . 
the 14th report of the campaign records an extension of this study ( stocks , 1937 ) , with 7 maps , to cancer of other sites ( tongue , mouth , jaw , larynx , bladder , prostate ) , and a final section ( stocks , 1939 ) , with 9 maps , deals with cancer of the uterus , vagina , ovaries and fallopian tubes , and of the skin , lung , rectum and bones in women . 
 no such study of cancer in relation to this , or any other , geographical area has ever been made , and no summary is attempted here of the results and suggestions for research which it contains . 
 ( 2 ) the changes in mortality from cancer of various organs in england and wales between 1911 and 1944 are described in a paper by stocks and mackay ( 1946 )  . 
 ( 3 ) the general register office has published a study by stocks ( registrar general , 1947 ) of cancer of the stomach , oesophagus , lung , larynx , breast , uterus , ovary and some other sites in relation to a number of localities and environmental factors ( urban and rural districts , counties , the 13 , largest cities in england , 30 large towns , metropolitan boroughs of london , social indices , number of persons per room , amount of sunshine , source of water supply ) during one or other or both of two periods , 1921 - 30 and 1940 - 44 . 
one may mention here two results which provide valuable indications for further research , namely ( a ) an inverse relationship between number of sunshine hours and deaths from cancer of the lung , and ( b ) a high incidence of cancer of the stomach in the northern and central counties of wales , especially in the former . 
the author says : " the purpose of this report is to present the statistical facts , and point out any peculiarities in distribution and correspondences with other measurable factors which appear , so that all possible clues may be followed up by further study . 
 a list has been compiled of the types of information about cancer in man in england and wales which are to be found in the publications of the general register office . 
i. - cancer of the lung and of the larynx . males , england and wales , 1921 - 1951 . ascribed to lung cancer , for cancer of the larynx there has been little change over the past twenty years . the preceding papers in this series ( kennaway and kennaway , 1951 ; kennaway and waller , 1953 ) compared the incidence during the period 1946 - 1949 . 
kennaway cancer of the lung and larynx as shown by death certificates in four classes of area ( london , county boroughs , other urban ' districts , rural districts ) in england and wales . 
for a particular sub - division of the country expresses the mortality in that area as a percentage of that for the whole of england and wales , allowance being made for any differences in the age - distribution . 
given as an indication of the relative importance of the two causes of death ; these measures of mortality will not be used in this analysis . the most striking feature of table 11 is the behaviour of the figures for the female larynx as previously described . whereas for cancer of the lung the male and female figures show similar trends the corresponding figures for the larynx show no such similarity . 
the next step is to see whether the geographical or the urbanization factor is the more important ; this can be done by a study of table iv and fig . 
3 and table iv that urbanization is the predominating factor : in each region , the mortality due to lung cancer increases from the rural to the urban areas and although the same is true of the male larynx , when we look at the figures foi the female larynx we find the exact contrary ; in every case the highest mortahty is in the fural districts . 
the comparison is particularly striking when we look at the s.m.r.s for the county of london ( the most densely populat - ed of all our areas ) and then at those for the sparsely populated rural districts inv.i ' ales ancl the north . for the purposes of this comparison the differences between the c.m.r. 
we cannot say whether the extremely high figures for the female larynx in wales ( where the population at risk is in any case small ) are more than an extreme manifestation of the reverse urbanization gradient or whether they m , ight be due , for instance , to some ethnographical factor . further study of eancer of the lung . another feature that emerges from the diagram is , that for cancer of the lung the urbanization gradient is consistently steeper in the men thad . 
of 160 for the county of london . it would be interesting to make a similar analysis with the urban districts ( or better with the county boroughs and urban districts combined ) but the labour would be prohibitive . it may be mentioned in this connection that since 1950 the registrar general has adopted a more realistic classification , which wfll considerably simphfy the study of many problems . 
with its large dormitory areas , the male s.m.r.s for cancer of the lung are all higher than in the sparsely populated s.w. , wales ii and north il in females the absence of such a clear association is partly a reflexion of the lesser gradient already noticed for women and partly due to the larger sampling errors to which these s.m.r.s are subject ; on the other hand the remarkably low female s.m.r. 
a possible explanation is that there are two aetiological factors at work , the one positively correlated with urbanization ( a ) and the other negatively ( b )  . 
the mortahty ratio for the larynx ranged from 60 for males of class i to 143 for males of class v , but it is significant that married wo ' men showed no significant social class gradient , thus suggesting that the factors responsible for the excess of cancee of this site amongst unskflled males are directly associated with occupation . " on the other hand there was in 1931 no marked social gradient for cancer of the lung . what connection is there between the occupational factor and urbanization ? we cannot answef that question in the absence of mortality rates analysed by urbanization simultaneously with occupation . 
if the figures in table viii are representative , they may be said to show ( a ) cancer of the larynx is four times as common in men as in women ; in men , intrinsic cancers are nearly twice as common as extrinsic , whereas in women extrinsic are four times as common as intrinsic ; as a consequence of ( a ) and ( b ) , intrinsic cancers appear nearly thirteen times as often in men as in women * and the extrinsic twice as often in men as in women . the conventional inclusion of cancers of the retro - cricoid region among laryngeal tumours is very unfortunate . " the term ( cancer of the larynx ) should be restricted to the so - called ' intrinsic ' group of cancers . 
kennaway mouth , tongue , and pharynx , angular stomatitis , hypochromic anaemia , achlorhydria , splenomegaly , and spoon nails , in which carcinoma ofthe post - cricoid region this condition was first described independedtly by may develop in later years . paterson from cardiff ( 1919 ) and by brown kery from the westem infirmary , glasgow ( 1919 ) and has become know - n by the names of two latee investigators as the " plummer - vinson " syndrome . neitherpaterson ( 1919 , 1937 ) nor brown kelly ( 1919 , 1931 ) suggest , either in their earher or later papers , that this affectioin . is especiafly common in their own districts , though any such frequency would have this syndrome is of qu ' ite especial interest in cancer research assisted recognition . because the features present during the earlier years may indicate a precancerous metabolic state , which may be treated succes - sfury by improved feeding and administration of iron ( see for instance hare ' n , 1938 ; waldenstrom , 1938 , and elkelesg 1942 )  . 
the forowing section represents an attempt to collect the literature on the paterson - kery syndrome in relation to cancer ; no attempt has been made to introduce any uniformity into the anatomical classificatioin adopted by the various authors . ahlbom ( 1937 ) records , from the radiumhemmet , stockholm ( 1931 - 1936 ) , the incidence of carcinoma of the post - cricoid region . ( a ) cancers of the hypopharynx are more frequent in women , in whom also a mucb higher proportion ( 90 per cent ) of these tumours affect the post - cricoid area , than in men . 
was in der diiit der drmeren schwedischen bevblkerung fehlt , sind vor allem eisenhaltige vegetabilien , obst und fleisch . " bingham and logan ( 1953 ) say " the incidence of hypochromic anaemia in northern ireland is considerable and . 
these trends apply equally when the figures are analysed according to the separate regions , but there are differences between the regions , which may or may not be due to differences in degrees of urbanization undetected by the classiin particular the s.m.r.s for wales are very low for the fication we have used . lung and male larynx but very high for the female larynx . 
the literature upon the relation of the paterson - kelly syndrome to cancer , and upon possible dietetic and social factors in this condition , is summarized . we are greatly indebted to w . 
croton oil painted concurrently caused no increase in the incidence of the significance of the skin tumours , nor did it decrease the latent period ; absence of co - carcinogenic action of croton oil is discussed . the author is greatly indebted to p . 
kirby. from the research department , glasgow royal cancer hospital . received for publication , june 28 , 1984 . activity the carcinogenic of orally - administered 2 - acetylaminofluorene , aaf , for a number of tissues , mainly epithelial , was first demonstrated by wilson , deeds and cox ( 1941 ) for the rat , and subsequently confirmed for this species by bielschowsky ( 1944 , 1946 ) and others , for mice of various strains ( armstrong and bonser , 1944 , 1947 ; foulds , 1947 ) , for the fowl ( bielschowsky and green , 1945 ) and for the cat ( harding , quoted by bielschowsky , 1947 )  . recently wilson , deeds and cox ( 1947a ) have reported their own findings in mice of three pure strains . 
aaf has now been shown to be a carcinogen ( when given per os ) in eight strains of mice : cba , if , riii , white label , strong a , c57 black , c3h , and bagg albino . 
of the first five strains mentioned , cba were most prone to both liver and bladder tumours ; strong a were the least susceptible ( armstrong and bonser , 1947 )  . 
 ( 1941 ) were at that time unable to elicit tumours in rats by subcutaneous implantation of aaf , and , in view of the probable hydrolysis of aaf in the intestine to 2 - aminofluorene , af , they suggested that aaf might be converted to af and that the latter product was the real carcinogen . might be expected that af would be more carcinogenic for rats than aaf in however , in a recent paper , wilson , deeds and similar feeding experiments . cox ( 1947b ) report tumours to have arisen more slowly and in fewer numbers in rats given af orally than in similar rats receiving aaf in the same basal diet . they suggest that af , being more soluble than aaf , may have been absorbed more rapidly and then excreted rapidly . 
af derived from aaf by hydrolysis in the intestine could only be absorbed as fast as it was liberated . however , against this view it must be said that af , once absorbed , should be excreted as fast in either case and that tissues in remote sites will stand the same chance of receiving af , whether af or aaf be given orally , provided the presentation it seems possible that the hydrolysis takes place after absorption ; is continuous . studies on the liver after ingestion of aaf , using the extraction technique of miller and baumann ( 1945 ) and the estimation method of westfall ( 1945 ) , should yield information to test this point . it is significant that wilson , deeds and cox ( 1947a ) report tumours and other changes after implantation of crystalline aaf for long periods . bielschowsky ( 1944 ) painted af in acetone thrice weekly on the epilated contrary to expectation , no tumours at the site of painting skin of wistar rats . occurred , but all 5 rats developed liver tumour by 280 days and one had a tumour of the ductus acusticus externus . 
at first , arachis oil was used as vehicle , but later , tricaprylin became available and was used in place of arachis oil . injections were made at intervals of approximately 4 weeks , in alternate flanks ; 0 5 ml . 
a female dying at 351 days showed no abnormality , but of 7 mice dying between 530 and 594 days , all showed one or more liver tumours , some solid , some diffuse , with three cases being notably vascular . six of these seven mice were females , the other mouse being the only male to survive more than 125 days . 
one female , killed at 582 days , showed a mammary adenocarcinoma , and another , killed the same day , had a granulosa - cell tumour of the ovary . ( c ) c3h mice . - thirteen mice survived 52 to 126 days ; the rest survived 206 days or more . three females , killed at 206 , 235 and 235 days respectively , had one or two mammary adenocarcinomas . 
a fourth female was killed at 242 days without any gross tumour . three males survived 409 , 426 and 506 days respectively ; the first and the last of these showed hepatoma ; the other had primary renal carcinoma . 
ten male and two female mice survived over 500 days , four of these dying between 602 and 616 days ; extensive leukaemic infiltration was seen in two of these mice , but no liver tumours ( or tumours in other sites ) were found in any . 
kidney and bladder tumours were not found , nor were mammary tumours . ( b ) cba mice . - only cysts with minimal tissue reaction were found at the sites of injection in these mice . 
a variety of degenerative changes were found in the liver in most mice ; a male , injected eight times and dying at 285 days , had hepatoma at the edge of the left lobe . 
hepatomas were also found in three mice injected 11 times ; in two males dying at 565 and 574 days respectively , and in a female dying at 630 days . 
no tumours were found in the bladder or kidney in any of these mice . ( c ) c3h mice . - no tumours were found at the sites of injection , only minimal tissue reaction . 
one injected male of this strain had hepatomas by 242 days ; two males of the painted group had hepatomas by 409 and 506 days respectively . burns and schenken ( 1943 ) record a spontaneous primary hepatoma in a c311 male 14.5 months ( 440 days ) old . thus the mouse dying at 506 days may well have borne spontaneous tumours , and this possibility may also apply to that dying at 409 days . 
the earliest case seems to be undoubtedly induced by af which is therefore probably carcinogenic for the liver when injected subcutaneously in male c3h mice . among 12 cba mice given 2 - acetylaminofluorene ( aaf ) orally by armstrong and bonser ( 1944 ) , which survived more than 12 weeks , four showed liver tumours , but two were females dying at 63 and 65 weeks respectively and therefore liable to bear spontaneous tumnours . armstrong and bonser ( 1947 ) record three malignant hepatomas in seven male mice and five benign hepatomas in eight females given aaf orally . 
the time required for these tumours to develop is not recorded , but the incidence is well above that for spontaneous hepatoma in this species and , moreover , the latter always appear to remain benign . 
hence aaf and af both appear to be carcinogenic for the liver of cba mice ; af is slightly active also in c3h and c57 black mice . armstrong and bonser ( 1944 , 1947 ) record a high incidence of bladder tumours , wilson et al . 
in the present series no bladder tumours were found in mice injected subcutaneously with af and only in one female cba mouse , painted with af and killed at 582 thus af seems to be a bladder carcinogen when given orally to c57 black days . mice , but not when painted or injected subcutaneously . 
c3h mice appear to be unaffected in this organ . the kidney was free from tumour in all three strains after injection of af . painted mice of the c57 black and cba strains likewise had no kidney tumours , but a probable renal carcinoma was found in a painted c3h mouse , a male dying wilson et al . 
 ( 1947b ) record a carcinoma of the kidney in one of at 426 days . their c57 black mice given af orally . armstrong and bonser do not record any kidney tumour in cba mice given aaf orally . neither compound is very active for mouse kidney . armstrong and bonser ( 1947 ) record one mammary cancer in 9 females given aaf orally and surviving more than 20 weeks . 
one cba female in the present series , painted with af , showed mammary adenocarcinoma at 582 days . spontaneous mammary tumours in this strain seem not to occur and the solitary tumour found in each series referred to above is therefore considered to be significant . 
extremely active material capable of s " rdng fivsh t clours in less than two weeks has been obtained from both chemically induced and spontaneous sarcom firozen at - 790 c . 
since it involves the quesbon , first raised by ehrlich in 1907 , in connection with a possible bacterial source of cancer , of whether extreme cold can be used to destroy mammalian cells , and multaneously to preserve any posdble intraor extra - cellular agent capable of starting a t aour de novo in if the continued activity of such refiigerated tisme is cells of another host . aour produced in the due to new host is merely a transplant . if , however , it can be shown that the cers in the refrigerated tissue are dead , then the n6w tumour must be produced by an agent ( which would then be the " continuing cause " of cancer ) which is a separate .val of cells of the original anhml , then the t 260 w . 
craigie entity from the cells in which it lives , and which is capable of surviving under such transm , ission would be " cell - free , " certain conditions when they are dead . and would place any tumour so produced in the class of virus tumours , among the known virus chicken tumours , the shope papilloma of rabbits , bittner 's mammary carcinoma and lucke " s adenocarcinoma of the frog . the proof that prolongecl refrigeration kills mammalian tumour cells is difficult , and we are aware that in the past it has always been held , except by cramer ( 1930 ) , that the survival of only a few cells in the tumour mass accounts for the tumour in the new host . we have investigated the problem from a variety ofangles and have concluded , as will appear , that the cells are dead . jn the first place it must be realized that the sarcomas of mice which we have used are three well known to laboratory woikers , one a methylcholanthrene sarcoma ( c.48 in the inbred strain c57 black ) , and the other two arising as stromal transformations in transplants of sporadic mammary cancers investigated by r . 
none of these procedures affect the activity of the refrigerated tissue , which remains as great as or greater thirdly , we have made histological examinations than that of the fresh tissue . of frozen tissue implants at intervals and have examined the material itself , finding , - however , neither any evidence for survival of cells , nor conclusive proof of their total destruction , since one cannot be certain that every cell has been examined . finally , being well aware that to all these methods of approach might be opposed the objection of the remote possibility of the exceptional survival of a few cells , we have proceeded to dxy the refrigerated tissue completely to dust this is universally allowed to be lethal in vacuo at a temperature of - - 25 ' c . to both normal and tumour cells , yet we have obtained highly active dry material it therefore appears impossible to avoid from all the three tumours studied . the conclusion that from both the chemically induced and the sporadic sarcomas a cell - free agent can be recovered , which on injection into appropriate mice is capable of starting the tumour afresh . 
during this period attempts had been made again and again to propagate the tumour with cell - fi - ee filtrates and with dry tissue , and all had previously failed . ( 2 ) a sarcoma of the strain r3 . 
the sarcoma which formed from the stromal connective tissue was separated from the mamm ry cancer by ludford by early transplantations by which the slower growmg carcinoma was lost . ( 3 ) a similar sarcoma derived from the stroma of a carcinoma of the strain all three tumours are soft , rapidly growing sarcomas . 
the ' ampouilie - - s were then transferred to a storage cabinet kept at - 79 ' c . after an appropriate interv - al of hours , days or months , an ampoule was taken out , thawed to room temperature , opened , and 0 - 05 c.c. 
or less of the contents inoculated subcutaneously in the right flank of mice of the appropriate strawhen these ampoules were opened it was always noted that a physical change ha - d taken place in their contents , which had become more homogeneous , softer and slightly sticky after freezing . 
twe - four experiments were made with inoculations at varying intervals with uniform ] ' good results ( table 1 )  . it wiu be noted that in the last experiment on the time frozen makes no difference to the results . the list the material had been frozen 201 days , and was inoculated not only into its mouse of origin , but also into four other atains . 
refrigeration in van ; ow media . from experiments with mouse embryo tissue ( mann , 1949 ) we know that treatment with glucose ( without refrigeration ) reduces the activity of normal mamm lian cells , that storage in glycerol at 4 ' c . them , and that a combination of dextrose and cystein severely damages them , while fiwzing alone for one mour cells using glycerol , hour ik - ill them all . dextrose , eystein , and distifed water with and without fiwzing were therefore performed . table ii shows that these procedures , known to kill normal cells , have no effect on the activity of tumour tissue , dextrose indeed appearing definitely beneficial ( cmigie , 1949 )  . it wiff be noted that the results in table i and table 11 are very similar , and are condstent with the presence of a t nour agent other than a living mamm lian cell . 
as an example of the amount of man pulation which such t aour mince will stand we can cite the protocol of an experimentwith the c48 t ilour , carried various experiments with t 262 w . 
the mortar was then taken out of the c02 snow and solid frozen tissue and buffer pounded vigorously with the pestle , to break up as far as possible any remaining whole t thirty c.c. 
of cold distilled water was added , and when the mixture was finally hquid it was spun for 15 minutes at 10 , 000 revolutions a minute . ' the supernatant fluid was reddi - sh in colour and was of a ph 6 - 0 ; the deposit , firmly . 
of sahne ( - 85 per cent nacl in distffled water ) and the emulsion injected into six c57 mice . the mice developed ical c48 tumours , which were large on the 14th day . fibns of the emulsion were examined under the microscope and ' m none could a whole cell be found ; all that could be seen consisted of naked nuclei and separated masses of cytoplasm . experiments such as this do not appear to lend any aours started bv fi - ozen tissues are transplants , support t - o the belief that the t i.e. 
even there are even fewer apparentl - v intact bv the mincer . cells , while after treatment with glucose or with distified water profound changes appear affecting both nucleus and cytoplasa detailed studv of these changes is being made by one of us and wir be pubhshed later . a series of sections of implants of tumour tissue ( both sarcoma and carcinoma ) frozen to 79 ' c . 
by the fourth day much of this tissue is beiing absorbed and removed by the host , and on the fifth and sixth days and subsequently , the begi of a new sarcoma can be seen in the connective tissues surrounding the ne ; brotic mass . 
the appearances do not suggest survival of any of the implanted tissue , but rather a fresh sarcomatous reaction of the encapsulating in the case of frozen carcinoma also no living subcutaneous tissues of the host . tumour ceus were seen , and by the seventh day the decrotic m was encapsulated and shrunken . 
they were successful , as was also a similar experiment with the or tumour which wasaxied fresh by craigie . it has not so far been possible to obtain active dxied material from the c48 without preliminary storage at - 79 ' c . a brief account of the metbod of drying must be given , though for details of the apparatus used craigie 's paper ( 1949 ) should be consulted . 
the tissue to oule or , if freshly miinced , diluted be dried is either taken from the storage a v ' n ' th an eqltal volume of 5 - 3 per cent dextrose and is run into the drying flask . it sbould be distributed as evenly as possible over the bottom of the flask in a thin layer . 
ofm / 150 eystein ph added after cirying to zero , pumping is then continued for a further half or one hour to be absolutely certain of the removal of the last traces of wate ' r . 
of which is injected subcutaneously in each mouse . before this method of drying was evolved , many unsuccessful experiments with these tumours , using the knox method of drying , had been cam ' ed out . even now a successful res - ult - is not obtained in every case , and - much further experimentation will be required to determine the optimum conditions . 
hall. from the hugh adam cancer research department of the medical school and the new zealand branch of the british empire cancer campaign , university of otago , dunedin . received for publication may 26 , 1953 . rats numerous attempts have been made to elucidate the role of the thyroid hormone in the development of chemically induced tumours . 
the relevant literature has been reviewed by miller and baumann ( 1951 ) who studied this problem in treated with dimethyl - amino - azobenzene . these authors mention some of the experimental difficulties encountered when the metabolic rate is altered by the administration of goitrogens or of thyroxthe action of thiourea , thiouracil and related compounds , however , is not limited to the thyroid ; they can affect also other organs , as for instance the liver ( fitzhugh complications of this kind can be avoided by means of and nelson , 1948 )  . surgery if hypothyroidism is the goal of the investigation . 
the effects of partial thyroidectomy are comparable with those obtained by goitrogens in doses too small to inhibit completely thyroxine synthesis . complete elimination of thyroid hormones resulting from either the administration of large doses of goitrogens or from the removal of the gland leads to a complex endocrine imbalance , the outstanding feature of which is a pronounced disturbance of growth . the pituitaries of such rats contain no acidophils and therefore no somatotrophin is formed . 
the thyrotrophic hormone , however , is secreted in elevated amounts . we have studied the action of aminofluorene ( a.f. ) and its acetyl derivative ( a.a.f. ) on the thyroidectomized rat , choosing these carcinogens because they induce tumours in more than one organ . 
one hundred and thirty were wistar rats ( 106 males , 9 of which were castrates , and 24 females ) and 17 were males of a piebald strain . forty - nine intact rats and 9 castrates served as controls ; eighty - nine were thyroidectomized . sixty - two of the 89 ( 70 per cent ) were considered to be completely thyroidectomized because their pituitaries were virtually free of acidophils . 
with the same the intact but not the thyroidamount of carcinogen during the remainder . after the 20th week the ectomized animals consumed all the food offered . in experiment 2 the milkanimals were maintained on ordinary stock diet . flour diet was given throughout , but for the first 20 weeks the diet was adjusted in such a way that 2 mg . 
in acetone 70 applications being given to the albino and 90 to the piebald rats . in this experiment rats which were obviously not completely thyroidectomized as indicated by their growth curve were kept separately from the other animals in in experiment 4 , 9 castrated order to avoid thyroxine intake from the excreta . and 30 intact rats were treated with a.a.f. 
daily. maintained on the wet diet supplemented by grain . in the 15th week 19 of the intact animals were thyroidectomized . liberal amounts of drinking water were available to all animals . in our experience thyroidectomized rats kept on a wet diet are in a better in long - term experiments state of nutrition than when they receive dry food . care has to be taken that excessive growth of the incisors does not interfere with their food consumption . the rats were weighed once weekly and examined for the presence of tumours . they were sacrificed when a neoplasm was suspected or when their general state of health made it advisable . 
the earliest hepatoma was found in the controls in the 18th week of the experiment , multiple benign cystic cholangiomata being already present in the partially thyroidectomized males the earliest hepatoma was at the 15th . discovered in the 28th week . 
no mammary cancers were seen in the thyroidectomized females , the majority of which were in anoestrus already in the third week of the experiment when vaginal smears were taken for the first time . table ii ( experiment 3 ) shows the results obtained with a.f. 
two appeared in intact , 3 in partial and 4 in completely thyroidectomized rats . in addition , one adenoma of the lung appeared in the latter group , and a cancer of the breast in the controls . in experiment 4 thyroidectomy was performed after a.a.f. 
had been fed all the controls developed hepatomas , the first being for a period of 13 weeks . found 7 weeks after the withdrawal of the carcinogen . thyroidectomy performed in the 15th week of the experiment was without the slightest influence on the development of these neoplasms , the first hepatoma appearing already in the 19th week . 
when at the 38th week the experiment was terminated each surviving animal was found to have hepatomatous and cholangiomatous lesions . these results are summarized in table iii , which includes also an additional table iii . - tumours induced by a.a.f. 
hall reduced , the glands containing little fluid whereas the weight of the testes was well maintained . in such animals an atrophy of the interstitial cells of the testis was found histologically , indicating inadequate stimulation by interstitial cell - stimulating hormone ( i.c.s.h. ) , and subsequent failure to produce androgens in amounts sufficient for the maintenance of the accessory sex organs . in this connection it might be remembered that none of the completely thyroidectomized females had a regular oestrous cycle . the adrenals did not show uniform changes . the width of the cortex tended to be less than normally ; the sudanophobic zone , present in intact males , was frequently absent , and the amount of lipoid stainable with oil red 0 was reduced considerably in some but little in other glands . 
some of the thyroidectomized animals were rather obese at the time they were sacrificed , which made correlation between organ and body weight unreliable . as in an earlier experiment ( bielschowsky , 1949 ) , neoplastic changes were found in the thyroid tissue of a.a.f. - treated animals in which a small fraction of the gland had escaped removal . in one instance a highly anaplastic tumour arising from such a thyroid rest was found at autopsy - worth mentioning because a tumour - cell embolus was seen in the periphery of this neoplasm , the only case in which evidence suggestive of malignancy was found in such a thyroid tumour . in the pituitary of this male wistar rat an adenoma was found . the tumour , the only one seen in these experiments , had the same morphology as the basophil adenomata present in aged rats which had received an iodinedeficient diet ( bielschowsky , 1953 )  . all the other pituitaries showed the typical picture of total or partial thyroidectomy , i.e. , absence of acidophils or marked reduction in their numbers with evidence of degranulation coupled with the appearance of " thyroidectomy ' " cells . the retro - bulbar tumours . the appearance of carcinomata in the orbital tissue of two rats of experiment 1 , a type of neoplasm only found in the thyroidectomized groups , led to a systematic search for lesions in the lacrymal glands . 
6 shows that they vary considerably in size and shape and have lost the pale foamy appearance of the normal glandular epithelium . their nuclei are hyperchromatic and dividing cells are present . since these changes were obviously of a neoplastic nature it seems justified to consider the retro - bulbar tumours as carcinomata arising from the epithelium of the lacrymal gland . in intact rats the lacrymal glands are of a brownish colour ; in many of the thyroidectomized animals they were more whitish and appeared also to be more moist than normally . sometimes these changes were bilateral , but not infrequently only one side was affected . histologically in thyroxine - deficient rats , treated with a.f. 
whether the absence of thyroxine is the main factor responsible for the results obtained so far we can only state that thyroidectomy prior remains to be investigated . to the administration of the fluorene derivatives renders the livers of rats unsusceptible to the carcinogenic action without preventing the induction of neothyroidectomy performed after the administration of plasms in other organs . effective amounts of these compounds did not retard the development of malignant it seems therefore that it is the early stage in carcinogenesis liver tumours . preliminary results of experiwhich is influenced by the removal of the thyroid . ments yet to be terminated point into the same direction . bielschowsky and hall , 1952 ; during 1952 evidence was obtained by three independent groups of workers griffin , ( moon , simpson and evans , 1952 ; rinfret and corsigilia , 1953 ) that the action of highly potent carcinogens can be " inhibited " by the removal of the pituitary or of the thyroid . 
the growth and development of most organs , with the possible exception of the brain , is dependent on hormonal stimulation , but there exist considerable differences in degree , as shown by the effects of hypophysectomy . 
the gonads , thyroid and adrenals atrophy always , but if the hypophysectomized rat receives adequate amounts of food the growth of the liver is proportional to body growth . thus neither liver nor the subcutaneous tissue can be compared with the target organs of specific trophic hormones , although crude pituitary extracts can induce disproportionate growth in the liver ( selye , 1949 ) and in acromegalics the soft tissue can increase in size . the role of the somatotrophic or growth hormone in normal or pathological growth is only imperfectly understood . 
growth can be promoted in hypophysectomized rats not only by somatotrophin but also by thyroxine , as shown by geschwind and li ( 1952 ) , or by insulin ( best , 1952 )  . 
a great variety of neoplasms has been obtained in intact but not in hypophysectomized rats injected for long periods with purified growth hormone ( moon , simpson , li and evans , .oestro1950a , 1950b , 1950c , 1951 ; koneff , moon , simpson , li and evans , 1951 ) gens can retard growth by inhibiting the production of somatotrophic hormone . this does not prevent carcinogenesis . 
 ( 1950a , 1950b , 1950c , 1951 ) as well as griffin and his collaborators ( 1953 ) used carcinogens which acted on one organ only . their results could be due to a failure of the hypophysectomized rat to metabolise the compound administered into the carcinogen proper . this possibility has to be considered since the discovery by bonser , clayson , jull and pyrah ( 1952 ) that 1 - hydroxy 2 - naphthylamine is the active agent when 2 - naphthylamine is administered . however in our case , the fact that extrahepatic tumours developed while the liver , the most susceptible of all organs in the intact male rat , failed to respond to the carcinogenic action of a.f. 
and its acetyl - derivative does not favour this interpretation . some of the neoplasms found in the thyroidectomized animals are so rare in our material that we cannot be quite sure that they were due to the action of a.a.f. neither in normal nor in experimental rats of our colony have we ever observed a papilloma of the stomach arising from the glandular mucosa or a tumour of the brain , but vasquez - lopez ( 1945 ) as well as hoch - ligeti and russell ( 1950 ) have described gliomas in rats treated with a.a.f. benign tumours arising in the mucosa of the uterus are not infrequent in aged rats of however , the tumour depicted in fig . 
3 differs from all others our colony . observed by its strong resemblance to a deciduoma . in dunedin carcinomata aiising in the lacrymal glands have been found only in four a.a.f. 
no account of the state of the endocrine organs was given . in our experience a low fat content of the diet per se does not favour the development of cancers of the lacrymal glands . 
the mice which survived to tumour age , though not themselves used for experiment , were not certainly representative of the whole colony and , owing to the concentration of tumours in famihes , the inclusion or omission of a single litter could greatly alter the tumour incidence calculated on the small nurabers available . 
the " effective total " ' is the number of mice which surv - ived to the age at which the earfiest tumour was detected in any of the groups , namely i 10 days in an f4 mouse of strain br4 ( blue label )  . 
many of the mice recorded as dead without tumour succumbed to epidemic infection about a year after the beginning of the experiment . tables 1 - 111 show that the incidence of tumours in the strains br4 ( pink label ) , br4 ( blue label ) , and br6 was unequivocally " high . " the three strains were substantially alike . 
tumours developed , indiscriminately as it seemed , in 11 wild , " 11 white , " and " black " mice in the f . - f4generations and continue to develop in " white " and " black " sublines up to the f6 generation . 
the later age - incidence of tumours in the f2 females was probably attributable to the breeding history ; the f2 females , in contrast with later generations , were not subjected to forced breeding . the incidence of tumours in the br16 strain ( table iv ) so far is extremely low . 
the great majority of the mice survive and more tumours may yet develop , but the average age is already higher than th ' e average age of tumour development in the other three strains . 
tumours were ground in - a mortar with sand and saline to make suspensions which ranged in strength , in different experiments , from 13 to 20 per cent w / v . 
the debris was removed by spinning in an ordinary centrifuge , and the supematant fluid was injected , at weekly intervals , into the dorsal subcutaneous tissues , each dose being 1 - 0 c.c. sixteen mice reeeived each 4 injections of extracts of bri tumours of the first or third transplanted generations , five received 3 injections and two received 2 injections . twelve mice received each i injection of an extract of a primary spontaneous c3h tumour and 3 injections of primary spontaneous r3 tumours , and seven mice received 3 injections of the r3 extracts only . all the extracts were similarly prepared . the females were caged with males and subjected to forced breeding , litters being removed within 48 hours ( usually within 24 hours ) of birth . table v summarizes the results at 89 weeks from the beginning of the experiment . 
the " effective totals " comprise the mice which survived to the age when the first tumour was detected ( 180 days in a mouse injected with bri extract )  . 
the average number of tumours per mouse was 2 - 5 , 24 mice having from 2 to 6 t aours each . aour was 25 weeks ; the earhest the average age at the first detection of a t tumour wa - s recorded at the age of 17 weeks , and the latest at 54 weeks . the 3 mice without tumours are alive at ages of 81 , 81 and 85 weeks respecit is noteworthy that although continuously with males they have had tively . no litters for about a year ; previoxwly litters were not recorded . 
no observations were made on virgin mice . incidence of tumours in ( c57 black ? x agew - free r3 ct ) f ] l hybri& . remale mice taken at random from the laboratorystock of c57 black were mated with males : firom a colony of r3 mice free from milk agent . i am indebted for the male mice to my coreague b . 
the f , , hybrids were subjected to forced breeding throughout their reproductive lives . one hundred female hybrids were reared ; 21 died without tumours at an average age of 21 weeks and 79 are alive at an average age of 57 weeks . 
the diversity of genetic constitution in the f2 and subsequent generations did not noticeably affect the incidence of tumours which developed indiscriminately in " black , " " white " and " wild " mice 4 ' white " and " w - fld " subhnes estabhshed by and in each of the " black , ly 31 selective breeding . 
the patemal contribution was not probably genetic for , as shown in this paper and in previous reports from this laboratory ( dmochowski , 1944 , 1945 ) , the c57 black x a hybrids developed tumours abundantly when tumour agent was supphed to them artificiafly . 
the uncompleted observ - ations on hybrids having fathers belonging to a subline of r3 mice deprived of tumour agent accorded with similar observations bv anderv - ont and dinnn ( 1948a , b , c ) in showing a substantial reduction in the incidence of tumours comparison with similar hybrids whose fathers derived from a line carrying the tumour agent . 
the experiment was open to the criticism , which anderv - ont and dunn apphed to their ow - n experiment , that the agent - fiee and agentbearing malet ; were separated by several generations of inbreeding and possibly differed geneticary . 
tumour agent was not demonstrable in the hybrids or in their tumours , and the offspring of tumour - bearing mice , whether obtained by back - crossing or by brother - sister matings , rarely developed tumours . 
two litters of - ( c x c3h ) f , were exceptional in that tumours developed in sisters at unusually early ages ( 4 - 10 months )  . the backcross offspring of two tumour - bearing females of one litter all developed tumours at average ages of 7 and 9 months respectively . 
the progeny of two tumour - bearing ( c57 black y x r3 ct ) - p . , females had a high incidence of mammary tuinours ( about 70 per cent ) through at least 5 generations . 
i fowl sarcoma material which had been subjected to repeated applications of cold possessed a greater tumour - producing activity than those prepared from similar material which had not been subjected to this ' treatment ( selbie and mcintosh , in explanation of this finding selbie and mcintosh ( 1939 ) suggested 1939 )  . that the freezing broke up the tissue fragments , ' and thus allowed a greater liberation of virus than would otherwise have been possible . in the course of some recent quantitative investigations into the effects of cold and desiccation on the rous no . 
the chromatographic study of riley ( 1950 ) in which adsorption of the rous virus was shown to take place on to a column of diatomaceous earth suggested that adsorption would also take place when this virus was passed through berkefold filters which are likewise composed of diatomaceous earth . in the present work an attempt has been made to assess the decrease in the tumour - producing activity of suspensions of the rous no . 
i fowl sarcoma virus experiments are also reported which which berkefeld filtration brings about . were designed to show whether or not this decrease was due to adsorption of the virus on to the berkefeld candle during filtration , and in addition , an investigation has been carried out to find whether repeated freezing and thawing affects the filterability of the rous virus . 
the tumour was removed , cut small with scissors , and disinte a mechanical blender ; the method ated in has been described in detail in a previous paper ( epstein and cook , 1951 )  . 
filtration was continued until the filter candle was quite empty , as shown by air bubbles being sucked through after the filtered after use each filter candle was tested by passing through it 80 c.c. 
a sample was taken from the resulting filtrate , part of it being set aside ready for inoculation and part being used to make dilutions in serial tenfold steps with sahne ; a portion of each dilution was kept for inoculation . experiment8 4 and 5 ( recovery of virus from filter )  . - these experiments were performed in their early part as a repetition of the foregoing in which samples of a virus suspension and the berkefeld filtrate derived from it were couected and diluted in serial tenfold steps with saline for inoculation . in addition , however , a sahne wash of the filter was prepared ; a sample was taken from the saline wash , part being set aside undiluted for inoculation and part being used to make dilutions in serial tenfold steps with saline . 
a portion of each dilution was kept for inoculation . experiment8 6 , 7 , 8 and 9 ( effect of freezing and thawing on filterability )  . disintegrated tumour was prepared and in ' each of these experiments was divided into two samples , one being left untreated and the other being subjected to repeated freezing and thawing . 
suspension berkefeld untreated frozen and thawed x 6 f : 61trate untreated frozenandthawed x 6 untreated frozen and thaweci x 6 - .10% virus suspension berkefeld filtrate - .10% virus suspension berkefeld filtrate 10% virus suspension berkefeld filtrate untreated frozenandthawed x 6 untreated frozenandthawed x 6 untreated frozenandthawed x 6 untreated frozenandthawed x 6 dilutions of preparation and number of tumours arising from 4 inoculatioins of each . 10 - 2 10 - 11 10 - 4 10 - 5 10 - 0 10 - 11 2 + ( 2 ) 0 3 + ( l ) filter test . - - - n prod . 
now , froni the results shown in table ii , it is clear that an appreciable amount of the tumour - producing activity losb when virus suspensions were passed through berkefeld candles could be recovered by washing saline through the latter after use . in the experiments shown in table ii the filters when tested retained in each case both chr . 
aureu8 making it impossible for the lost tumour - producing activity , recovered on washing the filters with saline , to have been due to cells . this recoverability of at least part of the tumour - producing activity lost on filtering rous virus suspensions gives further support for . 
epstein freezing and thawing were passed through a berkefeld candle to give a filtrate ' , as where those made from similar untreated disintegrated tumour were so filtered . the application of repeated freezing and thawing to rous sarcoirna material has thus been found not to increase the ability of the virus contained in it to pass berkefeld filters . 
the present work has also shown ( table 111 ) , in confirmation of that previously reported ( epstein , 1951 ) , that repeated freezing and thawing of mechanically disintegrat - ed rous tumour materizal did not release more virus on extraction than where no such treatment was applied . 
from these two facts it appears that repeated freezing and thawing has no action on the rous virus likely to make berkefeld filtrates of treated tumour material , prepared as described here , more active than those made from untreated material . 
the results shown in table iii demonstrate this clearly ; they are at variance with those reported by selbie and mcintosh ( 1939 )  . in attempting to relate the results of the present work to those of previous investigators with which they do not agree , two possible explanations require consideration : firstly , it must be remembered that selbie and mcintosh carried out their during that time the rous virus may possibly have investigations 13 years ago . undergone variations affecting its properties which might account for the variations in the experimental results obtained . secondly , the method of extracting the rous virus employed by selbie and mcintosh ( 1939 ) consisted of coarse mincing of the tumour material followed by repeated freezing and thawing was then applied to the grinding with sand . resulting preparation , and may well have contributed to the achieving of complete disintegration of the tumour and the maximum extraction of virus from it . 
in the present work , however , disintegration of the tumour material was brought about mechanicall before the cold was applied , and would seem to have been so complete that the repeated freezing and thawing could not have any further this is considered to be the most likely explanation of the contradiction effect . between the findings reported by selbie and mcintosh ( 1939 ) and those recorded in this communication . in consequence of the results of the present work it is thought that where in the future attempts are to be made to demonstrate the presence of viruses in tumours not hitherto known to possess them , borkefeld filtration , with or without previous repeated freezing and thawing of the material to be filtered , should be avoided . 
i fowl sarcoma virus are described . also described are experiments in which the effect of repeated freezing and thawing on the filterabihty of this virus has been investigated . susceptible inbred brown leghorn fowl have been used . the method used to disintegrate rous sarcoma tissue mechanically in order to make from it a virus suspension is set forth . 
the technique used to apply repeated freezing and thawing to disintegrated rous tumour is indicated , as is the technique used in berkefeld filtrat - ion of suspensions of the virus . a titration method has been employed in which preparations whose tumourproducing activities were to be compared have been diluted in serial tenfold steps with saline and inoculations made with each dilution . the results show that wben rous virus suspensions prepared by extracting disintegrated rous tumour with saline were passed through berkefeld filters , part of the virus became adsorbed on to the filter . 
1. received for publication march 25 , 1947 . tins investigation was undertaken to bring up to date the records of the middlesex hospital , and to attempt to discover whether there was any statistical evidence to support commonly held views on factors affecting prognosis and methods of treatment . 836 cases of carcinoma of the female breast treated during the years 1926 - 35 were analysed and a smaller group of 265 cases , treated during the years 1936 - 40 , were the subject of a further investigation to discover the effect of more modern methods of treatment . the hopes held at the start of this work have not been completely fulfilled . for such an investigation to give a clear cut statistical answer to all of the controversial questions , careful planning and equal distribution of cases , according to the extent of the disease and type of treatment used , would be necessary . this was not so in this series of cases . 
as a result the evidence on some points is too inconclusive to give an answer . careful analysis of results would seem to be essential if methods of treatment are to be guided by fact rather than by impressions . if , in the future , reliable figures on a large scale are to be obtained , co - ordination of policy in treatment and planning ahead in large medical formations will be necessary . whether this is acceptable or desirable may be open to argument , for it must inevitably mean some acceptance by each individual surgeon of the combined opinion of his colleagues . only thus , however , can the successful analysis of large series be substituted for the analysis of smaller series for individual surgeons . despite the difficulties that have arisen owing to the many variations in technique during the years covering this investigation , certain facts that may be of interest and value have emerged . 
some previously held views have been supported ; others appear to be incorrect . the histological findings in this series have been omitted owing to the impracticability of examining over 1000 sections in the time available . this in itself would make the basis of a separate inquiry . from the statistical point of view therefore it has been assumed that any variations in the histological grouping of the growths have been spread evenly throughout the series . the presentation of results of an investigation such as this is difficult . while the actual detailed figures and tables by which conclusions have been reached are of importance , their inclusion in the text would make reading wearisome . therefore simplified tables only have been included . * late surgical registrar ( demobilized )  . 
a case dying of other causes or of unknown causes cannot really be called a success or a failure . two ways of expressing the result seem to be possible - the survival rate or the mortality rate . 
the former has the advantage that it allows easier comparison with previous series that are almost universally expressed in terms of survival it would appear , however , that results expressed in terms of ( or cure ) rates . those actually dying of carcinoma of the breast will give a more accurate picture of effects of various factors influencing the prognosis . for these reasons the " mortality rate " has been used as a routine in this it has been expressed as the percentage of those cases dead from carcinoma paper . of the breast of all traced cases . 
when both ulceration and axillary gland involvement are present as in stage iiib cases the outlook is gloomy in the extreme . the survival rate for stage i cases is 51 - 4 per cent . this appears poor when compared with other series , but it should be remembered that this figure includes only those cases alive . 
any case dying of unknown cause or other cause in this method of calculating the survival rate would be counted as a failure . if such cases are excluded from the total the figure would be very close to 60 per cent . a point that is striking is the number of cases that die from a carcinoma of the breast during the 5 - 10 - year period . there is a consistent increase in mortality rates . 
a further subdivision was made of cases with slight attachment into those with attachment to the skin and those with attachment to deeper tissues . the mortality rate for these sub - groups was : deep attachment skin attachment percentage ~~~~~stage . 
when a growth lay between two quadrants it was described as lying in a " mid " position . thus there were the " mid - medial , " the " mid - inferior , " the " mid - lateral " and thbe " mid - superior " positions . 
the average age for stage i growths was 55 years , for stage ii growths 54 years , and for stage iii growths 59 years . the incidence of growths in decades was : decade . 0 - 39 40 - 49 50 - 59 60 - 69 70 - 79 80 - 89  . 
when associated with surgery the radiotherapy was either the implantation of radium into the wound at the time of operation according to the method described by sampson handley ( 1922 ) or prophylactic deep x - ray therapy . the latter was given in multiple intermittent sub - erythemal doses with medium voltage . 
as would be expected , this interval was increased with the stages of the disease . thus stage i cases had an average delay of 7 months , stage ii cases of 10 months and stage iii cases of 18 months . one can therefore reason that an average case has between 7 and 10 months ' unforgrace before the catastrophe of axillary gland involvement takes place . tunately there is too much variance in individual growths for this figure to be of anly real value . 
they should probably be called " insufficiently treated , " but have those under the heading " breast , been included in this analysis for convenience . contralateral " are those in which the evidence strongly suggests a true recurrence rather than a second primary . the low incidence of mediastinal recurrences is probably due to the fact that practitioners were likely to call any intrathoracic recurrences " pulmonary metathese figures , however , do not lend support to rowlands and turner stasis . " ( 1936 ) , who state that the mediastinum is the commonest site for a recurrence . this investigation has cleared up one point that has been debated in the past . there is a direct path of spread from the breast to the supraclavicular glands . of 91 cases that developed recurrences in those glands 17 were stage i cases , treated by radical mastectomy , and with axillary glands proved to be free from in view of the fact that the axillary glands were removed growth histologically . at operation and that path of spread permanently closed , the subsequent invasion of the supraclavicular glands must have been through a more direct path . relation of site of primary growth to site of recurrence . some quadrants of the breast have been considered to be more likely to metathus , inner quadrant growths have been held to give stasize in certain areas . secondaries in the chest more frequently . 
the ten to fifteen year period . no surgeon who has followed cases of carcinoma of the breast can have failed to see cases of recurrence occurring at long intervals after operation . these are often regarded as interesting rarities . 
the actual number that do develop these late recurrences is small owing to the cases that die early , and this has given the false impression that survival to five years means that the chance of recurrence is negligible . 
1. received for publication january 26 , 1949 . thie application of the methods of urinary cholesterol estimation given by burchell and maclagan ( 1949 ) to cancer and control cases will now be described . bmaterial urine specimens were obtained from 13 normal subjects and 116 patients admitted to westminster hospital or to westminster hospital ( .all saints ' ) twenty - five of these patients were suffering from diseases urological centre . thought to be unlikely to affect cholesterol excretion as shown in the tables , and 73 were suffering from various forms of cancer . 
sample of the mixed specimen , or a smaller aliquot in the case of a concentrated urine , was centrifuged , the deposit washed once with normal saline and extracted directly with three portions of boiling acetone . 
the acetone extract was evaporated to dryness , and the residue extracted with petroleum ether for the determination of cholesterol as above . the cholesterol content of the supernatant urine ( su ) was determined on 200 ml . 
the sex difference is mainly due to the larger number of epithelial cells and leucocytes in urinary deposits froimw omen . it appears likely from these figures that the total urinarcholesterol would not exceed 4 - 49 mg . 
maclagan it is evident from this that if albuminuria is present from whatever cause , the su may be expected to show an increase in cholesterol content , and such a rise is unlikely to be specifically related to cancer . 
of urine with phenol reagent as described by burchell and maclagan ( 1949 ) , where reasons are given for assuming that this method does , in fact , estimate a proteose - like substance . it will be seen from fig . 
the ud cholesterol is associated with the cells of the deposit and shows a marked sex difference , being much higher in women than in it appears to have no direct relation to cancer . 
the su cholesterol on men . the other hand is associated with a urinary proteose fraction , or with heatraised su cholesterol excretion in the coagulable protein when present . absence of albuminuria did occur in a small proportion of cases of cancer ( 5 out this gives a of 51 cases ) , although the increase was slight in 3 of these cases . total incidence of hypercholesteroluria in cancer of 9 - 8 per cent , which is somewhat lower than that reported by other workers . 
thus sobotka , bloch and rosenbloom ( 1940 ) found 20 - 6 per cent , and bruger and ehrlich ( 1943 ) 34 - 3 per cent of positive results . 
for example , bruger and ehrlich ( 1943 ) reported some rise of total urinary cholesterol in 11 out of 32 cases of cancer , but 5 of these had either albuminuria or excess of cells in the deposit or both , findings which , according to our experience , might have been sufficient to account for the hypercholesteroluria even in the absence of cancer . 
the exclusion of these cases would bring the incidence of positive results down to the figure of 22 - 2 per cent . , which does not differ significantly from our own finding of 9 - 8 per cent ( difference 12 - 4 , standard error of difference 8 - 2 )  . we must conclude , therefore , that hypercholesteroluria , while frequently due to associated albuminuria or pyuria , does occur in a small proportion of in such cases it is the supercases of cancer in the absence of these factors . natant urine cholesterol which is increased . 
the incidence is not high enough to make the estimation of any diagnostic value , but it is of theoretical interest , and presumably depends upon increased tissue breakdown as suggested by previous workers . it should be noted that the colorimetric method of estimation used is not entirely specific for cholesterol , and the possibility that other steroids might have given rise to the few positive results must be admitted . however , the earlier work of bloch and sobotka ( 1938 ) on pooled 100 litre specimens of urine suggests that the results probably were due to increase of cholesterol itself . the question of urinary proteose is of some interest in view of the work of winzler and burk ( 1943 ) on blood proteose and cancer in rats . 
bartholomew 's hospital , london , e.c.i. received for publication august 25 , 1949 . the question , whether the recent increase in deaths attributed to cancer of the lung is due to a real increase in the incidence of this disease , has been discussed the present paper , which brings forward no new data , is an by many writers . examination of some of the evidence offered on this subject . ( 1 ) the application of statistics from hospitals . the problem of finding the best index of a real increase in the incidence of lung cancer from hospital statistics is a difficult one . the relevant facts usually ascertainable at a hospital are : the annual total 1 . 
3 , 6 and 9 could be used as a measure 3 and 6 are open to objection on the grounds of the incidence of lung cancer . of possibly mistaken diagnosis , hence presumably 9 is the most accurate measure of what it is stated to be . as a measure of the population at risk , i.e. 
of becoming a case on which a post - mortem for cancer of the lung is done at a given hospital , we could use 1 , 2 , 4 , 5 , 7 or 8 . do these measures change in their quality of being representative of the the answer is that they all do so , because the cross - section general population ? of the population being admitted to hospital , whether of all cases or of cancer alone , changes , and therefore the cross - section of all deaths represented by deaths in hospital changes also . 
the assertion that the cross - section changes is based on knowledge that many people are now admitted to hospital who never would have been so admitted in the past - e.g. 
the same argument , that the cases would have been sufficiently serious to be admitted under any circumstances , could be applied , though with less certainty , to 2 , 4 , 5 , 7 , 8 . 
kennaway pathologists who deny that there is any satisfactory evidence of the suspicion is that where the incidence of lung cancer during recent years . such increase has appeared to have been conspicuous , there was formerly a low standard of accuracy of pathological diagnosis , and that the standard has improved with the passage of time . " real increase elusive disease has estimates of incidence , " for the foregoing reasons , comparisons of early and recent clinical or necropsy comparisons of the findings in different countries or in different hospitals , must be quite unreliable . so much depends on the personal experience of the clinicians and pathologists concerned , and current jotmrnals contain evidence enough that a uniformly high standard of diagnosis of this yet been attained by either . 
3 shows no steady rise , " which is perfectly true , and they conclude : " in our opinion the figures given illustrate that even a pronounced increase of the crude mortality rate for lung cancer among males , and almost only among males , does not necessarily mean an increase in incidence of that disease . 
presumably the more frequent detection of the disease is due to improvement of diagnostic procedures , and increased attention , and similar explanations may be correct in the case of occupations with an increased mortality from lung cancer . " one has difficulty in believing that any generalizations about cancer of the lung can be based upon such a peculiar succession of such small totals , drawn from a highly selected population , as those given in the third columnu of the table , namely 7 , 5 , 5 , 7 , 6 , 20 , 13 , 20 , 13 , 14 cases of pulmonary cancer . is one to believe that the totals 6 , 20 , 13 in the three consecutive years 1940 , 1941 and 1942 correspond to any similar annual incidence upon the whole population of denmark ? if there is no such parallelism , what is the value of these figures , and how can they provide a basis for the important generalization quoted above ? one may doubt whether the radiographic examination of any population for pulmonaty tuberculosis adds much to our knowledge of the total incidence of cancer of the lung . such a survey will , of course , reveal a number of cases , previously undetected , of such cancer . 
blackburn. from the department of haematology , the royal infirmary and ho8pital , sheffield . received for publication april 3 , 1954 . the forowing considerations led us to carry out a trial of stilboestrol in acute it is well know - n that the endocrine organs play an important part leukaemia . in the regulation of haemopoiesis , and many workers have reported the beneficial unfortunately , effects of acth and cortisone in some cases of this disease . however , remissions so induced are usuary only of short duration . re - treatment may again have a beneficl ' al effect , but eventually a refractory state is reached . on the other hand , " myelokentric " and " lymphokentric " acids , steroid - like principles extracted from urine ( afiller and turner , 1943 ) and from serum ( foster and miller , 1950 ) cause leukaemoid effects of myeloid and of lymphatic type furthermore , myelokentric respectively when injected into normal animals . acid has induced partial remissions in human cases of lymphoblastic leukaemia in the hands of miller , herbutt and jones ( 1947 )  . 
hence hormonal imbalance may play a part in the aetiology of leukaemia . finkelstein , gordon and charipper ( 1944 ) demonstrated that oestrogens have a depressant effect on the bone - marrow in certain conditions , but they did not study leukaemic states . burrows and horning ( 1952 ) have shown that not only are oestrogens careinoaenic , but they may be careinostatic , often restraining and causing regression of some human neoplasms such as carcinomata of the breast and prostate . 
they also state that the liabihty of mice to leucosis can be increased by oestrogens and reduced by androgens . furth ( 1952 ) , however , reminds us that in most strains of mice loukaemia is more common in the female , but in man it is more it is possible , therefore , that in human leukaemia oestrogens common in males . may have the opposite effect to that in niiee . dausset and schwarzman ( 1951 ) reported a study of 212 cases of acute leukaemia witb , regard to the influence of age and sex upon the frequency and cytological types . 
they also reviewed other series in the literature from these points of view , including both acute and chronic leukaemia . these authors state that between 18 and 50 years in both males and females there is an overwhelrning preponderance of myeloid leukaemia , while under the age of 18 and over the age of 50 lymphoid leukaemia occurs almost exclusively . 
as the former occurs most commonly during the period of maximal procreative activity , they suggest that there may be an endocrine effect on the lymphatic - mye - loid equilibrium , especially with regard to the sex hormones . stilb ' oestrol appears to have had a beneficial effect in single cases of chronic myeloid leukaemia ( loeper , lesourd and sterboul , 1947 ) and of chronic lymphatic leukaemia ( lemaire , loeper , housset and koupernik , 1947 )  . 
on admission to hospital in sheffield he was given 3 pints of packed cells and stilboestrol and penicillin therapy were begun . this was followed by an excellent clinical remission for 6 weeks , with complete disappearance of clinical splenomegaly and hepatomegaly , the latter organs having been palpable 2 below the respective costal margins at the commencement of treatment . 
no complete remissions occurred , but 3 patients had transient partial remissions . there is no evidence from this series to suggest that either the prognosis or the clinical course of acute leukaemia is altered by adding stilboestrol to other therapy . i am indebted to my medical and surgical colleagues in sheffield , to r . 
 data have been published which indicate that the average latent period for all methylcholanthrene - induced fibrosarcomas ( strong , 1948 ) and the survival time ( strong , 1950 ) of mice developing such tumours are both influenced by litter seriation . 
the latent period ( time between the subcutaneous injection of the carcinogen and the initiation or the initial growth of the ensuing fibrosarcoma ) was variouslv affected in the different strains bv the litter to which the mouse in mice of some strains ( prunt and f : of c67 x brs ) the latent period belonged . 
 ( strong , 1948 ) for the appearance of fibrosarcomas decreased in the successirn litters of the same pair of mice , while in other strains susceptibility to fibro sarcomas was relatively constant . 
the sunival time ( strong , 1950 ) of mice growing a chemically - induced fibrosarcoma ( time between the initial growth of the malig nancy and the death of the individual ) is also affected by litter seriation . 
 ' \\nen a mouse developed a fibrosarcoma in less than 100 days following the subcutaneous injection of methylcholanthrene it sunived an average of 52 days with the progressive growth of the tumour ifit belonged to a first litter . 
in the succeeding litters mice of the same age and latent i : eriod survived longer and longer with growing fibrosarcomas until , if they belonged to an eighth litter , they lived on an average of 130 days . 
these genes were derived from mice of the ancestral stocks jk and n which were used in the origin of the : xho stra the first three generations ( cba... " x jk ) were used for breeding purposes only . 
at the time of the separation of prunt from pbr descent , the average latent period for the appearance of methylcholanthrene - induced fibrosarcomas of the direct in the f 20 generation of the experimental maternal ancestry was 3695 days . 
these two untreated descents , prunt and 2prunt , should possess genetic similarity , and any biological differences that they have may be due either to divergent segregation from a residuum of genetic heterozygosity ( probably very small after 17 generations of brother - to - sistier matings ) or to new biological variability which has appeared in one or both untreated deseents following their separation from a common ancestry . 
the mice were fed a standard diet of nurishmix pellets ( pratt food company ) and water ad libitu a supplement of mixed grains ( oats , wheat and sunflower seeds ) and calf meal pellets were given to the mice once a week . 
the mice were examined periodically for tumoun ; , and the latent period taken to be the time at which a firm nodule at the site of the injection of the carcinogen began to increase progressively in si mice which developed tumours at sites other than the one at which the carcinogen had been injected were tabulated separately . 
 table i gives the percentage incidence of tumours in mice which developed in less than 100 days ( column e ) , together with the data obtained on all tumours at the site of injection of the carcinogen irrespective of latent period ( column d )  . 
 data on the total number of mice injected with methylcholanthrene ( column a ) , the number of mice which died without developing any tumour ( column b ) , and the total number of mice showing tumours irrespective of latent period and site are also given ( column c )  . 
since the two separate descents disclose similar genetic origin and show similar trends by which the females are consistently more susceptible to fibrosarcomas than the males , the data for both series may be added together . 
however , the present analysis of trends of susceptibility in s1icoessi.e litters discloses differences , and therefore the two strains , the prunt and the 2prunt , should be kept distinct . 
thus 27 2 pe : r cent of the females developed fi.brosa : rcomas within less than 100 days of latent period , whereas only 92 pe : r cent of the males developed similar tumou : rs during the same period , a difference of 180 pe : r cent in tumour susceptibility  . 
the trend for the percentage incidence of tumours developing in less than 100 days among females of successive litters was found to be y = 85 + 5 lz , with a standard deviation of the slope of 0 - 741 . 
comparison of this value with a no - trend or 0 - slope value by t test reveals that the observed trend is statistically significant ( since p = < 001 )  . 
 similarly the trend for the percentage incidence of tum.ours developing in less than 100 days among males of successive litters was found to be y = 132 - 12x , with a standard deviation of the slope c , f 0968 . 
 the analysis of the data thus discloses that there is an increasing sex differential in relation to chemically induced : fi.brosarcomas in successive litters in mice of the prunt descent . 
the difference between the mice of the two descents must , therefore , be associated with a mechanism which in the 2prunt descent changes in litter seriation at least in some strains of mice . 
 the maximal sexual differential is found in mice of the second litters ( 302 per cent ) , and this sex differential fluctuates in the succeeding litters and thus shows no significant trend . 
however , the data of the 2prunt descent are complicated by a high value for females of the second litter ( 382 per cent ) and a high value for males of the sixth litter ( 143 per cent )  . 
in one strain ( the chi ) males were more susceptible to chemically induced fibrosarcomas than were the females , whereas in the 15th inbred strain ( the cul ) the females were more susceptible to tumours than were the males . 
 the mechanism involved in the development of this new sexual differential in relation to chemically - induced fibrosarcomas in mice of the prunt descent gives a slight sex difference in mice belonging to the early litters of a breeding female , and apparently gradually increases in the succeeding litters . 
h the sex pattern of an individual is the reflection of the genetic constitution of the individua1 , then it is not clear whether mice of the early litters or mice of the later litters are to be considered the pattern for the species . 
but sex physiology is also under the influence of several hormones , and the sex pattern can be influenced significantly when a hormone is administered at an early age , preferably before birth . 
 the present investigation with methylcholanthrene has disclosed that several aspects of malignancy ( the average latent period , the survival time and the per centage susceptibility of tumours in mice of latent periods of less than 100 days ) are influenced by litter seriation . 
do hormones fluctuate in the female body with advancing litter frequency , pass the placental barrier and influence the subsequent physiology of the offspring at least in relation to malignancy and perhaps to other characteristics as well ? or are we to conclude that maturation phenomena in cytoplasm ( perhaps the mito chondria or other constituents ) are responsible for this transmission from mother to offspring which apparently is not through the genes ? perhaps another biological reason may eventually be found for the data at hand . 
these mice belonged to two separate descents derived from a common genetic orig in one descent , the prunt , there was an increasing sexual differential in relation to chemically - induced fibrosarcoma.s in the succeed320 l . 
strong. from the school of medicine , yale university , u.s.a. received for publication february 2 , 1949 . the idea of somatic mutation as an explanation for the origin of cancer has had a long and interesting history . its original use as an interpretation of cancer is usually associated with the names of murray and of boveri . these men arrived at the somatic mutation conclusion from different fields , murray from experimental cancer research , and boveri from his classical observations in experimental embryology . 
at that time he stated : " the existence of such tumours , the biological characters of which are retained through long periods of propagation , shows that the cellular transformation which initiates carcinomatous growth may take place in varying degrees . 
strong this biological alteration colours permanently their whole biological behaviour . is of such a kind that the cells are able to take up nourishment , increase in size and multiply indefinitely . 
they acquire an individuality and powers of resistance to injurious agencies superior to those of normal tissue elements . " boveri 's idea on the nature of the origin of cancer stemmed from his observations on atypical mitoses . 
he had suggested the possibility that by this means an unequal distribution of the chromosomes would ensue and thus lead to unconhe was loath to expand upon this concept until aichel trolled growth . ( 1911 ) , using boveri 's own observations on the development of the sea urchin egg , arrived at the conclusion that a malignant tumour was caused by a fusion boveri 's concept has not received wide recogof a tissue cell with a leucocyte . the essential feature of the idea is expressed in his own words ( boveri , nition . 1929 ) : " the essence of my theory is not abnormal mitosis , but in general , a however this may arise , the result definite abnormal chromosome - complex . beside the multipolar mitoses , which might would always be a definite tumour . depend either on a simultaneous multidivision of the centrosome or on distorting the parallelism between the division of the centrosome and the cell - division , asymmetrical mitosis should be chiefly considered for the origin of tumours . indeed , according to analogy with certain occurrences in sea urchins , these would depend on a lack in certain chromosomes of the power to divide ; this would result far more surely in tumour than would multipolar mitoses , which depend agencies which would act on chance for the distribution of their chromatin . most directly would be those that have the power of destroying definite chromoboveri , therefore , saw quite somes.of a cell , while leaving the others uninjured . " distinctly that irrespective of the mechanism of origin , the disturbed chromatin content is the essential feature in cellular physiology , including the abnormal condition of a tumorous growth . 
the pleomorphism of cancer cells and the irregular atypical mitoses so characteristic of their nuclei had been observed and carefully studied , however , since the middle of the nineteenth century . whitman ( 1919 ) wrote a critical review of von hansemann 's theory of aiiatyzzer ( 1916 ) expressed plasia in the origin of cancer in terms of modern genetics . the opinion that a somatic mutation may be involved in the origin of cancer . tyzzer stated , " there are marked differences in the behaviour of various tumours on transplantation in given classes of mice . 
even tumours arising in homogeneous races show such differences , and this may be attributed to the acquisition of new characteristics by the soma which are manifested in the development of the tumour . 
as a matter of fact some investigators express the opinion that tb.e two genetic phenomena are entirely antagonistic to each other . for example , a very recent article by bauer ( 1948 ) of heidelberg discusses at length that susceptibility to cancer in the human population is not inherited , and at the same time elaborates on the development of the concept that cancer arises as a somatic mutation . 
that a tendency to undergo somatic mutation may have a definite genetic basis in normal tissues has been discussed by east ( 1917 )  . this phenomenon has been encountered especially in plants , but also has been reported in the higher animals . an early example of a genetic influence on somatic mutations is discussed by whitman ( 1919 )  . 
a yellow chrysanthemum carrying white flowers on one branch . it is obvious that , since the colour of the flower is known to depend on definite factors , the development of a branch carrying flowers of a colour different from that of the flowers on the other branches could only arise through the failure of the factors to pass over , during mitosis , into the cell from which that branch developed . the branch , in other words , represents a somatic mutation due to asymmetrical mitosis . " many tumours have been described in a variety of genetic material . 
many of these tumnours are pigmented and occur especially in the early development of the individual , and some are associated with or are identical to lethal mutathese have been recorded by stark and bridges ( 1926 ) , wilson ( 1924 ) tions . and others in drosophila , by federly ( 1936 ) in lepidopterous larvae , and by many other investigators . most of these tumours are inherited by a multiple factor complex and , in the opinion of t . 
morgan , expressed to the author many years ago , at least one of the drosophila tumours arose as a mutation . time alone prevents the further discussion of this interesting genetic material and its bearing on the somatic mutation hypothesis . the next advance in the somatic mutation idea in relation to neoplastic lesions was undertaken by the present author , in 1918 . 
from that time onward until 1930 , a considerable amount of evidence was accumulated from the study of the transplantation of adenocarcinomata of the mammary gland in mice that eventually provided the first experimental evdence that a somatic mutation may be involved in the origin of cancer ( strong , 1926a , b )  . 
some of these data have been published , but a considerable amount has not . the development of this experimental approach to the nature of the origin of cancer was as follows : tyzzer and little investigated the transplantation of a sarcoma that originally arose in a japanese waltzing mouse . 
they found that the progressive growth of this transplantable tumour was dependent upon thesimultaneous presence of multiple mendelizing units strong and little , in 1920 , and later in 1924 , determined that two transplantable adenocarcinomata of the mammary gland in mice were dependent upon different genetic complexes for their continued the dbrb tumour was dependent upon the simultaneous presence of growth . two genes , whereas the dbra tumour was dependent upon the simultaneous presence of these same two genes , but required the presence , in the host , of a third gene . 
the presence of the third gene had no detectable influence on the growth of the dbrb tumnour . this geneticsimilarity and difference was obtained in the same series of mice in spite of the fact that the two tumours were histologically indistinguishable ( strong andlittle , 1920 ; little and strong , 1924 )  . the opinion of identical diagnosis was given by the late james ewing , as well as by francis carter wood . 
a third spontaneous tumour that arose in a dilute brown mouse ( given symbol dbrc ) provided evidence that six genes were involved originally in the growth of this tumour when transplanted into a series of suitable f2 individuals derived from a cross between mice of the dilute brown stock and mice of a totally unrelated stock , the well - known a stock . 
growth rates on the various transplantable tumours derived from the dbrc tumrour were determined . after several transplant generations a tumour was obtained that grew so rapidly that it was considered out of the normal range of growth for the original transplantable tumour . 
when the derived transplant was tested it was found that now its growth was dependent upon the simultaneous presence of only two genes . this sudden acquirement of growth capacity also resulted consequently in a new transplantability characteristic . 
a second sudden change subsequently took place , and a new derived ( mutant ) type of tumour would now grow in 75 per cent of all inoculated f2 mice ( observation 75 - 00 + : 23 - 002 - 79 )  . 
theprobable error difference between this newratio and the actual observation for the original dbrc tumour was 5813 per cent 3 ' 67 or 15 - 84 x p.e. this new derived transplantable tumnour continued to give a 3 : 1 ratio in a series of f2 mice for several transplant generations . eventually a new sudden change took place at which time the - new mutant type grew in practically all f2 mice ( observation 243 ' 00 + : 2 - 004 0 ' 94 )  . these new data in the f2 deviated from the ratio obtained with the original dbrc tumour as follows : 80 - 78 per cent 2 - 48 or 32 - 57 x p.e. there can be no doubt that sudden genetic changes are taking place somewhere in the relationship between the host and the transplanted tumour . since the mutant types and the original transplantable tumour were being compared in the same series of f2 mice , these sudden changes could not be taking place in the host but must be taking place within the tumour cell ( strong , 1926a , 1926b )  . another point that should also be emphasized is the fact that when the derived mutant transplantable tumour would grow in all f2 mice derived from a cross between the dilute brown and the a stocks , then , and not till then , would it grow in all mice irrespective of genetic relationship . in other words , it had lost all characteristics of tissue specificity . the transplanted tumour would grow invasively at a tremendous rate and would metastasize extensively . 
thus evidence was obtained that a highly specific , relatively benign , slow - growing transplantable tumour had progressively and suddenly acquired periodically new biological characteristics until finally it had been converted over into a carcinoma . 
toward the end of the series , however , especially at the terminal non - specific state , the tumour had become more cellular and had lost most of its original adenocarcinomatous arrangement . another series of investigations was performed on the transplantation of the 13 spontaneous tumours that mouse f1 79 gave rise to . this mouse was not only the common ancestor of the well known c , c3h , cba , c121 and chi strains of inbred mice , but also gave rise to a wealth of neoplastic tissue as follows : all 13 of her spontaneous tumours of mammary origin were tested out by trans102 l . 
and if one tumour tissue has deviated from the genetic constitution of the somatic tissue from which it arose , then possibly all tumours undergo the same process in their origin . the above phenomena especially of sudden changes taking place during the transplantability of spontaneous adenocarcinomas of the mammary gland in mice has been amply verified , not only by the investigation of the 11 other tumours derived from female f179 referred to previously , but also by many other all the phenomena of tumours derived from other mice in my laboratory . transplantation consistent with the genetic theory of transplantation were also verified by the independent work of bittner ( 1931 ) and by cloudman ( 1932a , b )  . eight years later little ( 1934 ) wrote a review on the genetic work on the transplanted tumour in mice in which he included a discussion of the somatic mutation in this paper little points out that he had outlined the genetic basis for idea . susceptibility and nonsusceptibility to transplanted tumours in 1914 ( little , 1914 )  . 
he states again in 1934 that " the bit of tumnour tissue to be transplanted has a genetic composition , which is determined by that of the animal in which it if this idea was exclusively true , then it is obvious that a somatic arises . " mutation could not have been involved in its origin since any mutational process it is indeed true that in the should alter or change the original genetic state . early transfer generations , the transplanted tumour derived originally from a spontaneous source does retain the characteristic of tissue specificity determined by the genetic constitution of the mouse , inthat it will grow only in individuals which are genetically related to the mouse that gave rise to the tumour . 
but it has now been definitely proven that this phenomenon of tissue specificity is periodically and progressively lost by sudden changes resulting in simpler and simpler mendelian ratios , until eventually the tumour retains no or very little tissue specificity which it originally had . these sudden or mutational changes have always produced more and more malignancy , as determined by percentage of takes , growth rate and eventual invasive and metastatic characteristics . has also been indicated that no two tumours , even though they be derived from the same mouse and present the same histological appearance , ever showed the same mendelian ratio when transplanted into a series of appropriate f2 individuals . 
when two transplantable tumours were derived from - the same mouse , some of the genetic complex involved in their successful transplantation is common to both tumours , whereas some are unique to either the one or the similarity of genetic transplantability complex indicates genetic other tumour . in this particular little 's concept of 1914 is relationship of origin for tumours . it is also evident that the more recently chemicallytherefore partially correct . induced tumours show , from their very origin , on an average , more malignancy , and thus less tissue specificity than do the spontaneous tumours that arise in it is probably true , although at present the same series of inbred or hybrid mice . impossible of proof , that there is some genetic mechanism within cells that determines to some extent normal cell relationship , but that under certain conditions this controlling genetic mechanism alters or changes , and by so doing permits an uncontrolled or cancerouscondition to arise somewhere in the biological this phenomenon of break of co - ordinating influence of system ( the organism )  . a definitive part is , i believe , the essential feature in the origin of cancer . 
strong following the experimental evidence reported by strong ( 1926a , b ) , and verified later by bittner ( 1931 ) and by cloudman ( 1932a , b )  . little ( 1941 ) stated the problem in different terms from those he used in 1914 . he now states : " in accepting as a working hypothesis the statement that cancer ilfils the requirements of a somatic mutation , namely , a sudden change which is perpetuated in succeeding cell generations , it must be noted that there are already on record two distinct general types of somatic mutation , either of which might be involved in the appearance of cancer . 
the other has a sporadic etiology dependent on various influences which affect individual cells or groups in the first category belong such cases as mutations in colour of cells directly . genes in rodents described by castle , pincus , bittner and others . 
one of castle 's cases is particularly interesting in that it shows several cases of mutations occurring in several generations of a single family of rabbits , thus indicating a definite cases of the second type have been recorded as the result of genetic basis . lockhart - mummery ( 1934 ) has published a exposure to radio - active agents . " book on mutations and cancer , and there have been several other articles dealing with this problem . these cannot be discussed at this time . the disovery that carcinogenic compounds can induce mutations when injected into suitable experimental animals has not originated the idea that cancer may arise by a process of somatic mutation , but rather has reopened interest in an old concept . 
some experimental evidence , although of an indirect nature , has been obtained , and it is clear that there is no evidence contrary to such a somatic mutation concept . 
on the other hand , the somatic - mutation theory hardly explains the embryonic features of malignant tumours ; and it does not explain why growths are more frequent in older than in younger individuals , because it has not been observed that mutations in cells of the gonads are more frequent in older than in younger persons . 
by this means he has reported many mutations ( notably sex - linked lethals ) with the carcinogenic hydrocarbons , and has stated that he has obtained a few chromosome breaks in his experimental material . it is an established fact that the term mutagenic is not an absolute characteristic for any physical or chemical agent . for example , it may be said that x - rays are a powerful mutagen . they are very effective in inducing mutations in drosophila and in neurospora , and to acertain extent in maize , but do so very poorly in mice . 
on the other hand , ultra - violet light appears to be more effective in inducing mutations in maize than in drosophila . again it must be taken into consideration that the different physical and chemical agentsbring about mutations in various ways . x - rays break chromosomes , thus leading to rearrangements of parts , transpositions and inversions , to deletions , etc . ultra - violet light , however , seems more effective in inducing point mutations in both corn and drosophila , possibly by a specific wave - length , 2600 , that is selectively absorbed by the nucleoproviding proteins of the chromosomes . 
strong sex ratios and in distorted mendelian ratios which may be later proven to be chromosomal , but so far all mutations induced by methylancholthrene in mice finally , the which have been tested have been proven to be point mutations . mustard gas derivatives , the fourth group of powerful mutagens seem very effective in breaking chromosomes , producing embryonic disturbances very similar to the effects of x - rays , but apparently may have another action on mutagenesis , since they appear to affect cells even before there be any evidence of cell division ( action therefore similar , but possibly different from that obtained with x - rays )  . carcinogenesis again is a relative rather than an absolute property . 
on the other hand , other species are extremely liable to great resistance to experimentally for example , the rhesus monkeys in new haven have been induced tumours . injected with methylcholanthrene for 15 years without producing a single neoone must conclude , therefore , that for this species methylplastic tumour . cholanthrene is not a carcinogen , or at least , if it is , the evidence for such a conclusion is still not available . 
the problem is even more complex than this , as will be indicated in the following discussion . not all of the biological variants obtained in mice with methylcholanthrene are genetic . 
the somatic mosaic may be due to a chromosomal aberration rather than a point mutation in somatic differentiation , although the actual mechanism involved in their origin cannot be determined . we have obtained , therefore , a multiplicity of biological effects when methylcholanthrene has been injected into a series of mice over many generations . whether all these phenomena are due to the original methylcholanthrene or to one or many of the derived metabolites is still not known . 
some of these effects are definite point mutations , some are non - genetic , some are non - genetic produced possibly by inhibitions of embryonic morphogenesis at critical periods , and other biological effects may have other mechanisms in their origin , such as abnormal distribution of chromosomes during morphogenesis . but these mice whose ancestry has been injected with methylcholanthrene for many generations are not only giving rise to a wealth of biological effects , but also to a great variety of cancers . 
the first genetic result was the production of germinal mutations which changed the rate at which fibrosarcomas appeared at the site of injection of methylcholanthrene ( a decreased latent period )  . 
the second genetic effect was the production of spontaneous lesions involving the mucus - secreting cells of the gastric mucosa following the induction of this same gastric lesion from the subcutaneous injection of methylcholanthrene . 
the appearance of this specific type of pathological lesion was brought about by a mutation on the " brown tagged " chromosome . several new sudden changes have appeared in the gastric lesion subline changing the latent period for the appearance of the lesion - a phenomenon that was obtained in the transplantation of adenocarcinomata of the mammary gland in mice and discussed in this same paper . 
bartholomew 's hospital , and the statistical research unit of the me - dical research council , london school of hygiene and tropical medicine . received for publication february 20 , 1951 further data on the arsenic content of cigarette - 3 . in an earher paper ( daff and kennaway , 1950 ) data were given for the arsenic content of 5 brands of cigarettes of british and american types , of 8 brands of turkish type , and of two - others ( french , rhodesian ) , and also for the amount of arsenic volatilized in smoking . 
and germany are those of saglam ( 1944 ) from turkey and of dungal ( 1950 ) from iceland . ( 4 ) population by aores . ( 2 ) number of autopsies showing cancer . the data which one would like to obtain from any given country are : a . 
from univer8ity clinic8 ( for men and women separatelv - preferably by ages )  . - ( i ) number of autopsies . number of autopsies showing cancer of lung . in the countries where a ( 5 ) is not available one must rely on b . 
le hastaliklari klinigi in 23 months ( among 2084 patients , 53 in a thousand )  . " cc all these statistics show that in our country , within the last 30 years , pulmonary carcinoma has increased in a great proportion . " saglam rejects cigarette - smoking as a factor in the incidence of bronchial " some authors believe that there exists a relationship between carcinoma . smoking tobacco and inhahng the smoke and pulmonary carcinoma . 
we do not hold for a long time , at least since 50 years , almost only cigarettes the same view . in spite of this the increase in pulmonary ca . 
kennaway data for 1934 and have removed 3 cases , all in men , described as benign tumours , from the total of primary lung tumours ( a chondroma in 1935 , another in 1939 , and a polyp in 1937 )  . 
the official figures for tobacco consumption ( hutson , 1937 ) and for population ( statesman 's year book , 1931 ) indicate an annual consumption of about 17 lb . 
he writes that the kinds of tobacco smoked in yugoslavia ( b ) type hercegovina ( cigarettes ) ; and are : " ( a ) type makedonija ( cigarettes ) ; ( c ) type vojcodina ( pipe and cigars )  . " these are of the oriental type , i.e. , they have a natural ' bouquet ' which gives the tobacco type makedonija . " only in the north - western part of yugoslavia there are smoked cigars and pipe . 
use of tobacco for snuffing is quite insignificant . before the last war the only import was some dutch tobacco for cigars - ; during the war some bulgarian and after it some american tobacco ( through u.n.r.r.a. ) was imported , but all these amounts were very small . we are also indebted to kosir and to f . 
among 20 , 681 autopsies , there were 3584 cases of cancer and 276 cases of cancer of the lung . these figures are compared with those from other countries in table ix . ( 3 ) it is , however , not necessary to be dependent on hospital statistics for an estimate of the incidence of cancer of the lung in switzerland , as vital statistics are available for - the whole country . 
the calculated death rates from cancer of the lung are shown in table x . the national figures are reasonably reliable ' as , according to jakobsen , " the doctor who has treated the deceased during his last illness is required to which must be fill in an official certificate stating the cause of death stated in medical terms as precisel.v as possible , and it is not permitted to use general diagnoses such as " disease of the heart " or " disease of the lungs . " the 16fl ravii i 12 . 
kennaway clearl no exact proportionaht however , reasonably close to the difference in cigarette consumption . in switzerland tobacco consumption was much the same as in england and wales , but death rates were only half as high . differences in cigarette consumption again agree with the differences in death rates better than do differences in total tobacco conthis is because a much smaher proportion of the tobacco is consumed sumption . in the form of cigarettes in switzerland than in england . has been found in the data so far available between the amount of tobacco smoked and the prevalence of cancer of the lung cancer of the lung appears to in different countries and at different periods . increase more rapidly than does the use of tobacco ; such a change in effect may occur at a certain level in the dosage of a drug . 
the figures from a single hospital in yugoslavia suggest an incidence of cancer of the lung comparable to the british figures of 30 years ago . we have no figures for the incidence of cancer of the lung upon the whole population of any east european country . 
the e - vidence available at the moment is against the direct carcinogenic importance of tobacco smoke , because it tends to exclude the two most obvious carcinogens , arsenic and benzpyrene , which one might expect to be present . 
known carcinogens is now so wide that one must consider other possibilities . ( 3 ) all the older data about cancer of the lung must be reviewed in the light of this connection with smoking ; one must reconsider the inverse relationship with sunhght ( stocks , 1947 ) and the very low incidence upon a rather curious - assortment of occupations , namely , agriculture , coal - niining , and mule - spinning ( kennaway and kennaway , 1947 )  . 
one cannot answer this question at present , but it is especiary important in countries where smokers buy the cheaper pipe tobacco to make their own cigarettes . norway one obtains in this way nearly twice as many cigarettes for a given sum ( jakobsen , personal communication )  . 
the incidence of cancer of the lung upon the two sexes is not very different ( death rate , male to female , i : 07 ) ; it is greater in urban than in rural districts , and this difference is greater in men than in women . 
the increase in mortality in the last 20 years has been greater in men than in women , and greater in the towns than in the country . ( 5 ) in sweden , snuff makes up a much larger fraction ( one - third in 1949 ) of the total tobacco products consumed than is recorded in other countries . ( 6 ) a comparison is made of the data available for the increases since 1931 in ( a ) deaths attributed to cancer of the lung , and ( b ) in the consumption of tobacco , in england and wales , norway and switzerland . 
the consumption of tobacco per head has been for the last 10 years rather higher in switzerland than in the united kingdom , and in norway has been about one - half that in the other two countries , while the crude death rates at the beginning and end of the period were m . 
kennaway rou - ahlv in the proportion of i 0 ( england and wales ) to 5 ( switzerland ) , and 2 cigarette consumption was approximately in the proportion of 4 ( norway )  . ( england and wales ) to 2 ( switzerland ) and i ( norway ) and was more in accord with the relative death rates . 
the increase in the number of deaths has been about the same ( twofold ) in all three countries , but the increase in consumption oftobacco and cigarettes has , been ' less . 
the differences in the incidence of cancer of the lung are therefore quite different in extent from those in the quantity of tobacco consumed ; they are m ' ore hke ( though stir different from ) those in the quantity of cigarettes consumed . 
the study of the relation between the national consumption of tobacco and the national incidence of cancer of , the lung has scarcely begun . we wish to thank saglam and prol p . 
causes an almost complete cessation ofepidermal mitotic activity , and the same effect is caused by phloridzin , which interferes with the phosphorylation of sugar . since insulin and phloridzin both exert their mitosis depressing effect bv reducing the availabifity of sugar , it appeared probable that a similar depression would also be induced bv starvation . 
12 hours of starvation the blood sugar level remained fairlv high , but the drop in the mitosis rate was pronounced . however , during the afternoon sleep period there was a marked rise in mitotic activitv at 14.00 hours to a figure of 4 - 1 0 - 35 , which is about half the figum reachc ; l by the well - fed controls . - after 24 hours ' starvation the blood sugar level had faren seriously , and mitotic .1gain , however , there was a slight activitv had reached a very low level . response to the period of rest , so that at 14.00 hours a figure of 2.0 0 - 21 was this is about a quarter of the figure for the control animals obtained . ..a&r 36 hours the blood sugar concentration had dropped to 100 mg . 
observations were next made on the effects of such diets on epidermal mitotic acti - %ity . in prehminary experiments determinati ' ons were made of the dailv food intake of threeor four - monthold strong cba males which were allowe ; 1 to feed ad libitum on a diet of rat cake . 
13ttllo ' ug14 66 per cent diet remaitied active aiid in excelleiit health , btit those which received a 50 per cent diet showed sigiis of ill - health , and it is dotibtftil whether they could have stirvived the treatnieiit for i - iiore tliaii another few ' weeks , at the end of the experiment at 20.00 hours all the niice wei - e killed and blood sugaiestimations were made . 
that middle age is characterized bv a generallv raised mitosis rate which must itself assist in the development of any latent tumour cells which may be present . ll ' hfle the reason for the increased initotic activitv is still obscure . 
this observation mav afford some explanation of the fact that middle age is characteristically the cancer age . since the development of latent tumour cells is assisted bv conditions of hyperplasia , it is reasonable to suppose that conditions of hypoplasia wih have the hyperplasia increases the chances that the latent tumour cells opposite effect . will be stimulated to multiplv . 
and so delavs the development of those tumours which do forand prevents altogether the appearance of manv which otherwise would forthus it is possible to provide a logical explanation of tannenbaum 's re - sults . 
and the fact that carbohvdrate - supply is the critical factor in both cell division and tumour genesis can be taken as corroborative evidence . at last it iis becoming possible to split the cancer problem into two separate parts : that which is coneemed with the formation of latent tumour cells . 
but it now appears possible that a practical control of cancer mav be developed from a thorough understanding of those factors which govern normal cell division . if hypoplasia can be maintained without damage to health . 
and reveal fewer pathological changes in the tissues . " this mav well be related to , the fact that hypoglyeaemia not onlv reduces the rate of cell division of a host . but also that of a parasite . 
a sin - iilar effect is produeed bv restricted diets . - kninials rationed to 66 per cent of what thev would eat if fed .4 , libitunt have an epidermal mitosis rate which is less than 40 per cent of that of well fed controls . if rationed to 50 per cent . 
the mitosis rate dxops to about 15 per cent of that of the controls . it is suggested that these observations provide an explanation of tannenbaum 's results on the prevention of tumour genesis bv diet restriction . 
mottram ( 1945 ) published the results of experiments designed to demonstrate a relationship between the tumour yield induced by benzpyrene and the number of epidermai mitoses present at the time of application of the carcinogen . painting the skin of rnice at midnight resulted in a higher yield ofpapillomata than did painting at midday . 
the concentration of aaf in the food was 0.03 per cent for 5 weeks and then 0 - 05 per cent for 20 weeks , the total period of administration extending over 25 weeks from october , 1945 , to april , 1946 . thereafter the mice received the standard diet of rat cubes for the rest of their lives and the control mice received that diet throughout . all mice had an the experiment was terminated in unrestricted - supply of food and water . the eighty - fourth week by killing the mice then surviving , namely 2 males which had eaten aaf and 3 control males . several attempts to control the localization of tumours were made on small during the third to sixth weeks of experiment 5 females of groups of mice . the aaf group and 5 control females were mated with vasectomized males and silk threads were tied in the pseudo - pregnant uterine horns to elicit deciduomata . in the twenty - second week of experiment , pellets containing 25 per cent of diethylstilboestrol ( b.d.h. ) in cholesterol and weighing 5 or 6 mg . 
the stilboestrol pellets shortened life , the testosterone tablets were harmless ; especially by causing pyometra . their possible effect on the induction of bladder tumours is mentioned below . granulation tissue , fibrosis and abscess were found in uterine horns where silk threads were tied but tumours were not recognized there . " spontaneous " tumours were found in 3 male control mice as follows : osteogenic sarcoma of the thigh , with secondary deposits in liver and lungs , in the forty - eighth week ; hepatoma in the sixty - third week ; and lymphoma in the sixty - eighth week . 
the average time was 50.7 weeks , but 8 of the tumours only 1 tumour occurred were found from the thirty - ninth to forty - sixth weeks . in an effective total of 8 mice carrying testosterone tablets ; 6 of the mice survived from 58 to 64 weeks without tumours . 
the incidence as a percentage of the effective total was 12.5 for aaf males with testosterone tablets , 73 - 3 for aaf males without testosterone , and 52 - 2 for all aaf males . most of the tumours were intravesical , pedunculated or sessile papilliferous tumours of transitionalor squamous - cell types , and conformed with the descriptions of armstrong and bonser ( 1944 ) , who distinguished benign and malignant forms but observed no extra - vesical extension . 
the distribution of tumours amongst these and less common sites depends on the species and on the strain of the animals used ( bielschowsky , 1946 , 1947 ; armstrong and bonser , 1947 ; dunning , curtis and madsen , 1947 ; harris , 1947 )  . harris concludes that " the site at which tumours may be induced by fluorene compounds is probably determined by the genetic constitution of the rat employed . " this statement , though true , is not a definitive explanation . 
the genetic constitution determines how particular cells react to particular stimuli ; remains to determine what reactions are iminportant in the production of tumours by acetylaminofluorene and how the reactions are variable in kind or degree . the importance of the genotype is accepted ; the urgent task is to elucidate its phenotypic expression . carcinogenic hydrocarbons affect tissues remote from the site of application and increase the incidence of certain tumours , notably tumours of the breast , long adenomas and leukaemia . 
many observations , summarized recently by enge ] breth - holm and rask - nielsen ( 1947 ) , suggest that the action is , essentially , an acceleration of spontaneous tumour development . 
some actions of acetylaminofluorene may be attributable to acceleration of a spontaneous disease as , for examnple , the increase of mammary tumours recorded by armstrong and in my experiment the evidence for an increase in the naturally high bonser . incidence of breast tumours in r3 mice was not decisive , and acetylaminofluorene did not accelerate or increase the incidence of lymphoma or sarcoma which occur , uncommonly , in normal r3 mice . 
the unequivocal effect of aminofluorene was the growth of tumours of the bladder which are not found in normal controls and which , as yet , have not been induced in mice by other carcinogens ( bonser , 1947 )  . in some strains of rats , acetylaminofluorene notably induces carcinoma of the external auditory canal , previously unrecorded . these and other comparable observations show that tumours induced by acetylaminofluorene do not grow preferentially in tissues prone to develop " spontaneous " tumours and are not accelerated " spontaneous " tumours . 
foulds hepatoma is much less frequent and , as my observations show , develops later than tumours of the bladder by about 20 weeks - a substantial fraction of the life of a mouse . consequently , intercurrent diseases , mammary tumours in females or bladder tumours in males kill most r3 mice before the response of the liver to aminofluorene is manifested by the growth of hepatoma . 
some geneticists maintain that the processes directed by allelomorphic genes differ only in speed . speed of reaction is probably one of the most important expressions of the genetic factors which govern the distribution of the tumours induced by acetylaminofluorene . 
the high and relatively early incidence of mammary tumours in female r3 mice presumably reduces the opportunities for other tumours to become evident , but it does not account for the complete absence of bladder tumours from the females in my experiment , or for the lower incidence in females compared with males in the 5 strains studied by armstrong and bonser . 
tumours of the bladder grew in about half the male mice which survived 9 months or longer from the beginning of the experiment . testosterone seemed to inhibit the induction of bladder tumours in males and none grew in females . 
jackson memorial laboratory , bar harbor , maine . received for publication april 20 , 1954 in a comparative study of alkaline phosphatase in tumors , greenstein ( 1942 ) noted that the mouse tumours studied possessed little or no alkahne phosphatase activity with the exception of spontaneous mammary tumors and lymphomas . comparative q values were calculated as the ratio of the percentage of disodiumphenyl phosphate hydrolyzed to milligrams of total n per cubic centimeters of several concentrations of n were taken and the q values remained tissue extract . remarkably constant in relation to nitrogen . 
the highest value for any tumor was the transplanted hepatoma 31 in rats with a q value of ' 542 . kabat and furth ( i 941 ) could not demonstrate alkahne phosphatase by means of gomori procedure in mammary adenocarcinoma spontaneously arising in c3h however , hard , pratt - thomas and belkin ( 1948 ) examined twenty - nine stock . spontaneous mammary carcinomas in c3h , a and dba mice and noted high alkaline phosphatase activity . 
the predominent picture in the mouse tumours examined was the high alkahne phosphatase activity shown by the cells of the acinar units while the stroma and vascular elements were free . 
descenden ' t of a mouse that was bom from a fertilized ovum transplanted into the uterug of a dba mouse this has gone through 320 transplant and was nursed by her dba mother . results from the jackson laboratory indicates 100 per cent transgenerations . plantability in c57bi , and their f , hybrids . 
the histological type is an adenocarcinoma ( sneh , cloudman and woodworth , 1948 )  . the tumor h2712 originated spontaneously in the mammarv gland of ' a c3h mouse in 1948 at the roscoe b . 
the histological type - is an adenocarcinoma . the tumor dbrb originated in the department of genetics , carnegie institute of wasliington in 1918 in the mammary gland of a dba / i mouse and has gone throuo ' h 845 transplant generations . refjults from the roscoe b . 
the histological type is an adenocarcinoma ( strong and little , 1920 ; ' little and strong , 1924 )  . the tumor 15091a originated in the laboratory of the university of a - fichigan in the mammary gland of an a albino mouse in 1928 ( cloudman , 1928 )  . this has gone through 341 transplant generations and shows 100 per cent transplantability in a albino and their f , hybrids . 
the histological type now is that of an anaplastic carcinoma . for the purposes of the experiment the animals were divided into four serieg . series 1 consisted of tumor e0771 transplanted into males and females of c57bl and their f , hybrids between c57bl and a / l . series ii consisted of tumor h2712 transplanted into c3h males and females . series iii consisted of tumor dbrb transplanted into dba male and female . series iv consisted of tumor 15091a transplanted into f , hybrids of c57bl and a / he male and female . the total number of animals of the four series were i 00 and 8 1 . all mice were transplanted with their respective tumor at the roscoe b . 
jackson memorial laboratory and sacrificed at intervals between 7 and 22 days or an average of 16 davs . the am - mals were kired by ether anesthesia and thin slices of the ever , spleen , adrenals , kidney , testes , ovary and the tumor were placed immediately into formoltissues placed in fo ' rmol - saline were stained saline and into ice - cold acetone . by the regular hemotoxyliin and eosin methods . tissues placed in ice - cold acetone were left for 24 hours with one change of acetone . 
they were then placed in cold absolute alcohol over night followed by two changes of benzol of 45 minutes e " ach . they were then imbedded and infiltrated in paraffin at 56 ' c . 
they were then dehydrated and mounted in permount . incubation times in the substrate were as follows : series 1 , ily ill : i minute , 5 miinutes , 15 minutes and 1 hour , and series iv : i.minute , 5 minutes , 15 minutes , i hour , ij hours , 2 hours and 21 hours . 
a total of 1124 shdes was prepared . the shdes were read and visually graded according to their intensities from i to 6 . in this way a relative assay could be arrived at which showed a distribution within each incubation time , and the earliest reaction or end point could be ascercontrols were run . 
at i minute incubation time 29 of the 39 reactions had a reaction intensity of one and hence this was considered as the " end point . " at 5 minutes there were no negati ' ve reactions , the majority of reactions being two or three . 
the distribution was , however , strikingly different from the other tumors and will be referred to in the subsequent section . series iii consisted of 48 transplanted dbrb mammary carcinomas . 
l. - tumor e0771 transplanted into c57bl and f , hydribs ( series i )  . alkaline phosphatase reaction at 15 minutes ' incubation tixne slides show irregular areas of activity . 
3. - tumor dbrb transplanted into dba ( series iii )  . alkaline phosphatase reaction at 15 minutes ' incubation tixne shows a tendency of the peripheral cells of islands to show more activity than central portion . 
7. - tumor h2712 transplanted into c3h ( series ii ) under high power magnification . note the peculiar and intense distribution at the borders of cells lining the lumens . in the center is also seen gomori positive acerular material in a very small lumen . 
4 , 5 , 6 at 60 minutes incubation period . it is quite evident that 1.5091 a exhibits no alkaline phosphatase activity and further extension of the incubation time to 2 - 1 hours showed no reaction except in the vessels . in series i tumor e0771 is composed of irregular islands of tumor tissue . these varv in size and shape . 
the islands are fairly solid with the exception of small areas where itimens can be seen . larger iiimens are lined by several rows and layers of cells . most of ' the lumen8 are very small . 
8 shows a photoreticular material with many large thin - walled vessels . micrograph of this tumor stained by hemotoxyl - in and eosin showing the islands of the interstitiat tumor tissue with an attempt at luminal and tubular forma - tion . tissue seen to the left is loose and reticular in nature . there seem to be attempts to form tubular structures . the phosphatase reaction began during the first minute of incubation time with a blackening or graying of the cytoplasm . this gave a gray appearance to the slide except in such areas where the blackening is much more pronounced . 
at this time enzyme activity large irregular can be demonstrated in many areas in the centres of the island . clefts can be distinguished and stand out prominently bv the activity of the enzyme of the cells lining the lumens . intraluminal material which is not apparent in the hemotoxylin and eosin preparation shows intense activity . small globules are present in the cytoplasm of many cells adjacent to lumens or attempted lumen formation . 
the connective tissue and vessels do not react . tumor dbrb iin series iii under hemotoxylin and eosin stain shows a more lobular distribution than either e0771 or h2712 and is shown in fig . 
the interstitial tissue is composed of loose connective tissue , connective tissue and large thin - walled vessels . with graded gomori stains the reaction has an " end point " at 15 minutes . here the areas of activity are irregular thoughout the tumor . 
some activity is there is a tendency for present in the small lumens but this is not marked . increased activity at the periphery of the lobule as shown in fig . 
the loose supporting connective tissue and vessels show no activity . in series iv tumor 15091a differs somewhat from the other 3 in that it is a fairly solid tumor not composed of islands or lobules . there are numerous mitosis and the cells vary more in size and shape . 
at i hour this showed rather marked activity . the cells of the peripheral portion of the nodules showed most intense activity . there is no essential difference between the various series . the liver shows , for the most part , two types of reaction . 
the ovary begins in most series with the 5 minute incubation time in the theca externa which shows progressive activity to i hour . ksmall stromal vessels also show activity . all the series were approximately the same . 
one difference that occurs in the e0771 is the presence of doubl - e layers of tumor cells in the attempt at acinar formation . in the 15091 a the tumor is solid with very few smar acini . the overall phosphatase reaction was very intense in e07 7 1 , very much less in this was evident in spite of the fact that h2712 and bdrb and none in 15091a . the rate of growth of the tumor was about the same in all the series . 
numerous hard , pratt - thoma 's and belkin ( 1948 ) mitoses were present in all the tumours . felt that there was a loss of alkahne phosphatase activity in the more anaplastic although it would seem in our series that the anaplastic tumor tumor cells . 15091a having no reaction would point toward such contention , the e0771 is a very rapidly growing tumor with numerous mitoses . 
we would prefer to delay our judgment on this issue until a larger variety and strains of tumors have been studied . an interesting and significant paper which has come to our attention as this work was completed was the observation of shelton ( 1952 )  . this investigator found a tumor in a 6 - month - old strain a female mouse that had been exposed to 400 r whole body x - radiation on the date of birth . 
lymphoma 1 was propagated in a mice from a large tumor mass located in the anterior mediastinum . lymphoma 2 was propagated by subcutaneous injection into strain a mice of fragments of lymph nodes from a mouse bearing the original tumor . strain i grew as a localized tumor with local invasion ' but no metastasis , but strain 2 reacted as an acute leukemia with rapid growth infiltration of the organs and high peripheral count . in determination of the alkahne phosphatase activity it was found the lymphoma 1 showed no reaction while lymphoma 2 showed a reaction as expressed by 5 mg . 
no detectable reaction could be seen by the gomori method in lymphoma i whereas lymphoma 2 was here we have a rapidly growing persumably anaplastic tumor strongly positive . showing an increase in alkahne phosphatase reaction . in our laboratory we have also determined the alkahne phosphatase activity as expressed in gamma of phosphorus per mflhgram of nitrogen at 30 minutes incubation time in a large series of these 4 mammary tumours . 
daab seemed to interfere with vitamin - a storage and hence to cut down food consumption , leading to a deficiency of some other kind , such as that suggested by zucker , berg and zucker ( 1945 ) , which was the immediate cause of the forestomach lesions . the present author ( 1947 ) was , however , unable to elicit such lesions in the stomachs of stock mice given daab orally , even up to 294 days , in either a balanced or one type of unbalanced diet . 
he concluded that otsuka 's diet ( which was grossly deficient in several essentials ) allowed a deficiency not existing in his own diets but necessary for eliciting such forestomach lesions in mice . he also found no tumours in similar mice injected subcutaneously with daab in arachis oil , on three occasions , up to 329 days after the first injection . 
daab thus appears not to be a carcinogen for the subcutaneous tissues of mice . hiowever , in another experiment which apparently broke fresh ground , the present author applied daab in acetone , in increasing strengths , to the nape of the neck of stock mice , and obtained two squamous carcinomas , one with spindlecell metaplasia , in 2 of 8 mice surviving 346 days or more . this seemed to be sufficient grounds for classing daab as a carcinogen for the skin of mice . a further series of experiments has now been carried out to check the previous findings with daab painted in acetone ; at the same time , the effect , if any , of added croton oil was investigated . 
at the commencement , all mice were painted with the solution containing croton oil ; after 15 days , the croton oil was withdrawn . croton oil was re - introduced for one - third of the mice after a further 167 days , and the experiments therefore fall into two groups : ( a ) initial croton oil , and ( b ) initial - plus - subsequent croton oil . applications were made to the nape of the neck , after clipping away hair , thrice weekly for a total period of 545 days . the basal diet throughout was rat - cake ( thomson , 1936 )  . ( a ) initial croton oil series . - the survival rates of mice surviving more than 200 days are shown in fig . 
kirby the commencement of painting ; of these , two showed acute yellow atrophy of hyperthe liver and one showed slight hyperkeratosis at the site of painting . keratosis , with or without necrosis or ulceration , was common after 200 days , but the first papilloma was found in a mouse killed after 320 days ' painting ; this papilloma grew as a coxcomb - shaped wart . 
the other mouse had a similar , though smaller , lesion which also proved to be a squamous carcinomna of low - grade malignancy . although a mouse dying after 435 days showed no gross abnormality at the site of painting , another dying after 449 days had two tumours in the painted area ; one of these was found to be a squamous carcinoma with invasion down to the depth of the muscle . 
a necrotic , warty outgrowth , showing parakeratosis beneath , and a multiple papillary growth , were found at the site of painting in mice painted for 495 and 545 days respectively , the latter dying at mice dying at 524 , 528 and 588 days , i.e. 
33 days after painting was stopped . 549 days respectively showed nothing more than a little hyperkeratosis at the the last survivor and one of the mice from group ( b ) unfortusites of painting . nately died at the same time ( 611 days ) and were examined post - mortem in the absence of the author . 
one of these mice showed early squamous carcinoma , and the other simple infected ulceration ; as there is no way of deciding which histological report belongs to which mouse , they will be excluded from consideration in comparing the results in the two groups . 
a mouse dying at 623 days showed no lesion at the site of injection . thus in 16 mice surviving more than 300 days ' painting with 5 per cent daab in acetone , 3 developed simple papilloma , and 3 others developed squamous hyperkeratosis and / or ulceration was found carcinoma , at the site of painting . in nearly all the rest . abdominal organs were only examined histologically when gross damage was visible , but the male dying at 449 days and one of the mice dying at 611 days showed amyloid changes in spleen , liver and kidney similar to those referred to in the previous paper ( kirby , 1947 )  . 
the mouse dying at 623 days showed pulmonary adenoma . ( b ) initial - plus - subsequent croton oil series . - survival rates , beyond 200 days , only slight are shown in fig . 
1. hyperkeratosis was found at the site of painting in 4 mice dying at 215 days and in 1 dying at 305 days . of 3 mice dying at 435 , 442 and 443 days respectively , all had papillomas , keratinized and partly necrotic , at the site of painting . 
of 17 mice painted for more than 400 days , 5 developed squamous carcinoma , and 5 others squamous papiiloma , at the site of painting , a tumour incidence of 60 per cent . 
the malignancy appears to have been low - grade in all cases , and metastases were never found . no evidence of spindle - cell metaplasia was seen in this series . 
as this substance is an intermediate in the manufacture of p - aminoazobenzene , the possible danger to workers handling it , especially in organic solvents , must not be overlooked . induction by daab of tumours at sites remote from that of application seems to be confined to the lung . 
no tumours were found in the liver of any mouse . co - carcinogen tests : neither the incidence of skin carcinomas - 3 / 11 ( surviving 400 days ) in group ( a ) and 1 / 5 in group ( b ) - nor the time of appearanceabout 400 days in either group - lends any weight to the view that croton oil acted as a co - carcinogen when applied concurrently with daab in group ( b )  . on the contrary , it would seem that croton oil had no effect either way on the induction of skin tumours . this suggests that the mechanism involved in carcinogenesis by daab differs from that of the polycyclic hydrocarbons . 
croton oil painted concurrently caused no increase in the incidence of the significance of the skin tumours , nor did it decrease the latent period ; absence of co - carcinogenic action of croton oil is discussed . the author is greatly indebted to p . 
kirby. from the research department , glasgow royal cancer hospital . received for publication , june 28 , 1984 . activity the carcinogenic of orally - administered 2 - acetylaminofluorene , aaf , for a number of tissues , mainly epithelial , was first demonstrated by wilson , deeds and cox ( 1941 ) for the rat , and subsequently confirmed for this species by bielschowsky ( 1944 , 1946 ) and others , for mice of various strains ( armstrong and bonser , 1944 , 1947 ; foulds , 1947 ) , for the fowl ( bielschowsky and green , 1945 ) and for the cat ( harding , quoted by bielschowsky , 1947 )  . recently wilson , deeds and cox ( 1947a ) have reported their own findings in mice of three pure strains . 
aaf has now been shown to be a carcinogen ( when given per os ) in eight strains of mice : cba , if , riii , white label , strong a , c57 black , c3h , and bagg albino . 
of the first five strains mentioned , cba were most prone to both liver and bladder tumours ; strong a were the least susceptible ( armstrong and bonser , 1947 )  . 
mark 's hospital , london . received for publication december 29 , 1949 . it is well known that different histological types of cancer vary in their rate of growth and liability to metastasise , but this relationship between histology cancer and spread is easier to study in some organs of the body than in others . of the intestine provides exceptionally good material for investigating this question becauise ; surgical operations are planned to remove a good stretch of bowel above and below the tumour as well as a wide field of lymphatic drainage in the mesentery . 
it happens , therefore , that the pathologist is presented not only with the tumour , but ' also with its surroundings , so he can first classify the tumour according to ' its histology , then measure the extent ' qf local spread by direct continuity , and finally record the number and position - of lymphatic metastases . when the histology and spread are compared in ' this way it soon becomes obvious that different histological ' varieties often behave differently , but a fairly big series of cases must be examined in order to express these differences quantiit takes a long time tatively and give them anything like precise significance . to collect many cases of cancer of one organ of the body such as the bowel at a general hospital admitting patients of all sorts , ' but this is done much more quickly in a special hospital like st . 
mark 's , which is intended primarily for in the last 21 years ( 1928 - 1948 inclusive ) diseases of the rectum and colon . 3 , 220 operation specimens of intestinal cancer were examined and dissected in the laboratory of st . 
mark 's hospital , the general distribution being as follows : 2 , 642 cases of cancer of the rectum , 429 of the colon , 51 of the anal canal , and 98 cases of multiple malignancy . in each case the records describe the extent of local spread and the n ' umber and position of all lymphatic metastases . preparation for this paper i ' have re - examined the sections of all these tumours and compared their histology ' and their local and lymphatic spread . since rectal cancer is much the largest of these groups , forming 82 per cent ' of all cases , it will be convenient to start with this . histological varieties of rectal cancer . the three main histological varieties of rectal cancer are adenocarcinoma , colloid ( or mucinous ) carcinoma and an undifferentiated variety which i shall call " anaplastic carcinoma simplex . " aden ? ocarcinoma is much the commonest variety , constituting 85 per cent its histological characteristics are well known , and it is sufficient of all cases . to point out that though the growth usually shows a tubular or acinar pattern there is as a rule very little evidence of mucous secretion , either in the cells or 60cuthbert e . 
the last two varieties were too few in number for analysis , but comparisons between adenocarcimoma and colloid showed once more that mucus thus , secreting or colloid tumours spread more rapidly than adenocarcinoma . at the time of operation , only 5 per cent of the colloid carcinomas were still stage 1 , i.e. 
dukes such relationship between histology and spread can only be established if the histological varieties are clearly distinct : as definitely different , let us say , as adenocarcinoma , colloid carcinoma and carcinoma simplex of the intestine . this is seldom the case . another handicap arises from the fact that in some organs of the body the injury caused by a malignant growth is much more attributable to its anatomical position than to any niceties of histology . this is particularly true of tumours of the kidney , ureter and bladder . 
lane. from the department of pathology , royal cancer ho8pital , london . received for publication june 7 , 1952 . scepticism is a healthy response to diagnosis of any tumour as angiosarcoin ' - 11 . to dispel all doubts , full necropsy and thorough histological exaniination of all lesions with indisputable evidence of the vasoformative natuire of the tumour and proof of metastasis are essential . 
many lymph nodes in the cervical regions , supraclavicular fossae and posterior triangles were enlarged ( up to 2 - 0 cmain diameter ) , soft , dark red and cystic . 
on the surface and in the substance of both lungs were numerous discrete , firm , red , spherical nodules ( up to 3 - 0 cdiameter ) whose cut surfaces resembled blood clot . other parts the paratracheal and mediastinal lymph nodes of the lungs were oedematous . were greyish - black and slightly enlarged . 
the common bile - duct was dilated and contained several small pigment calculi . the spleen was small , and on its surface was a cyst ( 1 - 2 cdiameter ) containing clear fluid.. 
the nuclei are pale - staining , vesicular and variable in size : in shape 's.pherical , ovoid or indented . mitotic figures are few , but within such aggregations capillary channels are forming by separation of the cells . 
he interpreted his case as a benign angioma producing metastases , and separated it sharply from a case described by theile ( 1904 ) in which all the lesions showed sarcomatous areas . his interpretation is not acceptable in pathology , and the histology of the lesions in shennan 's ( 1914 ) case was no less benign , yet penetration of a pulmonary vein shennan suggested that our criteria of malignancy were at fault in was found . regarding such lesions as histologically benign . 
livingstone and klemperer ( i 926 ) concluded that the lesions in these cases were not as benign histolozicallv as the authors believed , and they thought that all showed atypical areas suggestive of malignancy . stout ( i 943 ) confirmed this , and considered the same applied to the original lesion in robinson and castleman 's ( 1936 ) case . however , in this connection it is well know - n that other malignant tumours and their metastases sometimes show deceptively benign histological appearances ( e.g. , chondrosarcoma and carcinoma of prostate , thyroid or kidney )  . the present case seems to be of the same nature as these and , in addition , has fe ' atiires similar to some others in which the histological structure was more malignant . kettle ( 1918 ) described an angioblastic tumour of the leg with metastases in the inguinal lymph nodes , ulrich ( 1921 ) a similar tumour of the lumbar muscles with metastases in the lungs , and downing and manory ( 1930 ) multiple angiomatoid lesions appearing in successive crops over an area which had been bumt some months previously . in the last two cases intravascular extensions were present , which strongly suggests that the lesions other than the primary mallory ( 1 914 ) , however , states that some caverwere blood - bome metastases . nous haema - ngiomas - not only arise in veins but permeate their wa ' ils and , at various placeg , rupture them , infiltrate the tissues and produce lesions which , while simulating metastases , are , in reality , in contiguity . this must be unusual , and would clearly be an incorrect interpretation of some of the cases cited where the lesions are far apart and particularly where peripheral lesions are associated with pulmonary ones . 
on the other hand , if benign angiomatous lesions extend into the lumina of veins , it cannot be concluded from observing intravascular extension alone that multiple lesions are metastatic rather than multifocal . in the present case , however , tumour tissue , not in cont ' lguity with large masses , is demonstrable within pulmonary vessels and , of special interest , witbin perivascular lymphatics and afferents to cervical lymph nodes . 
the only acceptable explanation of such findings is that the lesions in the cervical lymph nodes and lungs are embolic metastases . this case does not appear to shed any new light on those angiomatous conditions having a " system " distrib - ution described by theile ( 1904 ) , jores ( 1908 ) , wright ( 1928 ) and de nava , squez ( 1936 )  . in all these the authors described primary angioblastic tumours of the spleen with metastases in the liver . in theile 's case there were additional lesions in the lungs and stomach . willis ( 1948 ) , while c ' onceding these authors ' interpretations may have been correct , points out the possibility of the lesions in their cases being multifocal in origin . evidence suggestive of such cases being malignant metastasizing neoplasms ( local infiltration , poor differentiation , mitoses and intravascular extensions ) is not sufficient to classify them , witb certainty , as such . 
tumour tissue was found within perineural lymphatics of the scalp , in the afferent lymphatics of cervical lymph nodes ' and within pulmonary blood - vessels . i am indebted to j . 
a. - ( 1934 ) ' the spread of tumours in the human body , ' london ( chiirchill ) , p 148 . - ( 1948 ) ' the pathology of tumours , ' london ( biitterworth ) , p . 
of 9 : 10dimethyl - 1 : 2 - benzanthracene into the lungs of mice of strain street formed a part of a comprehensive study ( rask - nielsen , 1948 ) carried out in an endeavour to confirin or repudiate the hypothesis that tumours can be induced only in tissues that produce tumours spontaneously , whereas tissues that do not produce tumours spontaneously are unable to develop tumours even following very powerful carcinogenic action . the experiments showed that direct application of 0 - 5 mg . 
to this end , 3 : 4 - benzpyrene , 1 : 2 : 5 : 6 dibenzanthracene , or 20 - methylcholanthrene , all in doses of 0 5 mg . , were introduced directly into the lungs of street mice . since application of 9 : 10 - dimethyl - 1 : 2 - benzanthracene to the lung had previously induced thymic tumours ( rask - nielsen , 1948 ) , the present experiments were presumed to afford information also about the tumours which the three hydrocarbons would be capable of inducing in the thymus . these experiments will be reported in the present paper , which also includes the previous experiments with 9 : 10 - dimethyl - 1 : 2 - benzanthracene for comparison . benzpyrene , dibenzanthracene , or methylcholanthrene , 0 5 mg . , was injected , suspended in 0 01 c.c. 
the technique was as follows : in order to make the path of the needle in the lung tissue as long as possible , the needlewas inserted through the abdominal wall , immediately below the right costal border , and plunged through the diaphragm and longitudinally upwards through about two - thirds of the chest , before the suspension was injected . the mice used were litter mates of strain street , aged 5 to 7 weeks , divided into four lots . one lot was left untreated as controls , whereas the other three were injected with the respective hydrocarbons . 
as far as possible , the litters were divided equally in all four lots , an equal number of males and females in each in the corresponding experiments carried out with 9 : 10 - dimethyl - 1 : 2lot . benzanthracene ( rask - nielsen , 1948 ) litters of street mice were divided into lots of equal number , one of which was set aside as a control group . 
the effective total is the number of mice living to be as old as the youngest tumour - bearing mouse , namely , 12 months . in the sections prepared for the study of the spindle - cell sarcomas and thymic tumours , small adenomas were observed in a few mice . 
as shown in table ii , this phenomenon ' occurred following injection of dibenzanthracene in 4 out of 21 mice aged 5 - 7 months , following injection of methylcholanthrene in 2 out of 29 mice aged 6 and 7 months , and following injection of 9 : 10 - dimethyl - 1 : 2 - benzanthracene in 1 out of 9 mice aged 5 months . these figures apply only to the adenomas , one , or at most two or three , in each mouse , observed in one section through the lungs . nothing is known about microscopically visible adenomas in the remaining part of the lungs '  . neither is it known whether a corresponding production of adenomas had taken place in the mice showing no grossly visible it is worth mentioning that untreated tumours , but it is considered probable . street mice do not usually exhibit microscopic adenomas . serial sections from 48 mice , ranging in age from four to twelve months ( rask - nielsen , 1948 ) , showed one adenoma , only microscopically visible , in a mouse aged 12 months . 
the present experiments , therefore , appear to indicate that 9 : 10 - dimethyl - 1 : 2 - benzanthracene , methylcholanthrene , and dibenzanthracene , and presumably also benzpyrene , have induced pulmonary adenomas . 
the explanation why these growths were in most cases visible only upon microscopic examination is probably afforded by the short survival time of the mice ( table i )  . although the experiments allow of but an estimate of the development of pulmonary adenoma , they appear to indicate that injection of dibenzanthracene has induced a more marked increase in the development of adenoma than did injection of benzpyrene , methylcholanthracene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene . the macroscopic adenomas as well as those visible only upon microscopic examination were of the ordinary , typical sub - pleural variety . in addition to the adenomas of the right lung , adenomas were also present in the left lung of a 7 - month - old mouse injected with dibenzanthracene and in the two 12 - month - old mice injected with 9 : 10 - dimethyl - 1 : 2 - benzanthracene . 
1rask - nielsen sarcomas of varying differentiation . associated with lymphosarcomatous thymic tumours . in two mice the spindle - cell sarcomas were table ii shows that spindle - cell sarcomas were observed following injection of benzpyrene in 2 out of 81 ( 2 - 5 per cent ) , following injection of dibenzanthracene in 14 out of 73 ( 19 per cent ) , and following injection of methylcholanthrene in 19 out of 59 mice ( 32 per cent ) , the effective total of experimental mice being the number of mice living to be as old as the youngest tumour - bearing mouse of all 4 groups , namely four months . 
the effective total of experimental mice was calculated on the basis of the number of mice living to be as old as the youngest mouse exhibiting a thymic tumour within all four groups , namely three months . with the exception of one spindle - cell sarcoma of the thymus , observed in a mouse injected with methylcholanthrene , all the growths were typical lymphosarcomas , made up of stem cells and accompanied by a frequently highly pronounced perivascular infiltration , particularly in the central areas of the lungs . 
one mouse injected with 9 : 10 - dimethyl - 1 : 2benzanthracene exhibited such violent infiltration without actual thymic tumour . the latent period of thymic tumours is given in table iii , which shows that the average latent period following injection of benzpyrene , dibenzanthracene , methylcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene was 20 , 16 , 10 and 16 weeks respectively . the experiments revealed that the carcinogenicity of the hydrocarbons used , in doses of 0 - 5 mg . 
none of the six cases of generalized leukaemia was affected with thymic tumour . on the whole , the experiments showed that the order of carcinogenicity of the four hydrocarbons , as estimated from the incidence of tumours induced , varied , when 0 5 mg . 
of the same four hydrocarbons ( rask - nielsen , 1950a ) which showed that the lung tissue of street mice was susceptible to this dose of dibenzanthracene , less so to this dose of 9 : 10 - dimethyl - 1 : 2 - benzanthracene , but failed to respond to benzpyrene and iiethylcholanthrene . these recent experiments also showed that the thymus was particularly susceptible to direct application of 0 - 02 mg . 
of 9 : 10 - dimethyl - 1 : 2 - benzanthracene and methylcholanthrene , less to the same dose of dibenzanthracene and least to the same dose of benzpyrene . the incidence of thymic tumours induced by the four hydrocarbons was therefore decreasing in the same order following injection of a small dose into the thymus ( rask - nielsen , 1950a ) and a large dose into the lung . the results cannot be compared with earlier experiments , since thymic tumours following a direct carcinogenic action on the lung or thymus have not been reported before , with the exception of a few instances of thymic lymuphosarcoma observed after injection of methylcholanthrene into the lung ( esmarch , 1940b )  . but such remote effect was not observed . it is evident that the carcinogenicity of 9 : 10 - dimethyl - 1 : 2 - benzanthracene for the interstitial connective tissue of the lungs differed from that of the other three hydrocarbons . 9 : 1 0 - dimethyl1 : 2 - benzanthracene proved to be non - carcinogenic for this tissue , whereas the carcinogenicity of the other three hydrocarbons increased in the same order as their carcinogenicity for the subcutaneous connective tissue following application of the same dose into this tissue ( rask - nielsen , 19501 ) , i.e. 
kemp. from ae university institute , for human genetics , copenhagen . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . from ancient times it has been observed that cancer often occurs familially the inheritance of tumour 's in human beings has been studied and discussed for centuries , and it has especiallv been the object of extensive systematic investigations during the last decade , , about 6 years ago , a group of collaborators at the university institute for human genetics - in copenhagen decided to make an attempt to investigate the the ' investigation has partlybeen carried genetics of various aspects of cancer . out in co - operation with the danish cancer registry , under the direction of j . 
clemmesen , the university institute of pathological anatomy , and the radium centre in copenhagen and numerous danish hospitals and clinics . the work was supported by kong christian x 's fond , landsforenigen til kraeftens bekaempelse and anders hasselbalchs fond . these investigations include genetic experiments ' in mice and studies in man . twin examinations were also initiated in co - operation with the cancer registry . the statistical - genealogical investigations have been performecl as a series of surveys each concerning a considerable number , usually sevetal hundreds , of probands or propositi with cancer of a ce - rtain - type , e.g. 
canc - er mammae , cancer uteri , cancer oesophagi , multiple cancer or leukaemia , picked at random from the population . these investigations were made by a number of physicians , each being a ecialist in the field his study coneems . 
the families have been studied thoroughly , and every case of cancer in the relatives has , so far as possible , been verified ; in that respeot these investigations differ from earlier , more compre hensive statistical studies in the heredity of cancer . 
cancer of the breast , uterus , stomach and rectum , their occasionally familial occurrence has been know - n for in order to elucidate the etiologic significance of hered ' itary many years . factors in these tumours , proband investigation has been carried out . jacobsen 's ( 1946 ) study on the heredity in breast cancer includes ' 200 probands , ( 197 women and 3 men ) with cancer of the breast . 
the investigations of the probands ' families comprise the following categories of relationsi : parents , brothers and sisters , grandparents and brothers and sisters of the parents . videbaek ( 1947 ) has investigated ' edigrees of 20 ' 9 patients with leukaemia and 200 control probands , using the same methods as jacobsen . the propositi - method of investigation is , of course , rather complicated and leaves room for several sources of error . it must be realized that the diagnoses and the information on the whole as regards the older or more distant groups of relations are rather unreliable . 
some of the grandparents , for instance , died more than 50 years ago , and at that time , diaanostic skill was more limited and hospital records and death certificates were more insufficient than to - day . furthermore , it is difficult to procure a comparable control , material , because the probands are normally more interested in the occurrence of cancer in the family than normal control probands are ; probably that is the reason why the information conceming the distant groups of relations in jacobsen 's control material is insufficient . also it must be considered that during recent years many cancer patients , e.g. 
suffering from skin cancer , get cured without knowing they have had cancer , and thus escapenotice by the investigator . it should also be pointed out that the calculation of the morbidity risk is a complicated method , and cannot always be relied on . 
lip and skin cancer , are not represented in the families of the probands , but cancer of most other forms , sites and types occurs in the relatives in about the same proportion as among the r ' elations of the control probands , and is comprised under the collect ' lve term " endogenous cancer as a whole . " according to jacobsen ( 1946 ) , a study of the case histories of the probands gives no basis for supposing that extemal factors play any important role in the development of breast cancer . 
an excess incidence of breast cancer among the female relatives of the probands and likewise a significant excess incidence of " endogenous cancer as a whole " in all the categories of relatives , both male and female , were found . this indicates hereditary predisposition as the chief factor in the development of breast cancer . breast cancer is dependent o ' n hereditary factors , and the tendency to this particular form of the diseas.e is bound up with an inherited predisposition to endogenous cancers endogenous cancer in general . 
the localization of the tumour is determined either by hereditary or extemal factors . in many pedigrees the general hereditary predisposition appears to be inherited as a dominant character . in the leukaemia proband material , the familial incidence of the disease was found to be at least 8 per cent . several types of leukaemia ( acute or chronic lymphoge ' neous or myelogenous , monocytic or stem - cell leukaemia ) may occur in the same family -  . 
the multiple occurrence of leukaemia in an individual family is usually not confined to some particular type , which indicates that leukal - imia is probably genetically a morbid - entity . among members of a family there seems to be an age correlation as regards the onset of leukaemia.. 
according to videbaek ( 1947 ) leukaemia , as such , is not simple domininherited ; it is a question of inherited disposition to the disease . ance or recessivity may possibly be excluded ; it may have a genetical - basis with incomplete dominance or polymeria ( homologous polymeric factors )  . hereditary predisposition to disease is generally regarded as polymeric . 
the expression of the character is furthermore dependent on the interaction between the genotype and environment . the incidence of pemicious anaemia is significantly higher among the relatives of patients with leukaemia than among the relatives of the control probands . the relation is probably due . 
among the relatives of the leukaemia patients there is a significantly excessive incidence cancer , of cancer as a whole , due to a high incidence of all forms of cancer . including leukaemia , is piobably a disease entity genetically dependent on a dominant gene common for all the different forms of " endogenous cancer . " according to videbaek 's oplinlon the - development of leukaemia seems to depend on various conditions , among others , on a non - specific hereditary predisposition to cancer , which is believed to be present in at least 20 per cent of thepopulation in general , and partly on one or several genes , the activity of which plays a role for the localization of the cancer to the leukon ; leukaemia seems to constitute an entity genetically and environmental changes influence the type of the disease . there is evidence that extemal factors also ' play a role in the development of leukaemia . 
of several cases of leukaemia in the same family is rather slight ; but the risk of getting cancer in near relatives of a patient with leukaemia is as high as almost 50 per cent . table iii shows some of the data from the breast cancer and leuka6mia material in relation to cancer risk . 
among the relatives of probands with cancer of the body of the uterus the incidence of " endogenous cancer " was high , and the relatives of probands with cancer of the cervix show the same frequency as the relations in the families of the patients with cancor of the cervix , of control probands . on the other hand , a relatively increased frequency of cancer of the oesophagus in this connection it is worth while to draw attention to the simiwas present . larity of the histological structure of cancer of the cervix and cancer of the in the families of probands suffering from cancer of the oesophagus oesophagus . investigated by mogensen ( unpublished data ) , cancer of the oesophagus was often found in a close male relative , the father or a brother of the proband . in these families , both the proband and the relative with cancer of the oesophagus 148 t . 
the differences could , however , not be significantly proved , owing to the insufficiency of the material , and the differences may be due to the fact that - the old propositi generally have less detailed and exact information about their relatives in earlier generations than the young propositi have . still the accordance of the experimental results and the clinical observations makes the significance of the latter probable . our investigations into the heredity of various aspects of cancer , have show - n that hereditary disposition is an important tumour - causing factor . it was found that it is the chief factor in the development of breast cancer , and many other tumours are more or less dependent on hereditary factors . 
the general cancer - tendency " ( likely not a general blastoma tendency ) occurs with considerable frequency in the population ( it is probablv higher than 20 per cent ) , and is possibly inherited as a character showing incomplete dominance . 
our investigations have shown that the tendency of tumour - localization has also a hereditary basis . the development of leu ' kaemia and cancer is probably due to a common hereditary . 
koller. from the chester beatty research institute , the royal cancer hospital , london . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . xeroderma pigmentosum ( hence referred to as x.p. ) , is marked by rougheniing , dryness , pigmentation and ulceration of the skthe condition is attributed to hypersensitivity of the skin , particularly that of the basal cell layer , to sunlight . the disease was first described adequately by kaposi in 1874 ( hebra and kaposi , 1874 )  . 
occurs in the first year of life , often within a few , months after birth . first , erythema develops on the skin , on those regions which are exposed to light , followed by freckling and frequently by telangiectasis . from these regions epithelioma or basal - cell carcinoma develops . 
the malignant change may take place not only in the skin , but also in the cornea and conjunctiva the genetical and chromosomal basis of x.p. the hereditary basis of x.p. 
was first investigated by siemens and kohn ( 1925 )  . they analysed 76 families , and cockayne ( 1933 ) brought this more up - to - date with a further 43 family histories . in both groups of data the incidence of consanguineous marriages was very high : 24 out of 76 and 16 out of 43 respectively , were first - cousin marriages . 
jv.7. reeeived for publication march 5 , 1949 . the pressure mincer described in this article was designed to facilitate the preparation of tumour suspensions for a quantitative studv of the survival of tumours in the frozen state . 
the choice of principle and design was determined by the foflowing requirements : ( a ) rapid reduction of tumour tissue to a suspension of fine fragments and separated ceus , ( b ) ease of aseptic manipulation , ( c ) mechanical simpficitv and ( d ) ease of cleaning . the essential feature of this instrument is a grooved plunger which operates in a closed eyfinder . 
the tissue is placed below ' the plunger , and on the application of pressure is forced through the grooves to the upper face . the niincer and its component parts are shown in fig . 
1. all parts are machined from brass and are chromium plated . * it is important to have the plungers ( c and d ) fitted to the body tube ( a ) with the minimum clearance consistent with smooth working . 
the nose of each plunger fits accumtely into the recess in the base plate ( b )  . similarlv the nose of the fine pliiin er fits accurately into the base of the coarse plunger . 
the diameter of the bodv tube is 1 - 6 cm . thus i mof displacement of the plung - er corresponds to a volume of 0 - 2 ml . cleaning is facilitated and design of the plungers is simplified bv the prov - ision of a detachable base plate . the operating screw ( f ) is of sufficient length to extrude the plungers from the lower end of the body tube . the various parts of the mincer are sterilized separately in glass tubes . 
the mincer is shaken immediately to disperse the mince if the coarse plunger has been used the cap and operating in the suspending fluid . screw are detached and the fine plunger is inserted . tlle cap and screw are replaced and mincing is completmed . the suspension may contain coarse fragments of fibrous tissue or portions of iiiince which have clotted before dispersal in the suspending fluid . these may be removed either by l ' ow speed centrifugation , or by filtering the suspension througli a column of glass ballotini of suitable diameter . the mincer , which is illustrated in fig . 
1 , is the sixth of a series desigiied to all models have proved most satisfactory for operate with grooved plungers . the purpose for which they are intended , and it might be suggested that this tvpe of mincer will , for special purposes , be suitable for preparing suspensions of manimalian tissue or fowl embryos infected with certain viruses or bacteria . i wish toacknowledge my indebtedness to w . 
powell. from the department of experimental pathology , mount vernon hospital , northwood , middlesex . received for publication april 30 , 1951 . in previous communications ( powell , 1944 , 1946a , 1946b , 1947 ) it has been suggested that many of the typical properties of tumour cells can be explained by the occurrence of a derangement of the submicroscopic protein framework it was also suggested that the growth of malignant cells of their protoplasm . might be inhibited by chemical compounds able to link together the ultrastructural protein fibrils of tumour cells , and thus simulate the arrangement of comparable fibrils in normal cells . disulphide bridges constitute one of the more important classes of interconnections between the fibrils of native proteins . 
the quinone was recovered from the fitered bisulphite solution by precipitation with sodium carbonate or sulphuric acid . further purification was carried out by repeated formation of the additive bisulphite compound and subsequent precipitation as above . 
the following transplantable tumours were used : carcinoma 63 , a fibrosarcoma ( ac ) of strong a mice , a spindle cell tumour and a squamous cell carcinoma of cba mice , a rapidly growing undifferentiated sarcoma ( rb ) and a mammary adenocarcinoma of riii mice . the tumours were grafted subcutaneously in the right flanks of the mice , in each experiment the implants being portions taken from one tumour . in each experiment mice with actively growing tumours were divided into groups , control and experimental . 
1. - effect of 1 per cent phenanthraquinone upon the growth of carcinoma 63 in a strain in all the text - figures the horizontally placed numbers indicate days after inoculation , mice . and the concentration of phenanthraquinone in the food is given as a percentage of the combined weights of flour and rat cake powder . the quinone used in this experiment possibly contained a trace of the hot tasting impurity , but treated mice showed no harmful effects from it . 
2 and 3 demonstrate the similarity of the results obtained in different experiments with a particular strain of tumour when the rate of tumour growth is approximately the same , and the concentration of the drug is constant . 
1 , in which the growth of the control tumours is appreciably faster . here , with a higher concentration of the drug , smaller initial sizes and slower intrinsic growth rates of the tumours , the inhibitory effects of the treatment are greater than in c ontrol a . 
the inhibition of several spontaneous mammary tumours of a and riii strains of mice by the quinone was comparable with that of the transplanted tumours . also , the growth of a transplantable mammary adeno . carcinoma of riii mice and a transplantable squamous cell carcinoma of cba mice was strongly inhibited . thus the growth of a variety of different tumours can be inhibited by phenanthraquinone under the conditions described . unpalatable cause loss of weight of the treated animals . samples of phenanthraquinone containing sufficient impurity to make it gastro - enteritis some270 a . 
the latter causes prepared food to be unpalatable , and can give rise , if present in sufficient amount , to gastrobut , by comparing the effects of samples of quinone of varying degrees enteritis . of palatability , it has been established that the purest samples are the least toxic this greater inhibition to mice and inhibit tumour growth to the greatest extent . of tumour growth may be due in part to a greater intake of food , and therefore detailed investigation of the effects of phenanthraquinone upon of quinone . tumours and of its possible value in tumour chemotherapy is dependent upon the preparation of the drug in a pure state . its further purification and alternative methods of synthesis are under investigation . the additive compound of phenanthraquinone with sodium metabisulphite is serial intraperitoneal very readily hydrolyzed in vivo to yield the free quinone . injections in mice of aqueous solutions of the quinone - bisulphite compound in sub - lethal doses at frequent intervals indicate that the liberated quinone is very rapidly metabolized in the body . in view of the rapid destruction of phenanthraquinone in vivo and of the rapid growth rates of many tumours , it is essential that continuous administration of the drug be maintained in order to expose the tumour cells to an effective concentration of the drug for sufficiently long periods . failure to achieve this could permit a proportion of the tumour cells to grow and in the early stages of an experiment cessation of treatment with the divide . quinone may result , in some instances , in stationary tumours recommencing growth . 
on the other hand , similar tumours continually subjected to the action of the quinone fail to grow and often regress completely . in these preliminary experiments the simplest method of ensuring an adequate and continual supply of the quinone , namely , by adding it to the food , was adopted . however , this method is not entirely satisfactory . adequately controlled experiments in which individual mice receive known amounts of quinone at definite times are necessary for detailed studies of the action of the drug . very little of the quinone in a concentration of 1 to 2 per cent in the food ingested by a mouse can be available for action on substrates in tumour cells , since there is a very great disparity between this amount and the lethal dose given as the bisulphite derivative by injection . 
much of the fed quinone may not be absorbed from the food , and the greater part of that reaching the body fluids may be metabolized . sodium salts of the phosphoric and sulphuric acid esters of 9 : 10 - phenanthrahydroquinone have been synthesized and tested for possible inhibitory effects on tumour growth , but they have been found to be unsuitable for the treatment of tumour - bearing mice . 
the former very readily hydrolyzes to give the hydroquinone , which readily oxidizes to the quinone , and the latter is extremely resistant to hydrolysis . preliminary experiments upon the administration of thiol compounds concurrently with phenanthraquinone to tumour - bearing mice appear to indicate that its inhibitory action on tumour the latter reacts with thiol groups in vivo . growth may be due , at least in part , to this effect . 
powell may enable phenanthraquinone to function as an oxidation - reduction catalyst and so disturb the natural oxidation - reduction balance of tumour cells , possibly to a greater extent than that of most normal cells . in view of its considerable chemical reactivity , as well as of its affinity for proteins , phenanthraquinone despite the possibility that would be expected to have multiple effects on cells . phenanthraquinone has in vivo the mode of action postulated earlier , that is , of forming cross - linkages between ultra - structural protein fibrils , it is emphasized that its actual mode of action remains a completely open question . 
the available evidence favours the view that over a certain range of concentration tumour cells are more sensitive than normal cells to the effects of phenanthraquinone . it has been reported by mitchell ( 1948 ) that the combined antimitotic effect of " synkavit " and x - rays is greater than the additive effects of both agents used singly . 
in giemsa preparations feulgen staining was the membrane appeared as a faintly stained pink line . completely ineffective , whilst after iron haematoxylin the membrane lost its stain early in the decolorising process . 
the mercuric bromphenol blue staining technique of mazia , brewer and alfert ( 1953 ) was tried and found to stain the membrane feebly . this method , however , proved useful for determining the relationship of the membrane to the spindle structure . examinat - ion of a large number of preparations has allowed the following description to be pieced together : 1 . 
telopha8e. - as the cytoplasm constricts to form two daughter cells , the membrane also constricts and finally , after fusion at the centre , separates into two complete membranes - - one to each daughter cell . 
7. examination of fresh smears of the tumour by phase contrast microscopy demonstrates the occurrence of this membrane within the living cell and dispels ' any possibility of its origin being that of a fixation artefact . 
the membrane , under these conditions , appears as a thin clear zone form ' mg a sharp line of demarcation between the karyoplasm and the cytoplasm . because of the overlying cytoplasm it is difficult to focus and photograph . in this particular tumour mitosis within a persistent membrane appears to be the standard type of division . 
3. other than that it was taken from a section of a hepatic metastasis of a carcinoma of the tonsil no further comment or information is it appears then that the phenomenon as described is not a completely given . isolated case but does occur occasionally in other material , but not with the regularity shown in this instance . it would not appear to be a fixation ar - tefact since it can be determined by phase contrast microscopy in living cells . further , the fact that such a wide variety of fixatives will preserve it is against such a view . 
on the basis of the evidence available it seems unhkely that such an event has taken place , and if so , takes no cogmsance of the fact that similar appearances do occur irregularly in other tumours . although no evidence can be adduced to show that this membrane arises de novo within each dividing cell it is possible to offer a fairly plausible explanation it has been demonstrated by chambers and of its appearance in this fashion . ludford ( 1932 ) that the cytoplasm of malignant cells has a ph value lying between 6 - 4 and 7 - 0 whilst the intranuclear ph is in excess of 7 - 2 . 
under such conditions a gradient of ph would occur . it is suggested that at some point on this gradi ' ent the isoelectric point of neighbouring cytoplasmic structural protein is reached . this would involve the localised precipitation of protein and the ensuing membrane appearance . if such an event does occur it suggests that intracytoplasmic disturbance during mitosis is minimal , otherwise one would expect distortion and breakage of the membrane . a mechanism of origin as suggested above would account for the isolated examples of similar appearances in other tumours . 
doniach. from the pathology department , postgraduate medical school of london , w.12. received for publication february 20 , 1953 . the increasing use of radioactive iodine in clinical medicine has made imperitive the experimental study of its possible carcinogenic action on the thyroid gland . radioactive iodine , like stable iodine , is rapidly concentrated by the thyroid , bound to protein in its colloid in the synthesis of thyroxine , and then gradually released from the gland as part of the normally secreted hormone . during these processes the follicular cells of the thyroid are submitted to a course of ionizing irradiation from the i131 , which gives out f and y rays . 
the duration of this irradiation is of the order of days , since the half - life of 1131 is 8 days and the effective half - life of intrafollicular hormone is also of the order of days in the normal human gland . the carcinogenic activity of ionizing radiations in general has been repeatedly demonstrated during the past 50 years . recently , the effects of ft irradiation from newly developed sources have been studied . raper , henshaw and snider ( 1951 ) reported that single doses of 4000 to 5000 rep ( roentgens equivalent physical ) of f rays from a p32 source induced skin tumours in rats . 
they also found that 13 , 400 rep given in daily exposures of 50 rep over a period of 348 days proved carcinogenic . glucksmann ( 1951 ) found epitheliomas in 4 out of 24 mice in an area of skin exposed 14 months previously to 7900 rep given in 30 seconds by an electron beam . it has proved necessary in the treatment of graves ' disease with radioactive iodine to administer an amount of 1131 calculated to give an overall irradiation to the thyroid gland of 8000 to 10 , 000 rep ( wayne , 1952 ) in order to produce a complete remission of the disease . this dosage lies within the range found to be carcinogenic to other animal tissues . but owing to the uneven distribution of radioactive iodine in the thyroid one cannot make a confident direct comparison , from the dosage point of view , between the animal experiments mentioned above and 1131 therapy of humans . the mechanism of the experimental production of tumours of the thyroid by goitrogens has been greatly clarified by the new zealand team of workers ( purves , griesbach and kennedy , 1951 )  . 
doniach in evaluating the possible danger of carcinogenesis by j131 one must consider not only the direct action of , rays on the cells , but also the indirect action of radiation damage , which leads to diminished thyroxine synthesis and a resultant increased thyrotrophic hormone production . 
a suitable dose of 1131 might therefore lead to a summation of two carcinogenic stimuli ; a short exposure to / 6 irradiation and a long exposure to stimulation by the pituitary . 
the latter could be ensured experimentally by giving a prolonged course of antithyroid drug subsequent to a dose of j131 . doniach ( 1950 ) found that 10 out of 16 rats , given 32 microcuries of 1131 ( 15 , 000 rep to the thyroid ) , developed adenomas . in a series of 5 rats given additional methylthiouracil for 14 months , the thyroids showed a striking increase in adenomas and i - n one instance a metastasizing carcinoma , in contrast to 16 rats tested for the same period with methylthiouracil alone , whose thyroids showed only occasional adenomas . this summating effect of a carcinogen with an antithyroid drug was first demonstrated by bielschowsky ( 1944 , 1045 ) , who used the carcinogen acetamidofluorene combined with allylgoldberg and chaikoff ( 1952 ) have recently reported the development thiourea . of poorly differentiated non - colloid - forming thyroid cancers in 7 out of 25 rats injected 12 to 2 years previously with 400 microcuries of i131 . 
the authors attributed the cancer development entirely to beta irradiation , and not to thyrotrophic hormone stimulation . the object of the experiments described below was to repeat previous investigations of the action of 30 microcuries of j131 alone and combined with methylthiouracil in a larger series of rats , and to compare these results with the effects of 5 and of 100 microcuries . 
the trachea and thyroid attached were fixed in helly 's fluid ; the thyroid was then dissected off and weighed to the nearest milligrathe thyroids were embedded in wax , all glands which weighed 30 mg . 
were secstained by haemalum and eosin . tioned at 6 levels , so arranged as to traverse the whole thickness of the thyroid three sections cut at each level at 5#t were mounted and at regular intervals . one of them stained by haemalum and eosthe spare sections in general were used for extra stains . 
followed 24 hours later by methylthiouracil in the drinking water until the end of the experiment . ( 8 ) 100 lsc 1131 , 30 , uc 1131 , 24 hours later methylthiouracil till end of experiment . 24 hours later methylthiouracil till end of experiment . 
they were taken off the drug for 4 weeks from the 6th to 7th month and were given the i131 in two doses , half at the beginning of the experiment and half 24 hours before commencing their second course of methylthiouracil . in july , 1951 , eight months after this experiment was begun , the thermostat broke down one night and the heating was unfortunately left full on . 
a further 40 rats died or were killed during the course of the experiment , wasted from interfortunately the differences in current infection . the findings between the major groups proved striking even with the reduced number of rats . 
the nuclei were paler than those of neighbouring follicle cells and showed occasional mitoses . the affected follicles had lost their original lining , and had tended to flatten out apart from the altered appearthe normally scalloped perifollicular reticulum . ance of the cells , these " solid " follicles were easily differentiated by serial section from the apparent solid follicles produced by tangential sections of normal ones . they occured both centrally and peripherally in the glands and varied in diameter from 50 to 200 , t . 
to this end , serial sections were examined of the growing thryoids of 5 rats aged .23 days and 5 rats aged 100 days . in none of them were any microadenomas seen . 
nor were there any structures seen resembling these microadenomas in sections of the developing thyroids of 15 - day and 19 - day rat embryos . the incidence of microadenomas in the 9 controls of the main experiment is there were no macroadenomas found similar to those seen in there was a great variation in rats ' and thyroids ' weights . 
the lining cells were about 15 , t tall with a voluminous eosinophilic cytoplasm and capillaries were prominent , and oval vesicular nuclei . did not indent the follicular cells as in the controls . in reticulin preparations the capillaries appeared pushed back by the hypertrophic follicular cells . 
the arrangement of the cells included solid sheets , packed solid trabeculae , closely packed tubules containing pale fluid , microand macrofollicles filled with watery or deeply eosinophilic colloid , and gross cystic follicles distended with colloid and lined by a papillary epitheium . engorged sinusoids were prominent in many of the adenomas . 
the majority , however , presented a closer affinity to those seen in the rats treated with 5 , uc 1131 alone except that the cells were a little taller . their nuclei varied in size and chromatisthe adenomas presented an exaggerated and bewildering variety of cell types and differentiation fundamentally similar to those produced by methylthiouracil alone . 
some of the very large adenomas appeared to be derived from the confluence of more than one tumour . colloid secretion was well marked in many tumours and a papillary arrangement was not rare . 
however , the major part of the bulk of even the large tumours was cellular rather than secretory in origin . solid areas of undifferentiated spheroidal cells were seen within some tumours as with methylthiouracil alone . rat 35b tongues of adenoma tissue were seen penetrating the capsule at one however , in the absence of evidence of permeation of extra - capsular point . veins or obvious morphology of cancer , malignancy was not diagnosed . 
the majority of the follicles appeared active but could be differentiated from those seen in rats treated with methylthiouracil alone , as they were smaller , less regular and showed a tendency to a syncytial arrangement of their lining cells . 
the rats ' weights were similar to those treated by methylthiouracil alone , but the thyroid weights were very considerably reduced to an average size comparable with that of the rats treated with 100 , uc 1131 alone . the pituitaries were similar to those of the rats treated with methylthiouracil alone . 
was injected with the same syringe into a glass vial containing a small pledgelet of cotton - wool . fifteen hours later in vivo measurements were made of the radioactivity of the rats ' thyroids and of the 1 ml . 
19.chart showing the average in vivo count - rates of radioactivity of the thyroid glands of 8 rats following an intraperitoneal injection of 9 - 2 yc 1131 . after 24 hours 4 of the rats ( lowermost curve ) were put on to methylthiouracil in their drinking water . 
the findings in the remaining 4 are charted in the middle curve ; the calculated loss of radio - activity due solely to the radioactive decay of il31 is charted in the uppermost curve . count - rate of standard at 15 hours was 10 , 700 . due to the normal radioactive decay of 1131 . 
the differential effects on these functions of varying doses of 1131 have been recently reported in 3 publications . skanse ( 1948 ) studied the effects of 1 , 10 and 50 , tc i131 on young cockerels primed with a short course of thyrotrophic hormone . 
a definite inhibition of normal thyroid growth was produced by 10 j#c and 50 , uc 1131 after 16 days but not of body growth . all the thyroids showed a growth response to thiouracil , less marked in the chicks given the higher dosages of 1131 . but this response to thiouracil was much more inskanse ( 1948 ) remarks that though hibited after 38 days than after 26 days . the major part of the radiation was received irn the first few days , it took a much longer time to produce the full biological effect on gland function . the calculated dosages of total radiation to the thyroid glands were 1700 rep in the 1 , uc group , 13 , 000 rep in the 10 , tc group and 60 , 000 rep in the 50 1c group . feller , chaikoff , taurog and jones ( 1949 ) studied the effects on adult male rats of single intraperitoneal doses of 24 , 300 and 875 4ac of 1131 . 
the average uptake of 1131 into the thyroids was 40 per cent between 23 and 48 hours after those treated with the two injection and was about equal in all the animals . higher doses showed an abnormally rapid depletion of the iodine that had been trapped during the first 24 to 48 hours . chemical analyses showed an increasing depletion of thyroid 1127 from 2 to 3 days onwards after the injection of the 300 and 875 jtc 1131 , whereas there was no loss after 6 days in animals given 24 1ac . the values of plasma protein bound iodine were not changed in the 24 , uc group but they fell steadily in the rats injected with 300 , uc from 3 - 6 , ug . 
the thyriod uptake in the 1 , uc reached 53 per cent 48 hours after receiving a tracer dose of i131 , but was significantly less in all the other groups . response to subsequent thiouracil was similarly impaired when tested . 
the thyroids of animals which had received 50 and 100 , tc 1131 demonstrated no capacity to increase in weight on a 30 - day course of thiouracil instituted 64 davs after the initial dose of radioactive iodine . even 5 jtc initial t131 impaired the capacity of the thyroid to increase in size ; the 194 i . 
in the animals given an initial dose of 1 iac 1131 . measurements of body weight showed no disturbance in animals which had received up to 20 , uc , a slight impairment in the 50 and 100 , uc groups and a marked disturbance in the 300 , uc group . 
the calculated maximum total irradiation doses delivered to the thyroid in rep were respectively 1800 in the 1 , uc , 5800 in the 5 , uc , 30 , 000 in the 20 , uc , 80 , 000 in the 50 1ac , 197 , 000 in the 100 , tc and 288 , 000 in the 300 / tc groups . effects of internal irradiation by j131 on thyroid histology . findlay and leblond ( 1948 ) studied the thyroid histology of two rats killed 6 days after a single injection of 1131 calculated to have given a total thyroid irradiation of about 20 , 000 rep . the rats had previously been maintained on a low iodine diet . most of the follicles , especially the central ones had lost their colloid , and were replaced by irregularly arranged solid groups of epithelial cells , some of which showed nuclear and cytoplasmic degeneration . interstitial oedema was pronounced , fibrosis and lymphocytic infiltration slight . 
many follicles in the periphery and isthmus were normal autoradiographs showed evidence of accumulation of iodine only in the surviving colloid containing follicles of the periphery . goldberg , chaikoff , lindsay and feller ( 1950 ) studied the progressive changes in the thyroids of adult rats given varied doses of 1131 and killed after intervals of 1 day , 2 days , 3 days , 1 week , 2 weeks , 3 weeks , 1 month , 6 months 875 1 , c ( 330 , 000 rep to gland centre at 72 hours ) produced a total and 8 months . destruction of the thyroids evident within 48 hours , associated with an intense fibrinous oedema and acute inflammatory changes , followed by fibroblastic proliferation and arterial thrombosis . 
by 3 weeks there was a total collagenous permeation of the original gland structure , which by 6 months was replaced by 525 itc produced essentially similar changes . a band of hyalinised collagen . there were , however , at 5 months a few surviving thyroid follicles at the poles , lined by bizarre granular cells thought to resemble the so - called hurthle cells of the human gland . at 8 months surviving thyroid cells appeared more numerous 300 / , tc ( 110 , 000 rep at and formed occasional colloid containing peripheral follicles . 72 hours ) produced extensive swelling and desquamation of thyroid cells within 24 hours , followed during the next 2 days by further degeneration and by interstitial inflammation which appeared resolved by 8 days . at 4 months the glands were lobular and made up of mixed disturbed and normal follicles . at 8 months the glands appeared essentially normal , though the follicle cell nuclei were hyperchromatic and interstitial tissue was increased . 
produced total thyroid cell necrosis in 2 days . following the administration of minimal thyroid - lethal doses , parenchymatous degenerative changes first appeared within a few days in the gland and were followed by an inflammatory picture . intrathyroidal doses of 2 , uc / mg . 
 ( 1952 ) described the histology of the thyroids at varying time intervals after administration to rats of i131 as a part of the study of functional changes quoted above . after 2 days parenchymal degeneration and interstitial inflammation were seen centrally in the 300 , #c group ; no significant changes after 48 days the 300 , #c group showed a virtual were seen in the other groups replacement by fibrous scar tissue . the other groups , including the rats given 1 / uc , all showed hypertrophy of follicle cells and diminution of colloid . 
from 30 , 000 rep upwards there is an increase in rate of loss of organically bound iodine from the thyroid , associated with radiation damage to the follicles . in general , functional disturbances precede histological changes . 
from 5000 rep upwards the thyroid cells are able to respond to activating stimuli by hypertrophy , but hyperplasia proves abnormally limited . bizarre thyroid cells are seen histologically up to 12 years and are accentuated by thiouracil treatment , increasing in number in thyroids submitted to 5800 rep upwards . 
even though irradiated thyroid cells are histologically abnormal , they appear by means of hypertrophy to synthesize enough thyroxine to maintain the animals ' health and growth after dosages up to 30 , 000 rep . calculation of dosage of radiation to the thyroid . calculations of radiation dosage to the thyroid following the administration of radioactive iodine can at the best only be rough estimates because of the con196 i . 
 ( 1949 ) pointed out that since the maximum range of the beta particles enmitted from i131 is comparable to the dimensions of the rat 's thyroid , a geometrical factor must be calculated to estimate the reduction in radiation dose at points near the surface of the gland as compared with the centre . 
by following the uptake of radioactive iodine into the thyroid and its sequential loss from the gland it is possible to estimate the total the conversion factor for rep was calculated by evans ( 1947 ) : radiation dose . 1 , kc per mg . 
the animals were all killed after 15 months and 5 , tc 1131 and methylthe rats on methylthiouracil alone showed no carcinomas . thiouracil led to the production of a greatly increased incidence of adenomas , these findings confirm the additive action of radiobut no definite carcinomas . active iodine in carcinogenesis by antithyroid drugs , and show that the range of 2270 to 16 , 200 rep was more effective than 380 to 2700 rep . in contrast , the methylthiouracil given to rats treated with 100 , tc i131 produced less adenomas this inhibition at a dosage level of 8400 to 60 , 000 than methylthiouracil alone . rep confirms the findings of maloof et al . 
 ( 1952 ) of the greatly diminished capacity adenomas of a similar of heavily irradiated thyroid cells to undergo hyperplasia . morphology to those present in the thyroids of rats treated with antithyroid drugs were found in the animals given 5 , uc and 30 , uc 1131 alone , the latter appearing more effective than the former . 
doniach and pituitaries of this group are significant . there are two points of evidence that a certain amount of thyroxine was being synthetized . firstly , the animals grew from an initial weight of 100 g . , when the radioactive iodine was first administered , to the full weight of 250 to 350 g . , at the end of the experiment . secondly , the pituitaries showed a good coinplement of well granulated alpha cells . purves and griesbach ( 1946 ) demonstrated that the iiaintenance of the alpha granulations is dependent upon a supply of thyroxine ; the pituitary alpha cells disappear after thyroidectomy and are restored by the daily administration of one - fifth or more of the normal thyroxine requirements . nevertheless , the beta cells showed the typical changes of a raised level of thyrotrophic hormone secretion described by griesbach and purves ( 1945 )  . this suggests that the irradiated thyroid glands were secreting at least one - fifth but less than the normal thyroxine requirements . the diminished capacity of the irradiated glands to regenerate prevented a return to quantitatively normal thyroxine synthesis , thus perpetuating an increased thyrotrophic hormone output and accounting for the hypertrophy of the thyroid cells . another possibility to be considered is that irradiated thyroid cells differ from normal in requiring a higher level of thyrotrophic hormone stimulation in order to secrete a normal quantity of thyroxine . similar changes in the thyroids and pituitaries were observed to a lesser extent in the 301 , c 1131 treated rats and to a slight extent in the thyroids only of the 5 , tc i131 group . the bizarre thyroid cell nuclei observed by maloof et al . 
 ( 1952 ) in 1131 treated rats were seen in the present experiment , and were also accentuated in rats treated by additional thiouracil . one cannot say whether the neoplastic cells arise from these or from their apparently normal neighbours . they do , however , constitute evidence of irreversible irradiation changes . 
we do not know the life span of thyroid cells , but it is almost inconceivable that they could survive and function without replacement for15 months , a period of nearly one half the animal 's life span . neoplasms in general arise in tissues made up of actively dividing cells . they do not arise from irreversibly differentiated cells such as neurones or keratinized epidermal cells . the chances of the development of neoplastic thyroid cells following irradiation are likely to vary directly with the number of post irradiation mitoses which take place . this number will be increased in the thyroid bythyrotrophic hormone stimulation . the proportion of cells which become neoplastic is presumably related to the dose of irradiation . the absence of adenomas in the100 , uc 1131 treated group is considered to be due to a lower incidence of dividing cells following irradiation than that which followed in the 30 and 5 1tc groups . adenomas might have been found after afurther 6 months since they were present , albeit in small number , in the 100 , tc treated rats submitted to additional thyrotrophic hormone stimulation by a prolonged course of methylthiouracil . 
one of these was a malignant anaplastic carcinoma transplantable into hosts without thyroxine deficiency . it was not dependent on a high level of thyrotrophic hormone , did not concentrate iodine , grew rapidly , and killed its hosts within a few weeks . the main difference between the action of antithyroid drugs alone and combined with the carcinogen acetamidofluorene is that with the latter treatment thyroid tumours appear considerably earlier and in greater number . bielschowsky ( 1949 ) found also that acetamidofluorene produced thyroid adenomas in the absence of a chemical goitrogen in the regenerating thyroids of subtotally thyroipurves et at . 
 ( 1951 ) have concluded that neoplastic cells arise dectomised rats . spontaneously in the normal rat thyroid and that the carcinogen acetamidofluorene seems to act by speeding up their formation , their further development and growth , however , being dependent upon a high thyrotrophic hormone level . this has been produced experimentally by the prolonged administeration of antithyroid drugs , or by prolonged iodine deficiency ( wegelin , 1927 )  . the results of the previous ( doniach , 1950 ) and the present experiments show that the action of radioactive iodine is comparable with that of the carcinogen acetamidofluorene . in addition , radioactive iodine on its own leads by partial inhibition of thyroxine synthesis to a prolonged rise in thyrotrophic hormone level . 
from the description of goldberg and chaikoff ( 1952 ) , the experimental thyroid carcinomas which resulted from an extremely intense irradiation with radioactive iodine appeared to be of a high grade malignancy . the possibility that a carcinoma of low grade malignancy might become anaplastic must be considered after the findings in the transplantation experiment of purves et al . 
 ( 195 1 ) ; the probability however is unknown . dangers of carcinogenesis to humans treated with j131 . after an exposure to 1800 rep from j131 , maloof et al . 
 ( 1952 ) found a normal thyroid histology in rats 11 years later . but following 5800 rep and upwards , hypertrophied thyroid cells and increasing numbers with abnormal nuclei were seen , accentuated by a short course of methylthiouracil . these cells persisted tracer doses of j131 in clinical medicine fall into the first category , up to 1 1 years . those therapy doses which lower thyroid function below normal into the second . from the experimental findings in rats it would appear that 9000 rep to the thyroid in graves ' disease must act chiefly by functional damage leading to diminished thyroxine production rather than by actual total destruction of the gland . this is borne out by the brief descriptions of chapman and evans ( 1949 ) , williams et al . 
 ( 1949 ) and shapiro ( 1950 ) , who noted no histological evidence of gross destruction in the thyroids of thyrotoxic patients after treatment with radioactive the hyperplastic thyroid of the thiouracil treated rat is not strictly iodine . comparable with the hyperplastic thyroid of thyrotoxicosis . there is certainly as yet no clear - cut evidence that the latter is associated with a high blood level 200 i . 
a raised production of thyrotrophic hormone . the conditions may thus be fulfilled for tumour production , i.e. , an initial radiation damage followed by prolonged thyrotrophic hormone stimulation . one would expect the latent period in humans to be many years , and it is possible that in time thyroxine production and thyrotrophic hormone levels might return to normal and the chances of tumour production be much diminished . this could be ensured by deliberate thyroxine medication . 
on present data therefore the carcinogenic danger of radioactive iodine appears to be the initiation of irreversible radiation damage to the thyroid . this renders a greater number of cells liable to tumour formation when later stimulated by thyrotrophic hormone than in the non - radiated gland . 
a proportion of the resultant tumours are likely to be carcinomas , probably of a low grade malignanoy . anaplastic carcinomas may develop , especially when very destructive doses of i131 are used . the dosage lies within the known carcinogenic range . in view of the experimental findings in rats ( of various strains and in different countries ) , it is probable that the present methods of clinical i131 therapy in thyrotoxicosis may eventually prove carcinogenic . 
the radioactive iodine was found to increase the formation of thyroid adenomas as compared with controls in the 5 and 30 1tc groups but not in the 100 , uc group . out of 20 rats treated with combined 30 , tc 1131 and methylthiouracil 5 developed thyroid carcinomas . 
the radiation dosage range to the thyroid of 2270 - 16 , 200 rep in the latter experiment is likely to include the dosage aimed at , of about 9000 rep , in the treatment of graves ' disease . 
the carcinogenic danger of radioiodine therapy is regarded as due to the production of irreversible cells changes in the thyroid , which render them more liable than normal cells to tumour formation when stimulated to undergo hyperplasia . at the same time , a dosage strong enough to interfere with thyroxine synthesis by radiation damage to the thyroid leads indirectly to a prolonged increased output of thyrotrophic hormone from the pituitary . this constitutes a perpetual stimulus to hyperplasia of the thyroid cells . it is thought that the present dosage of i131 used in the treatment of graves ' disease may eventually prove carcinogenic . i am grateful to drs . 
hall. from the cancer research laboratories of the new zealand branch of the british empire cancer campaign , medical school , university of otago , dunedin . received for publication january 1 , 1951 . kseveralmethods are available for studying the effect of prolonged stimu ( 1 ) repeated implanlation of the sex organs by gonadotropic hormones : tation of pituitaries obtained from castrates , ( 2 ) implantation of testis or ovary into the spleen of a castrated animal ( biskind and biskind , 1944 , 1945 ) and ( 3 ) parabiotic junction of a normal animal to a gonadectomized litter - mate . the first method is not very effective owing to the generally short survival of the grafted pituitaries . 
the ingenious method of the biskinds ( 1944 , 1945 ) , however , does not allow one to study how the increased hormonal output of the stimulated gonads affects the accessory sex organs , whereas in parabiotic animals this effect can be observed . 
we have fouiid in the literature only one reference to an investigation in which a similar experimental procedure has been used . strombeck and ekman ( 1949 ) fed a diet containing a.a.f. 
a breakdown of the junction is a rare event . operative mortality was practically nil , but in the second or third week after the operation a great number of pairs died due to incompatibility of the partners no pair sbowing signs of " parabiotic intoxication " survived longer than 5 weeks . the use of more closely inbred rats ( three generations of brother - sister mating ) did not lower the rate of mortality at this critical period . in most experiments acetylaminofluorene - vvas given by stomach tube to the normal partner , who received the carcinogen in doses of 4 mg . 
the treatment with the carcinogen was started 3 to 4 weeks after parabiosis had been established , when consistent gain in weight and the good condition of the animals showed that the operation had been successful . 
were given on 6 consecutive days by stomach tube and in another the carcinogen was given to the twins with their diet ( 4 mg . dailv to each rat for a period of 4 weeks )  . all the rats which received a.a.f. by stomach tube were fed the ordinary stock diet , consisting of meat meal , pollard , bran , maize meal , bone flour and whole wheat supplemented by cabbage . 
was administered with their food were kept for 4 w - eeks on a diet consisting of skimmed milk and whole meal flour supplemented by codliver oil and cabbage . subsequently they received the same food as the other pairs . the twins were killed when a tumour was suspected or when loss of weight indicated that they were in a precarious state of health . pituitary , testis , accessory sex organs , breast , suprarenal and liver of most pairs were studied histologically . 
the pituitaries were fixed in mercury - saline ( 6 per cent ) , the other organs in zenker or neutralized formol - saline . for staining of the pituitaries a modified papanicolau tecbnique was used ' the other organs were stained with ha , matoxylin - eosin or according to weigert - vail cxieson . the material presented consists of 20 r . , airs of parabiotic rats treated with a.a.f. 
the remaining 2 pairs consisted of litter - mates , none of which had been castrated . of the 6 pairs not treated with a.a.f. , 4 were combinations of a normal male joined to a castrated brother , while in the other 2 the male was joined to a spayed female . in addition , cc single " ' rats were treated with a.a.f. 
 - in a similar manner as the normal partners of parabiotic pairs . five young males received by stomach tube 15 doses of the carcinogen and to a group of 10 , 24 doses ofa.a.f. 
only benign lesions of the liver were seen when the animals were killed in the 52nd week of the experiment . in the group treated with 24 dosos malignant hepatomas were also found from the 37th week onwards . 
was seen in any of the rats joined to a partner to whom the carcinogen had been administered . these livers were macroscopically and histologically normal . in the pair of rats who had received a.a.f. 
the hyperplastic seminal vesicles contained macroscopically visible iiodules which were situated near the cephalad margin of the organ ; in addition a fifth neoplasm of microscopic size was found . in all 5 instances the fundamental histological change was the invasion of the muscular coat of the seminal vesicle by atypical glandular epithelium and therefore the lesion must be considered an adenocarcinoma . 
11 and 12 illustrate the appearance of the only tumour of the seminal vesicle found previously in our material . this large anaplastic carcinoma arose in a seminal vesicle of an albino rat of the " sheffield " strain which had received a diet containing a.a.f. 
and para - amino benzoic acid . in another case both seminal vesicles and prostates formed one large mass containing multiple cysts filled with yellowish creamy material . adhesions connected this mass with loops of the bowel . this - lesion was of inflammatory origin and no neoplastic changes were found in it although many sections were studied . as already mentioned not a single neoplastic lesion was found in the castrates joined to brothers treated with a.a.f. in the pair where both received the carcinogen with their food , the kidnev of the castrate showed a lesion of microscopic size which we have not found so far in rats treated with a.a.f. 
the whole picture resembled that of a benign tubular a4enoma of the kidney . morphological sign8 of increa8ed androgen secretion in the normal parabiotic male partner . the changes to be described were found in most cases and were i ' ndependent of the administration of a.a.f. 
the testes were frequently increased in size . their tubules were normal ; the leydig cers were large , having ample cytoplasm and in some animals their numbers h ' ad increased . 
the hyperplasia of prostate and in tlle latter the glandular part of seminal vesicle has already been mentioned . the organ was more stimulated than the outer mesenchyma ' l layer . this disproportionate growth led to compression of the epithehal folds lined by high cylindrical cells . 
the suprarenals of the intact partner differed histologically from those of the castrated twthe glomerulo 'sa of the former was denser and consisted mainly of cells the cytoplasm of which stained wen with eosin . however , thev - were not as frequent the fascicularis contained signet - ring cells . as in the example ifustrated by selye ( 1947 ) on p . 
133 of his text - book of endoin the castrate the glomerulosa was formed by large pale cells , the crinology . fascicularis was free of signet - ring cells and the reticularis was hyperaemic and better developed than in the normal twthe kidneys of the normal partner their surfa ' e was more granular and were larger than the ones of the castrate . histologically the tubular apparatus showed slight degenerative changes , the , connective tissue being more prominent , especially in the outer layer of the cortex . the pituitaries of the norma - i litter - mates were consistently smaher than in the castrates and were sometimes even ' below the weights normally found in our in these pituitaries the numbers of acidophils were increased rats of similar size . with a corresponding decrease in chromophobes . 
griesbach with faintl the periodate - feulgen technique , the cells gave a slight schiff reaction . this agglomeration of basophils was probably not a - permanent structure . zahler ( 1950 ) has described the appearance of nests of basophils in the pituitaries of rats treated with testosterone . the state of parabiosis did not seem to influence the growth of the rats , nor to increase their suseeptibihty tor a.a.f. in the two pairs where two normal males had been joined together , the animals treated with 24 doses of a.a.f. reached the same size as " single " rats , which had received the same dosage of the carcinogen . 
amounts as used in this investigation are administered . in this respect the carcinogen behaves like the steroid hormones which ass only from one to the other partner when extremely high concentrations are reached in the eirculat ' ion of one of them ( zeckwer , 1946 )  . the liver tumours obtained appeared after approximately the same interval as in " single " rats treated with similar amounts of a.a.f. metastases occurred in two instances , proving the malignant character of these hepatomas . 
although the hepatomatous liver was situated in the same peritoneal cavity as the hver of the untreated partner , the latter remained perfectly normal . there was not the slightest indication for an agent derived from the malignant hepatoma affecting the liver of the litter - mate . as mentioned in the introduction a constant flow of gonadotropins passes from the castrate to the normal partner stimulating its gonads . however , no tumours in this respect our experiments failed where of the testicles have been found . those of biskind and bisldnd ( 1945 ) and of twombly , meisel and stout ( 1949 ) these authors obtained tumours in testes which had been grafted succeeded . into the splee ' n . 
two further points should be considered . spermatogenesis is inhibited in testes situated in the abdomen and consequently the morphology of such gonads is considerably altered ; in additionil transplantation of a testis into the spleen involves traumatic injury . these two factors further studies seem are not present in the experimental procedure used by us . to be required to elucidate the conditions essential for tumour induction in the male gonad , a problem which has been recently reviewed by lipschutz ( 1950 )  . the androgens secreted by a testis transplanted into the spleen do not reach the general circulation and therefore the accessory sex organs of rats bearing such the normal parabiotic male joined to a gonadecgrafts are not stimulated . tomized litter - mate shows the effects of increased androgen secretion . in the pairs not treated with a.a.f. 
this stimulation did not lead to tumour formation in any of the target organs , but in the group treated with the carcinogen five tumours appeared in the seminal vesicles of normal partners . 
we have never found this type of tumour occurring spontaneously in the new zealand strain , nor have we seen it in " single " rats only once a carcinoma of the seminal vesicle was observed treated with a.a.f. in an albino rat of the " sheffield " strain treated with a.a.f. our combined material represents the post - mortem findings of nearly a thousand male rats treated with a.a.f. in the rat spontaneous tumours of the seminal vesicle are extremely rare and we have found in the literature only the case reported by flexner and jobling ( 1907 )  . in men , tumours of this organ are also of very lazarus ( 1946 ) has critically reviewed the cases reported , infrequent occurrence . and since then only a few additional observations have been recorded ( mccree , ] 1948 ; gee , 1948 )  . in the case of the thyroid , the carcinogenic action of a.a.f. 
the liyperplasia induced by increased amounts of androgens secreted by the stimulated testis enhances tlle susceptibflity of the seminal vesicle to the carcinogenic action of ' a.a.f. the ' fact that tumours of macroscopic size were found only in rats treated with 24 or more doses of 4 mg . 
and not in animals receiving less suggests that considerably more of the carcinogen is required to bring about tumour development in the stimulated seminal vesicle than was needed for the induction of adenomata in the hyperplastic thyroid ( hall , 1948 )  . that only one minute tumour of the seminal vesicle was found in an intact male joined to a spayed female is probably due to the lower dosage of a.a.f. given to this group and not to the nature of the gonadotropins of the spayed female . only 17 to 20 doses of the carcinogen were administered because great difficulties were encountered in keeping alive pairs of opposite sex for periods necessary for tumour development . however , our material is not large enough to decide this question . to summarize , we consider the tumours of the seminal vesicle to be due to a hormonal imbalance created by gonadotropins in the normal partner . these hormones , by stimulating the gonads of the ' normal partner , increase the androgen production of its testes and therefore are responsible for the hyperplasia of the although unable to promote tumour growth in the testes they , seminal vesicles . bring about conditions in which an accessory sex organ becomes susceptible to the . 
the possibility cannot be excluded that stin more prolonged androgenic stimulation may ultimately bring about tumour formation in the seminal vesicle without the aid of a.a.f. addend - um ( received for publication february 7 , 1951 )  . after the above paper had been submitted an additional pair of parabiotic rats had to be sacrificed . in this pair a normal male was joined in parabiosis to a castrate , the former having received 20 doses of a.a.f. 
left seminal vesicle with loops of small intestine and a hard small nodule was found embedded in these adhesions at approximately 3 mdistance from the upper margin of the fig . 
in normal male rats joined in parabiosis neoplasms were only to castrated or spayed litter - mates have been described . obtained in animals receiving the carcinogen and never in their untreated littermates . ( 2 ) benign or malignant tumours of the liver were found depending on the amounts of the carcinogen given and on the duration of the experiment . 
the mahgnant hepatomas metastasized to the lungs of the animal bearing the cancer of the liver , but never " infected " the other partner . these neoplasms are considered to be due to two factors ; tlle carcinogenic action of a.a.f. 
w.7. received for publication august 22 , 1949 . it has been suggested from studies of the action of inhibitors of s - metabolism on tumour induction by carcinogenic hydrocarbons that s - metabolism and the this association is process of carcinogenesis are closely linked ( crabtree , 1947 )  . emphasized when the properties of azo - carcinogens are considered . 
the products of their metabolism have been shown to inhibit the activities of urease ( potter , 1942 ) and succinoxidase ( elson and hoch - ligeti , 1944 ) , two enzymes dependent kensler , dexter and rhoads upon intact sh - groups for their proper functioning . ( 1942 ) studied the relative inhibitory action of a series of " split - products " on a standard diphospho - pyridine - nucleotide system , and sought to correlate this suggestive activity with the carcinogenic power of the parent azo - compound . parallelisms were found , but a clear - cut relationship did not emerge . much of this work has been based on the conception ( experimentally verified for p - dimethylaminoazobenzene by stevenson , dobriner and rhoads ( 1942 ) , and for azo - benzene by elson and warren ( 1944 ) ) that an azo - carcinogen is initially metabolized by the process of reductive fission with the liberation of an amine and a diamine , and that the latter is the effective carcinogen by virtue of its capacity to interfere with normal enzymic . 
a survey of the azo - compounds so far tested for carcinogenic activity makes it evident that in some cases the amine moiety of the reduced molecule plays a significant role in determining potency , e.g. 
on comparing p - dimethylaminoazobenzene with its p ' - methyl derivative , the introduction of the p ' - methyl group causes a change from a very strong to a very weak carcinogen . the present work was undertaken to probe this problem further . isomeric aminoazotoluenes were chosen as suitable for a study of the relative contributions made by the amines and diamines which would arise from their reduction . 3 ' - azotoluene ( o : o ) and the non - carcinogen well - known carcinogen 4 ' - amino - 2 2 ' - amino - 4 : 5 ' - azotoluene ( p : p ) served as bases of reference , and their behaviour was compared with that of the hybrid compounds o : p and p : o . 
water , at room temthe crystalline hydrochloride suspended in etoh perature ( mehner , 1902 )  . was neutralized with ammonia , and an equal volume of boiling water added . the free base was re - crystallized from aqueous etoh . 
the first characteristic abnormalities visible in the livers of rats differed from those commonly observed in the livers of mice , though the final pictures of tumour emergence were similar in both species . building up the general picture four grades of cellular change have been used . in rat livers perilobular necrosis constituted the primary change , and this was followed by regeneration of liver cells in the necrotic areas . in some regions of regeneration microscopic nodules of hepatoma made their appearance , and later these became visible to the eye as dull grey patches on the surface of the lobes . often a simultaneous intense proliferation of bile ducts was manifest in one or more lobes , and the early phases of cholangioma formation would coincide with the development of small hepatomas . 
no metastases were ever found . in mouse livers no preliminary necrosis was observed , but the cellular pattern became abnormal with great irregularity in the disposition and size of the nuclei . further distortion was accompanied by the formation of cells with giant vacuolated nuclei , which preceded the emergence of microscopic hepatomas . 
the fully developed hepatomas of mice were more malignant than those of rats as judged by the degree of atypical growth , though again no metastases were ever found . it will be noted that the earliest histological changes mentioned sometimes occurred in both rats and mice consuming the basal diet without dye - addition . this response of the liver to diets inadequate in several essential food factors may well reflect the basic disturbance of liver function which is a necessary precursor to the carcinogenic action of azo - compounds . ( b ) relative carcinogenic activity of the six isomeric amrnoazotoluene8 . considering the data summarized in table i from the point of view of the relative carcinogenic potency of these isomers , three points emerge : 1 . 
crabtree the possible influence of sex on the growth rate was assessed by keeping the rats of each series separated into three sub - groups containing respectively 10 males , 10 females and 5 males + 5 females . 
2. - growth curves of rats fed on the basal diet , with addition of 0 06 per cent oor p - toluidine . in the work reported here , the two carcinogenic isomers would yield o - toluidine , while 3 of the 4 growth - stimulating isomers would yield p - toluidine as the primary products of reductive fission . the possible effects on growth of these two toluidines were therefore tested . forty - five rats of the 52 strain , each weighing 110 - 130 g . , were divided into three groups of 15 . 
two groups were fed on the basal diet containing 0.06 per cent of either o - toluidine or p - toluidine , and the third group received the basal diet alone . 
each group of 15 rats was subdivided into three separated groups of 5 males , 5 females , and 5 containing males and females . in the latter group two litters were born during the first 3 months , but none subsequently . 
on the other ha ; nd , miller and miller ( 1947 ) emphasize the importance of the protein constitution of the host , and associate the likelihood of tumours developing with the degree to which an azo - compound is " bound " to the proteins of rat livers . in the case of rats consuming p - dimethylaminoazobenzene this fixation is prominent , but does not occur in species resistant to the carcinogenic action of the substance . these differences can only be attributed to the special properties of the proteins characteristic for each species . the " split - product " hypothesis . kirby ( 1945 ) has reviewed the work bearing on this hypothesis of the mechanism of carcinogenesis by azo - compounds , and throws doubt on its validity by citing several examples which fail to conform with its main premises . 
the experiments demonstrated that o : o and o : p were carcinogenic , while p : p and p : o were non - carcinogenic . reviewing these results in the light of the " split - product " hypothesis , no correlation between carcinogenic activity and the potential diamine fission products is found . 
p : p and o : p should yield the same " innocuous " o - toluylene diamine , while o : o and o : p should yield the same " active " .p - toluylene diamine , but the facts are otherwise , since each of these pairs contains one carcinogen and one non - carcinogen . by contrast , when the amine halves of the reduced molecule are considered , the results show that the two isomers which should yield p - toluidine on reductive fission - p : p and p : o - are non - carcinogenic , while the pair yielding o - toluidine in brief , if carcinogenic activity is indeed - o : o and o p - are carcinogenic . a consequence of the action of the " split - products , " it is the amine , and not the diamine , which determines the subsequent biological response . the literature contains several examples of the controlling influence which a methyl group exerts on carcinogenesis , when attached at a para position with miller and baumann ( 1945 ) compared the activities respect to the azo - group . of the o ' , m ' , and p ' methyl derivatives of p - dimethylaminoazobenzene with that of the parent compound . 
the m ' - compound was extremely active ( 7 rats out of 8 bearing liver tumours in 4 months ) , the o ' - compound moderately active ( 4 rats out of 9 bearing tumours in 8 months ) , and the p ' - compound was very weakly carcinogenic ( 1 rat out of 10 with a tumour in 10 months )  . 
nagao ( 1941 ) also found that p ' - methyl - p - dimethylaminoazobenzene was only a weak carcinogen , and that the substances formed by placing a further methyl group in the ring carrying the dimethylamino - group were entirely innocuous . sugiura ( 1948 ) tested a series of derivatives of p - methylaminoazobenzene containing an additional methyl group in the o ' , m ' or p ' positions . the order of potency - m ' > o ' > p ' was similar to that mentioned above . all these observations seem relevant to the present work . 
the common feature is the great loss of tumour - producing activity which results when a methyl group is added in the p ' position to the parent carcinogenic molecule , forming derivatives with the potentiality of liberating p - toluidine on reductive fission . a working hypothesis is put forward tentatively in an attempt to co - ordinate the data outlined above . 
when the structural features and the biological action of these six isomeric azotoluenes are considered , a correlation is evident between their growth - stimulating properties , their lack of carcinogenic power , and the presence of an additional methyl group in the position described . 
crabtree and hilbert ( 1888 ) fed the three isomers of acetotoluidine to dogs . o - acetotoluidine was oxidized to an aminophenol and isolated as methylbenzoxalone , while mand p - acetotoluidines were excreted as acetylated amino - benzoic acids . it may therefore be conjectured that all azo - compounds containing a methyl group at a position para to the azo - group will yield p - aminobenzoic acid as a final product of their metabolic degradation within the rat . the experiment pictured in fig . 
six isomeric aminoazotoluenes have been tested for their carcinogenic activity in the livers of mice and rats , when added at 0 06 per cent concentration to a standard , semi - synthetic diet . 
since the detoxication of p - toluidine can produce p - aminobenzoic acid , the possible relation between folic acid metabolism and the mechanism of cancer induction is considered . i am greatly indebted to e . 
bruzzone. from the department of experimental medicine , national health service of chile , santiago . received for publication june 9 , 1949 . abdominal fibroids induced in the guinea - pig by a - oestradiol ( nelson , 1937 ; lipschutz and iglesias , 1939 ) are prevented when progesterone or other 3 - ketosteroids are administered simultaneously with the oestrogen ( lipschutz and vargas , 1941 ; lipschutz , 1944 ; lipschutz , iglesias , bruzzone , fuenzalida and riesco , 1948 )  . 
he has shown that bacterial growth can be understood in terms of certain simple mathematical relationships , in spite of the fact that the molecular mechanisms involved are extraordinarily complicated . in this paper an attempt is made to see if such an approacli may help to throw a little light on the problem of tumour formation and growth . 
a brief review of carcinogene8i , 3 . the various ways of producing cancer have been reviewed in a recent paper by boyland ( 1952 )  . but it will help for the purposes of the present communicatioii to provide a summary of the results . ( a ) chemical carcinogens . - the first chemical compound to be identified as a carcinogenic agent was 1 : 2 : 5 : 6 - dibenzanthracene ( cook , hieger , kennaway and mayneord , 1932 )  . since that time , the polycyclic hydrocarbons have been investigated systematically from this point of view . 
a certain degree of specificity has been observed and it has been correlated to some extent with the presence of a region of high electron density ( k region , schmidt , 1939 ) , within the molecule . some recent work has suggested , however , that the carcinogenic activity of the polycyclic hydrocarbons may be related in part to their ability to undergo autooxidation and liberate free radicals ( alexander , 1952 )  . the second class of carcinogenic compounds includes mustard gas ( heston , 1950 ) , nitrogen mustards ( boyland and horning , 1949 ) , epoxides , mesyl glycols ( haddow and timmis , 19051 ) , etc . 
these compounds are all known to act as alkylating or esterifying agents and probably prodtice their effects on the body by this type of reaction . certain inorganic salts of beryllium and zinc can produce tumours ( bagg , 1936 )  . there are also a number of other chemical compoiinds , showing little relationship 260 f . 
urethane it might , from the ( nettleship and henshaw , 1943 ) is an example of this kind . nature of its amide group be expected to attack the secondary forces of cohesion known as hydrogen bonds , which play a most important part in maintaining the structure of biological organeres such as chromosomes ( ambrose and gopalayengar , 1952 )  . ( b ) physical methods of producing cancer . - it appears that the simple process of implanting an inert object such as a disc of bakelite ( tumer , 1941 ) or sheets of cellophane ( oppenheimer , oppenheimer and stout , 1948 ) into a tissue can produce a tumour , while an extreme change of temperature produced by the application of carbon dioxide snow ( berenblum , 1929 ) can have a similar effect . although the ionising radiations can induce cancer , it is probable that their mode of action is indirect and is due to the formation of free radicals ( butler and conway , 1952 )  . ( c ) biological carcinogens . - the well - known rous sarcoma can be propagated by virus particles ( rous , 1936 )  . certain parasitic organisms are able to cause a malignant change to occur in the tissue ( e.g. , phytomonas tumefaciens in plants , smith , 1916 )  . 
the spontaneous tumours , whose origins are unknown should perhaps be considered to be due to the action of a biological carcinogen . it was pointed out by haddow in 1938 that there was a striking multiplicity of tumour - producing agents and , as can be seen from the summary given above , the number has greatly increased since that time ( hartwell , 1951 )  . 
the agents appear to have one feature in common ; they may be expected to lead to a more random configuration of the molecular structure within the cell , than is present in the normal tissue . 
we will try , at a later stage , to see ff the models may have any bearing on the behaviour of real biological systems . ( a ) classical treatment . ( 1 ) simple growth . - we will consider the very simple system shown in fig . 
is considered to contain a dilute solution of metabolite molecules ; the molecules could , for example , be molecules of amino acids . it will be assumed that the solution is ideal ; i.e. , that the molecules are quite independent of each other and do not interact with the solvent molecules . 
the work in thermodynamic which has to be done is generally known as osmotic work . nomenclature the work which must be done on the system is in this case expressed as a change ofentropy . 
1. in real systems the energy required for the decrease of entropy is in some cases balanced by a change in the potential energy , e.g. , the formation of a chemical precipitate is accompanied by a decrease of potential energy , because forces of attraction occur betw ' een the molecules forming the precipitate and a closer approach of the molecules leads to a decrease of potential energy . ( 2 ) growth with differentiation . - we will at this stage consider the problem of growth with differentiation since it has been the subject of a beautiful study by tyler ( 1939 ) , using sea urchin eggs , although the treatment is not in this case strictly thermodynamic . the cells at the two cell stage of embryonic development are isolated . 
2d. it is possible to compare the energy requirements for growth in the case of the normal and dwarf embryos by making use of the principle of dimensional analysis ( galmeo , rayleigh , tolman , buckingham )  . these principles tell us that there is a relationsfii . 
the war thickness is d / a / 2 units and fie , 2 . ( in d the longer line between arrows indicates r . ) suppose that an invaginot d - umits as in the real dwarf embryo shown in fig . 
3b the molecules are shown to be arranged in a hnear sequence , inert gas . in the form of a polymer chain . in this case the chain is coiled in an irregular in fig . 
3a there are very few regtrictions upon they are called , in the three figures . it is only necessary that one molethe arrangement of the metabohte molecules . cule should not coincide with another and that they should an be confined within in fig . 
3b we see that the number of possible ways of the sphere of radius r . arranging the units is greatly reduced , because each unit must be maintained at a 264 e . 
a statistical thermodynamic treatment makes it possible to express the entropy ( s ) of the systems in terms of the number of conformations with the most probable energy . if n is the number of conformations with this energy : k log n , where k is a constant . the logarithmic form occurs because the result is obtained by integration over a large number of terms . it wffl be seen that the simple process of polymerization must lead to a decrease in the entropy of the systems and that any process leading to a preferred orientation of the polymer molecules must lead to a further decrease . let us now consider a case in which we have a number of the spherical units of the kind shown in fig . 
4b is shown a similar corection of units which are now arranged another . if we now consider the configurational entropy in a definite sequence or pattem . of the polymer chlains in an individual spherical unit , we see that in the case of fig . 
4b the restriction in the configurations of the spheres , produced by arranging them in a definite pattern , wfll also restrict the number of configurations of the polymer chain 's inside the spheres . quantitatively , the actual energy difference . 
the building up of biological structures takes place by a complicated process of cefl division in which metabohte molecules are constantly being absorbed from the surroundings , while energy sources are broken down to carbon dioxide and water and subsequently discarded ; i.e. , we are dealing with an open system in which there is a constant flow of material . 
4 and let us suppose for a moment that they represent living cells containin ' g protein , nucleic acid , polysaccharide and lipid molecules . in fig 4a they are considered : to be unicellular organisms which do not interact in any way ; in fig . 
now we may be able to produce a series of reversible processes whereby we could bring metabolite niolecules in dilute solution first within the semi - permeable membrane of the cell by a process of isothermal compression , then into an orientated configuration by a series of compressions and extensions in the sohd state . because no process can be more efficient than a reversible process the energy changes involved would be the least that could possibly occur in the formation of these structures . in the actual biological process of synthesis , where events take place at a finite rate , the energy requirements for synthesis must be greater than they would be in our hypothetical models , we have also neglected for a reversib - le process . changes of internal energy in the systethe formation of polymers involves the synthesis of chemical bonds between the nionomer units . 
the synthesis of the peptide bond - co - nh - from the free amino acids h2n - c - - cooh is an endothermic reaction which requires a supply of energy , and the same is true for other biological polymers . 
the two factors of irreversibility and internal energy changes will require that all growth processes will involve a continuous supply of energy in excess of that which would be required for the entropy component in our hypothetical models . 
but these factors do not prevent us from calculating the entropy term in a real biological system . fowler and guggenheim ( 1939 ) point out that material which is not in an equihbirum state still has a definite entropy . 
ambrose the cell , the number of units of which they are composed is very large and although the number of configurations is restricted it is still very large . in the succeeding sections in the present paper , we shafl attempt to make some purely quahtative observations on what we might expect to be the differences in energy requirements for the growth of normal cells and tumour cells , in so far as the entropy component is concerned . 
m corresponds , as before , to b corresponds to the entropy state of the materials incormetabohte molecules . porated within the embryonic cell . this is represented as a lower entropy than the cell a . 
because the cell contains within itself a molecular structure which is capable of interacting with other cers . b ' + d represents the cell when differentiated and fulfilling its proper function . 
an attack upon the cer which leads to a more randoni condition of its parts can lead to an increase of - entropy . we might expect to find therefore that such an attack would lead to a reversal of the sequence shown in fig . 
a cell ' vh11 remain in an equirbrium state , or wir grow , depending upon whether the rate of synthesis is equal to or greater than the rate of degradation of the striictural components . 
5c the cell is considered to be in an equihbrium state , i.e. , in the condition of dynamic equilibrium in a polypbase system suggested by gowland hopkins ( quoted by baldwin , 1947 )  . 
5c represents the energy requirement for the carrying out of the proper function of the cefl in its differentiated foras for the autosynthetic system , the synthesis of extra - cellular material is also associated with a condition of dynamic equilibriumany of the extracellular proteins , for example , represent unstable svstenis . insuhn exhibts a spontaneous denaturation jaqueous solution which appears to be due to an autocatalytic mechanism ( waugb , 1946 ; ambrose and elliott , 1951 )  . in order that a steady concentration of materials can be present in the organism , continual synthesis must occur to make up for the loss . 
the regionrrepresents the reservoir of energy producing material in the cell , together with its associated system of enzymes . in the normal differentiated cell all the levelsof a , dandrare steady . 
we note that the present simple theory accounts for the existence of the steady state in in any system in which a large number of chemical differentiated organisms . reactions occur in a stepwise sequence , the products of one reaction being utihzed by the next , as occurs in a series of enzymatic reactions in a unicerular orgamsm , the growth curve should obey an exponential law ( hinshelwood , 1952 ) , i.e. , the rate of growth is proportioned to the number of cers present . various possible explanations for this difference have been suggested as for example by rashevsky ( 1945 ) who proposes that each cer prodiices some substance which inhibits the growth of other cells . 
chromosome breakage may therefore be a gross manifestation of the kind of change in the synthetic mechanism which can produce cancer cells . gopal - ayengar ( 1953 ) has made an extensive studv of the chromosome abnormalities which are found in normal cells and in tumour cells , particularly ascites tumour cells . 
the ducts can be seen in cross section ; it will be seen that they are arranged in the form of honow cylinders with the cefls forming a single layer round the wall . in a case of carc ' moma it is the duct cers which become mahgnant . 
6. as in the analysis given in section iib , it would be possible to calculate the energy differences for the three forms of growth , if a reversible process for changing from one form to the other could be visuahzed . 
the increase in surface area associated with the formation of the new surface requires that work must be done to provide the surface energy . in addition , a posit ' lve pressure must be apphed witbin the bubble . 
6 will require still more . were an elastic solid much more work would have to be done to form the hollow it would be similar to blowing up a rubber tube . 
the successive stages in the loss of differentiation , in this case of duct carcinoma , do therefore appear to represe ' nt states of increasing entropy , at least in so far as the observed changes of form are concemed . phenomena of this kind are again clearly irustrated in the very complete account of the genetic origin and morphology of the melanomata by dawson it is generally agreed that the naevi are derived from cefls which would , ( 1925 )  . in normal tissue , be engaged in building up a layer or sheet type of tissue . 
the transition from a layer structure to a warty form and finafly to the smooth malignant tumour represent successive stages in the reduction of surface area / unit mass for the hquid case . 
as in the previous example , the elastic case would require successively increasing amounts of energy for the formation of the structure corresponding to a departure from the uniformly spherical form . we will now examine some changes associated with tumour growth , which are taking place on a molecular scale , and can be considered in terms of the analysis in fig . 
this is because the refractive index of the fibres measured parallel to their length is different from the refractive hidex measured perpendicular to their length ; the brightness of the fibres , for a given thickness , is in these pictures a measure of the degree of molecular orientation which has been achieved during the synthesis , e.g. , the fibres of fig . 
the fibroblast cells are still laying dow - n fibrous material , but it is much more wavy in appearance , as was the case for the tumour derived from the uterine wall . 
the tissue was stained for coragen , using the technique of van gieson . the tumour showed a considerable reduction in the amount of collagen present as compared with the nornial tissue . 
20 still gives a considerable colour due to - collagen . it will be seen that there is practically no detectable birefringence m the tumour region which is on the right of the field . this result suggests that there is a relative decrease in the amount of orientated fibrous material deposited in the tumour region . in fig 9 is shown a section of normal breast tissue , ' hotographed under the polarizing microscope . 
a fibrous structure can be seen but there is a complete absence of any birefringence . the experimental evidence given above therefore appears to be in agreemedt with the general conclusion of section iv , that tumour growth corresponds to disordered states of high entropy and that in so far as the forms of growth and molecular orientation of fibrous protein are concerned the successive stages of malignancy do in fact appear to be associated with successive increases of entropy . it may be pointed out that a number of other instances could be quoted in favour of the general picture . 
the principle may help a httle in understanding the relationship between carcinogenesis and growth inhibition , as first described by haddow ( 1947 )  . if the carcinogens do in fact have a disorganising effect upon the synthetic system , it is more likely that in a given instance they wir disorganise the structure to such an extent that it can no longer function at all . 
of the hydrocarbon suspended in arachis oil , by intraperitoneal injection , in no case , however , even with 100 mg . and the rats weighed daily as a group . average 1 : 2 : 5 : 6 - dibenzanthracene , after 9 days a second injection of growth rate of any group of rats observed . 1 : 2 : 5 : 6 - dibenzanthracene was given and again no the same amounts of constant effect was observed , but after several days considerable fluctuations in the growth rates occurred , and eventually 21 days after the first injection all the groups showed a lower average weight than the control group , which had although the average weight of the received injections of arachis oil alone . group which had received the two injections of 100 mg . 
1 : 2 : 5 : 6 - dibenzanthracene was slightly lower than that of the other group , there was no direct relation to the amount of hydrocarbon given , and the rats receiving 50 mg . had a higher average weight than the group which had been given 25 mg . 
of the other five left as controls . pituitary extract daily had practically no effect on the growth of the animals , but when the amount was increased to 1 c.c. 
1 : 2 : 5 : 6 - dibenzanthracene to rats maintained on a 20 per cent protein diet causes no immediate inhibition of growth , a delayed toxic effect occurs which ultimately results in death of all the animals . 
when the length of time survival of the dibenzanthracene - treated rats on the 20 per cent protein diet is compared with that of the similarly treated animals maintained on the 10 per cent protein diet , as shown in fig . 
6 , it is seen that although in the latter group there is an immediate growth inhibitory action , the animals survive for a longer period after treatment . ( mean survival time of 17 animals on the 20 per cent protein diet was 44 days after dibenzanthracene injection , whilst that of the same number of animals on the 10 per cent protein diet was 67 days . ) effect of 1 : 2 : 5 : 6 - dibenzanthracene on tail growth in rats maintained on a 20 per cent protein diet . an attempt was made to see if any growth - inhibiting action of 1 : 2 : 5 : 6 - dibenzanthracene could be demonstrated by measuring the increase in tail length of rats treated with this hydrocarbon . young male rats of about 50 g . 
the animals were lightly anaesthetized with ether , placed on x - ray film in the prone position , and skiagrams taken of the bones from the pelvic region to the tip of the tail . 
of stilboestrol was injected in all but two of the animals growth of the tail was markedly into each rat . inhibited , and in 3 rats tail growth practically ceased . 
the difference in the diets used is mainly of the protein content and , since the fat content of the diets is the same , their total it would thus appear that the procalorific values do not differ appreciably . tective action of the 20 per cent protein diet is directly attributable to its high this is confirmed by the protective action of the 25 per cent protein content . protein diet , which differs from the unprotective 10 per cent protein diet only in protein content . the growth - inhibitory action of the hydrocarbon does not appear to be the result of a direct action on the anterior lobe of the pituitary gland causing interadministration of growth hormone ference with growth hormone secretion . to rats maintained on the high protein diet and treated with dibenzanthracene does , in most cases , bring about some increase in growth , but appears at the same time to increase the toxic action of the hydrocarbon since this growth dibenzanthracene is increase is rapidly followed by the death of the animal . only very slightly soluble in body fluids , and when administered by intraperitoneal injection remains in the peritoneum for a considerable period of time . metabolism of the compound probably takes place by combination with since this combination is sulphydryl - containing substances as its first stage . not the direct cause of its growth - inhibiting action ( elson , goulden and warren , 1947 ) , it is probable that a later stage metabolic product is responsible for this effect . 
one of the effects of the growth hormone is to increase the total metabolism of the animal , and it seems likely that this results in increased absorption and metabolism of the dibenzanthracene from the peritoneum of the treated animal . 
of 1 : 2 : 5 : 6dibenzanthracene per rat usually results in very little growth inhibition for about 14 days , after which the animals , at varying intervals , lose weight rapidly and die . 
howatson. * from the cancer research department , royal beatson memorial hospital , glasgow . received for publication july 6 , 1953 . several attempts have been made to purify and isolate the particulate agent or virus associated with mammary carcinoma in certain strains of mice , with a view to its identification and the study of its morphology by electron microscopy . the conclusions reached by different observers , particularly about the average size of the particles identified with the active agent , have been considerably at variance . passey , dmochowski , reed and astbury ( 1950 ) and dmochowski , and passey ( 1952 ) have described an extensive investigation in which biological tests for the presence of the agent in extracts of tissues and milk from high and low cancer strain mice were correlated with the appearance of the same extracts in the electron microscope . 
they conclude that the tumour - inducing activity is associated with typical particles of diameter 200 - 300 a , preparations of high activity containing large numbers of these particles and inactive extracts containing none or very few . graff et al ( 1949 ) , using as starting material milk from riii and c57 mice , and c57 mice foster - nursed by riii mothers , claim to have isolated from infected milk , after treatment with chymotryspin and differential centrifugation , particles of diameter 750 - 1000 a which they regard as the mouse mammary carcinoma virus . 
 ( 1950 ) but this could hardly account for the large difference in size . porter and thompson ( 1948 ) carried out an electron microscope investigation of epithelial cells grown in tissue culture from spontaneous and transplanted adenocarcinoma in c3h mice . 
they found that in three out of six preparations spherical particles were present in the cytoplasm of the cells . these had a double structure - a dense centre portion of diameter about 750 a and a less dense outer zone of diameter approximately 1300 a . 
they conclude that their findings are consonant with the view that the particles represent the milk agent . huseby , barnum and bittner ( 1950 ) , on the other hand , observed particles of diameter 500 - 2500 a in extracts of milk and mammary gland tissue but were unable to distinguish in the active extracts any distinctive particles which could be identified with the virus . in view of the long period required to obtain results from biological tests for the agent , any method of assaying rapidly the activity would be of great value in experimental work . 
howatson it was thought that a new attack on the problem involving a direct comparison of extracts of tumours from agent - carrying and agent - free mice of the same strain might give a conclusive answer . for our experiments we were fortunate in having available , through the courtesy of b . 
a commercially produced atomiser or spray gun operated from the high - pressure air line was found to be satisfactory the specimen was deposited by directing a fine spray of droplets of the extract to be examined on to filmed specimen mounts . 
each droplet is a representative sample of the extract and most are small enough to be included in a single micrograph . thus to obtain information about a given extract it is necessary to photograph only a few droplet patterns instead of searching the whole field . 
as far as possible the treatment of agent - containing and agent - free tumours was identical . a weighed amount of tissue was homogenised for a few minutes in a glass homogeniser , the suspending fluid ( usually distilled water ) being added slowly to give a final tissue concentration of 2 per cent . 
both extracts contain much particulate material together with fragments of mitochondria , collagen fibres and other cellular debris . these larger fragments can be removed if desired by further centrifugation , leaving an array of macromolecular particles on a background composed of low molecular weight material , which is not generally resolved by the electron microscope . 
the particles are approximately spherical and , although covering a range of size , are predominantly of diameter 250 - 300 a , the size attributed to the milk agent by dmochowski and passey ( 1952 )  . the particle - size distribution based in each case on the measurement of 200 particles , is shown in histogram form in fig . 
the number of particles present in a given extract depends somewhat on the type of tumour , the efficiency of homogenisation and the centrifugal forces employed but provided the simple standard procedures outlined were adhered to , the variations were small . despite careful search , it was not found possible to detect any significant difference in the number , size or appearance of the particles present in the droplet patterns obtained from extracts of agent - containing and agent - free tumours . the failure to observe any difference in the tumour extracts is readily understood when similarly prepared extracts of normal organs are investigated . nearly every case examined , including spleen , liver , marrow , brain and lymph 396 a . 
14 ( c ) shows that diameter . in size - distribution , these presumably normal particles do not differ significantly from those derived from tumour tissue . it is apparent that simple fractionation procedures are not sufficient to effect a separation enabling the pathogenic particles to be distinguished from the numerous cell particulates of similar size and shape which are also present . 
14. - size distribution of particles in extracts of ( a ) agent - containing mouse m ary tumour , ( b ) agent - free mouse mammary tumour , and ( c ) normal mouse spleen . the field of the smaller animal viruses , where it has been satisfactorily overcome in only a few cases . 
an attempt was made to differentiate in this way between normal and infective particles by studying the action of the enzymes trypsin , chymotrypsin , ribonuclease and deoxyribonuclease on extracts of agent containing and agent - free tumours . 
the buffer salts , which crystallise on drying , can fairly readily be distinguished from organic material , but the latter shows a tendency to aggregate in the presence of electrolytes . this effect had previously 398 a . 
a comparison was made between extracts of the mill hill 2 endothelioma which has all the attributes of a " virus " tumour and the chemically - induced grch 16 tumour which in addition rous no . 
1 sarcoma and has no such " filterable " properties . biological tests for the infectivity normal chicken tissue extracts were examined . of the various preparations were carried out in many cases . the methods adopted were similar to those previously described , and need not fig . 
extracts of the first type regularly excite tamours on injection into susceptible birds , whereas the second type of extract , though apparently of similar particulate content , is these micrographs may be compared with fig . 
9 , which completely innocuous . shows an extract from a normal chicken spleen . it is again evident that the infective particles , if present , are masked by the large quantity of other particulate material which occurs in normal as well as tumour tissue extracts . 
the lower limit of size ( 600 a ) given by claude ( 1946 ) appears to be arbitrary . certainly most of the particles observed were smaller than this , though some shrinkage during desiccation may occur . 
the presence of still smaller cytoplasmic particles in cells fixed by osmium tetroxide has recently been demonstrated by high resolution electron micrographs of ultra - thin sections ( eaves , 1953 , private communication )  . there is no doubt that the particles observed in the present experiments are products of the disintegrated cells , the spraying method giving consistent and conclusive evidence of their presence in the extracts . 
the dissolving action of trypsin and chymotrypsin is a strong indication that they are protein in nature . the crystalline trypsin used was tested for the presence of particulate material by spraying on to coated specimen mounts a solution 100 times as strong as that used in the experiments . 
12 is shown a partially disintegrated mitochondrion with what appears to be an extrusion of particulate material . a group of mitochondrial membranes largely devoid of contents is illustrated in fig . 
it seems very probable that some of the particles observed in tissue extracts are derived from such disruptions . it is clear that the range of size of the normal cell particulates covers that of the smaller animal viruses . this is a major difficulty in the isolation of any presumed virus by purely physical methods such as differential centrifugation or in chemical composition also , the microsomes are found to be strikfiltration . ingly similar to certain known viruses , so that attempts at chemical or enzymatic separation may also fail . there remains the possibility of using the highly specific methods of serology , though even these may not distinguish normal from pathogenic particles unless the latter are of extraneous origin . the difficulty of identifying tumour - inciting particles , particularly the milk agent , by electron microscopy is enhanced by lack of independent data on size . estmates have been made by finding the centrifugal force required to clear the supernatant of infectious material . there have also been some attempts to deduce the approximate size of the milk agent by measurement of sedimentation rates in an ultracentrifuge ( kahler and bryan ( 1943 ) )  . 
the presence of normal particles and aggregates makes the interpretation of such experiments somewhat doubtful , but the evidence is in favour of the association of the infectivity with rather small particles of molecular weight 3 - 5 million , corresponding to a particle diameter of at most a few hundred angstroms . it is remarkable that no attempts appear to have been made to determine the approximate size of the milk factor particles by means of gradacol membranes , as has been done for example in the case of several fowl tumour viruses . 
by this method it should be possible to determine conclusively whether the infectivity is associated with particles in the large ( > 1000 a ) or small ( < 300 a ) size range . it is clear that further work is necessary to establish the elementary physical properties of the tumour viruses . 
the examination of tissue culture cells and of thin sections of fixed tissue may give valuable information , but is not likely to be conclusive because of the difficulty of relating the observations to biological tests . on the other hand , the method of extracting homogenised tissue , while convenient for biological testing , presents problems arising from the presence of much contaminating material which can only be satisfactorily solved by the discovery of some action highly specific to the virus , which can be used for its isolation . in conclusion it is emphasised that the presence in tumour extracts of particulate material in the size range of the smaller animal viruses is no indication that the particles are in any way related to virus activity , unless it can be conclusively 400 a . 
i fowl sarcoma material which had been subjected to repeated applications of cold possessed a greater tumour - producing activity than those prepared from similar material which had not been subjected to this ' treatment ( selbie and mcintosh , in explanation of this finding selbie and mcintosh ( 1939 ) suggested 1939 )  . that the freezing broke up the tissue fragments , ' and thus allowed a greater liberation of virus than would otherwise have been possible . in the course of some recent quantitative investigations into the effects of cold and desiccation on the rous no . 
the chromatographic study of riley ( 1950 ) in which adsorption of the rous virus was shown to take place on to a column of diatomaceous earth suggested that adsorption would also take place when this virus was passed through berkefold filters which are likewise composed of diatomaceous earth . in the present work an attempt has been made to assess the decrease in the tumour - producing activity of suspensions of the rous no . 
i fowl sarcoma virus experiments are also reported which which berkefeld filtration brings about . were designed to show whether or not this decrease was due to adsorption of the virus on to the berkefeld candle during filtration , and in addition , an investigation has been carried out to find whether repeated freezing and thawing affects the filterability of the rous virus . 
the tumour was removed , cut small with scissors , and disinte a mechanical blender ; the method ated in has been described in detail in a previous paper ( epstein and cook , 1951 )  . 
filtration was continued until the filter candle was quite empty , as shown by air bubbles being sucked through after the filtered after use each filter candle was tested by passing through it 80 c.c. 
a sample was taken from the resulting filtrate , part of it being set aside ready for inoculation and part being used to make dilutions in serial tenfold steps with sahne ; a portion of each dilution was kept for inoculation . experiment8 4 and 5 ( recovery of virus from filter )  . - these experiments were performed in their early part as a repetition of the foregoing in which samples of a virus suspension and the berkefeld filtrate derived from it were couected and diluted in serial tenfold steps with saline for inoculation . in addition , however , a sahne wash of the filter was prepared ; a sample was taken from the saline wash , part being set aside undiluted for inoculation and part being used to make dilutions in serial tenfold steps with saline . 
a portion of each dilution was kept for inoculation . experiment8 6 , 7 , 8 and 9 ( effect of freezing and thawing on filterability )  . disintegrated tumour was prepared and in ' each of these experiments was divided into two samples , one being left untreated and the other being subjected to repeated freezing and thawing . 
suspension berkefeld untreated frozen and thawed x 6 f : 61trate untreated frozenandthawed x 6 untreated frozen and thaweci x 6 - .10% virus suspension berkefeld filtrate - .10% virus suspension berkefeld filtrate 10% virus suspension berkefeld filtrate untreated frozenandthawed x 6 untreated frozenandthawed x 6 untreated frozenandthawed x 6 untreated frozenandthawed x 6 dilutions of preparation and number of tumours arising from 4 inoculatioins of each . 10 - 2 10 - 11 10 - 4 10 - 5 10 - 0 10 - 11 2 + ( 2 ) 0 3 + ( l ) filter test . - - - n prod . 
now , froni the results shown in table ii , it is clear that an appreciable amount of the tumour - producing activity losb when virus suspensions were passed through berkefeld candles could be recovered by washing saline through the latter after use . in the experiments shown in table ii the filters when tested retained in each case both chr . 
aureu8 making it impossible for the lost tumour - producing activity , recovered on washing the filters with saline , to have been due to cells . this recoverability of at least part of the tumour - producing activity lost on filtering rous virus suspensions gives further support for . 
epstein freezing and thawing were passed through a berkefeld candle to give a filtrate ' , as where those made from similar untreated disintegrated tumour were so filtered . the application of repeated freezing and thawing to rous sarcoirna material has thus been found not to increase the ability of the virus contained in it to pass berkefeld filters . 
the present work has also shown ( table 111 ) , in confirmation of that previously reported ( epstein , 1951 ) , that repeated freezing and thawing of mechanically disintegrat - ed rous tumour materizal did not release more virus on extraction than where no such treatment was applied . 
from these two facts it appears that repeated freezing and thawing has no action on the rous virus likely to make berkefeld filtrates of treated tumour material , prepared as described here , more active than those made from untreated material . 
the results shown in table iii demonstrate this clearly ; they are at variance with those reported by selbie and mcintosh ( 1939 )  . in attempting to relate the results of the present work to those of previous investigators with which they do not agree , two possible explanations require consideration : firstly , it must be remembered that selbie and mcintosh carried out their during that time the rous virus may possibly have investigations 13 years ago . undergone variations affecting its properties which might account for the variations in the experimental results obtained . secondly , the method of extracting the rous virus employed by selbie and mcintosh ( 1939 ) consisted of coarse mincing of the tumour material followed by repeated freezing and thawing was then applied to the grinding with sand . resulting preparation , and may well have contributed to the achieving of complete disintegration of the tumour and the maximum extraction of virus from it . 
in the present work , however , disintegration of the tumour material was brought about mechanicall before the cold was applied , and would seem to have been so complete that the repeated freezing and thawing could not have any further this is considered to be the most likely explanation of the contradiction effect . between the findings reported by selbie and mcintosh ( 1939 ) and those recorded in this communication . in consequence of the results of the present work it is thought that where in the future attempts are to be made to demonstrate the presence of viruses in tumours not hitherto known to possess them , borkefeld filtration , with or without previous repeated freezing and thawing of the material to be filtered , should be avoided . 
i fowl sarcoma virus are described . also described are experiments in which the effect of repeated freezing and thawing on the filterabihty of this virus has been investigated . susceptible inbred brown leghorn fowl have been used . the method used to disintegrate rous sarcoma tissue mechanically in order to make from it a virus suspension is set forth . 
the technique used to apply repeated freezing and thawing to disintegrated rous tumour is indicated , as is the technique used in berkefeld filtrat - ion of suspensions of the virus . a titration method has been employed in which preparations whose tumourproducing activities were to be compared have been diluted in serial tenfold steps with saline and inoculations made with each dilution . the results show that wben rous virus suspensions prepared by extracting disintegrated rous tumour with saline were passed through berkefeld filters , part of the virus became adsorbed on to the filter . 
some authors ( willis , 1948 ) believe that the association is mainly indirect , and that the nutritional features result chiefly from anorexia , ulceration and infection , to which , with cancers of the alimentary tract especially , are added disordered digestion and absorption of food . 
others consider that the connection may be morp , direct , perhaps through metabolic competition for circulating nutrients , and in - recent years animal experiments have lent some support for this hypothesis . a reduction in plasma albumin concentration has been noted both in cancer patients and in tumour - bearing animals ( abols , rekers , binkley , pack and rhoads , 1942 ; siebert , siebert , atno and campbell , i 947 ; huggins , 1949 )  . 
a - n early fall in the blood haemoglobin level ( greenstein , andervont and thompson , 11942 taylor and pollack , 1942 ; el mahairy , 1950 ) and marked reductions in tissue enzyme activity , e.g. , in liver catalase , in organs far d - istant from the growth have been similarly recorded ( greenstein , 1947 )  . while tb - ere is no doubt that a growing cancer often exerts widespread effects on general metabolism , no study has yet been made of any process common to both normal and tumour cells in whicb any such metabolic competition might be expected to disclose itself . 
with this in mind , therefore , it seemed profitable to niake a comparative study in normal and tumour - bearing animals of the occurrence of mitosis - a phase of the growth process which to the best of our present knowledge presents similar features in botb types of cell . 
in some experiments the protein content was doubled at the expense of the carbohydrate ; this " high - protein " diet contained 40 per cent of casewith the aid of a little water all the ingredients were mixed into a stiff paste which the mice ate readily . 
present work , bullough ( 1949b ) stated that changes in temperature within the range normally found indoors in this country had no noticeable effect on mitotic activitv in the skin of the ear . 
this anaplastic tumour grows readily in the strain of mouse used ; it has a high percentage of " takes , " and shows very little tendency to regress when once established . 
immediately after its removal the piece was trimmed all round in order to expose a raw edge which facilitated the penetration of the cold i per cent acetic acid solution in which it was at once immersed . 
after i to 2 hours in this solution ( the time depending on the size of the piece ) , it w ' as possible to slide the epithelium from both sides of the underlying connective tissues . 
after it had been covered with a similar piece of filter - paper the whole was moistened with fixative , compressed lightly between two coverslips held together with an elastic band , and immersed in fixative for at least an hour . the fixative used was a mixture of one part of glacial acetic acid with two parts of absolute alcohol ; exposure to this solul . - jon for several days did not greatly harm the cells , biit a period of not more than 24 hours gave optimal results . 
the " sandwich " was therefore removed intact from the coverslips , washed free from fixative in 33 per cent alcohol followed by water , and then soaked for a short time inn / 1 hci before it was replaced between the coverslipa and their rubber band . 
after about i hour the maximum degree of staining was reached , and a subsequent washing for a similar period in s02 water was needed to remove unchanged stain which would otherwise have become re - oxidized in the later treatment . 
changes in the mitotic activit qf ear epithelium in tumour - bearing m - ice . the results of three similar experiments which show the general effect of the growth of the tumour on the mitotic activity of the epidermal cells of the pinna are given in table i . 
the relation of the reduction in the mitotic activity of epidermal ce118 in tumoursince it is possible , as some authors have suggested , that systemic effects in persons or animals bearing tumours may be due more to depression of appetite and lowered food intake than to the direct competitive effect of the tumour itself , some experiments were performed to determine how far such indirect factors may be - the cause of the reduction in mitotic activity . 
since the tumours had reached about 10 per cent of the animal 's body weight at the time of death , the neoplastic tissue was resected before the final carcass weight was determined . from table ii it can be seen that even wlien the tumours had reached this lai - ge proportion of the body weight , the average carcass weight had not fallen from the time of implantation . 
although there was no sign of wasting in these tumour - bearing mice , and their behaviour continued to be typically active , the frequency of mitosis in the epidermal cells had fallen significantly . a further test of the inanition theory of reduction of mitosis lay in determining whetlier there was any correlation between the change in the weiglit of the mouse in the ' final 24 hours and the frequency of mitosis . 
since the mouse has a very higil food intake - 15 to 20 per cent of its body weight daily - any abst ' inence from eating is quickly revealed by a . 
in table iii the control and tumourbearing mic - e have been subdivided into two aroups on the basis of change of weight in the preceding 24 hours , and the mean number of mitoses per i 00 fields of the ear epidermis recorded . 
these general findings are in conformity with those of sherman , morton and mider ( i 9 , 50 ) , who observed that in tumour - bearing rats the nitrogen required for the nutrition of the tumour was derived from the diet until the growth reached about 10 per cent of the liost 's body weight , and that it was only after this proportion had been exceeded that this requirement was obtained at the expense of wasting of the body tissues . 
it is difficult , consequently , to attribute the decreased rate of multiplication of the epidermal cells in our mi - ce to any change ' comparable with ihe intoxication and cachexia often present in the later stages of neoplastic disease in man . an alternative explanatioii for our observations is that during the growth of such implanted . 
tumours nutrient substances essentia ' l for cell division may be diverted from normal to neoplastic cells to the detriment of the former . during periods of nutritional stress , such as severe malnutrition or pregnancy ( barcroft , 1946 ) , it is nowbelieved that a competition for circulating anabolites develops between cells , which be ' ars unequally on those of different types . 
should a coniparable contest for nutrients develop in neoplasia , the processes associated with the multiplication of ' normal cells might be amongst the first to reflect a deterioration in the metabolic state of the host . 
westlake avenue , l08angele8 , california . received for publication january 19 , 1951 . huggins , miller and jensen ( 1949 ) studied the thermocoagulability of the serum protein in health and disease in the presence of an extrinsic inhibitortheir results , however , while showing an abnormal behaviour iodoacetic acid . fo ' r mahgnant and certain non - mahgnant diseases , tend to establish a seeming relationship between cancer and tuberculosis . 
serum m micromoles of sodium iodoacetate in the nearest where 05 tube containing a firm clot preceding a tube in which the coagulum is a " shapeless viscous mass , .. 
or in the ori inal state before boiling . the serum protein determinations were carried out by the semi - micro kjeldahl procedure recommended by huggins , miller and jensen ( 1949 )  . every fifth determination was duplicated with an average agreement of 0 - 5 per cent . procedure was frequently checked for accuracy for the recovery of 5 - 0 mg . quantities of nitrogen by carrying out a complete determination with 23 - 6 mg . quantities of anhydrous ammonium sulfate with recovery in duplicate being 0 - 02 to 0 , 03 mg . 
the two myelomas were r - eceiving nitrogen mustards ; the leucaemias , x - rays and / or transfusions ; some of the advanced cases , polysaccharides or chymotrypsin ; eight of the breast cancer cases , testosterone . 
none of the patients in groups i and ii received any special diet , except that the most advanced , uncontrolled cases were getting either plasma transfusions or protein hydrolysates of one kind or another . all of them received an iron - vitamin preparation . 
for the series of cases in group iv merely reflects the ratio of concentration of iodoacetate as an inhibitor of coagulation for decreasing quantities of serum protein . there is no evidence that age distribution of the group tested played any significant role in the ratios obtained for the i.i. discussion analysis of the factors involved in the procedure showed that the coagulability of 52 per cent of the group i sera is abnormal for entirely different reasons from the sera ofgroups 11 and iii . 
evidence for this lack ofhomogeneity between the protein values and the degree of positive h.m.j. , obtained for tubercular sera and the sera from new untreated cancer soon became apparent , i.e. 
to the group i patients . in some the " positive " was altered to " negative , " andin there was good agreeothers the positive results became more or less positive . ment , however , for the i.i. 
values established by both kjeldahl and falhng - drop methods of protein estimations , for the remah - iing groups of cases . this led us to consider an " aberrant " or " combined - protein " as being responsible for the striking disagreement with the h.m.j. 
for the two types of disease . the possibihty that we were deahng with an increase in one of the normal fractions of the serum , the alpha globulins , reported to be increased in mahgnancy , led us to carry out the test on a sample of mucoprotein from cancerous serum , generously supphed by richard winzler , of the department of biochemistry , of the university of southem califomia , and a " bence jones " protein , isolated from the urine of one of the two myeloma cases in this series . 
neither ofthese substances yielded a positive i.i. if , as others have observed , the degree of increase of alpha globuhn is proportional to the severity of active tissue destruction , then apparently the alpha globulin plays no part in the huggins test , either for advanced tuberculosis , which certainly involves active tissue destruction , or in the early and new untreated cancer cases in our study . the question of the existence of modified serum protein molecules in various disease states , including mahgnancy , has been discussed recently by one of those whose published data estabhshed a close correlation between plasma viscosity , and the severity of the organic changes ( harkness , 1949 )  . 
added emphasis that we may be dealing with an altered protein in malignant tumours is given by the experimental observations ofhellwig ( 1949 ) , who found that as a rule the size ofspherical bodies in the form ofclusters , short - chains and aggregates from tumour extracts when examined by electron microscope was exceeffingly larger than that in benign or normal tissue . 
he concludes that these globules are not virus - like causative agents of cancer , but rather globular proteins , probable aggregates of the cytoplasmic globules due to an alteration in the cohoidal state of the cancer it is quite possible that this cytoplasmic material may be introduced into cell . the blood serum and may play a role in accounting for the positive i.i. 
duboff subjective element in the estiniation of the coaguluthe task for the future is the elimination of this factor , perhaps , by measuring the degree of coagulation by an appropriate electronic procedure characterized by the electrical resistance or potential of the coagulum . can one explain the paradox of the 22 negative h.m.j. 
tests have a pattern of deformation in one direction , it is not inconceivable that the former 22 cases have - a pattern of deformation in another direction that is not manifested in the test through the present combination ofreagents . 
furthermore , if the mechanism of action of this method is due to the increase of net negative charges on the protein molecule by the addition of sodium iodoacetate , then our results strongly suggest variations in the polar character of the proteiii molecule in the serum of certain phases of tumour development . the magnitude of relationship between absolute protein per cent and the ll demonstrated by group iii serum does not reflect the magnitude of the effect , when apphed to group i . 
the term " false positive " cannot be apphed ' there - t fore , to such tuberculosis sera , in the same sense as the term " positive " is applied to that of early cancerous sera , since the term " positive " itself is not tenableon the same basis . 
the serum of individuals undergoing some type of degenerative process , appears to possess an admixture of some elements , the source of which we do not yet comprehend , but the presence of which has been demonstrated by measurable function of the thermocoagulation of protein in the presence of an extrinsic inhibitor , iodoacetate . tentatively , we are inclined toward the conclusiozi that abnormality in the blood serum of some cancer patients , unhke that of some tuberculosis blood with a corresponding i.i. 
it is suggested that the use of the expression " false positive " or " pseudo positive " be elimiiaated from the terminology of cancer tests . the ' author wishes to tender his sincere thanks to clyde k . 
blackburn. from the department of haematology , the royal infirmary and ho8pital , sheffield . received for publication april 3 , 1954 . the forowing considerations led us to carry out a trial of stilboestrol in acute it is well know - n that the endocrine organs play an important part leukaemia . in the regulation of haemopoiesis , and many workers have reported the beneficial unfortunately , effects of acth and cortisone in some cases of this disease . however , remissions so induced are usuary only of short duration . re - treatment may again have a beneficl ' al effect , but eventually a refractory state is reached . on the other hand , " myelokentric " and " lymphokentric " acids , steroid - like principles extracted from urine ( afiller and turner , 1943 ) and from serum ( foster and miller , 1950 ) cause leukaemoid effects of myeloid and of lymphatic type furthermore , myelokentric respectively when injected into normal animals . acid has induced partial remissions in human cases of lymphoblastic leukaemia in the hands of miller , herbutt and jones ( 1947 )  . 
hence hormonal imbalance may play a part in the aetiology of leukaemia . finkelstein , gordon and charipper ( 1944 ) demonstrated that oestrogens have a depressant effect on the bone - marrow in certain conditions , but they did not study leukaemic states . burrows and horning ( 1952 ) have shown that not only are oestrogens careinoaenic , but they may be careinostatic , often restraining and causing regression of some human neoplasms such as carcinomata of the breast and prostate . 
they also state that the liabihty of mice to leucosis can be increased by oestrogens and reduced by androgens . furth ( 1952 ) , however , reminds us that in most strains of mice loukaemia is more common in the female , but in man it is more it is possible , therefore , that in human leukaemia oestrogens common in males . may have the opposite effect to that in niiee . dausset and schwarzman ( 1951 ) reported a study of 212 cases of acute leukaemia witb , regard to the influence of age and sex upon the frequency and cytological types . 
they also reviewed other series in the literature from these points of view , including both acute and chronic leukaemia . these authors state that between 18 and 50 years in both males and females there is an overwhelrning preponderance of myeloid leukaemia , while under the age of 18 and over the age of 50 lymphoid leukaemia occurs almost exclusively . 
as the former occurs most commonly during the period of maximal procreative activity , they suggest that there may be an endocrine effect on the lymphatic - mye - loid equilibrium , especially with regard to the sex hormones . stilb ' oestrol appears to have had a beneficial effect in single cases of chronic myeloid leukaemia ( loeper , lesourd and sterboul , 1947 ) and of chronic lymphatic leukaemia ( lemaire , loeper , housset and koupernik , 1947 )  . 
on admission to hospital in sheffield he was given 3 pints of packed cells and stilboestrol and penicillin therapy were begun . this was followed by an excellent clinical remission for 6 weeks , with complete disappearance of clinical splenomegaly and hepatomegaly , the latter organs having been palpable 2 below the respective costal margins at the commencement of treatment . 
no complete remissions occurred , but 3 patients had transient partial remissions . there is no evidence from this series to suggest that either the prognosis or the clinical course of acute leukaemia is altered by adding stilboestrol to other therapy . i am indebted to my medical and surgical colleagues in sheffield , to r . 
peacock. froni the research department , glavotr royal cancer hospital . received for publication april 6 , 1949 . it is a remark - able fact that while carcinogenic hydrocarbons readily , induce sarcoma in the connective tissues of fowls , the same agents have not vet been shown to induce epithehal tumours in this species . indeed until recentlv all attempts to induce epithelial tumours in fowls by any means seem to have f.iled. recently gottschalk ( 1948 ) mentioned iin uccessful attempts to induce hepatoma in 89 fowls fed with " massive " doses of p - dimethylaminoazobenzene ( da - ab ) , and maintained for over a year on a diet deficient in protein and riboflavine or enriched with biothe also quoted similar iin uccessu attempts to induce hepatoma with butter yerow by kinosita ( i940 ) , and other failures to induce epithelial tumours in general with various carcinogens . 
one case of hepatoma was observed by ober , guerin and boic ( 1933 ) in a bird inoculated 9 months previously with a mtrate of 3fill hill 2 endothelioma . this hepatoma was not transmissible , but birds grafted with fragments of hepatoma developed leucosis which was transmissible . 
the aetiolo&y of this hepatoma therefore is uncertain.induced epithehal tumours were amongst the teratomas obtained by michalowsky ( i 929 ) following the injection of 5 per cent zinc chloride into the testicles of cocks . duran - reynals ( 1946 ) , while trying to transmit primitive renal tumours in fowls , obtained sarcomas but no epithelial tumours in the inoculated birds . it may be that other workers have made extensive negative tests without them , but it seenis advisable to describe our ow - n mainlv negative recor attempts , which have now extended over a period of about 17 years , and have 3ielded only two carcinomas , apparently caused by 2 - acetylaminofluorene ( 2 - a - a - f )  . in contrast with these negative results , bielchowsky and green ( i945 ) obtained an anaplastic renal carcinoma in i of 5 rhode island red cocks maintained on a mixed diet to which was added 2aaf , at the rate of 3 - 30 mg . 
149 , previously recorded as bearing a tumour , was found to have a necrobiotic lesion in the region of the eneysted tar and a large haematoma in the breast muscle , but no sarcoma . ( 2 ) twenty - seven bpr fowls ' were painted on the right side of the comb witli tar and injected in the right breast muscle with the same sample of tar . while these experiments were running the first recognition of a pure hydrocarbon , 1 : 2 : 5 : 6 - dibenzanthracene ( db ) , as a carcinogen was reported by kennaway and hieger ( i 930 ) , and thereafter when the substance became available these birds were painted with a saturated solution of db in chloroform instead of tar . in view of the lack of obvious reaction to the previous tar painting , light cautery of the comb with a hot platinum wire was applied to survivors immediately before painting with db . 
pellet of 3 : 4 : 5 : 6dibenzearbazole ( dbc ) implanted into the right preening gland , followed by twice - weekly painting of the preening gland area with 0 - 1 per cent solution of croton oil in acetone . 
no tumours occurred in other birds in this experiment . ( 8 ) in preliminary experiments , 7 bl fowls were injected into the preeiiing gland with solutions of dmb in arachis oil . 
the fluorescent solution was expelled through the duct of the preening gland and , as there was no evidence of retention in the gland cavity after a few days , this type of experiment was abandoned . implants into the preening glands . tllree groups of 6 bl hens had the following pellets iniplanted into the left preening gland : 15 - 30 mg . 
the other birds had ar been implanted with similar perets of methylcholanthrene , n : n - dimethylami ioswbene , or 1 : 2 : 5 : 6 - dibenzanthracene into the right preening gland , without obvious effect . of the remaining 6 survivors after 17 months , 2 had palpable nodules in the wah of the crop . 
one of these , a bl hen , was kffled because it was rapidly losing weight and was found to have several ulcers in the crop varying in diameter from about i to 8 mm . , and partly covered by tenaceous slough . there were also numerous oily cysts in the connective tissues around the crop and in the muscular and submucous tissues of the crop itself representing renmant - 8 of previous injections of 2aaf in arachis oil . 
the re ndaer of the alimentarv tract was thoroughly examined but no other lesions were found . the hver and spleen were smafl and paler than normal but showed no locahzed lesions . 
the ovary was in a resting stage and the oviduct was involuted . sections of the ulcers in the crop show that it was the seat of at least 3 apparently separate squamous carcinomass . 
the low incidence of carcinoma in fowls n - iight be explained on these grounds . on the other hand , mammals differ in their susceptibility to the actioli of carcinogens . 
a case of keratinizing squamous carcinoma of the buccal mucosa in a fowl was described and well ifustrated bv puente - duany ( 1932 )  . the orilv case of spontaneous squamous carcinoma se ' en by us in over 3000 post - mortem examinations of fowls , over a period of 20 years , occurred in a bpr fowl that had been unsuccessfully graftedwith fragments firom a chemicauyinduced sarcoma . 
the absence of sebaceous follicles in fowls and the concentration of the sebaceous glands in the paired preening gland prompted us to implant potent carcinogens into the cavity of these glands . 
1. received for publication february 23 , 1948 . in a previous communication we reported that a strain of the shope rabbit papilloma had been transmitted for 10 serial passages in the domestic rabbit ( selbie and robinson , 1947 )  . 
the adaptation of this tumour virus as a transmissible infection in domestic rabbits occurred during experiments in which the simultaneous inoculation of shope papilloma virus and sheep dermatitis virus in domestic rabbits produced papillomas that proved infective to other rabbits ( selbie , 1946 )  . 
the further passage of this virus in domestic rabbits was materially helped by continuing the procedure of mixing a second virus suspension with the infective inoculum of papilloma virus , and also by treating the skin with croton oil before inoculation , but there was no evidence of an increase in the virulence of the virus suspensions during passage . in the present communication we shall show that carcinomatous transformation has occurred regularly in this transmissible papillomatosis , and in a mamner similar to that found in the non - infective papillomatosis that is produced in domestic rabbits by the inoculation of extracts of papillomas from the cotton - tail rabbit , the original host of the shope papilloma virus . 
thus in all rabbits frqm passage 4 in table i , area 1 represents normal skin inoculated with a 10 per cent extract of papillomas , area 2 , normal skin inoculated with a mixed extract of papillomas and sheep dermatitis lesions , area 3 , skin pre - treated with croton oil and inoculated with a 10 per cent extract of papillomas , and area 4 , skin pre - treated with croton oil and inoculated with the mixed virus suspensions . rabbit 2 , passage 2 was inoculated with papilloma extract on normal skin only , and in rabbit 4 , passage 3 , the procedures for areas 1 and 3 were omitted . the rabbits were examined at weekly intervals from the 7th week onwards . the tumours were charted and their size was measured by callipers at regular intervals . 
as was noted in the earlier communication ( selbie and robinson , 1947 ) , there was a tendency for individual papillomas to unite during development , and in some instances papillomas regressed completely . 
hence in this communication only those papillomas that were recognizable as single entities at 6 months in areas with confluent or semi - confluent papillomatosis will be considered . only a few papillomas could be distinguished as independent entities at 6 months , and no accurate count could be made , so that a fair estimate was given of 30 papillomas for confluent papillomatosis and 20 for semi - confluent papillomatosis . it became apparent early in this investigation that if the development of individual papillomas was to be studied over a prolonged period , cancers which arose in adjoining papillomas should be removed . 
1 are shown the times at which carcinomatous growths were first detected in passages 2 to 7 , passage 9 being omitted because the surviving rabbits have been observed for only 40 weeks after inoculation . it will be seen that the passage rabbit 2 __ to ~~ * : 6s weeks after inoculation fig . 
1. - times of observations of carcinomas in all rabbits from the 2nd to the 7th passage . each rabbit is represented by a line indicating the period of observation from the 40th week blocked circles indicate carcinomas arising from papillomas on skin treated onwards . with croton oil before inoculation , and open circles indicate carcinomas arising from papillomas on untreated skin . x = removal by operation of all remaining papillomas . 
the time at which glandular metastases were observed varied with the time at which the primary carcinomatous growth occurred , the limits being 33 weeks after inoculation in rabbit 2 , passage 9 , and 89 weeks in rabbit 2 , passage 2 , while the average time was 67 weeks for all the rabbits in the series . 
to draw any definite conclusions from this series concerning the incidence of glandular metastases as many of the primary growths were removed , and in consequence the opportunity for metastases to occur was reduced . 
2 , area 2 , the central papilloma with a concurrent thickening of the base . had slowly enlarged from the time of its original appearance to attain a diameter nine weeks later it measured 1 * 8 cin diameter and of 1 - 4 cat 53 weeks . the base had now thickened and was fleshy in appearance and consistency , in three weeks later , at 65 contras , t to the dry horny surface shown in fig . 
19. the secondary deposits in glands and lungs have all proved to be of the in many of squamous cell type showing varying degrees of differentiation . the lung metastases it can be seen that the infiltrating carcinoma cells form nodules within the alveolar spaces , so that the stroma of the deposit retains the architectural structure of the lung tissue . 
the time at which this change first occurs has tended to become shorter in successive passages , and has been reduced to 45 and 28 weeks in single rabbits of the 7th and 9th passages respecthis may indicate an increase in the virulence of the virus , but it is more tively . likely to be due to variations in the sensitivity of the rabbits . it has also been shown that the first occurrence of carcinomatous transformation in a rabbit is usually followed by others up to at least 5 in number and up to 85 weeks after indeed carcinomatous transformation occurs so regularly in this inoculation . transmissible infection that it would appear that all papillomas would show this change , provided that their evolution was not interrupted by the death of the host or by other factors such as spontaneous regression , infiltration from nearbv carcinomatous growth , or operative removal . carcinomatous transformation should then be regarded as a natural stage in the development of infective papillomatosis , and attributable only to the activity of the virus which initiates the infection . it is also clear from the work of kidd and rous ( 1938a , 1938b ) and mcintosh and selbie ( 1940 ) , who observed rapid transformation to malignancy in tar - induced papillomas infected with shope papilloma virus , that this virus is capable of causing immediate carcinomatous change . it is not therefore necessary to postulate an extraneous precipitating factor such as bacterial infection or an alteration in the virus itself to account for the change to malignancy , as suggested by rous , beard and kidd ( 1936 )  . although carcinomatous transformation would appear to be a natural stage in the development of this infection , it presents such a radical change in behaviour that it is difficult to see how it could be part of a continuous process . 
robinson cidence of tar tumours in mouse skin was increased at the site of injury by deep incision , numerous investigators have demonstrated the enhancing effect of unspecific irritation on the tumour - producing activity of carcinogenic substances . that chemical agents can also have this stimulating effect was shown by twort and twort ( 1928 ) , who accelerated the production of tar tumours in mice by pretreatment with oleic acid , and by berenblum ( 1941a , 1941b ) , who obtained a higher proportion of mice with tumours after painting with a dilute solution of benzpyrene by concurrent treatment with croton oil or by applying croton oil after a limited course of benzpyrene treatment . 
the possibility then had to be considered whether the hereditary condition acted through genetically transmitted differences in ovarian functional activity , or through an unequal response of mammary glands or genital tract to ovarian hormone . 
numerous and extensive observations were made with somewhat conflicting results , both on the nature of the oestrous cycle and on variations in organ sensitivity to hormonal stimulation , in strains of mice with differing mammary cancer incidence . when the existence of the third factor , i.e. 
the alveolar epithelium in this particular graft actually shows the various stages in the secretory cycle of the normal prostatic gland . it is interesting to compare the histology of these successfully vascularised grafts seen in fig . 
horning the prostatic it is relatively easy to detect by palpation non - vascularised grafts , as they are smaller and invariably softer when compared with successfully vascularised prostatic grafts , which are firmer on palpation , larger and invariably cystic in the earlier phases of growth , owing to active secretion of the glandular epithelium . non - vascularised graft fixed5fig . 
in this particular implant this was the only malignant focus within the entire graft . alveoli distended with secretion and with normal epithelium are seen adjacent to this exhausted alveolus from which this early malignant lesion arose . 
the proliferating epithelial components in all the early malignant foci break through the alveolar basement membrane , invariably forming tongue - like lesions which rapidly invade the fibromuscular stroma of the host as depicted in all prostatic grafts which have grown after treatment with 20in fig . 
10. methylcholanthrene , it was found possible to distinguish between three distinct types of early epithelial growth , all of which have been previously described in detail ( horning , 1949 )  . by studying the cytology and mode of growth in serial sections of these early invasive foci through later phases of development in other similar older grafts , it has been possible to predict the types of tumours which would have subsethere is one type which gives rise to a glandular carcinoma , quently arisen . both these types of and a second which develops into a squamous growth . lesions are easily recognised by their histological character , and both arise from the alveolar epithelium . the third type is the most uncommon variety , characterised by a stratified squamous metaplasia of the epithelium in sita , followed by a diffuse marginal growth into the stroma , which clearly arises from the duct occasionally some grafts show two or sometimes three types of epithelium . proliferating foci within the same implant . 
11. this shows a section of a graft treated with crystals of stilboestrol alone and fixed 4weeks after implantation . there is a complete inhibition of secretion after this period of grafting . every individual alveolus within the graft was entirely devoid of prostatic secretion , and the epithelial cells had undergone marked morphological changes . 
the prostatic epithelium at this period of treatment contrasts greatly with similar grafts treated with the female sex hormone after implantation in host mice for the same period of time . 
the alveolar epithelium not only maintains its glandular character , but in the majority of grafts testosterone propionate induces a pronounced stimulation of the prostatic secretions , invariably resulting in a cvstic dilatation of the alveoli . 
grafts combined with the carcinogen and sex hormones . 20 - methylcholanthrene and testosterone propionate . - three squamous - celled carcinomas developed from prostatic grafts impregnated with the carcinogen and the male sex hormone in strain a mice at intervals ranging from 7 to 9 weeks following implantation . one sarcoma arose in a c3h mouse after 8 weeks ( table i , group iii )  . 
the differences in histological structure between prostatic tumours derived from grafts treated with the carcinogen together with either the male or female sex hormone can best be appreciated by comparing fig . 
examination of pituitary and adrenal glands and gonads from host mice bearing grafts . examination of pituitaries from mice bearing grafts from all three groups of rodents treated either with the carcinogen alone or in combination with either of the sex hormones revealed no abnormal histological changes , with the exception of excessive amounts of colloid seen in the clefts of pituitaries from mice treated with stilboestrol and the carcinogen . there was no diminution of acidophiles or increase in chromophobe cells following implantation of the stilboestroltreated grafts . neither did the adrenal cortex reveal any histological abnormalities resulting from this treatment . 
horning of both lung and prostatic tissues have been previously described by the author in mice the survival of an homologous graft seems to be dependent ( 1949 , 1952 )  . upon the use of a closely inbred strain , since stock mice of indeterminate ancestry do not easily tolerate grafts of this kind . 
pan and gardner ( 1948 ) found an increased susceptibility to tumour formation from grafted uterine epithelium in pure line mice as compared with hybrids . recent experiments ( horning , 1952 ) have further indicated that the age of the donor providing the graft , and the age of the host mouse into which the grafts are implanted , also have an important bearing on the problem of graft other factors such as the reaction beween the graft and the host survival . mouse play an important role . it has been previously reported that more difficulty has been experienced in obtaining malignant tumours from lung grafts impregnated with 20 - methylcholanthrene than with similar grafts of other it was interesting to note that tissues which are normally under hormonal tissues . influence are much better tolerated as grafts in host mice of the same sex and strain than tissues which are to a greater extent ( such as the lung ) independent of hormone action ( horning , 1952 )  . nevertheless , a certain number of prostatic grafts , when implanted subcutaneously into host mice of the same strain as those of the donor , fail to survive irrespective as to whether the grafts were impregnated either with the carcinogen alone , or in combination with either the male or female sex hormone . 
the present experiments on the reaction between the implanted prostatic graft and the host bearing mouse have shown conclusively that the survival of the donor graft is dependent upon a rapid vascularisation within the subcutaneous tissues of the host mouse . 
the reason , however , why some grafts fail to become vascularised still remains obscure . the influence of steroid hormones on the behaviour and growth of prostatic cancer has been the subject of intensive investigation . 
1. - the skin of a c3h male mouse is cut and pinned back so as to expose an untreated homologous prostatic graft which had been growing subcutaneously for 6 weeks . 
6. - transverse section through an homologous prostatic graft which failed to become vascularised , fixed 6j weeks after subcutaneous implantation . the relationship of the grafted prostate to that of the skin of the host rodent is clearly shown . 
horning alveoli have completely broken down ; there is also evidence of lymphatic infiltration . the whole graft has been encapsulated and is slowly being absorbed by the tissues of the host mouse . 
 it has been found ( elson and lamerton , 1949 ) that the protein content of the diet has a profound influence on the response of the , valk.er rat carcinoma 256 to x - radiation . 
two effects were considered to be concerned in this response : ( a ) the initial inhibition of tumour growth and ( b ) the elimination of the inhibited tumour and cure of the animal . 
 although variations occur within a group of animals maintained on a standard diet of fixed composition , the general type of response to a suitably fractionated in animals maintained on the 5 per x - ray treatment is illustrated in fig . 
growth may be nearly stopped for a consider able time , but the tumour usually begins to grow again , at first slowly in animals maintained on a 20 and then more rapidly , finally causing death . 
the rate at which it decreases in size is at first fairly rapid , but gradually becomes slower , and in many cases the animal is then able to rid itself entirely of the tumour by a " shelling out " process or sometimes by the gradual complete regression of the tumour . 
 a detailed histological and c : ytological examination of tumours , particularly under conditions presented by a and b , was therefore undertaken in an attempt to elucidate the part played by diet in influencing the ultimate response of these tumours to radiation . 
they were kept in individual cages , and maintained on the 20 per cent or the 5 per cent protein diet for at lea.st 7 * r - arch fellow of the xorwegian defence research establishment . 
15 c under these conditions the dosage rate at the centre of the tumour is about 140 r / m h~ tuhnique . - - cross sections of the implanted tumours were made by means of a special cutter with parallel kni , es giving a section of about 5 m thickness . 
 the conventional method of propagation of the walker carcinoma consists of the insertion of small pieces of tumour ( approximately 7 x 5 x 5 mm . ) under the skin of rats . 
although factors such as age , sex , weight , etc . , and general condition may account for some of this variation , it is probably mainly an expression of genotypic differences present in the colony from which the rats used in these experiments were drawn . 
 with our present routine for breeding and selection of animals for tumour implantation , when the tumours of a group of ten rats are measured 8 days after implantation the measurements show a distribution of i or 2 large tumours , about 5 medium - sized tumours and the rest considerably smaller . 
that this is largely the result of genetical variation is shown by comparison of the growth rates of tumours in litter mates and by implantation of similar sized pieces of tumour in both flanks of the same animal . 
the animals were divided into 4 groups , each group consisting of 4 litter mates , 2 male and 2 female ; they were killed 14 days after implantation and the weights of their tumours recorded . 
it is seen that the 3 most rapidly growing and largest tumours ( over 35 g . ) all occurred in group 1 , whilst in group 3 none of the tumours grew well . 
the growth rates of both tum , ours were remarkably similar , and if a tumour implant in one flank failed to grow the corresponding tumour in the opposite flank also failed . 
the average daily weight increase of rat.s maintained on our 20 per cent protein diet is about 3 to 4 : g . , whilst that of those maintained on our 5 per cent protein diet is less than 05 g . 
 weight of tumours 14 : days after implantation taken from 85 animals maintained on the 20 per cent protein diet was 24 : g . , whilst that of 86 animals maintained on the 5 per cent protein diet was 20 g . 
thus the ratio between the tumour weight.s on 20 and on 5 per cent protein diet is 12 , and the average growth rate of tumours is only about 20 per cent higher in anima1s maintained on high prot.ein than in those receiving a low protein diet . 
la.merton for comparison of the histology of tumour grafts in animals maintained on high and low protiein diets transverse sections were made through the tumour implants and their surrounding tissue 4 , 7 , 8 , 10 and 15 days after implantation . 
 it was found that 4 days after grafting the int , ensity of the inflammatory reaction as estimated by the number of cells of the reticulo - endothelium accumulated around the graft was great.er in rats maintained on the 5 per cent than in those on the 20 per cent prot , ein diet . 
on the other hand , the capsule of connective tissue was much more distinct in rats on the 20 per cent than on the 5 per cent prot , ein diet . 
the boundary of the tumour is well defined in rats on the 20 per cent prot , ein diei , the migration of tumour cells is negligible and the tumour grows by the very high rat.a of cell proliferation at the periphery of the tumour parenchyma . 
on the 5 per cent prot , ein diet , how ever , there is no definit , e tumour boundary and many isolated tumour cells can be seen scatt , ered amongst the loose , primitive network of connective tissue , which included in this " incomplet , e " capsule are also many surrounds the tumour . 
 during the early stages of the " take " and growth of the implanted tumours the reactions of the surrounding tissues may be very complex and int , erpretation of the exact course of events is difficult , but in older tumours the histological features of the process are much more clearly defined . 
the cell - elements ofthe capsule undergo progressive : fibrous differentiation , which can be clearly seen in high prot , ein diet rats with 10 to 15 - days - old tumours . 
the : fibrous nature of the capsule is much less obvious in animals maintained on a low prot , ein diet , and its clear demarcation is obscured by the migrating tumour cells . 
 it should be emphasized that on both diets there may be a considerable variation in the " take " of the graft and in the spread of the implanted tumour in the " host , and instances have occasionally been encount , ered in which the tumour graft took and grew more rapidly in animals maintained on low than in those fed on high prot , ein diet . 
such cases were , however , rare , and the effect of the diet is so marked that the differences in capsule - formation and organization between animals maintained on high and low prot , eins diets can easily be det , ected in most cases . 
 in the study of the reaction of the host rat to the implantation of tumour grafts the fact that , the tumour graft is itself growing may very often obscure the observations of the organization of the newly formed connective tissue capsule . 
 it was felt that the introduction into the subcutaneous tissues of a " passive " non - growing hetierologous tissue fragment such as muscle inst , ead of the " active " tumour fragment , would make it easier to analyse the influence of environmental factors , etc . , on the host reaction . 
 pieces of muscle of about the sam~ size as the usual tumour implants , taken from the leg of a second rat were implanted under the skin of the host animal . 
 305 in the mbsequent reaction to this muscle implant two phases could be clearly distinguished : ( a ) the inflammatory tissue response , ( b ) the formation of a capsule around the implant . 
 the in : oammatory reaction ( a ) is intense 3 days after implantation in rats receiving either the 20 per cent or 5 per cent protein diet , but in those main tained on the 20 per cent protein diet it rapidly subsides and has almost dis appeared 5 days after grafting . 
 the 5 per cent protein diet rats , however , still show persistence of the inflam matory reaction at a time when the capsule is already well developed in 20 per cent protein diet animals . 
it appears that the prolonged persistence of the inflammatory reaction around the implant is related to the absence of the connective tissue capsu1e , the development of which is impaired or delayed in animals maintained on a diet deficient in prote the evidence derived from the histological investigation of muscle implants thus supports the conclusion reached from the tumour implant experiments that while maintenence of th~ animals on a low protein diet has no deleterious influence on the inflammatory reaction to the implant , it does interfere to a very large extent with the organization and development of the connective tissue capsule . 
 a quantitative analysis of radiation - induced injuries in cells of the walker carcinoma is difficult owing to the large number of chromosomes ( 2n = 40 ) in the relatively small tumour cell . 
 injuries to the chromosomes can be detected only in ana - telc : , phase during which the lagging of ' " acentric " chromosome fragments ( segments without the centromere ) can be seen . 
13. - dividing tumour cell in late anaphase with three acentric fragments , one lying out of focus , 6 hours after 300 r , 5 per cent protein diet . 
27. - the same tumour ( l . ) , showing the active tumour cell island which lies beyond the periphery of the tumour which occupies the bottom right hand corner . 
28. - the same tumour ( l . ) at a higher magnification to show that tumour cells which were scattered in the loose connective tissue capsule form foci of renewed activity after irradiation . 
 a comparison has been made of the frequency of tumour cells with various cytological abnormalities , such as chromosome fragments , bridges and micro nuclei at different times after irradiation of a six - day old walker tumour in rats kept on high and low protein diets . 
the data obtained ( table i ) do not represent the full extent of the radiation injury resulting from any particular treat ment , since an unknown proportion of injuries undergo restitution before the cytological examination is made and are thus lost for analysis . 
moreover , the acentric chromosome fragments can only be seen when they lie freely in the cytoplasm , and consequently those fragments which are mixed up with the normal chromosomes and moved to the pole escape detection . 
a similar difficulty arises when we attempt to estimate the true extent of the radiation injury to cells by the number of micro nuclei , since some of the chromosome fragments may be included in the daughter nuclei and some of the micronuclei can contain more than one fragment . 
on the assumption , however , that the chance for such events is the same in all the samples , it is justifiable to use the quantitative differences shown by the data as a basis for comparing differences in cell behaviour which may be induced by maintaining the animals on different diets . 
 the data of table i shows that the greatest amount of injury was found in tumour samples taken 12 hours after irradiation , suggesting that these samples contained cells which were , at the time of irradiation in the most sensitive period of the mitotic cycje . 
it is inferred on experimental evidence , derived from x - rayed pollen grains and root - tips cells ( darlington and lacour , 1945 ) that the most sensitive period coincides with the duplication of the chromosome filament , which process marks the beginning of prophase . 
since the injury in the cells is at a maximum at 12 hours after both 100 and 300 r , we may conclude that the duration of mitotic suppression does not differ over this range of dosage . 
 the number of cells with chromosome injuries and with micronuclei was found to be already quite high in the 6 hours ' sample , suggesting that the time interval between treatment and the first appearance of chromosome fragments may be shorter than 6 hours . 
therefore some rats were killed 4 hours after treatment , but although both chromosome fragments and bridges were observed in this early sample , their frequency could not be estimated because the so - called " physiological " effects of radiation grossly interfered with the analysis ( mar quardt , 1938 ; koller , 1943 )  . 
l. - uierton the number of resting cells with micronuclei increases up to 24 hours after treatment , but at 72 hours such cells have almost disappeared from the tumour . 
 comparison of the results obtained at different times after irradiation with both 100 rand 300 r ( table i ) , in all samples except those taken after 12 hours , shows no significant difference in the number of cells injured or the number of chromosome fragments per cell , between animals maintained on high or low protein diets . 
 the inconsistent behaviour observed in the 12 - hour samples may be related to the fact that all the mitotic cells in this sample represent those cells which were in their most sensitive stat , e when irradiated . 
it was , therefore , felt that the results obtained with the 12 - hour samples could not be relied upon and should be disregarded in view of the consistent results obtained with all the other samples . 
it is thus possible to compare the length of the inter - mitotic period on the two diets in order to find whether the duration of the mitotic cvcle is altered bv the diet or not . 
 the greatest amount of injury are those which at the time of irradiation were at in the x - rayed \\ ' alker carcinoma the the beginning of prophase of mitosis . 
 greatest amount of injury is found in the - 12 - hour sample and consequently the duration of mitosis from prophase to the end of telophase cannot be longer than 12 hours ; the cycle of the second division ( from prophase to telophase ) would occupy another 12 hours , thus lea , ing 20 hours for the duration of the inter mitotic period , if an allowance of 4 hours is made for the time lost by the radiation induced mitotic suppression . 
thus we may conclude that the active cells in the \\ ' alker carcinoma have a mitotic cycle of the order of 32 hours ( 20 hours spent in resting and 12 hours in mit - 0sis ) : this agrees with data obtained in similar experi ments in which irradiation is replaced by radiomimetic chemicals , such as the nitrogen mustards ( koller , unpublished communication )  . 
 from the observations of the frequency of cells in second mitosis 48 and 72 hours after irradiation with 100 or 300 r there was no indication that diet affects the duration of the mitotic cycle . 
at 6 days after the radiation treatment tissue fibrosis was much more developed , and the connective tissue capsule could be clearly distinguished from the actual tumour , since no tumour cells were present in this capsule zone . 
 it does , however , contain islands of active tumour cells , which , since the growth - inhibiting effect of a single dose of 1000 r is usually only temporary , no doubt represent centres from which the renewed growth of the tumour develops . 
 in the animals receiving the 5 per cent protein diet , the loosely organized con nective tissue capsule , 3 days after 1000 r , was not undergoing fibrosis to the same extent as the capsule in the 20 per cent protein diet animals . 
 six days after irradiation the tumour boundary which was previously very ill defi.ned , becomes more distinct , presumably owing to the fact that some of those tumour cells which were scattered in the connective tissue network and have survived the radiation treatment , have now undergone proliferation and brought about the formation of a new continuous tumour parenchyma . 
 w ' hile a single dose of 1000 r may cause considerable inhibition of growth of the walker rat carcinoma , and the inhibition may last for several days , complete regression of the tumour rarely occurs . 
the experiments with the single dose have shown , however , that at least in the 20 per cent protein diet animals , whilst the extent and rate of histological changes induced in the capsule or tumour bed is very favourable , it is insufficient to enable the animal to effect a cure . 
it is obvious , therefore , that the amount of radiation injury in the tumour cells must be increased without at the same time adversely affecting the favourable tissue response . 
it was therefore decided to increase the dose to 4000 r , which is of the order employed in the radiotherapy of human cancer , and a suitable method of fractionation for applying this dose was devised based on observations of the response of tumour capsule and tumour bed obtained in the single dose experi ments . 
the method employed can be illustrated as follows : 1000 r 500 r , 500 r 500 r , 500 r 500 r 250 r 250 r , in which represents two consecutive days on which no treatment was given . 
lamerton for the histological investigations 15 rats were treated with this fractionated dose , 7 of them being maintained on the 20 per cent and 8 on the 5 per cent protein diet . 
 two rats of each diet group h 1 , h ! ( high protein ) and l 1 , l 2 ( low protein ) were selected for histological examination ; of the remaining rats 4 out of the 5 maindied " 's e .. 
h 1 and h , indicate animals maintained on high protein diet and li and l , animals maintained on low protein diet at the time they were killed for histological examination . 
from similar results obtained in previous experiments ( elson and lamerton , 1949 ) and from a com parison of the growth curves of the tumours selected for histological investigation with those of the remainder of the groups shown in fig . 
22 it is reasonable to suppose that animals h 1 and h 2 on the high protein diet would have been cured , whereas li and l 2 maintained on the low protein diet would not . 
those of the high protein diet animals ( h1 and hz ) , however , had grown to a considerable maximum size and were then regressing , whilst those of the low protein diet animals ( l1 and lz ) had shown earlier retardation of growth , but were beginning to assume a more rapid growth rate . 
the animals h 1 and li had received a total dose of 3000 r ( in 5 fractions ) , whereas hz and lz had received the foll total dose of 4000 r ( in 8 fractions )  . 
 in assessing the response of tumours to radiation two effects must be con sidered : ( i ) the initial inhibition of tumour growth and ( 2 ) the elimination of the inhibited tumour and cure of the animal . 
in work with the walker rat carcinoma 256 it has previously been shown that the diet of the animal has a definite influence on each of these processes ( elson and lamerton , 1949 )  . 
 dealing first with process ( i ) , it has been shown that maintenance of the animal on a low protein diet favours the immediate growth inhibitory response of the implanted walker rat carcinoma 256 to radiation . 
it might be thought that this diet effect is related to an increased sensitivity of dividing tumour ce ] ls to radiation induced in some manner by the poor protein diet . 
furthermore , we do not feel that such differences as have been revealed in the course of the histological investigation of the tumour bed reported here offer any very satisfactory explanation of the greater immediat.e tumour response in the low protein diet animals , and we are inclined to believe that some more fundamental biochemical relation is involved . 
lamerton investigations with carcinogenic chemicals have suggest , ed that these sub stances may inhibit cellular growth by interfering with the normal processes of protein synthesis ( elson and warren , 1947 ; elson , 1949 )  . 
h this is the case it might be expected that animals in which the full capacity for protein synthesis is already restricted by a deficient protein diet would probably show an immediate growth inhibitory response of both animal and tumour to treatment . 
with ample protein to furnish more than suffi cient amino acid " building blocks ' for the full efficiency of protein synthesis would not be expected to show such an immediate reaction . 
it is not unlikely that x - radiation may act in a similar way and in order to throw more light on this problem the protein metabolism of irradiated animals maintained . 
 of the walker rat carcinoma a high protein diet has been shown to be of great assistance to the animal in the process of elimination of the inhibited tumour and the replacement of the tumour area by healthy tissue . 
that in the case of the implanted walker rat carcinoma 256 the main effect of the high protein diet is to ensure the development of a well organized . , extensive capsule of connective tissue around the growing tumour . 
response to radiation treat ment the ill - defined tissue capsule zone does not undergo fibrosis in the same way as does the firm capsule of the high protein diet animals . 
altho~h its main mass usually becomes necrotic , new tumour growth often develops in the incomplete capsule zone , from cells which have escaped the lethal action of the radiation . 
on a diet deficient in prote the effect of addition to the low protein diet of substances such as amino acids , particularly cystine and methionine , amino sugars , etc . , which may conceivably be involved . 
 313 taking into consideration the connective tissue reaction , devised treatment methods for epitheliomata , in which the total dose is of the order of 3000 r , far below the so - called " standard tumour lethal dose . " also it has been shown by jolles and koller ( 1950 ) that the tumour bed reaction can be influenced by a method of fractionation of the dose in space as well as time to give favourable therapeutic resu.jts. 
 the present animal experiments have shown that the character and organization of the tumour bed can be influenced by nutritional factors , and suggest that suitable regulation of nutritional conditions , such as , for instance , supplying a high protein diet , or supplementing the diet by protein hydrolysates , etc . , and by increasing protein anabolism by hormone administration , etc . , may jead to improvements in clinical response . 
 the effect of the protein content of the diet on the establishment and growth of implants of the walker rat carcinoma 256 , and on the response of this tumour to x - radiation , has been investigated . 
 the nature and extent of the inflammatory reaction has been found to be similar in animals maintained on both high ( 20 per cent ) and low ( 5 per cent ) protein diets , but in the low protein diet animals it persists for a longer period after implantation owing to slower and less complete development of the connec tive tissue capsule . 
 in assessing the response of the tumour to radiation two effects have been considered , ( a ) the initial inhibition of tumour growth , which is favoured by a low protein diet , and ( b ) the elimination of the inhibited tumour which is favoured by a high protein diet . 
 histological investigation has suggested that the favourable effect of a high protein diet on the elimination of the tumour is related to the development of the well organized capsule of connective tissue around the growing tumour . 
radia tion treatment , besides inhibiting division of the tumour cells , also increases the fibrosis in this capsu.je , which aids in the eventual elimination of the damaged tumour . 
 we wish to express our thanks for grants supporting this investigation from the british empire cancer campaign , the anna fuller fund , the jane coffin childs memorial fund for medical research and the u.s. 
may be important factors in the pathogenesis of cancer of deeply seated as well as of superficial organs indeed , early in the 19th century a careful local study of is hardly a new one . cancer deaths in verona was made by stern ( 1842 ) , the notion of cancer houses was looked into and fragmentary studies of cancer endemiology were made in the concept of cancer as a unitary disease switzerland , america and elsewhere . affecting organs rather at random has tended to discourage detailed research on site distributions . the general register office in london worked patiently upon the occupational aspects at successive census periods with increasing detail as death certification recently the danish cancer registry , initially of primary cancer sites improved . rather sceptical of some of the conclusions reached , has admitted that danish data tend to confirm them ( clemmesen , 1951 ) , and similar data have been pubin 1950 and 1951 the council for lished from the netherlands ( versluys , 1949 )  . co - ordination of international congresses of medical sciences arranged conferences on what was at first called " geographical pathology " , but has now become " endemiology " of cancer . very little has been written , however , on lung cancer from this aspect except with respect to tobacco , although it came under discussion at the first of the above - mentioned conferences ( c.c.i.c.m.s. , 1951 ; daff , doll and kennaway , 1951 )  . in the present paper the short term " lung cancer " is used to mean carcinoma and other malignant neoplasm of the bronchus , lung and pleura ; and when " mortality " is mentioned it is understood that whatever rate or index is used has been standardized for age . * the substance of this paper was communicated to the metropolitan brench of the society of medical officers of health on may 9 , 1952 , 100 p . 
at that time i still had to work upon the rates for 1921 - 30 , and failed to find any significant correlation either in the large towns or in the metropolitan boroughs between lung cancer mortality and the social class or overcrowding indices . recent research on correlation with tobacco smoking . between 1930 and 1946 the recorded rates in england and wales as a whole had been rising steadily , and to a surprising extent even when increasing use of x rays was considered . consequently the medical research council called a conference to advise whether any useful research could be undertaken to throw light on the causes . 
the result of that study was published in september , 1950 ( doll and hill , 1950 ) , and in my view it proved beyond doubt , in conjunction with american evidence of the same kind ( wynder and graham , 1950 ) that 102 p . 
stocks tobacco smoking is a very important factor in the causation of lung cancer . did not prove , however , that tobacco smoking is the only important factor in it has been suggested that the figures could mean that 90 per cent causation . of the lung cancer occurring in greater london is caused by tobacco ; but they do not necessarily mean that , and there are reasons for thinking that the proportion is - much lower , and that atmospheric pollution may be an additional factor . these reasons derive from some statistical facts not hitherto published . mortality in london in 1946 to 1949 . in the four years 1946 to 1949 the deaths of males attributed to lung cancer in in 1950 england and wales averaged 8183 annually , and of females 1774 . deaths of males exceeded 10 , 250 and those of females were just short of 2000 , and in 1951 the total reached 13 , 000 . 
the national rates at different ages are compared in table iv , which shows that at ages 35 - 45 the increase was 6 - fold , and at 55 - 75 it was more than 11 - fold . how much of this enormous increase has been due to more complete detection of the disease and how much to increased incidence we can only surmise . london county as a whole , allowing for age changes , male mortality increased about 8 - fold between the two periods ; and it is now about 60 per cent greater than in the country as a whole , and 21 times the rate for rural districts . 
1 shows the mortality distribution in 1946 - 49 . for 1921 - 30 there were two areas of specially high certified mortality , one in bermondsey , stepney , bethnal green , hackney and stoke newington , the other in hampstead , st . 
stocks wind direction as a possible factor . returning now to greater london , clark ( 1951 ) has shown that the logarithm of the population density per acre in successive zones diminishes in arithmetic progression on passing outwards from the business centre , and the same is true supposing domestic smoke to be an important factor in of other large cities . producing lung cancer , if there was no wind at all one would expect to find the highest incidence at the centre , diminishing in all directions outwards . if there is wind and it comes from all directions equally , a more diffused but still symmetrical distribution would be expected , with less contrast near the centre and more near the periphery . however , wind does not blow equally from all directions , and greenwich records over 12 - hour periods throughout the year 1950 show that the wind direction , when analysed into 8 sectors , was s.w. 
orr. from the department of experimental pathology and cancer research , medical school , university of leeds , and the de7partment of pathology , university of birmingham.. received for publication , april 23 , 1949 . the discovery of the milk factor or mammary tumour agent ( bittner , 1936 ) and the demonstration that three factors , namely , the genetic factor , the hormonal factor , and the milk factor , are essential for the development of spontaneous breast cancer in certain inbred strains of mice ( bittner , 1939 ) , was followed by investigations of the part played by the agent in the induction of breast cancer by oestrogenic hormone . 
lacassagne ( 1939a ) , lacassagne and danysz ( 1939 ) , twombly ( 1939 , 1940 ) , and later bittner ( 1940 , 1941 ) , gardner ( 1941a ) , shimnkin and andervont ( 1941 , 1942 ) , dmochowski and gye ( 19.44 ) , found that fosternursing of low - breast - cancer strain mice by high - breast - cancer strain females increases the incidence of breast cancer in the low - breast - cancer strain mice treated with oestrogenic hormones . 
tlhus male mice do not develop breast cancer , even if they are susceptible and have the mammary tumour agent , unless the hormonal or oestrogenic factor is supplied , and only few or no breast tumours are induced in low - breast - cancer strain mice , i.e. 
it is probable that a quantitative deficiency of any one factor can be overcome by a relative quantitative increase in the other two factors ( shimkin , 1945 )  . the accelerating influence of carcinogenic hydrocarbons on the appearance of breast cancer in mice of unmknow - n genetic constitution was first observed by maisin and coolen ( 1936 ) and perry and ginzton ( 1937 ) , while dobrovolskaiazavadskala and adamova ( 1938 , 1939 ) , were unable to observe a similar effect on inbred mice employed by theexperiments carried out by mider and morton ( 1939 ) , bonser and orr ( 1939 ) , strong and smith ( 1939 ) , bonser ( 1940 ) , strong and williams ( 1941 ) , engelbreth - holm ( 1941 ) , engelbreth - holm and lefevre ( 1941 ) , orr ( 1943 ) , kirschbaum , lawrason , kaplan and bittner ( 1944 ) , kirschbaum , williams and bittner ( 1946 ) , shimkin and bryan ( 1943 ) , strong ( 1945 ) , orr ( 1946 ) , demonstrated that carcinogenic hydrocarbons induce the appearance of breast cancer in females of low - cancer strains or accelerate the development of breast tumours in female mice of high - cancer strains . 
in these experiments it was also shown that oestrogenic influence is important in the induction of breast cancer by carcinogenic hydrocarbons , since mice developing these tumours in the absence of treatment with oestrogens were females , with one exception , a cba male ( orr , 1943 )  . 
the male mice of both strains , when 60 - 70 days old , were divided into three groups : mice of the first group received oestrone and methylcholanthrene , mice of the second group methylcholanthrene alone , and mice of the third group oestrone alone . 
c57 strain females , when 6 weeks old , were divided into two groups : mice of the first group were forcibly bred , mice of the second group were maintained as virgins ; both groups were treated with methylcholanthrene alone . oestrone was applied as a 0.02 per cent solution of keto - hydroxy - oestrone in alcohol , by painting the mice twice weekly for a period of 12 months . 
methylcholanthrene was administered according to the method described by orr ( 1946 )  . sixteen drops of 0 - 5 per cent solution in sweet almond oil were applied , at fortnightly intervals , to the skin of mice , four on each side of the dorsal and ventral surfaces of each animal . the c57 females of both groups received fortnightly applications of methylcholanthrene from the age of 6 weeks till death or the appearance of a tumour . in male mice the mammary gland is in a rudimentary state and they do not have nipples ( lacassagne , 1936 )  . 
administration of oestrogenic hormones leads to the progressive development of the mammary glands described in detail by turner and gomez ( 1934 ) , burrows ( 1935 , 1936 ) , gardner ( 1935 , 1939 , 1941b ) , lacassagne ( 1939b ) , loeb ( 1940 ) , loeb and suntzeff ( 1941 )  . 
because of these observations and the findings that breast cancer can be induced by methylcholanthrene in males treated simultaneously with oestrogens ( orr , 1943 ) , the c57 and c3h strain males were painted for 3 months with oestrone before the treatment with methylcholanthrene . 
after 3 months of painting with oestrone both the 057 and c3h males received their first application of methylcholanthrene which was then continued at fortnightly intervals until death or appearance of a tumour , except in the group of c3h males painted with oestrone which received only 14 applications of methylcholanthrene . 
two 057 males and one c57 female , which were treated with methylcholanthrene , developed general enlargement of lymphoid tissue , and in the c57 male which developed breast cancer a lymphosarcoma was found in the abdominal cavity . 
one c57 virgin female developed a spindle - celled sarcoma in the subcutaneous tissue . skin tumours were found in 10 out of 18 c57 males treated with methylcholanthrene alone and in 10 out of 35 c57 males treated with oestrone and methylcholanthrene . 
squamous metaplasia was observed in two tumours induced in 03h males by oestrone and .methylcholanthrene. the breast tumours induced in c57 mice , both male and female mice , showed a much greater degree of squamous metaplasia than the breast tumours induced in some of the induced tumours , as in the case of spontaneous in c3h male mice . tumours , variations in structure between different parts of the same tumour were found . 
sometimes the tumour cells were packed in solid sheets while elsewhere they occurred singly or - in small groups surrounded by an abundant stroma ; in some parts acinar structure could be clearly seen while in other parts it was lost entirely ; in places elongated cords of spindle - shaped tumour cells were found . 
thus the observations recorded by previous workers in this field were confirmed and the influence of hormonal factors on the development of carcinogen - induced breast cancer in mice shown . mammary tumours were also induced in c57 low - breast - cancer strain females , both breeding and non - breeding . 
orr results of other investigators . in mice , both males and females , which lack the mammary tumour agent . it is , therefore , possible to induce breast cancer in the present experiments breast cancer was induced in mice of a sub - line of c57 black low - breast - cancer strain which has a low susceptibility to spontaneous breast cancer . 
breast tumours developed in c57 black strain females , both breeding and non - breeding , after treatment with methylcholanthrene , and a c57 black strain male after combined treatment with oestrone and methylcholanthrene . it is not known whether the failure of kirschbaum , williams and bittner ( 1946 ) to induce breast cancer in breeding c57 black strain females with methylcholanthrene was due to the different method of application of methylcholanthrene or to differences in susceptibility of the two sub - lines of the c57 strano tumours were observed in either c3h or c57 black strain males treated with methylcholanthrene alone . this supports the findings of other workers that hormonal factors play a part in the development of tumours induced by methylcholanthrene . orr ( 1943 ) , however , reported the induction of breast cancer in one out of 16 cba low - breast - cancer strain males after intranasal administration of methylcholanthrene in the absence of treatment with oestrogen . 
he also obtained breast cancer in virgin mice of two low - breast - cancer strains ( if and cba ) after treatment with methylcholanthrene . in the present experiments tumours developed in two non - breeding c57 females treated with methylcholanthrene . mider and morton ( 1939 ) failed to induce breast cancer in non - breeding dba high - breast - cancer strain mice , while strong and smith ( 1939 ) , strong and williams ( 1941 ) and strong ( 1945 ) in their successful experiments on the induction of breast cancer in jk , nh and nho low - breast - cancer strain mice employed breeding females only . the present experiments confirm the findings of other workers that breast tumours can be induped in male mice of susceptible strains after treatment with oestrogenic hormones ( shimkin and andervont , 1941 , 1942 ; bittner , 1941 ; dmochowski and gye , 1944 ; bonser , 1944a , 1944b )  . the present findings also confirm the observation that mammary tumours develop in mice of resistant strains following treatment with methylcholanthrene . 
the c57 low - breastcancer strain mice of the sub - line used , when foster - nursed soon after their birth by riii high - breast - cancer strain females , develop an incidence of 11 per cent of breast tumours , but fail to develop breast cancer when given the tumour agent at the age of 4 - 6 weeks , even after large quantities of the agent and in spite of increased hormonal stimulation by repeated pregnancies ( dmochowski , thus mature mice of this strain though resistant to the mammary 1948 )  . tumour agent are susceptible to a different agent , i.e. 
methylcholanthrene. the treatment with oestrogenic hormones failed to induce breast cancer in c57 low - cancer strain males . this again confirms the previous findings ( twombly , 1939 , 1940 ; bittner , 1940 , 1941 ; shimkin and andervont , 1941 , 1942 ; dmochowski and gye , 1944 ) that an increased oestrogenic stimulation overcomes the threshold of lowor non - susceptibility and results in the development of breast tumours only in the presence of the mammary tumour agent . treatment with methylcholanthrene induced in c57 black low - cancer strain females , breast tumours which , although similar in their structure to spontaneous breast cancer of highand of low - breast - cancer strain mice , show an increased incidence of squamous metaplasia . 
1. received for publication january 21 , 1948 . surgery in the form of the so - called radical operation is in general at the present time the principal weapon in the treatment of carcinoma of the breast . what it can achieve and its limitations are now fairly well established . 
thus it is known that if a patient with carcinoma of the breast has microscopical invasion of the axillary glands , the strong probabilities are that the disease has passed beyond the local area and that the patient will sooner or later succumb it is to the disease , although there will be a minority of fortunate exceptions . also known that if the axillary glands are not invaded the chances that the patient will be cured of the disease are appreciably increased . 
the present article attempts to assess the comparative results of a personal series of cases in which various techniques of treatment were used . the technical surgical problem in carcinoma of the breast has been rendered clearer by modem work on lymphatic anatomy , and in particular by that of gray ( 1939 )  . this has shown , firstly , that the dermis is a plane rich in lvmphatics and hence a rich potential plane of spread of carcinoma , particularly if the growth has spread into or near the skin ; and secondly , that the deep fascia is a plane devoid of or very poor in lymphatics , and hence not an important potential plane of spread . the former fact suggests greater radicalism in removal of skin , and the latter removes the main pathological reason for the routine sacrifice of the pectoralis major muscle . accordingly , since the appearance of gray 's work we have modified our technique to remove more skin , in our more recent cases skin grafting in a high proportion , and we have gradually abandoned routine sacrifice of the pectoralis major , only removing it if actually invaded , which is rare and late . the argument is sometimes used that the removal of the pectoralis major is necessary for the adequate dissection of the axilla , and that in any case its nerve supply is bound to be cut . these technical arguments are with elevation of the arm , retraction of the pectoralis major and not valid . removal of the pectoralis minor it is easy to do a complete clearance of the axillary glands and fatty tissue right up to the apex of the axilla , and at the same time to preserve the lateral pectoral nerve , the main nerve supply to the pectoralis apart from this modified radical operation there are smaller series of major . cases which have been treated in other ways , e.g. 
the comparison between the figures of standard radical and the modified radical operation in this series is rendered more difficult in that the modified radical was evolved out of the standard radical , and hence has not been done for so long . 
survivals it would therefore seem fair to conclude that these figures bring no evidence to support the view that the addition of the removal of the pectoralis major muscle brings any increase in the survival figures , and to raise the question whether the routine removal of this muscle should remain an essential technical point . a further way in which the two operations can be compared is by the comparative incidence of recurrence in the operative area , i.e. 
skin , chest wall and out of 42 traced standard radical operations there were 10 cases with axilla . of these , 7 were recurrence in the operative area , chiefly skin recurrences . cases with original lymphatic glandular involvement and 3 without such involveout of 40 traced modified radical operations there were 7 local recurment . of these , 5 were cases with original lymphatic glandular involvement rences . while the incidence in both is too high , and and 2 without such involvement . approximates to the 22 per cent noted by truscott in the middlesex hospital series , the standard radical shows no lower incidence of local recurrence than the modified . the 3 other types of procedure which have been carried out were : ( 1 ) in the first place there were 10 cases in which partial mastectomy was combined with the usual full axillary dissection after the removal of the pectoralis minor . ( 2 ) secondly , there were 9 cases in which a simple removal of the breast was combined with irradiation to the axilla . ( 3 ) thirdly , there were 7 cases in which irradiation only of the breast was combined with axillary dissection . the last group comprised cases which were all advanced , the glands being invaded in all . 
one case died as a result of the operation ; the other 6 died of the disease at intervals varying from 6 months to 4 years after treatment . moreover , in a high proportion of cases - 4 out of 6 cases which survived operationthere was either failure of the irradiation to get rid of the original primary growth in the breast , or recurrence of the growth locally after apparent disappearance . in view of the advanced character of these cases , the ultimate fatal result was likely whatever form of treatment was adopted . 
of the 2 cases with invaded glands , 1 was alive with the disease at 5 years and 1 died of other causes at 2 of the 5 cases with glands not invaded , 3 were alive and well at 10 years , years . 9 years , and 5 years , 1 was alive with the disease at 8 years , and 1 had died of other causes 1 year after operation . there were also 3 cases in which no histological note was made of the condition of the axillary glands ; of these , 1 was alive and well at 6 years and 2 died of the disease . 
from the point of view of survival after operation , this group compares favourably with other groups . but the procedure has been abandoned because of the occasional further development of carcinoma in the portion of the breast remaining . this happened in 2 of the cases of this series , and it also happened in other similar cases in a private series , in spite of the fact that , as already noted , only small and apparently early cases were considered suitable for this procedure , that a wide area of breast tissue around the growth was removed , and that post - operative irradiation was it was concluded , therefore , that while in an occasional case given as a routine . partial mastectomy combined with a dissection of the axilla might be justifiable a conclusion supporting that of fitzwilliams ( 1940 ) and of mitchener , bailey and price ( 1937 ) - the danger of further development of carcinoma in the remaining breast tissue rendered the procedure an unwise routine . the last group was of 9 cases in which simple removal of the breast was the only surgery performed , the axilla being treated by irradiation . these cases wvere usually elderly patients with apparently early growths . 
the main routine removal is not necessary ? advantages of preserving the pectoralis major are three . firstly , there is the cosmetic consideration , mutilation being much less with the pectoralis major preserved as compared with the skeleton - like prominence of ribs and costal cartilages after - its removal . 
and if there is no curative advantage in removal of the muscle , cosmetic considerations , although secondary , are entitled to a place . secondly , there is less loss of blood if the muscle is not removed , and consequently less operative shock . while in most cases this does not amount to a point of much practical importance , in old or feeble patients it may . with preservation of the pectoralis major combined surgical treatment of the breast and axillary contents is , in our experience , much less upsetting than simple mastectomy combined with irradiation to the axilla , and we have as already stated for this reason largely abandoned the latter procedure . 
1. received for publication january 13 , 1948 . one of the implications underlying the work of huggins and hodges ( 1941 ) on the factors governing prostatic hypertrophy is that malignant prostatic cells are not fully , if at all , autonomous . that is , they are still controlled in some measure by the same factors that control normal prostatic cells . specifically , this is certainly true of their susceptibility to the influence of circulating androgens and oestrogens . carcinoma of the prostate is essentially a disease of old age . the possibility exists that the chief factor in deciding the individual 's susceptibility to this disease may be his androgenic state , that is , the level of circulating androgens in his blood , particularly during the later decades of life . the only practical method for ascertaining androgenic state is a determination of 17 - ketosteroids excreted in the urine of the subject . in the hands of many different workers ( barnett , henly , morris and warren , 1946 ) this method has revealed a very wide range of excretion of 17 - ketosteroids by normal men , at least in the lower age - groups . 
carr it is considered that the same proportion of the reproductive life of a - human female would bring her to 21 years of age , and that of a mouse to 41 moiiths , this emphasizes the very restricted nature of the sample usually studied . most of the data on spontaneous tumours comes from reports from poultry pathology laboratories , and is given as a percentage of all cases of deaths sent in for examination . this causes a serious under - estimate for several reasons for example , many of the deaths are due to s . 
pullorum and coccidial infections which strike the immature chick long before cancer age ; further , pathological investigations are usually only requested when a si - idden rise in mortality suggests an epizootic is beginning , while isolated deaths , which would include those due to cancer , are not always submitted for investigation post mortem . thirdly , there is little agreement among poultry pathologists upon the classification of cancer . 
the data available are thus no guide to " cancer incidence " in fowls , in the sense that this can be defined for mice and man , and are , for the reasons suggested above , usually a gross underestimate . 
although many such figures are available from various parts of the world it will perhaps be sufficient to compare the tumour incidence in the edinburgh flock , where all birds dying are examinedpodmortem , with data given bv goss ( 1940 ) , where a similar analysis has been made with flocks totalling 24 , 900 birds . 
out of 675 female birds dying since 1932 in the edinburgh flock at ages ranging from i to 9 years , only 50 , or 7 - 4per cent of the total adult mortality , gave evidence of neoplastic or allied conditions . 
the edinburgh flock in general is thus a " low cancer " line of considerable ' interest . at present it is sufficient to indicate that complications due to spontaneous cancer can be neglected in considering the resiilts which follow a preliminary 8tudy0f 8u8ceptibility . the first analysis was made upon a series of 429 birds inoculated with cell - free rous no . 
the susceptibility of each bird was graded a ' ceording to the following scheme : negative result ( 0 ) , regression of tumours ( r ) , tumour response to i to 4 , for increasing lasses in all . 
the largest size and malignancy of the induced sarcoma at death or after 28 days was used as an indicator of the susceptibility of the bird . the grading was ' done by inspection . weighing the tumour is unlikely to be more accurate because of the difficulty of clean dissection , and the neglect of such factors as the size and condition of the host , the invasiveness of the tumour , and the presence of large blood - clots and mucoid fluids within its substance . in addition to differences in susceptibility of the host other possible causes of variation were considered , such as sex , season , site of inoculation , number of inoculations , dose of virus , and presence of other factors , such as antibodies injected with the virus . 
no consistent sex difference in susceptibility was noted during the work , and , as was later seen in the analysis , sex does not seem to affect the susceptibility to any detectable extent . 
teratoma testis ( michaelowsky , 1928 ; falin and gromzewa , 1939 ; bagg , 1936 ) ; transplantable sarcoma ( peacock , 1935 ) ; chemical induction ( murphy and sturm , 1941 ) , an analysis of the susceptibility of these young chicks to the rous no . 
i sarcoma showed no seasonal trend ( carr , 1942 )  . that the site of inocul - ation is of little importance in influencing tumour growth was shown by gye and purdy ( 1 931 ) ; it was claimed by them that the resistance depends upon the dose of virus inoculation . no support for this claim could be found by carr ( 1942 , 1943a and b ) , and the results described below indicate that any such variation is inconsiderable . that the other factors mentioned , viz . 
number of inoculations - and presence of other materials , were probably of sl ' l ' ght importance was concluded from several experiments in which only one of these factors varied in an otherwise identically treated g ' roup . 
a large number of the experiinents found in the literature illustrate this point , which is seen to be confirmed in the analyses that follow . the birds comprising the first group of tested animals were from most - of the " all the year round " hatching had been necessary to maintain institute lines . an even supply of experimental chicks , but not many matingswere represented by more than a few tested chicks . in fact , the 429 birds were descended from 33 sires and 147 dams , and many matings had but one tested offspring . 
carr the various institute lines ; these were all selected for physiological characters associated with egg production . dividing each line into two clear classes , negatives and non - negatives , the difference between the breeding line ( with the largest number ) and non - moult line was examined . 
a similar test on the most conspicuous of the other negative tumour groups , intensity , gave a value of chisquare 1 - 23 , which is of no significance , being the variation that would occur in i out of 4 random samples . it was therefore unnecessary to test the rest of the since the regressio ' ns ( r ) are equal to the negatives in the breeding line , groups . but more frequent than the negatives in the non - moult line , the frequency of regressions in the non - moult line is therefore even more significantly disproportionate than the number of negatives , so that this line has an obviously high resistance to the production of fatal cancer by the rous no . 
at about the close of the period when the first analy 'sis was made , the breeding programme at edinburgh resulted in a large proportion of chicks provided for experimental inoculations being derived from a single pen of the breeding line . these chicks were all offspring of a single sire , f651 , and dams fairly closely related to him . .the annual population of the breeding line is larger than that in any of the other groups constituting the flock , and the method of selection used is such that they are also less inbred . in table iv the responses of the groups of progeny from 14 females mated to f651 are illustrated . it is obvious that there is considerably variation among the groups ; in the first three the responses are mainly restricted to the two highest types , and in the fourth the same tendency is only slightly less marked . in the next six progenies ( g196 - g866 ) they are distributed fairly evenly over all the classifications except the completely negative one . 
carr this tendency for the susceptibility of chicks from certain individual matings to fall into a rather narrow range has been encountered in other pens of birds , and knowledge of its existence has been made use of both in providing susceptible chicks for experimentation 4nd avo - iding the progeny of dams whose offspring were known to give a poor response . 
it had been noted that when the non - moult chicks included in the original analysis were grouped according to sires , one of the latter , h573 , stood out as producing particularly resistant progeny ( table v )  . fact , when the data from his chicks were omitted the difference between the responses of chicks from the breeding and non - moult lines were no longer signifiit seemed probable then that the disproportionate number of regressions cant . and negatives produced by h573 was not due to the character non - moult as such , but to some mechanism which can . 
on the other hand , to have carried out an experiment on a large number of birds in the hope that one of the rare resistant class was included would require labour and accommodation far beyond the facilities of any place engaged in fowl tumour work at this time.. the dams of the offspring of h573 analysed in table v were all fairly close relatives of the cock himself , and the way was thus opened for breeding a line of birds which would include a large proportion of resistant animals . it was arranged to carry out a small series of tests on the progeny of h573 , and almost all the birds tested gave either very ismall tumours , or more often , complete regressions . 
the slight shift towards greater resistance in the first 1941 test in both halves ofthe table suggests that some environmental factor leading t ' o a greater inhibitive effect on tumour growth may have been operative then . when the line had been thus established , a number of females , which had been tested and found to produce resistant offspring with a male of their own line , were then outcrossed to a non - moult cock , a descendant of the group from which the non - susceptible ( n - s ) line had been extracted . 
1 sarcoma virus varies from 40 per cent ( fischer , 1927 ) to 4 = 5 per cent ( gye and purdy , these figures may be complicated , however , by different rates of spon1931 )  . taneous sarcoma occurring in the population , either causing " natural " - or this complication is " induced " antibodies to be formed in the tested animal . probably absent at 6 weeks ( the age used here ) as no antibodies are present at this stage ( amies , 1937 ; andrewes , 1939 ; carr , 1943b ) , though they occur in resistance also varies with the age of the bird ( duranyounger and older chicks . reynals , 1940 ; rous and murphy , 1914 ; carr , 1943b ) , so a standard of age for testing is requisite for comparison . in the selection experiment for high and low susceptibility to jungherr sarcoma , carried out by cole ( 1941 ) for example , a resistant line with only 12 und impossible to raise the per cent susceptibility was obtained , but it was high incidence line much above the . 
original 70 per cent ; the cause of this may have been acquired r ' ather than a genetic immunity , since transmission from the immune female to the chick via the egg - yolk ( andrewes , 1939 ; carr , 1944 ) cannot be excluded , for progeny were tested at 7 - 18 days ,  . 
a time when yolk antibody is possibly still present in the chick . acquired immunity was ruled out as a cause of resistance of the n - s line . perhaps the most useful comparison which can be ' made is that between the present analysis of responses of the edinburgh flock to the filtrable tumour rous no . 
1 , and those of birds from the same stock to chemical tumour inducing material as demonstrated in the work of peacock , a report on which has been published ( greenwood and peacock , 1945 )  . 
the data , which cover the behaviour of 4 lines for the 10 - year period from 1935 - 1944 , are interesting both in their points of si ' milarity and dissimilarity to the material already discussed : they were classified only into positive and negative groups , but the non - moult line again showed itself the most resistant to cbemically induced tumours with a susceptibility of about 30 per cent , while breeding and large egg gave a figure close to 40 per cent and intensity had the highest susceptibility with 60 per cent since the early analysis of rous data places breeding ' as highest in posit ' lves . order of susceptibility , this difference in rank order might reflect inconsistency in the relative responses of the two lines to the different types of tumou ' r , but it appears more likely that with continued inbreeding the intensity line has chanced to become more susceptible . 
when most of the inbred lines were tested it was found that one in particular showed an obviously high resistance to the production of fatal cancer by the rous no . 
calcutt oestrogens : oestrone and diethystilboestrol . a group of arsenicals chosen in view of neubauer 's ( i947 ) implication of arsenicals as carcinogem ' c agents . three unrelated compounds : nitrogen mustard ( shown to be carcinogenic by boyland and homing , 1949 ) , urethane ( shown to be carcinogenic by jaff6 , 1947 ) and light green f.s. 
numbers represent duration of exposure in minutes to filtered ultraviolet radiatioxi required to cause death of 90 per cent of the cultures . with the exception of the oestrogens none of the agents tested compare in comparisons among the compounds tested effectiveness with 3 : 4 benzpyrene . suggest a certain degree of correlation with carcinogenicity . 
whether the effects achieved are a true photodynamic response as occurs with fluorescein and other dye stuffs , or ate a consequence of intracellular action by the radiation leading to increased susceptibility to a toxic agent , as calcutt ( i 950 ) has show - n to occur in the case of certain - sh inhibitors must remain in doubt . 
on the other hand , it appears possible that the radiation has brought about such an intracenular change that the chemical carcinogen is now able to attack a much greater amount of substrate than is normary the case . 
thus complete disruption of the intracellular functioning and death occurs , rather than ' a partial disruption which manifests itself as the carcinogenic change . certain evidence supporting such a view exists calcutt ( 1950 ) showed that irradiation with wave - lengths in the literature . greater than 3300 a increased the availabihty of intracellular - sh groups . such treatment prior to the addition of a photosensitising agent was show - n by calcutt ( 1951 ) to enhance the photodynamic response . 
with a stroke of 6 cat a rate of 90 per minute , and melanin formation estimated at appropriate intervals by observing the extinction coefficients of the solution with an e.e.l. 
on 15 occasions there was acceleration averaging approximately 0 - 3 per cent as compared with the control . on the assumption that the errors inevitably present will tend to operate equally in either direction , the probability of obtaining 15 results out of 17 in one direction is ( approximately ) only i in 500 , so that the results are statisticany significant . the possibility of the acceleration being due to change in ph was reconsidered . the ph of the various solutions employed was estimated , electrometrically , using a glass electrode . 
one of these paths is through the physiology of hormone production , a second is through the physiology of the propagation and transmission of the milk agent , and a third possible path is through the physiology within the mammary tissue cell governing its reaction to the hormonal stimulation or the milk agent . other paths may exist , and it is probable that these three are interwoven . proof of the effect of genic action in relation to the hormonal stimulation resulted from crosses between strain a in which the incidence in the virgin females is low althougb that of the breeders is high , and strain ch , in which the incidence in the virgin females as well as the breeders is high . results of such crosses were reported by bittner , h ' useby , visscber , ball and smith ( 1944 ) , heston and andervont ( i 944 ) , and bittner and huseby ( i 946 )  . 
heston incidence occurred among the virgin f , females resulting from mating strain a females to ' ch males as well as in the reciprocal f , virgins , together with evidence of segregation in the f2 generation , indicated that the difference between the strains was primarily a genetic difference . such a difference was to be regarded as either a difference in horinone metabolism , or a difference in the reaction of the mammary gland cell to horinone such evidence as the fact that added oestrogen stimulation yielded stimulation . tumours ' m ' strain a virgins , ' and the relationship of number of litters to tumour incidence in strain a reported by jones ( 1940 ) , strongly indicated a difference studies of the oestrus cycles of virgin females of strains in hormone stimulation . a and ch and their reciprocal f , hybrids reported by deringer , heston and andervont ( 1945 ) , however , failed to show any difference in the cycles , except that in the low - tumout group of virgin strain a females the onset of oestrus was these observations , therefore , suggested later than in the high - tubiour groups . that at least a part of the genetic difference could be manifested through the physiology within the mammary gland cell . in an attempt to determine the physiological mechanisms through which the genetic differences are manifest , huseby and bittner ( 1947 ) also have carried out a number of studies , including ovarian transplantation to f , hybrid mice , ovariectomy , vaginal smearing , and histologic examination of the genital tissues . these studies have indicated that more than ' one endocrine organ is affected . we have become more interested in the second path of gene action - that it has concemed with the propagation and transmission of the milk agent . been observed by a number of investigators that certain strains will propagate all the . 
high - mammary tumour strains the agent , whereas others will not . normally transmit the agent from generation to generation , and even low - tumour strains may have the same innate capacity as andervont ( 1945 ) has reported for strain c . 
on the other hand , bittner ( 1948 ) has found tumours in his descendants of strain c57 black females into which the agent was introduced , and fekete and little ( 1942 ) bave reported mammary tumours in descendants of c , , 7 black females that had developed in strain dba uteri from transferred ova . 
thus the situat ' lon m regard to the capacities of the various strains to propagate the agent is not clear . by crossing high - tumour strain c , h females with low tumour strain c57 black males , and comparing the two . 
types of backeross females produced by backcrossmg the f , females to both the ch and c.7black males , definite evidence of genetic differences in the ability to propagate and transmit the agent was revealed ( heston , deringer and andervont , 1945 )  . 
the possibility of an intracellular origin of the agent also enters into consideration . in some respects the picture is comparable to the gene - kappa relationship stuclied by sonneborn ( 1945 ) and co - workers in parameciuthe picture is not as , simple , however , in that there is . 
our attention has been directed toward tumours that arise in females in which the agent cannot be demonstrated ( heston , deringer and levillain , unpublished data )  . in order to obtain a line of strain ch friae of the milk agent a litter of 3 females and 3 males were removed from their c3h mother by cesarean section and fostered upon c57 black female . 
these females were later mated to their male littermates , and subsequently the line has been maintained by brother x sister matings , the young being nursed upon their own mothers . in this line ; designated as c3hb , mammary tumours are arising . in 194 of the females of this line 14 months of age and older and extending through the first 5 generations to date , 47 , or 24 per cent , have developed mammary tumours at an average age of 18 - 9 months ; seventy - eight have died without mammary tumours at an average age of 16 months , and 69 are still living at an average age of 18 months . study of the histologic section of 37 of these tumours has not revealed mucli dissimilarity between these and the usual ch mammary tumours . nine , however , ' have show - n areas of squamous metaplasia with pearl formation similar to that described by kirschbaum , williams and bittner ( 1946 ) in mammary tumours induced by methylcholanthrene in the absence of the milk agent such areas also occasionally occur in normal strain ch females of older age , suggesting that the occurrence of squamous areas may be characteristic of older age rather than specifically owing to the possible absence of the milk agent . three of the tumours arising in these c3hb females have been transplanted into other c3hb females , and in each case the transplant has grown . we have no evidence , however , of a milk agent in the etiology of these tumours . distribution of the tumour - bearing females in the pedigree chart does not show segregation of tumour families , as ' would be expected if the agent were present . furthermore , we have found no evidence of the agent in cell - free extracts of these these extracts varied from 2 to 5 per cent , and were prepared in 0 - 005 m tumours . .phosphate buffer ph 7 - 0 with a waring blendor ; cleared in a multispeed centrifuge at 18 , 000 g.. 
heston extracts premonths of age and older , and none has yet developed a tumour . pared with the same technique from tumours from c3h females produce tumours in c3hb test females in approximately 8 to 10 months . this is not presented as absolute proof that the agent is not present . if it is , however , it is not comparable to that in c3h females , nor is there any evidence of its being built up comparable to that of c3h . if the agent is not present we have proof that the accumulation of genetic factors and of non - genetic factors other than the milk agent can cause the tumour threshold to be surpassed . this light the milk agent would be comparable to the carcinogens in the induction of lung tumours , where the presence of the carcinogen appears to merely increase the probability that the tumour will appear and at an earlier age ( heston , 1942a , b )  . while all of these factors have been shown to alter the probability that the normal mammary tissue cell may be transformed into a malignant cell , these investigations have not answered the question as to what constitutes this change to malignancy . 
parsons. from the department of chemistry , the university , manchester , 13 , and the royal eye hospital , southwark , london . received for publication august 15 , 1949 . the effects of injection of the four nucleotides obtained from ribonucleic acid on the tissues of normal and tumour - bearing mice have been described ( barakan , barker , gulland and parsons , 1948 ; parsons , gulland and barker , further experiments have now been carried out to note the action 1947 )  . of purine and pyrimidine bases on sarcoma growth , and to correlate if possible the biological activities of the compounds with their chemical structure . these experiments fall into two groups : ( a ) those relating to the amino and hydroxy purines , ( b ) those relating to uracil and its derivatives . both pure - line and stock mice were grafted with homologous or heterologous sarcomas , including c57 and s37 and the crocker sarcoma , the latter known to be very refractory to inhibitory action ( badger , elson , haddow , hewett and robinsoir , 1942 )  . 
the technique for treatment of the grafted mice was similar to that previously described , but the standard dose ( 0025 g . ) was reduced in proportion to the toxicity of any particular compound , or where the condition of the mouse necessitated this . insoluble or relatively insoluble compounds such as xanthine , guanine , adenine or hypoxanthine were administered as fine suspensions in the same media as used for the soluble compounds . examination of the tissues at varying intervals showed that all compounds injected as suspensions were rapidly removed within 24 hours with the exception of guanine , the relative inactivity of which on tumour growth seems to be due to its marked insolubility . deposits of the injected guanine were found at the site of injection long after the last dose . table i summarizes the results obtained . 
the total number of control mice was in all cases the same as the total number of treated mice . the amino and hydroxy purines . it had been noted that adenylic acid or adenosine produced shock when injected into mice , and it seems probable that this effect was due to the adenine radical , of which the pyrimidine ring is in a lower state of oxidation than those of the other compounds used which do not induce shock . injection of adenine in doses comparable with those used for adenosine or adenylic acid has been found to cause immediate and profound shock with heavy mortality , the minimum sublethal dose being 0005 g . 
parsons radical , but may be connected with the presence of the amino group in position 6 in the adenine radical . xanthine injected in tumour - bearing mice was removed from the tissues injected into in 24 hours , but no inhibition of sarcoma growth was observed . normal mice in doses of from 0 - 02 - 0 * 025 g . 
2 , where it wir be seen that the addition to the medium of the drug in a concentration of 60 mg . / litre reduces mitosis to less than one half . 
the drug was given intraperitoneary in doses of 5 y twice daily over a 5 - day period . there was no difference between treated and untreated mice in the time of disposal . ar experimental animals have shown a temporary loss of weight after being given the drug . effed , 8 on human malignant di8ea8e . this report , which is prehminary in nature , describes the testing of the compound in 17 patients suffering from leukaemia , polycvthaemia vera , lymphadenoma , multiple myeloma and three types of carcinoma . cases were chosen because they were unfavourable or too advanced for other forms of treatment . this choice of the least favourable cases - makes it harder to compare the effects ofthe drug with effects obtained with other forms oftherapy . it is , however , of value to compare in any individual patient the effects of the drug against those of any other type of appropriate treatment given either prior or subsequent to 9500 . the drug was given intravenously in doses ranging from 0 - 09 mg . 
probably represents a working range within which toxic effects on the bone marrow are not serious . side effects were slight ; half the patients had anorexia or nausea , generary very shght . 
the dose used in this case resulted in a temporary fan in haemoglobin and a fall in the white blood count to 1000 per c.mm. , at which time she was given a simple blood transfusion . 
at the end of this remission she was suffering from lassitude and following treatment with abdominal discomfort , and a rising white blood , count . 9500 her well - being improved ; her white cell count fell and the haemoglobin , which was 86 per cent , rose slightlv . primitive cells fell from 26 per cent to 14 per cent within 4 davs . 
the siibsequent historyof this patient was complicated , 2 months - after treatment , by , ' hepatogenous jaundice with leukopenia . four months after treatment the ' haemoglobin began to fall and the white cell count commenced to rise , and sore throat appeared , primitive cells rising above the she was re - treated a month later with 9500 , no beneficial pre - treatment level . effects being observed in the week that elapsed between treatment and death . post - mortem examination showed a massive leukaemic infiltration of liver , kidneys and spleen . 
the bone - marrow from femur and sternum appeared active . multiple capillary haemorrhages were present in the myocardium and brain . is difficult to assess the effect of treatment in this case owing to the complicating factors . 
the i - emission , however , was not as satisfactory as that previously obtained with x - rays . myeloblastic leukaemia of naegeli type . - this was a terminal case which had been treated previously only with transfusions . within 7 days after treatment the haemoglobin rose and the white cell count fell from 145 , 000 to within normal limits . primitive cells fell from a pre - treatment level of 76 per cent to 37 per cent and the myeloblasts and premyelocytes disappeared completely . however , this remission , although dramatic , was short . 
an improvement in the leukaemic condition was prompt . five days after the first treatment the total white cell count was within normal limits and immature cells had been reduced from 40 per cent to ' 6 per cent of the total . 
a good remission was noted 20 davs after treatment , which compared well with her first and best remission fohowing splenic irradiation . the patient felt better within a few days . 
the remission as far as the blood count was concerned after 9500 a similar reduction in red cells and haemoglobin lasted one month . this las ' ted 4 months , after which the symptoms recurred . 
none ( transfusion ) ( bleeding from tumour ) ca8e ix . generalized lymphadenoma ( section proved )  . - this patient was nevertheless the enlarged nodes decreased given a rather low dose of 9500 . very temporarily and the skin itching from which he suffered disappeared for - about a week . 
a drill - biopsy of the mass did not yield conclusive proof of lymphadenoma , which was nevertheless following treatment the itching was reduced and probable on clinical grounds . the skin , which was dry and iethyotic , became more normal in texture . 
the relief of symptoms this patient showed an interesting initial rise in the lasted less than 3 months . polymorphonuclear count at 4 days , prior to the onset of leukopenia . 
on both these occasions improvement in well - being occurred and some reduction took place in the size of his enlarged liver , - the improvement after the second course of nitrogen mustard being much less . on admission for treatment with 9500 , the liver was enlarged and oedema of the legs was present . 
none of them responded to the drug . case xv was later given a second course of treatment simultaneously with x - ray therapy , both agents being given as weekly treatments for growth - restraint . 
a leukopenia is generary seen , especiary at higher dose levels . this is due to a fall in both granular and lymphocyte series . the fafl in the granular cells may be preceded by a transitory rise over 3 to 4 days , not seen unless blood counts are repeated soon after treatment . 
effect of 9500 on peripheral blood count in a non - leukaemic case . no initial rise has been seen in the lymphocyte count , which reaches the lowest level 1 to 7 days after the end of treatment . complete recovery is slow and would seem to take about 2 months . 
for these two reasons we have waited for several weeks before instituting a second course of treatment in any patient . an extended clinical trial of 9500 would , however , seem to be justified on several grounds : first because it may be found effective in diseases other than those quoted ; even among the cases described there would seem to be a place for secondly , it could be regarded as a it in the treatment of polycythaemia . pleasanter alternative to nitrogen mustard , since , unlike nitrogen mustard , 9500 does not produce gastric effects and there is no fear of local thrombosis . 
thirdly , the drug is active ifgiven by mouth ; we have so far not tried its clinical effectiveness by this method , since , animal experiments have demonstrated that by this route the haematological response was less predictable . there is one disadvantage to an easily given drug of such potency . it is possible that it might be used without the constant supervision and check of blood counts which is necessary . 
as with all cytotoxic agents , its use should be contemplated only by those with facilities for adequate laboratory examinations . the tissue culture work has been carried out by m . 
bartholomew 's hospital , london , e.c.i. received for publication august 25 , 1949 . the question , whether the recent increase in deaths attributed to cancer of the lung is due to a real increase in the incidence of this disease , has been discussed the present paper , which brings forward no new data , is an by many writers . examination of some of the evidence offered on this subject . ( 1 ) the application of statistics from hospitals . the problem of finding the best index of a real increase in the incidence of lung cancer from hospital statistics is a difficult one . the relevant facts usually ascertainable at a hospital are : the annual total 1 . 
3 , 6 and 9 could be used as a measure 3 and 6 are open to objection on the grounds of the incidence of lung cancer . of possibly mistaken diagnosis , hence presumably 9 is the most accurate measure of what it is stated to be . as a measure of the population at risk , i.e. 
of becoming a case on which a post - mortem for cancer of the lung is done at a given hospital , we could use 1 , 2 , 4 , 5 , 7 or 8 . do these measures change in their quality of being representative of the the answer is that they all do so , because the cross - section general population ? of the population being admitted to hospital , whether of all cases or of cancer alone , changes , and therefore the cross - section of all deaths represented by deaths in hospital changes also . 
the assertion that the cross - section changes is based on knowledge that many people are now admitted to hospital who never would have been so admitted in the past - e.g. 
the same argument , that the cases would have been sufficiently serious to be admitted under any circumstances , could be applied , though with less certainty , to 2 , 4 , 5 , 7 , 8 . 
kennaway pathologists who deny that there is any satisfactory evidence of the suspicion is that where the incidence of lung cancer during recent years . such increase has appeared to have been conspicuous , there was formerly a low standard of accuracy of pathological diagnosis , and that the standard has improved with the passage of time . " real increase elusive disease has estimates of incidence , " for the foregoing reasons , comparisons of early and recent clinical or necropsy comparisons of the findings in different countries or in different hospitals , must be quite unreliable . so much depends on the personal experience of the clinicians and pathologists concerned , and current jotmrnals contain evidence enough that a uniformly high standard of diagnosis of this yet been attained by either . 
3 shows no steady rise , " which is perfectly true , and they conclude : " in our opinion the figures given illustrate that even a pronounced increase of the crude mortality rate for lung cancer among males , and almost only among males , does not necessarily mean an increase in incidence of that disease . 
presumably the more frequent detection of the disease is due to improvement of diagnostic procedures , and increased attention , and similar explanations may be correct in the case of occupations with an increased mortality from lung cancer . " one has difficulty in believing that any generalizations about cancer of the lung can be based upon such a peculiar succession of such small totals , drawn from a highly selected population , as those given in the third columnu of the table , namely 7 , 5 , 5 , 7 , 6 , 20 , 13 , 20 , 13 , 14 cases of pulmonary cancer . is one to believe that the totals 6 , 20 , 13 in the three consecutive years 1940 , 1941 and 1942 correspond to any similar annual incidence upon the whole population of denmark ? if there is no such parallelism , what is the value of these figures , and how can they provide a basis for the important generalization quoted above ? one may doubt whether the radiographic examination of any population for pulmonaty tuberculosis adds much to our knowledge of the total incidence of cancer of the lung . such a survey will , of course , reveal a number of cases , previously undetected , of such cancer . 
7. received for publication february 3 , 1949 . one of the surprising elements in bittner 's discovery of the " milk factor " is the apparent entry of the virus into the bodies of the young mice via the it is , however , obviousthat during suckling a small amount alimentary canal . of milk may also enter the nostrils , and that the nasal mucosa may offer an alternative port of entry . it also seems possible that the milk factor might be destroyed by digestion in the stomach . if this were so it would be difficult to recover milk factor from the stomach contents of suckling mice . 
the unfortunately the experiresult was entirely negative in the 40 mice so treated ment was not adequately controlled , in that none of the mice were tested for susceptibility by means of extracts known to contain the virus . 
jackson memorial laboratory , bar harbor , me . received for publication december 16 , 1948 . it is known from the work of andervont and bryan ( 1944 ) and green , moosey and bittner ( 1946 ) that the milk agent is antigenic for the rabbit and the rat . if , as is probable , the agent , is a virus one would expect it to be antigenic for the susceptible species . 
the nature of the s35 substance . the presence of s35 in the cytoplasm of myeloid cells after culture in s35 sulphate was all the more interesting since most mammalian cells will not utilise experiments were designed to obtain information on the nature of sulphate . the s25 substance in the myeloid cells . 
the summarised findings are presented in table i . ( 1 ) since 2 - 3 hours ' washing of the slides in running water , or 1 hours ' incubation at 370 c . 
a search was therefore made for a sulphate compound in these cells . although most sulphates form an insoluble precipitate with barium , it has been reported that the barium salt of chondroitin sulphate is soluble in water it was thought that the s35 in the cells might ( bray , gregory and stacey , 1944 )  . be in a form related to the chondroitin sulphates , therefore experiments were carried out to test the barium solubility of the su compound in the cells . both 1 m and 0 - 1 m ba ( oh ) 2 removed all the cells from the slides , but this could be prevented by m.aking up the ba ( oh ) 2 solutions in 10 per cent formalin . the morphology of the cells on the slides thus treated was unaltered , and it was found that 15 minutes ' treatment with 1 m or 0 - 1 m ba ( oh ) 2 formalin at 20 c . removed all isotope from the cells . formalin alone did not appear to remove any s35 . it had to be ascertained whether the effect of ba ( oh ) 2 was a specific ba effect slides subjected to distilled water alkalinised with or due to the alkaline ph . nh3 to ph 9 - 10 for 15 minutes at 200 c . 
for one hour or longer . that the s35 substance is not closely related to hyaluronic acids . ( 6 ) no parallelism could be detected between the behaviour of the s35 substance and those polysaccharides and other substances which give a positive hotchkiss reaction ( periodic acid schiff reagent )  . 
for 1 hour , the s3 substance was not . all hotchkiss - positive substances ( fresh human saliva , 1 hour at 370 c . ) , but it did not affect the isotope content of the cells . 
the uptake of methionine s35 . at the beginning of the experiments it was considered to be unlikely that s35 administered as sulphate to the culture medium would be transformed by the cells to sh groups . 
oliver s35 sulphate administered in vivo to rats has been shown to be taken up into the chondroitin sulphate of the growing cartilage ( dziewiatkowsky , benesch and benesch , 1949 ; dziewiatkowsky , 1949 ; 1951a , 1951b , 1952 )  . irrespective of whether sulphate or sulphite s35 compounds were given to rats in vivo , activity this finding has was found in the bone marrow by singher and marinelli ( 1945 )  . been confirmed by dziewiatkowsky ( 1949 , 1952 ) using whole bone autoradiographs and it was thought not to be chondroitin sulphate , but to be inorganic sulphate this sulphur after the first 30 minutes sulphur which is precipitated by ba ( oh ) 2 . of administration , is incorporated into a more complex compound from which the sulphur is slowly removed . the s35 substance in the myeloid cells of the bone marrow cultured in vitro it is possible that the dose of s35 sulphate given is removed by barium salts . to the rats by dziewiatkowsky was too small to be detectable in whole bone autoradiographs in the acid formalin fixed bones ( 5 / tc . / 7 - day - old rat in one series and 1 - 25 , tc . / 7 - day - old - rat in the other series of experiments )  . at this stage of the work it is probably too speculative to attempt to correlate the specific s35 sulphate uptake of the myeloid cells with the specific action of myleran ( 1 - 4 dimethanesulphonyloxybutane ) on the myeloid cells . 
doll. from the statistical research unit of the medical research council , london school of hygiene , keppel stred , kondon , w.c.i. received for publication november 28 , 1953 . attempts to derive theoretical laws from changes in the death rate with age have a long history . 
they have not , in general , been very fruitful and there has - been some hesitation in applying the technique to the study of cancer . recently , however , two hypotheses about the mechanism of carcinogenesis have been put forward , which have been derived from analysis of cancer mortahty fisher and horomon ( 1951 ) used statistics from the united states statistics . for cancer of the stomach in women , and nordling ( i953 ) , classing all sites together , used statistics for cancer in men from britain , france , norway and the u.s.a. both found that , within the age group 25 - 74 years , the logarithm of the death rate increased in direct proportion to the logarithm of the age , but about six times as rapidly ; in other words , the death rate increased proportionany with the sixth power of the age . 
death rates in some age groups under 24 years were . higher than would be expected had this basis been a general law throughout iffe . rates for the age groups above 75 years were considered unreliable and were excluded . in interpreting these observations , both assumed that mortahty gave a good indication of incidence and treated the data as if they referred to age specific incidence rates . 
they considered that cancer in youth might be affected by special factors which were unhkely to operate at later ages and they , therefore , felt justified in basing their hypotheses on the data recorded for adults . fisher and horomon ( 1951 ) pointed out that the observed relationship between age and mortahty could result if a colony of six or seven cancer cells was a critical size below which independent growth was not sustained . thig hypothesis , however , also leads to the conclusion that cancer incidence should be proportional to the fifth or sixth power of the concentration of the effective carcinogen whereas experimental data suggest that , in general , tumour incidence and concentration of the carcinogen vary ' in arithmetical proportion . 
the hypothesis in its simple form is , therefore , untenable . nordling ( 1 - 953 ) , on the other hand , suggested that the observed relationship would be explained if a cancer cell was the end - result of sev ' en successive mutations . this hypothesis does not lead to the observed result in all circumstances . does so only if the probability of occurrence of each mutation remaihs constant throughout hfe . in this case and so long as the occurrence of each mutation p . 
the logarithm of the incidence rate will then be directly proportional to the logarithm of the age and will increase six times as rapidly , ix , log rate 6 log t + a constant . in contrast to fisher and hollomon 's ( 1951 ) hypothesis this leads to the conclusion that the final rate of tumour formation wir be directly proportional to the concentration of an applied carcinogen , so long as the probability of occurrence of a mutation is proportional to the concentration of the carcinogenic factor and different factors are required to effect different mutations . in his analysis , nordling ( 1953 ) grouped all types of cancer in men together and considered them as a whole . 
he gave no detailed figures for cancer in women , but stated that for cancer of the sex organs the increase in mortahty was fairly small above the age of 4.5 and that for other sites the mortality seemed " to increase according to the sixth power of the age both before and after the forties but not during the decade of the menopause when the increase is smaller . " he considered that the entire increase with age in cancer incidence among adults was not wholly explicable by a mechanism of multiple mutations but that hormonal control of growth might play an independent part . 
1 - 4 show the logarithms of the male and female death rates from cancer of the commonest sites in england and wales in 1950 and 1.951 ( registrar general , 19521 1953 ) , plotted against the logarithms of the mid - points of the age groups . for each sex , all those sites are shown for which more than 1000 deaths were recorded in each of the two years . 
are less reliable than those for the subsequent ones since they are based on much smaller numbers , and both standard errors and ( to a lesser extent ) arithmetical errors are much larger . for example , the standard error of the death rate from gastric cancer in women is 18 per cent of the rate for the first age group ( 25 - 29 years ) and .2 per cent of the rate for the last ( 70 - 74 years )  . that is to say , the logarithms of the true rates for these age groups are likely to lie within a range of - .0 - 13 and - .0 - 02 respectively of those showm in fig . 
i. - change in mortality with age for cancer of the oesophagus , stomach and pancreas in men and for cancer of the stomach and pancreas in women shown on a double logarithmic scale , that is , the logarithm of the death rate per million persons plotted against the logarithm of the mid - point of the age group . 
the straight line through the points has been drawn arbitrarily to give the best fit , subject to the gradient being 6 to 1 . cancer of the stomach , colon , rectum and pancreas in women - the observations fall fairly close to the lines . in some , however ( cancer of the colon in men , cancer of the stomach , colon and rectum in women ) , the observations fall closer to lines with less steep gradients . 
the relatively high rates at the younger ages could , however , result if the population contained a group of subjects speciahy susceptible to cancer of these sites in early life - and so far as cancer of the p . 
doll colon and rectum is concerned , such a group is in fact found in subjects of polyposis coli . the actual regression coefficients for all the first group of cancers are shown in all the mortahty rates for this group , table i ; they vary from 4 - 97 to 6 - 48 . therefore , show the same sort of association with age as was reported by fisher andhoromon ( 1951 ) andbynordling ( 1953 )  . 
3. - change in mortality with age for cancer of the lung , bladder and prostate in men and for cancer of the lung in women , shown as in fig . 
1. i 0 - 1 - 6 consists of cancers for which there is already reason to believe that the strengths of some of the factors responsible for their development are variable . cancers of the prostate , breast , ovary , and cervix and corpus uteri are all believed to be influenced by endocrine secretions , which vary 1 ' n each individual in the course of his life ; a proportion of the cases of cancer of tho lung is believed to be related to cigarette smoking which has become more prevalent in the last 50 years and a proportion of the cases of cancer of the bladder is due to occupational hazards , to which men have been exposed for various periods at various ages . 
on the hypothesis that carcinogenesis is a multi - stage process , therefore , cancer at these sites would not be expected to show a uniform relationship between death rates and any power of the age . 
doll the sort of irregularities to be expected will depend on the periods when the carcinogenic factors are most active and on which of the stages in the process of carcinogenesis are affected . 
an increased rate of production for a short time during early life will provide a larger number of altered cells to be acted upon by other factors in the future , and wfll therefore appreciably affect the incidence at , say , age 60 . 
the weight depends both on the time of operation of the carcinogenic factor concemed and on the order of the cellular change which it affects . if t is the age at which the cancer incidence is observed , to the age at which the subjects are exposed to the factor , and s takes a value between i and 6 according as the change effected is the first , or sixth , then the weight is proportional to second , tos - i ( t - to ) 6 - 8 . hence it can be show - n that the weight by which a varying probability of the first mutation would be multiplied is highest at age 0 and decreases rapidly throughout life . 
the weight for the probabihty of the second change reaches its maximum one - fifth of the way through the exposure period ; that for the third change , for factors effecting the seventh change ' , two - fifths of the way ; and so on . the cancer incidence will be directly proportional to the rate of production of this change at the time of observation , and the previous behaviour of this rate will be irrelevant ( i.e. , will have zero weight )  . since the weighted mean of the varying probabihty will in general depend on the age , t , the overall incidence at age t is no longer proportional to the sixth power of t . 
doll old ages , can be attributed to the fact that the populations concerned belong to if mortality generations which smoked fewer cigarettes than subsequent ones . at different ages is examined for cohorts born in different five - year periods , the effect disappears . the concept of carcinogenesis as a multi - stage process also makes it easy to understand the mechanism of the latent period which occurs after exposure to a for example , kennaway carcinogenic agent before the appearance of a tumour . ( 1947 ) has demonstrated that circumcision deferred until the fourteenth year of life fails to give the complete protection against cancer of the penis that it provides when carried out on the eighth day ; in other words some change must take place within the first 14 years of life which eventually leads to the development of the disease after a latent period which may be as long as 70 years . 
on the hypothesis that penile cancer is the end - result of a series of seven successive cellular changes - the first of which occurs only in the presence of the prepuce , it can be shown that at age 53 ( the average age * of all the patients referred to in table ii ) the relative risks of developing the disease when circumcision is carried out at the mid - points of shrek and lenowitz 's ( 1947 ) age periods are 0 - 30 , 0 - 77 , 0 - 98 and 1 - 00 ( see mathematical appendix )  . children circumcised during the first six years of life are , however , most likely to have been operated on within the first few weeks , in which case the theoretical risk for this group would be of the order of 0 - 01 . 
on the other hand , u the present data were held to be equally accurate at all ages ( including the oldest ) it would be possible to obtain a quite different mathematical relationship . thirdly , other mechanisms than that of a multi - stage process can also be postulated to account for the observed relationship - and one has , in fact , been suggested by fisher and hollomon ( 1951 )  . moreover , some other diseases show similar types of increase with age ( e.g. , cerebral haemorrhage , coronary thrombosis and gastric ulcer ) and it is difficult to believe that they should all be dependent on the same type of mechanism . bereilblum and shubik ( 1949 ) , in summarizing the results of their experiments , have , however , stated that " whatever interpretation is adopted as a base line for research , the recognition that careinogenesis is at least a two - stage process , should invariably be bome in mind "  . it is , therefore , natural to see whether a twostage process - or even a more complex multi - stage one can account for the human data . 
from the analysis that has been made here , it would seem that a complex process of perhaps six or seven stages could account for : sites , and ( 1 ) the rapid increase in mortahty with age observed in cancer of some ( 2 ) the irregularity in the increase in cancer of some other sites ( 3 ) the long latent period observed after exposure to a carc ' mogen ( 4 ) clinical observation . 
doll the mortality rates for cancer of the lung , bladder and prostate in men and for cancer of the lung , breast , ovary and cervix and corpus uteri in women also accord with the theory , if it is postulated that the carcinogenic factors responsible have varied in strength . a formula has been obtained which can be used to weight the strengths of the carcinogenic factors at different periods and it is shown that the time when the strength of the factors responsible for the individual changes is of greatest importance varies according to which change in the series is affected . 
the conclusion provides a possible explanation for the observation that circumcision exerts an important protective effect against the development of cancer of the penis only if it be carried out early in life . we are most grateful to r . 
more precisely , we assume that the probability that the sth change occurs in the small interval i changes have already occurred , is p , ( to ) dto where ( tw to + dto ) , given that s all the other p 's are assumed to be constant . 
then p , ( to ) is a function of to . the probability that the sth change occurs in the interval ( to , to + dto ) , and the rth in the interval ( t , t + dt ) , is the product of ( i ) the probability that exactly s i changes occur in the interval  . 
we shall ignore the variation in age amongst the patients , and consider the expected incidence of penile cancer at t = 53 years ( the average age of all the patients referred to in table ii )  . 
3. received for publication february 6 , 1947 . following the discovery by haddow and sexton ( 1946 ) of the effects of ethylcarbamate ( urethane ) on the growth and differentiation of the walker rat carcinoma , the action of this substance in human leukaemia was described by paterson , apthomas , haddow and watkinson ( 1946 )  . since the early experiments of warburg in 1910 , ethylphenylcarbamate ( phenylurethane ) had been known to arrest the division of the sea - urchin egg at metaphase . 
a similar effect in plant cells , closely resembling that of colchicine , was discovered in 1939 by lefevre and by simonet and guinochet ( 1939 ) , and was further studied by gavaudan ( 1943 ) and deysson ( 1944 )  . ludford ( 1936 ) treated tissue cultures with a 2 per cent solution of ethylcarbamate and noted abnormal metaphases and a considerable amount of nuclear and cellular degeneration . similar results were obtained by geiersbach ( 1939 ) , and ostergren ( 1944 ) also claimed that ethylcarbamate arrested mitosis at metaphase in alliutempleman and sexton ( 1945 ) , investigating the growth - inhibiting properties of numerous carbamic esters in plants , found , however , that ethylcarbamate was inactive in this respect , although marked activity was shown by ethyl phenylcarbamate and it was this work which led haddow and sexton isopropyl phenylcarbamate . to investigate the action of carbamic esters on tumour growth , and to the discovery that in this case ethylcarbamate itself is effective . these authors suggested that this substance might belong to the group of caryoclastic ( nuclear ) poisons studied by a . 
described by gorer ( 1946 ) was utilized , in which large stem - cells produced a diffuse infiltration of lymph nodes , spleen , liver and kidneys , leading to death of the mice in from 14 to 22 days after subcutaneous grafting of leukaemic tissue . enumeration of reticulocytes was made from dry blood smears , following postvital staining with * associe du fonds national belge de la recherche scientifique . 
the nucleus then disintegrates , the thymonucleic acid material forming shell - like structures covering an acidophil sphere , which also contains some ribonucleic acid ( by the further destruction ribonuclease method ) and the remnant of the nucleolus . leads to irregular fragments , with a positive or negative feulgen reaction . 
52 and within 3 days the number of reticulocytes was close to the initial value . no significant change in the numbers of red blood cells , or in the leucocytes , was observed . these results may be compared with those following the injection of colchicine , when the reticulocyte fall is marked and the minimum is also reached in 48 hours . 
the erythroblastic mitoses are arrested in metaphase by colchicine during the first hours following its injection , and the delayed decrease of the number of reticulocytes is a consequence of the time needed for the maturation of the erythroblasts . 
by comparing the histological pictures found in these last two groups it is possible to appreciate the specific effects of ethylcarbamate . ( ii ) blood - picture . - the principal changes were an increase in the percentage of granulocytes and a decrease in the numbers of reticulocytes . 
no evident atrophy of the mucosa , nor ulceration . leukaemic infiltrations : no evidence of increased cell - destruction nor mitotic abnormalities . in animals losing weight during the experiment , splenic and lymphoid atrophy is more pronounced . 
the bone - marrow remains very cellular , with a there is no evidence of aplasia . high proportion of immature granulocytes . in the thymus the atrophy of the cortical region is complete , the epithelial cells this picture of " inverted thymus " is found after the pycnotic only remaining . destruction of thymus cells by mitotic poisons ( dustin , 1929 ) or non - specific in this case it is probable that the stimuli ( selye , 1937 ) , and in inanition . ethylcarbamate injections and the loss of body weight have additive effects . no marked changes are found in other organs . * rosin and doljanski ( 1944 ) have described inclusions in liver cells of rats treated with urethane , which they believe are red blood cells engulfed in cytoplasm and even in the nucleus . 
for 5 days , there was an increase in leucocytes from 9200 to 22 , 800 , and in granulocytes from 33 to 58 per cent . the bone - marrow showed very active granulopoiesis . bring about any aplasia of the bone - marrow in the rabbit . these preliminary results indicate that large doses of ethylcarbamate do not 2 . 
the possible relations between mitotic poisoning and the therapeutic action of ethylcarbamate in human leukaemia are discussed . this work has been supported by grants to the royal cancer hospital ( free ) from the british empire cancer campaign , the anna fuller fund , and the jane coffin childs memorial fund . 
kirby , research department , glasgow royal cancer hospital . received for publication march 4 , 1948 . althoulgh the claims of roffo ( 1938 , 1939a , 1939b , 1941 ) to have induced adenocarcinoma of the stomach in rats given orally fats or cholesterol which had been heated to 3500 c . 
for half - an - hour have not been confirmed ( beck and peacock , 1941 ; kirby , 1943 , 1944 , 1945 ; morris , larsen and lippincott , 1943 ) , the positive results obtained by other routes in mice by other workers make a good case for regarding the products of such pyrolyses as carcinogenic . thus beck ( 1941 ) found sarcomas in 2 of 12 mice at the site of injection of cottonseed oil , previously heated to 340 - 360 c . 
for 1 hour , and steiner , steele and koch ( 1943 ) reported sarcomas in 3 of 9 mice injected with sesame oil heated to 3500 c . these latter workers found no tumours in similar mice injected with cholesterol that had been heated to 2000 c . 
for half - an - hour , and another sarcoma in 1 of 9 mice surviving more than 340 days after subcutaneous injection with a residue left after removing dicholesteryl ether and a4cholestenone from cholesterol heated in the same way ; these tumours were closely associated with the sites of injection . negative results were obtained by these workers when mice were injected subcutaneously with cholesterol that had been heated to 4300 c . 
of the remaining 14 , 5 died or were killed between 400 and 500 days , 1 was killed at 533 days , 1 died and 2 were killed between 500 and 600 days and 3 were killed at 735 days . bronchiectatic abscesses were found in most animals surviving 400 days ; there was no other frequent lesion . 
the stomachs were all normal , save for that of a rat dying after 616 days which had the haemorrhagic erosions of the glandular zone commonly found in rats in a state of inanition . 
shortly after the paintings had been commenced , 0 5 per cent of croton oil was added to the benzene solution in the hope of speeding up or enhancing the action of any carcinogen present in the c.o.h. after 258 days ' experimentation , a 15 per cent benzene solution of c.o.h , containing 0 5 per cent croton oil , replaced the original 10 per cent solution ; 2 males and 5 females survived long enough to be treated with the stronger three other male mice were painted with the 10 per cent - solution solution . for 168 days and then with the 15 per cent solution . atrophic changes at the site of painting were seen in mice dying at 80 days after the beginning of the experiment , but even in 2 females painted 258 days with the 10 per cent solution and then 374 days with the 15 per cent solution , and surviving totals of 640 and 656 days respectively , no further lesion was found . fourteen mice showed fatty changes in the liver , sometimes with extensive necrosis , but no hyperplastic changes were seen in this organ . 
the first mouse to die survived 80 days after the first injection ; 2 others died before 100 days , 10 survived 100 to 200 days , 2 from 200 to 300 days , 2 from 300 to 400 days , 5 from 400 to 500 days , and 1 survived 518 days . a mild histiocytic reaction was seen around sites of injection , but no sign of fatty changes in the liver were rare , but in mice any tumour was ever found . dying at 126 , 130 and 384 days after the first injection there were leukemic changes involving the liver and spleen in the first , the liver in the second , and the liver , spleen , kidney and lungs in the third mouse . ( c ) cholesteryl linoleate ( heated ) in mice . linoleic acid was prepared from cottonseed oil ( organic syntheses , 1942 ) and converted to the acid chloride by refluxing with oxalyl chloride . purified cholesterol was heated with linoleyl chloride on the water - bath for 3 hours , and purified as for the oleate . 
in the left flank , 31 days after the injection in the other flank . eight mice survived 100 to 200 days after the first injection , 1 for 247 days , 1 for 357 days , 2 for 470 days , 1 for 509 days , 1 for 558 days and 1 for 653 days . at the site of injection nothing beyond a mild histiocytic reaction was found in any mouse . 
and the time was 2 hours . as the esters were prepared by a non - pyrolytic method and were subsequently purified till non - fluorescent , any polycyclic hydrocarbon present in the residue after heating would have arisen as a direct result of the heating . 
no chemical experiments have been made to determine the nature of the components of the but the biological tests reported here gave no evidence of carcinoresidue . genicity in these residues for the skin or subcutaneous tissues of stock mice . such tumours as did arise in the mice used were almost certainly spontaneous . damage to the liver and the spleen was frequent , and the occurrence of leukemic infiltration was significant and probably attributable to the injections . it now seems that cholesterol and its naturally occurring esters may not be an important source of carcinogens in heated food . 
the results of the experiments described in this paper lend no support to the results reported by beck , kirby and peacock ( 1945 ) , who administered cholesterol heated to 3000 c . 
for the same period , as recorded by those authors , also of the negative findings of steiner , steele and koch ( 1943 ) with cholesterol heated to 2000 and to 300 c . 
it is concluded from this work and from other reports in the literature that cholesterol and its esters heated to reasonable dfooking temperatures for a reasonable cooking period have not been proved to yield carcinogenic residues . the author is indebted to p . 
no definite conclusions were obtained with regard to the influence of the thyroid gland , but the results showed a remarkable reduction of mammary cancer in one of the two strains used . preliminary experiments ( vazquez - lopez , 1946 ; morris , dubnik and dalton , 1946a , b ) showed that thiourea ingestion produced a continuous anoestrus due to ovarian atrophy and the consequent underdevelopment of the mammary glands . 
vazquez - lopez breeding females only were used from the two lines of r3 mice , and both breeders and virgins from the c3h strathe breeders were allowed to rear their first litters and , after weaning , the mothers were taken for the experiment . the litters of the c3h breeders provided the majority of the virgins employed . in all groups care was taken to divide animals of the same litters between the experimental and control groups . the animals were housed in metal boxes , 6 to 8 in each , and fed rat cubes breeders and virgins of the c3h strain were separated , but and water ' ad lib . the two lines of r3 breeders were mixed together . thiourea was administered in the drinking water , beginning with a 0 1 per cent solution and increasing the concentration as much as possible without endangering the survival of the animals . 
the approximate amount of fluid ingested was determined by dividing the total content of the water bottles by the number of animals in the box . all the animals were individually marked . 
the age of the breeders at the beginning of thiourea ingestion was between 3 and 4 months . the virgins were 3 months old , so that the mammary gland was fully developed before the action of the drug started . the period of administration for some of the r3 animals was a year , so that most of the animals with tumours died during the period of ingestion . for the c3h mice , both breeders and virgins , it was 6 months , so that the animals were under normal conditions again when 9 or 10 months old . 
even concentrations of 1 per cent could be used before the mice showed toxic signs such as loss of weight and reduction of water intake . if the solutions were kept between 0 - 2 per cent and 0 * 5 per cent the r3 mice could be maintained for most of their lives without any apparent difference from the controls . 
per animal per day , and if the concentration of the drug was not reduced , many it was possible to reach a concentration of 0 5 per cent in most animals died . boxes , but it could be maintained only for one or two weeks . solutions of 0 - 2 and 0.1 per cent were used most of the time , and even with these doses the intolerance to the drug and mounting mortality necessitated the withdrawal of the after some days without thiourea the mice recovered drug after 4 or 5 months . and the drug could then be administered again , but the recurrence of toxic it was preferable to maintain the 6 months ' period without symptoms was rapid . interruption , even at the risk of losing more animals in the last months of treatment . the doses administered were therefore variable for the different animals and for different periods for the same animal , but from the approximate estimate of water intake it may be assumed that the minimum of thiourea ingested per day was between 2 and 3 mg . 
daily. effects on the thyroid gland . in the r3 mice the ingestion of thiourea provoked the typical hypertrophy this effect was and hyperplasia with great vascularity , loss of colloid , etc . evident even with a 0 - 2 per cent solution , and became more pronounced in proportion to the length of treatment and increased concentration . 
the mice surviving after the withdrawal of the drug had thyroids of normal size and structure without any signs of the former hyperplasia . the effects of thiourea in c3h mice were observed in the experimental animals that died during the period of ingestion of the drug . 
as the great majority of these mice restricted their water intake to a minimum in the weeks before their death , it could be argued that they were not actually under the action of the for this reason additional mice not included in the experiment were used drug . to test the effect under identical conditions , and were killed when the actual ingestion of thiourea was known . in all the 03h mice of the experiment the results of the examination of the thyroid gland were similar . thiourea administered in the drinking water did there was clearly not produce hyperplasia or hypertrophy of the thyroid . congestion of the organ which might cause a slight increase in size , but the histological picture remained normal , showing follicles filled with colloid and lined by cubic epitheliunone of the mice that died during the period of thiourea ingestion showed changes in the microscopical picture . 
among 20 additional female adult mice killed after drinking solutions of 0 - 2 to 0 5 per cent for periods of a week to 2 months , with actual ingestion of about 5 mg . 
the small difference in favour of the thiourea group was not significant , for the small number of animals and the lower tumour age of this group was also against any inhibitory effect of thiourea . all the tumours appeared during the period of treatment when some of the mice had received thiourea for 10 months without interruption . mammary cancer in c3h breeders . - of 49 mice at the start of the experiment , only 29 ( effective number ) reached the age at which the earliest tumour appeared . the other 20 died as a consequence of thiourea ingestion . eight of the 29 table i . - lymphoma incidence in r3 breeding female8 ( mh subline )  . total effective mice with number . 
the earliest developed in a mouse 367 days old , 80 days after the withthis was only 10 days less than the average tumour age drawal of thiourea . these figures confirmed the assumpfor the control group , which was 377 days . tion that ovarian function and mammary development were normal in the experimental animals at the average tumour age of the normal mice . in spite of these normal conditions the percentage of mammary cancer in the thiourea - treated mice was 28 per cent compared with 54 per cent for the controls . 
vazquez - lopez mammary cancer in c3h virgins . - twenty - one animals died during the period of thiourea ingestion , and 64 mice survived the 6 months of treatment and five among the 64 reached the period of appearance of the first tumour . in the developed marmmary cancer ( 8 per cent ) , at the average age of 571 days . control group 40 out of 96 animals ( 43 per cent ) developed tumours at the average age of 432 days . 
the animals treated were 270 days old when thiourea was withdrawn , so that ovarian activity and mammary gland development were presumably normal not only long before the average tumour age of the controls , but also very nearly when the first tumour appeared among the normal mice . 
assuming that after the end of thiourea administration the mice needed a month for total recovery , they would be comparable with the normals when 300 days old . only 4 mammary cancers developed in the control group below this age . the decrease in cancer incidence in the thiourea - treated virgins was highly significant ( x2 = 20 9 ) , and confirms the results in c3h breeders . in this group the average tumour age was also later than in the controls . 
the average life span of mice without tumours was longer , but with smaller differences from the control mice than in the breeders . microscopical study of organs in thiourea - treated c3h mice . a detailed study of the organs of c3h mice after longer periods of thiouracil and thiourea ingestion was published by dalton et al . 
1 and 2 show condition and weight of the mouse rather than with its age . glands of control and experimental mice of approximately the same age . the two main differences between thiourea - treated and control mice are the number of nodules of alveolar hyperplasia and the width of the ducts . 
the alveolar nodules of one gland or even of all the glands in a single mouse cannot be used to distinguish a thiourea - treated from a control mouse ; in some thioureatreated animals the number and distribution of nodules is the same as in the controls . 
the thiourea - treated mice , as a whole , had considerably fewer nodules of alveolar hyperplasia than the control mice , and the average number of nodules per mouse was less than half the figure for the controls . there are no records of comparative counts in similar experiments with reduced mammary cancer incidence , but huseby and bittner ( 1946 ) report that less than 1 nodule per 4 glands was found in some animals more than 340 days old kept on the restricted diet in the experiments of huseby et al . 
vazquez - lopez to indiscriminate reduction affecting equally all the glands of each animal , but to a clear decrease of the number of glands with ' nodules . only 32 per cent of the glands in the thiourea - treated mice had nodules compared with 51 per cent in there were also significant differences in the distribution the control group . and the average number of nodules for glands in each group , but the main effect of the thiourea administration is to increase the number of glands without any nodules . 
as the hormonal and systemic influences are the same for all the mammary glands in each mouse the cause of these differences between glands in the same mouse must be the result of local factors whose activity is restricted to the fields represented by particular glands . thiourea acts systemically mainly by stopping ovarian function and oestrogen production . 
at the post - mortem examination the ducts appeared full of whitish material , which made them conspicuous to the naked eye . it seemed therefore to be due to engorgement by a secretory product , but it could exist in glands without any indication of alveolar proliferafig . 
some ovaries appeared in regressed condition without corpora lutea or follicular development ; this occurred with the same frequency in both groups . most ovaries had follicles in all stages of development , and some of the corpora lutea became hyalinized , forming large homogeneous masses with few cells . this formation of corpora albicantis is probably a strain characteristic , since fekete ( 1946 ) found them in the dba high cancer strain , but never in the c57 black strahuseby et al . ( 1945 ) found them only in one c311 mouse with mammary - cancer , and in none of the diet restricted animals of their experiment . that is probably another of the characteristics in which the c3h mice used here differ from those in american laboratories . 
the corpora albicantis were very prominent among the cancerbearing animals , and their ovaries owed their large size partly to these structures . apart from their size , however , the ovaries of mice with tumours showed mature follicles and abundant corpora lutea , which suggested normal activity . these findings were contrary to the results of allen , diddle , strong , burford and gardner ( 1935 ) in several strains of mice , including the c31 . in all groups the condition of the uterus reflects that of the ovaries having tall epithelium , extensive glandular development and loose cellular stroma in the animals with well functioning ovaries and signs of regression in those with ovarian atrophy . no differences were found in the adrenal glands of thiourea - treated mice compared with the controls . 
the most important change , affecting both groups equally , was the presence of amyloid degeneration , which appeared on the borderline between cortex and medulla and progressed towards the glomerular zone with advancing age . in the oldest animals amyloid invaded most of the cortex , and only two or three layers of cortical cells remained intact . 
the medulla was never affected . " brown degeneration " was , on the contrary , never found in c311 mice , but was almost constant in r3 animals of high or low mammary cancer lines . 
the possibility of a specific activity of thiourea on blood - forming tissues and their neoplasms suggested by the agranulocytic reactions in patients treated with goitrogenic substances is not supported by the results in the mh high lymphoma line which agree with clinical reports of treatment of leukaemic patients ( limarzi , kulasavage and pirani , 1946 ; hansen - pruss , 1947 )  . that lack of oestrogen is the effective factor is shown also by the normal incidence of cancer corresponding with regular oestrus in spite of thiourea administration in r3 mice . 
the action of progesterone is still a matter for discussion ( lacassagne , 1937 ; heiman , 1945 ; burrows and hoch - ligeti , 1946 )  . indirect ways of decreasing oestrogenic activity give , however , less clear results . although low cystine diets completely inhibit mammary cancer in c3h mice ( white and andervont , 1943 ) , the effects of stilboestrol pellets which restore the development of the mammary glands raise the incidence only to 44 per cent compared with 92 per cent in the controls ( white and white , 1944 )  . in similar experiments , ball , huseby and visscher ( 1946 ) found that in spite of continuous administration of stilboestrol the mammary glands of strain a mice maintained on restricted diets during 15 months were considerably less developed than those of control mice . 
the possibility of other hormonal factors influencing mammary cancer development is also suggested by the results of shimkin and wyman ( 1945 ) , who found greater reduction in adrenalectomized c3h mice than after ovariectomy , and by the observation of wallace , wallace and mills ( 1945 ) of persistence of effects of temperature in mammary cancer incidence after ovariectomy . the results of temporary lack of oestrogenic activity caused by thiourea show that reduction of mammary cancer is not due to defective glandular development , and therefore that the hormonal effects are not limited7 to the morphogenesis of tissue susceptible to carcinogenic agents . 
mammary glands of two groups of mice of the same strain with different cancer incidences have identical morphology , and only differ in the total number of nodules ofalveolar hyperplasia in each group . 
huseby and bittner ( 1946 ) have shown by the study of c3h and hybrid mice with or without the " milk influence " that this influence is necessary for the presence of nodules . 
the distension of ducts found also in the thioureatreated group seems to be a sign of excessive oestrogenic stimulation , and may indicate compensatory excess after thiourea withdrawal . if the hormonal influences are sufficient for the alveolar development the smaller number of glands with nodules , which is the main result of thiourea administration , must be due to local factors . 
the lack of oestrogens ( and its possible compensation afterwards ) affects all the glands of the mice equally . these results point to the possibility of effects on local factors and producing different consequences in each gland of the same animal . 
the local factor involved in the persistence of alveolar nodules is the milk factor , and the distribution of nodules suggests that it is affected by thiourea administration . there are no grounds for supposing that thiourea can directly influence the milk factor , but there are some in favour of an indirect action resulting from the lack of oestrogens . apart from the considerable number of experiments on the effects of oestrogen adninistration on cancer incidence , there is evidence even in normal circumstances of hormonal influences in breeding and forced breeding , increasing the number of tumours . 
the higher incideixce in mice born in later litters compared with the earliest from the same mother has been explained by the different concentration of the milk influence with advancing age ( bittner , 1942a )  . if the increased hormonal stimulation is the cause of increase in the amount or activity of the milk influence , it is probable that the converse holds true also , and that the lack of hormones acts in the opposite sense . the relative importance of the hormonal influence among the three factors necessary for the genesis of spontaneous mammary cancer in mice is not exactly opinions range * from that of shimkin and andervont ( 1941 ) , who known . consider the hormonal factors as necessary only for the creation of a substratum for the carcinogenic action of the factor transmitted by the milk , to that of warner , reinhard and goltz ( 1945 ) , who maintain the dominance in certain cases of the inherited susceptibility upon the concentration of the milk agent . loeb , suntzeff , burns and schenken ( 1944 ) believe that the oestrogens act by stimulating the growth of the mammary tissue and sensitizing it to all types of stimuli , and bonser ( 1945 ) as a developing factor acting upon breast tissues already sensitized by the milk factor . 
the only common feature of all these opinions is to consider the different factors as completely independent variables . on this basis the opinion of bittner ( 1942b ) that each influence must be considered as complementary to the others and all equally important is , besides being noncontroversial , nearest to the observed facts . 
but if there are some factors which are affected and increased , or even created de novo by interaction of the others , the relative significance of each would not be the same . the effect of genetic susceptibility on some aspects of the milk factor activities has been already proved by heston , deringer and andervont ( 1945 )  . 
w.3. received for publication july 16 , 1949 . in an investigation of the body growthand tumour growth - inhibiting action of carcinogenic substances , it was found that the nature of the inhibition is profoundly influenced by the protein content of the diet ( elson and warren , 1947 ; elson and haddow , 1947 ; elson , 1949 )  . in rats maintained on a 20 per cent protein diet injection of the carcinogen usually has little immediate effect on body growth although a delayed action , resulting in rapid loss of weight followed by death , may occur later . 
carcinogenic hydrocarbon 1 : 2 : 5 : 6 - dibenzanthracene 24 hours after implantation of walker carcinoma 256 in rats maintained on a 20 per cent protein diet results in very little difference in size and weight of the tumours from those of controls . if , however , the animals are fed a 5 per cent protein diet the tumours of those similarly treated with dibenzanthracene were found to be only one - quarter the weight of those of controls when the rats were killed 13 days after implantation ( elson and haddow , 1947 )  . 
hewitt. from the john burford carlill laboratories , westminster hospital , london . received for publication may 26 , 1953 . in a previous paper ( hewitt , 1953 ) a method for the preparation and titration of single - cell suspensions of sarcoma 37 was described . 
each mouse received 4 subcutaneous inoculations of the appropriate cell dose , one in each axilla and one in each grothe new - born mice were allowed to remain with their mothers throughout the experiments . 
1 the points plotted represent the percentage incidence of palpable tumours from inocula containing various numbers of viable tumour cells ( expressed logarithmically ) calculated from the cell count of a dense suspension and the dilution factor . the points shown were obtained from the data of various experiments . although the points are insufficient in number and accuracy to disclose the true character of the curve relating log . 
cell dose and tumour incidence , they serve to show the general trend of the relationship . litters born to mothers which had been rendered completely resistant to s37 by their having regressed a tumour before pregnancy ensued gave results which did not depart appreciably from those indicated in the graph . the td50 , read from the graph , is approximately 9 viable tumour cells . this figure is less than that obtained for the titration of c3h sarcoma in c3h mice over one year old , that is , 18 viable cells . certain technical difficulties have the effect of reducing the observed percentage of tumours obtained from specified cell doses below the maximum value . 
owing to the fact that the tumours which form in the suckling mice quickly reach a size which jeopardises health and movements , some animals die with tumours in 2 or 3 of the inoculated sites before all sites have been observed for a sufficiently long period to exclude tumour formation in thethe incidence of tumours recorded for any group thus tends to be submaximal . 
a further difficulty is that a proportion of each inoculum volume often exudes from the needle track after withdrawl of the needle . cell counts and volume measurements of the exuded fluid have shown that a quarter or more of the inoculated cells are lost in this way . if these known errors were to be eliminated , the points in the graph would be shifted slightly upward and to the left of their present positions , and the td50 would be rather lower than is obtained from the results as they stand . the effect of the diluent on the activity of sarcoma cells in dilute suspensions . craigie ( 1949 ) , discussing various technical requirements for the quantitative transplantation of tumour cells , drew attention to the inimical effects of various 386 h . 
hewitt in a later paper ( craigie , lind , diluents upon the viability of tumour cells . hayward , and begg , 1951 ) an account was given of certain atypical cells which composed about 5 per cent . 
the number of various mean doses of viable 837 cells . beside each point is the number of sites inoculated at that dose level . diluents in which inoculated cells were suspended : o tyrode solution . a , 0 5 per cent gelatine in tyrode solution . * 33 per cent mouse aacitic fluid in tyrode solution . a 10 per cent ascitic fluid in tyrode solution . the suspensions used to obtain the points shown in fig . 
the order of inoculation was so arranged that the interval elapsing between the time of preparation of the dilute suspension and the average time at which the mice of any litter were inoculated was equal for all the litters . 
hewitt quantitative transplantation of s37 in mature mice of different age - groups . a single - cell suspension of s37 was titrated in three series of mice , all from the same albino stock that provided the new - born mice and belonging to the following age - groups : 18 - 25 days ; 143 - 174 days ; 268 - 296 days . 
the incidence of palpable tumours in the inoculated sites was recorded for a period of 27 days following inoculation . in table i the td50 value given by each series is given together with its limits of error . 
the difference between the youngest and the oldest mice is not significant , but the td50 given by the oldest mice is considerably lower than that given by the mice of interthis last different , however , does not attain a significant level by mediate age . the irwin and cheeseman ( 1939 ) test . 
the systemic mechanisms by which resistance is manifested are cellular and humoral . in the case of resistance to tissue grafts , it appears that cells primarily are concerned in the resistance mnechanisms ( murphy , 1926 )  . 
young mice would therefore not be expected to possess resistance against a homologous tumour by virtue of maternal serum factors reaching them by the transplacental route before birth or by the colostrum after birth . in the course of the present studies it has been observed that a litter from a mother which was completely resistant to s37 , a tumour having regressed in her before pregnancy ensued , showed the gross developthe same high susceptibility as the litters of normal mothers . ment of the lymphatic system appears to be quite advanced in new - born animals as indicated by the presence of the thymus and by the existence of lymphocytes if it is assumed that the lymphocyte is responsible for tumour in the circulation . immunity , then the low resistance of new - born mice must be ascribed to functional immaturity of the lymphatic system . the td50 given by the titration of s37 in new - born mice , as will be seen fronm the trend of the points shown in the fig . 
1 , is about 9 viable sarcoma cells . graph suggests that the percentage of tumours to be expected from an average it is of interest to note that furth and inoculum of 1 viable cell is about 7 . kahn ( 1937 ) succeeded in transplanting leukaemia to about 5 per cent . 
kahn and furth ( 1938 ) obtained only about 20 per cent of tumours from subcutaneous sites inoculated with 50 - 100 viable sarcoma cells in circumstances where there was no genetic difference between the animal in which the tumour arose and those to which it was transplanted . 
a c3h sarcoma gave a td50 of 18 viable it is evident from tumour cells when titrated in old c3h mice ( hewitt , 1953 )  . these comparisons that the results of quantitative transplantation of s37 in newborn mice of a heterogeneous strain of which the adults exhibit some resistance to small inocula , are compared with those obtained for similar tumours within a genetically homogeneous tumour - host systethe use of new - born mice therefore provides a more uniform and more sensitive system for the detection or assay of viable tumour cells in circumstances where , owing to limited facilities or to the use of genetically unknown tumours , a genetically homogeneous system cannot be achieved . it will be seen from fig . 
2 , however , that quantitative resistance increases this being so , it is likely that very differperceptibly within the first week of life . ent quantitative results would be obtained from the titration in new - born mice of tumours with a slower growth rate than s37 . in these circumstances resistance factors could produce their effects before the tumours became palpable . 
a lymphoma which occurred spontaneously in a mouse of the albino strain used in these experiments gave a td50 of over 10 , 000 viable cells when titrated in newborn mice ; krebs ' carcinoma ascitic cells gave a td50 of over 2000 viable cells . it must be concluded from the results of titrating s37 in new - born mice that the high td50 levels obtained in adult mice of the same stock ( i.e. , about 1600 ) were due to immunity factors and not to intrinsic limitations of the proliferative power of the cells . an estimate can be made of the proportion of inoculated s37 cells which are capable of continued proliferation if it is assumed that such cells are not subject to any hazard affecting their proliferation once they have been successfully in these circumstances the dose - response curve deposited in the host tissues . would represent the chances of getting one or more " taking units " in random samples ( inocula ) taken from suspensions containing different mean densities of 390 h . 
1 , a suspension which gives 37 per cent of negative sites ( 63 per cent of takes ) contained a mean density of about 17 tumour cells per inoculum , and this evidently constitutes a single " taking unit . " thus , when it is assumed that there are no influences at the inoculated site which inhibit continued proliferation of a cell intrinsically capable of giving rise to a palpable tumour , then the results reported indicate that such cells are present in a proportion of about 1 : 17 ( 6 per cent ) of the population of cells designated as living s37 cells on the grounds of their resistance to staining with trypan blue the frequency with which abnormal mitoses and and their diameters ( > 9 , )  . cellular pleomorphy are found in rapidly growing tumours would seem to indicate that there may be a continuous production of cells which , though alive , are various observations have been intrinsically incapable of indefinite proliferation . fischer ( 1935 ) was unable to cultivate made which suggest that this is the case . solid s37 in vitro , and concluded that dying cells exceeded living cells in this lasnitzki ( 1952 ) found that the majority of s37 ascites cells failed to tumour . she found also that one - third to two - thirds of the mitoses seen divide in vitro . since it is unlikely that all mitotic in the ascitic cells in vivo were abnormal . abnormalities are visible , it is possible that the proportion of mitoses which are koller and smithers ( 1946 ) give experiabnormal in vivo may reach 50 per cent . mental proof that loss of chromosomes or of chromosome segments leads to the death of the cell . 
on the other hand , there is evidence that cells with a defective chromosome complement may survive and divide under conditions where contiguity between the cells is preserved , while being unable to do so when isolated these considerations favour the assumption from one another ( koller , 1947 )  . that a significant proportion of the s37 ascitic cells are unlikely to be capable of furthermore , if the cells should indefinite proliferation and tumour formation . be dependent upon one another for a stimulus to divide , dilution may reduce the proliferative power of an inoculum , not by damaging individual cells , but by abolishing essential mutual influences between the cells . 
quantitative transplantation of s37 in new - born mice of a heterogeneous strain gave results similar to those obtained for the transplantation of a c3h sarcoma in adult c3h mice . 
fodden. from the department of pathology , university of liverpool , and the liverpool cancer control organization . received for publication august 20 , 1948 . in his ' textbook of pathological anatomy ' rokitansky ( 1861 ) made his classical statement that pyloric cancer was exactly bounded by the pyloric ring , and that the growth never reached beyond into the duodenufrom this time it appears that the majority of observers , with the early exception of brinton ( 1864 ) , commented upon the integrity of the duodenum in cases of carcinoma of the stomach . 
many well - known surgical teachers spoke of the habitual immunity of the duodenum from invasion . kocher ( 1893 ) , mikulicz ( 1898 ) and most ( 1899 ) believed it to be always constant . kocher ventured that it was a problem of extreme interest to consider why gastric carcinoma grows in almost all cases towards the cardia , yet stops , on the contrary , at the duodenopyloric junction . it was brinton who first took especial exception to this proposition of rokitansky . 
he brought against it criticisms founded upon numerous personal caseobservations : " we may justifiably apply to it a criticism of unusual severitya criticism which , even if it weigh every word , will scarcely do more than the author 's ( rokitansky 's ) terse and weighty proposition really deserves . " from 125 cancers of the pylorus studied by brinton , there were no less than ten cases in which the disease was not bounded by the valve , but passed beyond it for a variable distance , often an inch or two inches , into the duodenuhe gave no information concerning the method of this spread . brinton concluded by saying the rules which rokitansky had the merit of laying down were , in this respect , like many others in pathology , of general though not of universal importance ; their value was not much affected by occasional exceptions . this question of duodenal invasion by pyloric cancer seemed to present a surgical problem of out of a large series of gastric carcinoma cun6o ( 1903 ) took 11 j . 
fodden some magnitude , and the frequency and degree of its occurrence has been the object of several subsequent researches . carle and fantino ( 1898 ) , discussing the pathology and treatment of carcinoma of the stomach , expressed disagreement with kocher . they mention three cases out of fourteen gastric resections in which neoplastic infiltration had spread under brunner 's glands for a distance of one to three centimetres . in addition , these authors stated that such a progression of the growth towards the duodenum necessitates an extension of the surgical resection as far as the second part of the duodenum . other later surgical authors , notably borrmann ( 1901 ) and cuneo ( 1903 ) , attached considerable importance to brinton 's " occasional exceptions " with reference to the spread of cancer into the duodenum . cuneo ( 1900 ) , during his classical work on the lymphatic propagation of pyloric cancer , was already investigating the accepted state of immunity of the duodenuhe remarked on the disaccord between the macroscopic aspect - the abrupt termination of a gastric cancer at the level of the pylorus and the results of the histological examination . this examination systematically diminished , he said , the percentage of the duodenal integrity . cancers of the pylorus , and subjected their distal extension to a critical macroscopic and microscopic examination . 
but , he goes on to say , it is impossible to ignore the fact that such a wide resection complicates the operation , and necessitates a dissection of the duodenum from the pancreas . the researches of fenwick and fenwick ( 1902 ) do not lend support to brinton 's findings , as they discovered out of a series of 87 pyloric cancers only 2 cases which demonstrated lymphatic spread into the duodenum . these authors remarked that though malignant growths of the pylorus may project into the lumen of the duodenum , they rarely implicated its walls . however , it is open to question whether their histological investigations were sufficiently careful to give reliable evidence , and the conclusions they advanced could scarcely have been founded upon their own results . moynihan ( 1926 ) was very familiar with the possibility of duodenal permeation in gastric cancer , and stressed that the duodenal integrity was more apparent than real . 
he quoted several of the authors already mentioned , and advocated the removal in all cases of pyloric cancer of the whole of the first portion of the duodenum . sherren ( 1932 ) , describing the methods of spread of gastric cancer , mentioned his own surgical familiarity with duodenal infiltration by carcinoma . 
a study of the microscopical anatomy of this region , in relation to the morbid process in situ , may help to clear up some components of each problem . to cun6o ( 1900 ) the apparent arrest of a cancer at the pylorus was due , for him it depended upon an absence of conabove all , to a mechanical cause . tinuity between the gastric and duodenal submucous spaces - a continuity broken by the annular muscle of the pylorus , and by a condensation of cellular tissue within the submucosa to form a dividing septum . his gelatine injections into the gastric submucosa near the pylorus met with an " invincible obstacle . " at the same time he admitted that though it would be ludicrous to consider such barriers as absolute in opposing gastric cancer , they still played the principal role in the protection of the duodenum against neoplastic invasion . for brinton ( 1864 ) and for fenwick and fenwick ( 1902 ) the reason was again anatomical . 
the muscular coats of the two viscera along the line of fusion were so distinct from one another that a direct continuity could scarcely be said to these authors made the analogy between the duodenal attachment to exist . the stomach and the manner in which the vagina embraces the neck of the uterus . to them a growth of the pylorus was more apt to infiltrate the contiguous walls of . 
in their opinion it was obvious that the duodenum may possibly be invaded from the pylorus by the in addition , extension of cancer along the submucous and subserous channels . both jamieson and dobson and cun6o emphasized the final possibility of retrograde lymphatic spread . 
as these nodes also receive vessels from the that this may be of some duodenum , an indirect communication also exists . importance was stressed by moynihan ( 1926 ) when he says that the implication of a single gland may so sufficiently disturb the direction of the lymph current that cancer cells from a primary growth may pursue an erratic course . horton ( 1928 ) working upon stomachs removed from young subjects one to three hours after death , injected 35 with coloured gelatine or indian ink . 
two of the present surgical specimens were small cancer - ulcers upon the lesser curvature of the pyloric antrum , and cancer had invaded on the gastric side only the submucosa , with extension in one case into the pyloric sphincter muscle . 
yet both these specimens showed cancer islands within duodenal lymphatics at a distance of almost 1 ' 5 cfrom the pyloro - duodenal junction . this was also instanced by a cabot case no . 
25472 ( 1939 ) of the massachusetts general hospital , in which specimen a small malignant ulcer of the pylorus was limited to the mucosa except for a small extension below the muscularis mucosae . 
the only structure apparently offering any kind of barrier action was the gland layer of brunner . it has been the experience of the majority of authors that the layer of brunner glands remains free , in spite of many , and long , extensions of gastric cancer beyond the pylorus . in addition , whatever the method of propagation , it is exceptional that the mucosal epithelium of the 246 j . 
a resection of almost 3 cof the duodenum was made . microscopically the duodenal growth was so proliferative in the muscular and serous layers that one could not avoid an impression that an even greater length of duodenal resection would have been advisable . 
davie for his help with the plan of this research during its initial stages , and those pathologists and surgeons of the liverpool regional hospitals who have so kindly supplied me with specimens and helpful data . 
1. received for publication june 9 , 1948 . recent reviews of the literature on the association between asbestosis and lung cancer reveal different opinions as to whether asbestosis has been an aetiological factor in these cases . homburger , in 1943 , reviewing nineteen known cases found no reliable answer to the problem , whereas wedler in the same year considered there was a significantly high incidence of lung cancers in autopsied cases of asbestosis . kennaway and kennaway ( 1947 ) , who examined this problem as part of their broader statistical study of lung cancer , also leave the question unanswered . the statistical difficulties are due to the small numbers of asbestos workers , and to paucity of published autopsy records of such cases . the following case is therefore presented : 294 a . 
croton oil painted concurrently caused no increase in the incidence of the significance of the skin tumours , nor did it decrease the latent period ; absence of co - carcinogenic action of croton oil is discussed . the author is greatly indebted to p . 
kirby. from the research department , glasgow royal cancer hospital . received for publication , june 28 , 1984 . activity the carcinogenic of orally - administered 2 - acetylaminofluorene , aaf , for a number of tissues , mainly epithelial , was first demonstrated by wilson , deeds and cox ( 1941 ) for the rat , and subsequently confirmed for this species by bielschowsky ( 1944 , 1946 ) and others , for mice of various strains ( armstrong and bonser , 1944 , 1947 ; foulds , 1947 ) , for the fowl ( bielschowsky and green , 1945 ) and for the cat ( harding , quoted by bielschowsky , 1947 )  . recently wilson , deeds and cox ( 1947a ) have reported their own findings in mice of three pure strains . 
aaf has now been shown to be a carcinogen ( when given per os ) in eight strains of mice : cba , if , riii , white label , strong a , c57 black , c3h , and bagg albino . 
of the first five strains mentioned , cba were most prone to both liver and bladder tumours ; strong a were the least susceptible ( armstrong and bonser , 1947 )  . 
 ( 1941 ) were at that time unable to elicit tumours in rats by subcutaneous implantation of aaf , and , in view of the probable hydrolysis of aaf in the intestine to 2 - aminofluorene , af , they suggested that aaf might be converted to af and that the latter product was the real carcinogen . might be expected that af would be more carcinogenic for rats than aaf in however , in a recent paper , wilson , deeds and similar feeding experiments . cox ( 1947b ) report tumours to have arisen more slowly and in fewer numbers in rats given af orally than in similar rats receiving aaf in the same basal diet . they suggest that af , being more soluble than aaf , may have been absorbed more rapidly and then excreted rapidly . 
af derived from aaf by hydrolysis in the intestine could only be absorbed as fast as it was liberated . however , against this view it must be said that af , once absorbed , should be excreted as fast in either case and that tissues in remote sites will stand the same chance of receiving af , whether af or aaf be given orally , provided the presentation it seems possible that the hydrolysis takes place after absorption ; is continuous . studies on the liver after ingestion of aaf , using the extraction technique of miller and baumann ( 1945 ) and the estimation method of westfall ( 1945 ) , should yield information to test this point . it is significant that wilson , deeds and cox ( 1947a ) report tumours and other changes after implantation of crystalline aaf for long periods . bielschowsky ( 1944 ) painted af in acetone thrice weekly on the epilated contrary to expectation , no tumours at the site of painting skin of wistar rats . occurred , but all 5 rats developed liver tumour by 280 days and one had a tumour of the ductus acusticus externus . 
at first , arachis oil was used as vehicle , but later , tricaprylin became available and was used in place of arachis oil . injections were made at intervals of approximately 4 weeks , in alternate flanks ; 0 5 ml . 
a female dying at 351 days showed no abnormality , but of 7 mice dying between 530 and 594 days , all showed one or more liver tumours , some solid , some diffuse , with three cases being notably vascular . six of these seven mice were females , the other mouse being the only male to survive more than 125 days . 
one female , killed at 582 days , showed a mammary adenocarcinoma , and another , killed the same day , had a granulosa - cell tumour of the ovary . ( c ) c3h mice . - thirteen mice survived 52 to 126 days ; the rest survived 206 days or more . three females , killed at 206 , 235 and 235 days respectively , had one or two mammary adenocarcinomas . 
a fourth female was killed at 242 days without any gross tumour . three males survived 409 , 426 and 506 days respectively ; the first and the last of these showed hepatoma ; the other had primary renal carcinoma . 
ten male and two female mice survived over 500 days , four of these dying between 602 and 616 days ; extensive leukaemic infiltration was seen in two of these mice , but no liver tumours ( or tumours in other sites ) were found in any . 
kidney and bladder tumours were not found , nor were mammary tumours . ( b ) cba mice . - only cysts with minimal tissue reaction were found at the sites of injection in these mice . 
a variety of degenerative changes were found in the liver in most mice ; a male , injected eight times and dying at 285 days , had hepatoma at the edge of the left lobe . 
hepatomas were also found in three mice injected 11 times ; in two males dying at 565 and 574 days respectively , and in a female dying at 630 days . 
no tumours were found in the bladder or kidney in any of these mice . ( c ) c3h mice . - no tumours were found at the sites of injection , only minimal tissue reaction . 
one injected male of this strain had hepatomas by 242 days ; two males of the painted group had hepatomas by 409 and 506 days respectively . burns and schenken ( 1943 ) record a spontaneous primary hepatoma in a c311 male 14.5 months ( 440 days ) old . thus the mouse dying at 506 days may well have borne spontaneous tumours , and this possibility may also apply to that dying at 409 days . 
the earliest case seems to be undoubtedly induced by af which is therefore probably carcinogenic for the liver when injected subcutaneously in male c3h mice . among 12 cba mice given 2 - acetylaminofluorene ( aaf ) orally by armstrong and bonser ( 1944 ) , which survived more than 12 weeks , four showed liver tumours , but two were females dying at 63 and 65 weeks respectively and therefore liable to bear spontaneous tumnours . armstrong and bonser ( 1947 ) record three malignant hepatomas in seven male mice and five benign hepatomas in eight females given aaf orally . 
the time required for these tumours to develop is not recorded , but the incidence is well above that for spontaneous hepatoma in this species and , moreover , the latter always appear to remain benign . 
hence aaf and af both appear to be carcinogenic for the liver of cba mice ; af is slightly active also in c3h and c57 black mice . armstrong and bonser ( 1944 , 1947 ) record a high incidence of bladder tumours , wilson et al . 
in the present series no bladder tumours were found in mice injected subcutaneously with af and only in one female cba mouse , painted with af and killed at 582 thus af seems to be a bladder carcinogen when given orally to c57 black days . mice , but not when painted or injected subcutaneously . 
c3h mice appear to be unaffected in this organ . the kidney was free from tumour in all three strains after injection of af . painted mice of the c57 black and cba strains likewise had no kidney tumours , but a probable renal carcinoma was found in a painted c3h mouse , a male dying wilson et al . 
 ( 1947b ) record a carcinoma of the kidney in one of at 426 days . their c57 black mice given af orally . armstrong and bonser do not record any kidney tumour in cba mice given aaf orally . neither compound is very active for mouse kidney . armstrong and bonser ( 1947 ) record one mammary cancer in 9 females given aaf orally and surviving more than 20 weeks . 
one cba female in the present series , painted with af , showed mammary adenocarcinoma at 582 days . spontaneous mammary tumours in this strain seem not to occur and the solitary tumour found in each series referred to above is therefore considered to be significant . 
1949. although convenient and entirely suitable for the purposes for which they are employed , the u8ual methods of maintaining and utilizing transplantable tumours are not well adapted to special needs in experimental oncology , particularly when quantitative refinements and the desirability of repeating experiments with aliquot portions of the same tumour suspension are important considerations . the basis of any method which might meet such requirements must necessarily be one in which a number of separate and sin - iilar portions of a tumour can be preserved with some assurance that different portions tested at different - times will exhibit sirnilar activities . this means that the tumour tissue must be reduced to a fine state of division and homogeneous suspension and subjected to a method of preservation whereby its capacity to induce tumours remains constant for a long time . it is well known that growth may be obtained on transplantation of frozen and thawed tu ' mour tissue . although breedis and furth ( 1938 ) demonstrated the feasibility of preserving neoplastic cells in the frozen state for periods up to 400 days , this useful method does not seem to have been adopted to the extent that might have been expected . 
most of the observations have been made using the c3h sarcoma referred to by gye , begg , mann and craigie ( 1949 )  . pr " ration of tumour mmpennow . - the tumours were reduced to the necessary - state of subdivision by means of the pressure mincer described by craigie ( 1949 ) and the mince dispersed immediately in diluting fluid . 
the diluting fluids were freshly prepared from reboiled sterile distilled water and concentrated preparations of the required solutes . in experiments in which different diluting fluids were compared , a low primary dilution was first made in fluid of suitable composition and from this the secondary dilutions in the other fluids were prepared . 
were given subcutaneously in the approexcept in limited experiments , four sites in the anterior priate strain of mice . abdominal wall were used , these being approximately the centres of the upper and lower right and left quadrants . the " rtival of tumour 8uspen8iow in sau 8olulion& when a solution of sodium chloride is frozen at a temperature above 21t . ice crystalhzes out and the salt is concentrated as a strong solution ( 30 per cent ) between the cryistals . if a cer suspension in 34 volumes of 0 - 85 per cent nacl 20 ' c . 
in the strong salt solutions , in others the material was held in the frozen state for several hours at selected temperatures above and below that of the eutectic of nacl ; the results showed that although complete inactivation might require several hours , the initial rate of inactivation referable to electrolyte concentration was undesirably high . survival of tumour 8u8pen8ion8 in dextro8e solutiom . in view of the difficulties that might be expected to arise in attempts to obtain adequate preservation of activity in tumour suspensions frozen in inorganic salt solutions , the possibihty of substituting a suitable non - electrolyte was considered . of water - soluble organic materials , accordingly it was planned to test a variet but dextrose , the first of these selected for test , was found to have such a favourabl . 
effect that no attempt has yet been made to find substances more suitable for the purpose . because of the varied nature of the comparative tests which have been carried out and the introduction of a number of improvements in technique , it is not possible to present a synopsis of the results on a quantitative basis . table i provides a brief summary which , at best , merely shows that there is no contraindication to the use of - dextrose solution as a suspending fluid . 
16 - 25 m / 150cysteinehcim / 15onaohm / l5ona2hpoi , s = 0 - 85pereentn&o ; r four compamtive injections were msule in each mouse and the figure given in the cohnnn headed mouse group " ] indicates the arrangement of injections , eg . 
1 : 300 n&c1 the tumour mince was first thoroughly mixed with an equal volume of 0 - 85 per cent nacl and the mi iture was diluted i in 15 in the stated diluents . 
the first test was made after the suspensions had been kept frozen for 4 days . the lag periods observed in this test are not comparable w ' ith those in the later tests because of changes in technique of thawing , diluting and injecting , and also because of the use of a eysteine - phosphate.saline mixture in the later tests . however , it would appear legitimate to compare the activity of the material frozen for 253 days in the mixture of dextrose and 40 per cent glycerol withthe average activity of fresh c3h sarcoma suspension in ringer . 
further investigation is desirable not onlv with a view to improvements that might facifitate studies in which the tise of preserved tumour material is preferable , but also with the object of dete - riiiining the mecha i ms of surv - ival of activity . 
the varietv of pkvsical and physico - chemical factors which may he involved and the potential coniplexitv of their interplav need not be detailed , but some of the points which require investigation from the practical point of view mav be mentioned . thev are as follows : 1 . 
the development of a suitable fluid for dilution of thawed material . tumour ' suspensions which have been frozen may show a definite drop in activitv in 15 to 30 minutes after thawing . 
on the degree to which the material is diluted . it will have been noted from tables 11 and iii that cysteine phosphate buffer mixtures have been used as diluting fluids . 
the experimental evidence for the use of dilutina fluid of this composition is contradictorv and suggests a different approach to this problem . another matter which merits further investigation is the effect of dextrose on the nuclei of tumour c , - - ils as viewed with the phase contrast microscope . 
after preservation in the frozen state , sarcoma and c#rcinoma suspensions in dextrose solution show a greater and more consistent retention of activity than suspensions prepared with saline and ringer.. 
bartholomew 's hospital , london . received for publication may 15 , 1951 the data given below have been collected in continuation of two earlier studies ( kennaway and kennaway , 1936 , 1947 )  . stocks ( 1936 , 1947 ) has compared the death rates from cancer of the lung in males during the years 1921 to 1930 in london , and in the county boroughs , other urban districts , and rural districts of england and wales , and has shown that the rate increased with increasing urban conditions . * the same method has now been applied to the data , for both sexes ( table ii ) , of a later period ( 1946 to 1949 ) , when a great increase in deaths attributed to cancer of the lung has taken place . 
as recently as 1929 the numbers of cancers of the larynx , and of the lung , in males , were about equal ( table i ) ; since then , deaths attributed to the latter have increased enormously . 
the crude death rate for males has been falling in recent years ( 1946 to 1949 ) and in view of the ageing population this indicates an actual decrease in the incidence ; the death rate for females has been remarkably constant since these considerations show that the pooling of data for the larynx and 1935 . lung under any such heading as " respiratory system " is very undesirable . the standardized death rates show no perceptible difference in either sex between the figures for the 14 years 1926 to 1939 immediately preceding the war , and the since 1942 standardized death rates have been means for the period 1921 to 1930 . superseded by comparative mortality indices , which compare the death rate in each year with that of 1938 . . 
22 - 5 = 1 - 0 100 ' 0 82 - 2 17 - 8 100.0 the data at present available on the social incidence of cancer of the larynx show a gradient which is steep in men and absent in women ( table vi )  . 
hence the increased consumption of tobacco in recent years has not affected this form of cancer . ( 5 ) thus cancer of the larynx in men , and in women , differs in geographical , anatomical and social distribution , and in changing prevalence at the present time , and should be regarded as constituting two separate diseases . ( 6 ) the sexual distribution of intrinsic and extrinsic cancer of the larynx appears to be changing . we are greatly indebted to w . 
phillips , of the general register office , for a large part of the material contained in this paper , for help in the preparation of it , and for advice upon many matters . 
oliver. from the radiotherapy and cancer research departments , london ho8piw , london , e.i. received for publication january 25 , 1951 . the distribution of radioactive phosphorus can be investigated in vivo using a thin - walled g.m. 
the maximum range for beta paitioles of p32 in soft tissue is 8 mm . , but the half - value thickness is only of the order of 0 - 6 to 0 - 8 mconsequently , measurements on the skin can only indicate the amount of phosphorus in the superficial layers of the body ( effectively some 3 mdeep )  . however , under favourable conditions , such measurements can be used to demonstrate the increased phosphorus up - take by malignant tumours . low - beer , glenn - bell , mccorkle and stone ( 1946 ) have used this method with some success , as a diagnostic procedure , but its value is reduced by the low penetration of the beta rays and by the increased up - take also found in inflammatory conditions . 
phosphate buffer at ph 7 - 35 . it has been found advisable to check , by counter measurements , that the radioactive material has actuary left the site of injection , as , even after taking more than ordinary care , some unsatisfactory injections have been detected . this is particularly important , of course , when giving the isotope therapeutically , as dose calculations assume that the whole of the material enters the blood streano side effects of the injection were observed . 
the tumour may have received 4 to 8 times the dose calculated above , a total which is in excess of the generally agreed " tolerance " level . this was , however , of no consequence as the site was to re ' ceive an x - ray dose of 3000 to 4000 r . a number of sites over the tumour , on the diseased breast , and at corresponding points on the normal breast , were marked with gentian violet , and measurements of the activities were made with a counter tube applied directly f . 
the background rate was in each case the complete set of measurechecked before and after the series . ments was repeated and a mean value for each site was used . it was not feasible to prolong the counting time at any site ab ' ove about 3 minutes . 
as the count rates with this tracer dose were rather low , the measurements were usually limited to 1000 counts ( 3 per cent standard deviation ) or , after several days and over normal tissue , to only 100 counts ( 10 per cent standard deviation )  . consequently , the ratios of count rates over tumour and normal skin were not obtained very accurately , but the results sufficed to demonstrate large changes . series of measurements were made before , during , and 4 to 6 weeks after the treatment , at which time the x - ray erythema had subsided but the skin of the irradiated breast remained highly pigmented . observations were made on altemate days during 2 to 3 weeks . after intravenous injection , the radioactive phosphorus could be demonstrated immediately ( 5 to 8 seconds ) in the tissues of the breast , but the concentrations continued to increase in both healthy and dis6ased breasts for 10 to considerably lower count rates were observed when the next series 15 minutes . of measurements were made after an interval of 2 days , a change probably due to the excretion of p32 ' thereafter the fall was found to follow a roughly exponential form , corresponding to a " biological half - hfe " of between 7 and 9 typical cases are ifustrated in fig . 
i. and over both axillae are also included . it is of interest to note that the readings , over the forehead ( indicating thep . , 2 content of the frontal bone ) increased to the level found over the tumour and then decreased more slowly than the latter . values of the ratio of count rates over the diseased breast to those over the healthy breast are presented in fig . 
a sudden drop in the ratio occurred after the third irradiation . four weeks after the end of the treatment a second tracer dose was given , and the results obtained are shown in fig . 
for the first three readings the skin was still very red . by the time the erythema had subsided the count rates were rather low , but they appeared to be higher than normal over the whole of the diseased breast , without any locahzed . 
at a later date the authors hope to continue the investigation , although working at different institutions . the countrate due to p..2 was fodnd to be very much higher ( between 3 and 8 times ) over malignant mammary tumours attached to the skin , than over the corresponding parts of the healthy breast . 
no such , change occurred during after erythema stilboestrol treatment in a case which did not respond clinically . had subsided the ratios of measurements over the two breasts were found to be similar to those before treatmentbut the primary growth was still present in all these cases . the authors wish to thank sykes , the chief pharmacist at the hos ital , for preparing the material for intravenous injections , and k . 
1. received for publication january 26 , 1949 . thie application of the methods of urinary cholesterol estimation given by burchell and maclagan ( 1949 ) to cancer and control cases will now be described . bmaterial urine specimens were obtained from 13 normal subjects and 116 patients admitted to westminster hospital or to westminster hospital ( .all saints ' ) twenty - five of these patients were suffering from diseases urological centre . thought to be unlikely to affect cholesterol excretion as shown in the tables , and 73 were suffering from various forms of cancer . 
sample of the mixed specimen , or a smaller aliquot in the case of a concentrated urine , was centrifuged , the deposit washed once with normal saline and extracted directly with three portions of boiling acetone . 
the acetone extract was evaporated to dryness , and the residue extracted with petroleum ether for the determination of cholesterol as above . the cholesterol content of the supernatant urine ( su ) was determined on 200 ml . 
the sex difference is mainly due to the larger number of epithelial cells and leucocytes in urinary deposits froimw omen . it appears likely from these figures that the total urinarcholesterol would not exceed 4 - 49 mg . 
maclagan it is evident from this that if albuminuria is present from whatever cause , the su may be expected to show an increase in cholesterol content , and such a rise is unlikely to be specifically related to cancer . 
of urine with phenol reagent as described by burchell and maclagan ( 1949 ) , where reasons are given for assuming that this method does , in fact , estimate a proteose - like substance . it will be seen from fig . 
the ud cholesterol is associated with the cells of the deposit and shows a marked sex difference , being much higher in women than in it appears to have no direct relation to cancer . 
the su cholesterol on men . the other hand is associated with a urinary proteose fraction , or with heatraised su cholesterol excretion in the coagulable protein when present . absence of albuminuria did occur in a small proportion of cases of cancer ( 5 out this gives a of 51 cases ) , although the increase was slight in 3 of these cases . total incidence of hypercholesteroluria in cancer of 9 - 8 per cent , which is somewhat lower than that reported by other workers . 
thus sobotka , bloch and rosenbloom ( 1940 ) found 20 - 6 per cent , and bruger and ehrlich ( 1943 ) 34 - 3 per cent of positive results . 
for example , bruger and ehrlich ( 1943 ) reported some rise of total urinary cholesterol in 11 out of 32 cases of cancer , but 5 of these had either albuminuria or excess of cells in the deposit or both , findings which , according to our experience , might have been sufficient to account for the hypercholesteroluria even in the absence of cancer . 
the exclusion of these cases would bring the incidence of positive results down to the figure of 22 - 2 per cent . , which does not differ significantly from our own finding of 9 - 8 per cent ( difference 12 - 4 , standard error of difference 8 - 2 )  . we must conclude , therefore , that hypercholesteroluria , while frequently due to associated albuminuria or pyuria , does occur in a small proportion of in such cases it is the supercases of cancer in the absence of these factors . natant urine cholesterol which is increased . 
the incidence is not high enough to make the estimation of any diagnostic value , but it is of theoretical interest , and presumably depends upon increased tissue breakdown as suggested by previous workers . it should be noted that the colorimetric method of estimation used is not entirely specific for cholesterol , and the possibility that other steroids might have given rise to the few positive results must be admitted . however , the earlier work of bloch and sobotka ( 1938 ) on pooled 100 litre specimens of urine suggests that the results probably were due to increase of cholesterol itself . the question of urinary proteose is of some interest in view of the work of winzler and burk ( 1943 ) on blood proteose and cancer in rats . 
the histology was typical of lymphosarcoma , the cells being chiefly of the " lymphoblastic " type . local spread had occurred upwards in the submucosa for a short distance , and there was infiltration of adjacent rectal muscle but no noticeable spread in perirectal fat . 
the tumour was softer in consistence than most carcinomas and the base of the ulcer was covered by a greyish slough . both " lymphoblastic " and " lymphocytic " cells present . extensive spread in rectal muscle and commencing invasion of perirectal fat . 
the adenocarcinoma had infiltrated more deeply , but there was no sign of venous spread and the lymphatic glands were all free from metastases . we have given careful consideration to the possibility that this might actually be only one tumour , exhibiting an undifferentiated pattern in one part and a differentiated glandular pattern in another , as was suggested by gr . 
tumour b is a melanoma with four lymphatic metastases containing melantumour a is an adenocarcinoma with two lymphatic metastases free from pigment . section of tumour a showing adenocarcinoma , fig . 
1945 , and found to have a fibrous nodular tumour on posterior quadrant of lower third of rectum . biopsy showed spindle cell sarcoma apparently of low grade malignancy . seven years previously patient had had the coccyx removed in another hospital , and three years later a small tumour had been found in the rectum which was reported as a mass of fibrous tissue . synchronous combined excision of rectum by o . 
more than 4 inches of healthy bowel both tumours had given separated the melanoma from the adenocarcinoma . rise to lymphatic metastases , those from the melanoma being pigmented , whereas those from the adenocarcinoma contained no melana unique pathological specimen . 
twenty years ago weeks ( 1927 ) found reference to 100 cases of rectal sarcoma , but he regarded many as of doubtful validity and remarked - " if the questionable cases were discarded it is certain that the number would be reduced by one half . " we agree with this comment and have formed the impression that many of the cases which until recent years were recorded in the literature as " sarcomas " were probably examples of anaplastic carcinoma . this criticism does not apply to the cases reported in the last 15 to 20 years . most authors who have written about this subject seeinm to take the view that all varieties of sarcoma tend to run a rapidly fatal course , but we think that each of the four varieties of malignancy has this attitude needs qualification . to some extent its own characteristics and peculiarities and the prognosis differs considerably in each . lymphosarcoma is the commonest form of sarcoma of the rectum . it may manifest itself either as a single localized tumour or give rise to a crop of tumours bensaude ( 1929 ) was one of the first to spread over a long stretch of the bowel . draw attention to the diffuse or generalized variety of lymphosarcoma . in one of our cases ( case 3 ) the disease affected the whole rectum and distal end of the pelvic colon , so that in describing the primary focus we could not speak of a particular site of origin , but only of a region of involvement . 
the largest tumour was in the lower third of the rectum , but the other smaller tumours at a higher level were certainly not secondary growths resulting from the transportation of tumour cells , but were obviously new foci of lymphosarcoma developing indein spite of this unfavourable feature of lymphosarcoma the prognosis pendently . after surgical treatment would seem to be fairly good on the whole . 
at present there is insufficient evidence on which to base a comparison because it is only within recent years that these tumours interest in the subject have been separated out from other varieties of sarcoma . of reticulosis , stimulated by the writings of robb - smith ( 1938 ) , has had considerreticulum cell sarcoma is certainly a rarer tumour able influence in this respect . in the rectum than lymphosarcoma , and we think that it will probably be found to have a worse prognosis . spindle cell sarcoma is also a rare form of malignancy in the rectum . it is the one most easy to distinguish clinically from carcinoma because it obviously arises from the tissues of the bowel wall and not from the surface mucous membrane . the firm solid structure and covering of intact mucosa are of special significance . it has already been mentioned that in their histology these tumours give the impression of being of a relatively benign character . all who have written about melanoma speak of it as the most malignant of all the tumours now being considered . 
we agree with the view expressed by linder and wood ( 1936 ) that melanomas arise from the skin of the anal canal and tend to grow up into the rectum and that they metastasize early . 
the lymphatic glands may contain more pigment than the primary tumour , but it is worth mentioning that the haemorrhoidal and paracolic lymphatic glands may contain melanin apart altogether from the presence of a melanotic tumour . 
bussey although the cases we have examined personally are only ten in number they do provide material for comparison with the much commoner tumour , carcinoma of the rectum . in the end , of course , these rarer forms of malignancy can only be identified by detailed study of their histology , but there are some features in their gross characters which would make an experienced surgeon suspect that he was dealing with something " out of the ordinary . " we have summarized these by setting them out in tabular form ( table i )  . finally we have left to the end what we consider to be the most interesting feature of these rare tumours , namely , the frequency of multiple foci of malignancy . in four of our ten cases more than one tumour was found in the rectum , and in two cases the second tumour was of a completely different histological type . 
this raises the question both of multiple malignancy and dissimilar primary tumours . multiple malignancy is commoner in the rectum than is usually supposed . it so happens that we are in a position to give facts about this question because for many years we have been making observations on the frequency of the occurrence of multiple primary carcinoma and have found that in operation specimens of rectal cancer removed by a combined operation more than one primary rectal carcinoma is present in 4 per cent of cases ( over 2 , 000 examined )  . moreover we have records of many additional cases in which a second carcinoma was present in the colon in association with rectal cancer , so we were not surprised to find multiple tumours in our cases of lymphosarcomas ; in fact , we expected this to be the case . the occurrence of dissimilar primary tumours was , however , a complete surprise , and as far as we have been able to find out has not been previously recorded as a characteristic of these rarer forms of malignancy . in any organ of the body the existence of two tumours of a different histological type is a rare phenomenon . it is indeed remarkable that this unusual combination should have occurred twice in a series of only ten cases . 
we have searched through the literature but found no reference to the simultaneous occurrence of carcinoma and sarcoma in the rectum , though kreibig ( 1929 ) mentions a case of carcinoma plus lymphosarcoma in the ileo - caecal region . as far as the general relationship between carcinoma and sarcoma is concerned we note that warren and gates ( 1932 ) in a study of this subject were only able to collect from the literature 25 instances of the co - occurrence of carcinoma and sarcoma as separate tumours in the same organ . three were cases of sarcoma and carcinoma of the breast , twelve were of the uterus , and ten were in miscellaneous organs , including four cases of the combination of carcinoma and 1ynphosarcoma of the stomach . they found no recorded case of carcinoma and sarcoma of the rectum or indeed of carcinoma of the rectum associated with sarcoma of any other part of the intestine . 
melanoma arises always from the ano - rectal region and spreads upwards into the rectum . it metastasizes early and runs a rapid course . in four of the ten cases we are reporting more than one malignant tumour was present in the rectuone of these was an example of multiple lymphosarcoma and another of multiple reticulum cell sarcoma . in these cases tlhe associated tumours were of the same histological type , but in two other cases the associated tumours were of completely different histological type . 
she complained of cough , haemoptyses and loss of weight for about four months , but since october , 1944 , she had been feelmg listless and noticing palpitations and dyspnoea on exertion . 
a little lymphatic permeation was traced to the base of this lobe and involved the diaphragthe lower part of the lower lobe showed a fairly marked collapse together with a slight fibrosis . the left upper lobe was well aerated , but showed a sharply defined , firm area of congestion ( suggesting venous infarction )  . 
adjacent broncho - pulmonary lymph nodes are almost completely infiltrated . section of a main pulmonary vein shows neoplastic cells infiltrating the wall of the vessel ; in places these have reached the lumen and lined the wall with a thin layer of squamous carcinoma . 
ante - mortem thrombi have resulted , and some regions show early organization of the thrombus , which itself contains typical neoplastic cells . section of the left lower lobe shows lymphatic permeation by neoplasm , marked collapse and areas of oedema and haemorrhage . 
intra - alveolar phagocytes containing iron and carbon are numerous , and foreign body giant cells are seen in relation to the typical golden - yellow asbestos bodies lying in the alveoli and the finer lung trabeculae . there is marked subpleural fibrosis not related to neoplastic infiltration , but a consequence of the asbestosis . 
one section of this lobe shows that the neoplastic cells , although preserving most of the features of squamous carcinoma , nevertheless show a definite tendency to acinus formation , and here there is much secretion of mucus into the intercellular 252 r . 
the period of exposure also was long ( seven years ) , and although this is usual , cases have been reported of a neop ] asm developing after considerably shorter exposures . 
1. received for publication july 1 , 1948 . in the course of experiments on a transplantable mouse sarcoma it was observed that fresh saline extracts of tumour tissue agglutinated mouse and rabbit red cells . 
when extract and red cell suspension were mixed on a slide agglutination became visible to the naked eye within 30 seconds and appeared to be complete within 2 minutes . a number of different mouse and rat tumours , and a wide range of normal tissues , have been examined for haemagglutinating activity . 
horning. from the chester beally research institute of the royal cancer hospital , london , s.w.3. received for publication december 12 , 1948 . recfnt experience has shown that many of the growth - inhibiting agents used in the palliative treatment of cancer are carcinogenic . 
they also cause specific damage to cell nuclei and chromosomes and are able to induce mutations . the association of these biological effects of ( 1 ) growth inhibition , ( 2 ) chromosome damage , ( 3 ) production of mutations and ( 4 ) induction of cancer suggests if the that they may have a common fimundamental biochemical mechanism . induction of cancer is indeed a somatic mutation , then cancer induction might be included as a special mutation . 
the fact that x - rays can produce cancer in man was published in 1902 ( frieben , 1902 ) , seven years after rontgen 's discovery muiiller ( 1928 ) found that x - rays are mutagenic , and later mather of x - rays . and stone ( 1933 ) and koller ( 1934 ) described the chromosome damage following irradiation . 
the idea that cancer arises as a somatic mutation was supported by the demonstration of an increased incidence of mutations occurring in mice this was shown with methylcholanthrene treated with chemical carcinogens . by strong ( 1945 ) and with 1 : 2 : 5 : 6 - dibenzanthracene by carr ( 1947 )  . carcinogenic hydrocarbons inhibit the growth of animals and the establishment and growth of transplanted tumours ( haddow , scott and scott , 1937 )  . 
body - weight of freshly made aqueous solutions of nitrogen the first group was given methyl di ( 2 - chloroethyl ) amine hydromustard . chloride ( hn2 ) in a concentration of 1 mg . 
the second group received the same dose of tri ( 2 - chloroethyl ) amine hydrochloride ( hn3 ) for 10 weeks , after which time only 4 mice remained alive and injections were stopped . post - mortem findings of the mice which died within a week of an injection usually showed congestion of the alimentary tract or lungs . 
with the doses used all the coloured mice showed the effect of no nervous symptoms were seen . greying of hair ( boyland et al . , 1948 ) similar to that produced by x - rays ( hance and murphy , 1926 ) or by subcutaneously implanted plutonium ( prosser , painter , lisco , brues , jacobson and swift , 1947 )  . 
hornin - g occur spontaneously , and the tumours were larger and more malignant than those generally encountered in untreated mice . the carcinogenic action of the nitrogen mustards is very slow , the earliest lung tumour and lymphosarcoma being seen at 284 and 347 days respectively . berenblum and shubik ( 1947 ) have shown that carcinogenesis can be divided into an initial stage in which cells are irreversibly changed into latent tumrnour cells , and a development stage which can be brought about by cocarcinogens such as croton oil . 
the incidence of tumours expressed as quantal response is probably dependent on the initiating action , but the rate of appearance of the tumours depends upon cocarcinogenic action . the present authors consider that the initial irreversible conversion to latent tumour cells is the change which is associated with chromosome damage and mutations . 
the nitrogen mustards are possibly active in initiating the carcinoin order to test this hypothesis genic change but poor in developing action . experiments are in hand in which mice are being treated with nitrogen mustard and croton oil . a possible explanation of the association between inhibition of growth and carcinogenic power is that the inhibition is due to interference with cell division in growing tissues . 
the drugs under discussion reduce the rate of growth by impeding mitosis . this interference with mitosis is likely to increase the chances of a somatic mutation from normal to malignant cells occurring . 
of 14 mice which survived more than 250 days , 10 had tumours including lung tumours ( 8 ) , lymphosarcomas ( 2 ) , a uterine fibromyoma and a spindle - celled sarcoma at site of injection . this investigation has been supported by grants to the royal cancer hospital from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the u.s. 
3. received for publication january 18 , 1949 . the investigation of carcinogenic substances which have been obtained from human tissues ( kleinenberg , neufach and shabad , 1940 ) and from other biological sources has been the subject of earlier publications from this institute ( hieger , 1940 , 1941 , 1946 , 1947 ) , reporting that : 1 . 
whittick. from the department of pathology , royal cancer hospital , london . received for publication december 13 , 1952 . there is an astonishing neglect in the literature of the benign cutaneous condition described by maccormac and scarff in 1936 , and named by them molluscum sebaceuan alternative name , kerato - acanthoma , has since been applied , and this has the merit of preventing confusion with molluscum contagiosum , an unrelated condition . it has been the subject of only 4 papers , all by british authors , maccormac and scarff ( 1936 ) , musso and gordon ( 1950 ) , rook and whimster ( 1950 ) and beare ( 1953 ) , and does not yet appear to have reached text - books of dermatology or pathology . that this in no way reflects the incidence of molluscum sebaceum is certain . indeed , it is not an uncommon condition , and is still very frequently misdiagnosed as squamous - cell carcinoma by both dermatologist and pathologist . smith , in 1934 , described the occurrence in a young man of multiple primary squamous - cell carcinomas of the skin which healed spontaneously and he was unable to find any comparable case in the literature . since that time there have been eight papers on the subject ( table ii ) with descriptions of similar lesions in 11 patients . comparison of the clinical and pathological descriptions of these cases with the natural history and the structure of molluscum sebaceum at once suggests the probability that all the recorded cases of spontaneously healing epithelioma of the skin are in fact instances of molluscum sebaceum . the following account is based on a series of 7 cases of molluscum sebaceum which after biopsy diagnosis were untreated and allowed to run their natural course to spontaneous regression . 
whittick that the lesion of molluscum sebaceum closely simulates highly differentiated squamous carcinoma will be apparent from the histological description and illustrations . there is no single feature which will allow differentiation . 
about this central plug of keratin is a broad , dull red , convex and smooth - surfaced epidermal riwith regression there is gradual flattening of the lesion , and finally the keratin plug falls off to leave a clean , slightly depressed scar . ordinary squamous carcinoma usually has a much slower rate of growth with progressive increase in size for several months . although rapid growth may occur , it is usually accompanied by early involvement of the regional lymph that rapidity of growth has not been accompanied by metastasis to the glands . local lymph nodes in the spontaneously regressing cases has indeed been stressed by some of the authors . 
whittick local and lymphatic spread . were the alleged cases of spontaneously healing epithelioma true instances of squamous carcinoma there should be good evidence of local destructive invasion and lymphatic extension , but this is lacking . in over half the recorded cases the regional glands are not mentioned and , in view of the long survival period in these cases , it may reasonably be presumed that they were not involved . example in smith 's ( 1948 ) case 1 there is a history of lesions for 21 years and in his case 2 for 29 years . 
lack of lymphatic involvement was mentioned by dunn and smith ( 1934 ) , and grzybowski ( 1950 ) comments on " the lack of involvement of lymph nodes in spite of the 9 years ' duration of in only one case , charteris ' second ( charteris , 1951 ) , is enlargethe disease . " ment of lymphatic glands mentioned , and these were found , histologically , to be tumour - free . local invasion , too , appears to have been very limited in the spontaneously healing cases , being restricted to local penetration into the dermis . thus , dunn and smith ( 1934 ) , " the invasive process at its height never appears to transgress this feature applies equally well to molluscum the limits of the true skin . " description by two authors of local tissue destruction in sponsebaceum . taneously healing epithelioma requires comment . smith ( 1948 ) , when recording the subsequent history of his case 1 , states that he was an irregular attender and " permitted much further destruction of the soft tissues of his face , ' and that he now wore a prosthesis to cover extensive destruction of his nose . this on first reading seems proof of an infiltrating and destructive malignant growth , but it must be pointed out that in the previous paragraph we are told that following treatment of a lesion of the right leg by radium , the same patient had to undergo amputation of his leg because of necrosis of the tibia . lesions of his face had been treated by contact x - ray therapy . if this extensive destruction of the nose , requiring a prosthesis , was indeed due to squamous carcinoma , then the lack of lymphatic extension and the ultimate spontaneous healing ( sic ) make this case even more remarkable . 
chadwin. since completion of this paper two other relevant communications have currie and smith ( 1952 ) , under the title " multiple primary sponappeared . taneous - healing squamous - cell carcinomata of the skin " , describe 2 new cases . they maintain that the lesions they describe are unrelated to molluscum sebaceum . whittle and lyell ( 1952 ) , in commenting on a case of molluscum 'sebaceum which f . 
7. received for publication february 3 , 1949 . one of the surprising elements in bittner 's discovery of the " milk factor " is the apparent entry of the virus into the bodies of the young mice via the it is , however , obviousthat during suckling a small amount alimentary canal . of milk may also enter the nostrils , and that the nasal mucosa may offer an alternative port of entry . it also seems possible that the milk factor might be destroyed by digestion in the stomach . if this were so it would be difficult to recover milk factor from the stomach contents of suckling mice . 
the unfortunately the experiresult was entirely negative in the 40 mice so treated ment was not adequately controlled , in that none of the mice were tested for susceptibility by means of extracts known to contain the virus . 
jackson memorial laboratory , bar harbor , me . received for publication december 16 , 1948 . it is known from the work of andervont and bryan ( 1944 ) and green , moosey and bittner ( 1946 ) that the milk agent is antigenic for the rabbit and the rat . if , as is probable , the agent , is a virus one would expect it to be antigenic for the susceptible species . 
modem technique - 3 of microscopy , particularly phase - contrast , by greatly facilitating the study of fiving cells have resulted in greater use being made of tissue cultures for morphological studies . 
when cells migrate from an explant in vitro , they tend to spread out so that around the periphery of an outgrowth they are considerably flattened . this is most obvious in fluid culture media where the cells furthest away from the explant may be reduced to little such cells are ideal for the study of cytoplasmic structure , more than a fine film . as many investigators have realised . 
the necessity of rapid fixation , in order to obtain perfect preservation of chromosome structure has also resulted in the common practice of using squash preparations and smears for the study of nuclear strucsuch procedures possess the further merit of eliminating the possibihty tures . of slight morphological alterations being brought about by the prolonged dehydrating , clearing and imbedding necessary for the preparation of sections . nevertheless ah these methods have the common disadvantage of rendering difficult the correct appreciation of the spatial arrangement of intranuclear structures . in this respect the older method of studying stained sections of fixed tissues presents definite advantages . 
by cutting sections of approximately the same thickness as the average diameter of the cell nuclei , one obtains preparations with whole nuclei and shces of nuclei of varying thickness . 
yet with all fixed preparations of cers there arise doubts as to the validity of the finest structural details which are detectable , especially when they approach the limits of mic ' roscopic resolution . so the results of the study of fixed and stained cells have been correlated with observations made by other techniques , which have included the microscopical examination of living cers immediately after their removal from the animal body . structural organization of the nucleus seen in sections . the ideal type of cell with which to commence an investigation of this kind would be one with a large nucleus , single nucleolus and well - defined chromatin granules . 
most nearly fulfilling these requirements were the cells of a mouse adenocareinoma ( t27 )  . its selection was further influenced by the fact that it had been employed in several previous researches ( ludford , 1924 , 1930 , 1932 a , 1932 b , 1933 , 1934 ) so that the structure of its cells , and their behaviour under a variety of experimental conditions , as well as their growth characteristics , both in vivo and in vitro , were already well known . the same methods of fixation and staining were adopted as were formerly used for the study of chromosomes ( ludford , 1930 ) , except that after iron - alumhaematoxylin staining the differentiation was not carried so far as is usual in making chromos ' ome preparations . frozen sections stained by the feulgen technique were also found most useful . for demonstrating the smallest structural details it is doubtful whether any method can excel the results obtained by flemming fixation followed by intense staining with iron - alum - haematox.ylin when the surface of a nucleus from such a preparation is examined there are to be seen numerous minute granules varying in size . 
4 depicts a slice through the membranes in the process of section cutting . here are seen the same peripheral granules , and also the centre of a nucleus . strands connecting the two nucleoli with the membrane . 
3 , which is another slice from in this one , some well - defined strings of granules are the surface of a nucleus . discernible , while in the adjacent fig . 
the latter obviously represent an early stage in the formation of the prophase ch - romosomes . actually in a section of a rapidly growing tumour it is impo - ssible to determine ex ' actly when the prophase does . 
8 they appear as single threads , and granules are perceptible on some of them . it thus seems that the nucleoli are connected with the periphery of the nucleus by chromosomes , and also by threads of a different nature . frequently the latter appear to be attached distally to a chromosome . examination of prophases at the stage when the nuclear membrane is undergoing dissolution will sometime reveal chromosomes connected with remnants of nucleoli . 
13 represents part of a cell of the same carcinoma on the edge of a 2 - days - old culture , which had been fixed in flemming 's fluid , and intensely stained with iron - alum - haematoxylthe fine peripheral granules beneath the nuclear membrane which are shown in fig . 
16 and 17 , these are projection drawings ( indicated by " p " in the legends )  . there are included in the plane of each drawing bodies distributed throughout the whole thus each drawing constitutes a diagrammatic representation of the nucleus . structures as if they were projected on to the equatorial plane . 
this does not mean none is present , because extremely thin threads might only be visible when coated with dyestuff , and this may have beeil removed in the early stage of differentiating with the iron - aluthe nucleus seen in fig . 
each of the nucleoli is surrounded by particles which appear to have been emitted froin its surface . if observation is now extended to feulgen - stained cultures it becomes evident that the nucleolus is of a dual nature . 
the latter constitutes what caspersson ( 1947 ) has termed " the nucleolar associated chromat - in " and to which he attributes a special role in it can be distinguished from the material of which the bulk protein synthesis . of the nucleolus is composed in the living condition , and in fixed preparations after a variety of staining methods . 
on the basis of the reaction of the two nucleolar components to staining by the feulgen and the pyronine - methyl - green techniques it is concluded that the chromatin is composed of appreciable amounts of deoxyribose nucleotides , and the remainder of the nucleolus of ribose nucleotides . there is considerable variation in the amount of nucleolar chromatin in different cers , as is demonstrated by fig . 
20. in one form of cellular degeneration as has previously been mentioned , particles are discharged from the surface of the nucleolus . comparison of cells stained by the iron - alum - haematoxylin technique , such as that show - n in fig . 
the latter are stained by haematoxylin , but are invisible in feulgen preparations . there are also distinguishable in nucleoli varying numbers of argentophile bodies . page , regan and maccarty ( i 938 ) found that both types of inclusions were more numerous in malignant than in non - malignant cells , and that " the more ma - lignant the neoplasm , the greater the number of intra - nucleolar bodies . " examination of nucleoh with the electron microscope has suggested the existence of a more comphcated structure . 
the hmit of resolution attained with the ultra - violet this is the best resolution represented in microscope is only about 0 - 1 micron . the figures ' illustrating this paper . occasionaby when a nucleolus is highly vacuolated its appearance is rather deceptive , and might erroneously be interpreted as being reticulate . 
one wonders whether the coniphcated internal structure which has been described may be the result of a slight distortion induced by the procedures involved in preparing sections for examination by the electron microscope . 
the vacuolated appearance is not an artefact of fixation as it is visible in hving cells . distribution of nucleic acids in the nucleus . as a matter of convenience , for the purpose of description , it is proposed to refer to the material of which the nucleolus is mainly composed as " plasmosomin "  . 
the nucleolar chromatin contains sufficient deoxyribose nucleotides to stain intensely by the feulgen techiiique , while plasmosomin this does not ehminate the possibility that in the latter deoxyribose does not . nucleotides may be present in such small quantities as to be below the limit of sensitivity of the feulgen techn ' ique , upon the vahdity of which as a tes t for deoxyribonucleic acid this only definitely known chemical difference between nucleolar chromatin and plasmosomin depends . cytogeneticists find it convenient to use the terms " euchromatin " and their usage is based upon the conclusion that at the heterochromatin "  . end of mitosis as the chromosomes uncoil deoxyribonucleic acid remains attached at certain loci ( heterochromatin ) , and is discharged from the rest of since it has been impossible to see whether the chromosome ( euchromatin )  . this actually happens in the cells employed in this investigation no attempt has been made to distinguish between two types of chromatthe term " chromatin " is used in this paper to describe nuclear material which gives a positive reaction with the feulgen test , and which is not visibly connected with the nucleolus . whether one studies fixed and stained feulgen preparations , or ultra - violet micrographs of living cells , it becomes obvious that there must be an increase of deoxyribonucleic acid at prophase , and a corresponding decrease during the evidence has already been adduced that the reconstruction phase of mitosis . chromosomes are represented in the " resting " nucleus by the fine granules at its surface , and on strands connecting the nucleolus with the nuclear membrane . these granules appear to be faintly stained by the feulgen technique . 
but it is doubtful whether any definite conclusion can be justifiably drawn from pale staining , as it has been pointed out , most of these minute particles are just ifthey fail to stain that does above , or below , the liniits ofmicroscopic resolution . not necessarily mean that they contain no deoxyribonucleic acid . it might well be that the amounts present in such small particles would be undetectable by the techni ' que . also very faint staining could result from absorption of traces of diffuse dyestuff . 
the latter usually appears to be very faintly coloured in feulgen preparations , and the nuclear periphery is always most clearly defined there is by comparison an even in the absence of cytoplasmic counterstaining . intense staining of larger peripheral particles , and of others on the filaments connecting the nucleoli with one another and with the nuclear membrane . 
30 is an ultra - violet micrograph of some flattened coagulated nuclei from another mouse carcinoma ( af )  . it will be noticed that the superficial structure is very similar to that draw - n in fig . 
they have been regarded as the chromosomes , or fragments of chromosomes , of the interphase nucleus , but this interpretation of their nature has been disputed by lamb ( 1950 )  . it is highly probable that they are identical with the strands of material exhibiting strong absorption of ultra - violet radiations of 2570 a wave - length , which are seen in fig . 
the absorbing material presumably comprises the fine granules , which for reasons already stated are regarded as representing the chromosomes of the interphase probably their volume is augmented at the time of nuclear coagulation nucleus . as the result of the accretion of additionaldeoxyribonucleic acid from the nuclear sap , by a piocess analogous to that which occurs at the prophase of mitosis . relationship between nucleolar chromatin and plasmosomin . on the basis of the preceding considerations it is concluded that the highest concentration of deoxyribonucleic acid is in the nucleolar chromatin and ' bodies deoxyribonucleic acid is also present in the minute granules derived from it . which represent the interphase chromosomes and in the nuclear sap . considerable evidence has been adduced by other investigators to prove that the plasmosome is particularly rich in oxyribonucleic acid . the functional relationship between nucleolar chromatin and plasmosomin requires furtber investigation . 
the observations that are reported in this paper are consistent with two possibifities . either nucleolar chromatin and plasmosomin are built up from the same simple precursors , and there are altemate pathways of metabolism the 122 r . 
ludford course of which can be deflected so as to lead to the formation of either oiie or or , there are contained in plasmosomin enzynie systems the other substance . responsible for the synthesis of the substances comprising nucleolar chromatin from certain of its chemicary simpler constituents ; or perhaps for breaking dow - n plasmosomin and converting it into nucleolar chromatthe latter notion finds support from the behaviour of the nucleolus during the formation of the chromofig . 
36 and 37 are ultra - violet micrographs of hving prophase somes at prophase . nuclei of a sarcoma ( rb )  . in the former the surface of the nucleus is in focus and the peripheral chromosomes are seen in process of formation . in the latter the nucleoli in the interior of the nucleus are in focus . 
the darker nucleolar chromatin is distinguishable from the lighter plasmosomthe nucleoli are in process of disintegration , and there is a considerable production of nucleolar after the chromosomes are fully formed , small spherical masses of chromatin . plasmosomin are often distinguishable devoid of any chromatat this stage all the feulgen positive material has been deposited on the chromosomes . 
the fonner was photograpbed from a 3 - days - old primary culture of mammary carcinoma ( ad ) in a strain mice ; the latter from a 5 - days - old primary culture of mammary gland from a low - cancerstrain mouse ( c57 )  . 
38 exhibited the greatest degree of polymorphisnote also in this figure the derangement of mitosis which has resulted in two daughter nuclei with numerous karyomeres instead of nuclei . despite the similaritv of the nuclear structure of the cers of fig . 
38 and 39 explants of carcinomata give rise to sheet their behaviour in vitro differs . growths of cells with greater reg - ularity and rapidity than do those of mammary glands . 
the cehs of other mammary cancers induced by carcinogenic compounds , independently of the milk factor , exhibit greater abnormalities , which distinguish them from normal mammary gland cells . there is corresponding variation in the extent to which sarcoma cells differ from fibroblasts with respect to nuclear structure . 
the former is a photomicrograph of a 7 - days - old primary culture of mouse - embryo - heart fibroblasts , and the latter of a 3 - days - old culture of a sarcoma ( aa ) which originated fig . 
34 and 35 mosomin and nucleolar chromatin are included in the drawing . are ultra - violet micrographs of a cell of the same sarcoma , which was the most rapidly growing of the tumours which have been studied in the course of this since all the fig . 
ludford of these the " simplest and rarest type " involved the formation reconstruction . of chromosomal vesicles , or karyomeres . this was " long ago described by biitschli and fol in the blastomeres of segmenting eggs and since observed in embryonic cells of many species.. in this process each chromosome is converted into a small vesicle exactly hke a minature nucleus , the whole group then fusing together progressively so as to form first an irregular , chambered structure and finally a smgyle nucleus . 
from the outer wall of this , apparently , arises the nuclear menibrane , while the inner walls of the vesicles break down irregularly to form the nuclear network "  . 
he considers that the interphase nucleus " probably consists of closely packed , firmly adherent , swollen chromosomes ( chromosomal vesicles or karyomeres )  . " this condition is brought about by the telophase chromosomes swelling to form vesicles whicli adhere to one another . 
each vesicle retains its identity throughout the interphase . " during prophase each chromosome sinks into a dense gel which is separated from its neighbours by the fluid which collects between them . " lewis ( 1947 ) points out that amitosis and nuclear fragmentation would be readily explicable as resulting from the loss of adhesion between chromosomal vesicles . since nuclear formation by the fusion of chromosomal vesicles is said to be speciary characteristic of embryonic cells , it would not be surprising to find the same process occurring in malignant cells which they resemble in many respects . karyomeres are often clearly distinguishable in dividing cancer cells . attention has already been directed to the example in the middle of fig . 
28 and 29 could originate from the cohesion of karyomeres , formed , not as lewis ( 1947 ) suggested , by the swelhng of chromosomes , but by their spreading out over the surface of after coalescence of the latter , the chromosomes would adhere to the vesicles . internal surface of the external walls of the vesicles , which form the nuclear membrane . 
instead of the inner walls of the vesicles breaking down irregularly to form a nuclear network as wilson ( 1925 ) suggested , they would constitute the strands which extend between the nucleoli and the cell membrane . 
to bring ' about such an arrangement it would be necessary to postulate the existence of some mutually repellant force between the chromosomes and the nucleolus at this stage , so that the latter was forced into the centre of the coherent vesicles . from a cursory examination which has been made of different tissues of a number of mammals , including man , it appears that their nuclear structure is essentially the same as that which has been described , but no comparable study has been made of the nuclei of lower animals , or plants . apparently there is a fundamental difference between the nuclear structure of the higher animals and the higher plants . according to the recent work of chayen , davies and miles ( 1953 ) the interphase nucleus of plants ( vicia , allium , zea , tradescantia ) consists of a peripheral zone containing the chromosomes , a middle zone with a protein content , the width of which varies with the state of mitotic activity , and an inner zone occupied by the nucleoli . 
the most striking morphological feature is the manner in which most of the chromosomes are spread out over a spherical area , therebv brinain - a about maximum exposure to the cytoplasm on the outside , and to subsiances emitted from the nucleolus on the inside . 
some of the mitochondria and other granules are applied to the surface of the nucleus , and only clearly , the thickness of its membrane separates them from the chromosomes . substances which penetrate the plasma membrane must pass through the cordon of mitochondria before reaching the nucleus , and between the chromosomes if they are to get to the nucleolar system . in pioneer studies on living cells in tissue cultures , lewis and lewis ( 1915 ) followed the movements of mitochondria backwards and forwards between the nucleus and the cell periphery , and recently pomerat ( 1953 ) has observed rotary movements of the nucleus in epithelial cells growing in vitro . reasons have already been adduced for believing that the mitochondria are involved in protein synthesis ( ludford , smiles and welch , 1948a , 1948b . ) , and attention has been directed to the correlation between . 
hypertrophy of the nucleolar system , proliferation of mitochondria and increased nucleotide content of the cytoplasm ( ludford , 1951 )  . such observations as these tend to emphasise that the cell as a whole is a unified functional system . it is reasonable to suppose that the performance of its fundamental vital processes necessitates intimate correlation of the functional activities of all its organerae . recently brenner ( 1953 ) has deduced from the appearance presented by the nucleus in phase - contrast photomicrographs and ultra - violet micrographs ( ludford and smiles , 1950a , 1950b . ) , and from the results of ultra - centrifugation experiments carried out by himself and others ( beams , 1948 ; claude , 1943 ) that segments of chromosomes are attached to the inner surface of the nuclear mem " these segments maintain their continuity with the remaining parts of brane . the chromosomes which , as uncoiled threads , occupy the inside of the interphase nucleus . " on the basis of caspersson 's ( 1950 ) hypothesis that heterochromatic regions of the chromosomes control protein synthesis brenner ( 1953 ) has proposed that " the nuclear membrane heterochromatin with its specific genes controls the synthesis of equally specific microsomes , each desoxyribonucleic acid directing the synthesis of a characteristic type of ribonucleoprotein "  . " protein synthesis is a two phase reaction " , according to haurowitz and crampton ( 1952 )  . in its first phase , an expanded peptide film acts as a template on which a layer of amino acids is absorbed . 
the peptide film is maintained in the expanded state , its only efficient form , by combining with nucleic acids to form a nucleoin the second phase of protein synthesis , the peptide chain is folded protein . to form ' a three - dimensional globular molecule . haurowitz and crampton ( 1952 ) suggest that the highly specific peptide chains are probably first formed in the nucleus , and that they pass out into the cytoplasm where they are specifically since antigens are deposited mainly in cytoplasmic granules in liver folded . cells it is concluded that the folding of the peptide chains takes place in these granules . 
as haurowitz and crampton ( 1952 ) admit , their evidence that the first phase occurs inside the nucleus is equivocal , while certain of their experimental results indicate that it takes place in the cytoplasmic granules . 
the peptide ffim which haurowitz and crampton ( i952 ) suggest acts as a template in protein synthesis might be locahsed on the surface of the occasionally fibroblasts migrating from explants in tissue cultures mitochondria . leave behind them small pieces of cytoplasm which contain mitochondria and other granules . 
one possible reason for this is that the function of mitochondria is controlled by substances produced by the chromosomes . certain observations also suggest that the latter are dependent upon substances supphed by the nucleolar system . in conclusion , it should be pointed out that cells may undergo malignant transformation without any alteration occurring in their nuclear structure that can be detected by the present methods of microscopy . this is understandable if as has been suggested ( lufford , 1952 ) the cytological basis of malignancy ie ; an imbalance in the genes brought about by processes which result in ( 1 ) the loss of some chromosomes , or parts of chromosomes , and ( 2 ) the intranuclear duphhcation of others . 
this implies that with improvements in microscopical technique it should be possible to distinguish differences between the chromosomes which are spread out on the inner surface of the nuclear membranes of malignant cells and their non - mahgnant prototypes . 
accorcling to caspersson and santesson ( 1942 ) the heterochromatin system of malignant cers is stimulated to abnormal activity . this leads to disturbances in the formation of cytoplasmic proteins and in the reproduction of gene protein , which result in abnormal growth . 
it would be more compatible with the results of the present study if hypertrophy of the nucleolar system and a hyperchromatinic condition of the nucleus were the morphological expression of an increased growth rate rather than being indicative of malignant growth . it has not been possible to identify the nucleolar organizer on the chromosomes of the cells examined during the course of this work . so it remains to be deter ' mined whether increase in size of the nucleolar system is the result of duplication of chromosomes bearing nucleolar orgadizers . there is , however , indirect evidence that this may be the case ( biesele , poyner and painter , 1942 )  . the studies with ultra - violet microscopy described in this paper were carried out in the national institute for medical research and constitute part of a wider 130 r . 
hall. from the hugh adam cancer research department of the medical school and the new zealand branch of the british empire cancer campaign , university of otago , dunedin . received for publication may 26 , 1953 . rats numerous attempts have been made to elucidate the role of the thyroid hormone in the development of chemically induced tumours . 
the relevant literature has been reviewed by miller and baumann ( 1951 ) who studied this problem in treated with dimethyl - amino - azobenzene . these authors mention some of the experimental difficulties encountered when the metabolic rate is altered by the administration of goitrogens or of thyroxthe action of thiourea , thiouracil and related compounds , however , is not limited to the thyroid ; they can affect also other organs , as for instance the liver ( fitzhugh complications of this kind can be avoided by means of and nelson , 1948 )  . surgery if hypothyroidism is the goal of the investigation . 
the effects of partial thyroidectomy are comparable with those obtained by goitrogens in doses too small to inhibit completely thyroxine synthesis . complete elimination of thyroid hormones resulting from either the administration of large doses of goitrogens or from the removal of the gland leads to a complex endocrine imbalance , the outstanding feature of which is a pronounced disturbance of growth . the pituitaries of such rats contain no acidophils and therefore no somatotrophin is formed . 
the thyrotrophic hormone , however , is secreted in elevated amounts . we have studied the action of aminofluorene ( a.f. ) and its acetyl derivative ( a.a.f. ) on the thyroidectomized rat , choosing these carcinogens because they induce tumours in more than one organ . 
one hundred and thirty were wistar rats ( 106 males , 9 of which were castrates , and 24 females ) and 17 were males of a piebald strain . forty - nine intact rats and 9 castrates served as controls ; eighty - nine were thyroidectomized . sixty - two of the 89 ( 70 per cent ) were considered to be completely thyroidectomized because their pituitaries were virtually free of acidophils . 
with the same the intact but not the thyroidamount of carcinogen during the remainder . after the 20th week the ectomized animals consumed all the food offered . in experiment 2 the milkanimals were maintained on ordinary stock diet . flour diet was given throughout , but for the first 20 weeks the diet was adjusted in such a way that 2 mg . 
in acetone 70 applications being given to the albino and 90 to the piebald rats . in this experiment rats which were obviously not completely thyroidectomized as indicated by their growth curve were kept separately from the other animals in in experiment 4 , 9 castrated order to avoid thyroxine intake from the excreta . and 30 intact rats were treated with a.a.f. 
daily. maintained on the wet diet supplemented by grain . in the 15th week 19 of the intact animals were thyroidectomized . liberal amounts of drinking water were available to all animals . in our experience thyroidectomized rats kept on a wet diet are in a better in long - term experiments state of nutrition than when they receive dry food . care has to be taken that excessive growth of the incisors does not interfere with their food consumption . the rats were weighed once weekly and examined for the presence of tumours . they were sacrificed when a neoplasm was suspected or when their general state of health made it advisable . 
the earliest hepatoma was found in the controls in the 18th week of the experiment , multiple benign cystic cholangiomata being already present in the partially thyroidectomized males the earliest hepatoma was at the 15th . discovered in the 28th week . 
no mammary cancers were seen in the thyroidectomized females , the majority of which were in anoestrus already in the third week of the experiment when vaginal smears were taken for the first time . table ii ( experiment 3 ) shows the results obtained with a.f. 
two appeared in intact , 3 in partial and 4 in completely thyroidectomized rats . in addition , one adenoma of the lung appeared in the latter group , and a cancer of the breast in the controls . in experiment 4 thyroidectomy was performed after a.a.f. 
had been fed all the controls developed hepatomas , the first being for a period of 13 weeks . found 7 weeks after the withdrawal of the carcinogen . thyroidectomy performed in the 15th week of the experiment was without the slightest influence on the development of these neoplasms , the first hepatoma appearing already in the 19th week . 
when at the 38th week the experiment was terminated each surviving animal was found to have hepatomatous and cholangiomatous lesions . these results are summarized in table iii , which includes also an additional table iii . - tumours induced by a.a.f. 
hall reduced , the glands containing little fluid whereas the weight of the testes was well maintained . in such animals an atrophy of the interstitial cells of the testis was found histologically , indicating inadequate stimulation by interstitial cell - stimulating hormone ( i.c.s.h. ) , and subsequent failure to produce androgens in amounts sufficient for the maintenance of the accessory sex organs . in this connection it might be remembered that none of the completely thyroidectomized females had a regular oestrous cycle . the adrenals did not show uniform changes . the width of the cortex tended to be less than normally ; the sudanophobic zone , present in intact males , was frequently absent , and the amount of lipoid stainable with oil red 0 was reduced considerably in some but little in other glands . 
some of the thyroidectomized animals were rather obese at the time they were sacrificed , which made correlation between organ and body weight unreliable . as in an earlier experiment ( bielschowsky , 1949 ) , neoplastic changes were found in the thyroid tissue of a.a.f. - treated animals in which a small fraction of the gland had escaped removal . in one instance a highly anaplastic tumour arising from such a thyroid rest was found at autopsy - worth mentioning because a tumour - cell embolus was seen in the periphery of this neoplasm , the only case in which evidence suggestive of malignancy was found in such a thyroid tumour . in the pituitary of this male wistar rat an adenoma was found . the tumour , the only one seen in these experiments , had the same morphology as the basophil adenomata present in aged rats which had received an iodinedeficient diet ( bielschowsky , 1953 )  . all the other pituitaries showed the typical picture of total or partial thyroidectomy , i.e. , absence of acidophils or marked reduction in their numbers with evidence of degranulation coupled with the appearance of " thyroidectomy ' " cells . the retro - bulbar tumours . the appearance of carcinomata in the orbital tissue of two rats of experiment 1 , a type of neoplasm only found in the thyroidectomized groups , led to a systematic search for lesions in the lacrymal glands . 
6 shows that they vary considerably in size and shape and have lost the pale foamy appearance of the normal glandular epithelium . their nuclei are hyperchromatic and dividing cells are present . since these changes were obviously of a neoplastic nature it seems justified to consider the retro - bulbar tumours as carcinomata arising from the epithelium of the lacrymal gland . in intact rats the lacrymal glands are of a brownish colour ; in many of the thyroidectomized animals they were more whitish and appeared also to be more moist than normally . sometimes these changes were bilateral , but not infrequently only one side was affected . histologically in thyroxine - deficient rats , treated with a.f. 
whether the absence of thyroxine is the main factor responsible for the results obtained so far we can only state that thyroidectomy prior remains to be investigated . to the administration of the fluorene derivatives renders the livers of rats unsusceptible to the carcinogenic action without preventing the induction of neothyroidectomy performed after the administration of plasms in other organs . effective amounts of these compounds did not retard the development of malignant it seems therefore that it is the early stage in carcinogenesis liver tumours . preliminary results of experiwhich is influenced by the removal of the thyroid . ments yet to be terminated point into the same direction . bielschowsky and hall , 1952 ; during 1952 evidence was obtained by three independent groups of workers griffin , ( moon , simpson and evans , 1952 ; rinfret and corsigilia , 1953 ) that the action of highly potent carcinogens can be " inhibited " by the removal of the pituitary or of the thyroid . 
the growth and development of most organs , with the possible exception of the brain , is dependent on hormonal stimulation , but there exist considerable differences in degree , as shown by the effects of hypophysectomy . 
the gonads , thyroid and adrenals atrophy always , but if the hypophysectomized rat receives adequate amounts of food the growth of the liver is proportional to body growth . thus neither liver nor the subcutaneous tissue can be compared with the target organs of specific trophic hormones , although crude pituitary extracts can induce disproportionate growth in the liver ( selye , 1949 ) and in acromegalics the soft tissue can increase in size . the role of the somatotrophic or growth hormone in normal or pathological growth is only imperfectly understood . 
growth can be promoted in hypophysectomized rats not only by somatotrophin but also by thyroxine , as shown by geschwind and li ( 1952 ) , or by insulin ( best , 1952 )  . 
a great variety of neoplasms has been obtained in intact but not in hypophysectomized rats injected for long periods with purified growth hormone ( moon , simpson , li and evans , .oestro1950a , 1950b , 1950c , 1951 ; koneff , moon , simpson , li and evans , 1951 ) gens can retard growth by inhibiting the production of somatotrophic hormone . this does not prevent carcinogenesis . 
 ( 1950a , 1950b , 1950c , 1951 ) as well as griffin and his collaborators ( 1953 ) used carcinogens which acted on one organ only . their results could be due to a failure of the hypophysectomized rat to metabolise the compound administered into the carcinogen proper . this possibility has to be considered since the discovery by bonser , clayson , jull and pyrah ( 1952 ) that 1 - hydroxy 2 - naphthylamine is the active agent when 2 - naphthylamine is administered . however in our case , the fact that extrahepatic tumours developed while the liver , the most susceptible of all organs in the intact male rat , failed to respond to the carcinogenic action of a.f. 
and its acetyl - derivative does not favour this interpretation . some of the neoplasms found in the thyroidectomized animals are so rare in our material that we cannot be quite sure that they were due to the action of a.a.f. neither in normal nor in experimental rats of our colony have we ever observed a papilloma of the stomach arising from the glandular mucosa or a tumour of the brain , but vasquez - lopez ( 1945 ) as well as hoch - ligeti and russell ( 1950 ) have described gliomas in rats treated with a.a.f. benign tumours arising in the mucosa of the uterus are not infrequent in aged rats of however , the tumour depicted in fig . 
3 differs from all others our colony . observed by its strong resemblance to a deciduoma . in dunedin carcinomata aiising in the lacrymal glands have been found only in four a.a.f. 
no account of the state of the endocrine organs was given . in our experience a low fat content of the diet per se does not favour the development of cancers of the lacrymal glands . 
of tissue was homogenised in a total volume of 50 ml . , more sucrose being added later to dilute the homogenate to this , as was shown by direct comparison , a final concentration of 10 per cent . had no effect on subsequent fractionation . it was found in preliminary experiments that maximal liberation of cytoplasmic proteins into the supernatant fluid was achieved by homogenisation lasting for 1 to 2 minutes . the separation of the cell components was carried out by means of differential centrifugation at a temperature of 20 to 40 c . 
in a " spinco " ( specialised instruments corporation , belmont , california ) model e ultracentrifuge , except for the preliminary removal of nuclei , unbroken cells , debris , etc . , which was carried out in an ordinary low - speed centrifuge . 
the centrifugal procedure with some modifications was based on those , originally described by claude ( 1943 , 1946 ) and developed by hogeboom , claude , and hotchkiss ( 1946 ) , hogeboom , schneider , and pallade ( 1948 ) , schneider ( 1946b )  . in some of the later experiments it was based on that of schneider and hogeboom ( 1950a )  . 
stickland oxidase activity of each fraction was determined by the method described by umbreit , burris and stauffer ( 1945 ) and the results expressed as q02 ( n )  . 
a concentration of the enzyme in this fraction was also found in normal lactating breast tissue of highand low - cancer - strain mice . while the microsomal fractions of rat and mouse liver showed only a small amount of the enzyme , the same fractions of breast tissue revealed an appreciable quantity of it . in order to establish that this activity was a true property of these fractions , on some occasions the activity was determined after washing and was found to be unaltered . these results expressed as specific activity of the enzyme in the respective fractions are shown in table iii . 
hogeboom and schneider ( 1950 ) observed partial inactivation of succinoxidase after sonic disintegration of mitochondria . the possibility of contamination with mitochondria could not be excluded by histological examination alone . mitochondria were invariably observed in smears of microsome fractions , but in considerably smaller numbers than in the mitochondrial fractions : it is , however , impossible to make such comparisons quantitative . 
the chief arguments against contamination with whole mitochondria are first , that in rat liver no succinoxidase was found in the microsomes ( or negligible quantity ) , and second , that in a number of experiments with mammary tumour tissues the same mitochondria were sedimented in two parallel ways , at 5000 times gravity and at 8000 times gravity , and in the latter case the activity of the microsomes subsequently obtained was only slightly lower than in the former . the possibility of contamination of microsome fractions by fragments of broken mitochondria cannot easily be disposed of . clearly such contamination was not observed in liver microsome fractions , obtained in similar manner as those from normal and malignant mammary tissues . 
the results showed clearly that mitochondria from normal and malignant mammary cells of mice are not more fragile than those from liver , and if anything rather less . it can therefore be deduced that mammary cell mitochondria are not appreciably fragmented during homogenisation , and that consequently the enzymic activity present in the microsome fractions from these cells is likely to be a true property of microsomes present in these fractions . 
the ready fragmentability of liver - cell mitochondria in the potter - elvehjen homogeniser after they have been separated from other cell components is at a first glance not easily reconciled with the fact that no damage appears to occur to these cellular components during the homogenisation of the tissue . this difference is presumably due to the protection of the mitochondria against friction and damage by the presence in the latter case of larger cell fragments . the enzyme activity of microsomal fractions of normal and malignant breast tissues remained practically unaltered in spite of washings in isotonic sucrose 258 l . 
stickland solution , which again points against the possibility of the enzyme being adsorbed on microsomes . from the experiments of price , miller and miller ( 1948 ) , price , miller , miller and weber ( 1949a , 1949b ) on rat hepatoma and of schneider and hogeboom ( 1950b ) on mouse hepatoma , it is now known that in both rat and mouse hepatoma , the protein content of the mitochondrial and microsomal fractions is much lower than that in similar fractions of normal rat and mouse liver . further , it has been shown in these studies that in rat and mouse hepatoma the succinoxidase content of the mitochondrial fraction is lower than that in normal rat and mouse liver , the total activity being 5 times lower and the specific activity 2 times lower , in spite of the same distribution of the enzyme in normal and malignant livers . in the present experiments no significant difference was observed between normal and malignant mammary cells , either in the total amount of succinoxidase or in its distribution between the various fractions of these cells . 
a curious point , so far unexplained , is that although in liver homogenates 100 per cent recovery of succinoxidase could be obtained in the fractions , in mammary tissues the recovery was much lower , amounting on the average to only 70 per cent . no difference was found between highand low - cancer - strain mice either in the protein and succinoxidase content or in the distribution of these in the various fractions , but the mammary tumour tissue in each case showed a reduced content of mitochondria , compared with the normal mammary tissue , which agrees with that found by schneider and hogeboom ( 1950b ) in mouse hepatomas . the reliability of the simplified centrifugal procedure used in the majority of the experiments has been tested by the use on three occasions of the more complicated procedure of schneider and hogeboom ( 1950a ) , which gave substanit may perhaps be of interest to mention that stern tially the same results . ( 1939 ) demonstrated the association of succinoxidase with particles of microsome size in beef heart muscle . a small point worthy of mention is that for greater convenience of making the enzyme assays , the samples of washed particles from rat and mouse liver and mammary tissues were kept overnight at - 79 c . 
at that time research into their pharmacological and toxicological properties showed that certain of their effects were strikingly similar to those of ionizing radiation ( gilman and philips , 1946 ; kamofsky , graef and smith , 1948 ; philips , 1950 )  . this led to further investigations of their action as mutagenic agents and as growth inhibitors and their importance in these connections quickly became apparent . 
tumours were selected for treatment on the 6th or 7th day after implantation . the standard dose level adapted as the basis for comparison of chemical and x - ray effects was 1 mg . 
casarini analyses showed that 200 r might be considered to be an " equivalent " dose , i.e. , it produced in tumour and bone marrow the same amount and the same type of cellular injuries up to 24 hours after administration ( koller , unpublished )  . 
body weight throughout the experiments . for cytological analysis small pieces of tumours were fixed in acetic alcohol mixture ( 1 : 3 ) , and squash preparations were made and stained with feulgen 's for histological study fragments were fixed in bouin 's solution , basic fuchsin . embedded in paraffin wax , and sections cut at 5 . 
were stained with haematoxylin and orange - g . cytological effects : method of analysis . the method used for estimating cellular injuries is the same as was employed by devik , elson , koller and lamerton ( 1950 )  . cells in post - metaphase stages were selected . 
the importance of some biological variables ( age , sex , diet , etc . ) has already been discussed ; devil and coworkers ( 1950 ) demonstrated by analysis that the data , obtained by the same method as used in the present study , do in fact provide a valid basis for comparison . but as will be seen , the effects observed 72 hours after treatment by x ray and hn2 were in any case qualitatively so different that they could not be compared on a quantitative basis . x - ray effects : localised treatment ( 200 r )  . the tumours only were irradiated and cytological effects were analysed at 6 , 12 , 24 , 48 , 72 , 96 , 120 , 144 and 168 hours after treatment . 
date when the animal was killed . this is also the sample in which the number of chromosome fragments per cell is at a maximuthe damage is less 24 hours after irradiation , and it diminishes further in the 48 and 72 - hour samples . in tumours 4 to 6 days after treatment the number of dividing tumour cells with abnormalities is very small . our observations indicate that 200 r is insufficient to inhibit the growth of the walker carcinoma ; the growth rate of treated tumours 6 days after irradiation was found this finding is in close agreement with that to be the same as that of the controls . of devik and co - workers ( 1950 )  . hn2 - induced cytological effects . it has already been reported by the senior author that a dose of 1 mg . 
by including such cells in the analysis , the true number of injured cells is reduced ( compare the 144 and 168 hour samples , table iib )  . ' 0060 - / time after treatment in hours fig . 
they are particularly evident in young tumour implants and are found in large numbers at the periphery of growalthough these cells are normally present in the walker carcinoma , ing tumours . they play a small part in the histological organisation of the tumour . 
the great and rapid increase in histiocytes after hn2 administration , which takes place in the cellular tumour parenchyma , has important consequences . table iib shows the drastic change which occurs in the cell composition of the tumour . 
the proliferation of those tumours cells which may recover from nuclear or cytoplasmic disturbances was found to be seriously hindered by the altered environmental conditions . establishment of a solid tumour parenchyma does occur occasionally in the region of the connective - tissue capsule . 
the histological structure of this particular region is known to differ greatly from that of the tumour , and the different type of reaction to hn2 is presumably correlated with this . in conclusion we wish to emphasize the important fact that 72 hours after hn2 administration a series of changes takes place which result in the complete transformation of the histological structure of the walker carcinoma . 
the effect is , however , temporary ; the animals were already gaining weight again 7 days after treatment . in this respect the effect of hn2 is much more drastic than was observed after  . 
body weight ( intraperitoneal injection )  . while the cellular injury in the femoral bone marrow induced by 500 r was much more drastic than that produced by the hn2 " ld50 - equivalent " this x - ray dose was found to be still insufficient to bring about by way of the systemic effects the same amount of cellular and the same kind of histological changes which have been observed after hn2 administration . 
the delay in the developmental cycle may last 12 hours . this is indicated by the fact that in the 12 - hour sample 6 cells with chromosome injuries were observed out of 27 in which the chromosome abnormality suggested that they were already the frequency distribution of the injured cells in mitosis during irradiation . observed in the various samples is a further indication that cell development has been retarded . while the highest proportion of injured cells is seen 12 hours after exposure to 300 r , the maximum damage was in the 48 - hour tumour sample 182 p . 
the true significance of this observation lies in the relationship which it has to the primary reactions induced by the two ' agents . the view is now widely accepted that during irradiation ionisation takes place in the cell , followed immediately by the formation of free radicals of the water molecules ( lea , 1946 )  . this event represents the first step in the complex similarly reaction - chain which in time leads to a definite biological phenomenon . there is no substantial delay between administration of hn2 and its primary reaction in the organisthe rate of hydrolysis of nitrogen mustard is extremely high in a biological system , and it has been shown recently by batemann , klopp and cromer ( 1951 ) that it remains " active " only for a few minutes after intravenous injection . this is the main reason which allows us to compare the cellular effects of x ray and hn2 in tumour samples taken at the same time after treatment and to determine the relative sensitivity of the various stages of the mitotic cycle . the measure of sensitivity of a cell is the frequency of chromosome injuries observed at a given time . 
the interval between treatment and fixing the cell for analysis indicates the cell stage during treatment . using this criterion the radiation sensitivity of the mitotic cycle has been determined in pollen grains of tradescantia ( koller , 1946 )  . if our present data are interpreted on the same criterion , then we must draw the conclusion that tumour cells of the walker carcinoma are most sensitive to x rays at the end ofthe resting stage or beginning of prophase , while they are least sensitive to hn2 at this stage . 
revell ( 1952 ) employed a new and critical method in the study of chromosome effects of several substances ( mustards , epoxides , etc . ) and came to the same conclusion . 
the fact that x ray ' and hn2 initiate their effects at different stages strongly suggests that their mode of action is different . thus , for instance , we may assume that x rays act directly on definite linkages of the already synthesized polypeptide structure of the prophase chromosome thread , while a chemical agent affects the ' resting stage chromosome - filament either before or during the process of synthesis . this aspect of the chemical effects is discussed in more detail by revell ( 1952 )  . the higher sensitivity of the resting stage to the chemical agents has another implication . 
the non - dividing ( intermitotic or " resting " ) cells are ' believed to be functionally the most active cells , and often referred to as cells in the " metait is not unlikely that the degeneration of many bolic phase " ( hughes , 1952 )  . non - dividing tumour cells which we observed after hn2 administration is due to a gross disturbance in this metabolic phase . if it is found that chemical agents act preferentially on cells in the resting stage , a new approach may possibly be opened to the chemotherapy of cancer . because the functional or morphological characteristics of cells are determined 184 p . 
our experiment demonstrated such difference between tumour cells and histiocytes . the study of the cytological behaviour of the walker carcinoma under x ray and hn2 treatment has accordingly led to the conclusion that the mode of action of these agents differs , and there is other experimental evidence of different kinds to support this conclusion . 
no such reduction was observed when nitrogen mustard in barley , mutations of particular genes was used ( auerbach and moser , 1951 )  . were induced with a higher frequency by hn2 than was expected , indicating some specificity of action ( gustafsson and mackey , 1948 )  . 
cytological analysis of the femoral bone marrow and implanted walker carcinoma of the rat has shown that up to 24 hours after treatment , 200 roentgens produce the same amount of chromosome injuries as 1 mg . 
the difference in behaviour shown by the walker carcinoma after irradiation and after nitrogen mustard treatment indicates that the primary basic reactions initiated by these agents are fundamentally different . this investigation has been supported by grants to the royal cancer hospital and chester beatty research institute from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the national cancer institute of the national institutes of health , u.s. 
the centrifugary - cleared extract was adjusted to i per cent with 20 per cent saline and the crude mucoprotein , etc . , precipitated by addition of two volumes of alcohol . 
the washed deposit was redissolved in 1 per cent saline , adjusted to ph 7 - 5 , and digested for 24 hours at room temperature with commercial trypsthe mixture was then filtered with the aid of hyflo super - cel and reprecipitated with 2 volumes of alcohol . 
the yield of protein - free , crude polysaccharide was about 2 per cent of the acetone - dried tumour tissue . the material contained polysaccharide and pentosenucleic acid , and the analytical data were : nitrogen ( kjeldahl ) varying between 5 - 2 and 6 - 3 per cent ; phosphorus ( fiske and subbarow ) 1 - 7 to 1 - 8 per cent ; and sulphur ( paulson ) 0 - 6 per cent . 
the ninhydrin reaction was negative . metachromatic sta ' m ' mg with azure a ( sylv6n and malmgren , 1952 ) revealed the presence of one orthochromatic component and another presenting alcohol - resistant metachromatic precipitates . 
d was also degraded by testis hyaluronidase at a similar rate to other such hyaluronates . glucose ( glucosamine ) could be demonstrated by following acid hvdrolvsis onl paper electrophoresis in borate buffer ( consden and stanier , 1952 )  . in addition , infra - red spectral measurements kindly performed by s . 
the two spectra were identical in the region 680 - 980 cm . - ' , showing the two materials to have the same molecular skeleton ( orr , 1954 )  . 
the only difference lay in the relative intensities of the bands due to the acid and amide carbonyl groups . however , the acid : amide ratio in sample d cannot be more than 5 per cent greater than that in the purified umbilical hyaluronate . nature of the_8uiphur - containing material . the metachromatic precipitate formed by azure a treatment of sample b was almost insoluble and further information about its composition could not be obtained . 
attempts were therefore made to remove the nucleic acid and the hyaluronate from the starting material by successive ribonuclease and hyaluroafter removal of the hydrolysis products by dialysis it was nidase treatments . thought possible to obtain the s - bearing material in a purified and soluble state . however , this latter material exhibited a powerful inhibitory effect on hyaluroin one experiment , when 30 mg . 
the s content of the remaining non - digested material was 0 - 49 per in the course of this long digestion , however , a small precipitate was cent . formed , which had a n content of 10 - 0 per cent and s content of 4 - 8 per cent . these figures suggested that a new product had been formed between the protein hyaluronidase and a s - containing polysaccharide . if the polysaccharide is assumed to contain 3 per cent nitrogen , the nitrogen value of the precipitate would fit a protein content of about 55 per cent , and hence a polybaccharide content of about 45 per cent . 
the intermediate protein - free material ( sample a ) contained about 70 per cent hyaluronate , 25 per cent nucleic acid , and about 5 per cent of a sulphur - be ' aring polysaccharide presenting some biological characteristics of heparthe largest part of the polysaccharide material present is thus beyond doubt hyaluronic acid with identical molar characteristics with that obtained from mammahan sources . 
the rous hyaluronate has probably a lower particle size than the hyaluronate from normal tissues , and the high viscosity of the intercellular rous material seems partly due to the protein components . the identification of heparin in the sulphur - bearing polysaccharide has not been fury established . 
the same study indicated that an excessive output of ethanolamine frequently occurred in the urine of patients with severe parenchymal liver disease , but that in such cases it was always accompanied by an excess of many other amino - acids . 
the presence in the urine of large quantities of ethanolamine , as an isolated abnormality , in the patient with primary carcinoma of the liver was therefore of some interest . its excretion might have resulted from a disorder of metabolism consequent on non - specific liver damage or from some peculiar form of neoplastic cell metabolism ; or it might even have represented a hitherto unrecognised error of metabolism which preceded and led to the development of a primary carcinoma in the liver . it has for some years been recognised , as a result mainly of animal experiment , that ethanolamine plays an important role as an intermediary in the metabolism of phospholipids and amino - acids . 
1. - some metabolic inter - relationships involving ethanolamine and other compounds . experimental dietary deficiency of choline has also been extensively studied . in rats it has been shown to lead to the production of fatty livers , followed after some time by cirrhosis . 
more recent work has shown that this may be followed eventually by the development of hepatoma - like tumours ( copeland and salmon , 1946 ; staub , viollier and werthemann , 1948 )  . furthermore , choline deficiency of a severity not sufficient to produce cirrhosis predisposes the liver to the carcinogenic action of butter yellow ( opie , 1944 ; buckley , buckley and snipes , 1951 )  . in the human hepatomata that occur in tropical countries there is ample evidence that dietary factors are concerned ( berman , 1951 )  . 
il - , a housewife , was aged 45 years at the time of her death in 1950 . apart from an attack of jaundice at the age of 7 she was in good health until april , 1939 , when , at the age of 34 , she had a febrile illness with delirium and a she had a second similar attack in october that year , and productive cough . this , like the first , lasted about 3 weeks . she suffered from similar attacks each in that year her illness was more severe and was associated winter until 1942 . with generalised aches and pains and vomiting . since that time she suffered from morning vomiting and also a burning pain , relieved by alkalis , behind the despite these regular winter illnesses and an increasing lower end of her sternum . sense of tiredness she continued with her work in a munitions factory until 1945 . from then until her death in 1950 she worked as a housewife . in january , 1947 , she first noticed a painless lump in her abdomen . in march of that year , following an illness with fever and malaise , she noticed that her abdomen was becoming tender to touch , her appetite was failing and the morning vomiting was becoming more severe . it was at this time that she was first seen and admitted for investigation at university college hospital . both parents and her 4 siblings were all alive and well . examination revealed a pale , slightly cyanosed , nonicteric woman of 8 st . 
the pulse was regular at 90 and the blood - pressure was 110 / 60 mhg . there were rhonchi over both lung fields and bilateral basal rales . in the nervous system the pupils were normal , the kneeand ankle - jerks were absent and the plantar responses were flexor . 
was normal , the circulation time was 17 seconds from arm to lung and 35 seconds from arm to tongue . the cyanosis was rapidly and completely relieved by breathing oxygen . whilst in hospital she ran a continuous low - grade fever . 
the metabolic studies carried out during this period are described later . opportunity was also taken at this time to examine chromatographically the urines of both parents and the other 4 siblings ; all showed a normal concentration and pattern of amino - acids . at the conclusion of the metabolic studies the patient went home much improved for her fortnight 's rest and largely pain - free for the first time for 2 years . she was instructed to take methionine 1 g . 
ethanolamine labelled with 50 per cent atom excess of 15n . on june 21 , 1950 , she was readmitted to hospital with an attack of bronchopneumonia . apart from her chest infection and gross oedema of the legs her general condition was unchanged . she volunteered the information that since taking choline her abdomen had felt looser and had been less painful . pneumonia was successfully treated with penicillin , and whilst on this her fever was . 
cameron reported on the histological sections of the liver as follows : " the tumour is undoubtedly a hepatoma ; it has not changed in character between 1947 , when the biopsy was taken , and 1950 . the most notable 170 c . 
each 24 - hour urine was analysed chromatographically for amino - acids and chemically for in addition blood specimens were drawn soon after the last dose ethanolamine . of each supplement had been taken and were analysed for amino - acids . further 24 - hour urine specimens were collected from her as an outpatient after she had been for 4 weeks on 10 g . 
7. apart from the very strong spot given by ethanolamine the remaining spots are of similar strength and pattern to those found in many normal urines . there was , however , an increase to a slightly abnormal level of the strength of the cystine spot during the patient 's last few months of life , and the unidentified weak " under proline " is not commonly found in urine whether normal or pathological . 
the only clearly identified gross abnormality was , nevertheless , the increased excretion of ethanolamine . these results clearly suggested that the ethanolamine was not the result of variable extrinsic factors ( such as diet ) , but was more likely to be due to a continuing metabolic abnormality . the plasma chromatograms were quite normal , except for a faint trace of ethanolamine . this indicated a definite , if slight , increase in the ethanolamine concentration of the plasma since the quantity ( 625 ' , d . ) of desalted plasma ultrafiltrate analysed was not sufficient to reveal the ethanolamine present in the plasma of a normal person . 
the urine to be analysed was placed at the right - hand bottom comer of the paper . phenol was run as the first solvent in the direction from right to left , followed by collidine - lutidine in an upward direction as the second solvent . 
8. - section of rat hepatoma kindly provided by copeland . hepatocellular type of tumour produced by prolonged feeding on a choline deficient diet ; ( no carcinogens added )  . note the difference from the histology shown in the illustrations of the tumour of c . 
9. it is seen that the output of " apparent ethanolamine " increased most on the day after the ethanolamine had been given and was probably still increased on the second day . 
the " increase " after serine was almost certainly due entirely to serine and not to additional ethanolamine , since the chromatograms showed a greatly increased serine output on this day and serine also gives rise , in the assay method , to its equivalent of " apparent ethanolamine " ( see above )  . 
walshe it has been involved were very small and the " spots " only just detectable . shown that many of the known amino - acidurias result mainly , if not entirely , from a raised renal clearance ( low threshold ) for amino - acids ( dent , 1951b )  . is not necessary to invoke this mechanism as a cause for the ethanolamine excretion here , since the normal subject who took ethanolamine by mouth produced a comparable urinary output at an induced blood level roughly similar to that of the patient . 
we suggest that it can best be understood in terms of an increased membrane permeability , on the part of the tumour cells , for ethanolamine . if such abnormnal permeability existed , a larger percentage of the loading dose of ethanolamine would pass from the extra - cellular fluid to the cells of the patient than it would in the case of the normal control . 
the urine from 7 cases of extensive secondary carcinoma of the liver ( appendix b ) was also investigated with negative results . it is not clear from the evidence at present available whether there is a specific , though rare , type of hepatic neoplasm characterised by an increased urinary excretion of ethanolamine or whether any tumour , if large enough , would give rise to a similar finding . 
ch3 + ch3 ch20h ( c . ) ch2n ( ch3 ) 2 + ch3 ch20h ( d . ) ch2n ( ch3 ) 3 ch20h ( choline )  . but , as has been mentioned already , we now prefer the theory of an increased membrane permeability for ethanolamine . 
the principal objection , perhaps , to the theory of a metabolic block is that if it were appreciable im extent it should have resulted in some degree of choline deficiency as well as in the accumulation of unmetabolisable ethanolamine . in experimental animals choline deficiency leads to fatty infiltration of the liver followed by fibrosis and , if sufficiently 176 c . 
we are , therefore , unable to accept the possibility that the large urinary excretion of ethanolamine resulted from a disturbance of the known metabolism of choline or one of its important intermediate metabolites . 
we prefer to believe that it was caused by some other property of this particular type of heptoma , such as a disturbance of " cell membrane permeability . " a further problem has been posed by the complete failure to increase the excretion of ethanolamine in the experiments in which large doses of its known biochemical precursors ( glycine and serine ) were given by mouth . this fact appears to underline further the difficulties encountered in attempting to interpret the results of this type of " classical " experiment . presumably the compounds failed to reach the cellular site where they would have been converted into ethanolamine and , therefore , that our patient did not provide a suitable opportunity to study normal ethanolamine metabolism by the rather crude methods at out disposal . 
the prospect of success would have been much greater using isotopically labelled precursors , since isolation from urine of pure samples of ethanolamine for isotype analysis presents no great difficulty . in conclusion we wish to thank sir harold himsworth for permission to publish this case , professor m . 
copeland for his very great kindness in lending us his original blocks of rat hepatoma tissue ; also the following for permission to investigate the cases referrred to in the appendices : a . 
a chemical method of analysis suggested that the output of ethanolamine this was confirmed by a rough quantitative was of the order of 0 - 5 to 1 - 0 g . 
as this substance is probably not readily taken up even in normals from the extracellular fluids by the tissue cells or from the glomerular filtrate by the renal tubule cells , it was therefore readily excreted into the urine . 
the presumed source of the ethanolamine was the neoplastic liver cell , and the enormous mass of these cells ( about a quarter of her body weight ) in the patient was probably sufficient to account for a greatly excessive production of this compound . 
he had a cholecystectomy for gall in 1950 he had an attack of renal colic and a ureteric calculus was stones in 1942 . in 1951 he was admitted to hospital with severe upper abdominal and demonstrated . laparotomy revealed a moderate enlargement of the liver , with left shoulder pain . very numerous white opaque nodules scattered throughout the liver substance . 
h - , aged 53 years . apart from a cholecysfectomy in 1950 he was in good health until shortly before admission to hospital when he was seized with a severe low back pain , greatly aggravated by movement . 
a diagnosis was made of carcinoma of the bronchus with secondaries in the lumbar spine and liver . his course was marked by very rapid enlargement of the liver and progressive cachexia . 
nielsen. from the danish cancer registry under the national anti - cancer league , copenhagen , denmark . received for publication april 30 , 1951 . in comparing mortality figures for cancer from various countries for the years around 1938 , clemmesen and busk ( 1947a , 1947b , 1948a , 1949a , 1949b ) found that while denmark ranked third for total mortality from cancer , her figures for females were highest among the countries investigated , surpassing even switzerland and england , for which countries the total mortality was higher . appeared that the high mortality figures for danish women were caused primarily by a high mortality from cancers of " accessible site . " from figures given in the series of articles quoted , it is seen that the incidence of cancer as expressed by the figures from the danish cancer registry for 1942 to 1944 was higher for copenhagen than for the provincial towns , which in their turn exceeded the incidence for rural areas . consequently , in the following paper the incidence of cancer in copenhagen will be studied separately , with particular reference to social conditions , social class being expressed in terms of annual house rent for various subdistricts of greater copenhagen . it is an established fact that expenditure on housing is a more reliable indicator of the social status of a family than the annual income of the breadwinner . 
the level of house rent in copenhagen was fixed during the period studied , and the wartime shortage of housing which prevailed during the entire period must have restricted the number of changes of residence . 
hence several factors working together tended to stabilize some of the variables which would be inclined to disturb a study such as this . the city of copenhagen , the capital of denmark , has one million inhabitants , another million live that is , about a quarter of the total for the whole country . in the provincial towns , and two millions in rural areas . medical facilities in copenhagen left very little to be desired during the period examined , in spite of current political and military events . 
nielsen the reference of cases of cancer to distinct geographical location has , however , inforin the present study been made without regard to the place of treatment . mation on cases was collected by the cancer registry , and each case was referred to the subdistrict corresponding to the address of the patient when first seen in hospital for cancer . 
the cancer registry collects notifications from hospitals all over denmark of all cases of cancer seen , and separately of all post - mortem examinations performed on cases of cancer . for patients not entering hospitals it is assumed that death certificates will give sufficient information , but it will appear that such cases amount to rather insignificant numbers in copenhagen . further details of the activities of the danish cancer registry have been given elsewhere by clemmesen and busk ( 1948b , 1948c ) clemmesen , busk and nielsen ( 1949 ) , and clemmesen ( 1950 , 1951 )  . the subdivision of the greater copenhagen area into 22 subdistricts used for the present study had originally been worked out for various administrative purposes , and proved useful because detailed figures for the distribution of the population by age were available for each subdistrict . 
the wealthy boroughs of frederiksberg and gentofte had , however , to be treated as separate entities because ot the absence of such information for their subdistricts . after a careful analysis of the figures for each site of cancer in each of the 22 subdistricts , it became possible to collect subdistricts within the same range of house rent into however , the average annual house rent of five major classes or " districts . " each subdistrict is given together with the relative values for cervical , mammary and pulmonary cancer in table v . in order to describe the material from a medical point of view table i has been worked out . 
we denote the observed number in subdistrict v comprising all age groups . by l we denote the total number of person - years of exposure , and by c the addition of the subscripts v computed number of persons developing cancer . and s to l and c has the same meaning as described for 0 . if the morbidity from cancer were identical for all subdistricts of the town , we would expect the number of cancer cases at a given age to be distributed on the subdistricts in the same manner as the number of person - years of exposure for a given age . consequently we obtain the computed number c , 8 from the equationlvs . and this number should be compared with the observed number ov.. now the number ov , , is usually small ; we therefore take this number for all age groups and make the comparison for all of them at the same time . 
nielsen pondingly the incidence of cervical , mammary and pulmonary cancer is given as a percentage of the values computed for each subdistrict , with full allowance for differences in age distribution of the population o.. 
nielsen between the social status of the various subdistricts and the incidence of cervical cancer demonstrated in table v is striking to anybody familiar with the city . the irregularity presented by district ii , which mainly consists of the borough of frederiksberg , showing an unexpectedly high frequency of cervical cancer , can by no means be ascribed to a particularly high birth rate in the borough , since this rate is lower than for gentofte , and also lower than the average for the - ~~~~~.... . 
from these areas patients with cervical cancer are centralized for treatment in the radiumstations of the anti - cancer league , situated in the towns of copenhagen , aarhus and odense . 
nielsen connection with the development of cancer , it should be pointed out that the cases have been puboccurrence of cervical cancer in virgins is questionable . lished of cervical cancer in children ( heckel , 1950 ) , but these have been adenocarcinomata , so that it may be desirable in statistical work to separate this group from squamous cell cancers of the cervix . 
paper the clinical aspects of androgen therapy in 70 cases of advanced mammary cancer in women are described , the literature surveyed , and the effect of androgens compared with that of castration carried out by surgery and by the prophylactic use of androgens in mammary cancer as x - irradiation . described by prudente ( 1945 ) is not discussed here . the investigation was begun in december , 1947 , and since then sufficient experience has been gained to permit an assessment to be made in general terms of the place of androgens in treatment . 
the pellets were inserted through a skin incision 1 clong in the lower abdominal quadrants , and pushed through radially to rest on the external oblique aponeurosis between 5 and 10 cfrom the incision , the pellets lying at points on a circle with the incision as centre . absorption from these pellets depends on a variety of local factors , including their relation to surrounding fat , adjacent fascia , lymphatic plexuses and encapin three patients who came to autopsy 55 , 82 and sulation by fibrous tissue . 93 days respectively after insertion , the pellets were removed , allowed to dry for 48 hours and weighed . 
per month for their evocation when injections of testosterone propionate are used ( geist , salmon and gaines , 19388 ; geist , salmon and walter , 1940 ) , representing daily doses of nearly double the maximal ( initial ) daily absorption from ten 100 meg . 
were given 3 - 7 times weekly , but later opinion came to advocate larger and larger doses of the order of 100 mg . daily , or even twice daily . the authors of the latest progress report of the council on pharmacy and chemistry ( 1949 ) , however , no longer favour heavy dosage , and consider that there is no advantage in exceeding 150 mg . 
daily for the first 2 - 4 weeks , given . to halve this dose if the patient is responding favourably , or to continue for another all 30 patients who derived month if there is no evidence of specific benefit . benefit from androgen therapy showed clear evidence of it within 8 weeks , and in most cases within the first month . 
no patient who failed to respond after 8 weeks of treatment did so after a longer interval , and it is probably not worth continuing treatment after 10 weeks in the absence of specific response . cannot be said from the small number of cases in this series whether such cases should be transferred to testosterone propionate injections , but the general impression gained has been that patients likely to benefit substantially from androgen therapy are extremnely sensitive to its action , in whichever form it is given , and do as well on doses just large enough to suppress inenstruation in the average premenopausal woman as they do on inuch larger doses . 
on the other hand , most cases which fail to respond to the smaller doses do no better when the dose is increased or the route of administration changed , but the minority which does so led to the tendency already mentioned to advocate heavy dosage . patients given methyltestosterone were advised to leave the tablets ( 50 mig . ) under the tongue , and to allow them to dissolve without chewing or swallowing . the time taken for solution varied between 10 and 30 minutes in different individuals , and a few patients disliked the bitter taste of the substance . duration of treatment in cases responding favourably . no definite recommendation can be given with regard to the length of time cutler and schlemenson , reporting 19 cases , administration should be continued . advised continuing injections until palliation was no longer being obtained the american council already referred to ( cutler and schlemenson , 1948 )  . found that the most favourable results were obtained when injections were conin this series it has frequently tinued until a total of 3 0 g . 
methyltestosterone daily , commenced 6 months after the second implantation and continued for a further 4 months . widespread evidence of fresh activity of the carcinoma then appeared , accompanied by recurrence of pain testosterone propionate injections 100 mg . 
as far as the effect on menstruation is concerned , it may therefore be said that the hormone absorbed from 50 mg . sublingual methyltestosterone is less potent than 10 mg . 
testosterone ( table marked facial hirsuties was present in the second of these cases at the ii )  . time of death , 12 weeks after implantation , not more than 250 mg . 
amenorrhoea persisted for weight gain , 4 months , and weight gain continued during the same period . and subjective benefit , occurred without other side - effects in patients who were it therefore appears that the given methyltestosterone in 40 mg . 
in the first month are bilitated patients is very striking . common , and with the other " tonic " effects are independent of the specific effect in case 65 for example 7 lb . 
in the second 4 months . clinical oedema , however , was seen in only 3 cases , and was always slight in in a few of the amount , and confined to the ankles and lower half of the legs . patients with post - mastectomy oedema of the arm , an increase in the swelling of the arm followed testosterone administration , but this was more closely related to spread of the disease than to the treatment , for when lesions regressed , the lymphoedema sometimes diminished , even when rapid increase in weight was during the initial period of weight gain , some of the occurring , as in case 44 . patients stated that they passed less water , but no measurements have been carried out . much of the initial rapid weight gain is due to the effects of electrolyte , and particularly sodium retention , which holds equivalent quantities of water in the body . this effect is a feature of the activity of many steroid hormones , notably progesterone , oestradiol , and of kendall 's compounds desoxycorticosterone , e and f . 
daily for 6 months and 1 year respectively . they were abundant across the back , and were also present on the cheeks and chin . the skin , which was heavily infected , had the lumpy appearance typical of adolescent pustular acne . in case 44 hirsuties was nminimal , consisting of a sparse growth of soft hairs on either side of the upper lip , but was much more developed in case 63 . in 7 cases facial hirsuties reached an extreme degree , the sides of the face being covered with thick downy hair between 1 and 2 clong ( cases 7 , 9 , 24 , 25 , 56 , 63 )  . in cases 9 and 56 , after 6 months ' treatment the hairs increased in calibre , and resembled the stiff bristles of the male beard . there was some variation in the changes in the scalp hair . 
when fully developed they form a characteristic syndrome , which has been observed in 3 patients in this series . it was first seen when 2 patients ( cases 10 and 45 ) were given 80 mg . 
testosterone. in case 10 , after taking the tablets for 2 days , the patient complained of extreme weakness , drowsiness , severe headache , nausea , and increase in the dyspnoea which was her initial complaint , and due to pulmonary and pleural metastases . 
the symptoms subsided rapidly after she stopped taking the tablets . in case 45 the patient took the tablets for 5 days , during the last 3 of which she felt generally ill , nauseated , and complained of increase in the severity of her backache . 
on the 5th day she was distressed by vomiting , abdominal distension and pain , and took no more tablets , after which her condition improved rapidly . one week later she again attempted to take the tablets , but with exactly the same result . case 30 was a woman of 45 who had been previously treated for 2 years by repeated doses of x - rays for widespread skeletal recurrences for a stage iv carcinoma , and had had induction of an d . 
daily for one month , towards the end of which she complained of increase in the severity of her pains , dizziness , nausea and vomiting , and general malaise . 
the symptoms abated within a day or two of discontinuing the drug . she was asked to resume the tablets a fortnight later , but the symptoms recurred after one week . case 47 , doses of 35 mg . 
by a " moderate success " is meant a case in which symptomatic relief was short - lived ( mostly less than 6 months ) , or not accompanied by considerable objective evidence of regression or by restoration of function . all other cases are classed as failures , even when non - specific benefit was marked and increased the patients ' range of activity . 
testosterone propionate three times weekly without benefit after 6 weeks . she is classed as a " moderate success " in view the remaining patients obtained less benefit , and 3 were of the initial response . never able to leave their beds , although all volunteered that their pains were improved . one of these declared that she had not felt so well nor had so little pain for 2 years , 20 months of which had been spent in bed . case 66 was a woman of 44 years with extensive metastasis to the spine which was responsible for gross collapse of the bodies of dorsal vertebrae 7 - 11 . had been unable to walk or stand for 6 weeks owing to severe proprioceptive loss in both legs , a short course of radiotherapy having conferred no benefit . 
a mild paraplegia was present , and there was some impairment of sensation to light touch , deep pressure and pinprick from the level of the umbilicus downwards . there was , in addition , a girdle of almost.complete anaesthesia to touch and pinprick over the distribution of dorsal segments 7 - 10 . curiously , sensation over the paravertebral regions of these segments was normal . there was no hyperalgesic zone , and no disturbance of sphincter control . the patient was given 28 daily injections of 100 mg . 
two other patients with dyspnoea as one in cases 3 , 10 , 24 of several symptoms obtained some relief after treatment . and 63 the rapidity with which the breathing improved was astonishing , and colnparable with the speedy relief of bone pain in the cases mentioned above . in case 25 , however , with dyspnoea at rest , no significant improvement had ten oz . 
galton with a conjugate defect of elevation , thought to indicate a lesion in the anterior this lesion could have been of vascular origin , part of the oculomotor nucleus . or might have been due to a metastasis . that the latter was the more likely is suggested by the development 6 months later of diminished sensation to touch this patient took methyland pinprick over the right trigeminal distribution . testosterone 50 - 100 mg . 
daily thereafter , also showed marked regression of axillary and supraclavicular lymph nodes , though some of these were still just palpable 4 months later . this patient relapsed 11 months later . case 35 was a stage iv growth in a woman of 36 years . she had nodes in both axillae . 
one year previously she had been given radiotherapy to the primary growth and to the axilla , and 6 months previously had been given pelvic five months later she was given irradiation for induction of the menopause . * methyltestosterone sublingually 80 nig . 
31 premenopausal cases with bone deposits . of the 31 cases , 3 received palliative radiotherapy to the affected bones ( cases 2 , 27 , 69 ) and are not included in the figures . 
of the remainder , 8 were premenopausal cases , all but 2 of whom received great benefit from androgen therapy . three of these were the bedridden patients referred to above , who were able to resume their normal activities within a few weeks of being treated with testosterone , and remained in good health for over 1 year in 2 cases ( cases 3 , 7 , 37 )  . 
the fourth was a housewife of 45 with extensive spinal , costal and pelvic deposits , whose activities were drastically curtailed by pain . she also secured complete relief from pain in the month after methyltestosterone therapy was d . 
galton begun and is well 6 months later ( case 26 )  . case 4 was a nulliparous woman of 49 complaining of pain in the left hip and right shoulder , the latter exacerbated by the smallest movements of the arm , active or passive . 
no deposits were seen radiologically to account for the hip pain , but the medial end of the right clavicle was swollen and tender , expanded by a tumour measuring 4 x 6 cm . after taking methyltestosterone 50 mg . 
daily for one month , the complete range of shoulder movements was restored , the patient was without pain , and the bony swelling no longer tender to percussion , this latter finding being a characteristic result of the treatment . six months later the swelling is slightly smaller , but intrathoracic metastases have appeared and the general condition has deteriorated . of the 3 remaining premenopausal cases , 1 ( case 47 ) , a para - 2 aged 38 , attended hospital 9 months after radical mastectomy with severe anaemia and pains in back , hips and shoulders . she was intolerant to doses of methyltestosterone greater than 30 mg . , and although the dose was increased in 5 mg . 
on 3 occasions the treatment had to be abandoned each time , owing to the sudden onset of headache , nausea , fever , drowsiness and increased intensity of the pains . these symptoms subsided within a day or two on withholding the hormone . case 66 , who presented with paraplegia of 6 weeks ' duration , has been referred to above . 
the last premenopausal case ( case 10 ) , a para - l aged 45 , had had a right radical mastectomy 2 years previously for a lump in the breast present for 1 year . she attended hospital with cough , dyspnoea , pain in the chest and stiff neck . 
methyltestosterone arising in submammary lymph nodes . daily , and in 3 months ' time was walking well and without pain . in addition surprisingly she the parasternal swelling had become greatly reduced in size . showed on examination 3 - 5 cof shortening of the right femur , but no impairment of movement about the hip - joint , within the limits imposed by the rigidity of her paralysis agitans , and the x - ray revealed an unusual subcapital fracture of the neck with downward and backward displacement of the capital fragment . the second case was of a nullipara aged 51 , who had been recurrence - free for 10 years after a radical mastectomy , when she developed backache , which persisted , increased in severity , eventually confining her to bed . multiple deposits of secondary carcinoma filled most of the dorsal and lumbar vertebrae , and all the pelvic bones . within a few days of the implantation of 500 mg . 
testosterone the pain abated , walking was quickly resumed , and she is pain - free 14 months later without further treatment . the nature of the pain is therefore open to question , but the patient gave no history of previous chronic backache , the onset of the pain coincided with the finding of multiple secondary deposits in ' the appropriate bones , and relief promptly followed implantation of a very small dose of testosterone . testosterone was also given to 5 young patients in whom an artificial menoin the first and last pause had been earlier induced ( cases 5 , 30 , 50 , 62 and 70 )  . of these cases pain was relieved , but in the first it was never severe , and in the last its recurrence followed the appearance of further metastases . the difference in response by premenopausal and postmenopausal cases just mentioned was not met with in the series of 70 cases described by adair , mellors , farrow , woodard , escher and urban ( 1949 ) , or in the larger series of 285 cases analysed by the council on pharmacy and chemistry ( 1949 )  . in adair 's series 9 out of 48 cases with skeletal metastases benefited from androgen therapy , but no difference in response was noted in premenopausal and postmenopausal cases ( 12 of the 48 cases were premenopausal , compared with 8 out of 28 in the present in the council 's series of 285 cases , the ages ranging from 25 - 79 years , series )  . favourable effects were evidently independent of age . 
no explanation is offered for this discrepancy . post - treatment changes in bone . it is difficult to account for the rapid relief of skeletal pain brought about by equally striking is the speedy disappearance of tenderness to testosterone . percussion of affected bones , and the later diminution in size of bony swellings radiologically all that can be observed are the due to subperiosteal deposits . changes in position and concentration of minerals in the neighbourhood of a deposit following testosterone administration , but these changes are characthey consist in the homogeneous deposition of minerals in the bone teristic . surrounding the deposit , so that at first the deposits acquire a more definite outline , and may appear more extensive in size and number . this is a common appearance 2 months after commencing treatment , but soon gives way to a more uniform but rather structureless appearance , as the areas of decalcification in the deposits become filled in from the periphery with deposited minerals . after 6 months this process usually comes to a standstill . it is questionable whether this confers increased strength on the bones in which it recalcification d . 
the same is true of cases with bone deposits , and in the illustrations in the first two papers just cited fresh osteolytic deposits are present in bones showing extensive recalcification round earlier deposits . several instances of this phenomenon have been met with in the present series . the paradox is probably to be explained by the fact that the metabolic processes accelerated by the androgen proceed most rapidly at the beginning of treatment , and then slow down to a stationary though raised level . 
he had learned of " the custom in certain countries to remove the ovaries of the cow after calving if it is wished to keep up the supply of milk , and that if this is done the cow will go on giving milk indefinitely , " and this " pointed to one organ holding the control over the secretion of another and separate organ , and thus explained the absence of that distinct nervous control that i pointed out as characteristic of the mamina . " beatson 's first case will be described in some detail , as it illustrates very well the kind of result that may be obtained by testosterone therapy as well as by castration . the patient was a married woman of 33 years , with 2 children , in fair general health , and menstruating regularly . three years previously she had noticed a lump in the breast while suckling her first child . this increased in size after the birth of her second child 20 months later . 
when first seen there was a mass 5 x 3 inches with ulceration of the skin of the breast over an area of 1 square inch and adjacent skin nodules . radical mastectomy was performed on 25 . 
95 , but 3 months later an ulcerated recurrence in the scar was found , and a fortnight later had increased in size to 21 x 31 inches . the whole chest wall was studded with skin nodules , but no lymph nodes were felt . 
95 the " largest area of disease " measured 1i x 2 inches . eight months later regression continued . the patient lived until april , 1899 , dying 46 months after castration , with fresh recurrences in skin and spine ( thomson , 1902 )  . seconid case was that of a woman aged 40 , with massive involvement of the whole breast by carcinoma , with extensive infiltration of skin , axillary and cervical nodes as far as the chin ; the opposite cervical nodes were also involved , and she complained of pain in neck and arm . after castration the pain was relieved , and regression and softening of the primary mass and of the nodes occurred , lasting 5 months . thus in the first 2 cases in which castration was used , shrinkage of the primary growth , regression of skin deposits and of involved nodes , general improvement , and relief of pain were described . six years later the method had been used extensively , and its value sunmmed up by beatson ( morris , 1902 ) as follows : " it is not easy to say beforehand if the operation will do good ; but from the cases recently published by abbe , of new york ( thomson , 1902 ; abbe , 1901 ) , it would seem that it is not contra - indicated after the menopause th ' value of an operation may be judged by statistics and by personal impressions . both may be deceptive , though both may contain in them the germs of truth . i believe that from both standpoints the evidence is in favour of the utility of oophorectomy in certain cases , in prolonging life and lessening pain . it has never , as far as i know , done any harm , and its mortality has been nil the treatment has been placed before the profession , because i felt that d . 
galton they should judge its effects themselves and if , in their opinion , after a fair trial , it is found wanting , then i hope it will be abandoned and forgotten . " oophorectomy passed out of fashion a few years later , and was slowly superseded by " x - ray castration , " and in the last 10 years by " medical castration " with androgens also . boyd ( 1900 ) reported the results of oophorectomy in 54 cases of mammary cancer . six cases out of 46 showed remissions lasting for 2 years or more , and 17 out of 46 derived some benefit , but in most of these , recurrences occurred between 6 and 12 months later . with one exception the treatment failed in all the patients who had passed the menopause , and the maximum benefit seemed to be derived by women over 40 and still menstruating . 
two years later thomson ( 1902 ) of edinburgh collected and published the results in 80 inoperable cases castrated by several surgeons . in 40 of the cases some imnprovement took place , although this was negligible in 11 , and only temporary in 11 others ( under 12 months ' survival following oophorectomy )  . 
in 18 , however , decided improvement was recorded , " remarkable " in 4 . thirteen cases survived more than 20 months , and 4 between 40 and 46 months . of the 29 more favourable cases , 6 had ceased menstruating , and 3 were 70 years of age , and of the 20 women still menstruating , 12 were between 40 and 50 years of age . 
thomson concluded that the value of castration , though limited , had been established beyond doubt , but , like beatson ( 1896 ) , stressed the unpredictability of the results . 
jessett " had operated on 5 cases , and admlitted that the patients complained of less pain , but in no single case was there any improvenment in the local disease . 
he also noted that beneficial results occurred sometimes after the menopause . bruce clarke recorded a case in which castration was followed within 6 weeks by rapid subsidence of pain and regression of a chest wall recurrence , the patient being in good health 5 years later . in this case unfortunately the age was not stated , but the original excision of the growth was performed 2 years before castration , and a recurrence excised 1 year before ( lett , 1905 )  . in spite of the well - documented reports described above , castration for mammary cancer fell out of favour , no doubt because of the absence of precise indications , the large number of poor results and the increasing success obtained by local radiotherapy . morris ( 1902 ) stressed the difficulty of assessing the results , and compared " beatson 's treatment " with the favourable results claimed for the injection of coley 's fluid ( heat killed broth cultures of streptococci obtained from erysipelas lesions , and of bacillus prodigiosus ) in cases of spindlecelled sarcoma . 
he found that in the cancer - bearing group the incidence of complete oophorectomy before carcinoma was diagnosed was 1.5 per cent , whereas in the non - cancer group it was 15 - 4 per cent , or ten times as great . these figures implied that castration might have protected a small number of women from the subsequent development of mammary carcinoma . arguing on these lines horsley , late in 1937 , performed bilateral oophorectomy on the first of a series of patients immediately after radical mastectomy , in the hope of deferring the onset of recurrence . 
by june , 1944 , recurrences had occurred in only 4 out of the 25 patients who had been observed for between 9 months and nearly 7 years . horsley felt that the appearance of metastases had been delayed by castration ( horsley , 1944 , 1945 )  . snapper castrated 22 patients after radical mastectomy , and in addition treated them for 3 months with injections of testosterone propionate 25 mg . 
of methyltestosterone was given on the day after oophorectomy , but in view of subsequent experience with this hormone , it is probable that the immediate effect was due to the oophorectomy alone . a case of intrathoracic recurrence in a woman of 40 years , 2 years after radical mastectomy for stage ii carcinoma , in whom relief of dyspnoea was observed 4 days after castration , and during the next 2 months absorption of nialignant pleural effusion and resolution of pulmonary parenchymal deposits took place , was reported by jochweds , baranowicz and horecki ( 1948 )  . the effects of surgical castration may be summarized by saying that it confers definite benefit on a small percentage of cases of carcinoma of the breast , even in an advanced stage , as shown by relief of severe bone pain , recalcification of areas of destroyed bone , regression of primary and secondary manifestations of disease , and conspicuous improvement in general health lasting uisually for several months only , but sometimes for several years . 
the most favourable cases are those in the premenopausal group in women , though striking improvement occasionally follows castration in older women , and in the small number of cases reported in males the best results are to be expected in elderly patients . in passing it should be noted that some of the remarkable spontaneous regressions which occur , and which may resemble in all respects those already described , are probably the result of " self - castration , " both ovaries being completely destroyed by metastases . 
ahlbom 1920 , and described his ( 1930 ) attempted a statistical analysis of his cases , but as 147 out of 163 cases received treatment to other sites as well as to the pelvis , and his series included very few instances of women in the most favourable age group , he failed very few clinical data are presented in to demonstrate any positive effects . ahlbom 's paper , and in spite of his obvious anxiety to attain statistical precision , it is perhaps surprising that he could quote no examples of undoubted success similar to those reported so often in cases subjected to surgical castration . 
clarkson and barker ( 1936 ) reported a case of mammary carcinoma in a woman of 41 with axillary node involvement , and deposits in a metacarpal , a tarsal phalanx , femur and ilium , in which recalcification of destroyed areas in the skeleton the patient was in followed ovarian irradiation and general body irradiation . good health 5 years later ; the ovarian irradiation was considered to be the main cause of the good result . dresser ( 1936 ) reported the results of ovarian irradiation in 59 cases with skeletal metastases , having selected this group for special observation because of the dramatic benefit conferred on two women with generalized skeletal and other deposits after they had received small doses ( 700 r ) of x - ravs directed to in both cases the periods ceased , general the pelvis for local relief of pain . regression of deposits occurred , with skeletal recalcification , and in the second case multiple pulmonary deposits disappeared ; the patient led an active life for of dresser 's 59 cases , 30 were under another 3 years , largely symptom - free . 45 years of age , and 29 had passed the menopause . 
the discrepancy between the results of the early surgical cases , in which castration was believed to be contra - indicated in the presence of bone metastasis , and the more recent results in which skeletal metastasis is regarded as one of the most favourable indications for ovarian irradiation , is probably adequately explained by the lack of satisfactory x - rays in the early work , so that the extent and incidence of bone metastasis was less accurately known . the effects of androgens in mammary carcinoma . among the first reports of the use of testosterone for mammary carcinoma were those of ulrich ( 1939a , b ) and of loeser ( 1941 )  . the latter used intramuscular injections and also subcutaneous implants of testosterone propionate . the first 3 cases were recurrence free at the time treatment was begun , but remained so for the next 3 to 4 years , whereas all had been treated by x - rays or surgery for recurrences shortly after the original operation ( 6 months , 8 months and 2 years respectively )  . farrow and woodard ( 1942 ) felt that there was a specially close relation between susceptibility to skeletal metastasis and ovarian activity , and were thus led to use testosterone for cases with bone deposits . 
doses gilven on alternate days . the case reports published by adair and herrmann ( 1946 ) illustrate very well the kind of result which may follow the use of testosterone therapy . weight gains , general improvement , rapid relief of pain previously intractable , regression of primary growths and secondary deposits , and increased calcification of bony deposits were recorded . the following are especially noteworthy : ( 1 ) the ages of the patients . - one of the best responses occurred in a woman of 63 years , though the other successes were in women of 47 , 44 and 42 years compare also taylor , slaughter , smejkal , fowler and preston ( 1948 ) , of age . who report andillustrate regression of pulmonary deposits in a woman of 70 , and the progress report of the american council on pharmacy and chemistry ( council on pharmacy and chemistry , 1949 ) , in which the response to androgens in 285 patients ranging from 25 - 79 years was evidently independent of age . in a later paper adair ( 1947 ) reports a dramatic result in a woman of 71 who had been confined to bed for 10 months with severe pain and pathological fractures due to widespread metastases in spine , pelvis and ribs . three weeks after commencing testosterone therapy she remarked on her improved sense of well being , and 4 weeks later left her bed . 
two years and 4 months after she was still up and about and in good health , the only untoward effect being irritation from the enlarged clitoris . this case recalls some of those treated by surgical castration ( thomson , 1902 )  . ( 2 ) the speed of response . - in case 4 relief of pain was evident within1 week of the first injection , and in case 3 regression in primary and metastatic growths was noted one month later . ( 3 ) the favourable effect on skeletal metastases . - the earlier results of adair ( 1947 ) suggested that the best results of androgen therapy were to be expected in cases with metastases in bone . however , equally dramatic results have been obtained in cases with pulmonary deposits and skin deposits , but no secondaries in bone of the common osteolytic type revealed by x - rays . these results are said to be much less common than in cases with bone deposits . thus adair stated : " in only a small percentage of cases is improvement to be anticipated where carcinoma involves soft tissues such as liver , lungs , brain and local skin recurrence . it is true that in a few instances there have been striking improvements where an advanced ulcerating breast cancer with surrounding skin nodules , axillary nodes and neck nodes were involved ; where masses were metastatic to the lungs ; and in one instance where the patient was having convulsions from metastatic disease in the brain receive no benefit  . 
in weight , her periods had not recurred , and the mass in the breast none of the nodes was more than 1 cacross , and the skin was no longer palpable . deposits had undergone complete regression , being visible only as brownish impalpable mottlings . 
48 signs of masculinization had appeared , namely slight hirsuties of chin , and lips , and a deepening of the voice . she complained of slight swelling of the feet her weight was 10 st . 
ii.49 she attended hospital complaining of severe backache , and on examination the nodes felt previously were found to be hard and much enlarged , numerous deposits not exceeding 3 min diameter were present in the skin of the left breast , and the liver edge , which was thickened , firm and somewhat irregular was felt in the right iliac fossa . 
47. - admitted to royal cancer hospital . on examination she was in good general condition , but bedridden with crippling pain . there were 3 ulcerated recurrences along the left mastectomy scar , the two larger measuring 2 x 4 and 5 x 3 crespectively , with irregular thickened raised edges , fixed bases and coarsely nodular floors . 
in 9 months , had recurrence of low back pain ; the mass in the upper inner quadrant of the right breast was larger , as were the axillary nodes ; the bony parasternal swelling in the left 4th interspace had ulcerated through the skin . there were numerous hemispherical bony projections on the vault of the skull , on the frontal bone , on the right clavicle . x - rays showed many fresh osteolytic deposits in spine , ribs and pelvis , side by side with old sclerosed deposits , which were less dense than before . injections of testosterone propionate 100 mg . 
viii.44. - left radical mastectomy for stage i carcinoma of breast . postremained well until april , 1948 , when first noticed breathlessness on effort , which june , 1948 . - signs of large left pleural effusion . 
49 the only abnormality found was slightly diminished radiologically there is now only obliteration of the left expansion at the left base . costophrenic sulcus , and the parenchymal opacities are no longer visible . she was last seen on 25 . 
48 the entire area was paler in colour , the young skin over it thicker , but there was still one small discharging area . this dried up during the next two months , dressings were discarded and therapy discontinued , but on 1 . 
bartholomew 's hospital , london , e.c.1. received for publication december 22 , 1948 . in an earlier publication ( robinson , 1948 ) the results obtained in a study of 17 - ketosteroid excretion in men of different age - groups were reported . special attention was paid to quantitative dlifferences in total ketosteroid excretion during the later decades of life . 
the method involves adsorption of the 17 - ketosteroids on a column of alumina from benzene solution followed by fractional elution with benzene of increasing ethanol content . the amount of 17 - ketosteroid present in each eluate is determined by the zimmerpreliminary experiments with the method described by these mann reaction . authors showed that separation and estimation of the steroid components could be achieved , but that reproducible results depended on careful standardization of the alumina and of the conditions of elution . 
of total 17 - ketosteroid was found to be the most suitable amount , and sufficient urine from a 24 or 48 - hour collection was hydrolysed and extracted to furnish a quantity in excess of 5 mg . 
was evaporated to dryness , and two successive portions of pure benzene ( 5 ml . ) added and distilled off to remove the last traces of alcohol prior to solution in benzene for adsorption on alumina . ( 2 ) stamndardization of alumina and adsorption columns . since merck 's alumina was not available , many samples of alumina were examined in order to obtain a product with the desired activity . spence " type h " alumina was finally selected for this purpose . 
when samples of this alumina are exposed to air ( by spreading the material in thin layers and exposing it to the moist air of the laboratory ) they gradually lose their adsorptive activity . this loss of activity is accompanied by a decrease in ph of aqueous suspensions of the alumina . suspensions prepared by mixing alumina with distilled water ( 1 part a1203 with 2 parts distilled water , by weight ) show an initial ph of 105 before deactivation and a gradual decrease to ph 9 - 3 after 2 to 3 days ' deactivation . the adsorptive power of the alumina was checked at intervals during the deactivating process by employing brockman 's method of standardization , using mixtures of dyes ( brockmann and schodder , 1941 )  . 
gurr , and further purified by solution in benzene and filtration through alumina followed by crystallization from benzene ( sudan red ) or alcohol ( sudan yellow )  . for standardization , 1 ml . of this dye solution is adsorbed on a column ( 50 x 14 mm . ) prepared from a suspension of alumina ( 7 g . ) in benzene - petroleum ether ( 1 : 4 ) and eluted with 30 ml . 
the alumina is considered to have suitable adsorptive power when the yellow band reaches the bottom of the column , while the red band moves down about 10 mm . the alumina columns for adsorption of the urine extracts are contained in glass tubes of 14 minternal diameter fitted with glass taps at the lower end . above the tap a plug of cotton - wool is inserted and the alnmina filling is added above the plug . 
fractions. these fractions are numbered successively 1 - 43 . ( 4 ) assay of eluted fractions . the solvent is removed from each fractional eluate and the residue dissolved in 2 ml . 
the observed colorimetric values are corrected when necessary for interfering chromogens ( robinson , 1948 )  . ( 5 ) recording of chronatograms and identification of con8tituents . the amount of 17 - ketosteroid in each eluate is plotted as the ordinate against an abscissa corresponding to the serial number of the eluate . 
with normal urine as many as nine peaks may occur , but in no case was the number less than seven . dingemanse , huis in ' t veld and de laat ( 1946 ) adopted a system of numbering in which successive peaks on the curve were indicated by roman numerals i - vi , the lowest numeral corresponding to the peak with the lowest eluate serial numbers . this system was used in the present work to facilitate comparison with the results of these authors . in some urines , however , small quantities of a component occurred which appeared to be different from any of the 8 main fractions , and this component was allocated to a sub - group hia . 
the substance originarlly referred to as " 17 - ketosteroid hi " ( dingemanse , huis in ' t veld and de laat , 1946 ; dingemanse , huis in ' t veld and hartogh - katz , 1948a ) was later shown to be i - androsten - 6 - ol - 17 - one ( dingemanse , huis in ' t veld and hartoghkatz , 1948b ; barton and klyne , 1948 )  . the dutch workers isolated this substance from the urine of a two - year - old girl with an adrenal tumour , but found only small quantities in the urine of normal persons . in the presence of hydrochloric acid this substance gives rise to chlorodehydroisoandrrone and dehydroisoandrosterone , and such a conversion may occur durijg the preliminary hydrolysis of the urine . in the present investigation confirmation of these identities for peaks mn , rv and v was obtained ( a ) by the isolation of the constituents of peaks rv and v and the preparation of crystalline acetates and benzoates therefrom , ( b ) by the urinary 17 - ketosteroids application of a colour reaction ( patterson , 1947 ) to the constituents of peak ni , ( c ) by identification of the peaks formed by authentic specimens of dehydroi&oandrosterone , androsterone and aetiocholan - 3 - ( x ) - ol - 17 - one . in order to study the reproducibility of the method and the type of curves to be expected , known amounts of dehydroisoandrosterone , androsterone and aetiocholan - 3 - ( x ) - ol - 17 - one were chromstographed alone and in mixtures containing varying proportions of these three steroids . 
the curves obtained in these experiments revealed immediately a problem that has to be faced in determining the amount of ketosteroid represented by any one peak . this is the complication introduced by the fact that the minimum values in the depressions between peaks are not always zero . 
the question therefore arises as to how the amount of ketosteroid corresponding to such minimum values should be partitioned between two peaks on either side of the minimuthree treatments were considered : ( i ) half of the minimum value might be allotted to each of the adjacent peaks ; ( ii ) the whole of the mimmum value might be added to the preceding peak ; ( iii ) the descending curve of the preceding peak might be projected down to the abscissa axis , and the additional values thus formed added to the preceding peak while corresponding deductions are made from the succeeding peak . these three methods were tested by their application to the model chromatograms obtained with the known mixtures of the three steroids menin general it was found that the projection method ( iii ) gave a tioned above . closer approximation to the actual amounts of the individual steroids than did either method ( i ) or method ( ii )  . this method was therefore adopted as standard for computing the amounts of 17 - ketosteroids represented by different peaks . a striking example of the reproducibility of the method has recently been encountered . 
1. the curve of case 0 was obtained on an extract from a 10 - day collection of urine from a boy aged three . in cases 1 and 2 it was necessary to collect urine for 2 to 3 days in order to obtain sufficient ketosteroid for analysis . 
the percentage distribution of the total ketosteroids among the different peaks is given in table i for all the normal males investigated with the exception of case 0 , in which the peaks normally present in adult curves could not be differentiated . urines from 2 cases of benign hyperplasia of the prostate and from 6 cases of carcinoma of this gland were also examined , and the corresponding curves and percentage compositions of these extracts are shown in fig . 
1. - 17 - ketosteroid content of eluates from chromatograms of urines from normal males case 0 ( not included in table i )  . three - year - old boy . incomplete differentiation into cases 1 , 8 , 17 represent the predominant type in which androsterone exceeds aetiocases 2 and 5 are unusual types in which aetiocholanolone exceeds androsterone . case 13 is a man , aged 50 ; 17 - ketosteroid output 20 mg . 
per day ; dehydroi / androcholanolone . sterone 34 per cent of total ketosteroid . .420 urinary 17 - ktogsrerrds case 20 case 19 ly~~~~~~~~~~~l case21 case22 case 23 case 24 case 25 case 26 eluate number fio . 
peak ii , average value 11 - 7 per cent , ranges from 2 to 34 per cent of the total , peak iv averages 30 per cent , with a range from 8 - 4 to 49 per cent , and peak v has a mean it will be seen that the of 24 - 2 per cent , with a range from 11 to 38 per cent . average output of androsterone exceeds that of actiocholanolone in the ratio only in three of the 18 cases shown in table i does the output of 1 - 25 : 1 - 0 . aetiocholanolone notably exceed that of androsterone ( cases 2 , 3 and 5 ) ; in the other 15 cases the amount of the former ketosteroid is either approximately equal to or less than the amount of androsterone . luriary 17 - ketosteroimds a comparison of the data shown in table ii with those of table i shows , however , what appears to be a significant change in pattern . in the urines from the cases of prostatic disease there is a consistent preponderance of peak v over peak iv . this is illustrated in fig . 
3. - relative excretions of dehydroisoandrosterone , androsterone and aetiocholanolone in normal males and in males with prostatic disease . cases 13 - 18 , normal . cases 19 - 20 , prostatic hyperplasia . cases 21 - 26 , prostatic carcinoma . amounts of dehydroisoandrosterone and aetiocholanolone are shown relative to the same amount ( 100ug . ) of androsterone in all cases . three major peaks are shown for extracts prepared from urines of six normal males over 50 years of age ( cases 13 - 18 ) , and from the urines of two subjects with prostatic hyperplasia ( cases 19 and 20 ) , and six patients with carcinoma of the prostate ( cases 21 - 26 )  . utrines from the carcinoma cases were obtained before oestrogen therapy was begun , and those from the benign hyperplasias before operation . 
for convenience of comparison , the amounts of peaks in and v are shown relative to the same amount ( 100lg . ) of peak rv ( androsterone ) in it will be seen that the most striking feature is the relative increase in all cases . peak v in the cases suffering from prostatic disease . in the normal males over 50 years of age the amount of this peak is equal to or less than the amount of androsterone , but in the 8 cases of prostatic disease it is present in considerable excess . as mentioned earlier , the preliminary experiments with known mixtures of 17 - ketosteroids showed that peak v normally indicates the presence of aetiocholanolone , and the total amount represented by this peak is a measure of the quantity of this steroid in the original mixture . it may be provisionally assumed , therefore , that the increased size of this peak in prostatic disease indicates a a . 
goulden relative increase in the output of aetiocholan - 3 - ( x ) - ol - 17 - one , although the possibility is not excluded that the incrased peak size is caused by the inclusion of a second substance ( of at present unknown nature ) which is eluted with the aetiocholanolone . 
a decision on this question can be made only when sufficient of the material present in this peak has been accumulated to allow of its identification , and experiments are in progress with this object in view . if it is assumed that aetiocholanolone is the substance that is increased in relative amount in prostatic disease , the cause of this increase is at the moment obscure . this ketosteroid has been recognized as a transformation product of more than one other steroid . callow ( 1939 ) isolated aetiocholanolone and androsterone in approximately equ%l amounts from the urine of normal men , and also much larger , but still approximately equal , amounts from the urine of a man treated with testosterone . these two isomers appear to be end - products of testosterone metabolism , and to be formed in about equal amounts from this hormone . 
an explanation of increased testosterone metabolism does.not appear to fit the present observations , however , since they show an increase in aetiocholanolone relative to androsterone . in this connection it may be remarked that callow 's finding of approximately equal amounts of these two ketosteroids in normal male urine was based on experiments with a pooled sample of urine , and an examination of table i shows that in individual urines the ratio between the amounts of androsterone and aetiocholanolone is not constant , although the average values are approximately equal . aetiocholan - 3 - ( c ) - ol - 17 - one has also been shown to be a metabolite of dehydrosoandrosterone . 
mason and kepler ( 1945 , 1947 ) found that administration of dehydroandsterone acetate by intramuscular injection in oil to patients with very low outputs of 17 - ketosteroids ( a man with anterior pituitary deficiency and a man and a woman with addison 's disease ) led to greatly increased excretion of both aetiocholanolone and androsterone . in the two male subjects the amount of androsterone excreted exceeded that of aetiocholanolone by approximately 75 per cent , while in the female patient the aetiocholanolone was about 4 - 5 times as much as the androsterone . the observed increase in the ratio of aetiocholanolone to androsterone in the cases of prostatic disease might be produced by an increase in the absolute amount of aetiocholanolone , or by a decrease in the absolute amount of androsterone excreted , or by both simultaneously . the amounts of 3 - ( , ) - hydroxyketosteroids , androsterone and aetiocholanolone excreted in 24 - hours were calculated for the cases illustrated in fig . 
3. normal males in the later decades have been examined . such a comparison will be possible when further in a study of z - ketosteroid excretion in patients with neoplastic disease dobriner , rhoads , lieberman , hill and fieser ( 1944 ) found abnormal patterns in in the one case of prostatic cancer reported in several cancerous conditions . their paper there was a great excess of aetiocholanolone as compared with androthey found a similar relation in a case of carcinoma of the larynx and sterone . a case of carcinoma of the breast . 
the presence of the agent in mammary tumour cells after 42 transplantations in c57 black low - cancer - strain mice cbaracterised by low susceptibility to mammary cancer and lack of the agent again raised the question what part is played by the mammary tumour inducing agent im the propagation of the transplanted breast tumour cells , and whether bho cells will continue to multiply in the same way should the agent disappear from the bittner , evans and green ( 1945 ) reported the presence of the agent after cells . 10 serial passages of high - cancer - strain tumour cells in ag - ent - free but susceptible mice , and concluded that the agent is continuously produced in the transplanted tumour cells . in an attempt to ascertain whether the presence of the agent is a permanent feature of the transplanted cells , the c57 x transplantable mammary tumour was again tested for the presence of the agent after 86 serial transplant 's in c57 black low - cancer - strain mice . 
the method of preparation of the tissue for testing and the test itself were the same as those employed for the 42nd transplant of the tumour in whicb the agent was found to be present . 
 ' they succeeded in the recovery of small amounts of papilloma v ' irus from the first and second transplant of carcinoma cells in now - bom rabbits , but failed to recover the virus from tumours of the third and fourth passage . 
the same authors reported positive neutralisation and complement - fixation test - s between papiroma vi ' lrug iand sera of adult rabbits in which a carcinoma originally derived from a v ' irus papilloma was transplanted for 22 the 46th and 50th tumour transsuccessive passages . plants failed to give a positi - ve compl - e ' ment - fixation test . 
they concluded that the " virus was - no longer present in the attempts tumour , although the morphology of - the tumour , remained unaltered . to reinfect the tumours by placing them in a v ' l ' r - us s - aspension or mjecting papiltransplants of the carcinoma loma virus int - ravenously into rabbits be - ar ' m ' yielded dubious results . serological tests m mice similar to those carried out in rabbits by smith , kidd ancl rous ( 1947 ) in order to ascertain the . 
presence of a lat - ent or masked mammary tumour induc ' mg agent in cells of the , 86th transplant could not be of any help in this respect . 
no atte - mpts were made to test the nells of the 86th transplant c57 xmanimar tumou ' r by grafting the tumour tisgue into susceptible mice in view of , the previous observations by various authors . 
thus transplantation of mammary tumour tissue with the agent into susceptible mice has either failed to transfer the agent ( andervont , 1949 ) , or has induced only a low incidence of tumours ( humniel and little , 1949 )  . it has also been found to be a poor source of the a ' gent ( barnum , ball and bittner , 1947 )  . it was therefore considered an unsatisfactory method for testing the transplantreinfection of the tumour able c57 x tumour for the presence of the agent . tissue wit - h the mammary tumour agent was not carried out because of the observations of smith , kidd and rous ( 1947 ) , although it is quite posgible that it would in connection with the negative result obtained have yielded unequivocal results . with the 86th transplant , another test for the presence of the agent in cells of the so far no tumours have been observed 101st tumour transplant was carried out . in an of the test mice , but it is too early to draw a conclusion , as all the mice bittner ( 1952 , personal comare still alive , havi ' n ' g lived now for 11 months . munication ) has found the agent present in the 15th transplant of a c3h mammary tumour in agent - free cm mice , while in t - he cells , of the 7th transplant , of the same tumour it was apparently difficult to detect . it is not known whether a similar situation may arise with the c57 x transplant ' able mammary tumour , although the agent could not be detected in the 86th s ' en ' al passage by the same means which revealed its presence in the 42nd transplant . 
the agent or bittner virus , as it is described by some authors , may have been altered in some unknown way , possibly by mutation . it may have become closely associated with one of the particulate this close integration of the agent with the tumour elements of the tumour cells . cers may have produced a state in which it was unable to survive the death of the tumour cells during extraction procedures preparatory to the test . 
kreyberg. from the institutt for generell og eksperimentell patologi , universitetet i oslo . received for publication april 24 , 1952 . the importance of using pure , inbred strains in cancer research is now generally accepted . strong ( 1942 ) , emphasizing this point , gave a survey of the origin of some of the best known strains , originating from his laboratory . 
the new informal document , mouse news letter , acts as a most valuable source of information as to a great many strains used all over the world . the characteristics of the different strains as to susceptibility to development of spontaneous tumours , reaction to carcingenic agents , as well as susceptibility to transplantation and other biological responses may be very marked and very different . it is therefore of great importance to have a great number of different strains with marked characteristics , in order to supply research workers with the best material possible for their special needs . the purpose of the present paper is to describe the origin , development and some of the features of our strain " white label "  . the first animals were obtained from a commercial dealer in oslo , a young man who used to supply a number of laboratories with albino mice , and who , from time to time , added animals of different origin to his stock . 
the figure shows , however , very clearly how two lines were developing with extreme differences as to the formation of spontaneous mammary carcinomas . " line 27 " produced a high , and an increasingly higher percentage of mammary tumours . 
from f2 and up to and including f14 , when this line became extinct , mammary tumours occurred in every generation , and from fg until f14 16 out of 18 females developed such tumours . from the sister of no . 
2 indicated by an arrow . in the 11 generations ( f5 - f15 ) in which there were 102 females , not a single instance of mammary carcinoma was observed . such was the situation in 1935 . in the following years the brother - to - sister matings were continued and many sidelines died out , or were not continued , but " line 426 " was kept until the war interrupted the experiment at f37 . in table i is given a complete record of the females of all the generations descending from pair ( 2 + 3 ) up to f37 . in the first column is indicated the generation . 
in the second column is given the total number of females in each generation . in the third column is given the number of females belonging to " line 426 " ; from f15 all the females belong to this line , as this is the only line surviving . in the fourth column is given the total number of mammary carcinomas occurring in each generation . finally the 24 columns show the number of animals dying in each month after birth , as well as the occurrence of mammary carcinomas , the figures in brackets . at the bottom of the table the sum total is recorded , as well as the reversed figures , indicating the number of females alive at the end of each month . table i gives a clear picture of the great number of mammary tumours occurring in the first heterozygous generations . 
from f12 it is only " line 27 " which still contributes to the presentation of mammary tumours , and from f14 when this line becomes extinct , only one single mammary tumour occurs ( that is in " line 426 " )  . 
an exception , indicated by a cross , will be mentioned later . this means that " line 426 " , during 34 generations , comprising 1595 females , presents one single case of mammary carcinoma . 
bonser , university of leeds , wrote me in august , 1949 , regarding this question as follows : " i still keep ' white label ' mice in this laboratory . 
by suckling ' white label ' babies on riii mothers i showed that they were susceptible to the riii milk factor , which i regard as a potent factor . never published these experiments , and they were only done on small numbers of mice , but they point strongly to the fact that ' white label ' mice in leeds have the milk factor , and are susceptible to it . " bonser wrote me a further letter in february , 1951 , stating that " mammary cancers still occur in our line and we regard the incidence as being about 30 per cent in mice which live to be 12 months of age or more , but i have not any recent accurate estimate of the mammary cancer incidence , because we have been very short of accommodation lately . addition : " now , in 1952 , we find that 7 of 33 females over 10 months of age have developed mammary cancer , usually rather late in life . but we make no attempt to assess the mammary cancer incidence accurately as we usually dispose of breeding females when they reach the age of one year . " i also had the following information , dated january , 1951 , from w . 
s. bullough : " my experienoe with these mice falls into two periods . first when i was working in the zoology department in leeds and when i obtained the mice from bonser . then mammary carcinoma was common in females of from 11 months of age onwards . i have no figures now , but my recollection is that it developed in not less than 40 per cent of the older females . also there was the odd occurrence in a male , though this was of course rare . " further : " this colony was allowed to die out in 1944 , but in 1946 i obtained two females and a male from bonser and started a new colony in the university of sheffield . since then a colony of some 200 - 300 mice has been maintained . . 
kreyberg further , in 1952 : " the final chapter in the story starts in 1949 when , in the autumn , i took the milk factor out by fostering one family with a strong 's cba female . 
my present colony is entirely derived from this one family , and now mammary cancer is exceedingly rare . so my present stock of your mice indeed i cannot remember when i last had a case . is without the milk factor , and i suppose it is no use for your own present purposes . " i regret very much that i cannot definitely state so , but i have strong reasons to believe that the animals sent to leeds in may , 1934 , were descendants from the pair ( 4 + 5 ) ofmy " white label "  . 
at present one " white label " strain ( leeds ) carries the milk factor and produces about 30 per cent of mammary carcinomas in females reaching the age of 12 months or more . this strain has the characteristics of the branch ( 4 + 5 ) of the original material . 
another " white label " strain ( oslo ) is devoid of the milk factor and produces practically no mammary carcinomas spontaneously . this strain is probably one of the lowest mammary for future references it is therefore of great imcancer strains in existence . therefore portance to distinguish between these two " white label " strains ; the leeds strain will be designated wll and the oslo strain wlo . 
the two strains most probably have only a heterozygous founding mother in common . this experiment has been carried out for more than twenty years . it would not have been possible without the assistance of my collaborator miss hj . 
aasland , who continued the experiment during the first years of the war , until illness and an untimely death ended her devoted and loyal partnership . during the remaining years of the war the strain was maintained at a reduced scale through the initiative and faithful service of e . 
koller. from the chester beatty research institute , the royal cancer hospital , london . given at the symposium on the genetics of cancer , london , june 24 and 25 , 1948 . xeroderma pigmentosum ( hence referred to as x.p. ) , is marked by rougheniing , dryness , pigmentation and ulceration of the skthe condition is attributed to hypersensitivity of the skin , particularly that of the basal cell layer , to sunlight . the disease was first described adequately by kaposi in 1874 ( hebra and kaposi , 1874 )  . 
occurs in the first year of life , often within a few , months after birth . first , erythema develops on the skin , on those regions which are exposed to light , followed by freckling and frequently by telangiectasis . from these regions epithelioma or basal - cell carcinoma develops . 
the malignant change may take place not only in the skin , but also in the cornea and conjunctiva the genetical and chromosomal basis of x.p. the hereditary basis of x.p. 
was first investigated by siemens and kohn ( 1925 )  . they analysed 76 families , and cockayne ( 1933 ) brought this more up - to - date with a further 43 family histories . in both groups of data the incidence of consanguineous marriages was very high : 24 out of 76 and 16 out of 43 respectively , were first - cousin marriages . 
is one of those which is borne in that particular region of the sex chromosome , common to x and y . it may not be superfluous to describe the cytological mechanism which underlies incomplete sex - linkage . the genetical basis of incomplete sex - linkage is clear , and is already described 150 p . 
they found thait during the first meiotic d ' ivi ' lsion of the male rat , one or two chiasmata are forined between the x and y chromosomes , and that the shape of the sex bivalent is determined by the position of chiasmata in relation to the centromere and differential segment . 
the structure of the bivalent is determined by the position of the chiasmata ; the frequencies of the various bivalents are shown by the number of percentages beside the figures . similar chromosome behaviour wak ; observed in man . 
the fact that the heteromorphic pair present in the chromosome set of the human male , forms a very easily observable unequal or asymmetrical bivalent during meiosis , is - well known from the - works of painter ( 1923 ) , evans and swezy ( 1929 )  . 
when a ' man inherits such incompletely sex - linked gene from his mother , it will be in his x chromosome , but occasionally it may cross - o ' ver to the y consequently the man will transmit the gene to most of his daughters and to a similarly , if he inherits it from his . 
father , he , will transmit it few of his sons . to most of his sons and to a few of his daughters . human genetics is greatly indebted to j . 
he analysed 82 family histories collected from various sources , and by using ingemoug statistical methods drew the conclusion thatthe incomplete sex - linkage of the g ' ene x.p. 
he made the suggestion tha ' t one of the 82 families on which analysis was based should be excluded on intemal evidence , which would further loosen linkage , and in this case the true position of x.p. 
the data obtained from these cases has given further information on the hereditary basis of this morbid condition , and has shown the 'significance of the pathological symptoms , including the degree of manifestation and the time of onset of the disease . 
of one year the whole skin of the left 'side of her face came up in red blisters after being exposed to the sun . she was treated with calomel lotion . 
the condition it was treated by " caustic pencl ' l , " and six months later , was diagnosed as x.p. in 1943 another lesion developed on the right when it recurred , by radium . cheek , which was similarly treated by radiuthe patient 's skin of the exposed both the pathological skin conparts ( face , hands , legs ) shows some scarring . ditions and the histological analysis of the lesions indicated x.p. 
the parents are unrelated ; father is of a dark complexion , mother has some slight freckling search through family histories on the cheek , which is of the common type . of near relatives and sibs did not reveal any similar conditions . 
at that time some of the freckles developed into small ulcers , which healed slowly . she found out , by experience , that strong sunlight accentuates the lesions , and since the age of 40 she has taken care not to expose herself to direct sunli.ght. 
the matemal and patemal grandfathers were brothers.. the eldest brother , frank , hischildren and grandchildren are all normal . isabel , the patient concemed , was the second child , but before her birth one ' miscarriage took place . 
her sister , dorothy , is one year younger ; she is afflicted with the dorothy shows freckling on the face disease in the same mild manner as isabel . and forearm , which is somewhat less severe than that of - her elder sister '  . a younger brother , thomas , was born after isabel . 
the high number of miscarriages and the death of the sixth child , a girl , on the day following birth , may , not unlikely , find its sidney died at the age of 25 explanation in the consanguineous marr ' lage . up to his death he appeared to be normal . there are two unusual features in the history of the hfamily which require explanation . 
in the hfamily does not conform closely to expectations ; the number of cross - overs is higher than could be expected . in order to explain the exceptional pathological features and the unexpected segregation of x.p. 
in the sexe - s in this particular family , the followina possibilities may be considered : ( a ) this condition - may be due to an independent autosomal gene , or ( b ) the gene x.p. 
the increased distance of the gene from the differential segment would loosen linkage with sex , and its altered position may also lead to a lower degree of malignancy . the data at our disposal from this one family , however , is too meagre to draw definite conclusions , whether we are dealing here with a distinct autosomal gene or with position effect . 
bather. from the poultry research centre , edinburgh , 9 . received for publication november 18 , 1953 . considerable interest has been centred lately on the use of ascites tumours in rats and mice for biological research . 
such tumours include , in mice , the ebrlich and krebs - 2 carcinomata ( loewenthal and jahn , 1932 ; klein and klein , 1951 ) and s - 37 and malignant lymphoma ( goldie and felix , 1951 ) and , in rats , the yoshida sarcoma , the mtk sarcomata i and 11 ( tanaka and kan ' o , 1951 ) and the hirosaki sarcoma ( makino and kano ' , 1953 )  . 
the growth of these tumours is characterized by the formation of large numbers of discrete tumour cers , living in a compatible medium ( peritoneal fluid ) which lend themselves admirably to various biochemical studies . during the course ofinvestigations into the nature of the virus of rous sarcoma , an ascitic variant of the tumour was estabhshed early in 1953 in order to see if infective virus could be obtained in a more pure forthe fact that rous no . 
of the suspension was no evidence of necrosis . inoculated into the abdominal cavity of each of 2 6 - week old chickens from a known rous susceptible strain maintained at this centre . 
most of the negative results can be attributed to failure of the inoculum to enter the abdomen and , usually , subcutaneous tumours grew at the site of entry of the needle . the rapid growth of the rous tissue and its invasion of the intemal organs has been observed in all subsequent passages . 
smar nodules of tumour tissue attach themselves to the surface of the organs and then proceed to infiltrate the membrane and musculature , often penetrating to the interior of the organ itsell of 30 birds from the ist to the 12th passages autopsied 9 - 19 days after the inoculation of the tumour , the following tissues showed invasion microscopically and grossly : gizzard ( 30 ) , pancreas ( 27 ) , duodenum ( 27 ) , spleen ( 25 ) , ovary ( 17 out of 20 ) , testis ( 5 out of 10 ) , liver ( 12 ) , heart ( 10 ) , adrenal ( 10 ) , kidney ( 7 ) , and lungs in the cases of the ovary and pancreas , invasion has frequently pr ' ogressed ( 1 )  . to such an extent that only a few fragments of normal tissue remain , almost the whole organ having been replaced by tumour tissue . 
pale yellow , viscous fluid present in a 6 - week - old bird after 10 - 1 2 days ' incubation , and , on occasion , as much as 60 ml . 
the cells account for approximately 10 per cent of the fluid volume . counts of the cells made from stained smears ( giemsa ) at variou 's times during the passaging of the tumour show that of over 2000 cells counted approximately 50 per cent are round tumour cehs , and the remainder leukocytes , lymphocytes and connective tissue cehs . this proportion has remained unchanged throughout the 18 passages so far maintained . 
on various occasions , virus or whole cells from ascitic fluid have been inoculated into the muscles of birds and , again , there is an immediate return to the normal histological picture of a solid rous no . 
1 shows the typical appearance of the fluid using iron haematoxylin stathe cytoplasmic and nuclear changes in rous sarcoma cells cultivated in vitro have been described ( tenenbaum and doljanski , 1941 ; doljanski and tenenbaum , 1943 ) and many of the descriptions apply to the appearance of the cells grown intraperitoneahy . 
the blue staining granule and thread network in the peripheral cytoplasm ( giemsa stain ) and the dense central zone can be seen , as well as the large cytoplasmic vacuoles and clubshaped pseudopodia . 
bather scattered at random and sometimes arranged round the periphery of the nucleus . the gathering of this granular material into the centre of the nucleus , leaving a clear zone between it and the nuclear membrane as described by tenenbaum and doljanski ( 1941 ) , is only rarely seen in these preparations . large round or rod - shaped , densely staining nucleoh are common and irregularly shaped ones are frequently found . multinucleate cells are present and many contain fragmented nuclei with as many as 15 - 20 fragments . measurement of the frequency of multinucleate cells is given in a later section . ascitic fluid examined microscopically by dark field illumination on the warm stage provides an excellent opportunity to observe the living cells for long periods of time . 
the lace - edge appearance of the .cells is typical of fresh preparations and the cell membrane tends to become more regular after a few hours . in the peripheral area of the cytoplasm , and in the pseudopodia , a very fine " mist " of minute particles can sometimes be seen , although this does not occur in every cell . 
the club - shaped pseudopodia described by doljanski and te ' nenbaum ( 1943 ) are a common feature and sometimes become detached , forming free spherical " bubbles " of protoplasm , usuary shimmering with the rapid brownian movement of very fine particles . similar vesicles are seen , especially in the clumps of aggregated cells in which either particles or an interwoven mass of fine filaments appears . 
they have been show - n to be present not only in pathological blood conditions , b ' ut also in normal blood after it has been kept for several hours under sterile conditions . in the rous ascitic tumour and in erythroleukaemic blood ( campbell , 1952 ) filamentous structures are present i fresh preparations and may be associated with the high rate of c ' ell degeneration . the possibility that they may represent a method of virus release from infected cells must be borne in mind . similar structures have been observed associated with cells infected with influenza virus by hoyle ( 1950 ) and wyckoff ( 1951 )  . a peculiar filamentous structure encountered , only occasionauy , is represented by the spear - shaped process shown in fig . 
the outer part of the thread becomes an external , free floating filament and the inner part withdraws to the cell , forming a small protrusion on the cell membrane . 
this type of structure usually occurs in cells having a poorly defined nucleas under conditions of dark - ground inumination . the fluid surrounding the cers also contains numerous tiny rapidly moving particles which scatter light . multinucleate cells show up very well and , occaascitic rous no . 
the samples were taken between the 10th and only cers containing morphologically 14th days after inoculation of the tumour . such cells arise because normal nuclei are included in the multinucleate forms . of failure of cell cleavage after nuclear division . 
the incidences of karyorrhexis and mitosis after 10 - 1 4 days ' tumour growth have not altered to any significant extent . number of nuclei per cell . karyorrhexis mitosis infective viru8 in ascite8 and 8olid rou8 8arcomata . the amounts of infective virus contained in either the cytoplasm of the washed cells or in the cell - free fluid have been determined by means of the day - old chick titration method first described by carr and harris ( 1951 )  . 
bather table ii shows the results for the first i 0 passages , along with two sets of figures obtained for solid rous sarcoma tissue and cell - free exudate . 
the virus titres of fluid and cell contents follow each other fairly closely . in 4 of the 7 pairs of results , however , the intracellular virus shows a higher titre by one logio dose . in this respect the ascitic tumour behaves in the same way as the sohd sarcoma and its exudate . edimation of total 4cpurified " viru8 material in cell8 and cell - free fluid of the rou8 in view of the differences encountered in the infectivity titres of the fluid and cehs , estimates have been made of the amounts of virus material obtainable from both sources . 
the " purified " virus was isolated by the fractional centrifugation method of carr and harris ( 1951 )  . ascites fluid was first treated with hyaluronidase to reduce the viscosity . 
the cells were then centrifuged off , washed in 0 - 85 per cent saline , lysed in distilled water and the cell debris discarded . both the cell extract and the fluid were then deposited in the servall s.s. 
the resulting pellets were treated with trypsin in m / 5 phosphate solution , clarified and deposited agathe amounts of virus material obtained in this way were estimated by the biuret method described in a previous pubhcation ( bather , 1953 )  . virus content is expressed as ml . 
dry weight per unit of tissue or fluid . during the washing of the cers , a cell count was done in a haemacytometer . table iii summarizes the results and includes an estimate of the virus per cell in solid rous sarcoma tissue . 
the figure is based on the average virus yields , as reported elsewhere ( bather , 1953 ) and an approximate cer count using the method of afizen and petermann ( 1952 )  . this method utifizes controlled homogenization in sucrose and acetic acid solutions containhag calcium chloride , ( 0 - 0023 m cac12 is used here )  . after suitable dilution , a count can be made of the whole cells and nuclei in a haemacytometer . 
an average figure for rous sarcoma , based on five different tumours was found to be 32 - 2 x 107 cells per g . with a standard deviation of + 2 - 8 . 
bather peritoneal fluid containing suspended round cehs . it seems probable that this type of conversion does not depend on the selection of round cells since when the tumour invades the abdominal organs , the secondary growth reverts to the normal spindle - cell form immediately . moreover , virus or whole fluids , from the ascites tumour , when inoculated intramuscularly , produces a typical solid rous doljanski and tenenbaum ( 1941 ) have described the reversible transsarcoma . formation of the one type olf rous cell to the other in tissue culture . 
thus the rous sarcoma , in chickens , closely resembles s37 sarcoma and t2146 tumour in mice , both of which have been shown to form ascites tumours by reversible adaptation ( lasnitzki , 1953 )  . results from the first ten passages of the ascites tumour indicate that the cell - free ascitic fluid contains infective virus to an extent , roughly , of that contained in a 10 per cent extract of the cehs . similar observations have been made on the liquid exudate from sohd rous sarcomata . there are various ways in the first place , of course , in which the virus may be released from the cells . virus might be released upon necrosis and disintegration of the cell . secondly , there is the possibihty that the filaments , which are abundant even in fresh preparations of rous ascites fluid , may represent a method of eiectinlr virus particles . 
of the sohd tumour growing in birds of the same age . in terms of dry weight of virus material , this infective titre was given by 0 - 30 m.g " purified " virus for the ascites tumour and 0 - 46 mg . 
the ascites produced is made up of cells ( 10 per cent ) and a pale yellow viscous fluid ( 90 per cent ) both of which contain infective virus . 
the cells are mostly dispersed singly but some are aggregated into small clumps . approximately 50 per cent of them are round tumour cells , the remainder lymphocytes , leucocytes and connective tissue cehs . 
after 10 - 14 days ' growth , 10 - 5 per cent of the tumour cells are multinucleate ( with 2 - 4 nuclei ) 1 - 8 per cent contain pyknotic , fragmentary nuclei ( karyorrhexis ) and 1 - 1 per cent are undergoing mitosis . 
no improvement in the yields of infective virus , as detectable by the day - old chick titration method , has been obtained from either washed cehs or cell - free fluid of the rous ascites tumour when compared with the sohd rous no . 
86 x 10 9 mg fluid exhibits the same , or more often , all expenses in connection with this work were borne by the british empire cancer campaign . i should fike to thank j . 
they reported an increase of urinary cholesterol in 19 out of 92 cancer patients . later , bruger and ehrlich ( 1943 ) , using a similar method of estimation , found a higher incidence of hypercholeshowever , the teroluria , 11 of their 32 cases giving results above normal limits . actual concentration of cholesterol reported by bruger and ehrlich in normal urine was approximately twice as great as that found by sobotka , bloch and rosenbloom . it appeared , therefore , that the methods used in these two studies must have been significantly different , and we felt that further work on the technique of estimation was needed . while admitting the possible non - specificity of the liebermann - burchard reaction , we felt that this type of method was the only one likely to find immediate clinical application , and it does appear to have given results consistent with the original work of bloch and sobotka . 
an attempt was made to correct for this error by the introduction of a blank reading , which was obtained by adding to half the urinary extract in 5 ml . 
the general procedure was to filter the urine slowly through a 3 - inch wide column of adsorbent from 1 to 3 inches in length , and after washing the column with water , to elute with 40 ml . 
maclagan treated with the liebermann - burchard reagent as described below under aluminthe final chloroform solution was invariably colourless , ium tungstate method . and gave negligible blank values when treated with 09 ml . 
the large tarry residue after alcohol - ether extraction was difficult to extract with petroleum ether and recovery of added cholesterol was poor , ranging from 30 to 70 per cent in various experiments . in this method a gross excess of sulphuric acid is used which is difficult to wash out of the precipitate and results in charring . 
for 20 minutes , and the green colour compared in the photoelectric absorptiometer ( king - gallenkamp ) with the ilford spectrum red filter ( maximum transmission 660mi . ) a preliminary calibration curve showed that beer 's law was well obeyed up to optical densities of 0 - 5 . 
proteose. the results given above under adsorption methods indicate a definite association between urinary cholesterol and protein when present , and suggest a possible association between cholesterol and proteose in normal urine . further evidence of the latter association was sought by estimating the nitrogen content of the aluminium tungstate precipitate obtained ( a ) after washing the precipitate with water as above , and ( b ) after dialysis of the original urine before precipitation . it was assumed that any nitrogen remaining in the precipitate after these procedures was attributable to urinary proteose . ( a ) washing of aluminium tungstate precipitate . - the relationship between cholesterol and proteose was investigated by serial washing of the aluminium in this experiment four identical samples of 100 ml . 
some support for this assumption was obtained by treating the washed precipitate with biuret reagent ( hiller , 1927 ) and also with the phenol reagent of folin and ciocalteu ( 1927 ) as follows : the precipitate from 5 ml . 
of normal urine with added cholesterol ( 0 - 5 mg . ) were duplicate dialysed in a collodion sac against running tap - water for 16 hours . samples were similarly dialysed for 40 and 64 hours . 
of the dialysed urine were precipitated with aluminium tungstate , and the nitrogen content of the precipitate determined by the kjeldahl method as above , without further washing . from the result of this experiment , as shown in table x , it can be seen that the m . 
the precipitated protein was removed by centrifugation , washed once with 0 - 5 per cent acetic acid and extracted three times with boiling acetone , the acetone extract evaporated to dryness and the residue extracted with petroleum ether for cholesterol determination as above . 
the experiments reported give some support to the hypothesis that the urinary cholesterol is normally associated with a urinary proteose fraction , and also with heat - coagulable protein if present . removal of heat coagulable protein does not , however , carry down the whole of the native cholesterol . urine is not a homogeneous substance , and the varying distribution of cholesterol between the deposit and supernatant urine which we have demonstrated is obviously relevant to clinical studies . this factor has been recognized previously , e.g. 
bruger in 1935 reported up to 40 per cent of the cholesterol in the urinary deposit in cases of nephritis . however , most authors have not recognized its importance , and have included the deposit even though pathological in certain cases ( sobotka , bloch and rosenbloom , 1940 ; bruger and ehrlich , 1943 )  . 
much or all of the urinary cholesterol may at times be found in the urinary deposit , or associated with heat - coagulable protein when present . this work was aided by a grant from the british empire cancer campaign to westminster hospital . 
pyrene per animal and the same procedure followed . 1 : 2 : 5 : 6 - dibenzanthracene . for the determination of lipid and nucleic acid phosphorus the animal was weighed and then killed by dislocation of the neck . the liver was removed immediately , weighed , and a sample of about 500 mg . 
from each of two lobes was analysed for lipid , " pentosenucleic acid " ( p.n.a.p. ) and " desoxypentosenucleic acid " ( d.n.a.p. ) phosphorus by a modification of the method of schmidt and thannhauser ( 1945 )  . in this modification the whole of the separation is carried out in a single centrifuge tube and transfer of material is thereby avoided . the tubes have a ground neck to which may be fitted a condenser for refiuxing the solvent in the lipid extraction stage . the dry weight of the liver was determined by drying a weighed sample of the organ in an air oven at 110 c . 
has occurred , and the decrease is due solely to an increase in the concentration of d.n.a.p. there was no significant difference in the liver weight : body weight ratio between the groups of animals on 5 per cent and 20 per cent protein diets . influence of 1 : 2 : 5 : 6 - dibenzanthracene . administration diet on either l : 2 : 5 : 6 - dibenzanthracene produced a marked increase in the p.n.a.p. 
1 , which shows the growth curves of six animals , three of which were killed before any very marked growth inhibitory effect of the carcinogen was observed , and three after considerable loss in weight had the p.n.a.p. 
concentration , and a decrease in p.n.a.p. concentration was also found in the low protein group . administration of the non - carcinogenic hydrocarbon pyrene to rats maintained on the 5 per cent protein diet produced no significant change in the nucleic acid balance . the increase which was found in the liver weight : body weight ratio in the carcinogen - treated rats did not appear to be a result of any increase in the water or neutral fat content of the livers . kennaway , kennaway and warren ( 1944 ) have observed a similarly - increased ratio in mice treated with carcinogenic hydrocarbons . non - carcinogenic substances gave only irregular results . 
no explanation of this increase in liver weight was advanced . the possibility that the increase is related to a differential inhibitory action of the carcinogen on the growth of the animal body as a whole compared with the growth of the liver is being investigated . in considering the possible relationship of the decrease in the d.n.a.p ; concentration in the livers of the carcinogen - treated rats to growth inhibition and carcinogenesis , it is of interest that gopal - ayengar ( 1947 ) has shown that in epidermal carcinogenesis , induced experimentally in mice by application of 20 - methylcholanthrene , the initial effect of the compound was to produce a decrease in the desoxyribosenucleic content of chromosome threads isolated from the epidermal cells . the low desoxyribosenucleic acid content persisted during.the precancerous ( hyperplastic ) stage and was then followed by an increase when malignancy ensued . stowell ( 1945 ) found that x - irradiation of transplanted mouse mammary carcinoma brought about an initial decrease in cellular desoxyribosenucleic acid content , and mitchell ( 1942 ) found a small increase in cytoplasmic pentose nucleotides in biopsied specimens of x - irradiated human tumours . 
w.3. received for publication march 1 , 1952 . some of the effects of ionising radiations are associated with formation of such effects are often reduced free hydroxyl radicals and possibly of peroxides . for these under anaerobic conditions and increased in the presence of oxygen . reasons it appeared possible that conditions which would increase the concentration of hydrogen peroxide in tissues might augment the biological effects of of the possible ways of increasing radiosensitivity by such a radiation . mechanism , two have been investigated . the first depends upon increasing the concentration of substrates , the metabolism of which is known to produce hydrogen peroxide . such substrates are those oxidised by flavine enzymes , including aldehydes , xanthine , hypoxanthine this method is being investigated by administration of and d - amino acids . suitable substrates and riboflavin , the latter in attempts to increase the concentration of flavin enzymes of the tumours . a second method of increasing hydrogen peroxide concentration of tissues depends upon the inhibition of the enzymes involved in hydrogen peroxide thus by inhibition of catalase and peroxidase of tissues this destrucdestruction . tion and utilisation of hydrogen peroxide might be prevented and its concentration in cells should increase . this was attempted without success in the present paper . many of the known catalase inhibitors including sodium azide and cyanide are also respiratory poisons . 
x 77 , 500 so , where ko = the reaction constant at zero time expressed in logarithms to base 10 and so = the h202 concentration at zero time . 
kat.f. qo21 - 29 x 10 - ' mxh20 activity of a tissue to the other metabolic processes expressed in q values . the tables of this catalase activity is expressed as qo21 29 x lothis expression makes it easier to relate the catalase the catalase activity is determined at 0 c . 
the testis probably oxidised primary carbohydrate . recent work has shown that ionising radiations ( taylor , greenstein and radiomimetic hollaender , smith , 1950 ) induce depolymerization of deoxyribonucleic acid . 
some of the biological effects of radiation may be due to such an action occurring in in the case of ionising radiations the effect is probably due to fr~e the cell . hydroxyl radicals which are produced in irradiated water . if increase in hydrogen peroxide concentration should increase sensitivity to x - rays , then addition of hydrogen peroxide to a solution of deoxyribonucleic acid should augment the depolymerising action of x - rays . such an effect has indeed been found by conway and butler ( 1952 )  . a large number of substances have been reported as catalase poisons , and some of these are listed in table i in order of potency . in the present work the activity of catalase poisons is compared with their toxicity to mice and an attempt made to measure the inhibition in vivo . 
the toxicities are also listed for some of the compounds , and the ratio of the concentrations causing inhibition of the enzyme to the toxicity expressed as the ld 50 ( calculated on a molar basis ) is given in table i . 
gallico the poisoning of catalase in vivo is difficult to estimate owing to the reversibility of the poisoning . blaschko ( 1935a ) showed that of a number of catalase poisons only potassium chlorate produced irreversible inhibition . 
the pretreatment with the catalase poisons tried did not modify the effect of radiation on the tumour . reduction of sensitivity of mice treated with sodium azide and hydroxylamine to x - radiation . groups of each stock of 10 mice were exposed to 700 r irradiation from an x - ray tube operated at 220 kvp . 
the result with azide is similar to that obtained by bacq ( 1951 ) , but the result with hydroxylamine appears to be a new finding in general agreement with bacq 's work . a4 [ 2 ' ' ' " 45 1 : contro . 2 : - inece wit 1.5per kg ; nan3 15m.bfoeradato. 
gallico the search for a poison more specific for catalase than is azide was also unsuccessful . sodium azide and hydroxylamine are much the most specific catalase poisons of the compounds examined . p - hydroxyphenylazide had only 1 / 50 of the activity of sodium azide ( calculated on a molar basis )  . this difference is exactiy the same as that found between hydroxylamine and phenylhydroxylamine . on the other hand , phenylhydrazine appears to be a more potent inhibitor than hydrazine ( blaschko , 1935a )  . 
the introduction of a methyl group into the hydroxylamine molecule ( o - methyl - hydroxylamine ) reduced the activity 400 fold . the inhibition produced by diethyl - p - phenylenediamine was of the same order as that described for dimethyl - p - phenylenediamine by homer and betzel ( 1950 )  . the figures on the ratio of catalase inhibiting concentration to lethal dose show that sodium azide is the most favourable catalase poison as well as the most active . 
the median lethal dose of sodium azide should give , a concentration of azide which is one thousand times that causing 50 per cent inhibition of catalase . thus , sodium azide is probably the safest catalase poison for use in vivo in spite of its high toxicity . the increase in poisoning activity of azide with decrease in the ph is similar to that found for the effect of formate and acetate by agner and theorell ( 1946 ) , who showed that anions in general combine with catalase and inactivate it to an extent increasing with decrease in ph . these authors explained this as due to the anion displacing the hydroxyl group of the catalase and it is possible that azide acts in the same way . 
the data of agner and theorell ( 1946 ) on poisoning of catalase with formate at different ph values are analogous to those found for azide ( table iv ) as shown in table xi . 
the replacement of a hydrogen of formic acid by ch3 as in acetic acid reduces the activity 800 fold ( agner and theorell , 1946 ) , which is the same order as that produced by the introduction of an o - methyl group in hydroxylamine . thus the poisons may combine readily with catalase , possibly replacing a hydroxyl group or hydrogen peroxide because of their shape and size . in testing this hypothesis , methylamine was found to be a poison ( of the same order as hydrazine ) , but ethyl formate and formamide , which it was hoped would be as effective as undissociated formic acid , were both found to be inactive . while the poisoning with hydrazoic acid and formic acid may depend upon the entire undissociated molecule , the poisoning with hydroxylamine and hlydrazine appeared to be independent of the ph . 
now in the cases of hydrazoic acid and formic acid , ionisation would result in loss of a hydrogen atom ( and gain of a charge ) , so that the ion would have less structural resemblance to hydrogen peroxide . 
gallico ( 3 ) poisoning of catalase of liver and tumour of rats was demonstrated after injection of azide . ( 4 ) injection of small doses of azide or hydroxylamine into rats immediately before x - irradiation did not increase the radiosensitivity of tumours . injection of large doses of azide or hydroxylamine into mice before irradiation reduced the mortality from x - irradiation of the whole body . ( 5 ) catalase activity could be expressed as a qo21 - 29 x 10h202 value in p11 . 
the investigation was supported by grants to the royal cancer hospital and chester beatty research institute from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund , and the national cancer institute of the national institutes of health , u.s. 
cook. from the bland sutton institute of pathology and the barnato joel laboratories , middlesex hospital , london , w.1. received for publication april 5 , 1951 . the effects of high - frequency electric fields on living tissues , micro - organisms and viruses have been extensively investigated in the last fifty years . short - wave fields were first applied to animal tumours by schereschewsky ( 1928 ) using a transplantable mouse sarcoma , and by schereschewsky and andervont ( 1928 ) working with the rous fowl sarcoma ; these workers claimed to have produced complete regression of a number of the tumours following their results , together with those of subsesubjection to electric fields in vivo . quent workers who have reported investigations into the effects of short waves on animal tumour tissue in vivo and in vitro , were reviewed by dickens , evans and weil - malherbe ( 1936 )  . 
from a consideration of previous studies and as a result of their own extensive investigations performed with tumour tissue to which short - wave fields were applied both in vitro and in vivo , dickens , evans and weil - malherbe ( 1936 , 1937 ) concluded that , when heat effects were eliminated , ultra - short waves had no action on tumours or isolated tissues ; all the findings reported were , in their view , due to the action of heat . the many studies concerned with the effects of high - frequency electric fields on bacteria , bacterial toxins , viruses and unicellular protozoa which followed the original experiments of d ' arsonval and charrin ( 1896a , 1896b ) have been reviewed by burton ( 1949 )  . in commenting on the extreme variation of the results reported , burton ( 1949 ) emphasized that it still remained to be determined whether or not any action of the short waves existed apart from heating effects in the suspending medium . a recent claim was made by nyrop ( 1946 ) to have discovered a so - called specific effect distinct from heat effects , when pulsed fields at a frequency of 20 mc / s were applied to bacterium coli cultures in a fluid medium , the virus of foot and mouth disease , and unspecified tissue cultures . this claim was been criticized on the grounds that energy absorption by ionic and dipolar processes in the medium immediately surrounding the bacterium or virus might have resulted in a local temperature rise sufficiently high to destroy it , even though the general temperature of the test specimen were kept below the lethal level ( jackson , 1946 )  . 
they were between 8 and 14 weeks old when inoculated and belonged to two of the institute 's lines , which have been described by greenwood , blyth and carr ( 1948 ) , or crosses derived from them ( intensity , breeding , breeding hen x intensity cock , intensity hen x breeding cock )  . 
both the age at which the birds were inoculated and their distribution within the various line groups were determined by the exigencies of the supply . preparation of material for irradiation . for each experiment a bird with a large actively growing sarcoma of anything from 8 to 35 days ' growth from the date of inoculation was selected as a source of tumour material . 
the speed and the duration of the run of this machine was varied with each individual tumour , but was so arranged as to give homogenization of the resulting the tissue ; disintegrated material was placed in tubes and centrifuged very lightly ( in a horizontal centrifuge accelerated to 2000 - r.p.and at once decelerated ) , so as to bring all the contained air to the surface as a sharply demarcated layer of foam , which was then removed . 
the material obtained in this way , referred to in this paper as " disintegrated tumour , " was either mounted at once for irradiation , as described below , or was used in the preparation of other material for irradiation as follows : this was usually achieved in less than 1 minute . where a preparation of disintegrated tumour largely free of cells was to be irradiated , it was made by placing 4 c.c. 
the filings and tissue debris were separated off after the period of shaking by centrifuging in a horizontal centrifuge for 5 minutes at 2000 r.p.the supernatant fluid so obtained was drawn off and centrifuged again for 15 minutes at 6000 r.p.in order to throw down at least the greater part of any remaining cells . 
the supernatant fluid resulting from this final centrifugation , designated " virus suspension " , was drawn off ready for irradiation . water flow calorimeter c02 ice specimen standin wave icatoa from magnetron jacket for freezing mixture specimen at centre of waveguide ( maximum field strength ) 1 1 + 1 specimen at side of waveguide ( field of low intensity ) fig . 
with the experimental conditions used this peak field was given by1016v / a volts cm . - 1 , where a - average power in watts . where a section of the guide was filled with carbon dioxide ice the field at the central point of the section depended as well on the length of the section filled and on the dielectric constant of the carbon dioxide ice . this latter had been found ( in a separate experiment ) to be 1.6 at 3000 mc / s , and the length of the guide filled with the carbon dioxide ice was adjusted so as to be half the wave - length of the radiation in the ice . 
under suic ' h conditions the block of carbon dioxide ice was non - reflecting and the field strength at the central point was given bythe field in a frozen specimen at the central point of the carbon diqxide ice blbck differed from that in the ice in the absence of the specimen , since the dielectric constant of the frozen material differed from that of the ice . although the dielectric constant at 3000 mc / s of disintegrated tumour or virus suspension at room temperature is high ( between 40 and 80 ) , in the frozen state it drops to the region of 2 , not far removed from the dielectric constant of the carbon dioxide ice . 
the overall exposure time in each experiment was thirty minutes , corresponding to 9 x 105 pulses of 0.6 x 106 seconds ' duration each . the total time for which the field was operative was therefore 0.54 seconds in each thirty - minute exposure . 
cook surrounding the virus could take place ( experiment 1 , irradiation without cooling ) , and under conditions where precautions had been taken to prevent such energy absorption ( experiments 2 , 3 , 4 , 5 , irradiation with cooling )  . it is considered that the method of cooling employed was such as to keep the temperature of the material exposed to irradiation below 70 c . exposure to a temperature of below 70 c . 
on the other hand , absorption at a resonant frequency increases as the such absorption does not occur in water at microwave temperature falls . frequencies , but may possibly take place in large molecules or parts of them . thus , in the irradiation of frozen material , absorption by ionic conduction and dipolar orientation was avoided . 
at the frequency of 3000 mc / s . the results in table i can be attributed to energy absorption by ionic and dipolar processes in the medium surrounding the virus causing a general temperature rise well above the lethal level . thus the results of the present experiments show that any effects of the microwave field upon the rous no . 
where such heat production was eliminated , microwaves of a frequency of 3000 mc / s were found to have no demonstrable effect on the virus of the rous fowl sarcoma as judged by changes in its tumour - producing activity . 
where heat production was allowed to take place the tum6ur - producing activity was abolished . the expenses of this investigation were borne by the british empire cancer campaign . the authors wish to express their thanks to professor j . 
calcutt. from the department of cancer research , mount vernon hospital , and the radium institute , northwood , middlesex . received for publication april 16 , 194 ' the question of the involvement of the polycyclic hydrocarbons with sulphydryl groups during the process of carcinogenesis has been under discussion for a ceitain indirect evidence exists and has been reviewed by crabtree long time . ( 1947 ) , who concludes that the available evidence does not warrant any decision as to whether the involvement is direct or not . in other directions mueller and rusch ( 194t3 ) could obtain no effect upon the activity of urease - - this being dependent upon the integrity of the - sh groups - with benzpyrene solution . 
on the other hand rondoni and bassi ( 1948 ) have found benzpyrene to inhibit the papainaise digestion of gelatin and also the cathepsins of rat sarcoma and horse liver . 
the non - carcinogenic hydrocarbons , phenanthrene , anthracene and pyrene , had no action . calcutt and newhouse ( 1948 ) also found that the photodynamic action of benzpyrene was inhibited by cysteine hydrochloride . further work ( calcutt , 1948 ) showed that certain other - sh - containing compounds were also effective as inhibitors of photodynamic action . in the attempt to find the mechanism of this action it was found that after incubation of a colloidal suspension of benzpyrene in a solution of cysteine hydrochloride the characteristic yellow - green fluorescence colour of the benzpyrene changed to preliminary attempts to isolate this blue fluorescing compound were pale blue . unsuccessful , but it was found that the mixture no longer gave a positive test this implied the inhibition of the - sh group of the with sodium nitroprusside . cysteine and formed the starting - point for further work . the inhibition of - sh groups . using colloidal benzpyrene in distilled water , tests were carried out with a in each case the technique was the same . equal aniounts series of compounds . of a solution of the sulphydryl - containing compound were placed in each of two tubes . 
with slightly alkahne nlixtures , however , a small amount of blue fluorescing compound was obtained in solution . for all the cases mentioned above incubation has to be continued for upwards of 11 hours at a temperature of 65 ' c . 
before any inhibition became apparent . at lower temperatures the action was very slow , and at room temperature - 25 ' c . - there appeared to be no effect whatever . prelim ' mary trials having indicated that caffeine solutions had fittle effect upon - sh as detected by nitroprusside , some of the previous experiments were repeated , using a solution of benzpyrene in a 3 per cent caffeine solution . 
inhibition of - sh was achieved as before , but this time inuch more rapidly - 30 nlinutes at 650 c . isolation of the reaction products . under the conditions so far investigated the yield of the pale blue fluorescing product of the reactions has only been very small . nevertheless it has been found possible to isolate products from both the alkahne and acid reaction rmxtures . 
from the alkahne reaction raixture a water soluble compound was derived . this is soluble in organic reagents , strongly adsorb6d to silica , strongly adsorbed to alurnina , fluoresces a whitish - blue colour in ultra - violet light . 
on addition of dilute acid it changes to a blue fluorescing compound which is soluble in organic reagents insoluble in water but soluble in dilute alkali . from the acid reaction mixture a com ound has been separated wliich is soluble in organic reagents , soluble in dilute alka ' li , insoluble in water , adsorbed strongly to alumina and is weakly adsorbed to silica , moving down slowly as elution is continued . thus in their physical properties these compounds show a remarkable similarity to those separated from aninials and designated by weigert and mottrani ( 1946 ) as bpx . , , bpfj aind bpf21 this latter apparently being identical with the compound characterized by berenblum , crowfoot , holiday and schoental ( 1943 ) as 8 . 
furthermore the evidence suggests a considerable parallelism , even if not identity , with the course of events after the introduction of benzpyrene into the animal body . whilst the apparent identity of the fluorescence spectra does not - imply strict cheniical identity , it does mean the very close relationship of the substances concerned . from this it is reasonable to suggest that the interaction of benzpyrene with a - sh containing compound gives rise to a substance of the bpxj type . this , bowever , is in the presence of acid successively broken to compounds of bpfj and bpf2 type . it has already been suggested by crabtree ( 1947 ) that the detoxication of benzpyrene is by way of - sh compounds . in view of the evidence presented above this must now be regarded as being most probable . crabtree ( 1940 , 1944 , 1945 ) has as a result of his work with - sh inhibitors suggested the involvement of sulphur in carcinogenesis caused by the polycyclic hydrocarbons . this is further reinforced by the recent work of lusky , braun and woodard ( 1947 ) , who inhibited the carcinogenic action - of the benzpyrene by application of b.a.l. 
 ( 2 : 3 - dimercaptopropanol )  . additionally , evidence has been put forward by weigert , calcutt and powell ( 1947 ) to the effect that detoxication occurs at the site of careinogenesis . 
korteweg. victorieplein 45 , amskrdam , neturlands . received for publication february 12 , 1951 . most curves indicating the cancer death rates per million living in the different age - groups rise continuously with advancing age . 
the numbers of lung cancer deaths in the netherlands and in england and wales , 1125 and 5941 respectively , were large enough to exclude the possibility that these exceptions to the rule might be caused by chance only . is this decrease of the cancer death rate at a relatively early age a characteristic of lung cancer or is there some other explanation ? cia l%22 r . 
2 , which is derived from table l the age curves for males in all yeargroups given show the same early decline of the lung cancer death rate , with the .2 ^ ^ ^ 35 - 44 45 - 54 55 - 64 65 - 74 75 + years fig . 
3 , constructed from the numbers following one another vertically , show us , for each age - group separately , the increasing lung cancer mortahty in the course of years . 
3 we can derive , by interpolation , for each year and each age - group separately the approximate values of the cancer death rates . this has been done for the years 1915 , 1925 and 1935 . 
4 it is necessary to take the following points into consideration : cancer only develops after a long period of preparation , which in most cases can be counted in decades . those who at the age of 80 contract cancer , do so partly because of a tendency to cancer years before - let us say at the age of 70 . 
they are recruited from the group of the younger ones , whose tendency to cancer is also known , as it is given by the length of the ordinate belonging to that age in fig . 
4. it would be wrong , therefore , to compare in this respect persons who in ' 1945 were 80 years of age with persons surely this comparison should be who , in the same year , were 70 years of age . made with those who , ten years earlier , in 1935 , belonged to that age - group . 
we must presume , therefore , that it is not only the younger people who are endangered by these irritative factors . third : let us suppose that all males were exposed to these irritative factors to about the same degree , and that in each of the last 40 years the quantity of these factors had increased considerably . 
were this so , then really we would expect to find an " age curve " for lung cancer approximately such as we did if one fact proves the reality of the great increase of lung cancer in the find . last 40 years , it is the sbape of its " age curve , " now demoilstrated as being an illusion only . artificiary , with older age , the lung cancer age curve is pushed down . at this moment , the increase of lung cancer in the younger age - groups came to a halt , even then it would - progress in the older age - gr6ups up tir the moment when theillusionary age curve changed into the real one . 
we can ' ut it in another way : at this moment the lung cancer mortalitv is lower than corresponds mr - ith the tota - i amount of the causative irritative factors . the lung cancer " ceifing is lying at a far higher level than the mortality figures would suggest . up to the age - group 55 to 64 inclusive the shape of - the illusionarv age curve is about normal ; it is only after that , that the sharp dechne begins . in 1945 , in england and wales , in males less than 65 years of age , the number of deaths from lung cancer was 33 - 8 per cent of those from " all cancers with the exclusion of lung - cancer " ( registrar - general , 1947 )  . 
6 this also means that in this case the total number of cancer deaths in males would have ' been 30 , 835 + 10422 = 41 , 257 , and not 36 , 776 , which was the number given in the statistical review for 1945 ( registrar - general , 1947 )  . following the same reasoning it appears that in 1949 , in the netherlands , for males this " ceiling " was lying at a level of 1.710 , whereas the lung cancer deaths registered numbered 1125 only . it is clear that the " ceiling " will never be reached except after a long period of rest , with stationary lung cancer death rates in the younger age - groups . 
6. - balance of lung cancer mortality in males , england dnd wales , 1945 : - _ rears ..1 - - lung cancer deaths recorded deficit lung cancer risk lung cancer age curve after correction . ..... 
pseudo lung cancer age curve . 5941 4481 10 , 422 after having studied this table we no longer wonder that in england and wales . cancer in males is again on the increase . 
and still , if in 1948 the " ceiling " of lung cancer had been reached , the total number of cancer deaths would not have been 40 , 026 , but more than 46 , 000 ! in females lung cancer is also increasing . 
an analysis of its age curve , such as i have made in this paper for lung cancer in males , shows us that , just as formales , the real age curve for females closely resembles that for the " non - hormonal cancers " ( cancers other than those of breast and uterus ) in females . the problem which lung cancer presents to us is a very serious one , not only for england and wales , but also for the netherlands and many other countries . * in the review for 1948 ( registrar - general , 1950 ) the numbers for lung cancer are only given in combination with those for cancer of the mediastinum . during the last 40 years cancer of the mediastinum has not changed much in frequency . 
the number of cockerels was too in all examinations consmall to admit a proper comparison between sexes . cerning weight , ratio of cortex : medulla and cholesterol content , however , the examined cockerel adrenals did not differ from the female ones . 
each group in the following , control as well as lymphomatosis groups , thus included one to three cockerels . elliot and tuckett ( 1906 ) found no positive correlation between adrenal weight and body weight in adult birds , and our figures support their observations . if the normal birds are equally divided according to body weight into one light and one heavy group , the former had on the contrary some higher mean adrenal weight . 
the gland weights are therefore given in absolute figures . about half of each examined group was composed of white leghorn birds , while the other half consisted of rhode island reds , barred plymouth rocks and crossbreds . 
as was stated concerning sexes , this material did not indicate still , if such differences exist , which may very well differences between breeds . be demonstrated with bigger breed groups , their effect ought to have been fairly eliminated in this investigation by similar breed distribution within the compared groups of birds . control birds as well as lymphomatosis birds were collected during the same seasons - autumn and winter . 
in order to reduce the error produced by the uneven distribution of the cortex within the gland , part of the gland periphery was thus always made part of the picture . the picture was then enlarged to an area of about 300 cm.2 the total area , with the fibrous capsule and notable vessels excluded , and the area of the cortex were determined by planimetry . 
216.833 11273 1 - 61 the difference between gland weights of lymphomatosis birds and normal birds , 63 - 23811 - 334 , is highly significant ( t = 5579 * * * for df = 58 )  . 
the tumour size in neural lymphomatosis is always considerably less than in the visceral variety . the measurements of cortical and medullary areas clearly show that the enlargement is entirely caused by increase of the cortex . 
la than from comparison is in fact decreased . of the means , as two lymphocytosis cases showed exceptionally high cholesterol values and thus brought the mean to a higher level than that characteristic of the majority of cases . 
the impression was that lymphomatosis in a more or less advanced stage is characterised by a big adrenal cortex which in most cases is relatively poorer in cholesterol than normal cortex . the histological examination now and then showed cases of lymphomatosis with considerable disappearance of sudanophil substances but hardly revealed the slight but systematic deprivation as did the chemical determination . as will be shown in a later paper , acutely running experimental lymphoid tumours in chicks ( a transplantable strain of lymphoid tumour derived from a case of spontaneous lymphomatosis ) runs with a still more marked depletion of cholesterol than spontaneous , chronic lymphomatosis as well as with adrenal enlargement . this would correspond with sokoloff 's first stage of adrenal hyperactivity in rous sarcoma . 
he concluded that the second stage was one of hypoactivity and lipoid storage . the results of our investigation indicate , however , that in avian lymphomatosis the second stage is also characterised by hyperactivity . 
a less probable alternative explanation would be that the cortex does not grow as a consequence of increased demand of steroids but because of difficulties in producing theon the contrary , the parallel with selye 's ( 1950 ) general adaptation syndrome with increased adrenal activity first during the alarm reaction and later in the stage of resistance is obvious . 
3. received for publication april 21 , 1951 . studies of the electrophoretic behaviour of sera from patients bearing malignant and non - malignant tumours have been carried out by various workers with the view to their utilization as diagnostic or prognostic tests for cancer . 
polarography has also been investigated as a possible clinical tool for diagnosis or prognosis following brdicka 's ( 1933 ) discovery that proteins give a characteristic " catalytic double wave " in ammoniacal cobalt salt solutions . applications of this method to the study of sera have shown differences between specimens obtained from normal and pathological cases , and the results of an examination of over 100 sera from cancer subjects has been published by one of us ( butler , although good correlation between the wave height and the pathological 1951 )  . condition was obtained , a number of false positive and false negative results were included , the latter particularly in cases of cancer of the buccal cavity and skin . the electrophoretic behaviour of sera has been discussed by a number of workers ( seibert , seibert , atno and campbell , 1947 ; petermann and hogness , 1948a , 1948b ) , and the most consistent changes found in pathological conditions were increases in the c1and a2 - globulin levels . however , no specific changes have been found for any particular clinical conditions ( mides , alling and morton , 1950 )  . the work of winzler and his colleagues ( winzler , devor and mehl , 1947 ; winzler , devor , mehl and smyth , 1948 ; winzler and smyth , 1948 ; mehl , humphrey and winzler , 1949 ; mehl , golden and winzler , 1949 ; weimer , mehl and winzler , 1950 ) , has shown that a mucoprotein , isolated from normal plasma , appears to be responsible for the polarographic filtrate wave . this mucoprotein migrates in the al - globulin fraction , when examined electrophoretically at ph 8 ' 4 in barbiturate buffer . it has an isoelectric point at ph 1 ' 8 and still has a negative charge at ph 4 ' 5 . 
the acidic protein fraction demonstrated in cases of gastric cancers by petermann and hogness ( 1948b ) has been shown to be a similar mucoprotemayer ( 1942 ) had previously isolated a " mucoid - like substance " from horse serum which he claimed was the polarographically active seibert et al . 
 ( 1947 ) showed that increases in a2 - globulin were paralsubstance . leled by increases in the polysaccharide content of the serum . these results suggest that the polarographic and electrophoretic patterns of cancer sera may be due to mucoproteins which migrate in the a - globulin group . 
the results were expressed either as the height of the filtrate wave , or as the protein index of muller and davis ( 1947 ) or as the blood index ( butler , 1951 )  . the results of the electrophoretic measurements were expressed in terms of the areas ( measured by means of a planimeter ) under each of the peaks of the descending differential patterns ( longsworth and macinnes , 1940 ; svensson , 1943 )  . 
the relative composition was expressed by computing the percentage contribution of the area under any one peak with respect to the area under the whole pattern , excluding the boundary anomaly . 
a statistical evaluation of the results was therefore necessary in order for this an estimation of the change in per cent to draw any valid conclusions . and absolute composition from the normal to the pathological condition was made . 
no such increase in this fraction was observed in the two lymphosarcoma cases investigated here , nor in any of the three cases investigated by petermann , karnofsky and hogness ( 1948 )  . calculation of correlation coefficients between the component peak areas and the polarographic fitrate wave heights ( f ) and blood indices ( bi ) indicate significant relationships between the ocl - globulin area and the filtrate wave heights and blood indices factors in the pathological group . it is of interest and importance that no correlation between the ocl - globulin content and the polarographic factors was found in the normal group , and similarly none of significance if the normal and pathological groups are considered as one population . this is demonstrated in the correlation diagram shown in fig . 
3. correlations between the oq - globulin content and the polarographic indices were not found when percentage composition was considered , indicating that complications by other variable factors may occur . calculations of the correlation coefficients and inspection of the correlation diagrams shown in fig . 
correlations between the serum composition and polarographic factors are discussed , and their relation to the suggested anomalous mucoprotein content in the ocl - globulin fraction is indicated . we wish to thank d . 
the investigation has been supported by grants from the british empire cancer campaign , the jane coffin childs memorial fund for medical research , the anna fuller fund and the u.s. 
pda was all rats received greens once ' %eekly . added in a concentration of 0 - 06 per cent . the diet and water were given ad libitum . twenty of 50 rats r ' eceiving this diet served as controls , whilst the remaining 30 rats each received - a daily addition of 10 ml . 
in two of the tumours ( rat ca 801 on the pda control diet and rat cl 917 receiving fresh milk ) pancreatic tissue was recognized and the origin of the tuniours . 
he describes these extraas being similar to reticulo - sarcomas or " composed of spindleordinarv tiimours shaped cells and multi - nucleated giant cells . as another deviiation some tumour cells . 
grouped in bulbous masses , show an evident tendenev to concentiric arrangement of cells which are more or less keratinized towards the centre sin - tilar to ordinarv squamous cell epithelionias . " the hver of rat cl 912 was infiltrated , %ith tumour cells . over the two - vear period in which the semi - synthetic diet was used , some 150 rats receivmg this diet without the addition of pda have been dissected . during this period carcinomas of the no pancreatic tumour was encountered . small intestine were found in three piebald and in one albino rat . in the present series of 50 rats fed pda one gimilar intestinal carcinoma was found . 
tumours not localized in the liver have not been observed previously , partly because of the preference of the compound for the liver and partly because experiments in which the liver has been protected ' were terminated too early for ttimours to develop elsewhere . whether or not the substances in the diet which defer or prevent tlle produetion of hepatic tun ' iours by feeding pda are really anticarcinogenic or only protect the liver has been questioned . it seems that in the case of milk at any rate only the liver is protected from the carcinogenic activity of pda , and that tumour development generally is not prevented . it is remarkable that the extra - hepatic tumours should arise in an intestinal gland , and this seems to siiggest that organs which might be connected with the metabolism of pda are attacked . the conception that milk has a protective action on the liver only is interesting in ' view of the general plan of these experiments , the object of which was to find , if possible , an explanation of the prevalence of hepatic tumours in the natives in it might be assumed that the effect of a careinocertain parts of africa and asia . - genic factor which produces hepatic tumours , given a certain set of dietary habits and environmental conditions can be modified when the conditions differ . 
the usefulness of ultraviolet absorption in studying solutions of methylcholanthrene in different solvents and the physico - qhemical significance of spectroscopic data suggested an approach to the standardization problem . it has become necessary for us to discontinue work on the suspensions , and there is no likelihood of our returning to the matter . 
at the end of the exposure time the paste , which had been kept moist through the 42 - day period , was extracted for 24 hours with 35 ml . 
3. - ultraviolet absorption curves from a " protected " suspension of mnethylcholanthrene after 80 days ' exposure to diffuse davlight . curves a , b , c as in fig . 
4. - ultraviolet absorption curves from an " unprotected " suspension of methylcholanthrene after 80 days ' exposure to diffuse daylight . curves a , b , c as in fig . 
4 , a , the contribution of scatter predominates . it is evident that these solutions differ markedly in the type of suspended material , and this might well result in substantial differences in biological behaviour . in order to arrive at a representative selective absorption curve the scatter component must be subtracted from the observed data . 
5. - ultraviolet absorption curves of a saline extract of ground , moist methylcholanthrene crystals which had been exposed to diffuse daylight 42 days before the extract was prepared . curves a , b , c as in fig . 
the procedure for making these approximations is as follows : from an inspection of the curve plotted from the spectrophotometer data the contribution of scatter and turbidity is estimated and a smooth curve characteristic of scatter and turbidity is drawn to approximate this contribution . 
the ratio of the difference obtained as above and the density value at the same wave - length of a known concentration of the solute dissolved in a solvent in which scatter is absent is determined . 
the ratio so found is used as a multiplying factor which is applied to the density values of the reference curve ( known solute in true solution ) at several wave - lengths . this product is subtracted from the density values at corresponding wave - lengths of the mixed scatter - absorption curve to give a series of density values which are plotted - , and ' a smooth curve is fitted to the points so determined . 
the procedure as outlined gives a family of curves , with each member progressing towards a more accurate estimation and being uniquely related to the known absorption curve of the solute , and a mixed curve which is assumed to be composed of true absorption of the solute and a scatter - turbidity component . such a series of approximations can be made when one knows from other sources the true absorption spectrum of the solute , and can use this information as a standard of reference . the above procedure has been used to determine the scatter curve presented in the figures of this paper . 
5 shows the absorption of th3 extract from the ground methylcholanthrene there is a large scatter contribution , otherwise the curve bears little crystals . resemblance to the curves from the suspensions . 
belcher. from the wards and the bland - sutton institute of pathology , the middlesex hospital , london , w.1. received for publicatiod , may 16 , 1952 . adenocarcinoma in the oesophagus may arise in three ways : ( 1 ) as an upward extension of a carcinoma of the stomach , ( 2 ) as malignant change in the mucous glands that are normally found in the oesophageal submucosa , and ( 3 ) from ectopic gastric mucosa . the first is not uncommon ; the second is rare . the third , also rare , is the type that concerns us here . in 1950 carrie reported a case of adenocarcinoma of the oesophagus that had arisen in an area of ectopic gastric mucosa . 
he reviewed the literature and likened the lesion to the unicorn in that many authors had described it , but only one had ever seen it . although he makes no reference to the possibility of a hernia being present , the description of the specimen , coupled with the fact that the tumour was in the cricothyroid region ( where ectopic gastric mucous membrane is most frequently encountered - schridde ( 1904 ) ) , makes it certain that this was indeed a genuine example of this rare lesion . bosher and taylor ( 1951 ) describe a case in which ectopic gastric mucosa was present in the oesophagus . there was reflux oesophagitis and stricture formation at the level of the aortic arch . at first sight this would appear to be a case similar to the one about to be described , but it seems more likely that it is another example of hiatus hernia with extreme secondary shortening of the oesophagus , as the barium meal strongly suggests that only a small portion of the stomach is in the abdomen . although they state that at operation the hernia was small , it is notoriously difficult to distinguish stomach from gullet on external appearances alone . 
he had no difficulty with fluids . one week prior to admission food stuck in the same place and was regurgitated . since then solid food would not pass at all . and no glands were palpable . on examination the patient looked well . there was no wasting or dehydration on 14 . 
the oesophagus was removed from a point 2 inches above the tumour to the cardia and the free end implanted into the upper part of the stomach . post - operatively the patient had some fever and pylorospasm but was eventually discharged from hospital well on 4 . 
the mucous membrane above the tumour was entirely squamous in type and was normal for the oesophagus ; that below the growth was entirely glandular apart from a few islands of squamous epithelium about 2 inches above the lower limit of excision . 
the lower half of the oesophagus contains only smooth muscle in its muscular coat . in the case described , striated muscle was present down to and including the site of the adenocarcinoma . this represents a point about 5 inches above the junction of gullet and stomach . 
the normal gullet is about 10 inches long as meastired from the termination of the pharynx at the level of the cricoid cartilage to the cardiac orifice of the stomach . it would thus appear that the striated muscle in this case had a normal distribution . however , the circular muscle - fibres at the squamo - glandular junction appear to have thickened to form a sphincter . 
this constitutes a departure from normal , and it may have prevented regurgitation of acid secreted by the gastric mucosa lining the lower half of the gullet . this may well have prevented the development of oesophagitis earlier in the patient 's life . there was definite histological evidence in this case that the adenocarcinoma had arisen in the glandular mucous membrane immediately adjacent to the junction of the squamous and glandular epithelium . the emphasis is placed on " glandular " , for this showed varied degrees of chronic inflammatory and atrophic changes which obscured the normal picture of a gastric type of mucous membrane . these changes conform to those that may be seen in stomachs that are affected by chronic gastritis , including the atrophic type . 
thus we conclude that the lower half of the gullet in this case was lined by gastric mucous membrane that was the seat of chronic inflammatory and atrophic changes , which may well have been a factor in the development of carcinoma . the rare occurrence of adenocarcinoma in the oesophagus , other than those cases that have obviously spread from a gastric origin , has been put down in the 130 13 . 
of these large towns other than london 42 are located in the northern region of england and 41 in the remainder of england and wales , these groups being designated as " north " and " south " in this paper . 
the total deaths in all county boroughs , numbering 70 , 110 , were divided by the census population at the centre of the period , 1931 , and " expected ratios " of deaths to population obtained for each of the 16 sex - age groups . 
the census population of each town at each sex - age group was then multiplied by the corresponding " expected ratio , " giving the " expected " deaths in that group in 1921 - 39 . 
the actual deaths in a particular age group , or at all ages , divided by the expected deaths at the corresponding ages , or by the summation of them in all the age groups , and multiplied by 100 , gave for each sex comparative mortality ratios ( c.m.r. ) at each age group and at all ages . 
these are only approximate indices , since no correction has been made for irregular population trends in some of the towns ; but in no instance would the error from that cause exceed 5 per cent , and for only a few towns would it exceed 2 per cent . 
the values range from 130 to 55 , those which are greater than 100 by at least twice the standard deviation being denoted by a + sign , and those less than 100 by twice the standard deviation are denoted by a sign . 
stocks as a percentage of the expected deaths , giving a series of group c.m.r. 's , indi cating how the relative excess or deficiency of mortality characterizing the towns within the group changed according to age . 
 other digestive indices : similar ratios for deaths from cancer of the liver and causes included in the international groups for diseases of the diges tive system except appendicitis and peptic ulcer . 
 in table i 23 of the towns had c.m.r. 's exceeding 100 by twice their standard deviation or more , and 30 had c.m.r. 's less than 100 by that amount . 
no more than 4 out of the 83 would be expected to give values differing from 100 by as much as this on account of random variations due to a small number of deaths , so it is evident that the deviations for 49 of the towns cannot be so accounted for . 
was from 142 to 61 , with 27 towns showing significant excess over 100 and 27 a significant deficiency , so the deviations for 50 of the towns cannot be accollnted for by random variation . 
 and the social class index on the one hand and the age index on the other have been calculated separately for the 42 northern towns and 41 other towns , and also for the 83 together . 
the values given in table iii show that cancer of stomach mortality is positively correlated with the proportion of unskilled workers in the populapion , more so in south than north ; and in england and wales as a whole the coefficients are about + 5 for each sex . 
there is , however , a strong negative correlation between the social class index and age index , mean ing that towns with larger proportions of unskilled labour tend to have smaller proportions of their adult populations with ages over 55 . 
when the age index is kept constant cancer of stomach is still positively correlated with social class index to the extent of + 3 to + 4 , and this agrees with a similar result for the metropolitan boroughs of london in 1921 - 30 ( registrar - general , 1948 )  . 
 it is now seen that there is also a small negative correlation between cancer of stomach and the proportion of people of the same sex alive at ages 55 and over , and that this does not disappear when the social class index is made constant . 
 this is important , because it shows that the great variation in cancer of stomach rates in the towns is not due to mere differences in the correctness of certification of this cause of death by doctors . 
it has been suggested that the notable differences between cancer of stomach rates recorded in britain , denmark and switzerland may be due to excessive statement of this as cause of death in parts of those countries . 
if that were so it would be expected that the over - state ment would be greater amongst old than amongst young people , since the care devoted to diagnosis and correct statement of cause of death inevitably diminishes after about age 55 . 
consequently , if the great differences in standardized death rates in different towns , and in social grades , were due to excessive statement of cancer of stomach in certain of them , those with high rates would tend to have larger proportions of old people . 
for males the contrast is greatest at ages between 35 and 55 , when the death rates in the aggregate of 20 towns forming group ( a ) were just double those in the 18 towns forming group ( d ) ; and after 55 the relative excess diminishes to only 35 per cent at ages 75 and over . 
for females the excess in group ( a ) compared with group ( d ) was around 90 per cent up to age 65 , and then diminished to 45 per cent at 75 and over . 
 a pronounced decrease in the dispersion of death rates as age advances after 45 in males and after 55 in females is to be seen in table v , where rates for cancer of the stomach in the different social classes of the population of england and wales in 1930 - 32 are compared in the same way . 
for males the excess mor tality in class v , unskilled labourers , compared with that in classes i - ii , pro fessional and higher graded occupations , was as great as 86 per cent at 35 - 45 , and diminished progressively to only 8 per cent at 70 and over . 
for the wives of men in class v and single women in unskilled occupations the excess was 80 per cent at 45 - 55 , and fell to 37 per cent at 70 and over . 
 these relations with age are the reverse of what would be expected if the large differences in causes of stomach mortality between various large towns and between social classes arose from differing accuracy of death certification . 
 it will be seen from table 13 of that publication that the dispersion of rates according to a housing density grouping were much smaller at ages over 65 than at 45 - 65 . 
if the differences between cancer rates in groups ( a ) and ( d ) of table iv were due to more complete diagnosis , or excessive diagnosis , of stomach cancer in ( a ) than ( d ) , there must have been corresponding deficiencies in causes of death other than cancer in the towns of group ( a )  . 
the total deaths in all the county boroughs during 1931 - 39 from the various groups of causes concerned , and from cancer of the stomach , at ages 45 - 65 and at 65 and over were as shown in table vii . 
10 , 568 at the age - groups 45 - 65 , 65 and over , the totals of cancer of stomach deaths were not much different from the totals of digestive diseases excluding peptic ulcer and appendicitis , and since the great bulk of any transfer of deaths into or out of the cancer group by wrong certification must pass out of or into the " other digestive " group , this means that a strong negative correlation must exist between death rates attributed to the two groups if the large variation in stomach cancer rates arises from diagnostic differences amongst the towns . 
 indeed , if this were the main cause , doubling the stomach cancer rate ( as in group ( a ) compared with group ( d ) towns ) would involve almost abolishing the rate for other digestive diseases . 
transfer might also occur between stomach cancer and peptic ulcer as a result of mis taken diagnosis , but the numbers of deaths attributed to the latter group were small in comparison with those attributed to the former , except amongst males aged 45 - 65 . 
it follows that the transfer of the whole of them to cancer , if that were possible , in certain towns would fail to account for the excess of certified cancer in those towns ; and even large negative correlations between the two causes could not account for the variation in stomach cancer amongst males over 65 or amongst females of either age group . 
 table vi shows that for males of both age groups cancer of stomach death rates had no appreciable correlation with either peptic ulcer or other digestive diseases ; for females of both age groups there was a small but statistically insig nificant negative correlation with peptic ulcer , and a small just significant positive correlation with other digestive diseases in the country as a whole . 
 since none of the factors tested above can account for the differences in tables i and ii , the remaining explanation is that some extrinsic irritant factor is concerned which differed in intensity in the various towns . 
the curious contrasts in cancer of stomach mortality in london boroughs when grouped according to their source of water supply ( registrar - general , 1947 ) , correlation coefficients were calculated between the c.m.r. 
for cancer of the stomach during 1921 - 39 and the estimated total hardness of thewater supply of the 83 towns during 1911 - 31 , as shown in tables i and ii . 
it has to be remembered that the location of certain industries has been influenced to some extent in the past by the need for a soft water supply , and that in the north of england much of the industrial population is served by soft water . 
of the 42 northern towns 23 had water supplies with less than 7 degrees , or 10 parts per 100 , 000 of total hardness ; their average social class index was about 37 per cent unskilled and partly skilled workers . 
the 9 northern towns with water supplies of 20 or more parts per 100 , 000 total hardness had an average social class ' lildex about 42 per cent ; and the correlation between hardness and social index was in the 41 towns elsewhere there was no correlation between significantly positive . 
 the coefficients of correlation in table iii between cancer of stomach mor tality and hardness were positive in the north for males and negative in the south for each sex ; and when all the towns are grouped according to an ascending scale of water hardness , it appears that the c.m.r. 
no expla nation is offered for this , but the : figures are placed on record because they might at some future time fit in with other facts ( table viii )  . 
 102 100 llo 100 100 whatever irritant may be concerned in the production of gastric cancer , the effect of greater intensity of the irritant in one environment than in another might be ( 1 ) to increase the proportion of people developing cancer at each age without changing the latent period of develop : ment ; ( 2 ) to shorten the average latent period before cancer appears without changing the proportions of people affected , or ( 3 ) to increase the proportion affected and also shorten the latent period . 
if it is a long - continued mechanical or chemical injury to cells the predominant effect to be expected from increased intensity of action would be a shortening of the latent period , without necessarily increasing the proportion of people affected , although that might also occur . 
the ratios between death rates in groups of towns and between social groups would not be expected to fall with advancing age after 50 or 60 as in tables iv and v , and this suggests that the irritant is not an infective organis assuming some form of chemical or mechanical irritant is concerned , the latent period before cancer appears will vary rather widely about a mean value in the manner characteristic of most measurable vital factors ; and if the latent periods of gastric cancers in residents of all towns could be measured they would form a distribution approximating to the " normal " type . 
 it would be possible to reproduce the observed age - incidence of deaths from gastric cancer on the supposition that the irritant begins to affect a certain pro portion , p , of people who are susceptible to it at about 15 years of age , and th.at at each year of age thereafter an additional proportion p / k become susceptible to it and begin to be affected . 
 if , for example , the mean latent period before death were 20 years , with a standard deviation of 5 and normal distribution , k being a suitable constant , the numbers of deaths at successive quinquennial age periods from 25 - 29 to 65 - 69 would give a reasonably good fit to the deaths registered in england and wales in 194 7 . 
a shortening of the latent period in the towns where the irritant was most intense and a lengthening of it in those towns where it was least intense would then result in the ratio between the respective death rates diminishing with advancing age after about 40 , as in table iv . 
the observed facts appear to be consistent with such an explanation , but a careful study of the mathematics of the assumptions outlined above is needed before definite conclusions can be reached . 
 the death rates from cancer of the stomach in the 83 county boroughs of england and wales in the period 1921 - 39 show great differences , which cannot be explained either by chance variations , or by differing accuracy of certification of the cause of death . 
standardized mortality tends to be greater in the northern towns , in towns with a low proportion of people of advanced age and in towns with a high proportion of men in unskilled and partly skilled occupations . 
 cancer of the stomach death rates of men were unrelated with those for peptic ulcer or other digestive diseases ; but amongst women there was a small negative correlation with peptic ulcer and a positive correlation with other digestive diseases . 
shown bv irregular movements of the indicator between 3 ' and these bursts last for a few seconds , and are separated bv shghtlv longer after the indicator has re - ached zero . 
grow and form large embrvomas which persist for months or indefinitely . the following series of experiments was , undertaken to gain knowledge of the beha - viour of such embrvo grafts under various conditions . 
the teratomas consisted of a me ' lange of normal tissues arranged - in an irregular manner skin , cartilage , bone , around cysts containing hair , skin and various secretions . marrow , muscle , fat , cubical and columnar epithelium , lymphoid tissue , blood vessels , glandular structures and pigment were all found . 
no necrotic patches were present , nor was there evidence of any reaction on the part of the host . in order to discover the best time to transplant such a primary teratoma for passaging mice were killed once a week , beginning a week after inoculation , the ' teratoma removed , lightly minced with scissors and a small portion ( approximately 0 - 03 - 0 - 05 c.c. ) iiioculated with a grafting needle into the right flank of in this generation increase in six cm mice . size of the graft occurred in 66 per cent of transplants done before the 4th week , in 33 per cent or less in those between the 4th and the 8th week , while after the 10th week practically no increase in size took place , the small masses either persisting in practically the same state as when implanted , or actually disappearing . several of those passaged at the first and second weeks were again divided and a portion transplanted . these only increased to between 12 x 6 mand 4 x 4 this is the 2ageneration . 
the e of 8toring findy min - ed embryo tiww in glycerol at 40 c . - the embryo tissue was passed through the craigie pressure mi ioer and then stored in ampoules at 4 ' c . 
extremely active material capable of s " rdng fivsh t clours in less than two weeks has been obtained from both chemically induced and spontaneous sarcom firozen at - 790 c . 
almost all cases of leukaemia in 2955 days . the aka line are lymphogenous or of a very ' immature type - the so - called stem - cell leukaemia . the low leukaemia line which we have used for the cross - breediilg is called b . this line is also inbred . 
among hundreds of b mice we have previously observed , only one case of lymphogenous leukaemia was found . in the fl there was found 43 per cent of deaths due to leukaemia ; the age distribution of these mice dying from leukaemia is shown in fig . 
the age distribution is somewhat wider than in aka mice and the peak is displaced about 300 days later , so that in th ' is case the average lifetime for mice dying from leukaemia is 59119 - 6 days . in the f2 we encountered 37 per cent cases of leukaemia , and the distribution of age appears to be very wide , as shown by fig . 
the curve may be regarded as a combination of two distributions , one corresponding to the aka mice and one corresponding to the fl . the backcross derived from the fl crossed with aka shows a rise in the frequency of leukaemia to 49 per cent , and the curve concerning the distribut ' ion of age shows , as is seen from fig . 
l. - the age distribution of mice dying from leukaemia within the aka line - - - - - and the a ' ckli ii i t 60days ] days age lunit = 60daysj fig . 
the curve for the f2 shows a tendency to a bimodal form . you will see that , in spite of the genotypical uniformity of the mice of the aka line and the fl , leukaemia only develops.in respectively 63 per cent and 43 per cent of the animals . 
the percentages mentioned as is the case with the figures from previous experiments - calculated by comparing the number of mice dying from leukaemia with the total number of day , ; fig . 
4. - age distribution of leukaemia in backeross of fl mice to b line . dead mice , the animals dying before the first case of leukaemia occurs not being included . it is quite evident that this mode of calculation is entirely inadequate , because deaths caused by other reasons than leukaemia ( such as intercurrent diseases ) , will influence the result to a very high degree . 
the frequency in the fl is not so great as in the aka line , but this can be in part due to the fact that the cases appear at an average age of 300 days later , so that the deaths from other causes will decrease the frequency of leukaemia . the figures found in ' this material , as seen from the following considerations , support the view that the inheritance may depend on one single dominant gene . if we suppose that this is the case , we can calculate the expected numbers of leukaemic animals in the f2 and backcrosses to the parent lines on the basis of the observations in the aka and the fl mice . these results are calculated in table 1 , taking into account the deaths from other causes . these figures agree very well with the observations , but in the calculated mortality curves the agreement was not so evident . 
the difference is not significant . if we assume the presence of two genes the calculated number will only be 8 - 2 '  . these data thus support the hypothesis of a single domi ' nant gene . the variation in the average lifetime of the leukaemic animals has previously been described by macdowell , potter and tayl ' or ( 1945 ) , macdowell and richter ( 1935 ) , furth and barnes ( 1941 ) , kirschbaum ( 1944 ) , and cole and furth ( 1941 ) in similar crossbreeding experiments . 
the phenomenon seems therefore to be independent of the character of the lines used , which fact seems to refute the previous supposition that casual changes in the average lifetime of all the mice may influence the result . i would sooner say that the discovery confirms the supposition that the immature leukaemic cells arise by a somatic mutation in cells which possess a labile 112 g . 
where and how this mutation arises could be a if the animals are homozygous with regard to the labile gene , matter of chance . the mutation will naturally arise earlierand more frequently than ' is the case if the animals are only heterozygous . 
we spent more than eight months working on one such incidental problem , which had to be solved before we could proceed with the main work . this effort was well rewarded , however . 
we not only improved our experimental approach , but also acquired information that will further our understanding of the intricate role played by biological factors in regulating the influence of external agencies on living cells . in view of all this , i should like to point out that our investigations of the genetic potencies of carcinogens are still in an early stage . 
bartholomew 's hospital , london , e.c.1. received for publication february 11 , 1952 . radium and thorium are widely distributed throughout the earth 's crust , although , as yet , no large deposits have been found ( it has been estimated that uranium and thorium exist in as much as 4 and 12 parts per million respectively )  . both these materials decay through a radioactive series , and in each case one ' these two radioactive gases escape into the member of the series is gaseous . atmosphere where their respective decay products will be formed and these prothere are other sources ducts will probably attach themselves to dust particles . of naturally occurring radioactive material ( actinium , which decays to gaseous actinon ; potassium ; rubidium and carbon 14 ) , but these are insignificant compared to members of the radium and thorium series . the presence of radioactive material in the atmosphere was first observed by their observations were confirmed by other workers elster and geitel ( 1901 )  . most of these early determinations were made by in various parts of the world . the charged wire method , which gave quite good qualitative results . 
the rate of air flow depended on the length of tubing connecting the pump and filter - holder , but was always between 30 and 35 litres a minute . it was measured by a u - tube manometer , and controlled by a screw clip . 
the collecting time was 20 minutes , which does not necessarily give the maximum measurable activity , but allows the experiment to be completed in an hour . the efficiency of the filter was examined in a series of experiments in which one , two or three filter - papers of different types were used in series as a backing for the whatman no . 
as it was not possible to obtain standard samples of each member of the radium and thorium series , we determined the efficiency of the counter for measuring the ft particles from three radioactive these efficiencies were plotted against energy , and the efficiency for the isotopes . , f emitting members of the radium and thorium series were read from this graph . the efficiency of the counter for measuring a particles cannot be determined in the same way as for f8 particles ; since an unknown number of a particles will be absorbed in the filter - paper . in order to calculate the ac efficiency , a dust sample was taken and counted in the usual way ; a piece of aluminium foil ( thick enough to absorb all the ac particles ) was then inserted between the filter - paper and the geiger counter , and the count was continued . this experiment was the proportion of ac to ft particles emitted by repeated for a series of samples . the dust was deduced theoretically , and the proportion of a particles which were counted was determined from the drop in counting rate caused by interposing the aluminium foil . 
dawson the data for kew were taken unless there was a significant difference between these two sites , in which case that day was ignored or mean values were taken . 
dawson than those taken in the morning . rothamsted is a third - order station of the meteorological office and more accurate correlation of weather phenomena and activity were possible ; the conclusions drawn from the hospital results were confirmed . the activity was greater if the ground was dry or drying . 
the floor of the cellar was only 4 below street level ; there was some ventilation from a window and the door leading to the main part of the house . 
the cellar had not been used for several in order to avoid disturbing the dust , the pump and filter - holder were weeks . kept outside the cellar ( table iii )  . 
the proportion of radon atoms that will decay whilst passing through the filter - paper is negligible , but when one considers the very large absorptive capacity of carbon for radon , it is rather surprising that no radon was found . we have not investigated the proportion of the other members of the radioactive series that will adhere to dust particles . carmichael and tunniciffe ( 1948 ) removed the dust from a closed room by fanning the air across a greasy plate and noted the diminution of activity in an air sample . 
on introducing smoke there was an immediate increase in activity , showing that in a small room there is never an appreciable quantity of free radioactive atoms - they either become attached to dust or migrate to the walls . 
shelter tolerance ( maximum concentration ) 11 , 800 100 , 000 the figure for droitwich spa was taken from a brochure issued by the local council . our inquiries as to who made the original measurements were not very successful , but it is believed that they were made by professor h . 
schrodinger , at seeham ; 8 - 9 x 10 - 12 curie / metre3 of air . simpsoin ( 1905 ) made a very exacting survey of the air - borne radioactive material in lapland in 1904 , using the charged wire method ( table vi )  . 
read and mottram ( 1939 ) have published the results of some determinations of the radon concentration in the radium laboratories at mount vernon hospital , at the radium institute , and in the radium workshops of messrs . 
 ( all in or near london )  . in the last case a concentration of 22 x 10 - 7 curie / metre3 of air was observed . evans ( 1950 ) has calculated the dose received by joachimstal ( jachymov ) miners in a working day through inhaling radon . 
bartholomew 's hospital , in the city of london ; rothamsted , a semi - rural area , thirty miles from london ; chiswick , geographically in middlesex but actually a semi - industrial part of london ; and in the centre of manchester . 
the results were similar to those of other observers in different parts ofthe world ( table v )  . large day - to - day variations in activity were observed , but these can be explained by variations in the weather - the more stationary the air , the greater the concentration of active material . 
the slight differences between the four sites mentioned above may be seasonal . the experimental procedure was not sufficiently accurate to show whether thoron or its decay products were present . radon , absorbed on dust particles , was not detected . 
no variation with height up to 100 above ground level was observed . the results obtained in rooms with varying degrees of ventilation are of in the laboratory there was usually twice the activity found at the interest . open - air site on the roof . 
at chiswick , ventilating the room lowered the activity by as much as one - half , whilst in the coal - cellar the activity was 14 times greater than at the site in the garden . in the post office air - raid shelter the ventilation was as restricted as any found in habitable buildings ; the activity was 120 times as high as at the open - air control site , i.e. , nearly one - eighth the tolerance concentration of radon . in every case the large day - to - day variations were similar to those at the control site . these large amounts are due to the greater emanating area in a room ( compared with the open air ) from which the parent radon can escape , and to the restricted ventilation which will allow the radon concentration to build up . 
the amounts show no considerable difference between urban and rural districts , but there are large day - to - day variations which in situations out of doors are affected chiefly by the wind ; the more stationary the air , the greater in closed places , e.g. , an air - raid shelter underground , the amount the activity . may be 100 or more times greater than those in the street outside , but even these are small in comparison with the lowest amounts considered harmful to man . i wish to thank professor j . 
fisk , of the general post office , london , for their kindness in providing facilities for this investigation , which has been supported by grants from the medical research council , the british empire cancer cami wish to express my indebtedness to t . 
no definite conclusions were obtained with regard to the influence of the thyroid gland , but the results showed a remarkable reduction of mammary cancer in one of the two strains used . preliminary experiments ( vazquez - lopez , 1946 ; morris , dubnik and dalton , 1946a , b ) showed that thiourea ingestion produced a continuous anoestrus due to ovarian atrophy and the consequent underdevelopment of the mammary glands . 
vazquez - lopez breeding females only were used from the two lines of r3 mice , and both breeders and virgins from the c3h strathe breeders were allowed to rear their first litters and , after weaning , the mothers were taken for the experiment . the litters of the c3h breeders provided the majority of the virgins employed . in all groups care was taken to divide animals of the same litters between the experimental and control groups . the animals were housed in metal boxes , 6 to 8 in each , and fed rat cubes breeders and virgins of the c3h strain were separated , but and water ' ad lib . the two lines of r3 breeders were mixed together . thiourea was administered in the drinking water , beginning with a 0 1 per cent solution and increasing the concentration as much as possible without endangering the survival of the animals . 
the approximate amount of fluid ingested was determined by dividing the total content of the water bottles by the number of animals in the box . all the animals were individually marked . 
the age of the breeders at the beginning of thiourea ingestion was between 3 and 4 months . the virgins were 3 months old , so that the mammary gland was fully developed before the action of the drug started . the period of administration for some of the r3 animals was a year , so that most of the animals with tumours died during the period of ingestion . for the c3h mice , both breeders and virgins , it was 6 months , so that the animals were under normal conditions again when 9 or 10 months old . 
even concentrations of 1 per cent could be used before the mice showed toxic signs such as loss of weight and reduction of water intake . if the solutions were kept between 0 - 2 per cent and 0 * 5 per cent the r3 mice could be maintained for most of their lives without any apparent difference from the controls . 
per animal per day , and if the concentration of the drug was not reduced , many it was possible to reach a concentration of 0 5 per cent in most animals died . boxes , but it could be maintained only for one or two weeks . solutions of 0 - 2 and 0.1 per cent were used most of the time , and even with these doses the intolerance to the drug and mounting mortality necessitated the withdrawal of the after some days without thiourea the mice recovered drug after 4 or 5 months . and the drug could then be administered again , but the recurrence of toxic it was preferable to maintain the 6 months ' period without symptoms was rapid . interruption , even at the risk of losing more animals in the last months of treatment . the doses administered were therefore variable for the different animals and for different periods for the same animal , but from the approximate estimate of water intake it may be assumed that the minimum of thiourea ingested per day was between 2 and 3 mg . 
daily. effects on the thyroid gland . in the r3 mice the ingestion of thiourea provoked the typical hypertrophy this effect was and hyperplasia with great vascularity , loss of colloid , etc . evident even with a 0 - 2 per cent solution , and became more pronounced in proportion to the length of treatment and increased concentration . 
the mice surviving after the withdrawal of the drug had thyroids of normal size and structure without any signs of the former hyperplasia . the effects of thiourea in c3h mice were observed in the experimental animals that died during the period of ingestion of the drug . 
as the great majority of these mice restricted their water intake to a minimum in the weeks before their death , it could be argued that they were not actually under the action of the for this reason additional mice not included in the experiment were used drug . to test the effect under identical conditions , and were killed when the actual ingestion of thiourea was known . in all the 03h mice of the experiment the results of the examination of the thyroid gland were similar . thiourea administered in the drinking water did there was clearly not produce hyperplasia or hypertrophy of the thyroid . congestion of the organ which might cause a slight increase in size , but the histological picture remained normal , showing follicles filled with colloid and lined by cubic epitheliunone of the mice that died during the period of thiourea ingestion showed changes in the microscopical picture . 
among 20 additional female adult mice killed after drinking solutions of 0 - 2 to 0 5 per cent for periods of a week to 2 months , with actual ingestion of about 5 mg . 
the small difference in favour of the thiourea group was not significant , for the small number of animals and the lower tumour age of this group was also against any inhibitory effect of thiourea . all the tumours appeared during the period of treatment when some of the mice had received thiourea for 10 months without interruption . mammary cancer in c3h breeders . - of 49 mice at the start of the experiment , only 29 ( effective number ) reached the age at which the earliest tumour appeared . the other 20 died as a consequence of thiourea ingestion . eight of the 29 table i . - lymphoma incidence in r3 breeding female8 ( mh subline )  . total effective mice with number . 
the earliest developed in a mouse 367 days old , 80 days after the withthis was only 10 days less than the average tumour age drawal of thiourea . these figures confirmed the assumpfor the control group , which was 377 days . tion that ovarian function and mammary development were normal in the experimental animals at the average tumour age of the normal mice . in spite of these normal conditions the percentage of mammary cancer in the thiourea - treated mice was 28 per cent compared with 54 per cent for the controls . 
vazquez - lopez mammary cancer in c3h virgins . - twenty - one animals died during the period of thiourea ingestion , and 64 mice survived the 6 months of treatment and five among the 64 reached the period of appearance of the first tumour . in the developed marmmary cancer ( 8 per cent ) , at the average age of 571 days . control group 40 out of 96 animals ( 43 per cent ) developed tumours at the average age of 432 days . 
the animals treated were 270 days old when thiourea was withdrawn , so that ovarian activity and mammary gland development were presumably normal not only long before the average tumour age of the controls , but also very nearly when the first tumour appeared among the normal mice . 
assuming that after the end of thiourea administration the mice needed a month for total recovery , they would be comparable with the normals when 300 days old . only 4 mammary cancers developed in the control group below this age . the decrease in cancer incidence in the thiourea - treated virgins was highly significant ( x2 = 20 9 ) , and confirms the results in c3h breeders . in this group the average tumour age was also later than in the controls . 
the average life span of mice without tumours was longer , but with smaller differences from the control mice than in the breeders . microscopical study of organs in thiourea - treated c3h mice . a detailed study of the organs of c3h mice after longer periods of thiouracil and thiourea ingestion was published by dalton et al . 
1 and 2 show condition and weight of the mouse rather than with its age . glands of control and experimental mice of approximately the same age . the two main differences between thiourea - treated and control mice are the number of nodules of alveolar hyperplasia and the width of the ducts . 
the alveolar nodules of one gland or even of all the glands in a single mouse cannot be used to distinguish a thiourea - treated from a control mouse ; in some thioureatreated animals the number and distribution of nodules is the same as in the controls . 
the thiourea - treated mice , as a whole , had considerably fewer nodules of alveolar hyperplasia than the control mice , and the average number of nodules per mouse was less than half the figure for the controls . there are no records of comparative counts in similar experiments with reduced mammary cancer incidence , but huseby and bittner ( 1946 ) report that less than 1 nodule per 4 glands was found in some animals more than 340 days old kept on the restricted diet in the experiments of huseby et al . 
vazquez - lopez to indiscriminate reduction affecting equally all the glands of each animal , but to a clear decrease of the number of glands with ' nodules . only 32 per cent of the glands in the thiourea - treated mice had nodules compared with 51 per cent in there were also significant differences in the distribution the control group . and the average number of nodules for glands in each group , but the main effect of the thiourea administration is to increase the number of glands without any nodules . 
as the hormonal and systemic influences are the same for all the mammary glands in each mouse the cause of these differences between glands in the same mouse must be the result of local factors whose activity is restricted to the fields represented by particular glands . thiourea acts systemically mainly by stopping ovarian function and oestrogen production . 
at the post - mortem examination the ducts appeared full of whitish material , which made them conspicuous to the naked eye . it seemed therefore to be due to engorgement by a secretory product , but it could exist in glands without any indication of alveolar proliferafig . 
some ovaries appeared in regressed condition without corpora lutea or follicular development ; this occurred with the same frequency in both groups . most ovaries had follicles in all stages of development , and some of the corpora lutea became hyalinized , forming large homogeneous masses with few cells . this formation of corpora albicantis is probably a strain characteristic , since fekete ( 1946 ) found them in the dba high cancer strain , but never in the c57 black strahuseby et al . ( 1945 ) found them only in one c311 mouse with mammary - cancer , and in none of the diet restricted animals of their experiment . that is probably another of the characteristics in which the c3h mice used here differ from those in american laboratories . 
the corpora albicantis were very prominent among the cancerbearing animals , and their ovaries owed their large size partly to these structures . apart from their size , however , the ovaries of mice with tumours showed mature follicles and abundant corpora lutea , which suggested normal activity . these findings were contrary to the results of allen , diddle , strong , burford and gardner ( 1935 ) in several strains of mice , including the c31 . in all groups the condition of the uterus reflects that of the ovaries having tall epithelium , extensive glandular development and loose cellular stroma in the animals with well functioning ovaries and signs of regression in those with ovarian atrophy . no differences were found in the adrenal glands of thiourea - treated mice compared with the controls . 
the most important change , affecting both groups equally , was the presence of amyloid degeneration , which appeared on the borderline between cortex and medulla and progressed towards the glomerular zone with advancing age . in the oldest animals amyloid invaded most of the cortex , and only two or three layers of cortical cells remained intact . 
the medulla was never affected . " brown degeneration " was , on the contrary , never found in c311 mice , but was almost constant in r3 animals of high or low mammary cancer lines . 
the possibility of a specific activity of thiourea on blood - forming tissues and their neoplasms suggested by the agranulocytic reactions in patients treated with goitrogenic substances is not supported by the results in the mh high lymphoma line which agree with clinical reports of treatment of leukaemic patients ( limarzi , kulasavage and pirani , 1946 ; hansen - pruss , 1947 )  . that lack of oestrogen is the effective factor is shown also by the normal incidence of cancer corresponding with regular oestrus in spite of thiourea administration in r3 mice . 
the action of progesterone is still a matter for discussion ( lacassagne , 1937 ; heiman , 1945 ; burrows and hoch - ligeti , 1946 )  . indirect ways of decreasing oestrogenic activity give , however , less clear results . although low cystine diets completely inhibit mammary cancer in c3h mice ( white and andervont , 1943 ) , the effects of stilboestrol pellets which restore the development of the mammary glands raise the incidence only to 44 per cent compared with 92 per cent in the controls ( white and white , 1944 )  . in similar experiments , ball , huseby and visscher ( 1946 ) found that in spite of continuous administration of stilboestrol the mammary glands of strain a mice maintained on restricted diets during 15 months were considerably less developed than those of control mice . 
the possibility of other hormonal factors influencing mammary cancer development is also suggested by the results of shimkin and wyman ( 1945 ) , who found greater reduction in adrenalectomized c3h mice than after ovariectomy , and by the observation of wallace , wallace and mills ( 1945 ) of persistence of effects of temperature in mammary cancer incidence after ovariectomy . the results of temporary lack of oestrogenic activity caused by thiourea show that reduction of mammary cancer is not due to defective glandular development , and therefore that the hormonal effects are not limited7 to the morphogenesis of tissue susceptible to carcinogenic agents . 
mammary glands of two groups of mice of the same strain with different cancer incidences have identical morphology , and only differ in the total number of nodules ofalveolar hyperplasia in each group . 
huseby and bittner ( 1946 ) have shown by the study of c3h and hybrid mice with or without the " milk influence " that this influence is necessary for the presence of nodules . 
the distension of ducts found also in the thioureatreated group seems to be a sign of excessive oestrogenic stimulation , and may indicate compensatory excess after thiourea withdrawal . if the hormonal influences are sufficient for the alveolar development the smaller number of glands with nodules , which is the main result of thiourea administration , must be due to local factors . 
the lack of oestrogens ( and its possible compensation afterwards ) affects all the glands of the mice equally . these results point to the possibility of effects on local factors and producing different consequences in each gland of the same animal . 
the local factor involved in the persistence of alveolar nodules is the milk factor , and the distribution of nodules suggests that it is affected by thiourea administration . there are no grounds for supposing that thiourea can directly influence the milk factor , but there are some in favour of an indirect action resulting from the lack of oestrogens . apart from the considerable number of experiments on the effects of oestrogen adninistration on cancer incidence , there is evidence even in normal circumstances of hormonal influences in breeding and forced breeding , increasing the number of tumours . 
the higher incideixce in mice born in later litters compared with the earliest from the same mother has been explained by the different concentration of the milk influence with advancing age ( bittner , 1942a )  . if the increased hormonal stimulation is the cause of increase in the amount or activity of the milk influence , it is probable that the converse holds true also , and that the lack of hormones acts in the opposite sense . the relative importance of the hormonal influence among the three factors necessary for the genesis of spontaneous mammary cancer in mice is not exactly opinions range * from that of shimkin and andervont ( 1941 ) , who known . consider the hormonal factors as necessary only for the creation of a substratum for the carcinogenic action of the factor transmitted by the milk , to that of warner , reinhard and goltz ( 1945 ) , who maintain the dominance in certain cases of the inherited susceptibility upon the concentration of the milk agent . loeb , suntzeff , burns and schenken ( 1944 ) believe that the oestrogens act by stimulating the growth of the mammary tissue and sensitizing it to all types of stimuli , and bonser ( 1945 ) as a developing factor acting upon breast tissues already sensitized by the milk factor . 
the only common feature of all these opinions is to consider the different factors as completely independent variables . on this basis the opinion of bittner ( 1942b ) that each influence must be considered as complementary to the others and all equally important is , besides being noncontroversial , nearest to the observed facts . 
but if there are some factors which are affected and increased , or even created de novo by interaction of the others , the relative significance of each would not be the same . the effect of genetic susceptibility on some aspects of the milk factor activities has been already proved by heston , deringer and andervont ( 1945 )  . 
w.3. received for publication july 16 , 1949 . in an investigation of the body growthand tumour growth - inhibiting action of carcinogenic substances , it was found that the nature of the inhibition is profoundly influenced by the protein content of the diet ( elson and warren , 1947 ; elson and haddow , 1947 ; elson , 1949 )  . in rats maintained on a 20 per cent protein diet injection of the carcinogen usually has little immediate effect on body growth although a delayed action , resulting in rapid loss of weight followed by death , may occur later . 
carcinogenic hydrocarbon 1 : 2 : 5 : 6 - dibenzanthracene 24 hours after implantation of walker carcinoma 256 in rats maintained on a 20 per cent protein diet results in very little difference in size and weight of the tumours from those of controls . if , however , the animals are fed a 5 per cent protein diet the tumours of those similarly treated with dibenzanthracene were found to be only one - quarter the weight of those of controls when the rats were killed 13 days after implantation ( elson and haddow , 1947 )  . 
harris. * from the chester beatty research in.3titute , royal cancer hospital , london , s.w.3. received for publication january 11 , 1951 . themajor requirement for the investigation of the physical and chemical properties of the rous no . 
i sarcoma agent is a source of " purified " agent of a uniformly high infectivity , and which may be stored without loss of this activity , since it is not always convenient to compress the investigation to within the relatively short period in which the purified agent is stable in vitro . this paper describes a method for the production of concentrates of the vir ' us in a form suitable for storage , and the storage problem itself is considered in the following paper . a variety of chemical and physical methods have hitherto been used for separating and concentrating the agent from biologically - inactive tumour protein and nucleoproteins . claude ( 1935a ) found that such contaminants could be removed by adsorption , on to freshlv prepared aluminium bvdroxide gel , and the carbohydrate contaminant by precipitation with gelatthe agent was not directly affected , and a - combined chemical fractionation and dialysis gave a 25 - fold concentration in - terms of dry weight ( claude , 1935b )  . this method was also investigated by dmochowski ( 1948b ) , who recorded a 50 per cent increase in the activity of the agent compared with the startino , c5 filtrate . shemin , sproul and jobling ( 1940 ) , and shemin and sproul ( 1942 ) precipitated the agent from filtrates by addition of papain or of histone . 
nitrogen ( the range was 1 - 3 x 10 - 3 mg . to 7 x 10 - 7 mg . ) were found to be infective . concentration of the agent by centrifugation was first described by ledingham and gye in 1935 and fractional centrifugation methods have since been widely used ( mcintosh , 1935 ; amies , 1937 ; claude , 1937 , 1938 , 1939 , 1940 ; claude and rothen , 1940 ; pollard , 1938 , 1939 ; stern and duran - reynals , 1939 ; dmochowski , 1948a )  . claude ( 1938 , 1939 ) isolated a fraction corresponding to less than 3 - 5 per cent of the dry weight of the original extract which , in amounts corresponding to 4 - 0 x 10 - 10 mg . 
harris pollard ( 1939 ) and amies and carr ( 1939 ) were able to overcome the first difficulty by precipitat - ing the agent from a clarified extract by adjusting the ph to 5.0 to 5 - 5 . 
the isoelectric point of the purified agent is 3 - 5 , but tumour extracts deposit a mucoprotein at ph 5 - 0 , which takes down the agent with it . the aggregated agent , etc . , was then further concentrated by a low - speed centrithe aggregates were.broken down by tryptic digestion at fugation procedure . ph 8 - 8 to 9 - 0 and the released agent further " purified " by fractional centrifugation . alternatively , the ' mucoprotein may be hydrolysed by incubation of the extract - with hyaluronidase , which has no deleterious effect upon the agent ( siturm , and duran - reynals , 1932 ; shemin and sproul , 1942 )  . 
the agent may then be deposited directly from the non - viscous extract . bryan , riley , deihl and voorhees ( 1947 ) have avoided this difficulty by the simple , but uneconomical , procedure of rejecting the first , viscous extract . a further method which has been claimed to apply to the purification of small arrlounts of agent is that of chromatography on celite ( riley , 1948 )  . 
the agent is strongly adsorbed to celite from physiological salt solution , but may be eluted intermsoftheratio , biologicalactivity : withverydilute ( o - 001m ) saltsolution . nitrogen content , a 3to 7 - fold enrichment was obtained from a partially ' - purified three of the above methods , papain precipitation , fractional tumour extract . centrifugation after precipitation at ph 5 - 0 and direct deposition after treatment of the initial extract with hyaluronidase , have been reinvestigated from the point of view of the preparation of large quantities of agent in a form suitable for storage . 
a further method , methanol precipitation , hitherto applied to a number of other animal viruses , has also been investigated . cox , van der scheer , aiston and bohnel ( 1947 ) found that influenza virus ( from arantoic fluid ) could be precipitated in active form from suspensions in phosphate buffer at ph 7 - 0 to 8 - 0 by addition of methanol to a final concentration of 15 to 30 per cent . 
sharples air - driven supercentrifuge , stainles - 3 the rous agent becomes progressively more thermolabile as purification centrifuge b was used in a cold - room at o ' c . , and c was adjusted to the sharples centrifuge ( a ) was cooled with the centrifugal procedures used are listed below and steel bowls . - ( i ) clarifica ( ii ) deposition at ( iii ) deposition at ph 7 - 0 . 
the bulk of the tumour was extracted in the waring " blendor " with 10 volumes of water containing 1 : 10 , 000 hcn , and the small sample " minced with scissors " and extracted into a similar medium . suitable dilutions of these extracts were injected into fowls . 
0.005 m buffer at ph 7 - 2 containing hyaluronidase and 1 : 10 , 000 ticn . the tissue suspension was clarified ( b , i ) and the agent deposited from the supernatant ( b , ii )  . 
the control suspension ( a ) was ' assayed comparatively against ( b ) - resuspended papain - agent complex , etc . , ( b ) - supematant and ( c )  . 
and methanolic buffer solutions prepared , and cooled to these buffers contained ( a ) 40 per cent methancil , ( b ) 50 per cent methanol and ( c ) 60 per cent . methanol respectively in 0 - 005 m buffer . equal volumes of ( a ) , ( b ) , ( c ) or buffer ( d ) - control , were added to volumes of the supernatant . 
an equal volume of 50 per cent methanolic buffer was added under the same conditions as method 1 and the resuspended deposit assayed against the extract . the assay showed that the alcohol - deposited agent had only i per cent of the activity of the control suspension . ( 3 ) a similar clarified extract was prepared , cooled to o ' c . 
the deposit was resuspended in 0 - 005 m buffer at ph 7 - 2 , clarified ( b , i ) and the agent in the supernatant deposited ( b , ii )  . the pellet was finary resuspended in 0 - 005 m buffer , ph 7 - 2 , adjusted in concentration to the equivalent of i g . 
de osition after precipitation at ph 5 - 0 . a 10 per cent fresh tumour tissue suspension was prepared in the usual way , but with the omission of hyaluronidase . 
the air - driven sharples supereentrifuge with a maximum speed of rotation of 50 , 000 r.p. ( 62 , 000 g . ) was used by stanley in 1945 for the concentration of influenza virus for vaccine production . 
for deposition of the virus the stainlesssteel centrifuge bowl was invariably lined with cell ' ophane ( 7 / 1000 in . ) which may ( a ) be readily withdrawn and which ( b ) minimizes contact of the virus with metals . when unrolled this " liner " invariably showed a boundary , the distance of which from the bottom of the bowl , varied with the rate of flow of the virus in terms of total nitrogen distribution , the suspension through the centrifuge . deposit was uniformly distributed above and below the boundary , although the virus content of the top and bottom fractions differed considerably . 
the " liner was therefore divided at the boundary and the deposits removed and separately resuspended in 0 - 01 m buffer at ph 7 - 2 ( dband dt )  . 
per cent crystalline trypsin was added to each , the suspensions incubated at room temperature for 40 minutes and the virus re - deposited ( a , iii ) ( sb , st - supernatants and dbj , dt , - deposits )  . 
fresh tumour tissue was disintegrated with 10 volumes of 0 - 005 m phosphate buffer at ph 7 - 2 containing 1 : 10 , 000 hcn - but without hyaluronidase - and the suspension clarified ( a , i )  . 
88. the " liner " was removed and the total deposit ( d . , ) resuspended in 375 ml . 0 - 005 m phosphate buffer at ph 7 - 5 to 8 - 0 containing a few mg . 
harris constant standard could be obtained or that the subsequent comparison would be unaffected by such factors as the season of the year or the nature of the medium in which the virus was suspended . 
the first group ( " limiting dilution " methods ) had , also , the advantage of giving some degree of absolute measure corresponding to the actual number of tumour - producing particles . two injection routines have been favoured by prev - ious workers ; either the intradermal or the intramuscular . 
the former allows several different dilutions to be tested in the same bird , but accurate localization of the injection is rendered difficult by the paper - thin structure of the avian skin . moreover , the frequent occurrence of resistant fowls necessitates replication of the tests . intramuscular injections involve a more readily standardized reaction site , but 6 - week - old birds frequently show a variable and unpredictable resistance to the virus . such resistant birds may not react to 1000 times the virus dose which will produce tumours in susceptible birds , and if the end - point , ( m.i.d. ) is dependent , as may be shown , upon a poisson distribution of virus particles , then a large number of 6 - week - old fowls would be required for an accurate assay . it is inconvenient to use large numbers of birds of this age for a single assay and for such reasons the use of embryos or of day - old chicks , which may readily be obtained in large numbers , was investigated . 
the survivors are killed and examined at 28 - days . sudden deaths in the young birds as a result of the " haemorrhagic disease " described by milford and duranreynals ( 1943 ) did not occur when the inoculum was given into the leg muscle . irregular results were obtained in the assay when the . 
harris trypsin ( which removes more than 60 per cent of the non - virus proteins ) gives a product containing only 2 per cent of the nitrogen of the clarified tumour extracts , but possessing almost ar the virus activity . 
a biological assay method using very young chicks has beerr developed . these chicks are found to be more sensitive to the virus than older birds and are obviously more convenient to handle and maintain . the authors wish to express their thanks to professor a . 
the number of cockerels was too in all examinations consmall to admit a proper comparison between sexes . cerning weight , ratio of cortex : medulla and cholesterol content , however , the examined cockerel adrenals did not differ from the female ones . 
each group in the following , control as well as lymphomatosis groups , thus included one to three cockerels . elliot and tuckett ( 1906 ) found no positive correlation between adrenal weight and body weight in adult birds , and our figures support their observations . if the normal birds are equally divided according to body weight into one light and one heavy group , the former had on the contrary some higher mean adrenal weight . 
the gland weights are therefore given in absolute figures . about half of each examined group was composed of white leghorn birds , while the other half consisted of rhode island reds , barred plymouth rocks and crossbreds . 
as was stated concerning sexes , this material did not indicate still , if such differences exist , which may very well differences between breeds . be demonstrated with bigger breed groups , their effect ought to have been fairly eliminated in this investigation by similar breed distribution within the compared groups of birds . control birds as well as lymphomatosis birds were collected during the same seasons - autumn and winter . 
in order to reduce the error produced by the uneven distribution of the cortex within the gland , part of the gland periphery was thus always made part of the picture . the picture was then enlarged to an area of about 300 cm.2 the total area , with the fibrous capsule and notable vessels excluded , and the area of the cortex were determined by planimetry . 
216.833 11273 1 - 61 the difference between gland weights of lymphomatosis birds and normal birds , 63 - 23811 - 334 , is highly significant ( t = 5579 * * * for df = 58 )  . 
the tumour size in neural lymphomatosis is always considerably less than in the visceral variety . the measurements of cortical and medullary areas clearly show that the enlargement is entirely caused by increase of the cortex . 
la than from comparison is in fact decreased . of the means , as two lymphocytosis cases showed exceptionally high cholesterol values and thus brought the mean to a higher level than that characteristic of the majority of cases . 
the impression was that lymphomatosis in a more or less advanced stage is characterised by a big adrenal cortex which in most cases is relatively poorer in cholesterol than normal cortex . the histological examination now and then showed cases of lymphomatosis with considerable disappearance of sudanophil substances but hardly revealed the slight but systematic deprivation as did the chemical determination . as will be shown in a later paper , acutely running experimental lymphoid tumours in chicks ( a transplantable strain of lymphoid tumour derived from a case of spontaneous lymphomatosis ) runs with a still more marked depletion of cholesterol than spontaneous , chronic lymphomatosis as well as with adrenal enlargement . this would correspond with sokoloff 's first stage of adrenal hyperactivity in rous sarcoma . 
he concluded that the second stage was one of hypoactivity and lipoid storage . the results of our investigation indicate , however , that in avian lymphomatosis the second stage is also characterised by hyperactivity . 
a less probable alternative explanation would be that the cortex does not grow as a consequence of increased demand of steroids but because of difficulties in producing theon the contrary , the parallel with selye 's ( 1950 ) general adaptation syndrome with increased adrenal activity first during the alarm reaction and later in the stage of resistance is obvious . 
further , as cortisone fails to produce this effect when it is applied in the " pre - induction " and " induction " phase of carcinogenesis , no support is given to mottram 's hypothesis , that the inducing action of a carcinogen is exerted on a dividing cell . 
the number of cells in mitosis in the cortisone pre - treated animals during the period of " induction " would be few or none and on this hypothesis far less papillomata should have appeared whereas the numbers equalled that of the controls . baserga and shubik ( 1954 ) have obtained essentially siniilar results . 
the findings of green and savigear ( 1951 ) may bear on this point . they showed that after 4 applications of dmb , over 14 days , the epidermal cells of the mouse ear became relatively refractory to the antimitotic action of cortisone given systematically . this was confirmed by an in vitro technique ( green , 1952 )  . it might be expected therefore that chemical carcinogenesis would not be delayed or prevented by cortisone , whereas in fact the present results show that it was . 
a possible explanation of this apparent discrepancy is that the time of appearance of resistance to cortisone depends directly on the rate of mitosis . if this rate is strongly diminished ( by cortisone ) from the outset of carcinogen treatment resistance would then appear much more slowly . 
at the time of its appearing however the treated area of epidermis would be rich in cells in the " induction " phase of carcinogenesis since cortisone does not affect this process . such a mass of cells , after a long exposure to the carcinogen , could be envisaged , when finally they had become completely resistant to cortisone , as emerging as a frank carcinoma . 
doniach. from the pathology department , postgraduate medical school of london , w.12. received for publication february 20 , 1953 . the increasing use of radioactive iodine in clinical medicine has made imperitive the experimental study of its possible carcinogenic action on the thyroid gland . radioactive iodine , like stable iodine , is rapidly concentrated by the thyroid , bound to protein in its colloid in the synthesis of thyroxine , and then gradually released from the gland as part of the normally secreted hormone . during these processes the follicular cells of the thyroid are submitted to a course of ionizing irradiation from the i131 , which gives out f and y rays . 
the duration of this irradiation is of the order of days , since the half - life of 1131 is 8 days and the effective half - life of intrafollicular hormone is also of the order of days in the normal human gland . the carcinogenic activity of ionizing radiations in general has been repeatedly demonstrated during the past 50 years . recently , the effects of ft irradiation from newly developed sources have been studied . raper , henshaw and snider ( 1951 ) reported that single doses of 4000 to 5000 rep ( roentgens equivalent physical ) of f rays from a p32 source induced skin tumours in rats . 
they also found that 13 , 400 rep given in daily exposures of 50 rep over a period of 348 days proved carcinogenic . glucksmann ( 1951 ) found epitheliomas in 4 out of 24 mice in an area of skin exposed 14 months previously to 7900 rep given in 30 seconds by an electron beam . it has proved necessary in the treatment of graves ' disease with radioactive iodine to administer an amount of 1131 calculated to give an overall irradiation to the thyroid gland of 8000 to 10 , 000 rep ( wayne , 1952 ) in order to produce a complete remission of the disease . this dosage lies within the range found to be carcinogenic to other animal tissues . but owing to the uneven distribution of radioactive iodine in the thyroid one cannot make a confident direct comparison , from the dosage point of view , between the animal experiments mentioned above and 1131 therapy of humans . the mechanism of the experimental production of tumours of the thyroid by goitrogens has been greatly clarified by the new zealand team of workers ( purves , griesbach and kennedy , 1951 )  . 
doniach in evaluating the possible danger of carcinogenesis by j131 one must consider not only the direct action of , rays on the cells , but also the indirect action of radiation damage , which leads to diminished thyroxine synthesis and a resultant increased thyrotrophic hormone production . 
a suitable dose of 1131 might therefore lead to a summation of two carcinogenic stimuli ; a short exposure to / 6 irradiation and a long exposure to stimulation by the pituitary . 
the latter could be ensured experimentally by giving a prolonged course of antithyroid drug subsequent to a dose of j131 . doniach ( 1950 ) found that 10 out of 16 rats , given 32 microcuries of 1131 ( 15 , 000 rep to the thyroid ) , developed adenomas . in a series of 5 rats given additional methylthiouracil for 14 months , the thyroids showed a striking increase in adenomas and i - n one instance a metastasizing carcinoma , in contrast to 16 rats tested for the same period with methylthiouracil alone , whose thyroids showed only occasional adenomas . this summating effect of a carcinogen with an antithyroid drug was first demonstrated by bielschowsky ( 1944 , 1045 ) , who used the carcinogen acetamidofluorene combined with allylgoldberg and chaikoff ( 1952 ) have recently reported the development thiourea . of poorly differentiated non - colloid - forming thyroid cancers in 7 out of 25 rats injected 12 to 2 years previously with 400 microcuries of i131 . 
the authors attributed the cancer development entirely to beta irradiation , and not to thyrotrophic hormone stimulation . the object of the experiments described below was to repeat previous investigations of the action of 30 microcuries of j131 alone and combined with methylthiouracil in a larger series of rats , and to compare these results with the effects of 5 and of 100 microcuries . 
the trachea and thyroid attached were fixed in helly 's fluid ; the thyroid was then dissected off and weighed to the nearest milligrathe thyroids were embedded in wax , all glands which weighed 30 mg . 
were secstained by haemalum and eosin . tioned at 6 levels , so arranged as to traverse the whole thickness of the thyroid three sections cut at each level at 5#t were mounted and at regular intervals . one of them stained by haemalum and eosthe spare sections in general were used for extra stains . 
followed 24 hours later by methylthiouracil in the drinking water until the end of the experiment . ( 8 ) 100 lsc 1131 , 30 , uc 1131 , 24 hours later methylthiouracil till end of experiment . 24 hours later methylthiouracil till end of experiment . 
they were taken off the drug for 4 weeks from the 6th to 7th month and were given the i131 in two doses , half at the beginning of the experiment and half 24 hours before commencing their second course of methylthiouracil . in july , 1951 , eight months after this experiment was begun , the thermostat broke down one night and the heating was unfortunately left full on . 
a further 40 rats died or were killed during the course of the experiment , wasted from interfortunately the differences in current infection . the findings between the major groups proved striking even with the reduced number of rats . 
the nuclei were paler than those of neighbouring follicle cells and showed occasional mitoses . the affected follicles had lost their original lining , and had tended to flatten out apart from the altered appearthe normally scalloped perifollicular reticulum . ance of the cells , these " solid " follicles were easily differentiated by serial section from the apparent solid follicles produced by tangential sections of normal ones . they occured both centrally and peripherally in the glands and varied in diameter from 50 to 200 , t . 
to this end , serial sections were examined of the growing thryoids of 5 rats aged .23 days and 5 rats aged 100 days . in none of them were any microadenomas seen . 
nor were there any structures seen resembling these microadenomas in sections of the developing thyroids of 15 - day and 19 - day rat embryos . the incidence of microadenomas in the 9 controls of the main experiment is there were no macroadenomas found similar to those seen in there was a great variation in rats ' and thyroids ' weights . 
the lining cells were about 15 , t tall with a voluminous eosinophilic cytoplasm and capillaries were prominent , and oval vesicular nuclei . did not indent the follicular cells as in the controls . in reticulin preparations the capillaries appeared pushed back by the hypertrophic follicular cells . 
the arrangement of the cells included solid sheets , packed solid trabeculae , closely packed tubules containing pale fluid , microand macrofollicles filled with watery or deeply eosinophilic colloid , and gross cystic follicles distended with colloid and lined by a papillary epitheium . engorged sinusoids were prominent in many of the adenomas . 
the majority , however , presented a closer affinity to those seen in the rats treated with 5 , uc 1131 alone except that the cells were a little taller . their nuclei varied in size and chromatisthe adenomas presented an exaggerated and bewildering variety of cell types and differentiation fundamentally similar to those produced by methylthiouracil alone . 
some of the very large adenomas appeared to be derived from the confluence of more than one tumour . colloid secretion was well marked in many tumours and a papillary arrangement was not rare . 
however , the major part of the bulk of even the large tumours was cellular rather than secretory in origin . solid areas of undifferentiated spheroidal cells were seen within some tumours as with methylthiouracil alone . rat 35b tongues of adenoma tissue were seen penetrating the capsule at one however , in the absence of evidence of permeation of extra - capsular point . veins or obvious morphology of cancer , malignancy was not diagnosed . 
the majority of the follicles appeared active but could be differentiated from those seen in rats treated with methylthiouracil alone , as they were smaller , less regular and showed a tendency to a syncytial arrangement of their lining cells . 
the rats ' weights were similar to those treated by methylthiouracil alone , but the thyroid weights were very considerably reduced to an average size comparable with that of the rats treated with 100 , uc 1131 alone . the pituitaries were similar to those of the rats treated with methylthiouracil alone . 
was injected with the same syringe into a glass vial containing a small pledgelet of cotton - wool . fifteen hours later in vivo measurements were made of the radioactivity of the rats ' thyroids and of the 1 ml . 
19.chart showing the average in vivo count - rates of radioactivity of the thyroid glands of 8 rats following an intraperitoneal injection of 9 - 2 yc 1131 . after 24 hours 4 of the rats ( lowermost curve ) were put on to methylthiouracil in their drinking water . 
the findings in the remaining 4 are charted in the middle curve ; the calculated loss of radio - activity due solely to the radioactive decay of il31 is charted in the uppermost curve . count - rate of standard at 15 hours was 10 , 700 . due to the normal radioactive decay of 1131 . 
the differential effects on these functions of varying doses of 1131 have been recently reported in 3 publications . skanse ( 1948 ) studied the effects of 1 , 10 and 50 , tc i131 on young cockerels primed with a short course of thyrotrophic hormone . 
a definite inhibition of normal thyroid growth was produced by 10 j#c and 50 , uc 1131 after 16 days but not of body growth . all the thyroids showed a growth response to thiouracil , less marked in the chicks given the higher dosages of 1131 . but this response to thiouracil was much more inskanse ( 1948 ) remarks that though hibited after 38 days than after 26 days . the major part of the radiation was received irn the first few days , it took a much longer time to produce the full biological effect on gland function . the calculated dosages of total radiation to the thyroid glands were 1700 rep in the 1 , uc group , 13 , 000 rep in the 10 , tc group and 60 , 000 rep in the 50 1c group . feller , chaikoff , taurog and jones ( 1949 ) studied the effects on adult male rats of single intraperitoneal doses of 24 , 300 and 875 4ac of 1131 . 
the average uptake of 1131 into the thyroids was 40 per cent between 23 and 48 hours after those treated with the two injection and was about equal in all the animals . higher doses showed an abnormally rapid depletion of the iodine that had been trapped during the first 24 to 48 hours . chemical analyses showed an increasing depletion of thyroid 1127 from 2 to 3 days onwards after the injection of the 300 and 875 jtc 1131 , whereas there was no loss after 6 days in animals given 24 1ac . the values of plasma protein bound iodine were not changed in the 24 , uc group but they fell steadily in the rats injected with 300 , uc from 3 - 6 , ug . 
the thyriod uptake in the 1 , uc reached 53 per cent 48 hours after receiving a tracer dose of i131 , but was significantly less in all the other groups . response to subsequent thiouracil was similarly impaired when tested . 
the thyroids of animals which had received 50 and 100 , tc 1131 demonstrated no capacity to increase in weight on a 30 - day course of thiouracil instituted 64 davs after the initial dose of radioactive iodine . even 5 jtc initial t131 impaired the capacity of the thyroid to increase in size ; the 194 i . 
in the animals given an initial dose of 1 iac 1131 . measurements of body weight showed no disturbance in animals which had received up to 20 , uc , a slight impairment in the 50 and 100 , uc groups and a marked disturbance in the 300 , uc group . 
the calculated maximum total irradiation doses delivered to the thyroid in rep were respectively 1800 in the 1 , uc , 5800 in the 5 , uc , 30 , 000 in the 20 , uc , 80 , 000 in the 50 1ac , 197 , 000 in the 100 , tc and 288 , 000 in the 300 / tc groups . effects of internal irradiation by j131 on thyroid histology . findlay and leblond ( 1948 ) studied the thyroid histology of two rats killed 6 days after a single injection of 1131 calculated to have given a total thyroid irradiation of about 20 , 000 rep . the rats had previously been maintained on a low iodine diet . most of the follicles , especially the central ones had lost their colloid , and were replaced by irregularly arranged solid groups of epithelial cells , some of which showed nuclear and cytoplasmic degeneration . interstitial oedema was pronounced , fibrosis and lymphocytic infiltration slight . 
many follicles in the periphery and isthmus were normal autoradiographs showed evidence of accumulation of iodine only in the surviving colloid containing follicles of the periphery . goldberg , chaikoff , lindsay and feller ( 1950 ) studied the progressive changes in the thyroids of adult rats given varied doses of 1131 and killed after intervals of 1 day , 2 days , 3 days , 1 week , 2 weeks , 3 weeks , 1 month , 6 months 875 1 , c ( 330 , 000 rep to gland centre at 72 hours ) produced a total and 8 months . destruction of the thyroids evident within 48 hours , associated with an intense fibrinous oedema and acute inflammatory changes , followed by fibroblastic proliferation and arterial thrombosis . 
by 3 weeks there was a total collagenous permeation of the original gland structure , which by 6 months was replaced by 525 itc produced essentially similar changes . a band of hyalinised collagen . there were , however , at 5 months a few surviving thyroid follicles at the poles , lined by bizarre granular cells thought to resemble the so - called hurthle cells of the human gland . at 8 months surviving thyroid cells appeared more numerous 300 / , tc ( 110 , 000 rep at and formed occasional colloid containing peripheral follicles . 72 hours ) produced extensive swelling and desquamation of thyroid cells within 24 hours , followed during the next 2 days by further degeneration and by interstitial inflammation which appeared resolved by 8 days . at 4 months the glands were lobular and made up of mixed disturbed and normal follicles . at 8 months the glands appeared essentially normal , though the follicle cell nuclei were hyperchromatic and interstitial tissue was increased . 
produced total thyroid cell necrosis in 2 days . following the administration of minimal thyroid - lethal doses , parenchymatous degenerative changes first appeared within a few days in the gland and were followed by an inflammatory picture . intrathyroidal doses of 2 , uc / mg . 
 ( 1952 ) described the histology of the thyroids at varying time intervals after administration to rats of i131 as a part of the study of functional changes quoted above . after 2 days parenchymal degeneration and interstitial inflammation were seen centrally in the 300 , #c group ; no significant changes after 48 days the 300 , #c group showed a virtual were seen in the other groups replacement by fibrous scar tissue . the other groups , including the rats given 1 / uc , all showed hypertrophy of follicle cells and diminution of colloid . 
from 30 , 000 rep upwards there is an increase in rate of loss of organically bound iodine from the thyroid , associated with radiation damage to the follicles . in general , functional disturbances precede histological changes . 
from 5000 rep upwards the thyroid cells are able to respond to activating stimuli by hypertrophy , but hyperplasia proves abnormally limited . bizarre thyroid cells are seen histologically up to 12 years and are accentuated by thiouracil treatment , increasing in number in thyroids submitted to 5800 rep upwards . 
even though irradiated thyroid cells are histologically abnormal , they appear by means of hypertrophy to synthesize enough thyroxine to maintain the animals ' health and growth after dosages up to 30 , 000 rep . calculation of dosage of radiation to the thyroid . calculations of radiation dosage to the thyroid following the administration of radioactive iodine can at the best only be rough estimates because of the con196 i . 
 ( 1949 ) pointed out that since the maximum range of the beta particles enmitted from i131 is comparable to the dimensions of the rat 's thyroid , a geometrical factor must be calculated to estimate the reduction in radiation dose at points near the surface of the gland as compared with the centre . 
by following the uptake of radioactive iodine into the thyroid and its sequential loss from the gland it is possible to estimate the total the conversion factor for rep was calculated by evans ( 1947 ) : radiation dose . 1 , kc per mg . 
the animals were all killed after 15 months and 5 , tc 1131 and methylthe rats on methylthiouracil alone showed no carcinomas . thiouracil led to the production of a greatly increased incidence of adenomas , these findings confirm the additive action of radiobut no definite carcinomas . active iodine in carcinogenesis by antithyroid drugs , and show that the range of 2270 to 16 , 200 rep was more effective than 380 to 2700 rep . in contrast , the methylthiouracil given to rats treated with 100 , tc i131 produced less adenomas this inhibition at a dosage level of 8400 to 60 , 000 than methylthiouracil alone . rep confirms the findings of maloof et al . 
 ( 1952 ) of the greatly diminished capacity adenomas of a similar of heavily irradiated thyroid cells to undergo hyperplasia . morphology to those present in the thyroids of rats treated with antithyroid drugs were found in the animals given 5 , uc and 30 , uc 1131 alone , the latter appearing more effective than the former . 
doniach and pituitaries of this group are significant . there are two points of evidence that a certain amount of thyroxine was being synthetized . firstly , the animals grew from an initial weight of 100 g . , when the radioactive iodine was first administered , to the full weight of 250 to 350 g . , at the end of the experiment . secondly , the pituitaries showed a good coinplement of well granulated alpha cells . purves and griesbach ( 1946 ) demonstrated that the iiaintenance of the alpha granulations is dependent upon a supply of thyroxine ; the pituitary alpha cells disappear after thyroidectomy and are restored by the daily administration of one - fifth or more of the normal thyroxine requirements . nevertheless , the beta cells showed the typical changes of a raised level of thyrotrophic hormone secretion described by griesbach and purves ( 1945 )  . this suggests that the irradiated thyroid glands were secreting at least one - fifth but less than the normal thyroxine requirements . the diminished capacity of the irradiated glands to regenerate prevented a return to quantitatively normal thyroxine synthesis , thus perpetuating an increased thyrotrophic hormone output and accounting for the hypertrophy of the thyroid cells . another possibility to be considered is that irradiated thyroid cells differ from normal in requiring a higher level of thyrotrophic hormone stimulation in order to secrete a normal quantity of thyroxine . similar changes in the thyroids and pituitaries were observed to a lesser extent in the 301 , c 1131 treated rats and to a slight extent in the thyroids only of the 5 , tc i131 group . the bizarre thyroid cell nuclei observed by maloof et al . 
 ( 1952 ) in 1131 treated rats were seen in the present experiment , and were also accentuated in rats treated by additional thiouracil . one cannot say whether the neoplastic cells arise from these or from their apparently normal neighbours . they do , however , constitute evidence of irreversible irradiation changes . 
we do not know the life span of thyroid cells , but it is almost inconceivable that they could survive and function without replacement for15 months , a period of nearly one half the animal 's life span . neoplasms in general arise in tissues made up of actively dividing cells . they do not arise from irreversibly differentiated cells such as neurones or keratinized epidermal cells . the chances of the development of neoplastic thyroid cells following irradiation are likely to vary directly with the number of post irradiation mitoses which take place . this number will be increased in the thyroid bythyrotrophic hormone stimulation . the proportion of cells which become neoplastic is presumably related to the dose of irradiation . the absence of adenomas in the100 , uc 1131 treated group is considered to be due to a lower incidence of dividing cells following irradiation than that which followed in the 30 and 5 1tc groups . adenomas might have been found after afurther 6 months since they were present , albeit in small number , in the 100 , tc treated rats submitted to additional thyrotrophic hormone stimulation by a prolonged course of methylthiouracil . 
one of these was a malignant anaplastic carcinoma transplantable into hosts without thyroxine deficiency . it was not dependent on a high level of thyrotrophic hormone , did not concentrate iodine , grew rapidly , and killed its hosts within a few weeks . the main difference between the action of antithyroid drugs alone and combined with the carcinogen acetamidofluorene is that with the latter treatment thyroid tumours appear considerably earlier and in greater number . bielschowsky ( 1949 ) found also that acetamidofluorene produced thyroid adenomas in the absence of a chemical goitrogen in the regenerating thyroids of subtotally thyroipurves et at . 
 ( 1951 ) have concluded that neoplastic cells arise dectomised rats . spontaneously in the normal rat thyroid and that the carcinogen acetamidofluorene seems to act by speeding up their formation , their further development and growth , however , being dependent upon a high thyrotrophic hormone level . this has been produced experimentally by the prolonged administeration of antithyroid drugs , or by prolonged iodine deficiency ( wegelin , 1927 )  . the results of the previous ( doniach , 1950 ) and the present experiments show that the action of radioactive iodine is comparable with that of the carcinogen acetamidofluorene . in addition , radioactive iodine on its own leads by partial inhibition of thyroxine synthesis to a prolonged rise in thyrotrophic hormone level . 
from the description of goldberg and chaikoff ( 1952 ) , the experimental thyroid carcinomas which resulted from an extremely intense irradiation with radioactive iodine appeared to be of a high grade malignancy . the possibility that a carcinoma of low grade malignancy might become anaplastic must be considered after the findings in the transplantation experiment of purves et al . 
 ( 195 1 ) ; the probability however is unknown . dangers of carcinogenesis to humans treated with j131 . after an exposure to 1800 rep from j131 , maloof et al . 
 ( 1952 ) found a normal thyroid histology in rats 11 years later . but following 5800 rep and upwards , hypertrophied thyroid cells and increasing numbers with abnormal nuclei were seen , accentuated by a short course of methylthiouracil . these cells persisted tracer doses of j131 in clinical medicine fall into the first category , up to 1 1 years . those therapy doses which lower thyroid function below normal into the second . from the experimental findings in rats it would appear that 9000 rep to the thyroid in graves ' disease must act chiefly by functional damage leading to diminished thyroxine production rather than by actual total destruction of the gland . this is borne out by the brief descriptions of chapman and evans ( 1949 ) , williams et al . 
 ( 1949 ) and shapiro ( 1950 ) , who noted no histological evidence of gross destruction in the thyroids of thyrotoxic patients after treatment with radioactive the hyperplastic thyroid of the thiouracil treated rat is not strictly iodine . comparable with the hyperplastic thyroid of thyrotoxicosis . there is certainly as yet no clear - cut evidence that the latter is associated with a high blood level 200 i . 
a raised production of thyrotrophic hormone . the conditions may thus be fulfilled for tumour production , i.e. , an initial radiation damage followed by prolonged thyrotrophic hormone stimulation . one would expect the latent period in humans to be many years , and it is possible that in time thyroxine production and thyrotrophic hormone levels might return to normal and the chances of tumour production be much diminished . this could be ensured by deliberate thyroxine medication . 
on present data therefore the carcinogenic danger of radioactive iodine appears to be the initiation of irreversible radiation damage to the thyroid . this renders a greater number of cells liable to tumour formation when later stimulated by thyrotrophic hormone than in the non - radiated gland . 
a proportion of the resultant tumours are likely to be carcinomas , probably of a low grade malignanoy . anaplastic carcinomas may develop , especially when very destructive doses of i131 are used . the dosage lies within the known carcinogenic range . in view of the experimental findings in rats ( of various strains and in different countries ) , it is probable that the present methods of clinical i131 therapy in thyrotoxicosis may eventually prove carcinogenic . 
the radioactive iodine was found to increase the formation of thyroid adenomas as compared with controls in the 5 and 30 1tc groups but not in the 100 , uc group . out of 20 rats treated with combined 30 , tc 1131 and methylthiouracil 5 developed thyroid carcinomas . 
the radiation dosage range to the thyroid of 2270 - 16 , 200 rep in the latter experiment is likely to include the dosage aimed at , of about 9000 rep , in the treatment of graves ' disease . 
the carcinogenic danger of radioiodine therapy is regarded as due to the production of irreversible cells changes in the thyroid , which render them more liable than normal cells to tumour formation when stimulated to undergo hyperplasia . at the same time , a dosage strong enough to interfere with thyroxine synthesis by radiation damage to the thyroid leads indirectly to a prolonged increased output of thyrotrophic hormone from the pituitary . this constitutes a perpetual stimulus to hyperplasia of the thyroid cells . it is thought that the present dosage of i131 used in the treatment of graves ' disease may eventually prove carcinogenic . i am grateful to drs . 
of 9 : 10 : dimethyl - 1 : 2 - benzanthracene ; specific tumours of the thymus and lung , which are prone to spontaneous tulour developmnent in this strain , were induced by this treatment , whereas the mammary and subcutaneous tissues which are also prone to spontaneous tumour developmnent did not respond . the testis and kidney , in which spontaneous tumours have never been observed , and the spleen , lymph nodes and bone marrow , inl which tumours are not presumed to develop spontaneously , also proved insusceptible to this slight carcinogenic influence , and did not respond to a very powerful direct carcinogeniic influence . 
paraffin of the same batch as that used for analogous experiments performed with 9 : 10 - dimethyl - 1 : 2 - benzanthracene ( engelbreth - holm and rask - nielsen , 1947 ; rask - nielsen , 1948 )  . the technique of application was the same as that used in earlier experiments . 
rask - nielsen zanthracene - induced specific tumours , lymphosarcomatous hyperplasia of the thymic gland in 1i7 per cent , 6.7 per cent , 10 4 per cent and 13 per cent , the effective total being the number of mice whose survival time was at least that of the youngest tumour - bearing animal within all four groups , namely , three months . in addition a thymic spindle - cell sarcoma was found in one animal injected with methylcholanthrene . injections of three of the hydrocarbons into the lung induced thymic tumours in 2 , 2 and 4 per cent following the injection of benzpyrene , dibenzanthracene and 9 : 10 - dimethyl - 1 : 2 - benzanthracene respectively . 
the average latent period , the interval between injection and the death of the animal , following injections into the thymus of benzpyrene , dibenzanthracene , methylcholanthrene , and 9 : 10 - dimethyl - 1 : 2 - benzanthracene was 15 , 14 , 16 and 21 weeks , respectively ; the minimum latent period of the three latter hydrocarbons was 11 , 14 and 10 weeks , respectively . 
analogous negative results were observed by others , using mice from various strains ( esmarch , 1940 ; strong and smith , 1939 )  . experiments including the nho strain of mice , however , exhibit positive results ( strong and smith , 1939 ; strong and williams , 1941 ; strong , 1945 )  . 
from these experiments it is rather difficult to form an estimate of the susceptibility of the mammary tissue to carcinogenic hydrocarbons , since susceptibility is dependent on simultaneous hormonal stimulation as well as on the presence of the milk agent . since the present experinments included only non - breeding mice . 
the hormonal stimulation was at least not maximal . street mice have been used in all the experiments recorded here and the deductions made apply only to mice of that strain . the susceptibility to carcinogenic action of various tissues being genetically determined ( lefevre , 1945 ) it is necessary , in order to elucidate the susceptibility to a direct carcinogenic action of a particular tissue , to examine animals from different strains under identical experinmental conditions . such investigations , for the time being with application of 9 : 10 - dimethyl - 1 : 2 - benzanthracene to the thymus , lung and subcutaneous 116 r . 
moroney. from the leicester general h08pital and the colleges qf technology and commerce , leicester . received for publication juno 3 , 1952 . does chronic g " tric ulcer tend to undergo malignant change ? the importance of this question is beyond doubt , both because of the high incidence of gastric ulcer , and because many patients suffering from it are still treated medically over long periods before reference to a surgeon . 
the answer to it is also of considerable importance to the surgeon , owing to the great difficulty of assessing at laparotomy whether early malignant change may have already if the development of secondary carcinoma supervened on chronic ulceration . is really as common as some pathologists ' figures would appear to indicate , there might be a strong case for an e ' ven more radical gastrectomy than is usually carried out for such lesions . conflicting clinical and pathological evidence . the consensus of opinion in the medical literature is that gastric ulcer is a definite predisposing cause of carcinoma , but there is profound disagreement among pathologists about the percentage of cases ' which undergo such malignant change . 
udaondo ( 1939 ) , in an extensive survey of the world literatu ' re , found estimat - es of the incidence of " ulcer - cancer " which ranged frotn 0 to 100 per obviously , some statistical cent , with most intermediate values represented . uncertainty must be present in the majority of these assessmeints , yet there is usually quite inadequate evidence in the published data to lead to its detection . the only general conclusion that can be drawn from a study of these papers is that the authors ' confidence in the more extraordinary estimates seems to vary inversely with the amount of evidence at their disposal . since , according to the registrar - general 's returns , s ' omething like 14 , 000 people die each year from cancer of the stomach , it is not surprising that the heavy incidence of gastric ulcer in the population should have suggested that there was some connection between the two conditions . 
moroney as regards the stomach , and suggests that the incidence of mahgnant change must be very considerably lower than is suggested by most pathologists ' figures . livingstone and pack ( 1939 ) assess the average survival of patients admitted to hospital with inoperable cancer of the stomach at under 4 months , whilst the total duration of untreated primary gastric carcinoma is often under a year , from the onset of the first chnical symptoms until death supervenes . chronic gastric ulcer , on the other hand , appears to be relatively benign . 
the importance of this is amply justified in view of the gravity of the problem at issue ; particularly so since the ultimate verdict of malignancy must so frequently depend on a but , apart ' from the fact that no two histologists will microscopical opinion . whollv agree on the evidence which justifies such an opinion , the same pathologist not infrequently changes his criteria on reviewing the same series of specimens after a lapse of years . this , of course , is bound to occur as the result of increasing experience ; yet it means that the findings of an individual pathologist over a lengthy series of cases are only likely to be sufficiently homogeneous for statistical purposes if the time i - nvolved in the assessment of his data is not too lengthy , in terms of his tendency to change his pathological criteria . equally , it means that there is grave statistical objection to " averaging " blindly the data of until pathologists in general are able to come to an different pathologists . agreement to assess their findings on common criteria as to what constitutes malignant change in an ulcer and what differentiates this from a cancer arising de novo , each set of figures must be judged independently on internal statistical criteria , 1 4 . 
the only statistical task then remaining would be that of estimating the frequency of its occurrence . but no such agreement on the microscopical findings and their histological interpretation appears probable as ven amongst the most experienced workers . 
on the contrary , the conflicting evidence and extreme variations in the published pathological data make any attempt at mathematical analysis of them futile . as has already been suggested , the chnical evidence of malignant change in pre - existing gastric ulcer is a relative rarity in the collective experience of both thus , as soon as doubts are cast on the infauibility surgeons ' and pathologists . of histological diagnosis , it would seem that the only logical basis for continued belief in " ulcer - cancer " as a comparatively common entity is the analogy of the causative influence of chronic inflammation on subsequent development of carcinoma elsewhere in the body . such arguments by analogy may , however , be most fallacious , and can directly contravene the famous principle first enunciated by william of occam several centuries ago - " entia non sunt multiplicanda praeter nece88itatem . " the importance of this principle in scientific thought , of which it forms one of the main pillars , arises from the fact that it is impossible in practice to prove a universal negative by inductive processes . 
an example will make this clear . our ancestors , influenced by superstition rather than by scientific method , were constantly inventing ad hoc explanations for things in terms of witches , goblins , evil eyes , fairies and leprechauns which the whole weight of philosophy and christianity has not yet succeeded in completely eradicating . 
the survival of such hypotheses is understandable on the grounds that they are easy to conceive , better than no explanation at all and , once accepted , virtually impossible to disprove . 
and then we shall always be countered by the fellow who is positive he saw several the other night such hypotheses are by their very nature invulnerable . in contrast , the opposite scientific hypothesis that the genu8 leprechaun does not exist , except possibly as a freak of natural development in isolated instancesis extremely vulnerable . indisputable evidence of widespread loprechaun activity will entirely refute it , even if no actual leprechaun can be produced for examination . it is essential that this characteristic be present in any scientific hypothesis , so that the collection of sufficient opposition evidence can establish its falsity . adoption o the null hypothesi8 . applying these basic principles to the problem of " ulcer - cancer , " can it be said that this conception has really been adequately demonstrated clinically , 218 a . 
moroney or have we or even that it forms an essential entity in morbid anatomy perhaps accepted its existence with little more justification than our ancestors had in welcoming the leprechaun ? the very phraseology of the relevant literature - " the incidence of ulcer - cancer probably does not exceed x per cent suggests that this ma be the case , and that pathologists are themselves engaged in an attempt to depreciate its frequency of occurrence . it would seem , therefore , that a more profitable approach to the problem will be to attack it from the opposite direction , by the assumption of a " nufl hypothesis "  . in other words , to investigate the situation on the postulate that ulcer and cancer always occur independently in the stomach , in the aetiological sense , and that their occasional intimate association is entirply a matter of pure chance . failing the demonstration of " ulcer - cancer " as a necessary and unmistakable microscopical entity , such a null hypothesis could still be chanenged by statistical evidence that the relative frequency of occurrence of associated ulcer if the frequency and cancer is significantlv areater than the hypothesis predicts . of such associated lesions is so high that it is unlikely to have arisen by chance , the aetiological connection would be estabhshed , but even then this might only indicate that ulcer is a favoured site for the development of a carcinoma destined however , since it is on the relative frequencies of these to arise ' m any case . lesions that the null hypothesis must stand or fall , it is now important to survey the position statistically . 
and this is best carried out ' m general terms in order to avoid errors present in the conflicting pathological figures , and any profitless mathematical resolution of them . in - such an investigation , general figures of cancer incidence are obviously valueless . 
the only data worthy of consideration are thos ' e which have been verified pathologically , and the analysis must therefore be carried from the population at large up to the point where gastric specimens arrive at the patholoin the statistical model of the situation about to be constructed , it is gist . assumed that the specimens eventually arriving at the pathologist are drawn from a population ' whose characteristics with respect to both gastric ulcer and carcinoma may be regarded as stable over a period of time covered by any particular analysis ; and that , by virtue both of its size and its autogenerative properties , the composition of this population remains substantially unaffected by the withdrawal of the specimens . it will also be assumed that u1cer and cancer occur quite independently . development of the statistical model . in the population postulated therewill . 
i with the frequencies stated , the left - hand compartments of the diagrams representing the pyloric zone and the right - hand ones the lesser curvature ; the two lower sections showing the position with respect to the relative frequencies of double lesions occurring in the same region , compared with double lesions which are sited in separate regions of the stomach . 
we shall refer to such double lesions occurring in the same region of the stomacb as " amalgamated lesions " throughout the remainder of this paper , even if they are actually separate . within this limited selection of the whole data evidence might be found of a tendency for co - existing ulcer and cancer lesions to become amalgamated in this sense more frequently thad predicted by the null hypothesis , on wbicb basis the expected value of the ratio of amalgamat - ed lesions to non - amalgamated lesions is seen from fig . 
moroney the developmaint of a cancer , if not an actual aetiolooical factor in its developit will be - seen that this ratio has the statistical advantage that it does ment . not include the imponderable quantities u and c , but depends only on the site it wfll . 
i gives the expected distribution of an cases of if the null hypothesis is true , ulcer and carcinoma into the various categories . we should expect that a randoni collection of pathological specimens from the population at large would agree with the predicted ratios within the linlits of sampling error . but , of course , pathological specimens are not collected at random , and it is therefore essential to consider in some detail the effect of the selection chain along which patients have to pass before their stomachs become pathological specimens . the first group illustrated in the model shown in fig . 
1 , those cases which have neither ulcer nor cancer , will , of course , be entirely missing from the pathologist 's data . is it likely that ulcer of consider next the two categories of simple ulcer . the pyloric canal will have the same probability of pass ' mg along the reference chain to the pathologist as ulcer at the lesser curve ? prepyloric ulcer , in its uncomplicated form , is notoriously difficult to demonstrate radiologicany but , once diagnosed with certainty , is usually operated on without delay , since so many of these lesions prove eventually to have been malignant since their benign ulcers at this site tend to give rise to early symptoms from the onset . secondary pylorospasm which they cause ; yet they are often undetected until pyloric obstruction supervenes later , as the result of gradual stenosis , or unless acute perforation occurs . 
moroney hand , it is more often inoperable at laparotomy , and therefore is less hkely to reach the pathologist as a specimen . there is thus a complex selection mechanism operating along the whole of the reference chain , from the differential symptomatology in the patient through only after all the medical practitioner or consulting physician to the surgeon . this does the stomach become a potential pathological specimen , the likehhood of which is again govemed by the surgeon 's technical skill , and the influence of this on his decision whether to operate and finally to resect . moreover , still other factors may influence this selection of specimens , which will be different for each pathologist . 
the number of patients with gastric ulcer under observation by the medical side of the hospital wif be one of these , for associated " ulcercancer " lesions will have a better chance of being diagnosed early if the chronic ulcer lesions are kept under continual scrutiny by the consultant physician rather than being referred back to their own farnily doctors for routine treatment . further , the alteration in symptomatology resulting from the development of a secondary cancer in these cases is often relatively smah in the early stages . much depends on the vigilance and diagnostic skill of the physician concerned . the almost universal tendency among reporters is to ignore these very important weightings of their figures , and to hope that in the end they win cancel each other out over a large series . comparison of one series with another - or even the first and second part of the same observer 's series - soon demonstrates that this does not happen . 
the fact is that each pathologist 's series must be considered a unique set , not only because of his particular pathological criteria for " ulcer - cancer " but , perhaps even more , because his experience will include a unique set of weights in the data . introduction of the weighting factors . it is now evident that the simple model shown in fig . 
2 appropriate weighting factors have been introduced , which will take unique values for each individual pathologist in accordance with the varying nature of the particular selection chain along which his specimens have passed . 
the group of the population having neither ulcer nor cancer will be completely absent from such specimens and so will have weight zero . this is the only weight that the data of all pathologists will . 
and w6 , are the weightings for referability of associated ulcer and cancer losions in separate compartments of the same stomach - the pathological data for the frequency of wbich is scanty and its clinical recognition difficult . 
moroney if the individual pathologist could be given this ratio of the phcit values . weiahts concerned , and the values for u and c , he could then calculate the expected values for a and d3 , against which the observed values for these ratios in his own series could be tested . the evaluation of u and c from existin - a fi - aures is , however , rendered impossible by the effect of the reference chain and the different criteria adopted for the boundaries of the various stomach zones , nearly all the pubhshed work on stomach pathology conflicting in this respect . minor differences on the latter score between different series - may be partially taken up in the weights w7 and w8 , since all comparisons wif be intemal ones within each set of individual data , but the question is of academic interest only so long as marked reference chain separate independent research , deliberately designed to eliminate effects persist . moreover , the effect of reference chains , would be necessary for their estimation . even if the individual pathologist was supplied with values for u and c , he would still be unable to determine whether his observed values for a and a differed from the null hypothesis expectation for these ratios . 
the ratio w7 is inherently a property of his own series , representing the effect of the reference chain operating in his particular case . it can thorefore only be determined by using his own observed frequencies for u and c and checking them against those established manifestly , he cannot use his own data through such an independent survey . both to establish the expected value of the expressions d2 and d3 , and then to see if his observed values differ from expectation . 
the position , from the point of view of the individual pathologist , is that significant departures in this respect from the null hyporthesis predictions are inextricably confused with the effect of the reference chain ; and the same applies , even mo ' re , to the ratios a2 and a 35 which are under the influence of the reference chain to a greater extent . its implication is that no pathologist , however competent , and no consensus of opinion among pathologists , however widespread , can refute the null hypothesis on the basis of existing figures . it follows inevitably that the solution to this problem of the incidence of cc ulcer - cancer " must await a research project specifically designed to remove the insuperable obstacle facino , the individual pathologist - the effect of the reference chain represented by the weights w in our analysis . 
the results of such an investigation could then be evaluated by means of the ratios al and dl , which only involve the site ' distribution factors u and c . it would be essential for this purpose to establish some sufficiently accurate convention defining the admittedly , these are not boundaries between the various stomach zones . always easy to demarcate in practice , but the contrivance ot ' some effective standard in this respect ought not to present insuperable difficulties . the most hopeful way of establishing reliable values for u and c would appear to be by planned , clinical research at a number of large centres . the assiduous co - operation of all the local general practitioners surrounding these centres would be an essential , so that every case of a suspected stomach lesion reaches them at the earliest possible moment . 
the research would have to be based on several centres , whose respective findings could finally be checked for statistical homogeneity , and these cent - res ought to be carefully select ' ed . 
they should be situated at large - population centres which are growing , to minimise loss of patients during prolonged observation from drift to other areas ; and in provincial towns rather than in very large cities , where it might be difficult to trace their admission to , or treatment at , a large number of alternative hospitals for a gastric emergency or some intercurrent disease . if the establishment of such centres were practicable , it might be possible to eliminate the reference chain weigbts w for all practical purposes , and thus - trrive at reliable values for the site distribution factors u and c . there are , of course , dangers of leakage in the procedure outlined . in addition to the inevitable loss of some patients during the prolonged observation necessary , there is the certainty that some cases would not reach autopsy . moreover , there will be a fraction of the population who will not seek any medical advice until the disease has progressed too far for any statistical value to be elicited regarding the site diagnosis . this is not the place to discuss the details of such an investigation , but the essential problem regarding such losses is not so much their magnitude as whether they are likely to introduce bias in the determination of u and c . .if unbiased estimates of u and c could be ob - tained in this way , the data collected would suffice to test the null hypothesis expectations . cases with single lesions could be used to provide values for these quantities , and thus for the expected values of al and dl , of a high degree of accuracy deriving from the large number of observations on which they would be based . cases with double lesions would then give an adequate check on such results , using the incidence figures of ulcer and cancer in different stomach zones for this purpose in addition to those of amalgamated lesions in the sa - me zone . 
ghadially. from the department of pathology , the univemity of sheffleld . received for publication may 18 , 1951 . havingobserved that regeneration of hair in a clipped area on the back of a rabbit did not occur uniformly over the entire area , and occurred after varying intervals of time in different animals , it was decided to investigate the mode of hence , a band of hair , approximately regeneration of hair on the rabbit trunk . 4 inches wide , completely encircling the trunk , was removed from a few rabbits , and it was observed that the depilated skin was not uniformly pink , but that there were roughly linear bluish - black bilaterally symmetrical zones . besides these major dark zones , there were , in some animals , a few small irregular patches of a similar colour . 
the skin in these dark zones felt thicker than the rest of the after two days , when the animals were inspected , it was found that there skin . was prohfic hair growth in the dark zones , which continued until the hair reached its normal length , but during all this time no hair growth was observed in the pink zones . 
for a further period of 12 weeks with 2 per cent w / w , 9 : 10 - dimethyl - 1 : 2 - benzanthracene in lanohne , which was warmed to melting - point to facihtate apphcation . 
the animals were photographed at the beginning ofthe experiment and on numerous subsequent occasions . skin biopsies were taken at intervals from 3 experimental and 2 control animals . these were fixed in alcoholic bouin and sections were stained with haematoxylin 354 h . 
with the appearance of the papillomata changes began to occur in the surrounding skin ; the hair on the painted side now failed to show the vigorous growth it had shown so far . 
as already stated , by this time the whole of the skin on the painted side had attained a uniform appearance , and no distinction between active and quiescent zones was seen . 
the epidermis was much thicker than either the this change appeared to extend down active or quiescent skin before painting . into the folhcles , which were more prominent and deeply seated and showed the usual arrangement in groups . 
mottram ( 1944a , 1944b ) showed that the skin of mice can be sensitized by painting with croton oil , so that a subsequent single application of 3 : 4 - benzpyrene leads to an abundant production of tumours and a single application of carcinogen followed by repeated applications of croton oil also procluces tumours . 
hence mottram ( 1944b ) concluded that carcinogenesis was composed of three phases : ( 1 ) a " sensitizing factor " which could be brought about by preliminary treatment with croton oil , acting presumably in a non - specific manner by causina hyperplasia , on the supposition that proliferating cells were more responsive than resting cells to the specific ( 2 ) a " specific cellular reaction " induced carcinogenic action which followed . by the specific action ( even of a single application ) of a carcinogen , this representing the essential neoplastic change . ( 3 ) a " developing factor " responsible for the actual appearance of a visible wart , and produced by croton oil of by a carberenblum and shubik ( 1947a , 1947b ) confirmed the latter part of his cilnogen . observations , but found no evidence to suggest that a prelimi - nary croton oil hyperplasia had an augmenting influence on tumour production , which would 356 h . 
the depilated skin showed bila ' terally symmetrical dark zones which showed prolific hair growth within a few days , the rest of the skin remaining 9 : 10 - dimethyl - i : 2 - benzanthracene.in lanoline was painted on the left bald . half of 6 animals ; the remaining 4 were painted with lanoline . 
the following changes were observed : ( 1 ) within 30 days the painted area in the experimental animals became dark and showed prolific hair growth , while on the opposite side there was suppression of hair growth , the skin becoming bald . ( 2 ) in all animals initial papiromata appeared at the site of an originary active zone . 
the first papilloma appeared after 53 days . ( 3 ) after the appearance of papillomata hair growth ceased and zones of activity appeared on the opposite side . ( 4 ) the first carcinoma appeared after 81 days at the site of an originary active zone . it was concluded that ( a ) the naturally occurring zones of increased mitotic activity which continued for some time after the first painting must have acted as a promoting agent ; ( b ) it seems more probable that the tumours arose from hair folfcles , and not the epidermis , as the former are the site of increased mitotic activity during hair growth . it gives us great pleasure to express our thanks to professor h . 
eye hospital , southwark , london . received for publication december 15 , 1950 . in a previous communication ( barker , dhar and parsons , 1949 ) the effects on sarcoma growth in mice produced by treatment with some derivatives of purine and pyrimidine compounds were recorded . further experiments described below have extended the range of pyrimidine compounds studied , and an attempt has been made to correlate molecular structure with biological activity . 
the compounds employed fall into the forowing groups : ( 1 ) cytidyfic acid and alhed compounds . ( 2 ) barbituric acid , its imino derivatives and related compounds . ( 3 ) acyclic analogues of some of the above compounds . pure line or stock mice were grafted with the homologous c57 or the heterologous 837 or crocker sarcomas . 
the technique for treatment was similar to that previously described ( barakan , barker , guband and parsons , 1948 ) , the standard dose ( 0 - 025 g . ) being reclueed in proportion to the toxicity of the particular compound . 
table i summarizes the statistical analysis has shown that the differences in tumour results obtained . weights for treated and untreated grafted mice are significant for groups 2 , 10 , ii and 12 . 
cytosine and uracil , on the other hand , are not utilized in nucleic acid synthesis . this suggested that examination should be made of the action of cytosine when injected into grafted mice . 
the behaviour of 4 - aminouracil appears to be specifically associated with its chemical structure , since the introduction of the sulphur atom at position 2 to give 2 - thio - 4 - amino - 6oxypyrimidine is sufficient to abohsh its inhibitory action . it is considered possible that the marked difference in activity between 4 - aminouracil and 5aminouracil is due to the difference in the electron - availability at the free positions of the two molecules ( positions 4 and 5 respectively ) , which would influence the abihty of the tissues to metabohze the compounds by oxidation . since 4 - aminouracil may also be regarded in its tautomeric form as 4 - iminobarbituric acid , a systematic study was made of barbituric acid and its derivatives , all of which are characterized by high chemical reactivity at position 5 . 
parsons ( 3 ) the 8pecificity of the heterocyclic ring . in the above discussio ' n of the biological act ' ivity of the varl ' ous constituent groups in the pyrimidine derivati - ves the structures were considered only as part of the heterocychc system . in order to determi e whether the ring structure of the compounds is essential to the activities observed three acychc compounds in the first , carbamido - acetamidine , the whole of the structure have been tested . of 4 - aniinouracil is present except for the carbon atom at position 2 . in the second , acetyl urea , the configurations at positions 1 , 2 , 3 and 6 of 4 - aminouracil the third , acetamidine , possesses a similar grouping of atoms to are inaitated . that at position 4 of 4 - aminouracil . 
bartholomew 's hospital , london . received for publication february 3 , 1953 . this investigation was planned at a meeting on august 29 , 1949 , at the baggeridge colliery , staffordshire , ' arranged by a . 
some small series of cases suggest that silicosis may predispose to cancer of the ' lung , but the general indication of the literature is that silicosis is not active in this respect . 
hence the area where there is most pneumokoniosis shows a low incidence of lung cancer . the prevalence of pneumokoniosis in any area is indicated by the number of compensation cases arising under the workmen 's compensation acts and the industrial injuries scheme . 
4. - numbers of deaths from cancer of the lung in coal miners , and of wage - earners on colliery books , from 1921 . 1930 1940 face may be included , but this criterion must be difficult to apply to non - stationary however , in practice , the doubtful cases may not be very numerous , workers . and one must match the entry on the death certificate as nearly as possible with one of the official occupations . the increase in deaths from cancer of the lung . the increase in deaths per annum attributed to cancer of the lung from 1921 to 1950 is shown in tables iii and ix and in fig . 
some possible reasons for these differences are discussed . ( 2 ) in the last 30 years the mortality from cancer of the lung has increased in coal miners in the same way as in the general population ; in view of the peculiarities of the miner 's life , this fact calls for further inquiry . ( 3 ) the incidence of cancer of the lung differs ( a ) in face - workers and in other it is low coal miners , and ( b ) in the various coalfields of england and wales . in the south wales coalfield , where pneumokoniosis is most prevalent . we are indebted to the officers of the national coal board named at the begining of this paper for the suggestions which initiated this inquiry . 
w.7. received for publication august 22 , 1949 . it has been suggested from studies of the action of inhibitors of s - metabolism on tumour induction by carcinogenic hydrocarbons that s - metabolism and the this association is process of carcinogenesis are closely linked ( crabtree , 1947 )  . emphasized when the properties of azo - carcinogens are considered . 
the products of their metabolism have been shown to inhibit the activities of urease ( potter , 1942 ) and succinoxidase ( elson and hoch - ligeti , 1944 ) , two enzymes dependent kensler , dexter and rhoads upon intact sh - groups for their proper functioning . ( 1942 ) studied the relative inhibitory action of a series of " split - products " on a standard diphospho - pyridine - nucleotide system , and sought to correlate this suggestive activity with the carcinogenic power of the parent azo - compound . parallelisms were found , but a clear - cut relationship did not emerge . much of this work has been based on the conception ( experimentally verified for p - dimethylaminoazobenzene by stevenson , dobriner and rhoads ( 1942 ) , and for azo - benzene by elson and warren ( 1944 ) ) that an azo - carcinogen is initially metabolized by the process of reductive fission with the liberation of an amine and a diamine , and that the latter is the effective carcinogen by virtue of its capacity to interfere with normal enzymic . 
a survey of the azo - compounds so far tested for carcinogenic activity makes it evident that in some cases the amine moiety of the reduced molecule plays a significant role in determining potency , e.g. 
on comparing p - dimethylaminoazobenzene with its p ' - methyl derivative , the introduction of the p ' - methyl group causes a change from a very strong to a very weak carcinogen . the present work was undertaken to probe this problem further . isomeric aminoazotoluenes were chosen as suitable for a study of the relative contributions made by the amines and diamines which would arise from their reduction . 3 ' - azotoluene ( o : o ) and the non - carcinogen well - known carcinogen 4 ' - amino - 2 2 ' - amino - 4 : 5 ' - azotoluene ( p : p ) served as bases of reference , and their behaviour was compared with that of the hybrid compounds o : p and p : o . 
water , at room temthe crystalline hydrochloride suspended in etoh perature ( mehner , 1902 )  . was neutralized with ammonia , and an equal volume of boiling water added . the free base was re - crystallized from aqueous etoh . 
the first characteristic abnormalities visible in the livers of rats differed from those commonly observed in the livers of mice , though the final pictures of tumour emergence were similar in both species . building up the general picture four grades of cellular change have been used . in rat livers perilobular necrosis constituted the primary change , and this was followed by regeneration of liver cells in the necrotic areas . in some regions of regeneration microscopic nodules of hepatoma made their appearance , and later these became visible to the eye as dull grey patches on the surface of the lobes . often a simultaneous intense proliferation of bile ducts was manifest in one or more lobes , and the early phases of cholangioma formation would coincide with the development of small hepatomas . 
no metastases were ever found . in mouse livers no preliminary necrosis was observed , but the cellular pattern became abnormal with great irregularity in the disposition and size of the nuclei . further distortion was accompanied by the formation of cells with giant vacuolated nuclei , which preceded the emergence of microscopic hepatomas . 
the fully developed hepatomas of mice were more malignant than those of rats as judged by the degree of atypical growth , though again no metastases were ever found . it will be noted that the earliest histological changes mentioned sometimes occurred in both rats and mice consuming the basal diet without dye - addition . this response of the liver to diets inadequate in several essential food factors may well reflect the basic disturbance of liver function which is a necessary precursor to the carcinogenic action of azo - compounds . ( b ) relative carcinogenic activity of the six isomeric amrnoazotoluene8 . considering the data summarized in table i from the point of view of the relative carcinogenic potency of these isomers , three points emerge : 1 . 
crabtree the possible influence of sex on the growth rate was assessed by keeping the rats of each series separated into three sub - groups containing respectively 10 males , 10 females and 5 males + 5 females . 
2. - growth curves of rats fed on the basal diet , with addition of 0 06 per cent oor p - toluidine . in the work reported here , the two carcinogenic isomers would yield o - toluidine , while 3 of the 4 growth - stimulating isomers would yield p - toluidine as the primary products of reductive fission . the possible effects on growth of these two toluidines were therefore tested . forty - five rats of the 52 strain , each weighing 110 - 130 g . , were divided into three groups of 15 . 
two groups were fed on the basal diet containing 0.06 per cent of either o - toluidine or p - toluidine , and the third group received the basal diet alone . 
each group of 15 rats was subdivided into three separated groups of 5 males , 5 females , and 5 containing males and females . in the latter group two litters were born during the first 3 months , but none subsequently . 
on the other ha ; nd , miller and miller ( 1947 ) emphasize the importance of the protein constitution of the host , and associate the likelihood of tumours developing with the degree to which an azo - compound is " bound " to the proteins of rat livers . in the case of rats consuming p - dimethylaminoazobenzene this fixation is prominent , but does not occur in species resistant to the carcinogenic action of the substance . these differences can only be attributed to the special properties of the proteins characteristic for each species . the " split - product " hypothesis . kirby ( 1945 ) has reviewed the work bearing on this hypothesis of the mechanism of carcinogenesis by azo - compounds , and throws doubt on its validity by citing several examples which fail to conform with its main premises . 
the experiments demonstrated that o : o and o : p were carcinogenic , while p : p and p : o were non - carcinogenic . reviewing these results in the light of the " split - product " hypothesis , no correlation between carcinogenic activity and the potential diamine fission products is found . 
p : p and o : p should yield the same " innocuous " o - toluylene diamine , while o : o and o : p should yield the same " active " .p - toluylene diamine , but the facts are otherwise , since each of these pairs contains one carcinogen and one non - carcinogen . by contrast , when the amine halves of the reduced molecule are considered , the results show that the two isomers which should yield p - toluidine on reductive fission - p : p and p : o - are non - carcinogenic , while the pair yielding o - toluidine in brief , if carcinogenic activity is indeed - o : o and o p - are carcinogenic . a consequence of the action of the " split - products , " it is the amine , and not the diamine , which determines the subsequent biological response . the literature contains several examples of the controlling influence which a methyl group exerts on carcinogenesis , when attached at a para position with miller and baumann ( 1945 ) compared the activities respect to the azo - group . of the o ' , m ' , and p ' methyl derivatives of p - dimethylaminoazobenzene with that of the parent compound . 
the m ' - compound was extremely active ( 7 rats out of 8 bearing liver tumours in 4 months ) , the o ' - compound moderately active ( 4 rats out of 9 bearing tumours in 8 months ) , and the p ' - compound was very weakly carcinogenic ( 1 rat out of 10 with a tumour in 10 months )  . 
nagao ( 1941 ) also found that p ' - methyl - p - dimethylaminoazobenzene was only a weak carcinogen , and that the substances formed by placing a further methyl group in the ring carrying the dimethylamino - group were entirely innocuous . sugiura ( 1948 ) tested a series of derivatives of p - methylaminoazobenzene containing an additional methyl group in the o ' , m ' or p ' positions . the order of potency - m ' > o ' > p ' was similar to that mentioned above . all these observations seem relevant to the present work . 
the common feature is the great loss of tumour - producing activity which results when a methyl group is added in the p ' position to the parent carcinogenic molecule , forming derivatives with the potentiality of liberating p - toluidine on reductive fission . a working hypothesis is put forward tentatively in an attempt to co - ordinate the data outlined above . 
when the structural features and the biological action of these six isomeric azotoluenes are considered , a correlation is evident between their growth - stimulating properties , their lack of carcinogenic power , and the presence of an additional methyl group in the position described . 
crabtree and hilbert ( 1888 ) fed the three isomers of acetotoluidine to dogs . o - acetotoluidine was oxidized to an aminophenol and isolated as methylbenzoxalone , while mand p - acetotoluidines were excreted as acetylated amino - benzoic acids . it may therefore be conjectured that all azo - compounds containing a methyl group at a position para to the azo - group will yield p - aminobenzoic acid as a final product of their metabolic degradation within the rat . the experiment pictured in fig . 
six isomeric aminoazotoluenes have been tested for their carcinogenic activity in the livers of mice and rats , when added at 0 06 per cent concentration to a standard , semi - synthetic diet . 
since the detoxication of p - toluidine can produce p - aminobenzoic acid , the possible relation between folic acid metabolism and the mechanism of cancer induction is considered . i am greatly indebted to e . 
bruzzone. from the department of experimental medicine , national health service of chile , santiago . received for publication june 9 , 1949 . abdominal fibroids induced in the guinea - pig by a - oestradiol ( nelson , 1937 ; lipschutz and iglesias , 1939 ) are prevented when progesterone or other 3 - ketosteroids are administered simultaneously with the oestrogen ( lipschutz and vargas , 1941 ; lipschutz , 1944 ; lipschutz , iglesias , bruzzone , fuenzalida and riesco , 1948 )  . 
as a differerit method of approach , studies are in progress on the antagonisation of the antimitotic action of tetra - sodium 2 - methyl - 1 : 4 - naphthohyd - roquinone diphosphate ( compound 1 ) by nucleotides , nucleosides , purines and pyrimidines and some other compounds ( mitchell , 1950 , 1951 )  . this paper is an account of the cytological effects of a series of 29 selectect 318 j . 
marrian. details of preparations have been published as follows : compounds 11 and iv ( friedmann , marrian and simon - reuss , 1948a ) , compounds xx - xxiii ( friedmann , marrian and simon - reuss , 1948b ) , compounds viii , ix and xxiv ( friedmann , marrian and simon - reuss 1952a )  . we are indebted to f . 
the cytological effects are considered in relation to those of compound 1 . of especial interest from the point of view of the selection of compounds as possible therapeutic radiosensitisers is the appearance of mitotic abnormalities in concentrations which produce mitotic inhibition without gross toxic effects on the resting cells . 
the most important abnormalities studied are chromosome fragmentation , anaphase bridges , metaphase chromosomes with regions of impaired stainabihty and with irregular and beaded structure , metaphases with clumping of the chromosomes , arrested metaphases and other spindle abnormalities , of which many of the types described by barber and callan ( 1943 ) have been noted . 
as already discussed ( mitchell and simonreuss ' 1952 ) , it seems likely that the most relevant cytological abnormalities are chromosome fragmentation , anaphase bridges and chromosome aberrations in examples of the various types of cytological effects observed with this general . series of compounds are show - n in lb ' ig . 
on the basis of the concentration required to procluce 50 per cent mitotic inhibition , hydroquinone diphosphate ( xvi ) is about twice as active as hydroquinone ( xv ) , but the increase of mitotic inhibition with concentration is much more rapid in the case of the former than with the latter . 
somewhat sirnilarly , for 50 per cent mitotic inhibition , phenyl phosphate ( xviii ) is more active than phenol ( xvii ) by a factor of about 20 , but the increase of mitotic inhibition with concentration is much less rapid in the case of phenyl phosphate than for phenol . the only exception so far to the finding of increased antimitotic activity on phosphorylation is in the case of resorcinol . friedmann and simonreuss found that 50 per cent mitotic inhibition is produced by resorcinol at 6 x 10 - 8m concentration but by resoreinol diphosphate at about 5 x 10 - 7m . - kt these concentrations both compounds showed few abnormal mitoses . the usual increase in antimitotic activity on phosphorylation is not associated with any change in character of the cytological effects . 
the frequency of cytological abnormalities appears to be of the same order for the phospborylated and non - phosphorylated compound at concentrations which produce the same mitotic inhibition . ( 2 ) methyl group . the methyl group plays an important part in modifying the biological action , especially from the point of view of practical applications . moreover , among methyl derivatives , the limitations of the use of mitotic inhibition as a sorting test are emphasised . in the chick fibroblast cultures , compound 11 is more active than compound i as a mitotic inhibitor by a factor of about 1000 , and it also shows potentiation of mitotic inhibition in combination with x - rays . however , compound ii appears to be ineffective as a radiosensitiser for the jensen rat sarcoma , and did not produce a focal reaction in the tumour after intravenous injection in a few it may be mentioned that its use in man in high doses may be cases in man . undesirable because of the possibility of induction of cataract , analogous to the experimental naphthalene cataract in rabbits ( boume , 1937 )  . it is of interest to compare the methyl free compound 11 , tetra - sodium 1 : 4 - naphthohydroquinone diphosphate , with the 2 - methyl derivative , compound 1 , and with the 2 : 3 - dimethyl derivative , compound xxviii . 
no other compound examined showed this behaviour . compound 11 showed an increase in the number of metaphases by a factor of about 2 - 5 on increasing the concentration for 50 per cent mitotic inhibition by a factor of io . it bas been show - n in the preceding paper ( mitcher and simon - reuss , 1952 ) that compound i is somewhat unstable in aqileous solution in the absence of oxygen at 39 ' c . 
one may speculate and suggest the possibihty of combination of the phosphates with arginine side cha ' ms of histones the chromosome structure . biological action of 2 : 3 - dimethyl - 1 : 4 - naphthohydroquinone diphosphate , tetrasodium salt ( compound xxviii )  . - the biological action of compound xxviii differs considerably from that of ar the other c ' , ompounds . 
even in concentration 2 x 10 - 6m ( though not at 5 x 10 - 7m ) , which produces no detectable mitotic inhibition , there is metaphase accumulation by about 50 per cent above the fraction of metaphases in the controls , together with spindle abnormalities . as an example of the frequency of relevant chromosome aberrations , it will be seen from table iii that after application in concentration 4 x 10 - 6mfor 24 hours , out of 534 cells in mitosis , there were 74 cells in metaphase showing chromosome fragmentation and 17 anaphase bridges . it appears that with compound xxviii there is more rejoining of chromosome breaks than with moreover , compound xxviii only any of the other compounds examined . starts to show effects on resting cells in high con ' entrations associated with almost complete mitot - ic inhibition ; this behaviour suggests low toxicity . detailed studies of the combination of the effects of compound xxviii and x - radiation on the chick fibroblast cultures have been made by the summation method . 
the results of one experiment are given in table iii . it is concluded that under the experimental conditions , the combination of the action of compound xxviii and of x - radiation shows potentiation of mitotic inhibition and that the mechanism of action of the two agents is different . ( 3 ) carboxyl group . the compound most closely resembling compound xxviii in biological action is compound xi , the hexasodium salt of 1 : 4 - dihydroxy - 2 : 3 - naphthalene dicarboxylic acid diphosphate . replacement of the methyl groups in the 2 and 3 positions in compound xxviii by carboxyl groups slightly reduces the activity as measured by mitotic inhibition and considerably reduces the metaphase effects , so that at 50 per cent mitotic inhibition there is metaphase accumulation by about 25 per cent and sphadle abnormalities are much less frequent . 
compound vi produces clumped metaphases with some chromosome fragmentation and many undivided telophases , but practically no anaphase bridges . metaphase accumulation appears at a concentration which produces about 70 per cent mitotic inhibition ; this is associated with negligible effect on resting ceus . the weak metaphase arrest with compound vi is perhaps associated . 
simon - reuss 5 - methyl - 4 : 7 - thionaphthene quinone ( xxvii ) is active when tested in solution in cerosolve and gum ghatti , and produces 50 per cent rnitotic inhibiti ' on m approximately 5 x 10 - 6m concentration . 
mitotic inhibitor than compound ( xiv ) by a factor of 2 , but produces metaphase accumulation and abnormal mitoses , mainly clumped metaphases , chromosome fragmentation and multipolar cells , at all concentrations showing mitotic inhibition . the tetra - sodium salt of hydroquinone diphosphate ( xvi ) is a very active compound , and produces 50 per cent mitotic inhibition at almost exactly the same concentrat - ion , 3 x 10 - 9m , as does compound il in this region of concentratioin it also produces few abnormal mitoses . 
simon - reuss variably increased by phosphorylation , often by a factor of 5 or more . these results and those with dinitrophenol suggest that blockage of the entry of cells into mitosis depends upon inhibition of synthetic processes mvolving phosit is interesting that from the non - protein moiety of a phosphorylation . phorylase has been isolated a yellow pigment tentatively identified as 2 - methylit seems unlikely that at the concentrations 1 : 4 - naphthoquinone ( buell , 1952 )  . used there is interference with glycolysis ( gemmill , 1949 )  . the comparison of the cytological effects of different compounds of closely related chemical constitution and also of ionising radiations makes it possible to separate some of the main types of mechanism of action of these agents on proliferating cells as follows : ( a ) blockage of the entry of ceus into mitosis , without specification of the exact time of the action and presumably including pre - prophase and antephase this is the characteristic action of compound 1 , and in this case is inhibition . other less clearly associated with relatively few chromosomal abnormalities . defined examples are compounds x and xv . ( b ) metapbase arrest and disturbances of the spindle mechanism apparent - ly examples of this type of action in association similar to the effects of coichicine . with ( a ) are compounds 11 , vi , viii , xi , xxvii and xxx at the higher concentrations , compound ix at low concentrations and compound xxviii iso - naphthazarin produces metaphase over a wide range of concentrations . arrest with little or no inhibition of the entry of cells into mitosis . ( c ) chromosome , including chromatid , brea - kage - with varyina degrees of rejoinability of the broken ends . 
these experiments suggest that the tetra - godium salt of 2 : 3 - dimethyl - 1 : 4naphthohydroquinone diphosphate , compound xxviii , is the most suitable compound for further investigation as a possible therapeutic radiosensitiser . in addition to the help acknowledged in the text , e . 
paper the clinical aspects of androgen therapy in 70 cases of advanced mammary cancer in women are described , the literature surveyed , and the effect of androgens compared with that of castration carried out by surgery and by the prophylactic use of androgens in mammary cancer as x - irradiation . described by prudente ( 1945 ) is not discussed here . the investigation was begun in december , 1947 , and since then sufficient experience has been gained to permit an assessment to be made in general terms of the place of androgens in treatment . 
the pellets were inserted through a skin incision 1 clong in the lower abdominal quadrants , and pushed through radially to rest on the external oblique aponeurosis between 5 and 10 cfrom the incision , the pellets lying at points on a circle with the incision as centre . absorption from these pellets depends on a variety of local factors , including their relation to surrounding fat , adjacent fascia , lymphatic plexuses and encapin three patients who came to autopsy 55 , 82 and sulation by fibrous tissue . 93 days respectively after insertion , the pellets were removed , allowed to dry for 48 hours and weighed . 
per month for their evocation when injections of testosterone propionate are used ( geist , salmon and gaines , 19388 ; geist , salmon and walter , 1940 ) , representing daily doses of nearly double the maximal ( initial ) daily absorption from ten 100 meg . 
were given 3 - 7 times weekly , but later opinion came to advocate larger and larger doses of the order of 100 mg . daily , or even twice daily . the authors of the latest progress report of the council on pharmacy and chemistry ( 1949 ) , however , no longer favour heavy dosage , and consider that there is no advantage in exceeding 150 mg . 
daily for the first 2 - 4 weeks , given . to halve this dose if the patient is responding favourably , or to continue for another all 30 patients who derived month if there is no evidence of specific benefit . benefit from androgen therapy showed clear evidence of it within 8 weeks , and in most cases within the first month . 
no patient who failed to respond after 8 weeks of treatment did so after a longer interval , and it is probably not worth continuing treatment after 10 weeks in the absence of specific response . cannot be said from the small number of cases in this series whether such cases should be transferred to testosterone propionate injections , but the general impression gained has been that patients likely to benefit substantially from androgen therapy are extremnely sensitive to its action , in whichever form it is given , and do as well on doses just large enough to suppress inenstruation in the average premenopausal woman as they do on inuch larger doses . 
on the other hand , most cases which fail to respond to the smaller doses do no better when the dose is increased or the route of administration changed , but the minority which does so led to the tendency already mentioned to advocate heavy dosage . patients given methyltestosterone were advised to leave the tablets ( 50 mig . ) under the tongue , and to allow them to dissolve without chewing or swallowing . the time taken for solution varied between 10 and 30 minutes in different individuals , and a few patients disliked the bitter taste of the substance . duration of treatment in cases responding favourably . no definite recommendation can be given with regard to the length of time cutler and schlemenson , reporting 19 cases , administration should be continued . advised continuing injections until palliation was no longer being obtained the american council already referred to ( cutler and schlemenson , 1948 )  . found that the most favourable results were obtained when injections were conin this series it has frequently tinued until a total of 3 0 g . 
methyltestosterone daily , commenced 6 months after the second implantation and continued for a further 4 months . widespread evidence of fresh activity of the carcinoma then appeared , accompanied by recurrence of pain testosterone propionate injections 100 mg . 
as far as the effect on menstruation is concerned , it may therefore be said that the hormone absorbed from 50 mg . sublingual methyltestosterone is less potent than 10 mg . 
testosterone ( table marked facial hirsuties was present in the second of these cases at the ii )  . time of death , 12 weeks after implantation , not more than 250 mg . 
amenorrhoea persisted for weight gain , 4 months , and weight gain continued during the same period . and subjective benefit , occurred without other side - effects in patients who were it therefore appears that the given methyltestosterone in 40 mg . 
in the first month are bilitated patients is very striking . common , and with the other " tonic " effects are independent of the specific effect in case 65 for example 7 lb . 
in the second 4 months . clinical oedema , however , was seen in only 3 cases , and was always slight in in a few of the amount , and confined to the ankles and lower half of the legs . patients with post - mastectomy oedema of the arm , an increase in the swelling of the arm followed testosterone administration , but this was more closely related to spread of the disease than to the treatment , for when lesions regressed , the lymphoedema sometimes diminished , even when rapid increase in weight was during the initial period of weight gain , some of the occurring , as in case 44 . patients stated that they passed less water , but no measurements have been carried out . much of the initial rapid weight gain is due to the effects of electrolyte , and particularly sodium retention , which holds equivalent quantities of water in the body . this effect is a feature of the activity of many steroid hormones , notably progesterone , oestradiol , and of kendall 's compounds desoxycorticosterone , e and f . 
daily for 6 months and 1 year respectively . they were abundant across the back , and were also present on the cheeks and chin . the skin , which was heavily infected , had the lumpy appearance typical of adolescent pustular acne . in case 44 hirsuties was nminimal , consisting of a sparse growth of soft hairs on either side of the upper lip , but was much more developed in case 63 . in 7 cases facial hirsuties reached an extreme degree , the sides of the face being covered with thick downy hair between 1 and 2 clong ( cases 7 , 9 , 24 , 25 , 56 , 63 )  . in cases 9 and 56 , after 6 months ' treatment the hairs increased in calibre , and resembled the stiff bristles of the male beard . there was some variation in the changes in the scalp hair . 
when fully developed they form a characteristic syndrome , which has been observed in 3 patients in this series . it was first seen when 2 patients ( cases 10 and 45 ) were given 80 mg . 
testosterone. in case 10 , after taking the tablets for 2 days , the patient complained of extreme weakness , drowsiness , severe headache , nausea , and increase in the dyspnoea which was her initial complaint , and due to pulmonary and pleural metastases . 
the symptoms subsided rapidly after she stopped taking the tablets . in case 45 the patient took the tablets for 5 days , during the last 3 of which she felt generally ill , nauseated , and complained of increase in the severity of her backache . 
on the 5th day she was distressed by vomiting , abdominal distension and pain , and took no more tablets , after which her condition improved rapidly . one week later she again attempted to take the tablets , but with exactly the same result . case 30 was a woman of 45 who had been previously treated for 2 years by repeated doses of x - rays for widespread skeletal recurrences for a stage iv carcinoma , and had had induction of an d . 
daily for one month , towards the end of which she complained of increase in the severity of her pains , dizziness , nausea and vomiting , and general malaise . 
the symptoms abated within a day or two of discontinuing the drug . she was asked to resume the tablets a fortnight later , but the symptoms recurred after one week . case 47 , doses of 35 mg . 
by a " moderate success " is meant a case in which symptomatic relief was short - lived ( mostly less than 6 months ) , or not accompanied by considerable objective evidence of regression or by restoration of function . all other cases are classed as failures , even when non - specific benefit was marked and increased the patients ' range of activity . 
testosterone propionate three times weekly without benefit after 6 weeks . she is classed as a " moderate success " in view the remaining patients obtained less benefit , and 3 were of the initial response . never able to leave their beds , although all volunteered that their pains were improved . one of these declared that she had not felt so well nor had so little pain for 2 years , 20 months of which had been spent in bed . case 66 was a woman of 44 years with extensive metastasis to the spine which was responsible for gross collapse of the bodies of dorsal vertebrae 7 - 11 . had been unable to walk or stand for 6 weeks owing to severe proprioceptive loss in both legs , a short course of radiotherapy having conferred no benefit . 
a mild paraplegia was present , and there was some impairment of sensation to light touch , deep pressure and pinprick from the level of the umbilicus downwards . there was , in addition , a girdle of almost.complete anaesthesia to touch and pinprick over the distribution of dorsal segments 7 - 10 . curiously , sensation over the paravertebral regions of these segments was normal . there was no hyperalgesic zone , and no disturbance of sphincter control . the patient was given 28 daily injections of 100 mg . 
two other patients with dyspnoea as one in cases 3 , 10 , 24 of several symptoms obtained some relief after treatment . and 63 the rapidity with which the breathing improved was astonishing , and colnparable with the speedy relief of bone pain in the cases mentioned above . in case 25 , however , with dyspnoea at rest , no significant improvement had ten oz . 
galton with a conjugate defect of elevation , thought to indicate a lesion in the anterior this lesion could have been of vascular origin , part of the oculomotor nucleus . or might have been due to a metastasis . that the latter was the more likely is suggested by the development 6 months later of diminished sensation to touch this patient took methyland pinprick over the right trigeminal distribution . testosterone 50 - 100 mg . 
daily thereafter , also showed marked regression of axillary and supraclavicular lymph nodes , though some of these were still just palpable 4 months later . this patient relapsed 11 months later . case 35 was a stage iv growth in a woman of 36 years . she had nodes in both axillae . 
one year previously she had been given radiotherapy to the primary growth and to the axilla , and 6 months previously had been given pelvic five months later she was given irradiation for induction of the menopause . * methyltestosterone sublingually 80 nig . 
31 premenopausal cases with bone deposits . of the 31 cases , 3 received palliative radiotherapy to the affected bones ( cases 2 , 27 , 69 ) and are not included in the figures . 
of the remainder , 8 were premenopausal cases , all but 2 of whom received great benefit from androgen therapy . three of these were the bedridden patients referred to above , who were able to resume their normal activities within a few weeks of being treated with testosterone , and remained in good health for over 1 year in 2 cases ( cases 3 , 7 , 37 )  . 
the fourth was a housewife of 45 with extensive spinal , costal and pelvic deposits , whose activities were drastically curtailed by pain . she also secured complete relief from pain in the month after methyltestosterone therapy was d . 
galton begun and is well 6 months later ( case 26 )  . case 4 was a nulliparous woman of 49 complaining of pain in the left hip and right shoulder , the latter exacerbated by the smallest movements of the arm , active or passive . 
no deposits were seen radiologically to account for the hip pain , but the medial end of the right clavicle was swollen and tender , expanded by a tumour measuring 4 x 6 cm . after taking methyltestosterone 50 mg . 
daily for one month , the complete range of shoulder movements was restored , the patient was without pain , and the bony swelling no longer tender to percussion , this latter finding being a characteristic result of the treatment . six months later the swelling is slightly smaller , but intrathoracic metastases have appeared and the general condition has deteriorated . of the 3 remaining premenopausal cases , 1 ( case 47 ) , a para - 2 aged 38 , attended hospital 9 months after radical mastectomy with severe anaemia and pains in back , hips and shoulders . she was intolerant to doses of methyltestosterone greater than 30 mg . , and although the dose was increased in 5 mg . 
on 3 occasions the treatment had to be abandoned each time , owing to the sudden onset of headache , nausea , fever , drowsiness and increased intensity of the pains . these symptoms subsided within a day or two on withholding the hormone . case 66 , who presented with paraplegia of 6 weeks ' duration , has been referred to above . 
the last premenopausal case ( case 10 ) , a para - l aged 45 , had had a right radical mastectomy 2 years previously for a lump in the breast present for 1 year . she attended hospital with cough , dyspnoea , pain in the chest and stiff neck . 
methyltestosterone arising in submammary lymph nodes . daily , and in 3 months ' time was walking well and without pain . in addition surprisingly she the parasternal swelling had become greatly reduced in size . showed on examination 3 - 5 cof shortening of the right femur , but no impairment of movement about the hip - joint , within the limits imposed by the rigidity of her paralysis agitans , and the x - ray revealed an unusual subcapital fracture of the neck with downward and backward displacement of the capital fragment . the second case was of a nullipara aged 51 , who had been recurrence - free for 10 years after a radical mastectomy , when she developed backache , which persisted , increased in severity , eventually confining her to bed . multiple deposits of secondary carcinoma filled most of the dorsal and lumbar vertebrae , and all the pelvic bones . within a few days of the implantation of 500 mg . 
testosterone the pain abated , walking was quickly resumed , and she is pain - free 14 months later without further treatment . the nature of the pain is therefore open to question , but the patient gave no history of previous chronic backache , the onset of the pain coincided with the finding of multiple secondary deposits in ' the appropriate bones , and relief promptly followed implantation of a very small dose of testosterone . testosterone was also given to 5 young patients in whom an artificial menoin the first and last pause had been earlier induced ( cases 5 , 30 , 50 , 62 and 70 )  . of these cases pain was relieved , but in the first it was never severe , and in the last its recurrence followed the appearance of further metastases . the difference in response by premenopausal and postmenopausal cases just mentioned was not met with in the series of 70 cases described by adair , mellors , farrow , woodard , escher and urban ( 1949 ) , or in the larger series of 285 cases analysed by the council on pharmacy and chemistry ( 1949 )  . in adair 's series 9 out of 48 cases with skeletal metastases benefited from androgen therapy , but no difference in response was noted in premenopausal and postmenopausal cases ( 12 of the 48 cases were premenopausal , compared with 8 out of 28 in the present in the council 's series of 285 cases , the ages ranging from 25 - 79 years , series )  . favourable effects were evidently independent of age . 
no explanation is offered for this discrepancy . post - treatment changes in bone . it is difficult to account for the rapid relief of skeletal pain brought about by equally striking is the speedy disappearance of tenderness to testosterone . percussion of affected bones , and the later diminution in size of bony swellings radiologically all that can be observed are the due to subperiosteal deposits . changes in position and concentration of minerals in the neighbourhood of a deposit following testosterone administration , but these changes are characthey consist in the homogeneous deposition of minerals in the bone teristic . surrounding the deposit , so that at first the deposits acquire a more definite outline , and may appear more extensive in size and number . this is a common appearance 2 months after commencing treatment , but soon gives way to a more uniform but rather structureless appearance , as the areas of decalcification in the deposits become filled in from the periphery with deposited minerals . after 6 months this process usually comes to a standstill . it is questionable whether this confers increased strength on the bones in which it recalcification d . 
the same is true of cases with bone deposits , and in the illustrations in the first two papers just cited fresh osteolytic deposits are present in bones showing extensive recalcification round earlier deposits . several instances of this phenomenon have been met with in the present series . the paradox is probably to be explained by the fact that the metabolic processes accelerated by the androgen proceed most rapidly at the beginning of treatment , and then slow down to a stationary though raised level . 
he had learned of " the custom in certain countries to remove the ovaries of the cow after calving if it is wished to keep up the supply of milk , and that if this is done the cow will go on giving milk indefinitely , " and this " pointed to one organ holding the control over the secretion of another and separate organ , and thus explained the absence of that distinct nervous control that i pointed out as characteristic of the mamina . " beatson 's first case will be described in some detail , as it illustrates very well the kind of result that may be obtained by testosterone therapy as well as by castration . the patient was a married woman of 33 years , with 2 children , in fair general health , and menstruating regularly . three years previously she had noticed a lump in the breast while suckling her first child . this increased in size after the birth of her second child 20 months later . 
when first seen there was a mass 5 x 3 inches with ulceration of the skin of the breast over an area of 1 square inch and adjacent skin nodules . radical mastectomy was performed on 25 . 
95 , but 3 months later an ulcerated recurrence in the scar was found , and a fortnight later had increased in size to 21 x 31 inches . the whole chest wall was studded with skin nodules , but no lymph nodes were felt . 
95 the " largest area of disease " measured 1i x 2 inches . eight months later regression continued . the patient lived until april , 1899 , dying 46 months after castration , with fresh recurrences in skin and spine ( thomson , 1902 )  . seconid case was that of a woman aged 40 , with massive involvement of the whole breast by carcinoma , with extensive infiltration of skin , axillary and cervical nodes as far as the chin ; the opposite cervical nodes were also involved , and she complained of pain in neck and arm . after castration the pain was relieved , and regression and softening of the primary mass and of the nodes occurred , lasting 5 months . thus in the first 2 cases in which castration was used , shrinkage of the primary growth , regression of skin deposits and of involved nodes , general improvement , and relief of pain were described . six years later the method had been used extensively , and its value sunmmed up by beatson ( morris , 1902 ) as follows : " it is not easy to say beforehand if the operation will do good ; but from the cases recently published by abbe , of new york ( thomson , 1902 ; abbe , 1901 ) , it would seem that it is not contra - indicated after the menopause th ' value of an operation may be judged by statistics and by personal impressions . both may be deceptive , though both may contain in them the germs of truth . i believe that from both standpoints the evidence is in favour of the utility of oophorectomy in certain cases , in prolonging life and lessening pain . it has never , as far as i know , done any harm , and its mortality has been nil the treatment has been placed before the profession , because i felt that d . 
galton they should judge its effects themselves and if , in their opinion , after a fair trial , it is found wanting , then i hope it will be abandoned and forgotten . " oophorectomy passed out of fashion a few years later , and was slowly superseded by " x - ray castration , " and in the last 10 years by " medical castration " with androgens also . boyd ( 1900 ) reported the results of oophorectomy in 54 cases of mammary cancer . six cases out of 46 showed remissions lasting for 2 years or more , and 17 out of 46 derived some benefit , but in most of these , recurrences occurred between 6 and 12 months later . with one exception the treatment failed in all the patients who had passed the menopause , and the maximum benefit seemed to be derived by women over 40 and still menstruating . 
two years later thomson ( 1902 ) of edinburgh collected and published the results in 80 inoperable cases castrated by several surgeons . in 40 of the cases some imnprovement took place , although this was negligible in 11 , and only temporary in 11 others ( under 12 months ' survival following oophorectomy )  . 
in 18 , however , decided improvement was recorded , " remarkable " in 4 . thirteen cases survived more than 20 months , and 4 between 40 and 46 months . of the 29 more favourable cases , 6 had ceased menstruating , and 3 were 70 years of age , and of the 20 women still menstruating , 12 were between 40 and 50 years of age . 
thomson concluded that the value of castration , though limited , had been established beyond doubt , but , like beatson ( 1896 ) , stressed the unpredictability of the results . 
jessett " had operated on 5 cases , and admlitted that the patients complained of less pain , but in no single case was there any improvenment in the local disease . 
he also noted that beneficial results occurred sometimes after the menopause . bruce clarke recorded a case in which castration was followed within 6 weeks by rapid subsidence of pain and regression of a chest wall recurrence , the patient being in good health 5 years later . in this case unfortunately the age was not stated , but the original excision of the growth was performed 2 years before castration , and a recurrence excised 1 year before ( lett , 1905 )  . in spite of the well - documented reports described above , castration for mammary cancer fell out of favour , no doubt because of the absence of precise indications , the large number of poor results and the increasing success obtained by local radiotherapy . morris ( 1902 ) stressed the difficulty of assessing the results , and compared " beatson 's treatment " with the favourable results claimed for the injection of coley 's fluid ( heat killed broth cultures of streptococci obtained from erysipelas lesions , and of bacillus prodigiosus ) in cases of spindlecelled sarcoma . 
he found that in the cancer - bearing group the incidence of complete oophorectomy before carcinoma was diagnosed was 1.5 per cent , whereas in the non - cancer group it was 15 - 4 per cent , or ten times as great . these figures implied that castration might have protected a small number of women from the subsequent development of mammary carcinoma . arguing on these lines horsley , late in 1937 , performed bilateral oophorectomy on the first of a series of patients immediately after radical mastectomy , in the hope of deferring the onset of recurrence . 
by june , 1944 , recurrences had occurred in only 4 out of the 25 patients who had been observed for between 9 months and nearly 7 years . horsley felt that the appearance of metastases had been delayed by castration ( horsley , 1944 , 1945 )  . snapper castrated 22 patients after radical mastectomy , and in addition treated them for 3 months with injections of testosterone propionate 25 mg . 
of methyltestosterone was given on the day after oophorectomy , but in view of subsequent experience with this hormone , it is probable that the immediate effect was due to the oophorectomy alone . a case of intrathoracic recurrence in a woman of 40 years , 2 years after radical mastectomy for stage ii carcinoma , in whom relief of dyspnoea was observed 4 days after castration , and during the next 2 months absorption of nialignant pleural effusion and resolution of pulmonary parenchymal deposits took place , was reported by jochweds , baranowicz and horecki ( 1948 )  . the effects of surgical castration may be summarized by saying that it confers definite benefit on a small percentage of cases of carcinoma of the breast , even in an advanced stage , as shown by relief of severe bone pain , recalcification of areas of destroyed bone , regression of primary and secondary manifestations of disease , and conspicuous improvement in general health lasting uisually for several months only , but sometimes for several years . 
the most favourable cases are those in the premenopausal group in women , though striking improvement occasionally follows castration in older women , and in the small number of cases reported in males the best results are to be expected in elderly patients . in passing it should be noted that some of the remarkable spontaneous regressions which occur , and which may resemble in all respects those already described , are probably the result of " self - castration , " both ovaries being completely destroyed by metastases . 
ahlbom 1920 , and described his ( 1930 ) attempted a statistical analysis of his cases , but as 147 out of 163 cases received treatment to other sites as well as to the pelvis , and his series included very few instances of women in the most favourable age group , he failed very few clinical data are presented in to demonstrate any positive effects . ahlbom 's paper , and in spite of his obvious anxiety to attain statistical precision , it is perhaps surprising that he could quote no examples of undoubted success similar to those reported so often in cases subjected to surgical castration . 
clarkson and barker ( 1936 ) reported a case of mammary carcinoma in a woman of 41 with axillary node involvement , and deposits in a metacarpal , a tarsal phalanx , femur and ilium , in which recalcification of destroyed areas in the skeleton the patient was in followed ovarian irradiation and general body irradiation . good health 5 years later ; the ovarian irradiation was considered to be the main cause of the good result . dresser ( 1936 ) reported the results of ovarian irradiation in 59 cases with skeletal metastases , having selected this group for special observation because of the dramatic benefit conferred on two women with generalized skeletal and other deposits after they had received small doses ( 700 r ) of x - ravs directed to in both cases the periods ceased , general the pelvis for local relief of pain . regression of deposits occurred , with skeletal recalcification , and in the second case multiple pulmonary deposits disappeared ; the patient led an active life for of dresser 's 59 cases , 30 were under another 3 years , largely symptom - free . 45 years of age , and 29 had passed the menopause . 
the discrepancy between the results of the early surgical cases , in which castration was believed to be contra - indicated in the presence of bone metastasis , and the more recent results in which skeletal metastasis is regarded as one of the most favourable indications for ovarian irradiation , is probably adequately explained by the lack of satisfactory x - rays in the early work , so that the extent and incidence of bone metastasis was less accurately known . the effects of androgens in mammary carcinoma . among the first reports of the use of testosterone for mammary carcinoma were those of ulrich ( 1939a , b ) and of loeser ( 1941 )  . the latter used intramuscular injections and also subcutaneous implants of testosterone propionate . the first 3 cases were recurrence free at the time treatment was begun , but remained so for the next 3 to 4 years , whereas all had been treated by x - rays or surgery for recurrences shortly after the original operation ( 6 months , 8 months and 2 years respectively )  . farrow and woodard ( 1942 ) felt that there was a specially close relation between susceptibility to skeletal metastasis and ovarian activity , and were thus led to use testosterone for cases with bone deposits . 
doses gilven on alternate days . the case reports published by adair and herrmann ( 1946 ) illustrate very well the kind of result which may follow the use of testosterone therapy . weight gains , general improvement , rapid relief of pain previously intractable , regression of primary growths and secondary deposits , and increased calcification of bony deposits were recorded . the following are especially noteworthy : ( 1 ) the ages of the patients . - one of the best responses occurred in a woman of 63 years , though the other successes were in women of 47 , 44 and 42 years compare also taylor , slaughter , smejkal , fowler and preston ( 1948 ) , of age . who report andillustrate regression of pulmonary deposits in a woman of 70 , and the progress report of the american council on pharmacy and chemistry ( council on pharmacy and chemistry , 1949 ) , in which the response to androgens in 285 patients ranging from 25 - 79 years was evidently independent of age . in a later paper adair ( 1947 ) reports a dramatic result in a woman of 71 who had been confined to bed for 10 months with severe pain and pathological fractures due to widespread metastases in spine , pelvis and ribs . three weeks after commencing testosterone therapy she remarked on her improved sense of well being , and 4 weeks later left her bed . 
two years and 4 months after she was still up and about and in good health , the only untoward effect being irritation from the enlarged clitoris . this case recalls some of those treated by surgical castration ( thomson , 1902 )  . ( 2 ) the speed of response . - in case 4 relief of pain was evident within1 week of the first injection , and in case 3 regression in primary and metastatic growths was noted one month later . ( 3 ) the favourable effect on skeletal metastases . - the earlier results of adair ( 1947 ) suggested that the best results of androgen therapy were to be expected in cases with metastases in bone . however , equally dramatic results have been obtained in cases with pulmonary deposits and skin deposits , but no secondaries in bone of the common osteolytic type revealed by x - rays . these results are said to be much less common than in cases with bone deposits . thus adair stated : " in only a small percentage of cases is improvement to be anticipated where carcinoma involves soft tissues such as liver , lungs , brain and local skin recurrence . it is true that in a few instances there have been striking improvements where an advanced ulcerating breast cancer with surrounding skin nodules , axillary nodes and neck nodes were involved ; where masses were metastatic to the lungs ; and in one instance where the patient was having convulsions from metastatic disease in the brain receive no benefit  . 
in weight , her periods had not recurred , and the mass in the breast none of the nodes was more than 1 cacross , and the skin was no longer palpable . deposits had undergone complete regression , being visible only as brownish impalpable mottlings . 
48 signs of masculinization had appeared , namely slight hirsuties of chin , and lips , and a deepening of the voice . she complained of slight swelling of the feet her weight was 10 st . 
ii.49 she attended hospital complaining of severe backache , and on examination the nodes felt previously were found to be hard and much enlarged , numerous deposits not exceeding 3 min diameter were present in the skin of the left breast , and the liver edge , which was thickened , firm and somewhat irregular was felt in the right iliac fossa . 
47. - admitted to royal cancer hospital . on examination she was in good general condition , but bedridden with crippling pain . there were 3 ulcerated recurrences along the left mastectomy scar , the two larger measuring 2 x 4 and 5 x 3 crespectively , with irregular thickened raised edges , fixed bases and coarsely nodular floors . 
in 9 months , had recurrence of low back pain ; the mass in the upper inner quadrant of the right breast was larger , as were the axillary nodes ; the bony parasternal swelling in the left 4th interspace had ulcerated through the skin . there were numerous hemispherical bony projections on the vault of the skull , on the frontal bone , on the right clavicle . x - rays showed many fresh osteolytic deposits in spine , ribs and pelvis , side by side with old sclerosed deposits , which were less dense than before . injections of testosterone propionate 100 mg . 
viii.44. - left radical mastectomy for stage i carcinoma of breast . postremained well until april , 1948 , when first noticed breathlessness on effort , which june , 1948 . - signs of large left pleural effusion . 
49 the only abnormality found was slightly diminished radiologically there is now only obliteration of the left expansion at the left base . costophrenic sulcus , and the parenchymal opacities are no longer visible . she was last seen on 25 . 
48 the entire area was paler in colour , the young skin over it thicker , but there was still one small discharging area . this dried up during the next two months , dressings were discarded and therapy discontinued , but on 1 . 
minutes. this degree ' of hydrolysis was found to remove ar non - dna phosphorus as wer as all non - dna adenine from the cells , while leaving dna phosphorus and dna adenine in situ , thus obviating the necessity for the use of the einzyme ribonuclease ( lajtha , 1954b )  . adenine 14c administered to cells appears both as labelled adenine and labelled guanine in the dna ( hamilton , 1953 )  . no attempts to separate labelled adenine from labehed guanine have been made in the experiments ; the activity of the dna has been measured as a whole . the autoradiographs were exposed for 10 - 14 days . 
ar autoradiographs belonging to the same experiment were coated with the same batch of stripping film , exposed the same length of time at the same temperature ( 3 - 4 ' c . ) , and developed in one batch of developer simultaneously , and , finally , were stained simul368 l . 
on each slide 100 - 200 nuclei were counted , and grains were counted over - 5 - 10 showing the strongest autoradiographs . this was to obtain the values for the maximum degree of dna synthesis and was done after surveying repeated counts at different times were performed to tes - t the over 500 nuclei . reprodiicibihty of the counts , and it was found that with the above technique the same observer showed ain error not greater than 10 - 15 per cent . for the calculations on the quantity of isotope i ' ricorporated into the cell , it was assumed ( 1 ) that the geometry of the autoradiographs was such that only 50 per cent of the electrons emitted frothe disintegrations reached the photograpbic emulsion , and ( 2 ) that the 32p electrons produced 0 - 7 grains per incident electron , and the 14c electrons 2 gfai - ns per incident electron ( lamerton , 1950 )  . if the exposure tiine and the half life of the isotope in question as well as the grain count per nueleus and the grain yield per electron of the isotope are known , then the number of the atoms of the isotope withiii the nucleus can be calculated . the technique is sensitive enough to detect 20 - 30 32p atoms per cen . because of the very long half - hfe of 14c ( and because exposure times were limited to the relatively short period of 14 - 30 days ) the minimum necessary number of 14c atoms per nucleus to show an autoradiograph is of the order of 106 . in preliminary experiments the maximum dna 32p uptake per nucleus was found to be the order of 600 atoms ( > i 00 grains in 14 days ' exposure 07 grains / electron )  . 
the labelling obtained in vitro of the dna is therefore of the order of i : 3 x 107 . if the cehs cannot differentiate between 31p and 32p then the total phosphorus pool available for the cens must also have been labered in the ratio of the order of i : 3 x 107 . thus for 5 , ac . 
in seruthe addition of adeniine 14c into the culture medium does not represent the labelling of a pool , but the provision of adenine to the cers which would otherwise have to synthesise it . 
the marked ability of the cellsto take up adenine from the cultur - e medium is shown by the fact that the average maximum uptake per nucleus was of the order of 1 - 2 x 107 atoms dna 14c ( 50 grains in 10 , days ' expostire , 2 grains / electron )  . 
i ' he cell cycle . if the cells svnthesised dna throughout the entire intermitotic period , then , after a few hours of culture in the presence of the isotope all the cers should contain labelled dna . 
ellis fore the cells within a hours of the end of the period of dna synthesis at the start of the culture in isotope wif not be labered , and , similarly , cers enterina the period of dna synthesis during the culture time ( t ) and spending less than a hours 11111hours fig . 
the length of the s period is also indicat - ed by the gradual increase of the grain count / nuclei up to about 15 hours , then reaching the maximum average value for a given concentration of the isotope in the culture mediuthe length of the total cen cycle can also be calculated in a different way . 
3 illustrates the timing this timing , in of the cell cycle obtained with the methods outhned above . principle agrees well with that found in the bean root by howard and pelc ( 1951 )  . it can be seen from tables i and ii and fig . 
the reason for this difference is , firstly the differences betweein eilergy of the beta particles emitted by 14c and the higher energy32p electrons result in a greater scatter and , consequently , in a higher background , thus interfering with the accuracy of the c ' secondly , while the half hfe of 14c is a neghgible problem when the isotope dilutions are added to the culture medium , variations in volume to allow for the decay are a also , diie to the decay of 32p and to the fact that32p is so - lirce of error with32p  . supplied in3lpphosphate buffer , the ratioof 31 to 32pwill not be constant : the degree of labelling of the phosphorus pool will be variable . these factors all contribute to the lesser accuracy of the counts in cultures with 32plabelling as compared with the 14c labelling . 25 - 30hours 12 - 15 hours 3 - 4hours g2 m fig . 
rate , of dna synthe , 8i8 in different type8 of bone marrow cei18 . in these experiments only those types of cells were found to synthesise dna which are known to be capable of mitosis . 
3 represents the average values for the majority of the dividing cells of the bone marrow , i.e. , promyelocytes , myelocytes , pronormoblasts , basophihc normoblasts and early polychromatic normoblasts . in a few experiments , however , where it was found to be possible to count early normoblasts and early myeloid cells separately , a shorter cycle than in fig . 
the affect of x - ray irradiation on dna synthesis large doses of x - rays ( 5000 r in 15 minutes , 140 kv , i . / mal filter ) exerted a marked inhibition on dna synthesis . 
14. - post - irradiation dna synthesis . was not a recovery in the sense of ability to synthesise normal amounts of dna , but the entry of some 0 , cers into the s period for a hmited time . it appears that ar 01 cehs are damaged by a dose of 5000 r . the effect of irradiation on theg2 period is indicated by the fa ' ct that no mitoses were observed in any of the irradiated cultures . a dose of 5000 r produced a marked degeneration of the cers in the cultures , but over 6 hour culture times were needed to show the first morphological signs 378 l . 
in a sense this could be better defined , as the assembly of the dna experiments with the synthesis , of the purines and pyrimidines from molecule . labeued one carbon compound precursors ( e.g. , formate 14c ) are in progress . the timing of the cer cycle is , in principle , in good agreement with that it is expected that described in the bean root cell by howard and pelc ( 1951 )  . the timing of the cer cycle in different . 
the total cycle time was found to be of the order of 40 - 48 hours for the average dividing bone marrow cers ( promyelocytes , myelocytes , pronormoblasts , basophihc and polychromatic normoblasts )  . 
bowles , md2 , 3 introduction fibroblast growth factor receptors ( fgfrs ) 1 through 4 are transmembrane tyrosine kinase receptors that play a key role in cell survival , differentiation , migration , angiogenesis , and carcinogenesis.1 uncontrolled activation of fgfr signaling has been described in almost every type of malignancy and typically is the result of amplication or activating mutation affecting the fgfr genes.2 these aberrations can one of function as cancer drivers but also may inuence prognosis and sensitivity to treatment.3 - 5 only two fgfr - specic inhibitors , erdatinib and pemigatinib , have been approved by the us food and drug administration , though a number of multikinase kinase inhibitors ( mkis ) have some degree of fgfr2 inhibiting properties . although fgfr1 and fgfr3 mutations are more frequent overall , activation of fgfr2 is common in patients with endometrial adenocarcinoma , cholangiocarcinoma , gastric adenocarcinoma , and ameloblastoma , a rare and difcult - to - treat odontogenic tumor.2 , 6 - 9 here , we present the case of a patient with ameloblastoma harboring an activating fgfr2 y375c mutation who had signicant tumor regression in response to treatment with lenvatinib . 
a specimen from a repeated biopsy was sent for nextgeneration sequencing using cancerselect 125 ( personal genome diagnostics , baltimore , md )  . analysis revealed clonal fgfr2 y375c , an activating mutation in the transmembrane domain causing constitutive receptor dimerization through the formation of intermolecular disulde bonds.12 although fgfr2 aberrations are common in ameloblastoma , this point mutation appears not to have been identied previously . 
first characterized in bearestevenson cutis gyrate syndrome , y375c is rare in cancers but has been described in adenoid cystic carcinoma and endometrial carcinoma.13 , 14 a second potential driver mutation affecting the hedgehog signaling pathway , smo l412f , was also found at a lower allele fraction . 
frequently seen in ameloblastoma as well as basal cell carcinoma , medulloblastoma , and a subset of meningiomas , this activating mutation alters the drug - binding pocket of smo , conferring resistance to smo inhibitors such as vismodegib and itraconazole.6 a third mutation , palb2 h786y , was reported but is of unclear signicance , having never been associated with human disease . 
although sensitivity to fgfr inhibition varies by type of mutation , drug - binding site , and degree of fgfr specicity , 15 , 16 cancer cell lines harboring fgfr2 y375c mutations were previously found to be responsive to nonselective pan - fgfr inhibition in vitro.17 because the fgfr - specic inhibitors were not yet commercially available , lenvatinib was selected because of its favorable half maximal inhibitory concentration for fgfr2 ( 27 nmol / l ) and efcacy in other malignancies . the patient started receiving the standard dose for radioactive - iodine refractory thyroid cancer of 24 mg daily . his dose was reduced to 20 mg daily after 1 month , then 20 mg alternating with 10 mg daily after an additional month . 
he experienced typical adverse effects of grade 2 hypertension , grade 2 hypothyroidism , grade 1 diarrhea , and grade 2 weight loss . on follow - up imaging at 6 months , he experienced a partial response with 40% shrinkage , per recist , version 1.1 ( fig 1 )  . 
as of this writing , the patient has been receiving this treatment for 13 months and has a continued partial response . discussion ameloblastoma is a locally invasive , typically benign distransformation with ease that can undergo malignant regional or distant metastasis , sometimes occurring decades after initial presentation.18 - 23 surgery is the mainstay of treatment , although conservative enucleation and curettage are associated with recurrence rates as high as 60% to 90%.24 radical surgery with wide en bloc resection improves these rates but at the cost of disgurement and high morbidity . 
overall , guidance regarding use of adjuvant treatment modalities is lacking . given the dearth of effective and tolerable treatment options , reports of targetable mutations dominating the genetic landscape of ameloblastoma were met with great interest.6 - 8 a large percentage of ameloblastomas , especially those arising from the mandible , have braf v600e mutation . 
ameloblastomas harboring braf v600e mutation are sensitive to braf inhibition in vitro at clinically relevant drug concentrations.6 multiple case reports have demonstrated durable clinical response to braf inhibition or combined braf / mek inhibition , on the basis of braf status.26 - 30 a second , and typically mutually exclusive , molecular phenotype featured mutations in fgfr2 , including c382r and v395d in the transmembrane domain and n549k in the kinase domatogether , braf and fgfr2 mutations are present in approximately 80% of ameloblastomas , with additional somatic mutations in smo , cttnb1 , pik3ca , and smarcb1 . interestingly , the patient we report on here had nearly 90% allele frequency of fgfr2 y375c , suggesting this may have been the initial truncal mutation . 
the implications of clonality for fgfr point mutations and fusions are not well understood , but truncal amplication of fgfr2 is an important predictor of drug response in gastric cancer.31 in a small trial of the selective fgfr inhibitor azd4547 in fgfr2 - amplied gastroesophageal cancer , robust , singleagent clinical response was restricted to high copy - number amplication events with associated high expression of fgfr2 mrna and fgfr2 protethe mechanism for this fig 1 . 
 case report effect was thought to be transactivation of alternate receptor tyrosine kinases resulting in a distinct oncogene addiction phenotype characterized by fgfr - dependent phosphatidylinositol - 3 - kinase and mammalian target of rapamycin signaling . although prospective trials in ameloblastoma continue to insight into be limited by low case numbers , additional treatment of this disease may be drawn from other , molecularly similar cancer types , including endometrial and gastric adenocarcinomas . 
fgfr2 mutations occur in approximately 10% of both tumor types and are mutually exclusive , with kras mutations suggesting a shared signaling mechanism.9 , 32 , 33 in vitro data from endometrial cancer conrmed fgfr2 activation results in increased mapk signaling that is abrogated by fgfr inhibition.34 , 35 these preclinical data prompted a phase ii trial of lenvatinib in advanced endometrial cancer , which reported an objective response rate of 14% and a clinical benet rate of 37% without selection for fgfr status.36 conrmatory trials of fgfr inhibition in endometrial cancer , both alone and in combination with pembrolizumab or other checkpoint blockade , are ongoing.37 subgroup analysis of biomarkerselected populations in studies like these may be a helpful surrogate for utility in rare cancers such as ameloblastoma . complicating the generalization of fgfr inhibitor trial data are the multiple mechanisms of fgfr dysregulation . 
although studies typically lump together patients with any fgfr aberration , the type of mutationfgfr overexpression including gene amplication , increased ligandbinding afnity or ligand expression , or ligand - independent receptor activationresults in differential effects on fgfr signaling . 
using mkis as an example , brivanib primarily affects cells with fgfr1 amplication , dovitinib inhibits fgfr1 - 3 kinase activity in a predominately liganddependent fashion , and ponatinib targets fgfr1 - 4 with three patterns of signaling alteration we have described.17 although the exibility of some nonselective mkis in targeting multiple fgfr aberrations may broaden their use , it comes at the cost of increased toxicity . 
in contrast , early data from selective fgfr tkis demonstrated a favorable adverse effect prole but more limited efcacy.38 , 39 characterizing drug - susceptibility phenotypes will be crucial for the continued development of these agents and other approaches to fgfr inhibition , including monoclonal antibody or peptide inhibitors and fgf ligand traps . although lenvatinib was chosen in this case to target fgfr2 , it is possible the patients response was due to inhibition of other targets , such as vascular endothelial growth factor receptors , platelet - derived growth factors , or kit . 
assessment of phosphorylated - fgfr2 by immunohistochemistry before and after therapy could clarify if his response was due to on - target or off - target effects , but he declined a repeated biopsy procedure . 
lenvatinib has been effective in thyroid , renal , and hepatocellular carcinomas without identiable mutation or overexpression of these kinases , suggesting the mechanism underlying drug sensitivity is incompletely understood.37 most clinical trials of lenvatinib have been in solid tumor types selected on the basis of response to other inhibitors of angiogenesis , but these agents have not been investigated in ameloblastoma . more studies are needed to clarify the role of fgf signaling in drug response and identify predictive biomarkers for lenvatinib . 
clin cancer res 22 : 259 - 267 , 2016 donnem t , al - shibli k , al - saad s , et al : prognostic impact of broblast growth factor 2 in non - small cell lung cancer : coexpression with vegfr - 3 and pdgf - b predicts poor survival . 
j thorac oncol 4 : 578 - 585 , 2009 turner n , pearson a , sharpe r , et al : fgfr1 amplication drives endocrine therapy resistance and is a therapeutic target in breast cancer . 
ware ke , hinz tk , kleczko e , et al : a mechanism of resistance to getinib mediated by cellular reprogramming and the acquisition of an fgf2 - fgfr1 autocrine growth loop . 
nat genet 46 : 722 - 725 , 2014 [ erratum : nat genet 47 : 97 , 2015 ] kurppa kj , cat on j , morgan pr , et al : high frequency of braf v600e mutations in ameloblastoma . 
j pathol 232 : 492 - 498 , 2014 brown na , rolland d , mchugh jb , et al : activating fgfr2 - ras - braf mutations in ameloblastoma . 
clin cancer res 20 : 5517 - 5526 , 2014 dienstmann r , rodon j , prat a , et al : genomic aberrations in the fgfr pathway : opportunities for targeted therapies in solid tumors . 
byron sa , chen h , wortmann a , et al : the n550k / h mutations in fgfr2 confer differential resistance to pd173074 , dovitinib , and ponatinib atp - competitive 17 . 
gozgit jm , wong mj , moran l , et al : ponatinib ( ap24534 ) , a multitargeted pan - fgfr inhibitor with activity in multiple fgfr - amplied or mutated cancer 18 . 
brunet m , khalifa e , italiano a : enabling precision medicine for rare head and neck tumors : the example of braf / mek targeting in patients with metastatic 27 . 
faden dl , algazi a : durable treatment of ameloblastoma with single agent brafi re : clinical and radiographic response with combined braf - targeted therapy in stage 4 ameloblastoma . 
byron sa , gartside m powell ma , et al : fgfr2 point mutations in 466 endometrioid endometrial tumors : relationship with msi , kras , pik3ca , ctnnb1 mutations and clinicopathological features . 
plos one 7 : e30801 , 2012 [ erratum : plos one 7 , 2012 doi : 10.1371 / annotation / 0bfaecca - 0f87 - 43fe - 97ccf2ae3ddeb6d5 ] 33 . 
konecny ge , kolarova t , obrien na , et al : activity of the broblast growth factor receptor inhibitors dovitinib ( tki258 ) and nvp - bgj398 in human endometrial cancer cells . 
chae yk , ranganath k , hammerman ps , et al : inhibition of the broblast growth factor receptor ( fgfr ) pathway : the current landscape and barriers to clinical application . 
 o accurate rna sequencing from formalin - fixed cancer tissue to represent high - quality transcriptome from frozen tissue purpose accurate transcriptional sequencing ( rna - seq ) from formalin - fixed paraffin embedded ( ffpe ) tumor samples presents an important challenge for translational research and diagnostic development . 
we evaluated the accuracy of rna - seq data generated from ffpe samples in terms of expression profiling . methods we designed a biospecimen study to directly compare gene expression results from different protocols to prepare libraries for rna - seq from human breast cancer tissues , with randomization to fresh frozen ( ff ) or ffpe conditions . 
the protocols were compared using multiple computational methods to assess alignment of reads to a reference genome , the uniformity and continuity of coverage , the variance and correlation of overall gene expression , patterns of measuring coding sequence , phenotypic patterns of gene expression , and measurements from representative multigene signatures . results the principal determinant of variance in gene expression was use of exon capture probes , followed by the conditions of preservation ( ff v ffpe ) and phenotypic differences between breast cancers . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction although it is generally best to identify gene expression biomarkers from cancer tissues using the highest quality of rna purified from fresh frozen ( ff ) samples , any subsequent development toward diagnostic testing will require translation for use with formalin - fixed paraffin - embedded ( ffpe ) tissue samples . 
however , the variably fragmented and chemically modified rna derived from ffpe samples presents a challenge for accurate measurement of gene expression.1 , 2 in a different context , there is great interest to perform transcriptome sequencing ( rna - seq ) for biomarker discovery research using large cohorts of precious archival ffpe samples from completed clinical trials . 
different approaches to generating libraries for rna - seq include selection of mrna by targeting the poly ( a ) tail ( mrna protocol ) , depletion of more abundant ribosomal rna ( rrna depletion ) using jialu li chunxiao fu terence p . 
 a 80c freezer ( ff ) or 10% neutral buffered formalin and paraffin - embedded as an ffpe tissue block.10 phenotypically , the nine breast cancers were defined by the pathologic status of hormone receptors ( hrs ) and human epidermal growth factor receptor 2 ( her2 ) as hr - positive / her2 - negative in five , hr - positive / her2 positive in one , and triple receptor - negative in three . 
a dnase - i treatment step was included in both . construction of rna - seq library and sequencing full details of all methods for library construction and sequencing of rna samples are in the data supplement . 
an overview diagram of the different rna - seq library protocols is shown in figure 1 , and details of the number of libraries prepared , starting rna requirement , cost , and duration to perform each protocol are summarized in the data supplement . the mrna protocol ( ff only ) used oligo - dt beads for poly ( a ) + mrna enrichment , followed by standard procedures of truseq rna sample prep kit v2 ( illumina , san diego , ca )  . 
then the rrna - depleted srna was used as the template for the mrna protocol described above . the cr protocol was performed using truseq access rnaseq kit ( illumina ) , using random primers . 
no technical replicates could share the same sequencing lane . rna - seq data analysis full details of all data analysis methods and an overview diagram of the analysis plan are provided in the data supplement . 
scatter plot of the first three principal components for count per millionnormalized and variance stabilizing transformed counts of 20 , 381 coding region ( cr ) - targeted poly ( a ) + genes . 
the rnaseq data generated from the srna protocol had a significantly lower concordant pair alignment rate as compared with those from non - srna protocols ( p < .001 ; data supplement )  . 
using the cr protocol , mapping was highly concordant between ff and ffpe and the exonic mapping rate was increased compared with non - cr methods ( data supplement )  . 
overall , the number of genes with read coverage ( transcripts per million [ tpm ] > 0.1 ) was slightly higher in ffpe samples than in ff samples for both non - cr and cr protocols ( data supplement ) .12 uniformity and continuity of read coverage of transcripts uniformity of read coverage was measured by the mean coefficient of variation , and continuity of coverage as the percentage of gaps without read coverage , across the top 1 , 000 highly expressed transcripts ( data supplement )  . 
 principal component analysis of expression of a total of 20 , 381 cr protocol targeted poly ( a ) + genes for all libraries showed that the 26.5% of total variation captured by the first principal component was due to use of exon capture probes ( cr protocol ) , and 20.6% from the second and third components due to the combined effects of ffpe and biologic differences ( fig 2 )  . 
hierarchical clustering results , with high confidence ( average bootstrap probability , 0.93 ) , showed that the major tumor phenotypes ( hr - positive v hr - negative ) and the source tumor clustered together with ffpe samples ( data supplement )  . 
comparing ff and ffpe samples using the same totalrna protocol , the log ratio values were still centered around zero at different mean expression levels ( fig 3b )  . 
difference in measurements as log ratio ( m ) versus mean average expression ( a ) of each gene ( ma plot ) of 20 , 381 coding region ( cr ) targeted poly ( a ) + genes for tumor sample c when using ff.k.totalrna sample c library as the reference . 
m is the log2 - transformed expression of a gene from first library divided by that from the second library , and a is the mean log2 transformed expression of the gene . 
generally , the cr protocol tended to overly enrich the highly expressed genes and was more likely to not capture low expressed genes ( fig 3c ; data supplement )  . 
this was not improved by prior demodification of methylol adducts from ffpe tissuederived rna using heat and amines or the srna protocol ( fig 4 ; data supplement )  . 
although both approaches seemed to slightly increase concordance of expression , neither was statistically significant . after further investigating these protocol induced biases , we calculated the number of genes that would be considered as differentially expressed or false positives compared with each reference ff standard protocol ( data supplement )  . 
cr , coding region protocol ; dem , demodification ; ff , fresh frozen ; ffpe , formalin - fixed paraffin - embedded ; srna , sense rna protocol . and triple receptornegative breast cancers within each protocol . 
the p value from de analysis followed the ideal uniform distribution for non - de genes , with a spike close to zero for the de genes ( data supplement )  . 
 principal component analyses demonstrated the following order of variables influencing gene expression measurements from rna - sequencing : whether the library preparation protocol used exon capture for cr , whether the sample was from ff tissue or ffpe tissue , and the biologic phenotype of the breast cancer based on hrs and her2 receptor status ( fig 2 )  . 
nevertheless , we identified one protocol , ffpe.k.totalrna , with consistently good transcript coverage uniformity and continuity , most concordant expression , and least differential expression when compared with the different non - cr protocols with fresh tissue . 
it had a reasonable requirement of total rna input ( 100 ng ) for ffpe biopsy samples . the first translational research scenario that we posed , in the introduction section , considered the best pairing of protocols that would enable discovery using ff samples with intention to later translate for use with ffpe samples . 
this interpretation was supported by the quality of read coverage , pattern of coding sequence expression , and translation of overall or phenotype - related gene expression profiles and prognostic signatures . the cr protocols yielded concordant results , but different from all other ( non - cr ) protocols . 
 also , changes to the population of exon capture probes within a commercial kit over time could be a potential risk to this approach . the most generalizable results for discovery research from ffpe samples were obtained using the total.rna protocols without exon capture . 
for our second scenario , therefore , we prefer the k.totalrna protocol for best representation of the transcriptome in ffpe samples used for discovery researchaiming to represent the transcriptional information that ff samples would have provided . our third translational research scenario involves the translation of an existing gene expression signature that was previously developed using a different method ( eg , microarray ) or a particular rna - seq protocol . 
the inclusion of random and dt primers and the t7 promoter region ( srna protocol ) to simulate the ff.mrna protocol produced good concordance overall but introduced a high number of nonconcordant mapped reads , nonuniformity , and discontinuity of read coverage across the transcriptome . limitations to our study include small sample size ( although cancers were selected to represent biologic diversity ) ; optimally short time to fixation of tissues and possibly , as a result , a modest degree of degradation of ffpe samples ( dv200 ranges from 65% to 85% ) ; optimal amount of input rna used for non - cr protocols ( at least 100 ng ) ; and lack of generalizability ( single institution conditions of tissue processing )  . 
one tumor ( sample n ) seems to be compromised by unknown technical processing ; our study conclusions , whenever involving this sample , are based on robust point estimates ( eg , median estimates in fig 4 ) across all samples to avoid being driven by its outlier effect . 
for more information about asco 's conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . jialu li stock and other ownership interests : genomic health chunxiao fu no relationship to disclose terence p . 
fraser symmans stock and other ownership interests : ionis pharmaceuticals , nuvera biosciences , delphi diagnostics consulting or advisory role : genentech patents , royalties , other intellectual property : patent pending for gene expression measurement of sensitivity to endocrine therapy travel , accommodations , expenses : luminex supported by the cancer prevention research institute of texas grant no . 
masuda n , ohnishi t , kawamoto s , et al : analysis of chemical modification of rna from formalin - fixed samples and optimization of molecular biology applications for such samples . 
fumagalli d , blanchet - cohen a , brown d , et al : transfer of clinically relevant gene expression signatures in breast cancer : from affymetrix microarray to illumina rna - sequencing technology . 
zhao w , he x , hoadley ka , et al : comparison of rna - seq by poly ( a ) capture , ribosomal rna depletion , and dna microarray for expression profiling . 
loi s , haibe - kains b , majjaj s , et al : pik3ca mutations associated with gene signature of low mtorc1 signaling and better outcomes in estrogen receptor - positive breast cancer . 
the patient declined surgery , and the centrally located rll tumor was treated with stereotactic body radiation therapy ( sbrt ) at a dose of 50 gy in five fractions . 
 six months later , the patient presented with a 3 - month history of right hip and left shoulder pain , which was a biopsy - proven recurrence of the rll primary with diffuse bony metastases . 
 the patient consented to an institutional review boardapproved protocol ( #226210 at the university of california , davis )  . tumor and germline genomic sequencing assays plasma ctdna was isolated from 10 ml of whole blood drawn in streck cell - free dna tubes , enriched by hybrid capture to target exons of 70 genes and critical introns of six genes , and sequenced to an average depth of approximately 15 , 000 on an illumina nextseq500 ( guardant360 assay ; guardant health , redwood , ca ) at a clinical laboratory improvement actcertified commercial laboratory.6 germline dna was isolated from the patients pbmcs and enriched for targeted regions using a hybridization - based protocol and was sequenced with 50 or greater depth using illumina technology at a commercial genetic testing laboratory ( invitae , san francisco , ca )  . 
 methods for in vitro studies are described in detail in the data supplement . this patients family history suggests a hereditary predisposition to lung cancer : three other individuals across three generations had a history of lung cancer ( data supplement )  . 
tumor genomic profiling of plasma ctdna with the guardant360 assay identified concurrent low ( 0.3% ) mutation allelic frequency ( maf ) of egfr l858r and high ( 51% ) maf of egfr t790m ( fig 1a - 1b )  . 
 the patient was referred to a genetic counselor , and germline dna sequencing confirmed that this patient carried a germline egfr t790m mutation . we determined the in vitro cytotoxicity of egfr tkis on this patients pbmcs using a permanent epstein barr virustransformed lymphoblastoid cell line , a good surrogate for the patients germline genomic materials , 11 , 12 established before initiation of any systemic treatment . 
we found that the lymphoblastoid cells ( fig 2a ) and the patients pbmcs ( fig 2b ) were resistant to all first - , second - , and third - generation egfr tkis tested . 
consistent with previous reports , 13 h3255 cells ( which harbored only an oncogenic egfr l858r mutation ) were sensitive to all egfr tkis ( fig 2c ) , whereas h1975 cells ( which harbored both oncogenic egfr l858r and t790m mutations ) were resistant to erlotinib but sensitive to afatinib and osimertinib ( fig 2d )  . 
we found that the patients pbmcs and pbmc - derived cells did not express egfr and akt protein , the two key signaling molecules that mediate the downstream oncogenic signaling pathways in h3255 and h1975 cells , by western blots ( fig 2e )  . 
we also confirmed that there was no egfr mrna expression in patients pbmcs or in the patient - derived ebv - transformed lymphoblastoid cell line ( data supplement )  . 
thus , afatinib and osimertinib could be used safely in this patient with a germline egfr t790 mutation . during the in vitro studies , the patient first received palliative radiation for the right hip pa he had stable disease after first - line combination chemotherapy with carboplatin , pemetrexed , and bevacizumab for four cycles , and he experienced tumor progression at the primary rll and metastatic bony lesions after maintenance treatment with pemetrexed and bevacizumab for four cycles . 
a restaging positron emission tomography ( pet ) / ct scan 2 months after afatinib treatment began revealed extensive tumor progression in the primary rll tumor and multiple bone metastases . 
serial guardant360 assays revealed that the changes in the maf of egfr l858r in plasma ctdna correlated with the tumor responses to chemotherapy , afatinib , and osimertinib ; the maf of egfr t790m remained at approximately 50% ( fig 1a - 1b )  . 
time points ( ie , dates ) were selected on the basis of radiographic assessments at baseline and after each treatment according to recist version 1.1 during the entire disease course . 
targeted ngs of malignant cells in pleural effusion by foundationone ( foundation medicine , cambridge , ma ) revealed multiple genomic alterations , including egfr l858r and t790m ( fig 1c )  . 
similar to plasma ctdna analysis , egfr genotyping of the patients tumor dna by droplet digital polymerase chain reaction revealed that the maf of egfr l858r in tumor dna increased with tumor progression , whereas the maf of egfr t790m remained at approximately 60% ( fig 1c )  . 
the patient did not tolerate subsequent treatment on a clinical trial and died on hospice approximately 3 months later . discussion routine clinical application of multiplex tumor genomic profiling has increased the detection rate of rare germline mutations that may affect the patients clinical care and that raise concerns for cancer risks in family carriers.15 , 16 the maf of a somatic mutation in the plasma ctdna is usually much lower than that of archived tumor dna , whereas the maf of germline egfr t790m remains at 50% to 60% in plasma ctdna and tumor dna . 
results from the inherit study ( nct01754025 ) , which provided free genetic counseling and tested for lung cancer in patients and family members with an egfr t790m mutation at diagnosis and at longitudinal surveillance with serial ct scans , 17 are highly anticipated . patients with lung cancer who have a germline egfr t790m usually harbor a distinct spectrum of one or more concurrent oncogenic egfr mutations ( data supplement )  . 
the median progression - free survival was 4.9 months in the pooled analysis of patients ( the data supplement ) , whereas the median progression - free survival was 9 to 13 months in patients with egfr tkisensitive somatic egfr mutations.18 furthermore , data from our patient and the patients in the data supplement also revealed less clinical benefit from chemotherapy and radiation , which suggests tumor resistance to these standard therapeutic strategies . 
stollenwerk , tianhong li provision of study material or patients : debbie lewis , yanhong zhang , jamie hung , jenna welborn , tianhong li data analysis and interpretation : weijie ma , jidong shan , wenwu xiao , yanhong zhang , sixi wei , kit s . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . weijie ma no relationship to disclose jay gong no relationship to disclose jidong shan no relationship to disclose debbie lewis no relationship to disclose wenwu xiao no relationship to disclose elizabeth h . 
moore no relationship to disclose yanhong zhang no relationship to disclose jamie hung no relationship to disclose patents , royalties , other intellectual property : patent for device and method for assessing beam quality in computed tomography by measuring the half - value layer ( inst ) sixi wei no relationship to disclose jeanna welborn no relationship to disclose nicholas s . 
lam leadership : lamnotherapeutics stock and other ownership interests : lamnotherapeutics , lp therapeutics , cardioprobe patents , royalties , other intellectual property : i have more than 20 issued patents , many with the university of california , davis ( no royalty received in the past 2 years )  . tianhong li consulting or advisory role : foundation medicine , takeda , puma research funding : foundation medicine ( inst ) , pfizer ( inst ) , astrazeneca ( inst ) , hengrui ( inst ) acknowledgment we dedicate this work to the late jeannine h . 
mans stock and other ownership interests : concert pharmaceuticals , corcept therapeutics , varex imaging , verasterm , ziopharm oncology affiliations weijie ma , jay gong , wenwu xiao , elizabeth h . 
3 - ( 4 , 5 - dimethylthiazol - 2 - yl ) - 5 - ( 3 - carboxymethoxyphenyl ) - 2 - ( 4 - sulfophenyl ) - 2h - tetrazolium assay for ebv - transformed lymphoblastoid cell line established from ( a ) this patient , ( b ) the patients pbmcs , ( c ) h3255 , and ( d ) h1975 . 
 ( e ) the expression of egfr and downstream signaling molecules in the ebv - transformed lymphoblastoid cells and pbmcs from this patient , h3255 , and h1975 are shown . 
mulloy r , ferrand a , kim y , et al : epidermal growth factor receptor mutants from human lung cancers exhibit enhanced catalytic activity and increased sensitivity to gefitinib . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
ancevski hunter k , friedland dm , villaruz lc , et al : first - line osimertinib in patients with treatment - naive somatic or germline egfr t790m - mutant metastatic nsclc . 
hussain t , kotnis a , sarin r , et al : establishment and characterization of lymphoblastoid cell lines from patients with multiple primary neoplasms in the upper aero - digestive tract & healthy individuals . 
li d , shimamura t , ji h , et al : bronchial and peripheral murine lung carcinomas induced by t790m - l858r mutant egfr respond to hki - 272 and rapamycin combination therapy . 
meric - bernstam f , brusco l , daniels m , et al : incidental germline variants in 1 , 000 advanced cancers on a prospective somatic genomic profiling protocol . 
hu y , alden rs , odegaard ji , et al : discrimination of germline egfr t790m mutations in plasma cell - free dna allows study of prevalence across 31 , 414 cancer patients . 
oxnard gr , heng jc , root ej , et al : initial results of a prospective , multicenter trial to study inherited lung cancer risk associated with germline egfr t790m : inherit egfr . 
kris mg , natale rb , herbst rs , et al : efficacy of gefitinib , an inhibitor of the epidermal growth factor receptor tyrosine kinase , in symptomatic patients with non - small cell lung cancer : a randomized trial . 
 clinical observation of improved outcomes of patients with brca 1 / 2 breast cancer treated with everolimus prior to dna - damaging therapy introduction the mammalian target of rapamycin ( mtor ) pathway comprises mtor complexes 1 and 2 ( mtorc1 / 2 ) and is primarily responsible for maintaining cellular growth and proliferation . 
although it is known to act as a catalyst toward anabolic synthesis , mtorc1 also is responsible for mitigating cellular catabolic processes , namely autophagy.1 mtorc2 complements mtorc1 in anabolic processes.2 phosphoinositide 3 - kinase ( pi3k ) and phosphatase and tensin homolog ( pten ) genetic mutations frequently are found in many tumor types , including breast cancer.3 these genes are important in regulating the downstream activation of the mtor pathway . 
many drugs have been developed to target the mtor pathway , including the mtorc1 inhibitor ( mtori ) everolimus.2 , 4 poly ( adp - ribose ) polymerase ( parp ) is a family of enzymes that repairs damaged dna . 
treatment with a parp inhibitor ( parpi ) prevents dna repair in cancer cells during homologous recombination ( hr ) events in patients with brca1 / 2 mutations , which leads to cell death through synthetic lethality.5 brca1 / 2 germline mutations are found in approximately 5% of unselected breast cancers , with higher prevalence in high - risk cohorts.6 activation of the pi3k / mtor pathway is important in decreasing the effect of brca1 / 2 mutations by stabilizing hr.7 ibrahim et al8 showed that when pi3k is inhibited , hr is impaired , which results in sensitization of brca wild - type triple - negative breast cancer cells to parpis . 
the details of the cohort are listed in table 1 . our analysis revealed that six patients among the 14 treated in brocade had experienced exceptional responses to treatment ; these six had been treated with the mtori everolimus before commencing study therapy . 
the patient with the second - best response had a documented pten deletion and nearly the same pfs at 29.2 months but did not receive veliparib with her carboplatin doublet . discussion most of the preclinical data of the role of the pik3ca / mtor pathway in dna damage sensitivity was carried out with concurrent therapeutic combinations . 
 these adaptive changes can persist over time , which allows one to use a treatment to sensitize a patients tumors to a subsequent therapy.14 , 15 the observed difference in pfs between eve + and eve patients raises the possibility that prior mtori exposure may render brca1 / 2 mutated breast cancer more susceptible to subsequent dna - damaging therapy . the interaction between activating pik3ca mutations or pten deletions and this sensitizing effect by mtori cannot be fully evaluated in this limited case series . 
however , it seems that the presence of these genomic abnormalities did not preclude those patients from deriving a significant benefit from subsequent dna - damaging therapy . in addition to the usual limitations and biases of case series , our analysis was limited by the heterogeneity of patient characteristics , prior treatments received , and study treatment assigned . 
this precludes us from specifically concluding how much of the observed clinical benefit in the eve + group was a result of improving the activity of the cytotoxic chemotherapy or the veliparib ( if given )  . 
in addition , veliparib did not significantly increase the median pfs of the experimental arm compared with the control arm in the overall study , so the effect of the treatment assignment may be minor in explaining the difference between the eve + and eve arms . 
the pfs of these two patients was similar to the main study population , so including them in the analysis with the other estrogen receptor positive patients is unlikely to change the main analysis . 
future studies in patients with brca1 / 2 mutations also should examine sequential treatment strategies by administering pi3kcai / mtori agents for one to two cycles as a sensitizing therapy before switching to a parpi or dna - damaging cytotoxic chemotherapy . 
han research funding : abbvie ( inst ) , prescient therapeutics ( inst ) , tapimmune ( inst ) , seattle genetics ( inst ) , g1 therapeutics ( inst ) , bristol - myers squibb ( inst ) , pfizer ( inst ) , novartis ( inst ) hatem h . 
lee moffitt cancer center and research institute , tampa , fl . presented at the 2017 annual meeting of the american society of clinical oncology , chicago , il , june 2 - 6 , 2017 . prior presentation references 10 : 18 , 2018 2012 150 , 2009 2017 1 . 
ibrahim yh , garca - garca c , serra v , et al : pi3k inhibition impairs brca1 / 2 expression and sensitizes brca - proficient triple - negative breast cancer to parp inhibition . 
mo w , liu q , lin cc , et al : mtor inhibitors suppress homologous recombination repair and synergize with parp inhibitors via regulating suv39h1 in brca - proficient triple - negative breast cancer . 
juvekar a , burga ln , hu h , et al : combining a pi3k inhibitor with a parp inhibitor provides an effective therapy for brca1 - related breast cancer . 
beuvink i , boulay a , fumagalli s , et al : the mtor inhibitor rad001 sensitizes tumor cells to dna - damaged induced apoptosis through inhibition of p21 translation . 
oreilly t , mcsheehy pmj , wartmann m , et al : evaluation of the mtor inhibitor , everolimus , in combination with cytotoxic antitumor agents using human tumor models in vitro and in vivo . 
han hs , diras v , robson m , et al : veliparib with temozolomide or carboplatin / paclitaxel versus placebo with carboplatin / paclitaxel in patients with brca1 / 2 locally recurrent / metastatic breast cancer : randomized phase ii study . 
 c rare pediatric invasive gliobroma has braf v600e mutation and transiently responds to targeted therapy before progressive clonal evolution kristiyana kaneva , md1 ; kee kiat yeo , md1 ; debra hawes , md1 , 2 ; jianling ji , md1 , 2 ; jaclyn a . 
a ventriculo - peritoneal shunt was subsequently placed to relieve the hydrocephalus . temporal microscopically , the tumor showed a biphasic growth pattern with an astrocytic component arranged in nests and cords surrounded by anastomosing bands of mesenchymal tissue ( fig 2 )  . 
the astrocytic component expressed glial brillary acidic protein ( gfap ) and showed mild - to - moderate cellular atypia , mitotic rate , and ki - 67 labeling index of 6% to 7% without palisading necrosis or glomeruloid endothelial proliferation , which is consistent with a low - grade glial neoplasthe mesenchymal component was cytologically bland , showed no mitotic activity , and did not express gfap . 
these features were consistent with a diagnosis of gliobroma , which consists of both mesenchymal and glial elements and has a low proliferation index ( fig 2 )  . signicant clinical improvement followed the initiation of dexamethasone , partial resection , and relief of hydrocephalus ; however , two careful attempts to wean the corticosteroids were unsuccessful . 
magnetic resonance ( mr ) spectroscopy at that time demonstrated highgrade featuresfor example , prominent cholinein the residual mass ( fig 3 )  . molecular studies using the oncoscan ( thermo fisher scientic , waltham , ma ) chromosomal microarray platform , which has been validated for brafv600e , revealed brafv600e mutation and biallelic deletion of cdkn2a ( table 1 )  . 
in children , cdkn2a / b loss has been found in gliomas and ependymomas.1 - 3 immunohistochemistry revealed mutant brafv600e in the glial elements of the tumor and absence of p16 ( cdkn2a ) in both glial and mesenchymal components ( fig 2 ) , which is consistent with the molecular analysis that shows brafv600e mutation and biallelic deletion of cdkn2a / b ( table 1 )  . the inltrative nature of the tumor ; the inability to wean the patient off dexamethasone ; the molecular studies showing a brafv600e mutation and deletion of cdkn2a , which portend a worse prognosis in pediatric glioma patients1 , 2 , 4 ; and the high - grade features on mr spectroscopy raised concern for the presence of high - grade inltrative components in the residual tumor despite the low - grade appearance of its resected portions . 
furthermore , in view of the poor prognosis of incompletely resected gliobromas ( fig 4 and data supplement ) , absence of established therapy for them , and an actionable mutation found in the patients tumor , targeted therapy was initiated . reports of emerging resistance to braf inhibitor monotherapy in patients with melanoma and improved survival with combined therapy prompted us to recommend combining braf inhibitor with mitogenactivated protein kinase ( mapk ) kinase ( mek ) inhibitor.5 the patient thus received vemurafenib 550 mg / m2 per dose two times per day ( a braf inhibitor ) and trametinib 4 mg / m2 per day ( an mek inhibitor )  . 
 ( o and p ) mri at 15 months shows a newly emerging dominant enhancing mass involving the posterior left temporal lobe with associated mass effect and deviation of the midbrain . tumors , was at more moderate levels . 
spectroscopy continued to suggest a lower grade lesion compared with pretherapy spectroscopy , similar to that at 9.5 weeks on therapy ( fig 3 and not liver transaminases prompted shown )  . 
 ( a ) hematoxylin and eosin ( h&e ) stained section of tumor showing biphasic growth pattern with nests of glial cells ( black arrow ) surrounded by bands of mesenchymal tissue ( white arrow )  . 
nuclei not in g0 phase are positive for ki - 67 ( dab , brown ) , whereas nuclei in g0 phase are negative ( hematoxylin , blue )  . 
 ( e and f ) in contrast to the trichrome and reticulin stains , glial brillary acidic protein ( gfap ) is expressed in the glial component of the tumor ( dab , brown ) and not in the mesenchymal component ( hematoxylin , blue )  . 
 ( j and k ) large areas of the glial components of the tumor were positive for the brafv600e - mutated protein ( dab , brown , ihc ) , although some regions did not express it . 
 ( n - r ) at recurrence , the tumor showed high - grade regions that were invasive into the lower - grade regions ( n ) , were highly cellular ( p ) , and had abundant mitotic gures ( q ; panels correspond to the dotted regions in panel p )  . 
the tumor continued to express the mutant brafv600e in many of the high - grade regions , although as in the original low - grade tumor , there were areas that were negative for this mutation ( r )  . routine mri at 15 months while on braf inhibitor ( vemurafenib ) plus mek inhibitor therapy revealed new growth with imaging features of a high - grade tumor , similar to pretherapy mr spectroscopy ( figs 1 and 3 )  . 
reresection showed gliobroma with areas of low - grade morphology which was ( trametinib ) similar to the original tumor , along with extensive areas that now contained high - grade features ( fig 2 )  . 
high - grade features included increased cellularity , high mitotic rate , and regions with markedly elevated mitotic index ( ki - 67 positive in up to 70% to 80% of nuclei )  . 
mr spectroscopy also demonstrates metabolic heterogeneity with markedly different levels of glycine ( glyc ) in different parts of the lesion with unclear signicance . lactate ( lac ) is observed in both regions of interest at approximately equal levels . 
 ( i and j ) at 15 months of targeted therapy , the newly the spectrum in the region of emerging mass shows signicantly increased cho that is consistent with proliferative tumor . 
brafv600e is not shown but present on chromosomal microarray , which has been validated for this mutation . abbreviation : cnv , copy number variant . proceeded to receive intensity - modulated radiation therapy to the tumor . molecular studies of the recurrent tumor again revealed the brafv600e mutation ( oncokids next - generation sequencing panel and oncoscan chromosomal microarray ) and the cdkn2a biallelic deletion ( oncoscan )  . 
on the basis of author - reported histopathology , patients with highgrade tumors had signicantly worse overall survival compared with low - grade tumors ( p , .001 ; fig 4 ) , similar to prior assessment.15 survival of patients who underwent complete resection was not signicantly different from that of patients with partial resection or biopsy ( p = .108 ; fig 4 )  . to date , only two patients with gliobroma have been reported to have experienced a response to chemotherapy . both were infants with unresectable low - grade gliobromas . 
one experienced a response to carboplatin and vincristine36 and the other to metronomic vinblastine.32 analysis of the rare published cases presented here is limited in that it depends on individual case reports that mostly provide relatively short and incomplete follow - up and may represent an unbalanced cohort of patients . 
thus , although this summary , to our knowledge , is the most comprehensive review of published gliobroma cases to date , these limitations must be considered . our patient provides four novel ndings with regard to gliobroma : this is the rst report , to our knowledge , on gliobroma with a molecularly proven brafv600e mutation and cdkn2a biallelic deletion ; the rst patient with gliobroma reported to receive targeted therapy and to respond to braf plus mek inhibition , albeit only for limited time ; the rst gliobroma described to acquire pdgfra and ptpn11 mutations upon recurrence as a high - grade glioma resistant to braf and mek inhibition ; and a rare opportunity to view the rapid molecular evolution of this tumor , with ( rst recurrence ) and without ( second recurrence ) therapy with braf plus mek inhibition . 
of interest , the brafv600e mutation in our patient was only found in the glial elements of the tumor , which suggests that the mesenchymal regions may be reactive to the glial pathology rather than independently tumorigenic . 
survival status ( alive / dead ) was not reported for ve of the 44 published patients , and duration of survival was not reported for ve others for whom survival status was reported . 
 ( a ) age of distribution at diagnosis of gliobroma . ( b ) overall survival for the 35 patients with gliobroma for whom survival data were reported ( of a total of 45 )  . 
at risk : glial and mesenchymal components , it is not known if this is a result of the deletion of cdkn2a in both compartments or if cdkn2a is deleted in one compartment and its expression is merely low in the other . 
it is interesting that in another glial tumor , ganglioglioma , brafv600e - expressing cells were mostly those with neuronal capacity or both neuronal and glial capacity.39 in contrast to that shown in our patient , in those gangliogliomas , p16 was robustly expressed.39 brafv600e oncogenic mutation is reported in 17% of pediatric low - grade gliomas.1 , 4 , 40 - 42 to date , brafv600e mutation has not been reported in gliobromas . 
one case report stated that braf mutations are present in approximately 50% of gliobromas7 ; however , the authors case did not have a braf mutation and no reference was provided to support the statement . 
this can be achieved best by a next - generation sequencing panel that covers both molecular alterations , such as the childrens hospital los angelesdeveloped oncokids panel.46 considering the poor response of incompletely resected brafv600e - mutated and cdkn2a - deleted pediatric lowgrade gliomas to chemotherapy and irradiation , 4 as well as the aggressive behavior of our patients tumor at presentation , we elected to treat him with the brafv600e inhibitor vemurafenib combined with the mek inhibitor trametinib . 
oncokids next - generation sequencing cancer panel findings from second reresection ( second recurrence , third tumor sample ) classication gene name exon genomic position dna change protein change strong clinical signicance ( tier i ) braf chr7 : 140 , 453 , 136 c . 
the results of this nal sample demonstrate two variants of strong clinical signicance ( braf and pik3ca ) and three variants of potential clinical signicance ( ptpn11 , pdgfra , and tp53 )  . abbreviation : chr , chromosome . brafv600e tumors to braf inhibitor monotherapy include an increase in braf dimers , braf splice variants , neuroblastoma ras viral oncogene homolog ( nras ) and kirsten rat sarcoma viral oncogene homolog ( kras ) mutations , braf amplications , mek mutations , and others.49 , 51 , 52 these render extracellular regulated kinase signaling insensitive to braf inhibitors while the downstream mek remains a viable target . 
combining a braf inhibitor with an mek inhibitor is thought to help retain tumor responsiveness and to have lower adverse effects compared with braf monotherapy.47 , 49 , 50 , 53 - 55 trametinib and other mek inhibitors are in clinical trials for pediatric patients . 
whereas preclinical research suggested a benet to combining a braf inhibitor and / or mek inhibitor with a cyclin - dependent kinase 4 / 6 inhibitor in tumors with both brafv600e and cdkn2a deletion , 57 , 58 peer - reviewed clinical data on the safety and efcacy of such combination were not available when the patient presented . our patients tumor showed clinical and radiographic response to vemurafenib and trametinib for more than 12 months . 
although it is possible that intratumor heterogeneity was the basis for their absence in the sample tested from the original tumor , their coexistence with the brafv600e mutation and cdkn2a deletion in the recurrent sample suggests that they are newly acquired and may have played a role in the recurrence . 
it is not known if these new mutations are in tumor cells that express the mutant braf protein or in those that stain negative for it ( fig 2r )  . overexpression and mutations in pdgfra are frequent in pediatric gliomas and in other cancers , with mutations occurring in more than 20% of high - grade gliomas but only rarely in low - grade ones.59 - 61 the pdgfra mutation , in addition to the aggressive nature of our patients recurrent glioma , supported the use of radiation therapy for the recurrence.61 mutations in d842 , located in the activation loop of pdgfra , 62 comprise more than one third of pdgfra substitution mutations reported to date in the cosmic catalogue ( 610 of 1 , 705 ) , with the majority ( 95% ) being d842v.63 , 64 to imatinib pdgfra - d842v renders pdgfra resistant in vitro , 64 - 66 but it remains sensitive to crenolanib , a newer pdgfra inhibitor that is currently in clinical trials.63 , 64 however , pdgfra - d842y , the mutation in our patients tumor , is moderately resistant to imatinib in vitro and is not as sensitive to crenolanib as the d842v mutant or the wild - type receptor.65 ptpn11 ( shp - 2 ) is mutated in the germline in noonan and leopard syndromes as well as somatically in cancer.67 across cancers , ptpn11 is mutated in 1 , 320 ( 1.9% ) of 70 , 712 cancer samples reported in cosmic.64 ptpn11 mutations are observed in both low - grade and high - grade pediatric gliomas.61 the ptpn11 ala72val ( a72v ) mutation in our patients recurrent tumor is located in the n - terminal sh2 domain of ptpn11 and is predicted to be a gain - of - function mutation.68 of the total 1 , 285 ptpn11 substitution mutations reported in cosmic , 180 are in alanine 72 , the second most mutated amino acid after glutamine 76 . 
several ptpn11 inhibitors are now beginning clinical trials in cancer in adults.69 in this respect , it is interesting that in mice ptpn11 can mediate glioma formation downstream of pdgfra overexpression and ink4a ( cdkn2a ) loss.70 it is therefore conceivable that , with this gliobromas pdgfra - d842y and ptpn11 - a72v activating mutations and the biallelic deletion in cdkn2a , this pathway may have contributed to the recurrent tumor in our patient . the serial acquisition of new mutations on subsequent recurrent specimens is consistent with clonal evolution of disease . 
pik3ca mutations are found in 21% of pediatric gliomas compared with 17% in adult glioblastomas71 , 72 ( table 2 )  . in summary , to our knowledge , this is the rst published report of a gliobroma that harbors a brafv600e mutation , the rst report on a gliobroma that responded to targeted therapy , and a unique view of clonal evolution of this rare tumor . 
biegel provision of study material or patients : kristiyana kaneva , debra hawes collection and assembly of data : kristiyana kaneva , kee kiat yeo , debra hawes , stefan bluml , mark d . 
nelson patents , royalties , other intellectual property : royalties from a book published in 2012 expert testimony : mdnelson , jr no other potential conicts of interest were reported . acknowledgment the authors thank yang fusheng for the expert immunohistochemistry contribution . 
mistry m , zhukova n , merico d , et al : braf mutation and cdkn2a deletion dene a clinically distinct subgroup of childhood secondary high - grade glioma . j clin oncol 33 : 1015 - 1022 , 2015 2 . 
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j clin oncol 35 : 2934 - 2941 , 2017 johnson db , flaherty kt , weber js , et al : combined braf ( dabrafenib ) and mek inhibition ( trametinib ) in patients with brafv600 - mutant melanoma experiencing progression with single - agent braf inhibitor . 
j neuropathol exp neurol 37 : 300 , 1978 ahmad mu , barborie a , pizer b , et al : midbrain gliobroma presenting in adulthood following cure of a childhood intraventricular pilocytic astrocytoma . pediatr neurosurg 52 : 151 - 154 , 2017 altamirano e , jones mc , drut r : gliobroma . 
escalante abril pa , salazar mf , l opez garca nl , et al : who grade iv gliobroma : a grading label denoting malignancy for an otherwise commonly misinterpreted neoplasj pathol transl med 49 : 325 - 330 , 2015 [ erratum : j pathol transl med 49 : 538 , 2015 ] 16 . 
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schindler g , capper d , meyer j , et al : analysis of braf v600e mutation in 1 , 320 nervous system tumors reveals high mutation frequencies in pleomorphic xanthoastrocytoma , ganglioglioma and extra - cerebellar pilocytic astrocytoma . 
clin cancer res 17 : 4790 - 4798 , 2011 jones dt , kocialkowski s , liu l , et al : tandem duplication producing a novel oncogenic braf fusion gene denes the majority of pilocytic astrocytomas . cancer res 68 : 8673 - 8677 , 2008 45 . 
j neurooncol 131 : 495 - 505 , 2017 johanns tm , ferguson cj , grierson pm , et al : rapid clinical and radiographic response with combined dabrafenib and trametinib in adults with braf - mutated high - grade glioma . 
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falchook gs , lewis kd , infante jr , et al : activity of the oral mek inhibitor trametinib in patients with advanced melanoma : a phase 1 dose - escalation trial . lancet oncol 13 : 782 - 789 , 2012 54 . 
king aj , arnone mr , bleam mr , et al : dabrafenib ; preclinical characterization , increased efcacy when combined with trametinib , while braf / mek tool combination reduced skin lesions . 
huillard e , hashizume r , phillips jj , et al : cooperative interactions of brafv600e kinase and cdkn2a locus deciency in pediatric malignant astrocytoma as a basis for rational therapy . 
cancer res 73 : 6219 - 6229 , 2013 johnson a , severson e , gay l , et al : comprehensive genomic proling of 282 pediatric lowand high - grade gliomas reveals genomic drivers , tumor mutational burden , and hypermutation signatures . 
liang l , yan xe , yin y , et al : structural and biochemical studies of the pdgfra kinase domabiochem biophys res commun 477 : 667 - 672 , 2016 63 . 
lasota j , dansonka - mieszkowska a , sobin lh , et al : a great majority of gists with pdgfra mutations represent gastric tumors of low or no malignant potential . lab invest 84 : 874 - 883 , 2004 64 . 
dempke wcm , uciechowski p , fenchel k , et al : targeting shp - 1 , 2 and ship pathways : a novel strategy for cancer treatment ? oncology 95 : 257 - 269 , 2018 70 . 
liu kw , feng h , bachoo r , et al : shp - 2 / ptpn11 mediates gliomagenesis driven by pdgfra and ink4a / arf aberrations in mice and humans . 
we have previously reported preliminary results of our precision medicine prograhere , we present response and survival outcomes for 637 additional patients who were referred for phase i trials and were treated with matched targeted therapy ( mtt ) when available . patients and methods patients with advanced cancer who underwent tumor genomic analyses were treated with mtt when available . results overall , 1 , 179 ( 82.1% ) of 1 , 436 patients had one or more alterations ( median age , 59.7 years ; men , 41.2% ) ; 637 had one or more actionable aberrations and were treated with mtt ( n = 390 ) or non - mtt ( n = 247 )  . 
patients with phosphatidylinositol 3 - kinase ( pi3k ) and mitogenactivated protein kinase pathway alterations matched to pi3k / akt / mammalian target of rapamycin axis inhibitors alone demonstrated outcomes comparable to unmatched patients . conclusion our results support the use of genomic matching . 
in 2007 , we initiated the impact ( initiative for molecular profiling and advanced cancer therapy ) trial , a personalized medicine program for patients who were referred to the phase i clinical trials program at md anderson cancer center . 
personalized , or precision , medicine uses traditional and emerging concepts with regard to the genetic and environmental basis of disease to individualize prevention , diagnosis , and treatment , 1 , 2 and integrates tumor genetics of individual patients into medical practice.3 the aim of the personalized medicine program is to use tumor molecular profiling to optimize the selection of targeted therapies for patients who are considered for phase i clinical trial participation . 
 here , we present results for 1 , 436 additional patients who underwent clinical - grade molecular profiling before treatment in the phase i clinical trials prograwe demonstrate that matched targeted therapy ( mtt ) is associated with improved outcomes . 
group 2 : mtt with tp53 match and inclusion of vegf / vegfr therapy as targeted therapy against tp53 ; non - mtt ( all others ) .13 group 3 : negative matches include only mtt against an alteration in the pi3k axis in the presence of kras or braf or another mek pathway mutation ( the latter being a known resistance pathway ) and no mek / raf inhibitor ; negative matches do not include patients with additional positive matches ; positive mtt minus negative matches include patients who had mtt ( without considering tp53 mutations matched to vegf / vegfr inhibitors ) minus the negative matches ; non - mtt ( patients who had no mtt minus the negative matches )  . 
baseline characteristics of 637 patients with mutations by type of therapy nonmatched ( n = 247 ) matched ( n = 390 ) characteristic age , years , 60 > 60 female male no . 
patients whose tumors had a molecular aberration were preferably treated in a clinical trial with a matched targeted agent when available . if two or more molecular aberrations were present , patients were preferably treated in a trial of therapies that targeted both aberrations . 
if such a trial was unavailable , a physicians choice of a trial that targeted one aberration was permitted ( appendix )  . definition of matched therapy a patients tumor was considered matched with a targeted therapy if a drug was known to inhibit the aberration at low nanomolar concentrations or if an antibody targeted the alteration product , per literature data 9 - 12 ( appendix )  . 
subset analyses are listed in table 1 . end points and statistical methods statistical analyses were performed by a biostatistician ( k.h. ) using s - plus software for windows ( version 8.2 ; tibco software , palo alto , ca )  . 
by using response evaluation criteria in solid tumors ( recist ) guidelines , 14 , 15 we assessed objective response rates ( complete response [ cr ] and partial response [ pr ] ) , clinical benefit rates ( stable disease [ sd ] > 6 months plus pr plus cr ) , and rates of failure - free survival ( ffs ) and overall survival ( os )  . 
failure - free survival and overall survival in patient subgroups . group 1 : matched targeted therapy ( mtt ) versus overall , 390 patients ( 27% of 1 , 436 total patients ; or 61.2% of 637 patients ) received matched therapy and 247 ( 17.2% ) received nonmatched therapy . tumor types treated are listed in table 3 . 
group 2 : mtt with tp53 ( includes matching as previously published plus inclusion of antivascular endothelial growth factor [ vegf ] therapy as targeted therapy against tp53 ) versus nonmtt . 
group 3 : mtt minus negative matches ( includes patients who had matched targeted therapy , without considering tp53 mutations matched to vegf / vegf receptor p = .041 ; table 1 and figs 1a and 1b )  . 
group 4 : mtt with tp53 match minus negative matches ( includes tp53 mutation matches to vegf / vegfr inhibitors but excludes negative matches ) versus negative matches ( see definition for group 3 ; table 1 ) versus non - mtt . ( g ) failure - free survival . ( h ) overall survival . 
group 5 : non - mtt ( includes nontargeted therapy or targeted therapy against an alteration in the pi3k axis in the presence of kras or braf or other mek pathway mutation and no mek / raf inhibitor ) versus mtt ( includes all other groups , including tp53 matches )  . 
no difference was observed in the unmatched group . group 3 analysis the group 3 analysis was similar to that of group 1 , except that we isolated a group of 36 patients who had negative matches , a term applied when patients were matched by virtue of a pi3k pathway alteration to a pi3k / akt / mtor axis inhibitor , but a ras / raf / mek alteration was also present and not matched to a drug . 
these results showed that negative matches attained rates of cr / pr and sd > 6 months / cr / pr that were similar to those of unmatched patients , and that ffs and os were equivalent . 
these results are consistent with the hypothesis that matching patients who harbor a pi3k and a mapk pathway alteration to a pi3k pathway inhibitor alone does not improve outcomes.8 , 16 group 4 analysis the group 4 analysis was similar to that of group 2 , which included tp53 mutations matched to vegf / vegfr inhibitors , except that we again isolated the group of 36 patients who had negative matches . 
these results demonstrate that negative matches had rates of cr / pr and sd > 6 months / cr / pr that were similar to those of unmatched patients , and that ffs and os were similar . 
conversely , depending on the outcome parameter , negatively matched patients either had significantly worse outcomes or trended toward worse outcomes compared with positively matched patients . group 5 analysis the group 5 analysis compared positively matched patients , which included tp53 mutations matched to vegf / vegfr inhibitors , with negatively matched patientsas defined for group 4plus unmatched patients . 
these results demonstrate that , for all outcome parameters , matched patients , which included tp53 mutations matched to vegf / vegfr inhibitors , did significantly better than the combined group of unmatched and negatively matched patients . discussion the application of precision medicine using targeted agents to inhibit the function of tumor molecular alterations is a complex process . 
 ( f ) failurefree survival according to objective response ( cr + pr , yes ) versus no response ( no ) in patients who received in this retrospective analysis , we report 1 , 436 patients who underwent prospective molecular profiling with a clia - certified test . 
of 637 treated patients with at least one alteration , 61% ( n = 390 patients ; 27% of the total 1 , 436 patients ) received mtt and 39% received non - mtt . 
this number is similar to that of other studies ; tumors that were interrogated with larger panels of genes are more likely to have alterations.13 , 17 , 18 indeed , in some reports , approximately 95% of patients from whom adequate tissue is obtained are found to have molecular alterations.13 , 16 - 20 the complexity of using precision medicine is explained , in part , by the coexistence of multiple molecular alterations , as seen in our population , the lack of efficient targeted agents for all alterations , and the fact that some alterations are more difficult to target than others.19 this observation is consistent with previously published results that have demonstrated that a matching scorenumber of matches divided by number of alterationscorrelates well with all outcome parameters.13 a limitation of the current analysis relates to the fact that gene panels of different sizes were used for molecular profiling , and , hence , the impact of the number of alterations in each patient could be confounded by the panel size . several previous studies have been performed with variable results . 
for instance , the shiva triala randomized molecular navigation trialdid not achieve its endpoints16 ; however , approximately 80% of patients in shiva were matched to single - agent hormone modulators or mtor inhibitors.21 , 22 our current results confirm that single - agent pi3k pathway inhibitors are generally not effective , especially in patients with concomitant mapk pathway alterations . 
indeed , for these patients , targeting the pi3k pathway without targeting the mapk pathway was associated with outcomes that were indistinguishable from , or numerically worse than , those in unmatched patients ( table 1 and figs 1e to 1h )  . 
outcome parameters were favorable in groups that included patients who were matched in this way , and the strongest p values were observed in the group of patients that both included tp53 alterations matched to vegf / vegfr inhibitors and excluded patients who harbored both pi3k and mapk pathway alterations matched to only pi3k / akt / mtor axis inhibitors ( group 5 ; table 1 and fig 1 )  . 
these observations are supportive of previously published findings that tp53 may be a targetable alteration , and suggest that , in patients with pi3k pathway anomalies , the presence of mapk resistance alterations must be addressed . our study had several limitations . 
third , molecular analysis was performed by using archival tissue in most patients , tissue was sometimes inadequate for testing all available molecular aberrations , and the availability of clia - certified tests varied over the years and , thus , some molecular profiles became suboptimal by later standards . 
to address the limitations of this study , we have initiated the impact 2 trial , a phase ii randomized study evaluating molecular profiling and targeted therapy in metastatic cancer ( nct02152254 ) .6 , 7 multiple other nonrandomized trials of molecular profiling have been completed or are ongoing ( nct01771458 , nct01827384 , nct02154490 , nct01042379 , and nct01856296 ) .6 , 7 , 13 , 16 , 17 , 23 , 24 in conclusion , our analysis demonstrates that precision medicine is feasible in an academic setting and that it is associated with superior outcomes compared with non - mtt in patients with advanced cancer . 
the rate of matching was approximately 27% in our group of patients , which is consistent with some previous studies but higher than that observed in other trials.6 , 7 , 13 , 17 , 18 higher rates of matching may be associated with larger gene panels , which produce more potentially actionable alterations , 18 with more robust clinical trial portfolios and with molecular studies with flexible algorithms and eligibility criteria that are not overly restrictive . 
kies , russell broaddus , john mendelsohn , razelle kurzrock collection and assembly of data : apostolia - maria tsimberidou , yang ye , carrie cartwright data analysis and interpretation : apostolia - maria tsimberidou , kenneth r . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs. org / site / ifc . apostolia - maria tsimberidou research funding : emd serono ( inst ) , baxter ( inst ) , foundation medicine ( inst ) , onyx pharmaceuticals ( inst ) , bayer ( inst ) , boston biomedical ( inst ) , placon therapeutics ( inst ) david s . 
hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack pharmaceuticals , bayer consulting or advisory role : baxter , bayer research funding : novartis , genentech , eisai , astrazeneca , pfizer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly travel , accommodations , expenses : loxo , mirna therapeutics other relationship : oncorena the following represents disclosure information provided by authors of this manuscript . 
kies no relationship to disclose russell broaddus no relationship to disclose john mendelsohn leadership : merrimack pharmaceuticals stock and other ownership interests : merrimack pharmaceuticals patents , royalties , other intellectual property : royalty payments from university of california san diego travel , accommodations , expenses : merck kenneth r . 
hess , the university of texas md anderson cancer center , houston , tx ; and razelle kurzrock , university of california , san diego , san diego , ca . supported in part by the alberto barretto donor fund , the jamie hope donor fund , funding from and zane w . 
wheler j , tsimberidou am , hong d , et al : survival of 1 , 181 patients in a phase i clinic : the md anderson clinical center for targeted therapy experience . 
druker bj , talpaz m , resta dj , et al : efficacy and safety of a specific inhibitor of the bcr - abl tyrosine kinase in chronic myeloid leukemia . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
clin cancer res 20 : 4827 - 4836 , 2014 janku f , hong ds , fu s , et al : assessing pik3ca and pten in early - phase trials with pi3k / akt / mtor inhibitors . cell reports 6 : 377 - 387 , 2014 9 . 
said r , hong ds , warneke cl , et al : p53 mutations in advanced cancers : clinical characteristics , outcomes , and correlation between progression - free survival and bevacizumab - containing therapy . 
koehler k , liebner d , chen jl : tp53 mutational status is predictive of pazopanib response in advanced sarcomas . ann oncol 27 : 539 - 543 , 2016 11 . 
schwaederle m , lazar v , validire p , et al : vegf - a expression correlates with tp53 mutations in non - small cell lung cancer : implications for antiangiogenesis therapy . 
therasse p , arbuck sg , eisenhauer ea , et al : new guidelines to evaluate the response to treatment in solid tumors . european organization for research and treatment of cancer , national cancer institute of the united states , national cancer institute of canada . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
le tourneau c , kurzrock r : targeted therapies : what have we learned from shiva ? nat rev clin oncol oncotarget 5 : 3871 - 3879 , 2014 drugs . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular profiling of patients tumors to find potential targets and select treatments for their refractory cancers . 
mol cancer ther 16 : e579 - e580 , 2015 14 : 847 - 856 , 2015 patients methods in brief , patients with advanced or metastatic cancer for whom standard - of - care therapy had been exhausted or for whom no food and drug administrationapproved therapy was available for their indication were referred for participation in phase i clinical trials . 
all protocols required that participants have evidence of evaluable or measurable disease according to recist guidelines14 , 15 and an eastern cooperative oncology group performance status of 0 to 2 . 
additional eligibility criteria varied depending on which specific phase 1 clinical trial in which the patient enrolled . archival formalin - fixed , paraffin - embedded tissue blocks or tissue from fine - needle aspiration or surgical biopsies was used for profiling . 
molecular and / or immunohistochemistry assays were performed when tissue was available by using standard operating procedures and pcr - based sequencing technology . tumor molecular profiling for 637 patients was performed in the following laboratories : md anderson cancer center ( hotspot testing of 11 genes , n = 282 ; 46 genes , n = 145 ; and 50 genes , n = 20 ; patients , n = 447 ) , foundation medicine ( nextgeneration sequencing of 182 genes ; patients , n = 151 ) , knight diagnostics ( 48 genes ; patients , n = 20 ) , and other cliacertified laboratories ( patients , n = 19 )  . analysis of molecular aberrations dna was extracted from microdissected , paraffin - embedded tumor samples , and the coding regions for specific exons , depending on the test ordered , were analyzed for the following genes : pik3ca ( exon 9 : codons 532 to 554 ; exon 20 : codons 1 , 011 to 1 , 062 ) ; braf ( exon 15 : codons 595 to 600 ) ; kras and nras ( exon 2 : codons 12 , 13 , and 61 ) ; egfr ( exons 18 to 21 of the kinase domain ) ; kit ( exons 9 , 11 , 13 , and 17 ) ; gnaq ( exon 5 ) ; tp53 ( exons 4 to 9 ) ; met ( exon 2 : codon 375 ; exon 11 : codon 848 ; exon 14 : codons 988 and 1010 ; exon 16 : codons 1112 and 1124 ; exon 19 : codons 1 , 248 , 1 , 253 , and 1 , 268 ) ; and ret ( exon 10 : codons 609 , 611 , 618 , and 620 ; exon 11 : codon 634 ; exon 16 : codon 918 )  . 
the sensitivity of mutation assays for the detection of pik3ca , braf , kras , nras , gnaq , and met mutations was approximately one in 10 mutation - bearing cells in the microdissected area . 
loss of expression of the tumor suppressor nuclear protein , pten , was determined by using immunohistochemical staining with the monoclonal mouse anti - human pten clone 6h2 ( code m3627 ; dako , carpinteria , ca )  . 
with the availability of next - generation sequencing , some patient tumors were assessed by more extensive molecular profiling of 48 or more genes at md anderson or in other clia - certified laboratories . selected patients also had tumor molecular profiling using next - generation sequencing performed by foundation medicine ( cambridge , ma )  . 
genomic libraries were captured for 3 , 230 exons in 182 cancer - related genes plus 37 introns from 14 genes that are often rearranged in cancer and sequenced to an average median depth of 734 3 with 99% of bases covered  . 
alternatively , fluorescent in situ hybridization analysis was used to measure the copy number of her2 / neu . before the use of next - generation sequencing , the clia pathology laboratory prioritized the testing of molecular aberrations on the basis of their known frequency in cancer and / or whether they were perceived as actionable or as having other clinical relevance to patients . 
treating physicians requested all available molecular tests that were clia - certified at md anderson cancer center at the time a patient who was interested in receiving treatment in the phase i clinical trials program presented to the phase i clinic . 
if tissue available for analysis was limited , the treating physician prioritized molecular testing on the basis of tumor type and the availability of clinical trials that could impact specific targets . treatment treatment regimens included one or more drugs . 
allocation of patients to investigational treatment varied over time according to protocol availability , eligibility criteria , histologic diagnosis , the patients prior response to therapy , potential toxicity , insurance coverage , and patient preference or physician choice . 
physicians prioritized matched therapyversus nonmatched therapyon the basis of the following criteria : patients had an actionable molecular aberration ; matched targeted therapy ( mtt ) was available ; patients met the eligibility criteria ; insurance coverage was obtained ; and patients agreed to comply with study requirements . 
 sponsored studies ( further limiting the number of patients enrolled per institution ) , and restrictions associated with eligibility criteria , not all patients with an actionable aberration could be treated on a protocol with matched therapy . definition of matched therapy pik3ca mutations and pten loss could be targeted by inhibitors of akt and mammalian target of rapamycin , as well as phosphatidylinositol 3 - kinase ( pi3k ) , as akt and mammalian target of rapamycin are downstream of activated pik3ca and because both pik3ca mutations and pten loss , which usually reflects pten mutation , activate pi3k . 
braf mutations could also be targeted by braf inhibitors . other aberrations , such as ret , egfr , kit , and met mutations , were targeted by drugs that inhibit the respective activated kinase with 50% inhibitory concentration ( ic50 ) in the low nanomolar range . 
tp53 mutations were not initially considered actionable by drugs available in our trials ; however , with more recent emerging data , 8 - 11 tp53 mutations were considered actionable by vascular endothelial growth factor ( vegf ) / vegf receptor ( vegfr ) inhibitors , and an appropriate secondary analysis on this basis was included . 
we performed subset analyses for clinical outcome comparisons using the following ( table 1 , footnote ) : group 1 : mtt , as previously published6 , 7 ; non - mtt ( all others )  . 
group 3 : negative matches , which includes only mtt against an alteration in the pi3k axis in the presence of kras or braf or another mek pathway mutation ( the latter being a known resistance pathway ) and no mek / raf inhibitor.8 negative matches do not include patients with additional positive matches ; positive mtt minus negative matches , which includes patients who had mtt ( without considering tp53 mutations matched to vegf / vegfr inhibitors ) minus the negative matches ; non - mtt refers to patients who had no mtt minus the negative matches . 
group 5 : mtt with tp53 match minus negative matches refers to all matched groups , including tp53 matches to vegf / vegfr inhibitors , but excluding negative matches ( group 4 negative matches excluded ) ; non - mtt plus negative matches includes patients without a match as well as mtt against an alteration in the pi3k axis in the presence of kras or braf or other mek pathway mutation ( the latter being a known resistance pathway ) and no mek / raf inhibitor ( group 4 negative matches included )  . the rationale for subset analyses is as follows : group 1 is straightforward and consistent with our previously published analyses.6 , 7 group 2 included anti - vegf / vegfr agents matched to tp53 alterations . 
recent studies demonstrated that altered tp53 upregulates angiogenesis and vegf - a.11 in addition , published data from our group and other investigators showed that patients with tp53 alterations have improved outcomes if treated with anti - vegf / vegfr agents.9 - 12 therefore , we did a subset analysis ( group 2 ) to examine matched versus unmatched therapy , including tp53 alterations matched to anti - vegf / vegfr agents . 
negative matches pertained to individuals who had both a pi3k axis alteration and a kras or braf or other mek pathway mutationthe latter being a known resistance pathwayand were matched only with a pi3k axis inhibitor . 
several investigators suggest that these patients are resistant to a pi3k axis inhibitor , likely because the mapk pathway is not targeted.8 , 17 , 18 in groups 4 and 5 , we further explored analyses that included negative matches together with unmatched patients as well as tp53 alterations matched to vegf / vegfr inhibitors . end points and statistical methods matched versus unmatched and grouping was verified by one of the coauthors ( r.k. ) who was blinded to outcome data at the time that designation was assigned . overall survival ( os ) was measured from the initiation of participation in the phase i trial until death or last follow - up . failure - free survival ( ffs ) was measured from the first day of treatment on a clinical trial until the date of discontinuation of treatment of any reason , including disease progression , treatment toxicity , or death , whichever came first . 
the decision to discontinue treatment on protocol was made by the treating physician and was based on the patients history , clinical presentation , and imaging studies ( response assessment using recist criteria )  . 
all p values presented are two sided , and the statistical significance level was p < .05. we also performed landmark analyses for ffs and os at 2 months , as we previously published.7 we omitted patients with event times or censoring times of , 2 months and stratified outcome by overall response status . we also compared matched responders with nonmatched responders ( supplemental file )  . results objective response in patients who were treated with matched and nonmatched therapy by tumor type and molecular alterations is shown in appendix tables a1 and a2 . 
the small numbers of patients in the subgroups preclude robust analyses . we also performed a 2 - month landmark analysis that compared ffs and os between matched responders and nonmatched responders . 
the small numbers of patients in the subgroups preclude robust analyses for most comparisons . we then performed an analysis , excluding patients with estrogen receptor / progesterone receptor overexpression from the matched therapy group . 
 ( c ) analysis excluding patients with estrogen receptor ( er ) / progesterone receptor ( pr ) overexpression - based matching from the matched therapy group 1 : failurefree survival . 
 novel egfr v834l germline mutation associated with familial lung adenocarcinoma introduction lung cancer is a worldwide , known disease with a high mortality rate and is often related to nicotine abuse . 
this analysis revealed a well - known oncogenic l858r mutation along with a v834l variant , which are both egfr exon 21 substitutions and are present in the same allele ( in cis )  . 
 the v834l variant seemed to be present in the germline , because both normal adjacent lymph node tissue and lymphocyte - derived dna from whole blood of the index patient showed this variant . the patient was treated with the egfr tyrosine kinase inhibitor ( tki ) erlotinib . 
the patients father died at a young age as the result of massive hemoptysis , without a diagnosis . after written consent and permission were obtained from the index patient and family members , egfr mutation and germline variation analyses were performed on tumor samples and healthy tissue , respectively , of the three affected relatives . 
 v834l l858r v834l l858r t790m v834l l858r t790m c797s the deaths of the index patients brother , sister , and daughter , no blood was available ; only archival formalin - fixed paraffin - embedded normal and tumor tissues were available . like our index patient , all three affected family members had a heterozygous egfr v834l germline variant in normal tissue and the same somatic egfr l858r mutation in cis with the v834l variant in their respective tumor tissues . 
to our knowledge , this is the first report of a family with multiple cases of nsclc associated with germline transmission of an egfr v834l germline variant ; all tumors in the four family members additionally harbored a somatic egfr l858r mutation in cis . 
all except one of the known v834l carriers developed lung cancer during their lifespan , but so far none of the investigated noncarriers . there are only a few reports documenting families with proven inherited egfr variants over generations that probably conferred predisposition to lung cancer.1 , 2 in a family with egfr v843i mutations , four family members in two generations ( three of them with proven germline variants ) developed lung adenocarcinoma.1 as in the family we studied , all of these adenocarcinomas displayed a somatically - acquired l858r mutation in cis with v843i . 
interestingly , multiple distinct synchronous tumors of the index patient displayed different additional egfr mutations ( ie , deletions of 3 and 15 bp in exon 19 and l858r ) .2 a report by bell et al3 describes a family with five members affected by lung cancer . 
proven germline egfr t790m mutations were present in three patients in two generations.3 in distinct lesions in two of these patients , the mutation co - occurred with different egfr substitutions ( l858r , l747t751del , and g716a ) , all in cis with t790m . 
 because t790m is a well - known tki resistance mutation , no response was observed upon gefitinib treatment in the only tki - treated patient of this family , as expected . incidental cases of germline egfr variants in patients with lung cancer have been reported . 
 these have included variants such as v769m , r776h , and t790m substitutions in exon 20 and r831c , v843i , and p848l substitutions in exon 21.4 - 9 however , in the absence of family histories , it is unclear whether these variants predisposed these patients to lung cancer . 
although this is a relatively small cohort , this may indicate that the v834l variant is not or only weakly oncogenic and by itself is not sufficient to drive uncontrolled growth . 
however , when a second oncogenic mutation in cis is present , cell growth accelerates more than proportionally . this hypothesis is in line with eight described egfr v834l variants found in the catalogue of somatic mutations in cancer database.9 the v834l variant in the lung tumors of all of these patients , with unknown germline status , is accompanied by the l858r mutation ( seven times ) or by an exon 19 deletion.10 - 12 the reason for the apparent preference of v834l for l858r is unclear . 
this is possibly because the energy balance of the egfr v769msubstituted protein does not favor combination with l858r.9 structural and functional analysis of the v834l variant alone and / or in combination with strong oncogenic driver mutations can provide additional mechanistic information on its pathogenicity and preferred association with other oncogenic egfr mutations . until now , lung cancer surveillance programs have been mainly recommended for active smokers or patients with a smoking history of 30 pack years but who have stopped within the last 15 years . 
for more information about ascos conflict of interest policy , please refer to or ascopubs.org / po / author - center . cor van der leest honoraria : roche , boehringer ingelheim , bristol - myers squibb consulting or advisory role : roche , abbvie , boehringer ingelheim , bristol - myers squibb rute m . 
aerts stock and other ownership interests : amphera consulting or advisory role : eli lilly , genentech , bristol - myers squibb , msd oncology , boehringer ingelheim , amphera speakers bureau : astrazeneca patents , royalties , other intellectual property : an allogenic lysate for vaccination ( inst ) winand n.m. 
van noesel j , van der ven wh , van os ta , et al : activating germline r776h mutation in the epidermal growth factor receptor associated with lung cancer with squamous differentiation . 
prim n , legrain m , guerin e , et al : germ - line exon 21 egfr mutations , v843i and p848l , in nonsmall cell lung cancer patients . 
heon s , yeap by , britt gj , et al : development of central nervous system metastases in patients with advanced non - small cell lung cancer and somatic egfr mutations treated with gefitinib or erlotinib . 
wu sg , chang yl , hsu yc , et al : good response to gefitinib in lung adenocarcinoma of complex epidermal growth factor receptor ( egfr ) mutations with the classical mutation pattern . 
tam iy , chung lp , suen ws , et al : distinct epidermal growth factor receptor and kras mutation patterns in non - small cell lung cancer patients with different tobacco exposure and clinicopathologic features . 
 molecular testing in patients with castration - resistant prostate cancer and its impact on clinical decision making purpose metastatic castration - resistant prostate cancer ( crpc ) is the lethal form of the disease . many groups have performed mutational or immunohistochemistry ( ihc ) testing in metastatic crpc to identify treatment targets . 
we report our institutions experience with mutational and ihc testing in patients with metastatic crpc and its impact on clinical decision making and patient outcomes . methods between 2012 and 2015 , 59 patients with crpc underwent metastatic tissue biopsies and were genotyped with a 37cancer gene panel in a clinical laboratory improvement amendmentscertified laboratory . 
a retrospective chart review was performed to determine whether the genomic information was acted upon and the outcome of patients whose treatment was guided by molecular testing . results forty - six of 59 patients with crpc ( 78.0% ) had biopsies with adequate tumor for mutational testing . 
thirty - one of 46 subjects ( 67.4% ) had mutations identified by sequencing . of the 35 patients with crpc whose biopsies were evaluated for pten expression by ihc testing , 13 had pten loss . 
two patients had treatment on the basis of molecular testing , and one of these subjects had greater tumor control with molecularly guided therapy than his immediate prior therapy . conclusion targeted sequencing and ihc can identify clinically informative molecular abnormalities in crpc . 
actionability of abnormalities identified in metastatic crpc may be improved with access to clinical trials , insurance approval for unapproved uses of existing anticancer drugs , and larger gene sequencing panels that include more frequently mutated genes . introduction prostate cancer is the second - leading cause of cancer - related death in men in the united states , and more than 26 , 000 men are predicted to die as a result of prostate cancer in 2017.1 nearly all of these deaths occur as a result of metastatic tumors . the principal treatment of metastatic prostate cancer is androgen - deprivation therapy or other treatments that disrupt the function of the androgen receptor ( ar ) protedespite these treatments , progression to lethal castration - resistant prostate cancer ( crpc ) is nearly universal . 
once a tumor becomes resistant to ar - targeted therapy , few effective treatment options remathis underscores the urgent need to identify important molecular targets that may guide not only drug development but also clinical decision making for patients . technological advances in sequencing have led to the identification of molecular abnormalities present in cancers . 
 several cancer types , including melanoma and adenocarcinoma of the lung.2 - 4 hospitals across the country are increasingly implementing tumorsequencing platforms to help guide therapy for patients with advanced cancers . several studies have reported the frequency of abnormalities detected with mutational testing in advanced cancers.5 in crpc , recent work demonstrates that these tumors share many aberrations in oncogenic pathways found in other solid tumors.6 , 7 indeed , the majority of patients with crpc have alterations in pten or phosphatidylinositol 3 - kinase ( pi3k ) .8 , 9 importantly , both pi3k and akt inhibitors are in clinical testing . thus , there is a strong rationale to test for abnormalities in pten , pi3k , and other alterations that may be targeted with specific therapies . 
however , molecular testing is not routinely performed in patients with crpc , and the utility of targeted molecular testing in this disease is unknown . moreover , there is limited information on the frequency with which molecular testing guides therapy , as well as limited information on the outcomes of patients whose treatment was guided by molecular testing . in this article , we describe our experience with mutational testing and pten immunohistochemistry ( ihc ) in a clinical laboratory improvement amendments ( clia ) certified laboratory to guide therapy in men with metastatic crpc . 
finally , we present outcomes of the patients whose treatment was guided by molecular testing . methods biopsies and subsequent mutational profiling and ihc testing were performed under an oregon health & science university institutional review board ( irb ) approved metastatic tissue collection protocol . 
progression was defined as soft tissue progression by response evaluation criteria in solid tumors ( recist ) version 1.1 , bone scan progression by the presence of at least two new lesions , symptomatic progression in an area of radiologicalevident disease , or prostate - specific antigen progression defined as levels  . 
those who received first - generation oral antiandrogens ( flutamide , bicalutamide , nilutamide ) as their most recent systemic therapy before biopsy had to have progressed after at least 4 weeks of antiandrogen discontinuation . 
patients had to have an eastern cooperative oncology group performance status of 0 to 3 , a platelet count > 75 , 000 / ml , prothrombin time or international normalized ratio and activated partial thromboplastin time , 1.5 times the upper limit of normal , and the ability to discontinue anticoagulation for at least 1 week before tumor biopsy . 
patients without prior orchiectomy continued medical castration therapy while they were participating in the study . all patients signed an informed consent form before biopsy . metastatic tissue was collected by computed tomography or ultrasound - guided biopsies performed at oregon health & science university in accordance with the standard operating procedure and institutional standards , with the goal of minimizing patient risk . 
biopsies were fixed in 10% neutral - buffered formalin for 8 hours and then transferred to 70% ethanol , paraffin embedded , and subsequently stained with hematoxylin and eosall hematoxylin and eosinstained slides were examined by a pathologist ( g.v.t. ) , who reviewed tumor content and decided if the sample was adequate for molecular testing . 
generated clinical reports , which were given to the treating clinician within 6 weeks . these reports included a discussion of the clinical significance and potential actionability of the findings on the basis of type of aberration , existing agents , or ongoing clinical trials . 
actionable is defined on the basis of the 2017 joint association for molecular pathology , asco , and college of american pathologists guidelines.10 mutations were grouped according to evidence - based variant categorization into three tiers , ie , tier 1 : variants of strong clinical significance ; tier ii : variants of potential clinical significance ; and tier iii : variants of unknown clinical significance . 
in total , 46 of 59 patients with crpc ( 78.0% ) had biopsies with adequate tumor to submit for genetrails mutational testing ( fig 1c )  . of the 46 patients who had sufficient tumor for mutational testing , 31 ( 67.4% ) had one or more mutational abnormalities identified by sequencing ( fig 2 , appendix table a1 )  . 
of 31 patients , 18 had at least one potentially actionable mutation , seven had at least one mutation of uncertain significance , and six had only nonactionable mutations . we also determined the frequency with which the mutational abnormalities were present in the patient cohort . 
there was a trend toward pten mutations and loss of pten protein expression by ihc testing ( fishers exact test two - tailed p value .075 ; fig 3b )  . we also examined the frequency with which potentially actionable alterations were actually acted upon . 
in both cases , these patients had mutational abnormalities in the pten / pi3k pathway . patient 1 was 77 years of age , had metastatic crpc , and experienced clinical and disease progression after 14 weeks of enzalutamide therapy . a biopsy of his iliac bone was performed , and testing revealed a pten p.i33fs * 11 somatic mutation and loss of pten protein expression by ihc . 
however , he developed clinical and disease progression 8 weeks later ( fig 4 )  . patient 2 was 67 years of age and had metastatic crpc ; his prostate - specific antigen level was decreasing in the setting of disease progression . biopsy of a pelvic mass revealed somatic mutations of fgfr3 , notch1 , and rb1 ; pten loss was found by ihc testing . 
on the basis of pten loss , as shown by ihc testing of his biopsy specimen , he was enrolled in a clinical trial of a pi3k inhibitor . his symptoms of pain improved , and his scans showed stable disease for 19 weeks before clinical and radiographic progression was eventually determined ( fig 4 )  . discussion advances in next - generation sequencing have improved our ability to identify tumor genomic alterations . 
baseline characteristics of 59 patients with metastatic castration - resistant prostate cancer characteristic age ( years ) median range median interquartile range total gleason score ( % ) time from initial diagnosis of prostate adenocarcinoma to biopsy ( years ) ecog performance status ( % ) psa at time of biopsy ( ng / ml ) median interquartile range no . 
importantly , results of mutational testing were available within 6 weeks ( mean time , 14 days ) , and all results were shared with the patients and treating providers . sixty - seven percent ( 31 of 46 ) of patients were found to have mutations . 
pten was inactivated by loss of expression or mutation in 19 of 46 ( 41.3% ) patient biopsy specimens , which is consistent with other reports.8 , 14 preclinical studies suggest that rb1 - mutant tumors do not respond to cdk4 / 6 inhibitors , and all of the rb1 aberrations we found were predicted to be loss of function . 
however , these rb1 aberrations were reported as nonactionable because there are currently no effective strategies to target tumors with mutant retinoblastoma protetsc2 mutations were regarded as potentially actionable because of the predicted activation of mammalian target of rapamycin signaling and possible increased sensitivity to mammalian target of rapamycin inhibitors such as everolimus . 
forty - eight percent ( 22 of 46 ) of tested cases had mutations involving the pi3k pathway , 4.3% ( two of 46 ) involving raf kinases , and 4.3% ( two of 46 ) involving cdk inhibitors , which is similar to previous studies.7 other potentially actionable mutations identified included targets of existing anticancer therapies such as egfr , erbb2 , and kit . 
ras / raf pathway abnormalities and cdk mutations were also seen in a subset of patients ; there were agents targeting these pathways in clinical testing or approved for melanoma treatment at the time patients were enrolled in our biopsy protocol . 
despite 31 of 46 patients ( 58% ) having a theoretically actionable mutation , true actionability was limited because only two of 46 of our patients ( 4% ) were prescribed agents that could block the identified gene alteration . 
possible reasons include the lack of information on the importance of these mutations in crpc and the lack of insurance coverage to prescribe these medicines for off - label uses in patients with crpc . 
this lack of insurance coverage is probably because of the absence of positive basket trials showing a benefit of molecularly guided therapy versus standard therapies.15 moreover , lack of nearby or onsite clinical trials with these abbreviations : crpc , metastatic castration - resistant prostate cancer ; ecog , eastern cooperative oncology group ; psa , prostate - specific antigen . obtaining adequate tumor from patients with metastatic crpc , particularly those with bone metastases , has been notoriously difficult.11 - 13 however , nearly 80.0% of our biopsy specimens had sufficient dna for tumor sequencing , including 71.0% of bone biopsy specimens . 
finally , many of the patients in our study had not exhausted all of the approved therapies for metastatic crpc . this was also probably a contributing factor to why so few patients with theoretically actionable molecular alterations received molecularly guided therapy . pi3k / akt / pten pathway abnormalities were quite common in our cohort , and both subjects who received molecularly guided therapy received a pi3k inhibitor . 
the first patient progressed immediately ( ie , as of the first assessment ) , and his progression - free survival with molecularly guided therapy was nearly identical to that with his immediate prior therapy . 
moreover , we did not have ontreatment biopsies or progression biopsies during pi3k inhibitor treatment , so we are unable to determine whether the drugs adequately hit the fig 4 . 
swimmer plots illustrating patients time on treatment of the therapy given immediately before molecular testing and time on treatment with a phosphatidylinositol 3 - kinase ( pi3k ) inhibitor that was guided by molecular testing . 
radiographic progression was the reason for treatment discontinuation in all cases . 14 weeks 8 weeks enzalutamide 11 weeks docetaxel carboplatin 19 weeks prior therapy pi3k inhibitor radiographic progression time on therapy ( weeks ) target in each subject . 
finally , prior work has shown that pi3k inhibition leads to reciprocal feedback and activation of the ar pathway.16 indeed , the subject who did not respond to pi3k inhibition had an adenocarcinoma , whereas the patient who seemed to derive greater benefit from pi3k inhibitor treatment had an arnegative neuroendocrine tumor . 
thus , it is possible that the latter patient did not have adaptive ar activation in response to pi3k inhibition . finally , because our targeted panel only examined 37 genes for mutations , we cannot rule out the possibility that the first , nonresponding patients tumor had additional genomic abnormalities that were more consequential than his pik3ca mutation and pten loss . 
functional testing in tumor avatars from metastatic biopsies may help clarify the importance of molecular alterations found in tumor biopsy specimens , and we are currently developing these cultures from metastatic biopsy samples . 
finally , it is unclear if intrapatient tumor heterogeneity with clones that did not harbor a pik3ca mutation or pten loss also contributed to disease progression in the first subject . our panel included only 37 genes , which was another limitation of our study . 
since adoption of the panel used in this study , robinson et al7 have performed exome sequencing of metastatic crpc tumors and identified additional genes frequently altered in metastatic crpc . 
in that report , robinson et al7 reported that 89% of patients with crpc harbored a clinically actionable mutation . however , upon examination of the mutations that were identified , it is uncertain what proportion of these identified alterations could truly be used to guide therapy . 
indeed , 63% of patients had genetic alterations of the ar pathway ; however , it is unclear which therapies should be used in men who harbor these genetic alterations of the ar pathway . 
moreover , several of the other genetic alterations described in that report are not readily targetable ( ie , wnt pathway , cell cycle pathway , p53 alterations )  . 
similarly , we report finding a mutation in 67% ( 31 of 46 ) of our patients , with 58% ( 18 of 31 ) harboring at least one potentially actionable mutation ( ie , a drug was either approved or in clinical testing to block that genetic alteration )  . 
subsequent work has demonstrated a low frequency of ar mutations , including activating ar f877l mutations in this patient population.17 moreover , robinson et al reported that a high proportion of tumors among patients with crpc ( 19.3% ) harbored aberrations in dna repair pathway genes such as brca2 , brca1 , or atm . 
those patients whose tumors harbored mutations or copy number loss of these and other related dna repair genes seemed to have the greatest benefit.18 on the basis of the frequency with which these abnormalities are found in crpc , we anticipate that we would have identified 10 additional subjects with an actionable alteration if our panel had included mutational and copy number testing for genes in the dna repair pathway . 
recently , we expanded our mutational panel to include dna repair genes with the hope that we identify patients who may benefit from poly ( adp - ribose ) polymerase inhibitor or platinumbased therapy . importantly , even with more comprehensive sequencing panels , many hurdles related to access to therapy must be overcome to make molecular testing truly actionable . 
both of the patients in our cohort who had therapy guided by molecular testing results enrolled in clinical trials with investigational agents , and one patient traveled out of state several hundred miles to receive his therapy . 
one solution to this is single - patient investigational new drug applications for compassionate use , although that process is time consuming and requires dedicated staff to assist with these requests . tumors from other patients had molecular abnormalities that could have been targeted with an existing approved agent . 
insurance company disapproval was one reason ; thus a critical aspect of making molecular abnormalities actionable is insurance approval for unapproved uses of existing anticancer drugs . we are in a new era of cancer treatment , wherein molecular testing of tumors is commonplace . 
foster honoraria : civco medical solutions molecular testing in patients with castration - resistant prostate cancer and its impact on clinical decision making the following represents disclosure information provided by authors of this manuscript . 
tao no relationship to disclose shawna bailey research funding : janssen research & development ( inst ) , medivation ( inst ) , millennium ( inst ) , aragon pharmaceuticals ( inst ) , bristol - myers squibb ( inst ) , oncogenex ( inst ) , astellas scientific & medical affairs ( inst ) , bayer ( inst ) , myriad genetics ( inst ) , sotio ( inst ) , sanofi ( inst ) , zenith epigenetics ( inst ) , boehringer ingelheim pharmaceuticals ( inst ) , merck ( inst ) tomasz m . 
beer stock and other ownership interests : salarius pharmaceuticals consulting or advisory role : astrazeneca , churchill pharmaceuticals , dendreon , janssen biotech , janssen oncology , janssen research & development , johnson & johnson , janssen japan , roche research funding : astellas pharma ( inst ) , bristol - myers squibb ( inst ) , dendreon ( inst ) , janssen research & development ( inst ) , medivation ( inst ) , oncogenex ( inst ) , sotio ( inst ) , sotio , theraclone sciences ( inst ) , boehringer ingelheim ( inst ) erik foss research funding : coinvestigator for a research grant from moximed for magnetic resonance imaging of potential and postoperative patients undergoing kinespring knee implant surgery ( an orthopedic implant designed to alleviate degenerative joint pain )  . brooke beckett no relationship to disclose alice fung speakers bureau : guerbet affiliations alexander guimaraes honoraria : philips healthcare 2015 ( $1 , 500 ) ; siemens medical solutions 2014 ( $2 , 000 ) speakers bureau : siemens medical solutions 2014 travel , accommodations , expenses : siemens medical solutions 2014 , philips healthcare 2015 jeremy p . 
graff honoraria : bayer , astellas medivation , janssen oncology consulting or advisory role : exelixis research funding : sanofi ( inst ) , medivation ( inst ) , bristol - myers squibb ( inst ) , merck sharp & dohme ( inst ) , janssen oncology ( inst ) patents , royalties , other intellectual property : oncoresponse : exceptional responders travel , accommodations , expenses : bayer , merck sharp & dohme , clovis oncology kristine m . 
small stock and other ownership interests : fortis therapeutics , harpoon therapeutics honoraria : janssen - cilag consulting or advisory role : fortis therapeutics , gilead sciences research funding : janssen ( inst ) christopher l . 
alumkal consulting or advisory role : astellas pharma , bayer research funding : aragon pharmaceuticals ( inst ) , astellas pharma ( inst ) , millennium ( inst ) , novartis ( inst ) , zenith epigenetics ( inst ) derrick l . 
small , university of california , san francisco , san francisco , ca . support supported by a stand up to cancerprostate cancer foundation prostate dream team translational cancer research grant ( su2c - aacr - dt0409 )  . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors based on molecular profiles : early results from mypathway , an open - label , phase iia umbrella basket study . 
cheng hh , klemfuss n , montgomery b , et al : a pilot study of clinical targeted next generation sequencing for prostate cancer : consequences for treatment and genetic counseling . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
mckay rr , zukotynski ka , werner l , et al : imaging , procedural and clinical variables associated with tumor yield on bone biopsy in metastatic castration - resistant prostate cancer . 
spritzer ce , afonso pd , vinson en , et al : bone marrow biopsy : rna isolation with expression profiling in men with metastatic castration - resistant prostate cancerfactors affecting diagnostic success . 
ross rw , halabi s , ou ss , et al : predictors of prostate cancer tissue acquisition by an undirected core bone marrow biopsy in metastatic castration - resistant prostate cancera cancer and leukemia group b study . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
azad aa , volik sv , wyatt aw , et al : androgen receptor gene aberrations in circulating cell - free dna : biomarkers of therapeutic resistance in castration - resistant prostate cancer . 
specific molecular abnormalities identified and pten expression status ( continued ) patient no . biopsy site sample identifier loss of pten expression by ihc testing ( indicated by x ) bone bone dtb - oh - 181 dtb - oh - 187 lymph node dtb - oh - 190 bladder dtb - oh - 200 liver dtb - oh - 202 abbreviation : ihc , immunohistochemistry . abnormality rb1 copy number loss ( t3 )  . pten copy number loss ( t2 )  . 
staging magnetic resonance imaging ( mri ) of the pelvis conrmed a large inltrative tumor 6 cm from the anus ; no metastases were detected in the thorax plus abdominal computed tomography ( ct ) scans . 
at this point , all ras and brafv600e mutational analysis by quantitative polymerase chain reaction did not reveal alterations . the patient then started chemotherapy with modied uorouracil , folinic acid and oxaliplatin regimen plus panitumumab . 
cytoreductive surgery was undertaken in march 2017 and the pathologist reported a 2.5 - cm , mucinous adenocarcinoma extensively invading the mesorectum , with a focus of adenocarcinoma in the resection margin , regression grade 5 ( american joint committee on cancers ajcc cancer staging manual , 7th edition , classication : ypt4bn2amx , r1 )  . one year later , ct scans showed progressive disease with pelvic lymph node metastasis and a peritoneal lesion with secondary left uretero - hydronephrosis . second - line chemotherapy with folinic acid plus uorouracil plus irinotecan hydrochloride plus aibercept was started in july 2018 , but progressive disease was documented in october 2018 . 
he signed an informed consent form authorizing molecular prescreening and use of de - identied clinical and molecular data for research purposes and clinical trial matching . we conducted an in - house , targeted , amplicon - based , 60 - gene next - generation sequencing ( ngs ) test that covers the most frequently mutated genes in colorectal cancer.1 apc , ras , and braf genes were wild type , but we found mutations in tp53 ( p.k132r ) , rnf43 ( p.a19fs ) , and notch1 ( p.v1578del ; table 1 )  . 
but we complemented the genomics proling with a customized in - house fusion panel that was negative for translocations involving 19 genes , including clinically validated targets ( e.g. , alk , ros1 , ntrk ) as well as fusions in notch1 , notch2 , and wnt pathway genes rspo2 and rspo3 . 
the case was then discussed at the institutional molecular tumor board meeting to dene potential matched targeted therapeutic strategies for notch1 and / or rnf43 mutations . first , we assessed the functionality of the mutations , per oncokb ( a precision oncology knowledge database ) .2 both notch1 and tp53 variants have been reported as oncogenic in different databases , whereas the rnf43 mutation is a novel frameshift the coding sequence . event predicted to disrupt variant allele fractions ( vaf ) of notch1 , rnf43 , and tp53 were 3% , 53% , and 53% , respectively , suggesting that notch1 mutation might be a subclonal event , while rnf43 and tp53 mutations are clonal ( truncal ) events ( table 1 )  . 
it is known that in - frame mutations in the negative regulatory region , where p.v1578del is located , lead to ligand - independent notch1 activation through continuous cleavage of the receptor , allowing the migration of the notch intracellular domain to the nucleus and subsequent pathway activation.3 we decided to complement genomic analysis with notch1 immunohistochemistry to get additional insights on its functionality and subclonality . in line with ngs results showing low vaf of the mutation , less than 1% of cancer cells stained positive for notch1 ( table 1 )  . 
a previous study with transcriptomic and phosphoproteomic proling showed deregulation of the notch pathway in this context.4 whether a notch inhibitor has antitumor activity in the anti - egfr refractory setting with emerging notch1 subclonal mutations is unknown . 
we have previously shown no association between vafs of kras , braf , or pik3ca mutations and time to progression on targeted therapies matched to these alterations in metastatic colorectal cancer , potentially related to the limited antitumor activity of the used drugs.1 loss - of - function mutations in the ubiquitin ligases rnf43 are early drivers in colorectal cancer carcinogenesis ; they activate the wnt / - catenin pathway in a ligand - independent manner.5 rnf43 is a negative wnt feedback regulator , and preclinical models of rnf43 mutated cancers are sensitive to inhibitors of the wnt secretion porcupine.6 these mutations are strongly enriched but not restricted to hypermutated microsatellite instable tumors . 
notably , a patient with rnf43 - mutated colorectal cancer had partial response to the rst - in - man porcupine inhibitor wnt974 as monotherapy.7 this agent is not in clinical investigation in colorectal cancers any longer ; there has been a shift toward combination strategies with immuno - oncology drugs in tumors where wnt activation has been reported to induce immunosuppression and checkpoint inhibitor resistance , such as melanoma . 
other agents potentially active in a wnt hypersensitive context , characterized by mutations in rnf43 / znfr3 or gain - of - function chromosome translocations involving rspo2 and rspo3 ( and lacking downstream apc inactivating mutations ) , include antibodies targeting wnt receptor lrp5 / 6.8 , 9 given the clonality and predicted truncal driverness of rnf43 mutation and the absence of apc alterations , we decided to prioritize a phase i clinical trial with a rstin - class lrp5 / lrp6 antagonist bi 905677 ( clinicaltrials.gov identier : nct03604445 )  . 
at our institution , we consider novel therapies guided by molecular proling in patients with good performance status before the use of regimens known to have small response rates in unselected populations . 
clonality may be used to guide target prioritization when the level of evidence for actionability of the co - existing alterations is comparable ( clinical trial matching with investigational agents , as in this case )  . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . guillem argiles consulting or advisory role : hoffman la roche , bristol - myers squibb , roche , bayer , servier travel , accommodations , expenses : bayer , roche , amgen , servier analia azaro consulting or advisory role : orion , amcure elena garralda consulting or advisory role : roche , ellipses pharma , neomed therapeutics , janssen , boehringer ingelheim , astrazeneca / medimmune , seattle genetics , tfs speakers bureau : msd oncology , bristol - myers squibb research funding : novartis travel , accommodations , expenses : bristol - myers squibb , menarini , glycotope , merck sharp & dohme josep tabernero consulting or advisory role : bayer , boehringer ingelheim , eli lilly , msd oncology , merck serono , novartis , sano , taiho pharmaceutical , merrimack , peptomyc , rafael pharmaceuticals , symphogen , chugai pharma , ipsen , merus , pzer , seattle genetics , array biopharma , astrazeneca , beigene , genentech , genmab , halozyme , imugene , inection biosciences , kura , menarini , molecular partners , pharmacyclics , proteodesign , roche , seattle genetics , servier , vcn biosciences , biocartis , foundation medicine , haliodx sas , roche diagnostics paolo nuciforo honoraria : bayer , novartis , msd oncology consulting or advisory role : bayer , msd oncology travel , accommodations , expenses : novartis ana vivancos consulting or advisory role : guardant health , novartis , bayer health rodrigo dienstmann consulting or advisory role : roche speakers bureau : roche , ipsen , sano , symphogen , amgen , msd oncology , servier research funding : merck no other potential conicts of interest were reported . acknowledgment any views , opinions , ndings , conclusions , or recommendations expressed in this material are those solely of the author ( s ) and do not necessarily reect those of european society for medical oncology or any pharmaceutical company . references 11 : 1263 - 1272 , 2017 1 . 
brijwani n , jain m , dhandapani m , et al : rationally co - targeting divergent pathways in kras wild - type colorectal cancers by canscript technology reveals tumor dependence on notch and erbb2 . 
nat genet 46 : 1264 - 1266 , 2014 van de wetering m , francies he , francis jm , et al : prospective derivation of a living organoid biobank of colorectal cancer patients . 
cell 161 : 933 - 945 , 2015 janku f , connolly r , lorusso p , et al : phase i study of wnt974 , a rst - in - class porcupine inhibitor , in advanced solid tumors . 
 diamond - blackfan anemia predisposing to myelodysplastic syndrome in early adulthood diamond - blackfan anemia ( dba ) is an inherited bone marrow failure syndrome ( ibmfs ) , characterized by congenital pure red cell aplasia typically presenting within the first months of life.1 - 4 hematologic abnormalities in dba include macrocytic or normocytic anemia and normocellular bone marrow with scarce erythroid precursors , often associated with short stature and phenotypic anomalies including craniofacial , musculoskeletal , and cardiac malformations.1 - 5 the most common pattern of inheritance is autosomal dominant , observed in 40% to 45% of cases with a frequency of two to seven cases per one million live births.2 - 5 establishing the diagnosis of classic dba is based on criteria originally described by diamond et al , 5a which included age younger than 1 year and the aforementioned hematologic abnormalities , without other significant cytopenias.5 supportive criteria include a family history , an elevated erythrocyte adenosine deaminase level , and / or an elevated fetal hemoglobin level at diagnosis ; confirmation is now possible by molecular identification of ribosomal protein mutations associated with dba.1 - 5 the most frequent ribosomal protein gene mutation is rsp19 , accounting for almost 25% of cases.6 , 7 other heterozygous mutations identified include the rps24 , rps17 , rpl5 , rps10 , rpl11 , rpl35a , rpl15 , and rps26 genes.7 , 8 overall ,  . 
11 different ribosomal gene mutations are linked to dba , accounting for approximately 70% of cases.2 , 9 , 10 the preferential sensitivity of erythroid precursors to constitutional ribosomal mutations represents a complex and multifactorial pathophysiology , which remains incompletely understood . 
potential mechanisms have been recently reviewed in detail and include impaired erythroid differentiation and increased erythroid apoptosis.2 , 11 - 14 mutations in ribosomal proteins lead to indirect and excessive activation of p53 , which is implicated in increased erythroid precursor apoptosis2 - 4 via inhibition of the p53 - degradation protein ( the murine double minute 2 protein ) .15 , 16 other mechanisms include reduced levels of mrna translation , which affect the expression of critical erythroid proteins.1 , 3 current treatment options for dba include recurrent red - cell transfusions , corticosteroid therapy , and allogeneic stem - cell transplant in refractory cases . 
herein , we describe the cases of two adult patients referred to our institution at the time of early - onset mds and diagnosed with dba related to a constitutional disease - associated mutation or deletion of rps19 . case 1 a 44 - year - old woman was referred for pancytopenia and fatigue . 
dinardo author affiliations and support information ( if applicable ) appear at the end of this article . the views expressed in the article are the views of the authors and do not reflect an official position of the institution . corresponding author : courtney d . 
one month before presentation , a blood count showed a hemoglobin level of 5.6 g / dl , a platelet count of 91 3 103 / ml , and a wbc count of 3.0 3 103 / ml . 
she was referred to our institution , where a repeat hematology evaluation confirmed pancytopenia with mean corpuscular volume 110 fl , and anisocytosis and ovalocytes were identified on manual review . 
blasts were not increased , and no ring sideroblasts or reticulin fibrosis was detected ( fig 1 )  . findings fulfilled diagnostic criteria of mds with multilineage dysplasia.20a a 28 - gene mutation analysis was negative for somatic mutations , including aslx1 , idh1 , idh2 , jak2 , kit , n / kras , nmp1 , tet2 , and tp53 . 
conventional cytogenetics demonstrated a diploid female karyotype ; array comparative genomic hybridization was negative for copy number losses or gains in chromosomes 5 , 7 , 8 , 17 , or 20 . 
he did not require additional therapy , and his counts stabilized throughout adulthood without additional therapy . at age 30 years , he was reportedly diagnosed with hemochromatosis and treated with periodic phlebotomies . 
patient 1 : ( a ) the bone marrow trephine biopsy demonstrated a hypercellular marrow . ( b ) bone marrow aspirate smears demonstrated dysplasia involving the megakaryocytic and erythroid lineages predominantly . 
a 28 - gene somatic mutation analysis identified a tp53 missense mutation in exon 8 and an asxl1 frameshift mutation in exon 12 ; no additional mutations were detected ( fig 2 )  . 
he was given hypomethylating agent therapy with intravenous azacitidine 75 mg / m2 daily for days 1 to 5 , which he has received for three cycles . discussion the development of mds in patients with dba was summarized in 2010 by shimamura and alter.19 their systematic review of 970 patients found 13 cases of aml and / or mds . 
in their prospective cohort of 63 patients , no cases of leukemia were found after 6 years and 1 , 449 person - years of followup.19 in 2012 , vlachos et al20 reviewed the dbar , which included a cohort of  . 
in the dbar , the rate of mds / aml was approximately 1% ( six of 608 cases ) after 20 years and 9 , 458 person - years of follow - up.20 the median age was 28 years at the time of mds development ( range , 2 to 51 years ) and 44.5 years for aml ( range , 44 to 45 years )  . 
overall , these patients had a 287 - fold increased risk of developing mds and a 29.7 - fold risk of developing aml.20 an updated review of the dbar in 2016 revealed that of 702 patients with  . 
12 , 000 person - years of followup , three patients had developed aml and eight had developed mds.21 there is no evidence of specific association of any particular dba genotype with a cancer type or frequency.21 mds is typically a disease of advanced age , with a median age at mds diagnosis of 76 years.20a , 23 in fig 2 . 
 contrast , hereditary predisposition syndromes are associated with the development of mds at a younger age.19 recognizing a genetic predisposition to malignancy has major implications for risk stratification and treatment decisions , such as selection of appropriate transplant donors and reduced - intensity conditioning regimens . 
other advantages include augmented cancer surveillance and genetic testing for patients and at - risk family members.24 , 25 proposed guidelines to identify potential hereditary predisposition syndromes in mds include age at diagnosis of younger than 50 years with either a family history of aml / mds or a personal history of cytopenias ; bleeding tendencies ; skin , skeletal , or nail abnormalities ; unexplained liver disease ; or pulmonary fibrosis and / or alveolar proteinosis.24 the majority of patients with ibmfs , including dba , are diagnosed during childhood with hematologic abnormalities and recognizable phenotypes ; however , some patients with milder expression of disease have subtle extrahematopoietic findings that are ultimately only identified after diagnosis with mds , aml , or solid tumors.24 , 25 as somatic and germline genetic analysis becomes more widely available , we can better identify patients with ibmfss ( eg , fanconi anemia , dyskeratosis congenita , shwachman - diamond syndrome , and dba ) in those with hematologic malignancies at earlier ages , particularly using next - generation gene panel sequencing of predisposition genes.24 , 25 the cumulative malignancy risk of nearly 20% by the age of 40 years , and the 287 - fold increase in lifetime risk of mds with dba , approaches that of other ibmfss . 
bannon no relationship to disclose rashmi kanagal - shamanna no relationship to disclose jessica shafer foglesong no relationship to disclose yesid alvarado no relationship to disclose gautam borthakur no relationship to disclose courtney d . 
fumagalli s , di cara a , neb - gulati a , et al : absence of nucleolar disruption after impairment of 40s ribosome biogenesis reveals an rpl11 - translation - dependent mechanism of p53 induction . 
lee h , lyssikatos c , atsidaftos e , et al : remission in patients with diamond blackfan anemia ( dba ) appears to be unrestricted by phenotype or genotype . 
sj ogren se , siva k , soneji s , et al : glucocorticoids improve erythroid progenitor maintenance and dampen trp53 response in a mouse model of diamond - blackfan anaemia . 
vlachos a , rosenberg ps , kang j , et al : myelodysplastic syndrome and gastrointestinal carcinomas characterize the cancer risk in diamond blackfan anemia : a report from the diamond blackfan anemia registry . 
babushok dv , bessler m : genetic predisposition syndromes : when should they be considered in the work - up of mds ? best pract res clin haematol 28 : 55 - 68 , 2015 25 . 
kutler di , singh b , satagopan j , et al : a 20 - year perspective on the international fanconi anemia registry ( ifar )  . blood 101 : 1249 - 1256 , 2003 29 . 
dores gm , devesa ss , curtis re , et al : acute leukemia incidence and patient survival among children and adults in the united states , 2001 - 2007 . 
this is reflected in the current national comprehensive cancer network ( nccn ) guidelines , which state that genetic testing for brca1 / brca2 should be offered to patients with pdac with close relatives with a brca - associated cancer or to those of ashkenazi jewish ( aj ) ancestry.3 , 4 in the nccn guidelines that focus specifically on pdac , recommendations for genetic evaluation are broad , which suggests that those patients with early - onset pdac , a family history of cancer , or aj ancestry should be referred for genetic counseling.4 the rapidly evolving era of precision oncology , as well as the observation that some of these underlying germline variants are clinically actionable , raises the question of whether our current testing criteria are sufficiently inclusive . 
the three articles that accompany this editorial highlight the importance of germline testing and the need for a broader approach for genetic risk assessment in pdac . to better understand the prevalence of germline mutations in pdac , smith et al5 evaluated germline susceptibility in a high - risk group of patients with pdac who were known to harbor founder mutations . 
the authors assessed 150 patients with pdac with french canadian ( fc ) ancestry for both germline fc founder and nonfounder mutations in four dna - damage repair genesbrca1 , brca2 , palb2 , and atmcomparing mutation rates with 236 patients who were not selected for fc ancestry.5 among the fc group , a 5.3% founder mutation rate was observed . 
for nonaj or - fc patients , the authors suggest that full analysis of the aforementioned genes should be completed in patients with pdac who are diagnosed at age < 50 years or who have a strong family history of hrd - related cancers.5 these recommendations somewhat parallel the current expanded nccn guidelines , with the additional consideration of fc ancestry given the comparable germline mutation rates in fc and aj founder populations . alicia latham schwark zsofia k . 
 in contrast , in the article by reiss et al , 8 the authors suggest that a lower threshold for germline assessment of brca1 , brca2 , and palb2 in patients with pdac may be warranted . 
in this retrospective analysis , clinical outcomes , including overall survival ( os ) and response to chemotherapy , of 29 patients with advanced pdac with known pathogenic variants in brca1 , brca2 , or palb2 were compared with 58 stage , age at diagnosis , year of diagnosis , and gender matched controls.8 improved os was observed in hrd mutationpositive patients who received platinumbased therapy , specifically with 1 - year os in mutation - positive patients being 94% compared with 60% in the control group.8 of importance , mutation status did not predict an improved os in the nonplatinum group.8 this suggests that hrd mutation status may be predictive of the response to platinum therapy , but , by itself , may not be a prognostic marker , although additional studies are needed for clarification . 
interestingly , patients who were at higher risk of harboring a genetic mutation on the basis of clinical parametersthat is , young age , strong family history of cancer , or aj ancestrywere not the majority of patients who were found to have germline alterations , and , therefore , most mutation - positive patients with pdac did not meet current nccn guidelines for testing.8 this is similar to another study that suggested that the majority of brca mutationpositive patients with pdac do not meet traditional testing criteria.7 given the improved os in platinum - treated hrd mutationpositive patients , as well as the lack of clinical parameters that accurately identify hrd mutation carriers , either upfront germline testing or reflex germline assessment after suggestive tumor testing was recommended.8 a potential alternative to germline testing is the development of specific mutation signatures that predict for hrd . 
in the study by shahda et al , 11 91 tumor samples were assessed for an hrd score , with an immediate dropout of 34 samples that failed analysis as a result of low tumor cellularity , 11 which highlights the difficulty in assessing pancreatic tumor tissue for genetic information . 
70% of pdacs , respectively.14 , 18 , 19 given the lack of clinically actionable somatic driver mutations in pdac , it would then seem that an approximate 5% germline mutation prevalence in unselected , nonfounder populations in hrd - associated genes , with implications for treatment , 14 , 19 may be our most promising tool yet for pdac precision oncology . 
in light of the recent us food and drug administration approval of immune checkpoint inhibitors , such as pembrolizumab , for the treatment of all mismatch repair deficient solid tumors , 20 whether evaluation for mismatch repair deficient statuspresent in approximately 1% of pdacsis also warranted remains another important consideration.12 , 19 , 21 , 22 such genomic assessment may seem daunting . there may be concern that the overall burden of testing all pdacs for germline variants is unreasonable . 
 ovarian cancer for brca1 / 2 and colorectal cancer for lynch syndrome , recently updated nccn guidelines now also recommend that all patients with metastatic prostate cancer be referred for genetic evaluation and consideration of testing for brca and related genes.3 this is on the basis of the recent finding that 5% to 11% of such patients harbor underlying germline genetic mutations in dna repair genes , with both prognostic and predictive implications.23 in contrast to prostate cancer , the vast majority of patients with pdac succumb to their disease , with a 5 - year survival of only 8% , which highlights the critical need for identifying opportunities for precision oncology for all patients with pdac.24 , 25 given the dearth of clinically actionable somatic mutations in pdac , as well as our inability to accurately capture all hrdpdacs on the basis of clinical variables , universal germline genetic assessment to identify , at minimum , the 5% of hrdpdacs with emerging treatment and targeted therapy implicationsseems to be a clinically reasonable undertaking . 
beyond the opportunity for precision oncology , knowledge of the presence of an inherited cancer predisposition syndrome will allow for the incorporation of precision prevention oncology for at - risk family members . 
stadler consulting or advisory role : allergan ( i ) , genentech ( i ) , regeneron ( i ) , optos ( i ) , adverum ( i ) alicia latham schwark no relationship to disclose affiliations alicia latham schwark and zsofia k . 
smith al , wc , cuggia a , et al : reflex testing for germline brca1 , brca2 , palb2 and atm mutations in pancreatic cancer : mutation prevalence and clinical outcomes from two canadian research registries . 
telli ml , timms km , reid j , et al : homologous recombination deficiency ( hrd ) score predicts response to platinum - containing neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
domchek sm , aghajanian c , shapira - frommer r , et al : efficacy and safety of olaparib monotherapy in germline brca1 / 2 mutation carriers with advanced ovarian cancer and three or more lines of prior therapy . 
 o duodenal - jejunal flexure gi stromal tumor frequently heralds somatic nf1 and notch pathway mutations purpose gi stromal tumors ( gists ) are commonly associated with somatic mutations in kit and pdgfra . 
we define the anatomic distribution of nf1 alterations in gist . methods we describe the demographic / clinicopathologic features of 177 patients from two institutions whose gists underwent next - generation sequencing of 315 cancer - related genes . results we initially identified six ( 9.7% ) of 62 gists with nf1 genomic alterations from the first cohort . 
of the five djf gists with any nf1 alteration , three ( 60% ) had kit mutations , and three ( 60% ) had notch pathway mutations ( notch2 , maml2 , cdc73 )  . 
we validated these findings in a second cohort of 115 gists , where two ( 40% ) of five unifocal nf1 - mutated gists arose at the djf , and one of these also had a notch pathway mutation ( ep300 )  . conclusion broad genomic profiling of adult gists has revealed that nf1 alterations are enriched in djf gists . 
 ( ie , kras , nras , hras ) by increasing the catalytic conversion of the active form ( ras - gtp ) to the inactive form ( ras - gdp ) .14 pathogenic nf1 variants disrupt the normal function of neurofibromin and result in constitutive ras activation.15 this activation increases downstream signaling through braf / craf - mediated activation of the mitogen - activated protein kinase pathway and hence , facilitates tumor initiation and progression.16 until recently , nf1 mutations in gist were believed to be primarily of germline origin , associated with clinical nf - 1 , and combined with a second somatic mutation in the tumor . 
thus , our understanding of nf1 in gist continues to evolve . approximately 30% of all gists occur in the small intestine , 1 which measures approximately 5 to 6 m in length.18 most small bowel gists are associated with somatic kit mutations , whereas a subset is associated with nf1 mutations.19 the small bowel is divided into three anatomically , histologically , and functionally distinct segments , namely the duodenum , jejunum , and ileum.18 although some studies distinguish duodenal gists from other small bowel gists , most combine them and do not characterize the biology of tumors on the basis of these distinct locations . 
moreover , the exact transition from jejunum to ileum is somewhat arbitrary , but the duodenal - jejunal flexure ( djf ) , also known as the ligament of treitz , represents a clear anatomic site that marks the transition from duodenum to jejunuto date , no study of gists has specifically characterized tumors that arise from the djf . 
the current study , however , started with presumably sporadic gists , which led to the unexpected finding that somatic nf1 mutations in gists are more prevalent than previously suspected and that they are enriched in tumors that arise from the djf . methods primary study population patient demographic and tumor clinicopathologic data were retrospectively collected in an unbiased fashion from every patient with pathologically confirmed gist seen within the university of california , san diego ( ucsd ) , health system from january 1 , 2000 , to april 30 , 2017 , under a ucsd institutional review boardapproved protocol . 
available operating notes or imaging reports were reviewed for these 165 patients to distinguish the primary site of origin of any small bowel gist as duodenal , djf , jejunal , or ileal . comprehensive genomic profiling of the 165 patients with gist in the cohort , 62 underwent next - generation sequencing ( ngs ) of coding regions of cancer - related genes . 
dna was extracted from formalin - fixed paraffin - embedded ( ffpe ) sections that contained a minimum of 20% tumor tissue and were used for comprehensive genomic profiling with hybridization - captured , adaptor ligationbased libraries . 
the number of genes in the foundationone panel has evolved over time as new data on cancer - related genes have been published and currently includes 315 cancerrelated genes plus select introns from 28 genes often rearranged or altered in solid tumor cancers . however , all versions of the assay simultaneously analyze the extracted dna for base substitutions , short insertions and deletions , amplifications and homozygous deletions , and gene rearrangements with > 99% sensitivity.20 specimens submitted to the ucsd clinical genomics laboratory underwent ngs of the exons of 397 genes involved in pathways that control growth or differentiation and are known to be frequently mutated in solid tumors . 
coverage depth ranged from 2833 to 8303 across all sequenced tumor samples from both the foundationone and the ucsd assays . nontumor tissue sequencing patients found to have nf1 mutations in their tumor tissue were also tested for germline nf1 mutation . four samples tested by using dna extracted from ffpe sections of adjacent normal tissue or peripheral blood underwent ngs cancer - related mutation panel testing by the ucsd clinical genomics laboratory as just described . 
one additional sample was tested by using commercially available targeted sequencing of the nf1 gene from peripheral blood by arup laboratories ( salt lake city , ut )  . secondary study population a confirmatory cohort of  . 
1 , 000 patients with pathologically confirmed gists from memorial sloan kettering cancer center ( mskcc ) with retrospectively collected patient demographic and tumor clinicopathologic data also were analyzed under an institutional review boardapproved protocol . 
data included age , sex , primary gist site , tumor size , and pathologic characteristics . one hundred fifteen patients with gists had ngs results available in the msk - impact ( integrated mutation profiling of actionable cancer targets ) platform , which characterized frozen or ffpe tumor specimens for somatic dna mutations , copy number alterations , and select rearrangements of 341 cancer - associated genes.21 statistical analysis all statistical analyses were performed with stata 9.0 software ( statacorp , college station , tx )  . comparisons between groups were performed by using the two - sample test of proportions . 
none of these patients had previously known clinical manifestations of nf - 1 ( eg , cafe au lait spots ; axillary / inguinal freckling ; dermal neurofibromas ; lisch nodules ; iris hamartomas ; nervous system tumors , including malignant peripheral nerve sheath tumors [ mpnsts ] , pancreatic neuroendocrine tumors , pheochromocytomas , or other sarcomas ] ) .10 therefore , the application of expanded ngs panels to characterize the mutational profile of gists identified an unappreciated subset of patients with nf1 genomic alterations in their tumors but no clinical evidence of nf - 1 . nf1 genomic alterations in gist frequently occur at the djf of the six patients with gist for whom we identified nf1 genomic alterations , five ( 83.3% ) had unifocal tumors at the djf , and one ( 16.7% ) had a unifocal tumor in the stomach ( fig 1a )  . 
the demographic , clinicopathologic , and genomic characteristics of these nine patients with djf tumors are listed in table 1 ( n = 7 ngs gists ) and the data supplement ( n = 2 non - ngs gists )  . 
given the infrequency of nf1 genomic alterations in gist , the djf appears to be an over - represented focus of nf1 mutant tumors . nf1 genomic alterations in gist are primarily somatic but can herald mild neurofibromatosis nf1 genomic alterations for each patient are listed in table 2 . 
although none of the patients had known prior clinical evidence of nf - 1 , we next obtained nontumor dna from blood or nontumor tissue to determine whether any of these patients had germline nf1 mutations . 
 ( a ) from a total of 165 patients ( university of california , san diego [ ucsd ] ) with pathologically confirmed gists , 62 had available next generation sequencing ( ngs )  . 
this finding is consistent with the mild phenotype / low penetrance reported in other patients with this germline nf1 mutation.22 nf1 genomic alterations in gists are associated with other cancer - related mutations at the genomic level , the ucsd cohort ngs data generally parallel the known distribution of driver mutations in gists ( fig 2 )  . 
of the 65 driver mutations identified in the 62 gists , oncogenic kit ( 63% ) , pdgfra ( 11% ) , and sdh subunit ( 11% ) mutations were most frequent , whereas braf and kras mutations were less common . moreover , nf1 mutations ( six of 65 ) represented 9% of total genomic alterations . 
the loss of the nf1 tumor suppressor gene often leads to additional chromosomal alterations , but second - hit mutations and / or loss of heterozygosity are necessary to promote tumorigenesis.23 therefore , we analyzed a cohort of five patients with nf1 mutant djf gists for additional cancer - related gene mutations . 
demographic and clinicopathologic characteristics of these two patients are listed in table 3 , with the characteristics of the remaining five patients without djf and / or multifocal gists listed in the data supplement . 
in addition to an nf1 mutation , one patient had a concomitant mutation in ep300 , which encodes a histone acetyltransferase / transcriptional coactivator that has been previously reported to interact with maml1 and maml2 to potentiate notch signaling.24 this supports our earlier observation that unifocal nf1 mutant djf gists also can have impaired notch signaling . 
in summary , 40% of unifocal nf1 mutant gists in the mskcc cohort were localized at the djf , which corroborates the high rate ( 83.3% ) of similar tumors in the ucsd cohort . 
we now show in two single - institution cohorts of patients with gists that 6.1% ( mskcc , seven of 115 ) to 9.7% ( ucsd , six of 62 ) have nf1 alterations . 
if we exclude the 17 patients who overlap with our previous study ( two of whom have nf1 mutations [ ucsd patients 3 and 5 in the current study ] ) , we show that 8.9% ( four of 45 ) of patients with gists have nf1 alterations . 
taken together , nf1 mutation frequencies range from 6% to 10% in gist and are higher than previously appreciated but similar to our recent analysis.7 for the first time in our knowledge , we show that broad genomic profiling of djf or ligament of treitz gists in adults reveals frequent nf1 alterations ( somatic and / or germline ) that occur even in the absence of clinical nf - 1 . 
 yes high high high high pathologic feature tumor resection yes tumor size , cm 13 mitotic index / 5 mm2 high cellular morphology mixed spindle / epithelioid histologic grade g2 immunostain positivity dog - 1 genomic alterations somatic kit ( af ) kit exon somatic nf1 ( af ) ( 30% ) none other somatic alterations ( af ) none table 2 . 
of the 62 patients with gi stromal tumors with available next generation sequencing , 65 known driver mutations were identified : 41 in kit , seven in pdgfra , six in nf1 , seven in succinate dehydrogenase ( sdh ) subunits ( a , b , c , or d ) , two in braf , and two in kras . awareness of the risk of additional tumors ( eg , dermal neurofibromas , nervous system tumors [ including mpnsts , pancreatic neuroendocrine tumors , pheochromocytomas , and other sarcomas ] ) 10 and allows for earlier screening of these nf - 1associated tumors , although whether different malignancies and gists have unique presentation patterns remains to be determined ; and diagnosis of nf - 1 allows for genetic counseling and testing of potentially affected family members . 
of note , individuals can have segmental mosaicism of nf - 1 , which occurs when an nf1 somatic mutation occurs early in embryonic development such that only the tissues derived from the nf1 - mutated cell carry the mutation while the remaining tissues are wild type.26 as with ucsd patient 2 , a clinical genetics work - up may be indicated for patients with nf1 mutations on tumor profiling that could indicate a germline rather than a somatic origin . tumor development in the setting of nf1 genomic alterations is associated with additional second - hit mutations.23 we now have shown that djf tumors with nf1 genomic alteration also can harbor concurrent kit mutations . 
in general , most kit mutations portend imatinib sensitivity , whereas nf1 mutations do not.3 , 27 consistent with this aforementioned drug sensitivity , tumors with a high risk of recurrence are recommended for adjuvant imatinib on the basis of the american college of surgeons oncology group z900128 and scandinavian sarcoma group xviii / aio29 trials where cumulative results demonstrated improved relapse - free survival ( rfs ) and overall survival with 36 months of adjuvant imatinib in patients with high - risk disease . 
in our cohort , three patients with djf gists had a high risk of recurrence by validated risk assessment models.30 , 31 ucsd patient 4 lacked a kit mutation and was predicted to not respond to imatinib therapy ; instead , this patient could experience toxicity . 
this approach was supported by eortc - 62005 and southwest oncology group s0033 / cancer and leukemia group b 150105 phase iii trials that collectively demonstrated improved response rates and rfs in patients with advanced gists and kit exon 9 mutations treated with high - dose imatinib ( 800 mg daily ) compared with standard - dose imatinib ( 400 mg daily ) .32 the patient also had a germline nf1 variant and ultimately developed a local recurrence after 5 years of adjuvant imatinib therapy . ucsd patient 3 had a known kit exon 11 mutation and was treated with dose - escalated imatinib followed by the multikinase inhibitor sunitinib for metastatic disease . 
a brief trial of the mammalian target of rapamycin inhibitor everolimus in combination with imatinib was attempted to block parallel signaling pathways , but the patient rapidly succumbed to the disease . much like patients with metastatic colorectal cancer who are tested for pan - ras mutations before treatment targeting upstream cell surface receptors ( ie , epidermal growth factor receptor ) , 33 , 34 we propose that patients with djf gists be tested for nf1 ( which would activate ras ) and braf v600e genomic alterations ( which two of the patients with djf gists also harbored ) before being offered imatinib therapy , which targets upstream kit . we have recently shown that notch1 can be mutated in both wild - type and nonwild - type gists.7 we now add evidence that implicates the notch signaling pathway in gists . 
we identified another tumor with a mutation in cdc73 , which encodes the rna polymerase iiassociated factor complex protein parafibromin and was recently reported to potentiate notch signaling by binding to the nicd.36 we also found an ep300 mutation in the validation cohort that could abrogate signaling of the notch transcriptional complex . of note , notch signaling was reported to have a tumor suppressor function in gist by downregulating kit mrna expression.37 this prior study also demonstrated that patients with gists with low hes1 expression had shorter rfs times than those with high hes1 expression . whether loss - of - function mutations in notch pathway genes that lead to decreased hes1 expression contribute to gist tumorigenesis remains to be determined . 
nf1 regulates mek / smad3 / jagged1 / hes1dependent glial and neuronal differentiation.38 notch has also been reported to mediate transformation of benign plexiform neurofibromas into mpnsts in the setting of nf - 1 , 39 which suggests an alternate oncogenic role of notch in nf - 1 . 
more studies are required to elucidate the biologic significance of notch pathway mutations in gist , including nf - 1associated gist . finally , the mechanism by which nf1 mutations lead to gists that specifically arise at the djf remains unclear . 
summary of duodenal - jejunal flexure genomic alterations . tumor size , mitotic index ( mi ) , and genomic alterations for patients with duodenal - jejunal flexure gi stromal tumors ( gists ) from both cohorts are presented and organized by known driver genes and notch pathway alterations . somatic and germline mutations are annotated by color for mutation type . snp , single nucleotide polymorphism . cdc73 ep300 notch2 maml2 asxl1 men1 erbb4 tsc2 bcor ( per 5 mm2 ) high unknown genomic alteration nonsense frameshift missense in - frame indel deletion splicing ( somatic ) ( germline ) ( somatic ) braf ( somatic ) arid1a ( somatic ) notch pathway other pacemaker activity.42 one could postulate that this region of chromatin on 17q is open and transcriptionally active at the djf . 
belinsky no relationship to disclose margaret von mehren consulting or advisory role : cytrx , blueprint medicines , janssen pharmaceuticals , deciphera pharmaceuticals research funding : arqule travel , accommodations , expenses : janssen pharmaceuticals , blueprint medicines , novartis , arog pharmaceuticals other relationship : national comprehensive cancer network john a . 
thorson no relationship to disclose lisa madlensky employment : janssen pharmaceuticals ( i ) patents , royalties , other intellectual property : husband has patents through his employment with janssen pharmaceuticals ; these are methods patents and not related to any therapeutics ( i ) timothy bowler employment : regenxbio ( i ) stock and other ownership interests : regenxbio ( i ) francesco dangelo no relationship to disclose dwayne g . 
sicklick , university of california , san diego , la jolla , ca ; martina de siena and francesco dangelo , sapienza e universit `a di roma , rome , italy ; benjamin medina , timothy bowler , and ronald p . 
ma gl , murphy jd , martinez me , et al : epidemiology of gastrointestinal stromal tumors in the era of histology codes : results of a population - based study . 
hechtman jf , zehir a , mitchell t , et al : novel oncogene and tumor suppressor mutations in kit and pdgfra wild type gastrointestinal stromal tumors revealed by next generation sequencing . 
burgoyne am , somaiah n , sicklick jk : gastrointestinal stromal tumors in the setting of multiple tumor syndromes . curr opin oncol 26 : 408 - 414 , 2014 11 . 
belinsky mg , rink l , cai kq , et al : somatic loss of function mutations in neurofibromin 1 and myc associated factor x genes identified by exome - wide sequencing in a wild - type gist case . 
miettinen m , fetsch jf , sobin lh , et al : gastrointestinal stromal tumors in patients with neurofibromatosis 1 : a clinicopathologic and molecular genetic study of 45 cases . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
messiaen l , vogt j , bengesser k , et al : mosaic type - 1 nf1 microdeletions as a cause of both generalized and segmental neurofibromatosis type - 1 ( nf1 )  . 
dematteo rp , ballman kv , antonescu cr , et al : adjuvant imatinib mesylate after resection of localised , primary gastrointestinal stromal tumour : a randomised , double - blind , placebo - controlled trial . 
gastrointestinal stromal tumor meta - analysis group ( metagist ) : comparison of two doses of imatinib for the treatment of unresectable or metastatic gastrointestinal stromal tumors : a meta - analysis of 1 , 640 patients . 
pietrantonio f , cremolini c , petrelli f , et al : first - line anti - egfr monoclonal antibodies in panras wild - type metastatic colorectal cancer : a systematic review and meta - analysis . 
sorich mj , wiese md , rowland a , et al : extended ras mutations and anti - egfr monoclonal antibody survival benefit in metastatic colorectal cancer : a meta - analysis of randomized , controlled trials . 
a 5 - hmc model predicting outcome in high - risk patients was established using linear discriminant analysis . results comparison of lowversus high - risk tumors in the discovery cohort revealed 577 genes with differential 5 - hmc . 
hierarchical clustering of tumors from the discovery and validation cohorts using these genes identied two main clusters highly associated with established prognostic markers , clinical risk group , and outcome . genes with increased 5 - hmc and expression in the favorable cluster were enriched for pathways of neuronal differentiation and kras activation , whereas genes involved in inammation and the prc2 complex were identied in the unfavorable cluster . 
this technology has shown dynamic alterations in 5 - hmc patterns in rare hematopoietic cell populations.3 , 4 furthermore , nano - hmc - seal requires as little as 100 ng of dna from frozen tissue , enabling analysis of clinical samples with limited available tissue . 
more recently , 5 - hmc signatures in cell - free dna have been generated and shown to be robust diagnostic biomarkers for adult human cancer.5 , 6 neuroblastoma is characterized by a broad spectrum of clinical behavior , reecting its biologic heterogeneity.7 a combination of clinical and biologic prognostic markers , including age , stage , mycn status , ploidy , and histology , is used to classify risk and stratify treatment of patients with neuroblastoma . 
 applebaum et al context key objective recently , 5 - hydroxymethylcytosine ( 5 - hmc ) proles have been developed as a diagnostic biomarker for adult malignancies . to investigate the prognostic value of this dna modication in neuroblastoma , we applied nano - hmc - seal , a revolutionary , low - cost , genome - wide technology that requires minimal input dna , to prole 5 - hmc in 109 tumors . knowledge generated grouping of all tumors using genes with differential 5 - hmc in the discovery cohort identied two clusters highly associated with established prognostic markers , clinical risk - group , and outcome . 
using 5 - hmc levels in high - risk patients from the discovery cohort , we developed an outcome prediction model that successfully identied events an independent cohort ( n = 24 ) of high - risk patients . relevance 5 - hmc proling could provide information on factors that determine the clinical behavior of neuroblastoma ( ie , mycn status , copy number alterations , and transcriptional networks ) using one simple assay . 
ongoing efforts include prospectively testing the prognostic value of 5 - hmc proles from tumors and cell - free dna . disease , outcomes remain poor for high - risk ( hr ) patients , with fewer than half achieving long - term survival.7 signicant heterogeneity exists within hr tumors , 7 and new biomarkers are needed to distinguish patients who will respond to standard treatments from those who may benet from alternative approaches . 
clinical data for the cog cohort were extracted from the international neuroblastoma risk group database.7 differences in clinical and tumor characteristics were evaluated with fishers exact tests and t tests for categorical and continuous variables , respectively . 
all protocols were approved by local institutional review boards . nano - 5 - hmc - seal library preparation and sequencing nano - hmc - seal libraries were constructed from 100 ng of genomic dna , as described.3 , 4 fifty base - pair , paired - end libraries were sequenced on an illumina nextseq 500 ( san diego , ca )  . 
differences between log - transformed quantity of 5 - hmc between risk groups according to genomic feature were assessed by paired t tests with benjamini - hochberg correction.12 cpg islands were downloaded from the university of california , santa cruz , genome browser , and cpg shores were dened as 2 - kb regions adjacent to each cpg island . 
enhancer regions were annotated from prior studies in neuroblastoma cell lines from the enhancer atlas13 and van groningen et al.14 chromosomal copy number evaluation dna from hr tumors was analyzed using the oncoscan affymetrix microarray platform , following the manufacturers instructions ( affymetrix , santa clara , ca )  . 
read counts of 5 - hmc for the entire gene body and rna sequencing ( rna - seq ) across exons were loaded into the deseq2 v1.20.018 package in r , version 3.5.0 ( r project , old / 3.5.0 / ) with a model that adjusted for sex and batch . 
sensitivity and specicity were determined for the validation cohort.22 matthews correlation coefcients ( mcc ) were generated to determine the t of the model.23 similar to other correlation statistics , a score of 1 denotes a perfect model . 
kaplan - meier curves and hazard ratios were generated according to predicted event and survival status in prism , version 6.0h ( graphpad software , san diego , ca )  . results patient characteristics and outcome the discovery cohort included 51 patients with lr ( n = 24 ) , ir ( n = 11 ) , and hr ( n = 16 ) tumors . 
for the 36 lr patients with evaluable outcomes , the 5 - year eventfree survival ( efs ) was 94.4% ( se , 3.8% ) and the overall survival ( os ) was 100% . 
because of the unique biology conferred by amplication of the mycn oncogene , 25 we compared the accumulation of gene body 5 - hmc in the eight mycn - amplied hr tumors with accumulation in the 24 lr tumors , and then analyzed 5 - hmc levels in the eight non - mycnamplied hr tumors compared with the same lr tumors ( data supplement )  . hierarchical clustering of the pooled discovery and validation tumors ( n = 89 lr , ir , and hr tumors ) using these 577 genes revealed two primary clusters that correlated highly with prognostic markers , clinical risk group , and outcome ( fig 2a )  . 
among the ve ir patients in cluster 2 , three had an event and two died , which highlights the potential for 5 - hmc proles to rene risk stratication . 
because chromosomal aberrations vary according to mycn status , we conducted copy number analysis on nine available hr tumors from the discovery cohort , ve of which were mycn amplied and four were non - mycn amplied . 
interestingly , 131 ( 88.5% ) of the 148 genes were located on chromosome 1p , suggesting nano - hmc - seal has the potential to identify copy number alterations within tumor subsets . 
chromosome 1p contains several genes with important biologic including chd5 , casz1 , functions in neuroblastoma , arid1a , and mtor ( fig 3b - 3e ) .27 increased 5 - hmc was also detected in several additional genes in tumors with chromosome 1p loss , including tumor - promoting genes abcg1 and s100b mapping to chromosome 21q . gene expression , 5 - hmc levels , and cellular pathway analysis to further explore the biology of cluster 1 and cluster 2 tumors , we examined the 3 , 320 genes with differential 5 - hmc between these tumors ( data supplement )  . 
genes with elevated 5 - hmc in cluster 1 , compared with cluster 2 tumors , showed enrichment for gene ontology ( go ) pathways of neuronal differentiation , similar to prior analysis of genes expressed in lr tumors.28 also identied were oncogenic signatures of activated kras signaling and suppression of bmi1 and mel18 , integral components of the polycomb repressive complex 1 ( prc1 )  . 
in contrast , cluster 2 tumors had elevated 5 - hmc compared with cluster 1 tumors in genes enriched for pathways of an inammatory response and oncogenic signatures including activation of ezh2 and the prc2 complex , transcriptional networks reported previously in hr tumors ( fig 4a and 4b ) .29 because 5 - hmc is a marker of transcriptional activation , we performed rna - seq on one hr , 11 ir , and 17 lr tumors from cluster 1 and 17 hr and three lr tumors from cluster 2 ( data supplement )  . 
genes with increased expression in cluster 1 were highly represented for neuronal differentiation . in cluster 2 , overexpressed genes were enriched for pathways of embryo development and morphogenesis ( data supplement )  . differential 5 - hmc was assessed in these same 48 tumors , identifying 2 , 722 genes that met signicance and ltering criteria ( data supplement )  . 
to estimate the degree of sharing between genes with differential 5 - hmc and expression , we extracted the rna - seq differential fold change and calculated the p value for each of the genes with signicantly differential 5 - hmc.30 using the 1 statistic , 24 we estimated that 62% of the 2 , 722 genes with signicantly differential 5 - hmc were also differentially expressed between the two clusters . 
 a applebaum et al cohort age at diagnosis event survival mycn risk cohort discovery validation age at diagnosis < 12 months 12 - 18 months 19 months to 5 years > 5 years event unknown survival alive deceased unknown mycn nonamplified amplified unknown risk cohort 1 cohort 2 p < .001 years since diagnosis cluster 1 cluster 2 p < .001 years since diagnosis no . 
 ( a ) clustering of nine hr tumors with known copy number at chromosome 1p . genes with differential 5 - hmc predominate on chromosome 1p , highlighting the underlying chromosomal aberration . 
 ( b - e ) genome browser views of 5 - hmc signals detected in four genes ( chd5 , casz1 , arid1a , mtor ) with known biologic functions in neuroblastoma , illustrating decreased 5 - hmc in tumors with chromosome 1p aberrations that likely modulate tumor biology . 
pathway enrichment analysis for differentially regulated genes from cluster 1 and cluster 2 tumors . genes with increased 5hmc in cluster 1 tumors were enriched for gene ontology ( go ) pathways of neuronal differentiation and oncogenic signatures of activated kras signaling and genes that are regulated by bmi1 and mel18 . ( b ) cluster 2 tumors had increased 5 - hmc in genes enriched for go pathways of an inammatory response . 
 5 - hydroxymethycytosine proling in neuroblastoma tumors and oncogenic signatures of activated kras signaling . cluster 2 tumors were enriched for go pathways of embryo development and morphogenesis and oncogenic signatures including activation of il - 2 , il - 15 , and the prc2 complex ( fig 4c and 4d )  . predicted event predicted no event 5 - hmc as a predictive biomarker of outcome in hr patients we performed an exploratory evaluation of 5 - hmc levels as a prognostic marker for patients classied as hr ( data supplement )  . 
the lda model trained on hr patients in the discovery cohort based on their os correctly predicted efs in 18 of 24 patients from the combined validation and cog cohorts . 
in contrast , cluster 2 contained the majority of tumors that were clinically classied as hr ( 27 of the 29 evaluated ) , ve ir tumors , and ve lr tumors . 
three of the ve ir patients in cluster 2 relapsed and two died , suggesting 5 - hmc proles may provide additional prognostic information in these non - highrisk cohorts . we also demonstrate 5 - hmc levels may be prognostic of efs but not os in hr patients . 
 ( a ) event - free survival was signicantly better for patients who were predicted not to have an event , although no signicant difference in ( b ) overall survival was observed in those predicted to be alive or not . esophageal , pancreatic , liver , and colon cancers.5 , 35 to our knowledge , this is the rst study to show that gene - specic 5 - hmc proles may also be prognostic of patient outcomes . chromosomal copy number variation is commonly detected in neuroblastoma , and patterns of chromosomal aberrations are strongly prognostic of survival.26 we show for 5 - hmc proling to identify segmental the potential chromosomal aberrations without the need for additional testing . 
 applebaum et al there is increasing evidence that 5 - hmc plays an important role in activating transcription , and that variation in 5 - hmc positively correlates with gene expression levels.4 we found many genes with both increased expression and 5 - hmc , which is consistent with other tumor types.3 , 4 in the favorable cluster 1 tumors , we found go enrichment of neuronal differentiation from the genes with increased in 5hmc and expression . 
neuronal differentiation is a hallmark of lr tumors , 38 and studies indicate hras expression drives this phenotype.39 pathway analysis also suggested a role for the prc1 complex , which promotes gene silencing by monoubiquitinating histone 2a.40 additional efforts are needed to conrm our ndings , which could provide additional evidence for targeting bmi1 in neuroblastoma.41 in the unfavorable cluster 2 tumors , we found that the genes with increased 5 - hmc and expression were enriched for prc2 complex target genes . 
upregulation of ezh2 , an integral part of leads to the transcriptional repression of differentiation genes and maintains stem - like cell properties.42 recent studies have established the prc2 complex has high - binding afnity for the prc2 complex , methylated cytosines , 43 making a direct connection between histone and dna epigenetics.44 in addition , ezh2 is integral to the biology of hr neuroblastoma and considered a potential therapeutic target in the disease.45 can rapidly nano - hmc - seal identify 5 - hmc levels genomewide , using a cost - effective sequencing approach that requires low sample input and no specialized biospecimen handling . 
although a number of prognostic gene expression signatures have been validated in neuroblastoma , 28 , 46 - 48 these biomarkers have not been integrated into the clinic , in part because of challenges obtaining high - quality rna from diagnostic tumor samples . moreover , neuroblastoma tumorigenesis and phenotype are thought to be driven by epigenetic reprogramming , 49 driving the need for new epigenetic biomarkers . 
5 - hmc proling could provide information on factors that determine the clinical behavior of neuroblastoma : mycn status , copy - number alterations , and transcriptional networks , using one simple assay . 
k12ca139160 and k08ca226237 ( m.a.a. ) , and national institutes of health grants 1ul1tr002389 - 01 and 5ul1tr002389 - 02 that fund the university of chicago institute for translational medicine . 
the international neuroblastoma risk group ( inrg ) database is supported in part by the william guy forbeck research foundation , st baldricks foundation , little heroes cancer research fund , childrens neuroblastoma cancer foundation , neuroblastoma childrens cancer foundation , super jake foundation , and alexs lemonade stand foundation . 
 5 - hydroxymethycytosine proling in neuroblastoma tumors robert grossman stock and other ownership interests : tempus health , healthseq consulting or advisory role : healthseq research funding : abbvie lucy a . 
godley honoraria : agios patents , royalties , other intellectual property : royalties from uptodate , inc . chuan he stock and other ownership interests : accent therapeutics , epican genetech consulting or advisory role : accent therapeutics patents , royalties , other intellectual property : wisegene licensed tab - seq from the university of chicago susan l . 
cohn stock and other ownership interests : united therapeutics ( i ) , varian medical systems ( i ) , united therapeutics , vermillion , resmed ( i ) , merck ( i ) , merck , stryker ( i ) , stryker , amgen ( i ) , pzer ( i ) , abbvie , amgen , jazz pharmaceuticals , eli lilly , sano , varex imaging , pzer , united therapeutics ( inst ) , merck ( inst ) no other potential conicts of interest were reported . acknowledgment we thank the center for research informatics of the university of chicago for use of the gardner high - performance computing cluster and the cancer center support grant ( p30 ca014599 ) for support of the genomics core facility . 
we thank the childrens oncology group ( cog ) neuroblastoma biobank for providing dna specimens and arlene naranjo at the cog statistics and data center for support . the contents are solely the responsibility of the authors and do not necessarily represent the ofcial views of the national institutes of health . references vasanthakumar a , godley la : 5 - hydroxymethylcytosine in cancer : signicance in diagnosis and therapy . 
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oberthuer a , juraeva d , hero b , et al : revised risk estimation and treatment stratication of lowand intermediate - risk neuroblastoma patients by integrating clinical and molecular prognostic markers . 
nature 431 : 873 - 878 , 2004 infante jr , bedard pl , shapiro g , et al : phase 1 results of ptc596 , a novel small molecule targeting cancer stem cells ( cscs ) by reducing levels of bmi1 protej clin oncol 35 : 2574 , 2017 ( 15_suppl ) 42 . 
oberthuer a , juraeva d , li l , et al : comparison of performance of one - color and two - color gene - expression analyses in predicting clinical endpoints of neuroblastoma patients . 
marachelian a , villablanca jg , liu cw , et al : expression of ve neuroblastoma genes in bone marrow or blood of patients with relapsed / refractory neuroblastoma provides a new biomarker for disease and prognosis . 
 novel alk fusion , ppfibp1 - alk , in pancreatic ductal adenocarcinoma responsive to alectinib and lorlatinib arjan gower , md , ms1 ; barry golestany , md2 ; jun gong , md3 ; aatur d . 
singhi , md , phd4 ; and andrew eugene hendifar , md , mph3 introduction pancreatic cancer is the seventh leading cause of cancer death among men and women worldwide , with  . 
430 , 000 deaths in 2018.1 despite advances in surgical techniques , radiation , and systemic treatment in the past few decades , overall survival for pancreatic cancer is extremely poor , with a 5 - year survival rate of 9%.2 current systemic treatment regimens for metastatic pancreatic cancer include folfirinox ( uorouracil , folic acid , oxaliplatin , and irinotecan ) , gemcitabine plus nab - paclitaxel , and liposomal irinotecan with uorouracil.3 - 6 approximately 88% - 95% of pancreatic adenocarcinomas harbor kras driver mutations . 
in row 1 , the circled hepatic lesion in the right lobe of the liver at baseline ( a ) before alectinib decreased in size ( b ) 2 months after alectinib . 
the patient experienced progression during alectinib treatment after 5 months and experienced progression during uorouracil , folic acid , oxaliplatin , and irinotecan treatment shortly thereafter . fluorescence in situ hybridization ( fish ) was negative . 
it has been shown that fish may have different sensitivities of detecting alk compared with next - generation sequencing or immunohistochemistry.27 of note , molecular proling was negative for kras , microsatellite instability , nf1 and p53 inactivating mutations , and cdkn2a / b loss . proling was positive for brca2 c.8007a.g ( silent ) and cdkn1b 407a.g , both of unknown clinical signicance . patient was started on folfirinox with radiographic response . 
however , because of the adverse effects of chemotherapy , including nausea and neuropathy , the patient was switched to alectinib 600 mg twice daily , given her alk fusion status . 
subsequent cell - free plasma ( guardant360 ; guardant health , redwood city , ca ) showed newly acquired alk mutations g1202r and v1180l in addition to the ppfibp1 - alk translocation . 
the patients disease has been stable on lorlatinib on 2 - month follow - up imaging , and she continues to be treated with lorlatinib ( figs 2 and 3 )  . discussion currently , there are no fda - approved targeted therapies for pancreatic cancer , and standard chemotherapy ( folfirinox ) for metastatic pancreatic cancer is quite toxic , with a median overall survival of approximately 11 months.3 to our knowledge , we present the seventh case of alk - positive metastatic pancreatic cancer with a novel ppfibp1 - alk fusion gene and the rst patient to be treated with alectinib as rst - line targeted therapy . 
the patient ultimately acquired alectinib - resistant alk mutations g1202r and v1180l ; however , the disease has been stable on the third - generation alk inhibitor lorlatinib . alk translocation in pancreatic cancer was rst described in 2017 , and there have been only 6 documented cases of alk - positive pancreatic adenocarcinoma through literature review ( table 1 )  . 
although the prevalence of the alk fusion gene is rare , at 0.16% , the prevalence increases to 1.3%.among patients , 50 years old12 the majority of alk fusion partners seen in nsclc includes eml4 , but other partners include strn , kcnq , klc1 , kif5b , ppm1b , and tgf genes.28 ppfibp1 - alk gene fusion was rst described in 2011 in a patient with pulmonary inammatory myobroblastic tumor29 and subsequently was described in epithelioid brous histiocytoma , 30 but it has never been described in nsclc or pancreatic cancer . 
of the 6 patients with alk - positive pancreatic cancer , 4 patients had eml4alk translocation , 1 patient had strn - alk , and 1 patient had a dctn1 - alk translocation ( table 1 )  . 
 case report 3 / 19 4 / 19 5 / 19 7 / 19 9 / 19 12 / 19 1 / 20 3 / 20 3w pain + bloating ; us , pet / ct : liver lesions folfirinox #2 - 6 ; dose reduction due to adverse effects ct imaging : stable disease biopsy with acquired resistance mutations ; progression on folfirinox #7 - 8 ; start lorlatinib biopsy : pancreatic adenocarcinoma ; folfirinox #1 ct imaging : stable disease ; start alectinib ct imaging : progressive disease ct imaging : stable disease inferior r hepatic lobe posterior r hepatic lobe folfirinox alectinib lorlatinib folfirinox 3 / 1 / 19 5 / 1 / 19 7 / 1 / 19 9 / 1 / 19 11 / 1 / 19 1 / 1 / 20 3 / 1 / 20 date fig 2 . 
# , dose number ; 3w , 3 - week ; ct , computed tomography ; folfirinox , uorouracil , folic acid , oxaliplatin , and irinotecan ; pet , positron emission tomography ; r , right ; us , ultrasound . and proliferative capabilities , ultimately leading to activation of different signaling pathways.28 in nsclc , alk fusion is an oncogenic driver that is generally mutually exclusive of kras mutation16 ; however , there are reports of concomitant kras and alk fusion double alteration that may confer worse prognosis.31 all 7 patients with alk - positive pancreatic cancer were kras wild type , suggesting , albeit in a small sample size , that alk translocation drives oncogenesis and that these 2 oncogenic drivers are mutually exclusive . 
this case demonstrates the rst time , to our knowledge , that alectinib has been used as the rst targeted therapy , and the development of known alectinib - resistant alk mutations suggests that alk - positive pancreatic cancer acquires resistance in a fashion similar to that of nsclc . there is a clear unmet medical need for novel therapeutic approaches in pancreatic cancer . 
a recent study in metastatic pancreatic cancer with germ - line brca mutations ( 7% prevalence ) regardless of kras mutation status showed increased pfs with the poly adp ribose polymerase inhibitor olaparib after rst - line platinum - based chemotherapy.4 in a recent phase ii basket study , 2 of 9 patients who had pancreatic cancer with her2 amplication / overexpression experienced responses to her2 - targeted therapies trastuzumab plus pertuzumab . 
additionally , a patient who had pancreatic cancer and braf gene fusion ( cux1 - braf ) had a partial response to the braf - targeted therapy vemurafenib.32 last , 3 patients who had pancreatic cancer with ntrk1 and ros1 gene fusions experienced responses to entrectinib , a targeted inhibitor of these genes.33 these studies are additional proof of concept that targeted therapies can be used successfully when paired with the right genomic alteration and that alk inhibitors may be of substantial clinical benet in the right patient . 
in row 1 , the circled hepatic lesion after disease progression on uorouracil , folic acid , oxaliplatin , and irinotecan ( a ) before lorlatinib was stable in size ( b ) 2 months after lorlatinib treatment . 
the patient currently continues to be treated with lorlatinib . 38% of kras wild - type tumors have genomic alterations that could activate the mapk signaling cascade.9 identication of molecular alterations in patients with kras wild - type status that may drive oncogenesis will help guide therapeutic intervention in a small but clinically relevant population . alk translocations are rare in pancreatic cancer . 
this is , to the rst report of ppfibp1 - alk rearour knowledge , rangement in pancreatic or nsclc , the rst reported patient with pancreatic cancer to be treated with alectinib as the rst targeted therapy , and the rst patient to be treated with lorlatinib after acquired resistance to alectinib with stabilization of disease . 
all 7 occurrences of alk - positive pancreatic cancer have been kras wild type ; given that 6 of the 7 patients were , age 50 years , there may be clinical benet to screen young patients with pancreatic cancer who are kras negative for the alk gene fusion , as they may benet from alk inhibitors , which may lead to improved overall survival . 
clinical characteristics of patients with alk - positive pancreatic cancer patient case age ( years ) alk rearrangement exon 13 eml4 - exon 20 alk ( 1 ) crizotinib ; ( 2 ) ceritinib ; ( 3 ) alectinib alk inhibitor ( in order of treatment ) ( 1 ) crizotinib ( 1 ) crizotinib unknown none ( 1 ) crizotinib ; ( 2 ) alectinib duration of survival ( months ) unknown unknown ppfibp1 - alk ( 1 ) alectinib ; ( 2 ) lorlatinib exon 6 eml4 - exon 20 alk exon 3 strn - exon 20 alk exon 6 eml4 - exon 20 alk exon 6 eml4 - exon 20 alk dctn1 - alk note . 
singhi , andrew eugene hendifar collection and assembly of data : arjan gower , barry golestany , andrew eugene hendifar data analysis and interpretation : arjan gower , jun gong , aatur d . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / authors / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . jun gong honoraria : amgen , astellas pharma , clinical congress consultants , qed therapeutics , exelixis , elsevier consulting or advisory role : amgen , astellas pharma , clinical congress consultants , qed therapeutics , exelixis , elsevier aatur d . 
singhi honoraria : foundation medicine andrew eugene hendifar consulting or advisory role : novartis , ipsen , perthera , celgene , abbvie research funding : ipsen travel , accommodations , expenses : halozyme no other potential conicts of interest were reported . references bray f , ferlay j , soerjomataram i , et al : global cancer statistics 2018 : globocan estimates of incidence and mortality worldwide for 36 cancers in 185 countries . 
ca cancer j clin 69 : 7 - 34 , 2019 conroy t , desseigne f , ychou m , et al : folfirinox versus gemcitabine for metastatic pancreatic cancer . 
n engl j med 364 : 1817 - 1825 , 2011 golan t , hammel p , reni m , et al : maintenance olaparib for germline brca - mutated metastatic pancreatic cancer . 
n engl j med 381 : 317 - 327 , 2019 von hoff dd , ervin t , arena fp , et al : increased survival in pancreatic cancer with nab - paclitaxel plus gemcitabine . 
wang - gillam a , li cp , bodoky g , et al : nanoliposomal irinotecan with uorouracil and folinic acid in metastatic pancreatic cancer after previous gemcitabinebased therapy ( napoli - 1 ) : a global , randomised , open - label , phase 3 trial . 
lancet 387 : 545 - 557 , 2016 biankin av , waddell n , kassahn ks , et al : pancreatic cancer genomes reveal aberrations in axon guidance pathway genes . 
nature 518 : 495 - 501 , 2015 singhi ad , george b , greenbowe jr , et al : real - time targeted genome prole analysis of pancreatic ductal adenocarcinomas identies genetic alterations that might be targeted with existing drugs or used as biomarkers . 
lin e , li l , guan y , et al : exon array proling detects eml4 - alk fusion in breast , colorectal , and nonsmall - cell lung cancers . 
kelly lm , barila g , liu p , et al : identication of the transforming strn - alk fusion as a potential therapeutic target in the aggressive forms of thyroid cancer . 
no e j , lovejoy a , ignatius ou , s - h , et al : alk mutation status before and after alectinib treatment in locally advanced or metastatic alk - positive nsclc : pooled analysis of two prospective trials . 
solomon bj , besse b , bauer tm , et al : lorlatinib in patients with alk - positive nonsmall - cell lung cancer : results from a global phase 2 study . 
zou hy , friboulet l , kodack dp , et al : pf - 06463922 , an alk / ros1 inhibitor , overcomes resistance to rst and second generation alk inhibitors in preclinical 27 . 
lin c , shi x , yang s , et al : comparison of alk detection by fish , ihc , and ngs to predict benet from crizotinib in advanced nonsmall - cell lung cancer . 
takeuchi k , soda m , togashi y , et al : pulmonary inammatory myobroblastic tumor expressing a novel fusion , ppfibp1 - alk : reappraisal of anti - alk immunohistochemistry as a tool for novel alk fusion identication . 
ulivi p , chiadini e , dazzi c , et al : nonsquamous , nonsmall - cell lung cancer patients who carry a double mutation of egfr , eml4 - alk or kras : frequency , clinical - pathological characteristics , and response to therapy . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecular proles : results from mypathway , an open - label , phase iia multiple basket study . 
 identifying erbb2 activating mutations in her2 - negative breast cancer : clinical impact of institute - wide genomic testing and enrollment in matched therapy trials pedro exman , md1 ; ana c . 
our primary aim was to describe the proportion of patients with a qualifying erbb2 mutation identied by our institutional genomic panel ( oncomap or oncopanel ) who enrolled in the trial . 
associations were calculated using fishers exact test . results we identied a total of 1 , 045 patients with metastatic breast cancer without erbb2 amplication who had available genomic testing results . 
of these , 42 patients were found to have erbb2 mutation and 19 patients ( 1.8% ) were eligible for the trial on the basis of the presence of an activating mutation , 18 of which were identied by oncopanel testing . 
fifty - eight percent of potentially eligible patients were approached , and 33.3% of eligible patients enrolled in the trial guided exclusively by oncopanel testing . conclusion more than one half of eligible patients were approached for trial participation and , signicantly , one third of those were enrolled in nct01670877 . 
 exman et al context key objective although tumor genomic sequencing has become more accessible , bridging the gap between patients with targetable mutations and recruitment to specic trials remains a challenge . 
this phase ii study has been active at dfci since 2013 , with consistent slot availability during this time . patients we included 1 , 817 patients in the profile cohort with mbc who had available genomic proling results between august 1 , 2011 , and june 1 , 2017 . 
from the ccpm cohort , we included patients with metastatic her2 - negative ( per ihc and / or fish ) breast cancer in whom targeted genomic panel results were available between june 22 , 2015 , and june we collected data on those patients who consented to be in the profile cohort and who had available oncomap or oncopanel . 
clinical data abstraction was performed via medical record review and included age and stage at initial diagnosis , date of recurrence , histologic features , and date of death or last follow - up . 
clinical her2 status was dened by the 2013 asco / college of american pathologists guidelines.7 survival data were collected through a combination of medical record review and linkage to the national death index . 
all data are stored in a custom redcap database . genomic analysis genomic testing was performed in a clia - certied environment within the center for advanced molecular diagnostics at brigham and womens hospital . 
 excluded patients with her2 - positive disease ( n = 772 ) profile cohort patients with mbc with at least one dfci visit and available oncopanel results between 2011 and 2017 ( n = 1 , 817 ) patients with er - positive / her2negative mbc with oncopanel result ( n = 1 , 045 ) patients with erbb2 mutation previously detected by other genomic test modality ( n = 1 ) erbb2 activating mutations in her2 metastatic breast cancer ccpm cohort patients with mbc with at least one dfci visit and available oncopanel results between 2015 and 2017 ( n = 194 ) excluded patients with her2 - positive disease ( n = 28 ) patients with her2negative mbc with oncopanel result ( n = 166 ) patients with erbb2 mutations ( n = 42 ) patients with eligible erbb2 mutations diagnosed by profile ( n = 18 ) patients approached by trial team after oncopanel result ( n = 11 ) patients approached by trial team after ccpm result ( n = 1 ) patients with eligible erbb2 mutations diagnosed by ccpm ( n = 6 ) patients with erbb2 mutations ( n = 10 ) patients enrolled on the basis of oncopanel results ( n = 6 ) patients enrolled on the basis of ccpm result ( n = 1 ) fig 1 . 
dfci , danafarber cancer institute ; er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; mbc , metastatic breast cancer . muther trial this multi - institutional phase ii clinical trial ( clinicaltrials.gov identier : nct 01670877 ) evaluates the efcacy of neratinib in patients with her2 - negative ( per ihc and / or fish ) , erbb2 - mutant mbc . 
the study opened to accrual at dfci on september 20 , 2013 , and it remains open as of december 18 , 2018 . trial matching in 2016 , we instituted several programs , such as the ending metastatic breast cancer for everyone ( embrace ) program for patients with mbc , 11 the matchminer platform , 12 and an interactive web - based trial - matching tool13 ( data supplement ) to assist physicians in trial selection . 
through these programs , key data from oncopanel ( derived either from the profile or ccpm protocols ) , as well as results from other research testing conducted in a clia - environment , were collated into a central database . the data supplement presents details of the embrace prograa custom report ( data supplement ) was shared with the medical oncologist by a designated research coordinator at the time of a patients visit to facilitate realtime trial matching . 
in addition , a custom query for erbb2 alterations was created within the matchminer platform and allowed for the identication of all patients with breast cancer with an erbb2 alteration at dfci . 
this list was used to reach out directly to treating physicians as an extra outreach method to capture patients who might not have a return visit to dfci scheduled . statistical analysis the primary objective of our study was to describe the proportion of patients in the prespecied profile cohort with eligible erbb2 mutations detected by genomic analysis who enrolled in the selected trial . 
secondary objectives included describing the proportion of patients approached for trial screening , the median time from genomic testing results to trial enrollment , the median time from genomic testing to death , and overall survival ( os )  . 
os was dened as the time from diagnosis of metastatic disease ( by imaging or biopsy ) to death from any cause and was estimated using the kaplan - meier method . 
between august 2011 and june 2017 , 1 , 045 patients with her2 - negative mbc consented to the profile protocol and had successful genomic testing . oncopanel was performed in most of the patients of this cohort ( 98.8% , n = 1 , 032 of 1 , 045 )  . 
forty - two patients ( 4.0% ) were found to have erbb2 mutations in their tumors , and of these , 19 ( 1.8% ) had mutations eligible for the trial ( 18 detected by oncopanel , none by oncomap , and one by commercial panel )  . 
between june 2015 and june 2017 , 166 patients with her2 - negative mbc underwent successful oncopanel testing of a fresh tumor biopsy as part of the ccpm initiative ( fig 1 )  . 
in terms of our prespecied primary end point , the proportion of patients with eligible erbb2 mutations who enrolled in the selected neratinib trial on the basis of only oncopanel results was 33.3% ( six of 18 ) , representing 0.5% of the total tested population ( six of 1 , 045 )  . 
one additional patient with a previously known erbb2 mutation detected through commercial testing enrolled in the neratinib trial ; another patient enrolled in the trial on the basis of testing of a fresh metastatic specimen collected in the ccpm protocol ( fig 1 )  . all patients who enrolled in the trial had other multiple mutations detected by oncopanel ( data supplement ) , but none received additional treatment guided by another specic mutation . 
for patients with eligible erbb2 mutations , the median os was not reached ( data supplement )  . among 1 , 045 patients with her2 - negative mbc with available genomic results between 2011 and 2017 and included in our profile cohort , we identied a total of 19 patients with erbb2 mutations that rendered them eligible for the neratinib trial . 
although the total number of enrolled patients ( n = 8 ) at dfci was low , our site was the second - highest accruing site nationally , reecting the low overall prevalence of erbb2 mutations in breast cancer . we observed that the conversion rate from genomic result to trial enrollment was numerically higher in the profile cohort compared with the ccpm cohort , although the patients in the ccpm cohort were not approached because they had stable disease on current therapy . 
patients who enrolled in the trial had received a median of four ( range , one to six ) lines of systemic treatment in the metastatic ( mets ) setting before oncopanel results were available . 
in addition , 75% ( six of eight ) of the registered patients were enrolled after the rst progression after the oncopanel result was available and 25% ( two of eight ) after the second progression . 
 erbb2 activating mutations in her2 metastatic breast cancer mutated and eligible mutated not mutated test technical lack of an adequate archival sample , insufcient archival material , or failure ( the last being uncommon )  . 
because patients were not randomly assigned to undergo testing , we cannot denitively comment on the impact of enterprise - wide testing versus an approach of more selective testing at the time of clinical need . 
the potential for referral bias , given the long median interval between initial metastatic diagnosis and oncopanel testing , and the possibility that only more t patients were able to travel to our site later in their disease course , could have diluted differences in survival by erbb2 mutation status . 
in addition , 20% of patients with eligible mutations were lost to follow - up . the rarity of the patient population meant that only 0.5% of the total tested population ultimately enrolled in the neratinib study . 
it is notable that the median time from metastatic diagnosis to oncopanel result in mutated patients was 7.0 months , and in large part , this reected patients being referred to our institution after having lived with a diagnosis of mbc for some time before their initial visit . our data illustrate the hurdles involved in identifying and enrolling patients with rare molecular alterations in clinical trials . 
we believe that our data suggest that broad - based testing , the development of systems with the ability to query genomic testing results across a clinic population , and robust strategies to approach patients will be critical to the success of studies enrolling rare subsets . 
1 , 000 women to enroll eight patients in the selected trial ; however , this testing simultaneously identied patients for multiple other trials , in a tissueand timeefcient manner . one half of the patients enrolled in the neratinib trial were also potentially eligible for other simultaneous trials on the basis of targetable mutations such as in palb2 or pik3ca ( data supplement )  . 
a direct assessment of the drug activity of neratinib ( with or without fulvestrant ) will be performed in the muther trial , and progression - free survival will be evaluated as a secondary end point.17 a strength of our study is the selection of a specic clinical trial with wide slot availability over an extended period to evaluate the conversion rate from biomarker result to trial enrollment . 
a slightly lower conversion rate was observed by wheler et al , 5 who prospectively evaluated 500 patients ( only 16% with breast cancer ) ; 22% of them received directly guided treatment after tumor molecular proling . 
meric - bernstam et al18 evaluated 2 , 000 patients with different cancer types ; 7% of patients with potentially actionable alterations were enrolled in a specic mutation - driven trial , and 4% were treated in a trial with a molecular rationale . 
the safir - 01 study enrolled 423 patients with advanced breast cancer , and 13% of them were considered eligible for a mutationguided clinical trial.3 our study has several limitations . 
although all new patients to dfci were approached for participation in the overarching protocol allowing for tumor testing , we did not prospectively collect the decline rate , nor did we collect reasons for decline . 
not all consented patients with mbc underwent tumor testing , for a variety of reasons , including affiliations 1dana - farber cancer institute , boston , ma 2washington university school of medicine , st . 
freedman research funding : puma biotechnology ( inst ) , eisai ( inst ) lorenzo trippa consulting or advisory role : galera therapeutics romualdo barroso - sousa consulting or advisory role : lilly speakers bureau : roche , bristol - myers squibb travel , accommodations , expenses : roche simona di lascio honoraria : roche / genentech ethan cerami stock and other ownership interests : blueprint medicines honoraria : merck travel , accommodations , expenses : merck margaret s . 
tolaney consulting or advisory role : novartis , pzer , merck , lilly , nektar , nanostring technologies , astrazeneca , puma biotechnology , genentech , eisai , immunomedics , sano , celldex , bristol - myers squibb , paxman , seattle genetics research funding : genentech / roche ( inst ) , merck ( inst ) , exelixis ( inst ) , pzer ( inst ) , lilly ( inst ) , novartis ( inst ) , bristol - myers squibb ( inst ) , eisai ( inst ) , astrazeneca ( inst ) , nanostring technologies ( inst ) , cyclacel ( inst ) , nektar ( inst ) , immunomedics ( inst ) travel , accommodations , expenses : astrazeneca , lilly , merck , nektar , novartis , pzer , genentech / roche , immunomedics , eisai , nanostring technologies , puma biotechnology , celldex ian e . 
krop employment : amag pharmaceuticals ( i ) leadership : amag pharmaceuticals ( i ) stock and other ownership interests : amag pharmaceuticals ( i ) honoraria : genentech / roche consulting or advisory role : genentech / roche , daiichi sankyo , context therapeutics , macrogenics , taiho pharmaceutical research funding : genentech / roche ( inst ) , seattle genetics ( inst ) , pzer ( inst ) , daiichi sankyo ( inst ) ron bose honoraria : genentech , foundation medicine consulting or advisory role : genentech research funding : puma biotechnology ( inst ) bruce e . 
johnson research funding : novartis ( inst ) , toshiba ( inst ) , novartis ( inst ) , novartis ( inst ) patents , royalties , other intellectual property : dana - farber cancer institute cynthia x . 
ma consulting or advisory role : pzer , novartis , syndax , lilly , biovica , tempus , seattle genetics , agendia , myriad genetics , lilly research funding : pzer ( inst ) , eisai ( inst ) , puma ( inst ) travel , accommodations , expenses : syndax , lilly , agendia , pzer deborah a . 
winer stock and other ownership interests : verastem honoraria : genentech / roche , tesaro , genomic health consulting or advisory role : leap therapeutics , seattle genetics , jounce therapeutics , glaxosmithkline , carrick therapeutics , lilly research funding : genentech ( inst ) , novartis ( inst ) , merck ( inst ) nikhil wagle stock and other ownership interests : foundation medicine honoraria : lilly consulting or advisory role : novartis , lilly research funding : novartis , puma biotechnology nancy u . 
 erbb2 activating mutations in her2 metastatic breast cancer acknowledgment we thank kaitlyn bifolck for her editorial support . references 5 , 2010 ] andre f , mardis e , salm m , et al : prioritizing targets for precision cancer medicine . 
gynecol oncol 148 : 585 - 590 , 2018 andr e f , bachelot t , commo f , et al : comparative genomic hybridisation array and dna sequencing to direct treatment of metastatic breast cancer : a multicentre , prospective trial ( safir01 / unicancer )  . 
lancet oncol 15 : 267 - 274 , 2014 schwaederle m , zhao m , lee jj , et al : impact of precision medicine in diverse cancers : a meta - analysis of phase ii clinical trials . 
cancer res 76 : 3690 - 3701 , 2016 sholl lm , do k , shivdasani p , et al : institutional implementation of clinical tumor proling on an unselected cancer population . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
plos one 4 : e7887 , 2009 [ erratum : plos one garcia ep , minkovsky a , jia y , et al : validation of oncopanel : a targeted next - generation sequencing assay for the detection of somatic variants in cancer . 
ramkissoon sh , bandopadhayay p , hwang j , et al : clinical targeted exome - based sequencing in combination with genome - wide copy number proling : precision medicine analysis of 203 pediatric brain tumors . 
hughes me , frank es , merrill ms , et al : embrace ( ending metastatic breast cancer for everyone ) : a comprehensive approach to improve the care of patients with metastatic breast cancer . 
lindsay j , del vecchio fitz c , zwiesler z , et al : matchminer : an open source computational platform for real - time matching of cancer patients to precision medicine clinical trials using genomic and clinical criteria . 
fish , phd1 , 3 , 4 introduction immune checkpoint inhibitors ( icis ) have signicantly improved advanced cancer outcomes.1 , 2 although icis unleash antitumor immune responses , negating natural immune inhibitory mechanisms can result in the development of self - reactive immune cells and an array of immune - related adverse events ( iraes ) .3 although reports of serious myocarditis have emerged , 4 - 9 data on long - term outcomes following an episode of ici - associated myocarditis are limited and molecular analyses on surviving patients are lacking . 
here , we report a case of recurrent myocarditis in a patient previously treated with a programmed death ligand 1 ( pd - l1 ) inhibitor ( durvalumab ) , an ici that blocks the binding of pd - l1 to programmed cell death protein 1 and cd80.10 molecular investigations revealed cytokine modulations suggestive of a sustained t - helper 1 ( th1 ) - like cellular immune response as well as unique antigen - bound serum autoantibodies , highlighting a induction of potential autoantibody production in iraes . role for th1 - cell - dependent case initial presentation a 67 - year - old woman presented to the emergency department with severe sudden - onset chest pain 2 days after receiving the 12th cycle of pd - l1 inhibitor ( 48 weeks after starting ici ) for the treatment of metastatic urothelial carcinoma ( fig 1a )  . 
she was previously treated for remote triple - negative right - sided breast invasive ductal carcinoma with surgery ; cyclophosphamide , epirubicin , and 5 - uorouracil chemotherapy ; and radiation . 
her treatment was largely uneventful , with only a noted diagnosis of hypothyroidism after receiving the 7th cycle of pd - l1 inhibitor , which was treated with hormone replacement therapy without interruption of ici . although the patient was hemodynamically stable , cardiac laboratory investigations revealed high - sensitivity troponin i levels were elevated at 4 , 114 ng per l ( reference range , , 26 ng per l ) , and brain natriuretic peptide levels ( bnp ) were elevated at 2 , 275 pg per ml ( reference range , , 100 pg per ml ) ( figs 1b and 1c , data supplement )  . 
2d echocardiogram demonstrated severely decreased biventricular systolic function , with a left ventricular ejection fraction ( lvef ) of 20% , right ventricular ( rv ) fraction area change of 22% , and a left ventricular ( lv ) thrombus ( fig 1d and video 1 )  . 
with a history of ici treatment , together with clinical , ecg ( fig 2a ) , and imaging ndings , a diagnosis of ici - associated myocarditis was made . 
treatment with intravenous methylprednisolone ( 2 mg / kg / d ) , furosemide , betablocker , angiotensin - converting enzyme inhibitor , and low - molecular - weight heparin was initiated . 
cardiovascular magnetic resonance ( cmr ) imaging conrmed severe biventricular dysfunction , mild pericardial effusion , and demonstrated late gadolinium enhancement ( lge ) involving the basal and apical segments predominantly in a subepicardial distribution ( video 2 , data supplement )  . 
follow - up ecg remained abnormal with low - voltage qrs complex as well as persistent st elevation ( fig 2b )  . the patient was discharged home in stable condition on 90 mg oral prednisone with a plan to taper and discontinue in 8 weeks . 
 echocardiogram ( apical the patient demonstrating four chamber view ) of biventricular dysfunction as well as a focused apex view with contrast showing a thrombus ( admission )  . case report evidence of pulmonary emboli , whereas whole - body computed tomography scanning showed no evidence of metastatic disease . 
there was signicant clinical recovery 1 month after discharge , with echocardiography revealing partial recovery of lv function ( lvef = 40% ; global longitudinal strain = 17.1% ) ; however , rv systolic function remained severely reduced ( rv fraction area change 17% , data supplement )  . 
ecg remained abnormal with low - voltage qrs , however , now with right bundle branch block ( fig 2c )  . recurrent presentation four months after the initial event , and without resumption of ici treatment , the patient presented to the cardiology clinic with extreme fatigue . 
she was admitted and a subsequent cmr conrmed the severity of lv dysfunction , multiple new lv thrombi , larger pericardial effusion , and a mild interval worsening of nonischemic pattern lge ( data supplement )  . a cardiac biopsy ( figs 2e and 2f ) conrmed the diagnosis of myocarditis with predominantly t cells ( fig 2g ) and macrophages ( fig 2h ) ; polymerase chain reaction was negative for cardiotropic viruses.11 given the biopsy result , she was diagnosed with recurrence of ici - associated myocarditis . 
she deteriorated and subsequently succumbed to heart failure a year - and - a - half later . methods the patient was enrolled in this research ethics boardapproved case report at the university health network after obtaining informed written consent . 
next - generation sequencing ( immunoseq ) , cytokine multiplex assays , targeted microrna proling , and a mass spectrometry - based assay to identify serum autoantibody complexes with their cognate antigens were performed ( for a detailed description of the methods , see the data supplement )  . results analysis of the distribution , clonality , and diversity of t - cell receptors pre - recurrence ( january ) and during treatment for recurrence of myocarditis ( march onward ) with immunosuppressants revealed limited clonal modulation ( data supplement )  . 
multiplex analysis of cytokines ( luminex , austin , tx ) in serum revealed remarkably high concentrations of t - cellderived cytokines during recurrence despite withdrawal of ici therapy and initiation of immunosuppressants . 
substratifying by t - helper ( th ) cell subtype revealed that there was an apparent dominance of th1 - cellenriched cytokines over th2 - cellenriched cytokines ( figs 3a and 3b ; data supplement )  . quantication of 92 micrornas ( fluidigm , san francisco , ca ) with known inammatory and cardiac roles revealed two micrornas ( mir - 130a - 3p and mir - 122 - 5 ) that displayed consistent upregulation and downregulation , respectively , in parallel with circulating cytokine abundance . 
increases in mir - 130a - 3p ( figs 3b and 3c ) appeared to correlate with declines in interleukin ( il ) - 4 , 12 whereas decreases in mir122 - 5p , a noted negative regulator of il - 1 , appeared to be associated with elevations in il - 1 ( figs 3a and 3c ) .13 principal component and pathway analysis of differentially regulated micrornas ( cross - timepoint comparison ) revealed modulation during treatment course ( data supplement )  . to assess the downstream effects of a potentially aberrant th1 cell response , we examined antigen - bound serum autoantibodies . 
it was noteworthy that the patient experienced hypothyroidism after receiving ici as we identied antithyroglobulin autoantibody across all sample collection points ( roche electrochemiluminescent assay ) ( data supplement )  . 
a mass spectrometry - based assay14 - 16 to identify serum autoantibodies complexed with their cognate antigens detected thirteen autoantibodies related to cardiac and coagulative pathway ( fig 3d ; data supplement )  . 
by contrast , the recurrent presentation , although displaying low ejection fraction and elevated bnp ( c and d ) , did not display markedly elevated troponin levels ( b )  . 
follow - up ecg after initial presentation shows persistence of st elevation and development of low - voltage ecg ( b )  . ecg one month after initial presentation shows low - voltage ecg and development of right bundle branch block ( rbbb , c )  . 
myocardial biopsy ( e ) demonstrated mixed inammation ( yellow arrow ) with some associated myocyte damage ( orange arrow ) and some healing injury ( green star ) near relatively uninvolved myocardium ( cyan star ) ; higher - power image is also shown ( f ) ; hematoxylin and eosin staining ; digital acquisition ; scale bars as shown = 100 m . immunohistochemistry demonstrated that most of this inltrate was composed of cd3positive t cells ( g , stained cells in brown ) and cd68 - positive macrophages ( h , stained cells in brown )  . 
avr , augmented vector right ; avl , augmented vector left ; avf , augmented vector foot . cmr showing the presence of severe biventricular dysfunction , mild pericardial effusion , and a short axis late gadolinium enhancement ( lge ) stack showing lge in a subepicardial distribution involving the basal and apical segments ( admission )  . although iraes often develop within the rst few weeks to months after initiation of treatment , these events can present at any time , including after cessation of ici therapy . 
luminex - based analysis of circulating inammatory cytokines revealed consistently elevated responses enriched in th1 cell cytokines ( a ) in contrast to th2 cell cytokines ( b )  . two mirs related to cardiac function and inammation displayed consistent trends in expression with mir - 130 - 3p trending upward and mir - 122 - 5p trending downward ( c )  . 
serum autoantibody complexes were observed consistently in the programmed cell death protein - 1 ligand 1induced fulminant myocarditis patient compared to ageand sex - matched control patients ( n = 7 ) , and a patient with myocarditis from systemic lupus erythematosus ( n = 1 ; d )  . serum autoantibody complex data are displayed as relative expression ( average protein intensity ) with data presented as the mean 6 the standard deviation . 
 case report surveillance after an episode of myocarditis , and the necessity for rapid and effective immunosuppression.4 treatment with high - dose glucocorticoids and mmf appeared to improve symptomology ; however , it may have failed to affect the underlying etiology as bnp levels remained marginally abnormal while high levels of inammatory cytokines and autoantibodies persisted . 
it is possible that in addition to generating autoreactive t cells against cardiac epitopes ( a proposed cause of ici - mediated myocarditis ) , icis may also induce th1 - dependent pathogenic autoantibody production ( data supplement )  . patients presenting with symptoms suggestive of ici - related myocarditis present a signicant diagnostic challenge . cardiac troponins can be negative in cases of myocarditis.20 indeed , in this case , troponins were only intermittently and mildly elevated during myocarditis recurrence . 
the diagnostic value of echocardiography and ecg is often limited , with ndings suggestive of myocarditis either absent initially or lacking specicity.4 , 6 the addition of cmr may be to detect benecial owing to its potential inammation , edema , and brosis within myocardial tissue . 
however , lge alone has low sensitivity and accuracy in diagnosing chronic or recurrent myocarditis , and cmr is difcult in hemodynamically unstable patients.21 although the recovery of lv function and resolution of symptoms followed by a separate recurrence of symptoms consistent with acute myocarditis is suggestive of a distinct myocarditis event , one other possibility could include the persistence of subclinical inammation between episodes , leading to smouldering myocarditis and subsequent heart raises awareness that serious iraes can occur after ici discontinuation , and without re - exposure , reinforcing the importance of cardiovascular surveillance after an episode of ici - associated myocarditis along with detailed diagnostic work - ups . 
fish provision of study materials or patients : nazanin aghel , paaladinesh thavendiranathan collection and assembly of data : nazanin aghel , dakota gustafson , ashley di meo , milena music , michael a . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . support preparation of this paper used the resources of the toronto general hospital research institute , university health network , toronto , canada . 
hansen consulting or advisory role : merck , glaxosmithkline , bristol - myers squibb , eisai research funding : karyopharm therapeutics , merck , bristol - myers squibb , boehringer ingelheim , glaxosmithkline , roche / genentech , janssen , astrazeneca / medimmune , astellas pharma , macrogenics paaladinesh thavendiranathan honoraria : amgen no other potential conicts of interest were reported . acknowledgment the authors would like to thank the peter munk cardiac centre cardiovascular biobank for the assistance provided with the clinical sample storage , maintenance , and retrieval . references antonia sj , villegas a , daniel d , et al : durvalumab after chemoradiotherapy in stage iii non - small - cell lung cancer . 
n engl j med 377 : 1919 - 1929 , 2017 larkin j , chiarion - sileni v , gonzalez r , et al : combined nivolumab and ipilimumab or monotherapy in untreated melanoma . 
n engl j med 373 : 23 - 34 , 2015 puzanov i , diab a , abdallah k , et al : managing toxicities associated with immune checkpoint inhibitors : consensus recommendations from the society for immunotherapy of cancer ( sitc ) toxicity management working group . 
j am coll cardiol 71 : 1755 - 1764 , 2018 l aubli h , balmelli c , bossard m , et al : acute heart failure due to autoimmune myocarditis under pembrolizumab treatment for metastatic melanoma . j immunother cancer 3 : 11 , 2015 8 . 
mir h , alhussein m , alrashidi s , et al : cardiac complications associated with checkpoint inhibition : a systematic review of the literature in an important emerging area . 
hsu sh , wang b , kota j , et al : essential metabolic , anti - inammatory , and anti - tumorigenic functions of mir - 122 in liver . 
ohyama k , yoshimi h , aibara n , et al : immune complexome analysis reveals the specic and frequent presence of immune complex antigens in lung cancer patients : a pilot study . 
recent work has determined that 20% to 30% of mcrpc tumors harbor alterations that result in the loss of dna repair capacity , in particular , the homologous recombination pathway.1 , 2 in turn , these alterations may predict response to poly - adp ribosylase ( parp ) inhibitors and platinum chemotherapy , which provides opportunities for precision therapy using agents that are not currently standard or available for mcrpc.3 , 4 in ovarian canceralso frequently marked by homologous recombination deficiencyplatinum is the standard front - line treatment , and parp inhibitors olaparib , niraparib , and rucaparib are now us food and drug administrationapproved for brca1 / 2mutated tumors . 
reversion mutations inbrca1 / 2 , 5 - 8 and more recently in rad51c and rad51d , 9 have previously been described as a mechanism of resistance to platinum and parp inhibitors in ovarian cancer and thus also represent an important consideration in patients with prostate cancer . recently , reversion mutations to restore brca1 / 2 function have been observed in prostate tumors sampled by biopsy and in circulating tumor dna ( ctdna ) from patients who were treated with parp inhibitors.10 , 11 here , we describe a case of a patient with mcrpc who exhibited polyclonal brca2 reversion mutations at the time of disease progression when receiving platinum chemotherapy . 
to our knowledge , this is the first report of brca2 reversions occurring in a patient with prostate cancer in the setting of platinum treatment and mediating resistance to therapy . our patient presented with a prostate - specific antigen ( psa ) of 8.6 ng / ml and gleason 4 + 5 prostate adenocarcinoma in october 2011 at 65 years of age . 
he underwent a radical prostatectomy with bilateral pelvic lymph node dissection in january 2012 with pt3br1n1 ( american joint committee on cancer 7 ) , gleason 5 + 4 staging . 
postoperative psa in april 2012 was 2.7 ng / ml ; restaging scans demonstrated bone involvement in the left iliac wing and l4 vertebral body without lymph node or visceral involvement . he was initially treated with bicalutamide and leuprolide ( a luteinizing hormonereleasing hormone agonist ) , which resulted in undetectable psa by may 2013 . 
in june 2016 , he began treatment with enzalutamide 160 mg once daily , but was noted to have primary refractory disease with a psa increase to 370.3 ng / ml in 1 month . 
black arrow denotes time of circulating tumor dna ( ctdna ) collection . in october 2016 , carboplatin area under the curve 5 was administered based on the results of the metastatic tumor biopsy sequencing . 
after seven cycles , psa increased to 428.1 ng / ml on april 12 , 2017 , concurrent with ctdna draw . samples from the primary prostate tumor , germline dna , and a ctdna sample that was obtained at the time of progression on carboplatin ( march 2017 ) were sequenced by using a clinically validated tumor sequencing next - generation sequencing assay12 and compared with the prechemotherapy metastasis biopsy . 
a frameshift mutation in brca2 ( p.n2452mfs * 17 ) as well as in spop and tp53 mutations were identified in the primary tumor and metastasis ( table 1 )  . 
we did not observe evidence of a germline pathogenic variant . we performed targeted next - generation sequencing on ctdna at the time of progression to 1 , 6103 mean coverage , and identified 90 brca2 reads that carried the frameshift mutation and 1 , 181 wild - type brca2 reads . 
of importance , no reversion mutations were detected in the primary or germline samples . secondary somatic mutations of brca1 / 2 mutations that restore the wild - type open reading frame were initially described as a mechanism of resistance to platinum chemotherapy in ovarian cancer and have subsequently been reported in patients with prostate cancer who were treated with parp inhibitors.5 , 10 , 11 to our knowledge , this is the first example of reversion mutations in the ctdna of a patient with prostate cancer associated with resistance to platinum chemotherapy . our finding provides evidence that polyclonal reversion is a mechanism of resistance to platinum chemotherapy in patients with prostate cancer . prospective clinical trials of parp inhibitors and platinum to exploit the molecular vulnerabilities of prostate cancer with dna repair defects are now underway , and although there is great enthusiasm , resistance to these strategies is expected . we previously described a series of patients with prostate cancer with biallelic brca2 inactivation who had exceptional and sometimes extended responses to carboplatin - based therapy ( up to 3 years ) .4 in addition , a recent retrospective analysis of patients whose prostate cancer was refractory to taxanes found that six ( 75% ) of eight patients who were carriers of pathogenic germline brca2 variants had a psa50 response from 12 weeks of carboplatin plus docetaxel therapy compared with 23 ( 17% ) of 133 noncarriers.15 two prospective clinical trials that are investigating carboplatin table 1 . 
dashed outline represents second allele . sequencing reads with secondary mutations in the plasma circulating tumor dna ( ctdna ) sample taken at the time of progression on carboplatin ( bottom )  . 
images were rendered by using the integrative genomics viewer.13 , 14 with docetaxel for patients with mcrpc and dna repair defects are currently recruiting patients ( clinicaltrials.gov identifiers : nct02598895 and nct02985021 ) and may be opportunities to explore this and other potential resistance mechanisms . the recent finding of secondary reversion mutations in patients with prostate cancer after parp inhibitor therapy occurred within 8 to 10 months of initiating therapy.10 , 11 in our patient , resistance emerged after the same apparent mechanism over approximately 7 months , a more abbreviated benefit compared with the multiple years of response to platinum - based therapy that we have observed and on which we have previously reported.4 our patients case provides evidence that reversion mutations selected by platinum chemotherapies can occur at a similar pace as parp inhibitors and implies that additional factors that are yet to be characterized influence the chronology of resistance to dna - damaging agents . 
although we did not detect a second inactivating mutation in our patient , it is possible that an undetected methylation or a complex rearrangement could be present . nonetheless , evidence of reversion mutations that restore gene function and that temporally coincide with clinical progression during platinum therapy together make a strong case that brca2 gene function was disrupted in the primary and metastatic tumor . it is possible that the mechanism of initial gene inactivation affects resistance . 
for example , patients with biallelic copy loss may be less likely to restore functional copy and thus have a longer response duration compared with those with biallelic singlenucleotide substitutions and / or indels , which might restore gene function more readily to give rise to resistance . 
in addition , although platinum and parp inhibitors share reversion as a mechanism of resistance , patients with ovarian cancer resistant to parp inhibitors can still exhibit sensitivity to platinum , which demonstrates that there are differences as well.16 many unanswered questions remain regarding the noninvasive assessment of resistance . 
 only been identified after selective treatment pressure and not as de novo events , although the lack of detection may reflect mutation levels that are lower than the sensitivity of assays used to detect reversion events . 
in this case , we did not have matched tumor biopsy and ctdna for each clinically relevant time point , although the samples we collected demonstrated proof of an important mechanism of resistance to platinumany in the field are investigating concordance and representative sampling of tumor versus ctdna , which will be important to clinical practice . another critical issue is whether early reversion clones specifically and reliably predict the development and pace of clinical resistance , the differences between platinum and parp inhibitors , and what other potential relevant genetic , epigenetic , and microenvironmental modifying factors are at play . 
nelson consulting or advisory role : janssen oncology , astellas pharma , genentech bruce montgomery research funding : essa pharma , medivation , astellas pharma , janssen oncology , ferring pharmaceuticals colin c . 
pritchard no relationship to disclose acknowledgment we thank arul chinnaiyan , daniel robinson , hiep nguyen , and the stand up to cancer / prostate cancer foundation precision oncology team for their assistance with the collection and analysis of the metastatic biopsy . affiliations support references 417 - 425 , 2017 1697 - 1708 , 2015 all authors , university of washington ; heather h . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . j mol diagn 16 : 56 - 67 , 2014 13 . 
ang je , gourley c , powell cb , et al : efficacy of chemotherapy in brca1 / 2 mutation carrier ovarian cancer in the setting of parp inhibitor resistance : a multi - institutional study . 
 c brca2 - associated prostate cancer in a patient with spinal and bulbar muscular atrophy introduction spinal and bulbar muscular atrophy ( sbma ) , or kennedys disease , is a rare x - linked recessive disorder characterized by expanded cag trinucleotide repeats involving exon 1 of the androgen receptor ( ar ) gene and a variable adult onset of muscle weakness , atrophy , fasciculation , tremor , and hyporeflexia or areflexia involving the proximal limb and bulbar musculature , with usually a slowly progressive course , and findings of androgen insensitivity , including gynecomastia , impotence , reduced fertility from oligospermia , testicular atrophy , and normal or increased testosterone levels , which may precede the neuromuscular symptoms by a decade.1 , 2 because cag repeat length is inversely correlated with the transactivation function of the ar , a higher number of cags has been associated with a much lower incidence of developing prostate cancer.3 , 4 ar signaling is a critical driver of prostate cancer development and progression . 
during this time , his initial prostate biopsy was re - reviewed and classified as mixed gleason 5 + 5 adenocarcinoma and small - cell carcinoma ( fig 2a )  . 
on the basis of re - reading his pathology and his presentation with aggressive disease ( which included liver metastases ) , carboplatin chemotherapy was added to the last four cycles of docetaxel . 
 re - evaluation after chemotherapy showed a persistent undetectable psa , decreased size of liver lesions , and reduced enhancement of several of the bone lesions . during this follow - up time , the patient gave his informed consent to participate in molecular studies ( institutional review board #1305013903 )  . 
 capillary electrophoresis was performed to calculate the size of the ar gene trinucleotide repeat , and it confirmed a genetic diagnosis of sbma with approximately 49 repeats in both germline and tumor dna ( fig 2b )  . 
gene expression and protein analysis5 , 6 revealed relatively high ar as well as expression of ar - target genes such as psa ( klk3 ) and tmprss2 ( fig 2c ; appendix figs a1 and a2 )  . targeted deep sequencing7 was performed of both his tumor and germline dna . 
pritchard himisha beltran author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : himisha beltran , md , joan and sanford i . 
his serum psa decreased approximately 75% at 1 month after initiating talozoparib ( last psa , 0.5 ng / ml )  . discussion prostate cancer arises as an androgen - driven disease . 
even in castration - resistant prostate cancer , the ar remains a key driver.9 this has been the basis for the clinical use of potent ar targeted drugs ( eg , abiraterone and enzalutamide )  . prostate cancer risk and outcomes have been associated with serum androgen levels and polymorphisms involving the ar gene . 
loh favored variation type frameshift insertion nonframeshift deletion large deletion variation type frameshift insertion single copy loss on chr13 in a region that includes brca2 and 10 11 12 13141516 17 18 19202122 x fig 2 . 
 ( a ) prostate biopsy hematoxylin and eosin stained photomicrographs showing mixed gleason 5 + 5 prostate cancer adenocarcinoma with neuroendocrine differentiation ( top panel ) and small - cell carcinoma ( bottom panel )  . 
 ( c ) expression of ar signaling genes ( klk3 , tmprss2 ) was performed by using a nanostring assay with custom probe sets previously used for studies of primary prostate cancer , castration - resistant prostate cancer , and neuroendocrine prostate cancer formalin - fixed paraffin - embedded biopsy tissue.5 , 6 horizontal bars represent median values . 
 ( d ) genomic landscape identified by tumor sequencing displayed germline brca2 pathogenic frameshift mutation ( c.3975_3978dup ) , with clear loss of heterozygosity ( loh ) in the tumor . 
additional somatic ( tumor ) mutations were detected in the patients tumor , including an foxa1 inframe deletion and tp53 mutation as well as copy number alterations involving myc , rb1 , and brca2 genes . 
this occurs after the association of ar with its ligand , which results in the exposition of the polyglutamine tract eliciting an interaction with another polyglutamine ar or the production of aberrant ar conformational modifications.11 , 16 , 17 this knowledge has led to the investigation of adt in these individuals , suggesting that long - term adt might delay functional decline , 18 , 19 although our patient did not experience a significant improvement in his sbma symptoms after the initiation of adt . 
molecular pathogenesis of spinal and bulbar muscular atrophy ( sbma ) and potential risk of prostate cancer associated with altered polyglutamine ( polyq ) chain length in the androgen receptor ( ar )  . 
the ar contains a c - terminal ligand - binding domain ( lbd ) , a central dna - binding domain ( dbd ) that attaches to androgen - responsive target genes , and an n - terminal domain ( ntd ) that influences transcription efficiency . 
exon 1 of the ar gene contains a polymorphic sequence of cag repeats , which usually varies in number up to 40 ( normal ) , and encodes polyglutamine stretches of ar transactivation doma under normal conditions , the ar first interacts with its ligand dihydrotestosterone ( dht ) and then migrates to the cell nucleus , where it interacts with specific dna sequences inducing transcription of androgen target genes , including klk3 ( prostate - specific antigen [ psa ] ) and other genes . 
 polyglutamine ar ( polyq - ar ) also migrates to the nucleus after binding with testosterone , and once it is in the nucleus , it can no longer interact properly with ar target genes . 
 damage to motor neurons can result both from cell - autonomous and noncell - autonomous toxic processes , the latter arising in other cell types such as skeletal muscle cells . 
in the age of precision medicine , the molecular profile of our patients tumor also highlights critical opportunities to translate genomics into clinical care . although ar was expressed , it is likely that this ar - expressing tumor was less dependent on ar signaling . 
consistent with this , this patients tumor exhibited alterations in both rb1 and tp53 , genes previously associated with the development of nonar - driven prostate cancer , lineage plasticity , and the neuroendocrine prostate cancer phenotype.5 , 24 - 26 this might also explain the patients lack of durable response to enzalutamide and the observed mixed small - cell morphologic features of his tumor at diagnosis . 
 in addition , his chemotherapy responsiveness is a clinical hallmark of a recognizable subset , aggressive variant of prostate cancer , which shares clinical and molecular features with small - cell carcinomas.27 , 28 additional mechanisms that may be the drivers of disease initiation beyond the ar in this case include loss of dna repair through the presence of a pathogenetic brca2 mutation and tumor loss of heterozygosity , or they could be biologically interconnected , as shown in studies of breast cancer in which the length of the ar - cag repeat affected the timing of cancer diagnosis in brca1 mutation carriers , likely through modulation of hormonal responses of mammary epithelial cells.29 recent studies showed a relatively high incidence of both germline and somatic alterations involving dna repair genes such as brca2 in patients with advanced prostate cancer.30 - 32 these alterations likely play a critical role in the pathogenesis of more aggressive prostate cancers , leading to an increased probability of the development of lethal disease . 
a germline brca2 mutation confers an increased risk of developing prostate cancer ( 8.6 - fold in men age 65 years or younger ) 33 and has been demonstrated to be an independent poor prognostic factor associated with higher rates of developing metastatic disease and shorter survival.34 in patients with metastatic castration - resistant prostate cancer treated with standard therapies , evidence on the prognostic and predictive role of dna repair alterations is still conflicting , 35 - 37 although brca2 carriers have been reported to have poorer outcomes overall compared with those who do not carry brca2.38 in this patient , the presence of a brca2 mutation may have trumped or bypassed the need for high ar signaling during the development of prostate cancer . 
the influence of dna repair alterations on the development of small - cell neuroendocrine prostate cancer and therapy response also warrants further study . notably , the germline brca2 mutation was not suspected on the basis of family history ; thus , it had important implications for his family members ( ie , cancer screening ) and helped in selecting therapy for hi tumor cells that harbor dna repair gene alterations are more susceptible to drugs that induce dna damage such as platinum - based chemotherapy39 , 40 or those that impair alternative dna repair pathways , 30 as shown in our patient ( who had a response to platinum and is currently responding to parp inhibitor therapy )  . 
it may also be informative to re - evaluate this patient at the time of progression on telazoparib for acquired brca2 reversion41 , 42 or other mechanisms of resistance , given the multiple drivers present in this case . our case outlines the striking clinical course and favorable treatment response of a patient with a rare genetic neuromuscular disease that harbors clinical and molecular features of an aggressive variant of prostate cancer treated with a precision oncology approach . 
a germline brca2 mutation likely overcame the need for high ar signaling ( evidenced by sbma as well as the small - cell features ) , and the acquisition of tp53 and rb1 alterations further supported non - ar driven disease , contributing to its clinical aggressiveness and lack of durable response to enzalutamide . 
pritchard , himisha beltran manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors michael sigouros no relationship to disclose andrea sboner no relationship to disclose colin c . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . himisha beltran consulting or advisory role : janssen oncology , sanofi , genzyme , glaxosmithkline , abbvie research funding : astellas pharma ( inst ) , janssen oncology ( inst ) , abbvie / stemcentrx , eli lilly ( inst ) , millennium pharmaceuticals ( inst ) affiliations vincenza conteduca , michael sigouros , andrea sboner , and himisha beltran , weill cornell medicine ; andrea sboner and himisha beltran , weill cornell medicine - new york presbyterian hospital , new york , ny ; vincenza conteduca , istituto scientifico romagnolo per lo studio e la cura dei tumori , istituto di ricovero e cura a carattere scientifico , meldola , italy ; and colin c . 
kosaka t , miyajima a , kikuchi e , et al : a case of spinal and bulbar muscular atrophy with highstage and high - gleason score prostate cancer responded to maximal androgen blockade therapy . 
beltran h , wyatt aw , chedgy ec , et al : impact of therapy on genomics and transcriptomics in high - risk prostate cancer treated with neoadjuvant docetaxel and androgen deprivation therapy . 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . 
freedman ml , pearce cl , penney kl , et al : systematic evaluation of genetic variation at the androgen receptor locus and risk of prostate cancer in a multiethnic cohort study . 
lindstrm s , zheng sl , wiklund f , et al : systematic replication study of reported genetic associations in prostate cancer : strong support for genetic variation in the androgen pathway . 
kumar r , atamna h , zakharov mn , et al : role of the androgen receptor cag repeat polymorphism in prostate cancer , and spinal and bulbar muscular atrophy . 
hashizume a , katsuno m , suzuki k , et al : long - term treatment with leuprorelin for spinal and bulbar muscular atrophy : natural history - controlled study . 
yasui t , akita h , itoh y , et al : cag repeats in the androgen receptor : a case of spinal and bulbar muscular atrophy associated with prostate cancer . 
kote - jarai z , leongamornlert d , saunders e , et al : brca2 is a moderate penetrance gene contributing to young - onset prostate cancer : implications for genetic testing in prostate cancer patients . 
castro e , goh c , olmos d , et al : germline brca mutations are associated with higher risk of nodal involvement , distant metastasis , and poor survival outcomes in prostate cancer . 
mateo j , cheng hh , beltran h , et al : clinical outcome of prostate cancer patients with germline dna repair mutations : retrospective analysis from an international study . 
antonarakis es , lu c , luber b , et al : germline dna - repair gene mutations and outcomes in men with metastatic castration - resistant prostate cancer receiving first - line abiraterone and enzalutamide . 
castro marcos e , romero laorden n , piulats rodriguez jm , et al : prorepair - b : a prospective cohort study of dna repair defects in metastatic castration resistant prostate cancer ( mcrpc )  . 
pomerantz mm , spisk s , jia l , et al : the association between germline brca2 variants and sensitivity to platinum - based chemotherapy among men with metastatic prostate cancer . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
jonkers j , meuwissen r , van der gulden h , et al : synergistic tumor suppressor activity of brca2 and p53 in a conditional mouse model for breast cancer . 
gene expression was performed by using the nanostring ncounter assay with custom probe sets previously used for studies of primary prostate cancer ( pca ) , castration - resistant prostate cancer ( crpc ) , and neuroendocrine prostate cancer ( nepc ) using formalin fixed paraffin - embedded tissue . 
henick , md1 ; matthew ingham , md1 ; maryam shirazi , md2 ; charles marboe , md2 ; andrew turk , md2 ; susan hsiao , md , phd2 ; and mahesh m . 
intervening surveillance scans were unremarkable ; however , the patient experienced a 10 - pound weight loss over 2 months that culminated in acute - onset exertional dyspnea and chest pain , prompting admission . 
the patient was evaluated by cardiothoracic surgery and deemed not to be a surgical candidate . positron emission tomography ( pet ) ct conrmed uorodeoxyglucose avidity in the hypermetabolic mass , scattered left lung nodules , and an intralumina soft tissue mass in the distal colon proximal to the anastomosis as well as a right thyroid lesion ( fig 1 )  . 
restaging ct of the chest after 2 cycles revealed decreasing peripheral opacities in the left upper lobe , a decrease in irregular left - sided lung nodules , and a decrease in the extent of tumor thrombus , with an increase in patency of the left pulmonary artery and interval resolution of cavitation within the tumor thrombus . 
in addition , the vaf of 67% indicated loss of heterozygosity in the tumor , raising the possibility of a germline alteration ( germline testing has not been performed )  . 
because the msi status was indeterminate by ngs , msi testing by polymerase chain reaction ( pcr ) fragment analysis using ve quasimonomorphic mononucleotide repeats ( msi analysis system , version 1.2 ; promega , madison , wi ) was performed but was indeterminate , because normal dna for comparison was unavailable . 
using dna extracted from peripheral blood for comparison , msi with an altered allele at four of ve tested loci ( nr - 21 ; bat - 26 ; bat - 25 ; mono - 27 ; fig 3 ) was detected . 
positron emission tomography / computed tomography results ( a ) at baseline , ( b ) after treatment with doxorubicin plus olaratumab before pembrolizumab administration , and ( c ) after 8 cycles of pembrolizumab . with chemotherapy , the patient was amenable to treatment with pembrolizumab and began therapy . 
after 8 cycles of treatment , intervening pet - ct results have shown an additional decrease in the extravascular component of the pulmonary artery tumor with evolving dystrophic calcication , no evidence of tumor thrombus , stable ndings in the lungs likely consistent with pulmonary infarcts , an avid hypermetabolic right thyroid nodule , and a decrease in soft tissue nodularity at the suture line . discussion intimal sarcoma of the pulmonary artery is a rare tumor ( incidence , approximately 0.001%2 , 3 ) , and the scant existing medical literature highlights individual cases of response to various combinations of surgery , 4 chemotherapy , 5 and radiation.6 the molecular landscape of such tumors is not well characterized . studies of immune checkpoint blockade have demonstrated mixed results in the treatment of sarcomas . 
the phase ii alliance a091401 study examined nivolumab monotherapy and nivolumab plus ipiliumumab in the treatment of metastatic sarcoma.7 two of 38 patients experienced conrmed responses with nivolumab treatment , and six of 38 experienced responses to the combination.7 in a single - arm , phase ii study of pembrolizumab in soft tissue sarcoma or bone sarcoma cohorts , the overall response endpoint was not met , though seven of 40 patients with soft tissue sarcoma and two of 10 patients with liposarcoma experienced responses.8 preliminary activity was seen ( 3 - month progression - free survival , 72.7% ) with the combination of axitinib and pembrolizumab in a single - arm , phase ii study in alveolar soft - palate sarcomas.9 on may 23 , 2017 , the us food and drug administration ( fda ) approved pembrolizumab for the second - line treatment fig 2 . 
penta c and penta d are polymorphic pentanucleotide markers that show identity between the tumor and normal samples . of msi - high ( msi - h ) or mmr - decient ( dmmr ) solid tumors on the basis of ndings in patients retrospectively identied ( keynote - 012 , - 028 , and - 158 ) and prospectively enrolled ( keynote - 016 , - 158 ) .10 , 11 in these trials , msi status was identied prospectively by local laboratory - developed pcr ( n = 60 of 149 patients ) , ihc ( n = 47 of 149 ) , or both ( n = 42 of 149 ) ; retrospectively , 14 of 149 patients were identied by a central laboratorydeveloped pcr test.12 in practice , dmmr status is established by ihc for expression of mmr proteins ( mlh1 , msh2 , msh6 , and pms2 ) , and msi - h is demonstrated by multiplexed pcr of either the national cancer institute panel of two mononucleotide and three dinucleotide the more widely used panel of ve quasimarkers or monomorphic mononucleotide markers ( promega , madison , wi )  . 
at columbia university irving medical center , both ihc and pcr are used , as either can miss individual cases.13 in addition , large ngs panels , such as the one performed in the case , can be used to evaluate for msi . 
the cccp assay interrogates 8 , 682 monoand di - nucleotide repeat loci a 1.27 - mb region of interest and classies tumors as microsatellite stable or unstable according to the number of altered microsatellite loci.14 cases that cannot be denitively classied as microsatellite stable or unstable by the cccp assay are rare and were not seen in the more than 200 cases used in validation , which encompassed a range of tumor types . although the efcacy of programmed death 1 blockade in microsatellite - unstable tumors is well established , 10 , 11 , 15 to our knowledge this is the rst report of a clinical outcome of an intimal sarcoma associated with treatment with immune checkpoint blockade . 
we present this case in part for that reason but also to highlight challenges in executing the mmr - deciency testing that is critical to identify patients who may benet this fdaapproved indication ( table 1 )  . 
assays to evaluate microsatellite instability / mismatch repair deciency at columbia university irving medical center technique pcr fragment analysis what is five quasi - monomorphic mononucleotide evaluated ? repeats ( promega msi evaluation system ; promega , madison , wi ) indel variant detection in microsatellite repeat tracts ( columbia combined cancer panel , a 468 - gene ngs panel ) loss of expression of mlh1 , mlh2 , msh6 , pms2 in tumor cells limitations ? tumor percentage ; tissue type ( eg , lower sensitivity for endometrial or prostate cancers16 ; cancers in constitutional mismatch repair deciency17 ) can affect sensitivity . 
small biopsies , reactive non - neoplastic cells expressing mmr proteins , and loss - of - function variants with retained epitopes can cause false - normal ihc results , while msi testing in noncolorectal cancers may be more difcult to interpret.18 despite their greater overall sensitivity , individual results of ngs panels may be affected by heterogeneity in rates of alterations of individual repeats across tumor types , 19 especially in noncolorectal and endometrial cancers , as highlighted by this case and in a survey of 15 , 045 tumors in which lynch syndrome was identied in 1.6% ( 13 of 699 ) of msi - indeterminate tumors , predominantly noncolon / endometrial cancers ( 10 of 13 ) all of which showed abnormal ihc ( 10 of 10 tested cases ) .20 furthermore , commonly used markers ( by the national cancer institute and promega ) are not among the most frequently altered repeats in the cancer genome atlas exome data , 21 implying that that tests that use limited numbers of markers yield false negatives . 
therefore , when faced with advanced cancers with few options , multimodality testing for mmr deciency may be warranted . affiliations 1department of medicine , medical oncology , columbia university irving medical center , new york city , ny 2department of pathology , molecular pathology , columbia university irving medical center , new york city , ny subject matter of this manuscript . 
henick stock and other ownership interests : abbvie consulting or advisory role : boehringer ingelheim matthew ingham consulting or advisory role : daiichi sankyo research funding : apexigen ( inst ) , mirati therapeutics ( inst ) , ptc therapeutics ( inst ) travel , accommodations , expenses : mirati therapeutics , genentech andrew turk employment : ventana medical systems , bristol - myers squibb , medarex , bayer consulting or advisory role : bayer , bristol - myers squibb , ventana medical systems susan hsiao honoraria : medscape , illumina consulting or advisory role : ventana medical systems , bristol - myers squibb , loxo research funding : bristol - myers squibb mahesh m . 
mansukhani travel , accommodations , expenses : bristol - myers squibb , promega , er squibb sons no other potential conicts of interest were reported . references colmbia university department of pathology and cell biology : columbia combined cancer panel ( cccp )  . 
specialties / personalized - genomic - medicine / oncology - testing / columbia - combined - cancer - panel choi ey , yoon yw , kwon hm , et al : a case of pulmonary artery intimal sarcoma diagnosed with multislice ct scan with 3d reconstruction . 
yonsei med j 45 : 547 - 551 , 2004 alsou b , slater m , smith pp , et al : pulmonary artery sarcoma mimicking massive pulmonary embolus : a case report . 
asian cardiovasc thorac ann 14 : e71 - e73 , 2006 akomea - agyin c , dussek je , anderson dr , et al : pulmonary artery sarcoma mimicking pulmonary embolism : successful surgical intervention . 
ann thorac surg 61 : 1536 - 1538 , 1996 cantaloube m , moureau - zabotto l , mescam l , et al : metastatic intimal sarcoma of the pulmonary artery sensitive to carboplatin - vinorelbine chemotherapy : case report and literature review . 
case rep oncol 11 : 21 - 28 , 2018 long hq , qin q , xie ch : response of pulmonary artery intimal sarcoma to surgery , radiotherapy and chemotherapy : a case report . 
j med case reports 2 : 217 , 2008 dangelo sp , mahoney mr , van tine ba , et al : nivolumab with or without ipilimumab treatment for metastatic sarcoma ( alliance a091401 ) : two open - label , non - comparative , randomised , phase 2 trials . 
lancet oncol 19 : 416 - 426 , 2018 tawbi ha , burgess m , bolejack v , et al : pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
wilky ba , trucco mm , subhawong tk , et al : axitinib plus pembrolizumab in patients with advanced sarcomas including alveolar soft - part sarcoma : a singlecentre , single - arm , phase 2 trial . 
waalkes a , smith n , penewit k , et al : accurate pan - cancer molecular diagnosis of microsatellite instability by single - molecule molecular inversion probe capture and high - throughput sequencing . 
bakry d , aronson m , durno c , et al : genetic and clinical determinants of constitutional mismatch repair deciency syndrome : report from the constitutional mismatch repair deciency consortiueur j cancer 50 : 987 - 996 , 2014 . 
 c active disclosure of secondary germline findings to deceased research participants personal representatives : process and outcomes introduction somatic mutation profiling of tumors is performed in both clinical and research settings , often to identify patients with cancer who are candidates for targeted therapies . 
profiling also can be performed through simultaneous analysis of tumor and normal ( germline ) dna , which allows for identification of mutations unique to the tumor by subtracting germline variants . 
both the american college of medical genetics and genomics ( acmg ) 1 , 2 and asco3 recommend that disclosure of actionable secondary germline findings from tumor - normal paired testing be offered to patients . although these guidelines address clinical testing , they are also a starting point in considering secondary germline findings identified upon research testing . 
we reported our experience with return of secondary germline findings to living patients with advanced cancer who participated in a study of tumor - normal paired research testing.4 by using the acmg gene list2 ( plus palb2 ) as the disclosure threshold , we found that all contacted patients agreed to genetic counseling and testing . given both the poor prognosis of patients with advanced cancer and the long turnaround times of research testing , an unfortunate reality is that secondary germline findings are discovered after the patient has died . 
chan et al5 described disclosure to a decedents family upon the decedents request and advocated for a policy of at least passive disclosure of clinically significant results to relatives who request thepassive disclosure is unlikely in the context of somatic mutation profiling studies because relatives are likely unaware of possible secondary germline findings . wolf et al6 reported consensus recommendations with regard to returning research participants genomicresultstorelatives , includingthatresearchers may return results to relatives but are not obligated to do so , and emphasized the key role of the deceased participants representative ( eg , his or her personal representative [ pr ] as defined by the health insurance portability and accountability act ) as the initial contact and decision maker about disposition of the results . 
amendola et al7 described active disclosure of a germline ( possibly mosaic ) tp53 mutation to a decedents spouse and subsequent testing of relatives . disclosure of secondary findings to families of deceased participants has a potential benefit . 
in our previous studies , participants reported wanting to receive clinically relevant genetic findings.4 , 8 secondary findings can occur in the absence of suggestive personal / family history , which makes it unlikely that relatives would otherwise learn about the mutation . 
in this article , we report our experience with active disclosure of secondary germline findings to deceased participants prs . methods patients with cancer under consideration for genomically informed clinical trials were enrolled in an institutional review board ( irb ) approved protocol for genomic profiling with optional germline testing ( clinicaltrials.gov identifier : nct01772771 )  . 
this study was activated february 2012 ; patients enrolled after october 9 , 2013 , were also offered a companion protocol that ascertained molly daniels chetna wathoo lauren brusco karen h . 
 their preferences for return of secondary results to their pr in the event of their death . to address secondary findings in deceased participants who consented before the companion protocol , we sought advice from irb , legal , and ethics services . 
consensus was reached that the benefit of return of results to families outweighed the risk . the irb - approved revised protocol allowed disclosure of results to families of patients who died before soliciting their preferences . secondary germline findings were identified as previously described.4 we limited results return to pathogenic variants with established clinical utility ( acmg list2 plus palb2 ) not already identified through clinical testing . 
we took a conservative approach of disclosure to the affidavit - verified pr ( fig 1 )  . results we identified 16 secondary findings in decedents ( table 1 )  . 
results indicated a germline pathogenic tp53 mutation , which was disclosed to his wife . case 3 : a 69 - year - old man of partially ashkenazi jewish ancestry with recently diagnosed metastatic pancreatic adenocarcinoma presented for treatment . 
results indicated the germline ashkenazi jewish founder brca2 mutation , which was disclosed to his daughter . consistent with clinical practice and our disclosure practice for living study participants , we did not contact other relatives . 
a relative with no personal history of cancer has subsequently received positive test results for the familial mutation . case 1 : a 58 - year - old woman with recurrent high - grade serous ovarian cancer presented for discussion of phase i trials . 
she died 4 months after study consent . results indicated a germline pathogenic brca1 mutation , which was disclosed to her son . case 2 : a 74 - year - old man with recurrent metastatic melanoma presented for treatment . discussion management of secondary genetic findings in research studies is controversial , even more so when the participant is deceased . 
a relative subsequently underwent predictive genetic testing and can now benefit from more - intensive screening and by taking preventive action . study participant confirmed deceased at time pathogenic germline secondary finding identified . 
study coordinator calls participants next of kin as listed in ehr , up to three times ( n = 16 )  . no response contact made study coordinator mails introductory letter to next of kin ( n = 6 )  . pr declined discussion of secondary finding ( n = 2 )  . next of kin either verbally confirms that he or she is the pr or provides contact information for the pr . 
study coordinator mails affidavit with return envelope to pr ( n = 8 )  . no response to contact , no additional attempts made ( n = 6 )  . affidavit not returned affidavit returned study coordinator calls to confirm that pr received affidavit letter . 
of participants mutation gene brca2 tp53 brca1 palb2 apc * msh6 pten tsc2 i2675dfsx6 , s1764kfsx3 , e1493vfsx10 , s1982rfsx22 r282q , m237i , f270l , d324h v1757a , g1809v g1121vfsx3 , s254ifsx3 g267efsx26 l164rfsx3 l164rfsx3 q1284sfsx39 * germline apc mutation consistent with clinical presentation , but because no documentation indicated that the causative mutation had previously been identified , the participant was considered to not have been already aware of this finding . the participants in case 1 and 3 met established brca1 / brca2 testing criteria ; however , germline testing had not occurred . 
identification of the familial mutation also has the benefit of refining risk assessment ( eg , 5% to 10% chance brca positive if mother had ovarian cancer v 50% chance of brca positive if mother was brca positive ) , and relatives who test negative can be reassured . the participant in case 2 did not meet tp53 testing criteria , thus that the relatives would otherwise have undergone genetic testing is unlikely . we are not certain that this is a true germline mutation because alternate explanations , such as clonal hematopoiesis , 9 have not been ruled out . nonetheless , the testing of relatives is reasonable because relatives who test negative can be reassured . 
if a relative tests positive , then a germline mutation would be confirmed , and the subsequent changes in medical management would be substantial , even in the absence of a significant family history.10 identification and disclosure of secondary germline findings is labor intensive and is even more so when the study participant has died . 
as the field evolves , situations will continue in which information discovered during the normal course of research or clinical care will be significant for relatives in the future , even if not known to be so today . 
one option , particularly for academic medical centers engaged in both clinical care and research , would be to elicit patients global preferences at the front door with regard to disclosure of secondary findings after their death . after initial contact was made , two prs actively declined additional information . 
even if the participant designates a contact person at the time of consent , that does not mean that this person will necessarily be aware of that designation , let alone be welcoming of contact . researchers engaged in results disclosure should continue to be aware of the importance of offering findings in a noncoercive manner . in conclusion , active disclosure of secondary germline research findings to the prs of deceased study participants can be done successfully and ethically and can be of direct benefit to relatives who were unlikely to receive these results any other way . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . molly daniels no relationship to disclose chetna wathoo no relationship to disclose lauren brusco employment : celgene karen h . 
litton consulting or advisory role : novartis , medivation , pfizer research funding : novartis , bristol - myers squibb ( inst ) , medivation , genentech , pfizer patents , royalties , other intellectual property : uptodate travel , accommodations , expenses : medivation karina eterovic no relationship to disclose ugur aytac no relationship to disclose john mendelsohn leadership : merrimack pharmaceuticals stock and other ownership interests : merrimack pharmaceuticals patents , royalties , other intellectual property : royalty payments from the university of california , san diego travel , accommodations , expenses : merck gordon b . 
mills stock and other ownership interests : catena pharmaceuticals , ptv sciences , spindletop ventures , myriad genetics , immunome honoraria : symphogen , nuevolution , astrazeneca , isis pharmaceuticals , eli lilly , novartis , allostery , immunome consulting or advisory role : adventis , astrazeneca , catena pharmaceuticals , critical outcome technologies , millennium pharmaceuticals , nuevolution , precision medicine research associates , provista diagnostics , signalchem , symphogen , allostery , isis pharmaceuticals , medimmune , eli lilly , novartis , tarveda therapeutics , taurx research funding : adelson medical research foundation , astrazeneca , critical outcome technologies , nanostring technologies , komipharm international , the breast cancer research foundation , karus therapeutics , illumina , millennium pharmaceuticals patents , royalties , other intellectual property : homologous recombination deficiency assay to myriad genetics travel , accommodations , expenses : astrazeneca , symphogen , isis pharmaceuticals , medimmune , eli lilly , novartis , immunome , allostery , pfizer ken chen no relationship to disclose funda meric - bernstam honoraria : dialecta , sumitomo group consulting or advisory role : genentech , inflection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwinhealth , grail research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer ag , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , effective pharmaceuticals , curis , pfizer affiliations all authors : the university of texas md anderson cancer center , houston , tx . support supported in part by the cancer prevention and research institute of texas ( rp150535 ) , sheikh khalifa bin zayed al nahyan institute for personalized cancer therapy grant no . 
national comprehensive cancer network : genetic / familial high - risk assessment : breast and ovarian ( version 2.2017 ) , nccn clinical practice guidelines in oncology ( nccn guidelines ) , 2017 . 
to inform targeted treatment strategies , 3 , 476 clinically advanced prostate tumors were analyzed by cgp for genomic alterations ( gas ) and signatures of genomic instability . methods prostate cancer samples ( 1 , 660 primary site and 1 , 816 metastatic site tumors from unmatched patients ) were prospectively analyzed by cgp ( foundationone assay ; foundation medicine , cambridge , ma ) for gas and genomic signatures ( genome - wide loss of heterozygosity [ gloh ] , microsatellite instability [ msi ] status , tumor mutational burden [ tmb ] )  . results frequently altered genes were tp53 ( 44% ) , pten ( 32% ) , tmprss2 - erg ( 31% ) , and ar ( 23% )  . 
potentially targetable gas were frequently identied in dna repair , phosphatidylinositol 3 - kinase , and ras / raf / mek pathways . dna repair pathway gas included homologous recombination repair ( 23% ) , fanconi anemia ( 5% ) , cdk12 ( 6% ) , and mismatch repair ( 4% ) gas . 
metastatic site tumors were enriched for the 11q13 amplicon ( ccnd1 / fgf19 / fgf4 / fgf3 ) and gas in ar , lyn , myc , ncor1 , pik3cb , and rb1 compared with primary tumors . conclusion routine clinical cgp in the real - world setting identied gas that are investigational biomarkers for targeted therapies in 57% of cases . 
2019 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction genomic alterations ( gas ) that drive prostate cancer have been elucidated by proling primary tumors.1 , 2 comprehensive genomic proling ( cgp ) is increasingly used for routine clinical management of patients with prostate cancer , 3 with accumulating evidence associating gas with responses to therapy . 
 chung et al context key objective in this study , we use real - world data from routine prospective clinical genomic proling to evaluate genomic alterations ( gas ) and genomic signatures in primary and metastatic prostate cancer . knowledge generated we evaluated the landscape of gas in prostate cancer and identied those that are enriched in metastatic site tumors . approximately 3% of cases had high microsatellite instability and / or high tumor mutational burden status . 
genomic signatures , including microsatellite instability , tumor mutational burden , and genome - wide loss of heterozygosity , may further rene biomarker development for poly ( adp - ribose ) polymerase inhibitors and immunotherapies . samples using a validated assay16 ( foundationone ; foundation medicine , cambridge , ma ; appendix table a1 )  . 
the pathologic diagnosis of each case was conrmed on routine hematoxylin and eosinstained slides . results were analyzed for gas and gene signatures ( tmb , msi , genome - wide loss of heterozygosity [ gloh ] )  . 
germline / somatic mutation calls were predicted without a matched normal ; in validation testing of 480 tumor - only sequencing calls against matched normal samples , accuracy was 95% for somatic and 99% for germline calls.17 enrichment was dened as the difference in ga frequency between metastatic and primary sites . 
activating braf or raf1 fusions / rearrangements were observed in 1.2% of cases ( 35 braf and seven raf1 ; appendix fig a2 )  . the pi3k / akt / mammalian target of rapamycin ( mtor ) pathway was frequently altered ( 40.8% ; figs 1b and 1c )  . as expected , pten gas were frequent , and we observed in pik3ca , activating mutations and amplications pik3cb , akt1 / 2 / 3 , mtor , and rictor and loss - offunction alterations in pik3r1 / 2 and tsc1 / 2 . 
ras / raf / mek pathway alterations ( 5.7% ; figs 1b and 1f ) included oncogenic braf mutations ( appendix fig a2 ) , braf / raf1 rearrangements , activating mutations in raf1 / araf , kras / nras / hras and map2k1 / 2 , and nf1 loss - of - function alterations . 
 chung et al cdk12 ga ( p , .001 ) , and braf rearrangements / mutations ( p , .001 ; fig 1b )  . to compare primary and metastatic site tumors , we assessed relative enrichment in gas ( fig 1g ; appendix table a3 )  . 
predicted germline mutations were identied in 57.8% of brca2 - , 25.0% of brca1 - , 35.8% of atm - , 80.0% of chek2 - , 52.2% of fanca - , 42.3% of msh2 - , 20.0% of msh6 - , 25.0% of mlh1 - , and 44.4% of pms2 - mutated cases ; only 9.2% of cdk12 - mutated cases harbored a predicted germline mutation ( fig 2c )  . genomic signatures : gloh in addition to gas in individual dna repair genes , genomic signatures represent the phenotypic readout of deleterious dna repair and are potential predictive biomarkers . 
we evaluated the association between gloh and dna repair gas ( fig 2d )  . consistent with the established relationship between brca1 / 2 and hrd , 21 brca1 / 2 - altered cases ( both predicted germline and somatic mutations ) were more frequently gloh - h compared with the overall data set ( fig 2d )  . to evaluate the potential relevance of non - brca1 / 2 dna repair genes as biomarkers for parp inhibition , we assessed their association with gloh . 
gloh - h frequency was comparable between the overall data set and cases with non - brca1 / 2 dna repair gas , although cases with homozygous deletions in non - brca1 / 2 hrr pathway or fa / icl pathway genes were more frequently gloh - h ( appendix fig a4b )  . 
 ( b ) frequency of major pathway alterations , including ets fusions , braf rearrangements / mutations , spop / cul3 mutations , cdk12 gas , idh1 / 2 mutations , ar gas , phosphatidylinositol 3 - kinase ( pi3k ) pathway gas , homologous recombination gas , g1 / s - cell cycle gas , wnt pathway gas , fanconi anemia / interstrand crosslink repair ( fa / icl ) repair pathway gas , ras / raf / mek pathway gas ( other than braf ) , mismatch repair gas , and pole mutations ( see figs 1c to 1f for details )  . 
 ( c to f ) gas identied in each pathway , including the ( c ) pi3k / akt / mammalian target of rapamycin ( mtor ) pathway , ( d ) g1 / s - cell cycle pathway , ( e ) wnt pathway , and ( f ) ras / raf / mek pathway ( nf1 mutation , rearrangement , or copy number loss ; braf or raf1 mutations or rearrangements ; araf , k / n / h - ras , or map2k1 / 2 mutations were included ) ; percent of altered cases is indicated . 
genes that were enriched ( difference between primary site v metastatic site frequency ) by at least 2% are indicated ( all p , .05 by fishers exact test [ two - tailed ] ) , with genes enriched at least twofold indicated in red ( all p , .001 by fishers exact test [ two - tailed ] )  . 
msi status was assessable for 3 , 326 cases , and overall , 87 of 3 , 326 of cases ( 2.6% ) were msi - h ( 2.0% primary site , 3.1% metastatic site tumors )  . 
for the remaining cases , tmb - h phenotype was not attributed to msi - h or pole . landscape of ets fusions and ar gas in total , 1 , 236 ets fusions were detected ( one sample harbored two ets fusions ; fig 1b )  . 
tmprss2 - erg comprised the majority ( 87.7% ) of ets fusions ( fig 3a ) , with the remaining consisting of etv1 ( 8.5% ) , etv4 ( 2.6% ) , and etv5 ( 1.2% ) with diverse fusion partners , including several not previously described ( fig 3b )  . 
we also identied breakpoints that juxtaposed tmprss2 with the intergenic region upstream of erg ( 0.1 to 75 kb upstream ; fig 3c ) ; similar upstream intergenic breakpoints were observed for tmprss2 fusions with etv4 ( 10 of 32 cases ) and etv5 ( two of 15 cases )  . ar gas are associated with castration - resistant disease and were most enriched in metastatic site tumors ( 39.7% of metastatic site and 3.7% of primary site tumors ; fig 1g )  . 
five hundred fty - ve of 557 cnas were amplications ( median copy number , 24 ; range , six to 366 ) ; two homozygous deletions that encompass exons 5 to 7 or exons 5 to 8 are likely activating.27 ar missense mutations were observed in 6.9% of cases ( 1.3% primary site and 11.9% metastatic site ) , and most were ligandbinding domain antiandrogen resistance mutations ( fig 4b ) .28 finally , ar rearrangements were observed in 1.3% of cases ( 0.4% primary site and 2.2% metastatic site ) ; however , because the sequencing strategy was not explicitly designed to detect ar rearrangements and does not fully cover ar intronic regions , the true frequency of ar rearrangements is difcult to establish . 
gas that co - occur with targetable gas ( fig 1b ) and their impact on response to therapy warrant consideration in biomarker - driven trials . msi - h and tmb - h have been associated with immunotherapy benet , 10 , 24 , 25 and gloh - h has been associated with parp inhibitor benet21 ; therefore , assessment of signatures of genomic instability potentially expands the population of patients addressable with immunotherapy or targeted therapy . we identied a subset of tmprss2 rearrangements fused to upstream intergenic regions of erg , etv4 , or etv5 as well as novel ets fusion partners . 
 cgp of primary and metastatic prostate tumors etv4 ( 32 ; 2.6% ) etv5 ( 15 ; 1.2% ) etv1 ( 105 ; 8.5% ) tmprss2 - erg ( 1 , 084 ; 87.7% ) etv1 etv4 etv5 intron 4 ( n = 38 ) erg gene ( nm_004449 chr21 : 40033704 - 39751950 ) intron 3 ( n = 940 ) intron 1 ( n = 58 ) upstream ( 108 bp - 75 kbp ) ( n = 39 ) intron 2 ( n = 9 ) erg exon 1 genomic coordinates : chr21 : 40020000 40040000 40060000 40080000 40100000 40120000 fig 3 . 
consistent with distinct molecular subsets of prostate cancer , 1 , 8 ets fusions were mutually exclusive with spop / cul3 , cdk12 mutations , or braf rearrangements / mutations that may potentially comprise a clinically relevant genomic subset.30 , 31 diverse ar gas can mediate androgen axis inhibitor resistance28 , 29 and were strongly enriched in metastatic site tumors . 
ar rearrangements that disrupted the ligand - binding domain can mediate resistance to current ar inhibitors.29 development of novel ar inhibitors that target the diverse spectrum of ar alterations is needed . 
 ( a ) ar genomic alterations ( gas ) were identied in 721 cases , including amplication ( red ) , mutation ( green ) , and rearrangements ( purple )  . 
of note , 11q13 amplication is associated with endocrine resistance in breast cancer and potentially targetable by broblast growth factor receptor inhibitors32 - 34 and , therefore , warrants investigation in prostate cancer . 
second , cdkn2a gas were enriched in metastatic site tumors ( 1.9 - fold ) , and although not previously described in primary versus metastatic studies , 1 - 3 acquired cdkn2a alterations were described in enzalutamide - resistant tumors.15 metastatic enrichment of cell cycle gas suggests that cdk4 / 6 inhibitors could be explored . 
 cgp of primary and metastatic prostate tumors certain hrr genes , mmr genes , or msi status ; identication of such dna repair ga by tumor sequencing warrants follow - up germline testing and genetic counseling . 
however , compared with a recent study , 3 we identify similar relative proportions of germline / somatic mutations for frequently mutated hrr genes ( brca2 , atm , chek2 )  . 
furthermore , another study of prostate cancer similarly identied germline mutations for many of the dna repair genes evaluated here.37 we also describe potential cdk12 germline mutations ( four of 12 were rs138292741 )  . 
although not identied in one recent study of cdk12 in prostate cancer , 8 germline truncating cdk12 mutations were described in other studies , cluding prostate cancer , 38 - 40 and in germline databases.40 although preclinical studies have identied non - brca1 / 2 hrr genes , their association with hrd phenotype in clinical samples is unclear . 
identication of gloh - h cases lacking dna repair gas ( appendix fig a4a ) may have clinical value , but further investigation in parp inhibitor trials is required to assess the clinical utility of gloh as a biomarker in prostate cancer . similarly , dna repair gas were associated with msi - h or tmb - h genomic signatures that are associated with benet from immunotherapy ( fig 2 ; appendix fig a5 )  . 
a subset of msi / tmb - h cases do not harbor corresponding dna repair gas potentially because gas may occur in genes involved in dna repair that have not yet been discovered , complex rearrangements with intronic breakpoints may be challenging to detect , or genomic instability can occur through mechanisms such as gene silencing or extrinsic dna damage . limitations of this study should be acknowledged . 
furthermore , because samples were collected for routine clinical testing , primary samples in this cohort may be biased toward patients who have received prior treatment or developed metastatic disease that resulted in a distinct genomic landscape from untreated primary tumors . 
chung employment : foundation medicine ninad dewal employment : foundation medicine stock and other ownership interests : foundation medicine ethan sokol employment : foundation medicine paul mathew honoraria : exelixis patents , royalties , other intellectual property : patent pending on new therapeutic invention travel , accommodations , expenses : exelixis robert whitehead employment : unitedhealthcare , cancer treatment centers of america sherri z . 
pal honoraria : novartis , medivation , astellas pharma consulting or advisory role : pzer , novartis , aveo , myriad pharmaceuticals , genentech , exelixis , bristol - myers squibb , astellas pharma , ipsen , eisai research funding : medivation richard j . 
lee consulting or advisory role : janssen pharmaceuticals , exelixis research funding : janssen pharmaceuticals andrea necchi employment : bayer ag ( i ) stock and other ownership interests : bayer ag ( i ) honoraria : roche , merck , astrazeneca , janssen pharmaceuticals , foundation medicine consulting or advisory role : merck sharp & dohme , roche , bayer ag , astrazeneca , clovis oncology , janssen pharmaceuticals , incyte , seattle genetics , astellas pharma , bristol - myers squibb , rainier therapeutics research funding : merck sharp & dohme ( inst ) , astrazeneca ( inst ) travel , accommodations , expenses : roche , merck sharp & dohme , astrazeneca , janssen pharmaceuticals other relationship : bayer ag ( i ) jeffrey p . 
gregg consulting or advisory role : astrazeneca , bristol - myers squibb , roche , foundation medicine speakers bureau : astrazeneca , foundation medicine , bristol - myers squibb primo lara jr honoraria : pzer consulting or advisory role : exelixis , pzer , astrazeneca , bayer ag , genentech , roche , janssen pharmaceuticals , bristol - myers squibb , abbvie , turnstone bio , foundation medicine , merck , cellmax life , nektar research funding : millennium pharmaceuticals ( inst ) , polaris ( inst ) , glaxosmithkline ( inst ) , genentech ( inst ) , aragon pharmaceuticals ( inst ) , janssen pharmaceuticals ( inst ) , heat biologics ( inst ) , tracon pharma ( inst ) , merck ( inst ) , pharmacyclics ( inst ) , incyte ( inst ) emmanuel s . 
antonarakis honoraria : sano , dendreon , medivation , janssen pharmaceuticals , essa , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , medivation , janssen pharmaceuticals , essa , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen pharmaceuticals ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : co - inventor of a biomarker technology that has been licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation vincent a . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : revolution medicines patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center jeffrey s . 
 cgp of primary and metastatic prostate tumors research funding : bayer ag ( inst ) , bristol - myers squibb ( inst ) , glaxosmithkline ( inst ) , medivation ( inst ) , takeda pharmaceuticals ( inst ) , novartis ( inst ) , pzer ( inst ) , bn immunotherapeutics ( inst ) , tracon pharma ( inst ) , rexahn pharmaceuticals ( inst ) , amgen ( inst ) , astrazeneca ( inst ) , active biotech ( inst ) , bavarian nordic ( inst ) , calithera biosciences ( inst ) , celldex ( inst ) , eisai ( inst ) , genentech ( inst ) , immunomedics ( inst ) , janssen pharmaceuticals ( inst ) , merck ( inst ) , newlink genetics ( inst ) , prometheus ( inst ) , sano ( inst ) no other potential conicts of interest were reported . references abeshouse a , ahn j , akbani r , et al : the molecular taxonomy of primary prostate cancer . 
nat genet 50 : 645 - 651 , 2018 abida w , armenia j , gopalan a , et al : prospective genomic proling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making . 
n engl j med 373 : 1697 - 1708 , 2015 de bono js , de giorgi u , massard c , et al : pten loss as a predictive biomarker for the akt inhibitor ipatasertib combined with abiraterone acetate in patients with metastatic castration - resistant prostate cancer ( mcrpc )  . 
mateo j , ganji g , lemech c , et al : a rst - time - in - human study of gsk2636771 , a phosphoinositide 3 kinase beta - selective inhibitor , in patients with advanced 8 . 
clin cancer res 23 : 5981 - 5992 , 2017 2018 lee l , ali s , genega e , et al : aggressive - variant microsatellite - stable pole mutant prostate cancer with high mutation burden and durable response to immune checkpoint inhibitor therapy . 
cell 161 : 1215 - 1228 , 2015 [ erratum : cell 162 : 454 , 2015 ] joseph jd , lu n , qian j , et al : a clinically relevant androgen receptor mutation confers resistance to second - generation antiandrogens enzalutamide and arn509 . 
han gc , hwang j , wankowicz sam , et al : genomic resistance patterns to second - generation androgen blockade in paired tumor biopsies of metastatic castration - resistant prostate cancer . 
mateo j , chakravarty d , dienstmann r , et al : a framework to rank genomic alterations as targets for cancer precision medicine : the esmo scale for clinical actionability of molecular targets ( escat )  . 
bajrami i , frankum jr , konde a , et al : genome - wide proling of genetic synthetic lethality identies cdk12 as a novel determinant of parp1 / 2 inhibitor sensitivity . 
blazek d , kohoutek j , bartholomeeusen k , et al : the cyclin k / cdk12 complex maintains genomic stability via regulation of expression of dna damage response 21 . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
coleman rl , oza am , lorusso d , et al : rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
carbone dp , reck m , paz - ares l , et al : first - line nivolumab in stage iv or recurrent non - small - cell lung cancer . 
giltnane jm , hutchinson ke , stricker tp , et al : genomic proling of er + breast cancers after short - term estrogen suppression reveals alterations associated with endocrine resistance . 
luen sj , asher r , lee ck , et al : association of somatic driver alterations with prognosis in postmenopausal , hormone receptor - positive , her2 - negative early breast cancer : a secondary analysis of the big 1 - 98 randomized clinical trial . 
soria j - c , debraud f , bahleda r , et al : phase i / iia study evaluating the safety , efcacy , pharmacokinetics , and pharmacodynamics of lucitanib in advanced solid tumors . 
brovkina oi , shigapova l , chudakova da , et al : the ethnic - specic spectrum of germline nucleotide variants in dna damage response and repair genes in hereditary breast and ovarian cancer patients of tatar descent . 
popova t , mani e e , boeva v , et al : ovarian cancers harboring inactivating mutations in cdk12 display a distinct genomic instability pattern characterized by large tandem duplications . 
abida w , bryce ah , vogelzang nj , et al : preliminary results from triton2 : a phase ii study of rucaparib in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) associated with homologous recombination repair ( hrr ) gene alterations . 
clarke n , wiechno p , alekseev b , et al : olaparib combined with abiraterone in patients with metastatic castration - resistant prostate cancer : a randomised , double - blind , placebo - controlled , phase 2 trial . 
 cgp of primary and metastatic prostate tumors appendix methods approval for this study , including a waiver of informed consent and health insurance portability and accountability act waiver of authorization , was obtained from the western institutional review board ( protocol 20152817 )  . 
comprehensive genomic proling ( cgp ) results were reported clinically by prospective sequencing of tissue samples from 3 , 476 unique patients with prostate cancer ( august 2014 to february 2018 ) using a validated hybrid capture - based cgp assay ( foundationone [ baitset version t7 was used during this period ] ) 16 in a clinical laboratory improvement amendmentscertied , college of american pathologistsaccredited , new york stateapproved laboratory ( foundation medicine , cambridge , ma )  . 
for patients with multiple submitted samples , only a single sample was included , and the sample with the highest sequencing quality metrics was included . age and site of specimen collection were abstracted from the accompanying pathology reports , clinical notes , and requisition forms submitted by the treating physician . 
specimens included 1 , 660 primary site tumors and 1 , 816 metastatic site tumors ( appendix fig a1 )  . the pathologic diagnosis of each case was conrmed on routine hematoxylin and eosinstained slides , and all samples forwarded for dna extraction contained a minimum of 20% tumor nuclei . 
cgp was performed on hybridization - captured , adaptor ligation - based libraries to a median coverage depth of 743 for 395 cancer - related genes plus select introns from 31 genes frequently rearranged in cancer ( appendix table a1 )  . 
for ets fusions , targeted regions were tmprss2 ( introns 1 to 3 ) , erg ( all exons ) , etv1 ( introns 3 to 4 ) , etv4 ( intron 8 ) , and etv5 ( introns 6 to 7 )  . insertions / deresults were analyzed for base substitutions , short letions , rearrangements , and copy number alterations ( amplication and homozygous deletion )  . 
genomic alterations ( gas ) were called as reportable if the specic variant was present in the catalog of somatic mutations in cancer database ( forbes et al : nucleic acids res 45 : d777 - d783 , 2017 ) , if the variant has been characterized as pathogenic , or if the variant had likely functional status ( disruptive alterations in tumor suppressor genes ) ; all other variants were classied as variants of unknown signicance . to compare relative enrichments in primary site and metastatic site tumors , genes altered at a 2% or greater frequency were assessed for enrichment . 
enrichment was dened as the difference in frequency of gene alteration between metastatic site and primary site samples . to determine microsatellite instability status , 114 intronic homopolymer repeat loci on the foundationone panel were analyzed for length variability and compiled into an overall microsatellite instability score through principal components analysis ( chalmers et al : genome med 9 : 34 , 2017 )  . 
tumor mutational burden was calculated as the number of somatic base substitutions or insertions / deletions per megabase of the coding region target territory of the test ( 1.1 mb ) after ltering to remove known somatic and deleterious mutations and extrapolating that value to the exome or genome as a whole ( chalmers et al : genome med 9 : 34 , 2017 )  . 
tumor mutational burden was categorized as low ( fewer than six mutations / mb ) , intermediate ( six to 20 mutations / mb ) , or high ( 20 mutations / mb or more ; chalmers et al : genome med 9 : 34 , 2017 )  . 
germline , somatic , and zygosity statuses for mutations were determined without matched normal tissue as previously described17 ; in validation testing of 480 germline / somatic calls from tumor - only sequencing with matched normal reference samples , accuracy was 95% for somatic calls and 99% for germline calls . 
biallelic inactivation was dened as mutations under loss of heterozygosity ( loh ) as determined by zygosity status.17 percent genome - wide loh ( gloh ) was used as a marker of homologous recombination deciency and calculated as described , and a gloh score of 14% or greater was dened as gloh - high.21 potentially targetable gas were dened as those that have been associated with response to targeted therapy in prostate cancer , homologous recombination repair gas that have been associated with responses to poly ( adp - ribose ) polymerase inhibitors , or gas associated with response to targeted therapy in multiple other tumor types and were ranked according to modied european society for medical oncology scale for clinical actionability of molecular targets criteria.18 ln ( unk ) ln ( d ) ln ( l ) liver bone lung other prostate ( n = 1 , 660 ) metastasis ( n = 1 , 816 ) neuroendocrine ( 4% ) undifferentiated ( 3% ) acinar ( 93% ) fig a1 . 
for fusion , exons ( e ) are annotated with the last exon included in the 5 ( cid : 3 ) partner and the rst exon included in the 3 ( cid : 3 ) partner . 
in addition , braf rearrangements at intron 9 ( n = 6 ) and intron 7 ( n = 1 ) and raf1 rearrangement at intron 7 with no clear fusion partner were identied ( data not shown )  . 
 ( a ) genome - wide loss of heterozygosity ( gloh ) score was assessable for 2 , 624 cases , and cases with 14% or more gloh were designated loh - high ( loh - h )  . 
loh - h cases were assessed for the presence ( green ) or absence ( yellow ) of a genomic alteration ( ga ) in the homologous recombination repair ( hrr ) or fanconi anemia / interstrand crosslink repair ( fa / icl ) pathway . 
 ( b ) genes were grouped together into hrr pathway ( excluding non - brca1 / 2 ) or fa / icl pathway ( fanc ) ; genes were categorized as in figure 2a . 
 ( a ) microsatellite instability ( msi ) status was assessable for 3 , 326 cases , and each case was designated as msi - high ( msi - h ) , msi - low ( msi - l ) , or microsatellite stable ( mss )  . 
the percent tmb - high ( tmb - h ) or tmb of 10 or more mutations ( mut ) / mb cases in primary site and metastatic site tumors is indicated . 
 cdkn2c - null leiomyosarcoma : a novel , genomically distinct class of tp53 / rb1wild - type tumor with frequent cic genomic alterations and 1p / 19q - codeletion erik a . 
here , we searched for recurrent actionable genomic alterations in lms that occur in the absence of common untreatable oncogenic drivers . methods tissues from 276 , 645 unique advanced cancers , including 2 , 570 uterine and soft tissue lms , were sequenced by hybrid - capturebased next - generation dna and rna sequencing / comprehensive genomic proling of up to 406 genes . 
we further validated our ndings in two publicly available datasets : the cancer genome atlas and the project genie initiative . conclusion cdkn2c - null lms denes a genomically distinct tumor that may have prognostic and / or therapeutic clinical implications , including possible use of specic cyclin - dependent kinase inhibitors . jco precis oncol 4 : 955 - 971 . 
 williams et al context key objective leiomyosarcoma ( lms ) , an aggressive tumor with limited curative options , shows frequent mutations in tp53 and rb1 but few actionable genomic alterations . 
here , we searched for recurrent actionable genetic alterations in lms . knowledge generated a novel , genomically distinct class of lms ( 3.0% ; 77 of 2 , 570 cases ) harbor homozygous loss of cdkn2c , which encodes the cyclin - dependent kinase inhibitor - 2c . 
cdkn2c - null lms lack typical tp53 and rb1 mutations ; show concurrent homozygous deletion of cic , cdkn2a , and rad51b ; and show frequent 1p / 19q - codeletion . relevance the nding of recurrent cdkn2c - null lms provides insight into tumor biology and raises the possibility for use of specic cyclin - dependent kinase inhibitors in this aggressive disease . from the uterus , with signicantly low frequency of tp53 and rb1 gas . methods cohort and genomic analyses comprehensive genomic proling was performed in a clinical laboratory improvement amendmentscertied , college of american pathologistsaccredited laboratory ( foundation medicine , cambridge , ma )  . 
20% estimated percent tumor nuclei in each case , for which the percent tumor nuclei equals 100 times the number of tumor cells divided by total number of nucleated cells . 
the samples were assayed by adaptor ligation hybrid capture , performed for all coding exons of 236 ( v1 ) , 315 ( v2 ) , or 405 ( v3 ) cancer - related genes plus select introns from 19 ( v1 ) , 28 ( v2 ) , or 31 ( v3 ) genes frequently rearranged in cancer ( appendix table a1 ) .11 , 12 for samples with available rna , targeted rna sequencing was performed for rearrangement analysis in 265 genes.12 sequencing of captured libraries was performed using the illumina hiseq 4000 system ( illumina , san diego , ca ) to a mean exon coverage depth of targeted regions of  . 500 , and sequences were analyzed for gas , including short variant alterations ( base substitutions , insertions , and deletions ) , copy number alterations ( focal amplications and homozygous deletions ) , and select gene fusions or rearrangements.11 , 13 , 14 to maximize mutation detection accuracy ( sensitivity and specicity ) in impure clinical specimens , the test was previously optimized and validated to detect base substitutions at a 5% mutant allele frequency , indels with a 10% mutant allele frequency with 99% accuracy , and fusions occurring within baited introns / exons with  . 
6 - 8 copies depending on tumor ploidy and homozygous deletions was performed as previously described.11 in brief , the aligned dna sequences of each tumor specimen were normalized against a process - matched normal , producing log - ratio and minor allele frequency data . 
a gibbs sampler tted copy number model and a grid - based model were tted to the segmented log - ratio and minor allele frequency data , producing genome - wide copy number estimates . 
finally , the degrees - of - t of candidate models returned by gibbs sampling and grid sampling were compared , and the optimal model was selected by an automated heuristic . signal - to - noise ratios for each genomic segment were used to determine gain or loss per chromosome arm on the basis of tumor purity and ploidy ; the sum of segment sizes determined the fraction of each arm gained or lost . chromosomes were assessed for arm - level aneuploidy , dened as positive if  . 
the cohort of cdkn2c - null lms comprised 77 cases , each from a different patient , that were submitted to foundation medicine for comprehensive genomic proling during routine clinical care . 
human investigations were performed after approval by a local human investigations committee and in accordance with an assurance led with and approved by the department of health and human services , when appropriate . 
clinicopathologic data , including patient age , sex , tumor site , and figo stage or ajcc ( 8th edition ) stage , were extracted from the accompanying pathology report.4 , 16 primary site data were not available for a subset of patient cases ( indeterminant primary )  . 
these patients were signicantly older than the remainder of the lms cohort ( median age , 61 v 57 years ; p = .0009 , mann - whitney u test )  . 
patients were enriched for female sex compared with the remainder of the lms cohort ( 99% [ 76 of 77 ] v 79% [ 1 , 968 of 2 , 493 ] ; p , .0001 , fishers exact test )  . 
six female patients had a prior history of leiomyomatosis ( n = 2 ) or uterine smooth muscle tumor of uncertain malignant potential ( stump ; n = 4 )  . 
the majority of cdkn2c - null lms patients showed clinically advanced / metastatic disease , with 62% of conrmed uterine primary occurrences documented at figo stage iv ( n = 34 of 55 ) and 86% of indeterminant or soft tissue primary cases documented at ajcc stage iv ( n = 19 / 22 ) , as summarized indeterminant figo staging ( uterine primary ) no . 
locations of the sequenced tumor specimens are summarized in appendix table a2 . comprehensive genomic proling of cdkn2c - null lms the distribution of gas in the 77 cdkn2c - null lms is displayed in figure 1 . 
the frequent gas were identied in cic at 19q13.2 , most cdkn2a , and rad51b ( table 2 ) , and unsupervised analysis showed signicant enrichment of these alterations in the cdkn2c - null cohort ( appendix fig a1 )  . 
no other signicant differences based on age were identied . comparison of patient cases on the basis of clinical stage , three patients had two separate tissue specimens analyzed ( appendix table a4 )  . 
additional recurrent chromosomal arm - level changes were identied in the 72 patient cases available , including most frequently aneuploidy of chromosomes 6p ( n = 35 ) , 9p ( n = 19 ) , 10q ( n = 28 ) , 11p ( n = 39 ) , 13q ( n = 46 ) , 14q ( n = 46 ) , and 16q ( n = 52 )  . a review of 1p / 19q - codeletion status in available lms patient cases without homozygous deletion of cdkn2c ( n = 1 , 212 ) revealed 62 1p / 19q - codeleted lms ( 5% ; fig 2c )  . 
all four occurred in uterine lms ( one of which with a history of stump )  . all non - lms sarcoma patient cases in the foundation medicine dataset ( n = 12 , 097 ) were evaluated for cdkn2c status . 
these included diverse sarcoma diagnoses , including six high - grade sarcomas not otherwise specied , two osteosarcomas , two malignant peripheral nerve sheath tumors , and two inammatory myobroblastic tumors . 
both were alk rearrangementpositive tumors in women ( ages , 63 and 72 years )  . we also searched our entire lms cohort ( n = 2 , 570 ) for cases with pathogenic alterations in cdkn2c other than homozygous deletion . 
 ( a ) cdkn2c - null lms with a truncating variant in cic ( p.q907 * ) and homozygous deletion of cdkn2a at chromosome 9p21.3 ( red arrow )  . 
 ( c ) cdkn2c - retained lms with deep deletion of rb1 at chromosome 13q14.2 ( red arrow ) and a cn plot of high complexity . and rad51b were identied ; 1p / 19q status was not available . histopathology histopathologic evaluation was performed on all available high - resolution digital pathology h&e slides of our cohort of cdkn2c - null lms ( n = 70 )  . 
histopathology of cdkn2c - null leiomyosarcoma ranged from ( a , b ) epithelioid to ( c ) spindled ( hematoxylin & eosin [ h&e ] stains , 200 )  . 
 ( d ) occasional cases showed focal myxoid histology ( h&e stain , 200 )  . progesterone receptor ( 24 of 26 ; remaining two with focal positivity )  . 
cdkn2c - null lms were also positive for desmin ( 30 of 33 ; remaining three with focal positivity ) , smooth muscle actin ( 25 of 25 ) , muscle - specic actin ( 11 of 11 ) , and caldesmon ( 6 of 6 )  . 
patient cases showed frequent homozygous loss of cic ( n = 5 [ 42% ] of 12 ) , cdkn2a ( n = 4 [ 33% ] of 12 ) , and rad51b ( n = 3 [ 25% ] of 12 ) , and all were wild type for tp53 , rb1 , and atrx ( n = 12 of 12 )  . discussion in 2 , 570 patient cases of lms , cdkn2c - null lms ( n = 77 ; 3.0% ) comprised a genomically distinct molecular subgroup . cdkn2c - null lms typically lacked mutations in tp53 , rb1 , and atrx but showed frequent 1p / 19q - codeletion ( 81% ) , and nearly half ( 40.3% ) showed homozygous deletion or inactivating truncations of cic . 
 cdkn2c loss denes class of tp53 / rb1wild - type leiomyosarcoma which enhances fas - mediated apoptosis , and its loss may contribute to tumor pathogenesis.29 the cic gene on chromosome 19q13.2 represses genes induced downstream to rtk pathway activation.30 in the absence of rtk signaling , cic blocks transcription of genes that have diverse effects on cellular proliferation , metabolism , and migration.31 along with single copy loss of cic on 19q , concurrent inactivating mutations in cic are identied in a high percentage of oligodendrogliomas.32 whole - arm 1p / 19q - codeletion , with concurrent mutation in idh1 or idh2 , is entity - dening for oligodendrogliomas.33 - 35 oligodendrogliomas are associated with relatively long overall survival , and treatment strategies are often stratied on the basis of 1p / 19q status.36 - 38 the codeletion is a result of unbalanced translocation between two chromosomes , with subsequent loss of der ( 1 ; 19 ) ( p10 ; q10 ) , likely because chromosomes 1 and 19 are near each other in the nonrandom organization of the nucleus.39 - 41 a large percentage of oligodendrogliomas also show cic and fubp1 mutations.31 our cohort of cdkn2c - null lms shows notable similarities and differences to oligodendroglioma ; 40% of our cohort showed an inactivating alteration in cic , most commonly homozygous deletion . 
rare sarcoma - like tumors originating from oligodendrogliomas have been reported , with documented idh1 mutation and 1p / 19q - codeletion , and have been termed oligosarcoma.42 - 44 rodriguez et al43 identied 6 of 7 patient cases of oligosarcoma with at least focal smooth muscle actin positivity of the sarcomatous component by immunohistochemistry and one patient case with smooth muscle differentiation by electron microscopy . 
these results indicate a similarity in differentiation to our cohort of lms . among all sarcomas with cdkn2c loss , 1p / 19q - codeletion appears to be nearly exclusive to lms . 
in our overall lms cohort , however , occasional cdkn2c - retained lms showed tp53 and rb1 alterations and were positive by the 1p / 19qcodeletion detection algorithwe speculate that , given the complexity of these genomically unstable occurrences , occasional cdkn2c - retained lms satisfy these criteria ( fig 2c )  . as such , identication of homozygous deletion of cdkn2c may be the most specic distinguishing feature . cytogenetic ndings in lms and leiomyoma have been previously reported , although without characterization of cdkn2c status . 
a greater frequency of 1p loss has been documented in metastasized lms.45 from a cytogenetics study of 800 uterine leiomyomata , nine diploid occurrences with 1p loss were identied , with other associated alterations , particularly chromosome 19 and / or chromosome 22 loss.46 transcriptional proling of two of the 1p - deleted leiomyomas in that study showed alignment with malignant lms in a hierarchical clustering analysis.46 in another study , 1p loss was identied in approximately one quarter of uterine cellular leiomyomata.47 three reports on a total of eight pulmonary - based benign metastasizing leiomyoma reported 19q and 22q terminal deletion in each case.48 - 50 rare uterine leiomyomas with gas in rad51b have also been identied.51 the overlap in gas between our cohort of cdkn2c - null lms and a subset of leiomyoma of uncertain cdkn2c status in the literature suggests a possible connection between these entities . evaluations of gas in epithelioid or myxoid uterine smooth muscle neoplasms are limited in the literature.52 - 56 although a high percentage of cdkn2c - null lms in our study demonstrated epithelioid features on histology , histology was also varied . 
immunohistochemistry results extracted from pathology reports were typical for uterine lms , with expression of characteristic smooth muscle markers.57 given the overall low response rate of lms to standard therapies , the identication of this targetable alteration in cdkn2c may be useful for treatment decisions . 
cdk4 / 6 inhibitors have previously shown effectiveness in a lms with a cdkn2a alteration.10 nearly half of the cdkn2c - null lms harbored loss of cdkn2a ; cdk4 / 6 inhibitors may be effective in replacing the loss of inhibition of cdk4 / 6 that results from cdkn2c and cdkn2a loss in these patient cases that recur after standard chemotherapy regimens . 
a minor subset of cdkn2c - null and / or 1p / 19q - codeleted lms harbored activating fusions in alk , braf , fgfr1 , and ntrk1 , for which targeted inhibitors may be of utility.9 limitations of this study include its retrospective nature and the enrichment for aggressive tumors , mostly metastatic to distant sites . 
the latter may be due to collection bias from submission of specimens later in the disease course . additional studies will be needed to correlate the nding of cdkn2c loss in lms with prognostic data and treatment outcomes . 
williams , md , 150 second st , cambridge , ma 02141 ; twitter : @erikawilliamsm1 ; e - mail : erwilliams@foundationmedicine.com. meagan montesion stock and other ownership interests : roche ethan s . 
hoffmann - la roche radwa sharaf employment : foundation medicine stock and other ownership interests : roche brennan decker stock and other ownership interests : avidea technologies consulting or advisory role : foundation medicine , avidea technologies kevin jon williams stock and other ownership interests : hygieia , gemphire therapeutics consulting or advisory role : gemphire therapeutics research funding : novo nordisk jeffrey m . 
venstrom employment : genentech , foundation medicine leadership : genentech stock and other ownership interests : genentech research funding : genentech , roche , foundation medicine travel , accommodations , expenses : genentech brian m . 
alexander employment : foundation medicine leadership : foundation medicine stock and other ownership interests : roche research funding : eli lilly ( inst ) , puma ( inst ) , celgene ( inst ) ( optional ) open payments link : physician / 854258 / summary jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : celsius therapeutics research funding : foundation medicine lee a . 
elvin employment : foundation medicine no other potential conicts of interest were reported . acknowledgment we thank the american association for cancer research and appreciate its nancial and material support in the development of the american association for cancer research project genie registry , and we thank members of the consortium for their commitment to data sharing . references roberts me , aynardi jt , chu cs : uterine leiomyosarcoma : a review of the literature and update on management options . 
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holzmann c , markowski dn , koczan d , et al : genome - wide acquired uniparental disomy as well as chromosomal gains and losses in a uterine epithelioid leiomyoma . 
reyes c , karamurzin y , frizzell n , et al : uterine smooth muscle tumors with features suggesting fumarate hydratase aberration : detailed morphologic analysis and correlation with s - ( 2 - succino ) - cysteine immunohistochemistry . 
 cdkn2c loss denes class of tp53 / rb1wild - type leiomyosarcoma appendix attribute negative not significant positive % frequency cdkn2c faf1 tp53 sex : male atrx chr2p_loss chr1p_loss cdkn2a cdkn2b rad51b sex : female chr19q_loss chr14q_loss log2 odds ratio fig a1 . 
red and blue indicate positive and negative correlation , respectively , in cdkn2c - null leiomyosarcoma ( n = 77 ) compared with the remainder of the leiomyosarcoma cohort ( n = 2 , 493 )  . 
 clinical use of precision oncology decision support purpose precision oncology is hindered by the lack of decision support for determining the functional and therapeutic significance of genomic alterations in tumors and relevant clinically available options . 
to bridge this knowledge gap , we established a precision oncology decision support team that provides annotations at the alteration level and subsequently determined whether clinical decision making was influenced . methods genomic alterations were annotated to determine actionability on the basis of a variants known or potential functional and / or therapeutic significance . 
a webbased survey was implemented to capture the reasons genotype - matched therapies were not pursued . results the precision oncology decision support team processed 1 , 669 requests for annotation of 4 , 084 alterations ( 2 , 254 unique ) across 49 tumor types for 1 , 197 patients . 
sixty - six percent of patients had at least one actionable / potentially actionable alteration , and 20.6% of patients ( 110 of 535 ) annotated enrolled in a genotype - matched trial . 
clinicians cited a variety of reasons that patients with actionable alterations did not enroll in trials . conclusion over half of alterations annotated were of unknown significance or nonactionable . physicians were more likely to enroll a patient in a genotype - matched trial when an annotation supported actionability . 
 research indicates that clinicians are unlikely to use sources that take longer than 30 seconds to retrieve data10 and that information presented in graphical summaries enhances interpretation , improving health care quality.11 , 12 second , limited information may be exposed because these web sites are public facing . 
third , novel alterations continue to be discovered , and information is rapidly evolving , generally outpacing the rate of updates . thus , there is a need for an on - demand , real - time clinical interpretation service that annotates all requested alterations , beyond those available within accessible knowledge bases , to determine their actionability . the precision oncology decision support system ( pods ) was established at the university of texas md anderson cancer center in recognition of these needs.9 herein , we report our experience with large - scale , institution - wide decision support and its initial clinical utility . 
all requestors indicating the same physician as the contact for correspondence were considered a teastatistical significance was evaluated by a x2 test . annotation process and return of reports pods scientists receive requests , access our knowledge base of variant annotations , and review and update content as applicable.9 , 13 reports consist of a data summary with references and alteration frequency from external ( cbioportal , cosmic [ catalogue of somatic mutations in cancer ] ) and internal databases . 
in 2015 , reports evolved to routinely contain a functional significance , gene , and alteration - level actionability call ( table 1 ) .7 , 12 all reports are reviewed by the medical director and returned via e - mail . 
starting in august 2015 , reports referencing clia - validated panels were deposited within md andersons electronic health record ( ehr )  . manual review of clinical data medical records of 539 patients annotated in 2015 through clinician - initiated requests or for treatment planning conferences were reviewed for the presence of a clinical trial entrance note in the patients ehr . 
potential matches between the annotated variants and targeted therapy used within the trial were manually recorded . clinical decision follow - up surveys a web - based survey was initiated in 2015 , and 236 surveys were sent to annotation requestors with a 1 - month postannotation delivery date to ascertain whether the patient matched to genomically guided therapy . 
for patients not enrolled to receive therapy on the basis of the annotation provided , the survey inquired as to the reasons why . results patient annotation requests the pods team processed 1 , 669 requests for 1 , 197 patients , most in 2014 and 2015 ( data supplement )  . 
multiple requests for the same patient may have been due to additional alterations requested for annotation , different clinicians requesting annotation of the same molecular report , or the same molecular report requested for different venues in which the patient was evaluated ( eg , clinic visit v treatment planning conference )  . 
clinician - initiated requests originated from treating physicians and team members for point - of - care decisions on the basis of molecular testing or from clinical trial teams screening for patients to enroll in genotype - matched trials . fifty - six physician teams initiated requests for 724 patients and ranged from one to 176 per team , with two requests being the median ( data supplement )  . 
because not all aspects of protein function can possibly be determined , the functional significance is likely benign there is peer - reviewed published literature showing that the alteration has an inactivating or inferred inactivating effect on an oncogene . there is peer - reviewed published literature showing that the alteration has an activating or inferred activating effect on a tumor suppressor that enhances its function as a tumor suppressor overall , 4 , 084 variant - level annotations were provided for 2 , 254 unique alterations . 
genes most commonly annotated as part of a full panel request included tp53 , kras , and pik3ca , representing the three most commonly mutated genes in the genome ( fig 1c )  . 
the percentage of requests is shown for ( a ) each indicated tumor type ( top 25 ) and ( b ) annotation type ( full panel or select alterations )  . 
genes with 20 or more annotations are shown . actionable genes and alterations a gene is actionable if there are clinically available therapies that directly or indirectly targe alterations in the gene and / or there are clinical trials selecting for alterations in the gene . of the 4 , 084 annotations , 3 , 166 ( 78% ) were within a gene defined as actionable at the time of annotation ( fig 2a ; data supplement )  . 
in 2015 , annotation reports evolved to contain an actionable variant call describing the alterations functional and therapeutic significance , with classification into four broad categories actionable ( further subcategorized by source : literature based , inferred , or functional genomics ) , potentially actionable , unknown , and nonactionable ( table 1 ) 9which was provided with 2 , 444 annotations delivered for 669 patients . 
a total of 794 ( 32.5% ) annotations were actionable , 230 ( 9.4% ) were potentially actionable , 725 ( 29.7% ) were unknown , and 697 ( 28.4% ) were not actionable ( fig 2b )  . 
the total number of annotations in 2015 and the subset that was actionable / potentially actionable are shown per the patients tumor type ( fig 2e and data supplement , respectively )  . 
the actionability of kras has been controversial , particularly in colorectal cancer.14 - 16 when excluding kras as actionable , most actionable annotations were provided for breast cancer patients ( n = 90 ; data supplement )  . clinical utility of annotations we then asked whether physicians acted more often on alterations with evidence of actionability ( data supplement )  . 
we manually recorded clinical follow - up data by accessing the ehrs of 539 patients requested for annotation by clinicians or for treatment planning conferences . four patients were excluded : two had mutations that were actionable only for resistance to therapy , and two because of insufficient follow - up since physician notification . 
for the remaining 535 patients , variant annotation data were filtered , such that each patient in the data set is represented by a single alteration ( fig 3a )  . 
the fraction of patients represented by the highest variant call ( yellow column ) and the corresponding fraction of patients with that call enrolled in a trial ( gray column )  . 
the fraction of patients represented by the highest variant call ( yellow column ) and the corresponding fraction of patients with that call enrolled in a trial ( gray column )  . 
of patients with variant call enrolled in a trial ( % ) yes : literature based 214 ( 40.0 ) 49 ( 22.9 ) yes : inferred 54 ( 10.1 ) 26 ( 48.1 ) potentially 65 ( 12.1 ) 17 ( 26.2 ) unknown 136 ( 25.4 ) 16 ( 11.8 ) no ( nonactionable ) 66 ( 12.3 ) 2 ( 3 ) p < .001 actionable / potentially actionable alterations unknown alterations nonactionable alterations actionable variant classification total no . 
alterations of 214 patients ( 40% ) were classified into the yes : literature based category ; 54 ( 10.1% ) were classified into the yes : inferred category ; 65 ( 12.1% ) were classified into the potentially category ; 136 ( 25.4% ) were classified into the unknown category ; and 66 ( 12.3% ) were classified into the no ( nonactionable ) category ( fig 3a , yellow column )  . 
patients with actionable alterations in pten ( n = 20 ) , pik3ca ( n = 11 ) , and erbb2 ( n = 10 ) most frequently enrolled in a trial ( fig 4 ) , paralleling the data showing a large number of actionable / potentially actionable annotations delivered for pik3ca and pten ( fig 2d ; data supplement )  . to understand why physicians may not have acted on potentially actionable alterations , we introduced a web - based survey in 2015 to accompany physician - initiated requests . 
a combination of survey responses and manual review revealed that 26.8% of annotations ( 59 of 221 ) led to a genotypematched trial ( fig 3c , gray column )  . 
the latter had another well - characterized oncogenic variant ( idh1 r132c , akt1 e17k , or fgf3 and fgf4 amplifications ) or an alteration clearly inferable as actionable ( early truncating ptch1 mutation ) , where either decision support was not needed or was previously supplied outside the survey group . finally , three patients ( 3.3% ) elected to be treated elsewhere . among 161 patients with variants classified as yes : literature based and yes : inferred , there were fig 4 . 
reasons patients did not enroll in genotype - matched trials after precision oncology decision support annotations , as stated by the survey respondents patients ( n = 161 ) patients with yes : literature based and yes : inferred variants ( n = 42 ) patients with variants annotated as potentially actionable ( n = 29 ) patients with variants annotated as unknown and no for actionability ( n = 90 ) 71 ( 44.1 ) 5 ( 11.9 ) 9 ( 31.0 ) 57 ( 63.3 ) reasons patient did not enroll in trial physician stated annotation does not support trial enrollment , no . 
reasons included another alteration pursued ( two patients ) , the patient was responding to current therapy ( six patients ) , and the patient elected treatment elsewhere ( nine patients )  . 
other reasons included nongenotype - matched treatment options pursued ( five patients ) and ineligibility ( 11 patients )  . in five instances , physicians indicated that the annotation did not support trial enrollment , which we investigated further . 
 toxicity - related deaths in patients treated with targeted therapies.17 - 20 however , few biomarkers have an indication for treatment with a food and drug administrationapproved drug specific to the patients tumor type , 21 - 27 and a limited number of patients with potentially actionable alterations receive genotype - matched therapies in experimental contexts.3 - 7 one contributing factor may be a lack of decision support , as suggested by the cancer genome evaluation committee , which found that physicians are often overwhelmed by data of uncertain significance and that sound guidelines are essential for determining clinical action.28 moreover , we previously reported modest differences in trial enrollment between patients with or without potentially actionable alterations.3 assessing a new population of patients where decision support was provided , we observed that physicians acted more often when the function of the alteration was known . the necessity for real - time decision support is clear from the large volume of requests received from numerous physicians ( data supplement ) treating patients with diverse tumor types for alterations in a range of genes . 
however , bias likely exists toward physicians leading targeted therapy trials and for genes targeted by those therapies . the pods team is frequently asked to provide an annotation for sequencing reports from commercial vendors that produce end - to - end reports , some already containing alteration - level annotations . distinguishing factors of pods reports are a clear call of functional effect9 ( eg , activating , inactivating , unknown ) , a range of variant - level actionability categories on the basis of experimental evidence , and inclusion of all md anderson genotype - matched clinical trials in current reports . previous studies reported high rates of alterations in actionable genes , 4 , 29 - 33 and we provided an annotation in at least one actionable gene for 97% of patients in our cohort . 
using the target ( tumor alterations relevant for genomics - driven therapy ) database and phial ( precision heuristics for interpreting the alteration landscape ) algorithm to rank alterations followed by manual annotation for only selected patients , a study showed that 90% of patients have clinically relevant alterations.34 conversely , we found that 66% of patients annotated have at least one potentially actionable alteration on the basis of manual curation of all aberrations . 
potential differences between the studies include ( 1 ) the inclusion of potentially actionable diagnostic or prognostic alterations by van allen et al34 and not in our study ; ( 2 ) we provided annotations for only requested alterations , and few annotation requests were obtained for well - established alterations ( eg , braf v600e ) ; and ( 3 ) the difference in the number of patients assessed by manual curation in the two studies . among all annotations with an actionable variant call , only 32.5% were classified as actionable , with another 9.4% classified as potentially actionable . even within genes that are considered actionable , 47.4% of the annotations either had no evidence to support actionability or were not actionable . moreover , 58% of the genomic alterations annotated and evaluable for frequency have not been reported in the cosmic database ( data supplement )  . 
these data highlight the need to define actionability at the variant , rather than gene , level . to determine whether physicians acted according to the evidence presented in the pods reports , we followed 535 patients . 
thus , physicians more often act on alterations when sufficient evidence is provided that they may be driver events . the most often - cited reason that patients did not enroll in genotype - matched trials was that the annotation did not support trial enrollment . 
mills shaw , john mendelsohn , funda meric - bernstam provision of study materials or patients : sarina piha - paul , vivek subbiah , david hong , kenna r . 
mills shaw , funda meric - bernstam data analysis and interpretation : amber johnson , yekaterinab . khotskaya , lauren brusco , jia zeng , vijakumar holla , ann m . bailey , md abu shufean , russell broaddus , gordon b . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . jia zeng stock and other ownership interests : amgen , mckesson , mylan , adamas pharmaceuticals amber johnson no relationship to disclose yekaterina b . 
s anchez no relationship to disclose md abu shufean no relationship to disclose sarina piha - paul consulting or advisory role : genentech research funding : glaxosmithkline , xuanzhu , puma biotechnology , novartis , merck sharp & dohme , curis , principa biopharma , biomarin , helix biopharma , bayer , abbvie , incyte , five prime therapeutics , cerulean pharma , medimmune , medivation vivek subbiah research funding : novartis , glaxosmithkline , nanocarrier , northwest biotherapeutics , roche / genentech , bergpharma , bayer , incyte , fujifilm , pharmamar , d3 , pfizer , amgen , abbvie , multivir , bluprint medicines travel , accommodations , expenses : novartis , pharmamar , fujifilm david hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack , bayer consulting or advisory role : baxter , bayer research funding : novartis , genentech , eisai , astrazeneca , pfizer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly travel , accommodations , expenses : loxo , mirna therapeutics other relationship : oncorena mark routbort no relationship to disclose russell broaddus no relationship to disclose kenna r . 
stockley tl , oza am , berman hk , et al : molecular profiling of advanced solid tumors and patient outcomes with genotype - matched clinical trials : the princess margaret impact / compact trial . 
j pers med 3 : 306 - 325 , 2013 johnson a , zeng j , bailey am , et al : the right drugs at the right time for the right patient : the md anderson precision oncology decision support platfordrug discov today 20 : 1433 - 1438 , 2015 10 . 
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bennouna j , lang i , valladares - ayerbes m , et al : a phase ii , open - label , randomised study to assess the efficacy and safety of the mek1 / 2 inhibitor azd6244 ( arry - 142886 ) versus capecitabine monotherapy in patients with colorectal cancer who have failed one or two prior chemotherapeutic regimens . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
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van allen em , wagle n , stojanov p , et al : whole - exome sequencing and clinical interpretation of formalin - fixed , paraffin - embedded tumor samples to guide precision cancer medicine . 
lolkema1 introduction the vhl gene is a tumor suppressor gene located at chromosome 3p25 , 1 and its protein has multiple functions linked to multiple effector proteins.2 aberrations in the vhl gene are associated with sporadic clear cell renal cell carcinomas ( ccrccs ) , sporadic hemangioblastomas , pheochromocytomas , pancreatic islet cell tumors , endolymphatic sac tumors , and benign cysts affecting various organs.3 germline inthe vhl gene causes the autosomal activation of dominant von hippel - lindau ( vhl ) syndrome . 
vhl is rarely mutated outside of the context of rcc or vhl syndromeassociated malignancies.4 biallelic vhl inactivation caused by genetic and epigenetic alterations ( including dna methylation , histone modications , and coincidental loss of genes localized adjacent to the vhl chromosome locus ) has been described.2 in both hereditary and sporadic tumors , vhl mutations are heterogeneous.5 the encoded vhl protein ( pvhl ) plays an important role in ubiquitination and proteosomal degradation of hypoxia inducible factor - 1 ( hif - 1 )  . 
our aim was to investigate the ( epi ) genetic background of this patients disease and to determine whether the identied vhl mutation could be a driving mutation in this patients fdcs . methods case report in 2013 , a 29 - year - old female patient presented with a large abdominally located mass and multiple hepatic lesions . 
a histologic biopsy from a liver lesion showed an epithelioid and spindle cell malignant neoplasm with scattered lymphocytes . immunohistochemistry ( ihc ) results matched the pattern of fdcs with exfollicular dendritic cell markers cd21 , pression of cd23 , and cd359 ( fig 1a - c )  . 
on the basis of radiologic diagnosis , the pattern did not t an rcc . this was further supported by a negative paired box gene 8 ( pax8 ) ihc result ( fig 1d )  . the clinical course of our patients disease is outlined in figure 2 . 
the second - line treatment was pazopanib , which resulted in unexpected stable disease for 22 months . rendering additional the patient participated in the dutch national center for personalized cancer treatment ( cpct ) - 02 program , 10 tumor sampling for whole - genome sequencing ( wgs ) analysis before and after treatment with pazopanib . 
wgs was performed on the illumina hiseq x platform with 100 ng dna as input using standard protocols ( pairedend 2 150 base pairs ; illumina , san diego , ca )  . within the framework of cpct - 02 , all germline variants are ltered , which guarantees that only somatic variants are reported . 
hif - 1 ihc showed positive nuclear staining ( e ) , and glucose transporter 1 ( glut1 ) ihc showed positive staining ( f )  . results genomic landscape the identied c.119delc vhl frameshift mutation led to a truncated pvhl ( p.pro40fs ; fig 4 )  . 
both biopsies showed genome - wide aberrations , with large chromosomal copy number alterations , structural rearrangements , and mutations in a broad spectrum of loci ( fig 5 )  . 
the patient received eight cycles of chop ( cyclophosphamide , doxorubicin , vincristine , prednisone ) , which resulted 6 months later ( t6 ) in metabolic complete remission ( cr )  . 
after that ( t36 ) , the patient showed pd and participated in a phase 1 trial with immunotherapy ( cd40 agonistic monoclonal antibody ) in combination with vanucizumab ( anti - angiopoietin - 2 and anti - vegf [ vascular endothelial growth factor ] ) for 11 months . 
both results provide circumstantial evidence for functional loss of pvhl.7 , 10 discussion our analysis revealed a unique patient with fdcs harboring a somatic functional vhl aberration , which is the rst description of a vhl mutation in sarcoma.14 because fdcs is a rare mesenchymal neoplasm with a largely unknown and rather complex genetic landscape15 and is unknown for harboring vhl aberrations , we veried specic ihcbased markers to conrm the diagnosis and to reject metastatic rcc ( mrcc ) as an alternative diagnosis . 
the positive hif - 1 ihc result may indicate a functional loss of pvhl ; in this patient , it was a consequence of mutation and potential methylation - derived changes leading to biallelic vhl gene inactivation . 
although most evidence in fdcs has been found for the involvement of the ras / raf signaling pathway , 16 , 17 we did not identify mitogen - activated protein kinase ( mapk ) alterations in our patient . 
a mutant allele - specic imbalance as a consequence of allele - specic amplication has been described.18 , 19 however , this seems to be a more common aspect with activating mutations . 
recurrent vhl locus amplications have not been described in ccrcc ; therefore , it does not seem to be a common aberration . however , these reports did not specically investigate post - tyrosine kinase samples.2 , 20 , 21 numerous nonspecic chromosomal translocations were present in the pretreatment biopsy , with a remarkable decline in the number of structural variants ( svs ) following treatment with pazopanib . 
treatment of cancer may have an inuence on involved processes and subsequently on patterns and frequency of svs.22 alterations in the number of svs between time points in a patients malignancy may also be a consequence of tumor evolution and selective survival of subclonal populations as a result of the selective pressure of treatment , similar to variable somatic alterations that cause the emergence of drug resistance.23 the changes in the genomic landscape between the two biopsies obtained in our patient could be associated with the observed disease response during treatment with pazopanib.24 moreover , the fact that the mutated vhl gene has been amplied in our patients disease over time emphasizes its importance and potential as a driver mutation . upregulated vegf is associated with the hif pathway . 
pazopanib , a multikinase inhibitor with activity against the vegf receptor and platelet - derived growth factor and receptors , is effective in the treatment of mrcc25 and metastatic sarcoma.26 during treatment with pazopanib , our patient had stable disease for 22 months . 
in march 2016 , progressive disease was revealed on a conventional ct scan ( a ) and on a positron emission tomography scan ( b ) before the start of treatment with pazopanib . 
untranslated regions ( utr ) and exonic regions are depicted by rectangular boxes ( colored dark blue and dark gold , respectively ) , and intronic regions are depicted by black lines . 
 ( c ) protein sequences of wild - type ( wt ) pvhl and mutant pvhl , colored by protein domains ; ( gxeex ) 8 is shown in light blue , - domain in light gold , and - domain in red . 
 ( the vhl gene model is on the basis of ensembl transcript nm_000551.2 and the protein model is on the basis of the uniprotkb p40337 entry . ) red asterisk indicates stop codon . 
moreover , saygin et al27 performed a pooled analysis of data from 462 patients with fdcs , showing a median survival for patients with metastatic disease of 9 months ( range , 0.25 to 72 months ) and a 2 - year survival rate of 15.8% ; these results suggest that the long pfs is not the result of better prognostic features of fdcs . 
the relatively long pfs during our patients last treatment , which consisted of the combination of a cd40 agonistic monoclonal antibody and an antiangiopoietin - 2 and anti - vegf bispecic monoclonal antibody , could possibly be explained by the effect of the latter drug ( vanucizumab )  . 
these data imply that the vhl mutation in our patient may predict a biologic behavior more similar to mrcc than to a metastatic sarcoma in response to treatment with pazopanib . 
these ndings are not sufcient to make an argument for vegf - targeted therapies in fdcs , because this is the rst case of a vhl - mutated fdcs as far as we know . indirect evidence for pvhl functional although hif stabilization and glut1 accumulation are , at the most , loss , a limitation of this case report is the absence of methylation analysis looking further into epigenetic silencing of the vhl gene . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . florence atra travel , accommodations , expenses : abbvie , astellas pharma paul j . 
van diest consulting or advisory role : panterhei ( inst ) patents , royalties , other intellectual property : ddx3 as a biomarker for cancer and methods related thereto ( inst ) geert j.l.h. 
we thank hartwig medical foundation for providing wholegenome sequencing data and for performing analysis of these data . moreover , this patient was entered into the center for personalized cancer treatment ( cpct ) - 02 study . 
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the tumor was negative for programmed death ligand 1 ( pd - l1 ) expression ( tumor proportion score , 1% ) .24 postoperative imaging 6 weeks later revealed two lowdensity liver lesions measuring 1.5 cm ( segment 4a ) and 1.9 cm ( segment 2 ; fig 2a ) , which were hypermetabolic on an 18 - uorodeoxyglucose ( fdg ) positron emission tomography ( pet ) / computed tomography scan . 
after two cycles of carboplatin and etoposide , 10 new liver lesions were evident on imaging ( fig 2b )  . he subsequently enrolled in a phase ii study of pembrolizumab ( 10 mg / kg intravenously [ iv ] every 2 weeks ) for patients with msi - h tumors ( clinicaltrials.gov identier : nct01876511 )  . 
these required discontinuation of pembrolizumab after 10 months despite ongoing disease response to treatment ( fig 2d )  . hypothyroidism the patient underwent total proctocolectomy ; both tumors were t1n0 . 
msi testing ( internal ucsf500 assay ; ucsf clinical cancer genomics laboratory ) and mmr protein immunohistochemistry of the resected colon cancer sample conrmed msi - h status and loss of mlh1 expression in the tumor and normal samples . 
by cycle 11 of pembrolizumab , worsening hypothyroidism was evident , peaking at cycle 13 with thyroidstimulating hormone levels of 79.2 iu / ml ( free t4 , 0.6 ng / dl ; total t3 , 63 ng / dl )  . 
 new - onset diabetic ketoacidosis / insulin - dependent diabetes mellitus arthritis whitman et al at 10 months after starting pembrolizumab ( cycle 19 ) , the patient presented with diabetic ketoacidosis ( dka ) ; he had blood glucose levels  . 
given the lack of data supporting use in this setting , corticosteroids were not immediately started , although grade 4 autoimmune type 1 insulin - dependent diabetes mellitus was suspected.25 pembrolizumab was discontinued , and daily insulin therapy was initiated . myocarditis the patient experienced bradyarrhythmias with complete heart block while recovering from dka . 
the troponin level was elevated at 7.4 g / l ( normal , 0.05 g / l ) , the electrocardiogram showed new inferior q waves , and the echocardiogram revealed a depressed ejection fraction ( 30% - 35% ) and regional wall motion abnormalities consistent with coronary artery disease . 
he was monitored with serial echocardiograms , electrocardiograms , and troponin levels for 20 months without evidence of recurrent myocarditis . at 5 months after treatment initiation , the patient noticed grade 1 stiffness and discomfort in his knees , ankles , hands , and bilateral wrists . 
differential diagnosis favored an autoimmune process , with an elevated erythrocyte sedimentation rate of 77 mm / h ( normal , 10 mm / h ) and a c - reactive protein level of 98.0 mg / l ( normal , 6 mg / l )  . 
within 24 hours of initiating corticosteroids for myocarditis , he experienced near - complete resolution of arthritic symptoms . autoimmune hepatitis at 4 months after discontinuation of immunotherapy , and within 3 weeks of completing the initial corticosteroid taper for myocarditis and arthritis , the patient was admitted for asymptomatic grade 3 transaminitis , with an alt level of 990 u / l ( normal , 60 u / l ) and an ast level of 791 u / l ( normal , 42 u / l )  . he was treated with high - dose iv methylprednisolone followed by prednisone 1 mg / kg orally ( tapered over 10 months ) with rapid improvement in liver function tests . 
work - up was negative for cytomegalovirus ; epstein - barr virus ; and hepatitis a , b , c , d , and e infections . follow - up imaging revealed two residual 18f - fdgpost - treatment petnegative liver lesions ( 1 cm and 0.6 cm ; fig 4b )  . 
computed tomography ( ct ) scan of abdomen / pelvis ( a ) 6 weeks after resection of primary tumors ( two lesions , largest was 1.9 cm ) , prechemotherapy ; ( b ) after two cycles of carboplatin / etoposide ( at least 10 lesions , largest was 3 cm ) ; ( c ) after three cycles of pembrolizumab ; and ( d ) after 11 cycles ( 5 months ) of pembrolizumab . responses to checkpoint blockade in ls are hypothesized to be the result of higher mutational load as a result of mmr deciency , which is associated with more mutationassociated neoantigens . 
his arthritis is controlled with methotrexate , and he remains on insulin for type 1 diabetes mellitus and on levothyroxine for hypothyroidishis myocarditis and hepatitis are in remission . discussion presence of a germline mutation in the mmr gene mlh1 with loss of the wild - type allele in the nec component suggests that the nec developed as a consequence of ls in this patient . this case , coupled with data suggesting that approximately 10%26 - 29 of gi necs ( including mixed adenoneuroendocrine carcinomas ) are msi - h ( predominantly from mlh1 methylation ) , underscores the need to consider ls in patients with colorectal nec and the potential value of msi testing in these tumors . 
checkpoint inhibitor ( cpi ) therapy is compelling given the paucity of treatments for platinum - refractory colorectal nec , the tissue / site - agnostic approval of pembrolizumab for msi - h tumors , 30 and evidence suggesting that cpis have activity in mmr - decient / msi - h cancers whether associated with ls or developing sporadically ( eg , in the setting of mlh1 promoter methylation31 - 33 )  . our patient experienced ve iraes . 
regarding immunotherapy - related diabetes , one series suggested that gad65 autoantibodies were present in 60% of patients and that a small proportion harbored a cd8 + t - cell response to a t1dm antigen.34 , 35 gad65 autoantibodies were absent in our patient , suggesting a lower probability of undiagnosed autoimmune disease and underscoring the need for validated markers of response and toxicity for patients treated with cpis.36 the relationship between toxicity and efcacy remains ill dened37 ( appendix )  . 
whether underlying ls increased the risk for iraes is unclear , but a germline mlh1 mutation could theoretically predispose a patient to mutations in normal tissue that are immunologically recognized . 
however , previous reports of cpi therapy in patients with msi - h tumors have not suggested a higher incidence of iraes in this population.5 , 31 , 32 , 38 the patient was treated with a relatively high dose ( 10 mg / kg iv every 2 weeks ) of pembrolizumab compared with the us food and drug administration approved dose for msi - h cancers ( 200 mg iv every 3 weeks ) ; this difference also may have contributed to iraes . jco precision oncology fig 3 . 
n engl j med 363 : 711 - 723 , 2010 topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of antipd - 1 antibody in cancer . 
n engl j med 366 : 2443 - 2454 , 2012 brahmer j , reckamp kl , baas p , et al : nivolumab versus docetaxel in advanced squamous - cell nonsmall - cell lung cancer . 
n engl j med 373 : 123 - 135 , 2015 larkin j , chiarion - sileni v , gonzalez r , et al : combined nivolumab and ipilimumab or monotherapy in untreated melanoma . 
n engl j med 372 : 2509 - 2520 , 2015 le dt , uram jn , wang h , et al : pd - 1 blockade in mismatch repair decient non - colorectal gastrointestinal cancers . 
j clin oncol 34 , 2016 ( suppl ; abstr 195 ) kl oppel g , perren a , heitz pu : the gastroenteropancreatic neuroendocrine cell system and its tumors : the who classication . 
antonia sj , l opez - martin ja , bendell j , et al : nivolumab alone and nivolumab plus ipilimumab in recurrent small - cell lung cancer ( checkmate 032 ) : a multicentre , open - label , phase 1 / 2 trial . 
paraghamian se , longoria tc , eskander rn : metastatic small cell neuroendocrine carcinoma of the cervix treated with the pd - 1 inhibitor , nivolumab : a case report . 
vijayvergia n , dasari a , ross ea , et al : pembrolizumab ( p ) monotherapy in patients with previously treated metastatic high grade neuroendocrine neoplasms ( hg - nens )  . 
mulvey c , raj np , chan ja , et al : phase ii study of pembrolizumab - based therapy in previously treated extrapulmonary poorly differentiated neuroendocrine carcinomas : results of part a ( pembrolizumab alone )  . 
kaufman hl , russell js , hamid o , et al : updated efcacy of avelumab in patients with previously treated metastatic merkel cell carcinoma after 1 year of follow - up : javelin merkel 200 , a phase 2 clinical trial . 
kervarrec t , samimi m , gaboriaud p , et al : detection of the merkel cell polyomavirus in the neuroendocrine component of combined merkel cell carcinoma . virchows arch 472 : 825 - 837 , 2018 24 . 
j immunother cancer 5 : 40 , 2017 jesinghaus m , konukiewitz b , keller g , et al : colorectal mixed adenoneuroendocrine carcinomas and neuroendocrine carcinomas are genetically closely related to colorectal adenocarcinomas . 
la rosa s , marando a , furlan d , et al : colorectal poorly differentiated neuroendocrine carcinomas and mixed adenoneuroendocrine carcinomas : insights into the diagnostic immunophenotype , assessment of methylation prole , and search for prognostic markers . 
overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repairdecient or microsatellite instabilityhigh colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
puzanov i , diab a , abdallah k , et al : managing toxicities associated with immune checkpoint inhibitors : consensus recommendations from the society for immunotherapy of cancer ( sitc ) toxicity management working group . 
overman mj , lonardi s , wong kym , et al : durable clinical benet with nivolumab plus ipilimumab in dna mismatch repair - decient / microsatellite instabilityhigh metastatic colorectal cancer . 
galon j , costes a , sanchez - cabo f , et al : type , density , and location of immune cells within human colorectal tumors predict clinical outcome . 
llosa nj , cruise m , tam a , et al : the vigorous immune microenvironment of microsatellite instable colon cancer is balanced by multiple counter - inhibitory 313 : 1960 - 1964 , 2006 checkpoints . 
strosberg jr , coppola d , klimstra ds , et al : the nanets consensus guidelines for the diagnosis and management of poorly differentiated ( high - grade ) extrapulmonary neuroendocrine carcinomas . 
 checkpoint blockade in msi - high neuroendocrine carcinoma appendix summary us food and drug administration approvals of immunotherapy in may 2017 , the us food and drug administration approved pembrolizumab for unresectable or metastatic microsatellite instability high ( msi - h ) or mismatch repairdecient solid tumors that have progressed on prior standard treatment . 
in august 2017 , nivolumab was approved for msi - h colorectal cancer . modest activity has been demonstrated in advanced small - cell lung cancer , leading to drug approvals in rst - line ( atezolizumab plus chemotherapy ) and platinum - refractory settings.12 , 13 , 20 - 22 checkpoint inhibitors have an established role in merkel cell carcinoma , which is a virally mediated disease.21 - 23 beyond that , the role of immunotherapy in extrapulmonary neuroendocrine carcinomas ( necs ) remains ill dened . 
however , three recent pilot studies suggest minimal activity ( response rate , 10% ) of singleagent checkpoint inhibitors in unselected patients with extrapulmonary necs.15 - 17 a growing body of literature has served to clarify the nature and optimal management of immune - related adverse events . 
some reports suggest that patients with grade 3 immune - related adverse events experience longer median time to progression and higher radiographic response . recent biomarker data suggest a high rate of programmed death 1 ( pd1 ) / programmed death ligand 1 expression in poorly differentiated necs of the gi tract ( roberts ja , et al : hum pathol 70 : 49 - 54 ) and a greater proportion of msi - h in high - grade necs , mixed adenoneuroendocrine carcinomas , and insulinomas than in low - grade gastroenteropancreatic neuroendocrine tumors ( weber mm , fottner c : oncol res treat 41 : 306312 , 2018 )  . 
 o egfr genotyping of matched urine , plasma , and tumor tissue in patients with nonsmall - cell lung cancer treated with rociletinib , an egfr tyrosine kinase inhibitor jonathan w . 
wakelee author affiliations and support information ( if applicable ) appear at the end of this article . ( continued ) purpose liquid biopsies represent an attractive alternative to tissue biopsies , particularly rebiopsies , in determining patient eligibility for targeted therapies . 
we evaluated epidermal growth factor receptor ( egfr ) t790m detection in matched urine , plasma , and tissue and the clinical outcomes of patients with advanced nonsmall - cell lung cancer treated with rociletinib . methods tissue ( n = 540 ) , plasma ( n = 482 ) , and urine ( n = 213 ) were collected from evaluable patients enrolled in tiger - x , a phase i / ii study . 
genotyping was performed by therascreen egfr testing in tissue , beaming in plasma , and a quantitative short footprint assay ( trovera ) in urine , which was used to further examine discordant samples . results positive percent agreement with tissue t790m results was similar for urine ( 82% ; 142 of 173 ) and plasma ( 81% ; 313 of 387 ) genotyping . 
the ability to identify mutations in plasma was strongly associated with m stage ( p < .001 ) ; rate of t790m detection for patients with m1a / m0 disease increased from 54% for plasma alone to 85% when urine and plasma were both examined . 
objective response rates of patients who were t790m positive were comparable between tumor ( 34% ) , plasma ( 32% ) , and urine ( 37% )  . conclusion clinical response to rociletinib was comparable irrespective of whether t790m status was identified by liquid or tissue biopsy . 
combined , urine and plasma identified a higher percentage of patients who were t790m positive than tumor genotyping alone and improved detection of t790m , particularly in the absence of distant metastases . 
2018 by american society of clinical oncology introduction although tyrosine kinase inhibitors ( tkis ) targeting the epidermal growth factor receptor ( egfr ) have transformed the treatment of patients with egfr - mutant nonsmall - cell lung cancer ( nsclc ) , clinical responses are frequently brief . 
acquired resistance often develops within 10 to 16 months of treatment initiation.1 - 4 emergence of the gatekeeper egfr t790m mutation , which increases the atp - binding affinity of the oncogenic receptor , accounts for resistance in most patients.5 , 6 several third generation , mutant - selective inhibitors have been developed to target t790m , including osimertinib , rociletinib , nazartinib ( egf816 ) , avitinib ( ac0010 ) , olmutinib ( hm61713 / bi1482694 ) , asp8273 , and pf06747775.7 - 11 these agents target egfr - activating and t790m - resistance mutations , while largely sparing the wild - type receptor and minimizing related on - target toxicities . 
wakelee , md , stanford university , thoracic oncology , 875 blake wilbur dr , rm 2233 mc 5826 , stanford , ca 94305 ; e - mail : hwakelee@stanford.edu. t790m mutationpositive nsclc has been impressive and led to the accelerated approval of osimertinib in the united states.12 given their predictive value , the ability to detect driver and resistance egfr mutations is paramount in improving patient outcomes . 
tumor tissue genotyping is the current standard of care ; however , tumor tissue genotyping can be associated with biopsy - related complications ( ie , pneumothorax , bleeding , and infection ) because of its invasive nature.13 , 14 it is estimated that 20% of tissue biopsies are uninformative as a result of tumor inaccessibility , inadequate sample collection , or intratumoral heterogeneity.15 , 16 these challenges are pronounced in patients who have developed egfr - tki resistance and require a rebiopsy . 
in a study of 120 eligible patients experiencing disease progression while receiving an egfr - tki , 45 ( 38% ) did not undergo rebiopsy because of inaccessible tumor sites , patient refusal , or decision of the treating physician.17 the noninvasive genotyping of circulating tumor dna ( ctdna ) in plasma can identify predictive biomarkers while improving the patient experience . 
accordingly , plasma - based egfr mutation tests have been approved for use as companion diagnostics by health authorities in europe and the united states.18 ctdna from blood undergoes glomerular filtration in the kidney and can be detected in urine . 
 the feasibility of using urine to detect somatic alterations identified in matched plasma and / or tumor has been demonstrated in proof - of concept studies , unveiling urine as an alternative specimen type that can be collected with fewer constraints than tissue or plasma.19 - 21 previously , we reported that egfr mutations can be detected with high sensitivity in urine of patients with advanced nsclc using a short footprint mutation enrichment next - generation sequencing assay ( trovera ; trovagene , san diego , ca ) .19 in the tiger - x phase i / ii study , we examined the clinical utility of t790m urine genotyping in a large cohort of patients with advanced nsclc who received rociletinib . methods patients and study design for this analysis of patients enrolled in the tiger - x trial ( clinicaltrials.gov identifier : nct01526928 ) , all patients initiating treatment with rociletinib ( 500 , 625 , or 750 mg twice a day hydrobromide formulation ) were evaluable . 
confirmed objective response rate ( orr ) , progression - free survival ( pfs ) , and duration of response ( dor ) were assessed per response evaluation criteria in solid tumors version 1.1 ( recist ) by the investigators . 
tiger - x was approved by the institutional review board at each study site and conducted in accordance with the declaration of helsinki and good clinical practice guidelines of the international conference on harmonization . 
additional details regarding sample collection and processing are described elsewhere.19 statistical analysis clopper - pearson methods were used to obtain percentage point estimates and the 95% ci for analysis of orr as well as for percent agreement between two sample types . 
 tiger - x safety population : all patients treated at 500 , 625 , or 750 mg twice a day ( n = 548 ) did not participate in urine collection ( n = 335 ) clinical site did not submit biopsy ( n = 8 ) clinical site did not submit plasma ( n = 66 ) patients with pretreatment urine submitted for egfr testing by trovera ( n = 213 ) patients with pretreatment tumor submitted for egfr testing by therascreen ( n = 500 ) or cobas ( n = 40 ) patients with pretreatment plasma submitted for egfr testing by beaming ( n = 482 ) patients with matched urine and tumor for diagnostic comparison ( n = 209 ) patients with matched plasma and tumor for diagnostic comparison ( n = 475 ) fig 1 . 
the tiger - x safety population included all patients who received at least one dose of rociletinib and who were treated at 500 , 625 , or 750 mg twice a day . 
egfr , epidermal growth factor receptor . patients with matched urine and plasma for diagnostic comparison ( n = 181 ) patients with matched urine , plasma , and tumor for diagnostic comparison ( n = 177 ) results patient population among 548 evaluable patients , 540 tissue , 482 plasma , and 213 urine pretreatment samples were submitted for central egfr testing ( fig 1 )  . 
the biomarker analysis population was enriched for patients who were t790m positive by tumor genotype ( 500 of 548 with local and / or central tumor t790m - positive result ; 91.2% ; data supplement ) relative to an unselected population with acquired resistance to egfr - tkis . egfr mutation detection in liquid and tissue biopsies to examine the clinical validity of urine and plasma testing , concordance with tissue egfr genotyping results was evaluated . 
these 23 patients were retested on a second plasma test platform ( trovera ) , and 22 ( 95.7% ) were confirmed to be t790m positive ( data supplement )  . next , we compared urine and tumor egfr results . 
 a negative / inadequate by all 7 ( 4.0% ) positive by urine positive by plasma positive by tissue positive by plasma or urine positive by tissue or plasma positive by tissue or urine positive by at least one fig 2 . 
among the 41 patients who were t790m discordant , we observed an even split between patients who were t790m urine positive / plasma negative ( n = 21 ) and urine negative / plasma positive ( n = 20 )  . 
urine af was generally lower than plasma af ( p < .001 ; data supplement ) independent of test platform ( data supplement ) , which may reflect postrenal shedding of nontumor cell - free dna from the bladder into urine , contributing to background.23 among 43 patients for whom urine af exceeded the matched plasma af , no target or nontarget lesions were identified in the urinary system ( data supplement )  . a three - way diagnostic comparison was conducted for the patients with matched tumor , plasma , and urine . 
in addition , genotyping of each sample type uniquely identified patients who were t790m positive , including eight by tumor , five by urine , and three by plasma ( fig 2b )  . clinical response in patients who are t790m positive and t790m negative identified by different sample types all patients with central t790m genotyping were considered evaluable for efficacy . 
at risk : plasma 120 116 tissue 150 143 urine 62 plasma 374 282 192 135 tissue 443 354 255 182 125 urine 169 132 censored plasma tissue urine fig 3 . 
the high relative response rate of patients who were tumor t790m centrally negative was likely because most patients ( 59.5% ; 25 of 42 ) had a known local t790m - positive tumor result . 
in urine , no significant correlation between t790m : act and depth of response was found ( data supplement )  . clinical characteristics and mutation detection in liquid biopsies next , we examined clinical characteristics potentially predictive of ability to identify mutations in urine and plasma . 
patients in whom t790m was identified in plasma also had a greater median baseline tumor burden than those without detectable t790m ( as measured by the sum of longest diameters , 65 v 43 mm , respectively ; p < .001 ; data supplement )  . 
 this complementarity reflects the differences in plasma and urine ctdna levels within patients , which may depend on the rates of tumor dna shedding , ctdna degradation in blood versus urine , renal filtration , and excretion of ctdna in urine.23 the ppa for t790m detection between urine and plasma with tumor as reference was 82% and 81% , respectively ( table 1 )  . 
the ppa for plasma in this study was somewhat higher than previously described for t790m ( 70% to 73% ) in a similar patient population using the same testing methodology ( beaming ) .22 , 27 this difference could be explained by the substantially higher median tumor burden and frequency of distant metastatic disease observed compared with our previous report.22 this observation illustrates that clinical characteristics should be appropriately considered when comparing plasma ctdna assay sensitivities across different studies . in contrast to the high sensitivity of detection , the npa for t790m in urine and plasma with tumor as the reference was 31% and 43% , respectively . 
 the low apparent specificity likely reflects the subclonal , heterogeneous nature of the t790m resistance mutation , which can give rise to a false - negative result in a tumor biopsy because of sampling error.24 , 28 notably , for the majority of patients who were discordant t790m plasma or urine positive / tumor negative , the mutation was detected by at least one other test platform , and those patients had a demonstrable response to rociletinib , suggesting that they are indeed tumor false negative and urine / plasma true positive . 
patients identified as t790m negative by central tumor testing displayed a lower orr when treated with rociletinib as compared with patients who were centrally genotyped t790m tumor positive ( 21% v 34% )  . 
however , a formal comparison was not performed , because 60% of centrally genotyped , t790m tumor - negative patients had a locally assessed t790m - positive result in the same biopsy , confounding analysis of clinical outcomes in this cohort . 
discordance between local and central tumor results occurred in < 5% of evaluable patients and may be attributable to molecular heterogeneity between tumor sections , low tumor cellularity within the specimen , differential test sensitivities , or a combination of these . 
when stratified on the basis of local tissue test results , patients who were centrally negative with a corresponding locally negative or locally unknown t790m result had an orr of 6% . 
consistent with our previous findings in smaller patient cohorts , 22 m stage was a strong predictor of the ability to identify mutations in plasma ; t790m was more readily detected in patients with m1b ( 89% ) versus m1a / m0 ( 54% ) disease . 
urine testing identified both patients with m1a / m0 and m1b disease with high sensitivity ( 74% and 83% , respectively ) , suggesting that all patients would be good candidates for a urine test or for a combination of urine and plasma tests , where the combined sensitivity ( 85% and 94% for m1a / m0 and m1b , respectively ) was even higher than for either specimen alone . the cobas egfr mutation test v2 using plasma specimens recently became the first liquid biopsy test approved by the us food and drug administration as a companion diagnostic to identify patients with t790m - positive metastatic nsclc eligible for treatment with osimertinib.29 if after disease progression while receiving firstor second - generation egfrtkis patients receive plasma - based t790m genotyping , with consideration of additional urine analysis to increase sensitivity , this would simultaneously circumvent the pitfalls associated with tissue rebiopsies and minimize the test turnaround time for patients who test t790m positive or who are not candidates for tumor rebiopsy . 
wakelee between a scheduled percutaneous tumor biopsy and receipt of an egfr result by the treating physician.30 , 31 in our study , all three sample types were found to identify unique patients who were t790m positive . 
on the basis of a recent pharmacoeconomic assessment , urine testing alone obviates the need for rebiopsy in 48% of patients progressing on first - generation egfr - tkis.32 this not only improves patient experience but also results in a twoto 10 - fold cost savings as a result of a reduction in expenses incurred for biopsy - related complications and tissue - based molecular tests.32 one limitation is that an enriched population of patients with known tumor t790m mutations was enrolled ; therefore , our study was not optimally positioned to investigate clinical outcomes of patients who were t790m positive by liquid biopsy alone . 
goldman consulting or advisory role : astrazeneca , bristol - myers squibb , clovis oncology , genentech , lilly , trovagene , vortex biosciences , amgen speakers ' bureau : merck research funding : eli lilly , genentech , astex pharmaceuticals , clovis oncology , bristol - myers squibb , astrazeneca / medimmune , threshold pharmaceuticals , array biopharma , celgene , abbvie , astellas pharma , corvus pharmaceuticals chris karlovich employment : clovis oncology stock and other ownership interests : clovis oncology lecia v . 
sequist honoraria : astrazeneca consulting or advisory role : astrazeneca , genentech , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , merck ( inst ) , pfizer ( inst ) vlada melnikova employment : trovagene aleksandra franovic employment : guardant health , trovagene , ignyta shirish m . 
gadgeel consulting or advisory role : pfizer , boehringer ingelheim , genentech , ariad pharmaceuticals , astrazeneca , bristol - myers squibb speakers ' bureau : astrazeneca research funding : pfizer ( inst ) , clovis oncology ( inst ) , merck ( inst ) , genentech ( inst ) , incyte ( inst ) , millennium ( inst ) , astrazeneca / medimmune ( inst ) , bristol - myers squibb ( inst ) , halozyme ( inst ) , acerta pharma ( inst ) , acea biosciences ( inst ) , janssen oncology ( inst ) , novartis ( inst ) , five prime therapeutics ( inst ) , oncomed ( inst ) travel , accommodations , expenses : ariad pharmaceuticals / takeda , genentech karen l . 
reckamp consulting or advisory role : amgen , boehringer ingelheim , ariad pharmaceuticals , astellas pharma , nektar , euclises pharmaceuticals , tesaro research funding : bristol - myers squibb ( inst ) , pfizer ( inst ) , novartis ( inst ) , ariad pharmaceuticals ( inst ) , clovis oncology ( inst ) , xcovery ( inst ) , gilead sciences ( inst ) , pfizer ( inst ) , adaptimmune therapeutics ( inst ) , genentech ( inst ) , boehringer ingelheim , abbvie d . 
ross camidge honoraria : roche , g1 therapeutics , mersana therapeutics , takeda research funding : takeda maurice prol consulting or advisory role : eli lilly , genentech , pfizer , astrazeneca , boehringer ingelheim , merck sharp & dohme , bristol - myers squibb , novartis , amgen research funding : astrazeneca ( inst ) , roche ( inst ) travel , accommodations , expenses : astrazeneca , roche , bristol - myers squibb sai - hong ignatius ou honoraria : pfizer , roche pharma ag , genentech , araid / takeda , novartis , astrazeneca , foundation medicine consulting or advisory role : pfizer , roche / genentech , novartis , astrazeneca , takeda / ariad , foundation medicine speakers ' bureau : genentech , astrazeneca , takeda / araid research funding : pfizer ( inst ) , roche pharma ag ( inst ) , astrazeneca / medimmune ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , ariad pharmaceuticals ( inst ) , ignyta ( inst ) , peregrine pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , astellas pharma ( inst ) , chugai pharmaceutical ( inst ) stephen v . 
langer honoraria : bristol - myers squibb , genentech , eli lilly / imclone research funding : clovis oncology , astrazeneca , astellas pharma , incyte , eli lilly jean - charles soria employment : medimmune honoraria : roche , astrazeneca , sanofi , servier , pierre fabre mark a . 
socinski honoraria : genentech , bristol - myers squibb , celgene , astrazeneca consulting or advisory role : genentech speakers ' bureau : genentech , bristol - myers squibb , astrazeneca , boehringer ingelheim research funding : pfizer ( inst ) , genentech tarek m . 
mekhail honoraria : genentech , eli lilly , bristol - myers squibb , merck , boehringer ingelheim speakers ' bureau : genentech , eli lilly , bristol - myers squibb , merck benjamin j . 
solomon honoraria : bristol - myers squibb , astrazeneca consulting or advisory role : bristol - myers squibb ( inst ) , merck sharp & dohme ( inst ) , astrazeneca , pfizer ( inst ) , genentech ( inst ) , eisai research funding : pfizer ( inst ) patents , royalties , other intellectual property : royalties from veristrat ( biodesix ) travel , accommodations , expenses : astrazeneca , roche , merck , bristol - myers squibb , novartis consulting or advisory role : genentech , eli lilly / imclone , merck , abbott biotherapeutics , bayer healthcare pharmaceuticals / onyx , clarient , clovis oncology , celgene , cancer support community , bristol - myers squibb , ariad pharmaceuticals , takeda , astrazeneca research funding : merck ( inst ) , advantagene ( inst ) , clovis oncology ( inst ) , celgene ( inst ) , inovio pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , genentech ( inst ) , stemcentrx ( inst ) other relationship : eli lilly , amgen , peregrine pharmaceuticals , synta pharmaceuticals joel w . 
neal consulting or advisory role : clovis oncology , boehringer ingelheim , armo biosciences , nektar , ariad pharmaceuticals / takeda , caret , astrazeneca , eli lilly research funding : genentech , merck , arqule , novartis , boehringer ingelheim , nektar , exelixis , ariad pharmaceuticals / takeda darrin despain employment : clovis oncology stock and other ownership interests : clovis oncology sergey yurasov employment : clovis oncology , immune design leadership : immune design stock and other ownership interests : clovis oncology , immune design jason b . 
natale consulting or advisory role : astrazeneca , eli lilly travel , accommodations , expenses : clovis oncology , juno therapeutics research funding : amgen , astrazeneca , bristol - myers squibb ( inst ) gregory a . 
otterson consulting or advisory role : amgen ( inst ) , novartis ( inst ) , takeda ( inst ) , merck ( inst ) research funding : genentech ( inst ) , pfizer ( inst ) , bristolmyers squibb ( inst ) , clovis oncology ( inst ) , novartis ( inst ) , acerta pharma ( inst ) , ignyta ( inst ) , merck ( inst ) vassiliki papadimitrakopoulou consulting or advisory role : clovis oncology , genentech , merck , biothera pharmaceuticals , eli lilly , janssen , genentech , gensignia life sciences , astrazeneca , ariad pharmaceuticals , nektar research funding : merck ( inst ) , novartis ( inst ) , celgene ( inst ) , clovis oncology ( inst ) , bayer healthcare pharmaceuticals ( inst ) , bristol - myers squibb ( inst ) , astrazeneca ( inst ) , pfizer ( inst ) , janssen oncology ( inst ) , acea biosciences ( inst ) mark erlander employment : trovagene leadership : trovagene stock and other ownership interests : trovagene mitch raponi employment : clovis oncology , beigene stock and other ownership interests : clovis oncology , beigene heather a . 
natale , cedars - sinai medical center , los angeles ; vlada melnikova , aleksandra franovic , and mark erlander , trovagene , san diego ; karen reckamp , city of hope comprehensive cancer center , duarte ; sai - hong ignatius ou , university of california irvine school of medicine , orange ; joel w . 
gadgeel , karmanos cancer institute , wayne state university , detroit , mi ; maurice prol , centre lon brard , lyon ; jean - charles soria , institut gustave roussy , villejuif , france ; stephen v . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as first - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
yu ha , arcila me , rekhtman n , et al : analysis of tumor specimens at the time of acquired resistance to egfr - tki therapy in 155 patients with egfr - mutant lung cancers . 
park k , lee j , lee k , et al : updated safety and efficacy results from phase i / ii study of hm61713 in patients ( pts ) with egfr mutation positive non - small cell lung cancer ( nsclc ) who failed previous egfr - tyrosine kinase inhibitor ( tki )  . 
tan ds - w , yang j , leighl nb , et al : first - in - human phase i study of egf816 , a third generation , mutant - selective egfr tyrosine kinase inhibitor , in advanced nonsmall - cell lung cancer ( nsclc ) harboring t790m . 
douillard jy , ostoros g , cobo m , et al : gefitinib treatment in egfr mutated caucasian nsclc : circulating - free tumor dna as a surrogate for determination of egfr status . 
yoon hj , lee hy , lee ks , et al : repeat biopsy for mutational analysis of non - small cell lung cancers resistant to previous chemotherapy : adequacy and complications . 
kawamura t , kenmotsu h , taira t , et al : rebiopsy for patients with non - small - cell lung cancer after epidermal growth factor receptor - tyrosine kinase inhibitor failure . 
janku f , vibat cr , kosco k , et al : braf v600e mutations in urine and plasma cell - free dna from patients with erdheim - chester disease . 
hyman dm , diamond el , vibat cr , et al : prospective blinded study of brafv600e mutation detection in cell - free dna of patients with systemic histiocytic disorders . 
karlovich c , goldman jw , sun jm , et al : assessment of egfr mutation status in matched plasma and tumor tissue of nsclc patients from a phase i study of rociletinib ( co - 1686 )  . 
su yh , wang m , brenner de , et al : human urine contains small , 150 to 250 nucleotide - sized , soluble dna derived from the circulation and may be useful in the detection of colorectal cancer . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfr t790 wild - type clones following treatment of t790m - positive cancers with a third generation egfr inhibitor . 
tseng js , yang ty , tsai cr , et al : dynamic plasma egfr mutation status as a predictor of egfr - tki efficacy in patients with egfr - mutant lung adenocarcinoma . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - small - cell lung cancer . 
suda k , murakami i , katayama t , et al : reciprocal and complementary role of met amplification and egfr t790m mutation in acquired resistance to kinase inhibitors in lung cancer . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
 new medicare coverage policy for next - generation tumor sequencing : a key shift in coverage criteria with broad implications beyond medicare the centers for medicare and medicaid services ( cms ) recently issued a national coverage determination on next - generation tumor sequencing ( ngts ) tests for patients with advanced cancer ( see appendix for definitions )  . 
the cms policy provides coverage for ngts tests that received a positive us food and drug administration ( fda ) review and that have fda - approved indications for patients with advanced solid cancers . 
 more than 300 comments were submitted to cms during the public comment period on the draft issuance , and numerous commentaries and news items have been published . in this commentary , we argue that the new cms policy1 presents a key shift in coverage criteria for ngts tests and has important implications beyond medicare for private payer and medicaid coverage policies.2 our commentary draws on our prior and ongoing studies of coverage policies.1 - 3 we also use insights from a meeting held on march 9 , 2018 , and an accompanying survey conducted with the ucsf center for translational and policy research on personalized medicine ( transpers ) payer advisory board . 
the board includes senior executives from the largest private health plans , a medicaid plan , and leading regional private plans , as well as other thought leaders with expertise in coverage and reimbursement by medicare and other payers.4 we also build on our prior work that examined the broader health policy implications of the new cms policy.5 , 6 although observers have commented on the importance of the policy for private payers , there has been no assessment of the policys implications for these payers and for medicaid plans . 
our previous work showed limited coverage of ngts tests by private payers , 7 and our more recent analyses of the largest private payers ( unpublished data ) confirmed that coverage of ngts tests specifically is variable . 
some payers cover ngts tests only for specific cancer sites ( eg , nonsmall - cell lung cancer ) , and others cover only panels with a limited number of genes ( eg , fewer than 50 genes )  . 
for state medicaid plans , we are unaware of any published analyses of coverage policies for ngts tests , but coverage has been described as limited and variable.8 why the cms policy represents a key shift in coverage criteria the new cms policy represents a departure from medicares previous criteria , as well as from criteria currently used for coverage of ngts tests by private payers and medicaid plans , in several ways ( table 1 )  . notably , some private payers use criteria that were not included in the cms policy ( eg , that sequential single - gene testing must be found to be impractical for a patient before they will cover a gene panel )  . 
douglas author affiliations and support information ( if applicable ) appear at the end of this article . the views expressed in this article are his or her own and not an official position of their respective institutions or funders . corresponding author : kathryn a . 
however , contrary to a common assumption , private payers and medicaid do not always follow medicare policies because medicare decisions are only one of many factors that they consider . 
 for example , a review of 47 medicare national coverage determinations for medical devices found that medicare policies were equivalent to the corresponding private payer policies only approximately half of the time.10 medicaid policies are different for each state and thus can be even more variable . in our discussions with payers , we found that many of them are unsure of their plans or do not plan to change their policies to match the cms policy , at least in the short ter payers stated that the new cms policy provides some benefits and a step forward . 
however , they also perceived that it creates concerns that have to be addressed as a result of the significant shift in criteria used , as described in the previous section ( why the cms policy represents a key shift in coverage criteria )  . 
private payers and medicaid plans that decide to change their coverage policies to match those of cms will need to make adaptations . one key difference in the situation faced by private payers versus cms is that private payers do not have the option of the second coverage pathway that is included in the cms policy namely , the use of medicare administrative contractors to make local coverage decisions for tests not already covered by the national policy . 
 the medicare program thus has the flexibility to adapt policies to local situations , whereas private payers typically do not have the flexibility to have differing policies at the national and local levels . 
 for example , although an fda positive review is required by the medicare national coverage policy , medicare local policies may not require this level of review , whereas private payers will have to either require an fda positive review or not require it . changes in coverage policies are also likely to have ripple effects on the laboratory and medical center industries that will require adaptation by private payers and medicaid plans . 
it is possible that the cms national coverage policy requirement for a positive fda review will encourage smaller laboratories to submit their tests for approval and thus increase the number of approved tests . 
the result may be that private payers and medicaid plans have fewer testing options for their patients . the criteria used in the cms policy will also require the refinement of definitions , such as how advanced cancer is measured ( eg , by incorporating the evolving concept of tumor mutational burden in solid tumors )  . 
of particular importance will be whether there are billing codes ( ie , current procedural terminology codes ) that capture the needed information and that are consistently adopted and implemented . 
however , we recently found that there remain large gaps in the codes used for multigene tests as a category and wide variation in whether and how they are implemented.11 we also found that some payers are considering or implementing other approaches to deal with coverage issues for ngts tests that differ from the approach used by cms . 
for example , some payers are providing broader coverage but doing so while also implementing utilization management programs ( eg , preauthorization requirements , contracting agreements , and / or use of laboratory benefit managers )  . 
in the medium to long term , we expect to see an evolution of coverage such that at least some private payers and medicaid plans will establish positive coverage policies for ngts tests in at least some clinical situations . by viewing the past development of ngts policies , we observe that they have evolved over time and that the cms policy emerged from the gaps in that evolution.3 a number of experts have called for adaptation of coverage frameworks for next - generation sequencing tests , 1 , 2 , 12 and several frameworks have been proposed.12 - 14 these approaches all have pros and cons , and their acceptance and implementation have varied.3 regardless , it is clear that the lack of positive coverage policies for ngts tests ( where payers agree to pay for the test provided that criteria are met ) was a gap , and cms determined that they needed to address that gap . we can speculate that private payer coverage will evolve over time with at least some policies that provide broad coverage for ngts tests . 
private plans servicing medicare advantage plans have a mandate to cover ngts tests for those enrolleesa dichotomy in their own policy that may move them toward consistent coverage for all enrollees . 
trosman jr , weldon cb , douglas mp , et al : payer coverage for hereditary cancer panels : barriers , opportunities , and implications for the precision medicine initiative . 
trosman jr , weldon cb , kelley rk , et al : challenges of coverage policy development for nextgeneration tumor sequencing panels : experts and payers weigh j natl compr canc netw 13 : 311 - 318 , 2015 3 . 
center for translational and policy research on personalized medicine ( transpers ) at the university of california , san francisco : transpers program on evidence and reimbursement for personalized medicine . 
phillips ka : evolving payer coverage policies on genomic sequencing tests : beginning of the end or end of the beginning ? jama 319 : 2379 - 2380 , 2018 6 . 
phillips ka , deverka pa , hooker gw , et al : genetic test availability and spending : where are we now ? where are we going ? health aff ( millwood ) 37 : 710 - 716 , 2018 12 . 
after receiving institutional review boardapproved informed consent , targeted next - generation sequencing was performed on 20 patients formalin - xed parafn embedded tumors to characterize genomic alterations across 287 cancer - related genes . 
reverse phase protein array ( rppa ) analysis was performed on both the baseline biopsy and rd specimens , when available . results two of 20 rd tissues were her2 negative per next - generation sequencing ; one sample had insufcient tissue . 
although prevalence of individual tp53 and pik3ca mutations was only modestly higher than published estimates for those in her2 + primary bcs ( 55% and 32% for tp53 and pik3ca , respectively ) , prevalence of these as comutations appeared higher ( 41% ) , compared with less than 10% in several series . 
however , the pcr rate with preoperative her2 - targeted therapy and chemotherapy is only 40% to 60%.4 determining molecular alterations in cancers that persist despite preoperative therapy may dene cancer subtypes for which alternative therapies may be required and may identify important targets . 
pi3k pathway alterations have been associated with poorer outcomes in most her2 + metastatic and neoadjuvant trials , although not with adjuvant her2 - based therapy.5 - 7 tumors with either pten loss or pik3ca mutations are less likely to achieve a pcr after neoadjuvant anthracyclinetaxanebased chemotherapy plus her2 - targeted treatment , even with dual her2 - targeted treatments . 
 holmes et al context key objective to determine if potential nonresponders to therapy can be identied at baseline biopsy before initiation of her2 therapy by using a combination of genomic and proteomic assays . knowledge generated patients with her2 - positive breast cancer who do not achieve pathologic complete response ( pcr ) while receiving her2 therapy may harbor mutations and genomic amplications before therapy , or mutations may develop during or after therapy . 
thus , the presence of pik3ca / tp53 comutations is critical clinical information for selecting the optimal therapy regimen . relevance pretreatment proteomic and genomic molecular signatures reveal potential drug targets and driver mutations , respectively . tumors with pik3ca / tp53 comutations are less likely to achieve pcr and are more likely require additional therapies . 
seventeen had an evaluable amount of rd tissue for ngs and / or rppa analyses ( fig 1 ; data supplement )  . methods and materials targeted ngs was performed on hybridization - captured , adaptor ligationbased libraries using dna extracted from four 10 - micron , formalin - xed parafn - embedded ( ffpe ) sections cut from patients rd specimens ( n = 17 ) and pretreatment biopsy specimens ( n = 6 )  . 
all specimens yielded the minimum required 50 ng of dna at extraction , with the required minimum of 20% nuclei derived from tumor . all coding exons ( n = 3 , 769 ) of 287 cancer - related genes and 47 introns from 19 genes that are frequently rearranged in cancer were sequenced on the illumina hiseq platform ( san diego , ca ) at an average depth exceeding 700 times . 
sequence data were analyzed for all classes of genomic alterations , including base substitutions , short insertions / deletions , focal amplications , homozygous deletions , and gene fusions / rearrangements , as previously described.12 mutation - detection accuracy ( sensitivity and specicity ) was optimized for commonly impure clinical specimens.13 phosphoprotein expression analysis was also performed on the ffpe samples using an rppa platform at a clinical laboratory improvement amendmentscertied laboratory ( theranostics health , gaithersburg , md )  . 
the distribution of tp53 and pik3ca mutations ( mut ) and cdk12 amplications ( amp ) in 17 patients with human epidermal growth factor receptor ( her2 ) - positive breast cancer with residual disease ( rd )  . 
amplication of cdk12 ( which regulates expression of the dna damage response [ ddr ] genes brca1 , rad51 , atr , fanc1 , fancd2 , fancf , and xrcc2 , and which promotes homologous recombination14 ) was observed in eight of the 17 ( 47% ) her2 + rd specimens . of the two originally her2 + cancers that were not her2 amplied on ngs of rd tissue , one was triple negative ( ie , er , progesterone receptor negative , her2 ; patient 20 ) with mutations in pik3ca and map3k1 as well as high - level amplication of fgfr1 and znf703 . 
the second her2 rd specimen was er and progesterone receptor positive ( patient 16 ) and had tp53 and apc mutations with highlevel amplication of mcl1 and egfr ( data supplement 1 )  . pretreatment biopsy specimens because of minute amounts of tissue in archival core needle biopsy specimens , only six pretreatment biopsy specimens were sufcient to be analyzed by ngs ( table 1 )  . 
of the ve patients with matched tissue ( pretreatment and rd tissue ) , all carried a tp53 mutation that was present before treatment and retained in the rd tissue . 
cdk12 amplication was observed in two pretreatment biopsy specimens ( and preserved in the rd tissue ) , and both samples also contained the pik3ca / tp53 comutation . rppa exploratory analyses the small number of patients with rd in this study set , coupled with the limited rd tissue samples , precluded the utility of deep sequencing for novel mutations . 
the clinical and molecular importance of the identied genomic alterations was conrmed by quantifying levels of the associated phosphorylated proteins , which are the targets of us food and drug administrationapproved therapies ( table 1 ; fig 3 )  . 
retrospective analysis of rppa data obtained from frozen pretreatment biopsy specimens coltrial10 revealed that eight of lected during the clinical 12 patients with her2 + bc who did not achieve pcr expressed either higher pi3k and / or pten ser380 protein levels before treatment , compared with their population mean levels ( fig 3 )  . 
of the six patients with comutations , three ( patients 1 , 3 , and 7 ) had higher pten ser380 activity than the population mean , and three ( patients 13 , 18 , and 21 ) had lower levels . 
in contrast , pretreatment biopsy specimens from patients whose rd tissue did not have comutations indicated signicant interactions between akt - phospho - akt and erbb family proteins , phospho - fox01 / 03 - pi3k - mtor pathway , and lc3b - akt , signifying activated growth , proliferation , and autophagy ( table 2 )  . microdissected ffpe tumor tissues were adequate for evaluation by rppa in 12 of the 17 her2 + rd specimens , and six of these had comutations . 
in pretreatment biopsy specimens from patients who did not achieve pathologic complete response ( pcr ) , higher pten ser380 levels ( representing lower overall pten phosphatase activity in the cancers ) were associated with activation of akt and mtor signaling . 
rppa analysis was also available on two specimens for comparison : ( 1 ) the pretreatment biopsy specimen of patient 8 , whose disease did not achieve pcr and who did not have adequate rd tissue for analysis ; and ( 2 ) patient 16 , who was her2 + by ngs ( data supplement )  . discussion in this study of preoperative her2 - directed therapy , we performed biopsies at baseline and after 14 days of treatment to correlate ngs and rppa ndings with the development of pcr versus no pcr at denitive surgery . 
in previously published results , we showed that development of pcr correlated with low expression of egfr tyr1068 , phospho - foxo , and autophagy signaling ( low lc3b ) and high expression of phospho - pten on the baseline biopsy specimens.10 in the current study , we evaluated 17 patients her2 - amplied treatment - refractory rd tissue by ngs and rppa . 
the main ndings from these analyses were that pik3ca mutations were present in the rd tissue only in the context of comutation with tp53 , that pik3ca and tp53 comutations occurred in seven of 17 of the rd samples ( 41% ) , and that the comutated rd tissue indicated activation of egfr , akt , and mtor signaling on rppa . the cancer gene atlas network identied three common somatic mutations in bc , including tp53 , mutated in 37% , pik3ca in 38% , and gata3 in 11%.15 mutations in pi3k and tp53 occurred in 45% and 12% of luminal a , 29% and 29% in luminal b , 39% and 72% of her2 + , and 9% and 80% of basal - like bcs , respectively . 
as noted by skoulidis et al , 21 in dening molecular subgroups of kras - mutant lung adenocarcinoma , cooccurring genetic events may be major determinants of signaling and may highlight dependencies that can be exploited therapeutically . some in vitro data support the hypothesis of cooperativity . croessmann et al22 created single and double mutants of pik3ca by knock - in h1047r or e454k and tp53 by knock - in r248w in the nontumorigenic mcf10a immortalized human breast epithelial cells . 
compared with the the double mutants had a signicant single mutants , growth advantage and displayed anchorage - independent growth , although they were not tumorigenic when injected into athymic nude mice . 
adams instability that et al23 also generated pik3ca and tp53 double - mutant mice and observed the development of mammary cancers with rapid kinetics leading to decreased survival compared with single - mutant animals . loss of tp53 and pik3ca mutations after bc neoadjuvant chemotherapy is associated with a favorable prognosis.18 in 242 patients with bcs comprising all subtypes , 206 had rd . 
combined analyses of both cohorts showed that only four pretreatment biopsy specimens contained comutations in tp53 and pik3ca , and only two rd samples contained the comutations after chemotherapy . kotoula et al19 evaluated whether the outcome of early bc in patients who were treated with adjuvant chemotherapy was affected by comutation of tp53 and pik3ca . 
the entire coding region of tp53 , as well as hot - spot exons of pik3ca ( namely , exons 9 and 20 ) were evaluated in 568 tumors from patients treated with anthracycline and taxane therapy before the availability of h , and in 1 , 093 cancers from the post - trastuzumab era . 
in the entire cohort , pik3ca - only mutation was signicantly associated with better outcome , independent of til density , compared with tp53 - only and none or both mutations . additional evidence supporting oncogene cooperativity comes from cancer cell line enrichment analysis , which correlates response to anticancer agents with multilevelomics data.24 kim et al24 reported that genotypic categories of the cell lines could be distinguished by assessing the effects of coordinate mutations in the context of tp53mutant versus wild - type cancers . 
pi3k inhibitors were more effective in cell lines with tp53 and pik3ca comutations than in those with wild - type tp53 . several trials have reported lower pcr rates with preoperative chemotherapy plus her2 - targeted therapies in patients whose her2 + cancers contain pik3ca mutations or in pten - low or phospho - 4ebp1 - high , pik3ca wild - type her2 + bcs.8 , 9 , 25 , 26 interestingly , in our trial , all the rd tissues that had been treated with preoperative chemotherapy with either h , l , or h + l , and those containing a pik3ca mutation , also contained a tp53 mutation . 
the therapeutic implications of these comutations in primary - refractory her2 + bc are not known ; however , kim et al24 have shown that pi3k inhibitors may be more effective in bc cell lines that have both tp53 and pik3ca mutations than in those that have only a pik3ca mutation . cdk12 amplication was observed in eight of the 17 rd specimens ( 47% ) , four of which also harbored tp53 and pik3ca comutations . 
cdk12 is located on chromosome 17q12 , just 165 to 267 kb proximal to erbb2 and is frequently coamplied with erbb2 in human bcs.27 , 28 cdk12 plays a critical role in the ddr and maintenance of genomic integrity , and also inuences atm levels and bc migratory capacity by regulating alternative last exon splicing.13 deletion or inhibition of cdk12 in cell lines or patient - derived xenografts impairs ddr and homologous recombination repair and decreases atm levels , thereby inducing brca - ness and sensitivity to parp inhibition.13 , 27 - 30 in 13% of her2 + bcs , the breakpoint of the her2 amplicon is within the cdk12 allele , likely leading to loss of the cdk12 tumor suppressor function.28 conversely , cdk12 can act as an oncogene , whereby cdk12 amplication and overexpression lead to tumor aggressiveness , increased migration and invasiveness , and poor clinical outcome.15 , 27 in the current study , the entire cdk12 gene was amplied in the rd tissues and there was no evidence of truncated cdk12 . 
it is also possible that cdk12 amplication was a passenger alteration in the her2 + rd tissues . the her2 + comutated rd tissue after preoperative h versus l versus h + l treatments showed activation on rppa of egfr and the pi3k / akt pathway . 
some pik3ca mutations in her2 - amplied models enhance her family signaling by the production of heregulin.31 resistance of her2 + cell lines to lapatinib is mediated by heregulindriven activation egfr / her3 / pi3k signaling.32 in addition , the egfr ligand amphiregulin is induced in the context of a pik3ca mutation in luminal as well as basal - like bcs , leading to egfr - driven proliferation.33 whether tp53 comutation inuences which egfr ligand ( or ligands ) is produced by pik3ca - mutant her2 + cells is not known . this study has some limitations . 
in addition , because ngs was done on the rd and a few available pretreatment biopsy specimens , this study cannot suggest whether the pcr rate in the comutant her2 + cancers is lower than the pcr rate in cancers with a single mutation and / or in cancers with wild type for both genes . 
 pik3ca tp53 comutation in her2 + breast cancer residual disease cell inltrates , and noncoding regulatory mechanisms associated with therapy resistance.34 - 36 shi et al8 conducted whole - exome sequencing of primary bcs in the neoaltto trial and showed that pathway - level alterations , not single gene mutations , were predictive of her2 - targeted therapy resistance . 
last , at the time the patients in our study were treated , the signicance of stromal til was not appreciated , and til were not assessed in this study.36 in conclusion , this study provides insights into the molecular alterations present within her2 + rd tissue after preoperative chemotherapy and h , l , or h + l treatment . 
levin , virginia espina , joyce oshaughnessy provision of study material or patients : frankie ann holmes , ying cao , lea krekow , kristi mcintyre , cynthia osborne , lance liotta collection and assembly of data : frankie ann holmes , maren k . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . frankie ann holmes consulting or advisory role : agendia , novartis , genomic health , myriad genetics , genentech , puma biotechnology , eli lilly , myriad genetics , novartis , amgen travel , accommodations , expenses : genomic health , puma biotechnology sohail balasubramanian employment : foundation medicine stock and other ownership interests : foundation medicine travel , accommodations , expenses : foundation medicine jeffrey s . 
j clin oncol 32 : 3744 - 3752 , 2014 slamon dj , eiermann w , robert nj , et al : ten year follow - up of bcirg - 006 comparing doxorubicin plus cyclophosphamide followed by docetaxel ( act ) with doxorubicin plus cyclophosphamide followed by docetaxel and trastuzumab ( acth ) with docetaxel , carboplatin and trastuzumab ( tch ) in her2 + early breast cancer . 
presented at san antonio breast cancer symposium , san antonio , tx , december 11 , 2015 chan a , delaloge s , holmes fa , et al : neratinib after trastuzumab - based adjuvant therapy in patients with her2 - positive breast cancer ( extenet ) : a multicentre , randomised , double - blind , placebo - controlled , phase 3 trial . 
lancet oncol 17 : 367 - 377 , 2016 cortazar p , zhang l , untch m , et al : pathological complete response and long - term clinical benet in breast cancer : the ctneobc pooled analysis . 
lancet 384 : 164 - 172 , 2014 gingras i , gebhart g , de azambuja e , et al : her2 - positive breast cancer is lost in translation : time for patient - centered research . 
nat rev clin oncol 14 : 669 - 681 , 2017 goel s , krop ie : pik3ca mutations in her2 - positive breast cancer : an ongoing conundruann oncol 27 : 1368 - 1372 , 2016 zardavas d , te marvelde l , milne rl , et al : tumor pik3ca genotype and prognosis in early - stage breast cancer : a pooled analysis of individual patient data . j clin oncol 36 : 981 - 990 , 2018 shi w , jiang t , nuciforo p , et al : pathway level alterations rather than mutations in single genes predict response to her2 - targeted therapies in the neo - altto trial . 
ann oncol 28 : 128 - 135 , 2017 loibl s , majewski i , guarneri v , et al : pik3ca mutations are associated with reduced pathological complete response rates in primary her2 - positive breast cancer : pooled analysis of 967 patients from ve prospective trials investigating lapatinib and trastuzumab . 
holmes fa , espina v , liotta la , et al : pathologic complete response after preoperative anti - her2 therapy correlates with alterations in pten , foxo , phosphorylated stat5 , and autophagy protein signaling . 
blazek d , kohoutek j , bartholomeeusen k , et al : the cyclin k / cdk12 complex maintains genomic stability via regulation of expression of dna damage response genes . 
boyault s , drouet y , navarro c , et al : mutational characterization of individual breast tumors : tp53 and pi3k pathway genes are frequently and distinctively mutated in different subtypes . 
nature 486 : 400 - 404 , 2012 jiang y - z , yu k - d , bao j , et al : favorable prognostic impact in loss of tp53 and pik3ca mutations after neoadjuvant chemotherapy in breast cancer . 
kotoula v , karavasilis v , zagouri f , et al : effects of tp53 and pik3ca mutations in early breast cancer : a matter of co - mutation and tumor - inltrating lymphocytes . 
luen sj , asher r , lee ck , et al : association of somatic driver alterations with prognosis in postmenopausal , hormone receptor - positive , her2 - negative early breast cancer . 
skoulidis f , byers la , diao l , et al : co - occurring genomic alterations dene major subsets of kras - mutant lung adenocarcinoma with distinct biology , immune proles , and therapeutic vulnerabilities . 
croessmann s , wong hy , zabransky dj , et al : pik3ca mutations and tp53 alterations cooperate to increase cancerous phenotypes and tumor heterogeneity . breast cancer res treat 162 : 451 - 464 , 2017 23 . 
rimawi mf , de angelis c , contreras a , et al : low pten levels and pik3ca mutations predict resistance to neoadjuvant lapatinib and trastuzumab without chemotherapy in patients with her2 over - expressing breast cancer . 
loibl s , darb - esfahani s , huober j , et al : integrated analysis of pten and p4ebp1 protein expression as predictors for pcr in her2 - positive breast cancer . 
cell division 12 : 7 , 2017 doi : 01.1186 / s13008 - 017 - 0033 - x johnson sf , cruz c , greifenberg ak , et al : cdk12 inhibition reverses de novo and acquired parp inhibitor resistance in brca wild - type and mutated models of triple - negative breast cancer . 
cell reports 17 : 2367 - 2381 , 2016 iniguez ab , stolte b , wang ej , et al : ews / fli confers tumor cell synthetic lethality to cdk12 inhibition in ewing sarcoma . 
perez ea , thompson ea , ballman kv , et al : genomic analysis reveals that immune function genes are strongly linked to clinical outcome in the north central cancer treatment group n9831 adjuvant trastuzumab trial . 
in this clinical trial , we applied these technologies to map the activity of signal pathway proteins in the human epidermal growth factor receptor ( her2 ) network , before and after patients received lapatinib ( l ) , or trastuzumab ( h ) , alone or in combination.10 because these two classes of molecular inhibitors target different parts the trial design provided a means to gather direct in vivo information about potential molecular mechanisms of additive or synergistic activity . the her2 / egfr signaling cascade , methods specimen collection and preservation we collected 16 - gauge core needle breast biopsy specimens before and after her2 targeted therapy and placed the specimens in a proprietary , ethanol - based xative for transport at 4c to george mason university ( mueller c , et al : plos one 6 : e23780 , 2011 )  . 
preand post - treatment core needle biopsy specimens were processed and analyzed at george mason university , center for applied proteomics and molecular medicine . archival formalin - xed parafn - embedded ( ffpe ) pretreatment and residual disease ( rd ) specimens were collected after informed consent was given . 
the specimen identication numbers are listed in appendix table a1 . laser capture microdissection frozen tissue sections from preand post - treatment core - needle biopsy specimens were xed in 70% ethanol , stained with mayers hematoxylin , dehydrated in graded alcohols ( 70% , 95% , 100% ) , and cleared in xylene . 
microdissected cells were stored at 80c before lysis reverse phase protein microarray printing . ffpe tissue sections for the pretreatment and rd specimens were subjected to laser capture microdissection of tumor tissue using an arcturusxt ( thermo fisher scientic ) in near - infrared capture mode . microdissected cells were stored at 80c before lysis and reverse phase protein microarray printing . reverse phase protein array construction / staining ( theralink assay ) the microdissected cells were subjected to lysis with a 10% ( volumeto - volume ratio ) solution of tris ( 2 - carboxyethyl ) phosphine ( tcep ; pierce , rockford , il ) or a 2.5% solution of 2 - mercaptioethanol ( sigmaaldrich , st louis , mo ) in tissue protein extraction reagent ( t - per ; pierce ) and tris - glycine 2x sds buffer ( thermo fisher scientic )  . 
cell lysates were stored at 80c before microarray construction . cellular lysates were printed in two - fold dilution series on glass - backed nitrocellulose array slides ( fast slides ; whatman , florham park , nj , or sartorius stedim biotech sa , germany ) using an aushon 2470 arrayer ( aushon biosystems , billerica , ma ) equipped with 350 - m pins . 
the negative control slide was incubated with antibody diluent ( agilent )  . secondary antibody was goat anti - rabbit igg h + l ( 1 : 7 , 500 ; vector labs , burlingame , ca ) or rabbit anti - mouse igg ( 1 : 10 ; agilent )  . subsequent signal detection was amplied via horseradish peroxidasemediated biotinyl tyramide deposition with chromogenic detection ( diaminobenzidine ) for the preand post - treatment specimens or uorescent dye ( cy5 ) for the rd specimens . total protein per microarray spot was determined with a sypro ruby protein stain ( thermo fisher scientic ) per manufacturers directions and imaged with a ccd camera ( novaray ; alpha innotech , san leandro , ca ) or genepix scanner ( molecular devices )  . reverse phase protein array analysis the frozen preand post - treatment study set was analyzed in four batches : june 2008 ( n = 23 intent - to - treatevaluable [ itt - e ] samples ) , october 2008 ( n = 12 itt - e samples ) , april 2009 ( n = 29 itt - e samples ) , and november 2010 ( n = 95 itt - e samples )  . 
on each array set , the undiluted spot was used to quantify protein levels for patient samples . array slides were scanned at 600 dpi on a atbed scanner ( umax powerlook ; umax technologies , taiwan ) and saved in a .tiff format ( adobe photoshop ; adobe , san jose , ca )  . 
if the coefcient of variance between replicates was greater than 20% , the spot was agged and a value of coefcient of variance too high was reported . signal intensity from the secondary antibody - alone ( negative control ) slide was subtracted from the signal intensity of the primary antibody slide . 
the scores are reported as a value from 0 to 3 on the basis of the population mean for each individual analyte . spearmans correlations and mann - whitney u tests were performed on one pretreatment biopsy specimen and 12 patients rd specimens to compare samples with pik3ca - tp53 comutation with those without comutation ( table a3 ; data supplement 2 )  . statistical analysis all biomarker analyses were conducted on the itt - e population . wilcoxon rank - sum test was used to calculate group differences if the data were not normally distributed ( espina v , et al : plos one 5 : e10240 , 2010 )  . 
student t test was used if the data were normally distributed ( r software , r project for statistical computing ; sas , sas institute , cary , nc )  . 
we gathered proteomic data on the state of the signal pathway networks directly or indirectly inuenced by her2 in the tumor cells at three distinct time points related to therapy : ( 1 ) before administration of h or l or h + l ; ( 2 ) after 14 days of l or h or h + l therapy ; and ( 3 ) in the rd tissue specimens after h or l or h + l and chemotherapy.10 we correlated the data for the before and after h or l or h + l therapy to the pcr . specimens 16 and 20 ( us oncology identication numbers 1 and 195 , respectively ) had equivocal her2 immunohistochemistry results in the post - treatment specimens . 
evaluation of specimen 20 by reverse phase protein array for egfr / her2 family activation conrmed that the her2 , her2 tyr1248 , and her3 levels were greater than 1 sd below the populations means , compared with the study population data . 
however , we discovered activation of egfr in the posttreatment tumor specimen , compared with the study population ( specimen 20 : egfr = 32.27 , population mean = 27.95 ; data supplement 1 )  . heterogeneous signal transduction pathway signaling in rd specimens autophagy - , inammation - , and proliferation - associated proteins were activated in the rd specimens , but there was a lack of concordance between protein activation and pik3ca / tp53 comutations ( data supplement 1 )  . 
compensatory or adaptive changes after therapy provide insights concerning whether that pathway is an essential or collateral driver of the cancer . integrated genomic and proteomic analysis can elucidate the interplay between potential driver mutations and signal transduction pathways . pten catalytic activity is necessary for its tumor suppressor function . most pten missense mutations affect the phosphatase domain and cause a loss in pten phosphatase activity ( torres j , et al : j biol chem 276 : 993 - 998 , 2001 )  . 
many pten nonsense or frame - shift mutations are targeted to the c - terminal domain of the protein , which harbors serine phosphorylation sites ( torres j , et al : j biol chem 276 : 993 - 998 , 2001 )  . 
increased phosphorylation at ser380 results in decreased pten activity ( ie , less tumor suppression through pi3 ; yang z , et al : oncotarget 6 : 31916 - 31926 , 2015 ; yu h , et al : nat rev cancer 4 : 91 - 105 , 2004 )  . 
pten is phosphorylated at ser 380 by casein kinase 2 ( ck2 ) , thus stabilizing pten but suppressing its phosphatase activity ( torres j , et al : j biol chem 276 : 993 - 998 , 2001 )  . 
pd - 1 was recently shown to inhibit this stabilizing phosphorylation of ser380 in the c - terminal domain of pten ( patsoukis n , et al : mol cell biol 33 : 3091 - 3098 , 2013 )  . 
ck2 is a target of pd - 1 and pd - 1 has been shown to decrease pten expression while increasing pten activity , which , in turn , inhibits the pi3k / akt pathway ( patsoukis n , et al : mol cell biol 33 : 3091 - 3098 , 2013 )  . 
thus , the higher phosphorylation levels of pten ser380 that we identied in patients with pik3ca / tp53 comutations ( fig 3 ) could contribute to tumor proliferation and thus a lack of pcr . 
the role of immune cell function and pd - 1 expression in these specimens could also modulate tumor proliferation . inammation and jak / stat signal pathways overexpression of her2 in breast cancer cell lines has been induced , in part , by jak2 and prolactin ( yamauchi t , et al : j bio chem 275 : 33937 - 33944 , 2000 )  . 
jak2 is required for phosphorylation of the signal transducers and activators of transcription ( stat ) proteins stat3 and stat5 , thus activating a survival / proliferation axis ( watson cj , et al : cell death differ 21 : 185 - 186 , 2014 )  . 
cd4 / cd8 dual immunohistochemistry using biocare medical ( pacheco , ca ) antibody cocktail was performed to assess the location , quantity , and type of t cells in the preand post - treatment specimens . 
murray leslie samuel paolo nuciforo jose jimenez guillem argiles rodrigo dienstmann josef tabernero lucia picariello luca messerini stefania nobili enrico mini kieran sheahan elizabeth ryan ( continued ) purpose transcriptomic profiling of colorectal cancer ( crc ) has led to the identification of four consensus molecular subtypes ( cms1 to 4 ) that have prognostic value in stage ii and iii disease . 
2018 by american society of clinical oncology introduction colorectal cancer ( crc ) has the third highest worldwide incidence.1 although 75% of patients present with operable diseasemainly stages ii and iiiapproximately 40% experience disease recurrence.2 compared with surgery alone , adjuvant chemotherapy improves survival in only approximately 3% of patients with stage ii disease , rising to 15% to 20% for those with stage iii disease . 
 contributed equally to this work . corresponding author : daniel longley , phd , centre for cancer research and cell biology , queens university belfast , 97 lisburn rd , belfast , bt9 7bl united kingdom ; e - mail : d.longley@qub.ac.uk. licensed under the creative commons attribution 4.0 license significant advances have been made in the molecular stratification of crc , leading to the identification of four consensus molecular subtypes ( cms1 to 4 ) .3 cms1 is enriched for microsatellite instability , is immune rich , and correlates with good prognosis , and cms4 is stromal rich , with high levels of cancer - associated fibroblasts , and has a relatively poor prognosis . 
 cms3 is defined by the activation of multiple metabolic pathways , potentially as a result of its enrichment for kras mutations.4 the epithelial - rich cms2 is the largest group , accounting for approximately 40% of all tumors . 
of these , 188 samples with > 50% tumor content passed quality control and were subjected to rna and dna analysis ( appendix )  . transcriptomics high - quality transcriptomics data were obtained for 156 of the 188 samples ( almac xcel array ; almac diagnostics , craigavon , united kingdom )  . 
residual technical batch effects were corrected using the combat method ( sva package ) , and data were deposited in the national center for biotechnology information gene expression omnibus repository ( gse103479 )  . 
the clinical pathologic details of this cohort are provided in table 1 . data analysis gse3958210 and gse1433311 crc data sets were downloaded from the national center for biotechnology information gene expression omnibus repository and their respective cel files uploaded into r . 
similar results were obtained in the larger gse39582 cohort for stage ii disease ( log - rank test p = .071 ) , whereas in stage iii disease , this correlation reached significance ( p = .001 ; data supplement )  . 
when we combined the taxonomy and gse39582 cohorts to increase statistical power , the benefit from adjuvant chemotherapy for cms2 was significant in both stage ii disease ( log - rank test p = .02 ; hazard ratio [ hr ] , 0.21 [ wald test p = 3.52 102 ] ; fig 1a ) and stage iii disease ( log - rank test p < .001 ; hr , 0.22 [ wald test p = 1.48 104 ] ; fig 1b )  . 
of note , no significant benefit from adjuvant chemotherapy was observed in cms1 or cms4 , although a nonsignificant trend was observed in cms4 stage iii disease ( log - rank test p = .089 ; data supplement )  . these results suggest that the more epithelial cms2 and cms3 subgroups benefit from adjuvant chemotherapy . 
in support of this , in a combined analysis of cms2 and cms3 , benefit from adjuvant chemotherapy was significant in both stage ii disease ( log - rank test p = .0042 ; hr , 0.16 [ wald test p = .012 ] ; fig 1c ) and stage iii disease ( log - rank test p < .001 ; hr , 0.20 [ wald test p = 1.14 106 ] ; fig 1d )  . 
in contrast , in a combined analysis of the cms1 and cms4 subgroups , no benefit from adjuvant chemotherapy was observed ( data supplement )  . when cms2 subgroup results for stage ii disease were adjusted for t stage ( t4 v t3 ) , age , and sex using cox proportional hazards regression analysis , the significance of the benefit from chemotherapy was lost ( hr , 0.31 ; wald test p = .121 ; log likelihood ratio , 7.0 105 ; fig 1e ) ; however , in stage iii disease , adjusting for t stage ( t4 or n2 v t1 to t3 / n1 ) , age , and sex , the significance of benefit from chemotherapy in cms2 was maintained ( hr , 0.27 ; wald test p = .007 ; log likelihood p = 3.25 105 ; fig 1f )  . 
in cox proportional hazards regression analyses of the combined cms2 and cms3 subgroups , the significance of benefit from chemotherapy was maintained in stage ii disease ( hr , 0.23 ; wald test p = .049 ; log likelihood ratio , 2.72 105 ; fig 1g ) and stage iii disease ( hr , 0.21 ; wald test p < .001 ; log likelihood p = 3.19 107 ; fig 1h )  . clinical implications of tumor - intrinsic stratification in cms2 as previously reported , 6 there are limited associations between cms and cris classifications for example , cms4 is distributed relatively evenly between the five cris subtypes ( data supplement ) ; however , some clear patterns were observed , with cms2 almost exclusively distributed between cris - c , - d , and - e ( fig 2a )  . 
 subsequently , we investigated whether substratification of cms2 into cris - c , - d , or - e could identify a more specific subset of patients with stage ii and iii disease who derive benefit from adjuvant chemotherapy . 
these results were confirmed in an additional independent cohort , gse14333 ( logrank test p = .02 ; hr , 0.12 [ wald test p = .05 ] ; data supplement )  . 
in the other 2 cris subgroups ( cris - a and - b ) , no significant benefit from adjuvant chemotherapy was observed in either stage ii or iii disease , although a nonsignificant trend was observed in cris - a for stage iii disease ( p = .057 ; data supplement ) , which is consistent with this subgroup being enriched for cms3 , where a significant benefit was observed ( data supplement )  . 
when cris - c results were adjusted for t stage , age , and sex using cox proportional hazards regression analyses , the benefit from chemotherapy maintained significance in stage ii disease ( hr , 0.12 ; wald test p = .045 ; log likelihood p = .0054 ; fig 2d ) and stage iii disease ( hr , 0.27 ; wald test p = .02 ; log likelihood p = 1.11 103 ; fig 2e ) ; furthermore , for combined stage ii and iii disease , adjusted hr was 0.20 ( wald test p < .001 ; log likelihood p = 7.5 106 ; data supplement )  . 
 ( a and b ) kaplan - meier plots of 5 - year overall survival ( os ) for consensus molecular subtype 2 ( cms2 ) patients who received adjuvant fluorouracil ( fu ) - based treatment ( gold ) and those who did not receive treatment ( surgery alone , blue ) , in the ( a ) stage ii combined ( taxonomy and gse39582 ) cohort and the ( b ) stage iii combined ( taxonomy and gse39582 ) cohort . 
 ( c and d ) kaplan - meier plots for 5 - year os for combined cms2 and cms3 patients in the ( c ) stage ii combined ( taxonomy and gse39582 ) cohort and the ( d ) stage iii combined ( taxonomy and gse39582 ) cohort . 
to account for potential intratumoral heterogeneity of putative biomarkers in specific tumor regions , tmas were generated from the taxonomy cohort to incorporate three cores each from ct , if , and tumor - adjacent sr regions . 
cd8 and cd3 levels were defined using immunohistochemistry , and patients were stratified into high and low groups using the median as cutoff ( representative cd8 and cd3 images ; figs 3a and 3b )  . 
we further assessed cd8 + lymphocytes in histologically normal tissue adjacent to the tumor and found no difference in survival between high and low cd8 levels ( log - rank test p = .72 ; data supplement )  . 
of note , no correlations were found between cd3 + lymphocyte levels and prognosis ( if log - rank test p = .55 ; sr log - rank test p = .75 ; ct log - rank test p = .8 ; normal log - rank test p = .82 ; data supplement )  . for each patient , cd8 scores in each tumor subregion correlated closely with one another ( p < .001 ; data supplement )  . 
 as expected on the basis of correlations for individual regions ( data supplement ) , applying this tumor average score to the combined stage ii and iii taxonomy cohort revealed that high levels of cd8 + lymphocytes identified cris - c patients with good prognosis ( log - rank p = .0031 ; hr , 12.18 [ wald test p = .0191 ] ; fig 4a )  . 
in contrast , average cd3 scores , which again did not correlate closely with average cd8 scores ( fig 3c ) , were not prognostic ( fig 4b )  . 
of note , cd8 mrna expression was unable to distinguish good and poor prognosis patients ( log - rank p = .83 ; data supplement ) , which indicates the need for immunohistochemistry in combination with transcriptomic profiling for effective prognostication . 
 ( e - h ) forest plots show the results from the adjusted cox proportional hazards regression analysis for the ( e ) stage ii cms2 combined cohort , the ( f ) stage iii cms2 combined cohort , the ( g ) stage ii cms2 and cms3 combined cohort , and the ( h ) stage iii cms2 and cms3 combined cohort . 
for adjusted analyses , data are stratified by treatment and adjusted for t stage , sex , and age in stage ii , and for age and sex in stage iii . 
 ( a ) caleydo plots display mapping of patient samples from the consensus molecular subtype 2 to the colorectal cancer intrinsic subtypes ( cris ) in the combined ( taxonomy and gse39582 ) data sets . 
 ( a and b ) representative images of samples display high and low ( a ) cd8 and ( b ) cd3 expression in each of the three tumor regions sampled : invasive front ( if ) , stromal rich ( sr ) , and central tumor ( ct )  . 
 ( a - c ) kaplan meier plots of patients with ( a ) cd8 - high versus cd8 - low stage ii and iii disease in the colorectal cancer intrinsic subtype ( cris ) - c surgery - only , taxonomy cohort ; ( b ) cd3 - high versus cd3 - low stage ii and iii disease in the cris - c surgery - only , taxonomy cohort ; and ( c ) cd8 - high versus cd8low stage ii disease in the cris - c surgery - only , taxonomy cohort . 
therapeutic benefit from adjuvant chemotherapy is modest for this group as a whole , with an absolute improvement in survival of approximately 3%.18 - 22 currently , additional pathologic characteristics , such as obstruction , perforation , extramural venous invasion , and t stage ( t4 ) , are used to identify poor prognostic stage ii disease and guide the decision of whether to start chemotherapy treatment.23 additional methods of assessing the risk of recurrence in the adjuvant disease setting have been the focus of many studies in recent years , 24 - 29 which has led to the development of the 12 - gene oncotype dx assay.30 this algorithm has been extensively clinically tested31 - 33 and demonstrated to identify patients with stage ii disease who are at higher risk of recurrence and patients with stage iii disease who are at lower risk of recurrence.34 , 35 additional signatures have been proposed , including the 18 - gene prognostic classifier , known as coloprint , 36 and the 634 - gene prognostic classifier , known as coldx.27 the current study indicates that the transcriptionally definable cms2 / cris - c patient subgroup may be the cohort of patients within stage ii disease that benefits from standard adjuvant fu - based chemotherapy . 
these data correlate well with our previous study on the prognostic significance of immune - derived programmed death ligand 1 mrna expression in crc , in which we postulated that patients with low immune infiltrates would significantly benefit from adjuvant fu - based chemotherapy after surgery.9 , 37 meta - analysis of the idea ( international duration evaluation of adjuvant chemotherapy ) collaboration examined whether a 3 - month duration of oxaliplatin containing adjuvant chemotherapyfolfox4 , modified folfox6 , or xeloxis as effective as a 6 - month schedule in patients with stage iii crc . 
this study found that the 3 - month treatment was almost as effective as the 6 - month treatment and reduced the risk of treatment associated toxicity , thus concluding that a 3 - month treatment would be more beneficial for patients with low - risk ( t1 to 3 / n1 tumors ) stage iii disease.38 our study suggests that levels of cd8 + lymphocytes could also be used to identify such low - risk patients , at least in the cris - c subgroup . 
of note , cris - c is enriched for mutant tp53 and wild - type kras tumors , 6 but neither of these established molecular markers provided additional information with regard to disease outcome within the cris - c subgroup . collectively , these results provide the first evidence of the predictive value of the now well established cms and more recently described cris transcription - based classification systems . 
 our results also emphasize the utility of combining cms and cris subtyping in a substratification strategy to maximize clinical benefit from adjuvant fu - based chemotherapy in patients with stage ii and iii crc . 
murray , leslie samuel , jose jimenez , guillem argiles , lucia picariello , luca messerini , stefania nobili , enrico mini , elizabeth ryan , sandra van schaeybroeck , daniel b . 
longley tumor - infiltrating lymphocytes , would potentially enable the prospective identification of the cris - c / cd8 - low stage ii patients who significantly benefit from adjuvant fu - based chemotherapy . 
however , we recognize that there are a number of limitations in the current study , which was conducted on a relatively small number of retrospective samples that were collected outside of clinical trials , and we realize that this hypothesis - generating study now requires validation in either larger patient cohorts or stratified trial cohorts enriched for the cris - c patient subtype . 
nonetheless , this study suggests that transcription - based classification systems , such as cms and cris , have the potential to be developed into patient stratification tools and , when used alone or alongside other molecular pathology approaches , such as immunohistochemistry , could enable the selection of patients with crc who are most likely to benefit from adjuvant chemotherapy , while at the same time sparing nonresponders the potentially harmful treatment related adverse events and sequelae of chemotherapy . 
of importance , the cris subtyping method uses gene expression from tumor epithelial cells only and is independent of stromal - derived signals ; therefore , the cris subgroups can be detected irrespective of the profiling technology used or the tissue source.15 such robustness and reproducibility are critical for clinical translation . 
murray , leslie samuel , paolo nuciforo , jose jimenez , guillem argiles , josef tabernero , lucia picariello , luca messerini , stefania nobili , enrico mini , kieran sheahan , elizabeth ryan , sandra van schaeybroeck , mark lawler , daniel b . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . richard wilson consulting or advisory role : merck serono , sirtex medical , amgen , servier , clovis oncology , halozyme , bristol - myers squibb research funding : almac group ( inst ) travel , accommodations , expenses : merck serono , amgen vicky m . 
murray research funding : vertebrate antibodies ( inst ) leslie samuel consulting or advisory role : mundipharma research funding : mologen ( inst ) , roche ( inst ) , merck ( inst ) , eli lilly ( inst ) , taiho pharmaceutical ( inst ) travel , accommodations , expenses : mologen wendy l . 
longley stock and other ownership interests : fusion antibodies consulting or advisory role : astex pharmaceuticals sandra van schaeybroeck no relationship to disclose mark lawler honoraria : pfizer research funding : astex pharmaceuticals patents , royalties , other intellectual property : inhibitors of the antiapoptotic protein flip travel , accommodations , expenses : astex pharmaceuticals affiliations wendy l . 
murray and leslie samuel , national health service grampian , aberdeen , united kingdom ; najeeb ashraf syed and puthen veettil jithesh , sidra medical and research center , qatar ; paolo nuciforo , jose jimenez , guillem argiles , rodrigo dienstmann , and josef tabernero , university hospital vall dhebron , barcelona , spain ; lucia picariello , luca messerini , stefania nobili , and enrico mini , university of florence , florence , italy ; and kieran sheahan and elizabeth ryan , university college dublin , dublin , ireland . funded by cancer research uk grants no . 
lenz h - j , ou f - s , venook ap , et al : impact of consensus molecular subtyping ( cms ) on overall survival ( os ) and progression free survival ( pfs ) in patients ( pts ) with metastatic colorectal cancer ( mcrc ) : analysis of calgb / swog 80405 ( alliance )  . 
dunne pd , mcart dg , bradley ca , et al : challenging the cancer molecular stratification dogma : intratumoral heterogeneity undermines consensus molecular subtypes and potential diagnostic value in colorectal cancer . 
marisa l , de reynis a , duval a , et al : gene expression classification of colon cancer into molecular subtypes : characterization , validation , and prognostic value . 
jorissen rn , gibbs p , christie m , et al : metastasis - associated gene expression changes predict poor outcomes in patients with dukes stage b and c colorectal cancer . 
galon j , costes a , sanchez - cabo f , et al : type , density , and location of immune cells within human colorectal tumors predict clinical outcome . 
hutchins gga , treanor d , wright a , et al : intratumoral stromal morphometry predicts disease recurrence but not response to 5 - fluorouracil : results from the quasar trial of colorectal cancer . 
roepman p , schlicker a , tabernero j , et al : colorectal cancer intrinsic subtypes predict chemotherapy benefit , deficient mismatch repair and epithelial - to - mesenchymal transition . 
figueredo a , charette ml , maroun j , et al : adjuvant therapy for stage ii colon cancer : a systematic review from the cancer care ontario program in evidence - based cares gastrointestinal cancer disease site group . 
kelley rk , venook ap : prognostic and predictive markers in stage ii colon cancer : is there a role for gene expression profiling ? clin colorectal cancer 10 : 73 - 80 , 2011 26 . 
kennedy rd , bylesjo m , kerr p , et al : development and independent validation of a prognostic assay for stage ii colon cancer using formalin - fixed paraffin - embedded tissue . 
tabernero j , salazar r , roepman r , et al : additional validation of a genomic signature ( coloprint ) for the risk stratification of stage ii colon cancer patients . 
oconnell mj , lavery i , yothers g , et al : relationship between tumor gene expression and recurrence in four independent studies of patients with stage ii / iii colon cancer treated with surgery alone or surgery plus adjuvant fluorouracil plus leucovorj clin oncol 28 : 3937 - 3944 , 2010 31 . 
gray rg , quirke p , handley k , et al : validation study of a quantitative multigene reverse transcriptase - polymerase chain reaction assay for assessment of recurrence risk in patients with stage ii colon cancer . 
venook ap , niedzwiecki d , lopatin m , et al : biologic determinants of tumor recurrence in stage ii colon cancer : validation study of the 12 - gene recurrence score in cancer and leukemia group b ( calgb ) 9581 . 
cartwright t , chao c , lee m , et al : effect of the 12 - gene colon cancer assay results on adjuvant treatment recommendations in patients with stage ii colon cancer . 
srivastava g , renfro la , behrens rj , et al : prospective multicenter study of the impact of oncotype dx colon cancer assay results on treatment recommendations in stage ii colon cancer patients . 
dunne pd , mcart dg , oreilly pg , et al : immune - derived pd - l1 gene expression defines a subgroup of stage ii / iii colorectal cancer patients with favorable prognosis who may be harmed by sdjuvant chemotherapy . 
shi q , sobrero af , shields af , et al : prospective pooled analysis of six phase iii trials investigating duration of adjuvant ( adjuv ) oxaliplatin - based therapy ( 3 vs 6 months ) for patients ( pts ) with stage iii colon cancer ( cc ) : the idea ( international duration evaluation of adjuvant chemotherapy ) collaboration . 
 appendix development of a multiomics patient cohort the taxonomy cohort was assembled from an initial cohort of 363 patients with stage ii and iii disease from four european centers ( vall dhebron institute of oncology , barcelona , spain ; st vincents university hospital , dublin , ireland ; university of florence , florence , italy ; and university of aberdeen , aberdeen , united kingdom )  . 
this work was approved by the medicine , dentistry , and biomedical sciences school ethics committee ( ref : 12 / 12v4 )  . samples from 194 patients with 50% or more tumor content as assessed by hematoxylin and eosin staining were subjected to rna extraction . 
 data for samples were preprocessed and aligned according to best practices ( broad institute : tute.org / gatk / discussion / 3060 / how - should - i - pre - process - data - from - multiplexed - sequencing - and - multi - library - designs ) using burrows - wheeler aligner for alignment and gatk 3.4 for realignment and recalibration . 
cd8 was detected using the anti - cd8 antibody c8 / 144b ( dako , carpinteria , ca ) using the leica bond max staining platform ( leica microsystems , wetzlar , germany )  . 
for each tumor core , cd3 + and cd8 + t - cell populations were scored using the open access image analysis software qupath ( bankhead p , et al : sci rep 7 : 16878 , 2017 )  . 
measurements of tissue area and positive cell counts for each core provided cell density measurements , which are expressed as the number of positive cells per square millimeter of tissue . 
high and low cd3 / cd8 levels were calculated using the median level as cutoff . statistical analyses for kaplan - meier survival analysis and cox proportional hazards regression analysis , significance was assessed using log - rank and wald tests , respectively . 
cox proportional hazards regression analysis was used to assess overall survival at 5 years for adjuvant chemotherapy before and after adjustment for age , t stage , and sex ( stage ii and iii ) and age , sex , and stage ( stage ii and iii combined )  . 
 c subgrouping of unfavorable histology neuroblastomas with immunohistochemistry toward precision prognosis and therapy stratication naohiko ikegaki , phd1 and hiroyuki shimada , md , phd2 , for the international neuroblastoma pathology committee introduction neuroblastoma , as well dened by willis , 1 is an embryonal tumor of neural crest origtumors of the neuroblastoma group include neuroblastoma , ganglioneuroblastoma , and ganglioneuroma . 
we believe that all ganglioneuromas were once neuroblastomas in the early stage of tumor development.1 , 2 they are collectively called peripheral neuroblastic tumors ( pnts ) and are known to present with a wide range of clinical behavior , from spontaneous regression and tumor maturation to aggressive progression that is refractory to intensive treatment . 
these observations have led us to seek additional immunohistochemical biomarkers that are tightly associated with aggressive behaviorsthat is , unresponsiveness or resistance to the current intensive multimodal therapyof certain uh tumors . 
to address this problem , we and others have sought and identied the expression of potentially drug - targetable proteins that are responsible for their aggressive progression in the uh group . 
when we seek such biomarkers , they are preferably actionable / druggable by existing pharmaceutical agents , us food and drug administration approved , or currently tested in human clinical trials . 
of note , these three types of highly aggressive neuroblastomasthat is , myc - driven neuroblastoma , alt phenotype neuroblastoma because of atrx loss , and tert - overexpressing neuroblastoma with gene rearrangementare mutually exclusive and seem to comprise the majority of therapy - resistant or refractory uh neuroblastomas . these three markersthat is , myc family proteins , tert , and atrx can be the subjects of immunohistochemical assay and potentially incorporated in future inpc . it should be noted that other than the above gene and expression alterations found in aggressive uh neuroblastomas , alk mutations and amplication are found in approximately 10% of sporadic neuroblastoma cases.20 , 21 it was also found that alk gene amplication and f1174 mutations are associated with mycn amplication.22 moreover , alk overexpression as a result of alk amplication / mutations seems to be responsible for its oncogenic activity23 ; however , the prognostic signicance of alk mutations / overexpression has been controversial , as some reports suggest an association of alk mutations / overexpression with fatal outcomes of the disease , whereas others suggest otherwise.22 , 23 in particular , regairaz et al24 showed immunohistochemically that expression of alk and its active form palk was observed in many neuroblastomas independent of alk mutation / amplication . 
in this regard , myc / mycn and tert overexpression26 - 29 has been linked to the stemness of tumor cells , and direct and indirect therapeutic targeting of these alterations suppresses the stemness of aggressive and therapy - resistant uh neuroblastomas . 
similarly , alt is linked to tumor stem cells.30 , 31 these observations allow us to incorporate the information into the inpc toward the goal of precision prognosis and therapy stratication . our plan is to rene the uh neuroblastoma stratication using immunohistopathologic analysis with antipan - myc antibody ( or anti - mycn and anti - myc ) , anti - tert antibody , and anti - atrx antibody . 
it is expected that the nonresponder to current high - risk therapymyc , tert , and atl subgroups could be separated from the possible respondernull subgroupwith a high probability before the initiation of therapy : myc subgroup : myc - driven neuroblastoma shows augmented expression of mycn protein and / or myc proteas myc family protein overexpression stimulates rrna synthesis and protein translation , neuroblastoma cells in this subgroup often exhibit prominent nucleolar formationnucleolar hypertrophyand hypertrophic cell morphology.13 , 14 because of the presence of one to a few prominent nucleoli , myc - driven neuroblastoma is cytologically distinguishable from the conventional small blue - cell neuroblastoma with salt - and - pepper nuclei . myc - driven neuroblastomas , which comprise more than 50% of high - risk neuroblastomas , includes rare and unique tumor , named large - cell neuroblastoma , characterized by the bulls eye appearance of enlarged and uniquely open euchromatin - rich nuclei that contain highly conspicuous nucleoli.33 most large - cell neuroblastomas overexpress higher levels of mycn or myc protein than other myc - driven neuroblastomas . 
their euchromatin - rich open nuclei suggest the stem celllike nature of the tumor cells.29 a considerable number of myc - driven neuroblastomas are also associated with tert overexpression , as tert is a direct transcriptional target of myc family proteins . 
tert can also stabilize myc protein via its noncanonical enzymatic function , creating a positive feedback loop between mycn / myc and tert expression.34 , 35 tert subgroup : tert is the protein component of telomerase , which also includes terc , the telomerase rna component . 
immunohistochemical grading of tert is performed in essentially the same way as that of myc family proteins . estimated survival of each subgroup is based on wang et al12 and valentijn et al.18 to exclude the possibility of overlooking alt cases with atrx point mutations with no atrx loss and / or rare daxx mutations , patients older than age 5 years in the null group can be subjected to additional screening by either rdna32 or telomeric uorescence in situ hybridization assay.32a likely a result of long - range genomic rearrangements but not to promoter mutations in neuroblastoma.36 tert promoter hypermethylation may also be involved in its activating mechanism.37 , 38 alt subgroup : atrx loss results in the alt phenotype . atrx mutation is rarely observed in the myc and tert subgroups , and loss of atrx is exclusively observed in patients with neuroblastoma older than age 5 years.17 because a normal atrx function is to insert the variant histone h3 , namely h3.3 , in concert with daxx , into chromatin to maintain transcriptionally active euchromatin , 39 atrx loss may result in a more transcriptionally inactive heterochromatic state . 
thus , histologic / cytologic appearance of the alt subgroup could be the conventional type with salt - and - pepper nuclei . null subgroup : there are still uh neuroblastomas without myc family protein overexpression , tert overexpression , and atrx loss . 
strategies under consideration include , but are not limited to , transcriptional repression of myc and mycn genes by g - quadruplex ( g4 ) stabilizers , 42 , 43 bromodomain and extraterminal protein inhibitors , 44 , 45 and inhibitors of a transcriptional cyclin - dependent kinase 746 , 47 ; destabilization of mycn by aurora kinase a inhibitors48 and of myc and mycn proteins by ras signaling pathway inhibitors49 - 51 ; and translational blockade of myc mrna by eif4f inhibition and stabilization of rna g4 by rna g4 ligands.52 , 53 we recognize that uh tumors with high - level myc family protein expression tend to exhibit hypertrophic nucleoli , 13 , 14 which indicates that they are highly active in rrna synthesis and protein translation . 
small - molecule inhibitors , including cx - 5461 , an rna polymerase i inhibitor , and halofuginone , a protein translation inhibitor , could therefore effectively target these pathophysiologic features . as we have shown , these inhibitors in fact downregulate myc family protein expression in neuroblastoma cells.13 for those patients with tert - overexpressing neuroblastoma , telomerase inhibitors can be considered . 
if so , is there any other way by which the alt phenotype can be suppressed ? to address this question , we need to understand the mechanism of how atrx loss leads to alt . 
it has become evident that the acquisition of the alt phenotype uses the dna replication stress response , 30 which involves a cascade of events , including the obligatory activation of atr ( ataxia telangiectasia and rad3 related ) kinase . azd6738 is a novel potent and selective inhibitor of atr kinase with ic50 values of less than 1 mm in cell - based assays58 and would effectively target alt tumor cells . conclusion prognosis and therapy stratication of neuroblastomas have steadily improved since the introduction of the evans staging system59 with age used as a prognostic factor60 ; however , 5 - year survival of patients with high - risk neuroblastoma , dened by the international neuroblastoma risk group system ( inrg ) , remains at approximately 40% or lower.61 , 62 the same is true for the uh neuroblastoma group , which essentially overlaps high - risk neuroblastomas.8 , 63 unfortunately , no additional renement for the inrg has been proposed since 2009.61 the proposed histologic subgrouping of uh neuroblastomas represents a practical and immediately implementable approach with which to create the category leading to the most devastating clinical outcome , namely extremely unfavorable histology ( euh ) neuroblastoma . 
we expect that conventional uh neuroblastoma tumorsthat is , the null subgroupwould , we hope , respond to the current multimodal high - intensity therapy designed for high - risk neuroblastoma , whereas euh tumorsthat is , those of the myc , tert , and alt subgroupswould not . 
for those euh tumors , appropriate therapy protocols will have to be designed and tested . on the basis of our ndings , 12 myc family protein immunohistochemistry is already incorporated in the childrens oncology group pathology analysis as an integrated biomarker of neuroblastoma . 
similar attempts are now underway for tert and atrx immunohistochemistry for precision prognosis and the stratication of neuroblastoma . furthermore , we are planning to perform correlative studies between tert protein expression and tert gene rearrangements and between atrx protein loss and atrx gene mutations / deletions . 
for more information about ascos conict of interest policy , please refer to or po.ascopubs.org / site / ifc . no potential conicts of interest were reported . references willis r : neuroblastoma and ganglioneuroma . 
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 elevated levels of brafv600 mutant circulating tumor dna and circulating hepatocyte growth factor are associated with poor prognosis in patients with metastatic melanoma purpose we performed a retrospective exploratory analysis to evaluate the prognostic and predictive effect of two circulating biomarkers , brafv600 mutant circulating tumor dna ( ctdna ) and circulating hepatocyte growth factor ( chgf ) , in metastatic melanoma . materials and methods this study evaluated patients from brim - 3 , a phase iii trial comparing vemurafenib and dacarbazine in 675 patients with brafv600 mutated advanced melanoma . 
the use of circulating biomarkers has been an attractive strategy , primarily because of the ease of sample collection , and in the case of circulating tumor dna ( ctdna ) william lu luciana burton james larkin paul b . 
 and circulating tumor cells , the possibility that a traditional tissue biopsy may not reflect the current mutational landscape of a patients cancer.4 - 6 in this study , we characterized two circulating biomarkers for brafv600 - positive metastatic melanoma with the goal of using a combined multibiomarker approach to assess patient risk . approximately half of melanomas harbor mutations in the braf gene , and over 90% of these braf mutations occur at a single site , valine 600 ( v600 ) .7 - 9 early ctdna studies demonstrated the ability to detect brafv600e ctdna in patient serum and plasma , and in addition , some studies showed that the presence of ctdna correlated with worse survival and stage.10 - 19 some studies performed longitudinally demonstrated that a decrease in ctdna was observed after treatment but increases at progression.20 - 24 these studies have suggested that ctdna may be a useful prognostic indicator and , given the rapid kinetics of ctdna , 25 , 26 may also be useful in monitoring patients to predict disease progression . the introduction of braf inhibitor therapies , such as vemurafenib , have dramatically prolonged the survival of patients with braf - mutated metastatic melanoma.2 , 3 , 8 , 27 however , patients treated with braf inhibitor therapy often relapse , and mechanisms by which tumors obtain resistance are of considerable interest.3 , 27 , 28 one mechanism that has been described is the activation of the met signaling pathway by hepatocyte growth factor ( hgf ) .29 , 30 like ctdna , hgf is also detectable in circulation and can potentially be used as a prognostic or predictive biomarker . 
 studies assessing hgf as a circulating cancer biomarker have supported the idea that high levels of this ligand can support tumor growth , and elevated circulating hgf ( chgf ) has been associated with poor survival and worse stage in a variety of cancers.29 , 31 - 33 here , we present a retrospective exploratory analysis characterizing brafv600 mutant ctdna and chgf . 
although the use of these biomarkers has been studied before , this is , to our knowledge , the largest study of this kind using patients from a single randomized clinical trial comparing a braf inhibitor with a chemotherapy control . 
this test has been reported to also detect the v600k and v600d mutations . a total of 675 patients were randomly assigned to the chemotherapeutic drug dacarbazine ( 1 , 000 mg / m2 of body surface area by intravenous infusion every 3 weeks ; n = 338 ) or the braf inhibitor vemurafenib ( 960 mg twice daily orally ; n = 337 )  . 
samples from 605 patients ( 1 , 164 samples ) were available for ctdna analysis , and samples from 563 patients ( 665 samples ) were available for chgf analysis . investigations were performed after approval by a local human investigations committee and in accordance with an assurance filed with and approved by the department of health and human services , where appropriate . 
data were anonymized to protect the identities of research participants . ctdna assessment cell - free dna ( cfdna ) was extracted from 500 l of plasma using the qiaamp circulating nucleic acid kit ( 55114 ; qiagen , hilden , germany ) and eluted in 50 l of supplied buffer . 
all ctdna counts in this study are presented as a fraction of v600 mutant ctdna to wildtype v600 cfdna . hgf assessment chgf levels were measured by enzyme - linked immunosorbent assay as previously described.35 lower limit of quantification was determined to be 210 pg / ml using serial dilution experiments with recombinant human hgf . gene expression analysis gene expression was analyzed using 200 ng of total rna using the nanostring ncounter gene expression assay ( nanostring technologies , seattle , wa ) following manufacturers instructions . 
for data normalization , raw counts were log transformed and standardized to the geometric mean of each sample . statistical analysis kaplan - meier analysis was used to estimate overall survival ( os ) , postprogression survival , and median survival . 
the relationship between ctdna fractions , chgf , ldh , eastern cooperative oncology group ( ecog ) status , stage , treatment , sum of longest diameters , total metastases , and time point was assessed using student t test and tukey honest significant difference test . 
partitioning analysis was performed using jmp genomics ( version 8.0 ; sas institute )  . results circulating biomarkers and patient survival to determine whether baseline brafv600 mutant ctdna could be a prognostic factor in the metastatic melanoma , droplet digital polymerase chain reaction was initially used to evaluate brafv600 mutant ctdna levels in patients in the two treatment arms in the brim - 3 clinical trial ( fig 1 ; appendix table a1 )  . 
 shorter os was observed in vemurafenib - treated patients with detectable baseline levels of v600 mutant ctdna fraction compared with patients having undetectable levels of ctdna ( fig 2a )  . 
 furthermore , when patients with detectable levels of baseline ctdna were categorized into high and low subgroups , patients with high baseline ctdna had significantly shorter os than did those with low baseline ctdna ( fig 2b )  . 
notably , high levels of v600 mutant ctdna fraction were also a poor prognostic factor among dacarbazine treated patients . with the goal of using a combined biomarker approach to assess patient risk , we also measured baseline chgf levels of brim - 3 patients . 
in both vemurafeniband dacarbazine treated patients , high levels of baseline chgf were associated with significantly shorter os ( fig 2c )  . no statistical interaction was observed between baseline chgf and the treatment arm , nor did we observe interaction between baseline brafv600 mutant ctdna and the treatment arm , suggesting that these two biomarkers are not predictive in this setting . 
together , these results suggest that high levels of baseline ctdna and chgf are poor prognostic factors in patients with metastatic melanoma , regardless of treatment . longitudinal tumor monitoring using circulating biomarkers in addition to baseline measurements , we also assessed the utility of circulating biomarkers for longitudinal monitoring . 
 randomly assigned ( n = 675 ) allocation allocated to vemurafenib received allocated intervention ( n = 337 ) ( n = 335 ) analysis allocated to dacarbazine received allocated intervention ( n = 338 ) ( n = 289 ) ctdna analysis analyzed patients baseline samples c2d1 samples pd samples excluded from analysis samples unavailable all samples available failed ddpcr ( n = 324 ) ( n = 293 ) ( n = 282 ) ( n = 71 ) ( n = 11 ) ( n = 8 ) ( n = 3 ) chgf analysis analyzed patients baseline samples pd samples excluded from analysis samples unavailable all samples available failed chgf elisa ( n = 308 ) ( n = 302 ) ( n = 72 ) ( n = 27 ) ( n = 16 ) ( n = 11 ) ctdna analysis analyzed patients baseline samples c2d1 samples pd samples excluded from analysis samples unavailable all samples available failed ddpcr ( n = 281 ) ( n = 258 ) ( n = 219 ) ( n = 41 ) ( n = 8 ) ( n = 1 ) ( n = 7 ) chgf analysis analyzed patients baseline samples pd samples excluded from analysis samples unavailable all samples available failed chgf elisa ( n = 255 ) ( n = 249 ) ( n = 42 ) ( n = 34 ) ( n = 14 ) ( n = 20 ) fig 1 . 
 c2d1 , cycle 2 day 1 ; chgf , circulating hepatocyte growth factor ; ctdna , circulating tumor dna ; ddpcr , droplet digital polymerase chain reaction ; elisa , enzyme - linked immunosorbent assay ; pd , progressive disease . 
 patients longitudinally have demonstrated a reduction in patient ctdna levels after drug treatment and an increase at disease progression , changes thought to be reflective of the tumor burden in patients responsive and refractory to treatment.10 , 16 - 24 although our study only analyzed three time points as opposed to the more frequent monitoring performed by others , a significant reduction of mutant ctdna while receiving treatment at c2d1 followed by a significant increase in ctdna at disease progression was observed in patients in both treatment arms ( appendix fig a1b )  . we did not observe correlations between ctdna levels at c2d1 and survival , nor did we observe that decreases in ctdna levels between baseline and c2d1 correlated with survival or response ( data not shown )  . 
to our knowledge , this is the first study demonstrating that ctdna measured at progression can predict postprogression survival in patients with melanoma . approximately half of patients ( 62 of 112 ) with samples at disease progression had corresponding baseline samples with detectable ctdna . 
 among the vemurafenib - treated patients , those with a greater than two - fold decrease of brafv600 ctdna fraction between the baseline and progression time point experienced significantly longer postprogression survival than did those who experienced either no change or a greater than two - fold increase ( fig 3b )  . 
a similar correlation was not observed for chgf collected at disease progression , nor did we find that change in chgf between baseline and progression correlated with survival or response . circulating hgf and met signaling met - dependent signaling is associated with proliferation , metastasis , and activation of signaling pathways , including the pi3k pathway and the mapk pathway ; all processes that could contribute to a worse prognosis.36 to establish whether elevated chgf detected in patients contributes to met receptor activation , parallel experiments were performed analyzing met tumor rna . 
 a vemurafenib - treated patients dacarbazine - treated patients baseline v600 mutant ctdna detectable , n = 188 , 11.4 mo undetectable , n = 105 , 21.4 mo baseline v600 mutant ctdna detectable , n = 172 , 7.9 mo undetectable , n = 86 , 21 mo time ( months ) no . 
median survival of patients is displayed in the legend . groups , including high chgf / high met , high chgf / low met , low chgf / high met , and low chgf / low met . 
in contrast , patients with low chgf / low met performed the best , with os median values of 14.5 months ( vemurafenib ) versus 17.2 months ( dacarbazine )  . 
patients with high levels of baseline plasma circulating hepatocyte growth factor ( chgf ) and high tumor met expression have significantly shorter overall survival ( os ) than patients in other categories in both treatment arms . 
all covariables modeled , with the exception of stage , were significant independent predictors for os , indicating that the biomarkers included in this analysis are capable of contributing independently valuable insight regarding patient prognosis ( table 2 )  . a combined biomarker approach to assessing risk in patients with melanoma next , we assessed combining these prognostic biomarkers in a stepwise approach to evaluate patient risk . 
incorporating both baseline ctdna and baseline chgf biomarker data generated in this study with prognostic factors ldh level , ecog performance status , and stage , we defined four risk groups for vemurafenib - treated patients using partitioning analysis ( fig 5a )  . 
unpaired two - tailed t test was used to determine significance between groups . abbreviations : ctdna , circulating tumor dna ; ecog , eastern cooperative oncology group ; ldh , lactate dehydrogenase . was the first decisive factor , splitting the population into patients with a baseline brafv600 mutant ctdna fraction greater than and less than 0.039. 
this created four nodes : group 1 ( ctdna fraction < 0.039 , ecog status = 0 ) , group 2 ( ctdna fraction < 0.039 , ecog status = 1 ) , group 3 ( ctdna fraction > 0.039 , chgf < 438 pg / ml ) , and group 4 ( ctdna fraction > 0.039 , chgf > 438 pg / ml )  . patients with high levels of ctdna and chgf in group 4 had significantly shorter os than patients in any other group , with a median survival of 7.3 months ( fig 5b )  . 
although braf plus mek inhibitor combinations have been approved , single - agent braf inhibition is still widely used ; the brim - 3 study design allowed us to analyze a uniquely large patient cohort and characterize our biomarkers of interest for predictive or prognostic potential . 
here , we show that both brafv600 mutant ctdna and chgf are independent prognostic factors for patients with brafv600 mutant metastatic melanoma . recent publications analyzing ctdna in patients with metastatic melanoma have detected baseline mutant ctdna in approximately 70% to 80% of patients with mutation - positive tumors.14 , 15 , 17 , 18 this study detected mutant ctdna at baseline table 2 . 
 b 288 patients median os : 14.2 months v600 mutant ctdna fraction < 0.039 v600 mutant ctdna fraction > 0.039 156 patients median os : 20.0 months 132 patients median os : 10.0 months ecog status ecog status baseline chgf < 438 pg / ml baseline chgf > 438 pg / ml 123 patients median os : 22.0 months 33 patients median os : 12.3 months 68 patients median os : 11.5 months 64 patients median os : 7.3 months group 1 group 2 group 3 group 4 group 1 , n = 123 group 2 , n = 33 group 3 , n = 68 group 4 , n = 64 no . 
vemurafenib treated patients with elevated levels of baseline v600 circulating tumor dna ( ctdna ) and elevated levels of baseline circulating hepatocyte growth factor ( chgf ) are a high - risk patient group . 
 ( a ) decision tree for risk stratification : vemurafenib treated patients with eastern cooperative oncology group ( ecog ) performance status , baseline v600 ctdna , and baseline chgf data were stratified into four risk groups using recursive partitioning analysis . 
these findings , along with others , suggest that the differences in ctdna seem to primarily reflect tumor burden rather than the fraction of brafv600 mutant tumor cells within the tumor . we hypothesized that chgf could serve as a marker of resistance to vemurafenib . 
hgf can signal to met to reactivate the mapk pathway ; therefore , high levels of hgf may act as a potential resistance mechanism in patients treated with braf inhibitors.29 , 30 although there have been two studies evaluating the use of chgf as a biomarker for metastatic melanoma , 43 , 44 to our knowledge , this study is the first to evaluate the use of chgf as a biomarker in patients treated with a braf inhibitor in comparison with patients in a chemotherapy treatment group . 
this result suggests that although chgf may play a role in vemurafenib resistance , it likely also contributes to more aggressive disease , even in the absence of mapk pathway inhibition . it has been reported that hgf originating from stromal cells in the tumor microenvironment could contribute to mapk and pi3k - akt pathway activation.30 our findings from this study focused on circulating hgf , and the origin of the growth factor remains unclear . 
 findings do suggest that the hgf relevant to patient survival may be secreted from outside of the tumor microenvironment . a single biomarker can reveal one aspect of disease and can help in assessing patient risk , but the integration of multiple biomarkers is likely to provide greater insight . 
using partitioning analysis , we were able to categorize patients into four risk groups , with the highest risk group consisting of patients with high brafv600 mutant ctdna and high chgf . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . william lu employment : genentech / roche research funding : genentech / roche luciana burton employment : genentech / roche james larkin honoraria : eisai , bristol - myers squibb , msd , glaxosmithkline , kyocera , pfizer , novartis , roche / genentech , secarna , pierre fabre , eusa pharma consulting or advisory role : eisai , bristol - myers squibb , msd , glaxosmithkline , kyocera , pfizer , novartis , roche / genentech , secarna , pierre fabre , eusa pharma research funding : pfizer ( inst ) , novartis ( inst ) travel , accommodations , expenses : bristol - myers squibb , pfizer , novartis , roche / genentech paul b . 
chapman honoraria : bristol - myers squibb , glaxosmithkline , genentech / roche , provectus , momenta pharmaceuticals , daiichi sankyo consulting or advisory role : bristol - myers squibb , glaxosmithkline , genentech / roche , daiichi sankyo , provectus , momenta pharmaceuticals research funding : glaxosmithkline , genentech / roche , bristol - myers squibb , pfizer travel , accommodations , expenses : bristol - myers squibb paolo a . 
sosman honoraria : amgen , merck , array biopharma , bristolmyers squibb , amgen , merck , array biopharma , bristolmyers squibb ivor caro employment : genentech / roche stock or other ownership : roche grant a . 
mcarthur research funding : celgene ( inst ) , genentech / roche ( inst ) , bristol - myers squibb ( inst ) , amgen ( inst ) , array biopharma ( inst ) , novartis / pfizer ( inst ) ilsung chang employment : genentech / roche stock and other ownership : roche / genentech honoraria : roche / genentech consulting or advisory role : roche / genentech elicia penuel employment : genentech / roche stock and other ownership : genentech / roche yibing yan employment : roche / genentech stock and other ownership : roche / genentech patents , royalties , other intellectual property : roche / genentech matthew j . 
wongchenko employment : genentech / roche travel , accommodations , expenses : roche / genentech stock and other ownership : genentech / roche other relationship : roche / genentech stock and other ownership : ariad affiliations william lu , luciana burton , ilsung chang , ivor caro , elicia penuel , yibing yan , and matthew j . 
wongchenko , genentech , south san francisco ; antoni ribas , the jonsson comprehensive cancer center at university of california , los angeles , ca ; james larkin , the royal marsden nhs foundation trust , london , united kingdom ; paul b . 
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santiago - walker a , gagnon r , mazumdar j , et al : correlation of braf mutation status in circulating - free dna and tumor and association with clinical outcome across four brafi and meki clinical trials . 
schreuer m , meersseman g , van den herrewegen s , et al : quantitative assessment of braf v600 mutant circulating cell - free tumor dna as a tool for therapeutic monitoring in metastatic melanoma patients treated with braf / mek inhibitors . 
xi l , pham tht , payabyab ec , et al : circulating tumor dna as an early indicator of response to t - cell transfer immunotherapy in metastatic melanoma . 
chang ga , tadepalli js , shao y , et al : sensitivity of plasma brafmutant and nrasmutant cell - free dna assays to detect metastatic melanoma in patients with low recist scores and non - recist disease progression . 
janku f , huang hj , claes b , et al : braf mutation testing in cell - free dna from the plasma of patients with advanced cancers using a rapid , automated molecular diagnostics systemol cancer ther 15 : 1397 - 1404 , 2016 20 . 
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gonzalez - cao m , mayo - de - las - casas c , molina - vila ma , et al : braf mutation analysis in circulating free tumor dna of melanoma patients treated with braf inhibitors . 
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mcarthur ga , chapman pb , robert c , et al : safety and efficacy of vemurafenib in braf ( v600e ) and braf ( v600k ) mutation - positive melanoma ( brim - 3 ) : extended follow - up of a phase 3 , randomised , open - label study . 
busam kj , hedvat c , pulitzer m , et al : immunohistochemical analysis of braf ( v600e ) expression of primary and metastatic melanoma and comparison with mutation status and melanocyte differentiation antigens of metastatic lesions . 
 ( a ) baseline v600 mutant ctdna fraction and baseline chgf levels were not significantly different between patients from either treatment ardata points measured below the lower limit of quantitation are shown in the gray shaded region . 
 ( b ) v600 mutant ctdna fraction decreased post - treatment at cycle 2 day 1 ( c2d1 ) but returned to elevated levels at progression in patients in both treatment arms . 
 ( a ) larger tumor burden as determined by the sum of the longest diameters of target lesions correlated with higher levels of baseline v600 mutant ctdna fraction as well as high levels of baseline chgf . 
 tukey honest significant difference ( hsd ) test was used to determine significance between patients categorized by ctdna , and unpaired two - tailed t test was used for patients categorized by chgf . 
brim - 3 patient characteristics overview vemurafenib treated ( n = 337 ) dacarbazine treated ( n = 338 ) 56 ( 21 - 86 ) 52.5 ( 17 - 86 ) characteristic age , years ( range ) median sex , no . 
 use of low - frequency driver mutations detected by cell - free circulating tumor dna to guide targeted therapy in nonsmall - cell lung cancer : a multicenter case series purpose to evaluate the clinical outcome of patients with nonsmall - cell lung cancer treated by targeting low variant allelic frequency ( vaf ) driver mutations identified through cell - free dna ( cfdna ) next - generation sequencing ( ngs )  . 
detection of driver mutations in cancer is critically important in the age of targeted therapy , where both tumor - based as well as cfdna sequencing methods have been used for therapeutic decision making . 
we hypothesized that vaf should not be predictive of response and that low vaf alterations detected by cfdna ngs can respond to targeted therapy . patients and methods a multicenter retrospective case review was performed to identify patients with nonsmall - cell lung cancer who received targeted molecular therapy on the basis of findings of low vaf alterations in cfdna ngs . 
mutations at low vaf were defined as < 0.2% mutated cfdna molecules in a background of wild - type cfdna . results one hundred seventy - two patients underwent cfdna ngs testing . 
2018 by american society of clinical oncology introduction advances in the sensitivity and accuracy of plasma cell - free dna ( cfdna ) sequencing now allow for somatic genomic tumor alterations to be detected by cfdna next - generation sequencing ( ngs ) at the level of 0.02% variant allelic frequency ( vaf ) .1 this raises the question of whether targetable driver mutations that are detected at low frequencies , defined herein as < 0.2% vaf , retain importance even in the setting of other genomic alterations at higher vaf . 
 specific cases spanning each of the three major types of mutationssingle nucleotide variants ( snvs ) , insertion - deletion mutations ( indels ) , and fusionsare discussed . approximately 20% to 30% of tumors from patients with lung adenocarcinoma have targetable miriam t . 
 oncogenic driver mutations in alk , braf , egfr , erbb2 ( her2 ) , met , ret , and ros1.2 , 3 lung cancer patients with nonsmall - cell ( nsclc ) treated with targeted molecular therapies against these oncogenic driver mutations have been found to have prolonged survival compared4 , 5 with patients treated with standard chemotherapy , with improved treatment - related toxicity and quality of life.6 - 8 given these results , the national comprehensive cancer network now recommends that patients with metastatic nonsquamous nsclc have broad molecular profiling of their tumor performed , with cfdna as a secondary option if repeat tissue biopsy is not feasible.9 as tumor cells become necrotic and undergo apoptosis , they release circulating fragments of dna . 
with advances in ngs , it is now possible to detect cfdna from blood samples with significant accuracy and precision.10 , 11 three major approaches exist for analyzing cfdna in peripheral blood . 
the first uses probes to capture hotspots , or regions commonly mutated in selected genes ; an example of this approach is digital droplet polymerase chain reaction.12 the second uses ngs but requires a tumor tissue sample to identify specific mutations , which are used as a reference to select probes to specific regions in cfdna.13 , 14 the third method uses ngs but targets a gene panel of interest using complete exon sequencing in a blinded approach.15 , 16 mutations are quantified and represented as a vaf calculated as the total number of molecules with a given mutation divided by the total number of mutant plus wild - type molecules . detection of cfdna allows for tumor monitoring at disease progression via serial peripheral blood samples and , in the future , may eliminate the need for tumor biopsies or repetitive biopsies in patients with advanced cancer when the initial biopsy is inadequate , unobtainable for genomic testing , or uninformative , or when the patients cancer has progressed despite treatment.17 - 19 the quantity of cfdna has been shown to correlate with tumor staging and prognosis.17 , 20 limitations of cfdna include testing in patients with low disease burden and in patients with bone or brain metastasis , who may have quantities of cfdna below the limit of detection ( lod ) for currently available assays . 
although these false - negative results limit the application of cfdna ngs to a rule - in test , more than a dozen nsclc studies have shown that targetable genomic alterations detected in plasma predict response similarly to those detected in tissue.21 - 24 however , it is unclear whether variants at low allele fractions are as responsive to targeted therapy as those at high allele fractions . 
 samples were sent to a clinical laboratory improvement amendments ( clia ) certified , college of american pathologistsaccredited , new york state department of healthapproved clinical laboratory ( guardant health , redwood city , ca ) for clinical cfdna ngs testing ( guardant360 ) from one of three institutions ( university of california , san diego [ ucsd ] , duke university , or northwestern university )  . 
for this project , a vaf 0.2% was defined as low vaf because this is the 25th percentile vaf detected on guardant360 ( the median or 50th percentile is 0.39% ) in > 5 , 000 patient samples.1 medical records were reviewed in accordance with the respective institutional review board guidelines of ucsd , duke university , and northwestern university . 
response evaluation criteria in solid tumors ( recist v1.1 ) were used to assess response to treatment . tissue ngs individuals had tumor tissue from primary or metastatic sites sent for targeted tumor tissue ngs before or at approximately the same time as their cfdna analysis . 
tissue - based ngs was done at either ucsd , duke , foundation medicine ( foundation one ; cambridge , ma ) , or caris ( phoenix , az )  . 
the lower lod for this assay was 5% , meaning that a mutant allele can be detected in a 95% wild - type allele background ( or 10% neoplastic cell content )  . 
coverage of at least 250 was required to detect a mutation at the 5% lod . egfr sequencing , ros1 and alk fluorescent in situ hybridization testing neogenomics laboratories ( fort meyers , fl ) performed egfr sequencing , which included bidirectional sequencing of exons 18 to 21 of the egfr gene for detection of egfr - activating mutations and tyrosine kinase inhibitor resistance mutations ( including t790m )  . 
tumor enrichment was performed before extraction ( detailed information can be found on the neogenomics web site ) .29 ros1 and eml4 - alk fluorescent in situ hybridization ( fish ) testing was performed by response genetics ( los angeles , ca ) , and a positive test on fish was considered to be > 15% probe binding . plasma cell - free circulating dna analysis the cfdna ngs analysis was performed at guardant health ( guardant360 )  . 
the exons of up to 73 cancer genes were captured using biotinylated custom bait oligonucleotides ( agilent , la jolla , ca ) , resulting in a 148 , 000 base pair ( 78 kb ) capture footprint . 
these algorithms quantify the absolute number of unique dna fragments at a given nucleotide position , thereby enabling circulating tumor dna to be quantitatively measured as a fraction of total cfdna . 
because patients were not enrolled in a prospective clinical trial , assessments were not standardized across the cohort . results between september 2015 and september 2017 , six clinicians from the three institutions ( ucsd , duke university , and northwestern university ) identified 192 orders from 172 unique patients with a diagnosis of nsclc and in whom cfdna was detected . 
although pfs was roughly as expected in this small cohort , the median os of < 15 months is somewhat shorter than expected for egfrand alk positive patients , especially because the median pfs of patients receiving targeted therapies was 12 months . 
this finding of lower than expected os may be because of sample size , or it is possible that patients with driver mutations present at low vaf have a worse prognosis compared with patients with driver mutations at more standard frequencies . 
there may also be other negative prognostic factors associated with low vaf that are not yet known . met exon 14 skipping mutations represent a clinically unique molecular subtype of nsclc and are found in approximately 3% of all nsclc cases.32 met exon 14 mutations can be detected via tumor ngs or with cfdna ngs , which represents a novel detection method because currently , no other alternative detection modalities ( eg , immunohistochemistry or fish ) exist for this mutation . 
thus the met exon 14 skipping mutation can lead to increased activation of c - met , resulting in oncogenic driver mutation potential.33 fusions and midsize indels ( > 50 bp ; eg , met exon 14 skipping variants ) are especially challenging to detect in cfdna . 
as illustrated by case 8 , detection of met exon 14 skipping mutations can significantly affect the use of existing agents ( eg , crizotinib ) or novel agents ( eg , glesatinib ) for treatment . it is now known that intratumoral heterogeneity is associated with an increased risk of recurrence or death . 
 possible , all targetable driver mutations , both early in treatment and as the tumor evolves.34 using interval liquid biopsies on the basis of radiographic progression of an otherwise nonbiopsiable lesion can provide early detection of drug resistance and thus lead to early treatment intervention . 
this was illustrated by patient 5 , who declined invasive tumor biopsy and underwent repeat cfdna testing at the time of radiologic progression , which was 16 months after his initial cfdna testing . 
 a modest - sized prospective clinical trial by kim et al21 used cfdna - guided matched therapy when tissue was insufficient or unobtainable for ngs in patients with metastatic gastric cancer , nsclc , or melanoma . 
additional prospective studies are needed to further examine the value of early detection of resistance mechanisms before clinical evidence of progression and to determine if early detection and intervention truly influences os and pfs . in this series , patients were selected on the basis of the presence of low vaf driver mutations detected in cfdna . 
it has been reported that a subgroup of patients does not release tumor cfdna into their circulation , whereas other patients convert from having circulating tumor cfdna to noncirculating tumor cfdna after treatment , for reasons that include low tumor burden , slow - growing or inactive tumor growth , or therapeutic response.35 if safe , a tissue biopsy should be performed in patients who initially had detectable mutations on cfdna who no longer have detectable mutations but have clear progression of disease . 
there are several ongoing large prospective trials , including the azd9291 first time in patients ascending dose study ( aura ) , which serially compared cfdna versus tumor ngs over time in patients with egfr t790m mutations who were receiving osimertinib , which may help to address these clinical scenarios.16 one patient ( patient 10 ) was noted to have both eml4 - alk and ros1 mutations detected on tissue fish testing at the time of diagnosis . 
 difficulty detecting the mutation because recurrence of disease was located in the brain or the possibility that ros1 was present below the lod for the cfdna assay after 1 year of treatment . 
the patient was transitioned to hospice shortly after cfdna testing was done , and no additional testing was performed to confirm the presence of ros1 rearrangement . to our knowledge , this is the first case series examining treatment outcomes for patients with nsclc with low vaf driver mutations detected by cfdna . 
most patients had other passenger mutations that were present at a higher proportion compared with the low - frequency driver mutation , and the therapeutic significance of relatively low vaf driver mutations has not been previously reported . 
patel manuscript writing : all authors final approval of manuscript : all authors in the sensitivity and specificity of liquid biopsy , the ability to detect and confer clinical benefit to patients on the basis of these results will continue to improve with technological advances in cfdna . 
from this small case series , it seems that even at low vaf , targetable driver mutations retain clinical importance , even in the setting of other genomic alterations at higher vaf . 
mohindra consulting or advisory role : astrazeneca , genentech travel , accommodations , expenses : astrazeneca stock and other ownership interests : pfizer ( i ) lindsey shantzer no relationship to disclose ingrid l . 
patel consulting or advisory role : ariad , abbvie , astrazeneca jeffrey clarke consulting or advisory role : inivata , premier speakers bureau : guardant health , merck stock and other ownership interests : guardant health , biolase research funding : guardant health research funding : medpacto , genentech , bristol - myers squibb , adaptimmune , spectrum pharmaceuticals , abbvie , moderna therapeutics james christensen employment : mirati therapeutics stock and other ownership interests : mirati therapeutics , bluebird bio patents , royalties , other intellectual property : multiple patents in last 2 years while employed at mirati therapeutics covering discovery of kras , lsd1 , and ezh2 inhibitors . 
patel consulting or advisory role : eli lilly , novartis , bristolmyers squibb , astrazeneca / medimmune speakers bureau : merck , boehringer ingelheim research funding : bristol - myers squibb ( inst ) , eli lilly ( inst ) , incyte ( inst ) , medimmune ( inst ) , pfizer ( inst ) , genentech ( inst ) , xcovery ( inst ) affiliations miriam t . 
patel , university of chicago school of medicine , chicago , il ; lindsey shantzer and jeffrey clarke , duke university medical center , durham , nc ; ingrid l . 
lanman , guardant health , redwood city ; and james christensen , mirati therapeutics , san diego , ca . references 77 : 5705 , 2017 ( suppl 13 : abstr ) 1 . 
paik pk , varghese am , sima cs , et al : response to erlotinib in patients with egfr mutant advanced non - small cell lung cancers with a squamous or squamous - like component . 
aisner dl , sholl lm , berry ld , et al : the impact of smoking and tp53 mutations in lung adenocarcinoma patients with targetable mutationsthe lung cancer mutation consortium ( lcmc2 )  . 
zhou c , wu yl , chen g , et al : erlotinib versus chemotherapy as first - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
sequist lv , yang jc , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
oxnard gr , paweletz cp , kuang y , et al : noninvasive detection of response and resistance in egfr - mutant lung cancer using quantitative next - generation genotyping of cell - free plasma dna . 
valle a , audigier - valette c , herbreteau g , et al : rapid clearance of circulating tumor dna during treatment with azd9291 of a lung cancer patient presenting the resistance egfr t790m mutation . 
kim st , banks kc , lee s - h , et al : prospective feasibility study for using cell - free circulating tumor dnaguided therapy in refractory metastatic solid cancers : an interim analysis . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
rozenblum ab , ilouze m , dudnik e , et al : clinical impact of hybrid capture - based next - generation sequencing on changes in treatment decisions in lung cancer . 
camidge dr , bang yj , kwak el , et al : activity and safety of crizotinib in patients with alk - positive non - small - cell lung cancer : updated results from a phase 1 study . 
awad mm , oxnard gr , jackman dm , et al : met exon 14 mutations in non - small - cell lung cancer are associated with advanced age and stage - dependent met genomic amplification and c - met overexpression . 
peschard p , fournier tm , lamorte l , et al : mutation of the c - cbl tkb domain binding site on the met receptor tyrosine kinase converts it into a transforming protemol cell 8 : 995 - 1004 , 2001 34 . 
lin c - c , shih jy , yu cj , et al : outcomes in patients with non - small - cell lung cancer and acquired thr790met mutation treated with osimertinib : a genomic study . 
 smart cancer navigator : a framework for implementing asco workshop recommendations to enable precision cancer medicine purpose data standards and interoperability are critical for improving care for patients with cancer . 
to facilitate improved patient care , several recommendations for data sharing and standardization were made to the community . methods to address these recommendations , we developed smart cancer navigator , a web application that uses application programming interfaces to gather clinical and genomic data from 11 public knowledge bases ranging from basic to clinical content coverage ; three ( civic , clinvar , and oncokb ) explicitly linked genomic variants to clinical factors such as prognosis and treatment selection . 
we illustrated the utility of this application by selecting one of the monthly case studies presented by the asco university molecular oncology tumor board : ovarian cancer ( brca mutation )  . 
 results smart cancer navigator aggregates and contextualizes data from 11 different knowledge bases and stores user queries in a lightweight web application that can link into fast healthcare interoperability resourcesenabled electronic health records . 
a comparison of the three clinico - genomic knowledge bases indicated substantial differences in coverage at the gene and variant levels . conclusion smart cancer navigator has immediate relevance to practicing oncologists and others . 
2018 by american society of clinical oncology introduction precision medicine is a model for disease prevention and treatment that considers variability in genes , environment , and lifestyle across individuals.1 to expand and broaden this model , the federal government invested $215 million in establishing the precision medicine initiative in 2015 , with a large portion of the funding devoted to precision oncology.2 , 3 advances in molecular profiling to identify actionable genetic aberrations provided a compelling rationale for this initial emphasis.4 - 6 in may 2016 , asco convened a data standards and interoperability summit to address the critical data sharing and standardization issues that could impede the realization of precision oncology . in typical genomic workflows , oncologists request genomic analysis of a recurrent or metastatic tumor , and genomics laboratories return variably structured narrative reports of the genes and variants they identified , which are often scanned into the patients electronic health record ( ehr )  . 
 some reports are more than 20 pages long , including characterization of genetic variants , potential targeted therapies , and relevant clinical trial information , whereas others may be brief and may lack any interpretation . 
facing a lack of clear actionability ( ie , translation of genomic findings into treatment recommendations ) , potential bias in report curation , and potentially outdated information , oncologists often have to access additional knowledge bases to obtain more comprehensive , up - to - date disease - gene - variant information . 
inconsistencies among knowledge bases ( eg , differences in querying syntax and graphical user interfaces ) lead to inconvenience and inefficiency ; furthermore , oncologists must re - enter patient data every time they need to update their queries . because of these issues , attendees at the 2016 asco omics and precision oncology ( opo ) workshop called for the development of new software applications to help community oncologists interpret the ever - increasing volumes of genomic data critical for selecting treatment.7 here we describe smart cancer navigator , a software application ( app ) we developed to facilitate knowledge base queries and identify actionable information for practicing oncologists . 
the purpose of this article is to describe the development of and demonstrate the utility of the smart cancer navigator and to disseminate it to the oncology community for implementation and feedback . methods app overview smart cancer navigator securely links patient - specific data from ehr and genomics laboratories to multiple independent knowledge bases to facilitate efficient and effective querying of disease - gene - variant information . 
the web - based app was built by a team of software developers at the biomedical cybernetics laboratory at the boston childrens hospital computational health informatics program and harvard medical school who used an angular and bootstrap front - end framework . 
the app , prepopulated with relevant information from genomic laboratories and ehrs , provides an interface that oncologists can use to query evidence from several cancer - focused , genomic , clinico - genomic , and clinical trials knowledge bases . 
through built - in feedback functionality , meaningful responses regarding the usability and efficacy of the app can be collected for continuing improvement . smart cancer navigator is a modular app built by using substitutable medical apps reusable technology ( smart ) on fast healthcare interoperability resources ( fhir ) technology . 
 the smart on fhir platform was chosen to ensure interoperability with as many ehr systems as possible.8 - 10 smart on fhir facilitates the development of apps that can connect to health data systems ( eg , ehrs , personally controlled health records , health information exchanges ) without any custom configuration.8 , 11 , 12 through the development of application programming interfaces ( apis [ apps ] ) developed on the smart platform are substitutable : just as applications on a mobile technology platform such as apples operating system ( ios ) are separated from the core system and services ( eg , camera , geolocation ) , apps on the smart platform are separated from health data systems ( the equivalent of the core system and services on ios )  . login and authentication smart cancer navigator can be linked to a patients api - enabled ehr . 
because smart on fhir - enabled ehrs provides an oauth2based approach for secure login and authentication , the user can login and authorize the app for data access once the user has been authenticated with the ehr ( ie , has provided a username and password linked to appropriate credentials ) .9 once successfully authenticated and authorized , the app can be populated with relevant patient and practitioner information stored in the local environment . nomenclature , drop - down menus , data entry , and queries after logging in and optionally linking to a patients ehr , the user is presented with an interface for querying gene - variant combinations ( fig 1 )  . 
smart cancer navigator uses a hybrid data entry field that allows filtering via text entry followed by selection from a drop - down menu , which ensures efficient and consistent querying of gene - variant combinations . 
name and age are randomly generated ; any resemblance to an actual person is purely coincidental . field , the complementary drop - down list is populated in real time with suggested gene - variant combinations from the linked knowledge bases ( fig 1 )  . 
using this real - time service guarantees access to the latest available gene - variant information . the user begins a query by typing in the search bar , and the apps search algorithm efficiently sifts through thousands of known gene - variant combinations . 
this approach enables users to select gene - variant combinations without having to adhere to formal nomenclature or having to know the latest gene names . for executing queries , the app uses the following standards : genes are represented using hugo gene nomenclature committeeapproved symbols and national center for biotechnology information entrez gene ids , and variants are represented using the human genome variation society ( hgvs ) protein and genomic reference sequences.13 - 16 once the user has selected the appropriate gene variant combination , smart cancer navigator translates the combination into relevant api calls and populates an expandable view containing the results . 
these searches and results can then be saved to the patients ehr . knowledge bases and apis smart cancer navigator accesses 11 knowledge bases : ( 1 ) clinical interpretations of variants in cancer ( civic ) , ( 2 ) clinvar , ( 3 ) catalogue of somatic mutations in cancer ( cosmic ) , ( 4 ) combined annotation dependent depletion ( cadd ) , ( 5 ) database for nonsynonymous snps functional predictions ( dbnsfp ) , ( 6 ) database for single nucleotide polymorphisms ( dbsnp ) , ( 7 ) cancer genome ( 8 ) precision medicine interpreter knowledgebase ( pmkb ) , ( 9 ) oncokb , ( 10 ) drug - gene interaction database ( dgidb ) , and ( 11 ) clinicaltrials.gov.17 - 27 these knowledge bases were selected because at least some or all of their content was freely available through apis in mid to late 2017 . ( cgi ) , variant annotation information from civic is queried via standardized apis that use the hgvs genomic reference sequence id through the myvariant.info restful service28 and via a proprietary api format . 
this field often provides information on prognostic implications , potential drug treatment options , and context on previous or ongoing clinical research on the variant . summary pathways list of pathways associated with the normally functioning gene . functional prediction and characterization a numeric score , rank , boolean operator , or text string describing the characterization of a variant ( eg , benign , gain of function )  . subsection gene , variant gene variant coordinates and details series of fields describing the location of the gene or variant . 
usually includes chromosome number , reference or alternate allele , start and end position , codon position , and reference codon . gene , variant type variant tab : series of fields describing the variant type ( eg , single nucleotide polymorphisms , single nucleotide variation ) and predicted consequence of the mutation ( eg , missense , nonsense )  . 
 gene tab : series of fields describing the gene type ( eg , protein - coding )  . gene , variant aliases and ids series of fields containing aliases and ids ( eg , entrez ) for genes . origin of variant text field or boolean operator that characterizes the variant as somatic , germline , or both . known diseases cancer subtypes that the variant is known to be implicated in . suggested treatment ( effective drugs ) potential drug treatment options . 
drug suggestions are often accompanied with a text field containing the name of the implicated disease , as well as a short description of predictive implications for users of the drug . tumor site and traits a text field containing information regarding the tumor from which the variant was discovered . variant supporting evidence quality of evidence clinical trials pointers to publications , conference proceedings , or other evidence that support assertions , in particular , suggested treatments . subjective or validated scales that rate the quality of supporting evidence , such as the levels of evidence scale used by oncokb . table of values from clinicaltrials.gov api : trials are separated into two tables : variantassociated trials and gene - associated trials . 
each table has the following 5 columns : ( 1 ) clinical trial id , ( 2 ) phase , ( 3 ) therapies , ( 4 ) title of trial , and ( 5 ) recruitment status . clinical trials gene variant variant variant variant variant through 7 are queried with myvariant.info , and knowledge bases 8 through 11 are queried using their own api formats . 
if the knowledge bases fail to return data for a query , the app records a knowledge base gap . displaying results upon selecting a gene - variant combination , the app queries the knowledge bases and then returns results in an expandable view . 
for example , when interacting with the functional prediction ( clinical significance ) field in the variant subsection , users can view evidence from clinvar and relevant accession numbers . because smart cancer navigator compiles information from many different data sources , there may be instances in which sources present conflicting information . 
upon clicking the link , the user can view all interpretations and respective data sources in a tabular format . interface with ehrs and local servers smart cancer navigator follows smart on fhir specifications to connect to ehrs and interpret patient context.9 optionally , users can also manually enter patient data ; by default , only non - protected health information ( phi ) is exposed to the external apis . 
in accordance with smart on fhir specifications , the observation resource is separate from the patient resource , but includes a link to the patient resource id to ensure that this information remains linked . 
during development , the following test systems were used : the healthcare services platform consortium sandbox29 to simulate ehrs and the fhir genomics server30 server to simulate a genomics archive communications system . knowledge base analysis in addition to developing smart cancer navigator , we performed analyses to examine concordance among publicly available knowledge bases . 
briefly , a 62 - year - old woman underwent optimal debulking for advanced - stage hgsoc and remained in complete remission for 3 years after first - line platinum doublet therapy . 
she then relapsed with platinum - sensitive disease and attained a second complete remission ( see data supplement for full case description ; materials used with permission )  . under current national comprehensive cancer network clinical practice guidelines , 34 , 35 this patient with hgsoc should have received genetic counseling , regardless of family history . 
 because testing at diagnosis frequently does not occur , 36 , 37 we present the following hypothetical results from next - generation sequencing panel testing conducted at the time of relapse : ( 1 ) brca1 p.trp1815ter at 50% allele frequency , consistent with a germ line variant ; ( 2 ) brca1 p.cys61gly at 10% allele frequency , consistent with a somatic variant ; and ( 3 ) an etv6 - ntrk3 fusion ( data supplement )  . in the de facto workflow , medical oncologists and tumor board coordinators face significant obstacles when they attempt to corroborate and enrich these genetic testing reports that use multiple knowledge bases.38 for each search , data must be manually entered ; in addition , nonstandardized nomenclature between reports and knowledge bases can lead to inconvenience and the omission of crucial information . 
furthermore , search results are not captured in a format amenable to ehr integration , which may diminish rapid translation.7 , 39 the smart cancer navigator app removes these obstacles . to begin , the oncologist logs in , chooses the appropriate patient from the ehrs , and launches smart cancer navigator , with prepopulated patient data , including name , sex , age , and any previously queried gene - variant combinations . 
a separate query would be made for each gene - variant combination ; smart cancer navigator automatically saves each query , allowing for subsequent re - querying of knowledge bases at a later time without the need for redundant data entry . immediately after entering each query , the user can interact with the results for each gene - variant combination . 
in gene results ( fig 2 ) , the user is presented with relevant summaries and descriptions as well as important details ( gene symbols and ids , gene type , aliases , genomic position , and pathways )  . 
the variant results provide relevant descriptions , evidence items , and details , such as variant type , functional prediction , coordinates , tumor site , knowledge base ids , mutation frequency , and suggested treatments ( data supplement )  . 
a prose description of the gene and its function is provided on the left ; structured information from the knowledge bases is presented in tabular format on the right . site - agnostic trials , including the nci - match basket trial ( nct02465060 : nci - match : targeted therapy directed by genetic testing in treating patients with advanced refractory solid tumors , lymphomas , or multiple myeloma ) , which contains larotrectinib in arm z1e . 
comparing variants present in the two cancer - focused knowledge bases ( civic and oncokb ) , we found only 8.1% ( 432 of 5 , 317 ) unique variants in common ( data supplement )  . using the functional annotation tool database for annotation , visualization and integrated discovery ( david45 ) , we performed gene enrichment analysis on data from civic , clinvar , and oncokb . 
the kyoto encyclopedia of genes and genomes ( kegg46 ) pathways in cancer genes were identified in all three databases , with 4.1% of clinvar genes , 30.8% of civic genes , and 34.1% of oncokb genes associated with kegg pathways ( all p < .001 via davids ease score threshold , 47 a modified fishers exact p value )  . 
 a database analysis : comparison of genes in clinvar , civic , and oncokb database analysis : comparison of genes in clinvar , civic , and oncokb that are involved in kegg pathways in cancer1 6105 civic ( 90 ) clinvar ( 236 ) oncokb ( 93 ) civic ( 328 ) clinvar ( 6 , 425 ) oncokb ( 273 ) 1analysis performed using data available on august 5 , 2017 total = 6 , 548 1analysis performed using data available on august 5 , 2017 total = 393 fig 3 . 
venn diagrams for a comparison of genes in ( a ) clinvar , clinical interpretations of variants in cancer ( civic ) , and oncokb and ( b ) clinvar , civic , and oncokb that are involved in kyoto encyclopedia of genes and genomes ( kegg ) pathways in cancer . 
third , inconsistency in interpretation is addressed by providing multiple interpretations from numerous knowledge bases , with the aim of presenting a more holistic approach on the basis of multiple up - to - date knowledge sources . 
fourth , with simple drop - down interfaces in the search / query view and well - organized structured outputs in the results view , oncologists can readily access disease - gene - variant information without any formal training . 
in addition , smart cancer navigator links genomic information to relevant clinical trials , provided that they have the relevant hgvs protein or genomic reference sequences , thereby addressing another key opo workshop recommendation . analysis of existing knowledge bases revealed fairly disparate coverage at the gene and variant levels . 
 be enriched for germ line variants means that cancer - focused knowledge bases should also have substantial germ line information.52 , 53 whether differences in coverage of the cancer - focused knowledge bases reflect differing priorities versus incomplete curation is unclear ; active efforts such as the variant interpretation for cancer consortium54 are underway to coordinate efforts and maximize interoperability . 
it is expected that more cancer - specific knowledge base content will become available via public apis ; our analysis was limited to civic and oncokb because of their api availability . review of the clinvar clinical significance results , which were enriched with variants of unknown significance , makes apparent the ongoing need for the interpretation and discovery of actionable variants . 
after the recent advances in next generation sequencing technologies , it is clear that there is still much work to be done in studying new variants and providing relevant information regarding actionable variants to oncologists.55 - 57 in addition , differences between proprietary and standardized apis pose an obstacle to directly incorporating data from some knowledge bases . 
 they would need to familiarize themselves with the structure of the apis and would find that different combinations of operations and internal terminologies or ids are often needed to access data across knowledge bases . 
because data granularity , specificity , and nomenclature may differ , and evidence reliability ratings are not readily translatable across knowledge bases , this highlights a need for better representation of genomic data and adoption of uniform standards . 
indeed , there is much work to be done to facilitate data sharing between different organizations ; nevertheless , our application serves to mitigate these gaps in data sharing by linking multiple knowledge bases together through one convenient solution . in its current state , smart cancer navigator is focused on data aggregation , and it presents data in a simple tabular format . 
more sophisticated methods of data visualization are necessary , in particular to highlight the co - occurrence of mutations , which is increasingly clinically relevant.58 we have previously shown that standard visual tools such as the pie chart do not scale when dealing with large numbers of genes and variants.59 to address this challenge , the biovis community recently convened a challenge workshop and will soon be formulating recommendations.60 although smart cancer navigator allows users to select a relevant patient condition and then select a gene - variant doublet , true clinical decision support in oncology requires a triplet of disease - gene - variant information and , in many cases , further metadata such as prior treatments received . 
current knowledge base api architecture does not meet this need , because most provide only end points for the querying of genes and variants or provide end points for other relevant clinical information that may not presently return data . 
the clinical trials example shown in the data supplement illustrates this challenge , because only one of the identified trials is directly relevant to the patient with relapsed hgsoc . it must also be acknowledged that apps such as smart cancer navigator may be seen as a security risk by some organizations . 
although smart on fhir apps have a security structure that meets or exceeds the requirements set forth by the health insurance portability and accountability act , 9 genetic information is nonetheless highly sensitive . 
first , we designed the app to be simple to use , but we are mindful of the fact that clinicians are under intense time pressures that are not expected to abate anytime soon . 
second , we assume that the app ecosystem will evolve rapidly11 , 12 , 62 ; endorsement by large ehr vendors through activities such as epics app orchard63 and cerners participation in the hl7 argonaut project is encouraging . 
however , for the app ecosystem to reach its full potential , apps must be able to write to ehrs or to intermediary systems that subsequently communicate with ehrs , such as genomics archive computer system.10 , 39 , 64 finally , we assume that the regulatory environment for apps , which are considered software as a medical device by the us food and drug administration under certain circumstances , 65 , 66 will remain on the track that has recently been indicated ; expensive regulatory burdens would likely stifle the environment of open - source apps because costs could not be recouped . in light of recent discussions regarding data sharing , 67 we believe that our framework acts as a model for facilitating a symbiotic relationship between clinicians , clinical researchers , and bioinformatics data scientists . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . clinical application , it also holds value as a tool for clinical researchers and knowledge base curators . 
although concerns of policy , privacy , and practicality must still be worked out to ensure that data sharing is efficient , sustainable , and secure , smart cancer navigator illustrates the benefits that are conferred when parties work together to share resources and knowledge . finally , smart cancer navigator seeks to support oncologists in the interpretation of ever increasing volume of patient molecular data.68 - 70 by linking directly to patient ehr systems , genomic laboratories , and multiple authoritative knowledge bases , smart cancer navigator can serve as an educational resource for clinical oncologists , trainees , patients , and researchers . 
 furthermore , smart cancer navigators use of apis , which are mandated by the 21st century cures act , 71 provides for a truly modular application that can be easily integrated into many environments . 
warner stock and other ownership interests : hemonc.org ishaan prasad no relationship to disclose makiah bennett no relationship to disclose monica arniella no relationship to disclose alicia beeghly - fadiel no relationship to disclose kenneth d . 
mandl , and gil alterovitz , boston childrens hospital / harvard medical school , boston ; gil alterovitz , massachusetts institute of technology , cambridge , ma ; and monica arniella , duke university , durham , nc supported in part by grants no . 
hughes ks , ambinder ep , hess gp , et al : identifying health information technology needs of oncologists to facilitate the adoption of genomic medicine : recommendations from the 2016 american society of clinical oncology omics and precision oncology workshop . 
forbes sa , tang g , bindal n , et al : cosmic ( the catalogue of somatic mutations in cancer ) : a resource to investigate acquired mutations in human cancer . 
liu x , wu c , li c , et al : dbnsfp v3.0 : a one - stop database of functional predictions and annotations for human nonsynonymous and splice - site snvs . 
national center for biotechnology information : dbsnp : database of single nucleotide polymorphisms ( snps ) and multiple small - scale variations that include insertions / deletions , microsatellites , and non - polymorphic variants . 
ihnen m , zu eulenburg c , kolarova t , et al : therapeutic potential of the poly ( adp - ribose ) polymerase inhibitor rucaparib for the treatment of sporadic human ovarian cancer . 
mcneish ia , oza am , coleman rl , et al : results of ariel2 : a phase 2 trial to prospectively identify ovarian cancer patients likely to respond to rucaparib using tumor genetic analysis . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
hyman dm , laetsch tw , kummar s , et al : the efficacy of larotrectinib ( loxo - 101 ) , a selective tropomyosin receptor kinase ( trk ) inhibitor , in adult and pediatric trk fusion cancers . 
huang dw , sherman bt , tan q , et al : the david gene functional classification tool : a novel biological module - centric algorithm to functionally analyze large gene lists . 
alexandrov lb , nik - zainal s , wedge dc , et al : signatures of mutational processes in human nat rev genet 14 : 703 - 718 , 2013 cancer . 
ghazani aa , oliver nm , st pierre jp , et al : assigning clinical meaning to somatic and germline whole - exome sequencing data in a prospective cancer precision medicine study . 
blakely cm , watkins tbk , wu w , et al : evolution and clinical impact of co - occurring genetic alterations in advanced - stage egfr - mutant lung cancers . 
 potentially curative targeted therapy for undifferentiated high - grade sarcoma developing after malignant transformation of a braf v600emutated ameloblastic fibroma nikolay zhukov , md , phd1 , 2 ; yulia mareeva , md1 ; dmitry konovalov , md1 ; alexander druy , md , phd1 ; nikolay grachev , md , phd1 ; and dmitry litvinov , md1 introduction ameloblastic broma ( af ) is a rare benign odontogenic tumor , consisting of odontogenic epithelium and mesenchymal tissues . 
most afs can be cured by radical enucleation or wide excision , but some tumors are initially unresectable or become unresectable after relapse because of locally invasive behavior or malignant transformation to ameloblastic brosarcoma ( afs ) .1 , 2 currently , there are no established curative or even effective palliative treatments for unresectable af or its malignant derivates . 
within 2 years of diagnosis , the patient had undergone three consecutive attempts at tumor resection with r2 to r1 margins in local low - volume hospitals , but the disease continued to recur locally . after the third recurrence , the patient was admitted to a high - volume federal oncology center , where a biopsy revealed the malignant transformation of af into afs . the tumor retained its biphasic morphology , but the cytologically benign epithelial component was covered by highly mitotic atypical mesenchymal tissue ( figs 1c and 1d )  . 
because the tumor was borderline resectable , the patient had experienced multiple recurrences , and malignant transformation of the tumor had been conrmed ; aggressive soft tissue sarcoma oriented chemotherapy aimed at tumor shrinkage was administered . 
disease remained stable after second - line therapy with dactinomycin , carboplatin , and etoposide and third - line therapy with irinotecan and cisplatwhy secondand third - line treatments were administered is unclear , but in our opinion , this conrmed tumor chemotherapy resistance at this point . after chemotherapy , the patient underwent a fourth attempt at potentially curative surgery , and r0 resection was achieved . 
after pathologic examination , the tumor still had biphasic afs morphologic features with benign epithelial and malignant mesenchymal components , both with weak signs of chemotherapy - induced pathologic response . nine months later , the tumor recurred , with massive extension into the pterygopalatine and infratemporal fossae , and the patient was admitted to our hospital for the next attempt at radical curative - intent surgery . pathologic examination of the resected tumor , which had retained its afs morphology , revealed r1 margins , which we treated with adjuvant radiotherapy , with target volume dosing of 59.4 gy to the tumor bed . because of the high chance of recurrence and chemotherapy resistance of the tumor , we performed an extensive search for potential drug targets for noncytotoxic therapy and found a braf v600e mutation in the tumor , indicating the tumor could respond to anti - braf / mek therapy . 
primary tumor , an ameloblastic broma ; magnication at ( a ) 40 and ( b ) 200 , showing a benign biphasic tumor with odontogenic epithelial glands and hypocellular mesenchymal component . third relapsed tumor morphology , diagnosed as ameloblastic brosarcoma , magnication at ( c ) 40 and ( d ) 200 , showing benign odontogenic epithelial glands surrounded by atypical mesenchymal tumor with numerous mitotic gures . 
 case report eleven months later , in january 2018 , the tumor recurred again and was unresectable because of its size and the involvement of major vessels and the base of the skull ( fig 2a )  . 
the benign epithelial component we previously observed was lost , and the tumor had aggressive small round cell morphology and was nearly 80% ki - 67 positive . there was no expression of epithelial or hematolymphoid markers and no precise immunophenotype , with cells negative for ck ae1 / ae3 , p63 , gfap , calponin , cd99 , cd45 , desmin , s100 , ck19 , ck18 , ema , and cd34 ini1 , p16 , and fli1 after and positive for vimentin , immunohistochemical staining . 
 ( a ) magnetic resonance imaging ( mri ) of the large soft tissue lesion in the right mandibular , with spreading into the pterygopalatine fossa and parapharyngeal space ; soft tissues of both the buccal region and neck , with involvement of major vessels and base of the skull , shown at right . 
radical curative - intent surgery was performed in september 2018 ( fig 2d ) , and pathologic examination revealed r0 margins and complete pathomorphologic and even complete molecular tumor regression , with no signs of vital tumor and no braf v600e in highly sensitive allele - specic polymerase chain reaction of resected tissue . 
 case report adjuvant vemurafenib and cobimetinib therapy was discontinued in august 2019 , and at the time of this report , the patient , now 16 years of age , has survived for 18 months since the start of targeted therapy and has remained disease free for 11 months since his last surgery . discussion the braf v600e mutation is a valid drug target in some tumors , including melanoma , nonsmall - cell lung cancer , and anaplastic thyroid cancer ; anti - braf / mek therapy has led to high objective response rates and prolonged survival in these tumors.11 - 13 however , this effect is not universal , and in other tumors ( eg , colorectal cancer ) , braf v600e does not predict high efcacy of targeted therapy.14 accordingly , the presence of a braf mutation in af does not automatically imply the high efcacy of anti - braf / mek therapy in these tumors , especially those with complete morphologic transformation , as occurred in our patient . here we demonstrate an intrinsic characteristic of a braf mutation in af and its malignant derivates ; the mutation was retained during all stages of disease transformation . 
there are some reports about the effectiveness of anti - braf or anti - braf / mek therapy for ab and malignant ab , but there are no data on its use for braf - positive af.7 , 8 this report conrms a class effect of braf v600e in odontogenic tumors , irrespective of denitive tumor type . the pattern of transformation is also of interest , because braf mutation in odontogenic tumors is usually associated with the epithelial component , which was completely lost during transformation in our patient.3 the mechanism underlying the transformation from the initially benign tumor to the aggressive sarcoma is unclear , and such a transformation has not been previously observed in this tumor type , to our knowledge ; therefore , we plan to perform wholegenome next - generation sequencing to evaluate genetic markers associated with this transformation . to our knowledge , at the time of submission , this is the rst published report of the stepwise transformation of af to a high - grade usrcs , with complete disappearance of the epithelial component . 
furthermore , again to our knowledge , this is the rst report of a complete pathologic and molecular response of braf v600emutated highgrade usrcs to anti - braf / mek therapy , with the possibility of long - term disease control or even a cure after subsequent radical surgery with adjuvant anti - braf / mek therapy . 
one limitation of this case report is that a longer follow - up period after the cessation of anti - braf / mek therapy is required to distinguish between cure and prolonged control of persistent subclinical residual tumor . in conclusion , the braf v600e mutation is one of the primary oncogenic drivers in odontogenic tumors , even during malignant transformation . 
anti - braf / mek therapy is highly effective in malignant odontogenic tumors with braf v600e and , in combination with subsequent surgery , can be curative in patients with otherwise incurable disease . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . nikolay zhukov honoraria : novartis , teva , biocad , nutricia , takeda , astrazeneca , pzer , bristol - myers squibb , servier consulting or advisory role : pzer research funding : takeda travel , accommodations , expenses : biocad no other potential conicts of interest were reported . acknowledgment we conrm that written informed consent was obtained from the patients legal guardian . 
j oral pathol med 47 : 315 - 325 , 2018 kobayashi k , murakami r , fujii t , et al : malignant transformation of ameloblastic broma to ameloblastic brosarcoma : case report and review of the literature . j craniomaxillofac surg 33 : 352 - 355 , 2005 brown na , rolland d , mchugh jb , et al : activating fgfr2 - ras - braf mutations in ameloblastoma . 
clin cancer res 20 : 5517 - 5526 , 2014 kurppa kj , cat on j , morgan pr , et al : high frequency of braf v600e mutations in ameloblastoma . 
j pathol 232 : 492 - 498 , 2014 sweeney rt , mcclary ac , myers br , et al : identication of recurrent smo and braf mutations in ameloblastomas . 
nat genet 46 : 722 - 725 , 2014 [ erratum : nat genet 47 : 97 , 2015 ] brunner p , bihl m , jundt g , et al : braf p.v600e mutations are not unique to ameloblastoma and are shared by other odontogenic tumors with ameloblastic morphology . 
oral oncol 51 : e77 - e78 , 2015 tan s , pollack jr , kaplan mj , et al : braf inhibitor treatment of primary braf - mutant ameloblastoma with pathologic assessment of response . 
oral surg oral med oral pathol oral radiol 122 : e5 - e7 , 2016 kaye fj , ivey am , drane we , et al : clinical and radiographic response with combined braf - targeted therapy in stage 4 ameloblastoma . 
j natl cancer inst 107 : 378 , 2014 diniz mg , gomes cc , de sousa sf , et al : oncogenic signalling pathways in benign odontogenic cysts and tumours . 
planchard d , smit ef , groen hjm , et al : dabrafenib plus trametinib in patients with previously untreated brafv600e - mutant metastatic non - small - cell lung cancer : an open - label , phase 2 trial . 
de moor author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license corresponding author : andrew n . 
freedman , phd , epidemiology and genomics research program , division of ( continued ) purpose there are no nationally representative data on oncologists use of next - generation sequencing ( ngs ) testing in practice . 
the purpose of this study was to investigate how oncologists in the united states use ngs tests to evaluate patients with cancer and to inform treatment recommendations . methods the study used data from the national survey of precision medicine in cancer treatment , which was mailed to a nationally representative sample of oncologists in 2017 ( n = 1 , 281 ; cooperation rate = 38% )  . 
of these oncologists , 34.0% used them often to guide treatment decisions for patients with advanced refractory disease , 29.1% to determine eligibility for clinical trials , and 17.5% to decide on off - label use of food and drug administrationapproved drugs . 
oncologists younger than 50 years of age , holding a faculty appointment , having genomics training , seeing more than 50 unique patients per month , and having access to a molecular tumor board were more likely to use ngs tests . conclusion in 2017 , most oncologists in the united states were using ngs tests to guide treatment decisions for their patients . 
multimarker panels also include dna and rna analysis through next - generation sequencing ( ngs ) technologies , including custom panels that profile multiple actionable driver genes and tumor characteristics that may guide the selection of targeted therapies . despite advances in precision oncology , comparatively little empirical research is available that assesses the expectations and experiences of oncologists in the united states who may use these genomic tools to care for patients with cancer . 
to date , most studies have evaluated physicians experiences with specific genomic tests for individual gene mutations.3 - 5 studies that have attempted to assess providers experiences with custom ngs tumor panels6 - 9 have focused on intended rather than actual use . 
furthermore , previous studies of physicians use of ngs tests were on the basis of small samples and were conducted in tertiary referral centers ; as a result , their findings may not represent how oncology is practiced in the united states . 
currently , there are no nationally representative data describing oncologists awareness , knowledge , and use of ngs testing to inform patient care , especially in community practice settings . with the increasing application of precision oncology , understanding how oncologists use genomic tests in their practice and the factors that affect their use is essential to ensure that patients who can benefit receive appropriate testing and follow - up . 
the purpose of this study was to investigate how oncologists in the united states use ngs tests to evaluate patients with cancer and inform treatment recommendations . methods data source this study used data from the national survey of precision medicine in cancer treatment , a nationally representative survey of hematologists , hematologists / oncologists , and oncologists sponsored by the national cancer institute ( nci ) , the national human genomic research institute , and the american cancer society . 
 of the remaining 3 , 378 oncologists with verified contact information , 1 , 281 completed the survey ( cooperation rate = 38%10 )  . a survey packet containing a personalized invitation letter from the nci , an endorsement letter from asco , a pen with the studys name printed on it , a self - administered paper questionnaire , and a business reply envelope was mailed to eligible oncologists . 
participants received a $50 honorarium for completing the survey . the questionnaire ( data supplement ) took 20 minutes to complete on average , and data were collected from february through may of 2017 . 
information was ascertained about oncologists demographics , training , academic affiliation , specialty , and patient volume , and their practice characteristics , including practice setting , structure , and resources to support genomic testing . 
 information about oncologists use of commercially available multimarker tumor panels and noncommercial tumor panels performed at academic medical centers was collected , as were data on the clinical scenarios in which ngs test were used . 
because of differences in how survey questions were worded ( eg , some explicitly stated the exclusion of oncotype dx ) , sensitivity analyses were conducted to examine whether oncologists who reported using other gene expression tests , including the breast cancer index , mammaprint , prosigna , and / or myplan lung cancer , differed in their use of ngs tests from those who did not use these gene expression tests . 
the survey weights were applied in all analyses of the data and provide statistical adjustment so that respondents are representative of the population of practicing oncologists in the united states . each oncologist was classified as a user of ngs tests if he or she reported using at least one specific multimarker panel with ngs technologies profiling multiple actionable driver genes for guiding treatment decisions in the past 12 months . 
multivariable models were estimated to examine the independent association between each physician demographic and practice characteristic and the likelihood of ngs testing , when adjusting for the other characteristics in the model . 
all analyses were conducted using sudaan release 11.0.1 ( rti international , research triangle park , nc )  . results characteristics of survey respondents characteristics of the 1 , 281 oncologists who completed the survey are listed in table 1 . 
 more than one half of respondents ( 56.9% ) spent at least 90% of their time in patient care and almost one half ( 49.3% ) spent less than 10% of their time teaching ( data not shown )  . prevalence of ngs test use and predictors of test use to guide treatment decisions overall , 75.6% of oncologists reported using ngs tests in the past 12 months to guide treatment decisions ; use differed according to the physicians demographic and practice characteristics ( table 2 )  . 
oncologists who treated only patients with hematologic malignancies were less likely to use ngs tests than were oncologists who treated both solid and hematologic malignancies and those who only treated patients with solid tumors . 
oncologists who held a faculty appointment , had some training in genomics , or were part of a practice that had a molecular tumor board were more likely to use ngs tests than were those who did not have these characteristics . 
in addition , those who treated fewer than 50 patients with cancer per month were more likely to use ngs tests than were oncologists who treated more than 50 patients with cancer per month . 
the likelihood of ngs use was not statistically significantly associated with other provider and practice characteristics assessed . in this survey , oncologists in the united states were asked how often they used 11 commercially available ngs tests or a noncommercial ngs test during the past 12 months ( fig 1 )  . 
moreover , among oncologists who ordered any of these ngs tests ( n = 959 ) , 28.2% ordered one test , 31.7% ordered two tests , 23.3% ordered three tests , and 16.7% ordered four or more tests in the past 12 months . ngs test use practice patterns oncologists use of ngs test results varied by clinical presentation ( fig 2 )  . 
characteristics of oncologist respondents in the united states to the 2017 national survey of precision medicine in cancer treatment ( continued ) total ( n = 1 , 281 ) unweighted percentage ( % ) * weighted percentage ( % ) * characteristic no . 
we found that oncologists who used the breast cancer index , mammaprint , prosigna , and / or myplan lung cancer did not differ in the way they answered these questions in nine out of 10 comparisons . 
when analyses were restricted to oncologists who treated a high volume of patients with breast cancer , there were no differences in test use between oncologists who used the breast cancer index , mammaprint , and prosigna and those who did not ( data not shown )  . respondents were explicitly directed to exclude oncotype dx when answering questions about ngs testing for different clinical purposes . 
use of ngs testing during the past 12 months among oncologists in the united states , by physician demographics and practice characteristics ( continued ) total ( n = 1 , 281 ) ngs user ( unadjusted % ) ngs user ( adjusted % ) 95% ci adjusted or ( 95% ci ) characteristic sees patients at academic center or medical school no . 
twenty - five percent ( n = 319 ) indicated that they referred their patients to another location or provider for ngs testing ; among these oncologists , 84.4% ( n = 257 ) referred to an academic medical center , 82.1% ( n = 240 ) to a clinical trial , and 18.2% ( n = 51 ) to an oncologist outside of their practice ( data not shown )  . discussion in this nationally representative study of 1 , 281 oncologists , we examined how ngs tests are currently used in clinical practice and whether use is influenced by physician and practice characteristics . 
 initial diagnosis rare cancers advanced refractory disease unknown origin never rarely sometimes often reported using ngs test results to guide patient care , and the use of ngs tests differed by oncologists demographic and practice characteristics . 
 for example , younger oncologists were more likely to be ngs test users , suggesting that they may have had more recent training in genomic testing or that they are more receptive to the incorporation of ngs testing in their practice . 
 having a faculty appointment and access to a molecular tumor board were also associated with ngs test use , perhaps reflecting greater access to in - house ngs tests in academic settings or more involvement in clinical research . 
 not surprisingly , oncologists who treated only patients with hematologic malignancies were less likely to use ngs tests than were oncologists who treated both solid and hematologic malignancies or those who treated only patients with solid tumors , suggesting that ngs tests may be ordered reflexively by pathologists rather than by oncologists . 
use of next generation sequencing tests by clinical purpose during the past 12 months among oncologists in the united states . molecular testing for patients with hematologic malignancies . oncologists reported using ngs most often for patients with advanced refractory disease , but also used these tests often for patients diagnosed with a rare cancer or cancers of unknown origin and / or for patients with an initial diagnosis of cancer . 
these results may reflect oncologists use of ngs testing to inform treatment strategies when established therapies have failed or when there is uncertainty about the usefulness of existing treatment guidelines for less common clinical situations . 
with the recent approval of multiple therapeutic agents targeting specific driver mutations , oncologists may send a patients tumors for sequencing with the hope of identifying treatments that are potentially efficacious for their patients particular molecular tumor subtype . 
in our survey , more than one third of oncologists reported using ngs test results often to guide the use of an fda approved therapy . advances in precision oncology pose challenges for oncologists . 
at the time of the survey in may 2017 , nonsmall - cell lung cancer was the only cancer type for which there was a consensus recommendation for ngs use.13 furthermore , no professional group other than the national comprehensive cancer network has yet issued evidence - based guidelines recommending the use of ngs testing . 
 however , as the number of single - gene or focused - indication ( eg , microsatellite instability ) tests that are components of the standardized evaluation of common malignancies has grown , oncologists are increasingly faced with decisions about whether to order several targeted tests or a single ngs panel . there has also been an effort by pharmaceutical companies to develop tissue - agnostic cancer drugs that target a specific genetic marker independent of tumor type.14 given the prospect of tissue - agnostic labeling , the use of ngs will only grow , and in the absence of clinical guidelines informing ngs use , it is likely that many providers will experience uncertainty about how to clearly integrate this information into clinical care decisions . 
 treatment recommendations , suggesting that oncologists are already confronted with a large volume of genomic information that they must interpret . that ngs test results are frequently ambiguous presents another challenge for oncologists . 
in addition , 25% indicated that they referred patients to other providers for ngs testing , possibly suggesting a lack of expertise or resources for ordering and interpreting ngs tests . 
several academic and commercial groups have responded to this need , developing online decision support resources for genomic medicine , such as personalized cancer therapy , my cancer genome , and oncokb , with the goal of providing an accessible platform to oncologists.15 however , more work is needed to ensure that patients who can benefit from these new technologies receive appropriate testing and follow - up . a third challenge for oncologists is the lack of clinical usefulness data for many of the available ngs tests . 
two major , ongoing clinical trials , ( national cancer institute nci - match molecular analysis for therapy choice ) , 16 and pediatric match ( national cancer institute childrens oncology group pediatric match trial ) , will generate evidence to establish clinical usefulness to fill some of these gaps . 
furthermore , ascos targeted agent and profiling utilization registry ( tapur ) study17 and cureone ( formerly called med - c ) are building registries of ngs testing data to enhance informed treatment recommendations difficulty in interpreting results never / rarely sometimes often understanding of how testing is being used and its impact on patient outcomes.18 insurers are also recognizing the cost efficiencies of ngs panel testing as opposed to multiple single - gene testing for specific cancer - site indications but are grappling with a lack of clinical usefulness data for testing cancers broadly . 
 effective march 16 , 2018 , the centers for medicare & medicaid services has allowed non fda - approved assays run in clinical laboratory improvement amendmentscertified laboratories to be reimbursed , dependent on decisions made by local medicare administrative contractors.19 it is unclear whether and under what circumstances commercial private payers will decide to reimburse for ngs testing broadly for cancer . 
our findings offer an important baseline that could be used to evaluate the impact of these coverage decisions on ngs test use because our data were collected before implementation of these key changes in coverage . our study has several limitations . 
first , the cooperation rate was lower than that of previous surveys of physicians on the topic of genomic and genetic test use , 7 , 20 and responders may have differed from nonresponders in terms of their genomic testing practices and other characteristics such as academic affiliation . 
however , respondents are representative of the population of practicing oncologists in the united states in terms of age , sex , and geographic location on the basis of statistical adjustment for nonresponse using data available on the survey 's sample frame . another limitation is that we were unable to assess how oncologists use the tests in specific clinical situations and for which cancer types they are ordering these tests . 
however , these limitations are offset by several strengths of the study , including the nationally representative sample of practicing oncologists in a wide variety of practice settings and the large sample size , which allowed us to analyze multiple factors associated with ngs use and to examine a variety of practice patterns . the majority of oncologists in the united states use ngs tests to guide patient care , even in the absence of evidence - based practice guidelines . 
schilsky research funding : astrazeneca ( inst ) , bayer ag ( inst ) , bristol - myers squibb ( inst ) , genentech / roche ( inst ) , eli lilly ( inst ) , merck ( inst ) , pfizer ( inst ) deborah schrag consulting or advisory role : journal of the american medical association research funding : pfizer other relationship : journal of the american medical association naoko i . 
simonds stock and other ownership interests : cvs health ( i ) , walgreens boots alliance , anthem foundation , anthem foundation ( i ) , celgene ( i ) , cvs health , johnson & johnson , johnson & johnson ( i ) , walgreens boots alliance ( i ) , labcorp , labcorp ( i ) , valeant pharmaceuticals international , valeant pharmaceuticals international ( i ) , endo pharmaceuticals ( i ) , aetna ( i ) helmneh m . 
miller fa , hayeems rz , bytautas jp , et al : testing personalized medicine : patient and physician expectations of next - generation genomic sequencing in late - stage cancer care . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental findings : results from the canseq study . 
johnson lm , valdez jm , quinn ea , et al : integrating next - generation sequencing into pediatric oncology practice : an assessment of physician confidence and understanding of clinical genomics . 
 appendix physician characteristics included age , sex , race or ethnicity , faculty appointment , training in genomic testing ( eg , instruction throughout residency and / or fellowship , professional lectures or seminars , symposiums , conferences , or continuing medical education )  . 
practice characteristics , such as region , urbanicity , type of practice ( solo , single specialty group , multispecialty group , other ) , academic affiliation , and number of unique patients with cancer seen per month were also collected . 
in addition , questions were asked about whether the oncologists practice setting has a genomic or molecular tumor board , policies for genomic testing use , and / or an electronic medical record that provides alerts when a genomic test is recommended . 
an oncologists specialty was defined using information on type ( s ) of patients with cancer seen : only patients with solid tumors , only those with hematologic malignancies , or both . 
age and demographic characteristics other than race or ethnicity were obtained from the american medical association masterfile . an oncologists was classified as a user of next - generation sequencing ( ngs ) tests if he or she reported use , in the past 12 months , of specific multimarker panels with ngs technologies profiling multiple actionable driver genes used to guide treatment decisions . 
the following tests were included in this definition : cancerselect or cancer complete , caris molecular intelligence or target now , cgi complete , foundationone , foundationoneheme , foundationact , gps cancer , guardant360 , omniseq comprehensive , onkosight tumor panels , solid tumor mutation panel ( arup laboratories ) , and noncommercial tumor panels . 
multimarker tests that use gene - expression profiling ( eg , oncotype dx for breast cancer ) , primarily used to predict prognosis and / or the likelihood of recurrence , were not classified as ngs tests . 
tan author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license corresponding author : david s.p. 
indeed , hrd - related genetic aberrations may confer a similar clinical phenotype to gboc , 7 , 8 including improved responses and longer progression - free survival ( pfs ) in patients receiving maintenance parpi treatment.9 - 11 few effective treatment options exist for patients with recurrent hgsoc ( rhgsoc ) , especially in the context of malignant bowel obstruction , where the use of bevacizumab is associated with a higher risk of bowel perforation.12 we present the case of a patient with a germline pathogenic rad51c mutation who received salvage treatment for terminal malignant bowel obstruction with sixth - line carboplatin and pegylated liposomal doxorubicin ( pld ) , followed by maintenance olaparib . a 57 - year - old chinese woman was referred to our institution after hgsoc relapse . 
she first received the hgsoc diagnosis at 53 years of age , with no family history of breast or ovarian cancer , and had received initial treatment elsewhere ( table 1 )  . 
at first relapse of hgsoc ( after a 28 - month pfi ) , she received carboplatin plus pld every 4 weeks for six cycles , followed by secondary debulking . 
she received four cycles of carboplatin every 3 weeks with dose - dense paclitaxel once per week , followed by two cycles of cisplatin substituted for carboplatin , owing to grade 2 carboplatin hypersensitivity . 
complete response was achieved with a nadir ca - 125 concentration of 90 u / ml . three months later , however , the patients ca - 125 level rose to 571 u / ml , at which point she transferred care to our institution . 
clinical presentation and treatment summary treatment received at another institution presentation and treatment date may 2010 july 2010 july - nov 2010 mar 2013 apr - june 2013 july 2013 sept - nov 2013 june 2014 july - nov 2014 jan 2015 feb 2015 apr - june 2015 june 2015 june - nov 2015 feb - june 2016 june 2016 july - oct 2016 nov 2014 ca - 125 level nadir of 90 u / ml . complete response determined from repeated ct scan . transfer of care to our institution genetic testing performed using invitae panel . hgsoc diagnosed at another institution . 
 switched to cisplatin ( 75 mg / m2 ) and paclitaxel ( 175 mg / m2 ) every 3 weeks for two more cycles in view of grade 2 hypersensitivity to carboplatin . biochemical recurrence ; ttp : 3 months ; ca - 125 level : 571 u / ml . 
no measurable disease seen on ct scan . genetic testing showed pathogenic grad51c mutation . symptomatic hgsoc relapse ; pfi now 5 months ; ca - 125 level : 3 , 145 u / ml . 
intestinal obstruction resolved with conservative management . switched to fourth - line carboplatin ( auc 5 ) with desensitization protocol and gemcitabine ( 1 , 000 mg / m2 , days 1 and 8 ) every 3 weeks . carboplatin ( auc 5 ) treatment continued with desensitization protocol and gemcitabine ( 1 , 000 mg / m2 , days 1 and 8 ) every 3 weeks ; total of eight cycles with partial response . 
ct scan shows residual 3.6 - cm pelvic implant . ct scans showed new ascites and increasing size of peritoneal implant . patient enrolled in phase i study of low - dose whole abdominal radiation therapy ( 60 cgy fractions , 2 d / wk , twice on each of those days ) , in combination with weekly paclitaxel ( 80 mg / m2 )  . 
pfs while receiving olaparib treatment : 7 months . underwent surgical exploration and defunctioning jejunostomy . july 2017 multiple levels of malignant small - bowel obstruction developed . patient referred to hospice care . 
she joined a phase i trial of kpt330 ( clinicaltrials.gov identifier : nct02078349 ) , but her disease progressed after 2 months , and she had an intestinal obstruction from worsening peritoneal metastases . 
after eight cycles , sustained partial response ( pr ) was achieved according to gynecologic cancer intergroup criteria.14 the ca - 125 concentration improved from 7 , 550 u / ml to 368 u / ml . 
the patient was given a chemotherapy holiday . unfortunately , after another short ttp of 2 months , there was symptomatic disease progression , and the patient was enrolled in a phase ii clinical trial of low - dose , whole - abdomen radiation combined with weekly paclitaxel treatment . 
this approach was based on the knowledge that genomic hrd could enable prediction of response to dna - damaging agents such as carboplatin and topoisomerase iia inhibitors.15 the patient chose carboplatin plus pld every 4 weeks , and her disease responded according to gynecologic cancer intergroup criteria . 
the patient was experiencing grade 2 fatigue and , in view of emerging data at that time on the efficacy of parpis in tumors with hrd , 16 a complete break from treatment , versus off - label maintenance therapy with olaparib capsules , was discussed . 
 she chose the latter option . because of financial constraints , the patient was prescribed olaparib capsules 200 mg twice daily ( rather than the 400 - mg twice - daily standard dosing ) , but her disease continued to respond , with a reduction in ca - 125 level from 1 , 405 u / ml to a nadir of 44.7 u / ml ( fig 2 )  . 
after 6 months of olaparib treatment , scans confirmed pr by response evaluation criteria in solid tumors ( recist ) , version 1.1 , with improved ascites and resolution of a perihepatic peritoneal deposit ( fig 1 )  . unfortunately , the patients disease relapsed a month later with small - bowel obstruction and required parenteral nutrition . 
 ( a and b ) june 2016 ( preplatinum rechallenge ) : left lung lesion ( curved arrow ) , ascites , and peritoneal thickening ( double arrow )  . 
 ( e and f ) april 2017 resolution of ascites and of the deposit at the hepatic hilum after 6 months of olaparib treatment ( originally seen in ( d ) , arrow )  . many to be a preterminal event.17 retrospective data show limited responses from chemotherapy.17 yet , this patient responded remarkably to sixthline carboplatin plus pld and , per the recent us food and drug administration approval for maintenance parpis , derived significant benefit from olaparib , even at an off - label dose of 200 mg twice daily . 
notably , biologically effective inhibition of parp by olaparib capsules has been demonstrated even at 100 mg twice daily.18 to our knowledge , this report is the first to describe the clinical effect of this specific grad51c variant on treatment selection and patient outcome in rhgsoc . the cancer genome atlas project showed approximately 30% of hgsoc cases harbor nonbrca1 / 2 mutation - related hrd . 
 more recently , olaparib , 7 - 9 niraparib , 10 and rucaparib16 were approved for use in patients who have received at least two prior treatments of platinum - based chemotherapy and are platinum responsive . 
of note , all patients eligible for the landmark phase iii trials , 9 - 11 leading to approval of parpi for this indication , had experienced a ttp after penultimate platinum exposure of 6 months , which was not the case in our patient . efficacy data on resensitization to platinum based chemotherapy and thresholds constituting an effective pfi are ambiguous . 
dramatic reduction of ca - 125 level from 17 , 256 u / ml to 867.7 u / ml was noted after the patient commenced receiving carboplatin plus pld treatment . 
analyses revealed a frameshift - truncating mutation of tp53bp1 , which is associated with olaparib resistance.33 reversion mutations in rad51c have also been described in acquired rucaparib resistance.34 unfortunately , at the time of disease progression , surgeons were unable to obtain an adequate tumor sample for analysis of resistance mechanisms in the patient in the current report . in conclusion , patients with ovarian cancer with grad51c mutations may benefit from similar treatment paradigms as brca1 / 2 - mut disease . 
 darwin tay no relationship to disclose valerie heong consulting or advisory role : roche ; astrazeneca patents , royalties , other intellectual property : royalties received for drug venetoclax travel , accommodations , expenses : astrazeneca soo chin lee honoraria : roche ; astrazeneca ; pfizer ; novartis consulting or advisory role : pfizer ; novartis ; astrazeneca ; roche ; eisai research funding : eisai ; taiho pharmaceutical ; bayer ; aslan pharmaceuticals expert testimony : novartis travel , accommodations , expenses : roche ; novartis ; pfizer ; act genomics yee liang thian no relationship to disclose pei yi ong no relationship to disclose samuel g.w. 
jeyasekharan honoraria : msd oncology yi wan lim no relationship to disclose siew eng lim no relationship to disclose research funding : astrazeneca ; perkin elmer travel , accommodations , expenses : perkin elmer joseph ng no relationship to disclose jeffrey j.h. 
tan honoraria : astrazeneca ; roche consulting or advisory role : astrazeneca ; roche research funding : astrazeneca ( inst ) ; karyopharm therapeutics ( inst ) ; bayer ( inst ) travel , accommodations , expenses : merck sharp & dohme ; merck serono ; astrazeneca ; bayer ; roche affiliations natalie y.l. 
alsop k , fereday s , meldrum c , et al : brca mutation frequency and patterns of treatment response in brca mutation - positive women with ovarian cancer : a report from the australian ovarian cancer study group . 
song h , dicks e , ramus sj , et al : contribution of germline mutations in the rad51b , rad51c , and rad51d genes to ovarian cancer in the population . 
swisher em , harrell mi , lin k , et al : brca1 and rad51c promoter hypermethylation confer sensitivity to the parp inhibitor rucaparib in patients with relapsed , platinum - sensitive ovarian carcinoma in ariel2 part 1 . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
pujade - lauraine e , ledermann ja , selle f , et al : olaparib tablets as maintenance therapy in patients with platinum - sensitive , relapsed ovarian cancer and a brca1 / 2 mutation ( solo2 / engot - ov21 ) : a double - blind , randomised , placebo - controlled , phase 3 trial . 
coleman rl , oza am , lorusso d , et al : rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebocontrolled , phase 3 trial . 
rustin gj , vergote i , eisenhauer e , et al : definitions for response and progression in ovarian cancer clinical trials incorporating recist 1.1 and ca 125 agreed by the gynecological cancer intergroup ( gcig )  . 
tan ds , kaye sb : chemotherapy for patients with brca1 and brca2 - mutated ovarian cancer : same or different ? am soc clin oncol educ book 35 : 114 - 121 , 2015 16 . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
kaye sb , lubinski j , matulonis u , et al : phase ii , open - label , randomized , multicenter study comparing the efficacy and safety of olaparib , a poly ( adp - ribose ) polymerase inhibitor , and pegylated liposomal doxorubicin in patients with brca1 or brca2 mutations and recurrent ovarian cancer . 
gayarre j , martn - gimeno p , osorio a , et al : characterisation of the novel deleterious rad51c p.arg312trp variant and prioritisation criteria for functional analysis of rad51c missense changes . 
hatanaka a , yamazoe m , sale je , et al : similar effects of brca2 truncation and rad51 paralog deficiency on immunoglobulin v gene diversification in dt40 cells support an early role for rad51 paralogs in homologous recombination . 
yokoyama h , sarai n , kagawa w , et al : preferential binding to branched dna strands and strand - annealing activity of the human rad51b , rad51c , rad51d and xrcc2 protein complex . 
somyajit k , mishra a , jameei a , et al : enhanced non - homologous end joining contributes toward synthetic lethality of pathological rad51c mutants with poly ( adp - ribose ) polymerase . 
ghiringhelli f , richard c , chevrier s , et al : efficiency of olaparib in colorectal cancer patients with an alteration of the homologous repair proteworld j gastroenterol 22 : 10680 - 10686 , 2016 33 . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
 exceptional response to akt inhibition in patients with breast cancer and germline pten mutations belinda kingston , mbchb1 ; caroline bailleux , md2 ; suzette delaloge , md , msc2 ; gaia schiavon , md , phd3 ; veronique scott , phd2 ; magali lacroix - triki , md , phd2 ; t . 
hedley carr , phd3 ; iwanka kozarewa , phd3 ; heidrun gevensleben , md4 ; zoe kemp , phd5 ; alex pearson , phd1 ; nicholas turner , md , phd1 , 5 ; and fabrice andr e , md , phd2 introduction cowden syndrome is an autosomal dominant genetic disease with an estimated incidence of one in 200 , 000 . 
pip3 functions as a secondary messenger in the pi3k pathway that binds and activates proteins that have a pleckstrin homology domain , such as akt1 , and triggers their activation and localization to the plasma membrane , promoting cellular proliferation and survival.4 germline pten loss - of - function mutations may result in dominant akt activation as a driving oncogenic event in cowden - related breast tumors.5 preclinical evidence suggests that cancers with akt activation have increased sensitivity to akt inhibition.6 preliminary clinical evidence is derived from phase i and ii trials in patients with breast cancers bearing somatic mutations in the pi3k / akt / mtor pathway.7 - 11 inhibitor of all three isoforms of capivasertib ( azd5363 , astrazeneca ) is a potent and selective oral serine / threonine kinase akt ( ie , akt1 , 2 , 3 ) and has preclinical evidence of efcacy as monotherapy or in combination with cytotoxic and targeted therapies.12 - 15 despite the encouraging progression - free survival observed with capivasertib monotherapy in heavily pretreated patients with akt1 e17kmutant breast and gynecologic cancers , 9 recist response rates in phase i studies only reached 22% ( table 1 ) .8 , 9 , 16 because pten loss activates akt1 , we hypothesized that tumors from patients with cowden syndrome could be sensitive to this drug family . which was estrogen ( er ) and progesterone receptor negative , human epidermal growth factor receptor 2 ( her2 ) negative , and was designated grade iii invasive carcinoma of no special type ( nst )  . 
the patient received six cycles of neoadjuvant cyclophosphamide 600 mg / m2 , epirubicin 75 mg / m2 , and docetaxel 100 mg / m2 before a mastectomy with left axillary lymph node dissection ( revealing residual disease in 10 of 18 lymph nodes ) and adjuvant radiotherapy . eight months later , the patient experienced relapse with cutaneous disease and thoracic nodal volvement . 
after enrolling in safir02 ( clinicaltrials.gov identier : nct02299999 ) , targeted panel sequencing ( ion torrent pgm ; thermo fisher scientic , villebon , france ) of a fresh tumor biopsy sample revealed the presence of a heterozygous germline pten mutation ( c.389g.a , rs121909229 ) alongside other variants ( fig 1a ; data supplement )  . 
in the context of safir02 , the patient was randomly assigned to maintenance targeted therapy and received capivasertib 480 mg twice per day , 4 days on and 3 days off . 
on the right side , she presented with a t3 , erpositive and progesterone receptorpositive , her2negative , grade ii invasive carcinoma nst with 20 of 23 involved lymph nodes . 
in may 2010 , the patient received six cycles of chemotherapy every 3 weeks ( uorouracil 600 mg / m2 , epirubicin 75 mg / m2 , and cyclophosphamide 600 mg / m2 ) before starting maintenance tamoxifen . 
she received eight cycles of paclitaxel ( 90 mg / m2 on days 1 , 8 , and 15 of a 28 - day cycle ) combined with capivasertib ( 360 mg twice per day on days 2 - 5 , 9 - 12 , and 16 - 18 of each 28 - day in june 2013 , a computed tomography scan cycle )  . showed a complete response of the liver metastases . 
she had a conrmed maintained response in may 2014 until progression occurred in june 2014a progression - free survival of 19 monthsand a maintained complete response for 12 months on capivasertib alone ( fig 2c )  . 
plasma circulating tumor dna analysis from baseline and progression time points during the beech study showed no major changes ( data supplement )  . discussion the akt inhibitor capivasertib has been examined in early - phase trials ( table 1 ) , and no complete responses have been noted , yet both patients with cowden syndrome presented here had durable complete responses to capivasertib . 
cdc14 , phosphatase domaillustration from ( b ) immunohistochemistry demonstrating ( i ) absent pten staining in the tumor and ( ii ) cytoplasmic and membranous expression of pakt in the 40% of tumor cells . 
cdc14 , phosphatase domaillustration from ( b ) pten immunohistochemistry from ( i ) control tissue and ( ii ) noncancerous and ( iii and iv ) tumor - containing lymph node . 
 ( c ) computed tomography ( ct ) scans during the patients time on capivasertib , with white arrows indicating disease in the liver : ( i ) october 2012 , baseline ct demonstrating a liver deposit ; ( ii ) january 2013 , ct following two cycles of paclitaxel and capivasertib ; ( iii ) ct demonstrating continued complete response on maintenance capivasertib 7 months after cessation of paclitaxel ; and ( iv ) may 2014 , nal ct before progression june 2014 . nonmalignant cells carrying a germline pten mutation to pi3k - pathway inhibition . 
similar to the cases presented here , no severe toxicity was noted in the pilot study , 21 with just one patient experiencing a grade 3 adverse event ( hypophosphatemia / hypercholesterolemia )  . in recent years , drugs targeting the pi3k / akt / mtor pathway have been developed . 
in contrast , akt inhibitors in combination with paclitaxel have been shown to be more active in patients with triple - negative breast cancers harboring a pik3ca / pten / akt1 pathway alteration.7 , 10 similarly , pi3k inhibitors have demonstrated activity in patients with pik3ca mutations.22 , 23 of note in case 2 is the presence of the second - hit pten stop - gain mutation y88x , present with an af of 25.5%. however , the presence of a tp53 mutation at an af of 51.9% indicates that this second - hit mutation is subclonal rather than a truncal driver mutation . 
explanations for the pten phenotype in case 1 include undetected loh , pten promotor hypermethylation , 24 , 25 complex pten genomic rearrangements , 26 and post - translational modication.27 contrary to the two - hit model by knudson et al28 of tumorigenesis in tumor suppressor genes , pten aberrations appear to be protumorigenic in the absence of a second hit . in 2010 , alimonti et al29 demonstrated that pten hypermorphic mice ( with 80% of the normal pten protein level ) had a greater propensity to tumorigenesis than mice with two functional alleles but were less tumorigenic than pten heterozygous mice , supporting a haploinsufciency model of tumorigenesis in pten aberrations . a later in vivo study of pten knock - in mouse models suggested that the conformation of pten underlies the dominant - negative behavior of pten heterozygous mutants . 
this supports the rationale that pten heterozygous mutants act in a dominant - negative manner to promote tumorigenesis . the patients in the cases presented here were treated with combination chemotherapy and capivasertib followed by capivasertib monotherapy . 
the patient in case 1 had previously demonstrated tumor resistance to taxane therapy , with residual disease after neoadjuvant chemotherapy and a short progression - free survival after treatment of primary breast cancer . 
the second patient achieved a complete response with the combination of paclitaxel and capivasertib and maintained this complete response for a period of 12 months on capivasertib alone , suggesting that capivasertib was highly active in this patient . in summary , these two patients with breast cancer and different germline pten mutations both showed a dramatic response to capivasertib superior to that seen in early trials of the drug . 
 magali lacroix - triki leadership : mypl stock and other ownership interests : mypl honoraria : myriad genetics , genomic health consulting or advisory role : roche travel , accommodations , expenses : agendia t . 
hedley carr employment : astrazeneca stock and other ownership interests : astrazeneca iwanka kozarewa employment : astrazeneca stock and other ownership interests : astrazeneca kingston et al zoe kemp honoraria : lilly honoraria : astrazeneca nicholas turner consulting or advisory role : roche , novartis , astrazeneca , pzer , bicycle therapeutics , bristol - myers squibb , merck sharp & dohme , tesaro , lilly research funding : pzer ( inst ) , roche ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , bio - rad ( inst ) , guardant health ( inst ) fabrice andr e research funding : astrazeneca ( inst ) , novartis ( inst ) , pzer ( inst ) , lilly ( inst ) , roche ( inst ) , daiichi ( inst ) travel , accommodations , expenses : novartis , roche , glaxosmithkline , astrazeneca no other potential conicts of interest were reported . references tan mh , mester jl , ngeow j , et al : lifetime cancer risks in individuals with germline pten mutations . 
j med genet 37 : 828 - 830 , 2000 lee yr , chen m , pandol pp : the functions and regulation of the pten tumour suppressor : new modes and prospects . 
miller tw , p erez - torres m , narasanna a , et al : loss of phosphatase and tensin homologue deleted on chromosome 10 engages erbb3 and insulin - like growth factor - i receptor signaling to promote antiestrogen resistance in breast cancer . 
oncogene 24 : 7455 - 7464 , 2005 davies br , guan n , logie a , et al : tumors with akt1e17k mutations are rational targets for single agent or combination therapy with akt inhibitors . 
mol cancer ther 14 : 2441 - 2451 , 2015 kim sb , dent r , im sa , et al : ipatasertib plus paclitaxel versus placebo plus paclitaxel as rst - line therapy for metastatic triple - negative breast cancer ( lotus ) : a multicentre , randomised , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 18 : 1360 - 1372 , 2017 banerji u , dean ej , p erez - fidalgo ja , et al : a phase i open - label study to identify a dosing regimen of the pan - akt inhibitor azd5363 for evaluation in solid tumors and in pik3ca - mutated breast and gynecologic cancers . 
schmid p , abraham j , chan s , et al : azd5363 plus paclitaxel versus placebo plus paclitaxel as rst - line therapy for metastatic triple - negative breast cancer ( pakt ) : a randomised , double - blind , placebo - controlled , phase ii trial . 
patnaik a , appleman lj , tolcher aw , et al : first - in - human phase i study of copanlisib ( bay 80 - 6946 ) , an intravenous pan - class i phosphatidylinositol 3 - kinase inhibitor , in patients with advanced solid tumors and non - hodgkins lymphomas . 
zhang c , xu b , liu p : addition of the p110 inhibitor byl719 overcomes targeted therapy resistance in cells from her2 - positive - pten - loss breast cancer . tumour biol 37 : 14831 - 14839 , 2016 14 . 
yu y , savage re , eathiraj s , et al : targeting akt1 - e17k and the pi3k / akt pathway with an allosteric akt inhibitor , arq 092 . 
agarwal r , liebe s , turski ml , et al : targeted therapy for genetic cancer syndromes : von hippel - lindau disease , cowden syndrome , and proteus syndrome . discov med 19 : 109 - 116 , 2015 77 : 787 - 795 , 2016 68 : 7066 - 7072 , 2008 16 . 
pediatr res 75 : 527 - 534 , 2014 iacobas i , burrows pe , adams dm , et al : oral rapamycin in the treatment of patients with hamartoma syndromes and pten mutation . 
komiya t , blumenthal gm , ballas ms , et al : a pilot study of sirolimus ( s ) in subjects with cowden syndrome ( cs ) with germ - line mutations in pten . 
baselga j , dent sf , cort es j , et al : phase iii study of taselisib ( gdc - 0032 ) + fulvestrant ( fulv ) v fulv in patients ( pts ) with estrogen receptor ( er ) - positive , pik3ca - mutant ( mut ) , locally advanced or metastatic breast cancer ( mbc ) : primary analysis from sandpiper . 
a chest computed tomography scan coupled with an 18f - labeled uorodeoxyglucosepositron emission tomography scan identied a metabolically active lymphadenomegaly in the mediastinuflow cytometric analysis identied a bone marrow ( bm ) blast population ( fig 1a ) that was transferase , terminal deoxynucleotidyl negative for cd2 , cd4 , cd8 , and cd1a and positive for human leukocyte antigen ( hla - dr ) , cd38 , cd117 , cd33 , cd34 , cd56 , cd99 , cycd3 , cd5 , cd7 , cd10 , cd19 , and cd13 . because of a t - all immature phenotype9 , 10 and a myeloid interface , and despite cd5 expression , this patient was diagnosed with near - etp all.11 molecular cytogenetic studies showed the presence of ddx3xmllt10 fusion gene derived from a three - way t ( x ; 3 ; 10 ) ( p11 ; ? ; p13 ) translocation . 
molecular cytogenetic studies revealed an abnormal karyotype characterized by an isolated numerical abnormality ( ie , 47 , xx , + 4 [ 6 ] / 46xx [ 4 ] ) , a rearrangement of bcl11b , and an internal tandem duplication of flt3 ( fig 1a )  . because of advanced age and comorbidities , patient was treated with prednisone 0.5 mg / kg and vincristine 1.4 mg / m2 ( days 1 , 8 , 15 , and 22 ) , without achieving hematologic remission . 
scoring the response in relation to data for t - all on a drp platform , 8 the b - cell lymphoma 2 ( bcl2 ) inhibitor bh - 3 mimetic venetoclax ( abt - 199 ) and the proteasome inhibitor bortezomib ranked in all three cases among the most active drugs ( fig 1b )  . 
next , we validated the activity of venetoclax and bortezomib using an open microwell microuidic platform developed by cellply15 ( bologna , italy ; figs 1c and 1d ) and an atp - based cellular viability assay ( fig 1e ) on etp cells that , consistent with data reported in the literature , 16 , 17 express a high level of bcl2 ( fig 1af )  . on the basis of these ndings , individualized treatment with venetoclax and bortezomib ( vebo ) was then administered on an outpatient basis , sequentially or in combination , as off - label agents after approval by the relevant institutional review board . 
all patients received a cycle with venetoclax ( 800 mg per day 28 days ) by mouth and bortezomib ( 1.3 mg / m2 twice a week 2 [ upr1 , upr2 ] or 4 [ upg3 ] ) , with no evidence of major toxicities . 
upr1 and upr2 received antiviral prophylaxis with acyclovir , whereas upg3 received antimycotic treatment with micafungin . patients obtained a hematologic complete ( upr2 ) or partial remission ( upr1 and upg3 ) assessed a month after vebo initial treatment quantied by morphology , ow cytometry analysis , and uorescence in situ hybridization on bone marrow cells ( figs 1g and 1h )  . 
dose - response curves were generated as previously published using ve - point drug dilutions in duplicate.8 a ranked list of top hits was generated according to the criteria , emax ( ie , the % viability at the maximal drug concentration used ) of less than 15% and signicant ( p , .05 ) difference of half maximal inhibitory concentration ( ic50 ) value for each drug compared with the median ic50 for each particular drug in the reference data set.8 in bold : venetoclax and bortezomib ( vebo )  . 
 ( c ) effect of 24 hours of the vehicle ( dimethyl sulfoxide ) , 10 mm hydrogen peroxide ( h2o2 ) , venetoclax , and bortezomib on cellular viability as measured by a functional proling , on the basis of laboratory - on - a - chip technology , which allows testing the response of live tumor cells exposed to anticancer drugs in an automated process developed by cellply . 
high - content time - lapsed imaging was performed for 24 hours , every 12 hours , on cells in 480 microwells ( 75 m diameter ) at a 1 px - 1 m resolution at each time point / condition tested . 
 ( g ) bm cytology at relapse ( pre vebo ) and after completion of treatment with vebo ( post vebo ; may - gr unwald giemsa staining at 63 )  . 
the marrow contains 50% ( patient 1 [ upr1 ] ) , 90% ( patient 2 [ upr2 ] ) , and 28% ( patient 3 [ upg3 ] ) of lymphoid blasts before treatment , which decreased rapidly after vebo . 
a 500 - cell count was performed based on examination of multiple elds to assess hematologic remission ( complete remission indicates a blast percentage , 5% in the bm )  . 
 ( i ) percentage of ddx3x - mllt10 ( upr1 ) and etv6 / cdkn1bdel ( upg3 ) fish - positive bm cells during vebo treatment and after an allogeneic hematopoietic stem - cell transplantation . 
the analysis was performed on 500 to 1 , 000 interphase nuclei for each experiment ; the cutoff for ddx3x - mllt10 fusion was 2% and for etv6 / cdkn1bdel was 3% . 
this is , for example , the case of - secretase inhibitors in notch1mutated t - all.21 an alternative option is to develop individualized approaches on the basis of pattern of responses to small molecule inhibitors.22 a rst example was the development of a drp in primary acute myeloid leukemia samples . 
the ex vivo testing of 187 drugs in 28 consecutive acute myeloid leukemia cases22 led to the identication of ve major taxonomic drug - response subtypes with distinct genomic features . 
importantly , therapies on the basis of drp resulted in several clinical responses.22 more recently , frismantas et al8 extended this idea and reported a proof - of - concept study by testing 60 drugs in 68 all cases . 
interestingly li et al27 demonstrated that venetoclax acts synergistically with the mcl1 - specic inhibitor s63845 in a broad panel of t - all cell lines and in zebrash embryos undergoing transplantation with t - all cells . 
moreover , venetoclax showed clinical activity in patients with t - all both in combination with chemotherapy28 or decitabine , 29 suggesting that it may be safely included in different therapeutic regimens . in addition , bortezomib has recently emerged as a potential modulator of the oncogenic t - all driver notch1 . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . antonio pierini consulting or advisory role : pzer , biotest patents , royalties , other intellectual property : antibody to deliver cells for islet engraftment in diabetes jean - pierre bourquin travel , accommodations , expenses : servier , amgen cristina mecucci patents , royalties , other intellectual property : patent on npm1 mutations in acute myeloid leukemia with normal karyotype no other potential conicts of interest were reported . references deangelo dj , yu d , johnson jl , et al : nelarabine induces complete remissions in adults with relapsed or refractory t - lineage acute lymphoblastic leukemia or lymphoblastic lymphoma : cancer and leukemia group b study 19801 . 
blood 109 : 5136 - 5142 , 2007 bassan r , bourquin jp , deangelo dj , et al : new approaches to the management of adult acute lymphoblastic leukemia . 
blood 126 : 833 - 841 , 2015 inukai t , kiyokawa n , campana d , et al : clinical signicance of early t - cell precursor acute lymphoblastic leukaemia : results of the tokyo childrens cancer study group study l99 - 15 . 
front med 6 : 416 - 420 , 2012 jain n , lamb av , obrien s , et al : early t - cell precursor acute lymphoblastic leukemia / lymphoma ( etp - all / lbl ) in adolescents and adults : a high - risk subtype . 
blood 127 : 1863 - 1869 , 2016 brammer je , saliba rm , jorgensen jl , et al : multi - center analysis of the effect of t - cell acute lymphoblastic leukemia subtype and minimal residual disease on allogeneic stem cell transplantation outcomes . 
bone marrow transplant 52 : 20 - 27 , 2017 frismantas v , dobay mp , rinaldi a , et al : ex vivo drug response proling detects recurrent sensitivity patterns in drug - resistant acute lymphoblastic leukemia . blood 129 : e26 - e37 , 2017 chopra a , bakhshi s , pramanik sk , et al : immunophenotypic analysis of t - acute lymphoblastic leukemia . 
coustan - smith e , mullighan cg , onciu m , et al : early t - cell precursor leukaemia : a subtype of very high - risk acute lymphoblastic leukaemia . lancet oncol 10 : 147 - 156 , 2009 2017 11 . 
murphy sb , bowman wp , abromowitch m , et al : results of treatment of advanced - stage burkitts lymphoma and b cell ( sig + ) acute lymphoblastic leukemia with high - dose fractionated cyclophosphamide and coordinated high - dose methotrexate and cytarabine . 
kantarjian h , thomas d , obrien s , et al : long - term follow - up results of hyperfractionated cyclophosphamide , vincristine , doxorubicin , and dexamethasone ( hyper - cvad ) , a dose - intensive regimen , in adult acute lymphocytic leukemia . 
bassan r , masciulli a , intermesoli t , et al : final results of northern italy leukemia group ( nilg ) trial 10 / 07 combining pediatric - type therapy with minimal residual disease study and risk - oriented hematopoietic cell transplantation in adult acute lymphoblastic leukemia ( all )  . 
rocchi l , faenza a , rambelli l , et al : ex - vivo drug response proling for precision medicine approaches in acute myeloid leukemia with the open microwell microuidic platforblood 128 : 1675 , 2016 124 : 3738 - 3747 , 2014 16 . 
peirs s , matthijssens f , goossens s , et al : abt - 199 mediated inhibition of bcl - 2 as a novel therapeutic strategy in t - cell acute lymphoblastic leukemia . 
punnoose ea , leverson jd , peale f , et al : expression prole of bcl - 2 , bcl - xl , and mcl - 1 predicts pharmacological response to the bcl - 2 selective antagonist venetoclax in multiple myeloma models . 
chonghaile tn , roderick je , gleneld c , et al : maturation stage of t - cell acute lymphoblastic leukemia determines bcl - 2 versus bcl - xl dependence and cancer discov 3 : 1416 - 1429 , 2013 sensitivity to abt - 199 . 
li z , he s , look at : the mcl1 - specic inhibitor s63845 acts synergistically with venetoclax / abt - 199 to induce apoptosis in t - cell acute lymphoblastic 28 . 
rahmat lt , nguyen a , abdulhaq h , et al : venetoclax in combination with decitabine for relapsed t - cell acute lymphoblastic leukemia after allogeneic hematopoietic cell transplant . 
koyama d , kikuchi j , hiraoka n , et al : proteasome inhibitors exert cytotoxicity and increase chemosensitivity via transcriptional repression of notch1 in t - cell acute lymphoblastic leukemia . 
 clinical equipoise for trials of novel biologic therapies , therapeutic success rates , and predictors of success : a meta - analysis purpose the demand for more rapid access to novel biologic therapies than randomized controlled trials can deliver is a topic of ongoing study and debate . 
we aimed to inform this debate by estimating therapeutic success from phase iii trials comparing novel biologic therapies with standard of care and identifying predictors of success . methods this was a meta - analysis of phase iii trials evaluating novel biologic therapies in advanced breast , colorectal , lung , and prostate cancers . 
therapeutic success was defined as statistically significant results for the primary end point favoring novel biologic therapies . results of 119 included phase iii trials ( 76 , 726 patients ) , therapeutic success was 41% , with a statistically significant relative reduction in disease progression and death for novel biologic therapies over standard of care of 20% and 8% . 
therapeutic success of phase iii trials with and without a preceding phase ii trial were 43% and 30% , respectively conclusion therapeutic success of novel biologic therapies in phase iii trials , including therapies with a matching predictive biomarker , was modest and has not significantly improved over time . 
2017 by american society of clinical oncology introduction advancement in genomic medicine has led to rapid development of novel biologic therapies ( nbts ) that target aberrant pathways in cancer . the success of some of these agents , 1 - 5 whose efficacy was evident from early - phase trials , has led to calls for expediting drug development , evaluation , and approval . 
the introduction of accelerated access programs in europe and the united states recognizes the potential value of using nonrandomized early - phase trials to support new drug approvals.6 , 7 however , there are serious concerns about the risk of relying on lessrobust evidence , and the evidence requirements for nbts is a topic of ongoing debate among the research community.8 - 12 although the requirement for phase iii randomized controlled trials ( rcts ) for assessing the efficacy of conventional treatments is well established , 13 - 15 this issue has not been definitively addressed for targeted therapies . central to the argument for retaining phase iii rcts to generate evidence is the assumption of equipoise . 
thus , critical questions for the evaluation of nbts are : does the evidence to date support the belief that nbts are associated with superior therapeutic success ( ts ) over nontargeted standard - of - care ( soc ) doah cho felicia t . 
characteristics of included phase iii randomized controlled trials and proportion of treatment comparisons achieving therapeutic success ( 119 trials , 132 treatment comparisons ) ( continued ) randomized treatment comparisons therapeutic success 16 ( 33 ) 37 ( 44 ) note . 
this information is critical to the ethics of continuing to require phase iii rcts of nbt versus a control soc treatment after promising results from early - phase studies . this study aims to assess whether existing phase iii evidence demonstrates that , as a class , nbts are superior to soc . 
we also sought to identify predictors of ts and to specifically examine whether the rate of success was higher for trials that used a personalized approach by selecting a population defined by a predictive biomarker . methods we searched the medline and embase databases to identify rcts published in english from january 1 , 1990 to january 31 , 2014 ( data supplement )  . 
we also hand - searched published meta - analyses , conference proceedings , clinical trial registries , reference lists , and citations of included studies . trials were eligible if they evaluated the superiority of nbts over soc and reported overall survival ( os ) or pfs . 
soc treatments were chemotherapy , endocrine therapy , or best supportive care . rcts were excluded if they involved radiotherapy or vaccine therapy , included nbts in all arms , or were of noninferiority design . we identified prior studies referenced by the included rcts . 
we defined prior studies as providing enough matched evidence to inform phase iii rcts if they assessed the same monotherapy or combination in the same advanced tumor population as the included rct . 
if not reported , these were estimated where possible using the methods described by parmar and colleagues.19 we plotted the distributions of the hr point estimates for pfs and os from phase iii trials to describe the spread of ts . 
distribution of overall therapeutic success ( ts ) for novel versus standard therapies for : ( a ) overall survival ( os ) and ( b ) progression - free survival ( pfs ) for randomized controlled trials ( rcts ) overall , and ( c ) os and ( d ) pfs for rcts with a biomarkerselected population . 
trial characteristics are summarized in table 1 ( individual trial characteristics , data supplement )  . we used logistic regression to identify characteristics of the phase iii rcts and preliminary evidence studies that predicted ts in phase iii rcts . 
we examined the correlation between objective tumor responses ( otrs ) reported in the nbt arms of the phase iii and companion phase ii trials using weighted linear regression . results the search strategy identified 132 randomized comparisons from 119 eligible phase iii rcts , comprising 76 , 726 patients ( appendix fig a1 , online only ; data supplement )  . 
pfs was used as the primary end point in 22 ( 92% ) , 22 ( 37% ) , two ( 17% ) , and 12 ( 32% ) breast , lung , prostate , and colorectal comparisons , respectively . 
os was used as the primary end point in two ( 8% ) , 37 ( 63% ) , nine ( 75% ) , and 19 ( 51% ) breast , lung , prostate , and colorectal comparisons , respectively . 
ts was highest in breast ( 15 comparisons , 63% ) , followed by colorectal ( 15 comparisons , 41% ) , lung ( 21 comparisons , 36% ) and prostate cancer ( two comparisons , 17% ) rcts . 
of 70 rcts with nonstatistically significant findings , four ( 6% ) were inconclusive because of premature closure secondary to slow accrual . figures 1a and 1b show distributions of hrs for os and pfs for all phase iii rcts . 
nbts were associated with a 20% and 8% statistically significant relative reduction in the risk of disease progression and death , respectively , over soc ( fig 2a )  . 
a statistically significant relative advantage of nbt versus soc for pfs and os was also observed within each tumor group , although there was substantial heterogeneity between tumor groups ( fig 2a )  . thirty - four comparisons from 29 ( 24% ) rcts were conducted in biomarker - selected populations . 
the shapiro - wilk test indicated that the results deviated from normality . nbts were associated with a statistically significant 28% and 8% relative reduction in disease progression and death , respectively , over soc ( fig 2b )  . a biomarker - selected population was associated with a 4.74 - fold increase in ts compared with rcts with an unselected population ( table 2 )  . trials that used pfs as the primary end point were associated with a 5.22 - fold increase in ts compared with rcts using os ( table 2 )  . 
this evidence was derived from phase i , single - arm phase ii , randomized phase ii , and randomized phase iii trials for 23 ( 17% ) , 41 ( 31% ) , 10 ( 8% ) , and 27 ( 20% ) phase iii comparisons , respectively . 
alternative preliminary evidence used to justify the included phase iii rcts were : monotherapy studies when the phase iii comparison was combination therapy , combination therapy with a different conventional backbone treatment to the included phase iii comparison , evidence from other solid cancers , evidence from observational studies , and evidence from retrospective biomarker analyses or unselected populations for phase iii randomized comparisons in biomarker - selected populations ( data supplement )  . 
in this sample , otr in phase ii trials correlated poorly with otr in the subsequent phase iii trials ( r2 = 0.15 ; appendix fig a2 , online only )  . 
for example , 73% of the randomized arms in the national cancer institutesponsored cooperative oncology group trials were in the setting of early rather than advanced cancer . despite sobering overall ts rates , even in the current era of nbt , debate about the need for phase iii rcts after promising results in earlierphase studies has largely focused on biomarkerselected populations.11 our findings provide some support for the concern that equipoise may be lost for such treatments that progress to testing in phase iii rcts . 
however , later studies showed responses in patients with tumors lacking egfr expression , 26 , 27 whereas significantly lower responses were seen in patients with tumors harboring a mutation in the kirsten - rat sarcoma gene ( k - ras ) .28 , 29 supportive evidence of this was shown in retrospective correlative biomarker analyses of rcts30 , 31 and confirmed by meta - analyses.32 , 33 cetuximab and panitumumab efficacy was restricted to k - ras wild - type patients , and there was no additional benefit of adding egfr - monoclonal antibodies to chemotherapy over chemotherapy alone in patients harboring mutations . 
past rcts30 , 31 of egfr - monoclonal antibodies with chemotherapy against chemotherapy alone allowed for this qualitative interaction between k - ras status and randomized treatment to be examined in an unbiased manner . 
consistent with other studies , seruga et al20 reported that 32% of phase iii trials did not have an appropriate preceding phase ii trial , and more than half of these trials failed to show ts . 
single - arm phase ii trials are also increasingly considered as not sufficiently informative for the decision to proceed to a phase iii rct.34 , 35 although a review of predominantly chemotherapy trials reported limited advantage of randomized over single - arm phase ii studies , 36 randomized phase ii trials with concurrent controls have been considered to be more informative for nbts.34 , 35 in the current study , an association between the level of evidence of preliminary trials ( phase i , single - arm phase ii , randomized phase ii , and randomized phase iii ) and ts of subsequent phase iii rcts was not demonstrated . 
we also excluded certain classes of drugs , such as vaccines , as we considered the mechanism of action of these therapies differed from other biologics , so our findings may not be generalizable to these other classes . despite the advances in genomic medicine and examples of exceptional success for some new therapies , the evidence for their ts from our review remains modest . 
despite calls that nonrandomized evidence may be sufficient in this era of targeted therapy , our review indicates that equipoise remains and supports the ongoing ethical and scientific requirement for phase iii rcts to provide a more definitive and valid estimate of treatment efficacy and a predictive and prognostic value of potential biomarkers . 
links no relationship to disclose should be confirmed using a larger sample size of comparisons . randomized phase ii trials may also have an important role in addressing the problem of optimal dose finding of targeted therapies . 
the maximum tolerated dose defined by the traditional dose - finding strategy for cytotoxic therapies may not be the optimal dose for targeted therapies where interand intrapatient variability has a greater effect on treatment efficacy and toxicity.37 , 38 randomized phase ii trials should be used to a larger degree to compare the efficacy and toxicity of different doses , better define long - term toxicity , and identify targeted therapies amenable to dose escalation or reduction.37 - 40 the main strength of our study is that we have comprehensively reviewed all published rcts that compared nbts against soc providing a contemporary review of predictors of ts . 
 chee khoon lee honoraria : astrazeneca travel , accommodations , expenses : astrazeneca acknowledgment we thank rhana pike ( national health and medical research council clinical trials centre ) for editorial support . affiliations doah cho , felicia t . 
lord , the university of notre dame , darlinghurst , new south wales , australia . supported in part by national health and medical research council ( nhmrc ) postgraduate research scholarship ( medical / dental ) no . 
shaw at , kim dw , nakagawa k , et al : crizotinib versus chemotherapy in advanced alk - positive lung cancer . n engl j med 368 : 2385 - 2394 , 2013 3 . 
camidge dr , bang yj , kwak el , et al : activity and safety of crizotinib in patients with alk - positive non - small - cell lung cancer : updated results from a phase 1 study . 
kim dw , ahn mj , shi y , et al : results of a global phase ii study with crizotinib in advanced alk - positive nonsmall cell lung cancer ( nsclc )  . 
european medicines agency : draft guideline on the scientific application and the practical arrangements necessary to implement the procedure for accelerated assessment pursuant to article 14 ( 9 ) of regulation ( ec ) no 726 / 2004 ( revision 1 )  . 
avorn j , kesselheim as : the 21st century cures actwill it take us back in time ? n engl j med 372 : 2473 - 2475 , 2015 9 . 
kurzrock r : on the shoulders of giants : cooperative groups and clinical trial design - past , present , and future . presented at american society of clinical oncology annual meeting , chicago , il , june 1 - 5 , 2016 10 . 
yao jc , meric - bernstam f , lee jj , et al : accelerated approval and breakthrough therapy designation : oncology drug development on speed ? clin cancer res 19 : 4305 - 4308 , 2013 11 . 
menis j , hasan b , besse b : new clinical research strategies in thoracic oncology : clinical trial design , adaptive , basket and umbrella trials , new end - points and new evaluations of response . 
djulbegovic b , kumar a , glasziou pp , et al : new treatments compared to established treatments in randomized trials . cochrane database syst rev 10 : mr000024 , 2012 15 . 
djulbegovic b , kumar a , soares hp , et al : treatment success in cancer : new cancer treatment successes identified in phase 3 randomized controlled trials conducted by the national cancer institute - sponsored cooperative oncology groups , 1955 to 2006 . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
herbst rs , gandara dr , hirsch fr , et al : lung master protocol ( lung - map ) - a biomarker - driven protocol for accelerating development of therapies for squamous cell lung cancer : swog s1400 . 
van cutsem e , peeters m , siena s , et al : open - label phase iii trial of panitumumab plus best supportive care compared with best supportive care alone in patients with chemotherapy - refractory metastatic colorectal cancer . 
saltz lb , rubin m , hochster h , et al : cetuximab ( imc - c225 ) plus irinotecan ( cpt - 11 ) is active in cpt - 11 refractory colorectal cancer ( crc ) that expresses epidermal growth factor receptor ( egfr )  . 
chung ky , shia j , kemeny ne , et al : cetuximab shows activity in colorectal cancer patients with tumors that do not express the epidermal growth factor receptor by immunohistochemistry . 
adelstein ba , dobbins ta , harris ca , et al : a systematic review and meta - analysis of kras status as the determinant of response to anti - egfr antibodies and the impact of partner chemotherapy in metastatic colorectal cancer . 
liang rf , zheng ll : the efficacy and safety of panitumumab in the treatment of patients with metastatic colorectal cancer : a meta - analysis from five randomized controlled trials . 
fromer mj : oncology drug dosing : can an optimal dose be fine - tuned for each patient ? issues / december - 15 - 2013 / oncology - drug - dosing - can - an - optimal - dose - be - fine - tuned - for - each - patient / 39 . 
companion phase ii trials , testing the same novel biologic therapies as the phase iii trials , were identified for 54% ( n = 64 ) of included phase iii trials . 
 predisposition to lung adenocarcinoma in a family harboring the germline egfr v843i mutation kouki ohtsuka , md , phd1 ; hiroaki ohnishi , md , phd1 ; masachika fujiwara , md , phd1 ; takeshi morii , md , phd1 ; satsuki matsushima1 ; wataru ogura1 ; satoko yamasaki , md1 ; tomonori kishino , md , phd1 ; ryota tanaka , md , phd1 ; and takashi watanabe , md , phd1 introduction in patients with nonsmall - cell mutations in the tyrosine kinase domain of epidermal growth factor receptor ( egfr ) , most commonly a deletion in exon 19 or an l858r substitution in exon 21 , are frequent lung cancer . 
these egfr mutations are speculated to constitutively activate egfr through phosphorylation and impart tumorigenic properties.1 most egfr mutations occur in somatic tumor tissue , with germline egfr mutations being extremely rare.2 , 3 as a scarce the germline egfr t790m or germline example , v843i mutation has been identied in several families susceptible to lung cancer.2 - 6 to several treatments , we previously reported multiple cases of lung adenocarcinoma in a family with the germline egfr v843i mutation.5 the proband had advanced - stage cancer including egfr resistant tyrosine kinase inhibitors , resulting in poor therapeutic outcomes . 
however , tumors of the proband and other family members both harbored the same somatic egfr l858r mutation in addition to the germline v843i mutation , and it is unclear how these two genetic mutations affected the prognosis of lung cancer in those patients . 
no other family history of malignant disease was revealed on a detailed interview ( table 1 )  . sample preparation the study was approved by the ethics committee of the participating institutes , and written informed consent was obtained from the proband and two family members with lung cancer . 
peripheral blood mononuclear cells of the proband , cancerous pleural effusion from the proband , and formalin - xed parafnembedded tumor samples from her mother and younger brother were subjected to genetic analysis . genomic dna was extracted from these samples for next - generation sequencing ( ngs ) analysis using the dneasy blood & tissue kit ( qiagen , hilden , germany )  . wgs analysis we performed wgs using genomic dna extracted from cancer cells harvested from the cancerous pleural effusion and compared it to that of whole blood . paired - end sequencing was performed using illuminas ngs platforms hiseq x ten system ( illumina , san diego , ca )  . 
 egfr v843i mutation and lung adenocarcinoma we adopted driver gene mutations registered in the catalogue of somatic mutations in cancer ( cosmic ) database , predicted functional consequences using sift and polyphen - 2 software , or categorized them as pathogenic or likely pathogenic per the clinvar database . 
furthermore , we examined known causative germline mutations of hereditary cancers and somatic mutations of major cancerrelated genes among the gene alterations in the proband . ts analysis for ts analysis , we used the ion ampliseq custom panel and ion torrent pgm deep sequencing ion ampliseq cancer hotspot panel v2 ( thermo fisher scientic , waltham , ma )  . 
we examined mutations in 50 cancer - related genes in tumor dna derived from the proband and two of her family members . genomic study wgs revealed the previously reported germline egfr v843i mutation ; however , no other germline oncogenic mutations were observed in the peripheral blood and cancerous pleural effusion of the proband . 
in the clinvar database , the egfr v843i mutation has been registered as likely pathogenic , and the tp53 r248w mutation is pathogenic . other genetic abnormalities , including insertions / deletions , copy - number variations , and structural variations of cancer - related genes , were not detected in blood or cancer cells of the proband ( tables 1 and 2 )  . 
whole - genome sequencing analysis for the proband germline / somatic gene mutation pleural effusion blood egfr v843i l858r tp53 r248w germline somatic somatic via wgs analysis in families harboring the germline egfr mutation ( table 1 ) .4 - 6 wgs analysis of peripheral blood samples of the proband revealed no known genetic abnormalities for hereditary cancers other than the germline egfr v843i mutation , further supporting the possibility that this mutation causes familial lung adenocarcinoma ( tables 1 and 2 )  . 
according to the tohoku university tohoku medical megabank organization database , frequency of the egfr v843i germline mutation is low , amounting to one in 3 , 509 healthy japanese individuals ; however , it is considered an important germline mutation associated with the risk of lung carcinogenesis.8 , 9 furthermore , the somatic tp53 r248w mutation was detected only in cancer cells of the proband but not the other two family members ( tables 2 and 3 )  . 
the other 48 cancer - related oncogenes assessed via ts analysis were not mutated in tumors of any of the family members . although this is an anecdotal case , the present results suggest that the tp53 mutation may serve as a prognostic factor predicting worse drug sensitivity and poor therapeutic outcomes in lung cancer harboring a germline egfr mutation . 
recent studies have reported that lung cancers with both egfr and tp53 mutations are associated with a poor prognosis.10 - 12 the present ndings support our hypothesis that lung cancers harboring egfr and tp53 mutations are refractory and have a poor prognosis , suggesting that analysis of tumor - related oncogenes via wgs or ts may help predict the clinical course of familial lung cancer cases . furthermore , mutations in genes other than egfr are reportedly associated with familial accumulation of lung including germline rb1 , her2 , or tp53 mutacancer , tions.3 , 13 among these , li - fraumeni syndrome , characterized table 3 . 
 ohtsuka et al by germline tp53 mutations , is potentially the most frequent multiple cancer syndrome associated with an increased risk of lung cancer.3 high - throughput analysis of genes associated with multiple cancers , particularly tp53 , is therefore crucial to elucidate the genetic background of patients with familial lung cancer . 
considering the high prevalence of tp53 mutations , somatic or germline , in cases of solitary or hereditary lung cancer , tp53 mutations are apparently an equally prominent cause of lung cancer as egfr mutations . the genome of family in conclusion , ngs analysis of members with the germline egfr v843i mutation reinforced the hypothesis that this mutation predisposes individuals to familial lung adenocarcinoma . 
n engl j med 362 : 2380 - 2388 , 2010 bell dw , gore i , okimoto ra , et al : inherited susceptibility to lung cancer may be associated with the t790m drug resistance mutation in egfr . 
nat genet 37 : 1315 - 1316 , 2005 oxnard gr , nguyen ks , costa db : germline mutations in driver oncogenes and inherited lung cancer risk independent of smoking history . 
j natl cancer inst 106 : djt361 , 2014 ikeda k , nomori h , mori t , et al : novel germline mutation : egfr v843i in patient with multiple lung adenocarcinomas and family members with lung cancer . ann thorac surg 85 : 1430 - 1432 , 2008 ohtsuka k , ohnishi h , kurai d , et al : familial lung adenocarcinoma caused by the egfr v843i germ - line mutation . 
matsushima s , ohtsuka k , ohnishi h , et al : v843i , a lung cancer predisposing egfr mutation , is responsible for resistance to egfr tyrosine kinase inhibitors . j thorac oncol 9 : 1377 - 1384 , 2014 8 . 
nat commun 6 : 8018 , 2015 yasuda j , kinoshita k , katsuoka f , et al : genome analyses for the tohoku medical megabank project towards establishment of personalized healthcare . j biochem 165 : 139 - 158 , 2019 10 . 
labb e c , cabanero m , korpanty gj , et al : prognostic and predictive effects of tp53 co - mutation in patients with egfr - mutated non - small cell lung cancer 11 . 
aggarwal c , davis cw , mick r , et al : inuence of tp53 mutation on survival in patients with advanced egfr - mutant nonsmall - cell lung cancer . 
liu dh , zhao zr , lin yb , et al : prognostic effect of tp53 and pkd co - mutations in patients with resected epidermal growth factor receptor - mutated lung 13 . 
in her article , she cited win et al , 3 who similarly concluded ( after reviewing 15 studies of breast cancer risk in patients with ls ) that a correlation between ls and breast cancer remains inconclusive . 
predisposition to breast cancer has been difcult to prove ( on the basis of studies of ls populations ) , but it might be possible to identify members of ls families who carry a germline pathogenic mismatch repair ( mmr ) variant that is likely to predispose them to breast cancer . for example , the immunohistochemical ngerprint of ls - related cancers has decient mmr ( dmmr ) protein expression that is demonstrated in nearly all cancers related to ls . 
breast cancer specimens are now commonly tested for mmr protein expression , in part because the us food and drug administration approved checkpoint inhibitor therapy for dmmr metastatic breast cancer.4 however , sporadic breast cancers are rarely associated with dmmr.3 , 5 thus , it seems reasonable that identifying dmmr in a patient with ls and breast cancer strongly suggests that the germline pathogenic mmr variant predisposed that patient to breast cancer . 
but it is possible that the loss of mmr expression was not the gatekeeper or cancer - initiating event ; instead , a later driver event may have contributed to the cancer phenotype . 
the natural history of ls and responsiveness to checkpoint inhibitor therapies in patients who have dmmr breast cancers may or may not be similar to the response in patients with sporadic dmmr breast cancers . 
it is also unclear whether risk factors besides the germline mmr mutation are involved in transformation to dmmr breast cancer . family members who harbor the same germline pathogenic variant might be at similar risk for developing ls - related breast cancers . 
the magnitude of risk for developing a dmmr breast cancer in a member of an ls family that has 1 or more members who have also developed breast cancer would be known only after mmr assays of breast cancers from several members of that family . 
this could be quite difcult , given that breast cancer tissue from family members from past generations might not be available . counseling patients in ls families , it remains crucial to recognize that personal and family history of breast cancer remain the standard basis for predicting risk of developing breast cancer , regardless of whether an ls family member is found to have a dmmror a procient mmr - expressing breast cancer . 
the possibility of ascertainment bias would prevent concluding that the same lost mmr expression in breast cancers from 1 ls family would imply the same likelihood of patients developing dmmr breast cancers in another ls family . as win et al3 noted , individual tumor testing results suggest that mmr deciency is involved with breast cancers in some individuals with lynch syndrome . future studies might include assays to detect mmr expression in patients with ls and breast cancer . 
stoll j , rosenthal e , cummings s , et al : no evidence of increased risk of breast cancer in women with lynch syndrome identied by multigene panel testing . 
katz , md1 ; huamin wang , md , phd1 ; xuemei wang , ms1 ; laura prakash , md1 ; milind javle , md1 ; rachna shroff , md1 ; david fogelman , md1 ; santiago avila1 ; mohamed zaid , md1 ; dalia elganainy , md1 ; yeonju lee , phd1 ; christopher h . 
we prospectively evaluated uorouracil , leucovorin , irinotecan , and oxaliplatin ( folfirinox ) - based treatment and imaging - based biomarkers for borderline resectable pdac . methods eligible patients had treatment - nave , histology - conrmed pdac and one or more high - risk features : mesenteric vessel involvement , ca 19 - 9 level of 500 mg / dl or greater , and indeterminate metastatic lesions . patients received modied folfirinox and chemoradiation before anticipated pancreatectomy . 
overall survival ( os ) and progression - free survival ( pfs ) were estimated using the kaplan - meier method , and subgroups were compared using log - rank tests . results thirty - three patients initiated therapy ; 45% underwent pancreatectomy . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction personalized treatment of patients with pancreatic ductal adenocarcinoma ( pdac ) has been limited by the dearth of validated biomarkers . 
ca 19 - 9 is the only food and drug administrationapproved prognostic biomarker for pdac , but it is limited to patients with sialyl lewis apositive genotype . terpretation of this test can be unreliable.1 , 2 smad4 , 3 which transduces intracellular signaling of transforming growth factor beta , and human equilibrative nucleoside transporter 14 - 6 may be useful in guiding therapy , 3 , 7 but prospective validation has been unsuccessful , highlighting the need for robust biomarker integration for pdac clinical trials . 
in a disease that is at - large systemically disseminated on presentation with a propensity for early progression while receiving therapy , there is an unmet need for predictive bioindicate benet from local markers for pdac that therapies , such as radiation and surgical resection . we have identied ct - based biomarkers using morphologic characteristics of pdac , 8 , 9 each identifying distinct prognostic groups . 
 koay et al context key objective few effective therapies exist for pancreatic ductal adenocarcinoma ( pdac ) , and no biomarkers have been validated to personalize therapy for this aggressive disease . 
we report a phase ii clinical trial of preoperative modied uorouracil , leucovorin , irinotecan , and oxaliplatin ( folfirinox ) and chemoradiation for patients with high - risk borderline resectable pdac , powered to differentiate a resection rate of 60% from 40% . 
we examined whether computed tomography ( ct ) based biomarkers had prognostic association with outcomes . knowledge generated the preoperative regimen achieved a resection rate of 45% , lower than the desired 60% rate in this high - risk population . notably , both a baseline ct - based biomarker ( delta classication ) and post - treatment ct - based biomarker ( interface response ) were associated with outcomes . 
in retrospect , the trial was enriched for patients with poor prognostic biomarkers . relevance the validation of biomarkers derived from standard - of - care ct imaging supports the development of trials that use these as integral biomarkers and may lead to personalized therapeutic management for localized pdac . a standard - of - care pancreas protocol ct , high - delta pdac tumors exhibit an abrupt changeor deltain hounseld units ( hu ) between the visualized tumor and normal pancreas , and low - delta pdac tumors do not exhibit such a change . 
after preoperative therapy , tumors with a type i response remain or become well dened at the interface of tumor and parenchyma , whereas those with a type ii response become less dened at the interface . 
notably , these ct - based biomarkers associate with pathologic features of pdac , such as the extent of stromal reaction10 and pathologic response to therapy.9 we prospectively evaluated clinical associations of ctbased delta scores and ct - interface responses in patients who received preoperative modied uorouracil , leucovorin , irinotecan , and oxaliplatin ( folfirinox ) and gemcitabine - based chemoradiation for localized cancers at high risk for early metastatic progression . 
the primary objective was rate of resection after preoperative therapy , and secondary objectives included toxicity rates , overall survival ( os ) , progression - free survival , and correlation with the imaging - based biomarkers . artery ( sma ) , celiac artery measuring less than or equal to 180 of the arterys circumference , and / or the common hepatic artery11 ; a serum ca 19 - 9 level of 500 mg / dl or more in the presence of a bilirubin level of 2.0 mg / dl or less ; and radiographic ndings consistent with malignant peripancreatic lymphadenopathy outside the planned radiation or surgical eld or liver or peritoneal lesions concerning but not diagnostic for metastatic disease . patients were also required to have an eastern cooperative oncology group performance status ( ps ) of 0 to 1 , 12 an absolute neutrophil count of more than 1 , 500 cells / mm3 , a platelet count of at least 100 , 000 cells / mm3 , a serum creatinine level less than 2 mg / dl , a serum bilirubin level less than 2 mg / dl , and hepatic transaminases less than ve times the upper limits of normal . 
the severity of each patients comorbidity prole was graded as 0 ( none ) , 1 ( mild ) , 2 ( moderate ) , or 3 ( severe ) .13 methods patient eligibility and disease staging the institutional review board at the university of texas md anderson cancer center approved the study protocol ( clinicaltrials.gov identier : nct01560949 ) , and all patients provided written informed consent . 
modied folfirinox , consisting of oxaliplatin ( 75 mg / m2 ) delivered over a 2 - hour period , followed by irinotecan ( 150 mg / m2 ) given over a 90 - minute period , and a continuous infusion of uorouracil ( 2 , 000 mg / m2 ) over 46 hours , was administered once every two weeks for a total of six doses . 
3d conformal radiation therapy at a total dose of 50.4 gy in 28 fractions ( 1.8 gy / fraction ) to the gross tumor volume plus the 1.5to 2 - cm margin was prescribed . 
in addition , delayed gastric emptying and postpancreatectomy hemorrhage were graded using international study group of pancreatic surgery denitions.26 , 27 follow - up patients were evaluated every 4 months after treatment . 
secondary clinical end points included r0 resection rate , toxicity rates , progression - free survival ( date of diagnosis to date of disease progression , date of recurrence , or date of death , whichever came rst ) , os ( date of diagnosis to date of death ) , and patterns of local and distant failure . 
additional assessments included associations of the delta classication and interface response with survival . patient demographic and clinical characteristics were summarized using median ( range ) for continuous variables and frequency ( percentage ) for categorical variables . 
the associations between binary variables , such as between delta classication or margin status and interface response , were presented using bar plots and were assessed for signicance using fishers exact test . 
the probabilities of patients registered ( n = 34 ) initiated mfolfirinox ( n = 33 ) initiated chemoradiation ( n = 23 ) underwent pancreatectomy ( n = 15 ) withdrew consent ( n = 1 ) did not complete mfolfirinox ( n = 6 ) ps / toxicity ( n = 4 ) comorbidities ( n = 1 ) progression of disease with metastasis ( n = 1 ) completed mfolfirinox local progression of disease ( n = 2 ) progression of disease with metastasis ( n = 2 ) progression of disease with metastasis ( n = 5 ) local progression of disease ( n = 1 ) resection aborted due to local tumor ( n = 1 ) factors comorbidities ( n = 1 ) os and pfs were estimated using the kaplan - meier method.28 log - rank tests were used to assess the differences in os or pfs between subgroups of patients dened by delta classication , interface response , and clinical factors ( jmp , sas institute , cary , nc )  . 
adverse events were summarized by frequency , grade , and event type . the simons optimum two - stage design was applied for this study.29 a sample size of 33 was chosen to differentiate between a good resectability rate of 60% and a poor resectability rate of 40% with 80% power and at a signicance level of .10. 
by the end of the trial , lack of efcacy would have been claimed if 16 or fewer patients underwent surgery among the total 33 enrolled patients . results patients from august 2012 through november 2015 , 34 patients enrolled in the study . 
the tumor of 14 patients ( 42% ) had a radiographic interface with the smvportal vein , and that of 16 ( 48% ) had a radiographic interface between both the smvportal vein as well as with the sma , celiac trunk , or the hepatic artery . 
major adverse events within 90 days of pancreatectomy occurred in three of the 15 patients ( 20% ) who underwent pancreatectomy , including postpancreatectomy hemorrhage of grade b ( n = 1 ) and grade c ( n = 1 ) and delayed gastric emptying of grade c ( n = 2 )  . 
there was no perioperative ( 90 - day ) mortality ( appendix table a1 )  . pathologic response and margins the histopathologic characteristics of the 15 resected tumors are listed in table 3 . 
ten of the 15 specimens ( 67% ) had negative ( r0 ) surgical margins ; cancer cells were identied at or within 1 mm of the sma margin in four patients and at the sma and bile duct margin in one patient . 
 ( a ) percent change in size of target lesions for each patient who nished therapy on protocol and had images available for re - review at restaging on the basis of recist ( response evaluation criteria in solid tumor ; n = 23 )  . 
within the progressive disease ( pd ) group , one patient had local progression ( light blue ) , three had distant progression ( gray ) , and two had local and distant progression ( light red )  . 
 ( c ) delta classication from computed tomography ( ct ) scans , showing a low - delta tumor without a distinct interface ( arrow , left ) and a high - delta tumor with a distinct interface ( arrow , right )  . 
events are based on common terminology criteria for adverse events , version 4 . * elevated levels of alkaline phosphatase , alt , and / or ast . imaging biomarkers ct - based delta classication . 
patients who exhibited a type ii interface response were less likely to undergo pancreatectomy compared with those who exhibited a type i response ( figs 2b and 2d ; appendix fig a2 )  . 
the interface response is a visual classication whereby type i responses demonstrate that the tumor / pancreas interface remains or becomes well dened , whereas type ii responses show the interface becomes less dened after treatment.9 arterial and portal venous phases of the pancreas protocol ct scan are used for the delta and interface response metrics . 
surgical and pathologic findings in patients who underwent resection at mdacc ( n = 15 ) discussion variable procedure performed pancreatoduodenectomy distal pancreatectomy vascular resection and reconstruction * isolated venous isolated arterial combined venous and arterial surgical margins tumor differentiation moderate poor % viable tumor no . 
first , the ndings align with our previous observation that preoperative treatment sequencing accurately discriminates patients who are likely to achieve a survival benet from surgery from those who are not.19 the median os of the 15 resected patients was 42.1 months , and ve patients remain alive without evidence of disease recurrence . 
the median os of all patients , 24 months , was similar to that of the alliance for clinical trials in oncology ( clinicaltrials.gov identier : ( alliance ) a021101 trial nct01821612 ) .30 from the baseline and operative characteristics ( median ca 19 - 9 of 200 and 500 in eight patients ; 48% of patients with both arterial and venous involvement , and a high rate of vein resections / reconstructions [ 14 of 15 resected tumors ] ) , it is clear that this study population was enriched with cancers that were both anatomically and biologically advanced . 
indeed , we have previously found baseline ca 19 - 9 values to not be predictive of outcomes , 2 but have observed that changes in ca 19 - 9 are meaningful.32 the scientic basis of the delta classication and interface response seems to involve associations with degrees of stromal inltrate , biologic drivers of the disease , and pathologic response to therapy.8 , 9 a combined approach of baseline and post - treatment imagingbased biomarkers using an early interim look may help inform preoperative and adaptive treatment recommendations for medical and surgical therapies , given both the demonthe imaging - based biostrated prognostic associations of markers and the association of margin status with interface response . 
 ct - based biomarkers in a borderline resectable pancreatic cancer although positron emission tomographyct has shown promise as a diagnostic and prognostic marker for pdac , it has inherent limitations with false negatives ( eg , cold tumors ) , false positives ( eg , pancreatitis ) , and higher cost.33 - 37 our trial used aggressive cytotoxic regimens to treat patients with unfavorable clinical features without regard to the ct - based biomarkers . 
the data show that this unselected approach to therapy leads to rates of radiographic partial response ( 23% ) within the range of previous studies ( 12% to 44% ) .31 , 38 although this approach had reasonable toxicity rates ( table 2 ) , the rates of resection were not as favorable as anticipated . 
the alliance protocol a021501 ( clinicaltrials.gov identier : nct02839343 ) will evaluate the role of hypofractionated radiotherapy in the preoperative setting for patients with borderline resectable disease who were selected only by failure to experience progression on induction chemotherapy.39 however , treatment intensication or selection for new combination systemic agents may be most appropriately considered in patients with high - delta tumors or type ii responses . 
we gratefully acknowledge support from the andrew sabin family fellowship , the sheikh ahmed center for pancreatic cancer research , institutional funds from the university of texas md anderson cancer center , the khalifa foundation , equipment support by ge healthcare and the center of advanced biomedical imaging , philips healthcare , and cancer center support ( core ) grant no . 
was supported by national institutes of health ( u54ca210181 - 01 , u54ca143837 , 1u01ca196403 - 01 , 1u01ca200468 - 01 , 1u01ca214263 - 01a1 , 1r01ca218004 - 01 , and 1r01ca221971 - 01a1 ) , the pancreatic cancer action network ( 1420 - 25 - koay ) , and the radiological society of north america ( rsd1429 )  . our study also highlights the need for rational and relevant end points for a borderline resectable trial that can be translated to a target population . 
in planning prospective trials for borderline resectable pancreas cancer , our results indicate that resection rate alone as a primary end point is inadequate . until additional validation of our response readout available , os and disease - free survival need to be considered as coprimary or primary end points . in conclusion , our data suggest that modied folfirinox followed by chemoradiation has a resection rate similar to historical controls for patients with borderline the novel resectable pdac . 
katz , huamin wang , laura prakash , milind javle , rachna shroff , david fogelman , santiago avila , mohamed zaid , dalia elganainy , yeonju lee , prajnan das , eric p . 
katz consulting or advisory role : alcresta therapeutics , abbvie milind javle other relationship : rafael pharmaceuticals , incyte , pieris pharmaceuticals , merck , merck serono , novartis , seattle genetics , beigene , qed therapeutics , bayer rachna shroff consulting or advisory role : halozyme , seattle genetics , exelixis , merck , qed therapeutics , debio pharma research funding : lilly , celgene , agios , halozyme , pieris pharmaceuticals , taiho pharmaceutical david fogelman stock and other ownership interests : gtx consulting or advisory role : incyte dalia elganainy employment : agios ( i ) stock and other ownership interests : agios ( i ) christopher h . 
crane honoraria : celgene sunil krishnan research funding : celgene ( inst ) , elekta ( inst ) patents , royalties , other intellectual property : receive royalties from a nanotechnology book i co - edited for taylor and francis , md anderson invention disclosures led to patent lings on a number of topics related to nanoparticles and / or minibeam radiation ; some are licensed out or options to license given out travel , accommodations , expenses : tae life sciences prajnan das consulting or advisory role : adlai nortye jason b . 
pct / us2016 / 065763 , entitled polymeric drug delivery systems for treatment of disease , by chun li et al ; in the name of board of regents , the university of texas system eric p . 
lee honoraria : boston scientic , olympus consulting or advisory role : boston scientic research funding : olympus travel , accommodations , expenses : boston scientic anirban maitra honoraria : celgene patents , royalties , other intellectual property : royalties from hangzhou guangkeande ( cosmos ) biotechnology company for blood - based biomarkers of early pancreatic cancer ; i do not own stocks in the company nor do i have any research or grant funding from them robert a . 
varadhachary employment : fannin partners ( i ) leadership : fannin partners ( i ) , pulmotect ( i ) , stock and other ownership interests : fannin partners ( i ) honoraria : celgene , merrimack , rexahn pharmaceuticals , momenta pharmaceuticals , sobi , armo biosciences consulting or advisory role : celgene , merrimack , rexahn pharmaceuticals , momenta pharmaceuticals research funding : merck ( inst ) , pici patents , royalties , other intellectual property : spouse is inventor on a pending patent for an elisa diagnostic platform not related to my area of research ( i ) , spouse is an inventor of use patents relating to recombinant human lactoferrin ; the molecule is no longer in development and patents are being allowed to lapse as payments come due ( i ) travel , accommodations , expenses : celgene , merrimack , sobi no other potential conicts of interest were reported . acknowledgment the authors thank michiko iwasaki for research nurse support and data retrieval . references passerini r , cassatella mc , boveri s , et al : the pitfalls of ca19 - 9 : routine testing and comparison of two automated immunoassays in a reference oncology center . 
am j clin pathol 138 : 281 - 287 , 2012 katz mh , varadhachary gr , fleming jb , et al : serum ca 19 - 9 as a marker of resectability and survival in patients with potentially resectable pancreatic cancer treated with neoadjuvant chemoradiation . 
ann surg oncol 17 : 1794 - 1801 , 2010 iacobuzio - donahue ca , fu b , yachida s , et al : dpc4 gene status of the primary carcinoma correlates with patterns of failure in patients with pancreatic cancer . j clin oncol 27 : 1806 - 1813 , 2009 elebro j , ben dror l , heby m , et al : prognostic effect of hent1 , dck and hur expression by morphological type in periampullary adenocarcinoma , including pancreatic cancer . 
acta oncol 55 : 286 - 296 , 2016 greenhalf w , ghaneh p , neoptolemos jp , et al : pancreatic cancer hent1 expression and survival from gemcitabine in patients from the espac - 3 trial . 
world j gastroenterol 20 : 8482 - 8490 , 2014 loehrer sr pjl , powell me , cardenes hr , et al : a randomized phase iii study of gemcitabine in combination with radiation therapy versus gemcitabine alone in patients with localized , unresectable pancreatic cancer : e4201 . 
j clin oncol 26 : 4506 , 2008 ( 15 suppl ; abstr ) koay ej , lee y , cristini v , et al : a visually apparent and quantiable ct imaging feature identies biophysical subtypes of pancreatic ductal adenocarcinoma . clin cancer res 24 : 5883 - 5894 , 2018 amer am , zaid m , chaudhury b , et al : imaging - based biomarkers : changes in the tumor interface of pancreatic ductal adenocarcinoma on computed tomography scans indicate response to cytotoxic therapy . 
blazer m , wu c , goldberg rm , et al : neoadjuvant modied ( m ) folfirinox for locally advanced unresectable ( lapc ) and borderline resectable ( brpc ) adenocarcinoma of the pancreas . 
allen pj , kuk d , castillo cf , et al : multi - institutional validation study of the american joint commission on cancer ( 8th edition ) changes for t and n staging in patients with pancreatic adenocarcinoma . 
wente mn , bassi c , dervenis c , et al : delayed gastric emptying ( dge ) after pancreatic surgery : a suggested denition by the international study group of pancreatic surgery ( isgps )  . 
katz mh , shi q , ahmad sa , et al : preoperative modied folfirinox treatment followed by capecitabine - based chemoradiation for borderline resectable pancreatic cancer : alliance for clinical trials in oncology trial a021101 . 
murphy je , wo jy , ryan dp , et al : total neoadjuvant therapy with folfirinox followed by individualized chemoradiotherapy for borderline resectable pancreatic adenocarcinoma : a phase 2 clinical trial . 
tzeng cw , balachandran a , ahmad m , et al : serum carbohydrate antigen 19 - 9 represents a marker of response to neoadjuvant therapy in patients with borderline resectable pancreatic cancer . 
asagi a , ohta k , nasu j , et al : utility of contrast - enhanced fdg - pet / ct in the clinical management of pancreatic cancer : impact on diagnosis , staging , evaluation of treatment response , and detection of recurrence . 
katz mh , fleming jb , bhosale p , et al : response of borderline resectable pancreatic cancer to neoadjuvant therapy is not reected by radiographic indicators . j roentgenol 174 : 1005 - 1008 , 2000 cancer 118 : 5749 - 5756 , 2012 39 . 
 appendix koay et al mfolfirinox d ose 1 d ose 2 d ose 3 d ose 4 d ose 5 d ose 6 ebrt 5 weekly gemcitabine d ose 1 d ose 2 d ose 3 d ose 4 d ose 5 surgery weeks systemic phase chemoradiation phase 3 4 5 11 12 13 disease progression or decline in ps protocol fig a1 . 
after initiating mfolfirinox ( uorouracil , leucovorin , irinotecan , oxaliplatin ) , patients would have restaging to assess imaging - based response ( type i v type ii )  . 
patients who show a type ii response would change chemotherapy , while those who have a type i response would continue with mfolifirnox . selective radiation therapy ( rt ) would be delivered or not delivered based on clinical and anatomical factors . 
finally , we characterize the in vitro use of entrectinib against a common alk fusion gatekeeper resistance mutation . methods genomic profiling we performed broad , hybrid capturebased next - generation sequencing using the integrated mutational profiling of actionable cancer targets assay and hisequation 2500 ( illumina , san diego , ca ) .14 alk immunohistochemistry and fluorescence in situ hybridization alk immunohistochemistry was performed using the ventana alk ( d5f3 ) cdx assay ( ventana medical systems , tucson , az )  . 
response , assessed by response evaluation criteria in solid tumors ( recist ) version 1.1 , was monitored by computed tomography ( ct ) imaging performed at baseline , 4 weeks after treatment initiation , and approximately every 8 weeks thereafter.15 treatment was administered until the patient experienced disease progression or unacceptable toxicity . 
permission to publish the patients case was obtained from his health care proxy . generation of engineered ba / f3 cells expressing vcl - alk fusion proteins cdnas that encode vcl - alk and vcl - alk l1196m fusion proteins were inserted into lentiviral vector pvlpuro - ef1a - mcs ( biosettia , san diego , ca )  . 
 transduced ba / f3 cells were selected in puromycin in rpmi 1640 media that contained 10% fetal bovine serum and 10 ng / ml mouse il - 3 ( thermo fisher scientific , waltham , ma ) for 2 weeks . 
 antiproliferative activities of entrectinib and crizotinib in engineered ba / f3 cells results cells seeded at 5 , 000 cells per well in 96 - well plates ( corning , corning , ny ) were treated with serial dilutions of entrectinib ( ignyta , san diego , ca ) and crizotinib ( selleckchem , houston , tx ) added in duplicate to the wells . 
data are averaged from at least two independent experiments and with an r2 of more than 0.9. western blot analysis ten million cells were treated with drug at the indicated concentrations for 2 hours , washed with phosphate - buffered saline , and lysed in 1 radioimmunoprecipitation assay buffer ( emd millipore , billerica , ma ) with benzonase , protease inhibitor , and phosphatase inhibitor cocktails ( emd millipore )  . 
exons 1 to 16 of vcl are fused to exons 20 to 26 of alk , which include the kinase domain . tpm3 eml4 rad51ap2 eml4 22 exons 26 exons exon 1 exon 16 exon 20 - 26 identification of rccs harboring alk fusions a total of 561 samples from 517 patients with rcc were sequenced using broad , hybrid capture based next - generation sequencing ( integrated mutational profiling of actionable cancer targets assay ) .14 , 16 , 17 three ( 0.6% ) of 517 patients with renal cell cancer had tumors that harbored alk fusions . in renal cell cancer , several fusion partners with alk have been previously identified , including vcl , tpm3 , and eml412 , 18 , 19 ( fig 1a )  . 
 the three alk fusions identified in our data set are represented in figure 1b and consist of unclassified - type rcc harboring an vcl - alk fusion developing in a patient with sickle cell trait , chromophobe - type rcc harboring an rad51ap2 - alk fusion , and unclassified - type rcc with an eml4 - alk fusion ( table 1 )  . of these three patients , one was eligible for therapy with a targeted agent against alk , as described below . 
he underwent a right radical nephrectomy , revealing a stage iii ( pt3an1 ) high - grade ( nuclear grade iv ) rcc with rhabdoid and pleomorphic features and nine of 23 positive lymph nodes . 
ct scan 2 months later demonstrated no evidence of recurrence . next - generation sequencing of the primary tumor identified a vcl - alk translocation generating a fusion between exon 16 of vcl and exon 20 of alk ( fig 1c )  . 
clinicopathologic characteristics and therapeutic interventions in patients with alk fusionpositive renal cell carcinoma case age at diagnosis , years pathology fusion additional alterations systemic therapy received vcl - alk none entrectinib renal cell carcinoma , unclassified type renal cell carcinoma , chromophobe type alkrad51ap2 * tert promoter variant pazopanib malt1 h257r nivolumab + bevacizumab nivolumab + lenvatinib lenvatinib + everolimus eml4 - alk tp53 d257y everolimus + bevacizumab renal cell carcinoma , unclassified type erbb4 t194s mst1r f803s dot1l g1358v nivolumab cabozantib abbreviations : alk , anaplastic lymphoma kinase ; f , female ; m ; male . * next - generation sequencing performed on the sarcomatous component of a metastasis . tumor and the age of the patient , hemoglobin electrophoresis was performed , discovering the presence of sickle cell trait.20 entrectinib demonstrates superior in vitro target inhibition and antitumor effect compared with crizotinib twelve months after nephrectomy , surveillance imaging demonstrated confluent lymphadenopathy in the right retrocrural space and an enlarged left superior mediastinal metastatic node . 
given evidence that suggested activity of entrectinib , a multikinase inhibitor of alk , ros1 , trka , trkb , and trkc , against common alk resistance mutations and improved cns penetration compared with crizotinib , the patient enrolled in a clinical trial of entrectinib ( rxdx - 101 ; clinicaltrials.gov identifier : nct02097810 ) .21 four weeks after commencing entrectinib 600 mg per day , a ct scan demonstrated a 31.4% decrease in disease , or partial response . 
the patient maintained excellent performance status throughout treatment , tolerating entrectinib well with the exception of grade 1 peripheral lower extremity edema and grade 2 weight gahis response to entrectinib continued for 19 months , after which imaging revealed radiographic disease progression with increased mediastinal adenopathy , which led to the discontinuation of entrectinib . we interrogated the activity of entrectinib against alk fusions and its common resistance mutations with ba / f3 cell lines that were engineered to overexpress vcl - alk and vclalk l1196m fusion proteins . 
vcl - alk l1196m , a key gatekeeper mutation in the atp binding pocket , confers resistance to crizotinib.22 , 23 for ba / f3 cells that harbor the vcl - alk fusion , entrectinib was more potent than crizotinib ( ic50 = 90.8 nm for entrectinib ; ic50 = 253.0 nm for crizotinib ; fig 3a )  . 
entrectinib and crizotinib both resulted in reduced levels of phospho - alk and the inhibition of phosphorylation of downstream targets , phospholipase c , extracellular signalregulated kinase , and signal transducer and activator of transcription 3 ( fig 3b )  . 
the introduction of the alk l1196m mutation to the vcl - alk construct ( ba / f3 - vcl - alk l1196m ) conferred significantly reduced sensitivity to crizotinib , with an ic50 proliferation value of more than 1 , 000 nm ; however , ba / f3 - vcl - alk l1196m cells remained sensitive to entrectinib , with an ic50 value that was only modestly increased compared with that of ba / f3 - vcl - alk cells ( ic50 = 111.9 nm ; fig 3a )  . 
recently , response to alectinib was reported in patients with metastatic papillary rcc.24 the case detailed here of durable clinical response in a patient with rccadditionally underscores the utility of alk inhibition in alk - rearranged rcc and the potential of targeting alk fusions irrespective of histology . large - scale sequencing efforts have increased the ability to identify alk fusions . 
given their low frequency , single analyte testing for specific alterations is impractical ; however , the increasingly widespread availability of multiplexed next - generation sequencing enhances the feasibility of detecting targetable fusions . 
screening efforts can lead to the detection of other actionable mutations in rcc , such as alterations that involve met , pten , bap1 , mtor , pik3ca , and birc7.25 , 26 clinical outcomes for nonclear - cell rcc ( ncrcc ) remain poor compared with clear - cell rcc . 
despite the small proportion of patients with alk fusion positive rcc , failure to screen in this patient would have prevented the delivery of a well tolerated therapy with a durable response that lasted 19 months . 
 ( b ) treatment of wt ba / f3 vcl - alk and resistant baf3 vcl - alk l1196m cell lines with entrectinib leads to more complete inhibition of downstream targets phosphophospholipase c ( plc ) and phosphosignal transducer and activator of transcription 3 ( stat3 ) compared with crizotinib . 
erk , extracellular regulated kinase . observed in other fusions led to the opening of a multicenter , phase ii basket trial of entrectinib ( clinicaltrials.gov identifier : nct02568267 )  . ultimately , as with this patient , resistance to therapy almost inevitably develops . 
 arcila , hikmat al - ahmadie , gary li , alexander drilon roopal patel employment : ignyta provision of study materials or patients : chung - han lee stock and other ownership interests : ignyta collection and assembly of data : jessica j . 
tao no relationship to disclose ge wei stock and other ownership interests : ignyta , halozyme research funding : ignyta patents , royalties , other intellectual property : ignyta , halozyme travel , accommodations , expenses : ignyta patrick fagan employment : ignyta stock and other ownership interests : ignyta travel , accommodations , expenses : ignyta xueli hao no relationship to disclose julia a . 
arcila consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe , raindance technologies hikmat al - ahmadie consulting or advisory role : bristol - myers squibb , emd serono chung - han lee consulting or advisory role : exelixis , eisai research funding : pfizer ( inst ) , eisai ( inst ) , bristol - myers squibb ( inst ) , calithera biosciences ( inst ) travel , accommodations , expenses : eisai gary li employment : ignyta alexander drilon consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pfizer , blueprint medicines , genentech , takeda , helsinn therapeutics , beigene affiliations jessica j . 
arcila , hikmat al - ahmadie , chung - han lee , and alexander drilon , memorial sloan kettering cancer center ; alexander drilon , weill cornell medical center , new york , ny ; ge wei , roopal patel , patrick fagan , and gary li , ignyta , san diego , ca ; xueli hao , st louis pathology associates , mercy hospital , st louis , mo ; and julia a . 
cui jj , tran - dub m , shen h , et al : structure based drug design of crizotinib ( pf - 02341066 ) , a potent and selective dual inhibitor of mesenchymal - epithelial transition factor ( c - met ) kinase and anaplastic lymphoma kinase ( alk )  . 
lin e , li l , guan y , et al : exon array profiling detects eml4 - alk fusion in breast , colorectal , and nonsmall - cell lung cancers . 
sugawara e , togashi y , kuroda n , et al : identification of anaplastic lymphoma kinase fusions in renal cancer : large - scale immunohistochemical screening by the intercalated antibody - enhanced polymer method . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
hyman dm , solit db , arcila me , et al : precision medicine at memorial sloan kettering cancer center : clinical next - generation sequencing enabling next - generation targeted therapy trials . 
debelenko lv , raimondi sc , daw n , et al : renal cell carcinoma with novel vcl - alk fusion : new representative of alk - associated tumor spectrumod pathol 24 : 430 - 442 , 2011 19 . 
smith ne , deyrup at , mario - enriquez a , et al : vcl - alk renal cell carcinoma in children with sickle - cell trait : the eighth sickle - cell nephropathy ? am j surg pathol 38 : 858 - 863 , 2014 21 . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multitargeted pan - trk , ros1 , and alk inhibitor entrectinib : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . 
lee j - l , ahn j - h , lim hy , et al : multicenter phase ii study of sunitinib in patients with non clear cell renal cell carcinoma . 
tannir nm , jonasch e , albiges l , et al : everolimus versus sunitinib prospective evaluation in metastatic nonclear cell renal cell carcinoma ( espn ) : a randomized multicenter phase 2 trial . 
ardini e , menichincheri m , banfi p , et al : entrectinib , a pan - trk , ros1 , and alk inhibitor with activity in multiple molecularly defined cancer indications . 
robson , md10 purpose screening and prevention decisions for women at increased risk of developing breast cancer depend on genetic and clinical factors to estimate risk and select appropriate interventions . 
a combined risk score ( crs ) of an 86single - nucleotide polymorphism polygenic risk score and the tyrer - cuzick v7.02 clinical risk estimator was generated with attenuation for confounding by family history . 
calibration and discriminatory accuracy of the crs were evaluated in two independent validation cohorts of women of european ancestry ( n = 1 , 615 and n = 518 )  . 
risk stratication with a 20% risk threshold was compared between crs and tyrer - cuzick in an independent clinical cohort ( n = 32 , 576 )  . results simulation studies conrmed that the fixed - stratied method produced accurate risk estimation across patients with different family history . 
in an analysis with both crs and tyrer - cuzick as predictors of breast cancer , crs added signicant discrimination independent of that captured by tyrer - cuzick ( p , 1011 in validation 1 ; p , 107 in validation 2 )  . 
in an independent cohort , 18% of women shifted breast cancer risk categories from their tyrer - cuzickbased risk compared with risk estimates by crs . conclusion integrating clinical and polygenic factors into a risk model offers more effective risk stratication and supports a personalized genomic approach to breast cancer screening and prevention . jco precis oncol 5 : 307 - 316 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction mammography and adjuvant treatment of early - stage disease are widely used for the mitigation of morbidity and mortality in invasive breast cancer.1 effective prevention requires the identication of higher - risk individuals , which has typically involved family history evaluation , assessment of clinical and lifestyle factors , and testing for the presence of pathogenic variants ( pvs ) in a limited number of highor moderate - risk breast cancer genes.2 although guidelines for pv carriers have long recommended enhanced screening and discussion of surgical prevention measures , they do not adequately address the increased risk for unaffected pv - negative women with a strong family history of breast cancer . 
we examined confounding and interaction between an 86 - snp polygenic risk score and each clinical factor in the tyrer - cuzick model to inform the development of a combined clinical and polygenic risk score . 
20% lifetime risk of developing breast cancer . improved risk stratication from the combined risk score can help target the use of more intense screening strategies for unaffected women with truly elevated risk based on clinical and genetic factors . here , we describe the development and validation of a strategy for integrating a snp score with a validated clinical risk model , with attenuation for correlated effects . 
clinical testing cohort data were subdivided according to successive time intervals to ensure the independence of development and validation activities ( fig 1 ) ; this included two development sets ( development 1 and 2 ) , one validation set ( validation 1 ) , and one clinical performance population . 
genetic testing for all patients was performed at a clinical laboratory improvement amendments - approved and college of american pathology - approved laboratory ( myriad genetics , inc . , salt lake city , ut ) by next - generation sequencing.34 hybridization probes for the 86 snps in the prs were included in the sequencing panel.33 women were eligible if they were of age 18 - 84 years , of european ancestry ( ashkenazi and non - ashkenazi ; selfreported ) , and negative for likely pvs or pvs in 11 breast cancerrelated genes ( brca1 , brca2 , tp53 , pten , stk11 , cdh1 , palb2 , chek2 , atm , nbn , and bard1 )  . patients were excluded as unaffected controls if they reported a history of ductal carcinoma in situ , lobular carcinoma in situ , hyperplasia , or unspecied breast disease . women were excluded from the clinical testing cohort if they were submitted from states that disallow the research use of samples after completion of genetic testing . 
all studies were conducted with institutional review board ( irb ) oversight ( quorum review irb #31713 , 32556 , 32608 )  . development 1 included women from the clinical testing cohort unaffected by cancer of any type accrued between june 1 , 2017 and august 11 , 2017 ( n = 5 , 489 )  . 
development 2 ( n = 141 , 160 ) included 112 , 232 women unaffected by breast cancer and 28 , 928 breast cancer cases from the clinical testing cohort accrued between august 11 , 2017 and january 11 , 2019 . 
clinical characteristics of this set were previously reported.33 validation 1 consisted of women in the clinical testing cohort accrued between june 1 , 2017 and august 10 , 2017 ( n = 1 , 615 )  . 
controls included unaffected women submitted for genetic testing because of possible hereditary nonpolyposis colorectal cancer syndrome as these patients have a breast cancer family history consistent with that of general population controls . for validation 2 , a consecutive series of women who presented to four breast cancer screening centers ( elizabeth wende breast care , the breast center of nwa , bethesda health , and cuda women 's health center / cape cod healthcare ) were prospectively recruited between february 6 , 2017 and november 11 , 2017 ( n = 518 )  . 
 integrating clinical and polygenic factors to predict cancer risk cohort description noisulcni noisulcxe accrual findings development n = 5 , 489 clinical testing cohort : 18 - 84 years old , european ancestry , pv - negative , from states that allow research use of data or samples post - testing history of breast cancer , dcis , lcis , hyperplasia , or unspecified breast disease ; eligible for validation set 1 development n = 141 , 160 clinical testing cohort : same inclusion criteria as development set 1 controls could not have a history of dcis , lcis , hyperplasia , or unspecified breast disease validation 1 clinical testing cohort : same basic inclusion or exclusion criteria as development set 2 cases : breast cancer diagnosis , submitted for testing due to suspicion of hboc within 1 year of diagnosis controls : unaffected women submitted for testing due to suspicion of hnpcc prospectively acquired case - control study enrolled from imaging centers cases : pathologically confirmed first diagnosis of invasive breast cancer 12 mos . preenrollment or incident breast cancer 6 mos . 
for each factor , we conducted a simple linear regression with prs as the dependent variable and the clinical factor as the independent variable . from these models , we examined regression coefcients , p values based on f - statistics , and pearson correlation coefcients . design of the combined risk score . 
to calculate absolute risk incorporating tyrer - cuzick and prs , we developed a fixed - stratied method ( data supplement ) to attenuate prs after xing the effects of confounded factors from the tyrer - cuzick model and to constrain risk separately within strata of the confounders . 
absolute risk for a woman in strata k was calculated as follows : ( cid : 3 ) exp { prs + ck } , ( cid : 1 ) 1 tc where represents the per - unit log ( or ) of the prs from a multivariable logistic regression model with the effect of breast cancer family history xed . 
the combined risk score ( crs ) was validated in two independent studies ( table 1 ) : a clinical testing set ( validation 1 ; n = 1 , 615 ) and the prospective case - control cohort ( validation 2 ; n = 518 )  . 
exploratory analyses tested calibration of the crs by comparing average absolute risk estimates with those from the tyrer - cuzick model ; with proper calibration , we expected to observe the same average risk for tyrer - cuzick as for the crs among unaffected controls . 
these analyses were conducted separately for rlr and 5 - year risk of developing breast cancer . weighted logistic regression was used with weights for unaffected controls calculated such that average tyrercuzick rlr matched general population rates ( data supplement )  . performance of the 86 - snp prs . 
in contrast , for women with family history , the fixed - stratied method matched risks from multivariable co - estimation , whereas the unadjusted model overestimated risk ( data supplement )  . clinical validations validation 1 included 988 ( 61% ) breast cancer cases and 627 ( 39% ) unaffected controls ( table 1 )  . 
overall , 362 ( 22% ) patients reported breast cancer in 1 rst - degree relative and 620 ( 38% ) in 1 second - degree relative . the prospectively collected case - control validation 2 included 256 ( 49% ) breast cancer cases and 262 ( 51% ) unaffected controls ( table 1 )  . 
nearly one third ( 29% ) of patients reported breast cancer in a rst - degree relative and 204 ( 39% ) patients in 1 second - degree relative . in both validations , rlr and 5 - year risk estimates of the crs and tyrer - cuzick were signicantly associated with breast cancer ( table 2 and fig 2 )  . 
in a model with both risk predictors , the crs added signicant discrimination independent of that captured by tyrer - cuzick for both rlr ( p , 1011 in validation 1 ; p , 107 in validation 2 ) and 5year risk ( p , 1011 in validation 1 ; p , 107 in validation 2 ; data supplement )  . although all patients in validation 2 provided complete tyrer - cuzick risk factor questionnaires , data on tyrercuzick variables were incomplete for some patients in validation 1 . 
analyses were repeated in the subset of patients with complete information for all tyrer - cuzick risk factors with results similar to those from the full data set ( data supplement )  . calibration of the crs was examined by comparing average risk estimates with those from tyrer - cuzick in the control samples from either validation . 
 hughes et al average remaining lifetime risk in validation cohort 1 ( n = 627 ) average 5 - year risk in validation cohort 1 ( n = 627 ) crs mean ( 95% ci ) tyrercuzick mean ( 95% ci ) fig 3 . 
estimates for average remaining lifetime ( a and c ) and 5 - year risk ( b and d ) for unaffected controls in validation 1 ( a - b ) and validation 2 ( c - d )  . patients were grouped into 5 - year age bins , and average risks were evaluated according to crs and tyrer - cuzick . 95% cis are also reported . 
addition of the 86 - snp score signicantly improved discrimination relative to the tyrer - cuzick model for predicting risk of breast cancer , and the crs model showed excellent calibration across age groups . 
20% - 25% lifetime risk of breast cancer to improve early - stage cancer detection.36 in a clinical testing population , we showed that for 33% of pv - negative women , the crs - estimated risk was  . 
distribution of crs risk estimates in unaffected women . remaining lifetime risk ( rlr ) in a population of unaffected women ( clinical performance population , n = 32 , 576 ; excluded women with ductal carcinoma in situ , lobular carcinoma in situ , hyperplasia , or unspecied breast disease ) according to crs with thresholds at 20% ( increased ) and 50% ( high ) rlr . 
blue squares indicate patients with discordance between the scores ( eg , the tyrer - cuzick model produced a score that indicated a patient had low rlr , but the same patient was determined to have increased rlr by the crs model )  . 
crs , combined risk score . performance integrating clinical and polygenic factors to predict cancer risk increased risk ( crs > 20% ) 33.1% high risk ( crs > 50% ) 0.6% 3000 2500 2000 1500 1000 rlr according to crs ( % ) remaining lifetime risk according to tyrer - cuzick ( 20% ) increased ( > 20% ) crs total 56.5% n = 18 , 398 10.5% n = 3 , 407 67.0% n = 21 , 805 8.0% n = 2 , 619 25.0% n = 8 , 152 33.0% n = 10 , 771 64.5% n = 21 , 017 35.5% n = 11 , 559 100% n = 32 , 576 tyrer - cuzick or crs - based risk discordant increased risk ( > 20% ) high risk ( > 50% ) tyrer - cuzick remaining lifetime risk ( % ) women ( 8% ) who would have been categorized as , 20% using tyrer - cuzickestimated risk alone . combinations of prss with the tyrer - cuzick model have been presented previously , generally without attenuation for confounding . 
an 88 - snp score was added to tyrercuzick under the assumption of independence in a nested case - control study.25 although the snp score added disit had poor crimination to the tyrer - cuzick prediction , calibration . 
first , previous examinations of confounding often evaluated the correlations between a prs and a model rather than individual clinical factors.21 , 25 , 26 this approach might have obscured associations between prs and clinical factors with a stronger genetic component . 
second , genetic overlap is more likely with a larger prs since casting a wider for cancer - associated snps is more likely to also the genetic component of capture a larger fraction of clinical risk . 
1 rst - degree relative or those with second - degree relatives . limitations of the present study include a potential ascertainment bias in the clinical testing population cohorts . qualication for genetic testing is often based on family history . 
it has been previously shown that this potential bias can be avoided by accounting for family history in a multivariable model.38 , 39 consequently , all analyses presented here were conducted by multivariable co - estimation . 
in support of this approach , results from validation 1 ( clinical testing samples ) were similar to results obtained in validation 2 , for which participants were prospectively collected and were unaffected by potential bias due to selection for hereditary cancer testing . 
evaluation of the crs in a prospectively collected , unselected populationbased sample is being pursued.40 future work to expand assessment tools such as tyrer - cuzick and the prs for non - european ancestries will be required to apply these tools to other ancestry populations . 
however , subanalysis of validation 1 in women with complete tyrer - cuzick information showed similar results as the whole data set , indicating that missing information did not substantially affect the analysis . this crs model is suitable for reporting age - specic risk of developing breast cancer for unaffected women of european descent with or without signicant family history . 
it is currently the only tyrer - cuzickbased model fully adjusted for the shared risk between snps and family history and is therefore less likely to overestimate risk in women with a family history of breast cancer . 
lanchbury data analysis and interpretation : elisha hughes , placede tshiaba , susanne wagner , eric rosenthal , benjamin roa , shannon gallagher , stephanie meek , wade hedegard , susan m . 
 integrating clinical and polygenic factors to predict cancer risk benjamin roa employment : myriad genetics leadership : myriad genetics stock and other ownership interests : myriad genetics research funding : myriad genetics patents , royalties , other intellectual property : intellectual property held by employer myriad genetics travel , accommodations , expenses : myriad genetics shannon gallagher employment : myriad genetics stock and other ownership interests : myriad genetics stephanie meek employment : myriad genetics stock and other ownership interests : myriad genetics kathryn dalton speakers bureau : myriad genetics danna f . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca , clovis oncology judy garber consulting or advisory role : novartis , gtx , helix biopharma , konica minolta , aleta biotherapeutics , h3 biomedicine , kronos bio research funding : novartis , ambry genetics , invitae , myriad genetics other relationship : susan g . 
lanchbury employment : myriad genetics leadership : myriad genetics stock and other ownership interests : myriad genetics patents , royalties , other intellectual property : i am an inventor on multiple patents led by myriad genetics travel , accommodations , expenses : myriad genetics alexander gutin employment : myriad genetics stock and other ownership interests : myriad genetics , gilead sciences mark e . 
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br j cancer 98 : 1457 - 1466 , 2008 costantino jp , gail mh , pee d , et al : validation studies for models projecting the risk of invasive and total breast cancer incidence . 
taylor a , brady af , frayling im , et al : consensus for genes to be included on cancer panel tests offered by uk genetics services : guidelines of the uk cancer 11 . 
mccarthy am , armstrong k , handorf e , et al : incremental impact of breast cancer snp panel on risk classication in a screening population of white and african american women . 
zhang x , rice m , tworoger ss , et al : addition of a polygenic risk score , mammographic density , and endogenous hormones to existing breast cancer risk prediction models : a nested casecontrol study . 
lakeman imm , hilbers fs , rodrguez - girondo m , et al : addition of a 161 - snp polygenic risk score to family history - based risk prediction : impact on clinical management in non - brca1 / 2 breast cancer families . 
dite gs , macinnis rj , bickerstaffe a , et al : breast cancer risk prediction using clinical models and 77 independent risk - associated snps for women aged under 50 years : australian breast cancer family registry . 
cuzick j , brentnall ar , segal c , et al : impact of a panel of 88 single nucleotide polymorphisms on the risk of breast cancer in high - risk women : results from two randomized tamoxifen prevention trials . 
j clin oncol 35 : 743 - 750 , 2016 van veen em , brentnall ar , byers h , et al : use of single - nucleotide polymorphisms and mammographic density plus classic risk factors for breast cancer risk prediction . 
brentnall ar , van veen em , harkness ef , et al : a casecontrol evaluation of 143 single nucleotide polymorphisms for breast cancer risk stratication with classical factors and mammographic density . 
evans dg , brentnall a , byers h , et al : the impact of a panel of 18 snps on breast cancer risk in women attending a uk familial screening clinic : a casecontrol study . 
jco precis oncol 4 : 585 - 592 , 2020 judkins t , leclair b , bowles k , et al : development and analytical validation of a 25 - gene next generation sequencing panel that includes the brca1 and brca2 genes to assess hereditary cancer risk . 
carbone , md , phd4 immunotherapy , the advent of including immune checkpoint inhibitors ( icis ) , has contributed to improved survival in patients with lung cancer.1 three antiprogrammed death - 1 ( pd - 1 ) / programmed death ligand 1 ( pd - l1 ) therapies , nivolumab , pembrolizumab , and atezolizumab , are approved by the us food and drug administration ( fda ) for the treatment of patients with advanced nonsmall - cell lung cancer ( nsclc ) in the rst - line setting.2 - 4 despite the improvements in survival seen with icis , there remains a subset of patients who do not benet from ici monotherapy or combination treatments.5 as a result , many research efforts have been initiated to identify biomarkers predictive of response to treatment with icis . 
predictive biomarkers that have entered clinical practice include pd - l1 expression on tumor and immune cells , and tumor mutational burden.2 - 4 , 6 , 7 however , the accuracy of predictions of patient response based on current biomarkers leaves ample room for improvement . 
successful attempts will likely rely on integrated models combining multiple features . the scientic to tackle such complex challenges , community has become increasingly interested in the possibilities offered by data sharing and crowdsourcing as a framework for mobilizing groups of people with shared interests around the world and bringing forward augmented solutions to the existing problems while encouraging collaboration . 
in this context , data sharing can be executed according to two paradigms.8 in the data - to - modeler paradigm , both training and validation data sets are provided to participants . 
the model - to - data paradigm , where participants submit containerized models to organizers , allows validation data sets to remain hidden from participants , which both protects condential data and helps ensure unbiased assessment of predictions . 
these approaches are instrumental broadening our understanding of tumor biology and the tumor microenvironment , which will ultimately drive precision medicine with immunotherapy . to enable such collaboration among scientists and physicians , dialogue on reverse engineering and assessment methods ( dream ) challenges engage experts from around the world and offer novel solutions to biological problems.9 since the rst dream challenges were initiated in 2006 , more than 60 have completed , with analysis results generated through virtual collaborative interactions.10 in oncology , crowdsourcing approaches have been used in multiple tumor types since 2012 for augmenting the work of teams generating data , developing protocols for randomized controlled trials , developing prognostic models , and assessing healthcare behaviors on a large scale.11 more specically , three key dream challenges in oncology have demonstrated the value of crowdsourcing for the development of prognosis models or the renement of diagnostic methods . 
 vincent et al following on from these successful dream challenges , experts in lung cancer have shown interest in accessing primary clinical trial data to explore alternative biomarkers to pd - l1 expression and tumor mutational burden . 
the antipd - 1 response prediction challenge will be the rst dream challenge focused on the prediction of response to immuno - oncology therapies using data from a large phase iii clinical trial , with the goal of addressing the need for additional predictive biomarkers to use with icis in patients with nsclc . 
moreover , this initiative will also enhance the understanding of tumor biology and provide further insights into the potential mechanisms underpinning treatment resistance to icis . challenge objectives the antipd - 1 response prediction challenge will focus on developing models that are predictive of benet from ici treatment , specically nivolumab monotherapy , using patient samples obtained during the conduct of a clinical trial . clinical trial data related to nivolumab , including data related to pd - l1 expression , tumor mutational burden , and tumor transcriptomics , will be used to assess the performance of predictive models submitted in a crowdsourced challenge setting . 
the testing data set will use deidentied data from checkmate 026 ( clinicaltrials.gov identier : nct02041533 ) , a phase iii trial that compared nivolumab with platinum - based chemotherapy in patients with metastatic or recurrent nsclc and pd - l1 tumor expression 5%.15 critically , the data set from checkmate 026 is large , randomized , mature , and well annotated , allowing it to support robust testing of predictive models . 
this challenge also lays the foundation for potential future challenges as the immunooncology landscape is rapidly evolving . the antipd - 1 response prediction challenge aims to assess the accuracy of models for predicting clinical outcomes after nivolumab monotherapy , including efcacy end points such as overall survival , progression - free survival , and best overall response , applying clinical and genomic data from checkmate 026 . 
the challenge will comprise three subchallenges , and their objectives are summarized in figure 1 . challenge design framework has been developed to receive and evaluate dockerized models , which are in silico packages comitself plus necessary software compoprising the model nents to run the model as developed by the participant team . the challenge is open to anyone who will be able to construct models for submission , subject to specications in the challenge rules , including experts and innovators in genomics , computational biology , and translational biomarker development . 
participants can sign up on the synapse website.16 to facilitate data ingestion , participants will have access to a small synthetic data set with the same formatting as the validation data set . 
the full synthetic data set can be downloaded on the synapse website.17 in the rst phase , participants will construct models using any data available to thethe iatlas platform , 18 a database supporting the study of interactions between cancer and the immune microenvironment , hosts harmonized genomics data and associated clinical annotations from published immuno - oncology studies . 
participants can use these as training data sets or to augment other training data already available to them.19 participants could also use professor shirley lius labs tide resources , 20 a computational framework that integrated and modeled data from 189 human cancer studies , comprising 33 , 197 samples.21 more resources to consider are listed on the antipd - 1 response prediction challenge website.16 participants dockerized models will be applied to the checkmate 026 data and evaluated during the competitive phase . 
performance metrics , such as area under the receiver operating characteristic or precision - recall curves and harrells c - index , will be used to assess the predictive performance of participants models in each arm of the checkmate 026 trial . top - performing teams will be invited to participate in the collaborative model - development phase , during which data will be analyzed and interpreted to deepen the understanding of the submitted models . 
eventually , opportunities for additional subchallenges and potential projects will be dened based on the learnings from the current challenge , and teams submitting the best - performing models will have the opportunity to co - author the planned publication in accordance with medical publication standards and best practices . the challenge will rely on a partnership between sage the organization supporting the dream bionetworks , challenge initiatives , and bristol myers squibb and will comprise three phases : competitive , collaborative , and nal . 
the anticipated outcome and impact the identied models are expected to identify potential biomarkers of response to nivolumab monotherapy and may then be applied to predict which patients are more likely to derive clinical benet from icis . 
nsclc , nonsmallcell lung cancer ; os , overall survival ; pd , progressive disease ; pd - 1 , programmed death - 1 ; pfs , progression - free survival . dream challenge challenge question 1 predict response to nivolumab , in terms of pfs , via an immune checkpointspecific model using clinical , demographic , and gene expression data challenge question 2 predict response to nivolumab , in terms of os , via an immune checkpointspecific model using clinical , demographic , and gene expression data challenge question 3 predict which patients will have a best overall response of pd checkmate 026 mature data set from a large randomized phase iii clinical trial in patients with nsclc nivolumab chemotherapy dream challenge impact ( cid : 129 ) provide biomarkers with predictive value for patients via a transparent and collaborative approach ( cid : 129 ) lay the foundation for understanding the utility of biomarkers in the setting of combination therapy patients . 
it is anticipated that some of the models may also have prognostic value for patients with nsclc . phenotype , thereby increasing their responsiveness to ici therapies . the challenge results should also provide a deeper understanding of biological mechanisms resulting in tumor resistance to treatment and assist in understanding why patients with advanced nsclc receiving nivolumab had similar efcacy outcomes to patients receiving chemotherapy in checkmate 026 . 
an improved understanding of the biological mechanisms behind resistance could pave the way to therapeutic interventions that immunologically activate tumors that do not display an immune - inltrated successful completion of this dream challenge will provide a model for future collaborations among industry , academia , and citizen scientists to discover determinants of response or resistance to immunotherapy , facilitating rapid development of clinically actionable biomarkers . 
szustakowski employment : bristol myers squibb stock and other ownership interests : bristol myers squibb research funding : bristol myers squibb patents , royalties , other intellectual property : i am an employee of bristol myers squibb , and an inventor on one or more pending patent applications , including applications for tmb as a predictive biomarker of immunotherapy travel , accommodations , expenses : bristol myers squibb parul doshi employment : bristol myers squibb stock and other ownership interests : bristol myers squibb travel , accommodations , expenses : bristol myers squibb justin guinney consulting or advisory role : astrazeneca research funding : celgene , genentech / roche , bristol myers squibb david p . 
carbone manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors references american cancer society : facts & figures 2020 reports largest one - year drop in cancer mortality . 
sambi m , bagheri l , szewczuk mr : current challenges in cancer immunotherapy : multimodal approaches to improve efcacy and patient response rates . j oncol 2019 : 4508794 , 2019 bristol myers squibb : yervoy ( ipilimumab ) [ package insert ]  . 
nat biotechnol 36 : 391 - 392 , 2018 saez - rodriguez j , costello jc , friend sh , et al : crowdsourcing biomedical research : leveraging communities as innovation engines . 
guinney j , wang t , laajala td , et al : prediction of overall survival for patients with metastatic castration - resistant prostate cancer : development of a prognostic model through a crowdsourced challenge with open clinical trial data . 
carbone dp , reck m , paz - ares l , et al : first - line nivolumab in stage iv or recurrent non - small - cell lung cancer . 
immunity 48 : 812 - 830.e814 , 2018 jiang p , gu s , pan d , et al : signatures of t cell dysfunction and exclusion predict cancer immunotherapy response . 
 acquired met exon 14 alteration drives secondary resistance to epidermal growth factor receptor tyrosine kinase inhibitor in egfr - mutated lung cancer ken suzawa , md , phd1 ; michael ofn , md1 ; adam j . 
in this study , we used targeted ngs with memorial sloan kettering integrated mutation proling of actionable cancer targets ( msk - impact ) , 12 immunohistochemistry , cell - free dna testing , and uorescence in situ hybridization to evaluate acquired resistance mediated by metex14 . 
furthermore , we used in vitro functional studies to establish metex14 as a novel mechanism of acquired resistance to egfr tkis . we used msk - impact , a large - panel ngs assay , to detect mutations , copy - number alterations , and select gene fusions involving up to 468 cancer - associated genes.12 metex14 was introduced into pc9 and h1975 cells as follows . 
briey , full - length metex14 was polymerase chain reaction amplied and subcloned into plenti - cmv - blast lentiviral vector ( plasmid 17451 ; addgene , cambridge , ma )  . 
the patient restarted erlotinib ( 100 mg daily ) with clinical and radiologic response for 12.5 months , at which time computed tomography revealed an increase in the dominant right upper lobe mass . 
 ( b - d ) representative images showing ( b ) baseline scan ( at time of progression during osimertinib monotherapy ) , ( c ) response to crizotinib monotherapy , and ( d ) response to combined crizotinib and osimertinib therapy . 
 ( * ) the patient initially received 1.4 months of combination osimertinib and savolitinib in a clinical trial , but treatment was changed to monotherapy with osimertinib because of intolerable toxicity . 
 ( ) as of 10 months of ongoing treatment with osimertinib and crizotinib . l858r mutation , no evidence of egfr t790m , and a new metex14 ( c.2899g.a ) alteration and met amplication ( fold change , 2.5 ; fig 1a ; appendix table a1 )  . 
therapy was changed to osimertinib with savolitinib daily ( clinicaltrials . gov identier : nct02143466 ) for 1.4 months , after which savolitinib was stopped because of toxicity and single - agent osimertinib 80 mg daily was continued . 
the patient continued to receive combination therapy with durable clinical and radiographic benet for more than 9 months . to dene the role of metex14 in mediating resistance to egfr tkis , we generated two isogenic egfr - mutant nonsmall - cell lung cancer ( nsclc ) cell models using pc9 ( exon 19 deletion ) and h1975 cells ( l858r and t790m ) by transduction with lentiviral vectors driving expression of metex14 ( fig 2a )  . 
western blot analysis showed that phosphorylation of egfr and its downstream effectors akt and erk was inhibited by osimertinib in pc9 cells transduced with empty plasmids ( pc9 empty ) , but phosphorylation of egfr , metex14 , and downstream effectors remained unaffected by osimertinib treatment in pc9 metex14 cells ( fig 2b )  . 
each condition was assayed in triplicate determinations ; data were normalized for cell number by measuring cell viability and shown relative to the control group ( mean 6 standard deviation )  . 
combination treatment with epidermal growth factor receptor ( egfr ) and met inhibitors is effective against met exon 14 skipping alteration ( metex14 ) induced drug resistance in egfr - mutant nonsmall - cell lung cancer cells . 
 ( c ) cells were treated with osimertinib ( 1 mm ) , crizotinib ( 1 mm ) , or a combination of the two agents for 3 hours , and lysates were subjected to immunoblotting . 
 ( e ) caspase 3 / 7 activity was analyzed in pc9 metex14 cells that were treated with osimertinib ( 1 mm ) , crizotinib ( 200 nm ) , or a combination of osimertinib ( 1 mm ) and crizotinib ( 200 nm ) for 48 hours . 
each condition was assayed in triplicate determinations , and data were normalized for cell number by measuring cell viability and are shown relative to the control group ( mean 6 standard deviation )  . 
pc9 metex14 cells showed a reduction in osimertinib - induced caspase 3 / 7 activation compared with pc9 - empty cells ( p , .001 ; fig 2d )  . 
together , these results indicate that metex14 induces resistance to osimertinib in egfr - mutant nsclc cells . investigated whether metex14 - mediated rewe next sistance to egfr tkis could be overcome by combination therapy with egfr and met inhibitors . 
as expected , crizotinib inhibited metex14 phosphorylation in pc9 metex14 cells ; however , phosphorylation of egfr , akt , and erk remained largely unchanged ( fig 3a ) , suggesting that egfr is still signaling effectively in pc9 metex14 cells . similarly , crizotinib was ineffective at modulating growth of egfr - mutated cell lines , with or without metex14 expression ( fig 3b )  . 
in agreement with these results , inhibition of egfr and met caused signicantly dual higher activation of caspase 3 / 7 ( fig 3e )  . discussion our study highlights the importance of serial and diverse molecular analyses , including ngs , to evaluate acquired alterations in the post - tki setting . 
although the patient did not respond to met - targeted therapy alone , the patient continued to have a durable clinical response to combination osimertinib and crizotinib , with stable disease by recist criteria and without notable toxicity . 
crizotinib restored sensitivity to egfr tkis ; however , crizotinib alone was not enough to suppress growth . two previous reports have demonstrated co - occurrence of egfr and metex14 mutations . 
in the rst report , three ( 0.2% ) of 1 , 590 patients with nsclc harbored concomitant egfr and metex14 mutations , one of whom received combination treatment with met ( volitinib ) and egfrtargeted therapies ( getinib ) , yielding a partial response.16 the second report noted one patient case of sarcomatoid carcinoma with egfr and metex14 alterations.17 in our msk - impact testing experience of 866 patient cases of egfr - mutant lung adenocarcinomas ( as of october 15 , 2018 ) , only two patients showed this combination of alterations : the patient described here , with acquired resistance , and a patient separate primaries at diagnosis . in whom the alterations were present the clinical benet of the combination of metand egfrtargeted therapies in patients with nsclc with acquired met amplicationmediated resistance to egfr tkis has trials , with varying tolerability been explored in clinical dependent upon the agents being combined.18 our ndings provide a rationale for future clinical evaluation of this combination approach , given its tolerability and efcacy in this case , for patients with egfr and metex14 mutations . furthermore , given the recent reports of secondary - site mutations in the met kinase domain , such as d1228n / v and y1230c , as mechanisms of acquired resistance to crizotinib in patients with metex14 , 19 it is plausible that these secondary met mutations will also emerge as mechanisms of resistance to the combination of osimertinib and crizotinib . we found that expression of metex14 upregulated phosphorylation of egfr itself , presumably via crossphosphorylation , because met is known to interact with egfr and drive the activity of egfr , 20 which resulted in blunting of the inhibition of egfr phosphorylation by egfr tkis . 
yu , romel somwar , marc ladanyi data analysis and interpretation : ken suzawa , michael ofn , adam j . schoenfeld , igor odintsov , daniel lu , alexander drilon , helena a . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter michael ofn consulting or advisory role : pharmamar travel , accommodations , expenses : bristol - myers squibb , merck sharp & dohme maria e . 
rudin consulting or advisory role : bristol - myers squibb , abbvie , seattle genetics , harpoon therapeutics , genentech / roche , astrazeneca , ascentage pharma , bicycle therapeutics , celgene , daiichi sankyo , ipsen , loxo , pharmamar , elucida oncology , bridge medicines research funding : abbvie / stemcentrx ( inst ) , viralytics ( inst ) , merck ( inst ) , daiichi sankyo ( inst ) alexander drilon honoraria : medscape , onclive , peervoice , physicians education resources , targeted oncology , more health , research to practice , foundation medicine , peerview consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pzer , blueprint medicines , genentech / roche , helsinn therapeutics , beigene , hengrui therapeutics , exelixis , bayer healthcare pharmaceuticals , tyra biosciences , verastem , takeda / ariad / millennium pharmaceuticals , bergenbio , more health patents , royalties , other intellectual property : wolters kluwer ( royalties for pocket oncology ) other relationship : merck , glaxosmithkline , teva pharmaceuticals industries , taiho pharmaceutical helena a . 
yu consulting or advisory role : astrazeneca , eli lilly research funding : clovis oncology ( inst ) , astrazeneca ( inst ) , astellas pharma ( inst ) , eli lilly ( inst ) , novartis ( inst ) , pzer ( inst ) , daiichi sankyo ( inst ) travel , accommodations , expenses : eli lilly other relationship : astellas pharma gregory j . 
 acquired met exon 14 alteration and resistance to egfr tkis references yu ha , suzawa k , jordan e , et al : concurrent alterations in egfr - mutant lung cancers associated with resistance to egfr kinase inhibitors and characterization of mtor as a mediator of resistance . 
clin cancer res 24 : 3108 - 3118 , 2018 ofn m , somwar r , rekhtman n , et al : acquired alk and ret gene fusions as mechanisms of resistance to osimertinib in egfr - mutant lung cancers . 
jama oncol 4 : 1527 - 1534 , 2018 bean j , brennan c , shih jy , et al : met amplication occurs with or without t790m mutations in egfr mutant lung tumors with acquired resistance to getinib or erlotinib . 
proc natl acad sci usa 104 : 20932 - 20937 , 2007 onozato r , kosaka t , kuwano h , et al : activation of met by gene amplication or by splice mutations deleting the juxtamembrane domain in primary resected lung cancers . 
j thorac oncol 4 : 5 - 11 , 2009 kong - beltran m , seshagiri s , zha j , et al : somatic mutations lead to an oncogenic deletion of met in lung cancer . 
cancer res 66 : 283 - 289 , 2006 paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
cancer discov 5 : 842 - 849 , 2015 drilon ae , camidge dr , ou s - hi , et al : efcacy and safety of crizotinib in patients ( pts ) with advanced met exon 14 - altered non - small cell lung cancer ( nsclc )  . 34 , 2016 ( suppl ; abstr 108 ) drilon a , ou s - h , clark j , et al : antitumor activity and safety of crizotinib in patients with met exon 14 - altered advanced non - small cell lung cancer . 
felip e , horn l , patel jd , et al : tepotinib in patients with advanced non - small cell lung cancer ( nsclc ) harboring met exon 14 - skipping mutations : phase ii trial . 
wolf j , han j , nishio m , et al : geometry mono - 1 : phase ii , multicenter study of met inhibitor capmatinib ( inc280 ) in egfr wt , met - dysregulated advanced nsclc . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
pennell na , neal jw , chaft je , et al : select : a phase ii trial of adjuvant erlotinib in patients with resected epidermal growth factor receptormutant nonsmallcharacteristics . 
borsu l , intrieri j , thampi l , et al : clinical application of picodroplet digital pcr technology for rapid detection of egfr t790m in next - generation sequencing libraries and dna from limited tumor samples . 
ou si , govindan r , eaton kd , et al : phase i results from a study of crizotinib in combination with erlotinib in patients with advanced nonsquamous non - small cell lung cancer . 
 future of evidence synthesis in precision oncology : between systematic reviews and biocuration precision medicine refers to the tailoring of interventions to patients using approaches that go beyond traditional clinical characteristics ( eg , age , sex , disease , symptoms , and medical history ) by considering biomarkers consisting of genetic characteristics or molecular profiles.1 in particular , precision oncology ( po ) 2 includes both the development of novel cancer therapies targeting specific changes that occur in some individuals but not others ( eg , inherited mutations or somatic mutations that arise in the carcinogenesis process ) and the stratification of individuals according to existing interventions ( eg , via screening programs tiered by genetic risk or chemotherapies predicted to work for certain molecular profiles ) , which is expected to show improved outcomes in the resulting subgroups . 
 herein , we discuss two approaches for synthesizing evidence for or against the use of specific po interventions , namely , systematic reviews ( srs ) and biocuration , and argue that their engagement with each other could facilitate the timely delivery of appropriate po interventions . cancer is known to be highly heterogeneous , and clinical responses differ among patients . 
 po thus includes a wide variety of applications , including both the use of targeted therapies against particular changes occurring in individual tumorssuch imatinib against the bcr - abl fusion in chronic myeloid leukemia , 3 vemurafenib4 and dabrafenib5 against specific braf mutations in melanoma , and trastuzumab against her2 - postive breast cancer6and the assignment between existing therapy classes via biomarkers that are not direct drug targets . 
this can be based either on the activation of certain pathways , as in the case of egfr inhibitors in kras - wild type colon cancer , 7 , 8 or on gene expression signatures or other molecular characteristics ( ie , oncotype dx test for breast cancer , used to predict recurrence and likely benefit of chemotherapy ) .9 , 10 these biomarkers are well - established and have been approved by the us food and drug administration for specific cancer types . the biomarkers discussed in the previous paragraph are classified as having the highest level of evidence for clinical use in society guidelines ( eg , those jointly put forward by the association for molecular pathology , asco , and the college of american pathologists ) .11 to be meaningful for clinical decision making , biomarkers should have high predictive performance ( ie , they can be used to stratify patients into treatment groups with differential outcomes )  . 
most research to date , however , has assessed whether biomarkers are prognostic ( ie , are associated with a clinical outcome for untreated or standardof - care patients ) .12 it is often the case that the supporting literature includes few if any randomized control trials.13 as a result , lower levels of evidence may be assigned , eg , to biomarkers that predict response to a treatment based on well - powered studies evaluated by expert consensus or that predict response in a different tumor type than that being studied . many conceptual frameworks have been proposed to facilitate clinical decision making by helping end users ( especially patients and clinicians ) assess the evidence for or against the use of medical tests , including biomarkers.14 , 15 with minor variations , the different frameworks involve a stepwise approach that starts with analytic validity ( laboratory reproducibility ) , proceeds to clinical validity ( predictive accuracy , including sensitivity , specificity , and positive and negative predictive values ) and clinical utility ( use of the biomarker leads directly to improvements in outcomes like survival and quality of life ) , and eventually assesses the cost effectiveness of the biomarker . 
comparison of key features of systematic reviews and biocuration feature systematic reviews biocuration overall approach top down ; starts with a key scientific question and develops evidence base around it either top down or bottom up ; starts with a number of scientific questions or allows individual articles to be curated and slotted into categories evidence assessment exhaustive literature searches and systematic multiple frameworks exist assessment of evidence presence of bias systematic assessment of the risk of bias higher chance for bias by selecting studies with delivery approach peer - reviewed article or whitepaper research approach team usually assembled at the start of the project often relies on crowdsourcing and expert review of updating significant lag closer to real time , depending on availability of authors or curators multidisciplinary teams , often exclude or reduce role of primary study authors or subject matter experts due to risk of bias scientists and clinicians , who are frequently subject matter experts , from a variety of fields , and often with an expert panel to resolve conflicting interpretations significant findings database of entries may include summary of findings and links to original studies and other resources entries curators as with all tests in clinical practice , tests related to biomarkers are delivered within given health care settings , and currently , little structured evidence exists in regard to how po can successfully be implemented for particular sets of patients , with different degrees of access to health care , across diverse health care systems . 
the first is the traditional evidence appraisal that applies the well - established concepts of evidence - based medicine ( ebm ) .17 , 18 ebm integrates a physicians clinical experience with scientific evidence that has undergone an sr , which involves extensive surveying of the literature followed by a synthesis of the primary studies.19 the second is biocuration , which refers to the distillation and integration of biologic information from scientific literature and large data sets using databaseor research field specific , controlled vocabularies or ontologies ; it is a cornerstone of bioinformatics.20 both disciplines have the same overarching goal of bringing to patients only the interventions proven to be effective by carefully balancing benefits and harms , doing so in different ways ; srs start with a particular question and systematically develop the evidence base around it , whereas biocuration may be either top - down or bottom - up and usually involves more real - time updating . 
we compare key aspects of these two approaches in table 1 and summarize important feature of specific curated databases in appendix table a1 . the goal of srs is to allow a comprehensive and global view of the available evidence base on a particular question of interest by analyzing primary studies that meet prespecified eligibility criteria via explicit , reproducible methodologies that minimize bias . 
the typical steps involved in an sr include identification of the clinical question , specification of eligibility criteria , systematic search for all studies that meet these criteria , extraction of evidence from eligible studies and assessment of their methodologic rigor , and analysis and qualitative and / or quantitative synthesis ( meta - analysis ) of the extracted data.19 an sr is typically structured around the picots elements : the population toward which the findings will be applicable , the intervention , the comparisons being performed , the clinical outcomes , the timing of the eligible studies , and the clinical setting . 
during the course of decades , a toolbox of methods has been developed in srs and ebm to evaluate key elements of published studies including systematic biases , statistical precision , applicability to a target clinical setting , and others.21 - 23 evidence for specific interventions on the basis of supporting srs is generally considered strong . 
 clinical practice guidelines on the basis of srs that support the use of a genomic test as tier one ( ready to implement in clinical practice24 ) and those that are not based on srs as tier two ( may be useful in the context of informed clinical decision making24 )  . in general , sr teams are multidisciplinary , consisting of clinicians , content experts , methodologists , statisticians , and librarians . 
because researchers may often be influenced by their own investment in the field when interpreting the evidence base , 25 ideally , parties involved in a sr should have no personal vested interests in the topic of the sr . 
although content experts are critical for the clinical interpretation of primary studies and for putting them in context with the broader evidence , their role as authors in srs has been debated.26 however , since srs have various degrees of complexity , relevant sponsors often make decisions on a case - by - case basis by thoroughly reviewing the potential conflicts of individual researchers . 
for example , the agency for healthcare and research quality evidence - based practice centers program has a set of guidelines for how different types of conflicts should be handled and alleviated.27 given that precision medicine is a relatively new and rapidly evolving field with potentially more complex statistical analyses and contextual questions compared to traditional studies , including and relying on content experts is more critical . synthesis of evidence from po studies encounters a number of specific challenges . 
consider for instance a cochrane review of first - line treatments in individuals with egfr - mutated noncurable stage iiib to iv nonsquamous nonsmall - cell lung cancer , which included 19 rcts.28 the overall conclusion was that the tyrosine kinase inhibitor therapies ( erlotinib , gefitinib , and afatinib ) led to improved progression - free survival but not to improved overall survival , whereas the monoclonal antibody cetuximab did not show any improved outcomes . 
while this study included 19 rcts total , comparing targeted therapies to chemotherapy or best supportive care , the number of rcts conducted for each therapy was between two and eight and the study designs , outcome measures , and analyses performed and reported varied . 
srs have also identified existing evidence gaps for other prevision medicine interventions , such as the lack of robust evidence for tailoring smoking cessation interventions on the basis of germline genetic variation.29 many issues with the sr of evidence for po interventions will be solved in time , as more studies accumulate , but it is important to note that the desire for new therapies may be at a historical high given the stated promise of precision medicine and po in particular . 
however , another challenge that will linger is that the definition of precision medicine will continue to make it difficult to satisfy the picots framework as , for example , more drugs are tested separately in different subsets of patients ( eg , if the same biomarker is considered for different tumor types ) or molecular tests rapidly evolve to add more biomarkers or change how they are tested ( eg , protein expression , gene expression , or dna amplification ) .13 new rct designs such as umbrella and basket trials are now being implemented to meet some of these challenges . 
although other study designs may provide additional valuable information on specific treatments , the question of clinical utility , in particular , is difficult to answer in the absence of evidence from rcts . biocuration identifies and summarizes biomedical results , including potentially those from srs , into bioinformatic databases , often by using controlled vocabularies and prespecified standards.20 a text summary of the evidence related to specific scientific questions may also be included , along with links to the original studies or other resources . 
in particular , medical curation focuses on disease associations and genetic factors and includes efforts like the omim ( online mendelian inheritance in man ) database30 as well as specialized databases for particular genes , variants , and diseases . 
clinvar , a public archive of relationships among medically important germline and somatic variants and human phenotypes , was launched in april 2013.31 biocuration generally provides more immediate updating than formal srs , but the lack of a unified systematic framework may lead to only partial or inconsistent results . 
 curators , resulting in a wealth of information but also in issues such as contradictory interpretations and many variants of uncertain significance.32 the clingen ( clinical genome resource ) initiative aims to resolve some of these problems and answer the critical questions of clinical validity , disease causality ( pathogenicity ) , and clinical actionability by standardizing data collection and sharing and implementing an approach for consensus among expert curators.32 many other cancer - specific databases now exist for synthesizing evidence for po approaches , 33 - 37 leading clingen to recently develop recommendations and guidelines for defining cancer somatic variants on the basis of their diagnostic , prognostic , and predictive roles , using evidence of their significance and clinical utility.38 in a translational field such as po , where molecular genomics and clinical practice come together , a particular challenge for biocuration is that each content area has its own detailed terminology ( eg , specific diseases and syndromes can be described using icd - 10 codes39 and snomed terms40 )  . 
however , mapping these terminologies to specific causal mutations , as well as to biomarkers and tratments , can often be a challenge . biocurators come from a wide variety of backgrounds , usually in biology , biochemistry , or medical genetics , and increasingly have interdisciplinary training that includes computer and information sciences , with subject matter experts playing an important role in the field of biocuration.20 , 41 a growing number of clinical laboratories in hospitals and community clinics are now also conducting molecular diagnostic testing to identify sequence variants and inform treatment decisions for patients , in which case the curation is often performed by molecular pathologists as well as clinicians . 
the expert panels used by resources such as clingen to resolve conflicting interpretations and curate variants of unknown significance include medical professionals , medical geneticists , clinical laboratory diagnosticians and molecular pathologists that have a long standing scope of work in the disease gene in question . an example of a curated cancer database is the recently released civic ( clinical interpretation of variants in cancer ) database , 36 which provides associations between drugs and genes or variants in specific cancer types . 
however , the authors state the presence of a bias toward positive associations with treatment outcomes ( 91% of records show support for the use of a therapy ) , which illustrates the absence of a systematic , unbiased framework for identifying the evidence base . 
given that civic considers many different types of studies and that studies of cancer drugs may have many different designs , it is true that it would be extremely challenging to have a fixed list of terms that would be applicable to all studies and easily translatable into picots terminology . in general , literature searches for srs are typically more exhaustive and thorough than for curated databases , where eligible studies tend to be identified by experts in a given field . 
 although currently this may have little direct impact on identifying relevant studies for biocuration , given the small number of clinical po publications , this will eventually become a major issue in the next years , because the field will need to deal with increasing amounts of published and unpublished evidence . 
srs also tend to have more well - defined a priori eligibility criteria that a study has to meet to be considered in the evidence synthesis ; in contrast , biocuration approaches show more variability and rely more on individual experts in the field . 
although biocuration currently lacks a standardized and widely accepted framework to assess the quality of published evidence , several efforts are under way to change this.38 , 42 - 44 beyond trying to develop standardized frameworks for biocuration , a number of other approaches for improving curated databases have been considered , including the use of specific incentives . 
the emphasis on a systematic survey of the literature which includes non - significant results that is present in srs is also not an explicit part of the biocuration philosophy . 
for example , if the ebm community engages the biocuration community , they may find ways of incorporating more elements of the picots framework into existing and future databases . there is often a tension between systematic , unbiased syntheses and assessments versus timely and accessible curated information , and the highly promising field of po is a clear example that shows the difficulties in finding a good solution that considers both of these dimensions . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . approaches , and products , instead of continuing to proceed on parallel paths . 
curated databases will continue to be an initial first stop for many researchers and clinicians , especially because srs may lag years behind current studies , and decisions often need to be made in cases where srs are lacking . 
 however , more training is needed for users to understand that , for example , a higher risk of bias exists for finding more significant associations when consulting a curated po database than when using a sr . 
obrien sg , guilhot f , larson ra , et al ; iris investigators : imatinib compared with interferon and low - dose cytarabine for newly diagnosed chronic - phase chronic myeloid leukemia . 
hauschild a , grob j - j , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
slamon dj , leyland - jones b , shak s , et al : use of chemotherapy plus a monoclonal antibody against her2 for metastatic breast cancer that overexpresses her2 . 
de roock w , piessevaux h , de schutter j , et al : kras wild - type state predicts survival and is associated to early radiological response in metastatic colorectal cancer treated with cetuximab . 
calonge n , klein rd , berg js , et al : recommendations from the egapp working group : does the use of oncotype dx tumor gene expression profiling to guide treatment decisions improve outcomes in patients with breast cancer ?  . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
panagiotou oa , ioannidis jp : primary study authors of significant studies are more likely to believe that a strong association exists in a heterogeneous meta - analysis compared with methodologists . 
greenhalgh j , dwan k , boland a , et al : first - line treatment of advanced epidermal growth factor receptor ( egfr ) mutation positive non - squamous non - small cell lung cancer . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
hunter je , irving sa , biesecker lg , et al : a standardized , evidence - based protocol to assess clinical actionability of genetic disorders associated with genomic variation . 
strande nt , riggs er , buchanan ah , et al : evaluating the clinical validity of gene - disease associations : an evidence - based framework developed by the clinical genome resource . 
uniprot is not disease focused ; omim , clinvar , and clingen are disease agnostic ; the remaining databases are specific to cancer . abbreviations : asco , american society of clinical oncology ; civic , clinical interpretation of variants in cancer ; clingen , clinical genome resource ; cosmic , catalogue of somatic mutations in cancer ; fda , us food and drug administration ; nccn , national comprehensive cancer network ; nih , national institutes of health ; omim , online mendelian inheritance in man ; po , precision oncology . 
nucleic acids res 43 : d204 - d212 , 2015 . landrum mj , lee jm , benson m , et al : clinvar : public archive of interpretations of clinically relevant variants . 
nucleic acids res 44 : d862 - d868 , 2016 forbes sa , beare d , boutselakis h , et al : cosmic : somatic cancer genetics at high - resolution . 
nucleic acids res 45 : d777 - d783 , 2017 . taylor ad , micheel cm , anderson ia , et al : the path ( way ) less traveled : a pathway - oriented approach to providing information about precision cancer medicine on my cancer genome . 
in the clinical pharmacogenetics implementation consortium guideline , fluoropyrimidine treatment in homozygous dpyd variant carriers is discouraged , which implies that a potentially effective anticancer therapy is withheld from these patients.5 in this article , six unique patients with a homozygous or compound heterozygous dpyd variant allele genotype who were treated with tailored fluoropyrimidine treatment are described . 
analyses were part of individual patient care , so institutional review board approval was not applicable . genotyping results showed a homozygous or compound heterozygous dpyd genotype , and the functional effects of these genotypes were uncertatherefore , pretreatment dpd activity was measured in peripheral blood mononuclear cells ( pbmcs )  . 
dpd activity was used to reach an individualized dose , in which the percentage of remaining dpd activity was used as guideline for the starting dose ( expressed as percentage of the originally planned dose )  . pharmacokinetic analyses in three of six patients were performed to investigate whether applied dose reductions were adequate . 
pretreatment plasma uracil , the endogenous dpd substrate , and dihydrouracil levels were quantified ; results were unknown before the start of treatment . results clinical course of treatment patient characteristics are listed in table 1.6 - 9 linda m . 
therefore , it was decided to drastically reduce the capecitabine dose from 2 , 300 mg ( 1 , 000 mg / m2 ) twice daily to 150 mg twice daily ( 6.5% of planned dose ) and to start with capecitabine monotherapy . 
the adverse events resolved within 1 week ( neutropenia ) to 2 months ( diarrhea , mucositis )  . after a 2 - month period without any anticancer therapy , the patient had fully recovered , and monotherapy with capecitabine was restarted . 
on the basis of the severe toxicity and the pharmacokinetic results of the first cycle , the dose was reduced more to 150 mg once every 5 days ( ie , 0.65% of originally planned dose )  . 
this female patient with locally advanced colorectal carcinoma had a planned treatment that consisted of neoadjuvant chemotherapy ( capecitabine 825 mg / m2 twice daily , or 1 , 500 mg ) combined with radiotherapy ( 5 - week schedule )  . pretreatment dpyd screening revealed that the patient was homozygous for c.2846a.t ; dpd activity was reduced to 29% . 
it was decided to reduce the capecitabine dose to 500 mg once daily ( ie , 17% of planned doseslightly lower than recommended dose of 29% on the basis of dpd activity , as decided by physician and patient )  . 
dpd activity was reduced to 45% . remaining dpd activity was more than 50% reduced , so it was considered likely that this patient was a compound heterozygous carrier ( variants present on different alleles )  . 
in the first cycle , capecitabine was reduced to 1 , 800 mg daily ( 51% of planned daily dose of 3 , 500 mg ; 1 , 750 mg / m2 ) , which was tolerated without toxicity . 
however , the patient developed grade 2 thrombocytopenia after 8 days , and the daily capecitabine dose was adjusted to 1 , 000 mg for the rest of the cycle . platelets increased again until normal values were reached . 
after three cycles , disease progression was established , and capecitabine treatment was discontinued . pharmacokinetic results in all three patients , additional pharmacokinetic measurements were performed ( fig 1 )  . 
for patient 1 , only levels of capecitabine and of the metabolites 59 - deoxy - 5 - fluorocytidine , 59 - deoxy5 - fluorouridine , and fu could be quantified ; other fu metabolites were not detectable . 
results of noncompartmental analysis of the pharmacokinetic results in plasma are listed in table 2 and include values normalized to control values.10 in patient 1 , fu exposure was highly increased : the mean area under the plasma concentration - time curve ( auc ) of fu was 4 , 024 ng 3 h / ml , which is 10 times higher than in other pharmacokinetic studies with capecitabine.10 - 13 these results were used for the decision to lower the dose 10 - fold in the second cycle . baseline uracil and dihydrouracil levels are listed in table 1 . 
results of urine analysis for patient 1 are shown in appendix figure a1 . discussion to our knowledge , this is the first report to describe prospectively identified patients , who are homozygous or compound heterozygous for dpyd variants , who could be treated safely with fluoropyrimidines . 
for all three patients , the results after the first intake of capecitabine are depicted . capecitabine patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) 5 ' - dfcr patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) time ( h ) 5 ' - dfur time ( h ) 5 - fu patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) 5 , 000 4 , 000 3 , 000 2 , 000 1 , 000 4 , 000 3 , 000 2 , 000 1 , 000 2 , 500 2 , 000 1 , 500 1 , 000 2 , 500 2 , 000 1 , 500 1 , 000 1 , 200 time ( h ) fuh2 time ( h ) fupa patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) time ( h ) time ( h ) fbal patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) time ( h ) pretreatment identification of the patient homozygous for dpyd * 2a with complete dpd deficiency saved this patient from receipt of a full fluoropyrimidine dose , which most likely would have been fatal . 
in patients who are not dpd deficient , fluoro - b - alanine is the major urinary metabolite , 13 , 20 whereas this metabolite was not present in the urine analyzed in the case presented in this paper . 
for example , mir27a polymorphisms could play a role in variation of dpd activity , because these polymorphisms reduce dpd activity.26 , 27 in conclusion , we showed that fluoropyrimidine treatment in homozygous or compound heterozygous dpyd variant allele carriers is feasible and that therapy does not have to be withheld . 
van der veldt consulting or advisory role : ipsen ( inst ) , roche ( inst ) , bristol - myers squibb ( inst ) , pfizer ( inst ) , msd oncology ( inst ) travel , accommodations , expenses : roche paul hamberg no relationship to disclose andr e b.p. 
bioanalysis 7 : 519 - 529 , 2015 van kuilenburg ab , van lenthe h , tromp a , et al : pitfalls in the diagnosis of patients with a partial dihydropyrimidine dehydrogenase deficiency . 
deenen mj , meulendijks d , boot h , et al : phase 1a / 1b and pharmacogenetic study of docetaxel , oxaliplatin and capecitabine in patients with advanced cancer of the stomach or the gastroesophageal junction . 
judson ir , beale pj , trigo jm , et al : a human capecitabine excretion balance and pharmacokinetic study after administration of a single oral dose of 14c - labelled drug . 
van kuilenburg ab , muller ew , haasjes j , et al : lethal outcome of a patient with a complete dihydropyrimidine dehydrogenase ( dpd ) deficiency after administration of 5 - fluorouracil : frequency of the common ivs14 + 1g.a mutation causing dpd deficiency . 
meinsma r , fernandez - salguero p , van kuilenburg ab , et al : human polymorphism in drug metabolism : mutation in the dihydropyrimidine dehydrogenase gene results in exon skipping and thymine uracilurea . 
van kuilenburg ab , meijer j , mul an , et al : intragenic deletions and a deep intronic mutation affecting pre - mrna splicing in the dihydropyrimidine dehydrogenase gene as novel mechanisms causing 5 - fluorouracil toxicity . 
offer sm , butterfield gl , jerde cr , et al : micrornas mir - 27a and mir - 27b directly regulate liver dihydropyrimidine dehydrogenase expression through two conserved binding sites . 
froehlich tk , amstutz u , aebi s , et al : clinical importance of risk variants in the dihydropyrimidine dehydrogenase gene for the prediction of early - onset fluoropyrimidine toxicity . 
int j cancer 136 : 730 - 739 , 2015 patients were treated at three different institutes in the netherlands ( the netherlands cancer institute , amsterdam ; erasmus medical center , rotterdam ; fransciscus gasthuis & vlietland , rotterdam )  . 
toxicity was scored according to the common terminology criteria for adverse events , version 4.03. dpyd genotyping genomic dna was isolated from peripheral blood cells , and screening for the dpyd variants dpyd * 2a ( ivs14 + 1g.a , rs3918290 ) , c.2846a.t ( rs67376798 ) , c.1679t.g ( dpyd * 13 , rs55886062 ) , and c.1236g.a ( rs56038477 ) was performed by using standard operating procedures in two different institutes ( the netherlands cancer institute , amsterdam , and erasmus medical center , rotterdam )  . 
in the netherlands cancer institute , screening for dpyd variants was performed with the roche lightcycler 480ii platform ( roche diagnostics , almere , the netherlands ) by using commercially available probes and primers ( tib molbiol , berlin , germany ) , and results were confirmed by direct sequencing . 
at the erasmus medical center , each sample was genotyped on two different platformstaqman ( with predefined drug - metabolizing enzyme [ dme ] assays ) and pcrrestriction fragment length polymorphism ( rflp ) assaysto allow checks for potentially wrong genotyping . 
both laboratories participated during the study in the dutch national quality control program for dpyd proficiency testing , in which all four dpyd variants were included . dihydropyrimidine dehydrogenase activity in peripheral blood mononuclear cells dihydropyrimidine dehydrogenase ( dpd ) activity was measured in peripheral blood mononuclear cells ( pbmcs ) , isolated from a baseline ( pretreatment ) peripheral blood sample . 
one of two comparable validated methods by van kuilenburg et al7 or pluim et al6 was used ; both used radiolabeled thymine ( 14c - labeled thymine or 3h - labeled thymine ) as a substrate and consisted of high - performance liquid chromatography ( hplc ) with online radioisotope detection and with liquid scintillation counting . 
analytes were extracted by protein precipitation ; chromatographic separation was performed on an acquity ultra - performance liquid chromatography hss t3 column ( acquity waters , milford , ma ) and were analyzed with ms / ms with an electrospray ionization source ( jacobs ba et al : j pharm biomed anal 126 : 75 - 82 , 2016 )  . 
all samples were measured at one institute ( the netherlands cancer institute )  . pharmacokinetic measurements peripheral blood samples for patient 1 were obtained for pharmacokinetic analysis on cycle 1 , day 1 ( c1d1 ) ; cycle 2 , day 1 ( c2d1 ) ; and cycle 2 , day 16 ( c2d16 )  . 
 results dihydrouracil - uracil levels capecitabine intake ( at predose , and at 15 minutes , 30 minutes , 1 hour , 2 hours , 3 hours , 4 hours , 6 hours , 8 hours , and 10 hours after capecitabine intake )  . 
for patients 2 and 3 , samples were collected only on c1d1 , on the same time points as for patient 1 , except for the latest time point ( the sample 10 hours after capecitabine intake was not collected for patient 2 , and the last sample was collected at 12 hours instead of at 10 hours for patient 3 )  . 
for patients 2 and 3 , pharmacokinetic results were not known during treatment , because samples were analyzed after treatment had finished . capecitabine and its metabolites , 59 - deoxy - 5 - fluorocytidine ( 59 - dfcr ) , 59 - deoxy - 5 - fluorouridine ( 59 - dfur ) , fluorouracil ( fu ) , dihydro - 5 - fluorouracil ( fuh2 ) , a - fluoro - ureidopropionic acid ( fupa ) , and fluoro - b - alanine ( fbal ) , were quantified by using hplc coupled to electrospray ms / ms . 
two individual validated assays were used : one for the simultaneous quantification of capecitabine , 59 - dfcr and 59 - dfur and another for fu , fuh2 , fupa , and fbal ( deenen mj et al : j chromatogr b analyt technol biomed life sci 913 - 914 : 30 - 40 , 2013 )  . 
all pharmacokinetic samples were measured at the same institute ( the netherlands cancer institute )  . together with the sample for dpd activity in pbmcs , a pretreatment plasma sample was taken to measure uracil and dihydrouracil levels ( table 1 )  . 
for patients 2 and 3 , uracil levels were increased compared with reference levels ( a value of 28.7 ng / ml for patient 2 and of 35.6 ng / ml for patient 3 ) , and both values were within the top 1% of reference values . 
dihydrouracil levels were in the normal range for patients 2 and 3 compared with reference levels . other homozygous dpyd variant allele carriers three additional patients with a homozygous dpyd variant genotype were identified during routine dpyd screening ( table 1 )  . 
it is unclear why there is a relatively high variation of the effect of this genotype on dpd phenotype in patients , and more research on this variant is advised . in addition , one patient with a homozygous c.2846a.t genotype ( patient 4 ) was identified . 
according to the calculated dpd activity score , as described by henricks et al , 4 it could be concluded that a 50% dose reduction would be appropriate for homozygous c.2846a.t carriers , because a 25% dose reduction is recommended for heterozygous carriers of this variant . 
with the recent increase in integrative clinical sequencing for pediatric patients with cancer , our understanding of the dicer1 syndrome continues to evolve , as new and rare pathogenic variants are reported . 
as the frequency of integrative clinical sequencing increases , discussions regarding challenges encountered in the interpretation of sequencing results are essential to continue to advance the eld of cancer predisposition . 
the purpose of this work was to identify patients with somatic and / or germline dicer1 variants in our patient population and to discuss sequencing interpretation and the clinical recommendations that result from the integrative clinical sequencing results . methods patients were enrolled in the peds - mioncoseq study . 
2019 by american society of clinical oncology introduction the dicer1 gene is located on chromosome 14 ( 14q32.13 ) and encodes the dicer protedicer is an rnase iii enzyme functioning in micro - rna ( mirna ) processing . 
mirnas are single - stranded , noncoding rnas that target mrnas by binding to complementary mrna sequences , increasing their degradation and suppressing translation.1 through its ability to regulate mirna processing , dicer1 plays a critical role in cellular mrna expression and in early development.1 , 2 with respect to human disease , more than 130 germline and 95 somatic dicer1 mutations have been reported.2 the majority of somatic dicer1 mutations are hotspot mutations in the rnase iiib domain ; however , somatic mutations are reported to be elsewhere , including the domain of unknown function.2 germline dicer1 mutations have been reported in all of the 10 major domains and spanning regions.3 dicer1 syndrome , caused by pathogenic variants in dicer1 , is an inherited condition associated with an increased risk of developing pleuropulmonary blastoma ( ppb ) , multinodular goiter , cystic nephroma , sertoli - leydig cell tumors of the ovary , and other rare tumors . 
 bailey et al context the goal of this work was to describe sequencing interpretation challenges and clinical recommendations in patients with dicer1 somatic and / or germline variants identied on integrative sequencing . this work suggests that postzygotic mosaicism may play a signicant role in the development of dicer1 - associated tumors . furthermore , we report a patient with a dicer1 variant of uncertain signicance whose clinical course and response to treatment was highly unusual , suggesting this variant could be clinically meaningful . the use of integrative clinical sequencing has signicantly expanded in pediatric oncology in the past 5 years . 
reports also include a dicer1 syndrome family with both somatic and germline pathogenic variants found in family members with different types of dicer1 - related cancers.15 to our knowledge , our group reported the rst real - time , integrative clinical sequencing ( ics ) study in the pediatric oncology population in 2015.16 since that time , the role of real - time ics of tumors and germline samples in the pediatric oncology population has continued to expand.17 - 19 however , the interpretation of genetic variants and their translation into the clinical setting remain challenging . when sequencing results identify germline dicer1 variants in pediatric oncology patients , counseling and screening implications for family members are affected . 
the purpose of this work was to highlight ( 1 ) somatic and / or germline dicer1 pathogenic variants identied in our pediatric oncology sequencing cohort , ( 2 ) challenges encountered with sequencing result interpretation with respect to dicer1 , and ( 3 ) current patient and family screening recommendations . methods patients the pediatric patients described were treated at c.s. 
patients were enrolled in a prospective , institutional review boardapproved ics trial ( peds - mioncoseq ) 16 and underwent paired tumor / normal whole - exome sequencing and tumor transcriptome sequencing . 
peds - mioncoseq is an ongoing precision oncology cohort and focused on enrolling highrisk , relapsed / refractory , and rare pediatric and young adult ( younger than 25 years of age ) patients with cancer . integrative clinical sequencing specics of the sequencing procedure and bioinformatics analyses have been previously described.16 briey , germline sequence and copy number variants , as well as somatic mutations , copy number alterations / variants , insertions and deletions , gene fusions , and gene expression , were identied.20 , 21 pathogenicity of germline variants was determined through a review of the published literature and publically available databases ( ie , clinvar )  . clinical relevance of somatic variants was investigated using an integrated approach incorporating technical considerations ( eg , recurrence , variant allele fraction , expression levels , and predictive algorithms for pathogenicity ) , variant - specic information ( ie , clinvar , published literature , and curated gene - specic resources ) , and published correlations of drug and variant sensitivity proles . results four patients with somatic and / or germline dicer1 pathogenic variants were identied among the rst 300 patients enrolled in peds - mioncoseq ( table 1 )  . 
we detail the patient presentations , diagnoses , variant terpretation , and clinical actions taken on the basis of these results . patient 1 : a patient with a hotspot somatic variant and a germline pathogenic dicer1 variant patient 1 presented at 3 years of age with a history of left arm and abdominal paan abdominal x - ray was performed , and a left - sided pleural effusion was incidentally noted . 
surveillance for dicer1 - related tumors was initiated for the patients sister ( 6 years old at time of genetic testing ) and included baseline chest ct ( to screen for ppb ) , with a chest x - ray at 8 years of age , annual ultrasound scans of the abdomen and neck ( to screen for ovarian and kidney tumors and thyroid tumors , spectively ) , and annual serum markers to screen for ovarian tumors . 
the father received an annual ultrasound scan of the thyroid gland only , because dicer1 - associated cancers affecting males primarily present in childhood . the bony metastatic lesions completely responded to chemotherapy , and the patient underwent primary mass resection followed by two more cycles of chemotherapy . the resected mass showed mostly viable ppb , with malignant cartilaginous nodules overrun by an anaplastic prostate cancer multinodular goiter s / p thyroidectomy prostate cancer fig 1 . 
patient 1 continued to have disease progression despite chemotherapy , and the decision was made to transition to comfort care . patient 2 : a patient with a germline dicer1 variant of unknown signicance patient 2 initially presented at 3 years of age with a left lower quadrant / pelvic mass . 
remarkably , the patient had an excellent response to therapy and was deemed disease free at age 5 years . at 19 years of age , patient 2 presented to our medical center with severe abdominal and back paimaging revealed concern for new / recurrent widely metastatic disease , because a pelvic mass was noted along with multiple spine and liver lesions . 
palliative radiation was initiated for pain control , and the patient enrolled in the peds - mioncoseq study . sequencing results revealed a germline dicer1 variant of uncertain signicance ( vus ) ( table 1 )  . 
sequencing of the original tumor ( from 3 years of age ) was attempted for comparison / to determine whether this was a metachronous tumor ; however , only sparse , poor - quality material was available , and sequencing could not be performed . 
although vuss are not disclosed per the pedsmioncoseq protocol , at times , a recommendation for clinical germline genetic testing may be made for patients with striking personal / family histories . 
the majority of vuss will be reclassied as likely benign / benign , 22 but for those that are reclassied as likely pathogenic / pathogenic , there can be signicant implications for patients and their relatives . 
patient 2 died at 20 years of age as a result of metastatic disease . patient 3 : a patient with low - level dicer1 mosaicism patient 3 initially presented at 22 months of age with a leftsided pneumonia and pneumothorax . 
a persistent air - lled cystic cavity was present in the left chest and observed with imaging for approximately 3 months before a diserial agnosis of ppb was made after resection of the left lower lobe of the lung . 
regardless , clinical germline genetic testing of dicer1 was recommended but not pursued because of the out - of - pocket cost . approximately 6 months later , patient 3 was enrolled in the peds - mioncoseq study . 
 ( a ) he image ( 40 ) of the original tumor showing mixed morphology with alveolar pattern in the top half and more abundant rhabdomyoblastic differentiation in the lower half . ( b ) he image ( 400 ) of the late recurrence tumor showing spindle - shaped and round cell tumor cells with focal rhabdomyoblastic differentiation . 
as such , no signicant somatic copy number variations , point mutations , indels , or gene fusions were able to be called . no germline variants were considered reportable at this time . this patient also enrolled in the national institutes of healths ( nihs ) pleuropulmonary blastoma dicer1 syndrome study , which includes germline and somatic sequencing , approximately 1 year after initial diagnosis . germline sequencing identied a mosaic germline dicer1 pathogenic variant ( table 1 ; fig 3 ) in 2% of the allelic reads in the patients blood sample . 
both parents enrolled in the study , and their germline testing was negative for the dicer1 pathogenic variant , consistent with the low - level mosaicism detected in the patients blood sample . 
this somatic variant is commonly seen in dicer1 syndromeassociated tumors and involves the rnase iiib domain of dicer1 . analysis of the raw data available from the peds - mioncoseq the germline dicer1 pathogenic study indicates that variant identied by the nih was present in 2% of germline variant reads in our study as well . 
this patient continues to receive annual chest ct scans with no evidence of disease and undergoes annual kidney ultrasound scans , thyroid examinations , and targeted physical examinations as screening for other potential tumors . patient 4 : a patient with a rare dicer1 - associated tumor patient 4 presented at 3 years of age with headaches , photophobia , and hydrocephalus . 
the patient received ve cycles of chemotherapy , consisting of vincristine , etoposide , cyclophosphamide , and cisplatin , with tumor resection performed after the second cycle because of an increase in tumor size . 
the patient also underwent autologous bone marrow transplantation . a year later , an mri scan revealed an enhancing mass overlying the left middle cerebellar peduncle , suggestive of recurrent disease . 
in a previous study , 25 low - level mosaicism in four children with multiple dicer1 - associated tumors in whom no germline dicer1 variant had been identied by conventional sequencing techniques was observed . 
patient 4 contributes to the literature on dicer1 syndrome and illustrates how ics can be useful in identifying germline variants in individuals with rare cancers . from a cancer treatment perspective , all four of these challenging patients revealed dicer1 variants ; however , to date , there are no there are no clinically available pediatric therapies targeting specic mirnas . 
the possibility of targeting mirnas and dicer function in the future is currently being explored.26 from a genetic counseling standpoint , once a germline dicer1 pathogenic variant is identied , germline genetic testing is recommended for rst - degree relatives . 
approximately 13% to 20% of individuals with detectable germline dicer1 pathogenic variants have de novo variants , whereas 80% to 87% are inherited.9 , 27 germline genetic testing can provide tumor risk information to probands and their relatives and provide information regarding recurrence risk for future pregnancies . 
in families where the dicer1 variant is inherited , reports indicate it is uncommon to have multiple individuals diagnosed with ppb ; however , there may be higher penetrance of other manifestations , including goiters and benign lung cysts . 
family members lacking the familial dicer1 mutation do not need surveillance , whereas those who have inherited this variant should be observed according to current surveillance recommendations . screening recommendations at our institution evolved over time and are based on literature review , expert opinion , and patient preferences . 
beyond this age , for female adolescent and adult patients , we discuss symptoms and signs of hormone excess related to sex cordstromal tumors , such as hirsutism , virilization , and menstrual abnormalities . 
for all other manifestations , we recommended a detailed physical examination . recently , consensus guidelines for surveillance were published by the international ppb registry , which are largely in accordance with our institutions age - specic recommendations . 
these guidelines were developed at the rst international dicer1 symposium in may 2016.7 recommendations for surveillance begin in the prenatal period , with a third - trimester ultrasound for detection of large lung cysts that require intervention at birth . 
these differences reect the natural uncertainty in screening approaches for a recently described hereditary tumor syndrome , which aim to integrate the morbidity and the unknown mortality of syndrome - associated tumors , incidence in the target population , and presumed cost effectiveness and patient burden . least 10 years of age and do not tumor and germline sequencing in the pediatric oncology patient population has rapidly expanded in recent years . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . no potential conicts of interest were reported . references peng y , croce cm : the role of micrornas in human cancer . 
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int j cancer 141 : 2030 - 2036 , 2017 slade i , bacchelli c , davies h , et al : dicer1 syndrome : clarifying the diagnosis , clinical features and management implications of a pleiotropic tumour predisposition syndrome . 
hum mutat 32 : 1381 - 1384 , 2011 schultz kap , williams gm , kamihara j , et al : dicer1 and associated conditions : identication of at - risk individuals and recommended surveillance strategies . clin cancer res 24 : 2251 - 2261 , 2018 8 . 
science 325 : 965 , 2009 brenneman m , field a , yang j , et al : temporal order of rnase iiib and loss - of - function mutations during development determines phenotype in pleuropulmonary blastoma / dicer1 syndrome : a unique variant of the two - hit tumor suppression model . 
schultz ka , pacheco mc , yang j , et al : ovarian sex cord - stromal tumors , pleuropulmonary blastoma and dicer1 mutations : a report from the international pleuropulmonary blastoma registry . 
schultz ka , yang j , doros l , et al : dicer1 - pleuropulmonary blastoma familial tumor predisposition syndrome : a unique constellation of neoplastic conditions . dev pathol 18 : 504 - 511 , 2015 pediatr blood cancer 61 : 1695 - 1697 , 2014 pathol case rev 19 : 90 - 100 , 2014 22 : 564 - 567 , 2014 14 . 
fern andez - martnez l , villegas ja , santamara i , et al : identication of somatic and germ - line dicer1 mutations in pleuropulmonary blastoma , cystic nephroma and rhabdomyosarcoma tumors within a dicer1 syndrome pedigree . 
kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identies pathogenic germline mutations , and directs targeted therapy . 
marks lj , oberg ja , pendrick d , et al : precision medicine in children and young adults with hematologic malignancies and blood disorders : the columbia university experience . 
messinger yh , stewart dr , priest jr , et al : pleuropulmonary blastoma : a report on 350 central pathology - conrmed pleuropulmonary blastoma cases by the international pleuropulmonary blastoma registry . 
 clinical factors that affect the establishment of soft tissue sarcoma patient - derived orthotopic xenografts : a university of california , los angeles , sarcoma program prospective clinical trial tara a . 
eilber , md , division of surgical oncology , university of california , los angeles , 10833 leconte ave , room 54 - 140 chs , los angeles , ca 90095 - 1782 ; e - mail : fceilber@mednet.ucla.edu. purpose given the diverse and aggressive nature of soft tissue sarcomas ( stss ) , a need exists for more - precise therapy . 
this study assessed the feasibility of incorporating pdoxs into the clinical setting and identifying factors associated with pdox establishment . patients and methods from may 2015 to may 2016 , 107 patients with biopsy - proven or potential sts were enrolled . 
tumors exposed to radiation preoperatively did not establish ( zero of 11 [ 0% ] ) , and tumors exposed to neoadjuvant chemotherapy had a lower er ( 31.9% ) than untreated tumors . 
2017 by american society of clinical oncology introduction over the past decade , there has been an evolution toward a personalized approach to the treatment of cancer in which individual patient and tumor characteristics are used to guide therapy . 
although responders tend to have significantly improved outcomes , nonresponders endure the toxic adverse effects of treatment without survival benefit.2 , 3 collectively , the rarity , histologic diversity , high risk of metastasis , and poor response rates to systemic therapy highlight the rationale and immediate need for more personalized sarcoma therapy . 
pdxs maintain genetic similarity with and mimic the therapeutic responses of a patients tumor.4 within stss , multiple subcutaneous pdx models have been developed and have shown promise for replicating the tumor histology , clinical chemosensitivity , growth kinetics , and local disease progression of a patients tumor.5 - 8 patient - derived orthotopic xenograft ( pdox ) models in which the patient - derived tissue is implanted into the corresponding anatomic location by a technique called surgical orthotopic implantation ( soi ) have also been shown to produce patterns of invasion and metastatic spread that have not been demonstrated in the subcutaneous pdx models.8 - 15 as well , pdox models have been shown to faithfully reproduce the histology of the human tumor16 , 17 and to have unique clinical applicability . 
in particular , pdox models have been shown to produce tumor response and resistance that mirror that of the patient.18 smith et al19 demonstrated that xenograftability of liposarcomas correlate directly with patient outcomes . 
by building upon the results of these previous studies , pdox models seem to present the best opportunity to test multiple potentially active systemic agents ( chemotherapy , targeted therapy , etc ) in a preclinical model , which shields patients from the potential toxicity of inactive drugs and identifies effective therapies that improve outcomes . 
all patients elected to enroll and were consented preoperatively . mice athymic nu / nu female nude mice ( anticancer , san diego , ca ) 4 to 6 weeks old were used to xenograft human tissues . 
all animal studies were conducted with an anticancer institutional animal care and use committee protocol specifically approved for this study and in accordance with the principles and procedures outlined in the national institutes of health guide for the care and use of animals under assurance number a3873 - 1.8 , 18 all surgical experiments were done under anesthesia and with analgesia to minimize suffering . 
anesthesia was administered by subcutaneous injection of a 0.02 - ml solution of 20 mg / kg ketamine , 15.2 mg / kg xylazine , and 0.48 mg / kg acepromazine maleate . 
all animals were fed an autoclaved laboratory rodent diet and housed in a barrier facility on a high - efficiency particulate arrestancefiltered rack under standard conditions of 12 - hour light / dark cycles . 
these procedures are similar to the standard of care at our facility and have been previously documented.8 , 18 tumor acquisition and xenograft establishment intraoperatively at the time of tumor resection , a tissue sample was obtained by the operating surgeon ( f.c.e. ) and transported to anticancerpdox on ice for immediate soi in nude mice . each tumor sample was divided into 5 - mm fragments . 
tumor fragments were then implanted both subcutaneously and orthotopically into nude mice using a well - validated protocol.8 , 15 , 18 , 20 - 24 soi procedures were then followed for orthotopic models specific to each tumor site.8 , 11 , 15 , 18 , 20 - 27 for extremity tumors , 10 - mm skin incisions were made in the corresponding anatomic site , and then a single tumor fragment was placed orthotopically between muscle layers . 
wounds were closed with 6 - 0 nylon suture ( ethilon ; ethicon , bridgewater , nj )  . nude mice were monitored for tumor growth for up to 6 months after implantation . 
in every pdox , the histopathology of the established tumors was compared with the original patients tumor and verified for concordance by a specialized sarcoma pathologist ( s.m.d. ) ; this method for histopathologic validation has been previously published by our group.8 , 15 , 18 , 20 , 23 , 24 , 26 , 28 established pdoxs were maintained for future study of potential systemic agents . statistical methods for all patients enrolled in the trial , demographics and clinical data were prospectively collected , and xenograft data ( time to establishment ) were obtained in collaboration with anticancer . 
neoadjuvant treatment information was collected for all patients . only therapy that occurred in the neoadjuvant setting before tumor excision was included in this analysis because the tumor sample used for xenograft implantation was only exposed to therapy that occurred before resection . 
tumors exposed to neoadjuvant therapy were graded by their pathologic response on the basis of the percent response indicated by a specialized sarcoma pathologist . given that xenografts were established only from high - grade tumors , factors associated with establishment and time to establishment were analyzed among the high - grade cohort . 
the rate of establishment , which indicated that the tumor was successfully engrafted and serially passaged , was measured in days from the time of original engraftment to the time adequate growth was achieved from serial passage . 
factors associated with establishment time were analyzed with survival functions using log - rank tests for equality and nonparametric methods for distribution . results study population all 107 patients approached for study enrollment elected to enroll . 
similar numbers of male and female patients were enrolled ( 48% female )  . median patient age was 61 years ( range , 16 to 91 years ) , and median tumor size was 7.6 cm ( range , 0.9 to 38 cm )  . 
the majority of tumors were high grade ( 67% ) , and the most common subtypes were liposarcoma ( 25% ) and leiomyosarcoma ( 14% )  . tumors spanned 28 histologic subtypes ( appendix table a2 , online only )  . 
given that only high - grade tumors were established , the high - grade subpopulation is the focus of the remaining analysis . high - grade cohort pdox development was attempted for 72 patients with high - grade stss . 
for patients who underwent neoadjuvant therapy , the median time between completion of neoadjuvant therapy and tumor resection was 35 days ( range , 9 to 74 days )  . factors associated with establishment of sarcoma pdox model no low - grade stss were established as pdoxs ( zero of 32 )  . 
patient and tumor characteristics for all high - grade tumors and by xenograft success characteristic high grade only ( n = 72 ) successful xenografts only ( n = 32 ) unsuccessful xenografts only ( n = 40 ) female male grade high presentation primary location extremity size , cm , 10  . 
no difference in the likelihood of pdox establishment was found by sex , age , presentation ( primary , recurrent , or metastatic ) , location , subtype , or size . establishment rates varied by subtype ( appendix table a2 )  . 
factors associated with patient - derived orthotopic xenograft establishment among high - grade tumors establishment rate among high - grade tumors ( n = 72 ) univariable logistic regression ( n = 72 ) characteristic % ( no . ) female male grade high presentation primary location extremity size , cm , 10  . 
only one patient with osteosarcoma and one with rhabdomyosarcoma were enrolled , and both tissue samples led to a successful pdox . among high - grade primary stss , 45.5% ( 20 of 44 ) established . 
primary versus recurrent / metastatic tumors : factors associated with patient - derived orthotopic xenograft establishment all high - grade primary tumors ( n = 44 ) high - grade primary establishment rates ( n = 20 ) all high - grade metastatic / recurrent tumors ( n = 28 ) high - grade metastatic / recurrent establishment rates ( n = 12 ) characteristic abdomen / retroperitoneum female male location extremity size , cm , 10  . 
on the basis of establishment rates alone , neoadjuvant treatment seems to have a consistent effect on primary and metastatic / recurrent stss ( table 3 )  . among untreated stss , 61.9% ( 26 of 42 ) were established . 
untreated high - grade tumors : factors associated with establishment high - grade untreated tumors ( n = 42 ) high - grade untreated establishment - rate ( n = 26 ) characteristic female male presentation primary location extremity size , cm , 10  . 
compared with untreated patients , no difference in time to establishment was observed for patients who received neoadjuvant therapy ( p = .180 ; fig 2 )  . specifically , given that none of the grafts exposed to radiation established , no difference in time to establishment was found when untreated grafts were compared with those exposed to neoadjuvant chemotherapy alone . 
furthermore , the study indicates that patients who receive no treatment before tumor resection are most likely to benefit , such that 61.9% of those patients tumors were successfully xenografted . 
the champions oncology trial , which developed 29 subcutaneous pdx models , indicated that growth rates varied and documented an establishment rate of 76% but did not indicate which patient or tumor factors predicted establishment.29 to appropriately select patients for xenograft studies , we first sought to understand which tumors are most likely to grow as xenografts . in the current study , we prospectively enrolled all patients who underwent resection of an sts at a single institution over a 1 - year period . 
specifically , low - grade tumors universally failed to grow , whereas high - grade tumors had an overall establishment rate of 44.4% ( 32 of 72 ) , which no treatment ct only xrt only ct + xrt n = 42 n = 19 days n = 5 n = 6 fig 1 . 
specifically , we found no correlation between the time to establishment and previous treatment - , subtype - , or patient - related factors . the median time to establishment of a xenograft among those that established was 53 days , which indicates that xenografts can be developed over a short period . 
we acknowledge that this amount of time required for xenograft establishment and serial drug testing may take longer than the patients recovery from surgery ; therefore , at present we believe that the results of xenograft testing should be used to supplement care and potentially define second - line therapies rather than replace standard treatments . the current study is limited by the sample size and diverse study population . 
although statistical analyses of the overall group were feasible , smaller subgroup analyses were limited , and therefore , conclusions about individual subtypes or treatment factors could not be made with a high degree of certainty . as we move forward with the use of pdxs as a tool for personalizing sarcoma therapy , we must be cognizant of the patient population with the greatest potential to benefit : patients with high - grade tumors that have not been exposed to neoadjuvant radiation therapy or those without a significant treatment response . 
eilber provision of study materials or patients : kei kawaguchi , yungfeng li , nicholas bernthal , bartosz chmielowski , arun s . singh collection and assembly of data : tara a . 
elliott no relationship to disclose kei kawaguchi no relationship to disclose tasuku kiyuna no relationship to disclose kentaro igarashi no relationship to disclose yungfeng li no relationship to disclose joseph g . 
 nicholas bernthal honoraria : daiichi sankyo consulting or advisory role : onkos surgical , bonesupport research funding : onkos surgical speakers bureau : genentech , roche , janssen pharmaceuticals travel , accommodations , expenses : genentech , roche , bristol - myers squibb , janssen pharmaceuticals , merck jane yanagawa no relationship to disclose anusha kalbasi no relationship to disclose noah federman stock and other ownership interests : genmab , kite pharma consulting or advisory role : zelda therapeutics bartosz chmielowski consulting or advisory role : amgen , bristol - myers squibb , merck , genentech , roche , eisai , immunocore arun s . 
singh consulting or advisory role : eli lilly , daiichi sankyo speakers bureau : eli lilly , eisai travel , accommodations , expenses : eli lilly , daiichi sankyo , eisai stock and other ownership interests : anticancer - pdox robert m . 
hoffman , anticancer ; and takashi murakami , kei kawaguchi , tasuku kiyuna , kentaro igarashi , and robert m . hoffman , university of california , san diego , san diego , ca . supported by the robert wood johnson clinical scholars program and the west los angeles veteran affairs health services research and development center for innovation ( t.a.r. ) and national cancer institute grant no . 
donahue tr , kattan mw , nelson sd , et al : evaluation of neoadjuvant therapy and histopathologic response in primary , high - grade retroperitoneal sarcomas using the sarcoma nomogracancer 116 : 3883 - 3891 , 2010 3 . 
hiroshima y , zhang y , zhang n , et al : patient - derived orthotopic xenograft ( pdox ) nude mouse model of soft - tissue sarcoma more closely mimics the patient behavior in contrast to the subcutaneous ectopic model . 
furukawa t , kubota t , watanabe m , et al : orthotopic transplantation of histologically intact clinical specimens of stomach cancer to nude mice : correlation of metastatic sites in mouse and individual patient donors . 
igarashi k , kawaguchi k , kiyuna t , et al : patient - derived orthotopic xenograft ( pdox ) mouse model of adult rhabdomyosarcoma invades and recurs after resection in contrast to the subcutaneous ectopic model . 
murakami t , singh as , kiyuna t , et al : effective molecular targeting of cdk4 / 6 and igf - 1r in a rare fus - erg fusion cdkn2a - deletion doxorubicin - resistant ewings sarcoma patient - derived orthotopic xenograft ( pdox ) nude - mouse model . 
smith kb , tran lm , tam bm , et al : novel dedifferentiated liposarcoma xenograft models reveal pten downregulation as a malignant signature and response to pi3k pathway inhibition . 
kiyuna t , murakami t , tome y , et al : high efficacy of tumor - targeting salmonella typhimurium a1 - r on a doxorubicinand dactolisib - resistant follicular dendritic - cell sarcoma in a patient - derived orthotopic xenograft pdox nude mouse model . 
kiyuna t , murakami t , tome y , et al : labeling the stroma of a patient - derived orthotopic xenograft ( pdox ) mouse model of undifferentiated pleomorphic soft - tissue sarcoma with red fluorescent protein for rapid non - invasive imaging for drug screening . 
yamamoto m , zhao m , hiroshima y , et al : efficacy of tumor - targeting salmonella a1 - r on a melanoma patientderived orthotopic xenograft ( pdox ) nude - mouse model . 
kawaguchi k , igarashi k , murakami t , et al : tumor - targeting salmonella typhimurium a1 - r combined with temozolomide regresses malignant melanoma with a braf - v600e mutation in a patient - derived orthotopic xenograft ( pdox ) model . 
kawaguchi k , murakami t , chmielowski b , et al : vemurafenib - resistant braf - v600e - mutated melanoma is regressed by mek - targeting drug trametinib , but not cobimetinib in a patient - derived orthotopic xenograft ( pdox ) mouse model . 
murakami t , delong j , eilber fc , et al : tumor - targeting salmonella typhimurium a1 - r in combination with doxorubicin eradicate soft tissue sarcoma in a patient - derived orthotopic xenograft ( pdox ) model . 
murakami t , igarashi k , kawaguchi k , et al : tumor - targeting salmonella typhimurium a1 - r regresses an osteosarcoma in a patient - derived xenograft model resistant to a molecular - targeting drug . 
kawaguchi k , igarashi k , murakami t , et al : tumor - targeting salmonella typhimurium a1 - r sensitizes melanoma with a braf - v600e mutation to vemurafenib in a patient - derived orthotopic xenograft ( pdox ) nude mouse model . j cell biochem 118 : 2314 - 2319 , 2017 28 . 
igarashi k , kawaguchi k , murakami t , et al : intra - arterial administration of tumor - targeting salmonella typhimurium a1 - r regresses a cisplatin - resistant relapsed osteosarcoma in a patient - derived orthotopic xenograft ( pdox ) mouse model . 
patient and tumor characteristics ( high grade and low grade ) characteristic all xenografts ( n = 107 ) female male grade high presentation primary location trunk extremity size , cm , 10  . 
 association of germline genetic test type and results with patient cancer worry after diagnosis of breast cancer background there are concerns that multigene panel testing compared with brca1 / 2 - only testing after diagnosis of breast cancer may lead to unnecessary patient worry about cancer because of more ambiguous results . methods patients with breast cancer diagnosed from 2013 to 2015 and accrued from seer registries in georgia and los angeles were surveyed ( n = 5 , 080 ; response rate , 70% ) , and responses were merged with seer data and germline genetic testing and results . 
we examined patient reports of cancer worry by test type and results in 1 , 063 women who linked to a genetic test and reported undergoing testing . results more than half of the sample ( n = 640 ; 60.2% ) received brca1 / 2 - only testing versus 423 patients ( 39.8% ) who had a multigene panel . 
a minority of tested patients reported substantial cancer worry after treatment : 11.1% ( n = 130 ) reported higher impact of cancer worry , and 15.1% ( n = 162 ) reported a high frequency of cancer worry ( worrying often or almost always ) in the past month . 
2018 by american society of clinical oncology introduction multiple - gene panel ( mgp ) testing has rapidly replaced brca1 / 2 - only testing after diagnosis of breast cancer.1 however , genetic testing use in patients who need it seems to be low.2 , 3 one barrier to more robust uptake of mgp testing is uncertainty about its clinical utility . 
indeed , some have argued that mgp testing should not replace brca1 / 2 - only testing , even in patients with higher pretest risk of a pathogenic mutation , because of these concerns about patient reactions , 4 whereas others strongly disagree.5 current clinical guidelines that recommend genetic testing in women at elevated pretest risk of carrying a pathogenic variant do not specify how many genes should be tested . 
we sent surveys to 7 , 810 patients : 507 patients were ineligible because of the exclusions noted previously or were deceased , institutionalized , too ill , or unable to complete a survey in spanish or english , leaving 7 , 303 patients . 
virtually all patients ( 5 , 026 ) had complete information for the test linkage phase , of whom 1 , 272 ( 25.3% ) linked to a genetic test result , 1 , 063 of whom ( 21.2% ) reported receipt of genetic testing in the survey . survey responses were merged with seer clinical data and genetic testing information obtained from four laboratories ( ambry genetics , aliso viejo , ca ; genedx , gaithersburg , md ; invitae , san francisco , ca ; myriad genetics , salt lake city , ut ) that performed nearly all germline cancer genetic testing in the study regions . 
test type and results were merged to 5 , 026 patients with complete information on all variables for seer genetic testing linkage using a probabilistic matching strategy performed by information management services ( rockville , md )  . 
the safe harbor method was used to de - identify the data set before transfer to the university of michigan for analysis.9 the collaboration was covered under data use agreements between the university of michigan , genetic laboratories , and information management services . 
the research was approved by institutional review boards of the university of michigan , emory university , the university of southern california , the georgia department of public health , the california state committee for the protection of human subjects , and california cancer registry . 
waivers of informed consent and authorization were approved , given the use of a third - party honest broker to conduct the linkage and create a de - identified data set for analyses . measures we used two questions to evaluate patient worry about future cancer . 
forest plot ( adjusted odds ratios and 95% cis ) for results of a multivariable model regressing a binary variable indicating higher versus low impact of cancer worry on test type , controlling for selected predisposing , clinical , and treatment factors and weighted for survey design and nonresponse . 
er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; hs , high school ; mgp , multigene panel ; pr , progesterone receptor ; ref , reference . made it difficult for you to carry out your usual daily activities at home or work ? ; made you feel distant from family or friends ? ( responses were based on 5 - point likert categories from almost never to almost always )  . 
we developed a scale by averaging the responses across the three items to create a continuous range from 1 to 5 , with higher values indicating greater impact of cancer worry . 
we then created a binary variable indicating higher impact of cancer worry versus low impact using a cut point of 3.0 , which corresponded to responses of sometimes , often , or almost always . 
we also measured frequency of cancer worry for validation , which was assessed using a single item : in the past month , how often have you worried about your cancer coming back ? ( almost never to almost always ; five point categories )  . 
genetic laboratories provided results at the level of the gene tested ( eg , brca1 ) and the clinical interpretation sent to the ordering clinician ( consisting of pathogenic , likely pathogenic , uncertain significance , likely benign , or benign )  . 
we categorized a test that assessed only brca1 / 2 as brca1 / 2 only and a test that assessed any additional gene ( eg , atm , chek2 ) as a multigene panel . 
if patients received both tests on separate occasions ( eg , a brca1 / 2 - only test and later mgp ) , they were coded as having received mgp . 
we assessed clinical factors related to future cancer risk ( tumor behavior , triple - negative disease , nodal status , bilateral disease ) , treatments received , age ( in 10 - year groups ) , education , and family history . 
 defined as having two or more first - degree relatives with breast cancer ; any relatives with ovarian cancer , sarcoma , or male breast cancer ; ashkenazi jewish ancestry ; or a family history of a mutation - conferring risk ( eg , brca1 / 2 )  . statistical analysis we first examined cancer worry variables by test type , test results , and selected covariables . 
a minority of tested patients reported substantial cancer worry after treatment : 11.1% ( n = 130 ) reported high impact of cancer worry , and 15.1% ( n = 162 ) reported high frequency of worry ( worrying often or almost always in the past month )  . 
we observed similar findings in a model of frequency of cancer worry ( data not shown )  . figure 1 shows the results of a multivariable model regressing a binary variable indicating higher versus low impact of cancer worry on test type , controlling for selected predisposing , clinical , and treatment factors . 
in sensitivity analyses , we examined different permutations of the cancer worry variables , including different cut points for higher worry , and using a continuous variable , and results were consistent . discussion we found that the type of genetic testing patients received ( mgp v brca1 / 2 only ) was not associated with their report of cancer - related worry ( impact or frequency )  . 
 as noted in our prior work , cancer - related worry was associated with younger age and lower educational level , but not clinical factors.10 , 11 strengths of this study include a large population based sample of patients recently diagnosed with breast cancer and accrued shortly after the advent of multigene panel testing in the community , genetic testing results from companies linked to seer clinical data , and granular information about patients , including their report of cancer - related worry . 
we excluded them from the analytic sample because we did not think it was valid to assess the association of a test type with attitudes about health risk among patients who did not recall that they had the test . 
finally , generalizability of the findings are limited to two large geographic regions of the united states . the results from this study and our prior work suggest that testing more genes versus brca1 / 2 alone does not seem to foment more negative patient reactions . 
our prior research in this cohort suggested that mgp testing ( v brca1 / 2only testing ) does not lead to inappropriate rates of contralateral prophylactic mastectomy.1 virtually all testers in this study received some form of genetic counseling , 6 and our results suggest these efforts may sufficiently frame results in a manner that did not alarm patients . 
kurian manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors paul abrahamse no relationship to disclose sarah t . 
dolinsky , cgc , and melissa pronold at ambry genetics , delores bowman and benjamin solomon at genedx , edward esplin and stephen lincoln at invitae , and johnathan lancaster and brian dechairo at myriad genetics for their collaboration on the genetic test data linkage to seer data . 
the collection of los angeles county cancer incidence data used in this study was supported by the california department of public health pursuant to california health and safety code section 103885 , centers for disease control and preventions ( cdcs ) national program of cancer registries , under cooperative agreement 5nu58dp003862 - 04 / dp003862 , the national cancer institutes seer program under contract hhsn261201000140c awarded to the cancer prevention institute of california , contract hhsn261201000035c awarded to the university of southern california , and contract hhsn261201000034c awarded to the public health institute . 
the collection of cancer incidence data in georgia was supported by contract hhsn261201300015i , task order hhsn26100006 from the national cancer institute and cooperative agreement 5nu58dp003875 - 04 - 00 from the cdc . 
us department of health & human services : guidance regarding methods for de - identification of protected health information in accordance with the health insurance portability and accountability act ( hipaa ) privacy rule . 
janz nk , li y , zikmund - fisher bj , et al : the impact of doctor - patient communication on patients perceptions of their risk of breast cancer recurrence . 
forest plot ( adjusted odds ratios and 95% cis ) showing results of multivariable logistic regression for higher impact of cancer worry ( complete case n = 1 , 044 )  . 
 alk testing trends and patterns among community practices in the united states purpose targeted therapy of alk in patients with metastatic nonsquamous nonsmall - cell lung cancer ( nsclc ) and alk rearrangements improves outcomes compared with chemotherapy . 
logistic regression was used to examine the association between demographic and clinical characteristics and testing for alk rearrangements . results of 31 , 483 patients analyzed from the database , 16 , 726 patients ( 53.1% ) were tested for alk rearrangements . 
median ( interquartile range ) time from laboratory receipt of sample to first alk test result was 7 ( 7 ) days ; median time from advanced diagnosis to first alk test result was 25 ( 29 ) days . 
patients who were older , male , had a history of smoking , lived in non - western us regions , and who had recurrent disease or squamous histology were less likely to be tested for alk . 
2018 by american society of clinical oncology introduction recent advances in molecular genetics have increased the opportunity for precision medicine in metastatic nonsquamous nonsmall - cell lung cancer ( nsclc )  . 
for instance , translocation of the anaplastic lymphoma kinase ( alk ) gene is found in approximately 2% to 8% of all patients with nsclc and occurs primarily in patients who are never - smokers or light ex - smokers with adenocarcinoma histology.1 - 4 in addition to representing a distinct molecular nsclc subtype , alk rearrangements are indicative of tumor cell susceptibility to alk inhibitors.5 targeted inhibition of alk in patients with alk rearrangements can decrease tumor burden and significantly increase progression - free survival compared with chemotherapy.3 , 6 the first alk inhibitor , crizotinib , along with the vysis alk break apart fish probe kit , was given accelerated approval by the us food and drug administration ( fda ) in 2011 . 
since then , other firstand second - generation alk inhibitors have been approved , including ceritinib in 2014 and alectinib in 2015 . the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology ( cap / iaslc / amp ) molecular testing and national comprehensive cancer network ( nccn ) peter b . 
 nsclc treatment guidelines recommend testing for alk , egfr , and ros1 in lung adenocarcinomas and in nsclc where an adenocarcinoma component cannot be excluded , regardless of clinical characteristics.1 , 7 , 8 fluorescent in situ hybridization ( fish ) or immunohistochemistry ( ihc ) are assays recommended by cap / iaslc / amp guidelines for the detection of alk rearrangements before selection of targeted therapy.8 in addition to fish , the alk ( d5f3 ) cdx assay ( ventana medical systems , tucson , az ) and foundationone cdx ( foundation medicine , cambridge , ma ) are ihc and next - generation sequencing ( ngs ) assays , respectively , that are fda approved to identify patients eligible for alk inhibitor treatment . 
alk rearrangements could also be detected using polymerase chain reaction , but no fda - approved assay is available to date , and this method is not currently recommended in guidelines.8 numerous challenges associated with molecular testing of malignancies may affect adoption of molecular testing guidelines and performance of alk testing in clinical practice . 
a major challenge in molecular testing is inadequate tissue samples.9 , 10 for example , in a study that examined the workflow of molecular testing for 157 lung cancer specimens , successful testing of all molecular targets could not be completed for 19% of specimens.11 additional challenges may include tumor heterogeneity , complex results that require multidisciplinary input , education and training of laboratory and staff , availability of assays , and patient affordability.9 , 10 in a retrospective analysis of 814 patients in new jersey and maryland with nonsquamous nsclc who were identified using the cota database ( cota , new york , ny ) , which extracts and organizes data from electronic health records , only 65% underwent alk testing , indicating limited integration of molecular testing recommendations into clinical practice.12 given the clinical benefit of alk inhibitor therapy in patients with nsclc with alk rearrangements , evaluation of alk testing using large , real - world , geographically diverse data sources is warranted . 
the objective of this study was to assess real - world alk testing patterns among community practices in the united states in patients with advanced nsclc from january 2011 through may 2017 . methods study overview and database description this was a retrospective analysis using the flatiron health electronic health record ( ehr ) derived database , a longitudinal , demographically and geographically diverse database.13 the database includes > 265 cancer clinics ( approximately 800 sites of care ) representing more than 2 million active us patients with cancer available for analysis . 
the current analysis was limited to data from community practices and included 34 , 911 patients diagnosed with advanced nsclc ( stage iiib or iv by american joint committee on cancer 7th edition ) from january 2011 through may 2017 . 
insurance information was categorized into commercial ( including those with dual medicare or medicaid coverage ) , medicare ( including dual medicaid coverage ) , medicaid , and other / unknown . 
 ( % ) unless otherwise noted . abbreviations : alk , anaplastic lymphoma kinase ; iqr , interquartile range , q3 - q1 ; nos , not otherwise specified ; nsclc , nonsmall - cell lung cancer . date specimens were received by the laboratory to the test report date . data analysis statistical analyses were primarily descriptive , with frequencies calculated for categorical data and means , medians , interquartile ranges ( iqrs ) , and standard deviations ( sds ) calculated for continuous data . 
odds ratios ( ors ) and 95% cis were calculated by logistic regression to examine the association between demographic and clinical characteristics and testing for alk rearrangements . results patient characteristics overall , 34 , 911 patients with advanced nsclc were identified from the flatiron health ehr - derived database from january 2011 through may 2017 ; 31 , 483 met the selection criteria and were included in the analysis . 
most of the samples used for alk testing were tissue ( 93.7% ; 15 , 664 of 16 , 726 ) ; 2.6% ( 439 of 16 , 726 ) were blood , and the rest were unknown . 
of the total 21 , 639 patients with nonsquamous histology , 66.9% ( 14 , 478 of 21 , 639 ) were tested for alk , and of the 7 , 923 patients with squamous histology , 18.5% ( 1 , 466 of 7 , 923 ) were tested for alk . 
 among the patients who had nonsquamous histology and who were not tested for alk , 87.2% ( 6 , 025 of 6 , 913 ) had a history of smoking , and among those with a squamous histology and who were either tested or not tested for alk , 91.5% ( 1 , 320 of 1 , 443 ) and 95.6% ( 5 , 992 of 6 , 268 ) , respectively , had a history of smoking . 
overall , 16 , 726 of 31 , 483 ( 53.1% ) patients were tested for alk , with 633 of 16 , 726 ( 3.8% ) patients positive for alk ( 581 of 14 , 478 [ 4.0% ] nonsquamous histology , 24 of 1 , 466 [ 1.6% ] squamous histology , and 28 of 782 [ 3.6% ] not otherwise specified histology )  . alk testing patterns alk testing rates by year of advanced diagnosis steadily increased over time from an average of 32.4% ( 1 , 093 of 3 , 371 ) in 2011 to 62.1% ( 3 , 526 of 5 , 680 ) in 2016 for all patients with advanced nsclc , from 41.1% ( 935 of 2 , 273 ) in 2011 to 75.1% ( 2 , 947 of 3 , 924 ) in 2016 for patients with nonsquamous histology , and from 12.1% ( 101 of 832 ) in 2011 to 26.5% ( 372 of 1 , 403 ) in 2016 for patients with squamous histology ( fig 1a )  . 
with test 2012 2014 year 178 201 245 368 395 471 483 446 525 595 593 625 665 765 717 746 728 801 891 820 860 805 787 702 631 2015 2013 2016 2017 squamous , no . 
 age , years 55 - 64 v < 55 65 - 74 v < 55 75 - 84 v < 55 85 + v < 55 female v male race asian v white black or african american v white other race v white missing v white hispanic v non - hispanic ethnicity histology nos v non squamous squamous v non squamous disease type recurrent v de novo unknown v de novo smoking status history of smoking v no history unknown history v no history insurance medicaid v commercial medicare v commercial other v commercial region midwest v west northeast v west south v west missing v west fig 2 . 
the overall median ( iqr ) turnaround time from the date samples were received by the laboratory to the test report date was 7 ( 7 ) days and ranged from 6 days for fish to 12 days for ngs ( table 2 )  . 
the overall median ( iqr ) time from advanced diagnosis date to first alk test result date was 25 ( 29 ) days ( table 2 ) and differed by type of test and insurance type . 
 median ( iqr ) times from advanced diagnosis to first alk test result for fish were 20 ( 19 ) , 22 ( 31 ) , and 23 ( 27 ) days for commercial insurance , medicaid , and medicare , respectively , and for ngs were 37 ( 34 ) , 58 ( 159 ) , and 41 ( 105 ) days , respectively ( table 2 )  . 
on the basis of tests conducted by foundation medicine ( cambridge , ma ) laboratory , the overall agreement between ngs and fish was 97.6% ( 360 of 369 )  . 
the percentage of tests positive by ngs that were initially negative by fish was 1.9% ( 7 of 369 )  . treatment before alk test results among patients tested for alk who had valid tissue collection and test result dates , 21.5% ( 3 , 290 of 15 , 320 ) initiated therapy before receiving their first alk test results . 
percentage of patients initiating treatment before first anaplastic lymphoma kinase ( alk ) test result . discussion this retrospective analysis of patients with advanced nsclc treated at community practices between january 2011 and may 2017 found that 53.1% of all patients , 66.9% of patients with nonsquamous histology , and 18.5% of patients with squamous histology were tested for alk rearrangements . 
cap / iaslc / amp and nccn guidelines recommend alk testing be conducted for patients with nsclc that has an adenocarcinoma component.7 , 8 however , alk testing may also be considered for patients with nsclc who have mixed histology , who are of young age , or who are without a history of tobacco exposure.7 , 8 the current analysis confirms and extends the findings of a retrospective analysis of 814 patients with nonsquamous nsclc treated in community centers in the united states , which found an overall 65% alk testing rate for the years 2013 to 2015.12 alk testing rates increased over time , reaching 75% in 2016 in patients with nonsquamous histology , indicating improvement in adherence to alk testing recommendations as well as physician recognition of the clinical benefits of alk targeted therapy . 
 the reasons for lack of testing were not captured in the flatiron health database , although possible reasons may include evolution of best practices and guidelines across the study period , patient disease severity , and insufficient tissue ( as was observed in 16% to 21% of patients in other nsclc studies ) .4 , 14 , 15 blood - based assays could address the issue of insufficient tissue , and research in this field is emerging.16 patients with squamous histology were less likely to be alk tested , which is consistent with guidelines that state there is no evidence to recommend alk testing in patients with typical squamous histology who do not have other clinical features to prompt alk testing.7 , 8 in the current analysis , testing rates increased over time in patients with squamous histology , and , overall , 1.6% had an alk rearrangement . 
the increased testing rate for patients with squamous histology may be due to a general increase in the perceived benefit of alk inhibitors for alk - positive nsclc by physicians or to the release of cap / iaslc / amp and nccn guidelines that suggest selectively testing patients with squamous histology , such as patients who are never - smokers or former light smokers.1 , 17 the likelihood of alk testing decreased as age increased . 
patients with alk - positive disease in clinical studies tended to be younger , nonsmokers , and have adenocarcinoma , perhaps increasing the likelihood that these patients would have been tested for alk positivity despite guidelines recommending that all patients with nonsquamous disease be tested . 
in addition , the current analysis suggests there may also be socioeconomic barriers to alk testing ; medicaid patients were 40% less likely to be tested than patients with commercial insurance . 
collectively , these results suggest that additional education on alk testing in the community oncology setting is warranted . in our study , fish was the most commonly ordered genomic testing method , which was not unexpected , given that fish was the only recommended and fda - approved assay during the majority of the time period for our study . 
 updated 2018 cap / iaslc / amp and nccn guidelines now recommend fish or ihc for alk testing.7 , 8 with the rapidly changing landscape of fda - approved assays , such as the 2017 approval of the foundationone cdx ngs assay , the distribution of assays used will likely continue to evolve . 
indeed , in our study we observed a trend of declining use of fish and an increase in the use of ngs and , to a lesser extent , ihc . 
there is a trend in clinical practice to use ngs as the primary testing method to identify all targetable alterations.18 , 19 turnaround times for laboratory receipt of sample to test results were consistently less than 2 weeks across different test types , including ngs . 
the reasons for this variation are unknown ; however , potential reasons for longer times for some patients may include the ordering process for biomarker testing , sample shipment to the laboratory , and sample processing . 
for example , a previous study in metastatic colon cancer found that testing performed at a nonlocal or noncancer centeraffiliated laboratory was associated with greater likelihood of a testing delay.20 the current study was conducted in the community setting , and the majority of biomarker testing was done in commercial laboratories , which may be one of the possible explanations for the observed variance in times . 
in addition , the 14 - day rule may also have contributed to the variation in times for some medicare patients , because testing may have been delayed to avoid reimbursement complexities . numerically , ngs had a longer time from advanced diagnosis to alk test result for both medicare and medicaid patients . 
given that turnaround times for ngs were similar across insurance types and only accounted for a minor portion of the time from advanced diagnosis to alk test result , this may imply that delays in ordering ngs , which was not an approved test during the study period , may have existed . 
additional research is needed to determine if this trend will continue in the future , particularly given the 2017 simultaneous fda approval of ngs tests for tumor profiling and centers for medicare & medicaid services approval of coverage for fda - approved ngs tests , which may substantially improve the ability to provide more timely access to ngs testing.21 , 22 the lack of alk testing or delay in results may have serious clinical implications , given the efficacy of alk inhibitors in patients with alk rearrangements.3 , 6 , 23 , 24 in a head - to - head comparison , a second - generation alk inhibitor ( alectinib ) exhibited a median progression - free survival of 34.8 months , compared with 10.9 months with a first - generation alk inhibitor ( crizotinib ) .24 , 25 delays in alk testing may potentially lead to delayed treatment , 15 and , as is seen in other cancers , delays in treatment may lead to poorer outcomes.26 , 27 although additional research is needed to assess the impact of delays on outcomes , specifically in alk - positive nsclc , alk testing is needed to help facilitate timely treatment with an efficacious alk inhibitor . day - level granularity of biomarker testing ordered date is not always available in ehr data , which has limited our ability to interpret and determine reasons for observed delays in testing . 
 last , this study focused on community practices in the united states , and hence the results of this study may not be generalizable to all clinical practices . the results of the current analysis indicate that the frequency of alk testing in patients with advanced nsclc treated in community centers in the united states has increased over time . 
 however , certain subgroups of patients , such as patients receiving medicaid , were less likely to be tested , suggesting that additional education on genomic testing and investigation into socioeconomic barriers is warranted . 
 laura chu employment : genentech stock and other ownership interests : roche ravindra gupta employment : genentech katja schulze employment : genentech stock and other ownership interests : genentech matthew a . 
gubens consulting or advisory role : bristol - myers squibb , ariad pharmaceuticals , genentech , astrazeneca , abbvie , novartis , mersana therapeutics research funding : celgene ( inst ) , merck ( inst ) , novartis ( inst ) , genentech ( inst ) , oncomed ( inst ) acknowledgment medical writing and editorial assistance was provided by erin p . 
illei , johns hopkins university school of medicine , baltimore , md ; william wong , laura chu , ravindra gupta , and katja schulze , genentech , south san francisco ; matthew a . 
gubens , university of california , san francisco , ca ; and ning wu , pro unlimited , boca raton , fl . support supported by genentech , south san francisco , ca . prior presentation presented in part at the international association for the study of lung cancer 18th world conference on lung cancer , yokohama , japan , october 15 - 18 , 2017 . 
lindeman ni , cagle pt , beasley mb , et al : molecular testing guideline for selection of lung cancer patients for egfr and alk tyrosine kinase inhibitors : guideline from the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology . 
korpanty gj , graham dm , vincent md , et al : biomarkers that currently affect clinical practice in lung cancer : egfr , alk , met , ros - 1 , and kras . 
lindeman ni , cagle pt , aisner dl , et al : updated molecular testing guideline for the selection of lung cancer patients for treatment with targeted tyrosine kinase inhibitors : guideline from the college of american pathologists , the international association for the study of lung cancer , and the association for molecular pathology . 
distasio m , chen y , rangachari d , et al : molecular testing turnaround time for non - small cell lung cancer in routine clinicalpractice confirms feasibility of cap / iaslc / amp guideline recommendations : a single - center analysis . 
mayo - de - las - casas c , garzn ibez m , jordana - ariza n , et al : an update on liquid biopsy analysis for diagnostic and monitoring applications in non - small cell lung cancer . 
suh jh , johnson a , albacker l , et al : comprehensive genomic profiling facilitates implementation of the national comprehensive cancer network guidelines for lung cancer biomarker testing and identifies patients who may benefit from enrollment in mechanism - driven clinical trials . 
jensen ts , chin j , baldwin j , et al : proposed decision memo for next generation sequencing ( ngs ) for medicare beneficiaries with advanced cancer ( cag - 00450n )  . 
soria jc , tan dsw , chiari r , et al : first - line ceritinib versus platinum - based chemotherapy in advanced alk - rearranged non - small - cell lung cancer ( ascend - 4 ) : a randomised , open - label , phase 3 study . 
 o addition of chemotherapy is associated with decreased survival in early - stage ( t1 - 2n0m0 ) glottic squamous cell carcinoma treated with definitive radiotherapy purpose the role of chemoradiation ( crt ) in treating patients with early - stage glottic squamous cell carcinoma ( scc ) , especially for t2n0m0 glottic scc with impaired vocal cord mobility , remains unexplored . 
we sought to evaluate the impact of crt on survival in early - stage glottic scc by using the seer database . patients and methods we included patients with localized ( t1 - 4n0m0 ) glottic scc ( n = 4 , 743 ) diagnosed between 2004 and 2014 and treated with definitive radiotherapy ( rt ) alone , crt , or laryngectomy alone in the seer database . 
disease - specific mortality ( dsm ) was evaluated via multivariable regression using a competing risk model that accounts for other - cause mortality as a competing risk event for dsm . 
2019 by american society of clinical oncology introduction definitive treatment with radiotherapy ( rt ) for t1 - 2n0m0 squamous cell carcinomas ( scc ) of the glottis remains a standard of care in the united states and can help to preserve voice quality . 
several studies have shown lc rates for t1 and t2 glottic cancer treated with transoral laser microsurgery to range from 77% to 92% and 66% to 88% , respectively , 1 - 5 whereas open surgical procedures for glottic scc demonstrated a lc rate of 86% to 98%.2 , 6 - 10 the lc rate for early - stage glottic cancer treated with definitive rt depends significantly on t stage , with studies showing lc rates of 82% to 94% for t1 disease11 - 17 and 61% to 80% for t2 disease.11 - 13 , 15 - 19 the decreased lc for t2 glottic cancers treated with rt alone was thought to be attributed to a subset of patients with impaired vocal cord chenyang wang amar u . 
 the radiation therapy oncology group 9111 trial established concurrent crt as the standard treatment of t3 glottic cancer.28 the lc benefit associated with crt in the setting of t3 glottic cancer has raised the question of whether the subset of patients with t2 glottic cancer with impaired vocal cord mobility should be treated with crt as well , given the suboptimal outcomes with rt alone . 
seer routinely collects data on patient demographics , primary tumor site , morphology , stage at diagnosis , first course of treatment , and follow up for vital status . for this study , we selected patients diagnosed with n0m0 scc of the glottic larynx diagnosed from january 1 , 2004 , to december 31 , 2014 , who underwent definitive rt , crt , or subtotal or total laryngectomy . 
we excluded patients who had non - scc histology , unknown tumor grade , unknown race , unknown surgical status , unknown t stage , more than one primary malignancy , no active follow - up , or age younger than 18 years . 
this study was reviewed and approved by the institutional review board of the university of california , los angeles . statistical analysis extracted variables included age at diagnosis , sex , race , year of diagnosis , t stage , and tumor grade . 
analysis of variance , kruskal - wallis rank sum tests , and 2 tests were used to characterize differences in variables of interest between different treatment cohorts for continuous , ordinal , and categorical variables , respectively . 
 follow - up time was calculated via the reverse kaplan - meier method described by schemper and smith , 30 in which alive at last follow - up was designated the event of interest while death from any cause was censored . 
seer determines death and cause of death via algorithms to process death certificates , taking into account causes of deaths in conjunction with tumor sequence , site of original cancer diagnosis , and comorbidities . 
 to account for other - cause mortality ( ocm ) as a competing risk for dsm , multivariable regression analyses on the basis of the competing risk model as described by fine and gray31 were applied to the survival analysis while adjusting for age , year of diagnosis , sex , race , t stage , definitive treatment modality , and tumor grade . 
for t2n0 disease , an additional subset analysis was carried out on the basis of vocal cord impairment status to investigate whether patients with t2n0 disease with vocal cord impairment selectively benefit from crt . 
the validity of proportional hazards assumption was evaluated via schoenfeld residuals . to adjust for covariables and determine whether the addition of chemotherapy to rt affected dsm in patients with t1 - 4n0m0 glottic scc , we adopted propensity score matching ( psm ) via a nearest neighbor approach to balance patient characteristics including age , year of diagnosis , sex , race , and tumor grade between the rt and crt cohorts for each t stage . 
propensity score , first defined by rosenbaum and rubin32 as the probability of treatment assignment on the basis of a set of observed baseline patient characteristics , provides the means to retrospectively balance distribution of patient characteristics and thereby minimize effects of unmeasured confounders on treatment outcomes . 
the cumulative incidences of dsm and ocm after psm were plotted to illustrate the difference between rt and crt cohorts for each t stage , and their distributions were evaluated via a k - sample test described by gray.33 all statistical analyses were carried out using r version 3.4.1 ( r foundation for statistical computing , vienna , austria ) with two - sided testing and a statistical significance threshold of p = .05. results patient characteristics patient characteristics , stratified by definite treatment modality consisting of rt , crt , and subtotal or total laryngectomy , are listed in table 1 . 
patients who underwent rt alone tended to be older , with a median age of 66 years , compared with patients who underwent crt and surgery , who had median ages of 62 and 63 years , respectively . 
these patients were also more likely to present with higher tumor grade . multivariable regression for dsm and the results of the multivariable regression for dsm according to the competing risk model , accounting for ocm as a competing risk , are listed in table 2 . 
 plots of schoenfeld residuals versus failure times are shown in appendix figure a2 . subgroup multivariable regression for dsm using a competing risk model stratified by t stage the results of subgroup multivariable regression for dsm stratified by t stage are listed in table 3 . 
more recent year of diagnosis was not associated with any significant difference in dsm . cumulative incidence of dsm and ocm for rt and crt after psm patient characteristics stratified by definitive treatment modality before and after psm are listed in appendix tables a1 and a2 , respectively . 
a recent phase ii trial of concurrent crt with a fluoropyrimidine agent for t2n0m0 scc of the larynx ( 70% ) , oropharynx ( 16% ) , and hypopharynx ( 14% ) demonstrated a 3 - year lc rate of 89.0% and a 3 - year overall survival rate of 97.2%.29 another study by bhateja et al25 demonstrated superior lc in patients receiving crt for t2b - 3n0 - 2 glottic cancers compared with patients receiving rt alone for t2n0m0 glottic cancer with impaired vocal cord mobility ( t2bn0 ) , suggesting a potential therapeutic benefit of crt in this setting . 
in this study , 51.6% of the t2bn0 patients treated with rt alone received altered fractionation ( > 2.1 gy per fraction or twice - a - day fractionation ) compared with 38.5% of patients in the crt cohort . 
of note , the crt cohort contained only one patient with t2bn0 and one patient with t2bn1 ; therefore , it is difficult to assess the impact of crt on patients with t2bn0 disease . 
in accordance with the results from bhateja et al , 25 our study also demonstrated that patients with t3n0 glottic scc had decreased dsm with crt compared with rt alone . 
cumulative incidence plots of disease specific mortality ( dsm ) and other - cause mortality ( ocm ) for glottic squamous cell carcinoma at each t stage after propensity score matching . 
to our knowledge , our data from this study are the first to question the utility of chemotherapy in addition to rt for t2bn0 glottic scc . one possible hypothesis for the increase in dsm for patients with t1 - 2n0 glottic scc treated with crt may be treatment prolongation as a result of increased toxicity . 
rt treatment time prolongation past 40 days has been shown to correlate with decreased lc from 95% to 100% to 79% to 84%.13 , 34 additional factors that can contribute to the observed survival detriment in crt may be lower total rt dose and dose per fraction as a result of the higher combined toxicity with chemotherapy , because it has been established that total rt dose less than 65 gy results in decreased lc.2 , 10 , 13 , 14 , 35 furthermore , a randomized prospective study has shown that 2.25 gy per fraction , as compared with 2 gy per fraction , results in significantly improved lc.36 meanwhile , the survival benefit associated with chemotherapy in locally advanced glottic scc may be attributed to improved lc secondary to chemotherapy sensitization and / or additional regional and distant control , which could compensate for the decrease in lc associated with potential treatment prolongation . this study had several important limitations inherent to the seer database , including lack of information on radiation dose , treating physician experience , the type of treatment institution , and sequence of chemotherapy relative to rt , which prevented us from distinguishing between concurrent versus induction chemotherapy . 
however , given the relatively rare use of induction chemotherapy in the modern era for t1 - 2n0 glottic scc , it is reasonable to assume that the patients in the crt cohort of this study predominantly received concurrent crt . 
steinberg honoraria : viewray consulting or advisory role : viewray research funding : viewray , accuray travel , accommodations , expenses : viewray robert chin travel , accommodations , expenses : varian medical systems , brainlab affiliations chenyang wang , amar u . 
spector jg , sessions dg , chao ksc , et al : stage i ( t1 n0 m0 ) squamous cell carcinoma of the laryngeal glottis : therapeutic results and voice preservation . 
laccourreye o , muscatello l , laccourreye l , et al : supracricoid partial laryngectomy with cricohyoidoepiglottopexy for early glottic carcinoma classified as t1 - t2n0 invading the anterior commissure . 
marshak g , brenner b , shvero j , et al : prognostic factors for local control of early glottic cancer : the rabin medical center retrospective study on 207 patients . 
le q - tx , fu kk , kroll s , et al : influence of fraction size , total dose , and overall time on local control of t1t2 glottic carcinoma . 
cellai e , frata p , magrini sm , et al : radical radiotherapy for early glottic cancer : results in a series of 1087 patients from two italian radiation oncology centersi . 
warde p , osullivan b , bristow rg , et al : t1 / t2 glottic cancer managed by external beam radiotherapy : the influence of pretreatment hemoglobin on local control . 
mendenhall wm , parsons jt , million rr , et al : t1t2 squamous cell carcinoma of the glottic larynx treated with radiation therapy : relationship of dose - fractionation factors to local control and complications . 
frata p , cellai e , magrini sm , et al : radical radiotherapy for early glottic cancer : results in a series of 1087 patients from two italian radiation oncology centersii . 
garden as , forster k , wong p - f , et al : results of radiotherapy for t2n0 glottic carcinoma : does the 2 stand for twice - daily treatment ? int j radiat oncol biol phys 55 : 322 - 328 , 2003 20 . 
compton cc , byrd dr , garcia - aguilar j ( eds ) : ajcc cancer staging atlas : a companion to the seventh editions of the ajcc cancer staging manual and handbook ( ed 2 )  . 
gorphe p , blanchard p , breuskin i , et al : vocal fold mobility as the main prognostic factor of treatment outcomes and survival in stage ii squamous cell carcinomas of the glottic larynx . 
forastiere aa , zhang q , weber rs , et al : long - term results of rtog 91 - 11 : a comparison of three nonsurgical treatment strategies to preserve the larynx in patients with locally advanced larynx cancer . 
taguchi t , takahashi m , nishimura g , et al : phase ii study of concurrent chemoradiotherapy with s - 1 in patients with stage ii ( t2n0m0 ) squamous cell carcinoma of the pharynx or larynx . 
van der voet jcm , keus rb , hart aam , et al : the impact of treatment time and smoking on local control and complications in t1 glottic cancer . 
yamazaki h , nishiyama k , tanaka e , et al : radiotherapy for early glottic carcinoma ( t1n0m0 ) : results of prospective randomized study of radiation fraction size and overall treatment time . 
in the clinical pharmacogenetics implementation consortium guideline , fluoropyrimidine treatment in homozygous dpyd variant carriers is discouraged , which implies that a potentially effective anticancer therapy is withheld from these patients.5 in this article , six unique patients with a homozygous or compound heterozygous dpyd variant allele genotype who were treated with tailored fluoropyrimidine treatment are described . 
analyses were part of individual patient care , so institutional review board approval was not applicable . genotyping results showed a homozygous or compound heterozygous dpyd genotype , and the functional effects of these genotypes were uncertatherefore , pretreatment dpd activity was measured in peripheral blood mononuclear cells ( pbmcs )  . 
dpd activity was used to reach an individualized dose , in which the percentage of remaining dpd activity was used as guideline for the starting dose ( expressed as percentage of the originally planned dose )  . pharmacokinetic analyses in three of six patients were performed to investigate whether applied dose reductions were adequate . 
pretreatment plasma uracil , the endogenous dpd substrate , and dihydrouracil levels were quantified ; results were unknown before the start of treatment . results clinical course of treatment patient characteristics are listed in table 1.6 - 9 linda m . 
therefore , it was decided to drastically reduce the capecitabine dose from 2 , 300 mg ( 1 , 000 mg / m2 ) twice daily to 150 mg twice daily ( 6.5% of planned dose ) and to start with capecitabine monotherapy . 
the adverse events resolved within 1 week ( neutropenia ) to 2 months ( diarrhea , mucositis )  . after a 2 - month period without any anticancer therapy , the patient had fully recovered , and monotherapy with capecitabine was restarted . 
on the basis of the severe toxicity and the pharmacokinetic results of the first cycle , the dose was reduced more to 150 mg once every 5 days ( ie , 0.65% of originally planned dose )  . 
this female patient with locally advanced colorectal carcinoma had a planned treatment that consisted of neoadjuvant chemotherapy ( capecitabine 825 mg / m2 twice daily , or 1 , 500 mg ) combined with radiotherapy ( 5 - week schedule )  . pretreatment dpyd screening revealed that the patient was homozygous for c.2846a.t ; dpd activity was reduced to 29% . 
it was decided to reduce the capecitabine dose to 500 mg once daily ( ie , 17% of planned doseslightly lower than recommended dose of 29% on the basis of dpd activity , as decided by physician and patient )  . 
dpd activity was reduced to 45% . remaining dpd activity was more than 50% reduced , so it was considered likely that this patient was a compound heterozygous carrier ( variants present on different alleles )  . 
in the first cycle , capecitabine was reduced to 1 , 800 mg daily ( 51% of planned daily dose of 3 , 500 mg ; 1 , 750 mg / m2 ) , which was tolerated without toxicity . 
however , the patient developed grade 2 thrombocytopenia after 8 days , and the daily capecitabine dose was adjusted to 1 , 000 mg for the rest of the cycle . platelets increased again until normal values were reached . 
after three cycles , disease progression was established , and capecitabine treatment was discontinued . pharmacokinetic results in all three patients , additional pharmacokinetic measurements were performed ( fig 1 )  . 
for patient 1 , only levels of capecitabine and of the metabolites 59 - deoxy - 5 - fluorocytidine , 59 - deoxy5 - fluorouridine , and fu could be quantified ; other fu metabolites were not detectable . 
results of noncompartmental analysis of the pharmacokinetic results in plasma are listed in table 2 and include values normalized to control values.10 in patient 1 , fu exposure was highly increased : the mean area under the plasma concentration - time curve ( auc ) of fu was 4 , 024 ng 3 h / ml , which is 10 times higher than in other pharmacokinetic studies with capecitabine.10 - 13 these results were used for the decision to lower the dose 10 - fold in the second cycle . baseline uracil and dihydrouracil levels are listed in table 1 . 
results of urine analysis for patient 1 are shown in appendix figure a1 . discussion to our knowledge , this is the first report to describe prospectively identified patients , who are homozygous or compound heterozygous for dpyd variants , who could be treated safely with fluoropyrimidines . 
for all three patients , the results after the first intake of capecitabine are depicted . capecitabine patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) 5 ' - dfcr patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) time ( h ) 5 ' - dfur time ( h ) 5 - fu patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) patient 1 ( homozygous dpyd * 2a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) 5 , 000 4 , 000 3 , 000 2 , 000 1 , 000 4 , 000 3 , 000 2 , 000 1 , 000 2 , 500 2 , 000 1 , 500 1 , 000 2 , 500 2 , 000 1 , 500 1 , 000 1 , 200 time ( h ) fuh2 time ( h ) fupa patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) time ( h ) time ( h ) fbal patient 2 ( homozygous c.2846a > t ) patient 3 ( c.2846a > t and c.1236g > a ) time ( h ) pretreatment identification of the patient homozygous for dpyd * 2a with complete dpd deficiency saved this patient from receipt of a full fluoropyrimidine dose , which most likely would have been fatal . 
in patients who are not dpd deficient , fluoro - b - alanine is the major urinary metabolite , 13 , 20 whereas this metabolite was not present in the urine analyzed in the case presented in this paper . 
for example , mir27a polymorphisms could play a role in variation of dpd activity , because these polymorphisms reduce dpd activity.26 , 27 in conclusion , we showed that fluoropyrimidine treatment in homozygous or compound heterozygous dpyd variant allele carriers is feasible and that therapy does not have to be withheld . 
van der veldt consulting or advisory role : ipsen ( inst ) , roche ( inst ) , bristol - myers squibb ( inst ) , pfizer ( inst ) , msd oncology ( inst ) travel , accommodations , expenses : roche paul hamberg no relationship to disclose andr e b.p. 
bioanalysis 7 : 519 - 529 , 2015 van kuilenburg ab , van lenthe h , tromp a , et al : pitfalls in the diagnosis of patients with a partial dihydropyrimidine dehydrogenase deficiency . 
deenen mj , meulendijks d , boot h , et al : phase 1a / 1b and pharmacogenetic study of docetaxel , oxaliplatin and capecitabine in patients with advanced cancer of the stomach or the gastroesophageal junction . 
judson ir , beale pj , trigo jm , et al : a human capecitabine excretion balance and pharmacokinetic study after administration of a single oral dose of 14c - labelled drug . 
van kuilenburg ab , muller ew , haasjes j , et al : lethal outcome of a patient with a complete dihydropyrimidine dehydrogenase ( dpd ) deficiency after administration of 5 - fluorouracil : frequency of the common ivs14 + 1g.a mutation causing dpd deficiency . 
meinsma r , fernandez - salguero p , van kuilenburg ab , et al : human polymorphism in drug metabolism : mutation in the dihydropyrimidine dehydrogenase gene results in exon skipping and thymine uracilurea . 
van kuilenburg ab , meijer j , mul an , et al : intragenic deletions and a deep intronic mutation affecting pre - mrna splicing in the dihydropyrimidine dehydrogenase gene as novel mechanisms causing 5 - fluorouracil toxicity . 
offer sm , butterfield gl , jerde cr , et al : micrornas mir - 27a and mir - 27b directly regulate liver dihydropyrimidine dehydrogenase expression through two conserved binding sites . 
froehlich tk , amstutz u , aebi s , et al : clinical importance of risk variants in the dihydropyrimidine dehydrogenase gene for the prediction of early - onset fluoropyrimidine toxicity . 
int j cancer 136 : 730 - 739 , 2015 patients were treated at three different institutes in the netherlands ( the netherlands cancer institute , amsterdam ; erasmus medical center , rotterdam ; fransciscus gasthuis & vlietland , rotterdam )  . 
toxicity was scored according to the common terminology criteria for adverse events , version 4.03. dpyd genotyping genomic dna was isolated from peripheral blood cells , and screening for the dpyd variants dpyd * 2a ( ivs14 + 1g.a , rs3918290 ) , c.2846a.t ( rs67376798 ) , c.1679t.g ( dpyd * 13 , rs55886062 ) , and c.1236g.a ( rs56038477 ) was performed by using standard operating procedures in two different institutes ( the netherlands cancer institute , amsterdam , and erasmus medical center , rotterdam )  . 
in the netherlands cancer institute , screening for dpyd variants was performed with the roche lightcycler 480ii platform ( roche diagnostics , almere , the netherlands ) by using commercially available probes and primers ( tib molbiol , berlin , germany ) , and results were confirmed by direct sequencing . 
at the erasmus medical center , each sample was genotyped on two different platformstaqman ( with predefined drug - metabolizing enzyme [ dme ] assays ) and pcrrestriction fragment length polymorphism ( rflp ) assaysto allow checks for potentially wrong genotyping . 
both laboratories participated during the study in the dutch national quality control program for dpyd proficiency testing , in which all four dpyd variants were included . dihydropyrimidine dehydrogenase activity in peripheral blood mononuclear cells dihydropyrimidine dehydrogenase ( dpd ) activity was measured in peripheral blood mononuclear cells ( pbmcs ) , isolated from a baseline ( pretreatment ) peripheral blood sample . 
one of two comparable validated methods by van kuilenburg et al7 or pluim et al6 was used ; both used radiolabeled thymine ( 14c - labeled thymine or 3h - labeled thymine ) as a substrate and consisted of high - performance liquid chromatography ( hplc ) with online radioisotope detection and with liquid scintillation counting . 
analytes were extracted by protein precipitation ; chromatographic separation was performed on an acquity ultra - performance liquid chromatography hss t3 column ( acquity waters , milford , ma ) and were analyzed with ms / ms with an electrospray ionization source ( jacobs ba et al : j pharm biomed anal 126 : 75 - 82 , 2016 )  . 
all samples were measured at one institute ( the netherlands cancer institute )  . pharmacokinetic measurements peripheral blood samples for patient 1 were obtained for pharmacokinetic analysis on cycle 1 , day 1 ( c1d1 ) ; cycle 2 , day 1 ( c2d1 ) ; and cycle 2 , day 16 ( c2d16 )  . 
 results dihydrouracil - uracil levels capecitabine intake ( at predose , and at 15 minutes , 30 minutes , 1 hour , 2 hours , 3 hours , 4 hours , 6 hours , 8 hours , and 10 hours after capecitabine intake )  . 
for patients 2 and 3 , samples were collected only on c1d1 , on the same time points as for patient 1 , except for the latest time point ( the sample 10 hours after capecitabine intake was not collected for patient 2 , and the last sample was collected at 12 hours instead of at 10 hours for patient 3 )  . 
for patients 2 and 3 , pharmacokinetic results were not known during treatment , because samples were analyzed after treatment had finished . capecitabine and its metabolites , 59 - deoxy - 5 - fluorocytidine ( 59 - dfcr ) , 59 - deoxy - 5 - fluorouridine ( 59 - dfur ) , fluorouracil ( fu ) , dihydro - 5 - fluorouracil ( fuh2 ) , a - fluoro - ureidopropionic acid ( fupa ) , and fluoro - b - alanine ( fbal ) , were quantified by using hplc coupled to electrospray ms / ms . 
two individual validated assays were used : one for the simultaneous quantification of capecitabine , 59 - dfcr and 59 - dfur and another for fu , fuh2 , fupa , and fbal ( deenen mj et al : j chromatogr b analyt technol biomed life sci 913 - 914 : 30 - 40 , 2013 )  . 
all pharmacokinetic samples were measured at the same institute ( the netherlands cancer institute )  . together with the sample for dpd activity in pbmcs , a pretreatment plasma sample was taken to measure uracil and dihydrouracil levels ( table 1 )  . 
for patients 2 and 3 , uracil levels were increased compared with reference levels ( a value of 28.7 ng / ml for patient 2 and of 35.6 ng / ml for patient 3 ) , and both values were within the top 1% of reference values . 
dihydrouracil levels were in the normal range for patients 2 and 3 compared with reference levels . other homozygous dpyd variant allele carriers three additional patients with a homozygous dpyd variant genotype were identified during routine dpyd screening ( table 1 )  . 
it is unclear why there is a relatively high variation of the effect of this genotype on dpd phenotype in patients , and more research on this variant is advised . in addition , one patient with a homozygous c.2846a.t genotype ( patient 4 ) was identified . 
according to the calculated dpd activity score , as described by henricks et al , 4 it could be concluded that a 50% dose reduction would be appropriate for homozygous c.2846a.t carriers , because a 25% dose reduction is recommended for heterozygous carriers of this variant . 
recent work has determined that 20% to 30% of mcrpc tumors harbor alterations that result in the loss of dna repair capacity , in particular , the homologous recombination pathway.1 , 2 in turn , these alterations may predict response to poly - adp ribosylase ( parp ) inhibitors and platinum chemotherapy , which provides opportunities for precision therapy using agents that are not currently standard or available for mcrpc.3 , 4 in ovarian canceralso frequently marked by homologous recombination deficiencyplatinum is the standard front - line treatment , and parp inhibitors olaparib , niraparib , and rucaparib are now us food and drug administrationapproved for brca1 / 2mutated tumors . 
reversion mutations inbrca1 / 2 , 5 - 8 and more recently in rad51c and rad51d , 9 have previously been described as a mechanism of resistance to platinum and parp inhibitors in ovarian cancer and thus also represent an important consideration in patients with prostate cancer . recently , reversion mutations to restore brca1 / 2 function have been observed in prostate tumors sampled by biopsy and in circulating tumor dna ( ctdna ) from patients who were treated with parp inhibitors.10 , 11 here , we describe a case of a patient with mcrpc who exhibited polyclonal brca2 reversion mutations at the time of disease progression when receiving platinum chemotherapy . 
to our knowledge , this is the first report of brca2 reversions occurring in a patient with prostate cancer in the setting of platinum treatment and mediating resistance to therapy . our patient presented with a prostate - specific antigen ( psa ) of 8.6 ng / ml and gleason 4 + 5 prostate adenocarcinoma in october 2011 at 65 years of age . 
he underwent a radical prostatectomy with bilateral pelvic lymph node dissection in january 2012 with pt3br1n1 ( american joint committee on cancer 7 ) , gleason 5 + 4 staging . 
postoperative psa in april 2012 was 2.7 ng / ml ; restaging scans demonstrated bone involvement in the left iliac wing and l4 vertebral body without lymph node or visceral involvement . he was initially treated with bicalutamide and leuprolide ( a luteinizing hormonereleasing hormone agonist ) , which resulted in undetectable psa by may 2013 . 
in june 2016 , he began treatment with enzalutamide 160 mg once daily , but was noted to have primary refractory disease with a psa increase to 370.3 ng / ml in 1 month . 
black arrow denotes time of circulating tumor dna ( ctdna ) collection . in october 2016 , carboplatin area under the curve 5 was administered based on the results of the metastatic tumor biopsy sequencing . 
after seven cycles , psa increased to 428.1 ng / ml on april 12 , 2017 , concurrent with ctdna draw . samples from the primary prostate tumor , germline dna , and a ctdna sample that was obtained at the time of progression on carboplatin ( march 2017 ) were sequenced by using a clinically validated tumor sequencing next - generation sequencing assay12 and compared with the prechemotherapy metastasis biopsy . 
a frameshift mutation in brca2 ( p.n2452mfs * 17 ) as well as in spop and tp53 mutations were identified in the primary tumor and metastasis ( table 1 )  . 
we did not observe evidence of a germline pathogenic variant . we performed targeted next - generation sequencing on ctdna at the time of progression to 1 , 6103 mean coverage , and identified 90 brca2 reads that carried the frameshift mutation and 1 , 181 wild - type brca2 reads . 
of importance , no reversion mutations were detected in the primary or germline samples . secondary somatic mutations of brca1 / 2 mutations that restore the wild - type open reading frame were initially described as a mechanism of resistance to platinum chemotherapy in ovarian cancer and have subsequently been reported in patients with prostate cancer who were treated with parp inhibitors.5 , 10 , 11 to our knowledge , this is the first example of reversion mutations in the ctdna of a patient with prostate cancer associated with resistance to platinum chemotherapy . our finding provides evidence that polyclonal reversion is a mechanism of resistance to platinum chemotherapy in patients with prostate cancer . prospective clinical trials of parp inhibitors and platinum to exploit the molecular vulnerabilities of prostate cancer with dna repair defects are now underway , and although there is great enthusiasm , resistance to these strategies is expected . we previously described a series of patients with prostate cancer with biallelic brca2 inactivation who had exceptional and sometimes extended responses to carboplatin - based therapy ( up to 3 years ) .4 in addition , a recent retrospective analysis of patients whose prostate cancer was refractory to taxanes found that six ( 75% ) of eight patients who were carriers of pathogenic germline brca2 variants had a psa50 response from 12 weeks of carboplatin plus docetaxel therapy compared with 23 ( 17% ) of 133 noncarriers.15 two prospective clinical trials that are investigating carboplatin table 1 . 
dashed outline represents second allele . sequencing reads with secondary mutations in the plasma circulating tumor dna ( ctdna ) sample taken at the time of progression on carboplatin ( bottom )  . 
images were rendered by using the integrative genomics viewer.13 , 14 with docetaxel for patients with mcrpc and dna repair defects are currently recruiting patients ( clinicaltrials.gov identifiers : nct02598895 and nct02985021 ) and may be opportunities to explore this and other potential resistance mechanisms . the recent finding of secondary reversion mutations in patients with prostate cancer after parp inhibitor therapy occurred within 8 to 10 months of initiating therapy.10 , 11 in our patient , resistance emerged after the same apparent mechanism over approximately 7 months , a more abbreviated benefit compared with the multiple years of response to platinum - based therapy that we have observed and on which we have previously reported.4 our patients case provides evidence that reversion mutations selected by platinum chemotherapies can occur at a similar pace as parp inhibitors and implies that additional factors that are yet to be characterized influence the chronology of resistance to dna - damaging agents . 
although we did not detect a second inactivating mutation in our patient , it is possible that an undetected methylation or a complex rearrangement could be present . nonetheless , evidence of reversion mutations that restore gene function and that temporally coincide with clinical progression during platinum therapy together make a strong case that brca2 gene function was disrupted in the primary and metastatic tumor . it is possible that the mechanism of initial gene inactivation affects resistance . 
for example , patients with biallelic copy loss may be less likely to restore functional copy and thus have a longer response duration compared with those with biallelic singlenucleotide substitutions and / or indels , which might restore gene function more readily to give rise to resistance . 
in addition , although platinum and parp inhibitors share reversion as a mechanism of resistance , patients with ovarian cancer resistant to parp inhibitors can still exhibit sensitivity to platinum , which demonstrates that there are differences as well.16 many unanswered questions remain regarding the noninvasive assessment of resistance . 
 only been identified after selective treatment pressure and not as de novo events , although the lack of detection may reflect mutation levels that are lower than the sensitivity of assays used to detect reversion events . 
in this case , we did not have matched tumor biopsy and ctdna for each clinically relevant time point , although the samples we collected demonstrated proof of an important mechanism of resistance to platinumany in the field are investigating concordance and representative sampling of tumor versus ctdna , which will be important to clinical practice . another critical issue is whether early reversion clones specifically and reliably predict the development and pace of clinical resistance , the differences between platinum and parp inhibitors , and what other potential relevant genetic , epigenetic , and microenvironmental modifying factors are at play . 
nelson consulting or advisory role : janssen oncology , astellas pharma , genentech bruce montgomery research funding : essa pharma , medivation , astellas pharma , janssen oncology , ferring pharmaceuticals colin c . 
pritchard no relationship to disclose acknowledgment we thank arul chinnaiyan , daniel robinson , hiep nguyen , and the stand up to cancer / prostate cancer foundation precision oncology team for their assistance with the collection and analysis of the metastatic biopsy . affiliations support references 417 - 425 , 2017 1697 - 1708 , 2015 all authors , university of washington ; heather h . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . j mol diagn 16 : 56 - 67 , 2014 13 . 
ang je , gourley c , powell cb , et al : efficacy of chemotherapy in brca1 / 2 mutation carrier ovarian cancer in the setting of parp inhibitor resistance : a multi - institutional study . 
 concordance of genomic variants in matched primary breast cancer , metastatic tumor , and circulating tumor dna : the mirror study fernando moreno , md1 ; javier gayarre , phd1 ; sara l opez - tarruella , md , phd1 , 4 , 5 ; mara del monte - mill an1 ; antonio c . 
picornell , phd1 ; enrique alvarez1 ; jos e angel garca - saenz , md , phd1 ; yolanda jerez , md1 ; iv an m arquez - rodas , md , phd1 ; isabel echavarra , md , phd1 ; maribel palomero , md1 ; coralia bueno , md2 ; ana mara arag on bod3 ; marta sanchez muoz , phd3 ; ricardo gonz alez del val , md , phd1 ; oscar bueno , md4 ; mara cebollero - presmanes , md5 ; inmaculada ocaa1 ; ainhoa arias1 ; paula romero , msc1 ; tatiana massarrah1 ; roco ramos - medina , phd1 ; and miguel martn , md , phd1 , 4 , 5 purpose genetic heterogeneity between primary tumors and their metastatic lesions has been documented in several breast cancer studies . 
however , the selection of therapy for patients with metastatic breast cancer and the search for biomarkers for targeted therapy are often based on ndings from the primary tumor , mainly because of the difculty of distant metastasis core biopsies . 
in addition , we identied 13 variants in metastatic tissue and ctdna not present in primary tumor . conclusion we identied genomic variants present in metastatic biopsies and plasma ctdna that were not present in the primary tumor . 
2019 by american society of clinical oncology introduction breast cancer is a heterogeneous disease with different clinical characteristics , disease courses , and responses.1 traditional biomarkers ( estrogen receptor [ er ] , progesterone receptor [ pr ] , and human epidermal growth factor receptor 2 [ her2 ] ) and imaging techniques play important roles in tumor diagnosis and treatment selection.2 however , these biomarkers only offer partial insight into the biology of the tumors . 
in recent years , technologic advances in genomics and the implementation of multi - institutional initiatives have improved our understanding of the landscape of genomic alterations in breast cancer.3 biopsies of metastatic sites are considered the gold standard for both the characterization of genomic alterations in patients with metastatic breast cancer and the search for prognostic and predictive biomarkers . 
 moreno et al context key objective the objective of this study was to evaluate the concordance of genomic variants between primary tumor tissue , metastatic tissue , and circulating tumor dna ( ctdna ) in patients with metastatic breast cancer . knowledge generated next - generation sequencing of metastatic samples shows mutations not present in the primary tumor . 
ctdna analysis with ion torrent technology identied the majority ( 97.2% ) of variants present in primary and metastatic tumors . relevance genotyping of metastases offers additional information for primary tumor analysis . 
ctdna can be used to detect genomic alterations in patients with metastatic breast cancer and could be an alternative to metastatic tissue samples . to determine the concordance of genomic alterations among primary breast cancer , metastatic breast cancer lesions , and ctdna , we conducted the mirror study ( clinicaltrials.gov identier : nct02626039 )  . 
all patients provided written informed consent for the study . patients included in the study had histologically conrmed progressive metastatic breast cancer before starting a new line of treatment and were at least 18 years old . 
exclusion criteria were metastatic bone disease only , coagulation disorders , and eastern cooperative oncology group performance status of 3 or 4.10 study objectives the primary objective of this study was to assess the concordance of genomic variants between primary tumor tissue and metastatic tissue in patients with metastatic breast cancer . 
secondary objectives included determining ctdna mutation proles from peripheral blood and comparing them with those from the primary tumor and metastatic tissue . study procedures eligible patients underwent a biopsy of a metastatic site . blood samples were obtained within a window of 30 days , spanning 15 days before or after the biopsy procedure . parafn blocks of matched primary tumor and metastasis tissues , as well as plasma samples , were used for genomic studies . 
the mirror project was a pilot study , and the sample size was established empirically . a recruitment rate of two fully evaluable patients per month for up to 2 years was considered a reasonable target . 
for solid tumor and ctdna samples , a minimum mean coverage of 5 , 000 and 15 , 000 , respectively , was established . we focused on single - nucleotide substitutions and small indels . 
single - nucleotide substitutions were ltered as follows : ( 1 ) rare variants ( minor allele frequency , 0.01 ) , ( 2 ) variants in coding exons and splice junctions ; ( 3 ) variants predicted to produce synonymous amino acid changes were discarded ( we selected only high / mediumimpact variants : frameshift indels and nonsense , missense , and canonical splice - site variants ; appendix ) ; ( 4 ) we then discarded benign and probably benign classied variants , as dened in different databases , which are listed in table 2 . 
variants were classied according to the american college of medical genetics and genomics guidelines.16 identication of variants from ffpe samples and plasma for ffpe - derived dna , variant calls with a mutant allelic fraction of 2% or greater in the paired solid tumor ( primary and metastasis ) tissues were selected . 
for ctdna , variants with at least two reads in one strand supporting variant alleles with a minimum region - coverage depth of 20 were retained . three comparisons were made sequentially . 
finally , to identify potential mechanisms of resistance to specic therapies , we analyzed genetic variants present in both metastatic tissue and ctdna but not in primary tumors ( fig 1 )  . conrmation of selected variants selected variants identied by ion torrent technology was conrmed using ngs technology ( illumina , san diego , ca ) the genomic unit of university hospital gregorio mara on ( madrid , spain )  . 
we designed a customized truseq panel ( custom amplicon low input kit , illumina ) to sequence 116 amplicons . genomic dna ( 10 ng ) was used to prepare libraries from two pools of paired oligos , following the manufacturers recommendations ( truseq custom amplicon low input kit , procedure dual strand v04 ; illumina )  . 
the libraries were sequenced on a miseq platform ( illumina ) with miseq reagent v2 ( 2 150 bp )  . sequence data were analyzed using the miseq reporter 2.6.2 ( illumina ) and igv win 2.4.3 software ( broad institute and the regents of the university of california )  . patient characteristics and samples analyzed between november 2013 and march 2017 , 80 patients who met the inclusion criteria and provided informed consent were enrolled ( fig 2 )  . 
 moreno et al primary tumor customized 54 - cancer gene panel ( ion torrent technology ) metastatic tumor plasma ( ctdna ) common variants present in primary tumor , metastatic tumor , and ctdna . common variants present in metastatic tumor and ctdna , not present in primary tumor . genetic variant validation ( illumina techonology ) fig 1 . 
dna was obtained from primary tumors , metastases ( liver , lung , skin , brain , lymph nodes , local relapse in breast , and bone ) , and plasma samples . 
genomic variants were identied using ion torrent technology ( thermofisher scientic , waltham , ma ) and were validated using illumina technology ( illumina , san diego , ca )  . when we reached the intended sample size of 40 patients who met the inclusion criteria , and with valid samples from the three sources ( primary and metastatic tumor biopsies and plasma ) , we proceeded to genomic variant analyses . pathologic analysis of primary tumors revealed that 17 patients ( 42.5% ) had hormone receptor - positive / her2negative disease , 15 patients ( 37.5% ) had her2 - positive disease , and seven patients ( 17.5% ) had triple - negative disease . 
pathologic analysis of metastatic biopsies revealed that 14 patients ( 35% ) had hormone receptor - positive / her2 - negative disease , 16 ( 40% ) had her2 - positive disease , and 10 ( 25% ) had the triple - negative phenotype . all patients had received antitumor drug therapy in the adjuvant and / or metastatic setting . 
most patients ( n = 33 ; 82.5% ) had received drug therapy for advanced disease , and only seven patients ( 17.5% ) had not received treatment in the metastatic setting . 
thirty - ve patients were previously exposed to ( neo ) adjuvant therapy , whereas ve patients had not received drug treatment of early - stage breast cancer ( table 3 )  . 
missense variants were the most frequently observed ( 81 ; 76% ) , followed by nonsense variants ( 13 ; 12% ) , frameshift variants ( 10 ; 9% ) , and indels not leading to frameshift ( 3 ; 3% ; appendix fig a1 )  . twenty - two of the variants were considered pathogenic ( 21% ) , 10 were considered likely pathogenic ( 9% ) , and 75 were of uncertain signicance ( 70% ; fig 4b )  . 
erbb2 mutations ( val777_ gly777insglyserpro and val777leu ) were found only in her2 - positive tumors , with a mutation frequency in her2 - positive metastatic tumors of 12.5%. variant analysis using ion torrent technology the median read coverage was 6 , 930 ( range , 5 , 354 to 9 , 324 ) for primary and metastatic tumor tissues and 15 , 400 ( range , 10 , 942 to 24 , 090 ) for ctdna . 
most of the variants ( 107 of 110 ) we identied 13 variants in metastatic tumors and ctdna that were not detected in the corresponding primary tumors ( fig 4d )  . 
 ( % ) er positive / her2 negative er positive / her2 positive er negative / her2 positive er negative / her2 negative ki 67 primary , % ( range ) ki 67 metastasis , % ( range ) stage at diagnosis , no . 
 ( % ) abbreviations : er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; n / a , not available . in the metastatic setting than in the adjuvant setting ( three v one patient , respectively )  . conrmation of selected variants using illumina technology material was available for independent validation using illumina technology for 38 of the 40 patients . 
of the 13 variants commonly detected in metastatic tumors and ctdna samples but not in the primary tumors using ion torrent , 12 ( 92.3% ) were conrmed by illumina data ( fig 3 )  . discussion tumor genotyping is an important and evolving area of research in metastatic breast cancer . 
in many metastatic breast cancer clinical trials involving predictive biomarker identication , primary tumors have been mainly used because metastatic samples are more difcult to obtathe precise bias introduced by this approach is unknown . various studies have shown substantial genomic differences between primary and metastatic breast cancer tissues , which probably arise as a consequence of tumor evolution under the selective pressure of therapies.4 , 5 in the primary tumors . we used two independent ngs platforms to identify and conrm single - nucleotide changes and indels in primary tumor and metastases from 40 patients with breast cancer . 
in addition , we identied 13 pathogenic or likely pathogenic variants that were present in metastatic tumors and plasma samples , but illumina technology conrmed 85.5% of primary and metastatic common variants originally detected by ion torrent . 
these ndings conrm those of previous studies suggesting that , although most variants present in the primary tumor were also present in metastatic tissue , mutations not present in the primary tumor can be found in metastases.4 , 5 , 17 therefore , metastatic tissue and , alternatively , ctdna , rather than primary tumor tissue could be the most appropriate source of dna material identifying biomarkers for new drugs in breast cancer clinical trials or for selecting patients for current targeted therapies . the detection of ctdna variants in patients with metastatic cancer primarily depends on variant allele frequencies in plasma.18 - 20 because of the extremely low ratio of ctdna / cell - free dna in the blood , ctdna detection largely depends on new technologies with high sensitivity and specicity . 
roth e et al26 used a similar approach to analyze 2 , 800 cosmic mutations distributed across 50 genes using ion ampliseq cancer hotspot panel v2 ( life technologies , carlsbad , ca ) in matched plasma and metastatic tumor samples collected simultaneously . 
the concordance between ctdna and tissue biopsy results in breast cancer suggests that ctdna assays could be condently used to molecularly stratify patients for prognostic and predictive purposes . taken together , our results show that ctdna can be used to detect genomic alterations in patients with metastatic breast cancer . 
if conrmed in larger studies , this nding might be of relevant practical interest , eliminate the need for many invasive biopsies , and allow monitoring of metastatic breast cancer over the course of the disease . one of the challenges in the treatment of metastatic breast cancer is the emergence of mechanisms of resistance . increased knowledge of resistance mechanisms may help to select targeted therapies at the time of progression . 
we identied six likely pathogenic variants in three different genes , esr1 , akt1 , and braf , that are present in metastatic tissues and plasma , but not in primary tumors . esr1 mutations are associated with resistance to aromatase inhibitors , but may be sensitive to fulvestrant , an estrogen receptor downregulator.27 we detected esr1 mutations in ctdna and metastatic biopsies of four patients . 
consistent with previous reports , esr1 mutations were present only in er - positive patients with breast cancer previously treated with aromatase inhibitors and were predominantly acquired during the treatment of metastatic disease.28 the strengths of this study include the availability of triple - matched samples from individual patients with breast cancer , concomitant extraction of blood and biopsy samples , and the rigorous analytic methodology . one of the limitations of our study is the lack of study of ctdna to identify variants of germinal orighowever , many variants can be considered somatic if they meet certain criteria ( a variant allele fraction substantially less than 50% , a recurrent somatic variant with clinical signicance in cancer , is not commonly observed in population databases )  . 
nearly all the variants ( 107 of 110 ) were also detected in plasma circulating tumor dna ( ctdna )  . thirteen variants were identied in metastatic tumor and ctdna samples , but not in the corresponding primary tumor . 
however , the main objective of the study was the correlation between ndings in primary tumor , the nature metastases , and ctdna regardless of ( inherited or acquired ) of the variant . 
other limitations include a low number of patients , a relatively large fraction of patients for whom the three determinations were not available , heterogeneity of breast cancer phenotypes , and differential drug exposure of the pathese biases , we are tients . 
 moreno et al tp53 kmt2c pik3ca ptpn14 brca2 lrp1b gata3 erbb2 tbx3 ptprd pik3r1 ncor1 herc1 ctnna1 ctcf cdh5 cdh1 araf tbx5 runx1 pten map3k1 kras foxp1 egfr cdkn1b ccnd3 brca1 akt1 aff2 fig 4 . 
characteristics of variants identied in ( a ) distrithis study . bution , per gene , of the 107 common variants in primary tumors , metastatic tumors , and cirtumor dna culating ( ctdna )  . 
 mirror study : breast cancer tumor and ctdna genomic concordance in conclusion , our study showed that mutations present in breast cancer metastases , but not in the primary tumor , can be identied using ngs technologies . 
 moreno et al ricardo gonz alez del val research funding : novartis ( inst ) travel , accommodations , expenses : daiichi sankyo oscar bueno research funding : novartis ( inst ) inmaculada ocaa research funding : novartis ( inst ) ainhoa arias research funding : novartis ( inst ) paula romero research funding : novartis ( inst ) tatiana massarrah consulting or advisory role : novartis , astrazeneca , seom , roche , novartis speakers bureau : roche research funding : novartis ( inst ) patents , royalties , other intellectual property : methods for selecting , manipulating , and isolating circulating tumor cells in body uids by laserassisted transfer ( inst ) travel , accommodations , expenses : novartis , astrazeneca , novartis roco ramos - medina research funding : novartis ( inst ) patents , royalties , other intellectual property : methods for selecting , manipulating , and isolating circulating tumor cells in body uids by laserassisted transfer ( inst ) miguel martn consulting or advisory role : genentech , novartis , pzer , eli lilly , astrazeneca , taiho pharmaceutical , pharmamar research funding : novartis ( inst ) , roche patents , royalties , other intellectual property : methods for selecting , manipulating , and isolating circulant tumor cells in body uids by lasser transfer no other potential conicts of interest were reported . acknowledgment the authors thank carmen flores for collaboration on this study , as well as the patients with breast cancer who agreed to participate . references balko jm , stricker tp , arteaga cl : the genomic map of breast cancer : which roads lead to better targeted therapies ? breast cancer res 15 : 209 , 2013 colomer r , aranda - l opez i , albanell j , et al : biomarkers in breast cancer : a consensus statement by the spanish society of medical oncology and the spanish society of pathology . 
clin transl oncol 20 : 815 - 826 , 2018 [ erratum : clin transl oncol 20 : 1093 - 1095 ] swanton c , soria j - c , bardelli a , et al : consensus on precision medicine for metastatic cancers : a report from the map conference . 
mol cancer ther 13 : 1382 - 1389 , 2014 goswami rs , patel kp , singh rr , et al : hotspot mutation panel testing reveals clonal evolution in a study of 265 paired primary and metastatic tumors . 
n engl j med 366 : 883 - 892 , 2012 russnes hg , navin n , hicks j , et al : insight into the heterogeneity of breast cancer through next - generation sequencing . 
j clin invest 121 : 3810 - 3818 , 2011 gonzalez - rivera m , picornell ac , alvarez el , et al : a cross - sectional comparison of druggable mutations in primary tumors , metastatic tissue , circulating tumor cells , and cell - free circulating dna in patients with metastatic breast cancer : the mirror study protocol . 
hammond meh , hayes df , dowsett m , et al : american society of clinical oncology / college of american pathologists guideline recommendations for immunohistochemical testing of estrogen and progesterone receptors in breast cancer . 
wolff ac , hammond meh , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
sci transl med 6 : 224ra24 , 2014 jovelet c , ileana e , le deley m - c , et al : circulating cell - free tumor dna analysis of 50 genes by next - generation sequencing in the prospective moscato trial . clin cancer res 22 : 2960 - 2968 , 2016 20 . 
kim st , lee w - s , lanman rb , et al : prospective blinded study of somatic mutation detection in cell - free dna utilizing a targeted 54 - gene next generation sequencing panel in metastatic solid tumor patients . 
roth e f , laes j - f , lambrechts d , et al : plasma circulating tumor dna as an alternative to metastatic biopsies for mutational analysis in breast cancer . 
schiavon g , hrebien s , garcia - murillas i , et al : analysis of esr1 mutation in circulating tumor dna demonstrates evolution during therapy for metastatic breast oncol 25 : 1959 - 1965 , 2014 34 : 2961 - 2968 , 2016 cancer . 
brody , phd3 ; lola rahib , phd4 ; emily lyons , ma4 ; patricia de arbeloa , md2 ; andrew hendifar , md , mph5 ; sameh mikhail , md6 ; vincent chung , md7 ; davendra p.s. 
matrisian , phd , mba4 ; and emanuel petricoin iii , phd2 , 9 purpose up to 25% of pancreatic adenocarcinomas ( pdacs ) harbor mutations in the homologous recombination dna damage response ( hr - ddr ) pathway . 
although known to affect responsiveness to dnadamaging chemotherapy , the prognostic relevance of these mutations is unclear and outcomes in patients with pdac who harbor hr - ddr mutations beyond brca1 / 2 remain unexplored . methods we evaluated 820 patients with pdac enrolled in the know your tumor program for whom we had collected comprehensive genomic testing results and longitudinal clinical outcomes . 
mos in patients with mutations in all three hr - ddrmut groups was greater than that for phr - ddr patients , but this difference was lost in platinum - nave patients . conclusion patients with advanced hr - ddrmut have improved mos when treated with platinum - based therapy compared with phr - ddr patients . 
with a 5 - year median overall survival ( mos ) of only 9% , pdac is poised to become the second leading cause of cancer - related death in the united states.1 treatment of metastatic pdac has improved with the use of uorouracil , oxaliplatin , and irinotecan ( folfirinox ) , and gemcitabine plus nab - paclitaxel , but mos remains less than 1 year.2 , 3 however , there is a substantial group of outlier patients whose survival exceeds the median of less than 1 year . 
 pishvaian et al context key objective up to 25% of pancreatic adenocarcinomas ( pdacs ) harbor mutations in the homologous recombination dna damage response ( hr - ddr ) pathway . 
we evaluated 820 patients with pdac who were enrolled in the know your tumor program for whom we had collected comprehensive genomic proling data and longitudinal clinical outcomes to assess the prognostic and predictive value of hr - ddr mutations . knowledge generated patients with advanced pdac and the presence of a somatic or germline hr - ddr mutation have an improved median overall survival ( mos ) when treated with platinum - based therapy compared with patients with no hr - ddr mutation . 
in platinumnave patients , there is no mos difference , which suggests that hr - ddr status has no pure prognostic value . relevance these ndings support the need to test all patients with advanced pdac to ensure that patients whose tumors harbor hr - ddr mutations receive the benet of treatment with platinum - based therapy . prolonged stable disease of 15 patients with pdac who were treated with parpi - based therapy , whereas kaufman et al21 reported one complete response and four partial responses of 23 brca - mutated patients with pdac who were treated with olaparib . 
combinations with chemotherapy may be even more promising , as oreilly et al17 reported a 78% response to the combination of gemcitabine , cisplatin , and veliparib in patients with brcaor palb2mutated pdacs . the treatments received , or we evaluated whether patients with hr - ddrmutated tumors have a biologically better prognosis , irrespective if patients with hrddrmutated tumors have longer than average survival strictly because the underlying mutation predicts for a high degree of responsiveness to platinum - based therapies ( part of the standard of care )  . methods patient recruitment into the know your tumor registry as reported , 4 patients with pdac were identied through the pancreatic cancer action network patient central call center , referred to perthera , and enrolled via an institutional review boardapproved registry protocol . 
study protocol , amendments , and informed consent forms were approved by the new england institutional review board . vestigators obtained informed consent from each participant or participants guardian before enrollment . 
the research was conducted in accordance with recognized ethical guidelines , including the declaration of helsinki , for international organizations of medical scicouncil ences , belmont report , and us common rule , as described during training in good clinical practice guidelines ( collaborative institutional training initiative training )  . patients with biopsy - conrmed pdac were included in the analysis cohort . 
patients with pancreatic adenosquamous carcinoma or other histologic subtypes were excluded . next - generation dna sequencing and identication of hr - ddr status formalin - xed , parafn - embedded blocks and / or slides were collected by surgical resection ( eg , whipple procedure or distal pancreatectomy ) , core - needle biopsy , or ne - needle aspiration . 
coverage of hr - ddr genes tested was relatively uniform with 97% of genomic testing completed by foundation medicine ( cambridge , ma ) , 1% by caris life sciences ( irving , tx ) , and the remaining by including in - house pathology deother partments . 
genomic alterations reported by the testing laboratory included both somatic and germline mutations ; however , it is important to note that the germline versus somatic status of each mutation could not be determined on the basis of tumor proling without parallel genetic sequencing of matched normal blood or tissue . patient tumor genomic proles were reviewed and pathogenic mutations were conrmed by pertheras molecular tumor board participants on a case - by - case basis . 
tumors that harbored no hr - ddr mutations were labeled ddr procient ( phr - ddr )  . results patient history and outcomes enrolled patients signed a health insurance portability and accountability act waiver , and for patient history and longitudinal outcomes assessment , patient coordinators the patients requested updated medical records until death . 
to reduce variability as a result of the timing of enrollment and to establish a denitive starting point for the determination of mos , survival was calculated from the initial date of diagnosis of pdac until death . 
patients were categorized herein as those who underwent a resection of the primary tumor at any point during their treatment history ( resected ) or and as those who had advanced disease at presentation , including locally advanced , never resected patients , and patients with metastatic disease at presentation . 
furthermore , patients were designated as platinum exposed if they received any platinum - containing therapy at any point during the course of their pancreatic cancer survival . statistical analysis all statistical analyses were performed in an r / bioconductor programming environment.22 mos was measured from the date of initial diagnosis until the date of death or the last date the patient was known to be alive . median progression - free survival ( mpfs ) was measured from the start date to the last date the patient was known to be on treatment without progression of disease . 
differences between groups were evaluated for statistical signicance using cox proportional hazards regression models ( the coxph function in the r survival package )  . computed values reported include mpfs , mos , p values , hazard ratios , and 95% cis for hazard ratios . a multivariable approach was implemented to delineate prognostic versus predictive effects of hr - ddr status using the entire analysis cohort . 
given the limitations of interpreting several pairwise comparisons across small groups of patients , we accounted for three binary independent factors : platinum exposure , hr - drr status , and resectability . 
multivariable cox proportional hazards regression was performed on os analysis data by factoring in platinum exposure as one variable , the presence of an hr - ddr alteration as a second variable , interaction between the rst and second variable , and a third variable to account for the patients resection status , which is known to have a highly signicant prognostic impact on os . of 1 , 140 patients with pdac who were enrolled in the know your tumor program between january 2013 and the end of december 2018 , 820 patients with molecular testing results , collection of longitudinal outcomes , and adequate treatment history were included in the analysis cohort . median age at diagnosis was 62 years ( range , 28 to 90 years ) , 52% of patients were male , and 81% of patients were white ( table 1 )  . 
prevalence of somatic or germline hr - ddr mutations ( 16.5% ) and other baseline characteristics was not signicantly different within the resectable and advanced cohorts ( table 1 )  . 
at a median follow - up of 637 days and 386 days for the resected and advanced cohorts , respectively , 47.6% of patients were last known to be alive and 29.2% of patients had not received platinum - based therapy . 
twentyve percent of deceased patients never received any platinum - based therapy . assessing the prognostic value of hr - ddr mutations in platinum - nave patients to assess the prognostic value of the presence of an hrddr mutation , in the absence of the confounding variable of the known predictive value of response to platinum - based therapy , we chose to assess outcomes in patients who never received platinum - based therapy at any time during their pancreatic cancer survival . 
these patients were labeled platinum nave and included 108 resected and 133 advanced patients for analysis ( table 1 and figs 1a and 1b )  . differences in mos were not statistically signicant when comparing hr - ddrmut with phr - ddr patients whose disease was platinum nave in both the resected and advanced subgroups . 
thus , there was no apparent positive prognostic value associated with the presence of an hrddr mutation in platinum - nave patients with pdac . conrming the predictive value for platinum - based therapy of an hr - ddr mutation we also assessed the predictive value for platinum - based therapy of an hr - ddr mutation ( figs 1c and 1d and table 2 )  . 
percentages of patients on the basis of ethnicity / race were only calculated for those for whom ethnicity / abbreviations : hr - ddrmut , homologous recombination dna damage response mutated ; n / a , not applicable ( demographic percentages were calculated for patients for whom the ethnicity / race were known ) ; pdac , pancreatic adenocarcinoma ; phr - ddr , homologous recombination dna damage response procient . after the diagnosis of pdac was established , then the patient was considered platinum treated . 
platinum - based regimens typically included folfirinox ( 85% in rst line and 39% in second line ) ; infusional uorouracil , leucovorin , and oxaliplatin ( 10% in rst line and 52% in second line ) ; or cisplatin with or without gemcitabine ( 3% in rst line and 7% in second line )  . 
variables in the analysis included the main effect of hr - ddr mutations ( prognostic term ) , the main effect of platinum exposure ( treatment term ) , an interaction between these two variables ( predictive term ) , and surgical status ( resectability term )  . 
genomic mutations in homologous recombination dna damage response ( hr - ddr ) genes are not prognostically favorable in patients with pancreatic adenocarcinoma who did not receive platinum - based chemotherapy . 
median overall survival ( mos ) differences on the basis of hr - ddr status were not signicant in platinum - nave patients diagnosed with either ( a ) resectable or ( b ) advanced disease . 
for patients with advanced disease who received platinum - based therapy , there was also an increased progression - free survival for hr - ddrmutated ( hr - ddrmut ) versus hr - ddrprocient ( phr - ddr ) patients in both the ( e ) rst line and ( f ) second line and later setting . 
instead , this trend ( not signicant ) suggested a potentially unfavorable prognostic effect for patients with mutations in the hr - ddr pathway , as shown in figures 1a and 1b . 
when factoring these four variables into our analysis , this model captures the value of hr - ddr mutations as a predictive class of biomarkers for increased responsiveness to platinum agents ( table 3 ) and indicates that this benet is not likely associated with an independent prognostic effect of hr - ddr mutations . assessing which ddr mutation confers the most predictive value the ddr pathway encompasses a functionally diverse network of interacting components spanning more than 50 enzymes ( fig 2 ) , many of which are critical for different aspects of the ddr process across a wide range of biologic contexts . 
atm and atr are critical for sensing double - stranded dna breaks and initiating a series of processes that allow a cell to recognize dna damage and halt the cell cycle until the damage is repaired . 
finally , mrn complex proteins and fanconi anemia core proteins play secondary , yet critical roles in the hr - ddr process . to assess which hr - ddr mutation ( s ) conferred the strongest predictive value to platinum - based therapy , we grouped the hr - ddr mutations into three groups ( fig 2 )  . 
hr - ddr subclassications ( group 1 , group 2 , and group 3 ) are based on the strength of evidence supporting each genes association with increased responsiveness to poly ( adp - ribose ) polymerase inhibitors and / or platinum agents . outcomes for each of the three groups were compared with phr - ddr patient outcomes . 
the number of patients in each group was small , but analysis that was focused on advanced patients conrmed that presence of an hr - ddr mutation is not prognostic , but is predictive of response to platinum - based that therapy . 
advanced pancreatic adenocarcinoma tumors with genomic mutations in hr - ddr genes were compared with the hr - ddrprocient ( phr - ddr ) cohort separately for groups 1 , 2 , and 3 , dened as follows : group 1 ( those with known clinical evidence of predictive value ) ; group 2 ( other genes with strong preclinical evidence of a suspected predictive value ) ; and group 3 ( other genes with preclinical evidence of a role in hr - ddr )  . 
in fact , there may be a trend toward worse outcomes in platinum - nave hr - ddrmut patients compared with platinum - nave phr - ddr patients , although not statistically signicant . in contrast , patients with advanced pdac with hr - ddrmut tumors who received at least one platinum - based regimen had a signicantly longer mos ( by nearly a full year ) compared with platinum - treated patients with phr - ddr tumors . 
this trend was also observed in resected patients who received any platinum - based therapy with an mos difference of nearly 1.5 years that we anticipate will become signicant as this cohort grows and data mature . 
moreover , for hr - ddrmut patients , mos was three times greater in the platinum - exposed versus platinum - nave patients . these results suggest that optimal therapy for hr - ddrmut patients includes a platinum - containing regimen . 
it is currently estimated that 17% to 25% of pdacs harbor somatic or germline hr - ddr mutations , 5 - 7 , 9 - 13 but only 50% of advanced patients are treated with platinum - based therapy in the rstline setting , and less than 50% of patients treated in the rstline go on to receive second - line therapy at all.2 this suggests that up to 25% of patientsnumerically up to 1 , 500 patients with pdac annuallywith hr - ddr mutated tumors are not being optimally treated with platinum - based therapy during the course of their pancreatic cancer survival . 
in addition , it is possible that patients with hr - ddrmutated pdacs who have undergone resection would have a greater chance for cure with an adjuvant platinum - based regimen , such as folfirinox , 23 instead of a nonplatinum - based regimen , such as gemcitabine plus capecitabine.24 there are limitations to this registry study . 
although testing results and treatment considerations were provided to the treating oncologist in real time , there was no prospective intervention to ensure that patients were treated according to the molecular test results . 
thus , this was a retrospective analysis of patients prospectively captured into the registry . longitudinal outcomes data were not yet furthermore , mature or not available for approximately 28% ( 320 of 1 , 140 ) of patients enrolled . 
second , although parallel genetic sequencing results of normal tissue or blood samples were not available to assess the germline status of the hrddr mutations identied in this study , approximately 54% of alterations in this pathway are estimated to be of germline origin on the basis of next - generation sequencing of pdac tumors.25 the relative impact of somatic versus germline hr - ddr mutations on responsiveness to platinums or parpi remains an important question to be answered , and one recent study in pdac demonstrated that patients with conrmed somatic - only brca2 mutations did still respond to the parpi rucaparib.19 additional studies are warranted to investigate the scope of hr - ddr pathway genes / variants and the types of molecular alterations ( eg , germline mutations with or without loss of heterozygosity in the tumor ) that are of clinical relevance . nevertheless , universal adoption of molecular proling of patients with pdac is growing , despite being a controversial issue . 
in april 2019 , the national comprehensive cancer network ( nccn ) modied their language for germline testing for patients with pdac.26 recognizing that up to 40% of patients with germline hr - ddrmutated pdac do not have any signicant family history to suggest a predisposing syndrome , such as a breast / ovarian cancer syndrome , 27 the new nccn guidelines state that germline testing is recommended for all patients with pancreatic cancer . 
recognizing that even somatic hr - ddr mutations may be therapeutically relevant and that germline testing alone may miss patients who could potentially benet from platinum - based therapy , the nccn went on to state that tumor / somatic testing is also recommended for patients with advanced pdac to identify uncommon but actionable mutations . 
matrisian , emmanuel petricoin iii administrative support : kimberly mason provision of study materials or patients : patricia de arbeloa , andrew hendifar , kimberly mason collection and assembly of data : michael j . 
pishvaian stock and other ownership interests : perthera honoraria : caris life sciences , celgene , sirtex medical , merrimack pharmaceuticals consulting or advisory role : caris life sciences , perthera , celgene , sirtex medical , astrazeneca , medimmune , renovorx , armo biosciences , rafael pharmaceuticals , ignyta , merck research funding : genentech ( inst ) , celldex ( inst ) , merck ( inst ) , glaxosmithkline ( inst ) , medimmune ( inst ) , pzer ( inst ) , gilead sciences ( inst ) , regeneron ( inst ) , novartis ( inst ) , karyopharm therapeutics ( inst ) , pharmacyclics ( inst ) , bristol - myers squibb ( inst ) , bayer ( inst ) , curegenix ( inst ) , calithera biosciences ( inst ) , tesaro ( inst ) , bavarian nordic ( inst ) , halozyme ( inst ) , armo biosciences ( inst ) , fibrogen ( inst ) , celgene ( inst ) patents , royalties , other intellectual property : perthera patient matching algorithm travel , accommodations , expenses : caris life sciences , sirtex medical , perthera , astrazeneca , medimmune edik m . 
blais employment : astrazeneca ( i ) , perthera stock and other ownership interests : perthera patents , royalties , other intellectual property : inventor on patents led by perthera ( as an employee ) jonathan r . 
brody stock and other ownership interests : perthera consulting or advisory role : perthera travel , accommodations , expenses : perthera patricia de arbeloa employment : perthera andrew hendifar consulting or advisory role : novartis , ipsen , perthera , celgene , abbvie research funding : ipsen travel , accommodations , expenses : halozyme sameh mikhail consulting or advisory role : ipsen , perthera vincent chung consulting or advisory role : celgene , perthera , ipsen , five prime therapeutics speakers bureau : celgene , ipsen , astrazeneca davendra p.s. 
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n engl j med 369 : 1691 - 1703 , 2013 pishvaian mj , bender rj , halverson d , et al : molecular proling of patients with pancreatic cancer : initial results from the know your tumor initiative . 
clin cancer res 24 : 5018 - 5027 , 2018 aguirre aj , nowak ja , camarda nd , et al : real - time genomic characterization of advanced pancreatic cancer to enable precision medicine . 
cancer discov 8 : 1096 - 1111 , 2018 lowery ma , jordan ej , basturk o , et al : real - time genomic proling of pancreatic ductal adenocarcinoma : potential actionability and correlation with clinical phenotype . 
clin cancer res 23 : 6094 - 6100 , 2017 bailey p , chang dk , nones k , et al : genomic analyses identify molecular subtypes of pancreatic cancer . 
domchek sm , aghajanian c , shapira - frommer r , et al : efcacy and safety of olaparib monotherapy in germline brca1 / 2 mutation carriers with advanced ovarian cancer and three or more lines of prior therapy . 
lowery ma , kelsen dp , stadler zk , et al : an emerging entity : pancreatic adenocarcinoma associated with a known brca mutationclinical descriptors , treatment implications , and future directions . 
oreilly em , lee jw , lowery ma , et al : phase 1 trial evaluating cisplatin , gemcitabine , and veliparib in 2 patient cohorts : germline brca mutation carriers and wild - type brca pancreatic ductal adenocarcinoma . 
oreilly em , lowery ma , segal mf , et al : phase ib trial of cisplatin ( c ) , gemcitabine ( g ) , and veliparib ( v ) in patients with known or potential brca or palb2mutated pancreas adenocarcinoma ( pc )  . 
neoptolemos jp , palmer dh , ghaneh p , et al : comparison of adjuvant gemcitabine and capecitabine with gemcitabine monotherapy in patients with resected pancreatic cancer ( espac - 4 ) : a multicentre , open - label , randomised , phase 3 trial . 
singhi ad , george b , greenbowe jr , et al : real - time targeted genome prole analysis of pancreatic ductal adenocarcinomas identies genetic alterations that might be targeted with existing drugs or used as biomarkers . 
 precision oncology in sarcomas : divide and conquer roberto carmagnani pestana , md1 ; roman groisberg , md1 ; jason roszik , phd , mba1 ; and vivek subbiah , md1 sarcomas are a heterogeneous group of rare malignancies that exhibit remarkable heterogeneity , with more than 50 subtypes recognized . 
advances in next - generation sequencing technology have resulted in the discovery of genetic events in these mesenchymal tumors , which in addition to enhancing understanding of the biology , have opened up avenues for molecularly targeted therapy and immunotherapy . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction sarcomas are a heterogeneous group of mesenchymal malignancies that comprise less than 1% of adult and 12% of pediatric cancers.1 , 2 the who has dened more than 50 sarcoma subtypes , including a wide array of tumors that arise from adipose , muscular , tissues.3 treatment bone , cartilage , and vascular options for patients with advanced soft tissue sarcomas ( stss ) are limited , and a one - size - ts - all paradigm has prevailed despite the diverse nature of stss . for metastatic stss , anthracycline - based chemotherapy remains the backbone of rst - line treatment regimens.4 however , efcacy is limited , with a median progression - free survival ( mpfs ) of approximately 6 months , and the incidence of treatment - associated adverse events ( aes ) is high.5 therefore , more individualized treatment options are critical to improve the survival and quality of life of this patient population . reecting sts heterogeneity , multiple molecular pathways are implicated in the development and progression of these cancers . 
the characterization of specic genetic aberrations has led to the identication of novel diagnostic , prognostic , and predictive biomarkers.6 an understanding of the prevalence and function of specic genetic alterations in sts subtypes is critical to developing more - effective diagnostic tests and therapeutic approaches . 
targeted therapies have the potential to produce signicant tumor response by disrupting molecular pathways that drive oncogenesis , thus providing highly personalized treatment.7 a recent report by lucchesi et al8 analyzed 584 patients with sts in the american association for cancer research ( aacr ) project genomics evidence neoplasia information exchange ( genie ) database and identied that 41% of patients harbored a genetic to inuence therapy . 
acalteration with potential cordingly , a single - center report by boddu et al9 analyzed 114 patients with sarcoma and identied that 49% carried a mutation deemed actionable ; 15 patients had next - generation sequencing ( ngs ) guided therapies , with 26% of these achieving clinical benet ( table 1 )  . 
studies that evaluated ngs in patients with sarcoma first author population boddu9 adult , sts and bone cote10 adult , sts and bone lucchesi8 adult , sts bone bone no . 
molecular approaches to detect the protein products of these fusion genes , such as uorescence in situ hybridization and reverse transcriptase polymerase chain reaction , can aid in the diagnosis of these tumors . 
the majority of clinical trials that have assessed chemotherapy for advanced stss have included heterogeneous populations , which complicates the assessment of clinical activity in specic subtypes . anthracyclines remain the most - used agents in the rst - line treatment of metastatic sts . 
 precision oncology in sarcomas alveolar rhabdomyosarcoma alveolar soft part sarcoma angiosarcoma chondroblastic osteosarcoma chondrosarcoma clear cell sarcoma dedifferentiated chondrosarcoma dedifferentiated liposarcoma dermatofibrosarcoma protuberans desmoid / aggressive fibromatosis desmoplastic small - round - cell tumor embryonal rhabdomyosarcoma endometrial stromal sarcoma epithelioid hemangioendothelioma epithelioid sarcoma ewing sarcoma extraskeletal myxoid chondrosarcoma fibrosarcoma follicular dendritic cell sarcoma hemangioma histiocytic dendritic cell sarcoma inflammatory myofibroblastic tumor intimal sarcoma leiomyosarcoma liposarcoma low - grade fibromyxoid sarcoma mesenchymal chondrosarcoma metaplastic carcinosarcoma myxofibrosarcoma myxoid chondrosarcoma myxoid / round - cell liposarcoma ossifying fibromyxoid tumor osteoblastic osteosarcoma osteosarcoma ovarian carcinosarcoma / malignant mixed mesodermal tumor perivascular epithelioid cell tumor pleomorphic liposarcoma pleomorphic rhabdomyosarcoma rhabdomyosarcoma round cell sarcoma , nos sarcoma , nos sarcomatoid renal cell carcinoma sclerosing epithelioid fibrosarcoma secondary osteosarcoma small cell osteosarcoma solitary fibrous tumor / hemangiopericytoma spindle cell rhabdomyosarcoma synovial sarcoma tenosynovial giant cell tumor diffuse type undifferentiated pleomorphic sarcoma / malignant fibrous histiocytoma / high - grade spindle cell sarcoma undifferentiated uterine sarcoma uterine adenosarcoma uterine carcinosarcoma / uterine malignant mixed mllerian tumor uterine leiomyosarcoma uterine perivascular epithelioid cell tumor uterine sarcoma , other well - differentiated liposarcoma fig 1 . 
adapted and updated from subbiah et al.122 abbreviations : c , clinical evidence ; ctla - 4 , cytotoxic t - cell lymphocyte - 4 ; gist , gi stromal tumor ; her2 , human epidermal growth factor receptor 2 ; mpnst , malignant peripheral nerve sheath tumor ; p , preclinical evidence ; pd - 1 , programmed cell death 1 ; pd - li , programmed cell death ligand 1 ; pecoma , perivascular epithelioid cell tumor ; sts , soft tissue sarcoma . limited to patients with liposarcoma.128 trabectedin , a synthetic alkaloid derived from the caribbean tunicate ecteinascidia turbinata , was approved by the food and drug administration ( fda ) for patients with advanced liposarcoma and leiomyosarcoma who received prior anthracycline - based regimens on the basis of a phase ii clinical trial that demonstrated its superiority to dacarbazine.129 retrospective reports have shown particular benet of therapy with trabectedin for myxoid liposarcoma ( orr , 51% ; disease control rate [ dcr ] , 90% ) , which achieved an mpfs of 14 months in patients who received multiple lines treatment.130 pazopanib is a multitargeted , smallmolecule tyrosine kinase inhibitor ( tki )  . 
however , as has been recently demonstrated in other rare tumor types that have led to fda - approved therapies , it is possible to establish efcacy with low patient numbers . 
therefore , trial designs are innovative clinical required to determine clinical benet of new therapies in patients with rare sts subtypes . basket trials are an emerging model of trial design centered on the assumption that the existence of a specic molecular aberration or biomarker predicts the benet of targeted therapies , regardless of cancer tissue of origin.136 the success of basket trials predominantly depends on the strength of the evidence that demonstrates tumor dependence on the targeted pathways and on reliable inhibition of the target by the drug.136 one example is the basket trial of vemurafenib for tumors that harbor a brafv600 mutation.71 vemurafenib is an orally available tki of braf , with higher selectivity for the brafv600 mutant form , that had been approved previously for patients with brafv600e mutationpositive metastatic melanoma.137 in this trial with six prespecied cohorts , there was one anecdotal response in a patient with clearinstitute cell sarcoma . 
some investigators are moving beyond searching for driver mutations and instead asking whether ngs can predict response or resistance to therapy ; others are creating expression proles that go beyond individual genes . 
ngs has the potential to become , in the coming years , an established platform of choice for researchers who are studying sarcomas . to date , many investigators have attempted to identify recurrent aberrations using ngs . 
they may be responsible for accelerated growth in advanced disease but are unlikely to be the sole cause of the malignancy . identication of these mutations is important , and with so much diversity in involved pathways , an individualized approach is necessary for proper sarcoma treatment . fruit bowl hypothesis current paradigm future paradigm one treatment for sarcoma precision therapy on the basis of molecular subtype fig 2 . 
for patients with few treatment options , a rationally chosen clinical trial on the basis of ngs - derived data is the best chance for prolonged survival . to demonstrate the ability of ngs to detect gene fusions , qadir et al138 designed child - seq , a pilot platform that rapidly screens cancer tissue for particular gene fusions characteristic of specic sarcomas . 
results demonstrated that the technique could reliably identify gene fusions in their corresponding tumor type without false positives . although this platform was limited to four particular childhood sarcomas , it is legitimate to conceptualize a more robust tool that could identify dozens or even hundreds of fusions . 
in fact , currently there are commercially available tools for molecular tissue testing that include detection of fusions ; identication of pathognomonic genetic alterations could enable a clinical diagnosis that is based solely on sequencing data . 
shukla et al139 demonstrated the feasibility of detecting ewsr1 fusions in plasma derived cell - free dna from patients with ewing sarcoma and desmoplastic small round - cell tumor . in general , ngs has proven to be a highly reliable technology . 
however , sanger sequencing of the patients tumor as well as her fathers germline testing revealed that the mlh1 mutation was a variant of unknown signicance rather than a pathogenic mutation . 
although this is a single case report , it highlights that even very robust technologies are subject to error . ngs for prediction ngs has the potential to identify specic molecular subtypes with particular sensitivity or resistance to approved treatments . 
to date , however , there have been few examples of ngs being used as a predictive tool in sarcomas , and it important to recognize that the examples discussed herein are preliminary and should be interpreted with caution . 
undoubtedly , as more patients undergo sequencing as part of their clinical care , patterns of response to therapy will emerge . koehler et al141 retrospectively reviewed 19 patients treated with pazopanib who also received ngs of their tumors . 
the authors found that the mpfs was signicantly longer in patients with tp53 mutant advanced sts ( 208 days ) than in those with tp53 wild - type tumors ( 136 days )  . lim et al142 performed ngs - based comprehensive genomic proling on 39 paired samples from tumor and normal tissue from patients treated with everolimus . 
these hypothesis - generating data reinforce the possibility of using ngs as a predictive tool in response to therapy . designing clinical trials on the basis of ngs wang et al143 performed a retrospective study of 75 patients with sarcomas who were referred to the clinical center for targeted therapy at md anderson cancer center . 
the majority of these tumors were sarcomas . multiomics studies included whole - exome sequencing ; germline , whole - transcriptome sequencing ; and singlenucleotide polymorphism array analysis of the tumor . germline cancer - associated gene mutations were reported in seven patients . 
one patient had an epithelioid imt that was identied to contain an ranbp2 - anaplastic lymphoma kinase ( alk ) fusion ; he experienced a complete response to crizotinib for 8 months . harris et al13 applied the same approach as chang et al144 to 89 pediatric tumors . 
this lack of response may have been due to the lower - quality preclinical evidence on which two of the recommendations were based . worst et al145 conducted the rst true prospective ngsbased trial with therapeutic intent . 
in this pilot study , 57 patients were enrolled from 20 centers ; approximately one half had sarcomas . one half of the patients harbored a potentially druggable alteration , and 10 patients went on to receive targeted therapy . 
however , because this was a pilot study designed to assess feasibility , there was no follow - up of patients who were treated with personalized targeted therapy and outcomes were not reported . 
early results with the use of inhibitors , however , have not been encouraging across all subtypes . therefore , the development of immunotherapy for sarcomas also benets from a precision oncology approach both in identifying predictive biomarkers and in developing strategies targeted to specic antigens . in the phase ii sarc028 trial ( clinicaltrials.gov identier : nct02301039 ) of pembrolizumab , an orr of 18% was seen in stss , with a 12 - week pfs of 55%.92 , 147 of note , this trial enrolled 40 patients with sts , including four tumor types ; subgroup analysis of the results identied encouraging activity in ups and dedifferentiated liposarcoma but not in other cohorts . 
combination of nivolumab and ipilimumab has provided promising efcacy in certain sts subtypes , with orr and mpfs in the range of those produced by standard - of - care options ; responses were observed in patients with leiomyosarcoma , myxobrosarcoma , ups , and angiosarcoma.148 furthermore , activity in specic subtypes has been suggested by retrospective studies . 
in a case series , two patients with chordoma experienced responses to single - agent antiprogrammed cell death ligand 1 ( pd - l1 ) antibodies , 149 and a review of patients enrolled in early - phase trials demonstrated that alveolar soft - part sarcoma was the most responsive subgroup to checkpoint blockade.91 , 150 the heterogeneity in the benet of checkpoint inhibitors across sarcoma subtypes observed in these early - phase trials highlights the need for a precision approach to immunotherapy in these diverse tumors , and research to identify predictive biomarkers is warranted . one challenge is that at this time , the immune microenvironment of specic subtypes is not sufciently characthe immune terized , and detailed characterization of microenvironment in each subtype is a major task . examples of potential predictive biomarkers to allow for selection of sarcomas sensitive to immune checkpoint inhibition include microsatellite instability ( msi ) status and pd - l1 expression in the tumor and microenvironment . 
in addition , responses were long lasting , with 78% lasting for 6 months or more.151 a recently published pan - cancer analysis identied that 5.7% of 785 sts cases analyzed were msi high , which highlights the relevance of this indication for sts.152 with regard to pd - l1 status , a recent meta - analysis with data from 1 , 451 patients and 15 independent studies identied pd - l1 expression to be independently associated with poorer os and event - free survival in bone and stss.153 however , the predictive value of pd - l1 in selecting patients with sarcoma for immune checkpoint inhibition is still under evaluation , and clinical activity of checkpoint inhibitors in these trials were seen even in the absence of pd - l1 expression.92 furthermore , cancer / testis antigens have been explored as potential targets for immunotherapy in sts and provide the utmost example of precision immunotherapy by targeting specic antigens . 
patients with kit exon 11 mutations have been identied as sensitive to imatinib , whereas patients with a kit exon 9 mutation , identied in 10% to 20% , respond poorly to imatinib at standard doses.155 most patients , however , eventually will develop resistance to treatment . 
in spite of the exceptional advances with rstline imatinib , the results with targeted treatments for later lines of therapy have been disappointing , emphasizing the need for new therapeutic approaches . 
imatinib dose escalation is one option for patients who have experienced disease progression on imatinib , and approximately 20% remain progression free for 1 year at the higher dose , especially among those with exon 9 mutations.162 furthermore , additional tkis are under development to optimize the treatment of imatinib - resistant gist . 
in addition , regorafenib was recently approved by the fda as a third - line therapy and has shown promising activity in patients with exon 17 mutations , which confer resistance to imatinib and sunitinib . 
co - occurring alterations in kit - mutated gi stromal tumor in the association for cancer research project genomics evidence neoplasia information exchange database ( n = 31 )  . available evidence indicates that kit mutation is likely an early event in the development of gist as suggested by the presence of activating kit mutations in gastric precursor lesions . 
in a previous study , 74% of gists analyzed had at least one nondriver genetic abnormality.164 in that report , the most frequently mutated genes were tp53 , rb1 , setd2 , pten , max , pik3ca , and tsc1 , and the most prevalent copy number alteration in kit - mutated gist was cdkn2a deletion.164 in addition , activation of alternate receptor tyrosine kinases has been suggested as a mechanism of resistance to currently approved tkis . 
for illustration , previous studies have identied that mutations that involve the rb1 gene are associated with high - risk tumors and aggressive clinical behavior and that activating mutations in the ras and phosphatidylinositol 3 - kinase pathways contribute to tki resistance.166 , 167 figure 4 illustrates co - occurring genetic alterations in kit - mutated gist in the aacr project genie database . in conclusion , sarcomas are a rare group of mesenchymal tumors in which the integration of ngs for diagnosis and management has provided informative evidence for precision medicine . 
the challenge to evaluate these mutations across rare cancer subtypes requires the careful characterization of these genetic alterations to further dene compelling drivers with therapeutic implications as well as novel models of clinical trial design . 
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martin , md1 introduction we read with interest two recently published articles in jco precision oncology that provide valuable insight regarding stk11 , an emerging biomarker in nonsmall - cell lung cancer ( nsclc ) .1 , 2 initially , shen et al1 detailed their ndings with the statistical learning tool oncocast . 
they identied stk11 as one of several prognostic genes afliated with poor survival from 1 , 054 patients with advanced lung adenocarcinoma proled with msk - impact next - generation sequencing ( ngs )  . 
by dividing the cohort into genomic risk - stratication groups , the authors highlighted the complexity of stk11 co - mutation patterns with other high - risk genes , including keap1 , kras , tp53 , and smarca4 . 
in the article by bange et al , 2 the authors retrospectively demonstrated heterogeneity of outcomes among patients with stk11 - mutated , advanced nsclc on the basis of co - mutation status . they reported that kras co - mutated cases had worse progression - free and overall survival outcomes after rst - line chemotherapy compared with tp53 . taken together , these ndings and others3 - 5 indicate that further work is warranted to characterize stk11 as an nsclc biomarker and to identify unique therapeutic approaches for patients with high - risk stk11mutated nsclc . 
a lumpectomy was performed in april 2014 , and adjuvant treatment included 12 doses of weekly paclitaxel , 1 year of trastuzumab , a partial breast radiation , and continuation on letrozole . 
a biopsy showed lung adenocarcinoma , and positron emission tomography ( pet ) / ct showed no additional disease . she received a robotic lobectomy , and pathologic staging revealed iiia disease . 
postoperative pet / ct in august showed a mildly hypermetabolic 1 - cm focus in the right middle lobe of the lung without other disease ; magnetic resonance imaging of the brain was negative . after radiologic review , it was initially believed that this focus represented postsurgical hypermetabolism , and close follow - up was recommended . 
she received adjuvant cisplatin and pemetrexed on day 1 of 21 - day cycles ; ct scans in october , after two of four cycles , showed no new disease . 
pet / ct revealed hypermetabolic disease limited to the 4 - cm adrenal mass . the adrenal and right middle - lobe lung lesions were biopsied , and both conrmed lung adenocarcinoma . she was referred for surgical evaluation but was not a candidate . 
testing included immunohistochemistry ( ihc ) , tumor mutational burden ( tmb ) , and 592 - gene ngs including egfr , braf , met , and her2 , as well as the previously mentioned high - risk genes stk11 , keap1 , kras , and tp53 ( nextseq ; illumina [ san diego , ca ] ) .6 ros1 and alk fusions were detected using the archerdx fusion assay ( archer fusionplex solid tumor kit )  . 
proling showed no targetable mutations , programmed death - ligand 1 ( pd - l1 ) ihc expression 0% ( 22c3 ; dako [ santa clara , ca ] ) , and tmb 15 mutations / megabase . 
no keap1 or tp53 mutations were identied . intravenous nivolumab 3 mg every 2 weeks and 1 mg / kg ipilimumab every 6 weeks were initiated in june 2018 . both treatments were withheld in july when the patient developed symptomatic autoimmune hyperthyroidism that necessitated treatment with methimazole and atenolol . 
nivolumab was resumed in august with symptom resolution , when ct scans showed a small increase in size of her adrenal metastasis with reduction of the right middle - lobe lesion . 
 nivolumab / ipilimumab in stk11 - mutated nonsmall - cell lung cancer by bange et al.2 although characterized by caris life sciences as a pathogenic mutation , we recognize that explicit pathogenicity of r39fs cannot be conrmed by commercial ngs alone . 
however , it should be noted that several studies have shown that frameshift variants ( including those of exon 1 ) generally express little stk11 protein by ihc , which serves as a reliable marker for loss of stk11.15 , 16 we recognize the complexity of dening high - risk stk11 molecular subsets from commercial ngs . 
martin consulting or advisory role : seattle genetics no other potential conicts of interest were reported . references shen r , martin a , ni a , et al : harnessing clinical sequencing data for survival stratication of patients with metastatic lung adenocarcinomas . 
cancer discov 8 : 822 - 835 , 2018 arbour kc , jordan e , kim hr , et al : effects of co - occurring genomic alterations on outcomes in patients with kras - mutant non - small cell lung cancer . 
clin cancer res 24 : 334 - 340 , 2018 skoulidis f , arbour kc , hellmann md , et al : association of stk11 / lkb1 genomic alterations with lack of benet from the addition of pembrolizumab to platinum doublet chemotherapy in non - squamous non - small cell lung cancer . 
vanderwalde a , spetzler d , xiao n , et al : microsatellite instability status determined by next - generation sequencing and compared with pd - l1 and tumor mutational burden in 11 , 348 patients . 
cancer med 7 : 746 - 756 , 2018 rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
nat rev drug discov 18 : 197 - 218 , 2019 ready n , hellmann md , awad mm , et al : first - line nivolumab plus ipilimumab in advanced non - small - cell lung cancer ( checkmate 568 ) : outcomes by programmed death ligand 1 and tumor mutational burden as biomarkers . 
frank r , schefer m , merkelbach - bruse s , et al : clinical and pathological characteristics of keap1and nfe2l2 - mutated non - small cell lung carcinoma 13 . 
p ecuchet n , laurent - puig p , mansuet - lupo a , et al : different prognostic impact of stk11 mutations in non - squamous non - small - cell lung cancer . 
brody , phd3 ; lola rahib , phd4 ; emily lyons , ma4 ; patricia de arbeloa , md2 ; andrew hendifar , md , mph5 ; sameh mikhail , md6 ; vincent chung , md7 ; davendra p.s. 
matrisian , phd , mba4 ; and emanuel petricoin iii , phd2 , 9 purpose up to 25% of pancreatic adenocarcinomas ( pdacs ) harbor mutations in the homologous recombination dna damage response ( hr - ddr ) pathway . 
although known to affect responsiveness to dnadamaging chemotherapy , the prognostic relevance of these mutations is unclear and outcomes in patients with pdac who harbor hr - ddr mutations beyond brca1 / 2 remain unexplored . methods we evaluated 820 patients with pdac enrolled in the know your tumor program for whom we had collected comprehensive genomic testing results and longitudinal clinical outcomes . 
mos in patients with mutations in all three hr - ddrmut groups was greater than that for phr - ddr patients , but this difference was lost in platinum - nave patients . conclusion patients with advanced hr - ddrmut have improved mos when treated with platinum - based therapy compared with phr - ddr patients . 
with a 5 - year median overall survival ( mos ) of only 9% , pdac is poised to become the second leading cause of cancer - related death in the united states.1 treatment of metastatic pdac has improved with the use of uorouracil , oxaliplatin , and irinotecan ( folfirinox ) , and gemcitabine plus nab - paclitaxel , but mos remains less than 1 year.2 , 3 however , there is a substantial group of outlier patients whose survival exceeds the median of less than 1 year . 
 pishvaian et al context key objective up to 25% of pancreatic adenocarcinomas ( pdacs ) harbor mutations in the homologous recombination dna damage response ( hr - ddr ) pathway . 
we evaluated 820 patients with pdac who were enrolled in the know your tumor program for whom we had collected comprehensive genomic proling data and longitudinal clinical outcomes to assess the prognostic and predictive value of hr - ddr mutations . knowledge generated patients with advanced pdac and the presence of a somatic or germline hr - ddr mutation have an improved median overall survival ( mos ) when treated with platinum - based therapy compared with patients with no hr - ddr mutation . 
in platinumnave patients , there is no mos difference , which suggests that hr - ddr status has no pure prognostic value . relevance these ndings support the need to test all patients with advanced pdac to ensure that patients whose tumors harbor hr - ddr mutations receive the benet of treatment with platinum - based therapy . prolonged stable disease of 15 patients with pdac who were treated with parpi - based therapy , whereas kaufman et al21 reported one complete response and four partial responses of 23 brca - mutated patients with pdac who were treated with olaparib . 
combinations with chemotherapy may be even more promising , as oreilly et al17 reported a 78% response to the combination of gemcitabine , cisplatin , and veliparib in patients with brcaor palb2mutated pdacs . the treatments received , or we evaluated whether patients with hr - ddrmutated tumors have a biologically better prognosis , irrespective if patients with hrddrmutated tumors have longer than average survival strictly because the underlying mutation predicts for a high degree of responsiveness to platinum - based therapies ( part of the standard of care )  . methods patient recruitment into the know your tumor registry as reported , 4 patients with pdac were identied through the pancreatic cancer action network patient central call center , referred to perthera , and enrolled via an institutional review boardapproved registry protocol . 
study protocol , amendments , and informed consent forms were approved by the new england institutional review board . vestigators obtained informed consent from each participant or participants guardian before enrollment . 
the research was conducted in accordance with recognized ethical guidelines , including the declaration of helsinki , for international organizations of medical scicouncil ences , belmont report , and us common rule , as described during training in good clinical practice guidelines ( collaborative institutional training initiative training )  . patients with biopsy - conrmed pdac were included in the analysis cohort . 
patients with pancreatic adenosquamous carcinoma or other histologic subtypes were excluded . next - generation dna sequencing and identication of hr - ddr status formalin - xed , parafn - embedded blocks and / or slides were collected by surgical resection ( eg , whipple procedure or distal pancreatectomy ) , core - needle biopsy , or ne - needle aspiration . 
coverage of hr - ddr genes tested was relatively uniform with 97% of genomic testing completed by foundation medicine ( cambridge , ma ) , 1% by caris life sciences ( irving , tx ) , and the remaining by including in - house pathology deother partments . 
genomic alterations reported by the testing laboratory included both somatic and germline mutations ; however , it is important to note that the germline versus somatic status of each mutation could not be determined on the basis of tumor proling without parallel genetic sequencing of matched normal blood or tissue . patient tumor genomic proles were reviewed and pathogenic mutations were conrmed by pertheras molecular tumor board participants on a case - by - case basis . 
tumors that harbored no hr - ddr mutations were labeled ddr procient ( phr - ddr )  . results patient history and outcomes enrolled patients signed a health insurance portability and accountability act waiver , and for patient history and longitudinal outcomes assessment , patient coordinators the patients requested updated medical records until death . 
to reduce variability as a result of the timing of enrollment and to establish a denitive starting point for the determination of mos , survival was calculated from the initial date of diagnosis of pdac until death . 
patients were categorized herein as those who underwent a resection of the primary tumor at any point during their treatment history ( resected ) or and as those who had advanced disease at presentation , including locally advanced , never resected patients , and patients with metastatic disease at presentation . 
furthermore , patients were designated as platinum exposed if they received any platinum - containing therapy at any point during the course of their pancreatic cancer survival . statistical analysis all statistical analyses were performed in an r / bioconductor programming environment.22 mos was measured from the date of initial diagnosis until the date of death or the last date the patient was known to be alive . median progression - free survival ( mpfs ) was measured from the start date to the last date the patient was known to be on treatment without progression of disease . 
differences between groups were evaluated for statistical signicance using cox proportional hazards regression models ( the coxph function in the r survival package )  . computed values reported include mpfs , mos , p values , hazard ratios , and 95% cis for hazard ratios . a multivariable approach was implemented to delineate prognostic versus predictive effects of hr - ddr status using the entire analysis cohort . 
given the limitations of interpreting several pairwise comparisons across small groups of patients , we accounted for three binary independent factors : platinum exposure , hr - drr status , and resectability . 
multivariable cox proportional hazards regression was performed on os analysis data by factoring in platinum exposure as one variable , the presence of an hr - ddr alteration as a second variable , interaction between the rst and second variable , and a third variable to account for the patients resection status , which is known to have a highly signicant prognostic impact on os . of 1 , 140 patients with pdac who were enrolled in the know your tumor program between january 2013 and the end of december 2018 , 820 patients with molecular testing results , collection of longitudinal outcomes , and adequate treatment history were included in the analysis cohort . median age at diagnosis was 62 years ( range , 28 to 90 years ) , 52% of patients were male , and 81% of patients were white ( table 1 )  . 
prevalence of somatic or germline hr - ddr mutations ( 16.5% ) and other baseline characteristics was not signicantly different within the resectable and advanced cohorts ( table 1 )  . 
at a median follow - up of 637 days and 386 days for the resected and advanced cohorts , respectively , 47.6% of patients were last known to be alive and 29.2% of patients had not received platinum - based therapy . 
twentyve percent of deceased patients never received any platinum - based therapy . assessing the prognostic value of hr - ddr mutations in platinum - nave patients to assess the prognostic value of the presence of an hrddr mutation , in the absence of the confounding variable of the known predictive value of response to platinum - based therapy , we chose to assess outcomes in patients who never received platinum - based therapy at any time during their pancreatic cancer survival . 
these patients were labeled platinum nave and included 108 resected and 133 advanced patients for analysis ( table 1 and figs 1a and 1b )  . differences in mos were not statistically signicant when comparing hr - ddrmut with phr - ddr patients whose disease was platinum nave in both the resected and advanced subgroups . 
thus , there was no apparent positive prognostic value associated with the presence of an hrddr mutation in platinum - nave patients with pdac . conrming the predictive value for platinum - based therapy of an hr - ddr mutation we also assessed the predictive value for platinum - based therapy of an hr - ddr mutation ( figs 1c and 1d and table 2 )  . 
percentages of patients on the basis of ethnicity / race were only calculated for those for whom ethnicity / abbreviations : hr - ddrmut , homologous recombination dna damage response mutated ; n / a , not applicable ( demographic percentages were calculated for patients for whom the ethnicity / race were known ) ; pdac , pancreatic adenocarcinoma ; phr - ddr , homologous recombination dna damage response procient . after the diagnosis of pdac was established , then the patient was considered platinum treated . 
platinum - based regimens typically included folfirinox ( 85% in rst line and 39% in second line ) ; infusional uorouracil , leucovorin , and oxaliplatin ( 10% in rst line and 52% in second line ) ; or cisplatin with or without gemcitabine ( 3% in rst line and 7% in second line )  . 
variables in the analysis included the main effect of hr - ddr mutations ( prognostic term ) , the main effect of platinum exposure ( treatment term ) , an interaction between these two variables ( predictive term ) , and surgical status ( resectability term )  . 
genomic mutations in homologous recombination dna damage response ( hr - ddr ) genes are not prognostically favorable in patients with pancreatic adenocarcinoma who did not receive platinum - based chemotherapy . 
median overall survival ( mos ) differences on the basis of hr - ddr status were not signicant in platinum - nave patients diagnosed with either ( a ) resectable or ( b ) advanced disease . 
for patients with advanced disease who received platinum - based therapy , there was also an increased progression - free survival for hr - ddrmutated ( hr - ddrmut ) versus hr - ddrprocient ( phr - ddr ) patients in both the ( e ) rst line and ( f ) second line and later setting . 
instead , this trend ( not signicant ) suggested a potentially unfavorable prognostic effect for patients with mutations in the hr - ddr pathway , as shown in figures 1a and 1b . 
when factoring these four variables into our analysis , this model captures the value of hr - ddr mutations as a predictive class of biomarkers for increased responsiveness to platinum agents ( table 3 ) and indicates that this benet is not likely associated with an independent prognostic effect of hr - ddr mutations . assessing which ddr mutation confers the most predictive value the ddr pathway encompasses a functionally diverse network of interacting components spanning more than 50 enzymes ( fig 2 ) , many of which are critical for different aspects of the ddr process across a wide range of biologic contexts . 
atm and atr are critical for sensing double - stranded dna breaks and initiating a series of processes that allow a cell to recognize dna damage and halt the cell cycle until the damage is repaired . 
finally , mrn complex proteins and fanconi anemia core proteins play secondary , yet critical roles in the hr - ddr process . to assess which hr - ddr mutation ( s ) conferred the strongest predictive value to platinum - based therapy , we grouped the hr - ddr mutations into three groups ( fig 2 )  . 
hr - ddr subclassications ( group 1 , group 2 , and group 3 ) are based on the strength of evidence supporting each genes association with increased responsiveness to poly ( adp - ribose ) polymerase inhibitors and / or platinum agents . outcomes for each of the three groups were compared with phr - ddr patient outcomes . 
the number of patients in each group was small , but analysis that was focused on advanced patients conrmed that presence of an hr - ddr mutation is not prognostic , but is predictive of response to platinum - based that therapy . 
advanced pancreatic adenocarcinoma tumors with genomic mutations in hr - ddr genes were compared with the hr - ddrprocient ( phr - ddr ) cohort separately for groups 1 , 2 , and 3 , dened as follows : group 1 ( those with known clinical evidence of predictive value ) ; group 2 ( other genes with strong preclinical evidence of a suspected predictive value ) ; and group 3 ( other genes with preclinical evidence of a role in hr - ddr )  . 
in fact , there may be a trend toward worse outcomes in platinum - nave hr - ddrmut patients compared with platinum - nave phr - ddr patients , although not statistically signicant . in contrast , patients with advanced pdac with hr - ddrmut tumors who received at least one platinum - based regimen had a signicantly longer mos ( by nearly a full year ) compared with platinum - treated patients with phr - ddr tumors . 
this trend was also observed in resected patients who received any platinum - based therapy with an mos difference of nearly 1.5 years that we anticipate will become signicant as this cohort grows and data mature . 
moreover , for hr - ddrmut patients , mos was three times greater in the platinum - exposed versus platinum - nave patients . these results suggest that optimal therapy for hr - ddrmut patients includes a platinum - containing regimen . 
it is currently estimated that 17% to 25% of pdacs harbor somatic or germline hr - ddr mutations , 5 - 7 , 9 - 13 but only 50% of advanced patients are treated with platinum - based therapy in the rstline setting , and less than 50% of patients treated in the rstline go on to receive second - line therapy at all.2 this suggests that up to 25% of patientsnumerically up to 1 , 500 patients with pdac annuallywith hr - ddr mutated tumors are not being optimally treated with platinum - based therapy during the course of their pancreatic cancer survival . 
in addition , it is possible that patients with hr - ddrmutated pdacs who have undergone resection would have a greater chance for cure with an adjuvant platinum - based regimen , such as folfirinox , 23 instead of a nonplatinum - based regimen , such as gemcitabine plus capecitabine.24 there are limitations to this registry study . 
although testing results and treatment considerations were provided to the treating oncologist in real time , there was no prospective intervention to ensure that patients were treated according to the molecular test results . 
thus , this was a retrospective analysis of patients prospectively captured into the registry . longitudinal outcomes data were not yet furthermore , mature or not available for approximately 28% ( 320 of 1 , 140 ) of patients enrolled . 
second , although parallel genetic sequencing results of normal tissue or blood samples were not available to assess the germline status of the hrddr mutations identied in this study , approximately 54% of alterations in this pathway are estimated to be of germline origin on the basis of next - generation sequencing of pdac tumors.25 the relative impact of somatic versus germline hr - ddr mutations on responsiveness to platinums or parpi remains an important question to be answered , and one recent study in pdac demonstrated that patients with conrmed somatic - only brca2 mutations did still respond to the parpi rucaparib.19 additional studies are warranted to investigate the scope of hr - ddr pathway genes / variants and the types of molecular alterations ( eg , germline mutations with or without loss of heterozygosity in the tumor ) that are of clinical relevance . nevertheless , universal adoption of molecular proling of patients with pdac is growing , despite being a controversial issue . 
in april 2019 , the national comprehensive cancer network ( nccn ) modied their language for germline testing for patients with pdac.26 recognizing that up to 40% of patients with germline hr - ddrmutated pdac do not have any signicant family history to suggest a predisposing syndrome , such as a breast / ovarian cancer syndrome , 27 the new nccn guidelines state that germline testing is recommended for all patients with pancreatic cancer . 
recognizing that even somatic hr - ddr mutations may be therapeutically relevant and that germline testing alone may miss patients who could potentially benet from platinum - based therapy , the nccn went on to state that tumor / somatic testing is also recommended for patients with advanced pdac to identify uncommon but actionable mutations . 
matrisian , emmanuel petricoin iii administrative support : kimberly mason provision of study materials or patients : patricia de arbeloa , andrew hendifar , kimberly mason collection and assembly of data : michael j . 
pishvaian stock and other ownership interests : perthera honoraria : caris life sciences , celgene , sirtex medical , merrimack pharmaceuticals consulting or advisory role : caris life sciences , perthera , celgene , sirtex medical , astrazeneca , medimmune , renovorx , armo biosciences , rafael pharmaceuticals , ignyta , merck research funding : genentech ( inst ) , celldex ( inst ) , merck ( inst ) , glaxosmithkline ( inst ) , medimmune ( inst ) , pzer ( inst ) , gilead sciences ( inst ) , regeneron ( inst ) , novartis ( inst ) , karyopharm therapeutics ( inst ) , pharmacyclics ( inst ) , bristol - myers squibb ( inst ) , bayer ( inst ) , curegenix ( inst ) , calithera biosciences ( inst ) , tesaro ( inst ) , bavarian nordic ( inst ) , halozyme ( inst ) , armo biosciences ( inst ) , fibrogen ( inst ) , celgene ( inst ) patents , royalties , other intellectual property : perthera patient matching algorithm travel , accommodations , expenses : caris life sciences , sirtex medical , perthera , astrazeneca , medimmune edik m . 
blais employment : astrazeneca ( i ) , perthera stock and other ownership interests : perthera patents , royalties , other intellectual property : inventor on patents led by perthera ( as an employee ) jonathan r . 
brody stock and other ownership interests : perthera consulting or advisory role : perthera travel , accommodations , expenses : perthera patricia de arbeloa employment : perthera andrew hendifar consulting or advisory role : novartis , ipsen , perthera , celgene , abbvie research funding : ipsen travel , accommodations , expenses : halozyme sameh mikhail consulting or advisory role : ipsen , perthera vincent chung consulting or advisory role : celgene , perthera , ipsen , five prime therapeutics speakers bureau : celgene , ipsen , astrazeneca davendra p.s. 
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n engl j med 364 : 1817 - 1825 , 2011 von hoff dd , ervin t , arena fp , et al : increased survival in pancreatic cancer with nab - paclitaxel plus gemcitabine . 
n engl j med 369 : 1691 - 1703 , 2013 pishvaian mj , bender rj , halverson d , et al : molecular proling of patients with pancreatic cancer : initial results from the know your tumor initiative . 
clin cancer res 24 : 5018 - 5027 , 2018 aguirre aj , nowak ja , camarda nd , et al : real - time genomic characterization of advanced pancreatic cancer to enable precision medicine . 
cancer discov 8 : 1096 - 1111 , 2018 lowery ma , jordan ej , basturk o , et al : real - time genomic proling of pancreatic ductal adenocarcinoma : potential actionability and correlation with clinical phenotype . 
clin cancer res 23 : 6094 - 6100 , 2017 bailey p , chang dk , nones k , et al : genomic analyses identify molecular subtypes of pancreatic cancer . 
domchek sm , aghajanian c , shapira - frommer r , et al : efcacy and safety of olaparib monotherapy in germline brca1 / 2 mutation carriers with advanced ovarian cancer and three or more lines of prior therapy . 
lowery ma , kelsen dp , stadler zk , et al : an emerging entity : pancreatic adenocarcinoma associated with a known brca mutationclinical descriptors , treatment implications , and future directions . 
oreilly em , lee jw , lowery ma , et al : phase 1 trial evaluating cisplatin , gemcitabine , and veliparib in 2 patient cohorts : germline brca mutation carriers and wild - type brca pancreatic ductal adenocarcinoma . 
oreilly em , lowery ma , segal mf , et al : phase ib trial of cisplatin ( c ) , gemcitabine ( g ) , and veliparib ( v ) in patients with known or potential brca or palb2mutated pancreas adenocarcinoma ( pc )  . 
neoptolemos jp , palmer dh , ghaneh p , et al : comparison of adjuvant gemcitabine and capecitabine with gemcitabine monotherapy in patients with resected pancreatic cancer ( espac - 4 ) : a multicentre , open - label , randomised , phase 3 trial . 
singhi ad , george b , greenbowe jr , et al : real - time targeted genome prole analysis of pancreatic ductal adenocarcinomas identies genetic alterations that might be targeted with existing drugs or used as biomarkers . 
 biomarkers intratumoral transcriptome heterogeneity is associated with patient prognosis and sidedness in patients with colorectal cancer treated with anti - egfr therapy from the co.20 trial elisa fontana , md , phd1 , 2 ; gift nyamundanda , phd1 , 2 ; david cunningham , md3 ; dongsheng tu , phd4 ; maggie c.u. 
siu , md8 ; francesco sclafani , md3 , 9 ; katherine eason , phd1 ; chanthirika ragulan , msc1 , 2 ; maria antonietta bali , md , phd10 , 11 ; sanna hulkki - wilson , bsc1 ; jonathan m . 
waring , mbbs , phd13 ; mirella giordano , phd14 ; patrick lawrence , ms1 , 2 ; daniel nava rodrigues , md3 ; ruwaida begum , bsc3 ; jeremy d . 
price , md16 ; chiara cremolini , md17 , 18 ; naureen starling , mbbs , mrcp , md ( res ) 3 ; filippo pietrantonio , md19 , 20 ; livio trusolino , md , phd21 , 22 ; christopher j . 
ocallaghan , dvm , msc , phd4 ; and anguraj sadanandam , phd1 , 2 purpose metastatic colorectal cancers ( mcrcs ) assigned to the transit - amplifying ( ta ) crcassigner subtype are more sensitive to antiepidermal growth factor receptor ( egfr ) therapy . 
progression - free survival ( pfs ) , overall survival ( os ) , and disease control rate ( dcr ) according to ta - ness classication were assessed by univariate and multivariate analyses . results the ta - ness was measured in 772 samples from 712 patients . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction epidermal growth factor receptor ( egfr ) - targeting antibodies cetuximab and panitumumab are available treatment options for approximately 40% of patients with metastatic colorectal cancer ( mcrc ) .1 patient selection based on ras and braf wild - type status and sidedness has improved overall response rates and survival outcomes . 
nevertheless , 30% - 60% of eligible patients do not benet from these expensive drugs.2 - 4 as a shift from the traditional paradigm of negative molecular selection , we previously demonstrated that the transit - amplifying ( ta ) crcassigner ( crca ) subtype was enriched for cetuximab - responsive tumors , 5 a nding independently validated in a clinical study , 6 in a panel of crc xenografts5 and cell lines.5 , 7 however , responses were also seen in other groups , such as the poorly differentiated stem - like subtype , 5 , 7 albeit at a lower frequency . 
 intratumoral transcriptome heterogeneity and anti - egfr therapy context key objective to evaluate whether the presence of the transit - amplifying ( ta ) subtype gene signature ( dubbed as ta - ness classication ) representing the intratumoral transcriptome heterogeneity is associated with antiepidermal growth factor receptor ( egfr ) therapy outcomes . knowledge generated the ta - ness classication is an easily detectable biomarker of intratumoral transcriptome heterogeneity , which was retrospectively evaluated in 712 patient samples , including those from a clinical ( co.20 ) trial , which showed prognostic signicance in patients treated with anti - egfr therapy . 
this biomarker provides additional biologic insights for the association between ras / braf wild - type left - sided tumors ( enriched for ta - high ) and anti - egfr therapy benet . relevance with further validation , ta - ness may represent a positive selection biomarker for patients with ras / braf wild - type left - sided metastatic colorectal cancer who are most likely to benet from anti - egfr therapy . ta subtype tumors are characterized by gene signatures similar to normal ta cells of the colonic crypt , that is , those in transit between stem cells in the crypt base and differentiated cells at the top of the crypt.5 after asymmetric division , stem cells generate rapidly proliferating ta cells characterized by increased egfr expression that eventually differentiate into goblet cells and enterocytes.8 , 9 we evaluated a hypothesis that tumors with increased ta gene signature expression ( irrespective of ta or other subtypes ) may be associated with anti - egfr therapy outcomes . 
the discovery cohort included chemorefractory patients ( n = 84 ) who had received anti - egfr therapy as a single agent or in combination with chemotherapy after progression while receiving irinotecan ( during or within 3 months from the end of treatment ) as part of standard treatment at the royal marsden hospital ( rmh ; n = 59 ; united kingdom , ethics committee : 10 / h0308 / 28 ; and clinicaltrials.gov identier : nct02112357 ) or within the context of a case - control study in italian institutions ( pressing , n = 25 ; ethics committee area vasta nord ovest number 1333 / 173 )  . 
nineteen and 12 patients from the rmh cohort were treated before the implementation of kras testing ( august 2009 ) and extended ras testing ( december 2011 ) , respectively.11 , 12 all patient samples from the pressing study had extended ras / braf wildtype tumors . one of the clinical validation cohorts included 121 patients with kras exon 2 wild - type tumors who had received single - agent cetuximab within the control arm of the co.20 phase iii randomized clinical trial ( clinicaltrials.gov identier : nct00640471 ) .13 this correlative analysis was approved by the joint canadian cancer trial group and australasian gastrointestinal trial group ( cctg / agitg ) correlative sciences and tumor biology committee . two additional public gene expression datasets ( n = 397 ; not treated with anti - egfr therapy ) of primary crc samples ( gse39582 ; n = 328 ) and liver mcrc lesions ( gse73255 ; n = 69 ) were evaluated.14 , 15 only samples with known kras wild - type status were selected . nucleic acids extraction formalin - xed parafn - embedded ( ffpe ) tissues were least evaluated by a trained pathologist ; areas with at 30% of tumor content were marked on hematoxylin and eosin slides and macrodissected in unstained slides ( 7to 10 - m thickness )  . 
after deparafnization , total rna and dna were simultaneously isolated using the ambion recoverall kit ( discovery ) or qiaamp nucleic acid ffpe tissue kit ( validation ) and quantied with nanodrop 2000 spectrophotometer ( thermo fisher , waltham , ma ) according to the manufacturers instructions . 
 a fontana et al discovery cohort retrospective tissue collections validation cohort 1 prospectively enrolled in the co.20 study outcome cohort ta - ness no . median pfs ( months ) univariate analysis hazard ratio ( 95% ci ) log - rank multivariate analysis hazard ratio ( 95% ci ) cox regression rmh cohort ( n = 90 ) italian cohort ( n = 42 ) patients ( out of 374 in cetuximab arm ) ( n = 163 ) patients with quality rna ( n = 65 ) patients with quality rna ( n = 25 ) patients with quality rna ( n = 146 ) excluded because of low tumor content in the block or low rna conc . 
 after extraction ( n = 25 ) patients excluded because of qc flag after ncounter analysis ( n = 6 ) patients excluded for anti - egfr in refractory setting as re - challenge ( n = 17 ) patients excluded because of qc flag after ncounter analysis ( n = 0 ) patients for final analysis ( n = 59 ) patients for final analysis ( n = 25 ) patients for final analysis ( n = 121 ) patients excluded because of low tumor content in the block or low rna conc . 
covariates included in the validation cohort : eastern cooperative oncology group performance status , sex , age , baseline lactate dehydrogenase level , baseline alkaline phosphatase , baseline hemoglobin , number of disease sites , number of previous chemotherapy drug classes , prior vegfr target therapy , and presence of liver metastases . 
conc. , concentration ; egfr , epidermal growth factor receptor ; pdx , patient - derived xenograft ; qc , quality control ; rmh , royal marsden hospital . ve published crca - 38 centroids ( expression summary of each gene in each subtype ) 16 and gene expression , each sample was assigned either to ta - high ( increased expression of ta signature genes ) or ta - low ( reduced expression ) ta - ness classes . 
when gene expression proles were compared with the ve crca - 38 centroids , ve correlation coefcients ( one for each subtype - centroid ) were calculated for each sample . 
the coefcients were then ranked from highest to lowest ; ta - high samples were those with a correlation coefcient value for the ta centroid ranking within the rst three highest values ; ta - low samples were those with a correlation coefcient for the ta centroid , which is second to last or the lowest . 
therefore , the ta - ness classication represents a measure of transcriptome - based intratumoral heterogeneity in mcrc , based on the idea that each sample can contain more than one subtype . 
this best cut - off for ta - ness classication was established based on the highest accuracy in dening disease control , measured as area under the curve ( auc ) of a receiver operating characteristic ( roc ) curve ( appendix fig a1 )  . statistical analysis progression - free survival ( pfs ) was the primary endpoint . overall survival ( os ) , disease control rate ( dcr ) , and response rate were secondary endpoints . 
fishers exact test was used to compare categorical variables , and wilcoxon signed rank test with p , .05 was used to assess the association between ta - ness classes and percentage of tumor shrinkage ( using recist ) criteria in a subgroup of the discovery cohort . 
although the statistical analysis of discovery cohort was performed by the institute of cancer research statistician , the validation cohort was independently analyzed by cctg / agitg investigators blinded to the biomarker cut - off analysis . 
additional methods are available in the data supplement . results retrospective antiegfr - treated tumor samples from 205 patients were identied from the discovery and validation ( co.20 ) cohorts after clinical review and quality control of the tumor blocks and tumor - derived rna ( fig 1a )  . 
 intratumoral transcriptome heterogeneity and anti - egfr therapy cohort from 30 patients along with 30 patient - derived xenografts ( pdxs ; derived from the patient tumors ) that were treated with anti - egfr therapy or vehicle ( control ) were subjected to the same crca gene expression assay . 
in addition , publicly available gene expression microarray data for 80 patients with mcrc ( treated with anti - egfr therapy ) was included as an additional clinical validation cohort.17 this publicly available cohort also served to validate ta - ness classication using a different platform ( microarrays ; fig 1a )  . patient characteristics for discovery and validation co.20 cohorts are shown in the data supplement . 
with the exception of sex , there were no signicant differences in patients characteristics between the co.20 subgroup included in this analysis and the overall co.20 clinical trial cohort ( data supplement )  . using conventional subtyping , 15 of 84 samples belonged to the ta subtype in the discovery cohort . 
the association of ta - ness classication with both pfs and dcr remained signicant after adjusting for multiple variables in both the discovery and validation cohorts ( fig 1b )  . 
conversely , after adjusting for multiple variables , signicant association of ta - ness with os was only borderline ( or not signicant with p = .1 in the discovery cohort and p = .06 in the validation cohort ; data supplement ) ; postprogression treatment information was not available . in the discovery cohort , ta - high tumors ( 62% ; n = 52 ) were predominantly ras / braf wild - type ( 69% ; n = 36 ) and were found in the left side of the colon ( 79% ; n = 41 )  . 
this result was mirrored in the experimental cohort , 18 , 19 in which 30 ras / braf wild - type liver metastases were classied into ta - high ( n = 16 ) and ta - low ( n = 14 ) classes . 
the percentage of cetuximab - induced tumor volume change in the pdx - based mouse - propagated patient metastatic tumors was signicantly associated ( p , .042 ) with the ta - ness signature ( fig 3b )  . in the discovery cohort , the ta - ness classication was assessed using samples from primary tumors in 76% of patients and samples from metastatic sites in 24% of patients . 
to further conrm that the association was independent of the diagnostic sample of origin and to further validate the results , we examined the khambata - ford publicly available ( microarray ) dataset17 of mcrc samples from patients treated with cetuximab . 
to further conrm that the ta - ness can be assessed in both primary tumors and metastatic lesions , kras wild - type samples from two publicly available datasets14 , 15 were selected ; 328 primary tumors and 69 liver metastases were classied into ta - high and ta - low . 
similar distribution of the two classes was demonstrated ( fig 3c )  . beyond ras / braf mutational status , sidedness is a recognized selection factor for anti - egfr therapy benet : patients with left - sided tumors benet more than patients with right - sided tumors.4 however , the biology behind this association remains unclear . 
first , we further conrmed signicant association ( p , .001 ) between ta - ness classication and sidedness in kras wild - type primary tumors ( gse39582 ; fig 3d )  . 
then , we sought to discover whether the ta - ness classication could further rene the selection of patients in addition to ras / braf status and sidedness . within discovery and validation cohorts ( n = 205 ) , highsensitivity next - generation sequencing ras / braf mutational analysis was available for 118 patients : 71 were classied as ras / braf wild - type , of which 53 were assigned to ta - high ( 75% ) class . 
 ( a ) a waterfall plot showing a subgroup of patients within the discovery cohort ( n = 35 ) showing disease response ( treated with anti epidermal growth factor receptor [ egfr ] drug ) according to recist criteria and ta - ness classication . 
 ( b ) a waterfall plot showing change in tumor ( percent ) volume in anti - egfrtreated mouse - propagated patient tumor samples ( n = 30 ) compared with matched control treated ( baseline ; n = 30 ) mouse - propagated patient tumors . 
the bars in the graph show ta - ness classication for the matched patient metastatic liver samples ( n = 30 ) , and the bars below the graph show the same classication for matched mousepropagated patient tumors ( treated v control )  . 
this classication has the advantage of providing a qualitative assessment in all the samples , including the non - ta subtypes , overcoming the limitations posed by intratumoral heterogeneity when using the conventional molecular subtyping classication as a potential tool to assess benet from anti - egfr therapy . 
kaplan - meier survival curves of patients with transit - amplifying ( ta ) - high versus ta - low tumors treated with antiepidermal growth factor receptor ( egfr ) therapy . 
 fontana et al ( and potentially clinical benet ) in patients treated with anti - egfrbased therapy in our discovery cohort ; this was validated in a kras exon 2 wild - type trial cohort of cetuximab - onlytreated patients , 13 which has the advantage of properly assessing prognostic value in a homogeneously treated population and in the absence of confounding effect of chemotherapy . 
moreover , ta - low assignment was enriched for ras / braf - mutant tumors , providing a potential alternative method to estimate prognosis and may be a treatment benet from anti - egfr therapy when the mutational status is missing . 
this signature and its association with anti - egfr treatment outcomes were also conrmed in the publicly available samples from patients with mcrc17 and the preclinical pdx models treated with cetuximab.18 , 19 finally , the taness classication retained prognostic signicance when assessed in either archival primary tumors or metastatic samples in multiple cohorts . 
this is highly clinically relethe classication can be vant , because it means that assessed in metastatic lesions when the primary tumor sample is not available or of poor quality ; however , intrapatient concordance was not assessed ; therefore , additional validation is required . several studies have now evaluated the association between single genes or micrornas ( ereg / areg , her2 , her3 , epha2 , or mir - 31 - 3p ) and responses to anti - egfr therapy.20 in contrast , we evaluated a rened form of our previously published gene expression signature ( with multiple genes ) to identify biologically different crc subtypes with distinct cellular phenotypes.5 , 16 the subtypes summarize a complex network of pathways potentially associated with therapeutic responses , simplifying multiple levels of information derived from heterogeneous samples . hence , the deployment of subtypes and their signatures , instead of single genes , has the advantage of reducing the dimension of complexity without losing biologic information . 
although the crca and consensus molecular subtype ( cms ) classications are highly concordant , 16 , 21 cms classication was not assessed here because it is technically challenging to dichotomize samples into two groups based on the current cms classier ( with multiple centroids )  . this study has some limitations . 
the identication of such patients in the context of clinical trials is challenging ; in fact , the negative predictive value of ras / braf mutations was retrospectively demonstrated in multiple clinical trials , and to our knowledge , none of them was designed with an up - front prospective inclusion of extended ras / braf wild - type tumors . 
last , this was a proof - of - concept study and was retrospectively designed on preexisting tissue collections in the absence of a control group , limiting the assessment of a ta - ness biomarker as prognostic rather than predictive . 
shapiro , chiara cremolini , filippo pietrantonio , livio trusolino , anguraj sadanandam data analysis and interpretation : elisa fontana , gift nyamundanda , david cunningham , dongsheng tu , maggie c . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . elisa fontana consulting or advisory role : astellas pharma ( i ) , celgene ( i ) , servier ( i ) , bristol myers squibb ( i ) patents , royalties , other intellectual property : patent no : 1716712.3 pending ( i ) travel , accommodations , expenses : bristol myers squibb ( i ) , servier ( i ) gift nyamundanda patents , royalties , other intellectual property : prognostic and treatment response prediction in gastric cancer priority patent csc / bp7295892 , patient classication and prognostic method patent application number pct / ep2019 / 053845 , patent application number 2011213.2 david cunningham stock and other ownership interests : ovibio consulting or advisory role : ovibio research funding : astrazeneca ( inst ) , amgen ( inst ) , sano ( inst ) , merrimack ( inst ) , celgene ( inst ) , medimmune ( inst ) , bayer ( inst ) , 4sc ( inst ) , clovis oncology ( inst ) , eli lilly ( inst ) , janssen ( inst ) , merck ( inst ) maggie c . 
siu leadership : treadwell therapeutics ( i ) stock and other ownership interests : agios ( i ) consulting or advisory role : merck , astrazeneca / medimmune , morphosys , roche , loxo , voronoi , oncorus , symphogen , mirati therapeutics , gsk , seattle genetics , treadwell therapeutics , arvinas , navire research funding : bristol myers squibb ( inst ) , genentech ( inst ) , glaxosmithkline ( inst ) , merck ( inst ) , novartis ( inst ) , pzer ( inst ) , medimmune ( inst ) , astrazeneca ( inst ) , boehringer ingelheim ( inst ) , bayer ( inst ) , amgen ( inst ) , astellas pharma ( inst ) , shattuck labs ( inst ) , symphogen ( inst ) , avid ( inst ) , mirati therapeutics ( inst ) , intensity therapeutics ( inst ) , karyopharm therapeutics ( inst ) francesco sclafani consulting or advisory role : bayer research funding : bayer ( inst ) , astrazeneca ( inst ) , roche ( inst ) , bristol myers squibb ( inst ) travel , accommodations , expenses : bayer , eli lilly jonathan m . 
waring employment : astrazeneca leadership : pillar biosciences , xing technologies , ori healthcare stock and other ownership interests : genentech , roche ( i ) , pillar biosciences , xing technologies consulting or advisory role : pillar biosciences , xing technologies , ori healthcare travel , accommodations , expenses : pillar biosciences , xing technologies timothy j . 
 fontana et al travel , accommodations , expenses : roche , servier naureen starling honoraria : eli lilly , msd oncology , merck serono , pierre fabre , servier consulting or advisory role : servier , astra zeneca , pzer research funding : astra zeneca ( inst ) , pzer / emd serono ( inst ) , bms ( inst ) travel , accommodations , expenses : msd oncology filippo pietrantonio consulting or advisory role : amgen , merck serono , bayer , eli lilly , sano , roche , servier research funding : bristol myers squibb livio trusolino honoraria : eli lilly , astrazeneca , merck research funding : symphogen ( inst ) , merus ( inst ) , pzer ( inst ) , servier ( inst ) , menarini ( inst ) anguraj sadanandam consulting or advisory role : ploughshare innovations research funding : merck , pierre fabre , bristol myers squibb patents , royalties , other intellectual property : patent colorectal cancer classication with differential prognosis and personalized therapeutic responses ( patent number pct / ib2013 / 060416 ) , prognostic and treatment response prediction in gastric cancer priority patent csc / bp7295892 , patent patient classication and prognostic method ( gep - net ) priority patent ep18425009.0 , patent molecular predictors of therapeutic response to specic anti - cancer agents ( patent number us9506926b2 ) no other potential conicts of interest were reported . acknowledgment we thank all patients and families participating in the studies included in this article . 
tebbutt , hagen kennecke , gabriella fontanini , eugenia zanella , and andrea bertotti for their contributions in the studies included in this article . references van cutsem e , cervantes a , adam r , et al : esmo consensus guidelines for the management of patients with metastatic colorectal cancer . 
ann oncol 27 : 1386 - 1422 , 2016 de roock w , claes b , bernasconi d , et al : effects of kras , braf , nras , and pik3ca mutations on the efcacy of cetuximab plus chemotherapy in chemotherapy - refractory metastatic colorectal cancer : a retrospective consortium analysis . 
lancet oncol 11 : 753 - 762 , 2010 cremolini c , morano f , moretto r , et al : negative hyper - selection of metastatic colorectal cancer patients for anti - egfr monoclonal antibodies : the pressing case - control study . 
ann oncol 28 : 3009 - 3014 , 2017 tejpar s , stintzing s , ciardiello f , et al : prognostic and predictive relevance of primary tumor location in patients with ras wild - type metastatic colorectal cancer : retrospective analyses of the crystal and fire - 3 trials . 
jama oncol 3 : 194 - 201 , 2017 [ erratum : jama oncol 3 : 1742 , 2017 ] sadanandam a , lyssiotis ca , homicsko k , et al : a colorectal cancer classication system that associates cellular phenotype and responses to therapy . 
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stem cells int 2017 : 7602951 , 2017 yang yp , ma h , starchenko a , et al : a chimeric egfr protein reporter mouse reveals egfr localization and trafcking in vivo . 
national institute for health and care excellence : cetuximab for the rst - line treatment of metastatic colorectal cancer : technical appraisal guidance [ ta176 ]  . 30 : 520 - 527 , 2019 12 . 
national institute for health and care excellence : panitumumab in combination with chemotherapy for the treatment of metastatic colorectal cancer ( terminated appraisal ) : technical appraisal guidance [ ta240 ]  . 
marisa l , de reyni `es a , duval a , et al : gene expression classication of colon cancer into molecular subtypes : characterization , validation , and prognostic value . 
plos med 10 : e1001453 , 2013 isella c , brundu f , bellomo se , et al : selective analysis of cancer - cell intrinsic transcriptional traits denes novel clinically relevant subtypes of colorectal cancer . 
khambata - ford s , garrett cr , meropol nj , et al : expression of epiregulin and amphiregulin and k - ras mutation status predict disease control in metastatic colorectal cancer patients treated with cetuximab . 
bertotti a , migliardi g , galimi f , et al : a molecularly annotated platform of patient - derived xenografts ( xenopatients ) identies her2 as an effective therapeutic target in cetuximab - resistant colorectal cancer . 
zanella er , galimi f , sassi f , et al : igf2 is an actionable target that identies a distinct subpopulation of colorectal cancer patients with marginal response to 20 . 
receiver operating characteristic ( roc ) curve to determine the best cut - off to dene disease control rate in the discovery cohort . 1 represents samples classied into transit - amplifying ( ta ) tumor with highest ( rank ) correlation with crcassigner ( crca ) - 38 centroids . 
 ( a ) kaplan - meier survival curve of patients with transit - amplifying ( ta ) tumor versus non - ta tumor in the discovery cohort subtyped using conventional subtyping approach . 
 decision - making preferences about secondary germline findings that arise from tumor genomic profiling among patients with advanced cancers purpose in patients with advanced cancers , tumor genomic profiling ( tgp ) can reveal secondary germline findings ( sgfs ) with regard to inherited disease risks . 
this study examined the process by which patients with advanced cancers would decide about whether to learn these sgfs and their preferences about specific challenging decision scenarios , including whether patients should be required to receive sgfs and whether sgfs should be returned to the family after a patients death . patients and methods we conducted qualitative semistructured interviews with 40 patients with advanced breast , bladder , colorectal , or lung cancer who had undergone tgp . 
data were collected on participants perspectives about the hypothetical decision to learn their sgfs , including their anticipated approach to the decision - making process , and their preferences about challenging decision scenarios . 
data were evaluated by thematic content analysis . results we identified themes with regard to participants preferred degree of decisional autonomy , perceived vital role of doctors , information needs , and anticipated process of deliberation . 
most participants stated that patients should be able to make a choice about receiving actionable sgfs , and a majority stated that sgfs should be available to family after a patients death . conclusion these results provide insight into sgf decision - making processes of patients with advanced cancers , which can allow clinicians to provide patients with optimal decision support in this context . 
these germline variants are considered secondary findings when actively sought by researchers or clinicians ( or incidental findings when not ) because they arise outside the original purpose of tgp.1 , 2 secondary germline findings ( sgfs ) that indicate risks for various health conditions are likely to be detected in a sizable minority of patients who receive tgp ; for example , presumed pathogenic germline variants have been observed jada g . 
this decision is likely to be challenging , particularly for patients with advanced cancers who are currently the primary users of tgp ( because of its utility for identifying eligibility for clinical trials of novel therapeutics5 , 6 )  . 
these individuals must choose whether to learn information about their future disease risks and potential shared familial risks while facing a poor prognosis and the psychosocial challenges of a terminal diagnosis.7 although patients with varying stages of cancer have reported interest in receiving such information from tgp in real8 and hypothetical9 - 11 settings , how patients decide whether to learn sgfs is unclear . 
understanding the decision - making processes of patients with advanced cancers would allow clinicians to anticipate patient informational and decision support needs in this context . the current study describes processes by which patients with advanced cancers decide whether to learn sgfs that arise from tgp . 
we analyzed qualitative data collected through an investigation of attitudes about sgfs among patients who received tgp at our institution.12 these patients were informed about the possible incidental discovery of germline variants during tgp consent conducted by their primary medical oncologists ; however , because our institution did not routinely conduct secondary analyses at the time of this study , none of the patients had made a definitive decision about learning their sgfs . 
 we also assessed preferences with regard to specific challenging decision scenarios , including whether patients should be required to receive sgfs and whether sgfs should be returned to the family after a patients death . study methods are described in detail elsewhere.12 in brief , we recruited 40 adults with advanced breast , bladder , colorectal , or lung cancer who had undergone tgp with an institutional somatic sequencing panel ( msk - impact [ memorial sloan kettering - integrated mutation profiling of actionable targets ] 13 , 14 )  . 
 the memorial sloan kettering cancer center institutional review board approved this study . individual semistructured interviews15 - 18 were conducted with participants in person or by telephone on the basis of participant preference . 
we categorized participant responses into four key themes and relevant subthemes ( indicated by italicized text ) ; illustrative quotes appear in table 2 . theme 1 : degree of decisional autonomy as participants considered how they would decide whether to learn sgfs , a spectrum emerged with regard to participants preferred degree of decisional control and autonomy from close others . 
influential factors for this perspective included a view that the decision was my choice because it involved highly personal information fundamentally related to my body and a desire to avoid burdening others , particularly family , with potentially distressing information . a second group of participants preferred that close others play a consultative role in the decision making process . 
these participants anticipated communicating with close others about the option to learn sgfs and would consider their advice and opinions but would ultimately make the final decision on their own . 
some in this group noted that their familys views were highly valued but would not be determinants in their decision making . finally , a smaller group preferred that close others serve as active partners in decision making . 
others explained that their family members should be actively involved in this decision because sgfs may have direct health - related implications for them . participants who anticipated the involvement of others in their decision making also described their process of selecting close others for communication about the option of learning sgfs . 
decision - making process and preferences regarding secondary germline findings and illustrative participant quotes participant quote theme theme 1 : degree of decisional autonomy patient as an autonomous decision maker well , i think that would be up to me to decide , so i wouldnt be asking my family what they think about doing that . 
 ( f / cc ) close others play a well , id like their input , but ultimately , i make the decisions for what...kind of consultative role in the decision - making process treatment....i would make the final decision . 
 ( f / brc ) close others serve as active partners in decision making process of selecting close others for communication i would expect my wife to be involved....i trust her knowledge and judgment in these matters . 
i dont think my husband could deal with it , so i dont want him burdened with it , and i dont think my step - kids have enough...skin in the game , so to speak , that they should actually be involved in making the decision and i guess i feel similarly about sisters and brother that thats too distant . 
 ( f / cc ) theme 2 : vital role of doctors nature and quality of the doctor - patient relationship primary source of relevant and valuable information theme 3 : information needs clinical benefit meaning tainty testing procedure believe me , its been a rough road , and so like i said , my oncologist and i , we have a good understanding . 
he was the one that put me in the tumor profiling and also on this new research , and anything he decides with me , im okay with it because we have that doctor - patient trust . 
i mean , you know , if they tell me to go get this test , i go get that test....i do it because i think its in the interest of my health.you know , you would have to make a strong argument for that case , but if he was insistent , i would do it . 
 ( m / blc ) i think from a personal standpoint i would ask...how realistic do you think , or how probable do you think , something that came up as high risk is likely to happen , or is there anything i can do to prevent it ? i mean , its more so in the latter that i would care about more if theres anything i can do to prevent it , to minimize the risk . 
is it certain mutations , is it only certain diseases that were talking about , or...is it kind of open ended ? ...i guess i would want to learn more and hear more about the science of what the mutations might mean . 
 ( m / cc ) degree of scientific uncerwhat im trying to have connection with is that if this testing were predictive of something , they would be more interested than if [ with ] this testing , nobody understood or knew how to interpret the results . 
so i guess it would be depending [ on ] how far along the continuum we are in being able to use this information [ that ] would make a difference . 
 ( m / lc ) yes , and if its nothing invasive and they wont...poke me anymore and they wont do anything to me , its fine with me....i would like to know . 
decision - making process and preferences regarding secondary germline findings and illustrative participant quotes ( continued ) theme participant quote who will have access who would have that information , would health care providers...have to have access to that or insurance providers have to have access to that information ? ( f / brc ) yes , what are the possible ramifications , like everything ? like the question that i have now , like what havent i thought of that could be a possible ramification of knowing ? yeah . 
 ( f / brc ) negative implications or harms theme 4 : process of deliberation ing process deliberative decision - makthe only potential benefit i see is if it discovers something that could be dealt with and prevent serious illness or genetic problems in the future . 
 ( m / cc ) take time to decide i think i would want to think about it and talk about it a little more before i made that quick decision , yeah . 
but i dont think its something that we would shy away fro ( m / lc ) well , i think i would research mutations first and find out a little about it before i answered him , but my nature is to go ahead and find out as much information as i can . 
 ( f / blc ) no need to engage in i would say , great , where do i sign ? when i first got diagnosed , i offered to extensive deliberation have my dna sequenced , and the doctor said , why would you bother ? theres only 30 markers , and weve already looked at theso yeah , to me , it was like a no - brainer and required no thought . 
so for me , its really once i understand what exactly ill be getting out of the study or what benefit it can provide , thats enough of what i need to make a decision on . 
i wouldnt want to procrastinate...it would be my decision....id discuss with family members...my husband and my sister , but...it would be my decision ultimately , and id really want to make it quickly . 
the interviewer described secondary germline findings as follows : i mentioned that with tumor genomic profiling , sometimes the lab will also look for mutations in the genes in your normal cells . 
 abbreviations : blc , bladder cancer ; brc , breast cancer ; cc , colorectal cancer ; f , female ; lc , lung cancer ; m , male . theme 2 : vital role of doctors participants perceived their doctors ( ie , oncologists ) as a vital influence on their decision making . 
for example , several participants reported great trust in their doctors on the basis of a foundation of past experiences and certainty that their doctors will act in their best interests . 
several participants anticipated that their doctors would possess expertise with regard to a range of issues relevant to sgfs and thus could help them to acquire all essential information . theme 3 : information needs participants described a typology of information that they would require to make an educated decision about learning sgfs , including an explanation of whether sgfs would provide a clinical benefit to the patient , his or her family , or other cancer patients and whether these benefits would outweigh possible harms ; assistance in interpreting the meaning of sgfs , such as the degree of certainty of the results and meaning of specific mutations ; degree of scientific uncertainty of sgfs and confidence in their applicability to health decisions ; description of the testing procedure in terms of the invasiveness of sample acquisition ; information about who will have access to the findings ( eg , insurers , health care providers ) ; and negative implications or harms of learning sgfs for the patient and family , including unanticipated consequences . 
many participants stated that they would ask questions about these issues to feel adequately informed , yet a minority doubted that they would have any specific questions if presented with this decision primarily because of placing a high innate value on sgfs . theme 4 : process of deliberation two preferences emerged among participants with regard to the necessity to engage in an extensive decision - making process . 
 ( a detailed description of these perceived benefits and harms is provided elsewhere.12 ) participants described procedural aspects of their deliberation and expressed a preference to take time to decide , during which they would consider the option on their own and seek out information about the value of sgfs . 
furthermore , a few participants expressed a preference to conduct independent research to learn more about receiving sgfs and the meaning of potential mutations . a minority of the sample articulated no need to engage in an extensive deliberation to determine their interest in sgfs . 
 finally , some described a sense of urgency about learning sgfs and stated the necessity to gain and act upon this information quickly to benefit their current health directly . preferences with regard to decision scenarios during the interview , participants were presented with challenging scenarios and asked to describe their preferences for how clinicians should handle these situations . 
first , in response to the debate about the disclosure of sgfs , 26 - 29 we asked participants whether findings about diseases that have effective medical interventions or medication adverse effects ( ie , actionable sgfs ) should always be returned to patients . 
most participants ( 28 [ 70% ] of 40 ) stated that patients should be able to choose whether to receive this information , whereas a minority ( 12 [ 30% ] of 40 ) stated that such information should always be disclosed to patients . participants also were asked to decide whether they believed that if actionable sgfs were detected after a patients death , then these findings should be made available to a patients family or significant other . 
a subset of participants ( 16 [ 69.5% ] of 23 ) also expressed a belief that patients should be required to provide consent for this disclosure before their death , such as at the time of agreeing to tgp , whereas fewer ( seven [ 30.5% ] of 23 ) deemed patient consent unnecessary . 
preferences with regard to specific decision scenarios that involve secondary germline findings and illustrative participant quotes participant quote question should actionable secondary germline findings * always be returned to patients ? yes ( 30% ) yes , i agree with that because they may not want to know , but theyre still going to be affected by it . 
because at least theyd have the opportunity to know...whats going on with thethey may not want to know , and it may be painful , but i think that they should be told . 
i think of a very close friend that was diagnosed with cancer , and he was in his 20s , and he survived , but when i learned that i had cancer , i reached out to him , and he said that at his lowest point he begged , i dont want to know any more information . 
and that was part of the healing for him , so i always think about that because that was a poignant point that he made , and i think its so personal . 
 ( f / brc ) should actionable secondary germline findings be made available to a patients family or significant other if a patient has died ? yes ( 90% ) unsure ( 5% ) no ( 5% ) should nonactionable secondary germline findings be made available to a patients family or significant other if a patient has died ? yes . 
well , if it in any way could...impact the timing of treatment or care for someone else in the family , they should....i would want them to know about it....i guess at the end of the day that you should get consent from the patient...as to what youre going to do with anything...you take from the ( m / lc ) you got a coin ; you wanna flip a coin ? because the problem that comes to me is that my family is very tight , and it wouldnt be a problem with my family , but you always have a family that [ is ] ...on the outs , so to speak , and if you tell one , you got to tell all . 
 ( m / lc ) thats a good question because im thinking that if the spouse , for example , were told after the person passed away that we had discovered this , i guess the first reaction would be , how come we didnt discover it earlier while the person was still alive and there may have been time for some kind of treatment ? so it might cause some kind of anger . 
preferences with regard to specific decision scenarios that involve secondary germline findings and illustrative participant quotes ( continued ) question unsure ( 2.5% ) no ( 15% ) participant quote i can project how i might think in the future , but its hard for me to say at this time in a practical way how i would feel about , you know , releasing . 
if they want the information they should go and get it...and i think that if they get it just because it was available for me , like as part of my estate , heres her genetic testing , and again , ill use my brother because he has the kids . 
if...he sees in black and white that theres an indicator that we have a genei have a gene so that becomes a family gene - - so hes now gotten a worry he didnt ask for in his life . 
 abbreviations : blc , bladder cancer ; brc , breast cancer ; cc , colorectal cancer ; f , female ; lc , lung cancer ; m , male . * in the interview , actionable secondary germline findings were described as follows : there are different ways to think about the many kinds of mutations or disease risks that you could theoretically learn about . 
when doctors know that someone has one of these mutations , they can recommend ways to help prevent a disease from developing or help find it earlier when it is more likely to be treatable . 
the doctors may also change the kinds of medications that they prescribe . in the interview , nonactionable secondary germline findings were described as follows : it is also possible that the lab will find mutations for conditions that do not have recommended or effective medical interventions . 
 but when two carriers of the same recessive mutation have a child , then the child could have the disease . unsure about whether actionable sgfs should be available to a patients family after death ( two [ 5% ] of 40 ) or stated that such information should not be made available ( two [ 5% ] of 40 )  . 
 preferences against disclosure were due to concerns about negative emotional implications of such information for families . participants were similarly asked to decide whether they believed that sgfs about diseases without effective medical interventions or that indicate one is a healthy carrier for recessive diseases ( ie , nonactionable sgfs ) should be made available to a patients family after a patients death . 
most participants who provided an opinion regarding consent reported that patients should be required to consent to the disclosure of this information to their families ( 11 [ 92% ] of 12 )  . 
fewer ( six [ 15% ] of 40 ) stated that nonactionable sgfs should not be made available to family after a patients death because of concerns about negative emotional reactions and the limited ability to intervene with such diseases . 
 finally , when comparing the preferences of participants with regard to the return of actionable versus nonactionable sgfs to family after a patients death , 22.5% ( nine of 40 ) were discordant in their preferences across these scenarios . discussion this study clarifies the decision - making processes of patients with advanced cancer with regard to sgfs from tgp . 
however , consistent with other medical decision contexts , 30 - 34 variability existed in participants preferences for involving others , including spouses / partners , children , and siblings , in their decision making . 
consequently , when presenting the option of learning sgfs , clinicians must allow patients to solicit input from close others and help to navigate challenges inherent in decision making with multiple individuals.35 additional research should investigate how such interpersonal influences shape , hinder , or support patients sgfs decision making . participants anticipated that their doctors ( ie , oncologists ) would be the primary source of guidance for this decision . 
participants also anticipated that they would have extensive questions about the benefits , harms , interpretation , and process of obtaining sgfs and would expect their oncologists to provide answers . 
however , research has demonstrated that this may not be feasible because many oncologists have limited experience with germline testing and express concerns about their ability to address challenges presented by sgfs.8 several approaches may help to bridge this gap between patient expectations and oncologist preparedness , including oncologist - targeted communication training , novel patient education materials , and referral to genetic counselors to address patient questions . 
future research should evaluate which of these approaches are most effective at achieving the delicate balance between meeting patients information needs and practical challenges of cancer care delivery ( eg , time demands , workforce limitations )  . 
research should also examine how various models of patient education ( eg , oncologist led , genetics professional led ) influence patient sgfs decisions and how patients weigh the opinions of various care providers in this context . many participants anticipated a preference to undergo a thoughtful deliberation about the prospect of learning sgfs . 
research suggests that the adoption of a more intuitive decision - making approach can yield similar outcomes to deliberative decision making , 36 although both approaches have benefits and drawbacks.37 of note , some participants preferences for a quick decision were motivated by beliefs that sgfs would provide clinical utility or necessitate urgent action for them to reap health benefits . 
accordingly , clinicians must ensure that all patients , including those immediately enthusiastic or accepting of sgfs , accurately understand the limitations of this risk information . these results also provide insight into preferences of patients with advanced cancers with regard to challenging scenarios that involve the return of sgfs . 
consistent with american college of medical genetics and genomics recommendations4 and expert opinion , 38 most participants stated that patients should choose whether they want to receive actionable sgfs from tgp . 
participants generally were more supportive of the return of actionable sgfs to family after a patients death than nonactionable sgfs ; although , in both instances , a majority supported the sharing of this information with family largely because of perceived family health benefits . 
the qualitative design enabled an in - depth analysis of the decision - making preferences of a sample of patients with advanced cancers diverse in diagnosis , sex , and health status . 
however , the majority was well - educated ( 85% reporting at least some college ) ; decision - making preferences and processes of these individuals may differ from those with less formal education . 
additional limitations are that this sample was racially and ethnically homogenous , recruited from one institution , and assessed at a time when the decision about learning sgfs was hypothetical in nature ; thus , the findings may not be generalizable to the broader population of patients with advanced cancers treated in other care settings who are navigating this decision in real time . 
recommendations for developing precision oncology programs with regard to how to manage and support patient decision making about secondary germline findings from tumor genomic profiling develop educational materials about tumor genomic profiling ( tgp ) and secondary germline findings ( sgfs ) that can be easily disseminated to and understood by close others ( eg , siblings , children , spouses / partners ) who may play a role in a patients decision making . ensure that individuals who lead education and consent discussions about the return of sgfs are prepared to help patients with varying preferences for decisional autonomy from their close others . patients attribute high trust and expertise to their oncologists ; therefore , prepare oncologists to serve as a primary resource who can provide balanced advice to patients about sgf decisions . create patient educational materials that provide clear information about the potential benefits and harms of sgfs . 
 distinguish between potential outcomes of sgfs for patients ( with a consideration of their cancer stage and prognosis ) and their families . ensure that patients understand that the decision to undergo tgp is separate from the decision about return of sgfs and that varying potential benefits and harms of each choice exist . structure education and consent discussions about tgp and the return of sgfs to be temporally flexible and , therefore , capable of accommodating patients preferences to take time to deliberate , seek additional input from close others , and conduct independent research . give patients a choice about the return of actionable sgfs . 
either opt - in or opt - out models of germline variant management could allow such patient choice , but each has unique implications for resources to support informed patient decision making and subsequent uptake of sgfs . require patients to make decisions about the management of actionable and nonactionable sgfs in the event of their death at the time of consenting to tgp and the return of sgfs . in conclusion , this study provides important insight into how patients with advanced cancers approach the decision to learn sgfs and informs how developing precision oncology programs can manage the reporting of germline variants from tgp ( table 4 )  . 
patient preferences for involvement in this decision can be accommodated in both opt - in and opt - out models , although these models likely will differ in the resources necessary to support patient deliberation and in the number of patients who select to receive sgfs.42 , 43 although most patients likely will want to retain decisional control in this context , some will desire time and space to include family and other influential figures in their decision making . 
whereas the tgp decision may be time sensitive because of treatment implications , patients may benefit from efforts to ensure that the decision to receive sgfs can be pursued on a different temporal schedule that aligns with their preferences for information seeking and deliberation . 
thus , educational and communication interventions targeted to patients , their families , and oncologists are needed to provide clear information that contextualizes the meaning of sgfs in the advanced cancer setting , assist the weighing of benefits and harms , and allow patients to explore and express their preferences about specific categories of sgfs and management of this information in the event of their death . 
presidential commission for the study of bioethical issues : anticipate and communicate : ethical management of incidental and secondary findings in the clinical , research , and direct - to consumer contexts ( december 2013 report of the presidential commission for the study of bioethical issues )  . 
tripathy d , harnden k , blackwell k , et al : next generation sequencing and tumor mutation profiling : are we ready for routine use in the oncology clinic ? bmc med 12 : 140 , 2014 6 . 
parsons dw , roy a , plon se , et al : clinical tumor sequencing : an incidental casualty of the american college of medical genetics and genomics recommendations for reporting of incidental findings . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental findings : results from the canseq study . 
hamilton jg , shuk e , genoff mc , et al : interest and attitudes of patients with advanced cancer with regard to secondary germline findings from tumor genomic profiling . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
burke w , antommaria ah , bennett r , et al : recommendations for returning genomic incidental findings ? we need to talk ! genet med 15 : 854 - 859 , 2013 27 . 
stiggelbout am , jansen sj , otten w , et al : how important is the opinion of significant others to cancer patients adjuvant chemotherapy decision - making ? support care cancer 15 : 319 - 325 , 2007 35 . 
laidsaar - powell rc , butow pn , bu s , et al : physician - patient - companion communication and decision - making : a systematic review of triadic medical consultations . 
scheuner mt , peredo j , benkendorf j , et al : reporting genomic secondary findings : acmg members weigh genet med 17 : 27 - 35 , 2015 39 . 
kaphingst ka , ivanovich j , biesecker bb , et al : preferences for return of incidental findings from genome sequencing among women diagnosed with breast cancer at a young age . 
 megakaryocyte potentiating factor as a predictive biomarker for therapies against malignant mesothelioma purpose effective biomarkers for malignant mesothelioma ( mm ) are needed for clinical management and the development of mesothelin - targeted therapies . 
we evaluated serum megakaryocyte potentiating factor ( mpf ) as a biomarker predictive of treatment outcome in patients with mm and for developing mesothelin - targeted therapies . materials and methods serial serum samples from patients with mm in two clinical trials of an antimesothelin immunotoxin were tested with our clinically validated mpf assay . 
mpf was further evaluated for an association with response to an antimesothelin therapy and for disease monitoring . results there was a significant reduction of serum mpf in patients with elevated baseline and radiologic response , with an average change from 52% to 78% after one to six cycles . 
 potentiating factor ( mpf ) and membrane - bound mesothelin.15 , 16 previous studies showed correlations between the computed tomography ( ct ) response and arbitrarily chosen 10% to 25% reduced serum mesothelin after chemotherapy.17 - 21 such low cutoff values are incompatible with a 30% reduction in tumor determined with ct , would contribute to high degrees of false signals , and would make it more difficult to correlate with clinical outcomes . the currently available mesomark test ( fujirebio , malvern , pa ) detects serum mesothelin , which is subject to the interference by mesothelin - targeted antibody - based agents . 
we developed and validated an assay for mpf and further showed that elevated mpf is a worse prognostic biomarker in patients with mm.22 its effectiveness for monitoring therapies is not known . 
the first trial was a phase i study with a standard dose of pemetrexed and cisplatin , and the antimesothelin immunotoxin ss1p ( nct01445392 ) in chemotherapy - nave patients with pleural mesothelioma.19 twenty patients were evaluable , 12 with partial response ( pr ) , three with stable disease ( sd ) , and five with progressive disease ( pd )  . 
the patients had received one to six ( and an average of three ) previous therapies.8 all patients were evaluated for responses : three with pr , three with sd , and four with pd . 
tumor responses were determined on the basis of ct and calculated in accordance to modified response evaluation criteria in solid tumors ( mrecist ) criteria for mesothelioma . statistical analyses prism , version 7.0 ( graphpad , la jolla , ca ) was used for statistical analysis . 
 kaplan - meier survival analyses were performed to determine log - rank hazard ratio ( hr ) and p value of mpf response or ct response patients on pfs or os . 
on the basis of the linear regression analysis of corresponding changes in ct and mpf in these 20 patients with mm , a 30% change in ct was interpolated to a 47% change in mpf level ( fig 1b )  . 
thus , a rounded 50% change in serum mpf was selected as the cutoff for mpf response , which corresponded to approximately 30% change in ct using mrecist . the serum mpf test enables continuous and multiple measurements during treatment . 
among pr patients with an elevated mpf using the upper limit of normal at 1.2 ng / ml , 22 there was an average of 52% change in mpf after one cycle ( p < .001 ; n = 12 ; fig 1c )  . 
in contrast , for the patients who did not have a ct response , there was no significant reduction of mpf ( n = 14 ; fig 1d )  . 
thus , the treatment induced reduction of serum mpf may be an informative biomarker of objective response in patients with mm with elevated baseline mpf . kaplan - meier analyses were performed to compare pfs and os of both trials . 
thus , the data suggest that a 50% change in mpf after systemic therapies is strongly associated with improved pfs . reduction of mpf after systemic treatment as a potential biomarker for better os the mpf response was further correlated with os . 
landmark analysis of os for mpf and ct response was performed , with a landmark date at 91 days , at which time all patients had experienced a response but one . 
 ( a ) analysis of the changes in serum mpf in patients with partial response ( pr ) , stable disease ( sd ) , and progressive disease ( pd )  . 
all data are shown as mean standard deviation . depletion regimen of pentostatin and cyclophosphamide , major cancer regressions were observed and were attributed primarily to the activities of ss1p.8 the nonparametric mann - whitney test showed that the patients with pr ( by ct ) had elevated baseline serum mpf levels , which were higher than those in the nonresponse group ( p = .033 ; fig 3a )  . 
thus , data suggest that elevated baseline serum mpf may be associated with the response to an effective antimesothelin therapy in patients with refractory mm , whereas the mpf response is associated with improved survival in these patients ( p = .012 ; appendix fig a4 )  . 
 20 pfs since in - study date ( months ) os since in - study date ( months ) mpf response mpf nonresponse log - rank p < .001 hazard ratio = 0.279 ct response ct nonresponse log - rank p = .022 hazard ratio = 0.457 mpf response mpf nonresponse log - rank p = .004 hazard ratio = 0.361 ct response ct nonresponse log - rank p = .035 hazard ratio = 0.476 pfs since in - study date ( months ) os since in - study date ( months ) fig 2 . 
 ( a ) progression - free survival ( pfs ) and ( b ) overall survival ( os ) using mpf response at a threshold of 50% or more after therapies . 
 ( c ) progression - free survival and ( d ) os for patients with malignant mesothelioma using computed tomography ( ct ) response on the basis of modified response evaluation criteria in solid tumors . 
102 was a 50 - year - old man with extensive peritoneal involvement and received two cycles of ss1p because of ss1p antibody development.8 he had a delayed response with substantial tumor shrinkage at 7 months . 
103 , a 56 - year - old woman with pleural mesothelioma , had rapid disease progression before treatment and was the only patient who completed all six cycles of therapy . 
105 , pr response progression cutoff response progress response time since in - study date ( months ) time since in - study date ( months ) cutoff cutoff fig 3 . 
elevated baseline megakaryocyte potentiating factor ( mpf ) associated with response and long - term follow - up of individual patients with major tumor regression after antimesothelin and immune suppression . 
there was evidence of increased serum mpf at the time of disease progression for all . discussion our study indicates that the serum mpf test is effective in monitoring systemic therapies for patients with mm , because the patients with mpf responses have much better pfs and os than those without , regardless of baseline levels . 
in mm , recist needs to be modified because one - dimensional measurement of the nonspherical growth pattern was difficult.24 the mrecist requires repeated total tumor measurements on two occasions 4 weeks apart for pr determination.25 the quantitative changes of serum mpf may provide an alternative , lowcost , and nonradiative assessment of therapy response in patients with mm with elevated mpf . 
 we used a more stringent cutoff value of a 50% change in mpf to define the biomarker response compared with the previous reports17 - 21 ; this cutoff was supported by our correlative analysis of ct and mpf responses in patients with mm . 
such a stringent cutoff correlates with the mrecist criterion of a 30% reduction in the sum for all target lesions and thus leads to a significant reduction of false - positive reports during monitoring . 
thus , in addition to confirming the association between changes in mpf and patients response to systemic therapy , 18 our results further showed that an mpf biomarker response is associated with improved pfs and os . as the cleavage product during mesothelin maturation with a short half - life in blood , 22 , 26 serum mpf levels reflect the expression of target antigen mesothelin on tumor cells , without being bound by the therapeutic agents . 
in fact , in untreated mesothelioma patients , there is a strong correlation between mpf and soluble mesothelin.22 , 27 the mpf test could be valuable for the clinical development of mesothelin targeted therapies and for monitoring targeted therapies against mm . 
therefore , serum mpf could facilitate long - term disease monitoring and provide a noninvasive assessment of the drug - target mesothelin expression in mm at the time of disease progression , which can be critical for evaluating alternative therapies . one of the most important issues in the development of targeted therapies is the stratification of the intended patient population . 
mesothelin is ubiquitously detected in epithelioid mm by immunohistochemistry ( table 1 ) ; therefore , mesothelin immunohistochemistry is not predictive of response to mesothelin - targeted therapies in mm , and a different biomarker test is required . 
 there are many challenges for a serum - based test for patient selection , including the expression of the tumor antigen by nontumor cells and the variations in shedding of it by tumor cells . 
 in addition , it is possible that serum mpf may be influenced by renal dysfunction in patients receiving nephrotoxic chemotherapies because prior reports showed elevated serum mpf in patients with renal disease.28 , 29 however , the patients described in our study had normal renal functions at the time of enrollment . 
although our previous data suggested that patients with mm with elevated mpf have a worse prognosis , 22 the results here suggest that the reduction of serum mpf in patients with refractory mm is associated with improved clinical outcome . 
vogelzang nj , rusthoven jj , symanowski j , et al : phase iii study of pemetrexed in combination with cisplatin versus cisplatin alone in patients with malignant pleural mesothelioma . 
hassan r , cohen sj , phillips m , et al : phase i clinical trial of the chimeric anti - mesothelin monoclonal antibody morab - 009 in patients with mesothelin - expressing cancers . 
golfier s , kopitz c , kahnert a , et al : anetumab ravtansine : a novel mesothelin - targeting antibody - drug conjugate cures tumors with heterogeneous target expression favored by bystander effect . 
le dt , brockstedt dg , nir - paz r , et al : a live - attenuated listeria vaccine ( anz - 100 ) and a live - attenuated listeria vaccine expressing mesothelin ( crs - 207 ) for advanced cancers : phase i studies of safety and immune induction . 
hollevoet k , nackaerts k , gosselin r , et al : soluble mesothelin , megakaryocyte potentiating factor , and osteopontin as markers of patient response and outcome in mesothelioma . 
hassan r , sharon e , thomas a , et al : phase 1 study of the antimesothelin immunotoxin ss1p in combination with pemetrexed and cisplatin for front - line therapy of pleural mesothelioma and correlation of tumor response with serum mesothelin , megakaryocyte potentiating factor , and cancer antigen 125 . 
creaney j , francis rj , dick im , et al : serum soluble mesothelin concentrations in malignant pleural mesothelioma : relationship to tumor volume , clinical stage and changes in tumor burden . 
hooper ce , lyburn id , searle j , et al : the south west area mesothelioma and pemetrexed trial : a multicentre prospective observational study evaluating novel markers of chemotherapy response and prognostication . 
onda m , nagata s , ho m , et al : megakaryocyte potentiation factor cleaved from mesothelin precursor is a useful tumor marker in the serum of patients with mesothelioma . 
iwahori k , osaki t , serada s , et al : megakaryocyte potentiating factor as a tumor marker of malignant pleural mesothelioma : evaluation in comparison with mesothel lung cancer 62 : 45 - 54 , 2008 28 . 
briefly , the mpf assay uses capture antibody mpf49 ( 2a , ) , which binds to mpf topographic epitope 3 , and detection antibody mpf25 ( 1 , ) , which binds to epitope 1.26 mpf49 was biotinylated , and mpf25 was conjugated with sulfo - tag nhs - ester ( meso - scale diagnostics , rockville , md )  . 
after incubation for 1 hour at room temperature , plates were washed , and the serially diluted mpf calibrator , 1 : 10 diluted sample serum , and reference samples were added and further incubated for 1 hour . 
the data were analyzed with workbench 4.0 software ( meso - scale diagnostic ) for determining the concentration of mpf in serum samples using the 4 parameter logistic nonlinear regression model . 
vokes , md1 , 2 ; david liu , md1 , 2 ; biagio ricciuti , md1 ; elizabeth jimenez - aguilar , md3 ; hira rizvi4 ; felix dietlein , md , phd1 , 2 ; meng xiao he5 ; claire a . 
elmarakeby , phd1 , 2 ; jeffrey girshman , md4 ; anika adeni1 ; francisco sanchez - vega , phd4 ; nikolaus schultz , phd4 ; suzanne dahlberg , phd1 ; ahmet zehir , phd4 ; pasi a . 
awad , md , phd1 purpose heterogeneity in tumor mutational burden ( tmb ) quantication across sequencing platforms limits the application and further study of this potential biomarker of response to immune checkpoint inhibitors ( icis )  . we hypothesized that harmonization of tmb across platforms would enable integration of distinct clinical data sets to better characterize the association between tmb and ici response . methods cohorts of patients with nonsmall - cell lung cancer sequenced by 1 of 3 targeted panels or by wholeexome sequencing ( wes ) were compared ( n = 7 , 297 )  . 
in subcohorts of patients treated with icis ( dana - farber cancer institute n = 272 ; memorial sloan kettering cancer center n = 227 ) , the association between tmb and outcome was assessed . 
receiver operating characteristic curves yielded an area under the curve of 0.614 , with no natural inection point . conclusion the z score conversion harmonizes tmb values and enables integration of data sets derived from different sequencing panels . 
tmb quantication from targeted next - generation sequencing ( ngs ) panels has been shown to correlate with whole - exome sequencing ( wes ) derived tmb13 , 18 - 20 and to associate with ici response , which makes the clinical assessment of tmb practically feasible.19 , 21 to date , the only approved biomarkers of ici response are mismatch repair deciency and , in nonsmall - cell lung cancer ( nsclc ) , programmed cell death - ligand 1 ( pd - l1 ) expression . 
 vokes et al context key objective it is not known how to account for differences in tumor mutational burden ( tmb ) generated by different sequencing assays . we sought to address assay heterogeneity in tmb quantication by developing a technique to harmonize tmb across assays and applied this technique to a pool of distinct clinical cohorts to better characterize the association between tmb and response to immune checkpoint inhibitors . knowledge generated tmb differs across sequencing assays because of differences in gene panels and sequencing pipelines . 
from this pooled analysis , we observed that tmb may not associate with response in patients who are never - smokers or harbor targetable oncogenes , and tmb thresholds yield signicant trade - offs in sensitivity and specicity . relevance standardization of z scores harmonizes tmb values across assays for pooled analysis . 
it is not known whether this threshold heterogeneity reects different tmb quantication that arises from different platforms , variation across patient cohorts , or unknown clinical or biologic effects on the association between tmb and response . given these questions , we sought to develop a strategy to harmonize tmb across ngs platforms . 
we applied this method to integrate multiple clinically annotated cohorts and to more fully characterize the relationship between tmb and ici response to add nuance and context to our current understanding . 
we focused on nsclc because of the early interest in applying tmb to clinical practice in this disease subtype24 - 26 and to avoid confounding of tmb by tumor type.27 methods study population three cohorts of patients with nsclc whose tumors had been proled by a targeted ngs panel were evaluated . these panel cohorts were compared with a fourth wes cohort from the cancer genome atlas ( tcga )  . dana - farber cancer institute cohort . 
patients at the danafarber cancer institute ( dfci ) whose tumors had undergone oncopanel ngs were included if they had advanced nsclc and had consented to institutional review boardapproved protocols . 
somatic wes data from nsclcs sequenced by tcga31 were downloaded from the cbioportal for cancer genomics . the dfci cohort was sequenced as previously described.32 , 33 in brief , tumor dna was extracted and used for customdesigned hybrid capture library preparation . 
all variants were reviewed for technical quality.34 finally , minimize inadvertent inclusion of germline variants , consistent with previous aggregation efforts , 35 an additional germline lter was applied to exclude events present in the exome aggregation consortium with an allele count  . 
foundation medicine uses an internal algorithm to lter putative germline events . tmb was uniformly calculated for each sample as the number of nonsynonymous mutations per megabase ( mb ) of genome covered . 
scans were reviewed by thoracic radiologists at each institution , and response was determined using recist version 1.1.37 progression - free survival was assessed from the start of ici treatment until the date of progression or death ; patients without progression were censored at last scan . 
6 months was dened as durable clinical benet ( dcb ) ; no durable benet ( ndb ) was dened as progressive disease ( pd ) or sd 6 months . 
patients censored before 6 months of follow - up were considered not evaluable . statistical analysis cohort - specic gene mutation averages were calculated by summing the number of mutations in each gene within a cohort and dividing the total by the number of patients in the cohort . 
the linear correlation between log average mutations per gene in the panel cohorts versus tcga was evaluated using pearsons correlation coefcient . power transformations were used to normalize cohortspecic tmb distributions ; tukeys ladder of powers38 in the rcompanion package39 was used to identify the optimal transformation coefcient . 
receiver operating characteristic ( roc ) curve analyses were performed using the proc and optimalcutpoints packages.41 , 42 exploratory cutoffs were selected to maximize the distance to the y = x line ( youdens index ) , maximize specicity with sensitivity  . 
human investigations were performed after approval by a local human investigations committee and in accordance with an assurance led with and approved by the department of health and human services , where appropriate . results comparison of tmb quantication across panel and wes platforms patients with nsclc whose tumors had undergone sequencing through oncopanel ( n = 1 , 157 ) , msk - impact ( n = 1 , 520 ) , foundation medicine ( n = 3 , 476 ) , or tcga ( n = 1 , 144 ) were included ( n = 7 , 297 ; see data supplement for cohort diagram and clinical characteristics )  . 
to determine whether tmb differed between platforms , we plotted the distribution of tmb within each cohort ( fig 1a )  . tmb distributions differed between cohorts , and targeted panels were associated with higher tmb values than wes . because targeted panels sequence fewer bases with focused inclusion of mutated cancer genes , we hypothesized that the higher tmb measurements associated with ngs panels were attributable to gene selection . 
we tested this by subsetting the wes data to include only those genes captured by the targeted panels ( downsampling ; data supplement ; fig 1b ) and found that downsampled distributions retained greater tmb counts than the unltered tcga distribution , which suggests that gene panel composition contributes to the observed difference in tmb distributions between cohorts . 
however , the relative differences were less pronounced than in the real - world cohort comparisons , which suggests that assay - specic differences , such as depth of sequencing and the absence of a paired germline sample , might also contribute to inter - test variation . to further examine assay - specic sources of variation in tmb across panels , we compared the average number of mutations per gene in each cohort against the tcga averages , surmising that this could reect differences in assay performance or mutation calling ( figs 1c - e )  . 
the left side shows the kernel density plot of unadjusted tmb values in each cohort , and the right side shows the transformed density plot of tmb z scores that demonstrate high overlap . 
use of a power transformation converted the right - skewed tmb distributions ( fig 1f ) to normal distributions ( skewness values 0.06 ; data supplement ) , and standardization to z scores brought the tmb distributions into good concordance ( fig 1f ) with  . 
sampling simulations ( data supplement ) suggest that this negative nding may be due to decreased power in this subset , although lower tmb values and distinct biology may also contribute ( data supplement )  . 
similar exploratory analyses of patients who harbor targetable oncogenic drivers did not demonstrate an association between tmb z score and dcb ( total n = 74 ) , although power in these small driver subgroups was also limited ( fig 2e )  . 
300 may be necessary to detect a difference in tmb between patients with dcb and ndb in groups with lower response rates or effect sizes ( data supplement )  . tmb thresholds and response given the heterogeneity in previously identied thresholds and the percentile cut points used to identify such thresholds , we used our pooled cohort to systematically explore the relationship between tmb and response to icis across the tmb distribution . 
we calculated the rate of dcb and cr / pr with increasing tmb thresholds in the pooled and separate ici cohorts ( fig 3a ; data supplement )  . table 2 lists the tmb z scores and values associated with each threshold . 
we noted , however , that this could arise from enriching for high tmb outliers and therefore calculated the rate of dcb within each tmb decile ( joint cohort shown in fig 3b ; separate cohorts shown in the data supplement )  . 
in this analysis , we noted high dcb rates in the highest deciles ( 40.4% in patients with tmb z scores between the 80th and 90th percentiles ; 53.1% in patients with tmb z scores 90th percentile ) and low rates in the lowest deciles ( 16.7% in patients with tmb z scores , 10th percentile )  . 
the pattern of association between pd - l1 and dcb was similar to tmb , with increasing rates of dcb with higher pd - l1 thresholds but more variability within pd - l1 score groupings ( data supplement )  . given the heterogeneity of response rates over the mid - tmb distribution , we used roc curve analysis to formally quantify how well tmb z scores discriminate between dcb and ndb . roc analysis yielded an area under the curve ( auc ) of 0.614. 
the youdens index cutoff was associated with a sensitivity of 61.8% and a specicity of 57.3% , which resulted in undertreatment of 12% of patients and overtreatment of 30% ( fig 3d ; table 3 )  . 
analysis of tmb thresholds with respect to progression - free survival , rather than response , demonstrated similar results ( data supplement )  . abbreviations : cr , complete response ; ctla - 4 , cytotoxic t - cell lymphocyte - 4 ; dcb , durable clinical benet ; dfci , dana - farber cancer institute ; mskcc , memorial sloan kettering cancer center ; ndb , no durable benet ; pd , progressive disease ; pd - ( l ) 1 , programmed cell death 1 or programmed cell death - ligand 1 ; pr , partial response ; sd , stable disease . discussion we present a pragmatic comparison of tmb calculated from targeted panels and wes and apply tmb z score conversion to enable harmonized analyses . 
in addition , our use of realworld data sets allows us to incorporate and account for sources of variation not captured by in silico downsampling analyses , such as differences in mutation / indel calling pipelines , depth of coverage , and germline ltration . 
tmb z score deciles were selected as cut points , and rate of dcb was calculated for patients in the joint cohorts whose tmb z scores were greater than or equal to the cut point . 
auc , area under the curve . efforts , 22 , 43 which focus on standardization of tmb denitions and reporting and eventually aim to generate gold standard cell lines for benchmarking . 
we anticipate that our approach will be of immediate use to both clinicians and researchers and anticipate that it can be easily applied to other platforms and relevant tumor types . although the association between tmb and response to icis in nsclc has been demonstrated , less is understood about how clinical and biologic features affect this association . 
equivalent tumor mutational burden ( tmb ) values in the dfci , mskcc , foundation medicine , and tcga cohorts are shown . abbreviations : dfci , dana - farber cancer institute ; mskcc , memorial sloan kettering cancer center ; tcga , the cancer genome atlas . underpowered to detect a difference , and our power simulations indicated that larger cohorts are needed and caution against denitive conclusions in these small subgroup analyses . 
however , we also observed that neversmokers who benetted from icis had markedly lower tmb values than ever - smokers who did not , which suggests that further study to identify tmb - independent predictors of response in never - smokers may be warranted and raises the important possibility that the clinical application of tmb as a biomarker will need to take clinical and biologic features into account . the importance of context is further emphasized by our analysis of tmb thresholds . 
prior analyses have generally focused on identifying a single threshold to dene tmbhigh and tmb - low subgroups , with variation in selected thresholds across studies.13 , 15 , 26 , 44 our systematic analysis of tmb thresholds illustrates additional nuances in the relationship between tmb and response . 
we observed enrichment in dcb with higher tmb thresholds , as expected , but weaker discrimination in the midrange of tmb values without a single , natural biologic inection point . these ndings may account for some of the observed heterogeneity among previously proposed thresholds , as there may be a range of values that discriminate similarly between responders and nonresponders . 
in addition , our data suggest that the choice of a given threshold must be decided within a goal - specic context that considers the relative efcacy of the alternative treatment ; a tmb threshold selected to enrich for response to rst - line therapy may be different than a threshold selected for second - line therapy . 
of note , tmb is independent of pdl1 expression , 12 , 13 with similar biomarker performance : increasing expression is associated with improved efcacy without a natural cut point , there is variability in dcb enrichment within deciles of expression , and distinct thresholds are appropriately applied on the basis of the specic treatment scenario ( ie , 50% , 1% , none ) .3 , 5 , 45 ultimately , these data do not answer whether and how tmb should be applied to clinical practice , as this must be examined through prospective clinical trials , but add nuance to our understanding of how tmb associates with response . one limitation of this study is that our comparison of tmbs assumes that the observed distinctions reect differences in platforms rather than in patients / samples . 
we were not able to account for clinical and tumor features because of inconsistent sample annotation but note that our large cohorts help to mitigate sampling bias , and the overall consistencies in shape of distribution are reassuring . whether tmb distributions should be more narrowly table 3 . 
 vokes et al dened by sample features , such as histology or stage , is an open question , and the normalization we describe here can be adjusted as more is learned . 
at present , however , tmb is compared across patients and biopsy specimens without reference to these sample characteristics , which makes this aggregated approach consistent with current clinical practice . in conclusion , we provide a practical approach to the challenge of standardizing tmb across platforms , and we apply this approach to integrate distinct data sets to better understand how tmb associates with response . 
is a damon runyon clinical investigator supported ( in part ) by the damon runyon cancer research foundation ( ci - 98 - 18 ) and is a member of the parker institute for cancer immunotherapy . 
margolis employment : verana health suzanne dahlberg consulting or advisory role : astrazeneca patents , royalties , other intellectual property : patent pending for a statistical model assessing tumor growth ( inst ) pasi a . 
vokes , biagio ricciuti , elizabeth jimenez - aguilar , hira rizvi , jeffrey girshman , anika adeni , suzanne dahlberg , ahmet zehir , mizuki nishino , renato umeton , lynette m . 
sholl honoraria : astrazeneca consulting or advisory role : foghorn therapeutics , loxo oncology research funding : genentech ( inst ) travel , accommodations , expenses : bristol - myers squibb eliezer m . 
van allen stock and other ownership interests : syapse , tango therapeutics , genome medical , microsoft , ervaxx consulting or advisory role : syapse , roche , third rock ventures , takeda pharmaceuticals , novartis , genome medical , invitae , illumina , tango therapeutics , ervaxx speakers bureau : illumina research funding : bristol - myers squibb , novartis patents , royalties , other intellectual property : patent on discovery of retained intron as source of cancer neoantigens ( inst ) , patent on discovery of chromatin regulators as biomarkers of response to cancer immunotherapy ( inst ) , patent on clinical interpretation algorithms using cancer molecular data ( inst ) travel , accommodations , expenses : roche , genentech matthew d . 
hellmann stock and other ownership interests : shattuck labs honoraria : astrazeneca , bristol - myers squibb consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca , medimmune , novartis , janssen pharmaceuticals , nektar , syndax , mirati therapeutics , shattuck labs research funding : bristol - myers squibb ( inst ) patents , royalties , other intellectual property : a patent has been led by memorial sloan kettering ( pct / us2015 / 062208 ) for the use of tumor mutation burden for prediction of immunotherapy efcacy and which is licensed to personal genome diagnostics ( inst ) travel , accommodations , expenses : astrazeneca , bristol - myers squibb mark m . 
awad consulting or advisory role : genentech , merck , pzer , boehringer ingelheim , abbvie , astrazeneca , medimmune , clovis oncology , nektar , bristol - myers squibb , ariad pharmaceuticals , foundation medicine , syndax , novartis , blueprint medicines , maverick therapeutics research funding : bristol - myers squibb , genentech ( inst ) , roche ( inst ) , eli lilly ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) no other potential conicts of interest were reported . references garon eb , rizvi na , hui r , et al : pembrolizumab for the treatment of non - small - cell lung cancer . 
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hansen , md , phd1 , 2 ; lars henrik jensen , md , phd1 , 2 ; and anders jakobsen , dmsc1 , 2 purpose analysis of circulating tumor dna ( ctdna ) is a potential improvement in precision medicine . 
plasma samples represented healthy donors and localized and metastatic crcs . results the level of neuropeptide ymethylated dna in the tissue cohorts differed between nonmalignant and malignant / premalignant tissues with minimal overlap . 
furthermore , meth - ctdna was detected in plasma from 100% of patients with metastatic disease , compared with 67% of those with localized disease and 8% of healthy donors . 
2019 by american society of clinical oncology introduction circulating tumor - specic dna ( ctdna ) is an attractive biomarker for obvious reasons , such as easily repeated access , better reection of overall tumor biology , and timely correct tumor mutational status . 
consequently , the era is marked by enthusiasm , but it should be noted that its clinical utility , with few exceptions , remains to be proven.1 ctdna can be determined by the presence of tumorspecic genetic or epigenetic alterations . 
ngs allows identication of mutations of interest and is a relatively broad approach applicable in the identication of mutational patterns and quantication of specic mutations , but this method is time and resource consuming . 
different platforms may lead to contradictive results , as shown in a recent report , with only 60% agreement between analyses of the same mutations.2 the second method relies on pcr with analysis of specic mutations . 
compared with ngs , pcr , especially digital pcr , has a faster data turnaround time3 and lower costs , but direct pcr is only applicable in the fraction of patients with known specic mutations . in colorectal cancer ( crc ) , ras / raf mutations are of interest , because their presence in tumor tissue contraindicates treatment with monoclonal antibodies cetuximab and panitumumab . 
multiplex technology allows for screening of 27 mutations in the same analysis , 4 but even so , only approximately 60% of patients present with a ras / raf - mutated tumor . 
 thomsen et al context key objective can circulating tumor - specic methylated dna serve as a universal biomarker in colorectal cancer ? knowledge generated methylated dna was tumor specic in different cohorts including tissue as well as plasma . 
high correlation was found between mutated and methylated dna in both localized and metastatic disease . relevance circulating tumor - specic methylated dna holds promise as a universal colorectal cancer marker that can be analyzed in a simple , highly reproducible approach . most of these patients , the same tumor - specic mutation is detectable in ctdna ( mut - ctdna )  . 
dna was eluted in 50 ml of nuclease - free water and further diluted with nuclease - free water , if necessary . aberrant methylation is an early event in carcinogenesis and occurs in almost all malignant tumors as methylation of promoter regions causing inactivation of genes . 
this , along with the stability of methylation changes , makes it a relevant biomarker for early diagnosis.5 analysis of abnormally methylated dna in plasma ( meth - ctdna ) has been proposed for screening , 6 and a test for crc has been approved by the us food and drug administration.7 however , because of insufcient sensitivity and specicity , it has not been generally accepted . 
the neuropeptide y gene ( npy ) has been correlated with invasion and proliferation.8 , 9 exogenous npy has been shown to inuence the growth of malignant cholangiocarcinoma cells in vitro and inhibit invasion of crc cells . 
in this disease , hypermethylation of the npy promoter region has been correlated with inactivation of gene expression and therefore carcinogenesis , and currently , hypermethylation of the npy gene is suggested as a blood - based biomarker.10 - 12 the purpose of our study was to compare mutated dna with methylated dna in malignant and nonmalignant colorectal tissue and plasma with the aim of determining a method applicable in all patients with crc . plasma sampling and purication in edta tubes , 9 - ml blood samples were collected from donors and different cohorts of patients . 
plasma was centrifuged again at 10 , 000 g for 10 minutes before purication , and cysteine - rich polycomb - like protein 1 ( cpp1 ) dna fragments were added as exogenous internal control.13 dna from patients was puried from 2 2 or 2 4 ml of plasma on the qiasymphony sp instrument using the qiasymphony circulating nucleic acid kit ( qiagen , hilden , germany ) according to manufacturer instructions . dna from healthy donors was puried from 1 4 ml of plasma . dna was eluted in 60 ml of the supplied buffer and water added to 400 ml . 
three 15 - mm slices of ffpe tissue were subjected to 180 ml of incubation buffer and 20 ml of protein kinase k overnight at 70c ; 400 ml of lysis buffer adenomas and tumor tissue samples were screened for ras / raf mutations as previously described.14 samples from adjacent tissue and plasma were analyzed for the specic mutation by droplet digital pcr in two wells . positive controls for each mutation ( gblocks ; idt , carolville , ia ) or mutated fragments generated according to spindler et al , 15 genomic donor dna , and water were included in the analyses as controls . 
patients with mcrc had plasma analyzed both at baseline and after the rst treatment cycle . tissue methylation in 25 nonneoplastic specimens , all but one were nonmethylated ( 4% were npy positive )  . 
figure 1 shows the results of the tissue npy methylation analysis , with methylated npy presented as actual clearly shows that the level of npy methylation was different in malignant and nonmalignant tissues . 
the range of npy fractions . mutated and methylated dna in colorectal cancer methylation analysis tumor - specic methylated dna was dened as dna with methylation of the npy gene.12 before droplet digital pcr methylation analysis , bisulte conversion of circulating and ffpe - isolated dna was performed as recommended by the manufacturer ( zymo research , irvine , ca )  . 
water and a pool of lymphocyte dna from cancer - free individuals were included in each round of analyses as negative controls ; universal human methylated control dna ( zymo research ) and epitech control dna ( qiagen ) were included as positive controls . 
the upper limit of the 95% ci was 1.8% , and therefore , the cutoff value was set to 2% . limit of blank in plasma limit of blank ( lob ) in the mutation analysis was determined by donor controls . 
because fewer than two fampositive droplets were observed in all analyses of the genomic donor dna controls and plasma dna from healthy individuals as previously described , 16 plasma samples with more than two fam - positive droplets in two wells were classied as positive . lob in the methylation analysis was dened as the quantity of npy droplets counted in control dna samples from a test cohort of healthy individuals ( n = 50 )  . 
correlations are also illustrated in the scatter plots shown in figures 3 , 4a , and 4b , which represent correlation between meth - ctdna and mut - ctdna in the localized and metastatic settings at baseline and in the metastatic setting after the rst treatment cycle , respectively . discussion our study on tissue and plasma samples from donors and different stages of crc indicates that meth - ctdna correlated with mut - ctdna across the cohorts and that methctdna was detectable in cases without activating dna mutations . 
therefore , meth - ctdna may be a universal biomarker in crc from the perspectives of detection and monitoring . key challenges in cancer management are early diagnosis and close monitoring during treatment and follow - up with minimal harm to the patients . 
in the landscape of tumor markers , ctdna represents a relatively new approach with the potential for progress in cancer management , because it contains the same molecular alterations as the corresponding tumor and potential metastases . 
even so , clinical utility has been limited . recently , presence of ctdna was conrmed in wt patients using epigenetic modications such as hypermethylation.17 - 19 meth - ctdna seems to represent tumor - specic dna and is found in nearly all colorectal adenocarcinomas , 10 as opposed to ctdna based on ras / raf mutations . 
three recent studies have suggested that hypermethylation of the npy gene may serve as a biomarker for monitoring the treatment of crc , 10 , 11 , 20 but a detailed comparison of mutated and methylated dna motivated our study . the level of methylation varied among different cohorts with malignant and nonmalignant tissues , the latter in general being negative . 
fifty healthy donors were only analyzed for methylated ctdna ( methctdna ) , and 20 healthy donors were analyzed for kras g12d mutated ctdna ( mut - ctdna )  . 
plasma was drawn from patients with localized ras / raf - mutated tumors ( n = 27 ) and metastatic ras / rafmutated tumors ( n = 20 ) and analyzed for the same specic mutations and methylation . methylation in tumors did not overlap that of nonmalignant npy methylation , except in three cases ( 3% )  . plasma methylation figure 2 shows the plasma analysis of different cohorts . samples from healthy donors showed that four ( 8% ) of 50 had detectable meth - ctdna above the lob . 
furthermore , the analysis showed that 67% ( 18 of 27 ) of patients with localized crc had mut - ctdna , compared with 52% ( 14 of 27 ) with meth - ctdna . 
scatter plot showing correlation of methylated circulating tumor dna ( ctdna ) and mutated ctdna ( mut - ctdna ) in localized disease . almost complete separation of malignant and nonmalignant tissues based on the statistical variation of the observed frequencies in healthy individuals . 
adjacent tissue showed npy hypermethylation in one third of the samples , although they were just positive ; none were mutated , despite ras / raf mutations in the nearby tumor . 
scatter plots showing correlation of methylated circulating tumor dna ( ctdna ) and mutated ctdna ( mut - ctdna ) in metastatic colorectal cancer ( a ) at baseline and ( b ) after one cycle of treatment . furthermore methylation is an early event in carcinogenesis , 22 which may represent a potential universal biomarker.23 all tumor tissue samples were hypermethylated irrespective of mutational status and to the same extent as ras / raf - mutated adenomas . 
this indicates that aberrant methylation takes place as an early part of cancer progression , which can predispose to additional genetic alterations.24 possibly , these epigenetic changes give an important and early window for therapeutic interventions in patients with crc . plasma analyses showed that the frequency of patients with ctdna varied depending on disease stage . 
lob of two positive droplets per reaction determined in a test cohort of 50 healthy donors seems in good agreement with previous results reporting an lob of 3.30 on the basis of 17 control dna samples without hypermethylated npy.11 the two self - reported healthy donor cohorts with 4% ( two of 50 ) and 8% ( four of 50 ) of patients having more than two positive droplets per reaction indicate good agreement . 
therefore , occurrence of aberrant methylation with increasing age does not seem to be a major problethe false - positive rate may be acceptable for patients with advanced disease , and therefore , clinical application of meth - ctdna in metastatic disease seems encouraging . 
in localized tumors , two thirds of patients harbored mut - ctdna and meth - ctdna , which is in accordance with current literature.10 in the metastatic setting , all indicating its potential as patients had meth - ctdna , a general biomarker . 
they found that 77% had detectable ctdna at baseline , assessed by mut - ctdna and meth - ctdna . boeckx et al11 reported that 87.5% of all baseline plasma samples were positive for npy methylation in 24 patients with mcrc . 
varying methods of analysis , which lack standardization throughout the eld of research in ctdna , are one obvious reason for the lower frequency of patients with detectable ctdna compared with our ndings . correlation between mut - ctdna and meth - ctdna was investigated to compare the two potential biomarkers . 
this is in agreement with previous studies concluding that methylated markers in ctdna could replace tumor - specic mutations in the blood.10 this conclusion was based on a correlation coefcient of r = 0.94 between mut - ctdna ( kras , braf , and tp53 ) and meth - ctdna ( npy )  . 
we did not investigate the potential role of meth - ctdna in monitoring wt patients , but we found a strong correlation between mut - ctdna and meth - ctdna after one cycle of treatment , which emphasizes the role of meth - ctdna in treatment monitoring . 
taken together , the current literature indicates high agreement between mut - ctdna and meth - ctdna , 10 , 11 , 20 further supported by our results . a minor disadvantage in the methylation assays is the need for bisulte conversion , which can degrade dna and therefore requires additional material . 
however , the need for prior establishment of mutation status , as with mutctdna , is bypassed , and therefore , meth - ctdna is applicable in nearly all patients with crc . 
it should be noted that meth - ctdna is not relevant in the selection of patients for targeted treatment with epidermal growth factor receptor inhibitors . in conclusion , to our knowledge , our study represents the rst detailed comparison of methylated and mutated dna in normal tissue as well as in localized and metastatic tumors . 
this indicates that hypermethylated npy in plasma is applicable as a universal biomarker in all patients with mcrc , but further investigation of clinical utility is warranted . affiliations 1danish colorectal cancer center south , vejle hospital , vejle , denmark 2university of southern denmark , odense , denmark relationships are self - held unless noted . 
all relationships are considered compensated . lars henrik jensen research funding : merck sharp & dohme ( inst ) travel , accommodations , expenses : bayer healthcare pharmaceuticals no other potential conicts of interest were reported . acknowledgment we thank the study participants and the staff at vejle hospital who collected samples for this study . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
jama oncol 4 : 868 - 870 , 2018 thierry ar , el messaoudi s , mollevi c , et al : clinical utility of circulating dna analysis for rapid detection of actionable mutations to select metastatic colorectal patients for anti - egfr treatment . 
front mol biosci 2 : 13 , 2015 church tr , wandell m , lofton - day c , et al : prospective evaluation of methylated sept9 in plasma for detection of asymptomatic colorectal cancer . 
boeckx n , op de beeck k , beyens m , et al : mutation and methylation analysis of circulating tumor dna can be used for the follow - up of metastatic colorectal cancer patients . 
roperch jp , incitti r , forbin s , et al : aberrant methylation of npy , penk , and wif1 as a promising marker for blood - based diagnosis of colorectal cancer . 
spindler kl , pallisgaard n , vogelius i , et al : quantitative cell - free dna , kras , and braf mutations in plasma from patients with metastatic colorectal cancer during treatment with cetuximab and irinotecan . 
thomsen cb , hansen tf , andersen rf , et al : monitoring the effect of rst line treatment in ras / raf mutated metastatic colorectal cancer by serial analysis of tumor specic dna in plasma . 
garlan f , laurent - puig p , sefrioui d , et al : early evaluation of circulating tumor dna as marker of therapeutic efcacy in metastatic colorectal cancer patients ( placol study )  . 
step two was 44 cycles at 95c for 15 seconds and 56c for 1 minute , with a 1.5c per second ramp rate . step three was at 98c for 10 minutes . 
carriers are predisposed to a higher risk for developing colorectal , endometrial , and extracolonic cancers , including cancers of the stomach , ovary , small bowel , hepatobiliary and urinary tracts , skin , pancreas , and prostate . 
primary brain tumors ( pbts ) are a rare feature of ls , with an estimated lifetime risk of 1% to 6%.1 , 2 here , we report the case of a patient with a who grade iii glioneuronal tumor and pathogenic germline msh2 variant . 
microscopic examination revealed a high - grade glioma with eosinophilic granular bodies , elevated mitotic activity ( approximately 10 / 10 high - power eld [ hpf ] ) , vascular proliferation , and necrosis consistent with an anaplastic glioneuronal tumor ( who grade iii )  . tumor cells were positive for glial brillary acidic protein ( gfap ) and synaptophysin ( fig 2 )  . 
the mib - 1 proliferative index ( ki - 67 ) was approximately 10% . the patients initial postoperative imaging revealed no residual disease ; therefore , no adjuvant therapy was offered . 
postoperative head ct ( c ) with and ( d ) without contrast at the patients most recent follow up , 105 months postinitial diagnosis , shows postoperative changes of the left frontal lobe without evidence of tumor recurrence . disease progression identied pathogenic genomic alterations in six genesnf1 , pdgfra , atm , tp53 , ctnna1 , and msh2and 18 variants of uncertain signicance ( table 1 )  . 
follow - up ihc studies identied a loss of msh2 and msh6 protein expression in tumor cells , which is consistent with an ls - associated tumor and underlying msh2 germline mutation . 
microscopic examination revealed a high - grade glial neoplasm with ( a ) scattered pleomorphic cells , ( b ) spindle cells , and mitotic activity . necrosis and vascular proliferation were observed . 
immunostains showed that the tumor is positive for ( c ) gfap and ( d ) synaptophys ( e ) ki - 67 was moderately elevated and a ( f ) neurolament stain was negative within the tumor , highlighting a compact growth pattern . 
immunohistochemistry identied loss of ( g ) msh2 and ( h ) msh6 protein expression in tumor cells , with retained nuclear expression in the normal endothelial cells in the blood vessels . magnication of all images is 200 . 
glioblastoma is the most common pbt associated with ls.3 astrocytoma , oligodendroglioma , gliosarcoma , medulloblastoma , and neuroblastoma have also been reported.4 individuals with msh2 mutations have higher rates of pbts compared with carriers of other mmr mutations.5 the average age of pbt diagnosis occurs a decade earlier in individuals with ls , 4 and the age range for msh2 carriers is 33 to 53 years.1 , 3 , 6 , 7 ls is one of several hereditary cancer syndromes that predispose to pbts and other systemic cancers . 
therefore , interrogation of personal and family history of malignancies is critical for patients with d 70s dx 47 d 52 d 50s d 50s d 30s d 50s d 40s d 60 dx 42 5 polyps 2 polyps throat abdominal cancer , other breast cancer colorectal cancer glioneuronal tumor fig 3 . 
the patients family history is notable for multiple maternal family members affected with early - onset colorectal cancer , including his mother and multiple maternal aunts , uncles , and cousins . 
next - generation sequencing of 236 genes in the patients tumor specimen ( solid tumor panel ; foundationone , cambridge , ma ) identied pathogenic genomic alterations in six genes and 18 variants of uncertain signicance . * follow - up sequencing of msh2 in the patients saliva sample ( ambry genetics , aliso viejo , ca ) also identied the msh2 mutation in the germline sample . pbt as for all patients with cancer . 
referral for genetic counseling and germline testing is recommended for any patient with pbt with multiple relatives affected with earlyonset cancers , individual ( s ) with multiple primary cancers , and / or rare or syndrome - specic patterns of malignancies.8 , 9 appropriate germline genetic testing may result in additional screening guidelines and the identication of other at - risk relatives.10 ls surveillance guidelines include colonoscopy every 1 to 2 years starting at age 20 to 25 years or 10 years before the earliest crc diagnosis in the family.11 histologic ndings in this patients pbt showed overlapping features between anaplastic pleomorphic xanthoastrocytoma , who grade iii , and glioblastoma . 
genetic alterations that are present in the tumor tissuethat is , nf1 , pdgfra , and tp53 mutationshave been described in glioblastomas12 , 13 ; however , survival of 8 years would be unusual for a patient with glioblastoma . one indicator that germline molecular testing was warranted for this patient was the identication of an msh2 mutation in his tumor specimen . 
studies that have evaluated the yield of germline variants after somatic testing indicate that a small but signicant number of tumors possess germline mutations related to hereditary cancer predisposition syndromes.14 - 17 currently , consideration of follow - up germline testing is recommended after identication of somatic egfr t790m mutations in lung cancer or brca1 / 2 mutations in any tumor.18 - 21 interpretation of somatic mmr mutations , however , is more complex . hampel et al22 used tumor sequencing to screen for ls in a cohort of patients with crc in which a positive screen for ls was given to any patient who had mutation ( s ) identied in at least one mmr gene at a variant allele fraction that was suggestive of a germline mutation , with msi and braf v600e status taken into account . 
therefore , whereas the identication of somatic mmr mutation ( s ) is not diagnostic of ls , it does suggest that follow - up germline evaluation is warranted in these patients . identifying germline and / or somatic mmr mutations may affect treatment offerings , such as consideration for immune checkpoint inhibitors ( icis ) , which target checkpoint receptors of mmr - decient cancers.23 - 25 early studies have demonstrated that icis can effectively treat high tmb cancers ; mmr - decient tumors can possess 10 to 100 times the tmb compared with mmr - procient cancers.26 - 28 glioblastoma specimens from patients with constitutional mmr deciency caused by biallelic germline mmr mutations have signicantly higher tmb compared with sporadic gliomas and other pbts.29 whereas icis have primarily been evaluated in crc and endometrial carcinomas , therapeutic potential has been demonstrated in other mmrdecient tumors . 
in patients with recurrent tumors , high tmb may indicate resistance to traditional chemotherapy and necessitate targeted treatment with icis or other immunotherapies.30 these results must be validated on a larger scale to inform clinicians of the potential therapeutic benets of ici in this subset of patients . in conclusion , we report the rst case of an individual with anaplastic glioneuronal tumor with atypical histologic features and paired somatic and germline msh2 mutations , indicating the diversity of pbts observed within ls . 
the presence of mmr gene mutation ( s ) in tumor specimens indicate that additional genetic evaluation is warranted . ihc , msi , and tmb analyses are also supportive of an ls diagnosis . 
furthermore , a family history evaluation for multiple relatives affected with early - onset cancers , dividual ( s ) with multiple primary cancers , and / or rare or syndrome - specic patterns of malignancies is imperative for all patients with pbt . 
in addition , identifying mmr deciency in the germline or tumor specimens may be an indication for targeted therapy via ici or other immunotherapies in the future . affiliations 1the university of texas md anderson cancer center , houston , tx 2university of texas health science center at houston , houston , tx 3foundation medicine , morrisville , nc 4wake forest school of medicine , winston - salem , nc relationships are self - held unless noted . 
qualmann provision of study materials or patients : jay - jiguang zhu , krista j . qualmann collection and assembly of data : sarah azam , jay - jiguang zhu , krista j . 
ramkissoon employment : foundation medicine stock and other ownership interests : foundation medicine sigmund hsu consulting or advisory role : abbvie , cns pharmaceuticals research funding : abbvie patents , royalties , other intellectual property : partial patent holder , royalties ; at the time of ling , was associated with md anderson cancer center jay - jiguang zhu consulting or advisory role : tocagen research funding : novocure ( inst ) , boston biomedical ( inst ) , five prime therapeutics ( inst ) , tocagen ( inst ) , immunocellular therapeutics ( inst ) travel , accommodations , expenses : zai lab krista j . 
qualmann employment : my gene counsel no other potential conicts of interest were reported . references vasen hfa , stormorken a , menko fh , et al : msh2 mutation carriers are at higher risk of cancer than mlh1 mutation carriers : a study of hereditary nonpolyposis colorectal cancer families . 
int j cancer 81 : 214 - 218 , 1999 therkildsen c , ladelund s , rambech e , et al : glioblastomas , astrocytomas and oligodendrogliomas linked to lynch syndrome . 
n engl j med 348 : 919 - 932 , 2003 vasen hfa , sanders eacm , taal bg , et al : the risk of brain tumours in hereditary non - polyposis colorectal cancer ( hnpcc )  . 
hampel h , bennett rl , buchanan a , et al : a practice guideline from the american college of medical genetics and genomics and the national society of genetic counselors : referral indications for cancer predisposition assessment . 
catenacci dv , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
b. , et al : molecular testing guideline for selection of lung cancer patients for egfr and alk tyrosine kinase inhibitors : guideline from the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology . 
hampel h , pearlman r , beightol m , et al : assessment of tumor sequencing as a replacement for lynch syndrome screening and current molecular tests for patients with colorectal cancer . 
sloan ea , ring kl , willis bc , et al : pd - l1 expression in mismatch repair - decient endometrial carcinomas , including lynch syndrome - associated and mlh1 promoter hypermethylated tumors . 
science 357 : 409 - 413 , 2017 johnson a , severson e , gay l , et al : comprehensive genomic proling of 282 pediatric lowand high - grade gliomas reveals genomic drivers , tumor mutational burden , and hypermutation signatures . 
 genomic and immune proling of a patient with triple - negative breast cancer that progressed during neoadjuvant chemotherapy plus pd - l1 blockade david casadevall , md1 , 2 ; xiaotong li , phd1 ; ryan l . 
wali , phd1 ; natalia buza , md1 ; vasiliki pelekanou , md , phd1 ; arjun dhawan , md1 ; julia foldi , md , phd1 ; borbala szekely , md , phd1 , 3 ; francesc lopez - giraldez , phd4 ; christos hatzis , phd1 ; and lajos pusztai , md , dphil1 introduction preliminary results from neoadjuvant trials combining immune checkpoint blockade ( icb ) with standardof - care chemotherapy suggest high pathologic complete response rates that range between 50% and 80% in triple - negative breast cancer ( tnbc ) .1 - 3 adding atezolizumab to nab - paclitaxel for rst - line treatment of metastatic tnbc signicantly improved response rate and progression - free survival compared with nabpaclitaxel alone , suggesting synergy between icb and chemotherapy.4 however , not all patients respond to icb , and a minority exhibit rapid progression of their disease.5 patients who experience exceptionally favorable or unfavorable responses provide unique opportunities for studying disease biology and for identifying response markers . 
progression during neoadjuvant chemotherapy is a rare event in tnbc . here , we report results from the molecular analysis of a tnbc that rapidly progressed during neoadjuvant chemotherapy plus programmed death - ligand 1 ( pdl1 ) blockade in a clinical trial neoadjuvant medi4736 concomitant with weekly nab - paclitaxel and dosedense ac for stage i - iii triple negative breast cancer ( clinicaltrials.gov identier : nct02489448 )  . 
baseline tumor - inltrating lymphocyte ( til ) count was 10% ( cd4 , 5% ; cd8 , 5% ; and cd20 , 1% ) , macrophage ( cd68 ) was 1% , and tumor cellularity was 50% . 
the patient agreed to participate in a neoadjuvant phase i / ii clinical trial that combined durvalumab ( 10 mg / kg once every 2 weeks ) with once - per - week nabpaclitaxel ( 100 mg / m2 ) for 12 cycles and dosedense doxorubicin plus cyclophosphamide ( ddac ) for 4 cycles . 
after 8 weeks of nab - paclitaxel plus durvalumab , physical examination showed increased tumor size and new skin edema conrmed by repeat mammogram and ultrasonograrepeat cnb showed 60% tumor cellularity but also an increase in til count to 20% ( cd4 , 10% to 15% ; cd8 , 5% ; and cd20 , 0% ) and an increase in macrophages ( cd68 , 20% )  . 
nab - paclitaxel was stopped but because of the increased immune inltration , durvalumab was continued , and the patient was administered ddac , which led to disease stabilization after four courses of therapy . 
because of the apparent clinical benet , she received two additional courses of ddac without durvalumab off protocol and underwent right skin - sparing mastectomy and lymph node dissection . pathology showed extensive multifocal disease ( largest focus , 2.4 cm ; tumor cellularity , 40% ) with lymphovascular invasion in the breast and more than 10 positive axillary lymph nodes ( ypt2 , ypn3 )  . 
immune cell proportions in the mastectomy were tils , 20% ; cd4 , 10% ; cd8 , 10% ; cd20 , 1% ; and cd68 , 10% . dna and rna were extracted from formalin - xed parafn - embedded sections of tumor samples obtained at baseline , at week 8 , and from the mastectomy . 
til counts and immune cell subtypes were determined by routine pathology and immunohistochemistry . when we compared our patients baseline expression of 26 immune cell types and 100 immune function metagenes with those in the reference cohort , her neutrophil metagene expression was below the 2.5th percentile , whereas the cell cycle and immunosuppression metagenes were above the 97.5th percentile of the reference distribution ( fig 1a ) , indicating a highly proliferative tumor with an immunosuppressed microenvironment . 
the tumor also showed low expression of two previously validated immunotherapy predictive gene signatures , 8 , 9 indicating low probability of response to icb ( fig 1b )  . 
single - gene level analysis revealed signicantly low expression of 27 genes including pdcd1 , cd8a , and klrc2 ( fig 1c ) , suggesting impaired t - cell and natural killer ( nk ) cell activity . 
in addition , we found high exincluding tgfb , hla - g , cd63 , pression of 33 genes , ccl28 , and cxcl16 ( fig 1d ) , which are associated with an immune evasive phenotype , increased cell motility , and invasion . 
overall , greater changes were observed between week 8 and mastectomy ( ddac treatment ) than between baseline and week 8 ( nab - paclitaxel treatment )  . we observed upregulation of fos , abcb1 , kir3dl3 , gzma , and gzmk in the mastectomy ( single - gene and metagene expression changes are provided in the data supplement )  . 
to study this further , we next analyzed t - cell exclusion and dysfunction features using the tumor immune dysfunction and exclusion ( tide ) method ( data supplement ) .10 in concordance with our previous ndings , cytotoxic t - cell inltration increased during the second period . 
however , this was accompanied by an increase in t - cell dysfunction score , indicating an ineffective immune response ( fig 2b )  . we also performed whole - exome sequencing of baseline and mastectomy specimens . 
other mutations with the highest variant allele frequency at baseline included znf385c , cacna1e , nxpe1 , and dync1h1 , which have poorly understood functions in cancer ( fig 2c ; data supplement )  . 
we also detected amplications in fgfr1 , fgf2 , fgf3 , myc , mcl1 , ccnd1 , and tgfb2 and deletions in cdkn2a and cdkn2b ( data supplement )  . 
by using sciclone ( waltham , ma ) 11 and clonevol , 12 we identied four distinct tumor clones , all present at baseline and in the mastectomy specimen , with little evidence for clonal selection during therapy ( figs 2c - d )  . 
compound heterozygous inactivating mutations cause severe combined immune deciency.14 discussion this cancer showed primary resistance to nab - paclitaxel and ddac chemotherapy concurrent with an anti - pd - l1 agent . 
the tumor harbored several poor prognostic genomic alterations at diagnosis , including a p53 mutation and coamplication of myc and mcl1 , both of which are implicated in chemotherapy resistance.15 , 16 the expression of permeability glycoprotein ( p - glycoprotein ; abcb1 ) , a drugefux transporter that mediates taxane and anthracycline resistance in vitro , also increased during treatment.17 we observed a measurable increase in intratumor ammatory response by the end of the treatment ( data supplement ) , but unfortunately this did not translate into clinical antitumor activity . 
tgf activation in cancers has been linked to primary chemotherapy resistance and also to immune evasion and resistance to pd - l1 blockade in multiple experimental systems.18 - 21 furthermore , r175h p53 mutation that this cancer harbored has been shown to render cancers insensitive to the growth inhibitory effects of tgf.22 on the basis of these ndings , we hypothesize that the high expression of tgfb2 by this tumor may have contributed to its immune escape and its resistance to chemotherapy . 
another notable feature of this cancer was the low level of expression of programmed cell death protein 1 ( pd1 ) at the time of diagnosis and the high level of expression of hla - g . 
categories in which our patients score is above the 97.5th percentile ( red dots ) or below the 2.5th percentile ( teal dots ) are highlighted , are shown as bold numbers , and are described in the legend key . 
finally , genes for which our patient had expression values below the 2.5th ( panel c , teal squares ) or above the 97.5th ( panel d , red squares ) bootstrap distribution percentiles are shown . 
legend boxes and bold numbers show categories for which we observed an increase or decrease of 0.5 log2 fold change between either baseline and 8 weeks ( rst period ) and / or 8 weeks and mastectomy ( second period )  . 
 ( b ) tumor immune dysfunction and exclusion ( tide ) - based ( data supplement ) t - cell dysfunction and exclusion shown together with correlation coefcients of the gene expression values for our patient with cancer - associated broblast ( caf ) , myeloid - derived suppressor cell ( mdsc ) , and m2 tumor - associated macrophages ( tam m2 ) signatures . 
 ( c ) variant allele frequency ( vaf ) plot ( left ) and shplot ( right ) illustrating the clonal architecture and evolution ( based on sciclone [ waltham , ma ] and clonevol tools ; data supplement ) of the tumor between baseline and mastectomy time points . 
ifng , interferon gamma signature ; math , mutant allele tumor heterogeneity ; til , tumor - inltrating lymphocyte ; tlr , toll - like receptor . contributed to the poor outcome . 
however , the ndings pose at least one testable therapeutic hypothesis : tgf - targeting therapies ( eg , galunisertib , m7824 , tew7197 , ly - 3200882 , fresolimumab , and nis793 ) may have improved the efcacy of pd - l1 blockade in this particular individual . in summary , this case demonstrates the complexity of chemotherapy and immunotherapy resistance mechanisms and suggests that multiple different biologic processes may contribute to disease progression during treatment . we nd it reassuring that previously published icb response signatures predicted low sensitivity to pd1 / pd - l1 blockade for this patient . 
for more information about asco 's conict of interest lajos pusztai honoraria : merck , astrazeneca / medimmune , pzer , syndax pharmaceuticals , almac diagnostics , pieris pharmaceuticals , genentech , immunomedics , eisai , seattle genetics / astellas pharma , biotheranostics consulting or advisory role : h3 biomedicine , merck , novartis , pieriandx , seattle genetics , syndax pharmaceuticals , athenex research funding : merck , genentech , seattle genetics , astrazeneca no other potential conicts of interest were reported . acknowledgment we thank erika esteve , md , for her invaluable support throughout the study period ; xavier monzonis , md , and santiago balseiro , md , for their insightful suggestions ; tao qing and michal marczyk for their frequent inputs regarding methodologic and technical aspects of the manuscript ; and jeremia walah ( developer of structural variation and indel analysis by assembly ) and peng jiang ( developer of tumor immune dysfunction and exclusion score ) for their feedback regarding the use and interpretation of their tools . references pusztai l , hofstatter ew , chung gg , et al : durvalumab ( medi4736 ) concurrent with nab - paclitaxel and dose dense doxorubicin cyclophosphamide ( ddac ) as neoadjuvant therapy for triple negative breast cancer ( tnbc )  . 
j clin oncol 36 , 2018 ( suppl ; abstr 586 ) loibl s , untch m , burchardi n , et al : randomized phase ii neoadjuvant study ( geparnuevo ) to investigate the addition of durvalumab to a taxane - anthracycline containing chemotherapy in triple negative breast cancer ( tnbc )  . 
nanda r , liu mc , yau c , et al : pembrolizumab plus standard neoadjuvant therapy for high - risk breast cancer ( bc ) : results from i - spy 2 . 
j clin oncol 35 , 2017 ( suppl ; abstr 506 ) schmid p , adams s , rugo hs , et al : atezolizumab and nab - paclitaxel in advanced triple - negative breast cancer . 
n engl j med 379 : 2108 - 2121 , 2018 ferrara r , mezquita l , texier m , et al : hyperprogressive disease in patients with advanced non - small cell lung cancer treated with pd - 1 / pd - l1 inhibitors or with single - agent chemotherapy . 
ann oncol 29 : 2232 - 2239 , 2018 shi w , jiang t , nuciforo p , et al : pathway level alterations rather than mutations in single genes predict response to her2 - targeted therapies in the neo - altto trial . 
ann oncol 28 : 128 - 135 , 2017 ayers m , lunceford j , nebozhyn m , et al : ifn - - related mrna prole predicts clinical response to pd - 1 blockade . 
j clin invest 127 : 2930 - 2940 , 2017 fehrenbacher l , spira a , ballinger m , et al : atezolizumab versus docetaxel for patients with previously treated non - small - cell lung cancer ( poplar ) : a multicentre , open - label , phase 2 randomised controlled trial . 
lancet 387 : 1837 - 1846 , 2016 jiang p , gu s , pan d , et al : signatures of t cell dysfunction and exclusion predict cancer immunotherapy response . 
ann oncol 28 : 3076 - 3082 , 2017 imamura t , takase m , nishihara a , et al : smad6 inhibits signalling by the tgf - beta superfamily . 
lee k , giltnane jm , balko jm , et al : myc and mcl1 cooperatively promote chemotherapy - resistant breast cancer stem cells via regulation of mitochondrial oxidative phosphorylation . 
when the efcacy of a new therapy may be limited to a biomarker - dened subgroup , the choice of an appropriate randomized clinical trial design should be guided by the strength of the biomarkers credentials . 
if there is strong evidence that the treatment is likely to be more benecial in the biomarker - positive patients but a meaningful benet is also possible in the biomarker - negative patients , then a properly powered biomarker - stratied design ( eg , a subgroup - specic or marker sequential test strategy ) would provide the most rigorous determination of the sensitive populations . 
if the evidence supporting the predictive value of the biomarker is weak and the treatment is expected to work in the overall population , then a fallback design could be used . 
2019 by american society of clinical oncology introduction as a result of advances in biotechnology and improved understanding of cancer biology , therapeutic development in oncology has largely shifted from a focus on cytotoxic agents toward novel molecularly targeted and immune anticancer therapies . 
efcient development of these new anticancer drugs requires identication of predictive biomarkers that can reliably differentiate the patient population into a subgroup that benets from the therapy versus the remaining population , in whom the benet - to - risk ratio is not sufcient for the therapy to be recommended . 
in such settings , the traditional broad - eligibility randomized clinical trial ( rct ) that focuses on assessing the overall treatment effect in the entire study population may be suboptimal because this strategy may miss effective agents or result in recommending therapy to patients who do not benet from it . 
design efciency considerations are particularly important in rare population settings that require balancing feasibility and evidential requirements . relevance this article provides a practical guide for designing a biomarker - based phase iii rct . 
careful selection of an appropriate phase iii design strategy that integrates evaluation of a new anticancer therapy and its companion diagnostic can ensure proper use of resources and enhance the scientic rigor of trials in the era of precision oncology . probability of incorrectly recommending an ineffective therapy ; the power , which is the probability of correctly recommending an effective therapy ; and the target treatment effect , which is the treatment effect that the study has a desired power to identify . 
for a desired target treatment effect , the rct sample size will depend on the design type i error and power ; a smaller type i error and / or higher power require more precision in estimating the treatment effect and thus larger sample sizes . 
most phase iii trials in oncology use time - to - event end points ( eg , progression - free survival or overall survival [ os ] ) , with the target treatment effect expressed in terms of the hazard ratio ( hr )  . 
with a time - to - event end point , the precision of the hr estimate is a function of the number of observed events ; thus , the sample size will also depend on the event rates , accrual rates , and length of follow - up . biomarker with very strong credentials when there is sufciently strong evidence that the treatis limited to a specic biomarker - dened ment effect subgroup ( eg , biomarker - positive patients ) , then the socalled enrichment design is often used ( fig 1a )  . 
thus , the enrichment design avoids treating patients with an experimental therapy that is not expected to work for them . the sample size calculation for enrichment designs is the same as for traditional ( untargeted ) rcts that do not involve biomarkers . 
however , to identify biomarker - positive patients , an enrichment design must either include its own screening component or depend on outside screening ( eg , from next - generation sequencing )  . 
note that when biomarker positivity is low in the patient population , many patients will need to be screened to identify the number of biomarker - positive patients necessary to complete the study . 
for example , the brim3 trial ( clinicaltrials.gov identier : nct01006980 ) , 5 which evaluated a braf inhibitor vemurafenib in patients with brafv600e - mutated melanoma , had to screen 2 , 107 patients with melanoma to enroll 675 patients with the braf mutation . 
when the biomarker is indeed predictive in identifying patients who benet from the therapy , an enrichment design is quite efcient because it can dramatically reduce the number of randomly assigned patients required ( by focusing the trial on a population with an undiluted treatment effect ) .6 despite its advantages , the enrichment design has some limitations . 
if the targeted therapy indeed benets all patients regardless of biomarker status , then restricting the trial population to only biomarker - positive patients slows trial accrual and limits the patient population that can ultimately be helped by the therapy . biomarker with strong credentials at the time a denitive trial is being designed , there is often sufcient evidence to assume that the targeted therapy is more likely to benet biomarker - positive patients than the biomarker - negative patients , but a potential treatment benet in biomarker - negative patients cannot be ruled out . in this case , a design that randomly assigns patients to the experimental and control treatments within biomarkerdened subgroups , the so - called biomarker - stratied design , would be the most appropriate approach for a combined assessment of the therapy and the companion biomarker . 
a biomarker - stratied trial could provide sufciently reliable information on the distribution of the riskbenet ratio of the new therapy across biomarker subgroups to inform treatment efcacy and the need for the biomarker to guide treatment use . biomarker - positive and biomarker - negative ( subgroup - specic ) strategy . 
m , marker ; m + , marker positive ; m , marker negative ; rx , treatment ; sig , signicant . the biomarker - positive and biomarker - negative patient subgroups . 
ideally , this subgroup - specic strategy should be powered to detect clinically relevant treatment effects in each subgroup , albeit in practice , the biomarker - positive subgroup is often prioritized . 
because the biomarker - positive patients are typically expected to derive more benet from the targeted therapy than the biomarker - negative patients , the design could assume a larger treatment effect for the former . because the design involves testing of two subpopulations , the overall study - wise probability of recommending an ineffective therapy to any subpopulation ( overall type i error or overall signicance level of the design ) is inated if no the multiple testing is made . 
in a well - established approach , one allocates the overall between the biomarker - positive and biomarker - negative tests , as follows : signicance level 1 ( 1 ) to testing the biomarker - positive subgroup and signicance level 2 , calculated as 1 , to testing the biomarker - negative subgroup . 
then , one can use recycling techniques to optimize the design by specifying the sequence in which the subgroups are tested , with the level from an earlier signicance test redistributed to the subsequent test.7 - 9 for example , one can rst test the biomarker - positive subgroup at signicance level 1 . 
if that test is signicant , then 1 is redistributed to testing the biomarker - negative subgroup , resulting in an = 2 + 1 signicance level available for testing the biomarkernegative subgroup ; if the test of the biomarker - positive subgroup is not signicant , then an 2 signicance level is used for the biomarker - negative test ( fig 1b )  . 
this provides considerable exibility for adjusting the design to a particular setting ; at one extreme , one can allocate only half of the overall to the initial testing of the biomarkerpositive subgroup ( 1 = / 2 )  . 
more typically , a sequential subgroup - specic approach allocates the entire signicance level to rst test the biomarker - positive subgroup . this is appropriate because one believes it is unlikely that the treatment works in the biomarker - negative subgroup unless it also works in the biomarker - positive subgroup . 
if the biomarker - positive test is signicant , then is redistributed to testing the biomarker - negative subgroup ; if the biomarker - positive test is negative , all testing is stopped ( fig 1c )  . 
the trial was designed to rst test the kras wild - type subgroup at the 1 = .025 signicance level , with testing of the kras - mutated subgroup ( at the 2 = .025 signicance level ) conditional on observing a signicant result in the kras wild - type subgroup . biomarker - positive and overall strategy . 
to account for testing of the two populations , the biomarker - positive / overall designs use multiple testing procedures similar to those used in the subgroup - specic designs . 
other biomarker - positive / overall designs are implemented in a fully sequential manner , rst testing the biomarkerpositive population at the signicance level , and then , if signicant , the overall population at the signicance level . 
note that some trials apply this design in the reverse order ; they rst test the overall population , and only if this test is signicant do they then test the biomarker - positive population.14 requiring a signicant result in the overall population to test the biomarker - positive subgroup is not logical and can result in failing to detect benet limited to the biomarker - positive population . 
for example , the impassion130 trial ( clinicaltrials.gov identier : nct02425891 ) , which tested the addition of atezolizumab to chemotherapy in metastatic breast cancer , was not able to formally test os in the pd - l1positive population because the test in the overall population was not signicant.14 implementation , a major regardless of the particular concern with the biomarker - positive / overall testing approach is that when the benet of the treatment is limited to the biomarker - positive patients , the design may inappropriately recommend the treatment to the biomarkernegative subgroup.8 , 15 , 16 this is because a statistically signicant result in the overall population may be driven by a large treatment effect in the biomarker - positive patients even with no effect in the biomarker - negative subgroup . treatment efcacy is from the clinical perspective , demonstrated in the biomarker - positive patients , then the only relevant question is whether the treatment works in the biomarker - negative patients . 
a potential concern with the subgroup - specic testing strategy is that it has lower power for therapies with moderate treatment effects that are similar across the biomarker subgroups , relative to the designs based on testing the overall population . 
 ( indeed , this is often used to justify the biomarker - positive / overall strategy . ) this concern is addressed by the marker sequential test ( mast ) design17 ( fig 1e ) , which incorporates sequential tests of the treatment effect in the biomarkerpositive subgroup , biomarker - negative subgroup , and overall population ( while controlling the probability of recommending an ineffective therapy to either biomarkerpositive or biomarker - negative patients at signicance level )  . 
for example , a phase iii study of blinatumomab ( ecog e1910 ; clinicaltrials.gov identier : nct02003222 ) in acute lymphoblastic leukemia evaluated minimum residual disease as a predictive biomarker for blinatumomab15 using the mast design . the mast design requires a slightly larger sample size ( approximately 4% ) than the sequential subgroup - specic design ( because the biomarker - positive subgroup is tested at the reduced signicance level 1 )  . 
at the same time , it has considerably higher power in situations where the treatment effect is homogeneous across the biomarker subgroups.17 biomarker with weak credentials the treatment effect when the treatment is expected to be broadly effective ( ie , reliable evidence for predictive value of the biomarker is lacking ) , the most appropriate strategy would be a design that enrolls all patients regardless of their biomarker status and focuses on the treatment effect in the overall population . 
however , it is still possible to incorporate a prospectively specied , statistically rigorous contingency plan to accommodate evaluation of a biomarker - dened subgroup if the test in the overall population is negative.11 this is known as a fallback design . in a fallback design , the treatment effect is rst tested in the overall population using a slightly reduced signicance level of 1 . 
if the results are positive , then the treatment is recommended for the overall population ; if the results are negative , then the test of treatment effect is performed in the biomarker - positive subgroup at a signicance level of ( 1 ) ( fig 1f )  . 
because of the relatively small reduction in the signicance level for the overall population test , the fallback design results only in a marginal ination of sample size compared with a traditional rct that uses the entire signicance level on the overall test.11 statistically speaking , the fallback approach is identical to the biomarkerpositive / overall strategy ( described earlier ) , and thus , it does not control for the probability of incorrectly recommending treatment to biomarker - negative patients when they do not benet from it . 
therefore , use of this design should be limited to settings where the treatment is expected to be widely benecial and the biomarker prevalence is low ( , 20% )  . 
when the prevalence is low , overall results are unlikely to be driven by the biomarker - positive effect , and conducting a subgroup - specic design may be infeasible . 
even when the use of the fallback design is considered justied , one should always include estimation of the treatment effect in the biomarker - negative patients as a secondary goal . unlike the designs described earlier , the fallback design is initially focused on testing the overall population , so there is no need to know patient biomarker status up front . 
however , in some situations , it may be difcult to ascertain the biomarker status before randomization ( eg , when the biomarker assay turnaround time is not short )  . 
theoretically , one can still use the biomarkerstratied approaches described earlier by allowing biomarker assessment to be performed after randomization ; this is sometimes known as the all - comers approach . 
however , because some patients may not have their biomarker status determined ( eg , due to missing or tumor specimen or assay failure ) , for the subgroup - specic designs , the primary analysis is limited to patients with determined status ( for the mast and the biomarker - positive / overall designs , all patients can be used in the overall test )  . if the biomarker assessments are done without knowledge of the randomized treatment assignment and outcome , this approach provides an unbiased evaluation of the biomarker . 
unfortunately , use of the all - comers approach is generally not practical for biomarkers with strong credenthese designs prospectively specify intials : some of dependent sample size goals for the biomarker - positive and biomarker - negative subgroups , and most others include interim monitoring that may at some point restrict accrual to one of the subgroups ( see interim monitoring )  . 
an advantage of obtaining the biomarker assessment up front is that only patients used in the analyses will be enrolled . furthermore , in some settings , the requirement of having a biomarker assessment to enter the study may encourage more rigorous specimen handling and thus improve the biomarker ascertainment success rate . 
suppose one is evaluating a new treatment in a setting where the median os with the current standard of care is 12 months ( in both biomarker subgroups ) and the expected accrual rate is 30 patients per month . 
for each biomarker subgroup , the table lists the probability of recommending the new therapy for that subgroup along with sample sizes , accrual durations , and for practical reasons , biofollow - up periods ( note that marker trials are usually designed to have accrual open to both groups , with the overall sample size dened by the sample size required for the biomarker - positive subgroup )  . the rst step in the design is to determine the number of biomarker - positive patients needed to detect the target treatment effect for that subgroup . 
in the current setting , for biomarkers with 50% , 25% , and 10% prevalence , one needs to enroll 300 , 240 , and 150 patients , respectively , to have acceptable power for an hr of 0.6. 
implementation of the biomarker designs for a range of biomarker prevalences biomarker positive biomarker negative design power ( % ; probability recommending for the subgroup ) sample size , no . accrual + follow - up time ( months ) power ( % ; probability recommending for the subgroup ) sample size , no . accrual + follow - up time ( months ) 50% biomarker prevalence ; target effects : biomarker - positive hr , 0.6 ; biomarker - negative hr , 0.7 25% biomarker prevalence ; target effects : biomarker - positive hr , 0.6 ; biomarker - negative hr , 0.75 enrichment design subgroup specic with recycling : 50% / 50% split sequential subgroup specic mast design biomarker positive and overall : 50% / 50% split enrichment design subgroup specic with recycling : 76% / 24% split sequential subgroup specic mast design biomarker positive and overall : 76% / 24% split enrichment design subgroup specic with recycling : 80% / 20% split sequential subgroup specic mast design fallback : 80% ( overall ) / 20% ( biomarker positive ) split 20 + 9 20 + 14 20 + 9 20 + 10 20 + 14 32 + 12 32 + 16 32 + 12 32 + 14 32 + 16 50 + 18 50 + 26 50 + 18 50 + 22 20 + 9 10% biomarker prevalence ; target effects : biomarker - positive hr , 0.6 ; biomarker - negative hr , 0.75 1350 1350 1350 20 + 40 20 + 40 20 + 40 20 + 14 32 + 16 32 + 11 32 + 14 32 + 16 50 + 9 50 + 9 50 + 9 20 + 20 note . 
when biomarker - positive prevalence is relatively high ( close to 50% ) , additional ( longer ) follow - up will be required on the biomarker - negative patients to achieve acceptable power for detecting the desired target effect . conversely , when the biomarker prevalence is low , additional ( longer ) follow - up may be required for the data to mature in the biomarker - positive subgroup . for the mast , biomarker - positive / overall , and fallback designs in table 1 , the probabilities of recommending therapy for a given subgroup include recommendations that are based on both the subgroup - specic and the overall tests . 
one can see in table 1 that for the biomarkers in the 25% to 50% range , mast , biomarker - positive / overall , and subgroup - specic with recycling designs provide the best power in the situations where treatment is benecial in both subgroups . 
however , it is important to remember that , unlike the biomarker - positive / overall design , the mast approach is explicitly designed to control for the probability of an incorrect treatment recommendation for biomarker - negative patients . 
one can see that although the mast design controls the probability of recommending ineffective therapy to biomarker - negative patients at 2.5% , this probability could be high for the biomarker - positive / overall design ( eg , 69% and 40% in 50% and 25% prevalence cases , respectively )  . 
for example , in the clinical settings considered in table 1 , if the biomarker prevalence is 10% , then it takes 50 months to enroll 150 biomarker - positive patients ( 1 , 500 patient total ) to have 80% power for an hr of 0.6 ( after an additional 18 months of follow - up )  . 
in rare biomarker settings where the biomarker credentials are weak ( ie , the treatment is expected to have broad benet ) , one can use the fallback design ( eg , with 10% prevalence , a 600 - patient fallback design would have 82% power when there is some effect in both biomarker subgroups ; table 1 )  . 
note that in this rare biomarker setting , when the treatment effect is limited to the biomarker - positive patients , the probability of the fallback design incorrectly recommending ineffective therapy to the biomarker - negative patients is low ( 5% ; table 2 )  . 
in this case , one would need to design the study so that enrollment of biomarkernegative patients can be stopped ( after the required number of these patients are enrolled ) , with only biomarkerpositive enrollment allowed thereafter . 
similarly , if the biomarker prevalence is greater than 50% , then one may have to continue accrual to the biomarker - negative subgroup after the biomarker - positive subgroup nishes accrual . 
 phase iii precision medicine trial designs treatment is likely to be more benecial in the biomarkerpositive patients but a meaningful benet is also possible in the biomarker - negative subgroup , then a properly powered biomarker - stratied design using a subgroup - specic strategy with recycling or the mast strategy would provide the most accurate and efcient determination of the sensitive population . 
if the evidence supporting the predictive value of the biomarker is weak and the treatment is expected to work in the overall population , then a fallback design could be used . biomarker - driven randomized phase iii trials are resource intensive and often take a long time to complete . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . no potential conicts of interest were reported . references sargent dj , conley ba , allegra c , et al : clinical trial designs for predictive marker validation in cancer treatment trials . 
clin cancer res 14 : 4358 - 4367 , 2008 chapman pb , hauschild a , robert c , et al : improved survival with vemurafenib in melanoma with braf v600e mutation . 
stat med 24 : 329 - 339 , 2005 bretz f , maurer w , brannath w , et al : a graphical approach to sequentially rejective multiple test procedures . 
douillard jy , siena s , cassidy j , et al : randomized , phase iii trial of panitumumab with infusional uorouracil , leucovorin , and oxaliplatin ( folfox4 ) versus folfox4 alone as rst - line treatment in patients with previously untreated metastatic colorectal cancer : the prime study . 
rittmeyer a , barlesi f , waterkamp d , et al : atezolizumab versus docetaxel in patients with previously treated non - small - cell lung cancer ( oak ) : a phase 3 , open - label , multicentre randomised controlled trial . 
powles t , dur an i , van der heijden ms , et al : atezolizumab versus chemotherapy in patients with platinum - treated locally advanced or metastatic urothelial carcinoma ( imvigor211 ) : a multicentre , open - label , phase 3 randomised controlled trial . 
clin trials 11 : 19 - 27 , 2014 jiang w , freidlin b , simon r : biomarker - adaptive threshold design : a procedure for evaluating treatment with possible biomarker - dened subset effect . 
dreno b , thompson jf , smithers bm , et al : mage - a3 immunotherapeutic as adjuvant therapy for patients with resected , mage - a3 - positive , stage iii melanoma ( derma ) : a double - blind , randomised , placebo - controlled , phase 3 trial . 
genomic profiling was performed on 703 appendiceal cancer specimens to compare the mutation profiles of appendiceal subtypes to crc and other cancers , with the ultimate aim to identify potential biomarkers and novel therapeutic targets . methods tumor specimens were submitted to a clinical laboratory improvement amendmentscertified laboratory ( foundation medicine , cambridge , ma ) for hybrid - capturebased sequencing of 3 , 769 exons from 315 cancer - related genes and 47 introns of 28 genes commonly rearranged in cancer . 
kras ( 35% to 81% ) and gnas ( 8% to 72% ) were the most frequent alterations in epithelial cancers ; apc and tp53 mutations were significantly less frequent in appendiceal cancers relative to crc . 
the mutation status of gnas and tp53 strongly predicted os ( median , 37.1 months for tp53 mutant v 75.8 gnas - tp53 wild type v 115.5 gnas mutant ; log - rank p = .0031 ) and performed as well as grade in risk stratifying patients . conclusion epithelial appendiceal cancers and goblet cell carcinoids show differences in kras and gnas mutation frequencies and have mutation profiles distinct from crc . 
2018 by american society of clinical oncology introduction the rarity of appendiceal neoplasms has made it difficult to conduct prospective or randomized clinical trials to guide therapy for these tumors . 
 the small number of appendiceal tumors that are detected , in many cases as an incidental finding in < 1% of appendectomy specimens , 1 comprise multiple histopathologic subtypes , including noninvasive mucinous neoplasms , mucinous and nonmucinous adenocarcinomas , carcinoids , goblet cell carcinoids ( gccs , now also called goblet cell tumors ) , and signet ring cell carcinomas.2 early - stage cancers can be treated definitively with surgery , and selected patients derive long - term benefit from cytoreductive surgery and heated intraperitoneal chemotherapy ( hipec ) .3 however , there is no standard of care for the systemic treatment of advanced , unresectable disease . in the absence of randomized phase iii data , the majority of medical oncologists use colorectal cancer ( crc ) chemotherapy regimens for the treatment of unresectable epithelial appendiceal neoplasms , as is currently recommended by the national comprehensive cancer network guidelines . 
clinical and demographic patient characteristics by subtype median age ( years ) sex ratio m : f subtype mucinous adenocarcinoma adenocarcinoma goblet cell carcinoid pseudomyxoma peritonei signet ring carcinoma 43 : 57 42 : 58 36 : 64 46 : 54 49 : 51 mutation analysis revealed kras to be the most frequently mutated gene in mad ( 77% ) , ad ( 56% ) , and pmp ( 81% ) and the second most frequently mutated gene in srcc ( 35% )  . 
in contrast , kras mutations were significantly less frequent in gccs ( 13% ; 2 p < .001 ) , where tp53 ( 33% ) was the most frequently mutated gene ( fig 1b ; appendix fig a1a )  . 
braf , brca1 , cdkn1b , cdkn2a , myc , pten , and tgfbr2 mutations were present in < 10% of cases across all subtypes ( table 2 )  . 
gnas and kras were the only gene pair significantly comutated ( odds ratio , 6.8 ; bonferroni corrected p = 8.6x10 - 17 ) ; gnas and tp53 were the only gene pair significantly mutually exclusive ( odds ratio , 0.20 ; bonferroni corrected p = 6.7x10 - 13 ; fig 1c ; data supplement )  . pathway - based analysis of mutation profiles genetic aberrations were subsequently grouped by signaling pathway ( appendix table a1 )  . 
 components of the ras / raf signaling pathway ( ie , braf , hras , kras , and nras ) were the most frequently altered genes in epithelial appendix cancers , occurring in > 80% of mads and pmps , 60% of ads , but only 33% of gccs ( 2 p < .001 ; fig 1d )  . 
alterations in homologous recombination deficiency genes were observed in > 50% of all subtypes but were most prevalent in srcc ( 80% ) fluorouracil , leucovorin , and oxaliplatin ; fluorouracil , leucovorin , and irinotecan ; and targeted agents in appendiceal adenocarcinomas compared with crc , 8 , 9 it is known that appendiceal neoplasms have a better prognosis after cytoreductive surgery with hipec treatment.10 there is also a growing body of data showing that there are clear molecular differences between appendiceal and colorectal cancers.11 - 14 here we present a cohort of 703 molecularly profiled appendiceal neoplasms , the largest such cohort to date in this rare disease . 
comparing the mutational landscapes across histologic subtypes we find significant differences in kras , gnas , and fat3 mutation prevalence and confirm that mutational profiles of appendiceal neoplasms are distinct from crc and other gi cancers . 
 in addition , we identify that patients can be risk stratified using the combined mutation status of gnas and tp53 and that outcomes are favorable for patients with kras wild - type disease when treated with irinotecan . results mutation landscape of appendiceal neoplasms the 703 cases were categorized into four different histopathological subtypes consistent with the recently updated consensus classification from the peritoneal surface oncology group international ; in addition , cases of pseudomyxoma peritonei ( pmp ) were included , because this syndrome usually arises from the appendix.2 the majority were either mucinous adenocarcinomas ( mad , 46% ) or adenocarcinomas ( ad , 30% ) , with the rest being gccs ( 12% ) , pmps ( 7.7% ) , or signet ring cell carcinoma ( srcc , 5.3% ; appendix ; table 1 )  . 
the majority of specimens submitted for sequencing came from intraperitoneal metastatic deposits , although there were also primary appendiceal tumors and a small number of lung , liver , and bone metastases ( fig 1a )  . 
data presented as % frequency . abbreviations : ad , adenocarcinoma ; crc , colorectal cancer ; gcc , goblet cell carcinoid ; mad , mucinous adenocarcinoma ; msi - h , microsatellite instability - high ; pdac , pancreatic ductal adenocarcinoma ; pmp , pseudomyxoma peritonei . comparison of genomic aberrations in appendix , colorectal , and pancreas cancers given the clinical practice of treating metastatic appendiceal cancers with crc regimens , we compared genomic alteration profiles of the appendiceal subtypes with those of 10 , 000 crcs profiled by the same laboratory ( table 2 )  . 
the high frequency of kras mutations observed in multiple appendiceal subtypes prompted inquiry into possible parallels with ( pdac ) , pancreatic ductal adenocarcinoma which harbors kras mutations in up to 95% of cases.16 sequencing of 2 , 800 pancreatic tumors revealed kras mutations in 87% of pdacs . 
there tended to be a higher frequency of microsatellite unstable or tumor mutational burdenhigh srccs and ads compared with mads ( table 2 ; appendix fig a1e )  . histopathologic and molecular features predictive of survival to determine the influence of histologic and molecular features on clinical outcomes , a retrospective review of a single - institution case series was performed . 
similar to the full 703 - patient cohort , the majority of cases were either ads ( n = 17 ) or mads ( n = 33 ) , with fewer low - grade appendiceal mucinous neoplasms that manifested as pmps ( n = 13 ) and few srccs ( n = 9 )  . 
data for chemotherapy treatment were available for 60 patients , showing that the majority were treated with a fluoropyrimidine and either oxaliplatin or irinotecan ( appendix ; table 3 )  . overall survival ( os ) , determined from time of initial diagnosis , was similar for ad and mad ( logrank p = .29 ; appendix fig a2a ) , so these groups were combined in subsequent analyses . 
 ( % ) unless otherwise noted . abbreviations : egfr , epidermal growth factor receptor ; hipec , heated intraperitoneal chemotherapy ; lamn , low - grade appendiceal mucinous neoplasms ; pd1 , programmed cell death protein 1 ; pd - l1 , programmed death ligand 1 ; pmp , pseudomyxoma peritonei ; sd , standard deviation ; vegf , vascular endothelial growth factor . for srccs ( p = .11 ; fig 2a )  . 
 however , use of irinotecan in any line of therapy was associated with a survival advantage in kras wild - type tumors ( log - rank p = .041 ; fig 2f ) but not in kras mutant tumors ( log - rank p = .32 ; appendix fig a2b )  . 
low - grade tumors were enriched for gnas mutations ( 72% v 18% for high grade ; 2 p < .001 ; appendix fig a3a ) , consistent with our prior report , 14 whereas highgrade tumors were enriched for tp53 mutations ( 56% v 6.9% for low grade ; 2 p < .001 ; appendix fig a3b )  . to assess the relative contributions of mutation and grade to the observed os differences , a cox proportional hazard analysis was performed including age , sex , kras , gnas , tp53 , and grade as covariates . 
however , the effect of tp53 mutation on survival was independent of grade , with the rare low - grade , tp53 - mutant tumors having os similar to other tp53 - mutant tumors ( median , 24.6 months ; fig 3b )  . 
at risk : irinotecan 8 no irinotecan 15 time ( months ) the mutational profile of 703 appendix neoplasms provides insight into the molecular aberrations that differentiate histologic subtypes and identifies putative prognostic and predictive biomarkers that may help guide treatment in this rare malignancy . 
compared with ad , mad , and pmp , kras and gnas mutations were much less frequent in gccs , whereas mutations in fat3 and arid1a were more frequent ( figs 1b and 1c )  . 
 these differences were also seen in the pathway analysis , in which gccs had less - frequent alterations of the ras / raf pathway relative to epithelial appendiceal cancers ( fig 1d )  . 
at risk : gnas mut 28 tp53 mut 25 neither 18 high - gnas mutant moderate - gnas mutant p = .011 low - gnas mutant time ( months ) no . 
these data also show that all of the appendiceal subtypes are molecularly distinct from crc , with more frequent gnas mutation and significantly lower prevalence of apc and tp53 mutations , which are key pathogenic alterations in crc . 
 the mutation profiles of ad and srcc bore the most resemblance to crc , with ad and crc sharing similar frequencies of mutation in kras , smad4 , and arid1a ; of note , appendiceal ads have been referred to as colonic - type adenocarcinoma , given clinical behavior more similar to crc.20 , 27 in this series , srcc had the worst prognosis of the epithelial appendiceal tumors and also has a clinical course similar to crc.28 the frequent comutation of kras and gnas in mad , ad , and pmp parallels the molecular profile of intraductal papillary mucinous neoplasms.14 , 29 notably , both intraductal papillary mucinous neoplasms and , in particular , gnas mutant appendiceal cancers are characterized by mucin production and a generally indolent clinical course . 
the differences in mutation profiles between the epithelial appendiceal tumors can be at least partially explained by grade , with significant association of gnas mutation with low - grade tumors and tp53 mutation with highgrade tumors ( appendix figs a3a and a3b )  . 
 consistent with this is the higher incidence of tp53 mutation and lower incidence of gnas mutation in srccs , which are by definition all high grade . histologic grade was also a strong predictor of survival ( fig 2b ) , consistent with prior reports.17 , 30 we did not observe a significant difference in os between ad and mad ; however , the distribution of tumor grade was similar between these two subtypes in our study . 
 conversely , tp53 mutation was an independent predictor of poor survival , with low - grade , tp53 - mutant tumors having survival similar to that of high - grade tumors . 
in addition , because appendiceal tumors are so rare , they are difficult to diagnose pathologically and are frequently overinterpreted by community pathologists.31 although gnas mutation is not an independent predictor of survival , because gnas and tp53 mutations occur mutually exclusive of each other and are associated with lowand high - grade tumors , respectively , the two genes can be substituted for grade to predict survival . 
the survival stratification achieved with the gnas - tp53 biomarker is similar to grade , an important observation , given that it is now much easier to obtain a mutation profile than an expert pathology review in the community oncology setting . the absence of a gnas mutation in the majority of high - grade tumors and the mutual exclusivity of tp53 and gnas mutations both strongly suggest that most high - grade appendiceal tumors occur de novo , rather than progressing from low - grade tumors , confirming , on a larger scale , our previous observations.14 however , there were a minority of tumors with both tp53 and gnas mutation ( n = 41 ; 6.7% ) , suggesting that transformation from low grade to high grade can occur . 
serial biopsy or serial measurement of circulating tumor dna would be needed to confirm that these tp53 mutations did in fact occur after the formation of a low - grade , gnas mutant tumor . 
however , given the low propensity for appendiceal tumors to spread beyond the abdominal cavity , there may be limited tumor dna in circulation , potentially making bloodbased tumor detection difficult . 
indeed , three of the four university of california , san diego , patients who underwent circulating tumor dna sequencing had no reportable alterations . regarding predictive biomarkers , kras wildtype status was associated with better survival in the subset of patients treated with irinotecan . 
a retrospective study in metastatic crc reported better response to irinotecan in patients with wild - type versus mutant plasma kras.32 however , a larger prospective study found that mutant kras was associated with poor survival but not with response to irinotecan in crc.33 regarding targeted therapies , there are unfortunately few clinically actionable mutations in appendiceal cancers , although the ras / raf signaling pathway is frequently altered in epithelial appendiceal cancers . 
data on therapeutic targeting of the ras / raf cascade in appendiceal tumors are limited , although a recent case report described clinical benefit in a patient with appendiceal mad harboring a gnas r201h mutation who was treated with trametinib.34 because only eight patients in this cohort received an anti - egfr antibody , we were unable to assess interactions between kras mutation status and response to these agents . a major limitation of this study is its retrospective design . 
with regard to the 703 - patient cohort , clinical information such as precise tnm stage was not available , but the fact that > 80% of specimens submitted came from metastases indicates that the majority of patients had stage iv disease . 
although specimens were independently reviewed by pathologists to confirm the diagnosis before undergoing sequencing , subtype definitions are potentially subject to variability and overlap , because there was no consensus classification system for appendiceal neoplasms and pmp until recently.2 for example , pmp is an inherently imprecise term used to describe the clinical syndrome of mucinous peritoneal dissemination from an appendiceal neoplas pmp encompasses a spectrum of both highand low - grade lesions but does not reference the histopathologic characteristics of the appendiceal primary from which it arises . 
 newer classification schemes separate pmps with low - grade and high - grade features ( also known as disseminated peritoneal adenomucinosis and peritoneal mucinous carcinomatosis , respectively35 ) and pmp with signet ring cells.2 because this study did not distinguish between these subtypes , we are unable to report on genomic differences associated with grade in the larger 70 - patient cohort . 
in addition , analysis of interactions between genotype and specific drugs are confounded by the fact that most patients received multiple lines of therapy . this study of unprecedented size in this rare disease highlights important molecular differences between different subtypes of appendix cancer and identifies gnas and tp53 mutation status as a prognostic biomarker . 
this comprehensive portrait of the molecular landscape of appendix cancer will help with the design of future clinical studies to develop and test therapeutic strategies specific to this disease . in conclusion , appendiceal neoplasms have molecular profiles that are distinct from crc and are characterized by frequent gnas and kras mutations , especially in low - grade tumors . 
ross employment : foundation medicine leadership : foundation medicine financial support : john paul shen , paul fanta , trey ideker administrative support : john paul shen , paul fanta stock and other ownership interests : foundation medicine provision of study material or patients : john paul shen , jeffrey s . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center miriam t . 
ali employment : foundation medicine leadership : incyte stock and other ownership interests : exelixis , blueprint medicines , agios pharmaceuticalas , genocea biosciences patents , royalties , other intellectual property : patents via foundation medicine and seres health joel baumgartner research funding : merck andrew lowy consulting or advisory role : halozyme , merck research funding : mitsubishi tanabe pharma , syros pharmaceuticals expert testimony : merck ascopubs.org / journal / po jco precision oncology 9 justin k . 
 paul fanta no relationship to disclose trey ideker leadership : data4cure consulting or advisory role : ideaya biosciences , genetic modifiers newco , merck , la jolla institute for allergy and immunology research funding : pfizer travel , accommodations , expenses : sage bionetworks sherri z . 
chen , david xu , joel baumgartner , andrew lowy , paul fanta , trey ideker , and olivier harismendy , university of california , san diego , la jolla , ca ; jeffrey s . 
carr nj , cecil td , mohamed f , et al : a consensus for classification and pathologic reporting of pseudomyxoma peritonei and associated appendiceal neoplasia : the results of the peritoneal surface oncology group international ( psogi ) modified delphi process . 
sugarbaker ph , bijelic l , chang d , et al : neoadjuvant folfox chemotherapy in 34 consecutive patients with mucinous peritoneal carcinomatosis of appendiceal origj surg oncol 102 : 576581 , 2010 5 . 
farquharson al , pranesh n , witham g , et al : a phase ii study evaluating the use of concurrent mitomycin c and capecitabine in patients with advanced unresectable pseudomyxoma peritonei . 
garin l , corbinais s , boucher e , et al : adenocarcinoid of the appendix vermiformis : complete and persistent remission after chemotherapy ( folfox ) of a metastatic case . 
tejani ma , ter veer a , milne d , et al : systemic therapy for advanced appendiceal adenocarcinoma : an analysis from the nccn oncology outcomes database for colorectal cancer . 
johncilla m , stachler m , misdraji j , et al : mutational landscape of goblet cell carcinoids and adenocarcinoma ex goblet cell carcinoids of the appendix is distinct from typical carcinoids and colorectal adenocarcinomas . 
borazanci e , millis sz , kimbrough j , et al : potential actionable targets in appendiceal cancer detected by immunohistochemistry , fluorescent in situ hybridization , and mutational analysis . 
alakus h , babicky ml , ghosh p , et al : genome - wide mutational landscape of mucinous carcinomatosis peritonei of appendiceal orig genome med 6 : 43 , 2014 [ erratum : genome med 6 : 53 , 2014 ] 15 . 
reid md , basturk o , shaib wl , et al : adenocarcinoma ex - goblet cell carcinoid ( appendicealtype crypt cell adenocarcinoma ) is a morphologically distinct entity with highly aggressive behavior and frequent association with peritoneal / intra - abdominal dissemination : an analysis of 77 cases . 
singhi ad , davison jm , choudry ha , et al : gnas is frequently mutated in both low - grade and high - grade disseminated appendiceal mucinous neoplasms but does not affect survival . 
mccusker me , cot tr , clegg lx , et al : primary malignant neoplasms of the appendix : a population - based study from the surveillance , epidemiology and end - results program , 19731998 . 
asare ea , compton cc , hanna nn , et al : the impact of stage , grade , and mucinous histology on the efficacy of systemic chemotherapy in adenocarcinomas of the appendix : analysis of the national cancer data base . 
 appendix tumor tissue from 703 patients with appendiceal cancer was submitted to a clinical laboratory improvement amendments certified laboratory ( foundation medicine , cambridge , ma ) for dna sequencing and variant calling . 
a minimum of 50 ng of dna was extracted and a hybrid - capture method used to capture 3 , 769 exons from 315 cancer - related genes and 47 introns of 28 genes commonly rearranged in cancer ; this material was then sequenced to high ( average , 756x ) uniform coverage allowing for evaluation of genomic alterations , including base substitutions , indels , amplifications , copy number alterations , and fusions / rearrangements . 
clinical characteristics and outcomes , including tumor histology , grade , stage , overall survival ( os ) , and chemotherapy given were determined from review of the electronic medical record . 
sequencing failed quality control in two cases , and two patients with only blood - based cell - free dna sequencing were excluded , leaving 76 patients available for analysis . 
because there were only four goblet cell carcinoids , these were removed from survival analysis . for mutual exclusivity and comutation analysis , goblet cell carcinoid tumors and microsatellite instability - high tumors were removed , and a fishers exact test was performed for all gene combinations , followed by bonferroni multiple hypothesis correction . 
 lynch syndrome and breast cancer risk : weighing the data wendy kohlmann , ms , cgc1 as we continue to expand our understanding of the genotype - phenotype correlations in lynch syndrome ( ls ) , we must be cautious in the design of studies and interpretation of ndings to responsibly serve our patients with ls with as accurate information as possible . 
although pathogenic variants ( pvs ) in the mismatch repair ( mmr ) genes mlh1 , msh2 / epcam , msh6 , and pms2 are all associated with ls , each gene is associated with a unique risk prole . 
mlh1 and msh2 have been associated with the highest risk for ls - associated cancers , whereas risk for colorectal cancer is signicantly lower for msh6 and pms2 pv carriers.1 in studies of high - risk colorectal cancer cohorts , msh6 and pms2 pvs are less commonly identied than mlh1 and msh2 , but use of clinical multigene panel testing is expanding the identication of carriers of pvs in these genes , often in individuals and families lacking the classic pattern of cancers associated with ls.2 , 3 the large data sets being generated by genetic testing laboratories can be assets for research and can allow for gene - specic risk analysis . however , analytical caution needs to be taken to account for the biases that arise from patient selection for clinical genetic testing , and family history and clinical data provided to commercial laboratories may be incorrect or inaccurate . in the article accompanying this editorial , stoll et al2 add data from a large cohort of mmr carriers and demonstrate a successful strategy for using commercial laboratory data to assess associations between pvs and cancer risk . 
however , to account for the study population having a more signicant cancer history than the general population , pv carriers were also compared with other subpopulations within the laboratory cohort , including women who were negative for a pv in any cancer predisposition gene when testing was performed for evaluation for hereditary breast or ovarian cancer ( hboc ) and / or ls , evaluation for hboc only , and evaluation for ls only . no excess in breast cancer risk was noted when compared with seer or any laboratory comparison group for any of the mmr genes . in the cohort in the study by stoll et al , 2 pvs in msh6 and pms2 were more common in women undergoing genetic testing for the indication of hboc than in women being tested as a result of suspicion of ls . other studies of clinical testing populations have also found a predominance of msh6 and pms2 pvs in individuals meeting hboc guidelines rather than ls.4 however , this pattern does not conrm that these genetic variants increased the risk for breast cancer . this distribution of pvs in laboratory cohorts likely reects that , other than msh6 - associated endometrial cancer risk , pvs in msh6 and pms2 confer only a modest risk for colorectal and other lsassociated cancers . 
stoll et al2 have provided a systematic examination of a large laboratory cohort using the proper comparison groups to put the frequency of msh6 and pms2 pvs by testing criteria into context and have provided strong evidence against the association of breast cancer with any of the mmr genes . before widespread panel testing , most analyses of breast cancer risk and ls had come from small studies.5 data from studies with larger samples are now becoming available . 
signicant breast cancer history may be a result of other factors , and genetic testing of other affected family members may be warranted to determine whether there is an additional pv segregating in the family and contributing to that cancer risk . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . wendy kohlmann employment : biofire diagnostics ( i ) no other potential conicts of interest were reported . references dominguez - valentin m , sampson jr , sepp al a tt , et al : cancer risks by gene , age , and gender in 6350 carriers of pathogenic mismatch repair variants : findings from the prospective lynch syndrome database . 
cancer epidemiol biomarkers prev 26 : 404 - 412 , 2017 espenschied cr , laduca h , li s , et al : multigene panel testing provides a new prospective on lynch syndrome . 
mller p , sepp al a tt , bernstein i , et al : cancer risk and survival in path_mmr carriers by gene and gender up to 75 years of age : a report from the prospective lynch syndrome database . 
gut 67 : 1306 - 1316 , 2018 ten broeke sw , van der klift hm , tops cmj , et al : cancer risks for pms2 - associated lynch syndrome . 
j clin oncol 36 : 2961 - 2968 , 2018 slavin tp , maxwell kn , lilyquist j , et al : the contribution of pathogenic variants in breast cancer susceptibility genes to familial breast cancer risk . 
npj breast cancer 3 : 22 , 2017 therkildsen c , ladelund s , smith - hansen l , et al : towards geneand gender - based risk estimates in lynch syndrome ; age - specic incidences for 13 extracolorectal cancer types . 
evans dg , woodward er , lalloo f , et al : are women with pathogenic variants in pms2 and msh6 really at high lifetime risk of breast cancer ? genet med 13 . 
2018 : is breast cancer truly caused by msh6 and pms2 variants or is it simply due to a high prevalence of these variants in the population ? genet med 21 : 256 - 257 , 2019 14 . 
in this analysis the hypothesis , we explore with an unsupervised learning algorithm whether distinct subtypes of btcp exist and whether they can provide new insights into clinical practice . methods partitioning around a k - medoids algorithm on a large data set of patients with btcp , previously collected by the italian oncologic pain survey group , was used to identify possible subgroups of btcp . 
a free online tool was created for new patients cluster computation to validate these clusters in future studies and provide handy indications for personalized btcp therapy . conclusion this work proposes a classication for btcp and identies subgroups of patients with unique efcacy of different pain medications . 
this work supports the theory that the optimal dose of btcp opioids depends on the dose of basal opioids and identies novel values that are possibly useful for future trials . 
these results will allow us to target btcp therapy on the basis of patient characteristics and to dene a precision medicine strategy also for supportive care . jco precis oncol 4 : 1339 - 1349 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction breakthrough cancer pain ( btcp ) is a common event that affects a considerable proportion of patients with cancer.1 a variety of denitions for btcp have been proposed2 , 3 . 
according to the italian oncologic pain survey ( iops ) study group , 4 btcp should be dened as a relevant change in pain intensity of severe intensity in patients who receive an effective treatment with opioids.4 ( p963 ) nevertheless , despite this unique denition , btcp encloses a wide range of manifestations that differ , among other features , in intensity , duration , frequency , and triggering events . btcp represents a clinically relevant condition with a negative impact on the patients quality of life . 
patients characteristics characteristic value ( n = 4 , 016 ) 2 , 202 ( 54.8 ) male sex interview setting oncology pain therapy palliative care radiotherapy treatment corticosteroids anticonvulsant drugs acetaminophen constipation drugs anxiolytic drugs antidepressant drugs antiemetic drugs nsaids cannabis treatment setting inpatient outpatient domicile day hospital hospice cancer type lung breast pancreas colon prostate rectum stomach bladder at present , several gaps exist in the knowledge of btcp management . 
these partially unanswered questions , among others , concern the optimal drug administration route , pharmacokinetics , the balance between rapid - onset and slow - onset opioids , and the eventual difference of btcp response deriving from clinical features , such as stage , primary site , or metastases . in this analysis , it was thus hypothesized that the unique btcp denition might actually enclose diverse pathologic entities , possibly with peculiar clinical needs and specic responses to drugs . 
these so - called unsupervised learning algorithms have already been extensively used , for example , for the identication of breast cancer subtypes.6 nevertheless , to our knowledge , no authors have yet tried to explore the issue of btcp management using these techniques . to fulll this purpose , we used data that were collected by the iops group in a large , multicentric national study5 , 7 , 8 that enrolled 4 , 056 patients from 32 centers with opioidcontrolled basal pain suffering from btcp . 
this work is therefore a secondary analysis of the iops group survey that aims to identify novel subtypes of btcp through the use of unsupervised learning algorithms . methods patients enrollment and data collection details concerning the enrollment of patients are extensively described in the main paper from the iops group.5 in brief , local ethical committees approved the protocol , and written informed consent was obtained from each patient . interviews were performed in different settings , in particular , oncology , pain therapy , palliative care , and radiotherapy . 
a comprehensive list of clinical variables was collected for each patient that consisted of basal pain and btcp site , duration , frequency , intensity , relieving factors , triggers , drugs , primary cancer site and stage , and concomitant symptoms for a total of 1 , 086 1340 2020 by american society of clinical oncology multiple primary average age , years ( range ) karnofsky performance status ( range ) baseline pain , nrs scale ( range ) note . 
 breakthrough cancer pain clinical features and opioids response features with less than 5% of missing data and associated with a corrected p value of , .1 and , for categorical features , a log2 odds ratio greater than 1 were used to build a multivariable logistic regression . 
to investigate the correlationsimultaneously for all patients and on the same scalebetween the amount of opioids used and btcp therapy satisfaction , all doses of opioid drugs were converted10 to equivalent intravenous morphine doses and expressed as a total daily dose : one for btcp - directed opioids and for basal pain opioids . 
doses were converted to oral morto intravenous morphine doses and not phine doses because intravenous morphine has been increasingly used in different clinical settings and would provide more interpretable graphics in results . 
moreover , to explore the interaction of fast - acting and long - acting opioid dosages , we calculated for each patient the btcp opioidstobasal pain opioids ratio ( opr )  . 
a polynomial logistic regression was used to catch nonlinear relationships between opioid doses and therapy satisfaction . cluster computation and visualization features dening the clinical characteristics of btcp were selected to perform clusters computation . 
the above - mentioned features were used to calculate a dissimilarity matrix using a cluster package11 ; presence of background pain pain intensity 4 of 10 four or fewer episodes per day breakthrough pain presence of peaks well distinguished from background pain intensity cluster fig 1 . 
 ( a ) algorithm used for the diagnosis of breakthrough cancer pain ( btcp ) during patients enrollment in the italian oncologic pain survey ( modied from mercadante et al8 )  . 
 ( b ) a two - dimensional t - distributed stochastic neighbor embedding projection of all patients , colored by their clusters , on the basis of the following btcp features : number of btcp episodes , btcp peaks duration , btcp type , btcp intensity , number of days since the beginning of btcp episodes , eventual benet from pharmacotherapy , eventual benet from rest , and whether btcp was enhanced by movements . each point represents a patient . 
silhouette statistics14 were calculated for each run , and the optimal number of clusters was manually picked as being that with the best trade - off between silhouette statistics and reasonable clinical interpretation . 
we used complete - linkage hierarchical clustering with 12 clusters , along with rand index calculation , to explore the replicability of clusters with a different algorithm . t - distributed stochastic neighbor embedding15 algorithm was used to project dissimilarities between patients in a bidimensional space , with closer points representing patients with more similar clinical btcp features . 
an online tool allows for the repetition of the performed classication on new sets of patients.16 clusters analysis t - test , mann - whitney test , and 2 test were used to assess the association of parametric , nonparametric , and categorical features , respectively , with each cluster . 
patients characteristics are listed in table 1 . cluster computation to investigate whether subtypes of btcp exist , we used btcp features to build an unsupervised clustering model . the number of btcp episodes , btcp peaks duration , btcp type , btcp intensity , number of days since the beginning of btcp episodes , the eventual benet from pharmacotherapy , the eventual benet from rest , and whether btcp was enhanced by movements were the eight btcp - dening variables selected for the nal model , which was built with the k - medoids algorithwe chose 12 as an optimal trade - off between the average width of clusters silhouette ( 0.45 ; appendix fig a1a ) and the interpretability of the clusters themselves . 
 pantano et al figure 1 shows the algorithm used to dene btp ( fig 1a ) t - distributed stochastic neighbor and a 2 - dimensional embedding projection of all patients , colored by their clusters ( fig 1b )  . 
an online tool is available for the classication of new patients according to our method.16 characteristics of btcp clusters we analyzed the enrichment of the eight btcp - dening variables and of other clinical features among the clusters . a description of each cluster is available in table 2 . 
a summary of btcp features according to cluster is presented in figure 2 . btcp therapy satisfaction finally , we tried to assess what inuenced patient - reported btcp therapy satisfaction . 
after converting the opioid dose to a unique scalecorresponding to the equivalent dose of intravenous morphinewe investigated using a nonlinear model the inuence of basal opioid dose , btcp opioid dose , and opr on patient - reported therapy satisfaction . 
of higher therapy satisfaction lower therapy satisfaction btcp opioids dose / basal pain opioids dose higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction btcp opioids dose ( mg ) basal pain opioids dose ( mg ) fig 3 . 
this roughly corresponds to a daily dose of sublingual fentanyl 100 g for btcp and a daily dose of oral morphine 30 mg as the basal opioid dose . we separately performed the same analyses on previously dened clusters ( fig 3d )  . 
for clusters 1 , 6 , and 10 , the satisfaction seemed to grow indenitely with an increase of the opr opioids , whereas clusters 7 , 8 , and 11 seemed to have clear , optimal peaks of opr . 
despite the interpretation being challenged by some large cis , we can say from these data that , depending on the cluster , optimal opr ranges from 15% to 50% . discussion this paper demonstrates a novel approach for the investigation of btcp . 
we acknowledge that this study was not designed to perform this analysis and , moreover , that the large number of clusters might interfere with their interpretability and clinical utility . 
nevertheless , this study represents a proof - ofconcept for this investigational approach . cluster 1 cluster 2 cluster 3 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction cluster 4 cluster 5 cluster 6 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction cluster 7 cluster 8 cluster 9 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction cluster 10 cluster 11 cluster 12 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction fig 3 . 
using our same data , another group proposed 0.20 ( one fth ) as the optimal ratio.5 nevertheless , they used a frequentistic approach , as 0.20 is simply the most common ratio among the cohort . 
this possibly suggests that , instead of starting btcp opioid titration with the lowest possible dosage , as proposed previously , 28 titration could start immediately with an optimal opioid dosage . moreover , cluster analysis reveals that this ratio might not be the same for all patients : some patients might benet from a higher btcp opioid dosage ( cluster 2 and 7 ) , whereas others might benet from a lower one ( cluster 11 )  . 
finally , for some patients , we did not observe an upper threshold for this ratio ( cluster 1 , 6 , and 9 ) , perhaps pointing out patients for whom a strong btcp opioid dosage increase is required . the interpretation is made difcult by the multiple associations and , at this stage , is not mature enough to suggest any immediate change in clinical practice . 
however , we made available an online free tool16 that allows for the classication of new patients according to our algorithm and returns a proposed btcp therapy which depends on the patient cluster optimal opr and basal opioid dose . 
we suggest that this tool might be used in the future to prospectively validate the clinical importance of our clusters in clinical practice and to compare our proposed opioid dosages in settings different from ours . the presence of distinct btcp phenotypes , each one associated with specic clinical features , could also be a reection of diverse underlying pathophysiologic mechanisms : our work suggests that preclinical research might gain insight into these possible differences and help the development of a tailored therapy also for btcp . the main limitation of our study is the appropriateness of collected data for the scope of our work . 
we believe that a prospective study specically designed for the investigation of btcp clusterspossibly with long - term follow - up and therapy success outcomes and not limited to a single timepoint evaluationmight enable a clearer identication of distinct clusters . 
businco hospital , asl 8 , cagliari , italy 20department of biotechnological and applied clinical sciences , section of clinical epidemiology and environmental medicine , university of laquila , laquila , italy 21section of clinical pharmacology and oncology , department of health sciences , university of florence , florence , italy 22department of medicine and surgery sciences , university of bologna , bologna , italy 23paintherapy , s . 
croce e carle hospital , cuneo , italy 24pain therapy ics maugeri , irccs foundation , pavia , italy 25medical oncology , azienda sanitaria universitaria integrata di trieste , trieste , italy 26medical oncology , azienda sanitaria universitaria integrata di udine , udine , italy 27palliative care and oncologic pain service , s . 
pain 41 : 273 - 281 , 1990 portenoy rk , payne d , jacobsen p : breakthrough pain : characteristics and impact in patients with cancer papain 81 : 129 - 134 , 1999 4 . 
mercadante s , marchetti p , cuomo a , et al : breakthrough pain and its treatment : critical review and recommendations of iops ( italian oncologic pain survey ) expert group . 
mercadante s , marchetti p , cuomo a , et al : breakthrough cancer pain : preliminary data of the italian oncologic pain multisetting multicentric survey ( iopsms )  . 
mercadante s , lazzari m , reale c , et al : italian oncological pain survey ( iops ) : a multicentre italian study of breakthrough pain performed in different settings . benjamini y , hochberg y : controlling the false discovery rate : a practical and powerful approach to multiple testing . 
davies an , dickman a , reid c , et al : the management of cancer - related breakthrough pain : recommendations of a task group of the science committee of the association for palliative medicine of great britain and ireland . 
the appropriate number of clusters for additional analyses was found to be 12 , an optimal trade - off between the average width of clusters silhouette ( 0.45 ) and the interpretability of clusters themselves . ( b ) heatmap showing the concordance of pam clustering with complete - linkage hierarchical clustering . 
 circulating tumor dna predicts the response and prognosis in patients with early breast cancer receiving neoadjuvant chemotherapy shunying li , phd1 , 2 ; hongna lai , phd1 , 2 ; jieqiong liu , md1 , 2 ; yujie liu , phd1 , 2 ; liang jin , md1 , 2 ; yudong li , phd1 , 2 ; fengtao liu , md1 , 2 ; yuhua gong , ms3 ; yanfang guan , phd3 ; xin yi , phd3 ; qianfeng shi , md1 , 2 ; zijie cai , md1 , 2 ; qian li , md1 , 2 ; ying li , md1 ; mengdi zhu , md1 , 2 ; jingru wang , md1 , 2 ; yaping yang , md1 , 2 ; wei wei , md4 ; dong yin , phd1 , 2 ; erwei song , md , phd1 , 2 ; and qiang liu , md , phd1 , 2 purpose many patients with breast cancer still relapse after curative treatment . 
serial plasma samples before , during , and after nac and paired tumor biopsies were harvested and subjected to deep targeted sequencing using a large next - generation sequencing panel that covers 1 , 021 cancerrelated genes . results positive baseline ctdna was detected in 21 of 44 patients before nac . 
more importantly , positive baseline ctdna is signicantly associated with worse disease - free survival ( p = .011 ) and overall survival ( p = .004 ) in patients with early breast cancer , especially in estrogen receptornegative patients . conclusion our study demonstrated that ctdna can be used to predict tumor response to nac and prognosis in early breast cancer , providing information to tailor an individuals therapeutic regimen . jco precis oncol 4 : 244 - 257 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction breast cancer is the most commonly diagnosed cancer and the leading cause of cancer death in women worldwide.1 although early breast cancer is a curable disease , up to 40% of such patients still relapse after surgery.2 it is believed that breast cancer is a systemic disease and that clinically undetectable micrometastases often happened before the diagnosis.3 , 4 how to distinguish patients with early breast cancer with high relapse risk from those with low risk remains a critical and challenging clinical question . neoadjuvant chemotherapy ( nac ) is often used in patients with locally advanced or triple - negative / her2positive early breast cancer before surgery to decrease tumor size and enable breast - conserving surgery . 
the current consensus to monitor response to nac is clinical examination backed up by radiologic and sonographic measures.5 however , these measures are quite subjective and have poor interand intraobserver reproducibility.6 moreover , given the heterogeneity of cancer , a reliable method to examine the overall response from local , regional , and micrometastatic lesions in patients with early breast cancer is still lacking . circulating tumor dnas ( ctdnas ) are mutated gene fragments that are exclusively shed by cancer cells into blood , 7 which can be detected by digital polymerase chain reaction ( dpcr ) 8 or sequencing . 
 ctdna predicts prognosis in breast cancer context key objective can the presence and dynamic change of circulating tumor dna ( ctdna ) predict the tumor response and prognosis in patients with breast cancer receiving neoadjuvant chemotherapy ( nac ) ? knowledge generated using a next - generation sequencing panel of 1 , 021 genes , positive baseline ctdna was identied in 21 of 44 patients with early breast cancer before nac . 
positive ctdna before nac was associated with signicantly worse disease - free survival and overall survival , especially in estrogen receptor ( er ) negative patients . relevance our study demonstrates that ctdna has signicant value to complement imaging to monitor tumor response and predict prognosis in patients with early breast cancer , providing information to tailor an individuals therapeutic regimen . 
the high relapse rate in er - negative patients with positive ctdna indicates that it may be necessary to escalate treatment in these high - risk patients . patients with early breast cancer after surgery , ctdna by dpcr predicted metastasis at 7.9 - 11 months earlier than clinical relapse.11 , 12 a few studies also explored the role of ctdna in patients with breast cancer who received nac . 
it was reported that ctdna change during nac was correlated with tumor response13 - 15 or relapse , 16 , 17 although two of them only used dpcr to detect a single gene ( metrassf1a14 or tp5316 ) , and the other study only correlated the ctdna disappearance after the rst cycle of nac with two patients who achieved pathologic complete response.13 advances in next - generation sequencing ( ngs ) 18 technology have enabled the rapid identication and broad coverage of tumor - specic genomic alterations in cell - free dna ( cfdna ) of individual patients.19 - 21 the ngs assay provides an opportunity to screen more genes at a single time point and avoid missing mutations absent in biopsy because of intratumor heterogenicity . 
for patient cohort , sample collection and processing , and ngs sequencing and data analysis , please see the data supplement . statistical analysis the primary end point of this study was to evaluate the clinical value of the presence and dynamic change of ctdna to predict the tumor response and prognosis in patients with breast cancer treated with neoadjuvant chemotherapy . 
all statistical analyses were performed with graphpad prism version 6.0 or r version 3.4.1. results clinicopathological features of patients a total of 52 patients with early breast cancer who received nac were prospectively enrolled in the study since 2013 . eight patients were excluded from further study because of insufcient cfdna in plasma before nac ( fig 1 )  . the clinicopathological features of the 44 patients in the study are listed in table 1 and the data supplement . 
after surgery , the patients were followed up every 6 months . during the follow - up ( median , 46 months ; range , 11 - 68 months ) , 11 patients ( 25% ) had distant metastasis , and 9 of them died of metastatic breast cancer . baseline mutated dnas in plasma and tumor all baseline plasma samples , matched blood cells , and 32 paired tumor biopsy samples underwent parallel targeted ngs to screen for point mutations and structural variants , using the ngs panel of 1 , 021 cancer - related genes that covers a region of 1.1 mb ( data supplement ) .24 after deduplication , the median depths of unique coverage were 984 for primary tumor and 1 , 225 for plasma dna . 
the analysts were blinded to clinical and follow - up information during the analysis of sequencing data . among the 44 patients , 21 patients were found to have positive baseline ctdna . 
a total of 72 mutations in 46 genes were found in these 21 samples , with 1 - 8 ( median , 3 ) mutations per sample ( data supplement )  . 
tp53 ( 20 / 32 ) , pi3kca ( 13 / 32 ) , nf1 ( 5 / 32 ) , and gata3 ( 4 / 32 ) were the most frequently mutated genes in tumor ( fig 2c )  . in the 32 patients with both tumor and plasma sequencing data , 14 had concordant / partially concordant mutations in plasma and tumor , 16 patients had mutations only in tumor with negative ctdna , and the other two patients ( p034 and p036 ) had completely different mutations in tumor and plasma ( fig 2b )  . 
in the 16 patients with positive ctdna , 14 ( 87.5% ) of them had one or more mutations conrmed independently in tumor sequencing data , indicating that most positive ctdna represents tumor - specic mutations in the primary tumors . 
among the 33 concordant mutations found in both tumor and plasma of the 14 patients , tp53 ( 12 / 14 ) and pik3ca ( 4 / 14 ) mutations were the most frequent ( fig 2d )  . changes of ctdna and tumor response during nac the current gold standard to monitor tumor response during nac is ultrasound or magnetic resonance imaging , although it is subjective and sometimes falls behind the histologic changes . 
to explore whether ctdna surpasses imaging in monitoring or predicting overall tumor response , all plasma samples collected during nac in the 20 patients ( 1 patient was excluded because of insufcient cfdna in subsequent plasma samples ) with positive baseline ctdna were sequenced and compared with baseline data to track the dynamic changes of ctdna during nac ( data supplement )  . in this study , tumor response was dened as cr / pr / sd / pd using recist1.1 criteria when the imaging data of local / regional tumor before surgery was compared with that before nac . 
of the 20 assessable patients , 11 did not respond to nac ( including a patient with pd ) , and 9 responded to nac ( response rate , 45% )  . however , patient 038 ( p038 ) , who was dened as pr according to imaging , had an increasing ctdna amount ( clonal variant allele frequency [ vaf ] ) during all cycles of nac , 25 and a persisting high ctdna even after surgery , although she did not have any clinical metastasis before surgery . 
follow - up showed that she had multiple distant metastases ( liver , lung , and bone ) at 21 months and died at 46 months after surgery ( appendix fig a2 )  . 
the increase of ctdna in this case indicated the early micrometastases undetected by imaging did not respond to nac well , although the primary tumor did , suggesting that ctdna is better than imaging of local tumor to monitor the overall response to nac . next we did a longitudinal analysis of ctdna changes during nac and correlated it with local tumor response . p038 was excluded from this analysis because of discrepant tumor and ctdna data . 
the ctdna amount ( clonal vaf ) in baseline plasma was set as 100% , and those in subsequent plasma from the same patient were normalized it was found that patients who to the baseline value . responded to nac had more decreasing ctdna than patients who did not respond to nac ( fig 3a )  . 
the difference was signicant after the second cycle ( p = .03 ) and all cycles of nac ( p = .02 ) but was not statistically signicant after the rst cycle of nac ( p = .290 ; figs 3b - 3d )  . next , we constructed roc22 curves to compare the efcacy of ctdna amount ( clonal vaf ) and ultrasound to predict the response to nac ( fig 4 )  . 
it was found that clonal vaf after 2 cycles , clonal vaf before surgery , and ultrasound after 2 cycles were all predictive of the response to nac before surgery . 
the optimal criteria of clonal vaf in predicting the response to nac , as determined by the roc plots , are 40% drop in clonal vaf after 2 cycles and 60% drop in clonal vaf before surgery , respectively . 
the optimal criterion of ultrasound after 2 cycles was 20% decrease in the longest diameter of tumor in our study . concordant mutations between tumor and plasma were also identied in two patients with smaller tumor and negative lymph nodes ( t2n0m0 )  . 
the er - negative patients with negative baseline ctdna had 100% dfs and os , whereas those with positive baseline ctdna had a dfs / os of only approximately 36% . among the 20 patients with positive baseline ctdna ( one patient ruled out due to lack of subsequent samples ) , 6 of them turned negative and 14 remained positive for the ctdna before surgery . 
six out of 8 ( 75% ) er - negative patients with persistent positive ctdna relapsed , whereas only 1 out of 3 ( 33% ) such patients with negative ctdna before surgery relapsed , although the difference was not statistically signicant because of small sample size ( appendix figure a4 )  . discussion in this study , we used targeted deep sequencing of cfdna with a panel of 1 , 021 cancer - related genes to screen for mutated ctdna in patients with early breast cancer and found that 21 out of 44 patients had positive ctdna . 
more importantly , positive ctdna before nac is signicantly associated with worse prognosis in patients with early breast cancer , with the signicance mainly derived from er - negative patients . many patients with early breast cancer still relapse after surgery because of clinically undetectable micrometastases . 
current imaging methods are not sensitive enough to detect micrometastatic lesions ; even the most sensitive positron emission tomographycomputed tomography has the resolution limit at 4 mm.26 recently , ctdna has been suggested to be an ideal tumor biomarker because of its specicity , stability , and sensitivity . 
it is shown to be better than traditional biomarkers and imaging in predicting the relapse or progression in both early and metastatic cancer.9 , 11 , 12 , 27 - 29 however , the best method to measure ctdna is uncertadpcr is cheaper and easier , but it only measures one or few known mutations . 
to our knowledge , this study used the largest ngs panel so far to look for ctdna in patients with early breast cancer . using the large 1 , 021 - gene panel , somatic mutations were found in all the tumor biopsies . 
more importantly , positive ctdna was found in 47% of patients with early breast cancer and 73% of er - negative patients , which was consistent with previous reports.12 , 16 , 17 , 30 , 31 the majority of the ctdna was conrmed in tumor mutation data , suggesting that ctdna can be used to detect tumor - specic fig 2 . 
 ( c , d ) clonal vaf in no - response patients was signicantly higher than that in response patient after ( c ) 2 , and ( d ) all cycles of nac . 
in the 21 patients with positive baseline ctdna , 16 patients had paired plasma and tumor biopsy samples for ngs analysis , and 14 / 16 had at least one mutation conrmed in primary tumors . 
with the high specicity , at 98.72% , the discrepancy between the mutations in plasma and the mutations in tumor may be explained by the small tumor biopsy specimen not representing the whole primary tumor or micrometastasis . 
but this study also identied 24% ( 5 / 21 ) of patients with positive ctdna who had mutations other than tp53 and pi3kca . interestingly , our data showed that dynamic change of ctdna can be used to monitor and predict the response to nac in early breast cancer . 
kaplan - meier curve compares the disease - free survival ( dfs ) and overall survival ( os ) in patients with breast cancer with positive or negative baseline circulating tumor dna ( ctdna )  . 
nbc , negative baseline ctdna ; pbc , positive baseline ctdna . the change of ctdna level after 2 cycles of nac predicted local tumor response to nac better than ultrasound , although this was not statistically signicant . 
interestingly , none of the four er - negative patients with negative baseline ctdna relapsed during the follow - up , which was strikingly different from the high relapse rate in er - negative patients with positive baseline ctdna . 
other limitations of this study include limited sample size and suboptimal nac cycles , which hinder further subgroup analysis . in conclusion , our study demonstrates the feasibility and validity of ctdna in patients with early breast cancer receiving nac . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . yuhua gong employment : geneplus - beijing yanfang guan employment : geneplus - beijing xin yi employment : geneplus - beijing qiang liu consulting or advisory role : novartis , astrazeneca speakers bureau : pzer , roche , novartis , astrazeneca , eisai no other potential conicts of interest were reported . references bray f , ferlay j , soerjomataram i , et al : global cancer statistics 2018 : globocan estimates of incidence and mortality worldwide for 36 cancers in 185 countries . 
ca cancer j clin 68 : 394 - 424 , 2018 early breast cancer trialists collaborative group ( ebctcg ) , davies c , godwin j , et al : relevance of breast cancer hormone receptors and other factors to the efcacy of adjuvant tamoxifen : patient - level meta - analysis of randomised trials . 
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schiavon g , hrebien s , garcia - murillas i , et al : analysis of esr1 mutation in circulating tumor dna demonstrates evolution during therapy for metastatic breast 11 . 
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robin x , turck n , hainard a , et al : proc : an open - source package for r and s + to analyze and compare roc curves . 
roth e f , silva mj , venet d , et al : circulating tumor dna in her2 - amplied breast cancer : a translational research substudy of the neoaltto phase iii trial . 
 li et al et * 4 2 weeks after surgery no liver metastasis after surgery liver metastasis after 1 cycle b aselin e after 2 cycles b efore surg ery after 3 cycles after surg ery cycles 24 months fig a2 . 
et * 4 , 4 cycles of epirubicin and docetaxel . p031 ( t2n0m0 ) p041 ( t2n0m0 ) tuba3c tp53 raf1 pik3ca notch2 tsc2 tp53 gab2 dnmt3a brd3 fig a3 . 
little is known about the experiences of individuals tested for cdh1 variants in the multigene panel testing era . methods participants recruited from the prospective registry of multiplex testing completed a cross - sectional self - report survey regarding cdh1 genetic testing experiences , medical management , and psychosocial adaptation . results discordance existed in interpretations of cdh1 results ; 13.3% of cases had disagreements in variant classications among commercial laboratories , and 21.4% had disagreements between participant self - report and clinvar classication . 
2019 by american society of clinical oncology introduction hereditary diffuse gastric cancer syndrome ( hdgc ) , attributed to germline cdh1 pathogenic variants ( pv ) , is associated with increased risk for diffuse gastric cancer ( dgc ) and invasive lobular breast cancer ( lbc )  . 
germline cdh1 pv are present in approximately 40% of hdgc families , 1 and 1% to 3% individuals with gastric cancer have a cdh1 pv.2 reported cumulative lifetime dgc risk ranges from 50% to 80%.1 , 3 - 5 prophylactic gastrectomy is a standard management recommendation for individuals with cdh1 pv , given the inability of endoscopic surveillance to reliably identify dgc.5 because of cumulative lifetime lbc risk estimates ranging from 39% to 52% , recommendations for those with cdh1 pv include breast cancer screening via annual mammography , with consideration of breast magnetic resonance imaging beginning at age 30 years ; risk - reducing mastectomy decisions may occur dependent on family history.3 , 6 before the advent of multigene panel testing ( mgpt ) for hereditary cancer susceptibility , candidates for cdh1 genetic testing were evaluated on criteria dened by the international gastric cancer linkage including a conrmed case of dgc consortium , younger than age 40 years , at least two cases of dgc at any age , or the presence of both dgc and lbc younger than age 50 years.5 , 7 thus , individuals undergoing cdh1 gene analysis had a signicant perfamily history of hdgc - associated sonal and / or cancers . 
 hamilton et al context key objective germline cdh1 variants that are associated with hereditary diffuse gastric cancer syndrome ( hdgc ) are rare , but growth in multigene panel testing is leading to patients with limited personal exposure to hdgc being confronted with such results . 
we addressed the question of what are the genetic testing experiences , medical management , and psychosocial adaptation of patients with cdh1 variants identied through multigene panel testing ? knowledge generated discordant interpretations of cdh1 results were observed across testing laboratories , as well as among participants reporting of their results . 
participants with pathogenic cdh1 variants were more likely than those with variants of uncertain signicance to receive recommendations for prophylactic gastrectomy , yet both groups perceived similar , moderate levels of risk for gastric cancer . relevance findings highlight the unique informational and psychosocial needs of patients living with cdh1 variants , suggesting that they may benet from support tailored to the challenges associated with their particular risk status . genetic testing services are increasingly offered outside the cancer genetics specialty , such as via primary care providers , surgeons , and direct - to - consumer companies.10 - 12 given the variability by which preand post - test genetic counseling and testing for cdh1 are currently provided , we sought to characterize the genetic testing experiences , medical management , and psychosocial adaptation of individuals living with cdh1 variants . methods participants participants were recruited from the prospective registry of multiplex testing ( prompt ) , an online genetic registry founded by investigators at memorial sloan kettering , the university of pennsylvania , dana - farber cancer institute , and mayo clinic for individuals age 18 years or older tested for cancer susceptibility genes as part of any commercial mgpt . 
on self - selected enrollment in prompt , individuals consent to participate in the registry ; complete a baseline questionnaire of personal / family history , genetic testing results , and demographic information ; and share their testing report with prompt staff . 
a centralized institutional review board ( chesapeake irb ) approved this research . procedure study data were collected using redcap software13 through an online cross - sectional survey e - mailed to prompt participants with a self - reported cdh1 variant . invitations including a link to the survey ( with two reminders for nonresponders ) were e - mailed to 135 eligible individuals from september to december , 2017 . 
participants reported their understanding of their cdh1 result ( response options : positive genetic test result , likely positive genetic test result , variant of uncertain signicance , negative genetic test result , my test results are not clear to me ) and the year when they learned their result . 
we assessed personal ( yes , no ) and family history ( yes , no , uncertain ) of breast and gastric cancer , and details ( eg , surgery date ) regarding personal cancer treatment . 
recommendation by a health care provider for risk - reducing mastectomy , meeting with a gastroenterologist , and prophylactic gastrectomy , as well as adoption of breast magnetic resonance imaging , risk - reducing mastectomy , meeting with a gastroenterologist , upper endoscopy , and prophylactic gastrectomy , were assessed ( yes , no , unsure )  . 
genetic knowledge was assessed with 21 items regarding basic genetic concepts and aspects of mgpt selected or modied from the university of north carolina genomic knowledge scale.15 cdh1 knowledge was assessed with six investigator - designed items regarding cancer risks and inheritance of cdh1 variants . item response options were true , false , and don ' t know . 
items adapted from the national cancer institute health information national trends survey assessed absolute perceived cancer risks ( how likely are you to get [ breast / gastric ] cancer in your lifetime ? ; 1 = very unlikely to 5 = very likely ) and affective perceived cancer risks ( i feel like i could easily get [ breast / gastric ] cancer in my lifetime ; 1 = i feel very strongly that this will not happen to 5 = i feel very strongly that this will happen ) .16 decision - making experiences . 
ten items selected or modied from quality of a published measure21 assessed positive ( example : my cdh1 test result allows me to take control of my health ; = 0.75 ) and negative ( example : because of my cdh1 test result , i feel awed and stigmatized ; = 0.79 ) effects of cdh1 genetic testing on quality of life . 
three investigator - designed items assessed whether patients shared their cdh1 results with family , why this information was not shared with family , and family interest in genetic testing . statistical analysis seventy - one individuals responded to the survey ( 53% response rate ; appendix figure a1 ) ; however , three respondents did not have a cdh1 result and were excluded from all analyses . 
conicting interpretation was dened as either disagreement among one or more commercial laboratories in variant classications ( evaluable participants : n = 60 ) , or disagreement between participant self - report and clinvar classication ( evaluable participants : n = 56 )  . 
 medical and psychosocial experiences after cdh1 variant detection second , to determine how individuals understanding of their cdh1 results were associated with their medical and psychosocial experiences , we evaluated the survey data of the 60 respondents who self - reported either a pv ( ie , positive genetic test result or likely positive genetic test result ) or variant of uncertain signicance ( vus )  . 
data were examined for missing values ; patients missing responses to more than 20% of variables were excluded ( n = 3 ) , and average values on the basis of existing items were computed for scales missing less than or equal to 20% of items . 
of concern , three of these cases ( 25% of cases with participant / clinvar disagreement ; 5.4% of evaluable sample ) involved participant self - report of pv ( ie , positive genetic test result or likely positive genetic test result ) but clinvar and test report classication of vus . 
dashes indicate that a p value was not computed because of inadequate cell size . ||individuals with a complete stomach at the time of survey completion only . abbreviations : pv , pathogenic variant ; vus , variant of uncertain signicance . * responses of uncertain or unsure were combined with responses of no for analyses . females with at least one healthy breast at the time of learning their cdh1 results only . females with at least one healthy breast at the time of survey completion only . individuals with a complete stomach at the time of learning their cdh1 results only . least one healthy breast at the time of learning their cdh1 results , a minority ( 25.0% ) reported that a health recommended risk - reducing care provider had ever mastectomy ; no differences in recommendation receipt were observed based on cdh1 result . 
experiences with genetic testing among participants with cdh1 variants experience pv ( n = 16 ) vus ( n = 41 ) total ( n = 57 ) ever offered cancer genetic counseling yes , pros and cons discussed but i didn ' t 0 ( 0 ) unsure ever received cancer genetic counseling was given options to have different numbers of genes tested for hereditary cancer don ' t know was sufciently informed about pros and cons of having different numbers of genes tested for hereditary cancer yes , given sufcient information yes , pros and cons discussed but more information would have been helpful understand no , pros and cons not discussed not sure i felt sufciently informed would have preferred more time to decide about how many genes to have tested don ' t know was informed about possibility of identifying vus when deciding whether to undergo testing yes , i was informed and i understood yes , i was informed but it was not clear what that meant informed after i received results no , i was never informed not sure i was informed would have preferred more time to discuss options with family , friends , or health care providers before having genetic testing don ' t know no . 
approximately 39% of the sample recalled being given options to have different numbers of genes tested for hereditary cancer ; of these they received sufcient participants , most ( 68.2% ) felt information about the pros and cons of having different numbers of genes tested . 
specically , those with pv and vus both reported mean scores for the measures of perceived gastric cancer risks consistent with scale midpoints ( ie , absolute perceived gastric cancer risk : neither unlikely nor likely ; affective perceived gastric cancer risk : i feel i am just as likely to get cancer as i am to not get cancer )  . 
regarding emotional outcomes , participants with pv reported greater distress ( p .001 ) and were more likely to be worried about future discrimination on the basis of their cdh1 result ( p = .05 ) than those with vus . participants reported low decisional regret ( mean , 13.13 , 0 to 100 scale ) regarding cdh1 testing , irrespective of their result . 
consistent with a separate analysis of laboratory interpretations of variants identied by hereditary cancer mgpt , 27 discrepancies were not 13.3% of cases , laboratories differed in their interpretation of cdh1 variant pathogenicity . 
dashes indicate that a p value was not computed because of inadequate cell size . abbreviations : pv , pathogenic variant ; vus , variant of uncertain signicance . * missing response ( n = 1 )  . asked only among those who had not shared cdh1 results with all family ( n = 19 ) and participants could select more than one response . free - text responses included i ' m adopted , so my results don ' t apply to them , and most family members would not nd meaningful . asked only among those who shared with ( some ) family , and responses of yes . 
future research should examine how and why such misunderstandings arise and their implications for patients and families . time , differential provider the survey data indicated that , consistent with clinical guidelines , 5 only participants with a pv reported ever receiving a recommendation to undergo prophylactic gastrectomy . 
however , fewer than half of these individuals recalled receiving this recommendation , and receipt of this recommendation was not associated with clinical factors relevant to the timing of this surgical intervention , such as family gastric cancer history or patient age . 
it is unclear why certain individuals with cdh1 pv have been advised to pursue prophylactic gastrectomy and others have not . although there is speculation that the lifetime risk of gastric cancer may be lower in individuals with cdh1 pv and no family history of gastric cancer ( compared with those with a family history ) , at the current time a discussion of gastrectomy remains standard of care.26 , 28 their despite growing access to genetic testing through nongenetics health care providers , most participants were offered and received genetic counseling . 
 medical and psychosocial experiences after cdh1 variant detection patients understand the risks and benets and feel prepared to make an informed decision about mgpt . results also demonstrate that individuals with cdh1 pv and vus each have unique informational and emotional needs . 
those with vus were also less satised with their health care providers knowledge about the result ; however , it is not possible to discern whether this reects a lack of provider familiarity or existing limitations in scientic knowledge about risks and appropriate management of these variants . 
furthermore , although those with pv accurately perceived themselves to be at greater risk for breast cancer than did those with vus , these individuals had similar perceived risks for gastric cancer , which on average reected scale midpoints . 
risk perceptions are important for promoting cancer prevention behaviors , 30 , 31 including management of hdgc8 ; research is needed to understand why some with cdh1 pv seem to hold inaccurate risk perceptions . 
participants with pv did experience greater distress ; however , levels of distress were modest in this sample , consistent with a recent analysis of patient experiences with mgpt for hereditary breast and ovarian cancer.14 this study has several limitations . 
consequently , these ndings may not be generalizable to the individuals with cdh1 variants . broader population of furthermore , analyses used self - reported data regarding individuals medical and genetic testing experiences . 
nonetheless , this research extends beyond past work , which has largely focused on cdh1 mutation carriers prophylactic surgical decision making and adjustment , 8 , 32 - 34 to provide novel insight into the experiences of individuals with cdh1 variants in the era of mgpt . in conclusion , although many with cdh1 pv or vus are satised with their decision to pursue genetic testing , these individuals have unique informational and psychosocial needs . 
low levels of reported recommendations for prophylactic gastrectomy and perceived gastric cancer risks among those with cdh1 pv are particularly worrisome , suggesting a need for strategies ( eg , innovative applications of risk communication principles , 35 - 37 enhanced provider genetics education38 ) to more effectively engage and educate patients and providers about relevant medical management and cancer risks . 
long employment : depuy synthes companies ( i ) stock and other ownership interests : depuy synthes companies ( i ) travel , accommodations , expenses : depuy synthes companies ( i ) fergus j . 
couch consulting or advisory role : astrazeneca research funding : grail travel , accommodations , expenses : grail , qiagen , ambry genetics research funding : novartis ( i ) , ambry genetics , susan g . 
komen for the cure ( i ) , aacr , diana helis henry medical foundation ( i ) , james p . wilmot foundation ( i ) , adrienne helis malvin medical research foundation ( i ) , global biological standards institute ( i ) , breast cancer research foundation mark e . 
robson honoraria : astrazeneca , pzer consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , pzer ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca susan m . 
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balmaa j , digiovanni l , gaddam p , et al : conicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . oncol genomic med 4 : 232 - 236 , 2016 j clin oncol 33 : 3660 - 3667 , 2015 30 . 
katapodi mc , lee ka , facione nc , et al : predictors of perceived breast cancer risk and the relation between perceived risk and breast cancer screening : a meta - analytic review . 
hallowell n , lawton j , badger s , et al : the psychosocial impact of undergoing prophylactic total gastrectomy ( ptg ) to manage the risk of hereditary diffuse gastric cancer ( hdgc )  . 
worster e , liu x , richardson s , et al : the impact of prophylactic total gastrectomy on health - related quality of life : a prospective cohort study . 
odoherty k , suthers gk : risky communication : pitfalls in counseling about risk , and how to avoid thej genet couns 16 : 409 - 417 , 2007 36 . 
wolfe cr , reyna vf , widmer cl , et al : efcacy of a web - based intelligent tutoring system for communicating genetic risk of breast cancer : a fuzzy - trace theory approach . 
 appendix hamilton et al sent survey invitation ( n = 135 ) survey respondents ( n = 71 ) excluded : test report indicated no cdh1 result ( n = 3 ) survey respondents with self - reported understanding of their cdh1 result ( n = 68 ) excluded : respondent did not provide site - specific variant or test report respondent did provide sitespecific variant but it could not be found within the cdh1 gene in clinvar ( n = 5 ) ( n = 3 ) excluded : respondent self - reported understanding of their cdh1 result as my test results are not clear to me respondent self - reported understanding of their cdh1 result as negative genetic test result respondent missing responses to greater than 20% of study variables ( n = 4 ) * ( n = 3 ) ( n = 3 ) evaluable sample for analysis of disagreement among commercial laboratories in variant classifications ( n = 60 ) evaluable sample for analysis of how pv or vus cdh1 results are associated with medical and psychosocial experiences ( n = 57 ) excluded : respondent self - reported understanding of their cdh1 result as my test results are not clear to me ( n = 4 ) * evaluable sample for analysis of disagreement between participant self - report and clinvar classification ( n = 56 ) fig a1 . 
study diagra ( * ) indicates that these excluded cases are the same ; these cases are repeated in the gure to more clearly explain the derivation of the samples used in the study analyses . 
 c association of germline palb2 mutation and response to platinumbased chemotherapy in metastatic breast cancer : a case series case 1 a 51 - year - old female was diagnosed with stage iiia ( ct3 cn2 m0 ) triple - negative invasive ductal carcinoma of the right - side breast . 
at the time of diagnosis , the patient underwent genetic evaluation that was negative for a germline mutation in brca1 and brca2 . six months after completion of her primary therapy , the patient developed recurrent disease in the right - side chest wall and breast . 
next generation sequencing ( foundationone ; foundation medicine , cambridge , ma ) performed on her biopsy specimens showed loss of pten , mutations in partner and localizer of brca2 ( palb2 ) r170fs * 14 , arid2 r890fs * 49 , atrx k108fs * 35 , and ctnna1 duplication of exons 4 to 7 . 
given the finding of a palb2 mutation in the tumor , repeat genetic counseling was advised with expanded germline testing , which showed a pathogenic mutation in palb2 3323dela ( fig 1 )  . 
the patient has remained disease free for 30 months . case 2 a 47 - year - old female was diagnosed with stage ia ( pt1c n0 m0 ) invasive ductal carcinoma of the right - side breast that was estrogen receptor and progesterone receptor positive and human epidermal growth factor receptor 2 ( her2 ) negative ( table 1 )  . 
 two years later , she developed metastatic disease to the lung and chest wall , and biopsy findings were consistent with invasive ductal carcinoma that was weakly estrogen receptor positive ( 20% ) , progesterone receptor negative , and her2 unamplified by fluorescent in situ hybridization . 
 she was treated with multiple lines of endocrine therapy ( fulvestrant , letrozole , and palbociclib ) and chemotherapy ( single agents nab - paclitaxel , eribulin , and navelbine and a combination cyclophosphamide , methotrexate , and fluorouracil regimen ) but progressed with an ulcerating leftside chest wall mass ( fig 3 )  . 
the patient was then treated with carboplatin with near - complete resolution , which was sustained for 2 months ( fig 3 ) ; however , her treatment was stopped because of recurrent thrombocytopenia . 
gene profiling results for each patient . in kdmsa , cdk6 , lyn , and myc ; a homozygous deletion in fat1 ; and a mutation in palb2 y1108fs * 16 were observed . 
509_510delga ( fig 1 )  . discussion palb2 is a tumor suppressor gene that interacts with brca2 and is required for some functions of brca2 in dna repair pathways.1 after interaction with brca2 , palb2 facilitates nuclear localization of the palb2 - brca2 complex , which is then involved in dna repair through homologous recombination.2 germline mutations in palb2 are associated with an increased risk of breast and pancreatic cancer.3 approximately 1% to 3% of women with familial breast cancer harbor a monoallelic mutation in palb2.4 in addition , approximately 1% of patients with triple - negative breast cancer carry such a mutation.5 the lifetime risk of developing breast cancer by age 70 years for a female palb2 mutation carrier depends on family history.6 for those with no family history , the risk of developing breast cancer is 33% , whereas for those with two or more family members with breast cancer , the risk is 58%.6 compared with age - matched cohorts , the relative risk of breast cancer development for women with a palb2 mutation who are younger than 40 years , 40 to 60 years , and older than 60 years is increased by eight - , six to eight - , and fivefold , respectively . 
the risk for development of breast cancer in women who carry a deleterious palb2 mutation seems to differ among ethnic groups.7 , 8 molecular profiling has led to the development of novel therapeutic strategies . 
such mutations in homologous recombination ( hr ) pathways have been shown to improve sensitivity to dna - targeting agents and represent an important therapeutic target . targeted agents have increased treatment efficacy in a variety of breast cancer subtypes . 
these include endocrine manipulation with or without the addition of cyclin - dependent kinase 4 and 6 inhibitors or mammalian target for rapamycin inhibitors for hormone - sensitive disease or her2 - targeted agents for her2 - overexpressed tumors . 
approximately 70% of individuals with germline mutations in brca1 or brca2 and 30% with germline palb2 mutations have triple - negative disease.6 , 9 current data on clinical outcomes in patients fig 2 . 
 in addition , the development of polyp ( adp ribosome ) polymerase ( parp ) inhibitors has introduced the synthetic lethality concept by targeting the base excision repair pathway , which provides a way for targeting both dna repair pathways in patients with a brca defect . 
thus , inactivating mutations in these genes lead to defective hr - mediated dna repair , which makes cancer cells more susceptible to dna - targeting agents.10 increased sensitivity to dna - targeted therapy is described in a variety of solid tumors that harbor palb2 mutations . 
 a previous report described a case of gemcitabine resistant pancreatic cancer with somatic and germline palb2 mutations with an excellent and durable response to platinum agents.11 furthermore , earlier studies have shown improved overall survival and platinum responsiveness in patients with germline or somatic mutations in hr genes and ovarian , fallopian tube , and peritoneal carcinomas.12 although previous case series have documented improved disease response to platinum agents with a variety of solid tumors that harbor palb2 mutations , we present the first documentation to our knowledge of metastatic palb2 - associated breast cancer . 
the patient with a palb2 mutation ( case 1 ) treated with carboplatin had not only a complete response but also a prolonged duration of response of 30 months , which is clinically meaningful . 
a possible explanation for a cancer escape mechanism and retained platinum sensitivity is tumor dormancy or transitory senescence.13 fungating breast lesions present a clinical challenge and can have a severe effect on quality of life . 
these case reports provide additional evidence that platinum agents seem active in metastatic breast cancers , particularly among patients with germline palb2 mutations . the patient with a germline palb2 mutation who had a durable response to carboplatin had several somatic mutations , including pten loss . 
the progect study also seeks to understand predictors of response to neoadjuvant and adjuvant chemotherapy in triple - negative breast cancer associated with a variety of germline mutations , including palb2 . 
ongoing trials are evaluating the efficacy of parp inhibitors ( clinicaltrials . gov identifier : nct02401347 ) and checkpoint kinase 1 inhibitors ( clinicaltrials.gov identifier : nct02873975 ) in women with germline or somatic mutations in hr pathway genes , including palb2 . 
the role of pten in hr is controversial ; however , pten loss and sensitivity to dna - damaging agents , including platinum and parp inhibitors , have been described.14 , 15 a recent study reported long - term responses to maintenance olaparib in patients with brca1 / 2 and pten mutated metastatic ovarian cancer.16 we hypothesize that the combination of germline palb2 mutation and alteration in pten are responsible for the response noted . 
the second patient had a somatic mutation in stag2 , which is a core subunit of a multifunctional cohesion complex , and its mutations have been associated with increased sensitivity to inhibitors of dna repair.17 , 18 whether somatic stag2 mutations contributed to increased platinum sensitivity is unclear . palb2 mutations are associated with higher mortality independent of tumor stage , type of chemotherapy , or hormone receptor status.19 additional studies are required to evaluate whether women with palb2 mutations are at an increased risk of death . 
couch fj , hart sn , sharma p , et al : inherited mutations in 17 breast cancer susceptibility genes among a large triple - negative breast cancer cohort unselected for family history of breast cancer . 
haanp m , pylks k , moilanen js , et al : evaluation of the need for routine clinical testing of palb2 c.1592delt mutation in brca negative northern finnish breast cancer families . 
villarroel mc , rajeshkumar nv , garrido - laguna i , et al : personalizing cancer treatment in the age of global genomic analyses : palb2 gene mutations and the response to dna damaging agents in pancreatic cancer . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
lheureux s , lai z , dougherty ba , et al : long - term responders on olaparib maintenance in high - grade serous ovarian cancer : clinical and molecular characterization . 
 epicapture : a urine dna methylation test for early detection of aggressive prostate cancer purpose liquid biopsies that noninvasively detect molecular correlates of aggressive prostate cancer ( pca ) could be used to triage patients , reducing the burdens of unnecessary invasive prostate biopsy and enabling early detection of high - risk disease . 
epicapture was performed by quantitative methylation - specific polymerase chain reaction in dna isolated from prebiopsy urine sediments and evaluated by receiver operating characteristic and decision curves ( clinical benefit )  . 
the epicapture score was developed and validated on a two thirds training set to one third test set . results higher methylation of epicapture genes was significantly associated with increasing aggressiveness in pca tissues . 
2019 by american society of clinical oncology introduction prostate cancer ( pca ) is the most common noncutaneous malignancy in men and the third leading cause of cancer - related deaths in men in the western world . 
 with an aging population , spread of westernized diet , and increasing use of prostate - specific antigen ( psa ) testing , this figure is predicted to double by 2035.1 pca demonstrates extreme clinical heterogeneity . 
overall , 10 - year survival rates are close to 100%2 ; thus , there is much interest in strategies to reduce overtreatment of low / intermediate risk tumors.3 however , more than 300 , 000 men die as a result of pca each year . 
this stark figure , together with the knowledge that overtreatment comes with the high price of prevalent life - changing side effects , illustrates the need for tools to selectively identify high - risk pca ( those tumors with a high propensity to metastasize ) at an early stage , while the disease is potentially curable . research is ongoing into methods to address this need and better risk - stratify patients . 
urinary analysis of molecular correlates of aggressive disease could be used to triage patients and identify those who actually require an invasive prostate biopsy to histologically diagnose and grade their disease . in 2012 , movember launched four collaborative global action plan ( gap ) initiatives , focusing on pca biomarkers in urine , plasma , serum , and exosomes . 
 underpinning this aim was the cooperative establishment of prebiopsy postdigital rectal examination ( dre ) urine biorepositories at each institution , with a confederated database housing accompanying clinical , pathologic , and lifestyle data . 
six centers from the united states ( emory healthcare , atlanta , ga ) , canada ( university health network and lunenfeld - tanenbaum research institute , sinai health systems , toronto ) , and europe ( st jamess hospital , mater misericordiae university hospital , and tallaght hospital , all in ireland ; norfolk and norwich university hospital , england ) , collected prebiopsy , postdre urine ( 50 ml ) between january 2012 and october 2015 . 
exclusion criteria included previous diagnosis of pca , active urinary tract infection , recent prostate biopsy or transurethral resection of the prostate ( less than 6 wk ) , and confirmed presence of metastatic disease ( by pelvic magnetic resonance imaging or bone scan )  . 
 in total , urine samples were collected from 503 men , with matched formalin - fixed paraffin embedded trus biopsy cores acquired , where available ( fig 1 )  . 
in addition to this prebiopsy population , a retrospective analysis of the epicapture gene loci was performed on two independent cohorts of prostate tissues ( fig a2 ; data supplement )  . sample collection , processing , and epicapture analysis urine samples were stored on ice and processed within 4 hours of collection , following a movember gap1 standard operating procedure . 
details of nucleic acid isolation and quantification and epicapture analysis are provided in appendix table a1 and the data supplement . statistical analysis statistical analyses were performed with r version 3.4.1 and graphpad prism version 6 . 
 clinical utility was assessed by decision curve analysis ( dca ) .16 results epicapture genes demonstrate prognostic utility in prostate tissues mindful that most potential biomarkers fail to translate to the clinic , 17 we first set out to verify the prognostic utility of each epicapture constituent gene by measuring its methylation in two independent cohorts of radical prostatectomy samples . 
there was strong evidence for differences in mean methylation - values between four different groups ( benign , low - risk , aggressive , and metastatic pca ) in a small cohort of prostate tissues ( subjected to epithelial cell enrichment ) measured using the infinium humanmethylation450 beadchip ( fig 2a )  . 
 extracting freely available data from the same analytical platform for a larger the cancer genome atlas cohort yielded similar results ; each epicapture gene demonstrated significantly higher levels of dna methylation in clinically significant and high - risk tumors , relative to histologically benign tissue ( fig 2b )  . 
logistic regression models were developed using a 319 - specimen training set ( corresponding to 70% of the total cohort ) and then evaluated for their ability to correctly predict cancer / high - grade cancer / high - risk cancer in the remaining test set . 
not forgetting the clinical significance of gleason 7 disease , we also applied the revised five - grade grouping system , 18 with a view to detecting group 3 ( gleason 4 and 3 ) and above . 
the combination of epicapture and psa gave the best model ( auc , 0.82 ; sensitivity , 0.73 ; specificity , 0.76 ; appendix fig a1 ; appendix table a2 )  . we next evaluated the training set data to select an epicapture score cutoff that could best inform the decision on whether to perform a biopsy . 
finally , dca showed that at this threshold , epicapture demonstrated a net benefit over psa in the decision on whether to perform a biopsy , enabling a 15% reduction in prostate biopsies ( figs 3i and 3j )  . epicapture genes show high reproducibility by independent analysis to examine the robustness of epicapture , a matched quantitative methylation specific pcr analysis of two of the panel ( g1 : gstp1 , and g5 : apc ) was carried out in two independent laboratories on 236 of the urine samples . 
 ( a ) laser capture microdissected enriched prostate epithelial cells from benign prostate tissue ( procured from men undergoing radical cystoprostatectomy for bladder cancer , with no clinical or histologic evidence of prostate cancer [ pca ] ) and low - risk , aggressive , and metastatic pca . 
 ( b ) data extracted from the tcga repository for matched - benign prostate tissue and low - risk , significant , and high - risk pca , all procured from men undergoing radical prostatectomy . 
the performance of epicapture compared with / in conjunction with prostate - specific antigen ( psa ; treated as a continuous variable ) in the test set ( n = 134 ) for predicting each end point was assessed by receiver operating characteristic curves : ( a ) cancer ( v no cancer detected on transrectal ultrasound biopsy ) , ( b ) high - grade cancer ( gleason score greater than or equal to 8 v all else ) , ( c ) damico high - risk cancer ( v all else ) , and ( d ) capra ( cancer of the prostate risk assesment ) high - risk cancer ( v all else )  . 
the distribution of epicapture scores in the whole study population ( n = 453 ) , viewed by ( e ) biopsy outcome , ( f ) gleason grade , ( g ) risk categorization by damico risk - classification systems , and ( h ) risk categorization by capra risk - classification systethe epicapture score was calculated for each sample by summing the normalized index of methylation ( data supplement ) for g1 to g6 . 
epicapture score distributions were analyzed by t test or one - way analysis of variance ( anova ) , followed by post hoc analyses using the tukey - kramer multiple comparisons test . 
furthermore , matched data were available for 18 of 30 high - risk / grade samples that were epicapture negative , of which 15 ( 83.33% ) and 16 ( 88.89% ) were also negative for g1 and g5 , respectively , in the independent analysis . parallel epicapture analysis in urine and matched biopsy cores highlights value of liquid biopsy pca is renowned for its multifocal nature . 
matched formalin fixed paraffin - embedded biopsy cores were available for a proportion of patients , enabling parallel epicapture analysis on multiple tumor foci and urine from individual men ( n = 15 )  . 
the most interesting insights came from the matched analysis of urine with multiple biopsy cores , of which two notable cases are highlighted . patient sjh149 was diagnosed with a minute focus of gleason score 6 adenocarcinoma . 
this finding could suggest that the source of the tumor dna analyzed in urine could have been the high - grade tumor , which was not sampled on the original biopsy . 
 in contrast , patient sjh189 was diagnosed with a high - percentage , high - grade ( intermixed patterns of grade 4 and 5 ) pca on both sides of his prostate . 
so , despite pathologic heterogeneity within the gland , the three tumor areas seemed to be epigenetically homogeneous . discussion in this urine pca biomarker study , we evaluated the performance of epicapture , a six - gene dna methylation panel , for noninvasive detection of pca and more specifically high - grade or high - risk pca in urine from patients referred for prostate biopsy on the basis of elevated psa and / or abnormal dre . 
complying with remark guidelines , we describe a new dna methylation - based urine test for early detection of aggressive pca . many prostate tumors display a protracted disease trajectory , almost indolent in behavior.19 the widespread use of the serum psa test in many countries has significantly increased the incidence and thus overtreatment of these lowrisk cancers with little likelihood of clinical manifestation.20 - 23 an important first consideration in developing epicapture was to therefore critically appraise the evidence for prognostic utility of each constituent gene . 
conversely , however , it is estimated that approximately two thirds of men undergoing invasive prostate biopsy have no tumor diagnosed , because of the high false positive rate of serum psa.23 , 24 as such , millions fig 3 . 
 ( i ) decision curve analysis demonstrated net clinical benefit of performing biopsy on patients in the test set on the basis of an epicapture score greater than 1.25 versus psa greater than or equal to 3 ng / ml across a range of clinically relevant threshold probabilities ( the risk of cancer , such that a patient would choose to undergo biopsy by weighing the relative harms of false - positive and false - negative predictions )  . 
 ( a ) two of the six epicapture assays ( g1 : gstp1 and g5 : apc ) were analyzed independently in laboratories in ireland ( perry ) and canada ( bapat ) by quantitative methylation specific pcr in urine sediments from 236 of 453 men in the study . 
 relevant subsets were then considered by applying the study end points : ( b ) men with biopsy - positive disease , ( c ) men with high - grade ( gleason score greater than or equal to 8 ) prostate cancer , and men with highrisk prostate cancer defined by ( d ) damico , and ( e ) capra ( cancer of the prostate risk assessment ) classification . 
 repeat biopsy ( 8 months later ) sjh149 urine biopsy core ( s ) sample type base apex base apex histologically benign gleason 6 gleason 7 gleason ( cid : 116 ) 8 urine tissue sjh189 urine biopsy core ( s ) sample type fig 5 . 
 tumor presence is denoted by pink ( gleason score 6 ) , red ( gleason score 7 ) , or brown ( gleason score greater than or equal to 8 ) circles , with size indicative of percentage tumor in each core . 
 ( a ) low - risk prostate cancer sjh149 ( 62 years of age ; prostate - specific antigen , 3.08 ng / ml ) demonstrated that urine as a liquid biopsy is a viable alternative to sampling bias inherent to tissue needle biopsies . 
 sophisticated imaging technologies , such as magnetic resonance imaging , may improve the accuracy of prostate biopsy , 30 their widespread application is hampered by high cost , access to specialist equipment and personnel , interobserver subjectivity , and requirement for anesthesia . 
alternatively , transperineal biopsy enables a more complete sampling of the gland , including the anterior prostate , but also requires anesthesia and is thus unsuitable as a population - based detection method for such a prevalent disease . the dearth of blood - based prognostic biomarkers as a screening tool for aggressive pca in conjunction with limitations of the prostate biopsy in its various forms has led to excitement around urine biomarkers . 
physical manipulation of the prostate by dre , followed by a first - void urinalysis , could provide a simple , holistic insight into molecular alterations occurring in the prostate gland . 
indeed , many studies have demonstrated significant value in detecting and noninvasively monitoring several genitourinary malignancies through urine.31 - 34 some other prognostic urine indicators of aggressive pca have already been described . 
early studies demonstrated detection of gstp1 methylation in urine from patients with pca , although sensitivity was poor ( less than 30% ) .39 follow - up work expanded the repertoire of markers ( gstp1 , apc , and rar2 ) , which improved sensitivity to approximately 60%.40 the epicapture panel represents five commonly perturbed pathways in pca : intracellular detoxification , wnt and igf axes , cell cycle , and prostaglandin biosynthesis . 
in contrast , applying an epicapture threshold ( greater than 0.73 ; developed on training set ) did not markedly alter its diagnostic performance ( auc , 0.68 ) and delivered a 79% improvement over the tumor specificity of psa . in an effort to address the prognostic utility of epicapture within the context of the clinically heterogeneous gleason 7 disease , we applied the revised five - grade grouping system , 18 in addition to two widely used risk - classification systems . 
the epicapture performance characteristics represent a potential improvement on existing methods for patient stratification and for determining the need to perform biopsy , detecting 85% of highgrade tumors , with an npv of 98% . 
furthermore , the overlap of gstp1 and apc in the two gap1 urine dna methylation biomarker panels revealed excellent correlation in detection of aggressive pca , illustrating the robustness of these biomarkers . 
in the context of the diagnostic gray zone , psa 4 to 10 ng / ml , epicapture demonstrated potential for further classifying patients , positive in 40% of men with highgrade pca . 
 although these data are promising , a large prospective clinical trial is needed to assess whether epicapture offers a survival advantage . a limitation of our study is that the cohort is young ; analysis was only possible using biopsy as the end point . 
we cannot rule out the possibility that a proportion of our epicapture - positive urine samples in men with low - grade or benign tissues were indeed tumor cases missed on biopsy . 
evidence actually shows that dna methylation detected in histologically benign tissue ( due to an epigenetic field effect from the cancer ) , can be used as a tool to rule out the possibility that the biopsy missed the tumor . 
 for example , the confirm mdx test , which measures dna methylation at three genes ( gstp1 , apc , and rassf1 ) in histologically benign biopsy tissue cores , is used to guide the decision to repeat a biopsy.41 conversely , 14 of 47 ( 29.79% ) high - grade tumors were epicapture negative . 
independent analysis revealed concordant negativity in more than 80% of these men , and lowering the epicapture threshold did alter this result ; they were negative across all six markers . 
we believe that the most likely reason is interoperator differences in dre ; these high - risk / grade cancers were epicapture negative because they had insufficient / undetectable prostate cells present in their urine . 
 relationships may not relate to the subject matter of this enable confirmation of the presence of prostate cells in the urine , validating its suitability for epicapture analysis and ultimately improving the performance of the test . 
future work will also investigate the intra - individual reproducibility of epicapture by repeated measures in men . finally , to the best of our knowledge , this is the first pca biomarker study to perform a matched analysis of tissue and liquid biopsies . 
a more extensive project is now warranted to fully assess the effects of the multifocal nature of pca on signatures derived from liquid biopsies . epicapture could be used in conjunction with existing tools ( ie , psa and risk calculators ) to help guide the decision to biopsy . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . eve o ' reilly no relationship to disclose alexandra v . 
dale no relationship to disclose rick brugman no relationship to disclose gavin clarke no relationship to disclose olivia schmidt no relationship to disclose shane o ' meachair no relationship to disclose dattatraya patil no relationship to disclose kathryn l . 
pellegrini no relationship to disclose julia garcia no relationship to disclose fang zhao no relationship to disclose stephen finn honoraria : roche robert mills no relationship to disclose marcelino y . 
gallagher employment : oncomark leadership : oncomark neil fleshner honoraria : amgen , janssen oncology , bayer , sanofi , abbvie , ferring pharmaceuticals , astellas medivation consulting or advisory role : hybridyne health research funding : ferring ( inst ) , astellas pharma ( inst ) , janssen oncology ( inst ) , amgen ( inst ) , nucleix ( inst ) , progenix ( inst ) , spectracure ab ( inst ) research funding : amgen ( inst ) travel , accommodations , expenses : pfizer stock and other ownership interests : oncomark consulting or advisory role : carrick therapeutics research funding : carrick therapeutics patents , royalties , other intellectual property : two patents which have been licensed to oncomark travel , accommodations , expenses : oncomark rustom p . 
brewer patents , royalties , other intellectual property : patents held in drug discovery with novartis ( i ) , patents pending concerning cancer subtype detection and biomarkers with university of east anglia bharati bapat no relationship to disclose martin g . 
perry patents , royalties , other intellectual property : university college dublin holds a patent that relates to this work acknowledgment we thank the urologists and their teams at participating hospitals and the health research boardfunded dublin centre for clinical research network , affiliated research nurses , and technical staff , in particular john mccourt . 
we thank investigators drs robert vessella , and colm morrissey , and the patients and families who participated in the prostate cancer donor program at the university of washington medical center . 
bristow , director , manchester cancer research centre , chief academic officer and honorary consultant , christie nhs trust , university professor of cancer studies , university of manchester , manchester cancer research centre , university of manchester , manchester , uk . chris parker , royal marsden hospital , sutton , uk . ian mills , queens university belfast , centre for cancer research and cell biology , movember / prostate cancer uk centre of excellence , school of medicine , dentistry , and biomedical sciences . 
sanda , emory university school of medicine , atlanta , ga ; neil fleshner , julia garcia , fang zhao , and bharati bapat , university of toronto , toronto , ontario , canada ; robert mills , norfolk and norwich university hospital ; marcelino y . 
brewer , earlham institute , norwich , england . supported by grant funding from movember ( gap1 urine biomarker award ) , us prostate cancer foundation ( young investigator award , a.s.p. ) , science foundation ireland grants no . 
bastian pj , ellinger j , heukamp lc , et al : prognostic value of cpg island hypermethylation at ptgs2 , rar - beta , ednrb , and other gene loci in patients undergoing radical prostatectomy . 
damico av , whittington r , malkowicz sb , et al : biochemical outcome after radical prostatectomy , external beam radiation therapy , or interstitial radiation therapy for clinically localized prostate cancer . 
cooperberg mr , pasta dj , elkin ep , et al : the university of california , san francisco cancer of the prostate risk assessment score : a straightforward and reliable preoperative predictor of disease recurrence after radical prostatectomy . 
vickers aj , cronin am , roobol mj , et al : a four - kallikrein panel predicts prostate cancer in men with recent screening : data from the european randomized study of screening for prostate cancer , rotterdaclin cancer res 16 : 3232 - 3239 , 2010 29 . 
siddiqui mm , rais - bahrami s , turkbey b , et al : comparison of mr / ultrasound fusion - guided biopsy with ultrasound - guided biopsy for the diagnosis of prostate cancer . 
costa vl , henrique r , danielsen sa , et al : three epigenetic biomarkers , gdf15 , tmeff2 , and vim , accurately predict bladder cancer from dna - based analyses of urine samples . 
torres - ferreira j , ramalho - carvalho j , gomez a , et al : mir - 193b promoter methylation accurately detects prostate cancer in urine sediments and mir - 34b / c or mir - 129 - 2 promoter methylation define subsets of clinically aggressive tumors . 
wei jt , feng z , partin aw , et al : can urinary pca3 supplement psa in the early detection of prostate cancer ? j clin oncol 32 : 4066 - 4072 , 2014 35 . 
leyten gh , hessels d , jannink sa , et al : prospective multicentre evaluation of pca3 and tmprss2 - erg gene fusions as diagnostic and prognostic urinary biomarkers for prostate cancer . 
van neste l , partin aw , stewart gd , et al : risk score predicts high - grade prostate cancer in dna - methylation positive , histopathologically negative biopsies . 
 ( a ) the performance of epicapture compared to and in conjunction with prostate - specific antigen ( psa ; treated as a continuous variable ) in the test set ( n = 134 ) for predicting isup group 3 , 4 and 5 pca on biopsy was assessed by receiver operator characteristic curves . 
 ( b ) the distribution of epicapture scores in biopsy - negative ( no cancer detected ) v biopsy positive patients , categorized by isup group , shows increasing methylation by group . 
epicapture was performed in urine and matched formalin - fixed paraffin embedded biopsy cores from randomly selected biopsy - positive ( n = 15 : low - risk [ capra and damico , gleason score 6 ; intermediate risk , gleason score 7 ; and high risk , gleason score 8 ] ) patients . 
dna methylation of each gene is indicated by the nim ( normalised index of methylation ) , and for the collective panel , by the epicapture score ( nim sum g1 - g6 )  . 
each point represents a single sample ( biopsy core or urine ) , with the mean for each group indicated by a horizontal line ( yellow , urine ; blue , tissue )  . 
 multigene hereditary cancer panels reveal high - risk pancreatic cancer susceptibility genes purpose the relevance of inherited pathogenic mutations in cancer predisposition genes in pancreatic cancer is not well understood . 
we aimed to assess the characteristics of patients with pancreatic cancer referred for hereditary cancer genetic testing and to estimate the risk of pancreatic cancer associated with mutations in panel - based cancer predisposition genes in this high - risk population . methods patients with pancreatic cancer ( n = 1 , 652 ) were identified from a 140 , 000 patient cohort undergoing multigene panel testing of predisposition genes between march 2012 and june 2016 . 
gene - level mutation frequencies relative to exome aggregation consortium and genome aggregation database reference controls were assessed . results the frequency of germline cancer predisposition gene mutations among patients with pancreatic cancer was 20.73%. 
mutations in atm , brca2 , cdkn2a , msh2 , msh6 , palb2 , and tp53 were associated with high pancreatic cancer risk ( odds ratio , > 5 ) , and mutations in brca1 were associated with moderate risk ( odds ratio , > 2 )  . 
in a logistic regression model adjusted for age at diagnosis and family history of cancer , atm and brca2 mutations were associated with personal history of breast or pancreatic cancer , whereas palb2 mutations were associated with family history of breast or pancreatic cancer . conclusion these findings provide insight into the spectrum of mutations expected in patients with pancreatic cancer referred for cancer predisposition testing . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction pancreatic cancer ( pc ) is the fourth most common cause of death resulting from cancer in the united states.1 epidemiologic studies have suggested that 10% to 20% of pcs are associated with an inherited component , with familial pc , defined as kindreds containing at least two affected first - degree relatives , as an established entity of inherited disease.2 pc is a component of hereditary breast - ovarian cancer syndrome , 3 , 4 lynch syndrome , 5 , 6 familial adenomatous polyposis , 7 familial atypical multiple mole melanoma syndrome , 8 hereditary pancreatitis , 9 peutz - jeghers syndrome , 10 and li - fraumeni syndrome.11 recent studies involving familial pc kindreds have further characterized the role of brca1 / 2 , cdkn2a , atm , and palb2 in pc susceptibility.12 - 14 until recently , germline studies of pcs have focused on single cancer predisposition genes.15 , 16 the first panel - based study of 13 cancer predisposition genes among patients with pc identified 11 mutations ( 3.8% ) in atm , brca1 / 2 , mlh1 , msh2 , msh6 , and tp53 , 17 whereas a 22 - gene panelbased study identified atm , brca1 / 2 , chek2 , and palb2 mutations in 13% of 96 sequentially collected pcs.18 a majority of these mutations were identified in pcs with a family history of pancreatic , breast , ovarian , or colorectal cancer , suggesting that a better understanding of pc risk will depend on evaluation of families with broad constellations of tumors.18 more recently , panel - based approaches identified germline chunling hu holly laduca hermela shimelis eric c . 
 mutations in 4% ( 33 of 854 ) of patients with apparently sporadic pc19 and in 25% ( 44 of 176 ) of patients with advanced pc.20 here , we report results from panel - based clinical testing of 1 , 652 patients with pc from a large cohort of > 140 , 000 patients evaluated by a single diagnostic laboratory and calculate gene - specific risks of pc by comparison with exome aggregation consortium ( exac ) and genome aggregation database ( gnomad ) reference controls.21 , 22 methods study population patients with pc ( n = 1 , 819 ) were identified from a large cohort of > 140 , 000 patients undergoing multigene panel testing of seven to 49 cancer predisposition genes between march 2012 and june 2016 at ambry genetics23 ( aliso viejo , ca ; appendix table a1 )  . 
exclusion criteria , including the presence of neuroendocrine tumors or intraductal papillary mucinous neoplasms , reduced the number of patients for analysis ( n = 1 , 652 ; appendix )  . 
 the study was approved by the western institutional review board . multigene panel testing mutation testing was performed by sequencing of targeted custom capture products from several multigene panels and targeted chromosomal microarray analysis , as previously described.24 genomic dna was isolated from each patients blood or saliva specimen using a standardized methodology ( qiagen , valencia , ca )  . 
sequence enrichment was performed by incorporating the genomic dna into microfluidics chip or microdroplets along with primer pairs or by a bait - capture methodology using long biotinylated oligonucleotide probes ( raindance technologies , billerica , ma ; integrated dna technologies , san diego , ca ) , followed by polymerase chain reaction and then next - generation sequencing analysis ( illumina , san diego , ca ) of all coding exons plus at least five bases into the 5 and 3 ends of all the introns and untranslated regions . 
all mutations identified by ambry genetics are submitted to the clinvar public database . statistical methods the observed frequency of all pathogenic mutations within each gene in white patients with pc was compared with the frequency of pathogenic mutations in the exac non - finnish european ( nfe ) nonthe cancer genome atlas ( tcga ) reference control after data cleaning and filtering ( appendix ) as previously described.23 copy number variants in all genes and mutations in pseudogene homology regions ( pms2 exons 9 and 11 to 15 ) were excluded from cases and controls for risk estimation , because these alterations were not individually validated in exac or gnomad controls . 
although these gnomad controls partially overlap with exac nfe non - tcga controls , the substantially increased number along with updated variant calling algorithms identified gnomad as an independent reference control data set . 
 ( % ) patients of all ethnicities ( n = 1 , 652 ) white patients ( n = 1 , 256 ) age at pc diagnosis were evaluated using the kolmogorov - smirnov test . 
 compared with a median age at pc diagnosis of 70 years in surveillance , epidemiology , and end results registries between 2010 and 2014 , 26 the median age at diagnosis was 63 years among patients with pc . 
among white patients with pc , 38.1% had a firstor second - degree relative with pc , and 48.8% had a family history of breast cancer ( table 1 )  . 
similar frequencies were observed for patients with pc of all races and ethnicities . pathogenic mutations among patients with pc the combined frequency of mutations in genes from all hereditary cancer testing panels was 20.73% for patients with pc of any race or ethnicity and 21.12% for white patients ( appendix table a2 )  . 
brca2 was the most frequently mutated predisposition gene ( 4.64% ) among patients diagnosed at age 63 years , and atm was most frequently mutated ( 4.03% ) in patients with pc diagnosed at age > 63 years ( appendix table a4 )  . 
association analyses using gnomad reference controls confirmed all significant associations , and gene - specific risk estimates were highly similar , except for slightly attenuated risk for palb2 mutations and increased risk for tp53 ( appendix table a6 )  . the same genes were associated with increased pc risk when considering patients of all races and ethnicities compared with exac all race and ethnicity controls ( appendix table a7 ) and after excluding those who had previously tested negative for brca1 / 2 mutations before panel testing ( appendix table a8 )  . 
risk estimates for most genes were slightly diminished when including only those patients with pc for whom pc was the first cancer diagnosis , although msh2 and tp53 mutations were no longer significantly associated with moderate risk of pc because of the decreased number of mutations in patients with pc , and the modest or associated with chek2 was marginally significant ( appendix table a9 )  . 
in contrast , analyses using only exac nfe non - tcga variants in the high - quality pass category marginally increased the ors for each gene ( appendix table a10 )  . 
mutations in atm , brca2 , and palb2 were also more frequent in patients with pc with a family history of breast cancer ( first or second - degree relative ; table 3 )  . 
in contrast , only palb2 and msh2 displayed a substantial increase in mutation frequency among patients with a family history of pc , and only chek2 , msh2 , and tp53 had increased frequencies of mutation among patients with pc with a family history of colorectal cancer ( table 3 )  . 
 family history of pc ( p = .029 ) or breast cancer ( p = .0056 ) and the association of chek2 mutations with family history of colorectal cancer ( p = .014 ; table 4 )  . performance of genetic testing criteria among mutation carriers consensus clinical genetic testing guidelines include pc as a component tumor for seven of the confirmed pc genes in this study ( brca1 / 2 , msh2 , msh6 , atm , palb2 , and cdkn2a ) .27 - 29 clinical histories of patients with mutations in these genes were evaluated to determine whether the respective genetic testing criteria were met ( table 5 )  . 
although a majority of brca1 / 2 and all msh2 mutation carriers displayed histories consistent with testing criteria , 50.0% of atm , cdkn2a , palb2 , and msh6 carriers met criteria . 
in addition , no cdkn2a families met diagnostic criteria for familial atypical multiple mole melanoma syndrome , 30 and 38.9% ( seven of 18 ) did not report any personal or family history of melanoma . discussion here we report a study of cancer predisposition gene mutations among patients with pc on the basis of a cohort of individuals undergoing hereditary cancer multigene panel testing from a single clinical laboratory . 
results from case control studies of the pc cases and exac reference controls identified six genes associated with high risk ( or , > 5 ) of pc ( atm , brca2 , cdkn2a , msh6 , palb2 , and tp53 ) , consistent with previous smaller studies and segregation studies from pc families . 
msh2 was also associated with a high risk of pc ; however , additional studies are needed to confirm these findings , because this association was based on a limited number of mutations detected among pc cases . 
 here we show that brca1 mutations are associated with a moderate risk ( or , > 2 ) of pc , even in a series of sensitivity analyses accounting for potential modifying effects of other cancers . 
 chek2 mutations were also associated with a moderate risk of pc ; however , this association was either diminished ( or , < 2 ) or nonsignificant in several sensitivity analyses . 
one likely explanation is that stk11 mutations are unlikely to occur in the absence of pathognomonic clinical characteristics associated with peutz - jeghers syndrome , and therefore , patients with suspected peutz - jeghers syndrome may be referred for single - gene testing more often than multigene testing . 
pathogenic mutations in other panel genes were still sufficiently uncommon to allow assessment of associations with risk ( eg , apc , mlh1 )  . the risk estimates for pc associated with each of these established predisposition genes will help improve clinical pc risk assessment . 
for some genes , these results offer more precise estimates than previously reported , whereas for others , such as palb2 and atm , we are the first to characterize the level of risk , to our knowledge . 
 it should be noted that the interpretation of the risks reported here is specific to patients referred for hereditary cancer genetic testing based on a personal or family history of cancer ( at least one diagnosis of pc in the family ) , and thus , these data may not be applicable to the general population or unselected pc cohorts . 
despite the enrichment for cases with personal or family history of cancer , these risks are derived from a broader clinical cancer testing cohort compared with previous studies selected for classic syndromic phenotypes such as fammm and therefore demonstrate that pc risk from syndromic genes remains high across a range of clinical histories . 
furthermore , this enrichment presented an opportunity to explore predictors of germline mutations . in total , 13% of patients had mutations in genes significantly associated with increased risk for pc across a range of sensitivity analyses ( atm , brca1 , brca2 , cdkn2a , msh6 , palb2 , and tp53 )  . 
family history of breast , pancreatic , or colorectal cancer was a significant predictor of positive results , suggesting that histories of these cancers should specifically be considered as genetic testing guidelines evolve for pc . 
the remaining 9% ( 15 of 173 ) of mutations were found in the approximately 65% of patients with pc without a family history of these cancers , suggesting a mutation rate of only 2.1% in white patients with pc without a family history of cancer ( 15 mutations in 698 ) in the clinically tested cohort . 
additional studies of population - based series of patients with pc are needed to determine whether clinical panel testing should be considered for patients with pc unselected for family history . in practice , patients with pc may not benefit directly from genetic testing because of the high mortality rate for this cancer . 
however , knowledge of mutation status for genes such as brca1 / 2 and palb2 with respect to clinical trial eligibility for targeted agents such as poly ( adp - ribose ) polymerase inhibitors may make genetic testing more appealing . 
in addition , mutation - positive family members can significantly benefit from knowledge of increased risk for a variety of cancers , including pc , and mutation - negative family members can also adjust their cancer screening protocols accordingly . 
in addition , the international cancer of the pancreas screening consortium and the american college of gastroenterology 29 , 31 recommend that pc surveillance , including annual endoscopic ultrasound and / or magnetic resonance imaging , be considered for individuals with > 5% lifetime or relative risk for pc . 
in addition , although brca1 mutation carriers with a firstor second - degree relative with pc are included in the list of patients for whom pc screening should be considered , the moderate pc risk categorization for brca1 in this study suggests this may not be clinically indicated . exac nfe non - tcga controls were used in this study because of the lack of a large series of matched controls . 
although the use of large reference data sets is not ideal , the large sample size allows precise estimation of the frequency of mutations in individuals without cancer and is likely reflective of the general population . 
in addition , we applied many data cleaning steps and used consistent criteria for selection of mutations in the clinical cohort of patients with pc and the exac controls to ensure that the data sets were adequately normalized for case - control association analyses . 
in a recent assessment of the quality of clinical history information for patients undergoing hereditary cancer panel testing , pedigrees and / or clinic notes were provided for 46% of randomly selected patient cases ( unpublished data )  . 
 when compared with pedigrees and clinic notes , a vast majority of proband cancers were reported completely ( 95% ) and accurately ( > 99% ) on test requisition forms . 
among family members , 76% of melanomas and > 80% of breast , ovarian , colorectal , endometrial , and pancreatic cancers were reported with 98% accuracy on test requisition forms . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : ambry genetics chunling hu no relationship to disclose holly laduca employment : ambry genetics hermela shimelis no relationship to disclose eric c . 
lee no relationship to disclose brigette tippin davis employment : ambry genetics stock and other ownership interests : ambry genetics research funding : ambry genetics ( inst ) travel , accommodations , expenses : ambry genetics mary helen black employment : ambry genetics research funding : ambry genetics travel , accommodations , expenses : ambry genetics tina pesaran employment : ambry genetics stock and other ownership interests : ambry genetics travel , accommodations , expenses : ambry genetics david e . 
rahib l , smith bd , aizenberg r , et al : projecting cancer incidence and deaths to 2030 : the unexpected burden of thyroid , liver , and pancreas cancers in the united states . 
risch ha , mclaughlin jr , cole de , et al : population brca1 and brca2 mutation frequencies and cancer penetrances : a kin - cohort study in ontario , canada . 
ruijs mw , verhoef s , rookus ma , et al : tp53 germline mutation testing in 180 families suspected of li - fraumeni syndrome : mutation detection rate and relative frequency of cancers in different familial phenotypes . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
laduca h , stuenkel aj , dolinsky js , et al : utilization of multigene panels in hereditary cancer predisposition testing : analysis of more than 2 , 000 patients . 
canto mi , harinck f , hruban rh , et al : international cancer of the pancreas screening ( caps ) consortium summit on the management of patients with increased risk for familial pancreatic cancer . 
 appendix patient cases of pancreatic cancer a total of 1 , 819 patients with pancreatic cancer were identified in a cohort of 140 , 449 individuals undergoing clinical germline cancer panel testing between march 2012 and june 2016 at a clinical testing laboratory ( ambry genetics , aliso viejo , ca )  . 
all variants classified by ambry were submitted to clinvar . exome aggregation consortium reference controls the exome aggregation consortium ( exac ) contains exome sequence data from 60 , 706 unrelated individuals sequenced as part of various disease - specific and population genetic studies . 
exclusion of sequence data from these patient cases yielded exac non - nfe non - tcga reference controls . genome aggregation database reference controls the genome aggregation database ( gnomad ) contains sequencing data of 123 , 136 exomes and 15 , 496 genomes from unrelated individuals sequenced as part of various disease - specific and population genetic studies . 
 gnomad data cleaning and filtering restricted to gnomad nfe exome data combined with gnomad ashkenazi jewish exome data . genomics viewer and by frequency in control data from dbsnp . pathogenic variant classification rules : same as in exac rules 1 to 8 . review variants with allele count 15 by integrative allele number was calculated as average of all variants within the coding region of a gene of interest . 
bekelman , md2 , 4 , 6 , 7 the senseless killings of george floyd , ahmaud arbery , breonna taylor , and countless others have led to a national reckoning on institutional racism . medicine , race has long been used as a heuristic , or mental shortcut , used by clinicians to process information and make decisions within the time and cognitive constraints of our healthcare system.1 however , using race as a heuristic in medical decision making has the potential to accentuate cognitive biases and lead to deviations from rational decision making , even among the most well - intentioned of clinicians.2 furthermore , it is well recognized that race is a social , not a biological , construct ; as a result , the broad race categories used in medicine are heterogeneously dened and may be incongruent with genetic ancestry , particularly among minority patients.3 , 4 because cancer is inherently a disease of genetic aberration , using these race categories to make decisions in oncology may lead to the delivery of ineffective , or even detrimental , patient care . the rapid advancement of precision oncology , the use of molecular and genetic testing to tailor cancer therapies to individual patients , has uniquely positioned the eld of oncology to move beyond racebased medicine . 
since the discovery of the rst targeted therapy , imatinib , in the 1990s , over 80 targeted agents have been approved by the us food and drug administration for the treatment of numerous solid organ and hematologic malignancies.5 , 6 some of these precision oncology applications correlate with patient race . 
for instance , epidermal growth factor receptor ( egfr ) mutations in nonsmall - cell lung cancer are found in over 60% of patients of asian descent and strongly predict sensitivity to egfr tyrosine kinase inhibitors.7 , 8 similarly , several founder mutations in brca1 / 2 have been observed in multiple ethnic groups , including patients with ashkenazi jewish ancestry , and can be used to predict sensitivity to poly ( adp - ribose ) polymerase inhibitors in patients with breast , ovarian , prostate , and pancreatic cancers.9 - 14 fortunately , the tools of precision oncology enable the administration of agents such as egfr and poly ( adpribose ) polymerase inhibitors to be guided by genetic testing rather than race or ancestry . however , differential use of precision oncology has the potential to widen the very racial disparities that the eld seeks to eliminate.15 indeed , multiple studies have demonstrated decreased rates of genetic counseling , germline and somatic genetic testing , targeted therapy administration , genomic database participation , and clinical trial enrollment among minorities compared with white patients.16 - 22 there are many barriers to achieving the promise of precision oncology , including lack of access to and payment for testing , targeted treatment , and counseling . 
additionally , one major challenge is simply a lack of awareness among minority patients and clinicians.23 the rapid advancement of precision oncology has made it difcult for many clinicians to have the time and expertise to select appropriate genetic testing , interpret and apply test results , and educate patients on their implications.24 this challenge may be especially pertinent among minority - serving physicians , who have been shown to be less likely to refer to genetics and order germline testing for diseases such as breast and colorectal cancer.25 the resultant use of race as a heuristic in the setting of these time and cognitive constraints may lead to decisions that are inuenced by implicit bias , unconscious stereotypes , or attitudes toward people that inuence ones actions and behaviors . 
much like the general population , physicians have been found to have implicit bias with a preference for white over black patients and to associate race with their assessments of patient intelligence , risk - taking behavior , and adherence to medical advice.26 - 29 in turn , these perceptions have been linked to poorer communication , biased treatment recommendations , and unequal access to quality healthcare for minority patients.30 , 31 in this paper , we propose three strategies to advance health equity in precision oncology ( table 1 )  . 
ehr - based strategies to advance health equity in precision oncology ehr strategy key features default orders preselected ehr orders that are automatically applied unless a clinician actively modies them behavioral economics principle nudge decision making by taking advantage of individual status quo bias , or the tendency to favor the current state of affairs automated patient dashboards programs that harness the automation and computing power of the ehr to identify candidate patients for a given diagnostic or therapeutic intervention minimize choice overload by searching through a clinicians full patient panel to identify the subset that is eligible for precision oncology care clinician - directed clinical integration of standardized clinical pathways into the ehr for minimize choice overload by simplifying and facilitating use at the point of care complex clinical decision making use of electronic patient portals to send educational materials prime patients to initiate conversations with their clinicians about precision oncology and communicate normative feedback on its uptake among other patients about precision oncology note . 
we propose that behavioral economic principles should be leveraged to promote health equity in precision oncology as well . to steer the ehr offers a scalable , cost - effective approach to harnessing behavioral economic principles to advance health equity in precision oncology . 
defaultspreselected choices that are applied unless an individual actively changes themare powerful tools that take advantage of the status quo bias to nudge decision making while minimizing cognitive effort and preserving choice . 
this approach has been shown to optimize cancer care delivery by increasing high - value medication prescribing and reducing unnecessary daily imaging during palliative radiotherapy.36 , 37 in the precision oncology space , default orders in the ehr can be used to make direct referrals to genetics for patients who meet guideline criteria on the basis of factors such as tumor type and age , clinical characteristics that can be easily identied in the ehr . 
 advancing health equity in precision oncology decision altogether.47 - 49 the ehr is well equipped to solve the problem of choice overload through automated patient dashboards , which can efciently search through all the patients cared for by a given clinician or at a particular practice to identify a more limited pool of individuals who are eligible for a given intervention . 
this approach has been leveraged by multiple clinical trial matching programs to match patient and tumor characteristics from the ehr to study eligibility criteria , thereby enabling oncologists to identify study opportunities for individual patients . 
these programs have been effective in facilitating increased clinical trial participation not only within academic institutions but also at community oncology practices , sites that are more likely to serve minority and underserved populations.50 , 51 similar automated patient dashboards should be leveraged to identify candidate patients for other precision oncology opportunities that remain underutilized by minorities , such as genetics referrals , germline and somatic testing , targeted therapy administration , and genomic database participation . 
because this strategy matches patients to precision oncology care using the automation and computing power of the ehr rather than the heuristics of human decision making , it is likely to be more effective than individual clinicians in advancing health equity . clinical decision support systems decision support also mitigates choice overload by guiding individuals toward more desirable decisions while preserving their freedom of choice . 
in precision oncology , clinical pathways have emerged as a decision support strategy for clinicians to handle the elds ever - expanding scope and complexity.52 however , these pathways are ineffective unless they are seamlessly integrated into routine clinical practice to maximize their usefulness . 
embedding clinical decision support systems into the ehr has been shown to facilitate decision making in other areas of cancer diagnosis , treatment , and supportive care , 53 and it has been associated with decreased racial disparities in the management such as hypertension.39 this approach should also be leveraged to standardize precision oncology care for all patients , regardless of race . of nononcologic conditions perhaps an even more compelling clinician decision aid is a patients own request for a given medical intervention . 
priming , the use of subtle stimuli to activate thoughts and ideas , 54 is a powerful tool that can be directly used by patients to support clinicians in overcoming the use of race as a heuristic . 
first , we recognize that our proposed strategies do not fully combat the lack of access , nancial language barriers , and challenges , health literacy or longstanding history of mistrust in the healthcare system that have also impeded the adoption of precision oncology among minority patients . 
to be successful , ehr - based strategies informed by the principles of behavioral economics must be implemented as part of a broader , multifaceted approach that addresses all these challenges . second , the application of behavioral economics in medicine is still in its nascency , so there is a paucity of data on the impact of choice architecture redesign on subgroups within the population . 
future studies should incorporate the emerging concept of precision nudging to tailor behavioral economics interventions to specic patient populations as a strategy to ensure equal effectiveness for all . finally , the implementation of ehr - based strategies may require initial investment of nancial and human resources that is not feasible at all institutions . 
as implementation efforts get underway , we must monitor for and address any signs of differential uptake so that our proposed strategies do not inadvertently widen existing inequities in care . in conclusion , in this article , we present three ehr - based strategies that leverage the principles of behavioral economics to nudge oncologists away from the use of race as a heuristic in their decision making . 
 lau - min et al 4abramson cancer center , perelman school of medicine , university of pennsylvania , philadelphia , pa 5division of translational medicine and human genetics , department of medicine , perelman school of medicine , university of pennsylvania , philadelphia , pa 6department of radiation oncology , perelman school of medicine , university of pennsylvania , philadelphia , pa 7department of medical ethics and health policy , perelman school of medicine , university of pennsylvania , philadelphia , pa otherwise noted . 
guerra leadership : freenome , guardant health , genentech stock and other ownership interests : crispr therapeutics , beam therapeutics , intellia therapeutics , editas medicine honoraria : lundbeck ( i ) consulting or advisory role : bristol - myers squibb ( i ) speakers bureau : janssen , pzer ( i ) research funding : bristol - myers squibb ( inst ) travel , accommodations , expenses : lundbeck , janssen ( i ) uncompensated relationships : tapestry networks justin e . 
bekelman honoraria : unitedhealthcare , national comprehensive cancer network , cvs health , optum , american journal of managed care research funding : pzer , united health group , north carolina blue cross blue shield , embedded healthcare no other potential conicts of interest were reported . acknowledgment we thank mitesh patel , md , mba , and callie scott , msc , both at the university of pennsylvania , for their helpful comments during the writing of this manuscript . 
new york , farrar , straus and giroux , 2011 zhang f , finkelstein j : inconsistency in race and ethnic classication in pharmacogenetics studies and its potential clinical implications . 
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 systemic and cns activity of selective ret inhibition with selpercatinib ( loxo - 292 ) in a patient with ret - mutant medullary thyroid cancer with extensive cns metastases alexander andreev - drakhlin , md1 ; maria cabanillas , md1 ; behrang amini , md , phd1 ; and vivek subbiah , md1 introduction medullary thyroid cancer ( mtc ) is a neuroendocrine tumor that originates from the parafollicular cells ( or c cells ) of the thyroid gland and accounts for 1% to 2% of thyroid cancers in the united states.1 the cns is a rare site of metastasis in mtc , with , 15 cases reported in the medical literature ; however , the prevalence may be underreported because of the infrequent use of cns imaging in patients with mtc.1 , 2 the optimal treatment approach for patients with mtc with cns involvement is currently unknown . 
although surgical resection , radiation therapy , or stereotactic radiosurgery ( srs ) may improve local disease control in some patients , most still succumb to their disease within months after the diagnosis of cns metastases.1 - 4 the proto - oncogene ret ( rearranged during transfection ) , located on chromosome 10q11.2 , is central to development of a majority of cases of mtc.5 germline gain - of - function ret point mutations result in multiple endocrine neoplasia 2 , a hereditary syndrome associated with mtc and pheochromacytoma.6 , 7 similar somatic mutations occur in approximately 50% of sporadic mtc , approximately 20% of sporadic pheochromocytomas , and rarely in other cancer types.8 - 10 recent identication of highly potent and selective ret inhibitors holds great promise in the management of these ret - driven cancers as well as other ret - altered malignancies.11 - 14 in 2018 , selpercatinib ( loxo - 292 ) received us food and drug administration breakthrough therapy designation for treatment of patients with previously treated metastatic ret - mutant mtc , ret fusion - positive nonsmall - cell lung cancer , and ret fusionpositive thyroid cancers . 
durable intracranial responses with selpercatinib have been described in patients with brain metastases with ret fusionpositive lung and thyroid cancers.15 , 17 however , the activity of selpercatinib in patients with ret - mutant mtc with brain metastases and / or leptomeningeal disease ( lmd ) has not been characterized , to our knowledge . 
here , we describe a patient with ret m918tmutant mtc with extensive cns metastases who had a clinically meaningful durable response to selective ret inhibition with selpercatinib . case report total a 67 - year - old woman presented to a local hospital with bilateral neck swelling . 
positron emission tomography imaging showed metabolically active , left - side , level v lymph nodes ; a 1.1 - cm , hypermetabolic , right lower lobe lung nodule ; several hypermetabolic liver lesions ; as well as lytic lesions in the c5 vertebral body , l4 left lamina , and left posterior iliac wing . 
magnetic resonance imaging ( mri ) of the brain revealed a 4 - mm lesion in the right caudate nucleus . the patient presented to the university of texas md anderson cancer center for a second opinion . 
she was then treated with standard - of - care cabozantinib but experienced multiple adverse effects , including handand - foot syndrome , mucositis , weight loss , nausea , and diarrhea , requiring several dose reductions ultimately to 40 mg daily . 
 ( a ) magnetic resonance imaging ( mri ) oblique axial cerebellar images of the patients metastatic brain disease ( left panel ) before and ( right panel ) 8 weeks after the patient initiated treatment with selpercatinib . 
 ( c ) mri axial cerebellar and ( d ) sagittal thoracic spine images of the patients metastatic disease ( left panels ) before and ( right panels ) 33 weeks after the patient initiated treatment with selpercatinib . 
 ( e ) mri axial brain images demonstrating a new caudate lesion after 17 months of therapy with selpercatinib ( left panel ) before and ( right panel ) after stereotactic radiosurgery ( srs )  . 
 andreev - drakhlin et al given the absence of any remaining standard therapies with established benet , the patient enrolled in a phase i / ii study of selpercatinib in patients with advanced solid tumors ( libretto - 001 ; clinicaltrials.gov identier : nct03157128 )  . the patient provided written informed consent before enrollment . 
baseline imaging at the time of the treatment initiation with selpercatinib revealed bilateral central and lateral neck disease ; lytic lesions in the c5 , t4 , t8 , l1 vertebrae and left posterior hilum ; , nodular opacities in bilateral lungs ; interlobular septal thickening suspicious for lymphangitic carcinomatosis ; numerous hepatic lesions ( largest , 7 cm in the dome of liver ) ; 25 lesions in the brain and cerebellum ( largest , 7 mm in the left cerebellar hemisphere ; fig 2a and 1c , left panels ) , and a 5 - mm leptomeningeal nodule at the level of t11 ( fig 2d , left panel )  . calcitonin and cea levels measured 2 , 180 pg / ml and 12 , 312 ng / ml , respectively ( fig 2b )  . the patient experienced clinical response within the rst month of therapy , with resolution of baseline diarrhea and nausea , and with appetite improvement . 
at 17 months , an mri of the brain showed an isolated , new , 5 - mm left caudate lesion that was treated with srs ( fig 2e , left and right panels ) with continuation of selpercatinib . 
at 20 months , imaging revealed non - cns multifocal progression with a new 6 - mm bony lesion in the c7 vertebral body , as well as several new , right - side liver lobe lesions ( the largest measured 2 cm )  . 
the patients calcitonin level rose to 235.9 pg / ml ; her cea level remained unchanged . peripheral blood cell - free dna analysis at the time of systemic progression revealed only the presence of the previously identied ret m918t missense mutation . 
the patient declined a liver biopsy . cns disease remained in response until 22 months , when several new brain lesions were found to have developed ; these were managed with srs ( fig 2 )  . 
her treatment course has been complicated by several hospitalizations unrelated to selpercatinib . discussion metastatic dissemination of mtc to the cns is a rare but devastating complication associated with poor prognosis and no well - established treatment strategies.1 although limited evidence from previous reports suggests that surgical resection and / or radiation therapy may be used in select cases , there remains a strong need for novel treatment modalities with durable therapeutic responses.1 - 3 cns efcacy of multikinase inhibitors such as vandetanib or cabozantinib has not been reported in mtc . here , we present a report of successful treatment of the brain and leptomeningeal metastases with systemic therapy in a patient with ret - mutated mtc , using the purpose - built selective and cns - penetrant ret inhibitor selpercatinib . 
treatment with this agent resulted in complete and durable resolution of the measurable brain and leptomeningeal lesions in a patient with previous disease progression while she received cabozantinib and radiation therapy . 
 case report notably , the patients tumor harbored a heterozygous deletion in the cdkn2c gene linked to an aggressive disease phenotype in mtc.19 cdkn2c is a member of the ink4 family of cyclin - dependent kinase inhibitors that block the cell cycle progression in the g1 phase through interaction with cyclin - dependent kinases 4 and 6.19 cdkn2c is lost in approximately 40% to 50% mtcs and is associated with a signicantly shorter time to distant metastasis and decreased overall survival in mtc , an effect further enhanced by concomitant ret m918t mutation.19 , 21 in addition , an earlier report showed that cdkn2c haploinsufciency is associated with a strong trend toward reduced progressionin ret - mutated mtc treated with systemic free survival therapy.21 however , this relationship has not been studied in patients receiving selective ret inhibitors , to our knowledge , and the signicance of cdkn2c loss in this setting remains to be determined . the patient is continuing selpercatinib therapy , with gradual disease progression in the liver . 
a recent study demonstrated that ret solvent - front mutations ( ret g810s / g810r / g810c ) can cause on - target resistance to selective and multikinase ret inhibitors.22 a better understanding of mechanisms of acquired resistance to selective ret inhibitors and frequency of resistant alterations would guide the development of novel agents and combination therapies directed towards further improvement of treatment outcomes for patients with ret - altered malignancies . in conclusion , we observed a radiographically conrmed durable response with selpercatinib in a patient with a heavily pretreated ret m918tmutated mtc with extensive cns metastases . 
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nature 367 : 375 - 376 , 1994 elisei r , cosci b , romei c , et al : prognostic signicance of somatic ret oncogene mutations in sporadic medullary thyroid cancer : a 10 - year follow - up study . j clin endocrinol metab 93 : 682 - 687 , 2008 beldjord c , desclaux - arramond f , rafn - sanson m , et al : the ret protooncogene in sporadic pheochromocytomas : frequent men 2 - like mutations and new molecular defects . 
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the patient subsequently underwent neoadjuvant radiation in addition to receiving weekly carboplatin and paclitaxel , followed by esophagogastrectomy.7 pathology revealed moderately differentiated adenocarcinoma invading the adventitia ( pt3 ) , but none of the 14 lymph nodes were involved ( pn0 )  . 
one and a half years after resection , surveillance imaging revealed new concerning hypodensity in the liver , accompanied by an increase in the carcinoembryonic antigen ( cea ) levels . 
next - generation sequencing ( ngs ) was performed on biopsies from the time of initial and recurrent liver metastasis using the commercially available comprehensive genomic proling ( cgp ) assay from foundation medicine ( cambridge , ma ; table 1 )  . 
serial blood collections were also obtained to determine the presence of ctdna using a tumorinformed multiplex polymerase chain reaction - ngs assay from natera ( san carlos , ca ) designed from tumor genomic alterations ( table 1 )  . 
at the time of disease recurrence in the liver , the tumor - informed assay with an established analytical sensitivity5 revealed elevated levels of ctdna , measured in mean tumor molecules / ml of plasma ( fig 1 )  . the patient underwent the patient approximately 760 days postdiagnosis , received 6 cycles ( c6 ) of uorouracil ( fu ) , leucovorin , and oxaliplatin ( mfolfox6 ) , with radiographic response in the liver lesion . 
after another year ( approximately 1 , 490 days postdiagnosis ) , the patient developed a new fdgavid mass in the ablation cavity , accompanied by an increase in cea level . 
the patient received 1 cycle ( c1 ) of fu and leucovorin ( fu / lv ; approximately 1 , 520 days postdiagnosis ) , complicated by oral mucositis , followed by resection of the liver mass ( approximately 1 , 580 days postdiagnosis ) , and pathologically conrmed to be metastatic eac . 
after metastasectomy , surveillance imaging showed no evidence of recurrence , ctdna levels became negative , and the patient remains in remission , currently 11 months ( approximately 320 days ) postmetastasectomy . 
the use of more sensitive cancer detection methods may help optimize treatment approaches ( escalation or de - escalation of therapies ) in the localized setting . in this case study , the patient experienced oligometastatic recurrence despite aggressive trimodality therapy . 
although we were unable to assess ctdna in the localized setting for this patient , a recent study investigated ctdna in the context of neoadjuvant chemoradiation for localized esophageal cancer and showed that detectable ctdna levels postchemoradiation , along with metabolic imaging analysis , predicted tumor progression with 100% sensitivity versus ctdna alone ( 71% ) and imaging alone ( 57% ) .15 thus , detectable , ctdna could help clarify ambiguous ndings ( as observed in this case study ) and could help identify high - risk patients with mrd who could be upper limit of normal cea 1 , 000 0.01 1 , 370 1 , 523 1 , 677 1 , 826 1 , 219 time since diagnosis ( days ) 1 , 066 no evidence of disease or disease response ctdna - positive ( mtm / ml ) liver metastasis suspicious finding , subsequently resolved or stable ctdna - negative ( mtm / ml ) mfolfox6 suspicious finding , subsequently confirmed cea ( ng / ml ) fluorouracil / leucovorin fig 1 . 
another study evaluated prognosis based on the presence of detectable ctdna after neoadjuvant chemotherapy prior to cystectomy in patients with bladder cancer.3 the preoperative ctdna status was 100% sensitive in predicting pathologic complete response , suggesting that trials could strategize testdeferred surgery in patients with undetectable ctdna postneoadjuvant therapy . in this case study , the initial plan was to proceed with chemotherapy ( mfolfox6 ) , followed by metastasectomy for removal of any residual disease ; however , the latter was delayed because of the ambiguous ndings that showed enlarged pulmonary / soft tissue nodules ( table 2 ; fig 1 ) , requiring further follow - up . 
retrospectively , serial ctdna analysis suggested that chemotherapy was more effective than rfa in reducing the tumor burden , and thus , consideration of consolidation metastasectomy in lieu ofor soon afterrfa could have prevented the second local recurrence . 
 ( * ) brd4 and smad4 have 3 missing data points between september 2017 and june 2018 . mfolfox6 , 6 cycles of uorouracil , leucovorin , and oxaliplatin . this case study illustrates the potential advantage of using ctdna as a conrmatory , adjunctive surveillance tool . 
the early and continued increase in ctdna post - rfa showed the sensitivity and specicity of the ctdna assay in predicting disease recurrence by a lead time of 174 days compared with cea and 350 days before radiographic conrmation . 
cea is known to be a lagging indicator of disease and is relatively insensitive , nonspecic , and can be confounded by acute or chronic inammation , smoking , liver disease , and diabetesall common comorbidities in this patient population.16 in this particular case , the multiple postresection complications confounded the interpretation of an increase in cea , an increase that ultimately attenuated and has not translated into relapse by imaging or ctdna with 11 months of follow - up . 
this could be a faster and more accurate measure than following the standard approach of using radiographic progression - free survival alone . it is important to note that the tumor - informed ctdna assay is a personalized method that requires separate whole - exome sequencing of the tumor tissue to develop patient - specic primers . 
the customized design of this assay targeting a set of clonal mutations known to be present in the specic tumor leads to its high sensitivity and specicity ; it is not intended to be a discovery assay for assessment of actionable genomic targets , but rather , a tool for detecting mrd . 
it was notable to observe that genomic alterations in the primary tumor were detectable with the tumor - informed ctdna assay at the time of relapse , and they all appeared to track in parallel ( fig 2 )  . 
we did not observe evidence of signicant selection for or against clones harboring any of the genomic targets tested during treatment , but we cannot rule out the acquisition of additional subclonal genomic alterations . our study has certain limitations . 
another aspect is how often and how long a patient should be monitored in this setting . although tumor burden may be undetectable by the ctdna assay , the patient is still at risk and needs surveillance . however , given the features described , it is reasonable to test this assays utility in multiple disease settings as part of clinical trials in esophageal and other cancers . 
einstein research funding : trovagene ( inst ) , bristol - myers squibb ( inst ) nathan liang employment : natera stock and other ownership interests : natera meenakshi malhotra employment : natera stock and other ownership interests : natera alexey aleshin employment : natera stock and other ownership interests : natera consulting or advisory role : mission bio solomon moshkevich employment : natera , evidation health ( i ) stock and other ownership interests : natera patents , royalties , other intellectual property : named as inventor on a patent led by natera travel , accommodations , expenses : natera paul r . 
billings employment : natera leadership : trovagene , biological dynamics , omniseq , alveo biotechnologies stock and other ownership interests : natera , trovagene , biological dynamics , omniseq , alveo biotechnologies consulting or advisory role : bethesda group , guidepoint global eirini pectasides consulting or advisory role : clovis oncology research funding : bristol - myers squibb no other potential conicts of interest were reported . references shah m , denlinger cs : optimal post - treatment surveillance in cancer survivors : is more really better ? oncology ( williston park ) 29 : 230 - 240 , 2015 2 . 
natl j maxillofac surg 7 : 17 - 20 , 2016 christensen e , birkenkamp - demtr oder k , sethi h , et al : early detection of metastatic relapse and monitoring of therapeutic efcacy by ultra - deep sequencing of plasma cell - free dna in patients with urothelial bladder carcinoma . 
j clin oncol 37 : 1547 - 1557 , 2019 abbosh c , birkbak nj , wilson ga , et al : phylogenetic ctdna analysis depicts early - stage lung cancer evolution . 
nature 545 : 446 - 451 , 2017 [ erratum : nature 554 : 264 , 2018 ] coombes c , page k , salari r , et al : personalized detection of circulating tumor dna antedates breast cancer metastatic recurrence . 
clin cancer res 25 : 14255 - 4263 , 2019 reinert t , henriksen tv , christensen e , et al : analysis of plasma cell - free dna by ultradeep sequencing in patients with stages i to iii colorectal cancer . 
jama oncol 5 : 1124 - 1131 , 2019 shapiro j , van lanschot jjb , hulshof mccm , et al : neoadjuvant chemoradiotherapy plus surgery versus surgery alone for oesophageal or junctional cancer ( cross ) : long - term results of a randomised controlled trial . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
arch pathol lab med 142 : 1242 - 1253 , 2018 araujo dv , bratman sv , siu ll : designing circulating tumor dna - based interventional clinical trials in oncology . 
bray f , ferlay j , soerjomataram i , et al : global cancer statistics 2018 : globocan estimates of incidence and mortality worldwide for 36 cancers in 185 countries . 
hagerty2 ; and amanda gammon , ms1 , 2 purpose to compare the classication of genetic variants reported on tumor genomic proling ( tgp ) reports with germline classications on clinical test results and clinvar . 
somatic variant interpretations were compared with classications from germline test results as well as with clinvar interpretations . results of the 623 variants identied on tgp , 353 had a denitive classication in clinvar , and 103 were assayed with a germline test , with 66 of the variants tested observed in germline . 
analysis of somatic variants of uncertain signicance listed on tgp reports determined that 22% had a different interpretation compared with clinvar and that 32% differed from the interpretation on a germline test result . 
pathogenic variants on tgp test results were found to differ 13% and 5% of the time compared with clinvar interpretations and germline test results , respectively . conclusion these results suggest that tgp variants are often classied differently in a germline context . differences may be due to different processes in variant interpretation between somatic and germline laboratories . 
2019 by american society of clinical oncology introduction tumor genomic proling ( tgp ) is the application of next - generation sequencing to tumor samples for the purpose of targeted cancer treatment.1 tgp can aid in informing clinicians of treatment options because it allows for the identication of molecular targets for clinical trials or nonconventional therapy options . 
for example , tumors with a brca1 or brca2 pathogenic variant are more likely to respond to pharmaceuticals , like poly ( adp - ribose ) polymerase inhibitors , so the identication of one of these variants on tgp can lead to a different treatment option.2 , 3 other pharmaceuticals have been shown to be effective in tumors with defective mismatch repair.4 in contrast , germline genetic testing analyzes blood or saliva samples for genes associated with hereditary cancer predisposition syndromes . 
tgp and germline tests overlap in their analysis of hereditary cancer genes , and variants identied in a tumor on tgp may also be present in the germline.5 , 6 studies have shown that between 3% and 16% of tgp samples carry a pathogenic germline variant.7 , 8 asco recommends that physicians communicate incidental germline ndings to patients , which may lead to secondary germline analysis.1 thus , germline variants may inform treatment , and somatic variants may inform germline testing . 
given this overlap , it is crucial to consider classication of the variants because they may differ depending on the test type . tgp and germline testing have different purposes and indications as well as different recommended guidelines for variant interpretation . 
 moody et al context key objective are differences in variant interpretation between somatic and germline cancer genetic testing observed in a clinical setting ? knowledge generated both pathogenic mutations and variants of uncertain signicance found on somatic tumor testing have different classications when considered in a germline context . 
variants of uncertain signicance found on somatic tumor testing are more likely to have a different classication in germline than in pathogenic mutations . relevance health care providers may carefully consider both pathogenic and uncertain ndings on somatic tumor testing when they are found in genes that have germline relevance . 
these genes were selected on the basis of the wellestablished cancer risks and clear management recommendations associated with germline pathogenic variants as illustrated in current national comprehensive cancer network guidelines.9 , 10 variants were excluded if a specic nucleotide change was not reported for the variant , such as for whole - exon rearrangements or full gene loss , because these variants are less likely to be present in germline and often follow a different classication schema . 
study protocols with regard to patient data were subject to institutional review board approval ( university of utah )  . comparison with clinvar classications clinvar is a public archive of genetic variation that facilitates comparisons of variant classications between laboratories and research initiatives . 
classication categories in clinvar are consistent with those listed in the american college of medical genetics recommendations11 and include benign , likely benign , variant of uncertain signicance ( vus ) , likely pathogenic , and pathogenic . 
this facilitated an easier comparison with somatic classications since the tgp results only listed variants as pathogenic or uncertadifferences in classication between tumor and germline testing were considered clinically signicant if medical management recommendations would be made on the basis of one classication but not the other . 
a variant that is vus on one result and benign on another would not be clinically signicant . comparison with germline classications a subset of patients who had tgp also underwent germline testing within the study time frame . 
when results did not indicate any variant and were considered negative , germline testing laboratories were contacted to determine whether the somatic variant found on tgp was present in the germline and to determine its classication at the time of testing . 
variants were identied in 31 different tumor types , the majority of which were found in brain ( 19% ) , colorectal ( 15% ) , and prostate ( 13% ) tumors . 
frameshifts , nonsense , and in - frame insertions / deletions made up , 3% of the remaining vus variants , and no vus splice variants were seen ( fig 1 )  . somatic classications compared with clinvar of the 623 somatic variants found on tgp , 353 ( 56.7% ) had a denitive germline classication in clinvar . 
the majority of these somatic vuss were also classied as vuss in clinvar ( 203 of 260 ; 78.1% ) , while 48 somatic vus variants ( 18.5% ) were classied as benign and nine ( 3.5% ) as pathogenic in clinvar ( fig 2 )  . the additional 93 somatic variants analyzed in clinvar were classied as pathogenic on the tgp test result . 
of these differences , 30.4% ( 21 of 69 ) would result in different management recommendations and so are considered to have a clinically signicant difference in interpretation for this study ( table 1 )  . somatic classications compared with classications on germline test results of the 623 somatic variants assessed , 103 ( 16.4% ) were assayed using a germline test , and 66 ( 64% ) were observed in germline . 
the majority of these somatic vuss were also classied as vuss in the germline test results ( 32 of 47 ; 68.1% ) , while 12 ( 25.5% ) were classied as benign and three ( 6.4% ) as pathogenic in the germline test results . 
comparison of pathogenic tgp variants with the germline test results found that 18 ( 94.7% ) of 19 were also reported as pathogenic in the germline and only one ( 5.3% ) was classied as vus in the germline ( fig 2 )  . 
clinically signicant differences in interpretation were seen with four ( 25% ) of 16 variants ( table 2 )  . we assessed how many of the germline test results were returned after somatic test results were obtained to investigate the impact of tgp variant classication on clinic ow . 
the majority of patients had at least one pathogenic somatic mutation . however , when the patients who had germline testing after somatic testing were subdivided by length of time , those who had germline testing  . 
90 days after somatic testing were more likely to have solely a vus somatic result , which suggests that patients in this data set were not referred for germline testing on the basis of a vus found on tgp . discussion the results of this study demonstrate distinct differences in the interpretation of variants found in tgp test results compared with clinvar and clinical germline test results . specically , 23% and 32% of somatic variants classied as vus and 13% and 5% of somatic variants classied as pathogenic on tgp had a different interpretation in clinvar and germline test results , respectively . 
the tgp report suggests that the variant is not associated with targeted cancer therapy , and thus , no this result . action was recommended on the basis of however , a germline result that shows a pathogenic mutation in mlh1 does warrant changes to medical management recommendations because this patient would meet national comprehensive cancer network criteria for a diagnosis of lynch syndrome and increased cancer screening , and consideration of risk - reducing surgeries associated with mlh1 pathogenic variants would be indicated.10 in addition , these germline test results indicate that this patients family members also may have signicant cancer risks , and genetic testing may now be indicated for them if it was not previously . 
if germline testing had not been pursued after reviewing the tgp results , this important risks to information about additional cancer the patient and his or her family would not have been realized , which highlights the importance of providers understanding differences in germline and somatic variant interpretation . 
these results show that clinvar is a source of information for tgp variants that may have different interpretations in germline . tgp and germline genetic tests have different indications and outcomes and , as such , have different published variant interpretation guidelines . 
thus , discrepancies in classications of specic variants between tgp and germline laboratories do not necessarily indicate that one classication is incorrect : the tests are being used for different purposes , and the classication models used reect this difference . 
clinvar listed this variant as benign , and no submitter referenced the variant being found in a tumor . this demonstrates the utility of somatic variant databases in the classication of variants found in tgp and highlights how using uniquely somatic sources of evidence can lead to a different classication than in germline . in contrast , the purpose of a germline genetic test is to diagnose hereditary cancer predisposition syndromes and aid in the prediction of the risk of cancer in a patient . professional guidelines published in 2015 by the american college of medical genetics and genomics and the association for molecular pathology list sources of evidence unique to germline interpretation.11 these include segregation information , in trans and de novo ndings , and patient phenotype data . 
these guidelines also include many sources of information that are similarly listed in somatic classication guidelines , such as mutation type , minor allele frequency , germline variant databases , published functional and population studies , and in silico prediction tools ( fig 3 )  . 
these lines of evidence are not currently used in somatic variant classication , which may lead to differing classications for this variant . it is possible that the difference in variant interpretation guidelines between somatic and germline do not account for all of the differences in interpretation found in this study . disagreement with regard to variant interpretation in a strictly germline context has been previously demonstrated.14 - 17 disagreement between germline testing laboratories has been reported to be as high as 26%15 and disagreement between germline databases as  . 
30%.16 in a study where four germline laboratories agreed to share internal data and discuss their interpretation rationales , there was still a 13% difference in interpretation because of variation in interpreting guidelines.17 the rates of disagreement found in the literature are consistent with the ndings of the current study . 
the subjective nature of guideline interpretation previously demonstrated in germline variant classication may also contribute to the differences seen in this study between somatic and germline variant interpretation . another known difculty in variant interpretation is classifying missense variants . 
the gathering of data to help to classify missense vuss is difcult for both somatic and germline classications and may further contribute to the differences seen in this study . this study had some limitations . it was performed at a single center and included tgp results from a single commercial laboratory . 
in addition , the majority of the tgp test results were gathered before the publication of the somatic variant interpretation guidelines.12 updated classications could not be obtained from the tgp testing identied the somatic mutations in this laboratory that study , and it is unclear whether the interpretations of the variants reported in this study are now different on the basis of these guidelines . 
additional research is required to determine whether the rate of difference found in this study is generalizable to a wider patient population . family history , referral in conclusion , although literature has been published on variant interpretation in both the somatic and the germline context , none has compared variant interpretations between the two methods . 
we found that somatic vus reported on a tgp test have a different interpretation in 57 ( 22% ) of 260 cases compared with clinvar and in 15 ( 32% ) of 47 cases compared with germline test results . 
pathogenic mutations from tgp test results were found to have a different interpretation in 12 ( 13% ) of 93 variants compared with clinvar and in one ( 5% ) of 19 variants compared with germline test results . understanding the observed differences in variant classications as well as the philosophies behind somatic and germline variant interpretation may inform clinicians as they order germline testing for patients . 
moody , jennie vagher , whitney espinel , david goldgar , amanda gammon administrative support : amanda gammon provision of study material or patients : jennie vagher , whitney espinel , amanda gammon collection and assembly of data : emily w . 
 moody et al open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . jennie vagher consulting or advisory role : erin mundt , cgc no other potential conicts of interest were reported . acknowledgment this article is based on a research project conducted by e.w.m. 
we thank the university of utah graduate program in genetic counseling . references robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . j clin oncol 33 : 3660 - 3667 , 2015 2 . 
mccabe n , turner nc , lord cj , et al : deciency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
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lancet 376 : 235 - 244 , 2010 le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 jain r , savage mj , forman ad , et al : the relevance of hereditary cancer risks to precision oncology : what should providers consider when conducting tumor genomic proling ? j natl compr canc netw 14 : 795 - 806 , 2016 6 . 
hall mj , daly mb , ross ea , et al : germline variants in cancer risk genes detected by ngs - based comprehensive tumor genomic proling ( cgp )  . 
j clin oncol oncol 27 : 795 - 800 , 2016 33 , 2015 ( suppl ; abstr 11084 ) schrader ka , cheng dt , joseph v , et al : germline variants in targeted tumor sequencing using matched normal dna . 
jama oncol 2 : 104 - 111 , 2016 [ erratum : jama oncol 2 : 279 , 2016 ] daly mb , pilarski r , berry mp , et al : genetic / familial high - risk assessment : breast and ovarian , 2019 . 
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 exceptional response to akt inhibition in patients with breast cancer and germline pten mutations belinda kingston , mbchb1 ; caroline bailleux , md2 ; suzette delaloge , md , msc2 ; gaia schiavon , md , phd3 ; veronique scott , phd2 ; magali lacroix - triki , md , phd2 ; t . 
hedley carr , phd3 ; iwanka kozarewa , phd3 ; heidrun gevensleben , md4 ; zoe kemp , phd5 ; alex pearson , phd1 ; nicholas turner , md , phd1 , 5 ; and fabrice andr e , md , phd2 introduction cowden syndrome is an autosomal dominant genetic disease with an estimated incidence of one in 200 , 000 . 
pip3 functions as a secondary messenger in the pi3k pathway that binds and activates proteins that have a pleckstrin homology domain , such as akt1 , and triggers their activation and localization to the plasma membrane , promoting cellular proliferation and survival.4 germline pten loss - of - function mutations may result in dominant akt activation as a driving oncogenic event in cowden - related breast tumors.5 preclinical evidence suggests that cancers with akt activation have increased sensitivity to akt inhibition.6 preliminary clinical evidence is derived from phase i and ii trials in patients with breast cancers bearing somatic mutations in the pi3k / akt / mtor pathway.7 - 11 inhibitor of all three isoforms of capivasertib ( azd5363 , astrazeneca ) is a potent and selective oral serine / threonine kinase akt ( ie , akt1 , 2 , 3 ) and has preclinical evidence of efcacy as monotherapy or in combination with cytotoxic and targeted therapies.12 - 15 despite the encouraging progression - free survival observed with capivasertib monotherapy in heavily pretreated patients with akt1 e17kmutant breast and gynecologic cancers , 9 recist response rates in phase i studies only reached 22% ( table 1 ) .8 , 9 , 16 because pten loss activates akt1 , we hypothesized that tumors from patients with cowden syndrome could be sensitive to this drug family . which was estrogen ( er ) and progesterone receptor negative , human epidermal growth factor receptor 2 ( her2 ) negative , and was designated grade iii invasive carcinoma of no special type ( nst )  . 
the patient received six cycles of neoadjuvant cyclophosphamide 600 mg / m2 , epirubicin 75 mg / m2 , and docetaxel 100 mg / m2 before a mastectomy with left axillary lymph node dissection ( revealing residual disease in 10 of 18 lymph nodes ) and adjuvant radiotherapy . eight months later , the patient experienced relapse with cutaneous disease and thoracic nodal volvement . 
after enrolling in safir02 ( clinicaltrials.gov identier : nct02299999 ) , targeted panel sequencing ( ion torrent pgm ; thermo fisher scientic , villebon , france ) of a fresh tumor biopsy sample revealed the presence of a heterozygous germline pten mutation ( c.389g.a , rs121909229 ) alongside other variants ( fig 1a ; data supplement )  . 
in the context of safir02 , the patient was randomly assigned to maintenance targeted therapy and received capivasertib 480 mg twice per day , 4 days on and 3 days off . 
on the right side , she presented with a t3 , erpositive and progesterone receptorpositive , her2negative , grade ii invasive carcinoma nst with 20 of 23 involved lymph nodes . 
in may 2010 , the patient received six cycles of chemotherapy every 3 weeks ( uorouracil 600 mg / m2 , epirubicin 75 mg / m2 , and cyclophosphamide 600 mg / m2 ) before starting maintenance tamoxifen . 
she received eight cycles of paclitaxel ( 90 mg / m2 on days 1 , 8 , and 15 of a 28 - day cycle ) combined with capivasertib ( 360 mg twice per day on days 2 - 5 , 9 - 12 , and 16 - 18 of each 28 - day in june 2013 , a computed tomography scan cycle )  . showed a complete response of the liver metastases . 
she had a conrmed maintained response in may 2014 until progression occurred in june 2014a progression - free survival of 19 monthsand a maintained complete response for 12 months on capivasertib alone ( fig 2c )  . 
plasma circulating tumor dna analysis from baseline and progression time points during the beech study showed no major changes ( data supplement )  . discussion the akt inhibitor capivasertib has been examined in early - phase trials ( table 1 ) , and no complete responses have been noted , yet both patients with cowden syndrome presented here had durable complete responses to capivasertib . 
cdc14 , phosphatase domaillustration from ( b ) immunohistochemistry demonstrating ( i ) absent pten staining in the tumor and ( ii ) cytoplasmic and membranous expression of pakt in the 40% of tumor cells . 
cdc14 , phosphatase domaillustration from ( b ) pten immunohistochemistry from ( i ) control tissue and ( ii ) noncancerous and ( iii and iv ) tumor - containing lymph node . 
 ( c ) computed tomography ( ct ) scans during the patients time on capivasertib , with white arrows indicating disease in the liver : ( i ) october 2012 , baseline ct demonstrating a liver deposit ; ( ii ) january 2013 , ct following two cycles of paclitaxel and capivasertib ; ( iii ) ct demonstrating continued complete response on maintenance capivasertib 7 months after cessation of paclitaxel ; and ( iv ) may 2014 , nal ct before progression june 2014 . nonmalignant cells carrying a germline pten mutation to pi3k - pathway inhibition . 
similar to the cases presented here , no severe toxicity was noted in the pilot study , 21 with just one patient experiencing a grade 3 adverse event ( hypophosphatemia / hypercholesterolemia )  . in recent years , drugs targeting the pi3k / akt / mtor pathway have been developed . 
in contrast , akt inhibitors in combination with paclitaxel have been shown to be more active in patients with triple - negative breast cancers harboring a pik3ca / pten / akt1 pathway alteration.7 , 10 similarly , pi3k inhibitors have demonstrated activity in patients with pik3ca mutations.22 , 23 of note in case 2 is the presence of the second - hit pten stop - gain mutation y88x , present with an af of 25.5%. however , the presence of a tp53 mutation at an af of 51.9% indicates that this second - hit mutation is subclonal rather than a truncal driver mutation . 
explanations for the pten phenotype in case 1 include undetected loh , pten promotor hypermethylation , 24 , 25 complex pten genomic rearrangements , 26 and post - translational modication.27 contrary to the two - hit model by knudson et al28 of tumorigenesis in tumor suppressor genes , pten aberrations appear to be protumorigenic in the absence of a second hit . in 2010 , alimonti et al29 demonstrated that pten hypermorphic mice ( with 80% of the normal pten protein level ) had a greater propensity to tumorigenesis than mice with two functional alleles but were less tumorigenic than pten heterozygous mice , supporting a haploinsufciency model of tumorigenesis in pten aberrations . a later in vivo study of pten knock - in mouse models suggested that the conformation of pten underlies the dominant - negative behavior of pten heterozygous mutants . 
this supports the rationale that pten heterozygous mutants act in a dominant - negative manner to promote tumorigenesis . the patients in the cases presented here were treated with combination chemotherapy and capivasertib followed by capivasertib monotherapy . 
the patient in case 1 had previously demonstrated tumor resistance to taxane therapy , with residual disease after neoadjuvant chemotherapy and a short progression - free survival after treatment of primary breast cancer . 
the second patient achieved a complete response with the combination of paclitaxel and capivasertib and maintained this complete response for a period of 12 months on capivasertib alone , suggesting that capivasertib was highly active in this patient . in summary , these two patients with breast cancer and different germline pten mutations both showed a dramatic response to capivasertib superior to that seen in early trials of the drug . 
 magali lacroix - triki leadership : mypl stock and other ownership interests : mypl honoraria : myriad genetics , genomic health consulting or advisory role : roche travel , accommodations , expenses : agendia t . 
hedley carr employment : astrazeneca stock and other ownership interests : astrazeneca iwanka kozarewa employment : astrazeneca stock and other ownership interests : astrazeneca kingston et al zoe kemp honoraria : lilly honoraria : astrazeneca nicholas turner consulting or advisory role : roche , novartis , astrazeneca , pzer , bicycle therapeutics , bristol - myers squibb , merck sharp & dohme , tesaro , lilly research funding : pzer ( inst ) , roche ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , bio - rad ( inst ) , guardant health ( inst ) fabrice andr e research funding : astrazeneca ( inst ) , novartis ( inst ) , pzer ( inst ) , lilly ( inst ) , roche ( inst ) , daiichi ( inst ) travel , accommodations , expenses : novartis , roche , glaxosmithkline , astrazeneca no other potential conicts of interest were reported . references tan mh , mester jl , ngeow j , et al : lifetime cancer risks in individuals with germline pten mutations . 
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baselga j , dent sf , cort es j , et al : phase iii study of taselisib ( gdc - 0032 ) + fulvestrant ( fulv ) v fulv in patients ( pts ) with estrogen receptor ( er ) - positive , pik3ca - mutant ( mut ) , locally advanced or metastatic breast cancer ( mbc ) : primary analysis from sandpiper . 
thall , phd1 purpose despite the fact that almost any sample of patients with a particular disease is heterogeneous , most clinical trial designs ignore the possibility that treatment or dose effects may differ between prognostic or biologically dened subgroups . 
the purpose is to illustrate the benets of accounting prospectively for treatment - subgroup interactions and how utilities may be used to quantify risk - benet trade - offs . methods two bayesian clinical trial designs that perform subgroup - specic decision making and inference based on elicited utilities of patient outcomes are reviewed . 
the second is a sequentially adaptive trial of natural killer cells for treating hematologic malignancies that is based on ve time - to - event outcomes and that performs safety monitoring and optimizes cell dose within six disease subgroups . 
similarly , qualitatively different disease subtypes or biologically dened subgroups typically are ignored by the decision rules and hypotheses of conventional trial designs , aside from possibly stratifying on subgroups when randomly assigning patients . 
this problem persists in all phases of conventional trial designs , from early - phase dose - nding to randomized comparative trials . to illustrate the problem , consider a prospective randomized trial in patients with relapsed or refractory leukemia , with the aim of evaluating the effect on overall survival ( os ) of adding a new targeted agent , x , to standard chemotherapy . 
suppose that the historical mean os with chemotherapy is old = 15 months in older patients ( age 60 years or older ) and young = 24 months in younger patients ( age younger than 60 years ) , with two thirds of patients being older than age 60 years and one third being younger . 
a group sequential design comparing chemotherapy + x with chemotherapy constructed on the basis of the average mean os , avg = ( 2 / 3 ) old + ( 1 / 3 ) young , would have null mean os avg 0 = ( 2 / 3 ) 15 + ( 1 / 3 ) 24 = 18 months . suppose a design is constructed to target an improvement of 33% from avg 0 = 18 to avg * = 24 months , equivalently , a targeted hazard ratio of .75 in favor of chemotherapy + x . 
 thall context key objective an important question in designing and conducting clinical trials is whether and how a trial design should account explicitly and prospectively for patient heterogeneity when making treatment assignment decisions and reaching nal conclusions . the two designs reviewed in this article illustrate how a bayesian utility - based framework can be used to construct practical designs that account for patient heterogeneity . knowledge generated each of the two designsone is a randomized comparative trial and the other is a complex dose - nding trialis a novel methodology that has been published in the statistical literature . 
an aim of this review is to make members of the medical community aware that such designs exist so that they may consider taking this sort of approach in their own trials . relevance the bayesian utility - based approach may be used to construct designs for a wide variety of clinical trials that account for patient heterogeneity by making subgroup - specic , personalized treatment decisions . 
in the presence of patient heterogeneity , this approach renes treatment development and evaluation and thus is more likely to protect safety and provide benet for both the patients enrolled in the trial and future patients . chemotherapy alone in younger patients . 
suppose that , in fact , adding x to chemotherapy decreases mean os in older patients by 10% to 13.5 months but increases mean os in younger patients by 30% to 31.2 months , that is , there is a treatment - age subgroup interaction . 
thus , a group sequential test based on average mean os would be likely to conclude that adding x to chemotherapy fails to improve os , thus making a false - negative conclusion in younger patients . although post - trial data analyses accounting for age may show that chemotherapy + x is superior in younger patients , such an inference may be dismissed as post hoc data dredging , that is , searching the data set for subgroups in which the x effect is nominally signicant . 
arguing for the future use of chemotherapy + x in younger patients thus would be problematic , and it probably would be necessary to repeat the trial , if possible . this problem , consider a trial similar problems arise in early - phase trials in which the goal is to identify an optimal dose , dose pair , or ( dose , schedule ) combination for a new agent or treatment combination at the start of clinical evaluation . 
it has been well established that choosing a dose in a phase i trial on the basis of toxicity alone is a highly awed convention that can easily lead to choosing an unsafe or ineffective dose.1 , 2 as a rst example to optimize the dose d among ve levels ( 1 , 2 , 3 , 4 , 5 )  . 
if the continual reassessment method ( crm ) 3 is used to choose a dose with pr ( toxicity ) closest to .30 , then d = 3 is most likely to be chosen , whereas a 3 + 3 algorithm is most likely to choose either d = 2 or d = 3 . 
in practice , the best and worst outcomes are assigned respective utilities of 100 and 0 , and numerical utilities between these two values for termediate outcomes are elicited from the investigators planning the trial . 
during trial conduct , the posterior mean of uavg ( d , g ) is computed for each d , and the dose giving the largest value is selected for the next good - prognosis patient enrolled . 
the outcome is y = clavien - dindo postoperative morbidity ( pom ) , 7 - 10 scored within 30 days of surgery , a six - level ordinal variable with possible integer values from 0 ( normal recovery ) to 5 ( death )  . 
moreover , because differences in utilities between successive pom levels are far from being equal , using the raw scores 0 , 1 , 2 , 3 , 4 , 5 would also be a misleading way to quantify pom . the design accounts for patient heterogeneity by allowing possibly different conclusions within the subgroups p and s when comparing treatment n to c . 
a key property of the model is that all treatment and subgroup effect parameters vary with the level of pom score , so it is a robust generalization of the conventional proportional odds model.11 the model allows the magnitudes of the n - versus - c effects on y to differ between subgroups and is formulated to borrow strength between subgroups , with prior location parameters determined from elicited information on pom score . 
details are provided in murray et al.6 the trial will enroll a maximum of 200 patients , with an interim comparative test of the n - versus - s effect on pom score after n = 100 patients have been treated and evaluated and possibly a nal test at n = 200 within each subgroup p and s . 
elicited numerical utilities of 30 - day pom scores after esophageal resection pom score utility abbreviation : pom , postoperative morbidity . the subgroup - specic comparative tests , computed under the bayesian model , conclude that n is superior to c in subgroup g = p or s if ( cid : 4 ) ( cid : 1 ) ( cid : 3 ) ( cid : 1 ) uavg n , g  . 
the numerical cutoffs pcut ( 100 ) = .997 and pcut ( 200 ) = .976 were chosen by conducting the overall preliminary computer simulations to control within - subgroup type i error probability of the group sequential test procedure to be .025. 
to ensure balance and comparability with either design , patients were randomly assigned in blocks of four , so for each block of four patients within each prognostic subgroup , two receive nuprehab and two receive the control . the operating characteristics of the two designs are summarized in table 2 . 
the goals are to perform safety monitoring and to identify an optimal nk cell dose from the set { 105 , 106 , 107 } cells per kg of body weight ( hereafter dose levels 1 , 2 , 3 ) within each of the subgroups , while borrowing strength between subgroups . 
this is an example of a sequentially adaptive precision or personalized clinical trial . the trial has ve coprimary outcomes : the times from nk cell infusion to d = death , and the four nonfatal events 4 2019 by american society of clinical oncology p = disease progression , r = response , t = severe toxicity , and c = severe cytokine release syndrome . 
each patients events are monitored for a 365 - day follow - up period . denoting the time to event j by yj for j = d , p , r , t , c for each patient , each yj is a potential outcome because it may or may not be observed ; yp and yr are competing risks because , at most , one of these two events can occur ; the ve potential event times are highly associated with each other ; d censors any events that have not occurred , but such censoring is not independent ; and the distribution of y = ( yd , yp , yr , yt , yc ) varies substantially with disease subgroup . three challenges in designing an nk cell dose - nding trial are ( 1 ) if one ignores the subgroups , then there are high probabilities of making incorrect decisions within subgroups ; ( 2 ) on the basis of current knowledge about nk cell biology , the rates of the ve outcomes are neither monotone increasing nor decreasing in nk cell dose ; and ( 3 ) small to moderate sample sizes in early - phase trials limit the reliability of subgroup - specic decisions . 
the model includes a hierarchical structure with latent ( unobserved ) patient frailties to induce association among the ve outcomes and account for variability not explained by dose and subgroup . 
to establish a prior probability distribution , hyper parameters characterizing location were computed from elicited probabilities of particular combinations of events occurring during the rst 100 days of follow - up , and prior hyper parameters characterizing dispersion were calibrated to reect vague prior knowledge about dose effects . 
details are given in lee et al.14 first assigning utility 0 to any outcome for which the patient dies before day 100 , utilities of the 12 possible combinations of nonfatal outcomes during the rst 100 days following nk cell infusion were elicited from the principal investigator for the trial ( table 3 )  . denote the vector of binary indicators of the 12 possible nonfatal outcomes within 100 days by = ( p , r , t , c )  . 
elicited utilities of the 12 possible 100 - day outcomes for patients in the nk cell dose - finding trial who survive beyond 100 days given that u ( death within 100 days ) = 0 progression , response cytokine storm toxicity yes , no no , no no , yes note . 
the cytokine storm outcome corresponds to a 30 - day evaluation period . abbreviation : nk , natural killer . weighted by the probability distribution of [ |d , g ]  . 
during the trial , for each disease type , patients are randomly assigned among the three doses in order of entry to the trial by randomly permuting the integers ( 1 , 2 , 3 ) , subject to being in accordance with the safety rule . 
at the end of the trial , for each disease subgroup g , the nk cell dose d that is safe and that maximizes u ( d , g|data ) is chosen , with no dose chosen if all three are unsafe within subgroup g . to establish its operating characteristics , the design was simulated under each of six different possible dose - subgroup - outcome scenarios . 
table 4 summarizes the operating characteristics of the design in one particular scenario that includes dose - subgroup interactions , with some doses unsafe for some subgroups but not for others . 
the results in table 4 show that the design is likely to stop accrual to doses in subgroups in which they are unsafe and otherwise is likely to select the truly optimal dose in each subgroup . figure 1 compares the dose - nding design that makes subgroup - specic decisions with a similar design that ignores the six disease subgroups when performing safety monitoring and dose selection . 
histograms are given for the differences between the empirical proportions of pr ( stop| subgroup , dose ) and pr ( stop|dose ) , for truly safe doses ( fig 1a ) and for truly unsafe doses ( fig 1b ) on the basis of computer simulations under the six dose - subgroup - outcome scenarios . 
histograms of differences between empirical proportions of pr ( stop|subgroup , dose ) pr ( stop|dose ) are given for ( a ) truly safe doses , ( b ) truly unsafe doses , and ( c ) pr ( select|subgroup , dose ) pr ( select| dose ) differences showing the probabilities of correctly selecting truly optimal doses . pr ( stop|subgroup , dose ) , pr ( stop|dose ) for truly safe doses , the design that ignores subgroups has a much larger probability of incorrectly stopping treatment in subgroups in which doses are safe . 
for truly unsafe doses , the two designs have similar stopping probabilities , with the important the design with subgroup - specic safety exception that monitoring is about .40 more likely to stop accrual to truly unsafe doses within subgroups . 
figure 1c shows that the subgroup - specic design is much more likely to select truly optimal doses within disease subgroups . additional computer simulations ( not shown ) evaluated the behavior of the nk cell dose - nding design in cases in which the true underlying time - to - event distributions were log - logistic and thus differed substantially from the assumed weibull dose - subgroup - outcome probability model . the results show that the model and design are extremely robust to the true underlying event time distribution model the design persist . and that details are provided in lee et al.14 the nkcelldosending computer program for implementing this design is available at the superior properties of utility - based clinical trial designs for a wide variety of other settings , assuming that patients are homogeneous , are given in houede et al , 15 thall et al , 4 , 16 - 18 lee et al , 19 hobbs et al , 20 murray et al , 21 and xu et al.22 an explanation of how trial design can be formulated as utility - based clinical a decision - making problem is provided by mueller et al.23 the simulation results show that the designs that make subgroup - specic decisions are greatly superior to comignore patient peting conventional methodologies that heterogeneity and treatment - subgroup or dose - subgroup interactions when such subgroup effects are present . 
in the randomized comparative trial , this is seen in terms of extremely large within - subgroup type i and type ii error probabilities of the conventional design in cases of treatment - subgroup interactions . 
these results strongly suggest if patient heterogeneity is that trial designs should be known , conventional clinical replaced by designs that account explicitly and prospectively for patient subgroups and treatment - subgroup or dose - subgroup effects in trial design , conduct , and decision making . 
an important caveat is that , if enrollment to a trial is limited to a homogeneous patient population , then a design with subgroup - specic rules would be an inappropriate elaboration . affiliation 1the university of texas md anderson cancer center , houston , tx preprint version available on biorxiv . support supported by core grant no . 
 bayesian utility - based designs for oncology clinical trials references yan f , thall pf , lu kh , et al : phase i - ii clinical trial design : a state - of - the - art paradigm for dose nding . 
new york , ny , chapman and hall / crc , 2011 thall pf , nguyen hq : adaptive randomization to improve utility - based dose - nding with bivariate ordinal outcomes . 
j biopharm stat 22 : 785 - 801 , 2012 braga m , gianotti l , nespoli l , et al : nutritional approach in malnourished surgical patients : a prospective randomized study . 
semin thorac cardiovasc surg 19 : 79 - 88 , 2007 clavien pa , sanabria jr , strasberg sm : proposed classication of complications of surgery with examples of utility in cholecystectomy . 
surgery 111 : 518 - 526 , 1992 dindo d , demartines n , clavien pa : classication of surgical complications : a new proposal with evaluation in a cohort of 6336 patients and results of a survey . ann surg 240 : 205 - 213 , 2004 10 . 
hoyos v , savoldo b , quintarelli c , et al : engineering cd19 - specic t lymphocytes with interleukin - 15 and a suicide gene to enhance their anti - lymphoma / leukemia effects and safety . 
houede n , thall pf , nguyen h , et al : utility - based optimization of combination therapy using ordinal toxicity and efcacy in phase i / ii trials . 
xu y , thall pf , m uller p , et al : a decision - theoretic comparison of treatments to resolve air leaks after lung surgery based on nonparametric modeling . 
triplenegative breast cancer ( tnbc ) is dened by the lack of expression of estrogen receptor ( er ) , progesterone receptor , and human epidermal growth factor receptor 2 ( her2 ) .1 , 2 this subtype represents 15% to 20% of all breast cancers and is associated with the worst outcome of all subtypes , with greater tendency to distant recurrence in general and visceral metastasis in particular , including brain metastasis.3 , 4 to date , chemotherapy remains the standard of care for tnbc.5 molecular stratication of tnbc will have treatment implications.6 for example , approximately 40% of tnbc patients have expression of programmed death - ligand 1 ( pd - l1 ) protein in immune cells , and this biomarker predicts survival benet from anti - pd - l1 therapy in combination with chemotherapy in the rst - line metastatic setting.7 in addition , approximately 10% of patients with tnbc harbor a germline brca1 / 2 mutation , which confers sensitivity to platinum and / or poly ( adpribose ) polymerase ( parp ) inhibitors.2 , 8 parp is involved in the repair of dna single - strand breaks via the base excision pathway . 
parp inhibitors such as olaparib or talazoparib lead to an accumulation of double - strand dna breaks , resulting in the activation of homologous recombination repair , which can compensate for the lack of activity of the base excision pathway and repair the dna damage.9 however , patients with defects in the homologous recombination dna repair pathway cannot repair dna damages caused by parp inhibitors , and the tumor cell eventually dies ( a term known as synthetic lethality )  . the patient is a 46 - year - old woman diagnosed in december 2015 with stage iib ( ct3cn1 ) moderately differentiated invasive papillary carcinoma with marked tumoral inltrating lymphocytes10 ( 60% ) and the presence of vascular invasion . 
she had a mastectomy and lymphadenectomy in june 2016 . analysis of the surgical specimen revealed extensive invasive residual disease ( ypt2ypn1 ) with a tnbc images of vascular inphenotype and abundant vasion . 
she then underwent adjuvant radiation to the breast and started adjuvant endocrine therapy with tamoxifen ( clinical decision based on baseline er positivity )  . in august 2017 , a positron emission tomography scan revealed multiple pathologic deposits in the bone , lung , and mediastinum and a prepectoral lesion . 
biopsy of the lesion conrmed recurrence of the disease ( gata3 positivity ) and a tnbc phenotype with a ki - 67 of 70% and androgen receptornegative and tumor inltrating lymphocytes around 10% ( fig 1 )  . 
no germline mutation was detected . here , we describe a heavily pretreated patient with tnbc brain metastasis and a brca1 somatic mutation with a remarkable and durable response to parp inhibitor therapy . 
to our knowledge , this is the rst case report to demonstrate disease response to parp inhibition in a tnbc without a germline brca1 or brca2 mutation . the patient was treated with carboplatin and gemcitabine for six cycles , and she achieved a partial response ( fig 2 )  . 
 ( a ) the tumor ( hematoxylin and eosin stain ) was composed of neoplastic inltrative nests with scattered stromal tumor - inltrating lymphocytes with many images of ( b ) lymphovascular invasion ( cd31 )  . 
 ( g ) the tumor had a high proliferation index ( ki - 67 ) , and ( h ) programmed death - ligand 1 ( pd - l1 ) was negative in both the neoplasm and the stromal cells . emergency department with progressively worsening headache . 
a brain magnetic resonance imaging scan showed multiple metastases , the largest being found in the right frontal lobe with surrounding edema ( fig 3a )  . the patient consented to participate in a research project in which tumor proling at the dna and rna level was performed with results discussed at a molecular tumor board . the prepectoral lesion was used for all the molecular analyses . 
the results revealed somatic mutations in brca1 ( s1253fs * 10 9435_9436delgt ) and tp53 ( s37fs * 6 * ) , a low tumor mutational burden ( four mutations per megabase ) , and a stable microsatellite status . 
at the rna level , an ncounter - based breast cancer 360 panel was performed.11 this assay includes 752 breast cancerrelated genes and 23 signatures , the tumor inammation signature , 12 the pam50 subtype predictor , 13 and the tnbctype classications14 , 15 ( fig 4 )  . 
results revealed a pam50 basal - like subtype with the following features : high expression of brca - ness and dna scar signatures , high expression of proliferationrelated genes , low expression of androgen receptorand estrogen - regulated genes , low expression of cd8 t cells and pd - l1 , high expression of immunosuppressive genes or signatures such as transforming growth factorand regulatory t - cell signatures , and a tnbctype mesenchymal subtype . on the basis of these results , off - label use of olaparib 300 mg twice per day was indicated . 
consideration was given to introducing corticosteroids or delivering whole - brain radiotherapy ( wbrt ) , but after discussion with the patient , a clinical decision was made to start olaparib under close observation and without the addition of either radiotherapy or corticosteroids . 
after 2 weeks of treatment , neurologic symptoms improved , and a restaging magnetic resonance imaging scan at week 8 demonstrated a signicant reduction in the size of the brain lesions and disappearance of associated cerebral edema ( fig 3b )  . 
brca proteins play a critical role in the homologous recombination dna repair pathway.16 in the presence of a brca germline mutation , one allele is affected , and the occurrence of a genetic alteration in the other allele ( eg , through methylation or loss of heterozygosity ) leads to a nonfunctional brca and the appearance of breast cancer , among other cancers.9 to date , two phase iii clinical trials have shown that parp inhibition with olaparib17 or talazoparib18 is superior to standard chemotherapy in terms of progression - free survival in her2 - negative advanced breast cancer harboring a brca germline mutation . 
 short title neoadjuvant doxorubicin + cyclophosphamide followed by paclitaxel radiation completed sep 2016 ; adjuvant tamoxifen carboplatin + gemcitabine with clinical response ; treatment stopped for toxicities palliative radiotherapy for bone metastasis ; progression on capecitabine + vinorelbine olaparib initiated dec 2015 jul 2016 aug 2017 feb 2018 may 2018 diagnosed with stage iib ( ct3n1 ) ; er , 50% ; pr , 0% ; her2 - ki - 67 , 80% right mastectomy and alnd ; ypt2n1 ; tnbc ; ki - 67 , 40% metastatic disease , bone , lymph node , subcutaneous tissue ; tnbc reappearance of pain and progression of bone metastases brain metastases fig 2 . 
alnd , axillary lymph node dissection ; er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; pr , progesterone receptor ; tnbc , triple - negative breast cancer ; yp , pathologic staging after neoadjuvant therapy . patients with germline brca1 / 2 - mutated advanced breast cancer . 
brain magnetic resonance imaging before and after olaparib monotherapy . images before olaparib therapy show a cortical enhancing lesion on gadolinum - enhanced t1 - weighted imaging in the inferior frontal gyrus with perilesional edema visualized on uid - attenuated inversion recovery ( flair ) sequencing , as well as diffuse dural enhancement in the right hemisphere . 
selected signature scores are shown with the tumor inammation signature ( tis ) and pam50 signatures at the core ; the other signature scores are shown as bars around the riscores range from 0 to 1 mapped to quantiles of the population with invasive breast carcinoma in the cancer genome atlas ( tcga )  . 
apm , antigen processing machinery ; ar , androgen receptor ; brca - ness , brcaness signature ; cldl - ness , claudin - low subtype signature ; diffrn , differentiation ; dna scar , dna scar signature ; er , estrogen receptor ; her2 - e , her2 - enriched ; inm chmkn , inammatory chemokines ; pd - 1 , programmed cell death protein 1 ; pdl1 , programmed death - ligand 1 ; pgr , progesterone receptor ; tigit , t cell immunoreceptor and ig and itims domains ; treg , regulatory t cell . somatic mutations may also arise in genes involved in homologous recombination . 
early - phase clinical trials of parp inhibitors in metastatic tnbc and germline brca1 / 2 wild - type her2 - negative breast cancer with specic somatic genomic alterations such as brca1 / 2 mutations are underway ( eg , nct02401347 ; phase ii talazoparib in brca1 + brca2 wild - type & triple - neg / her2 - negative breast cancer / solid tumors and nct03330847 ; to assess safety and efcacy of agents targeting dna damage repair with olaparib versus olaparib monotherapy )  . the long - lasting response of breast cancer brain metastasis to olaparib in the absence of any other treatment is worth discussing . 
first , this suggests that olaparib , which had not previously been thought to cross the blood - brain barrier , 28 is able to get to the site of the tumor . 
concordant with this , other case reports with olaparib monotherapy have described regression of brain metastasis.29 , 30 second , olaparib , and other highly effective targeted systemic therapies , allow the delay of wbrt.31 - 35 this is important because wbrt can have a negative impact on quality of life and long - term neurocognitive functioning.36 thus , strategies to avoid , delay , or abrogate the effects of wbrt using systemic targeted therapies should be prioritized . in summary , comprehensive genomic alteration testing may provide novel clinical strategies for personalized therapy in advanced tnbc with improvement in overall survival and quality of life . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . tom as pascual consulting or advisory role : genentech research funding : genentech ( inst ) , msd oncology ( inst ) consulting or advisory role : bristol - myers squibb , diaceutics research funding : novartis travel , accommodations , expenses : pzer , boehringer ingelheim , menarini , msd , takeda pharmaceuticals , thermo fisher scientic maria vidal consulting or advisory role : novartis / pzer speakers bureau : novartis / pzer , genentech , eisai travel , accommodations , expenses : pzer montserrat muoz consulting or advisory role : eli lilly speakers bureau : roche travel , accommodations , expenses : roche , eli lilly aleix prat employment : novartis ( i ) honoraria : pzer , novartis , roche , msd oncology , eli lilly , daiichi sankyo consulting or advisory role : nanostring technologies ( inst ) , amgen , roche , novartis , pzer , bristol - myers squibb research funding : roche ( inst ) , novartis ( inst ) patents , royalties , other intellectual property : pct / ep2016 / 080056 : her2 as a predictor of response to dual her2 blockade in the absence of cytotoxic therapy travel , accommodations , expenses : daiichi sankyo other relationship : oncolytics biotech no other potential conicts of interest were reported . cristina teixid o honoraria : msd , pzer references bauer kr , brown m , cress rd , et al : descriptive analysis of estrogen receptor ( er ) - negative , progesterone receptor ( pr ) - negative , and her2 - negative invasive breast cancer , the so - called triple - negative phenotype : a population - based study from the california cancer registry . 
nature 490 : 61 - 70 , 2012 carey la , perou cm , livasy ca , et al : race , breast cancer subtypes , and survival in the carolina breast cancer study . 
jama 295 : 2492 - 2502 , 2006 dent r , trudeau m , pritchard ki , et al : triple - negative breast cancer : clinical features and patterns of recurrence . 
clin cancer res 13 : 4429 - 4434 , 2007 cardoso f , senkus e , costa a , et al : 4th eso - esmo international consensus guidelines for advanced breast cancer ( abc 4 )  . 
ann oncol 29 : 1634 - 1657 , 2018 prat a , adamo b , cheang mc , et al : molecular characterization of basal - like and non - basal - like triple - negative breast cancer . 
oncologist 18 : 123 - 133 , 2013 schmid p , adams s , rugo hs , et al : atezolizumab and nab - paclitaxel in advanced triple - negative breast cancer . 
n engl j med 379 : 2108 - 2121 , 2018 ahn sg , kim sj , kim c , et al : molecular classication of triple - negative breast cancer . 
j breast cancer 19 : 223 - 230 , 2016 ashworth a : a synthetic lethal therapeutic approach : poly ( adp ) ribose polymerase inhibitors for the treatment of cancers decient in dna double - strand break repair . 
salgado r , denkert c , demaria s , et al : the evaluation of tumor - inltrating lymphocytes ( tils ) in breast cancer : recommendations by an international tils 11 . 
lehmann bd , jovanovi c b , chen x , et al : renement of triple - negative breast cancer molecular subtypes : implications for neoadjuvant chemotherapy j clin invest 121 : 2750 - 2767 , 2011 selection . 
chandran ea , kennedy i : signicant tumor response to the poly ( adp - ribose ) polymerase inhibitor olaparib in heavily pretreated patient with ovarian carcinosarcoma harboring a germline rad51d mutation . 
ngoi nyl , tay d , heong v , et al : reversal of bowel obstruction with platinum - based chemotherapy and olaparib in recurrent , short platinum - free interval , rad51c germline mutationassociated ovarian cancer . 
winter c , nilsson mp , olsson e , et al : targeted sequencing of brca1 and brca2 across a large unselected breast cancer cohort suggests that one - third of mutations are somatic . 
sahgal a , soliman h , larson da : whole - brain radiation therapy of brain metastasis , in kim dg , lunsford ld ( eds ) : current and future management of brain metastasis . 
gaspar le , mehta mp , patchell ra , et al : the role of whole brain radiation therapy in the management of newly diagnosed brain metastases : a systematic review and evidence - based clinical practice guideline . 
bachelot t , romieu g , campone m , et al : lapatinib plus capecitabine in patients with previously untreated brain metastases from her2 - positive metastatic breast cancer ( landscape ) : a single - group phase 2 study . 
 outcomes of chemotherapy for microsatellite instablehigh metastatic colorectal cancers purpose microsatellite instable - high ( msi - h ) colorectal cancers ( crcs ) are known to carry better survival in the local disease stage even without treatment . 
the influence of types of treatment on survival of msi - h metastatic crcs ( mcrcs ) is still unclear and is evaluated in this study . materials and methods patients with msi - h mcrc treated with first - line chemotherapy , with or without bevacizumab , identified in the israeli population - based molecular epidemiology of colorectal cancer ( mecc ) study , were diagnosed between 1998 and 2013 and followed up until may 2017 ; msi status was determined by comparing 10 markers in tumor and normal tissue . 
dates of metastases and death and treatment details were extracted from oncology records . results among 590 patients treated for mcrc , 106 ( 18% ) had msi - h tumors . 
although treatment advances with modern protocols including antivascular endothelial growth factor and antiepidermal growth factor receptor ( egfr ) monoclonal antibodies1 - 3 prolonged median overall survival ( os ) of patients with crc to > 2 years , mcrc , unfortunately , is still an incurable disease in most cases . k - ras proto - oncogene ( kras ) or n - ras proto oncogene ( nras ) mutation ; the presence of a braf v600e mutation has a detrimental effect on overall survival ; the presence of human epidermal growth factor receptor 2 ( her2 ) in mcrc tumors suggests the possibility of benefit from anti - her2 biologic treatment ; and , more recently , microsatellite instable ( msi ) high tumors have been identified as candidates for immunotherapy.4 - 7 molecular heterogeneity in metastatic crcs influences treatment and outcome . 
anti - egfr agents are less effective in the presence of a loss of genomic stability is identified as an early step in colon cancer tumorigenesis and has pathologic , phenotypic , and clinical consequences.8 - 11 stephen b . 
 molecular analysis enables better understanding and separation of colorectal tumors now identified as carrying differences in clinical outcome.12 , 13 under this classification , tumors defined as consensus molecular subtype - 1 ( cms1 ) are characterized as microsatellite instable ( msi - h ) and hypermutated tumors.14 the clinical importance and exclusiveness of msi - h crcs have formerly been established.15 - 18 msi - h tumors have significantly better prognosis at early local stages of disease and rarely metastasize . 
cases identified in the mecc study were approached for risk - factors interview and contributed a venous blood sample after signing a consent form approved by carmel medical center in israel and the university of southern california in the united states . 
dna was extracted from both the peripheral blood and the tissue sample and was routinely studied for msi status , kras and braf mutations , as well as known founder mutations in mmr genes , mostly in ashkenazi jews . 
clinical follow - up included identification of treatment modalities used during the whole follow - up period and identification of changes in disease status , including identification of new metastases . 
details of treatments , as well as date of identification of metastases ( at diagnosis or during disease progression ) , were extracted from the medical files of the patients , which were extracted by experienced senior physicians . for this study , mecc cases that presented with metastatic disease at diagnosis or developed metastases during follow - up were sought . 
in addition to cases from the mecc population - based series , we recruited into the study other mcrc cases that were evaluated in our laboratory on the basis of their clinical presentation or suspicion of lynch syndrome to increase the size of the case series . 
detailed treatment options were grouped into three categories : fu or capecitabine only , combination chemotherapy ( oxaliplatin - based or irinotecan - based in combination with fluoropyrimidine ) , and combination chemotherapy with bevacizumab . 
 metastases with information on treatment details , and have available tissue and germline dna to analyze msi and braf status . laboratory assay dna was extracted using a commercial dna extraction kit . 
five loci of mononucleotide repeats ( bat25 , bat26 , bat40 , - catenin , and tgfbrii ) and five of dinucleotide repeats ( d2s123 , d5s346 , d10s197 , d17s250 , and d18s58 ) were amplified and tested . 
those include the five original bethesda panel markers and five additional monoand dinucleotide markers.33 results for each marker were registered as stable , unstable , equivocal , or suspected as loss of heterozygosity . 
most msi - h cases were also validated by immunohistochemistry tests of the mmr genes . mutations in codon 600 of braf were identified by direct sequencing of exon 15 of the braf gene . 
similarly , kras mutations in exon 12 , 13 , and 61 were identified using a taqman - based single - nucleotide polymorphism genotyping assay on the abi prism 7900ht sequence detection system ( applied biosystems ) in a 96 - well format . until the recorded date of death ( of any cause ) or the last date of available follow - up . 
overall survival was estimated with the use of kaplanmeier method and presented using medians and 2 - year and 5 - year survival probabilities . differences in os were summarized using hazard ratios ( hrs ) , estimated using cox proportional hazard modeling . 
the predictive effect of msi status on treatment effects was assessed using cox proportional hazard models with terms for treatment , msi status , and their interaction results patient population the study population consisted of 106 msi - h mcrc ( met / msi - h ) cases for which first - line chemotherapy - based treatment was identified . 
the metastatic msi - h group had mean age at treatment of 63 15 years , 54% female , 86% with jewish ethnicity , and 48% presenting at stage iv at diagnosis . 
generally , the met / mss group had comparable sex and ethnicity ( jewish / non - jewish ) distribution , as well as frequency of presenting at stage iv at diagnosis . 
this distribution reflects that fact that the patients with met / msi - h were younger at diagnosis ( proportion of patients younger than 50 years : 25% in met / msi - h group and only 10% in met / mss group )  . 
overall survival was calculated from the start date of first treatment of the first identified metastasis ( either at time of crc diagnosis or at time of disease progression ) and treatments for metastatic disease common first - line treatment chemotherapy for the metastatic disease in the msi - h group included fu + leucovorin ( lcv ) or capecitabine only in 21% ( n = 22 ) , combination chemotherapy protocols ( irinotecan based or oxaliplatin based ) in 33% ( n = 35 ) , and combination chemotherapy ( irinotecan based or oxaliplatin based ) and bevacizumab in 46% ( n = 49 ) of cases . 
demographic and disease characteristics of study participants with metastatic colorectal cancer by microsatellite instability status ( n = 590 ) characteristic metastatic msi - h ( n = 106 ) metastatic mss ( n = 484 ) age younger than 50 years at diagnosis female sex jewish ethnicity braf mutation positive stage iv at diagnosis right colon primary tumor location 26 ( 25 ) 57 ( 54 ) 88 * ( 86 ) 19 ( 18 ) 45 ( 48 ) 39 ( 38 ) note . 
 figure 1 presents frequency of the three classes across period years . second - line treatment was given to 55% of the patients treated before 2003 , 63% of those treated in 2003 to 2006 , and 68% of patients treated in 2007 and after . 
no difference in number of treatment lines was noticed between cases with msi - h and cases with mss tumors , probably reflecting the fact that in those years the treating oncologists were unaware of the msi status at time of treatment . in addition , in the msi - h population , the baseline characteristics of patients in the different treatment regimen were comparable ( data not shown )  . 
figure 4 presents os by treatment group , separately for patients with met / mss ( fig 4a ) and patients with met / msi - h ( fig 4b ) , in the homogenous population of braf - wt cases . 
 a sensitivity analysis adjusting for study period revealed similar results . prognostic effect of msi status in the braf - wt population the prognostic role of msi status in the metastatic disease setting was assessed in the population of patients who were indicated to receive an fu - only regimen as having the smallest or even no treatment effect , according to the literature . 
overall survival of patients with microsatellite instable , brafwild type metastatic colorectal cancer by treatment groups in the in the molecular epidemiology of colorectal cancer study , northern israel ( n = 87 )  . 
the mecc study reported here has recruited and collected materials over a time span of 17 years from close to 6 , 000 cases of crc and served as the source for the 590 cases who were diagnosed with , or later developed , metastases and for whom detailed treatment information was available . 
all cases participating in the final analysis were evaluated for their msi status , which was performed in only approximately two thirds of all cases recruited into mecc , with enrichment for suggestive phenotypes . in accordance with other published literature , cases with msi - high mcrc in our study were younger at diagnosis and had a higher proportion of braf mutations , 33 , 34 with a similar proportion of right - sided tumors . 
although msi - h tumors are described as having a much better prognosis than mss tumors for early - stage disease , the proportion of tumors diagnosed with metastases at the time of diagnosis was similar between msi - h cases and mss cases . 
the leading randomized controlled trials evaluating the effect of various chemotherapy regimens in mcrc were not randomized by msi status , and most have not provided subgroup analyses of the results according to their msi status . our study has three major findings . 
we verified that the survival of patients with mcrc indeed improved with the introduction of new chemotherapies but showed that the improvement in survival was limited to the met / mss , braf - wt cases and was not evident in the met / msi - h , braf - wt group of patients . 
we were unable to have a comparison with an observation - only group , and no future studies are likely to include such an arour observational data found no difference in os among metastatic msi - h cases between cases treated with a basic fu + lcv regimen only , compared with cases treated with any ( oxaliplatin or irinotecan ) combination chemotherapy with or without bevacizumab , whereas a significant os improvement was found with advanced chemotherapy in met / mss cases . 
similarly , we did not have any cases that were treated with immune checkpoint inhibitors at the time interval of the current analysis . few reports evaluated the effect of chemotherapy in met / msi - h cases . 
although early studies reported a positive effect of high - dose fu + lcv in patients with met / msi - h in comparison with patients with met / mss , 35 , 36 more recent studies of fu , in combination with irinotecan or oxaliplatin , did not show benefit.16 , 31 , 34 , 37 one study31 showed a trend toward benefit of oxaliplatin - based treatment in cases of msi - h mcrc . 
our data do not have enough power to evaluate specific therapeutic regimens . we chose to exclude from our study all metastatic cases that were not treated at all , because of the inability to assess the causes for no treatment and biases that could stem from it . 
comparison of os results in met / mss and met / msi - h groups supports biologic differences , with a baseline survival advantage for the msi - h group . 
effect of combination treatment on overall survival of patients with metastatic , brafwild type colorectal cancer by microsatellite instability status in the molecular epidemiology of colorectal cancer study , northern israel . 
 published data on the effect of braf mutation on prognosis in patients with met / msi - h were published on a group of crc stages ii to iv , 38 potentially underrepresenting the few cases with stage iv disease . 
extremely poor outcomes in this patient group support the use of the folfoxiri ( oxaliplatin , irinotecan , fluorouracil , leucovorin ) protocol in the unselected group of braf - mutated cases . 
given the much higher prevalence of braf mutations in the msi - h cases , 11 , 26 , 39 it is important to study the outcomes of folfoxiri in this subgroup of patients with met / msi - h . our study is limited by the relatively modest sample size of patients with msi - h mcrc . 
 advantages of our population - based sampling of incident cases with long - term follow - up include generalizability to community practice in a large and well - defined population . 
the representative , observational nature of the data from a large health system , in combination with molecular evaluation of all tumor tissues , offers a framework for understanding clinical practice over nearly two decades in a universally insured group of patients in a single country . msi status is becoming a cornerstone of individualized decision making with regard to a variety of potential oncological interventions , and this trend is likely to continue with the introduction of immunotherapy.40 , 41 routine mutational profiling of mcrc and specifically msi testing and other assays that designate deficient mismatch repair have already been recommended.39 , 42 , 43 the failure of conventional advanced treatments to improve survival in the meaningful subset of met / msi - h cases emphasizes the need to evaluate the role of the newly introduced immunotherapy as a first - line treatment in these cases with msi - h / braf - wt mcrc . in conclusion , therapeutic approaches to mcrc have changed dramatically during the past two decades , with increasing reliance on the molecular features of tumors to inform treatment decisions . 
gruber stock and other ownership interests : teva pharmaceuticals provision of study material or patients : flavio lejbkowicz collection and assembly of data : all authors data analysis and interpretation : katerina shulman , ofra barnett - griness , joel k . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . katerina shulman no relationship to disclose vered friedman no relationship to disclose joel k . 
gruber employment : brogent technologies leadership : brogent technologies stock and other ownership interests : brogent technologies , fulgent therapeutics consulting or advisory role : myriad genetics , fulgent therapeutics research funding : myriad genetics ( inst ) flavio lejbkowicz no relationship to disclose gad rennert no relationship to disclose affiliations katerina shulman , hillel yaffe medical center , hadera ; katerina shulman , ofra barnett - griness , vered friedman , flavio lejbkowicz , and gad rennert , carmel medical center , and technion , haifa , israel ; joel k . 
zhou sw , huang yy , wei y , et al : no survival benefit from adding cetuximab or panitumumab to oxaliplatin - based chemotherapy in the first - line treatment of metastatic colorectal cancer in kras wild type patients : a meta - analysis . 
chan dl , pavlakis n , shapiro j , et al : does the chemotherapy backbone impact on the efficacy of targeted agents in metastatic colorectal cancer ? a systematic review and meta - analysis of the literature . 
siena s , sartore - bianchi a , di nicolantonio f , et al : biomarkers predicting clinical outcome of epidermal growth factor receptor - targeted therapy in metastatic colorectal cancer . 
tol j , dijkstra jr , klomp m , et al : markers for egfr pathway activation as predictor of outcome in metastatic colorectal cancer patients treated with or without cetuximab . 
mller ci , schulmann k , reinacher - schick a , et al : predictive and prognostic value of microsatellite instability in patients with advanced colorectal cancer treated with a fluoropyrimidine and oxaliplatin containing first - line chemotherapy . 
sargent dj , marsoni s , monges g , et al : defective mismatch repair as a predictive marker for lack of efficacy of fluorouracil - based adjuvant therapy in colon cancer . 
weitzel jn , blazer kr , macdonald dj , et al : genetics , genomics , and cancer risk assessment : state of the art and future directions in the era of personalized medicine . 
webber em , kauffman tl , oconnor e , et al : systematic review of the predictive effect of msi status in colorectal cancer patients undergoing 5fu - based chemotherapy . 
des guetz g , schischmanoff o , nicolas p , et al : does microsatellite instability predict the efficacy of adjuvant chemotherapy in colorectal cancer ? a systematic review with meta - analysis . 
ribic cm , sargent dj , moore mj , et al : tumor microsatellite - instability status as a predictor of benefit from fluorouracil - based adjuvant chemotherapy for colon cancer . 
cremolini c , loupakis f , masi g , et al : folfoxiri or folfoxiri plus bevacizumab as first - line treatment of metastatic colorectal cancer : a propensity score - adjusted analysis from two randomized clinical trials . 
van cutsem e , khne c - h , lng i , et al : cetuximab plus irinotecan , fluorouracil , and leucovorin as first - line treatment for metastatic colorectal cancer : updated analysis of overall survival according to tumor kras and braf mutation status . 
peeters m , price tj , cervantes a , et al : randomized phase iii study of panitumumab with fluorouracil , leucovorin , and irinotecan ( folfiri ) compared with folfiri alone as secondline treatment in patients with metastatic colorectal cancer . 
tran b , kopetz s , tie j , et al : impact of braf mutation and microsatellite instability on the pattern of metastatic spread and prognosis in metastatic colorectal cancer . 
goldstein j , tran b , ensor j , et al : multicenter retrospective analysis of metastatic colorectal cancer ( crc ) with high - level microsatellite instability ( msi - h )  . 
liang j - t , huang k - c , lai h - s , et al : high - frequency microsatellite instability predicts better chemosensitivity to high - dose 5 - fluorouracil plus leucovorin chemotherapy for stage iv sporadic colorectal cancer after palliative bowel resection . 
brueckl wm , moesch c , brabletz t , et al : relationship between microsatellite instability , response and survival in palliative patients with colorectal cancer undergoing first - line chemotherapy . 
kim je , hong ys , ryu m - h , et al : association between deficient mismatch repair system and efficacy to irinotecan - containing chemotherapy in metastatic colon cancer . 
overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - deficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
dunne pd , oreilly pg , coleman hg , et al : stratified analysis reveals chemokine - like factor ( cklf ) as a potential prognostic marker in the msi - immune consensus molecular subtype cms1 of colorectal cancer . 
 genomic profiling to expand management options for locally advanced esophagogastric cancers : a proof of principle case introduction the management of locally advanced esophageal and gastric cancer is an evolving field , but despite improvement in response rates and surgical techniques , recurrence rates for stage iii disease remain high.1 , 2 surgical resection is potentially curative and associated with established morbidity and mortality risk , limiting surgery to medically fit patients . 
emerging data suggest a role for positron emission tomography ( pet ) adaptive treatment strategies and possibly incorporation of trastuzumab in neoadjuvant therapy for patients with human epidermal growth factor receptor 2 ( her2 ) positive disease.3 , 4 however , additional tumor biologic features are not incorporated routinely in the management of locally advanced disease . 
large collaborative molecular characterization efforts , including the cancer genome atlas , the asian cancer research group , and commercial sequencing databases , have highlighted genomically defined subgroups.5 - 9 within gastric and esophageal cancers , 4% to 22% are reportedly microsatellite instable ( msi - h ) , a subgroup that has demonstrated significant responsiveness to immune checkpoint inhibitors ( icpis ) in small metastatic data sets.10 , 11 the potential to incorporate this approach in earlier - stage disease is understudied , and , to our knowledge , we report the first case describing a complete response to pembrolizumab in an msi - h stage iii gastroesophageal junction ( gej ) adenocarcinoma with persistent disease after definitive chemoradiotherapy ( crt )  . 
staging petcomputed tomography ( ct ) demonstrated a large and intensely avid mass at the gej ( standardized uptake value of 20.3 ) with no evidence of distant disease ( fig 2 )  . 
pet - ct scanning was repeated 10 weeks after crt completion , demonstrating partial response with residual pet - avid mass at the gej ( standardized uptake value of 7.1 ) , confirmed by endoscopic evidence of persistent disease and symptomatic dysphagia ( fig 2 )  . 
to explore additional therapeutic options , the original gej biopsy was submitted for comprehensive genomic profiling ( foundationone ) , which revealed msi - h , a high tumor mutational burden ( tmb ) of 36 mutations per dna megabase , an absence of erbb2 ( her2 ) alterations , and several additional genomic alterations ( appendix table a1 )  . 
orthogonal immunohistochemical mismatch repair testing confirmed loss of mlh1 and pms2 , and mlh1 promoter polymerase chain reaction testing confirmed mlh1 promoter hypermethylation , all consistent with a sporadic msi - h tumor ( fig 1 )  . 
 ( a ) scattered luminal necrosis as well as punctate single cell apoptoses and frequent mitoses are visible . mismatch repair immunohistochemistry demonstrates loss of ( b ) mlh1 and ( c ) pms2 , with intact ( d ) msh6 and ( e ) msh2 . 
 ( a ) scattered tumor infiltrating lymphocytes were present , at a density of approximately one lymphocyte per five to 10 tumor cells . response with resolution of pet - avid gej mass ( fig 2 )  . 
at the time of submission , he continues on pembrolizumab and remains clinically asymptomatic with ongoing complete response now over 8 months . discussion the ability to identify the optimal therapy for each patient is the hallmark of the precision medicine paradigm but has largely remained elusive in esophagogastric cancers to date . 
in the nonmetastatic setting , attempts to incorporate biologic agents , including the antiepidermal growth factor receptor monoclonal antibodies and antiangiogenesis agents , have not improved outcomes.12 , 13 the fully accrued radiation therapy oncology group ( rtog ) - 1010 trial examining a role for trastuzumab in combination with crt in locoregional esophageal / gej adenocarcinoma may ultimately be the first to identify a molecularly selected group to derive benefit from a biologic agent during neoadjuvant therapy for resectable disease . 
however , at the present time , patients with persistent disease after definitive crt who are unfit for resection represent a difficult clinical scenario with limited established approaches and 3 - year survival less than 10% in some series.14 , 15 although only a single case is presented herein , we suggest that in locally advanced unresectable esophagogastric cancer there may be clinical utility to molecular profiling to expand potential treatment options . 
the cancer genome atlas data sets for gastric and esophageal cancer are almost exclusively derived from nonmetastatic surgical samples and report rates of msi - h of 22% and 0% , respectively ( 0% for confirmed esophageal adenocarcinoma , although three of 36 among gej tumors not clearly of esophageal origin ) .5 , 6 this differs somewhat from the 6% rate of msi - h reported from the capecitabine and oxaliplatin adjuvant study in stomach cancer ( classic ) trial analysis of resected stage ii to iii gastric cancer and the 6.7% rate of msi - h identified in the european medical research council adjuvant gastric infusional chemotherapy ( magic ) trial of resectable gastroesophageal cancer.16 in both data sets , msi - h appears to confer a favorable prognosis and unclear benefit from adjuvant or perioperative chemotherapy , analogous to stage ii colon cancer.17 - 19 although analyses from ongoing metastatic and locoregional trials will refine the incidence of msi - h tumors , a portion will be msi - h and thus will be optimal candidates for immunotherapy consideration as supported by our case . 
complete resolution of [ 18f ] fluorodeoxyglucose activity was observed after three doses of pembrolizumab , and imaging is shown in coronal , sagittal , and axial planes for reference . pretreatment 10 weeks postchemoradiotherapy 10 weeks postpembrolizumab start strong biologic rationale , including in nonmetastatic locally advanced unresectable patients who have progressed on prior therapy.20 the ongoing checkmate - 577 trial ( nct02743494 ) will be important to more clearly establish the role of icpis in the adjuvant / locoregional setting after concurrent crt and surgery with persistent disease , and analyses for msi testing as well as tmb will be important.21 importantly , there is scientific rationale for moving these agents into the true neoadjuvant setting when the primary tumor remains.22 , 23 notably , our patient was not deemed a surgical candidate and would not be eligible for this trial . additional small studies incorporating programmed death - 1 inhibitors into concurrent crt will likely add more details , and there is strong scientific rationale for this approach ( nct03044613 ) .22 more broadly , predictive biomarkers for icpis are critical to identify patients who are most likely ( or least likely ) to benefit from icpi incorporation . not surprisingly , our patient harbored an elevated tmb at 36 mutations / dna megabase . 
however , a fraction of microsatellite stable gi cancers have also been shown to have high tmb.24 next - generation sequencingderived tmb has emerged as a robust biomarker for icpi benefit across several tumor types.25 - 27 in a small retrospective series of esophagogastric cancers , it was suggested that msi - h or tmb of > 14 mutations / megabase was associated with icpi benefit , although larger series will be critical to refine tmb in esophago - gastric cancers ( note that tmb determination was slightly different in this study ) .28 overall , our case highlights the potential role for genomic profiling in this nonmetastatic clinical situation and suggests a possible treatment approach . 
klempner consulting or advisory role : eli lilly , boston biomedical , celgene , astellas pharma speakers bureau : foundation medicine travel , accommodations , expenses : eli lilly the following represents disclosure information provided by authors of this manuscript . 
schrock employment : foundation medicine stock and other ownership interests : foundation medicine joseph chao consulting or advisory role : eli lilly , bayer , five prime therapeutics , boston biomedical , merck research funding : merck ( inst ) , novonco therapeutics ( inst ) siraj m . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health on microbiome stuff in non - neoplastic disease ( i ) affiliations samuel j . 
klempner , cedars - sinai medical center ; winnie wu , providence saint johns hospital , los angeles ; joseph chao , city of hope comprehensive cancer center , duarte , ca ; and alexa b . 
oppedijk v , van der gaast a , van lanschot jj , et al : patterns of recurrence after surgery alone versus preoperative chemoradiotherapy and surgery in the cross trials . 
smyth ec , fassan m , cunningham d , et al : effect of pathologic tumor response and nodal status on survival in the medical research council adjuvant gastric infusional chemotherapy trial . 
lordick f , ott k , krause bj , et al : pet to assess early metabolic response and to guide treatment of adenocarcinoma of the oesophagogastric junction : the municon phase ii trial . 
goodman ka niedzwiecki d , hall n , et al : initial results of calgb 80803 ( alliance ) : a randomized phase ii trial of pet scan - directed combined modality therapy for esophageal cancer . 
ali sm , sanford em , klempner sj , et al : prospective comprehensive genomic profiling of advanced gastric carcinoma cases reveals frequent clinically relevant genomic alterations and new routes for targeted therapies . 
gainor jf , tan ds , de pas t , et al : progression - free and overall survival in alk - positive nsclc patients treated with sequential crizotinib and ceritinib . 
le dt , durham jn , smith kn , et al : mismatch - repair deficiency predicts response of solid tumors to pd - 1 blockade . science 357 : 409 - 414 , 2017 12 . 
cunningham d , stenning sp , smyth ec , et al : peri - operative chemotherapy with or without bevacizumab in operable oesophagogastric adenocarcinoma ( uk medical research council st03 ) : primary analysis results of a multicentre , open - label , randomised phase 2 - 3 trial . 
intergroup phase iii trial of neo - adjuvant chemotherapy , followed by chemoradiation and surgery with and without cetuximab in locally advanced esophageal carcinoma : first results from the sakk 75 / 08 trial . 
smyth ec , wotherspoon a , peckitt c , et al : mismatch repair deficiency , microsatellite instability , and survival : an exploratory analysis of the medical research council adjuvant gastric infusional chemotherapy ( magic ) trial . jama oncol 3 : 1197 - 1203 , 2017 17 . 
bang yj , kim yw , yang hk , et al : adjuvant capecitabine and oxaliplatin for gastric cancer after d2 gastrectomy ( classic ) : a phase 3 open - label , randomised controlled trial . 
kelly rj , lockhart ac , jonker dj , et al : checkmate 577 : a randomized , double - blind , phase 3 study of adjuvant nivolumab ( nivo ) or placebo in pts with resected esophageal ( e ) or gastroesophageal junction ( gej ) cancer . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
ku gy , sanchez - vega f , chatila w , et al : correlation of benefit from immune checkpoint inhibitors with next gen sequencing ( ngs ) profiles in esophagogastric cancer ( egc ) patients . 
the tumor was negative for programmed death ligand 1 ( pd - l1 ) expression ( tumor proportion score , 1% ) .24 postoperative imaging 6 weeks later revealed two lowdensity liver lesions measuring 1.5 cm ( segment 4a ) and 1.9 cm ( segment 2 ; fig 2a ) , which were hypermetabolic on an 18 - uorodeoxyglucose ( fdg ) positron emission tomography ( pet ) / computed tomography scan . 
after two cycles of carboplatin and etoposide , 10 new liver lesions were evident on imaging ( fig 2b )  . he subsequently enrolled in a phase ii study of pembrolizumab ( 10 mg / kg intravenously [ iv ] every 2 weeks ) for patients with msi - h tumors ( clinicaltrials.gov identier : nct01876511 )  . 
these required discontinuation of pembrolizumab after 10 months despite ongoing disease response to treatment ( fig 2d )  . hypothyroidism the patient underwent total proctocolectomy ; both tumors were t1n0 . 
msi testing ( internal ucsf500 assay ; ucsf clinical cancer genomics laboratory ) and mmr protein immunohistochemistry of the resected colon cancer sample conrmed msi - h status and loss of mlh1 expression in the tumor and normal samples . 
by cycle 11 of pembrolizumab , worsening hypothyroidism was evident , peaking at cycle 13 with thyroidstimulating hormone levels of 79.2 iu / ml ( free t4 , 0.6 ng / dl ; total t3 , 63 ng / dl )  . 
 new - onset diabetic ketoacidosis / insulin - dependent diabetes mellitus arthritis whitman et al at 10 months after starting pembrolizumab ( cycle 19 ) , the patient presented with diabetic ketoacidosis ( dka ) ; he had blood glucose levels  . 
given the lack of data supporting use in this setting , corticosteroids were not immediately started , although grade 4 autoimmune type 1 insulin - dependent diabetes mellitus was suspected.25 pembrolizumab was discontinued , and daily insulin therapy was initiated . myocarditis the patient experienced bradyarrhythmias with complete heart block while recovering from dka . 
the troponin level was elevated at 7.4 g / l ( normal , 0.05 g / l ) , the electrocardiogram showed new inferior q waves , and the echocardiogram revealed a depressed ejection fraction ( 30% - 35% ) and regional wall motion abnormalities consistent with coronary artery disease . 
he was monitored with serial echocardiograms , electrocardiograms , and troponin levels for 20 months without evidence of recurrent myocarditis . at 5 months after treatment initiation , the patient noticed grade 1 stiffness and discomfort in his knees , ankles , hands , and bilateral wrists . 
differential diagnosis favored an autoimmune process , with an elevated erythrocyte sedimentation rate of 77 mm / h ( normal , 10 mm / h ) and a c - reactive protein level of 98.0 mg / l ( normal , 6 mg / l )  . 
within 24 hours of initiating corticosteroids for myocarditis , he experienced near - complete resolution of arthritic symptoms . autoimmune hepatitis at 4 months after discontinuation of immunotherapy , and within 3 weeks of completing the initial corticosteroid taper for myocarditis and arthritis , the patient was admitted for asymptomatic grade 3 transaminitis , with an alt level of 990 u / l ( normal , 60 u / l ) and an ast level of 791 u / l ( normal , 42 u / l )  . he was treated with high - dose iv methylprednisolone followed by prednisone 1 mg / kg orally ( tapered over 10 months ) with rapid improvement in liver function tests . 
work - up was negative for cytomegalovirus ; epstein - barr virus ; and hepatitis a , b , c , d , and e infections . follow - up imaging revealed two residual 18f - fdgpost - treatment petnegative liver lesions ( 1 cm and 0.6 cm ; fig 4b )  . 
computed tomography ( ct ) scan of abdomen / pelvis ( a ) 6 weeks after resection of primary tumors ( two lesions , largest was 1.9 cm ) , prechemotherapy ; ( b ) after two cycles of carboplatin / etoposide ( at least 10 lesions , largest was 3 cm ) ; ( c ) after three cycles of pembrolizumab ; and ( d ) after 11 cycles ( 5 months ) of pembrolizumab . responses to checkpoint blockade in ls are hypothesized to be the result of higher mutational load as a result of mmr deciency , which is associated with more mutationassociated neoantigens . 
his arthritis is controlled with methotrexate , and he remains on insulin for type 1 diabetes mellitus and on levothyroxine for hypothyroidishis myocarditis and hepatitis are in remission . discussion presence of a germline mutation in the mmr gene mlh1 with loss of the wild - type allele in the nec component suggests that the nec developed as a consequence of ls in this patient . this case , coupled with data suggesting that approximately 10%26 - 29 of gi necs ( including mixed adenoneuroendocrine carcinomas ) are msi - h ( predominantly from mlh1 methylation ) , underscores the need to consider ls in patients with colorectal nec and the potential value of msi testing in these tumors . 
checkpoint inhibitor ( cpi ) therapy is compelling given the paucity of treatments for platinum - refractory colorectal nec , the tissue / site - agnostic approval of pembrolizumab for msi - h tumors , 30 and evidence suggesting that cpis have activity in mmr - decient / msi - h cancers whether associated with ls or developing sporadically ( eg , in the setting of mlh1 promoter methylation31 - 33 )  . our patient experienced ve iraes . 
regarding immunotherapy - related diabetes , one series suggested that gad65 autoantibodies were present in 60% of patients and that a small proportion harbored a cd8 + t - cell response to a t1dm antigen.34 , 35 gad65 autoantibodies were absent in our patient , suggesting a lower probability of undiagnosed autoimmune disease and underscoring the need for validated markers of response and toxicity for patients treated with cpis.36 the relationship between toxicity and efcacy remains ill dened37 ( appendix )  . 
whether underlying ls increased the risk for iraes is unclear , but a germline mlh1 mutation could theoretically predispose a patient to mutations in normal tissue that are immunologically recognized . 
however , previous reports of cpi therapy in patients with msi - h tumors have not suggested a higher incidence of iraes in this population.5 , 31 , 32 , 38 the patient was treated with a relatively high dose ( 10 mg / kg iv every 2 weeks ) of pembrolizumab compared with the us food and drug administration approved dose for msi - h cancers ( 200 mg iv every 3 weeks ) ; this difference also may have contributed to iraes . jco precision oncology fig 3 . 
n engl j med 363 : 711 - 723 , 2010 topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of antipd - 1 antibody in cancer . 
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vijayvergia n , dasari a , ross ea , et al : pembrolizumab ( p ) monotherapy in patients with previously treated metastatic high grade neuroendocrine neoplasms ( hg - nens )  . 
mulvey c , raj np , chan ja , et al : phase ii study of pembrolizumab - based therapy in previously treated extrapulmonary poorly differentiated neuroendocrine carcinomas : results of part a ( pembrolizumab alone )  . 
kaufman hl , russell js , hamid o , et al : updated efcacy of avelumab in patients with previously treated metastatic merkel cell carcinoma after 1 year of follow - up : javelin merkel 200 , a phase 2 clinical trial . 
kervarrec t , samimi m , gaboriaud p , et al : detection of the merkel cell polyomavirus in the neuroendocrine component of combined merkel cell carcinoma . virchows arch 472 : 825 - 837 , 2018 24 . 
j immunother cancer 5 : 40 , 2017 jesinghaus m , konukiewitz b , keller g , et al : colorectal mixed adenoneuroendocrine carcinomas and neuroendocrine carcinomas are genetically closely related to colorectal adenocarcinomas . 
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galon j , costes a , sanchez - cabo f , et al : type , density , and location of immune cells within human colorectal tumors predict clinical outcome . 
llosa nj , cruise m , tam a , et al : the vigorous immune microenvironment of microsatellite instable colon cancer is balanced by multiple counter - inhibitory 313 : 1960 - 1964 , 2006 checkpoints . 
strosberg jr , coppola d , klimstra ds , et al : the nanets consensus guidelines for the diagnosis and management of poorly differentiated ( high - grade ) extrapulmonary neuroendocrine carcinomas . 
 checkpoint blockade in msi - high neuroendocrine carcinoma appendix summary us food and drug administration approvals of immunotherapy in may 2017 , the us food and drug administration approved pembrolizumab for unresectable or metastatic microsatellite instability high ( msi - h ) or mismatch repairdecient solid tumors that have progressed on prior standard treatment . 
in august 2017 , nivolumab was approved for msi - h colorectal cancer . modest activity has been demonstrated in advanced small - cell lung cancer , leading to drug approvals in rst - line ( atezolizumab plus chemotherapy ) and platinum - refractory settings.12 , 13 , 20 - 22 checkpoint inhibitors have an established role in merkel cell carcinoma , which is a virally mediated disease.21 - 23 beyond that , the role of immunotherapy in extrapulmonary neuroendocrine carcinomas ( necs ) remains ill dened . 
however , three recent pilot studies suggest minimal activity ( response rate , 10% ) of singleagent checkpoint inhibitors in unselected patients with extrapulmonary necs.15 - 17 a growing body of literature has served to clarify the nature and optimal management of immune - related adverse events . 
some reports suggest that patients with grade 3 immune - related adverse events experience longer median time to progression and higher radiographic response . recent biomarker data suggest a high rate of programmed death 1 ( pd1 ) / programmed death ligand 1 expression in poorly differentiated necs of the gi tract ( roberts ja , et al : hum pathol 70 : 49 - 54 ) and a greater proportion of msi - h in high - grade necs , mixed adenoneuroendocrine carcinomas , and insulinomas than in low - grade gastroenteropancreatic neuroendocrine tumors ( weber mm , fottner c : oncol res treat 41 : 306312 , 2018 )  . 
biegel , phd1 , 2 introduction molecular alterations are increasingly becoming clinically useful adjuncts to histology and immunohistochemistry in the classication of pediatric cns tumors.1 , 2 in particular , mutations in idh , tp53 , braf , and histone h3 genes are diagnostic and prognostic in gliomas.2 , 3 however , because of the large and growing list of molecular alterations in brain tumors , targeted approaches to molecular testing , such as sanger sequencing , may fail to capture the driver alteration in a sample . 
despite recent advances in the classication of pediatric cns neoplasms , 2 integrated histopathologic and molecular diagnoses are challenging in many cases.1 powerful , genome - wide approaches used for molecular diagnosis include chromosomal microarray ( cma ) for the identication of copy - number alterations and next - generation sequencing ( ngs ) for single - nucleotide variants , insertions and deletions , and / or gene fusions . these methods benet from surveying a larger portion of the genome than single - gene testing approaches as well as an ability to identify novel alterations . 
recent studies have highlighted the clinical utility of routine proling of pediatric brain tumors with cma and / or ngs approaches.4 - 7 we present the case of a 7 - week - old girl found to have a large intraparenchymal mass in the right frontoparietal region of the brahistopathologic and cma analyses were not diagnostic for a specic subtype of pediatric brain tumor , although a breakpoint in met was identied with cma . 
further study of this tumor with an ngs panel designed for pediatric malignancies , oncokids ( oncomine childhood cancer research assay ; thermo fisher scientic , waltham , ma ) , identied a novel and targetable tripartite motif containing 24 ( trim24 ) - met gene fusion consistent with a diagnosis of high - grade glioma . 
computed tomography ( ct ) of the head revealed a large right parietal mass with central hemorrhage , associated 12 - mm midline shift , and obstructive hydrocephalus ( fig 1 )  . 
she was airlifted to the local childrens hospital , where she underwent emergent craniotomy for frontal external ventricular drain placement , partial evacuation of intracranial hemorrhage , and partial resection of the mass . 
intraoperative pathology consultation with frozen section interpretation showed a high - grade malignant neoplasextensive blood loss limited the extent of resection . postoperative course her immediate postoperative course was complicated by critically elevated intracranial pressures despite aggressive interventions . 
she died on postoperative day 5 . felt methods informed consent was obtained from the guardian before collection of tumor specimens for further analysis of dna and rna using cma and ngs . 
dna was extracted from frozen tumor tissue using the qiagen gentra puregene tissue kit , and rna was extracted with the qiagen rneasy mini rna extraction kit ( qiagen , valencia , ca )  . 
analysis of dna and rna was performed with the oncokids panel , a comprehensive dnaand rna - based ngs panel for pediatric malignancies , as described previously.8 cma analysis of tumor dna was performed according to manufacturer protocol ( oncoscan ; thermo fisher scientic ) .9 the trim24 - met fusion was conrmed by reverse transcription polymerase chain reaction and sanger sequencing . 
overall , these features were consistent with a high - grade neuroepithelial tumor . molecular findings chromosomal microarray analysis of the tumor specimen demonstrated gain of chromosomes 2 , 3 , 5 , 7 , 8 ( four copies ) , 9 , and 10 ( fig 3a )  . 
there was a 482 - kb area of high copy - number gain identied at 8q23.3 that overlapped the csmd3 gene ; the clinical signicance of this alteration was unclear . 
however , a small alteration at this locus could not be ruled out . oncokids analysis of the tumor sample revealed a gene fusion between exon 12 of trim24 ( enst00000415680 ) and exon 15 of met ( enst00000397752 ; fig 3c ) in 110 , 747 of 2 , 575 , 589 mapped reads . 
no variants of strong or potential clinical signicance were identied from the analysis of the dna data from oncokids , including variants within tp53 , braf , pik3ca , h3f3a , hist1h3b , and atrx . 
there is marked right cerebral hemisphere edema as well as mass effect with associated hydrocephalus and right to left midline shift . synthesized from 200 ng of total rna with the superscript iii rst - strand synthesis system ( thermo fisher scientic ) with oligo ( dt ) , followed by amplication with gene - specic primers . 
there was patchy expression of gfap ( fig 2c ) and olig2 and no immunoreactivity for neuron - specic enolase or synaptophysthe tumor was also immunonegative for ema , cytokeratin , smooth muscle actin , plap , immunoreactivity for smarcb1 and afp , and cd99 . smarca4 was retained in tumor cell nuclei . immunostaining for p53 ( d07 ) showed strong expression in a majority of tumor cells ; however , there was no corresponding tp53 deletion or point mutation identied with cma or the oncokids panel ( described in molecular findings )  . 
ki67labeling index exceeded 25% ( fig 2d )  . in this 7 - week - old patient , histopathologic review was consistent with a high - grade neuroepithelial tumor with an embryonal appearance and patchy expression of gfap and olig2 . 
treatment regimens for pediatric high - grade gliomas and embryonal tumors differ signicantly ; therefore , specic diagnosis is crucial for therapy.10 analysis with oncokids identied a novel trim24 - met gene fusion . 
 ( d ) ki - 67labeling index was high ( range , 25% to 60% )  . by the international cancer genome consortium identied gene fusions involving met in seven cases ( 12% ) .11 one met gene fusion observed in that study , ptprz1 - met , has in secondary also been reported as a recurrent event glioblastoma.12 in the context of cns malignancies , met gene fusions seem to be limited to glial neoplasms.11 , 12 met gene fusions , such as ptprz1 - met , carry an unfavorable prognosis in high - grade gliomas.14 trim24 encodes a protein that functions in mediating transcriptional control via the interaction with specic regions of nuclear receptors.15 trim24 has been observed as a 5 ( cid : 1 ) partner with several different driver fusion genes , including braf , fgfr1 , ntrk2 , and ret.16 - 19 the nding of a trim24 - met gene fusion expands the spectrum of met gene fusions in pediatric gliomas . 
this large sefusion has not been reported in several quencing efforts or in publicly available databases such as cosmic ( catalogue of somatic mutations in cancer ) .12 , 20 , 21 the ptprz1 - met fusion has been shown to increase met expression , 22 and several tyrosine kinase inhibitors have been or are currently in clinical trials for met - overexpressed or met - amplied cancers.23 - 25 one pediatric patient with ptprz1 - met fusionpositive glioblastoma experienced substantial tumor volume reduction after treatment with crizotinib.11 unfortunately , that child ultimately acquired resistance to met inhibition.11 it is possible that novel tyrosine kinase inhibitors or inhibition by multiple receptor tyrosine kinase inhibitors may be more effective for met inhibition than crizotinib.26 the patient described in our report died before met inhibition could be attempted ; however , routine molecular proling for met fusions should expand the therapeutic options for a signicant fraction of children with cns tumors . in this case , information from histopathology , ultrastructural analysis , and cma studies enabled the diagnosis of a high - grade neuroepithelial tumor with a few features suggestive of glial differentiation . 
 ( a ) whole - genome view from oncoscan chromosomal microarray ( cma ) in nexus copy number software ( version 9.0 ; biodiscovery , el segundo , ca ) demonstrating the copy - number gains of chromosomes 2 , 3 , 5 , 7 , 8 , 9 , and 10 . 
 novel trim24 - met fusion in a neonatal brain tumor such as ptprz1 - met , have been reported to demonstrate more aggressive biologic behavior , and unfortunately , our patient died soon after tumor resection.12 for future patients diagnosed with high - grade gliomas harboring the trim24 - met gene fusion , available therapeutic options would include inhibitors of met , such as crizotinib or cabozantinib.13 integration of the information from histopathologic , copynumber , and sequencing analyses enabled a substantial improvement in the diagnostic , prognostic , and therapeutic understanding of our patients tumor . 
hiemenz consulting or advisory role : loxo oncology travel , accommodations , expenses : thermo fisher scientic no other potential conicts of interest were reported . references aldape k , pster sm : next - generation molecular diagnostics , in berger ms , weller m ( eds ) : handbook of clinical neurology . 
cambridge , ma , elsevier , 2016 , pp 121 - 130 louis dn , perry a , reifenberger g , et al : the 2016 world health organization classication of tumors of the central nervous system : a summary . 
adv anat pathol 25 : 143 - 171 , 2018 roth jj , santi m , rorke - adams lb , et al : diagnostic application of high resolution single nucleotide polymorphism array analysis for children with brain tumors . cancer genet 207 : 111 - 123 , 2014 shao l , miller s , koschmann c , et al : clinical application of whole genome array improves the diagnosis of pediatric brain tumors . 
int j surg pathol 25 : 688 - 695 , 2017 sahm f , schrimpf d , jones dt , et al : next - generation sequencing in routine brain tumor diagnostics enables an integrated diagnosis and identies actionable targets . 
worst bc , van tilburg cm , balasubramanian gp , et al : next - generation personalised medicine for high - risk paediatric cancer patients : the inform pilot study . eur j cancer 65 : 91 - 101 , 2016 8 . 
j mol diagn 20 : 765 - 776 , 2018 foster jm , oumie a , togneri fs , et al : cross - laboratory validation of the oncoscan ffpe assay , a multiplex tool for whole genome tumour proling . 
j pediatr hematol oncol 38 : 249 - 260 , 2016 international cancer genome consortium pedbrain tumor project : recurrent met fusion genes represent a drug target in pediatric glioblastoma . 
bao zs , chen hm , yang my , et al : rna - seq of 272 gliomas revealed a novel , recurrent ptprz1 - met fusion transcript in secondary glioblastomas . 
belloni e , trubia m , gasparini p , et al : 8p11 myeloproliferative syndrome with a novel t ( 7 ; 8 ) translocation leading to fusion of the fgfr1 and tif1 genes . 
davies kd , ng tl , estrada - bernal a , et al : dramatic response to crizotinib in a patient with lung cancer positive for an hla - drb1 - met gene fusion . 
gazzaniga et al we are grateful for your comments on our recent publication1 that highlighted that nearly 50% of the patients with ras - mutated metastatic colorectal cancer and prior chemotherapy could display wildtype ras status in the circulating tumoral dna ( ctdna ) , and benet from the late introduction of an antiepidermal growth factor receptor ( egfr ) .2 we indeed acknowledge that your team had worked in a similar direction , and appropriately cited the report that your group published in 2019.3 this article also includes results from preliminary ndings in abstract forms . 
both of our works , as well as that from moati et al , 4 conrm the principle of expected efcacy from targeting egfr in the late stage of treatment of patients with ras - mutated colorectal cancer , if their liquid biopsy does not identify any ras mutation in the ctdna.2 - 4 however , there is a broad discrepancy in the rates of patients without ras mutation detection in plasma between these studies , ranging from 9 / 16 ( 56% ) , 2 through 5 / 11 ( 45% ) 3 to 8 / 36 ( 22% ) , 4 as also discussed in your opinion paper.5 a critical issue involves the conrmation of circulating tumoral dna in the absence of ras mutation , which could be reached through the detection of a persistent somatic mutation3 or the occurrence of wif1 / npy methylation.4 however , we concur and admit that these and other methods have intrinsic limitations , such that no standard one can currently ascertain the presence of circulating tumor dna in the absence of detected ras mutation.5 moreover , although their application drastically reduced the ras mutation conversion rate down to 6.6% - 14% , 3 , 4 this did not impair the fact that the introduction of an antiegfr apparently extended median progression - free survival to nearly 6 months in previously treated patients from both studies.2 , 3 therefore , we feel that two important issues need to be jointly addressed to advance the current guidelines for anti - egfr indication for metastatic colorectal cancer . 
gazzaniga p , nicolazzo c , caponnetto s , et al : about ras mutation clearance in plasma ctdna from ras - mutant colorectal cancer patients . jco precis oncol , 2021 2 . 
bouchahda m , saffroy r , karaboue a , et al : undetectable ras - mutant clones in plasma : possible implication for anti - egfr therapy and prognosis in patients with ras - mutant metastatic colorectal cancer . 
raimondi c , nicolazzo c , belardinilli f , et al : transient disappearance of ras mutant clones in plasma : a counterintuitive clinical use of egfr inhibitors in ras mutant metastatic colorectal cancer . 
nicolazzo c , belardinilli f , caponnetto s , et al : why the therapeutic impact of ras mutation clearance in plasma ctdna deserves to be further explored in metastatic colorectal cancer . 
in metastatic melanoma , the extent to which ctdna reflects changes in metabolic disease burden assessed by 18f - labeled fluorodeoxyglucose positron emission tomography ( fdg - pet ) is unknown . 
we assessed the role of ctdna analysis in combination with fdg - pet to monitor tumor burden and genomic heterogeneity throughout treatment . patients and methods we performed a comprehensive analysis of serial ctdna and fdg - pet in 52 patients who received systemic therapy for metastatic melanoma . 
next - generation sequencing and digital polymerase chain reaction were used to analyze plasma samples from the cohort . results ctdna levels were monitored across patients with mutant braf , nras , and braf / nras wild type disease . 
tert promoter mutant ctdna levels also paralleled changes in tumor burden , which provide an alternative marker for disease monitoring . of note , subcutaneous and cerebral disease sites were not well represented in plasma . 
the use of mitogen - activated protein kinase inhibitors ( mapki ) in patients with advanced braf mutant melanoma1 - 3 and , more immune checkpoint inhibitors4 , 5 has recently , led to improved overall survival . 
mcarthur shahneen sandhu sarah - jane dawson invasive and metastatic disease.8 moreover , clonal evolution of melanoma continues to occur during systemic therapy , with diverse resistance mechanisms observed at relapse.9 in patients with melanoma who receive systemic therapy , tumor burden and treatment responses currently are assessed through clinical evaluation , serial lactate dehydrogenase ( ldh ) levels , 10 and radiologic imaging with 18f - labeled fluorodeoxyglucose positron emission tomography ( fdgpet ) .11 fdg - pet provides unique functional information that enables an accurate assessment of changes in metabolic disease activity and tumor volume throughout treatment.11 although current imaging methods are effective at monitoring treatment response , complementary strategies are needed to assess molecular alterations and capture genomic evolution in the context of therapeutic resistance to guide treatment decisions . circulating tumor dna ( ctdna ) has emerged as a noninvasive biomarker to track tumor burden and allow monitoring of the cancer genome in blood across several malignancies.12 - 22 in melanoma , the relationship between ctdna levels and tumor burden as assessed by fdg - pet is unknown . 
three of the 52 patients also consented to multiregional tumor sampling after death as part of a rapid autopsy progratumor material and matched normal and plasma dna were retrospectively analyzed through targeted amplicon ( ta ) sequencing and digital polymerase chain reaction ( dpcr ) as well as through whole - exome sequencing ( wes ) and low - coverage wholein selected genome sequencing ( lc - wgs ) cases . 
the + symbol denotes the development of new sites of disease . statistics nonparametric spearman rank correlation was used to investigate associations between continuous variables , and the mann - whitney u test was used to assess associations between continuous and dichotomous variables . 
time to event was measured from the start of treatment to the first documentation of progression on fdg - pet , with the relative hazard ratio computed for each comparison . results ctdna is detectable across various molecular subtypes of metastatic melanoma fifty - two patients with a median age at diagnosis of 61 years ( range , 24 to 83 years ) were serially monitored with fdg - pet , ldh , and ctdna during therapy ( data supplement )  . 
on the left , columns correspond to patients and are ordered by mutational subtype and disease burden as assessed by 18f - labeled fluorodeoxyglucose positron emission tomography ( fdg - pet ) imaging . 
rows indicate the pretreatment fdg - pet disease volume , pretreatment lactate dehydrogenase ( ldh ) level , and pretreatment circulating tumor dna ( ctdna ) levels detected by dpcr ( both absolute and fractional concentrations shown )  . 
mutations are shown if they were found in a pretreatment tumor sample ( pink ) , in plasma ( green ) , or in both a pretreatment tumor sample and plasma ( gold )  . the type of pretreatment tumor material used for targeted amplicon sequencing in each patient is indicated . 
for patients mel - 70 , - 80 , and - 81 , pretreatment ctdna levels were not detectable ( left ) , but ctdna was detected at subsequent time points after treatment ( middle )  . 
 ( % ) primary metastatic mutation detected in : tumor plasma tumor only plasma only 2 - 10 10 - 50 50 - 100 site of disease present absent pretreatment ldh level ( ratio upper / normal ) ( 71% ) and seven patients ( 13% ) , respectively , and eight patients ( 15% ) were braf / nras wt . ctdna was detected in 39 ( 80% ) of 49 patients by ta sequencing and / or dpcr ( fig 1 )  . 
screening of matched plasma detected tert promoter mutations in 27 ( 75% ) of 36 patients . absolute levels of ctdna before treatment show variation according to sites of disease pretreatment plasma was available in 41 of 49 patients ( fig 1 )  . 
pretreatment ctdna levels varied among patients ( median , 1 , 112 copies / ml of plasma ; range , 63 to 97 , 000 copies / ml of plasma ) , which represented between 0.1% and 82% ( median , 5.4% ) of total circulating dna . 
of note , although a strong correlation existed between high metabolic disease burden as assessed by fdg - pet and high levels of ctdna before treatment , several discordant cases were observed ( fig 2 )  . 
we hypothesized that discordance may relate to a differential release of ctdna into the peripheral circulation dependent on specific anatomic sites of disease . consistent with this premise , patients with visceral , bone , or lymph node involvement often displayed high levels of ctdna despite at times low disease burden as detected by fdg - pet . 
in contrast , individuals with extensive subcutaneous disease consistently showed low levels of ctdna despite measurable levels of disease burden as assessed by fdg - pet ( data supplement )  . 
these findings are consistent with other studies that have shown low ctdna levels despite extensive cerebral disease.12 , 25 serial ctdna monitoring correlates with tumor burden and treatment response as assessed by fdg - pet we investigated whether ctdna levels correlate with changes in disease burden throughout treatment as assessed by ldh and fdg - pet . 
serial ctdna analysis was performed on 312 plasma samples by using dpcr for selected mutations identified from ta sequencing and compared with serial ldh measurements ( n = 329 ) and fdg - pet ( n = 244 ) across the series . 
of note , serial changes in mutant braf or nras ctdna levels closely reflected metabolic responses across multiple therapies , including mapki and immunotherapies ( figs 3b and 3c )  . 
by using a cox proportional hazards regression model , we identified that patients with an early decrease in ctdna levels ( between baseline and 1 to 4 weeks on treatment ) had improved pfs compared with patients where ctdna levels remained unchanged or increased over time ( fig 3e )  . 
similar findings were observed for patients who demonstrated an early decrease in tumor volume as assessed by fdg - pet ( fig 3e )  . although baseline levels of ldh were prognostic ( data supplement ) , no significant association between pfs and an early decline in ldh levels after treatment were found ( fig 3e )  . 
3 months were found to have a significantly greater log - fold reduction in ctdna levels at 1 to 4 weeks after treatment initiation compared with those who had a pfs , 3 months ( p = .03 ; fig 3f )  . 
rapid responses by ctdna were most notable after mapki therapy in keeping with the known response kinetics of these agents . tert promoter mutant ctdna provides an alternative marker for disease monitoring we next evaluated whether tert promoter mutations could be serially monitored in ctdna and whether levels correlated with disease burden . 
 ( a ) high ctdna levels detected in three patients with melanoma ( mel - 74 , mel - 2 , and mel - 111 ) , with 18f - labeled fluorodeoxyglucose positron emission tomography ( fdg - pet ) scans indicating only small - volume disease ( mel - 74 , small liver and adrenal deposits ; mel - 2 and mel - 111 , solitary liver deposit )  . 
 ( c ) low ctdna levels detected in three patients who presented with high - volume subcutaneous disease ( mel - 122 , mel - 92 , and mel - 4 ) as shown by fdg - pet imaging . 
 ( d ) low to undetectable levels of ctdna in two patients with isolated brain disease ( mel - 120 and mel - 5 ) as indicated by magnetic resonance imaging . 
all bar graphs are plotted to the same y - axis and on a logarithmic scale . mutations followed the same dynamic changes in ctdna as braf or nras mutations by analyzing plasma from all braf and nras mutant cases that were also tert promoter mutant ( n = 33 )  . 
paired plasma ( and tumor biopsy specimens where available ) before treatment and at disease progression were analyzed by using ta sequencing and lc - wgs / wes in selected cases . 
acquired nras mutations were the predominant genomic alteration identified through analysis of ctdna at the time of disease progression , as illustrated in patient mel - 76 ( fig 5a )  . 
circulating tumor dna ( ctdna ) levels correlate with the kinetics of 18f - labeled fluorodeoxyglucose positron emission tomography ( fdg - pet ) disease burden and patterns of response to therapy . 
 ( b ) dynamic changes in ctdna levels correlate with response to therapy as assessed by fdg - pet imaging in a patient with a braf v600k mutation ( mel - 97 ) who showed a complete metabolic response to dabrafenib + trametinib ( dab + tram ) treatment ; ( c ) a patient with an nras q61k mutation ( mel - 36 ) who displayed an initial response to several lines of therapy ( dedn6526a , radiotherapy [ rt ] / surgery [ sur ] , and temozolomide [ temo ] ) followed by disease progression before commencement of pembrolizumab ( pembro ) and then a mixed response to pembro treatment ; and ( d ) a patient with braf / nras mutant wild type ( mel - 39 ) with ctdna levels monitored through an rac1 p29s mutation during dedn6526a , rt , and abraxane treatment . 
wholebody fdg - pet scans are shown for each patient . before a routine fdg - pet scan that confirmed progressive metabolic disease , which highlights the ability of ctdna analysis to identify early treatment failure . 
for example , in patient mel - 31 , ta sequencing of plasma samples before and after vemurafenib + cobimetinib treatthe braf ment confirmed the presence of v600e mutation in addition to an increasing plasma abundance of map2k1 and pten mutations ( fig 5b )  . 
although the map2k1 e203k mutation was a likely cause for resistance in this individual , pten mutations also have been associated with diminished response to mapki therapy and may have contributed to the rapid emergence of the therapeutic resistance observed.26 in patient mel - 7 , ta sequencing and dpcr showed that changes in ctdna levels of two preexisting mutations ( braf and cdkn2a ) closely paralleled the dynamics of response and progression documented on fdg - pet ( fig 5c )  . 
 ( e ) global responses to therapy indicated by a cox proportional hazards regression model that assessed the relationship between progression - free survival ( pfs ) and the change in ctdna levels , fdg - pet volumes , or ldh levels between the pretreatment and early assessment time points . 
 + , development of new sites of disease ; cmr , complete metabolic response ; hr , hazard ratio ; mapki , mitogen - activated protein kinase inhibitor ; mmr , mixed metabolic response ; nivo , nivolumab ; pmd , progressive metabolic disease ; pmr , partial metabolic response ; smd , stable metabolic disease . akt1 mutation that represented a potential resistance mechanism to explain the short - lived response after recommencement of vemurafenib.27 finally , braf amplification is considered a common resistance mechanism to mapki therapy27 and may confound quantification of mutant braf ctdna levels for disease monitoring . 
therefore , we explored the ability of ctdna analysis to detect the presence of copy number alterations by performing plasma lc - wgs / wes in three patients treated with mapki therapy . 
these findings highlight the ability of plasma analysis to detect this mode of therapeutic resistance and emphasize the advantage of tracking tert mutations in parallel to reflect changes in tumor burden accurately . plasma dna captures spatial heterogeneity across multiple disease sites increasing appreciation of tumor heterogeneity has revealed the importance of assessing the full spectrum of molecular alterations present across multiple disease sites to appropriately guide treatment decisions . 
in contrast , plasma may overcome these limitations because it may represent a summation of molecular alterations across multiple disease sites.28 thus , we first sequenced multiple tumors collected at autopsy from patient mel - 99 with braf v600e mutant melanoma treated with vemurafenib ( data supplement )  . 
 ( b ) time course of a patient with braf / nras mutant wild type disease ( mel - 67 ) with ctdna levels tracked through a tert c . - 124 mutation during dedn6526a and pembrolizumab ( pembro ) treatment . 
 ( d ) time course of a patient with a braf v600e mutation ( mel - 28 ) with ctdna levels monitored through both a braf v600e and a tert c . - 124 mutation in plasma during vemurafenib ( vem ) treatment and radiotherapy ( rt )  . 
cmr , complete metabolic response ; pmd , progressive metabolic disease ; pmr , partial metabolic response ; smd , stable metabolic disease . subcutaneous metastasis , respectively , which were not detectable in either a bowel or mesenteric sample . 
mutant braf ctdna levels remained elevated throughout treatment , with targeted amplicon ( ta ) sequencing of plasma detecting the emergence of an acquired nras q61k mutation 18 weeks after starting treatment . 
 ( b ) ctdna analysis indicated acquired resistance to treatment in patient mel - 31 who presented with metastatic braf v600e positive disease that involved left - side pelvic lymph nodes , subcutaneous deposits , and solitary bone and lung metastases . 
the patient commenced combination therapy with vemurafenib and cobimetinib ( vem + cobi ) after disease progression in the pelvis with single - agent vem , which resulted in a short - lived ( 4 weeks ) partial metabolic response ( pmr ) ; the patient died 10 weeks after starting combination therapy as a result of rapid disease progression . 
 ( c ) this patient with braf v600k mutant disease ( mel - 7 ) initially presented with extensive disease over the left - side scapula and multiple pulmonary metastases and commenced vem for 2 months . 
 ( d ) patient mel - 1 initially presented with bulky disease of the bowel , lung , and lymph nodes and several sites of subcutaneous disease , which were braf v600e mutant positive . 
braf amplification was detected by whole - exome sequencing of a post - treatment bowel metastasis and low - coverage whole - genome sequencing of the plasma sample taken at disease progression . 
 disease sites but also demonstrates the ability of ctdna to capture genomic heterogeneity from multiple sites of disease that may be missed from a single tissue biopsy specimen . to comprehensively assess the extent to which ctdna was able to reflect spatial heterogeneity across various disease sites , we performed wes on multiregional tumor samples from two additional autopsy cases alongside matched plasma collected close to death ( fig 6 )  . 
for patient mel - 28 , 307 ubiquitous mutations ( present in all tumors ) , 36 shared mutations ( present in two or more tumors ) , and 36 private mutations ( present in only one tumor ) were detected ( fig 6a )  . 
for patient mel - 28 , the limited ability to detect private mutations in plasma was a result of the low mafs ( median maf , 9% for private mutations absent in plasma )  . 
for patient mel - 10 , the higher mafs observed for private mutations not detected in the plasma ( median maf , 38% ) compared with patient mel - 28 was likely a result of the limited ability to detect brain - specific private mutations ( median maf , 49% v 22% across other sites )  . discussion over the past decade , a major paradigm shift has occurred in the treatment of metastatic melanoma through clinical implementation of targeted therapeutics and immune checkpoint inhibitors . 
one potential avenue is through the use of ctdna analysis to provide patient - specific genomic information that can be monitored in real time during clinical management . mel - 28 ubiquitous shared private brain hilar lymph node liver pouch of douglas brain liver small bowel plasma hilar lymph node pouch of douglas liver brain plasma small bowel liver brain mel - 10 ubiquitous shared private 80% - 100% 60% - 80% 40% - 60% 20% - 40% 0% - 20% fig 6 . 
inference of the genomic architecture of disease as determined by whole - exome sequencing of multiregional tumor biopsy specimens and matched plasma from ( a ) patient mel - 28 and ( b ) patient mel - 10 . 
 previous reports16 - 22 have provided increasing evidence that ctdna has prognostic value in metastatic melanoma , with ctdna levels correlating with established measures of disease burden ( eg , ldh )  . 
this study provides the first correlative analysis to our knowledge that compares ctdna and fdg - pet imaging in this disease . fdg - pet has unique advantages in monitoring treatment responses in metastatic melanoma compared with other radiologic imaging techniques29 - 31 because it enables whole - body imaging with high sensitivity and specificity and can provide an early functional readout of response to targeted therapies.11 we reveal that ctdna levels correlate closely with changes in metabolic disease burden assessed through fdgpet and show that an early decline in ctdna levels provides an important alternative indicator of treatment response , which predicts patients with prolonged pfs . to fdgpet , a key strength of ctdna analysis is its ability to allow noninvasive sampling of the changing tumor genomic landscape under the selective pressure of therapy . 
in conjunction with other studies , 17 , 18 we highlight the ability of serial ctdna analysis to detect resistance mechanisms to mapki therapy to assist with the early identification of treatment failure and allow consideration of alternative therapeutic strategies . in contrast we monitored ctdna across all molecular subtypes of melanoma . 
previous reports have demonstrated the ability to measure ctdna levels through dpcr of braf and nras mutations ; however , the limitation of this approach in patients with copy number alterations that involve these genes has not been previously addressed . 
braf and nras amplifications are known to occur frequently in melanoma ( approximately 7% and 3% , respectively ) , 6 and in the current study , we show the advantage of plasma analysis in assessing the emergence of copy number alterations . 
the data highlight that tracking tert promoter mutations , in addition to braf and nras , offers an improved strategy for disease monitoring . in conclusion , ctdna can play a vital complementary role to functional imaging in metastatic melanoma because it can be used to monitor tumor response kinetics and can capture the mutational spectrum from many sites of disease . 
a significant limitation to ctdna monitoring is that subcutaneous and cerebral disease sites are not well represented in the plasma , and recognition of this limitation is pivotal if ctdna monitoring is to be integrated into routine clinical practice . 
 carleen cullinane no relationship to disclose damien kee no relationship to disclose benjamin brady consulting or advisory role : bristol - myers squibb , novartis , merck speakers bureau : bristol - myers squibb , merck travel , accommodations , expenses : bristol - myers squibb , merck fergal kelleher travel , accommodations , expenses : bristol - myers squibb mark a . 
mcarthur pfizer , celgene , ventana medical systems travel , accommodations , expenses : bristol - myers squibb , roche , novartis shahneen sandhu honoraria : bristol - myers squibb , amgen consulting or advisory role : bristol - myers squibb speakers bureau : bristol - myers squibb , merck sarah - jane dawson no relationship to disclose acknowledgment we thank the anatomical pathology department from the peter maccallum cancer centre and all other participating hospitals for assisting in the acquisition of tumor material . 
vergara stock and other ownership interests : genomedx patents , royalties , other intellectual property : co - inventor on three patents pending kenneth doig stock and other ownership interests : csl behring , healthscope jeanette m . 
colebatch no relationship to disclose jason li no relationship to disclose timothy semple no relationship to disclose christopher mintoff no relationship to disclose devbarna sinha no relationship to disclose paul yeh no relationship to disclose maria joao silva no relationship to disclose kathryn alsop no relationship to disclose heather thorne no relationship to disclose david e . 
papenfuss , walter eliza hall institute of medical research , melbourne , victoria , australia . supported by a peter maccallum cancer foundation grant , the national health and medical research council ( program grant app1053792 , project grant app1107126 ) , a pfizer study grant , a gundry perpetual endowment for melanoma research , and a viertel charitable foundation clinical investigator award . 
mcarthur ga , puzanov i , amaravadi r , et al : marked , homogeneous , and early [ 18f ] fluorodeoxyglucose - positron emission tomography responses to vemurafenib in braf - mutant advanced melanoma . 
lipson ej , velculescu ve , pritchard ts , et al : circulating tumor dna analysis as a real - time method for monitoring tumor burden in melanoma patients undergoing treatment with immune checkpoint blockade . 
schreuer m , meersseman g , van den herrewegen s , et al : quantitative assessment of braf v600 mutant circulating cell - free tumor dna as a tool for therapeutic monitoring in metastatic melanoma patients treated with braf / mek inhibitors . 
chang ga , tadepalli js , shao y , et al : sensitivity of plasma brafmutant and nrasmutant cell - free dna assays to detect metastatic melanoma in patients with low recist scores and non - recist disease progression . 
tsao sc , weiss j , hudson c , et al : monitoring response to therapy in melanoma by quantifying circulating tumour dna with droplet digital pcr for braf and nras mutations . 
xi l , pham th , payabyab ec , et al : circulating tumor dna as an early indicator of response to t - cell transfer immunotherapy in metastatic melanoma . 
santiago - walker a , gagnon r , mazumdar j , et al : correlation of braf mutation status in circulating - free dna and tumor and association with clinical outcome across four brafi and meki clinical trials . 
janku f , huang hj , claes b , et al : braf mutation testing in cell - free dna from the plasma of patients with advanced cancers using a rapid , automated molecular diagnostics systemol cancer ther 15 : 1397 - 1404 , 2016 23 . 
de mattos - arruda l , mayor r , ng ck , et al : cerebrospinal fluid - derived circulating tumour dna better represents the genomic alterations of brain tumours than plasma . 
long gv , fung c , menzies am , et al : increased mapk reactivation in early resistance to dabrafenib / trametinib combination therapy of braf - mutant metastatic melanoma . 
 olaparib monotherapy for brip1 - mutated high - grade serous endometrial cancer kohei nakamura , md , phd1 , 2 ; eriko aimono , md1 ; shigeki tanishima , md , phd3 ; mitsuho imai , md , phd1 ; akiko kawano nagatsuma , md , phd1 ; hideyuki hayashi , md , phd1 ; yuki yoshimura , md4 ; kentaro nakayama , md , phd4 ; satoru kyo , md , phd4 ; and hiroshi nishihara , md , phd1 introduction treatment the prognosis for women with high - grade endometrial cancers is poor , with little improvement in the last two decades.1 the mainstay of is surgery lymphadenectomy . ( hysterectomy ) with or without although adjuvant radiotherapy is considered standard for high - risk endometrial cancers , the added value of chemotherapy has been the subject of recent trials . 
recently , other mutations were reported in ovarian cancers , such as those in fanconi anemia genes ( eg , palb2 [ fancn ] , brip1 [ fancj ] , and rad51c ) and other genes involved in hrr ( eg , atm , bard1 , nbn , cdk12 , tp53 , and chek2 ) .2 , 3 poly ( adp - ribose ) polymerase ( parp1 ) is a dna repair enzyme involved in base excision and single - stranded break repair pathways.4 parp1 inhibition in hrrdecient cells blocks single - stranded dna break repair pathways , leaving only double - stranded dna break repair pathways functional . 
this results in synthetic lethality from the loss of homologous recombination and base excision repair , thus activating highly error - prone dna repair pathways , eventually causing cell death.5 , 6 parp inhibitors also trap parp - dna complexes at the replication fork , increase toxic nonhomologous end joining in parp1 - decient cells , and block parp1 / pol - mediated alternative end joining.7 the us food and drug administration ( fda ) has approved three parp inhibitors ( olaparib , rucaparib , and niraparib ) as monotherapies for breast and ovarian cancers . 
after surgery , the patient received six cycles of carboplatin and paclitaxel . there was also evidence of after rst - line chemotherapy , ct indicated stable disease based on recist 1.0 criteria , with only improvements in the cardiophrenic swollen lymph node ( fig 1 )  . 
after six cycles , ct revealed essentially stable disease without iliac in the para - aortic or left improvement swollen lymph nodes ( fig 1 )  . lateral targeted next - generation sequencing of the patients blood and resected specimen was performed using an in - house assay during treatment . 
a tp53 somatic point mutation ( p.r175h ) and somatic frameshift brip1 ( p.q554hfs * 35 ) alterations were detected as pathogenic variants in the tumor ; detailed information is provided in appendix figures a1 and a2 . 
secondary germ line examination found no american college of medical genetics and genomics recommended genes for testing . given her somatic brip1 mutation and ndings indicating loh high status , the potential efcacy of the parp inhibitor olaparib was discussed with the patient . 
9 months of olaparib and showed complete response on her most recent ct . discussion endometrial cancers are categorized into two main histologic types.8 type i endometrial tumors show endometrioid histology and typically express estrogen ( er ) and progesterone ( pr ) receptors . 
in contrast , type ii endometrial tumors do not exhibit endometrioid histology ( predominantly serous histology ) and are associated with poorer prognoses , with a 5 - year overall survival rate of 55%.1 type ii tumors neither express er / pr nor respond to endocrine therapy . 
meanwhile , type i tumors exhibit signicantly more pi3k pathway alterations ( primarily pten and pik3ca mutations ) .9 , 10 in our case , next - generation target panel sequencing results reected the molecular events observed in serous endometrial cancers , such as tp53 mutations . whereas brip1 is implicated in double - stranded dna break repair via hrr pathways , the frequency of brip1 mutations in type ii endometrial tumors remains unclear . in a previous study by heeke et al , 11 the prevalence of recombinationrelated gene mutations homologous across multiple cancer types was investigated in 52 , 426 malignant tumors . 
this has promoted clinical studies of parp inhibitors in contexts other than ovarian cancer . moreover , their potential therapeutic applications might be extended from germ line brca mutations to target a more diverse group of sporadic tumors , such as those with epigenetic disruption of brca1 / 2 function or genetically or epigenetically acquired aberrations in other important hrr pathway constituents.12 there is clinical evidence to support this theory , with olaparib approved by the fda as an alternative for patients with germ line or somatic brca1 / 2 mutations and as maintenance therapy after platinumbased chemotherapy in platinum - sensitive recurrent epithelial ovarian carcinoma , regardless of brca mutation status.13 hrr alterations are associated with brca1 / 2 mutations in high - grade serous endometrial cancers ; however , parp inhibitors await fda approval for this indication , and there are currently no trials of parp inhibitors in patients with endometrial cancers with brca or other hrr - associated genealterations . accumulating evidence indicates that patients with brip1 mutations have hrr deciency and are consequently hypersensitive to parp inhibition.14 brip1 is a brca1interacting protein ( the brip1 - brca1 interaction is important for hrr ) and associates with brca1 as cells progress through the s phase of the cell cycle.15 , 16 brip1 is a dna helicase that interacts with the cooh - terminal brct repeat of brca1 . 
brip1 is associated with the gm1 / 2 checkpoint , as well as the activation of chk1 , regulation of entry into the s phase , and maintenance of genomic stability.16 thus , if the complex involving brca1 and brip1 is involved in tumor suppression , mutations in the genes that encode these proteins should be associated with altered cancer risk . 
recently , three independent dnabased measures of genomic instability reecting underlying tumor homologous recombination dna repair deciency were developed based on loh , telomeric allelic imbalance , and large - scale state transitions.17 - 19 however , we could not determine the homologous recombination deciency score , because the relevant test is not covered by insurance in japan , and therefore , we could not prove this . 
however , we can hypothesize that the brip1 mutation results in hrr deciency and subsequently causes a high loh frequency and scattered allelic imbalance , potentially resulting in good response to parp inhibitors . in conclusion , we describe the case of a 70 - year - old woman exhibiting a durable clinical radiographic response to olaparib . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . support supported by the japan agency for medical research and development under grant no . 
lancet 387 : 1094 - 1108 , 2016 somyajit k , subramanya s , nagaraju g : rad51c : a novel cancer susceptibility gene is linked to fanconi anemia and breast cancer . 
carcinogenesis 31 : 2031 - 2038 , 2010 sigurdsson s , van komen s , bussen w , et al : mediator function of the human rad51b - rad51c complex in rad51 / rpa - catalyzed dna strand exchange . genes dev 15 : 3308 - 3318 , 2001 4 . 
morales j , li l , fattah fj , et al : review of poly ( adp - ribose ) polymerase ( parp ) mechanisms of action and rationale for targeting in cancer and other diseases . crit rev eukaryot gene expr 24 : 15 - 28 , 2014 farmer h , mccabe n , lord cj , et al : targeting the dna repair defect in brca mutant cells as a therapeutic strategy . 
nature 434 : 917 - 921 , 2005 ashworth a : a synthetic lethal therapeutic approach : poly ( adp ) ribose polymerase inhibitors for the treatment of cancers decient in dna double - strand break repair . 
j clin oncol 26 : 3785 - 3790 , 2008 konstantinopoulos pa , ceccaldi r , shapiro gi , et al : homologous recombination deciency : exploiting the fundamental vulnerability of ovarian cancer . 
gynecol oncol 15 : 10 - 17 , 1983 kandoth c , schultz n , cherniack ad , et al : cancer genome atlas research network : integrated genomic characterization of endometrial carcinoma . 
sato k , koyasu m , nomura s , et al : mutation status of rad51c , palb2 and brip1 in 100 japanese familial breast cancer cases without brca1 and brca2 oncogene 26 : 2157 - 2165 , 2007 mutations . 
dong y , hakimi ma , chen x , et al : regulation of brcc , a holoenzyme complex containing brca1 and brca2 , by a signalosome - like subunit and its role in 16 . 
genomic testing was performed on a plessision internal clinical sequencing apparatus ( keio university , tokyo , japan ) , which is used for all genome sequencingrelated analyses in our hospital ( keio university hospital )  . 
this apparatus was used to extract genomic dna from tumor samples and peripheral blood mononuclear cells extracted from patients with cancer , after the provision of consent to undergo comprehensive genomic testing . 
this study was conducted in accordance with the declaration of helsinki and title 45 , us code of federal regulations , part 46 , protection of human subjects , effective december 13 , 2001 . dna quality was checked by calculating the dna integrity number ( din ) using an agilent 2000 tapestation ( agilent technologies , waldbronn , germany ) before conducting targeted amplicon exome sequencing of the 160 genes implicated in cancer using the illumina miseq sequencing platform ( illumina , san diego , ca )  . 
cancer - specic changes in somatic genes , including single - nucleotide variants , insertions / deletions , and copynumber variations were detected and used to determine the tumor mutation burden . 
heterozygous germline mutations in brca1 or brca2 confer up to an 85% lifetime risk of breast and a 15% to 40% risk of ovarian cancer , and they significantly increase the risk of pancreatic , prostate , and male breast cancers.1 tumors in these patients have often lost the wild - type allele and therefore are hr deficient . 
in the absence of a functional copy of the brca gene that maintains dna integrity , the use of error - prone , nonhomologous end - joining repair mechanisms leads to an accumulation of genetic aberrations and promotes carcinogenesis.2 inhibition of poly ( adp - ribose ) polymerase ( parp ) induces synthetic lethality in cells with brca1 or brca2 deficiency , and clinical trials of parp inhibitors have demonstrated responses in brcamutated breast and ovarian cancers.3 the bestdescribed mechanisms of resistance to platinum agents and parp inhibitors in brca1 or brca2 carriers with ovarian cancer are secondary mutations that restore the open reading frame or reversion mutations that restore the wild - type protein.4 , 5 , 6 these mutations are present in more than 40% of recurrent platinum - resistant ovarian cancers and are more common in women with recurrent ovarian carcinoma who were previously treated for breast cancer3 , 6 . 
minimal data exist about resistance to single - agent parp inhibitor therapy in women with breast cancer.7 we report a case of a brca2 mutation carrier who received single - agent parp inhibitor therapy and had subsequent resistance conferred by a reversion mutation identified by targeted capture and massively parallel sequencing . carcinoma of the right breast with multiple positive regional lymph nodes , for which she underwent a mastectomy and axillary node dissection and received adjuvant chemotherapy with fluorouracil , epirubicin , andcyclophosphamidefollowed by tamoxifen for 5 years . 
additional details of her initial care are not available , and cancer surveillance was not performed . after presentation at age 72 with back pain , workup identified a left breast mass with extensive metastatic disease to the bone . 
biopsy of the breast mass confirmed a new primary invasive ductal carcinoma that stained positive for estrogen receptor and progesterone receptor expression and negative for her2 / neu . her disease was staged as ct4an2m1 , and she started anastrazole monotherapy . 
 genomic dna isolated from peripheral blood to evaluate for germline mutations in brca1 and brca2.8 the uw - oncoplex assay ( laboratory medicine , university of washington ) was used to perform whole - exome deep sequencing and copy number variation analysis to identify somatic mutations in dna isolated from formalin - fixed , paraffinembedded tumor tissue.8 , 9 neoplastic cellularity was assessed by estimating the fraction of neoplastic to nonneoplastic nuclei on a hematoxylin and eosin stained section by a trained pathologist . 
predicted allelic frequency for the retained alleles of heterozygous germline variant of brca2 ( and reference single nucleotide polymorphism [ snp ] 2126042 ) was calculated with the following formula : [ ( tumor percentage ) + ( nontumor percentage ) ] 4 [ ( tumor percentage ) + 2 ( nontumor percentage ) ]  . 
predicted allelic frequency for the wild - type brca2 ( and reference snps 1799943 , 1799955 , and 1801406 ) was calculated as 100 2 the predicted allelic frequency of the variant . the fred hutchinson cancer research center consortium institutional review board approved this study . 
the reference snps were mapped to separate brca2 alleles with a predicted germline allelic frequency of approximately 50% ( table 1 )  . the pre - veliparib sample ( a bony lesion ) had a lower neoplastic cellularity ( 25% ) than the postveliparib sample ( chest wall ; 78% )  . 
the variant allele frequency of rs2126042 , present on the same copy of the mutated brca2 allele , was 60% in the preand 92% in the post - treatment sample . 
the allelic frequency of mutated brca2 in the pre - treatment sample is consistent with the loss of heterozygosity of the wild - type allele ( table 1 ; fig 1 )  . 
in the posttreatment sample , the marked discrepancy in the allelic frequency of the mutated brca2 ( 50% ) and rs126042 ( 92% ; both expected to be on the same allele ) , along with the low allelic frequency of other heterozygous germline snps ( predicted frequency , approximately 18% ) present on different copies of the alleles , strongly supports the restoration of wildtype brca sequence on the mutated allele ( table 1 )  . these collective findings suggest a reversion of the brca2 frameshift deletion mutation on the mutant allele during treatment ( fig 1 )  . 
in the lymphocytes ( germline ) , the wild - type brca2 allele and the heterozygous reference single nucleotide polymorphisms ( snps ) rs1799943 , rs1799955 , and rs1801406 were detected , along with the brca2 c.9097dup and a heterozygous snp , 2126042 . 
this method greatly simplifies the detection of such events and has important implications for the clinical care of patients with brca - mutant disease . we predict that similar phenomena may be sensitively identified earlier , before disease progression , with new platforms that incorporate next - generation sequencing to circulating tumor dnaso - called liquid biopsies . we conclude that the somatic reversion mutation was the mechanism of resistance to parp inhibitor and was responsible for progression during therapy . 
in the germline sample , the wild - type brca2 allele and the heterozygous reference single nucleotide polymorphisms ( snps ) rs1799943 , rs1799955 , and rs1801406 were detected together , along with the brca2 c.9097dup and a heterozygous snp rs2126042 . 
gadi stock and other ownership interests : sengine precision medicine research funding : genentech / roche ( inst ) affiliations all authors , university of washington ; kalyan banda and v.k. 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . j mol diagn 16 : 56 - 67 , 2014 10 . 
computed tomography ( ct ) scan with ( a ) the index lesions in the breast ( arrows ) before parp inhibitor and ( b ) 5 months later , which demonstrates decreased volume of disease . 
the absolute numbers of variant alleles and total number of alleles are in parentheses . mutations in tp53 , depdc5 , plk2 , and tacc3 are present in both preand post - treatment biopsies but are enriched in the post - treatment sample . 
identification of biomarkers predictive of a benefit from trastuzumab will minimize overtreatment and lower health care costs . methods to identify possible single - gene biomarkers , an exploratory analysis of 3 , 669 gene probes not expected to be expressed in normal breast tissue was conducted . 
 disease - free survival ( dfs ) was used as the end point in a cox regression model , with the interaction term between c8a mrna and treatment as a categorical variable split on the cohort mean . results a significant interaction between c8a mrna and treatment was detected ( p < .001 ) , indicating a predictive response to trastuzumab treatment . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction breast cancer is the leading cause of cancer death among women worldwide.1 it is a heterogeneous disease , so to maximize benefit to the patient by individualizing treatment regimens , clinicians need a sound classification syste clinicopathologic variables , including the estrogen receptor 1 , progesterone receptor , and human epidermal growth factor receptor 2 ( her2 ) , are used to classify tumors as hormone positive , her2 positive ( her2 + ) , or triple negative and to guide treatment decisions . 
pam50 , oncotype dx , and mammaprint were developed using retrospective analysis of mrna gene expression data from breast cancer cohorts . identification of single genes or gene signatures that can be used to classify a breast cancer tumor as a subtype with known treatment strategies can improve outcomes and minimize unnecessary treatment . 
the identification that 15% to 25% of breast cancer tumors overexpress the her2 protein , a transmembrane tyrosine kinase that regulates growth and cell survival , resulted in the development of monoclonal antibody therapy that targets her2 . 
 the exploratory analysis identified c8a , a member of the membrane attack complex and part of the innate immune system , which was prognostic of outcome in the observation arm and predictive of benefit from trastuzumab . 
we also characterized c8a protein expression in stable cancer cell lines . methods study population the hera trial was an international , intergroup , open - label , phase iii randomized study.5 a total of 5 , 102 women with her2 + primary breast cancer ( after a minimum of four courses of standard chemotherapy ) were enrolled and assigned randomly to one of the following three treatment arms : observation ( no trastuzumab ) and 1 or 2 years of adjuvant trastuzumab administered intravenously every 3 weeks . 
an interim analysis5 showed that patients assigned to the 1 - year trastuzumab arm experienced a significantly lower hazard of a dfs event than those in the observation arthis finding resulted in a protocol amendment that allowed for observation patients to selectively crossover to trastuzumab treatment ( 1 or 2 years ) , with the restriction of being alive and disease - free as of may 16 , 2005 . 
the transhera tissue resource consisted of 1 , 203 blocks that originated from 15 countries and were processed at royal marsden hospital in the united kingdo in addition , an extra 600 - m core was taken from each block . 
sample rna was extracted using the expressart ffpe rnaready isolation kit ( amptec , hamburg , germany ) , which is optimized for isolation of total rna specifically from ffpe tissue samples , and eluted into a volume of 20 l . 
the biotinylated cdna is then immobilized to a streptavidin - coated solid support and annealed to a dasl assay pool of gene - specific oligonucleotides for extension and ligation followed by polymerase chain reaction amplification with a biotinylated and a fluorophore - labeled universal primer . 
 control ( liver and brain ) rna samples were included for each processed batch of 48 samples to ensure that rna processing was successful and for quality control and normalization of data between assay batches . 
cubic spline has been shown to combine the positive effects of quantile normalization and to avoid the drawbacks of discontinuous mapping of intensity values and no - rank preservation.11 analysis information from the hera database , with a clinical cutoff date of april 12 , 2012 , and 8 years of median follow - up , was used in the current study.7 the primary end point was dfs , defined as the time from random assignment to first occurrence of any of the following dfs events : recurrence of breast cancer at any site ; the development of ipsilateral or contralateral breast cancer , including ductal carcinoma in situ but not lobular carcinoma in situ ; second nonbreast malignant disease other than basal - cell or squamous - cell carcinoma of the skin or carcinoma in situ of the cervix ; or death as a result of any cause without documentation of a cancer related event . exploratory analysis of possible predictive biomarkers in this exploratory analysis , 3 , 669 gene mrna probes on the illumina humanht - 12 v3 array , which are based on normal breast tissue mrna expression profiles not expected to be expressed in breast tissue , 10 were used to conduct an exploratory analysis of possible predictive biomarkers.1 each probe was used in a cox proportional hazards regression predictive model as a categorical variable bifurcated on the mean of gene mrna expression . 
the list of probes ranked by interaction p value were then used to identify c8a as a gene of interest because it is not normally expressed in breast tissue and is a member of the membrane attack complex and part of the innate immune systea volcano plot of the exploratory analysis is shown in figure 1 . 
exploratory analysis of treatment interaction p value as a categorical variable split on probe mrna expression of 3 , 669 gene probes in the herceptin adjuvant cdna - mediated annealing , selection , extension , and ligation cohort that have zero expected expression in normal breast tissue . 
in the early events analysis , only early disease - defining events were taken into account ( ie , at 2.2 years of median follow - up time ) , when almost no patient had switched from observation to trastuzumab . 
 cox models were adjusted for several clinicopathologic factors : age , pathologic tumor size , progesterone receptor local , estrogen receptor local , tumor grade , menopausal status , nodal status , prior ( neo ) adjuvant chemotherapy , eastern cooperative oncology group performance status , race , and region . 
the weights for the ipw analysis were estimated using a time - varying covariate and the following two baseline covariates : age at study entry and prior ( neo ) adjuvant chemotherapy . 
follow - up time of each eligible patient was divided into 1 - month intervals , and the time - varying covariate was estimated as the within - interval cumulative time of eligibility to cross over . prognostic her2 + gastric cancer cohort we used the publicly available data from the hungarian academy of science ( has ) gastric cancer cohort to further explore c8a as a possible biomarker in her2 + gastric cancer.12 the has gastric cancer cohort is a collection of publicly available cohorts with outcome data profiled on the affymetrix platform ( santa clara , ca )  . 
molecular signature database ( version 4.0 ) gene sets tested included immunologic signatures ( n = 1 , 910 ) , canonical pathways ( n = 1 , 320 ) , molecular gene ontology terms ( n = 1 , 454 ) , microrna ( n = 221 ) , chromosome positions ( n = 326 ) , transcription factors ( n = 615 ) , chemical genetic perturbations ( n = 3 , 402 ) , and oncogenic signatures ( n = 189 )  . c8a mrna normal and cancer tissue expression profile the gtex web portal17 was used to generate a figure for the c8a mrna expression in normal tissues . 
figures that illustrate c8a mrna expression from cancer cell lines were generated using the cancer cell line portal.18 the cancer cell line encyclopedia was used to determine the c8a mrna mean and standard deviation in 1 , 036 cancer cell lines . 
tumor cell lines , hepatocellular carcinoma ( tma809 ) , lung cancer ( dms454 ) , triple negative breast cancer ( mda - 231 ) , her2 normal breast cancer ( mda - 175 ) , and her2 + breast cancer ( sk - br - 3 ) were used for c8a ihc staining . 
 the mrna expression profile suggests that for approximately 70% of the human epidermal growth factor 2positive cohort , c8a mrna was not expressed , and 30% had high expression of c8a mrna . 
kaplan - meier curve for disease - free survival ( dfs ) in the herceptin adjuvant cdna - mediated annealing , selection , extension , and ligation cohort , where the c8a mrna split on the mean represents c8a - low and c8a - high categories . 
the c8a phenotype is illustrated in the gsea histogram shown in figure 4 , with the top 50 genes enriched in the c8a - low group versus the top 50 genes enriched in the c8ahigh group . 
c8a is part of the innate immunity and membrane attack complex and clearly differentiated the enrichment of gene sets associated with immunologic response . c8a mrna expression the c8a mrna on / off expression profile in our analysis cohort suggests that c8a may be expressed in other cancer cell lines . 
on the basis of the results presented in the data supplement , we see that c8a is highly expressed in distinct ovarian , liver , stomach , pancreatic , lung , and hematopoietic / lymphoid cancer types . 
to verify that c8a mrna results in c8a protein expression , c8a antibody was used to stain available cancer cell lines , and the results are the data supplement . discussion identification of single genes or gene signatures that can be used to classify a breast cancer tumor as a subtype with known treatment strategies can improve outcomes and minimize unnecessary treatments . 
 the immune gene list from molecular signature database ( version 4.0 ) on the right represents the top 50 enriched immune genes in c8a - low versus c8ahigh samples and the top 50 enriched immune genes in c8a - high versus c8a - low samples . 
the cancer cell line encyclopedia data show that dms454_lung , ov90_ovary , and snu719_stomach are examples that have high expression of c8a and that c8a is a feature of those immortal cancer cell lines . c8a protein is a critical component of the membrane attack complex that inserts itself into the outer membrane of target cells and anchors the recruitment of c9 proteins to form a pore that leads to cell lysis and death.20 , 21 the membrane attack complex is a component in the complement system , which is part of the innate immune system found in plant and animals and evolved before adaptive immunity.22 the innate immune system can work independently of or be triggered by the adaptive immune system and plays a role in the monitoring of host cells that are damaged or have died and should be cleared.23 the complement system proteins are synthesized by the liver and normally circulate in the blood until stimulated by complement activation . 
molecular characterization of c8a high her2 + tumors may indicate that it is a new cancer phenotype that can escape the immune response and become an important mechanism in cancer that affects survival . 
goldhirsch a , gelber rd , piccart - gebhart mj , et al : 2 years versus 1 year of adjuvant trastuzumab for her2 - positive breast cancer ( hera ) : an open - label , randomised controlled trial . 
skedgel c , rayson d , younis t : is adjuvant trastuzumab a cost - effective therapy for her - 2 / neu - positive t1bn0 breast cancer ? ann oncol 24 : 1834 - 1840 , 2013 10 . 
benita y , cao z , giallourakis c , et al : gene enrichment profiles reveal t - cell development , differentiation , and lineage - specific transcription factors including zbtb25 as a novel nf - at repressor . 
gyrffy b , lanczky a , eklund ac , et al : an online survival analysis tool to rapidly assess the effect of 22 , 277 genes on breast cancer prognosis using microarray data of 1 , 809 patients . 
gyorffy b , lnczky a , szllsi z : implementing an online tool for genome - wide validation of survival - associated biomarkers in ovarian - cancer using microarray data from 1287 patients . 
gyrffy b , benke z , lnczky a , et al : recurrenceonline : an online analysis tool to determine breast cancer recurrence and hormone receptor status using microarray data . 
said ea , dupuy fp , trautmann l , et al : programmed death - 1 - induced interleukin - 10 production by monocytes impairs cd4 + t cell activation during hiv infection . 
to our knowledge , there are no previous reports of basal cell carcinoma of the prostate occurring in association with a germline brca2 mutation , as in the patient reported here ; however , brca2 mutations , which are a recognized risk factor for prostate adenocarcinoma , are increasingly recognized as a driver for more aggressive disease5 and as a potential therapeutic target . 
olaparib , a poly ( adp ribose ) polymerase ( parp ) inhibitor , has shown high response rates in patients with prostate cancer and defects in homologous repair.6 unfortunately , many patients receiving treatment with parp inhibitors may develop reversion mutations that restore brca function and reduce sensitivity to parp inhibition or confer resistance . 
to our knowledge , there are no reports of the successful treatment of patients with metastatic prostate cancer after brca reversion mutations . in this article , we present a patient with a germline brca2 mutation who developed de novo metastatic basal cell carcinoma of the prostate and experienced a complete clinical response with olaparib . 
 after a mixed response , the patient underwent metastasectomy and subsequently had minimal to no evidence of disease while continuing to receive olaparib maintenance . in january 2016 , a 77 - year - old man with a normal psa presented with urinary obstruction . 
a computed tomography ( ct ) scan confirmed dozens of soft tissue nodules in all lobes of both lungs , suggestive of metastatic disease , as well as an enlarged prostate with a hypodense lesion in the left lobe causing mass effect on the urethra , suggestive of malignancy . 
tumor cells stained diffusely positive for bcl2 and ttf1 ; focally positive for ck903 , ck20 , p63 , and ar ; and negative for ck7 , napsin a , chromogranin , synaptophysin , psa , erg , nkx3.1 , uroplakin , gata3 , and s100 . 
overall , the immunophenotype and morphology were compatible with basal cell carcinoma of the prostate , basaloid variant ( fig 1 )  . the patients lung metastases continued to grow rapidly , he was no longer ambulatory , and he joseph e . 
bhatt author affiliations and support information ( if applicable ) appear at the end of this article . the content is solely the responsibility of the authors and does not necessarily represent the official views of harvard catalyst , harvard university , and its affiliated academic health care centers or the national institutes of health . corresponding author : joseph e . 
 ( a ) x100 , ( b ) x400 , ( c ) x200 , and ( d ) x400 ; prostate biopsies demonstrated a high - grade carcinoma with basaloid morphology : monotonous cells with high nuclear to - cytoplasmic ratio , arranged in solid nests , with peripheral palisading , frequent comedonecrosis . 
we met him for an initial visit at this time , and targeted sequencing of his tumor was performed by foundationone ( foundation medicine , cambridge , ma ) , revealing a mutation in brca2 : s1982fs * 22 , also known as 6174delt , present at 70% allele frequency . 
after 2 months of treatment , he developed progressive macrocytic anemia , which is a known adverse effect of olaparib , and his dose was reduced to 300 mg twice daily . 
three months after initiating treatment , a ct scan of the torso revealed a dramatic response , with the innumerable pulmonary nodules and masses decreased in size and quantity throughout the lungs ( fig 2c ) and shrinkage of the hypodense lesion in the prostate . eight months after beginning treatment , the patient continued receiving olaparib , which was further dose reduced to 200 mg twice daily for anemia . 
the second mutation restored the open reading frame presumably restoring brca2 function , thereby mediating resistance to olaparib . because of frequent complicated urinary tract infections , we wished to avoid cytotoxic chemotherapy , and we continued giving olaparib while adding atezolizumab and androgen deprivation therapy ( adt ) with leuprolide acetate . 
we did not treat with adt initially because of what we thought would be a low likelihood of response for this type of tumor on the basis of the limited case series available , 8 but we added it at this point because of limited low - toxicity options . 
imaging again showed a mixed response : the four new lung nodules seen on the previous scan had disappeared , other nodules were stable to smaller , but the largest right subpleural nodule and one additional nodule continued to grow and cavitate . 
 the two growing lung nodules were resected , and the patient continues to receive olaparib monotherapy , now 28 months after diagnosis , with his most recent scan showing only a single 1.4 - cm nodule that continues to shrink . discussion we present a patient who was successfully treated for a rare disease that has no standard of care . 
the patient is notable for rationally selected targeted therapy with parp inhibition in a new tumor subtype and for further success in treatment after the development of a brca2 reversion mutation that seemed to confer resistance . 
parp inhibition is showing increasing promise across tumor types that harbor defects in homologous recombination , and mechanisms and patterns of resistance are being elucidated.9 in prostate cancer , the first case series6 reporting the successful treatment of tumors harboring defects in homologous repair with olaparib showed a response in 88% of patients with dna repair defects . 
long - term data are still evolving and have not yet been reported in this setting , but a recent abstract10 suggests that , at least in combination with adt , olaparib results in a median pfs of approximately 13 months in patients with metastatic prostate cancer . 
at the time of progression , various mechanisms of resistance have been reported , including brca2 reversion mutations , as in this patient , 11 which may be polyclonal , suggesting that these reversion mutations may be relatively common under the evolutionary pressure of parp inhibition . in the patient presented here , we elected to add atezolizumab in the hope that there could be a synergistic effect with parp inhibition . 
 preclinical rationale for this approach is based on cell culture and xenograft models where parp inhibitors upregulate pd - l1 expression , thereby attenuating anticancer immunity , and pd - l1 inhibitors resensitize tumors to t - cell killing , increasing therapeutic efficacy.12 clinical trials investigating these combinations are ongoing.13 , 14 after adding atezolizumab , this patient experienced a mixed response , and with only two lung nodules remaining , we elected to proceed with a metastasectomy . 
if reversion mutations are indeed common under the evolutionary pressure of parp inhibition , we hypothesize that the patient remains disease free , at least in part , as a result of continued efficacy of immune checkpoint blockade . 
in conclusion , to our knowledge , this is the first report of the successful treatment of basal cell prostate cancer with a parp inhibitor , and more importantly , the first report of the successful treatment of a brca2 - mutated tumor after a reversion mutation . 
 bhatt collection and assembly of data : all authors data analysis and interpretation : all authors manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors relationships may not relate to the subject matter of this manuscript . 
simper nb , jones cl , maclennan gt , et al : basal cell carcinoma of the prostate is an aggressive tumor with frequent loss of pten expression and overexpression of egfr . 
chang k , dai b , kong y , et al : basal cell carcinoma of the prostate : clinicopathologic analysis of three cases and a review of the literature . 
banda k , swisher em , wu d , et al : somatic reversion of germline brca2 mutation confers resistance to poly ( adp - ribose ) polymerase inhibitor therapy . 
clarke n , wiechno pj , alekseev b , et al : olaparib combined with abiraterone in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) : a randomized phase ii trial . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
karzai f , madan ra , owens h , et al : a phase 2 study of olaparib and durvalumab in metastatic castrate - resistant prostate cancer ( mcrpc ) in an unselected population . 
friedlander m , meniawy t , markman b , et al : a phase 1b study of the anti - pd - 1 monoclonal antibody bgb - a317 ( a317 ) in combination with the parp inhibitor bgb - 290 ( 290 ) in advanced solid tumors . 
 minimally invasive real - time detection of actionable mutations in patients with metastatic solid tumors using fine - needle and liquid biopsies purpose fine - needle biopsy ( fnb ) and liquid biopsy are minimally invasive methods of tumor sampling that provide feasible means to assess tumor genotypes in real time . 
 however , more data are needed to establish the strength of these methods by benchmarking against the current gold standard methods , core - needle biopsy ( cnb ) or surgical excision of the tumor . patients and methods eligible patients with advanced solid tumors were prospectively recruited . 
we performed mutation profiling using matched tumor dna obtained by cnb , fnb and liquid biopsy , and matrix - assisted laser desorption / ionization time - offlight custom mass - spectrometry or targeted next - generation dna sequencing . 
median dna yield from cnb and fnb were 775 ng ( interquartile range , 240 to 347 4ng ) and 649 ng ( interquartile range , 180 to1350 ng ) , respectively . 
2018 by american society of clinical oncology next - generation dna sequencing ( ngs ) of archival tumors is now routinely performed to identify actionable somatic mutations to guide treatment decisions in patients with solid tumors with either standard of care therapy or genotype matched clinical trials.1 - 5 fresh tumor biospecimens that are needed to accurately assess tumor genotype in real time are usually obtained by a core - needle biopsy ( cnb ) or surgical excision of the tumor ; however , these procedures are invasive and carry inherent risks , including bleeding , infection , and injuries to nearby tissues and / or organs , and often are not suitable for serial tumor samplings . 
noninvasive methods that readily allow that sampling of tumor or tumor - derived dna are therefore needed to overcome these limitations . fine - needle biopsy ( fnb ) is a minimally invasive and safe technique for tumor sampling . 
 sample processing , sufficient tumor dna can be obtained for screening of actionable mutations using ngs , considering that the input dna requirement for targeted ngs has decreased.7 - 9 circulating tumor dna ( ctdna ) obtained by liquid biopsy can now be used for tumor mutation profiling , 10 - 12 and this approach will be useful , particularly for those who do not have tumor lesions that are easily accessible to biopsy . 
the us food and drug administration have recently approved ctdna - based companion diagnostic tests in nonsmall - cell lung cancer to detect egfr exon 19 deletions or l858 mutations and egfr p.t790m mutation to select patients for treatment with egfr tyrosine kinase inhibitors erlotinib and osimertinib , respectively.13 in the current study , we identified prospectively actionable somatic mutations in a cohort of patients with advanced solid tumors using matched cnb , fnb , and ctdna to compare the performance of these methods in a realworld clinical setting . 
the study was approved by the university health network research ethics board ( #12 - 0361 - c )  . tumor tissue and blood collection fresh tumor tissue was procured by an image ( ultrasound or computed tomography ) - guided percutaneous biopsy of a metastatic lesion . 
the most recent formalin - fixed , paraffin embedded ( ffpe ) archival tumor specimen from the date of consent , either surgical excision or cnb , was obtained . tumor sample processing , pathologic evaluation , and dna extraction archival tumor samples were processed as previously described.4 cell recovery from fnb samples was optimized using a rapid onsite evaluation algorithm by cytopathologists.14 with each pass , a small , representative portion of the sample was expressed from the needle and used to produce one to two air - dried , direct smears that were then stained using a rapid romanowsky method and examined microscopically to judge the adequacy of the sampling . 
tumor content of the sample was estimated by manual microscopic examination of the adequacy assessment slides and expressed as a percentage of tumor cells ( tumor cells / total nucleated cell content )  . 
cell - free dna that contained ctdna was isolated from plasma using the qiagen circulating nucleic acids kit ( qiagen ) according to manufacturer instructions , with the exception that carrier trna was not used . 
 germline dna was isolated from the wbc fraction using either the standard manual phenol / chloroform extraction method or automated extraction . sequencing reads were aligned to the human genome reference using the burrows - wheeler aligner.16 somatic variants were called from the resulting bam files using strelka17and annotated with annovar.18 a minimum read depth of 500 at the location of the variant was required for mutation reporting . 
only mutations with > 5% af in ctdna and < 1% af in germline dna were reported to avoid false - positive results . mutation profiling of tumor and germline tumor dna from fnb and cnb as well as germline dna were profiled using one of three platforms : matrix - assisted laser desorption / ionization time - of - flight ( maldi - tof ) custom mass spectrometry ( massarray ; agena bioscience , san diego , ca ) assay that detects 279 hotspot mutations in 23 genes ( appendix table a1 ) at a limit of detection of 5% ; and two ngs assays : the truseq amplicon cancer panel ( illumina , san diego , ca ) , which covers mutations in 48 genes ( appendix table a2 ) , on the miseq sequencer ( illumina ) ; or the ion ampliseq cancer panel ( thermo fisher scientific ) , which covers mutations in 50 genes ( appendix table a3 ) , on the ion proton sequencer ( thermo fisher scientific ) as previously described.4 somatic variants identified have to meet laboratory defined thresholds of > 500 read depth coverage and allele frequency ( af ) of > 10% ; however , these analyses were performed as research analyses in a molecular diagnostics laboratory , and mutation results were not formally reported in the patients electronic medical records . 
profiling results from fresh biopsies and plasma samples were captured and stored in a research database on the medidata rave ( new york , ny ) platform . mutation profiling of plasma - derived ctdna thunderbolts cancer panel ( raindance technologies , billerica , ma ) , which can detect mutation in 50 genes , 15 was used to profile ctdna and germline dna . 
mutations classified as levels 1 , 2a , 2b , 3a , 3b , and 4 were considered actionable . clinical data collection patient and tumor characteristics , cancer treatment ( s ) before study entry , and subsequent treatments after molecular profiling were collected . 
 adverse events related to study procedures were recorded and graded according to the common terminology criteria for adverse events version 4.0.19 patients were folllowed up to 7 days after tumor biopsy via telephone for assessment of biopsy - related adverse events ( aes )  . 
combined fnb and cnb results of each patient were considered as tumor mutation results and compared with ctdna mutation results . results patients from october 2012 to january 2015 , 45 patients were enrolled . 
 cnb , core - needle biopsy ; fnb , fine - needle biopsy . safety of fresh tumor biopsy of the 41 patients biopsied , 12 ( 29% ) experienced 14 aes . 
other biopsy - related aes were grade 1 or 2 abdominal pain ( n = 10 ) , vomiting ( n = 2 ) , bleeding ( n = 1 ) , and fever ( n = 1 )  . feasibility of mutation analysis from fnb and cnb in the 41 patients biopsied , a median of three fnbs ( range , two to five fnbs ) and four cnbs ( range , one to five cnbs ) were obtained . 
of the remaining patients , five did not have tumor in cnb and one did not have tumor in fnb , which yielded 30 cnbs and 34 fnbs with sufficient tumor and dna for mutation profiling ( table 2 )  . 
whereas the dna yield from cnbs was generally higher than that from fnbs , all 34 fnbs yielded enough dna for mutation profiling . comparison of cnb and fnb mutation results of the 30 cnbs analyzed , 27 were profiled by miseq and three by maldi - tof custom mass spectrometry . 
in the remaining 22 patients , eight ( 20% of 41 total evaluable patients for mutation results ) had nine actionable mutations ( table 2 and fig 2 )  . 
blue , mutation detected ; red , mutation not detected ; gold , sample not available . actionable mutation plasma directly comparablesame patients , same biopsy site , and same profiling platformmutation calls were identical in 23 of 25 pairs , which resulted in 92% agreement ( table 3 )  . comparison of mutations detected in archival and fresh tumors there were 32 archival and fresh tumoreither cnb or fnbpairs ; however , results were only directly comparable in 23 pairs because the use of sequencing platform was not uniform in all cases . 
more mutations were detected in plasma compared with tumors , and mutation results were concordant in six ( 19% ) of 32 pairs ( summarized in table 4 )  . 
in both cases , tumor sequencing was performed using the truseq panel , and reviewing the tumor sequencing data revealed that position cdkn2a p.p114s was not covered but that pten p.s10n position was covered with > 3 , 000 coverage . 
in contrast , three actionable pik3ca mutations that were found in the cnb / fnb pairs were not detectable in plasma ( fig 2 ) ; afs of two pik3ca mutations were high in tumors ( 78% and 49% ) but low in the remaining one ( 9% )  . 
as the cutoff for mutation calling in plasma in this study was conservative , we reviewed the plasma sequencing data in three cases in which pik3ca mutation results were discordant and found that all three pik3ca mutations could be found in corresponding plasma with low afs ( pik3ca p.h1047r : af 2% ; pik3ca p.n345k : af 1% ; and pik3ca p.e545k : af 1% )  . 
none of these three mutations was found in germline sequencing . discussion the feasibility of targeted ngs of cytology samples to identify actionable mutations has been demonstrated in multiple solid tumor types20 - 26 ; however , results from several real - world studies have demonstrated that 30% to 50% of fnb samples were not suitable for ngs analysis because of low tumor cell content.21 , 23 , 27 , 28 a large retrospective study reported a success rate of 54% , which , albeit low , was comparable to results that were achieved with cnb at the same institution.28 in contrast , a high success rate ( > 90% ) can be achieved by using rapid onsite evaluation algorithm combined with optimized sample processing.22 our results support the growing body of evidence that suggests that optimally processed fnbs can be successfully used for mutation profiling with ngs , yielding results that are comparable to those of cnb . 
comparison of tumor and plasma mutations detected ( n = 32 ) ( continued ) tumor type tumor sequencing platform tumor mutations detected , shown with allele frequency ( % ) plasma mutations detected using thunderbolts cancer panel , shown with allele frequency ( % ) concordant patient mat - 034 melanoma miseq atm p.e2744k ( 33 ) , idh1 p.r132c ( 28 ) , nras p.q61h ( 26 ) idh1 p.r132c ( 19 ) , nras p.q61h ( 19 ) , tp53 p.r116w ( 19 ) mat - 035 melanoma mat - 036 ovarian mat - 037 breast miseq miseq miseq kit p.e861k ( 30 ) tp53 p.p151h ( 22 ) none detected none detected none detected atm p.t1819a ( 27 ) , csf1r p.s946n ( 7 ) , erbb2 p.n850s ( 8 ) , erbb4 p.c234y ( 5 ) , pdgfra p.p567l ( 4 ) , smad4 p.q183r ( 7 ) mat - 038 breast miseq pik3ca p.h1047r ( 14 ) , pik3ca p.h1048r ( 14 ) pik3ca p.h1047r ( 39 ) , pik3ca p.h1048r ( 39 ) mat - 039 melanoma miseq braf p.v600k ( 77 ) , idh1 p.r132c ( 32 ) akt p.i19n ( 8 ) , braf p.v600k ( 19 ) , erbb2 p.i767t ( 9 ) , met p.y1253h ( 11 ) , mat - 040 breast miseq egfr p.v292m ( 16 ) pik3ca p.n345k ( 49 ) , tp53 p.e2q ( 45 ) mat - 041 mat - 042 mat - 044 mat - 045 breast ovary breast breast miseq miseq miseq miseq tp53 p.n210fs ( 18 ) none detected pik3ca p.e545k ( 9 ) tp53 p.v272m ( 70 ) none detected none detected none detected none detected note . 
the time interval between the collection of the archival tumor and fresh tumor biopsies was approximately 5 years , and , during that interval , the patient received an aromatase inhibitor for approximately 3 years in the adjuvant setting and capecitabine chemotherapy for 18 months in the first - line metastatic setting . 
one possible explanation is that the pik3ca p.h1047r mutation , in this case , is clonal and the atm p.e1971d subclonal and atm mutant subclone arose during metastasis and / or treatment resistance . we have also demonstrated that actionable mutations can be detected from plasma - derived ctdna using raindance thunderbolts gene panel and ngs . 
using a cutoff af of 5% , three actionable pik3ca mutations that were detectable in the tumors of three patients with breast cancer were not detectable in plasma ; however , all three pik3ca mutations were indeed present in plasma at low af ( 1% to 2% )  . 
considering that afs of tumor - derived mutations in plasma in patients with solid tumors can be low and one requires an assay with a limit of detection of 0.1% or less to pick up the majority of ctdna mutations , our criteria for mutation calling in plasma were too conservative and limited the sensitivity of our assay . 
our results reinforce the fact that ctdna mutation assays with low limits of detection can indeed miss actionable mutations , and , when ctdna results are negative , every effort should be made to profile tumors . 
in one case with the cdkn2a p.p114s mutation in plasma , tumor sequencing did not cover the mutation position , and this is likely to be the reason for the discordance between tumor and plasma results . 
taken together , our results demonstrate that mutation profiling of ctdna can be used as a primary tool to detect actionable mutations and can also be used to monitor tumor genetic evolution overtime . 
of importance , results from recent studies that assessed the efficacy of pan phosphatidylinositol 3 - kinase ( pi3k ) inhibitors in hormone receptorpositive advanced breast cancers demonstrated that patients derived benefit from pan - pi3k inhibitors regardless of tumor pik3ca mutation status , 29 , 30 but that patients with pik3ca mutation in ctdna derived better clinical benefit in terms of tumor response and progression - free survival.30 these findings support tumor agnostic mutation testing from ctdna in the right clinical context . 
 use of multiple platforms has inherent bias in the ability to detect alterations in different genomic regions , an important caveat in comparing mutation results between fnb and cnb as well as between plasma and tumor . 
 we have to acknowledge that tumor structural tumor microenvironment , architecture and including immune infiltrates , cannot be assessed using fnb , an important limitation . our results indicate that , with proper specimen handling , processing , and assessment , cytology samples , such as the direct smear and / or cell block , and liquid biopsies are suitable for molecular profiling using ngs . 
bedard research funding : bristol - myers squibb ( inst ) , sanofi ( inst ) , astrazeneca ( inst ) , genentech ( inst ) , servier ( inst ) , glaxosmithkline ( inst ) , novartis ( inst ) , signalchem ( inst ) , ptc therapeutics ( inst ) , cascadian therapeutics ( inst ) , nektar ( inst ) , merck ( inst ) eitan amir honoraria : apobiologix john d . 
stockley honoraria : astrazeneca , bristol - myers squibb consulting or advisory role : astrazeneca , janssen pharmaceuticals , novartis , bristol - myers squibb research funding : astrazeneca suzanne kamel - reid consulting or advisory role : novartis , astrazeneca consulting or advisory role : merck , astrazeneca , medimmune , morphosys , symphony evolution research funding : bristol - myers squibb ( inst ) , genentech ( inst ) , glaxosmithkline ( inst ) , merck ( inst ) , novartis ( inst ) , pfizer ( inst ) , medimmune ( inst ) , astrazeneca ( inst ) , boehringer ingelheim ( inst ) , bayer ( inst ) , amgen ( inst ) , symphony evolution ( inst ) , astellas pharma ( inst ) aaron r . 
hansen honoraria : merck , astrazeneca , medimmune , pfizer , glaxosmithkline , novartis , merck serono , boehringer ingelheim , bristol - myers squibb research funding : karyopharm therapeutics ( inst ) , merck ( inst ) , bristol - myers squibb ( inst ) , boehringer ingelheim , glaxosmithkline ( inst ) , novartis ( inst ) acknowledgment we thank william geddie , md , retired staff pathologist of laboratory medicine program , university health network ( toronto , on , canada ) , for his contributions to the study . research funding : astrazeneca ( inst ) , immunovaccine ( inst ) travel , accommodations , expenses : astrazeneca affiliations kyaw l . 
hyman dm , solit db , arcila me , et al : precision medicine at memorial sloan kettering cancer center : clinical next - generation sequencing enabling next - generation targeted therapy trials . 
stockley tl , oza am , berman hk , et al : molecular profiling of advanced solid tumors and patient outcomes with genotype - matched clinical trials : the princess margaret impact / compact trial . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
roy - chowdhuri s , chen h , singh rr , et al : concurrent fine needle aspirations and core needle biopsies : a comparative study of substrates for next - generation sequencing in solid organ malignancies . 
kanagal - shamanna r , portier bp , singh rr , et al : next - generation sequencing - based multigene mutation profiling of solid tumors using fine needle aspiration samples : promises and challenges for routine clinical diagnostics . 
li h , durbin r : fast and accurate short read alignment with burrows - wheeler transfor cancer - panel / bioinformatics 25 : 1754 - 1760 , 2009 17 . 
dibardino dm , rawson dw , saqi a , et al : next - generation sequencing of non - small cell lung cancer using a customized , targeted sequencing panel : emphasis on small biopsy and cytology . 
gleeson fc , kipp br , voss js , et al : endoscopic ultrasound fine - needle aspiration cytology mutation profiling using targeted next - generation sequencing : personalized care for rectal cancer . 
padmanabhan v , steinmetz hb , rizzo ej , et al : improving adequacy of small biopsy and fineneedle aspiration specimens for molecular testing by next - generation sequencing in patients with lung cancer : a quality improvement study at dartmouth - hitchcock medical center . 
sakai k , takeda h , nishijima n , et al : targeted dna and rna sequencing of fine - needle biopsy ffpe specimens in patients with unresectable hepatocellular carcinoma treated with sorafenib . 
zheng g , tsai h , tseng lh , et al : test feasibility of next - generation sequencing assays in clinical mutation detection of small biopsy and fine needle aspiration specimens . 
gleeson fc , kerr se , kipp br , et al : targeted next generation sequencing of endoscopic ultrasound acquired cytology from ampullary and pancreatic adenocarcinoma has the potential to aid patient stratification for optimal therapy selection . 
krop ie , mayer ia , ganju v , et al : pictilisib for oestrogen receptor - positive , aromatase inhibitorresistant , advanced or metastatic breast cancer ( fergi ) : a randomised , double - blind , placebocontrolled , phase 2 trial . 
baselga j , im sa , iwata h , et al : buparlisib plus fulvestrant versus placebo plus fulvestrant in postmenopausal , hormone receptor - positive , her2 - negative , advanced breast cancer ( belle - 2 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
forty - eight genes included in the truseq amplicon cancer panel ( illumina ) , which includes 212 amplicons covering a total genomic region of 35.84 abl1 csf1r erbb4 fgfr3 gnaq jak2 kras akt1 braf cdh1 cdkn2a ctnnb1 egfr fbxw7 fgfr1 flt3 gna11 hnf1a hras jak3 mlh1 nras erbb2 fgfr2 gnas idh1 notch1 npm1 pdgfra pik3ca pten ptpn11 smad4 smarcb1 stk11 tp53 table a3 . 
responses to avelumab were observed regardless of pd - l1 expression , the presence or absence of tumor - inltrating therapy , and lymphocytes , multiple prior lines of somatic or germline origin of mmrd , which suggests that baseline clinical and pathologic characteristics could not predict response . 
ten of the 12 tumors were determined to be mmrd by oncopanel on the basis of mutational signature analysis using two independent algorithms , 4 , 5 which was consistent with the ihc determination . 
the remaining 2 tumors were determined to be mmrp by oncopanel and microsatellite stable using polymerase chain reactionthat is , both oncopanel and polymerase chain reaction were discordant with ihcand none of them responded to avelumab . 
 ( b ) frequency of common jak1 and b2m mutations found in our data set are compared with the frequency in the mismatch repairdecient ( mmrd ) endometrial cancers ( ecs ) from the cancer genome atlas ( tcga )  . 
fs , frameshift ; fsdel , frameshift deletion ; fsins , frameshift insertion ; nr , nonresponder ; or , objective response ; r , responder ; recur , recurrent . 
therefore , these 2 tumors were more likely to be mmrp and were excluded from the analysis . of the remaining 10 patients ( table 1 ) with tumors determined to be mmrd using both ihc and oncopanel , 3 exhibited an objective response to avelumab ( responders ) , whereas 7 did not ( nonresponders )  . 
all 7 nonresponders harbored either jak1 ( 6 tumors ) or b2m mutations ( 1 tumor ) , while only 1 of the 3 responders harbored a jak1 mutation ( fisher exact test , two - sided p = .067 ; fig 1a )  . 
in addition , of the 7 nonresponders , 4 harbored two mutations of jak1 ( 3 tumors ) or b2m ( 1 tumor ) , possibly reecting biallelic inactivation of these genes . 
all jak1 mutations were frameshift ( deletions or insertions ) , with the exception of two missense mutations that occurred together with frameshift mutations : a missense mutation q750r on the pseudokinase domain ( exon 16 ) and a missense mutation l1071p toward the end of the kinase domain ( exon 23 )  . 
frameshift jak1 mutations involved the hotspot position k860 / p861 ( deletions in 5 tumors and insertion in 1 tumor ) and the hotspot position p430 / l431 ( insertions in 2 tumors )  . 
 ( a ) number of indels , deletions , insertions , and tumor mutational burden , dened as the number of nonsynonymous mutations per mb for responders ( r ) and nonresponders ( nr ) in our data set . 
 ( b ) same as panel a comparing patients with endometrial cancer ( ec ) in the cancer genome atlas ( tcga ) data set with and without frameshift jak1 mutations . 
furthermore , in another data set ( msk - imp ) , which included 29 patients with recurrent mmrd ecs ( dened by ihc ) , 6 the overall frameshift jak1 mutations was 51.7% cidence of signicantly higher than that in the tcga data set , but comparable with that in our data set ( fig 1c )  . 
nonresponders had a signicantly higher number of total deletion mutations compared with responders ( p = .03 ) , but the number of total insertion mutations was not different ( fig 2a )  . 
 ( a ) exposure ( left ) and fraction ( right ) , dened as the exposure divided by the total number of single - nucleotide variants of signatures 20 . 
bottom : blue and red boxes and points indicate cases with and without frameshift ( fs ) jak1 mutations in whole - exome sequencing data from the cancer genome atlas ( tcga )  . 
to calculate the fraction , the exposure of each mmrd signature is divided by the sum of exposures of all mmrd signatures ( the contribution of the non - mmrd signatures is not shown as they did not vary signicantly across data sets )  . 
konstantinopoulos , md , phd , dana - farber cancer institute , 450 brookline ave , boston , ma 02115 ; e - mail : panagiotis_ konstantinopoulos@dfci.harvard.edu. support supported by the ludwig center at harvard and by a fund in memory of bina sareen . 
gulhan patents , royalties , other intellectual property : a provisional patent application is being drafted for an algorithm developed by the author for which a coversheet provisional has been led on september 24 , 2018 , titled computational method to identify mutational signatures from sequencing data ( inst ) joyce f . 
liu consulting or advisory role : tesaro , mersana , clovis oncology , genentech , glaxosmithkline research funding : genentech ( inst ) , astrazeneca ( inst ) , boston biomedical ( inst ) , atara biotherapeutics ( inst ) , acetylon ( inst ) , bristolmyers squibb ( inst ) , agenus ( inst ) , cytomx therapeutics ( inst ) , regeneron ( inst ) , tesaro ( inst ) , clovis oncology ( inst ) , surface oncology ( inst ) , 2x oncology ( inst ) , vigeo therapeutics ( inst ) , aravive ( inst ) , arch oncology ( inst ) travel , accommodations , expenses : astrazeneca , merck uncompensated relationships : merck , astrazeneca ursula a . 
konstantinopoulos consulting or advisory role : merck , vertex , astrazeneca , pzer , emd serono , tesaro , bayer research funding : pzer ( inst ) , eli lilly ( inst ) , tesaro ( inst ) , merck serono ( inst ) , astrazeneca ( inst ) , merck ( inst ) , bayer ( inst ) no other potential conicts of interest were reported . references aghajanian c , sill mw , darcy km , et al : phase ii trial of bevacizumab in recurrent or persistent endometrial cancer : a gynecologic oncology group study . 
j clin oncol 29 : 2259 - 2265 , 2011 alvarez ea , brady we , walker jl , et al : phase ii trial of combination bevacizumab and temsirolimus in the treatment of recurrent or persistent endometrial carcinoma : a gynecologic oncology group study . 
gynecol oncol 129 : 22 - 27 , 2013 konstantinopoulos pa , luo w , liu jf , et al : phase ii study of avelumab in patients with mismatch repair decient and mismatch repair procient recurrent / persistent endometrial cancer . 
j mol diagn 19 : 84 - 91 , 2017 gulhan dc , lee jj , melloni gem , et al : detecting the mutational signature of homologous recombination deciency in clinical samples . 
nat genet 51 : 912 - 919 , 2019 soumerai te , donoghue mta , bandlamudi c , et al : clinical utility of prospective molecular characterization in advanced endometrial cancer . 
clin cancer res 24 : 5939 - 5947 , 2018 alexandrov lb , nik - zainal s , wedge dc , et al : signatures of mutational processes in human cancer . 
gao j , shi lz , zhao h , et al : loss of ifn - gamma pathway genes in tumor cells as a mechanism of resistance to anti - ctla - 4 therapy . 
albacker la , wu j , smith p , et al : loss of function jak1 mutations occur at high frequency in cancers with microsatellite instability and are suggestive of 15 . 
howitt be , shukla sa , sholl lm , et al : association of polymerase e - mutated and microsatellite - instable endometrial cancers with neoantigen load , number of tumor - inltrating lymphocytes , and expression of pd - 1 and pd - l1 . 
aldubayan , md1 , 2 , 3 systematic tumor molecular proling of patients with cancer , using next - generation sequencing , has become an integrated part of current clinical oncology care , providing diagnostic , prognostic , therapeutic , and predictive utility and informing highly personalized molecular - based treatment decisions.1 - 3 until recently , most prospective tumor - proling programs of patients with cancer had primarily focused on exploring clinically actionable somatic alterations ( using tumor - only or paired tumor - normal sequencing ) and only used the concurrently generated or inferred germline data to achieve better variant ltration.3 , 4 however , during the past few years , there has been a growing interest in exploring the clinical utility of germline genetic variants in these clinical contexts to achieve a more comprehensive characterization of the genomic events driving tumor initiation , progression , and resistance . using whole - exome sequencing or selected gene panels , large tumor - normal sequencing efforts provided valuable insight into the prevalence of disruptive germline genomic alterations in various clinical settings . 
depending on the cancer type , the sequencing platform , and the variant calling pipeline , prior studies have shown a germline pathogenic variant prevalence between 3% in patients with primary cancer from earlier studies and up to 18% in selected high - risk advanced and metastatic cancer cohorts.5 - 7 building on these studies , and as reported in the article accompanying this editorial , dumbrava et al8 implemented a 201 - gene panel to capture the somatic and germline coding variants of 1 , 000 patients ( who had locally advanced or metastatic solid tumors and exhausted standard treatment options ) and subsequently deployed a tier - wise analysis approach to explore oncology - related clinically actionable germline alterations . 
for example , men with prostate cancer who carry pathogenic germline variants in brca2 and chek2 are , respectively , 27 times and ve times more likely to experience failure of initial hormonal therapy and progression to advanced metastatic disease.13 similarly , patients with colorectal cancer who have pathogenic germline alterations in atm tend to be more likely to have an advanced ( american joint committee on cancer stage 3 or stage 4 ) atm - decient tumors compared with patients with colorectal cancer carrying germline wild - type atm alleles.14 the predictive utility of such germline biomarkers can be clinically informative when weighing various treatment options where , selected clinical settings , a more interventional and aggressive treatment plan could be more appropriate than watchful waiting or active surveillance . systematic germline genomic analysis of patients with cancer can also pinpoint patients with certain inherited genomic defects whose tumors tend to be exquisitely sensitive to specic targeted treatment interventions , thus providing a therapeutic silver lining for these highly burdened patients . 
 editorial gene family , may also confer similar tumor sensitivity to poly ( adp - ribose ) polymerase inhibitors , potentially expanding the therapeutic utility of germline genomic characterization in patients with cancer.20 , 21 similarly , germline defects in the lynch syndrome genes ( mlh1 , msh2 , msh6 , and pms2 ) predispose to a whole array of dna mismatch repairdecient tumors that are selectively sensitive to immune checkpoint blockades ( such as monoclonal antibodies against programmed cell death protein 1 [ anti - pd - 1 ] and programmed death - ligand 1 [ anti - pd - l1 ] ) regardless of the cancers tissue of origin , underscoring the advantages of performing paired tumor - normal proling that simultaneously explores germline mismatch repair defects in conjunction with somatic hypermutation and microsatellite instability.22 identication of germline cancer - risk variants through tumor - focused molecular characterization also represents a unique opportunity to capture patients with inherited cancer predisposition syndromes , which has important ramications . 
first , almost all germline cancer predisposition syndromes confer susceptibility to multiple cancer types , some of which have gene - specic cancer surveillance recommendations aiming to improve survival through early detection and treatment of synchronous and metachronous primary tumors.23 , 24 so far , the national comprehensive cancer network has endorsed molecularspecic cancer screening and / or cancer risk reduction recommendations for patients with germline pathogenic variants in one or more of 31 different cancer predisposition genes.11 , 12 in addition , establishing the molecular diagnosis of a cancer predisposition syndrome in an individual triggers cascade testing of immediate family members whose risk of sharing the same pathogenic alteration could be as high as 50% and in whom implementing gene - specic cancer - preventive recommendations can be lifesaving . despite the clear clinical actionability of most germline cancer predisposition alterations , many patients discovered ( through tumor - focused molecular proling ) to carry such alterations do not receive formal clinical genetics evaluation to conrm the presence of germline mutation , establish the diagnosis , or receive appropriate counseling for cancer - risk management . 
as highlighted by another study accompanying this editorial , fishler et al25 retrospectively evaluated how their multidisciplinary genomic tumor board handled putative germline variants discovered from tumor - only sequencing of 34 women with advanced breast cancer . despite meeting the national comprehensive cancer network criteria for germline testing and having strong clinical and molecular features suggestive of an underlying germline cancer predisposition syndrome , approximately 40% of these patients , including some patients with suspected pathogenic germline alterations in pten and cdh1 ( where the overall lifetime cancer risk exceeds 80% ) , were not offered conrmatory germline testing or referred to clinical genetics , underscoring the importance of implementing a clear and easy - to - follow protocol to ensure full use of such results . 
ideally , all patients who are found to carry germline cancer - risk variants should be evaluated in the medical genetics or genetic counseling clinic , regardless of the clinical context . 
however , this approach may not be feasible in all clinical oncology settings , given the already overburdened genetic counseling system and the severe national and international shortage of clinical cancer geneticists and genetic counselors . 
to achieve this , however , educational programs in germline cancer genetics should be implemented through easily accessible didactic sessions ( during clinical oncology training ) , departmental seminars , hands - on workshops , online training modules , and conferencebased educational sessions . germline data generated as part of the tumor - focused genomic proling efforts provided a much - needed understanding of the diagnostic role and clinical utility of germline variant analysis in precision oncology . 
in addition , such programs provided large collections of thoroughly annotated clinical samples , which have been instrumental for exploring novel germline determinants of cancer risk , response to treatment , and disease progression.13 , 26 , 27 however , such programs face major technical , logistic , and clinical challenges that need to be addressed in a thorough and timely manner . 
technically , germline variant calling , using the matched normal sample , requires a distinct set of bioinformatics expertise and tools to minimize false - positive and false - negative results.28 furthermore , germline variant analysis should take into consideration the ancestral background of the examined patients , especially when conducting enrichment analysis to identify clinically informative molecular predictors . logistically , these programs should be multidisciplinary in nature , with a clear protocol for subsequent conrmatory germline testing and formal clinical genetics evaluation for all carriers of pathogenic germline variants . 
also , adequate pretest counseling for the possibility of identifying a germline alteration ( and its potential implications ) is critical to minimize post - test emotional stress.29 clinically , there is a substantial degree of uncertainty involving the clinical implications of some germline results . 
as reported by dumbrava et al8 and several other studies , almost all enrolled patients had germline variants of unknown clinical signicance , underscoring the importance of input from germline experts when evaluating such results . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . no potential conicts of interest were reported . references le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular proling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
j natl cancer inst 107 : djv193 , 2015 sholl lm , do k , shivdasani p , et al : institutional implementation of clinical tumor proling on an unselected cancer population . 
jci insight 1 : e87062 , 2016 zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
nat med 23 : 703 - 713 , 2017 [ erratum : nat med 23 : 1004 , 2017 ] jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
sci transl med 7 : 283ra53 , 2015 schrader ka , cheng dt , joseph v , et al : germline variants in targeted tumor sequencing using matched normal dna . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
jama 318 : 825 - 835 , 2017 dumbrava ei , brusco l , daniels ms , et al : expanded analysis of secondary germline ndings from matched tumor / normal sequencing identies additional clinically signicant mutations . 
mccabe n , turner nc , lord cj , et al : deciency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
rebbeck tr , friebel t , lynch ht , et al : bilateral prophylactic mastectomy reduces breast cancer risk in brca1 and brca2 mutation carriers : the prose study group . 
fishler kp , breese eh , walters - sen l , et al : experiences of a multidisciplinary genomic tumor board interpreting risk for underlying germline variants in tumoronly sequencing results . 
aldubayan sh , pyle lc , gamulin m , et al : association of inherited pathogenic variants in checkpoint kinase 2 ( chek2 ) with susceptibility to testicular germ cell 27 . 
van der auwera ga , carneiro mo , hartl c , et al : from fastq data to high condence variant calls : the genome analysis toolkit best practices pipeline . 
next - generation sequencing ( ngs ) of the primary tumor site using the oncomine comprehensive assay ( oca ; thermofisher scientic , west sacramento , ca ) detected the following genomic events : loss of function in tp53 ( c.1024c.t ) and pcm1 - alk fusion . 
the bioinformatician on the board conrmed the presence of soft - clipped reads at the ends of exon 20 in alk , and the clipped sequence was consistent with exon 23 in pcm - 1 ( fig 1 )  . 
the mtb members next searched 2 large databases , cosmic ( catalogue of somatic mutations in cancer ) and msk - impact ( memorial sloan ketteringintegrated mutation proling of actionable cancer targets ) to determine whether the pcm1 - alk fusion had ever been previously observed , but it had not . the mtb discussed the possibility that the alk fusion was a false - positive detection . 
in the past , ampliconincluding oca , were based ngs assays of dna , considered to be unable to detect unknown fusion variants , and therefore a capture - based dna or rna approach is preferred for ngs testing of alk fusions . however , the limitations of the amplicon - based assay have since been circumvented . 
in the rst step , during the analysis of the sequenced reads , all reads that are initially unaligned to the reference sequence are split in half and allowed to realign . 
another method to detect fusions involving unknown partners is to assess the 3 ( cid : 1 ) / 5 ( cid : 1 ) imbalance value.1 this step analyzes the expression levels of the 3 ( cid : 1 ) and 5 ( cid : 1 ) ends of each driver gene . 
for genes involved in a fusion event , the 3 ( cid : 1 ) end of the gene is now under different regulatory control and shows overexpression relative to the 5 ( cid : 1 ) end of the gene . 
in contrast , chimeric pcm1 - alk fusion transcripts were conrmed by direct sanger sequencing of the product , which was formed through a reciprocal translocation that joined the 5 ( cid : 1 ) end of pcm1 with the 3 ( cid : 1 ) exons of alk ( figs 3b and 3c )  . 
as with echinoderm microtubule - associated protein - like 4 ( eml4 ) - alk fusion found in lung cancer , pcm1 has multiple coiled - coil domains that are hypothesized to promote receptor activation by dimerization . 
integrative genomics viewer screenshot showing the breakpoint of the pcm1 - alk rearrangement detected by the oncomine comprehensive assay v3 . fresh - frozen tissues because treatment of samples with formalin and parafn , along with sample storage and extraction procedures , can result in signicant fragmentation , denaturation , and chemical modications of nucleic acids.3 although oca does not have a distinguishing nucleic acid sequence barcode incorporated into each amplicon , the number of barcodes detected in chimeric reads may pcm1 forward primer halted extension following pcr cycle this product function as a primer extension occurs pcm1 formation of chimera reads pcm1 fig 2 . 
 ( c ) schematic of the translocation event that creates the fusion gene pcm1 - alk ( upper ) and the functional domain structures of the pcm1 - alk protein ( bottom )  . the blue regions signify coiled - coil domains of pcm1 , and the red region indicates the tyrosine kinase domain of alk . 
 hosono et al recommended that alk status should be assessed by using two techniques and a third one in discordant cases for maximal sensitivity and specicity.10 however , discordance of results still continues to be a challenge . 
the fact that positive results for fish , ngs , and direct sequencing of alk mrna were accompanied by negative ihc results suggests the presence of posttranscriptional dysfunction or post - translational events affecting pcm1 - alk , but the precise mechanism is still unknown . in conclusion , whereas fish and direct sequencing conrmed the presence of pcm1 - alk fusion that was newly identied by a cancer genomic proling assay , the role of this fusion in tumor growth is still unclear because of the absence of protein expression . 
in addition , on the basis of a series of reports suggesting that activating fusions are responsible for acquired resistance to anti - egfr therapy , 13 - 15 the mtb also recommended repeating the genome proling test after the patient became resistant to standard chemotherapy . 
despite this , the patient could present as a suitable candidate for alk tyrosine kinase inhibitor therapy if a japanese compassionate use program were to be established in the future . 
notably , our institute has a system to treat patients with off - label drugs at the expense of the institute after receiving approval from the institutional review board when a tumor is positive for biomarkers that can predict its response to therapies approved by the japanese government for different types of tumor . 
 evaluation of alk fusion in colon cancer references lira me , choi yl , lim sm , et al : a single - tube multiplexed assay for detecting alk , ros1 , and ret fusions in lung cancer . 
haile s , corbett rd , bilobram s , et al : sources of erroneous sequences and artifact chimeric reads in next generation sequencing of genomic dna from formalin - xed parafn - embedded samples . 
nat med 20 : 1479 - 1484 , 2014 yakirevich e , resnick mb , mangray s , et al : oncogenic alk fusion in rare and aggressive subtype of colorectal adenocarcinoma as a potential therapeutic target . 
clin cancer res 22 : 3831 - 3840 , 2016 lindeman ni , cagle pt , aisner dl , et al : updated molecular testing guideline for the selection of lung cancer patients for treatment with targeted tyrosine kinase inhibitors : guideline from the college of american pathologists , the international association for the study of lung cancer , and the association for molecular pathology . 
j thorac oncol 10 : 1648 - 1652 , 2015 rogers tm , arnau gm , ryland gl , et al : multiplexed transcriptome analysis to detect alk , ros1 and ret rearrangements in lung cancer . 
sci rep 7 : 42259 , 2017 kalemkerian gp , narula n , kennedy eb , et al : molecular testing guideline for the selection of patients with lung cancer for treatment with targeted tyrosine kinase inhibitors : american society of clinical oncology endorsement of the college of american pathologists / international association for the study of lung cancer / association for molecular pathology clinical practice guideline update . 
letovanec i , finn s , zygoura p , et al : evaluation of ngs and rt - pcr methods for alk rearrangement in european nsclc patients : results from the european thoracic oncology platform lungscape project . 
marchetti a , di lorito a , pace mv , et al : alk protein analysis by ihc staining after recent regulatory changes : a comparison of two widely used approaches , revision of the literature , and a new testing algorithj thorac oncol 11 : 487 - 495 , 2016 13 . 
piotrowska z , isozaki h , lennerz jk , et al : landscape of acquired resistance to osimertinib in egfr - mutant nsclc and clinical validation of combined egfr and ret inhibition with osimertinib and blu - 667 for acquired ret fusion . 
liang w , he q , chen y , et al : metastatic eml4 - alk fusion detected by circulating dna genotyping in an egfr - mutated nsclc patient and successful management by adding alk inhibitors : a case report . 
daly c , castanaro c , zhang w , et al : fgfr3 - tacc3 fusion proteins act as naturally occurring drivers of tumor resistance by functionally substituting for egfr / erk signaling . 
clinical validation of ctdna using amplicon - based ngs analysis ( with a 36 - gene panel ) was performed against standard - of - care tissue molecular analysis in treatment - nave patients . the feasibility , utility , and prognostic value of ctdna as a dynamic marker of treatment efcacy was evaluated . results of tissue molecular prole were blinded during ctdna analysis . results of 214 patients with advanced nsclc who were recruited , 156 were treatment - nave patients and 58 were pretreated patients with unknown tissue molecular prole . 
for clinically relevant variants , concordance agreement between ctdna and tumor tissue analysis was 95% among 94 treatment - nave patients who had concurrent liquid and tumor biopsy molecular proles . sensitivity and specicity were 81% and 97% , respectively . 
 remon et al context key objective relevance to assess the feasibility and utility of circulating tumor dna ( ctdna ) by amplicon - based next - generation sequencing ( ngs ) analysis in a daily clinical setting in a cohort of patients with advanced nonsmall - cell lung cancer ( nsclc ) as an alternative approach to tissue molecular proling . knowledge generated these real - world data from a prospective study endorse ctdna molecular prole by amplicon - based ngs as an accurate and reliable tool to detect and monitor clinically relevant molecular alterations in patients with advanced nsclc . 
also , they endorse the theory that liquid biopsy may predict earlier than standard radiologic criteria the effectiveness of platinum - based chemotherapy . this large , real - world , prospective study in patients with advanced nsclc provides additional validation about ctdna for molecular proling and monitoring of alterations with high sensitivity and specicity to detect clinically relevant and actionable mutations when tissue biopsy is unavailable or uninformative . 
patients with advanced nsclc were eligible for the study if they were treatment nave for advanced disease and expected to receive rst - line platinum - based chemotherapy ( treatment - nave cohort ) or if the tissue - based molecular prole failed or was not performed on the primary tissue sample ( treated rescue cohort ; appendix fig a1 )  . 
all patients provided written informed consent for biomedical research approved by the institutional ethics committee under one of the two studies ( clinicaltrials . gov identier : nct02105168 ; or clinicaltrials.gov identier : nct02666612 ) to perform molecular analysis in tissue and plasma collections . 
in a subset of treatment - nave patients ( with or without tissue molecular proles ) who received standard platinum - based chemotherapy , additional blood specimens were collected at baseline and within 6 weeks of treatment initiation to match to the radiologic evaluation of the disease for clearance of baseline genomic alterations or emergence of new mutations after treatment . the study aimed to correlate detection of molecular abnormalities in tissue versus blood in treatment - nave patients , to evaluate the prognostic value of ctdna as a dynamic biomarker of treatment efcacy , and to assess the feasibility and utility of liquid biopsy in patients for whom tissue analysis failed . blood samples and ctdna isolation and sequencing blood for plasma preparation was collected into a single 10 - ml k2 edta tube before the start of platinum - based chemotherapy treatment or at the time of study enrollment for patients enrolled in the rescue cohort . in this study , plasma analysis was performed using invisionseq lung with an earlier 35 - gene panel8 ( n = 164 ) and a revised 36 - gene panel9 ( n = 50 , treatment - nave only ; appendix fig a2 )  . 
in this study , before analysis , we dened a core gene variant panel for clinically relevant gene mutation hotspots as follows : egfr exons 18 to 21 , braf v600 , met exon 14 , erbb2 ins 20 , and kras ; panel selections were based on recent recommendations of asco and international association for the study of lung cancer biomarker guidelines for ngs panels used in molecular proling.5 , 13 on the basis of emerging clinical interest , stk1114 also was included in the core gene panel . 
clinical validation ( concordance , sensitivity , specicity ) of invisionseq lung for snvs and indels was evaluated in patients with concurrent matched tissue analysis for these select gene variants . 
structural rearrangements ( alk , ros1 ) were not evaluated in this study , because this testing was unavailable until the end of the study ( as part of a revised plasma - based assay ) when insufcient plasma volume remained from the initial collection . all statistical analyses were performed using r version 3.2.5. in the concordance analysis , the data can be summarized as a two - by - two table , in which tissue data are the standard reference material . 
to evaluate the prognostic value of ctdna as a dynamic biomarker of treatment efcacy , all patients underwent tumor imaging , including computed tomography of the chest and abdomen and / or positron emission tomography scan at baseline . 
the obtained within 6 weeks after treatment senior radiologist ( c.c. ) centrally reviewed the response rate ( rr ) and determined the best response according to recist version 1.1.15 the objective rr was dened as the percentage of patients with response ( complete or partial ) at rst restaging after chemotherapy initiation . 
progressionfree survival ( pfs ) was calculated from the date of chemotherapy initiation until the date of progression by recist version 1.1 or death ( that occurred without recorded progression ) , and censoring was the date of last follow - up if the patient had not experienced progression . 
statistical methods for correlative and trend analyses are described in the data supplement . results from june 2015 through april 2017 , 214 patients with advanced nsclc were recruited ; 156 treatment - nave patients were included ( treatment - nave cohort ) , and patients with unknown molecular status were also enrolled ( n = 58 ; treated rescue cohort )  . 
characteristics of the patients at enrollment are provided in appendix table a1 . in the whole population , 41% were women and 17% were never smokers ; the population had predominantly stage iv disease ( 77% ) and the adenocarcinoma subtype ( 75% )  . molecular prole was unknown at the time of enrollment for 29% of treatment - nave patients and for 48% of the overall study population . tissue molecular proling among the 156 treatment - nave patients , 111 ( 71% ) had successful tissue molecular prole analyses . 
in these patients , somatic mutations were found in 78% of patients ( n = 87 ) ; the highest frequencies were in kras ( 27% ) , egfr ( 6% ) , and braf ( 5% )  . 
of the remaining 103 patients ( n = 45 , treatmentnave ; n = 58 treated rescue cohort ) without prior tissue molecular analyses , either molecular testing was not performed ( 44% ) or tissue biopsies had insufcient quality or cellularity for testing ( 51% ) or results were not reported in patient referral records . ctdna molecular proling liquid biopsy ctdna proling was successfully performed for 91% of all patients ( n = 194 ; appendix table a2 ) , from a median plasma volume of 3.7 ml for dna extraction ( range , 2.4 to 5 ml )  . 
the time to complete testing for this research study was 10 days from receipt of sample . in the treatment - nave cohort ( n = treatment - nave cohort . 156 ; appendix table a2 ) , liquid biopsy analysis was successful for 142 patients ( 91% ) and , of these , mutations were detected in 111 patients ( 78% ) ; the most frequent were tp53 ( 52% ) , kras ( 28% ) , stk11 ( 16% ) , egfr ( 9% ) , and braf ( 6% ; fig 1 )  . 
of treatment - nave patients without tissue molecular testing ( n = 45 ; appendix fig a1 ) , mutations were detected in 37 patients , of which clinically relevant mutations were detected in 16 patients ( n = 1 , erbb2 exon 20 ; n = 1 , egfr exons 18 to 21 ; n = 11 , kras with and without stk11 ; and n = 3 , stk11 )  . in the rescue cohort ( n = 58 ; treated rescue cohort . appendix table a2 ) , liquid biopsy analysis was successful in 52 patients ( 90% ) , of whom mutations were detected in 38 patients ( 73% ; fig 2 )  . 
mutations included egfr exon 20 / 21 mutation ( n = 3 patients ) , erbb2 exon 20 in - frame insertion ( n = 1 patient ) and amplication ( n = 1 patient ) , met amplication ( n = 1 patient ) ; braf p.v600e ( n = 1 patient ) , pik3ca ( n = 3 patients ) , fgfr1 amplication ( n = 3 patients ) , and idh1 ( n = 1 patient ) ; potentially actionable molecular alterations were identied in 27% of this cohort . kras was detected in an additional 10 patients ( 19% of the cohort , including one case with concurrent stk11 ) , and just the stk11 mutation was detected in one additional patient . overall , 48% of the rescue cohort had clinically relevant mutations detected with liquid biopsy , and , among those patients with mutations detected in the liquid biopsy , 10% received personalized treatment according to these results . the feasibility of the liquid biopsy in the pooled analysis for all patients with nsclc without tissue molecular prole regardless of treatment line and with a successful liquid biopsy ( n = 41 treatment - nave patients and n = 52 previously treated patients ) was 90% , and 73% of samples had a mutation detected . 
in this population , utility of liquid biopsy was 17% ( n = 16 patients with potentially actionable alterations : n = 2 treatment - nave patients and n = 14 pretreated patients ) , and an additional 25 patients ( 27% ) had clinically relevant molecular information , mainly kras mutation with or without stk11 mutation ( appendix table a3 )  . 
liquid biopsy circulating tumor dna ( ctdna ) molecular proles of the previously treated rescue cohort that had unknown tissue molecular proles from primary tissue , with successful plasma - based testing by invisionseq ( n = 52 )  . the median time between tissue biopsy and liquid biopsy collection was 34 days . 
overall , concordance for the broader panel in which concurrent tissue testing was performed was 95% ; sensitivity and specicity were 72% and 97% , respectively ( appendix table a4 )  . 
there was an increase in detection when plasma testing was used in addition to tissue testing ( appendix fig a3 )  . longitudinal analysis of liquid biopsy only : unselected chemotherapy first - line treatment within the treatment - nave cohort , 31 patients had successful dynamic collection of ctdna at baseline and at day 42 after treatment initiation ( rst radiologic evaluation )  . serial liquid biopsies among patients with positive liquid biopsy at baseline who had at least one somatic mutation to track ctdna ( n = 20 ) demonstrated that the mutation burden ratio was signicantly correlated with change in response per recist version 1.1 at clinical assessment on day 42 ( p = .008 ; fig 5 )  . 
in our population , 29% of treatment - nave patients had an unknown tissue molecular prole at the time of enrollment , similar to previous series8 ; however , in other series , the rate of failure had reached up to 46% of patients.16 by contrast , we have shown the successful feasibility of amplicon - based ngs ctdna plasma analysis from patients with lung cancer : only 9% of patients did not achieve a ctdna prole because of insufcient sequencing depth . 
true comparative analysis studies ( with both analyses centralized ) in an nsclc population have reported similar rates of concordance.16 , 18 other series in patients with nsclc have reported concordance rates that range from 60% to 90% for specic mutations ( egfr mutations ) .19 however , some recent data in the cancer population have reported signicant discordance between tissueand plasma - based ngs sequencing tests20 and between different liquid biopsy tests , 21 which highlights the importance of robust analytic and clinical validation data for the choice of tests used in clinical practice . as the numbers of targeted therapies available and approved in lung cancer increase over time , a need exists for companion diagnostics for real - time detection of therapeutically targetable genetic lesions . 
among those 103 tissue molecular proles regardless of patients without treatment line , the amplicon - based ctdna analysis was the only means for molecular prole in 90% of cases ; identied potential actionable molecular alterations in 17% of cases , which may have allowed an increased percentage of patients to get the benet of personalized treatment . although we did not perform tests for rearrangements in this study , because plasma volume collected was insufcient after the assay was available , the percentage of potential actionable alterations reported is similar to that of previous series3 and within the range of expected frequency of these mutations . 
liquid biopsy mutation correlation to response rate as calculated by change in radiologic response ( recist 1.1 ) versus change in mutation molecules , representative of tumor mutation burden , after rst - line platinum - based chemotherapy in an unselected cohort with advanced nonsmall - cell lung cancer ( n = 31 )  . 
in our cohort , 44% of patients without tissue biopsy had ctdnadetected clinically relevant mutations for personalized treatment as well as putative negative predictive markers of immunotherapy efcacy , such as stk11 mutation.14 , 26 also , ctdna testing demonstrated feasibility of use as complementary to tissue testing because detection of clinically relevant mutations increased when plasma testing was used . 
ctdna testing may have implications for monitoring treatment efcacy , clinical especially in patients with high afs or with decreased ctdna and stable radiologic disease by recist , as a potential earlier marker of response . 
all of these observations merit additional evaluation . it remains unknown what the appropriate number of genes to be screened in tumor type - specic gene panels or as universal tests irrespective of the tumor type will be . 
progression - free survival plot in unselected patients with advanced nonsmall - cell lung cancer treated with rst - line platinumbased chemotherapy ; plot compares circulating tumor dna ( ctdna ) mutations at baseline . 
plasma ctdna release is affected by many factors25 ; previous reports have identied tumor burden and metastatic sites as factors associated with ctdna release.26 these factors were not fully evaluated in this study but could explain lack of detected driver mutations in some patients . 
however , the ctdna blood analysis was centralized and , in most cases , provided expanded gene coverage for molecular proling . in conclusion , our data provide additional validation that ctdna with invisionseq lung , an amplicon - based technology , can be used for molecular proling and to monitor disease in patients with advanced nsclc with high sensitivity and specicity to detect clinically relevant and actionable mutations when tissue biopsy is unavailable or uninformative . 
n engl j med 377 : 849 - 861 , 2017 barlesi f , mazieres j , merlio j - p , et al : routine molecular proling of patients with advanced nonsmall - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
novello s , barlesi f , califano r , et al : metastatic nonsmall - cell lung cancer : esmo clinical practice guidelines for diagnosis , treatment and follow - up . 
ann oncol 27 : v1 - v27 , 2016 kalemkerian gp , narula n , kennedy eb , et al : molecular testing guideline for the selection of patients with lung cancer for treatment with targeted tyrosine kinase inhibitors : american society of clinical oncology endorsement of the college of american pathologists / international association for the study of lung cancer / association for molecular pathology clinical practice guideline update . 
j clin oncol 36 : 911 - 919 , 2018 gutierrez me , choi k , lanman rb , et al : genomic proling of advanced nonsmall cell lung cancer in community settings : gaps and opportunities . 
clin lung cancer 18 : 651 - 659 , 2017 tredan o , corset v , wang q , et al : routine molecular screening of advanced refractory cancer patients : an analysis of the rst 2 , 490 patients of the proler study . 
cancer 121 : 631 - 639 , couraud s , vaca - paniagua f , villar s , et al : noninvasive diagnosis of actionable mutations by deep sequencing of circulating free dna in lung cancer from never - smokers : a proof - of - concept study from biocast / ifct - 1002 . 
gale d , lawson arj , howarth k , et al : development of a highly sensitive liquid biopsy platform to detect clinically relevant cancer mutations at low allele plos one 13 : e0193802 , 2018 fractions in cell - free dna . 
lindeman ni , cagle pt , aisner dl , et al : updated molecular testing guideline for the selection of lung cancer patients for treatment with targeted tyrosine kinase inhibitors : guideline from the college of american pathologists , the international association for the study of lung cancer , and the association for molecular pathology . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
kwapisz d : the rst liquid biopsy test approved : is it a new era of mutation testing for nonsmall - cell lung cancer ? ann transl med 5 : 46 , 2017 20 . 
guibert n , hu y , feeney n , et al : amplicon - based next - generation sequencing of plasma cell - free dna for detection of driver and resistance mutations in advanced nonsmall - cell lung cancer . 
mezquita l , jovelet l , lacroix l , et al : an amplicon - based liquid biopsy for detecting alk and ros1 fusions and resistance mutations in advanced nonsmallcell lung cancer ( nsclc ) patients . 
kim st , banks kc , lee s - h , et al : prospective feasibility study for using cell - free circulating tumor dnaguided therapy in refractory metastatic solid cancers : an interim analysis . 
skoulidis f , carter bw , zhang j , et al : association of stk11 / lkb1 mutations with primary resistance to pd - 1 / pd - l1 axis blockade in pd - l1positive nonsquamous nsclc . 
j clin oncol 36 , 2018 ( suppl ; abstr 9028 ) jordan ej , kim hr , arcila me , et al : prospective comprehensive molecular characterization of lung adenocarcinomas for efcient patient matching to approved and emerging therapies . 
 remon et al appendix blood samples and circulating tumor dna isolation and sequencing samples were considered acceptable for analysis if the dna extraction procedure could recover at least 2 , 000 input copies of the genome , as measured by droplet digital polymerase chain reaction . 
the revised 36 - gene panel required an average depth of 10 , 000 , and a minimum locus - specic read - depth requirement of 3 , 000 was applied for lung cancer stratication hotspots ( including egfr exon 19 deletions , l858r , t790m , braf v600e , and common kras activating mutations )  . 
individual variants were called using the inivata in - house analytic pipeline for somatic mutation detection . statistical methods all statistical analyses were performed using r version 3.2.5. clinical validation : concordance , sensitivity , specicity tissue positive , false negative ( fn ) ; and liquid negative and tissue negative , true negative ( tn )  . the following denitions were used : concordance = ( tp + tn ) / ( tp + tn + fp + fn )  . 
 ngs - based liquid biopsy analysis in advanced nsclc patients with advanced nsclc enrolled ( n = 214 ) liquid biopsy qc fail ( n = 6 ) treated rescue cohort : unknown tissue molecular profile ( n = 58 ) utility cohort treatment nave ( n = 156 ) liquid biopsy qc fail ( n = 4 ) treatment nave : unknown tissue molecular profile ( n = 45 ) liquid biopsy qc fail ( n = 10 ) biopsies after 100 days ( n = 7 ) patients with tissue and liquid biopsy molecular profile ( n = 101 ) evaluable for clinical validation ( n = 94 ) validation cohort fig a1 . 
flowchart of enrollment and cohorts for analysis : patients with advanced nonsmall - cell lung cancer ( nsclc ) were eligible for the study if they were treatment nave and expected to receive rst - line platinum - based chemotherapy ( treatment - nave cohort ) or were previously treated but did not have tissue - based molecular prole of a primary tissue sample available . 
invision ( inivata , research triangle park , nc , and cambridge , united kingdom ) gene panels : indicated is the coverage per gene , including hotspots , comprehensive or full coverage of coding regions ( 70% to 100% tiling coverage ) , and copy number variants ( cnvs )  . 
clinical characteristics of the patients observed for the overall population , treatment - nave cohort , and treated rescue cohort ngs - based liquid biopsy analysis in advanced nsclc no . 
ultrasound imaging identied a hypoechoic nodule in the right breast ; right axillary lymph node ne - needle aspiration biopsy performed at previous hospital on day 13 revealed invasive carcinoma with a focal micropapillary pattern ( fig 1 )  . immunostaining of estrogen receptor ( er ) and progesterone receptor ( pgr ) was evaluated by using the allred score and the allred scores were positive ( proportion score [ ps ] 1 ( , 1% ) , intensity score [ is ] 2 ) and negative ( ps 0 , is 0 ) , respectively.12 , 13 the tumor was human epidermal growth factor 2 ( her2 ) negative ( immunohistochemistry [ ihc ] 0 )  . 
given these results , she was diagnosed with stage iv breast cancer . targeted next - generation sequencing ( ngs ) analysis using the foundationone companion diagnostic panel ( foundation medicine , cambridge , ma ) was performed on the right axillary lymph node specimen . 
the result of ngs was reported on day 58 , and the ngs identied a ccdc6 - ret fusion ( c1 ; r12 ) with no other reported genomic alterations known to contribute to human breast tumorigenesis , including none in brca1 or brca2 . 
consistent with local standard - of - care guidelines , she received treatment with tamoxifen plus goserelin from day 14 to day 91 , but these were discontinued due to progression in the right breast and new lesions detected in the left lower lung . 
rebiopsy of the right breast tumor revealed the following results : er allred score 2 ( ps 1 [ , 1% ] , is 1 ) , pgr allred score 2 ( ps 1 , is 1 ) , her2 ihc 2 + , her2 uorescence in situ hybridization negative ( her2 / her2 / cep ( centromere ) 17 = 0.9 ) , and programmed death ligand 1 ( sp142 ) expression on tumor - inltrating immune cells of 1% - 4% . 
on day 126 , she was started on treatment with selpercatinib at the recommended phase 2 dose of 160 mg twice daily in the libretto - 001 study after providing written informed consent from the patient to publish information and images . 
 case report sorafenib and vandetanib , multikinase inhibitors with preclinical inhibitory activity against ret , have been used to treat unselected patients with breast cancer , but minimal clinical activity was observed.14 , 15 a patient with ncoa4 - retpositive breast cancer experienced a partial response to the multikinase inhibitor cabozantinib in combination with trastuzumab and exemestane although the cabozantinib dose was reduced for toxicity , the total time on treatment was short , and the relative contribution of each agent to the overall antitumor activity was not known.8 in addition , although cabozantinib has preclinical inhibitory activity against ret , its much stronger inhibition of other kinases ( eg , vegfr2 ) likely accounts for its clinical activity.16 , 17 in contrast , in the current case , the highly selective and potent ret inhibitor selpercatinib demonstrated a durable singleagent response in a patient with ret fusionpositive breast cancer . to our knowledge , this is the rst report of a breast cancer patient with a complete and sustained response to selective , ret - targeted therapy and adds to the diversity of ret fusionpositive tumor types that may benet from selective ret inhibition . 
rothenberg , kazuhiko nakagawa financial support : elizabeth olek administrative support : elizabeth olek provision of study materials or patients : elizabeth olek collection and assembly of data : satomi watanabe , tomoyuki otani , takeshi yoshida , kazuko sakai , elizabeth olek , s . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . masayuki takeda honoraria : astrazeneca kk , chugai pharma , bristol - myers squibb , novartis , ono pharmaceutical kazuko sakai honoraria : roche diagnostics , bio - rad , astrazeneca , chugai pharma elizabeth olek employment : loxo oncology inc stock and other ownership interests : loxo oncology , inc travel , accommodations , expenses : loxo oncology , inc s . 
michael rothenberg employment : loxo , pzer stock and other ownership interests : loxo , pzer jennifer kherani employment : loxo oncology at lilly , ajax health , aisling capital , summus global leadership : ajax health and aisling capital stock and other ownership interests : ajax health and aisling capital consulting or advisory role : ajax health and aisling capital travel , accommodations , expenses : ajax health and aisling capital , loxo pearl p . 
nature 511 : 543 - 550 , 2014 yoshihara k , wang q , torres - garcia w , et al : the landscape and therapeutic relevance of cancer - associated transcript fusions . 
nat med 18 : 378 - 381 , 2012 lipson d , capelletti m , yelensky r , et al : identication of new alk and ret gene fusions from colorectal and lung cancer biopsies . 
nat commun 9 : 4821 , 2018 drilon a , oxnard gr , tan dsw , et al : efcacy of selpercatinib in ret fusion - positive non - small - cell lung cancer . 
allison kh , hammond meh , dowsett m , et al : estrogen and progesterone receptor testing in breast cancer : american society of clinical oncology / college of american pathologists guideline update . 
miller kd , trigo jm , wheeler c , et al : a multicenter phase ii trial of zd6474 , a vascular endothelial growth factor receptor - 2 and epidermal growth factor receptor tyrosine kinase inhibitor , in patients with previously treated metastatic breast cancer . 
drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 17 . 
schlumberger m , elisei r , m uller s , et al : overall survival analysis of exam , a phase iii trial of cabozantinib in patients with radiographically progressive 2 , single - arm trial . 
 r precision oncology and the universal health coverage system in japan hiromichi ebi , md , phd1 , 2 , 3 and hideaki bando , md , phd4 although precision oncology is transforming clinical management of patients with cancer , many hospitals face challenges to effectively implement precision oncology . 
the most promising development is that tests to prole the genomes of select cancers are now fully covered by the national health insurance systein may 2019 , two gene panels were approved with reimbursement : foundationone cdx cancer genomic prole and oncoguide ncc oncopanel system , the latter of which was developed in japan . 
to make better use of scarce resources , the reimbursement is restricted to patients with solid tumors that have progressed on standard chemotherapy , rare tumors , or tumors of unknown primary . 
in addition , japans national cancer center launched a center for cancer genomics and advanced therapeutics ( c - cat ) that collects genomic information and clinical characteristics of patients who received genomic proling tests . 
the centralized system under the national health insurance system could be a double - edged sword . although tight regulation may make it hard to keep up with the rapid development of precision oncology , a federated ecosystem for sharing clinical and genomic data will be a precious asset and allow for shared access to data . 
high - cost medical expense benet also denes maximum out - of - pocket payment month according to household income of the patient . for example , the maximum is roughly $800 for a household income of approximately $34 , 000$70 , 000 . 
although for - prot insurance companies have voluntary health insurance programs , holding this type of insurance does not exempt an individual from mandatory enrollment in the universal health coverage scheme . 
the role of voluntary health insurance is supplemental and complements social health insurance benet packages . prices for all drugs and devices reimbursed by the universal health coverage system are the ofcial price set by the government ( japanese ministry of health , labor , and welfare [ mhlw ] )  . 
if a physician uses an unapproved device or off - label drug , any costs related to the patient , including but not limited to blood tests and physician fees , are not reimbursed . 
therefore , any cancer genomic proling tests must be examined and approved by the pharmaceuticals and medical devices agency ( pmda ) and mhlw before insurance reimbursement is set by the government , unless all the cost is to be paid by the patients . 
 ebi et al context key objective to summarize the framework of precision oncology recently arranged in japan . knowledge generated the japanese government designated core , hub , and liaison hospitals for cancer genomic medicine . 
also , reimbursement applies only to patients who nished standard chemotherapy , as a way to restrict potentially unnecessary investigations . relevance each country must design a precision oncology initiative under their distinct social care systejapan is an example of a centralized precision oncology under a universal health care coverage system . for clinical trials , even when gene proling testing identies actionable alterations . the japanese mhlw has a structured system to promote the development of drugs and devices under governmental regulations . 
although system a is designed for intervention with approved drugs / devices or minimally invasive intervention with unapproved drugs / devices , system b is designed for unapproved drugs or medical technologies . 
the patientrequested therapy system is also expected to be used as the japanese version of what the united states has hailed as the compassionate use prograto start off - label drug treatment using patient - requested therapy systems , it is necessary to pass several review processes equivalent to clinical trials , and the cost of the unapproved medical care should be fully paid by the patients . 
second , similar to the breakthrough therapy designation by the us food and drug administration , mhlw has the sakigake program , an accelerated inspection scheme for rapid authorization of unapproved drugs and devices . 
beginning around 2010 , pan - cancer genome screening started in japan by using researchuse only next - generation sequencing ( ngs ) panels.2 to promote genome - based clinical trials , the nationwide genome screening consortium for lung cancer was launched in february 2013 . 
the group , lc - scrum - japan , originally aimed to identify patients harboring ros1 and ret fusions originally discovered in japan.3 in february 2014 , gi - screen - japan multicenter screening project also started for gi cancer . 
the project began to screen for braf , nras , and pik3ca mutations in patients with metastatic colorectal cancer , using multiplex polymerase chain reaction ( pcr ) and luminex ( xmap ) technology.4 in february 2015 , these two groups merged into scrumjapan and started to use oncomine comprehensive assays as a screening platform.5 with the advent of plasma - based genome screening , scrum - japan subsequently started plasma - based ngs using guardant 360 . 
the screening and associated clinical trials have been research based , funded by government agencies through grant mechanisms ( the japan agency for medical research and development or the national cancer center research and development fund ) as well as by pharmaceutical companies . 
therefore , patients were not required to pay screening costs for any of these studies . from february 2013 to december 2018 , 6 , 860 and 6 , 391 patients were enrolled in lc - scrum - japan and gi - screenjapan , respectively . 
on the basis of this screening platform , 28 umbrella and 20 basket - type genome - based studies have been conducted.6 one of the notable accomplishments was a clinical trial of vandetanib , for patients with ret - rearranged nonsmall - cell lung cancer ( nsclc ) identied by the screening . 
 precision oncology in japan results of clinical trials conducted by lc - scrum japan led to the approval of crizotinib for the treatment of ros1translocated nsclc and the combination of trametinib and dabrafenib for use in patients with braf v600e - mutant nsclc . 
scrum - japan also contributed to the approval of in vitro diagnostic testing by pmda including simultaneous detection of ras and braf mutations in colorectal cancer , 8 oncomine dx target test cdx ngs panel for egfr and braf mutations and ros1 and alk translocations in nsclc , pcr - based microsatellite instability testing for solid tumors , 9 and plasma - based ras mutation testing for colorectal cancer.10 another notable genome screening is the top - gear ( trial of oncopanel for gene proling to estimate both adverse events and response ) project , which is a prospective cohort study conducted by japans national cancer center ( ncc ) to investigate the feasibility and utility of an ngsbased panel customized for japanese patients with cancer ( ncc oncopanel ) .11 this work was carried out within the context of the sakigake program and clinical utility was investigated within the advanced medical care b system . during the second stage of the top - gear project , 187 patients with advanced solid tumors obtained the gene proling data , and 25 ( 13.3% ) of them have received molecular - targeted therapy on the basis of their genome alterations.12 the achievements of this project led to governmental approval for the oncoguide ncc oncopanel system . some other medical university hospitals are also developing their own genome screening systems . 
these tests are performed under the advanced medical care b systekyoto university hospital ( oncoprime ) 13 , 14 and keio university hospital ( plessision - rapid ) offer their screening service outside of the national health care systerecently , keio university hospital started a whole - exon sequencing service ( plessision - exome )  . 
importantly , the report also concluded that cancer genome medicine should be accomplished under a universal health coverage systeafter the report , the japanese government designated 11 hospitals throughout japan to serve as core hospitals for cancer genomic medicine . 
the eligibility to be designed as a hub hospital is based on their ability to organize their resources and infrastructure akin to the core hospitals , which have their own molecular tumor board ( mtb ) and organic capabilities to run clinical trials . in addition , core hospitals have more responsibilities to train fellows and clinical coordinators and to be involved in translational research . 
liaison hospitals , on the other hand , are dependent on core and hub hospitals for their sequencing , reports , and mtb ( fig 1 )  . from the academia side , three major japanese cancerrelated societies ( the japanese society of medical oncology [ jsmo ] , the japanese society of clinical oncology [ jsco ] , and the japanese cancer association [ jca ] ) issued consensus clinical practice guidelines for ngs - based cancer tests in october 2017.18 the guideline dened the evidence level of each genomic alteration suitable for the japanese medical care system in harmony with classications of evidence levels set by regulators in the united states and european union ( eu ) .19 in june 2018 , japans national cancer center founded the center for cancer genomics and advanced therapeutics ( c - cat ) to coordinate an integrated network of core , hub , and liaison hospitals . 
c - cat is expected to aggregate and deploy cancer genomic medicine information to advance the quality of health care offered under the universal health coverage system and to devise new modalities of health care ( fig 2 )  . 
first , the center has been constructing a cancer knowledge database ( ckdb ) optimized for japan to assist in decision making by mtbs . c - cat will collect and share updated information on clinical trials , promoting and improving matching between patients genomic data and clinical trials . 
oncoguide ncc oncopanel system is a 114 - gene ngs panel for tumor and germline analysis developed by japans ncc and health instrument maker sysmex corp , and foundationone cdx cancer genomic prole ( foundation medicine ) sequences 324 genes and also can detect microsatellite instability . oncoguide ncc oncopanel system was approved as a device combining the oncoguide ncc oncopanel kit and the oncoguide ncc oncopanel analyzing systein contrast , although foundation medicine had to be reviewed 11 core hospitals 34 hub hospitals 122 liaison hospitals their quality for sample analysis by pmda for the approval , pmda could not perform assessment as an in vitro diagnostic because the analysis was done in the united states . 
first , physicians submit tumor samples for foundationone cdx analysis to foundation medicine , and foundation medicine performs sequencing and reports the variant calls in an xml le , uploaded to a portal site created by chugai , a subsidiary of roche . 
because this step is not subject to reimbursement , and to set up a procedure suitable for reimbursement , physicians need to download the xml le from the portal site and then send it back to foundation medicine . 
in addition , the japanese act on the protection information denes genomic sequence as of personal personal information that was amended in response to the general data protection regulation enacted by the eu . 
on comply with the law , written consent consent , samples are sent to third parties outside of japan to analyze personal information and sequence data . after approval by pmda , the mhlw granted the use of these two gene panel analyses and set the ofcial price of reimbursement at the end of may 2019 . 
the second reimbursement is 480 , 000 , applied after the physician explains the results to patients following train personnel for precision medicine play central role in running clinical trials based on molecular profiling translational research run molecular tumor board run clinical trials based on molecular profiling provide patients with genomic testing interpretation is supported by core and hub hospitals refer patients to core and hub hospitals for clinical trial fig 1 . 
the test is approved for patients with solid tumors that have progressed on standard chemotherapy , with rare tumors , or with cancers of unknown primary . foundationone cdx is also approved for the use of companion diagnostic tests , such as those for the detection of egfr , ras , and braf mutations during standard care . for these companion dihowever , agnostic tests is much cheaper . 
furthermore , the results obtained outside of companion diagnostics will not be taken the reimbursement into consideration for decision making about treatment even when the test analyzes a number of genes . 
if a physician uses a test result during standard care , the difference for companion between the amount of reimbursement diagnostics and the actual cost paid to foundation medicine will be a decit for the hospital . 
if the physician wants to use the test results when the patient experiences progression while receiving standard therapy , additional reimbursement can be submitted as a fee for mtb ( 480 , 000 )  . 
 precision oncology in japan patient dies during standard care or fails to follow - up , it is unlikely that genome proling would be used during standard therapy in japan under current reimbursement rules . although only a few hospitals run these genome panels inhouse , most hospitals outsource these genomic proling tests to a clinical testing company . 
laboratories in core and hub hospitals are required to be certied by independent organizations such as iso15189 to handle patient samples . clinical testing companies also have clinical laboratory improvement amendments certication . 
formalin - xed and parafn - embedded samples ( and also blood samples in case of oncoguide ncc oncopanel system ) are prepared in each hospital and sent to the company . 
turnaround time in general is 16 to 22 days . to fulll its function as a data repository and to facilitate access to clinical data , a requirement of test granted by the government is that physicians need to submit detailed clinical data from patients with cancer to c - cat , including diagnostics , treatment , and outcomes information , as well as the raw bam or fastq and vcf or xml les ( fig 2 ; in japan , each hospital has an appendix table a1 )  . electronic platform that contains individual health records for patients . 
test results are usually reported in pdf les that are incorporated into electronic medical records , making it difcult for physicians to match patients with ongoing clinical trials or to identify patients who are eligible for new drugs when they become available . thus , a central data repository at c - cat will make it easier to identify candidates for clinical trials in a timely manner . using the submitted data , c - cat also issues their own report . 
ckdb1 is further divided into four databases : marker database listing genomic abnormalities such as egfr mutation or brca1 germline mutation ; drug database listing approved drugs or drugs under clinical trials in and outside of japan and their targets ; evidence database curated from biologic , clinical , and therapeutic information in multiple public information resources , including civic ( clinical interpretation of variants in cancer ) , brca exchange , clinvar , and cosmic ( catalogue of somatic mutations in cancer ) ; and a clinical trial database generated from clinicaltrials.gov as well as several japanese clinical trial registries . 
for instance , a patient with a druggable mutation needs to be treated by the appropriate drug , even as an off - label indication in the absence of a clinical trial or current approval . 
patient - requested therapy system , a japanese compassionate use program , has to be initiated by the request from a patient to the government with required documentation from physician . because the preparation of documents is a heavy burden for physicians , the system has not been widely adopted . also , as mentioned above , the cost of the drug has to be fully paid by the patient . 
to enable large basket / umbrella trials , a core facility supporting the protocol creation , drug distribution , monitoring , and audit will be needed , similar to the cancer therapy evaluation program in the united states . the other big challenge facing japanese precision oncology is the timing of reimbursements for genome proling tests . 
in addition , it was difcult to grant the use of cancer genomic proling during standard care because clear evidence for the benet of testing did not exist when consensus clinical practice guidelines for ngs - based cancer testing were published . 
for example , french clinical trials suggested the use of molecularly targeted agents outside established indications do not improve progression - free survival for heavily pretreated patients with cancer when compared with oncologists preferred treatment regimen.20 however , patients who experienced progression while receiving standard chemotherapy tend to have poor performance status and may not have enough time to wait for the results of genomic testing ; even in the very best case scenarios , their tumors will continue to grow and their health worsen each day that they are required to wait . 
currently , uncovered genome screening services are the only option for patients without rare tumors and before disease progression with standard therapy . quality and sustainability of mtbs are also challenging . 
however , a problem that arises is that it is challenging to demand this level of participation of physicians , given their limited availibility.21 overall , the cost for precision oncology is a heavy burden for hospitals . 
to put this into global perspective , memorial sloan kettering cancer center has already achieved clinical sequencing of 10 , 000 patients in the united states.22 furthermore , the united kingdom nished sequencing for  . 
in september 2019 , the mhlv unveiled a project with the goal of sequencing whole genomes from 100 , 000 patients with cancer over 3 years , a number chosen by referring to the united kingdoms sequencing achievements . 
although details of the project have not emerged yet , it is expected to result in the analyses of fresh frozen samples in collaboration with biobanks at core and hub hospitals . 
as the primary aim is to accelerate the development of new diagnostics and treatments , the project should be research based and funded by the japanese government and private sources . 
although the primary purpose of this initiative in precision oncology is to harness articial telligence ( ai ) for improved genomic analyses and drug target identication , the use of ai could connect genomic data with other prioritized areas in this initiative , such as pathology and radiology . 
the relatively homogenous genetic background of the japanese population and the detailed clinical outcomes collected by c - cat will be an advantage when harnessing the power of genomic data to develop new therapies . 
also , the genomic and clinical data would be integrated with other japanese databases , such as the medical genomics japan variant database and the japanese multi omics reference panel.23 conclusion in conclusion , precision oncology covered by the health insurance system has just begun in japan . 
on the other hand , although the japanese health care system has so far achieved excellent health outcomes with a relatively low cost , 24 the centralized structure under the national health insurance system with its inherent tight regulation may cause difculty in keeping up with the rapid development of precision oncology . 
in the united kingdom , genomics england was founded as a subsidiary limited company , as it was the most effective way to ensure the project running as quickly as possible . 
in the united states , for instance , protocols and treatment decisions surrounding personalized medicine are largely decided by the institutions treating the patients , with governing bodies like the national cancer institute playing ancillary roles and the ability to pay for patient care largely dictated by individuals private insurance policies . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . hiromichi ebi honoraria : taiho pharmaceutical , astrazeneca consulting or advisory role : merck serono , eli lilly , astellas pharma hideaki bando honoraria : taiho pharmaceutical , lilly japan , takeda , chugai pharma , sano , yakult honsha research funding : astrazeneca , sysmex no other potential conicts of interest were reported . acknowledgment we thank anthony faber , md ( vcu massey cancer center ) , for critical reading of the manuscript . references 48 : 559 - 564 , 2018 sakamoto h , rahman m , nomura s , et al : japan health system review . 
nat med 18 : 375 - 377 , 2012 bando h , yoshino t , shinozaki e , et al : simultaneous identication of 36 mutations in kras codons 61 and 146 , braf , nras , and pik3ca in a single reaction by multiplex assay kit . 
hovelson dh , mcdaniel as , cani ak , et al : development and validation of a scalable next - generation sequencing system for assessing relevant somatic variants in solid tumors . 
yoh k , seto t , satouchi m , et al : vandetanib in patients with previously treated ret - rearranged advanced non - small - cell lung cancer ( luret ) : an open - label , multicentre phase 2 trial . 
lancet respir med 5 : 42 - 50 , 2017 taniguchi h , okamoto w , muro k , et al : clinical validation of newly developed multiplex kit using luminex xmap technology for detecting simultaneous ras and braf mutations in colorectal cancer : results of the rasket - b study . 
neoplasia 20 : 1219 - 1226 , 2018 bando h , okamoto w , fukui t , et al : utility of the quasi - monomorphic variation range in unresectable metastatic colorectal cancer patients . 
bando h , kagawa y , kato t , et al : a multicentre , prospective study of plasma circulating tumour dna test for detecting ras mutation in patients with metastatic colorectal cancer . 
sunami k , ichikawa h , kubo t , et al : feasibility and utility of a panel testing for 114 cancer - associated genes in a clinical setting : a hospital - based study . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular proling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
nucleic acids res 46 : d551 - d557 , 2018 ikegami n , yoo bk , hashimoto h , et al : japanese universal health coverage : evolution , achievements , and challenges . 
 o year 1 in the molecular era of pediatric brain tumor diagnosis : application of universal clinical targeted sequencing in an unselected cohort of children purpose next - generation sequencing is gaining acceptance as a clinical tool to aid diagnosis and guide treatment of pediatric cancer . 
here , we report an unselected prospective cohort study to evaluate the clinical use of universal targeted sequencing in pediatric patients with brain tumors . methods we applied a universal sequencing protocol for all tumors of the cns undergoing diagnostic workup at seattle childrens hospital during the study period of november 2015 to november 2016 . 
all tumors were sequenced using the uw - oncoplex platform , which is a multiplexed targeted deep gene sequencing panel that detects genetic alterations in 262 cancer - related genes performed in a college of american pathologists accredited clinical laboratory improvements amendmentscertified laboratory . results eighty - eight patients underwent diagnostic evaluation during the study period , of which 85 tumors ( 95% ) yielded sufficient dna for sequencing , including 59 newly diagnosed and 26 relapsed . 
of these , 57 ( 67% ) had disease - defining or disease - modifying mutations , 44 ( 52% ) had potentially targetable mutations , and 31 ( 36% ) had mutations requiring germline follow - up . 
2018 by american society of clinical oncology introduction high - throughput genomic and epigenomic technologies have recently been used to thoroughly describe the genomic landscape of pediatric brain tumors.1 - 3 this work has transformed our understanding of the molecular basis of these diseases , 4 which are the leading cause of pediatric cancer death.5 the current challenge for the field of pediatric neuro - oncology is to translate this knowledge into clinical practice . the 2016 revision of the who classification of cns tumors has begun to incorporate molecular findings into tumor diagnosis in addition to traditional histopathology.6 however , there is currently no consensus regarding best - practice diagnostics for routine clinical practice . 
recently , a few institutions have reported the use of clinically validated next generation sequencing ( ngs ) panels to identify molecular alterations in selected subsets of pediatric patients with brain tumors.7 - 10 these studies demonstrated that molecular profiling is bonnie l . 
atrt , atypical teratoid rhabdoid tumor ; dnet , dysembryoplastic neuroepithelial tumor ; etmr , embryonal tumor with multilayer rosettes ; gg , ganglioglioma ; nos , not otherwise specified ; pxa , pleomorphic xanthoastrocytoma . feasible and that clinically relevant genetic alterations may be identified . methods instability the uw - oncoplex version 5 test is a multiplex gene sequencing panel used to detect alterations in 262 cancer - related genes , including single nucleotide variants , small insertions or deletions , amplifications , selected translocations , and microsatellite ( washington.edu / tests / genetics / uw - oncoplex )  . 
in a retrospective pilot study using this test , sequencing identified a large proportion of targetable mutations in high - grade supratentorial tumors.11 we hypothesized that the use of a selected or convenience cohort in our retrospective pilot as well as all prior studies may have identified a higher proportion of actionable findings that would not necessarily be applicable to the wider population of all patients undergoing pathologic diagnosis of pediatric brain tumor.7 - 12 we designed this follow - up , prospective , unselected cohort study to evaluate the feasibility and impact of the universal application of molecular tumor testing on routine pediatric brain tumor diagnosis and to also assess how molecular results may alter medical management . all tumors of the cns undergoing diagnostic evaluation at seattle childrens hospital from november 2015 to november 2016 were included in this study . 
details of the laboratory workflow and methods are included in the data supplement . results demographics and sample characteristics we identified 88 patients who met the clinical and diagnostic inclusion criteria ( fig 1 )  . 
 of these , 97% ( 85 of 88 ) had sufficient dna obtained for sequencing , and only three patients did not have adequate tissue in formalin - fixed paraffin - embedded ( ffpe ) blocks to perform ngs . 
of patients ( % ) * targeted agent braf inhibitor mek inhibitor fgfr inhibitor braf v600e , brafpa598t599insv ganglioglioma , pleomorphic xanthoastrocytoma , pilocytic astrocytoma , desmoplastic infantile ganglioglioma / astrocytoma kiaa1549 - braf fusion , nf1 mutations and deletions , ptpn11 mutation pilocytic astrocytoma , anaplastic astrocytoma , pleomorphic xanthoastocytoma fgfr1 mutations and duplication , fgfr3 fusions pilocytic astrocytoma , dysembryoplastic neuroepithelial tumor , diffuse astrocytoma , ganglioglioma mtor pathway inhibitor mtor , fbxw7 diffuse midline glioma , medulloblastoma smo inhibitor ptch1 mutations medulloblastoma pd1 / pdl1 inhibitor biallelic msh2 loss , pms2 mutation with loh anaplastic astrocytoma , medulloblastoma pdgfra inhibitor pdgfra amplification diffuse midline glioma met inhibitor kit inhibitor met amplification kit amplification diffuse midline glioma diffuse midline glioma cdk4 / 6 inhibitor cdk4 amplification glioblastoma ezh2 inhibitor loss of smarcb1 atypical teratoid rhabdoid tumor * ten patients had more than one targetable mutation in their tumors . 10 ( 12 ) 18 ( 21 ) 10 ( 12 ) 3 ( 4 ) 3 ( 4 ) 2 ( 2 ) 2 ( 2 ) 2 ( 2 ) 2 ( 2 ) 1 ( 1 ) 1 ( 1 ) were sequenced , including 59 newly diagnosed tumors and 15 tumors from patients with a radiologic relapse during the time of this study . 
 eleven additional patients had sequencing of newly resected recurrent tumors . patients were a median age of 10 years ( range , 3 months to 22 years ) and 49% female ( 42 of 85 )  . 
medical history included only three patients with previously known cancer predisposition syndrome ; two patients had neurofibromatosis type 1 and one had neurofibromatosis type 2 . genetic results the average depth of sequencing coverage was 441 ( range , 102 to 1 , 112 )  . 
five reports with turnaround times of > 60 days were from patients with minimal tissue that required cutting additional ffpe sections with subsequent repeat dna extraction . genetic result details are shown in data supplement 1 , and criteria for tiers of alterations are listed in appendix table a1 . 
genetic alterations were found to be disease defining or modifying in 67% ( n = 57 ) , targetable with an available therapeutic drug in 52% ( n = 44 ; table 1 ) , and potentially germline associated with cancer predisposition in 36% ( n = 31 )  . 
as of the last follow - up , seven patients ( 8% of total , 16% of those with an identified molecular target ) had been prescribed targeted agents ; molecularly targeted agents were obtained through insurance - approved off - label use in five patients and through enrollment in a clinical trial in two patients . analysis of tumor subtypes tumors were analyzed separately as high - grade glioma ( hgg ) , low - grade glioma ( lgg ) , medulloblastoma , and other rare pediatric cns tumors . 
 medulloblastoma ngs results were correlated with traditional histology , immunohistochemistry , and fluorescence in situ hybridization studies.6 , 13 all 20 medulloblastomas were able to be classified into subgroups as defined by the who , 6 , 14 including a wingless ( wnt ; n = 1 ) , sonic hedgehog ( shh ; n = 7 ) , or non - wnt / non - shh group ( n = 12 ; fig 3 )  . 
for example , one patient with a wnt pathway medulloblastoma had only weak nuclear beta catenin staining ; in this patient , the finding of a ctnnb1 mutation and copy loss consistent with monosomy 6 by ngs helped place this tumor firmly in the wnt - activated subgroup . 
in another instance , an shh group medulloblastoma that was gab1 immunopositive displayed ambiguous p53 immunohistochemical staining of approximately 40% of tumor cell nuclei ; ngs not only confirmed the shh subgroup by finding sufu mutations , but also confirmed that this tumor contained a tp53 mutation . 
as of the last follow - up , two patients in the relapsed shh group with ptch1 mutations had been prescribed smo inhibitors , one of whom experienced a partial response to treatment . forty - four lggs were analyzed ( fig 4 )  . 
 a , high - grade astrocytoma ; aa , anaplastic astrocytoma ; apa , anaplastic pilocytic astrocytoma ; dipg , diffuse intrinsic pontine glioma ; gbm , glioblastoma ; hgg , high - grade glioma , not otherwise specified . pik3ca pten smarcb1 msh2 idh1 pdgfra h3f3a atrx cdk6 cdkn2a tp53 ptpn11 v600 mutations and 10 braf - kiaa translocations . 
 twenty - nine patients with lgg had targetable mutations , and at the last follow - up , three patients had been prescribed targeted therapy with a braf inhibitor for braf v600e mutation , two at the time of recurrence and one as initial therapy for unresectable brainstem tumor . 
 three patients with lgg were confirmed to have germline mutations , including the two known patients with nf1 and one patient with a recurrent pleomorphic xanthoastrocytoma who was confirmed to have a germline tp53 mutation in addition to a braf v600e mutation in the tumor ; the patient was treated with a braf inhibitor instead of radiation for recurrent tumor and continues without disease progression with > 12 months of receiving targeted therapy . 
molecular profiling did not alter treatment of the 17 patients in the lgg group with completely resected primary tumors . eleven other uncommon tumors were evaluated ( fig 5 ) , including six nonmedulloblastoma embryonal tumors , choroid plexus carcinoma , choroid plexus papilloma , vestibular schwannoma , rhabdoid meningioma , and chordoma . 
one patient had a known nf2 mutation , and the other two patients tested negative for smarcb1 ( atypical teratoid rhabdoid tumor ) and tp53 ( choroid plexus carcinoma )  . analysis of primary versus recurrent tumors considering newly diagnosed patients , 85% ( n = 50 of 59 ) had clinically relevant mutations , including disease - defining or disease - modifying mutations in 76% of tumors ( n = 45 ) , targetable mutations in 46% of tumors ( n = 27 ) , and potentially germline mutations in 41% of tumors ( n = 24 )  . of the 15 primary tumors sequenced at the time of radiologic relapse , 10 ( 67% ) were found to have clinically significant molecular alterations considered disease defining , and nine ( 60% ) identified molecular targets for therapy . 
 of 11 tumors sequenced using newly resected tumor obtained at the time of recurrence , clinically significant alterations were identified in eight ( 73% )  . discussion germline sequencing germline dna was not collected at the time of somatic sequencing in this study . 
however , somatic sequencing identified mutations considered to be potentially germline in 31 of 85 of tumor samples ( 36% ) on the basis of variant interpretation , which led to initiation of clinical follow - up and genetic counseling to recommend germline evaluation . 
in this population , germline sequencing has been performed on 13 patients , and germline mutations were confirmed in nine patients ( 75% of those tested ; 10.6% of the study population ) as of the last follow - up . 
 one patient had ctnnb1 mutation with monosomy of chromosome six diagnostic of wingless ( wnt ) subgroup , seven had either ptch1 or sufu mutations characteristic of sonic hedgehog ( shh ) subgroup , and the other 12 were non - shh / nonwnt group ; three of our seven shh group tumors were tp53 mutant . 
in the group of newly diagnosed patients , alterations were identified in 85% of patients ( n = 50 of 59 ) , a finding that was contrary to our hypothesis that selected cohorts previously reported by our group and others may have been limited by a selection bias increasing the likelihood of clinically relevant findings.7 , 8 , 11 , 12 targetable mutations were identified in 44 tumors ( 52% ) , and seven of these patients ( 8% ) have been prescribed targeted therapeutic agents to date . 
this number likely underestimates the longer - term use of targeted therapy because the study has a relatively short follow - up period and there are effective standard treatment regimens of cytotoxic therapy for most diagnoses . 
if successful , the routine use of targeted agents will greatly increase in patients with pediatric brain tumors . the main aims of cancer genomic profiling tests are to identify somatic mutations . 
it is crucial to include genetic counseling in oncology care , ideally with a geneticist or genetic counselor embedded into the pediatric oncology clinic.15 in this study , we identified 31 patients ( 36% ) with potential germline mutations . 
 be difficult to overstate in a patient for whom radiation therapy is being considered , because the long - term second malignancy rate in these patients who undergo therapeutic irradiation approaches 100%.16 molecular profiling is important for the diagnosis and management of pediatric patients with brain tumors , 6 although at present , there are several competing platforms and currently no diagnostic gold standard . 
whatever platform is used must be clinically validated and should balance cost , turnaround time , and ability to identify clinically relevant mutations in small samples , which is no small task . 
 alternatively , many research studies have argued the advantages of potentially subclassifying pediatric brain tumors primarily by rna - based gene expression17 or methylation analyses.18 however , these types of platforms are difficult to establish fig 4 . 
the majority of low - grade gliomas in our series had dysregulated braf signaling , which included 10 ( 26% ) with braf fusions and 10 ( 26% ) with codon 600 mutations ; these alterations were considered both targetable and either disease defining or modifying . 
ag , angiocentric glioma ; da , diffuse astrocytoma ; dig / dia , desmoplastic infantile ganglioglioma or desmoplastic infantile astrocytoma ; dnet , dysembryoplastic neuroepithelial tumor ; ep , ependymoma ; gg , ganglioglioma ; lgg , low - grade glioma , not otherwise specified ; o , oligodendroglioma ; pa , pilocytic astrocytoma ; pma , pilomyxoid astrocytoma ; pxa , pleomorphic xanthoastrocytoma . atrx cdk6 cdkn2a tp53 ptpn11 fgfr3 fgfr1 braf with the degree of reliability that clinical testing requires for use on a single - patient basis , and even if molecular classification was established , expression or methylation analysis might not identify candidates for targeted therapy . 
as an example , although shh pathway medulloblastoma may be reliably identified with immunohistochemistry , 13 nanostring , 17 or methylation profiling , 18 none of these platforms is specific for the site of mutation , which is required for consideration of therapy with a smoothened inhibitor that would be predicted to be effective in ptch1 mutant tumors but unlikely to be effective in the case of downstream alterations , such as gli1 amplification . 
 similarly , braf inhibitor therapy is indicated in braf v600 mutant tumors but contraindicated in braf fusion.19 the detection of fusions such as braf using a dna - based platform such as uw - oncoplex requires the specific inclusion of intronic regions in sequencing . 
alternatively , rna - based sequencing analysis may have an advantage in identifying fusions and splice variants that would be missed on a dnabased platform that does not include intronic sequencing . although 80% of our patients had clinically relevant mutations identified , this means that 20% of tumors sequenced did not have clinically relevant mutations . 
one limitation of this study and other similar studies is that not all known clinically relevant genetic alterations are yet able to be identified on any one clinically validated panel . 
for example , the angiocentric glioma would be expected to have an myb fusion , 20 embryonal tumor with multilayer rosettes would be expected to have mir c19 cluster amplification , 21 and a subset of midline gliomas would be expected to have acvr1 alterations , which are not yet included in this version of the test.22 one advantage of using a targeted sequencing panel is the ability to add and validate targets rapidly with minimal increase in cost . 
however , turnaround time can be shortened with experience , because it is most dependent on clinical interpretation and data generation may be relatively short . another question that our study did not address was the cost comparison between sequential single - gene sequencing in specific diagnostic entities . 
although single - gene testing for the most common variations costs less than a panel , it is not clear that the overall cost of sequential sequencing would be decreased for the population . 
if even a small minority of patients required three - gene testing or subsequent biopsy if tissue were depleted , then there may be a benefit to the population from an initial multiplexed approach . molecular profiling may be particularly useful in patients in whom the histologic diagnosis is unclear . 
 mutations in smarcb1 ( p.p374rfs * 100 ) , bap1 ( p.q392 * ) , pten ( p.g36e ) , nf2 ( p.q319 * ) , and tp53 ( p.r175h ) were all considered both disease defining and potentially germline . 
because only two of our h3f3a k27m mutant diffuse midline gliomas were classic radiologic diffuse intrinsic pontine gliomas , it is important to evaluate for this diagnostic entity whenever a diffuse midline glial neoplasm is encountered . this study provides rigorous evidence regarding the use of routine molecular profiling of an unselected cohort of pediatric brain tumors . 
 on the basis of the analysis presented here , we recommend incorporation of routine molecular profiling into standard clinical practice for all newly diagnosed pediatric hggs , medulloblastomas , and incompletely resected lggs . 
this may be especially important in patients who have undergone stereotactic biopsy in which tumor tissue is severely limited . there was one subgroup in which sequencing did not affect medical care . 
lockwood travel , accommodations , expenses : cambridge healthtech institute shannon stasi no relationship to disclose jeffrey stevens stock and other ownership interests : seattle genetics amy lee no relationship to disclose jeffrey g . 
leary no relationship to disclose acknowledgment we extend our deepest thanks to michael astion , md , medical director of seattle childrens hospital department of laboratories , for his tireless support of this project . 
kool m , korshunov a , remke m , et al : molecular subgroups of medulloblastoma : an international meta - analysis of transcriptome , genetic aberrations , and clinical data of wnt , shh , group 3 , and group 4 medulloblastomas . 
kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identifies pathogenic germline mutations , and directs targeted therapy . 
ramkissoon sh , bandopadhayay p , hwang j , et al : clinical targeted exome - based sequencing in combination with genome - wide copy number profiling : precision medicine analysis of 203 pediatric brain tumors . 
bandopadhayay p , ramkissoon la , jain p , et al : myb - qki rearrangements in angiocentric glioma drive tumorigenicity through a tripartite mechanisnat genet 48 : 273 - 282 , 2016 21 . 
patients with medulloblastoma were subgrouped on the basis of both histology and standard immunohistochemistry methods for beta - catenin ( dako 1 : 200 ) , gab1 ( santa cruz 1 : 100 ) , and p53 ( protein tech 1 : 50 ) .13 the study pathologist estimated the percentage of tumor and selected appropriate formalin - fixed paraffin - embedded ( ffpe ) blocks for testing . 
it was collected at a separate encounter only if a possible deleterious germline mutation was detected that needed to be investigated further . template preparation , gene capture , massively parallel sequencing , and bioinformatics . sequencing was preformed using a clinically validated method performed in a college of american pathologistsaccredited clinical laboratory improvements amendmentscertified laboratory as previously reported ( pritchard et al , j mol diagn 16 : 56 - 67 , 2014 )  . 
sequencing libraries were prepared from dna samples and hybridized to a custom set of complementary rna biotinylated oligonucleotides targeting the exons of 262 genes and select intronic regions , for a total of > 1.4 mb of targeted dna sequenced ( agilent sureselect ; agilent technologies , santa clara , ca )  . 
uw - oncoplex assay version 5 is a targeted , massively parallel gene sequencing assay that detects mutations in 262 cancer - related genes ( washington.edu / uw - oncoplex )  . 
the test uses next - generation deep sequencing to detect mutations , including single nucleotide variants ( snvs ) , insertions and deletions ( indels ) , copy number changes including gene amplifications , selected structural rearrangements such as gene fusions , and microsatellite instability . 
uw - oncoplex was performed on samples from the seattle childrens hospital cohort , as previously described ( pritchard et al , j mol diagn 16 : 56 - 67 , 2014 ; salipante et al , clin chem 60 : 1192 - 1199 , 2014 )  . dna was extracted from ffpe solid tumor tissue samples using the gentra puregene dna isolation kit ( catalog #158489 ; qiagen , valencia , ca )  . 
hematoxylin and eosinstained slides were reviewed before dna extraction for all ffpe samples , and when feasible , macrodissection of tumor - containing regions was performed to enrich tumor cellularity . 
sequencing libraries were constructed from a minimum of 200 ng of dna using kapa hyper prep kits ( kapa biosystems , wilmington , ma ) , and hybridization was performed with custom agilent sureselect probes ( agilent technologies , santa clara , ca )  . 
dna sequencing was performed on a hiseq2500 sequencing system ( illumina , san diego , ca ) with 2 101bp , paired - end reads , and on a nextsequation 500 ( illumina ) with 2 150bp , paired - end reads according to the manufacturers instructions . 
for copy number variation ( cnv ) analysis , copy number states for individual probes were initially called using contra version 2.0.5 ( files ) with reference to a cnv control comprising reads from two independent rounds of library preparation and sequencing of the hapmap individual na12878 . 
adjacent exons were merged into larger segments if the read depths of their component baits were not significantly different ( p > .001 ) by students t test , and read - depth statistics were recalculated for the larger segments . 
filters are applied to exclude variants extremely unlikely to be clinically significant , including variants in intergenic dna , and variants are removed that are present at > 1% frequency in general population databases ( as reported by the exome variant server , 1000 genomes , and the exome aggregation consortium )  . 
variants of interest are subsequently evaluated in conjunction with a combination of multiple external databases ( cosmic , iarc , insight , clinvar ) , literature review ( for newly described mutations ) , and algorithms ( splice prediction tools )  . three separate expert molecular oncology reviewers independently cull data to a list of potentially reportable variants and review quality of data for variant calls by examining genotype quality score metrics , evaluating base call quality , assessing mapping quality , and evaluating other quality assessments as indicated for specific alterations . 
 once the molecular oncology experts agree on a final list of reportable variants , one laboratory director composes a fully customized , formal report that is available in the electronic health record . 
the shh subgroup was initially identified by mutations ( snvs , indels , structural alterations , and copy number alterations ) in ptch1 , smo , sufu , and copy loss for genes on the long arm of chromosome 10 . 
each month , all new patients were systematically reviewed in a presentation format consisting of clinical features and magnetic resonance imaging presented by a neuro - oncologist ( s.e.s.l. ) , histologic findings and photomicrographs by a pediatric pathologist ( b.l.c. ) , molecular results by a molecular pathologist ( c.m.l. ) followed by group discussion . 
the molecular tumor board welcomed rotating trainees from all disciplines and included attendance of trainees from oncology , neurosurgery , pathology , laboratory medicine , medical genetics , and medical students . 
when applicable , a new final integrated diagnosis was reported in the pathology addendum . genetic alterations were considered to be clinically significant as defined by meeting criteria for at least one of the following three categories : ( 1 ) alterations that define a diagnosis or molecular subtype , for example , an activating beta - catenin mutation in wnt - subtype medulloblastoma ; ( 2 ) alterations that identify a proven therapeutic target , such as braf v600e ; and / or ( 3 ) alterations that identify possible deleterious germline mutation associated with cancer predisposition syndrome , such as tp53 . 
with consideration of the variant allele fraction as well as previously described genes associated with cancer predisposition , additional constitutional follow - up testing was recommended for the patients with potential germline mutations , which was coordinated by a genetic counselor . 
 efcacy of vemurafenib in patients with nonsmall - cell lung cancer with braf v600 mutation : an open - label , single - arm cohort of the histology - independent ve - basket study vivek subbiah , md1 ; radj gervais , md2 ; gregory riely , md , phd3 ; antoine hollebecque , md4 ; jean - yves blay , md , phd5 ; enriqueta felip , md , phd6 ; martin schuler , md7 ; anthony gonalves , md , phd8 ; antonio italiano , md , phd9 ; vicki keedy , md10 ; ian chau , md11 ; igor puzanov , md12 ; noopur s . 
raje , md13 ; funda meric - bernstam , md1 ; martina makrutzki , md14 ; todd riehl , pharmd15 ; bethany pitcher , mmath16 ; jose baselga , md , phd3 , 17 ; and david m . 
hyman , md3 , 17 purpose to study whether braf v600 mutations in nonsmall - cell lung cancer ( nsclc ) may indicate sensitivity to the braf inhibitor vemurafenib , we included a cohort of patients with nsclc in the vemurafenib basket ( ve - basket ) study . 
we present results from this cohort . methods this open - label , histology - independent , phase ii study included six prespecied cohorts , including patients with nsclc , and a seventh all - comers cohort . 
because the prespecied clinical benet endpoint was met in the initial nsclc cohort , the cohort was expanded . results sixty - two patients with braf v600mutant nsclc were enrolled and treated : 13% ( n = 8 ) had received no prior systemic therapy , and 87% ( n = 54 ) had received prior therapies . 
the safety prole of vemurafenib was similar to that observed in melanoma studies . conclusion vemurafenib showed promising activity in patients with nsclc harboring braf v600 mutations . the safety prole of vemurafenib was similar to previous observations in patients with melanoma . 
 subbiah et al context key objective to establish the efcacy and safety of vemurafenib in patients with braf v600 mutation - positive nsclc who were enrolled in the histology - independent vemurafenib basket ( ve - basket ) trial . knowledge generated vemurafenib has prolonged efcacy in patients with braf v600mutant nsclc ( n = 62 ) , as demonstrated by a 37% overall response rate . 
no new safety signals were observed in this expanded cohort of patients with nsclc . relevance single - agent vemurafenib has clinically meaningful and durable activity in patients with nsclc harboring braf v600 mutations . 
this analysis adds to the overall ndings of the ve - basket trial , which demonstrated clinically relevant activity of vemurafenib in a number of solid tumors . clinical study of patients with braf v600emutated nsclc.14 dual braf / mek inhibition has also been investigated as rstand second - line treatment of patients with nsclc.15 , 16 we present the results from the expanded nsclc cohort of the vemurafenib basket trial . 
this trial assessed the efcacy of vemurafenib in seven cohorts of patients with braf v600mutated malignancies.17 ( ve - basket ) methods study design the ve - basket study was a multicenter , single - arm , phase ii study of vemurafenib in patients with a variety of nonmelanoma cancers harboring braf v600 mutations . braf v600 mutations were identied by means of mutational analysis assays routinely performed at each participating site . 
six prespecied cohorts were recruited , consisting of patients with nsclc , ovarian cancer , colorectal cancer , cholangiocarcinoma , breast cancer , and multiple myeloma ; all patients with solid tumors other than those mentioned were included in a seventh cohort . 
the design of this study has been described in detail elsewhere.17 this trial was performed in accordance with the provisions of the declaration of helsinki and good clinical practice guidelines . 
all patients provided written informed consent . patients patients were eligible for inclusion in the study if they were 16 years of age or older and had histologically conrmed , measurable ( response evaluation criteria in solid tumors [ recist ] , version 1.1 ) , braf v600 mutation - positive cancers that were refractory to standard therapy or for which standard or curative therapy did not exist or was not considered appropriate by the investigator . 
assessments were performed using computed tomography or magnetic resonance imaging of the chest , abdomen , and pelvis at baseline and then every 8 weeks until disease progression , death , or withdrawal from the study . 
adverse events ( aes ) were graded by the investigators using national cancer institute common terminology criteria for adverse events ( version 4.0 ) until 28 days after discontinuation of study treatment . 
aes of special interest were cutaneous squamous cell carcinoma ( scc ; keratoacanthoma , squamous cell carcinoma of the skin , and bowen disease ) , fatigue ( fatigue and asthenia ) , liver injury ( increased alt , ast , blood alkaline phosphatase , blood bilirubin , and gamma - glutamyltransferase ; hyperbilirubinemia , hepatocellular injury , and cholestatic jaundice ) , and prolonged qt interval . 
patients were assessed for aes at each clinic visit and as necessary throughout the study . outcomes the primary objective of the study was to evaluate the efcacy of vemurafenib in patients with braf v600 mutation - positive cancers . 
the primary end point for the nal analysis in the nsclc cohort was objective response rate ( orr ) , dened as the proportion of patients with an objective response ( complete response [ cr ] or partial response [ pr ] ) conrmed on two consecutive occasions 4 or more weeks apart . 
 vemurafenib in nsclc with braf v600 mutation : the ve - basket study objectives included assessments of clinical benet rate ( dened as the overall proportion of patients with a cr , pr , or stable disease lasting 6 months ) , duration of response , progression - free survival ( pfs ) , overall survival ( os ) , and safety . 
efcacy data were analyzed separately for patients who had received no prior therapy and for those with prior therapies . statistical analysis this was a modied , two - stage simon design study . 
stage i was complete when seven patients with measurable disease were enrolled and had completed a minimum of 8 weeks of treatment , developed progressive disease , prematurely withdrew , or died . 
an additional six or 12 patients could be enrolled , to 13 or 19 patients , depending on the results for stage i ; if two , three , or four of the initial seven patients responded to treatment , an additional 12 patients could be enrolled in stage ii ; if ve or more of the initial seven patients responded to treatment , an additional six patients were recruited . 
recruitment into any cohort / indication could be further expanded up to 70 patients if a response rate was demonstrated in stage ii of that cohort , according to the stopping rules dened in the protocol or a clear clinical benet for patients was observed , as determined by the steering committee . 
for the nsclc cohort , with 50 treated patients , the study would have approximately 90% power for the lower bound of the twosided 95% ci to exclude 20% , given a true orr of 40% . the lower bound of the 95% ci was set at 20% because established therapy in the second and later lines had an orr of less than 20% when the study was designed . 
most patients had adenocarcinoma ( n = 58 ; 94% ) , three patients ( 4.8% ) had cns metastases , and most were former smokers ( n = 36 ; 58% )  . among previously treated patients , the median number of prior systemic regimens was two ( interquartile range [ iqr ] , 1 to 2 ) ; the most common prior chemotherapies were platinum agents ( 39 of 54 patients ; 72% ) , pemetrexed ( 33 of 54 patients ; 61% ) , and taxanes ( 22 of 54 patients ; 41% )  . all patients ( n = 62 ) previously untreated ( n = 8 ) previously treated ( n = 54 ) 65 ( 59 - 74 ) 73 ( 65 - 79 ) 64 ( 57 - 72 ) table 1 . 
overall , the investigator - determined orr was 37% ( 95% ci , 25% to 50% ) , and the clinical benet ( cr plus pr plus stable disease lasting 6 months ) rate was 48% ( 95% ci , 36% to 61% )  . 
the median relative dose intensity achieved was 78% ( iqr , 64% to 91% ) overall . all 62 patients experienced at least one any - cause ae ; grade 3 or 4 aes occurred in 48 patients ( 77% ) , and two patients had grade 5 aes ( 3% ; one patient with sepsis , one with a pulmonary embolism and respiratory failure ; both patients had been previously treated , and none of the events were considered to be related to vemurafenib )  . table 3 lists all - cause and grade 3 or greater aes occurring in 20% or more of patients . aes leading to treatment interruption occurred in 25 of 62 patients ( 40% )  . 
treatment outcomes in patients with nonsmall - cell lung cancer outcome all patients ( n = 62 ) previously untreated ( n = 8 ) previously treated ( n = 54 ) investigator - assessed best response , no . 
 vemurafenib in nsclc with braf v600 mutation : the ve - basket study - 100 previously untreated patients partial response stable disease progressive disease previously treated patients time to progression time to response died alive time ( months ) before treatment after 2 months of treatment fig 1 . 
 ( b ) waterfall plot of maximum percent decrease from baseline in the sum of diameters of target tumors on the basis of investigator assessment : best overall response in individual patients . ( c ) pretherapy and post - therapy 18f - uorodeoxyglucose positron emission tomography images of a chemotherapy - naive patient with braf v600e mutationpositive nsclc . 
at risk previously untreated ( n = 8 ) previously treated ( n = 54 ) overall ( n = 62 ) censored previously untreated ( n = 8 ) previously treated ( n = 54 ) overall ( n = 62 ) censored no . 
at risk 9 12 15 18 21 24 27 30 33 36 39 time ( months ) time ( months ) previously untreated previously treated 54 45 36 29 22 16 12 11 overall 62 52 42 34 26 18 14 12 previously untreated previously treated overall fig 2 . 
a total of 82 serious aes occurred in 39 patients ( 63% ) , the most common of which were scc of the skin ( nine patients ; 15% ) and keratoacanthoma ( nine patients ; 15% ) , which was dened as a serious ae . 
in total , 25 patients ( 40% ) had serious aes considered by the investigator to be caused by vemurafenib ( keratoacanthoma , n = 9 ; scc of the skin , n = 9 ; basal cell carcinoma , n = 1 ; bowen disease , n = 1 ; acute kidney injury , n = 4 ; pericarditis , n = 1 ; stomatitis , n = 1 ; pyrexia , n = 1 ; hypersensitivity , n = 1 ; sepsis , n = 1 ; and dehydration , n = 1 ) ; serious aes not considered to be related to vemurafenib included pneumonia ( n = 2 ) , bronchitis ( n = 2 ) , dyspnea ( n = 3 ) , pericardial effusion ( n = 1 ) , sepsis ( n = 3 ) , pulmonary embolism ( n = 2 ) , and lung infection ( n = 2 )  . targetable oncogenic drivers in nsclc with robust clinical validation include egfr mutations and alk and ros1 fusions , but identifying other targetable , clinically important subgroups of nsclc is a high priority . 
in this context , we found that patients with braf v600emutated nsclc treated with vemurafenib had an orr of 37% , with similar response rates in previously treated and untreated patients . median os was 15 months in the overall patient population , but had not been reached in the group of previously untreated patients after 12 months of follow - up . 
similarly , our previously untreated patients had a median pfs of 12.9 months , which was considerably longer than the 6.5 months observed in patients who had received prior therapies . 
the safety prole of vemurafenib in our group of patients with nsclc was similar to that seen in patients with melanoma.10 , 18 no new safety signals were observed in this population . 
we suggest that future studies should examine additional combinations in patients with braf mutation - positive nsclc . in conclusion , the results of the present cohort analysis suggest a role for braf inhibition in patients with nsclc with braf mutations . 
 vemurafenib in nsclc with braf v600 mutation : the ve - basket study affiliations 1university of texas md anderson cancer center , houston , tx 2centre franois baclesse , caen , france 3memorial sloan kettering cancer center , new york , ny 4institut gustave roussy , villejuif , france 5centre l eon b erard , lyon , france 6vall dhebron university hospital and vall dhebron institute of oncology , barcelona , spain 7university hospital essen , essen , germany 8aix - marseille universit e , marseille , france 9institut bergonie , bordeaux , france 10vanderbilt university , nashville , tn 11the royal marsden nhs foundation trust , london , united kingdom 12roswell park cancer institute , buffalo , ny 13massachusetts general hospital , boston , ma 14f . 
hyman administrative support : vivek subbiah provision of study materials or patients : vivek subbiah , gregory riely , antoine hollebecque , jean - yves blay , enriqueta felip , martin schuler , anthony gonalves , antonio italiano , igor puzanov , funda meric - bernstam collection and assembly of data : vivek subbiah , radj gervais , gregory riely , antoine hollebecque , jean - yves blay , martin schuler , antonio italiano , vicki keedy , igor puzanov , funda meric - bernstam , martina makrutzki , todd riehl , david m . 
hyman data analysis and interpretation : vivek subbiah , radj gervais , antoine hollebecque , jean - yves blay , enriqueta felip , martin schuler , anthony gonalves , antonio italiano , vicki keedy , ian chau , igor puzanov , noopur s . 
raje consulting or advisory role : amgen , celgene , takeda , novartis , bristolmyers squibb , merck , janssen oncology research funding : astrazeneca ( inst ) funda meric - bernstam honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group , mersana research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pzer , effector therapeutics , abbvie , boehringer ingelheim ( i ) , guardant health ( inst ) , daiichi sankyo , glaxosmithkline martina makrutzki employment : roche todd riehl employment : genentech stock and other ownership interests : genentech bethany pitcher employment : hoffmann - la roche jose baselga leadership : innity pharmaceuticals , varian medical systems , bristolmyers squibb , foghorn stock and other ownership interests : pmv pharma , juno therapeutics , grail , tango , venthera , northern biologics , apogen biotechnologies , aura biosciences consulting or advisory role : novartis patents , royalties , other intellectual property : combination therapy using pdk1 and pi3k inhibitors , use of phosphoinositide 3 - kinase inhibitors for treatment of vascular malformations , inhibition of kmt2d for the treatment of cancer travel , accommodations , expenses : roche , daiichi sankyo david m . 
n engl j med 361 : 947 - 957 , 2009 solomon bj , mok t , kim d - w , et al : first - line crizotinib versus chemotherapy in alk - positive lung cancer . 
n engl j med 371 : 1963 - 1971 , 2014 thomas a , liu sv , subramaniam ds , et al : rening the treatment of nsclc according to histological and molecular subtypes . 
medicine ( baltimore ) 96 : e6552 , 2017 paik pk , arcila me , fara m , et al : clinical characteristics of patients with lung adenocarcinomas harboring braf mutations . 
mcarthur ga , chapman pb , robert c , et al : safety and efcacy of vemurafenib in braf ( v600e ) and braf ( v600k ) mutation - positive melanoma ( brim - 3 ) : extended follow - up of a phase 3 , randomised , open - label study . 
long gv , stroyakovskiy d , gogas h , et al : dabrafenib and trametinib versus dabrafenib and placebo for val600 braf - mutant melanoma : a multicentre , double - blind , phase 3 randomised controlled trial . 
ascierto pa , mcarthur ga , dr eno b , et al : cobimetinib combined with vemurafenib in advanced braf ( v600 ) - mutant melanoma ( cobrim ) : updated efcacy results from a randomised , double - blind , phase 3 trial . 
planchard d , kim tm , mazieres j , et al : dabrafenib in patients with braf ( v600e ) - positive advanced non - small - cell lung cancer : a single - arm , multicentre , open - label , phase 2 trial . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated brafv600e - mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
planchard d , smit ef , groen hjm , et al : dabrafenib plus trametinib in patients with previously untreated brafv600e - mutant metastatic non - small - cell lung cancer : an open - label , phase 2 trial . 
reis - filho , md , phd1 ; diana mandelker , md , phd1 ; and britta weigelt , phd1 purpose endometrial cancer ( ec ) is not considered a component of the hereditary breast and ovarian cancer syndrome but can arise in patients with germline brca1 / 2 ( gbrca1 / 2 ) mutations . 
we sought to determine if ecs in gbrca1 / 2 mutation carriers harbor biallelic alterations and / or features of hrd . methods of 769 patients with ec who underwent germline panel testing , 10 pathogenic gbrca1 / 2 mutation carriers were identied , and their tumorand normal - derived dna was subjected to massively parallel sequencing targeting at least 410 cancer - related genes . 
somatic mutations , copy number alterations , loss of heterozygosity , microsatellite instability ( msi ) , and genomic hrd features were assessed . results of the 13 patients included who had ec , eight harbored pathogenic gbrca1 mutations and ve harbored gbrca2 mutations . 
 smith et al context key objective to determine if endometrial cancers ( ecs ) that arise in patients with pathogenic brca1 or brca2 germline mutations are sporadic cancers or display genomic features of homologous recombination dna repair deciency ( hrd ) , which may guide treatment strategies . knowledge generated ecs in patients with brca1 germline mutations showed biallelic brca1 alterations coupled with genomic features of hrd . 
in contrast , only a subset of ecs in brca2 germline mutation carriers harbored biallelic brca2 alterations ; the remaining cases were likely sporadic cancers . relevance knowledge about the brca1 / 2 allele status and / or hrd features of ecs in patients with germline brca1 / 2 alterations may guide therapeutic decision making , given that tumors with biallelic alterations in brca1 / 2 have been associated with increased response to hr - targeted therapies such as platinum salts and parp inhibitors . brca1 / 2 alterations and show features of hr deciency , including the catalog of somatic mutations in cancer mutational signature 3 , signature multivariate analysis ( sigma ) hr deciency signature sig3 , or large - scale chromosomal breaks in the form of large - scale state transitions ( lsts )  . 
in addition , we assessed the clinicopathologic data of ecs in gbrca1 / 2 mutation carriers and explored the repertoire of somatic mutations present in these tumors . methods case selection all patients with ec and gbrca1 / 2 mutations who consented to germline analysis under an institutional review boardapproved protocol at memorial sloan kettering cancer center and whose tumors were subjected to targeted massively parallel sequencing via memorial sloan ketteringintegrated mutation proling of actionable cancer targets ( msk - impact ) 10 , 11 from july 2015 to may 2019 were identied ( n = 769 sequenced ; n = 10 with pathogenic gbrca1 / 2 mutation )  . 
all gbrca1 / 2 variants were reviewed by a board - certied molecular pathologist ( d.m. ) and classied according to the american college of medical genetics and genomics criteria12 as pathogenic . clinicopathologic data , including age at diagnosis , cancer stage , and past cancer history , were obtained from medical records . 
mlh1 promoter methylation was assessed in the clinical setting on dna obtained from formalin - xed parafn - embedded tumor samples , as previously described.28 statistical analyses fishers exact and mann - whitney u tests were used for comparison of categorical and continuous variables , respectively . 
two - tailed p , 0.05 was considered statistically signicant . results clinicopathologic features of ecs arising in gbrca1 / 2 carriers ten ecs from patients with pathogenic gbrca1 / 2 mutations subjected to msk - impact sequencing ( n = 769 ecs ; 1.3% ) and three subjected to wes by tcga ( n = 232 ecs ; 1.3% ) 13 were included in this study . 
of these 13 gbrca1 / 2associated ecs , eight and ve patients with ec harbored gbrca1 and germline brca2 ( gbrca2 ) mutations , respectively ( table 1 )  . 
the majority of gbrca1 / 2 - associated ecs ( n = 6 of 8 ; 75% ) displayed an endometrioid histology ( n = 2 and 4 international federation of gynecology and obstetrics [ figo ] grades ii and iii , respectively ) but lacked a solid / pseudoendometrioid / transitional cell - like pattern of morphology , which has been associated with gbrca1 / 2 mutations in high - grade serous ovarian cancers.29 , 30 in contrast , ecs from patients with pathogenic gbrca2 mutations were more heterogeneous at the phenotypic level , and included endometrioid ( n = 1 ; figo grade ii ) , carcinosarcoma ( n = 2 ) , high - grade ec not otherwise specied ( nos ; n = 1 ) and serous ( n = 1 ) cancers ( tables 1 and 2 )  . 
of note , none of the gbrca1 / 2 - associated ecs included in this study were of serous histology . gbrca1 / 2 - associated ecs presented at different clinical figo stages ( 2009 staging system31 )  . 
taken together , our data suggest the clinicopathologic features associated with ecs occurring in patients with pathogenic gbrca1 or gbrca2 mutations may be heterogeneous . biallelic brca1 / 2 alterations allele - specic copy number analysis revealed that 77% ( n = 10 of 13 ) of the ecs in patients with pathogenic gbrca1 / 2 mutations displayed biallelic inactivation of brca1 / 2 uniformly through loh of the wild - type allele ( table 2 ; fig 1 )  . 
not all ecs occurring in pathogenic gbrca1 / 2 mutation carriers harbored biallelic brca1 / 2 alterations , which have previously been associated with hr deciency.8 although all ecs in pathogenic gbrca1 mutation carriers ( 100% ) harbored biallelic brca1 inactivation , only two of the ve ecs ( 40% ) from patients with pathogenic gbrca2 mutations displayed biallelic brca2 inactivation ( table 2 ; fig 1 )  . biallelic brca1 / 2 inactivation was found across all histologic subtypes and clinical stages of ec . 
ecs in brca2 mutation carriers lacking loh of the wild - type allele are likely sporadic tumors ; all three were stage iii at diagnosis and were endometrioid grade ii , serous , or high - grade ecs ( table 2 ; fig 1 )  . 
 ( % ) unless otherwise indicated . abbreviations : msk - impact , memorial sloan ketteringintegrated mutation proling of actionable cancer targets ; nos , not otherwise specied ; tcga , the cancer genome atlas ; wes , whole - exome sequencing . * fishers exact and mann - whitney u tests were used for comparison of categorical and continuous variables , respectively . staging information was performed according to the international federation of gynecology and obstetrics system.31 past cancer histories and information regarding radiation exposure were available for the 10 msk - impact cases and reect cancers diagnosed and treated prior to the diagnosis of ec . 13 gbrca1 / 2 - associated ecs was six ( range , 2 to 38 ) , with a median of ve ( range , 2 to 32 ) nonsynonymous mutations ( data supplement )  . 
we observed that all ecs analyzed , irrespective of the presence of monoor biallelic brca1 / 2 alterations , harbored somatic tp53 mutations , of which 12 ( 92% ) were hotspot mutations ( fig 1 ; data supplement )  . 
alterations affecting the pi3k pathway were 4 2019 by american society of clinical oncology common , with pik3ca mutations present in ve ecs ( 38% ) , pik3r1 mutations in two ecs ( 15% ) , and pten mutations / homozygous deletions in three ecs ( 23% ; figs 1 and 2 )  . 
other recurrently altered genes included fat1 , ptch1 , kras , and map3k1 ( each n = 2 ; fig 1 , data supplement )  . we noted that bec - 1 , a likely sporadic ec from a gbrca2 mutation carrier with a monoallelic brca2 alteration , had a high mutational burden with 32 nonsynonymous somatic mutations . 
the ecs with very low levels of gene cnas ( ie , bec - 1 , bec - 6 , and bec - 12 ) had monoallelic brca2 alterations and were likely sporadic , with one ( bec - 1 ) being msi high , as mentioned . 
in addition , we found an nf1 homozygous deletion in the biallelic brca1 grade ii endometrioid tcga - 2 and a smarca4 homozygous deletion in the biallelic brca2 carcinosarcoma bec - 2 . 
of note , smarca4 ( brg1 ) loss is commonly found in unthe endometrium , 32 , 33 and differentiated carcinoma of bec - 2 was a carcinosarcoma with heterologous elements , which , in addition to the carcinoma and sarcomatous components , also displayed an undifferentiated component . 
finally , amplication of bcl6 , tp63 , and eed was found in the biallelic brca1 grade iii endometrioid tcga - 1 ec ( fig 2 )  . taken together , we found that ecs in patients with a gbrca1 / 2 mutation are heterogeneous at the mutational and gene copy number levels . 
we observed that ecs with biallelic brca1 / 2 alterations ( n = 10 ) had high lst scores , whereas ecs with monoallelic brca1 / 2 alterations did not ( table 2 ; fig 3a )  . 
nonsynonymous somatic mutations identied in 410 cancer - related cancer genes in ecs from germline brca1 ( n = 8 ) and germline brca2 ( n = 5 ) mutation carriers ( left ) are shown . the mutation types are color coded according to the legend . 
information on the germline mutation status , somatic loss of heterozygosity of brca1 / 2 , histologic type , microsatellite instability ( msi ) status , and sequencing type is provided in the phenobar below the sample names . 
tcga , the cancer genome atlas . with hr deciency ( fig 3b ) .14 given the limited number of snvs and indels in the ecs subjected to msk - impact sequencing , other genomic hr - deciency features such as indel length , microhomology , or mutational signatures using decomposition algorithms could not be used . therefore , we used sigma , a recently described , likelihoodbased measure signature analysis combined with machinelearning techniques , which can be used to detect the mutational signature sig3 associated with hr deciency from targeted gene panels including msk - impact ( sensitivity range , 48% to 62% for uterine cancers ) .25 consistent with the lst analysis , all six biallelic , brca1 / 2associated ecs subjected to msk - impact and with at least ve snvs displayed either a dominant hr deciency - related sig3 ( n = 2 ) or a dominant clock signature with secondary hr - deciency signatures sig3 ( n = 3 ) or sig834 ( n = 1 ) , to the two sporadic ecs with monoallelic in contrast brca2 alterations , which displayed msi ( sigma ) / signature 6 ( deconstructsigs ) and apobec signatures ( table 2 ; fig 3c )  . 
previous reports of ecs in this population have acknowledged that the prevalence of ec in gbrca1 / 2 mutation carriers is low.5 here , through an in - depth analysis of ecs from patients with pathogenic gbrca1 / 2 mutations , we demonstrate that the majority of these cases ( 77% ) harbored biallelic brca1 / 2 alterations and displayed genomic features of hrd , providing evidence to suggest an etiological link between the pathogenic gbrca1 / 2 mutations and the development of these ecs . 
in fact , this phenomenon was uniformly observed in patients with pathogenic gbrca1 mutations ; conversely , only two of the ve patients with pathogenic gbrca2 mutations had somatic inactivation of the brca2 wild - type allele and genomics features of hr deciency . 
in ovarian cancer , patients with hr - decient tumors have improved overall survival with platinum - based therapy and have better responses to hr deciencydirected treatments such as parp inhibitors than their wild - type counterparts.35 , 36 knowledge of the allele status of brca1 / 2 alterations and / or hr - deciency features could be benecial in therapeutic decision making for patients with gbrca1 / 2 mutations and ec . 
our analysis has demonstrated that not all ecs arising in the context of pathogenic gbrca2 mutations harbor loh of the wild - type allele and genomics features of hr deciency . 
in addition , it revealed that one of these cases was msi high , likely representing a sporadic ( ie , non - brca1 / 2 ) ec arising in a gbrca2 mutation carrier . 
in this context , this patient would potentially benet from immune checkpoint inhibitors , which have been approved for the management of recurrent msi - high / dna mmrdecient cancers.37 in fact , a recent case report highlighted a complete remission after pd - 1 blockade in a patient with mmr - decient ec and a pathogenic monoallelic gbrca1 mutation.38 the majority ( 75% ) of biallelic gbrca1 / 2 - associated ecs were of intermediate / high - grade endometrioid as opposed to serous histology in previous reports.5 , 6 all six biallelic gbrca1 / 2 - associated endometrioid ecs harbored tp53 mutations , had high lst scores , and relatively high levels of cnas ( table 2 ; fig 2 ) , and would likely be of copy - number high ( serous - like ) molecular subtype , as described by tcga.13 it should be noted , however , that of these six endometrioid ecs with biallelic brca1 alterations , four harbored somatic mutations characteristic of endometrioid ecs , including pik3ca mutations , pik3r1 mutations , and pten mutations / homozygous deletions . 
conversely , two of these ecs lacked alterations affecting genes recurrently altered in endometrioid ecs ( fig 1 ) , suggesting that at the these latter two cases resembled serous genetic level , rather than endometrioid carcinomas , and that there is heterogeneity in gbrca1 / 2 - associated ecs . 
carcinosarcomas of the uterus are rare , representing less than 5% of all uterine tumors.39 we noted a high frequency ( 30% ) of carcinosarcomas in the 10 gbrca1 / 2 - associated ecs subjected to msk - impact sequencing , whereas overall , only 10% of the 769 ecs subjected to germline mskimpact sequencing were carcinosarcomas ( remaining cases : 55% endometrioid , 15% serous , 10% endometrial cancer nos , 4% mixed endometrial , 3% clear cell , 1% deor undifferentiated , and 1% other )  . 
interestingly , recurrent somatic brca1 / 2 mutations and brca2 deletions also have been reported in uterine carcinosarcomas.40 - 42 these ndings suggest that ecs arising in gbrca1 / 2 mutation carriers are heterogeneous at the histologic level and are potentially enriched for endometrioid tumors and carcinosarcomas . the data presented here do provide insight into the genomics of ecs in patients with pathogenic gbrca1 / 2 mutations , which may play a role in the tumorigenesis and / or progression of ec in some patients . 
this study has several limitations , however , primarily driven by the small sample size , and it does not resolve the controversy of ec as a feature of hboc syndrome . 
the low incidence of these cases ( 1.3% ; n = 10 of 769 ecs subjected to germline mskimpact testing ) not only limits the sample size of this study but also , on its own , presents a challenge in dening ec as part of the hboc syndrome spectrum of malignancies . 
 brca1 / 2 endometrial cancer lsts mutational signatures ( decontructsigs ) signature 1 ( aging ) signature 3 ( hr defect ) signature 15 ( mmr defect ) signature 19 signature 20 ( mmr defect ) signature 24 signature 25 unknown tcga - 1 tcga - 2 tcga - 3 mlh1 biallelic brca1 / 2 ( n = 10 ) monoallelic brca2 ( n = 3 ) pms2 msh2 msh6 signature 1 aging signature 6 mmr defect signature 21 mmr defect unknown mutational signatures bec - 1 fig 3 . 
 ( a ) large - scale state transition ( lst ) scores in germline ( gbrca1 / 2 ) - associated endometrial cancers with biallelic ( n = 10 ) and monoallelic ( n = 3 ) brca1 / 2 alterations . 
 ( b ) mutational signatures dened by deconstructsigs24 in three gbrca1 / 2 - associated endometrial cancers from the cancer genome atlas ( tcga ) subjected to whole - exome sequencing.13 , 14 mutational signatures are color coded according to the legend on the right . 
 ( c ) immunohistochemical analysis of the ( left ) dna mismatch repair ( mmr ) proteins mlh1 , pms2 , msh2 , and msh6 and ( right ) mutational signatures of case bec - 1 , a monoallelic / sporadic gbrca1 / 2 - associated endometrial cancer . 
bec - 1 shows loss of mlh1 and pms2 expression , mlh1 promoter hypermethylation ( not shown ) , and dominant mutational signatures 6 and 21 associated with defective dna mmr . mutations in patients with ec nor the impact of these mutations on the outcome of patients with ec could be fully dened . 
although we have assessed the genomics features of hr deciency , including lsts and sigma hr deciency signature sig3 in all cases , hr deciency is more accurately assessed with whole - genome sequencing.43 hence , additional studies testing ecs developing in the context of pathogenic gbrca1 / 2 mutations but lacking loss of the wildtype allele by whole - genome sequencing are warranted . despite these limitations , here we demonstrate the importance of germline and somatic genetic characterization of ecs . 
in fact , ecs developing in the context of pathogenic gbrca1 / 2 mutations may harbor genomics features of hr deciency and be causally linked to the loss of function of these tumor suppressor genes . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . nadeem riaz honoraria : peerview speakers bureau : illumina research funding : bristol - myers squibb , pzer travel , accommodations , expenses : varian medical systems mark e . 
robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca , pzer other relationship : research to practice , clinical care options , physician education resource robert a . 
assignee : 2015 the regents of the university of california 8 / 18 / 2015 ( inst ) ; application : compositions and methods for the diagnosis and treatment of ovarian cancers that are associated with reduced smarca4 gene expression or protein function ( inst ) ; royalties from published books : cambridge university press and springer publishing jorge s . 
reis - filho consulting or advisory role : roche , invicro , ventana medical systems , volition rx , paige.ai , goldman sachs , novartis britta weigelt consulting or advisory role : roche ( i ) , invicro ( i ) , ventana medical systems ( i ) , volition rx ( i ) , paige.ai ( i ) , goldman sachs ( i ) , novartis ( i ) no other potential conicts of interest were reported . acknowlegement we thank the members of the molecular diagnostics service in the department of pathology , memorial sloan kettering cancer center . references gudmundsdottir k , ashworth a : the roles of brca1 and brca2 and associated proteins in the maintenance of genomic stability . 
oncogene 25 : 5864 - 5874 , 2006 king mc , marks jh , mandell jb : breast and ovarian cancer risks due to inherited mutations in brca1 and brca2 . 
nat rev clin oncol 13 : 41 - 54 , 2016 segev y , iqbal j , lubinski j , et al : the incidence of endometrial cancer in women with brca1 and brca2 mutations : an international prospective cohort study . gynecol oncol 130 : 127 - 131 , 2013 shu ca , pike mc , jotwani ar , et al : uterine cancer after risk - reducing salpingo - oophorectomy without hysterectomy in women with brca mutations . 
jama oncol 2 : 1434 - 1440 , 2016 pennington kp , walsh t , lee m , et al : brca1 , tp53 , and chek2 germline mutations in uterine serous carcinoma . 
cell 173 : 355 - 370.e14 , 2018 riaz n , blecua p , lim rs , et al : pan - cancer analysis of bi - allelic alterations in homologous recombination dna repair genes . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
ashley cw , da cruz paula a , kumar r , et al : analysis of mutational signatures in primary and metastatic endometrial cancer reveals distinct patterns of dna repair defects and shifts during tumor progression . 
geyer fc , li a , papanastasiou ad , et al : recurrent hotspot mutations in hras q61 and pi3k - akt pathway genes as drivers of breast adenomyoepitheliomas . nat commun 9 : 1816 , 2018 e131 , 2016 17 . 
karnezis an , hoang ln , coatham m , et al : loss of switch / sucrose non - fermenting complex protein expression is associated with dedifferentiation in endometrial carcinomas . 
ramalingam p , croce s , mccluggage wg : loss of expression of smarca4 ( brg1 ) , smarca2 ( brm ) and smarcb1 ( ini1 ) in undifferentiated carcinoma of the endometrium is not uncommon and is not always associated with rhabdoid morphology . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
dizon ds , dias - santagata d , bregar a , et al : complete remission following pembrolizumab in a woman with mismatch repair - decient endometrial cancer and a germline brca1 mutation . 
gynecol oncol 137 : 581 - 588 , 2015 jones s , stransky n , mccord cl , et al : genomic analyses of gynaecologic carcinosarcomas reveal frequent mutations in chromatin remodelling genes . 
zhao s , bellone s , lopez s , et al : mutational landscape of uterine and ovarian carcinosarcomas implicates histone genes in epithelial - mesenchymal transition . proc natl acad sci usa 113 : 12238 - 12243 , 2016 jones nl , xiu j , chatterjee - paer s , et al : distinct molecular landscapes between endometrioid and nonendometrioid uterine carcinomas . 
 c circulating cell - free tumor dna in the management of double primary tumors introduction synchronous lung and colorectal cancer ( crc ) occurrence in one individual is a rare event.1 - 3 the genomics of both malignancies have been extensively studied and found to be distinct . 
 broad molecular profiling in advanced non small - cell lung cancer is widely accepted and routinely used in selecting targeted therapy , because response rates ( rrs ) to single targeted agents are twoto three - fold higher than those to cytotoxic chemotherapy.4 - 11 in advanced crc , potentially targeted alterations are mostly detected in the braf gene ; however , the rr in crc is typically worse than in nonsmall - cell lung cancer ( rr range in crc , 10% to 15% )  . 
 in addition , in crc , expanded testing of the kras and nras genes is used as a negative predictor of antiepidermal growth factor receptor ( egfr ) antibody treatment.12 circulating cell - free tumor dna ( ctdna ) sequencing is a blood - based test , also known as liquid biopsy , which is currently widely used for tumor genomic profiling.13 in contrast to tissue biopsy , ctdna sequencing is a noninvasive approach and thus especially valuable where the tumor tissue obtained is insufficient for molecular testing . 
most importantly , liquid biopsy may provide a global summary of intraand intertumor heterogeneity.14 guardant 360 ( guardant health , redwood city , ca ) is a liquid biopsy test based on digital sequencing technology . 
 the clinical sensitivity and specificity of this test are comparable to those of tissue - based next - generation sequencing ( ngs ; analytic specificity of > 99.9999% at the per - nucleotide level ) .15 absolute variant allele fractions , including egfr and braf single - nucleotide variants , have been shown to tightly correlate with a well - validated orthogonal digital droplet polymerase chain reactionbased plasma analysis.16 we present a case of a patient with synchronous lung and colorectal cancers driven by two different oncogenic drivers ( egfr l858r and braf v600e for the lung and colorectal tumors , respectively )  . 
whereas the incidence of the abovementioned molecular aberrations in these tumor types ranges from 10% to 20% , 17 - 19 it is rare to discover both in the same individual . 
biopsy of the colonic mass confirmed a cdx2 - positive adenocarcinoma compatible with primary colonic orig positron emission tomographycomputed tomography scan showed the abovementioned tumor in the right colon and also demonstrated metastatic disease in the bones and a speculated right upper lobe ( rul ) lesion with an atelectatic component compatible with a second primary lung tumor ( fig 1a )  . 
a biopsy of both the rul lesion and the t9 lytic mass confirmed the diagnosis of metastatic lung adenocarcinoma in both tumor specimens ; tumor cells were positive for ttf1 and ck7 and negative for cdx2 and ck20 . because the rul lesion and the vertebral metastasis had insufficient tumor tissue for elizabeth dudnik tal twito iris faull addie dvir lior soussan - gutman ofer purim richard b . 
 ( a ) positron emission tomographycomputed tomography scan demonstrating metastatic disease in the spiculated right upper lobe ( rul ) lesion with an atelectatic component compatible with a second primary lung tumor . 
targeted ngs of the ctdna identified two driver mutations : egfr l858r at 2.4% mutant allele fraction ( maf ) and braf v600e mutation at 0.9% maf ( fig 2a )  . 
after the ctdna analysis , the tumor specimen obtained from the bone lesion was reviewed , and polymerase chain reaction analysis for egfr ( amoydx egfr 29 mutations detection ce - ivd kit ; xiamen , peoples republic of china ) was performed , confirming the presence of egfr l858r mutation in the bone metastasis . 
the origin of the braf v600e clone at that point remained unclear . when the patient was about to start treatment with anti - egfr therapy , she was diagnosed with acute large - bowel obstruction and underwent extended right hemicolectomy , which revealed moderately differentiated colonic adenocarcinoma infiltrating the pericolic fat with three involved regional lymph nodes and positive surgical margins ( pt3n2r1 )  . 
soon thereafter , the patient developed a large pericardial effusion , and pericardial window was performed , revealing no viable tumor in the pericardial tissue specimen . erlotinib was initiated , resulting in a significant shrinkage of the rul mass ; however , new liver metastases developed ( fig 1b )  . 
this time , braf testing as well as kras and nras testing was performed ( amoydx ce - ivd kit ) , revealing that the tumor was kras wild type and nras wild type and harbored a braf v600e mutation . after the diagnosis of metastatic crc , in march 2016 , capecitabine was added to erlotinib . 
although not known as driver mutations , these mutations are more common in crc than in lung cancer , and their mafs increased from the initial test to that performed after the patient received egfr inhibitors ( fig 2b )  . after the second ctdna testing , the treatment was switched to a combination of vemurafenib and erlotinib.20 - 22 however , the treatment was poorly tolerated ( severe diarrhea ) and was therefore discontinued after 1 month . 
previous genetic studies of crc have identified somatic mutations in four main candidate pathways : tgf - , wnt , p53 , and rtk - ras , all of which were identified as important contributors to crc development.29 among them , mutations in the smad4 , apc , fbxw7 , and braf genes were identified as recurrent mutations in patients with crc.29 - 31 in contrast , apc was suggested to be a gatekeeper , which regulates epithelial cells to develop into adenoma and even carcinoma cells.32 notably , not only did liquid biopsy detect both tumor driver mutations at the time of initial diagnosis , it also reflected the progression of the second primary colon tumor , early in the course of the disease , even before its growth was shown in imaging . 
a rise in the maf of braf v600e , a driver mutation , as well as other crc - associated mutations ( smad4 , apc , fbxw7 ) , alongside a drop in the maf of the egfr l858r mutation , suggested that the new retroperitoneal lesions were related to the crc . 
this finding is consistent with other reports showing how ctdna allele fractions serve as early indicators of response versus progression in earlyand late - stage crc.33 , 34 later on , liquid biopsy allowed simultaneous response monitoring of both tumors . 
however , it should be emphasized that for clinical application of monitoring with serial testing , the assay used must be validated not only for detecting mutations but also for accurate quantitation of variant allele fractions . 
our patient did not benefit from the braf inhibitor , possibly because single - agent braf inhibitor yields poor results in patients with crc with braf mutations.12 therefore , inhibition of multiple pathways and immunotherapy should have been considered.35 although tumor mutational burden was not assessed here , analysis of blood - derived ctdna demonstrated high mutation in november 2015 as well as in june 2016 ( fig 2 )  . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . elizabeth dudnik consulting or advisory role : boehringer ingelheim speakers bureau : boehringer ingelheim , roche , astrazeneca , pfizer , merck sharp & dohme , bristol - myers squibb , novartis research funding : boehringer ingelheim ofer purim no relationship to disclose richard b . 
lanman employment : guardant health , veracyte leadership : guardant health , biolase stock and other ownership interests : guardant health , biolase research funding : guardant health affiliations elizabeth dudnik and ofer purim , davidoff cancer center , rabin medical center , petach tikva ; tal twito , addie dvir , and lior soussan - gutman , teva pharmaceuticals industries , shoam , israel ; and iris faull and richard b . 
yun hr , yi lj , cho yk , et al : double primary malignancy in colorectal cancer patients : msi is the useful marker for predicting double primary tumors . 
chiang jm , yeh cy , changehien cr , et al : clinical features of second other - site primary cancers among sporadic colorectal cancer patients : a hospital - based study of 3 , 722 cases . 
zhou c , wu yl , chen g , et al : erlotinib versus chemotherapy as first - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
sequist lv , yang jc , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
mazires j , barlesi f , filleron t , et al : lung cancer patients with her2 mutations treated with chemotherapy and her2 - targeted drugs : results from the european euher2 cohort . 
paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
sarfaty m , moore a , neiman v , et al : ret fusion lung carcinoma : response to therapy and clinical features in a case series of 14 patients . 
prez - callejo d , romero a , provencio m , et al : liquid biopsy based biomarkers in non - small cell lung cancer for diagnosis and treatment monitoring . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
ulrich bc , nagy rj , odegaard ji , et al : cross - platform detection and quantification of actionable mutations in cell - free dna shows high concordance and correlation between next - generation sequencing and droplet digital pcr . 
pao w , miller va : epidermal growth factor receptor mutations , small - molecule kinase inhibitors , and non - small - cell lung cancer : current knowledge and future directions . 
sanz - garcia e , martinez am , elez e , et al : survival determinants with matched targeted therapies in braf mutant metastatic colorectal cancer ( mcrc )  . 
barlesi f , mazieres j , merlio jp , et al : routine molecular profiling of patients with advanced nonsmall - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
ohashi k , sequist lv , arcila me , et al : lung cancers with acquired resistance to egfr inhibitors occasionally harbor braf gene mutations but lack mutations in kras , nras , or mek1 . 
blakely cm , watkins tbk , wu w , et al : evolution and clinical impact of co - occurring genetic alterations in advanced - stage egfr - mutant lung cancers . 
kim st , lee ws , lanman rb , et al : prospective blinded study of somatic mutation detection in cell - free dna utilizing a targeted 54 - gene next generation sequencing panel in metastatic solid tumor patients . 
tie j , wang y , tomasetti c , et al : circulating tumor dna analysis detects minimal residual disease and predicts recurrence in patients with stage ii colon cancer . 
 role for nucleotide excision repair gene variants in oxaliplatin - induced peripheral neuropathy purpose oxaliplatin forms part of routine treatment of advanced colorectal cancer ; however , it often causes severe peripheral neuropathy , resulting in treatment discontinuation . 
we sought to determine the molecular and cellular mechanism underlying this toxicity . patients and methods we exome resequenced blood dna samples from nine patients with advanced colorectal cancer who had severe peripheral neuropathy associated with oxaliplatin ( pnao ) within 12 weeks of treatment . 
we tested the functionality of ercc4 variants using viability and dna repair assays in schizosaccharomyces pombe and human cell lines after exposure to oxaliplatin and ultraviolet light . results exome resequencing identified one patient carrying a novel germline truncating mutation in the nucleotide excision repair ( ner ) gene ercc4 . 
we subsequently found that multiple rare ercc4 nonsynonymous variants were over - represented in affected individuals ( p = 7.7 103 ) and three of these were defective in the repair of ultraviolet lightinduced dna damage ( p < 1 103 )  . 
2018 by american society of clinical oncology introduction oxaliplatin , a third - generation platinum drug , in combination with fluorouracil and leucovorin or oral capecitabine is standard treatment of locally advanced and metastatic colorectal cancer ( crc ) ; it improves both response and progression - free survival.1 , 2 it also improves disease - free survival in the adjuvant treatment of patients with stage ii and iii colon cancer.3 in addition , oxaliplatin is widely used to treat other gi malignancies . 
platinum agents exert their effects by forming interand intrastrand dna cross - links , 4 which stall the cell cycle , inhibit dna synthesis , 5 and trigger apoptosis.6 oxaliplatin also induces oxidative dna damage.7 peripheral neuropathy is a well - recognized dose limiting toxicity of oxaliplatin.8 , 9 high cumulative doses of oxaliplatin are associated with chronic peripheral nerve damage causing sensory ataxia and functional impairment.10 chronic sensory neuropathy has been observed in approximately half of patients who received oxaliplatin with infusional fluorouracil and leucovorin.11 importantly , it is neurotoxicity , rather than tumor progression , that is often the cause of treatment discontinuation.12 because neurotoxicity is not correlated with response , 12 it is considered a potentially avoidable adverse effect . 
cheadle author affiliations and support information ( if applicable ) appear at the end of this article . none of the sponsors played a role in the study design or in the collection , analysis , and interpretation of the data . corresponding author : jeremy p . 
 although numerous genetic associations with peripheral neuropathy have been proposed ( gstp1 , 16 - 19 agxt , 20 ercc1 , 21 , 22 fars2 , 22 tac1 , 22 scn10a , 23 scn4a , 23 vac14 , 24 and several genome - wide associated loci25 , 26 ) , none have been independently validated and introduced into patient stratification . 
patients with grade 3 or 4 peripheral neuropathy or who had had an oxaliplatin dose reduction as a result of severe peripheral neuropathy were classified as suffering from peripheral neuropathy associated with oxaliplatin ( pnao )  . 
patients with grade 2 peripheral neuropathy were excluded to allow a better discrimination between the two patient groups . molecular analyses we excluded known inherited neuropathies by carrying out multiplex ligation - dependent probe amplification analysis of pmp22 ( approximately 75% of patients with charcot - marie - tooth syndrome , the most common form of inherited neuropathy , have a 1.4 - mb duplication ) and by examining the exome resequencing data for pmp22 and 65 other genes associated with rare inherited neuropathies ( appendix )  . library fragments containing exomic dna were collected using the roche nimblegen seqcap ez exome library ( roche , basel , switzerland ) solution - based method . 
on average , across the exome , we had 55% ( range , 46% to 60% ) coverage of the open reading frame ( orf ) at 20 - fold depth . 
fastq files were processed through a sequence analysis pipeline using burrows - wheeler aligner software for sequence alignment and modules from the broad institutes genome analysis toolkit ( cambridge , ma ) to recalibrate quality scores , refine alignments around potential insertions or deletions ( indels ) , eliminate duplicate reads , call indel and single nucleotide polymorphism ( snp ) genotypes , generate quality control metrics , and apply quality filters to the genotype calls . 
ercc4 and ercc6 nonsynonymous variants were genotyped using kaspar ( lgc , teddington , united kingdom ) or beadarray ( illumina ) technologies ( appendix )  . functional analyses production of a schizosaccharomyces pombe rad16 base strain and the rad16 wild - type vector , cre recombinase - mediated cassette exchange , transformation of the base strain , site - directed mutagenesis , and treatment with oxaliplatin and ultraviolet light were carried out as described in the appendix . 
four hundred eighty epsteinbarr virustransformed human lymphoblastoid cell lines established from healthy white individuals ( european collection of authenticated cell cultures , salisbury , united kingdom ) were assayed for the ercc4 variants pro379ser , arg576thr , and glu875gly using kaspar . 
pombe were normalized to wild type and analyzed using spss v.23 ( spss , chicago , il ) analysis of variance ( anova ) with dunnett correction ( after transformation using the arcsine function )  . 
linkage disequilibrium was obtained using haploview v.4.2 ( broad institute )  . results of the 2 , 445 patients with advanced crc in the coin trial , 23% of patients who received oxaliplatin and fluorouracilbased therapy and 16% of patients who received oxaliplatin and capecitabinebased therapy had severe ( grade 3 ) peripheral neuropathy over the course of the trial.27 we focused on patients with severe pnao within the first 12 weeks of treatment ( appendix and table 1 ) as a potentially enriched group for causal germline mutations ( 63 patients )  . 
 although fewer of these patients responded to treatment at 12 weeks ( 47% , 26 of 55 patients with response data ; table 1 ) compared with patients without pnao ( grade 1 , n = 1 , 763 ; 57% , 884 of 1 , 542 patients with response data ) , this was not statistically significant ( p = 1.4 x 10 - 1 )  . nine of the 63 patients with severe pnao had exome resequencing of their germline blood dna samples . 
we identified , on average , 48 stop gains ( range , 40 to 56 stop gains ) and 88 indels ( range , 73 to 111 indels ) predicted to result in frameshift mutations , per patient exome ( appendix table a1 )  . 
we excluded known inherited neuropathies in these patients by pmp22 dosage analysis and by examining the resequencing data for 66 candidate genes ( no stop gains or truncating indels were predicted )  . novel truncating mutation in ercc4 variants not present in dbsnp v.132 ( assigned as novel ; national center for biotechnology information , bethesda , md ) were considered most likely to cause pnao ; we identified on average eight novel stop gains ( range , two to 11 stop gains ) and 28 novel frameshifting indels ( range , 16 to 57 indels ) per patient ( appendix table a1 )  . 
 we also considered that germline truncating mutations in genes involved in oxaliplatin transport , metabolism , or the repair of its associated damage might be responsible for pnao ; we identified 104 such genes from literature reviews ( appendix )  . 
all nine patients carried truncating variants in these selected genes ( range , one to four variants ) ; however , only one of these variants , in a single patient , was novel ( appendix table a1 )  . 
patient 8 carried the novel stop gain ser613x in the nucleotide excision repair ( ner ) gene ercc4 , which was confirmed by sanger sequencing of an independent pcr product ( appendix table a1 )  . 
we did not find any other coding region variants in the second ercc4 allele in patient 8 after direct sequence analysis of the patients entire orf and flanking intronic sequences . 
 functional analysis of the ercc4 stop mutation we investigated whether the ercc4 nonsense mutation induced sensitivity to oxaliplatin and ultraviolet light ( which causes cpds that are repaired by ner )  . 
after oxaliplatin treatment , we observed decreased survival for rad16 - ser585x ( p = 3.5 102 ) in comparison with wild - type rad16 ( rad16 + ) and , in a similar range with a control rad16 - deleted mutant ( rad16 ; fig 1a )  . 
 similarly , we observed decreased survival of uve1 - rad16 - ser585x after treatment with ultraviolet light ( p < 1 103 ; fig 1b )  . multiple rare ercc4 variants associated with peripheral neuropathy we sought further evidence for a role of ercc4 in pnao and sanger sequenced the ercc4 orf and flanking intronic sequences in all 63 patients with pnao . 
we did not find any additional stop gains or truncating indels ; however , we did identify four rare ( minor allele frequencies < 5% in dbsnp ) nonsynonymous variants ( pro379ser , rs1799802 in three patients ; his466gln , rs372950439 in one patient ; arg576thr , rs1800068 in one patient ; and glu875gly , rs1800124 in four patients ; table 1 )  . 
the ercc4 nonsense mutation induced sensitivity to oxaliplatin and ultraviolet ( uv ) light in a schizosaccharomyces pombe ( rad16 ) model syste average percent survival from ( a ) four independent experiments after oxaliplatin treatment or ( b ) three independent experiments after treatment with uv light for a control rad16 gene deletion mutant ( rad16 ) and rad16 - ser585x ( mimics ser613x seen in a patient with peripheral neuropathy associated with oxaliplatin ) , normalized to rad16 +  . 
 ser613x was not included in the total because it was only assayed in patients with pnao ; one patient with pnao carried arg576thr and glu875gly , and another without pnao carried pro379ser and glu875gly . 
values reflect the number of patients successfully genotyped ( totals for all variants )  . functional analysis of ercc4 nonsynonymous variants we sought evidence for causal effects of pro379ser , arg576thr , and glu875gly using epstein - barr virustransformed human lymphoblastoid cell lines established from healthy individuals who carried each variant in a heterozygous state ( n = 3 for each variant and wild - type controls )  . 
although treatment with ultraviolet light reduced viability in all lines , we did not observe any differences between wild - type and variant cell lines ( data not shown )  . 
in terms of repair capacity after dna damage with ultraviolet light , all wild - type cell lines showed noticeable repair 24 hours after treatment , with the majority of cpds being repaired by 48 hours ( fig 2 )  . 
in contrast , all three sets of variant cell lines displayed reduced repair in the initial ( p < 1 103 at both 24 and 48 hours ) and validation ( p < 1 103 at both 24 and 48 hours ) experiments ( fig 2 )  . rare ( table 1 ) and five common nonsynonymous variants , two synonymous variants , and one 5utr variant ; we genotyped nonsynonymous variants in all available patients . 
seven rare nonsynonymous variants were predicted to be damaging ( c55 - c65 ) , three of which ( asp425ala , pro694leu , and ser797cys ) were individually over - represented in patients with pnao ( table 3 )  . 
 combined , rare ercc6 nonsynonymous variants were highly associated with peripheral neuropathy ( present in 20.6% of patients [ 13 of 63 patients ] with pnao v 4.7% of patients [ 82 of 1 , 749 patients ] without pnao ; p = 2.4 108 ; table 3 )  . no common ercc6 nonsynonymous variants were associated with pnao . 
we identified nine combined analyses of ercc4 and ercc6 because private variants may skew statistical associations , we considered only rare ercc4 and ercc6 nonsynonymous variants that were present in two or more patients with pnao . 
 average cyclobutane pyrimidine dimer ( cpd ) concentrations ( in nanograms per milliliter ) after ultraviolet c ( 70 j ) irradiation in wild - type cells and cells carrying ( a ) pro379ser , ( b ) arg576thr , and ( c ) glu875gly over a 48 - hour period , showing the initial ( top panels ) and validation ( lower panels ) experiments . 
cpd concentrations are plotted as an average of two duplicate samples from the same experiment run on separate enzyme - linked immunosorbent assay plates , which are shown against time with se bars ( data from the wild - type cells are shown in a , b , and c )  . 
 1 - 3 , different cell lines ; c , wild - type control cell line ; v , variant cell line . pro379ser initial experiment arg576thr glu875gly untreated ( c1 - 3 , v1 - 3 ) untreated ( c1 - 3 , v1 - 3 ) untreated ( c1 - 3 , v1 - 3 ) time ( hours ) time ( hours ) time ( hours ) validation experiment c1 - 3 c1 - 3 v1 - 3 c1 - 3 v1 - 3 c1 - 3 untreated ( c1 - 3 , v1 - 3 ) untreated ( c1 - 3 , v1 - 3 ) untreated ( c1 - 3 , v1 - 3 ) time ( hours ) time ( hours ) time ( hours ) c1 - 3 v1 - 3 c1 - 3 discussion the rare variant hypothesis predicts that individually rare but collectively common inherited variants play a significant role in disease susceptibility.32 for example , rare nonsynonymous variants in the genes encoding apolipoprotein a1 , the atp binding cassette transporter a1 and lecithin cholesterol acyltransferase , are over - represented in individuals with low plasma levels of high - density lipoprotein cholesterol , a major risk factor for coronary atherosclerosis.33 furthermore , multiple rare nonsynonymous variants in apc play a significant role in inherited predisposition to colorectal adenomas.34 here , after identifying a novel ercc4 truncating mutation in a patient with pnao , we found that multiple rare ercc4 and ercc6 nonsynonymous variants were over - represented in affected individuals . 
two rare variants in dpyd have been associated with severe toxicity in patients receiving fluorouracil , 44 and a polymorphism in ugt - 1a has been linked to a higher risk of developing irinotecan - associated neutropenia and diarrhea45 ; however , none of these biomarkers have been introduced into routine clinical practice because of their poor sensitivity and specificity . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . hannah west no relationship to disclose michelle coffey no relationship to disclose michael j . 
adams honoraria : merck serono , servier , bristol - myers squibb , amgen consulting or advisory role : merck serono , amgen , servier speakers ' bureau : merck serono travel , accommodations , expenses : servier , amgen , merck serono oliver fleck no relationship to disclose timothy s . 
cheadle patents , royalties , other intellectual property : hold ipr and patents on mutyh variants and have received royalties from myriad acknowledgment we thank simon reed and edgar hartsuiker for helpful advice and shelley idziaszczyk , rebecca williams , marc naven , and christopher smith for technical support . affiliations hannah west , michelle coffey , james p . 
mcleod , debartolo family personalized medicine institute , moffitt cancer center , tampa , fl . supported by tenovus , the kidani trust , a cancer research uk development award from the cardiff cancer research uk centre , cancer research wales , the wales gene park , a knowledge economy skills scholarship , north west cancer research , and the wales assembly government national institute of social care and health research cancer genetics biomedical research unit . 
goldberg rm , sargent dj , morton rf , et al : a randomized controlled trial of fluorouracil plus leucovorin , irinotecan , and oxaliplatin combinations in patients with previously untreated metastatic colorectal cancer . 
johnson np , hoeschele jd , rahn ro , et al : mutagenicity , cytotoxicity , and dna binding of platinum ( ii ) - chloroammines in chinese hamster ovary cells . 
afzal s , jensen sa , srensen jb , et al : oxidative damage to guanine nucleosides following combination chemotherapy with 5 - fluorouracil and oxaliplatcancer chemother pharmacol 69 : 301 - 307 , 2012 8 . 
di cesare mannelli l , zanardelli m , failli p , et al : oxaliplatin - induced oxidative stress in nervous system - derived cellular models : could it correlate with in vivo neuropathy ? free radic biol med 61 : 143 - 150 , 2013 14 . 
grothey a , mcleod hl , green em , et al : glutathione s - transferase p1 i105v ( gstp1 i105v ) polymorphism is associated with early onset of oxaliplatin - induced neurotoxicity . 
peng z , wang q , gao j , et al : association between gstp1 ile105val polymorphism and oxaliplatin - induced neuropathy : a systematic review and meta - analysis . 
lecomte t , landi b , beaune p , et al : glutathione s - transferase p1 polymorphism ( ile105val ) predicts cumulative neuropathy in patients receiving oxaliplatin - based chemotherapy . 
argyriou aa , cavaletti g , antonacopoulou a , et al : voltage - gated sodium channel polymorphisms play a pivotal role in the development of oxaliplatin - induced peripheral neurotoxicity : results from a prospective multicenter study . 
hertz dl , owzar k , lessans s , et al : pharmacogenetic discovery in calgb ( alliance ) 90401 and mechanistic validation of a vac14 polymorphism that increases risk of docetaxel - induced neuropathy . 
dolan me , el charif o , wheeler he , et al : clinical and genome - wide analysis of cisplatininduced peripheral neuropathy in survivors of adult - onset cancer . 
preston tj , henderson jt , mccallum gp , et al : base excision repair of reactive oxygen speciesinitiated 7 , 8 - dihydro - 8 - oxo - 2 - deoxyguanosine inhibits the cytotoxicity of platinum anticancer drugs . 
broyl a , corthals sl , jongen jl , et al : mechanisms of peripheral neuropathy associated with bortezomib and vincristine in patients with newly diagnosed multiple myeloma : a prospective analysis of data from the hovon - 65 / gmmg - hd4 trial . 
reardon jt , vaisman a , chaney sg , et al : efficient nucleotide excision repair of cisplatin , oxaliplatin , and bis - aceto - ammine - dichloro - cyclohexylamine - platinum ( iv ) ( jm216 ) platinum intrastrand dna diadducts . 
troelstra c , van gool a , de wit j , et al : ercc6 , a member of a subfamily of putative helicases , is involved in cockaynes syndrome and preferential repair of active genes . 
fousteri m , vermeulen w , van zeeland aa , et al : cockayne syndrome a and b proteins differentially regulate recruitment of chromatin remodeling and repair factors to stalled rna polymerase ii in vivo . 
schwab m , zanger um , marx c , et al : role of genetic and nongenetic factors for fluorouracil treatment - related severe toxicity : a prospective clinical trial by the german 5 - fu toxicity study group . 
 appendix clinical assessment clinical assessment of patients from the coin trial occurred every 3 weeks , and toxicity data were recorded on clinical research forms at weeks 0 , 6 , 12 , and 24 . 
a quality - of - life questionnaire ( european organisation for research and treatment of cancer quality of life questionnaire c30 ) was also completed at 0 , 6 , 12 , and 24 weeks . 
patients with severe peripheral neuropathy had a minimum of grade 3 toxicity within the first 12 weeks of treatment , which was backed up by quality - of - life data . molecular analyses and exome resequencing using the exome resequencing data , the following genes associated with rare inherited neuropathies were analyzed : pmp22 , aars , aifm1 , atl1 , atp7a , bicd2 , bscl2 , cct5 , ctdp1 , dctn1 , dhtkd1 , dnajb2 , dnm2 , dnmt1 , dync1h1 , egr2 , fam134b , fbln5 , fgd4 , gars , gdap1 , gjb1 , gnb4 , hars , hint1 , hk1 , hspb1 , hspb3 , hspb8 , ighmbp2 , ikbkap , kars , kif1a , kif5a , litaf , lmna , lrsam1 , mars , med25 , mfn2 , mpz , mtmr13 , mtmr2 , myh14 , ndrg1 , ngfb , ntrk1 , pdk3 , plekhg5 , prnp , prps1 , prx , rab7 , reep1 , sbf1 , scn9a , setx , sh3tc2 , slc5a7 , sptlc1 , sptlc2 , tfg , trim2 , trpv4 , wnk1 , and yars . genes potentially involved in the pharmacokinetics and mechanism of action of platinum compounds were identified from literature reviews . 
four genes were involved in drug influx ( oct1 , oct2 , ctr1 , and hmate1 ) , three in trafficking ( ccs , cox17 , and sod1 ) , seven in detoxification ( mt1a , mt2a , nqo1 , gstt1 , gstp1 , gstm1 , and mpo ) , two in oxalate metabolism ( agxt and grhpr ) , three in sequestration ( atp7a , atp7b , and hah1 ) , 32 in dna damage response and subsequent signaling pathways ( spt16 , ssrp1 , hmgb1 , rag1 , rag2 , abl1 , rb1 , p53 , p73 , aurka , ccng2 , p38mapk , msk1 , mkk3 , mkk6 , histone h3 , erk , mek1 , mek2 , jnk , mkk4 , mkk7 , mpk1 , akt , nf - kb , xiap , bax , apaf1 , cyc , casp3 , casp6 , and casp9 ) , 46 in dna damage repair and the associated response pathways ( polb , polh , polm , rev3l , fanca , fancb , fancc , fancd2 , fance , fancf , fancg , fanci , fancl , fancm , fancn , faap100 , rm1 , fan1 , mlh1 , msh2 , msh6 , pms2 , atm , atr , chek1 , chek2 , brca1 , brca2 , gadd45 , ddb2 , cdc25c , cdc2 , csa , hr23b , rnapolii , rpa1 , ercc1 , ercc2 , ercc3 , ercc4 , ercc5 , ercc6 , xpa , xrcc1 , xrcc3 , and mgmt ) , and seven in drug efflux ( abcc1 , abcc2 , abcc3 , abcc4 , abcc5 , abcb1 , and abcg2 )  . polymerase chain reaction and sanger sequencing thermal cycling conditions consisted of an initial denaturation at 94c for 10 minutes , followed by 32 cycles of 94c for 30 seconds , 57c for 30 seconds , and 72c for 30 seconds , followed by a final elongation stage of 72c for 10 minutes . 
 polymerase chain reaction ( pcr ) products were purified using exosap , in which 15 l of pcr product was incubated with 2 u of exonuclease i ( new england biolabs , ipswich , ma ) and 2 u of shrimp alkaline phosphatase ( ge healthcare , chicago , il )  . 
samples were run on an abi 3100 genetic analyzer ( applied biosystems ) , and sequence data were viewed using sequencher v4.6 ( gene codes , ann arbor , mi )  . single nucleotide polymorphism genotyping genotyping of arg415gln ( rs1800067 ) in ercc4 and gly399asp ( rs2228528 ) , arg1213gly ( rs2228527 ) , and gln1413arg ( rs2228529 ) in ercc6 was carried out using illuminas fast - track genotyping service using their high - throughput beadarray technology ( illumina , san diego , ca )  . 
the overall genotyping success rate was 99.9% ( 8 , 731 of 8 , 744 genotypes were called successfully ) , and the concordance rate for previously sequenced samples ( n = 63 ) was 100% ( 252 of 252 genotypes were concordant )  . 
genotyping of pro379ser ( rs1799802 ) , arg576thr ( rs1800068 ) , his466gln ( rs372950439 ) , glu875gly ( rs1800124 ) , and rs1799800 in ercc4 and of asp425ala ( rs4253046 ) , gly446asp ( rs4253047 ) , pro694leu ( rs114852424 ) , ser797cys ( rs146043988 ) , gly929arg ( novel ) , phe1217cys ( rs61760166 ) , arg1230pro ( rs4253211 ) , ala1296thr ( rs139509516 ) , thr1441ile ( rs4253230 ) , and phe1437ile ( rs758679804 ) in ercc6 was carried out by lgc ( teddington , united kingdom ) using kaspar technology . 
the overall genotyping success rate was 97.5% ( 33 , 415 of 34 , 320 genotypes were called successfully ) , and the concordance rate for previously sequenced samples ( n = 63 ) was 99.9% ( 881 of 882 genotypes were concordant )  . 
in addition , these primers carried sequences corresponding to regions upstream and downstream of ura4 in the plasmid paw1 ( shown in lowercase ; forward : 5 - tccatccaaattggaaaattttcgcatcaaagtatttaacagctttcagaaatcaaaattgcaaattggaaaatctctacgaataacaccaccattaaatcggatccccgggttaattaa - 3 ; reverse : 5 - ttattaattaggtgcgcttaacattctatatatggtgaaccaatatatatcagatgtagaagcaaaaattaaatatattacaaaattataaaaaaataaagaattcgagctcgtttaaac - 3 )  . 
amplification of ura4 in paw1 ( linearized with acci ; new england biolabs ) was achieved by pcr to produce a 2.1 - kb product consisting of ura4 flanked by loxp / loxm sites ( loxp - ura4 - loxm ) and rad16 gene sequences , as previously described ( watson at , et al : gene 407 : 63 - 74 , 2008 )  . 
transformants were grown on minimal medium lacking uracil and restreaked on plates containing the same mediua replica plate was irradiated with 150 j / m2 of ultraviolet light to identify those with ultraviolet sensitivity , a characteristic of rad16 loss . 
extracted dna was sequenced at 5 and 3 lox sites to ensure their integrity . rad16 wild - type pcr product with flanking lox sites . the creation of a rad16 wild - type pcr product with flanking lox sites ( loxp - rad16 - loxm3 ) was performed using primers designed with lox sites incorporated ( forward : 5 - gggataacttcgtatagcatacattatacgaagttatatgcatcatcatcatcatcatggaggaggagaaacaaaggttcatttgcc - 3 ; reverse : 5 - gggataacttcgtatataataccatatacgaagttatttactcatagtcctttaactgttttcgg - 3 )  . 
pombe dna was carried out using phusion polymerase ( new england biolabs ) , with thermal cycling conditions consisting of an initial denaturation of 98c for 2 minutes , followed by 30 cycles of 98c for 30 seconds , 47c for 30 seconds , and 72c for 3 minutes and 30 seconds , with a final elongation of 72c for 10 minutes . 
pcr products were cleaned using a nucleospin gel and pcr clean - up kit ( macherey - nagel , bethlehem , pa )  . cre recombinase - mediated cassette exchange . cre recombinase - mediated cassette exchange was carried out using a paw8 - ccdb plasmid and the loxp - rad16 - loxm3 pcr product ; 170 ng of paw8 - ccdb , 90 ng of loxp - rad16 - loxm3 pcr product , and 2 u of cre recombinase ( new england biolab ) were incubated at 37c for 30 minutes , followed by 70c for 10 minutes . 
 aliquots of the cultures were plated on yea plates with added 5 - fluoroorotic acid ( 1 g / l ) to allow for growth of ura4 cells , which were streaked on master plates . 
functionality of the strains transformed with the wild - type rad16 was performed to determine any potential detrimental effects associated with the incorporation of the lox sites flanking the rad16 region . 
thermocycling conditions consisted of an initial denaturation at 95c for 1 minute , followed by 18 cycles of 95c for 50 seconds , 60c for 50 seconds , and 68c for 6 minutes , and a final elongation at 68c for 7 minutes . 
strains were mixed on sporulation medium ( malt extract agar ) , incubated for 2 days at 30c , and treated for 30 minutes with 30% ethanol to kill vegetative cells . 
the resulting strains were ol2123 ( smt - 0 loxp - rad16 + - loxm uve1 : : leu2 leu1 - 32 ura4 - d18 ) and ol2131 ( smt - 0 loxp - rad16 - s585x - loxm uve1 : : leu2 leu1 - 32 ura4 - d18 )  . drug and ultraviolet light treatments . a primary culture of cells was grown overnight in yel with shaking at 30c ; 107 cells were cultured in yel with and without 1 mm of oxaliplatfor the untreated cultures , an equivalent volume of dimethyl sulfoxide was added . 
 for ultraviolet light treatment , appropriate numbers of cells were irradiated with ultraviolet light using a stratalinker ( agilent ; 5 j / m2 for ol2116 [ rad16 uve1 ] and ol2131 [ rad16 - s585x uve1 ] and 20 j / m2 for ol2112 [ uve1 ) ]  . 
plates were incubated at 30c for 4 days , and survival rates were determined by counting colonies of treated compared with untreated plates . functional studies in human cells survival analyses . before survival analyses , 3 106 cells / ml were serum starved for 1 hour before treatment with ultraviolet light ( 40 jm2s1 ) irradiation . 
cells were resuspended in normal tissue culture media containing fetal bovine serum and antibiotics , and aliquots were removed at 0 , 4 , 24 , and 48 hours after treatment for analysis . 
dna samples were probed for cyclobutane pyrimidine dimers ( cpds ) using an enzyme - linked immunosorbent assay ( elisa ) kit according to the manufacturers instructions ( cell biolabs , san diego , ca )  . 
briefly , dna samples and a dna standard conjugated to a known amount of cpds were converted to single - stranded dna by incubation at 96c for 10 minutes followed by rapid chilling on ice for 10 minutes . 
wells were washed twice with cold phosphate - buffered saline , followed by hour - long incubations at room temperature with assay diluent , primary cpd antibody , blocking reagent , and secondary horseradish peroxidaseconjugated antibody , with wash steps between each incubation . 
 biological validation of rna sequencing data from formalinfixed paraffin - embedded primary melanomas purpose initiatives such as the cancer genome atlas and international cancer genome consortium have generated high - quality , multiplatform molecular data from thousands of frozen tumor samples . 
although these initiatives have provided invaluable insight into cancer biology , a tremendous potential resource remains largely untapped in formalin - fixed , paraffin - embedded ( ffpe ) samples that are more readily available but which can present technical challenges because of crosslinking of fragile molecules such as rna . materials and methods we extracted rna from ffpe primary melanomas and assessed two gene expression platformsgenome - wide rna sequencing and targeted nanostringfor their ability to generate coherent biologic signals . 
we also make comparisons to the cancer genome atlas and other publicly available melanoma datasets . results the comparison of the gene expression patterns to each other , to established biologic modules , and to clinical and immunohistochemical data confirmed the fidelity of biologic signals from both platforms using ffpe samples to known biology . 
moreover , correlations with patient outcome data were consistent with previous frozen - tissue based studies . conclusion ffpe samples from previously difficult - to - access cancer types , such as small primary melanomas , represent a valuable and previously unexploited source of analyte for rna sequencing and nanostring platforms . 
2018 by american society of clinical oncology introduction whole transcriptome rna sequencing ( rnaseq ) has drastically improved the fidelity , resolution , and comprehensiveness of global rna assessment compared with gene expression microarray technology . 
in addition to providing higher - quality assessment , particularly of low - expressing genes , it is unbound by hybridization constraints , meaning that micrornas and noncoding rnas , as well as multiple gene isoforms , exon - exon junctions , and fusion genes can also be assessed . 
these advantages have been leveraged to great effect in largescale efforts such as the cancer genome atlas ( tcga ) 1 and international cancer genome consortium , 2 where thousands of samples have been assessed together with high confidence and accuracy . one of the limitations of implementing rna - seq technology thus far has been the requirement for analytes prepared from frozen tissues.3 formalin fixed , paraffin - embedded ( ffpe ) samples are lawrence n . 
 much more plentiful but are also more susceptible to nucleic acid fragmentation and general sample deterioration , making the extraction of well - preserved rna for sequencing a difficult challenge.4 if , however , ffpe - derived rnaseq data could be optimized and standardized , it would exponentially expand the number of biospecimens available and streamline sample processing . 
moreover , in many cancer types , limiting the analyses to only frozen tissues may result in skewing of samples toward , for example , surgically resectable and / or bulky tumors , resulting in a sample population biased by selection . 
in the melanoma tcga dataset , which used frozen samples only , primary melanomas were heavily skewed toward very thick tumors ( median tumor thickness , 11 mm ) that correspond to an american joint committee on cancer t4 primary tumor.1 , 5 , 6 in contrast , the vast majority of cutaneous melanomas diagnosed in the united states have a tumor thickness 4 mm , most of which are 1 mm , and all of which generally undergo ffpe processing for diagnostic purposes . 
tumor thickness is a well - established , independent predictor of melanoma clinical outcome and the principle primary tumor factor for treatment decision making6 ; therefore , the lack of thinner , more clinically relevant primary melanomas in the tcga dataset limits a full molecular understanding of the disease and optimal potential translation to the clinic . 
ffpe samples offer the opportunity to include tumors across all tumor thicknesses in rna - seq datasets , for which we demonstrate feasibility in this study . to date , only 10 studies have assessed the technological feasibility of transcriptome - scale rna seq from analytes prepared from human ffpe tumor tissue.7 - 17 although these studies conducted technical quality controls of the data , including direct comparison of frozen and ffpe from the same samples , 7 - 10 , 15 the question of whether the data accurately reflected the underlying biology relied mainly on detecting large differences between either normal and tumor tissues8 or between transcriptionally distinct tumor subtypes , 8 - 14 , 16 leaving open the question of fidelity for more subtle gene expression differences between tumors . 
for full patient information , see the data supplement . rna extraction the high pure mirna isolation kit ( roche , basel , switzerland ) was used to extract rna , and the zymo - spin column ( zymo research , irvine , ca ) was used to remove melanin from all samples , regardless of melanin content , for consistency . 
additional details , including rnaseq run metrics , are reported in the data supplement . pathology - specific assessment we conducted pathologic assessment to quantify the tumor surface area before rna extraction , and we used this to predict the required number of 10 m slides to yield the minimum amount of total rna per case required . 
 a sort by correlation ( ( cid : 85 ) ) to previous median median of all genes ( per sample ) median of top 20% genes ( per sample ) median of genes with > 0.6 ( per sample ) median of genes with ( > 0.6 per sample ) i . 
 ( e ) final melanocyte gene set , tcga data . defining pathway scores our iterative subsetting approach to generating pathway scores depends on the quality of the initial input gene set . 
it makes two assumptions : highly cocorrelating genes largely represent shared biologic functionality , and high - quality input gene sets contain sufficiently strong signal from true biology genes such that when the initial crude score is calculated ( fig 1a ) , the true biology signal will emerge from the noise ( figs 1b and 1c )  . 
patient disease characteristics stratified by disease recurrence status for corresponding study specimens ( n = 38 ) ( continued ) no recurrence recurrence overall cohort characteristic cd8 score of tumor center not scored ( range ) mart1 / phh3 score , median 5.5 ( 0 - 47 ) 14 ( 0 - 122 ) 8.5 ( 0 - 122 ) the basis of eventual clinical outcome ( table 1 )  . 
of 1 , 362 38 ffpe primary melanomas no recurrence ( n = 18 ) > 60 months recurrence ( n = 20 ) 3 - 18 months rna extraction rna - seq > 21 , 000 genes nanostring 1 , 432 genes nanostring v rna - seq fig 2 . 
 ( b ) spearman correlation values for all 1 , 362 genes shared by the rna - seq and nanostring datasets , as well as stratified by expression and dynamic range . 
 initially , this seemed to indicate a limited overall correlation between platforms , but we reasoned that certain genes may seem to correlate poorly for causes unrelated to cross - platform fidelity . 
genes with low absolute expression ( n = 221 genes , 16% of total ) showed poor correlation across platforms , suggesting the existence of a limit of resolution ( fig 2b )  . 
the best interplatform - correlating genes had a significantly higher mad / m compared with the poorest interplatform correlating genes ( p < .001 ; figs 2c and 2d )  . 
after removing low - expressing ( < 1.0 average reads per kilobase million ) and low - dynamicrange genes ( < 0.25 mad / m ; n = 251 genes , 18% of total ; fig 2b ) , the percentage of genes with a spearman correlation value of > 0.5 improved from 68% to 84% ( 746 of 890 )  . 
for example , bub1 and top2a , both cell cyclerelated genes , are consistently coexpressed across a wide variety of datasets , including that of the current study ( appendix fig a1 )  . 
when this gene - togene cocorrelation analysis is extended to a larger scale to identify cocorrelating pathways , the overall strength of the correlations can gauge how well the underlying biology is captured by the quality of the dataset . 
we chose to use tcga melanoma data as a reference ground truth for identifying cocorrelating core pathway genes , on the basis of the high quality and quantity of data available , as well as the high degree of uniformity of the tcga pipeline.1 to simplify pathway analyses , we sought to create a pathway score for each pathway that accurately describes its relative activation state in each sample . 
one obstacle to this approach is that genes within existing defined biologic gene sets ( eg , from molecular signatures database [ msigdb ] ; gsea / msigdb ) 19 are not necessarily all cocorrelated with one another , potentially leading to a noisy score . 
therefore , we developed a method that repetitively iterates the score calculation on the basis of gene subsetting , until the score converges on a subset of highly cocorrelated genes . 
figure 1a illustrates this iterative process using the example of starting with the go_immune_system_process from msigdb to create an immune score ; a detailed description of the steps is presented in the data supplement . 
 figures 1b and 1c show examples of how the tcga immune and melanocyte scores change during each score iteration , and their final subset gene lists are shown in figures 1d and 1e . this high degree of cocorrelation of the final gene subset implies functional similarity within a broad pathway or cell type ; indeed , the final immune subset of 407 genes ( of an initial 1 , 984 ) was highly enriched for known true biology genes , including cd3 , cd8 , and cd4 genes ( fig 1d ; data supplement )  . 
of the 407 core immune genes we identified , 190 were present on both platforms and included core canonical immune genes such as cd3d / e / g , cd4 , cd8a / b , and cd86 , again retaining strong cocorrelation within each platform ( figs 3a and 3b )  . 
the majority of genes ( 154 of 190 ; 81% ) had a correlation of > 0.5 on both platforms , which further increased ( 140 of 163 ; 86% ) after removal of low - expressing genes . 
direct comparison of the final immune scores showed strong concordance between rna - seq and nanostring ( = 0.91 ) on a per - sample basis ( fig 3c )  . 
these results suggest that , after controlling for expression level , both platforms were able to successfully capture true positive immune genes while preserving biologic fidelity . we generated scores for additional signatures : cell cycle , skin , pigment , and epithelial - mesenchymal transition ( emt ; the list of starting gene sets and final gene subsets is given in the data supplement )  . 
first , we performed a hierarchical clustering of our dataset with 21 tcga tumor types using the most variable pan - cancer tcga genes and showed that our ffpe dataset clustered tightly with both cutaneous and uveal melanoma , primarily by the high expression of melanocyte - specific genes ( appendix fig a4 )  . 
finally , we examined a known pathway correlation among our five gene sets , shown in multiple cell - line studies : the emt and pigment signatures anticorrelate.21 in vivo , multiple stromal cell types express the emt signature , weakening the correlation . 
nevertheless , in the tcga dataset , among primary melanoma samples ( n = 103 ) , the emt and pigment signatures anticorrelated ( = 0.47 ; fig 3f )  . 
the cell cycle signature from rna - seq correlated well with ihc for mart1 / phh322 ( ie , cells double positive for mart1 , a melanoma marker , and phh3 , a marker of dividing cells ; fig 4a ) and the observed mitotic rate ( fig 4b )  . 
emt , epithelial - mesenchymal transition ; rna - seq , rna sequencing ; tcga , the cancer genome atlas . correlations were also detected in the nanostring dataset ( appendix fig a6 )  . 
this correlation was stronger for positive staining in the center of the tumor ( figs 4c and 4d ) compared with the periphery ( appendix fig a6 )  . we next sought to determine how pathway scores correlated with other clinical data . 
in addition , the melanocyte score negatively correlated with the chronic sun damage score ( fig 5c ) , which is a measure of the degree of solar elastosis in normal skin adjacent to the primary melanoma lesions in hematoxylin and - eosinstained tissue sections.23 finally , we performed an unbiased gene - set enrichment analysis to identify pathways that correlate with patient outcome . 
consistent with findings of previous gene expression studies of primary melanoma , 24 - 26 an increase in cell cycle gene expression was significantly enriched in samples of patients in whom melanoma eventually recurred ( fig 5d )  . 
to further substantiate the biologic fidelity of our gene - set scores , we next compared the cell cycle score between primary tumors from the recurrence versus no recurrence cohorts . 
in this study , we created an approach to assessing pathway scores that subsets gene lists by enriching for genes that together form functionally related sets of well - correlated expression patterns . 
for example , the use of unbiased whole - transcriptome rnaseq allows for robust discovery of unanticipated pathways of interest , using a vastly expanded set of archival ffpe samples . to our knowledge , our study is the first to assess the biologic fidelity of continuous differences in gene expression in ffpe - derived rna - seq data rather than bulk differences between tumor subtypes and / or normal tissue.7 - 17 it is also the first to directly compare ffpe - derived rna - seq data with nanostring data and with quantitative ihc findings . 
in the case of primary melanoma , cell cycle scores may help stratify patients with early - stage melanoma into those likely to relapse or not ; more broadly , the unbiased nature of rna - seq will enable uncovering novel biomarkers in a variety of settings . 
 we further suggest that our approach can be widely used to more accurately calculate pathway scores , because current methods process all genes in a gene set regardless of degree of cocorrelation . 
davies consulting or advisory role : glaxosmithkline , roche , novartis , sanofi , vaccinex , bristol - myers squibb , syndax , nanostring technologies research funding : glaxosmithkline ( inst ) , roche ( inst ) , astrazeneca ( inst ) , merck ( inst ) , oncothyreon ( inst ) , myriad genetics ( inst ) , sanofi alexander j . 
lazar employment : ge healthcare ( i ) leadership : beta cat pharmaceuticals , archer biosciences stock and other ownership interests : archer biosciences , beta cat pharmaceuticals honoraria : novartis , bristol - myers squibb , janssen oncology , roche consulting or advisory role : novartis , illumina , ge healthcare research funding : medimmune , astrazeneca , roche , novartis patents , royalties , other intellectual property : elsevier travel , accommodations , expenses : bristol - myers squibb , novartis jeffrey e . 
camargo cancer center , sao paulo , brazil ; and man kam kwong , hong kong polytechnic university , hong kong , china . support supported in part by the national institutes of health ( nih ) specialized program of research excellence melanoma grant no . 
 p30ca016672 ; a melanoma research alliance team science award ; generous philanthropic contributions to the university of texas md anderson melanoma moon shots program ; the dr miriam and sheldon g . 
adelson medical research foundation ; the robert and lynne grossman family foundation ; the michael and patricia booker melanoma research endowment ; aim at melanoma ; the university of texas rising stars award and the melanoma research alliance young investigator award 508743 , both to l.n.k. references 1696 , 2015 1 . 
gershenwald je , scolyer ra , hess kr , et al : melanoma staging : evidence - based changes in the american joint committee on cancer eighth edition cancer staging manual . 
eikrem o , beisland c , hjelle k , et al : transcriptome sequencing ( rnaseq ) enables utilization of formalin - fixed , paraffin - embedded biopsies with clear cell renal cell carcinoma for exploration of disease biology and biomarker development . 
jovanovi b , sheng q , seitz rs , et al : comparison of triple - negative breast cancer molecular subtyping using rna from matched fresh - frozen versus formalin - fixed paraffin - embedded tissue . 
morton ml , bai x , merry cr , et al : identification of mrnas and lincrnas associated with lung cancer progression using next - generation rna sequencing from laser micro - dissected archival ffpe tissue specimens . 
sharron lin x , hu l , sandy k , et al : differentiating progressive from nonprogressive t1 bladder cancer by gene expression profiling : applying rna - sequencing analysis on archived specimens . 
esteve - codina a , arpi o , martinez - garca m , et al : a comparison of rna - seq results from paired formalin - fixed paraffin - embedded and fresh - frozen glioblastoma tissue samples . 
nikitina as , sharova ei , danilenko sa , et al : novel rna biomarkers of prostate cancer revealed by rna - seq analysis of formalin - fixed samples obtained from russian patients . 
li j , fu c , speed tp , et al : accurate rna sequencing from formalin - fixed cancer tissue to represent high - quality transcriptome from frozen tissue . 
 ( c ) top : heatmap of the 38 formalin - fixed paraffin - embedded ( ffpe ) rna - seq dataset for all 407 tcga - derived immune gene - set genes . 
bottom : the median absolute deviation divided by the median ( mad / m ) for all 407 immune genes for each sample , a measure of correlative discordance within the immune signature . 
heatmaps showing the final fixedpoint gene sets for ( a ) epithelial - mesenchymal transition ( emt ) , ( b ) cell cycle , and ( c ) skin for rna sequencing ( rna - seq ) and nanostring . 
each gene - set member is correlated with its respective overall gene - set score , for primary melanomas only in the ( a ) the cancer genome atlas ( tcga ) and current formalin - fixed paraffin embedded ( ffpe ) rna - seq and ( b ) gse7553 and gse15605 datasets . 
 we note that the mitf / melanocyte pathway was not recovered , because of the smaller dataset ( n = 38 samples here v n = 333 in tcga ) and the lower variability in melanocyte gene expression , resulting in those genes not being among the top 5% . 
 ( b ) average reads per kilobase million ( rpkms ) for all genes within the five gene sets used in this study and for three gene sets not expected to be highly expressed in melanoma . 
 evolving intersection between inherited cancer genetics and therapeutic clinical trials in prostate cancer : a white paper from the germline genetics working group of the prostate cancer clinical trials consortium purpose advances in germline genetics , and related therapeutic opportunities , present new opportunities and challenges in prostate cancer . 
the prostate cancer clinical trials consortium germline genetics working group was established to address genetic testing for men with prostate cancer , especially those with advanced disease undergoing testing for treatment - related objectives and clinical trials . methods the prostate cancer clinical trials consortium germline genetics working group met monthly to discuss the current state of genetic testing of men with prostate cancer for therapeutic or clinical trial purposes . 
we assessed current institutional practices , developed a framework to address unique challenges in this population , and identified areas of future research . results genetic testing practices in men with prostate cancer vary across institutions ; however , there were several areas of agreement . 
cheng , md , phd , division of medical oncology , university of washington , 825 eastlake ave e , seattle , wa 98109 ; e - mail : hhcheng@ uw.edu. introduction although the contribution of heredity to prostate cancer has long been known , the underlying genetic causes remained elusive . 
 clarify patient preferences in genetic testing to guide prostate cancer treatment / clinical trial * collect family history tumor testing tumor testing germline testing discuss potential to identify germline findings pretest education by genetic counselor and / or oncologist depending on resources recommend gc if tumor sequencing suggestive ( eg , brca1 / 2 ) for dedicated , confirmatory germline testing recommend gc if germline results concerning for mutation ( eg , brca1 / 2 ) recommend gc post - test if germline mutation positive : discuss additional cancer risks for patient cascade testing in family if germline mutation negative or variant of uncertain significance : discuss additional genetic testing in family as appropriate or as indicated by family history if family history suggestive ( see table 2 ) fig 1 . 
for prostate cancer , genetic counseling and testing practices are newly driven by a growing interest in identifying patients who are candidates for enrollment in biomarker - selected clinical trials . 
this treatment - driven ascertainment , where patients are referred for germline testing in part for therapy selection , presents unique opportunities and challenges for practitioners regarding appropriate delivery of elements of genetic counseling in a feasible manner . the prostate cancer clinical trials consortium is a group of researchers from 11 institutions working together to develop novel therapeutics and biomarkers , translating scientific discoveries to improve standards of care in prostate cancer . 
for example , the brcaaway trial ( clinicaltrials.gov identifier : nct03012321 ) is a phase ii randomized trial of the parp inhibitor olaparib versus abiraterone versus the combination of the two agents in men with germline or somatic homologous recombination deficiency mutations . 
additional trials are exploring the efficacy of rucaparib , niraparib , and olaparib as single agent for men with metastatic castration - resistant prostate cancer and a deleterious genomic alteration , either germline or somatic , in brca2 , brca1 , and other ddr genes ( clinicaltrials . gov identifiers : nct02952534 , nct02975934 , nct02854436 , nct02987543 )  . 
the triumph ( trial of rucaparib in patients with metastatic hormone - sensitive prostate cancer harboring germline dna repair gene mutations ) trial ( clinicaltrials.gov identifier : nct03413995 ) will enroll men with metastatic hormone - sensitive prostate cancer and a germline ddr gene pathogenic alteration , who will be treated with the parp inhibitor rucaparib in the absence of hormonal therapy . 
clinical trials testing novel approaches to genetic testing title novel approaches genetic evaluation of menthe gem registry gentlemen : genetic testing for men with metastatic prostate cancer evaluating an alternative clinical genetics cancer care delivery model : a pilot study of patient outcomes prospective research registry of men with prostate cancer or at increased risk web - based consent and pretest counseling web - based and phone - based post - test counseling pathogenic and likely pathogenic mutation results are delivered by a genetic counselor over the phone and invited for in - person counseling consenting by primary oncologist or urologist , same - day blood draw standard pretest education and video risk assessment and delivery of results by a genetic counselor by telephone clinicaltrials.gov identifier nct03076242 nct03503097 nct02987543 progen : genetic counseling processes and outcomes among males with prostate cancer comparison of standard genetic counseling v video - based counseling with in - person counseling only for patients with germline mutations nct03328091 trial possibilities , and , second , inherited cancer risk . 
for providers , it is worth discussing and confirming patient goals before offering testingfor example , asking whether patients are interested primarily in treatment options , familial risk assessment , or both . 
table 2 summarizes clinical criteria to consider for referral to genetic counseling . this panel agrees that men with prostate cancer who undergo germline genetic testing for therapeutic or clinical trial options should receive pretest education on the implications of a positive result for themselves and for their families . 
in several recent studies of research somatic sequencing , germline mutations with clinical implications were identified.32 , 33 tumor sequencing may even be more sensitive in detecting genetic syndromes , such as lynch , than the traditional molecular tests.34 most commercial tumor assays do not specifically report whether a mutation is present in the germline , and some subtract the germline component , but the presence of well - described founder mutations may be highly suggestive . 
 for example , the ashkenazi jewish brca1 / 2 founder mutations ( brca1 185delag ; brca1 5382insc ; brca2 6174delt ) are almost always germline , not somatic , events , and ordering providers should be familiar with the somatic tumor profiling can also identify increased mutation load and msi , which can be associated with germline mmr mutations ( lynch syndrome ) .35 although it seems that most patients are interested in knowing secondary germline findings , they also expect their providers to offer decision making guidance and clarify key information.36 , 37 this panel agrees that men with prostate cancer who undergo tumor - based genetic testing for therapeutic or clinical trial options should be educated about the potential for uncovering germline mutations , which may warrant referral to a cancer genetic specialist for confirmatory germline testing . 
the traditional clinical genetics cancer care delivery modelwhere patients are referred to a genetic counselor for in - person , pretest risk assessment and education and in - person post - test counselingcannot meet the projected demand for testing of patients with prostate cancer , some facing time - sensitive treatment decisions . 
challenges and new research directions challenge or direction defining which patients should be offered germline genetic testing and at what point ( s ) in the diagnosis / treatment timeline the role of less - studied germline dna - damage repair genes for therapeutic decision making and clinical trial eligibility best framework and workflows for rapid testing for time - sensitive therapeutic decisions integration of cascade education and testing for family members ensuring historically underserved populations have access to genetic testing cancer and lynch syndromes . 
these barriers include process issues ( referral to genetic counseling and testing , access , wait times , insurance coverage ) ; physician knowledge , comfort , and time ; patients lack of awareness and understanding ; and refusal of testing . 
for example , > 85% of patients with ovarian cancer reported willingness to be tested if there were therapeutic implications or benefit to family , and a majority believed that genetic testing should be offered before or at the time of diagnosis.38 current barriers to genetic testing have been described in the context of testing for cancer predisposition in hereditary breast and ovarian when testing for therapeutic decision making , the ability to undergo assessment and testing and receive results in a timely manner is of utmost table 5 . 
newer approaches in cancer risk genetics include videoor phone - based pretest counseling and mainstreaming , an approach in which trained individuals provide standardized consenting and counseling before testing and genetics referral.39 the engage ( evaluation of a streamlined oncologist - led brca mutation testing and counseling model for patients with ovarian cancer ) study of oncologist - led brca1 / 2 mutation testing in women with ovarian cancer showed that this process is feasible , with high patient satisfaction.40 these alternate genetic counseling delivery approaches need to be studied for provider feasibility and patient acceptability . 
although awareness of cascade testing is important in any situation where a germline mutation is identified , it can be particularly important when genetic testing is performed for therapeutic selection . 
in contrast to patients who pursue genetic testing because of familial cancer risk , those who undergo germline testing for therapy selection may be less aware of the potential implications to family members , because they were not necessarily tested because of an identified familial risk . 
moreover , men with prostate cancer are often diagnosed when their children are adults , can pursue testing , and , if positive , undergo enhanced cancer screening or risk - reduction strategies . there are several known barriers for a patients communication of results to family members . 
 in brca1 / 2 screening studies , factors associated with of lack of communication include high worry about genetic risks , low interest or understanding of genomic information , and negative family history.57 - 59 men and second - degree relatives are less likely to pursue genetic testing.58 thus , there is an opportunity through education to increase familial communication of results . 
 framework for genetic testing was developed for individuals believed to be at risk for inherited syndromes , but this model requires adaptation for men with mpc who are increasingly referred for genetic testing to aid in treatment decisions . 
alumkal consulting or advisory role : astellas pharma , bayer ag , janssen biotech research funding : aragon pharmaceuticals ( inst ) , astellas pharma ( inst ) , novartis ( inst ) , zenith epigenetics ( inst ) , gilead sciences ( inst ) tomasz m . 
beer stock and other ownership interests : salarius pharmaceuticals consulting or advisory role : abbvie , astrazeneca , astellas pharma , bayer ag , boehringer ingelheim , clovis oncology , janssen biotech , janssen oncology , janssen research & development , johnson & johnson , janssen japan , merck , pfizer research funding : boehringer ingelheim ( inst ) , bristol - myers squibb / medarex ( inst ) , janssen research & development ( inst ) , medivation / astellas ( inst ) , oncogenex ( inst ) , sotio ( inst ) , sotio , theraclone sciences ( inst ) himisha beltran consulting or advisory role : janssen oncology , genzyme , glaxosmithkline , abbvie research funding : astellas pharma ( inst ) , janssen ( inst ) , abbvie / stemcentrx , eli lilly ( inst ) , millennium pharmaceuticals ( inst ) daniel j . 
heath honoraria : bayer , dendreon , sanofi consulting or advisory role : agensys speakers ' bureau : sanofi research funding : tokai pharmaceuticals ( inst ) , seattle genetics ( inst ) , agensys ( inst ) , dendreon ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , celldex therapeutics ( inst ) , inovio pharmaceuticals ( inst ) , celgene ( inst ) celestia s . 
higano employment : cti biopharma ( i ) leadership : cti biopharma ( i ) stock and other ownership interests : cti biopharma honoraria : genentech consulting or advisory role : bayer ag , ferring pharmaceuticals , orion , astellas pharma , clovis oncology , asana biosciences , endocyte , blue earth diagnostics , myriad genetics , tolmar , janssen research funding : aragon pharmaceuticals ( inst ) , astrazeneca ( inst ) , dendreon ( inst ) , genentech ( inst ) , medivation ( inst ) , emergent biosolutions ( inst ) , bayer ( inst ) , pfizer ( inst ) , roche ( inst ) , astellas pharma ( inst ) travel , accommodations , expenses : bayer ag , astellas pharma , clovis oncology , blue earth diagnostics , endocyte , ferring pharmaceuticals , genentech , orion pharma , menarini , myriad genetics , pfizer rana r . 
morgans honoraria : genentech , janssen , johnson & johnson , sanofi , astrazeneca consulting or advisory role : genentech , astrazeneca , sanofi akash patnaik honoraria : clovis oncology , merck , prime oncology consulting or advisory role : janssen oncology research funding : bristol - myers squibb ( inst ) , progenics pharmaceuticals ( inst ) , janssen oncology ( inst ) , clovis oncology ( inst ) travel , accommodations , expenses : clovis oncology , bristol - myers squibb , merck , prime oncology , janssen oncology charles j . 
ryan honoraria : janssen oncology , astellas pharma , bayer consulting or advisory role : bayer ag , millennium pharmaceuticals , ferring pharmaceuticals research funding : bind biosciences , karyopharm therapeutics , novartis walter m . 
stadler honoraria : cvs caremark , sotio , astrazeneca , bristolmyers squibb consulting or advisory role : cvs caremark , sotio , astrazeneca , bristol - myers squibb , eisai , bayer ag , pfizer , clovis oncology , genentech research funding : bayer ag ( inst ) , bristol - myers squibb ( inst ) , boehringer ingelheim ( inst ) , exelixis ( inst ) , novartis ( inst ) , genentech ( inst ) , glaxosmithkline ( inst ) , medivation ( inst ) , pfizer ( inst ) , merck ( inst ) , millennium pharmaceuticals ( inst ) , janssen ( inst ) , johnson & johnson ( inst ) , astrazeneca ( inst ) , abbvie ( inst ) , x4 pharmaceuticals ( inst ) , calithera biosciences ( inst ) other relationship : uptodate , american cancer society mary - ellen taplin honoraria : janssen - ortho , clovis oncology , astellas pharma , incyte , uptodate , research to practice consulting or advisory role : janssen - ortho , bayer ag , guidepoint global , best doctors , uptodate , clovis oncology , research to practice , myovant sciences , incyte research funding : janssen - ortho ( inst ) , medivation ( inst ) , bayer ( inst ) , tokai pharmaceuticals ( inst ) travel , accommodations , expenses : medivation , janssen oncology , tokai pharmaceuticals , astellas pharma , incyte noah d . 
antonarakis honoraria : sanofi , dendreon , medivation , janssen biotech , essa pharma , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sanofi , dendreon , medivation , janssen biotech , essa pharma , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sanofi ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : coinventor of a biomarker technology that has been licensed to qiagen travel , accommodations , expenses : sanofi , dendreon , medivation heather h . 
carlo and wassim abida , memorial sloan - kettering cancer center ; himisha beltran , weill cornell medical center ; jacob vinson , prostate cancer clinical trials consortium , new york , ny ; veda n . 
stadler , university of chicago , chicago , il ; and mary - ellen taplin , dana - farber cancer institute , boston , ma . supported by the office of the assistant secretary of defense for health affairs , through the prostate cancer research program under awards no . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
pomerantz mm , spisk s , jia l , et al : the association between germline brca2 variants and sensitivity to platinum - based chemotherapy among men with metastatic prostate cancer . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
antonarakis es , lu c , luber b , et al : germline dna - repair gene mutations and outcomes in men with metastatic castration - resistant prostate cancer receiving first - line abiraterone and enzalutamide . 
isaacsson velho p , silberstein jl , markowski mc , et al : intraductal / ductal histology and lymphovascular invasion are associated with germline dna - repair gene mutations in prostate cancer . 
castro e , goh c , olmos d , et al : germline brca mutations are associated with higher risk of nodal involvement , distant metastasis , and poor survival outcomes in prostate cancer . 
castro e , goh c , leongamornlert d , et al : effect of brca mutations on metastatic relapse and cause - specific survival after radical treatment for localised prostate cancer . 
na r , zheng sl , han m , et al : germline mutations in atm and brca1 / 2 distinguish risk for lethal and indolent prostate cancer and are associated with early age at death . 
aarnio m , sankila r , pukkala e , et al : cancer risk in mutation carriers of dna - mismatch - repair hum mutat 34 : 490 - 497 , 2013 genes . 
mller p , seppl tt , bernstein i , et al : cancer risk and survival in path_mmr carriers by gene and gender up to 75 years of age : a report from the prospective lynch syndrome database . 
abida w , armenia j , gopalan a , et al : prospective genomic profiling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making . 
gillessen s , attard g , beer tm , et al : management of patients with advanced prostate cancer : the report of the advanced prostate cancer consensus conference apccc 2017 . 
cheng hh , klemfuss n , montgomery b , et al : a pilot study of clinical targeted next generation sequencing for prostate cancer : consequences for treatment and genetic counseling . 
abida w , armenia j , gopalan a , et al : prospective genomic profiling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making . 
hampel h , pearlman r , beightol m , et al : assessment of tumor sequencing as a replacement for lynch syndrome screening and current molecular tests for patients with colorectal cancer . 
hamilton jg , shuk e , genoff mc , et al : interest and attitudes of patients with advanced cancer with regard to secondary germline findings from tumor genomic profiling . 
hamilton jg , shuk e , garzon mg , et al : decision - making preferences about secondary germline findings that arise from tumor genomic profiling among patients with advanced cancers . 
colombo n , huang g , scambia g , et al : evaluation of a streamlined oncologist - led brca mutation testing and counseling model for patients with ovarian cancer . 
jones t , mccarthy am , kim y , et al : predictors of brca1 / 2 genetic testing among black women with breast cancer : a population - based study . 
levy de , byfield sd , comstock cb , et al : underutilization of brca1 / 2 testing to guide breast cancer treatment : black and hispanic women particularly at risk . 
allford a , qureshi n , barwell j , et al : what hinders minority ethnic access to cancer genetics services and what may help ? eur j hum genet 22 : 866 - 874 , 2014 46 . 
vadaparampil st , wideroff l , breen n , et al : the impact of acculturation on awareness of genetic testing for increased cancer risk among hispanics in the year 2000 national health interview survey . 
moses ka , orom h , brasel a , et al : racial / ethnic disparity in treatment for prostate cancer : does cancer severity matter ? urology 99 : 76 - 83 , 2017 53 . 
elrick a , ashida s , ivanovich j , et al : psychosocial and clinical factors associated with family communication of cancer genetic test results among women diagnosed with breast cancer at a young age . 
 pten promoter variants are not associated with common cancers : implications for multigene panel testing purpose pten mutations are associated with breast , colon , endometrial , kidney , and thyroid cancers . 
most pten promoter alterations , however , are characterized as variants of unknown significance , and their contribution to cancer risk is unclear . materials and methods personal and family histories of 88 , 333 patients undergoing pten analysis as part of multigene panel testing ( mgpt ) were retrospectively reviewed . 
individuals were categorized as positive for one or more mutations ( patho ) , without mutations but carrying one or more promoter variant ( prom ) , or negative for alterations ( wt )  . 
a subsequent study by teresi et al identified promoter variants in five patients with cancer but observed no differences in pten transcription or transcription factor binding compared with wild - type controls.8 the authors did report , however , that altered mrna folding patterns predicted for two of the variants correlated with inhibition of pten translation , suggesting a role for nontraditional regulatory mechanisms in cs pathogenesis . 
demographic , family history , and clinical information ( sex , age , self - reported ethnicity , personal cancer history , age at diagnosis , and breast cancer pathology ) were collected from test requisition forms and clinic notes provided by ordering clinicians . 
demographic and clinical information relevant to the condition for which genetic testing was ordered , and consent to participate in research that included pten sequencing , was obtained for these individuals . 
because the presence of pathogenic and / or likely pathogenic mutations in other known cancer genes ( data supplement ) may influence pten variant classification ( ie , co - occurrence ) , we further excluded such carriers ( n = 12 , 560 )  . 
given that patients may be referred for genetic testing because of family history of disease in the absence of personal history , we performed three sensitivity analyses , comparing cases to controls with no firstdegree relatives with the cancer of interest , controls without any family history of the cancer of table 1 . 
 interest , and an independent collection of research controls who initially underwent genetic testing for inherited disorders unrelated to cancer . age of diagnosis for each phenotype among the patho , prom , and wt groups were tested using wilcoxon rank sum tests . molecular analysis molecular methods have been previously described.9 briefly , genomic dna was isolated from blood or saliva and quantified . 
initial data processing and base calling , including extraction of cluster intensities , was performed using rta 1.17.21.3 ( real time analysis , hiseq control software , version 2.0.10 ; illumina , san diego , ca )  . 
sequence reads were aligned to reference human genome grch37 using novoalign , version 3.02.07 ( novocraft technologies , selangor , malaysia ) and variant calls generated using gatk , version 3.2.2 ( broad institute , cambridge , ma )  . 
30 was required for variant calling . variants were annotated with the ambry variant analyzer ( ambry genetics , aliso viejo , ca ) and their clinical significance assessed using ambrys five - tier classification framework10 , 11 on the basis of guidelines published by the american college of medical genetics and genomics.12 sanger sequencing was performed to check regions with no or insufficient coverage and confirm or clear all variant calls except those known to be benign or likely benign . statistical analysis for each phenotype , we performed case / control association analyses using multivariate logistic regression , adjusted for race / ethnicity , age at testing , sex , and type of multigene panel ordered , as appropriate . 
we present adjusted odds ratios and 95% cis for two mutually exclusive groups : pten mutation ( pathogenic and / or likely pathogenic ) carriers ( pathos ) , and individuals without pten mutations but carrying one or more pten promoter variant ( proms ) , compared with those in whom no alteration was detected ( wts )  . 
differences in median results among the 88 , 333 patients eligible for analysis , we examined 52 , 517 female breast cancer cases , 4 , 099 colorectal cancer cases , 1 , 569 uterine / endometrial cancer cases , 643 thyroid cancer cases , and 956 kidney cancer cases , and 28 , 549 controls with no personal cancer history ( table 1 )  . 
compared with controls , breast and uterine / endometrial cancer cases tended to be slightly older , whereas colorectal , thyroid , and kidney cancer cases were of similar age at the time of genetic testing ( data supplement )  . 
the distribution of race / ethnicity was also relatively similar among cases and controls . a total of 268 unique pten variants were included in analyses : 219 proms , all of which were classified as vus , and 49 pathogenic variants in the coding region ( data supplement )  . 
there were no significant differences in the age of onset of any cancer for proms compared with wts . discussion limited data have suggested that at least some pten promoter variants may be associated with cs and increased cancer risks , particularly for breast , thyroid , and uterine cancers . 
however , this evidence is insufficient for clinical assessment ofriskassociatedwithptenpromotervariation.we therefore examined associations between promoter variants and cancer risks in a large cohort of patients tested at a clinical diagnostic laboratory using mgpt that included pten . 
we observed no difference between carriers of pten promoter variants and those with no pten alterations in either ptenassociated cancer risk or median age of cancer diagnosis . these observations were based on a large sample of nearly 90 , 000 patients for whom detailed clinical and family history information were available , which allowed us to account for potential confounders and bias in our analyses . 
moreover , our target - enrichment , highly sensitive assay and robust sequencing methods ensured adequate capture of true variants with high specificity and sensitivity . despite our large - scale systematic approach , our study has some limitations . 
although the primary phenotype of interest was breast cancer , analyses of patho associations with most other cancer types were underpowered because of low sample size , and we lack adequate data for analysis of nonmalignant features . 
we did not observe any patho carriers among kidney cancer cases or research controls , and only two to four carriers each among those with thyroid , colorectal , and uterine / endometrial cancers . 
our sensitivity analyses restricting controls to those without family history of the cancer of interest yielded results similar to the primary analysis , and we were able to replicate our findings using a modest - sized , independent sample of controls not enriched for family history of cancer . 
however , we acknowledge that some bias may still be present , particularly for analyses of colorectal cancer , where we did not observe a significant association with pten gene - region mutations . incomplete data on polyps and other clinical factors among controls may have influenced our findings . 
last , we note that although we did not observe any significant effects of individual promoter variants , it is possible that additional rare variation exists in the promoter region beyond what has been currently detected , which could be associated with cancer . promotor regions are not sequenced for most genes analyzed by clinical laboratories because of insufficient data regarding the pathogenicity of such variants , yet many clinical laboratories in the united states include the promoter in pten sequencing . however , the vast majority of identified promoter variants are classified as vus , which provides no direction for clinical management of patients carrying these variants . 
given that 10 times as many prom as patho carriers were observed in this cohort , the number of affected patients as well as the time and effort spent on promoter variant classification is substantial . 
pilarski r , stephens ja , noss r , et al : predicting pten mutations : an evaluation of cowden syndrome and bannayan - riley - ruvalcaba syndrome clinical features . 
tan mh , mester j , peterson c , et al : a clinical scoring system for selection of patients for pten mutation testing is proposed on the basis of a prospective study of 3042 probands . 
zhou xp , waite ka , pilarski r , et al : germline pten promoter mutations and deletions in cowden / bannayanriley - ruvalcaba syndrome result in aberrant pten protein and dysregulation of the phosphoinositol - 3 - kinase / akt pathway . 
landrum mj , lee jm , benson m , et al : clinvar : public archive of interpretations of clinically relevant variants . nucleic acids res 44 : d862 - d868 , 2016 8 . 
laduca h , stuenkel aj , dolinsky js , et al : utilization of multigene panels in hereditary cancer predisposition testing : analysis of more than 2 , 000 patients . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
 novel pde10a - braf fusion with concomitant nf1 mutation identified in an undifferentiated sarcoma of infancy with sustained response to trametinib introduction childhood cancers are relatively rare entities ( approximately 140 per million among children < 15 years of age ) .1 malignant solid tumors that occur in infants ( < 1 year of age ) constitute a uniquely heterogeneous subgroup . 
in general , they are driven by acquisition of potent oncogenes , including chimeric gene fusions , such as the etv6 - ntrk3 rearrangement in infantile fibrosarcoma , or loss of tumor suppressor genes , such as rb1 in retinoblastoma or smarcb1 in rhabdoid tumors.2 - 4 in addition , it is estimated that approximately 10% of pediatric cancers carry a mutation in a cancer predisposing gene.5 , 6 tumor of the cns , infantile fibrosarcoma , rhabdoid tumors , and undifferentiated sarcoma are among the most frequently encountered tumor types in infancy.7 - 9 many of the undifferentiated tumors are often considered orphan diseases , given the absence of distinctive histopathologic hallmarks , the small size of patient cohorts , and until recently , a limited molecular classification.10 consequently , standard - of - care guidelines for treatment of these pediatric patients are not soundly established . 
 in the past decade , the list of oncogenic chimeric gene fusions in cancers has grown exponentially.11 next - generation sequencing of the whole - transcriptome ( or tumor rna sequencing [ rnaseq ] ) now enables identification of cytogenetically silent gene fusions , as well as single nucleotide variants . 
abnormal tissue uptake was not documented by [ 125i ] metaiodobenzylguanidine scintigraphy . the patient underwent a surgical biopsy , and pathologic analysis of the specimen revealed an undifferentiated malignant sarcoma . 
histopathologic analysis showed a neoplasm composed of stphanie vairy loubna jouan mlanie bilodeau virginie dormoyraclet patrick gendron franoise couture france lveill frdrique tihy emmanuelle lemyre dorothe bouron - dal soglio nada jabado claudia l . 
circled area shows the mass with extension into the sacral medullary canal and foramen and compression of the left iliac ve ( b ) histologic analysis of the neoplasm composed of undifferentiated tumor cells and sparse collagenous stroma . 
cytogenetic analyses displayed a complex karyotype with multiple aberrations , including several trisomies ( of chromosomes 3 , 8 , 11 , and 17 ) , monosomy x , a balanced translocation t ( 1 ; 12 ) , and a 7q terminal deletion ( fig 1c )  . 
analyses by fluorescent in situ hybridization demonstrated no rearrangements of ss18 ( synovial sarcoma ) , etv6 ( infantile fibrosarcoma ) , dux4 , and ccnb3 ( ewing - like sarcoma ) but confirmed a 7q deletion using an internal probe . 
overall , karyotype and fish studies did not reveal a chromosomal anomaly specifically associated with pediatric sarcomas . chemotherapy ( vincristine , actinomycin , and cyclophosphamide regimen ) was urgently initiated while awaiting the final pathology report . 
surgical resection was declined , given the high risk of morbid neurologic sequelae , and the child was closely followed . progression of the residual mass was documented 18 months after the end of chemotherapy . 
given that pediatric sarcomas are frequently associated with chimeric gene fusions , and in the absence of a precise molecular diagnosis for this patient , tumor rnaseq was performed to uncover putative cancer driver alterations , including gene rearrangements . 
rnaseq analysis performed on the diagnostic tumor sample revealed an in - frame fusion between pde10a ( 6q27 ) exon 3 and braf ( 7q34 ) exon 9 ( fig 2a ; table a1 )  . 
 chimeric product pde10a - braf was confirmed by reverse transcriptase polymerase chain reaction using complementary dna from the tumor and subsequent direct sanger sequencing ( figs 2b and 2c )  . 
the pde10a and braf gene breakpoints were corroborated by array comparative genomic hybridization analysis of the diagnostic sample , and these alterations were present in a high proportion of cells ( 80% ; data supplement )  . the transcriptomic data set was also mined to predict damaging nucleotide alterations in a list of 2 , 604 cancer - related genes ( data supplement )  . 
 a pde10a chr6 ( q27 ) braf chr7 ( q34 ) 8 9 10 11 12 ras binding domain s365 kinase domain 11 12 14 15 pde10a - braf kinase domain ladder 500 bp pde10a - braf ( 300 bp ) pde10a exon 3 braf exon 9 breakpoint fig 2 . 
 ( b ) validation by reverse transcriptase polymerase chain reaction performed on tumor rna ( expected product size of 300 bp ) , normal control , and no rna template . 
the patient did not present any clinical stigmata of neurofibromatosis and tested negative for germline nf1 mutations ( the patient was referred to clinical genetics , physical evaluation , and sanger sequencing of peripheral blood cell dna ) , suggesting a somatic deletion of nf1 in neoplasm cells . 
the patient was also tested for constitutional tp53 gene alterations , but no pathogenic mutation was detected . because both braf and nf1 play converging roles in activating the rasmitogen - activated protein kinase ( mapk ) signaling pathway ( fig 3a ) , we evaluated the phosphorylation status of erk1 / 2 protein using immunohistochemistry . 
on the basis of genomic profiling of the diagnostic tumor sample , rescue treatment with an mek inhibitor ( trametinib 0.025mg / kg , equivalent to the recommended adult dose , 17 was proposed to the family )  . 
this rearrangement accordingly preserves the raf kinase domain while disrupting the upstream inhibitory cr2 domain encoded by exon 8 , removing the regulatory s365 phosphorylation site required for signal inhibition.25 , 26 in parallel , nf1 is a tumor suppressor that negatively regulates ras pathway . 
given that fulllength protein is 2819 amino acids , heterozygous loss of function of nf1 is predicted , leading to a sustained activation of the mapk pathway through ras phosphorylation . 
we therefore postulate that as previously hypothesized in melanomas , 28 nf1 mutation and pde10a - braf gene fusion could both converge to activate downstream mapk pathway in tumor cells , and functional interactions should be explored in pediatric sarcomas . in sum , we report a novel pde10a - braf chimeric gene fusion and somatic nf1 p . ( tyr80serfs * 26 ) deletion identified using rna sequencing in an infant diagnosed with undifferentiated pelvic sarcoma . 
 pediatric relapsed soft tissue sarcomas generally have a poor response to second - line chemotherapy.29 , 30 some studies of advanced soft tissue sarcomas showed minimal or no response to mek inhibitor , but correlation with mapk pathway alterations is lacking.31 , 32 this report underscores the critical impact of deep sequencing technologies on the molecular classification and clinical management of infant tumors . 
multicenter clinical trials will be critical to determine the frequency of braf fusions in infantile undifferentiated sarcoma and to test the therapeutic benefit of incorporating mek inhibitors or other agents targeting mapk pathway signaling into the chemotherapy backbone for these tumors . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . franoise couture no relationship to disclose france lveill no relationship to disclose frdrique tihy no relationship to disclose emmanuelle lemyre no relationship to disclose dorothe bouron - dal soglio no relationship to disclose nada jabado no relationship to disclose claudia l . 
kleinman no relationship to disclose monia marzouki no relationship to disclose sonia cellot no relationship to disclose acknowledgment stphanie vairy no relationship to disclose loubna jouan no relationship to disclose mlanie bilodeau no relationship to disclose virginie dormoy - raclet no relationship to disclose we sincerely thank the patients and their families for their outstanding support , as well as members of the pediatric hematology - oncology team of centre hospitalier universitaire sainte - justine . 
 affiliations stphanie vairy , mlanie bilodeau , monia marzouki , and sonia cellot , charles - bruneau cancer center ; stphanie vairy , loubna jouan , mlanie bilodeau , franoise couture , france lveill , frdrique tihy , emmanuelle lemyre , dorothe bouron - dal soglio , monia marzouki , and sonia cellot , centre hospitalier universitaire sainte - justine ; patrick gendron , emmanuelle lemyre , dorothe bouron - dal soglio , monia marzouki , and sonia cellot , universit de montral ; nada jabado and claudia l . 
jackson em , sievert aj , gai x , et al : genomic analysis using high - density single nucleotide polymorphism - based oligonucleotide arrays and multiplex ligation - dependent probe amplification provides a comprehensive analysis of ini1 / smarcb1 in malignant rhabdoid tumors . 
orbach d , rey a , oberlin o , et al : soft tissue sarcoma or malignant mesenchymal tumors in the first year of life : experience of the international society of pediatric oncology ( siop ) malignant mesenchymal tumor committee . 
hayes - jordan aa , spunt sl , poquette ca , et al : nonrhabdomyosarcoma soft tissue sarcomas in children : is age at diagnosis an important variable ? j pediatr surg 35 : 948 - 953 , 2000 ; discussion 953 - 954 9 . 
bishop aj , mcdonald mw , chang al , et al : infant brain tumors : incidence , survival , and the role of radiation based on surveillance , epidemiology , and end results ( seer ) data . 
turski ml , vidwans sj , janku f , et al : genomically driven tumors and actionability across histologies : braf - mutant cancers as a paradigmol cancer ther 15 : 533 - 547 , 2016 14 . 
shukla n , ameur n , yilmaz i , et al : oncogene mutation profiling of pediatric solid tumors reveals significant subsets of embryonal rhabdomyosarcoma and neuroblastoma with mutated genes in growth signaling pathways . 
kao yc , fletcher cdm , alaggio r , et al : recurrent braf gene fusions in a subset of pediatric spindle cell sarcomas : expanding the genetic spectrum of tumors with overlapping features with infantile fibrosarcoma . 
matallanas d , birtwistle m , romano d , et al : raf family kinases : old dogs have learned new biol 16 : 281 - 298 , 2015 tricks . 
subbiah v , meyer c , zinner r , et al : phase ib / ii study of the safety and efficacy of combination therapy with multikinase vegf inhibitor pazopanib and mek inhibitor trametinib in advanced soft tissue sarcoma . 
dembla v , groisberg r , hess k , et al : outcomes of patients with sarcoma enrolled in clinical trials of pazopanib combined with histone deacetylase , mtor , her2 , or mek inhibitors . 
list of candidate fusion genes detected by rna sequencing gene 1 ( 5 end fusion partner ) coordinates ( 5 end ) coordinates ( 3 end ) gene 2 ( 3 end fusion partner ) pde10a chr6 : 165895802 ensg00000250859 chr5 : 126847434 ensg00000268750 chr19 : 58331312 ensg00000236537 chr6 : 158733082 akr1c6p chr10 : 4951797 tvp23c - cdrt4 chr17 : 15343598 ensg00000236537 chr6 : 158703294 loc100507412 chrun_gl000220 : 114339 atp6v1f chr1 : 1271794 chr17 : 18707578 mmab chr12 : 110006325 tvp23c - cdrt4 chr17 : 15341516 ensg00000146426 chr6 : 155182131 scaf8 gli3 chr7 : 42129309 loc100507412 clasp2 chr3 : 33686248 ensg00000174444 chr15 : 66795841 kansl1 kansl1 tulp4 akr1e2 tvp23b rpl19 tulp4 tmem126b arglu1 rpl27 dvl1 tvp23b ccnd2 styx rasal2 tcf7l2 nav2 crybg3 nap1l1 plekha5 znf517 epas1 dzip1l mdm4 uba2 chr17 : 44171925 chr17 : 44171925 chr6 : 158735299 chr10 : 4872866 chr17 : 18707578 chr17 : 37360967 chr6 : 158735299 chr11 : 85339650 chr13 : 107211929 chr17 : 41154962 chr12 : 4411895 chr14 : 53197246 chr1 : 178136886 chr10 : 114861983 chr11 : 19389080 chr3 : 97594908 chr12 : 76470081 chr12 : 19408057 chr8 : 146029800 chr2 : 46537949 chr3 : 137782099 chr1 : 204502515 chr19 : 34945628 no . 
 frequent molecular subtype switching and gene expression alterations in lung and pleural metastasis from luminal atype breast cancer max klebe , ms1 ; carlo fremd , md2 ; mark kriegsmann , md1 ; katharina kriegsmann , md3 ; thomas albrecht , md1 ; verena thewes , phd2 , 6 ; martina kirchner , phd1 ; pornpimol charoentong , phd2 , 6 ; nadine volk , phd1 , 2 ; johannes haag , md4 ; ralph wirtz , phd5 ; thordur oskarsson , phd6 ; alexandra schulz , ms1 ; j org heil , md7 ; andreas schneeweiss , md8 ; hauke winter , md4 ; and peter sinn , md1 purpose conversion of tumor subtype frequently occurs in the course of metastatic breast cancer but is a poorly understood phenomenon . 
in luma cancers , 62 genes were identied with differential expression in metastatic versus primary disease , compared with only 10 differentially expressed genes in lumb , human epidermal growth factor receptor 2 ( her2 ) enriched , and basal subtypes combined . gene expression changes in luma cancers affected not only the repression of the estrogen receptor pathway and cell cyclerelated genes but also the wnt pathway , proteinases ( mme , mmp11 ) , and motility - associated cytoskeletal proteins ( ck5 , ck14 , ck17 )  . 
this involved 83 notable gene expression changes . conclusion our results indicate that gene expression changes and subsequent subtype conversion occur on a large scale in metastatic luminal atype breast cancer compared with other molecular subtypes . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction visceral metastases often occur as late events in the course of metastatic breast cancer and are generally followed by a rapidly fatal outcome . 
we examined changes in pam50 gene signatures in a matched - pair series of 57 breast cancer primaries and corresponding lung or pleural metastases to determine the nature and extent of tumor subtype conversion . knowledge generated subtype conversion to pam50 luminal b subtype was observed in the majority of luminal atype breast cancers . 
only few cases of primary luminal b , human epidermal growth factor receptor 2enriched , and basal - like subtypes converted to another pam50 category in metastasis . relevance pam50 - based subtype classication of breast cancer lung and pleural metastases may be different than that seen in the primary tumor , especially in primary luminal a cancers . 
this change in pam50 classication between primary and metastatic disease may affect response to systemic therapy and must be investigated . other three subtypes by tissue microarray analysis , 7 and basal subtypes in particular were more frequent than expected.9 in this study , we included patients with invasive breast cancer of all molecular subtypes and metachronous breast cancer with lung or pleural metastasis ( bclpm ) to provide insights into the upand downregulation of genes during the course of the disease . 
therefore , we retrospectively examined gene expression proles in a wellcharacterized , prospectively assembled group of patients with breast cancer and metachronous lung or pleural metastasis ( data supplement 2 , fig s1 )  . 
exclusion criteria included no availability or insufciency of tumor tissue from pbc or bclpm tumor tissue ( n = 11 ) , primary lung cancer after review of patient records ( n = 2 ) , and low rna content or not meeting quality control criteria of rna data ( n = 11 )  . gene expression analysis for the selection of tumor tissue for rna extraction , ffpe tissue blocks from the pbc and metastatic lesions were selected after reviewing all original tissue slides and were recut for hematoxylin & eosin sections , to be used for reference and to determine tumor cell content ( tumor surface area )  . 
microdissection was performed in most cases to avoid normal breast tissue contamination . a minimum of approximately 50 ng of total rna was used . hybridization time per cartridge was 16 hours before measurement . rna expression analysis was performed by measuring a custom panel of 269 breast cancerrelated genes and 11 housekeeping genes ( data supplement 2 , table s2 ) , using the ncounter platform ( nanostring technologies , seattle ca ) according to the manufacturers instructions . 
the gene panel cludes 25 published gene signatures with prognostic or predictive properties in luminal - type breast cancer with the aim to determine their role in metastatic disease ( data supplement 2 , table s3 )  . 
the selection of gene signatures covered by this list of genes includes nine proliferationrelated signatures , four estrogen receptorrelated signatures , one immune - related signature , and 11 signatures related to cancer pathways . 
for gene function , david bioinformatics resources were used ( version 6.8 ) , 17 , 18 and functional annotation analysis in the biological process category and kegg pathway enrichment were computed . 
all statistical calculations , except gene function analysis , were done using r , version 3.6.1.20 additional information is available in data supplement 1 . results patient characteristics a total of 57 patients with bclpm were included in this study . 
pam50 molecular subtype conversion occurred in the majority of luminal atype pbc ( n = 16 ; 57.1% ) , evolving mostly into luminal btype or her2 - type metastasis ( table 1 ; fig 1b )  . 
gene expression clustering of bclpm was clearly different from pbc in the low - risk category but not with cancers of high - risk subtypes ( figs 2a - 2b )  . this indicates a similar tumor biology of bclpm and pbc for tumors of high - risk subtypes but a different biology in the low - risk ( luminal a ) category . 
by tnm classication luma lumb her2 basal ( range ) initial metastatic site before the treatment of metastatic breast cancer lung or pleural metastasis endocrine therapy at time of metastatic other unknown biopsy yes , tamoxifen yes , aromatase inhibitor yes , gnrha no . 
similarly , heatmap clustering conrmed separate luminal a clusters for primary tumors and metastases ( fig 3 )  . pgr was signicantly downregulated ( p = .0015 , wilcoxon rank - sum test ) , and mki67 was not signicantly increased ( data supplement 2 , fig s5 )  . differential gene expression analysis to characterize which genes are involved in the process of bclpm , differential gene expression analysis was performed . 
these included 3 cytoskeletal proteins ( krt14 , krt17 , krt5 ) , 2 matrix metalloproteinases ( mmp11 , mme ) , and ankrd30a . the latter is a breast differentiation gene that is frequently expressed in the breast and in receptor - positive breast cancer.22 other molecular changes in metastases were linked to proliferation ( cdc6 , ccnb1 , mki67 , top2a , aurkb , pttg1 ) , cell cycle checkpoints ( brca2 , bub1 , bub1b , chek1 ) , and epithelial - mesenchymal transition ( emt ) genes . 
among the genes most relevant for therapy in breast cancer ( esr1 , pgr , her2 , mki67 ) , the expressions of esr1 and her2 were unaffected in bclpm , but subtype - specic changes the pam50 subtypes of pbc showed marked variation with regard to the extent of differential gene expression of this gene panel in bclpm . 
the greatest number of differentially expressed genes was seen in luminal atype breast cancer , with 47 and 11 downand upregulated genes , respectively , compared with fewer expression changes in metastatic high - risk tumors ( luminal b , her2 - enriched , basal - like ) , with six and four downand upregulated genes , respectively ( figs 4a - 4b )  . 
only 1 gene was downregulated in bclpm that was her2 enriched , and no genes reached signicance after adjustment for multiple testing in the basal - like subtype , which in part may be attributed to the comparably small sample sizes of 6 and 7 , respectively ( data supplement 2 , table s6 )  . 
of the genes repressed in luminal a metastases , several are associated with emt . four of these ( twist2 , twist1 , zeb1 , tgfb3 ) are key regulators of emt . 
multidimensional scaling ( umap ) of gene expression , showing ( a ) gene expression in primary versus metastatic cancers , and ( b ) pam50 subtypes of the primary and metastatic tumors . 
for luminal a ( luma ) subtype , two subtype clusters can be distinguished , ( bottom ) one for primary breast cancers , and ( top ) the smaller one representing lung metastases . 
lumb , luminal b ; her2 , human epidermal growth factor rector 2enriched ; basal , basal - like ; normal , normal - like subtype . with bclpm ( figs 2a - 2b ) , and the magnitude and type of gene expression changes in lung metastasis ( table 1 )  . 
thirty - four and 49 genes were signicantly upand downregulated , respectively , in bclpm from luminal a cancers with subtype switch ( adjusted p , .05 ) compared with only 7 genes downregulated and none upregulated in the nonsubtype switch group ( figs 4c - 4d )  . 
in luminal a cancers , subtype switch affected cell cycle and cell proliferation genes ( mitotic cell cycle checkpoint , sister chromatid cohesion , mitotic nuclear division , cell division ) and the p53 - signaling as well as progesterone - signaling pathways ( data supplement 2 , figs 4a and 4b )  . clustering of gene expression in luminal atype cancers to better characterize the phenomenon of subtype conversion in luminal a cancers , we set up a logistic model for the assessment of differential gene expression with and without subtype conversion . 
in the group of 28 luminal asubtype tumors , a subtype conversion was more likely to occur when genes involved in certain growth factors , nuclear proteins , and signaling molecules were upregulated ( gnaz , hoxb13 , vegfa ) and some genes involved in immune response and inammation ( foxp3 , cd8a , cd68 , csf1r ) were downregulated ( fig 5a )  . 
this included 10 genes of various functions with downregulation in metastases and 52 genes , also of diverse functions , that were upregulated after subtype switch ( fig 5b )  . 
this upregulation of a substantial number of genes suggests a common mechanism of gene regulation that is involved in subtype switching . comparison of gene signatures in luminal a and btype cancers for additional insight into the classes of genes involved in subtype switching , a couple of well - characterized gene signatures for estrogen receptor signaling , tumor proliferation , and hallmarks of cancer were analyzed in bclpm ( data supplement 2 , figs s6a and s6b )  . 
interestingly , and despite the different genes involved in these signatures , all 4 tumor proliferation signatures tested showed similar patterns of gene expression in metastases derived from luminal atype tumors with and without subtype switch . 
 klebe et al subtype luminal a luminal b basal - like her2 - enriched normal - like site breast primary lung metastasis expression subtype site brca2 diaph3 chek2 ccne2 aurka bub1 mki67 rrm2 cenpa exo1 mybl2 cep55 plk1 pttg1 cdc6 top2a tyms hif1a flvcr2 cd44 rragd uchl1 scrg1 qsox2 oxct1 krt7 cd24 fgfr4 phgdh cdca7 adgrg6 prkcb pim2 ptgds zeb2 tp53 il17rb rbbp8 krt5 krt14 krt17 tspyl5 elf5 vgll1 prom1 sfrp1 mmp12 mmp9 igfbp5 cxcl14 abl1 zeb1 twist2 twist1 snai2 aldh1a1 slc2a3 csnk1d fam213b fzr1 bbc3 rassf7 plau mmp11 tgfb3 ankrd30a tmem45b pik3ca col4a2 cdc42bpa gstm1 esm1 csnk1e znf703 ccnd1 ebf4 esr1 thsd4 tbc1d9 gata3 cxxc5 ca12 tff1 tff3 foxa1 spdef krt18 pak1 blvra cdk7 stk32b bcl2 stc2 greb1 mapt scube2 igf1r slc39a6 siah2 krt19 cldn4 ddr1 azgp1 fig 3 . 
tumors are discriminated according to their molecular subtype , with separation of metastatic luminal a tumors from primary luminal a cancers ( shown as blue bars across top )  . 
different patterns of gene expression changes are observed , with ( a ) signicantly more changes in the luminal a subtype compared with ( b ) high - risk tumors ( lumb , human epidermal growth factor receptor 2 ( her2 ) enriched , basal - like )  . 
within the luminal a subtype , gene expression changes were mostly conned to ( c ) tumors with subtype switch in lung metastasis compared with ( d ) nonswitched metastases . intrinsic tumor subtype as subtype conversion or subtype switch.26 our results indicate that evolution within cancer cell populations during metastasis leads to more transcriptomic and phenotypic changes than might be expected from the acquisition of genetic events . 
 molecular subtype switching in luminal atype breast cancer the pam50 subtype , subtype conversion only partly reects the changes occurring in tumor evolution , and our data indicate that , even the molecular without change of phenotype may still be different in the metastasis , especially in low - grade tumors . 
in multidimensional scaling , tumors of luminal a subtype in bclpm form a different cluster than luminal a subtype in the primary ( fig 2 ) , and , in the differential expression heatmap , they cluster with more aggressive subtypes ( fig 3 )  . 
along that line , relevant gene expression changes in brain metastases were found without change of pam50 subtype.28 when pam50 subtype conversion occurs , it can be regarded as an indicator of genetic remodeling in metastasis and as a risk factor of additional disease progression . 
of note , although estrogen receptor and her2 statuses as predictive clinical markers remained unchanged in this group , the proliferation rate greatly increased , and breast hormone receptor signaling declined . 
as such , although therapeutically relevant markers were unaltered upon subtype switch , remarkable changes occurred that are generally associated with a worsened malignant behavior and prognostic impact . the metastatic tumor cell the gene expression changes that were evident across all subtypes included evidence for increased mobility and invasive behavior of through downregulation of cytokeratins ( krt5 / 14 ) 29 ; tumor activation through downregulation of mmp1130 , 31 ; and deactivation of estrogen receptordependent pathways , as indicated by the downregulation of the progesterone receptor and the ankyrin repeat - domain gene ( ankrd30a )  . conversely , genes involved in emt and growth signaling were upregulated in all molecular subtypes ( data supplement 2 , fig s3 )  . 
as far as datasets are comparable , most changes found in bclpm have been reported to occur also in other metastatic sites , 27 , 32 with the exception of her2 , which was demonstrated to be upregulated in the brain28 ; however , it was not in our dataset . luminal a cancers undergoing a subtype switch were characterized by a much higher variability in gene expression in bclpm compared with high - risk carcinomas . this variability affected various molecular pathways . 
from gene expression data alone , it appears not possible to name a common denominator for the changes in metastasis of luminal a cancers that affected several dozens of genes . 
when trying to dissect the alterations that occur in subtype conversion , we found that primary tumors with low expression of inammation - related genes but increased expression of growth signalingassociated genes were more likely to undergo subtype conversion . 
in the metastatic tumor cell , the subtype switch was characterized by quite extensive gene expression changes of various molecular pathways , similar to the nding of important gene expression changes in  . 
100 genes in brain metastasis.29 no hypothesis about the root cause of changes for subtype conversion can be put forward , but the manifold changes of expression status in bclpm from luminal a cancers do indicate a major reprogramming of the tumor cell . limitations of this study include the use of a curated gene list . 
last but not least , although the discrimination of patients with breast cancer into specic cancer subtypes is a widely applied clinical concept with profound prognostic implications , luminal a and b cancers may much more represent a continuum rather than true distinct subtypes from a biologic point of view . in conclusion , we have shown that luminal atype breast cancer is most affected by subtype conversion and differential gene expression in matched metastases to lung or pleura involving but not limited to estrogen receptor signaling ( downregulation ) and tumor proliferation ( upregulation )  . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . carlo fremd honoraria : roche , pzer , celgene , astrazeneca , amgen consulting or advisory role : roche , pzer travel , accommodations , expenses : celgene , roche ralph wirtz employment : stratifyer molecular pathology gmbh stock and other ownership interests : stratifyer molecular pathology gmbh consulting or advisory role : janssen oncology ( inst ) , biontech ag ( inst ) research funding : janssen research & development ( inst ) patents , royalties , other intellectual property : royalties from biontech ( inst ) ; royalties from qiagen ( inst ) thordur oskarsson stock and other ownership interests : neovasc , cyclacel pharmaceuticals , windtree therapeutics , enzon pharmaceuticals patents , royalties , other intellectual property : migrastatins and uses thereof . 
description : the present invention provides compounds , pharmaceutically acceptable compositions thereof , and methods of using the same . other relationship : genentech j org heil honoraria : roche , siemens healthcare diagnostics , bard consulting or advisory role : roche , siemens healthcare diagnostics research funding : bard travel , accommodations , expenses : celgene andreas schneeweiss honoraria : roche pharma ag , celgene , astrazeneca , pzer , novartis , msd oncology , lilly , tesaro research funding : roche pharma ag ( inst ) , celgene ( inst ) , abbvie , molecular partners expert testimony : roche , astrazeneca travel , accommodations , expenses : roche , celgene hauke winter expert testimony : astrazeneca travel , accommodations , expenses : astrazeneca peter sinn honoraria : nanostring technologies , roche pharma ag research funding : roche pharma ag travel , accommodations , expenses : nanostring technologies no other potential conicts of interest were reported . references vanharanta s , massagu e j : origins of metastatic traits . 
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thompson am , jordan lb , quinlan p , et al : prospective comparison of switches in biomarker status between primary and recurrent breast cancer : the breast recurrence in tissues study ( brits )  . 
at resistance depends on activation of bypass pathways or development of secondary mutations in the driver oncogene.2 , 3 oncogenic fusions involving the ros1 gene are detected in approximately 1% to 2% of patients with nsclc and the majority of cases occur in tumors of adenocarcinoma histology.4 they are generated by the fusion of the 3 ( cid : 1 ) end of the ros1 gene containing the tyrosine kinase with a variety of partner genes , including gopc , slc34a2 , cd74 , tpm3 , sdc4 , ezr , lrig3 , kdelr2 , ccdc6 , among others.4 ros1 fusions function as primary oncogenic drivers following the oncogene addiction model.4 indeed , inhibition of ros1 with the small molecule tyrosine kinase inhibitor ( tki ) crizotinib induced durable responses in 72% of the patients with an ros1 - positive nsclc in the profile - 1001 study ( clinicaltrials.gov identier : nct00585195 ) , 5 leading to approval of crizotinib by regulatory agencies for this patient population . 
other tkis , including ceritinib , 6 lorlatinib , 7 and entrectinib , 8 have shown activity in this patient population as the eld evolves . our understanding of the landscape of resistance mechanisms for ros1 - positive nsclc is still evolving . although several tki options currently exist for patients with alk - positive nsclc and secondary alk mutations , effective tkis are limited for the ros1 - positive lung cancer population in the postcrizotinib setting.9 , 10 importantly , the molecular mechanisms of resistance are variable , which poses a barrier for the study of different drugs or drug combinations in molecularly dened cohorts of progressing patients in the form of clinical trials . 
here , we describe an unusual case of a ros1 - positive patient who developed a ros1 f2004v secondary mutation and whose cancer progressed in the brain and bone sites after 34 months of treatment with entrectinib , followed by dramatic response to lorlatinib . 
an ophthalmologic examination revealed a right amelanotic perifoveal choroidal tumor . subsequent evaluation with positron emission tomography / computed tomography scanning conrmed metastatic disease with multiple left lung nodules , left hilar lymphadenopathy , and bone lesions . 
interestingly , choroidal metastases have been reported in a number of cases of alk11 , 12 or other oncogene - driven lung cancer.13the patient was treated with radiation therapy to the metastatic lesion in the right eye , followed by rst - line crizotinib . 
the patient was initially treated at the recommended phase ii dose of 600 mg orally once daily for the rst eight 28 - day cycles , but she experienced asymptomatic progression in multiple , small brain metastases , which led to a decision to escalate the dose to 800 mg orally once daily , resulting in decrease in disease burden in the braafter another 18 cycles of entrectinib , an increase in the size of the brain lesions was noted . 
magnetic resonance images of brain ( t1 axial postcontrast series ) ( a ) before and ( b ) 1 month after treatment with lorlatinib , showing signiresponse of all cant metastatic brain lesions . progression in the brain developed with concomitant progression in osseous metastases . at the time of brain and bone progression , a secondary ros1 f2004v mutation was detected via circulating cellfree dna testing using a commercial next - generation sequencing assay . 
at that time , the patient was removed from the startrk - 1 study and therapy was begun with brigatinib , a compound approved for the treatment of lung cancers with alk fusions15 but also with activity against ros1.16 , 17 in addition , radiation of a metastatic choroidal lesion diagnosis with metastatic cd74 - ros1positive lung cancer entrectinib dose escalation ( 800 mg ) sar to progressing brain lesions progression in the brain and bones progression in the brain progression in the brain progression in the brain and bones crizotinib months entrectinib months brigatinib x1 month lorlatinib x6 months ( ongoing ) radiation to thoracic spine lesions detection of ros1 f2004v secondary mutation ( cfdna ) treatment x10 days fig 2 . 
secondary mutations in ros1 fusions reported in in vitro experiments in the literature and differential sensitivity to drugs with known ros1 activity . the numbers in the boxes correspond to the average concentration ( cave ) for the drug in steady state in patients , divided by the drug ic50 values calculated in ba / f3 cells expressing the mutant ros1 molecules . 
repotrectinib is another potent ros1 inhibitor with activity against many of these secondary mutations ; it is not shown in the gure because the rp2d is not known yet for this drug.29 cave values were calculated as the ratio of the area under the curve for 0 to 24 hours to 24 hours of the drug at steady state in patients.35 , 36 secondary mutations that have been reported in clinical cases are highlighted in red and the ros1 f2004v mutation described clinically for the rst time in this report is highlighted in purple . 
 ( * ) these alk mutations also are found in neuroblastoma . brigatinib had activity against cd74 - ros1 with f2004l in vitro.18 the patient also underwent radiation therapy for several thoracic spine progressing lesions . 
disease remains in control 6 months later , while the patient continues receiving lorlatinib ( fig 2 )  . although , to our knowledge , the ros1 f2004v has not been described before in patients , it is analogous to the alk f1174l mutation described in patients with neuroblastoma19 and confers paradoxic apoptosis to ba / f3 cells , a result of excessive oncogenic signaling through ros1 and p38mapk.20 also , a secondary f1174v mutation has been described in alk - positive lung cancer with resistance to crizotinib.21 instead , ba / f3 cells expressing ros1 f2004v low - dose ros1 inhibitor.20 survive in the presence of however , the patient in this report did not respond to withdrawal of brigatinib , and symptoms , namely headaches , developed from brain metastases . 
given that the concept of tki addiction is suggested in preclinical models only , 23 - 25 the approach of tki withdrawal cannot be recommended unless there is additional clinical validation . the molecular spectrum of secondary resistance to crizotinib and other ros1 inhibitors in ros1 fusionpositive patients with lung cancer is not yet well established . 
the two largest published cohorts include 16 patients from massachusetts general hospital26 and 12 patients from the university of colorado.27 in the massachusetts general hospital cohort , nine of 16 patients had a ros1 secondary mutation identied at the time of progression . 
seven of these patients harbored the g2032r mutation and none had the f2004v mutation . conversely , a ros1 compound secondary mutation ( l2026m / l1951r ) was identied in one of 12 patients in the university of colorado cohort . 
in addition , in this cohort , there was also activation of the her2 axis , an activating kit d816g mutation and a ctnnb1 s45f mutation , each case a possible mechanism of resistance to ros1 inhibition . 
figure 3 summarizes the in vitro10 , 16 , 20 , 28 - 33 and clinical10 , 27 , 30 , 34 data of ros1 secondary mutations reported in the literature . molecular testing during the course of treatment with a targeted therapy often identies molecular mechanisms of resistance to the inhibition of the driver oncogene.1 in the best - characterized cases of secondary resistance , there are data from large cohorts of patients and available effective tkis , as is the case with egfr t790m secondary mutation . nevertheless , predicting response to a tki in the presence of a secondary mutation in the driver oncogene might rely on less extensive clinical data or on preclinical data only . patient - derived cell lines , 27 ba / f3 cells engineered to express and depend on the driver oncogene of interest with and without the secondary mutation , 10 and xenograft tumors in mice29 serve as resistance models in many of these scenarios . 
in vitro development of resistance in cell - line models is possible by exposure to increasing doses of tkis for several months.37 alternatively , brief exposure to the mutagen n - ethyl - n - nitrosourea , followed by drug screening , can select for resistant clones.20 , 28 finally , it is possible for a clinician to encounter a case of resistance for which molecular testing might identify resistance mechanisms not described before . 
reports of such n of 1 cases , including outcomes , is an important resource that can guide treatment of cases with rare acquired resistance mutations . in conclusion , we show that ros1 f2004v secondary mutation confers resistance to entrectinib and brigatinib , and possibly other ros1 inhibitors , but is sensitive to lorlatinib . 
ou stock and other ownership interests : turning point therapeutics honoraria : pzer , roche pharma ag , roche , ariad / takeda , astrazeneca , foundation medicine , merck consulting or advisory role : pzer , roche , astrazeneca , takeda , foundation medicine , turning point therapeutics , ignyta speakers bureau : genentech , astrazeneca , takeda research funding : pzer ( inst ) , roche pharma ag ( inst ) , astrazeneca / medimmune ( inst ) , astrazeneca ( inst ) , ariad ( inst ) , ignyta ( inst ) , astellas pharma ( inst ) , chugai pharma ( inst ) , revolution medicines ( inst ) robert c . 
 lorlatinib for ros1 - positive lung cancer with f2004v mutation acknowledgment lorlatinib was obtained by the pzer expanded access program ( clinicaltrials.gov identier : nct03178071 )  . references pakkala s , ramalingam ss : personalized therapy for lung cancer : striking a moving target . 
jci insight 3 : e120858 , 2018 pao w , miller va , politi ka , et al : acquired resistance of lung adenocarcinomas to getinib or erlotinib is associated with a second mutation in the egfr kinase domaplos med 2 : e73 , 2005 turke ab , zejnullahu k , wu yl , et al : preexistence and clonal selection of met amplication in egfr mutant nsclc . 
clin cancer res 19 : 4040 - 4045 , 2013 shaw at , ou sh , bang yj , et al : crizotinib in ros1 - rearranged non - small - cell lung cancer . 
n engl j med 371 : 1963 - 1971 , 2014 lim sm , kim hr , lee js , et al : open - label , multicenter , phase ii study of ceritinib in patients with non - small - cell lung cancer harboring ros1 rearrangement . j clin oncol 35 : 2613 - 2618 , 2017 shaw at , felip e , bauer tm , et al : lorlatinib in non - small - cell lung cancer with alk or ros1 rearrangement : an international , multicentre , open - label , singlearm rst - in - man phase 1 trial . 
lancet oncol 18 : 1590 - 1599 , 2017 drilon a , siena s , ou si , et al : safety and antitumor activity of the multitargeted pan - trk , ros1 , and alk inhibitor entrectinib : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . 
facchinetti f , loriot y , kuo ms , et al : crizotinib - resistant ros1 mutations reveal a predictive kinase inhibitor sensitivity model for ros1and alk - rearranged lung cancers . 
clin cancer res 22 : 5983 - 5991 , 2016 jiang k , brownstein s , sekhon hs , et al : ocular metastasis of lung adenocarcinoma with elm4 - alk translocation : a case report with a review of the literature . saudi j ophthalmol 27 : 187 - 192 , 2013 12 . 
weickhardt aj , scheier b , burke jm , et al : local ablative therapy of oligoprogressive disease prolongs disease control by tyrosine kinase inhibitors in oncogeneaddicted non - small - cell lung cancer . 
gettinger sn , bazhenova la , langer cj , et al : activity and safety of brigatinib in alk - rearranged non - small - cell lung cancer and other malignancies : a singlearm , open - label , phase 1 / 2 trial . 
anjum r , vodala s , kohlmann a , et al : an in vitro mutagenesis screen identies l1951r and g2032r as drug - resistant mutants of cd74 - ros1 . 
debruyne dn , bhatnagar n , sharma b , et al : alk inhibitor resistance in alk ( f1174l ) - driven neuroblastoma is associated with axl activation and induction of 20 . 
suda k , tomizawa k , osada h , et al : conversion from the oncogene addiction to drug addiction by intensive inhibition of the egfr and met in lung cancer with activating egfr mutation . 
gainor jf , tseng d , yoda s , et al : patterns of metastatic spread and mechanisms of resistance to crizotinib in ros1 - positive non - small - cell lung cancer . 
drilon a , ou si , cho bc , et al : repotrectinib ( tpx - 0005 ) is a next - generation ros1 / trk / alk inhibitor that potently inhibits ros1 / trk / alk solvent - front 30 . 
song a , kim tm , kim dw , et al : molecular changes associated with acquired resistance to crizotinib in ros1 - rearranged non - small cell lung cancer . 
zou hy , li q , engstrom ld , et al : pf - 06463922 is a potent and selective next - generation ros1 / alk inhibitor capable of blocking crizotinib - resistant ros1 mutations . 
lacy s , nielsen j , yang b , et al : population exposure - response analysis of cabozantinib efcacy and safety endpoints in patients with renal cell carcinoma . cancer chemother pharmacol 81 : 1061 - 1070 , 2018 36 . 
zhang s , anjum r , squillace r , et al : the potent alk inhibitor brigatinib ( ap26113 ) overcomes mechanisms of resistance to rstand second - generation alk inhibitors in preclinical models . 
nelson - taylor sk , le at , yoo m , et al : resistance to ret - inhibition in ret - rearranged nsclc is mediated by reactivation of ras / mapk signaling . 
 phase i study of the braf inhibitor vemurafenib in combination with the mammalian target of rapamycin inhibitor everolimus in patients with braf - mutated malignancies vivek subbiah shiraj sen kenneth r . 
are co - first authors and contributed equally to this work . the funders had no role in the design of the study ; the collection , analysis , and interpretation of the data ; the writing of the article ; and the decision to submit the article for publication . corresponding author : vivek subbiah , md , department of investigational cancer therapeutics ( phase i clinical trials program ) , unit ( continued ) purpose parallel activation of the phosphatidylinositol 3 - kinasemammalian target of rapamycin pathway represents a mechanism of primary and acquired resistance to braf - targeted therapy , but the two pathways have yet to be cotargeted in humans . 
we performed a phase i study to evaluate the safety and activity of the braf inhibitor vemurafenib in combination with the mammalian target of rapamycin inhibitor everolimus in braf - mutated advanced solid tumors . patients and methods we performed a 3 + 3 dose - escalation study with escalating doses of both oral ( po ) vemurafenib administered twice a day and po everolimus administered daily . results twenty patients with advanced cancers were enrolled . 
 patients were heavily pretreated with prior braf or mek inhibitors ( n = 11 ) , phase i clinical trial therapy ( n = 10 ) , surgery ( n = 18 ) , radiation therapy ( n = 11 ) , and chemotherapy ( n = 13 )  . 
one of the two pediatric patients initially experienced grade 3 rash , but after dermatologic intervention , the patient remains on trial with partial response and no dose reduction at time of analysis . 
one pediatric patient with pleomorphic xanthroastrocytoma remains on protocol with continued clinical response after 38 cycles . conclusion the combination of vemurafenib 720 mg po twice a day and everolimus 5 mg po daily is safe and well tolerated and has activity across histologies , with partial responses noted in advanced nonsmall - cell lung cancer , melanoma , optic nerve glioma , and xanthroastrocytoma , including patients who previously experienced progression on braf and / or mek inhibitor therapy . 
a recent basket study of vemurafenib demonstrated clinical activity in patients with advanced nonmelanoma cancers.8 unfortunately , many patients exhibited primary and acquired resistance to therapy . reactivation of mapk signaling and activation of alternative parallel signaling pathways such as the phosphatidylinositol 3 - kinase ( pi3k ) mammalian target of rapamycin ( mtor ) pathway have been hypothesized to contribute to primary and acquired resistance to braf - targeted therapy.9 , 10 specifically , akt mutation , 9 pten deficiency , 11 and downstream mtor activation have been implicated in resistance to both vemurafenib and dabrafenib in metastatic melanoma , both clinically and in preclinical models.12 , 13 preclinical studies have demonstrated efficacy in dual targeting of both the mapk and pi3kmtor pathways in various tumor types.14 , 15 we also recently identified a strong association between co - occurring pi3k - mtor pathway aberrations and primary resistance to braf targeted therapy . 
all patients were treated at the clinical center for targeted therapy at the university of texas md anderson cancer center from september 2013 to august 2015 and met all the eligibility criteria . 
patients who had a myocardial infarction within 3 months before starting treatment , who were pregnant or breastfeeding , or who had undergone a major surgical procedure within 28 days were excluded . 
palliative radiation therapy was allowed during the study treatment . study design and treatment this study was a nonrandomized , open - label , standard 3 + 3 dose - escalation study of oral ( po ) vemurafenib , starting at a dose of 720 mg daily , and po everolimus , starting at a dose of 5 mg daily , for 28 days . 
the primary objectives were to determine the safety , mtd , and dose - limiting toxicity ( dlt ) of the combination of vemurafenib and everolimus in patients with braf - mutated advanced cancer . 
 two pediatric patients were enrolled onto this study and were treated with vemurafenib po 480 mg daily and everolimus po 2.5 mg daily , per body surface areabased dose adjustment . if a patient experienced new grade 3 or greater toxicity , treatment was withheld until the condition was addressed and it recovered to grade 1 or baseline . 
the patients continued treatment until they experienced disease progression or intolerable toxicities , until the treating physician or patient felt that it was not in the patients best interest to continue for any reason , or until consent was withdrawn for any other reason . all patients were evaluated for dlts during the first 28 days and evaluated in clinic every 28 days before initiation of each subsequent cycle . 
dlts were treatment - related grade 3 or 4 nonhematologic toxicities , as defined by the national cancer institute common terminology criteria for adverse events version 3.0 , or grade 4 hematologic toxicities lasting > 7 days or accompanied by fever or bleeding during the first 4 weeks of therapy . 
clinical laboratory improvement amendments ( clia ) certified next generation sequencing data were collected for each patient . response to therapy was assessed using response evaluation criteria in solid tumors ( recist ) version 1.1. 
median time to disease progression and os duration were determined using the kaplan - meier method . circulating tumor dna three patients agreed to have an optional blood draw to measure circulating tumor dna ( ctdna ) at baseline and at each restaging . 
at least 8 ng of unamplified cell - free dna were tested with a droplet digital polymerase chain reaction brafv600e mutationspecific assay and / or multiplex brafv600 screening kit ( bio - rad , hercules , ca ) to distinguish the wild - type allele from the three most common mutations ( brafv600e , brafv600k , and brafv600r ) using the qx200 droplet digital pcr system ( bio - rad ) according to the manufacturers standard protocol . 
planned dose schedule in patients who received the combination of vemurafenib and everolimus in a phase i study dose level vemurafenib orally twice a day ( mg ) everolimus orally once a day ( mg ) * body surface area - based dose adjustment was made ( level 1 ) for pediatric patients dose level 1 was the recommended phase ii dose . frequency for the multiplexed screening assay and < 0.1% mutant allele frequency per single well for the mutation - specific assays . results patient characteristics the demographics and clinical characteristics of the 20 patients who received at least one dose of vemurafenib and everolimus and completed the dlt window are listed in table 2 . 
the most common tumor types were melanoma ( n = 7 ) , glioma ( n = 5 ) , and thyroid cancer ( n = 4 ) , and one patient each had appendiceal cancer , colorectal cancer , nsclc , and unknown primary cancer . 
patients were heavily pretreated with prior therapies , including braf or mek inhibitor therapy ( n = 11 ) , prior phase i clinical trial therapy ( n = 10 ) , surgery ( n = 18 ) , radiotherapy ( n = 11 ) , and chemotherapy ( n = 13 )  . 
one patient had measurable disease but not evaluable disease , and a second patient was not evaluable as a result of withdrawing consent before the first restaging , but both patients cleared the toxicity window and therefore are included in the toxicity evaluation but not in the response evaluation . safety all 20 patients were evaluated for dlts . 
 five patients ( 25% ) had everolimus dose reductions throughout their therapy as a result of toxicity , and one patient had the vemurafenib dose reduced as a result of renal insufficiency . 
two patients without dlts withdrew consent before disease progression . response of the 18 patients evaluable for response , 11 patients ( 61% ) had objective tumor volume reduction as best response . 
two patients were not evaluable for response ; one patient had measurable but not evaluable disease and a second patient completed the dlt window but withdrew consent before restaging . prs were seen in patients with nsclc , melanoma , optic nerve glioma , and pleomorphic xanthroastrocytoma . 
of the nine patients who had disease progression on braf or mek inhibitors before enrolling onto this study , two ( 22% ) had prs and five ( 56% ) had stable disease with vemurafenib and everolimus . at the time of analysis , 14 patients ( 78% ) had discontinued therapy because of disease progression . 
 ( b ) representative restaging images of a patient with metastatic melanoma and a pten ( p95s ) mutation who had a partial response on vemurafenib and everolimus after disease progression on vemurafenib and px866 , an investigational pi3k inhibitor . 
astro , anaplastic astrocytoma ; at , anaplastic thyroid ; crc , colorectal cancer ; cup , cancer of unknown primary ; glio , glioblastoma ; glioma , optic nerve glioma ; mel , melanoma ; pt , papillary thyroid . prior braf or mek inhibitor use no prior braf or mek inhibitor use still on trial without progression pleomorphic xanthroastrocytoma remains on protocol with continued clinical response after 38 cycles . genomic profiling all evaluable patients underwent clia - certified clinical next - generation sequencing of at least 50 genes before trial enrollment . 
among the four patients who achieved pr , a patient with metastatic melanoma who had previously experienced progression on vemurafenib plus an investigational pi3k inhibitor ( px866 ) had a concurrent pten ( p95s ) mutation . 
a patient with nsclc whose tumor harbored an idh1 ( r132c ) mutation , arid2 alteration ( splice site 92 + 1 g > a ) , and ppp1r2a mutation ( r183w ) achieved a pr after previously experiencing progression on dabrafenib . 
all concurrent molecular aberrations and best response to therapy for each patient are listed in table 4 . circulating tumor dna patients enrolled onto this study were offered an optional blood draw to measure ctdna throughout the course of the study . 
 a third patient with a brafv600e mutation had detectable ctdna levels , which were measured at four time points throughout therapy and are depicted in figure 2 alongside the patients scans . 
dlts included fatigue ( 20% ) and rash ( 15% ) , but both were present in only one patient at the mtd and recommended phase ii dose of vemurafenib 720 mg twice daily and everolimus 5 mg daily . 
 the patient with glioblastoma who experienced a grade 3 rash had a resolution of his rash after initial everolimus discontinuation and was able to resume everolimus at a dose of 2.5 mg daily without toxicity . 
 the use of nonpharmacologic approaches , such as physical and mindfulness - based exercise therapy , 20 , 21 and pharmacologic approaches , such as corticosteroids22 in treating cancerand therapy related fatigue , has recently demonstrated efficacy in randomized controlled trials and may benefit these patients moving forward . we observed only one metabolic adverse event ( hypertriglyceridemia and hyperglycemia ) , which is attributed to mtor inhibitors . 
overall , most patients at the recommended phase ii dose tolerated the treatment well . our trial also demonstrates that the addition of an mtor inhibitor to everolimus treatment is able to overcome resistance to braf and / or mek inhibition in a subset of patients with braf - mutant advanced cancers . 
graphical depiction of a patients circulating tumor dna level of brafv600e ( shown as copies per milliliter of plasma ) while on treatment with vemurafenib plus everolimus with representative restaging scans and response to therapy , per response evaluation criteria in solid tumors ( recist ) 1.1. 
pd , progression of disease ; pr , partial response . baseline baseline july 16 , 2014 october 14 , 2014 november 12 , 2014 december 10 , 2014 the 20 patients in this study had a pr to therapy . 
 next - generation sequencing performed at the time of initial diagnosis revealed idh1 ( r132c ) , arid2 ( splice site 92 + 1 g > a ) , and ppp1r2a ( r183w ) aberrations . 
unfortunately , no molecular profiling was available at the time the patient experienced progression on dabrafenib immediately before enrolling onto this trial . a second patient with metastatic melanoma and a pten ( p95s ) mutation who had recently had disease progression on vemurafenib and px866 , an investigational pi3k inhibitor , also achieved a pr on our trial ( fig 1b )  . 
in vivo , pten - deficient , braf - mutated mouse models treated with vemurafenib and pi3k inhibitors also demonstrate synergistic antitumor activity.23 interestingly , this patient experienced progression on the vemurafenib and investigational pi3k inhibitor combination but responded with a pr to vemurafenib and everolimus . 
a 78 - year - old patient with metastatic papillary thyroid cancer whose tumor harbored a pik3ca ( h1047r ) mutation had 7 months of stable disease with a 27% reduction in tumor burden before having any disease progression . 
both of these patients had no co occurring genomic alterations identified on their tumors other than the brafv600e mutation , illustrating the fact that although co - occurring alterations may lead to activation of parallel signaling pathways that increase resistance to therapy in some patients , they may render other tumors susceptible to therapy when actionable . we have previously reported our institutions experience with implementing multiplex hotspot testing and the need to enroll patients onto genotype - matched trials when feasible.24 a number of the responders on this trial further support the hypothesis that the identification of actionable alterations can help guide the right patient to the right targeted therapy . 
all nonresponders were either previously treated with braf or mek inhibitor or harbored non - v600 braf mutations . in the patient with metastatic melanoma with measurable ctdna , the level of mutated brafv600e copies per milliliter decreased with clinical response and increased before subsequent restaging that demonstrated disease progression . 
previous studies have identified an association between detection and levels of circulating tumor dna and disease burden and survival across braf and mek inhibitor trials.27 it is plausible that this may explain why only wildtype braf was detectable in the plasma of these two patients . vitro data suggest that the combination of mek and mtor inhibition may be more effective than braf and mtor inhibition in activating bax and caspase - 3 and inducing caspase - dependent apoptosis in melanoma cell lines.31 future studies to investigate the safety and effectiveness of combining everolimus with both braf and mek inhibitors together are being planned . our study has several limitations , including a small patient population and the variety of molecular profiling platforms used . 
although all patients underwent clia - certified next generation sequencing of at least 40 genes , including those in the pi3k - mtor pathway , some patients underwent more extensive 400gene profiling . 
ideally , all patients should have a broader panel of testing to identify all actionable aberrations , both at the time of study initiation and at disease progression , to better understand the clonal evolution of tumors treated with vemurafenib and everolimus . 
 sherman , patrick hwu manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors in conclusion , the combination of vemurafenib and everolimus is safe and well tolerated and has clinical activity across histologies , with prs noted in patients with advanced nsclc , melanoma , optic nerve glioma , and xanthroastrocytoma . 
our results do not support the addition of everolimus based solely on alterations in the pi3k - mtor pathway ; however , given the responders who did harbor concurrent mutations in this pathway , further investigation in a larger cohort of molecularly matched patients with uniform genomic profiling is warranted . 
hess no relationship to disclose filip janku stock and other ownership interests : trovagene consulting or advisory role : deciphera , trovagene , novartis , sequenom , foundation medicine , guardant health , immunome research funding : novartis , biomed valley discoveries , roche , agios , astellas pharma , deciphera , symphony evolution , plexxikon , piqur , fujifilm other relationship : bio - rad david s . 
hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack , bayer consulting or advisory role : baxter , bayer , guidepoint global , janssen speakers ' bureau : genentech , janssen oncology research funding : novartis , genentech , eisai , astrazeneca , pfizer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer , bristol - myers squibb , genmab , ignyta , infinity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo , medimmune , molecular templates , takeda travel , accommodations , expenses : loxo , mirna therapeutics other relationship : oncorena , eisai soumen khatua no relationship to disclose research funding : phosplatin therapeutics travel , accommodations , expenses : phosplatin therapeutics javier munoz consulting or advisory role : kite pharma , pfizer , pharmacyclics , bayer , alexion pharmaceuticals , bristolmyers squibb , janssen , seattle genetics , gilead sciences , kyowa hakko kirin speakers ' bureau : kite pharma gerald s . 
falchook employment : sarah cannon research institute , healthone research funding : millennium , emd serono , celgene , medimmune , genmab , vegenics , novartis , astrazeneca , incyte , armo biosciences , kolltan pharmaceuticals , 3 - v biosciences , abbvie , aileron therapeutics , delmar pharmaceuticals , effector therapeutics , strategia therapeutics , fujifilm , hutchison medipharma , regeneron , biothera , curegenix , curis , eli lilly , jounce therapeutics , oncomed , precision oncology , syndax , taiho pharmaceutical , tesaro , takeda , beigene , ignyta , merck , rgenix , tarveda therapeutics , tocagen patents , royalties , other intellectual property : handbook of targeted cancer therapy travel , accommodations , expenses : millennium , sarah cannon research institute , emd serono , bristol - myers squibb roman groisberg no relationship to disclose apostolia m . 
tsimberidou consulting or advisory role : roche research funding : emd serono ( inst ) , baxter ( inst ) , foundation medicine ( inst ) , onyx ( inst ) , bayer ( inst ) , boston biomedical ( inst ) , placon ( inst ) , immatics ( inst ) , karus therapeutics ( inst ) , stem cells ( inst ) , obi pharma ( inst ) steven i . 
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penna i , molla a , grazia g , et al : primary cross - resistance to brafv600e - , mek1 / 2and pi3k / mtor - specific inhibitors in braf - mutant melanoma cells counteracted by dual pathway blockade . 
 clinical utility of clia - grade ar - v7 testing in patients with metastatic castration - resistant prostate cancer purpose a splice variant of the androgen receptor , ar - v7 , confers resistance to ar - targeted therapies ( atts ) but not taxane chemotherapies in patients with metastatic castrationresistant prostate cancer . 
since august 2015 , a clinical - grade assay to detect ar - v7 messenger rna expression in circulating tumors cells ( ctcs ) has been available to providers through a clinical laboratory improvement amendmentscertified laboratory at johns hopkins university . methods we contacted ordering providers of the first 150 consecutive tests by using a questionnaire - based survey to determine how the results of ar - v7 testing were used to influence clinical practice . results in all , 142 ( 95% ) of 150 questionnaires were completed by 38 providers from 29 sites across the united states and canada . 
prevalence of ar - v7 detection increased with prior exposure to atts ( abiraterone and enzalutamide nave , 22% ; after abiraterone or enzalutamide , 35% ; after abiraterone and enzalutamide , 43% )  . 
2017 by american society of clinical oncology introduction metastatic castration - resistant prostate cancer ( mcrpc ) remains dependent on androgen receptor ( ar ) signaling for survival in the presence low testosterone levels.1 two novel artargeted therapies ( atts ) , abiraterone and enzalutamide , induced high objective response rates and improved overall survival in patients with mcrpc.2 , 3 treatment with abiraterone or enzalutamide in the prechemotherapy setting led to a 50% decline in prostate - specific antigen ( psa50 ) response in 62% and 78% of these patients , respectively.2 , 3 however , sequential use of abiraterone and enzalutamide has resulted in much lower psa response rates with the use of the second att agent ( ie , abiraterone after enzalutamide , 10% to 15% ; enzalutamide after abiraterone , 20% to 30% ) .4 - 6 these data underscore the importance of identifying a predictive biomarker of resistance to att to prevent the use of subsequent futile therapy . potential mechanisms of resistance to att include ar amplification and mutation , as well as the expression of arsplicevariants.7a well - characterized mark c . 
eisenberger jun luo emmanuel s . antonarakis author affiliations and support information ( if applicable ) appear at the end of this article . the content is solely the responsibility of the authors and does not necessarily represent the official views of the national cancer institute or the national institutes of health . corresponding author : emmanuel s . 
 splice variant , ar - v7 , is a truncated form of fulllength ar ( ar - fl ) that lacks the ligand - binding domain but retains both the transactivation and dna - binding domains , allowing for constitutive ar signaling in the absence of androgen.8 - 10 in patients with mcrpc , detection of ar - v7 in circulating tumors cells ( ctcs ) was shown to predict resistance to novel atts.11 - 13 moreover , ar - v7 + patients had a significantly shorter overall survival , suggesting a prognostic value of ar - v7 in addition to its use as a predictive biomarker.11 , 13 chemotherapy is an alternative to att for arv7 + patients with mcrpc . 
detection of ar - v7 has been shown not to preclude response to taxanebased chemotherapy.14 , 15 further prospective investigation found a significant survival benefit with the use of taxanes versus atts in patients with ar - v7 + disease.16 interestingly , the presence of this splice variant is a dynamic feature with possible conversion from ar - v7 + to ar - v7 status after chemotherapy with taxanes.14 , 17 these data suggest that serial arv7 testing may guide the clinical treatment of patients with mcrpc . 
those patients with ar - v7 prostate cancer may continue to benefit from att , whereas chemotherapy may be more effective in patients with detectable ar - v7 transcript.18 if the clinical utility of ar - v7 testing can be confirmed , it may also have an economic benefit . in a recent study , we modeled the cost of treating all patients with mcrpc with abiraterone or enzalutamide versus using ar - v7 testing to direct treatment.19 by using a clinical scenario in which ar - v7 + patients were changed from treatment with abiraterone and / or enzalutamide to chemotherapy thus avoiding the cost of futile att therapy , ar - v7 testing resulted in a theoretical cost savings to the health care system of $150 million per year . 
to this end , since august 2015 , clinicalgrade ar - v7 testing performed in a clinical laboratory improvement amendments ( clia ) certified laboratory at johns hopkins university has been available to health care providers for clinical use.20 however , despite the commercial availability of this ar - v7 test , its clinical utility is unknown . 
here , we have retrospectively compiled questionnaire - based data on how ordering providers are applying the results of ar - v7 testing in their clinical practice to influence decision making . methods the analytical validation and test characteristics of our clia - grade ar - v7 assay have been described previously.20 our molecular pathology database was queried for all ar - v7 tests ordered by internal and external providers for clinical purposes . 
clinical results of this test were reported as ctc , ctc + / ar - v7 , or ctc + / ar - v7 + , because each of these categories is associated with different outcomes.12 a clinical utility questionnaire ( data supplement ) was generated for each ar - v7 test ordered and was mailed or e - mailed to each ordering provider . we defined a biomarker - based change in treatment as a confirmation of treatment choice or a change from one therapy to another after ar - v7 testing . 
the institutional review board at johns hopkins university approved this study and granted a waiver of consent to contact the provider of each ar - v7 test ordered because that was considered a clinical audit . 
the ordering provider was then contacted for participation and asked to complete a questionnaire pertaining to treatment decisions that were made on the basis of results of that specific ar - v7 test . 
if a provider did not wish to participate or the questionnaire was not returned after two attempts to contact the provider , data for that patient were not included in the analysis . one hundred fifty consecutive ar - v7 clinical test results were obtained between august 31 , 2015 , and august 31 , 2016 , representing the first 150 tests ordered . 
from these , 142 questionnaires ( 95% ) were completed and returned by 38 providers across 29 sites ( 28 in the united states [ in 22 states ] and one in canada )  . 
the significance level was set at p , .05 , and corrections were not performed for multiple comparisons . results information from 142 of 150 questionnaires sent ( 95% participant response rate ) were included in this analysis . 
the number of lines of additional systemic therapies for mcrpc among these patients was reported as follows : 24% ( n = 33 ) had received no other lines , 27% ( n = 39 ) had received one line , 27% ( n = 39 ) had received two lines , 13% ( n = 18 ) had received three lines , and 9% ( n = 13 ) had received four or more lines of systemic therapy before testing . 
of tests abiraterone enzalutamide abiraterone or enzalutamide abiraterone enzalutamide nave test result ctc 40 / 142 28.17 ctc + / ar - v7 42 / 142 29.58 8 / 40 20.0 11 / 40 27.5 21 / 40 52.5 8 / 42 19.0 20 / 42 47.62 14 / 42 33.33 ctc + / ar - v7 + 60 / 142 42.25 26 / 60 43.33 21 / 60 35.0 13 / 60 21.66 abbreviations : ar - v7 , androgen receptor splice variant 7 ; att , ar - targeted therapy ; ctc , circulating tumor cell ; n / n , number of patients in that category divided by total number of patients . overall , the prevalence of a ctc result was 28% , the prevalence of a ctc + / ar - v7 result was 30% , and the prevalence of a ctc + / ar - v7 + result was 42% . 
patients who were treated with abiraterone and / or enzalutamide resulted in a higher prevalence of ar - v7 detection compared with patients who were not treated with an att : 22% of treatment - nave patients were ar - v7 + ; after treatment with abiraterone or enzalutamide , 35% of patients were ar - v7 + ; and after treatment with abiraterone and enzalutamide , 43% of patients were ar - v7 +  . to assess the clinical utility of ar - v7 testing , providers were asked whether the ar - v7 status influenced their decision making . 
the majority of ar - v7 tests ( ctc or ctc + / ar - v7 ) did not change the clinical practice of the providers ( table 2 )  . 
however , almost two thirds ( 62% ) of ar - v7 + tests resulted in a change in management . in patients for whom treatment was changed , providers were then asked to specify the type of therapy selected on the basis of the test result . 
patients with an ar - v7 result ( ctc or ctc + / ar - v7 ) were preferentially treated with an att agent ( confirmed ar treatment , or changed from taxane to ar therapy )  . 
conversely , after an ar - v7 + result , most patients were changed from an att agent to taxane chemotherapy ( 43% ) or were enrolled in a clinical trial ( 43% )  . 
psa50 rr data were missing from 16% ( n = 12 ) and 22% ( n = 15 ) of questionnaires in which management was changed or not changed , respectively . we also investigated which systemic therapy was used in patients with mcrpc after progression on both abiraterone and enzalutamide , according to ar - v7 status ( table 5 )  . 
by contrast , ar - v7 + patients who had already received abiraterone and enzalutamide were more often treated on a clinical trial ( 54% ) compared with treatment using chemotherapy ( 19% )  . 
in the patients who were treated with docetaxel , those who were ar - v7 were commonly treated with standard chemotherapy ( ie , cabazitaxel ; 67% [ six of nine ] ) whereas ar - v7 + patients were more frequently placed on a clinical trial ( 58% [ 11 of 19 ] )  . finally , we examined provider treatment preferences for ar - v7 + patients irrespective of the prior therapies received ( table 6 )  . 
a minority of patients ( 7% ) received either enzalutamide or abiraterone despite an ar - v7 + result , whereas all ar - v7 + patients managed with observation ( 10% ) enrolled in hospice shortly thereafter . to summarize the data compiled from providers real - world experience with ar - v7 testing , we propose a hypothetical treatment algorithm for making decisions regarding patients with mcrpc using ar - v7 as a potential treatment - selection biomarker ( fig 1 )  . 
after first - line systemic therapy with abiraterone or enzalutamide , ar - v7 + patients would preferentially cross over to taxane - based therapy , whereas those who are ar - v7 may continue on a second att . 
because of occasional conversions from ar - v7 + to ar - v7 status , men progressing on taxane treatment can be retested and could potentially consider treatment with an att if the ar - v7 status reverts to negative . 
finally , even patients progressing after treatment with abiraterone and enzalutamide may be considered for ar - v7 testing if an ar - v7directed clinical trial is available . discussion the optimal sequencing of therapeutic agents in patients with mcrpc is unknown and remains a major challenge . 
to this end , the national comprehensive cancer network prostate cancer guidelines now suggest that ar - v7 testing can be considered and may play a role in guiding therapy selection in mcrpc , but at this time , these guidelines have not gone as far as recommending testing to determine treatment choice . 
in another recent consensus report , the majority of prostate cancer specialists polled ( 59% ) stated that ar - v7 testing would be useful for some ( majority or minority of ) patients with mcrpc.21 although further prospective validation of the predictive ability of ar - v7 is currently ongoing , here we investigated the clinical utility of ar - v7 testing in a real - world setting . we asked providers whether the result of the arv7 test influenced their clinical practice for that specific patient . 
although our findings are retrospective , they suggest that ar - v7 testing may possibly lead to improved clinical responses to treatment , at least in terms of psa50 rr . 
we did not assess for radiographic progression - free or overall survival , which may not have correlated with psa50 rr . the statistically significant psa50 rr difference between the change and no - change groups is largely driven by the ar - v7 + subgroup ( described in appendix table a3 )  . 
ar - v7 + patients for whom management did not change had a psa50 rr of 5% ( v 39% in ar - v71 patients for whom treatment was changed )  . 
we hypothesize that ar - v7 + patients in the change group were more commonly treated with chemotherapy compared with the no - change group , resulting in improved outcomes . 
we also acknowledge a high psa50 rr in ar - v7 + patients treated with chemotherapy and ar - v7 patients treated with att ( both in the change group )  . 
nonetheless , these data suggest that further prospective investigation is warranted to study biomarker - driven clinical outcomes . by using the treatment history captured by our questionnaires , we were able to observe an increasing prevalence of ar - v7 detection with prior exposure to atts , as expected . 
this finding is corroborated by the recent biomarker data from the armor3 - sv ( a study of galeterone compared with enzalutamide in men expressing androgen receptor splice variant - 7 mrna [ ar - v7 ] metastatic crpc ) trial , in which first - line patients with mcrpc who had previously received docetaxel for metastatic hormone - sensitive disease had a higher prevalence of ar - v7 detection compared with chemotherapy - nave patients.22 moreover , 79% of men with newly developed mcrpc had prior exposure to bicalutamide . 
the higher trend of ar - v7 + tests after treatment with docetaxel or bicalutamide , in the absence of a novel att , may suggest that total number of therapies ( ie , more advanced disease ) contributes to ar - v7 expression in addition to the known relationship with prior att exposure . 
another provocative hypothesis might be that docetaxel works as an ar - modulating therapy in prostate cancer , inhibiting microtubule - dependent nuclear transport of wild - type ar but not ar - v7 , thereby selecting for the emergence of ar - v7expressing clones during or after chemotherapy treatment . this study had some additional limitations . 
first , the prevalence of ar - v7 was probably overestimated compared with earlier reports because providers were more likely to order a test if the clinical scenario suggested that the test might be positive . other significant weaknesses of this analysis were its retrospective nature and reliance on selfreporting by providers . 
an audit of 14 randomly selected questionnaires determined that providers gave accurate responses to the questionnaire in most instances ( see appendix ) , suggesting that our data represent the true clinical course for each patient . 
finally , we concede that many patients will receive all atts approved by the us food and drug administration , regardless of ar - v7 status , because clinical responses to atts are sometimes observed in arv7 + patients.13 however , the clinical utility of arv7 testing may potentially be clearest in ar - v7 + patients who have additional atts still available for treatment . 
by identifying high - risk patients ( ie , arv7 + ) who have adequate performance status earlier in their mcrpc treatment , this would allow them to be treated with taxane therapy before the chemotherapy window closes . 
potential decision algorithm based on serial androgen receptor splice variant 7 ( ar - v7 ) testing across the castration - resistant prostate cancer landscape . after each line of therapy , we propose an algorithm for consideration of ar - v7 testing . 
after abiraterone and enzalutamide treatment , patients should be subject to ar - v7 testing only if an ar - v7directed clinical trial is available . ( * ) indicates limited clinical data supporting the use of atts in ar - v7 + patients that subsequently convert to ar - v7 . 
 ( ) denotes a clinical trial that does not require a positive ar - v7 test for ar - v7 patients , whereas ar - v7 + patients should consider an arv7directed trial , if available . first - line therapy clinical ar - v7 testing ? second - line therapy clinical ar - v7 testing ? third - line therapy abiraterone enzalutamide consider ar - v7directed clinical trial / taxane docetaxel taxane / trial enzalutamide abiraterone consider ar - v7directed clinical trial / taxane receive either chemotherapy or atts at their physicians discretion . we propose a decision algorithm using serial arv7 testing across the mcrpc landscape . 
this algorithm is based largely on published data suggesting that the presence of ar - v7 confers resistance to atts but does not influence response to taxane chemotherapy.11 , 13 , 14 , 16 we note that at this time , there is no clinical trial evidence to support the use of atts in ar - v7 + patients who convert to ar - v7 status after chemotherapy . 
in our study , 17 of 22 ar - v7 + patients were enrolled on a clinical trial that mandated ar - v7 detection as an entry criterion , suggesting that many of the tests in this study were ordered for the purpose of screening for a clinical trial . 
finally , there is ongoing debate in the prostate cancer community about whether ar - v7 detection is merely a proxy for ar amplification or overexpression and not an independent predictor of response to therapy or clinical outcomes.21 although several studies have shown that ar - v7 detection is indeed correlated with ar - fl expression , ar - v7 still remains independently prognostic in multivariable analysis after controlling for ar - fl levels.11 , 13 , 23 in conclusion , to our knowledge , this is the first study to examine the preliminary real - world clinical utility of clia - grade ar - v7 testing in patients with mcrpc . 
we show that ar - v7 testing influenced clinical decision making overall ( regardless of test results ) but that its utility was greatest in the setting of ar - v7 + results . 
 jun luo honoraria : gilead sciences , sanofi consulting or advisory role : tokai pharmaceuticals , sun pharmaceutical industries , janssen oncology research funding : sanofi ( inst ) , orion pharma ( inst ) , mirati therapeutics ( inst ) , gilead sciences ( inst ) , astellas pharma ( inst ) patents , royalties , other intellectual property : co - inventor of an ar - v7 biomarker technology assigned to johns hopkins university who licensed to tokai pharmaceuticals ; co - inventor of a technology licensed to qiagen emmanuel s . 
antonarakis honoraria : sanofi , dendreon , medivation , janssen biotech , essa , astellas pharma consulting or advisory role : sanofi , dendreon , medivation , janssen biotech , essa , astellas pharma research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sanofi ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) travel , accommodations , expenses : sanofi , dendreon , medivation mark c . 
w81xwh - 15 - 2 - 0050 and w81xwh - 12 - 1 - 0605 ( j.l. ) , johns hopkins prostate specialized programs of research excellence grant p50 ca058236 ( j.l. ) , the patrick c . 
beer tm , armstrong aj , rathkopf de , et al : enzalutamide in metastatic prostate cancer before chemotherapy . n engl j med 368 : 138 - 148 , 2013 n engl j med 371 : 424 - 433 , 2014 4 . 
maughan bl , luber b , nadal r , et al : comparing sequencing of abiraterone and enzalutamide in men with metastatic castration - resistant prostate cancer : a retrospective study . 
dehm sm , schmidt lj , heemers hv , et al : splicing of a novel androgen receptor exon generates a constitutively active androgen receptor that mediates prostate cancer therapy resistance . 
hu r , dunn ta , wei s , et al : ligand - independent androgen receptor variants derived from splicing of cryptic exons signify hormone - refractory prostate cancer . 
antonarakis es , lu c , wang h , et al : ar - v7 and resistance to enzalutamide and abiraterone in prostate cancer . n engl j med 371 : 1028 - 1038 , 2014 12 . 
antonarakis es , lu c , luber b , et al : clinical significance of androgen receptor splice variant - 7 mrna detection in circulating tumor cells of men with metastatic castration - resistant prostate cancer treated with firstand second - line abiraterone and enzalutamide . 
antonarakis es , lu c , luber b , et al : androgen receptor splice variant 7 and efficacy of taxane chemotherapy in patients with metastatic castration - resistant prostate cancer . 
onstenk w , sieuwerts am , kraan j , et al : efficacy of cabazitaxel in castration - resistant prostate cancer is independent of the presence of ar - v7 in circulating tumor cells . 
scher hi , lu d , schreiber na , et al : association of ar - v7 on circulating tumor cells as a treatment - specific biomarker with outcomes and survival in castration - resistant prostate cancer . 
sprenger c , uo t , plymate s : androgen receptor splice variant v7 ( ar - v7 ) in circulating tumor cells : a coming of age for ar splice variants ? ann oncol 26 : 1805 - 1807 , 2015 19 . 
markowski mc , frick kd , eshleman jr , et al : cost - savings analysis of ar - v7 testing in patients with metastatic castration - resistant prostate cancer eligible for treatment with abiraterone or enzalutamide . 
lokhandwala pm , riel sl , haley l , et al : analytical validation of androgen receptor splice variant 7 detection in a clinical laboratory improvement amendments ( clia ) laboratory setting . 
gillessen s , attard g , beer tm , et al : management of patients with advanced prostate cancer : the report of the advanced prostate cancer consensus conference apccc 2017 . 
taplin me , antonarakis es , ferrante kj , et al : clinical factors associated with ar - v7 detection in armor3 - sv , a randomized trial of galeterone ( gal ) vs enzalutamide ( enz ) in men with ar - v7 + metastatic castration - resistant prostate cancer ( mcrpc )  . 
silberstein j , luber b , wang h , et al : clinical significance of ar mrna quantification from circulating tumor cells ( ctcs ) in men with metastatic castration - resistant prostate cancer ( mcrpc ) treated with abiraterone ( abi ) or enzalutamide ( enza )  . 
j clin oncol 35 , 2017 ( suppl ; abstr 132 ) we further queried our database to investigate the difference in the 50% decline in prostate - specific antigen ( psa50 ) response rate ( rr ) between the change and no - change groups on the basis of androgen receptor splice variant 7 ( ar - v7 ) status . 
for patients with ar - v7 + disease , the psa50 rr in those who did not change therapy was 5.3% ( one of 19 ) compared with 38.7% ( 12 of 31 ) in the change group ( table a3 )  . 
in the ar - v72 patients , the psa50 rr was 45.45% ( 15 of 33 ) in the no - change group versus 68.88% ( 22 of 32 ) in the change group . 
within both the ar - v7 + and ar - v7 groups , there was no discernible difference in number of lines of therapy between the change and no - change group . 
we also examined psa50 rr by treatment choice in those patients who had a change in treatment ( these data were not solicited for patients who did not have a treatment change in the questionnaire )  . 
in the 14 questionnaires audited , we found two minor discrepancies : ( 1 ) bicalutamide was listed in error as a prior therapy ( one time ) , and ( 2 ) the correct clinical trial was misidentified for a patient ( one time )  . subjective responses ( ie , clinical helpfulness and change in management ) were not assessed . 
the authors stated that there are currently no trials of parp inhibitors in endometrial carcinoma , mainly because mutations in brip1 , brca1 , brca2 , and other homologous recombination ( hr ) related genes are too rare , being reported overall in , 5% of cases.2 in fact , the french group gineco ( groupe dinvestigateurs nationaux pour letude des cancers ovariens ) is conducting a national randomized phase ii trial evaluating olaparib as maintenance therapy in platinumsensitive advanced uterine carcinoma ( utola trial ; clinicaltrials.gov identier : nct03745950 ; fig 1 ) versus placebo . 
we anticipate that patients with endometrial tumors might benet from a parp inhibitor , even in cases of no brca or related genetic mutations . the hr - decient ( hrd ) phenotype was initially characterized in approximately 50% of high - grade serous ovarian carcinomas , and 20% to 25% of these had no brca1 or brca2 mutations.3 importantly , this phenotype is associated with clinical activity of platinum and parp inhibitors in platinumsensitive ovarian carcinomas regardless of brca mutations.4 , 5 according to the cancer genome atlas data , the hrd phenotype was also recently reported in 25% of uterine endometrial carcinomas.6 it is almost exclusively found in the serous - like , tp53 - mutated subtype , in which it represents nearly 50% of cases.7 molecular alterations responsible for the hrd phenotype in endometrial carcinoma have not been largely explored and remain to be identied , because brca1 promoter methylation seems uncommon.7 finally , hr deciency could be induced by platinum - based chemotherapy ; a recent study showed decreased expression of rad51 protein , a key partner of hr , after neoadjuvant chemotherapy in a subset of patients with ovarian cancer.8 in tp53 wild - type endometrioid carcinoma , common molecular alterations such as pten or arid1a loss have been also associated in vitro with signicant parp inhibitor activity.9 , 10 according to these preliminary data , inclusion criteria in the utola trial are not restricted to specic molecular alterations ; rather , patients could be enrolled if their disease is platinum sensitive , a well - recognized landmark of the hrd phenotype . 
patients are stratied according to mrr and tp53 immuno - phenotypes , and a large screening of molecular alterations , including hrd prole , will be conducted to determine the best candidates for parp inhibitor maintenance . in conclusion , we agree with nakamura et al1 that parp inhibitors should be explored in patients with advanced endometrial carcinoma , beyond those with rare mutations in brca or related genes . 
the secondary end points are overall survival , response rate , quality of life , safety , time from random assignment to rst and second subsequent therapies , and time from random assignment to second disease progression or death . 
exploratory analyses included homologous recombinationdecient ( hrd ) phenotype and multiple - gene next - generation sequencing , including brca1 and brca2 and other hrd - related genes ( tp53 , pten , pole , and arid1a ) , and microsatellite instability status . 
nature 474 : 609 - 615 , 2011 [ erratum : nature 490 : 298 , 2012 ] ray - coquard i , pautier p , pignata s , et al : olaparib plus bevacizumab as rstline maintenance in ovarian cancer . 
marquard am , eklund ac , joshi t , et al : pan - cancer analysis of genomic scar signatures associated with homologous recombination deciency suggests novel indications for existing cancer drugs . 
biomark res 3 : 9 , 2015 de jonge mm , auguste a , van wijk lm , et al : frequent homologous recombination deciency in high - grade endometrial carcinomas . 
clin cancer res 25 : 1087 - 1097 , 2019 kubelac p , genestie c , auguste a , et al : changes in dna damage response markers with treatment in advanced ovarian cancer . 
cancers ( basel ) 12 : 707 - 719 , 2020 dedes kj , wetterskog d , mendes - pereira am , et al : pten deciency in endometrioid endometrial adenocarcinomas predicts sensitivity to parp inhibitors . 
 systemic and cns activity of selective ret inhibition with selpercatinib ( loxo - 292 ) in a patient with ret - mutant medullary thyroid cancer with extensive cns metastases alexander andreev - drakhlin , md1 ; maria cabanillas , md1 ; behrang amini , md , phd1 ; and vivek subbiah , md1 introduction medullary thyroid cancer ( mtc ) is a neuroendocrine tumor that originates from the parafollicular cells ( or c cells ) of the thyroid gland and accounts for 1% to 2% of thyroid cancers in the united states.1 the cns is a rare site of metastasis in mtc , with , 15 cases reported in the medical literature ; however , the prevalence may be underreported because of the infrequent use of cns imaging in patients with mtc.1 , 2 the optimal treatment approach for patients with mtc with cns involvement is currently unknown . 
although surgical resection , radiation therapy , or stereotactic radiosurgery ( srs ) may improve local disease control in some patients , most still succumb to their disease within months after the diagnosis of cns metastases.1 - 4 the proto - oncogene ret ( rearranged during transfection ) , located on chromosome 10q11.2 , is central to development of a majority of cases of mtc.5 germline gain - of - function ret point mutations result in multiple endocrine neoplasia 2 , a hereditary syndrome associated with mtc and pheochromacytoma.6 , 7 similar somatic mutations occur in approximately 50% of sporadic mtc , approximately 20% of sporadic pheochromocytomas , and rarely in other cancer types.8 - 10 recent identication of highly potent and selective ret inhibitors holds great promise in the management of these ret - driven cancers as well as other ret - altered malignancies.11 - 14 in 2018 , selpercatinib ( loxo - 292 ) received us food and drug administration breakthrough therapy designation for treatment of patients with previously treated metastatic ret - mutant mtc , ret fusion - positive nonsmall - cell lung cancer , and ret fusionpositive thyroid cancers . 
durable intracranial responses with selpercatinib have been described in patients with brain metastases with ret fusionpositive lung and thyroid cancers.15 , 17 however , the activity of selpercatinib in patients with ret - mutant mtc with brain metastases and / or leptomeningeal disease ( lmd ) has not been characterized , to our knowledge . 
here , we describe a patient with ret m918tmutant mtc with extensive cns metastases who had a clinically meaningful durable response to selective ret inhibition with selpercatinib . case report total a 67 - year - old woman presented to a local hospital with bilateral neck swelling . 
positron emission tomography imaging showed metabolically active , left - side , level v lymph nodes ; a 1.1 - cm , hypermetabolic , right lower lobe lung nodule ; several hypermetabolic liver lesions ; as well as lytic lesions in the c5 vertebral body , l4 left lamina , and left posterior iliac wing . 
magnetic resonance imaging ( mri ) of the brain revealed a 4 - mm lesion in the right caudate nucleus . the patient presented to the university of texas md anderson cancer center for a second opinion . 
she was then treated with standard - of - care cabozantinib but experienced multiple adverse effects , including handand - foot syndrome , mucositis , weight loss , nausea , and diarrhea , requiring several dose reductions ultimately to 40 mg daily . 
 ( a ) magnetic resonance imaging ( mri ) oblique axial cerebellar images of the patients metastatic brain disease ( left panel ) before and ( right panel ) 8 weeks after the patient initiated treatment with selpercatinib . 
 ( c ) mri axial cerebellar and ( d ) sagittal thoracic spine images of the patients metastatic disease ( left panels ) before and ( right panels ) 33 weeks after the patient initiated treatment with selpercatinib . 
 ( e ) mri axial brain images demonstrating a new caudate lesion after 17 months of therapy with selpercatinib ( left panel ) before and ( right panel ) after stereotactic radiosurgery ( srs )  . 
 andreev - drakhlin et al given the absence of any remaining standard therapies with established benet , the patient enrolled in a phase i / ii study of selpercatinib in patients with advanced solid tumors ( libretto - 001 ; clinicaltrials.gov identier : nct03157128 )  . the patient provided written informed consent before enrollment . 
baseline imaging at the time of the treatment initiation with selpercatinib revealed bilateral central and lateral neck disease ; lytic lesions in the c5 , t4 , t8 , l1 vertebrae and left posterior hilum ; , nodular opacities in bilateral lungs ; interlobular septal thickening suspicious for lymphangitic carcinomatosis ; numerous hepatic lesions ( largest , 7 cm in the dome of liver ) ; 25 lesions in the brain and cerebellum ( largest , 7 mm in the left cerebellar hemisphere ; fig 2a and 1c , left panels ) , and a 5 - mm leptomeningeal nodule at the level of t11 ( fig 2d , left panel )  . calcitonin and cea levels measured 2 , 180 pg / ml and 12 , 312 ng / ml , respectively ( fig 2b )  . the patient experienced clinical response within the rst month of therapy , with resolution of baseline diarrhea and nausea , and with appetite improvement . 
at 17 months , an mri of the brain showed an isolated , new , 5 - mm left caudate lesion that was treated with srs ( fig 2e , left and right panels ) with continuation of selpercatinib . 
at 20 months , imaging revealed non - cns multifocal progression with a new 6 - mm bony lesion in the c7 vertebral body , as well as several new , right - side liver lobe lesions ( the largest measured 2 cm )  . 
the patients calcitonin level rose to 235.9 pg / ml ; her cea level remained unchanged . peripheral blood cell - free dna analysis at the time of systemic progression revealed only the presence of the previously identied ret m918t missense mutation . 
the patient declined a liver biopsy . cns disease remained in response until 22 months , when several new brain lesions were found to have developed ; these were managed with srs ( fig 2 )  . 
her treatment course has been complicated by several hospitalizations unrelated to selpercatinib . discussion metastatic dissemination of mtc to the cns is a rare but devastating complication associated with poor prognosis and no well - established treatment strategies.1 although limited evidence from previous reports suggests that surgical resection and / or radiation therapy may be used in select cases , there remains a strong need for novel treatment modalities with durable therapeutic responses.1 - 3 cns efcacy of multikinase inhibitors such as vandetanib or cabozantinib has not been reported in mtc . here , we present a report of successful treatment of the brain and leptomeningeal metastases with systemic therapy in a patient with ret - mutated mtc , using the purpose - built selective and cns - penetrant ret inhibitor selpercatinib . 
treatment with this agent resulted in complete and durable resolution of the measurable brain and leptomeningeal lesions in a patient with previous disease progression while she received cabozantinib and radiation therapy . 
 case report notably , the patients tumor harbored a heterozygous deletion in the cdkn2c gene linked to an aggressive disease phenotype in mtc.19 cdkn2c is a member of the ink4 family of cyclin - dependent kinase inhibitors that block the cell cycle progression in the g1 phase through interaction with cyclin - dependent kinases 4 and 6.19 cdkn2c is lost in approximately 40% to 50% mtcs and is associated with a signicantly shorter time to distant metastasis and decreased overall survival in mtc , an effect further enhanced by concomitant ret m918t mutation.19 , 21 in addition , an earlier report showed that cdkn2c haploinsufciency is associated with a strong trend toward reduced progressionin ret - mutated mtc treated with systemic free survival therapy.21 however , this relationship has not been studied in patients receiving selective ret inhibitors , to our knowledge , and the signicance of cdkn2c loss in this setting remains to be determined . the patient is continuing selpercatinib therapy , with gradual disease progression in the liver . 
a recent study demonstrated that ret solvent - front mutations ( ret g810s / g810r / g810c ) can cause on - target resistance to selective and multikinase ret inhibitors.22 a better understanding of mechanisms of acquired resistance to selective ret inhibitors and frequency of resistant alterations would guide the development of novel agents and combination therapies directed towards further improvement of treatment outcomes for patients with ret - altered malignancies . in conclusion , we observed a radiographically conrmed durable response with selpercatinib in a patient with a heavily pretreated ret m918tmutated mtc with extensive cns metastases . 
mcwilliams rr , giannini c , hay id , et al : management of brain metastases from thyroid carcinoma : a study of 16 pathologically conrmed cases over 25 years . cancer 98 : 356 - 362 , 2003 drilon a , hu zi , lai ggy , et al : targeting ret - driven cancers : lessons from evolving preclinical and clinical landscapes . 
hofstra rmw , landsvater rm , ceccherini i , et al : a mutation in the ret proto - oncogene associated with multiple endocrine neoplasia type 2b and sporadic medullary thyroid carcinoma . 
nature 367 : 375 - 376 , 1994 elisei r , cosci b , romei c , et al : prognostic signicance of somatic ret oncogene mutations in sporadic medullary thyroid cancer : a 10 - year follow - up study . j clin endocrinol metab 93 : 682 - 687 , 2008 beldjord c , desclaux - arramond f , rafn - sanson m , et al : the ret protooncogene in sporadic pheochromocytomas : frequent men 2 - like mutations and new molecular defects . 
guo r , schreyer m , chang jc , et al : response to selective ret inhibition with loxo - 292 in a patient with ret fusion - positive lung cancer with leptomeningeal metastases . 
drilon a , oxnard gr , wirth l , et al : a phase 1 / 2 trial of loxo - 292 in patients with ret fusion - positive lung cancers . 
maxwell je , gule - monroe mk , subbiah v , et al : novel use of a clinical laboratory improvements amendments ( clia ) - certied cyclin - dependent kinase n2c ( cdkn2c ) loss assay in sporadic medullary thyroid carcinoma . 
 undetectable ras - mutant clones in plasma : possible implication for anti - egfr therapy and prognosis in patients with ras - mutant metastatic colorectal cancer mohamed bouchahda , md1 - 4 ; raphael saffroy , phd5 ; abdoulaye karabou e , md2 , 6 ; jocelyne hamelin , phd5 ; pasquale innominato , md , phd2 , 7 , 8 ; faouzi saliba , md , phd9 ; francis l evi , md , phd1 , 2 , 8 ; nelly bosselut , md5 ; and antoinette lemoine , pharmd , phd5 purpose combining cetuximab with chemotherapy provides clinical benet to 60% of the patients with ras wild - type ( ras - wt ) metastatic colorectal cancer ( mcrc )  . 
the patients with raswt ctdna received cetuximab + uorouracil , leucovorin , and irinotecan ( folfiri ) , whereas those with ras - mt ctdna were treated with the oncologists choice of therapy . results of 16 registered patients , 11 were male and ve female . 
they were age 48 to 81 years , and they had unresectable metastatic adenocarcinoma from the colon ( n = 11 ) or rectum ( n = 5 ) , with a median of two metastatic sites . 
in the patients with wt ctdna , objective tumor response rate was 50.0% , including one complete response and four partial responses after a median number of 6 courses of cetuximab + folfiri ( range , 1 to 16 courses )  . 
this was particularly the case for the combination of cetuximab with uorouracil , leucovorin , and irinotecan ( folfiri ) or uorouracil , leucovorin , and oxaliplatin ( folfox ) .1 , 2 however , several studies have shown that the survival of those patients with tumor ras mutations ( ras - mt ) was shorter than for those with ras - wild - type ( ras - wt ) tumors.3 , 4 since 2014 , it has been recommended that only patients with ras - wt mcrc should receive an anti - egfr targeted agent.5 ras mutations have been found in 30% to 50% of patients with mcrc , 6 - 9 which makes these patients ineligible for egfr - targeted therapies . recent studies have demonstrated that the analysis of circulating tumor dna ( ctdna ) in blood samples , through its ability to recapitulate tumor heterogeneity , is a remarkable surrogate of tumor biopsy for detecting mutations.10 - 12 this technique has the advantage of being less invasive than a tissue biopsy and can be easily repeated over time . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue context key objective to determine whether the lack of ras mutation in a liquid biopsy supports the administration of an antiepidermal growth factor receptor ( egfr ) antibody , despite earlier documentation of a pathogenic ras mutation in the primary colorectal cancer ( crc )  . knowledge generated nearly half the patients in this pilot study received cetuximab - based chemotherapy , because no ras mutation was detected in the liquid biopsy , despite such mutations having been found in the primary tumor . 
the progression - free survival and the overall survival of these heavily pretreated patients largely exceeded those in patients whose liquid biopsy revealed ras mutation and who received chemotherapy only . relevance tracking the gain or loss of ras - mutated cancer clones through liquid biopsies along the course of crc disease may have a profound impact on its therapeutic management . 
this is achieved through enabling the administration of anti - egfr that was initially rejected on the basis of previous molecular testing of tissue . in the characterization of the dynamics of acquired resistance to anti - egfr therapies.13 to date , studies with liquid biopsy have been selectively focused on the early detection of the appearance of ras - mt clones in tumor deposits by analyzing ctdna in blood samples from patients with ras - wt primary crc13 as biomarkers of an increasing resistance to anti - egfr agents . 
indeed , no specication in the european marketing authorisation for cetuximab mentions that tumor ras testing should be determined on solid tumor tissue in order to allow for anti - egfr administration . 
this is also the case for the recommendations by the french high health authority regarding cetuximab use . all consecutive patients treated between august 2017 and february 2019 at one of three participating centers in france were screened for inclusion in this pilot study . 
inclusion required histologic or cytologic proof of colorectal adenocarcinoma , with a kirsten rat sarcoma viral oncogene homolog ( kras ) or neuroblastoma rat sarcoma viral oncogene homolog ( nras ) mutation ( nras - mt ) from a tissue biopsy . 
the massarray ultraseek procedure involves a 3 - step process consisting of the initial polyinactivation of unincorporated merase chain reaction , nucleotides by shrimp alkaline phosphatase , and a singlebase primer extension according to the manufacturers protocol . 
the products were then nano - dispensed onto a matrix - loaded silicon chip ( spectrochipii , agena bioscience ) , and the mutations were detected by matrixassisted laser desorption - ionizationtime of ight mass spectrometry . 
for our study , the sensitivity for the detection of clinically relevant ras gene mutations in ctdna was 88% for patients with crc liver metastases , in good agreement with bettegowda et al.16 we currently use these highly sensitive mass spectrometry ctdna analyses for monitoring treatment of patients with nonsmall - cell lung cancer or breast cancer in routine oncology practice . study treatment all patients had ras - mt tissue biopsies . 
the study population was divided in two groups according to the results of the ctdna mutational analysis : group 1 included the patients with ras - mt also found in plasma ; group 2 included the patients with ras - wt ctdna . 
the sum of the largest diameters of the target lesions was computed on the inclusion imaging and used as baseline for the quantication of tumor downsizing and response categorization according to recist . 
response was classied as complete response , partial response , stable , or progressive disease.15 statistical consideration this pilot exploratory study included consecutive patients , and no sample size was dened a priori . 
the durations of progression - free survival ( pfs ) and overall survival ( os ) were measured from inclusion until the date of progression or death , respectively , or that of last follow up , with the database locked on may 25 , 2019 . 
all analyses were performed with intentto - treat using spss v18.0 software ( spss , chicago , il )  . results patients sixteen patients with unresectable mcrc and ras - mt in a cancer tissue were registered at one of three centers in initial ras mutational status was dethis pilot study . termined in the resected primary tumor for 11 patients ( 69% ) or in a tumor biopsy for 5 patients ( 31% )  . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue two or more chemotherapy regimens for metastatic disease . two groups of patients were identied according to the results of ctdna mutational analysis at inclusion . 
group 1 received the investigators choice of chemotherapy regimens , which included bevacizumab + folfox for three patients , aibercept + folfiri for three patients , and regorafenib for one patient . 
baseline characteristics were similar in the 2 groups ( table 1 )  . safety data for the nine patients with ctdna ras - wt ( group 2 ) overall , the cetuximab + folfiri regimen was well tolerated . 
the main grade 1 or 2 clinical toxicities were fatigue , diarrhea , nausea or vomiting , mucositis , acneiform rash , and alopecia ( 6 [ 67% ] of 9 for all )  . 
this fourth - line protocol was well tolerated , with the most severe toxicities being grade 2 leukopenia , neutropenia , fatigue , and acneiform rash . discussion the patients in this study had advanced and chemotherapy - resistant metastatic disease , without any imbalance in apparent overall tumor burden that could reasonably inuence the liquid biopsy results . 
thus , no evidence supports the possibility that the differences in detection of ctdna ras mutation would be related to between - patient variations in tumor burden . the identication of a mutation in kras or nras from a cancer tissue biopsy precludes the use of anti - egfr treatment in association with chemotherapy against mcrc , based on consistent evidence.5 our group rst reported the occurrence of acquired kras mutations along the progression of colorectal metastases in patients treated with cetuximab . 
we then hypothesized that the late acquisition of kras mutations could represent a possible mechanism of secondary resistance to anti - egfr antibodies.18 however , the assumption of persisting ras - mt genotype for patients who received chemotherapy has not been challenged before now because of the expected evolutionary advantage of ras - mt clones.19 yet in this pilot study , we found that nearly half the patients with mcrc displayed no detectable ras - mt in ctdna , although their cancer tissue genotyping had demonstrated ras - mt . 
this nding raised several questions . first , is there a concordance between the ras mutational status of tumor tissues and that of ctdna ? several studies have highlighted discrepant results in ras mutational status for 10% - 15% of the patients tested , depending on the method used.11 , 14 , 20 vidal et al explained such plasmaversus - tissue ras discrepancies with spiral and temporal heterogeneity in ras - mt tumor clones within the tumor tissue.11 according to thierry et al , 20 such discrepancies could relate to the use of biopsies . 
other discrepancies that seemed to affect concordance were long intervals between assessments of the ras status in tumor tissue and that in the blood sample , resection of the tumor at the time of blood draw , tissue analyzed . grasselli et al14 ascribed the discrepancies in ras status to differences in technical sensitivity of the methods used for analysis or to heterogeneity . tumor site , and type of second , is there a change in ras status over time and / or during treatment ? this question does not yet have a clear answer . 
we were the rst to report 1 case of acquired kras mutation in metastases after progression under combined anti - egfr and doublet chemotherapy in 12 patients with kras - wt mcrc.18 other authors have highlighted the concurrent detection of sensitive and resistant clones to anti - egfr antibodies within tumor deposits from different locations in the same patient.21 - 24 this multiclonality could explain the dissociated antitumor responses that are frequently encountered in clinical practice . 
such tumor heterogeneity assumes the existence of wt clones sensitive to anti - egfr treatment alongside resistant mutant clones . interestingly , the team of raimondi et al25 recently reported the disappearance of ras - mt clones in ctdna after tumor progression while receiving bevacizumab and chemotherapy in 4 patients with ras - mt mcrc . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue feb 19 , 2019 before cetux + folfiri may 29 , 2019 after 6 courses sept 19 , 2019 after 12 courses target lesion target lesion target lesion fig 4 . 
case report illustrating exceptional efcacy of cetuximab + uorouracil , leucovorin , and irinotecan ( cetux + folfiri ) as fourth - line chemotherapy received by a 72 - year - old patient with kras mutation in tumor tissue but kras wild - type in liquid biopsy , upon inclusion in the study . 
indeed , the observed median pfs and os in these patients were similar to those reported for patients with ras - wt tumor tissue who received this combination as rst - line treatment for mcrc . 
our internal steering committee proposed to stop the pilot study , once the information was adequate for designing a randomized trial for testing the hypothesis further on the basis of an apparent three - fold increase in the median pfs of the experimental treatment compared with cetuximab - free chemotherapy . the intriguing and encouraging results of this exploratory trial need to be conrmed in randomized clinical trials . such validation steps are particularly relevant because all our patients with ras - wt ctdna received cetuximab ; thus , we cannot differentiate between a prognostic and a predictive role of ras - wt ctdna for outcomes of patients receiving cetuximab - based chemotherapy . 
 bouchahda et al than prognostic of an aggressive tumor biology.34 such consideration would further support the hypothesis of an added benet from cetuximab in this subgroup of patients . yet recent evidence suggests that the proportion of ras - mt in ctdna was a prognostic indicator for both os and pfs in patients with mcrc.35 this nding raised the question of a potential divide on the clinical signicance between tumor and ctdna genotyping , which this study cannot respond to . 
the fact that orrs exceeded 40% and were similar in both treatment groups suggested that all the patients included in the study were not completely resistant to chemotherapy and that those with ras - mt in the liquid biopsy could have a worse prognosis , as proposed by elz et al.35 however , single - agent cetuximab achieved only a 10% orr in patients with chemotherapy refractory mcrc , 36 despite prolonging pfs by 4 months . 
taken together , the literature results support a much greater value for pfs prolongation compared with orr as an efcacy end point , which supports the hypothesis that the liquid biopsy results have a predictive value . the lack of a prespecied sample size and the low number of patients in each group constitute the main limitations of our pilot salvage study . 
the three - fold increase in median pfs in the absence of any apparent bias does suggest that antiegfrbased chemotherapy could represent a promising option for nearly half the patients with initially documented ras - mt on tumor tissue at a later stage of their disease . our study was in line with the chronos study ( clinicaltrials.gov identier : nct03227926 ) , 37 whose design is based on the concept that crc genome adapts dynamically to intermittent anti - egfr drug schedules . 
a follow - up on our study would involve a randomized clinical trial in which eligible patients with ras - mt on solid tumor tissue undergo ras mutational status assessment in ctdna upon progression on chemotherapy . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue references venook ap , niedzwiecki d , lenz hj , et al : effect of rst - line chemotherapy combined with cetuximab or bevacizumab on overall survival in patients with kras wild - type advanced or metastatic colorectal cancer : a randomized clinical trial . 
jama 317 : 2392 - 2401 , 2017 tejpar s , stintzing s , ciardiello f , et al : prognostic and predictive relevance of primary tumor location in patients with ras wild - type metastatic colorectal cancer : retrospective analyses of the crystal and fire - 3 trials . 
modest dp , ricard i , heinemann v , et al : outcome according to kras - , nrasand braf - mutation as well as kras mutation variants : pooled analysis of ve randomized trials in metastatic colorectal cancer by the aio colorectal cancer study group . 
ann oncol 27 : 1746 - 1753 , 2016 de roock w , claes b , bernasconi d , et al : effects of kras , braf , nras , and pik3ca mutations on the efcacy of cetuximab plus chemotherapy in chemotherapy - refractory metastatic colorectal cancer : a retrospective consortium analysis . 
lancet oncol 11 : 753 - 762 , 2010 van cutsem e , cervantes a , nordlinger b , et al : metastatic colorectal cancer : esmo clinical practice guidelines for diagnosis , treatment and follow - up . 
ann oncol 25 : iii1 - iii9 , 2014 douillard jy , oliner ks , siena s , et al : panitumumab - folfox4 treatment and ras mutations in colorectal cancer . 
heinemann v , von weikersthal lf , decker t , et al : folfiri plus cetuximab versus folfiri plus bevacizumab as rst - line treatment for patients with metastatic colorectal cancer ( fire - 3 ) : a randomised , open - label , phase 3 trial . 
lancet oncol 15 : 1065 - 1075 , 2014 van cutsem e , lenz hj , k ohne ch , et al : fluorouracil , leucovorin , and irinotecan plus cetuximab treatment and ras mutations in colorectal cancer . 
j clin oncol 33 : 692 - 700 , 2015 peeters m , kafatos g , taylor a , et al : prevalence of ras mutations and individual variation patterns among patients with metastatic colorectal cancer : a pooled analysis of randomised controlled trials . 
vidal j , muinelo l , dalmases a , et al : plasma ctdna ras mutation analysis for the diagnosis and treatment monitoring of metastatic colorectal cancer patients . ann oncol 28 : 1325 - 1332 , 2017 12 . 
grasselli j , elez e , carat `u g , et al : concordance of bloodand tumor - based detection of ras mutations to guide anti - egfr therapy in metastatic colorectal cancer . 
bouchahda m , macarulla t , liedo g , et al : feasibility of cetuximab given with a simplied schedule every 2 weeks in advanced colorectal cancer : a multicenter , retrospective analysis . 
lacina l , coma m , dvor ankov a b , et al : evolution of cancer progression in the context of darwinisanticancer res 39 : 1 - 16 , 2019 20 . 
thierry ar , el messaoudi s , mollevi c , et al : clinical utility of circulating dna analysis for rapid detection of actionable mutations to select metastatic colorectal patients for anti - egfr treatment . 
raimondi c , nicolazzo c , belardinilli f , et al : transient disappearance of ras mutant clones in plasma : a counterintuitive clinical use of egfr inhibitors in ras mutant metastatic colorectal cancer . 
zhou m , yu p , hou k , et al : effect of ras status on anti - egfr monoclonal antibodies + 5 - fu infusion - based chemotherapy in rst - line treatment of metastatic colorectal cancer : a meta - analysis . 
giantonio bj , catalano pj , meropol nj , et al : bevacizumab in combination with oxaliplatin , uorouracil , and leucovorin ( folfox4 ) for previously treated metastatic colorectal cancer : results from the eastern cooperative oncology group study e3200 . 
van cutsem e , tabernero j , lakomy r , et al : addition of aibercept to uorouracil , leucovorin , and irinotecan improves survival in a phase iii randomized trial in patients with metastatic colorectal cancer previously treated with an oxaliplatin - based regimen . 
tabernero j , yoshino t , cohn al , et al : ramucirumab versus placebo in combination with second - line folfiri in patients with metastatic colorectal carcinoma that progressed during or after rst - line therapy with bevacizumab , oxaliplatin , and a uoropyrimidine ( raise ) : a randomised , double - blind , multicentre , phase 3 study . 
sobrero af , maurel j , fehrenbacher l , et al : epic : phase iii trial of cetuximab plus irinotecan after uoropyrimidine and oxaliplatin failure in patients with metastatic colorectal cancer . 
peeters m , oliner ks , price tj , et al : analysis of kras / nras mutations in a phase iii study of panitumumab with folfiri compared with folfiri alone as second - line treatment for metastatic colorectal cancer . 
de stefano a , rosanova m , malapelle u , et al : discordance in ras mutations between primary colon tumor and metastases : a real event or a matter of methodology ? int j biol markers 32 : e474 - e477 , 2017 34 . 
elez e , chianese c , sanz - garca e , et al : impact of circulating tumor dna mutant allele fraction on prognosis in ras - mutant metastatic colorectal cancer . 
siena s , bardelli a , sartore - bianchi a , et al : exploiting clonal evolution and liquid biopsy to overcome resistance to anti - egfr treatment in metastatic colorectal cancer : the chronos trial . 
we show that kit inhibition markedly decreased cell viability in melanoma cell lines with distinct kit mutations ; however , this effect was countered in the presence of hepatocyte growth factor ( hgf ) , the ligand for met . 
a physical examination revealed a raised , erythematous , and well - circumscribed cutaneous lesion on her left great toe , which the patient attributed to trauma that occurred several months earlier . 
staging computed tomography ( ct ) and positron emission tomography scans revealed left inguinal and left external iliac lymphadenopathy ; two soft - tissue densities in the left breast ( one biopsy proven to be melanoma ) ; numerous subcentimeter , hypodense liver lesions ; and multiple subcentimeter , subcutaneous nodules , suggestive of metastatic disease . 
gene mutation analysis of the metastatic melanoma tissue did not reveal mutations in braf or nras . after two cycles of biochemotherapy ( data supplement ) , restaging ct scans revealed overall stable disease and a mixed tumor response in the lymph nodes . 
the patient received whole - brain radiation therapy ( 30 gy in 10 fractions ) , then stereotactic radiosurgery , followed by combination treatment with temozolomide , cisplatin , and vinblastine . subsequent restaging showed new mediastinal lymphadenopathy and lung nodules . 
the patient received two cycles of a carboplatin - paclitaxel regimen before evidence of disease progression in the left inguinal lymph nodes , liver , and bra the patient was then treated with ipilimumab , which had just received us food and drug administration approval for metastatic melanoma , 3 mg / kg for four cycles . 
there was evidence of stable disease response to ipilimumab , with tumor reduction of 30% by immune - related response criteria overall with disease response in the brain , liver , and lymph nodes . 
after 19 months of disease control with ipilimumab treatment , a brain magnetic resonance imaging demonstrated a left frontal operculum metastasis with perilesional edema ( fig 1a , upper panel ) and positron emission tomography / ct junna oba sun - hee kim wei - lien wang mariana p . 
 ( a ) representative brain magnetic resonance images show left frontal operculum metastasis with perilesional edema pretreatment ( top panel ) and the on - treatment combination dasatinib and crizotinib therapy effect ( lower panel )  . 
 ( b ) polymerase chain reactionbased dna sequencing chromatogram showing a kit nucleotide transition ( 2464 a > t ) at codon 822 ( aat to tat ) in exon 17 from the patients acral melanoma metastatic tumor . 
 ( c ) hematoxylin and eosin ( he ) and immunohistochemical staining for total kit and phosphorylated kit ( p936 ) and total met in the patients primary ( upper panel ) and metastatic ( lower panel ) acral melanoma tumors ( original magnification , 20 )  . scanning showed new hypermetabolic activity in the mediastinal lymph nodes , which was verified to be metastatic melanoma by interventional radiology - guided fine - needle aspiration ( data not shown )  . 
kit mutations and copy number alterations in 4q ( kit ) and 11q ( ccnd1 ) for the melanoma cell lines cell line name exon 4q ( kit ) 11q ( ccnd1 ) kit mutation copy number increase aa change l576p w556 - k558 n822y s476i m230 melms 2391 ma - mel - 144 histopathologic examination of the patients primary and metastatic melanoma tumors showed widespread expression of phosphorylated / total kit protein in melanoma cells ( fig 1c )  . 
given the response to combination dasatinib and crizotinib therapy , we also assessed the expression of the met , for which crizotinib has high binding affinity , and observed positive staining in both primary and metastatic tumors , with moderately higher intensity in the metastatic tumor . to better understand the mechanism by which combination therapy resulted in the observed clinical response , we performed a molecular analysis of the melanoma cell line we established from the patients metastatic tumor ( cell line 2391 ) , as well as three other melanoma cell lines shown to have endogenous kit mutations ( namely , melms , ma - mel - 144 , and m230 ) .17 - 19 mutation analysis confirmed the presence of the 2464 a > t nucleotide transition in kit with a resultant n822y amino acid change in the activation loop within 2391 , the patients melanoma cell line ( data supplement )  . 
we verified the presence of each specific kit mutation within each cell line using targeted next - generation dna sequencing ( table 1 ; data supplement ) .20 no braf or nras mutations , or secondary mutations in kit were detected in any of the cell lines . we also determined the global chromosomal copy number alteration status within each kit - mutant melanoma cell line ( fig 2a ; table 1 )  . 
cell lines 2391 and ma - mel - 144 had chromosome 4q copy number elevation , which corresponds with the location of the kit locus , consistent with initial observations that kit mutations co - occur with kit amplifications.1 , 2 three of the four cell lines also had chromosome 11q copy number elevation , which corresponds with the location of the ccnd1 locus , also well described to be amplified in am tumors.21 , 22 thus , the patients cell line 2391 and others in our panel had characteristic genetic features observed in am tumors . to determine the endogenous constitutive activity of each kit mutation , we assessed the total and phosphorylated levels of kit in each melanoma cell line . 
western blot analysis showed phosphorylated kit to be present in all the kit - mutant melanoma cell lines in the presence or absence of serum ( fig 2b ) ; this was not observed in those without a kit mutation ( data supplement )  . 
each of the cell lines showed sensitivity to gene - specific kit knockdown and to multiple tkis that share kit as a target but have many nonoverlapping targets ( eg , dasatinib targets src - family kinases ) , whereas imatinib does not ( data not shown )  . 
cell lines 2391 ( kitn822y ) , melms ( kit556 - 558del ) , and ma - mel - 144 ( kits476i ) show amplification at 11q ( location of ccnd1 allele )  . 
cell viability assay of m230 ( kitl576p ) , melms ( kit556 - 558del ) , 2391 ( kitn822y ) , and ma - mel - 144 ( kits476i ) melanoma cell lines : no treatment , dasatinib ( 50 nm ) , dasatinib plus hgf ( 100 ng / ml ) , dasatinib plus hgf plus crizotinib ( 5 m ) , and crizotinib alone . of met may enhance the effect of single - agent dasatinib in the tumor setting . 
thus , we tested if the presence of hgf , the only known ligand for met , in the extracellular environment can modulate the reduction in cell viability observed with dasatinib treatment ( fig 2c )  . 
analysis of the patients tumor and cell line ( and three other kit - mutant cell lines ) suggests that the hgf - met axis may be a mechanism of de novo resistance in kit - mutant melanomas . the emergence of secondary mutations in kit is a common mechanism of clinical resistance to kit inhibition in kit - mutant gist.29 however , nearly all resistance observed in kit mutant melanoma occurs in the initial treatment setting , before the clonal evolution of secondary mutations can emerge , 10 - 13 , 23 - 26 suggesting that the presence of coactivating pathways may play a role in this primary resistance . the observed efficacy of the combination dasatinib and crizotinib could , in part , be due to the inhibition of multiple kinases ; however , the melanoma cell line studies indicate the primacy of the kit and met receptors to explain the observed results . 
furthermore , crizotinib alone was only effective in the presence of extracellular hgf , the only known met ligand , indicating crizotinibs modulation of the well - described hgf - met axis , for which it was initially designed.30 these data are consistent with those from preclinical studies showing that met inhibition increases the effect of imatinib in kit - mutant gist models.31 it is intriguing to speculate that the response to combination dasatinib and crizotinib may have been immunologically enhanced , given the patients prior tumor response to ipilimumab therapy . 
hong collection and assembly of data : junna oba , sunhee kim , wei - lien wang , mariana macedo , fernando carapeto , meredith a mckean , john van arnam , agda k . 
woodman manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors junna oba no relationship to disclose sun - hee kim no relationship to disclose wei - lien wang no relationship to disclose mariana p . 
haydu no relationship to disclose honoraria : novartis , bristol - myers squibb , janssen oncology , roche consulting or advisory role : novartis , illumina , ge healthcare research funding : medimmune , astrazeneca , roche , novartis patents , royalties , other intellectual property : elsevier travel , accommodations , expenses : bristol - myers squibb , novartis elizabeth a . 
hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack , bayer consulting or advisory role : baxter , bayer , guidepoint global , janssen research funding : novartis , genentech , eisai , astrazeneca , pfizer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer , bristol - myers squibb , genmab , ignyta , infinity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo , medimmune , molecular templates , takeda travel , accommodations , expenses : loxo , mirna therapeutics other relationship : oncorena chantale bernatchez stock and other ownership interests : lexicon ( i ) research funding : nektar , idera , iovance biotherapeutics , medimmune , pfizer , emd serono patents , royalties , other intellectual property : patent pending on btla as a marker for better cd8 t cells for adoptive immunotherapy alexander j . 
woodman no relationship to disclose acknowledgment leadership : beta cat pharmaceuticals , archer biosciences stock and other ownership interests : archer biosciences , beta cat pharmaceuticals we thank the center for environmental and molecular carcinogenesis anderson cancer center , smithville , tx , for antibody optimization . affiliations junna oba , sun - hee kim , wei - lien wang , mariana p . 
macedo , ac camargo cancer center , so paulo , brazil . supported by the university of texas system rising star award , national cancer institute ( nci ) specialized programs of research excellence ( spore ) in melanoma ( p50 ca093459 to d.s.h. ) ; developmental research project award , national institutes of health / nci cancer center support grant no . 
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woodman se , trent jc , stemke - hale k , et al : activity of dasatinib against l576p kit mutant melanoma : molecular , cellular , and clinical correlates . 
yang y , liu c , peng w , et al : antitumor t - cell responses contribute to the effects of dasatinib on c - kit mutant murine mastocytoma and are potentiated by anti - ox40 . 
hodi fs , corless cl , giobbie - hurder a , et al : imatinib for melanomas harboring mutationally activated or amplified kit arising on mucosal , acral , and chronically sun - damaged skj clin oncol 31 : 3182 - 3190 , 2013 11 . 
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kato s , jardim dl , johnson fm , et al : phase i study of the combination of crizotinib ( as a met inhibitor ) and dasatinib ( as a c - src inhibitor ) in patients with advanced cancer . 
todd jr , scurr ll , becker tm , et al : the mapk pathway functions as a redundant survival signal that reinforces the pi3k cascade in c - kit mutant melanoma . 
lee sj , kim tm , kim yj , et al : phase ii trial of nilotinib in patients with metastatic malignant melanoma harboring kit gene aberration : a multicenter trial of korean cancer study group ( un10 - 06 )  . 
kalinsky k , lee s , rubin km , et al : a phase 2 trial of dasatinib in patients with locally advanced or stage iv mucosal , acral , or vulvovaginal melanoma : a trial of the ecog - acrin cancer research group ( e2607 )  . 
 c response to mammalian target of rapamycinbased therapy and incidental finding of lynch syndrome in a patient with solid pseudopapillary neoplasm of the pancreas with akt1_e17k mutation introduction solid pseudopapillary neoplasms ( spns ) of the pancreas are exocrine neoplasms that predominantly affect young females and are considered to have low malignant potential . 
surgical resection offers patients an excellent chance of long - term survival , even in cases of local invasion , recurrence , and metastatic disease.1 - 3 recent studies have demonstrated that invasion of these neoplasms into muscular vessels , advanced tumor stage by european neuroendocrine tumors society classification , and distant metastasis correlated with poor prognosis.4 in such instances and especially when complete surgical resection is unattainableuse of salvage chemotherapy is needed.5 , 6 in this setting , some chemotherapy agents have offered favorable responses , 7 - 10 yet because of the scarce number of reported cases requiring this treatment modality , no regimen has been demonstrated as definitely superior.11 first described by frank in 1959 and histologically defined as spns by the who in 2010 , spns have been demonstrated to harbor somatic point mutations in exon 3 of ctnnb1 , the gene that encodes for - catenin , a downstream transcriptional activator in the wnt signaling pathway that is involved in cell growth regulation.12 , 13 spns have not previously been associated with genetic mutations linked to dna mismatch repair ( mmr ) syndromes , such as lynch syndrome and hereditary nonpolyposis colorectal cancer ( hnpcc ) syndrome . 
to clarify the likely oncologic diagnosis , additional workup was performed , including - fetoprotein , carcinoembryonic antigen , cancer antigen 125 , and cancer antigen 19 - 9 testing , with normal values . 
postoperatively , she developed acute gi bleeding from a gastric ulcer and remained admitted for more than 30 days . pathologic evaluation revealed a uniform grayish maroon , soft , necrotic , and hemorrhagic lesion macroscopically . 
herzog author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non - commercial no derivatives 4.0 license corresponding author : cynthia e . 
 ( c - f ) immunohistochemical staining showing that the liver metastasis is negative for pan - cytokeratin ( c ) and chromogranin ( d ) , but positive for nuclear expression of - catenin ( e ) and progesterone receptor ( f )  . 
hepatocytes , which are positive for pan - cytokeratin ( c ) and negative for nuclear expression of - catenin ( e ) and progesterone receptor ( f ) , serve as internal controls . 
magnification , 100 ( a - f )  . results were positive for vimentin , cd10 , - catenin , progesterone receptor , and synaptophysin , but negative for pan - cytokeratin and chromogranin ( fig 1 )  . 
these results were consistent with the diagnosis of an spn involving the pancreatic body and tail . on the patients first follow - up after 1 year , abdominal ultrasonography and computed tomography revealed multiple liver masses involving hepatic segments iii , vi , vii , and viii ; a tumoral thrombus in the spleno - portal venous confluence ; and enlargement of several lymph nodes that raised concern of metastases ( fig 2a )  . 
she was referred to the university of texas md anderson cancer center for additional management . at our institution , the pathologic findings of her primary and metastatic lesions were found to be identical to those obtained at the outside institution . 
she completed four cycles of chemotherapy with oxaliplatin , irinotecan , and fluorouracil , with subsequent computed tomography images that demonstrated mild progression of metastatic disease ( fig 2b )  . 
 ( a ) computed tomography ( ct ) scan of the liver dome showing metastatic solid pseudopapillary neoplasm in a 13 - year - old girl before arrival at our institution . 
 on the basis of the akt1 mutation , the patient was enrolled in a clinical trial ( clinicaltrials.gov identifier : nct01582191 ) , with each cycle consisting of 28 days of oral vandetanib ( 300 mg ) ; a multikinase inhibitor of epidermal growth factor receptor ( egfr ) , vascular endothelial growth factor receptor ( vegfr ) , and ret ; and oral everolimus ( 10 mg ) , a mammalian target of rapamycin ( mtor ) inhibitor . 
she was taken off the protocol and continued on single - agent everolimus at the same dosing schedule . the patient has remained on mtor - based therapy for more than 3 years with excellent performance status and stable disease ( 15% reduction ) from baseline tumor size ( fig 2c )  . 
she has had several episodes of mucositis that have been managed with topical corticosteroids and sucralfate or a brief interruption of therapy . fourteen months after the start of single - agent everolimus , additional genetic testing using targeted exome sequencing of 202 genes with tumor and matched normal dna resulted in the identification of a pathogenic germline msh6 mutation ( c.2147_2148delca ) , which is consistent with lynch syndrome / hnpcc syndrome and later confirmed in a clinical laboratory improvement amendmentscertified laboratory ( table 1 ) and via immunohistochemistry testing . 
 her mother underwent genetic testing and was found to be negative for the mutation . discussion to our knowledge , this is the first case reporting the use of genomic testing to guide the treatment of metastatic spn of the pancreas . 
pembrolizumab , a programmed death - 1 checkpoint inhibitor , recently demonstrated immune - related clinical benefit , which resulted in us food and drug administration approval for its use in mmr - deficient colorectal neoplasms.19 of importance , this genetic entity has also been reported in pancreatic neoplasms.20 geary et al21 investigated 130 families with mmr mutations that were comparable to that of our patient and reported 22 cases of early - onset pancreatic cancers . 
well - differentiated pancreatic neuroendocrine tumors , medullary carcinomas , and intraductal papillary mucinous neoplasms of the pancreas , among others , have been associated with microsatellite instability syndromes , 22 , 23 but spns have not been previously described in association with lynch syndrome . although a few case reports have demonstrated that chemotherapy agents offer variable degrees of activity toward this rare neoplasm , 7 - 11 we elected treatment with the well - known regimen for gi tumors , oxaliplatin , irinotecan , and fluorouracil ; however , the tumor progressed . 
recently , guo et al24 conducted whole genome sequencing analysis on nine patients spns and identified numerous genetic mutations , including usp9x , ep400 , pdk1 , med12 , htt and ar . 
met germline mutations have never been reported in association with spns , yet its presence in this case is of interest and could have also contributed , in part , to the development of this disease . 
molecular testing in this disease affords the opportunity of identifying a targetable mutation , as demonstrated in our case . targeting the phosphatidylinositol 3 - kinase / akt / mtor pathway , which is known for its participation in cell proliferation , apoptosis , and angiogenesis , 25 was effective in our patient with spn . 
analogous to the response achieved in cases of pancreatic neuroendocrine tumors , 26 treatment with everolimus , an oral signal transduction inhibitor that blocks mtor , resulted in stable disease . 
the patient continues to tolerate the treatment well , with most adverse events being managed successfully with medical treatment . although germline msh6 mutationassociated lynch syndrome / hnpcc syndrome and spn may have been separate entities arising coincidentally in our patient , suspicion of the genetic inherited disorder as an impending trigger for this neoplasm is warranted . 
obtaining longitudinal analysis of the mtor pathway activation posteverolimus as well as the akt_e17k mutation frequency in the tumor would have allowed us to obtain additional data ; however , we elected to keep research interventions in this pediatric patient at a minimum . spns should be considered in the differential diagnosis of pancreatic masses in patients with lynch syndrome / hnpcc syndrome . 
herzog financial support : vivek subbiah administrative support : vivek subbiah collection and assembly of data : branko cuglievan , vivek subbiah , huamin wang , ajaykumar morani , funda mericbernstam , cynthia e . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . branko cuglievan no relationship to disclose vivek subbiah consulting or advisory role : medimmune research funding : novartis ( inst ) , glaxosmithkline ( inst ) , nanocarrier ( inst ) , northwest biotherapeutics ( inst ) , genentech ( inst ) , berg pharma ( inst ) , bayer ( inst ) , incyte ( inst ) , fujifilm ( inst ) , pharmamar ( inst ) , d3 oncology solutions ( inst ) , pfizer ( inst ) , amgen ( inst ) , abbvie ( inst ) , multivir ( inst ) , blueprint medicines ( inst ) , loxo ( inst ) , vegenics ( inst ) , takeda ( inst ) , alfasigma ( inst ) , agensys ( inst ) , idera ( inst ) , boston biomedical ( inst ) , inhibrx ( inst ) , exelixis ( inst ) travel , accommodations , expenses : pharmamar , bayer ajaykumar morani no relationship to disclose funda meric - bernstam honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inflection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pfizer , effector therapeutics , abbvie , boehringer ingelheim ( i ) vijaykumar holla no relationship to disclose cynthia e . 
estrella js , li l , rashid a , et al : solid pseudopapillary neoplasm of the pancreas : clinicopathologic and survival analyses of 64 cases from a single institution . 
tang lh , aydin h , brennan mf , et al : clinically aggressive solid pseudopapillary tumors of the pancreas : a report of two cases with components of undifferentiated carcinoma and a comparative clinicopathologic analysis of 34 conventional cases . 
strauss jf , hirsch vj , rubey cn , et al : resection of a solid and papillary epithelial neoplasm of the pancreas following treatment with cis - platinum and 5 - fluorouracil : a case report . 
hofmann h , von haken r , werner j , et al : unresectable isolated hepatic metastases from solid pseudopapillary neoplasm of the pancreas : a case report of chemosaturation with high - dose melphalan . 
irtan s , galmiche - rolland l , elie c , et al : recurrence of solid pseudopapillary neoplasms of the pancreas : results of a nationwide study of risk factors and treatment modalities . 
abraham sc , klimstra ds , wilentz re , et al : solid - pseudopapillary tumors of the pancreas are genetically distinct from pancreatic ductal adenocarcinomas and almost always harbor betacatenin mutations . 
kastrinos f , mukherjee b , tayob n , et al : risk of pancreatic cancer in families with lynch engl j med 372 : 2509 - 2520 , 2015 syndrome . 
geary j , sasieni p , houlston r , et al : gene - related cancer spectrum in families with hereditary non - polyposis colorectal cancer ( hnpcc )  . 
sparr ja , bandipalliam p , redston ms , et al : intraductal papillary mucinous neoplasm of the pancreas with loss of mismatch repair in a patient with lynch syndrome . 
banville n , geraghty r , fox e , et al : medullary carcinoma of the pancreas in a man with hereditary nonpolyposis colorectal cancer due to a mutation of the msh2 mismatch repair gene . 
case series 2 and 3 included archival samples from men treated at johns hopkins hospital ( n = 21 ) and university of calgary ( n = 8 ) , respectively . 
the frequency of pathogenic / likely pathogenic mutations are reported . results overall , 25 patients ( 49% ) had at least one dna damage repair gene alteration , including seven ( 14% ) with a mismatch repair gene mutation and 16 ( 31% ) with a homologous repair mutation . 
activating mutations in the pi3k pathway ( n = 19 ; 37% ) , wnt pathway ( n = 16 ; 31% ) , and mapk pathway ( n = 8 ; 16% ) were common . conclusion this study strongly suggests that dpcs are enriched for actionable mutations , with approximately 50% of patients demonstrating dna damage repair pathway alteration ( s )  . 
2019 by american society of clinical oncology introduction ductal prostate cancer ( dpc ) is a rare prostate cancer variant characterized by large glands lined by tall , pseudostratied , columnar , neoplastic epithelial cells , typically arranged over brovascular cores or cribriform glands and associated with an aggressive clinical course.1 - 3 outcomes for dpc generally mirror those of gleason score 4 + 4 = 8 carcinomas , and tumors with at least 10% ductal morphology have been found to associate with a higher stage and suboptimal response to androgen deprivation.2 , 3 overall , approximately 3% of all prostate cancers have some component of ductal histology.2 , 4 although the histologic features of dpc are well described , there is relatively little information regarding the underlying molecular alterations associated with this prostate cancer subtype . 
fluorescence in situ hybridization studies have found that tmprss2 : erg fusions are present in 10% to 50% of patients with dpc , and erg protein expression ( consistent with tmprss2 : erg fusions ) is also present in this range.5 - 8 limited gene expression proling studies have found similarities between dpc and patients with acinar tumors , and there is molecular evidence that concurrent ductal and acinar tumors are clonally related.4 , 9 , 10 more recent immunohistochemical proling studies have demonstrated that positive phosphomammalian target of rapamycin staining correlated with risk of biochemical recurrence in patients with ductal carcinoma.11 in a separate study , it was found that loss of pten protein expression occurred more frequently in dpc compared with acinar adenocarcinoma , again , potentially implicating mammalian target of rapamycin signaling pathway in the pathobiology of dpc . 
 schweizer et al context key objective the key objective was to provide an overview of the genomic alterations associated with ductal prostate cancers . knowledge generated ductal prostate cancers are associated with a high incidence of mutations in dna repair genes . 
we previously reported the ngs results from a small series characterizing patients with dpc at our institution ( university of washington [ uw ] ) .12 in that preliminary study , we observed a high rate of dna damage repair ( ddr ) mutations , including loss - of - function mutations in mismatch repair ( mmr ) genes . 
building from our initial case series , we now report sequencing results from an expanded multiinstitutional collaborative cohort of 51 patients with dpc . methods study populations we assembled three case series comprising 51 patients with dpc from institutions in the united states and canada ( data supplement )  . 
all tumor tissue was sequenced on the targeted ngs assay uw - oncoplex according to previously published methods.12 , 13 case series 1 consisted of prostate cancer specimens ( radical prostatectomies and needle biopsies of prostate and metastatic tumors ) from 22 men actively receiving treatment at the university of washington / seattle cancer care alliance who were prospectively identied as having a diagnosis of dpc . 
preliminary sequencing results from this series have been previously published.12 all men provided informed consent to have their tissue sequenced as part of this study . case series 2 included 21 radical prostatectomy samples . 
a subset was obtained from a tissue microarray composed of primary prostatectomy specimens from men with either dpc ( n = 51 ) or gleason pattern 4 acinar prostatic adenocarcinoma ( n = 75 ) treated at johns hopkins hospital ( jhh ) between 1984 and 2004 . 
case series 3 included archival tissue from eight men treated by transurethral resection of the prostate at the university of calgary . blinded morphologic evaluation to reevaluate the morphologic classication of all patients in a blinded manner , an expert genitourinary pathologist ( j.i.e. ) examined scanned digital images of a representative slide from each patient corresponding to the formalin - xed parafn - embedded ( ffpe ) block that was macrodissected for sequencing . 
each patient was scored for percentage of the tumor that had ductal morphology overall , as well as the percentage of several described morphologic subtypes of ductal carcinoma : cribriform , papillary , gland - like , prostatic intraepithelial neoplasialike and solid . macrodissection of tumor tissue all tissue was previously ffpe . 
for patients with clinical follow - up ( uw and university of calgary , n = 28 ) , seven ( 25% ) were deceased , and 12 ( 43% ) had developed table 1 . 
demographics and characteristics characteristic median age ( range ) , years gleason * value 67.5 ( 47 - 94 ) metastatic disease at presentation source of tissue for sequencing turp prostatectomy prostate needle biopsy metastatic biopsy 4 ( 13 ) 7 ( 23 ) 18 ( 60 ) 1 ( 3 ) 11 ( 26 ) 8 ( 15 ) 29 ( 56 ) 11 ( 21 ) 3 ( 6 ) note . 
 ( % ) unless otherwise indicated . abbreviation : turp , transurethral resection of the prostate . * gleason score was only provided for patients with mixed ductalacinar histology ( n = 30 )  . disease state at time of initial presentation was only available for johns hopkins hospital and university of washington ( n = 43 )  . metastatic disease during long - term follow - up . 
additional demographics details are listed in table 1 . dpc genomics overall , our combined cohort of patients with dpc demonstrated a high number of recurrent genomic alterations ( fig 1 ; data supplement )  . 
twenty - ve ( 49% ) of 51 patients had at least one alteration in a ddr pathway gene . overall , seven of 51 patients ( 14% ) had evidence of mmr alterations , six of whom had evidence of hypermutation ( ie , 10 mutation per megabase ) , consistent with decient mmr ( one patient with monoallelic loss of msh2 was not hypermutated )  . 
compared with published genomic data from men with localized and castration - resistant prostate cancer ( crpc ) , our combined cohort of men with dpc was signicantly enriched for mutations in ddr genes ( both mmr and hr genes ) , as well as other genes of interest ( table 2 ) .20 , 21 additional recurrent genomic alterations . 
similar to localized and metastatic crpc , mutations in foxa1 were frequently observed ( n = 17 ; 33% ) .20 , 21 interestingly , mutations in genes involved in wnt signaling were also frequent ( n = 16 ; 31% )  . 
this includes activating / stabilizing mutations in ctnnb1 ( n = 4 ) , as well as inactivating mutations in apc ( n = 12 ) , a negative regulator of wnt pathway activation . 
pathogenic mutations were those predicted to either activate oncogenic signaling pathways ( eg , wntor pi3k - signaling ) or inactivate tumor suppressors ( eg , dna damage repair [ ddr ] genes , tp53 )  . 
hr , homologous recombination ; mmr , mismatch repair ; vus , variant of uncertain signicance . alterations co - occurred with pi3k - pathway alterations , including one patient with an apc and pik3ca mutation , and two patients with ctnnb1 and pik3ca mutations . 
compared with patients with crpc , there were fewer pten alterations and more pik3ca mutations in our dpc cohort , with an overall similar incidence of pi3k - pathway alterations ( table 2 )  . 
alterations in ar were infrequent ( n = 4 ; 8% ) ; however , the majority of tissue samples sequenced were primary prostate tissue that had not been exposed to hormonal therapies . 
although the quantity of dpc in each patient varied , there was no evidence that percentage of ductal involvement correlated with the underlying mutational prole , and a high frequency of ddr mutations was observed regardless of the overall quantity of dpc reported on secondary pathology review ( table 3 )  . discussion to our knowledge , this is the largest cohort of dpc to be examined by ngs . 
mutational frequencies for comparator data sets were derived from either the primary publications or extracted from cbioportal.20 - 23 cancer genome atlas . abbreviations : ddr , dna damage repair ; hr , homologous recombination ; mmr , mismatch repair ; rr , relative risk ; su2c , stand up 2 cancer ; tcga , the * the tcga data set comprises 333 men with localized prostate cancer.20 su2c - pcf international prostate cancer dream team discovery set comprises 150 men with metastatic castration - resistant prostate cancer . 
one patient classied as positive for ductal involvement did not provide an estimate on percent involvement . abbreviations : ddr , dna damage repair ; hrd , homologous recombination deciency ; mmr , mismatch repair . * three patients were indeterminate regarding whether the ddr alteration was germline versus somatic and were therefore excluded from this analysis . archival tissue , negating the need to obtain fresh metastatic tissue in men with more advanced disease . 
although we did not intentionally sequence the acinar carcinoma component in patients with mixed ductal - acinar tumors , the fact that concurrent ductal and acinar carcinomas share common erg rearrangements and other alterations suggests that the ddr alterations are likely shared between these components as well.4 , 9 this study adds to the literature suggesting that aggressive histologic subtypes of localized prostate cancer ( eg , primary gleason pattern 5 acinar carcinomas , small cell carcinomas , and now dpcs ) may be enriched for mmr defects.25 it is also notable that in addition to ddr alterations , there were a number of recurrently mutated genes , including those involved in wntand pi3k - signaling pathways . interestingly , and consistent with prior work from our group , we found that pi3k - signaling alterations occurred more commonly in ductal carcinoma via pik3ca mutations than by pten gene alterations , which is in contrast to unselected patients with metastatic crpc.6 , 21 these ndings are also consistent with a recent report examining genomic and transcriptomic differences between dpc and acinar prostate cancer foci from the same individual.9 however , in that report , it is worth noting that the authors did not observe enrichment for mmr alterations , and ddr alterations were relatively infrequent . 
we also conrmed that ets gene rearrangements were signicantly less common in patients with dpc compared with both primary ( the cancer genome atlas ) and metastatic ( stand up 2 cancerprostate cancer foundation ) patients with prostate cancer.4 importantly , because the ngs panel used in this study ( uw - oncoplex ) provides intronic gene coverage for rearrangement hotspot areas in tmprss2 and other recurrently rearranged genes , it has a higher degree of sensitivity for detecting ets fusions and other complex genomic rearrangements that could be missed by panels that only sequence exonic regions.13 , 26 these ndings indicate that alternative drivers may underlie dpc biology . another interesting observation was the apparent enrichment in patients with dpc for germline ddr gene alterations . 
in contrast , the uw cohort comprised prospectively identied men receiving care for prostate cancer in the clinic , and thus represented a real - world example of selecting patients for sequencing on the basis of histology . another key difference is that the jhh cohort only included patients who underwent prostatectomy , and no long - term follow - up data were available . 
given that all patients in the jhh cohort were considered to be prostatectomy candidates , this raises the possibility that these men had less aggressive disease , especially in light of the fact that 70% of men in the calgary and uw cohorts either died or developed metastatic disease . it is also notable that the uw cohort included a number of patients who were disputed in terms of whether dpc was present , and overall , 12 patients ( 26% ) included in this series who underwent secondary pathology review were felt to not contain signicant ductal features ( n = 11 from uw and n = 1 from jhh )  . 
 ductal prostate cancer genomics however , that all patients included in this analysis were believed to contain a component of ductal histology by at in addition , least one expert genitourinary pathologist . because slides from uw were not scanned before macrodissecting the ductal component , we cannot exclude the possibility that the slides sent for secondary review were not representative of the slides used for sequencing . 
in addition , the observed interpathologist variance is consistent with prior experience evaluating patients with dpc.28 importantly , there were no clear differences in mutational proles for patients felt to not possess a clear ductal component on secondary pathology review or between patients with pure versus mixed ductal histology ( table 3 )  . larger studies aimed at evaluating differences between patients with pure and mixed dpc and studies evaluating differences between ductal and acinar foci from the same patient are warranted but are beyond the scope of this study . in conclusion , despite the heterogeneity of our cohort , these results indicate that patients with any fraction of dpc should be offered ngs , given that the presence of dpc histology can serve as a rapid means to select patients enriched for actionable mutations , particularly in mmr and hr genes . 
schweizer consulting or advisory role : janssen research funding : janssen ( inst ) , astrazeneca ( inst ) , roche ( inst ) , pzer ( inst ) , zenith epigenetics ( inst ) , madison vaccines ( inst ) emmanuel s . 
antonarakis honoraria : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : co - inventor of a biomarker technology that has been licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation heather h . 
cheng research funding : inovio pharmaceuticals ( inst ) , sano ( inst ) , astellas medivation ( inst ) , janssen ( inst ) , clovis oncology ( inst ) , color foundation ( inst ) eric q . 
hsieh honoraria : hotspot therapeutics research funding : effector ( inst ) patents , royalties , other intellectual property : mtor modulators and uses thereofpatent number : 9629843 , use of translational proling to identify target molecules for therapeutic treatmentpublication number : 20140288097 peter s . 
nelson consulting or advisory role : janssen oncology , astellas pharma , genentech expert testimony : veneble - fitzpatrick law firm travel , accommodations , expenses : janssen oncology evan y . 
yu consulting or advisory role : janssen , bayer , merck , astrazeneca , emd serono , churchill pharmaceuticals , incyte , amgen , tolmar , qed , dendreon , seattle genetics , agensys ( inst ) , astellas pharma ( inst ) , dendreon ( inst ) , genentech ( inst ) , bayer ( inst ) , merck ( inst ) , seattle genetics ( inst ) r . 
true stock and other ownership interests : lightspeed micro research funding : ventana medical systems patents , royalties , other intellectual property : lens on an open - top lightsheet microscope jonathan i . 
histopathology 60 : 59 - 74 , 2012 brinker da , potter sr , epstein ji : ductal adenocarcinoma of the prostate diagnosed on needle biopsy : correlation with clinical and radical prostatectomy ndings and progression . 
am j surg pathol 23 : 1471 - 1479 , 1999 lotan tl , toubaji a , albadine r , et al : tmprss2 - erg gene fusions are infrequent in prostatic ductal adenocarcinomas . 
prostate 75 : 1610 - 1619 , 2015 vinceneux a , bruyere f , haillot o , et al : ductal adenocarcinoma of the prostate : clinical and biological proles . 
prole 77 : 1242 - 1250 , 2017 chaux a , albadine r , toubaji a , et al : immunohistochemistry for erg expression as a surrogate for tmprss2 - erg fusion detection in prostatic adenocarcinomas . 
am j surg pathol 35 : 1014 - 1020 , 2011 gillard m , lack j , pontier a , et al : integrative genomic analysis of coincident cancer foci implicates ctnnb1 and pten alterations in ductal prostate cancer . 
mod pathol 22 : 1273 - 1279 , 2009 jeong su , kekatpure ak , park jm , et al : diverse immunoprole of ductal adenocarcinoma of the prostate with an emphasis on the prognostic factors . 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . 
herawi m , epstein ji : immunohistochemical antibody cocktail staining ( p63 / hmwck / amacr ) of ductal adenocarcinoma and gleason pattern 4 cribriform and noncribriform acinar adenocarcinomas of the prostate . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
shlien a , campbell bb , de borja r , et al : combined hereditary and somatic mutations of replication error repair genes result in rapid onset of ultrahypermutated cancers . 
true l , gulati r , lange j , et al : histological patterns of ductal adenocarcinoma of prostate correlates with mutations in dna repair genes and may aid in selecting the type of systemic therapy for castration - resistant prostate carcinoma . 
 ductal prostate cancer genomics isaacsson velho p , silberstein jl , markowski mc , et al : intraductal / ductal histology and lymphovascular invasion are associated with germline dna - repair gene mutations in prostate cancer . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
 comprehensive analysis of the unfolded protein response in breast cancer subtypes purpose triple - negative breast cancers ( tnbcs ) are associated with a worse prognosis and patients with tnbc have fewer therapeutic options than patients with non - tnbc . 
recently , the ire1a - xbp1 branch of the unfolded protein response ( upr ) was implicated in tnbc prognosis on the basis of a relatively small patient population , suggesting the diagnostic and therapeutic value of this pathway in tnbcs . 
in addition , the ire1a - xbp1 and hypoxia - induced factor 1 a ( hif1a ) pathways have been identified as interacting partners in tnbc , suggesting a novel mechanism of regulation . 
to comprehensively evaluate and validate these findings , we investigated the relative activities and relevance to patient survival of the upr and hif1a pathways in different breast cancer subtypes in large populations of patients . materials and methods we performed a comprehensive analysis of gene expression and survival data from large cohorts of patients with breast cancer . 
the patients were stratified based on the average expression of the upr or hif1a gene signatures . results we identified a strong positive association between the xbp1 gene signature and estrogen receptorpositive status or the hif1a gene signature , as well as the predictive value of the xbp1 gene signature for survival of patients who are estrogen receptor negative , or have tnbc or her2 +  . 
2017 by american society of clinical oncology introduction triple - negative breast cancers ( tnbcs ) represent a breast cancer subpopulation lacking estrogen receptor ( er ) , progesterone receptor ( pr ) , and her2 expression.1 patients with tnbc have a worse prognosis than those with non - tnbc , suggesting more aggressive biologic behavior . 
the unfolded protein response ( upr ) is an adaptive process to alleviate endoplasmic reticulum stress during tumor growth and proliferation.2 one major upr signaling pathway , ire1a leading to activation of xbp1 , is implicated in multiple types of cancers , including breast cancer.3 a recent study reported that tnbc cell lines and primary tumor samples from patients with tnbc express higher levels of the activated form of xbp1 than non - tnbc.4 furthermore , this study also revealed that in tnbc cells , xbp1 coregulates hif1a target genes , and that both xbp1 and hif1a gene signatures were associated with poor prognosis in tnbc , but not in patients with er + breast cancer . 
for example , the expression of esr1 , gata3 , and xbp1 were highly correlated in breast cancer.5 , 6 in addition , xbp1 enhances the transactivation activity of era7 and was identified as an estrogenresponsive gene.8 recently , our laboratory identified that doxorubicin , a widely used chemotherapeutic agent in breast cancer treatment , is a potent inhibitor of xbp1 activation.9 therefore , clarifying the role of xbp1 in breast cancer prognosis would not only improve the application of existing treatment strategy but also would dadi jiang brandon turner jie song ruijiang li maximilian diehn quynh - thu le purvesh khatri albert c . 
using the same four luminal and six basal - like cell lines reported by chen et al , 4 ( a ) average expression of the xbp1 gene signature was higher in the luminal type , although not statistically significant , whereas ( b ) average expression of the atf4 / chop signature was significantly higher in the basal - like type . 
the cell line collection consists of 19 estrogen receptor ( er ) + and 32 er , or 25 triple - negative breast cancer ( tnbc ) and 26 non - tnbc cell lines defined on the basis of mrna / protein levels of er / progesterone receptor / her2 . 
 ( e ) the same analysis on microarray data of patients with breast cancer from the cancer genome atlas database ( n = 404 er + and n = 118 er , or n = 91 tnbc and n = 431 non - tnbc )  . 
 support the preclinical development of therapy on the basis of modulating xbp1 activity.10 , 11 in this study , we comprehensively investigated the activity of xbp1 , its relationship with the er status as well as the hif1a pathway , and its prognostic value in a large group of patients with breast cancer . 
the rnaseq ( n = 1 , 182 ; illumina hiseq ; illumina , san diego , ca ) and microarray ( n = 597 , a subset of the 1 , 182 patients ; agilentg4502a_07_3 array ; agilent technologies , santa clara , ca ) data with the clinical information of the patients with breast cancer were downloaded from the cancer genome atlas ( tcga ) database through the university of california santa cruz cancer browser . 
all signature and expression data were normalized as z - scores with a mean of 0 and standard deviation of 1 . differences in average expression ( microarray or rnaseq ) level of the gene signatures by er and tnbc status were assessed using the nonparametric wilcoxon rank - sum test . 
mrna expression levels of foxa1 , esr1 , and gata3 were first individually normalized ( mean , 0 ; standard deviation , 1 ) and then averaged together before comparing with either the xbp1 gene signature expression or xbp1 gene expression using regression . 
cox proportional hazards regression models were fit to breast cancer survival data , and the nonparametric log - rank test was used to test for significant differences in relapse - free survival ( rfs ) between subtypes of patients with high or low levels of average xbp1 , atf4 / chop , or hif1a gene signature expression . 
patient survival data up to 150 months were used for the analysis . cell culture and viability assay mda - mb - 231 , hs578t , mda - mb - 468 , mcf7 , t47d , and bt474 cells were purchased from american type culture collection ( manassas , va ) and maintained in dmem supplemented with 10% fetal bovine serum and 1% penicillinstreptomycin , and cells were cultured at 37c with 5% co2 . 
after 72 hours of treatment , xtt reagent ( american type culture collection ) was added to the wells , then cells were incubated for 2 hours , and cell viability was calculated with the following formula : absorbance = a475nm ( test ) a475nm ( blank ) a660nm ( test ) using a biotek synergy h1 plate reader ( biotek , winooski , vt )  . results first , we tested the initial conclusion of the previous study4 that basal - like breast cancer cell lines , which consist primarily of tnbc cells , express higher levels of the spliced / activated form of xbp1 compared with those of the luminal type , which consist primarily of er + cells.4 we found the average expression of the same xbp1 gene signature used by the previous investigators to measure xbp1 activity4 was actually higher in the same set of luminal ( n = 4 ) than basal - like ( n = 6 ) cell lines , albeit without statistical significance ( fig 1a )  . 
 2 average expression of the xbp1 gene signature was significantly higher in er + compared with cell lines , consistent with previous reports ( fig 1c ) .5 - 8 however , there was no statistically significant difference in the xbp1 signature between tnbc and non - tnbc cell lines ( fig 1c )  . in contrast , expression of the atf4 / chop sigor tnbc than in er + or nature was higher in er non - tnbc cell lines , respectively ( fig 1c )  . in established cell these observations lines prompted us to evaluate these pathways in tumor samples from patients with breast cancer . 
we performed the same analyses on 1 , 182 patients with breast cancer from tcga , on the basis of rnaseq ( fig 1d ) , 5 or a subset of 597 patients on the basis of microarray ( fig 1e ) , as well as 1 , 809 curated microarray gene expression profiles ( fig 1f ) .14 in each comparison , we found expression of the xbp1 gene signature was significantly higher in er + or non - tnbc than in er or tnbc tumor samples , respectively . 
overall , we identified a strong correlation between the expression of xbp1 , which is also a transcriptional target of activated xbp1 itself , 4 and er pathway genes ( ie , esr1 , gata3 , and foxa1 ; fig 2a and 2b )  . 
this relationship was also significant when we correlated the average expression of the xbp1 gene signature with the average er pathway gene expression ( fig 2c and 2d )  . these data are consistent with a previous report of xbp1 playing a crucial role in 17 - b - estradiolinduced growth of er + breast cancer cells.15 to test the reported coregulation of target gene expression by activated xbp1 and hif1a4 in a large cohort of patients with breast cancer , we performed similar correlation analysis using the tcga dataset . 
overall , we found a strong correlation between the xbp1 and hif1a gene signatures in patients either er + or er , and with non - tnbc or tnbc , who were from tcga ( fig 2e and 2f )  . 
this result confirms the molecular - level interaction between the two pathways with large - scale gene - expression data from patients and suggests the xbp1 and hif1a pathways are highly correlated in breast cancer regardless of the subtypes . to assess the influence of the upr and hif1a pathways on survival of patients with breast cancer and extend the analysis of the previous study4 to larger patient cohorts , we performed survival analyses of the 1 , 809 - patient data set , using the same high - low expression cutoff ( 58th percentile ) as previously reported.4 surprisingly , the xbp1 signature was not associated with worse rfs in the whole population of patients with breast cancer ( fig 3a , left )  . 
however , when the patient population was further stratified into tnbc versus , or her2 + versus non - tnbc , er + versus er , higher expression of the xbp1 signature her2 was associated with worse rfs in tnbc ( fig 3b , ( fig 3c , left ) , or her2 + ( fig 3d , left ) left ) , er patients , but not in patients positive for er ( fig 3c , left ) or negative for her2 ( fig 3d , left )  . 
interestingly , the atf4 / chop signature was not associated with rfs ( fig 3a , middle ) , even after stratification into either tnbc / non - tnbc , er + / 2 her2 + / 2 status ( fig 3b - 3d , middle )  . 
in contrast , the hif1a signature was significantly associated with rfs regardless of how the patients were stratified ( fig 3a - 3d , right )  . to evaluate whether using gene signature expression cutoffs at the extremes would reveal stronger association , we applied quartile ( the highest 25% v the lowest 25% ) cutoff and performed the same survival analysis . 
the atf4 / chop signature became significantly associated with rfs in the whole population ( data supplement ) and the xbp1 signature became significantly associated ( data with rfs in patients who were her2 supplement )  . 
however , the positive association between the xbp1 signature and rfs in the patients with non - tnbc using the 58th percentile cutoff became negative when using the quartile cutoff , which likely was due to the reduced number of patients in the new categories ( data supplement )  . 
nevertheless , the major conclusions of the current study remain unchanged . discussion in summary , on the basis of a comprehensive analysis on large cohorts of patients with breast cancer , our findings confirm the initial observations from chen et al4 that xbp1 activity was associated with a worse prognosis in tnbc , but not er + patients , and extend this relationship to ( fig 3c , left )  . 
correlation of xbp1 mrna expression and the xbp1 gene signature with estrogen receptor ( er ) pathway gene expression and correlation of the xbp1 and hif1a gene signatures in the the cancer genome atlas ( tcga ) breast cancer data set . 
correlation analysis of expression of the xbp1 gene and the average of three er pathway genes ( esr1 , foxa1 , and gata3 ) using ( a ) rnaseq or ( b ) microarray data from 1 , 182 patients with breast cancer in tcga breast cancer database and the same correlation analysis of the average expression of the xbp1 gene signature and the three er pathway genes on the basis of ( c ) rnaseq or ( d ) microarray data in the tcga database . 
 ( e , f ) correlation of the average expression of the xbp1 and hif1a gene signatures in the groups of patients with breast cancer , on the basis of the rnaseq data in the tcga database : ( e ) er + ( n = 600 patients , gold ) and er ( n = 179 patients , blue ) ; and ( f ) triple - negative breast cancer ( tnbc ; n = 125 patients , blue ) and non - tnbc ( n = 647 patients , gold )  . 
kaplan - meier graphs showing relapse - free survival ( rfs ) of the different subtypes of patients with breast cancer stratified by the xbp1 , atf4 / chop , or hif1a gene signatures . 
kaplan - meier graphs of rfs of ( a ) the total of 1 , 640 patients , ( b ) 225 patients with triple - negative breast cancer ( tnbc ) and 1 , 415 with non - tnbc , ( c ) 1 , 286 who are estrogen receptor ( er ) + and 354 who are er with rfs < 150 months separated by high and low ( with the 58th percentile cutoff used previously4 ) levels of the average expression of the xbp1 ( left column ) , atf4 / chop ( middle column ) , or hif1a ( right column ) gene signature . 
this may partially explain those who are her2 why the xbp1 - rfs association is stronger in than in those with tnbc patients who are er ( fig 3b and 3c , left ) , because some of the patients / her2 + are included in the patients who are er but not in the patients with tnbc . who are er however , through analyzing large - scale gene expression profiles , we identified that average expression of the same xbp1 gene signature reported by chen et al4 was higher in er + or non - tnbc or tnbc cell lines or patients , respecthan er tively ( fig 1c - 1f ) , to correct the initial conclusion by chen et al.4 these data are consistent with other previous studies . 
our findings suggest that , albeit with higher xbp1 activities , patients who are er + , and other patients with non - tnbc ( excluding her2 + ) , may not benefit from therapeutic strategies targeting xbp1 activity . 
the design and aims of the current study are summarized in the schematic shown in the data supplement . recently , we have shown that doxorubicin blocks xbp1 activation through the inhibition of ire1a rnase activity.9 these data suggest that pa , and possibly tients with tnbc , who are er those who are her2 + , may benefit the most from anthracycline - based therapies . 
davies mp , barraclough dl , stewart c , et al : expression and splicing of the unfolded protein response gene xbp - 1 are significantly associated with clinical outcome of endocrine - treated breast cancer . 
finlin bs , gau cl , murphy ga , et al : rerg is a novel ras - related , estrogen - regulated and growth - inhibitory gene in breast cancer . 
j biol chem 276 : 42259 - 42267 , 2001 jiang d , lynch c , medeiros bc , et al : identification of doxorubicin as an inhibitor of the ire1a - xbp1 axis of the unfolded protein response . 
jiang d , niwa m , koong ac : targeting the ire1a - xbp1 branch of the unfolded protein response in human diseases . semin cancer biol 33 : 48 - 56 , 2015 11 . 
gy orffy b , lanczky a , eklund ac , et al : an online survival analysis tool to rapidly assess the effect of 22 , 277 genes on breast cancer prognosis using microarray data of 1 , 809 patients . 
sengupta s , sharma cg , jordan vc : estrogen regulation of x - box binding protein - 1 and its role in estrogen induced growth of breast and endometrial cancer cells . 
lacroix m , leclercq g : about gata3 , hnf3a , and xbp1 , three genes co - expressed with the oestrogen receptoralpha gene ( esr1 ) in breast cancer . 
tozlu s , girault i , vacher s , et al : identification of novel genes that co - cluster with estrogen receptor alpha in breast tumor biopsy specimens , using a large - scale real - time reverse transcription - pcr approach . 
andres sa , wittliff jl : relationships of esr1 and xbp1 expression in human breast carcinoma and stromal cells isolated by laser capture microdissection compared to intact breast cancer tissue . 
wang dy , fulthorpe r , liss sn , et al : identification of estrogen - responsive genes by complementary deoxyribonucleic acid microarray and characterization of a novel early estrogen - induced gene : eeig1 . 
karn t , metzler d , ruckhaberle e , et al : data - driven derivation of cutoffs from a pool of 3 , 030 affymetrix arrays to stratify distinct clinical types of breast cancer . 
 e role of community - based genomics programs see accompanying article doi : increasingly , genomic changes in patients tumors are used to inform individualized management , although the optimal approach and impact of tumor profiling on cancer care , especially in the community setting , remain important research questions.1 , 2 challenges in applying precision medicine approaches include cost and access to genomic testing and to indicated therapies , lack of actionable gene alterations , education of all stakeholders , patient expectations , complexity of interpretation of data , access to big data solutions , and expansion of physicians comfort zones . 
arguably , the latter represents the most formidable challenge . in the article accompanying this editorial , burkard et al3 address many of these challenges in their report , implementation and clinical utility of an integrated academic - community regional molecular tumor board . 
the implementation of a novel wisconsin state - wide model , including a precision - medicine molecular tumor board ( pmmtb ) , an institutional review boardapproved registry protocol , and a journal club , allows for addressing many of the challenges of precision medicine . 
the authors point out that in the united states , much of precision medicine is implemented in an academic - center context , often in conjunction with robust clinical trial platforms , to include big data analytic informatics solutions . conversely , most patients are cared for outside of such academic systems.4 the challenge is to provide patients access , through their community - based providers , to the potential benefits of precision medicine . 
the described model is an academic and community partnership that allows for nextgeneration sequencing ( ngs ) through any clinical laboratory improvement amendmentscertified laboratory , and uses as its cornerstone a twiceweekly web - based pmmtb teleconference , provided as a free service . 
as with most molecular tumor boards ( mtbs ) , the focus is on prioritizing labeled and off - label therapies , as well as clinical trial options , on the basis of biologic profiling of the patients tumor . 
the model addresses the increasingly dynamic nature of the molecular pathology report with its interpretation of a specific genotype and its clinical importance often becoming outdated in the short term . the presence of an institutional review board approved registration trial assists in observing the clinical course of patients to include relevant outcomes . 
patients may have molecular profiling performed early in their clinical course ; thus , long - term follow - up allows for evaluating the downstream impact of the original molecular profiling or that of any subsequent repeat molecular profiling . this type registry is especially important given the uncertainties regarding the value proposition of precision medicine in daily practice . 
the construct of this tripartite model seeks to address the challenges of precision medicine , though the results reported by burkard et al3 emphasize the remaining barriers to successful implementation of precision medicine platforms in community settings and beyond . over approximately 1 year , a modest number of patients with metastatic / incurable cancer ( n 5 74 ) were presented at the pmmtb ; only 38 evaluable patients were enrolled in the registration trial , and some of these were enrolled retrospectively . 
 actionable target ( ie , molecularly targeted clinical trial and / or off - trial treatment ) was identified in 32 patients , with treatment accepted in only nine patients ( 28% )  . 
only one patient was enrolled in an instate clinical trial , although a total of 14 patients had clinical trial options within the state , and no patients were enrolled in out - of - state clinical trials . 
during much of the reported period in the registry trial , the national cancer institute molecular analysis for therapy choice ( match ) basket trial was on hold , and there was no access to the asco targeted agent and profiling utilization registry ( tapur ) basket trial . 
clinical benefit was seen in three of eight ( 38% ) evaluable patients , with a response evaluation criteria in solid tumors ( recist ) - defined response in one patient . this novel precision - medicine model aims at networking academic and community providers to deliver genomically driven care to patients closest to where they live and under the care of their community physicians . 
what role does cost play with regard to accessing ngs testing and targeted drugs ? given the wide range of ngs testing platforms , how is quality assured ? this is especially important because clinical laboratory improvement amendments certification does not address many quality dimensions inherent to ngs testing . in this report , the mean number of prior therapies for patients was two . 
when is the most effective time to perform ngs testing during a patients clinical course : earlier or later ? similarly , a range of ngs panel sizes was used , with a not - surprising suggestion that larger comprehensive panels are more frequently associated with treatment options . where does cost effectiveness guide us in selecting ngs panel size ? with regard to actionable gene alterations , it is remarkable that by recent analysis , the us food and drug administration has only approved 22 gene alterations with associated biomarkers.7 , 8 the key to defining labeled indications for targeted therapies is participation in clinical trials such as match and tapur . additional clinical trial approaches include prospective registration - type trials that contain detailed data elements , including demographic data , clinical outcomes measures , and quality - of - life and economic metrics that allow for long - term follow - up and planned statistical analyses . one aspect not referenced in the burkard et al3 report is the underlying informatics platforthe scalability of such a platform , as well as its interfacing capabilities , along with its analytic functions , are key , especially across a multisite network . 
in particular , a clinical - trials matching function that allows for prioritizing variables such as geographic distance and relevance to an individual patients unique characteristics , and those of their tumor , will facilitate identification of the most promising clinical trials for a given patient . 
in addition , engaging busy clinicians is always a challenge , and one presumed solution is to have approaches and platforms that align with their daily work flow , including integration into existing informatics platforms , most especially the electronic medical record , along with automatic extraction of data elements from existing electronic databases , which limits the need for form completion , whether electronic or manual . 
for example , maximal use of high quality databases , such as tumor registries or the seer program database , can help overcome the challenges of relying on semistructured data within the electronic medical record . the demonstration of the value proposition for precision medicine is a work in progress . 
it will require clinical trial experience with genomically driven therapies across a broad population of patients with varied tumor types , cared for by a range of providers , and in varied settings , to include the broad variety of community practices . 
the newer formulation of clinical trial design , whether the basket or umbrella type design or that of sophisticated registry trials , such as those described by burkard et al , will substantially facilitate the access to targeted therapy trials in the community setting.9 , 10 these trials provide guidance for community physicians in identifying gene alterations or biomarkers with appropriate targeted therapies and provide access to off - label targeted therapies . 
brown td , tittel pd , gold pj , et al : impact of a personalized medicine research program ( pmrp ) , using targeted tumor profiling and a cloud based clinical trials matching platform , on clinical decision - making . 
of interest , previous reports have identified germline mutations in driver oncogenes that are associated with lung cancers , such as epidermal growth factor receptor ( egfr ) , 1 - 6 receptor tyrosine - protein kinase erbb - 2 ( erbb2 ) , 7 and possibly others , 8 which suggests that heritable predisposition to lung cancer is a contributor in some cases . 
in this work , we describe a novel germline egfr v769m variant in a patient with multiple lung cancers , each of which harbors co - occurring somatic mutations in egfr . 
to our knowledge , we also describe for the first time the activating and sensitizing characteristics of egfr v769m in preclinical and in silico structural models . a 57 - year - old man was found to have five distinct lung nodules and no mediastinal or hilar lymphadenopathy , which raised the possibility of multiple synchronous lung cancers . 
the patient was a remote former smoker ( 34 packyears ) , quitting 21 years before presentation . he underwent several procedures to resect the five distinct lung nodules , each of which was determined to be lung adenocarcinoma . 
molecular analysis was performed on the five tumors and each revealed an egfr v769m alteration . in addition , the presence of distinct g719 mutations in egfr in several tumors suggested that these tumors represented independent primary lung cancers ( table 1 and appendix fig a1 , online only )  . as v769m is predicted to have a significant functional impact ( polyphen9 ) , the possibility of a germline variant was considered . 
the co - occurring somatic variant in exon 20 ( egfr s768i ) was found on the same allele as the germline egfr v769m . it was not possible to determine conclusively whether somatic mutations in exon 18 were similarly in cis with the germline variant given the genomic distance between the variants , which were captured separately and sequenced on distinct short reads in the genomic dna - based assay that was performed . 
he has remained without evidence of progressive disease or new lesions for more than 3 years . the egfr v769 codon is in exon 20 and corresponds to the region just after the c - helix of the egfr kinase domain.10 this variant is uncommonly identified in public databases ( 2 of 120 , 770 alleles in exome aggregation consortium11 ; 1 of 13 , 005 alleles in exome variant server12 )  . 
cases of ( presumably ) somatic egfr v769m mutations have been reported13 - 16 ; one patient received treatment with egfr tyrosine kinase inhibitors with no clinical response.14 as the functional and sensitizing impact of egfr v769m has not been ascopubs.org / journal / po jco precision oncology matthew d . 
consistent with an activated phenotype , p - akt ( s473 ) / akt and p - erk ( t202 / y204 ) / erk were increased in egfr v769m mutant compared with wild - type cells in an egf ligand - dependent setting ( fig 3 )  . 
the percent activation , quantified by the ratio of pegfr ( y1068 ) to total egfr , was inhibited by 50% in egfr v769m cells at an erlotinib concentration of 0.4 mm compared with 0.01 mm in egfr l858r cells ; 50% inhibition was not reached in egfr t790m cells at the doses fig 1 . 
to explore the functional impact of comutations in egfr on egfr v769m , we also examined 293t cells that were transfected with egfr v769m + g719c . activation of downstream pathways and sensitivity to erlotinib were both enhanced in the setting of egfr v769m plus g719c compared with egfr v769m alone ( appendix figs a2 and a3 , online only )  . we also used qualitative in silico structural modeling to assess the predicted functional impact of v769m on egfr kinase activity . 
we examined the location and interactions of the original valine residue in the three - dimensional structure of egfr in both inactive and activated conformations ( fig 5 )  . 
in the inactive conformation , the v769 residue is completely buried in the hydrophobic core of the protein globule where it has multiple noncovalent interactions with atoms of surrounding residues ( fig 5a )  . 
a substitution of the val residue with a large met residue will result in the destruction of molecular interaction and the destabilization of the inactive conformation of the kinase domain the activated conformation , the molecular surrounding of v769 undergoes significant changes , the total number of noncovalent interactions is reduced , and structural rearrangements that involve the dfg loop region facilitate the penetration and stabilization of atp ( fig 5b )  . thus , it is reasonable to hypothesize that the structural accommodation of met residue in the activated conformation costs less energy than in the inactive conformation . 
the total effect of the v769m mutation is an activation of egfr caused by a shift of the energy balance between activated and inactivated conformations as a result of significant destabilization of the inactivated state of the molecule . 
moreover , the quantitative energy balance also favors the activated / open conformation in egfr v769m and each of the comutant scenarios identified in this case ( appendix table a1 , online only )  . 
by contrast , the energy balance does not favor that activated state in the context of egfr v769m plus l858r , which perhaps explains the absence of this combination in our patient or other reported cases . mutant egfr represents a paradigmatic targetable oncogene in lung cancers and is present in almost 20% of lung adenocarcinomas . 
egfr v769m mutation activates mitogen - activated protein kinase and akt signaling . 293t cells were transiently transfected with plasmids that encode wild type ( wt ) egfr or egfr mutants with the following changes : v769m , l858r , and t790m . 
quantification of the protein expression of phospho - epidermal growth factor receptor ( pegfr ) , total egfr , phosphoerk ( perk ) , total - erk , phospho - akt ( pakt ) , and total akt was analyzed by using imagej . 
 ( * ) p , .05 , students t test , each condition compared to pegfr / egfr perk / erk pakt / akt have been several reports of patients with germline egfr t790m mutations that have occurred both sporadically and in families.1 , 3 , 5 , 18 , 19 much like the case we present here , the majority of germline egfr variants that have been detected in lung cancers are associated with secondary , somatic in egfr ( with some activating mutations exceptions1 , 3 , 17 , 19 )  . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . mutations in egfr further contribute to lung cancer oncogenesis . in summary , we describe an egfr v769m germline variant found in a patient with five synchronous lung cancers that represented several distinct primaries . 
our structural modeling and functional studies demonstrate that egfr v769m is activating and intermediately sensitive to erlotinib and support the proposed causal role of this variant in the development of multiple lung cancers in this patient . 
hellmann consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca , medimmune , novartis , janssen research funding : bristol - myers squibb , genentech takuo hayashi no relationship to disclose boris reva no relationship to disclose helena a . 
riely consulting or advisory role : novartis , genentech research funding : novartis ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , infinity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : novartis prasad s . 
robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , abbvie ( inst ) , biomarin ( inst ) , medivation ( inst ) , tesaro ( inst ) travel , accommodations , expenses : astrazeneca maria e . 
paik honoraria : celgene , bristol - myers squibb , lilly , ariad pharmaceuticals consulting or advisory role : celgene , lilly , ariad pharmaceuticals , bristol - myers squibb research funding : celgene , emd serono travel , accommodations , expenses : emd serono marc ladanyi honoraria : merck ( i ) consulting or advisory role : nccn / boehringer ingelheim afatinib targeted therapy advisory committee , nccn / astrazeneca tagrisso rfp advisory committee research funding : loxo pharmaceuticals ( inst ) affiliations matthew d . 
in the closed / inactive conformation , v769 is tightly packed in hydrophobic surroundings formed by the residues of two alpha helices ( 752 to 768 , 812 to 831 ) , betastrand ( 777 to 782 ) and two loop regions ( 769 to 776 and the conserved dfg loop region 855 to 857 , a key structural element that regulates kinase activity )  . 
in the open / active conformation , the three - dimensional ( 3d ) structure of the kinase domain changes drastically ( for example , see flipping of 3d position of glu865 shown in magenta in both panels ) and the molecular packing of v769 is relaxed . the total number of 4 atom - to - atom contacts is reduced from 34 in the closed conformation to 27 in the open conformation . the significant structural rearrangements involving the dfg loop region facilitate the penetration and stabilization of atp molecule ( b ; atp analog shown in brown )  . 
nat genet 37 : 1315 - 1316 , 2005 ikeda k , nomori h , mori t , et al : novel germline mutation : egfr v843i in patient with multiple lung adenocarcinomas and family members with lung cancer . 
ohtsuka k , ohnishi h , kurai d , et al : familial lung adenocarcinoma caused by the egfr v843i germ - line mutation . j thorac oncol 4 : 139 - 141 , 2009 j clin oncol 29 : e191 - e192 , 2011 5 . 
j thorac oncol 7 : 1049 - 1052 , 2012 van noesel j , van der ven wh , van os ta , et al : activating germline r776h mutation in the epidermal growth factor receptor associated with lung cancer with squamous differentiation . 
huang sf , liu hp , li lh , et al : high frequency of epidermal growth factor receptor mutations with complex patterns in non - small cell lung cancers related to gefitinib responsiveness in taiwan . 
wu jy , yu cj , chang yc , et al : effectiveness of tyrosine kinase inhibitors on uncommon epidermal growth factor receptor mutations of unknown clinical significance in non - small cell lung cancer . 
santis g , angell r , nickless g , et al : screening for egfr and kras mutations in endobronchial ultrasound derived transbronchial needle aspirates in non - small cell lung cancer using cold - pcr . 
girard n , lou e , azzoli cg , et al : analysis of genetic variants in never - smokers with lung cancer facilitated by an internet - based blood collection protocol : a preliminary report . 
jama oncol 2 : 104 - 111 , 2016 dnas from five tumor samples and blood were extracted and testing was performed by using a custom gene panel , mskampliseq , which covers 94 cancer - related genes . 
library construction was performed with 20 ng of formalin - fixed , paraffinembedded tumor and matched blood dna by multiplexed amplification of 891 regions tiled by 2 , 126 amplicons . sequencing was performed on an ion torrent pgm ( thermofisher , waltham , ma ) , and data were analyzed with a custom pipeline developed at memorial sloan kettering cancer center . 
aligned bam files generated by torrent suite ( thermofisher , waltham , ma ) were primer trimmed and variant calling was performed to detect single nucleotide and indel variants using varscan2 , which were annotated using annovar . 
for transient transfections , 293t human embryonic kidney cells were transfected ( 2 3 105 cells per well in sixwell plates ) by using fugene6 and 0.8 mg of plasmid dna . 
cells were grown in dmem with high glucose , 10% fetal bovine serum , 2 mm l - glutamine , 10 u / ml penicillin , and 10 mg / ml streptomycin at 37c and 5% co2 . 
after 36 hours , cells were serum starved in media that contained 0.1% serucells were treated with different concentrations of erlotinib ( selleckchem , houston , tx ) for 3 hours . 
three independent experiments were performed for all analyses . forward : 59 - cgaacgcaccggagcacagcactttgatctt - 39 , reverse : 59immunoblotting cells were lysed in 50 mm tris$hcl , ph 8.0 , 150 mm sodium chloride , 5 mm magnesium chloride , 1% triton x - 100 , 0.5% sodium deoxycholate , 0.1% sds , 40 mm sodium fluoride , 1 mm sodium orthovanadate , and complete protease inhibitors ( roche )  . 
after quantitation by bio - rad protein assays ( bio - rad , hercules , ca ) , approximately 50 mg of each sample was separated by gel electrophoresis on 4% to 12%bis - tris precast gels ( thermo fisher scientific life sciences , waltham , ma ) and transferred to 0.2 mm polyvinylidene difluoride membrane ( thermo fisher scientific life sciences ) by using wet / tank blotting systems ( bio - rad )  . 
specific proteins were detected by amersham ecl western blotting detection reagent ( thermo fisher scientific life sciences ) , and the following antibodies : antitotal egfr 1 : 2 , 500 ( bd transduction laboratories ) , antiphospho - egfr ( tyr - 1068 ) 1 : 1 , 000 ( cell signaling technology , danvers , ma ) , antitotal p44 / 42 mitogen - activated protein kinase ( erk1 / 2 ) 1 : 1000 ( cell signaling technology ) , antiphospho - p44 / 42 mitogen - activated protein kinase ( erk1 / 2 ; thr202 / tyr204 ; d13.14.4e ) 1 : 1000 ( cell signaling technology ) , antitotal akt 1 : 1000 ( cell signaling technology ) , antiphospho - akt ( ser473 ; d9e ) , antihorseradish peroxidaseconjugated anti - rabbit ig 1 : 10 , 000 ( r&d systems , minneapolis , mn ) , and horseradish peroxidaseconjugated anti - mouse igg 10 , 000 ( r&d systems )  . quantification of protein expression was analyzed by using imagej 2.0.0 - rc - 30 ( nih , bethesda , md )  . 
modeling of mutations in kinase domain of epidermal growth factor receptor ( egfr ) molecule was done for a chain region l703 - g983 using two template structures , 2gs6 for closed and 2gs7 for open conformations . 
this is a pooled analysis . competing interests the authors declare that they have no competing interests . publishers note springer nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations . author details 1service dhmatologie et thrapie cellulaire , hpital saint antoine , ap - hp , 168 rue du faubourg saint antoine , 75012 paris , france . 
16division of hematology and bone marrow transplantation , the chaim sheba medical center , tel - hashomer , tel aviv university ( tau ) , tel aviv , israel . received : 6 february 2018 accepted : 2 march 2018 reply to s . 
romero - cordoba et al we appreciate the commentary and analysis by romero - cordoba et al1 in their response to our recent article in jco precision oncology.2 our research groups pursue the common goal of elucidating immunologic differences between breast cancers that could inform future immunotherapy strategies . 
all immune metrics , including counts of tumor inltrating lymphocytes and other immune cells , as well as immune gene signatures , represent a continuum and display substantial variations across samples . nevertheless , it is possible to dene more versus less immune - rich cancers by any of these metrics , and for some types of analyses , such dichotomization is necessary , even using an arbitrary threshold . our study focused on the question of whether immune - rich estrogen receptor ( er ) positive and triple - negative ( tn ) breast cancers ( bcs ) have similar or different immune microenvironments . 
to perform this comparison across multiple types of molecular data , we had to dene a shared denition of immunerichness ; we used the 75th percentile of a total tumor inltrating lymphocyte gene expression score , which encompasses the expression of 11 immune cell populations , calculated across all samples as the threshold . 
we were delighted to see that this admittedly arbitrary denition of immune - richness corresponded reasonably well with the tnbc immune classication developed by romero - cordoba et al3 : 62% of our immune - rich cancers were classied as ima ( t cell - inamed ) and 21% as imc ( immune warm )  . 
several tnbc classications have been proposed using this method.3 - 6 despite the high and mostly positive correlation in immune gene expression in breast cancer tissues , the different classication schemas yield discordant results in a substantial minority of cases , partly because of different design principles and partly because of methodology . 
however , which classication schema or molecular marker is most useful in the clinic is yet to be determined in clinical trials . the clear majority of immune biomarker studies in breast cancer focus on tnbc because of the higher prevalence of tumor inltrating lymphocytes in this subtype . 
we hope that our article draws attention to immunotherapy opportunities in er - positive cancers , because in absolute numbers , there are more immune - rich er - positive cancers than immune - rich tnbcs . 
omeara t , marczyk m , qing t , et al : immunological differences between immune - rich estrogen receptor - positive and immune - rich triple - negative breast cancers . 
prado - v azquez g , g amez - pozo a , trilla - fuertes l , et al : a novel approach to triple - negative breast cancer molecular classication reveals a luminal immune - positive subgroup with good prognoses . 
j ez equel p , loussouarn d , gu erin - charbonnel c , et al : gene - expression molecular subtyping of triple - negative breast cancer tumours : importance of immune response . 
 efcacy of lorlatinib in primary crizotinib - resistant adult neuroblastoma harboring alk y1278s mutation antoine vasseur , md1 ; luc cabel , md1 ; romain geiss , md1 ; gudrun schleiermacher , md , phd1 ; ga elle pierron , phd1 ; maud kamal , phd1 ; nina jehanno , md1 ; guillaume bataillon , md1 ; jean - marc guinebretiere , md1 ; and laurence bozec , md1 introduction anaplastic lymphoma kinase ( alk ) encodes a highly conserved receptor tyrosine kinase described as an oncogene in anaplastic large - cell lymphoma and other cancers.1 alk fusions ( mostly alk - eml4 ) represent 3% to 7% of all nonsmall - cell lung cancers ( nsclcs ) , and these tumors are generally sensitive to crizotinib ( a tyrosine kinase inhibitor [ tki ] targeting alk ) as rstline therapy in the metastatic setting.2 neuroblastoma harbors activating somatic alk mutations in 8% to 9% of patients ( up to 14% of high - risk neuroblastomas ) , with mutations occurring in the tyrosine kinase domain at three key positions ( f1174 , f1245 , and r1275 ) , which account for approximately 85% of all alk mutations in neuroblastoma.3 activation of alk may also occur by genomic amplication in 3% to 4% of patients , and it has been suggested that patients with neuroblastoma who have genetic alterations of alk could also be treated with crizotinib.4 in this article , we report , to our knowledge for the rst time , the case of an adult patient with ganglioneuroblastoma harboring a somatic alk y1278s mutation with primary resistance to crizotinib , but which was highly sensitive to lorlatinib , a third - generation tki targeting alk genomic alterations . 
computed tomography ( ct ) the chest , abdomen , and pelvis showed scan of disseminated lymph node and vertebral bone lesions . 123i - metaiodobenzylguanidine ( 123i - mibg ) scintigraphy was positive with bone and lymph node metastases . 
laboratory tests showed normal lactate dehydrogenase levels and increased urinary catecholamines ( normetanephrine , 40 , 825 nmol / l ; metanephrine , 572 nmol / l )  . the patient received rst - line induction chemotherapy according to the rapid cisplatin , vincristine , carboplatin , etoposide , and cyclophosphamide ( cojec ) regimen.5 after eight cycles , stable disease was observed in lymph nodes , and progression was observed in bone lesions . 
four months after chemotherapy , clinical disease progression was observed with bone pain , and urinary catecholamines were increased ( normetanephrine , 104 , 651 nmol / l ; metanephrine , 1 , 208 nmol / l ) despite stable mibg scintigraphy and ct scan . a lymphadenectomy ( left subclavicular lymph node ) was performed before second - line therapy with topotecan and cyclophosphamide was started for complementary molecular and immunohistochemistry analyses . immunohistochemistry revealed expression of alk by 100% of tumor cells . 
targeted next - generation in alk , sequencing found a pathogenic variant ptyr1278ser , with an allelic frequency of 23% ( fig 1 )  . the patient was included in the french acs e protocol ( nct02034981 ; phase 2 study assessing efcacy and safety of crizotinib in patients harboring an alteration on alk , met or ros1 ) , and crizotinib was initiated in june 2017 ( 250 mg taken orally twice per day )  . 
treatment was stopped in october 2017 after rapid progression of symptomatic bone metastasis conrmed by mibg scintigraphy , with marked general physical deterioration ( eastern cooperative oncology group [ ecog ] performance status 3 ) , asthenia , anorexia , and weight loss . 
lorlatinib was then obtained from a pzer compassionate - use program and was initiated ( 100 mg taken orally once per day ) in november 2017 , with a signicant clinical benet after 2 weeks of treatment . after 2 months , the patient was asymptomatic with marked improvement of performance status ( from ecog 3 to ecog 0 )  . 
alk positivity by ( a ) immunochemistry and ( b ) next - generation sequencing . partial reossication of bone metastases in favor of treatment response ( left subclavicular lymph node , largest lymph node target lesion ; fig 2 )  . 
after 10 months , 123i - mibg scintigraphy re - evaluation of treatment showed a good partial metabolic response of the left supraclavicular lymph node inltration as seen on the single photon emission computed tomography scan associated with partial response of bone inltration . 
international society of pediatric oncology europe neuroblastoma group ( siopen ) score for bone extension6 , 7 was 30 on baseline scintigraphy , which decreased to a siopen score of 15 on the re - evaluation scintigraphy ( 50% decrease ; relative mibg score of 0.5 ; fig 3 )  . 
overall response according to the international neuroblastoma response criteria consensus was assessed as a partial response.8 after 12 months ( last evaluation in november 2018 ) , the clinical benet was maintained ( ct scan showed a partial reduction of 33% in tumor size [ recist1.1 ] corresponding to the nadir ; left subclavicular lymph node ; fig 2 )  . 
no toxicity was reported during treatment with lorlatinib except for grade 1 hypertriglyceridemia and grade 1 edema of the lower limbs ( common terminology criteria for adverse events [ ctcae ] v5 )  . discussion to our this case report of adult neuroblastoma shows , knowledge for the rst time , that lorlatinib , unlike crizotinib , can be effective in patients harboring an alk y1278s mutation . 
the most common resistance mutations after crizotinib therapy are the l1196m ( 5% to 10% ) and g1269a ( , 5% ) mutations , 9 and many other mutations have also been reported . 
these mutations confer various mechanisms of resistance , such as catalytic domain alteration , which causes atp competitive inhibitor resistance , as t790m mutation in the epidermal growth factor receptor ( egfr ) mutation alters the conformation and / or the atp - binding afnity of the kinase.10 lorlatinib , a third - generation alk inhibitor that also targets ros1 , is an attractive tki in patients with nsclc pretreated with rstor second - generation alk inhibitors because of its activity against most alk resistance mutations , such as g1202r mutations11 ( fig 4b )  . 
lorlatinib has demonstrated high clinical activity in alkor ros1 - rearranged nsclc in treatment - naive or crizotinib pretreated patients.12 in nsclc , the y1278s alk mutation has not been described in the clinical setting , and the efcacy of lorlatinib in nsclc remains unknown . 
however , a different mutation at the same position , y1278h , has been reported in nsclc cell lines that have the alk - eml4 fusion exposed to accelerated mutagenesis , 13 which was resistant to crizotinib . neuroblastoma is the most common solid tumor in children , but adult patients are exceptional , because fewer than 0.3 patients are diagnosed per million people per year.14 crizotinib has been shown to be less effective in neuroblastoma than in nsclc , in which alk mutations , rather than alk fusions , are a major oncogenic event in nearly 10% of the patients , 15 and alk is the most common somatically mutated gene . 
in a phase i / ii trial ( nct00939770 ; crizotinib in treating younger patients with relapsed or refractory solid tumors or anaplastic large cell lymphoma ) , 11 patients with alk - mutated neuroblastoma were treated with crizotinib . 
crystal structure of ( a ) crizotinib / alk and ( b ) lorlatinib / alk . in neuroblastoma reported that y1278s is oncogenic ( ligand - independent activation ) and that crizotinib is inlines effective in vitro and in vivo in neuroblastoma cell harboring the alk y1278s mutation , whereas lorlatinib seemed to be highly effective.19 y1278s is located in the the alk activation loop . 1278 - yrasyy - 1283 motif of donella - deana et al20 demonstrated the important role of initial phosphorylation of tyrosine y1278 for the a - loop activation in alk - npm fusion . 
a study of the crystal structure of alk conrmed this role and highlighted a tight interaction in the inactive form of alk between the unphosphorylated y1278 and a cysteine at position 1097.21 in our patient , a y1278 mutation from tyrosine to serine the phosphorylation and thus the alk should inhibit activation , 20 but guan et al19 showed in a preclinical study that y1278 phosphorylation in neuroblastomas was not for alk activation ( unlike phosphorylation of essential y1283 , which is essential )  . 
however , this hypothesis was not conrmed , so the mechanism of alk activation with y1278s mutation is controversial.19 the y1278s mutation seems to be a rare mutation , but it has been reported in six neuroblastoma patients ( catalogue of somatic mutation in cancer [ cosmic ] database ) .17 , 22 - 24 no clinical data regarding the efcacy of alk inhibitors were reported in these six tumors harboring a y1278s alk mutation , but in two patients , preclinical data showed an in vitro resistance to crizotinib ( high concentration that inhibits 50% [ ic50 ] )  . 
note that a clinical trial of lorlatinib for patients with alk - driven relapsed or refractory neuroblastoma is ongoing as part of the new approaches to neuroblastoma therapy ( nant ) consortium ; this trial ( nct03107988 ; study of lorlatinib [ pf - 06463922 ] , an oral small molecule inhibitor of alk / ros 1 , for patients with alk - driven relapsed or refractory neuroblastoma ) is not yet recruiting in europe , and results are pending . in conclusion , we show that lorlatinib is effective against the alk y1278s mutation in neuroblastoma , whereas this mutation confers primary resistance to crizotinib . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . gudrun schleiermacher honoraria : bristol - myers squibb research funding : bristol - myers squibb ( inst ) , pzer ( inst ) , msdavenir ( inst ) , roche ( inst ) travel , accommodations , expenses : roche no other potential conicts of interest were reported . references chiarle r , voena c , ambrogio c , et al : the anaplastic lymphoma kinase in the pathogenesis of cancer . 
nat rev cancer 8 : 11 - 23 , 2008 solomon bj , mok t , kim dw , et al : first - line crizotinib versus chemotherapy in alk - positive lung cancer . 
moss e yp , lim ms , voss sd , et al : safety and activity of crizotinib for paediatric patients with refractory solid tumours or anaplastic large - cell lymphoma : a childrens oncology group phase 1 consortium study . 
lancet oncol 14 : 472 - 480 , 2013 pearson ad , pinkerton cr , lewis ij , et al : high - dose rapid and standard induction chemotherapy for patients aged over 1 year with stage 4 neuroblastoma : a randomised trial . 
lancet oncol 9 : 247 - 256 , 2008 lewington v , lambert b , poetschger u , et al : 123i - mibg scintigraphy in neuroblastoma : development of a siopen semi - quantitative reporting , method by an international panel . 
matthay kk , shulkin b , ladenstein r , et al : criteria for evaluation of disease extent by ( 123 ) i - metaiodobenzylguanidine scans in neuroblastoma : a report for the international neuroblastoma risk group ( inrg ) task force . 
br j cancer 102 : 1319 - 1326 , 2010 park jr , bagatell r , cohn sl , et al : revisions to the international neuroblastoma response criteria : a consensus statement from the national cancer institute clinical trials planning meeting . 
shaw at , felip e , bauer tm , et al : lorlatinib in non - small - cell lung cancer with alk or ros1 rearrangement : an international , multicentre , open - label , singlearm rst - in - man phase 1 trial . 
yoda s , lin jj , lawrence ms , et al : sequential alk inhibitors can select for lorlatinib - resistant compound alk mutations in alk - positive lung cancer . 
cancer discov 8 : 714 - 729 , 2018 3 : 108ra114 , 2011 cell 26 : 682 - 694 , 2014 infarinato nr , park jh , krytska k , et al : the alk / ros1 inhibitor pf - 06463922 overcomes primary resistance to crizotinib in alk - driven neuroblastoma . 
donella - deana a , marin o , cesaro l , et al : unique substrate specicity of anaplastic lymphoma kinase ( alk ) : development of phosphoacceptor peptides for the assay of alk activity . 
lee cc , jia y , li n , et al : crystal structure of the alk ( anaplastic lymphoma kinase ) catalytic domabiochem j 430 : 425 - 437 , 2010 22 . 
de brouwer s , de preter k , kumps c , et al : meta - analysis of neuroblastomas reveals a skewed alk mutation spectrum in tumors with mycn amplication . 
clin cancer res 16 : 4353 - 4362 , 2010 janoueix - lerosey i , lequin d , brugi `eres l , et al : somatic and germline activating mutations of the alk kinase receptor in neuroblastoma . 
cgp altered physician treatment selection in 25% of evaluable patients ( n = 7 of 28 ) and was associated with improved progression - free survival . conclusion to our knowledge , this is the largest technical evaluation of the performance of cgp in sarcoma . cgp was effectively performed in the vast majority of sarcoma samples and altered physician treatment selection . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction sarcomas are uncommon , highly morbid cancers that constitute approximately 1% of all adult malignancies . currently , more than 70 recognized histologic subtypes exist , which makes them extremely challenging to accurately diagnosis and treat.1 sarcomas have multiple genomic alterations , including copy number changes , point mutations , insertions and deletions , and fusions.2 - 4 thus , detailed rna and dna sequence analysis is key for diagnosis as well as for treatment decision - making.5 is not surprising , that comprehensive therefore , genomic proling ( cgp ) is increasingly being used in the evaluation and management of bone and soft tissue sarcomas . 
cgp is the sequencing of dna and rna from tumor samples , which enables the identication of known and novel alterations that may drive inherent oncogenicity.6 - 9 cgp may rene the histologic tumor diagnosis , with its management.10 , 11 indeed , in a study by groisberg et al1 specic to sarcomas , the authors found 61% of 102 patients in a retrospective cohort had a potentially actionable genomic target . ramications despite the potential role that cgp may have in the treatment of sarcoma , the impact of dnaand rnabased cgp on physician decision - making is poorly documented.12 , 13 similarly , it is equally unclear what factors may contribute to the success or failure of cgp in an outpatient clinical setting . 
 challenges in sarcoma comprehensive genomic proling as mentioned previously is unknown ; neither are the relative contributions of biopsy site ( bone v soft tissue ) and methods ( ie , computed tomography [ ct ] - guided core needle biopsy v open excisional biopsy )  . 
to answer these questions , we herein report the results of two studies : the rst is a prospective clinical trial examining the impact of dnaand rna - based cgp on physician decision - making . the second is a retrospective analysis of the success and failure rates of cgp in an even larger patient cohort , which includes the aforementioned patients . methods sarcoma decision impact clinical trial study design . 
to examine the effects of cgp on physician decision - making , a prospective clinical trial ( the ohio state university [ osu ] institutional review board approval no . osu - 12067 ) was performed in collaboration with foundation medicine . 
the primary objectives of the study were to assess the feasibility and logistics associated with a clinical trial using a commercially available cgp platform ( foundationoneheme ; foundation medicine , cambridge , ma ) in an academic clinical setting and to determine the proportion of patients who would receive a cancer - related therapy based on cgp results . 
progression - free survival ( pfs ) was summarized using kaplan - meier survival analysis . the ohio state retrospective sarcoma study data following : date of sample procurement , method of specimen procurement ( eg , excisional biopsy , needle core biopsy , ne needle aspiration ) , biopsy site , specimen source ( hospital ) , and pathology classication by osu . 
the foundation medicine records were interrogated for all sarcoma samples sent by osu and the following information was compiled : specimen type ( formalin - xed parafn - embedded tissue blocks v unstained slides ) , morphologic tumor purity , dna and rna extraction yield , sequencing metrics , and the nature of the released report ( ie , pass , fail , or qualied )  . 
a qualied report indicates a sample for which it was unable to complete the entire cgp process ( eg , rna extraction , low tumor purity ) but for which some genomic information was obtained . in contrast , a passed report indicates a sample for which dna and rna proling was completed successfully . 
2 analysis was used to calculate the signicance of intergroup alterations . results physician decision - making was prospectively altered for 25% of patients with sarcoma who underwent cgp as part of a decision impact trial , patients with sarcoma whose disease had not yet progressed on the current line of therapy were approached to undergo cgp as part of the study . 
treating oncologists were blinded to cgp results time of progression ( based on imaging results )  . until treating oncologists rst documented their treatment decision for the patient with sarcoma without cgp results . cgp data were then released for review and the treating oncologist would note whether their treatment decision had been altered by the cgp results . 
 a hay et al patients with sarcoma diagnosis ( n = 34 ) treatment recommendations chosen before cgp patients with liposarcoma ( n = 15 ) patients with nonliposarcomatous sarcoma ( n = 19 ) no data on whether recommendation changed ( n = 3 ) did not switch therapy on the basis of cgp results ( n = 8 ) switched therapy on the basis of cgp results ( n = 4 ) no data on whether recommendation changed ( n = 3 ) did not switch therapy on the basis of cgp results ( n = 13 ) switched therapy on the basis of cgp results ( n = 3 ) patients assessed for eligibility ( n = 493 ) excluded ( n = 31 ) misdiagnosed or miscategorized tumors excluded ( n = 16 ) duplicates or no clinical data available excluded ( n = 41 ) samples that failed initial cgp remaining individuals evaluated ( n = 408 ) patients included in analysis ( n = 392 ) patients with preliminary reports ( n = 351 ) total no . 
of patients for whom full cgp analysis was completed ( n = 297 ) qualified ( n = 54 ) samples for which cgp could not be completed fig 1 . 
 ( % ) male female mean age ; median ( range ) , years data 14 ( 50 ) 14 ( 50 ) 57 ; 62 ( 2480 ) no change ( n = 12 ) changed ( n = 5 ) p = .03 altered , six patients received the selected treatment ; one patient died before initiating therapy . 
as an exploratory end point , we noted that the median pfs in the cgp - selected group was 124 days versus 54 days in the noncgpselection group ( p = .03 ; fig 2 )  . cgp was performed on almost 400 patients with sarcoma a total of 392 patients representing 413 unique samples were proled over 3 years . 
l - type sarcomas ( ie , leiomyosarcoma , liposarcoma ) constituted the greatest proportion of cases , and this is indicative by the preponderance of tp53 , rb1 alterations and mdm2 and cdk4 amplications ( table 3 )  . fifty - six of the 413 samples ( 13.6% ) had reports qualied for low tumor purity , failed rna extraction , or suboptimal sequencing metrics , whereas 10.7% ( n = 44 of 413 ) samples failed testing . 
examining sarcoma subtypes individually , leiomyosarcomas ( 74.0% ; n = 57 of 77 ) and liposarcomas ( 79.4% ; n = 50 of 63 ) had proportionally higher pass rates than did bone - based sarcomas . 
chordomas had the lowest successful initial genomic proling rate , with a 43% initial pass rate ( table 3 )  . biopsy site and method inuence successful cgp completion biopsy sites . 
the other category encompassed an array of sites , including , but not limited to , brain , eye , epicardium , aorta , lymph node , submandibular gland , bladder , prostate , testes , ovary , cervix , and vagina . 
this was partially due to nding duplicate patients ( ie , some data were obtained with patients identities removed , because they were included in the decision impact trial , which was blinded ; in unblinding , we found some individuals had been included twice )  . 
other reasons included being unable to locate individuals within ihis ( ohio state universitys electronic medical record ) and data necessary for additional analysis ( including biopsy location and method ) were unavailable . 
breakdown of the most common sarcomas subtypes proled sarcoma subtype qualied passed failed total bone - based chondrosarcoma osteosarcoma ewing chordoma soft tissue based leiomyosarcoma liposarcoma spindle cell liposarcoma myxoid liposarcoma pleomorphic liposarcoma well - differentiated liposarcoma dedifferentiated liposarcoma gist synovial myxobrosarcoma angiosarcoma fibromatosis dscrt epithelioid epithelioid hemangioendothelioma solitary brous tumor abbreviations : dscrt , desmoplastic small round cell tumor ; gist , gi stromal tumor . 180 2020 by american society of clinical oncology in conclusion , to our knowledge , this study is the only prospective evaluation of dnaand rna - based cgp in sarcoma on physician decision - making and the largest indepth evaluation of success of cgp in sarcoma to date . 
we note in this cohort that cgp in sarcoma is successful in a large majority of patients and alters physician treatment decision - making in an estimated 25% of patients . 
furthermore , this percentage may have been driven by the fact that the study data were from the era when cdk4 inhibitors were just starting to be considered for use off - label in adipocytic tumors , and conrmation of cdk4 amplication was critical for this drug selection . 
we would anticipate , as time progresses , the types of tumor for which there are dened targetable alterations will increase and thus there would be an increase in physician treatment - decision changes . 
a classic example would be that of gi tumors for which kit / pdgfr sequencing is now considered standard of care for determining whether a patient has these alterations and , if so , whether the patient has resistance alterations.17 a developing example would be that in leiomyosarcoma , where we have previously reported that homologous recombination alterations are a common feature of uterine leiomyosarcomas and may be amenable to parp inhibition.18 tumor location and tissue subtype signicantly clearly , inuence proling success , likely secondary to preanalytic variables that inuence quality of dna and rna , such as decalcication , tumor cellularity , and available tissue volume . 
of note , of the 36 bone biopsy samples that were collected in this study , pathology reports for only 13 mentioned the sample underwent decalcication ; however , no specications regarding the decalcication agent used or the xation times were documented in the report . 
protocols to prevent decalcication during sample processing may aid in yielding higher cgp success rates.19 , 20 in addition , obtaining excisional biopsy specimens rather than imaged - guided biopsy specimens seems to lead to greater likelihood of cgp success . in these studies , it should be mentioned that germline aberrations were not evaluated , because foundation medicine does not test for these . 
 challenges in sarcoma comprehensive genomic proling causes of sample failure causes of sample qualification low cellularity rna failure dna and rna failure dna failure unknown contamination rna failure failed rna metrics low tumor purity noisy cna data contamination rna failure and noisy cna data failed rna metrics and contamination low dna coverage unknown n = 44 samples n = 56 samples fig 3 . 
also , many of our samples are often obtained at outside hospitals , and there is no standardization of pathology report contents . in summary , sarcoma cgp appears to alter physician decision - making regarding treatment and may affect the ultimate outcome of the patient . 
chen consulting or advisory role : novartis , immune design , syapse speakers bureau : novartis , foundation medicine , eisai patents , royalties , other intellectual property : matchtx . no other potential conicts of interest were reported . references groisberg r , hong ds , holla v , et al : clinical genomic proling to identify actionable alterations for investigational therapies in patients with diverse sarcomas . oncotarget 8 : 39254 - 39267 , 2017 abeshouse a , adebamowo c , adebamowo sn , et al : comprehensive and integrated genomic characterization of adult soft 171 : 950 - 965.e28 , 2017 yakirevich e , madison r , fridman e , et al : comprehensive genomic proling of adult renal sarcomas provides insight into disease biology and opportunities for targeted therapies . 
cancer res 76 : 3690 - 3701 , 2016 fang w , ma y , yin jc , et al : comprehensive genomic proling identies novel genetic predictors of response to anti - pd - ( l ) 1 therapies in non - small cell lung cancer . 
clin cancer res 25 : 5015 - 5026 , 2019 chung jh , dewal n , sokol e , et al : prospective comprehensive genomic proling of primary and metastatic prostate tumors . 
jco precis oncol 3 : 1 - 23 , 2019 al - rohil rn , tarasen aj , carlson ja , et al : evaluation of 122 advanced - stage cutaneous squamous cell carcinomas by comprehensive genomic proling opens the door for new routes to targeted therapies . 
ross js , gay lm , wang k , et al : comprehensive genomic proles of metastatic and relapsed salivary gland carcinomas are associated with tumor type and reveal new routes to targeted therapies . 
rodriguez - rodriguez l , hirsheld km , rojas v , et al : use of comprehensive genomic proling to direct point - of - care management of patients with gynecologic 14 . 
thway k , rockcliffe s , gonzalez d , et al : utility of sarcoma - specic fusion gene analysis in parafn - embedded material for routine diagnosis at a specialist 16 . 
thway k , wren d , lee j , et al : evaluation of the optimal provision of formalin - xed , parafn - embedded material for reverse transcription - pcr in soft - tissue 21 : 1315 - 1325 , 2016 cancers . 
singh vm , salunga rc , huang vj , et al : analysis of the effect of various decalcication agents on the quantity and quality of nucleic acid ( dna and rna ) recovered from bone biopsies . 
choi s - e , hong sw , yoon so : proposal of an appropriate decalcication method of bone marrow biopsy specimens in the era of expanding genetic molecular study . 
therefore , less is known about the prevalence and extent of msi among other types of cancer . methods using our recently published msi - calling software , mantis , we analyzed wholeexome data from 11 , 139 tumor - normal pairs from the cancer genome atlas and therapeutically applicable research to generate effective treatments projects and external data sources across 39 cancer types . 
within a subset of these cancer types , we assessed mutation burden , mutational signatures , and somatic variants associated with msi . results we identified msi in 3.8% of all cancers assessedpresent in 27 of tumor typesmost notably adrenocortical carcinoma ( acc ) , cervical cancer ( cesc ) , and mesothelioma , in which msi has not yet been well described . 
in addition , msi - high acc and cesc tumors were observed to have a higher average mutational burden than microsatellite - stable acc and cesc tumors . conclusion we provide evidence of as - yet - unappreciated msi in several types of cancer . 
2017 by american society of clinical oncology introduction large - scale sequencing projects of cancer genomes have opened the door to studies that have identified putative biomarkers with potential clinical and therapeutic value , among them the presence or absence of microsatellite instability ( msi )  . 
microsatellites are defined as 10 to 60 base pair regions that contain multiple repeats of 1 to 5 base pair motifs.1 microsatellites occur at microsatellite loci , which are widely dispersed throughout the human genome . 
in normal cells , repeat count of microsatellites is verified and maintained during cell division by the mismatch repair ( mmr ) system , 2 , 3 one of many cellular dna repair mechanisms . 
after multiple cycles of cell division , cells with an impaired mmr system will develop varying lengths in their microsatellite sequences . mismatch repair deficiency is known to occur in some tumors , 2 either by somatic hypermutation of mmr genes , most commonly , mlh14 , 5 ; an inherited germline mmr pathway mutation , such as in lynch syndrome6 , 7 ; or double somatic mutations in mmr genes . 
 durable responses and a statistically significant improvement in overall survival.12 msi polymerase chain reaction ( pcr ) and immunohistochemistry are two molecular biology based methods that are in routine use for clinical msi testing . 
msi - pcr analyzes the distribution of microsatellite lengths at five standardized loci ( bethesda panel ) , 14 and immunohistochemistry detects the presence or absence of four proteins that are involved in the mmr pathway ( msh2 , msh6 , mlh1 , and pms2 )  . 
examples of such software include msings , 15 msisensor , 16 and mantis.17 a recent study by our group17 demonstrated that mantis achieves high sensitivity ( 97% ) and specificity ( 99% ) across six cancer typestested using samples with known msi status by msipcrand provides stable performance with varying numbers of microsatellite loci . 
because of this , mantis is particularly well suited for application to a wider variety of cancer types . as clinical msi testing is routinely performed only on colorectal and endometrial tumors , 18 the prevalence of msi in many other cancer types has been less well described . 
in addition , evidence exists that msi - pcr may be less accurate in other cancer types.19 a recent study by hause et al20 developed and applied the msi detection tool , mosaic , to perform a detailed survey of msi across 18 cancer types ( n = 5 , 930 cases ) ; however , many other cancer types have yet to be analyzed for msi . 
the ability to detect msi in novel cancer types would permit the investigation of immuneenhancing therapies in these cancers , with the potential to benefit previously unknown subsets of patients with cancer with msi . to perform a more comprehensive assessment of msi across many additional cancer types than those analyzed by hause et al , our study determined the prevalence of msi in 39 distinct cancer types ( n = 11 , 139 tumors from 11 , 080 patients ) by using our previously published msi - calling tool , mantis . methods data preprocessingthe cancer genome atlas and therapeutically applicable research to generate effective treatments for analysis , 10 , 701 cases of paired tumor - normal whole - exome sequencing data were obtained from the cancer genome atlas ( tcga ) 21 - 44 and therapeutically applicable research to generate effective treatments ( target ) 45 , 46 projects . 
data from all of these cases , with the exception of diffuse large b - cell lymphoma ( dlbcl ) were processed via our in - house automated pipeline , l - map ( landscape microsatellite analysis pathway )  . 
l - map is implemented in python and mysql and was run on the oakley supercomputer at the ohio supercomputing center.47 first , the metadata for all dna whole - exome bam files were downloaded from the genomic data commons ( gdc ) 48 and were converted to sql database entries . 
premarked duplicate reads were removed as above . data preprocessingother sources four hundred thirty cases of paired tumor - normal whole - exome sequencing data were obtained from the sequence read archive51 : 338 chronic lymphocytic leukemia cases from 279 patients from landau et al , 52 32 cutaneous t - cell lymphoma cases from choi et al , 53 51 nasopharyngeal carcinoma cases from zheng h et al , 54 and 8 cholangiocarcinoma cases from ong et al.55 fifteen additional cholangiocarcinoma cases were obtained from the european nucleotide archive56 from chan - on et al.57 all sample identifiers used are available in the data supplement . these cases were processed via l - map . 
coordinates for 2 , 539 microsatellite loci within or near the exomeoriginally introduced by salipante et al15 and used by later studies17 were converted from hg19 to hg38 by using liftover.61 nine unlifted loci were discarded , which left 2 , 530 regions that were used for analysis with mantis in all cohorts , with the exception of dlbcl ( data supplement )  . 
mantis was run with authorrecommended settings for whole - exome data minimum read quality , 20 ; minimum locus quality , 25 ; minimum locus coverage , 20 ; minimum repeat reads , one ; all other settings left at defaults . eight samples were observed to have fewer than 10 loci sufficiently covered and were dropped . 
variant annotation was performed by using annovar ( version 201602 - 01 ) 63 and gnu parallel.64 somatic mutations in the repair genes msh2 , msh6 , mlh1 , pms2 , exo1 , pold1 , and pole were determined by filtering variants with a dann68 , 69 pathogenicity score greater than 0.96 ( included in annovar )  . this threshold for dann was chosen as it was previously shown to provide optimal sensitivity and specificity.69 mutational signature calling was performed by using the tool deconstructsigs70 with the nature 2013 signatures set , which contains 27 signatures , 71 and the exome2genome normalization method . 
of 2 , 530 loci , we identified 22 loci that , within at least five cohorts , had an msi - h versus mss difference score greater than 0.75 and were sufficiently covered by at least 50% of samples in the cohort ( appendix table a2 )  . 
note that for chronic lymphocytic leukemia ( cll ) , the listed msi prevalence in panel a is out of 279 patients , and all 338 tumors are shown in panel b . 
acc , adrenocortical carcinoma ; aml , pediatric acute myeloid leukemia ( target ) ; blca , bladder carcinoma ; brca , breast carcinoma ; cesc , cervical squamous cell carcinoma and endocervical adenocarcinoma ; chol , cholangiocarcinoma ; coad , colon adenocarcinoma ; ctcl , cutaneous t - cell lymphoma ; dlbc , diffuse large b - cell lymphoma ; esca , esophageal carcinoma ; gbm , glioblastoma multiforme ; hnsc , head and neck squamous cell carcinoma ; kich , kidney chromophobe ; kirc , kidney renal clear cell carcinoma ; kirp , kidney renal papillary cell carcinoma ; laml , acute myeloid leukemia ( tcga ) ; lgg , lower - grade glioma ; lihc , liver hepatocellular carcinoma ; luad , lung adenocarcinoma ; lusc , lung squamous cell carcinoma ; meso , mesothelioma ; nbl , pediatric neuroblastoma ; npc , nasopharyngeal carcinoma ; ov , ovarian serous cystadenocarcinoma ; paad , pancreatic adenocarcinoma ; pcpg , pheochromocytoma and paraganglioma ; prad , prostate adenocarcinoma ; read , rectal adenocarcinoma ; sarc , sarcoma ; skcm , skin cutaneous melanoma ; stad , stomach adenocarcinoma ; tcgt , testicular germ cell tumor ; thca , thyroid carcinoma ; thym , thymoma ; ucec , uterine corpus endometrial carcinoma ; ucs , uterine carcinosarcoma ; uvm , uveal melanoma ; wt , wilms tumor . were within the set of 22 top - performing loci . these results indicate a striking heterogeneity of msi patterns across various types of cancer . all four disease types with the highest rates of msi prevalence were lynch syndromeassociated tumor types that have been previously known to exhibit msi : endometrial carcinoma , colon adenocarcinoma , gastric adenocarcinoma , and rectal adenocarcinoma . 
somatic variant calling was performed on whole - exome samples from these four cancer types , and the mean absolute number of somatic mutationsboth nonsynonymous and synonymouswas found to be increased among msi - h versus mss tumors within their own cohorts ( fig 3 )  . 
p values were calculated by using two - sided fishers exact test ( using signature presence or absence ) , with benjamini correction for multiple hypotheses.78 mmr pathway alterations msi - h lynch syndromeassociated tumors are known to lack the expression or function of at least one mmr protein ; therefore , we analyzed somatic mutations that were predicted to be deleterious ( by dann68 ) in the mmr genes msh2 , msh6 , mlh1 , pms2 , and exo1 , and the proofreading dna polymerases pold1 and pole , among msi - h and mss samples within acc , cesc , and meso ( appendix table a3 ; data supplement )  . 
although pold and pole are not considered mmr proteins , mutations in these genes have been shown to lead to somatic hypermutation.22 , 79 within these cohorts , 64% of msi - h cases and 7% of mss cases were found to contain at least one predicted deleterious somatic mutation in at least one of these genes ; however , given that these samples were sequenced with potentially different exome captures , together with the increased mutational burden of msi - h tumors , we could not determine the statistical significance of this finding . discussion in this study , we have performed , to our knowledge , the largest analysis of msi in human cancer exomes to date , including 11 , 139 whole - exome tumor - normal pairs from 39 types of cancer . compared with a study by hause et al , 20 we mantis score mantis score mantis score ascopubs.org / journal / po jco precision oncology 5 fig 2 . 
kernel density plots of mantis scores within ( a ) adrenocortical carcinoma ( acc ) , ( b ) cervical squamous cell carcinoma and endocervical adenocarcinoma ( cesc ) , and ( c ) mesothelioma ( meso )  . 
somatic mutational burden correlates with microsatellite instability high ( msi - h ) status within adrenocortical carcinoma ( acc ) and cervical squamous cell carcinoma and endocervical adenocarcinoma ( cesc )  . mutational burden is listed for ( a ) acc , ( b ) cesc , and ( c ) mesothelioma ( meso )  . 
previous studies of msi in acc have implicated lynch syndrome as a risk factor for familial acc80 , 81 ; however , to our knowledge , ngs - based msi analysis has not yet been applied to acc . msi - h colorectal tumors have been previously shown to be exceptionally sensitive to therapy with pd - 1 immune checkpoint inhibitors.12 identification of msi in novel tumor types may lead to an expanded role for immunotherapy and a broader scope of clinical msi testing.82 in addition , msi is known to be prognostic within colorectal cancer , 83 which may apply in other cancer types as well . 
clinical trials of immune checkpoint inhibitors are beginning or are underway in acc ( clinicaltrials.gov identifier : nct02673333 ) , cesc ( clinicaltrials.gov identifier : nct02635360 ) , and meso ( clinicaltrials.gov identifiers : nct02784171 , nct02991482 , nct02707666 , and nct02399371 ) , and a previous study of dendritic cell immunotherapy in acc84 demonstrated tumor marker but not clinical response . these studies may benefit from the retrospective evaluation of msi - h as a biomarker . 
prospective expansion of clinical msi testing to other cancer types may enlighten the prognostic and predictive value of msi - h for noncolorectal cancers . mmr deficiency is well recognized as the predominant cause of msi within colorectal , endometrial , and gastric cancers . 
if future studies indicate that msi in acc , cesc , and / or meso is indeed a result of mmr deficiency , the findings of this study may implicate previously unappreciated cancer types as being part of lynch syndrome . 
compared with germline alterations in mmr genes , somatic events are most often a result of hypermethylation of cpg islands in the promoter region of mlh1.4 additional investigation is needed to elucidate other molecular mechanisms that can lead to msi , as well as the downstream effects of msi on tumor - specific biology . 
in addition , of 9 , 569 tumors assessed in this study not within colorectal , endometrial , or gastric cancer , 77 ( 0.8% ) were msi - h . 
only 14 of these were within acc , cesc , or meso , which compromised the statistical power of our mutational signature analysis . a larger cohort of msi - h tumors would permit more comprehensive studies , including correlation with clinical data . in summary , we have detected msi in multiple cancer types , including acc , cesc , and meso , which indicates that msi may affect nonlynch syndrome tumor types . 
kautto no relationship to disclose affiliations all authors : the ohio state university , columbus , oh . support sameek roychowdhury stock and other ownership interests : johnson & johnson ( i ) research funding : takeda , ignyta acknowledgment we thank current and past members of the roychowdhury laboratory for their helpful insight and discussion . 
the chronic lymphocytic leukemia sequencing data ( dbgap : phs000922.v1.p1 ) used in this work was supported by national human genome research institute large - scale sequencing program grant no . 
kane mf , loda m , gaida gm , et al : methylation of the hmlh1 promoter correlates with lack of expression of hmlh1 in sporadic colon tumors and mismatch repair - defective human tumor cell lines . 
study of two large midwestern kindreds . 812 - 816 , 1993 arch intern med 117 : 206 - 212 , 1966 imai k , yamamoto h : carcinogenesis and microsatellite instability : the interrelationship between genetics and epigenetics . 
boland cr , thibodeau sn , hamilton sr , et al : a national cancer institute workshop on microsatellite instability for cancer detection and familial predisposition : development of international criteria for the determination of microsatellite instability in colorectal cancer . 
niu b , ye k , zhang q , et al : msisensor : microsatellite instability detection using paired tumor - normal sequence data . chem 60 : 1192 - 1199 , 2014 bioinformatics 30 : 1015 - 1016 , 2014 17 . 
giardiello fm , allen ji , axilbund je , et al : guidelines on genetic evaluation and management of lynch syndrome : a consensus statement by the us multi - society task force on colorectal cancer . 
faulkner rd , seedhouse ch , das - gupta ep , et al : bat - 25 and bat - 26 , two mononucleotide microsatellites , are not sensitive markers of microsatellite instability in acute myeloid leukaemia . 
cancer genome atlas research network : comprehensive genomic characterization of squamous cell lung cancers . nature 489 : 519 - 525 , 2012 [ erratum : nature 491 : 288 , 2012 ] 24 . 
hoadley ka , yau c , wolf dm , et al : multiplatform analysis of 12 cancer types reveals molecular classification within and across tissues of origcell 158 : 929 - 944 , 2014 33 . 
zheng s , cherniack ad , dewal n , et al : comprehensive pan - genomic characterization of adrenocortical carcinoma . cancer cell 29 : 723 - 736 , 2016 [ erratum : cancer cell 30 : 363 , 2016 ] 42 . 
zheng h , dai w , cheung akl , et al : whole - exome sequencing identifies multiple loss - of - function mutations of nf - kb pathway regulators in nasopharyngeal carcinoma . 
chan - on w , nairismagi m - l , ong ck , et al : exome sequencing identifies distinct mutational patterns in liver flukerelated and non - infection - related bile duct cancers . 
oleary na , wright mw , brister jr , et al : reference sequence ( refseq ) database at ncbi : current status , taxonomic expansion , and functional annotation . 
quang d , chen y , xie x : dann : a deep learning approach for annotating the pathogenicity of genetic variants . bioinformatics 31 : 761 - 763 , 2015 69 . 
bacher jw , flanagan la , smalley rl , et al : development of a fluorescent multiplex assay for detection of msi - high 1113 - 1120 , 2013 tumors . 
gatalica z , vranic s , xiu j , et al : high microsatellite instability ( msi - h ) colorectal carcinoma : a brief review of predictive biomarkers in the era of personalized medicine . 
challis bg , kandasamy n , powlson as , et al : familial adrenocortical carcinoma in association with lynch syndrome . j clin endocrinol metab 101 : 2269 - 2272 , 2016 81 . 
patterns of mutational signatures ( s ) across microsatellite instability cancers : ( a ) adrenocortical carcinoma ( acc ) , ( b ) cervical squamous cell carcinoma and endocervical adenocarcinoma ( cesc ) , and ( c ) mesothelioma ( meso )  . 
listed are the number of samples ( mss or msi - h ) with at least one predicted deleterious mutation in msh2 , msh6 , mlh1 , pms2 , exo1 , pold1 , and pole . mutations were called by using mutect ( variant calling in methods ) and included in this table if the dann pathogenicity score was  . 
idh1 / 2 mutations are associated with a more favorable prognosis among glioblastomas , whereas tumors with mgmt promoter hypermethylation are more likely to respond to treatment with alkylating agents.1 , 2 the pattern of genomic alterations can also provide insight into the origin and evolution of the tumor . 
for example , the presence of coexistent mutations in idh1 and atrx suggest a secondary glioma that has progressed from a lower - grade glioma.3 - 5 in addition to informing prognosis and diagnostic classification , some genomic alterations in glioma represent potential therapeutic targets . 
specifically , recurrent alterations in one of several receptor tyrosine kinases ( rtks ) , including egfr , pdgfra , met , and fgfr1 / 2 / 3 , have been observed in the majority of glioblastomas.6 unfortunately , efforts to develop genomically targeted therapy for the treatment of glioblastoma have been unsuccessful to date.7 it remains unknown the extent to which the lack of activity of targeted therapy may be attributed to so - called key alterations that do not represent true clonal drivers that are critical to tumor growth and progression compared with the simple inability of existing drugs to achieve therapeutic exposures within the cns . in addition to these more common genomic alterations , less common fusions that involve the kinase domain of tropomyosin receptor kinases ( trks ; a / b / c ) encoded by the genes , ntrk1 , ntrk2 , and ntrk3 have also been identified in gliomas.8 - 11 in other cancer types , selective inhibition of these trk fusions has resulted in remarkable efficacy12 ; however , it remains unknown whether this therapeutic strategy is effective in primary brain tumors . 
 disease progression nov 2011 may 2015 nov 2015 feb 2016 sept 2016 july 2016 primary resection resection resection and r temporal lobectomy adjuvant rt temozolomide lomustine + bevacizumab larotrectinib anaplastic astrocytoma grade iii temozolomide + ido inhibitor secondary gbm grade iv recurrent gbm temporal pole grade iii hippocampus grade iv central tumor grade iv mixed response fig 1 . 
three weeks into the treatment , a brain mri indicated a response to treatment , the degree of which was radiologically discrepant between disease sites ( fig 2 )  . 
 whereas there was significant periventricular response to larotrectinibtumor shrinkage of 67 52 mm to 8 4 mm , which corresponded to a partial response by response assessment in neuro - oncology criteria , and of 162 cm3 to 57 cm3 , which represented a 65% volumetric decreasethere was no shrinkage in the right supraorbital area and occipital lobe . 
she died of her disease shortly thereafter . we hypothesized that intratumoral heterogeneity of the fusion oncoprotein was the basis for the marked response to therapy observed in some areas of her tumor but not others . 
of interest , the ntrk fusion was not detected in either lesion , a finding that is consistent with the radiographic effects of larotrectinib and , overall , a subclonal sensitizing fusion . 
to better characterize the full extent of intratumoral heterogeneity , we subsequently performed whole - exome sequencing of her original tumor from the right temporal lobe and the three resected areas of her recurrence . 
only the hippocampal and central tumors contained a focal cdkn2a / b deletion and a mutational repertoire indicative of temozolomide - induced hypermutation ( figs 3b and 3c and data supplement )  . 
 moreover , the hippocampal and central tumors had distinct rtk alterations , including a pdgfra amplification in the hippocampal specimen and the eml4 - ntrk3 fusion in the central tumor . 
serial contrast t1 - weighted images at pretreatment ( left column ) show enhancing disease in the infundibulum ( green arrow #1 ) , basal ganglia ( green arrow #2 ) , frontal lobe ( green arrow #3 ) , subependyma , and corpus callosum ( green arrow #4 ) , which is improved by day 18 of treatment with larotrectinib ( middle column )  . 
at day 40 ( right column ) , there is worsening enhancing disease in the inferior frontal lobe ( red arrow #1 ) , occipital lobe ( red arrow #2 ) , leptomeninges ( red arrow #3 ) , and parietal lobe ( red arrow #4 )  . tumor , which suggests that multiple clonally related tumors underwent independent waves of therapy - associated mutagenesis . 
thus , our genomic characterization of the patients tumor confirmed profound intratumoral heterogeneity , including subclonality of the ntrk fusion . discussion gene fusions that involve the trk family of kinases have been identified in a wide array of adult and pediatric cancers in which they result in constitutive kinase activation and drive tumor growth.8 , 15 - 20 larotrectinib is a novel small - molecule inhibitor that specifically targets trk and has demonstrated unprecedented efficacy in trk fusionpositive cancers irrespective of tumor histology , with the majority of patients achieving rapid and durable clinical responses12 , 21 ; however , the efficacy of trk inhibition in gliomas is currently unknown . 
 ( b ) pattern of hallmark truncal mutations in idh1 , tp53 , and atrx across the initial tumor ( a ) and recurrent specimens ( b - d ) as well as private driver events in postprogression samples ( c and d , as indicated )  . 
 ( c ) overall somatic mutational burden ( top ) of all tumor samples is shown , which indicates hypermutation in lesions c and d , but not in the initial pretreatment tumor or post - tmz temporal pole tumor ( b )  . 
snv , single nucleotide variant . to therapeutic resistance and disease recurrence.22 , 23 this case highlights that molecular profiling of a single area may not capture the full genomic landscape of a tumor . 
kinase fusions , including trk fusions , are typically clonal when present in other diseases and thus represent some of the most vulnerable targets of novel therapeutics.8 the presence of the trk fusion in only one subclone suggests that distinct cell populations in this tumor relied on different driver alterations ; therefore , genomic heterogeneity limits , but does not preclude , clinical benefit from a targeted agent . 
another aspect of the profound intratumoral heterogeneity observed here was somatic hypermutation , a well - recognized consequence of temozolomide therapy that occurs in a subset of treated patients.24 when present , this may increase the risk of malignant progression via the introduction of novel driver mutations that activate pathways that are quiescent at diagnosis , but as evident here , does not preclude sensitivity to molecularly targeted therapy.25 the observation that hypermutation does not occur in all patients whose tumors are exposed to this therapy suggests that certain cancers are more vulnerable to the mutagenic effect of alkylating agents . 
our report demonstrates that susceptibility can differ even within a single tumor , resulting in hypermutation of some , but not all , subclones ; however , precisely what molecular context underlies these differences is not yet known . 
an improved understanding of what permits this phenotypic change and whether a biomarker of susceptibility to therapy induced hypermutation exists may ultimately lead to more informed treatment decisions for patients with glioma . in conclusion , these data suggest that trk fusions may represent potential therapeutic targets in glioblastoma , a disease with few effective therapies , and that larotrectinib has the potential for antitumor activity in cns tumors that harbor these fusions . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . alexander drilon consulting or advisory role : ignyta , loxo oncology consulting or advisory role : tp therapeutics , astrazeneca , pfizer , blueprint medicines , genentech , takeda pharmaceuticals , helsinn therapeutics , beigene thomas j . 
young stock and other ownership interests : agios , alexion pharmaceuticals , biogen , celgene , gilead sciences , karyopharm therapeutics , spark therapeutics , regeneron , stemline therapeutics , vertex consulting or advisory role : agios , puma biotechnology research funding : agios ( inst ) christian grommes consulting or advisory role : btg nora ku employment : loxo oncology stock and other ownership interests : loxo oncology , novartis ( i ) , biotheranostics ( i ) , pfizer ( i ) , amgen ( i ) , genentech ( i ) , astrazeneca ( i ) , macrogenics ( i ) , peregrine pharmaceuticals ( i ) , pierian bioscience ( i ) , cascadian therapeutics ( i ) travel , accommodations , expenses : novartis ( i ) , biotheranostics ( i ) , pfizer ( i ) , amgen ( i ) , genentech ( i ) , astrazeneca ( i ) , macrogenics ( i ) , peregrine pharmaceuticals ( i ) , pierian bioscience ( i ) david m . 
hyman consulting or advisory role : atara biotherapeutics , chugai pharma , cytomx therapeutics , boehringer ingelheim , astrazeneca , pfizer , bayer , debiopharm group , arqule , genentech research funding : astrazeneca , puma biotechnology , loxo oncology barry s . 
hyman , weill cornell medical college , new york , ny ; and nora ku , loxo oncology , stamford , ct . funded by the sontag foundation , american cancer society grant no . 
van den bent mj , baumert b , erridge sc , et al : interim results from the catnon trial ( eortc study 26053 - 22054 ) of treatment with concurrent and adjuvant temozolomide for 1p / 19q non - co - deleted anaplastic glioma : a phase 3 , randomised , open - label intergroup study . 
russell jp , powell dj , cunnane m , et al : the trk - t1 fusion protein induces neoplastic transformation of thyroid epitheliuoncogene 19 : 5729 - 5735 , 2000 16 . 
one year later , she presented with a recurrent ipsilateral breast mass and underwent a second lumpectomy , and her diagnosis was revised to secretory breast carcinoma on the basis of repeat histopathology evaluation . 
approximately 1 year later , her disease recurred locally , and she underwent a simple mastectomy with axillary lymph node dissection , followed by four cycles of carboplatin and docetaxel . 
less than a year later , she presented with a recurrent fungating mass in the left chest wall and was treated with two cycles of carboplatin and paclitaxel , with no clinical benefit . having exhausted all available options , her treating oncologist presented her case at a virtual multidisciplinary tumor board organized by the global cancer institute , a nonprofit organization focused on improving care of underserved patients with cancer . 
given the histologic diagnosis of secretory breast carcinoma , the board recommended molecular testing for an etv6 - ntrk3 fusion , the pathognomonic genomic alteration in this cancer type.1 to accomplish this , a formalin - fixed tumor block was paraffin - embedded ( ffpe ) located and analyzed at memorial sloan kettering cancer center ( mskcc ) , where the presence of an in - frame etv6 - ntrk3 fusion was confirmed by anchored multiplex rna sequencing ( figs 1a and 1b ) and separately by targeted hybridization capture - based dna and ultimately whole - genome sequencing ( wgs )  . 
immunohistochemistry with a pantropomyosin receptor kinase ( trk ) antibody confirmed overexpression in a perinuclear nuclear pattern , consistent with a fusion involving the nuclear transcription factor etv6 ( fig 1c )  . 
of note , both targeted capture - based sequencing and wgs also identified a tert promoter mutation , a common alteration in solid tumors that leads to increased expression of telomerase2 but to our knowledge has never been reported previously in secretory breast carcinoma . after confirmation of an expressed etv6 - ntrk3 fusion , which is known to result in constitutive trkc kinase activity , 1 treatment with a trk inhibitor was recommended by mskcc pediatric and medical oncology teams . 
ultimately , with approval from the us food and drug administration ( fda ) and loxo oncology ( stamford , ct ) , a single patient use protocol for larotrectinib ( loxo - 101 ) was written and opened for this patient at mskcc . methods anchored multiplex rna sequencing the tumor was analyzed using the msk - solid fusion assay , a targeted rna - based panel that uses the archer anchored multiplex polymerase chain reaction technology3 and next - generation sequencing to detect gene fusions . 
exons 1 to 5 of etv6 are fused to exons 15 to 18 of ntrk3 , which include the kinase domain . ( b ) representation of cdna sequencing reads supporting the etv6ntrk3 fusion transcript . red and blue rectangles represent bidirectional sequencing chimeric reads , where the exact location of the fusion breakpoint is indicated with a dotted vertical line and with an i symbol in the fusion transcript sequence . 
the median depth of coverage across all exons was 9723 . copy number and cellularity information for caveman were predicted with the battenberg algorithm6 using 1 , 000 genomes7 loci within the next - generation sequencing data . 
small somatic insertions and indels were identified using a modified version of pindel ( cgppindel ) .8 structural rearrangements were detected by an in - house algorithm , brass ( breakpoints via assembly ; brass )  . 
mutational signature analysis of the substitutions was performed using the r package deconstructsigs.9 small insertion / deletions were interrogated for the presence of either short tandem repeat or microhomology at the breakpoints , as described previously.10 data relating to this patient will be deposited in the european genome - phenome archive.11 wgs was performed using illumina x10 paired end sequencing standard methods under the auspices of the cancer alliance study in collaboration with the new york genome center . 
single - base substitutions were called using caveman ( cancer variants through expectation maximization ; github.io / caveman / ) , as described previously.6 trk immunohistochemistry expression of trkc , the protein product of ntrk3 , was detected via immunohistochemistry with antipan - trk abcam monoclonal antibody epr17341 in a 1 : 250 dilution . 
 expression of trk with at least weak ( 1 + ) intensity in a membranous , cytoplasmic , and / or nuclear pattern . larotrectinib treatment the treatment dose of the oral pan - trk inhibitor larotrectinib was 100 mg twice per day . 
significant and rapid reduction in size of the left chest mass was achieved within 1 week of starting therapy , with near - complete resolution after 2 months of therapy ( figs 2 and 3b )  . 
the patient tolerated larotrectinib well , with the only drug - related toxicities being two discrete episodes of dizziness ( grade 1 and 2 ) associated with postural change . she was provided with a 6 - month supply of larotrectinib and has since returned home for continued treatment by her oncologists in gopalganj , bangladesh , with plans to return to mskcc twice a year for follow - up . to further investigate the genomic landscape of this patients secretory breast carcinoma , a fresh pretreatment tumor biopsy was obtained and paired tumor - normal wgs performed . 
a total of 697 somatic alterations consisting of 530 singlenucleotide substitutions , 157 deletions ( indels ) , and 10 rearrangements were identified , although only two of these resulted in alteration of a coding region , and of these , only the etv6 - ntrk3 fusion was clonal . 
in addition , wgs also identified two reciprocal inversion events leading to a 9 , 500 - bp deletion containing the first exon of cdkn2a , followed later in this tumors evolution by a subclonal copy - neutral loss of heterozygosity as a result of loss of the wild - type allele and duplication of the mutated allele ( fig 4 )  . 
although the allele with focal deletion of cdkn2a seemed to be clonal , loss of the other allele was not . therefore , biallelic inactivation of cdkn2a was a subclonal event in this tumor . 
we will discuss this option with the family on their follow - up visit to mskcc . discussion ntrk1 , ntrk2 , and ntrk3 encode for the trka , trkb , and trkc receptor tyrosine kinases . oncogenic gene fusions involving the ntrk family of genes have been identified across numerous different tumor types and seem to result in constitutive activation of trk kinase activity.14 larotrectinib is an orally administered highly selective inhibitor , with nanomolar activity against all three trk protein isoforms.15 substantial tumor regressions with larotrectinib have been reported in a child with congenital fibrosarcoma bearing the etv6 - ntrk3 fusion , as well as an adult with a soft tissue sarcoma harboring an lmna - ntrk1 fusion.16 , 17 preliminary activity has also been described in multiple other ntrk fusionpositive cancer types with larotrectinib.18 in july 2016 , the fda granted breakthrough designation to larotrectinib for the treatment of unresectable or metastatic solid tumors bearing ntrk fusions.19 although targeted therapy of its extramammary counterpart has been reported , 20 this is the first report of a patient with secretory carcinoma of the breast treated with a trk inhibitor . 
secretory breast carcinoma is an extremely rare tumor type , accounting for , 0.02% of breast cancer cases.21 it is classically an indolent tumor , with primary management usually consisting of surgical resection . 
although initially believed to occur primarily in children , these tumors have subsequently been identified in both pediatric and adult - age patients.22 histologically , secretory breast carcinomas are characterized by their low - grade appearance , granular or vacuolated cytoplasm , and abundant intracellular and extracellular secretory material.19 furthermore , these tumors are generally triple negative for expression of estrogen receptor , progesterone receptor , and human epidermal growth factor receptor 2.22 although axillary involvement is seen in a significant proportion of patients , widely metastatic disease is uncommon.21 as a result , the role of radiation and chemotherapy is not established for patients with locally advanced or metastatic disease . secretory breast carcinomas are characterized by the etv6 - ntrk3 fusion . 
rearrangements are plotted as arcs inside the robust clinical response to a single - agent trk inhibitor , support previous data demonstrating etv6 - ntrk3 as a driver lesion.23 the 14 - yearold reported here , despite being heavily pretreated for 6 years and having a high burden of disease , achieved an almost immediate and complete response to larotrectinib that remains ongoing with minimal toxicity . 
1 year in duration , with the longest response approaching 2 years.24 whole - genome sequencing analysis reveals a simple mutation and clonal structure , predominantly defined by the fusion gene , mutation in the tert locus , and loss of cdkn2a . 
 ( e ) distribution of corrected variant allele frequency ( vaf ) identifying the etv6 - ntrk3 fusion and tert promoter mutation as clonal events . fusion as the primary mitogenic driver in this patients tumor from the initial presentation onward . along with being the first detailed genomic evaluation of secretory breast carcinoma to our knowledge , and establishing the extraordinary response of this subtype of breast cancer to larotrectinib , this report also describes a unique and dynamic collaboration between multiple international academic centers , global health initiatives , and the pharmaceutical industry . 
the global cancer institute began organizing virtual multidisciplinary tumor boards connecting oncology experts based in the united states and western europe with physicians from lowand middleincome countries in 2012 , with the goal of improving care of patients with cancer in underserved populations worldwide.28 although these tumor boards have typically focused on improving standard practice in the developing world , here we demonstrate how these boards can also lead to the implementation of investigational therapy with dramatic benefit . 
darnell no relationship to disclose elli papaemmanuil employment : tesaro ( i ) stock and other ownership interests : tesaro ( i ) honoraria : novartis , celgene speakers bureau : tesaro ( i ) research funding : celgene patents , royalties , other intellectual property : my husband receives royalties for azd5363 or azd5393 ( not sure ) , an akt inhibitor through the institute of cancer research in the united kingdom ( i ) travel , accommodations , expenses : celgene , novartis , tesaro ( i ) marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / boehringer ingelheim afatinib targeted therapy advisory committee , national comprehensive cancer network / astrazeneca tagrisso request for proposals advisory committee research funding : loxo oncology ( inst ) nora ku employment : loxo oncology stock and other ownership interests : loxo oncology honoraria : novartis ( i ) , biotheranostics ( i ) , pfizer ( i ) , amgen ( i ) , genentech ( i ) , astrazeneca ( i ) , macrogenics ( i ) , peregrine pharmaceuticals ( i ) , pierian biosciences ( i ) consulting or advisory role : baylor college of medicine ( i ) travel , accommodations , expenses : novartis ( i ) , biotheranostics ( i ) , pfizer ( i ) , amgen ( i ) , genentech ( i ) , astrazeneca ( i ) , macrogenics ( i ) , peregrine pharmaceuticals ( i ) , pierian biosciences ( i ) andrew l . 
kung consulting or advisory role : darwin health , mi bioresearch , imago biosciences patents , royalties , other intellectual property : royalty from licensing agreements with mi bioresearch jos e baselga leadership : infinity pharmaceuticals , varian medical systems , grail , foghorn stock or other ownership : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , varian medical systems , tango , foghorn , aura biomedical , apogen , northern biologics honoraria : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , northern biologics consulting or advisory role : eli lilly , novartis , grail patents , royalties , other intellectual property : combination therapy using pdk1 and pi3k inhibitors . 
may 16 travel , accommodations , expenses : roche / genentech alexander drilon honoraria : ignyta , exelixis , genentech , astrazeneca , blueprint medicines , loxo oncology consulting or advisory role : ariad pharmaceuticals research funding : foundation medicine david m . 
hyman consulting or advisory role : atara biotherapeutics , chugai pharma , cytomx therapeutics , boehringer ingelheim , astrazeneca research funding : astrazeneca , puma biotechnology , loxo oncology acknowledgment we thank muhammed yunus for his significant assistance in facilitating the patients travel to the united states for treatment . 
darnell , howard hughes medical institute , chevy chase , md ; and nora ku , loxo oncology , south san francisco , ca . affiliations support supported by national institutes of health grants no . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
cell 149 : 994 - 1007 , 2012 [ erratum : cell 162 : 924 , 2015 ] 1000 genomes project consortium , abecasis gr , auton a , et al : an integrated map of genetic variation from 1 , 092 human genomes . 
nik - zainal s , davies h , staaf j , et al : landscape of somatic mutations in 560 breast cancer whole - genome sequences . nature 534 : 47 - 54 , 2016 11 . 
nagasubramanian r , wei j , gordon p , et al : infantile fibrosarcoma with ntrk3 - etv6 fusion successfully treated with the tropomyosin - related kinase inhibitor loxo - 101 . 
doebele rc , davis le , vaishnavi a , et al : an oncogenic ntrk fusion in a patient with soft - tissue sarcoma with response to the tropomyosin - related kinase inhibitor loxo - 101 . 
drilon a , li g , dogan s , et al : what hides behind the masc : clinical response and acquired resistance to entrectinib after etv6 - ntrk3 identification in a mammary analogue secretory carcinoma ( masc )  . 
li d , xiao x , yang w , et al : secretory breast carcinoma : a clinicopathological and immunophenotypic study of 15 cases with a review of the literature . 
hong ds , dowlati a , burris iha , et al : 150o clinical safety and activity from a phase 1 study of loxo - 101 , a selective trka / b / c inhibitor , in solid - tumor patients with ntrk gene fusions . 
shern jf , chen l , chmielecki j , et al : comprehensive genomic analysis of rhabdomyosarcoma reveals a landscape of alterations affecting a common genetic axis in fusion - positive and fusion - negative tumors . 
shukla n , ameur n , yilmaz i , et al : oncogene mutation profiling of pediatric solid tumors reveals significant subsets of embryonal rhabdomyosarcoma and neuroblastoma with mutated genes in growth signaling pathways . 
louis j , bukowski a , mendoza rer , et al : global cancer institute ( gci ) multi - disciplinary tumor boards ( mtbs ) as an educational tool to improve guideline - based cancer clinical practice in lowand middle - income countries ( lmics )  . 
garcia , md3 ; amir momeni - boroujeni , md1 ; qi gao , mls1 ; jeeyeon baik , ba1 ; dory londono , bs1 ; ryma benayed , phd1 ; allison sigler , ma1 ; michael haddadin , md2 ; alexander v . 
goldberg , md , phd2 ; yanming zhang , md1 ; wenbin xiao , md , phd1 ; and caleb ho , md1 introduction ighcytokine receptorlike factor 2 ( crlf2 ) rearrangement is the most common mechanism of overexpression of crlf2 in precursor b - cell acute lymphoblastic leukemia ( b - all ) ; however , p2ry8 - crlf2 rearrangement or alternative alterations leading to crlf2 overexpression have also been observed , which are associated with increased relapse rate and progression.1 although many myeloid neoplasms , particularly acute myeloid leukemia ( aml ) , are associated with various recurrent genetic rearrangements and fusions , 2 alterations leading to crlf2 overexpression are exceedingly rare in aml . 
one patient with myelodysplastic syndrome with excess blasts - 1 ( mds - eb1 ) with crlf2 overexpression via multiple copies of an isodicentric y chromosome , without evidence of crlf2 rearrangement , has been reported.3 to our knowledge , we report the rst patient with aml arising from an mds , with a p2ry8 - crlf2 fusion , which responded to a myeloid regimen in a clinical trial of hypomethylating agent and immune checkpoint blockade combination therapy . 
at mskcc , karyotype analysis of the aml bone marrow aspirate specimen showed a normal male karyotype , and fish analysis was negative for the presence of kmt2a ( mll ) , evi1 , and cbfb translocations , and tp53 deletion . 
a targeted nextgeneration sequencing ( nsg ) panel ( msk - impact heme panel ; mskcc , new york , ny ) was performed on the bone marrow specimen obtained at the time of the aml diagnoses , which showed the alterations including mutations in asxl1 , listed in table 1 , kmt2d , runx1 , sf3b1 , tet2 , phf6 , rad21 , and xbp1 . 
evaluation of this bone marrow sample using an anchored multiplex polymerase chain reaction based , targeted rna sequencing assay for detection of fusions ( archer fusionplex , archerdx , boulder , co ) revealed the presence of a fusion between exon 1 of p2ry8 and exon 1 of crlf2 ( fig 1c )  . 
cell sorting , molecular characterization , and immunostaining characterized the myeloid origin of this fusion and subsequent signaling effects . relevance this patient was treated with the novel combination of decitabine and ipilimumab with an outstanding response . 
immune cell inltrates in the bone marrow with treatment suggests the response was related to the immune checkpoint inhibition . additional study of p2ry8 - crlf2 fusions and response to immunotherapy is warranted and could have implications for fusion discovery in novel disease contexts . sorting to isolate the leukemic blasts , myelomonocytic cells , lymphocytes . 
fish using the crlf2 breakand normal apart probe revealed the crlf2 rearrangement in a subset of the myeloid blasts ( 27.5% ) and myelomonocytic cells ( 19.5% ) but not in b cells ( fig 2 )  . fish evaluation of the prior bone marrow biopsy with mdseb1 was also performed , which showed the presence of the p2ry8 - crlf2 rearrangement in 10% of the cells ( appendix fig a1c )  . 
oncoscan array ( thermofisher , waltham , ma ) of the mds - eb1 biopsy did not reveal any unbalanced genomic changes or copy - neutral loss of heterozygosity ( data not shown ) , consistent with the normal fish study observed by the outside institution a year prior . 
targeted ngs sequencing ( msk - impact heme panel ) of the mds - eb1 bone marrow specimen also showed overlapping mutations with the aml bone marrow sample ( table 1 ) , but with acquisition of new mutations ( phf6 , rad21 , xbp1 ) in the aml sample , suggesting a myeloid primed hematopoietic stem cell / progenitor origin and clonal evolution with expansion of the clone with the p2ry8 - crlf2 rearrangement , likely due to acquisition of a loss - of - function mutation in phf6 , which led to downregulation of genes involved in normal b - cell development.4 total rna sequencing of the aml bone marrow specimen further conrmed the presence of the p2ry8 - crlf2 fusion along with overexpression of crlf2 ( fig 3a )  . 
principal component analysis comparing our patient with cohorts of aml or b - all from the target study5 showed that the patients neoplasm clustered with other patients with aml , conrming the myeloid differentiation of the blasts ( fig 3b )  . gene ontology analysis showed transcriptome - wide increases in cytokine - related signaling pathway genes potentially related to the p2ry8 - crlf2 fusion , as well as genes involved in regulating hematopoietic progenitor cell differentiation and the spliceosome ( fig 3c )  . because it is known that stat5 is activated by p2ry8crlf2 fusion in b - all , we performed immunohistochemistry ( ihc ) using phosphorylation - specic antibodies that showed increased stat5 phosphorylation and partial erk phosphorylation but not stat3 phosphorylation ( fig 4a )  . 
gene expression and ihc were largely correlated ; however , the results are interpreted in the context of the importance of signaling in leukemia overall , and these are not necessarily specic for p2ry8 - crlf2 fusion . cell sorting myeloid blasts monocytes 27.5% ( 55 / 200 ) 19.5% ( 22 / 113 ) bone marrow aspirate fluorescence in - situ hybridization 0% ( 0 / 174 ) b lymphocytes crlf2 fusion positive fig 2 . 
 ( b ) principal component analysis plot showing 2 strongest principal components ( pc1 on x - axis and pc2 on y - axis ) from publicly available data from aml ( green dots ) and b - all ( red dots ) patient samples compared with our patient with p2ry8 - crlf2 fusion ( blue dot )  . 
he was consented and enrolled in a study regimen consisting of standard - dose decitabine plus investigational administration of the cytotoxic t - lymphocyte associated protein - 4 ( ctla - 4 ) antagonist , ipilimumab ( clinicaltrials.gov identier : nct02890329 )  . 
after 2 cycles of combination therapy , he achieved complete remission with incomplete count recovery and shortly thereafter a full complete remission ( table 2 ) with negative measurable residual disease ( mrd ) status by a ow cytometric assay with a detection limit of 1 in 2 , 500 cells . 
this was accompanied by a robust molecular response with undetectable levels of the previously detected phf6 , runx1 , tet2 , and rad21 mutations , and a marked reduction in the variant allele frequencies for the mutations asxl1 ( 0.4% ) and sf3b1 ( 1.4% ) , likely representing mrd below the detection limit of ow cytometry . 
ihc was performed on the checkpoint molecules including programmed death ( pd ) - 1 , pd - ligand 1 ( pd - l1 ) and pd - l2 ( fig 4b )  . 
 ( c ) using multiplex immunouorescence microscopy , with digital image analysis , we found that the patients bone marrow was highly enriched with cd8 plus granzyme b ( gzmb ) plus t cells . 
we further identied a population of cd3 + cd4 + t cells at baseline . discussion crlf2 is the protein product of a synonymous gene located in the par1 on the short arm of the x chromosome and the y chromosome . 
it forms a heterodimer with interleukin 7 receptor alpha and is involved in lymphoid signaling pathways . activation of this receptor leads to activation of janus family tyrosine kinases and stat5 . 
deregulated expression of this gene has been described as the characteristic alteration in philadelphia chromosomelike b - all in adolescent and adult patients.7 , 8 russell et al9 showed that this subgroup of b - all has either a translocation juxtaposing the crlf2 to the igh gene on chromosome 14 ( t ( x ; 14 ) ( p22 ; q32 ) or t ( y ; 14 ) ( p11 ; q32 ) ) or a deletion of par1 region , resulting in overexpression of the crlf2 gene . 
this has been observed in down syndromerelated all as well as nondown syndrome all , supporting the cooperation of crlf2 events with other genetic alterations in progression of disease.11 however , irrespective of the clone size , presence of this rearrangement is associated with a higher relapse rate.12 there have been suggestions that the increased relapse rate may be due to other concurrent alterations , such as ikzf1 deletion.13 however , other studies have shown the rearrangement as well as the crlf2 overexpression to be independent predictors of worse outcome in b - all.14 , 15 until now , only one patient with myeloid neoplasm with crlf2 overexpression has been reported . 
however , this patient was associated with multiple copies of an isodicentric y chromosome and not associated with p2ry8crlf2 rearrangement.3 to our knowledge , our patient represents the rst p2ry8 - crlf2 rearrangement myeloid neoplasms , which in our patient was an aml arising from the underlying mds . 
the ow - sorted fish the p2ry8 - crlf2 was not analysis has shown that present in the b lymphocytes of this patient but only in the myeloid - lineage cells ( myeloid blasts and myelomonocytic cells )  . 
in addition , based on the results from total rna sequencing , our patients neoplasm clustered with other patients with aml , providing additional evidence for the myeloid differentiation of the blasts . 
furthermore , the alterations observed in this patient , including the p2ry8affiliations 1department of pathology , memorial sloan kettering cancer center , new york , ny 2leukemia service , department of medicine , memorial sloan kettering cancer center , new york , ny 3department of medical oncology , dana - farber cancer institute , boston , 4department of pathology , brigham and womens hospital , boston , ma crlf2 rearrangement , were present at the mds stage , suggesting a stem cell origin with selective pressure leading to development of aml . phf6 mutations are rare in de novo aml but relatively common in aml - mrc and exceedingly rare in b - all.16 , 17 phf6 and dnmt3a are the most common mutations in mixed phenotype acute leukemias ( mpal ) with t - lineage differentiation.18 phf6 is a critical component in lineage determination of precursor cells , especially between t and b lineages , and it is believed that a functioning phf6 is required for b - cell differentiation leading to selective abundance of this mutation in t - all and mpal with t - lineage differentiation.18 , 19 this notion is further supported by the observation that phf6 suppression leads to impaired tumor progression in b - all.4 it has also been shown that pax5 - decient pro - b cells can undergo myeloid - lineage differentiation in the presence of transcription factors , such as gata or cebpa.20 in our patient , the immunophenotype and rna expression data unequivocally point toward myeloid differentiation . 
although it is difcult to ascertain the functional consequences of the p2ry8 - crlf2 rearrangement and the acquired phf6 mutation at the time of aml transformation , we hypothesize that the two may interact in a way that led to the development of aml instead of b - all . remarkably , this patient with aml - mrc and phf6 , runx1 , tet2 , and rad21 mutations had an mrdnegative complete response by ow cytometry after just 4 cycles of combination decitabine with ipilimumab . 
although the complete results from clinical trials of these agents are needed to evaluate the efcacy and safety of this this patients exceptional response could combination , suggest the unique molecular characteristics of his tumor the p2ry8 - crlf2 may have been important , namely , fusion . 
recent evidence in head and neck cancers with oncogenic chromosomal rearrangements suggests that gene fusions may be a source of immunogenic neoantigens and stimulate t - cell responses that could be unleashed after immune checkpoint blockade.21 this patients t cells were positive for pd - 1 , suggesting a relation to the response to ctla - 4 blockade . 
garcia , wenbin xiao , caleb ho administrative support : jeeyeon baik , allison sigler collection and assembly of data : umut aypar , justin taylor , jacqueline s . garcia , amir momeni - boroujeni , qi gao , dory londono , ryma benayed , michael haddadin , alexander v . 
goldberg , yanming zhang , wenbin xiao , caleb ho data analysis and interpretation : umut aypar , justin taylor , jacqueline s . garcia , amir momeni - boroujeni , alexander v . 
garcia consulting or advisory role : abbvie research funding : abbvie ( inst ) , pzer ( inst ) , genentech ( inst ) , eli lilly ( inst ) maria e . 
arcila honoraria : invivoscribe , biocartis references mikhail roshal honoraria : celgene consulting or advisory role : agios , auron research funding : agios , roche , boehringer ingelheim ana lako employment : bristol - myers squibb scott j . 
rodig honoraria : perkin elmer , bristol - myers squibb consulting or advisory role : bristol - myers squibb research funding : bristol - myers squibb , merck , afmed therapeutics , kite pharma patents , royalties , other intellectual property : patent pending for use of antigalectin - 1 antibodies for diagnostic use travel , accommodations , expenses : roche , bristol - myers squibb aaron d . 
goldberg honoraria : dava oncology consulting or advisory role : abbvie , celgene , daiichi sankyo research funding : abbvie ( inst ) , adc therapeutics ( inst ) , pzer ( inst ) , arog ( inst ) travel , accommodations , expenses : arog open payments link : 1195852 / summary wenbin xiao research funding : stemline therapeutics ( inst ) caleb ho honoraria : invivoscribe travel , accommodations , expenses : invivoscribe no other potential conicts of interest were reported . acknowledgment we acknowledge the members of the memorial sloan kettering cancer center diagnostic molecular laboratory , cytogenetics laboratory , ow cytometry laboratory , and immunohistochemical stain laboratory for their support in performing the relevant assays . schm ah j , fedders b , panzer - gr umayer r , et al : molecular characterization of acute lymphoblastic leukemia with high crlf2 gene expression in childhood . pediatr blood cancer 64 : e26539 , 2017 arber da , orazi a , hasserjian r , et al : the 2016 revision to the world health organization classication of myeloid neoplasms and acute leukemia . 
meacham ce , lawton ln , soto - feliciano ym , et al : a genome - scale in vivo loss - of - function screen identies phf6 as a lineage - specic regulator of leukemia cell therapeutic target . 
nature 555 : 371 - 376 , 2018 patel ss , weirather jl , lipschitz m , et al : the microenvironmental niche in classic hodgkin lymphoma is enriched for ctla - 4 - positive t cells that are pd - 1negative . 
curr opin pharmacol 8 : 249 - 254 , 2008 vesely c , frech c , eckert c , et al : genomic and transcriptional landscape of p2ry8 - crlf2 - positive childhood acute lymphoblastic leukemia . 
leukemia 31 : 1491 - 1501 , 2017 russell lj , capasso m , vater i , et al : deregulated expression of cytokine receptor gene , crlf2 , is involved in lymphoid transformation in b - cell precursor acute lymphoblastic leukemia . 
potter n , jones l , blair h , et al : single - cell analysis identies crlf2 rearrangements as both early and late events in down syndrome and non - down syndrome leukemia . 
morak m , attarbaschi a , fischer s , et al : small sizes and indolent evolutionary dynamics challenge the potential role of p2ry8 - crlf2 - harboring clones as main relapse - driving force in childhood all . 
dou h , chen x , huang y , et al : prognostic signicance of p2ry8 - crlf2 and crlf2 overexpression may vary across risk subgroups of childhood b - cell acute lymphoblastic leukemia . 
fang q , zhao x , li q , et al : ikzf1 alterations and expression of crlf2 predict prognosis in adult chinese patients with b - cell precursor acute lymphoblastic leukemia . 
xiao w , bharadwaj m , levine m , et al : phf6 and dnmt3a mutations are enriched in distinct subgroups of mixed phenotype acute leukemia with t - lineage differentiation . 
presence of the p2ry8 - crlf2 fusion in earlier bone marrow biopsy with myelodysplastic syndrome ( mds )  . ( a ) photomicrographs of the bone marrow biopsy showing mds with excess blast - 1 ( mds - eb1 )  . 
 c significant clinical response to a mek inhibitor therapy in a patient with metastatic melanoma harboring an raf1 fusion introduction systemic therapy for metastatic melanoma has changed dramatically since the development of targeted drugs for braf - mutant melanoma and immune checkpoint inhibitors . 
the overall survival duration of those with advanced melanoma has improved significantly with these novel drugs , with the median survival duration now reaching nearly 2 years.1 - 3 the checkpoint inhibitors ( anti cytotoxic t - cell lymphocyte - 4 antibodies and anti - programmed cell death - 1 [ pd - 1 ] antibodies ) produce antitumor response through their ability to activate cytotoxic t - lymphocytes . 
although many of these clinical responses are durable , the median progression - free survival durations are approximately 2 to 3 months and 5 to 6 months with anti - ctla4 antibody and ipilimumab , respectively.4 - 7 a combination of nivolumab and ipilimumab improves the overall response rate and progression - free survival compared with anti - ctla4 antibody alone.7 for patients with metastatic v600 braf - mutant melanoma , combinations of a braf inhibitor and a mek inhibitor have been established as a standard therapy because of a high response rate and superior survival over single - agent braf inhibitors.1 - 3 however , approximately 50% of melanomas do not harbor a v600 braf mutation and therefore do not benefit from braf inhibitor therapy.8 for these patients with wildtype braf , the identification of relevant and actionable genetic alterations and the development of effective matched therapies are urgently needed . 
recently , next - generation sequencing ( ngs ) analyses have revealed a multitude of less frequent and less well - characterized genetic alterations in melanoma , and these findings could lead to the development of effective treatments . 
in october 2014 , he had recurrent melanoma in the right cervical lymph node , and by december 2014 , his disease had progressed in the cervical and intrathoracic lymph nodes and the liver . 
in january 2015 , the patient started treatment with the combination of nivolumab and ipilimumab , but the treatment was discontinued after two doses because of the development of diabetic ketoacidosis . 
from august 2015 to march 2016 , he was treated with single - agent nivolumab and subsequently nivolumab in combination with intralesional talimogene laherparepvec injection to the right cervical nodes , but by march 2016 , the disease had progressed in the right neck nodes and liver . 
 in april 2016 , he underwent a debulking radical right neck lymph node dissection for a palliative purpose . in october 2016 , the patient developed a painful right neck mass , and his performance status worsened ( eastern cooperative oncology group performance status of 2 )  . 
he was found to have rapid disease progression in the right supraclavicular , mediastinal , gastrohepatic , and portocaval lymph nodes ; the liver ; the spleen ; and the t - 12 spine . 
 melanoma specimen from the right neck node was analyzed for genetic alterations using a hybrid - capturebased ngs assay ( foundationone ) .9 the results were wild type for braf , nras , and kit ; however , a number of genetic alterations , including a ano10 - raf1 fusion , flt1 r281q , notch3 splice site 4404 - 1g > a , arid2 q760fs * 7 , pbrm1 loss , spta1 q1720 * , and tert promoter - 146c > t , were detected . 
because of the development of significant skin toxicity , the dose was reduced to 1.5 mg / d after 4 weeks and further down to 1 mg / d in january 2017 . 
the patients pain in the right neck and shoulder improved dramatically with the treatment , his performance status improved , and a computed tomography scan performed at 10 weeks showed significant regression of the metastatic lesions in the right supraclavicular , mediastinal , gastrohepatic , and portocaval lymph nodes ; the liver ; and the spleen ( fig 1 )  . 
treatment with another mek inhibitor was discussed with the patient , but because of rapid clinical deterioration and the concern for significant skin toxicity , he decided on palliative care , and he died in june 2017 . discussion in this article , we describe , to our knowledge , the first case of clinical benefit from an mek inhibitor in a patient with metastatic melanoma harboring an ano10 - raf1 fusion . 
the patients tumor did not harbor a v600 braf mutation , and therefore , selective braf inhibitors or mek inhibitors were not clinically indicated at the time of the treatment . 
without the comprehensive genomic testing capable of detecting gene fusions and rearrangements in addition to mutations and copy number changes , we could have missed the great response witnessed with the mek inhibitor , underscoring the importance of ngs analysis . 
it is not clear whether the tumor progression was caused by true acquired resistance to mek inhibition or by suboptimal dosing of the treatment because of the intolerable cutaneous toxicity . although a single base substitution at codon 600 is the most common genetic alteration in raf genes in melanoma , other raf gene alterations have been observed , with various functional consequences.10 many of the non - v600 braf mutations do not activate the mitogen - activated protein kinase ( mapk ) signaling pathway in as robust a manner as do v600 mutations , and they are largely insensitive to the braf v600 specific inhibitors dabrafenib and vemurafenib.11 genetic mutations in the other raf genes , such as araf and craf ( raf1 ) , are relatively rare.12 abnormal rearrangements of raf1 , including raf1 fusions , occur in approximately 1% of cutaneous melanomas , 13 and their prognostic significance is not known . 
some of these genetic alterations , such as esrp1 - raf1 fusion , were found to activate the mapk pathway and are capable of transforming cells.10 palanisamy et al10 showed that prostate epithelial cells expressing an esrp1 - raf1 fusion were sensitive to a combination of a raf inhibitor ( sorafenib ) and a mek inhibitor ( u0126 ) in vitro . 
although the function of ano10 - raf1 fusion , as found in our case , has not been described , it is likely that this alteration activates the mapk pathway because mek protein inhibition caused significant tumor regression in our case . 
the breakpoint in this case is in raf1 exon 7 and in the fact that the resulting in - frame fusion retains the raf1 kinase domain while removing the n - terminal auto - inhibitory domain ( fig 2 )  . 
this case , together with ours , strongly suggests the clinical relevance of raf gene fusions in melanoma and offers mek inhibitors as a potential therapeutic option for patients with raf fusionpositive tumors . 
for patients with melanoma harboring a braf fusion , there is a phase ii study of trametinib ( the national cancer institute molecular analysis for therapy choice [ nci - match ] trial [ clinicaltrials . gov identifier : nct02465060 ] ) ; however , at this time there is no specific trial for patients with raf1 fusionpositive melanoma . 
in addition to the clinical investigation of mek inhibitors , clinical studies of pan - raf inhibitors , such as sorafenib and regorafenib , should be encouraged on the basis of their preclinical antitumor activity in raf1 fusionassociated cells . furthermore , a mek inhibitorbased combination approach may lead to more durable disease control . 
several groups have demonstrated potential mechanisms of resistance to mek inhibition , including induction of immunoglobulin transcription factor 2 , 15 induction of signal transducer and activator of transcription 3 , 16 and amplification of cyclin - dependent kinase 4 and 6 , 17 among others . 
 furthermore , there is increasing evidence that mek inhibition leads to antigen - specific cd8 + t cells proliferation within the tumor and pro motes the survival of tumor - infiltrating cd8 + t cells.18 these phenomena were corroborated by experiments in which the addition of an mek inhibitor to an anti pd - 1 ( or pro grammed death - ligand 1 [ pd - l1 ] ) antibody resulted in durable and synergistic tumor regression.18 several clinical trials are evaluating the clinical efficacy of an mek inhibitor in combination with the checkpoint inhibitors in patients with melanoma ( clinicaltrials.gov identifiers : nct03149029 , nct03178851 , and nct02910700 )  . in conclusion , the ngs analysis of the melanoma lesion in our patients tumor was essential in identifying the clinically relevant genetic alteration , ano10 - raf1 fusion , and in selecting a mek inhibitor treatment that resulted in brief , but significant , tumor regression and symptom improvement . 
kim honoraria : genentech , glaxosmithkline , novartis , foundation medicine consulting or advisory role : genentech , glaxosmithkline , novartis , foundation medicine speakers ' bureau : bristol - myers squibb , merck , novartis research funding : glaxosmithkline ( inst ) , novartis ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , amgen , immune design ( inst ) travel , accommodations , expenses : genentech , bristol - myers squibb , merck , novartis thomas semrad consulting or advisory role : amgen , genentech , onyx pharmaceuticals , celgene , eisai , genzyme ( i ) research funding : eisai ( inst ) , millennium pharmaceuticals ( inst ) , novartis ( inst ) alexa b . 
ali employment : foundation medicine honoraria : emd merck serono research funding : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome stuff in non - neoplastic disease ( i ) mark singer no relationship to disclose jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine honoraria : pfizer mohammed kashani - sabet stock and other ownership interests : melanoma diagnostics , dnarx honoraria : cepheid consulting or advisory role : castle biosciences research funding : merck patents , royalties , other intellectual property : myriad genetics affiliations kevin b . 
kim , mark singer , and mohammed kashani - sabet , california pacific medical center research institute , san francisco ; thomas semrad , gene upshaw memorial tahoe forest cancer center , truckee , ca ; alexa b . 
long gv , stroyakovskiy d , gogas h , et al : dabrafenib and trametinib versus dabrafenib and placebo for val600 braf - mutant melanoma : a multicentre , double - blind , phase 3 randomised controlled trial . 
weber js , dangelo sp , minor d , et al : nivolumab versus chemotherapy in patients with advanced melanoma who progressed after anti - ctla - 4 treatment ( checkmate 037 ) : a randomised , controlled , open - label , phase 3 trial . 
bid hk , kibler a , phelps da , et al : development , characterization , and reversal of acquired resistance to the mek1 inhibitor selumetinib ( azd6244 ) in an in vivo model of childhood astrocytoma . 
ebert pjr , cheung j , yang y , et al : map kinase inhibition promotes t cell and anti - tumor activity in combination with pd - l1 checkpoint blockade . 
walsh , md1 , 2 ; rosalba sacca , phd1 ; temima wildman , ms1 ; kimberly amoroso , ms1 ; jennifer kennedy , ms1 ; liying zhang , md , phd1 ; ozge birsoy , phd1 ; diana mandelker , md , phd1 ; zoe steinsnyder1 ; alicia latham , md1 , 2 ; maria i . 
stadler , md1 , 2 ; and kenneth oft , md , mph1 , 2 introduction telomere length assessthe original dyskeratosis congenita , telomere syndrome , was clinically described more than 100 years ago on the basis of individuals who presented with a distinct rash , abnormal nails , and whitening of the tongue.1 from this rare syndrome , our clinical and molecular understanding of telomere syndromes has evolved and has now expanded to include aplastic anemia , myelodysplastic syndrome , and pulmonary brosis.2 - 5 the identication of patients with telomere syndromes is of signicant clinical importance because these patients are exquisitely sensitive to alkylating chemotherapeutic agents and ionizing radiation.6 - 8 precision medicine efforts that deploy tumor - normal sequencing have used various molecular assays and platforms to interrogate and annotate the cancer census genes.9 , 10 tert , a gene that encodes a key protein involved in telomere maintenance , has been analyzed predominantly to identify genomic alterations that occur in tumors.11 , 12 although constitutional telomere syndromes are recognized , they are rarely considered in the oncologists differential diagnosis unless a diagnosis of a telomere syndrome occurred before the patients cancer diagnosis.13 from january 2016 to may 2019 , unselected patients with advanced solid tumors were presented with the option to participate and consent to a memorial sloan kettering cancer center institutional review board approved protocol ( #12 - 245 ; clinicaltrials.gov identier : nct01775072 ) of tumor and germline dna sequencing . 
cancer types in our cohort included four female patients with breast cancer ( ages at diagnosis , 28 , 37 , 46 , and 58 years ) , one male patient with gall bladder adenocarcinoma ( age 33 years ) , one male patient with pancreatic ampullary adenocarcinoma ( age 45 years ) , and one male patient with two malignancies : lymphoma at age 58 years and prostate cancer at age 66 years . 
in the six patients with a solid tumor as their rst malignancy , all were younger than the median age of diagnosis in the general population for their type of cancer24 - 27 ( data supplement )  . clinical histories of three ( 42.8% ) of the seven patients were suggestive of telomere syndromes . 
individual i , diagnosed with breast cancer , endured therapy - induced radiation pneumonitis and refractory thrombocytopenia ; individual iv , diagnosed with ampulla of vater cancer , experienced premature graying and thrombocytopenia that preceded a cancer diagnosis at age 19 years ; and individual vii revealed a history of bone marrow failure in a family member with a segregating tert mutation and showed abnormal pulmonary function testing ( table 1 )  . an understanding of the genetic basis that contributes to therapeutic sensitivities is important for oncology patients who receive chemotherapy , radiation , and other biologic therapeutics . 
patients with telomere syndromes may manifest overt or subtle clinical ndings.5 moreover , for patients with both obvious and subtle telomere syndromes , exquisite treatment sensitivities have been reported.6 , 7 although only one in 1 , 571 individuals in this series of patients with advanced cancer showed a germline tert mutation , this could translate to more than 1 , 000 patients diagnosed with malignancies a year in the united states who may have increased therapeutic sensitivities . 
because telomere syndrome disorders are complex and exhibit anticipation , incomplete penetrance , multiple genes that underpin disease , recognized modiers , and both autosomal dominant and autosomal recessive patterns of inheritance , this estimate will be rened with time . however , until a clearer picture is possible , it seems reasonable for individuals with constitutional germline tert mutations to be considered for monitoring given the potential long - term sequalae from chemotherapy and radiation as well as increased organ - specic damage.7 , 8 , 31 for two individuals , telomere length testing through cytometric uorescence in situ hybridization identied telomere lengths in the 1st percentile or less ; in two additional individuals , telomere lengths were in the 10th percentile or telomere length less ; and in one additional testing failed because of low blood counts that did not recover after chemotherapy ( fig 1 )  . 
somatic mutation analysis of all ve individuals with germline tert mutations and tumor specimens available for analysis individual , integration of germline , somatic , and clinical data for patients in our cohort was also notable for somatic tp53 mutations and a younger age at cancer diagnosis compared with the general population . 
moreover , multiple tert single nucleotide polymorphisms have been shown to be associated with telomere length and breast and ovarian cancer risk.31 all this information together with telomere lengths may provide insights for stratifying patients with regard to age at presentation , outcome , and tumor evolution . lymphocytes granulocytes 99th percentile 50th percentile 90th percentile 99th percentile 50th percentile 90th percentile 1st percentile 10th percentile 1st percentile 10th percentile age ( years ) age ( years ) fig 1 . 
 e walsh et al e113rfs * 79 p308hfs * 43 l392vfs * 145 r486c v694m exon 4 deletion f1084 * telomerase rvt1 1 , 000 1 , 132 aa a86vfs * 55 y163 * m237i m273h / c truncating mutations missense mutations rvt1 i , v / vi fig 2 . 
walsh , md , memorial sloan kettering cancer center , 222 70th st , room 412 , new york , ny 10021 ; e - mail : walshm2@ makcc.org. support supported by the robert and kate niehaus center for inherited cancer genomics and members of the molecular diagnostics service in the department of pathology and the marie - jos ee and henry r . 
also receives grant support from the v foundation , corning fund , and crawford fund for pediatric genomics . all authors at memorial sloan kettering are supported by the memorial sloan kettering cancer center support grant / core grant through national cancer institute grant no . 
walsh , kimberly amoroso , liying zhang collection and assembly of data : rosalba sacca , temima wildman , kimberly amoroso , jennifer kennedy , ozge birsoy , zoe steinsnyder , alicia latham , maria i . 
carlo consulting or advisory role : pzer other relationship : prostate cancer foundation , robert wood johnson foundation karen cadoo research funding : astrazeneca ( inst ) , syndax ( inst ) travel , accommodations , expenses : astrazeneca mark robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca references research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca , pzer other relationship : research to practice , clinical care options , physician education resource zsoa k . 
stadler consulting or advisory role : allergan ( i ) , genentech ( i ) , roche ( i ) , regeneron pharmaceuticals ( inst ) , optos ( i ) , adverum ( i ) , biomarin ( i ) , alimera sciences ( i ) , novartis ( i ) , spark therapeutics ( i ) , fortress biotech ( i ) , regenxbio ( i ) no other potential conicts of interest were reported . zinsser f : atrophia cutis reticularis cum pigmentatione , dystrophia unguium et leukoplakia oris . 
n engl j med 361 : 2353 - 2365 , 2009 alder jk , guo n , kembou f , et al : telomere length is a determinant of emphysema susceptibility . 
am j respir crit care med 184 : 904 - 912 , 2011 alder jk , parry em , yegnasubramanian s , et al : telomere phenotypes in females with heterozygous mutations in the dyskeratosis congenita 1 ( dkc1 ) gene . hum mutat 34 : 1481 - 1485 , 2013 armanios m , blackburn eh : the telomere syndromes . 
nat rev genet 13 : 693 - 704 , 2012 [ erratum : nat rev genet 14 : 235 , 2013 ] agrusa je , bertuch aa , dinardo cd , et al : severe therapy - related toxicities after treatment for hodgkin lymphoma due to a pathogenic tert variant and shortened telomeres . 
pediatr blood cancer 66 : e27779 , 2019 de la fuente j , dokal i : dyskeratosis congenita : advances in the understanding of the telomerase defect and the role of stem cell transplantation . 
pediatr transplant 11 : 584 - 594 , 2007 dietz ac , orchard pj , baker ks , et al : disease - specic hematopoietic cell transplantation : nonmyeloablative conditioning regimen for dyskeratosis congenita . bone marrow transplant 46 : 98 - 104 , 2011 cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
rusch m , nakitandwe j , shurtleff s , et al : clinical cancer genomic proling by three - platform sequencing of whole genome , whole exome and transcriptome . nat commun 9 : 3962 , 2018 11 . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
hampel h , bennett rl , buchanan a , et al : a practice guideline from the american college of medical genetics and genomics and the national society of genetic counselors : referral indications for cancer predisposition assessment . 
weitzel jn , blazer kr , macdonald dj , et al : genetics , genomics , and cancer risk assessment : state of the art and future directions in the era of personalized medicine . 
noone am , cronin ka , altekruse sf , et al : cancer incidence and survival trends by subtype using data from the surveillance epidemiology and end results program , 1992 - 2013 . 
bojesen se , pooley ka , johnatty se , et al : multiple independent variants at the tert locus are associated with telomere length and risks of breast and ovarian cancer . 
 o stromal content is correlated with tissue site , contrast retention , and survival in pancreatic adenocarcinoma purpose desmoplastic stroma is a cardinal feature of primary pancreatic ductal adenocarcinoma ( pda ) , but its effects on the biology , prognosis , and therapeutic outcomes in the disease are not known . 
we developed an automated method to assess tumor stroma density ( tsd ) and investigated computed tomography ( ct ) correlates of stroma in pda . patients and methods we collected pda samples from rapid autopsy and resection series and digitally annotated samples to quantify tsd . 
2018 by american society of clinical oncology introduction primary pancreatic ductal adenocarcinoma ( pda ) tumors are composed of malignant epithelial cells infiltrating and surrounded by an abundant desmoplastic stroma ( ds ) that , in turn , typically composes most of the tumor volume.1 ds is a diverse matrix comprising many cell types ( eg , fibroblasts , pancreatic stellate cells , immune cells , blood vessels ) and extracellular matrix proteins such as collagen and hyaluronic acid.2 tumor epithelium and ds interact in important ways and mediate tumor growth , immune surveillance , metabolism , and , possibly , metastasis.3 - 6 the interest in therapeutically targeting ds in pda is increasing because of its purported role in impeding drug delivery and excluding immune cells from the tumor microenvironment.7 - 10 clinical trials targeting ds , however , have been disappointing , and more recent studies have found that reducing ds burden through various stroma - depletion strategies in mouse models can lead to more aggressive tumors.11 - 13 this underscores the complex role ds plays robert j . 
we applied this method to investigate the relationship between primary tumors and metastases in a cohort of patients with metastatic disease , and the relationship between tsd of primary tumors and survival in two cohorts of patients who had undergone tumor resection . another significant hurdle in the assessment of ds is the lack of noninvasive biomarkers that can inform us of the qualitative and quantitative aspects of the ds . 
 the university of california , san francisco ( ucsf ) , institutional pathology and imaging databases were queried to identify patients with pda who met the following inclusion and exclusion criteria : had undergone curative intent resection with pathology confirmation of pda , had standard preoperative , multiphase pancreatic protocol staging ct imaging within 60 days of surgery , did not have any neoadjuvant therapies , and had records of 12 months of imaging and clinical follow - up available for review . automated stroma quantification for the rapid autopsy cohort , tissue microarrays were used ; for the denmark and ucsf cohorts , whole - tissue sections were used . 
using definiens architect xd 2.4 and tissue studio 4.1 ( both definiens , munich , germany ) , the annotated images were segmented into different regions of interest ( rois ) : tumor epithelium , tumor desmoplasia , and glass . 
for each specimen , tumor stroma density ( tsd ) was calculated as follows : tsd = tumor desmoplasia area / total tumor area ct image acquisition and analysis standard , multiphase ct imaging was performed for staging purposes before surgery for all patients in the ucsf cohort . 
after intravenous injection of 120 ml of omnipaque 350 ct contrast material ( ge healthcare , chicago , il ) at a rate of 5 ml / second , a pancreatic parenchymal ( pp ) phase ct image and then a portovenous ( pv ) phase ct image were acquired . 
for each patient , the following normalized tumor enhancement ratios were calculated : pp phase = ( hutumor , pp hutumor , ne ) / ( huaorta , pp huaorta , ne ) pv phase = ( hutumor , pv hutumor , ne ) / ( huaorta , pv huaorta , ne )  . automated tsd was compared with manually quantified tsd and reviewed by a board - certified pathologist ( k.e.v. ) , blinded to clinical and pathologic data , in a set of 77 resected pda samples . 
overall survival ( os ) and recurrence - free survival ( rfs ) were compared in high versus low tsd groups using a cox proportional hazards model controlling for overall histologic tumor area , tumor differentiation , stage , american society of anesthesiologists classification , and smoking status . 
the likelihood ratio test was used to assess the relevance of variables relative to the reduced model with that variable removed . for the ucsf cohort , cox proportional hazards model as well as cox model with time - varying coefficients were used to analyze the rfs and os when stratified by high versus low tsd using the same threshold value as the denmark cohort , controlling for clinical and tumor pathology variables . 
for the tumor ct enhancement analysis of the ucsf cohort , the tumors were categorized as high versus low enhancement ratios using the median value , and a cox proportional hazards model was used to analyze the rfs and os controlling for clinical and tumor pathology variables . results correlation of automated and manual quantification of tsd automated quantification of tsd was optimized using whole - tissue sections of primary pda tumors . 
these results suggest that pda stroma is not uniformly abundant across metastatic sites and is least abundant in solid organ metastases . high tsd was a favorable prognostic factor in resectable pda tumors automated tsd quantification was performed on samples from 123 patients with available tissue from copenhagen , denmark.20 this included 63 men and 60 women , whose mean age was 62 years at the time of surgery ( range , 33 to 87 years )  . 
 ( b ) automated segmentation of tumor epithelium ( green ) and tumor stroma : fibrosis - high stroma ( yellow ) and fibrosis - low stroma ( pink ) ( magnification , 10 )  . 
this cohort included 20 men and 25 women undergoing resection at ucsf ( mean age , of 66.3 years [ range , 46 to 81 years ] ; table 1 )  . 
 ( a , b ) kaplan - meier curves of ( a ) rfs and ( b ) os for high versus low tsd in resected pancreatic adenocarcinoma ( pda ) specimens from the denmark patient cohort . 
 ( c , d ) kaplan - meier curves of rfs and os for high versus low tsd in resected pda specimens from the university of california , san francisco , patient cohort . 
these results suggest that patients in the ucsf cohort with high tsd had improved prognosis early on , but its protective effect diminished over time . preoperative ct enhancement patterns in patients with resectable pda tumors ct scanning of patients with pda classically demonstrates delayed enhancement after contrast administration.21 this pattern has been attributed to the presence of the abundant stroma.16 therefore , we investigated the association of ct enhancement in primary ( resected ) pda and tsd , as well as the association between ct enhancement and survival in the ucsf cohort . 
 ( a ) an example of a tumor with high normalized enhancement ratio at both pancreatic parenchymal ( pp ) and portovenous ( pv ) phases of the ct studies . 
 ( c , d ) kaplan - meier curves of recurrence - free survival ( rfs ) and overall survival ( os ) for high versus low pv tumor enhancement . 
tumor stromal density ( tsd ) is associated with portovenous ( pv ) computed tomography ( ct ) enhancement patterns in patients with resectable pancreatic ductal adenocarcinoma ( pda ) tumors . 
 box - and - whisker plots of tsd in tumors with high versus low normalized enhancement ratios in ( a ) the pancreatic parenchymal ( pp ) phase and ( b ) the pv phase . 
this algorithm was then used to demonstrate tsd varies across metastatic sites and that tsd of the primary tumor positively associates with survival . most pda patients die with metastases.22 although effective treatment of metastatic disease is the most important priority in pda , translational efforts and preclinical models have focused largely on primary tissues.23 we found significant differences in tsd across metastatic sites . 
prior work has demonstrated that metastatic pda tumors have limited driver - mutation heterogeneity when compared with the primary tumor and largely concordant tumor - specific gene expression patterns in samples across many primary and metastatic sites.17 , 24 however , metastatic sites may have different proteomic profiles.25 these important observations , coupled with our results , suggest the variation in tsd is a function of host organ - site physiology and not secondary to cancer genomic or epigenomic / transcriptional differences between the primary and metastatic tumors . 
different sites of pda likely react differently to tumor cells with respect to generation of ds that may have therapeutic implications . we found that tsd correlated with both rfs and os in a mature cohort of patients with resected pda tumors who did not undergo adjuvant therapy . 
our prognostic findings imply a protective role of stroma in pda pathogenesis , in agreement with prior studies that used subjective assessments of various stromal characteristics.3 , 7 , 26 in the ucsf cohort , where most patients received adjuvant therapy , a lower risk of recurrence or death was seen initially in patients with high tsd , but the risk for both increased over time , with the survival curves eventually crossing . 
the denmark cohort did not receive any adjuvant therapy.19 , 20 in contrast , 91% ( 41 of 45 ) of the patients in the ucsf cohort received adjuvant therapy soon after resection , which more recently has become the standard of care.27 interestingly , sinn et al8 showed that a qualitatively dense stroma in pda was associated with a significantly longer rfs and os in the conko - 001 trial , but this effect was restricted to patients in the observation group ( no adjuvant therapy until recurrence ) and not seen in patients randomly assigned to adjuvant gemcitabine.8 our findings , along with those of sinn et al , 8 suggest patients with tumors that have low tsd may benefit more from adjuvant chemotherapy , closing the survival gap between high tsd and low tsd seen in the denmark cohort . assessment of tsd is limited by the availability of adequate tissue samples . 
we showed that normalized tumor enhancement ratio at the pv phase on ct imaging was correlated with tsd and prognosis , in agreement with a prior study that demonstrated resected pda tumors with lower enhancement tended to be less fibrotic.16 the association between pda enhancement and tsd may be explained by the properties of the ct contrast materials that pass freely between the intravascular and extravascular extracellular space but do not cross intact cell membranes . 
another limitation of our study is that only one board - certified pathologist reviewed specimens for manual tsd quantification , from which we show good correlation between manual and automated tsd quantification . 
to limit any potential bias , manual quantification was done blinded to the results of automated quantification and all other clinical and pathologic data . in summary , we found tsd was lowest at solid organ metastases , and that higher tsd was positively associated with outcome in patients with resected pda tumors without adjuvant therapy . 
torphy no relationship to disclose zhen wang stock and other ownership interests : nextrast honoraria : ge healthcare ( inst ) research funding : guerbet ( inst ) patents , royalties , other intellectual property : nextrast ( inst ) travel , accommodations , expenses : ge healthcare ( inst ) aisha true - yasaki no relationship to disclose keith e . 
volmar no relationship to disclose rashid naim no relationship to disclose benjamin yeh stock and other ownership interests : nextrast honoraria : ge healthcare consulting or advisory role : ge healthcare research funding : ge healthcare , philips healthcare , guerbet patents , royalties , other intellectual property : patents related to imaging contrast materials travel , accommodations , expenses : ge healthcare julia s . 
hollingsworth stock and other ownership interests : sanguine therapeutics and diagnostics research funding : glycomimetics ( inst ) patents , royalties , other intellectual property : royalties on cell lines ( inst ) jen jen yeh no relationship to disclose eric a . 
sinn m , denkert c , striefler jk , et al : - smooth muscle actin expression and desmoplastic stromal reaction in pancreatic cancer : results from the conko - 001 study . 
catenacci dvt , junttila mr , karrison t , et al : randomized phase ib / ii study of gemcitabine plus placebo or vismodegib , a hedgehog pathway inhibitor , in patients with metastatic pancreatic cancer . 
zdemir bc , pentcheva - hoang t , carstens jl , et al : depletion of carcinoma - associated fibroblasts and fibrosis induces immunosuppression and accelerates pancreas cancer with reduced survival . 
iacobuzio - donahue ca , fu b , yachida s , et al : dpc4 gene status of the primary carcinoma correlates with patterns of failure in patients with pancreatic cancer . 
makohon - moore ap , zhang m , reiter jg , et al : limited heterogeneity of known driver gene mutations among the metastases of individual patients with pancreatic cancer . 
diana a , wang lm , dcosta z , et al : prognostic value , localization and correlation of pd - 1 / pd - l1 , cd8 and foxp3 with the desmoplastic stroma in pancreatic ductal adenocarcinoma . 
stein , md1 ; manjari pandey , md1 ; joanne xiu , phd2 ; hongseok tae , phd2 ; jeff swensen , phd2 ; sandeep mittal , md3 , 4 ; andrew j . 
variability existed for other luad metastasis sites , with adrenal metastases most likely to meet the cutoff of 10 mutations / mb ( 51% ) and bone metastases least likely to meet the cutoff ( 19% )  . 
checkmate 227 showed a 43% 1 - year progression - free survival ( pfs ) rate for patients with advanced nsclc with samples of 10 mutations / mb or greater receiving rstline nivolumab and ipilimumab compared with a pfs of 13% in patients who received platinum - based chemotherapy . 
 stein et al context key objective although tumor mutational burden ( tmb ) is an emerging biomarker described to predict benet to immune checkpoint inhibition in nonsmall - cell lung cancer , little is known about whether any difference exists between tmb and sample site , histology , or other tumor proling characteristics . knowledge generated in both lung adenocarcinoma and squamous cell carcinoma , tmb was more likely to be 10 mutations per megabase ( mb ) or greater in metastases compared with primary tumors and highest in lung adenocarcinoma brain metastases . 
lung squamous cell carcinoma primary tumors more commonly met this tmb cutoff than lung adenocarcinoma primary tumors ; poorly differentiated disease was more likely to have a tmb of 10 mutations / mb or greater . 
site - specic differences in programmed death ligand 1 positivity , stk11 and kras mutation rate , and other markers were observed along this tmb cutoff . relevance tmb is a heterogeneous biomarker in nsclc with important spatial and histologic distinctions . 
further work is needed to identify unique therapeutic approaches for brain metastases and other sites with high tmb . although a high tmb may predict for benet to icis in nsclc , additional information is necessary to maximize its clinical utility . 
here , we detail the distribution of tmb in nsclc based on sample site , comparing primary lesion data to metastases for both lung adenocarcinoma ( luad ) and lung squamous cell carcinoma ( lusc )  . methods study design and patients we evaluated a database of patients with advanced nsclc who underwent tumor proling between 2015 and 2017 with caris life sciences ( irving , tx ) , a clinical laboratory improvement amendmentscertied laboratory . 
luad nonbrain metastases were further subdivided into the following six categories as demarcated by the submitting provider : regional lymph thoracic , and other extranode , thoracic metastases . liver , bone , adrenal , tumor proling caris tumor proling included ihc , ngs , and tmb assessment , for which the methods have been previously described.10 , 11 the genomic dna of 592 cancer - related genes isolated from formalin - xed , parafn - embedded tumor samples were sequenced using nextseq ( illumina , san diego , ca )  . 
variants were detected with greater than 99% condence based on allele frequency and amplicon coverage , with an average sequencing depth of coverage greater than 500 times and analytic sensitivity of 5% variant frequency . 
tmb ( mutations per mb ) was calculated in accordance with the tmb harmonization project , 13 adding nonsynonymous , nonsense , in - frame indel and frameshift variants after ltering out presumed germline variants determined from the genome aggregation database ( release 2.1 ) , the single nucleotide polymorphism database human build 151 , and the caris in - house benign database . 
although ngs obtained from bone metastases with conventional decalcication methods with strong acids leads to reduced success rates , 14 we nd similar reporting rates of ngs and tmb for bone specimens compared with other sites by using an edta - based decalcication approach or nondecalcied specimens . pd - l1 ihc was completed on slides of tumor sections using procedures in accordance with the college of american pathologists . 
sp142 ( spring bioscience , pleasonton , ca ) was the antibody used against pd - l1 before january 2016 ; thereafter , the primary antibody was 22c3 ( dako , santa clara , ca )  . 
 distribution of tmb by sample site in nsclc pattern.15 for ros1 and alk fusion detection , anchored multiplex polymerase chain reaction was performed for targeted rna sequencing using the archerdx ( boulder , co ) fusion assay ( archer fusionplex solid tumor panel )  . the formalin - xed , parafn - embedded samples were microdissected to enrich to 20% or more tumor nuclei , and mrna was isolated and reverse transcribed into gene - specic complementary dna . 
the sensitivity of the assay allows for fusion detection present in 10% or more of cells . statistical analysis the rate that tmb was reported as 10 mutations / mb or greater and frequency of other established nsclc biomarkers , including paths in egfr , kras , stk11 , braf ( v600e ) , alk , and ros1 rearrangements and pd - l1 ihc ( 1% and 50% ) , were compared between primary lesions and metastases . 
in addition , we compared the rate of selected molecular alterations along a tmb cutoff of 10 mutations / mb to identify any site - specic differences . statistical analysis was completed using spss version 20.0 ( spss , chicago , il )  . 
the median age of patients with luad with primary tumors sampled ( n = 1 , 102 ) was 69 years ( range , 25 to 90 years ) compared with 66 years ( range , 28 to 90 years ) for patients with metastases ( n = 1 , 249 )  . 
the median age of patients with lusc primary tumors ( n = 779 ) was 71 years ( range , 23 to 90 years ) compared with 67 years ( range , 24 to 90 years ) for patients with metastases ( n = 294 )  . 
a similar percentage of primary luad and lusc tumors were poorly differentiated ( 20% v 26% , respectively ) compared with metastases ( 21% and 29% , respectively )  . of 10 tumor proling characteristics evaluated , six luad and four lusc differences were observed between primary and metastatic lesions ( table 1 )  . 
figure 2 depicts a scatter plot of tmb and pd - l1 for luad and lusc , for which no correlation was found . tmb increases with metastases and is highest in luad brain metastases to further assess luad and lusc by location , we divided metastases into brain and nonbrain metastases and compared them to primary tumors . 
both brain and nonbrain luad metastatic lesions were associated with increased stk11 and stk11 plus kras comutated paths and tmb of 10 mutations / mb or greater compared with primary tumors ( table 2 )  . in addition , compared with primary luad , patients with nonbrain metastasis were more likely to be male and alk rearranged and have higher rates of pd - l1 expression of 1% or greater and 50% or greater . 
figure 3a shows the rate that tmb was reported as 10 mutations / mb or greater based on sample site , comparing not only primary tumor and brain metastasis , but also nonbrain metastasis and six subdivisions ( table 3 )  . 
samples from adrenal metastases ( 51% ) and other extrathoracic metastases ( 43% ) were more likely to have a tmb of 10 mutations / mb or greater , and bone metastases ( 19% ) were less likely to have a tmb of 10 mutations / mb or greater . of 294 lusc metastases , 19 were brain metastases and 275 were other metastases . 
for lusc , a reduced frequency of egfr ( p = .025 ) and pd - l1 expression of 1% or greater ( p = .008 ) was found for metastases when tmb was 10 mutations / mb or greater ( appendix table a1 )  . 
nine of 10 and four of 10 sample site divisions had reduced egfr paths and alk rearrangements in cases where tmb was 10 mutations / mb or greater , respectively . 
here , we detail ndings from a large nsclc cohort with tmb data , providing novel insights with respect to tmb and sample acquisition site and histology , while also comparing the interplay of tmb with established and other emerging biomarkers . 
although wes may be considered a gold standard given its breadth , high cost and prolonged result times have contributed to the use of tmb from ngs panels . although more efcient and commercially available , accurate quantitation of tmb from ngs introduces additional nuance , including the number of genes needed for extrapolation ( ideally 1 mb ) , type of enrichment ( hybrid capture or amplication ) , and read depth.8 , 25 , 26 a limitation of our ngs data is that tmb was not correlated with wes from a subset of samples , although it was calculated in accordance with the tmb harmonization project.13 although we found that tmb was more likely to be 10 mutations / mb or greater in metastases compared with primary tumors , a range existed based on anatomic site for both luad and lusc , with brain and adrenal subgroups more likely and bone and liver lesions less likely to meet this cutoff in luad . 
 ( a ) frequency of lung adenocarcinomas ( luads ) with tumor mutational burden ( tmb ) of 10 mutations per megabase ( mb ) or greater varies by sample site and is highest in brain metastases . ( b ) lung squamous cell carcinoma ( lusc ) metastases are more likely to have a tmb of 10 mutations / mb or greater compared with primary tumor samples . 
although retrospective studies from trial patients or clinical practice have shown an amalgamation of improved overall response rates , pfs , and os for different icis at various tmb cutoffs , 24 , 26 prospective os benet remains to be shown . 
this could be particularly important for brain metastases , which occur in 40% of nsclcs , 40 portend a poor prognosis , and have historically lacked viable treatments.41 because standard chemotherapy has reduced blood - brain penetrance , 42 dual checkpoint inhibition should be compared with chemoimmunotherapy in this high - risk subgroup . we found that less than 3% of primary and 6% of metastatic egfr - mutated luad samples and no alk - rearranged samples had a tmb of 10 mutations / mb or greater . 
a comparatively elevated tmb in other patients correlates with recently described smoking and apolipoprotein b mrna - editing enzyme , catalytic polypeptide - like ( apobec ) mutation signatures.45 , 46 we observed several site - specic molecular combinations with tmb . 
furthermore , anatomic sites in luad including adrenal and other extrathoracic specimens were more likely to meet a threshold of 10 mutations / mb and have 1% or greater pd - l1 expression . 
because samples that are both pd - l1 positive and tmb high may derive improved benet from pd - 1 / pd - l1 inhibition , 29 our data show anatomic differences in this biomarker combination that could be clinically informative for icis . we found anatomic differences between tmb and stk11 , including the nding that luad metastases were less likely to be stk11 and kras comutated if tmb was 10 mutations / mb or greater . 
an emerging biomarker afliated with resistance to pd - 1 / pd - l1 inhibition and reduced immunogenicity in mouse models and patients with nsclc , 44 , 47 , 48 sitespecic differences in stk11 with tmb may add complexity to treating this molecular subset with novel approaches . another limitation of our study includes the reduced number of lusc metastases available , making analysis less powerful . 
furthermore , ndings such as a high egfr mutation rate in luad liver metastases could skew tmb accuracy . in addition , we are unable to provide prior therapies received for patients and the stage at time of tissue acquisition for primary tumor samples . 
although we show that surgically obtained primary tumors have similar rates of tmb of 10 mutations / mb or greater as other primary tumors , further evaluation is needed to determine whether a difference exists between , for example , early stage i and locally advanced stage iii disease or between stage iii and iv lesions . overall , we demonstrate that tmb is a site - specic biomarker in nsclc with important spatial and histologic differences . 
in both luad and lusc , the frequency of specimens with a tmb of 10 mutations / mb or greater is increased in metastases and highest with brain metastases . poorly differentiated disease from either histology was more likely to have a tmb of 10 mutations / mb or greater compared with other primary tumors or metastases . 
michael korn employment : caris life sciences leadership : caris life sciences stock and other ownership interests : oncocyte consulting or advisory role : merck sharp & dohme patents , royalties , other intellectual property : exelixis travel , accommodations , expenses : merck sharp & dohme amy b . 
heimberger stock and other ownership interests : celldex , caris life sciences consulting or advisory role : caris life sciences research funding : merck patents , royalties , other intellectual property : celldex travel , accommodations , expenses : caris life sciences mike g . 
martin consulting or advisory role : seattle genetics no other potential conicts of interest were reported . references yarchoan m , hopkins a , jaffee em : tumor mutational burden and response to pd - 1 inhibition . 
n engl j med 377 : 2500 - 2501 , 2017 ramalingam ss , hellmann ad , awad mm , et al : tumor mutational burden ( tmb ) as a biomarker for clinical benet from dual immune checkpoint blockade with nivolumab ( nivo ) + ipilimumab ( ipi ) in rst - line ( 1l ) non - small cell lung cancer ( nsclc ) : identication of tmb cutoff from checkmate 568 . 
n engl j med 378 : 2093 - 2104 , 2018 fr uh m , peters s : genomic features of response to combination immunotherapy in patients with lung cancer . 
mutational landscape determines sensitivity to pd - 1 blockade in non - small cell lung cancer . science 348 : 124 - 128 , 2015 carbone dp , reck m , paz - ares l , et al : first - line nivolumab in stage iv or recurrent non - small - cell lung cancer . 
hellmann md , nathanson t , rizvi h , et al : genomic features of response to combination immunotherapy in patients with advanced non - small - cell lung cancer . cancer cell 33 : 843 - 852.e4 , 2018 chalmers zr , connelly cf , fabrizio d , et al : analysis of 100 , 000 human cancer genomes reveals the landscape of tumor mutational burden . 
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vanderwalde a , spetzler d , xiao n , et al : microsatellite instability status determined by next - generation sequencing and compared with pd - l1 and tumor mutational burden in 11 , 348 patients . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
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cappuzzo f , mccleod m , hussein m , et al : impower130 : progression - free survival ( pfs ) and safety analysis from a randomised phase iii study of carboplatin + nab - paclitaxel ( cnp ) with or without atezolizumab ( atezo ) as rst - line ( 1l ) therapy in advanced non - squamous nsclc . 
reck m , rodrguez - abreu d , robinson ag , et al : updated analysis of keynote - 024 : pembrolizumab versus platinum - based chemotherapy for advanced nonsmall - cell lung cancer with pd - l1 tumor proportion score of 50% or greater . 
allg auer m , budczies j , christopoulos p , et al : implementing tumor mutational burden ( tmb ) analysis in routine diagnostics : a primer for molecular pathologists and clinicians . 
transl lung cancer res 7 : 703 - 715 , 2018 jamal - hanjani m , wilson ga , mcgranahan n , et al : tracking the evolution of non - small - cell lung cancer . 
gandara dr , paul sm , kowanetz m , et al : blood - based tumor mutational burden as a predictor of clinical benet in non - small - cell lung cancer patients treated with atezolizumab . 
rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
kowanetz m , zou w , shames ds , et al : tumor mutation burden ( tmb ) is associated with improved efcacy of atezolizumab in 1l + and 2l + nsclc patients . 2019 j clin oncol 34 : 9017 , 2016 ( suppl 15 ; abstr 9017 ) j thorac oncol 12 : s321 - s322 , 2017 33 . 
gandara d , kowanetz m , mok t , et al : blood - based biomarkers for cancer immunotherapy : tumor mutational burden in blood ( btmb ) is associated with improved atezolizumab ( atezo ) efcacy in 2l + nsclc ( poplar and oak )  . 
ross j , goldberg m , albacker l , et al : immune checkpoint inhibitor ( icpi ) efcacy and resistance det5ected by comprehensive genomic proling ( cgp ) in nonsmall cell lung cancer ( nsclc )  . 
singal g , miller p , agarwala v , et al : analyzing biomarkers of cancer immunotherapy ( cit ) response using a real - world clinico - genomic database . 
park w , lopes g , kwon d , et al : correlating isend and tumor mutation burden ( tmb ) with clinical outcomes of advanced non - small cell lung cancer ( ansclc ) patients on nivolumab . 
ready n , hellmann md , awad mm , et al : first - line nivolumab plus ipilimumab in advanced non - small - cell lung cancer ( checkmate 568 ) : outcomes by programmed death ligand 1 and tumor mutational burden as biomarkers . 
bristol - meyers squibb : bristol - myers squibb provides update on the ongoing regulatory review of opdivo plus low - dose yervoy in rst - line lung cancer patients with tumor mutational burden 10 mut / mb . 
schrock a , sharma n , peled n , et al : updated dataset assessing tumor mutation burden ( tmb ) as a biomarker for response to pd - 1 / pd - l1 targeted therapies in lung cancer ( lc )  . 
koyama s , akbay ea , li yy , et al : stk11 / lkb1 deciency promotes neutrophil recruitment and proinammatory cytokine production to suppress t - cell activity in the lung tumor microenvironment . 
 association of germline genetic test type and results with patient cancer worry after diagnosis of breast cancer background there are concerns that multigene panel testing compared with brca1 / 2 - only testing after diagnosis of breast cancer may lead to unnecessary patient worry about cancer because of more ambiguous results . methods patients with breast cancer diagnosed from 2013 to 2015 and accrued from seer registries in georgia and los angeles were surveyed ( n = 5 , 080 ; response rate , 70% ) , and responses were merged with seer data and germline genetic testing and results . 
we examined patient reports of cancer worry by test type and results in 1 , 063 women who linked to a genetic test and reported undergoing testing . results more than half of the sample ( n = 640 ; 60.2% ) received brca1 / 2 - only testing versus 423 patients ( 39.8% ) who had a multigene panel . 
a minority of tested patients reported substantial cancer worry after treatment : 11.1% ( n = 130 ) reported higher impact of cancer worry , and 15.1% ( n = 162 ) reported a high frequency of cancer worry ( worrying often or almost always ) in the past month . 
2018 by american society of clinical oncology introduction multiple - gene panel ( mgp ) testing has rapidly replaced brca1 / 2 - only testing after diagnosis of breast cancer.1 however , genetic testing use in patients who need it seems to be low.2 , 3 one barrier to more robust uptake of mgp testing is uncertainty about its clinical utility . 
indeed , some have argued that mgp testing should not replace brca1 / 2 - only testing , even in patients with higher pretest risk of a pathogenic mutation , because of these concerns about patient reactions , 4 whereas others strongly disagree.5 current clinical guidelines that recommend genetic testing in women at elevated pretest risk of carrying a pathogenic variant do not specify how many genes should be tested . 
we sent surveys to 7 , 810 patients : 507 patients were ineligible because of the exclusions noted previously or were deceased , institutionalized , too ill , or unable to complete a survey in spanish or english , leaving 7 , 303 patients . 
virtually all patients ( 5 , 026 ) had complete information for the test linkage phase , of whom 1 , 272 ( 25.3% ) linked to a genetic test result , 1 , 063 of whom ( 21.2% ) reported receipt of genetic testing in the survey . survey responses were merged with seer clinical data and genetic testing information obtained from four laboratories ( ambry genetics , aliso viejo , ca ; genedx , gaithersburg , md ; invitae , san francisco , ca ; myriad genetics , salt lake city , ut ) that performed nearly all germline cancer genetic testing in the study regions . 
test type and results were merged to 5 , 026 patients with complete information on all variables for seer genetic testing linkage using a probabilistic matching strategy performed by information management services ( rockville , md )  . 
the safe harbor method was used to de - identify the data set before transfer to the university of michigan for analysis.9 the collaboration was covered under data use agreements between the university of michigan , genetic laboratories , and information management services . 
the research was approved by institutional review boards of the university of michigan , emory university , the university of southern california , the georgia department of public health , the california state committee for the protection of human subjects , and california cancer registry . 
waivers of informed consent and authorization were approved , given the use of a third - party honest broker to conduct the linkage and create a de - identified data set for analyses . measures we used two questions to evaluate patient worry about future cancer . 
forest plot ( adjusted odds ratios and 95% cis ) for results of a multivariable model regressing a binary variable indicating higher versus low impact of cancer worry on test type , controlling for selected predisposing , clinical , and treatment factors and weighted for survey design and nonresponse . 
er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; hs , high school ; mgp , multigene panel ; pr , progesterone receptor ; ref , reference . made it difficult for you to carry out your usual daily activities at home or work ? ; made you feel distant from family or friends ? ( responses were based on 5 - point likert categories from almost never to almost always )  . 
we developed a scale by averaging the responses across the three items to create a continuous range from 1 to 5 , with higher values indicating greater impact of cancer worry . 
we then created a binary variable indicating higher impact of cancer worry versus low impact using a cut point of 3.0 , which corresponded to responses of sometimes , often , or almost always . 
we also measured frequency of cancer worry for validation , which was assessed using a single item : in the past month , how often have you worried about your cancer coming back ? ( almost never to almost always ; five point categories )  . 
genetic laboratories provided results at the level of the gene tested ( eg , brca1 ) and the clinical interpretation sent to the ordering clinician ( consisting of pathogenic , likely pathogenic , uncertain significance , likely benign , or benign )  . 
we categorized a test that assessed only brca1 / 2 as brca1 / 2 only and a test that assessed any additional gene ( eg , atm , chek2 ) as a multigene panel . 
if patients received both tests on separate occasions ( eg , a brca1 / 2 - only test and later mgp ) , they were coded as having received mgp . 
we assessed clinical factors related to future cancer risk ( tumor behavior , triple - negative disease , nodal status , bilateral disease ) , treatments received , age ( in 10 - year groups ) , education , and family history . 
 defined as having two or more first - degree relatives with breast cancer ; any relatives with ovarian cancer , sarcoma , or male breast cancer ; ashkenazi jewish ancestry ; or a family history of a mutation - conferring risk ( eg , brca1 / 2 )  . statistical analysis we first examined cancer worry variables by test type , test results , and selected covariables . 
a minority of tested patients reported substantial cancer worry after treatment : 11.1% ( n = 130 ) reported high impact of cancer worry , and 15.1% ( n = 162 ) reported high frequency of worry ( worrying often or almost always in the past month )  . 
we observed similar findings in a model of frequency of cancer worry ( data not shown )  . figure 1 shows the results of a multivariable model regressing a binary variable indicating higher versus low impact of cancer worry on test type , controlling for selected predisposing , clinical , and treatment factors . 
in sensitivity analyses , we examined different permutations of the cancer worry variables , including different cut points for higher worry , and using a continuous variable , and results were consistent . discussion we found that the type of genetic testing patients received ( mgp v brca1 / 2 only ) was not associated with their report of cancer - related worry ( impact or frequency )  . 
 as noted in our prior work , cancer - related worry was associated with younger age and lower educational level , but not clinical factors.10 , 11 strengths of this study include a large population based sample of patients recently diagnosed with breast cancer and accrued shortly after the advent of multigene panel testing in the community , genetic testing results from companies linked to seer clinical data , and granular information about patients , including their report of cancer - related worry . 
we excluded them from the analytic sample because we did not think it was valid to assess the association of a test type with attitudes about health risk among patients who did not recall that they had the test . 
finally , generalizability of the findings are limited to two large geographic regions of the united states . the results from this study and our prior work suggest that testing more genes versus brca1 / 2 alone does not seem to foment more negative patient reactions . 
our prior research in this cohort suggested that mgp testing ( v brca1 / 2only testing ) does not lead to inappropriate rates of contralateral prophylactic mastectomy.1 virtually all testers in this study received some form of genetic counseling , 6 and our results suggest these efforts may sufficiently frame results in a manner that did not alarm patients . 
kurian manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors paul abrahamse no relationship to disclose sarah t . 
dolinsky , cgc , and melissa pronold at ambry genetics , delores bowman and benjamin solomon at genedx , edward esplin and stephen lincoln at invitae , and johnathan lancaster and brian dechairo at myriad genetics for their collaboration on the genetic test data linkage to seer data . 
the collection of los angeles county cancer incidence data used in this study was supported by the california department of public health pursuant to california health and safety code section 103885 , centers for disease control and preventions ( cdcs ) national program of cancer registries , under cooperative agreement 5nu58dp003862 - 04 / dp003862 , the national cancer institutes seer program under contract hhsn261201000140c awarded to the cancer prevention institute of california , contract hhsn261201000035c awarded to the university of southern california , and contract hhsn261201000034c awarded to the public health institute . 
the collection of cancer incidence data in georgia was supported by contract hhsn261201300015i , task order hhsn26100006 from the national cancer institute and cooperative agreement 5nu58dp003875 - 04 - 00 from the cdc . 
us department of health & human services : guidance regarding methods for de - identification of protected health information in accordance with the health insurance portability and accountability act ( hipaa ) privacy rule . 
janz nk , li y , zikmund - fisher bj , et al : the impact of doctor - patient communication on patients perceptions of their risk of breast cancer recurrence . 
forest plot ( adjusted odds ratios and 95% cis ) showing results of multivariable logistic regression for higher impact of cancer worry ( complete case n = 1 , 044 )  . 
 genetic testing for prostate cancer in clinical practice see accompanying article doi : there is increasing recognition of the role of inherited single - gene high - penetrance mutations in prostate cancer predisposition . 
in some ways , we are now learning for prostate cancer what has been known in the breast and ovarian cancer communities for at least two decadesthat patients with inherited mutations in genes such as brca1 and brca2 represent a clinically meaningful subset and cause a sufficiently high proportion of lethal cancers to warrant consideration of genetic testing in the appropriate clinical context ( eg , early - onset diagnosis )  . 
10% of men with metastatic prostate cancer have inherited mutations in dna repair genes.1 - 4 mutations were also found in approximately 5% of men with highrisk localized disease , with far lower prevalence in low - risk indolent cancers.2 , 3 in parallel , there is strong emerging evidence that these mutations may predict response to poly - adp ribose polymerase ( parp ) inhibitors and platinum - based chemotherapy.5 - 7 these findings make genetic testing appealing for the purpose of treatment selection and risk stratification , and testing is readily accessible , with widespread commercial availability of clinical multigene cancer predisposition panels . 
however , we have incomplete knowledge about who is best to test , when to test , and , importantly , how to counsel patients on the results with regard to their personal and family cancer risks . 
for example , testing may be ordered for the primary purpose of treatment selection without adequate preand post - test counseling by oncologists or urologists who are unaccustomed to genetic testing . 
for these reasons , there is urgency to better understand issues related to genetic counseling of men with prostate cancer who undergo cancer predisposition genetic panel testing . in the article that accompanies this editorial , giri et al8 describe the results of the genetic evaluation of men ( gem ) study . 
mutations were detected in genes related to dna repair , including brca1 , brca2 , atm , brip1 , msh6 , and mutyh . the relatively common chek2 p.i157t lowpenetrance risk variant was excluded from the analysis . the study has several findings that are important to inform genetic counseling in men . 
first , there was a significant association of a family history of breast cancer and being a pathogenic mutation carrier , confirming findings from earlier studies and highlighting the importance of both asking men about family history of breast cancer and counseling men with a strong family history of breast cancer of potentially increased risk for inherited mutations also predisposing to prostate cancer . 
third , mutations may be detected in at - risk unaffected men in genes other than brca1 and brca2 for which there are no established prostate cancer risk estimates or screening guidelines . 
the two mutations detected in this context were in msh6 , a mismatch dna repair gene associated with lynch syndrome , and in brip1 , a homologous recombination dna repair gene best established in ovarian cancer predisposition . 
even for brca1 and brca2 mutation carriers , the guidelines have yet to be firmly established , with the national comprehensive cancer network guidelines committees for prostate cancer early detection and for breast / ovarian cancer genetic high - risk assessment currently providing slightly different screening recommendations.9 , 10 the ongoing international impact ( identification of men with a genetic predisposition to prostate cancer ) prostate cancer screening trial is expected to provide valuable data to inform screening guidelines for brca1 and brca2 mutation carriers and has begun to enroll men with mismatch dna repair gene mutations.11 however , management for at - risk , unaffected men with mutations in genes such as brip1 will need to rely on clinical findings and family history until more data are collected . large - panel genetic testing may be associated with a high rate of variants of uncertain significance ( vus )  . more than one third of men in the study ( 70 of 200 , 35% ) had a vus reported back . 
vus reports may be particularly problematic when communicated to a patient by a nongenetics expert , because of the risk that the result is misinterpreted as a positive or actionable mutation finding . 
it is generally accepted that patients with vus should be managed solely on the basis of clinical findings and family history , similar to the case of a negative genetic testing result . 
vus rates vary among laboratories performing multigene cancer predisposition testing , so it is important to learn the expected vus rate in the performing laboratory to appropriately counsel men undergoing testing . 
fortunately , vus rates in cancer predisposition panel reporting are decreasing as more information is learned about newer genes and variant classification procedures are updated . this study has important limitations . 
it is therefore difficult to draw conclusions on the prevalence of mutations in most of the subgroups , which do not approach statistical significance . a much larger cohort will be needed to answer some of these important questions . 
there are known prostate cancer predisposition variants such as hoxb13 p.g84e that were not tested , and the authors note that they plan to follow up with hoxb13 testing.12 in addition , mutyh heterozygous carriers were included among the 11 mutation - positive patients . 
a recent study did not find an association of mutyh carrier mutations and prostate cancer.13 we are beginning to see increased cancer predisposition panel testing for men in clinical practice , largely driven by the excitement of tailoring treatments for prostate cancer . 
hart sn , ellingson ms , schahl k , et al : determining the frequency of pathogenic germline variants from exome sequencing in patients with castrate - resistant prostate cancer . 
na r , zheng sl , han m , et al : germline mutations in atm and brca1 / 2 distinguish risk for lethal and indolent prostate cancer and are associated with early age at death . 
mateo j , carreira s , sandhu s , et al : dna - repair defects and olaparib in metastatic prostate cancer . n engl j med 373 : 1697 - 1708 , 2015 8 . 
bancroft ek , page ec , castro e , et al : targeted prostate cancer screening in brca1 and brca2 mutation carriers : results from the initial screening round of the impact study . 
shang z , zhu s , zhang h , et al : germline homeobox b13 ( hoxb13 ) g84e mutation and prostate cancer risk in european descendants : a meta - analysis of 24 , 213 cases and 73 , 631 controls . 
 characterization of the epidermal growth factor receptor t790m mutation in colorectal cancer introduction the epidermal growth factor receptor ( egfr ) t790m mutation is a commonly found mutation encountered in approximately 60% of patients with nonsmall - cell lung cancer ( nsclc ) .1 it is the most frequent cause of resistance to anti - egfr therapy in nsclc.1 the biology behind the resistance is that the egfr t790m mutation increases the affinity of egfr for atp and attenuates the binding affinity of first generation anti - egfr tyrosine kinase inhibitors ( tkis ; gefitinib ) as well as second - generation anti - egfr tkis ( dacomitinib ) .1 , 2 however , third - generation anti - egfr tkis ( osimertinib ) were found to be more potent against egfr t790m - mutant cancer1 , 3 and are currently approved for patients with egfr t790m mutationpositive nsclc.4 in contrast , the egfr t790m mutation is rarely found in colorectal cancer ( crc )  . 
in this study , we are the first to our knowledge to report and characterize a patient with an egfr t790m - mutated crc . adenocarcinoma , and pathology of the anorectal mass was intramucosal adenocarcinoma ( fig 1b )  . given the concern for potentially three primaries , the patient underwent a right lower lobe segmentectomy with pathology revealing poorly differentiated adenocarcinoma . 
finally , a right hemicolectomy was performed and demonstrated a low - grade mucinous adenocarcinoma , invading through the muscularis propria into pericolonic rectal tissues ; 0 / 25 lymph nodes did not contain cancer ( stage pt3n0 )  . 
biopsy of the colonic mass was consistent with moderately differentiated characterization of the egfr t790m mutant tumor our patient presented with four primary cancers ( breast , lung , colon , and rectal ) , and we were able to obtain samples on the breast , lung , and colon specimens for additional studies . 
 ( a ) positron emission tomography ( pet ) scan images showing ( i ) breast , ( ii ) colon , and ( iii ) lung tumors of the patient . 
photomicrographs of the colonic adenocarcinoma demonstrated infiltrative glands lined in some areas by pseudostratified dysplastic columnar epithelium consistent with colonic origclassic features of primary adenocarcinoma of the colon , including intraluminal necrosis and mucin production , were also evident . 
using our duke next - generation sequencing panel ( ionampliseq cancer hotspot panelv2 ) , which covers more than 2 , 800 cosmic ( catalogue of somatic mutations in cancer ) mutations from 50 cancer genes , all three primaries were found to have the egfr t790m mutation ( fig 1c ) , with allele frequencies of 42% to 52% , suggesting a possible germline origin for this mutation . 
in addition , the breast cancer was found to have a pik3ca ( n345k ) mutation ; the lung primary had erbb4 ( l933f ) , gnaq ( i226v ) , and tp53 ( n239s ) mutations ; and the colon primary had abl1 ( g259c ) , apc ( s1465wfs ) , and braf ( v600e ) mutations ( fig 1c )  . 
these results suggest that these tumors are biologically distinct . development of patient - derived models of cancer because the three tumors seemed biologically distinct , we decided to further characterize these tumors by generating patient - derived models of cancer ( patient - derived xenografts [ pdx ] and matched cell lines ) , as previously described.5 , 6 of the three primaries , we were only able to obtain patient - derived models of cancer from the colon cancer specimen . 
 ii oxaliplatin ( ic50 undefined ) irinotecan ( ic50 0.28 ( cid : 80 ) m ) fluorouracil ( ic50 4.3 ( cid : 80 ) m ) 1 , 000 log ( dose , nm ) control oxaliplatin control irinotecan control fluorouracil 1 , 500 1 , 000 1 , 500 1 , 000 treatment ( days ) treatment ( days ) treatment ( days ) fig 2 . 
 ( a ) histologic features of the patients ( i ) colon tumor , ( ii ) patient derived xenograft model , and ( iii ) matched cell line image . 
 ( b ) in vitro ic50 ( half maximal inhibitory concentration ) studies with oxaliplatin , irinotecan , and fluorouracil suggesting that patients colon tumor was resistant to oxaliplatin , sensitive to irinotecan , and indeterminate to fluorouracil . 
ic50 values of the three cytotoxic chemotherapeutic agents ( oxaliplatin , irinotecan , and fluorouracil ) were found to be 25 m , 0.2 m , and 4.3 m , respectively ( fig 2b )  . 
although our in vitro data were indeterminate for fluorouracil , our in vivo data suggest sensitivity to fluorouracil ( fig 2c )  . next , we performed in vitro ic50 studies with the three us food and drug administration approved egfr inhibitors ( cetuximab , erlotinib , osimertinib ) to determine the effect of antiegfr therapy in our egfr t790m mutant colon tumor . 
ic50 values were found to be 25 m ( cetuximab ) , 2 m ( erlotinib ) , and 0.38 m ( oximertinib ) , respectively ( fig 3a ) , suggesting that the tumor was resistant to cetuximab and erlotinib and sensitive to osimertinib . 
similar to nsclc , where egfr t790m mutation is resistant to erlotinib and sensitive to osimertinib , 7 our pdx tumor was also found to be resistant to erlotinib and sensitive to osimertinib ( fig 3b )  . the matched cell line was then used for high - throughput drug screening to identify drug sensitivity to 29 egfr inhibitors . 
 ( a ) in vitro ic50 studies ( half maximal inhibitory concentration ) with anti - egfr therapeutics suggesting that osimertinib , a third generation egfr inhibitor , caused more cell inhibition than cetuximab and erlotinib . 
her braf mutation indicated that she does not have lynch syndrome , but given the genetic disposition of the egfr t790m mutation in lung cancer9 and her family history ( patient has a brother with brain cancer , sister with brain and lung cancer , sister with lung cancer , and sister with throat cancer ) , it remains to be seen whether this mutation is acquired in crc . 
to date she remains disease free , although she has some indeterminate small lung nodules that are currently being followed . the ability to biobank her cancers allowed us to develop patient - derived models of cancer to investigate the biology of her cancer and to identify potential therapeutic agents . 
furthermore , her cancer allowed us to develop a precision medicine pipeline , where a patients cell lines can be used to perform in vitro drug screen with in vivo validation to identify the most beneficial therapy . 
specifically , our preclinical modeling suggests that her tumor is sensitive to irinotecan and fluorouracil but resistant to oxaliplatthis would suggest that if she were to experience recurrence with metastatic disease , we should consider an irinotecan - based therapy for her initial therapy . in addition , we identified osimertinib as an effective anti - egfr therapeutic for the treatment of her colon tumor . 
finally , high - throughput drug screening allowed us to test 29 different anti - egfr agents , including first - , second - , and third generation egfr inhibitors . 
similar to the studies on egfr t790m mutationpositive nsclc , 3 , 10 we observed sensitivity to the third - generation egfr inhibitors and resistance to the first - generation egfr inhibitors , suggesting that egfr t790m mutation in crc shows similar biologic features with nsclc . 
high - throughput drug screening using patient derived cell lines revealed sensitivity and resistance to a number of first - , second - , and third - generation epidermal growth factor receptor inhibitors . in conclusion , the development of a precision medicine pipeline using matched cell lines and pdx models can be a powerful tool to understand tumor biology and to test new therapies , and this approach can be used to quickly translate bench findings to the bedside and guide patient care . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . erdem altunel no relationship to disclose abed alhalim aljamal no relationship to disclose kristen deak consulting or advisory role : lineagen wayne glover no relationship to disclose shannon j . 
mccall no relationship to disclose michael datto no relationship to disclose john strickler stock and other ownership interests : oncomed consulting or advisory role : amgen , genentech , bayer , celgene , chugai / roche , astrazeneca , seattle genetics research funding : abbvie ( inst ) , gilead sciences ( inst ) , genentech ( inst ) , exelixis ( inst ) , oncomed ( inst ) , sanofi ( inst ) , regeneron ( inst ) , medimmune ( inst ) , cascadian therapeutics ( inst ) , seattle genetics , macrogenics , leap therapeutics , nektar therapeutics david s . 
saad n , poudel a , basnet a , et al : epidermal growth factor receptor t790m mutation - positive metastatic non - small - cell lung cancer : focus on osimertinib ( azd9291 )  . 
odogwu l , mathieu l , goldberg kb , et al : fda benefit - risk assessment of osimertinib for the treatment of metastatic non - small cell lung cancer harboring epidermal growth factor receptor t790m mutation . 
pao w , miller va , politi ka , et al : acquired resistance of lung adenocarcinomas to gefitinib or erlotinib is associated with a second mutation in the egfr kinase domaplos med 2 : e73 , 2005 8 . 
hu y , alden rs , odegaard ji , et al : discrimination of germline egfr t790m mutations in plasma cell - free dna allows study of prevalence across 31 , 414 cancer patients . 
barnes ta , okane gm , vincent md , et al : third - generation tyrosine kinase inhibitors targeting epidermal growth factor receptor mutations in non - small cell lung cancer . 
 appendix generation of the patient - derived xenografts and cell line . tumor sample was obtained under a duke institutional review boardapproved protocol ( pro00002435 ) , and written informed consent was provided vy the patient to participate in the study . 
all mouse experiments were performed in accordance with the animal guidelines and with the approval of the institutional animal care and use committee at duke university medical center . patient - derived xenograft ( pdx ) models were generated by injecting tumor samples into the flanks of 8to 10 - week - old jax nod.cb17 - prkdcscid - j mice obtained from the duke university rodent genetic and breeding core . 
to develop matched pdx cell line , harvested pdx tumor was homogenized and grown in 10 - cm2 tissue culturetreated dishes in cell culture media ( dmem media , 10% fetal calf serum , 1% penicillin and streptomycin ) at 5% co2 . 
cell line was authenticated using the duke university dna analysis facility human cell line authentication service by analyzing dna samples from each individual cell line for polymorphic short - tandem repeat markers using the geneprint 10 kit from promega ( madison , wi )  . high - throughput drug screening and in vitro ic50 studies ( half maximal inhibitory concentration )  . to perform high - throughput drug screening , robotic systems ( echo acoustic dispenser [ labcyte , san jose , ca ] for drug addition , well mate [ thermo fisher , waltham , ma ] for cell plating , and clarioscan [ bmg labtech , cary , nc ] for plate reading ) were used in each step of the screening process . 
a total of 384 well plates were first coated with a total of 2 , 100 drug compounds at a final concentration of 1 m , and then 1 , 000 cells / well were plated in the drug - precoated wells . 
three replicates were used for each drug . to perform ic50 studies , the cell lines were cultured in dmem plus 10% fetal bovine serum plus 1% penicillin / streptomycin and plated in drug - free medium at a concentration of 3 , 000 cells / well in 96 - well plate . 
 ic50 values were calculated using graphpad prism software ( la jolla , ca )  . in vivo drug sensitivity assays . mouse experiments were carried out in accordance with the animal guidelines and with the approval of the institutional animal care and use committee at the duke university medical center . 
to test drug sensitivities for each drug , 150 l of homogenized pdx tissuephosphate - buffered saline suspensions at 150 mg / ml concentration were subcutaneously injected into right flanks of five female and five male mice ( jax nod.cb17 - prkdcscid - j , 10 weeks old )  . 
randomly selected mice were treated with erlotinib ( 25 mg / kg ) or osimertinib ( 10 mg / kg ) orally five times a week ; oxaliplatin ( 10 mg / kg intraperitoneally per week ) , irinotecan ( 10 mg / kg intraperitoneally per week ) , fluorouracil ( 50 mg / kg intraperitoneally twice a week ) , and cetuximab ( 40 mg / kg intraperitoneally five times a week )  . 
hyman , md1 , 2 purpose matching patients to investigational therapies requires new tools to support physician decision making . we designed and implemented precision insight support engine ( precise ) , an automated , just - in - time , clinical - grade informatics platform to identify and dynamically track patients on the basis of molecular and clinical criteria . 
median time from sequencing to enrollment was 163 days ( interquartile range , 66 to 357 days ) , and from precise identication to enrollment 87 days ( interquartile range , 37 to 180 days )  . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction genomic data are increasingly used to guide both routine and investigational treatment decisions for patients with cancer . 
simultaneously , clinically validated broad next - generation sequencing platforms that permit the detection of multiple potentially actionable alterations are now accessible at the point of care.1 , 2 these improvements , however , have not been accompanied by commensurate advancements in the systems that are available to help physicians interpret and act on these data . indeed , previous experience with patients with advanced solid tumor who undergo genome proling suggests that only a minority5% to 24% , depending on the breadth of sequencing and practice settingare subsequently enrolled in genome - matched trials.3 - 8 numerous challenges exist in identifying and enrolling patients in appropriate genome - driven clinical trials . clinicians must correctly interpret sequencing data not only at the time of the initial results , but also longitudinally , as our understanding of genomic biomarkers and associated clinical evidence continuously evolves.9 enrolling patients in trials also requires access to , and up - to - date knowledge of , a changing portfolio of studies , each with its own study - specic eligibility criteria and dynamic slot availability . 
finally , all of this information must be readily accessible to the clinician at critical decision points in a patients care . to address these challenges , multiple strategies have emerged to facilitate matching patients to genomedriven clinical trials ( appendix table a1 )  . 
 tao et al context key objective new strategies to facilitate matching patients to genome - driven trials are needed to support physician decision making . precision insight support engine ( precise ) is an automated , just - in - time , clinical - grade informatics platform that identies and dynamically tracks patients on the basis of molecular and clinical criteria . 
to our knowledge , this represents the rst effort to evaluate outcomes of a bioinformatics patienttrial matching platform . knowledge generated precise identied nearly one half ( 43% ) of all enrollment in early - phase , genome - driven studies across a wide variety of tumor types and molecular alterations , with a 5 - month median time from sequencing to enrollment . 
a major area for improving matching efcacy is better integration of nonstructured , clinical eligibility criteria . relevance use of automated bioinformatics platforms represents an important means by which to increase clinical trial accrual and deliver precision oncology care to patients . straightforward of these approaches involves directly annotating molecular sequencing reports at initial sign - out to indicate the clinical signicance of each alteration and list potentially suitable clinical trials . 
multiple initiatives are underway to harmonize the annotation of individual variants and incorporate multitiered levels of evidence for actionability.10 - 12 some commercial laboratories and academic institutions have created on - demand molecular tumor boards that review molecular sequencing reports to make treatment recommendations and manually curate existing clinical trials for alterations of interest.13 all of these approaches have potential limitations . 
similarly , molecular tumor boards are time consuming , difcult to scale , and potentially inuenced by participants knowledge base and anecdotal experience . in response to these limitations and to address the ongoing unmet need of matching patients to clinical trials at our center , we created precision insight support engine ( precise ) , an automated , just - in - time , clinical - grade informatics platform to identify and dynamically track patients on the basis of molecular and clinical criteria . precise was designed to empower clinical investigators to proactively identify and recruit optimal candidates to their genome - driven trials . 
initially , limited proling data were generated via a mass spectrometrybased hotspot assay covering eight genes ( massarray ; sequenom , san diego , ca ) or an amplicon - based next - generation sequencing test covering 48 genes ( truseq amplicon cancer panel ; illumina , san diego , ca ) .14 a customized hybrid capture - based next - generation sequencing assay ( mskimpact ) was later performed per previously published methods.15 msk - impact can identify all classes of genomic alterationssingle - nucleotide variants , indels , copy number alterations , and select structural rearrangementsin up to 468 genes , depending on the assay version . 
these data are used for clinical report sign - out and delivery to the data warehouse that precise uses for patient identication.16 , 17 sequenced patients had cancer types for which proling was considered routine at the time performed or underwent clinical testing under a prospective institutional review boardapproved protocol that was designed to evaluate the utility of proling in these cancer types ( clinicaltrials.gov identier : nct01775072 )  . precise platform the precise platform was available to any principal investigator of an irb - approved therapeutic study that included molecular eligibility criteria . 
 outcomes of a physician support system for genome - driven oncology the functionality of the precise platform evolved during the study period on the basis of user feedback ( fig 1 )  . 
beginning in 2014 , precise was enhanced to offer notications , customized per study , of potentially clinically important events that could prompt a treatment change , such as upcoming appointments or restaging scans . 
for most of the study duration , precise notications were provided directly to the research team , which empowered them to further screen potential patients for appropriateness and notify treating physicians accordingly . 
use of this direct - to - primary oncologist notication function was at the discretion of the research teaall notications to the research team and the primary oncologist were generated as emails and did not directly integrate with the electronic medical record . cohort eligibility , data collection , and statistical analysis all precise cohorts for early - phase studiespilot , phase i , and phase i and iithat included at least one genomic eligibility criterion and that were created after april 16 , 2014 , were included for analysis . 
an internally developed mpath application was used to obtain the date that sequencing data was signed out and entered into the medical record for each patient , as well as the specic qualifying genomic alteration present . the msk institutional review board evaluated and approved a retrospective research protocol to evaluate precise platform outcomes . 
primary outcome measure was to determine what proportion of patients who were enrolled in the evaluated genome - driven studies was facilitated by precise . for the purpose of this analysis , enrollment was considered to be facilitated if precise identied the patient as eligible and generated a notication to either the research team or the primary oncologist before the enrollment date . 
to identify areas for future precise functionality enhancement , reasons for the failure of precise identify eligible patients before study enrollment were also explored through manual record review . in the relevant results study characteristics a total of 41 therapeutic trials used precise for genomic matching during the study period ( table 1 )  . 
the initial iteration ( version 1 ) of precise involved generating cohorts on the basis of complex genetic and clinical criteria dened by the studys principal investigator ( pi ) , which could then be sent to the pi at dened intervals . 
the capability of precise was later enhanced ( version 2 ) to enable pi notications triggered by certain events of interest , such as an upcoming patient appointment or computed tomography scan . 
present day ( version 3 ) precise can also incorporate a patients prior treatment history and allows for direct notication of the patients treating oncologist that a patient may be eligible for a study , often prompting an exchange between the treating oncologist and pi that initiates the patients future enrollment . 
of investigational agents antibody ( nonimmunotherapy ) therapeutic class * small molecule immunotherapy tumor type eligibility multiple breast lung ( nonsmall cell ) lymphoma mesothelioma glioma sarcoma prostate thoracic breast 5 - 10 10 - 15  . 
eight of 41 trials used the direct - to - oncologist notication system . principal investigator characteristics the 41 therapeutic trials were led by 19 unique principal investigators ( pis ) who individually led between one and ve studies ( table 1 )  . 
median time since the completion of terminal subspecialty training for pis was 7 years ( range , 2 to 27 years )  . patient matching during the study period , a total of 755 patients who were treated primarily by 150 unique oncologists were enrolled in 41 trials . 
precise prospectively identied 43% ( 327 of 755 ) of cases before patient enrollment , successfully notifying study investigators and / or the primary oncologist of the potential match ( fig 2 )  . 
reecting eligibility criteria among the trials , breast cancer ( 76 [ 23% ] of 327 ) and lung cancer ( 55 [ 17% ] of 327 ) were the most common tumor types among enrolled patients identied by precise . 
accounting for patients with more than one eligible molecular alteration , erbb2 ( 71 [ 21% ] of 335 ) was the most common genomic alteration , followed by pik3ca ( 47 [ 14% ] of 335 )  . at the individual protocol level , the percent of patients identied by precise before enrollment ranged from 0% to 100% . 
patients in whom the genomic alteration that ultimately led to enrollment did not meet the pre - established precise molecular criteria , as dened by the investigator , accounted for 33% ( 140 of 428 ) of missed cases . 
a lack of internal sequencing at the time of accrual accounted for 30% ( 127 of 428 ) of missed cases , predominantly among patients who enrolled on the basis of genomic proling that was performed outside the institution and was therefore not available for parsing by precise . 
another 23% ( 100 of 428 ) of cases was missed because precise cohort criteria that would have included the patient were amended only after the time of patient enrollment . 
several other technical and clinical reasons accounted for the remaining 14% ( 61 of 428 ) of cases , the majority of which ( 50 of 61 ) consisted of patients who did not meet clinical criteria available for * the total adds up to more than 41 as studies may include more than one agent class . twelve principal investigators had dual afliations with a diseasespecic group and the phase i group . one half ( 22 [ 54% ] of 41 ) of studies were phase i , and 61% ( 25 of 41 ) included multiple tumor types . 
of diseasespecic studies , the most common tumor types included breast cancer ( ve [ 12% ] of 41 ) and nonsmall - cell lung cancer ( four [ 10% ] of 41 )  . 
 ( b ) each column depicts patient enrollments by study principal investigator , with patient enrollment facilitated by precise shaded in blue and patient enrollment not facilitated by precise shaded in red . 
 ( c ) each column represents a unique study , with the absolute number of patients in each category labeled above ( non - precise ) and below ( precise enrollment ) each column . capture by precise , such as presence of triple - negative breast cancer , which was not always readily documented in the medical record . to further understand how physicians and patients use tumor genomic data to guide investigational treatment decisions , we evaluated the timing of enrollment relative to two important milestones : the completion of sequencing and the initial precise identication . 
upon evaluation of the 327 patients who were identied by precise and successfully enrolled in a genome - driven study , there was signicant variability in time intervals between these three events at the individual patient level . 
median time from sequencing to therapeutic enrollment was 163 days ( interquartile range , 66 to 357 days ; range , 5 to 1 , 281 days ) and from precise identication to enrollment 87 days ( interquartile range , 37 to 180 days ; range , 1 to 850 days ; fig 3 )  . 
reasons for delay from sequencing and precise identication to study enrollment included the availability of alternative routine therapy or a lack of need for treatment among patients without evidence of active disease . causes of patient attrition before enrollment to better understand the reasons why patients who were identied by precise did not subsequently enroll in the relevant therapeutic study , a representative cohort involving a multitumor phase i and ii expansion study of a targeted small molecule was selected for manual record review . 
of these 98 patients , 22 were immediately determined to be permanently ineligible or excluded as a result of a static characteristic that rendered the patient ineligible for the trial indenitely . 
these included having a second primary cancer ( n = 6 ) , a nonqualifying malignancy ( n = 6 ) , being deceased but not listed as such in the medical record ( n = 5 ) , and other reasons ( n = 5 )  . 
another 45% ( 10 of 22 ) involved a data element that was sometimes availablesecond primary cancer , prohibited prior therapy , and hiv / aidsfor use but not under all circumstances . 
for example , exclusions on the basis of prior therapy will miss agents administered at other medical centers or some oral anticancer agents , especially if dispensed by third - party pharmacies . after permanent exclusions , 76 potentially eligible patients remained . 
upon manual review , 78% ( 59 of 76 ) of patients did not immediately qualify for treatment at the time of the initial precise identication on the basis of not requiring active therapy ( n = 44 ) or ongoing response to current therapy ( n = 15 )  . 
collectively , 84% ( 59 of 70 ) of these temporary exclusion criteria are not consistently available for use by precise , primarily because the current disease status of the patient is not captured as a structured data element in the medical record . 
 a 2 , 000 1 , 500 1 , 000 500 1 , 000 1 , 500 outcomes of a physician support system for genome - driven oncology 1 , 400 1 , 200 1 , 000 sequencing to enrollment identification to enrollment patient sequencing identified by precise enrollment fig 3 . 
each series of three dots on a single vertical axis represents a single patients course , from initial sequencing ( blue dot ) to identication by precise ( precision insight support engine ; red dot ) to enrollment in the study ( gray dot )  . 
 ( b ) box and whisker plot showing the interval of time from sequencing to enrollment in the study ( left ; median , 163 days ) and from identication by precise to enrollment in the study ( right ; median , 87 days )  . therapies , rapidly deteriorating , or deemed inappropriate because of other issues , such as prior nonadherence . 
reasons for permanent or temporary exclusion from study qualication are depicted in blue ( criteria that is available for use by precise ) , red ( criteria that is sometimes available and could potentially be captured as an extractible structured data element ) , or teal ( criteria that is not yet available for use by precise )  . 
to our knowledge , this report represents the rst effort to evaluate real - world outcomes of an automated , just - in - time , clinicalgrade informatics platform to facilitate patient matching . we also discovered that a signicant time interval often elapses between the initial generation of tumor genomic data and subsequent enrollment in a matched study . specically , among those who ultimately accrue to a matched study , median duration from data generation to enrollment was 5 months , with some outliers enrolling up to 42 months later . 
these data emphasize the importance of supporting physician decision making longitudinally through a patients entire treatment . although these pilot data are encouraging , our analysis also identied areas of ongoing challenge for such matching systems as precise . 
of importance , nearly three quarters of initially identied patients were not immediately eligible on the basis of clinical factors that were not readily available for use by precise , most commonly related to challenges in algorithmically dening patient disease status . 
the result is that precise had a high false - positive rate that may ultimately limit the utility of this system for some indications , particularly for recruiting patients with more prevalent genomic alterations . 
indeed , a previous analysis of overall match rates at our institution that was conducted during roughly the same time period found a match rate of only 11% , despite 37% of patients harboring a potentially actionable alteration.5 taken together , these data demonstrate that even with the use of a sophisticated decision support system , there is an ongoing need for additional improvement in the methodologies to match patients to clinical trials on the basis of tumor genomic and clinical information . 
this requires developing agreed - upon standards , including discrete , structured criteria , for extracting clinical data from the electronic medical record . in the future , leveraging natural language processing and information extraction technologies may also enhance the ability to accurately capture unstructured data . this analysis has some important limitations . 
foremost , we considered any patient about whom precise successfully notied the pi or treating physician of potential eligibility before enrollment as an accrual that was potentially facilitated by the systehowever , we cannot determine exactly how many of these enrollments might have occurred without the use of this systeindeed , our study was retrospective in design and we cannot denitively make conclusions on the incremental value of precise . 
moreover , this analysis represents real - world use of precise by each pi , who were responsible for setting his or her own cohort criteria and using the results as he or she felt best complimented the practice . 
additional evaluation is needed to determine how the utility of this system is affected by recent features , such as full automation of direct - to - treating physician alerts triggered by critical events , like scans that show progression or rising tumor markers . precise is not the only system designed to address the emerging need of matching patients to relevant clinical trials on the basis of the patients genomic prole . 
several other centers have developed strategies by which to achieve this goal that range from on - site or virtual molecular tumor boards to automated matching platforms13 , 18 - 23 ( appendix table a1 )  . 
potential advantages of an automated informatics approach include scalability and the ability to track patients longitudinally and respond to changing molecular and clinical data . in summary , this pilot study of real - world use of precise to guide enrollment in genome - driven studies suggests that this type of real - time decision support system can meaningfully facilitate patient enrollment . 
harding consulting or advisory role : bristol - myers squibb , cytomx therapeutics , eli lilly , eisai research funding : bristol - myers squibb ( inst ) , pzer ( inst ) , eli lilly ( inst ) , novartis ( inst ) , incyte ( inst ) , calithera biosciences ( inst ) , polaris ( inst ) lillian m . 
smyth honoraria : astrazeneca , pzer consulting or advisory role : astrazeneca , genentech research funding : astrazeneca ( inst ) , genentech ( inst ) , puma biotechnology ( inst ) travel , accommodations , expenses : pzer , genentech , puma biotechnology research funding : novartis ( inst ) , genentech ( inst ) , debio pharmaceuticals ( inst ) , adc therapeutics ( inst ) , pzer ( inst ) , novita pharmaceuticals ( inst ) , clovis oncology ( inst ) , eli lilly ( inst ) , zymeworks ( inst ) travel , accommodations , expenses : taiho pharmaceutical , jounce therapeutics , pzer , astrazeneca other relationship : novartis , pzer , taiho pharmaceutical , jounce therapeutics alexander drilon honoraria : medscape , onclive , peervoice , physicians education resources , targeted oncology , more health , research to practice , foundation medicine , peerview consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pzer , blueprint medicines , genentech , helsinn therapeutics , beigene , hengrui therapeutics , exelixis , bayer , tyra biosciences , verastem , takeda , ariad pharmaceuticals , millennium pharmaceuticals , bergenbio , more health , eli lilly research funding : foundation medicine patents , royalties , other intellectual property : wolters kluwer ( royalties for pocket oncology ) other relationship : merck , glaxosmithkline , teva pharmaceuticals , taiho pharmaceutical , pzer , pharmamar , puma biotechnology marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso rfp advisory committee , takeda , bristol - myers squibb , bayer , merck ( i ) research funding : loxo ( inst ) , helsinn therapeutics david b . 
solit stock and other ownership interests : loxo consulting or advisory role : pzer , loxo , illumina , intezyne technologies , vivideon therapeutics travel , accommodations , expenses : merck michael f . 
jhaveri consulting or advisory role : novartis , pzer , spectrum pharmaceuticals , astrazeneca , taiho pharmaceutical , jounce therapeutics , adc therapeutics , synthon , intellisphere , bristol - myers squibb acknowledgment the authors thank alisa pinkhasik for assistance with study data . 
for providing inspiration for this report . references 33 : 2753 - 2762 , 2015 schram am , berger mf , hyman dm : precision oncology : charting a path forward to broader deployment of genomic proling . 
plos med 14 : e1002242 , 2017 cheng ml , berger mf , hyman dm , et al : clinical tumour sequencing for precision oncology : time for a universal strategy . 
nat rev cancer 18 : 527 - 528 , 2018 jordan ej , kim hr , arcila me , et al : prospective comprehensive molecular characterization of lung adenocarcinomas for efcient patient matching to approved and emerging therapies . 
j clin oncol zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
 tao et al stockley tl , oza am , berman hk , et al : molecular proling of advanced solid tumors and patient outcomes with genotype - matched clinical trials : the princess margaret impact / compact trial . 
mantripragada kc , olszewski aj , schumacher a , et al : clinical trial accrual targeting genomic alterations after next - generation sequencing at a non - national cancer institute - designated cancer prograj oncol pract 12 : e396 - e404 , 2016 8 . 
massard c , michiels s , fert e c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . cancer discov 7 : 586 - 595 , 2017 schram am , reales d , galle j , et al : oncologist use and perception of large panel next - generation tumor sequencing . 
taylor ad , micheel cm , anderson ia , et al : the path ( way ) less traveled : a pathway - oriented approach to providing information about precision cancer medicine on my cancer genome . 
mateo j , chakravarty d , dienstmann r , et al : a framework to rank genomic alterations as targets for cancer precision medicine : the esmo scale for clinical actionability of molecular targets ( escat )  . 
ann oncol 29 : 1895 - 1902 , 2018 johnson a , zeng j , bailey am , et al : the right drugs at the right time for the right patient : the md anderson precision oncology decision support platfordrug discov today 20 : 1433 - 1438 , 2015 14 . 
rekhtman n , paik pk , arcila me , et al : clarifying the spectrum of driver oncogene mutations in biomarker - veried squamous carcinoma of lung : lack of egfr / kras and presence of pik3ca / akt1 mutations . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
lindsay j , fitz cdv , zwiesler z , et al : matchminer : an open source computational platform for real - time matching of cancer patients to precision medicine clinical trials using genomic and clinical criteria . 
tao j , eubank mh , pamer e , et al : precise : a clinical - grade automated molecular eligibility screening and just - in - time ( jit ) physician decision support solution for molecularly - selected oncology trials . 
notications are generated from scheduled queries and use an open - source java e - mail package implemented as a database user - dened function to send emails from the sql statement . 
a web application using open - source javascript libraries allows system administrators to capture cohort logic and settings and provides end users the ability to annotate patient status for their study . 
 ( a ) each column depicts patient enrollments by study pi , with pis with the most years in practice on the left and the fewest years in practice on the right . 
it also re - examines some of the conventional wisdom that previously dominated clinical trial design and discusses development and internal validation of a predictive biomarker as a new paradigm for optimizing the intended - use subset for a treatment . 
some previous paradigms for clinical trial design can limit the development of more effective methods on the basis of prospectively planned adaptive methods , but useful new methods have been developed for analysis of genome - wide data and for the design of adaptively enriched studies . 
in many cases , the heterogeneity of populations eligible for clinical trials as traditionally dened makes it unlikely that molecularly targeted treatments will be effective for a majority of the eligible patients . 
with the completion of the human genome project and the initiation of large dna sequencing of human tumors , somatic mutations were discovered that accounted for the invasion and progression of cancers . 
it became evident that the traditional tumor classications on the basis of site and histologic type were inadequate for developing therapeutics . the discovery of somatic mutations led to major changes in the development of oncology drugs . 
the focus of oncology drug development switched to developing inhibitors of mutated protein kinases and blocking the protein products of amplied receptors . the new strategies of drug discovery required new strategies for clinical trial design . 
the traditional assumption that qualitative interactions are unlikely was frequently shown to be wrong . at about the same time , new whole - genome assays such as rna transcript microarrays , copy number microarrays , and methylation arrays were becoming available . 
the resulting statistical methods were based on classication and prediction , which enabled the development of classiers on the basis of high - dimensional assays for predicting prognosis and response to therapy for individual patients.3 , 4 this article will highlight some of the important developments in clinical trial design and classication analysis that have been stimulated by the dramatic changes in oncology drug development . 
 simon context key objective to describe new and innovative methods for discovering and using predictive biomarkers to develop effective treatments in the presence of patient heterogeneity . knowledge generated a method was developed for discovering and validating therapeutically relevant patient subsets using a new paradigm on the basis of predictive classication rather than multiple hypothesis testing . 
with the development of drugs targeted to specic genomic alterations , attention has shifted to phase ii studies with eligibility determined by specic genomic alterations rather than histologic type , the so - called basket clinical trial.5 - 9 large basket trials include multiple drugs , each with a targeted genomic alteration . 
patients have their tumors sequenced , and then they are assigned the drug appropriate to the genomic alteration found in their tumor . basket trials have generally been sized by using standard methods either for inference on the basis of all patients with the genomic alteration histologic type or for separate inference for each histologic type . 
recently , bayesian designs have been developed that attempt to share response information among histology baskets for patients whose tumor contains the same genomic alteration.10 some of these are based on hierarchical models of treatment effects . 
however , cunanan11 has shown that the prior distributions for such designs must be chosen carefully or the false - positive error for some histology baskets may be highly inated . 
if the accumulating information indicates homogeneity of response probabilities , then the baskets are essentially pooled and a small sample size sufces . cunanan12 developed a frequentist design on the basis of two - stage sampling . 
otherwise , sampling and inference are conducted independently for the baskets . the platform design is for settings with multiple treatments and multiple candidate biomarker strata.13 the design is based on the assumption that the candidate biomarkers are the same for each drug , which somewhat limits the realm of applications . 
most platform designs are bayesian designs and the term promising is interpreted to mean that the posterior probability of a positive phase iii trial is at least 80% . in a platform design , a patient is initially randomly assigned with equal probability to receive any of the drugs . 
the objective is to nd candidates for phase iii trials with a smaller total sample size than would be required for conducting a separate simon two - stage optimal trial in each of the strata.14 the bayesian models used are generally based on hierarchical modeling.13 , 15 freidlin et al16 developed a simpler phase ii trial design for a single drug with a single binary biomarker . 
 statistical methods for biomarker - driven clinical trials simon and maitournam17 , 18 studied the number of patients needed to screen and randomize for the enrichment design compared with a standard design , in which the assay is not performed . 
they found that the enrichment design generally requires many fewer randomly assigned patients . they showed that the ratio of number of required randomly assigned patients was approximately ( cid : 1 ) nenrichment nstandard ( cid : 1 ) te + + ( 1 ) te ( cid : 3 ) 2 where te + and te are the treatment effects in mutationpositive and mutation - negative patients , respectively , and denotes the proportion of mutation - positive patients . 
this formula indicates that the randomization ratio equals the reciprocal of the square of the treatment effects in the two trial designs . if the treatment effect in mutation - negative patients is zero , then the randomization ratio equals 2 . 
if the treatment effect in the mutation - negative patients equals half that in mutationpositive patients , then the randomization ratio becomes { + ( 1 ) / 2 } 2 , so if = 0.5 , then the randomization ratio equals 9 : 16 , and the enrichment design requires slightly more than one half the number of patients as the standard design . adaptive determination of the intended - use population the efciency of the enrichment design highlights the critical relationship between the required size of a phase iii clinical trial and the target treatment effect . 
simon et al19 developed a focused approach for using such archived tissues called the prospective - retrospective study design , which was used for establishing that patients with advanced colorectal cancer do not benet from anti - egfr antibodies if their tumors contain a mutation in the kras gene.20 this approach was also used in a structured manner in the development of the oncotype dx recurrence score as a prognostic and predictive signature for patients with stage i and stage ii breast cancer.21 in addition to using archived samples from a failed randomized controlled trial ( rct ) , adaptive methods have been developed for prospective design of an rct in a statistically rigorous way to adaptively identify the subset of patients who benet from the test treatment . 
some of these adaptive methods will be discussed , but their use has required regulators and clinical trialists to accept that the intended - use population need not be the full eligible population . by prospectively allocating some of the type i error rate to a planned subset analysis , 22 we do not need to use the convention that subset analysis should be performed only if the all - comers analysis is signicant or if there is a statistically signicant interaction . 
statisticians and clinical investigators have sometimes been slow to shed some of the conventional wisdom of the previous paradigm , such as the requirement that the intended - use population must be the eligible population . adaptive enrichment single binary candidate biomarker . 
the most common type of adaptive enrichment in phase iii trials involves whether to use a binary candidate biomarker to restrict eligibility . initially patients are characterized with regard to the biomarker and then randomly assigned to the test treatment or control , but the biomarker is not used to restrict eligibility . 
at some point during the trial an interim analysis is performed and one of three decisions is made : ( 1 ) the entire trial is closed for futility , ( 2 ) the trial continues accruing without any restriction on eligibility until its originally planned sample size is reached , or ( 3 ) accrual is continued only for biomarker - positive patients . 
in the third case , the total target accrual may be increased to adequately power the nal analysis for biomarker - positive patients . several authors have proposed designs for the binary biomarker case described previously.23 - 32 they contain multiplicity adjustments to account for the fact that inferences are being made for the treatment effect overall and for biomarker - positive patients . 
in many cases , there is a quantitative or semiquantitative biomarker that is thought to be predictive of which patients are most likely to benet . often , previous studies have not reliably established the relationship between biomarker value and likelihood of benet , and there is no adequately determined cut point for positivity . 
a recent example is the programmed deathligand 1 ( pd - l1 ) level of expression on nonsmall - cell lung tumors as a predictor of response to t - cell checkpoint therapy . because of regulators requirements that sponsors demonstrate statistically signicant effectiveness of the treatment of an intended - use population , most sponsors want to have the intended - use population dened at the outset . this may require using a cut point selected on the basis of inadequate phase ii trials . 
 simon of the relationship between biomarker level and treatment effectiveness . biomarkers , not for settings in which whole - genome data are used for classier development . there are only a few cases in which investigators use an adaptive design to determine an optimal cut point on the basis of interim data , perhaps because they are unaware of the new statistical designs that may achieve this in a statistically valid manner . jiang et al34 showed how one could test the null hypothesis of no treatment effect using a minimal p value statistic for which a p value for treatment effect is computed for the cases above each of the candidate cut points . 
their proposed analysis is performed at the end of the trial using the full data set and is based on the null distribution of the min - p - value statistic . 
this approach is easy to implement because it does not require any changes during the trial . the intended - use population is adaptively determined at the end of the trial . is adaptive in that simon and simon35 illustrated the use of their adaptive enrichment approach for modifying eligibility during the trial on the basis of an interim analysis of the relationship of biomarker value to treatment effect . 
the signicance test preserves the type i error , regardless of the strategy used for modifying eligibility . although the method is frequentist , they advocate using a bayesian model for selecting features and building the classier at interim analyses.33 the bayesian model can also be used for selecting an intended - use population . one of the questions about using adaptive enrichment is how to estimate the treatment effect in the adaptively selected intended - use population in an unbiased manner . simon and simon36 described how to use bootstrap resampling in an unbiased manner to estimate treatment effects for the intended - use population using data from periods that also determined how to modify eligibility . 
one approach involves developing separate prognostic scores for the active treatment group ( eg , h ( x ; a ) for the log hazard ratio relative to baseline hazard for a patient with covariate vector x receiving the active treatment ) and the control group ( h ( x ; c ) )  . 
that is , if the hazard of a failure event on treatment a is less than the hazard of that event on the control by a tolerance of at least c for a patient with baseline covariate vector x , then the predictive biomarker is considered to have value 1 , and otherwise to have value 0 . 
instead of using proportional hazards modeling as suggested here , one could use other methods such as random forest modeling37 or any other method of prognostic modeling . a major feature of the new paradigm for subset analysis introduced by the adaptive signature design ( asd ) is that nding an appropriate intent - to - treat subpopulation should be treated as a classication problem , not as a hypothesistesting problefinding a subset with a large apparent treatment effect is of little value because the resubstitution estimate of treatment effect is so often optimistically biased . the asd and cross - validated asd ( cv - asd ) provide unbiased estimates and tests of such treatment effects . simon38 described sensitivity , specicity , positive predictive value ( ppv ) , and negative predictive value ( npv ) for predictive classiers with survival time outcome . 
when the survival time for active treatment versus control has proportional hazards for classier - positive and classier - negative patients , then the ppv can be written38 ppv ( cid : 1 ) 1 + + where + denotes the hazard ratio of control versus active treatment of classier - positive patients . 
us food and drug administration ( fda ) guidance on the use of enrichment strategies describes the asd in a positive manner.42 practical experience in designing a clinical trial using the asd is described by sher et al , 43 simon , 44 and mi.45 where + denotes the prevalence of classier - positive patients . 
the asd and cv - asd to be described in a later section were originally described in terms of a specic kind of classier for gene expression data , but the concept is quite general and will be described here in its generality . 
it is not limited to high - dimension genomic data or signatures of gene expression measurements ; is best used with a moderate number of candidate predictive biomarkers . in fact , at the nal analysis , the patients randomly assigned in the clinical trial are randomly partitioned into a training set and a validation set . 
a predictive classier is developed by using only training set data . with the asd , however , one is permitted to develop only a single predictive classier , and it must be completely specied before the validation set data are used in any way . finally , the patients in the validation set are classied as likely to benet from the active treatment ( f ( x ) = 1 ) or not ( f ( x ) = 0 )  . 
the set of covariate vectors for which f ( x ) = 1 is considered the intended - use subset s : s = { x : f ( x ) = 1 }  . although the asd provides a new paradigm for subset analysis of rcts , its statistical power is limited because of the sample splitting . 
freidlin et al46 introduced an improved method called the cv - asd with improved power establishing the signicance of the treatment effect in the adaptively determined intended - use subset . 
we denote the resulting predictive classier as c ( a , d ) where d denotes the complete data set . the resubstitution estimator of treatment effect is denoted ( c ( a , d ) , d ) where the operator computes the empirical treatment effect on the subset of d for which classier c is positive . 
this new training starts from scratch ; that is , it does not use the feature selection steps of development of the full sample classier c . let ck ( a , dk ) denote the classier developed on dk . 
i is the prevalidation classication of patient i . having developed a single predictive classier using training data , the next step is to evaluate the treatment effect for patients in the validation set with covariate vectors in s . 
outcomes of those who received active treatment are compared with outcomes of those who received the control . because the validation set was not used to develop the classier , this comparison of outcomes is unbiased . after completing all k - folds of the cross - validation , all of the cases have been classied once . 
these { i } are called prevalidated indicators of the intended - use subset.47 let iu = { i : i = 1 } , the intended - use subset on the basis of the prevalidated predictive classications . 
 simon empirical treatment effect in iu , and take that as an approximation for the treatment effect in using the full sample classier c ( a , d ) with new cases in the future . 
simulation studies have shown that this estimator is much better than the resubstitution estimator but somewhat conservative.46 a statistical signicance test for treatment effect among future patients classied positive using c ( a , d ) is approximated by computing the permutation distribution of ( iu )  . for each permutation of the treatment labels , the crossvalidation procedure is repeated giving a new iu , say iu ( cid : 4 ) , and a new value of ( iu )  . 
with many permutations of the treatment labels , one can approximate the null distribution . the null hypothesis here is that there is no subset for which there is a positive treatment effect . 
zhang et al48 describe an alternative approach to de - biasing the resubstitution estimator ( c ( a , d ) , d ) using bootstrap sampling instead of using prevalidated classication . other phase iii designs zhao et al49 describe a method for using the results of a previous clinical trial of a treatment and control to select a subset of patients for a new rct . 
for higher - dimensional data , the authors recommend sample splitting or cross - validation to separate the development of predictive scores from the evaluation of the outcome difference in the selected patients . 
the authors assume that feature selection does not use the clinical trial data because a partial cross - validation approach in which feature selection is not repeated for each resampling is described and can be highly biased when feature selection uses the data.50 foster et al37 describe a method very similar to the cv - asd for binary outcome data in which the random forest method is used for developing prognostic prediction function in the active treatment and control groups . 
they also investigate bootstrap resampling to estimate the treatment effect in the selected subset . cv - asds are quite general with regard to the type of models used for predicting difference in expected outcome between treatment groups as a function of the covariate vector . 
these treatment effect estimates may be biased if the assumed parametric model is misspecied , however . outcome weighted learning is an approach to developing approximately optimum individualized treatment rules that are robust to model misspecication.51 , 52 sequentially adaptive interventions are multistage treatto tailor a sequence of ment strategies that attempt treatment interventions to the characteristics of individual patients and their responses to previous treatments . 
such a score can be based on the difference between a prognostic risk function ft ( x ) trained on the treatment group and a prognostic risk function fc ( x ) trained on the control group , where x denotes the vector of measured covariates . 
using the k - fold cross - validation approach of the cv - asd , these functions can be developed on dk training sets and used to compute prevalidated predictive scores ft ( xi ; dk ) fc ( xi ; dk ) for the cases in the withheld sets dk . 
these prevalidated predictive scores si being quantiles are thus in the range ( 0 , 1 )  . matsui et al55 suggest that these prevalidated scores be used as the independent variable in a proportional hazards model containing a main effect of the treatment and an interaction between treatment and prevalidated predictive score quantile . 
for any test statistic involving the estimated treatment effect scores , the null hypothesis of no treatment effect can be performed by permuting the treatment labels and repeating the cross - validation procedure . 
predictions for future patients require rst computing the predictive index quantile score for the new patient using quantiles of the full data set and then plugging that value into the tted proportional hazards model . cai et al56 described a two - stage procedure for estimating a predictive score . 
for high dimensional their approach is probably best used with covariates , prevalidated predictive scores . discussion the development of personalized oncology has been a consequence of the discovery of somatic driver mutations in tumors . 
development of drugs and companion diagnostics for inhibiting driver mutations has provided many two decades . therapeutic successes during the past complex statistical methods have not been necessary for developing predictive biomarkers in these cases because the presence of is the biomarker . the mutation itself however , most somatic mutations are not driver mutations , and identication of predictive biomarkers in those cases can be much more difcult . 
consequently , the fda developed a regulatory pathway in which the diagnostic was not labeled as distinguishing patients who are likely to benet from the drug from those who are not , but rather for identifying patients who have a tumor containing the mutation that makes them eligible for the approved drug . 
during the past two decades , numerous drugs and companion diagnostics for patients with cancer have been approved on the basis of the enrichment design . the question of whether to restrict eligibility to a phase iii trial on the basis of a binary biomarker or on the basis of the value of a quantitative biomarker frequently arises in the design of pivotal trials . 
having larger phase ii trials would provide better evidence for designing phase iii trials , but often the phase iii design decisions are made on the basis of insufcient phase ii data . 
the adaptive designs described in which eligibility is not initially restricted but may subsequently be restricted to biomarker - positive patients on the basis of a prespecied interim analysis are widely applicable . 
more general adaptive enrichment designs with multiple candidate biomarkers can be effective if markers are sufciently powerful their effects on outcome can be discovered at interim analyses . that the asd and cv - asd are easy to use because they do not require any eligibility changes during the course of the trial . they are adaptive in the sense that the intended - use population is adaptively determined by the trial data . however , because they do not adapt eligibility , the opportunity for power gains is limited . 
the cv - asd has much better power and is appropriate for settings in which strong candidate biomarkers are not known at the start of the trial . analyzing phase iii trials by using a continuous score biomarker that reects relative treatment effectiveness can provide medically useful information without the arbitrariness of specifying a cut point . 
it is important , however , to internally validate the calibration of the scoring function by using resampling methods as described here . trials for nding optimal dynamic regimes for clinical multistage decision making have not yet found much application in oncology but have been used effectively in other areas . some of the conventional wisdom that has guided the design and analysis of phase iii trials is undergoing reevaluation . 
for example , the paradigm of broad eligibility and the use of subset analysis on the basis of multiple hypothesis testing require re - evaluation . is not always for molecularly targeted treatments , reasonable to expect a signicant treatment effect for all eligible patients dened by using conventional histology and stage criteria . 
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new york , ny , chapman and hall / crc , 2015 antonijevic z , beckman ra ( eds ) : platform trial designs in drug development : umbrella trials and basket trials . 
new york , ny , chapman and hall / crc , 2018 berry sm , broglio kr , groshen s , et al : bayesian hierarchical modeling of patient subpopulations : efcient designs of phase ii oncology clinical trials . 
clin trials 10 : 720 - 734 , 2013 simon rm : primary site independent clinical trials in oncology , in antonijevic z , beckman ra : platform trial designs in drug development : umbrella trials and basket trials . 
bokemeyer c , kohne c , rougier p , et al : cetuximab with chemotherapy ( ct ) as rst - line treatment for metastatic colorectal cancer ( mcrc ) : analysis of the crystal and opus studies according to kras and braf mutation status . 
paik s , tang g , shak s , et al : gene expression and benet of chemotherapy in women with node - negative , estrogen receptor - positive breast cancer . 
biom j 51 : 358 - 374 , 2009 jenniso c , turnbull bw : conrmatory seamless phase ii / iii clinical trials with hypotheses selection at interim : opportunities and limitations . 
stat med 32 : 2695 - 2714 , 2013 jenkins m , stone a , jennison c : an adaptive seamless phase ii / iii design for oncology trials with subpopulation selection using correlated survival endpoints . pharm stat 10 : 347 - 356 , 2011 30 . 
biostatistics 19 : 27 - 41 , 2018 jiang w , freidlin b , simon r : biomarker - adaptive threshold design : a procedure for evaluating treatment with possible biomarker - dened subset effect . 
bai x , tsiatis aa , lu w , et al : optimal treatment regimes for survival endpoints using a locally - efcient doubly - robust estimator from a classication perspective . 2003 lifetime data anal 23 : 585 - 604 , 2017 52 . 
 o use of low - frequency driver mutations detected by cell - free circulating tumor dna to guide targeted therapy in nonsmall - cell lung cancer : a multicenter case series purpose to evaluate the clinical outcome of patients with nonsmall - cell lung cancer treated by targeting low variant allelic frequency ( vaf ) driver mutations identified through cell - free dna ( cfdna ) next - generation sequencing ( ngs )  . 
detection of driver mutations in cancer is critically important in the age of targeted therapy , where both tumor - based as well as cfdna sequencing methods have been used for therapeutic decision making . 
we hypothesized that vaf should not be predictive of response and that low vaf alterations detected by cfdna ngs can respond to targeted therapy . patients and methods a multicenter retrospective case review was performed to identify patients with nonsmall - cell lung cancer who received targeted molecular therapy on the basis of findings of low vaf alterations in cfdna ngs . 
mutations at low vaf were defined as < 0.2% mutated cfdna molecules in a background of wild - type cfdna . results one hundred seventy - two patients underwent cfdna ngs testing . 
2018 by american society of clinical oncology introduction advances in the sensitivity and accuracy of plasma cell - free dna ( cfdna ) sequencing now allow for somatic genomic tumor alterations to be detected by cfdna next - generation sequencing ( ngs ) at the level of 0.02% variant allelic frequency ( vaf ) .1 this raises the question of whether targetable driver mutations that are detected at low frequencies , defined herein as < 0.2% vaf , retain importance even in the setting of other genomic alterations at higher vaf . 
 specific cases spanning each of the three major types of mutationssingle nucleotide variants ( snvs ) , insertion - deletion mutations ( indels ) , and fusionsare discussed . approximately 20% to 30% of tumors from patients with lung adenocarcinoma have targetable miriam t . 
 oncogenic driver mutations in alk , braf , egfr , erbb2 ( her2 ) , met , ret , and ros1.2 , 3 lung cancer patients with nonsmall - cell ( nsclc ) treated with targeted molecular therapies against these oncogenic driver mutations have been found to have prolonged survival compared4 , 5 with patients treated with standard chemotherapy , with improved treatment - related toxicity and quality of life.6 - 8 given these results , the national comprehensive cancer network now recommends that patients with metastatic nonsquamous nsclc have broad molecular profiling of their tumor performed , with cfdna as a secondary option if repeat tissue biopsy is not feasible.9 as tumor cells become necrotic and undergo apoptosis , they release circulating fragments of dna . 
with advances in ngs , it is now possible to detect cfdna from blood samples with significant accuracy and precision.10 , 11 three major approaches exist for analyzing cfdna in peripheral blood . 
the first uses probes to capture hotspots , or regions commonly mutated in selected genes ; an example of this approach is digital droplet polymerase chain reaction.12 the second uses ngs but requires a tumor tissue sample to identify specific mutations , which are used as a reference to select probes to specific regions in cfdna.13 , 14 the third method uses ngs but targets a gene panel of interest using complete exon sequencing in a blinded approach.15 , 16 mutations are quantified and represented as a vaf calculated as the total number of molecules with a given mutation divided by the total number of mutant plus wild - type molecules . detection of cfdna allows for tumor monitoring at disease progression via serial peripheral blood samples and , in the future , may eliminate the need for tumor biopsies or repetitive biopsies in patients with advanced cancer when the initial biopsy is inadequate , unobtainable for genomic testing , or uninformative , or when the patients cancer has progressed despite treatment.17 - 19 the quantity of cfdna has been shown to correlate with tumor staging and prognosis.17 , 20 limitations of cfdna include testing in patients with low disease burden and in patients with bone or brain metastasis , who may have quantities of cfdna below the limit of detection ( lod ) for currently available assays . 
although these false - negative results limit the application of cfdna ngs to a rule - in test , more than a dozen nsclc studies have shown that targetable genomic alterations detected in plasma predict response similarly to those detected in tissue.21 - 24 however , it is unclear whether variants at low allele fractions are as responsive to targeted therapy as those at high allele fractions . 
 samples were sent to a clinical laboratory improvement amendments ( clia ) certified , college of american pathologistsaccredited , new york state department of healthapproved clinical laboratory ( guardant health , redwood city , ca ) for clinical cfdna ngs testing ( guardant360 ) from one of three institutions ( university of california , san diego [ ucsd ] , duke university , or northwestern university )  . 
for this project , a vaf 0.2% was defined as low vaf because this is the 25th percentile vaf detected on guardant360 ( the median or 50th percentile is 0.39% ) in > 5 , 000 patient samples.1 medical records were reviewed in accordance with the respective institutional review board guidelines of ucsd , duke university , and northwestern university . 
response evaluation criteria in solid tumors ( recist v1.1 ) were used to assess response to treatment . tissue ngs individuals had tumor tissue from primary or metastatic sites sent for targeted tumor tissue ngs before or at approximately the same time as their cfdna analysis . 
tissue - based ngs was done at either ucsd , duke , foundation medicine ( foundation one ; cambridge , ma ) , or caris ( phoenix , az )  . 
the lower lod for this assay was 5% , meaning that a mutant allele can be detected in a 95% wild - type allele background ( or 10% neoplastic cell content )  . 
coverage of at least 250 was required to detect a mutation at the 5% lod . egfr sequencing , ros1 and alk fluorescent in situ hybridization testing neogenomics laboratories ( fort meyers , fl ) performed egfr sequencing , which included bidirectional sequencing of exons 18 to 21 of the egfr gene for detection of egfr - activating mutations and tyrosine kinase inhibitor resistance mutations ( including t790m )  . 
tumor enrichment was performed before extraction ( detailed information can be found on the neogenomics web site ) .29 ros1 and eml4 - alk fluorescent in situ hybridization ( fish ) testing was performed by response genetics ( los angeles , ca ) , and a positive test on fish was considered to be > 15% probe binding . plasma cell - free circulating dna analysis the cfdna ngs analysis was performed at guardant health ( guardant360 )  . 
the exons of up to 73 cancer genes were captured using biotinylated custom bait oligonucleotides ( agilent , la jolla , ca ) , resulting in a 148 , 000 base pair ( 78 kb ) capture footprint . 
these algorithms quantify the absolute number of unique dna fragments at a given nucleotide position , thereby enabling circulating tumor dna to be quantitatively measured as a fraction of total cfdna . 
because patients were not enrolled in a prospective clinical trial , assessments were not standardized across the cohort . results between september 2015 and september 2017 , six clinicians from the three institutions ( ucsd , duke university , and northwestern university ) identified 192 orders from 172 unique patients with a diagnosis of nsclc and in whom cfdna was detected . 
although pfs was roughly as expected in this small cohort , the median os of < 15 months is somewhat shorter than expected for egfrand alk positive patients , especially because the median pfs of patients receiving targeted therapies was 12 months . 
this finding of lower than expected os may be because of sample size , or it is possible that patients with driver mutations present at low vaf have a worse prognosis compared with patients with driver mutations at more standard frequencies . 
there may also be other negative prognostic factors associated with low vaf that are not yet known . met exon 14 skipping mutations represent a clinically unique molecular subtype of nsclc and are found in approximately 3% of all nsclc cases.32 met exon 14 mutations can be detected via tumor ngs or with cfdna ngs , which represents a novel detection method because currently , no other alternative detection modalities ( eg , immunohistochemistry or fish ) exist for this mutation . 
thus the met exon 14 skipping mutation can lead to increased activation of c - met , resulting in oncogenic driver mutation potential.33 fusions and midsize indels ( > 50 bp ; eg , met exon 14 skipping variants ) are especially challenging to detect in cfdna . 
as illustrated by case 8 , detection of met exon 14 skipping mutations can significantly affect the use of existing agents ( eg , crizotinib ) or novel agents ( eg , glesatinib ) for treatment . it is now known that intratumoral heterogeneity is associated with an increased risk of recurrence or death . 
 possible , all targetable driver mutations , both early in treatment and as the tumor evolves.34 using interval liquid biopsies on the basis of radiographic progression of an otherwise nonbiopsiable lesion can provide early detection of drug resistance and thus lead to early treatment intervention . 
this was illustrated by patient 5 , who declined invasive tumor biopsy and underwent repeat cfdna testing at the time of radiologic progression , which was 16 months after his initial cfdna testing . 
 a modest - sized prospective clinical trial by kim et al21 used cfdna - guided matched therapy when tissue was insufficient or unobtainable for ngs in patients with metastatic gastric cancer , nsclc , or melanoma . 
additional prospective studies are needed to further examine the value of early detection of resistance mechanisms before clinical evidence of progression and to determine if early detection and intervention truly influences os and pfs . in this series , patients were selected on the basis of the presence of low vaf driver mutations detected in cfdna . 
it has been reported that a subgroup of patients does not release tumor cfdna into their circulation , whereas other patients convert from having circulating tumor cfdna to noncirculating tumor cfdna after treatment , for reasons that include low tumor burden , slow - growing or inactive tumor growth , or therapeutic response.35 if safe , a tissue biopsy should be performed in patients who initially had detectable mutations on cfdna who no longer have detectable mutations but have clear progression of disease . 
there are several ongoing large prospective trials , including the azd9291 first time in patients ascending dose study ( aura ) , which serially compared cfdna versus tumor ngs over time in patients with egfr t790m mutations who were receiving osimertinib , which may help to address these clinical scenarios.16 one patient ( patient 10 ) was noted to have both eml4 - alk and ros1 mutations detected on tissue fish testing at the time of diagnosis . 
 difficulty detecting the mutation because recurrence of disease was located in the brain or the possibility that ros1 was present below the lod for the cfdna assay after 1 year of treatment . 
the patient was transitioned to hospice shortly after cfdna testing was done , and no additional testing was performed to confirm the presence of ros1 rearrangement . to our knowledge , this is the first case series examining treatment outcomes for patients with nsclc with low vaf driver mutations detected by cfdna . 
most patients had other passenger mutations that were present at a higher proportion compared with the low - frequency driver mutation , and the therapeutic significance of relatively low vaf driver mutations has not been previously reported . 
patel manuscript writing : all authors final approval of manuscript : all authors in the sensitivity and specificity of liquid biopsy , the ability to detect and confer clinical benefit to patients on the basis of these results will continue to improve with technological advances in cfdna . 
from this small case series , it seems that even at low vaf , targetable driver mutations retain clinical importance , even in the setting of other genomic alterations at higher vaf . 
mohindra consulting or advisory role : astrazeneca , genentech travel , accommodations , expenses : astrazeneca stock and other ownership interests : pfizer ( i ) lindsey shantzer no relationship to disclose ingrid l . 
patel consulting or advisory role : ariad , abbvie , astrazeneca jeffrey clarke consulting or advisory role : inivata , premier speakers bureau : guardant health , merck stock and other ownership interests : guardant health , biolase research funding : guardant health research funding : medpacto , genentech , bristol - myers squibb , adaptimmune , spectrum pharmaceuticals , abbvie , moderna therapeutics james christensen employment : mirati therapeutics stock and other ownership interests : mirati therapeutics , bluebird bio patents , royalties , other intellectual property : multiple patents in last 2 years while employed at mirati therapeutics covering discovery of kras , lsd1 , and ezh2 inhibitors . 
patel consulting or advisory role : eli lilly , novartis , bristolmyers squibb , astrazeneca / medimmune speakers bureau : merck , boehringer ingelheim research funding : bristol - myers squibb ( inst ) , eli lilly ( inst ) , incyte ( inst ) , medimmune ( inst ) , pfizer ( inst ) , genentech ( inst ) , xcovery ( inst ) affiliations miriam t . 
patel , university of chicago school of medicine , chicago , il ; lindsey shantzer and jeffrey clarke , duke university medical center , durham , nc ; ingrid l . 
lanman , guardant health , redwood city ; and james christensen , mirati therapeutics , san diego , ca . references 77 : 5705 , 2017 ( suppl 13 : abstr ) 1 . 
paik pk , varghese am , sima cs , et al : response to erlotinib in patients with egfr mutant advanced non - small cell lung cancers with a squamous or squamous - like component . 
aisner dl , sholl lm , berry ld , et al : the impact of smoking and tp53 mutations in lung adenocarcinoma patients with targetable mutationsthe lung cancer mutation consortium ( lcmc2 )  . 
zhou c , wu yl , chen g , et al : erlotinib versus chemotherapy as first - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
sequist lv , yang jc , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
oxnard gr , paweletz cp , kuang y , et al : noninvasive detection of response and resistance in egfr - mutant lung cancer using quantitative next - generation genotyping of cell - free plasma dna . 
valle a , audigier - valette c , herbreteau g , et al : rapid clearance of circulating tumor dna during treatment with azd9291 of a lung cancer patient presenting the resistance egfr t790m mutation . 
kim st , banks kc , lee s - h , et al : prospective feasibility study for using cell - free circulating tumor dnaguided therapy in refractory metastatic solid cancers : an interim analysis . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
rozenblum ab , ilouze m , dudnik e , et al : clinical impact of hybrid capture - based next - generation sequencing on changes in treatment decisions in lung cancer . 
camidge dr , bang yj , kwak el , et al : activity and safety of crizotinib in patients with alk - positive non - small - cell lung cancer : updated results from a phase 1 study . 
awad mm , oxnard gr , jackman dm , et al : met exon 14 mutations in non - small - cell lung cancer are associated with advanced age and stage - dependent met genomic amplification and c - met overexpression . 
peschard p , fournier tm , lamorte l , et al : mutation of the c - cbl tkb domain binding site on the met receptor tyrosine kinase converts it into a transforming protemol cell 8 : 995 - 1004 , 2001 34 . 
lin c - c , shih jy , yu cj , et al : outcomes in patients with non - small - cell lung cancer and acquired thr790met mutation treated with osimertinib : a genomic study . 
 c clinical activity of olaparib in urothelial bladder cancer with dna damage response gene mutations introduction metastatic urothelial cancer has limited treatment options , especially when refractory to chemotherapy and immunotherapy . 
however , therapeutically targeting certain molecular alterations in the fgfr and erbb gene families has recently shown promise.1 - 5 comprehensive genomic sequencing efforts have also uncovered the presence of dna damage response ( ddr ) gene alterations , including ercc2 , brca1 , brca2 , and atm in up to 25% of patients with urothelial carcinoma.6 indeed , these alterations have been associated with response to platinum - based chemotherapy , as well as antiprogrammed death - 1 immunotherapy.7 - 11 inhibiting poly ( adp - ribose ) polymerase ( parp ) prevents repair of single strand dna breaks . 
thus , in the presence of homologous recombination gene mutations , parp inhibition leads to the accumulation of excessive dna damage , which becomes lethal to tumor cells.12 , 13 olaparib is a parp inhibitor with established efficacy in ovarian and breast cancers , and with emerging data in prostate cancer.14 - 16 however , there are no reported data on the clinical activity of this molecularly targeted therapy in urothelial bladder cancer . 
in this series , we present two patients with urothelial cancer with ddr mutations who both responded to therapy with olaparib . patient 1 in june 2013 , a 67 - year - old man presented with urinary obstructive symptoms , and a computed tomography ( ct ) scan demonstrated a lobular , asymmetric prostate gland . 
 his pathologic staging was pt4n2 , and from september to november of 2013 , he received adjuvant chemotherapy with gemcitabine and cisplatin , completing four cycles . the patient had no evidence of disease until june 2015 , when he was found to have a 1.1 - cm , left lower lobe lung nodule with prominent periaortic nodes , which were hypermetabolic on the basis of positron emission tomographyct scanning , consistent with metastatic disease . 
foundationone ( foundation medicine , cambridge , ma ) testing was performed on his primary tumor obtained from the prostatic urethral biopsy , which showed the tumor was microsatellite stable and had a low tumor mutational burden of four mutations per megabase . 
 one of these nodes was biopsied , and the tumor was sequenced using oncoplus , the university of chicago clinical laboratory improvement amendmentscertified next - generation sequencing platform.18 the brca1 n1018fs * 8 mutation was again detected . 
the chek2 mutation was indeed seen on the foundationone test from the original biopsy ; however , at that time , it was listed as a variant of unknown significance . 
this alteration has now been established as a germline founder mutation.19 by oncoplus , this new specimen was found to be microsatellite stable and had an intermediate tumor mutational burden of 12 mutations per megabase . 
he was found to have progression patient 2 in december 2013 , a 67 - year - old man underwent a cystoscopy for painless hematuria and was found to have a large friable area in the left bladder wall . 
the patient underwent chemotherapy with six cycles of gemcitabine and cisplatin for stage iv disease , with a complete response on the basis of ct scan , bone scan , and cystoscopy . 
he completed a course of radiotherapy ( 55 gy with 2.2 gy / fraction ) with concurrent capecitabine ( 825 mg / m2 twice per day ) in april 2017 for definitive local management . in september 2017 , a ct scan showed new hepatic lesions that were consistent with metastasis ( fig 1 )  . 
 next - generation sequencing was performed on the turbt specimen from january 2017 using oncoplus , which again identified a brca2 mutation ( c.7436 - 294_7567del ; table 1 )  . 
the mutyh g396d mutation ( previously reported as g382d ) found on his tumor testing was confirmed to be germline in orig the patient began receiving gemcitabine and cisplatin , and achieved another significant partial response after three cycles . 
he required a dose reduction to 300 mg twice per day because of thrombocytopenia , but continues receiving treatment as of september 2018 . discussion the parp enzyme is involved in base excision repair and is pivotal in repairing dna double strand breaks . 
mutation in brca1 / 2 predisposes cells to the effects of parp inhibition , which causes chromosomal instability , cell cycle arrest , and subsequent apoptosis.12 in cells with wild - type brca1 / 2 , dna repair by these proteins preserves the integrity of the dna . 
this functional buffering allows the cell to survive a variety of dna insults , but brca1 / 2 mutation leads to a loss of this compensation and renders the cell vulnerable to parp inhibition 's accumulation of dna defects , eventually leading to cell demise in the form of synthetic lethality.20 this synthetic lethality effect has formed the basis for clinical trials that led to approval of parp inhibitors in brca1 / 2 mutated ovarian and breast cancer.14 , 15 parp inhibitors have also been shown to have significant activity in patients with metastatic prostate cancer who harbor germline or somatic mutations in brca1 / 2.16 in bladder cancer , mutations in ercc2 , atm , and mmr genes are the most commonly mutated table 2 . 
 ddr and repair genes , but brca1 / 2 mutations are also found in up to 20% of patients ( fig 2 ) .21 , 22 here , we present the case reports of two patients with urothelial cancer with brca mutations who had clinical responses to parp inhibition with olaparib . 
these patients support the rationale for several recently initiated clinical trials investigating parp inhibitors in urothelial bladder cancer with ddr gene mutations ( table 2 )  . the first patient had a response lasting longer than a year , whereas the second patient has had an ongoing response lasting longer than 6 months . 
secondary resistance to parp inhibition can involve restoration of brca1 / 2 function , 53bp1 loss , or mdr1 upregulation.23 the rb1 loss observed in patient 1s tumor was not detected in the postolaparib biopsy . 
thus , the mechanism of acquired resistance in this patient may have been avoidance of synthetic lethality via rb1 reactivation , resulting in restoration of cell cycle arrest in the setting of dna damage.24 interestingly , neither of these patients responded to antiprogrammed death - 1 immunotherapy , which is unexpected , given data supporting a higher rate of clinical benefit with immunotherapy for patients with ddr alterations.11 this finding might be explained by the low tumor mutational burden observed in each patients initial tumor specimen ( four mutations per megabase ) and the finding that both tumors were microsatellite stable . 
sweis honoraria : bristol - myers squibb , exelixis , medscape brian heiss no relationship to disclose jeremy segal honoraria : bristol - myers squibb , abbvie research funding : abbvie lauren ritterhouse honoraria : bristol - myers squibb , abbvie research funding : abbvie travel , accommodations , expenses : bristol - myers squibb sabah kadri no relationship to disclose jane e . 
churpek honoraria : uptodate kenisha allen no relationship to disclose dawn conway no relationship to disclose carolyn marinier no relationship to disclose consulting or advisory role : bristol - myers squibb , exelixis , eisai norm d . 
stadler honoraria : cvs caremark , sotio , astrazeneca , bristolmyers squibb consulting or advisory role : cvs caremark , sotio , astrazeneca , bristol - myers squibb , eisai , bayer , pfizer , clovis oncology , genentech research funding : bayer ( inst ) , bristol - myers squibb ( inst ) , boehringer ingelheim ( inst ) , exelixis ( inst ) , novartis ( inst ) , genentech ( inst ) , glaxosmithkline ( inst ) , medivation ( inst ) , pfizer ( inst ) , merck ( inst ) , millennium ( inst ) , janssen ( inst ) , johnson & johnson ( inst ) , astrazeneca ( inst ) , abbvie ( inst ) , x4 pharma ( inst ) , calithera biosciences ( inst ) other relationship : uptodate , american cancer society affiliations all authors : university of chicago , chicago , il . support supported by national institutes of health grant no . 
hahn nm , bivalacqua tj , ross ae , et al : a phase ii trial of dovitinib in bcg - unresponsive urothelial carcinoma with fgfr3 mutations or overexpression : hoosier cancer research network trial hcrn 12 - 157 . 
nogova l , sequist lv , perez garcia jm , et al : evaluation of bgj398 , a fibroblast growth factor receptor 1 - 3 kinase inhibitor , in patients with advanced solid tumors harboring genetic alterations in fibroblast growth factor receptors : results of a global phase i , dose - escalation and dose - expansion study . 
loriot y , necchi a , park sh , et al : erdafitinib ( erda ; jnj - 42756493 ) , a pan - fibroblast growth factor receptor ( fgfr ) inhibitor , in patients ( pts ) with metastatic or unresectable urothelial carcinoma ( muc ) and fgfr alterations ( fgfra ) : phase 2 continuous versus intermittent dosing . 
plimack er , dunbrack rl , brennan ta , et al : defects in dna repair genes predict response to neoadjuvant cisplatin - based chemotherapy in muscle - invasive bladder cancer . 
iyer g , balar av , milowsky mi , et al : multicenter prospective phase ii trial of neoadjuvant dosedense gemcitabine plus cisplatin in patients with muscle - invasive bladder cancer . 
teo my , seier k , ostrovnaya i , et al : alterations in dna damage response and repair genes as potential marker of clinical benefit from pd - 1 / pd - l1 blockade in advanced urothelial cancers . 
bergman a , einbeigi z , olofsson u , et al : the western swedish brca1 founder mutation 3171ins5 ; a 3.7 cm conserved haplotype of today is a reminiscence of a 1500 - year - old mutation . 
kadri s , long bc , mujacic i , et al : clinical validation of a next - generation sequencing genomic oncology panel via cross - platform benchmarking against established amplicon sequencing assays . 
dhillon kk , taniguchi t : resistance to parp inhibitors mediated by secondary brca1 / 2 mutations , in curtin nj , sharma ra ( eds ) : parp inhibitors for cancer therapy . 
garsed dw , alsop k , fereday s , et al : homologous recombination dna repair pathway disruption and retinoblastoma protein loss are associated with exceptional survival in high - grade serous ovarian cancer . 
 mechanistic learning for combinatorial strategies with immuno - oncology drugs : can model - informed designs help investigators ? joseph ciccolini , pharmd , phd1 ; dominique barbolosi , phd1 ; nicolas andr e , md , phd1 , 2 ; fabrice barlesi , md , phd3 ; and s ebastien benzekry , phd4 the past couple of years have seen an unprecedented number of failures of clinical trials investigating combinatorial strategies with immuno - oncology drugs ( iods )  . beyond the highly publicized crashes of the mystic study1 ( antipd - l1 plus anti - ctla4 in nonsmall - cell lung cancer [ nsclc ] ) or the echo - 301 trial2 ( antipd - 1 and anti - ido in melanoma ) , many other attempts to combine immunotherapy with radiation therapy ( rt ) , 3 chemotherapy , 4 metronomic chemotherapy , 5 or antiangiogenics6 have similarly led to disappointing results . 
because successful immunotherapy is restricted today to a limited number of patients in a limited number of cancers ( melanoma , lung cancer , head and neck cancer , and kidney cancer , with 5 - year survival rates , 40% ) , developing appropriate strategies to stretch efcacy remains critical ( eg , by turning cold tumors [ noninammatory with lack of inltrating t cells ] into hot ones [ inltrated by t cells ] )  . 
several studies successfully associated conventional treatments with iods in comparative phase iii trials.7 , 8 however , these trials should not hide the high attrition rate of too many other studies . 
one of the common characteristics of the trials is the lack of computational pharmacology support , plus the lack of prior knowledge regarding the pharmacokinetics ( pk ) / pharmacodynamics ( pd ) relationships of the combined treatments . 
actually , comes from the fact that , sometimes , some combinatorial clinical trials manage to be successful . author affiliations and support information ( if applicable ) appear at the end of this article . accepted on march 20 , 2020 and published at ascopubs.org / journal / po on may 8 , 2020 : doi 1200 / po.19.00381 to improve the design of such combinatorial trials beyond trial - and - error methods , we propose an innovative strategy termed mechanistic learning ( fig 1 )  . we dene it as the combination of mechanistic modelingsimulation of the kinetics of pathophysiologic processesand statistical ( machine ) learning . using data generated from previous clinical trials and preclinical experiments , it consists in building computational models able to simulate and predict the toxicity and efcacy outcomes of candidate regimens . the optimal scheduling is then selected for clinical trial testing . 
limited options when performing combinatorial trials are therefore a major caveat , possibly explaining many failures , or at least limiting the conclusions regarding the real intrinsic potential of a given combination . 
for instance , in the checkmate032 study , the antipd - 1 nivolumab and the antictla4 ipilimumab were administered to patients with nsclc using only 2 dosing modes ( ie , 1 and 3 mg / kg and vice versa )  . 
these doses were chosen because they were already combined in a previous phase i study.9 in dose - nding trials , up to 5 dose levels ranging from 0.1 to 20 mg / kg have been tested for nivolumab and ipilimumab used as single agents without reaching dose - limiting toxicities.10 , 11 consequently , at least 25 different combinations in dosing could have been explored in checkmate - 032 , not to mention the countless variations in sequencing and scheduling . 
in the subsequent checkmate - 143 study , the same strategy failed to improve survival in patients with glioblastoma.12 another example of a poorly designed study is the modul umbrella trial , which tested a triple combination of uoropyrimidines , the antiangiogenic bevacizumab , and the antipd - l1 atezolizumab in patients with metastatic colorectal cancer ( mcrc )  . 
baseline data can be composed of demographic , clinical , pathologic ( eg , histologic type ) , molecular ( eg , genetic mutations ) , or biologic ( eg , blood counts ) variables . 
survival data ( eg , progression - free or overall survival ) can also be modeled with a mechanistic basis ( instead of biologically agnostic survival analysis based on , eg , cox regression ) , using adapted , survival learning statistical methods . 
ct1 , rst chemotherapy ; ct2 , second chemotherapy ; mtki , maintenance tyrosine kinase inhibitor ; ps , performance status ; tgi , tumor growth inhibition ; tki , tyrosine kinase inhibitor . surprisingly , in this study , all drugs were administered concomitantly at xed dosing . 
this combination failed to exhibit signicant efcacy in terms of progression - free survival , and thus , the conclusion was that adding atezolizumab to standard of care for maintenance in mcrc showed no benet.13 actually , this conclusion may sound peremptory because it is not possible to know whether or not different dosing or scheduling with exactly the same drugs would have performed better . 
for instance , trial of nivolumab , 23 the impact of dosing ( ie , 0.1 - 10 mg / kg ) on pd - 1 receptor occupancy was investigated . 
similar target engagement ( ie , 64% - 70% ) was achieved regardless of the dosing , thus prompting several observers to conclude that pk / pd relationships were at with iods and , therefore , that interpatient variability was not an issue . 
however , in this seminal study , pd - 1 inhibition was measured only on circulating t lymphocytes extracted from peripheral blood and not on inltrated t lymphocytes in the tumor microenvironment . 
importantly , the pharmacokinetics of most therapeutic monoclonal antibodies is characterized by large interindividual variability and reduced ability to diffuse the vascular space and reach solid tumors.24 out of therefore , to what extent differences in nivolumab dosing could affect or not target engagement at the tumor levels , and not only in circulating t cells , remains to be fully investigated . 
critically , it would also be highly informative to analyze the data generated using the initial model to close the mechanistic learning loop . using similar principles for tumor heterogeneity , others have proposed the concept of adaptive therapy , suggesting individuals be treated only upon disease progression.38 this was further successfully translated at bedside in patients with metastatic castration - resistant prostate cancer.39 such a strategy could help to personalize combinations of iods and aromatase inhibitors in the neoadjuvant treatment of breast cancer.40 despite their scarcity , these studies highlight how application of mathematical modeling in clinical trials in oncology is now feasible and can rationalize study design . these innovative methods are yet to be extended to iod combinations . 
modeling immunotherapy has recently been applied to gain insights on optimal modes for combinations with rt.41 - 43 for instance , kosinsky et al42 were able to simulate multiple sequences of antipd - 1 treatment in combination with rt and validated their results using preclinical data . 
 commentary the general modeling methodology that could be undertakenmechanistic learningis a combination of mechanistic modeling and statistical learning , either from machine learning , mixed - effects learning , 45 or survival learning , 46 for integration of the multimodal data arising from clinical trials or routine management ( fig 1 )  . 
as output , it would provide informative simulations of the effect of various doses and schedules to aid decisions in early clinical studies . these would consist of predicted probabilities of graded toxicities , tumor growth kinetics in response to treatment , and survival outcomes . 
of note , there is a major trend by health regulatory agencies such as the us food and drug administration to call for incorporating extensive modeling and simulation into clinical research.47 in this respect , and regarding the current challenges with iods , 48 we believe that mechanistic learning could be a valuable tool for decision making when setting up combinatorial strategies . conclusion after a rst phase of enthusiasm , success stories with immunotherapy seem to have reached a glass ceiling because many studies now fail to further stretch either response rates or survival.49 consequently , combining immune checkpoint inhibitors with other treatments likely to boost tumor immunity is a rising strategy in clinical oncology . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . joseph ciccolini honoraria : pierre fabre , pzer , roche , novartis research funding : roche , merck serono travel , accommodations , expenses : astrazeneca nicolas andr e research funding : bristol - myers squibb ( inst ) travel , accommodations , expenses : bristol - myers squibb fabrice barlesi honoraria : genentech , pzer , pierre fabre , astrazeneca , bristol - myers squibb , boehringer ingelheim , eli lilly , novartis , merck serono , msd oncology , takeda , bayer consulting or advisory role : genentech , pzer , novartis , pierre fabre , bristol - myers squibb , astrazeneca / medimmune , boehringer ingelheim , eli lilly , merck serono , msd oncology , takeda , bayer research funding : genentech ( inst ) , astrazeneca / medimmune ( inst ) , bristol - myers squibb ( inst ) , pierre fabre ( inst ) , abbvie ( inst ) , amgen ( inst ) , bayer ( inst ) , boehringer ingelheim ( inst ) , eisai ( inst ) , eli lilly ( inst ) , ipsen ( inst ) , innate pharma ( inst ) , novartis ( inst ) , merck serono ( inst ) , msd oncology ( inst ) , pzer ( inst ) , sano - aventis ( inst ) , takeda ( inst ) travel , accommodations , expenses : genentech , bristol - myers squibb , astrazeneca / medimmune , msd oncology no other potential conicts of interest were reported . acknowledgment we thank elena ivanchenko for graphic assistance . 
in memory of marie - christine masini . references 41 : 41 - 48 , 2019 rizvi na , chul cho b , reinmuth n , et al : durvalumab with or without tremelimumab vs platinum - based chemotherapy as rst - line treatment for metastatic nonsmall cell lung cancer : mystic . 
mcbride sm , sherman ej , tsai cj , et al : a phase ii randomized trial of nivolumab with stereotactic body radiotherapy ( sbrt ) versus nivolumab alone in metastatic ( m1 ) head and neck squamous cell carcinoma . 
 ciccolini et al rothschild s , zippelius a , savic s , et al : sakk 16 / 14 : anti - pd - l1 antibody durvalumab ( medi4736 ) in addition to neoadjuvant chemotherapy in patients with stage iiia ( n2 ) non - small cell lung cancer ( nsclc ) a multicenter single - arm phase ii trial . 
j clin oncol 36 , 2018 ( suppl 15 ; abstr tps8584 ) 1200 / jco.2018.36.15_suppl.tps8584 toulmonde m , penel n , adam j , et al : use of pd - 1 targeting , macrophage inltration , and ido pathway activation in sarcomas : a phase 2 clinical trial . 
jama oncol 4 : 93 - 97 , 2018 gao j , karam ja , tannir nm , et al : a pilot randomized study evaluating nivolumab ( nivo ) or nivo + bevacizumab ( bev ) or nivo + ipilimumab ( ipi ) in patients with metastatic renal cell carcinoma ( mrcc ) eligible for cytoreductive nephrectomy ( cn ) , metastasectomy ( ms ) or post - treatment biopsy ( bx )  . 
j clin oncol 36 , 2018 ( suppl 15 ; abstr 4520 ) socinski ma , jotte rm , cappuzzo f , et al : atezolizumab for rst - line treatment of metastatic nonsquamous nsclc . 
hellmann md , rizvi na , goldman jw , et al : nivolumab plus ipilimumab as rst - line treatment for advanced non - small - cell lung cancer ( checkmate 012 ) : results of an open - label , phase 1 , multicohort study . 
ribas a , camacho lh , lopez - berestein g , et al : antitumor activity in melanoma and anti - self responses in a phase i trial with the anti - cytotoxic t lymphocyteassociated antigen 4 monoclonal antibody cp - 675 , 206 . 
grothey a , tabernero j , arnold d , et al : fluoropyrimidine and bevacizumab plus or minus atezolizumab as rst - line treatment for braf wild type metastatic colorectal cancer : findings from the modul trial of biomarker - driven maintenance . 
schaer da , beckmann rp , dempsey ja , et al : the cdk4 / 6 inhibitor abemaciclib induces a t cell inamed tumor microenvironment and enhances the efcacy of pd - l1 checkpoint blockade . 
heery cr , osullivan - coyne g , madan ra , et al : avelumab for metastatic or locally advanced previously treated solid tumours ( javelin solid tumor ) : a phase 1a , multicohort , dose - escalation trial . 
lindauer a , valiathan cr , mehta k , et al : translational pharmacokinetic / pharmacodynamic modeling of tumor growth inhibition supports dose - range selection of the antipd - 1 antibody pembrolizumab . 
long gv , tykodi ss , schneider jg , et al : assessment of nivolumab exposure and clinical safety of 480 mg every 4 weeks at - dosing schedule in patients with cancer . 
h enin e , meille c , barbolosi d , et al : revisiting dosing regimen using pk / pd modeling : the model1 phase i / ii trial of docetaxel plus epirubicin in metastatic breast cancer patients . 
barlesi f , imbs d - c , tomasini p , et al : mathematical modeling for phase i cancer trials : a study of metronomic vinorelbine for advanced non - small cell lung cancer ( nsclc ) and mesothelioma patients . 
yu ha , sima c , feldman d , et al : phase 1 study of twice weekly pulse dose and daily low - dose erlotinib as initial treatment for patients with egfr - mutant lung cancers . 
poleszczuk jt , luddy ka , prokopiou s , et al : abscopal benets of localized radiotherapy depend on activated t cell trafcking and distribution between j immunother cancer 6 : 17 , 2018 metastatic lesions . 
claret l , girard p , hoff pm , et al : model - based prediction of phase iii overall survival in colorectal cancer on the basis of phase ii tumor dynamics . 
coosemans a , vankerckhoven a , baert t , et al : combining conventional therapy with immunotherapy : a risky business ? eur j cancer 113 : 41 - 44 , 2019 49 . 
komen big data for breast cancer initiative : how patient advocacy organizations can facilitate using big data to improve patient outcomes jerome jourquin , phd , ms1 ; stephanie birkey reffey , phd1 ; cheryl jernigan2 ; mia levy , md , phd3 ; glendon zinser , phd1 ; kimberly sabelko , phd1 ; jennifer pietenpol , phd4 ; and george sledge jr , md5 integrating different types of data , including electronic health records , imaging data , administrative and claims databases , large data repositories , the internet of things , genomics , and other omics data , is both a challenge and an opportunity that must be tackled head on . 
komen envisions a world with a seamless web of health care information , where patients are informed and empowered to use their data to improve their health care ; electronic health records ( ehrs ) are connected to other data sources to provide evidence - based support for clinical decision making ; many , if not all , patients participate in clinical research ; data systems are linked , secure , and easily accessible ; genomics and other omics are universally available and user friendly ; researchers can mine enhanced data sets to address questions ; and most importantly , fewer people die of breast cancer and quality of life improves for those living with the disease . 
komen convened three big data for breast cancer ( bd4bc ) meetings to foster open dialog among experts and strategically invited a wide array of participants ( patient advocates , oncologists , bioethicists , laboratory researchers , genomicand proteomics - based companies , big datafocused pharmaceutical companies , and data software companies ) to discuss the status of , challenges in , and barriers to optimizing big data and the opportunities big data can provide to advance health care ( fig 1 )  . the rst meeting ( new york , ny , october 2015 ) focused on the barriers , opportunities , needs , priorities , and solutions concerning the challenge of improving breast cancer research and care through big data . 
 jourquin et al bd4bc ( 2015 ) bd4bc\wc ( 2017 ) bd4bc3 ( 2018 ) all bd4bc meetings bioethics and policy data analytics and learning systems data integration and management funders omics government and insurance providers oncology and patient care patient advocate patient - centered data and systems fig 1 . 
omics experts were the most represented in the rst two meetings ( 35% and 29% , respectively )  . a more equal distribution of expertise was reached at the 2018 meeting among patient - centered data and systems , data analytics and learning systems , and data integration and management ( 15% to 23% each ) , highlighting the intent to work on solutions to big data challenges in breast cancer and implementation . 
looking at all 148 unique participants who attended komens bd4bc meetings , the most represented areas of expertise were omics ( 27% ) , data analytics and learning systems ( 19% ) , data integration and management ( 17% ) , and oncology and patient care ( 11% )  . 
bd4bc\wc , west coast ( second bd4bc meeting ) ; bd4bc3 , third bd4bc meeting . claims databases , large data repositories ( registries and cohorts ) , and genomics and other omics data . 
we share the insights gained from these meetings and komens planned actions to leverage big data to reduce the number of breast cancer deaths . as recently as 15 years ago , individual patient data were only available in paper charts located at a single institution and inaccessible to others outside that institution . 
data from epidemiologic studies , cooperative group trials , and individual laboratories were often quantitatively modest , dispersed , and not open to sharing except through manuscripts and public presentations.1 the world of data is rapidly changing , and the amount of data related to breast cancer has exploded . 
within the past decade , various types of data are now routinely collected : personal and family history ; breast density ; patient - reported outcomes ; imaging data ; clinical trial data ; genomics and other omics ; annotated mutations ; biospecimens ; and social , environmental , and behavioral data . 
one of us ( m.l. ) reported at the third bd4bc meeting that in 2015 , one health care systems ehr was accessed by 11 , 000 people per day , creating 6.8 million clinic notes that year , and was associated with 1.7 million outpatient electronic prescriptions and 15 million clinical communications that year . furthermore , genomics , proteomics , metabolomics , radiomics , and other emerging omics platforms are expanding the data generated in health care.3 decreasing costs and increasing availability of such tests allow clinicians to evaluate tumors via whole exome , genome , or deep sequencing . these are becoming part of the standard of care . 
afliations are at the time of each meeting . abbreviations : bd4bc\wc , west coast ( second bd4bc meeting ) ; bd4bc3 , third bd4bc meeting ; cloud , consortium for local ownership and use of data . area with a rapidly growing platform generating large amounts of individual - specic data is the internet of things ( iot ) , which includes all devices attached to the internet that generate data.4 wearable devices ( eg , tness trackers ) individual - specic generate continuous , multiparameter , data . 
by 2020 , an estimated 200 billion devices will be connected to the internet and generating continuous data , with approximately 30% of these data predicted to have medical applications.4 with rapid technologic advances and vast amounts of data come challenges that must be overcome to make efcient use of the technology and data being collected . 
big data technologies , such as ehrs , omics , and iot , provide great potential , but these technologies remain siloed and not interoperable.5 , 6 data are often limited geographically and by age group and type of care . 
the use of these technologies is also limited by the inability of different platforms to communicate with each other , hospital rewalls that create barriers to sharing data , privacy issues ( real and perceived ) , and the lack of nancial models to incentivize storage , sharing , and integration . 
 jourquin et al internet of things patient - reported outcomes and registries genomics other omics imaging data electronic health records integration big data for breast cancer research improved outcomes for patients with breast cancer fig 2 . 
the integration of various types of data ( patient - reported outcomes ; imaging data ; electronic health record data ; genomics and other omics ; and so on ) can fuel scientic discoveries and lead to improved outcomes for patients with breast cancer . multiple processing engines ; and a strong , unied security model . 
this includes the technology to support development of these systems and applications and harness the power of these enhanced data sets in big data projects . although data storage remains a challenge , many companies are creating scalable solutions for data storage , including health data . technologic innovation brings opportunities to accelerate research discovery and improve patient care . 
precision medicine can be achieved by using big data technologies to combine different types and sources of data to identify patterns , determine optimal treatments for individuals , and improve their outcomes.8 imaging is another technologic opportunity where big data can be leveraged in breast cancer . 
approximately 75 million mammograms are performed annually worldwide , currently requiring a large amount of personnel time to read and analyze the results of each test . emerging advances in articial intelligence ( ai ) methods ( eg , convolutional neural networks and deep learning ) are being used in mammography to distinguish patients with benign , malignant , and negative disease , 9 and objectively assess breast density.10 similar advances are taking place in magnetic resonance imaging , where machine learning is being used to predict patients response to therapy and outcomes.11 big data imaging applications can be used to automate image reading and generate reports without human interaction , allowing radiologists to only review images not easily interpreted by the algorithms . 
although these data are often not standardized , natural language processing and other advanced technologies such as ai can help simplify extraction of unstructured data.16 another challenge is that big data are less well curated than other classic data sets ( eg , prospective clinical trials and epidemiologic registries )  . 
perhaps the biggest barrier in big data research application is that basic laboratory and clinical translational researchers often have no expertise in the multidimensional analytics and visualization tools that big data requires . 
research funding organizations ( public and private ) often do not provide support to cover costs of data annotation , curation , and sharing , and they rarely support training programs focused on big data . applying big data to research applications offers enormous possibilities , with the potential to solve questions currently unanswerable in traditional research laboratories . 
 advancing big data for better breast cancer care and outcomes machine learning was successfully used on those data to identify mirna biomarkers in breast cancer.19 pros , rwd , and rwe represent other areas where big data can be generated and harnessed for research applications.15 pros include data collected directly from patients ( eg , quality of life and functional status ) that are not interpreted by physicians or others.20 because only approximately 3% of patients with cancer participate in clinical trials , big data approaches to pros and rwd / rwe may represent realistic ways of integrating information about under - represented populations and nding solutions to previously intractable clinical problems . 
these data are linked to deep , next - generation sequence proling across hundreds of cancer - related genes for each patients tumor , as assessed by foundation medicine ( cambridge , ma ) .23 pharmaceutical companies and the us food and drug administration are also active in the eld and understand the value of rwd / rwe in developing and regulating medical products.24 , 25 komens bd4bc meetings offered valuable insights into the great and unmet need to advance training in and improve access to big data . 
breast cancer researchers without a data science focus could be trained in the eld of data science by participating in workshops and conferences to learn new methods , skills , and techniques to advance their research projects using big data . 
effective use of big data to improve breast cancer care can also be facilitated by bringing together data set owners , both nonprot and forprot , with data scientists , with the goal of creating access to breast cancer data sets for research . 
several thousand patients with metastatic breast cancer have registered to share their data for research.27 a similar participation response was recently obtained by the national institutes of health ( nih ) with their all of us study.28 patients desire for new knowledge about their disease often outweighs their privacy concerns . 
still , many patients have questions about what control they have over their data , electronic accessibility , 26 privacy , and data security , and why data sharing is important . government laws and regulations make medical data one of the few remaining bastions of privacy . 
in addition to the health insurance portability and accountability act and ofce of human research protection , siloed data have additional barriers , including business or proprietary interests , privacy concerns , transaction costs associated with data infrastructure and data sharing , and the nature of local legacy systems . although data sharing has become more common , it is often inefcient because data must be standardized , deidentied , and possibly shared via an institutional review boardapproved study with appropriate participant consent . 
this presents another challenge because most patients only agree to one study at a time , meaning re - consent is needed for each use.29 the growing number of companies that view patient data as a commercial asset is particularly concerning . 
what a patient originally agreed to share with his or her initial consent may be unknown . whether data can be shared for additional investigations and commercial purposes is unknown.6 other challenges to data sharing include interface glitches , moving data between formats , and questions of whether the data depositor is legally liable if public data are misinterpreted by another user.7 some companies do not want their data placed in a centralized , accessible location because they want to retain control of them , retain exclusive rights to their analyses , and / or monetize the data and their usage . overall , little incentive exists to share or make data readily and easily accessible . patient advocacy organizations such as komen can help address some of the problems associated with data sharing , starting with educating and advocating for patient needs and concerns regarding privacy and data sharing . 
financial support for infrastructure , curation , de - identication , sustainability , and appropriate guidelines is necessary to implement this requirement.1 another highlight from komens bd4bc meetings is that motivation for sharing data may increase if patients learn the value of sharing information for big data - driven research and if the study results are shared with patients . 
this highlights the important role patient advocates can play in demanding that data be shared , such as pressuring different stakeholders to work together toward a common goal , urging sustainability of good ideas , and requesting that study results be shared with patients . 
such data can provide guidance on the likelihood a given patient with breast cancer will benet from chemotherapy.34 this type of testing has also stratied more than 15 subtypes of breast cancer , allowing omics data to inform prognoses and treatments.3 , 35 , 36 cases showing the actual value of big data in patient care are currently lacking . 
a few anecdotal examples of how big data are being integrated in the patient care workow exist . for example , one of us ( m.l. ) created an analytic dashboard to leverage patient data and show patients care status in nearreal time . 
the dashboard ultimately led to changing the policy and to women undergoing biopsy sooner . for millions of patients with breast cancer , ehrs represent an important , comprehensive resource for patient care . because patients continuously receive care , ehrs allow longitudinal tracking of long - term outcomes ( eg , time receiving therapy and safety events )  . 
ehr - based treatment plans are also being used to reduce medication errors compared with prior paper - based approaches , increase standardization , and allow retrieval of data for quality measures within institutions . challenges remain with ehr systems . 
with the integration of omics analyses in ehrs to drive clinical decision , ehr systems have become large enterprises , requiring large infrastructure and computational power many clinics cannot afford . 
current ehrs frequently decrease clinical efciency , demoralize physicians by turning them into data entry specialists , and decrease time of direct patient - physician interaction . physicians feel ehr systems exist primarily to aid hospital billing , rather than facilitate patient care . 
one of us ( g.s. ) highlighted what was at stake in improving how physicians interact with ehr systems to optimize patient care : save a doctors time , save a patients life . an identied opportunity for ehr systems is their ability to revolutionize how quality of care is assessed . 
including genomic and other omics data directly in ehrs should promote high - level clinical decision support and improved access to clinical trials to realize the full potential of precision medis higher - quality , more costicine . 
this trial used an ehr system to create a real - time registry of patients that alerted the health care team when participants missed appointments or had an unmet care milestone . 
the intervention imnavigation and clinical proved treatment completion and helped reduce racial disparities in treatment of these patients.38 accure exemplies the power of harnessing big data to address health disparities in breast cancer care . 
the patient populations at health systems with sophisticated ehrs , data sharing systems , and capabilities to collect and store biospecimens for later analysis are likely not representative of the true diversity of patients across all settings.37 thus , any advancement resulting from big data should be designed and implemented for the maximum number of individuals who can benet from it . 
minority populations should be adequately represented in data sets so that safe and effective treatment strategies for all patients can be drawn from the results of studies using them . increasing efforts to better classify breast cancer are driving wide use of molecularly based precision medicine in oncology practice . 
access to big data can supercharge these types of data - fueled studies by providing an ever - growing number of data points and characteristics about everyone within a population.37 ai may be able to identify patterns within subpopulations that predict the risk of occurrences , recurrences , and generally worse outcomes , as well as optimal , tailored treatment plans . 
these studies may allow more efcient access to care , better treatment adherence by patients within the continuum of care , and more precise identication and management of at - risk populations . 
big data may truly facilitate personalized medicine , regardless of race , ethnicity , or other characteristics . discussion with the growing availability of pros and rwd , ai will likely affect clinical practice and clinical trial design in the near term , and increase our understanding of patients response to therapy . yet , most of the general public and many patients are unaware of or have concerns about big data and its application to cancer research and treatment . 
developing and implementing educational resources ( eg , fact sheets , web portal on big data , patient advocate training ) will be critical to making data sharing understandable and easy . 
patients want to control the use of their data.4 an educated , engaged advocacy community is crucial for bd4bc to succeed . komen will start by developing an online knowledge portal designed as a hub of information for visitors to advance their knowledge about big data . meeting participants repeatedly mentioned the lack of both data scientists working in breast cancer and laboratory and clinical researchers who are uent in big data analytics . 
komen and similar organizations can support researcher education by providing funding opportunities to train breast cancer researchers in big data and attract data scientists to apply big data to solve remaining challenges in breast cancer.39 a central directory of existing breast cancer data sets available to big data scientists to use in breast cancer research is essential . in addition , support must exist for projects that will accelerate the technologic advancement and innovative thinking necessary to discover novel targets for precision medicine and provide earlier detection that will affect empower the public with information and tools to make data sharing understandable and easy to do big data for patients bd4bc communications bd4bc knowledge portal using big data to fuel scientific discoveries and accelerate the delivery of equitable , patient - focused care address challenges of incorporating big data applications into breast cancer research and clinical care big data travel scholarships bd4bc hackathons breast cancer data directory bd4bc meetings use big data to fuel scientific discoveries and accelerate the delivery of equitable , patient - focused care big data research projects bd4bc workshops fig 3 . 
komen is following a three - pronged approach ( white boxes ) in developing several programs ( pink boxes ) that will specically address some of the challenges identied during komens bd4bc meetings and detailed in this article . 
organizations such as komen can leverage their grant - making capabilities to identify and support big data research resources and projects that put the patient at the center of innovation to inform and accelerate the pace of breast cancer research and improve patient care . funding is needed to support data science projects and infrastructure for aggregation , visualization , and modeling of patientand laboratory - derived big data . 
public advocacy is needed so initiatives can leverage big data to support adherence to treatment and participation in clinical trials , and enforce safety , security , data standards , accessibility , and sharing requirements . 
protection of minorities and underserved populations in the big data revolution is needed to ensure these groups are included in the progress big data will make toward better breast cancer outcomes . in conclusion , many opportunities were identied at komens bd4bc meetings to harness big data to benet patients with breast cancer . 
strategies include educating the public to make data sharing understandable and easy , addressing challenges of incorporating big data applications into breast cancer research and clinical care , and funding data science projects . 
komen will continue to advocate for putting the patient at the center of innovation and support efforts using big data to fuel scientic discoveries and accelerate the delivery of improved , equitable , and patientfocused care . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . stephanie birkey reffey travel , accommodations , expenses : genentech mia levy employment : seqtech diagnostics ( i ) leadership : personalis stock and other ownership interests : personalis , genomoncology honoraria : roche consulting or advisory role : personalis , genomoncology , roche research funding : genomoncology patents , royalties , other intellectual property : royalties from genomoncology for licensing of mycancergenome content travel , accommodations , expenses : roche jennifer pietenpol stock and other ownership interests : bluebird bio , johnson & johnson , roche , gilead sciences ( i ) , quest diagnostics , illumina , kite pharma , novartis ( i ) research funding : incyte corporation ( inst ) patents , royalties , other intellectual property : jennifer pietenpol is an inventor ( pct / us2012 / 065724 ) of intellectual property ( tnbctype ) licensed by insight genetics other relationship : susan g . 
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denny j : aacr modernizing population sciences in the digital age , early progress on the all of us research prograpresented at the american association for cancer research , san diego , ca , february 19 - 22 , 2019 29 . 
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 beyond the androgen receptor : targeting actionable drivers of prostate cancer see accompanying article doi : more than 70 years ago , huggins et al1 exploited the exquisite and unique dependence of prostate cancer ( pc ) on androgenic hormones for survival and growth using a treatment strategy that foreshadowed the clinical benefits underlying the application of precision oncology . 
today , variations of androgen receptor ( ar ) pathway targeting remain the cornerstone of the initial management of men with metastatic pc , usually with gratifying responsesalthough unfortunately few cures . 
however , the advent and application of technologies capable of deep assessments of the full spectrum of molecular aberrations that underlie the development and progression of malignant neoplasms now forecast the near - term potential of new therapeutic approaches poised to change the near - exclusive reliance on ardirected interventions as initial treatment for advanced pc . studies using whole - exome sequencing and comprehensive rna sequencing , supported through the cancer genome atlas2 and stand up to cancer / prostate cancer foundation3 initiatives , have profiled hundreds of localized and castration - resistant metastatic pcs ( crpcs ) , resulting in the identification of numerous recurrent driver aberrations that comprise signaling programs and pathways for which there are pharmacologic inhibitors . 
lacking in these previous studies was an assessment of untreated metastatic tumors . in the article accompanying this editorial , abida et al4 have taken the first step in filling this knowledge gap . using a predefined gene panel , abida et al4 evaluated mutations and copy losses in key oncogenes and tumor suppressors across a spectrum of localized pc , untreated metastatic disease , and crpc . 
the tumor assays were conducted in a clinical laboratory improvement amendments environment using real - world clinical samples , which demonstrates the feasibility of molecular profiling to guide therapeutics , even in challenging situations such as evaluating bone metastases . overall , a high frequency of potentially actionable alterations were identified that included components of the phosphatidylinositol 3 - kinase ( pi3k ) pathway ( 24% ) , mitogen - activated protein kinase pathway ( 5% ) , and b - catenin program ( 15% )  . this study also confirmed previous reports that aberrations in genes involved in dna repair are common , particularly those involved in the process of homologous recombination repair.5 overall , 22% of tumors had somatic aberrations in a dna repair gene , and 19% were found to have a putative deleterious germ line mutation . 
this pc subtype is notable for therapeutics such as poly ( adp - ribose ) polymerase inhibitors and platinum - based chemotherapy that could exploit a dna repair vulnerability.6 , 7 however , it is important to recognize that it is currently unclear whether each gene comprising the dna repair machinery will exhibit enhanced responses to these agents , nor is it clear whether each type of aberration within a particular dna repair gene will confer congruent outcomes with respect to treatment response . 
preclinical studies using functional readouts of dna repair proficiency and clinical trials coupled with careful assessments of each dna damage response gene aberration will be required to confirm predictive associations . overall , there was substantial heterogeneity in the composition of putative cancer drivers between individuals , a finding that supports avoiding a onesize - fits - all approach to therapy . 
 number of matched tumors from the same patient demonstrated consistent truncal aberrations in tumor suppressors such as tp53 and brca2 and amplification of ar across each tumor evaluated . these results indicate that sampling a single metastatic site provides a reasonable assessment of the major molecular alterations that may influence treatment decisions . 
however , analyses of tumors across intervals of time and treatment indicated that molecular evolution does occur , with higher mutation counts in tumors sampled at later time points . consequently , it is not clear whether sampling a primary tumor or a metastatic tumor early in the course of disease will accurately reflect driver or resistance mechanisms that are operating later in the course of cancer progression . a distinguishing feature of the abida et al4 study involves the acquisition and assessment of metastatic tumors that had not been exposed to ar - directed therapy or other systemic treatment . comparing the features of these metastases with those of localized tumors serves to identify drivers of the metastatic process , and comparing their molecular composition with that of tumors withstanding ar - directed therapy serves to identify mechanisms contributing to treatment resistance . in the first comparison , it is notable that aberrations in ar did not occur , emphasizing that ar mutation and copy - number gain , frequent events in crpc , occur in response to pressures exerted by ar pathway inhibition and rarely or never arise as de novo drivers of pc . 
in addition to ar , the frequency of aberrations in tp53 , rb1 , pten , and atm was significantly increased in crpc compared with metastatic noncastrate disease , indicating potential roles in mediating castration resistance . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . interactions with the ar or ar program or if they promote pc growth through mechanisms that bypass ar requirements . 
although enriched in crpc , a substantial number of treatment - nave tumors did exhibit mutations or structural alterations in these genes , suggesting that cotargeting the aberrant pathways concurrently with the ar may serve to circumvent predestined pathways of resistance . that drug combinations current therapy for metastatic pc generally follows a paradigm of sequentially deploying a given therapeutic such as androgen deprivation to the point of resistance , switching to another agent such as abiraterone or enzalutamide , and treating again to resistance , until options are exhausted . 
nelson consulting or advisory role : janssen oncology , astellas pharma , genentech acknowledgment supported by national institutes of health grants no . p30ca15704 and p50ca097186 , us department of defense grant no . 
cancer genome atlas research network : the molecular taxonomy of primary prostate cancer . arch surg 43 : 209 - 223 , 1941 cell 163 : 1011 - 1025 , 2015 3 . 
mateo j , carreira s , sandhu s , et al : dna - repair defects and olaparib in metastatic prostate cancer . n engl j med 373 : 1697 - 1708 , 2015 7 . 
schweizer mt , zhou xc , wang h , et al : the influence of prior abiraterone treatment on the clinical activity of docetaxel in men with metastatic castration - resistant prostate cancer . 
smith mr , saad f , rathkopf de , et al : clinical outcomes from androgen signaling - directed therapy after treatment with abiraterone acetate and prednisone in patients with metastatic castration - resistant prostate cancer : post hoc analysis of cou - aa - 302 . 
 case of metastatic extramammary paget disease of the vulva treated successfully with trastuzumab emtansine introduction extramammary paget disease ( empd ) is a rare adenocarcinoma in situ that originates in skin that contains apocrine glands . 
empd is associated with invasive cancer in 4% to 20% of patients.1 in a series of 1 , 439 patients with invasive empd , 80.4% had localized disease , 17.1% had locoregional spread , and only 2.5% presented with distant disease.2 treatment is primarily surgical , but empd frequently is multicentric , and relapses are common regardless of treatment modality . 
since 2002 , she underwent six excisional procedures , three laser ablations , several courses of topical imiquimod treatment , external beam vulvar radiation to a dose of 56 gy to the perineum and the left - side inguinal nodes , and interstitial brachytherapy to 30 gy . 
her treatment was complicated by urethral swelling and eventually obstruction , requiring placement of a temporary suprapubic catheter and urethral reconstruction in late 2014 . in early 2016 , the patient noted worsening urinary retention , and a computed tomography ( ct ) urogram demonstrated two centrally hypodense liver lesions that measured up to 2.2 cm , multiple enlarged retroperitoneal lymph nodes , and a circumferential soft tissue mass that infiltrated the cervix and upper vagina . 
on examination under anesthesia , a paget lesion obliterated the perineum , including the urethra , vulva , and perianal area , and vaginoscopy was required to visualize the cervix . 
vulvar biopsy specimens confirmed invasive , poorly differentiated adenocarcinoma that had arisen from empd , with extensive lymphovascular space invasion and 3 + her2 immunostaining in > 10% of cells ( fig 1 )  . 
on the basis of high concordance between dna sequencingbased methods and fluorescent in situ hybridization ( fish ) in detecting erbb2 amplification , 5 fish was foregone . the patient underwent six cycles of carboplatin area under the curve of 5 mg ml / min and paclitaxel 175 mg / m2 chemotherapy every 21 days , gillian l . 
 ( a ) nests of extramammary paget disease in the epithelium ( black arrows ) with underlying invasive adenocarcinoma in the dermis ( red arrow ; hematoxylin - eosin stain magnification , 10 )  . 
 ( b ) strong , circumferential membranous staining of human epidermal growth factor receptor 2 ( her2 ) in extramammary paget disease and invasive tumor ( her2 immunohistochemical stain magnification , 10 )  . 
 ( c ) invasive adenocarcinoma ( hematoxylin and eosin stain magnification , 10 ) with ( d ) 3 + membranous staining of her2 ( her2 immunohistochemical stain magnification , 10 )  . with trastuzumab added from cycles 2 to 6 . 
repeat pet / ct scanning after 3 months of maintenance therapy revealed an intensely fdg - avid recurrent cervical and vaginal tumor and mildly enlarged and fdg - avid left - side external iliac nodes . 
treatment was well tolerated , with toxicity limited to grade 1 fatigue and grade 1 bleeding , including intermittent vaginal bleeding , hematuria , epistaxis , and gum bleeding , which started after cycle 2 . 
follow - up pet / ct scans were notable for markedly decreased size and metabolic activity of the primary pelvic lesion after cycle 3 and for complete resolution of disease on imaging after cycle 6 ( fig 2 )  . 
positron emission tomography / computed tomography ( a ) axial fusion , ( b ) sagittal fusion , and ( c ) maximum intensity projection images before ( top ) and after treatment ( bottom )  . 
 a hypermetabolic cervical mass ( arrow ) was seen with associated hydrometra , which had complete treatment response to chemotherapy . and hormonal suppression with letrozole.6 , 7 although insufficient data exist on the application of the current breast cancer asco - cap her2 testing guidelines8 to other cancer types , the amplification of her2 has been described in many cases of invasive empd ( table 1 )  . 
 multiple large , multicenter trials have firmly established the benefit of trastuzumab in the treatment of metastatic her2 - positive breast cancer , 9 which has led to consideration of trastuzumab in the treatment of invasive metastatic her2 - amplified empd . retrospective data have suggested that her2 overexpression is higher in patients with invasive empd than with noninvasive empd.19 furthermore , a significant correlation has been demonstrated among the presence of invasion , lymph node metastasis , and her2 overexpression.24 several case reports have demonstrated partial or complete response of widely metastatic empd on trastuzumab with or without paclitaxel ( table 2 )  . the mechanisms that underlie trastuzumabs clinical activity have not been completely table 1 . 
although tdm1 has been shown to be efficacious in patients with breast cancer with her2 - overexpressed malignancy unresponsive to trastuzumab , disease response has not been consistently demonstrated with other tumor types . 
 in her2 - positive unresectable gastric or gastroesophageal junction cancers with prior her2 - targeted therapy.36 the current patients favorable response indicates that in her2 positive invasive empd , tdm1 may be considered a viable treatment option . 
in addition , in hormone receptor and her2 - positive breast cancer , dual targeting of both signaling pathways may improve outcomes significantly.37 in breast cancer , bidirectional cross talk between the estrogen receptor and her2 pathways likely contributes to anti - her2 therapy resistance . 
 preclinical models with breast cancer cell lines have demonstrated a benefit to simultaneous hormone and her2 therapy over her2 - targeted therapy alone , but no phase ii or iii trials have compared the two.38 the tandem trial demonstrated a 2.4 - month survival benefit in postmenopausal patients with metastatic breast cancer who received anastrazole and trastuzumab versus hormonal therapy with anastrazole alone.39 hormone receptor immunohistochemistry was not examined in the current patient , but dual inhibition may be a theoretically superior strategy for treating hormone receptor and her2 - positive invasive empd . one limitation to this study is that the asco - cap her2 testing guidelines have not been routinely adopted or validated for tissues other than breast carcinoma ; thus , the her2 immunohistochemistry results may not be consistent or reliable in this tumor type . 
molecular subtyping has been used increasingly to find appropriate targeted therapies and may be more reliable than immunohistochemistry.23 vornicova et al7 reported a partial response that lasted 12 months in a male with adenocarcinoma with paget disease and negative her2 testing by both immunohistochemistry and fish , but received anti - her2 therapy on the basis of tumor somatic mutation testing alone ( table 2 )  . in light of the poor prognosis with metastatic epmd , paucity of treatment options , high incidence of her2 amplifications in empd , and favorable adverse effect profile of tdm1 , we suggest her2 testing and consideration of tdm1 treatment in patients with her2 overexpressed invasive empd who experience treatment failure with trastuzumab . 
ohara k , fujisawa y , yoshino k , et al : a proposal for a tnm staging system for extramammary paget disease : retrospective analysis of 301 patients with invasive primary tumors . 
vornicova o , hershkovitz d , yablonski - peretz t , et al : treatment of metastatic extramammary pagets disease associated with adnexal adenocarcinoma , with anti - her2 drugs based on genomic alteration erbb2 s310f . 
tchrakian n , flanagan l , harford j , et al : new asco / cap guideline recommendations for her2 testing increase the proportion of reflex in situ hybridization tests and of her2 positive breast cancers . 
ogawa t , nagashima y , wada h , et al : extramammary pagets disease : analysis of growth signal pathway from the human epidermal growth factor receptor 2 prote hum pathol 36 : 12731280 , 2005 16 . 
plaza ja , torres - cabala c , ivan d , et al : her - 2 / neu expression in extramammary paget disease : a clinicopathologic and immunohistochemistry study of 47 cases with and without underlying malignancy . 
villada g , farooq u , yu w , et al : extramammary paget disease of the vulva with underlying mammary - like lobular carcinoma : a case report and review of the literature . 
tanaka r , sasajima y , tsuda h , et al : concordance of the her2 protein and gene status between primary and corresponding lymph node metastatic sites of extramammary paget disease . 
tessier - cloutier b , asleh - aburaya k , shah v , et al : molecular subtyping of mammary - like adenocarcinoma of the vulva shows molecular similarity to breast carcinomas . 
barth p , dulaimi al - saleem e , edwards kw , et al : metastatic extramammary pagets disease of scrotum responds completely to single agent trastuzumab in a hemodialysis patient : case report , molecular profiling and brief review of the literature . 
arnould l , gelly m , penault - llorca f , et al : trastuzumab - based treatment of her2 - positive breast cancer : an antibody - dependent cellular cytotoxicity mechanism ? br j cancer 94 : 259 - 267 , 2006 31 . 
lewis phillips gd , li g , dugger dl , et al : targeting her2 - positive breast cancer with trastuzumab - dm1 , an antibody - cytotoxic drug conjugate . 
krop ie , kim sb , martin ag , et al : trastuzumab emtansine versus treatment of physicians choice in patients with previously treated her2 - positive metastatic breast cancer ( th3resa ) : final overall survival results from a randomised open - label phase 3 trial . 
thuss - patience pc , shah ma , ohtsu a , et al : trastuzumab emtansine versus taxane use for previously treated her2 - positive locally advanced or metastatic gastric or gastro - oesophageal junction adenocarcinoma ( gatsby ) : an international randomised , open - label , adaptive , phase 2 / 3 study . 
lousberg l , collignon j , jerusalem g : resistance to therapy in estrogen receptor positive and human epidermal growth factor 2 positive breast cancers : progress with latest therapeutic strategies . 
kaufman b , mackey jr , clemens mr , et al : trastuzumab plus anastrozole versus anastrozole alone for the treatment of postmenopausal women with human epidermal growth factor receptor 2 - positive , hormone receptor - positive metastatic breast cancer : results from the randomized phase iii tandem study . 
 r predictive and prognostic properties of human equilibrative nucleoside transporter 1 expression in gemcitabine - treated pancreatobiliary cancer : a metaanalysis purpose gemcitabine , the primary drug for the treatment of pancreatobiliary cancer ( pbc ) , requires human equilibrative nucleoside transporter 1 ( hent1 ) to enter cells . 
 high tumoral hent1 expression has been linked with improved survival among patients with pbc treated with gemcitabine ; however , this finding has been inconsistent , and studies used different expression assays . methods databases were reviewed for studies that examined hent1 and clinical outcome in pbc . 
five studies were excluded for redundancy , and 29 studies underwent detailed review . results on average , 51% of tumor samples had high hent1 expression ( range , 7% to 92% )  . 
among studies that examined hent1 expression and overall survival ( os ) , 58% ( 15 of 26 studies ) showed an association between high tumoral hent1 and improved os for gemcitabine - treated patients . 
an association between high tumoral hent1 expression and improved disease - free / progression - free survival ( dfs / pfs ) was demonstrated in 71% of studies ( 15 of 21 studies )  . 
2018 by american society of clinical oncology introduction the human equilibrative nucleoside transporter 1 ( hent1 ) is a member of the ent family of a sodium - independent nucleoside transporters encoded by the slc29 gene family . 
this meta - analysis examined whether immunohistochemistry of human equilibrative nucleoside transporter 1 ( hent1 ) had prognostic and / or predictive correlation with outcomes in gemcitabine - treated patients with pancreatobiliary cancer . 
it contains 29 studies and , to our knowledge , is the largest such meta - analysis to date . knowledge generated the pooled hazard ratio analyses demonstrated a link between high hent1 tumor expression and improved overall survival and disease - free / progression - free survival . 
this relationship is antibody dependent . relevance use of a validated hent1 immunohistochemistry assay before treatment could allow stratification of patients who would respond to gemcitabine and those who would not . 
the nonresponders could then be treated with another regimen , which would unnecessary toxicity and delay of effective treatment . the hent family of nucleoside transporters and hent1 in particularis expressed in many different types of malignant tumors , including colorectal cancer , 3 gastric cancer , 4 and pancreatobiliary cancer ( pbc ) .5 immunohistochemistry ( ihc ) analyses from various studies have shown that , on average , 51% of human pbcs display strong hent1 expression , although the rates of high or positive expression vary wildly , from as low as 7% to as high as 92% ( table 1 ) .6 - 34 interest in the hent family of transporters increased after it was found that they play a crucial role in facilitating the entry of cytotoxic nucleoside analogs , such as gemcitabine , cytarabine , and fluorouracil , into malignant cells . 
 gemcitabine relies almost entirely on hent1 and hent2 to gain entry into cells , and early in vitro studies showed that lack of hent1 expression confers high - level resistance to gemcitabine in gi tumor cell lines.35 this makes hent1 expression particularly important in pancreatic and biliary tract cancers , for which gemcitabine based treatments are commonly used.36 , 37 the biology of hent1 and its interactions with key chemotherapy drugs in pancreatic , gastric , colorectal , and other cancers has led to the interest in using hent1 tumor expression as a biomarker to predict the efficacy of gemcitabine and other cytotoxic nucleoside analogs , such as cladribine , cytarabine , fludarabine , fluorouracil , and the fluorouracil prodrug capecitabine . 
 since the late 1990s , at least five antihent1 antibodybased assays were developed to facilitate hent1 tumor expression testing via ihc ; development started with 10d7g2 in edmonton , canada . 
this antibody was first tested in cells of the cns , 38 breast cancer , 39 and hodgkin lymphoma40 and is now commercially developed by angam scientific ( hamden , ct ) and due north ( edmonton , alberta , canada )  . 
subsequently , commercial antibodies were developed by various providers , including the following : 11337 - 1 - ap by proteintech group ( rosemont , il ) , hent1 antibody by mbl international [ hereafter called mbl - hent1 ( woburn , ma ) ] , pab2255 by abnova corporation ( taipei city , taiwan ) , and sp120 by ventana medical systems ( oro valley , az )  . although early studies that used the 10d7g2 antibody assay consistently showed an association between high tumoral hent1 expression and improved outcomes among gemcitabine - treated patients with pbc , 6 - 9 later studies that used a variety of other assays and other antibodies did not consistently demonstrate this link . 
 methods statistical analysis we followed prisma ( preferred reporting items for systematic reviews and meta - analyses ) guidance to perform this study . search strategy we performed a review of the literature using keyword searches of the pubmed and embase databases for articles related to hent1 expression and its impact on pbc outcomes and / or response to treatment . 
the search terms were as follows : human ent1 and its synonyms ( ent1 , hent1 , slc29a1 , human equilibrative nucleoside transporter - 1 ) along with pbc and its synonyms ( pancreatic cancer , biliary tract cancer )  . 
study inclusion criteria included retrospective and prospective studies of patients with pbc , at least one subpopulation treated with gemcitabine , expression of hent1 reported and related to patient outcome , published in english , and full text available with a cutoff date of march 1 , 2018 . 
to determine if there were studies with redundant populations , studies by the same authors were examined to determine the type of cancer , the source of the patient sample , the study location ( s ) , the dates of patient inclusion , and the expression assay used . 
if there was consensus overlap in all of these criteria , then the older or smaller study was excluded unless the newer study was a subpopulation analysis . data extraction the data were extracted from the relevant studies into premade spreadsheets by one author and included the following : author ( s ) and affiliation ( s ) ; publication date ; journal ; cancer type ; treatment setting ; number of patients ; type of clinical sample ; methodology to determine hent1 expression ( if ihc , the antibody used ) ; hent1 scoring ; distribution of high and low hent1 ; and median overall survival ( os ) , disease - free survival ( dfs ) / relapse - free survival ( rfs ) , and progression - free survival ( pfs ) along with hazard ratios ( hrs ) , cis , and p values . 
single - arm studies that demonstrated association between hent1 expression and patient outcome were classified as positive for correlation . detailed analyses were only performed on ihcbased studies because of the low number of studies using other methods . 
the 2 test was performed with excel ( version 2013 ; microsoft , redmond , wa ) to determine whether the choice of antibody was associated with a significant difference in the likelihood of demonstrating a relationship between hent1 and clinical outcomes . 
forest plots were produced with code written by author d.y. each evaluable ihc study was examined using the remark ( reporting recommendations for tumor marker prognostic studies ) recommendations for completeness of biomarker reporting.41 this 20 - point checklist was completed with the corresponding page number for each study ; a point was awarded for each guideline completed , and half of a point was awarded for guidelines that were partially completed . 
 because the majority of studies were retrospective , sample sizes were not calculated as with a prospective study ; the rationale for sample size guideline was examined for effect size or power calculation on the basis of the available sample size . 
seventeen were removed because they were letters , editorials , or comments on studies ; 57 were reviews or meta - analyses ; 39 were animal models or laboratory experiments ; seven were in other cancer types ; one was a cost analysis ; one was a trial design ; and one was a pathology methodology paper . there were 51 studies identified for detailed analysis . 
among these , 34 examined hent1 expression relationship with clinical outcome using antihent1 antibodies , 6 - 34 , 42 - 46 whereas 10 used reverse transcriptase polymerase chain reaction , 47 - 56 and one used liquid chromatography / tandem mass spectrometry quantitative proteomics of hent1.57 there were two sets of studies that used the same patient population but different antibody assays , and both studies in each set were included in the analysis.11 , 12 , 19 , 28 of the 34 ihc studies , five were removed for redundant populations and assays.42 - 46 the remaining studies were excluded because of the following : the study examined small nucleotide polymorphisms of hent1 rather than expression ( n = 4 ) , 58 - 61 the study was a clinical trial exclusively in patients with low / negative hent1 ( n = 1 ) , 62 or the study did not correlate hent1 expression with survival ( n = 1 ; correlation with gemcitabine incorporation into dna63 )  . there was no consensus among studies that examined hent1 expression by reverse transcriptase polymerase chain reaction and improved survival . 
of the nine evaluable studies , five showed a correlation between hent1 mrna levels and improved survival.47 - 50 , 55 this may be in part to the differences in primers ( only two studies used the same set of primers ) , the gene ( s ) used for normalization of expression ( eg , gapdh ) , and the source of the mrna ( frozen , fresh , formalin - fixed , paraffin - embedded [ ffpe ] samples )  . 
 high hent1 and improved survival , 47 , 49 , 50 , 55 including one that used both ffpe and fresh biopsy samples in rna later.55 there was good concordance between hent1 expression from both preservation methods . 
the one study that was not evaluable performed survival analysis with multiple genes ( including hent1 ) but also examined the consistency of mrna and protein expression patterns of hent1.56 this analysis showed a reverse concordance : samples that had high mrna had low protein , and vice versa . the study that used liquid chromatography / tandem mass spectrometry to quantify hent1 expression was a pilot study and only examined eight patient samples . 
the study did not find a significant correlation between expression as a continuous variable and pfs.57 among the 29 ihc studies , a total of 3 , 979 patients were examined for hent1 expression , of whom 2 , 285 were treated with gemcitabine chemotherapy . 
more than half of these studies ( 18 of 29 , or 62% ) demonstrated that high hent1 tumor expression was significantly associated with improved outcomes ( at least one of the survival outcomes [ os , dfs , or pfs ] and / or time to progression [ ttp ] in gemcitabine - treated patients with pbc ; table 26 - 34 )  . 
 two of the studies found the opposite association : high hent1 was associated with shorter dfs or ttp ; eight studies showed no relationship between hent1 expression and survival outcomes . 
one study did not report p values for the survival analysis , although os was longer in the high - hent1 subpopulation . the first study to examine the relationship between hent1 expression and clinical outcome used the 10d7g2 mouse monoclonal antihent1 antibody.6 each study that used the 10d7g2 antihent1 antibody demonstrated a significant association between high hent1 tumor expression and improved dfs or pfs outcomes in gemcitabine - treated patients ( six of six studies , or 100% )  . 
in addition , all but one study that used the 10d7g2 anti - hent1 antibody demonstrated a significant association between high hent1 tumor expression and improved os outcomes in gemcitabine - treated patients ( seven of eight studies , or 88% )  . 
studies that used the mbl - hent1 antibody showed a correlation between hent1 expression and improved os ( two of two studies , or 100% ) and dfs / pfs ( one of one , or 100% )  . 
of the studies that used the pab2255 antibody , 67% showed a statistically significant and favorable association between high tumoral hent1 expression and improved outcomes ( two of three studies for both os and dfs / pfs )  . 
only 50% of studies that used the 11337 - 1 - ap antibody showed a statistically significant link ( one of two studies for each of os and dfs / pfs )  . 
studies using the sp120 antibody had the worst correlation rate : only two ( 22% ) of nine studies demonstrated significant os associations , and three ( 43% ) of seven demonstrated a dfs / pfs association . 
these antibody - dependent differences in prognostic abilities had a 2 test p of .024 for os and a p of .086 for dfs / pfs for the three most commonly used antibodies ( 10d7g2 [ n = 8 for os and 6 for dfs / pfs ] , sp120 [ n = 9 for os and 7 for dfs / pfs ] , and pab2255 [ n = 3 for os and 3 for dfs / pfs ] ; figs 2a and 2b )  . we also examined whether the lack of consistency among studies was due to treatment intent and found no difference in the proportion of studies in each setting ( 2 p = .18 ; fig 2c )  . 
among the studies that found a positive association between high hent1 and improved survival , 26% ( five of 19 studies ) were from the advanced setting , whereas 63% ( 12 of 19 studies ) and 11% ( two of 19 studies ) were adjuvant and neoadjuvant , respectively . 
the treatment setting for the negative association studies was 20% advanced ( two of 10 studies ) , 60% adjuvent ( six of 10 studies ) , and 20% neoadjuvant ( two of 10 studies )  . 
2 analysis for the positive association rates of studies that was based on the three most commonly used antibodies ( 10d7g2 , sp120 and pab2255 ) reveals a p value of .0237 for ( a ) overall survival and of .855 for ( b ) disease - free / progression - free survival , which suggests that antibody choice influences the likelihood of finding a statistically significant relationship between high tumoral human equilibrative nucleoside transporter 1 ( hent1 ) expression and improved outcomes . 
in the funnel plot , only four studies had an hr : sample size value outside the normalized mean shape , and they did not alter the overall funnel shape ( fig 4b )  . discussion protein abundance of hent1 in malignant cells is a promising predictive and prognostic biomarker for pbc tumors treated with gemcitabine chemotherapy . 
in the radiation therapy oncology group prospective , randomized , adjuvant clinical trial rtog 9704 that compared gemcitabine with fluorouracil , high hent1 expression assessed with the 10d7g2 antibody was associated with improved dfs and os in patients treated with gemcitabine but not in those treated with fluorouracil.7 this established hent1 as a predictive , not simply a prognostic , biomarker , because this effect was gemcitabine specific and the interaction between treatment allocation and hent1 status was significant . 
 randomized phase ii trial ( total enrollment , n = 367 ) investigated the prognostic role of hent1 in patients treated with co - 101 ( a lipid - drug conjugate of gemcitabine ) versus gemcitabine in metastatic pancreatic cancer . 
this study , which used the sp120 antibody , did not demonstrate a correlation of hent1 expression with outcomes in either treatment group.25 another sp120 study from the aio - pk0104 ( arbeitsgemeinschaft internistische onkologie ) randomized phase iii trial demonstrated that hent1 overexpression lacked a prognostic relationship with survival for patients treated with gemcitabine - based chemotherapy compared with surgery alone.27 all of the studies included in this meta - analysis examined the relationship between hent1 protein levels and outcomes in gemcitabine treated patients with pbc . 
although the pooled hr analyses for all studies and adjuvant alone demonstrated relationships between hent1 expression and os and dfs / pfs , this was not seen in the advanced / metastatic setting . 
this is likely the result of the small number of studies included in the analyses ( n = 4 and n = 3 , respectively ) and the antibodies used . 
the 10d7g2 studies had positive associations between high hent1 expression and clinical outcomes , 9 , 10 whereas the sp120 studies had no relationship with os and a negative association between high hent1 expression and pfs.25 , 26 the effect of hent1 expression on patient outcomes , regardless of therapy , has also been investigated . 
in this study , untreated patients with a high expression of hent1 had shorter median survival than patients with low hent1 expression , which indicated that high hent1 expression may be an independent negative prognostic factor . 
this relationship was not found in other studies.11 , 13 , 30 our analyses demonstrate that the likelihood of a positive prognostic study may be influenced by the anti - hent1 antibody used . 
whereas 100% of studies that used the 10d7g2 antibody found a relationship between high hent1 expression and improved os and / or dfs / pfs in patients with pbc who were treated with gemcitabine , signals from other antibodies were less consistent . during the past decade , at least eight different antibodies against ent1 have been developed by biotechnology firms in canada , taiwan , and the united states . 
the first of such antibodies , named 10d7g2 , was developed in edmonton , canada , at the cross cancer institute.38 approximately one third of all published studies about hent1 expression in pbc have used this murine monoclonal antibody . 
subsequent to the development of 10d7g2 , several rabbit - derived antibodies against hent1 for the purposes of ihc were separately developed and commercialized : 11337 - 1 - ap , mbl - hent1 , pab2255 , and sp120 . 
this antibody is an igg , rabbit - derived monoclonal antibody distributed by ventana medical systems in the united states for laboratory use on ffpe tissue stained with the benchmark ihc stainer ( ventana )  . as seen in figure 2 , there is a striking difference in the outcome correlation rates of studies that used the 10d7g2 antibody compared with those that used other antibodies . 
whereas studies that used the 10d7g2 antibody had an 88% to 100% rate of association between high hent1 and improved os and dfs / pfs , the correlation rates with other antibodies were lower . 
the set stained with the leica bond polymer refine detection kit ( leica biosystems , wetzlar , germany ) had very few highly stained cells compared with set 2 , which was stained using the recommended iview dab detection kit ( ventana ) .28 the same cut point was used for each pair of these comparisons , so this did not add an additional potential confounding factor . 
 another study compared cut point methodology for the same antibody and patient population.27 there were similar proportions of high and low hent1 expressers with each cut point , and neither resulted in a significant association between sp120 - determined hent1 expression and survival . both of the studies that performed direct antibody comparisons between sp120 and 10d7g2 showed that a high proportion of cells had discordant staining . 
the cluster with high staining with both antibodies was the most sensitive , the cluster with high 10d7g2 and low sp120 had an intermediate response , and the double - low cluster had a poor response . 
the high 10d7g2 and low sp120 discordant staining pattern occurred in 31% of the samples ( 70 of 227 samples ) .14 within set 2 of the study by svrcek et al28 , only 45% of high hent1 samples ( 25 of 55 samples ) , and 59% of low hent1 samples ( 49 of 83 samples ) were matched between the sp120 and 10d7g2 antibodies . 
monoclonal antibodies differ in target epitope , method of generation , and species of origconsequently , they may bind to different sites on the hent1 glycoprotein , or theoretically different isoforms , in a manner that influences the staining pattern , intensity , or specificity for formalin - fixed hent1 . 
studies have shown that differential expression of gemcitabine metabolism proteins , including deoxycytidine kinase , ribonucleoside reductases m1 and m2 , and hu antigen r , as well as other signaling pathways can affect clinical outcomes to gemcitabine treatment.11 , 64 , 65 in conclusion , on the basis of a comprehensive review of the literature , the likelihood of finding a predictive , prognostic , or correlative link between hent1 tumor expression and outcomes for gemcitabine - treated patients with pbc is linked to the anti - hent1 antibody used . 
 the ability to predict response to gemcitabine therapy according to the hent1 expression profile would allow stratification of patients with high hent1 to gemcitabine monotherapy or gemcitabine - containing regimens and patients with low hent1 to other regimens , including the combination chemotherapy folfirinox . 
spratlin honoraria : celgene , sanofi , lilly , imclone consulting or advisory role : celgene , sanofi , lilly , imclone , taiho pharmaceutical , astellas pharma research funding : sanofi travel , accommodations , expenses : astellas pharma john r . 
park j : human equilibrative nucleoside transporter subtype 1 : structure - function analysis using cysteine mutagenesis and thiol modifying techniques , pharmacology and toxicology [ doctoral thesis ]  . 
spratlin j , sangha r , glubrecht d , et al : the absence of human equilibrative nucleoside transporter 1 is associated with reduced survival in patients with gemcitabine - treated pancreas adenocarcinoma . 
marchal r , mackey jr , lai r , et al : human equilibrative nucleoside transporter 1 and human concentrative nucleoside transporter 3 predict survival after adjuvant gemcitabine therapy in resected pancreatic adenocarcinoma . 
santini d , schiavon g , vincenzi b , et al : human equilibrative nucleoside transporter 1 ( hent1 ) levels predict response to gemcitabine in patients with biliary tract cancer ( btc )  . 
borbath i , verbrugghe l , lai r , et al : human equilibrative nucleoside transporter 1 ( hent1 ) expression is a potential predictive tool for response to gemcitabine in patients with advanced cholangiocarcinoma . 
marechal r , bachet jb , mackey jr , et al : levels of gemcitabine transport and metabolism proteins predict survival times of patients treated with gemcitabine for pancreatic adenocarcinoma . 
murata y , hamada t , kishiwada m , et al : human equilibrative nucleoside transporter 1 expression is a strong independent prognostic factor in uicc t3 - t4 pancreatic cancer patients treated with preoperative gemcitabine - based chemoradiotherapy . 
kalloger se , riazy m , tessier - cloutier b , et al : a predictive analysis of the sp120 and 10d7g2 antibodies for human equilibrative nucleoside transporter 1 ( hent1 ) in pancreatic ductal adenocarcinoma treated with adjuvant gemcitabine . 
kawada n , uehara h , katayama k , et al : human equilibrative nucleoside transporter 1 level does not predict prognosis in pancreatic cancer patients treated with neoadjuvant chemoradiation including gemcitabine . 
murata a , amano r , yamada n , et al : prognostic predictive values of gemcitabine sensitivityrelated gene products for unresectable or recurrent biliary tract cancer treated with gemcitabine alone . 
woo sm , yoon ka , hong ek , et al : dck expression , a potential predictive biomarker in the adjuvant gemcitabine chemotherapy for biliary tract cancer after surgical resection : results from a phase ii study . 
aoyama t , kazama k , miyagi y , et al : predictive role of human equilibrative nucleoside transporter 1 in patients with pancreatic cancer treated by curative resection and gemcitabineonly adjuvant chemotherapy . 
yamada r , mizuno s , uchida k , et al : human equilibrative nucleoside transporter 1 expression in endoscopic ultrasonography - guided fine - needle aspiration biopsy samples is a strong predictor of clinical response and survival in the patients with pancreatic ductal adenocarcinoma undergoing gemcitabine - based chemoradiotherapy . 
nakagawa n , murakami y , uemura k , et al : combined analysis of intratumoral human equilibrative nucleoside transporter 1 ( hent1 ) and ribonucleotide reductase regulatory subunit m1 ( rrm1 ) expression is a powerful predictor of survival in patients with pancreatic carcinoma treated with adjuvant gemcitabine - based chemotherapy after operative resection . 
sasaki h , murakami y , uemura k , et al : concurrent analysis of human equilibrative nucleoside transporter 1 and ribonucleotide reductase subunit 1 expression increases predictive value for prognosis in cholangiocarcinoma patients treated with adjuvant gemcitabine - based chemotherapy . 
fisher sb , fisher ke , patel sh , et al : excision repair cross - complementing gene - 1 , ribonucleotide reductase subunit m1 , ribonucleotide reductase subunit m2 , and human equilibrative nucleoside transporter - 1 expression and prognostic value in biliary tract malignancy . 
fisher sb , patel sh , bagci p , et al : an analysis of human equilibrative nucleoside transporter - 1 , ribonucleoside reductase subunit m1 , ribonucleoside reductase subunit m2 , and excision repair cross - complementing gene - 1 expression in patients with resected pancreas adenocarcinoma : implications for adjuvant treatment . 
poplin e , wasan h , rolfe l , et al : randomized , multicenter , phase ii study of co - 101 versus gemcitabine in patients with metastatic pancreatic ductal adenocarcinoma : including a prospective evaluation of the role of hent1 in gemcitabine or co - 101 sensitivity . 
ormanns s , heinemann v , raponi m , et al : human equilibrative nucleoside transporter 1 is not predictive for gemcitabine efficacy in advanced pancreatic cancer : translational results from the aio - pk0104 phase iii study with the clone sp120 rabbit antibody . 
sinn m , riess h , sinn bv , et al : human equilibrative nucleoside transporter 1 expression analysed by the clone sp 120 rabbit antibody is not predictive in patients with pancreatic cancer treated with adjuvant gemcitabine : results from the conko - 001 trial . 
svrcek m , cros j , marchal r , et al : human equilibrative nucleoside transporter 1 testing in pancreatic ductal adenocarcinoma : a comparison between murine and rabbit antibodies . 
elebro j , ben dror l , heby m , et al : prognostic effect of hent1 , dck and hur expression by morphological type in periampullary adenocarcinoma , including pancreatic cancer . 
brandi g , deserti m , vasuri f , et al : membrane localization of human equilibrative nucleoside transporter 1 in tumor cells may predict response to adjuvant gemcitabine in resected cholangiocarcinoma patients . 
xiao jc , zhang tp , zhao yp : human equilibrative nucleoside transporter 1 ( hent1 ) predicts the asian patient response to gemcitabine - based chemotherapy in pancreatic cancer . 
neoptolemos jp , palmer dh , ghaneh p , et al : comparison of adjuvant gemcitabine and capecitabine with gemcitabine monotherapy in patients with resected pancreatic cancer ( espac - 4 ) : a multicentre , open - label , randomised , phase 3 trial . 
jennings ll , hao c , cabrita ma , et al : distinct regional distribution of human equilibrative nucleoside transporter proteins 1 and 2 ( hent1 and hent2 ) in the central nervous syste neuropharmacology 40 : 722 - 731 , 2001 39 . 
reiman t , clarke ml , dabbagh l , et al : differential expression of human equilibrative nucleoside transporter 1 ( hent1 ) protein in the reed - sternberg cells of hodgkins disease . 
kondo n , murakami y , uemura k , et al : combined analysis of dihydropyrimidine dehydrogenase and human equilibrative nucleoside transporter 1 expression predicts survival of pancreatic carcinoma patients treated with adjuvant gemcitabine plus s - 1 chemotherapy after surgical resection . 
morinaga s , nakamura y , watanabe t , et al : immunohistochemical analysis of human equilibrative nucleoside transporter - 1 ( hent1 ) predicts survival in resected pancreatic cancer patients treated with adjuvant gemcitabine monotherapy . 
kobayashi h , murakami y , uemura k , et al : human equilibrative nucleoside transporter 1 expression predicts survival of advanced cholangiocarcinoma patients treated with gemcitabinebased adjuvant chemotherapy after surgical resection . 
kobayashi m , mizuno s , murata y , et al : gemcitabine - based chemoradiotherapy followed by surgery for borderline resectable and locally unresectable pancreatic ductal adenocarcinoma : significance of the ca19 - 9 reduction rate and intratumoral human equilibrative nucleoside transporter 1 expression . 
giovannetti e , del tacca m , mey v , et al : transcription analysis of human equilibrative nucleoside transporter - 1 predicts survival in pancreas cancer patients treated with gemcitabine . 
kim r , tan a , lai kk , et al : prognostic roles of human equilibrative transporter 1 ( hent - 1 ) and ribonucleoside reductase subunit m1 ( rrm1 ) in resected pancreatic cancer . 
orlandi a , calegari ma , martini m , et al : gemcitabine versus folfirinox in patients with advanced pancreatic adenocarcinoma hent1 - positive : everything was not too bad back when everything seemed worse . 
ashida r , nakata b , shigekawa m , et al : gemcitabine sensitivity - related mrna expression in endoscopic ultrasound - guided fine - needle aspiration biopsy of unresectable pancreatic cancer . 
sierzega m , pach r , kulig p , et al : prognostic implications of expression profiling for gemcitabine - related genes ( hent1 , dck , rrm1 , rrm2 ) in patients with resectable pancreatic adenocarcinoma receiving adjuvant chemotherapy . 
ohmine k , kawaguchi k , ohtsuki s , et al : quantitative targeted proteomics of pancreatic cancer : deoxycytidine kinase protein level correlates to progression - free survival of patients receiving gemcitabine treatment . 
tanaka m , javle m , dong x , et al : gemcitabine metabolic and transporter gene polymorphisms are associated with drug toxicity and efficacy in patients with locally advanced pancreatic cancer . 
li d , pant s , ryan dp , et al : a phase ii , open - label , multicenter study to evaluate the antitumor efficacy of co - 1.01 as second - line therapy for gemcitabine - refractory patients with stage iv pancreatic adenocarcinoma and negative tumor hent1 expression . 
costantino cl , witkiewicz ak , kuwano y , et al : the role of hur in gemcitabine efficacy in pancreatic cancer : hur up - regulates the expression of the gemcitabine metabolizing enzyme deoxycytidine kinase . 
ferguson , mbbs , mrcp , frcr4 ; alessandra curioni - fontecedro , md , pd1 ; martin zoche , phd1 ; holger moch , md1 ; and bart vrugt , md , phd1 introduction malignant mesothelioma ( mm ) is a rare neoplasm arising from the mesothelial cell lining of the pleura ( 80% to 90% ) , but it can also develop in the peritoneum ( 10% to 15% ) , pericardium , and tunica vaginalis.1 , 2 because of the long latency of the disease , the age at diagnosis ranges from 54 to 65 years3 - 5 ; thus , mm rarely occurs in young patients and children . the frequency of both pleural and peritoneal mm is almost equal in patients younger than age 40 years . 
in addition , previous asbestos exposure is less common in peritoneal compared with pleural mm.6 peritoneal mesothelioma commonly presents with vague and unspecic symptoms , including abdominal distension and weight loss.7 consequently , the diagnosis of peritoneal mesothelioma generally is made at an advanced stage of the disease , 8 which partly explains the poor clinical outcome , even after optimal oncologic and surgical treatment . 
the median survival is less than 12 months in the majority of patients.9 , 10 patients with mm are not routinely analyzed for the presence of potentially drug - targetable gene mutations , including anaplastic lymphoma tyrosine kinase ( alk )  . 
by using targeted next - generation sequencing of tumor dna and rna , hung et al11 recently identied alk rearrangements with three novel alk fusion partners in a small subgroup of patients with peritoneal mm . 
the alk breakpoint was mapped to intron 19 in all three cases , the strn breakpoint to intron 3 , the atg16l1 breakpoint to intron 2 , and the tpmi1 breakpoint to the beginning of exon 9 . here we report a 13 - year - old girl with peritoneal mesothelioma harboring an strn - alk gene fusion , which was identied by comprehensive genomic proling ( cgp )  . 
images before treatment showed large - volume ascites , bilateral hydrotissue nephrosis , and widespread peritoneal soft deposits particularly within the pelvis and around the liver with scalloping of the liver margin ( fig 1 )  . 
she had no history of asbestos or radiation exposure . peritoneal biopsies were obtained by an explorative laparoscopy and submitted for a histologic and molecular work - up . pathology multiple peritoneal biopsies revealed a tumor with a mixed tubulopapillary and solid growth pattern . immunohistochemistry with positivity for ck5 / 6 and calretinin in the absence of expression of the epithelial marker berep - 4 and claudin - 4 conrmed the mesothelial origin of the tumor . 
even though necrosis and mitotic activity ( less than 1 mitosis per 10 high - power elds ) were not evident , growth pattern , cytonuclear atypia of the tumor cells , and immune prole fullled the criteria for malignant epithelioid mesothelioma ( figs 2a and 2b )  . 
images before treatment demonstrate large - volume ascites , bilateral hydronephrosis , and widespread peritoneal soft tissue deposits particularly within the pelvis ( all ndings marked by green arrows )  . 
 ( b ) schematic representation of the strn - alk fusion showing the 700 - amino - acid ( aa ) - long fusion gene , with 137 aas originating from the n terminus of strn and the remaining 562 aas originating from the c terminus of alk . 
 ( a ) immunohistochemical staining showing strong expression of alk protein ( original magnication 40 )  . ( b ) alk uorescent in situ hybridization break - apart probes showing one fused red - green signal and one red signal in 96% of the tumor cells compatible with 5 ( cid : 1 ) alk deletion ( original magnication 100 )  . for a transient and self - limiting rise in alanine aminotransferase ( alt ) , no adverse effects were noted . discussion we report a dramatic tumor regression after the rst cycle of ceritinib in a 13 - year - old girl with alk - rearranged peritoneal mm . 
the alk receptor can be translocated , mutated , or overexpressed in non - squamous nonsmall - cell lung cancer , inammatory myobroblastic tumors ( imts ) , and anaplastic large - cell lymphomas ( alcls ) .14 it is well known that pediatric patients with imts or alcl can show strong and sustained clinical response to the inhibitory effects of the alk - targeting drug crizotinib.15 peritoneal mm is an extremely rare tumor in children , but an almost complete response to an alk - targeting drug has never been described before . 
recently , loharamtaweethong et al16 reported a 10 - year - old girl with an alk - translocated peritoneal mm detected by fish and immunohistochemistry , but the exact fusion partner was not determined . 
genetic alterations frequently seen in pleural and peritoneal mesothelioma , including cdkn2a , bap - 1 , nf2 , and setd2 , are not detected in patients with alk - rearranged disease.11 even though the prevalence of alk - rearranged peritoneal mesotheliomas is low , alk alterations seem to be restricted to peritoneal mesothelioma only and do not occur in pleural mm . 
this is consistent with our observation , because we were unable to demonstrate alk expression in a tissue microarray containing tumor samples from 221 patients with pleural mesothelioma , including 22 females of whom three were younger than age 40 years ( unpublished data )  . in our patients tumor sample , we identied a rare alk fusion by cgp . 
the platform used in this study can detect all alk alterations ( including atg16l1 and tpm1 fusions ) and has been extensively validated.12 even in alk fishnegative patients , alk rearrangements could be identied by using this method.18 in our patient , we detected an strn - alk fusion with similar breakpoints but with a fusion in the alk - rearranged patient protein identical described by hung et al.11 the strn - alk fusion was an inframe alteration with breakpoints for strn in intron 3 and alk in intron 19 . to that patients with alk - rearranged mm cannot be distinguished from their conventional counterparts , but the differences in clinical presentation ( young patients with no history of asbestos exposure ) and the detection of isolated alk mutations would justify a separate tumor entity of alk - rearranged mesothelioma . 
in the absence of genetic alterations of cdkn2a , bap - 1 , nf2 , and setd2 , it is tempting to speculate that fusions involving the alk gene may represent the predominant oncogenic driver in peritoneal mm in young female patients . 
on the basis of the success of therapeutic alk inhibition in our patient , alk fusion screening by cgp is highly advised in peritoneal mms , especially in young patients . 
the promising response in our patient also stresses the need for investigations involving a larger cohort of young female patients with alkrearranged peritoneal mm to determine the efcacy and durability of alk inhibition . 
r uschoff , elise gradhand , alessandra curioni - fontecedro , martin zoche , holger moch , bart vrugt administrative support : holger moch provision of study materials or patients : elise gradhand , helen rees , martin zoche , bart vrugt collection and assembly of data : elise gradhand , abdullah kahraman , helen rees , jane l . 
hoffmann - la roche holger moch honoraria : roche consulting or advisory role : roche , deniens research funding : roche ( inst ) travel , accommodations , expenses : roche pharma travel , accommodations , expenses : deniens no other potential conicts of interest were reported . references 20 : 935 - 944 , 2009 ray m , kindler hl : malignant pleural mesothelioma : an update on biomarkers and treatment . 
cancer causes control beebe - dimmer jl , fryzek jp , yee cl , et al : mesothelioma in the united states : a surveillance , epidemiology , and end results ( seer ) - medicare investigation of treatment patterns and overall survival . 
eur j gynaecol oncol 18 : 141 - 143 , 1997 asensio ja , goldblatt p , thomford nr : primary malignant peritoneal mesothelioma : a report of seven cases and a review of the literature . 
arch surg 125 : 1477 - 1481 , 1990 thomas a , chen y , yu t , et al : distinctive clinical characteristics of malignant mesothelioma in young patients . 
tumori 89 : 269 - 273 , 2003 kaya h , sezgi c , tanrikulu ac , et al : prognostic factors inuencing survival in 35 patients with malignant peritoneal mesothelioma . 
fabrizio da , george tj jr , dunne rf , et al : beyond microsatellite testing : assessment of tumor mutational burden identies subsets of colorectal cancer who may respond to immune checkpoint inhibition . 
moss e yp , voss sd , lim ms , et al : targeting alk with crizotinib in pediatric anaplastic large cell lymphoma and inammatory myobroblastic tumor : a childrens oncology group study . 
loharamtaweethong k , puripat n , aoonjai n , et al : anaplastic lymphoma kinase ( alk ) translocation in paediatric malignant peritoneal mesothelioma : a case report of novel alk - related tumour spectruhistopathology 68 : 603 - 607 , 2016 17 . 
ali sm , ou shi , he j , et al : identifying alk rearrangements that are not detected by fish with targeted next - generation sequencing of lung carcinoma . 
brodeur , md1 , 5 , 7 purpose the diagnosis of cancer predisposition in pediatric patients with cancer is vital for treatment decisions , surveillance , and management of at - risk family members . 
characteristics of patients who underwent constitutional testing , including family history and variant loss of heterozygosity , were tracked . results from 1 , 023 patients who underwent somatic tumor sequencing in a 28 - month period , 210 variants were identied in 141 patients ( 13.8% ) that were concerning for cancer predisposition syndromes requiring intervention . 
among patients tested , 23 ( 56.1% ) of 41 total patients were diagnosed with a cancer predisposition syndrome . conclusion our data demonstrate that more than one third of variants in tumor somatic sequencing that were concerning for underlying cancer predisposition were constitutionally conrmed . 
2019 by american society of clinical oncology introduction the incidence of constitutional genetic aberrations leading to cancer predisposition in pediatric patients with cancer is estimated at 8% to 12%.1 - 4 results from large somatic sequencing studies conrm that this rate of constitutional aberrations can be inferred from somatic sequencing results.5 , 6 the timely diagnosis of a cancer predisposition syndrome can have signicant implications not only for the patient , but also for affected and unaffected family members . 
follow - up of any features of a cancer predisposition syndrome is essential for appropriate management , surveillance , and family planning for these individuals . clinical and historical features that suggest a pediatric patient with cancer may have a predisposition syndrome include a family history of the same cancer or related cancers , clinical features of a predisposition syndrome , bilateral / multifocal primary cancer or multiple cancers , certain types of cancer that rarely occur except in a predisposed patient , and a much earlier than expected age at diagnosis . 
 macfarland et al context key objective when a child is diagnosed with cancer , most families are uncertain why their child developed a rare and devastating disease . for an important minority , an underlying cancer predisposition syndrome as a result of a constitutional pathogenic variant may underlie malignancy ; however , these can be difcult to identify in patients who lack syndromic features and / or a family history of cancer . knowledge generated this study demonstrates that pathogenic variants identied through somatic next - generation sequencing can indicate the presence of a constitutional cancer - predisposing variant . 
as tumor sequencing becomes more common and comprehensive , it is important for both patients and family members that appropriate measures are in place for genetic counseling and subsequent constitutional testing . 
in this report , we describe our experience in conducting cancer predisposition evaluation on the basis of somatic sequencing ndings in cancer samples identied using in - house next - generation sequencing testing panels . 
these targeted panels provided comprehensive analysis of hematologic and solid tumors for fusion genes , single - nucleotide variants , insertion / deletion variants , and copy number variants for 117 to 238 genes13 , 14 ( appendix table a1 )  . 
once identied in tumor tissue , the potential for suspicious variants to be of constitutional origin was described in the somatic tumor report issued to the ordering physician , usually an oncologist . testing , these suspected constitutional variants were tagged by the genomic diagnostics laboratory for referral to the cancer predisposition program ( cpp )  . 
somatic panel testing was not used as a substitute for clinical judgment , and a patient with concerning features of cancer predisposition would always be referred to the cpp regardless of somatic panel results . 
 pediatric somatic sequencing identies cancer predisposition available , but a complete family history review was not conducted by an oncologist , geneticist , or genetic counselor for patients not seen by the cpp . 
factors included in the analysis of patients seen by the cpp included family history of cancer , presence of multifocal or bilateral disease , loss of heterozygosity in the tumor , and clinical features of diagnosis , such as clinical diagnostic criteria for neurobromatosis type 1 ( nf1 ) or tuberous sclerosis , in addition to the aforementioned referral criteria . 
tumor type association with the presence of a constitutional variant for example , rhabdoid tumor and smarcb1 pathogenic variantwas also tracked.7 data also included age at diagnosis and turnaround time of constitutional testing ( days between the result report of somatic testing and the date of constitutional testing )  . 
as detailed in results , some variants had been previously constitutionally conrmed , and some were conrmed on the basis of clinical features alone and did not have testing completed . 
constitutional testing was listed as incomplete in all cases in which the cpp did not meet with the family to discuss the variant , even if testing may not ultimately have been suggested . 
finally , results were deemed conclusive when the genetic testing was interpretable and inconclusive when additional sample would be required to make a denitive diagnosis . data were analyzed using stata and r statistical programming languages , and statistical signicance was determined using wilcoxon rank - sum test and 2 test , when appropriate . 
visualizations were generated using the ggplot2 package.16 the human investigations performed in this study were completed after approval by the childrens hospital of philadelphia institutional review board and in accordance with the requirements of the department of health and human services , where appropriate . results population demographics records were reviewed for 1 , 023 patients who underwent somatic panel testing between february 2016 and june 2018 . 
a total of 210 somatic variants in 141 patients were suspected to be constitutional pathogenic or likely pathogenic variants , which is 13.8% of patients who underwent somatic panel testing during this time period . 
vaf met criteria for referral ( 0.4 ) in 78% of cases ( n = 164 ) , including those with copy number variant in a potential cancer predisposition gene . 
the remainder of variants were referred for the presence of a founder mutation ( 2.9% ; n = 6 ) or a tumor typespecic variant concerning for cancer predisposition ( 55.2% ; n = 116 ) , and some patients were referred for multiple reasons . 
demographics demographic age , years , mean female male race / ethnicity white black other hispanic / latino primary v relapse primary relapse / recurrent somatic findings in predisposition genes a total of 210 variants were identied in a total of 66 genes . a heatmap of genes with a suspected constitutional variant identied in 2 or more individuals is shown in figure 1 ( full variant list , including tumor type , in appendix table a2 )  . 
the second most frequent gene with potential constitutional variants was nf1 ( 17% ; n = 27 , including 6 individuals with an identied tp53 variant ) , followed by smarcb1 , mutyh , apc , atm , msh6 , wt1 , and dicer1 . 
founder mutations were identied in 6 patientsfor example , 4 of the 7 variants identied in apc were i1307k , a known founder risk allele in the ashkenazi jewish population that does not lead to familial adenomatous polyposis , but confers increased cancer risk in adulthood.17 some variants identied had implications for immediate treatment decisions , such as tp53 variants that were identied in patients with anticipated radiation therapy , and an attempt was made to prioritize these patients for testing and counseling . 
frequency of concerning somatic variants identied , as described by frequency , tumor type ( liquid , non - cns solid , and cns ) , primary versus relapsed / refractory specimen , and specic cancer diagnosis . 
aml , acute myeloblastic leukemia ; at / rt , atypical teratoid / rhabdoid tumor ; b - all , b - acute lymphoblastic leukemia ; dnet , dysembryoplastic neuroepithelial tumor ; gist , gi stromal tumor ; jmml , juvenile myelomonocytic leukemia ; mpnst , malignant peripheral nerve sheath tumor ; t - all , t - acute lymphoblastic leukemia . dicer1 , wt1 , 11p loss / aberrations , and non - i1307k apc variantsand in these cases screening was initiated during ongoing cancer treatment after a constitutional diagnosis was made . of note , several heterozygous variants identied had implications for adult cancer risk , but did not change management in the pediatric age range ( msh6 , mutyh , atm , brca1 , and brca2 )  . 
testing decisions on these variants were made on a case - by - case basis , in discussion with the family and the oncologist , and in most cases , it was recommended that constitutional testing of the proband be deferred until age 18 years or older . 
occasionally in adolescent patients , preferred to complete testing . the patient constitutional testing a total of 210 variants were determined to warrant follow - up for potential constitutional alterations on the basis of initial somatic panel review ( fig 2 ; appendix table a2 )  . 
schematic representation of patients referred for constitutional includes patients who did not have testing performed for clinical reasons , patients who still require referral and genetic testing , and results of testing for the patients for whom testing was conducted . 
patients were presumed positive if they met clinical criteria for a diagnosis without the need for genetic testing , and were presumed negative when they did not meet clinical criteria for a diagnosis . 
of the total number of patients with a somatic tp53 variant ( n = 46 ) , 19.6% were constitutionally affected ( n = 9 ; includes those patients who previously tested positive )  . 
this was based on known familial mutations in apc i1307l ( n = 2 ) , brca1 ( n = 1 ) , and brca2 ( n = 1 ) , or on the basis of an existing clinical diagnosis in seven nf1 patients already being observed by the neurobromatosis clinic . in six variants in ve individuals , testing was presumed negative , as individuals did not meet criteria for a syndrome that was not present clinically . 
in these cases , variants were not included in the tested category in subsequent analyses ; however , it is important to note that constitutional testing is not always required to conrm or rule out a diagnosis . 
in some cases , constitutional testing was not performed after discussion with the family , per family preference and / or clinician recommendation . constitutional testing was deferred in a total of 4 variants associated with adult - onset cancer risk until adulthood after family history discussion with family and review of ( apc i1307l [ n = 2 ] , blm [ n = 1 ] , mutyh [ n = 1 ] )  . 
this would likely be the recommendation for other somatic variants in adult - onset predisposition syndromes included in the genetic testing not done category ; however , genetic counseling and family history review need to take place before constitutional testing is deferred completely . 
a total of 8 families8 patients and 12 variantspreferred not to pursue constitutional testing , in one case because of a lack of insurance approval for testing . referral still required finally , a large number of patients66 patients and 91 variantsstill require referral to the cpp before constitutional testing can be completed . 
our program is actively working to ensure that all families with a concerning somatic variant receive appropriate genetic counseling . characteristics of tested patients historically , the suspicion for constitutional cancer predisposition is based on clinical characteristics , including family history , physical features of a predisposition syndrome , presence of bilateral / multifocal disease , and / or a specic tumor type strongly associated with a predisposition syndrome . 
there was no signicant difference between those conrmed and not conrmed in vaf 0.4 or in tumor loss of heterozygosity . discussion somatic findings concerning for cancer predisposition of the more than 1 , 000 children , adolescents , and young adults who underwent somatic tumor testing in the 28 months included within this study period , 13.9% had somatic results that were concerning for a constitutional cancer predisposition . 
0.4 , although in 22.2% of variants vaf was lower than this threshold , and clinical suspicion based on the specic variant prompted cpp referral . as expected , given the frequency of both constitutional and somatic mutations , 2 , 18 tp53 was the most frequently mutated gene that prompted referral to the cpp . 
of the 21 patients with a tp53 mutation in tumor tissue who were referred for testing , 6 ( 28.6% ) were diagnosed with lfs on the basis of a constitutional nding of a known tp53 pathogenic / likely pathogenic variant , three of whom would not have been referred based on accepted lfs testing guidelines.15 , 19 even including all somatic variants , at least 19.6% of patients with somatic lfs variants are constitutionally affected , a proportion higher than that observed in the adult population . 
all of these patients are now being observed by the cpp and are receiving recommended surveillance.20 the next most frequent mutation found was in nf1 , but decisions about constitutional testing were sometimes made on the basis of the presence or absence of characteristic clinical features of nf1 . 
of note , for some variants clinical guidelines are not yet established , and in these cases families received genetic counseling regarding the lack of accepted tumor surveillance practices and / or additional study needed regarding the constitutional presence of a variant . 
in cases in which constitutional testing would not affect clinical managementfor example , no additional childhood surveillance would be required families were informed of the result and adult relatives were counseled that testing for themselves , but testing was usually not sent for the child . finally , a discussion of somatic mosaicism occurred in the setting of inconclusive or negative results , or in cases in which families decided not to pursue genetic testing because of lack of clinical features of a disorder . they could consider additional study is required to analyze the power of somatic panel testing to identify pediatric patients with constitutional cancer predisposition , with and without the incorporation of clinical data , such as multifocality , tumor type , syndromic features , and family history . 
in addition , many patients have not yet been referred to the cpp to discuss constitutional testing , and qualitative review would suggest a variety of reasons for this , including emotional stress on the family at the time of cancer diagnosis and the additional stress of predisposition evaluation during treatment , although this has not been systematically studied at our institution . 
we plan to continue offering genetic testing and counseling to patients not yet referred to ensure an eventual 100% referral rate . interpretation of somatic results concerning for cancer predisposition the most signicant differences in those constitutionally conrmed were known clinical risk factors , namely , a signicant / concerning family history of cancer and bilateral or multifocal disease . 
this suggests that vaf and loh alone are not sufcient to rule out a cancer predisposition syndrome . although it may seem surprising that tumor type was not predictive , this is consistent with the known prevalence of a cancer predisposition syndrome in these tumor types . thus , clinical predictors of cancer predisposition remain important in the interpretation of somatic results . more than one half of patients who received constitutional testing were found to have an underlying cancer predisposition syndrome , often requiring changes in treatment plan , ongoing surveillance , and familial testing . 
some of these patients could have been referred for testing on the basis of patient age , type of cancer , and / or family history of cancer ; however , others would not have been suspected as a result of a lack of these features . 
thus , the incorporation of somatic testing results proves to be an important supjudgment in identifying cancer preplement to clinical disposition syndromes . in conclusion , somatic tumor sequencing is a powerful tool in pediatric cancer to risk - stratify patients and identify appropriate therapy , and its use is becoming increasingly widespread . 
 macfarland et al 6department of biomedical and health informatics , childrens hospital of philadelphia , philadelphia , pa 7department of pediatrics , the perelman school of medicine at the university of pennsylvania , philadelphia , pa data analysis and interpretation : suzanne p . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . pichai raman consulting or advisory role : scholar rock travel , accommodations , expenses : scholar rock gerald wertheim employment : johnson & johnson ( i ) stock and other ownership interests : johnson & johnson ( i ) stephen p . 
hunger stock and other ownership interests : amgen , merck ( i ) , amgen ( i ) , pzer ( i ) honoraria : amgen consulting or advisory role : novartis no other potential conicts of interest were reported . references 2018 1990 2017 brodeur gm , nichols ke , plon se , et al : pediatric cancer predisposition and surveillance : an overview , and a tribute to alfred g . 
clin cancer res 23 : e1 - e5 , 2017 zhang j , walsh mf , wu g , et al : germline mutations in predisposition genes in pediatric cancer . 
n engl j med 373 : 2336 - 2346 , 2015 parsons dw , roy a , yang y , et al : diagnostic yield of clinical tumor and germline whole - exome sequencing for children with solid tumors . 
nature 555 : 371 - 376 , postema fam , hopman smj , aalfs cm , et al : childhood tumours with a high probability of being part of a tumour predisposition syndrome ; reason for referral for genetic consultation . 
science 250 : 1233 - 1238 , jongmans mc , loeffen jl , waanders e , et al : recognition of genetic predisposition in pediatric cancer patients : an easy - to - use selection tool . 
goudie c , cullinan n , villani a , et al : retrospective evaluation of a decision - support algorithm ( mipogg ) for genetic referrals for children with neuroblastic tumors . 
genome med 11 : 32 , 2019 jain p , surrey lf , straka j , et al : novel fgfr2 - ina fusion identied in two low - grade mixed neuronal - glial tumors drives oncogenesis via mapk and pi3k / mtor pathway activation . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
achatz mi , porter cc , brugi `eres l , et al : cancer screening recommendations and clinical management of inherited gastrointestinal cancer syndromes in 49 : 3680 - 3685 , 2013 37 : 865 - 876 , 2016 cancer res 77 : 1250 - 1260 , 2017 childhood . 
the recommendation process in mtbs , however , has not been well defined , which limits applicability to larger clinical trials and patient populations . methods we created four fictional patients on the basis of recent real cases with genomic information on mutations , fusions , copy numbers , and gene expression . 
there was heterogeneity in the interpretation of tumor and germline aberrations as well as in standards of prioritization . conclusion differences in the interpretation and recommendation process contribute to heterogeneity in mtb recommendations . 
however , a randomized phase ii trial comparing therapy based on tumor molecular profiling versus conventional therapy in patients with refractory cancer ( shiva ) is the only prospective trial to have investigated a personalized therapy with negative results.8 in addition , many reported case studies have been criticized for incompleteness of data.9 thus , precision medicine has been called an unproven hypothesis.10 several potential explanations for the negative results have been suggested , including the limitations of predefined treatment strategies such as those used in the shiva trial.11 , 12 personalized oncology relies on several steps . 
the complexity of molecular aberrations , tumor heterogeneity , and technical and clinical difficulties have been addressed.13 , 14 in addition , the resulting data have to be interpreted and transformed into a treatment recommendation by identifying and prioritizing predictive biomarkers . 
several proposals have been made on how to arrive at clearly reportable recommendations.8 , 16 , 17 most rely on the definition of evidence levels attributed to every single aberration and the interdisciplinary discussion of the aberrations with regard to patient situation , availability of drugs , and clinical trials in a molecular tumor board ( mtb )  . 
 although this process is largely unstandardized , it is critical to facilitate the transformation of patient benefit from case studies to larger populations . to assess standards and differences in the interpretation process , we asked mtbs worldwide to make treatment recommendations for four fictional patients presented with different profiles of genomic aberrations . methods creation of sample patients four fictional patients were created on the basis of recent real cases . 
the possibility that selected aberrations could have co - occurred was validated in cbioportal for cancer genomics.18 data provided for every patient included age , cancer type , time of initial diagnosis , location and time of diagnosis of metastases , prior therapies , eastern cooperative oncology group performance status , and mutational profile ( one - letter amino acid code )  . 
molecular data provided for some of the patients included allele frequency , gene fusions , copy number alterations , gene expression data ( rna sequencing , reads per kilobase per million mapped [ rpkm ] ) , and germline aberrations . 
we asked for the percentage of patients with actionable alterations presented at the mtb , as well as for methods of trial recruitment practices and variant of unknown significance ( vus ) interpretation strategies after compilation of the data . identification of molecular tumor boards mtbs worldwide were identified through literature search , personal contacts , and online representations . 
mtbs were asked to participate in the survey under the prerequisite that a connection between recommendations and the participating board could not be made . data analysis and interpretation completed questionnaires and treatment recommendations from the mtbs were collected , and an analysis was performed . 
allele frequency data were requested by another two tumor boards ( mtb 3 and 5 ) but were not provided . results identification of molecular tumor boards and response we were able to identify and contact 29 mtbs in nine countries . 
26 - yearold patient mean coverage > 500 panel sequencing : kras g12v , bcorl1 r1332 * , tp53 h214fs * 7 , cdkn2c l65f , ctnna1 k577_ l578 > tkl , map3k1 t949_e950inst , mycn e47fs * 8 p365a , jak1 i597m , fancl t367fs * 12 + pik3ca amplification ( > 6 copies ) , myc amplification ( > 6 copies ) , mycl1 amplification ( > 6 copies ) , sox2 amplification ( > 6 copies ) , mutyh amplification ( > 6 copies ) 3 . 
58 - yearold patient gene fusions : tmem111tdrd3 gene fusion , prkdccdh17 gene fusion , ext1magi2 gene fusion whole - exome sequencing ( aug 2014 ) : germline : brca2 k3326 * ( 1n )  . 
sample patients as provided to the mtbs ( continued ) patient clinical information sequencing fusion genes copy no . gene expression additional information tumor biopsy from pulmonary metastasis april 2016 after progression on chemotherapy / cetuximab . 
 tumor purity 60% , coverage > 500 pik3ca e545k ( 25% allele frequency ) , mapk1 e322k ( 10% allele frequency ) , fgfr3 d786n ( 30% allele frequency ) 4 . 
 one mtb also requested information on specific patient factors ( willingness to travel , tolerance of treatment )  . comparison of treatment recommendations mechanistically similar treatment strategies ( eg , sorafenib or pan - raf inhibitor ) were interpreted as identical strategies . 
 there was a maximum overlap of three identical treatment strategies ( case 4 ) , whereas the other three cases ( cases 1 to 3 ) had a maximum of two identical top treatment recommendations ( tables 2 - 5 )  . 
patient cases had been designed with variable numbers of genetic aberrations ( case 1 , five aberrations ; case 2 , 14 aberrations ; case 3 , 18 aberrations ; case 4 , three aberrations )  . 
overall , treatment recommendations were more similar for the case with the least genomic information ( case 4 ) than for cases with more and more complex information ( case 2 and case 3 )  . 
one tumor board required additional confirmation by loss - of - heterozygosity testing.20 another tumor board stated that , according to an internal guidance document , vuss were generally not considered . potential germline aberrations , underlying tumor sequencing results , were considered by two mtbs . 
 germline variants triggering genetic counseling recommendations included a cdh1 mutation in patient 1 ( considered by two mtbs ) and tp53 mutations in patients 1 and 2 ( considered by one mtb )  . in the two cases with aberrations of copy number ( case 2 ) or gene expression and gene fusion ( case 3 ) data provided in addition to the mutations , there was no recommendation bias toward any one of these aberration types . 
recommendations were made on the basis of mutation and gene expression ( by two tumor boards each in patient 3 ) and amplification data ( three tumor boards in patient 2 )  . as included in the clinical information on the cases , checkpoint inhibitors had been tried unsuccessfully in two of the patients ( patients 1 and 4 )  . 
immune checkpoint inhibition was considered as a treatment option by two mtbs in one of the remaining two patients ( patient 2 ) and was the only recommendation by one of these tumor boards . 
the overall make - up of the mtbs was comparable , with similar numbers of individuals and specialties ( 15 to 30 individuals representing medical oncology , pathology , and additional specialties including radiology , informatics , and biology )  . 
in addition , whole - exome sequencing was used by two tumor boards , and copy number analyses ( comparative genomic hybridization or nanostring ) were used by another two . 
one tumor board reported using rna sequencing and germline controls in their routine diagnostics pipeline . another measure for comparing the functionality of an mtb was the rate of successful translation of recommendations into treatments . 
in contrast , the percentage of patients with potential targetable alterations , as reported by the mtbs , was between 20% and 90% . to analyze the prioritization process , we assessed the evidence base used for the interpretation of aberrations . 
two mtbs considered allele frequencies , and one tumor board reported a specific cutoff for considering allele frequency measurements ( > 50% deviation from that which was expected from other mutations )  . 
participants specialties medical oncology , pathology , molecular pathology , and pharmacy molecular pathology laboratory screening program , phase i unit , lung unit , head and neck unit , gi unit , gynecologic unit , sarcoma unit , and genitourinary unit tumor board pharmacy , medical oncology , pathology , genetic counseling , pediatric oncology , informatics , surgical oncology , biochemistry , hematology / oncology , pharmaceutical sciences , toxicology , pharmacology , and interventional radiology medical oncology , pathology , molecular biology , radiology , and interventional radiology medical oncology , pathology , molecular pathology , bioinformatics , biology , and treating physician no . 
results of questionnaire assessing participating tumor boards ( continued ) question evidence level patients with actionable alterations , % translated into treatment , % patients in structured clinical followup , % internal document ( including journal club with up to three studies and at least one clinical trial for offlabel therapy ) registration in clinical trials of all patients possible tumor board clinical evidence in humans needed published evidence levels published evidence levels data not yet collected data not yet collected 40 - 45 80 - 90 note . 
ranking of aberrations according to standardized evidence levels was performed regularly by two tumor boards , whereas an internal evidence document was used by another tumor board . discussion mtbs were established to provide a platform for precision oncology implementation . 
 studies in human genetics have shown differences among laboratories when analyzing identical variants.21 to our knowledge , this is the first study to analyze heterogeneities in the recommendation process of mtbs worldwide . currently , no standards for workflows and setups of mtbs exist . 
treatment recommendations as provided by the respective molecular tumor boards for patient 1 tumor board recommendation provided rationale additional recommendation pan - raf inhibitor no targeted therapy clinical trial for kras mutation downstream effect kras mutation kras mutation sorafenib clinical trial kras mutation met and ret testing genetic counseling for cdh1 and tp53 mutations ( potential germline mutation ) docetaxel and selumetinib kras mutation ( data from phase ii clinical trial ) genetic counseling ( cdh1 mutation ; potential germline mutation ) n / a because of missing information note . 
treatment recommendations as provided by the respective molecular tumor boards for patient 2 tumor board recommendation provided rationale additional recommendation pik3ca , akt , or mtor pik3ca mutation jak1 allele frequency testing ( infiltrating blood cells ? ) and if consistent with tumor : ruxolitinib jak1 mutation ( after considering allele frequency ) immunotherapy , atezolizumab independent of biomarker phase i trial with bromodomain inhibitor myc amplification pik3ca or mtor inhibitor pik3ca amplification ( data from case study ) consider genetic counseling and potential germline testing ( mutation burden , tp53 mutation , patient age ) everolimus clinical trial ( pik3ca amplification ) , sorafenib ( kras mutation ) mek inhibitor ( tp53 and kras mutation ) or checkpoint inhibition ( independent of biomarker , despite potential jak1 resistance ) n / a because of missing information note . 
rationales were provided for only some of the recommendations and asked for if missing initially . abbreviation : n / a , not available . and workflow of mtbs , the availability of clinical studies , the interpretation of vuss and potential germline aberrations , and the resulting recommendations . 
however , even this limited study was sufficient to uncover fundamental differences and identify problems in the recommendation process , the identification and discussion of which can be expected to help inform existing mtbs and the design of future studies . 
thus , we limited our analysis to identified heterogeneities and their potential effect on the precision oncology initiative . the heterogeneity in treatment recommendations presented here could be viewed , at first glance , as disturbing . 
treatment recommendations as provided by the respective molecular tumor boards for patient 3 tumor board recommendation provided rationale additional recommendation parp inhibitor brca2 mutation clinical trial for met amplification met amplification her2 inhibitor ( erbb2 overexpression ) , fgfr inhibitor ( fgfr3 overexpression ) or met inhibitor ( met overexpression ) off - label trastuzumab and pertuzumab , trastuzumab and lapatinib ( erbb2 overexpression ) or off - label crizotinib ( met overexpression ) , or olaparib if brca2 loh verified pan - her inhibitor olaparib n / a because of missing information erbb2 or erbb3 overexpression fgfr - inhibitor phase i trial ( fgfr3 overexpression ) brca2 mutation ( vus with potential effect ) erbb2 ihc validation and inhibition ( erbb overexpression ) note . 
treatment recommendations as provided by the respective molecular tumor boards for patient 4 tumor board recommendation provided rationale additional recommendation fgfr inhibitor fgfr3 mutation pik3ca inhibitor ( pik3ca mutation ) , combination treatment pik3ca and fgfr inhibitor in phase i trial ( pik3ca and fgfr3 mutation ) clinical trial for pik3ca or fgfr3 mutation pik3ca and fgfr3 mutation if ineligible , off - label everolimus ( pik3ca mutation ) cetuximab and pik3ca inhibitor clinical trial pik3ca or mtor inhibition n / a because of missing information pik3ca mutation pik3ca mutation ( case report ) fgfr inhibitor clinical trial ( fgfr3 mutation ) note . 
rationales were provided for only some of the recommendations and asked for if missing initially . abbreviation : n / a , not available . based on clear diagnostic results , are heterogeneous , especially in the context of complex molecular data . 
this uncertainty was further underlined by the fact that , across most studies , only approximately 20% of patients entering molecular diagnostic programs were reported to receive treatment , despite the identification of potentially targetable alterations in many more patients , as reported by the centers . 
these numbers have been validated recently in a large precision oncology study using comprehensive sequencing data.22 the presence of well - defined genomic aberrations such as braf v600e mutations or the absence of aberrations in known genes could be expected to improve the concordance among centers . 
 yet the discordance among identified targetable alterations , initiated treatments , and treatment effects highlights that most patients discussed at mtbs are found between those more well defined ends of the spectrum , as represented by the sample patients . 
currently , only 1% to 10% of evidence items ( 64 of 5 , 100 and 25 of 477 ) in the clinical interpretations of variants in cancer ( civic ) 23 and oncokb databases24 have us food and drug administrationapproved or standard - of - care evidence level . 
a single - center predefinition of biomarkers as performed in the shiva trial may be unlikely to identify the best treatment option given the amount of heterogeneity among different centers.8 this argument is further supported by positive results from meta - analyses incorporating data from several centers.25 this might be caused by swarm intelligence when considering multiple biomarker - treatment associations . 
however , we believe that the issue of recommendation is more important in the precision medicine context because the biomarker - based choice of treatment is unique to this concept and was expected to be reproducible . in this study , differences were observed on several levels . 
after analyzing the results , we hypothesized that recommendation heterogeneity may have originated from the availability of clinical trials , from shortcomings in the identification of targets , or from differences within the prioritization workflow . 
therefore , it seemed unlikely that the identification of predictive biomarkers was a relevant factor ( even though a jak1 mutation was considered as a predictive biomarker by only one tumor board , in patient 2 )  . 
additional differences were observed regarding the interpretation of vuss , germline variants , potential germline events detected in tumor - only sequencing , and the recommendation of treatments outside of biomarker - driven indications . the provided brca2 vus highlighted differences in the interpretation of unclear variants . 
yet working principles such as the consideration of allele frequencies , vus prediction tools , hierarchies within identified aberrations , structured evidence bases for the identification of biomarker information and prioritization , and the use of evidence levels differed significantly . the interpretation and prioritization of genomic information is not a simple task . 
mutations identified in tumor - only sequencing might sometimes represent a germline event and should therefore be considered for validation.4 information on allele frequency might help in identifying these cases . 
metzeler , serge leyvraz , ulrich keilholz manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors the following represents disclosure information provided by authors of this manuscript . 
 marissa schuh no relationship to disclose christophe le tourneau honoraria : novartis , bristol - myers squibb consulting or advisory role : novartis , celgene research funding : celgene travel , accommodations , expenses : janssen - cilag , celgene consulting or advisory role : amgen , msd , bristolmyers squibb , merck serono , astrazeneca travel , accommodations , expenses : msd , bristol - myers squibb , astrazeneca serge leyvraz consulting or advisory role : loxo consulting or advisory role : loxo travel , accommodations , expenses : ipsen neus bast consulting or advisory role : bristol - myers squibb , nanobiotix mark e . 
metzeler , university hospital , lmu munich , munich , germany ; marissa schuh , markey cancer center , university of kentucky , lexington , ky ; christophe le tourneau , institut curie and inserm u900 research unit , saint - cloud ; christophe le tourneau , institut curie , paris ; christophe le tourneau , versailles - saint - quentin - en - yvelines university , montigny - le - bretonneux , france ; neus bast , vall dhebron institute of oncology , barcelona , spain ; and mark e . 
is a participant in the berlin institute of healthcharit clinical scientist program funded by the charituniversittsmedizin berlin and the berlin institute of health . presented in part at the annual meeting of the european society of medical oncology , madrid , spain , september 8 - 12 , 2017 . support prior presentation references 1 . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular profiling of patients tumors to find potential targets and select treatments for their refractory cancers . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
soria jc , flp a , maciel c , et al : select - 2 : a phase ii , double - blind , randomized , placebocontrolled study to assess the efficacy of selumetinib plus docetaxel as a second - line treatment of patients with advanced or metastatic non - small - cell lung cancer . 
amendola lm , jarvik gp , leo mc , et al : performance of acmg - amp variant - interpretation guidelines among nine laboratories in the clinical sequencing exploratory research consortiu am j hum genet 98 : 1067 - 1076 , 2016 [ erratum : am j hum genet 99 : 247 , 2016 ] 22 . 
massard c , michiels s , fert c , et al : high - throughput genomics and clinical outcome in hardto - treat advanced cancers : results of the moscato 01 trial . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
 precision trial drawer , a computational tool to assist planning of genomics - driven trials in oncology purpose trials that accrue participants on the basis of genetic biomarkers are a powerful means of testing targeted drugs , but they are often complicated by the rarity of the biomarker - positive population . 
however , bigger trials have higher chances of conflicting treatment allocations because of the coexistence of multiple actionable alterations ; allocation strategies greatly affect the efficiency of enrollment and should be carefully planned on the basis of relative mutation frequencies , leveraging information from large sequencing projects . methods we developed software named precision trial drawer ( ptd ) to estimate parameters that are useful for designing precision trials , most importantly , the number of patients needed to molecularly screen ( nnms ) and the allocation rule that maximizes patient accrual on the basis of mutation frequency , systematically assigning patients with conflicting allocations to the drug associated with the rarer mutation . 
we used data from the cancer genome atlas to show their potential in a 10 - arm imaginary trial of multiple cancers on the basis of genetic alterations suggested by the past molecular analysis for personalised therapy ( map ) conference . 
2018 by american society of clinical oncology introduction the availability of sequenced cancer genomes and the generation of new targeted drugs offer unprecedented opportunities for personalized treatment for patients with cancer . 
indeed , treatment within genomic - based clinical trials significantly improves clinical outcome.1 however , identification of the best biomarker - drug combination for patient stratification and treatment remains a critical research and ethical challenge . large multi - institutional projects such as the cancer genome atlas ( tcga ) revealed extreme heterogeneity of cancer mutational landscapes , with a prevalence of low - frequency mutations , giorgio e.m. 
are co - first authors . corresponding author : luca mazzarella , md , phd , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy ; e - mail : luca . 
 including those critical for tumor growth ( driver mutations ) and those that might be targetable by specific drugs ( actionable mutations ) .2 , 3 this scenario renders the conduction of adequately powered genome - based clinical trials prohibitive in many cases : the biomarker - positive population is often rare , and identifying it requires screening large numbers of patients . strategies to circumvent this issue are proposed through novel trial designs in which multiple drugs and / or their matched biomarkers are tested simultaneously . 
these novel designs , usually defined as basket ( one biomarker - drug pair , multiple histologies ) , umbrella ( multiple biomarker - drug pairs , one histology ) , or platform ( multiple biomarker - drug pairs , multiple histologies ) , 4 - 6 may allow reducing the number of patients needed to molecularly screen ( nnms ) to achieve the desired statistical power for multiple treatment subgroups . 
however , these approaches have potential disadvantages : first is the occurrence of a large fraction of patients with potential allocation conflicts resulting from the concomitance of genetic alterations associated with different drugs , 2 and second is the high costs and turnaround time of the molecular screening , which must include sequencing enough genomic space to accommodate the studys need . 
the latter will become more critical in the near future as more complex , polygenic genomic signatures are used as stratification biomarkers ( eg , multiple homologous recombination genes to establish brcaness as a predictor of response to poly [ adp - ribose ] polymerase [ parp ] inhibitors7 )  . 
 for these reasons , patient allocation to individual trial arms significantly deviates from expectations in multigenic umbrella trials , which leads to inadequate statistical power8 , 9 and the inability to reach conclusions . here , we present precision trial drawer ( ptd ) , a comprehensive bioinformatics tool that takes advantage of patient - level genomic information from tcga or alternative sources to simulate genomically characterized cohorts and provide critical parameters for designing genetic biomarker - driven trials . 
df is used to calculate the nnms ( ie , the minimum number of patients that should be tested to obtain the desired sample size as calculated on the expected treatment effect by using conventional power analyses )  . 
 actionable mutations refers to those genetic alterations that dictate a therapeutic choice within the trial . description of the package ptd includes a series of functions in the r programming language to ( 1 ) translate genomic information into genomic coordinates and optimize coordinates for the design of a targeted sequencing panel , ( 2 ) retrieve single or grouped genetic alteration frequencies from public databases ( by default tcga , but other sources can be used ) that maintain patient - level associations , ( 3 ) simulate genomically defined patient cohorts by extracting frequencies of co - occurrence of single or grouped mutations , and ( 4 ) calculate nnms for defined power and / or sample size ( fig 1a )  . 
in our imaginary trial , patients are allocated to 10 possible drugs , including inhibitors of parp , notch , met , her2 , fgfr , egfr , braf , alk , akt , and immune checkpoints , and covering all the allocations linked to the map biomarkers . 
allocation to checkpoint inhibitors was based on the detection of inactivating mutations in mlh or msh genes , regardless of tumor type , which are highly correlated with microsatellite instability , a now - established predictor of immune checkpoint response.11 , 12 ptd was then used to design a dedicated custom targeted sequencing panel , identify the optimal allocation rule , and estimate sample size and statistical power . the list of genomic features associated with each drug is provided in table 1 . 
illustrations of the workflow , the codes used for generating data , and detailed ptd functionalities are available at shinyapp.html. the first step involves designing the sequencing panel , which is imported as a standard excel table with official gene symbols , type and exact alteration to be considered , and two possible grouping variables ( gene - linked drug and , if desired , a generic group of any sort )  . 
 the panel can also be expanded to include genes or genomic positions without therapeutic information , which may nevertheless be relevant for prognostic stratification , prediction of drug toxicity , or a generic biologic interest ( grouped as driver genes in the example )  . four classes of genetic alterations can be explored : single nucleotide variants ( snvs ) , copy number alterations ( cnas ) , translocation - associated fusion transcripts , and gene expression . 
for panels that contain multiple alteration types ( eg , snvs and cnas ) , ptd will construct a reference data set with the intersection of the relative data sets in the source database ( not all patients in tcga have data from all sequencing platforms )  . in projects that allow inclusion of multiple tumor histologies , their frequency of occurrence in the real world is likely to differ significantly from the relative representation in the reference data set , and this can be corrected by ptd by weighting the probability of sample extraction . 
in this example , we used relative frequencies obtained from the national cancer institute seer program ( fig 2a shows the comparison between the tcga and the example populations )  . output the percentage of patients with at least one actionable alteration ( detected fraction ; df ) is probably the most crucial estimate that can be obtained through ptd , which is 65.4% in this example ( fig 2b )  . 
ptd allows breakdown of the df by drug or by disease histology ( fig 2c - d ) or any other prespecified group . to optimize panel design , one can evaluate the trade - off between the feature of interest ( eg , available drugs or the inclusion of genes with uncertain predictive power ) and the size of the genomic space to be sequenced . 
this trade - off can be visualized with a saturationplot that expresses the mean number of alterations per patient or the number of patients with at least x alterations as a cumulative function of the genomic space , with alterations ranked in descending frequency order ( absolute or gene lengthnormalized ; fig 2e )  . 
 the same plot can be obtained by using drugs or other grouping variables ( fig 2f )  . the coocmutexplot indicates the degree of co - occurrence of grouped genetic alterations , ascopubs.org / journal / po jco precision oncology 5 accepted formats . 
for instance , the braf v600e mutation can be coded using amino acid notation ( v600e ) , the single nucleotide polymorphism database ( dbsnp ) identifier ( rs113488022 ) , a set of genomic coordinates ( eg , chr7 : 140753336 140753337 ) , or as genomic variants ( 7 : 140753336 a > c )  . 
mutations of interest can be batch filtered with any set of genomic coordinates to eliminate variants likely to be passengers.3 , 13 in this example , we selected only variants listed as probably pathogenic in the catalogue of somatic mutations in cancer ( cosmic ) database , 14 thus eliminating 33.5% of the initial variants . 
alternatively , individual genes can be visually inspected and edited by using an interactive interface built on the lowmaca ( low frequency mutations analysis via consensus alignment ) algorithm15 ( manual filtering ; fig 1b )  . 
in this example , we manually excluded egfr t790m and pik3ca exon 20 mutations associated with resistance to first - generation egfr inhibitors.16 , 17 specific mutations and / or drugs can be associated with specific tumors and excluded from others . 
 ( b ) percentage of patients with at least one ( detection fraction ) or more actionable alterations ; detection fraction is broken down by ( c ) tumor type or ( d ) drug . 
this plot can be used to decide which drugs should be combined in the same trial because prioritizing those associated with highly mutually exclusive mutations will maximize the biomarker - positive population . power analysis and calculation of the nnms multidrug trials can be powered to test the experimental arm as a whole , ignoring the number of patients allocated to each individual drug , in which case the nnms is a simple linear function of the target sample size divided by the detection power ( in our example , if the given target sample size = n , the nnms will be n / 0.654 ; no allocation rule design )  . 
if this is a desired end point , the trial can be divided into a series of drug - specific subtrials , each having its own target sample size.9 probability of allocation can vary significantly if the associated biomarkers have very different prevalence . 
furthermore , increasing the number of competing arms also increases the likelihood of conflicting allocations ; rules to follow in such cases should be specified in advance to avoid allocation biases . 
immcheckp , immune checkpoint ; inh , inhibitor . general a priori considerations that do not take into account mutation frequencies ( eg , allocation to endocrine therapy only if no mutation is present8 ; manual allocation design )  . 
if information regarding the co - occurrence of mutations is not considered , proper nnms - based sample size calculation is not possible because considering each subtrial independently leads to gross overestimation . 
with ptd , arms can be ranked in order of expected frequency of allocation , so that if a patient bears mutations associated with two drugs , he or she will be systematically assigned to the one with the lowest frequency . 
in nonoptimal designs , allocation does not take into consideration the relative rarity of c , so that when all patients have been allocated , drug z has been allocated to fewer patients than statistically needed . 
 ( c ) comparison of percentages of patients that can be allocated to one or two of the molecular pathway - based subgroups ( real values for shiva and mean values for precision trial drawer [ ptd ] 95% ci are plotted )  . 
 ( d ) power calculations showing numbers needed to sequence for the overall ( bottom panel ) and pathway - specific subgroup trials ( top and middle panels )  . 
cna , copy number alteration ; snv , single nucleotide variant ; tcga , the cancer genome atlas . nnms based on the rule , and simulate patient allocation so that each drug - specific arm reaches at least the desired level of power ( optimal allocation design ; fig 3a )  . 
we can thus precisely quantify the advantage of an optimized umbrella design : for the given example , if one were to run 10 independent one - arm studies with a target sample size of 13 to show a response rate of 40% against historical controls of 10% ( for = .05 and power = 0.8 ) , a total of 4 , 276 patients would need to be sequenced to obtain 130 ( ie , 10 13 ) biomarker - positive patients . 
 the researcher to specify different types of end points ( time to event , progression - free survival , overall survival , time to progression , or proportions such as response rate and survival rate ) , number of arms , allocation ratios ( symmetric or asymmetric ) , and other conventional trial parameters . 
simulation results for oneor twoarm studies with time - to - event or proportion end points and with no , manual , or optimal allocation rules are provided in fig 3b . 
simulation results across a range of powers and target proportions are provided in fig 3c . retrospective evaluation of the shiva trial to test ptd in a real - world scenario , we retrospectively evaluated its ability to correctly predict population composition and treatment allocation in the recent shiva trial , a phase ii randomized trial comparing conventional therapy to multiple targeted agents on the basis of tumor molecular profiling . 
in shiva , 741 patients were subjected to a triad of molecular tests , including sequencing with a targeted enrichment panel ( ampliseq cancer panel , covering 45 tumor - associated genes or mutational hotspots ) , gene copy number analysis by cytoscan hd , and immunohistochemistry for three endocrine receptors . 
although ptd can include information on gene expression in the simulation , we removed endocrine receptors from the analyzed parameters because the correlation between rna - based and immunohistochemistry based quantification of endocrine receptors is poor ( appendix fig a1 )  . 
after data cleanup , 417 of 741 patients were left for analysis ( fig 4a )  . we constructed a ptd panel by using the actionable alterations in shiva and ran 100 trial simulations , extracting tumor histologies from tcga with probabilities equal to their frequencies in shiva and with allocation rules reproducing those adopted in the actual trial . 
alteration frequencies for individual genes were within 95% cis in most cases ( appendix fig a1a - b ) , except for low - frequency genes , for which 95% cis can be expected to be wide . 
consequently , observed versus predicted nnms was also quite similar ( fig 4d ; appendix fig a1d ) , demonstrating that ptd can correctly predict the number of patients needed to be subjected to molecular screening . discussion we report a versatile bioinformatics platform that is based on mutational databases to simulate genetic biomarker - driven clinical trials . 
in a retrospective analysis of the shiva trial , we demonstrated that our tool is able to predict the actual number of patients to be sequenced and has the power to detect overall and arm - specific efficacy signals . 
we believe that our tool will be instrumental in overcoming emerging issues in the design of precision oncology trials . the conceptual framework of precision medicine implies an increased fragmentation of disease entities into distinct subgroups identified by the presence of biomarkers that predict response to targeted agents . 
as previously highlighted by several authors , 6 , 20 for trials aimed at demonstrating efficacy of targeted drugs , 20 more biomarkers means rarer biomarkers , which in turn implies higher and more variable numbers of patients needed to be screened . 
 match screening trial ( targeted therapy directed by genetic testing in treating patients with advanced refractory solid tumors , lymphomas , or multiple myeloma ) , the largest trial of this type to date , an interim analysis after 795 patients were screened showed that only 2.5% of patients could be allocated to seven of the 10 targeted agents on trial.21 the possibility of better predicting accrual rate afforded by ptd would allow trialists to drop inefficient arms and / or modify trial design to maximize patient allocation . an unavoidable limitation of our methodology is that simulations are affected by the prevalence of mutations in available databases , which may not be representative of what is found in study populations . 
instead , most trials with targeted drugs are initially aimed at the metastatic setting , and the mutational profile of metastatic tumors can be significantly different from that of primary tumors . 
an ideal setting for ptd - based simulations with current tcga data may be the neoadjuvant / preoperative setting , which is increasingly used to evaluate novel drugs.23 the availability of clinical metadata , such as tumor size or nodal involvement , can be used to strengthen the representativeness of database samples . finally , some disease tumor types are under represented in mutational databases , which results in high variability and low confidence of corresponding simulations . 
melloni , alessandro guida , giuseppe curigliano , edoardo botteri , ruggero de maria , piergiuseppe pelicci , luca mazzarella financial support : giuseppe curigliano , piergiuseppe pelicci administrative support : giuseppe curigliano provision of study materials or patients : giuseppe curigliano , angela esposito , maud kamal , christoph le tourneau collection and assembly of data : giorgio e.m. 
 edoardo botteri no relationship to disclose angela esposito no relationship to disclose maud kamal no relationship to disclose laura riva employment : philips healthcare ( i ) alberto magi no relationship to disclose ruggero de maria no relationship to disclose christophe le tourneau honoraria : novartis , bristol - myers squibb piergiuseppe pelicci stock and other ownership : genextra consulting or advisory role : amgen , msd , bristolmyers squibb , merck serono , astrazeneca travel , accommodations , expenses : msd , bristol - myers squibb , astrazeneca luca mazzarella no relationship to disclose affiliations giorgio e.m. 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
le tourneau c , delord jp , gonalves a et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
lopez - chavez a , thomas a , rajan a , et al : molecular profiling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
pao w , miller va , politi ka , et al : acquired resistance of lung adenocarcinomas to gefitinib or erlotinib is associated with a second mutation in the egfr kinase domaplos med 2 : e73 , 2005 17 . 
mao c , yang zy , hu xf , et al : pik3ca exon 20 mutations as a potential biomarker for resistance to anti - egfr monoclonal antibodies in kras wild - type metastatic colorectal cancer : a systematic review and meta - analysis . 
the utility of ultra - deep genomic testing to predict and the impact of conditioning intensity to prevent mds relapse are unknown . methods targeted error - corrected dna sequencing was performed on preconditioning blood samples from patients with mds ( n = 48 ) from the blood and marrow transplant clinical trials network 0901 phase iii randomized clinical trial , which compared outcomes by allogeneic hematopoietic cell transplantation conditioning intensity in adult patients with , 5% marrow myeloblasts and no leukemic myeloblasts in blood on morphological analysis at the time of pretransplant assessment . 
clinical end points ( 53 - month median follow - up ) included transplant - related mortality ( trm ) , relapse , relapse - free survival ( rfs ) , and overall survival ( os )  . 
of the 48 patients examined , 14 experienced trm , 23 are relapse - free , and 11 relapsed , of which 7 died . results using a previously described set of 10 gene regions , 42% of patients ( n = 20 ) had mutations detectable before random assignment to reduced intensity conditioning ( ric ) or myeloablative conditioning ( mac )  . 
testing additional genes , including those associated with mds , did not improve prognostication . conclusion this study provides evidence that targeted dna sequencing in patients with mds before transplant can identify those with highest post - transplant relapse rates . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction myelodysplastic syndrome ( mds ) , one of the most common hematologic disorders , is a collection of clinically and genetically heterogeneous diseases . 
 dillon et al context key objective allogeneic hematopoetic cell transplantation ( allohct ) is the only curative therapy for myelodysplastic syndrome ( mds ) but is associated with suboptimal rates of transplant - related mortality ( trm )  . 
using samples from a randomized phase iii clinical trial comparing allohct conditioning intensity in patients with mds , this study examined the prognostic signicance of pretransplant genetic markers on post - transplant outcomes . knowledge generated the presence of mutations within a previously identied set of 10 gene regions before allohct was associated with increased rates of relapse and decreased relapse - free survival in patients with mds who received reduced intensity versus myeloablative conditioning . 
library preparation and pairedend 150 - bp sequencing were performed using unique dualsample indices on an hiseq 2500 ( rapid run mode ; illumina , san diego , ca ) as previously described.10 an average of 43 million paired - end reads were acquired per sample ( data supplement )  . 
details are provided in the data supplement . bioinformatics consensus sequences based on umi read families were mapped to human genome version hg19 ( build grch37 )  . de novo variant calls were made using a minimum allele frequency of 0.001 and were ltered using information regarding umi read families , background error rate models , unique start sites , strand - specic priming , and homopolymer runs . 
alternative approaches were used for insertional mutations in npm1 and flt3 internal tandem duplication . details are provided in the data supplement . statistical analysis kaplan - meier estimation and log - rank test were used for analysis of os and relapse - free survival ( rfs ) and grays test for competing risks of trm and relapse . 
details are provided in the data supplement . results patient cohort a total of 54 patients with mds participated in the bmtctn 0901 clinical trial , of which 48 had blood collected after study enrollment before random assignment to mac ( n = 25 ) or ric ( n = 23 ) conditioning regimens , which was used for genomic analysis in this study . 
this subset of patients was well - matched for baseline characteristics ( table 1 ) , and clinical outcomes were aligned with those previously reported ( data supplement )  . 
ngsg10 mutational status served as a strong predictor of relapse in this cohort of patients with mds , predicting 73% of relapses at 24 months ( 100% for those receiving mac ) , with a specicity of 78% ( 100% for those receiving ric ) ( data supplement )  . to ngsg10 mutational status , no signicant in contrast difference in rates of relapse or os was observed when stratifying patients by disease classication , disease risk group , or cytogenetic prognostic group ( data supplement )  . rates of relapse trended higher in patients with poor cytogenetics or categorized as high risk . 
inclusion of patients with poor cytogenetics before transplant with ngsg10 mutational status improved prediction of relapse at 24 months from 73% to 91% ( data supplement ) and was associated with signicantly higher rates of relapse compared with ngsg10 - negative patients ( data supplement )  . presence of mutations pretransplant predicts relapse by conditioning intensity the impact of conditioning intensity and ngsg10 next , mutational status was examined ( data supplement )  . 
inclusion of patients with poor cytogenetics before transplant with ngsg10 mutational status improved prediction of relapse at 24 months in the ric group to 89% , with a specicity of 89% , and is associated with signicantly increased rates of relapse and decreased rfs compared with patients receiving mac ( data supplement )  . screening for additional genes does not improve test performance the mutational spectrum of mds is complex , with many additional genes recurrently mutated beyond the 10 amlassociated genes described above.7 , 11 , 12 therefore , we expanded our testing to also cover regions in an additional 19 genes including those commonly found in mds at diagnosis ( asxl1 , bcor , cbl , cux1 , dnmt3a , etv6 , ezh2 , gata2 , kras , phf6 , ppm1d , ptpn11 , setbp1 , srsf2 , stag2 , tet2 , u2af1 , wt1 , and zrsr2 )  . 
 ( c ) 10 - gene ngspositive patients had signicantly decreased rfs ( 3 - year rfs , 34% v 71% , p = .006 ) and os ( 3year os , 55% v 79% , p = .045 ) compared with ngs - negative patients . 
the inclusion of dta ( dnmt3a , tet2 , and asxl1 ) genes , known to be associated with age - related clonal hematopoiesis , 13 , 14 resulted in reclassication of 21% ( n = 6 ) of ngsg10negative patients to positive . 
similar to what we observed in patients with aml , 10 samples testing positive for only dta mutations showed no difference in relapse rates or os compared with those testing negative . 
no relapses were observed in patients testing positive only for these 16 genes regardless of conditioning intensity , and only one death was observed ( trm in the mac group )  . 
limiting analysis to those testing positive for an ngsg10 mutation at or above 2.5% vaf reduced the sensitivity at 24 months from 73% to 45% ( data supplement )  . 
overall p values ( in bold ) : grays test for transplant - related mortality and relapse ; log - rank test for rfs and os . abbreviations : ngsg10 , next - generation sequencing 10 - gene ; pos , positive ; neg , negative ; mac , myeloablative conditioning ; ric , reduced intensity conditioning ; rfs , relapse - free survival ; freq , frequency ; os , overall survival ; ci , condence interval . on patient outcomes and found no signicant difference in os based on the mutation number ( data supplement ) or number of mutated genes ( data supplement )  . patients with mds with excess blasts although the requirement for inclusion in the bmt - ctn 0901 study was , 5% marrow myeloblasts and no leukemic myeloblasts in blood on morphological analysis at the time of pretransplant assessment , a total of 22 of the 54 patients with mds ( 41% ) treated on the bmt - ctn 0901 trial had an initial diagnosis of refractory anemia with excess blasts ( raeb ) i or ii ( ie , between 5% and 19% blasts )  . 
seven of these samples tested positive for ngs10g , for which survival was 0% for ric ( n = 2 , relapse ) and 60% for mac - treated patients ( with one death from each relapse and transplantrelated mortality )  . 
ngs10g - positive patients accounted for four of six relapses observed in the raeb cohort , and the other two patients had high - risk cytogenetics with a monosomal karyotype that would not be detectable using this ngs assay . discussion here , we present the impact of genetic mutations detected before random assignment to ric or mac , identied without knowledge of the mutations originally present at diagnosis , on transplant outcomes in patients with mds . 
detection of mutations using a dna - sequencing panel covering regions of 10 genes , previously shown to have utility at the same timepoint in patients with aml , 10 was associated with increased rates of relapse and decreased rfs and os . 
 ( a ) differences in rates of relapse were identied between subgroups dened by conditioning intensity ( ric or mac ) and mutational status ( p , .001 ) , with the highest rate occurring in 10 - gene ngspositive ( ngsg10 - positive ) patients with mds receiving ric . 
the prognostic signicance of the remaining mutations on relapse was dependent on conditioning intensity , with higher rates of relapse and lower rfs observed in patients randomly assigned to receive ric compared with mac . this study provides evidence that the benet of mac versus ric in reducing relapse is found in patients with mds with detectable mutations using a 10 - gene region dnasequencing panel before allohct . 
patients are displayed in columns and grouped by conditioning intensity ( ric or mac ] ) and clinical outcome ( relapse , no relapse , or transplant - related mortality [ trm ] )  . 
genes are displayed in rows and sorted by diagnostic panel groupings , including 10 - gene ( prognostic in aml ) , dta ( associated with age - related clonal hematopoiesis ) , and 16 - gene ( commonly mutated in mds )  . 
although the size of this cohort limits extrapolation , it is possible that the prognostic implications of tp53 mutation detection in patients with mds before allohct and the impact of conditioning intensity differ from those reported previously when those variants are found at a level below the limit of detection of routinely used ngs assays . 
in addition to vaf , other factors such as persistence since initial diagnosis , development during therapy , mutation type , functional classication , and zygosity are likely to be important for determining the relapse risk associated with detecting a tp53 mutation.15 - 22 although mutation detection by targeted dna sequencing before allohct was strongly associated with increased relapse and decreased rfs and these outcomes could be improved with mac , unlike in patients10 with aml , we did not detect an os advantage for conditioning intensication in those testing positive . 
this might have been due to limited sample size , predominately nonrelapse causes of death in this mds cohort ( 67% of deaths , compared with 39% in the previously reported aml cohort ) , or other factors . mds is a genetically heterogenous disease.1 , 11 , 12 , 23 as was observed previously , 8 we found that inclusion of a large number of genes resulted in the majority of patients having mutations present before transplant . 
furthermore , mutations in genes associated with clonal hematopoiesis ( dta ) or 16 other mds - associated genes outside of 10 - gene improve test performance . mutational status did not reanalysis of pretransplant mutational status using only the 10 genes reported here , from another study of patients with mds with , 5% myeloblasts before allohct , 8 conrms our nding of signicantly increased relapse rates in patients testing positive and receiving ric versus mac . 
the modest there are several sample size here offers only a partial sampling of the heterogenous genetics associated with mds , whereas differences in pretransplantation disease burden , biology , and prior treatment history further limit exact comparisons . the signicance of mutation detection before allohct might be inuenced by history of prior treatment , and previous work using the same testing in patients with aml included only those treated to cytomorphological remission before transplant . 
 mds relapse after allohct allohct.9 two randomized studies of conditioning intensity in mds have failed to show a difference in survival between mac and ric , 4 , 6 , 25 although we show here a trend toward improved survival with increased conditioning intensity for those with detectable mutations particularly in the raeb group ( ie , biology and treatment history most analogous to aml )  . 
prior work had shown a benet for increased conditioning intensity in patients with mds with ras pathway mutations ( nras , kras , ptpn11 , cbl , nf1 , rit1 , flt3 , and kit ) undergoing allohct.9 as relapse is not primary cause of death in patients with mds undergoing allohct , the choice of conditioning intensity is currently dependent on the estimated ability of a patient to tolerate transplant - related toxicity.26 allohct remains the only curative therapy for mds ; however , given the median age at diagnosis , many patients will not be eligible for myeloablative approaches.27 , 28 as it is now possible to determine the genomic basis of disease before and after transplantation , personalized approaches for allohct of patients with mds are now conceivable with targeted strategies for those with detectable tp53 , ras pathway ( including flt3 ) , immune augmentation , or other therapies potentially able to supplement the impact of chosen conditioning intensity to minimize relapse risk.29 - 31 idh and jak2 mutations , in conclusion , we show that in adult patients with mds with , 5% marrow myeloblasts and no leukemic myeloblasts in blood before allohct , ultra - deep dna sequencing for mutations in 10 gene regions previously shown to be high risk in patients with aml could identify a subset of 42% of patients who experienced the majority of post - transplant relapses . 
the cibmtr registry is supported primarily by the u24 - ca76518 from nhlbi , nci , and the national institute of allergy and infectious diseases and from hhsh234200637015c ( hrsa / dhhs ) to the center for international blood and marrow transplant research . 
blood 122 : 2943 - 2964 , 2013 luger sm , ringden o , zhang mj , et al : similar outcomes using myeloablative vs reduced - intensity allogeneic transplant preparative regimens for aml or mds . bone marrow transpl 47 : 203 - 211 , 2012 shimoni a , hardan i , shem - tov n , et al : allogeneic hematopoietic stem - cell transplantation in aml and mds using myeloablative versus reduced - intensity conditioning : the role of dose intensity . 
leukemia 20 : 322 - 328 , 2006 kroger n , iacobelli s , franke gn , et al : dose - reduced versus standard conditioning followed by allogeneic stem - cell transplantation for patients with myelodysplastic syndrome : a prospective randomized phase iii study of the ebmt ( ricmac trial )  . 
j clin oncol 35 : 2157 - 2164 , 2017 pulsipher ma : reduced intensity for myelodysplastic syndrome : worth the gamble ? j clin oncol 35 : 2106 - 2108 , 2017 scott bl , pasquini mc , logan br , et al : myeloablative versus reduced - intensity hematopoietic cell transplantation for acute myeloid leukemia and myelodysplastic syndromes . 
j clin oncol 35 : 1154 - 1161 , 2017 bejar r , stevenson ke , caughey b , et al : somatic mutations predict poor outcome in patients with myelodysplastic syndrome after hematopoietic stem - cell transplantation . 
n engl j med 379 : 1028 - 1041 , 2018 lindsley rc , saber w , mar bg , et al : prognostic mutations in myelodysplastic syndrome after stem - cell transplantation . 
n engl j med 371 : 2477 - 2487 , jaiswal s , fontanillas p , flannick j , et al : age - related clonal hematopoiesis associated with adverse outcomes . 
montalban - bravo g , kanagal - shamanna r , benton cb , et al : genomic context and tp53 allele frequency dene clinical outcomes in tp53 - mutated 16 . 
coombs cc , zehir a , devlin sm , et al : therapy - related clonal hematopoiesis in patients with non - hematologic cancers is common and associated with adverse 18 . 
al - kali a , zblewski d , foran jm , et al : outcome of myelodysplastic syndromes over time in the united states : a national cancer data base study from 20042013 . 
sorror ml , sandmaier bm , storer be , et al : long - term outcomes among older patients following nonmyeloablative conditioning and allogeneic hematopoietic cell transplantation for advanced hematologic malignancies . 
maslah n , salomao n , drevon l , et al : synergistic effects of prima - 1met ( apr - 246 ) and azacitidine in tp53 - mutated myelodysplastic syndromes and acute myeloid leukemia . 
wei , md1 cdk12 is a kinase that regulates several key cellular processes , including transcription and maintenance of genomic stability.1 the prevalence of cdk12 alterations is higher in metastatic castration - resistant prostate cancer ( mcrpc ; 7% ) compared with primary prostate cancer ( 1% ) , which indicates an association with an aggressive phenotype.2 in the articles accompanying this editorial in jco precision oncology , schweizer et al3 and antonarakis et al4 report on the clinical features and outcomes of patients with cdk12 - altered prostate cancer in two independent retrospective multicenter series . 
in both studies , the source of tumor dna included primary prostate , metastatic sites , and circulating tumor dna sequenced for cdk12 alteration status through a variety of commercial and inhouse sequencing platforms . schweizer et al3 identied 52 patients who harbored cdk12 mutations , and antonarakis et al4 identied 60 . in both studies , there was a roughly even split incidence of monoallelic or biallelic cdk12 inactivation . because of limitations in the diverse sequencing platforms used , neither series required biallelic mutations . 
in the schweizer series , median time from initiation of androgen deprivation therapy ( adt ) to development of crpc was 1.4 years , and in the antonarakis series , median progression - free survival ( pfs ) after initiation of adt was 12.3 months , which indicates short responses to primary adt . 
median overall survival ( os ) from time of metastasis was 3.9 years in the schweizer series , and median os from initiation of adt was 40.8 months in the antonarakis data set , which suggests poor prognosis . 
in the schweizer cohort , the unconrmed 50% prostate - specic antigen decline ( psa50 ) response rate to rst - line abiraterone and enzalutamide for crpc was approximately 70% ; however , median pfs was short at approximately 9 months . 
first , antonarakis et al required a conrmatory psa at least 4 weeks after the initial psa50 response , which was not required in the schweizer series and likely contributed to the lower psa response rate in the antonarakis study . 
de novo metastatic presentation is a poor prognostic factor that likely contributed to the shorter pfs with rst - line abiraterone and enzalutamide in the antonarakis study . these data are consistent with another recently published retrospective series by reimers et al5 that included 46 patients with advanced prostate cancer with cdk12 mutations . 
of note , the patients with cdk12 loss - of - function alterations had worse clinical outcomes compared with those with other mutations , including atm , brca1 / 2 , and tp53 . 
taken together , all three studies have consistently shown that cdk12 alterations portend aggressive clinical features and relative resistance to second - generation androgen signaling inhibitors . while the antonarakis and schweizer series represent the largest cdk12 - altered cohorts to date , they are both limited by their retrospective nature . 
clinical assessments were variable and not standardized , and there were no comparisons of cdk12 alteration with other genomically dened cohorts ( as in the reimers et al5 study )  . 
regardless , the authors should be commended for assembling these large data sets that help to inform on the prognostic implications of cdk12 - mutated prostate cancer . furthermore , these series include the largest cohort to date of outcomes in cdk12 - mutated prostate cancer after immune checkpoint blockade , shedding light on its predictive potential . 
two phase iii , randomized , placebocontrolled trials of ipilimumab in the postdocetaxel and predocetaxel mcrpc settings failed to meet their primary end point of os.6 , 7 pembrolizumab alone in mcrpc leads to low rates of either psa or radiographic response.8 while the prevalence of mismatch repair ( mmr ) deciency in crpc is low ( , 5% ) , 9 deciencies in mmr proteins are associated with higher psa and objective responses to pd - 1 / pd - l1 inhibitors.10 the response rate to pd - 1 / pd - l1 inhibitors in crpc is higher than the prevalence of mmr deciency , and some patients achieve responses without harboring mmr - decient tumors , which suggests that there are other currently undetermined biomarkers of clinical benet . cdk12 biallelic inactivating mutations lead to the formation of ftd , which results in increased prevalence of gene fusions , elevated antigen load , and inltration of t cells into the tumor microenvironment.2 these ndings suggest that tumors that harbor cdk12 loss may be immunogenic and susceptible to immunotherapy . in a small cohort of 4 pretreated patients with cdk12 - mutant mcrpc treated with an anti - pd - 1 immune checkpoint inhibitor , 2 experienced a marked psa decline.2 this suggests the potential of cdk12 as a predictive biomarker for immunotherapy , a hypothesis that can be scrutinized further with new data from the schweizer and antonarakis series . in the antonarakis series , 9 heavily pretreated men with mcrpc received a pd - 1 inhibitor , of whom 3 ( 33% ) achieved a conrmed psa50 response . 
in the schweizer series , 19 patients received diverse immunotherapy regimens , including pembrolizumab , atezolizumab , nivolumab and ipilimumab , durvalumab and tremelimumab , and atezolizumab and radium - 223 . 
objective responses were not assessed in this series . heterogeneity in patient population , prior therapies , and treatment regimens likely account for the differences in clinical outcomes to immune checkpoint inhibitors observed in these two studies . 
furthermore , the rate of objective responses and duration of disease control remain unclear . ultimately , prospective data are needed to further dene the role of cdk12 as a potential biomarker to predict response and benet to immune checkpoint inhibitors in advanced prostate cancer . 
toward this end , multiple prospective clinical trials are currently under way to explore outcomes to immune checkpoint inhibition in patients with prostate cancer who harbor cdk12 alterations or other dna damage repair defects ( table 1 )  . 
of note , these studies are prospectively enriching for genomic alterations of interest and cover a spectrum of disease states , including biochemically recurrent prostate cancer , metastatic hormone - sensitive prostate cancer , and mcrpc . 
for example , cdk12 loss is associated with amplication of cell cycle genes ccn1 and cdk4 , which suggests that cdk12 - mutated tumors may be susceptible to cdk4 / 6 inhibition.11 the combination of atezolizumab and abemaciclib is being studied in cdk12 - altered mcrpc ( clinicaltrials.gov identier : nct04272645 )  . optimal patient selection using clinical and genomic / molecular characteristics along with effective combination strategies are likely to move the needle for immunotherapy strategies in prostate cancer . 
despite the limitations of retrospective analysis , these data with rich clinical annotation suggest that patients with prostate cancer with cdk12 mutations have a poor prognosis and that novel therapies are needed . 
wei honoraria : onclive research funding : bristol - myers squibb travel , accommodations , expenses : corvus pharmaceuticals no other potential conicts of interest were reported . references blazek d , kohoutek j , bartholomeeusen k , et al : the cyclin k / cdk12 complex maintains genomic stability via regulation of expression of dna damage response genes . 
cell 173 : 1770 - 1782.e14 , 2018 schweizer mt , ha g , gulati r , et al : cdk12 - mutated prostate cancer : clinical outcomes with standard therapies and immune checkpoint blockade . 
eur urol 77 : 333 - 341 , 2020 kwon ed , drake cg , scher hi , et al : ipilimumab versus placebo after radiotherapy in patients with metastatic castration - resistant prostate cancer that had progressed after docetaxel chemotherapy ( ca184 - 043 ) : a multicentre , randomised , double - blind , phase 3 trial . 
lancet oncol 15 : 700 - 712 , 2014 beer tm , kwon ed , drake cg , et al : randomized , double - blind , phase iii trial of ipilimumab versus placebo in asymptomatic or minimally symptomatic patients with metastatic chemotherapy - naive castration - resistant prostate cancer . 
j clin oncol 38 : 395 - 405 , 2020 abida w , cheng ml , armenia j , et al : analysis of the prevalence of microsatellite instability in prostate cancer and response to immune checkpoint blockade . jama oncol 5 : 471 - 478 , 2019 10 . 
agarwal n , loriot y , mcgregor ba , et al : cabozantinib ( c ) in combination with atezolizumab ( a ) in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) : results of cohort 6 of the cosmic - 021 study . 
because poly ( adp - ribose ) polymerase inhibitors have significant activity in brca1 / 2 - mutant ovarian and breast cancers , rucapanc investigated the efficacy and safety of rucaparib in brca1 / 2 - mutant pancreatic cancer . patients and methods rucapanc enrolled patients with measurable locally advanced / metastatic pancreatic cancer who had received one to two prior chemotherapy regimens . 
four patients achieved a response ; two partial responses and one complete response ( cr ) were confirmed ( objective response rate , 15.8% ; 3 of 19 ) , with an additional cr unconfirmed . 
the disease control rate ( cr , partial response , or stable disease for 12 weeks ) was 31.6% ( 6 of 19 ) in all patients and 44.4% ( 4 of 9 ) in those who had received one prior chemotherapy regimen . 
these mutations are predicted to lead to the reversion of a somatic not germlinemutation . conclusion rucaparib provided clinical benefit to patients with advanced pancreatic cancer and a brca1 / 2 mutation , and demonstrated an acceptable safety profile . 
2018 by american society of clinical oncology introduction pancreatic cancer ( pc ) is projected to become the second leading cause of cancer death by 2020.1 the majority of pcs are diagnosed at an advanced stage , precluding a surgical , curative approach . 
in the setting of advanced disease , folfirinox treatment ( folinic acid [ leucovorin ] , fluorouracil , irinotecan , and oxaliplatin ) and gemcitabine in combination with nab - paclitaxel are the standards of care , with both demonstrating an improvement in overall survival compared with gemcitabine alone.2 , 3 in the second - line setting , prospective data have shown modest results , with response rates to chemotherapy generally less than 20% , 4 including second - line folfirinox or fluorouracil with nanoliposomal irinotecan.4 - 8 additional therapeutic options are needed . approximately 9% of unselected pcs are associated with a germline or somatic mutation in brca1 or brca2 ( brca1 / 2 ) .9 , 10 cells with a deleterious brca1 / 2 mutation and resultant homologous recombination deficiency are unable to repair dna double - strand breaks reliably11 , 12 and are thus sensitive to poly ( adp - ribose ) polymerase ( parp ) inhibition.13 - 16 studies have demonstrated clinical benefit with parp inhibitors in clinical trials of germline brca1 / 2 mutant breast and ovarian cancer . 
the study design was approved by the independent review board at each participating site and was conducted according to the provisions of the declaration of helsinki and the good clinical practice guidelines of the international conference on harmonization of technical requirements for registration of pharmaceuticals for human use . 
all patients provided written informed consent before participating in the trial . enrolled patients were men and women at least 18 years of age with histologically confirmed locally advanced or metastatic pancreatic adenocarcinoma with measureable disease and a known deleterious germline or somatic brca1 / 2 mutation by local testing . 
patients could have received up to two prior lines of chemotherapy in the locally advanced / metastatic setting , but could not have received prior therapy with a parp inhibitor . 
to infer loss of heterozygosity ( loh ) , the log - ratio profile of sequencing data was segmented , and the allele frequencies of sequenced genome - wide single nucleotide polymorphisms were used to estimate the copy and minor allele frequency for each segment . 
pretreatment plasma specimens were collected on day 1 of cycle 1 for circulating tumor dna ( ctdna ) analysis by foundation medicine , which is a hybrid capture - based next - generation sequencing assay that sequences the coding regions of 62 cancer - related genes , including brca1 / 2 . 
safety results were reported by analysis of adverse events ( aes ) and graded according to the common terminology criteria for adverse events ( version 4 )  . the safety analysis included all patients who received at least one dose of rucaparib . 
for inclusion in the objective response rate ( orr ) , a complete response ( cr ) or partial response ( pr ) per recist had to have been confirmed at least 28 days after the initial response was observed . 
the median age was 57 ( range , 41 to 75 ) years , 57.9% of patients ( 11 of 19 ) were male , the median number of prior chemotherapy regimens for locally advanced / metastatic disease ( excludes adjuvant treatment where progression occurred > 6 months after completion of treatment ) was two ( range , 1 to 3 ) , 78.9% of patients ( 15 of 19 ) had an eastern cooperative oncology group performance status of 1 , and 78.9% ( 15 of 19 ) had a brca2 mutation . 
as prespecified in the protocol , enrollment was stopped because of lack of responses in the first 15 patients evaluated ; the three confirmed responses occurred in the last four patients enrolled . after study closure , one patient continued therapy on an individual patient ind application . 
thirteen patients discontinued the study because of radiologic or clinical progression , two discontinued therapy within a week of beginning ( one because of investigator decision , the other for an unknown reason ) , one discontinued because of aes with simultaneous radiologic progression confirmed at the end of treatment , one discontinued because of an ae with ongoing sd , and one withdrew consent with an ongoing pr . 
patients received rucaparib for a median of 57 days in the study ( range , 2 to 504 days )  . brca1 and brca2 mutation status sixteen of 19 patients had a germline brca1 / 2 mutation . 
of the 16 tumors associated with a germline mutation , paired somatic sequencing was available in eight ; the allelic frequency of the known germline mutant allele was between 41% and 53% . 
this was counted as three separate chemotherapy treatment regimens per the protocol - specified criteria . circulating tumor dna samples for ctdna analyses at cycle 1 , day 1 ( before treatment with rucaparib ) were available for 16 patients , and somatic mutations were detected in 11 patients ( 10 of whom had kras mutations ; appendix table a1 )  . 
investigator - assessed responses ( recist ) in patients with pancreatic cancer and a brca mutation ( n = 19 ) unconfirmed cr / confirmed sd response not evaluable confirmed response rate ( cr or pr ) confirmed response rate ( cr or pr ) in patients with only one prior chemotherapy for locally advanced / metastatic disease disease control rate ( cr , pr , or sd 12 weeks ) all patients patients with only one prior chemotherapy regimen for locally advanced / metastatic disease no . 
in the first patient ( patient 5 ) , ctdna analysis detected the germline brca2 mutation c.7060c > t ( allele frequency , 48% ) , the somatic alteration c.1499_1499delg ( allele frequency , 22% ) , and the secondary somatic mutation c.1416_1420delgcatc ( allele frequency , 19% ) that restored the open reading frame of the brca2 gene . 
in the second patient ( patient 14 ) , ctdna analysis detected the germline brca2 mutation c.5946deit ( allele frequency , 46% ) , the somatic alteration c.1387dela ( allele frequency , 13% ) , and the secondary somatic mutation c.1355_1380deltaccaaaatcagagaagccattaaat , which also restored the open reading frame , but seemed to be subclonal ( with an allelic frequency of only 1% )  . 
this patient , who had also previously received folfirinox , developed significant clinical progression at day 18 , although target lesions were stable . assessment of allele - specific loh tumor was available for analysis in 10 patients . 
 rucaparib treatment stable disease complete response progressive disease partial response progressive disease reported on last day of treatment < 1 weekd patient of prior regimens received prior platinum platinum refractory brca mutation brca2 somatic brca1 germline brca2 germline brca1 germline brca2 germline brca2 germline brca1 germline brca2 germline brca2 germline brca1 germline brca2 germline brca2 germlineg brca2 germline brca2 germline brca2 germline brca2 germline brca2 germline brca2 somatic brca2 somatic sd 72 weeks sd 20 weeks sd 24 weeks pr 36 weeks pr 25 weeks cr 19 weeks pr 5 weeksi cycle fig 2 . 
 ( f ) patient discontinued because of adverse events ( aes ; grade 3 fatigue and grade 4 thrombocytopenia ) ; best response of stable disease ( sd ) was ongoing after the last day of treatment . 
the second patient had a somatic brca2 mutation ( c.1748t > a ) and had a cr as best response ( patient 19 )  . safety all patients had at least one treatment - emergent ae ( table 3 )  . 
two other patients died as a result of disease progression . discussion this study tested the efficacy of a single - agent parp inhibitor , rucaparib , in patients with advanced pc with a known deleterious brca1 / 2 mutation . 
adverse events were graded according to the national cancer institutes common terminology criteria for adverse events ( version 4 )  . * includes adverse events of thrombocytopenia and decreased platelet count . with a confirmed orr of 16% and an observed disease control rate of 32% . 
our findings suggest that there may be a role for parp inhibition in patients with a brca1 / 2 mutation , particularly in those whose disease has not progressed while taking prior platinum therapy . although this was a single - arm study , making comparisons to other agents difficult , the clinical relevance of our results merits comparison with other current standards of care for this patient population . 
 importantly , the only approved chemotherapy combination in the second - line setting , fluorouracil with nanoliposomal irinotecan , had an overall response rate of 7.7% in the pivotal registration study.8 other small single - center studies investigating folfirinox or other chemotherapy combinations in a refractory population show similarly low response rates , reflecting the known chemoresistance of this disease . 
 furthermore , as treatment options improve for pc , patients are even able to move beyond second - line therapy , for which there are no standard of care options . 
this underscores the importance of looking outside of chemotherapy options , particularly in patients with potentially targetable mutations . previous small studies investigating parp inhibition in brca - mutated pc have shown similar efficacy . 
the response rate of single - agent olaparib in patients with metastatic pc harboring a germline brca1 / 2 mutation who had received prior chemotherapy was 22%.20 a phase ii study of veliparib alone in 16 previously treated patients with brca - mutated pc demonstrated single - agent activity , with 25% of patients having sd for at least 4 months . 
analysis is ongoing to understand the role platinum sensitivity played in these four patients.21 when considered with the prior studies , these trials should provide insight into the clinical utility of single - agent parp inhibition in patients with pc and a known brca1 / 2 mutation . in this study , responses to rucaparib were seen in individuals harboring a germline or somatic brca1 / 2 mutation . 
because of significant stromal infiltration in pc , assessing allele frequency of somatic tumor alterations may be challenging . none of the four patients with a confirmed or unconfirmed response had experienced disease progression on prior platinum therapy ( one had never received platinum ) , and three of the four patients had only received one prior chemotherapy regimen for locally advanced or metastatic disease . 
this finding highlights the important question of the role of platinum sensitivity in the setting of advanced / metastatic pc and underscores a potential role for rucaparib as a treatment for patients whose tumors are not platinum refractory . 
similar findings were noted in patients with advanced ovarian cancer treated with olaparib , because the highest response rates were noted in patients who were deemed platinum sensitive rather than resistant or refractory.22 this will need to be investigated in a larger clinical study . 
 secondary mutations that likely confer resistance have been observed in patients with ovarian or prostate cancer who harbor a brca1 / 2 mutation and whose disease has progressed while receiving platinum chemotherapy or parp inhibitors ; however , these reports have demonstrated reversion mutations that have restored the open reading frame in the vicinity of the germline mutation . 
the majority ( but not all ) of brca1 / 2 - mutant breast and ovarian cancers have allele - specific loh23 ; however , the loss of the second allele is most commonly due to copy neutral loh and rarely due to a somatic mutation . 
both of these patients had previously been treated with oxaliplat several studies have demonstrated the presence of reversion mutations in patients previously treated with chemotherapy , particularly platinum based.24 - 27 our study has several limitations , including a small sample size and lack of corresponding somatic sequencing and ctdna analysis for some patients . rucaparib is a well - tolerated parp inhibitor that could be considered in patients with advanced pc with known brca1 / 2 mutations who have received prior chemotherapy . 
domchek research funding : prism biolab ( inst ) , genentech ( inst ) , novartis ( inst ) , newlink genetics ( inst ) , eli lilly ( inst ) , aduro biotech ( inst ) , pfizer ( inst ) , sanofi ( inst ) data analysis and interpretation : rachna t . 
shroff consulting or advisory role : celgene , codiak biosciences , agios , halozyme travel , accommodations , expenses : astrazeneca ravit geva honoraria : bristol - myers squibb , msd , eli lilly , medison , roche , novartis , janssen , pfizer , teva travel , accommodations , expenses : bristol - myers squibb , roche ron epelbaum no relationship to disclose lindsey rolfe employment : clovis oncology leadership : clovis oncology stock and other ownership interests : clovis oncology , celgene , biomarin travel , accommodations , expenses : clovis oncology sandra goble employment : clovis oncology stock and other ownership interests : clovis oncology research funding : eli lilly , celgene , agios , halozyme travel , accommodations , expenses : celgene , codiak biosciences , agios , halozyme kevin k . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb heidi giordano employment : clovis oncology stock and other ownership interests : clovis oncology acknowledgment research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) robert h . 
vonderheide honoraria : genentech , celgene consulting or advisory role : eli lilly , celldex research funding : eli lilly ( inst ) the authors thank lawrence leichman for his helpful input while the study was being designed . 
shroff , the university of texas md anderson cancer center , houston , tx ; andrew hendifar , cedars - sinai medical center , los angeles , ca ; robert r . 
mcwilliams , mayo clinic , rochester , mn ; ravit geva , tel aviv university , tel aviv ; ron epelbaum , rambam health care campus , haifa , israel ; lindsey rolfe , sandra goble , kevin k . 
rahib l , smith bd , aizenberg r , et al : projecting cancer incidence and deaths to 2030 : the unexpected burden of thyroid , liver , and pancreas cancers in the united states . 
assaf e , verlinde - carvalho m , delbaldo c , et al : 5 - fluorouracil / leucovorin combined with irinotecan and oxaliplatin ( folfirinox ) as second - line chemotherapy in patients with metastatic pancreatic adenocarcinoma . 
lee mg , lee sh , lee sj , et al : 5 - fluorouracil / leucovorin combined with irinotecan and oxaliplatin ( folfirinox ) as second - line chemotherapy in patients with advanced pancreatic cancer who have progressed on gemcitabine - based therapy . 
nagrial am , chin vt , sjoquist km , et al : second - line treatment in inoperable pancreatic adenocarcinoma : a systematic review and synthesis of all clinical trials . 
wang - gillam a , li cp , bodoky g , et al : nanoliposomal irinotecan with fluorouracil and folinic acid in metastatic pancreatic cancer after previous gemcitabine - based therapy ( napoli - 1 ) : a global , randomised , open - label , phase 3 trial . 
kristeleit r , shapiro gi , burris ha , et al : a phase i - ii study of the oral parp inhibitor rucaparib in patients with germline brca1 / 2 - mutated ovarian carcinoma or other solid tumors . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
lowery ma , kelsen dp , smith sc , et al : phase ii trial of veliparib ( v ) in patients ( pts ) with previously treated brca or palb2 - mutated ( mut ) pancreas adenocarcinoma ( pc )  . 
domchek sm , aghajanian c , shapira - frommer r , et al : efficacy and safety of olaparib monotherapy in germline brca1 / 2 mutation carriers with advanced ovarian cancer and three or more lines of prior therapy . 
afghahi a , timms km , vinayak s , et al : tumor brca1 reversion mutation arising during neoadjuvant platinum - based chemotherapy in triple - negative breast cancer is associated with therapy resistance . 
weigelt b , comino - mndez i , de bruijn i , et al : diverse brca1 and brca2 reversion mutations in circulating cell - free dna of therapy - resistant breast or ovarian cancer . 
schrock , phd4 ; giovanni randon , md1 ; sandra romero - cordoba , phd1 , 5 ; daniele rossini , md6 , 7 ; giovanni fuc `a , md1 ; jeffrey s . 
ross , md4 , 8 ; daisuke kotani , md9 ; russell madison , phd4 ; seung tae kim , md10 ; lisa salvatore , md11 ; alessandra raimondi , md1 ; filippo pagani , md1 ; beatrice borelli , md6 , 7 ; federica perrone1 ; maria di bartolomeo , md1 ; vincent a . 
clinical data were available for 27 at - raspositive and 467 negative cases from the italian collaboration , memorial sloan kettering cancer center , samsung medical center , and the breac study . results at - ras mutations were identied in 163 ( 0.9% ) of 18 , 270 mcrcs . 
pole exonuclease domain mutations had higher frequency ( 7% ) than expected and were found only in microsatellite - stable tumors with high tumor mutational burden ( tmb )  . 
on the basis of these ndings , the use of anti - egfr monoclonal antibodies cetuximab and panitumumab in metastatic colorectal cancer ( mcrc ) is now restricted to patients with ras wild - type tumors . several studies also showed that patients with rasmutated mcrc have poorer survival as compared with those with ras wild - type disease , also when treated with bevacizumab - containing rst - line regimens.5 hotspot mutations affecting codons other than 12 , 13 , 59 , 61 , 117 , and 146 account for a small subset of ras mutations . 
a retrospective , next - generation sequencing ( ngs ) based study of 177 patients6 showed that up to 2.8% of mcrcs bear atypical ras ( at - ras ) alterations . 
 pietrantonio et al context key objective to provide molecular and clinical characterization of atypical ras mutations ( ie , those occurring outside major hotspots in codon 12 , 13 , 59 , 61 , 117 , and 146 ) in metastatic colorectal cancer . knowledge generated we provide the rst evidence , to our knowledge , that the prognostic role of atypical ras mutations is superimposable to that of typical ras and that tumors bearing these alterations are characterized by a high prevalence of pole exonuclease domain mutations and high tumor mutational burden . relevance our results suggest the clinical meaning of atypical ras mutations as markers of activation of ras pathway and highlight the potential clinical relevance of testing at - rasmutated tumors for the presence of pole exonuclease domain mutations to identify a niche of patients who may be candidates for immunotherapy approaches . reveal mutations otherwise missed by hotspot - targeted realtime polymerase chain reaction or multiplex - hotspot maldi - tof technologies , which are included in recommendations by current guidelines.7 because of the widespread use of ngs and other comprehensive genomic proling techniques that allow sequencing of the entire coding regions of ras genes , at - ras mutations are being detected with increasing frequency . 
extended ras sequencing data for each screening platform are detailed in the data supplement . we were able to retrieve complete clinical data for 33 patients with at - rasmutated mcrc , and we compared them with a cohort of 467 at - rasnegative cases retrieved by the italian institutions and the breac study in terms of baseline characteristics and overall survival ( os )  . 
six patients were excluded because of the co - occurrence of typical ras or braf v600e mutations in their specimens . extended molecular data were available for patients from the memorial sloan kettering cancer center database and the foundation medicine database . 
functional at - ras mutation characterization , namely mapk pathway activation compared with ras wild - type status , was reported according to loree et al.9 mutational frequency of recurrently mutated genes was compared with historical data reported by yaeger et al10 in the setting of mcrc . 
the study was approved by the fondazione irccs istituto nazionale dei tumori di milano institutional review board ( study id : int 117 / 15 ) and conducted according to the ethical principles for medical research involving human subjects adopted in the declaration of helsinki . 
these included sex , age , eastern cooperative oncology group performance status , primary tumor location ( rightv left - sided ) , mucinous histology , primary tumor resection , time to metastases ( synchronous v metachronous ) , number of metastatic sites ( one v more than one ) , and microsatellite instability ( msi ) status . assessment of primary resistance to anti - egfr treatment to assess primary resistance to anti - egfr antibody therapies , we evaluated the response to anti - egfrs for patients with tumors bearing any at - ras mutation but no co - occurring typical ras or braf mutations . 
only patients receiving cetuximab or panitumumab monotherapy , or in combination with irinotecan if previous irinotecan refractoriness was clearly demonstrated , were included , as previously described.11 molecular analyses the type of at - ras mutations , the presence of nonsilent mutations , and comutated genes were analyzed for each case . 
this comprehensive analysis can overcome numerous biases that confound the analyses to nd driver mutations from the passenger ones . statistical analysis the fishers exact test , v2 test , or mann - whitney test were used when appropriate to assess the associations of at - ras mutations with investigated characteristics . 
we investigated the impact of at - ras mutations on os , dened as the time from diagnosis of metastatic disease to death or last followup for patients who were alive . 
the association of at - ras mutations and clinicopathological characteristics with os was assessed in univariate analyses , and a multivariable cox proportional hazard model was built , including as covariates variables associated with survival with a p value , .10 in the univariate analyses . 
 pietrantonio et al results clinicopathological and molecular features of patients bearing at - rasmutated mcrc as listed in table 1 , when focusing on the 27 patients with mcrc with clinical information available and isolated atras mutations , this population was not signicantly associated with any specic clinical or pathologic feature , as compared with braf , typical ras , or ras / braf wild - type subgroups . 
the list of specic at - ras mutations with functional characterization , co - occurring typical ras / braf v600 mutations , and msi status is detailed in the data supplement . in the foundation medicine ( from august 2012 to january 2018 ) and memorial sloan kettering cancer center ( from january 2014 to january 2018 ) data sets , 142 and 21 cases with at - ras mutations were retrieved out of a total of 16 , 324 and 1 , 946 mcrc samples analyzed from unique patients , respectively , with an overall incidence of 0.9%. a total of 56 unique at - ras mutations were detected ( fig 2a ) , of which 30 kras and three nras were known oncogenic missense mutations or indels as dened by the oncokb database . 
overall , at - kras and - nras mutations occur primarily in the gtpase domain and consequently may affect the ability of ras gtpase - activating proteins , such as nf1 , to bind ras and regulate its signaling ( data supplement )  . 
in our data set , a specic at - ras mutation could be possibly recognized as driver in 76% of cases , suggesting a functional effect of a subset of at - ras alterations in mcrc tumorigenesis . 
in 24% of cases with at - ras mutations possibly recognized as passengers , we then explored the cooccurrence with other mutational events to dene possible cooperative mechanisms involved in tumor growth . some unique frequently comutated genes with at - ras passenger mutations were involved in critical tumorigenic pathways such as mapk , atm , and ras positive regulation of phosphorylation signaling ( data supplement )  . recurrently mutated genes identied by ngs for memorial sloan kettering cancer center database and foundations medicine database patient screening sources ( n = 163 ) are outlined in the data supplement . 
regarding msi status from 133 at - ras tumors including most with available data , 8% of tumors were classied as msihigh ( msi - h ) and 92% as mss , in agreement with the frequency observed in typical ras - mutated tumors10 ( n = 354 ; msi - h , 11% ; mss , 89% )  . 
furthermore , typical ras and / or braf v600e mutations were more common in the tmb - high group ( 43% ) than in tmb low ( 28% )  . 
patient characteristics according to the presence of at - ras , braf , and typical ras mutations and ras / braf wild - type status at - ras mutated ( n = 27 ) braf mutated ( n = 17 ) ras mutated ( n = 176 ) ras / braf wild - type ( n = 274 ) characteristics female male age , years median ecog performance status primary tumor location right colon left colon rectum mucinous histology primary tumor resection time to metastases synchronous metachronous no . 
summary of mutagenesis and molecular features associated with atypical ras mutations in patients with extensive next - generation sequencing ( ngs ) data from screening sources of memorial sloan kettering cancer center database and foundation medicine database including 163 patients . ( a ) at - ras mutations oncoplot . 
the upper bar plot indicates the number of mutations per sample , and the right bar plot describes the mutational frequency among the overall population , indicating the variant classication by colors . 
kaplan - meier curves for overall survival ( os ) according to ras , atypical ras ( at - ras ) , and braf v600e mutational ( mut ) status . 
hr , hazard ratio ; na , non - assessable ; ref , reference . the primary resistance cohort ( data supplement ; table 3 )  . one patient experienced a partial response to panitumumab monotherapy , two patients had stable disease lasting less than 6 months , and three patients had progressive disease . 
all samples were assessed using the primary resistance in ras and braf wild - type metastatic colorectal cancer patients treated with anti - egfr monoclonal antibodies ( pressing ) panel , 11 which groups together several genomic alterations associated with anti - egfr primary resistance beyond ras and braf mutations . 
none of the resistant patients with at - ras mutations and primary resistance showed a concomitant genomic alteration known to be associated with anti - egfr primary resistance . discussion recent advances in the depiction of the molecular landscape of mcrc provides evidence for the potential impact of several biomarkers other than ras and braf mutational status and msi status for improving the clinical management of affected patients . 
here we focus on atras mutations to identify the similarities and differences of cases with at - ras versus those with typical ras mutations and their independent weight on patients outcomes . although we found that at - ras mutations are not associated with specic clinicopathological characteristics in mcrc , the prognostic role of isolated at - ras mutations typical ras seems highly superimposable with that of mutations , with a worse prognosis when compared with ras and braf v600e wild type and a clearly better outcome than the braf v600e mutant subgroup . 
supporting this , in a preliminary report loree et al9 functionally characterized a wide set of at - ras mutations by means of an ectopic expression assay , and although the median mapk activity of at - ras mutations was lower than that of typical ras mutations , it was higher than ras wild type . 
bold text indicates signicant p values . abbreviations : hr , hazard ratio ; msi , microsatellite instability ; mss , microsatellite stable ; ref , reference . intriguingly , a high proportion of cases with at - ras mutations ( 30% ) displayed co - occurring typical ras and / or braf v600e mutations . 
given that 92% of cases with at - ras mutations were mss and 83% were tmb low , the occurrence of at - ras mutations was not limited to hyperor ultramutated tumors enriched with passenger mutations . 
it is arguable that the mild hyperactivation of the oncogenic mapk pathway driven by some at - ras mutations may require additional hits ( eg , a co - occurring ras or nf1 mutation ) to efciently drive tumor progression . 
because our results on the negative predictive role of at - ras mutations on the efcacy of anti - egfrs are descriptive and could be biased by several confounding factors , they cannot be used to drive decision making in clinical practice . 
however , even if validation studies of our preliminary ndings are challenging , retrospective or pooled analyses of randomized clinical trials should be ideally carried out , possibly by means of targeted genomic panels including at - ras mutations combined with other multiple , albeit uncommon , primary resistance alterations , as recently performed by our group.26 we highly emphasize that a prospective international data set and preclinical collaborations should be established to better assess the individual role of specic at - ras mutations as predictive biomarkers . the main limitations of our study include the small subset of patients with at - rasmutated tumors with available data about clinical outcome , especially about response to antiegfr agents ; the lack of comprehensive genomic sequencing data for all patients included in the study ; and the heterogeneity of ngs platforms adopted . 
however , our data suggest a close phenotypic similarity between isolated at - ras and typical ras mutations that is reasonably driven by at - ras mutations with established increased mapk activity or by the cooperation of multiple activating signals in the mapk pathway . 
schrock , giovanni randon , daniele rossini , giovanni fuc `a , jeffrey s . ross , daisuke kotani , russell madison , seung tae kim , lisa salvatore , filippo pagani , beatrice borelli , federica perrone , jeeyun lee , takayuki yoshino , filippo de braud , alfredo falcone , jaclyn f . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . filippo pietrantonio consulting or advisory role : amgen , merck serono , bayer , eli lilly , sano , roche , servier rona yaeger research funding : array biopharma , glaxosmithkline , novartis , boehringer ingelheim travel , accommodations , expenses : array biopharma alexa b . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine research funding : foundation medicine daisuke kotani honoraria : merck serono , chugai pharmaceutical , takeda , eli lilly japan consulting or advisory role : merck serono russell madison employment : foundation medicine stock and other ownership interests : foundation medicine lisa salvatore honoraria : roche , merck serono , servier , bayer consulting or advisory role : merck serono , servier , bayer travel , accommodations , expenses : sano , merck serono , bayer maria di bartolomeo honoraria : eli lilly , msd oncology , servier consulting or advisory role : eli lilly , msd oncology research funding : eli lilly ( inst ) travel , accommodations , expenses : roche , sano vincent a . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine , mirati therapeutics consulting or advisory role : revolution medicines patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center siraj m . 
ali employment : foundation medicine leadership : incysus stock and other ownership interests : exelixis , blueprint medicines , agios pharmaceuticals , genocea biosciences consulting or advisory role : revolution medicines , azitra ( i ) , princepx tx ( i ) patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome stuff in nonneoplastic disease ( i ) takayuki yoshino research funding : chugai pharmaceutical ( inst ) , sano ( inst ) , sumitomo dainippon pharma ( inst ) , glaxosmithkline ( inst ) filippo de braud consulting or advisory role : ignyta , pzer , amgen , novartis , daiichi sankyo , bristol - myers squibb , domp `e , pierre fabre , roche , octimet oncology , incyte , teofarma , emd serono , pharm research associates speakers bureau : msd , novartis , bristol - myers squibb , roche , pzer , menarini research funding : novartis ( inst ) , roche ( inst ) , msd ( inst ) , ignyta ( inst ) , medimmune ( inst ) , nektar ( inst ) , bristol - myers squibb ( inst ) , merck serono ( inst ) , bayer ( inst ) , celgene ( inst ) , glaxosmithkline ( inst ) , boehringer ingelheim ( inst ) , eli lilly ( inst ) , pzer ( inst ) , servier ( inst ) alfredo falcone honoraria : eli lilly , roche , merck , servier , amgen consulting or advisory role : amgen , bayer , bristol - myers squibb , eli lilly , merck , roche , servier research funding : amgen ( inst ) , bayer ( inst ) , merck ( inst ) , roche ( inst ) , sano ( inst ) , msd ( inst ) , servier ( inst ) travel , accommodations , expenses : amgen , bayer , roche , merck , servier jaclyn f . 
nat rev cancer 11 : 761 - 774 , 2011 janakiraman m , vakiani e , zeng z , et al : genomic and biological characterization of exon 4 kras mutations in human cancer . 
cancer res 70 : 5901 - 5911 , 2010 douillard jy , oliner ks , siena s , et al : panitumumab - folfox4 treatment and ras mutations in colorectal cancer . 
n engl j med 369 : 1023 - 1034 , 2013 pietrantonio f , cremolini c , petrelli f , et al : first - line anti - egfr monoclonal antibodies in panras wild - type metastatic colorectal cancer : a systematic review and meta - analysis . 
crit rev oncol hematol 96 : 156 - 166 , 2015 cremolini c , loupakis f , antoniotti c , et al : folfoxiri plus bevacizumab versus folfiri plus bevacizumab as rst - line treatment of patients with metastatic colorectal cancer : updated overall survival and molecular subgroup analyses of the open - label , phase 3 tribe study . 
harl e a , filhine - tresarrieu p , husson m , et al : rare ras mutations in metastatic colorectal cancer detected during routine ras genotyping using next generation sequencing . 
ann oncol 29 : 44 - 70 , 2018 shinozaki e , yoshino t , yamazaki k , et al : clinical signicance of braf non - v600e mutations on the therapeutic effects of anti - egfr monoclonal antibody treatment in patients with pretreated metastatic colorectal cancer : the biomarker research for anti - egfr monoclonal antibodies by comprehensive cancer genomics ( breac ) study . 
br j cancer 117 : 1450 - 1458 , 2017 loree jm , miron b , holla v , et al : not all ras mutations created equal : functional and clinical characterization of 80 different kras and nras mutations . 
cremolini c , morano f , moretto r , et al : negative hyper - selection of metastatic colorectal cancer patients for anti - egfr monoclonal antibodies : the pressing case - control study . 
fabrizio da , george tj jr , dunne rf , et al : beyond microsatellite testing : assessment of tumor mutational burden identies subsets of colorectal cancer who may respond to immune checkpoint inhibition . 
kumar p , henikoff s , ng pc : predicting the effects of coding non - synonymous variants on protein function using the sift algorithnat protoc 4 : 1073 - 1081 , 9 : 34 , 2017 2009 19 . 
domingo e , freeman - mills l , rayner e , et al : somatic pole proofreading domain mutation , immune response , and prognosis in colorectal cancer : a retrospective , pooled biomarker study . 
cremolini c , di bartolomeo m , amatu a , et al : braf codons 594 and 596 mutations identify a new molecular subtype of metastatic colorectal cancer at favorable prognosis . 
morano f , corallo s , lonardi s , et al : negative hyper - selection of ras and braf wild - type metastatic colorectal cancer patients receiving panitumumab - based maintenance therapy : a pre - specied exploratory analysis of the valentino study . 
elvin , md , phd1 purpose vulvar squamous cell carcinoma ( vscc ) encompasses two predominant variants : one associated with detectable high - risk strains of human papillomavirus ( hrhpv ) and a second form often occurring in the context of chronic dermatitis in postmenopausal women . 
sixty - one percent of hpv + vsccs had a pathogenic alteration in the pi3k / mtor pathway , whereas hpv vsccs showed alterations in tp53 , tertp , cdkn2a , ccnd1 , and egfr , and biomarkers associated with responsiveness to immunotherapy . jco precis oncol 4 : 647 - 661 . 
90% of vulvar cancers and nearly 5% of all gynecologic cancers.1 , 2 radical excision imposes high morbidity , and one third of patients have been shown to experience recurrence after primary treatment.3 recent reports have shown durable responses with denitive or neoadjuvant chemoradiation for unresectable cancers.4 , 5 for patients with recurrence or distant metastasis , prognosis is poor , with an overall 2 - year survival rate of less than 15%.6 there is a critical need to improve our understanding of the molecular pathogenesis of vscc to provide insights that may guide more effective therapies . vscc develops through two distinct oncogenic pathways . 
this subgroup often associates with usual - type vulvar intraepithelial neoplasia ( vin ) , also known as high - grade squamous intraepithelial lesion.7 although other anogenital squamous cell neoplasms have  . 
 williams et al context key objective previous analyses have suggested genetic differences in vulvar squamous cell carcinoma based on human papillomavirus ( hpv ) status , but restricted sample volume and testing platforms have limited comprehensive identication of statistically signicant differences . 
in a large - scale comparative genomic study , what undiscovered genomic alterations distinguish high - risk hpv - driven versus dystrophic / inammatory - associated vulvar squamous cell carcinoma ? knowledge generated we identify signicantly different molecular proles based on hpv status . 
for genomic analyses , 60 ng of dna was extracted from 40 - m sections of 255 , 008 tumor samples , including 280 vscc specimens and 1 , 031 cervical squamous cell carcinoma ( cscc ) , each from a different patient , in formalin - xed parafnembedded ( ffpe ) tissue blocks . 
hpv genome sequences were detected by de novo assembly of nonhuman sequencing reads and nucleotide basic local alignment search tool ( blastn ) comparison against all viral nucleotide sequences in the national center for biotechnology information refseq database . 
hpv types identied in this study were stratied according to the hpv classication described by muoz et al , 8 with hpv 16 , 18 , 31 , 33 , and 58 labeled hrhpv + and hpv 6 labeled low risk . 
sequencing was performed on the primary tumor in 200 patients and on metastases in 80 ( 57 regional lymph nodes and 23 distant sites )  . hpv status and typing were determined on all 280 patient samples ; 102 / 280 vsccs ( 36% ) contained hrhpv sequences , predominantly hpv 16 ( 88% ; table 1 )  . 
for the 177 hpv vsccs , 137 were sequenced using the original primary tumors and 40 from metastatic site biopsies ( 10 distant , including seven lung , one pleural , one abdominal , and one to bone )  . comprehensive genomic proling figure 1 displays the distribution of gas by hpv status . 
the only specic point mutation with a signicant difference between hpv + and hpv was pik3ca e545k , an activating mutation that was signicantly enriched in hpv + vsccs ( table 2 )  . 
of vsccs cell - free circulating tumor dna ( ctdna ) was evaluated from blood specimens collected from 10 patients with vscc ( liquid biopsy ) using the hybrid capture - based illumina hi - seq ( illumina , san diego , ca ) technology . 
maximum somatic allele frequency was used to estimate the fraction of ctdna per methods previously described.30 , 31 mutational signatures mutational signatures were assessed for all tumor samples with at least 20 nondriver somatic missense alterations . signatures were given by analysis of the trinucleotide context and proled using the sanger cosmic signatures of mutational processes in human cancer.32 a positive signature required a sample to have at least a 40% t to a characterized mutational process , including apobec overexpression , exposure to ultraviolet light , hypofunction of the brca tumor suppressor , and defects in mismatch repair.32 immunohistochemistry programmed death - ligand 1 ( pd - l1 ) immunohistochemistry ( ihc ) was performed regularly in tandem with cgp to guide patient selection for immunotherapy . 
pd - l1 protein expression was assessed by ihc on 5 - micron ffpe tissue sections using the dako pd - l1 ihc22c3 pharmdx assay ( agilent ; santa clara , ca ; n = 52 vsccs ) or the ventana ( oro valley , az ) pd - l1 ( sp142 ) assay ( n = 21 vsccs ) , following each manufacturers instructions . 
dako pd - l1 expression was reported as a tumor proportion score , and ventana pd - l1 was reported as percent tumor area covered by positively staining tumor cells and immune cells . less than 1% staining was dened as negative , 1% - 49% was dened as low positive , and 50% was dened as high positive . clinicopathologic analysis of the vscc cohort a total of 280 vsccs were assayed with cgp ( foundation medicine ) , using material sent from treating institutions , from 2014 to 2019 . 
human investigations were performed after approval by a local human investigations committee and in accordance with an assurance led with and approved by the department of health and human services , where appropriate . 
amp , amplication ; mb , megabase ; msi , microsatellite instability ; msi - h , microsatellite instability - high ; mss , microsatellite stable ; mut , mutation ; pd - l1 , programmed death - ligand 1 ; tmb , tumor mutation burden . of each ga in the hpv and hpv + cohorts is included in appendix figures a2a and a2b , respectively . in the entire cohort : an hpv 16 ( + ) vscc with an mlh1 splice site mutation . frequencies of specic biomarkers associated with responsiveness to immunotherapy differed between the vscc subgroups ( fig 2 )  . 
all other gas , as well as age and pd - l1 ihc staining , showed no signicant differences between primary versus metastatic samples controlled for hpv status . comparison of hpv 16 with other hrhpv subtypes revealed no signicant differences in demographics , tmb , or sequenced site . 
thirty - three ( 12.6% ) were identied with an apobec ( apolipoprotein b mrna - editing enzyme , catalytic polypeptide - like ) signature ( 12 hpv + and 21 hpv ) , two with brca signature ( one hpv + , one hpv ) , seven with mismatch repair ( two hpv + , ve hpv ) , and a single tumor with ultraviolet signature ( hpv )  . 
three of four liquid biopsies showed at least one pathogenic ga present in the associated tissue biopsy ( appendix table a2 )  . separate from our 280 patients in the vscc cohort , ctdna was evaluated on six patients with known vscc but without tissue biopsy sequencing data . 
gas were detected in ve of six of these patients ( appendix table a2 )  . hpv + cscc ( n = 864 ) showed gas that were largely similar to what we found in hpv + vscc ( n = 103 ; appendix table a3 )  . 
although low in frequency , gas in kdm6a , ar , and cdk12 were signicantly higher in vscc versus cscc ( appendix table a3 )  . discussion in this study , hybrid capture - based dna sequencing was applied to a large series of patient tumors to better characterize the genomic landscape of vscc and to identify important genetic differences between hpv + and hpv disease . 
consistent with prior studies , a high rate of mutation was identied overall , with 98% of tumors in the analysis containing one or more known oncogenic mutations.17 , 18 mutational proles sharply differentiated hpv + and hpv disease . 
hpv + vscc showed mutations in the pi3k / mtor pathway , with 61% of tumors containing gas in the pathway , with the majority of gas showing signicant association with hpv + status ( table 2 )  . 
choschzick et al22 specically examined ccnd1 copy number changes in 183 vsccs and identied amplications in 22% , with a signicant association with hpv tumors.23 growdon pd - l1 ihc negative low positive high positive genomic alterations rearrangement short variant deletion not performed amplification fig 2 . 
of the 73 vulvar squamous cell carcinoma for which pd - l1 ihc was performed , 33% of hpv - negative and 9% of hpv - positive were pd - l1 tumor high - positive ; p = .04. 
histopathology of vulvar squamous cell carcinoma ranged from ( a ) well differentiated with abundant keratin to ( b ) poorly differentiated ( hematoxylin and eosin stains , 400 )  . 
 ( c ) programmed death - ligand 1 ( pd - l1 ) staining of human papillomavirus ( hpv ) negative vsccs showed signicantly higher frequency of high - positive tumors , whereas ( d ) hpvpositive disease was largely negative for pd - l1 stain ( pd - l1 immunohistochemistries , 400 )  . et al24 evaluated egfr amplication in 51 vsccs , and identied amplication in 12% of tumors , with signicant association with poor prognosis and hpv status . 
zie ba et al19 performed sequencing of 81 vsccs with a 50 - gene panel , and the results differed from other studies , most strikingly in the absence of clear genomic differences between hpv + and hpv disease . 
the authors reported tp53 and cdkn2a mutations in both hpv + and hpv vscc , whereas mutations in pik3ca , fbxw7 , hras , fgfr3 , stk11 , akt1 , smad4 , and pten were found at low frequencies in both types of vscc.19 zie ba et al19 noted , however , that the 2 hpv tests that they used gave highly inconsistent results and that those hpv tests had not been developed for analyzing tissue - derived dna.19 these difculties in identifying hpv + and hpv disease may account for the divergence of their results from several prior studies.16 - 18 , 20 in our study , hpv status clearly divided our large cohort into two signicantly different genomic - dened diseases . pi3k / mtor pathway mutations , including stk11 , a negative regulator of mtor signaling , have been described in a wide range of hpv - driven cancers.33 , 34 in our cohort , a signicantly higher rate of stk11 gas was observed in hpv + tumors sequenced from metastases , compared with hpv + tumors sequenced from the primary site . stk11 has been previously correlated with poor response to antiprogrammed death - 1 therapy in kras - mutant lung adenocarcinoma.35 it is conceivable that a similar role could exist in hpv + vscc as a putative tumor immuneescape mechanism , but additional studies are needed . a minority of vsccs showed distinctive mutational signatures . 
this signature reects apobec cytidine deaminase dna - editing activity36 , 37 and has been noted to be important in development of thoracic cancers , with possible implications for predicting response to immunotherapy.38 , 39 several of the gas observed to be signicantly enriched in the hpv cohort are in pathways functionally relevant to hpv pathogenesis . 
tp53 , tert , and cdkn2a are deregulated by hpv e6 and / or e7 , whereas egfr recycling is altered by hpv e5.40 - 42 beyond specic gas , key differences were identied in tmb and pd - l1 ihc staining patterns . 
hpv induces genomic instability , which may account for the increased tmb in the primary hpv + cohort.43 in addition , hpv infection reduces the cellular immune response by decreasing the interferon antiviral response.44 cgp may reveal opportunities for targeted therapies to be tested in clinical trials . 
kmt2d , an epigenetic modier , and transcription factor sox2 can activate and interact with the pi3k pathway.49 - 51 gas in both are enriched in hpv + vscc ( table 2 )  . 
tumors with gas in kmt2d may be sensitive to aurora kinase inhibition.52 in light of the many recent successes of immune checkpoint inhibitors , a careful approach to patient selection for clinical trials of these agents may be valuable . 
in our cohort , hpv vsccs showed a signicantly higher rate of pd - l1 ihc highpositive tumor staining , a higher rate of pdl1 amplication , and signicantly lower rates of stk11 alterations . 
vsccs in this category may benet from novel targeted therapeutics.53 other identied potential therapeutic targets include gas in receptor tyrosine kinases , cell cycle regulation , and the mapk pathway . 
early work in gas that affect epigenetic regulation indicates ezh2 inhibitors may be a viable therapeutic strategy.54 , 55 our study also provides a proof of concept that liquid biopsy detects ctdna in vscc , with three of four demonstrating at least one pathogenic ga detected in the tissue biopsy from the same patient . 
liquid biopsy may be a valuable method in vscc , and additional investigation is warranted . limitations in the study include the distinct patient population . tumor samples undergoing cgp are usually sent by clinicians seeking targeted therapy for patients with advanced disease . an additional limitation is the inadequate data on treatment history of the patients before tumor sequencing ; controls for tmb and resistance gas that may have arisen from local radiation or systemic treatment were not available . 
future work is needed to correlate genetic ndings with treatment exposure and follow - up data , which are not included in this study . in this study , we provided evidence that hpv + and hpv vscc are two distinct diseases , each with a characteristic molecular prole . 
 genomics of hpv + versus hpv vulvar squamous cell carcinoma rachel erlich employment : foundation medicine stock and other ownership interests : foundation medicine kevin jon williams stock and other ownership interests : hygieia stock and other ownership interests : gemphire therapeutics consulting or advisory role : gemphire therapeutics , inc . research funding : novo nordisk jeff m . 
venstrom employment : genentech , foundation medicine leadership : genentech stock and other ownership interests : genentech research funding : genentech , foundation medicine travel , accommodations , expenses : genentech brian m . 
alexander employment : foundation medicine leadership : foundation medicine stock and other ownership interests : roche research funding : eli lilly ( inst ) , puma ( inst ) , celgene ( inst ) open payments link : 854258 / summary nikunj shah employment : foundation medicine natalie danziger employment : foundation medicine eric a . 
severson employment : foundation medicine , partners healthcare stock and other ownership interests : foundation medicine jonathan keith killian employment : foundation medicine stock and other ownership interests : foundation medicine douglas i . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : celsius therapeutics research funding : foundation medicine julie y . 
hemmerich employment : foundation medicine stock and other ownership interests : foundation medicine ( inst ) acknowledgment we thank our colleagues for their helpful comments during the preparation of this article . references judson pl , habermann eb , baxter nn , et al : trends in the incidence of invasive and in situ vulvar carcinoma . 
moore dh , ali s , koh wj , et al : a phase ii trial of radiation therapy and weekly cisplatin chemotherapy for the treatment of locally - advanced squamous cell carcinoma of the vulva : a gynecologic oncology group study . 
n engl j med 348 : 518 - 527 , 2003 alemany l , saunier m , alvarado - cabrero i , et al : human papillomavirus dna prevalence and type distribution in anal carcinomas worldwide . 
adv anat pathol 24 : 201 - 214 , 2017 van der avoort ia , shirango h , hoevenaars bm , et al : vulvar squamous cell carcinoma is a multifactorial disease following two separate and independent pathways . 
virgili a , borghi a , toni g , et al : prospective clinical and epidemiologic study of vulvar lichen sclerosus : analysis of prevalence and severity of clinical features , together with historical and demographic associations . 
weberpals ji , lo b , duciaume mm , et al : vulvar squamous cell carcinoma ( vscc ) as two diseases : hpv status identies distinct mutational proles including oncogenic broblast growth factor receptor 3 . 
trietsch md , nooij ls , gaarenstroom kn , et al : genetic and epigenetic changes in vulvar squamous cell carcinoma and its precursor lesions : a review of the current literature . 
swarts dra , voorham qjm , van splunter ap , et al : molecular heterogeneity in human papillomavirus - dependent and - independent vulvar carcinogenesis . cancer med 7 : 4542 - 4553 , 2018 24 . 
halec g , alemany l , lloveras b , et al : pathogenic role of the eight probably / possibly carcinogenic hpv types 26 , 53 , 66 , 67 , 68 , 70 , 73 and 82 in cervical 9 : 34 , 2017 cancer . 
sakamoto j , kamiura s , okayama k , et al : single type infection of human papillomavirus as a cause for high - grade cervical intraepithelial neoplasia and invasive cancer in japan . 
clark ta , chung jh , kennedy m , et al : analytical validation of a hybrid capturebased next - generation sequencing clinical assay for genomic proling of cell - free circulating tumor dna . 
gregg jp , li g , pavlick d , et al : comprehensive genomic proling of ctdna in patients with colon cancer and its delity to the genomics of the tumor biopsy . j clin oncol 36 : 569 , 2018 ( 4 ; suppl ) 32 . 
wang s , jia m , he z , et al : apobec3b and apobec mutational signature as potential predictive markers for immunotherapy response in non - small cell lung cancer . 
gameiro sf , kolendowski b , zhang a , et al : human papillomavirus dysregulates the cellular apparatus controlling the methylation status of h3k27 in different human cancers to consistently alter gene expression regardless of tissue of origoncotarget 8 : 72564 - 72576 , 2017 42 . 
zhang b , srirangam a , potter da , et al : hpv16 e5 protein disrupts the c - cbl - egfr interaction and egfr ubiquitination in human foreskin keratinocytes . oncogene 24 : 2585 - 2588 , 2005 43 . 
song d , li h , li h , et al : effect of human papillomavirus infection on the immune system and its role in the course of cervical cancer . 
tinker av , ellard s , welch s , et al : phase ii study of temsirolimus ( cci - 779 ) in women with recurrent , unresectable , locally advanced or metastatic carcinoma of the cervix . 
oncol lett 12 : 4107 - 4116 , jung k , kang h , mehra r : targeting phosphoinositide 3 - kinase ( pi3k ) in head and neck squamous cell carcinoma ( hnscc )  . 
pi3k pathway regulates er - dependent transcription in breast cancer through the epigenetic regulator kmt2d . oncogene 37 : 1354 - 1368 , 2018 science 355 : 1324 - 1330 , 2017 51 . 
kalu nn , mazumdar t , peng s , et al : comprehensive pharmacogenomic proling of human papillomavirus - positive and - negative squamous cell carcinoma identies sensitivity to aurora kinase inhibition in kmt2d mutants . 
strauss j , heery cr , schlom j , et al : phase i trial of m7824 ( msb0011359c ) , a bifunctional fusion protein targeting pd - l1 and tgfb , in advanced solid tumors . clin cancer res 24 : 1287 - 1295 , 2018 idris s , lindsay c , kostiuk m , et al : investigation of ezh2 pathways for novel epigenetic treatment strategies in oropharyngeal cancer . 
lindsay cd , kostiuk ma , harris j , et al : efcacy of ezh2 inhibitory drugs in human papillomavirus - positive and human papillomavirus - negative oropharyngeal squamous cell carcinomas . 
 hpv negative ( n = 177 ) hpv positive ( n = 103 ) rearrangement short variant deletion amplification multiple rearrangement short variant deletion amplification multiple williams et al fig a2 . 
 systematic assessment of tumor purity and its clinical implications syed haider , phd1 , 2 ; svitlana tyekucheva , phd3 , 4 ; davide prandi , phd5 ; natalie s . 
laird , phd10 ; chris sander11 , 12 ; wenyi wang , phd13 ; francesca demichelis , phd5 , 14 ; massimo loda , md15 , 16 ; and paul c . 
as molecular proles are frequently generated using bulk tissue sections , they represent an admixture of multiple cell types ( including immune , stromal , and cancer cells ) interacting with each other . 
bulk mrna and microrna proles were subject to in silico deconvolution to estimate cancer cellspecic mrna and microrna proles . results we present a systematic comparison of 10 tumor purity estimation methods on a cohort of 333 prostate tumors . 
limited concordance between dnaand mrna - derived purity estimates remained a general pan - cancer phenomenon when tested in an additional 4 , 497 tumors spanning 12 cancer types . conclusion the choice of tumor purity estimation method may have a profound impact on the interpretation of genomic assays . 
taken together , these data highlight the need for improved assessment of tumor purity and quantitation of its inuences on the molecular hallmarks of cancers . jco precis oncol 4 : 995 - 1005 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the tumor microenvironment represents an admixture of multiple cell types and complex interactions between bona de cancer cells and surrounding stromal and immune cells.1 because a majority of highthroughput experiments are performed on bulk tissue samples , the resulting signal is usually confounded by nonmalignant tumor - adjacent cells ( tacs )  . variable tumor content and variable tac composition can impinge upon interpretations of molecular data and subsequent clinical decisions.2 - 4 to delineate true residual signal representing individual cell populations , it is crucial to accurately estimate tumor purity . 
tumor purity represents the fraction of cancer cells in a tumor and can be estimated either by expert pathologists reviewing tumor sections5 or in silico ( using epigenomic , genomic , or transcriptomic proles ) .6 pathologic estimates can be inconsistent5 and pragmatically may not always represent the region of tumor that is subject to molecular proling . 
although in silico estimates could circumvent these problems , it remains unclear to what extent these estimates vary across purity calling methods and with the underlying type of biomolecule ( eg , dna v rna )  . 
previous studies have quantied the pan - cancer purity landscape2 , 7 and compared a panel of tools for estimating tumor purity.6 however , systematic benchmarking of in silico tumor purity against matched pathologic estimates and its association with multimodal clinico - genomic proles remains to be elucidated . 
herein , we present systematic benchmarking of 10 purity estimation methods using dna , mrna , and microrna ( mirna ) proles in a 333patient clinically - coherent cohort8 with matched multiobserver pathologic estimates of purity . 
to determine the context specicity of these algorithms , we compared tumor purity estimates from multiobserver pathology to those from multiple algorithms working on different biomolecules ( eg , dna , rna )  . knowledge generated tumor purity estimates from in silico tools varied signicantly from pathology estimates . 
we recommend parameterizing genomic analyses with tumor purity estimated from the matched molecular analyte being analyzed . relevance tumor purity is a key criterion for sample inclusion in clinico - genomic studies and subsequent interpretation of molecular results . 
computational tools often require purity estimates ; we show that these are inuenced by the selected purity estimator . both molecularly driven clinical trials , as well as therapeutic and theranostic decisions , may be affected by these choices . quantify how molecular correlates of tumor purity can skew clinico - genomic interpretations as the result of variable estimates of cancer cell fraction . 
integer infers purity , ploidy , and subclonality from paired tumor and normal samples using the following principles : ( 1 ) models the relationship between the observed allelic frequencies and the underlying copy number changes , and the possible existences and impacts of multiple subclones that may often mislead inferences if not explicitly modeled ; ( 2 ) simultaneous statistic inference on the basis of both copy number changes and major allelic frequencies ; ( 3 ) restoration of information lost as a result of the guanine - cytosine content and actual sizes of each library insert and other specic biases of each genomic location ; ( 4 ) avoid making inferences when the signal - to - noise ratio is not ideal because of technical artifacts ; ( 5 ) an explicit modeling of whole - genome duplication events and whole - chromosome duplication events , which are common in cancer genomics and have huge impacts on the accurate inference of purity and ploidy ; the cancer genome atlas pan - cancer purity estimates were generated using processed rna - seq data ( for isopure ) downloaded from ( download version 2015 ) and snp6 array level - 1 data ( for ascat ) downloaded from gdc data portal . consensus pathology , dna , and mrna purity estimates multiobserver pathology reviews yielded purity ranges , 8 which were further collapsed into single - point estimates using the median value of purity range in deciles . 
dna ( absolute , ascat , clonet , integer , oncosnp ) and mrna ( demix and isopure - r ) based purity estimates were aggregated using median dna and mrna estimates , respectively . availability of data and materials all processed data are available either in the data supplement or uploaded to as speciﬁed in the data supplement . 
 haider et al ethics approval and consent to participate tissue contributing sites followed appropriate consent documentation and approved submission of cases to the cancer genome atlas , as detailed in the original publication.8 results prostate cancer presents complex intraand interpatient heterogeneity . 
it is an ideal model to study heterogeneity because of frequent surgical management via radical prostatectomy of the whole gland , allowing spatio - genomic studies.9 , 10 we collated pathologic , molecular , and clinical data sets from the cancer genome atlas ( tcga ) prostate marker study , which comprised 333 patients.8 purity estimates from multiple pathologists were consolidated , resulting in point estimates as previously described8 ( see methods )  . 
for a subset of cases , both top and bottom tissue block slides ( with sections acquired for molecular analysis in between these ) were assessed by multiple pathologists , demonstrating moderate correlation between pathologists ( top sections : pearsons r = 0.64 , p = 6.23 107 ; bottom sections : pearsons r = 0.53 , p = 8.93 103 ; data supplement fig 1a - b )  . 
a similar trend was observed between the pathology estimates of top and bottom sections ( pearsons r = 0.59 , p = 2.03 1012 ; data supplement fig 1c ) , highlighting potential inuence of spatial heterogeneity . 
in silico estimates of tumor purity were generated using nine methods11 - 18 that leverage dna ( methylation or copy number data ) , mrna , or mirna proles ( data supplement tables 1 and 2 ; methods )  . 
of note , leuc estimates on the basis of dna methylation data were right skewed , with a median purity of 0.9 ( leuc - other = 0.33 , p = 1.44 1095 , wilcoxon rank sum test )  . 
interestingly , all these methods were based on dna proles ( genomic or epigenomic ) , suggesting intrinsic limitations in estimating tumor purity from dna - based assays in this setting . 
these limitations could be explained by the dna prole itself , because samples with failed purity estimates exhibited quiet genomes with low numbers of somatic single nucleotide variants ( snvs ; data supplement fig 2a - b )  . 
pathology calls did not show clear evidence of low purity ; however , rnabased methods predicted a trend toward low purity for a subset of samples ( data supplement fig 2c )  . 
however , it is probable that some may also represent quiet cancer genomes , which are now increasingly recognized as a real phenomenon , particularly in prostate cancer.8 , 19 inspection of the complete sample set revealed no association with histologic heterogeneity ( rationalized as gleason score10 ; fig 1b , data supplement fig 3a - b )  . 
hence , we preclude spatial heterogeneity as the primary factor underlying this lack of concordance . these data highlight that variation and error proles among the intraplatform estimates are probably correlated and suffer from similar intrinsic limitations , independent of the specic algorithm used . 
therefore , we created consensus dna and mrna purity estimates using the median for each class of methods , hereafter referred to as dna and mrna estimates ( see methods )  . 
the differences between pathology estimates and either dna or mrna estimates were strongly correlated ( pearsons r = 0.81 , p = 4.68 1079 ; fig 2 ) , with 29.13% of cases demonstrating agreement ( within 15% purity of each other )  . 
 ( a ) distribution of tcga prostate tumor purity estimates ( n = 333 ) using in silico methods and consolidated multiobserver pathology reviews ; ( b ) patient - wise purity estimates grouped by gleason score . 
data from integer were available for 107 samples using the low - pass dna sequencing data ; ( c ) pearson correlation between purity estimates inferred using in silico methods and pathology reviews . 
of the dnaand mrna - based estimates , only two samples displayed discordant directions of effect relative to pathologic estimates ( purple and yellow dots in fig 2 ) , highlighting overall similarity in error proles of the underlying biomolecules . next , we assessed whether the key transcriptional and genomic biomarkers that underpin prostate cancer biology are dependent on tumor purity . 
to further delineate the relationship between tumor purity and somatic mutations , we stratied purity estimates by the mutation status of a panel of recurrently altered genes in prostate cancer.8 tumor purity determined by at least one prole was associated with six genes , including erg fusions and spop , foxa1 , and tp53 point mutations ( false discovery rate [ fdr ] adjusted p , .25 , wilcoxon rank sum test ; fig 3d , data supplement table 3 )  . 
for these six genes , tumor purity was moderately higher in mutant samples . to characterize this association between driver gene status and tumor purity , we evaluated the associations between tumor purity and the variant allele frequency ( vaf ) in samples carrying mutations ( fig 3e )  . 
however , pathology estimates of tumor purity were unable to accurately capture the vaf of these recurrently altered genes . next , we evaluated whether pathology , dna , mrna , and mirna purity estimates vary in their associations with individual genes or mirnas and to what extent these can be overcome by using in silico deconvolution.15 each of the four consensus purity estimators was individually correlated with ve molecular proles ( bulk / nave and deconvolved mrna abundance , bulk / nave and deconvolved mirna abundance , and bulk copy number data ; deconvolved proles were generated using isopure )  . 
nave mrna and mirna proles exhibited the greatest proportion of features correlated with tumor purity , which diminished after in silico deconvolution , highlighting potentially confounding tacs . with the exception of nave mirna proles , purity estimates were inversely correlated with molecular proles regardless of the underlying purity estimation prole ( data supplement fig 5a - f )  . 
these data suggest that the presence of genomic and transcriptomic correlates of tumor purity are likely to confound biologic and clinical interpretations . because dnaand mrna - based assays are most commonly used in cancer genomics , we asked if the purity estimates from these two analytes are comparable in other cancers . 
given the strong intra - analyte correlation ( fig 1c ) , we considered a representative dna - based method ( ascat ) and an mrna - based method ( isopure ) to estimate tumor purity for an additional 12 cancer types ( 4 , 497 tumor samples ) from tcga project ( fig 4b , prostate cancer data discussed above is shown for reference only )  . overall , all cancer types showed an average purity of at least 0.56. 
these data further underscore the importance of using analyte - matched purity estimates for bioinformatics analysis and subsequent interpretation . discussion herein , we provide evidence that tumor purity estimates manifest intrinsic properties of the underlying information used for purity estimation and exhibit only modest interprole concordance . 
however , interpathologist variation observed in our study , as well as previous studies , suggests that there are probably some inaccuracies in these estimates because of their subjectivity / qualitative nature.5 , 21 these discrepancies may also be a result of the lack of full spatial heterogeneity of the pathologic slide . 
genomic correlates of tumor purity as summarized using androgen receptor ( ar ) signature score ( a ) , percent genome altered ( [ pga ] , b ) , and mutation burden ( c )  . 
statistical tests were performed for genes with more than three mutant samples . therefore , idh1 , rb1 , akt1 , and chd1 ( displayed with x ) were deemed inappropriate for statistical testing . 
 ( a ) correlation between purity estimates derived using pathology , dna , mrna , and microrna ( mirna ) proles and molecular proles ( mrna.naive = bulk mrna abundance , mrna.isopure = deconvolved mrna abundance , mirna.naive = bulk mirna abundance , mirna.isopure = deconvolved mirna abundance , and cna = bulk copy number data ; deconvolved rna proles were generated using isopure )  . 
each feature ( genes for mrna and copy number aberration [ cna ] proles , mirnas for mirna proles ) was correlated with tumor purity estimators ( pathology , dna , rna , mirna ) separately . 
 ( b ) distribution of tumor purity estimates across 13 tcga tumor types ( 4 , 830 tumors ) using an in silico dna - based ( ascat ) and mrna - based ( isopure ) method . 
for clinico - genomic sequencing studies requiring a minimum purity threshold for inclusion in the study , an alternative to pathology estimates is to infer purity directly from the analyte by performing low - pass dna sequencing to lter low - purity samples.22 in addition to poor concordance between pathology and dna / rna - based tumor purity in prostate cancer , our pan - cancer data reported herein suggest that the purity estimates from dna and mrna proles also show limited concordance . 
the concordance between purity estimators also varies depending upon the tumor type and patterns of somatic changes it exhibits ( eg , dna - based methods rely on the presence of copy number aberrations )  . 
furthermore , previous studies have reported varying levels of concordance in purity estimates inferred from dnaand rna - based methods.2 , 23 for instance , aran et al2 show much stronger concordance between estimate24 ( rna - based purity estimator ) and absolute13 ( dna - based purity estimator ) compared with the rnaand dna - based methods in our study . 
because purity estimates vary across methods , consensus estimates on the basis of matched analyte type may further improve purity estimates and may also overcome missing values and normalize outlier estimates . 
after condent purity estimates have been created , one way to account for these is to adjust bioinformatics and statistical analyses for tumor purity , as stressed in previous studies.2 , 7 , 15 because bulk tumor proles are heterogeneous compositions of tumor cells and tacs featuring complex interplay , it is crucial to interpret the clinico - genomic proles in the context of the underlying heterogeneity.25 many in silico deconvolution techniques have been developed to estimate relative abundance of different cell types , 24 , 26 , 27 as well as techniques that transcriptomic11 , 12 , 15 , 18 , 23 and explicitly generate residual genomic14 proles of tumor - only and stromal - only cells . 
herein , we recommend researchers to consider deconvolution of bulk proles into individual component proles ( e.g. , cancer and stromal proles ) to improve sensitivity and specicity of downstream analyses.4 , 15 affiliations 1ontario institute for cancer research , toronto , ontario , canada 2the breast cancer now toby robins research centre , the institute of cancer research , london , united kingdom 3department of data sciences , dana - farber cancer institute , boston , 4department of biostatistics , harvard t.h. 
boutros provision of study material or patients : massimo loda collection and assembly of data : syed haider , svitlana tyekucheva , davide prandi , andrew wei xu , peter w . 
park honoraria : pzer consulting or advisory role : neuroinammation newco patents , royalties , other intellectual property : patent on mutational signature - based detection of homologous recombination deciency peter w . 
laird consulting or advisory role : progenity , anchordx patents , royalties , other intellectual property : received royalties annually through 2018 for inventions licensed to epigenomics ag by usc travel , accommodations , expenses : anchordx wenyi wang stock and other ownership interests : genomic health francesca demichelis patents , royalties , other intellectual property : co - inventor on a patent led by the university of michigan and the brigham and womens hospital covering the diagnostic and therapeutic elds for ets fusions in prostate cancer . 
boutros consulting or advisory role : biosymetrics patents , royalties , other intellectual property : holds patents on multiple biomarkers no other potential conicts of interest were reported . acknowledgment the results published herein are based , in part , upon data generated by tcga pilot project established by the national cancer institute and the national human genome research institute . 
nature 501 : 346 - 354 , 2013 fox ns , haider s , harris al , et al : landscape of transcriptomic interactions between breast cancer and its microenvironment . 
nat commun 10 : 3116 , 2019 smits aj , kummer ja , de bruin pc , et al : the estimation of tumor cell percentage for molecular testing by pathologists is not accurate . 
mod pathol 27 : 168 - 174 , 2014 yadav vk , de s : an assessment of computational methods for estimating purity and clonality using genomic data derived from heterogeneous tumor tissue samples . 
brief bioinform 16 : 232 - 241 , 2015 zheng x , zhang n , wu hj , et al : estimating and accounting for tumor purity in the analysis of dna methylation data from cancer studies . 
wang l , sebra rp , sfakianos jp , et al : a reference prole - free deconvolution method to infer cancer cell - intrinsic subtypes and tumor - type - specic stromal 24 . 
 impact of kras and tp53 co - mutations on outcomes after first - line systemic therapy among patients with stk11 - mutated advanced nonsmall - cell lung cancer erin bange , md1 ; melina e . 
langer , md1 ; erica carpenter , mba , phd1 ; and charu aggarwal , md , mph1 purpose the stk11 gene encodes a serine / threonine protein kinase that regulates cell polarity and functions as a tumor suppressor . 
we evaluated the impact of kras and tp53 co - mutations on outcomes after rst - line systemic therapy for patients with metastatic or recurrent nsclc that harbors stk11 mutations . methods we conducted a retrospective review of patients with metastatic nsclc and stk11 mutations treated at the university of pennsylvania . 
the kaplan - meier method was used to estimate overall survival ( os ) and progression - free survival ( pfs )  . results from february 2013 to december 2016 , samples from 1 , 385 patients with nsclc were analyzed by ngs ; of these , 77 patients ( 6% ) harbored an stk11 mutation ( n = 56 , tissue ; n = 21 , plasma )  . 
of the 62 patients included , 18 had an stk11 mutation alone , 19 had stk11 / kras , 18 had stk11 / tp53 , and seven had stk11 / kras / tp53 . 
the majority of the mutations found during routine testing are not actionable currently , but their presence likely has predictive and prognostic relevance . stk11 , also known as liver kinase b1 ( lkb1 ) , is a tumor suppressor and a negative regulator of mammalian target for rapamycin signaling . 
loss - offunction mutations in germline stk11 are associated with peutz - jeghers hereditary cancer syndrome . stk11 mutations are estimated to be present in 8% to 39% of all nsclc , with increased prevalence in smokers and patients with kras mutations.2 , 3 animal that stk11 mutations are critical studies suggest tumorigenesis , and in lung cancer differentiation , metastasis.4 , 5 mutations in stk11 have emerged as a potential prognostic and predictive marker in nsclc . 
 bange et al context key objective how do kras and tp53 co - mutations affect outcomes after rst - line systemic therapy in patients with nonsmall - cell lung cancer and stk11 mutations ? knowledge generated among patients with metastatic nsclc and tumor - associated stk11 mutations , co - mutation with tp53 conferred better progression - free survival ( pfs ) and overall survival ( os ) after rst - line therapy compared with patients who had a kras comutation.tp53 mutation in the presence of an stk11 / kras co - mutation also conferred better pfs and os compared with patients who had only the stk11 / kras co - mutation . relevance stk11 / kras co - mutation has been associated with worse pfs after chemotherapy , but co - mutation with tp53 may modulate outcomes after rst - line chemotherapy in this group and among patients with stk11 mutations without kras mutations . nsclc , which suggests that stk11 mutations may be a more heterogeneous group than previously thought.6 , 7 methods patient population co - mutation status may be another source of heterogeneity among patients with stk11 mutations . 
patients who received treatment outside the institution or had another concurrent malignancy were excluded . mutational analysis the center plasma was analyzed by guardant health ( redwood city , ca ) as described previously.16 solid tumor sequencing was performed at for personalized diagnostics clinical laboratory at the university of pennsylvania ( data supplement )  . 
one kras amplication ; one kras variant of unknown signicance ( vus ) , q61h ; and one tp53 vus ( a161s ) were not considered mutations in the respective genes . 
 outcomes in nsclc by stk11 co - mutations status statistical analysis led to discontinuation of descriptive statistics , including mean , median , and proportions , were used to summarize patient demographics and tumor characteristics . 
os was calculated from the start of systemic treatment of metastatic or recurrent disease to the date of death or last follow - up . patient data were censored at the last follow - up visit or on september 1 , 2017 , if still alive . 2 and kruskal - wallis analyses were used to assess differences in baseline characteristics between the mutation groups for categoric and continuous variables , respectively . cox proportional hazard models were used to determine the relationship of stk11 co - mutations to survival . 
the effect of co - mutation status on pfs and os was investigated by looking at four mutation groups ( stk11 alone , stk11 / kras , stk11 / tp53 , and stk11 / kras / tp53 ) separately as well as at individual mutation effects and interactions in a cox regression model . 
hrs from the cox model were reported . results baseline characteristics during a 42 - month period , 1 , 385 unique patients had sequencing of a lung neoplasm in either tissue ( n = 1 , 526 samples ) or plasma ( n = 245 samples )  . 
the majority ( 51 of 62 , or 82% ) of patients received platinum doubletbased therapy as the rst - line regimen ( table 1 )  . nine patients had a driver mutation and received targeted therapy at some point during treatment ( data supplement )  . five patients received immunotherapy as rst - line systemic therapy ( data supplement )  . 
the baseline characteristics were well balanced among these co - mutation groups , except that patients in the stk11 alone or stk11 / kras / tp53 group were slightly older ( p = .015 ; table 1 )  . 
the most common stk11 mutation was p.l282afs * 3 , which resulted in a frameshift mutation in exon 6 ( fig 2 )  . there was no correlation between the position of the stk11 mutation and co - mutation status . 
kras alterations occurred at codon positions 12 , 13 , 22 , and 61 , and each was considered disease associated by pathology report using pubfrequent mutation licly available databases . 
 ( a ) columns represent individual patients with mutation type specied by color ; missense mutations in stk11 were found in six patients , but specic point mutations were not identied . 
median progression - free survival ( pfs ) and median overall survival ( os ) for co - mutation groups among patients with stk11 mutation ( all mutations reported ) were determined using kaplan - meier methodology . 
all p values are compared with stk11 / kras . patients with tp53 / da - stk11 compared with tp53 / nonda - stk11 . patients with stk11 / kras mutations experienced shorter median os ( 7.1 months ) compared with stk11 alone ( 16.1 months ; log - rank p , .001 ) , stk11 / tp53 ( 28.3 months ; log - rank p , .001 ) , and stk11 / kras / tp53 ( 22 months ; log - rank p = .025 ; table 2 ; fig 3c )  . 
interestingly , we did not nd that stk11ex1 - 2 mutations were associated with an increased risk of progression or death compared with stk11ex3 - 9 mutations , in time ( months ) no . 
kaplan - meier curves of ( b ) pfs and ( d ) os of patients with stage iv or recurrent disease and tumors with disease - associated stk11 mutation . 
other co - factors considered in the analysis but found not to be independent predictors in the univariable model or signicant contributors to the multivariable model were smoking status , performance status at diagnosis , age at diagnosis , stage at presentation , and race / ethnicity ( tables 3 and 4 )  . 
analyses that excluded patients who received immunotherapy or targeted therapy still showed superior outcomes for patients with stk11 / tp53 co - mutations , even in the presence of a kras mutation ( data supplement )  . relevance of disease - associated variants of stk11 as part of an exploratory subset analysis , we repeated the pfs and os kaplan - meier analyses using only the stk11 mutations characterized as disease associated ( da - stk11 )  . when only da - stk11 mutations were included , there was no difference in median pfs between co - mutation groups of interest ( fig 3b )  . 
there remained a signicant difference in median os when stk11 / kras and stk11 / tp53 were compared ( 7.1 months v 39 months ; log - rank p = .01 ; fig 3d )  . discussion in the era of precision medicine , it has become increasingly important to understand the full implications of an everincreasing quantity of tumor genetic information obtained as part of routine sequencing of nsclcs . 
this study includes one of the largest cohorts of patients with stk11 mutations ( n = 62 ) , and to our knowledge it is the only study to specically evaluate stk11 co - mutations with tp53 and kras and their relationship to response to rst - line systemic therapy in patients with metastatic or recurrent disease . 
the results show that stk11 / kras co - mutation is associated with a worse median pfs and os after front - line chemotherapy compared with patients who had stk11 mutation alone , whereas patients who had the stk11 / tp53 co - mutation had improved outcomes . we found that , in the context of an stk11 mutation , tp53 mutation is associated with better outcomes even in the presence of mutant kras . 
of interest , when examined outside the context of stk11 , tp53 mutations reportedly have a deleterious effect on os and response to platinum - based therapy , especially in early - stage disease.19 - 22 tp53 has not previously been found to be predictive or prognostic in the presence of a kras mutation.9 , 10 mutations in the tp53 binding sites of the stk11 promoter have been associated with decreased stk11 expression in endometrial cancer.15 in nsclc , 82% of tp53 mutations are in the dna binding region ; therefore , a mutation in tp53 in nsclc could lead to decreased expression of a deleterious stk11 protein , such as a gain - of - function stk11 mutation in exons 1 to 2.6 , 23 however , we observed a survival benet for tp53 co - mutation with stk11 that was independent of the location of the stk11 mutation . 
univariable and multivariable cox regression models of the effect of mutation status and covariables on the risk of death ( ie , overall survival )  . reference for stk11 exon 1 / 2 is a mutation in stk11 exon 3 - 9 . 
the proportion of patients with stk11 mutations in exons 1 and 2 in our cohort was similar to that of the cohort described by p ecuchet et al6 ( 35% v 25% ) , who came to a different conclusion . 
although some patients in our study had earlystage progression ( 37.1% ) , patients with early - stage nonprogressive disease and patients who never received any systemic therapy were formally excluded ( fig 1 )  . 
therefore , if stk11ex1 - 2 mutations do confer a higher risk of recurrence after early - stage disease , we would not have been able to identify this risk , given the study design . in the context of an stk11 mutation , we found that kras mutation in the absence of tp53 co - mutation conferred a signicantly worse pfs and os after rst - line systemic therapy for metastatic or recurrent disease . 
facchinetti et al3 also found that stk11 / kras co - mutated tumors had a higher metastatic burden and a trend toward worse os . this deleterious interaction between stk11 and kras may be explained by previous data showing that stk11 mutations enhance kras mutationassociated gene expression.11 in theory , this interaction would lead to augmentation of downstream kras signaling driving tumorigenesis . 
this is also supported by the observation that an acceleration of kras - induced tumorigenesis and metastasis has been found in stk11 - null mice as well as in humans who lack stk11 expression.4 , 15 in a separate study , arbour et al9 found that kras / stk11 co - mutations were associated with shorter os in univariable analysis but not in multivariable analysis . 
in their cohort , stk11 co - mutation status with keap1 or nfe2l2 could have contributed to a shorter os.9 keap1 / nfe2l2 comutation occurred in 63% ( 60 of 95 ) of stk11 mutations in their cohort and was highly correlated with the kras / stk11 subgroup in another study.9 , 10 they did not report a correlation between keap1 / nfe2l2 and tp53 mutations . 
the tumor and plasma ngs panels reported in our study did not include keap1 or nfe2l2 mutations , so we were unable to assess the effect of these mutations on outcome . detection of kras and tp53 mutations via plasma or tissue raises the possibility that the detected mutations may be due to clonal hematopoiesis ( ch ) in the blood . 
in another series , ve of 33 tp53 mutations detected by plasma ngs were found in peripheral - blood cells but not in the tumor.24 the same series reported that most jak2 , some tp53 , and rare kras mutations detected in cell - free dna are from ch and not from the tumor . 
in our cohort , there was no signicant difference in the proportion of tp53 or kras mutations detected in tumor versus plasma ( table 1 )  . according to the series by hu et al , 24 it is possible that approximately one of the seven tp53 mutations detected by plasma testing was from ch ; even if true , this small proportion is unlikely to change our results . 
in addition , ch is associated with worse outcome after therapy , and we report better outcomes with a tp53 mutation.25 therefore , this possible misclassication would bias our result toward the null and imply that the observed association may be stronger than reported.26 limitations that must be our study has additional addressed . 
 outcomes in nsclc by stk11 co - mutations status study , we used a real - world measurement of pfs dened as time from the start of treatment until radiologic progression , clinical deterioration , death , or change of therapy . this has been shown to be an appropriate surrogate for response evaluation criteria in solid tumors ( recist ) based pfs used in clinical trials.27 in addition , studies that many commercially available assays do not disclose how they determine whether an alteration is disease associated ; thus , there may be variation among vendors in how they categorize mutations . look to characterize the prognostic or predictive signicance of mutations in a specic gene have used different denitions of mutation ( eg , nonsynonymous , pathogenic )  . 
we initially used all nonsynonymous mutations in stk11 but then performed a subset analysis using only disease - associated stk11 mutations ( ie , mutations classied as disease associated or pathogenic on the molecular report )  . 
this analysis is limited by the small sample sizeonly ve patients were in the da - stk11 / kras / tp53 co - mutation groupand so should be considered exploratory . 
future work must be done to standardize how classication of molecular alterations and identication inuence response to therapy and of mutations that prognosis . in summary , this study shows that the co - mutation status of stk11 - mutated nsclc contributes to the heterogeneity of this molecular subgroup . 
marmarelis stock and other ownership interests : gilead sciences , portola pharmaceuticals , merck , bluebird bio consulting or advisory role : boehringer ingelheim other relationship : novartis research funding : lilly ( inst ) travel , accommodations , expenses : trizell wei - ting hwang research funding : janssen ( i ) jeffrey c . 
thompson consulting or advisory role : oncocyte jason rosenbaum consulting or advisory role : genentech , roche , abbvie , bristol - myers squibb travel , accommodations , expenses : agilent , bristol - myers squibb , takeda , abbvie , genentech , roche joshua m . 
bauml consulting or advisory role : bristol - myers squibb , merck , astrazeneca , genentech , celgene , boehringer ingelheim , guardant health , takeda research funding : merck ( inst ) , carevive systems ( inst ) , novartis ( inst ) , incyte ( inst ) , bayer ( inst ) , janssen ( inst ) , astrazeneca ( inst ) , takeda ( inst ) christine ciunci research funding : celgene ( inst ) , merck ( inst ) roger b . 
cohen consulting or advisory role : heat biologics , takeda , alkermes , kyn therapeutics , innate pharma , cantargia ab , genocea biosciences research funding : heat biologics ( inst ) , merck ( inst ) , celldex ( inst ) , innate pharma ( inst ) , kyn therapeutics ( inst ) , xencor ( inst ) , genocea biosciences ( inst ) travel , accommodations , expenses : heat biologics , takeda , innate pharma , kyn therapeutics , alkermes corey j . 
 bange et al consulting or advisory role : genentech , roche , lilly , imclone , merck , abbott biotherapeutics , bayer , onyx , clarient , clovis oncology , celgene , cancer support community , bristol - myers squibb , ariad , takeda , astrazeneca , pzer , novocure research funding : merck ( inst ) , advantagene ( inst ) , clovis oncology ( inst ) , celegene ( inst ) , inovio pharmaceuticals ( inst ) , ariad ( inst ) , glaxosmithkline ( inst ) , genentech ( inst ) , roche ( inst ) , stem centrx ( inst ) , lilly ( inst ) other relationship : lilly , amgen , peregrine pharmaceuticals , synta erica carpenter honoraria : astrazeneca research funding : merck , janssen , becton dickinson patents , royalties , other intellectual property : invention disclosure entitled , methods and compositions for treating neuroblastoma ; invention disclosure entitled , methods and compositions for identifying , diagnosing and treating neuroblastoma travel , accommodations , expenses : astrazeneca , foundation medicine charu aggarwal consulting or advisory role : genentech , bristol - myers squibb , lilly , celgene , medimmune research funding : genentech ( inst ) , roche ( inst ) , incyte ( inst ) , macrogenics ( inst ) , merck sharp & dohme ( inst ) , astrazeneca ( inst ) , medimmune ( inst ) no other potential conicts of interest were reported . references cheng tyd , cramb sm , baade pd , et al : the international epidemiology of lung cancer : latest trends , disparities , and tumor characteristics . 
oncogene 26 : 5911 - 5918 , 2007 facchinetti f , bluthgen mv , tergemina - clain g , et al : lkb1 / stk11 mutations in nonsmall - cell lung cancer patients : descriptive analysis and prognostic value . lung cancer 112 : 62 - 68 , 2017 gill rk , yang sh , meerzaman d , et al : frequent homozygous deletion of the lkb1 / stk11 gene in nonsmall - cell lung cancer . 
nature 448 : 807 - 810 , 2007 p ecuchet n , laurent - puig p , mansuet - lupo a , et al : different prognostic impact of stk11 mutations in non - squamous nonsmall - cell lung cancer . 
oncotarget 8 : 23831 - 23840 , 2017 dahmani r , just pa , delay a , et al : a novel lkb1 isoform enhances ampk metabolic activity and displays oncogenic properties . 
oncogene 34 : 2337 - 2346 , 2015 chen z , cheng k , walton z , et al : a murine lung cancer co - clinical trial identies genetic modiers of therapeutic response . 
nature 483 : 613 - 617 , 2012 arbour kc , jordan e , kim hr , et al : effects of co - occurring genomic alterations on outcomes in patients with kras - mutant nonsmall - cell lung cancer . 
skoulidis f , byers la , diao l , et al : co - occurring genomic alterations dene major subsets of kras - mutant lung adenocarcinoma with distinct biology , immune proles , and therapeutic vulnerabilities . 
schabath mb , welsh ea , fulp wj , et al : differential association of stk11 and tp53 with kras mutationassociated gene expression , proliferation , and immune surveillance in lung adenocarcinoma . 
co nn , iglesias d , celestino j , et al : loss of lkb1 in high - grade endometrial carcinoma : lkb1 is a novel transcriptional target of p53 . 
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deben c , deschoolmeester v , lardon f , et al : tp53 and mdm2 genetic alterations in nonsmall - cell lung cancer : evaluating their prognostic and predictive value . 
ahrendt sa , hu y , buta m , et al : p53 mutations and survival in stage i nonsmall - cell lung cancer : results of a prospective study . 
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kandioler d , stamatis g , eberhardt w , et al : growing clinical evidence for the interaction of the p53 genotype and response to induction chemotherapy in advanced nonsmall - cell lung cancer . 
shajani - yi z , de abreu fb , peterson jd , et al : frequency of somatic tp53 mutations in combination with known pathogenic mutations in colon adenocarcinoma , nonsmall - cell lung carcinoma , and gliomas as identied by next - generation sequencing . 
coombs cc , zehir a , devlin sm , et al : therapy - related clonal hematopoiesis in patients with non - hematologic cancers is common and associated with adverse clinical outcomes . 
bartlett c , mardekian j , cotter m , et al : concordance of real - world progression - free survival ( pfs ) on endocrine therapy as rst line treatment for metastatic breast cancer using electronic health record with proper quality control versus conventional pfs from a phase 3 trial . 
a positron emission tomography computed tomography ( pet - ct ) scan in april 2012 demonstrated extensive malignancy in the oral cavity with bilateral level ib node metastases and a suggestive fluorodeoxyglucose - avid subcutaneous lesion posterior to the sixth cervical spinous process . 
he had a smoking history of 60 pack - years and denied alcohol use , and he had no family history of cancer . the patient received induction chemotherapy with docetaxel , cisplatin , and fluorouracil . 
the patient was enrolled in a randomized , placebo - controlled , phase ii study that consisted of docetaxel and cisplatin or carboplatin with or without erlotinib ( clinicaltrials . gov identifier : nct01064479 )  . 
unblinding of the study revealed that he received erlotinib . the patient was referred to the phase i clinic and participated in the impact2 trial , a randomized trial in precision medicine ( clinicaltrials . gov identifier : nct02152254 )  . 
he was randomly assigned to receive targeted therapy and was enrolled in a study with a selective panfgfr inhibitor that began in september 2015 . ecaterina ileana dumbrava rasha alfattal vincent a . 
next - generation sequencing genomic profile by foundation one ( august 2015 ) genomic profile genomic alterations fgf19 amplification ccnd1 amplification fgf4 amplification ccnd2 amplification fgf23 amplification cdkn2a / b loss fgf3 amplification chd2 d213n fgf6 amplification crebbp r1392 * emsy amplification kdm5a amplification kras amplification myc duplication exons 2 and 3 tp53 e204 * variants of unknown significance akt2 e323q atm e322d igf1r s909c klhl6 amplification atr amplification notch2 t239s bcl6 amplification pik3ca amplification blm r543h pik3cb amplification card11 truncation pik3r2 r559h cdkn1b amplification prdm1 k188e chd4 amplification ranbp2 amplification dicer1 a948t sox2 amplification ephb1 amplification terc amplification grm3 amplification prkci amplification note . 
other adverse events included grade 1 hand - foot syndrome , xerostomia , and mucositis . in march 2016 , ct imaging after six cycles demonstrated a complete radiologic response ( fig 3 )  . 
he then underwent whole - brain radiation therapy , and 5 weeks after the completion of this treatment , he died of acute myocardial infarction . discussion to our knowledge , this is the first case of a complete response to an fgfr inhibitor in a patient with hnscc harboring several fibroblast growth factor ( fgf ) amplifications . 
alterations of the fgf / fgfr signaling pathways play important roles in carcinogenesis , stimulating cancer cell proliferation and angiogenesis.8 deregulation of the fgfr pathway occurs in fgf ligands ( fgfs ) or receptors via gene mutations , translocations , fusions , or amplifications that lead to protein overexpression that results in the activation of the downstream signaling pathway.9 the fgfr family has four highly conserved transmembrane receptor tyrosine kinases ( fgfr1 to fgfr4 ) that differ in their ligand affinity and tissue distribution . 
selected genomic alterations are indicated by an asterisk ( * ) : fibroblast growth factor receptor ( fgfr ) pathway ( fgf19 , fgf4 , fgf23 , fgf3 , and fgf6 amplifications )  . 
selected variants of unknown significance are indicated by a filled square ( ) : kras amplification , pik3ca and pik3cb amplifications , and pik3r2 and protein kinase b ( akt ) mutations . 
binding of fgfs to fgfrs induces dimerization of the intracellular domain of the receptor and downstream activation of signaling.10 with the advent of next - generation sequencing , aberrations in fgfrs have been better characterized than fgf alterations . 
the most common mechanisms of fgf activation are gene amplification that leads to overexpression and mutations that lead to increased affinity for fgfrs.9 fgf amplifications have been observed in several tumor types.12 in hnscc , fgfr1 overexpression has been reported in > 75% of both human papillomavirus ( hpv ) positive and negative hnscc , and it is associated with poor survival.13 fgfr1 , fgfr2 , and fgfr3 amplifications , as well as fgfr3 - tacc3 fusions , have been identified in hpv - positive tumors.14 fgf3 , fgf4 , fgf19 , and ccnd1 , also amplified in this patient , colocalize on the same amplicon of 11q13 and are frequently coamplified . 
 in addition , 11q13 amplification is prevalent in hnsccparticularly hpv unrelated and tobacco inducedand has been reported to be associated with poor prognosis.15 , 16 although the hpv status of our patient was unknown , he was a heavy smoker throughout the course of his disease . there has been exponential progress in the field of fgfr targeting , owing to the development of novel agents that inhibit fgf ligands and receptors . 
because they simultaneously target vascular endothelial growth factor receptor , platelet - derived growth factor receptor , and fgfr signaling pathways , these compounds are being developed primarily as antiangiogenic agents . 
azd4547 has been investigated in fgfr2 - amplified gastric cancers and in fgfr1 - amplified breast cancer and nsclc.24 - 26 bgj398 induced a 40% overall response rate in patients with urothelial cancer and fgfr alterations . 
21 debio 1347 may inhibit the fgfr2 mutation v564f , which causes resistance to other drugs.27 monoclonal antibodies that target fgf / fgfr signaling by blocking ligand binding or preventing receptor dimerization are in clinical development.28 adverse effects associated with nonselective fgfr inhibitors include vascular endothelial growth factor receptorrelated toxicities , and with selective fgfr inhibitors , hyperphosphatemia as a result of fgf23 signaling.17 , 29 in our patient , hyperphosphatemia was managed with a low - phosphate diet , phosphate binders , and a dose reduction . 
use of a selective pan - fgfr inhibitor that targets multiple fgf amplificationsfgf3 , fgf4 , fgf6 , fgf19 , and fgf23was associated with a durable complete response in a patient with hnscc . 
borad mj , champion md , egan jb , et al : integrated genomic characterization reveals novel , therapeutically relevant drug targets in fgfr and egfr pathways in sporadic intrahepatic cholangiocarcinoma . 
smeets sj , braakhuis bjm , abbas s , et al : genome - wide dna copy number alterations in head and neck squamous cell carcinomas with or without oncogene - expressing human papillomavirus . 
chae yk , ranganath k , hammerman ps , et al : inhibition of the fibroblast growth factor receptor ( fgfr ) pathway : the current landscape and barriers to clinical application . 
gozgit jm , wong mj , moran l , et al : ponatinib ( ap24534 ) , a multitargeted pan - fgfr inhibitor with activity in multiple fgfr - amplified or mutated cancer models . 
soria j - c , debraud f , bahleda r , et al : phase i / iia study evaluating the safety , efficacy , pharmacokinetics , and pharmacodynamics of lucitanib in advanced solid tumors . 
milowsky mi , dittrich c , durn i , et al : phase 2 trial of dovitinib in patients with progressive fgfr3 - mutated or fgfr3 wild - type advanced urothelial carcinoma . 
nogova l , sequist lv , perez garcia jm , et al : evaluation of bgj398 , a fibroblast growth factor receptor 1 - 3 kinase inhibitor , in patients with advanced solid tumors harboring genetic alterations in fibroblast growth factor receptors : results of a global phase i , dose - escalation and dose - expansion study . 
tabernero j , bahleda r , dienstmann r , et al : phase i dose - escalation study of jnj - 42756493 , an oral pan - fibroblast growth factor receptor inhibitor , in patients with advanced solid tumors . 
saka h , kitagawa c , kogure y , et al : safety , tolerability and pharmacokinetics of the fibroblast growth factor receptor inhibitor azd4547 in japanese patients with advanced solid tumours : a phase i study . 
paik pk , shen r , berger mf , et al : a phase ib open - label multicenter study of azd4547 in patients with advanced squamous cell lung cancers . 
van cutsem e , bang y - j , mansoor w , et al : a randomized , open - label study of the efficacy and safety of azd4547 monotherapy versus paclitaxel for the treatment of advanced gastric adenocarcinoma with fgfr2 polysomy or gene amplification . 
seckl m , badman pd , liu x , et al : radical trial : a phase ib / iia study to assess the safety and efficacy of azd4547 in combination with either anastrozole or letrozole in er positive breast cancer patients progressing on these aromatase inhibitors ( ais )  . 
henner voss m , hierro c , heist rs , et al : debio 1347 , an oral fgfr inhibitor : results from a first - in - human , phase i dose - escalation study in patients with fgfr genomically activated advanced solid tumors . 
hierro c , rodon j , tabernero j : fibroblast growth factor ( fgf ) receptor / fgf inhibitors : novel targets and strategies for optimization of response of solid tumors . 
kono sa , marshall me , ware ke , et al : the fibroblast growth factor receptor signaling pathway as a mediator of intrinsic resistance to egfr - specific tyrosine kinase inhibitors in non - small cell lung cancer . 
terai h , soejima k , yasuda h , et al : activation of the fgf2 - fgfr1 autocrine pathway : a novel mechanism of acquired resistance to gefitinib in nsclc . 
ware ke , marshall me , heasley lr , et al : rapidly acquired resistance to egfr tyrosine kinase inhibitors in nsclc cell lines through de - repression of fgfr2 and fgfr3 expression . 
mizukami t , togashi y , naruki s , et al : significance of fgf9 gene in resistance to antiegfr therapies targeting colorectal cancer : a subset of colorectal cancer patients with fgf9 upregulation may be resistant to anti - egfr therapies . 
george , md1 ; and susan halabi , phd8 purpose androgen receptor splice variant 7 ( ar - v7 ) detection in circulating tumor cells ( ctcs ) is associated with a low probability of response and short progression - free ( pfs ) and overall survival ( os ) in men with metastatic castration - resistant prostate cancer ( mcrpc ) treated with enzalutamide or abiraterone . 
os , conrmed prostate - specic antigen ( psa ) , and objective radiologic responses were secondary end points . results we enrolled 118 men with mcrpc treated with abiraterone or enzalutamide , 51 of whom received subsequent docetaxel or cabazitaxel . 
all patients provided written informed consent under stitutional review board approval at all participating centers within the department of defensefunded prostate cancer clinical trial consortium.16 study design and assessments prophecy is a prospective multicenter study evaluating the ability of baseline ( pretreatment ) ar - v7 status in ctcs to predict treatment outcomes with abiraterone or enzalutamide as well as subsequent taxane chemotherapy upon disease progression . 
cellsearch ( menarini silicon biosystems , huntington valley , pa ) ctc enumeration was performed at these time points for all patients and processed in a college of american physicians / clinical laboratory improvement amendmentsapproved central laboratory at memorial sloan kettering cancer center.17 , 18 treatment selection was at the discretion of the treating physician without knowledge of ar - v7 status . 
all data sets were separately sent to the study statistician ( s.h. ) , who unblinded the data after database lock . analysis of ctcs ctcs were analyzed in two central laboratories , each blinded to the results of the other . 
baseline pretaxane characteristics of patients enrolled according to epic sciences ar - v7 status based on ar - v7 detection after abiraterone or enzalutamide and before taxane epic sciences ar - v7 status ( % ) positive ( n = 8 ) negative ( n = 42 ) 62 - 79 45 - 87 6 - 881 96.5 1 - 850 0 - 325 characteristic age , years median range race white black other gleason sum 8 - 10 kps 90 poor - risk feature psa , ng / ml median range taxane used docetaxel cabazitaxel months median range hemoglobin , 12 g / dl elevated alp elevated baseline serum ldh presence of liver metastasis presence of clinically signicant pain requiring cellsearch ctcs , cells per 7.5 ml opiates range median , % ( n = 32 ) psadt , 3 months prior docetaxel for mhspc  . 
20 bone metastases time from ar - v7 sample to chemotherapy start , 0 - 17 0 - 33 abbreviations : alp , alkaline phosphatase ; ar - v7 , androgen receptor splice variant 7 ; ctc , circulating tumor cell ; kps , karnofsky performance score ; ldh , lactate dehydrogenase ; mhspc , metastatic hormone - sensitive prostate cancer ; psa , prostate - specic antigen ; psadt , prostate - specic antigen doubling time . registration to clinical or radiographic progression or death , whichever occurred rst . 
radiographic progression was assessed at each center using pcwg3 - modied recist ( version 1.1 ) soft tissue and bone scan criteria.22 clinical progression was dened as a composite end point including death , escalating pain or other symptomatic progression , initiation of new systemic therapy , or a skeletal - related event . secondary clinical end points included conrmed 50% prostate - specic antigen ( psa ) decline , radiographic response per recist ( verson 1.1 ) , 23 and os , and these same outcomes for subsequent taxane chemotherapy . data analysis the primary objective of prophecy was to validate that patients with pretreatment ar - v7negative ctcs have prolonged pfs with abiraterone or enzalutamide compared with ar - v7positive patients . 
with longer follow - up , analyses of the time - toevent end points ( pfs and os ) were also updated , and patients who received taxane chemotherapy were observed for response , radiographic progression , and death . 
details regarding study design have been published elsewhere.9 patients with no evaluable ctcs were considered ar - v7 negative , and all patients with sufcient blood collection were analyzed regardless of their evaluable ctcs . 
in secondary analyses , the proportional hazards model was used for assessing the prognostic value of ar - v7 status for pfs and os after adjusting for validated prognostic factors ( risk score ) .14 , 15 , 24 for taxane outcomes , pfs was dened from the date of starting chemotherapy to clinical or radiographic progression or death , whichever occurred rst . 
no power or sample size analysis is provided for this secondary descriptive analysis , because prophecy was powered around the primary objective and previously reported . between may 2015 and january 2017 , we prospectively enrolled 118 men with high - risk mcrpc who were initiating treatment with abiraterone , enzalutamide , or both at one of ve academic medical centers . 
baseline characteristics of the cohort were previously published and included 36 men who had received prior enzalutamide or abiraterone therapy.9 of these 118 men treated with subsequent ar inhibitor therapy , 51 experienced progression and were treated with taxane chemotherapy , including docetaxel ( n = 42 ) or cabazitaxel ( n = 9 ; consort diagram provided in appendix fig a1 )  . 
baseline characteristics of these patients at the time of taxane chemotherapy are listed in table 1 based on epic sciences ar - v7 status and appendix table a1 based on johns hopkins ar - v7 status . 
as of the nal database lock on october 15 , 2019 , median follow - up times from study registration ( before abiraterone or enzalutamide treatment ) and taxane initiation were 35 and 23 months , respectively . 
table 2 and figure 1 summarize the results of pfs and os by baseline ar - v7 status for each ctc assay . conrmed 50% psa declines were observed in 11% and 30% of patients with ar - v7positive and ar - v7negative disease by johns hopkins assay , respectively , and radiographic responses ( complete or partial responses by recist [ version 1.1 ] criteria ) were seen in 7% and 9% of patients , respectively . 
results were unchanged when two patients with psa - only progression were considered censored ( appendix table a3 )  . os did not differ from the start of taxane chemotherapy by ar - v7 status . 
table 3 and figure 2 summarize the results of pfs and os by baseline ar - v7 status for each ctc assay . conrmed 50% psa responses with taxane therapy were observed in 36% and 32% of patients with ar - v7positive versus ar - v7negative disease by johns hopkins assay , respectively , and radiographic responses ( complete or partial responses by recist [ version 1.1 ] ) were observed in 10% and 20% of patients , respectively . 
conrmed 50% psa responses were observed in 40% and 33% of those with ar - v7positive versus ar - v7negative disease by epic sciences nuclear assay , respectively , and radiographic responses ( complete or partial responses by recist [ version 1.1 ] ) were observed in 13% and 17% of patients , respectively ( appendix fig a2 )  . 
 a pre - abi / enza at progression on abi / enza at progression on taxane nuclear localized ar - v7 ctc total ctc nuclear localized ar - v7 ctc nuclear localized ar - v7 ctc total ctc total ctc 123456789 2345789 * * * * * * * * patient id patient id patient id armstrong et al 123456789 2345789 patient id patient id patient id 123456789 2345789 patient id patient id patient id * * * * * * * fig 3 . 
bar plot demonstrating heterogeneity of androgen receptor splice variant 7 ( ar - v7 ) expression in circulating tumor cells ( ctcs ) by either the johns hopkins ( jhu ) messenger rna assay or the epic sciences nuclear protein assay collected from men in the prophecy study at one of three time points : ( a ) before abiraterone ( abi ) or enzalutamide ( enza ) therapy , ( b ) at progression during abiraterone or enzalutamide treatment , and ( c ) at progression during subsequent taxane chemotherapy . 
for the epic sciences nuclear protein assay , approximately 1 ml of blood is analyzed , and total and nuclear - localized ar - v7positive ctcs are expressed per 1 ml of blood . 
 ( * ) no data . disease pretreatment who received abiraterone or enzalutamide and pretaxane therapy . finally , we examined how ar - v7 changes during the treatment course from before abiraterone or enzalutamide to progression and then after progression during taxane chemotherapy . 
at baseline , ar - v7 positivity was 10% versus 24% by epic sciences and johns hopkins assays , respectively , with a majority of men with ar - v7positive disease by epic sciences ( nine of 11 ; 82% positive agreement ) also testing positive by johns hopkins assay . johns hopkinspositive , epic sciencesnegative results were observed , particularly in those men with low epic sciences ctcs or nonnuclear ar - v7 protein expression . although a majority of ctcs in men with mcrpc were ar - v7 negative , even in those with ar - v7positive disease , the proportion of ar - v7positive cells ranged from 1% to 100% ( median , 20% ; fig 3 )  . 
at progression during taxane chemotherapy , 33% ( four of 12 ) and 48% ( 12 of 25 ) of evaluable men had ar - v7 detected by epic sciences and johns hopkins criteria , respectively ( appendix table a4 )  . 
these results conrm previously published data showing ar - v7positive disease remains sensitive to taxane chemotherapy.11 - 13 in the secondor third - line mcrpc setting , cabazitaxel improves os and should be considered a reasonable third - line treatment option , 5 and docetaxel or cabazitaxel are effective treatments after progression with abiraterone or enzalutamide , with pfs estimates of 4 to 6 months in these poor - risk men.14 , 24 , 26 , 27 the results are particularly important with regard to current practice , given the recent proven benet and use of these same ar inhibitors in the metastatic hormone - sensitive pc and nonmetastatic crpc settings , where ar therapy cross - resistance concerns remain when a patient experiences progression to mcrpc during therapy.28 - 32 a majority of men with ar - v7positive disease by epic sciences assay ( nine [ 82% ] of 11 ) were also positive by johns hopkins assay ; however , 17 ( 60% ) of 28 patients with positive disease by johns hopkins assay were negative by epic sciences assay at baseline . 
these differences largely reect the differential sensitivities of the assays for ar - v7 detection in ctc - based rna expression versus protein and the distinction between nuclear versus cytoplasmic localization . 
some patients developed ar - v7positive disease at progression during abiraterone or enzalutamide treatment , despite being ar - v7 negative at baseline , whereas some men with ar - v7positive disease converted to arv7negative status at progression , illustrating the need to assess ctc biomarker status at each management decision point ( fig 3 )  . 
a limitation of our study includes the lack of random assignment to taxane or ar therapy based on arv7 test results , and as such , our results show a prognostic rather than predictive utility . 
 armstrong et al support supported by a grant from the prostate cancer foundation and movember ; by the department of defense prostate cancer clinical trials consortium , which provided infrastructural support ; by the national institutes of health and grant 1r01ca233585 - 01 , duke cancer institute ( dci ) grant no . 
p30 ca014236 , and dci shared resources for biostatistics , ow cytometry , and sequencing and genomic technologies ( a.j.a. ) ; in part by department of defense grants no . 
george , susan halabi manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors consulting or advisory role : bayer , sano , dendreon , medivation , janssen biotech , pzer , astellas scientic and medical affairs , clovis oncology , astrazeneca speakers bureau : dendreon , bayer research funding : dendreon ( inst ) , sano ( inst ) , bayer ( inst ) , pzer ( inst ) , novartis ( inst ) , janssen oncology ( inst ) , medivation ( inst ) , astellas pharma ( inst ) , gilead sciences ( inst ) , roche / genentech ( inst ) , active biotech ( inst ) , bristol myers squibb ( inst ) , constellation pharmaceuticals ( inst ) , merck ( inst ) patents , royalties , other intellectual property : circulating tumor cell novel capture technology ( inst ) travel , accommodations , expenses : dendreon , janssen biotech , bayer , astellas scientic and medical affairs jun luo consulting or advisory role : sun pharma , janssen oncology , tolero pharmaceuticals research funding : sano ( inst ) , orion pharma ( inst ) , mirati therapeutics ( inst ) , gilead sciences ( inst ) , astellas pharma ( inst ) , constellation pharmaceuticals ( inst ) , calibr ( inst ) , cardiff oncology ( inst ) patents , royalties , other intellectual property : coinventor of a technology assigned to johns hopkins university , which licensed to tokai pharmaceuticals ( inst ) ; coinventor of a technology licensed to qiagen ( inst ) ; coinventor of a technology licensed to a&g pharmaceuticals ( inst ) david m . 
nanus consulting or advisory role : roche / genentech research funding : novartis ( inst ) , boehringer ingelheim ( inst ) , zenith epigenetics ( inst ) , astrazeneca ( inst ) , immumedics ( inst ) , janssen ( inst ) , clovis oncology ( inst ) , pzer ( inst ) paraskevi giannakakou employment : novartis ( i ) stock and other ownership interests : novartis ( i ) patents , royalties , other intellectual property : coinventor on international patent application docket no . 
danila honoraria : angle , bayer , screencell , janssen oncology , pzer , aximmune , pzer , clovis oncology , astellas pharma consulting or advisory role : angle , bayer , sanador , aximmune , pzer , clovis oncology , astellas pharma , janssen scientic affairs research funding : prostate cancer foundation , genentech , janssen research & development ( inst ) patents , royalties , other intellectual property : gene expression prole associated with prostate cancer travel , accommodations , expenses : cambridge healthtech institute , prostate cancer foundation , screencell , stopcancer , american austrian open medical institute , janssen biotech , genzyme , pzer , janssen scientic affairs , astellas pharma andrew j . 
berry honoraria : pzer , merck , genomic health , janssen oncology consulting or advisory role : merck , pzer , genomic health , janssen oncology research funding : merck ( inst ) travel , accommodations , expenses : merck , pzer , genomic health , janssen oncology tian zhang leadership : capio biosciences ( i ) , archimmune therapeutics ( i ) stock and other ownership interests : capio biosciences ( i ) , archimmune therapeutics ( i ) , nanorobotics ( i ) honoraria : exelixis , genentech / roche , mjh life sciences , pacic genuity consulting or advisory role : janssen , genentech / roche , sano , exelixis , astrazeneca , pzer , bristol myers squibb , foundation medicine , pharmacyclics , amgen , merck , seattle genetics speakers bureau : exelixis , genentech / roche , genomic health , sano research funding : janssen ( inst ) , acerta pharma ( inst ) , pzer ( inst ) , merrimack ( inst ) , stem centrx ( inst ) , novartis ( inst ) , omniseq ( inst ) , personal genome diagnostics ( inst ) , regeneron ( inst ) , merck ( inst ) , mirati therapeutics ( inst ) , astellas pharma patents , royalties , other intellectual property : circulating tumor cell novel capture by c - met technology ( inst ) ; prochelators as targeted prodrugs for prostate cancer ( inst ) travel , accommodations , expenses : acerta pharma , genomic health , astrazeneca michael r . 
harrison consulting or advisory role : bayer , sano , exelixis , genentech , argos therapeutics , fujilm , janssen oncology , astrazeneca , pzer , bristol myers squibb speakers bureau : genentech , exelixis research funding : argos therapeutics ( inst ) , bristol myers squibb ( inst ) , genentech ( inst ) , pzer ( inst ) , medivation / astellas pharma ( inst ) , merck ( inst ) , clovis oncology ( inst ) , acerta pharma ( inst ) , astrazeneca ( inst ) changxue lu patents , royalties , other intellectual property : inventor of the patent that was licensed to qiagen and received royalty joseph d . 
scher leadership : asterias biotherapeutics stock and other ownership interests : asterias biotherapeutics honoraria : research to practice consulting or advisory role : janssen biotech , amgen , janssen research & development , menarini silicon biosystems , wirb - copernicus group , essa , sano , ambry genetics , konica minolta , pzer , bayer research funding : janssen ( inst ) , illumina ( inst ) , epic sciences ( inst ) , menarini silicon biosystems ( inst ) , thermosher scientic biomarkers ( inst ) travel , accommodations , expenses : asterias biotherapeutics , menarini silicon biosystems , amgen , wirb - copernicus group , konica minolta , essa , prostate cancer foundation , sano , bayer , phosplatin therapeutics richard wenstrup employment : epic sciences leadership : epic sciences stock and other ownership interests : epic sciences consulting or advisory role : blueprint genetics , resolys patents , royalties , other intellectual property : patent royalties from assurexhealth travel , accommodations , expenses : epic systems scott t . 
tagawa consulting or advisory role : medivation , astellas pharma , dendreon , janssen , bayer , genentech , endocyte , immunomedics , karyopharm therapeutics , abbvie , tolmar , qed , amgen , sano , pzer , clovis oncology , novartis , genomic health , point biopharma research funding : lilly ( inst ) , sano ( inst ) , janssen ( inst ) , astellas pharma ( inst ) , progenics ( inst ) , millennium pharmaceuticals ( inst ) , amgen ( inst ) , bristol myers squibb ( inst ) , dendreon ( inst ) , rexahn pharmaceuticals ( inst ) , bayer ( inst ) , genentech ( inst ) , newlink genetics ( inst ) , inovio pharmaceuticals ( inst ) , astrazeneca ( inst ) , immunomedics ( inst ) , novartis ( inst ) , aveo ( inst ) , boehringer ingelheim ( inst ) , merck ( inst ) , stem centrx ( inst ) , karyopharm therapeutics ( inst ) , abbvie ( inst ) , medivation ( inst ) , endocyte ( inst ) , exelixis ( inst ) , clovis oncology ( inst ) travel , accommodations , expenses : sano , immunomedics , amgen uncompensated relationships : telix pharmaceuticals , atlab pharma , phosplatin therapeutics emmanuel s . 
antonarakis honoraria : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , janssen biotech , essa , merck , astrazeneca , clovis oncology , lilly , bayer research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : coinventor of a biomarker technology that has been licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation daniel j . 
george leadership : capio biosciences honoraria : sano , bayer , exelixis , emd serono , onclive , pzer , urotoday , acceleron pharma , american association for cancer research , axess oncology , janssen oncology , millennium medical publishing consulting or advisory role : bayer , exelixis , pzer , sano , astellas pharma , innocrin pharma , bristol myers squibb , genentech , janssen , merck sharp & dohme , myovant sciences , astrazeneca , michael j . 
n engl j med 371 : 424 - 433 , 2014 de bono js , oudard s , ozguroglu m , et al : prednisone plus cabazitaxel or mitoxantrone for metastatic castration - resistant prostate cancer progressing after docetaxel treatment : a randomised open - label trial . 
n engl j med 368 : 138 - 148 , 2013 [ erratum : n engl j med 368 : 584 , 2013 ] tannock if , de wit r , berry wr , et al : docetaxel plus prednisone or mitoxantrone plus prednisone for advanced prostate cancer . 
n engl j med 351 : 1502 - 1512 , 2004 de wit r , de bono j , sternberg cn , et al : cabazitaxel versus abiraterone or enzalutamide in metastatic prostate cancer . 
n engl j med 381 : 2506 - 2518 , 2019 khalaf dj , annala m , taavitsainen s , et al : optimal sequencing of enzalutamide and abiraterone acetate plus prednisone in metastatic castration - resistant prostate cancer : a multicentre , randomised , open - label , phase 2 , crossover trial . 
ann oncol 24 : 1802 - 1807 , 2013 schrader aj , boegemann m , ohlmann ch , et al : enzalutamide in castration - resistant prostate cancer patients progressing after docetaxel and abiraterone . 
eur urol 65 : 30 - 36 , 2014 armstrong aj , halabi s , luo j , et al : prospective multicenter validation of androgen receptor splice variant 7 and hormone therapy resistance in high - risk castration - resistant prostate cancer : the prophecy study . 
scher hi , graf rp , schreiber na , et al : assessment of the validity of nuclear - localized androgen receptor splice variant 7 in circulating tumor cells as a predictive biomarker for castration - resistant prostate cancer . 
scher hi , lu d , schreiber na , et al : association of ar - v7 on circulating tumor cells as a treatment - specic biomarker with outcomes and survival in castrationresistant prostate cancer . 
antonarakis es , lu c , luber b , et al : androgen receptor splice variant 7 and efcacy of taxane chemotherapy in patients with metastatic castration - resistant 14 . 
de bono js , scher hi , montgomery rb , et al : circulating tumor cells predict survival benet from treatment in metastatic castration - resistant prostate cancer . clin cancer res 14 : 6302 - 6309 , 2008 [ erratum : clin cancer res 15 : 1506 , 2009 ] 18 . 
scher hi , heller g , molina a , et al : circulating tumor cell biomarker panel as an individual - level surrogate for survival in metastatic castration - resistant prostate cancer . 
antonarakis es , lu c , luber b , et al : clinical signicance of androgen receptor splice variant - 7 mrna detection in circulating tumor cells of men with metastatic castration - resistant prostate cancer treated with rstand second - line abiraterone and enzalutamide . 
markowski mc , silberstein jl , eshleman jr , et al : clinical utility of clia - grade ar - v7 testing in patients with metastatic castration - resistant prostate cancer . ( clia ) laboratory setting . 
scher hi , morris mj , stadler wm , et al : trial design and objectives for castration - resistant prostate cancer : updated recommendations from the prostate cancer clinical trials working group 3 . 
halabi s , lin cy , small ej , et al : prognostic model predicting metastatic castration - resistant prostate cancer survival in men treated with second - line chemotherapy . 
scher hi , graf rp , schreiber na , et al : phenotypic heterogeneity of circulating tumor cells informs clinical decisions between ar signaling inhibitors and taxanes in metastatic prostate cancer . 
eisenberger m , hardy - bessard ac , kim cs , et al : phase iii study comparing a reduced dose of cabazitaxel ( 20 mg / m2 ) and the currently approved dose ( 25 mg / m2 ) in postdocetaxel patients with metastatic castration - resistant prostate cancer : proselica . 
oudard s , fizazi k , sengelv l , et al : cabazitaxel versus docetaxel as rst - line therapy for patients with metastatic castration - resistant prostate cancer : a randomized phase iii trialfirstana . 
armstrong aj , szmulewitz rz , petrylak dp , et al : arches : a randomized , phase iii study of androgen deprivation therapy with enzalutamide or placebo in men with metastatic hormone - sensitive prostate cancer . 
aggarwal r , huang j , alumkal jj , et al : clinical and genomic characterization of treatment - emergent small - cell neuroendocrine prostate cancer : a multiinstitutional prospective study . 
de laere b , van dam pj , whitington t , et al : comprehensive proling of the androgen receptor in liquid biopsies from castration - resistant prostate cancer reveals novel intra - ar structural variation and splice variant expression patterns . 
kohli m , ho y , hillman dw , et al : androgen receptor variant ar - v9 is coexpressed with ar - v7 in prostate cancer metastases and predicts abiraterone commun 7 : 13668 , 2016 resistance . 
de laere b , oeyen s , mayrhofer m , et al : tp53 outperforms other androgen receptor biomarkers to predict abiraterone or enzalutamide outcome in metastatic castration - resistant prostate cancer . 
 armstrong et al appendix assessed for eligibility ( n = 131 ) did not meet inclusion criteria ( n = 13 ) received hormone therapy abiraterone enzalutamide both ( n = 118 ) ( n = 55 ) ( n = 58 ) ( n = 5 ) progression during treatment death during treatment ( n = 105 ) ( n = 4 ) received subsequent taxane therapy docetaxel cabazitaxel ( n = 51 ) ( n = 42 ) ( n = 9 ) progression during treatment death during treatment ( n = 46 ) ( n = 3 ) fig a1 . 
waterfall plots of best overall prostate - specic antigen ( psa ) decline from pretaxane baseline during therapy with docetaxel or cabazitaxel according to ( a ) epic sciences and ( b ) johns hopkins androgen receptor splice variant 7 ( ar - v7 ) status . 
baseline pretaxane characteristics of patients enrolled according to johns hopkins ar - v7 status johns hopkins ar - v7 status ( % ) positive ( n = 20 ) 48 - 82 negative ( n = 31 ) 45 - 87 elevated baseline serum ldh presence of liver metastasis presence of clinically signicant pain requiring opiates cellsearch ctcs , cells per 7.5 ml baseline pretaxane characteristic age , years median range race white black other gleason sum 8 - 10 poor - risk feature hemoglobin , 12 g / dl elevated alp range median , % ( n = 37 ) psadt , 3 months prior docetaxel for mhspc  . 
long terra lucas shreshtha madaan kristin mattie danielle mckenna susan montgomery sarah nielsen jacquelyn powers kim rainey christina rybak michelle savage christina seelaus ( continued ) purpose multigene panels ( mgps ) are increasingly being used despite questions regarding their clinical utility and no standard approach to genetic counseling . 
how frequently genetic providers use mgp testing and how patient - reported outcomes ( pros ) differ from targeted testing ( eg , brca1 / 2 only ) are unknown . methods we evaluated use of mgp testing and pros in participants undergoing cancer genetic testing in the multicenter communication of genetic test results by telephone study ( clinicaltrials.gov identifier : nct01736345 ) , a randomized study of telephone versus in - person disclosure of genetic test results . 
genetic providers offered targeted or mgp testing based on clinical assessment . results since the inclusion of mgp testing in 2014 , 395 patients ( 66% ) were offered mgp testing . 
being offered mgp testing was significantly associated with not having ashkenazi jewish ancestry , having a history of cancer , not having a mutation in the family , not having made a treatment decision , and study site . 
after demographic adjustment , patients offered mgp testing had lower general anxiety ( p = .04 ) , state anxiety ( p = .03 ) , depression ( p = .04 ) , and uncertainty ( p = .05 ) pre - disclosure compared with patients offered targeted testing . 
there was a greater increase in change in uncertainty ( p = .04 ) among patients who underwent mgp testing . conclusion mgp testing was more frequently offered to patients with lower anxiety , depression , and uncertainty and was associated with favorable outcomes , with the exception of a greater increase in uncertainty compared with patients who had targeted testing . 
delivery of genetic testing results by telephone is one of several adaptations to the traditional genetic counseling practice model that have been studied in an effort to improve counseling access through the more efficient use of resources.3 - 5 beginning in 2012 , as part of the national cancer institute funded multicenter communication of genetic test results by telephone ( cogent ) clinical trial , patients eligible for brca1 / 2 genetic testing for hereditary breast or ovarian cancer risk assessment were recruited and randomly assigned to in - person or telephone disclosure of genetic test results . 
primary outcomes of the cogent study6 have demonstrated that telephone disclosure is noninferior to in - person counseling across all primary and secondary short term outcomes . a robust literature on patient - reported outcomes ( pros ) of brca1 / 2 and targeted genetic testing exists , including two randomized studies of telephone delivery of both pretesting and post - testing genetic services for patients considering genetic testing for these genes.3 , 5 cogent is , to our knowledge , the first randomized study to examine uptake of mgp tests in the population of patients presenting for risk assessment to a tertiary high - risk clinic , as well as to report on pros among patients receiving traditional targeted gene counseling and testing compared with patients receiving counseling and testing adapted to mgps . 
 in the current study , trends in testing choices with the advent of mgp testing and across the cogent study time period and participating sites are reported , and pros previously reported in aggregate are analyzed by counseling and testing modality selected for the patient . methods study design , setting , and participants the cogent study was a multicenter , randomized , noninferiority trial comparing the psychosocial and behavioral outcomes of phone versus in - person disclosure of genetic test results . 
 initially designed to include targeted brca1 / 2 testing only , the study eligibility was adapted in may 2014 to add all clinical germline genetic testing for hereditary breast , gynecologic , and / or gi cancer syndromes , allowing individuals receiving either targeted testing or mgp testing . 
participants were recruited after in - person pretest counseling with a genetic counselor and completed pros at the time of enrollment ( after pretest counseling [ t0 ] ) and after results disclosure ( t1 )  . random assignment after completion of the survey given after pretest counseling , participants were assigned to either the in - person arm or telephone ar random assignment was stratified by study site and sex only . 
participants who did not want to receive results by telephone and thus were not willing to be randomly assigned were permitted to self - select in - person disclosure and were analyzed separately . all 22 genetic counseling professionals used a tiered and binned counseling model for pretest sessions where mgp testing was offered.7 , 8 all disclosures were made using standardized communication protocols and visual aids.7 - 9 both a genetic counseling professional and a medical provider were present when results were provided in person , whereas individuals who received results by telephone were recommended to return to their institution to meet with a medical provider . 
patients responded on a seven - item likert scale and could mark not applicable . statistical analysis for baseline analyses , we characterized variables using means , proportions , standard deviations , and ranges for age . 
variables included in the tables and regressions included age , sex , race ( white v nonwhite ) , education ( college graduate v less than a college degree ) , jewish ethnicity ( no or missing v yes ) , number of firstand second - degree relatives with cancer , known cancer mutation , treatment decision , random assignment or self - selecting for in - person disclosure arm , and study site . 
we did not include in the imputation analyses individuals missing both t0 and t1 response data because we felt that such individuals had too much missing data to reliably impute data . 
the criterion for statistical significance was p < .05. results use and predictors of mgp testing versus targeted testing in total , 600 participants were offered genetic testing after inclusion of mgp testing ; 62.7% of participants ( 376 of 600 participants ) underwent mgp testing , whereas 37.3% of participants underwent targeted testing ( fig 1 )  . 
 targeted testing was most frequently offered to patients with a known familial mutation ( 86% ) and to patients of ashkenazi jewish ancestry ( 67% ) , a population in which three founder mutations in brca1 / 2 are found at high frequency ( prevalence of approximately 1 : 40 )  . 
of note , of 395 patients offered mgp testing by the genetic counselor , a small fraction ( 19 [ 4.8% ] of 395 patients ) declined mgp testing and chose targeted testing . 
characteristics associated with being more likely to be offered mgp testing were older age , female sex , nonashkenazi jewish heritage , personal history of cancer , no known familial mutation , nonrandomization status ( ie , preference for in - person disclosure ) , and study site . the percentage of patients offered mgp testing increased over time ( from 57% in 2014 to 66% in 2015 ; p = .02 ) and was found to vary significantly by study site ( range , 46% to 81% of all tests offered ; fig 2 )  . 
identification of carriers and true - negative results were higher in the targeted testing group , which is likely secondary to a higher number of patients with a known familial mutation ( table 1 )  . 
the frequency of uncertain variants was higher in the mgp group ( 25% v 2% with targeted testing )  . pros assessed by offer of targeted testing versus mgp testing in full models , adjusting for baseline variables , pros were assessed and compared by whether patients were offered mgp testing or targeted testing . 
characteristics of participants in the cogent study after adaptation for mgp by type of testing offered offered targeted testing only ( n = 205 ) offered multigene panel testing ( n = 395 ) characteristic had mgp testing , no . 
finally , there were no significant differences in knowledge at any time point . discussion in the largest study to date of pros after mgp testing , we found that patients eligible for hereditary cancer risk assessment and offered mgp , compared with targeted testing , had similar predisclosure and postdisclosure knowledge levels but lower predisclosure anxiety , depression , and uncertainty . 
these results demonstrate that genetic counselors can incorporate mgp testing into their practice without compromising patient understanding , even when results are delivered by telephone.6 one of the concerns commonly raised with mgp testing is the possibility of knowledge deficits as a result of the complexity of information communicated . 
 the potential negative impact of information overload from mgp counseling or testing on psychological outcomes is not supported by our findings , because we found that postdisclosure anxiety and depression were similar between the mgp and targeted testing groups . 
when the lower levels of predisclosure anxiety and depression among participants offered mgp are considered , our results also suggest that counselors may be more likely to offer complex mgp testing to patients they feel are at lower risk of negative psychological outcomes . 
in this way , these findings suggest that counselors are more than just gatekeepers to genetic testing and that comprehensive counseling includes both knowledge exchange and shared decision making with patients about concerns and preferences for genetic evaluation . 
 in the higher rates of selection of in - person disclosure among patients offered mgp testing , we observe counselors and patients counterbalancing a patients ability to manage the complexity and uncertainty of mgp testing with the standard approach of in - person results disclosure . these findings suggest that telephone disclosure is readily scalable to mgp testing and thus has an important role in the future of genomic medicine . 
although other studies have previously supported the efficacy of alternative telephone - based modalities of genetics services delivery , 3 , 5 these studies have not included mgp testing and have , notably , not reported detailed pros . 
one study recruited women at increased risk of hereditary breast and / or ovarian cancer and randomly assigned participants to in - person or telephone counseling , whereas the second study randomly assigned women with at least a 10% risk of having a brca1 / 2 mutation but without cancer to telephone counseling versus usual care . 
in both studies , telephone counseling was noninferior to in - person counseling for the selected outcomes ( which included anxiety , cancer - specific distress , perceived control , and decisional conflict in one study5 and satisfaction , distress , physical functioning , decisional conflict , and knowledge at 3 months and 1 year in the other study3 ) , although these results are specific to brca1 / 2 testing . 
although pros were not ascertained , the rate of preference for and receipt of mastectomy was similar regardless of whether a brca1 / 2 pathogenic variant or a pathogenic variant in a gene other than brca1 / 2 was identified by mgp , arguing that mgp may lead to more mastectomies over time . 
pros have not been explored in other areas of medicine where mgp testing has entered clinical care . lower postdisclosure anxiety and distress among patients offered mgp testing is consistent with differences seen pre - disclosure and reflect counselorand patient - driven selection of less anxious patients toward mgp testing . 
for others , high pretest risk was secondary to a known familial mutation ; 50% of the targeted testing population had a known familial mutation compared with 4% of the mgp testing population . 
similarly , patients tested by mgp had lower pretest likelihood of a pathogenic mutation , although the risk of identifying uncertain variants was higher as a result of the larger number of genes sequenced . although no other randomized studies have been conducted involving mgp , lumish et al19 performed a post - test survey measuring pros in patients undergoing testing for hereditary breast or ovarian cancer and in whom mgp testing was performed . 
they found older age , nonwhite race or non - hispanic ethnicity , lower educational attainment , and lower knowledge to be associated with higher anxiety and adverse psychological effects from counseling . 
analyses by cancer status ( affected or unaffected ) and stratified by result also found differential impact on psychological outcomes.19 nonetheless , it remains uncertain how the differences would have changed had mgp testing been replaced by targeted testing . 
 intolerance related to genomic testing21 have shown that uncertainty intolerance is associated with impaired decision making , feelings of vulnerability , and other adverse psychological outcomes.22 overall , we found that use of mgp testing increased over the study period.23 several factors are likely driving this change , including the need for more efficient delivery of genetic services . 
 the declining costs and the competitive marketplace for commercial testing established by the us supreme courts decision against myriad genetic laboratories and gene patenting have improved access to genetic testing . 
regional and community hospitals may be particularly disadvantaged when it comes to access to genetic counseling services and thus could be the earliest beneficiaries of models that incorporate remote counseling and testing options . 
however , after accounting for nonrandom differences between the targeted and mgp testing groups , short - term postdisclosure pros were generally similar , suggesting that the benefits of counseling rest in the live conversation between the counselor and patient and not in their proximity . 
time and resource limitations have undermined the traditional rigorous preand post - test counseling model used in cogent ; for example , katz et al25 found that 47% of patients did not receive counseling . 
in addition , few cogent participants were tested to guide a breast cancer treatment decision , and a recent population - based study found that mgp testing was associated with lower rates of testing among patients with breast cancer who had preoperative testing.18 finally , it also possible that patients choosing an mgp test versus targeted testing do so with family and family cancer risks in mind , so there may be additional information on testing selection gained from studying patterns of communication of results with relatives . in summary , the world of clinical genetic testing is changing rapidly , and use of mgp testing has increased over time . 
post - test knowledge , general anxiety , and depression were no worse and state anxiety was lower among patients who received mgp testing compared with those who received targeted testing . 
 bradbury manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors the following represents disclosure information provided by authors of this manuscript . 
 stock and other ownership interests : canceriq , tempus travel , accommodations , expenses : hospital of the university of pennsylvania research funding : novartis ( inst ) other relationship : tempus , color genomics , genentech , myriad genetics , bio ventures for global health kim rainey no relationship to disclose linda j . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) kristin mattie no relationship to disclose danielle mckenna no relationship to disclose susan montgomery no relationship to disclose sarah nielsen no relationship to disclose jacquelyn powers employment : carevive systems honoraria : cureconnect consulting or advisory role : carevive systems christina rybak no relationship to disclose michelle savage no relationship to disclose christina seelaus no relationship to disclose jessica stoll no relationship to disclose jill e . 
olopade employment : canceriq ( i ) leadership : canceriq dominique fetzer no relationship to disclose amanda brandt no relationship to disclose rachelle chambers no relationship to disclose dana f . 
clark no relationship to disclose rikki gaber honoraria : canceriq cassandra gulden no relationship to disclose janice horte no relationship to disclose andrea forman consulting or advisory role : invitae , astrazeneca , ambry speakers ' bureau : astrazeneca , ambry genetics , invitae jessica m . 
daly , andrea forman , susan montgomery , kim rainey , christina rybak , and michelle savage , fox chase cancer center , temple university health system ; susan m . 
olopade , center for clinical cancer genetics and global health , the university of chicago ; pamela ganschow , rikki gaber , terra lucas , and christina seelaus , the john h . 
hospital of cook county ; rachelle chambers , cassandra gulden , shreshtha madaan , sarah nielsen , and jessica stoll , the university of chicago , chicago , il ; and generosa grana , dana f . 
clark , janice horte , kristin mattie , and xinxin ( shirley ) yao , md anderson cancer center at cooper , camden , nj . support supported by national cancer institute grant no . 
kinney ay , steffen le , brumbach bh , et al : randomized noninferiority trial of telephone delivery of brca1 / 2 genetic counseling compared with in - person counseling : 1 - year follow - up . 
bradbury ar , patrick - miller lj , egleston bl , et al : randomized noninferiority trial of telephone vs in - person disclosure of germline cancer genetic test results . 
bradbury ar , patrick - miller lj , egleston bl , et al : patient feedback and early outcome data with a novel tiered - binned model for multiplex breast cancer susceptibility testing . 
bradbury ar , patrick - miller l , long j , et al : development of a tiered and binned genetic counseling model for informed consent in the era of multiplex testing for cancer susceptibility . 
kelly k , leventhal h , marvin m , et al : cancer genetics knowledge and beliefs and receipt of results in ashkenazi jewish individuals receiving counseling for brca1 / 2 mutations . 
cella d , hughes c , peterman a , et al : a brief assessment of concerns associated with genetic testing for cancer : the multidimensional impact of cancer risk assessment ( micra ) questionnaire . 
pieterse ah , van dulmen am , beemer fa , et al : cancer genetic counseling : communication and counselees post - visit satisfaction , cognitions , anxiety , and needs fulfillment . 
biesecker bb , klein w , lewis kl , et al : how do research participants perceive uncertainty in genome sequencing ? genet med 16 : 977 - 980 , 2014 22 . 
 mendel goldnger ramaswamy govindan jhanelle gray stacy gray samantha greenberg malachi grifth * roman groisberg * torsten haferlach michael hall * anis hamid * heather hampel * fei han sigurdis haraldsdottir * derrick haslem * eric haura masanori hayashi brian henick * , * * daniel herchenhorn * kenneth hess j . 
kevin hicks kim hirsheld brian hobbs howard hochster * daanish hoda * ahmed hosny david hsu wenhui huang yi huang * hatim husain maha hussain * david hyman * alexia iasonos * meredith irwin * steven isakoff katherine janeway * yelena janjigian lingyun ji xuemei ji * * yuchao jiang markus joerger steven joffe * thomas kaley mohammed kashanisabet steve katz kevin kim david kirsch kedar kirtane eric klein samuel klempner * todd knepper wendy kohlmann * jill kolesar * ian krop * priti kumari shivaani kummar ava kwong andrea laghi * jacky wai - kei lam angela lamarca jean - michel lavoie rachel layperson * christophe le tourneau * amy leblanc j . 
jack lee * jochen lennerz * antonio lerario benjamin levy mark lewis * jessica lin * steven lipkin jingyi liu * minetta liu * stephen liu * christine lovly ying lu * luke maese * david malkin diana mandelker sharon manne aaron manseld veronica mariotti thomas martin carlotta masciocchi joaquin mateo * shigeyuki matsui * joan maurel * shannon mccall jeannine mccune * rose mcgee * funda meric - bernstam everett meyer * ropa mhlanga * * luca mologni clara montagut * lucas moreno * daniel morgenstern * motomi mori * kent mouw anwesha nag katherine nathanson daniel nava rodrigues stewart neill kim nichols donna niedzwiecki nicola normanno * david norris paolo nuciforo jennifer oberg * stephen oh * coral omene stephen opat eileen oreilly * piet ost geoffrey oxnard * sukhmani padda tuya pal jose palacios phillip palmbos wei pan nickolas papadopoulos * soo park jai patel shiven patel * cloud paweletz andrew pearson raquel perez - lopez * thomas permutt * emanuel petricoin * gina petroni * david piccioni gaelle pierron filippo pietrantonio zoa piotrowska sharon plon eric polley mei - yin polley * erqi pollom mark pomerantz steven powell * colin pritchard * kanwal raghav * nitya raj w . 
we demonstrated previously that pemetrexed - based chemotherapy can achieve an objective response rate of 45% and a median progression - free survival ( pfs ) of 19 months.3 furthermore , the activity of targeted therapy has improved dramatically with the introduction of selective ret inhibitors to the clinic . 
in early - phase testing , objective response rates with loxo - 2924 and blu - 6675 are 68% ( 26 of 38 ) and 50% ( seven of 14 ) , respectively . 
these outcomes exceed the modest activity observed previously with multikinase inhibitors such as cabozantinib6 and vandetanib.7 in contrast , the activity of immunotherapy in retrearranged lung cancers has not been well characterized . 
this represents a clear unmet need , given that all prior regulatory approvals of immune checkpoint inhibitors , either alone or in combination with chemotherapy , and in stage iii or iv disease , have technically included patients with ret - rearranged lung cancers.8 , 9 furthermore , although increasing levels of programmed death - ligand 1 ( pd - l1 ) expression and high tumor mutational burden ( tmb ) have been associated with benet from immune checkpoint blockade , 10 the immunophenotype of ret - rearranged lung cancers and the role of pd - l1 and tmb status in relation to benet with immunotherapy remain poorly described . 
we set out to characterize these factors . methods in this retrospective study , patients from memorial sloan kettering cancer center with ret - rearranged lung cancers diagnosed between 2009 and 2017 were identied under an institutional review board approved waiver . 
patients who received immunotherapy , dened as a monoclonal antibody against programmed cell death protein 1 ( pd - 1 ) or pd - l1 , were included in an analysis of treatment history . ret rearrangements were identied using targeted next - generation sequencing of dna ( memorial sloan ketteringintegrated mutation proling of actionable cancer targets [ msk - impact ] or foundation one ) or rna ( anchored multiplex polymerase chain reaction [ pcr ] ; memorial sloan kettering solid fusion panel ) in more contemporary samples , and uorescence in situ hybridization ( 10q11 and 6q22 break apart probe , reversemetasystems , altussheim , germany ) or transcriptase pcr in older samples.11 , 12 pd - l1 immunohistochemistry was evaluated using the e1l3n antibody ( cell signaling technology , danvers , ma ) , our institutional standard , which has been validated against a 22c3 kit performed in a commercial laboratory with comparable results.13 for uniformity , tmb ( reported as the number of nonsynonymous mutations per megabase ) was analyzed only for samples sequenced using msk - impact.14 , 15 the median tmb of ret - rearranged was compared with that of ret wildtype nsclcs ( mann - whitney u test )  . in patients with both baseline and serial on - treatment imaging , the best objective response to therapy ( response evaluation criteria in solid tumors [ recist ] v1.1 ) was determined by a study radiologist . 
time to treatment discontinuation ( ttd ) was dened as the time from therapy initiation to the last dose.16 pfs was dened as the time from therapy initiation to radiologic progression or death . 
ret rearrangement was identied as follows : dna - based next - generation sequencing ( 80% [ n = 59 ] ) , rnabased anchored multiplex pcr ( 1% [ n = 1 ] ) , uorescence in situ hybridization ( 15% [ n = 11 ] ) , and reverse - transcriptase pcr ( 4% [ n = 3 ] )  . 
clinicopathologic features of ret - rearranged lung cancers : summary of demographics and tumor molecular features of 74 patients with ret - rearranged lung cancers feature all patients ( n = 74 ) age , years median range sex , no . 
in 44 patients with sufcient tissue for tmb analysis , the median tmb was 1.75 mutations / mb ( range , 0 to 9.65 mutations / mb ) , signicantly lower ( p , .0001 ) than the median tmb of 5.27 mutations / mb ( range , 0 to 164.20 mutations / mb ) in 3 , 631 patients with ret wild - type nsclcs ( fig 1b )  . the clinical outcomes of immunotherapy in patients with advanced ret - rearranged lung cancers are summarized in table 2 . 
 ( a ) the programmed death - ligand 1 ( pd - l1 ) expression ( e1l3n , cell signaling ) of 26 ret - rearranged lung cancers with sufcient tissue for testing is shown . 
 ( b ) the tumor mutational burden ( tmb ) of 44 ret - rearranged lung cancers is displayed ( left ) relative to the tmb of 3 , 631 ret wild - type lung cancers ( right )  . 
for ease of representation , three outlier ret wild - type lung cancer samples with tmb greater than 75 mutations / mb that were included in the statistical analysis were excluded in this plot . nivolumab ( n = 6 ) , atezolizumab ( n = 2 ) , durvalumab ( n = 1 ) , or ipilimumab plus nivolumab ( n = 1 )  . 
dashes represent tumor samples in which tissue was insufcient for pd - l1 or tmb testing . abbreviations : cr , complete response ; pd , progressive disease ; pd - l1 , programmed death - ligand 1 ; pfs , progression - free survival ; sd , stable disease ; non - cr / non - pd , not cr and not pd in nontarget lesions ; tmb , tumor mutational burden . * treatment discontinued for toxicity . a total of 13 patients with ret - rearranged lung cancers were assessed for clinical and / or radiologic response . response to immunotherapy was not observed . 
progression of disease was observed in 62% of cases ( n = eight of 13 ; table 2 ) ; disease progression involved new or worsening brain metastases in three patients ( cases 4 , 6 , and 15 )  . 
stable disease was achieved in 23% ( three of 13 ) and non - cr / non - pd ( not complete reponse and not progressive disease in nontarget lesions ) in 15% ( two of 13 )  . 
 ret - rearranged nsclc : immunophenotype and immunotherapy response these ndings are consistent with a growing body of evidence uncovering poor outcomes with immune checkpoint inhibition in select oncogene - addicted lung in egfr - mutant and alk - rearranged lung cancers . cancers , early data on the decreased activity ( compared with unselected cancers ) of immunotherapy resulted in the exclusion of patients with these tumors in registrationenabling studies . 
furthermore , we showed previously that met exon 14altered nsclcs had low tmb and poor outcomes with immunotherapy.17 finally , an ongoing global registry ( immunotarget ) and independent series have shown similarly low response rates and short median pfs with single - agent immune checkpoint inhibition in lung cancers with oncogenic drivers.18 immunotarget had 16 patients in the ret - rearranged cohort and reported a response rate of 6% and median pfs of 2.1 months , comparable to the ndings in our study . the clinical implications of these observations relate to the sequence with which immunotherapy is used and the type of immunotherapy strategy selected . 
regarding the former , it is becoming increasingly clear that specic , targeted therapies ( selective ret inhibitors ) 2 , 4 , 19 and chemotherapy agents ( pemetrexed - containing regimens ) 3 can achieve superior outcomes compared with immunotherapy in this series . 
thus , is reasonable to consider the use of checkpoint inhibition only after select targeted therapies and platinum doublet - containing chemotherapy have been administered . note that high pd - l1 expression ( 50% or more ) was uncommon in ret - rearranged lung cancers in this study . only one case treated with immunotherapy highly expressed pd - l1 ( 50% ) and , despite this , still responded poorly to dual immune checkpoint inhibitor therapy ( case 16 )  . 
a recommendation regarding the use of pembrolizumab in treatment - nave , advanced ret - rearranged lung cancers with high pd - l1 expression cannot be made on the basis of our ndings , although its use should be approached with caution . 
in met exon 14altered lung cancers , tmb is similarly low ; although a higher proportion of tumors have high pd - l1 expression , this was not associated with increased benet with single - agent immunotherapy.17 finally , no patients in this series received the combination chemotherapy and immunotherapy that is currently approved for the treatment of egfr and alk wild - type advanced nsclc . 
prospective trials of immunotherapy combinations should incorporate comprehensive molecular proling to establish prospective data in driver - positive subpopulations of patients . in summary , most ret - rearranged lung cancers have low pd - l1 expression and low tmb , and response to immunotherapy was not observed in this series . 
although this study is limited by a small sample size , given the rarity of ret - rearranged nsclcs , these ndings remain meaningful and support evolving literature showing that outcomes with immune checkpoint inhibition are poor in select oncogene - addicted nsclcs . 
contributed equally to this work . support supported in part by the national cancer institute of the national institutes of health ( t32 ca009207 , p30 ca008748 )  . provision of study material or patients : gregory j . 
rudin consulting or advisory role : bristol - myers squibb , abbvie , seattle genetics , harpoon therapeutics , genentech / roche , astrazeneca , ascentage pharma , bicycle therapeutics , celgene , daiichi sankyo , ipsen , loxo , pharmamar , elucida oncology research funding : abbvie / stemcentrx ( inst ) , viralytics ( inst ) , merck ( inst ) , daiichi sankyo ( inst ) gregory j . 
riely research funding : novartis ( inst ) , roche / genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pzer ( inst ) , innity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) , mirati therapeutics ( inst ) , merck ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : merck sharp & dohme matthew d . 
hellmann stock and other ownership interests : shattuck labs honoraria : astrazeneca , bristol - myers squibb consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca / medimmune , novartis , janssen pharmaceuticals , nektar , syndax pharmaceuticals , mirati therapeutics , shattuck labs research funding : bristol - myers squibb ( inst ) patents , royalties , other intellectual property : a patent has been led by memorial sloan kettering ( pct / us2015 / 062208 ) for the use of tumor mutation burden for prediction of immunotherapy efcacy , and which is licensed to personal genome diagnostics ( inst ) travel , accommodations , expenses : astrazeneca , bristol - myers squibb maria arcila honoraria : invivoscribe consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe , raindance technologies mark g . 
li consulting or advisory role : roche , biosceptre international , thermo fisher scientic , mersana , guardant health , hengrui therapeutics research funding : roche / genentech ( inst ) , illumina ( inst ) , biomed valley discoveries ( inst ) , astrazeneca ( inst ) , grail ( inst ) , daiichi sankyo ( inst ) , hengrui therapeutics ( inst ) , guardant health ( inst ) marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso request for proposal advisory committee , takeda pharmaceuticals , bristol - myers squibb , bayer ag , merck ( i ) research funding : loxo ( inst ) , helsinn therapeutics alexander drilon honoraria : medscape , onclive , peervoice , physicians education resources , targeted oncology , more health , research to practice , foundation medicine , peerview consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pzer , blueprint medicines , genentech / roche , helsinn therapeutics , beigene , hengrui therapeutics , exelixis , bayer ag , tyra biosciences , verastem , takeda pharmaceuticals / ariad pharmaceuticals / millenium pharmaceuticals , bergenbio , more health patents , royalties , other intellectual property : wolters kluwer ( royalties for pocket oncology ) other relationship : merck , glaxosmithkline , teva pharmaceuticals industries , taiho pharmaceutical no other potential conicts of interest were reported . references stransky n , cerami e , schalm s , et al : the landscape of kinase fusions in cancer . 
nat commun 5 : 4846 , 2014 drilon a , hu zi , lai ggy , et al : targeting ret - driven cancers : lessons from evolving preclinical and clinical landscapes . 
nat rev clin oncol 15 : 151 - 167 , 2018 drilon a , bergagnini i , delasos l , et al : clinical outcomes with pemetrexed - based systemic therapies in ret - rearranged lung cancers . 
ann oncol 27 : 1286 - 1291 , 2016 oxnard gr , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer : an update from asco 2018 . 
toronto , canada , september 23 - 26 , 2018 subbiah v , taylor m , lin j , et al : abstract ct043 : highly potent and selective ret inhibitor , blu - 667 , achieves proof of concept in a phase i study of advanced , ret - altered solid tumors . 
drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 2 , single - arm trial . 
lancet oncol 17 : 1653 - 1660 , 2016 lee sh , lee jk , ahn mj , et al : vandetanib in pretreated patients with advanced non - small cell lung cancer - harboring ret rearrangement : a phase ii clinical trial . 
ann oncol 28 : 292 - 297 , 2017 gandhi l , rodrguez - abreu d , gadgeel s , et al : pembrolizumab plus chemotherapy in metastatic non - small - cell lung cancer . 
n engl j med 378 : 2078 - 2092 , 2018 reck m , rodrguez - abreu d , robinson ag , et al : pembrolizumab versus chemotherapy for pd - l1 - positive non - small - cell 375 : 1823 - 1833 , 2016 lung cancer . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
ofn m , rizvi h , tenet m , et al : tumor mutation burden and efcacy of egfr - tyrosine kinase inhibitors in patients with egfr - mutant lung cancers . 
sabari jk , leonardi gc , shu ca , et al : pd - l1 expression , tumor mutational burden , and response to immunotherapy in patients with met exon 14 altered lung 18 . 
mazieres j , drilon ae , mhanna l , et al : efcacy of immune - checkpoint inhibitors ( ici ) in non - small cell lung cancer ( nsclc ) patients harboring activating molecular alterations ( immunotarget )  . 
 ofn et al immunotherapy naive ( n = 46 ) immunotherapy administered ( n = 16 ) log - rank p = .35 time since metastasis diagnosis ( years ) no . 
overall survival from the diagnosis of metastatic disease was compared between patients who received an immune checkpoint inhibitor ( n = 16 ) and those who did not ( n = 46 )  . 
hung , md , phd1 ; dora dias - santagata , phd1 ; maristela onozato , md1 ; nikunj shah , bs2 ; eric severson , md2 ; daniel duncan , md2 ; brendan j . 
we characterized molecular and clinicopathologic features of the pertinent fusion - positive patient cases . results we identied 11 patients with thymomas harboring a gene fusion of kmt2a and mastermind - like transcriptional coactivator 2 ( maml2 )  . 
the frequency of kmt2a - maml2 fusion was 4% of all thymomas ( 10 of 242 ) and 6% of thymomas of b2 or b3 histology ( 10 of 169 )  . conclusion kmt2a - maml2 represents the rst recurrent fusion described in type b thymoma . 
the identication of this fusion offers insights into the biology of thymoma and may have clinical relevance for patients with disease refractory to conventional therapeutic modalities . jco precis oncol 4 : 109 - 115 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction thymoma , a neoplasm that arises from or exhibits thymic epithelial differentiation , is the most common tumor of the adult thymus.1 thymoma has a strong association with autoimmune diseases , particularly myasthenia gravis , which typically resolve upon successful tumor resection . 
we aim to identify recurrent genetic alterations present in this tumor . knowledge generated a subset of type b2 and b3 thymomas harbor recurrent gene fusions between lysine methyltransferase 2a ( kmt2a ) and mastermind - like transcriptional coactivator 2 ( maml2 )  . 
aside from rare case reports of hematologic neoplasms in the literature , the kmt2a - maml2 rearrangement seems specic to type b2 and b3 thymomas among human tumors . relevance the nding of recurrent kmt2a - maml2 fusion provides insights into tumor biology and potential therapeutic targets in type b2 and b3 thymomas , which are clinically aggressive with limited curative options . solid fusion assay analysis ( mgh solid fusion assay ; mgh , boston , ma ; data supplement provides list of gene targets ) and single - nucleotide variant and insertion / deletion analysis ( snapshot dna - based assay ; thermo fisher scientic , waltham , ma ; data supplement provides list of gene targets ) .7 the solid fusion assay used rna - based fusiontargeted anchored multiplex polymerase chain reaction ( archerdx primers , boulder , co ) and illumina ( san diego , ca ) sequencing . 
in brief , 60 ng of dna was extracted from 255 , 008 cancer specimens , including 242 thymoma specimens , in 40 m of formalin - xed , parafn - embedded tissue blocks . 
the samples were assayed by cgp using adaptor ligation , and hybrid capture was performed for all coding exons from 287 ( version 1 ) to 315 ( version 2 ) cancer - related genes plus select introns from 19 ( version 1 ) to 28 ( version 2 ) genes frequently rearranged in cancer ( data supplement )  . 
gtf2i included on any list of cancer - related genes . was not various samples were similarly assayed but performed in dna on 406 genes and selected introns of 31 genes involved in rearrangements ( data supplement ) and in rna on 265 genes commonly rearranged in cancer . 
sequences were analyzed for all classes of genomic alterations , including short variant alterations ( base substitutions , insertions , and deletions ) , copy - number alterations ( focal amplications and homozygous deletions ) , and select gene fusions or rearrangements by methods previously described.8 - 10 thymomas harboring a kmt2a - maml2 the cohort of fusion comprised 10 patient cases assayed with cgp ( foundation medicine ) during clinical care at other institutions . 
seven years later , the patient developed recurrent thymoma , with direct invasion of the lung , pericardium , and distal left main pulmonary artery , as well as metastasis to paratracheal lymph nodes ( fig 1a )  . the patient received induction chemotherapy and underwent surgical resection ( radical thymectomy , radical pericardiectomy , and left pneumonectomy ) , followed by paratracheal lymph node excision and radiotherapy . 
 ( a ) computed tomography of the chest from the patients rst recurrence demonstrates a 7.8 - cm anterior mediastinal mass ( arrow ) in contact with the pericardium , aorta , and portions of the main and left pulmonary arteries . 
 ( b ) histopathologic examination of the tumor shows sheets of large epithelioid cells lacking signicant lymphocytic inltration , consistent with type b3 thymoma ( hematoxylin and eosin stain ; magnication 400 )  . 
 ( d ) ihc for terminal deoxynucleotidyl lineage thymocytes associated with the tumor ( magnication 400 )  . transferase highlights scattered nuclei of t - cell recurrence of myasthenia gravis . 
the patient died as a result of complications of her thymoma 15 years after initial diagnosis . given the aggressive nature of this thymoma , molecular genetic assays were performed on the initial recurrence to lung , in an attempt to identify potentially targetable genetic alterations . 
this fusion assay result was reproduced on the patients subsequent paratracheal lymph node excision . kmt2a - maml2 fusion occurs in aggressive histologic subtypes of thymoma to determine the frequency of kmt2a - maml2 fusion in a cohort specically enriched in clinically more aggressive cases of thymoma , we reviewed a set of 242 patient cases of thymoma from the foundation medicine archives . 
the patient case was reviewed , and the original diagnosis was conrmed . the kmt2a - maml2 fusion was reamong thymomas , stricted to the most aggressive histologic thymoma subtypes , being present in 10 ( 5.9% ) of 169 thymomas that included b2 or b3 components , but 0 ( 0% ) of 64 of the remaining thymomas ( types a , ab , and b1 )  . 
no other known or likely pathogenic alterations were identied in 7 of 10 patient cases with a kmt2a - maml2 fusion , whereas a concurrent mutation in tp53 , arid1a , or sf3b1 was identied in 1 patient case each . 
of patients age at diagnosis , years final staging ( modied masaoka ) median range male female unknown histology b2 + b3 b3 + c 112 2020 by american society of clinical oncology discussion in the 243 patient cases of thymoma evaluated , we discovered a recurrent fusion of kmt2a and maml2 in 11 . this fusion seems to be highly specic to thymomas with aggressive histologic features , because all fusion - positive patient cases contained type b2 and / or b3 histology . 
the striking restriction of kmt2a - maml2 fusion to thymomas was underscored by the absence of the fusion in approximately 255 , 000 patient cases of diverse tumor types , including 366 thymic carcinomas , with the exception of a single patient case of plasmacytoma . kmt2a , rst described in 1991 , was initially termed mixedlineage leukemia - 1 because of its frequent appearance as a translocation partner in acute myeloid and lymphoid leukemias.12 the 36 - exon gene is located on chromosome 11q23 . 
the encoded protein binds dna and methylates histone h3 at lysine - 4 to regulate other genes , including several homeobox ( hox ) genes.13 kmt2a has been found to be a promiscuous translocation partner , with  . 
80 unique fusion partners identied.14 currently , there is no unifying theory on how kmt2a rearrangements lead to neoplasia.14 maml2 is a 5 - exon gene residing on chromosome 11q21 . 
maml2 and other maml family proteins are involved in notch pathwaymediated transcriptional activation.15 recurrent gene rearrangements involving maml2 have been described in mucoepidermoid carcinoma , in which fusion of the rst exon of the camp response element - binding proteinregulated transcription coactivator - 1 ( crtc1 ) with maml2 exons 2 to 5 leads to notch pathway disruption.16 the kmt2a - maml2 gene fusion results from inv ( 11 ) ( q21q23 ) , a cytogenetic abnormality rst reported in 1998 by obama et al17 in a patient with therapy - related acute myeloid leukemia . subsequent reports of the fusion are exceptionally rare and no . 
to our knowledge , only 8 patient cases have been reported , including 2 of acute myeloid leukemia , 2 of myelodysplastic syndrome , and 4 of acute lymphoblastic leukemia.17 - 22 reported fusion proteins in these patient cases involved regions similar to those identied in our cohort , with the exception of 2 patient cases reported by metlzer et al21 with maml2 breakpoints in introns 2 and 3 . prior functional studies of the kmt2a - maml2 construct have shown evidence of disrupted notch pathway signaling . 
in addition to describing the fusion in patient cases therapy - related myeloid neoplasms , nemoto et al19 the kmt2ademonstrated via luciferase assay that maml2 fusion suppresses promoter activation of the notch1 target gene hes1.19 gene expression proles from 2 patient cases of kmt2a - maml2positive t - cell acute lymphoblastic leukemia showed differential expression patterns relative to controls , suggesting activation of genes downstream of notch1.21 another study demonstrated oncogenic activity by kmt2a - maml2 fusion inserted into cell lines with sleeping - beauty vectors.23 the sum of these studies has demonstrated oncogenic function of kmt2a - maml2 fusion , likely via disruption of notch signaling . 
further study is warranted to examine the impact of this fusion on notch signaling . in patients with malignancies not amenable to traditional surgical or chemoradiotherapy protocols , targeted therapy offers an additional potential opportunity for disease control . 
early data suggest disease refractory to initial that maml2 fusionpositive mucoepidermoid carcinoma may respond to targeted therapeutics , including epidermal growth factor receptor inhibitors such as getinib.24 - 26 given the low tumor mutational burden seen in thymoma , identication of this small but genomically distinctive subset of kmt2a - maml2rearranged tumors may provide a therapeutic target in patients not responsive to traditional therapy . 
hasserjian , abner louissaint jr , erik a . williams manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors nikunj shah employment : foundation medicine eric severson employment : foundation medicine , partners healthcare stock and other ownership interests : foundation medicine daniel duncan employment : foundation medicine jeffrey s . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . dora dias - santagata consulting or advisory role : rarecyte ( i ) maristela onozato patents , royalties , other intellectual property : patent pending for multiplex fish assay , led on october 25 , 2019 ( no direct compensation related to this patent ) jo - anne vergilio employment : foundation medicine stock and other ownership interests : foundation medicine , roche valentina nardi consulting or advisory role : thermo fisher scientic ( i ) , cell signaling technology ( i ) robert p . 
hasserjian stock and other ownership interests : avanos medical , danaher , henry schein , hologic , idexx laboratories , johnson & johnson , kimberly clary , medtronic , stryker , cooper companies , thermo fisher scientic consulting or advisory role : jazz pharmaceuticals , promedior erik a . 
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ziemin - van der poel s , mccabe nr , gill hj , et al : identication of a gene , mll , that spans the breakpoint in 11q23 translocations associated with human leukemias . 
k ochert k , ullrich k , kreher s , et al : high - level expression of mastermind - like 2 contributes to aberrant activation of the notch signaling pathway in human lymphomas . 
tonon g , modi s , wu l , et al : t ( 11 ; 19 ) ( q21 ; p13 ) translocation in mucoepidermoid carcinoma creates a novel fusion product that disrupts a notch signaling pathway . 
obama k , furukawa y , tara m , et al : secondary monocytic leukemia with rearrangement of the mll gene occurring during the course of adult t - cell leukemia . int j hematol 68 : 323 - 326 , 1998 18 . 
mariani ra , silva m , caparelli e , et al : inv ( 11 ) ( q21q23 ) : kmt2a - maml2 , a recurrent genetic abnormality in t - cell therapy - related acute lymphoblastic leukemia . 
nemoto n , suzukawa k , shimizu s , et al : identication of a novel fusion gene mll - maml2 in secondary acute myelogenous leukemia and myelodysplastic syndrome with inv ( 11 ) ( q21q23 )  . 
tang g , lu x , wang sa , et al : homozygous inv ( 11 ) ( q21q23 ) and mll gene rearrangement in two patients with myeloid neoplasms . 
metzler m , staege ms , harder l , et al : inv ( 11 ) ( q21q23 ) fuses mll to the notch co - activator mastermind - like 2 in secondary t - cell acute lymphoblastic leukemia . 
chen z , chen j , gu y , et al : aberrantly activated areg - egfr signaling is required for the growth and survival of crtc1 - maml2 fusion - positive mucoe26 . 
li s , zhang z , tang h , et al : pathological complete response to getinib in a 10 - year - old boy with egfr - negative pulmonary mucoepidermoid carcinoma : a pidermoid carcinoma cells . 
 c sequential response to fgfr3 inhibition with subsequent exceptional response to atezolizumab in a patient with fgfr3 - tacc3 fusionpositive metastatic urothelial carcinoma introduction recent work has pointed to alterations in fibroblast growth factor receptors ( fgfrs ) as potential drivers of colder metastatic urothelial carcinoma ( muc ) microenvironments.1 , 2 fgfrs mediate cell proliferation , migration , differentiation , and survival.3 activating genomic alterations in fgfr3 are frequent in bladder cancer.4 - 6 in the muscle - invasive bladder cancer data set of the cancer genome atlas , fgfr3 alterations were found to be enriched in the luminal papillary subtype.7 clinical benefit from immune checkpoint inhibitors ( icis ) has been a major advance for many cancer types in recent years , including muc , leading to us food and drug administration approval.5 although durable clinical benefit is seen in multiple cancer types , objective response rates in muc are only 15% to 24%.8 mechanisms contributing to ici resistance and low response rates are poorly understood . a phase ii trial comparing the association between the cancer genome atlas mrna subtypes and response to atezolizumab , an antiprogrammed cell death ligand 1 ( pd - l1 ) monoclonal immunoglobulin g1 antibody , showed that the luminal cluster ( enriched for fgfr genomic alteration ) was associated with lower expression levels of cd8 + genes and lower response rates ( 10% ) .1 another study has shown that higher fgfr3 expression and fgfr3 pathway mutations are strongly associated with immune exclusion in bladder cancer.9 this association was also found in patients with bladder tumors harboring fgfr3 - tacc3 fusions.2 these observations suggest that patients harboring fgfr3 alterations are relatively poor candidates for ici therapy . herein , we report a patient with metastatic bladder cancer harboring an fgfr3 - tacc3 fusion and exhibiting an exceptional response to sequential fgfr3 inhibition and antipd - l1 blockade . 
as part of the standard care , the patient received three cycles of adjuvant cisplatin and gemcitabine chemotherapy . the patient demonstrated recurrent disease 5 months later when a computed tomography ( ct ) scan of the chest , abdomen , and pelvis ( cap ) showed two enlarged retroperitoneal lns , amin h . 
genomic profiling by next - generation sequencing ( oncopanel ; brigham and women 's hospital , boston , ma ) was requested on an archival formalin - fixed , paraffin - embedded block derived from the patients primary tumor , which showed an fgfr3 - tacc3 fusion involving intron 17 of fgfr3 and intron 10 of tacc3 . 
 the fgfr3 - tacc3 fusion breakpoints were confirmed by manual review using integrative genomics viewer ( fig 1 ) .10 the patient was then enrolled onto a clinical trial evaluating the combination of pazopanib and everolimus in may 2015 . 
however , the biopsy was insufficient for next - generation tumor sequencing but was sufficient for rnascope ( advanced cell diagnostics , newark , ca ) , a multiplex fluorescent in situ hybridization ( fish ) assay . 
 however , fgfr3 overexpression was seen by the rnascope assay ( fig 2 )  . the patient was enrolled onto a protocol in which he received treatment with both docetaxel and b - 701 ( a monoclonal antibody against fgfr3 ) and was found to have achieved complete remission ( cr ) 5 months later . 
 ( b ) patients lymph node ( after treatment with pazopanib and everolimus ) sample stained with hs - tacc3 - e11 - e16 - c1 ( green ) and hs - fgfr3 - e2e13 - c2 ( red )  . and the patient continues to be in cr 6 months later . discussion in this study , we describe a patient with an fgfr3 - altered muc that showed dramatic response to immunotherapy after receiving sequential treatment with an fgfr tyrosine kinase inhibitor and a monoclonal antibody against fgfr3 . 
next - generation sequencing showed an fgfr3 - tacc3 fusion , msh2 and msh6 homozygous deletions , and a tumor mutational burden of 22.9 mutations / mb ( data supplement )  . 
on the basis of the reported data in the literature , the question arises of what could be driving this unusual response to icis in the setting of an fgfr3 - altered cold tumor . several points of interest regarding this patient deserve to be highlighted and mentioned . 
first , interestingly , rnascope f luorescent in situ hybridization conducted on the ln site showing progression to docetaxel and b - 701 , was negative for the fgfr3 - tacc3 fusion . 
depletion of fgfr3 - tacc3 positive cells possibly molded the tumor microenvironment into a simple overexpressed fgfr tumor microenvironment , which can explain the subsequent cr obtained with the use of the different fgfr3 inhibitor b - 701 . 
however , this sequential response to two fgfr inhibitors is of interest and points to the possibility that sequential use of tyrosine kinase inhibitors and a monoclonal antibody might have different potency and nonoverlapping mechanisms of action for fgfr inhibition . the second intriguing point is the response seen with atezolizumab in this cold tumor . 
 ( mmr - d ) is an established biomarker to icis and has been shown to be associated with clinical benefit in several cancers.14 , 15 to determine whether our patients tumor was mmr - d and whether mmr - d could be driving the response to atezolizumab , we used two methods to assess mmr - d status . 
using a bayesian non - negative matrix factorization algorithm , we determined that our patients tumor has low cosmic 6 activity and thus lacks an mmr - d mutation signature.7 moreover , a recent study by the oncopanel team identified a cutoff value of > 40 mutations / mb or > 5 indels / mb in repeat regions to categorize a patients tumor as mmr - d , which was not the case in our patient ( 22.9 mutations / mb ; 4.8 indels / mb ) .16 in conclusion , on the basis of the present observation , this patients case provides evidence of a sequential response observed with the use of two different fgfr inhibitors with different mechanisms of action . 
however , high tumor mutational burden or the microsatellite instability mutant status can also explain this unexpected excellent response to the ici . one might envision combinatorial trials in patients with fgfr3 alterations involving fgfr3 inhibitors along with icis or studies of the use of these agents in the optimal sequence , which is probably fgfr3 inhibitors followed by a pd - 1 / pd - l1 inhibitor . 
choueiri honoraria : national comprehensive cancer network , uptodate consulting or advisory role : pfizer , bayer , novartis , glaxosmithkline , merck , bristol - myers squibb , genentech , eisai , foundation medicine , cerulean pharma , astrazeneca , peloton therapeutics , exelixis , prometheus laboratories , alligent , ipsen , corvus pharmaceuticals research funding : pfizer ( inst ) , novartis ( inst ) , merck ( inst ) , exelixis ( inst ) , tracon pharma ( inst ) , glaxosmithkline ( inst ) , bristol - myers squibb ( inst ) , astrazeneca ( inst ) , peloton therapeutics ( inst ) , genentech ( inst ) , celldex ( inst ) , agensys ( inst ) , eisai ( inst ) guru p . 
kwiatkowski consulting or advisory role : astrazeneca , genentech joaquim bellmunt honoraria : uptodate research funding : aadi consulting or advisory role : pierre fabre , astellas pharma , pfizer , merck , genentech , novartis , astrazeneca / medimmune , bristol - myers squibb research funding : millennium ( inst ) , sanofi ( inst ) travel , accommodations , expenses : pfizer , msd oncology affiliations amin h . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinumbased chemotherapy : a single - arm , multicentre , phase 2 trial . 
massard c , gordon ms , sharma s , et al : safety and efficacy of durvalumab ( medi4736 ) , an anti - programmed cell death ligand - 1 immune checkpoint inhibitor , in patients with advanced urothelial bladder cancer . 
necchi a , joseph rw , loriot y , et al : atezolizumab in platinum - treated locally advanced or metastatic urothelial carcinoma : post - progression outcomes from the phase ii imvigor210 study . 
sharma p , callahan mk , bono p , et al : nivolumab monotherapy in recurrent metastatic urothelial carcinoma ( checkmate 032 ) : a multicentre , open - label , two - stage , multi - arm , phase 1 / 2 trial . 
siefker - radtke ao , necchi a , rosenbaum e , et al : efficacy of programmed death 1 ( pd - 1 ) and programmed death 1 ligand ( pd - l1 ) inhibitors in patients with fgfr alterations : results from a data analysis of an ongoing phase 2 study of erdafitinib ( jnj - 42756493 ) , in patients ( pts ) with advanced urothelial cancer ( uc )  . 
 genetic testing and clinical management practices for variants in non - brca1 / 2 breast ( and breast / ovarian ) cancer susceptibility genes : an international survey by the evidence - based network for the interpretation of germline mutant alleles ( enigma ) clinical working group sarah m . 
domchek ros eeles anna efremidis ( continued ) purpose to describe a snapshot of international genetic testing practices , specifically regarding the use of multigene panels , for hereditary breast / ovarian cancers . 
we conducted a survey through the evidence - based network for the interpretation of germline mutant alleles ( enigma ) consortium , covering questions about 16 non - brca1 / 2 genes . methods data were collected via in - person and paper / electronic surveys . 
additional information was collected via country networks in the united kingdom and in italy . results responses from 61 cancer genetics practices across 20 countries showed that 16 genes were tested by > 50% of the centers , but only six ( palb2 , tp53 , pten , chek2 , atm , and brip1 ) were tested regularly . 
us centers tested the genes most often , whereas united kingdom and italian centers with no direct enigma affiliation at the time of the survey were the least likely to regularly test the most centers tested the 16 genes through multigene panels ; some centers tested tp53 , pten , and other cancer syndromeassociated genes individually . 
gene - specific guidelines for breast and ovarian cancer risk management were limited and differed among countries , especially with regard to starting age and type of imaging and risk - reducing surgery recommendations . conclusion currently , a small number of genes beyond brca1 / 2 are routinely analyzed worldwide , and management guidelines are limited and largely based on expert opinion . 
pedersen maria piane marianna puzzo mark robson maria rossing maria christina sini angela solano jana soukupova gianluca tedaldi manuel teixeira mads thomassen maria grazia tibiletti amanda toland therese trngren erica vaccari liliana varesco ana vega yvonne wallis barbara wappenschmidt jeffrey weitzel amanda b . 
currently , several multigene panels are available that include from < 10 to > 100 known or candidate cancer susceptibility genes , which are tested for diagnostic or research purposes . 
some panels are targeted at diverse cancers ( pan - cancer panels ) , whereas others target specific cancers only ( disease specific panels )  . the ability to run multigene panels at affordable prices has expanded the eligibility criteria and increased the demand for testing.1 - 5 however , the rapid pace at which candidate risk genes are moving from research based to clinical diagnostic testing has its drawbacks . 
the rate of variants of uncertain significance ( vus ) has increased proportionally to the extent of the sequenced genome.5 - 7 moreover , many genes currently included on multigene panels have imprecise cancer risk estimates , and there is no consensus on when to test for a given gene or how to manage a reported ( likely ) pathogenic variant.8 , 9 the aim of this study was to describe a snapshot of the landscape of international genetic testing practices and risk management approaches for bc and boc susceptibility genes beyond brca1 and brca2 . 
a survey was conducted among members of the evidence - based network for the interpretation of germline mutant alleles ( enigma ) , an international consortium focused on determining the clinical significance of variants in brca1 , brca2 , and other ( ascertained or suspected ) bc and boc susceptibility genes , providing expertise to global database and classification initiatives , and exploring optimal avenues of communication of such information at the provider and patient levels . 
additional information was collected via country networks in the united kingdom and in italy , from centers that were not directly involved in enigma research at the time of study initiation . in total , respondents represented cancer genetic experts from 61 centers across 20 countries . 
 to our knowledge , this is the first study to describe international testing practices and risk management guidelines for non - brca1 / 2 genes implicated in bc and boc susceptibility . methods this study was submitted for approval to the ethics committees of the two coordinating sites , the university of chicago and maastricht university . 
a survey about genetic testing practices for nonbrca1 / 2 bc and boc susceptibility genes was developed by enigma clinical working group ( cwg ) leaders during 2016 ( appendix table a1 )  . 
enigma members were invited to complete the survey if they had a clinical genetic testing or diagnostic laboratory affiliation and were involved in ordering , performing , or interpreting dna tests for inherited susceptibility to bc / boc at their center . 
an enigma member is currently defined as a researcher or research group ( consortium ) who is willing to work collaboratively toward classification of variants by contributing data from families and / or conducting statistical analysis or laboratory - based assays within a working group framework . 
there is no requirement for enigma members to state their primary role ( clinician , genetic counselor , laboratory scientist , basic researcher ) , but all members by definition have a research interest in the topic of gene / variant classification . individuals from the same center could work on the survey together or choose a designated representative to complete it , so only one survey per center was counted . 
in brief , an in - person survey of members of the cwg , consisting mainly of laboratory and clinical scientists from academic centers , was conducted during the enigma consortium meeting in limassol , cyprus , in january 2017 . 
 a total of 30 centers from 17 countries participated . a more detailed version of the survey was then distributed by e - mail ( paper / electronic survey ) to the same 30 centers that participated in the in - person survey and to additional enigma affiliated centers worldwide . 
participants were sent a copy of their answers and asked to verify them or to clarify any discrepancies . notably , in italy and in the united kingdom , the paper / electronic version of the survey was also distributed , via country networks , to centers that were not actively involved in enigma research . 
the effort comprised both the enigma - affiliated fondazione istituto di ricovero e cura a carattere scientifico istituto nazionale dei tumori ( milan ) and the santa chiara university hospital ( pisa ) , which were counted among the 38 participating enigma centers , and 14 additional centers , which were not directly affiliated with enigma at the time of the survey ( henceforth referred to as non - enigma ; fig 1 , lower right )  . 
of the 14 italian non - enigma centers , five were dedicated to diagnostic testing only , and nine were dedicated to both diagnostics and research ; moreover , half of them were university affiliated , and half were not . 
 completed the survey for her own enigma affiliated center ( one of the 38 participating enigma centers ) and also coordinated , with the assistance of y.w. , the distribution of the survey through surveymonkey via the association for clinical genetic science mailing list to cancer genetic leads from diagnostic laboratories providing genetic testing for the publicly funded national health service ( nhs )  . 
the recruitment flowchart and the global distribution of participants are illustrated in figure 1 . clinical utility to get a preliminary idea of the participants opinions about the clinical utility of the 16 genes on which the survey focused , the cwg members present at the 2017 enigma meeting in cyprus were asked to answer the following questions relating to each of them : should every patient with bc / oc who qualifies for ( brca1 / 2 ) genetic testing ( by criteria that we recognize may differ by country / center ) be tested for the gene ? and do you agree that the cancer risk associated with ( pathogenic variants in ) the gene is high enough to inform clinical management ? all participants ( n = 23 at this specific session ) stated that they would test every qualifying patient with bc ( as defined in the question ) for palb2 and every qualifying patient with oc ( as defined ) for brip1 , rad51c , and rad51d . 
results for the other nine genes were variable ( appendix fig a1a )  . with regard to clinical management , all participants agreed that palb2 , tp53 , cdh1 , pten , and stk11 along with brip1 , rad51c , and rad51d were associated with high enough ( bc or oc ) risk to alter clinical management . 
please note that 95% cis for this figure and for all the following figures are provided in appendix ( tables a2 - a10 )  . testing practices participants were also asked ( via in - person and / or paper / electronic surveys ) if and how frequently they tested each gene , the method ( single gene v gene panel ) and purpose of testing ( clinical v research ) , and the practices of reporting ( likely ) pathogenic variants and vus to patients . 
of centers that responded to the question varied by gene ( range , 29 to 38 centers ) .regularly was defined as ordered for > 50% of eligible patients ( ie , those who qualified for genetic testing , by criteria that we recognize may differ by center / country )  . 
even though each gene was tested by > 50% of the centers ( range , 52% to 100% ) , only palb2 , tp53 , pten , chek2 , atm , and brip1 were tested regularly by > 50% of centers . testing in a research setting in addition to the clinical setting was common for enigma centers ( appendix fig a2 )  . 
the genes that were most frequently tested ( ie , tested by at least > 30% of centers ) for research purposes only were : nbn , bard1 , rad50 , and mre11a . 
 single - gene testing was performed by a number of centers , varying from one to 21 , for : tp53 , pten , cdh1 , stk11 , palb2 , chek2 , nf1 , atm , men1 , and nbn ( in decreasing order of frequency ) , often based on a specific phenotype ( eg , pten hamartoma syndrome or neurofibromatosis type 1 ) , or these genes were tested as a reflex only when brca1 / 2 testing was noninformative . 
seven centers from four countries ( belgium , brazil , the netherlands , and spain ) testing chek2 only tested for the 1100delc variant . regarding the types of gene panels used , us respondents typically ordered broad cancer panels from commercial laboratories , although the specific panels varied depending on patient preferences , insurance considerations , and clinical scenarios . 
separately , the nine united kingdom nhs laboratories were asked , if you currently only report brca genes but might report broader panels in the future , what issues are major barriers / problems to overcome ? responses were chosen from a menu of nine options plus other , and the four main reasons selected ( by half or more of respondents ) were no request by the oncologists ( of note , nhs oncologists can ask directly for brca1 and brca2 testing but not for multigene panels ) , lengthy and laborious process of variant interpretation , lack of standardization of reporting , and lack of demand for testing . reporting practices and cascade testing . 
for genes analyzed through clinical testing , > 90% of enigma centers reported ( likely ) pathogenic variants to patients ( for chek2 and nbn , the percentages were slightly lower , at 88% and 71% , respectively ; fig 4 )  . 
some centers reported these variants only if the patient met criteria for the associated syndrome ( eg , hereditary diffuse gastric cancer for cdh1 , neurofibromatosis type 1 for nf1 )  . 
almost all centers ( 67% to 81% for nbn , rad50 , mre11a , and bard1 and > 90% for the other genes ) offered cascade testing to family members if a ( likely ) pathogenic variant was identified ( data not shown )  . 
notably , participants from the netherlands reported that they only tested first - degree relatives for chek2 1100delc variant when the estimated risk based on family history was lower than the risk conferred by having the variant , so testing for the variant had clinical utility because it would change surveillance recommendations.11 a high percentage ( 50% to 82% ) of enigma centers reported vus to patients ( fig 4 )  . 
 variant classification systems all respondents reported using the international agency for research on cancer five - tier classification system , 12 and many also used american college of medical genetics and genomics13 classification criteria . 
 the three methods are not mutually exclusive ; notably , the center in kuwait performs whole - genome sequencing for all cases , which is not represented in the figure . 
enigma , evidence - based network for the interpretation of germline mutant alleles . clinical management practices and guidelines most enigma centers ( 80% ) had risk management guidelines for a majority of non - brca1 / 2 genes considered reportable to patients ( fig 5 )  . 
 exceptions were bard1 , rad50 , and mre11a , for which 30% of centers had guidelines . although most enigma centers reported having some type of management guidelines for all genes except bard1 , rad50 , and mre11a , after review , only 10 of 20 countries had national guidelines for ( some of ) these genes ( table 1 )  . 
 furthermore , in some countries ( denmark and germany ) , the national guidelines were not gene specific ( ie , they were broken down by highand moderate - risk categories rather than by specific gene )  . 
ten countries had national guidelines for high - risk cancer syndromeassociated genes such as tp53 , cdh1 , and pten ( with the exception of belgium not having guidelines for cdh1 )  . 
the primary differences between countries were the starting age and type of diagnostic imaging ( mammography v magnetic resonance imaging [ mri ] v sonography ) and the policy on risk - reducing mastectomy . 
for instance , there was no consensus on the age to begin mammograms / mri for carriers of pathogenic variants in nf1 , men1 , palb2 ( age 25 v 30 years ) , or tp53 ( age 20 v 25 years )  . 
 the united kingdom guidelines differed from all others in that breast mri was not the standard imaging technique for carriers of pathogenic variants in other gene carriers ( except for tp53 )  . 
guidelines for risk - reducing mastectomy in carriers of palb2 pathogenic variants ranged among accepted ( n = 1 ) , consider depending on personal / family history ( n = 5 ) , and not enough evidence to recommend ( n = 1 )  . 
for pten and cdh1 , the guidelines that commented on preventive surgery ( four of the seven and five of the eight national guidelines , respectively ) mentioned risk - reducing mastectomy as a possible option . 
 subanalyses : enigma - us versus enigma - other centers and versus non - enigma centers discussion responses from the seven enigma centers in the united states ( enigma - us ) were compared with those of the other 31 enigma centers ( enigma - other )  . 
in addition , responses from 14 non - enigma centers in italy and nine non - enigma laboratories in the united kingdom were compared with those from 38 enigma centers across all countries . results of these comparisons are summarized in appendix figs a3 and a4 . 
a much smaller proportion of non - enigma centers from italy and the united kingdom tested each gene compared with enigma - affiliated centers ( appendix fig a3 )  . management guidelines were more likely to be available in the us - based enigma centers compared with the other enigma centers for all genes except bard1 , rad50 , mre11a , and men1 . 
of centers that responded varied by gene ( range , 12 to 36 centers responding about reporting pathogenic variants ; range , four to 20 centers responding about reporting vus )  . 
our global survey demonstrated that only a few genes are routinely analyzed beyond brca1 / 2 ; most centers clinically test them through multigene panels and report ( likely ) pathogenic variants ( and vus , to a slightly lesser extent ) to patients ; and gene - specific guidelines for bc and oc risk management are limited and differ between countries , especially in regard to starting age and type of imaging and risk - reducing surgery recommendations . with falling costs of sequencing and more genes being identified that are associated with increased bc and boc risk , multigene ( panel ) testing is becoming the northe results of our survey confirm this trend , showing that genes that are commonly offered on commercial panels were tested by > 50% of the surveyed centers . nevertheless , the value of multigene panel testing continues to be debated in the context of three main areas : limited additional yield of pathogenic variants in genes other than brca1 / 2 coupled with significantly increased interpretation workload , reliability of penetrance estimates for moderateor uncertain risk genes ( clinical validity ) , and evidence for informing management recommendations to improve patient outcomes ( clinical utility ) .9 our international survey demonstrates that the use of panel testing varies widely among countries . 
moreover , differences were observed when comparing enigma - affiliated centers with non - enigma italian and united kingdom centers ( with the latter testing nonbrca1 / 2 genes less than one third of the time )  . 
if management guidelines were available , centers were asked to specify the source of such guidelines ( local , national , or international , such as national comprehensive cancer network or national institute for health and care excellence )  . the genes included on panels was the most common concern raised by the participating centers . 
easton et al8 asserted that a genomic test should not be offered until its clinical validity is established8 ( p2 ) ; however , the utility of a gene needs to be continuously reconsidered as more data become available , and this can only be done by analyzing results from large cohorts of individuals who have been tested . 
concerns about the rates of vus were frequently expressed by the study participants , but just as variant rates have significantly decreased over the years for brca1 / 2 as a result of concerted classification efforts , the same trend will likely occur for other susceptibility genes , arguably at a faster pace as ( and provided that ) more laboratories worldwide contribute their testing data to population and peer - reviewed databases.5 , 28 , 29 despite the establishment of such databases , survey participants felt that robust , constantly updated international databases and global data sharing are still lacking . 
this is a worthy goal , but expert judgment in variant classification methods is still required , because fully automated approaches to variant classification that apply guidelines are not ready for clinical practice.6 at a basic level , some centers reported validation of the testing method as a barrier . 
therefore , it is important to recognize the technologic barriers in certain countries , although the transition to massively parallel sequencing is ultimately expected to increase throughput and optimize diagnosis without significantly elevating costs.30 there were also nonmedical barriers to implementing routine testing of many of these surveyed genes . 
insurance can be a major barrier in the united states , where , for example , medicare ( a us federal health insurance program for people who are age 65 years and for certain younger people with disabilities ) will only cover testing for individuals with a bc or oc diagnosis , and many insurers will not cover multigene panel testing if the patient has already had prior genetic testing . 
in many other countries , particularly those with national ( ie , universal ) health care , testing is approved on a gene - by - gene basis or as a package if research - derived evidence is considered robust enough to change clinical management . in terms of risk magnitudes , palb2 and tp53 are the only bc genes , in addition to brca1 / 2 , that consistently fall into the high - risk category across studies ( ie , confer levels of risk greater than four times that in the general population ) 8 ; the remainder have conflicting evidence regarding the risk category into which they fit.8 , 9 , 31 - 33 our survey confirmed that enigma centers test palb2 and tp53 relatively frequently and regard them as clinically actionable genes . 
 these two genes were tested much less consistently by non - enigma centers , evidencing the lack of consensus , even for genes that are generally regarded as high risk . 
 brip1 , rad51c , and rad51d are ever more accepted as oc but not bc risk predisposition genes ( two to five times the risk compared with the general population ) .15 , 32 notably , many respondents agreed that every patient with oc should be tested for these three genes ( in addition to brca1 / 2 )  . 
although there is currently no indication that oc treatment for a carrier of a pathogenic variant in one of these three genes would differ from that for a noncarrier , carriers may benefit from rrso at menopause . the uncertainties and inconsistencies regarding risk and testing practices are magnified when it comes to syndromic cancer genes like pten , cdh1 , stk11 , nf1 , nbn , and men1 , as well as genes conferring an uncertain risk such as bard1 , rad50 , and mre11a . 
although there is significant evidence for elevated bc risk and lobular bc risk in carriers of pathogenic variants in pten and in cdh1 , respectively , 34 - 36 it is likely that these bc risks ( and those from the other syndromic genes ) are overestimated and therefore unreliable , because they were derived from patients whose histories were consistent with these rare syndromes rather than from unselected patients.8 more robust and replicable penetrance estimates from large - cohort and population studies are certainly needed to further define risks . 
however , on the basis of both the evidence available from the literature and the results of our survey , which incorporate an international clinical perspective , the 16 genes can be grouped into five categories : high bc risk : palb2 , tp53 , pten , and cdh1 ; moderate bc risk : atm and chek2 ; bc risk of unclear magnitude ( but established risk for other cancer types ) : stk11 , nf1 , nbn , and men1 ; moderate oc risk : brip1 , rad51c , and rad51d ; and insufficient evidence for bc or oc risk : bard1 , rad50 , and mre11a . the clinical utility of multigene panel testing is assessed based on the improved outcomes of those managed by evidence - based surveillance or prevention approaches . 
a framework for management of moderate - risk bc / boc genes has been extensively reviewed by tung et al9 and includes a comparison of surveillance guidelines among the united states , united kingdom , and germany . 
there are limited national guidelines available even for genes such as palb2 , brip1 , rad51c , and rad51d , which most participants felt should always be tested because they importantly , are clinically actionable . 
this explains why the guidelines often differ in important aspects such as indication for risk - reducing surgery and type of diagnostic imaging recommendations . our study was initiated to provide a snapshot of enigma clinical practice for non - brca1 / 2 genes . 
because panel testing is currently being implemented in large regions of the world like asia , africa , and south america , similar surveys will need to be redistributed once more countries have established testing protocols . 
even at the time of the survey , testing protocols and surveillance recommendations were in flux in some countries , and broader gene panels were expected to be offered within a short time . 
 we acknowledge that our sampling of nonenigma centers was limited , and we aim to survey a more diverse collection of us , canadian , and other worldwide regional or community practices in future studies . massively parallel sequencing represents a transformational technology that we must learn to apply appropriately in health care . 
although the number of genes , other than brca1 / 2 , associated with bc / boc risk is growing , only a small subset of them have clinical utility at the moment . 
the goal of this study was to highlight the differences across countries and to determine what additional information and infrastructure are still needed to move toward more uniform testing practices and management guidelines internationally . our collected evidence suggests that the clinical usefulness of multigene panel testing for bc / boc predisposition can be improved by a better definition of the cancer risks associated with genetic variation in cancer susceptibility genes and by the availability of evidence - based management guidelines . 
to this end , it is key that clinicians share clinical and genetic data , through enigma and / or other international consortia focused on the clarification of the bc and oc risk associated with genetic variation , and that tested individuals are encouraged to participate in initiatives that collate genetic testing data and in long - term follow - up studies that evaluate intervention strategies . 
palmero , maria piane , marianna puzzo , maria christina sini , angela solano , manuel teixeira , mads thomassen , amanda toland , therese trngren , liliana varesco , jeffrey weitzel , encarna b . 
pedersen , maria piane , marianna puzzo , mark robson , maria rossing , maria christina sini , angela solano , jana soukupova , gianluca tedaldi , manuel teixeira , mads thomassen , maria grazia tibiletti , amanda toland , therese trngren , erica vaccari , liliana varesco , ana vega , barbara wappenschmidt , jeffrey weitzel , arcangela de nicolo , encarna b . 
 rien blok no relationship to disclose akira hirasawa research funding : astrazeneca maria adelaide caligo travel , accommodations , expenses : technogenetics mariarosaria calvello no relationship to disclose gabriele lorenzo capone no relationship to disclose pietro cavalli no relationship to disclose t.l. 
couch consulting or advisory role : astrazeneca research funding : grail other relationship : ambry genetics miguel de la hoya no relationship to disclose simona de toffol no relationship to disclose orland diez no relationship to disclose susan m . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) ros eeles honoraria : janssen - cilag speakers bureau : janssen - cilag anna efremidis no relationship to disclose florentia fostira no relationship to disclose david goldgar no relationship to disclose andreas hadjisavvas no relationship to disclose thomas v.o. 
hansen no relationship to disclose claude houdayer no relationship to disclose petra kleiblova no relationship to disclose sophie krieger no relationship to disclose conxi lzaro no relationship to disclose maria loizidou no relationship to disclose siranoush manoukian no relationship to disclose arjen r . 
 mark robson honoraria : astrazeneca erica vaccari consulting or advisory role : color genomics consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , pfizer ( inst ) travel , accommodations , expenses : astrazeneca liliana varesco consulting or advisory role : pfizer maria rossing no relationship to disclose maria christina sini no relationship to disclose angela solano no relationship to disclose jana soukupova no relationship to disclose gianluca tedaldi no relationship to disclose manuel teixeira no relationship to disclose mads thomassen no relationship to disclose maria grazia tibiletti no relationship to disclose amanda toland no relationship to disclose therese trngren honoraria : pfizer , astrazeneca ana vega no relationship to disclose yvonne wallis no relationship to disclose barbara wappenschmidt no relationship to disclose jeffrey weitzel no relationship to disclose amanda b . 
domchek , university of pennsylvania , philadelphia , pa ; anna efremidis , athens medical center ; florentia fostira , national centre for scientific research demokritos , athens , greece ; david goldgar , university of utah school of medicine , salt lake city , ut ; andreas hadjisavvas and maria loizidou , cyprus institute of neurology and genetics , nicosia , cyprus ; thomas v.o. 
pedersen , aalborg university hospital , aalborg , denmark ; akira hirasawa , keio university school of medicine , tokyo , japan ; claude houdayer , universit paris descartes and unicancer genetic group , paris ; sophie krieger , normandy university , cancer center f . 
palmero , barretos cancer hospital , barretos , so paulo , brazil ; mark robson , memorial sloan kettering cancer center , new york , ny ; angela solano , university of buenos aires , buenos aires , argentina ; manuel teixeira , instituto portugus de oncologia do porto francisco gentil , porto , portugal ; amanda toland , ohio state university , columbus , oh ; therese trngren , lund university , lund , sweden ; erica vaccari , dana - farber cancer institute , boston , ma ; barbara wappenschmidt , university hospital cologne and german consortium of hereditary breast and ovarian cancer , cologne , germany ; and jeffrey weitzel , city of hope , duarte , ca . support supported by grant no . 
couch fj , hart sn , sharma p , et al : inherited mutations in 17 breast cancer susceptibility genes among a large triple - negative breast cancer cohort unselected for family history of breast cancer . 
laduca h , stuenkel aj , dolinsky js , et al : utilization of multigene panels in hereditary cancer predisposition testing : analysis of more than 2 , 000 patients . 
maxwell kn , hart sn , vijai j , et al : evaluation of acmg - guideline - based variant classification of cancer susceptibility and non - cancer - associated genes in families affected by breast cancer . 
domchek sm , bradbury a , garber je , et al : multiplex genetic testing for cancer susceptibility : out on the high wire without a net ? j clin oncol 31 : 1267 - 1270 , 2013 8 . 
richards s , aziz n , bale s , et al : acmg laboratory quality assurance committee : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
janatov m , boreck m , soukupov j , et al : palb2 as another candidate gene for genetic testing in patients with hereditary breast cancer in czech republic [ in czech ]  . 
robays j , stordeur s , hulstaert f , et al : oncogenetic testing and follow - up for women with hereditary breast / ovarian cancer , li fraumeni syndrome and cowden syndrome . 
robays j , stordeur s , hulstaert f , et al : oncogenetic testing , diagnosis and follow - up in birt - hoggdub syndrome , familial atypical multiple mole melanoma syndrome and neurofibromatosis 1 and 2 . 
national institute for health and care excellence : familial breast cancer : classification , care and managing breast cancer and related risks in people with a family history of breast cancer . 
lincoln se , kobayashi y , anderson mj , et al : a systematic comparison of traditional and multigene panel testing for hereditary breast and ovarian cancer genes in more than 1000 patients . 
castra l , krieger s , rousselin a , et al : next - generation sequencing for the diagnosis of hereditary breast and ovarian cancer using genomic capture targeting multiple candidate genes . 
pharoah pd , guilford p , caldas c : incidence of gastric cancer and breast cancer in cdh1 ( e - cadherin ) mutation carriers from hereditary diffuse gastric cancer families . 
questions included in the surveys ( by mode of distribution ) ( continued ) question testing methods and setting which method is used to test for gene x ? in - person survey only which genes do you agree should be tested for every bc or oc patient eligible for genetic testing ? describe the gene panels currently used ( if any ) and if they are used in the diagnostic or research setting if you are not currently using gene panels but may in the future , what do you think is required before starting to use them ? ii variant classification classification system ii - 1 ii - 2 reporting and cascade testing of variants clinical i . 
questions included in the surveys ( by mode of distribution ) ( continued ) in - person survey only question ii - 3 variant interpretation in - person and paper surveys paper survey only surveymonkey * who takes responsibility for interpreting the clinical significance of the identified variants ? for cancer susceptibility genes : who takes responsibility for variant interpretation and reporting ? clinical scientist clinical geneticist genetic counselor oncologist ( medical / surgical ) other ( specify ) who takes responsibility for discussing the clinical significance / utility of an identified variant ? ( same choices as above ) are there clinical guidelines for managing patients who carry a pathogenic or likely pathogenic variant in a bc susceptibility gene ? iii risk management guidelines for which genes do you agree that the cancer - associated risks are high enough to alter clinical practice / management ? are management guidelines available at your center for patients with ( likely ) pathogenic variants in these genes ? yes , national guidelines yes , local guidelines or local adaptations of national guidelines no , guidelines are not currently available if clinical management guidelines are available at your center for the specified genes , please provide digital copy , reference , or web site link note . 
questions i - 4 and iii of the in - person survey were asked at a different time compared with the remainder of the survey ; therefore , answers were collected from only 23 centers . 
 these two questions were asked at a different time ( during evidence - based network for the interpretation of germline mutant alleles meeting in cyprus in january 2017 compared with survey questionnaire )  . 
the centers that tested each gene through research only were compared with the proportion of centers that tested the gene only clinically and proportion of those that tested the gene for both clinical and research purposes . 
genes tested regularly by evidence based network for the interpretation of germline mutant alleles ( enigma ) centers in the united states ( enigma - us ) versus other enigma centers ( enigma - other ) versus italian and united kingdom non - enigma centers . 
 of centers testing given gene regularly ( defined as ordered for > 50% of patients eligible for genetic testing , by criteria that we recognize may differ by center / country ) is shown above each bar . 
of centers that answered this question was four to seven , depending on the gene ; of the 31 enigma - other centers , a range of 22 to 30 centers answered this question . 
most preceding studies have retrospectively sought to identify high - risk criteria among patients who are at low risk for nodal metastasis.2 such studies are inherently awed , because patients were offered sln biopsy ( slnb ) only if the surgeon believed the pretest probability of sln positivity was sufciently high to justify the procedure . 
bellomo et al1 approached this problem differently by including only patients in whom slnb would be considered on the basis of mayo clinic clinicopathologic ( cp ) criteria , and then they identied those at sufciently low risk to forgo slnb . 
a few previous studies have also identied lowrisk subsets among such patients , but the criteria for selecting those patients have not been widely adopted in clinical practice.3 , 4 perhaps the most signicant contribution of the bellomo et al1 study to melanoma risk prediction is the incorporation of a gene - expression prole ( gep ) not as a stand - alone risk predictor , but a continuous risk model combined with cp risk factors ( cp - gep )  . 
this approach permits better transparency of the additive predictive value of the gep , use of continuous variables , and individualized risk prediction ( as opposed to classifying patients into discrete groups )  . 
this facilitates a discussion of the clinically relevant risk threshold for the individual patient.5 development of all future predictive markers should adhere to this standard . future studies must more clearly demonstrate clinical utility . 
a proportion of sln - positive patients would therapy.6 , 7 be eligible to receive effective adjuvant furthermore , by omitting slnb , patients would not benet from the improved recurrence - free survival associated with the procedure or the potential diseasespecic survival advantage seen in the subset of patients with a positive slnb.8 finally , sln positivity as an end point is itself inaccurate . 
the mslt - 1 ( clinicaltrials.gov identier : nct00275496 ) trial demonstrated a 27% false - negative rate for slnb in patients with sufcient long - term follow - up , and recurrences are frequently delayed in thin melanoma.8 any statements about the performance characteristics of slnb and slnb rrs in patients with thin melanomas and inadequate follow - up should be made with caution . we explored the potential clinical utility of the models by using decision curve analysis ( fig 1 ) and found the cp - gep model only incrementally superior to the cp model when offering slnb above a threshold of 5% . net benet for the cp - gep model increases with increasing risk threshold . 
this suggests that a clinician with an anxious , t patient ( ie , a low threshold , 5%10% , for slnb ) should perform the procedure regardless of the models . 
however , in a patient with comorbidities in whom a threshold of 20% is more appropriate , cp - gep would maximize the relative probability of identifying positive nodes while limiting unnecessary procedures . clearly , the clinical validity of combining gep with an effective cp - based risk score requires further study . as the authors appropriately acknowledge , external validation will be critical . 
for example , a net benet of 0.1 ( 10% ) for a model indicates that if it is used to guide sentinel lymph node ( sln ) biopsy , it is equivalent to performing an additional 10 positive sln biopsies per 100 patients treated . threshold probability refers to the level of predictive certainty at which a treatment would be chosen by a patient and physician . 
in this case , the threshold probability could be considered the sln positivity rate at which a surgeon would perform the procedure for a given patient . this decision reects the relative value a surgeon and / or patient ascribes to a positive versus a negative sln biopsy . 
a guide to interpreting decision curve analysis is available in vickers et al.10 sln biopsy for none ( solid black ) , sln biopsy for all ( solid gray ) , sln biopsy based on cp model ( dashed red ) , sln biopsy based on gep model ( dashed black ) , sln biopsy based on cp - gep model ( dashed green )  . 
reprinted with permission from bellomo et al.1 we laud the efforts of bellomo et al1 to reduce the frequency of slnb , a costly , imperfect , and occasionally morbid procedure . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . no potential conicts of interest were reported . references bellomo d , arias - mejias sm , ramana c , et al : model combining tumor molecular and clinicopathologic risk factors predicts sentinel lymph node metastasis in primary cutaneous melanoma . 
j clin oncol 31 : 4387 - 4393 , 2013 bartlett ek , peters mg , blair a , et al : identication of patients with intermediate thickness melanoma at low risk for sentinel lymph node positivity . 
ann surg oncol 23 : 250 - 256 , 2016 sinnamon aj , neuwirth mg , yalamanchi p , et al : association between patient age and lymph node positivity in thin melanoma . 
mulder p , dwarkasing jt , hollestein lm , et al : validation of a clinicopathologic and gene expression prole ( cp - gep ) model for sentinel lymph node metastasis in primary cutaneous melanoma . 
 clinical activity of pembrolizumab in a patient with metastatic triplenegative breast cancer without tumor programmed death - ligand 1 expression : a case report and correlative biomarker analysis sajjad bhatti jaimie heldstab carolyn lehn ossama tawfik ryan m . 
godwin priyanka sharma author affiliations appear at the end of this article . supported by the university of kansas research career award and the university of kansas cancer centers cancer center support grant ( p30 ca168524 ) biospecimen repository core facility . clinical trial information : nct02302742 . corresponding author : priyanka sharma , md , university of kansas medical center , 2330 shawnee mission parkway , suite 210 , westwood , ks 66205 ; e - mail : psharma2@ kumc.edu. introduction triple - negative breast cancer ( tnbc ) accounts for 10% to 20% of all breast cancers and is associated with poor prognosis.1 compared with hormone - positive breast cancer , tnbc is characterized by a higher proportion of visceral relapse and a short survival after development of metastatic disease , highlighting the pressing need for identification of more effective systemic therapies for this subgroup.2 , 3 cancers use multiple mechanisms to evade the immune response . 
pd - 1 and its ligands , programmed death - ligands 1 and 2 ( pd - l1 and pd - l2 ) , play a major role in maintenance of immune evasion.4 , 5 pd - l1 is aberrantly expressed in many malignancies , including tnbc.6 , 7 binding of pd - 1 to its ligands results in the downregulation of lymphocyte activation , and inhibition of the interaction between pd - 1 and its ligands promotes immune responses . 
in support of preclinical findings , there is emerging evidence of the clinical efficacy of agents targeting pd - 1 / pd - l1 in tnbc.8 - 10 pembrolizumab is a humanized monoclonal antibody that binds to pd - 1 . 
a recent study demonstrated that in pd - l1expressing advanced tnbc , pembrolizumab produced response rates of 18%.8 several studies are investigating pembrolizumab in earlyand advanced - stage tnbc.11 - 14 here we describe the case of a 48 - year - old woman with metastatic tnbc who , after exhausting all effective chemotherapeutic options , demonstrated excellent clinical and radiologic response to pembrolizumab ( tumor pd - l1 negative )  . 
six months after finishing adjuvant radiation , she developed recurrence in left axillary lymph nodes and received carboplatin plus gemcitabine plus iniparib in a clinical trial . after five cycles of treatment she was switched to ixabepilone ( because of an allergic reaction to carboplatin )  . 
1 year and then developed metastatic disease in the left cervical lymph nodes , which was rendered into complete radiologic response with cisplatin . after a 4 - month break from cisplatin , there was progression of left cervical adenopathy , which was treated with radiation . 
 neoadjuvant docetaxel + carboplatin + erlotinib ( clinical trial ) adjuvant adriamycin + cytoxan followed by radiation completed aug 2010 carboplatin + gemcitabine + iniparib ( clinical trial ) with clinical response ; treatment stopped for toxicities progression ixebepilone cisplatin 90 mg / m2 x five cycles with cr left supraclavicular radiation cisplatin ; stopped for toxicity progression on capecitabine + doxil pembrolizumab initiated eribulin sep 2009 feb 2010 jan 2011 aug 2011 nov 2012 jul 2013 jul 2014 may 2015 mar 2016 diagnosed with stage iii ( ct3n3 ) tnbc left lumpectomy and alnd ypt2n3a metastatic disease , left axilla left alnd ; all lymph nodes negative for cancer metastatic disease , left supraclavicular lymph nodes re - appearance of left supraclavicular and cervical adenopathy pulmonary metastasis left cervical ln biopsy ; grade 3 metastatic tnbc cisplatin with good clinical response ( cisplatin was discontinued because of nephrotoxicity )  . 
she then received various sequential single - agent chemotherapies with temporary disease stabilization as best response and eventually developed progressive left cervical and occipital adenopathy . she continued to maintain an excellent performance status and did not qualify for any available clinical trials . 
pd - l immunohistochemical testing ( details provided in data supplement ) of the cervical lymph nodes ( specimen obtained in may 2015 ) showed no ( 0% ) pd - l1 expression ( fig 2 )  . given the lack of other available treatment options and the presence of other tumor biomarkers , the decision was made to offer treatment with pembrolizumab ( 2 mg / kg ) , which was started in march 2016 . 
hypermethylation of the brca1 promoter has been proposed as one of the mechanisms for functionally inactivating the brca1 gene.16 - 18 brca1 mutationassociated cancers are known to demonstrate a high degree of genomic instability , a characteristic that is also shared by tumors with brca1 pm.19 genetically complex tumors exhibit a high nonsynchronous fig 1 . 
in 2011 , lehmann et al22 used a 2188 gene expression signature to stratify ( tnbc ) into six subtypes : basal - like 1 ( bl1 ) , basal - like 2 , mesenchymal , mesenchymal stem celllike , immunomodulatory ( im ) , and luminal androgen receptorlike ( lar )  . 
 of 10% to 19% in patients with pd - l1positive tnbc ( although different pd - l1 antibodies and / or cut points and laboratories were used to define pd - l1 positivity in trials ) .8 , 9 , 10 , 24a on the basis of encouraging phase i data , larger studies are evaluating pd - 1 / pd - l1 antibodies in unselected tnbc . 
for efficient evaluation of this new class of agents , there is a critical need to develop biomarkers of response that can be used to successfully select patients who are most likely to benefit . we report a case study of a patient with heavily pretreated ( six prior lines of chemotherapy ) metastatic tnbc who demonstrated clinical response to pembrolizumab . 
the metastatic tumor did not demonstrate pd - l1 expression ; however , other biomarkers were detected , which provide some insight into the clinical response noted in this case . tnbc is a molecularly heterogeneous entity for which additional subclassifications have been proposed . 
using the insight tnbctype assay , our patients tumor was classified into the bl1 subclass and also demonstrated positive im status . many of the genes involved in this im signature are associated with natural killer cells and activated t cells , implying an active immune response to the tumor ( unpublished data )  . 
in support of this hypothesis , a recent study of atezolizumab plus nab - paclitaxel in metastatic tnbc demonstrated that responders had higher baseline tils compared with nonresponders.25 a recent study also demonstrated that the correlation between tils and pd - l1 expression may not be linear in breast cancer.26 expression of pd - l1 on tumor cells is of interest as a biomarker of response to pd - 1 / pd - l1 inhibitors . 
however , there are several variables that affect the analytical validity of pd - l1 testing ; to date , there is no single validated antibody for this testing . pd - l1 is expressed in approximately 20% to 58% of tnbc , and it is not clear whether pd - l1 expression is predictive of response to immune therapy in tnbc.7 , 8 , 27 our patients tumor demonstrated lack of pd - l1 staining . 
given the concerns surrounding the analytic and clinical validity of pd - l1 testing , it is possible that this was a falsenegative test and that the tumor may show a different outcome if tested using a different assay and antibody . pd - l1 expression may be associated with clinical response to antipd - 1 / pd - l1 antibodies in patients with malignant melanoma or nonsquamous nsclc.28 however , a small proportion of patients with pd - l1negative cancers also benefit from antipd - 1 therapy.10 , 27 - 29 this indicates that using pd - l1 alone as a marker of selection and response to these agents might exclude some patients who could potentially benefit . translational studies to identify reliable biomarkers that would aid patient selection for immune therapy and further improve the riskbenefit ratio for these drugs are needed . 
 sajjad bhatti no relationship to disclose jaimie heldstab consulting or advisory role : novartis travel , accommodations , expenses : novartis carolyn lehn no relationship to disclose ossama tawfik stock and other ownership interests : radpath solutions consulting or advisory role : radpath solutions patents , royalties , other intellectual property : trays for tissue biopsy samples ; methods of making and methods of using thereof . 
hout employment : insight genetics leadership : insight genetics stock and other ownership interests : insight genetics patents , royalties , other intellectual property : i hold patents with insight genetics , but do not receive royalties . travel , accommodations , expenses : insight genetics rob s . 
seitz employment : insight genetics , bethesda group leadership : insight genetics , bethesda group stock and other ownership interests : insight genetics , bethesda group consulting or advisory role : foundation medicine , agendia , celsee diagnostics daniel b . 
godwin no relationship to disclose priyanka sharma consulting or advisory role : abbvie , myriad genetics research funding : novartis ( inst ) , celgene ( inst ) , bristolmyers squibb ( inst ) , cosmo biosciences ( inst ) travel , accommodations , expenses : abbvie , celgene , myriad genetics affiliations sajjad bhatti , jaimie heldstab , carolyn lehn , ossama tawfik , ryan m . 
kohler ba , sherman rl , howlader n , et al : annual report to the nation on the status of cancer , 1975 - 2011 , featuring incidence of breast cancer subtypes by race / ethnicity , poverty , and state . 
ghebeh h , mohammed s , al - omair a , et al : the b7 - h1 ( pd - l1 ) t lymphocyte - inhibitory molecule is expressed in breast cancer patients with infiltrating ductal carcinoma : correlation with important high - risk prognostic factors . neoplasia 8 : 190 - 198 , 2006 8 . 
emens la , braiteh fs , cassier p , et al : inhibition of pd - l1 by mpdl3280a leads to clinical activity in patients with metastatic triple - negative breast cancer . 
dirix l , takacs i , nikolinakos p : avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in patients with locally advanced or metastatic breast cancer : a phase 1b javelin solid tumor trial . 
loi s , sirtaine n , piette f , et al : prognostic and predictive value of tumor - infiltrating lymphocytes in a phase iii randomized adjuvant breast cancer trial in node - positive breast cancer comparing the addition of docetaxel to doxorubicin with doxorubicin - based chemotherapy : big 02 - 98 . 
wei m , grushko ta , dignam j , et al : brca1 promoter methylation in sporadic breast cancer is associated with reduced brca1 copy number and chromosome 17 aneusomy . 
adams s , diamond jr , hamilton ep , et al : phase ib trial of atezolizumab in combination with nab - paclitaxel in patients with metastatic triple - negative breast cancer ( mtnbc )  . 
tung n , garber je , hacker mr , et al : prevalence and predictors of androgen receptor and programmed death - ligand 1 in brca1 - associated and sporadic triple - negative breast cancer . 
gandini s , massi d , mandal`a m : pd - l1 expression in cancer patients receiving anti pd - 1 / pd - l1 antibodies : a systematic review and meta - analysis . 
spigel dr , reckamp kl , rizvi na , et al : a phase iii study ( checkmate 017 ) of nivolumab ( nivo ; anti - programmed death - 1 [ pd - 1 ] ) vs docetaxel ( doc ) in previously treated advanced or metastatic squamous ( sq ) cell non - small cell lung cancer ( nsclc )  . 
brock , mbbs , phd1 , 2 purpose the 21 - gene recurrence score ( rs ) is used to identify patients with hormone receptorpositive earlystage breast cancer who may benet from the addition of chemotherapy to endocrine therapy . 
 iorgulescu et al context key objective although grade 3 is considered a poor prognostic factor in estrogen receptorpositive , human epidermal growth factor receptor 2negative breast cancer , the predictive benet of multigene recurrence score ( rs ) testing in this subgroup remains unclear . knowledge generated our analysis of the national cancer database that comprises more than 70% of all newly diagnosed cancers in the united states reveals that rs results in grade 3 t1c / t2 n0 and n1 breast cancer provide important discriminatory information with regard to chemotherapy benet . 
in addition , our ndings reveal signicant variability in national patterns of rs testing and chemotherapy use for grade 3 tumors . relevance expanding national clinical guidelines with regard to the value of rs testing and increasing use of rs testing in grade 3 tumors may facilitate de - escalation of therapy in those with a low rs . tumor grade is prognostic and independently associated with risk for recurrence ; however , histopathologic high grade may not correlate well with the risk provided by in the planb trial ( clinicaltrials.gov identier : the rs . nct01049425 ) , approximately 50% of grade 3 tumors had an rs less than 31.13 the correlation of histologic grade with the predictive benet of rs has not been assessed comprehensively . 
the proportion of grade 3 tumors in the tailorx trial , although low , reects the typical grade distribution , which accounts for 17.8% of all included tumors across scores , and it was 22% in the original cohort for the development of the rs.1 as a result , the predictive benet of rs and its potential for preventing overtreatment in grade 3 invasive breast carcinomas may be underappreciated . 
rs risk groups were categorized as low ( less than 18 ) , intermediate ( 18 to 30 ) , and high ( 31 or higher ) as originally dened by paik et al.1 variables were coded according to the facility oncology registry data standards manual revised for 2013.20 variables of interest our primary outcomes of interest were receipt of rs testing ( yes / no ; with no dened as multigene signature testing neither ordered nor performed ) and overall survival ( os ) using national death index data provided by the ncdb and dened as the time from date of diagnosis to death , with patients censored at the date of last follow - up available in the ncdb ( december 31 , 2015 )  . 
er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; pr , progesterone receptor ; rs , recurrence score . multigene rs for grade 3 breast cancer women newly diagnosed with pt1c - 2 pn0 - 1 breast cancer from 2010 to 2015 excluded prior diagnosis of cancer metastatic disease at diagnosis unknown / negative er status unknown / negative pr status unknown / positive her2 status unknown nottingham grade unknown whether received multigene prediction assay multigene prediction assay other than rs treated entirely at an institution other than the initial diagnosing institution unknown / no breast surgery unknown / no endocrine therapy unknown / had neoadjuvant systemic therapy unknown whether received adjuvant chemotherapy excluded grade 1 and 2 invasive breast cancer study population : n0 - 1 t1c - 2 m0 er - positive / her2 - negative breast cancer treated with definitive surgery and endocrine therapy without neoadjuvant chemotherapy ( n = 172 , 937 ) grade 3 breast cancers for analysis ( n = 30 , 864 ) pn0 grade 3 ( n = 21 , 440 ) pn1 grade 3 ( n = 9 , 720 ) treatments received beyond chemotherapy ( ie , surgery type [ breast conserving surgery / mastectomy ] , adjuvant radiotherapy [ yes / no ] )  . statistical analyses rs testing by clinicopathologic characteristics for all patients was compared using 2 tests and t tests , as appropriate . 
multivariable logistic regression for receipt of rs testing was then performed , with stratication by pn status . to examine unadjusted differences in os by chemotherapy receipt and rs , kaplan - meier method and log - rank test were used . 
potential interaction effects of rs testing with adjuvant chemotherapy were explored using a previously described methodology.22 to evaluate the accuracy of rs testing and nottingham / bloom - richardson grade encoding , patients treated for breast cancer from 2010 to 2015 were queried from the cancer registry submitted data from brigham and womens hospital and dana - farber cancer institute . 
for patients with low rs , 9.1% received chemotherapy , which was not associated with a signicantly increased 5 - year unadjusted os rate ( p = .07 ; table 3 ; fig 2a )  . 
for patients with low rs , 25.9% received chemotherapy , and this was not associated with a signicantly increased unadjusted 5 - year os ( p = .27 ; table 3 ; fig 2b )  . 
of 351 adults with invasive breast carcinoma who had rs testing between 2010 and 2015 , 74.7% ( n = 259 ) were encoded and submitted for inclusion into cancer registries . 
nottingham / bloom - richardson grade was missing or incorrectly encoded in 6.6% of patients ( n = 17 ) , including 8.1% ( n = 3 ) with grade 3 disease . 
in particular , of the 37 grade 3 registry - submitted institutional patients with rs testing , 16.2% ( n = 6 ) had missing scores in registry data , and only 3.2% ( n = 1 ) were incorrectly encoded ( as no rs instead of an actual rs of 22 )  . discussion in this large national cohort , we evaluated the use of rs , use of adjuvant chemotherapy , and os for women with breast cancer , with a focus on high tumor grade . 
of note , chemotherapy was associated with signicant os improvements in grade 3 invasive breast cancers with high rs , and although associated with improved os in univariable analyses , insignicant termediate rs was not predictive of chemotherapy os benet when risk adjusted for clinicopathologic characteristics . 
to our knowledge , these ndings represent the largest analysis to date of the potential impact of rs on the outcomes and management of grade 3 tumors and suggest that the assumption that all pt1c / 2 pn0 / 1 , erpositive histopathologic grade 3 tumors are high risk and will consequently benet from adjuvant chemotherapy may be unmerited . although we await the rxponder trial nal results , the data presented here suggest that patients with a pt1c / 2 n0 / 1 grade 3 tumor with high rs derive benet from chemotherapy ( 92% 5 - year os with chemotherapy v 67% to 79% without ) , whereas grade 3 tumors with low and intermediate rs do not . 
our results further reinforce the utility of broad rs testing in grade 3 tumors and suggest that rs can help to distinguish the anticipated chemotherapy benet among this heterogeneous group of tumors . the rate of rs testing is less in pn1 disease than in pn0 disease ( 36% in 2015 v 72% in pn0 ) but is expanding in both groups because the importance of tumor biology is increasingly recognized . 
in our study , the increased use of rs testing in pn0 grade 3 disease ( 64.1% ) and lower rate of chemotherapy ( 9.1% ) in patients with low rs suggest that clinical practice is increasingly incorporating rs results into decision trees for pn0 grade 3 disease . 
however , our ndings also suggest that a signicant proportion of patients with pn1 grade 3 disease who do not undergo rs testing may be overtreated and receive chemotherapy with no added os benet . 
at risk no rs , no chemotherapy no rs , chemotherapy low rs , no chemotherapy low rs , chemotherapy intermediate rs , no chemotherapy 1 , 838 intermediate rs , chemotherapy high rs , no chemotherapy high rs , chemotherapy 3 , 058 3 , 446 2 , 569 2 , 335 3 , 081 2 , 961 3 , 401 2 , 501 1 , 790 2 , 300 3 , 026 2 , 545 3 , 034 2 , 133 1 , 508 1 , 987 2 , 605 1 , 832 2 , 298 1 , 504 1 , 028 1 , 406 1 , 812 1 , 193 1 , 538 1 , 147 no rs , no chemotherapy low rs , no chemotherapy no rs , chemotherapy low rs , chemotherapy intermediate rs , no chemotherapy intermediate rs , chemotherapy high rs , no chemotherapy high rs , chemotherapy time ( months ) no . 
at risk no rs , no chemotherapy no rs , chemotherapy low rs , no chemotherapy low rs , chemotherapy intermediate rs , no chemotherapy intermediate rs , chemotherapy high rs , no chemotherapy high rs , chemotherapy 1 , 005 4 , 803 4 , 742 4 , 231 3 , 127 2 , 045 1 , 145 no rs , no chemotherapy low rs , no chemotherapy no rs , chemotherapy low rs , chemotherapy intermediate rs , no chemotherapy intermediate rs , chemotherapy high rs , no chemotherapy high rs , chemotherapy fig 2 . 
overall survival ( os ) in patients with grade 3 invasive breast cancer , stratied by recurrence score ( rs )  . adjuvant chemotherapy os estimated by kaplan - meier method for patients with ( a ) pn0 and ( b ) pn1 grade 3 invasive breast cancer , stratied by rs and adjuvant chemotherapy , with an underlying number at risk table . adjuvant chemotherapy ( solid lines ) was associated with signicantly better median os than no adjuvant chemotherapy ( dashed lines ) for intermediate , high , and no rs . are notably higher than those reported in the planb trial ( 18% of grade 3 tumors ) .13 however , our ndings are in keeping with those reported in the microarray in nodenegative ( or 1 - 3 positive lymph node ) disease may avoid trial , where patients were chemotherapy ( mindact ) stratied by both anatomic and genomic risk using a 70gene signature . 
boldface indicates signicance at p , .05. abbreviations : ajcc , american joint committee on cancer ; hr , hazard ratio ; idc , invasive ductal carcinoma ; ilc , invasive lobular carcinoma ; imc , invasive mixed carcinoma ; pr , progesterone receptor ; ref , reference ; rs , recurrence score ; rt , radiotherapy . registryin our multi - institutional cohort of however , submitted patients , 92% with grade 3 disease demonstrated accurate grade coding of whom only 3% had an incorrectly encoded rs , which suggests that key breast cancerspecic factors are encoded into national registries with encouraging accuracy . 
in addition , the ncdb only includes os data , which precludes assessment of breast cancerspecic , progression - free , or recurrence - free survival , end points that may be of greater relevance in the clinical setting . 
as such , our median follow - up is only 41.3 months and the event rate only 6.2% ; nevertheless , we incorporated a large sample size that powered the detection of clinically relevant differences in rs predictive value . 
finally , the ncdb lacks detailed information about type , dose , and duration of chemotherapeutic and hormonal treatments and , in particular , has limited granular inuence clinical decision data about making about when to administer adjuvant chemotherapy . the factors that for example , across all patients with grade 3 disease who were not administered chemotherapy , the ncdb only encoded a reason in 27% ( 21% because chemotherapy was contraindicated and 7% because chemotherapy was recommended but refused by the patient )  . 
to help to address the lack of data about patient contraindications , we included charlson - deyo comorbidity index data in our riskadjusted analyses , and higher indices were associated with reduced chemotherapy use . 
furthermore , our ndings show signicant variability in national patterns of rs testing and chemotherapy use for grade 3 disease , which suggests opportunities for more comprehensive national guidelines for rs testing in high - grade tumors . 
lester employment : novartis institutes for biomedical research ( i ) , restorbio ( i ) leadership : blade therapeutics ( i ) stock and other ownership interests : novartis patents , royalties , other intellectual property : more than 20 patents issued and pending related to health care therapies ( i ) travel , accommodations , expenses : novartis ( i ) , blade therapeutics ( i ) elizabeth a . 
mittendorf honoraria : physician education resource consulting or advisory role : peregrine pharmaceuticals , tapimmune , sellas life sciences , merck , genomic health research funding : galena biopharma ( inst ) , genentech ( inst ) , roche ( inst ) , astrazeneca ( inst ) , emd serono ( inst ) no other potential conicts of interest were reported . acknowledgment we thank tari king , md , for helpful input and the cancer registrars at brigham and womens hospital and dana - farber cancer institute for invaluable assistance in data acquisition . references paik s , shak s , tang g , et al : a multigene assay to predict recurrence of tamoxifen - treated , node - negative breast cancer . 
n engl j med 351 : 2817 - 2826 , 2004 paik s , tang g , shak s , et al : gene expression and benet of chemotherapy in women with node - negative , estrogen receptor - positive breast cancer . 
j clin oncol 24 : 3726 - 3734 , 2006 albain ks , barlow we , shak s , et al : prognostic and predictive value of the 21 - gene recurrence score assay in postmenopausal women with node - positive , oestrogen - receptor - positive breast cancer on chemotherapy : a retrospective analysis of a randomised trial . 
lancet oncol 11 : 55 - 65 , 2010 dowsett m , cuzick j , wale c , et al : prediction of risk of distant recurrence using the 21 - gene recurrence score in node - negative and node - positive postmenopausal patients with breast cancer treated with anastrozole or tamoxifen : a transatac study . 
harris ln , ismaila n , mcshane lm , et al : use of biomarkers to guide decisions on adjuvant systemic therapy for women with early - stage invasive breast cancer : american society of clinical oncology clinical practice guideline . 
new york , ny , springer , 2017 sanders ma , wong sm , iorgulescu jb , et al : changes and clarications in the eighth edition of the ajcc cancer staging system for breast cancer . 
 multigene rs for grade 3 breast cancer giuliano ae , connolly jl , edge sb , et al : breast cancer - major changes in the american joint committee on cancer eighth edition cancer staging manual . 
wong wb , ramsey sd , barlow we , et al : the value of comparative effectiveness research : projected return on investment of the rxponder trial ( swog s1007 )  . 
gluz o , nitz ua , christgen m , et al : west german study group phase iii planb trial : first prospective outcome data for the 21 - gene recurrence score assay and concordance of prognostic markers by central and local pathology assessment . 
roberts mc , miller dp , shak s , et al : breast cancer - specic survival in patients with lymph node - positive hormone receptor - positive invasive breast cancer and oncotype dx recurrence score results in the seer database . 
j clin epidemiol 45 : 613 - 619 , 1992 iorgulescu jb , harary m , zogg ck , et al : improved risk - adjusted survival for melanoma brain metastases in the era of checkpoint blockade immunotherapies : results from a national cohort . 
yee martin kaiser heather landau jean - marie michot antoine hollebecque luisa veronese martina makrutzki bethany pitcher igor puzanov jose baselga author affiliations and support information ( if applicable ) appear at the end of this article . clinical trial information : nct01524978 . corresponding author : noopur raje , md , professional office building 216 , harvard medical school , 55 fruit st , boston , ma 02114 ; e - mail : nraje@mgh.harvard.edu. introduction multiple myeloma ( mm ) is a genetically heterogeneous , complex disease that arises as a result of a variety of mutations in pathways deregulating the intrinsic biology of the plasma cell.1 although immunomodulatory drugs and proteasome inhibitors have improved outcomes in patients with mm , 2 , 3 patients with relapsed or refractory disease have a poor prognosis.4 despite the identification of many of the genetic events involved in the development of mm , no treatments specifically targeting genetic mutations have been developed to date . 
additional study design details are described in the data supplement . patients patients in the mm cohort had to have previously treated , measurable , relapsed or refractory mm with confirmed brafv600 mutation . 
the presence of brafv600 mutations was confirmed retrospectively in a central laboratory using the roche companion diagnostic cobas 4800 braf v600 test or other standard methodology . assessments the following assessments for mm were performed 8 weeks after the start of therapy and every 4 weeks thereafter : serum protein electrophoresis with quantitation of monoclonal protein level ; urine protein electrophoresis using 24 - hour urine protein electrophoresis ; and serum levels of free light chains , lactate dehydrogenase , and - 2 microglobulbone marrow analysis was performed only to confirm complete response ( cr ) after two consecutive immunofixation analyses were negative . efficacy was evaluated using international myeloma working group uniform response criteria.17 , 18 evaluations were performed at baseline , 8 weeks after the start of vemurafenib administration , every 4 weeks thereafter during treatment , and at the end of treatment . 
responses were classed as cr , stringent cr , very good partial response ( vgpr ) , partial response ( pr ) , stable disease ( sd ) , progressive disease , and clinical relapse . 
responders were defined as those patients with pr or better ( ie , cr , stringent cr , pr , or vgpr )  . statistical analysis the primary efficacy end point of ve - basket was the response rate at week 8 . 
for the purposes of this analysis , two response assessments were required with no specified time between these assessments , although the protocol required that these two assessments be 4 weeks apart . an adaptive simon two - stage design was used to minimize the number of patients treated if vemurafenib was deemed ineffective for a specific tumor type . 
assuming response rates as specified in the hypothesis testing , a power of 80% for a high desirable response and 70% for a low desirable response , and a two - sided of 0.1 , the number of patients required in each cohort was seven for stage 1 , and 13 or 19 for stage 2 , depending on the results in stage 1 . 
however , if a clear clinical benefit was observed for patients in a cohort ( eg , the majority of patients recorded sd at week 8 and no cr or pr was recorded ) , then enrollment in stage 2 might be allowed for the cohort after discussion with the sponsor and study steering committee . 
the data presented here are the results of the final analysis . seven patients entered stage 1 of the mm cohort of the ve - basket study , followed by enrollment of an additional two patients because clear clinical benefit was observed , even though the prespecified minimal response rate was not achieved . 
the patient received palliative radiotherapy and eight cycles of lenalidomide , bortezomib , and dexamethasone before undergoing high - dose melphalan therapy with autologous stem - cell transplantation in november 2008 . 
baseline characteristics of patients with brafv600 mutationpositive multiple myeloma treated with vemurafenib patients with multiple myeloma ( n = 9 ) characteristic male female age , years , median ( range ) ecog performance status brafv600 mutation type * monoclonal protein v600e v600k iga kappa iga lambda igg kappa igg lambda risk stratification high standard lines of prior systemic therapies prior systemic therapies * immunomodulators ( lenalidomide , thalidomide , pomalidomide ) corticosteroids ( dexamethasone ) alkylating agents ( cyclophosphamide , melphalan , bendamustine ) proteasome inhibitors ( bortezomib , carfilzomib ) cytotoxic agents ( doxorubicin , idarubicin ) platinum agent ( cisplatin ) topoisomerase inhibitors ( etoposide ) novel antineoplastic agents ( acy - 1215 , cc - 223 ) note . 
 ( % ) unless indicated otherwise . abbreviations : ecog , eastern cooperative oncology group performance status ; ig , immunoglobulin . * on the basis of a manual review of the data . 
 testing was by snapshot ( n = 2 ) , capillary electrophoresis single - strand conformation analysis ( n = 2 ) , direct ( sanger ) sequencing ( n = 1 ) , sequenom ( n = 1 ) , single - strand conformation analysis ( n = 1 ) , 3730 dna analyzer ( n = 1 ) , and immunohistochemistry ( n = 1 )  . 
at the time of closure of the ve - basket study , the patient was still receiving treatment in the extension study . the second patient was diagnosed with smoldering mm in may 2006 and progressed to stage ii active mm in december 2009 , at which time he was treated with lenalidomide , bortezomib , and dexamethasone . 
 ( b ) change from baseline in serum m protein according to best overall response in individual patients with brafv600 mutation positive multiple myeloma treated with vemurafenib ( n = 9 )  . 
one patient with a substantial reduction in serum m protein level had an unconfirmed pr but was considered to have sd because the patient had pd at the subsequent assessment . 
 subsequent relapses were treated with cyclophosphamide , lenalidomide , and dexamethasone ( april 2013 ) ; carfilzomib , thalidomide , and dexamethasone ( august 2013 ) ; pomalidomide , bortezomib , and dexamethasone ( march 2014 ) ; and carfilzomib , pomalidomide , and dexamethasone ( august 2014 )  . 
snapshot testing of bone marrow aspirate identified an additional nras mutation at the time of relapse that had not been seen at study entry and was reported after study closure ; the original brafv600g mutation was also present at this time . one other patient , who had been treated previously with bortezomib and dexamethasone in the first line , the mammalian target of rapamycin inhibitor cc - 223 on relapse , and lenalidomide in the third line , had a vgpr after treatment with vemurafenib . 
one patient achieved an 83% reduction in serum monoclonal protein level and had a pr at one assessment but progressive disease at the next assessment , for a best overall response of sd . 
time to event details and change from baseline in serum monoclonal protein for individual patients are shown in figure 1 . at the time of study closure , disease progression was observed in six patients . 
median investigator assessed pfs was 4.63 months ( 95% ci , 2.89 months to not estimable ) ; the 6 - month pfs rate was 40% ( 95% ci , 6% to 74% ) , and the median time to progression was 4.63 months ( 95% ci , 2.89 months to not estimable )  . 
kaplan - meier plots of pfs and os are shown in the data supplement . safety the median vemurafenib dose intensity was 79% ( range , 51% to 100% )  . 
adverse events occurring in 20% of patients with brafv600 mutationpositive multiple myeloma treated with vemurafenib ( n = 9 ) any grade grade 3 or 4 event alopecia melanocytic nevus anemia hypokalemia keratosis pilaris skin papilloma sunburn acne back pain constipation diarrhea dysphonia fatigue * hyperkeratosis keratosis follicular leukoplakia oral rash papular seborrheic keratosis skin lesion xerosis upper respiratory tract infection blood alkaline phosphatase increase increased alanine aminotransferase note . 
one patient had grade 2 hypercalcemia , which was judged unrelated to vemurafenib treatment and resolved without treatment interruption , and a grade 3 chest infection , also unrelated to treatment , during which treatment was interrupted temporarily . 
the second patient had grade 4 diabetes that was judged unrelated to the study drug but resulted in dose reduction and grade 3 cellulitis that was also unrelated to treatment but required treatment interruption . 
 the final patient had treatment - related grade 4 sepsis that resolved with dose reduction and treatment - related grade 3 skin lesion and grade 2 upper respiratory infection that were not considered serious but resulted in permanent discontinuation of treatment . 
seven patients had at least one adverse event leading to dose reduction or interruption ( infections [ n = 4 ] , skin disorders [ n = 2 ] , anemia [ n = 1 ] , blood alkaline phosphatase increased [ n = 1 ] , keratosis follicular [ n = 1 ] , diabetes mellitus [ n = 1 ] , and acute kidney injury [ n = 1 ] ) ; one patient had a dose interruption for cataract surgery . qt prolongation , squamous cell carcinoma of the skin , and keratoacanthoma were not observed . 
however , identification of the brafv600 mutation as a driver mutation in mm may lead to patients with this mutation benefitting from targeted treatment with brafv600 inhibitors.1 , 7 , 20 in this study , we have shown that vemurafenib has promising efficacy in patients with brafv600 mutationpositive mm : two patients of nine had encouraging and long - lasting responses to treatment that were ongoing at the time of study closure , and an additional patient had a shorter response . 
these patients had been treated previously with bortezomib and lenalidomide , among other agents , suggesting that resistance mechanisms in those patients did not prevent response to vemurafenib . in this study , not all patients with the brafv600 mutation responded to therapy , providing us with the opportunity to study mechanisms of resistance in this patient population in the future . 
clonal evolution of mm cells and changes in the bone marrow environment have been implicated in resistance , 21 and alterations in the erk pathway are present in almost one half of patients with mm . 
interestingly , the patient in our study who relapsed after achieving a pr had acquired an nras mutation , suggesting an escape mechanism and possible resistance via this molecular pathway . 
 hyman , jean - yves blay , josep tabernero , jrgen wolf , igor puzanov , jose baselga provision of study material or patients : all authors collection and assembly of data : all authors data analysis and interpretation : noopur raje , martina makrutzki , bethany pitcher manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors mechanisms , including driver mutations within subclonal populations , may also account for differential responses . 
understanding resistance mechanisms could lead to the development of new therapies acting on the ras / raf pathway , either alone or in combination , or to the use of mek or pan - raf inhibitors . 
this subject is being addressed in an ongoing clinical trial using a braf inhibitor and a mek inhibitor ( dabrafenib and trametinib , respectively ; clinicaltrials.gov identifier : nct03091257 )  . the safety profile of vemurafenib in this patient cohort was broadly similar to that reported previously , 8 , 9 and no new safety signals were identified . 
cutaneous squamous cell carcinoma , which has been reported in vemurafenib treated patients in earlier studies , 8 , 9 was not observed in our patients . in conclusion , vemurafenib may be an appropriate and effective choice for patients with mm in whom a brafv600 mutation has been identified . 
because the ve - basket study included few patients with mm , additional studies are required to establish the role of vemurafenib , whether as monotherapy or in combination with other agents , for earlyor later - stage disease in the treatment of this poor - prognosis population . 
 ian chau honoraria : eli lilly , gilead sciences consulting or advisory role : eli lilly , bristol - myers squibb , msd , merck serono research funding : janssen - cilag ( inst ) , sanofi ( inst ) , merck serono ( inst ) , eli lilly ( inst ) travel , accommodations , expenses : msd , merck serono , sanofi , eli lilly , bristol - myers squibb martin kaiser honoraria : takeda pharmaceuticals , celgene , amgen , janssen oncology consulting or advisory role : janssen oncology , celgene , bristol - myers squibb , takeda pharmaceuticals , amgen , chugai pharmaceutical research funding : celgene travel , accommodations , expenses : takeda pharmaceuticals david m . 
yee consulting or advisory role : takeda pharmaceuticals , dexcel pharma , adaptive biotechnologies , celgene , janssen pharmaceuticals research funding : bristol - myers squibb ( inst ) , celgene ( inst ) bethany pitcher employment : f . 
hoffmann - la roche igor puzanov consulting or advisory role : amgen , roche / genentech , bristol - myers squibb travel , accommodations , expenses : amgen , merck jose baselga leadership : infinity pharmaceuticals , varian medical systems , grail , bristol - myers squibb stock or other ownership : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , varian medical systems , tango , foghorn , aura biomedical , apogen , northern biologics , bristol - myers squibb honoraria : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , northern biologics consulting or advisory role : eli lilly , novartis , grail patents , royalties , other intellectual property : combination therapy using pdk1 and pi3k inhibitors . 
hyman , heather landau , and jose baselga , memorial sloan kettering cancer center , new york ; igor puzanov , roswell park cancer institute , buffalo , ny ; vincent ribrag , jean - marie michot , and antoine hollebecque , institut gustave roussy , villejuif ; jean - yves blay , centre leonberard , lyon , france ; josep tabernero and elena elez , vall dhebron university hospital and institute of oncology , universitat autnoma de barcelona , barcelona , spain ; jrgen wolf , university hospital kln , kln , germany ; luisa veronese and martina makrutzki , f . 
hoffmann - la roche funded third - party writing and editorial support , which was provided by miller medical communications . presented in part at the 57th annual meeting of the american society of hematology , orlando , fl , december 5 - 8 , 2015 . support prior presentation references 1 . 
dimopoulos ma , swern as , li js , et al : efficacy and safety of long - term treatment with lenalidomide and dexamethasone in patients with relapsed / refractory multiple myeloma . 
kumar sk , lee jh , lahuerta jj , et al : risk of progression and survival in multiple myeloma relapsing after therapy with imids and bortezomib : a multicenter international myeloma working group study . 
walker ba , boyle em , wardell cp , et al : mutational spectrum , copy number changes , and outcome : results of a sequencing study of patients with newly diagnosed myeloma . 
mcarthur ga , chapman pb , robert c , et al : safety and efficacy of vemurafenib in braf ( v600e ) and braf ( v600k ) mutation - positive melanoma ( brim - 3 ) : extended follow - up of a phase 3 , randomised , open - label study . 
larkin j , del vecchio m , ascierto pa , et al : vemurafenib in patients with braf ( v600 ) mutated metastatic melanoma : an open - label , multicentre , safety study . 
subbiah v , gervais r , riely gj , et al : efficacy of vemurafenib in patients ( pts ) with nonsmall cell lung cancer ( nsclc ) with brafv600 mutation . 
hyman dm , kaley tj , hollebecque a , et al : vemurafenib in patients with brafv600 mutant glioma : a cohort of the histology - independent ve - basket study . 
diamond el , subbiah v , lockhart ac , et al : vemurafenib for brafv600 - mutant erdheimchester disease and langerhans cell histiocytosis : analysis of data from the histology - independent phase 2 open - label ve - basket study . 
rajkumar sv , harousseau jl , durie b , et al : consensus recommendations for the uniform reporting of clinical trials : report of the international myeloma workshop consensus panel 1 . 
kim , md , lineberger comprehensive cancer center , university of north carolina , 450 west dr , cb# 7295 , chapel hill , nc 27599 - 7295 ; e - mail : wykim@med.unc.edu. purpose urachal adenocarcinoma is a rare type of primary bladder adenocarcinoma that comprises less than 1% of all bladder cancers . 
we hypothesized that an in - depth molecular understanding of urachal adenocarcinoma would uncover rational therapeutic strategies . patients and methods we performed targeted exon sequencing and global transcriptome profiling of 12 urachal tumors to generate a comprehensive molecular portrait of urachal adenocarcinoma . 
a single patient with an msh6 mutation was treated with the antiprogrammed death - ligand 1 antibody , atezolizumab . results urachal adenocarcinoma closely resembles colorectal cancer at the level of rna expression , which extends previous observations that urachal tumors harbor genomic alterations that are found in colorectal adenocarcinoma . 
a patient with an msh6 mutation was treated with immune checkpoint blockade , which resulted in stable disease . conclusion because clinical trials are next to impossible for patients with rare tumors , precision oncology may be an important adjunct for treatment decisions . 
2017 by american society of clinical oncology introduction in the united states , bladder carcinoma is the 4th most common malignancy in men and the 9th most common in women.1 overall , an estimated 16 , 000 people died of bladder cancer in 2015 . bladder cancer takes on a spectrum of histomorphologic appearances . 
urachal carcinomas are a subtype of bladder adenocarcinoma that arises from the urachus , an embryologic remnant that connects the bladder and the allantois during fetal development.2 postnatally , fuses to become a fibrous cord known as the median umbilical ligament . 
 because of their frequent presentation at the dome of the bladder , urachal adenocarcinomas are clinically and pathologically grouped with bladder neoplasms and are typically seen by urologic oncologists and genitourinary pathologists . 
evidencebased treatment of this disease is hindered by its rarity ; thus , current treatment paradigms for urachal adenocarcinoma are primarily anecdotal in nature . as a result of the complex embryology of the allantois and cloaca , the cellular origin and molecular pathogenesis that drive the development of urachal adenocarcinoma are speculative.2 intestinal metaplasia or enteric rests are hypothesized as the histogenetic precursor of these tumors . 
although the genetics of urachal adenocarcinoma have been investigated by multiple groups , no reports on the global gene expression patterns of urachal adenocarcinoma have been published . one study selectively examined the prevalence of kras and braf mutations in high - stage urachal adenocarcinomas and , although they found no braf mutations , 42% harbored kras mutations.5 the study also noted a high rate of loss of protein expression for a number of genes that are correlated with microsatellite instability . 
a more recent study found a high rate of nf1 mutations via whole - exome sequencing of seven urachal adenocarcinomas.6 finally , another recent study showed that urachal adenocarcinomas harbor mutations in mitogen - activated protein kinase ( mapk ) pathways , similar to colorectal adenocarcinoma , and showed the potential for treatment with the antiepidermal growth factor receptor antibody cetuximab.7 herein , we report , to our knowledge , the first transcriptome analysis of urachal adenocarcinoma using whole - transcriptome profiling by rna sequencing . 
a pan - cancer transcriptomic analysis of urachal tumors comparing them with 12 cancers of different tissue origins suggest that their rna expression patterns most closely resemble colorectal adenocarcinoma and glioblastoma ( gbm )  . our work also validates reports that urachal adenocarcinomas harbor alterations that are typically found in colorectal carcinomathat is , apc , smad4 , and kras mutationbut extends those observations to show that a subset of urachal cancers has inactivation of genes that are involved in microsatellite instability ( msh2 , msh6 ) or hypermutation ( pole ) , and that all urachal tumors invariably have mutations of tp53 ( 100% )  . one patient with an msh6 mutation was treated with the antiprogrammed death - ligand 1 ( pdl1 ) antibody atezolizumab , which resulted in stable disease . 
thirteen primary urachal adenocarcinomas with formalin - fixed , paraffin - embedded ( ffpe ) tissue available at university of north carolina , chapel hill , were identified by using copath natural language search ( cerner corporation , kansas city , mo )  . 
hematoxylin and eosinstained slides and clinical history were reviewed by a board - certified pathologist ( s.e.w. ) to confirm the diagnosis on the basis of the following criteria : tumor in the dome or posterior wall of the bladder , sharp demarcation between tumor and surface epithelium , and exclusion of primary adenocarcinoma located elsewhere . 
the surgical procedure , tumor location within the bladder , histologic subtype , and tumor stage were all recorded from the accompanying pathology reports . rna expression for rna sequencing , rna was extracted from 10 - mm - thick unstained sections of ffpe blocks that were isolated from urachal tumors . 
extracted rna was converted to double - stranded cdna , and sequencing adapters were ligated by using the illumina rna access library prep protocol ( illumina , san diego , ca )  . samples were sequenced by paired - end , 100 - bp sequencing on an illumina hisequation 2000 at the high throughput sequencing core facility at the university of north carolina . 
sequence reads were aligned to the human reference transcriptome , and gene expression was generated as reads per kilobase of exon model per million mapped reads per gene by using mapsplice ( university of kentucky bioinformatics labs , lexington , ky )  . 
 clustering with the combined urachal ( sequenced urachal tumors ) and pancan ( tcga pan - cancer dataset13 ) data set was performed by using average linkage clustering with a centered correlation similarity metric with cluster 3.0 ( human genome center , tokyo , japan ) software on the top 10% most differentially expressed genes ( as determined by standard deviation ) across the combined pancan and urachal data set . 
a pearson correlation was calculated between each of the pancan tumor type centroids and each urachal tumor . clustering between the cancer genome atlas ( tcga ) bladder urothelial carcinoma ( blca ) , tcga colorectal adenocarcinoma ( coadread ) , and urachal samples was performed using average linkage clustering with a centered correlation similarity metric with cluster 3.0 software on the top 10% most differentially expressed genes after adjusting for batch effects as described above . targeted exon sequencing targeted exon sequencing was conducted through the uncseq pipeline as previously described.8 twelve of 13 urachal samples had both tumor and tumor - adjacent normal tissue submitted to the uncseq pipeline that passed quality control standards and were included in the dna analysis . 
analysis to identify significantly mutated genes , altered pathways , and clustering was confined to mutations that were classified as either having a moderate or high impact on protein function through uncseq . 
copy number alteration on a cohort level was derived by running genomic identification of significant targets in cancer ( gistic ) 2.0 on the gene pattern online platform.11 the dna mismatch repair ( mmr ) pathway was represented by the mlh1 , mlh3 , msh2 , msh3 , msh6 , and pms2 genes , with the pole gene included and separately identified . 
the insertion - to - deletion ratio was calculated by identifying the mutations that were identified as either nucleotide insertion or deletion events and dividing it by the total number of insertion and deletion events and single - nucleotide variant events ( total mutations ) in each sample . statistics a pearson correlation was performed in r between the pancan transcriptome centroids and the urachal sample expression values as detailed above . 
copy number alteration significance values were calculated using the gistic q - value metric . results urachal adenocarcinomas molecularly resemble colorectal adenocarcinoma and glioblastoma in a pan - cancer analysis thirteen urachal adenocarcinomas were identified from a search of the university of north carolina surgical pathology database ( table 1 )  . all were confirmed to be urachal adenocarcinomas on the basis of standard criteria ( patients and methods )  . 
in aggregate , these results support the notion that subsets of urachal tumors are molecularly similar to either colorectal cancer or gbm . urachal adenocarcinomas arise from an embryologic remnant of the allantois that is formed when the cloaca divides into an anterior and posterior portion . 
apc mutations were of particular interest , given it is uniquely mutated in colorectal cancers.13 although none of the mtor mutations has been previously reported , of interest , two of four of these mutations occur in the focal adhesion kinase targeting domain , where activating mutations have been previously described and shown to impart sensitivity to rapamycin.15 moreover , colorectal cancers seem to have one of the highest rate of mtor mutations across the published tcga data sets ( appendix fig a1 )  . 
 ( b ) unsupervised clustering of urachal , colorectal , and bladder mutation frequency across blca and coadread significantly mutated genes as defined by the the cancer genome atlas ( tcga )  . 
 ( c ) oncoprints of transforming growth factor ( tgf ) - b , mitogen - activated protein kinase ( mapk ) , and b - catenin pathway mutations in colorectal ( tcga ) , bladder ( tcga ) , and urachal ( uncseq ) tumors . 
 ( d ) a supervised heatmap of the frequency of tfg - b , mapk , and b - catenin pathway mutations in colorectal ( tcga ) , bladder ( tcga ) , and urachal ( uncseq ) tumors . 
 mlh1 msh2 msh6 pms2 pole 1% 1 , 000 urachal uncseq mutated mmr nonmutated mmr mutated pole colorectal uncseq bladder uncseq mutated mmr nonmutated mmr mutated pole bladder colorectal urachal bladder colorectal urachal fig 3 . 
 ( b ) supervised bar plot of the mutations / megabase ( mb ) across uncseq bladder , colorectal , and urachal samples , with samples that contain mutations in the dna mismatch repair ( mmr ) pathway indicated . ( c ) supervised bar plot of the ratio of insertions to deletions ( indel ) / mutation for uncseq bladder , colorectal , and urachal samples , with samples that contain mutations in the dna mismatch repair pathway indicated . loss , and tgfb activation by smad2 , smad3 , or smad4 mutations ( fig 2c )  . 
evaluation of a patient with urachal adenocarcinoma who was treated with atezolizumab . ( a ) spider plot of individual lesions and combined tumor burden of the atezolizumab - treated patient . 
 atezolizumab treatment results in stable disease programmed death - 1 ( pd - 1 ) blockade has resulted in significant responses in tumors with mmr deficiency.19 one of the patients whose urachal tumor was found to harbor an msh6 mutation was treated with the antipd - l1 antibody , atezolizumab . the patient received atezolizumab every 3 weeks with initial progression in target lesions ( two lung nodules and one hilar lymph node ) , followed by regression in the two lung nodules and an increase in the left hilar node associated with necrosis at second assessment ( figs 4a and 4b )  . 
grilley - olson consulting or advisory role : sanofi research funding : bayer ( inst ) , novartis ( inst ) , peregrine pharmaceuticals ( inst ) , nanocarrier ( inst ) , genentech ( inst ) , seattle genetics ( inst ) , medimmune ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) nirali m . 
weck no relationship to disclose peter black consulting or advisory role : abbvie , astellas pharma , janssen oncology , amgen , novartis , biocancell , sitka , cubist , bayer , merck , sanofi , biosyent , ferring , eli lilly , roche , spectrum pharmaceuticals , allergan speakers bureau : ferring , red leaf medical , new b innovation , iprogen patents , royalties , other intellectual property : 1 . 
milowsky research funding : mirati therapeutics ( inst ) , pfizer ( inst ) , cerulean pharma ( inst ) , merck ( inst ) , seattle genetics ( inst ) , acerta pharma ( inst ) , bioclin therapeutics ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) , x4 pharma ( inst ) , medimmune ( inst ) , incyte ( inst ) , innocrin pharma ( inst ) , inovio pharmaceuticals ( inst ) travel , accommodations , expenses : genentech d . 
neil hayes leadership : genecentric stock and other ownership interests : genecentric consulting or advisory role : genecentric patents , royalties , other intellectual property : i hold several diagnostic patents or pending patents in the area of solid tumor diagnostics william y . 
kim stock and other ownership interests : johnson & johnson , bristol - myers squibb , medivation , agios patents , royalties , other intellectual property : base47 bladder cancer subtype classifier acknowledgment we thank the members of the kim laboratory for useful discussions . 
singh h , liu y , xiao x , et al : whole exome sequencing of urachal adenocarcinoma reveals recurrent nf1 mutations . oncotarget 7 : 29211 - 29215 , 2016 7 . 
collazo - lorduy a , castillo - martin m , wang l , et al : urachal carcinoma shares genomic alterations with colorectal carcinoma and may respond to epidermal growth factor inhibition . 
zhao x , wang a , walter v , et al : combined targeted dna sequencing in non - small cell lung cancer ( nsclc ) using uncseq and ngscopy , and rna sequencing using uncqer for the detection of genetic aberrations in nsclc . plos one 10 : e0129280 , 2015 9 . 
mermel ch , schumacher se , hill b , et al : gistic2.0 facilitates sensitive and confident localization of the targets of focal somatic copy - number alteration in human cancers . 
li b , dewey cn : rsem : accurate transcript quantification from rna - seq data with or without a reference genome . bmc bioinformatics 12 : 323 , 2011 13 . 
hoadley ka , yau c , wolf dm , et al : multiplatform analysis of 12 cancer types reveals molecular classification within and across tissues of origcell 158 : 929 - 944 , 2014 14 . 
hodi fs , hwu w - j , kefford r , et al : evaluation of immune - related response criteria and recist v1.1 in patients with advanced melanoma treated with pembrolizumab . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
van allen em , miao d , schilling b , et al : genomic correlates of response to ctla - 4 blockade in metastatic jci insight 1 : e85902 , 2016 melanoma . 
verhaak rgw , hoadley ka , purdom e , et al : integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
this model combines the expression of eight genes in primary melanoma with breslow thickness and patient age to identify patients who may forgo a sentinel lymph node biopsy ( slnb ) because of their low risk of nodal metastasis . 
cp - gep can guide physicians on slnb referrals and reduce the frequency of slnb surgeries.4 the authors of both commentaries acknowledge the need for a tool to reduce the frequency of slnb procedures . 
bartlett et al1 appreciated our approach of incorporating cp variables into our model because it ensures transparency on the added value of the gep , and they nd the comparison of cp - gep and cp models appropriate . 
the authors of both commentaries reected on the evidence that supports the utility of the cp - gep model in clinical practice and elaborated on some methodologic considerations . both commentaries rightfully emphasized the need for adequately sized external validation and additional clinical utility studies before widespread clinical adoption of cp - gep . 
we agree that extensive validation in diverse patient populations and different geographical contexts is critical . for example , we recently validated the cp - gep model in a dutch retrospective patient cohort ( n = 211 ) 5 in which patient selection , surgical procedures , and pathologic assessment of slnb are signicantly different from clinical practice in the united states . 
cp - gep achieved an slnb reduction rate ( rr ) of 41% in t1 / t2 melanoma at a negative predictive value ( npv ) of 90.7%.5 additional studies are underway to elucidate cp - gep as an slnb reduction tool . 
slnb recommendations were made on the basis of individualized considerations and within the framework of institutional practice guidelines . we , in turn , derive institutional practice guidelines from established national and international guidelines . 
moreover , in terms of net benet , the cp - gep model is consistently superior to the cp model across a range of clinically reasonable risk thresholds with a more substantial gain for higher risk thresholds . varey et al2 rightfully observe that the npv is a function of the prevalence of slnb positivity in the population and , in particular , that npv decreases as the prevalence increases . 
second , the risk of metastasis to the sentinel lymph node ( sln ) ; as reected by npv and positive predictive value ( ppv ) upon taking a test is a clinically relevant metric in the process of making a decision for or against an slnb , as indicated by national comprehensive cancer network guidelines . 
furthermore , in a previous publication by mocellin et al , 9 team members thompson and scolyer themselves recommended building predictive models for sln metastasis with the aim of maximizing the npv and reducing the rate of slnb procedures through minimizing the error rate . 
in a consensus statement on the development of gep in cutaneous melanoma , grossman et al10 recently commented that gep - based tests should add to the npv of current models while minimizing false - negative predictions . bartlett et al discuss the stratication of the results by t categories . 
after consulting with dermatopathologists at mayo clinic , we concluded that the 140 excluded patients could results stratied by t category , and we hope that our data will enable physicians to critically assess the potential of cp - gep . 
knowing model performance within each t category ( as opposed to overall performance ) is likely to gain importance because the distribution of melanoma t categories is expected to change over time with more melanomas diagnosed at earlier t categories . 
we further sought to limit variability in our data by requiring slnb to be performed within 90 days of the diagnosis of primary melanoma.3 from our point of view , combining end points such as slnb status and regional recurrence can be problematic , because they occur on different time scales and vary in their methods of detection . 
the relatively high rate of patients who develop regional recurrences after negative slnb , however , highlights the need for better , more sensitive staging tools , such as the cp - gep model . 
accordingly , and to avoid missing stage iii disease , too many patients undergo invasive and costly slnb , which highlights the need for an slnb reduction tool . varey et al2 from the melanoma institute australia ( mia ) recently published a cp nomogram to predict the risk of sln metastasis.12 the mia nomogram is based on six cp variables : patient age , breslow thickness , ulceration , histologic subtype , mitotic rate , and lymphovascular invasion . in their commentary , the authors speculate that the mia nomogram outperforms the cp - gep model . 
therefore , since the mia nomogram is available online , we sought to assess the performance of the mia nomogram in our cohort.3 we found that the mia nomogram risk score could not be calculated for approximately 19% of the patients ( 143 of 754 ) in our cohort . 
of the 143 patients excluded , 140 were not suitable for the nomogram because of histologic type , and three patients were excluded because they were younger than age 18 years at biopsy . 
shown are models based on the mia nomogram , clinicopathologic variables ( cp model ) , and cp variables and a gene expression prole ( cp - gep )  . 
 correspondence not be consistently reclassied into the ve histologic types available for the mia nomograit is likely that in clinical practice , we would encounter a similar number of patients who are difcult to classify for the mia nomograit is important to note that 16.4% ( 23 ) of the 140 excluded patients showed sln metastasis . 
more data are needed to characterize our model fully , and to this end , we are currently implementing a comprehensive validation plan . domenico bellomo , phd skylinedx , rotterdam , the netherlands alina g . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . domenico bellomo employment : skylinedx stock and other ownership interests : synlogic , skylinedx patents , royalties , other intellectual property : gene signatures for predicting metastasis of melanoma tina j . 
hieken research funding : genentech ( inst ) alexander meves research funding : skylinedx ( inst ) patents , royalties , other intellectual property : mayo clinic has led several patent applications on which i am listed as an inventor . 
mulder eeap , dwarkasing jt , hollestein d , et al : validation of a clinicopathological and gene expression prole ( cp - gep ) model for sentinel lymph node metastasis in primary cutaneous melanoma . 
bioinformatics 21 : 3755 - 3762 , 2005 steyerberg ew , harrell fe jr , borsboom gj , et al : internal validation of predictive models : efciency of some procedures for logistic regression analysis . 
mocellin s , thompson jf , pasquali s , et al : sentinel node status prediction by four statistical models : results from a large bi - institutional series ( n = 1132 )  . 
mdm2 has increasing clinical relevance because inhibitors are under evaluation in clinical trials , and mdm2 amplification is a possible genomic correlate of accelerated progression , known as hyperprogression , after antipd - 1 / pd - l1 immunotherapy . 
we used next - generation sequencing ( ngs ) to ascertain mdm2 amplification status across a large number of diverse cancers . methods we interrogated the molecular profiles of 102 , 878 patients with diverse malignancies for mdm2 amplification and co - altered genes using clinical - grade ngs ( 182 to 465 genes )  . results mdm2 amplification occurred in 3.5% of patients ( 3 , 650 of 102 , 878 )  . 
an illustrative patient who harbored mdm2 amplification and experienced hyperprogression with an immune checkpoint inhibitor is presented . conclusion mdm2 amplification was found in 3.5% of 102 , 878 patients , 97.6% of whom harbored genomic co - alterations that were potentially targetable . 
the core function of mdm2 is to inhibit the tumor suppressor p53 , which is critical for regulating genes involved in dna repair , cell cycle , senescence , and apoptosis . 
when amplified , mdm2 facilitates proteasomal degradation of p53 , which promotes tumorigenesis.1 - 3 mdm2 amplification has been reported in multiple tumor types4 - 6 and is a hallmark of tumorigenesis.3 in certain tumor types , such as glioblastoma and well differentiated liposarcoma , mdm2 amplification and tp53 alterations are mutually exclusive , 4 , 5 which is consistent with the inhibitory function of mdm2 . 
however , in other tumors ( eg , osteosarcoma , esophageal cancer ) , mdm2 amplification and tp53 alterations co - occur.5 , 6 preclinical studies have suggested noncanonical p53 - independent roles for mdm2 . 
 for instance , an in vitro study that used an mdm2 - overexpressed / tp53 wild - type cancer cell line revealed a potential role for mdm2 in suppressing senescence in a tp53 - independent fashion.7 moreover , mdm2 - amplified / tp53null mice have a higher incidence of spontaneous tumorigenesis than tp53 - null mice shumei kato jeffrey s . 
 ( without mdm2 amplification ) .8 among several potential noncanonical roles for mdm2 , a functional angiogenesis effect has been proposed.9 indeed , a preclinical study showed that under hypoxic conditions , mdm2 - overexpressed / tp53 - null cancer cells produce vascular endothelial growth factor ( vegf ) mrna at higher levels than mdm2 - negative / tp53 - null cells . 
 hypoxia induces translocation of mdm2 from the nucleus to the cytoplasm , and subsequent binding of the mdm2 c - terminal domain to the 3untranslated region of vegf mrna increases mrna stability and translation.10 in addition , suppression of mdm2 activity with a small - molecule inhibitor leads to decreased hypoxia - inducible factor 1 and vegf expression , which support a role for mdm2 in angiogenesis.11 tp53 mutations also lead to increased vegf - a expression12 , 13 and have been associated with increased responsiveness to vegf / vegf receptor inhibitor therapy.14 - 16 taken together , these data suggest that mdm2 promotes angiogenesis through either inhibition of p53 or mechanisms independent of p53 . an understanding of mdm2 amplification status has clinical relevance for patients with cancer because mdm2 inhibitors are in early phase clinical development ( data supplemental )  . 
although preliminary results demonstrated no responses to mdm2 inhibitors among unselected patients , 17 - 19 responses occurred in wildtype tp53 liposarcoma ( mk - 8242 ; response rate [ rr ] , 11.1% [ three of 27 patients ] ) or melanoma ( amg232 ; rr , 28.6% [ six of 21 patients ] ) .20 , 21 mdm2 amplification also has been implicated as a potential marker for accelerated tumor growth with receipt of immune checkpoint inhibitors.22 this phenomenon is called hyperprogression and affects approximately 9% of patients who receive pd - 1 / pd - l1 inhibitors.23 hyperprogression has been defined as a time to treatment failure < 2 months from checkpoint inhibitor initiation , a > 50% increase in tumor burden compared with pre - immunotherapy imaging , and a more than two - fold increase in progression pace.22 to date , accelerated progression after antipd - 1 / pd - l1 agents has been reported by at least four groups.22 - 25 although the mechanisms that mediate this phenomenon remain unclear , we and others have demonstrated that mdm2 family gene amplifications and egfr alterations correlate with hyperprogression.22 , 25 given the clinical importance of mdm2 , we describe the landscape of cancer types that harbor mdm2 amplification and evaluate the comprehensive genomic profiles of 102 , 878 tumors from patients with malignancies . 
an illustrative patient with mdm2 amplification that demonstrated hyperprogression after checkpoint blockade is presented . methods patients we explored the mdm2 amplification status of patients with diverse malignances who were referred for comprehensive next - generation sequencing ( ngs ) from june 2012 through december 2016 ( n = 102 , 878 ; table 1 ; data supplement )  . 
this study was performed in accordance with the guidelines of the university of california , san diego , institutional review board with regard to analysis and consent . tissue samples and mutational analysis tumors were provided as formalin - fixed , paraffin embedded samples and evaluated by ngs in a clinical laboratory improvement amendments certified laboratory ( foundation medicine , cambridge , ma )  . 
the methods used for ngs have been validated and previously reported.26 - 29 dna was adaptor ligated , and hybrid capture was performed for all coding exons of 182 to 465 cancer - related genes plus select introns from 14 to 31 genes frequently rearranged in cancer ( data supplement )  . 
the median number of potentially targetable genomic co - alterations with either food and drug administrationapproved or investigational agents was three ( range , zero to 17 )  . analyses except those for tumor mutation burden ( tmb )  . cancer genomic data through publicly available data sets tmb was calculated on the basis of the total number of mutations counted per megabase.30 noncoding alterations , alterations reported as known somatic alterations in catalog of somatic mutations in cancer , truncations in tumor suppressor genes , and alterations predicted to be germline were not counted . 
high tmb was defined as 20 mutations / megabase . mdm2 amplification status was also curated from the genomics evidence neoplasia information exchange ( genie ) accessed in july 2017.31 - 33 end points , statistical methods , and case study descriptive statistics were used to summarize the cancer diagnoses and genomic alterations identified in the data set . 
comparison of rate of mdm2 amplification in the current report ( n = 102 , 878 samples ) versus in genomics evidence neoplasia information exchange ( genie ; n = 13 , 473 samples ) .31 data from genie were obtained as previously described.31 the 10 most common diagnoses that harbor mdm2 amplification from the current report were selected for the comparison . 
mdm2 amplifications were seen in 3.5% ( 3 , 650 of 102 , 878 ) of patients in the current report versus 5.5% ( 744 of 13 , 473 ) from genie . 
mdm2 amplification was most commonly seen among liposarcoma ( 63.6% [ 332 of 522 ] ) followed by gallbladder , adenocarcinoma ( 11.1% [ 62 of 554 ] ) ; sarcoma , not otherwise specified ( 10.7% [ 103 of 955 ] ) ; and urothelial carcinoma ( 10.4% [ 198 of 1 , 898 ] ; table 1 )  . 
 mdm2 amplification was not found among anaplastic and papillary carcinoma of thyroid ( zero of 166 and 376 , respectively ) and uncommonly among adenocarcinoma of the appendix , rectum , and colon ( 0.23% [ one of 440 ] , 0.28% [ four of 1 , 448 ] , and 0.33% [ 28 of 8 , 562 ] , respectively ; data supplement )  . 
in comparison , according to the genie database ( total , 13 , 473 samples ) , mdm2 amplification has been reported in 5.5% genomic co - alterations associated with mdm2 amplification among 3 , 650 patients with mdm2 amplification , 99.0% ( 3 , 613 ) were found to have genomic co - alterations ( data supplement )  . 
although uncommon , mismatch repair genes and pd - l1 amplification were co - altered in 2.2% ( 79 of 3 , 650 ) of patients ( table 2 )  . among patients with mdm2 amplification ( n = 3 , 650 ) , tp53 was co - altered in 733 . 
these differences in patient subsets were not seen in the genie data set perhaps because genie had considerably fewer patients ( approximately 13% of the patients in our data set )  . we have previously reported that mdm2 amplification can be associated with hyperprogression after treatment with antipd - 1 / pd - l1 agents.22 we describe herein a 36 - year - old woman ( not previously reported ) with adenocarcinoma of the gastro - esophageal junction who had stable disease ( sd ) while receiving second - line therapy with fluorouracil , oxaliplatin , and panitumumab ( fig 3 , left and middle )  . 
 the patient had rapid progression in the mediastinal and retroperitoneal lymph nodes as well as emergent massive ascites ( time to treatment failure , 3 weeks ; pace of progression increased by 6.4 - fold compared with the 4 months before the start of checkpoint blockade , and tumor burden increased 460% compared with pre immunotherapy imaging ; fig 3 )  . 
molecular profiling of the primary tumor revealed alterations , including amplifications in mdm2 , erbb3 , araf , cdk4 , and egfr and alterations in pik3ca , frs2 , gli1 , and ikzf1 . 
pd - 1 and pd - l1 immunohistochemistry was not evaluated . discussion we and others recently demonstrated that approximately 9% of patients treated with pd - 1 / pd - l1 checkpoint blockade exhibit a paradoxical acceleration in tumor progression ( designated as hyperprogression )  . 
this phenomenon associates with mdm2 amplification.22 - 24 therefore , caution is needed in treating patients who harbor mdm2 amplification with checkpoint inhibitors , and a thorough understanding of the mdm2 alteration landscape is clinically important . 
selected co - alterations that accompany mdm2 amplification and potential targeted therapies ( continued ) co - alteration examples of potential targeted therapies * tp53 - associated genes mismatch repair genes and pd - l1 amplification cd274 ( pd - l1 ) cdk4 cdk6 ccne1 tp53 mdm4 mlh1 msh2 msh6 pms2 no . 
mdm2 amplification most commonly has been seen in patients with liposarcoma ( 63.6% [ 332 of 522 ] ) 5 but discerned in a subset of most tumor types , albeit at different frequencies ( table 1 ; data supplement )  . 
certain diagnoses ( eg , anaplastic and papillary thyroid cancer ) were not associated with mdm2 amplification , and this anomaly was rare in acute myelocytic leukemia ( one of 1 , 006 patients ; data supplement )  . an understanding of the comprehensive landscape of mdm2 amplification also is therapeutically relevant because mdm2 inhibitors are in clinical development ( data supplement )  . 
clinical activity of mdm2 inhibitors among unselected diverse cancers has been limited17 - 19 ; however , occasional responses have been observed in individuals selected for wild - type tp53.20 , 21 the low response rate with single - agent mdm2 inhibitors may be due to the lack of patient selection for mdm2 amplification or to co - altered genes ( data supplement )  . 
accumulating evidence has suggested that the matched targeted therapy approach can demonstrate better clinical outcomes than a nonmatched approach , but this implies the need to select patients for the relevant aberration.34 - 37 wagner et al21 showed that responses with mk - 8242 ( mdm2 inhibitor ) were exclusively observed in patients with liposarcoma ( rr , 11.1% [ three or 27 ] ) whose molecular hallmark includes mdm2 amplification5 ( nonliposarcoma ; rr , 0% [ zero of 14 ] )  . 
on the other hand , even in a disease such as liposarcoma where > 60% of patients have mdm2 amplification , the rr is relatively low , which may be due to , as mentioned previously , the presence of co - alterations . 
indeed , the 12q13 - 15 amplicon on which mdm2 resides is large ( but discontinuous ) ; cdk4 and frs2 reside on the amplicon and frequently are co - amplified with mdm238 but are rarely abnormal in patients without mdm2 amplification ( data supplement )  . in keeping with the notion that co - alterations are important , we also assessed the alterations that co - occurred with mdm2 amplification . 
 the majority of mdm2 - amplified tumors harbored co - alterations ( 99% [ 3 , 613 of 3 , 650 ] ) ; the median number of alterations per patient was six ( range , one to 25 ; data supplement )  . 
among patients with mdm2 amplification ( n = 3 , 650 ) , 2.9% ( 105 ) had high tmb , 23.3% ( 852 ) had intermediate tmb , and 73.8% ( 2 , 693 ) had low tmb . 
in the current data set , certain cancers with mdm2 amplification were significantly less associated with high tmb than with mdm2 wild type ( sarcoma , not otherwise specified , 0% [ zero of 103 ] v 4.2% [ 36 of 852 ] , respectively [ p = .03 ] ; urothelial carcinoma , 3.5% [ seven of 198 ] v 11.8% [ 200 of 1 , 700 ] , respectively [ p < .001 ] ; glioblastoma , 0.4% [ one of 244 ] v 4.4% [ 120 of 2 , 725 ] , respectively [ p < .001 ] ) ; these subsets did not show significant differences in genie , but the number of patient samples in genie was considerably smaller ( data supplement )  . 
because frs2 and cdk4 are on the mdm2 amplicon , the targeting of them may warrant specific study . of note , we also observed that tp53 alterations were not mutually exclusive with mdm2 amplification , as previously reported.5 , 6 although tp53 alterations were less commonly seen in patients with mdm2 amplification compared with wild type ( data supplement ) , tp53 alterations were observed in 20.1% ( 733 of 3 , 650 ; fig 2 ; data supplement )  . 
one of the proposed noncanonical roles of mdm2 is to facilitate angiogenesis.39 zhou et al10 reported that mdm2 - overexpressed / tp53 - null cancer cells are associated with increased vegf mrna expression compared with mdm2 negative / tp53 - null cells . 
within 3 weeks , the patient showed marked clinical deterioration , and imaging showed rapid progression in mediastinal and retroperitoneal lymph nodes as well as emerging massive ascites ( right )  . 
pace of progression increased by 6.4 - fold , tumor burden increased by 460% compared with pre - immunotherapy imaging , and time to treatment failure was 3 weeks ( hyperprogression after immunotherapy previously defined as more than a two - fold increase in progression pace , a > 50% increase in tumor burden compared with pre - immunotherapy imaging , and a time to treatment failure < 2 months22 )  . 
the most common co - alterations associated with mdm2 amplification were cdk4 ( 43.6% [ 1 , 591 of 3 , 650 ] ) , frs2 ( 40.8% [ 1 , 491 of 3 , 650 ] ) , tp53 ( 20.1% [ 733 of 3 , 650 ] ) , cdkn2a ( 18.2% [ 665 of 3 , 650 ] ) , and egfr ( 12.7% [ 462 of 3 , 650 ] ; data supplement )  . cdk4 frs2 tp53 cdkn2a egfr ccnd1 cdkn2b kras fgf19 gli1 fgf4 pik3ca fgf3 tert fgfr1 pten erbb3 znf217 znf703 gnas arid1a erbb2 nkx2 - 1 frequency of mdm2 amplification ( % ) amplification mutation deletion fusion / rearrangement multiple alterations tmb . 
in the current study , we depict an individual with gastric cancer that harbored egfr as well as mdm2 amplification who had indolent disease ; the patient , however , showed explosive progression after being given the antipd - 1 inhibitor nivolumab ( fig 4 )  . 
whether patients who have both pd - l1 amplification ( a marker of sensitivity to checkpoint inhibitors in hodgkin disease43 ) and mdm2 amplification would respond to checkpoint blockade is unclear . 
because high tmb correlates with checkpoint blockade responsiveness , 44 , 45 this observation may partially explain resistance to pd - 1 / pd - l1 inhibitors in mdm2 - amplified tumors but does not clarify the mechanism that underlies the correlation between mdm2 amplification and hyperprogression . 
furthermore , how patients whose tumors have high tmb as well as mdm2 amplification would fare on checkpoint inhibitors is unclear ; however , one of our previously reported patients with mdm2 amplification who demonstrated hyperprogression with antipd - l1 immunotherapy had a high tmb.22 finally , an issue that merits prospective exploration is how a combination of mdm2 and checkpoint inhibitors would affect the risk of hyperprogression in patients whose cancers bear an mdm2 amplification . the current study has several limitations . 
first , the data set was de - identified , which limited the analyzable correlates ; thus , clinical questions such as the frequencies of mdm2 amplification that depend on the disease state ( early stage v metastatic and recurrent disease ) could not be evaluated . 
second , because the number of patients in each cancer type was based on the number of samples sent for ngs by the treating physicians , sample size bias is possible . 
despite these limitations , the current study provides , to our knowledge , the largest and most comprehensive analysis of mdm2 amplification in diverse malignancies to date . in summary , we have interrogated 102 , 878 patients with diverse cancers and demonstrated that amplification of mdm2 is found in 3.5% ( 3 , 650 ) of tumors . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . shumei kato no relationship to disclose jeffrey s . 
ito m , barys l , oreilly t , et al : comprehensive mapping of p53 pathway alterations reveals an apparent role for both snp309 and mdm2 amplification in sarcomagenesis . 
shibagaki i , tanaka h , shimada y , et al : p53 mutation , murine double minute 2 amplification , and human papillomavirus infection are frequently involved but not associated with each other in esophageal squamous cell carcinoma . 
kovatcheva m , liu dd , dickson ma , et al : mdm2 turnover and expression of atrx determine the choice between quiescence and senescence in response to cdk4 inhibition . 
lakoma a , barbieri e , agarwal s , et al : the mdm2 small - molecule inhibitor rg7388 leads to potent tumor inhibition in p53 wild - type neuroblastoma . 
schwaederl m , lazar v , validire p , et al : vegf - a expression correlates with tp53 mutations in non - small cell lung cancer : implications for antiangiogenesis therapy . 
said r , hong ds , warneke cl , et al : p53 mutations in advanced cancers : clinical characteristics , outcomes , and correlation between progression - free survival and bevacizumab - containing therapy . 
de jonge m , de weger va , dickson ma , et al : a phase i study of sar405838 , a novel human double minute 2 ( hdm2 ) antagonist , in patients with solid tumours . 
gounder mm , bauer tm , schwartz gk , et al : a phase 1 study of the mdm2 inhibitor ds - 3032b in patients ( pts ) with advanced solid tumors and lymphomas . 
kurzrock r , blay j - y , bui nguyen b , et al : a phase i study of mdm2 antagonist rg7112 in patients ( pts ) with relapsed / refractory solid tumors . 
moschos sj , sandhu sk , lewis kd , et al : phase 1 study of the p53 - mdm2 inhibitor amg 232 combined with trametinib plus dabrafenib or trametinib in patients ( pts ) with tp53 wild type ( tp53wt ) metastatic cutaneous melanoma ( mcm )  . 
wagner aj , banerji u , mahipal a , et al : phase i trial of the human double minute 2 inhibitor mk - 8242 in patients with advanced solid tumors . 
champiat s , dercle l , ammari s , et al : hyperprogressive disease is a new pattern of progression in cancer patients treated by anti - pd - 1 / pd - l1 . 
sada - bouzid e , defaucheux c , karabajakian a , et al : hyperprogression during anti - pd - 1 / pdl1 therapy in patients with recurrent and / or metastatic head and neck squamous cell carcinoma . 
singavi ak , menon s , kilari d , et al : predictive biomarkers for hyper - progression ( hp ) in response to immune checkpoint inhibitors ( ici ) analysis of somatic alterations ( sas )  . 
wagle n , berger mf , davis mj , et al : high - throughput detection of actionable genomic alterations in clinical tumor samples by targeted , massively parallel sequencing . 
roszik j , haydu le , hess kr , et al : novel algorithmic approach predicts tumor mutation load and correlates with immunotherapy clinical outcomes using a defined gene mutation set . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
mejia - guerrero s , quejada m , gokgoz n , et al : characterization of the 12q15 mdm2 and 12q13 - 14 cdk4 amplicons and clinical correlations in osteosarcoma . 
 computed tomographyderived radiomic metrics can identify responders to immunotherapy in ovarian cancer yuki himoto , md , phd1 , 2 ; harini veeraraghavan , phd1 ; junting zheng , ms1 ; dmitriy zamarin , md , phd1 , 3 ; alexandra snyder , md1 , 3 , 4 ; marinela capanu , phd1 ; stephanie nougaret , md , phd1 , 5 , 6 , 7 , 8 ; hebert a . 
disease burden ( total tumor volume , number of disease sites ) , radiomic measures of intertumor heterogeneity ( clustersite entropy , cluster - site dissimilarity ) , and intratumor heterogeneity of the largest lesion ( haralick texture features ) were computed . 
2019 by american society of clinical oncology introduction ( oc ) ovarian cancer is the deadliest gynecologic malignancy.1 , 2 most patients respond to cytoreductive surgery and platinum - based chemotherapy but eventually experience recurrence and develop chemotherapyresistant disease.3 poor outcomes relate to the loss in dna repair mechanisms , resulting in highly heterogeneous tumors that exhibit early clonal evolution and rapid onset of chemotherapy resistance.3 - 6 immunotherapy is a novel treatment paradigm that has emerged with improved understanding of the cancerimmunity cycle.7 immune checkpoint inhibitors are effective in multiple solid tumors . 
in ovarian cancer , early multiregion dissemination and profound tumor heterogeneity ( th ) limit the discovery of predictive biomarkers on the basis of the tissue samples from few individual tumors . 
we aimed to explore the potential of quantitative analysis of standard - of - care computed tomography ( ct ) to noninvasively capture spatial th and predict response to immunotherapy . knowledge generated quantitative analysis of pretreatment ct including radiomic measures of th may facilitate the delivery of precision medicine by identifying patients who derive most benet from immunotherapy . 
indeed , fewer disease sites and lower image - based intrath were two independent indicators of durable clinical benet ; higher inter - th was a single independent indicator of shorter time to off - treatment . relevance number of disease sites and radiomic measures of th derived from baseline ct are potential noninvasive predictive imaging biomarkers of response that require additional exploration in the context of multimodal approaches to ovarian cancer . medical decisions , including the selection of patients appropriate for treatment with chemoimmunotherapy . in patients with oc , contrast - enhanced computed tois the standard - of - care imaging to mography ( ce - ct ) evaluate disease extent at all phases of patient management , including initial diagnosis , post - treatment surveillance , disease recurrence , and assessment of response . although the response evaluation criteria in solid tumors ( recist ) version 1.1 and immune - related response criteria are applied to assess response to immunotherapies , there is a paucity of predictive biomarkers of response to chemotherapy , targeted therapy , and immunotherapy to facilitate the selection of rational individualized combination therapies.17 - 19 the potential of radiomics to model intraand inter - th on imaging to predict the response of oc to immunotherapy is an unexplored area . 
progression was dened as clinical deterioration and / or imaging progression according to immune - related recist.19 time to off - treatment was dened as the number of days between the rst treatment date and the off - study date . 
durable clinical benet was dened as progression - free survival of 24 or more weeks.20 - 22 ct analysis baseline ce - ct acquisition parameters , segmentation of the entire tumor burden , and computation of volumes of interest ( vois ) are described in the appendix . 
all locations were mutually exclusive . extraction of radiomic measures from baseline ct scans texture features were extracted directly from ct images without additional preprocessing to avoid imaging blur and spurious features . 
five intra - th measures ( haralick texture features ) derived from the lesion with the largest volume and two inter - th measures ( cluster - site entropy , clustersite dissimilarity ) were computed following the steps described here ( fig 1 ) .23 step 1 : per - voxel haralick texture features . 
of disease sites , locations with disease , total tumor volume intratumor heterogeneity computed from the lesion with the largest volume contrast correlation energy entropy homogeneity intertumor heterogeneity cluster - site entropy cluster - site dissimilarity clinical variables histology figo stage cytoreductive outcome platinum sensitivity status prior lines of chemotherapy fig 1 . 
the above per - voxel haralick texture measures were then used to compute intra - th measures ( step 2 ) and inter - th measures ( step 3 )  . step 2 : intratumor heterogeneity measures . 
we chose the lesion with the largest volume on the basis of the results of prior radiomic studies.26 , 27 intra - th measures were summarized as the mean of all per - voxel haralick texture features within voilargest - lesion . 
first , per - voxel haralick textures within all segmented tumors were clustered together to produce subregions within all lesions using the kernel k - means clustering method , where each subregion represents a group of voxels with highly similar texture values . 
we then described each subregion by the mean of all per - voxel haralick texture values within that subregion . second , pairwise subregion dissimilarities were computed as the euclidean distance between the subregion pairs , where each subregion was represented by the mean textural values inside that subregion . 
a highly textured dissimilarity map points to greater frequency of dissimilarities between subregions , whereas more a homogeneous map suggests less frequent dissimilarities between subregions . third , a group dissimilarity matrix was computed from the dissimilarity map for each patient . 
group dissimilarity matrix is a two - dimensional histogram that captures the frequency of dissimilarities between subregions and the number of neighboring dissimilar subregions . cluster - site entropy ( cse ) was computed directly from the all subregion pair dissimilarities . 
it captures the variability in dissimilarities between subregions and is calculated using the shannon entropy formula : cse ( cid : 3 ) 1 ( cid : 1 ) n n ( cid : 3 ) 1 ( cid : 1 ) ( cid : 3 ) log2 ( p ( dn ) ) , where n is the number of subregion pairs . cluster - site dissimilarity ( cludiss ) was derived from the group dissimilarity matrix . 
a sensitivity analysis was performed using crossvalidated least absolute shrinkage and selection operator ( lasso ) regression including all variables with 200 random repetitions.29 the variables in nal multivariable models were also selected more than 90% of the time by lasso regression . 
model discriminability was assessed with the receiver operating characteristic analysis and internally validated concordance statistics ( c - index ) .30 in multivariable logistic regression , bias - correct c - index was estimated using the bootstrapping technique . 
the r code used in the analysis is available for download through com / harveerar / jco - po - ovaryimmunotherapy . the correlations between the measures signicant at multivariable analyses ( number of disease sites , intra - th [ energylargest - lesion ] and inter - th [ cluster - site dissimilarity ] ) were tested with spearman correlation coefcient ( rs )  . 
 ( % ) unless otherwise noted . abbreviations : ce - ct , contrast - enhanced computed tomography ; figo , international federation of gynecology and obstetrics ; ln , abdominopelvic lymphadenopathy ; pd , peritoneal disease ; sd , standard deviation . results patients patient clinical characteristics are listed in table 1 . 
axial baseline computed tomography ( ct ) images from two different patients with energy ( a measure of intratumor heterogeneity ) overlaid on segmented tumors ( arrow points to the largest lesion )  . 
two box plots illustrate the univariable associations of baseline ct - derived number of disease sites and energylargest - lesion ( a measure of intratumor heterogeneity ) with durable clinical benet ( progression - free survival 24 weeks )  . 
ideally , these biomarkers should be based on noninvasive or minimally invasive approaches to capture / sample th and enable individualized treatment decisions in oc . our study highlights a novel noninvasive method to model spatial th via radiomic analysis of ct and demonstrates that quantitative image - based measures relate to clinical outcomesspecically , the prediction of response to immunotherapy . 
we found that fewer disease sites and lower intra - th of the largest lesion ( higher energylargest - lesion ) were the only indicators of durable clinical benet at multivariable analysis . 
combined fewer disease sites and lower intra - th ( higher energylargest - lesion ) were a composite indicator of durable clinical benet , with a c - index of 0.821. notably , none of the patients with more than seven disease sites experienced durable clinical benet . 
higher inter - th ( higher cluster - site dissimilarity ) was the only indicator of shorter time to off - treatment at multivariable analysis . clinical variables , ttv , and locations of disease on ce - ct were not predictive of response . 
plots of receiver operating characteristic curves demonstrating the discriminatory ability of the model to identify patients with durable clinical benet on the basis of number of disease sites , energylargest lesion , or both . delivery of precision medicine to patients with oc by identifying patients who may benet from immunotherapy . likely require additional immunotherapy has transformed the treatment of several solid and hematologic malignancies , but the efcacy varies across tumor types and patients.10 oc exhibits poor response to immune checkpoint inhibitors , with the biomarkers of response and resistance remaining unexplored . effective implementation will renement of sights into cancer - immune interactions , immune - response criteria , and development of multifactorial predictive biomarkers ( eg , cancer immunogram ) to personalize the selection of immunotherapy.32 , 33 at present , predictive biomarkers of response to immunotherapy include pd - 1 expression , tumor mutational / neoantigen burden assessment , tumor - inltrating lymphocyte evaluation , and immune gene expression assays.34 nevertheless , composite multimodal multifaceted biomarkers that noninvasively capture spatiotemporal th will likely be necessary to comprehensively assess immune tme and serve as clinical decision support for prognosis inference and prediction of response . th is an important element to consider and quantify in any oc cancer immunogram , because lower th has been associated with improved prognosis and better response to chemotherapy and immunotherapy.5 , 11 , 12 two recent articles highlight the importance of spatial th for accurate characterization of immune tme in oc . 
the major nding was that the immune tme varied in space and potentially shaped clonal selection in patients with newly diagnosed hgsoc . ce - ct is the standard - of - care imaging approach that is widely used for the evaluation of patients with oc . 
although baseline ce - ctderived predictive biomarkers of response to immunotherapy would be useful as clinical decision support tools , the interplay of radiomic measures with clinical outcomes in oc remains largely unexplored . 
few studies to date have evaluated the role of radiomics to model spatial th and capture immune tme.33 , 35 vargas et al35 proposed a novel method to compute interth on ce - ct and found higher inter - th to associate with shorter overall survival and greater risk of incomplete surgical resection in 38 patients with newly diagnosed advanced - stage hgsoc . 
in contrast to the approach used by vargas et al , 35 we computed inter - th between lesions rather than anatomic sites of disease for more comprehensive assessment of th . 
similar to vargas et al , 35 we demonstrated that higher inter - th measured on the baseline ce - ct was associated with worse outcomes , as indicated by shorter time to offtreatment . although the assessment of image - based inter - th is a promising approach , at present , the translation to routine trials is limited by laborclinical practice and clinical intensive multiregion tumor segmentation and complex computational analysis across multiple tumors . 
in the future , deep learning techniques may enable accurate semiautomated tumor delineation reducing manual effort . in the meantime , we also examined the value of such readily accessible quantitative measures as number of disease sites , ttv , and intra - th of lesion measured from the baseline ce - ct . 
we found fewer disease sites and lower intra - th of the largest lesion ( indicated by higher energylargest - lesion ) to be signicant indicators of durable clinical benet at multivariable analysis . 
this nding is potentially explained by a positive relationship between the number of disease sites and inter - th ( rs , 0.842 ) , with more disease sites increasing the probability of inter - th and reducing the likelihood of durable clinical benet . 
our study suggests that the number of disease sites is a measure that deserves additional investigation and potentially indirectly reects spatial th in oc . ttv on baseline ce - ct was not predictive of response to immunotherapy in our cohort . 
recognizing the substantial limitation of this measure in assessing tumor burden , peritoneal bulky disease was not predictive of chemotherapy response.36 , 37 the role of tumor volume / burden as a prognostic measure and a predictor of benet from immunotherapy requires additional investigation . 
in contrast , sun et al33 reported that tumor volume was not predictive of overall survival in patients with various cancer types treated with antipd - 1 and antipdl1 immunotherapy . only one prior study examined the interplay between radiomic analysis , effector t cells , tumor immune phenotypes , and response to immunotherapy.33 in this study , sun et al33 developed a ce - ctderived radiomic signature of cd8 cells by segmenting and extracting image - based features from either biopsied or largest lesion in patients with one of ve advanced solid malignant tumors . 
they then proceeded to validate their radiomic signature of cd8 cells in two independent cohorts and demonstrate the associations of radiomic signature of cd8 cells with tumor immune phenotype and response to immunotherapy , respectively . 
second , given the hypothesisgenerating nature of our study , a single experienced radiologist segmented all tumor on each baseline scan . automated or semi - automated methods to segment oc implants are currently absent . 
third , a small set of wellestablished image features ( ie , haralick textures ) were extracted because of the relatively small sample size and focus on image - based inter - th , a measure computed on the basis of haralick features.35 larger numbers of features , including new features ( eg , co - occurence of local anisotropic gradient orientations [ coliage ] ) , should be explored further , but require a large data set ( independent training and validation cohorts ) to reliably estimate the models performance . this will in conclusion , the number of disease sites and radiomic measures of th from baseline ce - ct are potential predictive imaging biomarkers of responsiveness to immunotherapy . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . dmitriy zamarin employment : acorda therapeutics ( i ) consulting or advisory role : biomed valley discoveries , merck , psioxus therapeutics , synlogic , western oncolytics , tesaro , agenus , trieza therapeutics , acm biolabs research funding : merck patents , royalties , other intellectual property : i hold a patent regarding the use of recombinant newcastle disease virus ( ndv ) for cancer therapy ( inst ) travel , accommodations , expenses : roche alexandra snyder employment : adaptive biotechnologies , merck stock and other ownership interests : merck consulting or advisory role : driver group research funding : bristol - myers squibb travel , accommodations , expenses : genentech , bristol - myers squibb margaret callahan employment : bristol - myers squibb ( i ) , celgene ( i ) , kleo pharmaceuticals ( i ) , bristol - myers squibb ( i ) consulting or advisory role : astrazeneca , moderna therapeutics , merck research funding : bristol - myers squibb ( inst ) other relationship : clinical care options , potomac center for medical education evis sala honoraria : siemens healthineers speakers bureau : siemens healthineers travel , accommodations , expenses : siemens healthineers yulia lakhman stock and other ownership interests : y - mabs therapeutics no other potential conicts of interest were reported . acknowledgment we thank joanne chin , mfa , els , for her editorial assistance with this manuscript . references torre la , trabert b , desantis ce , et al : ovarian cancer statistics , 2018 . 
nature 474 : 609 - 615 , 2011 [ erratum : nature 490 : 298 , 2012 ] schwarz rf , ng ck , cooke sl , et al : spatial and temporal heterogeneity in high - grade serous ovarian cancer : a phylogenetic analysis . 
plos med 12 : e1001789 , 2015 bashashati a , ha g , tone a , et al : distinct evolutionary trajectories of primary high - grade serous ovarian cancers revealed through spatial mutational proling . j pathol 231 : 21 - 34 , 2013 chen ds , mellman i : elements of cancer immunity and the cancer - immune set point . 
science 359 : 1350 - 1355 , 2018 jim enez - s anchez a , memon d , pourpe s , et al : heterogeneous tumor - immune microenvironments among differentially growing metastases in an ovarian cancer patient . 
shukuya t , mori k , amann jm , et al : relationship between overall survival and response or progression - free survival in advanced non - small cell lung cancer patients treated with anti - pd - 1 / pd - l1 antibodies . 
yoo ts , ackerman mj , lorensen we , et al : engineering and algorithm design for an image processing api : a technical report on itk - - the insight toolkit . 
rao sx , lambregts dm , schnerr rs , et al : ct texture analysis in colorectal liver metastases : a better way than size and volume measurements to assess response to chemotherapy ? united european gastroenterol j 4 : 257 - 263 , 2016 27 . 
lubner mg , stabo n , lubner sj , et al : ct textural analysis of hepatic metastatic colorectal cancer : pre - treatment tumor heterogeneity correlates with pathology and clinical outcomes . 
apte ap , iyer a , crispin - ortuzar m , et al : technical note : extension of cerr for computational radiomics : a comprehensive matlab platform for reproducible radiomics research . 
sun r , limkin ej , vakalopoulou m , et al : a radiomics approach to assess tumour - inltrating cd8 cells and response to anti - pd - 1 or anti - pd - l1 immunotherapy : an imaging biomarker , retrospective multicohort study . 
vargas ha , veeraraghavan h , micco m , et al : a novel representation of inter - site tumour heterogeneity from pre - treatment computed tomography textures classies ovarian cancers by clinical outcome . 
gordon an , tonda m , sun s , et al : long - term survival advantage for women treated with pegylated liposomal doxorubicin compared with topotecan in a phase 3 randomized study of recurrent and refractory epithelial ovarian cancer . 
gynecol oncol 95 : 1 - 8 , 2004 joseph rw , elassaiss - schaap j , kefford r , et al : baseline tumor size is an independent prognostic factor for overall survival in patients with melanoma treated with pembrolizumab . 
all baseline contrast - enhanced computed tomography scans ( ce - cts ) were acquired using multidetector ct scanners with 16 to 256 rows of detectors ( ge healthcare , chicago , il )  . 
five of 75 scans were performed at outside institutions and digitized into the institutional picture archiving and communication system ( centricity pacs ; ge healthcare , chicago , il )  . 
using the insight segmentation and registration toolkitsnap version 3.4 software , the radiologist traced the outer contour of each lesion on every axial slice with tumor ( yushkevich , et al : neuroimage 31 : 1116 - 1128 , 2006 )  . 
regions of interest ( rois ) belonging to the same lesion ( roilesion ) and originating from the set of contiguous craniocaudal images in the same anatomic location were summed to create the volume of interest for that lesion ( voilesion )  . 
volumes of interest for lesions with noncontiguous rois were obtained by summing the volumes of various groups of contiguous rois in the same ( cid : 3 ) ( cid : 1 ) n ( cid : 3 ) 1 anatomic location as follows : voitotal lesion voin lesion , where n is the number of groups of contiguous rois belonging to the same lesion . the radiomic features for the lesions were represented as a matrix of features with the row elements corresponding to the voxels enclosed within all the rois belonging to that lesion and the columns corresponding to the individual haralick textures . description of haralick texture features energy captures the average frequency of co - occurring ct intensities between neighboring voxels within a tumor , such that tumors with more homogeneous appearance have higher energy . 
correlation measures the frequency of positive or negative correlation of ct intensities between neighboring voxels within a tumor . initial patient cohort patients with recurrent oc who received pd - 1 or pd - l1 targeting antibodies alone or in combination with other immunotherapy ( n = 91 ) patients enrolled in ongoing single - arm prospective trials ( n = 90 ) patient treated off - label ( n = 1 ) exclusions ( n = 16 ) patients with absent baseline ce - ct ( n = 10 ) patients with image artifacts from orthopedic hardware ( n = 2 ) patients discontinued trial because of immune - mediated toxicity ( n = 4 ) final patient cohort patients included in each analysis ( n = 75 ) durable clinical benefit ( pfs 24 weeks ) time to off - treatment fig a1 . 
 radiomic predictors of response to immunotherapy baseline ct cluster - site dissimilarity , 1 , 648 ; time to off - treatment , 569 days baseline ct cluster - site dissimilarity 568 , 399 ; time to off - treatment , 42 days fig a2 . 
 pathogenic variants in less familiar cancer susceptibility genes : what happens after genetic testing ? purpose as genetic testing expands , patients are increasingly found to carry pathogenic variants in cancer susceptibility genes that are less familiar to most clinicians , specifically genes other than those causing hereditary breast ovarian cancer syndrome ( brca1 and brca2 ) and lynch syndrome . 
little is known about the subsequent behaviors of such patients in terms of managing cancer risks and informing relatives . methods all adult patients who were counseled and tested at the stanford cancer genetics clinic from january 2013 to july 2015 and had a pathogenic variant in a nonbrca1 / 2 , nonlynch syndrome gene were invited to participate in a telephone interview about adherence to risk - reducing recommendations , genetic testing by relatives , and new cancer incidence . results fifty - seven ( 40% ) of 142 eligible patients were successfully contacted , and all 57 patients participated ; median follow - up was 677 days ( range , 247 to 1 , 401 days )  . 
most patients ( 82% ; 95% ci , 70% to 90% ) recalled that a risk - reducing intervention ( screening , medication , or surgery ) was recommended , and most patients ( 85% ; 95% ci , 72% to 93% ) adhered to the recommendation . 
nearly all patients ( 91% ; 95% ci , 81% to 97% ) shared results with relatives , and most patients ( 78% ; 95% ci , 64% to 88% ) reported that a relative was subsequently tested . 
during the follow - up period , 9% of patients ( 95% ci , 3% to 19% ) developed second cancers , and in 14% of patients ( 95% ci , 7% to 26% ) , a first - degree relative developed cancer , some of which were detected by recommended screening . conclusion patients with a pathogenic variant in a less familiar cancer susceptibility gene report high adherence to risk - reducing interventions . 
furthermore , in the 57 carriers and subsequently tested relatives with two years of follow - up , a total of three cancers ( one in a proband and two in relatives ) were detected through interventions recommended on the basis of the pathogenic variant . 
 germline genetic testing is increasingly used to explain unusual or early - onset cancers in patients and to identify at - risk family members for targeted risk - reducing interventions . 
expert societies such as the national comprehensive cancer network and asco have developed guidelines to assist clinicians in determining which patients should have germline genetic testing.1 - 3 as guidelines have become more inclusive and the cost of genetic testing has decreased , pathogenic variants are increasingly discovered in those without a personal history of cancer , which can present a challenge for clinicians . 
 germline pathogenic variants in less familiar cancer genes ( eg , non - brca1 / 2 , nonlynch syndrome genes [ non - bl genes ] ) are increasingly recognized as determinants of cancer susceptibility . 
however , lack of clinician and patient familiarity with these lesser known genes may result in lower patient adherence to cancer risk reduction recommendations than with better characterized genes.4 in addition , little is known about how patients with mutations in less familiar genes disseminate and share results with their families . we aimed to assess the real - world outcomes and downstream impact of germline genetic testing on patients found to have pathogenic variants in non - bl genes . 
a cohort of such patients was interviewed about their understanding of cancer risks ; adherence to risk - reducing recommendations such as medications , surgery , or screening ; and downstream effects , including results communication to relatives and second cancer occurrence . methods study population we identified all adult ( 18 years old ) patients seen at the stanford cancer genetics clinic ( stanford , ca ) between january 2013 and july 2015 who had a pathogenic or likely pathogenic variant in a non - bl gene ( with lynch syndrome genes defined as mlh1 , msh2 , msh6 , pms2 , and epcam ) on germline clinical genetic testing . 
 variants were defined according to the report of clinical testing provided by clinical laboratory improvements amendmentcertified laboratories , according to guidelines of the american college of medical genetics.5 most patients presented to the clinic because they met national comprehensive cancer network guidelines for cancer genetics referral.1 survey design a short ( 10to 15 - minute ) phone survey was designed to address the following three major areas : first , did patients accurately recall and adhere to specific risk - reducing recommendations made by the cancer genetics clinic ? second , did family members complete recommended genetic testing ? third , did either the patient or any first - degree family members develop new cancers after genetics consultation ? if so , were these new cancers identified as a result of intensified screening as recommended by the clinic on the basis of genetic testing results ? patients were also interviewed about obstacles they encountered in completing risk - reducing recommendations or sharing results with their relatives . 
if he or she was not reached within three phone calls , he or she was sent a secure message through the electronic medical record patient portal with the contact information of the research teainformed consent was obtained by telephone before administration of the survey . 
this included race or ethnicity ( classified as non - hispanic [ nh ] white , hispanic , asian , ashkenazi jewish , native american , african american , or other ) , for which patients could elect multiple races or ethnicities if applicable . 
 information regarding personal and family history of cancer and recommendations made by the cancer genetics clinic were also collected from the electronic medical record . analysis patient demographic characteristics and personal and family history of cancer were tabulated . 
of the 57 patients contacted , 38 ( 67% ) were nh white , 11 ( 19% ) were hispanic , seven ( 12% ) were nh asian , three ( 5% ) were nh ashkenazi jewish , two ( 4% ) were nh native american , one ( 2% ) was nh african american , and two ( 4% ) were other . 
among the three patients with nbn mutations , one had the founder mutation c657_661del ( p.lys219asnfs * 16 ) , whereas the other two patients had other variants . overall , 47 interviewed patients ( 82% ; 95% ci , 70% to 90% ) recalled having any intervention recommended during their genetics consultation visit . 
clinical recommendations included changes in cancer screening ( 79% ; 95% ci , 67% to 88% ) , preventive surgery ( 14% ; 95% ci , 7% to 26% ) , and / or preventive medication ( 11% ; 95% ci , 5% to 21% ; fig 1a )  . 
forty - six patients ( 81% ; 95% ci , 68% to 89% ) recalled being recommended to undergo an intervention that was not already clearly indicated by their personal risk and / or family history of cancer . the most common changes recommended are listed in table 3 . 
the most frequently recommended surveillance strategies included increased frequency of colonoscopy ( n = 33 ; 58% [ 95% ci , 45% to 70% ] ) , annual breast magnetic resonance imaging ( mri ; n = 25 ; 44% [ 95% ci , 32% to 57% ] ) , upper endoscopy at regular intervals ( n = 9 ; 16% [ 95% ci , 8% to 28% ] ) , and annual full - body mri ( n = 4 ; 7% [ 95% ci , 2% to 17% ] )  . 
of these , five patients ( 9% ) were recommended to undergo mastectomy , five patients ( 9% ) were recommended to undergo bilateral salpingo - oophorectomy , and one patient was recommended to undergo hysterectomy . 
 ( b ) patient - reported adherence to recommendations , rate of disclosure to any family members , and reported further testing by at - risk family members . basis of personal or family cancer history in the absence of genetic testing results . most patients ( 85% ; 95% ci , 72% to 93% ) who were recommended to undergo the risk reduction measures listed in table 3 reported adhering to these recommendations ( fig 1b )  . 
reasons patients gave for not completing risk - reducing recommendations included difficulty scheduling procedures , pursuing a holistic approach , and contemplating surgical risks . analysis of patient behavior as it pertained to penetrance of the genetic variant is shown in table 4 . 
genes were categorized as high penetrance ( myh [ biallelic ] , palb2 , apc , tp53 , cdh1 , pten , sdhb , cdkn2a , and flcn ) , moderate penetrance ( chek2 , atm , nbn founder mutation , rad51c , and rad51d ) , and low penetrance ( myh [ monoallelic ] , mre11a , rad50 , apc i1307k variant , other nbn mutations , and chek2 i157t variant ) , as shown in appendix table a1 . 
adherence was high in all penetrance groups , without significant differences . nine percent ( 95% ci , 3% to 19% ) of patients reported a new incident cancer during the follow - up period , all of whom had reported adherence to risk reduction recommendations . 
 among these patients , one of the incident cancers , a breast cancer in a patient with a palb2 pathogenic variant , was detected because of screening recommendations ( breast mri ) made during genetics consultation . 
the other four cancers were detected incidentally and included the following : meningioma in a patient with a pten pathogenic variant , basal cell skin cancer in a patient with an nbn pathogenic variant ( nonfounder mutation ) , renal cell carcinoma in a patient with a monoallelic myh pathogenic variant , and chronic lymphocytic leukemia in a patient with an nbn pathogenic variant ( nonfounder mutation )  . 
no new cancers were reported among participants who were not undergoing recommended screening . seventy - nine percent ( 95% ci , 67% to 88% ) of patients recalled being counseled to advise family members to undergo genetic testing . 
 although most patients ( 91% ; 95% ci , 81% to 97% ) shared the testing results with their family members , some probands did not share their genetic testing results with any family members despite being advised to do so . 
of patients ( n = 57 ) % ( 95% ci ) increased surveillance increased frequency of colonoscopy screening annual breast magnetic resonance imaging upper endoscopy whole - body magnetic resonance imaging risk - reducing surgery bilateral mastectomy bilateral salpingooophorectomy risk - reducing medication tamoxifen aromatase inhibitor 58 ( 45 to 70 ) 44 ( 32 to 57 ) 16 ( 8 to 28 ) 7 ( 2 to 17 ) 9 ( 3 to 19 ) 9 ( 3 to 19 ) 9 ( 3 to 19 ) 2 ( 0 to 10 ) family member undergo subsequent genetic testing ( fig 1b )  . 
reported reasons why family members chose not to undergo genetic testing included elderly age , difficulty with insurance coverage , planning for testing in the future , and unable to get genetic testing overseas . 
 four probands reported that some relatives either explicitly refused to hear the probands genetic testing results or dismissed and ignored the results immediately upon being notified . in the time between their genetics clinic visit and study participation , eight patients ( 14% ; 95% ci , 7% to 26% ) reported that first - degree relatives were newly diagnosed with cancer . 
among the group of eight newly diagnosed relatives , two ( 25% ; 95% ci , 6% to 60% ) had cancers that were detected in screening recommended after identification of the familial pathogenic variant in the relative ( one with colon cancer who was undergoing recommended screening after an apc pathogenic variant [ high penetrance ] was detected and one with breast cancer who was undergoing intensified screening including breast mri after identification of a nbn pathogenic variant [ founder mutation ] )  . 
in the case of the apc carrier who developed colon cancer , the genetic testing results were instrumental to her receiving the colonoscopy that detected the cancer ; she would not have qualified for colonoscopy without the detected pathogenic variant because of her young age ( mid - 30s )  . 
 % ( 95% ci ) shared genetic testing results with family members at least one member of family received cascade genetic high penetrance moderate penetrance low penetrance high penetrance moderate penetrance low penetrance testing high penetrance moderate penetrance low penetrance 18 / 20 14 / 16 8 / 11 23 / 23 16 / 19 13 / 15 17 / 21 10 / 16 10 / 12 90 ( 69 to 98 ) 88 ( 63 to 98 ) 73 ( 43 to 91 ) 100 ( 83 to 100 ) 84 ( 62 to 95 ) 87 ( 61 to 98 ) 81 ( 59 to 92 ) 63 ( 39 to 82 ) 83 ( 54 to 97 ) note . 
thus , understanding how patients and their families react to identification of such less familiar , non - bl pathogenic variants is increasingly important for oncology practice . a limitation of our study is the relatively low participation rate ( 40% ) , which was a function of difficulty in reaching the study population after a median of 677 days since their clinical evaluation . 
it is reassuring , however , that all patients who were successfully contacted ( n = 57 ; 40% of the 142 eligible patients ) agreed to participate in the study , which may somewhat reduce selection bias . 
although generalizability may be limited , several striking results of this study suggest a potential benefit for counseling and testing of non - bl genes and warrant confirmation in larger studies . most notably , at 2 years after genetics consultation , we observed high patient adherence to gene - specific recommendations for cancer riskreducing interventions and dissemination of results to relatives . 
this is encouraging because it suggests that genetic testing not only had its intended effect in patients seen in the clinic , but may also have benefited their relatives in a cascade effect . 
other studies of women at high breast cancer risk suggest that self - reported adherence to recommended interventions are in line with our results ( 59% reported full adherence ) .6 within a relatively short follow - up interval , nearly 10% of patients in our small sample developed a second malignancy . 
 participants reported several new cancers in first - degree relatives , some identified because of screening interventions that were prompted by detection of the familial pathogenic variant after recommended cascade genetic testing . 
this emphasizes the potential benefits of cascade testing among relatives and subsequent risk reduction interventions . nearly one quarter of participants reported that relatives did not have genetic testing , despite clinicians recommendations and patients reported sharing of genetic information . 
this represents a significant opportunity for improvement in cascade genetic testing of relatives , which is an essential component of population - wide cancer prevention.7 - 9 patients offered several reasons for the lack of subsequent testing , including incomplete dissemination ( some patients did not share genetic information with all at - risk family members , in some cases because of their own fear of stigma or limited understanding ) , lack of patient contact with family members , lack of access to genetic counseling or testing by family members , 10 cost or insurance barriers to testing by family members , and a perceived stigma associated with pathogenic variants . 
it is also possible that family members may have been tested but did not share this information with the proband , because our contact was exclusively with the proband in this study . the observed dissemination of genetic testing results to at - risk family members in this study is concordant with prior research on brca1 / 2 and lynch syndrome genes . 
healey et al11 found that most patients disclosed their results to at least one at - risk family member ; larger family size , higher psychological distress score in the carrier , and broader geographic distribution of at - risk family members were associated with lower rates of fully informed families . 
earlier studies have suggested that patients are more likely to contact first - degree family members than more distant relatives ( eg , cousins ) with brca1 / 2 results.12 we found that the reported genetic testing rate among relatives was notably less than the reported rate of these relatives being informed of the results , consistent with studies of brca1 / 2 and lynch syndrome gene pathogenic variants.13 , 14 our finding of a similar conundrum among patients with less familiar pathogenic variants suggests the need for more effective , widely accessible approaches to cascade genetic testing of family members . our study has some limitations , in addition to the previously noted participation rate of 40% . 
 patients who could be successfully contacted and offered participation ( all of whom agreed to participate ) may have been more likely to adhere to recommendations than those who could not be contacted , so these results may overestimate adherence and the downstream impact of testing . 
for some patients , we could not verify adherence to recommended interventions directly because they received their longitudinal care in a different medical system than the tertiary center at which they had genetic testing , so it is possible that the true rates of adherence are less than reported here . large population - based studies will be crucial to understand the real - world outcomes of germline multiple - gene panel testing and its contribution to precision oncology . 
as more is learned about the prevalence , penetrance , and cancer phenotype of the less familiar pathogenic variants studied here , a richer evidence base will develop to inform practice guidelines for gene - specific cancer risk reduction . 
novel care delivery models , such as dedicated follow - up programs for pathogenic variant carriers to assess adherence , barriers to risk - reducing interventions , and cascade testing of relatives , will be essential to fulfill the promise of germline genetic testing . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . divya parikh no relationship to disclose jennifer l . 
daly mb , pilarski r , berry m , et al : nccn guidelines insights : genetic / familial high - risk assessment : breast and ovarian , version 2.2017. 
desjardin jt , dhawan ms , blanco a , et al : effects of gene penetrance on adherence to breast cancer screening recommendations ( bcsr ) among high - risk women . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
vetter l , keller m , bruckner t , et al : adherence to the breast cancer surveillance program for women at risk for familial breast and ovarian cancer versus overscreening : a monocenter study in germany . 
samimi g , bernardini mq , brody lc , et al : traceback : a proposed framework to increase identification and genetic counseling of brca1 and brca2 mutation carriers through familybased outreach . 
caswell - jin j , zimmer a , stedden w , et al : cascade genetic testing of relatives for hereditary cancer risk : first year of a low - cost , accessible family testing program.presented at the american college of medical genetics and genomics annual meeting , charlotte , nc , april 13 , 2018 10 . 
fehniger j , lin f , beattie ms , et al : family communication of brca1 / 2 results and family uptake of brca1 / 2 testing in a diverse population of brca1 / 2 carriers . 
 revisiting epidermal growth factor receptor ( egfr ) amplification as a target for anti - egfr therapy : analysis of cell - free circulating tumor dna in patients with advanced malignancies shumei kato ryosuke okamura manvita mareboina suzanna lee aaron goodman sandip p . 
contributed equally to this work . corresponding author : shumei kato , md , center for personalized cancer therapy and division of hematology and oncology , department of medicine , uc san diego moores cancer center , 3855 health sciences dr , la jolla , ca 92093 ; e - mail : smkato@ucsd.edu. licensed under the creative commons attribution 4.0 license purpose to date , evidence for tissue epidermal growth factor receptor ( egfr ) overexpression as a biomarker for anti - egfr therapies has been weak . 
we investigated the genomic landscape of egfr amplification in blood - derived cell - free tumor dna ( cfdna ) across diverse cancers and the role of anti - egfr therapies in achieving response . methods we assessed egfr amplification status among 28 , 584 patients with malignancies evaluated by clinical - grade next - generation sequencing ( ngs ) of blood - derived cfdna ( 54to 73 - gene panel )  . 
furthermore , we curated the clinical characteristics of 1 , 434 patients at the university of california san diego who had cfdna testing by this ngs test . results overall , egfr amplification was detected in cfdna from 8.5% of patients ( 2 , 423 of 28 , 584 ) , most commonly in colorectal ( 16.3% [ 458 of 2 , 807 ] ) , nonsmall - cell lung ( 9.0% [ 1 , 096 of 12 , 197 ] ) , and genitourinary cancers ( 8.1% [ 170 of 2 , 104 ] )  . 
most patients had genomic coalterations ( 96.9% [ 95 of 98 ] ) , frequently involving genes affecting other tyrosine kinases ( 72.4% [ 71 of 98 ] ) , mitogen - activated protein kinase cascades ( 56.1% [ 55 of 98 ] ) , cell - cycleassociated signals ( 52.0% [ 51 of 98 ] ) , and the phosphoinositide 3 - kinase pathway ( 35.7% [ 35 of 98 ] )  . 
egfr amplification emerged in serial cfdna after various anticancer therapies ( n = 6 ) , including checkpoint inhibitors ( n = 4 ) , suggesting a possible role for these amplifications in acquired resistance . 
nine evaluable patients with egfr amplification were treated with anti - egfrbased regimens ; five ( 55.6% ) achieved partial responses , including three patients whose tissue ngs lacked egfr amplification . conclusion egfr amplification was detected in cfdna among 8.5% of 28 , 584 diverse cancers . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction epidermal growth factor receptor ( egfr ) , also known as human epidermal growth factor receptor 1 ( her1 ) or erbb1 , is a receptor tyrosine kinase that belongs to the erbb family proteins . 
 phosphorylation of tyrosine residues in the egfr intracellular domaactivation of egfr leads to multiple downstream signals , including mitogen - activated protein kinase and phosphoinositide 3 - kinase pathways , which enhances cell proliferation and survival.1 , 2 functional activation of egfr via mutation or amplification / overexpression has been identified in many tumor types , including lung , head and neck , gastroesophageal , and colorectal cancers , and has been associated with proliferation , invasion , and metastasis.3 , 4 alterations in egfr have also been linked to primary resistance and accelerated tumor growth ( designated as hyperprogression ) from immune checkpoint inhibitors.5 - 7 because of its critical role in tumor aggressiveness , egfr has been an attractive target for anticancer therapy.1 to date , there are various anti - egfr therapies that are us food and drug administration approved , including erlotinib , gefitinib , afatinib , and osimertinib for nonsmall - cell lung cancer ( nsclc ) with specific activating egfr mutations , 8 cetuximab and panitumumab for colorectal cancer without kras or nras mutations , 9 cetuximab for head and neck cancer , 10 and necitumumab for squamous cell carcinoma of lung.11 biomarkers to predict response to anti - egfr therapies have been studied extensively . 
egfr and kras mutation status are widely used in lung and colorectal cancer , respectively.8 , 9 , 12 , 13 in contrast , egfr amplification and overexpression in tissue have not been well established as reliable biomarkers for anti - egfr agents , ( selected studies that investigated egfr amplification / overexpression as a predictive marker for anti - egfr therapies are summarized in the data supplement ) 11 , 14 - 19 . 
overall , a meta - analysis concluded that tissue egfr amplification status could not be demonstrated to be a consistent biomarker to predict the outcome from antiegfr therapies in colorectal cancer.20 although it is somewhat surprising that tissue egfr amplification / expression status has not been established as a reliable biomarker for anti - egfr therapies , potential reasons include heterogeneity between primary and metastatic lesions , dynamic changes in genomic alterations that may emerge along with therapeutic pressure or progression , presence of genomic coalterations associated with resistance , and potential differences in response to copy number gain due to aneuploidy versus focal egfr amplification.21 - 23 use of plasma - derived cell - free tumor dna ( cfdna ) to assess egfr status by next - generation sequencing ( ngs ) could conceivably overcome some of these limitations by detecting tumor - specific alterations that are shed into the bloodstream from multiple metastatic sites as well as the primary cancer.23 - 29 herein , we examined the genomic landscape of egfr amplification by interrogating blood derived cfdna from 28 , 584 patients with diverse malignancies using clinical - grade ngs . 
furthermore , we investigated the clinical characteristics , concordance between tissue ngs and cfdna , and therapeutic outcome after antiegfr therapies among a subset of 1 , 434 clinically annotated patients at the university of california , san diego ( ucsd ) , moores cancer center . methods patients the genomic landscape of egfr amplification among 28 , 584 diverse solid cancers that were referred to guardant health from march 2014 to february 2017 , were evaluated . 
furthermore , we have curated the clinical characteristics of 1 , 434 evaluable patients with diverse cancers at ucsd who had cfdna testing at guardant health starting in march 2014 . 
all investigations followed the guidelines of the ucsd institutional review board for data collection ( profile related evidence determining individualized cancer therapy ; clinicaltrials.gov identifier : nct02478931 ) and for any investigational therapies for which the patients consented ( data supplement )  . ngs for cfdna and tissue all cfdna analyses were performed at guardant health as previously described ( data supplement ) .26 tissue ngs was performed at foundation medicine , as previously described30 ( data supplement )  . end points and statistical methods patient characteristics , prevalence of egfr amplification , and genomic coalterations were summarized by descriptive statistics . 
the most common cancer harboring egfr amplification was colorectal cancer ( 16.3% [ 458 of 2 , 807 ] ) , followed by nonsmall - cell lung cancer ( 9.0% [ 1 , 096 of 12 , 197 ] ) and genitourinary cancers ( 8.1% [ 170 of 2 , 104 ] )  . 
 ( b ) prevalence of egfr amplification by cfdna among diverse cancer from university of california , san diego ( ucsd ) , cohort ( n = 1 , 434 )  . 
the most common cancer harboring egfr amplification was small - cell lung cancer ( 30.0% [ three of 10 ] ) , followed by breast cancer ( 14.7% [ 16 of 109 ] ) and colorectal cancer ( 12.6% [ 16 of 127 ] )  . 
 includes four patients with carcinoma of unknown primary ( + [ n = 1 ] , + + [ n = 2 ] , + + + [ n = 1 ] ) and two patients with adrenocortical carcinoma ( + + [ n = 2 ] )  . concordances between cfdna and tissue dna were described by percentage of concordance and value with standard error . 
on the other hand , coalterations in these genes were found significantly less frequently among patients without egfr amplification : coalterations in tp53 in 32.1% of patients , braf ( 4.9% ) , met ( 2.5% ) , cdk6 ( 1.4% ) , and pik3ca ( 8.8% ; all p < .001 ; fig 2 )  . 
when the genes were categorized according to their oncogenic roles , 72.4% ( 71 of 98 ) of patients with egfr amplification had at least one characterized coalteration potential targeted therapies for coalterations associated with egfr amplification in the ucsd cohort of 98 patients positive for egfr amplification , 96.9% ( 95 of 98 ) of patient tumors had at least one characterized coalteration . 
all these 95 malignancies harbored at least one characterized coalteration potentially targetable with us food and drug administration approved agents as onor off - label use . clinical characteristics of patients who had emerging egfr amplification with serial cfdna analyses six patients who initially tested negative for egfr amplification in both tissue ngs and cfdna were found to have emerging egfr amplification with serial cfdna analyses . 
 diagnosis timeline of emerging egfr amplification detected by cfdna analysis along with systemic therapy patient age ( y ) / 71 / m lung adenocarcinoma 50 / f breast cancer 69 / m hepatocellular carcinoma 44 / f breast cancer 56 / m anal squamous cell carcinoma 49 / m rectal adenocarcinoma fig 3 . 
six patients who initially tested negative for egfr amplification on tissue next - generation sequencing as well as cfdna were found to have egfr amplification with serial cfdna analyses after various treatments ; in four patients , treatment regimens included immune checkpoint inhibitors ( n = 4 ; patients 30 , 33 , 43 , and 46 )  . 
among 72 patients with egfr amplification ( without coexisting egfr mutations ) , nine received treatment regimens that included anti - egfr agents after cfdna testing ( appendix fig a3 )  . 
types of anti egfrbased regimens were as follows : monotherapy with anti - egfr antibody ( n = 1 ) , anti - egfr antibody plus another targeted agent ( n = 1 ) , egfr tyrosine kinase inhibitor plus another targeted agent ( n = 1 ) , anti - egfr antibody plus cytotoxic agents ( n = 2 ) , and dual antiegfr therapybased regimens ( combination of anti - egfr antibody plus egfr tyrosine kinase inhibitor ; n = 4 )  . 
overall , tumor reduction was seen in six of nine patients ( 66.7% ) , including five ( 55.6% ) who attained a partial response ( pr ) per recist 1.1 ( fig 4 )  . 
illustrative responders are depicted in figure 5.28 discussion we describe the comprehensive landscape of egfr amplification in cfdna among 28 , 584 patients with varied malignancies whose liquid biopsy was evaluated at a central , clinical - grade laboratory . 
overall , tumor reduction was seen in six of nine ( 66.7% ) , including five of nine ( 55.6% ) patients with partial response per response evaluation criteria in solid tumors 1.1. 
 egfr amplification ( 3 + ) mtor l387l ( 1.0% ) apc d2696y ( 2.4% ) arid1a p469l ( 3.5% ) ntrk1 a500v ( 4.5% ) arid1a s2269 * ( 4.6% ) brca2 d3260h ( 10.8% ) brca1 l30f ( 19.6% ) nf1 d2482y ( 20.7% ) brca1 g211e ( 26.7% ) akt1 e17k ( 66.5% ) egfr amplification ( ) esr1 e380q ( 0.1% ) tp53 y220c ( 0.1% ) brca1 g211e ( 0.3% ) egfr amplification ( ) esr1 e380q ( 0.2% ) akt1 e17k ( 0.3% ) cfdna months from the initiation of anti - egfr therapies cfdna before treatment imaging shown in figure 5b pembrolizumab cetuximab erlotinib before adding anti - egfr therapies cetuximab / erlotinib x 2 months cetuximab / erlotinib x ( cid : 3 ) 4 months pretreatment 9 weeks post cetuximab monotherapy at diagnosis cetuximab / erlotinib x 2 months cetuximab / erlotinib x 17 months fig 5 . 
a 55 - year - old woman with metastatic triple - negative breast cancer to bone and lung was treated with pembrolizumab with initial disease stability for more than 1 year , but then progression in the bones and deteriorating performance status requiring a wheelchair . 
 correlate better with response than protein expression , perhaps because of technical limitations associated with assessment of immunohistochemistry staining.31 - 34 prior studies looking at the relationship between egfr amplification and therapeutic response to egfr inhibitors showed inconsistent results ( data supplement )  . 
 indeed , pectasides et al23 demonstrated that , among patients with treatment - naive metastatic gastroesophageal cancers , discordant gene alterations between primary and metastatic tissue were common , being seen in 42% of patients . 
the concordance rate documented by pectasides et al23 is similar to that in the current report that showed an 89.3% concordance rate for egfr amplification between cfdna and tissue ngs ( data supplement )  . 
these results suggest that biopsy of a limited tumor focus can misrepresent the overall genomic condition of disease and , thus , may not be a completely accurate guide for targeted treatment . 
consistent with this concept , among our nine evaluable patients who harbored egfr amplification by cfdna analysis , anti - egfrbased therapies led to tumor reduction in 66.7% ( six of nine ) including 55.6% ( five of nine ) who achieved a pr ( fig 4 )  . 
our data are comparable to those of maron et al , 35 who showed a 58% ( four of seven ) objective response rate among patients with egfr - amplified gastric cancer ( all seven patients were positive for egfr amplification by tissue ngs , and six were positive by cfdna analysis )  . 
 importantly , dual inhibition with both an antibody and a small molecule targeting the same receptor has been investigated among patients with her2 - positive breast cancer and reported to have significantly higher response rates when compared with either drug alone.37 efficacy of dual - targeted therapy was also seen in patients with her2 - positive colon cancer that showed a 30% response rate with trastuzumab / lapatinib combination.38 similarly , early - phase clinical trials with dual - egfr inhibition ( cetuximab / afatinibor cetuximab / erlotinib - based therapy ) showed favorable clinical outcomes among patients with refractory nsclc and colorectal cancer.39 - 43 the mechanism by which dual inhibition operates is not fully elucidated , but preclinical studies suggest that kinase receptors may function via kinase - dependent and - independent mechanisms.44 , 45 although responses were seen in more than half of the patients with egfr amplification fig 5 . 
after starting anti - egfr agents , the patient achieved 16% tumor shrinkage per response evaluation criteria in solid tumors ( recist ) 1.1 ( b , left to right ) , with symptomatic improvement allowing the patient to ambulate without narcotics for pain control . 
a 53 - year - old woman with metastatic rectal adenocarcinoma to the liver and lungs presented after experiencing disease progression while receiving two lines of therapies ( infusional fluorouracil , leucovorin , and oxaliplatin with bevacizumab and fluorouracil , leucovorin , and irinotecan with bevacizumab )  . 
therapy was started with single - agent cetuximab , and a 44% reduction in tumor burden by recist 1.1 was seen ( progression - free survival , 6.0 months ; c , left to right )  . 
therapy with dual anti - egfr therapy ( cetuximab and erlotinib ) was started ( patient was also administered one dose of nivolumab on the basis of programmed death ligand 1 positive by immunohistochemistry ; however , held because of severe rash )  . 
indeed , as seen in figure 4 , of the nine patients with cfdna egfr amplification treated with egfr targeting agents , the four nonresponders had six to nine genomic coalterations , whereas the five responders had only zero to five coalterations per patient . 
furthermore , the patient with the greatest tumor regression and most durable response ( fig 4 , patient 25 ; progression - free survival , 18 months ) demonstrated no genomic coalterations on cfdna . 
of interest , patients who failed to achieve prolonged responses had coalterations in specific oncogenic pathways , including cdk4 / 6 , met , pdgfra , erbb2 , fgfr1 , pik3ca , akt1 , kras , and braf , some of which are known to be associated with resistance to anti - egfr therapies.46 , 47 considering that patients with egfr amplification had frequent potentially tractable coalterations ( fig 2 ; appendix figs a1and a2 ) , a customized combination strategy may be required.48 , 49 although current findings do not provide definitive proof of antitumor activity , these observations suggest that studies of appropriate combinations of drugs that target both the egfr amplification and the coalterations would be of interest . 
investigation of such an approach is currently ongoing ( clinicaltrial.gov identifier : nct02534675 ; i - predict [ study of molecular profile - related evidence to determine individualized therapy for advanced or poor prognosis cancers ] )  . interestingly , oxnard et al50 and abbosh et al51 have shown that more extensive disease burden corresponds to higher rates of cfdna detection . 
the finding of higher numbers of comutations in patients harboring egfr amplification events could therefore be a possible effect of increased aggressiveness and higher tumor burden ( with more extensive disease shedding more cfdna and thus permitting detection of more alterations ) , or , alternatively , higher numbers of comutations could be a cause of increased aggressiveness . 
this observation suggests that the association between survival and number of alterations is independent of the percent cfdna ( with the latter correlating with disease burden ; unpublished data )  . in the current report , we also identified patients whose egfr amplifications emerged in their liquid biopsy with serial testing after a variety of anticancer therapies ( n = 6 ; fig 3 )  . 
for instance , one patient who was treated with the egfr tyrosine kinase inhibitor erlotinib showed emergence of blood - derived egfr amplification after disease progression ( fig 4 ) , consistent with a previous report demonstrating tumor evolution with egfr amplification as a potential resistance mechanism to egfr tyrosine kinase inhibitor administration.52 perhaps relevant in this regard , all of our responders had an egfr antibody included in their regimen . 
although egfr alterations are reported to be associated with primary resistance and hyperprogression after immune checkpoint blockade , 6 , 7 the current observation may suggest that egfr amplification can also be a possible mechanism for acquired resistance after checkpoint blockades . 
 this is suggested by our representative patient who was treated with pembrolizumab , had a mixed response , and then received erlotinib and cetuximab ( in addition to ongoing pembrolizumab ) and showed reduction in egfr cfdna copy number as well as regression of tumor foci and improvement in pain and performance status ( fig 4 , patient 26 ; figs 5a and 5b ) .39 , 40 additional investigation is required to understand the complex interplay of response and resistance associated with egfr amplifications , egfr - targeting pharmaceuticals , and checkpoint blockade . there were several limitations to the current study . 
 yet , despite these limitations , the study provides a comprehensive analysis of egfr amplification detected from plasma - derived cfdna in a wide range of malignancies . in conclusion , among patients with diverse cancers ( n = 28 , 584 from a central laboratory ) , cfdna interrogated by clinical - grade ngs revealed that 8.5% of patients with solid cancers harbored egfr amplification . 
most patients found to have egfr amplification also had genomic coalterations that are , in theory , pharmacologically tractable ( 96.9% [ 95 of 98 ] ) by available drugs . 
anti - egfr based therapies among patients found to have egfr amplification by cfdna analysis achieved responses in 55.6% of patients ( five of nine ) , including in three individuals who failed to show egfr amplification on tissue ngs . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . shumei kato no relationship to disclose ryosuke okamura no relationship to disclose manvita mareboina no relationship to disclose aaron goodman consulting or advisory role : mitsubishi tanabe pharma , gerson lehrman group sandip p . 
patel consulting or advisory role : eli lilly , novartis , bristol - myers squibb , astrazeneca / medimmune , nektar , compugen speakers ' bureau : merck , boehringer ingelheim research funding : bristol - myers squibb ( inst ) , eli lilly ( inst ) , incyte ( inst ) , medimmune ( inst ) , pfizer ( inst ) , genentech ( inst ) , xcovery ( inst ) , amgen ( inst ) , astrazeneca / medimmune ( inst ) paul t . 
schwab stock and other ownership interests : samumed ( i ) patents , royalties , other intellectual property : the patent covers sialylated glycans and antibodies that specifically bind to them for early detection and diagnosis of cancer . 
raymond employment : trovagene , guardant health stock and other ownership interests : trovagene , guardant health suzanna lee stock and other ownership interests : invitae , gilead sciences , merck , juno therapeutics , sequenom richard b . 
lippman no relationship to disclose stock and other ownership interests : curematch , idbydna consulting or advisory role : actuate therapeutics , loxo oncology , xbiotech , neomed , roche speakers ' bureau : roche research funding : guardant health ( inst ) , sequenom ( inst ) , merck serono ( inst ) , genentech ( inst ) , pfizer ( inst ) , foundation medicine ( inst ) , incyte ( inst ) , konica minolta ( inst ) affiliations shumei kato , ryosuke okamura , manvita mareboina , suzanna lee , aaron goodman , sandip p . 
lanman , guardant health , redwood city , ca . supported in part by the joan and irwin jacobs philanthropic fund and by national cancer institute at the national institutes of health grant no . 
lu z , jiang g , blume - jensen p , et al : epidermal growth factor - induced tumor cell invasion and metastasis initiated by dephosphorylation and downregulation of focal adhesion kinase . 
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rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with nonsmall - cell lung cancer profiled with targeted next - generation sequencing . 
allegra cj , jessup jm , somerfield mr , et al : american society of clinical oncology provisional clinical opinion : testing for kras gene mutations in patients with metastatic colorectal carcinoma to predict response to anti - epidermal growth factor receptor monoclonal antibody therapy . 
thatcher n , hirsch fr , luft av , et al : necitumumab plus gemcitabine and cisplatin versus gemcitabine and cisplatin alone as first - line therapy in patients with stage iv squamous nonsmall - cell lung cancer ( squire ) : an open - label , randomised , controlled phase 3 trial . 
tsigelny if , wheler jj , greenberg jp , et al : molecular determinants of drug - specific sensitivity for epidermal growth factor receptor ( egfr ) exon 19 and 20 mutants in non - small cell lung cancer . 
wheler jj , falchook gs , tsimberidou am , et al : aberrations in the epidermal growth factor receptor gene in 958 patients with diverse advanced tumors : implications for therapy . 
bokemeyer c , bondarenko i , hartmann jt , et al : efficacy according to biomarker status of cetuximab plus folfox - 4 as first - line treatment for metastatic colorectal cancer : the opus study . 
herbst rs , redman mw , kim es , et al : cetuximab plus carboplatin and paclitaxel with or without bevacizumab versus carboplatin and paclitaxel with or without bevacizumab in advanced nsclc ( swog s0819 ) : a randomised , phase 3 study . 
licitra l , mesia r , rivera f , et al : evaluation of egfr gene copy number as a predictive biomarker for the efficacy of cetuximab in combination with chemotherapy in the first - line treatment of recurrent and / or metastatic squamous cell carcinoma of the head and neck : extreme study . 
lordick f , kang yk , chung hc , et al : capecitabine and cisplatin with or without cetuximab for patients with previously untreated advanced gastric cancer ( expand ) : a randomised , openlabel phase 3 trial . 
yang zy , shen wx , hu xf , et al : egfr gene copy number as a predictive biomarker for the treatment of metastatic colorectal cancer with anti - egfr monoclonal antibodies : a metaanalysis . 
misale s , di nicolantonio f , sartore - bianchi a , et al : resistance to anti - egfr therapy in colorectal cancer : from heterogeneity to convergent evolution . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
schwaederl mc , patel sp , husain h , et al : utility of genomic assessment of blood - derived circulating tumor dna ( ctdna ) in patients with advanced lung adenocarcinoma . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
kim st , banks kc , pectasides e , et al : impact of genomic alterations on lapatinib treatment outcome and cell - free genomic landscape during her2 therapy in her2 + gastric cancer patients . 
baselga j , bradbury i , eidtmann h , et al : lapatinib with trastuzumab for her2 - positive early breast cancer ( neoaltto ) : a randomised , open - label , multicentre , phase 3 trial . 
sartore - bianchi a , trusolino l , martino c , et al : dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - of - concept , multicentre , open - label , phase 2 trial . 
falchook gs , naing a , hong ds , et al : dual egfr inhibition in combination with anti - vegf treatment : a phase i clinical trial in non - small cell lung cancer . 
janjigian yy , smit ef , groen hj , et al : dual inhibition of egfr with afatinib and cetuximab in kinase inhibitor - resistant egfr - mutant lung cancer with and without t790m mutations . 
wheler jj , tsimberidou am , falchook gs , et al : combining erlotinib and cetuximab is associated with activity in patients with non - small cell lung cancer ( including squamous cell carcinomas ) and wild - type egfr or resistant mutations . 
wheler j , falchook g , tsimberidou am , et al : revisiting clinical trials using egfr inhibitorbased regimens in patients with advanced non - small cell lung cancer : a retrospective analysis of an md anderson cancer center phase i population . 
janku f , huang hj , angelo ls , et al : a kinase - independent biological activity for insulin growth factor - 1 receptor ( igf - 1r ) : implications for inhibition of the igf - 1r signal . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - small - cell lung cancer . 
mandelker , md1 ; semanti mukherjee , phd1 ; carolyn stewart1 ; deborah delair , md1 ; vignesh ravichandran1 ; preethi srinivasan , phd1 ; daire hurley3 ; yelena kemel1 ; angela g . 
abu - rustum , md1 , 2 ; and zsoa stadler , md1 , 2 purpose mutations in dna mismatch repair genes and pten , diagnostic of lynch and cowden syndromes , respectively , represent the only established inherited predisposition genes in endometrial cancer to date . 
per institutional standards , all tumors underwent lynch syndrome screening via immunohistochemistry ( ihc ) for mismatch repair proteins . results of 156 patients who consented to germline genetic testing , 118 ( 76% ) had stage i disease . 
twenty - four pathogenic germline variants were identied in 22 patients ( 14% ) : seven ( 4.5% ) had highly penetrant cancer syndromes and 15 ( 9.6% ) had variants in low - penetrance , moderate - penetrance , or recessive genes . 
the remaining 17 variants ( 71% ) were incremental ndings in lowand moderate - penetrance variants or genes associated with recessive disease . conclusion in unselected patients with predominantly low - risk , early - stage endometrial cancer , germline multigene panel testing identied cancer predisposition gene variants in 14% . 
they are associated with a signicant lifetime risk of ec , but they account for less than 5% of diagnoses.2 data regarding inherited risk in ec have been generated from selected patient populations , often ascertained from cancer genetics clinics from patients who have been referred because of a personal or family cancer history . 
for women with ls , ec is often the sentinel event , 3 and universal tumor screening of ec via mmr protein staining or microsatellite instability ( msi ) assessment is recommended.4 data regarding the breadth of inherited genetic mutations in an unselected ec patient population are limited . 
 cadoo et al context key objective to determine the prevalence of pathogenic germline variants in unselected patients with endometrial cancer . knowledge generated a custom next - generation sequencing panel , the memorial sloan ketteringintegrated mutation proling of actionable cancer targetsmsk - impactidentied 24 pathogenic germline variants in 22 patients ( 14% ) , including 4.5% who had pathogenic variants in high - penetrance genes . 
mismatch repair protein immunohistochemistry ( ihc ) screening identied all patients with lynch syndrome ( ls ; 3% of the overall cohort ) , representing the majority of high - penetrance variants . relevance in patients with predominantly low - risk endometrial cancer , identication of pathogenic germline variants via a multigene panel test may have implications in altering cancer screening and risk - reduction recommendations . 
electronic medical records were reviewed for demographic and clinical variables , including family history . sequencing , variant calling , and reporting of results memorial sloan ketteringintegrated mutation proling of actionable cancer targets ( msk - impact ) , a 468 - gene targeted capture panel , was used for tumor sequencing . germline analysis initially included a 76 - gene hereditary predisposition panel which was later revised to an 88 - gene panel ( appendix table a1 ) .6 - 8 for patients sequenced on the original panel , targeted review was performed for mutations in pole and pold . 
clinical variables in subsets dened by mutation status were compared by analysis of variance using graphpad prism version 7.01 ( graphpad , san diego , ca ) test tumor analysis for mmr deciency and ls screening institutional standards , all ecs undergo universal screening for ls via mmr protein immunohistochemistry ( ihc ) staining for mlh1 , msh2 , msh6 , and pms2.15 if mlh1 or pms2 are absent , reex mlh1 promoter methylation analysis is performed . 
in this study , msi status was also assessed via msi sensor , a computational algorithm that analyzes sequencing reads at designated microsatellite regions in tumor - normal pairs and reports the percentage of unstable loci as a cumulative score.16 an msi sensor score of 10 or greater indicates msi - high status ( msi - h ) , a score of 3 to 9 indicates msi - intermediate status ( msi - i ) , and a score of less than 3 indicates microsatellite stable status ( mss )  . results patient characteristics germline genetic testing was performed in 156 women ( fig 1 )  . 
the majority self - identied as white ( 83% ) , and 24% were ashkenazi jews . median ( range ) overweight or obese age , years median ( range ) 50 self - identied race asian black white aj heritage unknown stage histology carcinoma nos carcinosarcoma clear cell mixed serous endometrioid grade hysterectomies performed for endometrial cancer from april 2016 to may 2017 signed consent for somatic sequencing signed consent for germline sequencing pathogenic germline mutations identified ( n = 435 ) ( n = 179 ) ( n = 156 ) ( n = 24 ) fig 1 . 
one patient had a sister with ec in her 30s and no other ls - associated cancers in her family , and one patient had limited family history available ( table 2 )  . beyond the mmr genes , two other high - penetrance germline mutations were identied in brca1 and smarca4 ( table 2 )  . the brca1 mutation carrier had previously tested positive for this known familial mutation and underwent riskreducing salpingo - oophorectomy ( rrso ) without hysterectomy . 
a 72 - year - old woman who had clear cell ec lobular breast cancer when she was in her 40s and a family history of breast and prostate cancer had a deletion of smarca4 exon 17 - 18 identied with smarca4 ihc loss in her tumor . of these seven patients with high - penetrance mutations , six ( 86% ) met criteria for testing for the implicated gene betheir personal or family cancer history . 
the cause of smarca4 deletion carrier had no personal or family history of small cell ovarian tumors or rhabdoid tumor predisposition syndrome ( table 2 )  . lowand moderate - penetrance or recessive - only genes the other 17 ( 71% ) pathogenic germline mutations ( in 15 patients ) were in lowand moderate - penetrance or abbreviations : aj , ashkenazi jewish ; bmi , body mass index ; nos , not otherwise specied . recessive - only genes ( table 2 )  . 
the remaining mutations were in chek2 ( missense variant i157t ) , mre11a , mutyh , and reql4 . seven ( 47% ) of the 15 patients with variants in lowor moderate - penetrance or recessive genes met national comprehensive cancer network ( nccn ) criteria for brca testing on the basis of personal or family history . 
 inherited risk in the development of endometrial cancer there was no association of pathogenic germline mutations in these lowor moderate - penetrance or recessive - only genes compared with population controls ; however , the analysis is limited by the small size of the cohort . 
the remaining two patients were discordant , with each having a single mmr gene somatic mutation in a gene that does not correspond to the ihc loss . msi sensor score was concordant with ihc in 140 patients ( 90% ; 112 mss / ihc retained and 28 msi - h / mmrdecient ; fig 2b )  . 
however , only two ls - associated tumors ( 40% ) had an msi - h tumor phenotypetwo were msi - i and one was mss ( table 4 )  . 
her tumor had 46 somatic mutations , including dual mlh1 mutations , possibly driving the msi phenotype . discussion although next - generation sequencing has facilitated the widespread adoption of multigene panel germline testing , its clinical utility remains unclear.17 , 18 studies of unselected patients with colorectal , 19 ovarian , 20 and breast cancers21 have helped dene the range and prevalence of germline pathogenic cancer predisposition genes in these diseases . in addition , with broader genetic testing of patients with cancer , it has become evident that cancer stage may inuence the prevalence of germline mutations . 
for example , dna repair gene mutations are enriched in advanced - stage prostate cancer.8 conversely , early - stage colon cancer is enriched for germline mutations in the mmr genes.22 data regarding the spectrum of inherited risk in ec remains table 3 . 
 ( * ) biopsy at outside hospital ; no tumor remaining at hysterectomy . limited ; only one prior study5 has explored the role of germline multigene panel testing in a clinical cohort of patients with ec , testing for 25 genes using banked samples . 
ls mutations were identied in 6% of patients with ec , and another 3% had mutations in other genes . this 6% ls prevalence is on the upper end of what might be expected , with 2% to 6% reported in the literature and a generally accepted rate of approximately 3% , 23 - 27 raising the possibility of an ascertainment bias in the banked samples that were analyzed.5 applying a broad gene panel , analyses of selected patients with ec from tcga suggested that 16% of patients with ec harbor cancer predisposition mutations.28 we sought to determine the prevalence of cancer germline predisposition mutations in an unselected real - world clinical cohort of newly diagnosed patients with ec presenting for hysterectomy by using a large research multigene panel test . 
this reects the experience with traditional polymerase chain reactionbased msi testing in which lsassociated ecs have a lower proportion of unstable markers per tumor compared with colon cancer.34 in addition , unlike next - generation sequencingbased msi analysis , ihc testing is not vulnerable to low tumor purity . patients with brca mutations may be at increased risk of developing ec , although data are conicting and confounded by tamoxifen use.28 , 35 potential ec risk has important implications for counseling , because these women routinely undergo rrso without hysterectomy . 
similar to prior data , the patient with a brca mutation in our study had a high - grade ec.28 , 35 her tumor demonstrated loh at brca1 , suggesting the contribution of the brca1 mutation to development of ec . 
although a discussion of potential ec risk with brca mutation carriers undergoing rrso is reasonable , routine hysterectomy in this population is not currently warranted . smarca4 germline mutations result in rhabdoid tumor predisposition syndrome type 2 , an autosomal dominant cancer syndrome associated with aggressive soft tissue rhabdoid tumors , commonly in the brain ( atypical teratoid / rhabdoid tumors )  . 
for women , germline smarca4 mutations are associated with small cell carcinoma of the ovary , hypercalcemic type ; however , association with ec is unknown.36 median age at presentation is in the 20s ; no patients older than age 60 years have been reported.36 , 37 interestingly , ihc loss was demonstrated in our patient with ec and germline smarca4 mutation , raising the possibility that the mutation had a role in tumor development . the majority ( 71% ) of identied germline mutations were in lowor moderate - penetrance or autosomal recessive - only genes and most likely represent incidental ndings . 
given our relatively young population , of whom the majority had curable stage i cancer , the identication of incidental germline mutations may have signicant clinical implications for future risk reduction and identication of atrisk family members . although a number of these patients met current nccn criteria for brca testing , 38 the majority did not have prior breast or ovarian cancer gene testing . 
nationally reported rates of genetic testing are poor ; less than a third of eligible patients with breast cancer and 15% of patients with ovarian cancer have discussions about genetic testing.39 we have shown that genetic testing is acceptable to newly diagnosed ec patients if they are approached and offered testing . atm is not known to be associated with ec . 
although somatic pole mutations are relatively common , it is not clear that germline mutations predispose to ec.52 germline pold1 mutations have been associated with ec , but they are rare.52 in conclusion , we report a pilot study of large multigene panel germline testing for patients with newly diagnosed ec presenting for surgery . 
although our study is limited by a small sample size , predominantly white cohort , and overrepresentation of ashkenazi jewish heritage , it reects a prospective unselected cohort of patients with earlystage ec . we demonstrated the feasibility , acceptability , and yield of multigene germline testing in unselected patients with early - stage ec , and we found that the 3% incidence of ls in our study is comparable to that in the literature . 
cadoo , md , memorial sloan kettering cancer center , 300 east 66th st , 13th floor , new york , ny 10065 ; e - mail : cadook@mskcc.org. support supported in part by the romeo milio lynch syndrome foundation , the robert and kate niehaus center for inherited cancer genomics , the marie - jos ee and henry r . 
cadoo research funding : astrazeneca ( inst ) , syndax pharmaceuticals ( inst ) travel , accommodations , expenses : astrazeneca semanti mukherjee employment : regeneron pharmaceuticals stock and other ownership interests : regeneron pharmaceuticals research funding : regeneron pharmaceuticals dennis s . 
chi leadership : csurgeries stock and other ownership interests : bovie medical , verthermia , intuitive surgical , transenterix consulting or advisory role : bovie medical , verthermia elizabeth l . 
leitao jr honoraria : intuitive surgical research funding : kci travel , accommodations , expenses : intuitive surgical kara long roche travel , accommodations , expenses : intuitive surgical yukio sonoda patents , royalties , other intellectual property : patent pending for a surgical instrument ( uterine manipulator ) maria i . 
berger consulting or advisory role : roche research funding : illumina references david hyman consulting or advisory role : atara biotherapeutics , chugai pharmaceutical , cytomx therapeutics , boehringer ingelheim , astrazeneca , pzer , bayer , genentech research funding : astrazeneca , puma biotechnology , loxo oncology travel , accommodations , expenses : genentech , chugai pharmaceutical liying zhang employment : shanghai genome center ( i ) leadership : shanghai genome center ( i ) honoraria : future technology research travel , accommodations , expenses : shanghai genome center ( i ) , roche diagnostics asia pacic mark e . 
robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca , merck , pzer research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca carol aghajanian consulting or advisory role : clovis oncology , tesaro , mateon therapeutics , immunogen research funding : genentech ( inst ) , abbvie ( inst ) , clovis oncology ( inst ) , astrazeneca ( inst ) nadeem r . 
abu - rustum honoraria : prime oncology research funding : stryker / novadaq ( inst ) , olympus ( inst ) , grail ( inst ) travel , accommodations , expenses : prime oncology zsoa stadler allergan ( i ) , genentech ( i ) , regeneron pharmaceuticals ( i ) , optos ( i ) , adverum biotechnologies ( i ) , biomarin pharmaceuticals ( i ) , alimera sciences ( i ) , novartis ( i ) , spark therapeutics ( i ) , fortress biotech ( i ) , regenxbio ( i ) no other potential conicts of interest were reported . siegel rl , miller kd , jemal a : cancer statistics , 2017 . 
ca cancer j clin 67 : 7 - 30 , 2017 bruegl as , djordjevic b , batte b , et al : evaluation of clinical criteria for the identication of lynch syndrome among unselected patients with endometrial cancer . cancer prev res ( phila ) 7 : 686 - 697 , 2014 lu kh , dinh m , kohlmann w , et al : gynecologic cancer as a sentinel cancer for women with hereditary nonpolyposis colorectal cancer syndrome . 
obstet gynecol 105 : 569 - 574 , 2005 bruegl as , kernberg a , broaddus rr : importance of pcr - based tumor testing in the evaluation of lynch syndrome - associated endometrial cancer . 
adv anat pathol 24 : 372 - 378 , 2017 ring kl , bruegl as , allen ba , et al : germline multi - gene hereditary cancer panel testing in an unselected endometrial cancer cohort . 
mod pathol 29 : 1381 - 1389 , 2016 cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
j mol diagn 17 : 251 - 264 , 2015 zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
jama 318 : 825 - 835 , 2017 richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
hampel h , bennett rl , buchanan a , et al : a practice guideline from the american college of medical genetics and genomics and the national society of genetic counselors : referral indications for cancer predisposition assessment . 
weitzel jn , blazer kr , macdonald dj , et al : genetics , genomics , and cancer risk assessment : state of the art and future directions in the era of personalized medicine . 
domchek sm , bradbury a , garber je , et al : multiplex genetic testing for cancer susceptibility : out on the high wire without a net ? j clin oncol 31 : 1267 - 1270 , 18 . 
tung n , lin nu , kidd j , et al : frequency of germline mutations in 25 cancer susceptibility genes in a sequential series of patients with breast cancer . 
pearlman r , frankel wl , swanson b , et al : prevalence and spectrum of germline cancer susceptibility gene mutations among patients with early - onset j clin oncol 29 : 3008 - 3015 , 2011 oncol 34 : 1460 - 1468 , 2016 colorectal cancer . 
ferguson se , aronson m , pollett a , et al : performance characteristics of screening strategies for lynch syndrome in unselected women with newly diagnosed endometrial cancer who have undergone universal germline mutation testing . 
buchanan dd , tan yy , walsh md , et al : tumor mismatch repair immunohistochemistry and dna mlh1 methylation testing of patients with endometrial cancer diagnosed at age younger than 60 years optimizes triage for population - level germline mismatch repair gene mutation testing . 
ryan naj , morris j , green k , et al : association of mismatch repair mutation with age at cancer onset in lynch syndrome : implications for stratied surveillance netw 15 : 1465 - 1475 , 2017 instability . 
cosgrove cm , cohn de , hampel h , et al : epigenetic silencing of mlh1 in endometrial cancers is associated with larger tumor volume , increased rate of lymph node positivity and reduced recurrence - free survival . 
haraldsdottir s , hampel h , tomsic j , et al : colon and endometrial cancers with mismatch repair deciency can arise from somatic , rather than germline , mutations . 
abida w , armenia j , gopalan a , et al : prospective genomic proling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making . 
balmaa j , digiovanni l , gaddam p , et al : conicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
chek2 breast cancer case - control consortium : chek2 * 1100delc and susceptibility to breast cancer : a collaborative analysis involving 10 , 860 breast cancer cases and 9 , 065 controls from 10 studies . 
weischer m , nordestgaard bg , pharoah p , et al : chek2 * 1100delc heterozygosity in women with breast cancer associated with early death , breast cancerspecic death , and increased risk of a second breast cancer . 
stoffel em , mangu pb , gruber sb , et al : hereditary colorectal cancer syndromes : american society of clinical oncology clinical practice guideline endorsement of the familial risk - colorectal cancer : european society for medical oncology clinical practice guidelines . 
edwards jg , feldman g , goldberg j , et al : expanded carrier screening in reproductive medicine : points to considera joint statement of the american college of medical genetics and genomics , american college of obstetricians and gynecologists , national society of genetic counselors , perinatal quality foundation , and society for maternal - fetal medicine . 
bellido f , pineda m , aiza g , et al : pole and pold1 mutations in 529 kindred with familial colorectal cancer and / or polyposis : review of reported cases and recommendations for genetic testing and surveillance . 
egfr tyrosine kinase inhibitors ( tkis ) markedly increase progression - free survival in advanced disease.17 , 18 this discovery opened a new era of precision medicine leading to accelerated development and subsequent approval of drugs for several actionable genomic alterations in nsclc . 
while the molecular proling of nsclc is considered a standard of care in the advanced setting , the utility of molecular testing and targeted therapies in the adjuvant setting in early - stage nsclc has yet to be established . 
the br19 trial compared getinib versus placebo in a similar population.21 the trial closed prematurely after results of another trial showed detrimental effect of getinib after chemoradiation in stage iii nsclc.23 however , egfrmutant nsclc accounted for only 4% ( n = 15 ) of the patients . 
patients with resected stage ib - iiia ( american joint committee on cancer [ ajcc ] 7th edition ) adenocarcinoma with sensitizing egfr mutation were randomly assigned 1 : 1 to adjuvant osimertinib at the standard dose of 80 mg / d or matching placebo . 
random assignment was stratied by stage ( ib v ii v iiia ) , type of egfr mutation ( exon 19 del v l858r ) , and race ( asian v non - asian ) , but not based on receipt of adjuvant chemotherapy . 
patients received assigned treatment for a planned 3 - year duration or until disease recurrence , completion they met predetermined criteria for discontinuation . treatment , or if six - hundred eighty - two patients were randomly assigned to osimertinib ( n = 339 ) or placebo ( n = 343 )  . 
the published data are an unplanned interim analysis with the dfs data being only 33% mature ( 11% in osimertinib and 55% in placebo ) at the data cutoff date of january 17 , 2020 . 
similarly , dfs in the overall population ( including stage ib ) was also signicantly longer with a consistent benet seen across all predened subgroups ( age , smoking , race , stage , and type of egfr mutation )  . 
first , positron emission tomography - computed tomography ( pet - ct ) scan and brain mri were not mandated at screening in the study protocol.27 in the united states , pet - ct scan and brain mri are considered the standard of care for the complete staging of early - stage nsclc.28 data on proportion of patients with complete staging information ( pet - ct and brain mri ) in either arm are not available . 
in the adura trial , the median dfs and 2 - year dfs rate in the placebo arm are signicantly lower than those reported in historical trials , suggesting that suboptimal staging at baseline could have contributed to higher proportion of patients being understaged.29 , 30 compared to control arm , osimertinib showed an 82% reduction in risk for cns recurrence or death . 
however , this should be interpreted with caution , given limited follow - up and patients with occult intracranial metastatic disease missed on brain ct scans who get osimertinib are at an advantage because of potent cns activity . 
data regarding the recurrence rates adjusted by country or region of enrollment may be important as petct and brain mri are not readily available worldwide in resource - limited settings . second , about 40% of the patients did not get adjuvant chemotherapy . 
to accurately assess the benet of adjuvant osimertinib , adjuvant chemotherapy should have been offered to all patients in the control arm and not just left to the discretion of the attending physician . 
 commentary enrollment , port was considered a valid treatment option for resected stage iiia n2 disease . in retrospect , not allowing port and not mandating standard of care adjuvant chemotherapy with proven os benet among participants in the placebo arm may be more of an ethical consideration for patients and investigators rather than a confounding variable . 
in the adjuvant setting , in an asymptomatic context , daily treatment with osimertinib for up to 3 years can lead to considerable toxicity , especially if we consider that some patients have been already cured with surgery with or without adjuvant chemotherapy . in addition to some of the limitations mentioned above , several important aspects related to study outcomes remain to be dened . 
in the adjuvant setting , it is not known whether the 2 - year dfs superiority with egfr directed therapy will translate into an os benet with osimertinib . data from adjuvant / ctong 1104 trial suggest that the substantial dfs benet did not translate into os , a goldstandard measure of patient impact in the adjuvant setting . although pfs may be a reasonable surrogate for os in the metastatic setting , higher level of evidence is needed before advocating for dfs as a proxy for os benet in patients receiving adjuvant cancer therapies . 
unlike adaura , the alchemist trial is testing adjuvant egfrand alkdirected therapy using os as the primary end point . furthermore , it has been suggested that targeted therapies as cytostatic agents suppress micrometastatic disease progression , thereby delaying recurrence but not eliminating the disease completely . 
despite multiple studies across solid tumors , to our knowledge , imatinib is the only tki that has shown improved os when given in the adjuvant setting of high - risk gi stromal malignancies , 31 a disease with completely different molecular background compared with lung adenocarcinomas . 
of note , in the osimertinib arm of the adaura trial , about 15% of the patients who stopped the drug at 3 years experienced dfs event in the 6 - 9 months after drug discontinuation . 
this might suggest that recurrence - free survival is directly related to the length of drug exposure , and therefore adjuvant osimertinib might only delay recurrence and not cure the disease . 
in adaura , at the data cutoff , approximately 46% of patients in the placebo arm experienced disease reto know the post - protocol currence . treatment patterns , specically the proportion of patients in the placebo arm who received osimertinib at progression . if this percentage is lower than expected , then the dfs benet seen in adaura might only reect the suboptimal treatment of control arm upon progression . 
if similar it will be critical os can be achieved in the placebo arm with osimertinib treatment on recurrence , one can speculate that osimertinib has minimal effect on the natural history of the disease and is only delaying the inevitable relapsed disease . 
one can anticipate that having a nonngsbased molecular testing at the time of initial detection of the egfr mutation will make it hard to tease out the acquired , potentially actionable mechanisms of resistance at the dfs event . 
furthermore , development of acquired resistance mechanisms at relapse on osimertinib in the adjuvant setting could result in these patients missing the window of opportunity to receive osimertinib in the metastatic setting . robust biomarkers to predict durable clinical benet to adjuvant therapy are lacking . 
thus , it might not be as cost - effective to justify the use of osimertinib in the absence of an os benet , an issue that is contentious but is an important consideration from a societal healthcare perspective . 
furthermore , a proportion of patients who are probably cured of lung cancer with surgery alone may have unnecessary exposure to osimertinib and its toxicities with added hospitalizations . lowand middle - income countries might be affected the most because of lack of access to testing and drugs , as well as prohibitive costs . 
assessment of the quality of life ( qol ) while on therapy and beyond will also be a crucial parameter to consider the overall benet of treatment . in conclusion , os is the most important and clinically meaningful end point in the adjuvant setting . 
given the lack of evidence to demonstrate dfs as a validated surrogate end point with targeted therapy in the adjuvant setting , mature os data are recommended before a denitive statement on adjuvant osimertinib in egfr - mutant nsclc . we also worry that wide adoption of adura in the community might lead to lower use of adjuvant chemotherapy in favor of osimertinib . 
with the idmc decision to unblind and terminate the study early based on the perceived dfs benet , we might never know whether adjuvant osimertinib leads to a superior os versus treatment with osimertinib upon rst evidence of relapse . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . sonam puri consulting or advisory role : astrazeneca rodrigo dienstmann consulting or advisory role : roche , boehringer ingelheim speakers bureau : roche , ipsen , sano , msd oncology , servier , amgen research funding : merck no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2020 . 
ca cancer j clin 70 : 7 - 30 , 2020 besse b , le chevalier t : developments in the treatment of early nsclc : when to use chemotherapy . 
ann thorac surg 83 : 409 - 418 , 2007 pignon jp , tribodet h , scagliotti gv , et al : lung adjuvant cisplatin evaluation : a pooled analysis by the lace collaborative group . 
j clin oncol 26 : 3552 - 3559 , 2008 kris mg , gaspar le , chaft je , et al : adjuvant systemic therapy and adjuvant radiation therapy for stage i to iiia completely resected non - small - cell lung cancers : american society of clinical oncology / cancer care ontario clinical practice guideline update . 
j clin oncol 35 : 2960 - 2974 , 2017 arriagada r , auperin a , burdett s , et al : adjuvant chemotherapy , with or without postoperative radiotherapy , in operable non - small - cell lung cancer : two metaanalyses of individual patient data . 
lancet 375 : 1267 - 1277 , 2010 strauss gm , herndon je , maddaus ma , et al : adjuvant paclitaxel plus carboplatin compared with observation in stage ib non - small - cell lung cancer : calgb 9633 with the cancer and leukemia group b , radiation therapy oncology group , and north central cancer treatment group study groups . 
j clin oncol 26 : 5043 - 5051 , 2008 burdett s , rydzewska l , tierney jf , et al : a closer look at the effects of postoperative radiotherapy by stage and nodal status : updated results of an individual participant data meta - analysis in non - small - cell lung cancer . 
lung cancer 80 : 350 - 352 , 2013 burdett s , stewart l : postoperative radiotherapy in non - small - cell lung cancer : update of an individual patient data meta - analysis . 
robinson cg , patel ap , bradley jd , et al : postoperative radiotherapy for pathologic n2 non - small - cell lung cancer treated with adjuvant chemotherapy : a review of the national cancer data base . 
mikell jl , gillespie tw , hall wa , et al : postoperative radiotherapy is associated with better survival in non - small cell lung cancer with involved n2 lymph nodes : results of an analysis of the national cancer data base . 
corso cd , rutter ce , wilson ld , et al : re - evaluation of the role of postoperative radiotherapy and the impact of radiation dose for non - small - cell lung cancer using the national cancer database . 
fukuoka m , wu yl , thongprasert s , et al : biomarker analyses and nal overall survival results from a phase iii , randomized , open - label , rst - line study of getinib versus carboplatin / paclitaxel in clinically selected patients with advanced non - small - cell lung cancer in asia ( ipass ) , j clin oncol 29 : 2866 - 2874 , 2011 inoue a , kobayashi k , maemondo m , et al : updated overall survival results from a randomized phase iii trial comparing getinib with carboplatin - paclitaxel for chemo - nave non - small cell lung cancer with sensitive egfr gene mutations ( nej002 )  . 
zhong wz , wang q , mao wm , et al : getinib versus vinorelbine plus cisplatin as adjuvant treatment for stage ii - iiia ( n1 - n2 ) egfr - mutant nsclc ( adjuvant / ctong1104 ) : a randomised , open - label , phase 3 study . 
kelly k , altorki nk , eberhardt wee , et al : adjuvant erlotinib versus placebo in patients with stage ib - iiia nonsmall - cell lung cancer ( radiant ) : a randomized , double - blind , phase iii trial . 
wu yl , zhong w , wang q , et al : ctong1104 : adjuvant getinib versus chemotherapy for resected n1 - n2 nsclc with egfr mutationnal overall survival analysis of the randomized phase iii trial 1 analysis of the randomized phase iii trial . 
douillard jy , rosell r , de lena m , et al : adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ib - iiia non - small - cell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
arriagada r , de radiomedic - ina i , santiago c , et al : cisplatin - based adjuvant chemotherapy in patients with completely resected nonsmall - cell lung cancer . n engl j med 350 : 351 - 360 , 2004 joensuu h , eriksson m , sundby hall k , et al : survival outcomes associated with 3 years vs 1 year of adjuvant imatinib for patients with high - risk gastrointestinal stromal tumors : an analysis of a randomized clinical trial after 10 - year follow - up . 
abbosh c , frankell a , garnett a , et al : phylogenetic tracking and minimal residual disease detection using ctdna in early - stage nsclc : a lung tracerx study . cancer res 80 , 2020 ( suppl ; abstr ct023 ) 36 . 
li n , ou w , ye x , et al : pemetrexed - carboplatin adjuvant chemotherapy with or without getinib in resected stage iiia - n2 non - small cell lung cancer harbouring egfr mutations : a randomized , phase ii study . 
zhong wz , chen kn , chen c , et al : erlotinib versus gemcitabine plus cisplatin as neoadjuvant treatment of stage iiia - n2 egfr - mutant non - small - cell lung cancer ( emerging - ctong 1103 ) : a randomized phase ii study . 
pennell na , neal jw , chaft je , et al : select : a phase ii trial of adjuvant erlotinib in patients with resected epidermal growth factor receptor - mutant non - smallcell lung cancer . 
 comparative analysis of public knowledge bases for precision oncology steffen pallarz , phd1 ; manuela benary , phd1 , 2 ; mario lamping , md2 ; damian rieke , md2 , 3 ; johannes starlinger , md2 ; christine sers , phd2 , 4 ; david luis wiegandt1 ; marc seibert1 ; jurica seva , phd1 ; reinhold sch afer , phd2 , 4 ; ulrich keilholz , md2 ; and ulf leser , phd1 purpose precision oncology depends on the availability of up - to - date , comprehensive , and accurate information about associations between genetic variants and therapeutic options . 
we performed a quantitative and qualitative comparison of clinical interpretations of variants in cancer , oncokb , cancer gene census , database of curated mutations , cgi biomarkers ( the cancer genome interpreter biomarker database ) , tumor alterations relevant for genomics - driven therapy , and the precision medicine knowledge base . methods we downloaded each kb and restructured their content to describe variants , genes , drugs , and genedrug associations in a common format . 
for the analysis of clinically relevant gene - drug associations , we obtained lists of genes affected by genetic alterations and putative drug therapies for 113 patients with cancer whose cases were presented at the molecular tumor board ( mtb ) of the charit e comprehensive cancer center . results our analysis revealed that the kbs are largely overlapping but also that each source harbors a notable amount of unique information . 
the relative importance of a kb in terms of cancer genes was assessed in more detail by logistic regression , which revealed that all but one source had a notable impact on result quality . 
we conrmed these ndings using a second data set obtained from an independent mtb . conclusion to date , none of the existing publicly available kbs on gene - drug associations in precision oncology fully subsumes the others , but all of them exhibit specic strengths and weaknesses . 
2019 by american society of clinical oncology introduction precision oncology ( po ) is based on the molecular characterization of tumors and the integration of these data into clinical decision making.1 molecular characterizations typically are based on the identication of genomic variants by genomic sequencing , which results in patient - specic variant proles of single nucleotide variants , small insertions or deletions , copy number variations , and gene fusion load of the events . 
this bottleneck of clinical interpretation in po currently is based mostly on manual work and still lacks standardization.2 clinical variant interpretation must be based on published information.3 however , such information currently is dispersed across a number of databases , repositories , and web sites . 
 pallarz et al context key objective several knowledge bases that support the clinical evaluation of genetic variants in patients with cancer have emerged during the past years , but their mutual overlaps and extents are unknown . knowledge generated we compared seven knowledge bases and found that they share information only to a moderate extent and that they altogether lack important data . 
also , none of the knowledge bases is clearly more comprehensive than the others . relevance the creation of structured and easy - to - use knowledge bases to support precision oncology has made notable progress in the past years , yet the current systems remain incomplete and inhomogeneous . 
our results underline the necessity that , to obtain comprehensive information , oncologists must interrogate multiple knowledge bases and search relevant literature directly . we compared these kbs by measuring their mutual overlap of genes , drugs , and gene - drug associations and , if possible , by comparing each kbs content to actual treatment recommendations for 113 patients with cancer whose cases were discussed at the molecular tumor board ( mtb ) of the charit e comprehensive cancer center . 
results were conrmed using a second , independent set of recommendations for 10 patients with cancer . methods we performed pubmed searches and expert interviews to obtain a list of seven publicly available knowledge bases that aim at supporting medical decision making in precision oncology ( po - kb ) by providing structured information regarding the relationship between genes , variants , cancer entities , and therapies . 
specically , we used ( 1 ) civic ( clinical interpretations of variants in cancer ) , ( 2 ) oncokb , ( 3 ) cgc ( cancer gene census ) , ( 4 ) docm ( database of curated mutations ) , ( 5 ) cgi biomarkers ( the cancer genome interpreter biomarker database ) , ( 6 ) target ( tumor alterations relevant for genomics - driven therapy ) , and ( 7 ) pmkb ( the precision medicine knowledge base )  . 
the technical data integration procedure and normalization methods we developed for genes , variants , and drugs can be found in the data supplement . overlap comparison for a quantitative comparison , we computed the mutual overlap of all sources with regard to the set of genes , variants , drugs , and gene - drug associations they contain and visualized them using upset diagrams.12 for clustering of po - kbs , we rst computed pairwise distances using jaccards formula for set similarity and then applied hierarchical clustering ( data supplement )  . comparison of clinically relevant gene - drug associations we compared the content of each po - kb alone and in combinations versus recommendations of the charit e comprehensive cancer centers mtb ( n = 113 patient cases ) , at which results of comprehensive molecular table 1 . 
diagrams show the overlap between different precision oncology knowledge bases ( po - kbs ; identied by colors ) the matrices in the lower panels indicate po - kbs involved in an intersection , and the bar plots show the number of elements in this intersection . 
cgi , cgi biomarkers ( the cancer genome interpreter biomarker database ) ; civic , clinical interpretations of variants in cancer ; db , database ; docm , database of curated mutations ; pmkb , precision medicine knowledge base ; target , tumor alterations relevant for genomics - driven therapy . analysis ( whole - exome or panel sequencing , rna sequencing , immunohistochemical validations ) from patients with advanced cancer are discussed on a weekly basis . clinical interpretation of molecular alterations in the mtb is performed by a trained physician3 , 13 ; the data supplement contains details on this process . 
we measured the overlap between this reference set and different combinations of po - kbs for each patient using the metrics precision ( percentage of associations of a [ set of ] po - kb that is also contained in the reference ) , recall ( percentage of associations in the reference that is also contained in a [ set of ] po - kb ) and f1 measure ( harmonic mean between precision and recall )  . 
these measures are visually displayed later in the results , and more details can be found in the data supplement . to assess the predictive power of the different po - kbs , we proceeded as follows : for each association present in any of the po - kbs , a vector representation was constructed to encode its coverage by civic , cgi biomarkers , target , and oncokb , respectively . 
every gene - drug association that also was listed in the mtb associations was considered positive ( association relevant ; n = 345 cases ) , and all others were considered negative ( association not relevant ; n = 808 cases )  . 
 ( a ) percentage of patients for which any gene - drug associations were found when their presence was required in one to four po - kbs ( y - axis )  . 
each dot represents one patient , and only patients for whom at least one gene - drug association had been found were used . a 10 - fold cross - validation scheme to compute the out - ofsample error . 
eventually , a new model was trained on the entire training set to take this error into account ( using r package caret ) ; we report the results of the second model when applied on the test set . to validate our ndings , we used a second data set , which described treatment recommendations for patients with cancer , as derived at the molecularly aided stratication for tumor eradication ( masters ) 14 program at the national center for tumor diseases in heidelberg ( n = 10 ) and obtained from perera - bel et al.15 the normalization of gene and drug names for both data sets is described in the data supplement . 
to make results comparable to our rst data set , we removed all affected genes for which we did not have a single association in any of the po - kbs or for which no drug recommendation had been provided . 
to compensate for the positive bias in this set , we then added twice the number of genes chosen randomly from those we removed before . results overlap of studied kbs we downloaded and normalized seven publicly available databases that aim to support clinical decision making in po . we found that all databases overlap to a certain degree in the information they provide but also that each provided unique information . 
civic ( n = 89 genes ) and oncokb ( n = 86 genes ) have the second largest number of unique genes not mentioned in any other po - kb ; 49 genes were contained in all seven databases . 
the data supplement shows a hierarchical clustering of po - kbs on the basis of their overlaps in genes , variants , and gene - drug associations . although civic , oncokb , and pmkb share a highly similar goal and creation process and also obtain their data from the same origin ( scientic publications ) , each of them contains a substantial amount of unique genes . 
the most probable reason for this observation is that all po - kbs are small compared with the huge amounts of published data . the data supplement lists all genes contained in one or more of the databases . 
in addition , the four sources that contain drug information provide both shared and unique information ( fig 1b ) : 17 drugs are mentioned in all sources , and civic has the largest number of unique drugs ( n = 223 )  . 
similarly , civic shows the largest number of unique gene - drug associations ( n = 698 ; fig 1c )  . comparison of clinically relevant gene - drug associations we next compared the content of each po - kb and combinations thereof versus expert considerations for the 113 patients discussed at the charit e mtb at the level of genedrug associations . 
the number of drugs is high , because , for the analysis , drug classes ( eg , mammalian target of rapamycin inhibitors ) were expanded to all drugs of the respective class to match the granularity of information in different data sets . 
we analyzed which patients for whom the associations presented to the mtb also were contained in different po - kbs ( fig 2 ) and which fractions of gene - drug associations presented in the mtbs also would be found by specic combinations of po - kbs ( fig 3 )  . overall , the mtb discussed 203 different genes and 245 different drugs , of which 152 and 176 , respectively , were found in at least one po - kb . 
this implies that 25% of genes and 28% of drugs discussed in the mtb could not be found by our software in any of the po - kbs we considered . 
next , we computed the set of prioritized genes per patient and checked for how many of those had associations with drugs in at least one , two , three , or four po - kbs . 
 comparison of knowledge bases for precision oncology precision true positives ( tp ) false negatives ( fn ) recall false positives ( tn ) true negatives ( tn ) in po - kbs precision recall no . 
 ( b ) median precision ( blue ) , recall ( red ) and f1 ( harmonic mean between precision and recall ) score ( gray ) when considering an increasing number of precision oncology knowledge bases ( po - kbs ) to support gene - drug associations discussed by the molecular tumor board ( mtb ) experts . 
 ( c ) precision and ( d ) recall obtained by using different combination of po - kbs as boxplots ( median , 25th and 75th percentiles ; whiskers extend to the maximum values within 1.5 the interquartile range ; dots represent outliers )  . 
cgi , cgi biomarkers ( the cancer genome interpreter biomarker database ) ; civic , clinical interpretations of variants in cancer ; pr , precision and recall ; target , tumor alterations relevant for genomics - driven therapy . gene - drug association , the number of patients decreases to 42 . 
figure 2b shows that the number of potential suggestions per patient drops sharply with the required number of supporting po - kbs : when support by any two po - kbs was required , we obtained a median of ve associations per patient . 
the median increased to 12 if only one po - kb was required and decreased to two for three po - kbs and zero for four po - kbs . next , we considered the mtb associations as reference and the contents of the four po - kbs that contained genedrug associations as predictors . 
when the mtb reference gene - drug association was required to be contained in only one po - kbsthat is , the union of all po - kbs was used as predictorthe median recall for all patients reached approximately 46% ( fig 3b , blue line ) , whereas the median precision was low because of the large number of associations found in the po - kbs that were not discussed in the mtb ( fig 3b , orange line ; data supplement contains evaluation metrics )  . 
intuitively , this means that searching in more than one po - kb in our evaluation always led to nding more relevant data but at the cost of also nding more data that are irrelevant for the concrete patient according to the mtb . finally , we trained a logistic regression classier on evidence from all po - kbs using mtb associations as ground truth . 
on our withheld test set ( n = 288 gene - drug associations ) , this model reached an f1 score of 43% ( precision , 64% ; recall , 33% )  . 
on the nct data set , this model reached a precision of 100% at a recall of 38% , which resulted in a higher f1 score of 56% . the data supplement contains an interactive html page with the complete list of gene - drug associations of the berlin and the heidelberg data sets together with the information about which of the po - kbs contains which reference associations . discussion we performed a quantitative and qualitative comparison of the current content ( february 2019 ) of seven knowledge bases specialized in po . 
our results indicate that the pokbs have partly overlapping and partly unique results . compared with associations discussed for 113 patients in an mtb of a comprehensive cancer center at a university clinic , we found that po - kbs contain relevant information not present in any of the others . 
however , we also want to point out some limitations of our work that warrant additional studies . even after careful normalization of gene and drug names in all po - kbs ( data supplement ) , 809 of the 1 , 154 gene - drug associations of the mtb data set were not found in any of the po - kbs . 
possible reasons for their absence are that these genes are simply not yet curated , are grossly misspelled , or designate gene families rather than individual genes and so could not be matched by our normalization procedure . 
similarly , 157 associations with 69 unique drugs were not found because these drugs are not contained in any of the kbs ; 383 associations were missing because none of the po - kbs reported this particular association , although both the genes and the drugs were found in principle . our analysis showed that civic has the highest recall and f1 score compared with mtb associations when data from only one po - kb are considered ( ie , no combinations were allowed )  . 
these submissions could be the reason for the higher recall of po - kb combinations contained in civic ( fig 3d ) ; however , civic also simply contains the highest number of gene - drug associations among all po - kbs considered , which also positively inuences recall . 
separation of these two effects is difcult , but we note that regression results on the heidelberg data set , for which no bias toward civic exists , are even better than for the mtb data set . 
on both data sets , removal of civic from the training data left the precision of the learned model unchanged but induced a notable decrease in recall ( mtb , 33% decreased to 19% ; heidelberg , 38% decreased to 21% ) and , thus , in the f1 score ( mtb , 43% decreased to 29% ; heidelberg , 56% decreased to 35% )  . 
the fact that the decrease in recall was comparable in both data sets is an argument against a strong bias of the charit e mtb analysis toward civic ; the overall strong decrease originates from the large number of gene - drug associations only contained in civic . as reported , we trained a classier on combinations of the different po - kbs using the mtb associations as ground truth . 
however , we note that the reported results in terms of prediction accuracy cannot be considered as the ability to predict treatments in a clinical decision support setting for multiple reasons . 
second , we considered all associations in the mtb data as relevant without taking into account the nal decision of the mtb , which could be the recommendation of a single drug , could be a combination of drugs , or could disregard all discussed associations . 
fifth , the patient cases presented in the mtb represent a large variety of different tumor types , such as breast cancer , pancreatic cancer , leiomyosarcoma , ovarian cancer , liposarcoma , and neuroendocrine tumors ( data supplement )  . our analysis ignored the information on cancer types , because this level of detail frequently is missing in the po - kbs and , when present , uses a highly idiosyncratic nomenclature . 
note that analysis of recommendations derived from genomic information across different cancer types is commonplace in current studies about po.16 , 17 in conclusion , we here report a quantitative and qualitative comparison of precision oncology knowledge databases . our analysis shows that each of the databases contains , besides a rather small common core , a relevant amount of unique information . 
when we compared po - kb contents with gene - drug associations discussed in two mtbs , we found that a considerable fraction of information indeed can be found in some po - kbs but also that many presumably clinically relevant associations are not yet contained in any of them and that relevant information often is dispersed across different po - kbs . 
n engl j med 372 : 793 - 795 , 2015 good bm , ainscough bj , mcmichael jf , et al : organizing knowledge to enable personalization of medicine in cancer . 
nat rev cancer 4 : 177 - 183 , 2004 van allen em , wagle n , stojanov p , et al : whole - exome sequencing and clinical interpretation of formalin - xed , parafn - embedded tumor samples to guide precision cancer medicine . 
rieke dt , lamping m , klauschen f , et al : efcacy of a structured workow for the interpretation of comprehensive genomic analysis data in clinical routine . j clin oncol 36 , 2018 ( suppl ; abstr e24164 ) 14 . 
perera - bel j , hutter b , heining c , et al : from somatic variants towards precision oncology : evidence - driven reporting of treatment options in molecular tumor boards . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular proling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
massard c , michiels s , fert e c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . cancer discov 7 : 586 - 595 , 2017 18 . 
 postmortem somatic sequencing of tumors from patients with suspected lynch syndrome has clinical utility for surviving relatives introduction after a patient dies , the medical history stops unfolding and genetic evaluation typically ceases . 
 however , newer techniques may resolve uncertain diagnoses for patients and families , even years after a cancer diagnosis and including after the death of the affected individual . lynch syndrome is a highly penetrant , autosomal dominant , cancer predisposition syndrome caused by germline pathogenic variants in one of the following mismatch repair ( mmr ) genes : msh6 , msh2 , mlh1 , pms2 , or epcam . 
individuals with lynch syndrome have a high lifetime risk of cancer , including colorectal cancer ( crc ; risk range , 10% to 80% ) , endometrial cancer ( risk range , 16% to 60% ) , and others.1 clinical suggestion for lynch syndrome is subjectively based on personal and family history and objectively on tumor screening.2 - 6 tumor screening assesses mmr deficiency by identifying dna replication errors in microsatellite repeats ( microsatellite instability - high ) or by immunohistochemical ( ihc ) staining with decreased or absent expression in one or more mmr proteins.1 , 5 , 6 greater than 85% of lynch - associated tumors have a high level of microsatellite instability or abnormal findings by ihc staining.3 , 4 however , tumor screening is not diagnostic : 10% to 15% of sporadic crc tumors are also mmr deficient.2 , 4 , 7 , 8 screening of abnormal tumors should include assessment of sporadic causes of tumor mmr deficiency , including mlh1 hypermethylation or braf codon 600 mutations , and germline testing.1 , 5 , 8 , 9 probands with an mmr - deficient tumor but negative somatic or germline testing present a diagnostic and clinical management challenge.4 preventive recommendations for these individuals are not well defined and vary widely in practice.3 , 4 sequencing mmr - deficient tumors in individuals with unexplained , abnormal tumor screening is a powerful tool for refining the risk of lynch syndrome . 
probands personal and family histories and relevant information about the consultand characteristic consultand ; age , years probands age at diagnosis , years case a son ; 61 case b case c case d daughter ; 53 maternal first cousin ; 57 daughter ; 33 cancer site ( proband ) sigmoid colon sigmoid colon crc ; duodenal crc : 45 and 47 . 
maternal aunt : crc ( age , 53 years ) yes ; 2001 ( research , sequencing only ) ; negative ; and 2008 ; ( clinical , mlpa only ) ; negative uterus yes ; 2007 ; negative yes ; 2015 ; negative yes ; 2015 ; negative 5 fdr 4 fdr 3 fdr 3 fdr family history : lynchassociated cancer ( proband ) fulfilled amsterdam i criteria ( proband ) fulfilled revised bethesda criteria ( proband ) prior germline testing of proband ; year ; result no . 
of known relatives clinically affected by result insurance coverage no , self - pay obtained by consultand ? yes ( ministry of health , canada ) preauthorized , then denied . 
 appealed and approved at 50% coverage ( aetna ) yes ( blue cross federal ) abbreviations : crc , colorectal cancer ; fdr , first - degree relatives ; mlpa , multiplex ligationdependent probe amplification . improvement amendmentscertified university of washington genetics and solid tumors laboratory . 
coloseq tumor was ordered on behalf of a surviving relative to clarify an uncertain diagnosis of lynch syndrome and for an associated need for preventive surveillance and / or prophylactic surgery . 
table 1 describes the personal and family history of each proband and relevant information about the consultand . patient a was diagnosed with crc at age 78 years and died at age 82 years . 
the recommendation for early , high - risk surveillance for the consultands children was rescinded . patient b was diagnosed with colorectal cancer at age 82 years and died at age 87 years . 
coloseq tumor testing revealed two likely pathogenic somatic mutations in the tumor , msh2 c.1760 - 1g > a and msh2 p.c693r.16 the cancer surveillance plan was reassessed for the consultand and her siblings ; recommendation for colonoscopy was reduced to every 5 years . patient c was diagnosed with metachronous crc at ages 45 and 47 years and duodenal cancer at age 55 years . 
 considering prophylactic total hysterectomy with bso and currently await cascade testing results to guide this decision . patient d was diagnosed with endometrial cancer at age 58 years and died within a year . 
prophylactic hysterectomy and bso were no longer recommended for probands daughter . discussion clinical judgment often supports high - risk surveillance on the basis of an mmr - deficient tumor and / or personal and family history , even in the absence of a pathogenic germline variant . 
indeed , individuals with an mmr - deficient tumor and negative germline testing have a higher recurrence rate of crc compared with individuals with known sporadic cancer , leading to concern for a missed germline variant.4 , 7 , 8 despite universal tumor screening recommendations , compliance is inconsistent and may be preferentially performed with high clinical suspicion of lynch syndrome.17 , 18 preventive cancer screening carries cost and risk ; clarification of an uncertain diagnosis should be sought when clinically feasible.2 genetic testing is unique ; a result potentially provides information about a proband and relatives . 
however , surrogate testing is not equivalent to testing the affected person and carries its own risks.19 whenever possible , it is preferred to test the affected individual , even postmortem . genetic testing of deceased patients warrants special consideration and regulation.20 to our knowledge , this is the first report of clinical , postmortem , somatic sequencing used to actively change surviving relative management . 
 information considered ethical to disclose during a patients lifetime , such as imminent harm to identifiable individuals and / or potential benefit for at - risk individuals or public health , is considered ethical to disclose postmortem with the familys consent.20 resolving an uncertain but clinically suspected diagnosis of lynch syndrome falls within this paradigm . despite the clinical utility of resolving an uncertain diagnosis , several factors may hinder clinical uptake . 
patients may misunderstand the uncertainty of this result and erroneously believe they have lynch syndrome or not understand the results.20 coloseq tumor will likely only be offered if diagnosis is recognized as uncertain.5 , 21 , 22 next , test implementation requires significant genetic literacy , clinical judgment , and expertise that is not universally available.17 clinical pathology laboratories are required by the college of american pathologists to retain patient - tissue blocks for 10 years . 
last , insurance coverage for postmortem testing is challenging and , if denied , out - of - pocket cost is a deterrent.5 in this report , insurance coverage was obtained for three of four patients . 
these numbers are small and may reflect ascertainment bias of those who expected coverage or could self - pay . this case series has several important limitations , including comprising few cases and that patients receiving tumor screening may be a selected group , which could skew the high diagnostic rate and significant downstream benefits for surviving family members.18 nevertheless , this case series sufficiently demonstrates feasibility and clinical utility of resolving an uncertain lynch syndrome diagnosis in a deceased proband . in conclusion , postmortem paired tumor and germline sequencing is feasible , reliable , and offers a high diagnostic yield . 
lockwood administrative support : angela jacobson provision of study material or patients : angela jacobson , anna newlin , amanda hamblett , brian shirts , stephanie more , eric q . 
stanich patents , royalties , other intellectual property : i am an author for uptodate and receive royalties . stephanie more no relationship to disclose amanda hamblett stock and other ownership interests : edge therapeutics , achillion pharmaceuticals , cerecor , delcath systems , opko health , sonoma pharmaceuticals , sierra oncology , synthetic biologics , trevena , oncogenix , corbus pharmaceuticals , waveguide , osiris therapeutics , bristolmyers squibb , gilead sciences , cellectar biosciences , chimerix , contravir , stellar biotechnologies , innovate biopharmaceuticals , verastem jonathan f . 
tait stock and other ownership interests : merck ( i ) , amgen ( i ) , glaxosmithkline ( i ) research funding : evicore ( inst ) patents , royalties , other intellectual property : evicore copyrights ( inst ) brian shirts no relationship to disclose colin c . 
 stanich , ohio state university , columbus , oh ; stephanie more , sarah lawrence college , calgary , alberta , canada ; and amanda hamblett , middlesex hospital cancer center , middletown , ct . support supported by grant nih5t32gm007454 to h.m.b. 
weissman sm , burt r , church j , et al : identification of individuals at risk for lynch syndrome using targeted evaluations and genetic testing : national society of genetic counselors and the collaborative group of the americas on inherited colorectal cancer joint practice guideline . 
evaluation of genomic applications in practice and prevention ( egapp ) working group : recommendations from the egapp working group : genetic testing strategies in newly diagnosed individuals with colorectal cancer aimed at reducing morbidity and mortality from lynch syndrome in relatives . 
haraldsdottir s , hampel h , tomsic j , et al : colon and endometrial cancers with mismatch repair deficiency can arise from somatic , rather than germline , mutations . 
mensenkamp ar , vogelaar ip , van zelst - stams wa , et al : somatic mutations in mlh1 and msh2 are a frequent cause of mismatch - repair deficiency in lynch syndrome - like tumors . 
thompson ba , spurdle ab , plazzer jp , et al : application of a 5 - tiered scheme for standardized classification of 2 , 360 unique mismatch repair gene variants in the insight locus - specific database . 
beamer lc , grant ml , espenschied cr , et al : reflex immunohistochemistry and microsatellite instability testing of colorectal tumors for lynch syndrome among us cancer programs and follow - up of abnormal results . 
gallego cj , perez ml , burt a , et al : next generation sequencing in the clinic : a patterns of care study in a retrospective cohort of subjects referred to a genetic medicine clinic for suspected lynch syndrome . 
 breast and ovarian cancer penetrance estimates derived from germline multiple - gene sequencing results in women purpose multiple - gene , next - generation sequencing panels are increasingly used to assess hereditary cancer risks of patients with diverse personal and family cancer histories . 
the magnitude of breast and ovarian cancer risk associated with many clinically tested genes , and independent of family cancer history , remains to be quantified . methods we queried a commercial laboratory database of 95 , 561 women tested clinically for hereditary cancer risk with a 25 - gene ( apc , atm , bard1 , bmpr1a , brca1 , brca2 , brip1 , cdh1 , cdk4 , chek2 , mlh2 , msh2 , msh6 , mutyh , nbn , p14arf , p16 , palb2 , pms2 , pten , rad51c , rad51d , smad4 , stk11 , and tp53 ) next - generation sequencing panel . multivariable logistic regression models accounting for family history were used to examine the association between pathogenic mutations and breast or ovarian cancer . 
as a confirmatory approach , a matched case - control analysis was conducted , defining cases as patients with breast or ovarian cancer and controls as women without cancer . results one or more pathogenic mutations were detected in 6 , 775 ( 7% ) of 95 , 561 women . 
multivariable models and matched case - control analyses yielded similar results . conclusion among nearly 100 , 000 clinically tested women , 7% carried a pathogenic mutation in one or more cancer - associated genes . 
2017 by american society of clinical oncology introduction next - generation sequencing has dramatically expanded the scope and speed of genetic testing for hereditary cancer risk while simultaneously reducing cost.1 , 2 these advances are most evident in the approach to suspected hereditary breast and ovarian cancer ( hboc ) syndrome . 
this has begun to broaden our understanding of gene - specific phenotype , as mutations are found unexpectedly among patients with a cancer not thought to be associated with a particular gene.8 , 15 despite this progress , questions have arisen about the clinical validity and utility of multiple - gene panel testing . 
perhaps the greatest question pertains to the magnitude of cancer risk , or penetrance , associated with mutations in less widely tested genes included on many panels , such as allison w . 
questions regarding cancer risk have become especially pressing as decreasing costs have increased testing access for patients with a wider range of personal and family histories than previously required.16 with some exceptions , 17 - 19 studies estimating cancer risks have been small and underpowered , yielding imprecise estimates . 
this is problematic because our understanding of a patients cancer risk guides treatment recommendations for enhanced breast screening and preventive surgeries.20 - 24 for example , risk - reducing salpingo - oophorectomy is indicated with a mutation that confers a 10to 20fold increase over the average ovarian cancer risk ( an absolute risk of 20% to 40% ) , but may be excessive with a mutation causing only a two - fold elevation ( an absolute risk of 2% to 4% ) .20 penetrance estimates adjusted for family history represent the magnitude of risk that is independently genetic . 
adjusted penetrance may be estimated in an unbiased manner from clinical populations where factors related to ascertainment bias are well captured , and represent the magnitude of risk that is independently genetic.25 these adjusted penetrance estimates are applicable to women with no family history of cancer and may inform personalized assessments that combine genetic risks with environmental and lifestyle risk factors . with clinical uptake of multiple - gene panel testing increasing rapidly , cancer risk estimates that control for diverse family histories are urgently needed to inform genetic counseling . 
in this study , we analyzed a testing laboratorys data on germline sequencing with a 25 - gene panel in a large , real - world cohort using two complementary methods to determine novel estimates of mutation penetrance adjusted for family history . methods patients and hereditary cancer testing female patients who underwent testing with a 25gene hereditary cancer panel between september 2013 and september 2015 were evaluated . 
testing was performed at a clinical laboratory improvement amendments and college of american pathologyapproved laboratory ( myriad genetic laboratories ) for a panel of 25 genes ( apc , atm , bard1 , bmpr1a , brca1 , brca2 , brip1 , cdh1 , cdk4 , chek2 , mlh2 , msh2 , msh6 , mutyh , nbn , p14arf , p16 , palb2 , pms2 , pten , rad51c , rad51d , smad4 , stk11 , and tp53 ) .26 informed consent for clinical testing was obtained and clinical information was collected on the test requisition forms ( trfs )  . patient data were deidentified and no additional information was obtained from patients or providers . 
as such , this analysis was not subject to ethics board review . variants were classified using american college of medical genetics and genomics recommendations , with supporting linkage , biochemical , clinical , functional , and statistical data used for specific missense and intronic alterations.27 - 29 pathogenic variants are those that receive a laboratory classification of deleterious or suspected deleterious . 
classifications used in the analysis matched those reported clinically . clinical information from provider - completed trfs included ancestry , personal and family cancer history , cancer type ( s ) , and age ( s ) at diagnosis . patients were excluded from analysis if they had an incomplete trf , if they had testing using the 25gene panel after receiving negative test results from a single / limited gene panel , or if results suggested mosaicisno patient was excluded on the basis of race / ethnicity , age , or other characteristics . statistical methods all analyses were conducted using r version 3.0.2.30 two - sided p values are reported . 
given that we had prior hypotheses about the sequenced genes , no adjustments were made for multiple testing . we used two different statistical methods to quantify adjusted risks of invasive ductal carcinoma of the breast ( bc ) and invasive epithelial ovarian cancer ( oc ) associated with mutations in panel genes . 
for genes associated with childhood mortality ( eg , tp53 and stk11 ) , the penetrance estimates represent bc and oc risks among mutation carriers who survive to adulthood . multivariable logistic regression models for each gene , we constructed two multivariable models to estimate ( 1 ) bc risk and ( 2 ) oc risk . 
our hypothesis was that family histories may be over - reported among unaffected controls to meet insurance coverage criteria for genetic testing and / or under - reported among affected cases . 
using brca1 and palb2 as widely studied examples , we modified family histories by adding one fdr diagnosis of bc to cases and subtracting one fdr diagnosis from controls , selected uniformly at randorandom patient selections were repeated 1 , 000 times and results were reported as medians of 1 , 000 iterations . matched case - control analyses results cases were defined as female patients with a single diagnosis of bc or oc . 
cases and controls were matched 1 : 1 according to age ( 6 3 years ) , ancestry ( exact match ) , and family cancer history ( breast , ovarian , colon , uterine )  . 
p values , ors , and cis were calculated with the exact mcnemars test . mutation status , age , and ancestry were coded as for models ( data supplement )  . 
for tests of oc associations , we included an extra three - level matching variable for familial colon and uterine cancer : ( 1 ) at least one fdr with colon or uterine cancer before the age of 50 years ; ( 2 ) at least one fdr with colon or uterine cancer at the age of 50 years or older ; and ( 3 ) none of the above . sensitivity analysis age - specific cumulative bc risks on the basis of adjusted penetrance were compared with estimates for brca1 and brca2 on the basis of literature.31 - 35 cumulative risks were calculated according to the product - limit method , 36 with agespecific incidences estimated as the product of agespecific ors and general population incidences . age - specific ors were calculated by subsetting to the age categories reported by satagopan et al35 ( , 40 , 40 to 49 , and > 50 years ) , and were combined with age - specific seer37 incidence rates from 2009 to 2013 in 5 - year intervals . the magnitude of potential bias that could result from differential underor over - reporting of family we identified 95 , 561 eligible patients ( table 1 )  . 
this includes 2 , 771 mutations detected in 2 , 701 ( 10% ) bcaffected patients , and 715 mutations in 701 ( 14% ) oc - affectedpatients.overall , 3 , 007 ( 44% ) mutations were in brca1 / 2 and 3 , 768 ( 56% ) were in other genes . multivariable logistic regression models eight genes were significantly associated with bc : atm , bard1 , brca1 , brca2 , chek2 , palb2 , pten , and tp53 ( table 3 and fig 1 )  . 
as an exploratory analysis , we constructed a multivariable model ( as described in the methods section ) with lobular breast cancer as the dependent variable , which showed a strong association of cdh1 with lobular breast cancer ( table 3 )  . eleven genes were significantly associated with oc : atm , brca1 , brca2 , brip1 , mlh1 , msh6 , msh2 , nbn , rad51c , rad51d , and stk11 ( table 3 and fig 1 )  . matched case - control analyses overall , 19 , 056 patients were eligible as bc cases , 3 , 695 patients as oc cases , and 51 , 200 patients as cancer - free controls . 
we identified matched controls for 15 , 826 bc and 2 , 731 oc cases . risk estimates from matched case - control analyses and multivariable models were consistent ( table 3 , table 4 , and fig 1 )  . 
patient clinical characteristics age at hereditary cancer testing , years variable total patients * range median % < 50 ancestry western / northern european central / eastern european latin american / caribbean african native american asian ashkenazi near / middle eastern family cancer history no bc or oc 1 bc , no oc 1 oc , no bc > 2 bc , no oc > 2 oc , no bc > 2 bc or oc all patients no . 
accounting for family history resulted in a slightly lower adjusted bc risk compared with the unadjusted published estimates . we also investigated the impact of overor underreporting family cancer history for brca1 and palb2 . 
sensitivity analyses showed that risk estimates will be inflated if family history is overreported by controls and / or under - reported by cases , which would cause more severe cases to be matched to less severe controls . 
we used multivariable modeling and matched case - control approaches to estimate mutation penetrance for 25 cancer - associated genes , adjusting for age , race / ethnicity , and family cancer history . 
we did not observe increased bc risk with mutations in nbn , which was surprising because nbn is generally considered to be a moderate - penetrance breast cancer susceptibility gene.16 reports of bc risks associated with brip1 , rad51c , and rad51d mutations are mixed ; 38 , 39 our results suggest no greater than average risk . 
in addition , there have been some reports of increased bc incidence among individuals with mutations in the lynch syndrome genes msh6 and pms2 ; 40 - 43 however , our analysis showed no increased risk of bc for individuals with mutations in these genes . we found 11 genes significantly associated with increased oc risk : atm , brca1 , brca2 , brip1 , mlh1 , msh6 , msh2 , nbn , rad51c , rad51d , and stk11 . 
these results are consistent with prior studies of brca1 / 2 , brip1 , rad51c , and rad51d and the mismatch repair genes in oc susceptibility.17 , 43 - 52 for nbn , there has been prior speculation but no definite evidence of an oc association.50 to our knowledge , this is the first report of increased oc risk associated with a germline atm mutation . 
given estimates that as many as 1% of bc patients and 0.5% of the general population may carry an atm mutation , 53 - 55 with many having no family history of oc , defining their risk of developing oc is an urgent research priority . 
significant associations are in bold . abbreviation : na , not applicable . * no mutations were observed in cdk4 and analysis could not be performed . genes associated with increased risk of breast and ovarian cancer . genes associated with an increased risk of breast cancer only . genes associated with an increased risk of ovarian cancer only . kadditional analysis with analogous models to predict lobular breast cancer risk in cdh1 . with bard1 mutations , in contrast with some recent studies.56 the estimated oc risk calculated for palb2 was  . 
in light of a recent study reporting increased incidence of palb2 mutations in women with oc , 56 additional studies will be essential to understand the contribution of palb2 mutations to oc susceptibility . previous studies of bc and oc gene penetrance have used various designs , including kin cohort and case control.17 , 18 , 31 , 33 , 57 - 62 all study designs are subject to bias . 
odds ratios and 95% cis from multivariable logistic regression models ( blue ) and exact mcnemars tests ( gold ) of ( a ) breast cancer associations and ( b ) ovarian cancer associations . 
only genes with results from both models are shown . genes with a significant association with breast or ovarian cancer by multivariable regression are shown in bold . bard1 brca1 brca2 brip1 cdh1 cdkn2a ( p16 ) chek2 mlh1 msh2 msh6 mutyh palb2 pms2 rad51c rad51d tp53 cdkn2a ( p16 ) bard1 brca1 brca2 brip1 chek2 mlh1 msh6 palb2 pms2 rad51c rad51d odds ratio ( 95% ci ) 0.5 1 odds ratio ( 95% ci ) multivariable regression matched case / control ( exact mcnemar 's test ) result of more comprehensive sequencing of clinical samples . 
the clinical testing data set we used did not include related individuals ( required for kin - cohort analysis ) ; thus we used the two other penetrance study designs that are feasible with data of this kind , ie , multivariable logistic regression modeling and an analysis of cases matched to comparable controls from the same patient population.66 we controlled for ascertainment bias using standard methods for confounding variables , 25 which yielded adjusted ors that estimate the relative risk conferred by a gene mutation after accounting for family cancer history , race / ethnicity , and age . the concordant results of the two analytic methods we used ( logistic regression and matched case / control ) suggest that both adequately accounted for ascertainment bias . 
for example , patients with cancer often meet guidelines for genetic testing regardless of their family history ; thus it is possible that family history was reported less completely by ordering clinicians for cases than for controls ( who generally meet guidelines for insurance coverage of testing only because of their relatives cancer histories )  . 
significant associations are in bold . abbreviation : na , not applicable . * there were too few mutation carriers to generate an odds ratio for this gene . genes associated with increased risk of breast and ovarian cancer . genes associated with an increased risk of breast cancer only . genes associated with an increased risk of ovarian cancer only . the limitations of this study are balanced by its considerable strengths , most notably its size ( n = 95 , 561 ) and representation of patients who receive multiple - gene panel testing under the routine conditions of clinical practice . 
the results cannot replace controlled studies of mutation penetrance in unselected patients with bc , who lack early age at onset or strong family history ; such research will require analysis of population - based cohorts , which is underway . 
if confirmed , the current results may justify a case - by - case discussion of oc risk - reduction approaches with women who carry these mutations , considering family history as well as these genespecific risk estimates . because prophylactic surgery is invasive and irreversible , the burden of proof should be more stringent than for a screening intervention . 
if confirmed , the three - fold or greater oc risk estimates presented here for brip1 and rad51c / d would support their recent addition to guidelines criteria for risk - reducing salpingo - oophorectomy.20 however , the lower estimates of oc risk with atm and nbnareless clearly an indication for prophylactic in conclusion , we observed and quantified significant bc risks associated with eight genes and oc risks associated with 11 genes that are commonly sequenced on multiple - gene panels . 
kurian research funding : myriad genetics ( inst ) , invitae ( inst ) , ambry genetics ( inst ) , genomic health ( inst ) , genedx / bioreference ( inst ) ; genentech ( inst ) elisha hughes employment : myriad genetics stock and other ownership interests : myriad genetics elizabeth a . 
hall research funding : myriad genetics ( inst ) patents , royalties , other intellectual property : i share a patent with several fox chase investigators for a novel method to investigate hereditary colorectal cancer genes . 
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meijers - heijboer h , van den ouweland a , klijn j , et al : low - penetrance susceptibility to breast cancer due to chek2 ( * ) 1100delc in noncarriers of brca1 or brca2 mutations . 
evans dg , shenton a , woodward e , et al : penetrance estimates for brca1 and brca2 based on genetic testing in a clinical cancer genetics service setting : risks of breast / ovarian cancer quoted should reflect the cancer burden in the family . 
risch ha , mclaughlin jr , cole de , et al : population brca1 and brca2 mutation frequencies and cancer penetrances : a kin - cohort study in ontario , canada . 
song h , dicks e , ramus sj , et al : contribution of germline mutations in the rad51b , rad51c , and rad51d genes to ovarian cancer in the population . 
because poly ( adp - ribose ) polymerase inhibitors have significant activity in brca1 / 2 - mutant ovarian and breast cancers , rucapanc investigated the efficacy and safety of rucaparib in brca1 / 2 - mutant pancreatic cancer . patients and methods rucapanc enrolled patients with measurable locally advanced / metastatic pancreatic cancer who had received one to two prior chemotherapy regimens . 
four patients achieved a response ; two partial responses and one complete response ( cr ) were confirmed ( objective response rate , 15.8% ; 3 of 19 ) , with an additional cr unconfirmed . 
the disease control rate ( cr , partial response , or stable disease for 12 weeks ) was 31.6% ( 6 of 19 ) in all patients and 44.4% ( 4 of 9 ) in those who had received one prior chemotherapy regimen . 
these mutations are predicted to lead to the reversion of a somatic not germlinemutation . conclusion rucaparib provided clinical benefit to patients with advanced pancreatic cancer and a brca1 / 2 mutation , and demonstrated an acceptable safety profile . 
2018 by american society of clinical oncology introduction pancreatic cancer ( pc ) is projected to become the second leading cause of cancer death by 2020.1 the majority of pcs are diagnosed at an advanced stage , precluding a surgical , curative approach . 
in the setting of advanced disease , folfirinox treatment ( folinic acid [ leucovorin ] , fluorouracil , irinotecan , and oxaliplatin ) and gemcitabine in combination with nab - paclitaxel are the standards of care , with both demonstrating an improvement in overall survival compared with gemcitabine alone.2 , 3 in the second - line setting , prospective data have shown modest results , with response rates to chemotherapy generally less than 20% , 4 including second - line folfirinox or fluorouracil with nanoliposomal irinotecan.4 - 8 additional therapeutic options are needed . approximately 9% of unselected pcs are associated with a germline or somatic mutation in brca1 or brca2 ( brca1 / 2 ) .9 , 10 cells with a deleterious brca1 / 2 mutation and resultant homologous recombination deficiency are unable to repair dna double - strand breaks reliably11 , 12 and are thus sensitive to poly ( adp - ribose ) polymerase ( parp ) inhibition.13 - 16 studies have demonstrated clinical benefit with parp inhibitors in clinical trials of germline brca1 / 2 mutant breast and ovarian cancer . 
the study design was approved by the independent review board at each participating site and was conducted according to the provisions of the declaration of helsinki and the good clinical practice guidelines of the international conference on harmonization of technical requirements for registration of pharmaceuticals for human use . 
all patients provided written informed consent before participating in the trial . enrolled patients were men and women at least 18 years of age with histologically confirmed locally advanced or metastatic pancreatic adenocarcinoma with measureable disease and a known deleterious germline or somatic brca1 / 2 mutation by local testing . 
patients could have received up to two prior lines of chemotherapy in the locally advanced / metastatic setting , but could not have received prior therapy with a parp inhibitor . 
to infer loss of heterozygosity ( loh ) , the log - ratio profile of sequencing data was segmented , and the allele frequencies of sequenced genome - wide single nucleotide polymorphisms were used to estimate the copy and minor allele frequency for each segment . 
pretreatment plasma specimens were collected on day 1 of cycle 1 for circulating tumor dna ( ctdna ) analysis by foundation medicine , which is a hybrid capture - based next - generation sequencing assay that sequences the coding regions of 62 cancer - related genes , including brca1 / 2 . 
safety results were reported by analysis of adverse events ( aes ) and graded according to the common terminology criteria for adverse events ( version 4 )  . the safety analysis included all patients who received at least one dose of rucaparib . 
for inclusion in the objective response rate ( orr ) , a complete response ( cr ) or partial response ( pr ) per recist had to have been confirmed at least 28 days after the initial response was observed . 
the median age was 57 ( range , 41 to 75 ) years , 57.9% of patients ( 11 of 19 ) were male , the median number of prior chemotherapy regimens for locally advanced / metastatic disease ( excludes adjuvant treatment where progression occurred > 6 months after completion of treatment ) was two ( range , 1 to 3 ) , 78.9% of patients ( 15 of 19 ) had an eastern cooperative oncology group performance status of 1 , and 78.9% ( 15 of 19 ) had a brca2 mutation . 
as prespecified in the protocol , enrollment was stopped because of lack of responses in the first 15 patients evaluated ; the three confirmed responses occurred in the last four patients enrolled . after study closure , one patient continued therapy on an individual patient ind application . 
thirteen patients discontinued the study because of radiologic or clinical progression , two discontinued therapy within a week of beginning ( one because of investigator decision , the other for an unknown reason ) , one discontinued because of aes with simultaneous radiologic progression confirmed at the end of treatment , one discontinued because of an ae with ongoing sd , and one withdrew consent with an ongoing pr . 
patients received rucaparib for a median of 57 days in the study ( range , 2 to 504 days )  . brca1 and brca2 mutation status sixteen of 19 patients had a germline brca1 / 2 mutation . 
of the 16 tumors associated with a germline mutation , paired somatic sequencing was available in eight ; the allelic frequency of the known germline mutant allele was between 41% and 53% . 
this was counted as three separate chemotherapy treatment regimens per the protocol - specified criteria . circulating tumor dna samples for ctdna analyses at cycle 1 , day 1 ( before treatment with rucaparib ) were available for 16 patients , and somatic mutations were detected in 11 patients ( 10 of whom had kras mutations ; appendix table a1 )  . 
investigator - assessed responses ( recist ) in patients with pancreatic cancer and a brca mutation ( n = 19 ) unconfirmed cr / confirmed sd response not evaluable confirmed response rate ( cr or pr ) confirmed response rate ( cr or pr ) in patients with only one prior chemotherapy for locally advanced / metastatic disease disease control rate ( cr , pr , or sd 12 weeks ) all patients patients with only one prior chemotherapy regimen for locally advanced / metastatic disease no . 
in the first patient ( patient 5 ) , ctdna analysis detected the germline brca2 mutation c.7060c > t ( allele frequency , 48% ) , the somatic alteration c.1499_1499delg ( allele frequency , 22% ) , and the secondary somatic mutation c.1416_1420delgcatc ( allele frequency , 19% ) that restored the open reading frame of the brca2 gene . 
in the second patient ( patient 14 ) , ctdna analysis detected the germline brca2 mutation c.5946deit ( allele frequency , 46% ) , the somatic alteration c.1387dela ( allele frequency , 13% ) , and the secondary somatic mutation c.1355_1380deltaccaaaatcagagaagccattaaat , which also restored the open reading frame , but seemed to be subclonal ( with an allelic frequency of only 1% )  . 
this patient , who had also previously received folfirinox , developed significant clinical progression at day 18 , although target lesions were stable . assessment of allele - specific loh tumor was available for analysis in 10 patients . 
 rucaparib treatment stable disease complete response progressive disease partial response progressive disease reported on last day of treatment < 1 weekd patient of prior regimens received prior platinum platinum refractory brca mutation brca2 somatic brca1 germline brca2 germline brca1 germline brca2 germline brca2 germline brca1 germline brca2 germline brca2 germline brca1 germline brca2 germline brca2 germlineg brca2 germline brca2 germline brca2 germline brca2 germline brca2 germline brca2 somatic brca2 somatic sd 72 weeks sd 20 weeks sd 24 weeks pr 36 weeks pr 25 weeks cr 19 weeks pr 5 weeksi cycle fig 2 . 
 ( f ) patient discontinued because of adverse events ( aes ; grade 3 fatigue and grade 4 thrombocytopenia ) ; best response of stable disease ( sd ) was ongoing after the last day of treatment . 
the second patient had a somatic brca2 mutation ( c.1748t > a ) and had a cr as best response ( patient 19 )  . safety all patients had at least one treatment - emergent ae ( table 3 )  . 
two other patients died as a result of disease progression . discussion this study tested the efficacy of a single - agent parp inhibitor , rucaparib , in patients with advanced pc with a known deleterious brca1 / 2 mutation . 
adverse events were graded according to the national cancer institutes common terminology criteria for adverse events ( version 4 )  . * includes adverse events of thrombocytopenia and decreased platelet count . with a confirmed orr of 16% and an observed disease control rate of 32% . 
our findings suggest that there may be a role for parp inhibition in patients with a brca1 / 2 mutation , particularly in those whose disease has not progressed while taking prior platinum therapy . although this was a single - arm study , making comparisons to other agents difficult , the clinical relevance of our results merits comparison with other current standards of care for this patient population . 
 importantly , the only approved chemotherapy combination in the second - line setting , fluorouracil with nanoliposomal irinotecan , had an overall response rate of 7.7% in the pivotal registration study.8 other small single - center studies investigating folfirinox or other chemotherapy combinations in a refractory population show similarly low response rates , reflecting the known chemoresistance of this disease . 
 furthermore , as treatment options improve for pc , patients are even able to move beyond second - line therapy , for which there are no standard of care options . 
this underscores the importance of looking outside of chemotherapy options , particularly in patients with potentially targetable mutations . previous small studies investigating parp inhibition in brca - mutated pc have shown similar efficacy . 
the response rate of single - agent olaparib in patients with metastatic pc harboring a germline brca1 / 2 mutation who had received prior chemotherapy was 22%.20 a phase ii study of veliparib alone in 16 previously treated patients with brca - mutated pc demonstrated single - agent activity , with 25% of patients having sd for at least 4 months . 
analysis is ongoing to understand the role platinum sensitivity played in these four patients.21 when considered with the prior studies , these trials should provide insight into the clinical utility of single - agent parp inhibition in patients with pc and a known brca1 / 2 mutation . in this study , responses to rucaparib were seen in individuals harboring a germline or somatic brca1 / 2 mutation . 
because of significant stromal infiltration in pc , assessing allele frequency of somatic tumor alterations may be challenging . none of the four patients with a confirmed or unconfirmed response had experienced disease progression on prior platinum therapy ( one had never received platinum ) , and three of the four patients had only received one prior chemotherapy regimen for locally advanced or metastatic disease . 
this finding highlights the important question of the role of platinum sensitivity in the setting of advanced / metastatic pc and underscores a potential role for rucaparib as a treatment for patients whose tumors are not platinum refractory . 
similar findings were noted in patients with advanced ovarian cancer treated with olaparib , because the highest response rates were noted in patients who were deemed platinum sensitive rather than resistant or refractory.22 this will need to be investigated in a larger clinical study . 
 secondary mutations that likely confer resistance have been observed in patients with ovarian or prostate cancer who harbor a brca1 / 2 mutation and whose disease has progressed while receiving platinum chemotherapy or parp inhibitors ; however , these reports have demonstrated reversion mutations that have restored the open reading frame in the vicinity of the germline mutation . 
the majority ( but not all ) of brca1 / 2 - mutant breast and ovarian cancers have allele - specific loh23 ; however , the loss of the second allele is most commonly due to copy neutral loh and rarely due to a somatic mutation . 
both of these patients had previously been treated with oxaliplat several studies have demonstrated the presence of reversion mutations in patients previously treated with chemotherapy , particularly platinum based.24 - 27 our study has several limitations , including a small sample size and lack of corresponding somatic sequencing and ctdna analysis for some patients . rucaparib is a well - tolerated parp inhibitor that could be considered in patients with advanced pc with known brca1 / 2 mutations who have received prior chemotherapy . 
domchek research funding : prism biolab ( inst ) , genentech ( inst ) , novartis ( inst ) , newlink genetics ( inst ) , eli lilly ( inst ) , aduro biotech ( inst ) , pfizer ( inst ) , sanofi ( inst ) data analysis and interpretation : rachna t . 
shroff consulting or advisory role : celgene , codiak biosciences , agios , halozyme travel , accommodations , expenses : astrazeneca ravit geva honoraria : bristol - myers squibb , msd , eli lilly , medison , roche , novartis , janssen , pfizer , teva travel , accommodations , expenses : bristol - myers squibb , roche ron epelbaum no relationship to disclose lindsey rolfe employment : clovis oncology leadership : clovis oncology stock and other ownership interests : clovis oncology , celgene , biomarin travel , accommodations , expenses : clovis oncology sandra goble employment : clovis oncology stock and other ownership interests : clovis oncology research funding : eli lilly , celgene , agios , halozyme travel , accommodations , expenses : celgene , codiak biosciences , agios , halozyme kevin k . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb heidi giordano employment : clovis oncology stock and other ownership interests : clovis oncology acknowledgment research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) robert h . 
vonderheide honoraria : genentech , celgene consulting or advisory role : eli lilly , celldex research funding : eli lilly ( inst ) the authors thank lawrence leichman for his helpful input while the study was being designed . 
shroff , the university of texas md anderson cancer center , houston , tx ; andrew hendifar , cedars - sinai medical center , los angeles , ca ; robert r . 
mcwilliams , mayo clinic , rochester , mn ; ravit geva , tel aviv university , tel aviv ; ron epelbaum , rambam health care campus , haifa , israel ; lindsey rolfe , sandra goble , kevin k . 
rahib l , smith bd , aizenberg r , et al : projecting cancer incidence and deaths to 2030 : the unexpected burden of thyroid , liver , and pancreas cancers in the united states . 
assaf e , verlinde - carvalho m , delbaldo c , et al : 5 - fluorouracil / leucovorin combined with irinotecan and oxaliplatin ( folfirinox ) as second - line chemotherapy in patients with metastatic pancreatic adenocarcinoma . 
lee mg , lee sh , lee sj , et al : 5 - fluorouracil / leucovorin combined with irinotecan and oxaliplatin ( folfirinox ) as second - line chemotherapy in patients with advanced pancreatic cancer who have progressed on gemcitabine - based therapy . 
nagrial am , chin vt , sjoquist km , et al : second - line treatment in inoperable pancreatic adenocarcinoma : a systematic review and synthesis of all clinical trials . 
wang - gillam a , li cp , bodoky g , et al : nanoliposomal irinotecan with fluorouracil and folinic acid in metastatic pancreatic cancer after previous gemcitabine - based therapy ( napoli - 1 ) : a global , randomised , open - label , phase 3 trial . 
kristeleit r , shapiro gi , burris ha , et al : a phase i - ii study of the oral parp inhibitor rucaparib in patients with germline brca1 / 2 - mutated ovarian carcinoma or other solid tumors . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
lowery ma , kelsen dp , smith sc , et al : phase ii trial of veliparib ( v ) in patients ( pts ) with previously treated brca or palb2 - mutated ( mut ) pancreas adenocarcinoma ( pc )  . 
domchek sm , aghajanian c , shapira - frommer r , et al : efficacy and safety of olaparib monotherapy in germline brca1 / 2 mutation carriers with advanced ovarian cancer and three or more lines of prior therapy . 
afghahi a , timms km , vinayak s , et al : tumor brca1 reversion mutation arising during neoadjuvant platinum - based chemotherapy in triple - negative breast cancer is associated with therapy resistance . 
weigelt b , comino - mndez i , de bruijn i , et al : diverse brca1 and brca2 reversion mutations in circulating cell - free dna of therapy - resistant breast or ovarian cancer . 
post - test surveys on distress , uncertainty , and positive experiences were administered at 3 months ( 69% response rate ) and 1 year ( 57% response rate )  . results of 2 , 000 participants , 81% were female , 41% were hispanic , 26% were spanish speaking only , and 30% completed high school or less education . 
a total of 242 participants ( 12% ) carried one or more pathogenic variant ( positive ) , 689 ( 34% ) carried one or more variant of uncertain signicance ( vus ) , and 1 , 069 ( 53% ) carried no pathogenic variants or vus ( negative )  . 
after testing , few patients ( 4% ) had prophylactic surgery , most ( 92% ) never regretted testing , and most ( 80% ) wanted to know all results , even those of uncertain signicance . 
positive patients were twice as likely as negative / vus patients ( 83% v 41% ; p , .001 ) to encourage their relatives to be tested . conclusion in a racially / ethnically and socioeconomically diverse cohort , mgpt increased diagnostic yield . 
recent advances in massively parallel sequencing have expanded germline testing for hereditary cancer risk assessment.1 - 3 multiplex gene panel testing ( mgpt ) simultaneously analyzes multiple genes and may provide an advantage over sequential single - gene testing in terms of cost , speed , and clinical utility . 
 idos et al context what are the benets , harms , and patient experiences after germline multiplex gene panel testing for cancer susceptibility ? among 2 , 000 participants in this fully accrued , multicenter , prospective cohort study of hereditary cancer testing with a 25or 28 - gene panel , more than one quarter of the pathogenic variants identied were not clinically anticipated . 
reassuringly , at a median follow - up of 13 months , patients did not regret having undergone multiplex testing , did not overuse preventive surgery , and encouraged their family members to be tested in accordance with practice guidelines . multiplex genetic panel testing enhances the diagnostic yield of genetic testing without discernible harm to patients . 
this study also demonstrates that testing at lower predicted levels of pathogenic variant carriagea probability threshold of 2.5% which reects recent changes in clinical practice and guidelines , is effective and safe . 
overall , this study offers signicant and novel results on the performance of multiplex genetic testing and has broad implications for its clinical implementation and acceptance . cancer risk assessment , and it is crucial to learn more as more comprehensive sequencing approaches on the horizon . we designed a prospective cohort study of hereditary cancer testing with a multigene panel to measure the benets , harms , and patient experiences of mgpt . 
participants were consecutively recruited between july 2014 and november 2016 at three medical centersusc norris comprehensive cancer center , los angeles county and usc medical center , and stanford university cancer institute . 
there were 1 , 664 participants who underwent 25 - gene panel testing and 336 who underwent 28 - gene panel testing . sequencing and large rearrangement analysis were performed for all genes , except pold1 and pole ( sequencing only ) and epcam and grem1 ( large rearrangement only )  . sample preparation for ngs was performed from frozen dna using the raindance microdroplet polymerase chain reaction ( pcr ) system ( raindance technologies , billerica , ma ) .17 in brief , pcr products that represented exons and proximal splicing elements of patient dna were amplied in merged droplets that consisted of fragmented patient dna and select target enrichment primers . 
to circumvent highly homologous pseudogenes , we used modied sample preparation with longrange and nested pcr , followed by ngs on the illumina miseq platform , for portions of chek2 and pms2 . 
all clinically actionable variants identied by ngs , as well as regions that did not meet preset ngs quality metrics , were independently conrmed with orthogonal site - specic sanger sequencing . 
 multicenter study of multiplex panel testing supporting linkage , biochemical , clinical , functional , and statistical data used for specic missense and intronic alterations.18 - 20 gene variants classied as deleterious or that were suspected to be deleterious were considered pathogenic . 
variants classied as polymorphism or that favored polymorphism were considered benign . undergone mgpt , participants desired amount of mgpt results information , participants notication of relatives about mgpt results , and relatives genetic testing behaviors . 
participants were also asked if they had undergone specic surgical procedures ( mastectomy , salpingooophorectomy , or hysterectomy ) and the reason for these treatment , cancer prevention , or procedures ( cancer other ) .23 differential diagnoses statistical analysis differential diagnoses were generated for each participant after expert clinical genetics assessment , in which up to eight inherited cancer syndromes were ranked by estimated likelihood using such factors as personal and family cancer history , tumor characteristics , and physical examination21 ( data supplement )  . 
the genetics clinician then claried a level of suspicion for each syndrome in the differential diagnosis by stating whether she or he would for that syndrome specically if mgpt were not test available . questionnaire procedures participants were invited to answer a baseline questionnaire at the time of their genetics evaluation , with followup questionnaires 3 , 6 and 12 months after disclosure of mgpt results . 
e - mail participants who did not respond to the initial invitation link received two e - mail reminders over a course of 2 weeks before receiving a reminder phone call from study personnel . 
using a standardized script , all participants who received a reminder phone call were given the option to receive another e - mail invitation , another mailed paper questionnaire , or to complete the questionnaire over the phone . 
participants were considered nonresponders if they had not completed their questionnaire 2 months after the initial send date . patient - reported experiences we used the validated multidimensional impact of cancer risk assessment ( micra ) 22 instrument , which contains subscales that measure distress , uncertainty , and positive experiences in relation to genetic testing . 
additional questions evaluated intrusive thoughts about cancer and regret about having the primary aim of this study was to test the impact of genetic test resultspositive , vus , or negativeon patient experience . 
micra subscale scores were used for this aim . patients with one or more pathogenic variant were considered positive , whereas those with only benign or uncertain variants were considered vus and those with only benign variants were considered negative . 
assuming a pathogenic variant prevalence of 10% , a vus prevalence of 35% , and a negative test prevalence of 55% , with the standard deviation of micra scores being 4 , a sample size of 2 , 000 patients was needed to achieve more than 80% power to detect a difference of 1 in micra scores . data analysis was based on information gathered as of march 19 , 2018 . 
we used the pearson 2 test to assess the association between genetic test results and survey responses . negative binomial regression with a log link was used to analyze the association of genetic test results with micra subscale scores while adjusting for covariates that included clinical site , age , gender , ethnicity , education level , and personal history of cancer . 
common reasons for genetics referral include the following : cancer diagnosis at age 50 years or younger ( 39% ) , two or more rstor second - degree relatives with cancer ( 64% ) , and one or more family members diagnosed with cancer at younger than age 50 years ( 63% )  . 
participants were diverse both racially / ethnically and sociodemographically39% were hispanic ( primarily of mexican or central american ancestry ) , 40% non - hispanic white , 12% asian ( primarily of chinese and filipino ancestry ) , and 4% black . 
seventy - six patients31% of all pathogenic variant carriershad a germline mutation in brca1 and / or brca2 , and 39 ( 16% ) had a pathogenic variant in a mismatch repair gene conferring a diagnosis of lynch syndrome . 
of pathogenic mutations brca1 and brca2 genes associated with breast cancer genes associated with ovarian cancer lynch syndrome genes genes associated with colon , pancreatic , or gastric cancer tp53 ( 2% )  . 
among patients without pathogenic variants , 689 ( 34% ) had at least one vus , with up to four per patient ( table 2 )  . differential diagnosis versus mgpt results of 242 participants with pathogenic variants , 160 ( 66% ) had pathogenic variants in genes related to syndromes that were included in the pretest differential diagnosis . 
eightytwo patients ( 34% ) had pathogenic variants that were not clinically anticipatedmonoallelic mutyh ( n = 32 ; 39% ) , apc i1307k ( n = 13 ; 16% ) , chek2 ( n = 10 ; 12% ) , palb2 ( n = 8 ; 10% ) , atm ( n = 7 ; 9% ) , brip1 ( n = 4 ; 5% ) , brca2 ( n = 3 ; 4% ) , brca1 ( n = 2 ; 2% ) , pms2 ( n = 2 ; 2% ) , and tp53 ( n = 1 ; 1% )  . use of surgery after mgpt at a median follow - up of 13 months , 198 ( 13% ) of 1 , 573 returning surveys reported undergoing surgery after mgpt . surgery rates and stated reasons were as follows : mastectomy ( n = 162 [ 11.3% ] : 90% for cancer treatment , 30% for cancer prevention , and 2% for benign breast disease ) , salpingo - oophorectomy ( n = 43 [ 3% ] : 27% for cancer treatment and 56% for cancer prevention ) , and hysterectomy ( n = 23 [ 2% ] : 50% for cancer treatment , 18% for cancer prevention , and 9% for benign disease )  . 
to illustrate , there were 10 patients identied as having highpenetrance founder mutations in brca1 or brca2 , six of whom were found to have undergone or were considering risk - reducing mastectomy or oophorectomy . 
in comparison , there were 16 patients identied as carriers of the lowpenetrance apc i1307k allele , none of whom had undergone an inappropriate surgery ( data supplement )  . patient experiences with mgpt at a median follow - up of 4 months , the response rate was 69% . 
mean scores for each micra subscaledistress , uncertainty , or positive experiencesall differed signicantly between patients with positive test results compared with the group of patients with a negative or vus result ( table 3 )  . 
sociodemographic and clinical characteristics by genetic test result characteristic positive ( n = 242 ) negative ( n = 1 , 069 ) vus ( n = 689 ) total ( n = 2 , 000 ) idos et al clinical site , no . 
also , a higher proportion of patients testing negative as compared to positive reported that they did not regret learning their test results ( 95% v 85% ; p , .001 ; fig 2 )  . 
we found little evidence of patient harm and substantial evidence that patients understood the meaning of their mgpt results , as patients who tested positive for a pathogenic variant were more likely to encourage appropriate genetic testing in relatives compared with those who tested with vus or negative results . 
these results suggest an important contribution of mgpt to clinical cancer risk assessment of probands and their families . a striking result was that one in three identied pathogenic variants was missed in the differential diagnoses generated by expert clinicians . 
of note , few of the missed variants were in genes associated with well - known syndromesfor example , lynch syndrome , hereditary breast / ovarian cancerwhich likely reects clinicians greater familiarity with their presentation . instead , most were in moderate - penetrance genes that confer a twoto four - fold increase in cancer risk ( eg , atm and chek2 ) as well as low - penetrance mutations ( eg , monoallelic mutyh and apc i1307k )  . given the short history of widespread clinical testing of these genes , 24 - 27 their phenotype is less well characterized and more difcult for clinicians to recognize . 
some questions remain about the clinical benet to moderate - penetrance pathogenic of detecting lowvariants ; however , these variants meet criteria for intensied cancer screening according to current practice guidelines , 28 , 29 which makes them relevant to patient care . by identifying unexpected pathogenic variants , mgpt can broaden our understanding of genotype - phenotype correlations and the spectrum of associated cancer risks . concerns have been raised about high rates of identifying vus in mgpt . 
consistent with prior studies , we report a vus rate of 34%.5 - 8 recent studies found limited genomic condence among oncologists and that few ( less than 15% ) community physicians who order brca1 and brca2 tests understand the correct management of vus.27 , 31 , 32 we recently published that patients who receive vus results from genetic testing are substantially more likely to seek a second opinion from a new medical oncologist.33 a related concern is that mgpt results of unknown clinical relevance , whether vus or a pathogenic variant whose cancer risk is insufciently characterized , might prompt operations.34 - 36 invasive data from our prospective cohort study do not support this hypothetical concern . 
reassuringly , we found that prophylactic operations were not overusedonly 4% underwent prophylactic mastectomy , hysterectomy , or prophylactic irreversible salpingo - oophorectomy , and these procedures were no more frequent among patients with vus results than those with negative results . 
with a median follow - up time of these results do not 13 months after genetic testing , suggest an overuse of surgery after mgpt in this study . of note , overall yield of pathogenic variants in this study is 12% , which is similar to other studies . 
whereas panels may vary in the number of genes tested , all large panels , including the one used in this study , include genes that are associated with known syndromesthat is , hereditary breast / ovarian cancer and lynch syndromewhich account for the majority of pathogenic mutations identied in most multigene panel studies . 
our group previously examined the additional yield of mutations identied via multigene panel testing and found that by increasing the the frequency of mutations number of genes tested , identied also increased.37 , 38 independently , a recent study by mandelker et al39 demonstrated a 17.5% yield of pathogenic variants after sequencing 1 , 040 patients with advanced cancer using the memorial sloan kettering impact panel of 410 genes . patient - reported experiences were also reassuring . 
 multicenter study of multiplex panel testing genetic test results in a multitude of settings.40 we found that micra subscale scores varied signicantly between patients who tested positive compared with those who had a negative or vus test result , but scores did not vary between patients with a vus versus negative except in the category of uncertainty . 
these ndings suggest that patients rarely misinterpret vus with appropriate pretest genetic counseling as most vuss that are reclassied are ultimately reclassied to benign.15 , 41 on the contrary , these ndings suggest that patients understood the implications of their mgpt results , which is particularly encouraging in our population as approximately one third received high school education or less . 
the present results contrast with our recent nding of gaps in the understanding and management of vus in community practice , and serve to demonstrate the value of preand post - test counseling with proper anticipatory guidance by a trained professional.42 - 44 there are limited published data on pathogenic mutation rates among hispanics after multiplex gene panel testing , as hispanics are underrepresented in a majority of clinical studies . 
in our previous usc - based paper by ricker et al , 37 in which hispanic patients made up 47.6% ( n = 228 ) of the cohort , there was a pathogenic mutation frequency of 14.1% ( n = 33 )  . 
in a study by rosenthal et al , 11 among the 8% ( n = 19 , 795 ) of hispanic patients who underwent multigene panel testing , 6.7% ( n = 1 , 326 ) were found to have a pathogenic mutation . 
its considerable strengths include a prospective , multicenter design ; a diverse population in terms of race / ethnicity , language , testing at and education ; a high survey response rate ; and uniform pretest assessment by experienced genetic counselors . the participation rate of hispanic / latino , african american , and asian patients was high compared with other published studies . 
to our knowledge , it is the rst study to demonstrate that lower predicted levels of pathogenic variant carriage , which reects recent changes in clinical practice and guidelines , is effective and safe . 
this study offers signicant and novel results on the performance of multiplex genetic testing and has broad impliimplementation and acceptance . cations for its clinical looking forward , interim analysis of our data suggests that patients who are found to have a pathogenic variant in a highor moderate - risk gene are more likely to undergo appropriate screening and surveillance compared with those who tested negative or with a vus within 1 year of mgpt testing . for example , patients who were identied as carrying a pathogenic variant in a gene associated with lynch syndrome were four times as likely ( p , .001 ) to undergo colonoscopy compared with patients with a vus or negative genetic test result . encouragingly , this trend is consistent when we stratify by ethnicity in our hispanic cohort . its limitations include 13 months of follow - up time to date . in addition , our survey response rate decreased to 57% at 12 months from 69% at 3 months , as we primarily recruited from a clinical cohort , most of whom were affected with cancer and undergoing active treatment . 
contributed equally to this work . employees of myriad genetic laboratories served as coinvestigators in this study and provided material support , including germline testing and interpretation , as described in the manuscript . 
kurian research funding : myriad genetics ( inst ) other relationship : ambry genetics , color genomics , genedx , bioreference , invitae , genentech charit e ricker research funding : myriad genetics ( inst ) peter levonian consulting or advisory role : pwnhealth katrina lowstuter research funding : myriad genetics ( inst ) meredith a . 
mills research funding : myriad genetics ( inst ) , natera ( inst ) anne - renee hartman employment : myriad genetics , grail stock and other ownership interests : myriad genetics , grail richard j . 
wenstrup employment : oxford immunotec , myriad genetics leadership : oxford immunotec , myriad genetics stock and other ownership interests : oxford immunotec , myriad genetics patents , royalties , other intellectual property : founding patent holder , assurexhealth , since 2016 , a wholly owned subsidiary of myriad genetics johnathan m . 
lancaster employment : myriad genetics leadership : myriad genetics stock and other ownership interests : myriad genetics consulting or advisory role : protean biodiagnostics travel , accommodations , expenses : myriad genetics krystal brown employment : myriad genetics john kidd employment : myriad genetics consulting or advisory role : myriad genetics brent evans employment : myriad genetics stock and other ownership interests : myriad genetics travel , accommodations , expenses : myriad genetics kevin j . 
mcdonnell consulting or advisory role : brogent international research funding : myriad genetics uri ladabaum stock and other ownership interests : universal dx , lean medical consulting or advisory role : motus gi , medtronic / covidien ( given ) , quorum consulting , clinical genomics james m . 
gruber employment : brogent international leadership : brogent international stock and other ownership interests : brogent international , fulgent therapeutics consulting or advisory role : myriad genetics , fulgent therapeutics research funding : myriad genetics ( inst ) no other potential conicts of interest were reported . acknowledgment the authors thank blanca ovalle , serina ovalle , and angelica mora for their tremendous help in the recruitment and observation of study participants . references easton df , pharoah pd , antoniou ac , et al : gene - panel sequencing and the prediction of breast - cancer risk . 
walsh t , casadei s , lee mk , et al : mutations in 12 genes for inherited ovarian , fallopian tube , and peritoneal carcinoma identied by massively parallel sequencing . 
 multicenter study of multiplex panel testing clin genet 86 : 510 - 520 , 2014 oncol 36 : 414 - 424 , 2018 j clin oncol 33 : 3660 - 3667 , 2015 110 : 1059 - 1066 , 2018 3 . 
walsh t , lee mk , casadei s , et al : detection of inherited mutations for breast and ovarian cancer using genomic capture and massively parallel sequencing . proc natl acad sci usa 107 : 12629 - 12633 , 2010 yurgelun mb , allen b , kaldate rr , et al : identication of a variety of mutations in cancer predisposition genes in patients with suspected lynch syndrome . gastroenterology 149 : 604 - 613.e20 , 2015 yurgelun mb , kulke mh , fuchs cs , et al : cancer susceptibility gene mutations in individuals with colorectal cancer . 
j clin oncol 35 : 1086 - 1095 , 2017 tung n , lin nu , kidd j , et al : frequency of germline mutations in 25 cancer susceptibility genes in a sequential series of patients with breast cancer . 
j clin oncol 34 : 1460 - 1468 , 2016 thompson er , rowley sm , li n , et al : panel testing for familial breast cancer : calibrating the tension between research and clinical care . 
j clin oncol 34 : 1455 - 1459 , 2016 kurian aw , hare ee , mills ma , et al : clinical evaluation of a multiple - gene sequencing panel for hereditary cancer risk assessment . 
j clin oncol 32 : 2001 - 2009 , 2014 desmond a , kurian aw , gabree m , et al : clinical actionability of multigene panel testing for hereditary breast and ovarian cancer risk assessment . 
rosenthal et , bernhisel r , brown k , et al : clinical testing with a panel of 25 genes associated with increased cancer risk results in a signicant increase in clinically signicant ndings across a broad range of cancer histories . 
balmaa j , digiovanni l , gaddam p , et al : conicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
j clin oncol 34 : 4071 - 4078 , 2016 judkins t , leclair b , bowles k , et al : development and analytical validation of a 25 - gene next generation sequencing panel that includes the brca1 and brca2 genes to assess hereditary cancer risk . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
pruss d , morris b , hughes e , et al : development and validation of a new algorithm for the reclassication of genetic variants identied in the brca1 and brca2 20 . 
hampel h , bennett rl , buchanan a , et al : a practice guideline from the american college of medical genetics and genomics and the national society of genetic counselors : referral indications for cancer predisposition assessment . 
cella d , hughes c , peterman a , et al : a brief assessment of concerns associated with genetic testing for cancer : the multidimensional impact of cancer risk assessment ( micra ) questionnaire . 
yurgelun mb , mercado r , rosenblatt m , et al : impact of genetic testing on endometrial cancer risk - reducing practices in women at risk for lynch syndrome . gynecol oncol 127 : 544 - 551 , 2012 2013 netw 15 : 9 - 20 , 2017 canc netw 15 : 1465 - 1475 , 2017 prev res ( phila ) 4 : 9 - 22 , 2011 24 . 
j clin oncol genet test mol biomarkers 17 : 367 - 375 , 2013 35 : 2232 - 2239 , 2017 jama oncol 3 : 391 - 397 , 2017 susceptibility testing . 
bradbury ar , patrick - miller lj , egleston bl , et al : patient feedback and early outcome data with a novel tiered - binned model for multiplex breast cancer 35 . 
ricker c , culver jo , lowstuter k , et al : increased yield of actionable mutations using multi - gene panels to assess hereditary cancer susceptibility in an ethnically diverse clinical cohort . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
maxwell kn , hart sn , vijai j , et al : evaluation of acmg - guideline - based variant classication of cancer susceptibility and non - cancer - associated genes in families affected by breast cancer . 
 about ras mutation clearance in plasma ctdna from ras - mutant colorectal cancer patients bouchahda et al1 recently published in your journal . authors conducted a pilot study aimed to investigate the efcacy and safety of antiegfr - targeted therapy added to chemotherapy in patients with unresectable metastatic colorectal cancer with raswild - type circulating tumor dna ( ctdna ) but ras - mutant primary tumor . 
we would like to emphasize the following . in 2017 , our group for the rst time started to investigate the clearance of ras - mutant clones in plasma , supporting an unexpected negative selection of rasmutant clones during the clonal evolution of rasmutant metastatic colorectal cancer ( mcrc ) .2 one year later , we reported that ve patients with rasmutant ras ( ras - mt ) mcrc who switched to wildtype ras ( wt - ras ) in plasma ctdna received egfr inhibitors as a second - line treatment , achieving a durable clinical benet , 3 thus suggesting that ctdna analysis might reveal a therapeutically exploitable window of opportunity , characterized by the prevalence of wt - ras clones , which can be converted in a clinically meaningful benet for patients . 
we published a detailed case report4 in which we described the study of a patient with a primary n - ras - mutant colorectal cancer , who received second - line treatment with antiegfr , after failure of rst - line triplet chemotherapy plus bevacizumab , according to the absence of any clinically relevant mutation of ras genes in blood , achieving a partial response . 
with this background , we designed the currently ongoing kairos trial ( eudract number : 2019 - 001328 - 36 ) , aimed to investigate the efcacy and safety of second - line cetuximab plus chemotherapy treatment in initially ras - mt mcrc patients who converted to raswt at the time of rst progression.3 , 4 we regret having to note that bouchahda et al1 have not cited neither our publications nor have they named the kairos trial in their entire discussion . 
in fact , the authors state that the team of raimondi et al5 recently reported the disappearance of ras - mt clones in ctdna after tumor progression while receiving bevacizumab and chemotherapy in four patients with ras - mt mcrc . 
this last information is incorrect in that we prospectively enrolled mcrc patients at the time of progression of disease and the mutational status of ctdna was assessed before initiating a further line of therapy ( as far as we underthe same inclusion criteria as reported by stand , bouchahda et al1 in their study )  . 
furthermore , bouchahda et al strongly limited the discussion of our data to the number of patients who converted to wt - ras in plasma , omitting to specify that these patients were then treated with egfr blockade based on the results obtained in ctdna . 
in these patients , the introduction of anti - egfr agents , which would have not been supported by international guidelines , allowed to achieve a 12 - month , 10 - month , and 6 - month pfs in three patients treated in second - line setting and a pfs of 4 months in patients treated in fourth - line.5 these data should have been included and discussed . 
finally , the authors state that studies with liquid biopsy have been to date selectively focused on the early detection of the appearance of ras - mt clones in tumor deposits by analyzing ctdna in blood samples from patients with raswt primary tumors . 
bouchahda m , saffroy r , karaboue a , et al : undetectable rasmutant clones in plasma : possible implication for anti - egfr therapy and prognosis in patients with ras - mutant metastatic colorectal cancer . 
gazzaniga p , raimondi c , urbano f , et al : second line egfr - inhibitors in ras mutant metastatic colorectal cancer : the plasma ras wild type window of opportunity . 
gazzaniga p , raimondi c , urbano f , et al : egfr inhibitor as second - line therapy in a patient with mutant ras metastatic colorectal cancer : circulating tumor dna to personalize treatment . 
raimondi c , nicolazzo c , belardinilli f , et al : transient disappearance of ras mutant clones in plasma : a counterintuitive clinical use of egfr inhibitors in ras mutant metastatic colorectal cancer . 
nicolazzo c , belardinilli f , caponnetto s , et al : why the therapeutic impact of ras mutation clearance in plasma ctdna deserves to be further explored in metastatic colorectal cancer . 
 clinical utility of genomic profiling in the treatment of advanced sarcomas : a single - center experience see accompanying editorial doi : purpose sarcomas are a diverse group of malignant tumors that arise from soft tissues or bone . 
 in this study , we review our institutional experience with next - generation sequencing ( ngs ) based molecular profiling for nongi stromal tumors sarcomas , with a focus on the clinical utility of the results . patients and methods we retrospectively analyzed results of ngs performed on tumors from 114 patients with a diagnosis of sarcoma . 
for therapeutic trials and treatment guidelines , treatment options for sarcomas have historically frequently been lumped into broad categories ( eg , soft tissue sarcoma ) , despite highly divergent underlying disease biology and clinical behavior . 
furthermore , current treatment options for patients with advanced disease are limited and generally not curative , which highlights the need for novel approaches and greater understanding of disease biology . in recent years , there has been an increasing desire to personalize treatment of patients with advanced cancer via molecularly guided therapeutic selection . 
to a degree , sarcoma was on the forefront of successful molecularly targeted therapy with the clinical development of tyrosine kinase inhibitors against kit or pdgfra mutations for advanced gi stromal tumors ( gist ) in the early 2000s.1 for most other sarcoma subtypes , however , targetable mutations have not been widely described , and the clinical utility of routine spandana boddu christine m . 
 molecular profiling in sarcoma has not been established . in this study , we review our institutional experience with next - generation sequencing ( ngs ) based molecular profiling for non - gist sarcomas . 
 we review > 100 sarcoma cases that underwent comprehensive molecular profiling , with a focus on the clinical utility of the results , including molecular target identification , diagnostic clarification , and treatment outcomes . 
to our knowledge , this is one of the largest sarcoma specific analyses of this type to date . methods we used our personalized medicine clinical service ( pmcs ) database to identify all patients seen at the moffitt cancer center with a diagnosis of non - gist sarcoma who underwent commercial genomic testing between may 2013 and march 2017 . 
genomic findings from each patient were manually curated in the clinical genomic action committee database along with demographic , clinical , and histologic information , in addition to type and date of genomic test and date and source of biopsy specimen . 
all patients are reviewed either by the core members of the pmcs group weekly or by the moffitt molecular tumor board ( clinical genomic action committee ) on the basis of the complexity of the genetic results . 
 as previously described , clinical actionability is based on available literature , and recommendations are documented in the patients electronic medical record as a resource for the treating physicians.2 though tumor - only sequencing was performed , for findings that were felt to be potentially germline ( eg , previously reported pathogenic mutation in clinvar [ ncbi.nlm.nih.gov / clinvar / ] that could be either somatic or germline ) , a recommendation was given to the treating provider to refer the patient for genetic counseling and assessment . performed on identified patients to retrospectively collect treatments and outcomes data . 
genetic alterations were defined as clinically actionable if they had been documented in the literature to provide diagnostic or prognostic information or to predict response or resistance to commercially available or investigational agents . 
actionability was classified as predicting response to approved drugs available for the patients diagnosis ( on - label ) , for another diagnosis ( off - label ) , or investigational drugs being studied in humans for whom the genetic alteration has been shown to serve as a suggested biomarker for response . 
assessment of clinical actionability was limited to mutations previously reported or likely to be driver - mutations based on available literature and functional classification and did not consider analysis of variants of unknown significance . 
the study was approved by the university of south florida institutional review board . results we identified 114 patients with a diagnosis of non - gist sarcoma who underwent molecular profiling during the specified period . 
there were 51 men ( 45% ) and 63 women ( 55% ) in the cohort , with the median age at diagnosis of 55 ( interquartile range , 38 to 65 ) years . 
the most common disease histologies paralleled the most common sarcoma subtypes , such as leiomyosarcoma ( 16.7% ) , well - differentiated / dedifferentiated liposarcoma ( 12.2% ) , and undifferentiated pleomorphic sarcoma ( 10.5% ) as the most frequent soft tissue tumors . 
of small variants , truncating mutation types such as nonsense , frameshift , and splice site altogether ( n = 99 ) outnumbered missense mutations ( n = 65 )  . 
no patients had evidence of microsatellite instability . for five patients ( 4.4% ) , the genomic findings were felt to be diagnosis changing or diagnosis modifying by the treating physician . 
 one case of poorly differentiated sarcoma , favor neurogenic tumor / mpnst [ malignant peripheral nerve sheath tumor ] was diagnosed as synovial sarcoma after a typical ss18 - ssx2 fusion was detected by ngs and confirmed by conventional testing . 
in the remaining three cases , novel or seminovel fusions that were felt to be disease defining were detected in cases of small round cell sarcoma , not otherwise specified , including one each of ewsr1 - patz1 , bcor - zc3h7b , and phf1 - tfe3 . eighty - eight patients ( 77.2% ) had a therapeutic option recommended by the commercial ngs testing report . 
after review of the genomic findings by our institutional pmcs , 56 patients ( 49.1% ) were classified as having an actionable result ; the significant majority of these had both off - label targeted therapy and molecularly matched clinical trial options ( table 2 )  . 
of note , this number includes those in whom a standard treatment option was selected over an alternative ( eg , selection of pazopanib instead of an alternate , second - line agent because of molecular matching of this target ) and cases in which therapy selection was altered as a result of change in diagnosis . 
four of 15 ( 26.7% ) ngs - influenced therapies evaluable for outcome resulted in clinical benefit ( partial response or stable disease > 6 months )  . discussion in the past several years , there has been significant enthusiasm from patients and clinicians alike to personalize cancer therapy by fig 1 . 
more broadly , there have been indications that the use of molecular - based trial selection criteria leads to higher success rates within the context of early phase clinical trials.4 , 5 sarcomas , given their rarity , diversity , and lack of highly effective therapies in the majority of advanced cases , would seem a natural choice for such a personalized treatment approach . 
the genes most commonly affected by pathogenic mutations in our cohort mirror those most widely reported in sarcomas to date.6 our results are remarkably consistent with the limited published literature of the experience of clinical genomic profiling in sarcoma to date . 
in a separate study of 102 patients with sarcoma , groisberg et al8 reported a similar high rate of potentially actionable mutations , and furthermore that 16% of their cohort went on to receive molecularly guided therapy . 
this number , however , includes those who received therapy for mutations that could be assumed or tested without the need for ngs , such as mdm2 amplification in well differentiated / dedifferentiated liposarcoma . 
in a third study of 107 patients with sarcoma , ngs resulted in diagnosis change in 5% of patients and led to matched trials in 30%.9 this latest study has been presented in abstract form only ; therefore , details of the trial matching , outcomes , and whether ngs would truly have been necessary to detect the alterations of interest are not currently available . our study adds significantly to the existing literature on the clinical utility of ngs in the treatment of advanced sarcomas . 
furthermore , we report and account for the frequent situation where commercial ngs findings overlap with already known recurrent alterations , such as mdm2 / cdk4 amplification in well - differentiated / dedifferentiated liposarcoma . 
most critically , we describe the end point of clinical benefit , which is often omitted from molecular profiling reports . it is important for patients and clinicians to have a sense of expectations for clinical ngs . 
furthermore , without a true control comparator , it is impossible to say whether the patients who had treatment influenced by ngs did better than they would have done without this information . 
it is possible , for example , that the chondrosarcoma treated with prolonged stable disease was an indolent version of this malignancy that may have been stable for this period anyway . 
 to answer the important question of true clinical benefit of molecular profiling . despite the cited limitations , a minority of patients with sarcoma have their course profoundly influenced by clinical genomic profiling . 
looking forward , we expect the number of patients who have actionable ngs findings to steadily increase as more molecularly targeted therapies become available and as genomics becomes increasingly used as a biomarker for immunotherapy response . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . spandana boddu no relationship to disclose christine m . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
gounder mm , ali sm , robinson v , et al : impact of next - generation sequencing ( ngs ) on diagnostic and therapeutic options in soft - tissue and bone sarcoma . 
 aggressive - variant microsatellitestable pole mutant prostate cancer with high mutation burden and durable response to immune checkpoint inhibitor therapy the increasing application of next - generation tumor dna sequencing may define molecular subsets of prostate cancer for which precision medicine approaches are enabled . 
transrectal ultrasound guided needle biopsy demonstrated gleason 4 + 5 = 9 ( grade group 5 ) adenocarcinoma in 12 of 12 cores involving 95% to 100% of each core with perineural invasion . 
tumor cells stained positive for psa and negative for chromogranin and synaptophys radiologic staging studies indicated bilateral external iliac , common iliac , and retroperitoneal adenopathy without definitive evidence of bone metastases . 
with persistent bulky disease in the prostate on digital rectal examination at 12 weeks from the start of hormonal therapy , a repeat biopsy was performed , which demonstrated gleason 4 + 5 = 9 adenocarcinoma with focal synaptophysin expression . 
restaging studies showed only modest regression in pelvic adenopathy discordant with the brisk decline in psa , with tumor infiltrating the bladder base and seminal vesicles , and abutting the rectum with a preserved fat plane on magnetic resonance imaging . 
pathologic examination indicated a high - grade tumor with morphologic and immunohistochemical evidence of neuroendocrine differentiation ( synaptophysin and chromogranin expression ) with lymphocytic infiltration ( fig 1 ; appendix fig a1 )  . 
seminal vesicle involvement was absent , but there was extensive extraprostatic extension and multiple positive surgical margins including the bladder neck , and one of eight lymph nodes were involved.the patient did well in the postoperative period , with early recovery of continence ; however , restaging studies showed progressive retroperitoneal and pelvic adenopathy . 
repeat radiologic imaging after an interval on observation again demonstrated progressive pelvic adenopathy ( fig 2a )  . methodology genomic sequencing studies on the primary tumor were performed with the foundationone assay1 ( foundation medicine , cambridge , ma ) , and the tumor mutation burden was estimated as previously described.2 mutations of the androgen receptor , pten , tp53 , and atm , which have been previously implicated in the genomic landscape of prostate cancer , 3 , 4 were identified , along with a pole v511l mutation ( appendix table a1 )  . 
using all nondriver and nongermline missense mutations , we found that 77% of the alterations in the sample were attributable to the pole signature , making this the dominant signature over other lesions identified in the sample that have been implicated in dna repair , including tp53 , atm , or pten ( appendix table a1 )  . 
germline screens for inherited mutations included a screen for brca1 and brca2 ( ambry genetics , aliso viejo , ca ) and a breast - ovarian panel ( genedx , gaithersburg , md )  . 
infiltrating cd4 + and cd8 + lymphocytes were observed in a three to one ratio.the patients family history raised concerns of an autosomal - dominant inherited risk of prostate and breast cancer . 
his father had been diagnosed with high - grade prostate cancer at 76 years of age , and his two brothers had screen - detected low - risk prostate cancer at 54 and 48 years of age , respectively . 
one sister had died of triple - negative metastatic breast cancer at 45 years of age , and another was diagnosed with ductal carcinoma in situ at 55 years of age . 
 was identified in the father in brip1 ( c2392c > t [ p . arg798ter ] ) , along with a brip1 variant of uncertain significance ( c.3710c > a [ p.ser1237tyr ] ) ; the latter alone was found in the patient and two living siblings ( appendix fig a2 )  . 
given the early castration - resistant and chemotherapy - resistant progression of the patients disease and the high tumor mutation burden identified , he was started on immune checkpoint inhibitor blockade with pembrolizumab therapy 200 mg every 3 weeks intravenously . 
sixteen months later , he has remained without evidence of disease progression after 24 cycles of therapy , with residual subcentimeter pelvic nodes , a normal testosterone level without hormonal therapy , and an eastern cooperative oncology group performance score of zero . discussion to our knowledge , this first report in prostate cancer indicates the presence of a mutation in the highly conserved exonuclease domain of dna polymerase ( pole ) 7 in an aggressive - variant metastatic prostate cancer8 that presented with a bulky primary tumor , early castration , and chemotherapy resistance but with an excellent and durable subsequent response to immune checkpoint blockade . 
pole mutant cancers constitute a unique genomic subset of cancers described previously in colorectal and endometrial cancers.9 the somatic v411l mutation of pole has been associated with impaired dna proofreading repair and the generation of ultramutated tumor phenotypes that are microsatellite stable.9 , 10 mutations that could contribute to castration resistance ( androgen receptor , pten ) or dna damage repair insufficiency ( atm , tp53 ) were also identified , consistent with the known genomic landscape of prostate cancer.3 however , two methods of analyzing genomic signatures were used that implicate the pole lesion as the dominant source of the hypermutated phenotype in this case . 
 hypermutated phenotypes in prostate cancer are uncommon and were first identified in 12% of tumors ( 7 of 60 ) sourced from patient - derived xenografts and a rapid autopsy series.11 in this study set , hypermutated tumors , defined as > 300 somatic protein - altering mutations , were universally associated with micro satellite instability largely secondary to msh2 and msh6 structural rearrangements and not mlh1 epigenetic silencing , as is more commonly seen in colorectal and endometrial cancers with dna mismatch repair deficiency . 
 our case report suggests that microsatellite stable pole mutant prostate cancer represents a distinct , albeit exceedingly rare , genomic subset of highmutation - burden prostate cancers with demonstrable potential for high - quality and durable response to immune checkpoint blockade , similar to that reported in endometrial and colorectal pole mutant cancers.12 , 13although responses to immune checkpoint inhibitors in castration resistant prostate cancer have been uncommon to date , 14 - 16 in one study , three of 10 enzalutamide resistant tumors responded to pembrolizumab therapy.17 one evaluable tumor was found to be microsatellite unstable , and a second was microsatellite stable . 
to our knowledge , other that this case report , there are no data that link the control of prostate cancer with immune checkpoint inhibitors to genomically defined highmutation - burden subsets of prostate cancers , whether microsatellite stable or unstable . 
more studies will be required to establish whether high - quality and durable responses to immune checkpoint inhibitors as single agents will be confined to prostate tumors with high mutation burdens . 
hotspot germline genomic sequencing using commercially available assays via clinical genetics consultation did not identify a pathogenic lesion in the patient and two of the living siblings with cancer diagnoses , but his father was identified with a pathogenic brip1 variant along with the brip1 variant of uncertain significance found in his children . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . lisa lee no relationship to disclose elizabeth genega no relationship to disclose dallas reed no relationship to disclose ethan sokol no relationship to disclose paul mathew honoraria : exelixis patents , royalties , other intellectual property : patent pending on new therapeutic invention travel , accommodations , expenses : exelixis affiliations lisa lee , elizabeth genega , dallas reed , and paul mathew , tufts medical center , boston ; siraj ali and ethan sokol , foundation medicine , cambridge , references 1 . 
graff jn , puri s , bifulco cb , et al : sustained complete response to ctla - 4 blockade in a patient with metastatic , castration - resistant prostate cancer . 
kwon ed , drake cg , scher hi , et al : ipilimumab versus placebo after radiotherapy in patients with metastatic castration - resistant prostate cancer that had progressed after docetaxel chemotherapy ( ca184 - 043 ) : a multicentre , randomised , double - blind , phase 3 trial . 
kote - jarai z , jugurnauth s , mulholland s , et al : a recurrent truncating germline mutation in the brip1 / fancj gene and susceptibility to prostate cancer . 
 legend prostate cancer squamous cell carcinoma colorectal cancer thyroid cancer melanoma basal cell cancer breast cancer 61 years brip1 c.3710c > a ( p.ser1237tyr ) ; likely benign variant prostate cancer , 59 years gleason 9 60 years breast cancer ( unilateral ) , 54 years brip1 c.3710c > a , p.ser1237tyr ; likely benign variant 53 years prostate cancer , 52 years melanoma 49 years prostate cancer , 48 years basal cell cancer d . 
87 years colorectal cancer , 87 years 85 years brip1 c.2392c > t ( p.arg798ter ) ; pathogenic prostate cancer , 79 years squamous cell carcinoma 83 years thyroid cancer , 40s fig a2 . 
 epicapture : a urine dna methylation test for early detection of aggressive prostate cancer purpose liquid biopsies that noninvasively detect molecular correlates of aggressive prostate cancer ( pca ) could be used to triage patients , reducing the burdens of unnecessary invasive prostate biopsy and enabling early detection of high - risk disease . 
epicapture was performed by quantitative methylation - specific polymerase chain reaction in dna isolated from prebiopsy urine sediments and evaluated by receiver operating characteristic and decision curves ( clinical benefit )  . 
the epicapture score was developed and validated on a two thirds training set to one third test set . results higher methylation of epicapture genes was significantly associated with increasing aggressiveness in pca tissues . 
2019 by american society of clinical oncology introduction prostate cancer ( pca ) is the most common noncutaneous malignancy in men and the third leading cause of cancer - related deaths in men in the western world . 
 with an aging population , spread of westernized diet , and increasing use of prostate - specific antigen ( psa ) testing , this figure is predicted to double by 2035.1 pca demonstrates extreme clinical heterogeneity . 
overall , 10 - year survival rates are close to 100%2 ; thus , there is much interest in strategies to reduce overtreatment of low / intermediate risk tumors.3 however , more than 300 , 000 men die as a result of pca each year . 
this stark figure , together with the knowledge that overtreatment comes with the high price of prevalent life - changing side effects , illustrates the need for tools to selectively identify high - risk pca ( those tumors with a high propensity to metastasize ) at an early stage , while the disease is potentially curable . research is ongoing into methods to address this need and better risk - stratify patients . 
urinary analysis of molecular correlates of aggressive disease could be used to triage patients and identify those who actually require an invasive prostate biopsy to histologically diagnose and grade their disease . in 2012 , movember launched four collaborative global action plan ( gap ) initiatives , focusing on pca biomarkers in urine , plasma , serum , and exosomes . 
 underpinning this aim was the cooperative establishment of prebiopsy postdigital rectal examination ( dre ) urine biorepositories at each institution , with a confederated database housing accompanying clinical , pathologic , and lifestyle data . 
six centers from the united states ( emory healthcare , atlanta , ga ) , canada ( university health network and lunenfeld - tanenbaum research institute , sinai health systems , toronto ) , and europe ( st jamess hospital , mater misericordiae university hospital , and tallaght hospital , all in ireland ; norfolk and norwich university hospital , england ) , collected prebiopsy , postdre urine ( 50 ml ) between january 2012 and october 2015 . 
exclusion criteria included previous diagnosis of pca , active urinary tract infection , recent prostate biopsy or transurethral resection of the prostate ( less than 6 wk ) , and confirmed presence of metastatic disease ( by pelvic magnetic resonance imaging or bone scan )  . 
 in total , urine samples were collected from 503 men , with matched formalin - fixed paraffin embedded trus biopsy cores acquired , where available ( fig 1 )  . 
in addition to this prebiopsy population , a retrospective analysis of the epicapture gene loci was performed on two independent cohorts of prostate tissues ( fig a2 ; data supplement )  . sample collection , processing , and epicapture analysis urine samples were stored on ice and processed within 4 hours of collection , following a movember gap1 standard operating procedure . 
details of nucleic acid isolation and quantification and epicapture analysis are provided in appendix table a1 and the data supplement . statistical analysis statistical analyses were performed with r version 3.4.1 and graphpad prism version 6 . 
 clinical utility was assessed by decision curve analysis ( dca ) .16 results epicapture genes demonstrate prognostic utility in prostate tissues mindful that most potential biomarkers fail to translate to the clinic , 17 we first set out to verify the prognostic utility of each epicapture constituent gene by measuring its methylation in two independent cohorts of radical prostatectomy samples . 
there was strong evidence for differences in mean methylation - values between four different groups ( benign , low - risk , aggressive , and metastatic pca ) in a small cohort of prostate tissues ( subjected to epithelial cell enrichment ) measured using the infinium humanmethylation450 beadchip ( fig 2a )  . 
 extracting freely available data from the same analytical platform for a larger the cancer genome atlas cohort yielded similar results ; each epicapture gene demonstrated significantly higher levels of dna methylation in clinically significant and high - risk tumors , relative to histologically benign tissue ( fig 2b )  . 
logistic regression models were developed using a 319 - specimen training set ( corresponding to 70% of the total cohort ) and then evaluated for their ability to correctly predict cancer / high - grade cancer / high - risk cancer in the remaining test set . 
not forgetting the clinical significance of gleason 7 disease , we also applied the revised five - grade grouping system , 18 with a view to detecting group 3 ( gleason 4 and 3 ) and above . 
the combination of epicapture and psa gave the best model ( auc , 0.82 ; sensitivity , 0.73 ; specificity , 0.76 ; appendix fig a1 ; appendix table a2 )  . we next evaluated the training set data to select an epicapture score cutoff that could best inform the decision on whether to perform a biopsy . 
finally , dca showed that at this threshold , epicapture demonstrated a net benefit over psa in the decision on whether to perform a biopsy , enabling a 15% reduction in prostate biopsies ( figs 3i and 3j )  . epicapture genes show high reproducibility by independent analysis to examine the robustness of epicapture , a matched quantitative methylation specific pcr analysis of two of the panel ( g1 : gstp1 , and g5 : apc ) was carried out in two independent laboratories on 236 of the urine samples . 
 ( a ) laser capture microdissected enriched prostate epithelial cells from benign prostate tissue ( procured from men undergoing radical cystoprostatectomy for bladder cancer , with no clinical or histologic evidence of prostate cancer [ pca ] ) and low - risk , aggressive , and metastatic pca . 
 ( b ) data extracted from the tcga repository for matched - benign prostate tissue and low - risk , significant , and high - risk pca , all procured from men undergoing radical prostatectomy . 
the performance of epicapture compared with / in conjunction with prostate - specific antigen ( psa ; treated as a continuous variable ) in the test set ( n = 134 ) for predicting each end point was assessed by receiver operating characteristic curves : ( a ) cancer ( v no cancer detected on transrectal ultrasound biopsy ) , ( b ) high - grade cancer ( gleason score greater than or equal to 8 v all else ) , ( c ) damico high - risk cancer ( v all else ) , and ( d ) capra ( cancer of the prostate risk assesment ) high - risk cancer ( v all else )  . 
the distribution of epicapture scores in the whole study population ( n = 453 ) , viewed by ( e ) biopsy outcome , ( f ) gleason grade , ( g ) risk categorization by damico risk - classification systems , and ( h ) risk categorization by capra risk - classification systethe epicapture score was calculated for each sample by summing the normalized index of methylation ( data supplement ) for g1 to g6 . 
epicapture score distributions were analyzed by t test or one - way analysis of variance ( anova ) , followed by post hoc analyses using the tukey - kramer multiple comparisons test . 
furthermore , matched data were available for 18 of 30 high - risk / grade samples that were epicapture negative , of which 15 ( 83.33% ) and 16 ( 88.89% ) were also negative for g1 and g5 , respectively , in the independent analysis . parallel epicapture analysis in urine and matched biopsy cores highlights value of liquid biopsy pca is renowned for its multifocal nature . 
matched formalin fixed paraffin - embedded biopsy cores were available for a proportion of patients , enabling parallel epicapture analysis on multiple tumor foci and urine from individual men ( n = 15 )  . 
the most interesting insights came from the matched analysis of urine with multiple biopsy cores , of which two notable cases are highlighted . patient sjh149 was diagnosed with a minute focus of gleason score 6 adenocarcinoma . 
this finding could suggest that the source of the tumor dna analyzed in urine could have been the high - grade tumor , which was not sampled on the original biopsy . 
 in contrast , patient sjh189 was diagnosed with a high - percentage , high - grade ( intermixed patterns of grade 4 and 5 ) pca on both sides of his prostate . 
so , despite pathologic heterogeneity within the gland , the three tumor areas seemed to be epigenetically homogeneous . discussion in this urine pca biomarker study , we evaluated the performance of epicapture , a six - gene dna methylation panel , for noninvasive detection of pca and more specifically high - grade or high - risk pca in urine from patients referred for prostate biopsy on the basis of elevated psa and / or abnormal dre . 
complying with remark guidelines , we describe a new dna methylation - based urine test for early detection of aggressive pca . many prostate tumors display a protracted disease trajectory , almost indolent in behavior.19 the widespread use of the serum psa test in many countries has significantly increased the incidence and thus overtreatment of these lowrisk cancers with little likelihood of clinical manifestation.20 - 23 an important first consideration in developing epicapture was to therefore critically appraise the evidence for prognostic utility of each constituent gene . 
conversely , however , it is estimated that approximately two thirds of men undergoing invasive prostate biopsy have no tumor diagnosed , because of the high false positive rate of serum psa.23 , 24 as such , millions fig 3 . 
 ( i ) decision curve analysis demonstrated net clinical benefit of performing biopsy on patients in the test set on the basis of an epicapture score greater than 1.25 versus psa greater than or equal to 3 ng / ml across a range of clinically relevant threshold probabilities ( the risk of cancer , such that a patient would choose to undergo biopsy by weighing the relative harms of false - positive and false - negative predictions )  . 
 ( a ) two of the six epicapture assays ( g1 : gstp1 and g5 : apc ) were analyzed independently in laboratories in ireland ( perry ) and canada ( bapat ) by quantitative methylation specific pcr in urine sediments from 236 of 453 men in the study . 
 relevant subsets were then considered by applying the study end points : ( b ) men with biopsy - positive disease , ( c ) men with high - grade ( gleason score greater than or equal to 8 ) prostate cancer , and men with highrisk prostate cancer defined by ( d ) damico , and ( e ) capra ( cancer of the prostate risk assessment ) classification . 
 repeat biopsy ( 8 months later ) sjh149 urine biopsy core ( s ) sample type base apex base apex histologically benign gleason 6 gleason 7 gleason ( cid : 116 ) 8 urine tissue sjh189 urine biopsy core ( s ) sample type fig 5 . 
 tumor presence is denoted by pink ( gleason score 6 ) , red ( gleason score 7 ) , or brown ( gleason score greater than or equal to 8 ) circles , with size indicative of percentage tumor in each core . 
 ( a ) low - risk prostate cancer sjh149 ( 62 years of age ; prostate - specific antigen , 3.08 ng / ml ) demonstrated that urine as a liquid biopsy is a viable alternative to sampling bias inherent to tissue needle biopsies . 
 sophisticated imaging technologies , such as magnetic resonance imaging , may improve the accuracy of prostate biopsy , 30 their widespread application is hampered by high cost , access to specialist equipment and personnel , interobserver subjectivity , and requirement for anesthesia . 
alternatively , transperineal biopsy enables a more complete sampling of the gland , including the anterior prostate , but also requires anesthesia and is thus unsuitable as a population - based detection method for such a prevalent disease . the dearth of blood - based prognostic biomarkers as a screening tool for aggressive pca in conjunction with limitations of the prostate biopsy in its various forms has led to excitement around urine biomarkers . 
physical manipulation of the prostate by dre , followed by a first - void urinalysis , could provide a simple , holistic insight into molecular alterations occurring in the prostate gland . 
indeed , many studies have demonstrated significant value in detecting and noninvasively monitoring several genitourinary malignancies through urine.31 - 34 some other prognostic urine indicators of aggressive pca have already been described . 
early studies demonstrated detection of gstp1 methylation in urine from patients with pca , although sensitivity was poor ( less than 30% ) .39 follow - up work expanded the repertoire of markers ( gstp1 , apc , and rar2 ) , which improved sensitivity to approximately 60%.40 the epicapture panel represents five commonly perturbed pathways in pca : intracellular detoxification , wnt and igf axes , cell cycle , and prostaglandin biosynthesis . 
in contrast , applying an epicapture threshold ( greater than 0.73 ; developed on training set ) did not markedly alter its diagnostic performance ( auc , 0.68 ) and delivered a 79% improvement over the tumor specificity of psa . in an effort to address the prognostic utility of epicapture within the context of the clinically heterogeneous gleason 7 disease , we applied the revised five - grade grouping system , 18 in addition to two widely used risk - classification systems . 
the epicapture performance characteristics represent a potential improvement on existing methods for patient stratification and for determining the need to perform biopsy , detecting 85% of highgrade tumors , with an npv of 98% . 
furthermore , the overlap of gstp1 and apc in the two gap1 urine dna methylation biomarker panels revealed excellent correlation in detection of aggressive pca , illustrating the robustness of these biomarkers . 
in the context of the diagnostic gray zone , psa 4 to 10 ng / ml , epicapture demonstrated potential for further classifying patients , positive in 40% of men with highgrade pca . 
 although these data are promising , a large prospective clinical trial is needed to assess whether epicapture offers a survival advantage . a limitation of our study is that the cohort is young ; analysis was only possible using biopsy as the end point . 
we cannot rule out the possibility that a proportion of our epicapture - positive urine samples in men with low - grade or benign tissues were indeed tumor cases missed on biopsy . 
evidence actually shows that dna methylation detected in histologically benign tissue ( due to an epigenetic field effect from the cancer ) , can be used as a tool to rule out the possibility that the biopsy missed the tumor . 
 for example , the confirm mdx test , which measures dna methylation at three genes ( gstp1 , apc , and rassf1 ) in histologically benign biopsy tissue cores , is used to guide the decision to repeat a biopsy.41 conversely , 14 of 47 ( 29.79% ) high - grade tumors were epicapture negative . 
independent analysis revealed concordant negativity in more than 80% of these men , and lowering the epicapture threshold did alter this result ; they were negative across all six markers . 
we believe that the most likely reason is interoperator differences in dre ; these high - risk / grade cancers were epicapture negative because they had insufficient / undetectable prostate cells present in their urine . 
 relationships may not relate to the subject matter of this enable confirmation of the presence of prostate cells in the urine , validating its suitability for epicapture analysis and ultimately improving the performance of the test . 
future work will also investigate the intra - individual reproducibility of epicapture by repeated measures in men . finally , to the best of our knowledge , this is the first pca biomarker study to perform a matched analysis of tissue and liquid biopsies . 
a more extensive project is now warranted to fully assess the effects of the multifocal nature of pca on signatures derived from liquid biopsies . epicapture could be used in conjunction with existing tools ( ie , psa and risk calculators ) to help guide the decision to biopsy . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . eve o ' reilly no relationship to disclose alexandra v . 
dale no relationship to disclose rick brugman no relationship to disclose gavin clarke no relationship to disclose olivia schmidt no relationship to disclose shane o ' meachair no relationship to disclose dattatraya patil no relationship to disclose kathryn l . 
pellegrini no relationship to disclose julia garcia no relationship to disclose fang zhao no relationship to disclose stephen finn honoraria : roche robert mills no relationship to disclose marcelino y . 
gallagher employment : oncomark leadership : oncomark neil fleshner honoraria : amgen , janssen oncology , bayer , sanofi , abbvie , ferring pharmaceuticals , astellas medivation consulting or advisory role : hybridyne health research funding : ferring ( inst ) , astellas pharma ( inst ) , janssen oncology ( inst ) , amgen ( inst ) , nucleix ( inst ) , progenix ( inst ) , spectracure ab ( inst ) research funding : amgen ( inst ) travel , accommodations , expenses : pfizer stock and other ownership interests : oncomark consulting or advisory role : carrick therapeutics research funding : carrick therapeutics patents , royalties , other intellectual property : two patents which have been licensed to oncomark travel , accommodations , expenses : oncomark rustom p . 
brewer patents , royalties , other intellectual property : patents held in drug discovery with novartis ( i ) , patents pending concerning cancer subtype detection and biomarkers with university of east anglia bharati bapat no relationship to disclose martin g . 
perry patents , royalties , other intellectual property : university college dublin holds a patent that relates to this work acknowledgment we thank the urologists and their teams at participating hospitals and the health research boardfunded dublin centre for clinical research network , affiliated research nurses , and technical staff , in particular john mccourt . 
we thank investigators drs robert vessella , and colm morrissey , and the patients and families who participated in the prostate cancer donor program at the university of washington medical center . 
bristow , director , manchester cancer research centre , chief academic officer and honorary consultant , christie nhs trust , university professor of cancer studies , university of manchester , manchester cancer research centre , university of manchester , manchester , uk . chris parker , royal marsden hospital , sutton , uk . ian mills , queens university belfast , centre for cancer research and cell biology , movember / prostate cancer uk centre of excellence , school of medicine , dentistry , and biomedical sciences . 
sanda , emory university school of medicine , atlanta , ga ; neil fleshner , julia garcia , fang zhao , and bharati bapat , university of toronto , toronto , ontario , canada ; robert mills , norfolk and norwich university hospital ; marcelino y . 
brewer , earlham institute , norwich , england . supported by grant funding from movember ( gap1 urine biomarker award ) , us prostate cancer foundation ( young investigator award , a.s.p. ) , science foundation ireland grants no . 
bastian pj , ellinger j , heukamp lc , et al : prognostic value of cpg island hypermethylation at ptgs2 , rar - beta , ednrb , and other gene loci in patients undergoing radical prostatectomy . 
damico av , whittington r , malkowicz sb , et al : biochemical outcome after radical prostatectomy , external beam radiation therapy , or interstitial radiation therapy for clinically localized prostate cancer . 
cooperberg mr , pasta dj , elkin ep , et al : the university of california , san francisco cancer of the prostate risk assessment score : a straightforward and reliable preoperative predictor of disease recurrence after radical prostatectomy . 
vickers aj , cronin am , roobol mj , et al : a four - kallikrein panel predicts prostate cancer in men with recent screening : data from the european randomized study of screening for prostate cancer , rotterdaclin cancer res 16 : 3232 - 3239 , 2010 29 . 
siddiqui mm , rais - bahrami s , turkbey b , et al : comparison of mr / ultrasound fusion - guided biopsy with ultrasound - guided biopsy for the diagnosis of prostate cancer . 
costa vl , henrique r , danielsen sa , et al : three epigenetic biomarkers , gdf15 , tmeff2 , and vim , accurately predict bladder cancer from dna - based analyses of urine samples . 
torres - ferreira j , ramalho - carvalho j , gomez a , et al : mir - 193b promoter methylation accurately detects prostate cancer in urine sediments and mir - 34b / c or mir - 129 - 2 promoter methylation define subsets of clinically aggressive tumors . 
wei jt , feng z , partin aw , et al : can urinary pca3 supplement psa in the early detection of prostate cancer ? j clin oncol 32 : 4066 - 4072 , 2014 35 . 
leyten gh , hessels d , jannink sa , et al : prospective multicentre evaluation of pca3 and tmprss2 - erg gene fusions as diagnostic and prognostic urinary biomarkers for prostate cancer . 
van neste l , partin aw , stewart gd , et al : risk score predicts high - grade prostate cancer in dna - methylation positive , histopathologically negative biopsies . 
 ( a ) the performance of epicapture compared to and in conjunction with prostate - specific antigen ( psa ; treated as a continuous variable ) in the test set ( n = 134 ) for predicting isup group 3 , 4 and 5 pca on biopsy was assessed by receiver operator characteristic curves . 
 ( b ) the distribution of epicapture scores in biopsy - negative ( no cancer detected ) v biopsy positive patients , categorized by isup group , shows increasing methylation by group . 
epicapture was performed in urine and matched formalin - fixed paraffin embedded biopsy cores from randomly selected biopsy - positive ( n = 15 : low - risk [ capra and damico , gleason score 6 ; intermediate risk , gleason score 7 ; and high risk , gleason score 8 ] ) patients . 
dna methylation of each gene is indicated by the nim ( normalised index of methylation ) , and for the collective panel , by the epicapture score ( nim sum g1 - g6 )  . 
each point represents a single sample ( biopsy core or urine ) , with the mean for each group indicated by a horizontal line ( yellow , urine ; blue , tissue )  . 
 c wide and cystic brain metastases reveal ret - rearranged nonsmall - cell lung cancers francesco facchinetti , md , msc1 , 2 ; francesca bozzetti , md1 ; letizia gnetti , md1 ; roberta minari , phd1 ; pellegrino crafa , md1 ; sara elena rebuzzi , md1 ; roberto ferrara , md3 ; elisa gruppioni , phd4 ; elisa capizzi , phd4 ; ermanno giombelli , md1 ; girolamo crisi , md1 ; annalisa altimari , phd4 ; and marcello tiseo , md , phd1 , 5 introduction the detection of specic molecular activations ( eg , egfr , alk , ros1 , braf , met , ret ) is the basis of effective targeted treatments in nonsmall - cell lung cancer ( nsclc ) .1 in this eld , novel selective inhibitors extend survival outcomes , coupling global prolonged disease control and meaningful activity against metastases developing in the cns.2 lung tumors harboring egfr mutations or alk , ros1 , or ret rearrangements have a tendency toward more frequent cns spreading compared with wild - type ( wt ) nsclc.3 - 5 peculiar neuroradiologic characteristics have been reported for brain metastases from alkpositive nsclc , in terms of cystic aspects acquired after crizotinib treatment.6 - 8 such features can even be misleading , because intracranial cystic lesions from alk - rearranged tumors may be attributed to infectious diseases.9 here we report the histories of two patients presenting with wide cystic brain lesions that were neurosurgically removed and discovered to be metastases from ret - rearranged nsclc . 
brain computed tomography ( ct ) scan and magnetic resonance imaging ( mri ) were performed , documenting a unique bulky cystic - like lesion in the frontal region of the left hemisphere , the morphologic and functional characteristics of which were pathognomonic for an anaplastic astrocytoma ( fig 1 )  . 
a chest x - ray revealed a parahilar lesion of the left lung . diagnosis and staging neurosurgery was then performed with the radical removal of the wide cerebral lesion , the intraoperative macroscopic aspects of which were still in keeping with an anaplastic astrocytoma . 
the postoperative course was uneventful , with a rapid neurologic improvement . the histologic examination revealed a large ( 40 25 20 mm ) lesion , conrming the cystic structure that was evident at sampling ( fig 2a )  . 
ct and pet scans revealed a mass in the left pulmonary hilum and ipsilateral and contralateral lymph nodes ( ct4n3m1b according to tnm staging classication [ eighth edition ] ; fig 3 )  . 
considering the radiologic , pathologic , and molecular elements , which were clearly in line with a diagnosis of advanced nsclc , biopsies of the lung and nodal lesions were not performed . molecular analyses neither the molecular analyses nor ihc performed on the brain metastasis detected egfr , braf , or kras mutations or alk or ros1 rearrangements ; programmed death - 1 ligand ( clone sp263 ) was expressed by 10% of tumor cells . 
next - generation sequencing with a 52 - gene panel ( ion torrent oncomine focus assay kit ; thermo fisher scientic , waltham , ma ; gene list provided in data supplement ) was performed , and a kif5b - ret fusion was found ( figs 4a and 4b )  . 
ret rearrangement was conrmed by uorescence in situ hybridization analysis in 52% of tumor cells ( fig 4c )  . treatment received rst - line chemotherapy with the patient cisplatin and pemetrexed . 
postoperative stereotactic brain radiotherapy ( sbrt ) to the resection cavity was not performed , because available evidence supporting sbrt for better local control has not yet indicated a survival benet.10 , 11 brain mri after 4 months revealed normal surgical outcomes , with no residual disease . 
ct scan after four courses of cisplatin plus pemetrexed showed partial disease response , so the patient was switched to pemetrexed maintenance , four cycles of which led to further reduction of lymph node size , with continuing absence of brain disease on mri . 
no evidence is available concerning ret - rearranged nsclc , an entity of emerging interest given the current development of selective ret inhibitors , also active against cns disease . knowledge generated here we report the similar clinical histories of two patients with ret - positive nsclc , whose diagnoses were obtained on pathologic and molecular analyses performed on wide , cystic , and symptomatic brain metastases with a peculiar neuroradiologic presentation . relevance a characteristic behavior of cns lesions from ret - rearranged nsclc was recognized . 
the current or upcoming availability of selective , cns - active ret inhibitors strongly reinforces the importance of wide molecular screening of cns lung metastases , even more so in the presence of the reported neuroradiologic and pathologic features of brain lesions . the abrupt onset of dizziness , worsening headache , difculty with handgrip , and right homonymous hemianopsia . the observation of a large and cystic - like brain lesion in the left parietal - occipital region was followed by a contrastenhanced mri ( fig 5 )  . 
the brain imaging was suggestive for metastases from an extracerebral tumor . diagnosis and staging the whole - body ct scan documented a mass in the upper left lung lobe , with ipsilateral and contralateral nodal volvement in the hilar - mediastinal and retro - clavicular regions ( fig 6 ) , with clinical staging determined as ct2an3m1c . given the persisting neurologic symptoms , the patient underwent neurosurgery . the pathologic examination conrmed the radiologic hypothesis of a cavitated cystic ( fig 2f ) brain metastasis ( 40 30 20 mm ) from a lung tumor ( figs 2g to 2i )  . 
 ( a ) t1 weighted imaging ( wi ) and ( b ) t2 wi sequences show a well - delineated ( a ) hypointense and hyperintense mass in left frontal lobe cortex involving the subcortical area and deep white matter , ( c ) without dense dystrophic calcication or hemosiderin staining on t2 * gre . 
 ( d ) ttf - 1 ( 40 ) and ( e ) napsin a ( 40 ) immunohistochemistry showed diffuse ( d ) nuclear and ( e ) cytoplasmic positivity . 
 ( a ) a left parahilar lesion conditioning atelectasis was detected , together with ( b ) ipsilateral and ( c ) contralateral pathologic lymph nodes . elements supporting the diagnosis of nsclc , biopsies of the primary tumor and lymph nodes were not proposed . molecular analyses status of egfr , alk , ros1 , kras , braf , and met was found to wt , and ihc showed programmed death - 1 ligand ( clone sp263 ) negative status . 
again , targeted ngs was performed on the brain metastasis ( ion torrent oncomine focus assay kit ; thermo fisher scientic ; data supplement ) , and kif5b - ret fusion was revealed , conrmed by uorescence in situ hybridization analysis in 40% of tumor cells ( figs 4a to 4b and 4d )  . treatment because of the lack of trials with ret inhibitors in the rstline setting and the substantial benet potentially driven by pemetrexed , 12 pemetrexed was combined with cisplatin and administered as a rst - line treatment , once postsurgical recovery was complete . 
again , sbrt to the resection cavity was discussed but not performed , for the same reasons reported in the rst patient case15 , 16 and because of the presence of multiple brain metastases . 
 ( b ) next - generation sequencing analysis report showing the ret fusion with kif5b gene ( ion reporter software and irgv visualization [ thermo fisher scientic , waltham , ma ] ) detected in brain samples from patient cases 1 and 2 . 
t1 weighted imaging ( wi ) and t2 wi sequences show a well - delineated ( a ) hypointense and ( b ) hyperintense mass in left occipital lobe cortex , with a linear internal septum , involving the subcortical area and deep white matter , ( c ) without dense dystrophic calcication or hemosiderin staining on t2 * gre . 
 ( d ) axial t1 postcontrast imaging shows a large bilobed cystic - like supratentorial mass with ring enhancement , sharply delineated borders , and well - dened internal septu ( e ) the content is liquid , with no intralesional levels and with high diffusivity ( apparent diffusion coefcient , 0.00269 mm2 per second v csf , 0.00290 mm2 per second )  . 
similar radiologic appearance is shown by the following : ( g ) t1 wi before gadolinium administration , ( h ) t1 wi after gadolinium administration , and ( i ) t2 wi . imaging documented , in addition to the regular outcomes of the surgical intervention , signs of response in the two residual lesions ( data not shown )  . 
nevertheless , this was not conrmed in another series of ros1 - rearranged lung cancer with baseline brain involvement ; in that series , the ros1 partner gene was known in 17 patients for whom mri results were available.14 in ret - driven lung cancer , the most frequent fusion partner gene is kif5b , as observed in the two patient cases reported here . 
although no associations between ret partner genes and brain metastasis incidence have been anticipated , drilon et al5 reported that intracranial disease response to multitarget kinase inhibitors seemed to occur specically in nonkif5b - ret patient cases ( n = 2 of 5 ) , with no responses in the kif5bret patient cases ( n = 0 of 9 ) .5 at least ve cns responses to the selective ret inhibitor loxo - 292 were observed in ret - rearranged lung tumors ( n = 4 of 4 in the phase i study ) 15 , 16 harboring either kif5b ( n = 2 ) or non - kif5b ( clip - 1 ; n = 1 ) ret partner genes.15 - 17 because of the descriptive nature of our patient cases , no conclusion can be drawn with regard to a novel specic pattern of ret - rearranged lung tumors , potentially associated with large and cystic - like brain metastases at diagnosis . nevertheless , besides providing atypical and intriguing radiologic ndings , the surprising similarity between these two reports , together with the rarity of ret rearrangements in nsclc , suggests a characteristic behavior of cns lesions from this molecular subclass of tumors . 
these observations reinforce the importance of screening for nsclc molecular activations in addition to the canonical and frequent ones , with particular reference to ret fusions in the presence of atypical features of brain metastases . 
 ( a - c ) the lesion was not dissociable and was not completely distinguishable from an obstructive inammatory / atelectasic consolidation involving the entire lingula and part of the upper left lobe . 
 ( c , d ) bilateral hilar , mediastinal , and retro - clavicular lymph nodes were reported ( white arrows )  . involvement , with special regard to novel , specic agents , such as loxo - 292 and blu - 667.5 , 15 - 18 we hope that our two patients will not require further systemic treatment , meaning that their disease is controlled with the current chemotherapy and potential administration of radiotherapy . 
 large and cystic brain metastases from ret - rearranged nsclcs references reck m , rabe kf : precision diagnosis and treatment for advanced non - small - cell lung cancer . 
n engl j med 377 : 849 - 861 , 2017 remon j , besse b : brain metastases in oncogene - addicted non - small cell lung cancer patients : incidence and treatment . 
front oncol 8 : 88 , 2018 tan l , wu y , ma x , et al : a comprehensive meta - analysis of association between egfr mutation status and brain metastases in nsclc . 
pathol oncol res 25 : 791 - 799 , 2019 gainor jf , tseng d , yoda s , et al : patterns of metastatic spread and mechanisms of resistance to crizotinib in ros1 - positive nonsmall - cell lung cancer . 
j clin oncol 32 : e122 - e124 , 2014 saraceni c , li pm , gainor jf , et al : cystic brain metastases in nsclc harboring the eml4 - alk translocation after treatment with crizotinib . 
narayanan v , honce mj , mehrotra s , et al : cystic brain metastases occurring in anaplastic lymphoma kinase gene rearranged non - small - cell lung cancer patients receiving crizotinib . 
clin lung cancer 17 : 85 - 90 , 2016 kim sh , hyun jw , kim hj , et al : de novo cystic brain lesions mimicking neurocysticercosis in alk - positive lung cancer . 
mahajan a , ahmed s , mcaleer mf , et al : post - operative stereotactic radiosurgery versus observation for completely resected brain metastases : a single - centre , randomised , controlled , phase 3 trial . 
patil t , smith de , bunn pa , et al : the incidence of brain metastases in stage iv ros1 - rearranged non - small cell lung cancer and rate of central nervous system progression on crizotinib . 
drilon a , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
oxnard g , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer . 326 , 2013 27 : 1286 - 1291 , 2016 j thorac oncol 13 : 987 - 995 , 2018 oncol 36 , 2018 ( suppl ; abstr 102 ) j thorac oncol 13 : s349 - s350 , 2018 17 . 
 circulating tumor dna in nonsmall - cell lung cancer : a primer for the clinician circulating tumor dna ( ctdna ) consists of short , double - stranded dna fragments that are released into the circulation by tumor cells . 
the assays noninvasive nature , ability to reflect intratumoral heterogeneity , short turnaround time , and ability to obtain serial samples make it an attractive option compared with traditional tissue biopsy tumor sequencing . 
currently , this technology is mostly being used for the detection of egfr mutations in patients with advanced nonsmall - cell lung cancer where tissue is inadequate to detect egfr mutations that drive acquired resistance , most notably egfr t790m . 
emerging uses include the incorporation of ctdna testing into primary diagnosis , treatment monitoring , detection of minimal residual disease , and detection of early - stage disease in screening populations . 
2017 by american society of clinical oncology introduction including tumors , shed short , several tissues , double - stranded dna fragments called cell - free dna ( cfdna ) into the circulation.1 - 3 certain conditions that cause tissue damage , such as myocardial infarction , trauma , and cancer , can result in increased concentrations of cfdna.3 the cfdna derived from tumors , known as circulating tumor dna ( ctdna ) , is a product of apoptosis and necrosis and is distinguished from other cfdna by the presence of somatic mutations representative of tumor biology absent in normal cells . 
90% of all dna present in the plasma.4 , 5 in patients with advanced nonsmall - cell lung cancer ( nsclc ) , ctdna detection rates that range from 80% to  . 
unlike acquired t790m resistance to egfr tkis , one dominant secondary mutation appears not to exist , and second - generation alk inhibitors have shown high response rates in patients previously treated with crizotinib regardless of the presence of secondary alk mutations , which makes the role of a repeat biopsy less clear.27 however , emerging data suggest that specific secondary resistance alk mutations have important therapeutic implications . 
in a study that detected egfr mutations by an ngs assay , the sensitivity for urine was 93% for t790m , 80% for l858r , and 83% for exon 19 deletions . 
in nine patients monitored while receiving the third - generation egfr inhibitor rociletinib , a rapid decrease in urine ascopubs.org / journal / po jco precision oncology 7 t790m was 70% , and the objective response rate and median progression - free survival ( pfs ) with osimertinib were similar in patients with t790mpositive plasma or tumors.10 this finding suggests that with the use of ctdna testing , many patients can avoid a biopsy for t790m genotyping . 
however , because of the 30% false - negative rate of plasma genotyping , those with t790m - negative plasma still need to undergo tumor biopsy to determine the presence or absence of t790m.10 in addition to cases where ctdna is not detectable , tissue testing retains value in certain resistance mechanisms , such as small - cell transformation . thress et al24 performed ngs of cfdna from seven patients with t790m - mutated advanced lung cancer who had developed resistance to osimertinib and detected an acquired egfr c797s mutation . 
 t790m levels was observed by day 21.31 in a study of patients with t790m positivity , response was similar whether t790m status was identified by tissue , plasma ( through beaming ) , or urine ( through ngs ) .32 these data suggest that plasma and urine egfr analyses complement tissue biopsy specimen analysis in nsclc . brain metastasis is found in up to 40% patients with nsclc , 33 and ctdna analysis of patients with brain tumors has revealed either the absence or very low levels of tumor dna possibly as a result of the blood - brain barrier.34 one study used hybridization capturebased sequencing and ddpcr to characterize ctdna in csf of patients with brain lesions ( including brain metastasis from lung cancer ) and compared it with plasma ctdna.35 the authors concluded that csf ctdna has a significantly higher sensitivity than plasma for cns genomic alterations like egfr , pten , esr1 , idh1 , erbb2 , and fgfr2 and can be used to detect brain tumor mutations and monitor brain tumor progression ( sensitivity of ctdna was 58% v 0% in csf and plasma , respectively , in cns - restricted disease )  . 
hata et al37 investigated the response to osimertinib in 10 patients with leptomeningeal disease and showed that the drug might be more effective in csf of patients with t790m positivity than in those without csf t790m positivity . multigene testing as the number of genomic targets with matched therapies grows , the national comprehensive cancer network guidelines for nsclc recommend expanded genomic testing , including for egfr , alk , erbb2 , braf , met , ros1 , and ret.5 , 15 , 38 testing for all these alterations in addition to histopathologic and immune biomarker assessment pose a challenge when tissue biopsy samples are insufficient . 
in a study of patients with advanced nsclc , a tissue biopsy specimen with sufficient quality and quantity of dna for ngs was unobtainable for 52 ( 51% ) of 102 patients.7 two studies used ngs - based ctdna assays to evaluate , with high overall accuracy , somatic genomic profiles in patients with advanced nsclc  . 
15 , 000 patients with advanced - stage cancer with a concordance of 87% with matched tumor samples that increased to 98% when plasma and tissue testing was done , 6 months apart . 
the study detected actionable mutations in biopsy specimens with insufficient tissue ( alk fusion , egfr or braf activating mutations ) and with actionable resistance mutations at the time of progression ( met amplification or egfr t790m ) as well as in undergenotyped tumors ( braf v600e , or erbb2 indel )  . identification of nontargetable oncogenic drivers , such as kras mutations , that preclude the presence of other targetable alterations also guides clinicians to rapidly initiate alternative therapies , such as chemotherapy or immunotherapy.5 the detection of variants in other genes may lead to the off - label use of fda - approved therapies or enrollment in clinical trials of new therapeutic agents.7 several combinations of targeted therapies are based on resistance mechanisms and are being evaluated in lung cancer ( eg , mek and pi3k inhibitors in combination with egfr tkis ) , 41 which again underscores the need for real - time tumor genotyping to assess for resistance pathways . 
chabon et al43 identified several resistance mechanisms , including met , egfr , pik3ca , errb2 , kras , and rb1 , in patients with t790mmutated nsclc who received rociletinib . 
the study used cancer personalized profiling by deep sequencing ctdna analysis and found that 46% of patients ( 19 of 41 ) with t790m mutations had additional potential resistance mutations in the pretreatment plasma . 
this coexistence of different resistance mechanisms in the same patient may affect response to subsequent egfr tkis like rociletinib . treatment monitoring ctdna offers the possibility of serial testing for molecular monitoring of disease . 
 studies have demonstrated the predictive value of quantitative changes in egfr mutations in ctdna at various time points during tki treatment.1 a prospective analysis to validate ddpcr for the detection of common egfr and kras mutations in patients with advanced nsclc demonstrated that patients with complete resolution of ctdna at either 2 or 6 weeks after treatment exhibited a treatment discontinuation rate of 0% at the initial and 4% at the second imaging assessment . 
patients without complete resolution exhibited a treatment discontinuation rate of 33% at initial and 56% at second imaging . these patterns were postulated to correlate with radiographic response and emergence of acquired resistance.4 marchetti et al44 performed pcr and ultradeep ngs on serial plasma samples from 20 patients with advanced nsclc and known tissue and plasma egfr mutations before tki treatment . 
rapid responders who had at least a 50% decrease in plasma egfr copy number at 14 days had a greater mean percentage of tumor shrinkage than slow responders ( n = 6 ; 70% v 30% )  . 
a phase iii study evaluated egfr mutations in cfdna of patients randomly assigned to receive gemcitabine and platinum plus sequential erlotinib or placebo by using a cobas test.46 for patients treated in the erlotinib arm who were cfdna egfr positive at baseline , the disappearance of cfdna at cycle 3 was associated with significantly improved pfs ( hr , 0.38 ) and longer os ( hr , 0.45 ) compared with patients with persistence of cfdna egfr . the prognostic value of dynamic changes in ctdna has also been evaluated . 
additional studies are needed to evaluate end points such as pfs , os , and quality of life as a result of early detection of resistance . monitoring for minimal residual disease another potential application of ctdna is to evaluate for minimal residual disease ( mrd ) after curativeintent therapy , such as surgery and radiation.8 chaudhuri et al48 applied cancer personalized profiling by deep sequencing to detect ctdna in preand post - treatment blood samples from 41 patients with nonmetastatic lung cancer treated with chemoradiation , radiation , or surgery . 
these patients positive for mrd had a significantly worse outcome than patients without detectable ctdna mrd within 4 months of definitive treatment ( 3 - year freedom from progression , 0% v 92% [ hr , 38 ] ; 3 - year os , 8% v 75% [ hr , 12 ] )  . these data suggest that patients with residual ctdna after definitive treatment will be enriched for those who will ultimately develop recurrence . 
ctdna detection might facilitate the development of clinical trials that evaluate the escalation of therapy for patients at high risk for recurrence and the de - escalation of therapy for patients without residual disease . role in early diagnosis / screening the role of ctdna in early - stage disease also is being studied . 
bettegowda et al34 evaluated the ability of ctdna to detect tumors in patients with various malignancies at various clinical stages . forty - seven percent of patients with stage i cancers ( n = 49 ) had detectable ctdna , with the fraction of patients with detectable ctdna being 55% , 69% , and 82% for those with stage ii , iii , and iv cancers , respectively.34 trials are under way to assess the feasibility and utility of ngsbased ctdna to detect early - stage cancers in high - risk patients ( clinicaltrials.gov identifier : nct02612350 ; also project lunar48a )  . 
 mutation of interest in the patients tumor needs to be known to send for appropriate genomic panels . ctdna may be detectable before radiographically detectable disease , which raises the issue of managing such patients . 
nevertheless , early cancer detection remains a promising new avenue for ctdna that needs additional research . ctdna in the era of immune checkpoint therapy in the era of immune therapy for advanced nsclc , a key issue is the elucidation of a biomarker that can predict response and monitor disease . 
tumor dna sequencing has been shown to be a surrogate for total mutation burden , which predicts response and pfs with antiprogrammed death 1 inhibitors like pembrolizumab.49 however , total mutation burden analysis has been investigated only in tumor tissue , and a better understanding of ctdna is required before it can be applied for this purpose . lipson et al50 analyzed the ctdna of 12 patients with metastatic melanoma who underwent treatment with checkpoint inhibitors for the presence of hotspot somatic mutations in braf , ckit , nras , and tert by using beaming . 
hence , a negative result could signify that the tumor is not actively shedding ctdna , the patients disease is adequately controlled by therapy , or somatic variants either were not covered or were below the detection limit for the assay.7 in addition , any negative test result will need to be viewed in the overall context of ctdna and other molecular results . 
for example , in a patient with an egfr - mutated nsclc in the setting of acquired resistance , a negative egfr t790m test result is more likely to be a true negative if the original egfr mutation was detected with a significant allele frequency versus if the ctdna test did not identify either mutation . confidence in a positive test result extremely high analytic specificity and a positive predictive value that approaches 100% make false positives unlikely , so if a mutation is detected , it can be relied on as a true result . 
as expected , the allelic fraction of variants detected in ctdna is usually much smaller than that in tissue dna given that tumor - derived dna may be more diluted in the blood than in the tissue.7 the rare false positive result ( particularly t790m ) in plasma may be indicative of tissue heterogeneity in which the mutation was not identified but is present in tissue , which may be due to the timing of the biopsy and the location of the biopsy needle in the tumor . 
the only definitive method to clinically validate that the mutations detected in plasma are an accurate molecular proxy of disease biology in the context of it being absent in tissue is to correlate them with response to targeted inhibition . in the case of mutational events that are exclusive to certain types of cancers ( eg , egfr exon 19 deletion to nsclc ) , confidence of a positive result is higher than in genes that can be mutated in a variety of settings ( eg , tp53 )  . 
for instance , a small allelic fraction tp53 mutation in ctdna can originate from many sources ( eg , myelodysplastic syndrome ) , and in such cases , confidence is increased if the same mutation also has been detected in tumor . detection of concurrent malignancy / germline alterations the testing of cfdna will detect all dna that sheds into the circulation , and some findings may not be expected in the tumor of origin , may not match tumor tissue dna results , and may affect genes that are mutated in different tumor types ( eg , tp53 )  . 
a potential for detection of incidental hematologic malignancies exists , which , naturally , have high tumor burden in the blood , and results can be confounded by foreign dna , such as after transfusion or organ transplantation . another issue similar to what is seen with tissue genotyping is that one needs to be cautious about distinguishing somatic ( tumor ) versus germline alterations because germline dna is not analyzed in parallel . 
any mutation that affects genes implicated in familial syndromes should be considered specifically ( eg , brca ) , and mutations with high allele frequency ( between 30% and 70% ) should raise the possibility of being potentially associated with heterozygous germline mutation syndromes . in conclusion , tissue biopsy remains essential at least for primary diagnosis because tissue yields information about morphology , tumor type , site of origin , and the immune microenvironment . 
for instance , erbb2 ( her2 ) copy number amplification in nsclc does not predict tki response like it does in breast cancer.5 currently best validated in egfr - mutated lung cancer for primary molecular diagnosis and for egfr t790m testing , ctdna has proven to have excellent utility as a complement to tissue - based testing . 
singh no relationship to disclose xiaoling guo no relationship to disclose haiying cheng honoraria : astrazeneca , boehringer ingelheim , clovis oncology benjamin levy honoraria : genentech consulting or advisory role : eli lilly , boehringer ingelheim , genentech , roche , astrazeneca , celgene , pfizer , merck speakers bureau : eli lilly , genentech , roche balazs halmos consulting or advisory role : astrazeneca , boehringer ingelheim , celgene , genentech , roche , pfizer , eli lilly , foundation medicine research funding : merck , astrazeneca , mirati therapeutics , boehringer ingelheim , roche , genentech , ariad pharmaceuticals affiliations aditi p . 
singh , haiying cheng , xiaoling guo , and balazs halmos , montefiore medical center , bronx , ny ; and benjamin levy , johns hopkins sidney kimmel comprehensive cancer center at sibley memorial hospital , washington , dc . references oncologist 21 : 1121 - 1130 , 2016 1 . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - small - cell lung cancer . 
li t , kung hj , mack pc , et al : genotyping and genomic profiling of non - small - cell lung cancer : implications for current and future therapies . 
luo j , shen l , zheng d : diagnostic value of circulating free dna for the detection of egfr mutation status in nsclc : a systematic review and meta - analysis . 
kimura h , suminoe m , kasahara k , et al : evaluation of epidermal growth factor receptor mutation status in serum dna as a predictor of response to gefitinib ( iressa )  . 
douillard jy , ostoros g , cobo m , et al : gefitinib treatment in egfr mutated caucasian nsclc : circulating - free tumor dna as a surrogate for determination of egfr status . 
mao c , yuan jq , yang zy , et al : blood as a substitute for tumor tissue in detecting egfr mutations for guiding egfr tkis treatment of nonsmall cell lung cancer : a systematic review and meta - analysis . 
liu y , liu b , li xy , et al : a comparison of arms and direct sequencing for egfr mutation analysis and tyrosine kinase inhibitors treatment prediction in body fluid samples of non - small - cell lung cancer patients . 
wang j , wang b , chu h , et al : intrinsic resistance to egfr tyrosine kinase inhibitors in advanced non - small - cell lung cancer with activating egfr mutations . 
sequist lv , goldman jw , wakelee , ha , et al : efficacy of rociletinib ( co - 1686 ) in plasma - genotyped t790mpositive non - small cell lung cancer ( nsclc ) patients ( pts )  . 
zheng d , ye x , zhang mz , et al : plasma egfr t790m ctdna status is associated with clinical outcome in advanced nsclc patients with acquired egfr - tki resistance . 
thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . 
niederst mj , hu h , mulvey he , et al : the allelic context of the c797s mutation acquired upon treatment with thirdgeneration egfr inhibitors impacts sensitivity to subsequent treatment strategies . 
ihuegbu n , banks kc , fairclough sr , et al : non - invasive detection of crizotinib resistance in alk - rearranged lung adenocarcinoma directs treatment with next - generation alk inhibitors . 
wakelee ha , gadgeel sm , goldman jw , et al : epidermal growth factor receptor ( egfr ) genotyping of matched urine , plasma and tumor tissue from non - small cell lung cancer ( nsclc ) patients ( pts ) treated with rociletinib . 
barlesi f , gervais r , lena h , et al : pemetrexed and cisplatin as first - line chemotherapy for advanced non - small - cell lung cancer ( nsclc ) with asymptomatic inoperable brain metastases : a multicenter phase ii trial ( gfpc 07 - 01 )  . ann oncol 22 : 2466 - 2470 , 2011 34 . 
de mattos - arruda l , mayor r , ng ck , et al : cerebrospinal fluid - derived circulating tumour dna better represents the genomic alterations of brain tumours than plasma . 
sasaki s , yoshioka y , ko r , et al : diagnostic significance of cerebrospinal fluid egfr mutation analysis for leptomeningeal metastasis in non - small - cell lung cancer patients harboring an active egfr mutation following gefitinib therapy failure . 
hata a , nanjo s , okuda c , et al : osimertinib at 80 mg for refractory leptomeningeal metastases in t790m - positive egfr - mutant non - small cell lung cancer . 
zill oa , mortimer s , banks kc : somatic genomic landscape of over 15 , 000 patients with advanced - stage cancer from clinical next - generation sequencing analysis of circulating tumor dna . 
canale m , petracci e , delmonte a , et al : impact of tp53 mutations on outcome in egfr - mutated patients treated with first - line tyrosine kinase inhibitors . 
marchetti a , palma jf , felicioni l , et al : early prediction of response to tyrosine kinase inhibitors by quantification of egfr mutations in plasma of nsclc patients . 
tseng js , yang ty , tsai cr , et al : dynamic plasma egfr mutation status as a predictor of egfr - tki efficacy in patients with egfr - mutant lung adenocarcinoma . 
mok t , wu yl , lee js , et al : detection and dynamic changes of egfr mutations from circulating tumor dna as a predictor of survival outcomes in nsclc patients treated with first - line intercalated erlotinib and chemotherapy . clin cancer res 21 : 3196 - 3203 , 2015 47 . 
karachaliou n , mayo - de las casas c , queralt c , et al : association of egfr l858r mutation in circulating free dna with survival in the eurtac trial . 
lipson ej , velculescu ve , pritchard ts , et al : circulating tumor dna analysis as a real - time method for monitoring tumor burden in melanoma patients undergoing treatment with immune checkpoint blockade . 
 specifying the trueand falsepositive rates in basket trials in the clinical evaluation of anticancer therapies , after identification of a recommended dose , investigators typically seek evidence of drug efficacy in populations of patients hypothesized to benefit from it . 
the purpose of these signal - finding studies is to prioritize additional development and to determine whether drugs should be tested in randomized phase iii trials and , if so , in which populations of patients . 
because these identified populations usually are small and efficacy often is substantially better than that for available therapies , conclusions from single - arm trials of this nature can be used to inform off - label treatment decisions and sometimes lead to inclusion in treatment guidelines or regulatory approvals . 
an understanding of the performance characteristics of the novel clinical trial designs commonly used in this setting is critical to avoid inappropriate clinical decision making on the basis of false - positive clinical trial results . the group of patients in whom a therapy is hypothesized to have activity can be identified in a number of ways , including genomic and proteomic profiles , and activity of the drug can be influenced by histology or the primary tumor site . 
the combination of a hypothesized mechanism of action and uncertainty around the populations of patients who would likely benefit has encouraged a trend toward more - complex earlyphase trials.1 a major challenge is the desire to study the effects of the drug simultaneously in patients with different primary sites of disease or histologies with the goal of evaluating the efficacy of the drug in these contexts , often referred to as baskets.2 - 9 a related recent trend in clinical trial design has been increasing enthusiasm for the use of adaptive designs , whereby design parameters can be changed dynamically as the trial progresses and evidence about efficacy gradually emerges.10 a final important trend has been the use of bayesian design as a tool to evaluate the emerging evidence in a formal statistical model.11 - 15 many of these methods are predicated on the underlying expectation of broadly similar efficacy across baskets because the statistical model allows the sharing of information across baskets with the purpose of completing the trial in a shorter time frame with fewer patients than a traditional strategy whereby each basket is regarded as an independent phase ii trial . 
this combination of design complexity with sophisticated statistical modeling has led to situations in which important clinical trials are being launched without a broad understanding of the implications of the novel methods used , an issue that has been identified previously in the context of novel phase i study designs.16 in this commentary , we examine the properties of a particular bayesian adaptive design that increasingly is being used in the context of basket trials , and we use the clinical setting of a completed basket trial to demonstrate that the design is heavily tilted toward positive conclusions about the efficacy of the drug.17 the complexity of these modern methods makes having a clear understanding of the properties of design , characterized by easily interpretable measures , essential when planning a new clinical trial . although bayesian statistical analyses generally focus on reporting the probability that an individual drug works ( the so - called posterior probability ) , we believe that the evaluation of properties of designs in terms of the familiar metrics used in the context of clinical trials is important . 
these properties are the true - positive rate ( the probability that a truly effective agent will be shown to be effective [ often referred to as power ] ) and the falsepositive rate ( the probability that an ineffective agent is erroneously judged to be effective [ often referred to as the type i error ] )  . 
we generally like to keep the false - positive rate low because we do not want to encourage additional study of a drug that does not work , and we want the true - positive rate to be high because we want to be confident that if the drug truly works , its effectiveness will be recognized . 
therefore , to fully understand the implications of these data - sharing methods , we must calculate a more - elaborate set of trueand false - positive rates , specifically when the drug does not work at all , when it only works in one kristen m . 
 basket , when it only works in two baskets , and so forth . as an illustration of the clinical setting , we refer to the findings of a recent basket trial that investigated the effects of vemurafenib , a selective oral inhibitor of the braf kinase.2 the trial assessed efficacy in five disease - specific baskets : nonsmallcell lung cancer , colorectal cancer , cholangiocarcinoma , erdheim - chester disease or langerhans cell histiocytosis , and anaplastic thyroid cancer . 
the investigators concluded that the drug shows promising activity in the nonsmall - cell lung cancer basket and the erdheim - chester disease or langerhans cell histiocytosis basket but that it is inactive in colorectal cancer . 
although this trial did not use the bayesian hierarchical design proposed by berry et al , 17 we use the clinical setting of the vemurafenib trial to investigate the performance of the berry design . the bayesian hierarchical model is structured to capture the correlation between the anticipated efficacies of the drug across various baskets . 
this aggregation of evidence is rooted in a key feature of bayesian methods , the prior distribution of the between - basket variability , an entity that is prespecified by the analyst . 
in the context of a basket trial , this prior distribution essentially titrates the extent to which emerging evidence of drug efficacy from one basket can be used to bolster the evidence in other baskets . 
however , they presented a sensitivity analysis that concluded that the properties are actually relatively insensitive to this choice . we evaluated the false - positive and false - negative error rates for a hypothetical trial similar in structure to the vemurafenib trial , with five baskets and null and alternative response rates of 15% and 45% , respectively . 
we simulated trials by following the bayesian hierarchical design and conducted interim analyses after the first 10 patients were accrued and then after every additional five patients until a maximum of 19 patients per basket were enrolled . 
early stopping rules terminated accrual to individual baskets if the basket - specific posterior probability that the true response rate is greater than a midlevel response rate of 30% was , 5% ( stop for futility ) or  . 
at the end of the trial , the treatment was declared efficacious in a basket if the posterior probability that the response rate that exceeded the null value of 15% was  . 
for example , in the second row ( one active basket ) , basket 1 is the one in which the drug is truly active , whereas in baskets 2 to 5 , the drug is not active . 
in this scenario , we see that a 79% chance for observing a true - positive result exists in the active basket , whereas for each nonactive basket , the false - positive rate is 18% . 
the next column on the right captures the probability that one or more of the nonactive baskets is a false - positive finding , a term usually referred to as the family - wise error rate , a key criterion for evaluating multiple hypotheses in clinical trials.18 , 19 we see that this overall false - positive rate is 37% when the drug truly works in only one basket and rises to 57% when the drug does not work in only one basket . 
although the maximum trial size was set to 95 patients , the expected trial size ranged from 59 to 84 patients , depending on the true efficacy configuration of the baskets . 
the table also lists the family - wise error rates for the setting in which each basket is regarded as an entirely independent clinical trial wherein the false - positive rate is 10% . 
each basket displays the observed response rate ( rr ) from the vemurafenib trial for a particular disease ( sample sizes in parentheses )  . ( * ) patients received combination therapy ( vemurafenib 1 cetuximab )  . 
statistical properties of bayesian hierarchical design probability drug will be declared efficacious , % family - wise error rate , % * basket 1 basket 2 basket 3 basket 4 basket 5 hierarchical independent no . 
bold represents baskets in which the drug is active ; no bold represents baskets in which the drug is not active . * the family - wise error rate represents the probability that the drug has false - positive efficacy in any one or more of the nonactive baskets ( ie , the overall false - positive rate of the design given the number of baskets in which the drug is truly active )  . 
this is shown for both the bayesian hierarchical design and the setting in which all five baskets are considered to be independent clinical trials . close examination of table 1 demonstrates two complementary results from using the bayesian design . 
although the targeted overall false - positive rate of 10% has been achieved for the setting in which the drug has no efficacy ( ie , the drug works in none of the baskets as shown in the first row ) , this standard rapidly erodes as we investigate settings in which the drug works in some baskets but not in others . for example , if we look at the two active baskets row of the table , we see a high probability ( 94% ) of declaring each of the two active baskets to be efficacious . 
consider the most extreme case ( the four active baskets row of the table ) where we see that the nonactive basket has a false - positive rate of 57% . 
in this setting , the evidence typically is dominated by strong positive results from the four baskets in which the drug is truly active , and the imposition of the prior distribution encourages the model to interpret the results from all five baskets as strongly correlated ( ie , similar in efficacy ) , which leads to a high probability that the inactive basket will be classified incorrectly as active . 
in related work , we explored in depth options for modifying the bayesian design used in our simulations by examining various choices of prior distributions and of decision rules used , demonstrating that trials can be designed on the basis of hierarchical modeling with much better control of the familywise error rates.20 we believe that straightforward reporting of the various trueand false - positive rates , as listed in table 1 , are fundamental to understanding the merits of any proposed basket study design . seemingly innocuous choices , such as the use of a prior distribution that berry et al17 characterized as weak , which allows the data to shape the amount of borrowing , can actually have a substantial influence on the real risks of obtaining false - positive results . 
hyman consulting or advisory role : atara biotherapeutics , chugai pharmaceutical , cytomx therapeutics , boehringer ingelheim , astrazeneca research funding : astrazeneca , puma biotechnology , loxo oncology gregory j . 
riely consulting or advisory role : genentech research funding : novartis ( inst ) , roche ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , infinity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : novartis , merck sharp & dohme kristen m . 
begg no relationship to disclose affiliations all authors : memorial sloan kettering cancer center , new york , ny . supported in part through national cancer institute awards ca008748 and ca163251 . support references 33 : 975 - 977 , 2015 1 . 
hyman dm , puzanov i , subbiah v , et al : vemurafenib in multiple nonmelanoma cancers with braf v600 mutations . n engl j med 373 : 726 - 736 , 2015 3 . 
eortc network of core institutions : cross - tumoral phase 2 clinical trial exploring crizotinib ( pf - 02341066 ) in patients with advanced tumors induced by causal alterations of alk and / or met ( create ) , 2013 . 
lopez - chavez a , thomas a , rajan a , et al : molecular profiling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
burris ha , hurwitz h , perez ea , et al : mypathway : an open - label phase iia study of trastuzumab / pertuzumab , erlotinib , vemurafenib , and vismodegib in patients who have advanced solid tumors with mutations or gene expression abnormalities targeted by these agents . 
iasonos a , g onen m , bosl gj : scientific review of phase i protocols with novel dose - escalation designs : how much information is needed ? j clin oncol 33 : 2221 - 2225 , 2015 17 . 
chen c , li n , shentu y , et al : adaptive informational design of confirmatory phase iii trials with an uncertain biomarker effect to improve the probability of success . 
klein , md2 purpose to assess the association between the oncotype dx genomic prostate score ( gps ) result and longterm oncological outcomes following radical prostatectomy ( rp )  . methods we evaluated the association of the gps result assayed from the index lesion from rp tissue with the risk of distant metastases ( dm ) and prostate cancerspecic mortality ( pcsm ) over the 20 years following rp in a stratied cohort sample of 428 patients from 2 , 641 treated between 1987 and 2004 . 
exploratory analysis using presurgical parameters and the gps test as prognostic variables was performed to assess the additional value of the gps test on 20 - year risk of dm and pcsm . 
model discrimination was measured using the area under the receiver operating characteristic curve . results the gps test appears to be independently associated with both 20 - year risk of dm and pcsm with a low false discovery rate . 
accuracy of models including clinical risk factors alone appeared to improve when including the gps test in assessing risk of both end points . conclusion the results suggest that the gps test provides information on the risk for the meaningful long - term outcomes of dm and pcsm . jco precis oncol 5 : 442 - 449 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction long - term cancer outcomes are an important consideration when deciding between active surveillance ( as ) and immediate treatment for newly diagnosed prostate cancer . 
multiple prospective as studies that predominantly include patients at the lowest risk of progression have demonstrated a low risk of distant metastasis ( dm ) and prostate cancerspecic mortality ( pcsm ) with extended follow - up.1 , 2 however , these excellent outcomes with as require strict selection criteria and stringent follow - up with frequent repeat prostate biopsies . 
based on these studies , the current use of as for newly diagnosed men is increasing and now includes expanded selection criteria , including younger men with longer life expectancy and those with biopsy - dened pathologic features that fall outside eligibility criteria of older studies.3 it is long - term as outunknown whether the excellent comes observed for low - risk disease can be maintained in this expanded group using only traditional clinical variables and existing surveillance strategies . for example , although both pivot and protect showed no statistically signicant difference in pcsm between observation and immediate treatment intermediate - risk patients with up to a 12.7 - year followup , 4 , 5 the condence intervals for the hazard ratio ( hr ) do not exclude substantial benet of radical prostatectomy ( rp )  . 
furthermore , the long - term results of scandinavian prostate cancer group trial 4 demonstrated an 11.7% absolute risk reduction in pcsm with rp , corresponding to a relative risk of 0.55 , compared with conservative management.6 with up to a 29 - year follow - up , the results of this study are more reective of the lifetime risk of cancer recurrence and death in men with intermediateor high - risk features . 
 gps assay associated with long - term prostate cancer outcomes context key objective localized prostate cancer has an extended natural history , making immediate treatment decisions difcult without the understanding of long - term cancer risks . 
we sought to evaluate the association between the genomic prostate score ( gps ) test and long - term prostate cancer outcomes : distant metastasis and prostate cancerspecic mortality following radical prostatectomy . knowledge generated the gps test appeared to be associated with both distant metastasis and prostate cancerspecic mortality at a 20 - year followup in both univariable and multivariable models , where model discrimination was improved when the gps results were included . relevance the use of the gps test can provide risk assessment of long - term prostate cancer outcomes , beyond clinical factors alone , for patients with localized prostate cancer . traditionally used clinical information in assessing risk of adverse pathology ( ap ) at rp.7 , 8 van den eeden et al9 established the association of the gps test with risk of dm and pcsm over 10 years . 
in this report , we sought to evaluate whether the gps test is also associated with 20 - year risk of dm and pcsm and whether its use improves risk assessment for these end points compared with clinical variables alone . methods using a stratied cohort sampling design , so that a weighted analysis of the study cohort is representative of all patients ( n = 2 , 641 ) who underwent rp between 1987 and 2004 at our institution , we selected 501 patients for inclusion . 
among the remaining 441 patients , the nal analysis cohort comprised the 428 patients with evaluable primary gleason pattern in prostatectomy tissue ( fig 1 )  . all patients were selected from our prospective institutional review board ( irb ) approved database that includes clinical staging , pathology from biopsy and rp , and followup information . 
follow - up and outcome data were obtained through subsequent clinic visits , telephone calls , and semiannual follow - up letters obtained through august 1 , 2019 , approximately 10 years after the previously reported cutoff.7 multiple data reviews and quality checks were performed to ensure delity of the data set . high grade at rp was dened as grade group 3 or above ( gleason score 4 + 3 or higher )  . 
the time to event in patients who died without an event or who were alive without an event at the end of follow - up was considered censored in these analyses . 
each patient was weighted using the inverse sampling fraction in his stratulin and weis robust variance estimate was used.12 in the multivariable analysis , the gps result , preoperative prostatespecic antigen ( psa ) , clinical stage , and biopsy grade were used as covariables . 
the hr for continuous gps results was reported per 20 - gps unit increase , which approximated the difference between the average gps value in the highest 25% and the average gps value in the lowest 25% of patients based on the gps value distribution from previous studies.7 , 13 preoperative psa value was included in the model as log2 ( psa value )  . 
characteristics of the patients in the cohort sample biopsy gleason grade , % brooks et al 61 ( 6 ) 62 ( 57 - 66 ) mean ( sd ) median ( iqr ) race , % white black / afro - caribbean asian / hispanic / others year of surgery , % surgical gleason grade results clinical tumor stage , % pathologic tumor stage % 3 + 4 3 + 5 4 + 3 4 + 5 5 , 5 + 4 low / very low intermediate high 1987 - 1989 1990 - 1994 1995 - 1999 2000 - 2004  . 
summary statistics and percentages are estimated using cohort sampling weights so they estimate the distribution of characteristics in the full cohort of 2 , 641 patients from which the cohort sample ( n = 428 ) was drawn . abbreviations : aua , american urological association ; psa , prostate - specic antigen . for overoptimism of effect estimates involving the gps test . therefore , all estimates using the gps test as a covariable were corrected for regression to the mean ( rm ) 14 and false discovery rates ( fdrs ) were reported rather than p values ( data supplement )  . 
applying the rm correction for gps test , the absolute risk estimates were computed as the weighted average of the absolute risk estimates over the study population patient age for each ap status , with cis derived using the delta method . 
receiver operating characteristic ( roc ) curve estimates were based on these absolute risk estimates , correcting for bias 444 2021 by american society of clinical oncology inherent in roc curves ( data supplement ) , with and without the gps results as a covariable . 
differences between models in the roc area under the curve ( auc ) were tested for signicance using the bootstrap . the overall cohort consisted of predominantly american urological association ( aua ) lowand intermediate - risk patients with prostate cancer , 55% and 35% , respectively ( table 1 )  . 
the distribution of gps results , accounting for the stratied cohort sampling weighting , in the overall population and by biopsy gleason grade is shown in figure 2 . the gps result appeared to be highly associated with both dm and pcsm at 20 years of follow - up . 
 gps assay associated with long - term prostate cancer outcomes total cohort 2 , 641 patients with prostatectomy 19872004 501 patients selected 127 with clinical recurrence 374 without clinical recurrence 441 patients evaluable for clinical / pathology / gene expression 428 patients with evaluable primary gleason pattern in prostatectomy tissue 51 excluded for insufficient tumor 7 did not meet inclusion criteria 2 outlier gene profile fig 1 . 
of 2 , 641 patients who underwent rp between 1987 and 2004 , a cohort of 501 patients was selected using a 1 : 3 sampling design , which included all 127 patients who did and 374 patients who did not have a clinical recurrence . 
rm - corrected estimates of the 20 - year absolute risk of dm and pcsm as a function of gps result among aua low - risk patients and favorable intermediaterisk patients have functional form similar to the estimates for the overall population , with a large increase in risk for the gps result  . 
the number of events in this subgroup was insufcient for multivariable analysis . discussion previous validation studies have clearly shown the gps test and other prostate biopsybased gene expression proles to predict the presence of ap ( grade group 3 or higher or extraprostatic disease ) in rp specimens or serial needle biopsies in men on as or post - rp.7 , 8 , 15 although ap on biopsy or rp is prognostic regarding risk of recurrence , dm , and pcsm , 16 its use as a surrogate end point for these outcomes in men considering starting or staying on surveillance has been questioned with no clear short - term alternative.17 in this study , we sought to assess whether the gps result , based on pathologic evaluation of the index lesion on rp , in the original discovery cohort of this biomarker appeared to be associated with the more clinically meaningful outcomes of dm and pcsm at long - term followup . 
absolute risks of these outcomes , considering death from causes other than prostate cancer as a competing risk , showed a lowslope relationship with the gps result from 1 to 29 , with an inection point evident at a score 30 , above which the risk of dm or pcsm increased substantially , reaching an absolute risk of 38% for dm and 13% for pcsm at a score of 60 ( fig 3 )  . 
furthermore , we found that including the gps results in models assessing risk of dm and pcsm at 20 years improved discrimination compared with using clinical variables alone ( tables 2 and 3 ; fig 4a and 4b )  . 
other commercially available gene expression proles have reported similar ndings , albeit at earlier time points.18 - 21 treatment because key drivers of biological progression in patients on as are yet to be elucidated , an open question is what aspect of tumor biology commercially available gene expression proles may be measuring . 
detailed pathological analysis of the canary - pass study , a large , well - characterized as cohort , identied the presence of cribriform or stromagenic histology as the strongest predictor of cancer recurrence after in men who progressed to requiring therapy.22 the presence of cribriform glands has been shown in other studies to be associated with higher rates of biochemical recurrence after rp or radiation , as well as both dm and pcsm , 23 , 24 likely driven by the observation that these glands exhibit genomic features characteristic of aggressive disease.25 in a recent study of 194 men with national comprehensive cancer network very low - , low - , or intermediate - risk disease considering as , we observed that only those with the gps results above 29 had cribriform histology present on biopsy ( falzarano et al , manuscript submitted for publication )  . 
gps , genomic prostate score . observed that a gps result 29 was associated with grade reclassication on subsequent biopsy in a cohort of lowand intermediate - risk men on as , whereas in an underpowered study using a cohort of lower - risk men whose mean gps results were 21 , no association with grade progression was observed.17 together , these table 2 . 
however , a number of published observations support a role for decision making in men with higher scores : ( 1 ) multiple biopsy - based studies have validated that higher gps scores are associated with traditional histologic measures of ap ( dened as grade group 3 or extraprostatic disease , both of which are associated with worse outcomes ) 7 - 9 ; ( 2 ) the association of higher gps scores with histologic variants ( cribriform [ falzarano et al , manuscript submitted for publication ] and stromagenic26 histology ) shown to be associated with higher rates of recurrence in an as cohort ; 22 and ( 3 ) long - term data from the current study that link higher gps scores to the risk of meaningful clinical end points ( dm and pcsm )  . 
rm - corrected estimates with 95% condence intervals of the 20 - year absolute risk of distant metastasis ( a ) and prostate cancerspecic mortality ( b ) as a function of the gps result . 
 a 100% brooks et al 100% gps grade stage spline ( psa ) grade stage spline ( psa ) reference gps grade stage spline ( psa ) grade stage spline ( psa ) reference 0% 10% 20% 30% 40% 50% 60% 70% 80% 90% 100% 0% 10% 20% 30% 40% 50% 60% 70% 80% 90% 100% fig 4 . 
model - based rm - corrected , bias - corrected roc curve for dm ( a ) and pcsm ( b ) within 20 years of surgery with covariables : the gps result , high stage , high grade , and log2 psa . 
auc , area under the curve ; dm , distant metastases ; fpr , false positive rate ; gps , genomic prostate score ; pcsm , prostate cancerspecic mortality ; psa , prostate - specic antigen ; rm , regression to the mean ; roc , receiver operating characteristic ; tpr , true positive rate . strengths of this study include that the data were sourced from a prospectively maintained patient registry with locked baseline clinical , pathologic , and gene expression information ; centralized expert pathology review ; 20 - year followup , the longest reported in any similar study ; and independent verication of the statistical analysis . 
there are two limitations : ( 1 ) changes in standardized biopsy grading and stage migration since initial patient enrollment , although we note that all rp specimens were reviewed by an expert gu pathologist after the majority of substantive changes in prostate cancer grading occurred and ( 2 ) that this should be considered an exploratory analysis since the gps test was developed in this cohort . 
although the study by van den eeden et al9 largely replicates the results of this analysis , we believe that further validation in other cohorts is important to rmly establish our conclusions . in conclusion , with long - term follow - up , the gps test appears to be associated with both dm and pcsm and improves the accuracy of models containing clinical variables alone . 
these ndings suggest that genomic changes in the tumor tissue , quantied by the gps test , provide additional biological insight into the long - term risk of dm and pcsm . this information may be valuable to those considering as . prospective studies should be pursued to validate these results . affiliations 1scott department of urology , baylor college of medicine , houston , tx 2glickman urological and kidney institute , cleveland clinic , cleveland , 3department of anatomic pathology , university of alabama at birmingham , birmingham , al 4department of quantitative health sciences , cleveland clinic , cleveland , oh 5genomic health inc , an exact sciences corporation , redwood city , ca administrative support : tamer aboushwareb , eric a . 
 gps assay associated with long - term prostate cancer outcomes patents , royalties , other intellectual property : patent co - inventor on 17gene prostate assay with genomic health , inc conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . michael crager employment : exact sciences stock and other ownership interests : exact sciences travel , accommodations , expenses : genomic health ruixiao lu employment : genomic health , exact sciences stock and other ownership interests : genomic health , exact sciences consulting or advisory role : mission bio john abran employment : exact sciences stock and other ownership interests : exact sciences tamer aboushwareb employment : exact sciences stock and other ownership interests : exact sciences eric a . 
klein consulting or advisory role : grail no other potential conicts of interest were reported . references 2016 klotz l , vesprini d , sethukavalan p , et al : long - term follow - up of a large active surveillance cohort of patients with prostate cancer . 
j clin oncol 33 : 272 - 277 , 2015 tosoian jj , mamawala m , epstein ji , et al : intermediate and longer - term outcomes from a prospective active - surveillance program for favorable - risk prostate cancer . 
mahal ar , butler s , franco i , et al : conservative management of low - risk prostate cancer among young versus older men in the united states : trends and outcomes from a novel national database . 
n engl j med 377 : 132 - 142 , 2017 bill - axelson a , holmberg l , garmo h , et al : radical prostatectomy or watchful waiting in prostate cancer29 - year follow - up . 
n engl j med 379 : 2319 - 2329 , 2018 klein ea , cooperberg mr , magi - galluzzi c , et al : a 17 - gene assay to predict prostate cancer aggressiveness in the context of gleason grade heterogeneity , tumor multifocality , and biopsy undersampling . 
eur urol 66 : 550 - 560 , 2014 cullen j , rosner il , brand tc , et al : a biopsy - based 17 - gene genomic prostate score predicts recurrence after radical prostatectomy and adverse surgical pathology in a racially diverse population of men with clinically lowand intermediate - risk prostate cancer . 
eur urol 68 : 123 - 131 , 2015 van den eeden sk , lu r , zhang n , et al : a biopsy - based 17 - gene genomic prostate score as a predictor of metastases and prostate cancer death in surgically treated men with clinically localized disease . 
lin dw , zheng y , mckenney jk , et al : 17 - gene genomic prostate score test results in the canary prostate active surveillance study ( pass ) cohort . 
spratt de , youse k , deheshi s , et al : individual patient - level meta - analysis of the performance of the decipher genomic classier in high - risk men after prostatectomy to predict development of metastatic disease . 
klein ea , youse k , haddad z , et al : a genomic classier improves prediction of metastatic disease within 5 years after surgery in node - negative high - risk prostate cancer patients managed by radical prostatectomy without adjuvant therapy . 
cooperberg mr , davicioni e , crisan a , et al : combined value of validated clinical and genomic risk stratication tools for predicting prostate cancer mortality in a high - risk prostatectomy cohort . 
canter dj , freedland s , rajamani s , et al : analysis of the prognostic utility of the cell cycle progression ( ccp ) score generated from needle biopsy in men treated with denitive therapy . 
mckenney jk , wei w , hawley s , et al : histologic grading of prostatic adenocarcinoma can be further optimized : analysis of the relative prognostic strength of individual architectural patterns in 1275 patients from the canary retrospective cohort . 
kweldam cf , wildhagen mf , steyerberg ew , et al : cribriform growth is highly predictive for postoperative metastasis and disease - specic death in gleason score 7 prostate cancer . 
greenland ny , cowan je , chan e , et al : prostate biopsy histopathologic features correlate with a commercial gene expression assays reclassication of patient eur j cancer 66 : 26 - 33 , 2016 alterations . 
kornberg z , cooperberg mr , cowan je , et al : a 17 - gene genomic prostate score as a predictor of adverse pathology in men on active surveillance . 
 multi - institutional , prospective clinical utility study evaluating the impact of the 92 - gene assay ( cancertype id ) on final diagnosis and treatment planning in patients with metastatic cancer with an unknown or unclear diagnosis purpose metastatic cancers of unknown primary or with unclear diagnoses pose diagnostic and management challenges , often leading to poor outcomes . 
the current study assessed the clinical impact of the 92 - gene assay on diagnostic and treatment decisions for patients with unknown or uncertain diagnoses . methods patients in this prospective , multi - institutional , decision - impact study included those for whom the 92 - gene assay was ordered as part of routine care . 
the key study objective of clinical impact was calculated on the basis of changes in final diagnosis and treatment after testing . results data collection included 444 patients , 107 physicians ( 73 oncologists and 34 pathologists ) , and 28 sites . 
 physicians reported that the 92 - gene assay was used broadly for diagnostic dilemmas that ranged from single suspected tumor type ( 29% ) to a differential diagnosis of two or more suspected tumor types ( 30% ) or cancers of unknown primary ( 41% )  . 
integration of 92 - gene assay results led to a change in the recommended treatment in 47% of patients . conclusion findings from this clinical utility study demonstrate that the 92 - gene assay led to a change in treatment decisions in every other patient case . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction metastatic cancers that are initially characterized as unknown primary ( cup ) , or with other features that may lead to diagnostic uncertainty with respect to tumor type diagnosis , can prolong the clinicopathologic workup and result in delays in the initiation of treatment , additional costs , and relatively poor patient outcomes.1 - 3 sachdev p . 
schnabel fadi braiteh author affiliations and support information ( if applicable ) appear at the end of this article . licensed under the creative commons attribution 4.0 license corresponding author : sachdev p . 
numerous diagnostic and treatment strategies , such as enhanced pathologic techniques , molecular classification of tumor type and subtype , comprehensive mutational profiling , and novel combination regimens of cytotoxics plus biolo gics , have been proposed without universal consensus.4 - 10 investigational approaches to personalize the systemic treatment of metastatic cancer solely on the basis of the patients somatic genomic alterations , disregarding histologic context , have had mixed and disappointing results.11 - 14 results from several recent phase ii studies that evaluated targeted agents for specific genomic alterations across a variety of tumor types have provided evidence that mutations are not targetable in similar manners across tumor types.11 , 12 thus , the clinical utility of this approach is unclear . 
 whereas driver mutations matter , the integration of tumor type and subtype remains critical when considering the efficacy of a targeted therapy aimed at a putative driver mutation.15 given that empirical chemotherapy approaches are associated with poor prognosis in patients with cup or uncertain diagnoses , it might be more effective to refocus on methods with which to identify patient tumor type and subtype to guide therapy.1 , 16 gene expression profilingbased molecular classification of tumors might prove efficacious by helping to identify the primary tumor type and histologic subtype for patients with unknown or uncertain diagnoses . 
the primary objective was to assess clinical impact on the basis of changes in diagnostic and treatment decisions after the incorporation of 92 - gene assay results . methods study design observational in nature , the current study was prospectively defined to evaluate multidisciplinary clinical utility in patients for whom physicians ordered the 92 - gene assay as a clinical workup tool to help identify or narrow the tumor type and subtype diagnosis . 
prespecified objectives were to examine the diagnostic and clinical utility of the 92 - gene assay in oncology and pathology practice to characterize indications of use , and to evaluate its potential integration and impact on patient management by comparing changes in diagnosis and treatment selection after testing . data collection physicians were required to complete standard ized , discipline - specific questionnairespathology and oncologyafter receiving a 92 - gene assay test report . 
 the pathology ecrf consisted of 11 multiple choice questions and four questions that required written responses ( biopsy quality , number and types of immunohistochemistry [ ihc ] performed , and 92 - gene assay result )  . 
the medical oncologist ecrf consisted of 11 multiple choice questions and five questions that required written responses ( time between biopsy and treatment , clinical diagnosis for first - line treatment , name of first - line treatment , other diagnostic or clinical considerations for choosing first - line therapy , and 92 - gene assay result )  . 
 rna quality determined to be quantity not sufficient , in which a molecular prediction could not be determined , physicians completed quantity not sufficient ecrfs that consisted of four multiple choice questions and two questions that required written response ( biopsy quality and number of ihc performed )  . 
ecrf forms are included in the data supplement . physicians were instructed on the web portal and ecrf via a standardized training progra for the pathology questionnaire ( data supplement : pathology ecrf question 7 and oncology ecrf question 8 , respectively ) , physicians were instructed to align terminology with the 50 tumor types and subtypes classified by the 92 - gene assay . 
the testing laboratory was blinded to the working clinical diagnosis from the ecrf . 92 - gene assay the 92 - gene assay was performed as previously described.17 , 20 in brief , the assayreal - time rt pcrwas performed on isolated total rna from tumor cells that were enriched by either microdissection or laser microdissection . 
a prespecified computational algorithm generated probabilities for primary tumor type and subtype on the basis of the degree of similarity of the submitted sample to a reference database of gene expression information from more than 2 , 000 tumors of known tumor type . 
the test report provided a prediction of the main tumor type and subtype on the basis of the highest relative probability and any additional tumor types that cannot be ruled out . 
the report also provided a list of tumor types that could be excluded with 95% confidence . statistical analysis statistical considerations of study size were based on an anticipated treatment recommendation change rate of 35% , targeting a sample size of at least 156 patients to ensure a 95% two - sided ci width of 15% . 
the primary objective of the study was to measure the clinical impact of the 92 - gene assay results on the basis of changes in patient treatment , the narrowing of treatment options , or the elimination of a treatment option ( a , b , or c on question 15 of the oncology questionnaire in the data supplement )  . 
patients were considered eligible for a targeted agent if the physician responded a , " " b , " or c in question 15 and there was a us food and drug administrationapproved targeted therapy that was recommended by the national comprehensive cancer network for the molecular diagnosis provided by the 92 - gene assay . results patient enrollment began in february 2013 and closed october 2014 after enrolling 444 patients with 107 physicians73 medical oncologists and 34 pathologistsfrom 28 sites21 oncology sites and seven pathology sitesacross the united states . 
of the 444 patients enrolled , 397 had sufficient rna for analysis , which corresponded to an overall analytical success rate of 89% , taking into account samples that were determined to have insufficient tissue on pathology review before testing . 
a patient flow diagram is shown in figure 1 . biopsy and tumor characteristics the most common metastatic biopsy sites included the liver ( 23% ) , lymph nodes ( 17% ) , and lung ( 14% ; fig 2a )  . 
patient flow diagram showing the disposition of 92 - gene assay testing . patients submitted for testing ( n = 444 ) not reportable insufficient tissue or rna ( n = 47 ) reportable results ( n = 397 ) resulted to oncologist ( n = 271 ) resulted to pathologist ( n = 126 ) 92 - gene assay results ( n = 271 ) 92 - gene assay results ( n = 126 ) indeterminate ( n = 12 ) indeterminate ( n = 6 ) molecular diagnosis ( n = 259 ) molecular diagnosis ( n = 120 ) excluded did not receive anticancer therapy performance deaths patient choice other ( n = 56 ) ( n = 16 ) ( n = 8 ) ( n = 7 ) ( n = 25 ) patient received anticancer therapy ( n = 203 ) diagnostic testing and preassay diagnosis factors that contributed to an oncologists decision to order the 92 - gene assay were multidisciplinary and included the following : no primary site of origin after clinical review and imaging ( 42% ) , a pathology report that indicated a differential diagnosis ( 21% ) or that indicated an unknown primary site ( 20% ) , and distinguishing between new cancer versus recurrence ( 16% )  . 
 data that were collected to better characterize the sequence of diagnostic testing demonstrated that 72% of physicians responded that patients had pathology and ihc studies performed before the 92 - gene assay , 14% of samples were submitted for pathology and ihc evaluation and the 92 - gene assay concurrently , and approximately 14% of samples were submitted without an indication of the diagnostic sequence . 
the most common imaging tests were computed tomography scans ( 86% ) , fusion positron emission tomography / computed tomography scans ( 57% ) , magnetic resonance imaging ( 29% ) , ultrasound ( 28% ) , regular film radiographs ( 11% ) , or mammogram ( 11% ; data not shown )  . for pathologists , inconclusive ihc ( 50% ) was the most common reason for ordering the 92 - gene assay . 
the mean number of ihc stains performed before the molecular assay was ordered was 10 ( median , nine ; range , zero to 23 ; data not shown )  . 92 - gene assay results and impact on diagnosis of the 397 patients with sufficient tissue and rna for a reportable result , the 92 - gene assay provided a molecular - based tumor type and histologic subtype diagnosis in 379 patients ( 95.5% ) , whereas 4.5% had an indeterminate molecular diagnosis ( fig 1 )  . 
 ( * ) other indicates biopsy sites with fewer than three cases , encompassing uterus , gallbladder , gastroesophageal junction , spine , spleen , thyroid , and salivary gland . 
fna , fine - needle aspiration . liver lymph node lung peritoneal cavity or omentum soft tissue bone / marrow pleural cavity / pleura colon brain rectum skin breast bladder stomach pelvic mass retroperitoneum pericardial cavity adrenal gland pancreas mediastinum esophagus ovary duodenum other * core excision endoscopic other percentage percentage types . 
the most common diagnoses were pancreaticobiliary ( 21.9% ) , squamous cell carcinoma ( 10.1% ) , lung adenocarcinoma ( 9.3% ) , and intestinal ( 8.6% ) type tumors ( fig 3 )  . working diagnoses before the 92 - gene assay were assessed in the medical oncology subset ( n = 271 )  . 
preassay working diagnoses were reported as a single suspected site in 79 patients ( 29% ) , a differential diagnosis of two or more suspected sites in 80 patients ( 30% ) , and cup in 112 patients ( 41% ; fig 4a )  . 
comparison of the 92 - gene assay molecular diagnoses with preassay working diagnoses demonstrated that the assay provided a tumor type diagnosis that was not initially suspected in a large proportion of patients ( fig 4b )  . 
in patients with a single suspected primary site ( n = 79 ) , the 92 - gene assay confirmed the suspected diagnosis in 60% of patients but provided a tumor type result that was not initially suspected in 39% of patients . 
in patients with a differential diagnosis ( n = 80 ) , the 92 - gene assay narrowed the diagnosis in 66% of patients and provided a tumor type result that was not initially suspected in 27% of patients . 
in patients for whom the pathology report indicated cup site ( n = 112 ) , the assay provided a molecular tumor type prediction in 97% of patients . impact on treatment planning of the 271 oncologist - submitted cases , 203 patients ( 75% ) received anticancer treatment after the 92 - gene assay results were made available . 
the most common reasons for patients not receiving treatment were a rapid deterioration in the patients performance status ( 29% ) , patient death ( 14% ) , and a patient declination of treatment ( 13% ; fig 1 )  . 
molecular cancer classification predictions from submitted cases using the 92 - gene assay ( n = 397 )  . pancreaticobiliary squamous cell carcinoma lung adenocarcinoma intestine gastroesophageal adenocarcinoma urinary bladder neuroendocrine ovary breast adenocarcinoma liver hepatocellular carcinoma sarcoma head and neck salivary gland carcinoma prostate adenocarcinoma endometrial adenocarcinoma cervix adenocarcinoma melanoma kidney mesothelioma germ cell thyroid brain indeterminate skin basal cell carcinoma percentage ( fig 5a )  . 
the assay resulted in similar changes in treatment recommendations in all three scenarios of the original working diagnosis48% of cases with a single suspected primary ( n = 79 ) , 49% of differential diagnoses with two or more primaries ( n = 80 ) , and 42% of cases with an unknown primary site ( n = 112 )  . subset analysis within the most commonly predicted tumor type classesthose with 20 casesdemonstrated that physicians changed their recommended treatment in 58% of gi cancers ( n = 81 ) , 54% of gynecologic and breast cancers ( n = 28 ) , and 44% of lung cancers ( n = 27 ; fig 5b )  . 
mutational biomarker testing was most commonly ordered after the 92 - gene assay rendered a diagnosis of lung ( 81% ) or colorectal cancer ( 67% )  . discussion results from this large , multisite study have demonstrated that the 92 - gene assay was used across a spectrum of diagnostic uncertainty , beyond cups , and included cases with differential diagnoses and those with a suspected diagnosis for confirmatory testing . 
in addition , the assay provided a diagnosis that was not initially suspected in a substantial proportion of patients who had either a single suspected diagnosis or differential diagnosis before testing with the 92 - gene assay . 
 this clinical impact was more pronounced in gi and gynecologic and breast tumor types , which suggests that the 92 - gene assay may have additional utility in particular metastatic presentations in which standard approaches may be limited . 
 distribution of 92 - gene assay diagnostic results within the preassay working diagnosis classifications . differential diagnosis ( 30% ) unknown primary ( 41% ) single suspected site ( 29% ) indeterminate indeterminate indeterminate provided new diagnosis provided new diagnosis confirmed suspected diagnosis confirmed suspected diagnosis provided new diagnosis single suspected site differential diagnosis unknown primary approaches , what is both the current and future relevance of establishing the tumor type or cellular context of a metastatic cancer ? recent results from a number of basket trials have demonstrated that knowledge of tumor type and cellular context remains fundamental for the interpretation of potentially targetable dna mutations and the recommendation of treatment approaches in metastatic cancer . 
whereas molecularly targeted agents have been demonstrated to be effective in tumors that harbor a matching molecular alteration , a growing understanding of the importance of molecular heterogeneity and cellular context is emerging . 
for example , the efficacy of the targeted braf inhibitor , vemurafenib , has been shown to be mixed across a diverse set of nonmelanoma cancers with a braf v600 mutation11 and is well known to have poor efficacy in braf - mutated colorectal cancers.11 , 13 similarly , early results from the mypathway basket trial have demonstrated variable response rates in patients with identical mutations across different tumor types.14 finally , in a phase ii study in which patients with a specific molecular alteration were randomly assigned to receive treatment with a molecularly targeted agent or physicians choice of treatment , there was no difference in median progression - free survival between the two treatment groups.12 these data suggest that the effectiveness of targeting putative driver mutations with molecularly targeted agents may be dependent on the specific cellular context or tumor type . 
 no , treatment regimen was not changed ( 53% ) yes , treatment regimen was changed ( 47% ) gi cancers gynecological and breast cancers lung cancers treatment regimen was not changed ( 42% ) yes , treatment regimen was changed ( 58% ) treatment regimen was not changed ( 46% ) yes , treatment regimen was changed ( 54% ) treatment regimen was not changed ( 56% ) yes , treatment regimen was changed ( 44% ) fig 5 . 
 ( b ) impact of the 92 - gene assay on treatment decisions within tumor type subgroups that received therapy : gi cancers ( n = 81 ) , gynecologic and breast cancers ( n = 28 ) , and lung cancers ( n = 27 )  . breast adenocarcinoma , and lung adenocarcinoma.23 - 25 results presented here reinforce the continued relevance of tumor type diagnosis in optimizing treatment strategies that can potentially affect patient outcomes . 
with regard to pancreaticobiliary tumors , the 92 - gene assay also reports additional subtyping into gallbladder adenocarcinoma , pancreatic adenocarcinoma , or cholangiocarcinoma , which may inform treatment decisions for surgery type , neoadjuvant chemotherapy , or site - directed and targetable agents . 
in addition , a significant proportion of tumor types predicted by the 92 - gene assay , including lung adenocarcinoma , lung squamous , colorectal , gastroesophageal , urinary bladder , and neuroendocrine tumors , have not only specific chemotherapy approaches , but also us food and drug administrationapproved molecularly targeted therapies or immunotherapies . 
 decision making , with similar overall results , which supports the clinical utility of the assay.34 , 35 strengths of this study include the large number of patients and contributing physicians , which contributed to the generalizability of the study results . 
first , this was an observational study and no data on outcomes were collected ; however , previous studies have demonstrated that the use of the 92 - gene assay improved survival in patients with cup who were treated on the basis of assay results.16 , 34 although multiple aspects of the study design were prespecified and carefully planned , such as study physicians independently completing questionnaires , a blinded design such that the testing laboratory did not have knowledge of working diagnoses , and a preplanned statistical analysis , bias is an inherent feature of observational studies . 
this aspect of the cross - functional integration of molecular diagnostic results warrants investigation in future studies . this study demonstrated that the 92 - gene assay affected diagnosis and treatment selection in a significant proportion of patients , which supports the clinical utility of the assay as a standardized molecular approach to help streamline additional diagnostic testing in patients with metastatic cancer with unknown or uncertain diagnoses . 
schnabel data analysis and interpretation : all authors manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors lauren e . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : biotheranostics brock e . 
 fadi braiteh stock and other ownership interests : bristol - myers squibb , insys therapeutics , agios , clovis oncology , tesaro honoraria : genentech , insys therapeutics , bristol - myers squibb , amgen , boehringer ingelheim , astrazeneca , bayer , celgene , ipsen , incyte , taiho pharmaceutical , lexicon , ariad pharmaceuticals , eli lilly , abbott nutrition , heron consulting or advisory role : amgen , bristol - myers squibb , clovis oncology , boehringer ingelheim , ipsen , insys therapeutics , ambry genetics , genentech , eli lilly , incyte , bayer , sanofi , regeneron , astrazeneca , merck , celgene , lexicon , pfizer , merrimack pharmaceuticals speakers ' bureau : amgen , bristol - myers squibb , genentech , merck , pfizer , eli lilly , ipsen , insys therapeutics , incyte , boehringer ingelheim , astrazeneca , celgene , taiho pharmaceutical , merrimack pharmaceuticals , biotheranostics travel , accommodations , expenses : genentech , bristolmyers squibb , amgen , celgene , clovis oncology , tesaro , ipsen , insys therapeutics , incyte , heron , astrazeneca , medimmune , novartis , boehringer ingelheim , lexicon , taiho pharmaceutical , bayer , bayer , onyx pharmaceuticals , exelixis , regeneron , sanofi , merrimack pharmaceuticals , pfizer research funding : biotheranostics acknowledgment we thank andrea c . 
grschel s , bommer m , hutter b , et al : integration of genomics and histology revises diagnosis and enables effective therapy of refractory cancer of unknown primary with pdl1 amplification . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors based on molecular profiles : early results from mypathway , an open - label , phase iia umbrella basket study . 
hainsworth jd , rubin ms , spigel dr , et al : molecular gene expression profiling to predict the tissue of origin and direct site - specific therapy in patients with carcinoma of unknown primary site : a prospective trial of the sarah cannon research institute . 
weiss lm , chu p , schroeder be , et al : blinded comparator study of immunohistochemical analysis versus a 92 - gene cancer classifier in the diagnosis of the primary site in metastatic tumors . 
kim b , schroeder b , schnabel ca , et al : physician - reported clinical utility of the 92 - gene molecular classifier in tumors with uncertain diagnosis following standard clinicopathologic evaluation . 
ahmed ka , caudell jj , el - haddad g , et al : radiosensitivity differences between liver metastases based on primary histology suggest implications for clinical outcomes after stereotactic body radiation therapy  . 
spetzler d , xiao n , burnett k , et al : multi - platform molecular profiling of 1 , 180 patients increases median overall survival and influences treatment decision in 53% of cases . 
nystrom sj , hornberger jc , varadhachary gr , et al : clinical utility of gene - expression profiling for tumor - site origin in patients with metastatic or poorly differentiated cancer : impact on diagnosis , treatment , and survival . 
raghav k , mhadgut h , mcquade jl , et al : cancer of unknown primary in adolescents and young adults : clinicopathological features , prognostic factors and survival outcomes . 
hainsworth jd , schnabel ca , erlander mg , et al : a retrospective study of treatment outcomes in patients with carcinoma of unknown primary site and a colorectal cancer molecular profile . 
j nat cancer inst 105 : 782 - 790 , 2013 appendix we thank the following principal investigators of the clinical study sites who participated in the study : paul adams , md ( genesys hurley cancer institute ) , solhail akbani , md ( baptist hospitals of southeast texas ) , stephen anthony , do ( evergreen hematology - oncology ) , andrew j . 
brenner , md ( the university of texas health science center at san antonio ) , david campbell , md ( grass valley hematology - oncology medical group ) , arvind chaudhry , md , phd ( medical oncology associates ) , william gilles , md ( dignity health ) , h . 
carriers are predisposed to a higher risk for developing colorectal , endometrial , and extracolonic cancers , including cancers of the stomach , ovary , small bowel , hepatobiliary and urinary tracts , skin , pancreas , and prostate . 
primary brain tumors ( pbts ) are a rare feature of ls , with an estimated lifetime risk of 1% to 6%.1 , 2 here , we report the case of a patient with a who grade iii glioneuronal tumor and pathogenic germline msh2 variant . 
microscopic examination revealed a high - grade glioma with eosinophilic granular bodies , elevated mitotic activity ( approximately 10 / 10 high - power eld [ hpf ] ) , vascular proliferation , and necrosis consistent with an anaplastic glioneuronal tumor ( who grade iii )  . tumor cells were positive for glial brillary acidic protein ( gfap ) and synaptophysin ( fig 2 )  . 
the mib - 1 proliferative index ( ki - 67 ) was approximately 10% . the patients initial postoperative imaging revealed no residual disease ; therefore , no adjuvant therapy was offered . 
postoperative head ct ( c ) with and ( d ) without contrast at the patients most recent follow up , 105 months postinitial diagnosis , shows postoperative changes of the left frontal lobe without evidence of tumor recurrence . disease progression identied pathogenic genomic alterations in six genesnf1 , pdgfra , atm , tp53 , ctnna1 , and msh2and 18 variants of uncertain signicance ( table 1 )  . 
follow - up ihc studies identied a loss of msh2 and msh6 protein expression in tumor cells , which is consistent with an ls - associated tumor and underlying msh2 germline mutation . 
microscopic examination revealed a high - grade glial neoplasm with ( a ) scattered pleomorphic cells , ( b ) spindle cells , and mitotic activity . necrosis and vascular proliferation were observed . 
immunostains showed that the tumor is positive for ( c ) gfap and ( d ) synaptophys ( e ) ki - 67 was moderately elevated and a ( f ) neurolament stain was negative within the tumor , highlighting a compact growth pattern . 
immunohistochemistry identied loss of ( g ) msh2 and ( h ) msh6 protein expression in tumor cells , with retained nuclear expression in the normal endothelial cells in the blood vessels . magnication of all images is 200 . 
glioblastoma is the most common pbt associated with ls.3 astrocytoma , oligodendroglioma , gliosarcoma , medulloblastoma , and neuroblastoma have also been reported.4 individuals with msh2 mutations have higher rates of pbts compared with carriers of other mmr mutations.5 the average age of pbt diagnosis occurs a decade earlier in individuals with ls , 4 and the age range for msh2 carriers is 33 to 53 years.1 , 3 , 6 , 7 ls is one of several hereditary cancer syndromes that predispose to pbts and other systemic cancers . 
therefore , interrogation of personal and family history of malignancies is critical for patients with d 70s dx 47 d 52 d 50s d 50s d 30s d 50s d 40s d 60 dx 42 5 polyps 2 polyps throat abdominal cancer , other breast cancer colorectal cancer glioneuronal tumor fig 3 . 
the patients family history is notable for multiple maternal family members affected with early - onset colorectal cancer , including his mother and multiple maternal aunts , uncles , and cousins . 
next - generation sequencing of 236 genes in the patients tumor specimen ( solid tumor panel ; foundationone , cambridge , ma ) identied pathogenic genomic alterations in six genes and 18 variants of uncertain signicance . * follow - up sequencing of msh2 in the patients saliva sample ( ambry genetics , aliso viejo , ca ) also identied the msh2 mutation in the germline sample . pbt as for all patients with cancer . 
referral for genetic counseling and germline testing is recommended for any patient with pbt with multiple relatives affected with earlyonset cancers , individual ( s ) with multiple primary cancers , and / or rare or syndrome - specic patterns of malignancies.8 , 9 appropriate germline genetic testing may result in additional screening guidelines and the identication of other at - risk relatives.10 ls surveillance guidelines include colonoscopy every 1 to 2 years starting at age 20 to 25 years or 10 years before the earliest crc diagnosis in the family.11 histologic ndings in this patients pbt showed overlapping features between anaplastic pleomorphic xanthoastrocytoma , who grade iii , and glioblastoma . 
genetic alterations that are present in the tumor tissuethat is , nf1 , pdgfra , and tp53 mutationshave been described in glioblastomas12 , 13 ; however , survival of 8 years would be unusual for a patient with glioblastoma . one indicator that germline molecular testing was warranted for this patient was the identication of an msh2 mutation in his tumor specimen . 
studies that have evaluated the yield of germline variants after somatic testing indicate that a small but signicant number of tumors possess germline mutations related to hereditary cancer predisposition syndromes.14 - 17 currently , consideration of follow - up germline testing is recommended after identication of somatic egfr t790m mutations in lung cancer or brca1 / 2 mutations in any tumor.18 - 21 interpretation of somatic mmr mutations , however , is more complex . hampel et al22 used tumor sequencing to screen for ls in a cohort of patients with crc in which a positive screen for ls was given to any patient who had mutation ( s ) identied in at least one mmr gene at a variant allele fraction that was suggestive of a germline mutation , with msi and braf v600e status taken into account . 
therefore , whereas the identication of somatic mmr mutation ( s ) is not diagnostic of ls , it does suggest that follow - up germline evaluation is warranted in these patients . identifying germline and / or somatic mmr mutations may affect treatment offerings , such as consideration for immune checkpoint inhibitors ( icis ) , which target checkpoint receptors of mmr - decient cancers.23 - 25 early studies have demonstrated that icis can effectively treat high tmb cancers ; mmr - decient tumors can possess 10 to 100 times the tmb compared with mmr - procient cancers.26 - 28 glioblastoma specimens from patients with constitutional mmr deciency caused by biallelic germline mmr mutations have signicantly higher tmb compared with sporadic gliomas and other pbts.29 whereas icis have primarily been evaluated in crc and endometrial carcinomas , therapeutic potential has been demonstrated in other mmrdecient tumors . 
in patients with recurrent tumors , high tmb may indicate resistance to traditional chemotherapy and necessitate targeted treatment with icis or other immunotherapies.30 these results must be validated on a larger scale to inform clinicians of the potential therapeutic benets of ici in this subset of patients . in conclusion , we report the rst case of an individual with anaplastic glioneuronal tumor with atypical histologic features and paired somatic and germline msh2 mutations , indicating the diversity of pbts observed within ls . 
the presence of mmr gene mutation ( s ) in tumor specimens indicate that additional genetic evaluation is warranted . ihc , msi , and tmb analyses are also supportive of an ls diagnosis . 
furthermore , a family history evaluation for multiple relatives affected with early - onset cancers , dividual ( s ) with multiple primary cancers , and / or rare or syndrome - specic patterns of malignancies is imperative for all patients with pbt . 
in addition , identifying mmr deciency in the germline or tumor specimens may be an indication for targeted therapy via ici or other immunotherapies in the future . affiliations 1the university of texas md anderson cancer center , houston , tx 2university of texas health science center at houston , houston , tx 3foundation medicine , morrisville , nc 4wake forest school of medicine , winston - salem , nc relationships are self - held unless noted . 
qualmann provision of study materials or patients : jay - jiguang zhu , krista j . qualmann collection and assembly of data : sarah azam , jay - jiguang zhu , krista j . 
ramkissoon employment : foundation medicine stock and other ownership interests : foundation medicine sigmund hsu consulting or advisory role : abbvie , cns pharmaceuticals research funding : abbvie patents , royalties , other intellectual property : partial patent holder , royalties ; at the time of ling , was associated with md anderson cancer center jay - jiguang zhu consulting or advisory role : tocagen research funding : novocure ( inst ) , boston biomedical ( inst ) , five prime therapeutics ( inst ) , tocagen ( inst ) , immunocellular therapeutics ( inst ) travel , accommodations , expenses : zai lab krista j . 
qualmann employment : my gene counsel no other potential conicts of interest were reported . references vasen hfa , stormorken a , menko fh , et al : msh2 mutation carriers are at higher risk of cancer than mlh1 mutation carriers : a study of hereditary nonpolyposis colorectal cancer families . 
int j cancer 81 : 214 - 218 , 1999 therkildsen c , ladelund s , rambech e , et al : glioblastomas , astrocytomas and oligodendrogliomas linked to lynch syndrome . 
n engl j med 348 : 919 - 932 , 2003 vasen hfa , sanders eacm , taal bg , et al : the risk of brain tumours in hereditary non - polyposis colorectal cancer ( hnpcc )  . 
hampel h , bennett rl , buchanan a , et al : a practice guideline from the american college of medical genetics and genomics and the national society of genetic counselors : referral indications for cancer predisposition assessment . 
catenacci dv , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
b. , et al : molecular testing guideline for selection of lung cancer patients for egfr and alk tyrosine kinase inhibitors : guideline from the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology . 
hampel h , pearlman r , beightol m , et al : assessment of tumor sequencing as a replacement for lynch syndrome screening and current molecular tests for patients with colorectal cancer . 
sloan ea , ring kl , willis bc , et al : pd - l1 expression in mismatch repair - decient endometrial carcinomas , including lynch syndrome - associated and mlh1 promoter hypermethylated tumors . 
science 357 : 409 - 413 , 2017 johnson a , severson e , gay l , et al : comprehensive genomic proling of 282 pediatric lowand high - grade gliomas reveals genomic drivers , tumor mutational burden , and hypermutation signatures . 
 genomic proling identies outcome - relevant mechanisms of innate and acquired resistance to third - generation epidermal growth factor receptor tyrosine kinase inhibitor therapy in lung cancer sebastian michels , md1 ; carina heydt , phd1 ; bianca van veggel , md2 ; barbara deschler - baier , md3 ; nuria pardo , md4 ; kim monkhorst , md2 ; vanessa r usseler , md1 ; jan stratmann , md5 ; frank griesinger , md6 ; susanne steinhauser , phd7 ; anna kostenko , msc1 ; joachim diebold , md8 ; jana fassunke , phd1 ; rieke fischer , md1 ; walburga engel - riedel , md9 ; oliver gautschi , md8 ; eva geissinger , md10 ; stefan haneder , md1 ; michaela a . 
de langen , md2 ; alex martinez - marti , md4 ; lucia nogova , md1 ; thorsten persigehl , md1 ; dennis plenker , phd1 ; michael puesken , md1 ; ernst rodermann , md12 ; andreas rosenwald , md10 ; andreas h . 
scheel , md1 ; matthias schefer , md1 ; werner spengler , md13 ; ruth seggewiss - bernhardt , md14 ; johannes br agelmann , md1 , 7 ; martin sebastian , md5 ; bart vrugt , md15 ; martin hellmich , phd7 ; martin l . 
smit , md2 ; reinhard b uttner , md1 ; and j urgen wolf , md1 purpose third - generation epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitors ( tkis ) are effective in acquired resistance ( ar ) to early - generation egfr tkis in egfr - mutant lung cancer . 
we present the molecular proles of pretreatment and post - treatment samples from patients treated with third - generation egfr tkis and their impact on treatment outcomes . methods using the databases of two lung cancer networks and two lung cancer centers , we molecularly characterized 124 patients with egfr p.t790m - positive ar to early - generation egfr tkis . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction treatment with selective early - generation epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitors ( tkis ) has demonstrated high efcacy in patients with lung cancer harboring activating egfr mutations . 
we present a comprehensive analysis of cooccurring genetic aberrations in pretreatment and posttreatment tumor tissue and their contribution to innate resistance ( ir ) and ar to three third - generation egfr tkis . methods study design , patient selection , and tumor tissue collection to determine the frequency of co - occurring genetic aberrations in samples of egfr p.t790m - mediated resistance to early - generation egfr tkis , we systematically searched the databases of the network genomic medicine , the nowel network , the department of thoracic oncology of the netherlands cancer institute , and the institute of oncology at the vall dhebron university hospital for patients with nonsmall - cell lung cancer ( nsclc ) who fullled the following selection criteria ( cohort a ; patients a1 to a68 / b1 to b56 ; fig 1 ; data supplement ) : ( 1 ) presence of cohort a ( n = 124 ; 100% ) 1 . 
cnv , copy number variation ; egfr , epidermal growth factor receptor ; erbb2 , human epidermal receptor 2 growth factor gene ; met , mesenchymalepithelial transition factor ; mps , massively parallel sequencing ; nsclc , non small - cell lung cancer ; recist , response evaluation criteria in solid tumors ; seq , sequencing ; tki , tyrosine kinase inhibitor . excluded ( n = 68 ) excluded ( n = 27 ) cohort b ( n = 56 ; 45% ) 1 . 
patients were treated in the aura 1 / 3 trials ( osimertinib ; nct01802632 / nct02151981 ) , tiger - 2 / - 3 trials ( rociletinib ; nct02147990 / nct02322281 ) , cegf816x2101 trial ( nazartinib ; nct 02108964 ) , osimertinib compassionate use program ( cup ) , or clinical routine . 
patients treated in trials or the cup were selected according to the specic eligibility criteria . in a subset of patients from cohort b , a rebiopsy was performed at disease progression for identication of mechanisms of ar . 
these patients were grouped in cohort c ( fig 1 )  . in all patients , tumor tissue was collected in growing lesions by aspiration biopsy , core needle biopsy , or excisional biopsy ( data supplement )  . 
in patients screened within network genomic medicine ( a1 to a68 / b1 to b31 / b37 to b43 ) , mps was performed with an ion ampliseq custom dna panel ( thermo fisher scientic , waltham , ma ) and a miseq benchtop sequencer ( illumina , san diego , ca ) or with a generead dnaseq custom panel v2 ( qiagen , santa clarita , ca ) consisting of 205 amplicons.31 in patients screened within the nowel network ( a33 to a36 ) , sequencing was performed using the neoplus hybrid - capturebased approach ( neo new oncology , cologne , germany )  . 
in the post - treatment samples ( cohort c ) of b41 to b56 , met and erbb2 status was assessed by uorescence in situ hybridization or chromogen in situ hybridization only if cnvs were detected by mps . small - cell lung cancer transformation was assessed using microscopy by experienced pathologists . 
progression - free survival ( pfs ) indicated the time from treatment start until pd or death . overall survival ( os ) was dened as the time from rst diagnosis until death . 
differences in time - to - event distribution were evaluated by the log - rank test , and statistical association between any two categorical variables was assessed by fishers exact test ; 95% cis for proportions were calculated using the clopper - pearson ( binominal ) formula . 
map of genetic aberrations detected by sequencing ( single nucleotide variant [ snv ] and insertion / deletion [ indel ] ) and copy number variation ( cnv ) analyses in biopsy specimens of epidermal growth factor receptor ( egfr ) p.t790m - positive patients before treatment with a third - generation egfr tyrosine kinase inhibitor ( tki ; ie , osimertinib , rociletinib , nazartinib ; upper block ; cohort b ; n = 56 ) and at progression to the specic treatment ( lower block ; cohort c ; n = 29 )  . 
the change in the frequency of specic aberrations during the course of treatment in matched samples is indicated in the lower block on the far right ( matched )  . 
 ( a ) waterfall plot showing the best change in percent of the target lesions according to response evaluation criteria in solid tumors ( recist ) 1.1 per patient during treatment with a third - generation epidermal growth factor ceptor tyrosine ( egfr ) kinase inhibitor ( tki ; n = 56 ; cohort b )  . 
kaplan - meier graphs displaying ( b ) progressionfree survival and ( c ) overfor patients with egfr p.t790m - posinonsmall - cell lung tive cancer with ( nsclc ) and without mesenchymaltransition factor epithelial ( met ) amplication ( ampl ) , who received treatment with third - generation egfr tkis . both median overall survival and progression - free survival are dramatically reduced in the presence of met amplications . 
erbb2 , human epidermal growth factor receptor 2 gene ; wt , wild type . survival time ( months ) 144 168 192 72 96 120 time ( months ) no . 
at risk ampl ampl tumor stage , gender , smoking status , and the initial number of prior egfr tkis had no signicant impact on treatment outcomes ( table 1 )  . 
the patient received local radiotherapy and died approximately 1.5 months timeline showing the course of treatment of a 76 - year - old female patient initially diagnosed at stage ii . 
fu , follow - up ; pd , progressive disease . percentage of samples in which we detected acquired changes in the molecular pattern was 89% ( n = 23 )  . 
the third most common genetic changes in cohort c were acquisition of egfr p.c797s ( n = 3 of 29 ; 10% ) , of which two were in cis and one in trans position , and loss of p.t790m with acquisition of p.g724s ( n = 3 of 28 ; 11% )  . 
acquired mutations in braf ( p.v600e ) , tp53 ( p.e180 * ) , and pten ( p.s229 * ) were detected in one sample each ( 4% )  . 
 ( a ) map of genetic aberrations detected by sequencing ( single nucleotide variant [ snv ] and insertion / deletions [ indels ] ) and copy number variation ( cnv ) analyses in biopsy specimens collected after treatment with a third - generation epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitor ( tki ; cohort c ; n = 29 )  . 
patients were clustered in four groups : ( i ) changes outside of egfr only , ( ii ) changes in egfr and outside of egfr , ( iii ) changes in egfr only , and ( iv ) no changes found . 
the change in the frequency of specic aberrations during the course of treatment in matched samples is indicated in the lower block on the far right ( matched )  . 
erbb2 amplications were all found in samples that also harbored amplications of met . we therefore clustered the patients in four groups : ( i ) changes outside of egfr only , ( ii ) changes in egfr and outside of egfr , ( iii ) changes in egfr only , and ( iv ) no changes found ( fig 5a )  . 
in patients treated with osimertinib , a larger fraction belonged to cluster iii than cluster i or ii ( n = 10 ; 47 . 6% for iii v n = 5 ; 23.8% for i and ii )  . 
in patients treated with rociletinib , this trend was inversed ( changes in egfr , n = 0 ; 0% v no changes found , n = 4 ; 100% )  . 
however , most of these reports were not statistically signicant , and similarly , os , rr , and pfs were only numerically reduced in patients with tp53 mutations in our study.32 - 38 patient numbers with aberrations in pten , pik3ca , and erbb2 were low , and the differences in treatment efcacy were not statistically signicant . 
erbb2 , human epidermal growth factor receptor 2 gene ; freq , frequencies ; met , mesenchymal - epithelial transition factor ; pr , partial response ; sclc , small - cell lung cancer ; sd , stable disease ; wt , wild type . 
 michels et al met amplication was the second most frequent event associated with ar to third - generation egfr inhibition , and similar frequencies have been described in the literature.19 , 23 the high prevalence of met amplication in ir and ar points out the crucial role of met in egfr inhibitor resistance . 
in contrast , no patient treated with rociletinib displayed changes in egfr , and other studies have conrmed the absence of secondary egfr mutations in patients with progression while taking rociletinib.19 , 43 it is conceivable that this effect may be caused by a lower selection pressure of rociletinib on cells with on - target aberrations . 
however , differences in pfs or os after pd were not signicant . in summary , our study rst shows that molecular heterogeneity of p.t790m - mutant lung cancer with ar to earlygeneration egfr tkis inuences efcacy of thirdgeneration inhibitors . 
our observations also show the need to integrate information on co - occurring alterations in the design of clinical trials , aiming at a more precise identication of patients who benet from combined targeted treatment . 
but mechanisms of resistance to rst - line osimertinib have not been well characterized , and it is conceivable that recurrent mechanisms of resistance to egfr inhibition such as met amplication , met activation , and egfr p.c797s may also play a major role in this setting . affiliations 1university hospital of cologne , cologne , germany 2netherlands cancer institute , amsterdam , the netherlands 3university hospital of w urzburg and comprehensive cancer center mainfranken , w urzburg , germany 4vall d ' hebron university hospital , barcelona , spain 5university hospital of frankfurt , frankfurt , germany 6pius hospital oldenburg and lung cancer network nowel , oldenburg , germany 7university of cologne , cologne , germany 8cantonal hospital lucerne , lucerne , switzerland 9lung clinic merheim and hospitals of cologne , cologne , germany 10university of w urzburg and comprehensive cancer center mainfranken , w urzburg , germany 11robert bosch centrum f ur tumorerkrankungen , stuttgart , germany 12private practice in hematology and oncology , troisdorf , germany 13university hospital of t ubingen . 
smit , reinhard b uttner , juergen wolf data analysis and interpretation : sebastian michels , carina heydt , bianca van veggel , nuria pardo , kim monkhorst , frank griesinger , susanne steinhauser , michaela a . 
ihle , alex martinez - marti , lucia nogova , thorsten persigehl , dennis plenker , michael puesken , andreas rosenwald , werner spengler , martin sebastian , martin hellmich , enriqueta felip , sabine merkelbach - bruse , egbert f . 
de langen consulting or advisory role : astrazeneca ( inst ) , bristol - myers squibb ( inst ) , msd oncology ( inst ) , roche ( inst ) , boehringer ingelheim ( inst ) , pzer ( inst ) research funding : astrazeneca ( inst ) , bristol - myers squibb ( inst ) , merck serono ( inst ) , msd oncology ( inst ) , roche ( inst ) alex martinez - marti honoraria : roche , bristol - myers squibb , merck sharp & dohme , pzer , boehringer ingelheim consulting or advisory role : bristol - myers squibb , f . 
scheel honoraria : msd , bristol - myers squibb , roche , dako / agilent technologies consulting or advisory role : msd , bristol - myers squibb , roche , dako / agilent technologies matthias schefer honoraria : healthcare consulting cologne , boehringer ingelheim , takeda consulting or advisory role : boehringer ingelheim , takeda travel , accommodations , expenses : boehringer ingelheim ruth seggewiss - bernhardt honoraria : novartis , celgene , roche , bristol - myers squibb , ipsen , pzer , astrazeneca consulting or advisory role : msd , pzer travel , accommodations , expenses : astellas pharma , celgene , ipsen martin sebastian honoraria : astrazeneca , novartis , pzer / emd serono , msd , takeda , bristol - myers squibb , eli lilly , genentech , boehringer ingelheim , abbvie consulting or advisory role : genentech , msd , astrazeneca , abbvie , takeda , eli lilly , boehringer ingelheim , novartis , bristol - myers squibb , pzer , celgene travel , accommodations , expenses : pzer , takeda martin l . 
heukamp employment : neo new oncology , h amatopathologie hamburg honoraria : roche pharma , astrazeneca , bristol - myers squibb , boehringer ingelheim consulting or advisory role : roche pharma , bristol - myers squibb , novartis enriqueta felip consulting or advisory role : pzer , roche , boehringer ingelheim , astrazeneca , bristol - myers squibb , celgene , guardant health , novartis , takeda , abbvie , blueprint medicines , eli lilly , merck kgaa , merck sharp & dohme speakers ' bureau : astrazeneca , bristol - myers squibb , novartis , boehringer ingelheim , merck sharp & dohme , roche , pzer , abbvie , eli lilly , merck kgaa , takeda research funding : fundaci on merck salud ( inst ) , emd serono ( inst ) sabine merkelbach - bruse honoraria : astrazeneca , bristol - myers squibb , novartis , pzer , roche pharma consulting or advisory role : bristol - myers squibb , novartis , pzer egbert f . 
han jy , park k , kim sw , et al : first - signal : first - line single - agent iressa versus gemcitabine and cisplatin trial in never - smokers with adenocarcinoma of the lung . 
j clin oncol 30 : 1122 - 1128 , 2012 rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutationpositive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
lancet oncol 13 : 239 - 246 , 2012 zhou c , wu yl , chen g , et al : erlotinib versus chemotherapy as rst - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
lancet oncol 12 : 735 - 742 , 2011 sequist lv , yang jch , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
j clin oncol 31 : 3327 - 3334 , 2013 sequist lv , waltman ba , dias - santagata d , et al : genotypic and histological evolution of lung cancers acquiring resistance to egfr inhibitors . 
sci transl med 3 : 75ra26 , 2011 yu ha , arcila me , rekhtman n , et al : analysis of tumor specimens at the time of acquired resistance to egfr - tki therapy in 155 patients with egfr - mutant lung cancers . 
kasibhatla s , li j , tompkins c , et al : egf816 , a novel covalent inhibitor of mutant - selective epidermal growth factor receptor , overcomes t790m - mediated resistance in nsclc . 
cancer res 74 , 2014 ( suppl ; abstr 1733 ) j anne pa , yang jch , kim dw , et al : azd9291 in egfr inhibitor - resistant non - small - cell lung cancer . 
tan dsw , seto t , leighl nb , et al : first - in - human phase i study of egf816 , a third - generation , mutant - selective egfr tyrosine kinase inhibitor , in advanced non - small cell lung cancer ( nsclc ) harboring t790m . 
bean j , brennan c , shih jy , et al : met amplication occurs with or without t790m mutations in egfr mutant lung tumors with acquired resistance to getinib or erlotinib . 
schefer m , merkelbach - bruse s , bos m , et al : spatial tumor heterogeneity in lung cancer with acquired epidermal growth factor receptor - tyrosine kinase inhibitor resistance : targeting high - level met - amplication and egfr t790m mutation occurring at different sites in the same patient . 
blakely cm , watkins tbk , wu w , et al : evolution and clinical impact of co - occurring genetic alterations in advanced - stage egfr - mutant lung cancers . 
yang z , yang n , ou q , et al : investigating novel resistance mechanisms to third - generation egfr tyrosine kinase inhibitor osimertinib in non - small cell lung 26 . 
eberlein ca , stetson d , markovets aa , et al : acquired resistance to mutant - selective egfr inhibitor azd9291 is associated with increased dependence on ras cancer patients . 
k onig k , peifer m , fassunke j , et al : implementation of amplicon parallel sequencing leads to improvement of diagnosis and therapy of lung cancer patients . j thorac oncol 10 : 1049 - 1057 , 2015 32 . 
molina - vila ma , bertran - alamillo j , gasc o a , et al : nondisruptive p53 mutations are associated with shorter survival in patients with advanced non - small cell lung cancer . 
aisner dl , sholl lm , berry l , et al : the impact of smoking and tp53 mutations in lung adenocarcinoma patients with targetable mutations - the lung cancer mutation consortium ( lcmc2 )  . 
labb e c , cabanero m , korpanty gj , et al : prognostic and predictive effects of tp53 co - mutation in patients with egfr - mutated non - small cell lung cancer 36 . 
vanderlaan pa , rangachari d , mockus sm , et al : mutations in tp53 , pik3ca , pten and other genes in egfr mutated lung cancers : correlation with clinical ( nsclc )  . 
shepherd fa , lacas b , le teuff g , et al : pooled analysis of the prognostic and predictive effects of tp53 comutation status combined with kras or egfr mutation in early - stage resected non - small - cell lung cancer in four trials of adjuvant chemotherapy . 
canale m , petracci e , delmonte a , et al : impact of tp53 mutations on outcome in egfr - mutated patients treated with rst - line tyrosine kinase inhibitors . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a third - generation egfr inhibitor . 
thirty - one patients ( 38% ) and 17 patients ( 46% ) underwent germline testing from the automatic pipeline and other referrals , respectively , and of these patients , 23 ( 72% ) and four ( 24% ) had conrmed germline pathogenic variants ( gpvs ) , respectively . 
the majority of conrmed gpvs were in automatic referral genes , with brca2 being most common ( conrmed gpvs in 11 [ 85% ] of 13 patients tested ) , followed by palb2 ( ve [ 67% ] of six patients ) , brca1 ( two [ 40% ] of ve patients ) , msh6 ( two of three patients ) , and mlh1 ( two of two patients )  . 
germline testing was not performed in 50 ( 62% ) of 81 patients identied by automatic referral as a result of poor patient health or death ( 30% ) , lack of follow - up ( 30% ) , and patient refusal ( 30% )  . conclusion of patients undergoing tgp , 5% had somatic ndings triggering referral , and implementation of an automatic referral pipeline based solely on gene versus other clinical or molecular features resulted in a 74% germline conrmation . 
use of such testing has rapidly increased , with further growth anticipated.1 mutations identied on tumor sequencing may be acquired somatically , caused by postzygotic mosaicism , or identication of inherited through the germline . germline mutations potentially inuences treatment of the current cancer , may provide prognostic information about the potential development of future cancers , and has important implications for family members in terms of risk and prevention of disease.2 however , guidelines on both how to determine which somatic ndings may be potentially germline and the optimal clinical practice for referral and germline testing of patients undergoing tumor sequencing are not widely available , and there is no established standard of care.3 genomic testing of tumor tissue can be performed in tandem with germline testing ( via blood or sequence matched normal tissue ) 4 - 6 ; such tumor - germline paired sequencing allows determination of mutation etiology ( inherited v acquired )  . 
 clark et al context key objective as the use of somatic tumor genomic testing rapidly increases , a pipeline for referral of potential germline genetic ndings is critically needed . knowledge generated more than 70% of known cancer predisposition gene mutations identied in patients tumor genomic testing were conrmed to be germline . 
however , less than half of eligible patients underwent germline genetic testing as a result of poor patient health or death , lack of follow - up , and / or patient refusal . relevance our ndings indicate that patients with pathogenic mutations in well - characterized cancer predisposition genes should be referred for consideration of germline genetic testing , although signicant implementation challenges remain . be associated with hereditary cancer syndromes for both the patients and their family members . 
however , potential germline variants on tgp may be under - recognized.8 national comprehensive cancer network ( nccn ) guidelines are evolving ; they currently state that pathogenic variants in cancer susceptibility genes identied on tumor proling of any tumor type should undergo germline conrmation.9 however , the logistics of identifying potentially actionable germline mutations , such as those in brca1 and brca2 , from tgp can be complex , in large part as a result of the coordination of germline genetic testing for ill patients who may be unaware that their tumor testing could reveal inherited mutations . 
somatic pathogenic mutations as dened in cbioportal were downloaded from the provisional data sets of multiple tumor types in july 2015 ( data supplement ) and updated in july 2018 ( table 1 )  . 
original germline mutation rates were averaged from two large studies of patients with metastatic cancer5 , 6 and updated with tcga data , 11 and mutations were dened as reported in the original studies.5 , 6 , 11 the ratio of the germline mutation rate to total mutation rate was determined ( table 1 ; appendix fig a1 )  . 
genes were also annotated with the number of tumor types with somatic mutation rates greater than 10% ( data supplement )  . delineation of criteria for automatic referral for germline testing criteria for automatic referral for germline testing after tgp from june 2016 through june 2018 , the center for personalized diagnostics ( cpd ; college of american pathologists and clinical laboratory improvement amendments approved ) at penn medicine evaluated 2 , 308 unique tgp tests with either a 153 - gene panel ( n = 2 , 087 ) or a 47 - gene panel ( n = 221 ) , depending on the version of the panel available ( data supplement )  . 
a multidisciplinary team , including genetic counselors , medical oncologists , medical geneticists , and molecular pathologists , was established to determine which somatic results warranted automatic referral for germline genetic testing . 
 clark et al was not included in our analysis because of controversy over screening guidelines and its relatively high prevalence.12 implementation of germline testing referral pipeline solid tumor sequencing reports were signed out per clinical practice standards , and variants in the automatic referral pipeline were identied manually by the reviewing cpd attendings . 
language for clinical reports was created stating that additional testing would be necessary to determine whether the identied pathogenic variant on somatic testing was a germline pathogenic variant ( gpv )  . 
an e - mail was sent from the cpd to the ordering oncologist and a designated genetic counselor ( gc ) when a variant meeting automatic referral criteria was identied . 
initial disclosure of the somatic test results , including the possibility of a germline nding , was the responsibility of the ordering provider.13 after patients were made aware of somatic ndings by their oncologist , patients were contacted by the gc for coordination of care . 
molecular pathologists and oncologists also were encouraged to refer patients outside the automatic pipeline on the basis of genotype - phenotype correlation . data collection , chart review , and statistical analysis a university of pennsylvania institutional review board approved retrospective chart review was conducted , with data collected for all referrals within the automatic pipeline and other referrals based on tgp by the academic laboratory between june 2016 and june 2018 ( 81 referrals by automatic pipeline and 37 referrals outside the pipeline )  . data were collected on patient demographics , tumor type tested ( data supplement ) , and somatic and germline testing results . 
continuous variables were compared using the t test , and contingency tables were analyzed using fishers exact test . results referral characteristics from june 2016 to june 2018 , 2 , 308 patients underwent tgp at penn medicines cpd . 
of those patients , 118 ( 5.1% ) were referred for clinical germline genetic testing based on tgp performed at the cpd . referral of 81 patients was triggered by the automatic algorithm , and 37 patients were referred from either the molecular pathologist ( n = 21 ) or the patients physician ( n = 16 ; fig 2a )  . 
the majority of patients were white ( 88% ) and female ( 52% ) , and the mean age at tgp was tumor types 58 years ( table 2 )  . 
thirteen patients were referred for variants with a high likelihood in chek2 of being germline ( founder mutations ) ( n = 11 ) and one each for variants in atm and egfr ( fig 2a ; data supplement )  . 
direct referrals for germline genetic testing by the molecular pathologist and primary oncologists after a variant was found on tgp were largely based on genotype - phenotype concerns ( eg , tp53 mutations in patients with cancer age 45 years or younger or patients with brain tumors or sarcomas ; cdkn2a / cdk4 mutations in patients with melanoma )  . 
referrals of 21 patients by the molecular pathologist were initiated by e - mail to the gc and primary oncologist and included ndings in nine genes , most commonly tp53 ( fig 2a ; data supplement )  . treating physicians referred 16 patients with variants in 12 different genes ( fig 2a , data supplement )  . results of germline conrmation of 118 patients with referrals , 48 ( 41% ) underwent clinical genetic counseling and genetic testing ( fig 2a )  . 
genetic testing rates were similar for referrals from the automatic referral pipeline and those sent by the molecular pathologist ( 38% and 33% , respectively ) , whereas 63% of patients referred by their treating physician underwent genetic testing ( fig 2a )  . 
a majority of patients ( 27 [ 57% ] of 48 patients ) had variants that were conrmed gpvs , with 74% of automatic referrals being conrmed gpvs and 29% and 20% of molecular pathologist and treating physician referrals being conrmed gpvs ( fig 2a )  . 
the majority of patients ( 60% ) had multiplex panel testing ; however , 19% underwent a small custom panel , 17% were only tested for the variant by single - site testing , and 4% had ashkenazi jewish founder testing ( data supplement )  . the 81 patients referred by the automatic referral pipeline , the majority ( n = 59 ) were referred for variants in high - risk genes ( 73% ; fig 2b )  . 
genetic testing rates were highest for high - risk genes ( 28 referrals [ 47% ] underwent genetic testing compared with three referrals [ 14% ] in the other groups )  . 
mutations in the automatic referral pipeline were agged by the tumor testing laboratory , and an e - mail was sent from molecular pathologist to the ordering physician ( md ) and genetic counselor ( gc )  . 
results not included in the automatic referral pipeline but of concern to the molecular pathologist or ordering oncologist to be possibly germline were also e - mailed to the gc . 
the gc called the patient only after the somatic results were discussed with the patient by the ordering md , the patient agreed to be contacted , and the oncologist contacted the gc . 
an inperson cancer risk evaluation appointment was scheduled , and the appropriate germline testing modality was determined by gc at time of visit ( panel or single - site testing )  . 
results were provided by telephone by the gc , and patients with positive testing results along with their relatives were offered in - person follow - up visits for medical management . 
one hundred eighteen patients were referred for germline testing83 by the automatic pipeline , 20 by the testing laboratory at the discretion of the molecular pathologist , and 15 directly from the ordering physician . 
 ( b ) of the 83 patients referred by the automatic pipeline , 61 had mutations in high - risk genes ( brca1 , brca2 , palb2 , mlh1 , msh2 , and msh6 ) , nine had mutations in moderate - risk genes ( brip1 , rad51c , and rad51d ) , and 13 had mutations with high prior probability of being germline ( likely germline )  . 
 ( c ) in the 51 patients referred by the automatic pipeline but who did not undergo testing , patients were not seen as a result of death before scheduling an appointment , refusal of the consult by the patient , absence of referral placed by ordering physician , or other reason . or both ( fig 2c )  . 
 characteristic age , years mean range male race tumor type white black other lung brain breast other melanoma 526 ( 23 ) 676 ( 29 ) 519 ( 22 ) 125 ( 5 ) 59 ( 3 ) 25 ( 1 ) 122 ( 5 ) germline results in tumor - only genomic testing table 2 . 
 ( a ) in patients who presented for conrmatory germline testing , the age at diagnosis for patients with a conrmed germline pathogenic variant ( gpv ) versus somatic pathogenic variants ( spvs ) not conrmed to be in the germline . 
 ( c ) percentage of patients with a conrmed gpv versus an spv for whom the gene is known to be associated with the tumor where the variant was found . 
of 2 , 308 patients who underwent tgp at penn medicines cpd , 149 ( 6.6% ) had variants in the automatic referral genes , and 118 ( 5% ) were referred for clinical germline genetic testing . 
a majority of the variants tested were conrmed gpvs ( 27 [ 54% ] of 50 variants ) , with the highest germline conrmation rate in high - risk genes ( 21 [ 72% ] of 29 genes )  . 
thus , we have demonstrated that an automatic referral algorithm results in a high yield of conrmed germline mutations . in total , 27 ( 1.1% ) of 2 , 308 patients undergoing tgp had a conrmed gpv . 
germline ndings have been found by retrospective analysis in 4% to 12% of prior clinical tumor sequencing cohorts5 , 6 , 14 and in 8% of the tcga cohort , 11 with 2.8% of the tcga cohort having germline mutations in the genes selected for automatic referral in this study . 
if all 149 patients with mutations in automatic referral genes in our cohort had undergone germline testing , we would have expected 107 to have a germline mutation ( based on our 72% germline conrmation rate )  . 
a limitation of this study is that sequencing was not performed on all patients with metastatic disease at the university of pennsylvania ; in addition , germline sequencing was not performed in all dividuals with somatic sequencing . 
thus , we do not know the exact prevalence of germline mutations in our population . genes were chosen for automatic referral based on several factors , but the major determinant was the ratio of germline mutation rate to total ( germline plus somatic ) mutation rate calculated from public databases . 
thus , referring all individuals with mutations identied in such genes ( eg , tp53 and pten ) identied by tgp in the absence of other factors rarely results in a positive germline nding . 
however , other genes have higher mutation rates in the germline compared with somatic only ( eg , brca1 / 2 ) , and known founder mutations would likely always be germline . 
for example , in our study , all three ashkenazi jewish founder mutations in brca1 / 2 that were found on tgp were conrmed gpvs . the automatic referral algorithm did not rely on clinical characteristics or variant af or exclude patients with likely hypermutated tumors . 
the nding that germline af can be lower than the expected range of 50% or greater is consistent with prior data.15 multiple patients had germline mutations identied despite somatic testing done on tumors not generally considered part of the hereditary syndrome . 
the high germline conrmation rate for the automatic referral genes validates our approach of prioritizing the ratio of germline to total mutations of a gene , with lesser emphasis placed on af or tumor type . 
we have updated both germline and somatic mutation rates with current11 data ( table 1 ) , demonstrating that most of these genes have a ratio of germline mutation rate to total mutation rate of greater than 0.25. 
the only genes not included on our original list that t these criteria are atm and chek2 . we are adding all mutations in these genes to our referral list ( rather than restricting to certain mutations with high prior probability of being germline )  . other approaches for gene selection exist ; however , we wished to prioritize the highest impact genes related to prognosis or therapy , clinical trial enrollment ( eg , brca1 / 2 mutations and poly [ adp - ribose ] polymerase inhibitors ) , or effect on family members.16 - 19 in addition , we wished to assess the success of this approach and potential burdens before widening the scope . 
curation of the list of genes in which mutations prompt referral for germline genetic testing will be an ongoing process and will need to reect updates in guidelines from the american college of medical genetics and nccn . 
the automated referral algorithm had a high specicity , as 72% of ndings were conrmed gpvs . in patients for whom somatic sequencing triggered a referral by their oncologist without meeting criteria on the algorithm , only two patients ( 20% ) had conrmed gpvs ( atm and chek2 )  . 
as mentioned earlier , both genes are being added to our automated referral algorithm . criteria for germline genetic testing are rapidly evolving , and routine germline multiplex panel testing may soon become standard for all patients with metastatic disease . 
in our study , of 28 patients who underwent multiplex panels , either testing was negative ( n = 13 ) or only the somatic variant was found ( n = 15 ) , indicating that there may be limited incremental benet to expanded germline testing in patients with metastatic cancer who have undergone tumor testing . 
however , individuals with a high likelihood of having a germline mutation in a cancer susceptibility gene should be considered for germline testing even in the setting of a negative tgp . 
for example , in individuals with a strong family history of breast and ovarian cancer , approximately 10% of brca1 mutations are large genomic rearrangement , which may be more difcult to detect with current tgp assays . the majority of patients ( 61% ) with a somatic nding identied by the automatic referral pipeline were not seen by clinical cancer genetics services . 
published data suggest that patients express great interest in wishing to learn their germline status20 ; therefore , it is likely that patient and provider education and improved infrastructure for referrals are needed . 
 germline results in tumor - only genomic testing cancer therapy and symptom management , simplifying the process by which patients become aware of the possibility of germline ndings arising from tgp and have access to germline conrmation is critical . 
the ongoing communication and education in tumor proling ( comet ) trial ( clinicaltrials.gov identier : nct02823652 ) , a companion study to the national cancer institute molecular analysis for therapy choice ( nci - match ) trial , will provide additional information regarding best practices . genetic counseling challenges in this population of patients with advanced cancer included the substantial burden of patient illness ( including both symptom and appointment burdens , although considerable efforts were made to coordinate appointments with other visits )  . 
there was an appreciable time commitment by the gc that was not billable ( eg , discussions by phone ) , and a number of patients tested did not have insurance coverage because their tumor type did not meet published criteria for germline testing . 
nccn criteria for further genetic risk evaluation ( version 2.2019 ) now include individuals at any age with a known pathogenic variant or likely pathogenic variant in a cancer susceptibility gene found on tumor testing ; however , during the dates of our study , existing criteria included brca1 / 2 only.9 we performed a single - institution study and only evaluated ndings from penn medicines cpd ; thus , generalizability of this approach is not yet known . 
in addition , full somatic sequencing for all of the automatic referral genes was not performed on every patient as a result of availability of specic somatic sequencing panels at different points in time . 
we did not implement approaches such as telegenetics , which may further reduce patient burden ( although germline samples must still be obtained )  . we have demonstrated that an automated referral process for patients with mutations detected in tgp can lead to the identication of germline mutations in cancer susceptibility genes with implications for both patients and their family members . 
 clark et al jacquelyn powers employment : carevive systems honoraria : cureconnect consulting or advisory role : carevive systems travel , accommodations , expenses : hospital of the university of pennsylvania jessica m . 
long employment : depuy companies ( i ) stock and other ownership interests : depuy companies ( i ) travel , accommodations , expenses : depuy companies ( i ) payal shah stock and other ownership interests : johnson & johnson ( i ) , novartis ( i ) , novo nordisk ( i ) , pzer ( i ) , merck ( i ) , amgen , johnson & johnson , novo nordisk consulting or advisory role : tmunity therapeutics jennifer j.d. 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) no other potential conicts of interest were reported . references raymond vm , gray sw , roychowdhury s , et al : germline ndings in tumor - only sequencing : points to consider for clinicians and laboratories . 
j pathol 244 : 610 - 615 , 2018 arango np , brusco l , mills shaw kr , et al : a feasibility study of returning clinically actionable somatic genomic alterations identied in a research laboratory . oncotarget 8 : 41806 - 41814 , 2017 4 . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
ann oncol 27 : 795 - 800 , 2016 schrader ka , cheng dt , joseph v , et al : germline variants in targeted tumor sequencing using matched normal dna . 
jama oncol 2 : 104 - 111 , 2016 robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . j clin oncol 33 : 3660 - 3667 , 2015 catenacci dv , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 9 . 
yurgelun mb , chittenden ab , morales - oyarvide v , et al : germline cancer susceptibility gene variants , somatic second hits , and survival outcomes in patients with resected pancreatic cancer . 
bolton kl , chenevix - trench g , goh c , et al : association between brca1 and brca2 mutations and survival in women with invasive epithelial ovarian cancer . 2014 res 22 : 4087 - 4094 , 2016 jama 307 : 382 - 390 , 2012 33 : 244 - 250 , 2015 18 . 
hamilton jg , shuk e , garzon mg , et al : decision - making preferences about secondary germline ndings that arise from tumor genomic proling among patients with advanced cancers . 
 germline results in tumor - only genomic testing appendix brca1 brca2 palb2 mlh1 msh2 msh6 brip1 rad51c rad51d chek2 tp53 bap1 cdh1 cdkn2a men1 pten smad4 smarca4 stk11 tsc1 tsc2 original updated ratio of germline mutation rate to overall mutation rate fig a1 . 
 o prevalence of homologous recombinationrelated gene mutations across multiple cancer types purpose the prevalence of homologous recombination dna damage repair ( hr - ddr ) deficiencies among all tumor lineages is not well characterized . 
therapy directed toward homologous recombination ddr deficiency ( hrd ) is now approved in ovarian and breast cancer , and there may be additional opportunities for benefit for patients with other cancers . 
comprehensive evaluations for hrd are limited in part by the lack of a uniform , cost - effective method for testing and defining hrd . methods molecular profiles of 52 , 426 tumors were reviewed to identify pathogenic mutations in the hr - ddr genes arid1a , atm , atrx , bap1 , bard1 , blm , brca1 / 2 , brip1 , chek1 / 2 , fanca / c / d2 / e / f / g / l , mre11a , nbn , palb2 , rad50 , rad51 , rad51b , or wrn . 
 a total of 17 , 566 tumors were sequenced with ngs600 ( n = 592 genes ) , and 34 , 860 tumors underwent hotspot illumina miseq platform testing ( n = 47 genes )  . results of the tumors that underwent ngs600 testing , the overall frequency of hrddr mutations detected was 17.4% , and the most commonly mutated lineages were endometrial ( 34.4% ; n = 1 , 475 ) , biliary tract ( 28.9% ; n = 343 ) , bladder ( 23.9% ; n = 201 ) , hepatocellular ( 20.9% ; n = 115 ) , gastroesophageal ( 20.8% ; n = 619 ) , and ovarian ( 20.0% ; n = 2 , 489 )  . 
germline mutations in one or both of these genes place patients at heightened risk for development of breast , 1 - 6 ovarian , 1 - 6 prostate , 7 - 9 melanoma , 7 , 10 and pancreatic cancers7 , 10 - 12 during their lifetime . 
it has become apparent that brca interacts with a number of other dna repair proteins to form a complex system for ddr , including atm , rad51 , palb2 , mre11 , rad50 , nbn , and the fanconi anemia proteins.13 , 14 recent evidence suggests mutations in palb2 , atm , and the genes responsible for the mrn complex , rad50 , mre11 , and nbn , play a role in hereditary cancers.15 , 16 for example , palb2 mutation carriers have a lifetime risk of breast cancer development of approximately 50% , 17 , 18 and atm mutation carriers are at higher risk for development of breast , 19 , 20 pancreatic , 21 , 22 and prostate cancers.23 , 24 arielle l . 
in germline brca1 / 2 mutation carriers , exposure to platinum chemotherapy led to improved objective response rates in advanced triple - negative breast cancer versus taxanes ( 68% v 33% ) , 25 and overall survival in pancreatic cancer versus other nonplatinum chemotherapy ( 22 months v 9 months ) .26 mychoice hr - ddr deficiency ( hrd ) score - high triple - negative breast cancer responded better to platinum - based neoadjuvant therapy , with pathologic complete response ( cr ) rates of 27.5% versus 0% in the hr - ddrproficient cohort.27 the mychoice hrd score is frequently used to identify patients with hrd . 
it is a proprietary diagnostic test to assess a hrd phenotype , including an evaluation of loss of heterozygosity , telomeric allelic imbalance , and large - scale state transitions . on exposure to another class of dna - damaging agents , poly - adp ribose polymerase ( parp ) inhibitors , patients with germline or somatic deleterious mutations in the hr - ddr pathway have also achieved favorable responses . 
in this study , three patients had germline brca2 mutations , three patients had germline atm mutations , and the remaining responders had tumor expression of a deleterious mutation ( including palb2 , brca2 , brca1 , chek2 , fanca , and atm ) .35 all germline mutation carriers except for one patient with atm mutation responded to therapy . despite the exciting therapeutic potential of dna - damaging agents in patients with broader evidence of hrd , the prevalence of hrd among all tumors is largely unknown . 
the aim of our study was to determine the prevalence of hr - ddr pathogenic or presumed pathogenic mutations detected on tumor next - generation sequencing ( ngs ) testing across multiple cancer lineages , using commercially available dna sequencing ( ngs or sanger sequencing panel testing , multiplatform profiling ; caris life sciences [ caris ] , irving , tx ) to better define the proportion of patients who may benefit from such therapy . methods study design approval for this study was obtained from the georgetown university institutional review board . 
we defined hrd on tumor ngs testing as a mutation in the following genes , each of which has some activity within the hr - ddr pathway36 - 45 and has been included previously in hr - ddr biomarker clinical trials : arid1a , atm , atrx , bap1 , bard1 , blm , brca1 / 2 , brip1 , chek1 / 2 , fanca / c / d2 / e / f / g / l , mre11a , nbn , palb2 , rad50 , rad51 , rad51b , or wrn . 
frequencies of each mutation were determined for the total cohort , as well as for each cancer lineage ( biliary tract , bladder , breast , cervix , colorectal [ crc ] , endometrial , gastro esophageal [ ge ] , gastrointestinal stromal [ gist ] , glioma , head and neck , hepatocellular [ hcc ] , melanoma , neuroendocrine / small cell lung , nonsmall - cell lung [ nsclc ] , ovarian , pancreas , prostate , renal , sarcoma , thyroid , and unknown primary )  . ngs testing platforms hr - ddr mutation analysis from solid tumor biopsy specimens was determined by ngs at caris , a clinical laboratory improvement amendmentscertified laboratory . 
while 17 , 566 tumors were sequenced with ngs600 , 34 , 860 tumors underwent hotspot illumina miseq platform testing ( illumina truseq amplicon cancer hotspot panel , evaluating 47 genes including the hr - ddr genes atm , brca1 , and brca2 ; illumina , san diego , ca )  . 
tumor enrichment was achieved by harvesting targeted tissue by manual microdissection performed on all cases before molecular testing . the pathogenicity of gene variants identified were interpreted by board - certified molecular geneticists and categorized as pathogenic , presumed pathogenic , variant of unknown significance , presumed benign , or benign , according to american college of medical genetics and genomics standards on the basis of the level of evidence of published studies on the identified variants.46 , 47 only pathogenic or presumed pathogenic mutations were considered deleterious ; variants of unknown significance and variants that have not been previously reported in individuals affected by cancer in the literature were excluded . 
 deleterious mutations reported included frameshift mutations , premature stop codons , mutations shown to disrupt natural splicing , as well as point mutations ; deleterious mutations included those that have and have not been reported as causal for hereditary cancers . statistical analysis the proportion of pathogenic or presumed pathogenic mutations identified from all tumor specimens tested for each specific mutation were calculated for the total cohort and for each cancer lineage investigated . 
the total frequency of hr - ddr mutations in the complete cohort and per cancer lineage was calculated by dividing the number of tumors carrying at least one mutation by the total number of tumors tested , to avoid counting tumors carrying more than one hr - ddr mutation multiple times . 
the 95% cis were computed using the pearson - klopper exact method using r ( org / ) , and the graphics were generated by spss statistics , version 24 ( ibm , armonk , ny )  . results we evaluated 52 , 426 solid tumor pathologic specimens that underwent extended ngs for hrd . 
molecular profiling was performed on the primary tumor in 47.9% of cases ( n = 25 , 102 ) , and on a metastatic site of disease in 41.9% ( n = 21 , 956 )  . 
 within the tumor lineages , the frequencies of mutations varied ( tables 2 and 3 ; fig 2 )  . hr gene mutation frequency overall , pathogenic mutations within the homologous recombination pathway were seen in 17.4% of the 17 , 566 tumors tested with ngs600 , and 8.3% of the 52 , 426 solid tumors overall ( including 34 , 860 tumors that were evaluated for atm , brca1 , and brca2 mutations only on the hotspot panel )  . 
 brca1 / 2 mutations were seen predominately in ovarian and breast cancers , though pathogenic brca2 mutations were seen in high frequencies among gi and nonovarian genitourinary malignancies , as well . 
although palb2 mutations were less common overall and appreciated in only 0.6% of tumors tested , a significant proportion of palb2 mutations was found in bladder , breast , and gi malignancies . 
no pathogenic mutations were identified in bard1 , chek1 , fanca / d2 / e / f / g / l , rad51 , or rad51b ( table 4 )  . hr - ddr gene mutations were appreciated in both primary and metastatic lesions , though with different patterns . 
the remaining mutated hr - ddr genes ( blm , brip1 , chek2 , fancc , mre11a , nbn , palb2 , rad50 , and wrn ) had similar frequencies among primary and metastatic tissue evaluations . tumors with multiple hr gene mutations of the 17 , 566 tumors that underwent extended molecular profiling with the ngs600 platform , 362 were found to carry more than one hr - ddr pathway mutation , including 112 endometrial ( 7.6% ; n = 1 , 475 ) , 75 crc ( 3.1% ; n = 2 , 454 ) , 34 ovarian ( 1.4% ; n = 2 , 489 ) , 29 nsclc ( 0.9% ; n = 3 , 245 ) , 23 ge ( 3.7% ; n = 619 ) , 20 breast ( 1.2% ; n = 1 , 625 ) , and 15 biliary tract ( 4.4% ; n = 343 ) tumors . 
total bar height represents the overall frequency of hr - ddr deficient tumors within each lineage ; colored bar length represents the relative mutation frequency of individual genes in each cancer type . 
summary of homologous recombination dna damage repair mutations identified * overall , % ngs600 , % hotspot , % mutation arid1a brca2 brca1 atrx chek2 bap1 palb2 brip1 fancc rad50 mre11a abbreviation : n / a , not applicable . * no mutations identified : bard1 , chek1 , fanca / d2 / e / f / g / l , rad51 , rad51b . in this large - scale study of ngs molecular profiling of solid tumor samples across multiple cancer lineages , we confirmed hrd is common and was observed in 17.4% of the solid tumors evaluated by the ngs600 platform ( spanning 21 cancer lineages )  . 
in a recent evaluation of brca1 / 2 mutational patterns , for example , a model to detect brca1 / 2 deficiency failed to correlate brca1 / 2 mutational patterns with pathogenic mutations in several additional hr - ddr pathway genes , including atm , atr , chek2 , the fanc group of genes , palb2 , pten rad50 , and rad51c.48 the unique genetic signatures across the breadth of hr - ddr pathway genes are not well characterized , and , as such , it is unknown if the lack of a brca - like mutational pattern is associated with altered responses to parp inhibitors and dna - damaging chemotherapy . our reported frequencies of hrd are similar to previously published work , though a range of frequencies is appreciated ( table 5 )  . 
because there is not yet an established way to measure hrd , and previous studies have measured hrd by an hrd assay assessing large - scale transition scores and telomere allelic imbalances , germline mutations , somatic mutations , brca - like genetic signatures , or a combination of these methods , the differences in hrd prevalence may be related to nonuniformity of assessment . 
in addition , significant variation will occur between whole - exome sequencing versus use of hotspot panels , with the identification of hrd more common among studies that used whole - exome sequencing . 
within our study , 17 , 566 tumors ( 33.5% of the total 52 , 426 tumors tested ) underwent sequencing with the targeted whole - exome sequencing platform ngs600 , which evaluated tumors for 592 genes , assuming dna was sufficient . 
consequently , studies including an evaluation for pten mutations are expected to report higher frequencies of hrd . it is also possible frequencies of hrd may differ across studies as a result of differences in patient population . 
patients with tumors harboring hr - ddr pathway mutations may be more sensitive to dna - damaging chemotherapy and therefore less likely to recur after initial treatment of localized disease . 
although the clinical stage of patients included in our analysis at the time of tissue acquisition ( and if tissue was obtained at presentation ) was unknown , it is possible our population was enriched with patients with metastatic disease without hrd who were less likely to respond favorably to frontline treatment and , therefore , recurred . looking forward , classifying tumors as hr - ddr deficient will likely become increasingly important , as we now appreciate that hrd is common and has been associated with improved outcomes in some patients treated with dna - damaging therapies . 
several clinical trials are assessing in part the role of hrd in response to anticancer therapies and outcomes , including treatment with parp inhibitor therapy alone , but also in combinations with chemotherapy , radiation therapy , or immunotherapy to enhance antitumor efficacy . 
in tandem , it will be important to generate a consensus regarding uniform testing to identify appropriate patients for these tailored therapies . there are some limitations of this study to note . 
given the nature of the study , we evaluated patients tumor tissue for the presence of hr - ddr mutations and thus are unable to distinguish whether a given mutation was a somatic or germline mutation . 
we were also unable to assess tumors for epigenetic modifications such as dna methylation , which could also lead to significant and clinically relevant alterations in gene expression affecting functions of the hr pathway.57 , 58 in addition , hrd is defined by currently available literature regarding the suspected pathogenicity of each mutation . 
it is certainly possible that mutations labeled as a variant of unknown significance may prove important in the future , although the majority are reclassified as benign polymorphisms.59 - 61 we also recognize our results are influenced by the overrepresentation of certain cancer lineages , including ovarian ( n = 9 , 630 ) , nsclc ( n = 8 , 119 ) , crc ( n = 6 , 650 ) , breast ( n = 5 , 910 ) , and endometrial ( n = 5 , 540 ) cancers in the caris database . 
baker employment : caris life sciences , roche travel , accommodations , expenses : caris life sciences , roche honoraria : roche , amgen , bayer / onyx , taiho pharmaceutical , caris life sciences , celgene consulting or advisory role : roche , amgen , bayer / onyx , taiho pharmaceutical , caris life sciences , celgene speakers ' bureau : roche , amgen , bayer / onyx , celgene , taiho pharmaceutical research funding : bayer / onyx ( inst ) , roche ( inst ) , pfizer ( inst ) , amgen ( inst ) , boehringer ingelheim ( inst ) , medimmune ( inst ) claudine isaacs honoraria : roche , astrazeneca , pfizer , novartis , syndax , nanostring technologies consulting or advisory role : pfizer , roche , novartis , astrazeneca , medivation , nanostring technologies , syndax speakers ' bureau : genentech , pfizer , astrazeneca research funding : novartis ( inst ) , pfizer ( inst ) , genentech ( inst ) , tesaro patents , royalties , other intellectual property : uptodate , mcgraw hill publishing affiliations arielle l . 
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we show that kit inhibition markedly decreased cell viability in melanoma cell lines with distinct kit mutations ; however , this effect was countered in the presence of hepatocyte growth factor ( hgf ) , the ligand for met . 
a physical examination revealed a raised , erythematous , and well - circumscribed cutaneous lesion on her left great toe , which the patient attributed to trauma that occurred several months earlier . 
staging computed tomography ( ct ) and positron emission tomography scans revealed left inguinal and left external iliac lymphadenopathy ; two soft - tissue densities in the left breast ( one biopsy proven to be melanoma ) ; numerous subcentimeter , hypodense liver lesions ; and multiple subcentimeter , subcutaneous nodules , suggestive of metastatic disease . 
gene mutation analysis of the metastatic melanoma tissue did not reveal mutations in braf or nras . after two cycles of biochemotherapy ( data supplement ) , restaging ct scans revealed overall stable disease and a mixed tumor response in the lymph nodes . 
the patient received whole - brain radiation therapy ( 30 gy in 10 fractions ) , then stereotactic radiosurgery , followed by combination treatment with temozolomide , cisplatin , and vinblastine . subsequent restaging showed new mediastinal lymphadenopathy and lung nodules . 
the patient received two cycles of a carboplatin - paclitaxel regimen before evidence of disease progression in the left inguinal lymph nodes , liver , and bra the patient was then treated with ipilimumab , which had just received us food and drug administration approval for metastatic melanoma , 3 mg / kg for four cycles . 
there was evidence of stable disease response to ipilimumab , with tumor reduction of 30% by immune - related response criteria overall with disease response in the brain , liver , and lymph nodes . 
after 19 months of disease control with ipilimumab treatment , a brain magnetic resonance imaging demonstrated a left frontal operculum metastasis with perilesional edema ( fig 1a , upper panel ) and positron emission tomography / ct junna oba sun - hee kim wei - lien wang mariana p . 
 ( a ) representative brain magnetic resonance images show left frontal operculum metastasis with perilesional edema pretreatment ( top panel ) and the on - treatment combination dasatinib and crizotinib therapy effect ( lower panel )  . 
 ( b ) polymerase chain reactionbased dna sequencing chromatogram showing a kit nucleotide transition ( 2464 a > t ) at codon 822 ( aat to tat ) in exon 17 from the patients acral melanoma metastatic tumor . 
 ( c ) hematoxylin and eosin ( he ) and immunohistochemical staining for total kit and phosphorylated kit ( p936 ) and total met in the patients primary ( upper panel ) and metastatic ( lower panel ) acral melanoma tumors ( original magnification , 20 )  . scanning showed new hypermetabolic activity in the mediastinal lymph nodes , which was verified to be metastatic melanoma by interventional radiology - guided fine - needle aspiration ( data not shown )  . 
kit mutations and copy number alterations in 4q ( kit ) and 11q ( ccnd1 ) for the melanoma cell lines cell line name exon 4q ( kit ) 11q ( ccnd1 ) kit mutation copy number increase aa change l576p w556 - k558 n822y s476i m230 melms 2391 ma - mel - 144 histopathologic examination of the patients primary and metastatic melanoma tumors showed widespread expression of phosphorylated / total kit protein in melanoma cells ( fig 1c )  . 
given the response to combination dasatinib and crizotinib therapy , we also assessed the expression of the met , for which crizotinib has high binding affinity , and observed positive staining in both primary and metastatic tumors , with moderately higher intensity in the metastatic tumor . to better understand the mechanism by which combination therapy resulted in the observed clinical response , we performed a molecular analysis of the melanoma cell line we established from the patients metastatic tumor ( cell line 2391 ) , as well as three other melanoma cell lines shown to have endogenous kit mutations ( namely , melms , ma - mel - 144 , and m230 ) .17 - 19 mutation analysis confirmed the presence of the 2464 a > t nucleotide transition in kit with a resultant n822y amino acid change in the activation loop within 2391 , the patients melanoma cell line ( data supplement )  . 
we verified the presence of each specific kit mutation within each cell line using targeted next - generation dna sequencing ( table 1 ; data supplement ) .20 no braf or nras mutations , or secondary mutations in kit were detected in any of the cell lines . we also determined the global chromosomal copy number alteration status within each kit - mutant melanoma cell line ( fig 2a ; table 1 )  . 
cell lines 2391 and ma - mel - 144 had chromosome 4q copy number elevation , which corresponds with the location of the kit locus , consistent with initial observations that kit mutations co - occur with kit amplifications.1 , 2 three of the four cell lines also had chromosome 11q copy number elevation , which corresponds with the location of the ccnd1 locus , also well described to be amplified in am tumors.21 , 22 thus , the patients cell line 2391 and others in our panel had characteristic genetic features observed in am tumors . to determine the endogenous constitutive activity of each kit mutation , we assessed the total and phosphorylated levels of kit in each melanoma cell line . 
western blot analysis showed phosphorylated kit to be present in all the kit - mutant melanoma cell lines in the presence or absence of serum ( fig 2b ) ; this was not observed in those without a kit mutation ( data supplement )  . 
each of the cell lines showed sensitivity to gene - specific kit knockdown and to multiple tkis that share kit as a target but have many nonoverlapping targets ( eg , dasatinib targets src - family kinases ) , whereas imatinib does not ( data not shown )  . 
cell lines 2391 ( kitn822y ) , melms ( kit556 - 558del ) , and ma - mel - 144 ( kits476i ) show amplification at 11q ( location of ccnd1 allele )  . 
cell viability assay of m230 ( kitl576p ) , melms ( kit556 - 558del ) , 2391 ( kitn822y ) , and ma - mel - 144 ( kits476i ) melanoma cell lines : no treatment , dasatinib ( 50 nm ) , dasatinib plus hgf ( 100 ng / ml ) , dasatinib plus hgf plus crizotinib ( 5 m ) , and crizotinib alone . of met may enhance the effect of single - agent dasatinib in the tumor setting . 
thus , we tested if the presence of hgf , the only known ligand for met , in the extracellular environment can modulate the reduction in cell viability observed with dasatinib treatment ( fig 2c )  . 
analysis of the patients tumor and cell line ( and three other kit - mutant cell lines ) suggests that the hgf - met axis may be a mechanism of de novo resistance in kit - mutant melanomas . the emergence of secondary mutations in kit is a common mechanism of clinical resistance to kit inhibition in kit - mutant gist.29 however , nearly all resistance observed in kit mutant melanoma occurs in the initial treatment setting , before the clonal evolution of secondary mutations can emerge , 10 - 13 , 23 - 26 suggesting that the presence of coactivating pathways may play a role in this primary resistance . the observed efficacy of the combination dasatinib and crizotinib could , in part , be due to the inhibition of multiple kinases ; however , the melanoma cell line studies indicate the primacy of the kit and met receptors to explain the observed results . 
furthermore , crizotinib alone was only effective in the presence of extracellular hgf , the only known met ligand , indicating crizotinibs modulation of the well - described hgf - met axis , for which it was initially designed.30 these data are consistent with those from preclinical studies showing that met inhibition increases the effect of imatinib in kit - mutant gist models.31 it is intriguing to speculate that the response to combination dasatinib and crizotinib may have been immunologically enhanced , given the patients prior tumor response to ipilimumab therapy . 
hong collection and assembly of data : junna oba , sunhee kim , wei - lien wang , mariana macedo , fernando carapeto , meredith a mckean , john van arnam , agda k . 
woodman manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors junna oba no relationship to disclose sun - hee kim no relationship to disclose wei - lien wang no relationship to disclose mariana p . 
haydu no relationship to disclose honoraria : novartis , bristol - myers squibb , janssen oncology , roche consulting or advisory role : novartis , illumina , ge healthcare research funding : medimmune , astrazeneca , roche , novartis patents , royalties , other intellectual property : elsevier travel , accommodations , expenses : bristol - myers squibb , novartis elizabeth a . 
hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack , bayer consulting or advisory role : baxter , bayer , guidepoint global , janssen research funding : novartis , genentech , eisai , astrazeneca , pfizer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer , bristol - myers squibb , genmab , ignyta , infinity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo , medimmune , molecular templates , takeda travel , accommodations , expenses : loxo , mirna therapeutics other relationship : oncorena chantale bernatchez stock and other ownership interests : lexicon ( i ) research funding : nektar , idera , iovance biotherapeutics , medimmune , pfizer , emd serono patents , royalties , other intellectual property : patent pending on btla as a marker for better cd8 t cells for adoptive immunotherapy alexander j . 
woodman no relationship to disclose acknowledgment leadership : beta cat pharmaceuticals , archer biosciences stock and other ownership interests : archer biosciences , beta cat pharmaceuticals we thank the center for environmental and molecular carcinogenesis anderson cancer center , smithville , tx , for antibody optimization . affiliations junna oba , sun - hee kim , wei - lien wang , mariana p . 
macedo , ac camargo cancer center , so paulo , brazil . supported by the university of texas system rising star award , national cancer institute ( nci ) specialized programs of research excellence ( spore ) in melanoma ( p50 ca093459 to d.s.h. ) ; developmental research project award , national institutes of health / nci cancer center support grant no . 
torres - cabala ca , wang wl , trent j , et al : correlation between kit expression and kit mutation in melanoma : a study of 173 cases with emphasis on the acral - lentiginous / mucosal type . 
demetri gd , van oosterom at , garrett cr , et al : efficacy and safety of sunitinib in patients with advanced gastrointestinal stromal tumour after failure of imatinib : a randomised controlled trial . 
woodman se , trent jc , stemke - hale k , et al : activity of dasatinib against l576p kit mutant melanoma : molecular , cellular , and clinical correlates . 
yang y , liu c , peng w , et al : antitumor t - cell responses contribute to the effects of dasatinib on c - kit mutant murine mastocytoma and are potentiated by anti - ox40 . 
hodi fs , corless cl , giobbie - hurder a , et al : imatinib for melanomas harboring mutationally activated or amplified kit arising on mucosal , acral , and chronically sun - damaged skj clin oncol 31 : 3182 - 3190 , 2013 11 . 
guo j , si l , kong y , et al : phase ii , open - label , single - arm trial of imatinib mesylate in patients with metastatic melanoma harboring c - kit mutation or amplification . 
schittenhelm mm , shiraga s , schroeder a , et al : dasatinib ( bms - 354825 ) , a dual src / abl kinase inhibitor , inhibits the kinase activity of wild - type , juxtamembrane , and activation loop mutant kit isoforms associated with human malignancies . 
kato s , jardim dl , johnson fm , et al : phase i study of the combination of crizotinib ( as a met inhibitor ) and dasatinib ( as a c - src inhibitor ) in patients with advanced cancer . 
todd jr , scurr ll , becker tm , et al : the mapk pathway functions as a redundant survival signal that reinforces the pi3k cascade in c - kit mutant melanoma . 
lee sj , kim tm , kim yj , et al : phase ii trial of nilotinib in patients with metastatic malignant melanoma harboring kit gene aberration : a multicenter trial of korean cancer study group ( un10 - 06 )  . 
kalinsky k , lee s , rubin km , et al : a phase 2 trial of dasatinib in patients with locally advanced or stage iv mucosal , acral , or vulvovaginal melanoma : a trial of the ecog - acrin cancer research group ( e2607 )  . 
 multimodal approach to outcome prediction in metastatic castration - resistant prostate cancer by integrating functional imaging and plasma dna analysis vincenza conteduca , md , phd1 ; emanuela scarpi , phd1 ; federica matteucci , md1 ; paola caroli , md1 ; giorgia ravaglia , msc1 ; lorenzo fantini , md1 ; giorgia gurioli , msc1 ; giuseppe schepisi , md1 ; daniel wetterskog , phd2 ; cecilia menna , md , phd1 ; salvatore luca burgio , md1 ; cristian lolli , md1 ; giovanni paganelli , md1 ; gerhardt attard , md , phd2 ; and ugo de giorgi , md1 purpose biomarkers for treatment personalization in metastatic castration - resistant prostate cancer ( mcrpc ) could help improve patient outcomes . 
multiple tests on blood have reported associations with poorer outcome , including serum lactate dehydrogenase ( ldh ) , chromogranin a ( cga ) , neutrophil : lymphocyte ratio ( nlr ) , and , recently , copy number ( cn ) of androgen receptor ( ar ) in plasma dna . 
fchpet / ct scan was performed at baseline , and maximum standardized uptake value ( suvmax ) , total lesion activity ( tla ) , and metabolic tumor volume ( mtv ) were calculated . 
kaplan - meier curves showed signicantly worse progressionfree survival and overall survival in patients with plasma ar gain and higher suvmax , tla , and mtv values ( p , .001 in each prognostic group )  . 
it is now widely accepted that the majority of crpcs are still dependent on the androgen receptor ( ar ) signaling pathway , 4 , 5 and new ar pathway inhibitors such as enzalutamide and abiraterone have shown efcacy against crpc.6 - 9 biomarkers for personalizing treatment in metastatic crpc ( mcrpc ) could improve patient outcomes . 
multiple tests have revealed associations with a poorer outcome , including serum lactate dehydrogenase ( ldh ) , 10 visceral metastasis ( especially liver involvement10 - 12 ) , chromogranin a ( cga ) , 13 , 14 and neutrophil : lymphocyte ratio ( nlr ) .15 , 16 during the past few years , the potential for plasma dna analysis to improve clinical practice has substantially increased , with real - time molecular characterization that permits patient stratication and thus facilitates treatment decision making . 
 conteduca et al context key objective in the context of multiple biomarkers strategy , we assessed the role of plasma dna analysis in combination with functional imaging and other routinely obtained circulating biomarkers to perform a better prognostication of metastatic castrationresistant prostate cancer ( mcrpc ) in patients . knowledge generated androgen receptor copy number detected in plasma , choline - positron emission tomography parameters , and other clinical factors can be considered as independent predictors of overall survival . 
our nal parsimonious prognostic model from the multivariable analysis of overall survival permitted classication of patients with mcrpc into three risk groups according to the independent prognostic role of these biomarkers . relevance our results suggested the potential usefulness of integrating functional imaging with plasma dna analysis and other noninvasive biomarkers as a tool to improve treatment selection for patients with mcrpc . is now acknowledged as a therapy - guiding predictive and prognostic biomarker.17 - 21 , 22 furthermore , recent biologic data suggest an association between choline uptake and ar copy number ( cn ) .23 increased ar protein expression and / or signaling has been indirectly related to the upregulation of choline kinase alpha ( chka ) , which can bind directly to the ar ligandbinding domachka could be considered a sort of chaperone for ar , resulting in the ubiquitination and transcription and displayactivation of ar - dependent ing different functions involved in tumor growth and progression.23 the overexpression of chka protein in multiple tumors , including prostate cancer , leads to an increased uptake of choline and provides the rationale for using 18f - uorocholine positron emission tomography / computed tomography ( fch - pet / ct ) in this patient setting . 
in addition , early fch - pet / ct has been associated the decline in with clinical outcome , prostate - specic antigen ( psa ) in patients with mcrpc treated with abiraterone or enzalutamide.24 , 25 independently of our aim was to integrate functional imaging , represented as choline uptake in fch - pet / ct , with plasma ar status , clinical data , and other routinely obtained circulating biomarkers and to evaluate their association with outcome . 
twenty - six ( 24.8% ) were chemotherapy naive and 79 ( 75.2% ) had previously undergone chemotherapy . all had a histologically conrmed diagnosis of prostate adenocarcinoma treated with abiraterone or enzalutamide in preor postchemotherapy settings . 
the study included patients participating in a protocol approved by the institutional review board of istituto scientico romagnolo per lo studio e la cura dei tumori ( irst ) irccs , meldola , italy ( rec 2192 / 2013 )  . patients were treated with abiraterone 1 , 000 mg plus prednisone 5 mg twice per day or enzalutamide 160 mg alone once per day . 
in addition , serum ldh , alkaline phosphatase , complete blood count ( used to determine nlr ) , and serum cga were also measured within 1 week of starting therapy . 
in this study , fch - pet / ct was performed after 12 6 4 weeks of treatment . peripheral blood samples were collected from each patient at baseline and at the rst radiologic evaluation . 
total extracted plasma dna was quantied using the quant - it high sensitivity picogreen doublestranded dna assay kit ( invitrogen ) or by spectrophotometric evaluation ( nanodrop nd - 1000 ; celbio , milan , italy )  . 
semiquantitative criteria based on the maximum standardized uptake value ( suvmax ) and the target : background ratio were used to aid the visual analysis.26 the metabolic tumor volume ( mtv ) was calculated as the sum of each 3 - dimensional volume of interest . 
mtv is a purely volumetric entity , whereas tla also takes into account the metabolic activity of the lesion leading to an estimate of tumor activity ( data supplement )  . statistical analysis data were summarized by frequency for categorical variables and by cutoff using receiver operating characteristic ( roc ) curves and median and range for continuous variables . 
a comparison between baseline imaging and clinical , laboratory , and molecular features in patients with or without ar gain was performed using the median test ( wilcoxon )  . 
roc curve analysis was performed to estimate the best cutoff value of fch - pet / ct parameters ( tla , mtv , and suvmax ) and serum cga level considered as continuous variables . progression - free survival ( pfs ) was measured as the time between the rst day of abiraterone or enzalutamide treatment and the date of disease progression or death ( whichever came rst ) or last tumor evaluation . 
statistical analyses were performed with sas 9.4 software ( sas institute , cary , nc )  . a weibull multiple regression model was adopted to evaluate the combined impact of molecular , laboratory , and imaging features on survival . 
 ( c ) linear regression ( diagonal line ) between maximum standardized uptake value ( suvmax ) , total lesion activity ( tla ) , and metabolic tumor volume ( mtv )  . 
a box plot is shown with the thick horizontal line depicting the median value of suvmax , tla , and mtv in overall , pre - , and postchemotherapy patients . 
a , ar copy number amplied ; cga , chromogranin a ; cht , chemotherapy , ldh , lactate dehydrogenase ; n , ar copy number normal ; nci , nanocurie ; nlr , neutrophil : lymphocyte ratio . ability of functional imaging and plasma ar status to predict clinical outcomes at the time of the analysis , 90 ( 85.7% ) of the overall 105 patients ( 15 [ 57.7% ] of 26 before chemotherapy and 75 [ 92.4% ] of 79 patients after chemotherapy ) had progressive disease and 82 patients ( 78.1% ) had died ( 11 [ 42.3% ] before chemotherapy and 71 [ 88.6% ] after chemotherapy )  . 
chemotherapytreated patients were divided into four prognostic groups according to baseline ar status and tla , mtv , and suvmax values : ar normal , tla , mtv , and suvmax low ; ar gain , tla , mtv , and suvmax low ; ar normal , tla , mtv , and suvmax high ; and ar gain , tla , mtv , and suvmax high . they were characterized by a signicant difference in pfs ( p , .001 for tla , p = .003 for mtv , and p , .001 for suvmax ) and os ( p , .001 for tla , p , .001 for mtv , and p , .001 for suvmax ; data supplement )  . identication of imaging , molecular , and clinical features as independent predictors of treatment outcome we performed univariable and multivariable cox proportional hazards regression analysis of os to evaluate the prognostic impact of different factors . 
it is possible that the strong correlation among all pet / ct parameters abrogated the statistical signicance of tla and mtv in this analysis . coefcient by the smallest one as described in statistical analysis . 
the choice of time and number of groups with different prognoses was made in terms of clinical consideration , such as time at 15 months ( group i , 15 months : os was greater than 70% ; group ii , 15 months : os was 30% to 70% ; group iii , 15 months : os was less than 30% )  . 
in the training set , 27 patients ( 39.1% ) were attributed to risk group i , 13 ( 18.8% ) to risk group ii , and 29 ( 42.0% ) to risk group iii . the survival experience of the three patient groups was identied by the score . 
the larger two - thirds group of patients was used as a training set to construct the score , and the remaining one third was used as a validation set . table 2 shows the partial score value for each category , which was obtained by subdividing each regression this study examined the feasibility of using functional imaging to assess tumor burden and also to evaluate its predictive and prognostic role in crpc treated with abiraterone or enzalutamide . 
progression - free survival ( pfs ) and overall survival ( os ) according to copy number ( cn ) of androgen receptor ( ar ) and functional imaging in overall population of patients with castration - resistant prostate cancer who were treated with abiraterone or enzalutamide . 
of events median os ( months ) 95% ci 95% ci , 112 112 suvmax , 50 50 , 12 12 total lesion activity , 563 , 979 563 , 979 median no . 
kaplan - meier curves for overall survival ( os ) and relative survival ( months ) by risk group in the training set ( a ) and validation set ( b )  . 
in both treatment groups , survival experience of the three groups of patients was identied by the score . however , the identication of biomarkers could facilitate personalized next - line systemic therapy in a more accurately selected population . 
during the past decade , molecular stratication from tissue biopsy has provided several therapeutic targets and prognostic markers , but numerous factors can limit the usefulness of tissue biomarkers ( from both primary and secondary tumors )  . 
this clone may not necessarily be from the largest lesion or the lesion with the highest gleason grade , as conrmed by the lack of signicance of the gleason score with clinical outcome in our univariable analysis . 
moreover , a polyclonal metastasis - to - metastasis seeding may occur during disease progression.27 given the complex tumor heterogeneity , assessment of the archival primary tumor or metastatic biopsies for the clinical management of patients with crpc may not be adequate for or entirely representative of current tumor status . 
 a functional imaging and plasma dna analysis in crpc baseline ar normal ; dsdna 27 ng / ml re - evaluation ar normal ; dsdna 11 ng / ml baseline ar normal ; dsdna 51 ng / ml re - evaluation ar normal ; dsdna 31 ng / ml baseline ar normal ; dsdna 122 ng / ml re - evaluation ar normal ; dsdna 136 ng / ml baseline ar normal ; dsdna 69 ng / ml re - evaluation ar normal ; dsdna146 ng / ml fig 4 . 
impact of baseline androgen receptor ( ar ) copy number , cell - free dna , and choline uptake by 18f - uorocholine positron emission tomography / computed tomography on clinical outcome in patients with castration - resistant prostate cancer who were treated with abiraterone or enzalutamide . 
 ( a ) patient 1 ; 78 years of age ; gleason score 9 ( 4 + 5 ) ; 10 sites of nodal localization ; baseline ar normal ; tla = 290576.3 , mtv = 50.26 ; suvmax = 68.52 : treatment with abiraterone postdocetaxel for 7 months . 
 ( b ) patient 2 ; 80 years of age ; gleason score 7 ( 3 + 4 ) ; four sites of nodal localization ; baseline ar gain ; tla = 23745.7 ; mtv = 14.67 ; suvmax = 12.97 ; treatment with abiraterone postdocetaxel for 30 months . 
 ( c ) patient 3 ; 85 years of age ; gleason score 8 ( 4 + 4 ) ; 26 sites of bone localization ; baseline ar normal ; tla = 1292423.8 ; mtv = 279.85 ; suvmax = 206.49 ; treatment with abiraterone postdocetaxel for 12 months . 
 ( d ) patient 4 ; 87 years of age ; gleason score 8 ( 4 + 4 ) ; 10 sites of bone localization ; baseline ar gain ; tla = 599060 ; mtv = 142 ; suvmax = 49.25 ; treatment with enzalutamide postdocetaxel for 5 months . 
re - evaluation after 40 days of therapy : progressive disease . addition , this study was a retrospective single - center work . additional limitations are the small sample size , especially in the prechemotherapy group , and the presence of pet / ct indices as nonabsolute measures , which can be affected by technical issues such as pet scanner calibration , imaging reconstruction , image acquisition , and timing of tracer administration . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . cristian lolli travel , accommodations , expenses : janssen oncology gerhardt attard honoraria : janssen , astellas pharma , janssen ( i ) consulting or advisory role : janssen - cilag , veridex , ventana medical systems , astellas pharma , medivation , novartis , millennium pharmaceuticals , abbott laboratories , essa , bayer , pzer speakers ' bureau : janssen , astellas pharma , takeda , sano , ventana medical systems research funding : janssen ( inst ) , arno therapeutics ( inst ) , innocrin pharma ( inst ) patents , royalties , other intellectual property : i am on the icr rewards to inventors list for abiraterone acetate . travel , accommodations , expenses : janssen , astellas pharma , medivation , ventana medical systems , abbott laboratories , bayer , essa , janssen ( i ) , astellas pharma ( i ) , pzer other relationship : institute of cancer research ugo de giorgi consulting or advisory role : pzer , janssen , astellas pharma , sano , bristol - myers squibb , bayer , ipsen , merck , research funding : sano ( inst ) , astrazeneca ( inst ) , roche ( inst ) travel , accommodations , expenses : bristol - myers squibb , ipsen , janssen , pzer no other potential conicts of interest were reported . acknowledgment we thank gr ainne tierney for editorial assistance . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
ca cancer j clin 68 : 7 - 30 , 2018 ferlay j , soerjomataram i , dikshit r , et al : cancer incidence and mortality worldwide : sources , methods and major patterns in globocan 2012 . 
int j cancer 136 : e359 - e386 , 2015 gillessen s , omlin a , attard g , et al : management of patients with advanced prostate cancer : recommendations of the st gallen advanced prostate cancer consensus conference ( apccc ) 2015 . 
ann oncol 26 : 1589 - 1604 , 2015 kobayashi t , inoue t , kamba t , et al : experimental evidence of persistent androgen - receptor - dependency in castration - resistant prostate cancer . 
n engl j med 371 : 424 - 433 , 2014 scher hi , fizazi k , saad f , et al : increased survival with enzalutamide in prostate cancer after chemotherapy . 
n engl j med 367 : 1187 - 1197 , 2012 de bono js , logothetis cj , molina a , et al : abiraterone and increased survival in metastatic prostate cancer . 
n engl j med 364 : 1995 - 2005 , 2011 ryan cj , smith mr , de bono js , et al : abiraterone in metastatic prostate cancer without previous chemotherapy . 
chi kn , kheoh t , ryan cj , et al : a prognostic index model for predicting overall survival in patients with metastatic castration - resistant prostate cancer treated with abiraterone acetate after docetaxel . 
halabi s , lin cy , kelly wk , et al : updated prognostic model for predicting overall survival in rst - line chemotherapy for patients with metastatic castrationresistant prostate cancer . 
conteduca v , caffo o , fratino l , et al : impact of visceral metastases on outcome to abiraterone after docetaxel in castration - resistant prostate cancer patients . future oncol 11 : 2881 - 2891 , 2015 74 : 1691 - 1696 , 2014 21 : 487 - 493 , 2014 13 . 
conteduca v , crabb sj , jones rj , et al : persistent neutrophil to lymphocyte ratio .3 during treatment with enzalutamide and clinical outcome in patients with castration - resistant prostate cancer . 
salvi s , casadio v , conteduca v , et al : circulating cell - free ar and cyp17a1 copy number variations may associate with outcome of metastatic castrationresistant prostate cancer patients treated with abiraterone . 
salvi s , casadio v , conteduca v , et al : circulating ar copy number and outcome to enzalutamide in docetaxel - treated metastatic castration - resistant prostate cancer . 
conteduca v , wetterskog d , sharabiani mta , et al : androgen receptor gene status in plasma dna associates with worse outcome on enzalutamide or abiraterone for castration - resistant prostate cancer : a multi - institution correlative biomarker study . 
conteduca v , scarpi e , caroli p , et al : circulating androgen receptor combined with 18f - uorocholine pet / ct metabolic activity and outcome to androgen receptor signalling - directed therapies in castration - resistant prostate cancer . 
de giorgi u , caroli p , burgio sl , et al : early outcome prediction on 18f - uorocholine pet / ct in metastatic castration - resistant prostate cancer patients treated with abiraterone . 
de giorgi u , caroli p , scarpi e , et al : erratum to : ( 18 ) f - fluorocholine pet / ct for early response assessment in patients with metastatic castration - resistant prostate cancer treated with enzalutamide . 
mawlawi o , podoloff da , kohlmyer s , et al : performance characteristics of a newly developed pet / ct scanner using nema standards in 2d and 3d modes . j nucl med 45 : 1734 - 1742 , 2004 27 . 
conteduca v , caffo o , lolli c , et al : long - term clinical impact of psa surge in castration - resistant prostate cancer patients treated with abiraterone . 
science 355 : 84 - 88 , jahr s , hentze h , englisch s , et al : dna fragments in the blood plasma of cancer patients : quantitations and evidence for their origin from apoptotic and necrotic cells . 
khan k , rata m , cunningham d , et al : functional imaging and circulating biomarkers of response to regorafenib in treatment - refractory metastatic colorectal cancer patients in a prospective phase ii study . 
 cdkn2c - null leiomyosarcoma : a novel , genomically distinct class of tp53 / rb1wild - type tumor with frequent cic genomic alterations and 1p / 19q - codeletion erik a . 
here , we searched for recurrent actionable genomic alterations in lms that occur in the absence of common untreatable oncogenic drivers . methods tissues from 276 , 645 unique advanced cancers , including 2 , 570 uterine and soft tissue lms , were sequenced by hybrid - capturebased next - generation dna and rna sequencing / comprehensive genomic proling of up to 406 genes . 
we further validated our ndings in two publicly available datasets : the cancer genome atlas and the project genie initiative . conclusion cdkn2c - null lms denes a genomically distinct tumor that may have prognostic and / or therapeutic clinical implications , including possible use of specic cyclin - dependent kinase inhibitors . jco precis oncol 4 : 955 - 971 . 
 williams et al context key objective leiomyosarcoma ( lms ) , an aggressive tumor with limited curative options , shows frequent mutations in tp53 and rb1 but few actionable genomic alterations . 
here , we searched for recurrent actionable genetic alterations in lms . knowledge generated a novel , genomically distinct class of lms ( 3.0% ; 77 of 2 , 570 cases ) harbor homozygous loss of cdkn2c , which encodes the cyclin - dependent kinase inhibitor - 2c . 
cdkn2c - null lms lack typical tp53 and rb1 mutations ; show concurrent homozygous deletion of cic , cdkn2a , and rad51b ; and show frequent 1p / 19q - codeletion . relevance the nding of recurrent cdkn2c - null lms provides insight into tumor biology and raises the possibility for use of specic cyclin - dependent kinase inhibitors in this aggressive disease . from the uterus , with signicantly low frequency of tp53 and rb1 gas . methods cohort and genomic analyses comprehensive genomic proling was performed in a clinical laboratory improvement amendmentscertied , college of american pathologistsaccredited laboratory ( foundation medicine , cambridge , ma )  . 
20% estimated percent tumor nuclei in each case , for which the percent tumor nuclei equals 100 times the number of tumor cells divided by total number of nucleated cells . 
the samples were assayed by adaptor ligation hybrid capture , performed for all coding exons of 236 ( v1 ) , 315 ( v2 ) , or 405 ( v3 ) cancer - related genes plus select introns from 19 ( v1 ) , 28 ( v2 ) , or 31 ( v3 ) genes frequently rearranged in cancer ( appendix table a1 ) .11 , 12 for samples with available rna , targeted rna sequencing was performed for rearrangement analysis in 265 genes.12 sequencing of captured libraries was performed using the illumina hiseq 4000 system ( illumina , san diego , ca ) to a mean exon coverage depth of targeted regions of  . 500 , and sequences were analyzed for gas , including short variant alterations ( base substitutions , insertions , and deletions ) , copy number alterations ( focal amplications and homozygous deletions ) , and select gene fusions or rearrangements.11 , 13 , 14 to maximize mutation detection accuracy ( sensitivity and specicity ) in impure clinical specimens , the test was previously optimized and validated to detect base substitutions at a 5% mutant allele frequency , indels with a 10% mutant allele frequency with 99% accuracy , and fusions occurring within baited introns / exons with  . 
6 - 8 copies depending on tumor ploidy and homozygous deletions was performed as previously described.11 in brief , the aligned dna sequences of each tumor specimen were normalized against a process - matched normal , producing log - ratio and minor allele frequency data . 
a gibbs sampler tted copy number model and a grid - based model were tted to the segmented log - ratio and minor allele frequency data , producing genome - wide copy number estimates . 
finally , the degrees - of - t of candidate models returned by gibbs sampling and grid sampling were compared , and the optimal model was selected by an automated heuristic . signal - to - noise ratios for each genomic segment were used to determine gain or loss per chromosome arm on the basis of tumor purity and ploidy ; the sum of segment sizes determined the fraction of each arm gained or lost . chromosomes were assessed for arm - level aneuploidy , dened as positive if  . 
the cohort of cdkn2c - null lms comprised 77 cases , each from a different patient , that were submitted to foundation medicine for comprehensive genomic proling during routine clinical care . 
human investigations were performed after approval by a local human investigations committee and in accordance with an assurance led with and approved by the department of health and human services , when appropriate . 
clinicopathologic data , including patient age , sex , tumor site , and figo stage or ajcc ( 8th edition ) stage , were extracted from the accompanying pathology report.4 , 16 primary site data were not available for a subset of patient cases ( indeterminant primary )  . 
these patients were signicantly older than the remainder of the lms cohort ( median age , 61 v 57 years ; p = .0009 , mann - whitney u test )  . 
patients were enriched for female sex compared with the remainder of the lms cohort ( 99% [ 76 of 77 ] v 79% [ 1 , 968 of 2 , 493 ] ; p , .0001 , fishers exact test )  . 
six female patients had a prior history of leiomyomatosis ( n = 2 ) or uterine smooth muscle tumor of uncertain malignant potential ( stump ; n = 4 )  . 
the majority of cdkn2c - null lms patients showed clinically advanced / metastatic disease , with 62% of conrmed uterine primary occurrences documented at figo stage iv ( n = 34 of 55 ) and 86% of indeterminant or soft tissue primary cases documented at ajcc stage iv ( n = 19 / 22 ) , as summarized indeterminant figo staging ( uterine primary ) no . 
locations of the sequenced tumor specimens are summarized in appendix table a2 . comprehensive genomic proling of cdkn2c - null lms the distribution of gas in the 77 cdkn2c - null lms is displayed in figure 1 . 
the frequent gas were identied in cic at 19q13.2 , most cdkn2a , and rad51b ( table 2 ) , and unsupervised analysis showed signicant enrichment of these alterations in the cdkn2c - null cohort ( appendix fig a1 )  . 
no other signicant differences based on age were identied . comparison of patient cases on the basis of clinical stage , three patients had two separate tissue specimens analyzed ( appendix table a4 )  . 
additional recurrent chromosomal arm - level changes were identied in the 72 patient cases available , including most frequently aneuploidy of chromosomes 6p ( n = 35 ) , 9p ( n = 19 ) , 10q ( n = 28 ) , 11p ( n = 39 ) , 13q ( n = 46 ) , 14q ( n = 46 ) , and 16q ( n = 52 )  . a review of 1p / 19q - codeletion status in available lms patient cases without homozygous deletion of cdkn2c ( n = 1 , 212 ) revealed 62 1p / 19q - codeleted lms ( 5% ; fig 2c )  . 
all four occurred in uterine lms ( one of which with a history of stump )  . all non - lms sarcoma patient cases in the foundation medicine dataset ( n = 12 , 097 ) were evaluated for cdkn2c status . 
these included diverse sarcoma diagnoses , including six high - grade sarcomas not otherwise specied , two osteosarcomas , two malignant peripheral nerve sheath tumors , and two inammatory myobroblastic tumors . 
both were alk rearrangementpositive tumors in women ( ages , 63 and 72 years )  . we also searched our entire lms cohort ( n = 2 , 570 ) for cases with pathogenic alterations in cdkn2c other than homozygous deletion . 
 ( a ) cdkn2c - null lms with a truncating variant in cic ( p.q907 * ) and homozygous deletion of cdkn2a at chromosome 9p21.3 ( red arrow )  . 
 ( c ) cdkn2c - retained lms with deep deletion of rb1 at chromosome 13q14.2 ( red arrow ) and a cn plot of high complexity . and rad51b were identied ; 1p / 19q status was not available . histopathology histopathologic evaluation was performed on all available high - resolution digital pathology h&e slides of our cohort of cdkn2c - null lms ( n = 70 )  . 
histopathology of cdkn2c - null leiomyosarcoma ranged from ( a , b ) epithelioid to ( c ) spindled ( hematoxylin & eosin [ h&e ] stains , 200 )  . 
 ( d ) occasional cases showed focal myxoid histology ( h&e stain , 200 )  . progesterone receptor ( 24 of 26 ; remaining two with focal positivity )  . 
cdkn2c - null lms were also positive for desmin ( 30 of 33 ; remaining three with focal positivity ) , smooth muscle actin ( 25 of 25 ) , muscle - specic actin ( 11 of 11 ) , and caldesmon ( 6 of 6 )  . 
patient cases showed frequent homozygous loss of cic ( n = 5 [ 42% ] of 12 ) , cdkn2a ( n = 4 [ 33% ] of 12 ) , and rad51b ( n = 3 [ 25% ] of 12 ) , and all were wild type for tp53 , rb1 , and atrx ( n = 12 of 12 )  . discussion in 2 , 570 patient cases of lms , cdkn2c - null lms ( n = 77 ; 3.0% ) comprised a genomically distinct molecular subgroup . cdkn2c - null lms typically lacked mutations in tp53 , rb1 , and atrx but showed frequent 1p / 19q - codeletion ( 81% ) , and nearly half ( 40.3% ) showed homozygous deletion or inactivating truncations of cic . 
 cdkn2c loss denes class of tp53 / rb1wild - type leiomyosarcoma which enhances fas - mediated apoptosis , and its loss may contribute to tumor pathogenesis.29 the cic gene on chromosome 19q13.2 represses genes induced downstream to rtk pathway activation.30 in the absence of rtk signaling , cic blocks transcription of genes that have diverse effects on cellular proliferation , metabolism , and migration.31 along with single copy loss of cic on 19q , concurrent inactivating mutations in cic are identied in a high percentage of oligodendrogliomas.32 whole - arm 1p / 19q - codeletion , with concurrent mutation in idh1 or idh2 , is entity - dening for oligodendrogliomas.33 - 35 oligodendrogliomas are associated with relatively long overall survival , and treatment strategies are often stratied on the basis of 1p / 19q status.36 - 38 the codeletion is a result of unbalanced translocation between two chromosomes , with subsequent loss of der ( 1 ; 19 ) ( p10 ; q10 ) , likely because chromosomes 1 and 19 are near each other in the nonrandom organization of the nucleus.39 - 41 a large percentage of oligodendrogliomas also show cic and fubp1 mutations.31 our cohort of cdkn2c - null lms shows notable similarities and differences to oligodendroglioma ; 40% of our cohort showed an inactivating alteration in cic , most commonly homozygous deletion . 
rare sarcoma - like tumors originating from oligodendrogliomas have been reported , with documented idh1 mutation and 1p / 19q - codeletion , and have been termed oligosarcoma.42 - 44 rodriguez et al43 identied 6 of 7 patient cases of oligosarcoma with at least focal smooth muscle actin positivity of the sarcomatous component by immunohistochemistry and one patient case with smooth muscle differentiation by electron microscopy . 
these results indicate a similarity in differentiation to our cohort of lms . among all sarcomas with cdkn2c loss , 1p / 19q - codeletion appears to be nearly exclusive to lms . 
in our overall lms cohort , however , occasional cdkn2c - retained lms showed tp53 and rb1 alterations and were positive by the 1p / 19qcodeletion detection algorithwe speculate that , given the complexity of these genomically unstable occurrences , occasional cdkn2c - retained lms satisfy these criteria ( fig 2c )  . as such , identication of homozygous deletion of cdkn2c may be the most specic distinguishing feature . cytogenetic ndings in lms and leiomyoma have been previously reported , although without characterization of cdkn2c status . 
a greater frequency of 1p loss has been documented in metastasized lms.45 from a cytogenetics study of 800 uterine leiomyomata , nine diploid occurrences with 1p loss were identied , with other associated alterations , particularly chromosome 19 and / or chromosome 22 loss.46 transcriptional proling of two of the 1p - deleted leiomyomas in that study showed alignment with malignant lms in a hierarchical clustering analysis.46 in another study , 1p loss was identied in approximately one quarter of uterine cellular leiomyomata.47 three reports on a total of eight pulmonary - based benign metastasizing leiomyoma reported 19q and 22q terminal deletion in each case.48 - 50 rare uterine leiomyomas with gas in rad51b have also been identied.51 the overlap in gas between our cohort of cdkn2c - null lms and a subset of leiomyoma of uncertain cdkn2c status in the literature suggests a possible connection between these entities . evaluations of gas in epithelioid or myxoid uterine smooth muscle neoplasms are limited in the literature.52 - 56 although a high percentage of cdkn2c - null lms in our study demonstrated epithelioid features on histology , histology was also varied . 
immunohistochemistry results extracted from pathology reports were typical for uterine lms , with expression of characteristic smooth muscle markers.57 given the overall low response rate of lms to standard therapies , the identication of this targetable alteration in cdkn2c may be useful for treatment decisions . 
cdk4 / 6 inhibitors have previously shown effectiveness in a lms with a cdkn2a alteration.10 nearly half of the cdkn2c - null lms harbored loss of cdkn2a ; cdk4 / 6 inhibitors may be effective in replacing the loss of inhibition of cdk4 / 6 that results from cdkn2c and cdkn2a loss in these patient cases that recur after standard chemotherapy regimens . 
a minor subset of cdkn2c - null and / or 1p / 19q - codeleted lms harbored activating fusions in alk , braf , fgfr1 , and ntrk1 , for which targeted inhibitors may be of utility.9 limitations of this study include its retrospective nature and the enrichment for aggressive tumors , mostly metastatic to distant sites . 
the latter may be due to collection bias from submission of specimens later in the disease course . additional studies will be needed to correlate the nding of cdkn2c loss in lms with prognostic data and treatment outcomes . 
williams , md , 150 second st , cambridge , ma 02141 ; twitter : @erikawilliamsm1 ; e - mail : erwilliams@foundationmedicine.com. meagan montesion stock and other ownership interests : roche ethan s . 
hoffmann - la roche radwa sharaf employment : foundation medicine stock and other ownership interests : roche brennan decker stock and other ownership interests : avidea technologies consulting or advisory role : foundation medicine , avidea technologies kevin jon williams stock and other ownership interests : hygieia , gemphire therapeutics consulting or advisory role : gemphire therapeutics research funding : novo nordisk jeffrey m . 
venstrom employment : genentech , foundation medicine leadership : genentech stock and other ownership interests : genentech research funding : genentech , roche , foundation medicine travel , accommodations , expenses : genentech brian m . 
alexander employment : foundation medicine leadership : foundation medicine stock and other ownership interests : roche research funding : eli lilly ( inst ) , puma ( inst ) , celgene ( inst ) ( optional ) open payments link : physician / 854258 / summary jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : celsius therapeutics research funding : foundation medicine lee a . 
elvin employment : foundation medicine no other potential conicts of interest were reported . acknowledgment we thank the american association for cancer research and appreciate its nancial and material support in the development of the american association for cancer research project genie registry , and we thank members of the consortium for their commitment to data sharing . references roberts me , aynardi jt , chu cs : uterine leiomyosarcoma : a review of the literature and update on management options . 
gynecol oncol 151 : 562 - 572 , 2018 seagle bll , sobecki - rausch j , strohl ae , et al : prognosis and treatment of uterine leiomyosarcoma : a national cancer database study . 
moore kn , gunderson c , ramkissoon s , et al : comprehensive genomic proling of uterine leiomyosarcomas identies opportunities for personalized therapies . ann oncol 27 : vi309 , 2016 davis le , nusser kd , przybyl j , et al : discovery and characterization of recurrent , targetable alk fusions in leiomyosarcoma . 
frampton gm , fichtenholtz a , otto ga , et al : development and validation of a clinical cancer genomic proling test based on massively parallel dna seoncologist 22 : 416 - 421 , 2017 quencing . 
trabucco se , gowen k , maund sl , et al : a novel next - generation sequencing approach to detecting microsatellite instability and pan - tumor characterization of 1000 microsatellite instability - high cases in 67 , 000 patient samples . 
sweeney sm , cerami e , baras a , et al : aacr project genie : powering precision medicine through an international consortiucancer discov 7 : 818 - 831 , 2017 19 . 
guan kl , jenkins cw , li y , et al : growth suppression by p18 , a p16ink4 / mts1and p14ink4b / mts2 - related cdk6 inhibitor , correlates with wild - type prb function . 
genes dev 8 : 2939 - 2952 , 1994 jeffrey pd , tong l , pavletich np : structural basis of inhibition of cdk - cyclin complexes by ink4 inhibitors . 
kim kj , park mc , choi sj , et al : determination of three - dimensional structure and residues of the novel tumor suppressor aimp3 / p18 required for the interaction with atm . 
pohl u , cairncross jg , louis dn : homozygous deletions of the cdkn2c / p18ink4c gene on the short arm of chromosome 1 in anaplastic oligodendrogliomas . brain pathol 9 : 639 - 643 , 1999 28 . 
husemann k , wolter m , b uschges r , et al : identication of two distinct deleted regions on the short arm of chromosome 1 and rare mutation of the cdkn2c gene from 1p32 in oligodendroglial tumors . 
cell cycle 8 : 2528 - 2534 , 2009 jim enez g , shvartsman sy , paroush z : the capicua repressor : a general sensor of rtk signaling in development and disease . 
cairncross jg , ueki k , zlatescu mc , et al : specic genetic predictors of chemotherapeutic response and survival in patients with anaplastic oligodenneuropathol 131 : 803 - 820 , 2016 145 : 1175 - 1190 , 1994 j neuropathol exp neurol 54 : 91 - 95 , 1995 drogliomas . 
taal w , van der rijt ccd , dinjens wnm , et al : treatment of large low - grade oligodendroglial tumors with upfront procarbazine , lomustine , and vincristine chemotherapy with long follow - up : a retrospective cohort study with growth kinetics . 
grifn ca , burger p , morsberger l , et al : identication of der ( 1 ; 19 ) ( q10 ; p10 ) in ve oligodendrogliomas suggests mechanism of concurrent 1p and 19q loss . j neuropathol exp neurol 65 : 988 - 994 , 2006 jenkins rb , blair h , ballman k v . , et al : a t ( 1 ; 19 ) ( q10 ; p10 ) mediates the combined deletions of 1p and 19q and predicts a better prognosis of patients with oligodendroglioma . 
mandahl n , fletcher cdm , dal cin p , et al : comparative cytogenetic study of spindle cell and pleomorphic leiomyosarcomas of soft tissues : a report from the 46 . 
christacos nc , quade bj , dal cin p , et al : uterine leiomyomata with deletions of 1p represent a distinct cytogenetic subgroup associated with unusual histologic champ study group . 
bowen jm , cates jm , kash s , et al : genomic imbalances in benign metastasizing leiomyoma : characterization by conventional karyotypic , uorescence in situ hybridization , and whole genome snp array analysis . 
holzmann c , markowski dn , koczan d , et al : genome - wide acquired uniparental disomy as well as chromosomal gains and losses in a uterine epithelioid leiomyoma . 
reyes c , karamurzin y , frizzell n , et al : uterine smooth muscle tumors with features suggesting fumarate hydratase aberration : detailed morphologic analysis and correlation with s - ( 2 - succino ) - cysteine immunohistochemistry . 
 cdkn2c loss denes class of tp53 / rb1wild - type leiomyosarcoma appendix attribute negative not significant positive % frequency cdkn2c faf1 tp53 sex : male atrx chr2p_loss chr1p_loss cdkn2a cdkn2b rad51b sex : female chr19q_loss chr14q_loss log2 odds ratio fig a1 . 
red and blue indicate positive and negative correlation , respectively , in cdkn2c - null leiomyosarcoma ( n = 77 ) compared with the remainder of the leiomyosarcoma cohort ( n = 2 , 493 )  . 
henick , md1 ; matthew ingham , md1 ; maryam shirazi , md2 ; charles marboe , md2 ; andrew turk , md2 ; susan hsiao , md , phd2 ; and mahesh m . 
intervening surveillance scans were unremarkable ; however , the patient experienced a 10 - pound weight loss over 2 months that culminated in acute - onset exertional dyspnea and chest pain , prompting admission . 
the patient was evaluated by cardiothoracic surgery and deemed not to be a surgical candidate . positron emission tomography ( pet ) ct conrmed uorodeoxyglucose avidity in the hypermetabolic mass , scattered left lung nodules , and an intralumina soft tissue mass in the distal colon proximal to the anastomosis as well as a right thyroid lesion ( fig 1 )  . 
restaging ct of the chest after 2 cycles revealed decreasing peripheral opacities in the left upper lobe , a decrease in irregular left - sided lung nodules , and a decrease in the extent of tumor thrombus , with an increase in patency of the left pulmonary artery and interval resolution of cavitation within the tumor thrombus . 
in addition , the vaf of 67% indicated loss of heterozygosity in the tumor , raising the possibility of a germline alteration ( germline testing has not been performed )  . 
because the msi status was indeterminate by ngs , msi testing by polymerase chain reaction ( pcr ) fragment analysis using ve quasimonomorphic mononucleotide repeats ( msi analysis system , version 1.2 ; promega , madison , wi ) was performed but was indeterminate , because normal dna for comparison was unavailable . 
using dna extracted from peripheral blood for comparison , msi with an altered allele at four of ve tested loci ( nr - 21 ; bat - 26 ; bat - 25 ; mono - 27 ; fig 3 ) was detected . 
positron emission tomography / computed tomography results ( a ) at baseline , ( b ) after treatment with doxorubicin plus olaratumab before pembrolizumab administration , and ( c ) after 8 cycles of pembrolizumab . with chemotherapy , the patient was amenable to treatment with pembrolizumab and began therapy . 
after 8 cycles of treatment , intervening pet - ct results have shown an additional decrease in the extravascular component of the pulmonary artery tumor with evolving dystrophic calcication , no evidence of tumor thrombus , stable ndings in the lungs likely consistent with pulmonary infarcts , an avid hypermetabolic right thyroid nodule , and a decrease in soft tissue nodularity at the suture line . discussion intimal sarcoma of the pulmonary artery is a rare tumor ( incidence , approximately 0.001%2 , 3 ) , and the scant existing medical literature highlights individual cases of response to various combinations of surgery , 4 chemotherapy , 5 and radiation.6 the molecular landscape of such tumors is not well characterized . studies of immune checkpoint blockade have demonstrated mixed results in the treatment of sarcomas . 
the phase ii alliance a091401 study examined nivolumab monotherapy and nivolumab plus ipiliumumab in the treatment of metastatic sarcoma.7 two of 38 patients experienced conrmed responses with nivolumab treatment , and six of 38 experienced responses to the combination.7 in a single - arm , phase ii study of pembrolizumab in soft tissue sarcoma or bone sarcoma cohorts , the overall response endpoint was not met , though seven of 40 patients with soft tissue sarcoma and two of 10 patients with liposarcoma experienced responses.8 preliminary activity was seen ( 3 - month progression - free survival , 72.7% ) with the combination of axitinib and pembrolizumab in a single - arm , phase ii study in alveolar soft - palate sarcomas.9 on may 23 , 2017 , the us food and drug administration ( fda ) approved pembrolizumab for the second - line treatment fig 2 . 
penta c and penta d are polymorphic pentanucleotide markers that show identity between the tumor and normal samples . of msi - high ( msi - h ) or mmr - decient ( dmmr ) solid tumors on the basis of ndings in patients retrospectively identied ( keynote - 012 , - 028 , and - 158 ) and prospectively enrolled ( keynote - 016 , - 158 ) .10 , 11 in these trials , msi status was identied prospectively by local laboratory - developed pcr ( n = 60 of 149 patients ) , ihc ( n = 47 of 149 ) , or both ( n = 42 of 149 ) ; retrospectively , 14 of 149 patients were identied by a central laboratorydeveloped pcr test.12 in practice , dmmr status is established by ihc for expression of mmr proteins ( mlh1 , msh2 , msh6 , and pms2 ) , and msi - h is demonstrated by multiplexed pcr of either the national cancer institute panel of two mononucleotide and three dinucleotide the more widely used panel of ve quasimarkers or monomorphic mononucleotide markers ( promega , madison , wi )  . 
at columbia university irving medical center , both ihc and pcr are used , as either can miss individual cases.13 in addition , large ngs panels , such as the one performed in the case , can be used to evaluate for msi . 
the cccp assay interrogates 8 , 682 monoand di - nucleotide repeat loci a 1.27 - mb region of interest and classies tumors as microsatellite stable or unstable according to the number of altered microsatellite loci.14 cases that cannot be denitively classied as microsatellite stable or unstable by the cccp assay are rare and were not seen in the more than 200 cases used in validation , which encompassed a range of tumor types . although the efcacy of programmed death 1 blockade in microsatellite - unstable tumors is well established , 10 , 11 , 15 to our knowledge this is the rst report of a clinical outcome of an intimal sarcoma associated with treatment with immune checkpoint blockade . 
we present this case in part for that reason but also to highlight challenges in executing the mmr - deciency testing that is critical to identify patients who may benet this fdaapproved indication ( table 1 )  . 
assays to evaluate microsatellite instability / mismatch repair deciency at columbia university irving medical center technique pcr fragment analysis what is five quasi - monomorphic mononucleotide evaluated ? repeats ( promega msi evaluation system ; promega , madison , wi ) indel variant detection in microsatellite repeat tracts ( columbia combined cancer panel , a 468 - gene ngs panel ) loss of expression of mlh1 , mlh2 , msh6 , pms2 in tumor cells limitations ? tumor percentage ; tissue type ( eg , lower sensitivity for endometrial or prostate cancers16 ; cancers in constitutional mismatch repair deciency17 ) can affect sensitivity . 
small biopsies , reactive non - neoplastic cells expressing mmr proteins , and loss - of - function variants with retained epitopes can cause false - normal ihc results , while msi testing in noncolorectal cancers may be more difcult to interpret.18 despite their greater overall sensitivity , individual results of ngs panels may be affected by heterogeneity in rates of alterations of individual repeats across tumor types , 19 especially in noncolorectal and endometrial cancers , as highlighted by this case and in a survey of 15 , 045 tumors in which lynch syndrome was identied in 1.6% ( 13 of 699 ) of msi - indeterminate tumors , predominantly noncolon / endometrial cancers ( 10 of 13 ) all of which showed abnormal ihc ( 10 of 10 tested cases ) .20 furthermore , commonly used markers ( by the national cancer institute and promega ) are not among the most frequently altered repeats in the cancer genome atlas exome data , 21 implying that that tests that use limited numbers of markers yield false negatives . 
therefore , when faced with advanced cancers with few options , multimodality testing for mmr deciency may be warranted . affiliations 1department of medicine , medical oncology , columbia university irving medical center , new york city , ny 2department of pathology , molecular pathology , columbia university irving medical center , new york city , ny subject matter of this manuscript . 
henick stock and other ownership interests : abbvie consulting or advisory role : boehringer ingelheim matthew ingham consulting or advisory role : daiichi sankyo research funding : apexigen ( inst ) , mirati therapeutics ( inst ) , ptc therapeutics ( inst ) travel , accommodations , expenses : mirati therapeutics , genentech andrew turk employment : ventana medical systems , bristol - myers squibb , medarex , bayer consulting or advisory role : bayer , bristol - myers squibb , ventana medical systems susan hsiao honoraria : medscape , illumina consulting or advisory role : ventana medical systems , bristol - myers squibb , loxo research funding : bristol - myers squibb mahesh m . 
mansukhani travel , accommodations , expenses : bristol - myers squibb , promega , er squibb sons no other potential conicts of interest were reported . references colmbia university department of pathology and cell biology : columbia combined cancer panel ( cccp )  . 
specialties / personalized - genomic - medicine / oncology - testing / columbia - combined - cancer - panel choi ey , yoon yw , kwon hm , et al : a case of pulmonary artery intimal sarcoma diagnosed with multislice ct scan with 3d reconstruction . 
yonsei med j 45 : 547 - 551 , 2004 alsou b , slater m , smith pp , et al : pulmonary artery sarcoma mimicking massive pulmonary embolus : a case report . 
asian cardiovasc thorac ann 14 : e71 - e73 , 2006 akomea - agyin c , dussek je , anderson dr , et al : pulmonary artery sarcoma mimicking pulmonary embolism : successful surgical intervention . 
ann thorac surg 61 : 1536 - 1538 , 1996 cantaloube m , moureau - zabotto l , mescam l , et al : metastatic intimal sarcoma of the pulmonary artery sensitive to carboplatin - vinorelbine chemotherapy : case report and literature review . 
case rep oncol 11 : 21 - 28 , 2018 long hq , qin q , xie ch : response of pulmonary artery intimal sarcoma to surgery , radiotherapy and chemotherapy : a case report . 
j med case reports 2 : 217 , 2008 dangelo sp , mahoney mr , van tine ba , et al : nivolumab with or without ipilimumab treatment for metastatic sarcoma ( alliance a091401 ) : two open - label , non - comparative , randomised , phase 2 trials . 
lancet oncol 19 : 416 - 426 , 2018 tawbi ha , burgess m , bolejack v , et al : pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
wilky ba , trucco mm , subhawong tk , et al : axitinib plus pembrolizumab in patients with advanced sarcomas including alveolar soft - part sarcoma : a singlecentre , single - arm , phase 2 trial . 
waalkes a , smith n , penewit k , et al : accurate pan - cancer molecular diagnosis of microsatellite instability by single - molecule molecular inversion probe capture and high - throughput sequencing . 
bakry d , aronson m , durno c , et al : genetic and clinical determinants of constitutional mismatch repair deciency syndrome : report from the constitutional mismatch repair deciency consortiueur j cancer 50 : 987 - 996 , 2014 . 
this is reflected in the current national comprehensive cancer network ( nccn ) guidelines , which state that genetic testing for brca1 / brca2 should be offered to patients with pdac with close relatives with a brca - associated cancer or to those of ashkenazi jewish ( aj ) ancestry.3 , 4 in the nccn guidelines that focus specifically on pdac , recommendations for genetic evaluation are broad , which suggests that those patients with early - onset pdac , a family history of cancer , or aj ancestry should be referred for genetic counseling.4 the rapidly evolving era of precision oncology , as well as the observation that some of these underlying germline variants are clinically actionable , raises the question of whether our current testing criteria are sufficiently inclusive . 
the three articles that accompany this editorial highlight the importance of germline testing and the need for a broader approach for genetic risk assessment in pdac . to better understand the prevalence of germline mutations in pdac , smith et al5 evaluated germline susceptibility in a high - risk group of patients with pdac who were known to harbor founder mutations . 
the authors assessed 150 patients with pdac with french canadian ( fc ) ancestry for both germline fc founder and nonfounder mutations in four dna - damage repair genesbrca1 , brca2 , palb2 , and atmcomparing mutation rates with 236 patients who were not selected for fc ancestry.5 among the fc group , a 5.3% founder mutation rate was observed . 
for nonaj or - fc patients , the authors suggest that full analysis of the aforementioned genes should be completed in patients with pdac who are diagnosed at age < 50 years or who have a strong family history of hrd - related cancers.5 these recommendations somewhat parallel the current expanded nccn guidelines , with the additional consideration of fc ancestry given the comparable germline mutation rates in fc and aj founder populations . alicia latham schwark zsofia k . 
 in contrast , in the article by reiss et al , 8 the authors suggest that a lower threshold for germline assessment of brca1 , brca2 , and palb2 in patients with pdac may be warranted . 
in this retrospective analysis , clinical outcomes , including overall survival ( os ) and response to chemotherapy , of 29 patients with advanced pdac with known pathogenic variants in brca1 , brca2 , or palb2 were compared with 58 stage , age at diagnosis , year of diagnosis , and gender matched controls.8 improved os was observed in hrd mutationpositive patients who received platinumbased therapy , specifically with 1 - year os in mutation - positive patients being 94% compared with 60% in the control group.8 of importance , mutation status did not predict an improved os in the nonplatinum group.8 this suggests that hrd mutation status may be predictive of the response to platinum therapy , but , by itself , may not be a prognostic marker , although additional studies are needed for clarification . 
interestingly , patients who were at higher risk of harboring a genetic mutation on the basis of clinical parametersthat is , young age , strong family history of cancer , or aj ancestrywere not the majority of patients who were found to have germline alterations , and , therefore , most mutation - positive patients with pdac did not meet current nccn guidelines for testing.8 this is similar to another study that suggested that the majority of brca mutationpositive patients with pdac do not meet traditional testing criteria.7 given the improved os in platinum - treated hrd mutationpositive patients , as well as the lack of clinical parameters that accurately identify hrd mutation carriers , either upfront germline testing or reflex germline assessment after suggestive tumor testing was recommended.8 a potential alternative to germline testing is the development of specific mutation signatures that predict for hrd . 
in the study by shahda et al , 11 91 tumor samples were assessed for an hrd score , with an immediate dropout of 34 samples that failed analysis as a result of low tumor cellularity , 11 which highlights the difficulty in assessing pancreatic tumor tissue for genetic information . 
70% of pdacs , respectively.14 , 18 , 19 given the lack of clinically actionable somatic driver mutations in pdac , it would then seem that an approximate 5% germline mutation prevalence in unselected , nonfounder populations in hrd - associated genes , with implications for treatment , 14 , 19 may be our most promising tool yet for pdac precision oncology . 
in light of the recent us food and drug administration approval of immune checkpoint inhibitors , such as pembrolizumab , for the treatment of all mismatch repair deficient solid tumors , 20 whether evaluation for mismatch repair deficient statuspresent in approximately 1% of pdacsis also warranted remains another important consideration.12 , 19 , 21 , 22 such genomic assessment may seem daunting . there may be concern that the overall burden of testing all pdacs for germline variants is unreasonable . 
 ovarian cancer for brca1 / 2 and colorectal cancer for lynch syndrome , recently updated nccn guidelines now also recommend that all patients with metastatic prostate cancer be referred for genetic evaluation and consideration of testing for brca and related genes.3 this is on the basis of the recent finding that 5% to 11% of such patients harbor underlying germline genetic mutations in dna repair genes , with both prognostic and predictive implications.23 in contrast to prostate cancer , the vast majority of patients with pdac succumb to their disease , with a 5 - year survival of only 8% , which highlights the critical need for identifying opportunities for precision oncology for all patients with pdac.24 , 25 given the dearth of clinically actionable somatic mutations in pdac , as well as our inability to accurately capture all hrdpdacs on the basis of clinical variables , universal germline genetic assessment to identify , at minimum , the 5% of hrdpdacs with emerging treatment and targeted therapy implicationsseems to be a clinically reasonable undertaking . 
beyond the opportunity for precision oncology , knowledge of the presence of an inherited cancer predisposition syndrome will allow for the incorporation of precision prevention oncology for at - risk family members . 
stadler consulting or advisory role : allergan ( i ) , genentech ( i ) , regeneron ( i ) , optos ( i ) , adverum ( i ) alicia latham schwark no relationship to disclose affiliations alicia latham schwark and zsofia k . 
smith al , wc , cuggia a , et al : reflex testing for germline brca1 , brca2 , palb2 and atm mutations in pancreatic cancer : mutation prevalence and clinical outcomes from two canadian research registries . 
telli ml , timms km , reid j , et al : homologous recombination deficiency ( hrd ) score predicts response to platinum - containing neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
domchek sm , aghajanian c , shapira - frommer r , et al : efficacy and safety of olaparib monotherapy in germline brca1 / 2 mutation carriers with advanced ovarian cancer and three or more lines of prior therapy . 
a major barrier is that many conventional designs are inadequate for modern drug development , yet most novel adaptive designs are difcult to understand , require complicated statistical modeling , demand complex computation , and need expensive infrastructure for implementation . 
the objective of this article is to introduce and review a class of novel adaptive designs , known as model - assisted designs , to remove this barrier and increase the use of novel adaptive designs . 
model - assisted designs enjoy superior performance comparable to more complicated , model - based adaptive designs , but their decision rule can be pretabulated and included in the protocolthus implemented as simply as the conventional designs . 
we review state - of - the - art model - assisted designs for phase i clinical trials for single - agent , drug - combination and late - onset toxicity scenarios . 
as a result , conventional designs ( eg , the 3 + 3 design ) are still dominantly used despite relatively poor performance . there is an urgent need to increase the adoption of novel adaptive designs . the objective of this article is to introduce and review a class of novel phase i and ii designs , known as model - assisted designs , 10 - 12 to overcome this quandary of simplicity versus performance . 
model - assisted designs yield superior performance compared with the conventional algorithm - based designs and are comparable to more complicated ( model - based ) designs . with the model - assisted designs , the decision rule can be pretabulated and included in the protocol and , thus , implemented in as simple a way as the conventional designs . 
 yuan et al context key objective is there any novel adaptive design that is simple to implement ? knowledge generated this article introduces and reviews a class of novel phase i and ii designs , known as model - assisted designs , to provide a stateof - the - art approach to overcome the quandary of simplicity versus performance that hinders the adoption of novel adaptive designs . 
model - assisted designs yield superior performance compared with more complicated model - based designs , but the decision rule can be pretabulated and included in the protocol and , thus , implemented in as simple a way as the conventional designs . relevance model - assisted designs are easy to implement and have great potential to improve the efciency and success rate of earlyphase trials . estimate the dlt rate , and has a greater tendency to underdose patients ( ie , it treats patients at the doses lower than the mtd )  . 
despite decades of advocacy by statisticians , the use of the crm , however , is still limited because of statistical and computational complexity of the design.8 , 9 for appropriate use , the crm requires specialized expertise to choose and calibrate the dose - toxicity model and to re - estimate the model at each decision of dose escalation / de - escalation . 
examples of model - assisted designs include the modied toxicity probability interval ( mtpi ) design23 and its variation , mtpi - 224 ; bayesian optimal interval ( boin ) design25 , 26 ; and keyboard design22 ( fig 1 )  . 
given the data observed at current dose , mtpi makes the decision of dose escalation and de - escalation on the basis of the unit probability mass ( upm ) of the three intervals . 
the upm of an interval is dened as the posterior probability that p is within the interval divided by the length of the interval , calculated according to a statistical model known as the beta - binomial model . 
comparison of design characteristics among algorithm - based , model - based , and model - assisted phase i designs algorithm based model assisted model based design characteristic transparency and simplicity in the protocol dose escalation / de - escalation rule can be predetermined and included avoids computation - intensive , repeated estimation of the dose - toxicity curve model to make interim decisions flexibility size targets any prespecied dlt rate allows decision making when the cohort size deviates from the planned no . 
6 sample size can be calibrated to ensure good operating characteristics performance identies the mtd accurately allocates a high percentage of patients to the mtd provides good overdose control abbreviations : dlt , dose - limiting toxicity ; mtd , maximum - tolerated dose . the dose stays at the current dose . 
one deciency of mtpi is that it overly downweighs the overdosing probability , because the overdosing interval is typically wider than the proper dosing interval , which leads to a high risk of overdose of patients ( ie , treatment of a high percentage of patients at doses greater than the mtd ) .22 the keyboard design addresses the overdosing issue of mtpi by dening a series of equal - width dosing intervals ( or keys ) to represent the potential locations of p.22 the proper dosing interval is called the target key . 
the design makes the decision of dose escalation and de - escalation by examining the relative position between the target key and the strongest key , in which the strongest key is dened as the interval that the true dlt is most likely located . 
if the strongest key is on the left ( or right ) side of the target key , the observed data suggest that the current dose is most likely underdosing ( or overdosing ) ; thus , the design escalates ( or de - escalate ) the dose ; otherwise , the dose stays at the current dose . 
the keyboard design outperforms the mtpi with substantially lower risk of overdosing patients and better accuracy to identify the mtd.11 , 22 the variation of the mtpi ( ie , mtpi - 224 ) adopts the same dose escalation / de - escalation rule as the keyboard design but is less transparent . 
the mtpi - 2 relies on complicated procedures , such as occams razor and model selection . compared with the mtpi / mtpi - 2 and keyboard designs , the boin design is more straightforward and transparent ( fig 1 )  . 
let p denote the observed dlt rate at the current dose , dened as the number of patients experiencing dlt at the current dose divided by the total number of dltevaluable patients treated at the current dose . the boin design makes dose escalation / de - escalation recommendations simply by comparing p with prespecied dose escalation ( e ) and de - escalation ( d ) boundaries , as illustrated in figure 2 and described as follows : 1 . 
repeat step 2 until the prespecied maximum sample size is reached or the number of patients treated on a single level reaches a certain number ( eg , 12 )  . 
at that point , select the mtd as the dose at which the dlt estimate is closest to the target.25 , 26 figure 2 provides the default , optimal dose escalation and deescalation boundaries ( e , d ) for commonly used target dlt rates ,  . 
for patient safety , boin imposes an overdose control rule : if the observed data indicate that there is more than a 95% chance that the current dose is higher than and at least three patients have been treated , the current and higher doses are eliminated from the trial . 
to determine the next dose , the modied toxicity probability interval design calculates and compares the values of the three unit probability masses ( upms ) , whereas the keyboard design compares the location of the strongest key with respect to the target key . 
bayesian optimal interval compares the observed dlt rate at the current dose with the optimized dose escalation boundary , e , and de - escalation boundary , d . the simple and intuitive structure of boin gives it several unique advantages . 
because boin guarantees deescalation of the dose when the observed toxicity rate p is higher than the de - escalation boundary d , it is particularly easy for clinicians and regulatory agents to assess the safety of a trial with boin . 
for example , given a target dlt rate of = 0.25 , we know a priori that a phase i trial using boin guarantees de - escalation of the dose if the observed dlt rate is higher than 0.298. 
suppose that , for a phase i trial with a new compound , the regulatory agency mandates that the dose must be de - escalated if the observed toxicity rate is higher than 0.25. 
we can easily fulll that requirement by setting the target dlt rate at = 0.21 , such that boin guarantees de - escalation of the dose if the p 0.25. 
such exibility and observed toxicity rate of transparency are the important advantages of boin compared with the other model - assisted designs , such as mtpi / mtpi - 2 and keyboard designs . because model - assisted designs are built upon rigorous statistical theory , like model - based designs , they also enjoy the same exibility as the model - based designs . 
in addition , unlike the 3 + 3 design , for which the dose escalation and de - escalation decisions can be made only when we have three or six evaluable patients , boin allows decision making with incomplete cohorts in the face of dropouts as a result of dlt inevaluability . 
boin design has been used for various treatment agents , including chemotherapy ( clinicaltrials . gov identier : nct02942264 ) , radiotherapy ( clinicaltrials.gov identier : nct03114462 ) , checkpoint inhibitor ( clinicaltrials . gov identier : nct03600155 ) , monoclonal antibody ( clinicaltrials.gov identier : nct03577704 ) , oncolytic virus ( clinicaltrials.gov identier : nct02705196 ) , and t - cell immunotherapy ( clinicaltrials.gov identier : nct03318900 )  . boin also has also been used in nononcology trials , such as stem cell therapy for stroke patients with stroke.35 we used an ongoing national cancer institute phase i to ii trial ( clinicaltrials.gov identier : nct02942264 ) to illustrate the design . 
one of the trials objectives of was to identify the mtd of tg02 , a pyrimidine - based multikinase inhibitor combined with temozolomide in adult patients with recurrent anaplastic astrocytoma or glioblastoma . because of lack of effective treatments for this patient population , the target dlt rate was set at a relatively high value of 0.35. 
according to the toxicity prole of tg02 in other patients with cancer , the principal vestigator chose 200 mg of tg02 as the starting dose . according to the boin design , the dose will be escalated if the observed dlt rate at the current dose is lower than e = 0.276 , and it will be deescalated if the observed dlt rate is greater than d = 0.419 ( fig 2 )  . 
for example , if the dlt takes up to 8 weeks to evaluate and the accrual rate is one patient per week , on average , then ve new patients could be accrued while investigators wait to evaluate the previous three patients outcomes . 
the question is this : how can new patients receive timely treatment when the previous patients outcomes are pending ? a few model - based designs have been proposed to address this logistic issue , including the time - to - event crm ( titecrm ) 38 and data - argumentation crm ( da - crm ) .39 these designs support continuous accrual and yield superior performance in nding the mtd.39 , 40 however , like the crm , they are statistically and computationally complex and require repeated model tting after each cohort , which limits their use . model - assisted designs , including time - to - event boin ( tite - boin ) 29 and time - to - event keyboard ( tite - keyboard ) designs , 41 provide a well - performing and yet easy - toimplement approach to address late - onset toxicity . 
table 2 shows the tite - boin decision rule with a cohort size of three patients , which can be generated easily using the software described in the software section . 
during the trial , at the current dose , we counted the number of patients , the number of patients who experienced dlt , and the number of pending patients and their standard total follow - up times ( stft ) ; we then used the table to make the dose escalation / de - escalation decision . 
to illustrate the use of the tite - boin decision table , suppose that three patients have been treated at the current dose : one had a dlt , one had no dlt , and one has dlt data pending . 
according to table 2 , if the stft of the pending patient is greater than 0.88 , we treat the next cohort at the same dose ; otherwise , we de - escalate the dose . 
suppose that the next cohort of three patients is treated at the same dose and that , among the six treated patients , one patient had a dlt , two had no dlt , and three have dlt data pending . 
unlike single - agent trials with a string of ordered doses , combinations in the dose matrix are only partially ordered in toxicity , and multiple mtds ( ie , the mtd contour ) may exist in the dose matrix ( appendix fig a1 )  . 
numerous designs have been proposed to nd an mtd or the mtd contour for combination trials.28 , 42 - 52 almost all are model - based designs using a strategy similar to that of a crm : devise a model to describe the dose - toxicity surface and then , on the basis of accumulating data , continuously update the model estimate to select a dose for the new patient . 
because of their statistical and computational complexity , despite good performance , these model - based designs are rarely used for conducting trials . model - assisted designs provide a simple and robust approach to phase i combination trials.43 one example is the boin combination design , 28 which makes the decision of dose escalation / de - escalation according to the same rule as the single - agent boin design described in the modelassisted designs section , and thereby inherits the singleagent designs simplicity and good performance . 
the only difference is that , in combination trials , when we decide to escalate or de - escalate the dose , there is more than one neighboring dose to which we can move . 
dose escalation and de - escalation rule for tite - boin with a target dlt rate of 0.3 and a cohort size of three patients , with up to nine patients treated at a dose no . 
for example , simons optimal ( or minimax ) two - stage design53 could be classied as a model - assisted design in the sense that it is derived from a statistical model ( ie , a binomial model for response ) , but its go / no - go decision rule can be predetermined when the design parameters are specied . 
simons optimal two - stage designs are appropriate for the simple setting in which the end point is binary and quickly ascertainable , and these designs allow only one interim look . phase ii trials sometimes are more complicated and have more than one end point . 
table 3 provides four trial examples with different types of end points ( eg , ordinal end point and coprimary end points ) .54 - 56 in addition , multiple interim looks are useful to improve the exibility and efcacy of the trial , especially in basket and platform trials.57 - 59 the bayesian optimal phase ii ( bop2 ) design60 provides a simple , exible , and efcient model - assisted design to allow multiple interims and handle different types of phase ii trials under a unied framework . the key feature of bop2 is that , although the end points in the four examples are clinically different , they all can be represented using a variable y with k distinct categories , statistically known as a multinomial random variable . 
as an example , consider a treatment that is deemed ineffective if the objective response rate ( orr ) is , in which is a threshold prespecied by clinicians ( eg , = 20% )  . 
at each interim , the go / no - go decision is made according to the following bayesian stopping criteria : stop the trial if pr ( orr | data )  . 
given the response rate deemed ineffective ( ie , the null hypothesis ) and the response rate deemed desirable ( ie , the alternative hypothesis ) , the value of cn is chosen such that the type i error rate is controlled at a prespecied level and the statistical power is maximized . 
 ( see zhou et al60 for details . ) similar bayesian stopping criteria can be applied to other types of end points to determine whether the treatment promising.60 in the equation , as a model - assisted design , one important advantage of the bop2 design is that its stopping boundary can be enumerated and included in the trial protocol before the onset of the trial . 
when they conduct the trial , clinicians simply count the number of relevant events and make the go / no - go decision according to whether that count exceeds the boundary or not . 
if the end point requires a long time to be scored , clinicians may have to suspend the accrual and wait for the interim data mature to make interim decisions . 
use the design decision table to conduct the trial and make adaptive decisions ( eg , dose escalation / stay / deescalation or go / no - go )  . discussion one major barrier for the adaptation of novel adaptive designs is that these designs often are complicated to implement . 
model - assisted designs offer the superior performance compared with the more complicated , model - based adaptive designs but , once designed , can be implemented in as simple a way as the conventional designs . 
the approach establishes a new kiss principle : keep it simple and smart ! as in all trial designs , the design parameters for modelassisted designs must be carefully chosen to reect the clinical setting and the study objective . 
for the boin design , the target dlt rate can vary with the type of phase i studies . the maximum sample size must be realistic and attainable . for the bop2 design , the choice of using a binary end point or coprimary end point , and their null and target rates , depends on which disease type is studied and how effective the standard of care is . 
the number of interim analyses should account for both design efciency and the logistic complexity . the choice of designs parameters should be validated and carefully calibrated through extensive computer simulation to ensure that the design has desirable operating characteristics under a variety of scenarios . 
jack lee consulting or advisory role : abbvie no other potential conicts of interest were reported . references kessel m : the problems with todays pharmaceutical business : an outsiders view . 
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clin cancer res 23 : 3994 - 4003 , 2017 ji y , liu p , li y , et al : a modied toxicity probability interval method for dose - nding trials . 
ruppert as , shoben ab : overall success rate of a safe and efcacious drug : results using six phase 1 designs , each followed by standard phase 2 and 3 designs . 
mu r , yuan y , xu j , et al : gboin : a unied model - assisted phase i trial design accounting for toxicity grades , and binary or continuous end points . 
bernhardt mb , de guzman mm , grimes a , et al : rapid infusion of rituximab is well tolerated in children with hematologic , oncologic , and rheumatologic 34 . 
place ae , goldsmith k , bourquin j - p , et al : accelerating drug development in pediatric cancer : a novel phase i study design of venetoclax in relapsed / refractory 35 . 
postel - vinay s , gomez - roca c , molife lr , et al : phase i trials of molecularly targeted agents : should we pay more attention to late toxicities ? j clin oncol 29 : 1728 - 1735 , 2011 june ch , warshauer jt , bluestone ja : is autoimmunity the achilles heel of cancer immunotherapy ? nat med 23 : 540 - 547 , 2017 38 . 
zhang l , yuan y : designing early - phase drug combination trials , in oquigley et al ( eds ) : handbook of methods for designing , monitoring , and analyzing dose - finding trials . 
ying y , heng z , yanhong z : phase i cancer clinical trial design : single and combination agents , in peace et al ( eds ) : biopharmaceutical applied statistics symposium , volume 1 . 
sacchi s , marcheselli r , bari a , et al : safety and efcacy of lenalidomide in combination with rituximab in recurrent indolent non - follicular lymphoma : final results of a phase ii study conducted by the fondazione italiana linfomi . 
moore kn , sill mw , tenney me , et al : a phase ii trial of trebananib ( amg 386 ; ind#111071 ) , a selective angiopoietin 1 / 2 neutralizing peptibody , in patients with persistent / recurrent carcinoma of the endometrium : an nrg / gynecologic oncology group trial . 
 programmed cell death 1 ( pd - 1 ) ligand ( pd - l1 ) expression in solid tumors as a predictive biomarker of benefit from pd - 1 / pd - l1 axis inhibitors : a systematic review and meta - analysis monica khunger adrian v . 
pennell james stevenson sanjay mukhopadhyay kurt schalper vamsidhar velcheti monica khunger , sagar rakshit , sanjay mukhopadhyay , cleveland clinic ; adrian v . hernandez , university of connecticut / hartford hospital , universidad peruana de ciencias aplicades ; vinay pasupuleti , case western reserve university school of medicine ; nathan a . pennell , james stevenson and vamsidhar velcheti , taussig cancer center , cleveland , oh ; and kurt schalper , yale university school of medicine , new haven , ct . corresponding author : vamsidhar velcheti , md , facp , center for immuno - oncology research , cleveland clinic , cleveland , oh 44195 ; e - mail : velchev@ ccf.org. purpose drugs targeting the programmed cell death 1 ( pd - 1 ) / programmed cell death ligand 1 ( pd - l1 ) pathway show significant clinical activity across several tumor types . 
use of biomarker assays to predict response to these agents is an active area of research ; however , the predictive value of pd - l1 immunohistochemistry ( ihc ) assays is largely inconsistent across clinical trials . 
in this meta - analysis of clinical trials of pd - 1 / pd - l1targeted agents , we evaluate the predictive value of a tumor and tumor - infiltrating immune cell pd - l1 ihc assay as a biomarker for objective response to pd - 1 / pd - l1 inhibitors . methods we searched databases ( pubmed , medline , asco abstracts , european society for medical oncology abstracts , and scopus ) up until december 2016 for clinical trials using pd - 1 / pd - l1 inhibitors with reported pd - l1 biomarker data . 
objective response rates ( primary end point ) from all phase i to iii trials investigating nivolumab , pembrolizumab , atezolizumab , durvalumab , and avelumab in advanced solid tumors were collected . 
odds ratios ( ors ) for response in pd - l1positive patients compared with pd - l1negative patients were calculated using the dersimonian - laird random effects model to combine trials . 
we performed metaanalysis as per the preferred reporting items for systematic reviews and meta - analyses guidelines . results forty - one distinct trials with 6 , 664 patients were identified . 
2017 by american society of clinical oncology introduction tumors often evade the immune system by either ineffective antigen presentation or by using mechanisms to thwart an effector response.1 - 3 programmed cell death 1 ( pd - 1 ) is a negative regulator or checkpoint receptor on t cells that is a key determinant of induction of immune tolerance in the tumor microenvironment . 
pd - l1 and pd - l2 expression in the normal tissues is a major mechanism of physiologic peripheral immune tolerance to dampen tissue autoimmune responses after a sustained inflammatory response to tissue damage . 
pdl1 is upregulated in various tumor types including melanoma , nonsmall - cell lung cancer ( nsclc ) , and squamous cell head and neck carcinomas and is a major mechanism of immune evasion . 
in early trials with these agents , pd - l1 expression on tumor cells ( tcs ) , measured by immunohistochemistry ( ihc ) assay , was thought to be an important biomarker for predicting response to these agents.4 however , subsequent trials , particularly atezolizuincorporated both tc and tumormab trials , infiltrating immune cell ( ic ) pd - l1 expression , and this combined pd - l1 expression was also associated with significantly higher objective response rates ( orrs ) in clinical trials . 
pharmaceutical companies have developed different pd - l1 ihc assays , and their comparability and equivalence are the subject of active research.5 , 6 however , most such studies have included relatively small numbers of patients and have not used response or outcome as an end point . 
the databases searched included pubmed , medline , embase , asco abstracts , european society for medical oncology abstracts , google scholar , and scopus . the dates searched were from the inception of each database to december 4 , 2016 . 
the search terms included the following keywords : pd - 1 , pd - l1 , cd274 , programmed cell death receptor 1 , programmed cell death receptor ligand , immune checkpoint inhibitor , nivolumab , bms936558 , pembrolizumab , mk - 3475 , mpdl3280a , atezolizumab , avelumab , msb0010718c , durvalumab , medi - 4736 , predictive biomarker , and cancer immunotherapy . 
the following information was extracted : study design , study population and setting , mean patient age , type of cancer , type of treatment , pd - l1 expression cutoff values , and follow - up time . 
pd - l1 clones used for the evaluation of pd - l1 expression varied across different trials ; 16 studies used 28 - 8 , seven studies used 22c3 , 10 studies used sp142 , three studies used sp263 , and five studies used dako clone 73 - 10 ( dako , carpinteria , ca )  . 
among all of the included studies , 10 were randomized clinical trials , whereas the rest were single - arm trials . data synthesis and analysis study quality analysis some degree of heterogeneity was expected , and random - effects meta - analyses were performed using dersimonian - laird random effects models.10 to consider the sources of heterogeneity , the following two subgroup meta - analyses were prespecified : type of cancer and type of pd - l1 ihc assay . we used the inverse variance method to calculate pooled odds ratios ( ors ) and their 95% cis . 
i2 values of 30% to 60% represented a moderate level of heterogeneity . we used review manager ( revman 5.3 ; cochrane collaboration , copenhagen , denmark ) for our statistical analyses . results eligible studies our search retrieved 3 , 542 publications . 
the majority of the studies had high risk of bias on performance bias and detection bias . meta - analyses of the association between pd - l1 expression and orr no evidence of publication bias was observed in the funnel plot ( eggers test p = .4 ; appendix fig a2 , online only )  . 
there was low heterogeneity of effects across studies in all categories ( fig 2 )  . we performed a subgroup analysis across all nsclc trials simultaneously assessing cutoff values of 1% , 5% , and 10% for pd - l1positive tcs to identify the optimal ihc cutoff threshold . this analysis included the following four trials : brahmer et al , 14 borghaei et al , 15 rizvi et al , 17 and gettinger et al.20 all of these trials included patients with nsclc ( both squamous and nonsquamous histology ) treated with nivolumab and used the dako 28 - 8 antibody for pd - l1 ihc . 
there was limited heterogeneity of effects across studies in all subgroups ( figs 3a - c )  . an additional subgroup analysis was performed across different pd - l1 ihc assays ( fig 4 )  . 
forest plots representing odds ratios of objective response in programmed cell death ligand 1 ( pd - l1 ) positive patients compared with pd - l1negative patients across different cancer types . 
however , because of the paucity of data and power limitations , we could not compare tc and ic subgroups separately . a major objective of our study was to identify the optimal pd - l1 cutoff value associated with maximum objective response . 
this was achieved by performing a subgroup analysis of four trials simultaneously reporting objective response data for three different cut points ( 1% , 5% , and 10% ) in nsclc.14 , 15 , 17 , 20 we restricted the analysis to these four trials to remove heterogeneity associated with tumor type , treatment agents , and pdl1 antibody used for ihc assay . 
all four trials assessed patients with nsclc ( both squamous and nonsquamous histology ) treated with nivolumab and used the 28 - 8 ( dako ) clone for pd - l1 ihc . 
unfortunately , because of power limitations , we were unable to assess the optimal ihc cutoff points of the us food and drug administrationapproved pd - l1 antibodies 22c3 and sp142 . 
these issues may be significant and require additional study . a standardized biomarker such as tc and ic pdl1 expression can identify patients who will derive maximum benefit from these novel agents , sparing others from potentially harmful immune - related toxicities and elevated costs . 
 a vexing issue is the finding that , in some studies , patients respond to pd - 1 / pd - l1 axis inhibitors despite negative tumor pd - l1 expression . 
this assumes special importance in the current scenario of synergistic treatment combinations to enhance therapeutic response to antipd - 1 therapy . some other limitations to using tumor pd - l1 as a standardized biomarker include different collection times of the pathology specimen and the dynamic nature of the tumor microenvironment . 
pd - l1 staining in most cases is performed on archival formalin - fixed , paraffinembedded tissue , because fresh biopsies just before or close to treatment are often not available . 
it has been suggested that previous lines of therapy might alter tumor pd - l1 expression and may explain some of the confounding results across different trials.11 however , we believe this may not have been a significant confounder in our meta - analysis because , more recently , pd - 1 / pd - l1 inhibitor trials have included fresh biopsy specimens ( within 6 months of starting treatment ) , especially many of the recent trials with pd - 1 / pd - l1 inhibitors in the front - line setting.58 tumor pd - l1 expression  . 
the response rate and progressionfree survival ( primary end point of the study ) were higher in the pembrolizumab group than in the chemotherapy group ( orr , 44.8% in pembrolizumab arm v 27.8% in chemotherapy arm )  . 
this is in stark contrast to the results of the checkmate - 26 trial ( nivolumab v platinum - based chemotherapy in the front - line setting ) , which included treatment - nave patients with advanced nsclc and allowed a more liberal inclusion criterion of  . 
these studies further highlight the importance of incorporating pd - l1 expression into future trials of pd - 1 / pd - l1 moabs , especially in the front - line setting where patients have multiple treatment options . we used objective response as the primary end point of our analysis to ensure inclusion of maximum patients , because mature survival data were not available for many of the recent trials . 
for instance , in the checkmate 17 , checkmate 57 , poplar , and oak trials , objective response did not improve as much as the os in the pd - 1 / pd - l1 arm , suggesting postprogression survival advantage.14 , 15 , 49 , 50 however , this should not significantly affect our aim of establishing the validity of pd - l1 expression as a biomarker because orr is commonly used as a surrogate biomarker for clinical benefit in oncology . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . vinay pasupuleti no relationship to disclose sagar rakshit no relationship to disclose nathan a . 
pennell consulting or advisory role : boehringer ingelheim , astrazeneca , eli lilly , regeneron research funding : genentech ( inst ) , newlink genetics ( inst ) , clovis oncology ( inst ) , astex pharmaceuticals ( inst ) , celgene ( inst ) , astrazeneca ( inst ) , pfizer ( inst ) , merck james stevenson research funding : merck sharp & dohme ( inst ) , bayer ( inst ) , bristol - myers squibb ( inst ) sanjay mukhopadhyay research funding : philips healthcare other relationship : phillips kurt schalper honoraria : takeda research funding : vasculox , tesaro , onkaido therapeutics , genoptix , takeda vamsidhar velcheti honoraria : novartis , foundation medicine , merck , bristolmyers squibb , genentech consulting or advisory role : clovis oncology , genentech , bristol - myers squibb , merck , celgene , foundation medicine , astrazeneca / medimmune , genoptix research funding : genentech ( inst ) , trovagene ( inst ) , eisai ( inst ) , oncoplex diagnostics ( inst ) , alkermes ( inst ) , nantomics ( inst ) , genoptix ( inst ) , altor bioscience ( inst ) , merck ( inst ) , bristol - myers squibb ( inst ) , atreca ( inst ) , heat biologics ( inst ) , leap therapeutics ( inst ) travel , accommodations , expenses : astrazeneca / medimmune , eisai 1 . 
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hamid o , sosman ja , lawrence dp , et al : clinical activity , safety , and biomarkers of mpdl3280a , an engineered pd - l1 antibody in patients with locally advanced or metastatic melanoma ( mm )  . 
hodi fs , kluger h , sznol m , et al : long - term survival of ipilimumab - nave patients ( pts ) with advanced melanoma ( mel ) treated with nivolumab ( anti - pd - 1 ; bms - 936558 , ono - 4538 ) in a phase 1 trial . 
ribas a , puzanov i , dummer r , et al : pembrolizumab versus investigator - choice chemotherapy for ipilimumabrefractory melanoma ( keynote - 002 ) : a randomised , controlled , phase 2 trial . 
daud ai , wolchok jd , robert c , et al : programmed death - ligand 1 expression and response to the anti - programmed death 1 antibody pembrolizumab in melanoma . 
topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of anti - pd - 1 antibody in cancer . 2521 - 2532 , 2015 n engl j med 366 : 2443 - 2454 , 2012 30 . 
choueiri tk , fishman mn , escudier bj , et al : immunomodulatory activity of nivolumab in previously treated and untreated metastatic renal cell carcinoma ( mrcc ) : biomarker - based results from a randomized clinical trial . 
mcdermott df , sosman ja , sznol m , et al : atezolizumab , an antiprogrammed death - ligand 1 antibody , in metastatic renal cell carcinoma : long - term safety , clinical activity , and immune correlates from a phase ia study . 
plimack e , bellmunt j , gupta s , et al : pembrolizumab ( mk - 3475 ) for advanced urothelial cancer : updated results and biomarker analysis from keynote - 012 . 
apolo ab , infante jr , hamid o , et al : safety , clinical activity , and pd - l1 expression of avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in patients with metastatic urothelial carcinoma from the javelin solid tumor phase ib trial . 
massard c , gordon ms , sharma s , et al : safety and efficacy of durvalumab ( medi4736 ) , an anti - programmed cell death ligand - 1 immune checkpoint inhibitor , in patients with advanced urothelial bladder cancer . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
balar av , galsky md , rosenberg je , et al : atezolizumab as first - line treatment in cisplatin - ineligible patients with locally advanced and metastatic urothelial carcinoma : a single - arm , multicentre , phase 2 trial . 
sharma p , callahan mk , bono p , et al : nivolumab monotherapy in recurrent metastatic urothelial carcinoma ( checkmate 032 ) : a multicentre , open - label , two - stage , multi - arm , phase 1 / 2 trial . 
segal n , ou s , balmanoukian a , et al : safety and efficacy of medi4736 , an anti - pd - l1 antibody , in patients from a squamous cell carcinoma of the head and neck ( scchn ) expansion cohort . 
le dt , bendell jc , calvo e , et al : safety and activity of nivolumab monotherapy in advanced and metastatic ( a / m ) gastric or gastroesophageal junction cancer ( gc / gec ) : results from the checkmate - 032 study j clin oncol 34 , 2016 ( suppl 4s ; abstr 6 ) 43 . 
nishina t , shitara k , iwasa s , et al : safety , pd - l1 expression , and clinical activity of avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in japanese patients with advanced gastric or gastroesophageal junction cancer . 
chung hc , arkenau h - t , wyrwicz l , et al : safety , pd - l1 expression , and clinical activity of avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in patients with advanced gastric or gastroesophageal junction cancer . 
kaufman hl , russell j , hamid o , et al : avelumab in patients with chemotherapy - refractory metastatic merkel cell carcinoma : a multicentre , single - group , open - label , phase 2 trial . 
nghiem pt , bhatia s , lipson ej , et al : pd - 1 blockade with pembrolizumab in advanced merkel - cell carcinoma . n engl j med 374 : 2542 - 2552 , 2016 47 . 
antonia sj , l opez - martin ja , bendell j , et al : nivolumab alone and nivolumab plus ipilimumab in recurrent small - cell lung cancer ( checkmate 032 ) : a multicentre , open - label , phase 1 / 2 trial . 
wakelee h , patel jd , heist r , et al : phase ii trial of atezolizumab for patients with pd - l1 - selected advanced nsclc ( birch ) : updated efficacy and exploratory biomarker results : topic : medical oncology . 
rittmeyer a , barlesi f , waterkamp d , et al : atezolizumab versus docetaxel in patients with previously treated nonsmall - cell lung cancer ( oak ) : a phase 3 , open - label , multicentre randomised controlled trial . 
fehrenbacher l , spira a , ballinger m , et al : atezolizumab versus docetaxel for patients with previously treated nonsmall - cell lung cancer ( poplar ) : a multicentre , open - label , phase 2 randomised controlled trial . 
spiegel dr , chaft je , gettinger sn , et al : clinical activity and safety from a phase ii study ( fir ) of mpdl3280a ( anti - pdl1 ) in pd - l1selected patients with non - small cell lung cancer ( nsclc )  . 
carbognin l , pilotto s , milella m , et al : differential activity of nivolumab , pembrolizumab and mpdl3280a according to the tumor expression of programmed death - ligand - 1 ( pd - l1 ) : sensitivity analysis of trials in melanoma , lung and genitourinary cancers . 
aguiar pn jr , santoro il , tadokoro h , et al : the role of pd - l1 expression as a predictive biomarker in advanced nonsmall - cell lung cancer : a network meta - analysis . 
socinski m , creelan b , horn l , et al : nsclc , metastaticcheckmate 026 : a phase 3 trial of nivolumab vs investigators choice ( ic ) of platinum - based doublet chemotherapy ( pt - dc ) as first - line therapy for stage iv / recurrent programmed death ligand 1 ( pd - l1 ) - positive nsclc . 
poly ( adp - ribose ) polymerase inhibitors ( parpi ) represent one approach , as investigated in previous studies using olaparib.5 - 7 we describe a patient with an unresectable mgmt unmethylated , idh wild - type gbm . 
the patient was enrolled in an observational clinical study ( sponsored by strata through which wholeoncology , ann arbor , mi ) , exome and rna sequencing on formalin - xed parafn - embedded tumor tissue revealed loss - offunction mutations in atm and tumor protein 53 ( tp53 )  . 
the tumor was classied as tumor mutational burden ( tmb ) high , programmed death - ligand 1 ( pd - l1 ) low , and microsatellite stable ( mss ; table 1 )  . 
after completion of therapy , additional review of patients records revealed a germline msh6 loss - offunction mutation , which conrmed lynch syndrome . the genomic ndings and high likelihood of lynch syndrome , along with early - phase data suggesting safety and brain penetration , provided rationale for the treating oncologist to initiate olaparib with standard chemoradiation . 
she was also treated with alternating tumor - treating elds ( optune ; novocure , st helier , jersey ) , an externally applied , low - intensity electromagnetic eld treatment shown to improve survival by 4.9 months over maintenance temozolomide alone when used 18 hours per day.8 device compliance was limited , and treatment was discontinued after 1 month . 
outside hospital records included this nding on germline testing performed by ambry genetics ( aliso viejo , ca )  . msh6 is involved in dna mismatch repair ( appendix table a1 )  . 
most mutations are somatic , found almost exclusively after temozolomide therapy.11 in this setting , they are associated with resistance to alkylating agents , hypothesized to be the dominant mechanism of acquired temozolomide resistance after therapy , likely because of failure of temozolomideinduced dna damage to result in apoptosis in mismatch repairdecient ( dmmr ) cells.12 - 24 when msh6 mutations in treatment - nave patients with mgmt are present methylated , otherwise chemosensitive tumors , treatment response is markedly attenuated.13 beyond treatment resistance , ongoing temozolomide exposure after msh6 inactivation leads to a hypermutator phenotype and tumor progression.14 - 16 parpi restore sensitivity to temozolomide in dmmr cells.25 dmmr cells may also have increased resistance to radiotherapy.26 - 28 lynch syndrome was not identied by somatic testing . often , lynch syndrome is discovered after a tumor is found to be microsatellite instability high ( msi - h ) or dmmr on immunohistochemistry . 
msh6 - mutated brain tumors , however , are often not msi - h by standard polymerase chain reaction testing , and immunohistochemistry is not standardly performed.29 in this case , mss status was determined from next - generation sequencing ( ngs ) on the basis of length variant allele counts at multiple microsatellite loci . 
while alternate ngs methods have demonstrated sensitivity and specicity in brain tumors , this specic methodology in gbm is performance of unknown.30 , 31 while decient msh6 immunohistochemical staining would conrm a pathogenic mutation , intact staining would not rule out dmmr because some mutations result in intact expression of dysfunctional protein.32 - 35 the msh6 mutation was not reported by somatic testing because of its presence in a stretch of repeating cytosines , known as a homopolymer region . 
380 cns tumors associated with protein loss of function.45 as previously mentioned , p53 - decent cells may be particularly vulnerable to dna - damaging treatment when an atm mutation is present . 
conversely , the combination of dmmr and p53 - decient cells worsens response because of failed phosphorylation of p53 and , thus , failed cell arrest after treatment - induced dna damage.46 in general , cancers with mutant p53 have reduced sensitivity to chemotherapy and radiation ; however , there are many instances where mutant p53 has no effect or even enhances treatment effect.47 tmb high tmb was determined from ngs and included noncoding and coding , synonymous and nonsynonymous , and singlenucleotide and multinucleotide variants present at  . 
while frequently performed through immunohistochemistry , classication was based on sequencing results in this patient , using a score derived from the percent of maximum pd - l1 expression across tested tumor samples . 
this method is validated in a lung cancer cohort , but accuracy in gbm is less certapd - l1 is expressed on the surface of most glioma cells , with increased frequency in high - grade gliomas such as gbm , and variable detection is based on technique.52 - 54 of note , several studies demonstrated high pd - l1 association with worse survival gbm.55 there are no currently approved drugs that target pd - l1 in gbm , although several trials are ongoing . 
given the efcacy of programmed death 1 ( pd - 1 ) / pd - l1 blockade in dmmr tumors , immunotherapy could be considered.56 the pd - 1 inhibitor pembrolizumab is approved for all msi - h tumors , making it a treatment option for patients with lynch syndromeassociated cancers , which are typically msi - h . rationale for olaparib parp is involved in single - strand dna break and base excision repair . 
 file , morgan , and khagi expression in gbm.57 olaparib is a parpi that impairs the ddr , increasing treatment - induced chromosomal instability , cell cycle arrest , and apoptosis.58 in patients with germline brca1 / 2 mutations that impair double - strand dna break repair by homologous recombination , parpi cause synthetic lethality with signicant clinical benet.59 - 62 parpi also have efcacy in tumors with mutations in ddr including atm , and in patients with neither genes , a germline brca mutation nor other homologous recombination deciency.63 , 64 parpi have been used as monotherapy and in combination with radiation and chemotherapy to prevent the repair of treatment - induced dna breaks , thereby promoting tumor cell death . 
parpi increase sensitivity to temozolomide in cell and xenograft models of gbm.65 - 67 this effect persists in mgmt unmethylated tumors.68 parpi also restore sensitivity to temozolomide in dmmr cells.25 , 69 in addition , exposure to temozolomide before or concurrently with a parpi increases the magnitude of dna damage and led to complete regression of gbm cells in one study.70 this treatment - sensitizing effect is not present in patients with temozolomide resistance , which suggests optimal corporation in newly diagnosed gbm.71 there have been 3 phase i trials of olaparib with temozolomide and / or radiation in gbm . 
the oparatic trial conrmed tumor penetration and dosing schedule , with promising early results.5 , 7 paradigm - 2 investigated olaparib plus radiotherapy with or without temozolomide.6 , 72 these studies support the addition of olaparib to temozolomide and radiation as safe , well tolerated , and potentially radiosensitizing.5 discussion this patient had an excellent , durable response despite many factors that predict a poor prognosis . 
in addition , somatic msh6 loss - of - function mutations contribute to temozolomide resistance , glioma recurrence , and tumor progression , with similar effects expected from a deleterious germline mutation . 
while atm mutations improve treatment sensitivity , particularly with concurrent tp53 mutations , it is unlikely that this would result in a sustained , near - complete response with standard chemoradiation alone . 
it is also unlikely that tumor - treating elds improved clinical outcome given short duration of use . in addition to the general chemoand radiosensitizing properties of parpi , the ability for parpi to restore sensitivity to temozolomide in dmmr and mgmt unmethylated tumors , as well as efcacy of parpi in ddr - decient tumors , strongly suggests that olaparib was an essential component of the treatment regimen . 
the likelihood of olaparib - induced synthetic lethality is high , through impairment of single - stranded dna break repairs in a tumor already decient in base - base substitution , single - base insertion , and single - base deletion mismatch repair as well as double - stranded dna break repair . genomic sequencing allows identication of patients with targetable mutations who may benet from currently available treatments , which are increasing rapidly.73 this is particularly important for patients predicted to have poor outcomes with standard treatment and limited access to clinical trials . novel treatment approaches in the rst - line setting are needed . 
morgan honoraria : medscape , pharmacy times continuing education travel , accommodations , expenses : medscape , pharmacy times continuing education simon khagi research funding : lambda technologies no other potential conicts of interest were reported . acknowledgment we acknowledge jason merker , md , phd ; william kim , md ; shetal patel md , phd ; amber cipriani , pharmd ; and ashlynn messmore , ms , for their contributions to the university of north carolina multidisciplinary mtb . we also acknowledge carlos zamora , md , phd , for review of the radiographic images and scott tomlins , md , phd , co - founder and chief medical ofcer of strata oncology , for providing descriptions of the sequencing methodology . 
we thank the patient for allowing us to share a part of her story . references stupp r , mason wp , van den bent mj , et al : radiotherapy plus concomitant and adjuvant temozolomide for glioblastoma . 
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j clin oncol 36 , 2018 ( suppl ; abstr 2018 ) fulton b , short sc , james a , et al : paradigm - 2 : two parallel phase i studies of olaparib and radiotherapy or olaparib and radiotherapy plus temozolomide in patients with newly diagnosed glioblastoma , with treatment stratied by mgmt status . 
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jama 318 : 2306 - 2316 , 2017 edelmann w , yang k , umar a , et al : mutation in the mismatch repair gene msh6 causes cancer susceptibility . 
cahill dp , levine kk , betensky ra , et al : loss of the mismatch repair protein msh6 in human glioblastomas is associated with tumor progression during temozolomide treatment . 
nguyen sa , stechishin od , luchman ha , et al : novel msh6 mutations in treatment - nave glioblastoma and anaplastic oligodendroglioma contribute to temozolomide resistance independently of mgmt promoter methylation . 
liu l , markowitz s , gerson sl : mismatch repair mutations override alkyltransferase in conferring resistance to temozolomide but not to 1 , 3 - bis ( 2 - chloroethyl ) 1068 , 2008 [ erratum : nature 494 : 506 , 2013 ] nitrosourea . 
pepponi r , marra g , fuggetta mp , et al : the effect of o6 - alkylguanine - dna alkyltransferase and mismatch repair activities on the sensitivity of human melanoma cells to temozolomide , 1 , 3 - bis ( 2 - chloroethyl ) 1 - nitrosourea , and cisplatj pharmacol exp ther 304 : 661 - 668 , 2003 19 . 
hochhauser d , glynne - jones r , potter v , et al : a phase ii study of temozolomide in patients with advanced aerodigestive tract and colorectal cancers and methylation of the o6 - methylguanine - dna methyltransferase promoter . 
aquilina g , ceccotti s , martinelli s , et al : n - ( 2 - chloroethyl ) - n ( cid : 2 ) - cyclohexyl - n - nitrosourea sensitivity in mismatch repair - defective human cells . 
stark am , doukas a , hugo hh , et al : the expression of mismatch repair proteins mlh1 , msh2 and msh6 correlates with the ki67 proliferation index and survival in patients with recurrent glioblastoma . 
koi m , umar a , chauhan dp , et al : human chromosome 3 corrects mismatch repair deciency and microsatellite instability and reduces n - methyl - n ( cid : 2 ) - nitro - nnitrosoguanidine tolerance in colon tumor cells with homozygous hmlh1 mutation . 
curtin nj , wang lz , yiakouvaki a , et al : novel poly ( adp - ribose ) polymerase - 1 inhibitor , ag14361 , restores sensitivity to temozolomide in mismatch repairdecient cells . 
yan t , schupp je , hwang hs , et al : loss of dna mismatch repair imparts defective cdc2 signaling and g ( 2 ) arrest responses without altering survival after ionizing radiation . 
gylling ah , nieminen tt , abdel - rahman wm , et al : differential cancer predisposition in lynch syndrome : insights from molecular analysis of brain and urinary 30 . 
trabucco se , gowen k , maund sl , et al : a novel next - generation sequencing approach to detecting microsatellite instability and pan - tumor characterization of 1000 microsatellite instability - high cases in 67 , 000 patient samples . 
dudley b , brand re , thull d , et al : germline mlh1 mutations are frequently identied in lynch syndrome patients with colorectal and endometrial carcinoma demonstrating isolated loss of pms2 immunohistochemical expression . 
am j surg pathol 39 : 1114 - 1120 , 2015 iv ady g , madar l , dzsudzs ak e , et al : analytical parameters and validation of homopolymer detection in a pyrosequencing - based next generation sequencing systebmc genomics 19 : 158 , 2018 36 . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
int j radiat oncol biol phys 50 : 511 - 523 , 2001 19 : 3189 - 3200 , 2013 18 : 1899 - 1908 , 2019 jiang h , reinhardt hc , bartkova j , et al : the combined status of atm and p53 link tumor development with therapeutic response . 
tchelebi l , ashamalla h , graves p : mutant p53 and the response to chemotherapy and radiation , in deb s , deb s ( eds ) : mutant p53 and mdm2 in cancer . subcellular biochemistry , volume 85 . 
salem m , grothey a , kim e , et al : impact of mlh1 , pms2 , msh2 , and msh6 alterations on tumor mutation burden ( tmb ) and pd - l1 expression in 1 , 057 microsatellite instability - high ( msi - h ) tumors . 
tentori l , leonetti c , scarsella m , et al : systemic administration of gpi 15427 , a novel poly ( adp - ribose ) polymerase - 1 inhibitor , increases the antitumor activity of temozolomide against intracranial melanoma , glioma , lymphoma . 
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miknyoczki sj , jones - bolin s , pritchard s , et al : chemopotentiation of temozolomide , irinotecan , and cisplatin activity by cep - 6800 , a poly ( adp - ribose ) base excision repair . 
clarke mj , mulligan ea , grogan pt , et al : effective sensitization of temozolomide by abt - 888 is lost with development of temozolomide resistance in glioblastoma xenograft lines . 
lesueur p , lequesne j , grellard jm , et al : phase i / iia study of concomitant radiotherapy with olaparib and temozolomide in unresectable or partially resectable glioblastoma : ola - tmz - rte - 01 trial protocol . 
ahluwalia , md5 ; howard colman , md , phd6 ; geoffrey fell , ms1 ; evanthia galanis , md7 ; john de groot , md8 ; jan drappatz , md9 ; andrew b . 
wen , md1 purpose adequately prioritizing the numerous therapies and biomarkers available in late - stage testing for patients with glioblastoma ( gbm ) requires an efcient clinical testing platforwe developed and implemented insight ( individualized screening trial of innovative glioblastoma therapy ) as a novel adaptive platform trial ( apt ) to develop precision medicine approaches in gbm . methods insight compares experimental arms with a common control of standard concurrent temozolomide and radiation therapy followed by adjuvant temozolomide . 
at the initiation of insight , three experimental arms ( neratinib , abemaciclib , and cc - 115 ) , each with a proposed genomic biomarker , are tested simultaneously . 
as the trial progresses , randomization probabilities adapt on the basis of accumulating results using bayesian estimation of the biomarker - specic probability of treatment impact on progression - free survival . treatment arms may drop because of low probability of treatment impact on overall survival , and new arms may be added . 
detailed information on the statistical model and randomization algorithm is provided to stimulate discussion on trial design choices more generally and provide an example for other investigators developing apts . conclusion insight ( nct02977780 ) is an ongoing novel biomarker - based , bayesian apt for patients with newly diagnosed unmethylated gbm . 
clinical trials in the era of precision medicine must consider how to develop biomarker data during the trials , make efcient use of multiplexed biomarker screening , and develop assignment algorithms for patients positive for more than one biomarker . 
 alexander et al master protocols and adaptive platform trials ( apts ) have been proposed as attractive solutions to efciently address multiple therapeutic and biomarker hypotheses.5 - 7 we developed insight ( individualized screening trial of innovative glioblastoma therapy ) , a multisite investigator - initiated phase ii screening apt , as a solution to precision medicine development challenges for patients with gbm . 
insight was specically designed to enable efcient use of randomly assigned controls , generate information to support genomic biomarker development , and leverage the xed cost of trial development across more experimental therapies . methods eligibility patients are eligible for insight if they have newly diagnosed gbm with unmethylated o6 - methylguanine dna methyltransferase ( mgmt ) gene promoters and negative idh1 r132h mutationspecic immunohistochemistry . 
the marginal benet of temozolomide ( tmz ) in patients with unmethylated mgmt promoters8 offers the opportunity to test experimental therapies without combinations with tmz.9 , 10 this potentially accelerates the overall time for drug development ( by not needing prior separate phase i studies with tmz ) and eliminates the potential for subtherapeutic dose of the experimental agent as a result of overlapping toxicity with tmz.2 , 3 insight therefore can support experimental arms with tmz combinations or with the experimental agent alone . 
experimental therapies may also replace tmz in the concurrent radiation therapy ( rt ) portion ( if there is a compelling radiosensitizing hypothesis ) , the adjuvant portion , or both . a pure radiosensitizing agent or experimental rt regimen could theoretically replace standard rt / tmz while keeping the adjuvant tmz intact . eligibility for insight requires sufcient genotyping data to dene the predetermined biomarker categories for arms currently in the trial . 
additional details regarding the initial experimental arms and biomarkers are included in the data supplement . statistical considerations operating characteristics , and secondary analyses use the proportional hazards ( ph ) model for both pfs and os . there are several arguments to support the use of different outcomes for adaptive randomization ( pfs ) and nal efcacy evaluation ( os )  . 
the relationship between accrual rate and event timing is crucial for response - adaptive trials , because effective variation of randomization probabilities requires rapid generation of treatment effect estimates on the basis of an adequate number of individual outcomes . 
in addition , treatment effects may have a stronger signal on pfs , a relationship illustrated previously.12 finally , potential issues with pseudoprogression and pseudoresponse13 , 14 are mitigated by preserving os as the foundation for stopping rules and nal efcacy analyses . that is , promising early results of an experimental treatment accelerate the accrual rate of the corresponding arm without reducing the nal sample size of the other experimental arms . group - specic adaptive randomization probabilities . 
patients are randomly assigned using an adaptive algorithm that updates randomization probabilities for the various arms in each biomarker group monthly.15 the algorithm uses available information generated by insight ( the individual biomarker groups combined with individual pfs ) to determine the randomization probabilities that will be used to allocate patients for the subsequent month . 
the hazard function for each patient assigned to an experimental arm is modeled , rescaling the baseline by a factor that depends on treatment ( main effect ) , biomarker - specic coefcients , and biomarker - treatment interaction terms . 
we previously described the use of ph models for the computation of randomization probabilities.17 we indicate the individual prole withx ( cid : 1 ) ( x1 , x2 , x3 )  . 
the hazard function x , a ( t ) for the timeto - event outcome of a patient with biomarker prole x , randomly assigned to experimental arm a , is proportional to the baseline ( t )  . 
insight will randomly assign a maximum of 70 patients to each experimental arthe sample size for the initial set of arms is 70 patients per arm across four arms , for a total of 280 patients , but there are early stopping rules for futility in each arm , and other arms may be added as the trial is ongoing . 
such an increase will depend on the number of experimental arms added and the time at which they will start enrollment . the later new arms start enrolling , the larger the corresponding sample size expansion will be . 
indeed , when a new experimental arm is added , the design increases the control - specic sample size to guarantee enrollment of 70 patients in the control after the addition of a novel arwe previously described the adjustment of the control sample size with the addition of novel arms and potential futility early stopping of experimental arms in platforms.18 operating characteristics of outcome adaptive randomization are related to the accrual rate relative to the event rate , because information from events is used to alter probability of random assignment for newer patients . 
biomarker frequencies were assumed on the basis of data from prior genomic proling.19 monthly updates of the randomization probabilities are combined with a sequential decision rule that drops experimental arms when there is insufcient preliminary evidence to warrant additional investigation of the treatment based on the primary end point ( os )  . 
we describe a linear boundary that provides thresholds for predictive probabilities to dene the decision rule . 2 of the main effect prior normal distributions were used for the regression parameters  . 
they are a priori independent , and the variance a a is set to have the 80th and 20th percentiles that correspond to ( log [ 2 ] ; duplication of the hazard ) and ( log [ 1 / 2 ] )  . 
 alexander et al whereas for a hypothetic arm added later during the study , it increases with the number of patients randomly assigned to the novel arm and the concomitant random assignments to the control aradaptive randomization intervenes only after the initial burn - in period . as we discussed previously , 17 , 20 to preserve the power of detecting treatment effects , it is important to guarantee sufcient enrollment in the control arrandomization probabilities for the control are obtained by matching ( under the hypothesis that all the active arms will complete accrual and will not be stopped for futility ) the expected number of patients randomly assigned to the control and the planned sample size specic to the control . 
for example , if after 10 enrollments two patients have been assigned to the control , then the 11th patient is assigned to the control with a probability of ( 70 2 ) / ( 280 10 )  . 
the same approach is used if one experimental arm is dropped for futility or a novel arm is added , with the consequence of an expansion of the control sample size.18 burn - in randomization . 
this is an important difference with respect to other adaptive designs , which include a component of competition and negative correlation with the nal number of patients enrolled by different experimental arms . 
the accrual can be stopped earlier for an experimental arm ( before this maximum is reached ) only when the likelihood of a positive nal result becomes insufcient and triggers the early stopping on the basis of futility . 
as a consequence , the adaptive algorithm has a substantial impact on the duration the arm - specic accrual period , which tends to be shortened for the arms with positive treatment effects , with little effect on other operating characteristics . 
bayesian randomization can only modify the enrollment rate and accelerate accrual to the most promising arms , particularly for the patients who are more likely to benet from these treatments . 
we also predict future biomarker proles x using a standard dirichlet conjugate model . monthly , bayesian sampling is used to generate nal trial data from the predictive distribution , including the enrollment of future patients , and pfs and os outcomes , both for patients previously enrolled and for those who have not yet been enrolled . 
using bayesian terminology , we sample multiple times from the predictive distribution every month . these data sets , including the actual data generated up to a time point by the trial and a complementary component of probabilistically imputed data , describe expectation and uncertainty on how we predict the data to look at completion of the study ( including censored data points ) on the the available information . 
these computations basis of assume that the open arms will reach the nal sample size of 70 patients and allow us to derive a single predictive probability of interest for each experimental arm , at each interim analysis , of a well - dened event . 
prediction ( the probability that the arm - specic result will be signicant ) is used monthly to decide either to continue or to discontinue the study of the experimental ara key step of the process is the simulation of the baseline and the ph model parameters from the posterior at each interim analysis . 
these steps are iterated so that the relative frequency of generated arm - specic p values below the signicance threshold approximates the targeted prediction probability . the arm is stopped if the prediction probability of a positive result becomes small . 
a linear boundary that increases with the number of enrollments from 0 at the onset of the study up to 0.1 is used to dene monthly the cutoff for discontinuing or proceeding with the study of the experimental treatment . 
in the comparison of these simulations with a balanced design , keeping the described early stopping mechanism for futility , enrollment in arms with positive treatment effects was completed faster , with an average time reduction between 16% and 27% across simulation scenarios . a similar power analysis like that for pfs was repeated for os . 
although the power to reject the null was of course considerably the power to detect a signicant biomarker / reduced , treatment interaction ( null hypothesis : no treatment effect in the cdk - positive group ) in the secondary analyses was higher ( 0.66 ; table 2 )  . 
the noncompeting maximum number of patients ( ie , 70 ) per arm maintained the power of detecting a positive treatment effect for each experimental arm stable with respect to the presence of treatment effects on the remaining arms . sensitivity to pfs and os correlation seemed limited . 
we considered both different magnitudes of pfs and os hrs contrasting an experimental treatment and a control ( appendix table a2 ) and various pfs - os correlation degrees at the individual level . 
additional sensitivity analyses , including the probability of reporting a positive treatment effect for the biomarker - positive group under selected scenarios ( appendix table a4 ) , the power for arms added later during the course of the platform trial ( appendix table a5 ) , and the power assuming different possible accrual rates ( appendix table a6 ) , are included in the appendix . 
in contrast to alternative response - adaptive designs , the low correlation of accrual rate with nal armspecic sample size ( which , as described in methods , can be fewer than 70 patients only as a result of early stopping for futility ) induces little variations of power estimates across table 2 . 
in the middle column , only a single arm has positive treatment effects restricted to a single biomarker - positive subpopulation ( prevalence , 0.5 ) and hazard ratios ( hrs ) of 1 for the rest of the patients . 
accrual rate therefore correlates with time required to complete the arm evaluation , but it does not correlate with power . discussion clinical trials under master protocols have been proposed as a methodologic innovation to more efciently answer therapeutic development questions.6 , 7 , 22 such innovations are particularly important in the era of precision medicine , where biomarker testing adds complexity by increasing the testable hypotheses . 
platform trials under number of master protocols are intended to study multiple targeted therapies in the context of a single disease in a perpetual manner , with therapies allowed to enter or leave the platform on the basis of a decision algorithm.7 ( p63 ) potential efciencies include the conservation of control arms , multiplexed biomarker screening data , and reduced downtime because the trial infrastructure is maintained as treatment arms enter or leave the trial . 
platforms also enable innovative statistical approaches to increase efciency.23 - 27 insight is the rst biomarker - based apt designed to apply these general solutions to specic problems in therapeutic development for gbm.28 late - stage clinical trial failures are a major issue for therapeutic development in general1 and in gbm specically.2 , 3 failure in phase iii may be linked to erroneous go / no - go decisions on the basis of phase ii results that have different end points than the desired pivotal trial , overestimate treatment effects on the basis of comparisons with historical controls , or both . 
prior data have shown that effects on imaging - based end points such as response rate and pfs may not translate to effects on os.4 , 13 , 29 - 31 furthermore , comparison of end points like pfs and os with historical controls may overestimate treatment effects through selection bias , temporal drift , and failure to account for control variability.4 for these reasons , we chose to use os as the primary end point of in unmethylated gbm , the trial . survival postprogression is generally short , and there are no proven effective therapies at recurrence that increase the chance of detecting a true therapeutic impact on os.12 we included a randomly assigned control arm to avoid the pitfalls associated with comparison with historical controls for os in gbm.4 the platform design affords considerable efciency by using a single control arm for comparison against multiple therapies and offers patients a higher probability of being randomly assigned to an experimental arfurthermore , we use bayesian rar17 based on accumulating pfs results to increase the probability of random assignment to arms that showed more promise.28 , 32 we had previously shown that rar using an os end point was possible for recurrent gbm17 and additionally supported this approach in our simulations during the development of insight . 
however , to increase efciency , we opted to use pfs , because earlier end point assessment can more rapidly inuence randomization.16 if we were to nd a discordance between therapeutic impact on pfs and os , randomization probability would be altered , but decision making on the primary end point would remain unchanged . another advantage of platform trials is the efcient use of multiplexed genomic biomarker data for treatment assignments . 
gbm is characterized by redundant and overlapping alterations in several molecular pathways rather than mutually exclusive driver mutations.33 as such , patients can be positive for multiple genomic biomarkers . some platform trials like nci - match ( national cancer institute molecular analysis for therapy choice ) , 34 lung map ( lung cancer master protocol ) , 35 battle ( biomarkerintegrated approaches of targeted therapy for lung cancer elimination ) , 36 and n2m2 ( national center for tumor diseases neuro master match ) 37 generally deal with this situation through an assignment algorithm on the basis of relative evidence of biomarker - specic accrual and / or therapeutic efcacy . i - spy 2 ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) , in contrast , uses biomarker subgroupspecic randomization probabilities to allow data generated during the trial to drive the biomarker specicity of arm assignments.38 insight does the latter , starting with equal randomization among the experimental arms and allowing the rar procedure to prioritize randomization in a biomarker - specic way . 
for example , if only patients with egfr amplication in the neratinib arm were living longer than those in the control , the randomization algorithm would increase the probability of egfr - amplied patients assigned to neratinib ( regardless of their other biomarkers ) while potentially reducing assignment to neratinib for egfr wild - type patients . in fact , this situation occurred in i - spy 2 , where the adaptive randomization algorithm stopped assigning patients with human epidermal growth factor receptor 2 ( her2 ) negative / hormone receptorpositive cancer and those with her2negative / hormone receptornegative cancer to neratinib during the course of the trial , even as it reached the prespecied efcacy threshold in the her2 - positive / hormone receptor negative signature.39 this strategy may be optimal when there are limited pretrial data or a weak hypothesis suggesting a biomarker - specic effect . 
in these situations , more biomarker specicity may be desired from the start of the trial , and we have suggested ways to integrate this into a platform design.40 more generally , adding future biomarkers specic to additional experimental arms increases design complexity and requires appropriate denitions of the randomization probabilities . 
even though insight used randomization , we queried clinically annotated genomic data33 , 43 to investigate the possibility that the biomarkers we used had prognostic signicance or a variable relationship between pfs and os and found no such associations.19 although the perpetual clinical provided by the apt framework can provide signicant efciencies , it can create additional challenges as well . maintaining ongoing operations requires both nancial framework that trial models that support ongoing concerns and active pipeline development to maintain a regular ow of experimental arms . 
more complex bayesian designs require engaged clinical and statistical investigators and new ways of determining operating characteristics through simulation.44 reporting of trial results is complicated because of the separation between the master protocol and the armspecic data . 
arms that leave the trial because of success or failure need to be reported while the overall trial is still ongoing , which does not lend itself to traditional trial reporting best practices like consort . 
two recent publications from i - spy 2 are examples.39 , 45 conversely , reporting on the overall master protocol does not have a natural time point , although most groups publish a general description of the overall trial structure without results.35 , 36 , 38 , 41 in conclusion , insight is an ongoing novel biomarkerbased bayesian apt for patients with newly diagnosed unmethylated gbm . 
ahluwalia stock and other ownership interests : mimivax honoraria : prime oncology , elsevier , itamar medical ( i ) consulting or advisory role : monteris medical , astrazeneca , bristol - myers squibb , abbvie , cbt pharmaceuticals , kadmon , vbi vaccines research funding : novartis , tracon pharma , novocure , spectrum pharmaceuticals , eli lilly / imclone , boehringer ingelheim , astrazeneca howard colman honoraria : merck sharp & dohme consulting or advisory role : genentech , roche , novocure , omniox , insys therapeutics , abbvie research funding : newlink genetics , plexxikon , kadmon , orbus therapeutics , merck , dnatrix , abbvie , beigene evanthia galanis consulting or advisory role : genentech / roche ( inst ) , abbvie ( inst ) , oncorus research funding : genentech / roche ( inst ) , merck ( inst ) john de groot employment : helsinn therapeutics ( i ) , ziopharm oncology ( i ) leadership : ziopharm oncology ( i ) stock and other ownership interests : gilead sciences , ziopharm oncology ( i ) consulting or advisory role : celldex , deciphera , vascular biogenics , foundation medicine , genentech / roche , omniox , oxigene , abbvie , novogen , kadmon , merck , five prime therapeutics , insys therapeutics , astrazeneca , boston biomedical , gw pharmaceuticals , carthera research funding : deciphera , novartis , eli lilly , sano , emd serono , mundipharma patents , royalties , other intellectual property : sano , research support ; astrazeneca , research support ; emd serono , research support ; eli lilly , research support ; novartis , research support ; deciphera pharmaceuticals , research support jan drappatz employment : via oncology stock and other ownership interests : exelixis , bristol - myers squibb honoraria : uptodate , via oncology consulting or advisory role : oncorus , immunomix patents , royalties , other intellectual property : uptodate andrew b . 
burt nabors consulting or advisory role : bristol - myers squibb speakers bureau : merck / schering plough sandro santagata consulting or advisory role : rarecyte david schiff consulting or advisory role : orbus therapeutics , monteris medical , cavion ( inst ) research funding : bayer healthcare pharmaceuticals ( inst ) mary r . 
wen consulting or advisory role : abbvie , genentech / roche , agios , astrazeneca , karyopharm therapeutics , vivus , monteris medical , aurora biopharma , vascular biogenics , kadmon , ziopharm oncology , gw pharmaceuticals , eli lilly , immunomic therapeutics speakers bureau : merck , agios ( inst ) , abbvie ( inst ) , angiochem ( inst ) , genentech / roche ( inst ) , glaxosmithkline ( inst ) , astrazeneca ( inst ) , immunocellular therapeutics ( inst ) , karyopharm therapeutics ( inst ) , merck ( inst ) , novartis ( inst ) , oncoceutics ( inst ) , sano ( inst ) , ariad pharmaceuticals ( inst ) , vascular biogenics ( inst ) , eli lilly no other potential conicts of interest were reported references thomas dw , burns j , audette j , et al : clinical development success rates 2006 - 2015 . 
j clin oncol 35 : 2402 - 2409 , 2017 vanderbeek am , rahman r , fell g , et al : the clinical trials landscape for glioblastoma : is it adequate to develop new treatments ? neuro oncol 20 : 1034 - 1043 , 2018 grossman sa , schreck kc , ballman k , et al : point / counterpoint : randomized versus single - arm phase ii clinical trials for patients with newly diagnosed glioblastoma . 
nat rev clin oncol 9 : 199 - 207 , 2011 berry sm , connor jt , lewis rj : the platform trial : an efcient strategy for evaluating multiple treatments . 
n engl j med 377 : 62 - 70 , 2017 stupp r , hegi me , mason wp , et al : effects of radiotherapy with concomitant and adjuvant temozolomide versus radiotherapy alone on survival in glioblastoma in a randomised phase iii study : 5 - year analysis of the eortc - ncic trial . 
alexander bm , trippa l : getting it rst versus getting it right : weighing the value of and evidence for progression - free survival as a surrogate endpoint for overall survival in glioblastoma . 
han k , ren m , wick w , et al : progression - free survival as a surrogate endpoint for overall survival in glioblastoma : a literature - based meta - analysis from 91 trials . neuro - oncol 16 : 696 - 706 , 2014 30 . 
herbst rs , gandara dr , hirsch fr , et al : lung master protocol ( lung - map ) : a biomarker - driven protocol for accelerating development of therapies for squamous cell lung cancerswog s1400 . 
pfaff e , kessler t , balasubramanian gp , et al : feasibility of real - time molecular proling for patients with newly diagnosed glioblastoma without mgmt promoter hypermethylation : the nct neuro master match ( n2m2 ) pilot study . 
the phosphatidylinositol 3 - kinase ( pi3k ) / akt / mtor signaling axis plays a central role in cell growth , survival , motility , and metabolism in a variety of cancers ( fruman da , et al : nat rev drug discov 13 : 140 - 156 , 2014 ; engelman ja : nat rev cancer 9 : 550 - 562 , 2009 ) , including glioblastoma ( gbm ; brennan cw , et al : cell 155 : 462 - 477 , 2013 )  . 
dna - dependent protein kinase is a serine / threonine kinase involved in the repair of dna double - strand breaks ( collis sj , et al : oncogene 24 : 949 - 961 , 2005 ) , which are considered to be the most lethal dna lesions and the main driver of cellular death after treatment with ionizing radiation therapy ( rt )  . 
therefore , beyond its hypothesized growth - inhibitory effect as monotherapy , cc - 115 has the potential to be a radiation - sensitizing agent in the treatment of gbm ( zhao y , et al : cancer res 66 : 5354 - 5362 , 2006 )  . 
one phase ia / ib multicenter open - label clinical study established 10 mg twice per day as the recommended dose for cohort expansion and phase ii with near - maximal inhibition of phosphorylated akt and partial inhibition of phosphorylated 4ebp ( munster pn , et al : j clin oncol 34 , 2016 [ suppl ; abstr 2505 ] )  . 
because this dose has never been combined with rt , the treatment arm will start with a safety lead - in with the combination before expansion to the full phase ii setting . abemaciclib retinoblastoma ( rb ) protein is a key tumor suppressor that inhibits progression through the g1 checkpoint ( sherr cj : science 274 : 16721677 , 1996 )  . 
abemaciclib is a highly specic atp - competitive cdk4 / 6 inhibitor that induces reversible g1 phase cell - cycle arrest in rb - procient tumor models and is approved for hormone receptorpositive , human epidermal growth factor receptor 2 ( her2 ) negative advanced or metastatic breast cancer . orally dosed abemaciclib achieved brain exposures in excess of the concentrations required for cdk4 / 6 inhibition in an orthotopic rat gbm model and signicantly increased survival alone or in combination with tmz ( raub tj , et al : drug metab dispos 43 : 1360 - 1371 , 2015 )  . 
neratinib , an orally available potent irreversible small - molecule panerbb family tyrosine kinase inhibitor that targets the intracellular tyrosine kinase domains in egfr , is approved for her2 - positive breast cancer ( martin m , et al : lancet oncol 18 : 1688 - 1700 , 2017 ; cancer discov 7 : of1 , 2017 ) 39 and has shown activity in controlling and delaying cns progression of breast cancer metastases ( awada a , et al : jama oncol 2 : 1557 - 1564 , 2016 )  . 
in preclinical gbm studies , neratinib was shown to selectively cause cell death in cell lines harboring genetic activation of egfr and was more effective than other egfr inhibitors in lines harboring the extracellular domain mutations seen in gbm ( vivanco i , et al : cancer discov 2 : 458 - 471 , 2012 )  . 
neratinib has also been shown to exhibit potential for potent inhibition of amplied egfrvii and egfrviii in gbm patient - derived cell - line models ( francis jm , et al : cancer discov 4 : 956 - 971 , 2014 )  . 
neratinib is signicantly more potent than lapatinib in limiting the growth of primary gbm cell lines , and this increased potency is an attractive feature , given that negative clinical trials for lapatinib have been attributed to inadequate tumor concentrations of the drug ( vivanco i , et al )  . 
neratinib will be administered in place of tmz after standard concurrent rt / tmz . biomarkers prospective patients may have biomarker data already available from academic or commercial sources , or they may take advantage of a companion consortium ( abc2 allele consortium ) that generates free portable genotyping data using whole - exome sequencing and copy array testing performed in a clinical laboratory improvement amendmentscertied clinical laboratory for patient use in clinical trials . 
the biomarkers determined are as follows : egfr positive dened as patients with egfr amplication or mutation ; pi3k positive dened as patients with pik3ca mutation / amplication , pik3r1 mutation , akt3 amplication , pik3c2b  . 
one copy gain , or pten dual allele inactivation through either homozygous deletion or deletion plus an inactivating mutation ; and cdk positive dened as patients with rb1 wild type and cdk4 amplication , cdk6 amplication , or cdkn2a or cdkn2b  . 
one copy loss , or cdkn2a or cdkn2b one copy loss plus an inactivating mutation . for amplications listed , the genotyping report must state clear gene amplication and not gain , which is typically greater than a log2 ratio of + 2.0. 
copy number losses would be values of , 0.3 , and more than single copy deletions are inferred relative to baseline for the chromosome on which they are located ( eg , single copy chromosome 9 loss with additional loss of cdkn2a / b below this level in focal region )  . 
ve prior events reported in cosmic or are well - established hotspots known to be activating or inactivating mutations through experimental data or novel mutations that are predicted to be clearly inactivating , such as nonsense and frameshift mutations . 
heterozygous germline mutations in brca1 or brca2 confer up to an 85% lifetime risk of breast and a 15% to 40% risk of ovarian cancer , and they significantly increase the risk of pancreatic , prostate , and male breast cancers.1 tumors in these patients have often lost the wild - type allele and therefore are hr deficient . 
in the absence of a functional copy of the brca gene that maintains dna integrity , the use of error - prone , nonhomologous end - joining repair mechanisms leads to an accumulation of genetic aberrations and promotes carcinogenesis.2 inhibition of poly ( adp - ribose ) polymerase ( parp ) induces synthetic lethality in cells with brca1 or brca2 deficiency , and clinical trials of parp inhibitors have demonstrated responses in brcamutated breast and ovarian cancers.3 the bestdescribed mechanisms of resistance to platinum agents and parp inhibitors in brca1 or brca2 carriers with ovarian cancer are secondary mutations that restore the open reading frame or reversion mutations that restore the wild - type protein.4 , 5 , 6 these mutations are present in more than 40% of recurrent platinum - resistant ovarian cancers and are more common in women with recurrent ovarian carcinoma who were previously treated for breast cancer3 , 6 . 
minimal data exist about resistance to single - agent parp inhibitor therapy in women with breast cancer.7 we report a case of a brca2 mutation carrier who received single - agent parp inhibitor therapy and had subsequent resistance conferred by a reversion mutation identified by targeted capture and massively parallel sequencing . carcinoma of the right breast with multiple positive regional lymph nodes , for which she underwent a mastectomy and axillary node dissection and received adjuvant chemotherapy with fluorouracil , epirubicin , andcyclophosphamidefollowed by tamoxifen for 5 years . 
additional details of her initial care are not available , and cancer surveillance was not performed . after presentation at age 72 with back pain , workup identified a left breast mass with extensive metastatic disease to the bone . 
biopsy of the breast mass confirmed a new primary invasive ductal carcinoma that stained positive for estrogen receptor and progesterone receptor expression and negative for her2 / neu . her disease was staged as ct4an2m1 , and she started anastrazole monotherapy . 
 genomic dna isolated from peripheral blood to evaluate for germline mutations in brca1 and brca2.8 the uw - oncoplex assay ( laboratory medicine , university of washington ) was used to perform whole - exome deep sequencing and copy number variation analysis to identify somatic mutations in dna isolated from formalin - fixed , paraffinembedded tumor tissue.8 , 9 neoplastic cellularity was assessed by estimating the fraction of neoplastic to nonneoplastic nuclei on a hematoxylin and eosin stained section by a trained pathologist . 
predicted allelic frequency for the retained alleles of heterozygous germline variant of brca2 ( and reference single nucleotide polymorphism [ snp ] 2126042 ) was calculated with the following formula : [ ( tumor percentage ) + ( nontumor percentage ) ] 4 [ ( tumor percentage ) + 2 ( nontumor percentage ) ]  . 
predicted allelic frequency for the wild - type brca2 ( and reference snps 1799943 , 1799955 , and 1801406 ) was calculated as 100 2 the predicted allelic frequency of the variant . the fred hutchinson cancer research center consortium institutional review board approved this study . 
the reference snps were mapped to separate brca2 alleles with a predicted germline allelic frequency of approximately 50% ( table 1 )  . the pre - veliparib sample ( a bony lesion ) had a lower neoplastic cellularity ( 25% ) than the postveliparib sample ( chest wall ; 78% )  . 
the variant allele frequency of rs2126042 , present on the same copy of the mutated brca2 allele , was 60% in the preand 92% in the post - treatment sample . 
the allelic frequency of mutated brca2 in the pre - treatment sample is consistent with the loss of heterozygosity of the wild - type allele ( table 1 ; fig 1 )  . 
in the posttreatment sample , the marked discrepancy in the allelic frequency of the mutated brca2 ( 50% ) and rs126042 ( 92% ; both expected to be on the same allele ) , along with the low allelic frequency of other heterozygous germline snps ( predicted frequency , approximately 18% ) present on different copies of the alleles , strongly supports the restoration of wildtype brca sequence on the mutated allele ( table 1 )  . these collective findings suggest a reversion of the brca2 frameshift deletion mutation on the mutant allele during treatment ( fig 1 )  . 
in the lymphocytes ( germline ) , the wild - type brca2 allele and the heterozygous reference single nucleotide polymorphisms ( snps ) rs1799943 , rs1799955 , and rs1801406 were detected , along with the brca2 c.9097dup and a heterozygous snp , 2126042 . 
this method greatly simplifies the detection of such events and has important implications for the clinical care of patients with brca - mutant disease . we predict that similar phenomena may be sensitively identified earlier , before disease progression , with new platforms that incorporate next - generation sequencing to circulating tumor dnaso - called liquid biopsies . we conclude that the somatic reversion mutation was the mechanism of resistance to parp inhibitor and was responsible for progression during therapy . 
in the germline sample , the wild - type brca2 allele and the heterozygous reference single nucleotide polymorphisms ( snps ) rs1799943 , rs1799955 , and rs1801406 were detected together , along with the brca2 c.9097dup and a heterozygous snp rs2126042 . 
gadi stock and other ownership interests : sengine precision medicine research funding : genentech / roche ( inst ) affiliations all authors , university of washington ; kalyan banda and v.k. 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . j mol diagn 16 : 56 - 67 , 2014 10 . 
computed tomography ( ct ) scan with ( a ) the index lesions in the breast ( arrows ) before parp inhibitor and ( b ) 5 months later , which demonstrates decreased volume of disease . 
the absolute numbers of variant alleles and total number of alleles are in parentheses . mutations in tp53 , depdc5 , plk2 , and tacc3 are present in both preand post - treatment biopsies but are enriched in the post - treatment sample . 
 high response to cetuximab in a patient with egfr - amplied heavily pretreated metastatic triple - negative breast cancer renaud sabatier , md , phd1 , 2 ; marc lopez , phd1 ; arnaud guille , msc1 ; emilien billon , md1 ; nadine carbuccia , msc1 ; s everine garnier , phd1 ; jos e adelaide , msc1 ; jean - marc extra , md2 ; maria - antonietta cappiello , md2 ; emmanuelle charafe - jauffret , md , phd1 ; jihane pakradouni , phd2 ; patrice viens , md1 ; anthony gonalves , md , phd1 ; max chaffanet , phd1 ; daniel birnbaum , md , phd1 ; and franois bertucci , md , phd1 introduction represent triple - negative breast cancers ( tnbcs ) 15% of breast cancers , 1 and patients with tnbc have an increased likelihood of distant recurrence and death compared with women with estrogen receptor and / or human epidermal growth factor receptor 2 positive tumors.2 although early tnbcs display frequent epidermal growth factor ( egfr ) overexpression , 3 incidence of egfr gene alteration is not clearly known in metastatic samples , and egfrtargeted agent results have been disappointing for this subtype , whether used alone or with chemotherapy.4 , 5 receptor cetuximab is a chimeric monoclonal antibody ( mab ) specic for egfr ; it interacts with egfr and blocks the downstream pathway , which interferes with the proliferation of cancer cells . 
however , their place in tnbc treatment is unclear , because early clinical studies showed contradictory results.4 , 6 we identied a patient with progressive metastatic tnbc resistant to chemotherapy and immunotherapy . 
however , disease progression occurred 8 months after treatment initiation . we explored all the tumor samples we had from this patient to identify resistance mechanisms both at the genomic and protein levels . 
she received anthracyclines and taxane - based neoadjuvant chemotherapy and underwent mastectomy , which revealed a residual 6cm triple - negative inltrating ductal carcinoma as well as residual axillary lymph node involvement ( 9n + / 14 )  . treatment was completed by chest wall and lymph node irradiation . 
whole genomic proles were established by the array comparative genomic hybridization approach for the precetuximab biopsy ( blue line ) , postcetuximab biopsy ( brown line ) , and patient - derived xenograft ( pdx ) sample ( red line )  . 
from left to right , chromosome 7 ideogram with its genomic prole showing 7p11.2 amplication , with focus on the 52 , 072 , 97957 , 560 , 519 ( 5.48 mb ) amplied region that includes egfr gene . 
from left to right , chromosome 19 ideogram with its genomic prole showing 19q12 amplication , with focus on the 27 , 571 , 467 - 33 , 059 , 007 ( 5.48 mb ) amplied region that includes ccne1 gene . 
a new subcutaneous tumor biopsy was performed and analyzed by whole - genome array comparative genomic hybridization ( cgh ; highresolution 4 180 , 000 cgh microarray ; agilent technologies , massy , france ) and targeted next - generation sequencing ( nextseq500 ; illumina , san diego , ca ) as previously described.7 array cgh analysis identied focal amplication within the 7p12 region ( fig 2 ) , with  . 
before genomic results were known , the patient received additional therapies , including weekly paclitaxel , vinorelbine , and a programmed death - 1 inhibitor ( cpdr001x2101 trial ) , with subsequent visceral and cutaneous progression . in february 2017 , we proposed initiation of cetuximab therapy ( 250 mg / m2 per week ) as seventh - line therapy for metastatic disease . 
however , one of the main tyrosine kinase domains of egfr ( y1068 ) had lost its phosphorylation after progression , suggesting that egfr was no longer activated ( figs 4a and 4b )  . 
in contrast , akt phosphorylation was not modied after cetuximab treatment , suggesting no downstream activation of the phosphatidylinositol 3 - kinase in addition , sequencing ( pi3k ) / akt pathway ( fig 4a )  . showed a loss - of - function mutation of nf1 , absent in the precetuximab sample , suggesting that the mitogen - activated protein kinase ( mapk ) pathway might have been involved in cetuximab resistance . because she consented to participate in our permed - 01 trial , the patient also provided her consent to publication of data related to this prospective study . 
after a molecular tumor board decision , all clinical procedures were performed as routine clinical management . discussion we report here the case of a patient with heavily pretreated metastatic tnbc with egfr amplication who experienced a dramatic response to cetuximab as seventh - line treatment for metastatic disease . 
failure of egfr inhibitors in patients with tnbc may result not only from a lack of molecular data in the metastatic setting , but also from the misidentication of the right predictive molecular alteration . investigations exploring egfr mabs in breast clinical cancer have only correlated treatment efcacy with protein expression . 
first , immunohistochemistry is not excellent ( specicity , 78% ; sensitivity , 97% ) when compared with in situ hybridization.10 second , most cases of breast cancer with egfr overexpression involved gene polysomy instead of real gene amplication . 11 , 12 the biologic impact of these two alterations could be different , and amplied cases have been described as having better prognoses , 13 whereas polysomic cases seem to have poor outcomes.11 this prognostic impact could be correlated with treatment efcacy and higher sensitivity to egfr inhibitors.14 to evaluate how many patients with breast cancer could be candidates for this treatment , we explored egfr amplication incidence in primary breast tumors as well as in metastatic samples from the cancer genome atlas15 and genomics evidence neoplasia information exchange16 databases . 
cell lysates were separated on 7.5% sodium dodecyl sulfate polyacrylamide gel electrophoresis . loading charge was ve times more in the postcetuximab sample , taking into account tumor cellularity ( 20% )  . 
p - egfr ( y1068 ) expression was detectable in the precetuximab ( here is shown a sample from a patient - derived xenograft [ pdx ] model developed from the precetuximab biopsy ) and not in the postcetuximab sample , even after extended exposure time . 
this suggests that this subtype is more likely to benet from egfr inhibitors . most randomized clinical trials assessing egfr mab efcacy in breast cancer were not designed to explore treatment impact according to biologic features . 
in the tbcrc001 phase ii trial comparing cetuximab monotherapy with a combination of carboplatin and cetuximab for metastatic tnbc , survival was poor in both arms.17 gene expression analyses showed that cetuximab was active in the egfr pathway in a few cases . 
another phase ii trial , which compared cisplatin with cisplatin plus cetuximab in the same setting and did not include biomarker analysis , did not show overall response improvement with egfr inhibition.4 in a cohort of patients with egfr - overexpressing tnbc treated with a taxane and cetuximab doublet , median overall survival was 12 months.6 nevertheless , no correlation between response and egfr amplication status was investigated . in phase ii trials exploring the impact of cetuximabor panitumumab - based combinations in the neoadjuvant setting , 18 , 19 treatment table 1 . 
other alterations favoring secondary resistance to egfr inhibitors , such as downstream alterations in the pi3k / akt / mammalian target of rapamycin pathway , including kras , pi3kca , and akt mutations and pten deletions , were not observed in our patients tumor sample.31 , 32 other mechanisms of resistance were not fully explored in our work , such as amplication of met , which is involved in resistance to egfr inhibitors.33 another point we could not explore was whether the combination of egfr inhibitors and cytotoxic chemotherapies may be more efcient than monotherapies , as recommended for metastatic colorectal and head and neck cancers . 
efcacy of cetuximab and panitumumab as monotherapies is indeed poor in these contexts.34 , 35 regarding tnbc , platinum compounds are presumably efcient partners that may deserve to be explored , because tnbc tumors harbor frequent dna repair alterations.36 in conclusion , most clinical studies exploring anti - egfr mabs have been disappointing . 
our case of tnbc and recent data in cancers other than breast cancer suggest we should give more consideration to egfr amplication than single immunohistochemical protein expression in selecting patients with metastatic tnbc for clinical trials evaluating anti - egfr agents . 
mechanisms of resistance remain unclear in responders to egfr inhibitors . efcacy seemed to be linked not only to egfr protein expression but also to a high cd8 + / foxp3 - positive tumorinltrating lymphocyte ratio , suggesting a potential impact of antibody - dependent cellular cytotoxicity activation.20 , 21 egfr amplication was associated with clinical response to cetuximab in colon cancer , squamous cell lung cancer , and refractory gastroesophageal adenocarcinoma.22 - 24 egfr copy number was also described as correlating with egfr tyrosine kinase inhibitor ( tki ) efcacy in a metaanalysis including  . 
however , such a combination is unlikely to be developed in the clinical setting because of skin and digestive toxicities . results that would improve our understanding of mechanisms underlying secondary resistance to cetuximab are lacking . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . anthony gonalves research funding : merck sharp & dohme ( inst ) , bristol - myers squibb ( inst ) , novartis ( inst ) , cascadian therapeutics ( inst ) , nektar ( inst ) , boehringer ingelheim ( inst ) , eli lilly ( inst ) , abbvie ( inst ) , roche / genentech ( inst ) , astrazeneca ( inst ) , roche ( inst ) travel , accommodations , expenses : pzer , novartis , roche / genentech , celgene no other potential conicts of interest were reported . acknowledgment we thank the datacenter it and scientic computing of the centre de recherche en canc erologie de marseille , which provided computing resources for this study . references foulkes wd , smith ie , reis - filho js : triple - negative breast cancer . 
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levva s , kotoula v , kostopoulos i , et al : prognostic evaluation of epidermal growth factor receptor ( egfr ) genotype and phenotype parameters in triple - negative breast cancers . 
el guerrab a , bamdad m , kwiatkowski f , et al : anti - egfr monoclonal antibodies and egfr tyrosine kinase inhibitors as combination therapy for triple - negative breast cancer . 
carey la , rugo hs , marcom pk , et al : tbcrc 001 : randomized phase ii study of cetuximab in combination with carboplatin in stage iv triple - negative breast cancer . 
multicentric neoadjuvant phase ii study of panitumumab combined with an anthracycline / taxane based chemotherapy in operable triple negative breast cancer : identication of biologically - dened signatures predicting treatment impact . 
roberti mp , barrio mm , bravo ai , et al : il - 15 and il - 2 increase cetuximab - mediated cellular cytotoxicity against triple negative breast cancer cell lines 21 . 
roberti mp , juli a ep , rocca ys , et al : overexpression of cd85j in tnbc patients inhibits cetuximab - mediated nk - cell adcc but can be restored with cd85j 22 . 
moroni m , veronese s , benvenuti s , et al : gene copy number for epidermal growth factor receptor ( egfr ) and clinical response to antiegfr treatment in 23 . 
herbst rs , davies am , natale rb , et al : efcacy and safety of single - agent pertuzumab , a human epidermal receptor dimerization inhibitor , in patients with non 24 . 
zhang x , zhang y , tang h , et al : egfr gene copy number as a predictive / biomarker for patients with non - small - cell lung cancer receiving tyrosine kinase inhibitor treatment : a systematic review and meta - analysis . 
mei z , shao yw , lin p , et al : smad4 and nf1 mutations as potential biomarkers for poor prognosis to cetuximab - based therapy in chinese metastatic colorectal i10 - i19 , 2018 ( suppl ) cancer patients . 
personeni n , hendlisz a , gallez j , et al : correlation between the response to cetuximab alone or in combination with irinotecan and the activated / phosphorylated epidermal growth factor receptor in metastatic colorectal cancer . 
li `evre a , ouine b , canet j , et al : protein biomarkers predictive for response to anti - egfr treatment in ras wild - type metastatic colorectal carcinoma . 
therkildsen c , bergmann tk , henrichsen - schnack t , et al : the predictive value of kras , nras , braf , pik3ca and pten for anti - egfr treatment in metastatic colorectal cancer : a systematic review and meta - analysis . 
yang z , yang n , ou q , et al : investigating novel resistance mechanisms to third - generation egfr tyrosine kinase inhibitor osimertinib in non - small cell lung 33 . 
bean j , brennan c , shih j - y , et al : met amplication occurs with or without t790m mutations in egfr mutant lung tumors with acquired resistance to getinib cancer patients . 
segelov e , thavaneswaran s , waring pm , et al : response to cetuximab with or without irinotecan in patients with refractory metastatic colorectal cancer harboring the kras g13d mutation : australasian gastro - intestinal trials group icecream study . 
couch fj , hart sn , sharma p , et al : inherited mutations in 17 breast cancer susceptibility genes among a large triple - negative breast cancer cohort unselected for family history of breast cancer . 
however , the clinical application of these targeted drugs and diagnostics often remains unclear . however , this approach is not newdoctors have been trying to provide personalized care with high precision for centuries . 
for example , during the last 150 years , virchow developed microscopic pathology , roentgen introduced radiographic imaging , and bloom and richardson proposed a tumor grading scale ; all represented major leaps forward in personalized medicine that we still apply.1a - 1e more recent examples include tests for estrogen receptor in breast cancer to guide endocrine therapy and evaluation of the cd20 antigen on b - cell lymphomas to guide the use of anti - cd20 monoclonal antibodies . so , whats new ? we have new and exciting tools that rival those giants on whose shoulders we stand . 
however , to deliver personalized medicine as precisely as possible , we need high levels of evidence that use of these new therapies and diagnostic tests does , in fact , improve patient care . we agree with the skeptics in oncology who question the benefit of precision oncology , but we maintain that the answer is not to declare it all hype and walk away but to continue to learn how best to use it . 
rather than hope for luck , clinicians should continue to use the scientific method to make evidence - based decisions . in may 2013 , journal of clinical oncology published a special series on precision oncology . the success of this special series led asco to recognize both the plethora of research that is occurring in this field and the need to disseminate this information effectively to the oncology community . 
the special issue of jco featured articles that outlined the current and emerging technologies for tumor genomic profiling , 1f ways to build personalized medicine infrastructure at major cancer centers , 2 and various applications of genomic profiling for different cancer diagnoses . 
it will also provide researchers and clinicians with a reliable source of high - quality precision oncology research , reviews , and commentary essential to real - world cancer care . 
in addition to original clinical research , the journal will publish articles about key care delivery issues , such as value , quality , and cost - effectiveness , and about ethical , legal , and social considerations to inform clinical practice and shape this rapidly evolving field . we are thrilled to have james m . 
ford is a professor of medicine ( oncology ) , pediatrics ( medical genetics ) , and genetics and is the director of the stanford cancer genetics clinic and the cancer genomics program at the stanford cancer institute . 
hayes , university of michigan comprehensive cancer center , ann arbor , mi ; and julie vose , university of nebraska medical center , omaha , ne corresponding author : daniel f . 
 genetic targets for personalized targeted therapies in breast and gastrointestinal cancer as well as in examination of the role of dna repair in the treatment and prevention of cancer in families and populations . 
with the commencement of the targeted agent and profiling utilization registry ( tapur ) study , asco aims to describe both the safety and the efficacy of targeted anticancer drugs to catalog genomic profiling tests and to learn about the utility of registry data . 
in addition , with the launch by asco of cancerlinq , oncologists will have access to a massive database of treatment options and results of those treatments from millions of patient records . 
vose consulting or advisory role : bio connections research funding : celgene ( inst ) , genentech ( inst ) , incyte ( inst ) , janssen biotech ( inst ) , acerta pharma ( inst ) , kite pharma ( inst ) , seattle genetics ( inst ) , novartis ( inst ) , amgen ( inst ) , bristol - myers squibb ( inst ) , allos therapeutics ( inst ) references 1a . 
hammond me , hayes df , dowsett m , et al : american society of clinical oncology / college of american pathologists guideline recommendations for immunohistochemical testing of estrogen and progesterone receptors in breast cancer . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
 circulating tumor dna in nonsmall - cell lung cancer : a primer for the clinician circulating tumor dna ( ctdna ) consists of short , double - stranded dna fragments that are released into the circulation by tumor cells . 
the assays noninvasive nature , ability to reflect intratumoral heterogeneity , short turnaround time , and ability to obtain serial samples make it an attractive option compared with traditional tissue biopsy tumor sequencing . 
currently , this technology is mostly being used for the detection of egfr mutations in patients with advanced nonsmall - cell lung cancer where tissue is inadequate to detect egfr mutations that drive acquired resistance , most notably egfr t790m . 
emerging uses include the incorporation of ctdna testing into primary diagnosis , treatment monitoring , detection of minimal residual disease , and detection of early - stage disease in screening populations . 
2017 by american society of clinical oncology introduction including tumors , shed short , several tissues , double - stranded dna fragments called cell - free dna ( cfdna ) into the circulation.1 - 3 certain conditions that cause tissue damage , such as myocardial infarction , trauma , and cancer , can result in increased concentrations of cfdna.3 the cfdna derived from tumors , known as circulating tumor dna ( ctdna ) , is a product of apoptosis and necrosis and is distinguished from other cfdna by the presence of somatic mutations representative of tumor biology absent in normal cells . 
90% of all dna present in the plasma.4 , 5 in patients with advanced nonsmall - cell lung cancer ( nsclc ) , ctdna detection rates that range from 80% to  . 
unlike acquired t790m resistance to egfr tkis , one dominant secondary mutation appears not to exist , and second - generation alk inhibitors have shown high response rates in patients previously treated with crizotinib regardless of the presence of secondary alk mutations , which makes the role of a repeat biopsy less clear.27 however , emerging data suggest that specific secondary resistance alk mutations have important therapeutic implications . 
in a study that detected egfr mutations by an ngs assay , the sensitivity for urine was 93% for t790m , 80% for l858r , and 83% for exon 19 deletions . 
in nine patients monitored while receiving the third - generation egfr inhibitor rociletinib , a rapid decrease in urine ascopubs.org / journal / po jco precision oncology 7 t790m was 70% , and the objective response rate and median progression - free survival ( pfs ) with osimertinib were similar in patients with t790mpositive plasma or tumors.10 this finding suggests that with the use of ctdna testing , many patients can avoid a biopsy for t790m genotyping . 
however , because of the 30% false - negative rate of plasma genotyping , those with t790m - negative plasma still need to undergo tumor biopsy to determine the presence or absence of t790m.10 in addition to cases where ctdna is not detectable , tissue testing retains value in certain resistance mechanisms , such as small - cell transformation . thress et al24 performed ngs of cfdna from seven patients with t790m - mutated advanced lung cancer who had developed resistance to osimertinib and detected an acquired egfr c797s mutation . 
 t790m levels was observed by day 21.31 in a study of patients with t790m positivity , response was similar whether t790m status was identified by tissue , plasma ( through beaming ) , or urine ( through ngs ) .32 these data suggest that plasma and urine egfr analyses complement tissue biopsy specimen analysis in nsclc . brain metastasis is found in up to 40% patients with nsclc , 33 and ctdna analysis of patients with brain tumors has revealed either the absence or very low levels of tumor dna possibly as a result of the blood - brain barrier.34 one study used hybridization capturebased sequencing and ddpcr to characterize ctdna in csf of patients with brain lesions ( including brain metastasis from lung cancer ) and compared it with plasma ctdna.35 the authors concluded that csf ctdna has a significantly higher sensitivity than plasma for cns genomic alterations like egfr , pten , esr1 , idh1 , erbb2 , and fgfr2 and can be used to detect brain tumor mutations and monitor brain tumor progression ( sensitivity of ctdna was 58% v 0% in csf and plasma , respectively , in cns - restricted disease )  . 
hata et al37 investigated the response to osimertinib in 10 patients with leptomeningeal disease and showed that the drug might be more effective in csf of patients with t790m positivity than in those without csf t790m positivity . multigene testing as the number of genomic targets with matched therapies grows , the national comprehensive cancer network guidelines for nsclc recommend expanded genomic testing , including for egfr , alk , erbb2 , braf , met , ros1 , and ret.5 , 15 , 38 testing for all these alterations in addition to histopathologic and immune biomarker assessment pose a challenge when tissue biopsy samples are insufficient . 
in a study of patients with advanced nsclc , a tissue biopsy specimen with sufficient quality and quantity of dna for ngs was unobtainable for 52 ( 51% ) of 102 patients.7 two studies used ngs - based ctdna assays to evaluate , with high overall accuracy , somatic genomic profiles in patients with advanced nsclc  . 
15 , 000 patients with advanced - stage cancer with a concordance of 87% with matched tumor samples that increased to 98% when plasma and tissue testing was done , 6 months apart . 
the study detected actionable mutations in biopsy specimens with insufficient tissue ( alk fusion , egfr or braf activating mutations ) and with actionable resistance mutations at the time of progression ( met amplification or egfr t790m ) as well as in undergenotyped tumors ( braf v600e , or erbb2 indel )  . identification of nontargetable oncogenic drivers , such as kras mutations , that preclude the presence of other targetable alterations also guides clinicians to rapidly initiate alternative therapies , such as chemotherapy or immunotherapy.5 the detection of variants in other genes may lead to the off - label use of fda - approved therapies or enrollment in clinical trials of new therapeutic agents.7 several combinations of targeted therapies are based on resistance mechanisms and are being evaluated in lung cancer ( eg , mek and pi3k inhibitors in combination with egfr tkis ) , 41 which again underscores the need for real - time tumor genotyping to assess for resistance pathways . 
chabon et al43 identified several resistance mechanisms , including met , egfr , pik3ca , errb2 , kras , and rb1 , in patients with t790mmutated nsclc who received rociletinib . 
the study used cancer personalized profiling by deep sequencing ctdna analysis and found that 46% of patients ( 19 of 41 ) with t790m mutations had additional potential resistance mutations in the pretreatment plasma . 
this coexistence of different resistance mechanisms in the same patient may affect response to subsequent egfr tkis like rociletinib . treatment monitoring ctdna offers the possibility of serial testing for molecular monitoring of disease . 
 studies have demonstrated the predictive value of quantitative changes in egfr mutations in ctdna at various time points during tki treatment.1 a prospective analysis to validate ddpcr for the detection of common egfr and kras mutations in patients with advanced nsclc demonstrated that patients with complete resolution of ctdna at either 2 or 6 weeks after treatment exhibited a treatment discontinuation rate of 0% at the initial and 4% at the second imaging assessment . 
patients without complete resolution exhibited a treatment discontinuation rate of 33% at initial and 56% at second imaging . these patterns were postulated to correlate with radiographic response and emergence of acquired resistance.4 marchetti et al44 performed pcr and ultradeep ngs on serial plasma samples from 20 patients with advanced nsclc and known tissue and plasma egfr mutations before tki treatment . 
rapid responders who had at least a 50% decrease in plasma egfr copy number at 14 days had a greater mean percentage of tumor shrinkage than slow responders ( n = 6 ; 70% v 30% )  . 
a phase iii study evaluated egfr mutations in cfdna of patients randomly assigned to receive gemcitabine and platinum plus sequential erlotinib or placebo by using a cobas test.46 for patients treated in the erlotinib arm who were cfdna egfr positive at baseline , the disappearance of cfdna at cycle 3 was associated with significantly improved pfs ( hr , 0.38 ) and longer os ( hr , 0.45 ) compared with patients with persistence of cfdna egfr . the prognostic value of dynamic changes in ctdna has also been evaluated . 
additional studies are needed to evaluate end points such as pfs , os , and quality of life as a result of early detection of resistance . monitoring for minimal residual disease another potential application of ctdna is to evaluate for minimal residual disease ( mrd ) after curativeintent therapy , such as surgery and radiation.8 chaudhuri et al48 applied cancer personalized profiling by deep sequencing to detect ctdna in preand post - treatment blood samples from 41 patients with nonmetastatic lung cancer treated with chemoradiation , radiation , or surgery . 
these patients positive for mrd had a significantly worse outcome than patients without detectable ctdna mrd within 4 months of definitive treatment ( 3 - year freedom from progression , 0% v 92% [ hr , 38 ] ; 3 - year os , 8% v 75% [ hr , 12 ] )  . these data suggest that patients with residual ctdna after definitive treatment will be enriched for those who will ultimately develop recurrence . 
ctdna detection might facilitate the development of clinical trials that evaluate the escalation of therapy for patients at high risk for recurrence and the de - escalation of therapy for patients without residual disease . role in early diagnosis / screening the role of ctdna in early - stage disease also is being studied . 
bettegowda et al34 evaluated the ability of ctdna to detect tumors in patients with various malignancies at various clinical stages . forty - seven percent of patients with stage i cancers ( n = 49 ) had detectable ctdna , with the fraction of patients with detectable ctdna being 55% , 69% , and 82% for those with stage ii , iii , and iv cancers , respectively.34 trials are under way to assess the feasibility and utility of ngsbased ctdna to detect early - stage cancers in high - risk patients ( clinicaltrials.gov identifier : nct02612350 ; also project lunar48a )  . 
 mutation of interest in the patients tumor needs to be known to send for appropriate genomic panels . ctdna may be detectable before radiographically detectable disease , which raises the issue of managing such patients . 
nevertheless , early cancer detection remains a promising new avenue for ctdna that needs additional research . ctdna in the era of immune checkpoint therapy in the era of immune therapy for advanced nsclc , a key issue is the elucidation of a biomarker that can predict response and monitor disease . 
tumor dna sequencing has been shown to be a surrogate for total mutation burden , which predicts response and pfs with antiprogrammed death 1 inhibitors like pembrolizumab.49 however , total mutation burden analysis has been investigated only in tumor tissue , and a better understanding of ctdna is required before it can be applied for this purpose . lipson et al50 analyzed the ctdna of 12 patients with metastatic melanoma who underwent treatment with checkpoint inhibitors for the presence of hotspot somatic mutations in braf , ckit , nras , and tert by using beaming . 
hence , a negative result could signify that the tumor is not actively shedding ctdna , the patients disease is adequately controlled by therapy , or somatic variants either were not covered or were below the detection limit for the assay.7 in addition , any negative test result will need to be viewed in the overall context of ctdna and other molecular results . 
for example , in a patient with an egfr - mutated nsclc in the setting of acquired resistance , a negative egfr t790m test result is more likely to be a true negative if the original egfr mutation was detected with a significant allele frequency versus if the ctdna test did not identify either mutation . confidence in a positive test result extremely high analytic specificity and a positive predictive value that approaches 100% make false positives unlikely , so if a mutation is detected , it can be relied on as a true result . 
as expected , the allelic fraction of variants detected in ctdna is usually much smaller than that in tissue dna given that tumor - derived dna may be more diluted in the blood than in the tissue.7 the rare false positive result ( particularly t790m ) in plasma may be indicative of tissue heterogeneity in which the mutation was not identified but is present in tissue , which may be due to the timing of the biopsy and the location of the biopsy needle in the tumor . 
the only definitive method to clinically validate that the mutations detected in plasma are an accurate molecular proxy of disease biology in the context of it being absent in tissue is to correlate them with response to targeted inhibition . in the case of mutational events that are exclusive to certain types of cancers ( eg , egfr exon 19 deletion to nsclc ) , confidence of a positive result is higher than in genes that can be mutated in a variety of settings ( eg , tp53 )  . 
for instance , a small allelic fraction tp53 mutation in ctdna can originate from many sources ( eg , myelodysplastic syndrome ) , and in such cases , confidence is increased if the same mutation also has been detected in tumor . detection of concurrent malignancy / germline alterations the testing of cfdna will detect all dna that sheds into the circulation , and some findings may not be expected in the tumor of origin , may not match tumor tissue dna results , and may affect genes that are mutated in different tumor types ( eg , tp53 )  . 
a potential for detection of incidental hematologic malignancies exists , which , naturally , have high tumor burden in the blood , and results can be confounded by foreign dna , such as after transfusion or organ transplantation . another issue similar to what is seen with tissue genotyping is that one needs to be cautious about distinguishing somatic ( tumor ) versus germline alterations because germline dna is not analyzed in parallel . 
any mutation that affects genes implicated in familial syndromes should be considered specifically ( eg , brca ) , and mutations with high allele frequency ( between 30% and 70% ) should raise the possibility of being potentially associated with heterozygous germline mutation syndromes . in conclusion , tissue biopsy remains essential at least for primary diagnosis because tissue yields information about morphology , tumor type , site of origin , and the immune microenvironment . 
for instance , erbb2 ( her2 ) copy number amplification in nsclc does not predict tki response like it does in breast cancer.5 currently best validated in egfr - mutated lung cancer for primary molecular diagnosis and for egfr t790m testing , ctdna has proven to have excellent utility as a complement to tissue - based testing . 
singh no relationship to disclose xiaoling guo no relationship to disclose haiying cheng honoraria : astrazeneca , boehringer ingelheim , clovis oncology benjamin levy honoraria : genentech consulting or advisory role : eli lilly , boehringer ingelheim , genentech , roche , astrazeneca , celgene , pfizer , merck speakers bureau : eli lilly , genentech , roche balazs halmos consulting or advisory role : astrazeneca , boehringer ingelheim , celgene , genentech , roche , pfizer , eli lilly , foundation medicine research funding : merck , astrazeneca , mirati therapeutics , boehringer ingelheim , roche , genentech , ariad pharmaceuticals affiliations aditi p . 
singh , haiying cheng , xiaoling guo , and balazs halmos , montefiore medical center , bronx , ny ; and benjamin levy , johns hopkins sidney kimmel comprehensive cancer center at sibley memorial hospital , washington , dc . references oncologist 21 : 1121 - 1130 , 2016 1 . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - small - cell lung cancer . 
li t , kung hj , mack pc , et al : genotyping and genomic profiling of non - small - cell lung cancer : implications for current and future therapies . 
luo j , shen l , zheng d : diagnostic value of circulating free dna for the detection of egfr mutation status in nsclc : a systematic review and meta - analysis . 
kimura h , suminoe m , kasahara k , et al : evaluation of epidermal growth factor receptor mutation status in serum dna as a predictor of response to gefitinib ( iressa )  . 
douillard jy , ostoros g , cobo m , et al : gefitinib treatment in egfr mutated caucasian nsclc : circulating - free tumor dna as a surrogate for determination of egfr status . 
mao c , yuan jq , yang zy , et al : blood as a substitute for tumor tissue in detecting egfr mutations for guiding egfr tkis treatment of nonsmall cell lung cancer : a systematic review and meta - analysis . 
liu y , liu b , li xy , et al : a comparison of arms and direct sequencing for egfr mutation analysis and tyrosine kinase inhibitors treatment prediction in body fluid samples of non - small - cell lung cancer patients . 
wang j , wang b , chu h , et al : intrinsic resistance to egfr tyrosine kinase inhibitors in advanced non - small - cell lung cancer with activating egfr mutations . 
sequist lv , goldman jw , wakelee , ha , et al : efficacy of rociletinib ( co - 1686 ) in plasma - genotyped t790mpositive non - small cell lung cancer ( nsclc ) patients ( pts )  . 
zheng d , ye x , zhang mz , et al : plasma egfr t790m ctdna status is associated with clinical outcome in advanced nsclc patients with acquired egfr - tki resistance . 
thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . 
niederst mj , hu h , mulvey he , et al : the allelic context of the c797s mutation acquired upon treatment with thirdgeneration egfr inhibitors impacts sensitivity to subsequent treatment strategies . 
ihuegbu n , banks kc , fairclough sr , et al : non - invasive detection of crizotinib resistance in alk - rearranged lung adenocarcinoma directs treatment with next - generation alk inhibitors . 
wakelee ha , gadgeel sm , goldman jw , et al : epidermal growth factor receptor ( egfr ) genotyping of matched urine , plasma and tumor tissue from non - small cell lung cancer ( nsclc ) patients ( pts ) treated with rociletinib . 
barlesi f , gervais r , lena h , et al : pemetrexed and cisplatin as first - line chemotherapy for advanced non - small - cell lung cancer ( nsclc ) with asymptomatic inoperable brain metastases : a multicenter phase ii trial ( gfpc 07 - 01 )  . ann oncol 22 : 2466 - 2470 , 2011 34 . 
de mattos - arruda l , mayor r , ng ck , et al : cerebrospinal fluid - derived circulating tumour dna better represents the genomic alterations of brain tumours than plasma . 
sasaki s , yoshioka y , ko r , et al : diagnostic significance of cerebrospinal fluid egfr mutation analysis for leptomeningeal metastasis in non - small - cell lung cancer patients harboring an active egfr mutation following gefitinib therapy failure . 
hata a , nanjo s , okuda c , et al : osimertinib at 80 mg for refractory leptomeningeal metastases in t790m - positive egfr - mutant non - small cell lung cancer . 
zill oa , mortimer s , banks kc : somatic genomic landscape of over 15 , 000 patients with advanced - stage cancer from clinical next - generation sequencing analysis of circulating tumor dna . 
canale m , petracci e , delmonte a , et al : impact of tp53 mutations on outcome in egfr - mutated patients treated with first - line tyrosine kinase inhibitors . 
marchetti a , palma jf , felicioni l , et al : early prediction of response to tyrosine kinase inhibitors by quantification of egfr mutations in plasma of nsclc patients . 
tseng js , yang ty , tsai cr , et al : dynamic plasma egfr mutation status as a predictor of egfr - tki efficacy in patients with egfr - mutant lung adenocarcinoma . 
mok t , wu yl , lee js , et al : detection and dynamic changes of egfr mutations from circulating tumor dna as a predictor of survival outcomes in nsclc patients treated with first - line intercalated erlotinib and chemotherapy . clin cancer res 21 : 3196 - 3203 , 2015 47 . 
karachaliou n , mayo - de las casas c , queralt c , et al : association of egfr l858r mutation in circulating free dna with survival in the eurtac trial . 
lipson ej , velculescu ve , pritchard ts , et al : circulating tumor dna analysis as a real - time method for monitoring tumor burden in melanoma patients undergoing treatment with immune checkpoint blockade . 
pediatric methylation data were also compared systematically with the adult acc cohort from the cancer genome atlas ( tcga )  . results two pediatric act methylation groups were identied and showed differences in selected clinicopathologic and outcome characteristics . 
the a2 group was enriched for tp53 germline variants , younger age at onset , and favorable outcome . pediatric act methylation groups were maintained when international pediatric adrenocortical tumor registry cohort data were combined with tcga cohort data . 
when methylome ndings were combined with independent histopathologic review using the wieneke criteria , a high - risk population was identied with uniform fatal outcome . conclusion our results indicate dna methylation analysis can enhance current diagnostic algorithms . 
 clay et al context key objective risk stratication in pediatric adrenocortical tumors ( acts ) is challenging , because individual gene mutations and histomorphology do not reliably predict clinical risk . 
this study examined whether molecular subtypes of act could be detected using dna methylation proling and whether common act mutations differentially segregate into molecular groups . furthermore , we evaluated the prognostic signicance of molecular groups alone and in combination with histomorphologic risk models . knowledge generated two methylation groups were detected , distinct from adult act and enriched for specic mutations . 
methylation group may serve to highlight a high - risk treatment population in future risk - adaptive clinical trial designs . interplay of multiple genetic lesions that accumulate during tumorigenesis.7 recent advances in adult adrenocortical neoplasia studies have revealed distinct methylation patterns in non - neoplastic , benign , and malignant act samples.12 aggressive behavior has been associated with both global hypomethylation13 and cpg - island methylator phenotype ( cimp ) .9 this was expanded on by zheng et al14 in a comprehensive analysis of adult accs as part of the cancer genome atlas ( tcga ) , where levels of cpg - island methylation ( designated cimp - low , - intermediate , or - high ) were associated with an increasingly poor outcome . 
studies on methylation patterns in the pediatric population are lacking . we performed dna methylation analyses on 48 newly diagnosed acts from the international pediatric adrenocortical tumor registry ( ipactr ) to evaluate for distinct groups with prognostic signicance . 
methods of registry accrual and the sampling process have been described previously.4 histopathologic and clinical data were tabulated from existing databases . the outside diagnosis was recorded as initial clinical diagnosis for the purposes of this study . 
pathology central review was performed blinded to analysis data and included evaluation of wieneke criteria5 in all patients , with a subsequently assigned wieneke tumor classication ( scores : 0 - 2 , aca ; 3 , act with uncertain malignant potential [ actump ] ; 4 - 9 , acc )  . 
a summary of all clinical data can be seen in the data supplement . normal adrenal samples were obtained from non - neoplastic surgical specimens and autopsy tissues . immunohistochemical and molecular analysis immunohistochemical staining was performed for p53 ( diluted 1 : 200 ; #z2029m ; zeta corp , sierra madre , ca ) , - catenin ( undiluted ; #760 - 4242 ; ventana , tucson , az ) , and atrx ( 1 : 200 ; #hpa001906 ; sigma , st louis , mo ) and scored as either wild - type pattern ( ie , scattered nuclear positivity for p53 , membranous or cytoplasmic staining for - catenin , and intact nuclear staining for atrx ) or mutant pattern ( ie , absent or diffuse nuclear positivity for p53 , nuclear positivity for - catenin , and loss of nuclear stain for atrx )  . 
ki - 67 staining ( 1 : 200 ; #m7240 ; dako , santa clara , ca ) was scored manually as the raw percentage of ki67positive tumor cells and as an estimate rounded to the nearest 10th percentile . 
mutational status of tp53 , ctnnb1 , and atrx was determined using a combination of whole - genome sequencing ( wgs ) , whole - exome sequencing ( wes ) , sanger sequencing , and multiplex ligationdependent probe amplication ( mlpa )  . 
 dna methylation proling of pediatric adrenocortical tumors instances , multimodality testing was performed , and overall testing included the following genes : tp53 mutational ( sanger , n = 48 ; wes , n = 9 ; wgs , n = 1 ) , ctnnb1 ( sanger , n = 48 ; wes , n = 9 ; wgs , n = 1 ) , and atrx ( mlpa , n = 28 ; wes , n = 1 ; wgs , n = 1 )  . methylation proling and copy number analysis methylome analysis was performed using the human innium methylationepic beadchip array ( illumina , san diego , ca ) on 250 - 500 ng of dna extracted from formalinxed parafn - embedded ( ffpe ) tissues . 
samples were handled in accordance with the illumina innium hd methylation assay protocol , as published.15 a detailed description of data processing and methylation analysis is presented in the appendix . 
the group - wise methylation states of cpg - island sites were analyzed by mapping the top 20 , 000 most variably methylated probes from the combined tcga and ipactr datasets . gene set enrichment analysis gene set enrichment analysis ( gsea ) was performed using the top 20 , 000 most variably methylated probes between the two pediatric act groups . 
differential methylation patterns were mapped to specic gene loci , which were then secondarily cross - referenced to published gene sets by using established protocols.17 , 18 for a detailed description , see the appendix . clinicopathologic correlation summary statistics were calculated for values by the methylation group . 
survival analysis was performed to investigate the association of overall survival with histologic diagnosis , wieneke classication , and act methylation group using the log - rank test and cox regression models ( appendix )  . 
all p values reported were 2 - tailed and considered signicant if p .05. results demographics the demographic and clinical characteristics of the 48 pediatric act samples are presented in table 1 . 
the entire histologic spectrum of pediatric acts was present as classied by the wieneke criteria : aca ( n = 23 ) , act - ump ( n = 5 ) , and acc ( n = 19 ) , with 18 ( 38% ) stage i tumors , 10 ( 21% ) stage ii tumors , 15 ( 31% ) stage iii tumors , and ve ( 10% ) stage iv tumors . methylation and chromosomal copy number analysis we performed methylation proling on 48 acts and 12 normal control pediatric adrenal samples . 
by both unsupervised t - distributed stochastic neighbor embedding ( t - sne ) analysis ( fig 1a ) and hierarchical clustering ( fig 1b ) , we identied three distinct clusters of samples . 
these two tumor groups were 94.26% reproducible in a thorough bootstrap evaluation19 , 20 ( appendix )  . we observed several recurrent segmental chromosomal cnvs in both groups , including 4q and + 9q as previously reported ( figs 1c and 1d ) .7 we also identied distinct differences among groups ( fig 1e ) , with fewer recurrent chromosomal - level gains in the a1 group ( appendix fig a3 )  . 
all tumors in the tcga cohort were carcinomas , and median age at diagnosis was 49 years.14 visualization with t - sne highlighted the previously appreciated a1 , a2 , and pediatric control groups . 
tcga samples roughly clustered into groups that correlated with the published cimp - l , cimp - i , and cimp - h groups , although these designations are somewhat ambiguous , and several overlapping patients can be seen in the t - sne plot ( fig 3a )  . 
copy number analysis highlighted distinct copy number proles in the cimp groups ( appendix fig a4 )  . to further evaluate the relationship between pediatric acts and adult acts , we evaluated the methylation state at cpg islands across the tumor groups . 
in the tcga cohort , we reafrmed the presence of the cimp groups with the following mean beta values ( listed as % - methylated probes [ cimp - h , 69% ; cimp - i , 50% ; cimp - l , 29% ] )  . 
 ( a ) unsupervised analysis of dna methylation data visualized by t - distributed stochastic neighbor embedding ( t - sne ) plot identied 2 methylation groups , a1 and a2 . 
ihc , immunohistochemistry ; ump , uncertain malignant potential . the ipactr cohort , the a1 group showed greater cpgisland methylation when compared with the a2 group and the control samples ( fig 3b ) but not to the level of the cimp - h phenotypic patients ( a1 , 38% ; a2 , 23% ; control , 21% )  . 
unlike the adult tumors , noncpg - island methylation did not follow the same pattern as cpg islands , and overall , the a1 group was globally hypomethylated . clinicopathologic correlation occurred primarily in children younger than 4 years of age , whereas the a1 group showed an even age distribution ( fig 1b ; appendix fig a2b )  . 
no association was seen for sex , gross features ( ie , the size and weight of the tumor ) , or histologic diagnosis . the two methylation groups showed differences in selected clinicopathologic characteristics ( table 2 )  . 
cpgisland hypermethylator phenotypes ( cimps ) are noted as high ( cimp - h ) , intermediate ( cimp - i ) , or low ( cimp - l )  . 
p values are based on computed means for each patient . however , after strictly applying the wieneke criteria at central pathology review , we found that overall survival differed signicantly according to diagnosis ( p = .013 ; fig 4 )  . methylation grouping strongly correlated with overall survival ( p , .0001 ) , and except for one child in the a2 group who died of a separate primary brain tumor , all deaths directly attributable to acts occurred in the a1 group ( fig 4 )  . 
overall , bic indicates there is a 99.2% probability that the best predictive model for survival includes methylation class as one of its predictor variables . discussion our study demonstrates the potential of dna methylation proling to enhance current classication schemas by identifying prognostically relevant molecular groups in the pediatric population . 
clinical , histologic , immunophenotypic , and molecular characteristics by methylation group ( continued ) methylation group group a1 group a2 vascular invasion , present vascular invasion , absent soft - tissue invasion , present soft - tissue invasion , absent necrosis , any , present necrosis , any , absent mitoses  . 
clinical , histologic , immunophenotypic , and molecular characteristics by methylation group ( continued ) methylation group group a1 group a2 atrx wild - type pattern mutant pattern ( loss of staining ) note . 
bold type indicates statistical signicance . abbreviations : hpf , high power elds ; ipactr , international pediatric adrenocortical tumor registry . * local stage ( i / ii ) compared against nonlocalized stages ( iii / iv )  . virilization alone compared with all other categories . .321 clay et al because a proportion of tumors yield an intermediate score ( wieneke score = 3 ) , and the criteria can be difcult to apply outside of specialized centers . 
these limitations make the search for alternative predictive biomarkers a priority , because this ambiguity represents a major hurdle to the implementation of risk - adapted therapies . there are several advantages dna methylation proling offers as a clinical assay . 
for example , relevant prognostic groups have been extracted from dna methylation data in osteosarcoma , a tumor type characterized by heterogeneous driver mutations and genomic instability.31 because dna methylation marks are inherently linked to cell of origin , methylation class may represent a more biologically relevant and stable biomarker of disease than dna - sequence variation alone . between our two methylation groups , a1 tumors were associated with a worse prognosis . 
the aggressive nature of a1 tumors was also evident in other clinical variables , with patients from this group having a more advanced clinical stage , greater age , and a tendency to be treated with adjuvant chemotherapy . 
the discrepancy between p53 staining and tp53 mutational status is curious but represents a known shortcoming of interrogating the tp53 locus by immunohistochemical means34 ; additional factors , such as tissue xation , likely affected this analysis . our study identied several genes and key pathways involved in biologic processes and molecular functions . signicant genes included igf2 , gnas , and cldn1 , supporting a role of regulatory pathways such as signal transduction , cell growth , and cell signaling . 
this supports results from previous studies suggesting a role for these pathways in pediatric acts.26 - 29 , 35 gsea also identied differential methylation of genes involved in the prc2 pathway . 
this is particularly interesting , given the distribution of ctnnb1 alterations in this cohort , as the prc2 complex is involved in epigenetic regulation and is a known modulator of the wnt - signaling pathway.36 one limitation of the current study is our inability to validate our ndings in an independent pediatric clinical cohort . 
in addition to the unsupervised clustering features , analysis of cpg - island methylation highlighted distinct distributions of methylation marks , with an absence of hypermethylator phenotype in the pediatric samples . adult and pediatric acts also had unique copy number proles , with pediatric samples tending to show greater evidence of chromosomal losses . 
the pediatric tumors retained their methylation groups when combined with the adult patients , providing evidence for the stability of group assignments and suggesting that adult trial cohorts their pediatric are not appropriate comparisons for counterparts . 
validation of our molecular grouping in independent pediatric clinical cohorts will be a central focus of future studies , and international collaboration with carefully annotated data will be necessary to advance our knowledge of these rare tumors . in addition to methylation - based classication representing a signicant predictor of risk in our cohort , we also validated the effectiveness of the wieneke classication schema . 
at risk : high - risk low - risk combined histologic - and molecular - risk stratification high risk low risk 2 , 000 time ( days ) fig 4 . 
kaplan - meier plots of overall survival from disease based on ( a ) initial clinical diagnosis , ( b ) diagnosis rendered at the time of central review , ( c ) dna methylation group , and ( d ) combined risk stratication using central review and methylation - classication group . 
ump , uncertain malignant potential . risk stratication is to use a combinatorial system of risk assessment followed by risk - adapted or targeted therapy . this approach may optimize the exposure to therapy for patients with standard - risk disease , while maximizing the effectiveness of intervention in patients with high - risk disease . affiliation 1st jude childrens research hospital , memphis , tn b.a.o. 
clay , md , department of pathology , ms 250 , 262 danny thomas pl , memphis tn 38105 - 2794 ; michael.clay@stjude.org. support supported by the national institutes of health grant no . 
i receive small royalty on an annual basis patent pending for genotyping assays to identify mutations in xaf1 provisional application #62 / 659 , 427 ; foreign ling april 18 , 2019 no other potential conicts of interest were reported . acknowledgment the authors thank david w . 
endocr rev 25 : 309 - 340 , 2004 gulack bc , rialon kl , englum br , et al : factors associated with survival in pediatric adrenocortical carcinoma : an analysis of the national cancer data base ( ncdb )  . 
michalkiewicz e , sandrini r , figueiredo b , et al : clinical and outcome characteristics of children with adrenocortical tumors : a report from the international pediatric adrenocortical tumor registry . 
am j surg pathol 27 : 867 - 881 , 2003 gr obner sn , worst bc , weischenfeldt j , et al : the landscape of genomic alterations across childhood cancers . 
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nat commun 6 : 6302 , 2015 kebebew e , reiff e , duh qy , et al : extent of disease at presentation and outcome for adrenocortical carcinoma : have we made progress ? world j surg 30 : 872 - 878 , 2006 barreau o , assi e g , wilmot - roussel h , et al : identication of a cpg island methylator phenotype in adrenocortical carcinomas . 
pinto em , rodriguez - galindo c , pounds sb , et al : identication of clinical and biologic correlates associated with outcome in children with adrenocortical tumors without germline tp53 mutations : a st jude adrenocortical tumor registry and childrens oncology group study . 
zheng s , cherniack ad , dewal n , et al : cancer genome atlas research network : comprehensive pan - genomic characterization of adrenocortical carcinoma . cancer cell 30 : 363 , 2016 [ erratum : cancer cell 30 : 363 , 2016 ] 15 . 
moran s , arribas c , esteller m : validation of a dna methylation microarray for 850 , 000 cpg sites of the human genome enriched in enhancer sequences . epigenomics 8 : 389 - 399 , 2016 proc natl acad sci usa 102 : 15545 - 15550 , 2005 diabetes . 
albertin g , carraro g , petrelli l , et al : endothelin - 1 and adrenomedullin enhance the growth of human adrenocortical carcinoma - derived sw - 13 cell line by stimulating proliferation and inhibiting apoptosis . 
scholl ui , st olting g , nelson - williams c , et al : recurrent gain of function mutation in calcium channel cacna1h causes early - onset hypertension with primary aldosteroniselife 4 : e06315 , 2015 24 . 
swisshelm k , machl a , planitzer s , et al : semp1 , a senescence - associated cdna isolated from human mammary epithelial cells , is a member of an epithelial membrane protein superfamily . 
almeida mq , azevedo mf , xekouki p , et al : activation of cyclic amp signaling leads to different pathway alterations in lesions of the adrenal cortex caused by germline prkar1a defects versus those due to somatic gnas mutations . 
gao zh , suppola s , liu j , et al : association of h19 promoter methylation with the expression of h19 and igf - ii genes in adrenocortical tumors . 
 clay et al appendix processing of samples and methylation data the study cohort was derived from the international pediatric adrenocortical tumor registry database ( n = 110 total entries ) to include samples that satised two requirements , including those that contained sufcient dna for methylation analysis and those that had tumor sections for histologic review ( initial cohort , n = 73 )  . 
the resultant 48 patients were included in the study . all dna samples were quantied by the uorometric method ( qbit dsdna br assay , thermo fisher scientic , waltham , ma )  . 
the detection p value for each sample was computed , and only samples with a mean detection p value less than .05 were carried forward for subsequent analysis . additional quality control was performed by calculating the median log ( base 2 ) intensities for methylated and unmethylated signals for each array and excluding samples with unmethylated and methylated median intensity values below a cutoff of 9.5. functional normalization ( fortin jp , et al : genome biol 15 : 503 , 2014 ) with noob background correction and dye - bias normalization ( troche tj , et al : nucleic acids res 41 : e90 , 2013 ) was performed . 
specically , probes located on sex chromosomes , probes containing a nucleotide polymorphism ( dbsnp132 common ) within ve base pairs of and including the targeted cpg - site , probes mapping to multiple sites on hg19 ( allowing for one mismatch ) , and any cross - reactive probes were removed from the analysis ( pidsley r , et al : genome biol 17 : 208 , 2016 )  . 
the pearson correlation was calculated as the distance measured between samples , and the clustering was performed using the complete - linkage agglomerative method ( clifford h , et al : front genet 2 : 88 , 2011 )  . in brief , the result of the hierarchical clustering analysis previously mentioned was also recapitulated in a complementary analysis that exhaustively evaluated 16 , 000 euclidean - distance hierarchical clustering procedures ( hcps ) that used four different probe - selection methods ( choosing probes with the greatest standard deviation , median absolute deviation , most informative spacing statistic [ pawlikowska i , et al : bioinformatics 30 : 1400 - 1408 , 2014 ] , and the dip statistic21 modied to measure both evidence bimodality and distance between modes ) , selection of 1 - 1 , 000 probes , and dening two to ve groups with a post hoc evaluation of reproducibility of subgroup group assignments by exact k = 5 nearest neighbor exact bootstrap procedure ( steele bm , et al : mach learn 74 : 235 - 255 , 2009 ; four probeselection methods selection of up to 1 , 000 probes denition of two to ve groups = 4 1 , 000 4 = 16 , 000 hcps )  . 
the modied dip statistic was dened as 4 times the product of the hartigan and hartigan dip statistic and the difference between the data value dening the dip and the quantile of the unimodal distribution function corresponding to the value of the empirical distribution function of that value . 
in this way , the modied dip statistic considered both the strength of statistical evidence in favor of multimodality and the size of the gap between the two primary modes in the data . 
hcp 1141 selected the 286 probes with the greatest value of this modied dip statistic and dened two subgroups with 96.4% exact k = 5 nearest neighbor bootstrap assignment reproducibility . 
the two subgroups dened by hcp 1141 strongly associated with two subgroups dened by t - sne and complete - linkage agglomeration ( p = 1.5 108 ; table a3 )  . 
the wilcoxon rank - sum test was used to perform a post hoc comparison of the methylation values of all probe sets across the two subgroups dened by hcp 1141 . 
to adjust for multiplicity , we computed storeys q value ( storey jd , et al : proc natl acad sci usa ) using the pounds - cheng estimator of the proportion of tests with a true null hypothesis ( pounds s , et al : comput biol 12 : 482 - 495 , 2005 )  . 
the data supplement provides the modied dip statistic and wilcoxon results for the 286 probes selected by hcp 1141 . copy number analysis dna copy number variation ( cnv ) was inferred from the methylation data by using the conumee bioconductor package in r with the default settings.16 the combined intensities of all available cpg probes were normalized against that of pediatric non - neoplastic adrenal gland controls ( n = 12 ) and using a linear - regression approach . 
we used bic ews to evaluate the following six models of the association of survival with the wieneke criterion , the clinical diagnosis , and / or methylation group : ( 1 ) the null model , ( 2 ) the wieneke criterion as the sole predictor of survival , ( 3 ) the clinical diagnosis as the sole predictor of survival , ( 4 ) the methylation group as the sole predictor of survival , ( 5 ) the wieneke criterion and methylation group as predictors of survival , and ( 6 ) the clinical diagnosis and methylation group as predictors of survival . 
the bic ews for a specic statistical model range from 0 ( the data do not support the specic model ) to 1 ( the data overwhelmingly support the specic model ) , and the bic ews for a set of candidate models sum to 1 . 
 dna methylation proling of pediatric adrenocortical tumors cimp - high 13 14 15 16 17 18 19 2021 22 cimp - intermediate 13 14 15 16 17 18 19 2021 22 cimp - low 13 14 15 16 17 18 19 2021 22 chromosome fig a4 . 
modied disease staging system used by ipactr stage description tumor completely excised with negative margins , tumor weight 200 g , absence of metastatic disease tumor completely excised with negative margins , tumor weight  . 
15 mits / 20 hpf ( yes : no ) adjusted for atypical mitoses methylation group atypical mitoses ( yes : no ) adjusted for ki67 above 15% methylation group ki67  . 
lennerz author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license ( continued ) purpose targeted therapy is the cornerstone of treatment of advanced egfr - mutant nonsmall - cell lung cancer ( nsclc )  . 
here , we assessed workflows designed to rapidly identify patients with actionable egfr mutations and reduce time to initiation ( tti ) of epidermal growth factor receptor ( egfr ) directed therapy . patients and methods we performed rapid testing for egfr l858r mutations and exon 19 deletions on paraffin - embedded or frozen section biopsy specimens from newly diagnosed patients with metastatic nsclc by using an egfr - specific assay ( rapid test )  . 
to determine clinical utility , we assessed concordance with ngs results , turnaround time , and tti of egfr therapy , and we evaluated reimbursement data . results between january 2015 and september 2017 , we performed 243 rapid egfr tests and identified egfr mutations in 43 patients ( 18% )  . 
escalation of the initiative into an interdisciplinary ultra - rapid next - day frozen - section workflow for highly symptomatic patients ( n = 8 ) resulted in a reduction in the median ( standard deviation ) turnaround time to 1 0.4 days and allowed several patients to initiate therapy within 1 week of biopsy . 
2018 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license : introduction nonsmall - cell lung cancer ( nsclc ) is a heterogeneous disease composed of unique molecular subsets with distinct clinical outcomes.1 , 2 multiple randomized studies have established the superiority of molecularly targeted therapies versus chemotherapy for the treatment of egfr - mutant and alk - positive nsclc.3 - 6 in other molecular subsets , single - arm studies confirm that treatment with targeted therapies can induce durable responses.7 , 8 as drugs that target these molecular drivers are approved for first - line treatment , genotyping in newly diagnosed nsclc is considered the standard of care.9 because of the need to interrogate a growing number of genes , next - generation sequencing ( ngs ) has largely replaced traditional single - gene assays.10 guidelines endorsed by oncology and pathology societies recommend that molecular testing turnaround times not exceed 10 working days.9 genotyping by ngs requires complex bioinformatics that can create treatment delays . 
we selected egfr mutant nsclc on the basis of its relatively high prevalence ( 10% to 15% ) among patients with nsclc , 12 the lack of overlap between egfr mutations and other clinically relevant molecular alterations , 13 and the fact that egfr inhibitors were readily available for hospitalized patients . 
in the first phase ( january 2015 to may 2017 ) , rapid egfr testing was performed on tissue specimens from consecutive patients diagnosed with metastatic nsclc who were never smokers / minimal smokers ( 10 pack years ) or who were hospitalized at the time of diagnosis ( data supplement )  . 
we also identified a comparator population composed of 121 patients with egfr - mutant nsclc who were diagnosed before implementation of the rapid testing ( ie , historical cohort ; data supplement )  . 
isolated nucleic acids from tumor specimens were analyzed with our ngs assay that uses anchored multiplex pcr to detect single - nucleotide variants and insertions / deletions in a target set of cancer - related genes.15 in addition , we examined fusion transcripts and met exon 14 skipping by using an rna - based ngs solid - fusion assay.15 statistical and economic analysis for contingency analyses , we used t tests , fishers exact tests , and 2 statistics . 
we defined turnaround - time from the date of accessioning to the date of reporting , and we defined tti from the date of the diagnostic biopsy to the date of ingestion of an egfr tyrosine kinase inhibitor ( tki )  . 
 for economic assessment , we reviewed line items of reimbursement data ( january 3 , 2017 , to february 8 , 2018 ) and extracted ( by payor ) the number of encounters and claim adjustment codes , and defined reimbursed as a payment greater than 0 . 
note that there is a ( variable ) delay from reporting to treatment decision and initiation of therapy because of cost coverage determination , preauthorization requirements , etc.the ultra - rapid egfr testing pathway ( pathway c ) is a multidisciplinary workflow designed to improve turnaround time using fresh tissue ( frozen sections ) to extract nucleic acids . 
among the remaining 234 patients , 23 ( 10% ) did not have ngs results because of insufficient tissue or technical failure of ngs ( data supplement )  . diagnostic utility of the rapid egfr assay improvement in turnaround time . 
first , we compared the turnaround times of the rapid and ngs assays by reviewing all specimens submitted for genotyping between july 2014 and january 2017 ( fig 2b )  . 
through ngs , we identified one additional low - level ( allelic fraction , approximately 4% ) p.l858r case , which was missed by rapid egfr testing ( fig 3 )  . 
the mutation spectrum of the tumors that underwent rapid testing is depicted in figure 3 , and the data supplement shows probabilities of therapeutically actionable variants . clinical utility of rapid egfr testing tti of tki therapy . 
p values result from t test ( age ) , fishers exact test ( sex , histology ) , or 2 test ( ethnicity , smoking )  . * includes the patient with a false - negative egfr - positive result . tki as the primary measure of clinical utility of the rapid egfr test . 
we reviewed the medical records of the 39 patients with egfr - mutant disease who underwent both rapid testing and ngs to determine whether tki therapy was initiated before ngs results . 
 validation implementation of rapid egfr testing ngs panel rapid wt rapid mut rapid egfr assay rapid egfr assay exon 19 exon 20 exon 21 del / ins t790m l858r variant fig 2 . 
scatter plots portray turnaround times of all 243 rapid egfr samples ( jan 2015 to may 2017 ; black , egfr wild type [ wt ] ; red , egfr mutation [ mut ] detected ) and all specimens that underwent ngs ( gray dots ) during this period . 
a case report of a patient who benefitted from this effort and a summary of the experience to date are described in the next section . therapeutic utility of ultra - rapid testing . 
osimertinib was selected on the basis of its activity against leptomeningeal disease.19 within days , the cough resolved , and the patient experienced marked improvement in his swallowing and regained the ability to walk . 
figure 4d illustrates the difference in turnaround time for the rapid and ultra - rapid tests and the time to initiation of tki therapy for patients tested through each workflow ( fig 4d inset )  . 
the sites of disease and presenting symptoms of these patients are detailed in the data supplement , which also summarizes our ultra - rapid workflow . rapid testing is operationally and financially sustainable . 
the heatmap portrays clinicopathologic features ( top three rows ) , rapid egfr results , and key molecular drivers along with the results of next generation sequencing ( ngs ) based fusion detection , fluorescence in - situ hybridization ( fish ) , and ngs panel results . 
key findings include ( 1 ) an isolated false - negative rapid egfr result ( arrow ) , ( 2 ) the inability of the rapid egfr test to detect egfr mutations at other residues , ( 3 ) identification of at least one underlying driver mutation in more than 50% of all tested cases by using the integrated molecular diagnostic approach , and ( 4 ) the association between clinicopathologic features and certain key drivers ( eg , never - smoking women with adenocarcinoma and egfr v > 10 pack - year smoking history and kras )  . 
 review of 214 clinical encounters with 1 , 475 line items of reimbursement data showed large variability between payors ( range , 0% to 100% ) and that , overall , 63% of encounters received reimbursement ( fig 4f )  . 
these data indicate that rapid egfr testing in our practice is operationally and financially sustainable . discussion here , we report the results of a quality improvement initiative to explore parallel testing with a rapid egfr assay and ngs in newly diagnosed nsclc . 
our findings emphasize the diagnostic , clinical , and therapeutic utility of rapid egfr testing . metastatic nsclc is a devastating and incurable disease for which the prognosis is highly dependent on identification of actionable molecular drivers.2 the established efficacy of us food and drug administrationapproved targeted therapies in specific nsclc subsets and the increasing number of investigational compounds underscore the necessity of identification of molecular alterations in a timely fashion . 
 ( a ) event curve that shows rapid egfr test reporting times and a comparison of the tyrosine kinase inhibitor ( tki ) initiation times ( relative to date of diagnosis ) for patients in the rapid and historical cohorts . 
the second block shows the 49% of patients ( n = 17 of 35 patients ) with egfr - mutant disease who started a tki before next - generation sequencing ( ngs ) results were available . 
 ( c ) response to the egfr inhibitor osimertinib in a patient with nonsmall - cell lung cancer who underwent ultra - rapid egfr testing : ( left ) pretreatment image and ( right ) response after 3 weeks ; arrow indicates primary tumor . 
 ( d ) comparison of rapid test times ( average ) and the eight patients tested with the ultra - rapid protocol ( fig 1c ) ; inset shows event curve comparison of time to initiation of tki between the rapid and ultra - rapid subsets . 
 ( e ) turnaround times for rapid ( gray ) and ultra - rapid ( blue ) workflows in a 9 - month extended standardof - care evaluation phase ; red , cases with an egfr mutation . 
several studies suggest that genotyping with multiple single - gene assays may reduce reporting time20 , 21 ; however , selective interrogation of the ever - expanding set of targets is impractical and may be limited by tissue availability.22 at the time our initiative began , consensus guidelines supported testing newly diagnosed patients with nsclc for egfr mutations and rearrangements in alk and ros1.9 these mutually exclusive genetic alterations are predominantly found in neveror light - smokers.13 , 23 testing these alterations in two stages ( ie , restriction of testing for rearrangements to patients whose disease is wild type for egfr mutations ) may lead to unnecessary delays between diagnosis and initiation of treatment for a significant proportion of patients and potentially steer symptomatic patients away from molecularly targeted treatments . 
through co - testing , we detected alk and ros1 rearrangements in 11 and six patients , respectively , and identified molecular alterations with promising investigational therapies in more than 40 additional patients ( fig 3 )  . 
for example , in a recent retrospective analysis that involved 15 community oncology centers , the median turnaround time for egfr testing and ngs was 23 days and 30 days , respectively.24 although this practice is likely more common in the community setting , where in - house testing is infrequent , one study demonstrated that 19% of patients with egfr mutations or alk rearrangements at an academic medical center in canada initiated first - line chemotherapy before testing results became available.11 the sequence of therapies may be particularly important for those patients initially treated with immunotherapy , because recent studies demonstrate that immunotherapy is seldom effective for egfr - mutant nsclc and that treatment with immunotherapy before targeted therapy increases the likelihood of the development of significant toxicities.25 - 27 given these data , we believe that rapid testing should be performed in parallel with full ngs genotyping . with a parallel - testing approach , we successfully performed rapid testing and ngs in 90% of patients in our initiative with material from a single biopsy . 
because half of the patients with tissue / dna that was insufficient for the full ngs were effectively tested for both alk and ros1 rearrangements using either fluorescence in - situ hybridization or the fusion assay , 95% of the patients in the rapid cohort met the minimum molecular testing requirement proposed by current asco guidelines . 
although pcr - based plasma genotyping is an expedient alternative to ngsbased tissue genotyping , the sensitivity of liquid biopsy for detection of egfr mutations is lower than what we report here with the rapid assay.29 , 30 despite the high sensitivity and specificity of the rapid assay , half of the patients in our study did not start tki therapy before ngs results were available ( fig 4b )  . 
 because tti was assessed retrospectively for the historical cohort , the median of 37 days between diagnosis and tki therapy might be an overestimate ; however , a similar delay was observed in another study.31 it also is conceivable that the difference in tti might be explained by process improvements over time that have shortened the interval between requests for and receipt of a drug from specialty pharmacies . 
because tki use predated ngs results in approximately 50% of patients , the reduction in time to tki initiation in the rapid group relative to the historical cohort might also reflect faster ngs reporting times . 
the scale of ngs panels currently precludes significant reduction , and the median and mean turnaround times for ngs results in the ultrarapid cohort were 9 and 10 days , respectively . 
 as a result of the short duration of follow - up of our rapid cohort and imbalances between the rapid and historical groups ( including enrollment of patients in the rapid cohort into a consolidation radiation protocol ) , we were unable to evaluate differences in progression - free survival on egfr - directed therapy . 
lennerz the potential to defer brain radiation for these patients underscore the importance of rapid identification of egfr mutations.41 , 42 the small number of patients with egfr - mutant disease in our study also limits the potential impact of our findings . 
however , many laboratories are proficient in performing targeted egfr genotyping , 43 and our extended standard of care evaluation ( fig 4e ) and reimbursement analysis ( fig 4f ) indicate operational and financial sustainability . in summary , we demonstrate that expedited egfr genotyping enables early intervention with targeted therapies and allows symptomatic patients to access effective treatments . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ibiayi dagogo - jack honoraria : foundation medicine consulting or advisory role : boehringer ingelheim administrative support : christopher g . 
farago honoraria : foundation medicine vania nose no relationship to disclose consulting or advisory role : pharmamar , takeda , abbvie , loxo , stemcentrx research funding : pharmamar ( inst ) , abbvie ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , loxo ( inst ) , ignyta ( inst ) miguel rivera consulting or advisory role : loxom asubio ( i ) speakers ' bureau : pfizer ( i ) research funding : advanced cell diagnostics , affymetrix travel , accommodations , expenses : pharmamar , abbvie , stemcentrx patents , royalties , other intellectual property : patents with affymetrix justin f . 
gainor honoraria : merck , incyte , ariad , novartis , pfizer consulting or advisory role : genentech , bristol - myers squibb , theravance , loxo , takeda , array biopharma , amgen research funding : merck ( inst ) , novartis ( inst ) , genentech , bristol - myers squibb ( inst ) , adaptimmune ( inst ) , astrazeneca ( inst ) , ariad , jounce therapeutics ( inst ) , blueprint medicines ( inst ) , moderna therapeutics ( inst ) , tesaro ( inst ) travel , accommodations , expenses : affymetrix ginger jiang employment : novartis ( i ) zofia piotrowska consulting or advisory role : boehringer ingelheim , astrazeneca , ariad , takeda , superdimension , guardant health , novartis , abbvie research funding : novartis ( inst ) , ariad ( inst ) , takeda ( inst ) , guardant health ( inst ) rebecca s . 
heist consulting or advisory role : boehringer ingelheim research funding : abbvie ( inst ) , novartis ( inst ) , roche ( inst ) , incyte ( inst ) , celgene ( inst ) , mirati therapeutics ( inst ) , peregrine pharmaceuticals ( inst ) , exelixis ( inst ) , millenium ( inst ) , debiopharm group ( inst ) , corvus pharmaceuticals ( inst ) valentina nardi stock and other ownership interests : ksq therapeutics ( i ) , navicor ( i ) consulting or advisory role : thermo fisher scientific ( i ) , cell signaling technology ( i ) , raze ( i ) , caloric tests ( i ) dora dias - santagata no relationship to disclose long p . 
le stock and other ownership interests : archer biosciences consulting or advisory role : archer biosciences patents , royalties , other intellectual property : i am a co - inventor of the anchored multiplex pcr technology which is licensed to archerdx . 
sequist honoraria : astrazeneca consulting or advisory role : astrazeneca , genentech , roche , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , merck ( inst ) , pfizer ( inst ) , guardant health ( inst ) , incyte ( inst ) martha pitman consulting or advisory role : medtronic inga t . 
shaw honoraria : pfizer , novartis , roche , genentech , foundation medicine consulting or advisory role : pfizer , novartis , genentech , roche , ariad , ignyta , blueprint medicines , daiichi sankyo , emd serono , taiho pharmaceutical , kso therapeutics , natera , loxo , takeda research funding : pfizer , novartis , roche , genentech , a . 
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garassino mc , cho bc , kim jh , et al : durvalumab as third - line or later treatment for advanced nonsmall - cell lung cancer ( atlantic ) : an open - label , single - arm , phase 2 study . 
lee ck , man j , lord s , et al : clinical and molecular characteristics associated with survival among patients treated with checkpoint inhibitors for advanced nonsmall - cell lung carcinoma : a systematic review and meta - analysis . 
sholl lm , aisner dl , varella - garcia m , et al : multi - institutional oncogenic driver mutation analysis in lung adenocarcinoma : the lung cancer mutation consortium experience . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
lee ck , davies l , wu yl , et al : gefitinib or erlotinib vs chemotherapy for egfr mutation positive lung cancer : individual patient data meta - analysis of overall survival . 
yang jc , wu yl , schuler m , et al : afatinib versus cisplatin - based chemotherapy for egfr mutationpositive lung adenocarcinoma ( lux - lung 3 and lux - lung 6 ) : analysis of overall survival data from two randomised , phase 3 trials . 
vergnenegre a , massuti b , de marinis f , et al : economic analysis of first - line treatment with erlotinib in an egfr - mutated population with advanced nsclc . 
ting j , tien ho p , xiang p , et al : cost - effectiveness and value of information of erlotinib , afatinib , and cisplatin - pemetrexed for first - line treatment of advanced egfr mutationpositive nonsmall - cell lung cancer in the united states . 
lu s , ye m , ding l , et al : cost - effectiveness of gefitinib , icotinib , and pemetrexed - based chemotherapy as first - line treatments for advanced nonsmall - cell lung cancer in china . 
handorf ea , mcelligott s , vachani a , et al : cost effectiveness of personalized therapy for firstline treatment of stage iv and recurrent incurable adenocarcinoma of the lung . 
isla d , de castro j , juan o , et al : costs of adverse events associated with erlotinib or afatinib in first - line treatment of advanced egfr - positive nonsmall - cell lung cancer . 
park k , tan eh , obyrne k , et al : afatinib versus gefitinib as first - line treatment of patients with egfr mutationpositive nonsmall - cell lung cancer ( lux - lung 7 ) : a phase 2b , open - label , randomised controlled trial . 
schuler m , wu yl , hirsh v , et al : first - line afatinib versus chemotherapy in patients with non small - cell lung cancer and common epidermal growth factor receptor gene mutations and brain metastases . 
goss g , tsai cm , shepherd fa , et al : cns response to osimertinib in patients with t790mpositive advanced nsclc : pooled data from two phase ii trials . 
 patterns of metastatic spread and mechanisms of resistance to crizotinib in ros1 - positive nonsmall - cell lung cancer purpose the ros1 tyrosine kinase is activated through ros1 gene rearrangements in 1% to 2% of nonsmall - cell lung cancers ( nsclcs ) , which confer sensitivity to treatment with the anaplastic lymphoma kinase ( alk ) / ros1 / mesenchymal - epithelial transition factor inhibitor crizotinib . 
currently , insights into patterns of metastatic spread and mechanisms of crizotinib resistance among patients with ros1 - positive disease are limited . patients and methods we reviewed clinical and radiographic imaging data of patients with ros1and alk - positive nsclc to compare patterns of metastatic spread at initial metastatic diagnosis . 
to determine molecular mechanisms of crizotinib resistance , we analyzed repeat biopsy specimens from a cohort of patients with ros1 - positive disease who progressed on crizotinib . results we identified 39 and 196 patients with advanced ros1and alk - positive nsclc , respectively . 
ros1 mutations included g2032r ( 41% ) , d2033n ( 6% ) , and s1986f ( 6% )  . conclusion compared with alk rearrangements , ros1 rearrangements are associated with lower rates of extrathoracic metastases , including fewer brain metastases , at initial metastatic diagnosis . 
2017 by american society of clinical oncology introduction treatment paradigms for advanced nonsmallcell lung cancer ( nsclc ) continue to evolve and reflect a growing understanding of the genetic underpinnings of the disease . 
subsequent work has shown that such rearrangements are present in 1% to 2% of nsclcs and define a distinct molecular subgroup.2 - 4 of note , ros1 is phylogenetically related to the anaplastic lymphoma kinase ( alk ) receptor tyrosine kinase.5 thus , like alk rearrangements in nsclc , 6 , 7 ros1 fusions confer sensitivity to the alk / ros1 / mesenchymal - epithelial transition factor inhibitor crizotinib.3 in profile 1001 ( study of oral pf - 02341066 , a c - met / hepatocyte growth factor tyrosine kinase inhibitor , in patients with advanced cancer ) , crizotinib produced an objective response rate justin f . 
shaw author affiliations and support information ( if applicable ) appear at the end of this article . presented at the 2016 american society of clinical oncology annual meeting , chicago , il , june 3 - 7 , 2016 . corresponding author : alice t . 
on the basis of this activity , the us food and drug administration expanded crizotinibs approval to include patients with advanced , ros1 - positive nsclc.12 consistent with these reports , we observed several prolonged responses to crizotinib among patients with ros1 - positive nsclc at our institution . specifically , we observed particularly durable responses among patients with intrathoracic - only disease ( ie , m1a disease ) , 3 which led us to hypothesize that differences in malignant phenotypes between ros1 and alk rearrangements , including differences in patterns of metastatic spread , affect therapeutic outcomes . 
in one early study , doebele et al13 reported that alk rearrangements are associated with pericardial , pleural , and liver metastases compared with an egfr / kras / alk wild - type cohort . 
outside this report , however , few studies have evaluated patterns of metastatic spread according to molecular genotype in nsclc , and none have focused on ros1.14 , 15 in this study , we investigated the distribution of malignant disease at initial metastatic diagnosis and evaluated associations with clinical outcomes in ros1 - positive nsclc . 
data were updated as of january 2016 . all studies were performed under an institutional review boardapproved protocol . pfs was measured from the time of crizotinib initiation to investigator - assessed , radiographic progression or death in the absence of documented progression . 
overall survival ( os ) was measured from initiation of crizotinib until death . patients without a known date of death were censored at the time of last follow - up . in addition , patients with ros1 - positive nsclc who underwent repeat biopsies / resection of progressing lesions on crizotinib between july 2012 and december 2016 were identified . 
age and lines of therapy were analyzed by wilcoxon rank sum test . the kaplan - meier method was used to estimate pfs and os medians and probabilities , and the log - rank test was used to compare their differences between groups . 
no significant differences in baseline clinicopathologic characteristics were observed between groups ( data supplement ) , including no difference in the median number of prior lines of therapy before crizotinib ( median , 1 ; data supplement )  . 
to address whether this difference was confounded by prior therapy , we examined pfs among patients who received second - line crizotinib ( ie , after one prior therapy ) because this was the most common line of crizotinib in both cohorts ( ros1 , 60% ; alk , 42% )  . 
of note , 101 patients with alk - positive nsclc ( 58% ) received secondor thirdgeneration alk inhibitors after crizotinib , whereas only seven patients with ros1 - positive nsclc ( 23% ) received additional ros1 inhibitors ( p , .001 ; data supplement )  . 
thus , the longer median pfs with crizotinib among patients with ros1 - positive disease may have been partly offset by greater access to next - generation targeted therapies among patients with alk - positive disease . sites of metastatic disease to determine whether these clinical outcomes may have also been affected by distribution of metastatic disease , we compared sites of disease at initial metastatic diagnosis among patients with alkand ros1 - positive nsclc . 
metastatic involvement of a given anatomic site was determined on the basis of clinical staging ( tnm seventh edition ) .30 positron emission tomography - computed tomography ( ct ) and ct scans of the chest , abdomen , and pelvis were performed in 72% and 26% of patients with alk - positive nsclc and 82% and 18% of patients with ros1 - positive nsclc , respectively ( table 1 )  . 
brain magnetic resonance imaging ( alk , 76% ; ros1 , 82% ) or a head ct scan with intravenous contrast ( alk , 9% ; ros1 , 10% ) were also performed in most patients . 
in addition to having a lower rate of brain metastases at initial diagnosis , fewer patients with ros1 - positive nsclc developed brain metastases over time compared with those with alk - positive nsclc . 
the cumulative incidence of brain metastasis among patients with alkand ros1 - positive disease was 73% and 34% , respectively , at 5 years after initial metastatic diagnosis ( p , .001 ; fig 3a )  . 
percentages may not add to 100 because of rounding . abbreviations : ct , computed tomography ; ecog , eastern cooperative oncology group ; mri , magnetic resonance imaging ; pet , positron emission tomography . * includes one patient with adenosquamous histology . on the basis of performance status at initial metastatic presentation or at the first documented assessment . 
performance status was not available in four patients with alk - positive disease and one patient with ros1 - positive disease . systemic staging and neuroimaging studies were not done or were not available for review in five and 35 patients with alk - positive disease , respectively . 
four patients with alk - positive disease had both a brain mri and a head ct scan . neuroimaging studies were not done or not available for review in three patients with ros1 - positive disease . time was also greater among those with alkpositive disease ( 56% v 22% at 5 years ; p = .001 ; fig 3b )  . 
of note , 101 patients with alk - positive nsclc ( 58% ) received next - generation alk inhibitors ( ceritinib , 40% ; alectinib , 27% ; brigatinib , 3% ) after crizotinib ( data supplement ) ; however , 93% of these patients received such agents after the initial development of brain metastases . 
collectively , these findings suggest that alk - positive cancers have an increased tropism for the brain compared with ros1 - positive nsclcs . next , we evaluated outcomes of crizotinib treatment according to the presence of extrathoracic metastases ( ie , m1a v m1b disease )  . 
thus , this difference in pfs for crizotinib treatment outcomes between patients with alkand ros1 - positive nsclc in the overall study population may have been partly driven by the higher frequency of m1a disease among those with ros1 - positive disease because this group appears to derive greater benefit with crizotinib . ros1 : crizotinib resistance despite the effectiveness of crizotinib in alkand ros1 - positive nsclc , most patients acquire resistance . 
to investigate potential mechanisms of resistance to crizotinib in ros1 - positive nsclc , we analyzed postprogression biopsy specimens from patients with ros1 - positive disease who progressed on crizotinib treatment . 
all patients underwent tissue sampling within 7 days of crizotinib discontinuation . persistence of the original ros1 rearrangement was observed in nine ( 100% ) of nine postcrizotinib specimens available for testing ( repeat fish [ n = 2 ] , rt - pcr [ n = 5 ] , or ngs [ n = 2 ] )  . 
 ( d ) os as measured from the time of crizotinib initiation in the second - line setting . time since crizotinib initiation ( months ) time since crizotinib initiation ( months ) no . 
thus , ros1 resistance mutations were detected in a majority ( 10 [ 62.5% ] of 16 ) of patients with crizotinib resistance . because crizotinib has limited blood - brain barrier penetration , 31 we analyzed crizotinib - resistant samples by site of disease . 
among non - cns specimens ( n = 14 ) , the frequency of ros1 resistance mutations was 64% ( appendix fig a2 ) , with 50% of specimens harboring the ros1 g2032r mutation . 
among six specimens that underwent targeted ngs with the mgh snapshot platform , none was found to have high - level copy number changes in any analyzed gene ( data supplement )  . 
 a mgh047 - 5 ros1 g2032r mgh9018 - 1 ros1 wt biopsy ros1 wt ros1 wt ros1 g2032r ros1 g2032r ros1 g2032r ros1 s1986f ros1 g2032r * ros1 wt ros1 wt ros1 wt * mgh070 - 1 mgh096 - 1 mgh077 - 1 mgh080 - 2 mgh998 - 1 mgh508 - 1 mgh095 - 1 mgh996 - 1 mgh943 - 1 mgh995 - 1 mgh933 - 1 mgh081 - 1 mgh968 - 1 mgh986 - 1 fig 4 . 
mgh , massachusetts general hospital ; wt , wild type . g2032r ros1 d2033n ros1 wt ( 2 sites ) ros1 g2032r s1986f d2033n progression - free survival ( months ) ros1 g2032r discussion we observed that despite shared clinical features between ros1and alk - positive nsclcs , these genetic alterations were associated with different patterns of metastatic spread . 
although the shorter pfs with crizotinib treatment among patients with alk - positive nsclc may have been an influence in this series , we observed significantly higher rates of brain metastases at initial diagnosis ( ie , before exposure to crizotinib ) in this group . together , these observations suggest that alkrearranged nsclcs have a greater tropism for the cns . 
the majority of patients with alkpositive disease who developed brain metastases did so before receiving more cns penetrable , next - generation alk inhibitors , which provides an additional rationale for investigating the upfront use of next - generation alk inhibitors to prevent or delay the emergence of brain metastases . 
several ongoing first - line studies are comparing crizotinib with second - generation alk inhibitors ( eg , alex [ study comparing alectinib with crizotinib in treatment - naive anaplastic lymphoma kinasepositive advanced nonsmall cell lung cancer participants ] , alta - 1l [ phase iii study of brigatinib versus crizotinib in alk - positive advanced non small - cell lung cancer patients ] ) and have generally incorporated secondary end points focused on intracranial disease activity . one limitation of this analysis is that we observed a relatively higher frequency of baseline brain metastases in the alk - positive cohort than had other studies.6 , 13 although this observation may reflect differences in local imaging practices or referral patterns , such factors would have likely affected both alk and ros1 cohorts . 
nonetheless , several other studies have shown a comparable pfs to our series.8 - 11 of note , although patients with ros1 - positive disease had a longer median pfs with crizotinib treatment than patients with alk - positive disease , no difference in os was found between cohorts . 
we cannot exclude the possibility that this was due to unaccounted - for differences in patient characteristics , although the higher rates of next - generation targeted therapy use among patients with alk - positive disease may have offset the longer pfs with crizotinib treatment among patients with ros1positive disease . despite the significant activity of crizotinib , acquired resistance remains a challenge for patients with alkand ros1 - positive nsclc alike.16 , 43 - 45 thus far , insights into the mechanisms of resistance to crizotinib among those with ros1 - positive disease have been limited and generally consist of isolated case reports , small series , and preclinical evaluations.16 - 19 , 46 to date , seven different ros1 resistance mutations have been described.16 - 19 , 46 in addition , upregulation of bypass signaling pathways ( eg , egfr , ras , kit ) have also been reported.20 - 22 , 47 to our knowledge , we present the largest study of crizotinib resistance in ros1 - positive nsclc to date , which has found ros1 resistance mutations in a majority of specimens . 
 emerged through selection of pre - existing clones or through genetic evolution of drugtolerant cells.48 despite similarities between alk and ros1 , each has a different frequency and spectrum of on - target mechanisms of crizotinib resistance . 
indeed , patients with ros1 - positive nsclc have a much higher frequency of on - target resistance mutations , but such mutations are concentrated in a narrower segment of the kinase , which perhaps reflects the greater potency of crizotinib for ros1 than for alk . potential limitations of this analysis are that several different genotyping platforms were used . 
thus , we may have overlooked ros1 mutations outside this region . however , all specimens that underwent sanger sequencing and / or deep sequencing ( n = 8 ) were evaluated for mutations across the entire ros1 kinase domaanother important limitation is that we were unable to identify a mechanism of crizotinib resistance in all patients . 
thus , additional studies are necessary to elucidate other potentially target - independent mechanisms of crizotinib resistance . in alk - positive nsclc , second - generation alk inhibitors demonstrate significant activity in the crizotinib - resistant setting largely as a result of their greater potency against alk compared with crizotinib . 
beyond cabozantinib and tpx - 0005 , several other agents with ros1 activity are being evaluated , including entrectinib ( clinicaltrials.gov identifier nct02097810 ) , 53 ds - 6051b ( clinicaltrials.gov identifier nct02279433 ) , and lorlatinib ( clinicaltrials.gov identifier nct01970865 ) , 50 , 54 but these agents have not demonstrated clinical activity against ros1 g2032r to date ( data supplement )  . in summary , despite a shared susceptibility to crizotinib , alk and ros1 rearrangements differ in distributions of metastatic disease . 
nonetheless , acquired resistance to crizotinib remains a significant challenge for both molecular subsets . among patients with ros1 - positive nsclc , ros1 mutations ( most notably g2032r ) are the predominant mechanisms of resistance to crizotinib , which underscores the need for clinical development of next - generation ros1 inhibitors with activity against this mutation . 
provisional application to the us patent and trademark office ( application number 61817229 ) satoshi yoda no relationship to disclose ibiayi dagogo - jack no relationship to disclose luc friboulet no relationship to disclose jessica j . 
hubbeling no relationship to disclose leila dardaei no relationship to disclose james hardwick employment : pfizer stock and other ownership interests : pfizer travel , accommodations , expenses : pfizer donghui huang employment : pfizer stock and other ownership interests : pfizer travel , accommodations , expenses : pfizer mari mino - kenudson consulting or advisory role : merrimack , h3 biomedicine , acd pharmaceuticals , roche , genentech a . 
john iafrate stock and other ownership interests : archer biosciences consulting or advisory role : debiopharm group , constellation pharmaceuticals , chugai pharma , roche research funding : blueprint medicines patents , royalties , other intellectual property : archerdx exclusive license to amp technology anna f . 
farago honoraria : foundation medicine consulting or advisory role : pharmamar , merrimack , takeda pharmaceuticals , abbvie , intervention insights travel , accommodations , expenses : pharmamar , abbvie , stemcentrx aaron n . 
ferris no relationship to disclose zofia piotrowska consulting or advisory role : boehringer ingelheim , astrazeneca , ariad pharmaceuticals , takeda pharmaceuticals , superdimension research funding : guardant health ( inst ) alice t . 
shaw honoraria : pfizer , novartis , roche , genentech , foundation medicine consulting or advisory role : pfizer , novartis , genentech , roche , ariad pharmaceuticals , ignyta , blueprint medicines , daiichi sankyo , emd serono , taiho pharmaceutical , ksq therapeutics research funding : pfizer , novartis , roche , genentech acknowledgment we thank cyril h . 
shaw at , kim dw , nakagawa k , et al : crizotinib versus chemotherapy in advanced alk - positive lung cancer . med 371 : 2167 - 2177 , 2014 n engl j med 368 : 2385 - 2394 , 2013 8 . 
moro - sibilot d , faivre l , zalcman g , et al : crizotinib in patients with advanced ros1 - rearranged nonsmall - cell lung cancer ( nsclc ) : preliminary results of the acse phase ii trial . 
goto k , yang j , kim d , et al : phase ii study of crizotinib in east asian patients ( pts ) with ros1 - positive advanced nonsmall - cell lung cancer ( nsclc )  . 
russo a , franchina t , picone a , et al : different metastatic pattern according to the egfr mutational status in a cohort of lung adenocarcinomas ( adcs ) : a single - institution report . 
facchinetti f , loriot y , kuo ms , et al : crizotinib - resistant ros1 mutations reveal a predictive kinase inhibitor sensitivity model for ros1and alk - rearranged lung cancers . 
drilon a , somwar r , wagner jp , et al : a novel crizotinib - resistant solvent - front mutation responsive to cabozantinib therapy in a patient with ros1 - rearranged lung cancer . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
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gainor jf , ou sh , logan j , et al : the central nervous system as a sanctuary site in alk - positive nonsmall - cell lung j clin oncol 29 : e443 - e445 , 2011 cancer . 
soria jc , tan ds , chiari r , et al : first - line ceritinib versus platinum - based chemotherapy in advanced alkrearranged nonsmall - cell lung cancer ( ascend - 4 ) : a randomised , open - label , phase 3 study . 
gadgeel sm , shaw at , govindan r , et al : pooled analysis of cns response to alectinib in two studies of pretreated patients with alk - positive nonsmall - cell lung cancer . 
crin `o l , ahn mj , de marinis f , et al : multicenter phase ii study of whole - body and intracranial activity with ceritinib in patients with alk - rearranged nonsmall - cell lung cancer previously treated with chemotherapy and crizotinib : results from ascend - 2 . 
woo cg , seo s , kim sw , et al : differential protein stability and clinical responses of eml4 - alk fusion variants to various alk inhibitors in advanced alk - rearranged nonsmall cell lung cancer . 
huber kv , salah e , radic b , et al : stereospecific targeting of mth1 by ( s ) - crizotinib as an anticancer strategy . nature 508 : 222 - 227 , 2014 42 . 
shaw a , camidge d , engelman j , et al : clinical activity of crizotinib in advanced nonsmall - cell lung cancer ( nsclc ) harboring ros1 gene rearrangement . 
zou hy , li q , engstrom ld , et al : pf - 06463922 is a potent and selective next - generation ros1 / alk inhibitor capable of blocking crizotinib - resistant ros1 mutations . 
cui j , rogers e , zhai d , et al : ending the endless acquired tyrosine kinase resistance mutationsdesign of tpx0005 , a multi - target alk / ros1 / trk inhibitor with broad spectrum activity against wild - type and mutants including alk g1202r , ros1 g2032r , and trka g595r . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multi - targeted pan - trk , ros1 , and alk inhibitor entrectinib ( rxdx - 101 ) : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . cancer discov 7 : 400 - 409 , 2017 54 . 
solomon b , bauer t , felip e , et al : safety and efficacy of lorlatinib ( pf - 06463922 ) from the dose - escalation component of a study in patients with advanced alk + or ros1 + nonsmall - cell lung cancer ( nsclc )  . 
progressionfree survival ( pfs ) of alkand ros1 - positive patients with ( a ) m1a and ( b ) m1b disease . time since crizotinib initiation ( months ) time since crizotinib initiation ( months ) no . 
 c targeted next - generation sequencing reveals clinically actionable braf and esr1 mutations in low - grade serous ovarian carcinoma introduction low - grade serous ovarian cancer ( lgsoc ) is a rare ( < 5% ) subset of epithelial ovarian cancer with unique biologic , clinical , and genetic features.1 compared with those with high - grade soc ( hgsoc ) , the most common histologic subtype of ovarian cancer , patients with lgsoc are diagnosed at a younger age and have a better prognosis.2 , 3 standard - of - care treatment of advanced - stage lgsoc and hgsoc is similar : surgical cytoreduction plus platinum and taxane chemotherapy.4 however , lgsoc is less responsive to platinum - based chemotherapy compared with hgsoc , 5 , 6 possibly because of slower proliferation and fewer abnormalities in the homologous recombination repair pathway ( including brca1 or brca2 mutations ) in lgsoc.7 in contrast , lgsoc may benefit more from endocrine or hormonal therapy ( aromatase inhibitors [ ais ] or tamoxifen ) , because a greater proportion of lgsocs express estrogen and progesterone receptors.8 endocrine therapy is a common treatment of recurrent lgsoc , 9 and in retrospective studies , it provided benefit as maintenance therapy in the adjuvant setting.10 although recurrent lgsoc can follow a chronic , indolent course , it is incurable with current treatments , and patients often die as a result of their disease , highlighting the need for novel therapies . we describe two patients with lgsoc whose clinical management was informed by targeted panel next - generation sequencing ( ngs ) performed in our institution . 
the oncopanel test at dana - farber cancer institute consists of targeted ngs of formalin - fixed tumor samples covering exons of > 300 cancer - associated genes , plus intronic regions of genes involved in somatic rearrangements.11 - 13 oncopanel tests report mutations , insertions and deletions , copy number variations , and structural variants . 
we present clinically relevant alterations identified by oncopanel in two patients with recurrent lgsoc : a patient with a braf v600e mutation who derived clinical benefit from braf inhibitor vemurafenib , and a patient with progressive disease after durable response to hormonal therapy whose recurrent tumor harbored an esr1 mutation associated with resistance to antiestrogen therapy . 
 konstantinopoulos author affiliations and support information ( if applicable ) appear at the end of this article . licensed under the creative commons attribution 4.0 license corresponding author : panagiotis a . 
 b time since diagnosis ( years ) time since diagnosis ( years ) ca - 125 surgery carboplatin plus paclitaxel ca - 125 surgery carboplatin plus paclitaxel anastrozole bevacizumab vemurafenib carboplatin - based chemotherapy anastrozole plus leuprolide basis of oncopanel testing of her tumor from her recurrence surgery , which revealed a braf c.1799t > a ( p.v600e ) mutation ( appendix ) , she started vemurafenib at 480 mg twice daily , which was dose reduced to 240 mg twice daily because of cutaneous toxicity . 
two years later , she developed recurrent disease and underwent secondary cytoreduction of metastatic serous carcinoma at multiple sites in the abdomen and pelvis , followed by platinum - based chemotherapy . 
she underwent complete surgical cytoreduction , with pathology showing stage iii invasive serous borderline tumor and one area suggestive for lg serous discussion recent genomic profiling of lgsoc suggested several potential targetable pathways and highlighted dramatic differences in the genomes of lgsoc and hgsoc . 
braf v600e mutations are present in 35% of serous borderline cancers or lgsocs18 and are associated with better prognosis and decreased likelihood of requiring systemic therapy.18 despite the low prevalence of braf v600e mutations in patients with recurrent disease requiring treatment , this case highlights that this mutation may correlate with sensitivity to braf inhibitors , such as vemurafenib . 
two previous patient cases of lgsoc with braf v600e mutations and sustained response to vemurafenib were described.26 , 27 one patient was treated in a basket trial of solid tumors with braf v600e mutations and responded for at least 12 months.26 a second patient , who had experienced progression throughout chemotherapy , hormonal therapy , and antiangiogenic therapy , had a braf v600e mutation on a recurrence biopsy and was treated with vemurafenib , achieving clinical and radiographic responses.27 despite dose reduction because of skin rash , the patient continued to receive vemurafenib with an ongoing partial response for nearly 2 years.27 it is notable that both this patient and our patient seemed to respond to significantly lower doses of vemurafenib than the us food and drug administration approved dose in melanoma ( 960 mg orally twice daily ) , suggesting that lgsoc tumors with braf v600e mutations may be more sensitive to raf inhibition . 
given that not all solid tumors with braf v600e mutations respond to raf inhibition ( eg , braf - mutant colon cancers do not benefit from vemurafenib28 ) , these cases illustrate that recurrent lgsoc with a braf v600e mutation may derive clinical benefit from treatment with vemurafenib or other raf inhibitors , arguing for routine assessment of these mutations in recurrent lgsoc . 
selumetinib showed a 15% response rate in recurrent lgsoc in a phase ii trial.25 an exceptional responder in this trial had a response to selumetinib of > 5 years and had a deletion in map2k1 ( encoding mek1 ) , which has oncogenic activity.22 another patient with lgsoc and a kras g12d mutation had a response of > 7 years to selumetinib.29 our second case of recurrent lgsoc highlights that targeted ngs can elucidate the mechanism of resistance in a patient with excellent response to hormonal therapy and may help tailor future therapy . 
although esr1 mutations in the ligand - binding domain ( most commonly d538g and y537c / s / n ) have been reported in breast cancers treated with hormonal therapy , this is to our knowledge the first esr1 mutation reported in lgsoc.30 - 35 esr1 mutations are rare in primary , untreated breast cancers but prevalent in metastatic breast cancers resistant to hormonal therapy.30 , 33 , 35 , 36 structural alterations conferred by these activating mutations , including y537s , result in ligand - independent activation of the estrogen receptor and resistance to endocrine antagonists.30 , 36 , 37 it is reasonable to surmise that this mutation contributed to tumor progression during ai therapy . 
 of action downstream of the activated estrogen receptor and bypass the resistance mechanis for instance , the oral selective estrogen receptor degrader ( serd ) azd9496 potently binds and downregulates d538g and y537s esr1 proteins in vitro and was effective against breast cancer xenografts with y537s and other esr1 mutations , whereas the us food and drug administrationapproved serd fulvestrant had only a partial effect against y537s.38 , 39 combinations of antiestrogen agents such as ais or serds with targeted therapies such as mammalian target of rapamycin inhibitors ( eg , everolimus ) and cdk4 / 6 inhibitors ( eg , palbociclib and abemaciclib ) may also overcome resistance associated with esr1 mutations . 
in the paloma3 ( palbociclib ongoing trials in the management of breast cancer 3 ) trial of fulvestrant plus palbociclib versus placebo in ai - resistant patients , the benefit of addition of palbociclib to fulvestrant was seen irrespective of specific esr1 mutation.40 in bolero2 ( breast cancer trials of oral everolimus 2 ) trial of exemestane plus everolimus , the benefit of everolimus was evident in tumors with an esr1 d538g mutation but was not clear in y537s esr1mutated tumors because of low numbers.41 , 42 esr1 mutations can be detected by targeted sequencing in tumors and cell - free dna , indicating that clinical testing for these resistance mutations is feasible.35 , 36 , 42 tumor heterogeneity is an important challenge in interpreting targetable mutations . 
on a practical level , both patients maintained stable low - volume disease with the selected targeted therapy , and identifying different mutations in other lesions might not necessitate a change in management as long as the patients remain asymptomatic . in conclusion , our first case highlights the potential utility of testing for braf v600e by targeted sequencing in lgsoc , as well as the possibility of meaningful clinical response to even low doses of vemurafenib in patients with lgsoc with a braf v600e mutation . 
in the second case , targeted sequencing helped elucidate the mechanism of resistance in a patient with lgsoc with prolonged response to ai therapy , which could be relevant for selection of additional therapy to overcome resistance . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . collection and assembly of data : elizabeth h . 
matulonis consulting or advisory role : merck , eli lilly , geneos , 2x oncology , myriad genetics , clovis oncology , fujifilm research funding : merck , novartis panagiotis a . 
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garcia ep , minkovsky a , jia y , et al : validation of oncopanel : a targeted next - generation sequencing assay for the detection of somatic variants in cancer . 
grisham rn , iyer g , garg k , et al : braf mutation is associated with early stage disease and improved outcome in patients with low - grade serous ovarian cancer . 
tsang yt , deavers mt , sun cc , et al : kras ( but not braf ) mutations in ovarian serous borderline tumour are associated with recurrent low - grade serous carcinoma . 
gershenson dm , sun cc , wong kk : impact of mutational status on survival in low - grade serous carcinoma of the ovary or peritoneubr j cancer 113 : 1254 - 1258 , 2015 22 . 
grisham rn , sylvester be , won h , et al : extreme outlier analysis identifies occult mitogenactivated protein kinase pathway mutations in patients with low - grade serous ovarian cancer . 
farley j , brady we , vathipadiekal v , et al : selumetinib in women with recurrent low - grade serous carcinoma of the ovary or peritoneum : an open - label , single - arm , phase 2 study . 
combe p , chauvenet l , lefrre - belda ma , et al : sustained response to vemurafenib in a low grade serous ovarian cancer with a braf v600e mutation . 
takekuma m , wong kk , coleman rl : a long - term surviving patient with recurrent low - grade serous ovarian carcinoma treated with the mek1 / 2 inhibitor , selumetinib . 
weir hm , bradbury rh , lawson m , et al : azd9496 : an oral estrogen receptor inhibitor that blocks the growth of er - positive and esr1 - mutant breast tumors in preclinical models . 
chandarlapaty s , chen d , he w , et al : prevalence of esr1 mutations in cell - free dna and outcomes in metastatic breast cancer : a secondary analysis of the bolero - 2 clinical trial . 
 appendix description of test the oncopanel assay surveys exonic dna sequences of 300 cancer genes and 113 introns across 35 genes for rearrangement detection.11 dna is isolated from tissue containing at least 20% tumor and analyzed by massively parallel sequencing using a solution - phase agilent sureselect hybrid capture kit ( santa clara , ca ) and an illumina 2500 sequencer ( san diego , ca )  . 
 detection of somatic structural variants enables quantification and characterization of circulating tumor dna in children with solid tumors objective liquid biopsies are being rapidly used in adult cancers as new biomarkers of disease . 
therefore , we developed a next - generation sequencing approach to detect and quantify ctdna in the blood of patients with the most common pediatric solid tumors . methods detection of ctdna requires assays sensitive to somatic events typically observed in the cancer type being studied . 
we adapted an ultralow passage whole - genome sequencing approach to capture copy number variants and a hybrid capture sequencing assay to detect translocations in liquid biopsy samples from pediatric patients . results copy number changes seen by ultralow passage whole - genome sequencing enabled detection of ctdna in patients with osteosarcoma , neuroblastoma , alveolar rhabdomyosarcoma , and wilms tumor . 
we also found that disease - specific genomic biomarkers of prognosis were detectable in ctdna . conclusion this study demonstrates that liquid biopsy approaches that detect somatic structural variants are well suited to pediatric solid tumors . 
we show that children with the most common solid tumor malignancies have detectable levels of ctdna , which may be used to track disease response and identify genomic subclassifiers of disease . 
2018 by american society of clinical oncology introduction cancer remains one of the most common childhood causes of disease - related death in developed countries.1 patients with pediatric solid tumor malignancies are commonly treated with regimens that combine intensive chemotherapy , surgery , and radiation therapy.2 this approach has led to tremendous improvements in outcome , with overall cure rates for pediatric solid tumors now > 80%.3 however , these cures come at the cost of exposing patients to a high risk of long - term toxicities resulting in significant morbidity.4 in some diseases , such as wilms tumor , efforts to de - escalate therapy have resulted in stable cure rates for low - risk patients accompanied by reduced treatment toxicity.5 , 6 in other diseases , such as ewing sarcoma , a lack of prognostic biomarkers limit the ability to risk stratify therapy.7 , 8 in both cases , the development of new and more precise assays for risk stratification could improve outcomes by facilitating patient - specific treatment modifications . kelly klega alma imamovic - tuco gavin ha andrea n . 
crompton author affiliations and support information ( if applicable ) appear at the end of this article . the contents are solely the responsibility of the authors and do not necessarily represent the official views of the national institutes of health or other funding agencies . corresponding author : brian d . 
numerous studies have now demonstrated that circulating tumor dna ( ctdna ) levels in adults with cancer correlate with disease burden and track with treatment responses over time.9 - 14 the development of ctdna assays rely on identification and quantification of somatic mutations.9 , 15 many ctdna assays have been developed to detect highly recurrent hot - spot mutations that frequently drive adult malignancies.9 , 12 , 13 , 16 - 18 however , recent comprehensive sequencing efforts in pediatric cancers show that pediatric solid tumors are rarely driven by highly recurrent single - nucleotide variants.19 instead , structural variants , including chromosomal copy number changes and dna translocations , are common somatic events in these tumor types.20 - 26 to determine whether patients with childhood solid tumor malignancies express detectable levels of ctdna , we adapted two next - generation sequencing strategies to detect and quantify structural variants in the plasma of these patients . 
 we applied these assays to five of the most common types of pediatric solid tumors , excluding cns tumors , to quantify ctdna levels , identify genomic subtypes , and confirm the feasibility of using ctdna assays to track disease response to therapy . methods patients and tissue samples patients at the dana - farber cancer institute and boston childrens hospital were consented to an institutional review boardapproved protocol . 
patients were included if an initial peripheral blood , pleural effusion , or bone marrow sample was collected within 3 days from the start of chemotherapy and before a surgical resection . 
additional details are available in the data supplement . sequencing library preparation , sequencing alignment , and ultralow passage whole - genome sequencing coverage for all experiments , sequencing library preparation and sequencing data alignment were performed using standard techniques . 
additional details are available in the data supplement . translocation - specific sarcoma sequencing assay development and sequencing to detect pediatric sarcoma - specific translocations in cell - free dna , we developed a unique hybrid capture sequencing assay . 
first , we reviewed the literature to identify the genomic introns involved in oncogenic translocations in the ewsr1 , fus , cic , ccnb3 , pax3 , pax7 , and tp53 genes.20 , 21 , 25 - 33 second , we used the sureselect advanced design wizard ( agilent technologies , santa clara , ca ) to create capture probes targeting these regions and the coding regions of tp53 and stag2 with the following design options : sense strand , 3 tiling density , least stringent masking , balanced boosting , and region extensions of 10 bases from the 3 and 5 ends ( data supplement )  . 
the average measured coverage at enrichment sites for all samples tested by transs - seq was 655 ( range , 31 to 1 , 464 )  . sequencing analysis ulp - wgs analysis was performed using the ichorcna algorithm ( dinstitute / ichorcna ) , with manual curation of results.34 in brief , ulp - wgs uses relative sequencing coverage of whole - genome data and computational correction of sequencing bias to detect segmental copy number changes . 
 wild - type reads detected in each sample , we developed a custom algorithm designed to realign all sequencing reads to either the reference human genome or the patient - specific translocation positive reference sequence ( vanallenlab / peds_ctdna )  . 
the algorithm then reported the number of reads aligned at the patient - specific translocation breakpoint and the number of wild - type reads at the equivalent genomic base - pair location within the human reference genome . 
because each cancer genome contains one translocated and one wild - type allele , whereas germline genomes contain two wild - type alleles , we used the following formula to calculate the percentage of ctdna , where t equals the number of translocation reads and w equals the number of wild - type reads : % ctdna = t / { [ ( w - t ) / 2 ] + t }  . cell lines and digital droplet polymerase chain reaction the ew8 ewing sarcoma cell line dilution experiments , digital droplet polymerase chain reaction ( ddpcr ) methods , and ddpcr primers are listed in the data supplement . highest values originating from patients with neuroblastoma ( fig 1a )  . 
ulp - wgs was performed for each sample to detect and quantify ctdna by measuring segmental copy number changes as recently described.34 ctdna was detected in 50% of pretreatment plasma samples from patients with osteosarcoma , neuroblastoma , wilms tumor , and alveolar rhabdomyosarcoma . 
in patients with detectable ctdna , the pattern of segmental chromosomal copy number changes in cellfree dna matched the copy number pattern observed in the tumor biopsy from the same patient ( figs 1c and 1d ; data supplement )  . 
in four of the seven patients with ewing sarcoma with no detectable ctdna , ulp - wgs analysis of tumor biopsy dna material demonstrated no discernable segmental copy number changes ( fig 2 )  . 
this finding is consistent with previous reports that ewing sarcoma tumors have few highly recurrent somatic events other than the ewsr1 / ets translocations and suggests that an alternative method for detection of ctdna is necessary for this disease.21 , 26 results patients and samples a liquid biopsy sample was collected before the initiation of therapy from 45 pediatric patients with cancer with a confirmed diagnosis of ewing sarcoma ( n = 11 ) , osteosarcoma ( n = 10 ) , neuroblastoma ( n = 10 ) , wilms tumor ( n = 8 ) , or alveolar rhabdomyosarcoma ( n = 7 )  . 
dna from tumor biopsy material from patients with neuroblastoma and wilms tumor were not readily available . circulating tumor dna is detectable in patients with pediatric solid tumor malignancies total cell - free dna levels ranged from 2 ng to 3.5 g of dna per 1 ml of plasma , with the translocation detection outperforms copy number detection for ewing sarcoma to detect ctdna in translocation - positive tumors , we developed a novel hybrid - capture assay , termed transs - seq , designed to sequence intronic regions involved in genomic rearrangements in pediatric sarcomas . 
first , we confirmed that the assay could detect the expected translocations in a panel of ewing and ewing - like sarcomas and alveolar rhabdomyosarcomas ( data supplement )  . 
ddpcr in these samples confirmed the ability to detect and quantify the ew8 - specific ewsr1 / fli translocation across the range of dilutions ( fig 3a ; data supplement )  . 
 ( a ) quantity of cell - free dna extracted per ml of plasma or body fluid in patients with osteosarcoma ( ost ) , alveolar rhabdomyosarcoma ( arms ) , ewing sarcoma ( ews ) , wilms tumor ( wilms ) , and neuroblastoma ( nb )  . 
the color for each data point corresponds to the relative copy number change from baseline , with blue equal to two copies of the genomic location , green equal to copy number loss , and red equal to copy number gains . 
the same pattern of copy number changes is observed in dna sequenced from a tumor biopsy ( top ) and a pretreatment blood sample ( bottom ) in ( c ) a patient with osteosarcoma and ( d ) alveolar rhabdomyosarcoma . and detected ew8 dna at a concentration of 1.56% ( figs 3b and 3c ; data supplement )  . identical to the breakpoint observed from the tumor biopsy sample . transs - seq was then applied to cell - free dna samples from patients with ewing sarcoma and alveolar rhabdomyosarcoma . 
for five patients with ewing sarcoma and three patients with alveolar rhabdomyosarcoma , dna from tumor biopsy samples was also profiled by transs - seq ( data supplement )  . 
in all cases , the unique genomic breakpoint in the ctdna was previous studies in ewing sarcoma have used ddpcr assays that amplify patient - specific ews / ets translocations to measure ctdna levels in patients.36 - 38 to compare transs - seq with this previously validated approach , patient specific polymerase chain reaction primers were developed for a subset of ewing sarcoma and alveolar rhabdomyosarcoma samples ( data supplement )  . 
 mrd0006 ewing sarcoma mrd0019 ewing sarcoma 108765 14 16 18 20 23 x 108765 14 16 18 20 23 x 14 16 18 20 23 x 108765 14 16 18 20 23 x chromosome mrd0023 ewing sarcoma chromosome mrd0046 ewing sarcoma chromosome chromosome mrd0007 ewing sarcoma 108765 chromosome mrd0041 ewing sarcoma 108765 chromosome mrd0047 ewing sarcoma 14 16 18 20 23 x 108765 14 16 18 20 23 x 14 16 18 20 23 x 108765 chromosome fig 2 . 
genome - wide copy number plots from seven ewing sarcoma tumor biopsy samples detected by ultralow passage whole - genome sequencing in patients for which circulating tumor dna could not be detected from peripheral blood . 
in three of the four patients with ewing sarcoma for which no copy number change could be detected by ulp - wgs in the tumor ( mrd0006 , mrd0041 , mrd0047 ) , transsseq was able to detect an ewsr1 - fusion in the tumor and cell - free dna ( data supplement )  . 
in the fourth patient ( mrd0007 ) , transs - seq detected an ewsr1 / fli fusion in the tumor but not in cell - free dna ( data supplement )  . 
however , four patients with tumor necrosis < 70% ( mrd0031 , mrd0036 , mrd0040 , mrd0054 ) had detectable ctdna in at least one sample collected after initiation of chemotherapy ( fig 4d ; data supplement )  . 
 finally , in patients whose ctdna levels became undetectable with therapy but then experienced a clinical relapse or progression , ctdna was again detectable before the initiation of relapsed therapy ( fig 4b ; data supplement )  . genomic markers of poor outcome are detectable in ctdna we also examined whether disease - specific genomic markers of prognosis could be detected in ctdna . 
recent studies demonstrate that mutations in stag2 and tp53 may be associated with a worse outcome in ewing sarcoma.21 , 26 a frame - shift mutation in stag2 was detected by ctdna from one patient ( mrd0023 ) , and a mutation in tp53 was detected in another patient ( mrd0003 ; data supplement )  . 
in alveolar rhabdomyosarcoma , studies have demonstrated that patients with pax3 / foxo1 have a worse prognosis than patients with pax7 / foxo1 translocation.41 the foxo1 fluorescent in situ hybridization probe , which is used in the diagnostic work - up of alveolar rhabdomyosarcoma , confirms a foxo1 rearrangement but not the fusion partner . 
in osteosarcoma , copy number gains of chromosome arm 8q are associated with a poor outcome.42 - 44 ulp - wgs detected copy number gains in 8q in seven of nine osteosarcoma samples with detectable ctdna ( fig 1c ; data supplement )  . 
amplification of mycn is a well - established marker of poor prognosis in neuroblastoma.45 , 46 mycn amplification was detectable in the ctdna of two patients by ulp - wgs ( fig 5a ; data supplement )  . 
finally , in wilms tumor , copy number gains of 1q were associated with poor prognosis in favorable histology tumors.47 ulp - wgs detected 1q gain in copy number change but ulp - wgs was unable to detect ctdna from the same patient ( mrd0019 , mrd0023 , mrd0046 ) , transsseq detected low levels of ctdna , suggesting that transs - seq may have greater sensitivity for ctdna than ulp - wgs in ewing sarcoma ( data supplement )  . ctdna levels track with disease burden in pediatric solid tumors when comparing ctdna levels across cancer types , neuroblastoma demonstrated a significantly higher percentage of ctdna ( median , 55% ; range , 13% to 98% ) than other cancer types ( data supplement )  . 
in patients with newly diagnosed ewing sarcoma and alveolar rhabdomyosarcoma , ctdna levels declined rapidly after initiation of chemotherapy , often becoming undetectable by the start of the second cycle ( figs 4a and 4b ; data supplement )  . 
in osteosarcoma , studies have shown that a high percentage of tumor necrosis observed in the primary tumor after neoadjuvant chemotherapy is associated with a better prognosis.39 , 40 in five patients with newly diagnosed osteosarcoma , the percentage of tumor necrosis was available . 
the translocation - specific sarcoma sequencing assay ( transs - seq ) detects circulating tumor dna ( ctdna ) in ewing sarcoma ( ews ) and alveolar rhabdomyosarcoma ( arms )  . 
 samples are plotted on the x - axis by the percentage of ew8 by experimental dilution and on the y - axis by the percentage of ew8 dna detected by digital droplet polymerase chain reaction ( ddpcr )  . 
 ( d ) percentage of ctdna levels in cell - free dna samples from patients with ewing sarcoma and arms ( same samples as in figure 1b ) determined by transsseq . 
 percentage of ctdna levels from serial cell - free dna samples collected from four patients with ( a ) ewing sarcoma , ( b ) alveolar rhabdomyosarcoma , ( c - d ) osteosarcoma . 
blue dots indicate peripheral blood samples , and the red dot ( b ) indicates a bone marrow sample collected simultaneously with a blood sample . mrd0019 ewing sarcoma mrd0045 alveolar rhabdomyosarcoma bone marrow clinical course clinical course mrd0061 osteosarcoma mrd0036 osteosarcoma clinical course clinical course had detectable levels of ctdna . 
patients with neuroblastoma had the highest levels of ctdna , including two patients with > 1 g of cell - free dna per ml of plasma , which was nearly 100% composed of tumor dna . 
however , one obvious limitation to the use of ulp - wgs was in tumor types with low rates of copy number alterations , such as ewing sarcoma . recent liquid biopsy studies in ewing sarcoma have used the development of patient - specific ddpcr assays.36 - 38 although this approach has proven to be highly sensitive and quantitative , the development of each assay requires genomic profiling of large amounts of tumor biopsy material to establish the patient - specific oncogenic translocation . 
one recent study used a combination of ddpcr and hybrid capture sequencing to detect ewsr1 translocations in ewing sarcoma and desmoplastic small roundcell tumors.38 results showed that it is feasible to detect ewsr1 translocations directly from the plasma of these patients without first sequencing the tumor sample . 
despite the larger genomic region targeted for hybrid capture , the transs - seq assay detected ctdna in 10 of 11 pretreatment samples obtained from ewing sarcoma , similar to rates observed by other groups . 
we also demonstrated that quantification of ctdna levels was similar using either transs - seq or ddpcr . in this study , changes in ctdna levels were observed during a patients clinical course and corresponded to changes in disease burden . 
with next - generation sequencing becoming increasingly available for clinical decision making , we anticipate that our ctdna assays could also be adapted to clinical laboratory testing if they demonstrate significant improvements to risk stratification for pediatric solid tumors . 
 ( a ) sequencing coverage ( read counts ) across the mycn gene ( top ) and c - myc gene ( bottom ) from four cell - free dna samples from patients with neuroblastoma . 
therefore , prospective studies should be designed to obtain frequent samples throughout treatment so that the time points most predictive of outcome can be appropriately identified . finally , our study demonstrates that next generation sequencing of ctdna can detect existing genomic biomarkers of outcome and may provide another modality for genomic profiling of tumors in patients . 
furthermore , it remains unclear whether these genomic biomarkers are primarily clonal or heterogeneous events within a tumor or across tumors and whether the clonality of these genomic events changes in patients who relapse after therapy . 
recent studies demonstrate that ctdna can detect intratumor and multitumor heterogeneity and detect complex patterns of treatment resistance.52 - 55 with the emergence of new sequencing modifications that improve sensitivity and decrease sequencing errors , we believe that ctdna profiling by next - generation sequencing approaches will improve our understanding of tumor heterogeneity and patterns of somatic evolution in pediatric solid tumors.12 , 16 in addition , the assays described in this study could facilitate broader profiling of ctdna , such as deep whole - exome sequencing , by providing a mechanism to screen samples for the presence of sufficiently abundant ctdna , allowing selection of samples most likely to yield informative data . in summary , our study demonstrates that patients with pediatric solid tumors have detectable levels of ctdna , which can be measured with next generation sequencing approaches that do not require profiling of tumor biopsy material or patient - specific assays . 
disease - specific genomic hallmarks of pediatric solid tumors can also be identified in liquid biopsy samples , and ctdna levels correlate with disease burden and response to therapy over time . 
crompton manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors anwesha nag no relationship to disclose eliezer van allen stock and other ownership interests : syapse , tango therapeutics , genome medical consulting or advisory role : syapse , roche , third rock ventures , takeda , novartis , genome medical , invitae speakers ' bureau : illumina research funding : bristol - myers squibb , novartis elizabeth mullen no relationship to disclose steven g . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . katherine janeway no relationship to disclose matthew meyerson stock and other ownership interests : origimed consulting or advisory role : origimed research funding : bayer ( inst ) patents , royalties , other intellectual property : patent on egfr mutations for lung cancer diagnosis aaron r . 
crompton employment : mersana ( i ) , shire ( i ) stock and other ownership interests : mersana ( i ) , shire ( i ) acknowledgment we thank the boston childrens hospital biorepository for processing a portion of the blood samples . 
pediatr blood cancer 60 : 1083 - 1094 , 2013 kelly klega no relationship to disclose alma imamovic - tuco no relationship to disclose gavin ha no relationship to disclose andrea n . 
bhakta n , liu q , ness kk , et al : the cumulative burden of surviving childhood cancer : an initial report from the st jude lifetime cohort study ( sjlife )  . 
fernandez cv , perlman ej , mullen ea , et al : clinical outcome and biological predictors of relapse after nephrectomy only for very low - risk wilms tumor : a report from childrens oncology group aren0532 . 
oxnard gr , paweletz cp , kuang y , et al : noninvasive detection of response and resistance in egfr - mutant lung cancer using quantitative next - generation genotyping of cell - free plasma dna . 
parkinson ca , gale d , piskorz am , et al : exploratory analysis of tp53 mutations in circulating tumour dna as biomarkers of treatment response for patients with relapsed high - grade serous ovarian carcinoma : a retrospective study . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
yung tk , chan kc , mok ts , et al : single - molecule detection of epidermal growth factor receptor mutations in plasma by microfluidics digital pcr in non - small cell lung cancer patients . 
shern jf , chen l , chmielecki j , et al : comprehensive genomic analysis of rhabdomyosarcoma reveals a landscape of alterations affecting a common genetic axis in fusion - positive and fusionnegative tumors . 
tirode f , surdez d , ma x , et al : genomic landscape of ewing sarcoma defines an aggressive subtype with co - association of stag2 and tp53 mutations . 
kawamura - saito m , yamazaki y , kaneko k , et al : fusion between cic and dux4 up - regulates pea3 family genes in ewing - like sarcomas with t ( 4 ; 19 ) ( q35 ; q13 ) translocation . 
ng tl , osullivan mj , pallen cj , et al : ewing sarcoma with novel translocation t ( 2 ; 16 ) producing an in - frame fusion of fus and fev . 
sugita s , arai y , tonooka a , et al : a novel cic - foxo4 gene fusion in undifferentiated small round cell sarcoma : a genetically distinct variant of ewing - like sarcoma . 
yoshimoto m , graham c , chilton - macneill s , et al : detailed cytogenetic and array analysis of pediatric primitive sarcomas reveals a recurrent cic - dux4 fusion gene event . 
shukla nn , patel ja , magnan h , et al : plasma dna - based molecular diagnosis , prognostication , and monitoring of patients with ewsr1 fusion - positive sarcomas . 
meyers pa , schwartz cl , krailo m , et al : osteosarcoma : a randomized , prospective trial of the addition of ifosfamide and / or muramyl tripeptide to cisplatin , doxorubicin , and high - dose methotrexate . 
sorensen ph , lynch jc , qualman sj , et al : pax3 - fkhr and pax7 - fkhr gene fusions are prognostic indicators in alveolar rhabdomyosarcoma : a report from the childrens oncology group . 
tarkkanen m , elomaa i , blomqvist c , et al : dna sequence copy number increase at 8q : a potential new prognostic marker in high - grade osteosarcoma . 
gratias ej , dome js , jennings lj , et al : association of chromosome 1q gain with inferior survival in favorable - histology wilms tumor : a report from the childrens oncology group . 
lecomte t , berger a , zinzindohou f , et al : detection of free - circulating tumor - associated dna in plasma of colorectal cancer patients and its association with prognosis . 
tie j , wang y , tomasetti c , et al : circulating tumor dna analysis detects minimal residual disease and predicts recurrence in patients with stage ii colon cancer . 
vora a , goulden n , mitchell c , et al : augmented post - remission therapy for a minimal residual disease - defined high - risk subgroup of children and young people with clinical standard - risk and intermediate - risk acute lymphoblastic leukaemia ( ukall 2003 ) : a randomised controlled trial . 
de mattos - arruda l , weigelt b , cortes j , et al : capturing intra - tumor genetic heterogeneity by de novo mutation profiling of circulating cell - free tumor dna : a proof - of - principle . 
thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . 
 c smo syndrome : a unifying molecular diagnosis that suggests therapeutic opportunities introduction classically , diseases have been given eponymous or descriptive labels , but , as dna sequencing has revealed the same causal variants in ostensibly different disorders , 1 this inevitably has led to reappraisal of whether entities are better referred to by their underlying genetics or by their apparently distinct phenotypic appearance . 
moreover , the identification of common molecular mechanisms that underlie seemingly distinct syndromic entities can have therapeutic implications . the sonic hedgehog ( shh ) pathway is an important signaling cascade in development and cancer . 
germline pathogenic variants in ptch1 are responsible for 67% to 85%2 of occurrences of nevoid basal cell carcinoma syndrome ( nbccs ) , a condition characterized by multiple basal cell carcinomas ( bccs ) , calcification of the falx cerebri , palmoplantar pitting , odontogenic keratocysts , and other rare features . 
smaller contributions from ptch2 have been reported in patients with nbccs , 3 and germline mutations in sufu are described in approximately 5% of nbccs cases with a strong association to medulloblastoma development.4 ptch1 is a tumor suppressor gene that downregulates smoothened ( smo ) oncogenic activity in the shh pathway . 
recently , a unique mosaic activating mutation in smo c.1234c > t [ p.leu412phe ] has been reported as the only known cause of curry - jones syndrome ( crjs ) .5 crjs is a rare multisystem disorder that features iris colobomas , asymmetric facies , unilateral craniosynostosis , polydactyly , cutaneous syndactyly , intellectual disability , cerebral malformation , areas of hypopigmentation , ectopic hair growth , and structural and functional gi anomalies.5 cancer has not been reported in crjs . mosaicism occurs during postzygotic development with the gain of a mutation that results in localized or less severe phenotypes than congenital alterations.6 in 1987 , happle7 postulated that some conditions with a mosaic presentation of their phenotype are the result of mosaic activating mutations in oncogenes that are embryonically lethal . lack of confirmation of a clinical diagnosis after genetic testing of blood dna may suggest the presence of a mosaic alteration , but assessment of mosaicism is challenging , because only comprehensive studies that include testing of several tissue and high - sensitivity assays can provide conclusive answers . 
in addition , he has had one bcc on the right side of the upper chest , two on the back ( left and right ) , four on the scalp ( two left sided ) , and one on each side of the sternuhe was born with his left eyelid closed , and visual acuity in this eye was markedly reduced by the age 40 years . on examination , he had facial asymmetry , left iris coloboma , microphthalmia of the left eye , and an ectopic patch of hair under this eye ( figs 1a and 1b )  . 
short thin gold arrow , left frontal sinus ; long thin gold arrow , left maxillary sinus ; short thick blue arrow , right frontal sinus ; long thick blue arrow , right maxillary sinus . 
 magnetic resonance imaging , fluid attenuation inversion recovery acquisition of ( d ) axial , ( e ) coronal , and ( f ) left parasagittal contrast enhanced 1.5 - t , t1 weighted magnetic resonance images that show extensive polymicrogyria lining and deep , irregular sulci within the left middle frontal gyrus ( white arrows )  . 
contrast magnetic resonance imaging with gadolinium showed marked left - sided polymicrogyria that involved the left frontal lobe and anterior parietal region as well as cranial asymmetry with a smaller left hemisphere ( figs 1d - 1f ; data supplement )  . 
only one likely causal variant was common to all bccs and absent in blood dna : c.1234c > t ( p.leu412phe ) in smo ( figs 1g and 1h ; data supplement )  . 
the list of genes found to be altered in one or more of the bccs and the complete list of variants that passed our filters are provided in the data supplement . 
histogram shows the fractional abundance of mutant allele smo c.1234c > t ; p.leu412phe ( mut ) compared with the wild - type ( wt ) allele c.1234c by high - sensitivity ddpcr in a total of 29 samples from the proband and germline dna from nine healthy controls ( healthy c )  . 
moreover , we tested a total of 11 extra samples from the proband in the assay , including dna from a fibroblasts cell line derived from normal tissue adjacent to a tumor , dna from the tonsils that were removed at 5 years of age ( tonsil ) , dna from a swab of the right mouth epithelia ( m - epi - r ) and the left mouth epithelia ( m - epi - l ) , two different samples of saliva ( slv and slv - 2 ) , germline dna from blood ( blood ) , dna from a lymphoblastic cell line ( lcls ) , and dna from hair from the right and left side ( hair - r and hair - l , respectively )  . 
the nine healthy controls show fractional abundances of 0 to 0.02 , with the maximum total of positive droplets for the mutant allele in a healthy control of four of 21 , 307 wt droplets . 
moreover , somatic mosaicism for the identical smo mutation has been identified as the cause of crjs.5 recently the same oncogenic mutation has been identified in a case reported as mosaic nbccs but considered by others to represent happle - tinschert syndrome ( hts ) .8 , 9 it has also been found in a patient definitively diagnosed with hts , the main feature of which is the development of basaloid follicular hamartomas.10 we then quantified the mutation in 29 samples from the patient , including 15 normal tissues and 14 bccs , using high - resolution digital droplet polymerase chain reaction . 
 basal follicular hamartomas optic glioma hyperlipidemia macroglossia dysplastic ears cutaneous ossification lipodermoidof the conjunctiva ntal b r pits etin al d ntal a rtric alie nbccs basal cell carcinoma calcification of falx epidermal cysts ovarian fibromas benign tumours cutaneous syndactyly iris coloboma microphthalmia polymicrogyria * medulloblastoma cognitive anomalies polydactyly skeletal / cranial / cerebral anomalies pigmentation cataracts intestinal anomalies hemimegancephaly ectopic hair naevi cleft lip and palate okc macrocephaly cjrs asymmetric face heart anomalies trichoblastoma lymphangiomas instestinal hamartomas glaucoma fig 3 . 
comparison of the major reported features of nevoid basal cell carcinoma syndrome ( nbccs ) , curry - jones syndrome ( crjs ) , happle - tinschert syndrome ( hts ) , and the proband phenotype . 
in contrast , the mutation was detectable in fibroblast dna , in dna from normal tissue adjacent to bccs , in the left mouth epithelium ; a very low level was detected in the tonsils ( fig 2 ) , which confirmed its mosaic nature . our patient showed substantial phenotypic overlap between the reported features of crjs , hts , and nbccs ( fig 3 )  . 
the collection of driver mutations found in our patients bccs exhibited similarities with the altered pathways in medulloblastoma , in accordance with the catalog of driver mutations in recently described bccs ( data supplement )  . malfunctions of shh pathway members early in development lead to a wide range of neoplastic and non - neoplastic complications , which reflects the importance of the signaling levels in the outcome phenotype . 
in our patient , the presence of palmar pits and multiple bccs is shared with nbccs , 2 and polymicrogyria and facial asymmetry is shared with crjs and hts ( fig 3 ) .5 , 11 polymicrogyria , a disorder that affects the development of the cortex that features epilepsy and developmental delay , 12 has been reported in two of 11 occurrences of crjs.5 there is only one occurrence of polymicrogyria reported in the more commonly occurring nbccs , and this case was not confirmed molecularly.13 the mild presentation of disease in our patient compared with those of other reported patients with crjs , and the large phenotypic overlap shown in figure 3 , could suggest that some patients with negative clinical testing for ptch1 , sufu , and ptch2 may have been misdiagnosed with nbccs but may unknowingly have , genotypically , crjs . currently , vismodegib , an smo antagonist , can be used to treat patients with bccs . 
 our findings confirm that widely distributed somatic variants in genes other than ptch1 can cause bcc and that people with mosaic smo mutations might be at substantial lifetime risk for bcc . 
thus , molecular screening of several tissues , including bccs , is required for patients with suspected nbccs and no identified germline ptch1 pathogenic variant , because the presence of this smo mutation could allow more precise management . 
foulkes no relationship to disclose unsuspected smo activating mutations.15 this case highlights the difficulty faced in diagnosis of a rare mosaic condition and the need for molecular genetic testing to aid this process . identification of the causal variant has affected medical management . 
smo mutations have been reported in meningiomas , 16 medulloblastoma , 17 and ameloblastomas18 ; thus , we have initiated tumor surveillance with annual head and brain magnetic resonance imaging . 
also , the identification of a mosaic mutation means that the patient 's antecedents and siblings are not at risk for bcc or other nbccs - related disorders . in the current era , integration of molecular data is becoming fundamental to clarify clinical diagnosis and improve patient management . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . barbara rivera no relationship to disclose acknowledgment we thank the proband of this study for his tireless support along the course of the study . 
we thank the lablink facility in the centre for applied genomics ( toronto ) for their support with the digital - droplet polymerase chain reaction experiments . affiliations barbara rivera , a . 
foulkes wd , clarke ba , hasselblatt m , et al : no small surprise : small cell carcinoma of the ovary , hypercalcemic type , is a malignant rhabdoid tumor . 
twigg srf , hufnagel rb , miller ka , et al : a recurrent mosaic mutation in smo , encoding the hedgehog signal transducer smoothened , is the major cause of curry - jones syndrome . 
happle r : lethal genes surviving by mosaicism : a possible explanation for sporadic birth defects involving the skj am acad dermatol 16 : 899 - 906 , 1987 8 . 
happle r , tinschert s : happle - tinschert syndrome can be caused by a mosaic smo mutation and is suggested to be a variant of curry - jones syndrome . 
spector , md1 , 2 , 4 purpose the veterans health administration ( vha ) is the largest cancer care provider in the united states , with the added challenge of serving more than twice the percentage of patients with cancer in rural areas than the national average . 
the vha established the national precision oncology program in 2016 to implement and standardize the practice of precision oncology across the diverse vha system . methods tumor or peripheral blood specimens from veterans with advanced solid tumors who were eligible for treatment were submitted for next - generation sequencing ( ngs ) at two commercial laboratories . 
levelsof - evidence treatment recommendations were based on oncokb criteria . results from july 2016 to june 2018 , 3 , 698 samples from 72 vha facilities were submitted for ngs testing , of which 3 , 182 samples ( 86% ) were successfully sequenced . 
the most frequent therapies prescribed in response to ngs testing were immune checkpoint inhibitors , egfr kinase inhibitors , and parp inhibitors . conclusion clinical implementation of precision oncology is feasible across the vha health care system , including rural sites . 
the use of us food and drug administration ( fda ) approved therapies that target specic tumor mutations requires genomic analysis to demonstrate mutation expression in tumor tissue or circulating tumor dna ( ctdna )  . 
the development of scalable , cost - effective , high - throughput next - generation sequencing ( ngs ) technologies has made tumor molecular proling practical for clinical care . the veterans health administration ( vha ) is the largest integrated health care system in the united states and the largest provider of cancer care in the country . 
approximately 50 , 000 new cancer cases are reported annually through the veterans affairs central cancer registry.1 veterans receive cancer care in vha facilities across 152 hospitals and 1 , 400 clinics nationwide . with a common , systemwide electronic medical record system , the vha represents an ideal health care system to establish a nationwide , clinical - genomic precision oncology program and database . 
 poonnen et al context key objective what were the ndings of molecular testing of advanced solid - tumor malignancies performed through the veterans health administration national precision oncology program ? knowledge generated from july 2016 to june 2018 , 3 , 182 samples were sequenced , of which 34% were from patients in rural areas . 
mutations in genes associated with a neuroendocrine prostate cancer phenotype were expressed at increased frequency among veterans than in the general population . relevance our ndings demonstrate the feasibility of implementing a large - scale precision oncology program across heterogenous and geographically dispersed systems such as the vha , including rural settings with limited pathology infrastructure . veterans remain a unique population in terms of demographics and exposure history ; comparison between veteran and civilian tumor mutational proles may shed light on tumorigenesis and potential etiologies for unidentied mutational signatures . in addition , 36% of vha patients with cancer live in rural areas , compared with the national average of 14%.2 the vha established the national precision oncology program ( npop ) in 2016 to address these challenges.3 the npop was tasked with creating guidelines for genomic testing of clinical tumor samples across the vha health care system ; a particular emphasis was placed on making ngs technologies available to veterans in rural areas , facilitating access to fda - approved targeted therapies and immune checkpoint inhibitors , and increasing participation in clinical trials . 
here , we discuss the genomic prole of the 3 , 182 samples that were successfully sequenced through the npop and the targeted or immunotherapeutic drugs administered on the basis of molecular testing . methods patients genomic testing was recommended for patients with advanced solid tumors who were medically eligible to receive additional treatment with a targeted or immunotherapeutic drug . 
veterans with rural - urban commuting area codes greater than one , based on their zip code , received a rural designation , as dened by the vha ofce of rural health . tumor sequencing formalin - xed , parafn - embedded tumor sections or peripheral blood specimens for ctdna testing were sent two clinical laboratory improvement amendmentscertied genomic laboratories : personalis ( menlo park , ca ) or personal genome diagnostics ( pgdx ; to one of baltimore , md )  . 
molecular testing was performed using one of ve panels ( pgdx cancerselect 88 , 125 , and 203 ; personalis ace cancerplus ; and pgdx plasmaselect 64 ) included between 64 and 203 cancer - associated that genes with a large degree of overlap among the panels . samples submitted to personalis were sequenced at 500 - fold coverage , and those submitted to pgdx were sequenced between 1 , 000and 1 , 500 - fold coverage to improve the sensitivity of testing and identication of lowfrequency mutated alleles . 
tumor mutational burden ( tmb ) was dened and calculated using ibm watson for genomics ( wfg ) ( armonk , ny ) methodology ( appendix ) and was only available to providers through vha precision oncology consultation . hematoxylin and eosinstained slides were analyzed by a pathologist at the testing laboratories to verify tumor histology and the percent tumor content in each sample . additional details of these commercial tests can be found on the pgdx and personalis websites . levels of evidence for actionable mutations annotated clinical reports of mutations identied by ngs testing were provided by pgdx and personalis . 
on the basis of data in the variant call les , ibm wfg provided a second annotated report that included fda - approved targeted therapies and immunotherapies and available trials . 
of the samples submitted for ngs testing , 35% were from patients in rural areas , which is consistent with the higher percentage of vha patients with cancer who live in rural areas , compared with the rest of the nation.2 the demographics of the patients tested in the npop were consistent with a recent report from the va central cancer registry , 5 with men comprising 97% of vha patients with cancer and a median age of approximately 72 years ( fig 1b )  . 
adenocarcinomas of the lung , colon , and prostate were the three most frequent tumor types tested ( fig 1c ) , at 18% , 8% , and 29% , respectively , which is consistent with their prevalence among vha patients with cancer.5 molecular analysis the quantity and quality of dna obtained from tumor biopsy specimens can vary depending on the tumor type , biopsy site , and type of biopsy performed . 
fine - needle biopsies are more likely to yield inadequate dna content compared with biopsy specimens from larger - bore core needles.6 , 7 needle biopsy specimens of lung cancer , which often have signicant stromal tissue , and bone metastases are more likely to be associated with a low yield of tumor dna , often insufcient for ngs testing.8 , 9 of the 3 , 698 samples submitted for molecular analysis , 3 , 182 ( 86% ) had sufcient quantity and quality of tumor dna to be successfully sequenced . 
the ctdna assay ( plasmaselect 64 ) comprised 4% of the total samples submitted for sequencing ( appendix table a1 )  . the average turnaround time was 19 days . the most frequently mutated gene in our patient population , regardless of tumor type , was tp53 . 
mutations in tp53 were identied in 66% of all sequenced samples . atm was the second most frequently mutated gene , occurring in 28% of samples , followed by kras mutations ( 27% )  . 
these ndings were consistent with reports in other genomic databases ( eg , the cancer genome atlas , memorial sloan kettering integrated mutation proling of actionable cancer targets ) where there was a high frequency of tp53 mutations in lung , esophageal , colorectal , and breast cancers.10 , 11 unexpectedly , in prostate cancers sequenced through the npop , mutations in smarca4 , crebbp , tsc2 , kmt2a , and notch1 were more prevalent than mutations in ar , pik3ca , and kras.12 - 15 other tumor types had expected mutation frequencies , including glioblastoma , in which egfr mutations , notably the egfrviii mutation , are common.16 we also identied 10 ntrk gene rearrangements . 
these included etv6 - ntrk3 fusions in patients with nonsmallcell lung cancer , papillary thyroid cancer , and adenocarcinomas of the colon and breast ( appendix table a3 )  . ntrk gene rearrangements are clinically relevant with the recent fda approval of larotrectinib , an ntrk inhibtumors expressing ntrk gene itor for treatment of rearrangements.17 treatment recommended and prescribed clinical annotations of ngs results were provided by pgdx and personalis , in addition to a separate wfg analysis . 
the breakdown of treatment recommendations on the basis of levels of evidence in each of the most frequent tumor types is shown in fig 3b . overall , an actionable mutation was identied in 70% of tumors the samples sequenced . 
a level 2b treatment recommendation for off - label use of a targeted drug or immunotherapy in a different tumor type from the fda - approved indication was made in 9% of the cases . 
most samples ( approximately 52% ) expressed one or more actionable mutations for which there was no fda - approved therapy , either on or off label . under these circumstances , a clinical trial was the recommended treatment option ( levels of evidence 3a and b )  . not surprisingly , we found that tumors such as melanoma , for which there are several fda - approved targeted therapies on the basis of a relatively high frequency of braf mutations , had the highest percentage of level 1 treatment recommendations ( fig 3b )  . a total of 136 patients received the fda - approved targeted therapy or immunotherapy recommended in the annotated clinical report , either onor off - label , on the basis of the ngs results . 
programmed cell death protein 1 ( pd - 1 ) / programmed death - ligand 1 ( pd - l1 ) targeted immune checkpoint inhibitors were the most frequently prescribed treatment after ngs results . 
many of the patients who received immune inhibitors had advanced - stage lung adenocheckpoint carcinoma , for which checkpoint inhibitors are fda approved as a rstor second - line therapy without requiring ngs testing . 
twenty of these patients received an fdaapproved egfr tyrosine kinase inhibitor ( eg , erlotinib , osimertinib ) on the basis of the presence of exon 19 deletions or an exon 21 missense mutation ( l858r ) that leads to constitutive activation of egfr . 
nine patients were treated with crizotinib or alectinib , including ve with an emla4 - alk translocation , and two each for a ros1 translocation and met splice variants , respectively . 
two patients with braf v600e mutations received braf - mek inhibitors ( fig 4 )  . thirteen patients with advanced castration - resistant prostate cancer were treated with targeted therapies or immune checkpoint inhibitors on the basis of ngs ndings . 
seven patients with pathogenic mutations in dna repair genes were treated off - label with an fda - approved parp inhibitor , including four patients with brca1 and brca2 frameshift mutations and three patients with pathogenic atm and atr mutations . 
four patients with msi - high status , high tmb , or pathogenic mutations in specic dna mismatch repair gene ( eg , mlh1 ) were treated with an immune checkpoint inhibitor ( fig 5 )  . the 27 patients with colorectal cancer whose treatment was selected according to the ngs results , four were treated with a pd - 1 checkpoint inhibitor , on the basis of msi - high status or high tmb . 
 a highest level of watson evidence across all patients other : 29.3% level 3b : 40.8% level 1 : 8.4% level 2a : 1.1% level 2b : 8.9% level 3a : 11.5% poonnen et al lung cancers ( 1 , 461 ) colon adenocarcinoma ( 327 ) prostate cancers ( 320 ) unknown primary origin ( 251 ) melanoma ( 162 ) h & n squamous cell carcinoma ( 78 ) rectal adenocarcinoma ( 70 ) pancreatic adenocarcinoma ( 67 ) esophageal adenocarcinoma ( 56 ) urothelial carcinoma ( 48 ) renal cell carcinoma ( 42 ) gastric adenocarcinoma ( 40 ) hepatocellular carcinoma ( 36 ) breast adenocarcinoma ( 21 ) other ( 409 ) fig 3 . 
 ( a ) actionable alterations were annotated using watson for genomics ( wfg ) according to oncokb levels of evidence : food and drug administration ( fda ) - recognized predictive biomarkers ( level 1 ) , standard - ofcare biomarkers predictive of response to fda - approved therapies ( level 2 ) , and biomarkers predictive of response to therapeutic agents currently under investigation ( level 3 ) , with levels 2 and 3 further categorized by whether evidence existed for the particular tumor type in question ( 2a , 3a ) or a different tumor type ( 2b , 3b )  . 
recent published data from the centers for disease control and prevention indicate rural areas in the united states have higher cancer mortality rates than do urban areas , despite lower adjusted cancer incidence rates.18 moreover , although adjusted death rates for all cancer sites are decreasing , the decrease is at a slower pace in rural areas , further widening the rural - urban disparity in cancer - related mortality.18 one factor contributing to the widening gap in cancer death rates seems to be limited access to health care and cutting - edge technologies in rural areas . 
we made a concerted effort to enroll rural vha facilities in the npop and worked closely with pathologists at rural sites to improve the selection of samples for ngs testing to improve testing success rates . 
the result of these efforts was an 86% success rate for sequencing samples across the vha system , comparable to rates reported in other largescale characterization studies performed largely at academic centers.11 , 19 - 22 we implemented blood - based ctdna assays to enable rural sites with limited pathology infrastructure to participate in the program through a simple blood collection . 
the npop experience , therefore , may inform strategies to maximize participation of patients with cancer who live in rural areas in precision medicine programs in other health care systems . we found numerous similarities in the overall mutational pattern among the veteran population to previous molecular proling studies performed in the general population . for example , tp53 was one of the most commonly mutated genes in the vha cancer population , consistent with previous large - scale molecular proling efforts outside the vha.11 , 19 , 23 - 25 kras mutations were identied in more than one - fth of our patients , with the majority occurring in gi malignancies . 
these ndings are clinically signicant , because pathogenic kras , nras , and braf mutations are associated with therapeutic resistance to fdaapproved antibodies and small molecules targeting egfr in colorectal and nonsmall - cell lung cancers , respectively.26 mutations in apc , pik3ca , crebbp , and several other genes have been associated with oncogenesis in more common malignancies such as colorectal , lung , and breast carcinomas . 
although no targeted therapies are currently approved for these mutations , pi3k inhibitors are showing promising clinical activity in breast cancers that express activating pik3ca mutations.27 similarly , therapies are in development that specically target colorectal cancers that express mutant apc.28 mutations in alk , ros1 , and ret already have corresponding targeted therapies that are fda approved in several malignancies.29 analysis of our data showed several differences in both overall and specic frequency of gene variants . 
 ( a ) distribution of actionable mutations ( ie , eligible for onor off - label use of a food and drug administrationapproved targeted therapy or immune checkpoint inhibitor on the basis of ngs test results ) demonstrated by ngs . 
msi - h , microsatellite instabilityhigh ; tmb , tumor mutational burden . mutations were identied in almost one - quarter of all patient samples sequenced through the npop , which seems to be a higher rate than those reported in other non - vha studies.11 , 24 atm plays a key role in repair of dna doublestrand breaks . 
however , the relatively increased rate of pathogenic atm mutations seen in our patient population , particularly those with gastric or neuroendocrine tumors , may provide a potential therapeutic target , because preliminary clinical data suggest benet from the use of parp inhibitors in atm - decient cancers.30 atm and mutations in other dna mismatch repair genes have been linked to germline mutations . 
although we did not sequence normal tissue as part of the npop , patients whose tumors expressed potential germline mutations were offered genetic counseling . the molecular architecture of prostate cancers sequenced through the npop seems to differ from that previously reported in large , non - vha , prostate cancer genomic databases . 
 ( a ) distribution of actionable mutations ( ie , eligible for onor off - label use of an food and drug administrationapproved targeted therapy or immune checkpoint inhibitor on the basis of ngs test results ) demonstrated by ngs . 
tmb , tumor mutational burden . however , the frein neuroendocrine prostate cancers , quency of kmt2a mutations has been reported to be 14% , with similar ndings for dnmt2 and crebbp.13 transformation from prostate adenocarcinoma to a neuroendocrine phenotype has been reported in approximately 17% of patients , coincident with disease progression.32 that process is thought to be multifactorial , including specic gene rearrangements and epigenetic changes that were not tested here.13 although patients whose tumors were sequenced almost universally had advanced prostate cancer , the majority of samples sent for sequencing were from the original archived prostate biopsy specimens rather than metastatic sites of disease . 
therefore , we speculate that these genomic features suggestive of a neuroendocrine phenotype may have been present before initiation of androgen - deprivation therapy . overall differences in the genomic signatures in our patient population compared with previous non - vha studies are likely to be multifactorial in etiology . 
as previously posited , veterans represent a demographically unique population ; the vast majority of patients reported here were men , which skews ndings toward proles associated with common male cancers ( ie , lung , prostate , colorectal )  . 
veterans also differ from the general population in their occupational exposure history ( eg , agent orange ) , which increases risk of specic tumor types and may lead to a distinct mutational prole , compared with sporadic cases of similar histology . additional investigation directly comparing the mutational signatures of tumors sequenced through the npop to those of patients in the general population may be crucial to link particular occupational or environmental exposures to mutations expressed in their tumors . importantly , we have shown that implementation of ngs testing inuenced the treatment of veterans across the country . 
 ( a ) distribution of actionable mutations ( ie , eligible for onor off - label use of food and drug administrationapproved targeted therapy or immune checkpoint inhibitor on the basis of ngs test results ) demonstrated by ngs . 
kelley consulting or advisory role : astrazeneca , eisai , ibm japan research funding : bavarian nordic , novartis , astrazeneca , bristol - myers squibb other relationship : ibm neil l . 
spector stock and other ownership interests : eydis bio , bessor pharma research funding : immunolight patents , royalties , other intellectual property : i am on a patent related to my work with the company immunolight , and i am listed on a patent through eydis bio no other potential conicts of interest were reported . acknowledgment this project is a clinical / operational endeavor under the heading of the veterans health administration ( vha ) national precision oncology program , and our manuscript is a reporting of the results ( at 2 years ) of this clinical prograsimilar to funding for other aspects of veteran clinical care through the vha ( eg , laboratory testing , imaging , drugs / therapies ) , funding for the program is provided by national congressional budgeting ( either as a separate program or under general veterans health administration hematology / oncology funding ) , and no outside ( eg , industry , pharmaceutical ) funding sources are used for the program . details of this funding are publicly available as a matter of congressional budgeting . 
us department of veterans affairs ofce of research and development : precision oncology prograchakravarty d , gao j , phillips sm , et al : oncokb : a precision oncology knowledge base . 
mil med 182 : e1883 - e1891 , 2017 schneider f , smith ma , lane mc , et al : adequacy of core needle biopsy specimens and ne - needle aspirates for molecular testing of lung adenocarcinomas . am j clin pathol 143 : 193 - 200 , quiz 306 , 2015 ukasiewicz e , ziemiecka a , jakubowski w , et al : fine - needle versus core - needle biopsy which one to choose in preoperative assessment of focal lesions in the breasts ? literature review . 
j ultrason 17 : 267 - 274 , 2017 richter pd , ilacqua j : correlation between biopsy type and insufcient tissue availability for biomarker testing in ve solid cancer types . 
wu js , goldsmith jd , horwich pj , et al : bone and soft - tissue lesions : what factors affect diagnostic yield of image - guided core - needle biopsy ? radiology 248 : 962 - 970 , 2008 10 . 
henley sj , anderson rn , thomas cc , et al : invasive cancer incidence , 2004 - 2013 , and deaths , 2006 - 2015 , in nonmetropolitan and metropolitan counties united states . 
harris mh , dubois sg , glade bender jl , et al : multicenter feasibility study of tumor molecular proling to inform therapeutic decisions in advanced pediatric solid tumors : the individualized cancer therapy ( icat ) study . 
aggarwal r , huang j , alumkal jj , et al : clinical and genomic characterization of treatment - emergent small - cell neuroendocrine prostate cancer : a multiinstitutional prospective study . 
 poonnen et al appendix methods : assessment of tumor mutational burden tumor mutational burden ( tmb ) was dened as the number of coding , nonsynonymous mutations divided by the target region , which is estimated as the size of the genome ( in mbps ) covered by the assay . 
of samples ( % ) ( n = 111 ) tumor type lung prostate carcinoma of unknown primary pancreatic adenocarcinoma colon adenocarcinoma hepatocellular carcinoma esophageal adenocarcinoma duodenal adenocarcinoma cholangiocarcinoma follicular lymphoma 42 ( 38 ) 27 ( 24 ) 14 ( 13 ) 7 ( 6 ) 4 ( 4 ) 2 ( 2 ) 2 ( 2 ) 1 ( 1 ) 1 ( 1 ) 1 ( 1 ) table a2 . 
 fundamental concepts in the application of plasma genotyping ( liquid biopsy ) to egfr mutation detection in nonsmall - cell lung cancer plasma genotyping has rapidly evolved from an investigational technology into a standard - of - care tool used to direct therapy in metastatic nonsmall - cell lung cancer ( nsclc )  . 
the optimal use and interpretation of plasma genotyping requires understanding of cell - free dna biology , the assay characteristics of the available testing technologies , and the application of testing in each clinical scenario . 
 current recommendations for plasma genotyping in metastatic nsclc are limited to patients with newly diagnosed disease and those with acquired resistance to targeted therapy , in particular , epidermal growth factor receptor ( egfr ) kinase inhibitors . 
in newly diagnosed metastatic nsclc , under certain circumstances , plasma genotyping is useful for the detection of targetable genomic alterations or nontargetable driver alterations ( eg , kras ) that are mutually exclusive with targetable alterations . 
in patients with acquired resistance to therapy , such as egfr t790m - mediated acquired resistance to egfr kinase inhibitors , plasma genotyping may detect resistance mutations missed by standard tissue genotyping because of tumor heterogeneity . 
in both scenarios , the high specificity and positive predictive value of validated plasma genotyping assays allow for the reliable selection of therapy on the basis of a positive plasma genotyping result . 
this technology has become commonplace in prenatal research as well as cancer diagnostics and biomarker research.1 - 6 liquid biopsy has emerged as the colloquial term for the specific use of cfdna genotyping analysis to interrogate plasma , urine , and csf.7 , 8 this technology has been piloted in multiple solid tumor types to detect specific genomic alterations.2 , 4 , 5 its potential utility has been best demonstrated in lung cancer , where the rapid detection of targetable genomic alterations is key to selecting optimal systemic therapy.9 , 10 liquid biopsy technology has inarguably entered the realm of standard care in the treatment of nonsmall - cell lung cancer ( nsclc ) .11 , 12 multiple platforms for performing liquid biopsy have been evaluated for the detection of targetable genomic alterations in metastatic nsclc.9 , 10 , 12 - 20 the most rigorous of these studies have used either prospective sample testing or batched testing of samples collected from prospective clinical trials compared with standard tissue genotyping . 
 ( fda ) approval of a liquid biopsy assay using the cobas epidermal growth factor receptor ( egfr ) mutation test v2 ( roche molecular systems ) platform for the detection of egfr exon 19 del / l858r mutations as well as the egfr t790m resistance mutation constitutes the best example of the rapid transition of this technology from a research assay to a tool for guiding clinical care.21 furthermore , the commercial availability of multiple liquid biopsy assays for the detection of increasingly large panels of genomic alterations underscores the growing clinical role of this technology.22 , 23 the reliability , interpretation , and optimal use of liquid biopsy technology in lung cancer are potentially confusing , given the long history of the field and the number of testing platforms available . 
this hypotheses was confirmed by the detection of known mutations from a patients tumor in cfdna isolated from matched patient plasma.31 tumor - derived cfdna constitutes only a minor and potentially variable fraction of cfdna in a patient with an active malignancy , with the majority of the cfdna originating from normal tissue and blood cells.1 , 30 , 32 the careful isolation of cfdna from plasma as opposed to serum can potentially limit additional contamination with nontumor dna derived from the lysis of white blood cells during specimen processing.33 technical aspects of cfdna isolation , including prompt plasma processing and the use of dna - preservation tubes , may also reduce contamination with nontumor dna ( see specimen type and handling section ) .34 however , the relatively low frequency of tumor - derived cfdna present in the blood as well the short fragment length historically constituted key technical barriers to the reliable detection of tumor genomic alterations in cfdna . the advent of highly sensitive genotyping technologies now allows for the reliable genotyping of the tumor - derived component of plasma cfdna . 
a variety of highly sensitive validated platforms can detect specific genomic alterations in the small fraction of plasma cfdna that is derived from tumor cells ( see technology section ) .9 , 10 , 12 - 20 however , the fundamental limitation of any highly sensitive plasma genotyping assay is the degree to which a given tumor sheds cfdna into the peripheral circulation . 
the determinants of tumor cfdna shed are incompletely understood at present but are hypothesized to relate to both tumor burden and site of disease with tumor characteristics , which include histology , mitotic rate , and tumor vascularization.27 , 28 , 30 , 35 in studies of quantitative plasma genotyping of patients with metastatic nsclc , increasing disease burden , as measured by an increase in metastatic sites , as well as the presence of bone or liver metastases correlate with the concentration of tumor - derived cfdna.35 in all cases , the fraction of tumor - derived cfdna relative to total cfdna , and thus the degree of tumor cfdna shed , must be inferred from the detection of mutant cfdna relative to wild - type cfdna at a given genetic locus . 
the distinction between a shedding and nonshedding tumor is key to the understanding and interpretation of the results of any plasma genotyping assay in nsclc . technology the development of highly sensitive genotyping platforms propelled the analysis of the tumor - derived portion of cfdna from a laboratory curiosity to a potentially reliable clinical tool . 
however , both the presence and rate of cfdna shed vary among patients and directly affect the diagnostic sensitivity of plasma genotyping assays , which can contribute to false - negative results with these assays . circulating cell - free normal dna circulating tumor dna bloodstream normal tissue metastatic nsclc . 
however , the ability of individual plasma genotyping assays to detect specific types of genomic alterations is highly dependent on the testing platform , with the identification of complex rearrangements and copy number alterations being more difficult than the detection of point mutations . 
 analytical sensitivity and specificity refer to the technical ability of a genotyping assay to detect low levels of a given genomic alteration and distinguish it from other alterationsa metric that is most relevant for the development of laboratory tests and procedures . 
this review focuses primarily on clinical diagnostic sensitivity and specificity , which refer to the ability of an assay to accurately identify patients who have or do not have a given genomic alteration compared with a reference standardthe key criteria for using a test for making treatment decisions . cobas egfr mutation test and polymerase chain reactionbased approaches the cobas egfr mutation test is a real - time polymerase chain reaction ( pcr ) based assay originally developed for the purpose of detecting egfr sensitizing and t790m resistance mutations in tumor tissue . 
it is presently the only plasma genotyping assay with an fda indication for the detection of egfr mutations in metastatic nsclc for the purpose of initiating treatment with an egfr kinase inhibitor in both the initial and acquired resistance setting.21 the cobas assay was evaluated for these indications through retrospective testing of prospectively collected plasma samples from the ensure trial compared with standard tissue genotyping . 
 tissue biopsy negative t790m test metastatic site 1 metastatic site 2 blood draw positive t790m test egfrm - expressing tumor cell egfr - t790m - expressing tumor cell circulating cell - free normal dna t790m - negative ctdna t790m - positive ctdna circulating tumor dna circulating cell - free normal dna circulating tumor dna fig 2 . 
the presence of egfr t790m has been demonstrated to exhibit heterogeneity across metastatic sites , potentially resulting in false - negative results when performing tissue genotyping on a rebiopsy specimen taken from a nonrepresentative metastatic site . 
pooled data from these studies demonstrated a sensitivity of 61% ( 95% ci , 57% to 66% ) and specificity of 79% ( 95% ci , 70% to 85% ) for the detection of the egfr t790m mutation.38 a similar comparison was performed using prospectively collected samples from the aura3 study that randomly assigned patients with metastatic nsclc with egfr t790m mediated acquired resistance to egfr kinase inhibitors to either standard platinum - based chemotherapy or osimertinib.39 the study of the plasma cobas assay for egfr t790m in aura3 demonstrated a lower sensitivity of 51% ( 95% ci , 46% to 57% ) but similar specificity of 77% ( 95% ci , 71% to 83% ) .40 interestingly , both studies demonstrated near - perfect specificity for the detection of egfr exon 19 del and l858r , leading to suspicion that the lower specificity was secondary to heterogeneity of resistance mechanisms between metastatic sites within the same patient , thus rendering tumor tissue genotyping a nondefinitive reference standard . 
this hypothesis is supported by the finding that patients who are plasma - positive for egfr t790m exhibit clinical benefit similar to those who are tissue genotypingpositive and that repeat tissue biopsy of patients with acquired resistance led to discordant tissue genotyping results for egfr t790m but not egfr sensitizing mutations ( fig 2 ) .20 , 35 the cobas assay is the best - validated example of the use of pcr - based plasma genotyping assay to assess specific genetic hotspots corresponding to potentially targetable genomic alterations . 
 multiple other plasma genotyping assays have been evaluated for the detection of genomic alterations in metastatic nsclc in studies ranging in scope from analysis of prospectively collected banked plasma samples from large clinical trials to small retrospective series . 
these studies have demonstrated a consistent trend of high specificity but more modest sensitivity.9 , 41 , 42 plasma genotyping using pcr - based approaches is readily able to detect point mutations as well as defined stereotypical insertions and deletions . 
 however , the detection of complex rearrangements and copy number alterations using these platforms is challenging . droplet digital pcr and beads , emulsion , amplification , and magnetics genotyping emulsion digital pcr - based assays for plasma genotyping afford the ability to detect mutant cfdna in a highly sensitive but also quantitative manner . 
 study demonstrated that this assay was able to detect egfr exon 19 del and l858r mutations with a sensitivity of 82% and 74% , respectively , and a specificity of 100% . 
similar assay characteristics were reported for the detection of kras codon 12 mutations ( sensitivity 64% , specificity 100% ) .35 interestingly , similar sensitivity ( 77% ) but more modest specificity ( 63% ) was noted for the detection of egfr t790m . 
a subset of five patients initially reported as being falsely positive for egfr t790m by plasma genotyping were found to be truly positive on repeat tissue biopsy and genotyping of an alternative metastatic sitea finding not observed for any of the aforementioned driver mutations.35 this finding underscores the potentially heterogeneous nature of resistance mutations such as egfr t790m , whereby only growing sites of disease may possess the resistance mutation of interest . 
 tissue genotyping thus has the potential to be falsely negative when testing for an acquired resistance mutation , in contrast to plasma genotyping , which allows for the detection across metastatic sites within the same patient . beads , emulsion , amplification , and magnetics ( beaming ) based plasma genotyping assays have similarly been evaluated for the detection of egfr sensitizing and resistance mutations in patients with metastatic nsclc with acquired resistance to egfr kinase inhibitors . 
despite the rapid and quantitative nature of emulsion - based technologies , they are somewhat limited in terms of panel size and ability to multiplex . next - generation sequencing multiple next - generation sequencing ( ngs ) based platforms for plasma genotyping have been evaluated for the detection of genomic in nsclc.16 , 17 , 22 , 43 ngs - based alterations plasma genotyping assays have a greater ability to detect complex genomic alterations , such as complex rearrangements and high copy number alterations , that may be difficult to identify using other methods . 
a recent retrospective study of plasma samples collected in the biocast / ifct - 1002 study compared an ngsbased ( iontorrent , thermo fisher scientific , waltham , ma ) plasma genotyping assay to standard tissue genotyping in 68 matched samples of never - smokers with metastatic nsclc . 
this study demonstrated a sensitivity of 58% ( 95% ci , 43% to 71% ) and specificity of 87% ( 95% ci , 62% to 96% ) for the detection of mutations in key genes , including egfr , her2 , kras , braf , and pik3ca.16 a more recent retrospective study of 48 patients with metastatic nsclc comparing an ngs - based plasma genotyping assay performed on a miseq platform ( resolution bioscience ) to both ddpcr - based plasma genotyping and standard tissue genotyping revealed comparable sensitivity ( 77% , 48 of 62 positive cases detected ) and specificity ( 100% ; 95% ci , 90% to 100% ) , as well as the ability to reliably detect complex alterations , including alk and ros1 rearrangements.43 commercial plasma genotyping assays that use ngs - based platforms with expansive gene panels have been compared with tissue genotyping reference standard across multiple tumor types , and concordance rates between the two sample types are approximately 85% ( guardant360 , foundationact ) .22 , 23 other methods a multitude of other testing platforms have been used to develop plasma genotyping assays . 
 testing platforms are beyond the scope of this article and have been recently reviewed elsewhere . specimen type and handling careful and standardized methods for the isolation of cfdna from plasma are essential to optimize assay sensitivity and reproducibility . 
the collection of blood in a dna preservation tube , rapid sample processing , and the careful isolation of plasma in a fashion that minimizes cellular contamination ( centrifugation with double spin and disabled brake ) have been previously demonstrated to optimize sample quality for subsequent plasma genotyping.35 the use of plasma is preferable to serum , because the level of nontumor cfdna contamination is lower and less variable in plasma . 
the total cfdna level is frequently higher in serum samples , presumably because of white blood cell rupture during standard serum isolation , which requires allowing the blood sample to clot . 
plasma genotyping results can be available significantly faster compared with standard tissue genotyping for metastatic nsclc in both patients with newly diagnosed disease and those with disease progression while receiving initial targeted therapy.35 however , the optimal use and interpretation of plasma genotyping results hinges on specific details of the clinical scenario in which it is used . clinical actionability plasma genotyping assays consistently demonstrate high specificity and positive predictive value but modest sensitivity . 
the detection of a targetable genomic alteration in genes , including egfr , alk , ros1 , braf , met , ret , and her2 , provides useful information that may be directly used to select therapy . 
for instance , the detection of an egfr exon 19 del mutation in a patient with newly diagnosed metastatic nsclc may be used to initiate therapy with a firstor second - generation egfr kinase inhibitor ( eg , erlotinib , gefitinib , or afatinib )  . 
as a corollary , the detection of mutually exclusive , nontargetable driver genomic alterations ( eg , kras mutation ) is also useful because it provides reassurance that one of the aforementioned targetable genomic alterations is not present and that targeted therapy is not a therapeutic option.48 , 49 thus , plasma genotyping panels must be designed to detect clinically actionable genomic alterations as well as known nontargetable driver mutations . treatment status the established utility of plasma genotyping for the purpose of treatment selection in metastatic nsclc is limited to a small number of clinical scenarios . 
the best - evaluated use of plasma genotyping is for the selection of therapy in patients with newly diagnosed metastatic nsclc.15 , 37 validated plasma genotyping assays have been demonstrated to yield high sensitivity as well as near - perfect specificity for the detection of targetable genomic alterations in patients with newly diagnosed disease . 
plasma genotyping also has the capability to yield genotyping results with improved turnaround time and obviates the need for repeat biopsies in patients with newly diagnosed disease whose initial diagnostic biopsy samples are insufficient for tissue genotyping . patients with a targetable genomic alteration and acquired resistance to initial targeted therapy represent an additional clinical scenario in which plasma genotyping can guide therapy . 
the best - characterized example is the egfr t790m resistance mutation in metastatic nsclc that confers acquired resistance to firstand second - generation egfr kinase inhibitors but sensitivity to third - generation egfr kinase inhibitors . 
potentially targetable acquired resistance mutations , such as egfr t790m , emerge in a heterogeneous fashion in metastatic nsclc ; as a result , not all sites of disease may harbor a given resistance mutation , and thus the detection of such genomic alterations is inherently complex . plasma genotyping has also been evaluated with regard to monitoring the emergence of treatment resistance in patients already receiving therapy.50 , 51 the use of plasma genotyping in this context to detect early disease progression , in advance of clinical or radiographic evidence of progression , is presently investigational and should not be used to change treatment in the absence of objective evidence of disease progression . clinical stage the use of plasma genotyping has demonstrated utility for guiding therapy in metastatic nsclc but is investigational in nonmetastatic disease . 
the optimal use of this technology and interpretation of its results hinges on careful synthesis of three key concepts : cfdna biology , specific assay technology , and the individual clinical oncology of the individual patient ( fig 3 )  . patients with newly diagnosed disease plasma genotyping in a patient with newly diagnosed metastatic nsclc is most informative when a targetable genomic alteration ( eg , egfr , alk , ros1 , braf , met ) or a nontargetable mutually exclusive driver alteration ( eg , kras ) is found . 
the use of an fda - approved and rigorously validated plasma genotyping assay allows for immediate initiation of appropriate targeted or systemic therapy in the instance of a positive result , given the high specificity and positive predictive value of these assays . 
negative plasma genotyping results where no driver alteration is detected are not useful in guiding therapy , given the modest sensitivity of such assays , and should prompt appropriate tissue genotyping if not already initiated . 
importantly , caution must be exercised in interpreting low - level positive results near the limit of detection , particularly of nondriver alterations detected on poorly validated panels , as there exists the risk of assay artifact and a false - positive result . acquired resistance plasma genotyping should be used as the initial genotyping method in the setting of acquired resistance to targeted therapy in metastatic nsclc . 
this approach has the ability to obviate the need for repeat biopsy in many instances but also detects resistance mechanisms that may be missed on repeat tissue genotyping because of heterogeneity of resistance mechanisms . 
the absence of an identifiable resistance mutation should prompt repeat tissue biopsy and genotyping to rule out a false - negative result , as well as examine for alternative resistance mechanisms that are not easily identified through plasma genotyping , such as small - cell transformation or met amplification . 
as a corollary , a plasma genotyping result that fails to detect the original targetable alteration in a patient with acquired resistance should be considered indicative of the absence of tumor cfdna shed , and the result invariably a false negative . 
importantly , plasma testing for acquired resistance as well as repeat biopsy should only be initiated in patients with clinically or radiographically significant disease progression , to avoid inadvertently labeling a patients disease t790m negative because of testing before the emergence of clinical resistance . 
a recent retrospective study demonstrated improved sensitivity with the use of combined urine and plasma genotyping in a cohort of patients with metastatic resistant egfr - mutant nsclc.52 this finding supports the hypothesis that the use of multiple orthogonal testing strategies may be effective in enhancing overall diagnostic sensitivity . 
furthermore , the combination of plasma and tissue genotyping alone has the potential to surmount the modest sensitivity in the context of acquired resistance . the potential utility of serial quantitative plasma genotyping for the purpose of monitoring response to therapy , as well as the evolution of acquired resistance , constitutes another promising area of research . 
 therapeutic response in clinical trials of novel agents may allow for real - time monitoring of response to therapy as well as early prediction of potential mechanisms of acquired resistance . 
sacher , division of medical oncology and hematology , princess margaret cancer centre , university of toronto , toronto , ontario . references med 14 : 985 - 990 , 2008 1 . 
botezatu i , serdyuk o , potapova g , et al : genetic analysis of dna excreted in urine : a new approach for detecting specific genomic dna sequences from cells dying in an organisclin chem 46 : 1078 - 1084 , 2000 8 . 
chen ww , balaj l , liau lm , et al : beaming and droplet digital pcr analysis of mutant idh1 mrna in glioma patient serum and cerebrospinal fluid extracellular vesicles . 
karachaliou n , mayo - de las casas c , queralt c , et al : association of egfr l858r mutation in circulating free dna with survival in the eurtac trial . 
kimura h , suminoe m , kasahara k , et al : evaluation of epidermal growth factor receptor mutation status in serum dna as a predictor of response to gefitinib ( iressa )  . 
tan ds , yom ss , tsao ms , et al : the international association for the study of lung cancer consensus statement on optimizing management of egfr mutation - positive non - small cell lung cancer : status in 2016 . 
li bt , janku f , janne pa , et al : ultra - deep next generation sequencing ( ngs ) of plasma cell - free dna ( cfdna ) from patients with advanced lung cancers : results from the actionable genome consortiucancer res 76 , 2016 ( abstr 4342 ) 14 . 
karlovich c , goldman jw , sun jm , et al : assessment of egfr mutation status in matched plasma and tumor tissue of nsclc patients from a phase i study of rociletinib ( co - 1686 )  . 
mok t , wu yl , lee js , et al : detection and dynamic changes of egfr mutations from circulating tumor dna as a predictor of survival outcomes in nsclc patients treated with first - line intercalated erlotinib and chemotherapy . 
couraud s , vaca - paniagua f , villar s , et al : noninvasive diagnosis of actionable mutations by deep sequencing of circulating free dna in lung cancer from never - smokers : a proof - of - concept study from biocast / ifct - 1002 . 
goto k , ichinose y , ohe y , et al : epidermal growth factor receptor mutation status in circulating free dna in serum : from ipass , a phase iii study of gefitinib or carboplatin / paclitaxel in nonsmall cell lung cancer . 
douillard jy , ostoros g , cobo m , et al : gefitinib treatment in egfr mutated caucasian nsclc : circulating - free tumor dna as a surrogate for determination of egfr status . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - small - cell lung cancer . 
kim st , lee ws , lanman rb , et al : prospective blinded study of somatic mutation detection in cell - free dna utilizing a targeted 54 - gene next generation sequencing panel in metastatic solid tumor patients . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
jahr s , hentze h , englisch s , et al : dna fragments in the blood plasma of cancer patients : quantitations and evidence for their origin from apoptotic and necrotic cells . 
sacher a , dahlberg s , paweletz c , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
reck m , hagiwara k , han b , et al : ctdna determination of egfr mutation status in european and japanese patients with advanced nsclc : the assess study . 
jenkins s , yang jc , ramalingam ss , et al : plasma ctdna analysis for detection of the egfrt790m mutation in patients with advanced non - smallcell lung cancer . 
weber b , meldgaard p , hager h , et al : detection of egfr mutations in plasma and biopsies from non - small cell lung cancer patients by allele - specific pcr assays . 
yung tk , chan kc , mok ts , et al : single - molecule detection of epidermal growth factor receptor mutations in plasma by microfluidics digital pcr in non - small cell lung cancer patients . 
paweletz cp , sacher ag , raymond ck , et al : bias - corrected targeted next - generation sequencing for rapid , multiplexed detection of actionable alterations in cell - free dna from advanced lung cancer patients . 
hu c , liu x , chen y , et al : direct serum and tissue assay for egfr mutation in non - small cell lung cancer by high - resolution melting analysis . 
brevet m , johnson ml , azzoli cg , et al : detection of egfr mutations in plasma dna from lung cancer patients by mass spectrometry genotyping is predictive of tumor egfr status and response to egfr inhibitors . 
zhao j , ye x , xu y , et al : egfr mutation status of paired cerebrospinal fluid and plasma samples in egfrmutant non - small cell lung cancer with leptomeningeal metastases . 
sholl lm , aisner dl , varella - garcia m , et al : multi - institutional oncogenic driver mutation analysis in lung adenocarcinoma : the lung cancer mutation consortium experience . 
gainor jf , varghese am , ou sh , et al : alk rearrangements are mutually exclusive with mutations in egfr or kras : an analysis of 1 , 683 patients with non - small cell lung cancer . 
thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . 
sacher a , alden r , oconnell a , et al : a prospective study of rapid plasma genotyping utilizing sequential ddpcr and ngs in newly diagnosed advanced nsclc patients . 
 majority of b2m - mutant and - decient colorectal carcinomas achieve clinical benet from immune checkpoint inhibitor therapy and are microsatellite instability - high sumit middha , phd1 ; rona yaeger , md1 ; jinru shia , md1 ; zsoa k . 
hechtman , md1 purpose microsatellite instability - high ( msi - h ) colorectal carcinomas ( crcs ) show high rates of response to immune checkpoint inhibitors ( ios )  . 
all b2m - mutant crcs were assessed for expression of b2m , major histocompatibility complex class i , and programmed death - 1 ligand ( pd - l1 ) via immunohistochemistry and average cd3 + and cd8 + tumor - inltrating lymphocyte counts against a control group of msi - h b2m wild - type crcs . results fifty - nine ( 3.4% ) of 1 , 751 patients with crc harbored b2m mutations , with 84% ( 77 of 92 ) of the mutations predicted to be truncating . 
b2m mutation status was not associated with major histocompatibility complex class i expression , kras or braf mutation , tumor - inltrating lymphocyte level , or pd - l1 expression after adjustment for msi status . 
of 13 patients with b2m - mutant crc who received programmed death - 1 or pd - l1 ios , 11 ( 85% ) achieved clinical benet , dened as stable disease or partial response using response evaluation criteria in solid tumors criteria . conclusion b2m mutations occur in approximately 24% of msi - h crcs and are usually associated with loss of b2m expression . 
 middha et al context do b2m - mutant and decient colorectal carcinomas ( crcs ) respond to immune checkpoint inhibitors ? we found that b2m mutations are enriched in microsatellite instability - high crc , that these mutations commonly occur at coding microsatellite loci , and that these b2m mutations are truncating and associated with loss of b2m expression . 
of 13 patients with b2m - mutant crc and available recist data , six achieved stable disease , ve achieved partial response , and one experienced pseudoprogression . b2m mutations are not predictive of primary resistance to immune checkpoint inhibition in crc . administrationcleared , next - generation sequencing assay that interrogates  . 
presence of loss of heterozygosity ( loh ) was assessed via allelespecic copy - number analysis using the fraction and allelespecic copy number estimates from tumor sequencing ( facets ) algorithm14 and , in cases of low tumor content , via comparison of b2m mutation variant allele frequency against median variant allele frequency . 
clinical parameters , clinical response to immune checkpoint inhibitor therapy all patients with crc with msk - impact data and b2m mutations who underwent therapy with immune checkinhibitors ( ios ; durvalumab , nivolumab , or pempoint brolizumab ) before july 2018 were assessed for b2m expression ( ihc ) , response , stable disease ( sd ) , and progressive disease ( pd )  . 
formal response evaluation criteria in solid tumors ( recist ) scores were assessed via radiologic data as follows : complete response ( cr ) , disappearance of all target lesions , conrmed at 4 weeks ; partial response ( pr ) , 30% decrease , conrmed at 4 weeks ; pd , 20% increase over smallest sum observed ; and sd , meeting none of the other criteria . patients were deemed to have experienced clinical benet from ios if recist results were sd , pr , or cr . ihc staining for b2m using a polyclonal antibody with concentration of 1 : 6 , 000 ( catalog #a0072 ; dako , santa clara , ca ) , mhc class i using a monoclonal antibody with concentration of 1 : 200 ( catalog #14 - 9958 ; e - bioscience , carlsbad , ca ) , cd3 using a monoclonal antibody with concentration of 1 : 200 ( catalog #ncl - l - cd3 - 565 ; leica , lincolnshire , il ) , cd8 using a monoclonal antibody with concentration of 1 : 100 ( catalog #m7103 ; dako ) , and pd - l1 using a monoclonal antibody with concentration of 1 : 100 ( catalog #13684 ; cell signaling , danvers , ma ) was performed on all crcs with b2m mutations with available tissue as well as a set of 26 randomly selected wild - type ( wt ) crcs with in - house resection specimens and mskimpact testing ( performed between january 1 , 2014 , and october 31 , 2017 ) that were matched to the b2m - mutant group for prevalence of msi status . 
complete loss of b2m on ihc ( 0% of tumor cells with b2m expression ) was interpreted as loss of b2m expression . statistical analyses associations were assessed using pearsons 2 test with simulated p value based on 2 , 000 replicates for low count data . 
a cox proportional hazards model was tted to the data to calculate survival using the covariates of b2m mutation status , age at diagnosis , pathologic stage , msi status , proximal versus distal status , and kras , nras , braf , and pik3ca mutation status . 
these were each assessed through both univariable and multivariable cox regressions . r survival and survminer software packages were used to perform this analysis ( r foundation , vienna , austria )  . results molecular findings we rst sought to determine the spectrum of b2m mutations in a cohort of patients with crc ( n = 1 , 751 ) with msk - impact data ( appendix fig a1 )  . 
next , we classied the samples on the basis of whether they were microsatellite stable ( mss ) or unstable ( msi - h ) on the basis of genomic data . 
a medullary carcinoma of the colon shows immune - cell expression of programmed death - 1 ligand at the tumor - stroma interface , loss of b2m expression in tumor cells , retention of strong diffuse mhc class i expression in tumor cells ,  . 
twelve samples showed either loh or copy - neutral loh along with a clonal mutation , suggesting biallelic loss . b2m expression , mhc class i expression , and til level to evaluate the functional outcome of b2m mutations , we examined protein expression in samples with available tissue ( figs 1b and 1c ; appendix table a2 )  . 
because pdl1 status has been used as a predictive marker of ios and linked to expression of mhc class 1 , we performed pd - l1 ihc in available b2m - mutant and wt patient cases . 
thirtytwo ( 73% ) of 44 b2m - mutant and 13 ( 50% ) of 26 b2m wt crcs were positive for pd - l1 expression ( immune cells in tumor - stroma interface )  . 
average median cd3 + count per hpf was 22.3 in b2m - mutant and 37.3 in b2m wt crcs , whereas average median cd8 + count per hpf was 15.1 and 49 for b2m - mutant and b2m wt crcs , respectively . 
in comparison with b2m wt crcs matched for msi status , b2m - mutant crcs tended to have lower average levels of cd3 and cd8 per patient case ( fig 2a ) , these differences did not reach statistical significance . 
age , stage , and kras , nras , and braf status were associated with os , whereas pik3ca mutation status , msi status , and proximal versus distal location were not associated with os ( fig 2b ; appendix table a2 )  . response to immunotherapy because b2m mutations were identied as a possible resistance mechanism for checkpoint inhibition , we identied 13 ( msi - h , n = 11 ; mss , n = 2 ) patients with crc with b2m mutations who subsequently received io therapy , and we evaluated their response to treatment . 
 ( a ) box plot graphs of average cd3 ( left ) and cd8 ( right ) counts in b2m - mutant vs wild - type ( wt ) colorectal carcinoma ( crc ) show that median average cd3 and cd8 trend toward higher values in b2m wt carcinoma . ( b ) multivariable model showing the clinical variables associated with os of patients with crc in our cohort . 
analysis of their tumor response by recist criteria demonstrated pr in ve patients , sd in six patients , and pd in one patient , likely pseudoprogression ( fig 3a ; appendix table a3 )  . 
this response rate is in line with recent publications of ios in msi - h crc.8 , 9 of the two patients with mss tumors , one had an ultramutated pole hotspot mutated tumor and experienced tumor growth with io treatment but was able to continue treatment for 1 year , likely to be pseudoprogbecause growth was thought ression , and the other patient had sd during treatment with a combination of io treatment and targeted therapy ( after progression with targeted therapy alone )  . 
the association of b2m mutations with complete loss of expression on whole sections of pole s459f best response pseudoprogression partial response stable disease treatment stopped ongoing 40% 80% msi status io therapy b2m expression fig 3 . 
immune checkinhibitor ( io ) repoint sponse in b2m - mutant colorectal cancer ( crc )  . waterfall plot of io response in b2m - mutant crc ( colored by microsatellite instability [ msi ] status , type of b2m mutation , and type of io received )  . 
indeed , in the 42 b2m - mutant crcs analyzed by facets , 60% had evidence of either two clonal b2m mutations or one clonal b2m mutation and loh ( appendix table a1 )  . 
it is possible that the remaining b2m - mutant crcs have epigenetic modications as a mechanism of b2m silencing . unlike previous studies , 3 we found that b2m protein loss is not correlated with loss of mhc class i expression . 
we show that b2m mutation and loss do not correlate with mhc class i loss of expression , although the effect of b2m loss on the functional competence of mhc class i is known to be deleterious.16 limitations to our study include the retrospective analysis and relatively small number of patients treated with ios , as well as limitations in molecular testing for epigenetic issues and allele specicity of b2m mutations . most importantly , our study shows that b2m mutation and loss in immunotherapy - naive crc do not predict primary resistance to ios . 
we saw that most patients had some degree of regression with treatment ; larger , prospective studies are needed to clarify if the response rate and duration of response vary by b2m mutation status . however , our data indicate that patients with crc whose tumors harbor b2m mutations should not be excluded from io treatment . 
the clinical benet demonstrated in patients with b2m - decient crc who received ios may have resulted from the fact that despite b2m loss , there was still evidence of functional neoantigen recognition , as indicated by the high number of tils ( median , 22.3 per hpf ) still present in b2m - decient msi - h crc . 
 middha et al leonard saltz consulting or advisory role : mcneil ( i ) research funding : taiho pharmaceutical neil segal consulting or advisory role : bristol - myers squibb , pzer , astrazeneca / medimmune , imugene , roche / genentech , pieris pharmaceuticals , synlogic , aduro biotech , kyn therapeutics , boehringer ingelheim , merck , puretech , horizon pharma , emd serono , gritstone oncology , chugai pharma , trm oncology , ifm therapeutics , psioxus therapeutics research funding : medimmune , bristol - myers squibb , pzer , roche / genentech , merck , incyte marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso rfp advisory committee , takeda pharmaceuticals , bristol - myers squibb , bayer healthcare pharmaceuticals , merck ( i ) research funding : loxo ( inst ) , helsinn therapeutics ahmet zehir no relationship to disclose jaclyn f . 
hechtman honoraria : medscape consulting or advisory role : navigant consulting , axiom biotechnologies research funding : bayer no other potential conicts of interest were reported . references roberts ad , ordway dj , orme im : listeria monocytogenes infection in beta 2 microglobulin - decient mice . 
infect immun 61 : 1113 - 1116 , 1993 schaible ue , collins hl , priem f , et al : correction of the iron overload defect in beta - 2 - microglobulin knockout mice by lactoferrin abolishes their increased susceptibility to tuberculosis . 
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nat commun 8 : 1136 , 2017 janikovits j , m uller m , krzykalla j , et al : high numbers of pdcd1 ( pd - 1 ) - positive t cells and b2m mutations in microsatellite - unstable colorectal cancer . oncoimmunology 7 : e1390640 , 2017 grasso cs , giannakis m , wells dk , et al : genetic mechanisms of immune evasion in colorectal cancer . 
cancer discov 8 : 730 - 749 , 2018 le dt , uram jn , wang h , et al : pd - 1 blockade in tumors with mismatch - repair deciency . 
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cell 171 : 934 - 949.e16 , 2017 le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - decient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
clendenning m , huang a , jayasekara h , et al : somatic mutations of the coding microsatellites within the beta - 2 - microglobulin gene in mismatch repairdecient colorectal cancers and adenomas . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
consort diagramutation and immunohistochemistry analyses included data from 1 , 751 patients with colorectal cancer ( crc ) with memorial sloan kettering integrated mutation proling of actionable cancer targets testing . 
 o precision trial drawer , a computational tool to assist planning of genomics - driven trials in oncology purpose trials that accrue participants on the basis of genetic biomarkers are a powerful means of testing targeted drugs , but they are often complicated by the rarity of the biomarker - positive population . 
however , bigger trials have higher chances of conflicting treatment allocations because of the coexistence of multiple actionable alterations ; allocation strategies greatly affect the efficiency of enrollment and should be carefully planned on the basis of relative mutation frequencies , leveraging information from large sequencing projects . methods we developed software named precision trial drawer ( ptd ) to estimate parameters that are useful for designing precision trials , most importantly , the number of patients needed to molecularly screen ( nnms ) and the allocation rule that maximizes patient accrual on the basis of mutation frequency , systematically assigning patients with conflicting allocations to the drug associated with the rarer mutation . 
we used data from the cancer genome atlas to show their potential in a 10 - arm imaginary trial of multiple cancers on the basis of genetic alterations suggested by the past molecular analysis for personalised therapy ( map ) conference . 
2018 by american society of clinical oncology introduction the availability of sequenced cancer genomes and the generation of new targeted drugs offer unprecedented opportunities for personalized treatment for patients with cancer . 
indeed , treatment within genomic - based clinical trials significantly improves clinical outcome.1 however , identification of the best biomarker - drug combination for patient stratification and treatment remains a critical research and ethical challenge . large multi - institutional projects such as the cancer genome atlas ( tcga ) revealed extreme heterogeneity of cancer mutational landscapes , with a prevalence of low - frequency mutations , giorgio e.m. 
are co - first authors . corresponding author : luca mazzarella , md , phd , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy ; e - mail : luca . 
 including those critical for tumor growth ( driver mutations ) and those that might be targetable by specific drugs ( actionable mutations ) .2 , 3 this scenario renders the conduction of adequately powered genome - based clinical trials prohibitive in many cases : the biomarker - positive population is often rare , and identifying it requires screening large numbers of patients . strategies to circumvent this issue are proposed through novel trial designs in which multiple drugs and / or their matched biomarkers are tested simultaneously . 
these novel designs , usually defined as basket ( one biomarker - drug pair , multiple histologies ) , umbrella ( multiple biomarker - drug pairs , one histology ) , or platform ( multiple biomarker - drug pairs , multiple histologies ) , 4 - 6 may allow reducing the number of patients needed to molecularly screen ( nnms ) to achieve the desired statistical power for multiple treatment subgroups . 
however , these approaches have potential disadvantages : first is the occurrence of a large fraction of patients with potential allocation conflicts resulting from the concomitance of genetic alterations associated with different drugs , 2 and second is the high costs and turnaround time of the molecular screening , which must include sequencing enough genomic space to accommodate the studys need . 
the latter will become more critical in the near future as more complex , polygenic genomic signatures are used as stratification biomarkers ( eg , multiple homologous recombination genes to establish brcaness as a predictor of response to poly [ adp - ribose ] polymerase [ parp ] inhibitors7 )  . 
 for these reasons , patient allocation to individual trial arms significantly deviates from expectations in multigenic umbrella trials , which leads to inadequate statistical power8 , 9 and the inability to reach conclusions . here , we present precision trial drawer ( ptd ) , a comprehensive bioinformatics tool that takes advantage of patient - level genomic information from tcga or alternative sources to simulate genomically characterized cohorts and provide critical parameters for designing genetic biomarker - driven trials . 
df is used to calculate the nnms ( ie , the minimum number of patients that should be tested to obtain the desired sample size as calculated on the expected treatment effect by using conventional power analyses )  . 
 actionable mutations refers to those genetic alterations that dictate a therapeutic choice within the trial . description of the package ptd includes a series of functions in the r programming language to ( 1 ) translate genomic information into genomic coordinates and optimize coordinates for the design of a targeted sequencing panel , ( 2 ) retrieve single or grouped genetic alteration frequencies from public databases ( by default tcga , but other sources can be used ) that maintain patient - level associations , ( 3 ) simulate genomically defined patient cohorts by extracting frequencies of co - occurrence of single or grouped mutations , and ( 4 ) calculate nnms for defined power and / or sample size ( fig 1a )  . 
in our imaginary trial , patients are allocated to 10 possible drugs , including inhibitors of parp , notch , met , her2 , fgfr , egfr , braf , alk , akt , and immune checkpoints , and covering all the allocations linked to the map biomarkers . 
allocation to checkpoint inhibitors was based on the detection of inactivating mutations in mlh or msh genes , regardless of tumor type , which are highly correlated with microsatellite instability , a now - established predictor of immune checkpoint response.11 , 12 ptd was then used to design a dedicated custom targeted sequencing panel , identify the optimal allocation rule , and estimate sample size and statistical power . the list of genomic features associated with each drug is provided in table 1 . 
illustrations of the workflow , the codes used for generating data , and detailed ptd functionalities are available at shinyapp.html. the first step involves designing the sequencing panel , which is imported as a standard excel table with official gene symbols , type and exact alteration to be considered , and two possible grouping variables ( gene - linked drug and , if desired , a generic group of any sort )  . 
 the panel can also be expanded to include genes or genomic positions without therapeutic information , which may nevertheless be relevant for prognostic stratification , prediction of drug toxicity , or a generic biologic interest ( grouped as driver genes in the example )  . four classes of genetic alterations can be explored : single nucleotide variants ( snvs ) , copy number alterations ( cnas ) , translocation - associated fusion transcripts , and gene expression . 
for panels that contain multiple alteration types ( eg , snvs and cnas ) , ptd will construct a reference data set with the intersection of the relative data sets in the source database ( not all patients in tcga have data from all sequencing platforms )  . in projects that allow inclusion of multiple tumor histologies , their frequency of occurrence in the real world is likely to differ significantly from the relative representation in the reference data set , and this can be corrected by ptd by weighting the probability of sample extraction . 
in this example , we used relative frequencies obtained from the national cancer institute seer program ( fig 2a shows the comparison between the tcga and the example populations )  . output the percentage of patients with at least one actionable alteration ( detected fraction ; df ) is probably the most crucial estimate that can be obtained through ptd , which is 65.4% in this example ( fig 2b )  . 
ptd allows breakdown of the df by drug or by disease histology ( fig 2c - d ) or any other prespecified group . to optimize panel design , one can evaluate the trade - off between the feature of interest ( eg , available drugs or the inclusion of genes with uncertain predictive power ) and the size of the genomic space to be sequenced . 
this trade - off can be visualized with a saturationplot that expresses the mean number of alterations per patient or the number of patients with at least x alterations as a cumulative function of the genomic space , with alterations ranked in descending frequency order ( absolute or gene lengthnormalized ; fig 2e )  . 
 the same plot can be obtained by using drugs or other grouping variables ( fig 2f )  . the coocmutexplot indicates the degree of co - occurrence of grouped genetic alterations , ascopubs.org / journal / po jco precision oncology 5 accepted formats . 
for instance , the braf v600e mutation can be coded using amino acid notation ( v600e ) , the single nucleotide polymorphism database ( dbsnp ) identifier ( rs113488022 ) , a set of genomic coordinates ( eg , chr7 : 140753336 140753337 ) , or as genomic variants ( 7 : 140753336 a > c )  . 
mutations of interest can be batch filtered with any set of genomic coordinates to eliminate variants likely to be passengers.3 , 13 in this example , we selected only variants listed as probably pathogenic in the catalogue of somatic mutations in cancer ( cosmic ) database , 14 thus eliminating 33.5% of the initial variants . 
alternatively , individual genes can be visually inspected and edited by using an interactive interface built on the lowmaca ( low frequency mutations analysis via consensus alignment ) algorithm15 ( manual filtering ; fig 1b )  . 
in this example , we manually excluded egfr t790m and pik3ca exon 20 mutations associated with resistance to first - generation egfr inhibitors.16 , 17 specific mutations and / or drugs can be associated with specific tumors and excluded from others . 
 ( b ) percentage of patients with at least one ( detection fraction ) or more actionable alterations ; detection fraction is broken down by ( c ) tumor type or ( d ) drug . 
this plot can be used to decide which drugs should be combined in the same trial because prioritizing those associated with highly mutually exclusive mutations will maximize the biomarker - positive population . power analysis and calculation of the nnms multidrug trials can be powered to test the experimental arm as a whole , ignoring the number of patients allocated to each individual drug , in which case the nnms is a simple linear function of the target sample size divided by the detection power ( in our example , if the given target sample size = n , the nnms will be n / 0.654 ; no allocation rule design )  . 
if this is a desired end point , the trial can be divided into a series of drug - specific subtrials , each having its own target sample size.9 probability of allocation can vary significantly if the associated biomarkers have very different prevalence . 
furthermore , increasing the number of competing arms also increases the likelihood of conflicting allocations ; rules to follow in such cases should be specified in advance to avoid allocation biases . 
immcheckp , immune checkpoint ; inh , inhibitor . general a priori considerations that do not take into account mutation frequencies ( eg , allocation to endocrine therapy only if no mutation is present8 ; manual allocation design )  . 
if information regarding the co - occurrence of mutations is not considered , proper nnms - based sample size calculation is not possible because considering each subtrial independently leads to gross overestimation . 
with ptd , arms can be ranked in order of expected frequency of allocation , so that if a patient bears mutations associated with two drugs , he or she will be systematically assigned to the one with the lowest frequency . 
in nonoptimal designs , allocation does not take into consideration the relative rarity of c , so that when all patients have been allocated , drug z has been allocated to fewer patients than statistically needed . 
 ( c ) comparison of percentages of patients that can be allocated to one or two of the molecular pathway - based subgroups ( real values for shiva and mean values for precision trial drawer [ ptd ] 95% ci are plotted )  . 
 ( d ) power calculations showing numbers needed to sequence for the overall ( bottom panel ) and pathway - specific subgroup trials ( top and middle panels )  . 
cna , copy number alteration ; snv , single nucleotide variant ; tcga , the cancer genome atlas . nnms based on the rule , and simulate patient allocation so that each drug - specific arm reaches at least the desired level of power ( optimal allocation design ; fig 3a )  . 
we can thus precisely quantify the advantage of an optimized umbrella design : for the given example , if one were to run 10 independent one - arm studies with a target sample size of 13 to show a response rate of 40% against historical controls of 10% ( for = .05 and power = 0.8 ) , a total of 4 , 276 patients would need to be sequenced to obtain 130 ( ie , 10 13 ) biomarker - positive patients . 
 the researcher to specify different types of end points ( time to event , progression - free survival , overall survival , time to progression , or proportions such as response rate and survival rate ) , number of arms , allocation ratios ( symmetric or asymmetric ) , and other conventional trial parameters . 
simulation results for oneor twoarm studies with time - to - event or proportion end points and with no , manual , or optimal allocation rules are provided in fig 3b . 
simulation results across a range of powers and target proportions are provided in fig 3c . retrospective evaluation of the shiva trial to test ptd in a real - world scenario , we retrospectively evaluated its ability to correctly predict population composition and treatment allocation in the recent shiva trial , a phase ii randomized trial comparing conventional therapy to multiple targeted agents on the basis of tumor molecular profiling . 
in shiva , 741 patients were subjected to a triad of molecular tests , including sequencing with a targeted enrichment panel ( ampliseq cancer panel , covering 45 tumor - associated genes or mutational hotspots ) , gene copy number analysis by cytoscan hd , and immunohistochemistry for three endocrine receptors . 
although ptd can include information on gene expression in the simulation , we removed endocrine receptors from the analyzed parameters because the correlation between rna - based and immunohistochemistry based quantification of endocrine receptors is poor ( appendix fig a1 )  . 
after data cleanup , 417 of 741 patients were left for analysis ( fig 4a )  . we constructed a ptd panel by using the actionable alterations in shiva and ran 100 trial simulations , extracting tumor histologies from tcga with probabilities equal to their frequencies in shiva and with allocation rules reproducing those adopted in the actual trial . 
alteration frequencies for individual genes were within 95% cis in most cases ( appendix fig a1a - b ) , except for low - frequency genes , for which 95% cis can be expected to be wide . 
consequently , observed versus predicted nnms was also quite similar ( fig 4d ; appendix fig a1d ) , demonstrating that ptd can correctly predict the number of patients needed to be subjected to molecular screening . discussion we report a versatile bioinformatics platform that is based on mutational databases to simulate genetic biomarker - driven clinical trials . 
in a retrospective analysis of the shiva trial , we demonstrated that our tool is able to predict the actual number of patients to be sequenced and has the power to detect overall and arm - specific efficacy signals . 
we believe that our tool will be instrumental in overcoming emerging issues in the design of precision oncology trials . the conceptual framework of precision medicine implies an increased fragmentation of disease entities into distinct subgroups identified by the presence of biomarkers that predict response to targeted agents . 
as previously highlighted by several authors , 6 , 20 for trials aimed at demonstrating efficacy of targeted drugs , 20 more biomarkers means rarer biomarkers , which in turn implies higher and more variable numbers of patients needed to be screened . 
 match screening trial ( targeted therapy directed by genetic testing in treating patients with advanced refractory solid tumors , lymphomas , or multiple myeloma ) , the largest trial of this type to date , an interim analysis after 795 patients were screened showed that only 2.5% of patients could be allocated to seven of the 10 targeted agents on trial.21 the possibility of better predicting accrual rate afforded by ptd would allow trialists to drop inefficient arms and / or modify trial design to maximize patient allocation . an unavoidable limitation of our methodology is that simulations are affected by the prevalence of mutations in available databases , which may not be representative of what is found in study populations . 
instead , most trials with targeted drugs are initially aimed at the metastatic setting , and the mutational profile of metastatic tumors can be significantly different from that of primary tumors . 
an ideal setting for ptd - based simulations with current tcga data may be the neoadjuvant / preoperative setting , which is increasingly used to evaluate novel drugs.23 the availability of clinical metadata , such as tumor size or nodal involvement , can be used to strengthen the representativeness of database samples . finally , some disease tumor types are under represented in mutational databases , which results in high variability and low confidence of corresponding simulations . 
melloni , alessandro guida , giuseppe curigliano , edoardo botteri , ruggero de maria , piergiuseppe pelicci , luca mazzarella financial support : giuseppe curigliano , piergiuseppe pelicci administrative support : giuseppe curigliano provision of study materials or patients : giuseppe curigliano , angela esposito , maud kamal , christoph le tourneau collection and assembly of data : giorgio e.m. 
 edoardo botteri no relationship to disclose angela esposito no relationship to disclose maud kamal no relationship to disclose laura riva employment : philips healthcare ( i ) alberto magi no relationship to disclose ruggero de maria no relationship to disclose christophe le tourneau honoraria : novartis , bristol - myers squibb piergiuseppe pelicci stock and other ownership : genextra consulting or advisory role : amgen , msd , bristolmyers squibb , merck serono , astrazeneca travel , accommodations , expenses : msd , bristol - myers squibb , astrazeneca luca mazzarella no relationship to disclose affiliations giorgio e.m. 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
le tourneau c , delord jp , gonalves a et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
lopez - chavez a , thomas a , rajan a , et al : molecular profiling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
pao w , miller va , politi ka , et al : acquired resistance of lung adenocarcinomas to gefitinib or erlotinib is associated with a second mutation in the egfr kinase domaplos med 2 : e73 , 2005 17 . 
mao c , yang zy , hu xf , et al : pik3ca exon 20 mutations as a potential biomarker for resistance to anti - egfr monoclonal antibodies in kras wild - type metastatic colorectal cancer : a systematic review and meta - analysis . 
 o accurate rna sequencing from formalin - fixed cancer tissue to represent high - quality transcriptome from frozen tissue purpose accurate transcriptional sequencing ( rna - seq ) from formalin - fixed paraffin embedded ( ffpe ) tumor samples presents an important challenge for translational research and diagnostic development . 
we evaluated the accuracy of rna - seq data generated from ffpe samples in terms of expression profiling . methods we designed a biospecimen study to directly compare gene expression results from different protocols to prepare libraries for rna - seq from human breast cancer tissues , with randomization to fresh frozen ( ff ) or ffpe conditions . 
the protocols were compared using multiple computational methods to assess alignment of reads to a reference genome , the uniformity and continuity of coverage , the variance and correlation of overall gene expression , patterns of measuring coding sequence , phenotypic patterns of gene expression , and measurements from representative multigene signatures . results the principal determinant of variance in gene expression was use of exon capture probes , followed by the conditions of preservation ( ff v ffpe ) and phenotypic differences between breast cancers . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction although it is generally best to identify gene expression biomarkers from cancer tissues using the highest quality of rna purified from fresh frozen ( ff ) samples , any subsequent development toward diagnostic testing will require translation for use with formalin - fixed paraffin - embedded ( ffpe ) tissue samples . 
however , the variably fragmented and chemically modified rna derived from ffpe samples presents a challenge for accurate measurement of gene expression.1 , 2 in a different context , there is great interest to perform transcriptome sequencing ( rna - seq ) for biomarker discovery research using large cohorts of precious archival ffpe samples from completed clinical trials . 
different approaches to generating libraries for rna - seq include selection of mrna by targeting the poly ( a ) tail ( mrna protocol ) , depletion of more abundant ribosomal rna ( rrna depletion ) using jialu li chunxiao fu terence p . 
 a 80c freezer ( ff ) or 10% neutral buffered formalin and paraffin - embedded as an ffpe tissue block.10 phenotypically , the nine breast cancers were defined by the pathologic status of hormone receptors ( hrs ) and human epidermal growth factor receptor 2 ( her2 ) as hr - positive / her2 - negative in five , hr - positive / her2 positive in one , and triple receptor - negative in three . 
a dnase - i treatment step was included in both . construction of rna - seq library and sequencing full details of all methods for library construction and sequencing of rna samples are in the data supplement . 
an overview diagram of the different rna - seq library protocols is shown in figure 1 , and details of the number of libraries prepared , starting rna requirement , cost , and duration to perform each protocol are summarized in the data supplement . the mrna protocol ( ff only ) used oligo - dt beads for poly ( a ) + mrna enrichment , followed by standard procedures of truseq rna sample prep kit v2 ( illumina , san diego , ca )  . 
then the rrna - depleted srna was used as the template for the mrna protocol described above . the cr protocol was performed using truseq access rnaseq kit ( illumina ) , using random primers . 
no technical replicates could share the same sequencing lane . rna - seq data analysis full details of all data analysis methods and an overview diagram of the analysis plan are provided in the data supplement . 
scatter plot of the first three principal components for count per millionnormalized and variance stabilizing transformed counts of 20 , 381 coding region ( cr ) - targeted poly ( a ) + genes . 
the rnaseq data generated from the srna protocol had a significantly lower concordant pair alignment rate as compared with those from non - srna protocols ( p < .001 ; data supplement )  . 
using the cr protocol , mapping was highly concordant between ff and ffpe and the exonic mapping rate was increased compared with non - cr methods ( data supplement )  . 
overall , the number of genes with read coverage ( transcripts per million [ tpm ] > 0.1 ) was slightly higher in ffpe samples than in ff samples for both non - cr and cr protocols ( data supplement ) .12 uniformity and continuity of read coverage of transcripts uniformity of read coverage was measured by the mean coefficient of variation , and continuity of coverage as the percentage of gaps without read coverage , across the top 1 , 000 highly expressed transcripts ( data supplement )  . 
 principal component analysis of expression of a total of 20 , 381 cr protocol targeted poly ( a ) + genes for all libraries showed that the 26.5% of total variation captured by the first principal component was due to use of exon capture probes ( cr protocol ) , and 20.6% from the second and third components due to the combined effects of ffpe and biologic differences ( fig 2 )  . 
hierarchical clustering results , with high confidence ( average bootstrap probability , 0.93 ) , showed that the major tumor phenotypes ( hr - positive v hr - negative ) and the source tumor clustered together with ffpe samples ( data supplement )  . 
comparing ff and ffpe samples using the same totalrna protocol , the log ratio values were still centered around zero at different mean expression levels ( fig 3b )  . 
difference in measurements as log ratio ( m ) versus mean average expression ( a ) of each gene ( ma plot ) of 20 , 381 coding region ( cr ) targeted poly ( a ) + genes for tumor sample c when using ff.k.totalrna sample c library as the reference . 
m is the log2 - transformed expression of a gene from first library divided by that from the second library , and a is the mean log2 transformed expression of the gene . 
generally , the cr protocol tended to overly enrich the highly expressed genes and was more likely to not capture low expressed genes ( fig 3c ; data supplement )  . 
this was not improved by prior demodification of methylol adducts from ffpe tissuederived rna using heat and amines or the srna protocol ( fig 4 ; data supplement )  . 
although both approaches seemed to slightly increase concordance of expression , neither was statistically significant . after further investigating these protocol induced biases , we calculated the number of genes that would be considered as differentially expressed or false positives compared with each reference ff standard protocol ( data supplement )  . 
cr , coding region protocol ; dem , demodification ; ff , fresh frozen ; ffpe , formalin - fixed paraffin - embedded ; srna , sense rna protocol . and triple receptornegative breast cancers within each protocol . 
the p value from de analysis followed the ideal uniform distribution for non - de genes , with a spike close to zero for the de genes ( data supplement )  . 
 principal component analyses demonstrated the following order of variables influencing gene expression measurements from rna - sequencing : whether the library preparation protocol used exon capture for cr , whether the sample was from ff tissue or ffpe tissue , and the biologic phenotype of the breast cancer based on hrs and her2 receptor status ( fig 2 )  . 
nevertheless , we identified one protocol , ffpe.k.totalrna , with consistently good transcript coverage uniformity and continuity , most concordant expression , and least differential expression when compared with the different non - cr protocols with fresh tissue . 
it had a reasonable requirement of total rna input ( 100 ng ) for ffpe biopsy samples . the first translational research scenario that we posed , in the introduction section , considered the best pairing of protocols that would enable discovery using ff samples with intention to later translate for use with ffpe samples . 
this interpretation was supported by the quality of read coverage , pattern of coding sequence expression , and translation of overall or phenotype - related gene expression profiles and prognostic signatures . the cr protocols yielded concordant results , but different from all other ( non - cr ) protocols . 
 also , changes to the population of exon capture probes within a commercial kit over time could be a potential risk to this approach . the most generalizable results for discovery research from ffpe samples were obtained using the total.rna protocols without exon capture . 
for our second scenario , therefore , we prefer the k.totalrna protocol for best representation of the transcriptome in ffpe samples used for discovery researchaiming to represent the transcriptional information that ff samples would have provided . our third translational research scenario involves the translation of an existing gene expression signature that was previously developed using a different method ( eg , microarray ) or a particular rna - seq protocol . 
the inclusion of random and dt primers and the t7 promoter region ( srna protocol ) to simulate the ff.mrna protocol produced good concordance overall but introduced a high number of nonconcordant mapped reads , nonuniformity , and discontinuity of read coverage across the transcriptome . limitations to our study include small sample size ( although cancers were selected to represent biologic diversity ) ; optimally short time to fixation of tissues and possibly , as a result , a modest degree of degradation of ffpe samples ( dv200 ranges from 65% to 85% ) ; optimal amount of input rna used for non - cr protocols ( at least 100 ng ) ; and lack of generalizability ( single institution conditions of tissue processing )  . 
one tumor ( sample n ) seems to be compromised by unknown technical processing ; our study conclusions , whenever involving this sample , are based on robust point estimates ( eg , median estimates in fig 4 ) across all samples to avoid being driven by its outlier effect . 
for more information about asco 's conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . jialu li stock and other ownership interests : genomic health chunxiao fu no relationship to disclose terence p . 
fraser symmans stock and other ownership interests : ionis pharmaceuticals , nuvera biosciences , delphi diagnostics consulting or advisory role : genentech patents , royalties , other intellectual property : patent pending for gene expression measurement of sensitivity to endocrine therapy travel , accommodations , expenses : luminex supported by the cancer prevention research institute of texas grant no . 
masuda n , ohnishi t , kawamoto s , et al : analysis of chemical modification of rna from formalin - fixed samples and optimization of molecular biology applications for such samples . 
fumagalli d , blanchet - cohen a , brown d , et al : transfer of clinically relevant gene expression signatures in breast cancer : from affymetrix microarray to illumina rna - sequencing technology . 
zhao w , he x , hoadley ka , et al : comparison of rna - seq by poly ( a ) capture , ribosomal rna depletion , and dna microarray for expression profiling . 
loi s , haibe - kains b , majjaj s , et al : pik3ca mutations associated with gene signature of low mtorc1 signaling and better outcomes in estrogen receptor - positive breast cancer . 
in this analysis the hypothesis , we explore with an unsupervised learning algorithm whether distinct subtypes of btcp exist and whether they can provide new insights into clinical practice . methods partitioning around a k - medoids algorithm on a large data set of patients with btcp , previously collected by the italian oncologic pain survey group , was used to identify possible subgroups of btcp . 
a free online tool was created for new patients cluster computation to validate these clusters in future studies and provide handy indications for personalized btcp therapy . conclusion this work proposes a classication for btcp and identies subgroups of patients with unique efcacy of different pain medications . 
this work supports the theory that the optimal dose of btcp opioids depends on the dose of basal opioids and identies novel values that are possibly useful for future trials . 
these results will allow us to target btcp therapy on the basis of patient characteristics and to dene a precision medicine strategy also for supportive care . jco precis oncol 4 : 1339 - 1349 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction breakthrough cancer pain ( btcp ) is a common event that affects a considerable proportion of patients with cancer.1 a variety of denitions for btcp have been proposed2 , 3 . 
according to the italian oncologic pain survey ( iops ) study group , 4 btcp should be dened as a relevant change in pain intensity of severe intensity in patients who receive an effective treatment with opioids.4 ( p963 ) nevertheless , despite this unique denition , btcp encloses a wide range of manifestations that differ , among other features , in intensity , duration , frequency , and triggering events . btcp represents a clinically relevant condition with a negative impact on the patients quality of life . 
patients characteristics characteristic value ( n = 4 , 016 ) 2 , 202 ( 54.8 ) male sex interview setting oncology pain therapy palliative care radiotherapy treatment corticosteroids anticonvulsant drugs acetaminophen constipation drugs anxiolytic drugs antidepressant drugs antiemetic drugs nsaids cannabis treatment setting inpatient outpatient domicile day hospital hospice cancer type lung breast pancreas colon prostate rectum stomach bladder at present , several gaps exist in the knowledge of btcp management . 
these partially unanswered questions , among others , concern the optimal drug administration route , pharmacokinetics , the balance between rapid - onset and slow - onset opioids , and the eventual difference of btcp response deriving from clinical features , such as stage , primary site , or metastases . in this analysis , it was thus hypothesized that the unique btcp denition might actually enclose diverse pathologic entities , possibly with peculiar clinical needs and specic responses to drugs . 
these so - called unsupervised learning algorithms have already been extensively used , for example , for the identication of breast cancer subtypes.6 nevertheless , to our knowledge , no authors have yet tried to explore the issue of btcp management using these techniques . to fulll this purpose , we used data that were collected by the iops group in a large , multicentric national study5 , 7 , 8 that enrolled 4 , 056 patients from 32 centers with opioidcontrolled basal pain suffering from btcp . 
this work is therefore a secondary analysis of the iops group survey that aims to identify novel subtypes of btcp through the use of unsupervised learning algorithms . methods patients enrollment and data collection details concerning the enrollment of patients are extensively described in the main paper from the iops group.5 in brief , local ethical committees approved the protocol , and written informed consent was obtained from each patient . interviews were performed in different settings , in particular , oncology , pain therapy , palliative care , and radiotherapy . 
a comprehensive list of clinical variables was collected for each patient that consisted of basal pain and btcp site , duration , frequency , intensity , relieving factors , triggers , drugs , primary cancer site and stage , and concomitant symptoms for a total of 1 , 086 1340 2020 by american society of clinical oncology multiple primary average age , years ( range ) karnofsky performance status ( range ) baseline pain , nrs scale ( range ) note . 
 breakthrough cancer pain clinical features and opioids response features with less than 5% of missing data and associated with a corrected p value of , .1 and , for categorical features , a log2 odds ratio greater than 1 were used to build a multivariable logistic regression . 
to investigate the correlationsimultaneously for all patients and on the same scalebetween the amount of opioids used and btcp therapy satisfaction , all doses of opioid drugs were converted10 to equivalent intravenous morphine doses and expressed as a total daily dose : one for btcp - directed opioids and for basal pain opioids . 
doses were converted to oral morto intravenous morphine doses and not phine doses because intravenous morphine has been increasingly used in different clinical settings and would provide more interpretable graphics in results . 
moreover , to explore the interaction of fast - acting and long - acting opioid dosages , we calculated for each patient the btcp opioidstobasal pain opioids ratio ( opr )  . 
a polynomial logistic regression was used to catch nonlinear relationships between opioid doses and therapy satisfaction . cluster computation and visualization features dening the clinical characteristics of btcp were selected to perform clusters computation . 
the above - mentioned features were used to calculate a dissimilarity matrix using a cluster package11 ; presence of background pain pain intensity 4 of 10 four or fewer episodes per day breakthrough pain presence of peaks well distinguished from background pain intensity cluster fig 1 . 
 ( a ) algorithm used for the diagnosis of breakthrough cancer pain ( btcp ) during patients enrollment in the italian oncologic pain survey ( modied from mercadante et al8 )  . 
 ( b ) a two - dimensional t - distributed stochastic neighbor embedding projection of all patients , colored by their clusters , on the basis of the following btcp features : number of btcp episodes , btcp peaks duration , btcp type , btcp intensity , number of days since the beginning of btcp episodes , eventual benet from pharmacotherapy , eventual benet from rest , and whether btcp was enhanced by movements . each point represents a patient . 
silhouette statistics14 were calculated for each run , and the optimal number of clusters was manually picked as being that with the best trade - off between silhouette statistics and reasonable clinical interpretation . 
we used complete - linkage hierarchical clustering with 12 clusters , along with rand index calculation , to explore the replicability of clusters with a different algorithm . t - distributed stochastic neighbor embedding15 algorithm was used to project dissimilarities between patients in a bidimensional space , with closer points representing patients with more similar clinical btcp features . 
an online tool allows for the repetition of the performed classication on new sets of patients.16 clusters analysis t - test , mann - whitney test , and 2 test were used to assess the association of parametric , nonparametric , and categorical features , respectively , with each cluster . 
patients characteristics are listed in table 1 . cluster computation to investigate whether subtypes of btcp exist , we used btcp features to build an unsupervised clustering model . the number of btcp episodes , btcp peaks duration , btcp type , btcp intensity , number of days since the beginning of btcp episodes , the eventual benet from pharmacotherapy , the eventual benet from rest , and whether btcp was enhanced by movements were the eight btcp - dening variables selected for the nal model , which was built with the k - medoids algorithwe chose 12 as an optimal trade - off between the average width of clusters silhouette ( 0.45 ; appendix fig a1a ) and the interpretability of the clusters themselves . 
 pantano et al figure 1 shows the algorithm used to dene btp ( fig 1a ) t - distributed stochastic neighbor and a 2 - dimensional embedding projection of all patients , colored by their clusters ( fig 1b )  . 
an online tool is available for the classication of new patients according to our method.16 characteristics of btcp clusters we analyzed the enrichment of the eight btcp - dening variables and of other clinical features among the clusters . a description of each cluster is available in table 2 . 
a summary of btcp features according to cluster is presented in figure 2 . btcp therapy satisfaction finally , we tried to assess what inuenced patient - reported btcp therapy satisfaction . 
after converting the opioid dose to a unique scalecorresponding to the equivalent dose of intravenous morphinewe investigated using a nonlinear model the inuence of basal opioid dose , btcp opioid dose , and opr on patient - reported therapy satisfaction . 
of higher therapy satisfaction lower therapy satisfaction btcp opioids dose / basal pain opioids dose higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction btcp opioids dose ( mg ) basal pain opioids dose ( mg ) fig 3 . 
this roughly corresponds to a daily dose of sublingual fentanyl 100 g for btcp and a daily dose of oral morphine 30 mg as the basal opioid dose . we separately performed the same analyses on previously dened clusters ( fig 3d )  . 
for clusters 1 , 6 , and 10 , the satisfaction seemed to grow indenitely with an increase of the opr opioids , whereas clusters 7 , 8 , and 11 seemed to have clear , optimal peaks of opr . 
despite the interpretation being challenged by some large cis , we can say from these data that , depending on the cluster , optimal opr ranges from 15% to 50% . discussion this paper demonstrates a novel approach for the investigation of btcp . 
we acknowledge that this study was not designed to perform this analysis and , moreover , that the large number of clusters might interfere with their interpretability and clinical utility . 
nevertheless , this study represents a proof - ofconcept for this investigational approach . cluster 1 cluster 2 cluster 3 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction cluster 4 cluster 5 cluster 6 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction cluster 7 cluster 8 cluster 9 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction cluster 10 cluster 11 cluster 12 higher therapy satisfaction higher therapy satisfaction higher therapy satisfaction lower therapy satisfaction lower therapy satisfaction lower therapy satisfaction fig 3 . 
using our same data , another group proposed 0.20 ( one fth ) as the optimal ratio.5 nevertheless , they used a frequentistic approach , as 0.20 is simply the most common ratio among the cohort . 
this possibly suggests that , instead of starting btcp opioid titration with the lowest possible dosage , as proposed previously , 28 titration could start immediately with an optimal opioid dosage . moreover , cluster analysis reveals that this ratio might not be the same for all patients : some patients might benet from a higher btcp opioid dosage ( cluster 2 and 7 ) , whereas others might benet from a lower one ( cluster 11 )  . 
finally , for some patients , we did not observe an upper threshold for this ratio ( cluster 1 , 6 , and 9 ) , perhaps pointing out patients for whom a strong btcp opioid dosage increase is required . the interpretation is made difcult by the multiple associations and , at this stage , is not mature enough to suggest any immediate change in clinical practice . 
however , we made available an online free tool16 that allows for the classication of new patients according to our algorithm and returns a proposed btcp therapy which depends on the patient cluster optimal opr and basal opioid dose . 
we suggest that this tool might be used in the future to prospectively validate the clinical importance of our clusters in clinical practice and to compare our proposed opioid dosages in settings different from ours . the presence of distinct btcp phenotypes , each one associated with specic clinical features , could also be a reection of diverse underlying pathophysiologic mechanisms : our work suggests that preclinical research might gain insight into these possible differences and help the development of a tailored therapy also for btcp . the main limitation of our study is the appropriateness of collected data for the scope of our work . 
we believe that a prospective study specically designed for the investigation of btcp clusterspossibly with long - term follow - up and therapy success outcomes and not limited to a single timepoint evaluationmight enable a clearer identication of distinct clusters . 
businco hospital , asl 8 , cagliari , italy 20department of biotechnological and applied clinical sciences , section of clinical epidemiology and environmental medicine , university of laquila , laquila , italy 21section of clinical pharmacology and oncology , department of health sciences , university of florence , florence , italy 22department of medicine and surgery sciences , university of bologna , bologna , italy 23paintherapy , s . 
croce e carle hospital , cuneo , italy 24pain therapy ics maugeri , irccs foundation , pavia , italy 25medical oncology , azienda sanitaria universitaria integrata di trieste , trieste , italy 26medical oncology , azienda sanitaria universitaria integrata di udine , udine , italy 27palliative care and oncologic pain service , s . 
pain 41 : 273 - 281 , 1990 portenoy rk , payne d , jacobsen p : breakthrough pain : characteristics and impact in patients with cancer papain 81 : 129 - 134 , 1999 4 . 
mercadante s , marchetti p , cuomo a , et al : breakthrough pain and its treatment : critical review and recommendations of iops ( italian oncologic pain survey ) expert group . 
mercadante s , marchetti p , cuomo a , et al : breakthrough cancer pain : preliminary data of the italian oncologic pain multisetting multicentric survey ( iopsms )  . 
mercadante s , lazzari m , reale c , et al : italian oncological pain survey ( iops ) : a multicentre italian study of breakthrough pain performed in different settings . benjamini y , hochberg y : controlling the false discovery rate : a practical and powerful approach to multiple testing . 
davies an , dickman a , reid c , et al : the management of cancer - related breakthrough pain : recommendations of a task group of the science committee of the association for palliative medicine of great britain and ireland . 
the appropriate number of clusters for additional analyses was found to be 12 , an optimal trade - off between the average width of clusters silhouette ( 0.45 ) and the interpretability of clusters themselves . ( b ) heatmap showing the concordance of pam clustering with complete - linkage hierarchical clustering . 
survival curves , number of samples classied as tmb high , and predicted neoantigens were used to evaluate the differences between thresholds . results the distribution of tmb varied dramatically among cancer types . 
2019 by american society of clinical oncology introduction immunotherapy ; immunotherapy , especially checkpoint inhibition , has been added recently as a successful treatment option for some patients with cancer . 
it is based on the presence of neoantigens eliciting a response from t cells by recognizing these antigens as foreign and inltrating the tumor microenvironment.1 , 2 however , only a subset of patients respond to checkpoint inhibitor therefore , predictive biomarkers are critical to guide the selection of patients for these therapies . 
although high - level programmed death - ligand 1 expression , microsatellite instability , and mismatch - repair deciency have been deemed including tumor clinically relevant , other markers , mutational burden ( tmb ) , interferon gamma prole , and human leukocyte antigen ( hla ) genotype , have also exhibited promising results.3 tmb is commonly dened as the total number of somatic mutations in a tumor genome , divided by the number of bases sequenced in megabases ( mb ) .4 , 5 previously , patients with higher tmb ( tmb high ) demonstrated increased response to immunotherapy compared with patients with lower tmb ( tmb low ) , especially in nonsmallcell lung cancer.6 , 7 however , no consensus has been established to dene a standard threshold for tmb high . 
last , previous studies have adopted panel target sequencing with small regions of genomic dna , possibly excluding neoantigen candidates.8 therefore , exploring the tmb distribution with more extensive sequencing platforms , such as whole exome sequencing ( wes ) , can provide a more comprehensive view of tmb . 
 fernandez et al context threshold ? key objective can a cancer - specic tumor mutational burden ( tmb ) provide more useful information compared with a xed pan - cancer knowledge generated a cancer - specic tmb threshold can dynamically adjust to identify dramatically more patients as tmb high compared with a restrictive pan - cancer threshold . 
the additional patients do not have a signicantly different outcome compared with the other tmb - high patients . relevance when interpreting a patients tmb , the overall tmb seen in the specic cancer type should be taken into consideration to give the tmb context . reect tmb in each cancer type , the wcm threshold uses interquartile range ( iqr ) : mean ( tmb ) + 1.25 iqr ( tmb ) applied within each cancer , meaning each cancer type will have its own threshold reective of the distribution of mutations within that cancer type . 
predicted neoantigens for tcga samples were obtained through the cancer immunome atlas.23 tmb calculation tmb was calculated as the total number of nonsynonymous mutated bases in the tumor genome divided by the mb of the genome covered . 
the wcm advanced cohort was sequenced using our exact - 1 wes haloplex pipeline using tumor - normal pairs , 24 which covers 37 mb of the genome . samples were collected under a protocol approved by the institutional review board of weill cornell medical college , and written informed consent was obtained . 
because tmb is divided by the total size of genome sequenced to help adjust for technical batch effects , the size of sequenced regions was determined for each tcga cohort according to their respective publications.11 - 22 samples with purity of less than 50% according to absolute ( tcga ) or clonality estimate in tumors ( exact - 1 ; weill cornell medine clinical genomics lab , new york , ny ) were removed.25 , 26 germline variants and variants appearing in the exome aggregation consortium database with a frequency of at least 1% were removed to lter them out.27 variants with a variant allele frequency ( vaf ) of less than 10% were ltered out after correcting vaf for tumor purity by dividing vaf by purity . 
a summary of ltering steps can be seen in the data supplement . mutational signatures mutational signatures were determined using the deconstructsigs r package.28 for each sample , a matrix containing the frequency a mutation appears within a trinucleotide context was generated . 
this matrix was compared with the signatures published previously in the catalogue of somatic mutations in cancer , 29 resulting in signature contributions . statistical methods the wilcoxon rank sum test was used to compare sample distributions . 
for example , the tmb for prostate cancer in tcga ranged from 0.03 mutations / mb to 14.13 distribution of tmb for tcga samples cancer type distribution of tmb for wcm advanced samples threshold chalmers et al threshold chalmers et al cancer type fig 1 . 
however , the tmb for bladder cancer in tcga ranged from 0.04 mutations / mb to 99.68 mutations / mb , with a mean of 6.92 mutations / mb ( n = 375 )  . because of the higher frequency of metastatic samples in the wcm advanced cohort , we sought to understand how the distribution of tmb changes between primary and metastatic samples . 
the chalmers et al threshold is a constant cutoff of 20 mutations / mb for all cancer types , 4 whereas our custom wcm threshold is a formula of mean ( tmb ) + 1.25 iqr ( tmb ) , adapted from a study by zehir et al.5 the wcm threshold was applied per cancer to account for the variation in tmb among cancer types . data for patients treated with immunotherapy were not available for either cohort ; however , tcga survival outcomes were investigated to understand the differences in survival between tmb high and tmb low using both thresholds . 
tmb - high patients showed signicantly improved survival compared with tmb - low patients for blca using both the wcm threshold ( log - rank p value = .0014 ) and the chalmers et al threshold ( log - rank p value = .009 ; data supplement )  . 
lusc showed improved survival for tmb - high patients compared with tmb - low patients when using the wcm cutoff ( log - rank p value = .036 ) but not when using the chalmers et al cutoff ( log - rank p value = .11 ; data supplement )  . 
ucec also showed signicantly improved survival for tmb - high patients compared with tmb - low patients when using chalmers et al ( log - rank p value = .023 ) but did not reach signicance when using wcm ( log - rank p value = .055 ; data supplement )  . 
to further compare the performances of the two thresholds , timedependent roc curves were created at the 5 - year time point ( fig 2d ; data supplement )  . 
to explore the difference between the patients selected by the thresholds , we split the samples into three groups : tmb high , wcm - tmb high , and tmb low . 
the wcm - tmbhigh group contained samples classied as tmb high by wcm and tmb low by chalmers et al ( when chalmers et al had more tmb high classications [ ucec ] than wcm , we used chalmers - tmb high [ chm - tmb high ] )  . 
the tmb - low group contained samples classied as tmb low by both methods ( fig 2a )  . the wcm - tmbhigh group did not attain signicantly improved survival compared with the tmb - low group for blca ( log - rank p value = .072 ; fig 2b )  . 
the chalmers et al threshold did not classify any patients with kirc as tmb high . although the survival trends were not signicantly different between the cutoffs , the number of samples classied as tmb high differed between thresholds . 
out of 14 tcga cancer types investigated , eight cancers had a statistically larger tmb - high group for wcm compared with chalmers et al ( blca [ fold change = 1.9 ] , brca [ fold change = 6.7 ] , gbm [ fold change = 2.7 ] , kirc [ no high by chalmers ] , lgg [ fold change = 13.0 ] , ov [ fold change = 5.67 ] , prad [ no high by chalmers ] , and thca [ no high by chalmers ] ) ; ve cancers had no statistically signicant change in the number of tmb - high classications ( coad , kich , luad , lusc , and read ) ; and only ucec had a large number of tmb high classied by chalmers et al compared with wcm ( 2 test with yatess continuity correction ; p value , .05 ; fig 3a )  . 
predicted neoantigens from the cancer immunome atlas compared the tmbhigh , the wcm - tmbhigh , and the tmb - low groups for tcga samples ( fig 4a ) .23 the tmb - low group had signicantly fewer neoantigens than both the tmb - high ( wilcoxon p value , 2.3e - 16 ) and wcm - tmbhigh ( wilcoxon p value = 2.1e - 14 ) group . 
kaplan - meier survival curves comparing the tmb classications between the weill cornell medicine ( wcm ) threshold and the chalmers et al threshold for ( b ) blca and ( c ) kirc . 
for kirc , the chalmers et al threshold was too high to classify any samples as tmb high , resulting in only two groups : wcm - tmb high and tmb low . 
 ( d ) time - dependent receiver operating characteristic ( roc ) curve comparing the true positive ( tpr ) and false positive ( fpr ) rates for blca using both the chalmers et al threshold and the wcm threshold shows the area under the curve ( auc ) for both cutoffs at 5 years from diagnosis . 
because of the observed variation in tmb among cancer types , neoantigens were also compared between the tmb groups for each cancer ( figs 4b and 4c ; data supplement )  . 
prostate adenocarcinoma ( prad ) and kidney renal clear cell carcinoma ( kirc ) are excluded from the plot because the chalmers et al threshold did not classify any samples as tmb high . 
blue bars represent cancer types with a higher or equal number of tmb - high classications for the weill cornell medicine ( wcm ) threshold than the chalmers et al threshold . 
overall , the tmb - high and wcm - tmbhigh groups showed increased neoantigen counts compared with the tmb - low group . finally , mutational signatures were compared among tmb groups . 
distribution of predicted neoantigens for tmb high ( blue ) , tmb high weill cornell medicine ( wcm ; red ) , and tmb low ( teal ) for the cancer genome atlas ( tcga ) shown for ( a ) all cancers pooled together , ( b ) lung adenocarcinoma ( luad ) , and ( c ) bladder urothelial carcinoma ( blca )  . 
 ( a ) violin plots showing the distribution of the contribution of signature 10 ( defective polymerase - ) in tumor mutational burden ( tmb ) high , chalmers ( chm ) - tmb high , and tmb low . 
 ( b ) pca showing the signature contributions for uterine corpus endemetrial carcinoma ( ucec ) with tmb - high samples in blue , wcm - tmbhigh samples in red , and tmb - low samples in teal . 
only signatures 2 , 4 , 6 , 10 , 13 , 15 , 20 , 21 , and 26 were considered , to focus on signatures with the most relevant interpretations . 
for example , the chalmers et al cutoff of 20 mutations / mb is higher than the maximum tmb seen within tcga prostate cancer ( 14.13 mutations / mb ) ; however , using a lower threshold might be too lenient for tcga bladder cancer ( maximum tmb of 99.68 mutations / mb )  . 
the dramatic difference in tmb among cancer types led us to explore a tmb threshold applied in a cancer - specic manner . to a cancer - specic when comparing a pan - cancer threshold , we found we were able to maintain differences in survival trends between tmb high and tmb low , often while including more patients in the tmb - high group by using the cancer - specic threshold . 
using a tmb threshold that has a larger number of tmb - high classications while not having signicantly different survival trends than a more stringent threshold can potentially open treatment options to patients if they can be shown to respond well . 
hr , hazard ratio ; os , overall survival ; wcm , weill cornell medicine . seen in recent publications suggests that tmb alone is not a critical predictor of survival for nonimmunotherapy treatment response.6 , 37 , 38 differences in tmb distribution between the tcga and wcm advanced cohorts could be a result of biologic or technical differences . 
tcga contains primary tumor samples , and wcm advanced contains mostly metastatic tumor samples . when comparing different cohorts of patients , many technical differences can inuence tmb , making a static threshold potentially less accurate . 
after sequencing , the exact - 1 pipeline and tcga pipeline use different mutation callers and apply different quality lters . in addition , when comparing tmb among studies , it is important to understand the variants that were considered . 
 fernandez et al calculating tmb.6 , 38 , 39 targeted panels cover different genes and sizes of the genome and at a higher sequencing depth than wes , inuencing the estimated distribution of tmb . 
the panel must cover at least 2 mb of the genome to have high sensitivity and specicity when measuring tmb.8 a static threshold would not be able to adjust to the differing levels of tmb resulting from different panels . 
however , a dynamic threshold would be able to adjust for technical differences . the cancer - specic threshold adjusted for the variation in tmb ; however , the pan - cancer threshold classied more patients as tmb high for ucec . 
mutational signatures for these samples showed a cluster of patients with pole deciency , which led to a large number of mutations and a tmb distribution with a large iqr , 22 causing the cancerspecic threshold to be strict in this case . the survival analyses in this study were limited by a lack of patients undergoing immunotherapy treatment . 
in addition , the number of predicted neoantigens was compared per cancer , showing that a cancer - specic threshold identies patients with a higher number of neoantigens compared with tmb - low patients . moreover , tmb might depict only one factor in the success of immunotherapy . 
a recent study has shown that patients with melanoma and nonsmall - cell lung cancer with heterozygous hla class i exhibit improved survival compared with patients who are homozygous.40 because of the limitation of tcga data , we could not examine the role of hla class i in the current study . 
fernandez employment : celgene travel , accommodations , expenses : foundation medicine himisha beltran consulting or advisory role : janssen oncology , genzyme , glaxosmithkline , abbvie , astellas pharma , astrazeneca research funding : janssen ( inst ) , abbvie / stemcentrx ( inst ) , eli lilly ( inst ) travel , accommodations , expenses : janssen oncology bishoy m . 
faltas honoraria : digital science press publications research funding : eli lilly juan miguel mosquera research funding : personal genome diagnostics travel , accommodations , expenses : personal genome diagnostics david m . 
hoffmann la roche ag , novartis , astellas pharma research funding : eli lilly , janssen , millenium pharmaceuticals , sano patents , royalties , other intellectual property : us patent ( 7 , 767 , 393 and 7 , 229 , 774 ) , expression prole of prostate cancer , 2007 ; us patent ( 7 , 332 , 290 ) , detection of amacr cancer markers in urine , 2008 ; us patent ( 7 , 718 , 369 ) , recurrent gene fusions in prostate cancer , 2010 ; us patent ( 7 , 803 , 552 and 7 , 666 , 595 ) , biomarkers for predicting prostate cancer progression , 2010 ; us patent ( 7 , 981 , 609 b2 ) , methods for identifying and using snp panels , 2011 ; us patent ( 8 , 106 , 037 b2 ) , identication and treatment of estrogen responsive pca , 2012 ; us patent ( 9 , 090 , 899 b2 ) , methods of diagnosing and treating prostate cancer characterized by ndrg1 - erg fusion , 2015 ; us patent ( 9 , 458 , 213 b2 ) , compositions and methods for diagnosing prostate cancer based on detection of slc45a3 - elk4 fusion transcript , 2016 ; us patent ( 9 , 568 , 483 b2 ) , molecular subtyping , prognosis and treatment of prostate cancer , 2017 ; us patent ( 9 , 678 , 077 b2 ) , erg / tff3 / hmwck triple immunostain for detection of prostate cancer , 2017 ; us patent ( 61 , 408 , 341 ) , exploration of novel gene fusion in prostate cancer by rna - seq travel , accommodations , expenses : f . 
shah consulting or advisory role : astellas pharma , eli lilly japan research funding : gilead sciences ( inst ) , merck ( inst ) , boston biomedical ( inst ) , oncolys biopharma ( inst ) , bristol - myers squibb ( inst ) wei song employment : genentech ( i ) employment : cytokinetics ( i ) honoraria : foundation medicine , loxo consulting or advisory role : foundation medicine , loxo no other potential conicts of interest were reported . acknowledgment we thank juan sebastian andrade martinez for his previous work with the wcm advanced cohort and bhavneet bhinder for her advice on predicted neoantigens . references 2018 topalian sl , weiner gj , pardoll dm : cancer immunotherapy comes of age . 
j clin oncol 29 : 4828 - 4836 , 2011 topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of anti - pd - 1 antibody in cancer . 
n engl j med 366 : 2443 - 2454 , 2012 tray n , weber js , adams s : predictive biomarkers for checkpoint immunotherapy : current status and challenges for clinical application . 
cancer immunol res 6 : 1122 - 1128 , 2018 chalmers zr , connelly cf , fabrizio d , et al : analysis of 100 , 000 human cancer genomes reveals the landscape of tumor mutational burden . 
genome med 9 : 34 , 2017 zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
n engl j med 378 : 2093 - 2104 , rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
lancet 387 : 1909 - 1920 , 2016 buchhalter i , rempel e , endris v , et al : size matters : dissecting key parameters for panel - based tumor mutational burden analysis . 
plimack er , dunbrack rl , brennan ta , et al : defects in dna repair genes predict response to neoadjuvant cisplatin - based chemotherapy in muscle - invasive bladder cancer . 
biometrics 56 : 337 - 344 , 2000 johnson db , frampton gm , rioth mj , et al : targeted next generation sequencing identies markers of response to pd - 1 blockade . 
rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
 megakaryocyte potentiating factor as a predictive biomarker for therapies against malignant mesothelioma purpose effective biomarkers for malignant mesothelioma ( mm ) are needed for clinical management and the development of mesothelin - targeted therapies . 
we evaluated serum megakaryocyte potentiating factor ( mpf ) as a biomarker predictive of treatment outcome in patients with mm and for developing mesothelin - targeted therapies . materials and methods serial serum samples from patients with mm in two clinical trials of an antimesothelin immunotoxin were tested with our clinically validated mpf assay . 
mpf was further evaluated for an association with response to an antimesothelin therapy and for disease monitoring . results there was a significant reduction of serum mpf in patients with elevated baseline and radiologic response , with an average change from 52% to 78% after one to six cycles . 
 potentiating factor ( mpf ) and membrane - bound mesothelin.15 , 16 previous studies showed correlations between the computed tomography ( ct ) response and arbitrarily chosen 10% to 25% reduced serum mesothelin after chemotherapy.17 - 21 such low cutoff values are incompatible with a 30% reduction in tumor determined with ct , would contribute to high degrees of false signals , and would make it more difficult to correlate with clinical outcomes . the currently available mesomark test ( fujirebio , malvern , pa ) detects serum mesothelin , which is subject to the interference by mesothelin - targeted antibody - based agents . 
we developed and validated an assay for mpf and further showed that elevated mpf is a worse prognostic biomarker in patients with mm.22 its effectiveness for monitoring therapies is not known . 
the first trial was a phase i study with a standard dose of pemetrexed and cisplatin , and the antimesothelin immunotoxin ss1p ( nct01445392 ) in chemotherapy - nave patients with pleural mesothelioma.19 twenty patients were evaluable , 12 with partial response ( pr ) , three with stable disease ( sd ) , and five with progressive disease ( pd )  . 
the patients had received one to six ( and an average of three ) previous therapies.8 all patients were evaluated for responses : three with pr , three with sd , and four with pd . 
tumor responses were determined on the basis of ct and calculated in accordance to modified response evaluation criteria in solid tumors ( mrecist ) criteria for mesothelioma . statistical analyses prism , version 7.0 ( graphpad , la jolla , ca ) was used for statistical analysis . 
 kaplan - meier survival analyses were performed to determine log - rank hazard ratio ( hr ) and p value of mpf response or ct response patients on pfs or os . 
on the basis of the linear regression analysis of corresponding changes in ct and mpf in these 20 patients with mm , a 30% change in ct was interpolated to a 47% change in mpf level ( fig 1b )  . 
thus , a rounded 50% change in serum mpf was selected as the cutoff for mpf response , which corresponded to approximately 30% change in ct using mrecist . the serum mpf test enables continuous and multiple measurements during treatment . 
among pr patients with an elevated mpf using the upper limit of normal at 1.2 ng / ml , 22 there was an average of 52% change in mpf after one cycle ( p < .001 ; n = 12 ; fig 1c )  . 
in contrast , for the patients who did not have a ct response , there was no significant reduction of mpf ( n = 14 ; fig 1d )  . 
thus , the treatment induced reduction of serum mpf may be an informative biomarker of objective response in patients with mm with elevated baseline mpf . kaplan - meier analyses were performed to compare pfs and os of both trials . 
thus , the data suggest that a 50% change in mpf after systemic therapies is strongly associated with improved pfs . reduction of mpf after systemic treatment as a potential biomarker for better os the mpf response was further correlated with os . 
landmark analysis of os for mpf and ct response was performed , with a landmark date at 91 days , at which time all patients had experienced a response but one . 
 ( a ) analysis of the changes in serum mpf in patients with partial response ( pr ) , stable disease ( sd ) , and progressive disease ( pd )  . 
all data are shown as mean standard deviation . depletion regimen of pentostatin and cyclophosphamide , major cancer regressions were observed and were attributed primarily to the activities of ss1p.8 the nonparametric mann - whitney test showed that the patients with pr ( by ct ) had elevated baseline serum mpf levels , which were higher than those in the nonresponse group ( p = .033 ; fig 3a )  . 
thus , data suggest that elevated baseline serum mpf may be associated with the response to an effective antimesothelin therapy in patients with refractory mm , whereas the mpf response is associated with improved survival in these patients ( p = .012 ; appendix fig a4 )  . 
 20 pfs since in - study date ( months ) os since in - study date ( months ) mpf response mpf nonresponse log - rank p < .001 hazard ratio = 0.279 ct response ct nonresponse log - rank p = .022 hazard ratio = 0.457 mpf response mpf nonresponse log - rank p = .004 hazard ratio = 0.361 ct response ct nonresponse log - rank p = .035 hazard ratio = 0.476 pfs since in - study date ( months ) os since in - study date ( months ) fig 2 . 
 ( a ) progression - free survival ( pfs ) and ( b ) overall survival ( os ) using mpf response at a threshold of 50% or more after therapies . 
 ( c ) progression - free survival and ( d ) os for patients with malignant mesothelioma using computed tomography ( ct ) response on the basis of modified response evaluation criteria in solid tumors . 
102 was a 50 - year - old man with extensive peritoneal involvement and received two cycles of ss1p because of ss1p antibody development.8 he had a delayed response with substantial tumor shrinkage at 7 months . 
103 , a 56 - year - old woman with pleural mesothelioma , had rapid disease progression before treatment and was the only patient who completed all six cycles of therapy . 
105 , pr response progression cutoff response progress response time since in - study date ( months ) time since in - study date ( months ) cutoff cutoff fig 3 . 
elevated baseline megakaryocyte potentiating factor ( mpf ) associated with response and long - term follow - up of individual patients with major tumor regression after antimesothelin and immune suppression . 
there was evidence of increased serum mpf at the time of disease progression for all . discussion our study indicates that the serum mpf test is effective in monitoring systemic therapies for patients with mm , because the patients with mpf responses have much better pfs and os than those without , regardless of baseline levels . 
in mm , recist needs to be modified because one - dimensional measurement of the nonspherical growth pattern was difficult.24 the mrecist requires repeated total tumor measurements on two occasions 4 weeks apart for pr determination.25 the quantitative changes of serum mpf may provide an alternative , lowcost , and nonradiative assessment of therapy response in patients with mm with elevated mpf . 
 we used a more stringent cutoff value of a 50% change in mpf to define the biomarker response compared with the previous reports17 - 21 ; this cutoff was supported by our correlative analysis of ct and mpf responses in patients with mm . 
such a stringent cutoff correlates with the mrecist criterion of a 30% reduction in the sum for all target lesions and thus leads to a significant reduction of false - positive reports during monitoring . 
thus , in addition to confirming the association between changes in mpf and patients response to systemic therapy , 18 our results further showed that an mpf biomarker response is associated with improved pfs and os . as the cleavage product during mesothelin maturation with a short half - life in blood , 22 , 26 serum mpf levels reflect the expression of target antigen mesothelin on tumor cells , without being bound by the therapeutic agents . 
in fact , in untreated mesothelioma patients , there is a strong correlation between mpf and soluble mesothelin.22 , 27 the mpf test could be valuable for the clinical development of mesothelin targeted therapies and for monitoring targeted therapies against mm . 
therefore , serum mpf could facilitate long - term disease monitoring and provide a noninvasive assessment of the drug - target mesothelin expression in mm at the time of disease progression , which can be critical for evaluating alternative therapies . one of the most important issues in the development of targeted therapies is the stratification of the intended patient population . 
mesothelin is ubiquitously detected in epithelioid mm by immunohistochemistry ( table 1 ) ; therefore , mesothelin immunohistochemistry is not predictive of response to mesothelin - targeted therapies in mm , and a different biomarker test is required . 
 there are many challenges for a serum - based test for patient selection , including the expression of the tumor antigen by nontumor cells and the variations in shedding of it by tumor cells . 
 in addition , it is possible that serum mpf may be influenced by renal dysfunction in patients receiving nephrotoxic chemotherapies because prior reports showed elevated serum mpf in patients with renal disease.28 , 29 however , the patients described in our study had normal renal functions at the time of enrollment . 
although our previous data suggested that patients with mm with elevated mpf have a worse prognosis , 22 the results here suggest that the reduction of serum mpf in patients with refractory mm is associated with improved clinical outcome . 
vogelzang nj , rusthoven jj , symanowski j , et al : phase iii study of pemetrexed in combination with cisplatin versus cisplatin alone in patients with malignant pleural mesothelioma . 
hassan r , cohen sj , phillips m , et al : phase i clinical trial of the chimeric anti - mesothelin monoclonal antibody morab - 009 in patients with mesothelin - expressing cancers . 
golfier s , kopitz c , kahnert a , et al : anetumab ravtansine : a novel mesothelin - targeting antibody - drug conjugate cures tumors with heterogeneous target expression favored by bystander effect . 
le dt , brockstedt dg , nir - paz r , et al : a live - attenuated listeria vaccine ( anz - 100 ) and a live - attenuated listeria vaccine expressing mesothelin ( crs - 207 ) for advanced cancers : phase i studies of safety and immune induction . 
hollevoet k , nackaerts k , gosselin r , et al : soluble mesothelin , megakaryocyte potentiating factor , and osteopontin as markers of patient response and outcome in mesothelioma . 
hassan r , sharon e , thomas a , et al : phase 1 study of the antimesothelin immunotoxin ss1p in combination with pemetrexed and cisplatin for front - line therapy of pleural mesothelioma and correlation of tumor response with serum mesothelin , megakaryocyte potentiating factor , and cancer antigen 125 . 
creaney j , francis rj , dick im , et al : serum soluble mesothelin concentrations in malignant pleural mesothelioma : relationship to tumor volume , clinical stage and changes in tumor burden . 
hooper ce , lyburn id , searle j , et al : the south west area mesothelioma and pemetrexed trial : a multicentre prospective observational study evaluating novel markers of chemotherapy response and prognostication . 
onda m , nagata s , ho m , et al : megakaryocyte potentiation factor cleaved from mesothelin precursor is a useful tumor marker in the serum of patients with mesothelioma . 
iwahori k , osaki t , serada s , et al : megakaryocyte potentiating factor as a tumor marker of malignant pleural mesothelioma : evaluation in comparison with mesothel lung cancer 62 : 45 - 54 , 2008 28 . 
briefly , the mpf assay uses capture antibody mpf49 ( 2a , ) , which binds to mpf topographic epitope 3 , and detection antibody mpf25 ( 1 , ) , which binds to epitope 1.26 mpf49 was biotinylated , and mpf25 was conjugated with sulfo - tag nhs - ester ( meso - scale diagnostics , rockville , md )  . 
after incubation for 1 hour at room temperature , plates were washed , and the serially diluted mpf calibrator , 1 : 10 diluted sample serum , and reference samples were added and further incubated for 1 hour . 
the data were analyzed with workbench 4.0 software ( meso - scale diagnostic ) for determining the concentration of mpf in serum samples using the 4 parameter logistic nonlinear regression model . 
 efcacy of vemurafenib in patients with nonsmall - cell lung cancer with braf v600 mutation : an open - label , single - arm cohort of the histology - independent ve - basket study vivek subbiah , md1 ; radj gervais , md2 ; gregory riely , md , phd3 ; antoine hollebecque , md4 ; jean - yves blay , md , phd5 ; enriqueta felip , md , phd6 ; martin schuler , md7 ; anthony gonalves , md , phd8 ; antonio italiano , md , phd9 ; vicki keedy , md10 ; ian chau , md11 ; igor puzanov , md12 ; noopur s . 
raje , md13 ; funda meric - bernstam , md1 ; martina makrutzki , md14 ; todd riehl , pharmd15 ; bethany pitcher , mmath16 ; jose baselga , md , phd3 , 17 ; and david m . 
hyman , md3 , 17 purpose to study whether braf v600 mutations in nonsmall - cell lung cancer ( nsclc ) may indicate sensitivity to the braf inhibitor vemurafenib , we included a cohort of patients with nsclc in the vemurafenib basket ( ve - basket ) study . 
we present results from this cohort . methods this open - label , histology - independent , phase ii study included six prespecied cohorts , including patients with nsclc , and a seventh all - comers cohort . 
because the prespecied clinical benet endpoint was met in the initial nsclc cohort , the cohort was expanded . results sixty - two patients with braf v600mutant nsclc were enrolled and treated : 13% ( n = 8 ) had received no prior systemic therapy , and 87% ( n = 54 ) had received prior therapies . 
the safety prole of vemurafenib was similar to that observed in melanoma studies . conclusion vemurafenib showed promising activity in patients with nsclc harboring braf v600 mutations . the safety prole of vemurafenib was similar to previous observations in patients with melanoma . 
 subbiah et al context key objective to establish the efcacy and safety of vemurafenib in patients with braf v600 mutation - positive nsclc who were enrolled in the histology - independent vemurafenib basket ( ve - basket ) trial . knowledge generated vemurafenib has prolonged efcacy in patients with braf v600mutant nsclc ( n = 62 ) , as demonstrated by a 37% overall response rate . 
no new safety signals were observed in this expanded cohort of patients with nsclc . relevance single - agent vemurafenib has clinically meaningful and durable activity in patients with nsclc harboring braf v600 mutations . 
this analysis adds to the overall ndings of the ve - basket trial , which demonstrated clinically relevant activity of vemurafenib in a number of solid tumors . clinical study of patients with braf v600emutated nsclc.14 dual braf / mek inhibition has also been investigated as rstand second - line treatment of patients with nsclc.15 , 16 we present the results from the expanded nsclc cohort of the vemurafenib basket trial . 
this trial assessed the efcacy of vemurafenib in seven cohorts of patients with braf v600mutated malignancies.17 ( ve - basket ) methods study design the ve - basket study was a multicenter , single - arm , phase ii study of vemurafenib in patients with a variety of nonmelanoma cancers harboring braf v600 mutations . braf v600 mutations were identied by means of mutational analysis assays routinely performed at each participating site . 
six prespecied cohorts were recruited , consisting of patients with nsclc , ovarian cancer , colorectal cancer , cholangiocarcinoma , breast cancer , and multiple myeloma ; all patients with solid tumors other than those mentioned were included in a seventh cohort . 
the design of this study has been described in detail elsewhere.17 this trial was performed in accordance with the provisions of the declaration of helsinki and good clinical practice guidelines . 
all patients provided written informed consent . patients patients were eligible for inclusion in the study if they were 16 years of age or older and had histologically conrmed , measurable ( response evaluation criteria in solid tumors [ recist ] , version 1.1 ) , braf v600 mutation - positive cancers that were refractory to standard therapy or for which standard or curative therapy did not exist or was not considered appropriate by the investigator . 
assessments were performed using computed tomography or magnetic resonance imaging of the chest , abdomen , and pelvis at baseline and then every 8 weeks until disease progression , death , or withdrawal from the study . 
adverse events ( aes ) were graded by the investigators using national cancer institute common terminology criteria for adverse events ( version 4.0 ) until 28 days after discontinuation of study treatment . 
aes of special interest were cutaneous squamous cell carcinoma ( scc ; keratoacanthoma , squamous cell carcinoma of the skin , and bowen disease ) , fatigue ( fatigue and asthenia ) , liver injury ( increased alt , ast , blood alkaline phosphatase , blood bilirubin , and gamma - glutamyltransferase ; hyperbilirubinemia , hepatocellular injury , and cholestatic jaundice ) , and prolonged qt interval . 
patients were assessed for aes at each clinic visit and as necessary throughout the study . outcomes the primary objective of the study was to evaluate the efcacy of vemurafenib in patients with braf v600 mutation - positive cancers . 
the primary end point for the nal analysis in the nsclc cohort was objective response rate ( orr ) , dened as the proportion of patients with an objective response ( complete response [ cr ] or partial response [ pr ] ) conrmed on two consecutive occasions 4 or more weeks apart . 
 vemurafenib in nsclc with braf v600 mutation : the ve - basket study objectives included assessments of clinical benet rate ( dened as the overall proportion of patients with a cr , pr , or stable disease lasting 6 months ) , duration of response , progression - free survival ( pfs ) , overall survival ( os ) , and safety . 
efcacy data were analyzed separately for patients who had received no prior therapy and for those with prior therapies . statistical analysis this was a modied , two - stage simon design study . 
stage i was complete when seven patients with measurable disease were enrolled and had completed a minimum of 8 weeks of treatment , developed progressive disease , prematurely withdrew , or died . 
an additional six or 12 patients could be enrolled , to 13 or 19 patients , depending on the results for stage i ; if two , three , or four of the initial seven patients responded to treatment , an additional 12 patients could be enrolled in stage ii ; if ve or more of the initial seven patients responded to treatment , an additional six patients were recruited . 
recruitment into any cohort / indication could be further expanded up to 70 patients if a response rate was demonstrated in stage ii of that cohort , according to the stopping rules dened in the protocol or a clear clinical benet for patients was observed , as determined by the steering committee . 
for the nsclc cohort , with 50 treated patients , the study would have approximately 90% power for the lower bound of the twosided 95% ci to exclude 20% , given a true orr of 40% . the lower bound of the 95% ci was set at 20% because established therapy in the second and later lines had an orr of less than 20% when the study was designed . 
most patients had adenocarcinoma ( n = 58 ; 94% ) , three patients ( 4.8% ) had cns metastases , and most were former smokers ( n = 36 ; 58% )  . among previously treated patients , the median number of prior systemic regimens was two ( interquartile range [ iqr ] , 1 to 2 ) ; the most common prior chemotherapies were platinum agents ( 39 of 54 patients ; 72% ) , pemetrexed ( 33 of 54 patients ; 61% ) , and taxanes ( 22 of 54 patients ; 41% )  . all patients ( n = 62 ) previously untreated ( n = 8 ) previously treated ( n = 54 ) 65 ( 59 - 74 ) 73 ( 65 - 79 ) 64 ( 57 - 72 ) table 1 . 
overall , the investigator - determined orr was 37% ( 95% ci , 25% to 50% ) , and the clinical benet ( cr plus pr plus stable disease lasting 6 months ) rate was 48% ( 95% ci , 36% to 61% )  . 
the median relative dose intensity achieved was 78% ( iqr , 64% to 91% ) overall . all 62 patients experienced at least one any - cause ae ; grade 3 or 4 aes occurred in 48 patients ( 77% ) , and two patients had grade 5 aes ( 3% ; one patient with sepsis , one with a pulmonary embolism and respiratory failure ; both patients had been previously treated , and none of the events were considered to be related to vemurafenib )  . table 3 lists all - cause and grade 3 or greater aes occurring in 20% or more of patients . aes leading to treatment interruption occurred in 25 of 62 patients ( 40% )  . 
treatment outcomes in patients with nonsmall - cell lung cancer outcome all patients ( n = 62 ) previously untreated ( n = 8 ) previously treated ( n = 54 ) investigator - assessed best response , no . 
 vemurafenib in nsclc with braf v600 mutation : the ve - basket study - 100 previously untreated patients partial response stable disease progressive disease previously treated patients time to progression time to response died alive time ( months ) before treatment after 2 months of treatment fig 1 . 
 ( b ) waterfall plot of maximum percent decrease from baseline in the sum of diameters of target tumors on the basis of investigator assessment : best overall response in individual patients . ( c ) pretherapy and post - therapy 18f - uorodeoxyglucose positron emission tomography images of a chemotherapy - naive patient with braf v600e mutationpositive nsclc . 
at risk previously untreated ( n = 8 ) previously treated ( n = 54 ) overall ( n = 62 ) censored previously untreated ( n = 8 ) previously treated ( n = 54 ) overall ( n = 62 ) censored no . 
at risk 9 12 15 18 21 24 27 30 33 36 39 time ( months ) time ( months ) previously untreated previously treated 54 45 36 29 22 16 12 11 overall 62 52 42 34 26 18 14 12 previously untreated previously treated overall fig 2 . 
a total of 82 serious aes occurred in 39 patients ( 63% ) , the most common of which were scc of the skin ( nine patients ; 15% ) and keratoacanthoma ( nine patients ; 15% ) , which was dened as a serious ae . 
in total , 25 patients ( 40% ) had serious aes considered by the investigator to be caused by vemurafenib ( keratoacanthoma , n = 9 ; scc of the skin , n = 9 ; basal cell carcinoma , n = 1 ; bowen disease , n = 1 ; acute kidney injury , n = 4 ; pericarditis , n = 1 ; stomatitis , n = 1 ; pyrexia , n = 1 ; hypersensitivity , n = 1 ; sepsis , n = 1 ; and dehydration , n = 1 ) ; serious aes not considered to be related to vemurafenib included pneumonia ( n = 2 ) , bronchitis ( n = 2 ) , dyspnea ( n = 3 ) , pericardial effusion ( n = 1 ) , sepsis ( n = 3 ) , pulmonary embolism ( n = 2 ) , and lung infection ( n = 2 )  . targetable oncogenic drivers in nsclc with robust clinical validation include egfr mutations and alk and ros1 fusions , but identifying other targetable , clinically important subgroups of nsclc is a high priority . 
in this context , we found that patients with braf v600emutated nsclc treated with vemurafenib had an orr of 37% , with similar response rates in previously treated and untreated patients . median os was 15 months in the overall patient population , but had not been reached in the group of previously untreated patients after 12 months of follow - up . 
similarly , our previously untreated patients had a median pfs of 12.9 months , which was considerably longer than the 6.5 months observed in patients who had received prior therapies . 
the safety prole of vemurafenib in our group of patients with nsclc was similar to that seen in patients with melanoma.10 , 18 no new safety signals were observed in this population . 
we suggest that future studies should examine additional combinations in patients with braf mutation - positive nsclc . in conclusion , the results of the present cohort analysis suggest a role for braf inhibition in patients with nsclc with braf mutations . 
 vemurafenib in nsclc with braf v600 mutation : the ve - basket study affiliations 1university of texas md anderson cancer center , houston , tx 2centre franois baclesse , caen , france 3memorial sloan kettering cancer center , new york , ny 4institut gustave roussy , villejuif , france 5centre l eon b erard , lyon , france 6vall dhebron university hospital and vall dhebron institute of oncology , barcelona , spain 7university hospital essen , essen , germany 8aix - marseille universit e , marseille , france 9institut bergonie , bordeaux , france 10vanderbilt university , nashville , tn 11the royal marsden nhs foundation trust , london , united kingdom 12roswell park cancer institute , buffalo , ny 13massachusetts general hospital , boston , ma 14f . 
hyman administrative support : vivek subbiah provision of study materials or patients : vivek subbiah , gregory riely , antoine hollebecque , jean - yves blay , enriqueta felip , martin schuler , anthony gonalves , antonio italiano , igor puzanov , funda meric - bernstam collection and assembly of data : vivek subbiah , radj gervais , gregory riely , antoine hollebecque , jean - yves blay , martin schuler , antonio italiano , vicki keedy , igor puzanov , funda meric - bernstam , martina makrutzki , todd riehl , david m . 
hyman data analysis and interpretation : vivek subbiah , radj gervais , antoine hollebecque , jean - yves blay , enriqueta felip , martin schuler , anthony gonalves , antonio italiano , vicki keedy , ian chau , igor puzanov , noopur s . 
raje consulting or advisory role : amgen , celgene , takeda , novartis , bristolmyers squibb , merck , janssen oncology research funding : astrazeneca ( inst ) funda meric - bernstam honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group , mersana research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pzer , effector therapeutics , abbvie , boehringer ingelheim ( i ) , guardant health ( inst ) , daiichi sankyo , glaxosmithkline martina makrutzki employment : roche todd riehl employment : genentech stock and other ownership interests : genentech bethany pitcher employment : hoffmann - la roche jose baselga leadership : innity pharmaceuticals , varian medical systems , bristolmyers squibb , foghorn stock and other ownership interests : pmv pharma , juno therapeutics , grail , tango , venthera , northern biologics , apogen biotechnologies , aura biosciences consulting or advisory role : novartis patents , royalties , other intellectual property : combination therapy using pdk1 and pi3k inhibitors , use of phosphoinositide 3 - kinase inhibitors for treatment of vascular malformations , inhibition of kmt2d for the treatment of cancer travel , accommodations , expenses : roche , daiichi sankyo david m . 
n engl j med 361 : 947 - 957 , 2009 solomon bj , mok t , kim d - w , et al : first - line crizotinib versus chemotherapy in alk - positive lung cancer . 
n engl j med 371 : 1963 - 1971 , 2014 thomas a , liu sv , subramaniam ds , et al : rening the treatment of nsclc according to histological and molecular subtypes . 
medicine ( baltimore ) 96 : e6552 , 2017 paik pk , arcila me , fara m , et al : clinical characteristics of patients with lung adenocarcinomas harboring braf mutations . 
mcarthur ga , chapman pb , robert c , et al : safety and efcacy of vemurafenib in braf ( v600e ) and braf ( v600k ) mutation - positive melanoma ( brim - 3 ) : extended follow - up of a phase 3 , randomised , open - label study . 
long gv , stroyakovskiy d , gogas h , et al : dabrafenib and trametinib versus dabrafenib and placebo for val600 braf - mutant melanoma : a multicentre , double - blind , phase 3 randomised controlled trial . 
ascierto pa , mcarthur ga , dr eno b , et al : cobimetinib combined with vemurafenib in advanced braf ( v600 ) - mutant melanoma ( cobrim ) : updated efcacy results from a randomised , double - blind , phase 3 trial . 
planchard d , kim tm , mazieres j , et al : dabrafenib in patients with braf ( v600e ) - positive advanced non - small - cell lung cancer : a single - arm , multicentre , open - label , phase 2 trial . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated brafv600e - mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
planchard d , smit ef , groen hjm , et al : dabrafenib plus trametinib in patients with previously untreated brafv600e - mutant metastatic non - small - cell lung cancer : an open - label , phase 2 trial . 
 programmed death - ligand 1 expression in a large cohort of pediatric patients with solid tumor and association with clinicopathologic features in neuroblastoma purpose programmed death - ligand 1 ( pd - l1 ) expression represents a potential predictive biomarker of immune checkpoint blockade response . 
however , literature about the prevalence of pd - l1 expression in the pediatric cancer setting is discordant . methods pd - l1 expression was analyzed using immunohistochemistry in 500 pediatric tumors ( including neuroblastoma , sarcomas , and brain cancers )  . 
positive cases were further characterized , with cases with weak intensity pd - l1 staining reported as having low pd - l1 expression and cases with a moderate or strong intensity of staining considered to have high pd - l1 expression . results pd - l1positive staining was identified in 13% of cases , whereas high pd - l1 expression was found in 3% of cases . 
2017 by american society of clinical oncology introduction in recent years , the ability of tumor cells to exert an immunosuppressive action in their local microenvironment has been well described.1 escaping the host immune system occurs via multiple strategies , including loss of tumor antigens or reduced expression of major histocompatibility complex molecules , as well as via recruitment of immunosuppressive inflammatory cells or inadequate costimulation of t cells.2 as a consequence , the ability to evade host immunity has been recognized as one of the hallmarks of cancer.3 the expression of immune inhibitory ligands such as programmed death - ligand 1 ( pd - l1 ) is another strategy used by cancer cells to inhibit the immunologic response.4 pd - l1 is a trans - membrane surface glycoprotein overexpressed in many solid tumors , including carcinomas5 - 8 and melanoma.9 moreover , pd - l1 is one of the two known ligands for programmed death ( pd ) - 1 , a receptor expressed by immune system cells ( including activated t cells , regulatory t cells , b cells , natural killer cells , activated monocytes , and dendritic cells ) that negatively regulates their proliferation federica saletta ricardo e . 
antibody - mediated blockade of pd - l1 induced objective response rates in 6% to 17% and prolonged disease stabilization in 12% to 41% of patients with advanced cancers , including nonsmall - cell lung cancer , melanoma , and renal cell cancer.16 similarly , cumulative response rates for pd - 1 mab immunotherapy were achieved in 18% of patients with nonsmall - cell lung cancer , 28% of patients with melanoma , and 27% of patients with renal - cell cancer.13 despite these promising results achieved in adult cancers , the prevalence of pd - l1 expression in the pediatric setting and the potential use of mabs directed against pd - 1 have only started to be explored . 
the 53 analyzed cases included 18 neuroblastomas , eight extracranial germ - cell tumors , seven germinomas , seven hepatoblastomas , four medulloblatomas , four renal tumors , three rhabdomyosarcomas , and two atypical teratoid / rhabdoid tumors . 
in contrast , chowdhury et al20 observed 66 of 115 pd - l1positive samples ( 57% , ranging from 47% to 86% , depending on tumor type ) in a multitumor study including neuroblastoma , rhabdomyosarcoma , ewing sarcoma , and osteosarcoma . 
alveolar rhabdomyosarcoma showed the highest prevalence of pd - l1positive cases ( 12 of 14 [ 86% ] ) and patients with high - risk neuroblastoma were commonly pd - l1 positive ( 31 of 43 [ 72% ] )  . no previous study has reported associations between pd - l1 staining and the features of pediatric patients with cancer . 
here we present the clinicopathologic features of and survival analysis associated with pd - l1 expression in patients with neuroblastoma , with particular focus on the potential relationship between pd - l1 expression and the risk of cancer relapse . 
we identified a subcohort of patients with pd - l1positive staining and poor outcome , suggesting that pd - l1 may be a negative prognostic factor associated with an elevated risk of cancer recurrence . methods patient cohort the retrospective pediatric cohort consisted of 500 patients who underwent diagnostic biopsy or surgical resection at the childrens hospital at westmead , new south wales , australia . 
formalin - fixed paraffin - embedded hematoxylin and eosinstained tumor samples were reviewed by a histopathologist , and approved samples were used to construct tissue microarrays ( tmas ) using a manual tissue arrayer ( beecher mta1 , diagnostic technology , belrose , new south wales , australia ) and a 1 - mm unitma premade recipient block ( ub06 - 1 , diagnostic technology , belrose , new south wales , australia )  . 
 immunohistochemistry each tma was sectioned at 4 mm , and immunohistochemistry was performed using a bondrx automatic stainer ( leica biosystems , macquarie park , new south wales , australia )  . 
slide deparaffinization was performed with bond dewax solution , followed by alcohol dehydration . epitope retrieval was performed using hier2 buffer ( bond , ar9540 ) , and slides were incubated for 60 minutes at room temperature using a rabbit monoclonal antipd - l1 primary antibody ( e1l3n , no.13684 , cell signaling technology , genesearch , arundel , queensland , australia ) at 1 : 500 dilution in primary antibody diluent ( bond , ar9352 )  . 
staining was visualized using a polymer refine detection kit ( bond , ds9800 ) , and nuclei were counterstained with hematoxylin . tumors with > 1% of cells showing pd - l1 membrane staining ( or a combination of membrane and cytoplasmic staining ) of any intensity were considered pd - l1 positive . 
pd - l1 intensity was scored as weak , moderate , or strong by a histopathologist ( r.e.v. ) with specific expertise in pd - l1 staining assessment in patients with melanoma . 
similarly , fibrillary and stromal pd - l1 staining was also observed occasionally but was not scored positively because the significance of nonmembranous pd - l1 staining remains unclear . statistical analyses statistical analyses were undertaken using spss version 20.0 ( spss , chicago , il )  . 
bivariate relationships between pd - l1positive cases and patient features were analyzed with cross - tabulation , and significance was tested with fishers exact test . overall survival and relapse or progression - free survival were assessed using the kaplan - meier method , and significance was established using a log - rank ( mantel - cox ) test . 
statistical significance was set at p , .05 for two - sided tests . results prevalence of pd - l1positive pediatric patients with cancer as summarized in table 1 , in the overall cohort , 65 ( 13.0% ) of 500 cases were found to be pd - l1 positive . 
of these , 50 ( 76.9% ) of 65 showed weak pd - l1 intensity , whereas 15 ( 23.1% ) of 65 showed moderate to strong pd - l1 intensity . 
as such , in the overall cohort , only 15 ( 3.0% ) of 500 cases had moderate or strong pd - l1 positivity . neuroblastoma cases showed pd - l1 expression more commonly ( 48 of 254 [ 18.9% ] ) than did sarcomas or brain tumors . 
of the 48 positive cases , 40 ( 83.3% ) of 48 were weakly positive for pd - l1 , whereas eight ( 16.7% ) of 48 were moderately to strongly pd - l1 positive . 
overall , the distribution of weakly versus moderately or strongly positive pd - l1 staining in the neuroblastoma cohort was 15.7% ( 40 of 254 ) and 3.1% ( eight of 254 ) , respectively . 
in the brain tumor cohort , six ( 4.4% ) of 136 cases stained positively for pd - l1 , of which three ( 50.0% ) of six showed moderate to strong pd - l1 positivity . 
of the 96 sarcoma samples , seven ( 7.3% ) of 96 stained positively for pd - l1 , with only one of 96 cases ( an undifferentiated sarcoma ) being moderately positive . 
of the lymphoma cases , three ( 50% ) of six were pd - l1 positive ; two of these ( two of three [ 66.7% ] ) were moderately or strongly positive . 
one nasopharyngeal carcinoma showed moderate to strong pd - l1 staining . pd - l1 immunohistochemistry staining pattern observed although in this study only membranous pd - l1 staining was considered positive , together with the occasional combination of both membranous and cytoplasmic positive staining ( n = 5 ) , a range of other staining patterns was observed . 
an example of each pattern is presented in figure 1 ; they included membranous staining in the placenta as a positive control ( fig 1a ) , membranous tumor staining of weak , moderate , and strong intensity ( figs 1b , 1c , and 1d , respectively ) , as well as the combination of both membranous and cytoplasmic tumor pd - l1positive staining ( fig 1e )  . 
pd - l1 positive cytoplasmic ( fig 1f ) , fibrillary ( fig 1g ) , and schwannian stromal staining ( fig 1h ) were also observed , together with pd - l1positive macrophage ( fig 1i ) , but they were scored as negative . cytoplasmic pd - l1 staining was detected in 30 ( 11.8% ) of 254 neuroblastoma cases , ranging from weak ( n = 24 [ 80.0% ] ) to moderate or strong ( n = 6 [ 20.0% ] ) ; however , these cases were not considered pd - l1 positive . 
exclusive macrophage pd - l1 staining ( without pd - l1 positivity in tumor cells ) was detected in one ( 5.6% ) of 18 rhabdomyosarcomas , one ( 3.3% ) of 30 osteosarcomas , one ( 0.4% ) of 254 neuroblastomas , and one ( 2.6% ) of 38 lowgrade gliomas . 
the presence of macrophages was verified via hematoxylin and eosin staining observation . association with clinicopathologic features in pd - l1positive neuroblastoma cases information concerning a number of clinicopathologic features of the broader pediatric cohort was collated and tested ( using a two - sided fishers exact test ) for nonrandom associations with pd - l1 staining . 
interestingly , no differences in pd - l1 staining were found between biopsy specimens obtained before and after radiotherapy ( p = .702 ) , but a significant association between pd - l1 positivity and biopsy specimens obtained before chemotherapy was observed ( p = .044 ) , contrary to the suggestion of uehara et al.18 other clinicopathologic features that define patient prognosis in the neuroblastoma population at diagnosis include the mitosis - karyorrhexis index , shimada classification , mycn status , and overall patient risk ( table 2 )  . 
next , we sought to analyze whether pd - l1positive neuroblastoma cases were associated with cancer recurrence or progression ; however , no significant ( p = .939 ) association was observed ( fig 2b )  . 
although we did not find an association ( p = .508 ) between moderate to strong pd - l1 staining and overall survival ( fig 2c ) , the association with poorer relapse - free survival in this subcohort was significant ( p = .002 , fig 2d )  . 
programmed death - ligand 1 ( pd - l1 ) immunohistochemistry staining patterns . representative images of pd - l1 staining ( in brown ) and counterstained nuclei ( in blue )  . 
black arrows highlight examples of ( a ) pd - l1 staining in placenta used as positive control tissue ; pd - l1 membranous staining of ( b ) weak , ( c ) moderate , and ( d ) strong intensity in lymphoma ; and ( e ) pd - l1positive staining in both membrane and cytoplasm in neuroblastoma . 
 ( f ) exclusive cytoplasmic pdl1 staining and ( g ) pdl1positive schwannian stroma in neuroblastoma were considered negative . ( h ) pd - l1positive fibrillary staining in medulloblastoma and ( i ) pd - l1positive macrophages in osteosarcoma were also scored as negative . 
there were no differences in overall survival ( p = .298 ) or relapse - free survival ( p = .507 ) according to pd - l1 positivity of any intensity ( figs 3a and 3b )  . 
when restricting the analysis to the lowand intermediate - risk neuroblastoma cohort with moderate to strong pd - l1 staining , we found no association ( p = .524 ) with overall survival ( fig 3c ) but significantly ( p , .001 ) poorer relapse - free survival ( fig 3d )  . discussion since discovering that pd - 1 / pd - l1 binding promotes cancer tolerance by blocking the t - cell antigen receptor - induced stop signal , 22 substantial research effort has been aimed at targeting this interaction . 
a list of the pd - l1 antibodies and the staining and scoring methods used by other research groups is summarized in table 3 , which highlights the need for standardized immunohistochemistry methodology and a standardized scoring system for pd - l1positive cases . 
 ( a ) and ( b ) show overall survival and relapsefree survival ( in months ) in association with pd - l1 positivity ( of any intensity ) , respectively . 
 ( c ) and ( d ) show overall survival and relapse - free survival ( in months ) in association with moderate or strong pd - l1 staining intensity , respectively . 
for example , in a glioblastoma study , there was no association between fibrillary pd - l1 detection and overall survival in patients with glioblastoma.31 in our cohort , pd - l1 fibrillary staining was observed in only one of 38 medulloblastoma biopsy specimens , whereas pd - l1 schwannian stromal staining was detected in twelve of 254 patients with neuroblastoma . 
associations between programmed death - ligand 1 ( pd - l1 ) status and survival of patients with neuroblastoma ( nb ) with low and intermediate risk . kaplan - meier plots compare patient survival ( in months ) in the lowand intermediate - risk nb cohort . 
 ( a ) and ( b ) show overall survival and relapsefree survival ( in months ) in association with pd - l1 positivity ( of any intensity ) , respectively . 
 ( c ) and ( d ) show overall survival and relapse - free survival ( in months ) in association with moderate or strong pd - l1 staining intensity , respectively . 
previous reports have shown a discordant association between myc oncogene status and pd - l1 expression . in fact , casey et al36 stated that myc regulates the antitumor immune response through cd47 and pd - l1 in melanoma and nonsmall - cell lung cancer cell lines , whereas dondero et al37 showed that pd - l1 expression in neuroblastoma was interferon - gamma dependent and mycn independent . 
because strong pdl1 staining has been shown to correlate with an elevated mutation burden , 26 we can speculate that these cases may share an underlying dna repair deficit that results in an increased presence of neoantigens and particularly high pd - l1 expression . 
more studies are necessary to verify this hypothesis and to correlate mutation burden in children with stronger pd - l1 staining and a higher likelihood of cancer relapse despite favorable clinical features . pd - l1 may represent a novel predictive marker of cancer recurrence that could be used to identify the proportion of children who may benefit from pd - 1 / pd - l1 mab therapy . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . geoffrey mccowage research funding : novartis ( inst ) , merck ( inst ) acknowledgment we thank the patients and families who agreed to donate samples to the childrens hospital at westmead tumour bank . 
we also thank michael krivanek , md , of childrens hospital at westmead for his help with the histologic review of patient samples before tissue coring for tma construction , and jason madore of royal prince alfred hospital for his help in optimizing the immunohistochemistry protocol and staining interpretation . federica saletta no relationship to disclose ricardo e . 
blank c , gajewski tf , mackensen a : interaction of pd - l1 on tumor cells with pd - 1 on tumor - specific t cells as a mechanism of immune evasion : implications for tumor immunotherapy . 
karim r , jordanova es , piersma sj , et al : tumor - expressed b7 - h1 and b7 - dc in relation to pd - 1 + t - cell infiltration and survival of patients with cervical carcinoma . 
thompson rh , kuntz sm , leibovich bc , et al : tumor b7 - h1 is associated with poor prognosis in renal cell carcinoma patients with long - term follow - up . 
madore j , vilain re , menzies am , et al : pd - l1 expression in melanoma shows marked heterogeneity within and between patients : implications for anti - pd - 1 / pd - l1 clinical trials . 
freeman gj , long aj , iwai y , et al : engagement of the pd - 1 immunoinhibitory receptor by a novel b7 family member leads to negative regulation of lymphocyte activation . 
topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of anti - pd - 1 antibody in cancer . n engl j med 366 : 2443 - 2454 , 2012 14 . 
chowdhury f , dunn s , mitchell s , et al : pd - l1 and cd8 + pd1 + lymphocytes exist as targets in the pediatric tumor microenvironment for immunomodulatory therapy . 
fife bt , pauken ke , eagar tn , et al : interactions between pd - 1 and pd - l1 promote tolerance by blocking the tcr - induced stop signal . 
saletta f , wadham c , ziegler ds , et al : molecular profiling of childhood cancer : biomarkers and novel therapies . 703 - 718 , 2013 bba clin 1 : 59 - 77 , 2014 26 . 
madore j , strbenac d , vilain r , et al : pd - l1 negative status is associated with lower mutation burden , differential expression of immune - related genes , and worse survival in stage iii melanoma . 
mu cy , huang ja , chen y , et al : high expression of pd - l1 in lung cancer may contribute to poor prognosis and tumor cells immune escape through suppressing tumor infiltrating dendritic cells maturation . 
yang cy , lin mw , chang yl , et al : programmed cell death - ligand 1 expression in surgically resected stage i pulmonary adenocarcinoma and its correlation with driver mutations and clinical outcomes . 
preusser m , berghoff as , wick w , et al : clinical neuropathology mini - review 6 - 2015 : pd - l1 : emerging biomarker in glioblastoma ? clin neuropathol 34 : 313 - 321 , 2015 32 . 
taube jm , klein a , brahmer jr , et al : association of pd - 1 , pd - 1 ligands , and other features of the tumor immune microenvironment with response to anti - pd - 1 therapy . 
 exploitation of precision medicine trials data : examples of long responders from the shiva01 trial clmence basse claire morel cline callens galle pierron vincent servois anne vincentsalomon aude jobard marie alt francesco ricci delphine loirat marie - paule sablin marie bretagne mathilde saintghislain sgolne hescot anthony gonalves olivier tredan coraline dubot cline gavoille jean - pierre delord mario campone nicolas isambert lisa belin ivan bieche maud kamal christophe le tourneau author affiliations and support information ( if applicable ) appear at the end of this article . clinical trials information : nct01771458 . licensed under the creative commons attribution 4.0 license ( continued ) purpose precision medicine trials constitute a precious source of molecular data with prospective clinical annotations allowing the exploration of patients subpopulations according to specific clinical or biological questions . 
using the shiva01the first randomized trial comparing molecularly targeted therapy on the basis of tumor molecular profiling versus conventional chemotherapy in metastatic cancer patients who failed standard of care therapyannotated database , we report cases of patients treated in the trial with targeted therapy who experienced an objective response or prolonged disease stabilization in light of patients molecular alterations . patients and methods we selected all patients included in shiva01 treated with a molecularly targeted agent ( mta ) who experienced an objective response or disease stabilization that lasted longer than 6 months according to response evaluation criteria in solid tumors version 1.1. results among the 170 patients who received mtas in the shiva01 trial , 15 patients ( 9% ) experienced an objective response ( n = 3 ) or disease stabilization that lasted longer than 6 months ( n = 12 )  . 
the remaining four patients were treated with tamoxifen , erlotinib , imatinib , and vemurafenib on the basis of progesterone receptor expression , egfr amplification , kit mutation , and braf mutation , respectively . 
2018 by american society of clinical oncology introduction some molecularly targeted agents ( mtas ) have been demonstrated to dramatically improve the outcome of patients whose tumors harbor a matching molecular alteration.1 we know from the cancer genome atlas data that most of the druggable molecular alterations , including gene mutations and gene copy number alterations , exist across various tumor types , although their prevalence and functional significance may vary.2 on the basis of the latter observation , a key question has emerged : should patients with cancer be treated according to their molecular profile in a histology - agnostic way instead of by tumor type and histology , at least in the metastatic setting ? whereas nonrandomized and retrospective studies have suggested the histology - agnostic approach might be valid , 3 - 5 the shiva01 trialthe first randomized precision medicine trialdid not demonstrate a significant difference in progression - free survival ( pfs ) between matched targeted therapy and conventional treatment in patients who eventually experienced progression after standard - ofcare therapy.6 some patients who were treated in the shiva01 trial , however , seemed to benefit from targeted therapy . 
all patients who were enrolled in shiva01 previously received the standard treatment approved for their indication , including mtas , and had an eastern cooperative oncology group performance status of 0 or 1.8 within the shiva01 trial , mtas were administered according to a prespecified treatment algorithm and each mta was administered according to a matched molecular biomarker ( data supplement )  . 
techniques used included next generation sequencing ( ampliseq cancer panel on an ion torrent / pgm system ; thermo fisher scientific , waltham , ma ) for detecting mutations , cytoscan hd ( affymetrix , santa clara , ca ) for gene copy number alterations , and immunohistochemistry for hormone receptor protein expression assessment . 
we also recorded the total number of patients in shiva01 with the same tumor type treated with the same drug on the basis of the same molecular alteration . we assessed relationships between genomic alteration and clinical response using fishers exact test . 
of previous lines of treatment 24 - 71 gender male female age , years ecog performance status tumor type breast cancer cervical cancer colorectal cancer hepatocellular carcinoma nonsmall - cell lung cancer bladder carcinoma germline tumor ependymoma 6 ( 40 ) 9 ( 60 ) 2 ( 13 ) 7 ( 47 ) 3 ( 20 ) 3 ( 20 ) 4 ( 27 ) 11 ( 73 ) 4 ( 27 ) 3 ( 20 ) 1 ( 6.6 ) 1 ( 6.6 ) 1 ( 6.6 ) 1 ( 6.6 ) 1 ( 6.6 ) 1 ( 6.6 ) 1 ( 6.6 ) 1 ( 6.6 ) head and neck squamous cell carcinoma gastroesophageal carcinoma abbreviation : ecog , eastern cooperative oncology group . longer than 6 months , seven patients ( 47% ) had a molecular alteration that involved the hormone receptor pathway ( table 2 )  . 
six patients who were treated with abiraterone had androgen receptor ( ar ) protein expression that ranged from 40% to 100% , including three patients with breast cancer , one patient with hepatocellular carcinoma , and one patient with bladder cancer ( table 2 )  . 
the remaining patient with gastroesophageal cancer and a 30% progesterone receptor expression was treated with tamoxifen . five patients ( 33% ) who were treated with everolimus had a molecular alteration involving the phosphatidylinositol 3 - kinase ( pi3k ) / akt / mammalian target of rapamycin ( mtor ) pathway . 
among these patients , three patients cervical cancer , head and neck , and germline cancerhad a phosphatase and tensin homolog ( pten ) heterozygous deletion associated with a loss of protein expression . 
the two remaining patients consisted of one patient with cervical cancer with a pik3ca mutation ( glu542lys ) and another with breast cancer with both pten loss and pik3ca mutation ( glu545lys )  . 
proportion of patients treated with molecularly targeted therapy in shiva01 who achieved an objective response or disease stabilization lasting longer than 6 months molecularly targeted agent tumor type abiraterone breast cancer no . 
of patients in shiva01 with the same tumor type treated with the same drug bladder cancer ependymoma breast cancer cervical cancer germline tumor hnscc cervical cancer colorectal cancer gastroesophageal cancer nsclc everolimus erlotinib vemurafenib tamoxifen imatinib total abbreviations : hcc , hepatocellular carcinoma ; hnscc , head and neck squamous cell carcinoma ; nsclc , nonsmall - cell lung cancer . than a single patient with the same tumor type and were treated with the same mta matching an alteration in a specific signaling pathway . 
in total , 22 patients with breast cancer were treated with abiraterone , 12 patients with breast cancer with everolimus , and 10 patients with cervical cancer with everolimus ( table 3 )  . 
 within these three larger cohorts , the proportion of patients with an objective response or disease stabilization that lasted longer than 6 months varied from 8% to 20% ( table 3 )  . 
 taken together , 15 ( 28% ) of the 53 patients in these cohorts achieved an objective response or disease stabilization that lasted longer than 6 months ( table 3 )  . focus on patients treated with everolimus . 
theonly patient with breast cancer treated with everolimus who experienced a complete response had a pik3ca mutation ( glu545lys ) , as well as a kras mutation ( ala146thr ) , associated with heterozygous deletions in the atm , brca2 , cdh1 , pten , rb1 , smad4 , and tp53 genes ( table 2 and data supplement )  . 
of the 11 nonresponder patients with breast cancer , seven received everolimus on the basis of a pik3ca mutation ( 3 his1047arg , 2 glu545lys , and 2 glu542lys ) and four received everolimus on the basis of pten inactivation . 
one patient had a kras mutation ( gly12val ) , and five patients had a tp53 mutation ( data supplement )  . the two patients with cervical cancer treated with everolimus who achieved disease stabilization that lasted longer than 6 months had either a pik3ca mutation ( glu542lys ) or a pten heterozygous deletion with a loss of protein expression ( table 2 and data supplement )  . 
among the eight nonresponder patients with cervical cancer , four received everolimus on the basis of pik3ca mutation ( glu545lys ) , two on the basis of pten inactivation , and two on the basis of akt1 mutation ( glu17lys )  . 
in total , among the three patients who achieved an objective response or disease stabilization that lasted longer than 6 months , all had a double alteration affecting the pi3k / akt / mtor pathway . 
none of the four patients who experienced an objective response or disease stabilization that lasted longer than 6 months and for whom a complete molecular profile was available had a mutation in the tp53 gene compared with 10 ( 31% ) of 32 nonresponders with a complete molecular profile ( p = .47 ; data supplement )  . impact of molecular alteration burden in resistance to treatment . 
a median of five molecular alterations ( range , three to eight ) were detected in three patients treated with everolimus who experienced an objective response or disease stabilization that lasted longer than 6 months compared with a median of six alterations ( range , two to 21 ) in 19 nonresponder patients . 
a median of three molecular alterations ( range , one to eight ) were found in three patients treated with abiraterone who experienced an objective response or disease stabilization that lasted longer than 6 months compared with a median of five alterations ( range , one to 17 ) in 19 nonresponder patients . 
 the total number of molecular alterations was not significantly associated with resistance to treatment ( p = .41 ; data supplement )  . discussion using the shiva01 trials annotated database , we here report 15 patients ( 9% ) who experienced an objective response or prolonged disease stabilization among the 170 patients with any kind of cancer treated with an mta outside its indication in the shiva01 trial . 
the total number of molecular alterations was not significantly associated with resistance to treatment , which suggests that other mechanisms that require additional investigation are involved . patients experiencing an objective response or a disease stabilization that lasted longer than 6 months were less heavily pretreated than the entire patient population that was included in the shiva01 trial.6 this result is in agreement with several reports in the literature that suggest that the sooner mtas are administered in the course of the disease , the higher the efficacy.1 , 10 in the two largest cohorts in the shiva01 trial treated with everolimus or abiraterone , patients who experienced an objective response or disease stabilization that lasted longer than 6 months had fewer molecular alterations than nonresponder patients . 
efficacy of mtas administered in a manner similar to that of shiva01 correlated with the matching score.11 , 12 in agreement with a recent report , three of 22 patients with breast cancer expressing ar and treated with abiraterone experienced disease stabilization that lasted longer than 6 months.13 one patient with hepatocellular carcinoma , one with bladder carcinoma , and one with ependymoma treated with abiraterone in shiva01 experienced disease stabilization that lasted longer than 6 months ; however , no evidence of efficacy of antiandrogens in these cancer types has been reported in the literature.14 - 17 one patient with gastroesophageal carcinoma treated with tamoxifen on the basis of progesterone receptor expression had an 18 - month disease stabilization in the shiva01 trial . 
antitumor activity of tamoxifen in hormone receptors expressing gastric cancer cells has been reported.14 to date , no clinical trials have been reported , to our knowledge , evaluating this strategy in the clinic . all three patients treated with everolimus who achieved an objective response or disease stabilization that lasted longer than 6 months had a double alteration affecting the pi3k / akt / mtor pathway , whereas less than one half of nonresponder patients with breast and cervical cancer had a double alteration involving that pathway . 
thirty - five percent of patients with breast cancer with an alteration in the pi3k / akt / mtor pathway who were treated with various therapies that inhibited the pi3k / akt / mtor pathway in the safir01 study had an objective response or pfs that lasted longer than 16 weeks.16 the difference in terms of efficacy observed in safir01 might be related to the 16 - week threshold used for prolonged disease stabilizationinstead of the 6 months in our studyand that various drugs used sometimes in combination , including direct pi3k inhibitors in safir01 . 
in a phase ii trial that evaluated everolimus in unselected patients with refractory testicular germcell tumors , no objective response was observed with a pfs rate at 3 months of 40%.18 finally , three patients in shiva01 seemed to benefit from mtas that targeted epidermal growth factor receptor , kit , and braf mutations , which are clinically validated targets in other tumor types.19 - 22 of interest , the patient with braf v600emutated colorectal cancer experienced an unusual response to vemurafenib . 
partial responses to vemurafenib in patients with braf v600emutated colorectal cancer have previously been reported in the literature.23 the absence of tp53 mutations and pi3k pathway alterations in these patients may explain the partial response to vemurafenib , 24 although this remains speculative . in conclusion , the design of the shiva01 trial has several limitations . 
second , the treatment algorithm was unidimensional and did not account for resistance mechanisms.9 third , heavily pretreated patients were included in the trial , which reduced the likelihood that mtas might be effective . 
despite these caveats , shiva01 allowed for the integration of clinically annotated molecular data that were used to analyze patients with unusual responses to mtas.6 the exploitation of clinically annotated molecular data from precision medicine trials is clearly useful to pinpoint potential biomarkers of interest in assessing sensitivity or resistance to mtas . 
whereas an objective response with a single - agent mta clearly indicates treatment efficacy , using prolonged disease stabilization as a criterion is questionable.25 the example of the long - responder patients analysis , although bearing the above limitations , highlights the precious information that could be inferred from precision medicine trials data analyses . 
 many lessons could definitely be learned using this approach : the possibility to focus on patients subpopulation with specific clinical or molecular questions within the same prospective study ( in our case , patients experiencing an objective response or prolonged disease stabilization following treatment within the shiva01 trial ) ; the accessibility of centralized molecular data obtained using the same techniques and bioinformatics pipelines and thus avoiding multiple sites biases ; the identification of potential biomarkers of interest depending on the question asked ( in our case , global number of molecular alterations , several alterations in the same pathways , or tp53 mutations ) that required additional validation in independent cohorts ; and the importance of sharing data with other precision medicine clinical trials to enlarge specific subpopulation or to validate results . 
tumor mutational burden and microsatellite instability have been suggested as potential biomarkers of efficacy for immune checkpoint inhibitors.26 - 28 it remains to be determined how the incorporation of immunotherapy in shiva01 would have affected the results . 
anr - 10 - eqpx - 03 from the agence nationale de le recherche ( investissements davenir ) and site de recherche intgr contre le cancer inca - dgos - 4654 . 
slamon dj , leyland - jones b , shak s , et al : use of chemotherapy plus a monoclonal antibody against her2 for metastatic breast cancer that overexpresses her2 . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular profiling of patients tumors to find potential targets and select treatments for their refractory cancers . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
massard c , michiels s , fert c , et al : high - throughput genomics and clinical outcome in hardto - treat advanced cancers : results of the moscato 01 trial . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
belin l , kamal m , mauborgne c , et al : randomized phase ii trial comparing molecularly targeted therapy based on tumor molecular profiling versus conventional therapy in patients with refractory cancer : cross - over analysis from the shiva trial . 
migliardi g , sassi f , torti d , et al : inhibition of mek and pi3k / mtor suppresses tumor growth but does not cause tumor regression in patient - derived xenografts of ras - mutant colorectal carcinomas . 
bonnefoi h , grellety t , tredan o , et al : a phase ii trial of abiraterone acetate plus prednisone in patients with triple - negative androgen receptor positive locally advanced or metastatic breast cancer ( ucbg 12 - 1 )  . 
kameda c , nakamura m , tanaka h , et al : oestrogen receptor - alpha contributes to the regulation of the hedgehog signalling pathway in eralpha - positive gastric cancer . 
geiger jl , bauman je , gibson mk , et al : phase ii trial of everolimus in patients with previously treated recurrent or metastatic head and neck squamous cell carcinoma . 
andr f , bachelot t , commo f , et al : comparative genomic hybridisation array and dna sequencing to direct treatment of metastatic breast cancer : a multicentre , prospective trial ( safir01 / unicancer )  . 
andr f , hurvitz s , fasolo a , et al : molecular alterations and everolimus efficacy in human epidermal growth factor receptor 2 - overexpressing metastatic breast cancers : combined exploratory biomarker analysis from bolero - 1 and bolero - 3 . 
schilder rj , sill mw , lee yc , et al : a phase ii trial of erlotinib in recurrent squamous cell carcinoma of the cervix : a gynecologic oncology group study . 
santin ad , sill mw , mcmeekin ds , et al : phase ii trial of cetuximab in the treatment of persistent or recurrent squamous or non - squamous cell carcinoma of the cervix : a gynecologic oncology group study . 
goncalves a , fabbro m , lhomm c , et al : a phase ii trial to evaluate gefitinib as secondor third - line treatment in patients with recurring locoregionally advanced or metastatic cervical cancer . 
lu hy , zhang g , cheng qy , et al : expression and mutation of the c - kit gene and correlation with prognosis of small - cell lung cancer . 
mao m , tian f , mariadason jm , et al : resistance to braf inhibition in braf - mutant colon cancer can be overcome with pi3k inhibition or demethylating agents . 
le tourneau c , paoletti x , coquan e , et al : critical evaluation of disease stabilization as a measure of activity of systemic therapy : lessons from trials with arms in which patients do not receive active treatment . 
 mendel goldnger ramaswamy govindan jhanelle gray stacy gray samantha greenberg malachi grifth * roman groisberg * torsten haferlach michael hall * anis hamid * heather hampel * fei han sigurdis haraldsdottir * derrick haslem * eric haura masanori hayashi brian henick * , * * daniel herchenhorn * kenneth hess j . 
kevin hicks kim hirsheld brian hobbs howard hochster * daanish hoda * ahmed hosny david hsu wenhui huang yi huang * hatim husain maha hussain * david hyman * alexia iasonos * meredith irwin * steven isakoff katherine janeway * yelena janjigian lingyun ji xuemei ji * * yuchao jiang markus joerger steven joffe * thomas kaley mohammed kashanisabet steve katz kevin kim david kirsch kedar kirtane eric klein samuel klempner * todd knepper wendy kohlmann * jill kolesar * ian krop * priti kumari shivaani kummar ava kwong andrea laghi * jacky wai - kei lam angela lamarca jean - michel lavoie rachel layperson * christophe le tourneau * amy leblanc j . 
jack lee * jochen lennerz * antonio lerario benjamin levy mark lewis * jessica lin * steven lipkin jingyi liu * minetta liu * stephen liu * christine lovly ying lu * luke maese * david malkin diana mandelker sharon manne aaron manseld veronica mariotti thomas martin carlotta masciocchi joaquin mateo * shigeyuki matsui * joan maurel * shannon mccall jeannine mccune * rose mcgee * funda meric - bernstam everett meyer * ropa mhlanga * * luca mologni clara montagut * lucas moreno * daniel morgenstern * motomi mori * kent mouw anwesha nag katherine nathanson daniel nava rodrigues stewart neill kim nichols donna niedzwiecki nicola normanno * david norris paolo nuciforo jennifer oberg * stephen oh * coral omene stephen opat eileen oreilly * piet ost geoffrey oxnard * sukhmani padda tuya pal jose palacios phillip palmbos wei pan nickolas papadopoulos * soo park jai patel shiven patel * cloud paweletz andrew pearson raquel perez - lopez * thomas permutt * emanuel petricoin * gina petroni * david piccioni gaelle pierron filippo pietrantonio zoa piotrowska sharon plon eric polley mei - yin polley * erqi pollom mark pomerantz steven powell * colin pritchard * kanwal raghav * nitya raj w . 
 o genomic profiling of t - cell neoplasms reveals frequent jak1 and jak3 mutations with clonal evasion from targeted therapies purpose the promise of precision oncology is that identification of genomic alterations will direct the rational use of molecularly targeted therapy . 
in this study , we tested the feasibility of targeted next - generation sequencing in profiles of diverse t - cell neoplasms and focused on the therapeutic utility of targeting activated jak1 and jak3 in an index case . patients and methods using foundation one and foundation one heme assays , we performed genomic profiling on 91 consecutive t - cell neoplasms for alterations in 405 genes . 
the samples were sequenced to high uniform coverage with an illumina hiseq and averaged a coverage depth of greater than 500 for dna and more than 8m total pairs for rna . 
t - pll cells were analyzed by rna - seq , in vitro drug testing , mass cytometry , and phospho - flow . results one third of the samples had genomic aberrations in the jak - stat pathway , most often composed of jak1 and jak3 gain - of - function mutations . 
adult patients with precursor neoplasms , such as acute t - cell lymphoblastic leukemia ( t - all ) , or with mature neoplasms , such as t - cell non - hodgkin lymphoma ( t - nhl ) , have a 5 - year survival rate of 20% to 30% even after intensive multiagent chemotherapy.1 - 6 there are rare exceptions to these dismal outcomes , such as children and adolescents who have t - all or anaplastic large - cell lymphoma ( alcl ) with unique gene rearrangements ( ie , alk positivity or dusp22 positivity ) in whom 5 - year survival rates are greater than 70% to 80% with similar chemotherapy regimens.5 , 7 , 8 however , relapsed disease is challenging to cure . 
clearly , novel therapeutic approaches are needed , and the development of commercially available next - generation sequencing has raised the possibility that genomically directed therapy may be applied to t - cell leukemias and lymphomas . 
genomic profiling has been performed on several histopathologic subtypes of t - cell leukemias and lymphomas to better characterize the molecular genetics.9 - 13 interestingly , recent genomic profiling has discovered frequent allison greenplate kai wang rati m . 
 aberrations within the janus kinase ( jak ) signal transducer and activator of transcription ( stat ) pathway in both precursor ( t - all ) and mature ( t - nhl ) t - cell neoplasms , which suggests that jak kinase inhibition may be important therapeutically.14 jaks are encoded by four paralogous genes , jak1 , jak2 , jak3 , and tyk2 . 
jak1 mutations have been found in 10% of childhood t - alls.15 our laboratory and others have found jak3 mutations in cutaneous t - cell lymphoma ( ctcl ) , adult t - cell leukemia / lymphoma ( atll ) , t - cell prolymphocytic leukemia ( t - pll ) , and natural killer / t - cell lymphoma ( nktl ) .16 - 20 analyses of human leukemia lines and mouse models show that jak mutations typically are activating and cause constitutive signal transduction , which may be blocked by tyrosine kinase inhibitors . 
ruxolitinb is approved for use in myeloproliferative neoplasms , and tofacitinib is approved for rheumatoid arthritis.21 , 22 in this study , we deployed a commercially available hybrid - capture / next - generation sequencing platform to characterize major recurrent oncogene and tumor suppressor aberrations in 91 t - cell neoplasms . 
this targeted approach found that 33% of samples had jak - stat abnormalities , which included missense mutations in jak1 and jak3 , rearrangements in jak2 and jak3 , and missense mutations and amplifications of stat3 and stat5 . 
we analyzed an index case of t - pll , a deadly mature t - cell neoplasm with both jak1 and jak3 gain - of - function missense mutations.23 this patient with t - pll had experienced progression during multiple lines of chemotherapy but experienced disease response with ruxolitinib , a jak1 / 2 inhibitor . 
adaptor ligated libraries were created from dna and cdna as described.24 libraries were sequenced on illumina hiseq2500 ( illumina , san diego , ca ) to > 500 coverage depth for dna and > 8m total pairs for rna . 
dna and rna sequence data were processed with a customized analysis pipeline designed to accurately detect multiple classes of genomic alterationsspecifically , base substitutions , indels , focal gene amplifications , homozygous gene deletions , gene fusions , and genomic rearrangements ( data supplement ) .24 gene expression the rna sequencing workf low has been described previously . 
a description also is in the data supplement.26 phosphatase enzyme assay and inhibitor studies frozen preand post - treatment t - pll cells and jurkat cells were lysed in hypotonic buffer and prepared with cytosol , as described.27 ruxolitinib and tofacitinib were purchased from selleck chemicals ( houston , tx ) , and working solutions were prepared in dimethyl sufoxide ( dmso )  . 
cell viability was quantified with a cyquant assay ( invitrogen , carlsbad , ca ) , as described.17 , 27 statistical analyses were performed with graphpad prism ( la jolla , ca )  . results genomic profiling of t - cell leukemias and lymphomas we analyzed 91 occurrences of diverse t - cell leukemias and lymphomas for alterations in 405 cancer - causing genes by comprehensive hybrid capture of genomic dna followed by next generation sequencing ( data supplement )  . 
the cohort showed a marked male predominance for both immature and mature t - cell neoplasms ( 4 : 1 and 1.75 : 1 , respectively ; data supplement ) consistent with the epidemiology of these cancers.28 , 29 samples were sequenced at a mean exon depth of 489 by illumina hiseq . 
stat3 mutations ( 0% v 18% , p = .032 ) were more common in mature t - cell neoplasms ( table 1 ) ; 31.8% ( 29 of 91 samples ) had alterations in the jak - stat pathway . 
 jak3 , which involved 13% ( 12 of 91 samples ) of samples , was the most commonly mutated kinase , followed by jak1 , which was mutated in 7.7% ( seven of 91 samples )  . 
jak3 mutations were present with a similar frequency in t - all and in mature t - cell neoplasms ( fisher 's exact test , p = .19 ) but were highly frequent in certain mature t - cell neoplasms , such as t - pll ( five [ 71% ] of seven samples )  . 
interestingly , all five occurrences of t - pll had the m511i jak3 mutation ; all of the jak3 and jak1 mutations were in the catalogue of somatic mutations in cancer ( cosmic ; ac.uk / cosmic ) database , frequently within the pseudokinase domains of the proteins ( fig 2 ) .30 jak3 missense mutations have been identified previously in ctcl and atl.16 focal stat3 , stat5a , and stat5b amplifications were identified in two occurrences ( n = 1 each in ctcl and alcl ) , in addition to missense mutations within the sh2 domains of stat3 and stat5b , such as stat3 d661y / v in t - lgl ( fig 2 )  . 
jak1 and jak3 mutations were observed in the same tumor in five occurrences , but concordant mutations in the same cell could not be confirmed ( data supplement )  . 
 jak3 mutations were concordant with mutations in tp53 in four samples ; notch1 mutations , in four samples ; and cdkn2a deletions , in three samples ( data supplement )  . exceptional response of a jak1 - mutant t - pll we evaluated a 62 - year - old woman in our clinic with relapsed t - pll . 
she presented with constitutional symptoms , splenomegaly , and leukemic blood counts that had increased to greater than 150 , 000 / l and progressed through alemtuzumab ; cyclophosphamide , doxorubicin , vincristine , and prednisone ( chop ) ; romidepsin ; and pralatrexate . 
the t - pll cells were cd2 + cd3 + cd4 + cd7 + cd8cd56cd57 ( fig 3a ) , had clonal t - cell receptor rearrangement ( data not shown ) , and had infiltration of bone marrow ( figs 3b through 3e )  . 
 a cdkn2a / b substitution / indel gene amplification gene homozygous deletion truncation gene fusion / rearrangement tet2 jak3 tp53 stat3 jak1 stat5b stat5a cdkn2a / b tet2 notch1 jak3 tp53 stat3 nras dnmt3a jak1 rhoa mll2 arid1a stat5b fbxw7 abl1 traf3 stat5a stag2 runx1 pik3r1 cd36 tnfaip3 smarcb1 smarca4 setd2 pten pik3ca phf6 pask nup214 ncor1 kras jak2 idh2 hist1h1d etv6 crebbp1 ciita cdkn1b ccnd3 card11 brca2 bcor asxl1 genetic aberration t - all cdkn2a / b tet2 notch1 jak3 tp53 stat3 nras dnmt3a jak1 rhoa mll2 arid1a stat5b fbxw7 abl1 traf3 stat5a stag2 runx1 pik3r1 cd36 tnfaip3 smarcb1 smarca4 setd2 pten pik3ca phf6 pask nup214 ncor1 kras jak2 idh2 hist1h1d etv6 crebbp1 ciita cdkn1b ccnd3 card11 brca2 bcor asxl1 t - cell neoplasm subtype fig 1 . 
 , alpha helical domain , a dna binding domain ; ferm , the conserved domain named for its founding members ( band 4.2 , ezrin , radixin , and moesin ) ; jh1 , jak homology domain 1 , the functional kinase domain ; jh2 , jak homology domain 2 ( also known as the pseudokinase domain ) ; sh2 , src homology domain 2 ; stat - int , stat interaction domain . jak3 ferm 1000 1125 jak1 ferm 1000 1155 stat3 stat - int ( cid : 68 ) dna - binding 11 1213 14 15 18 19 22 23 stat5b stat - int dna - binding 17 18 ( cid : 68 ) and 78% , respectively , which suggests loss of heterozygosity ( data supplement )  . 
both jak1 and jak3 mutations had been described in hematologic malignancies and have proven to be oncogenic in various assays.20 , 30 - 32 the clonal jak1 mutation could be targeted by ruxolitinib , a kinase inhibitor with activity against jak1 / 2.21 the patient was agreeable to this off - label therapy and received 20 mg twice daily ; her peripheral count ( 90% t - pll ) declined from 142 , 000 / l to 85 , 000 / l within 5 days . 
during the 100 days before ruxolitinib therapy , the patient required 10 apheresis units of platelets and 7 units of packed red blood cells ; conversely , during ruxolitinib therapy , she received 3 apheresis units of platelets and 2 units of packed red blood cells . 
unfortunately , by day 116 , the leukemic blood count increased to 116 , 000 / l , and a bone marrow biopsy confirmed relapsed disease ( fig 3g )  . 
subtype of each individual sample : angioimmunoblastic t - cell lymphoma ( aitl ) ; anaplastic large - cell lymphoma ( alcl ) ; cutaneous t - cell lymphoma ( ctcl ) ; natural killer / t - cell ( nkt ) lymphoma ; peripheral t - cell lymphoma ( ptcl ) ; t - all ; t - cell large granular leukemia ( t - lgl ) ; and t - cell prolymphocytic leukemia ( t - pll )  . 
 genetic and immunophenotypic analysis of resistance to ruxolitinib therapy at relapse , the jak3 m511i allele frequency had increased from 5% to 28% , whereas the allele frequency of jak1 v658f had decreased from 40% to 18% in the t - pll cells ( fig 3f )  . 
the pre and post - ruxolitinib t - pll cells were analyzed by rna sequencing , in which the steady state abundance of mutant mrnas approximated the allele frequencies ( data supplement )  . 
the multidimensional staining pattern was analyzed by visne , an algorithm that maps cells on to a two - dimensional plot.33 peripheral - blood mononuclear cells from healthy donors were stratified into distinct cell populations that corresponded to specific lineages : cd4 + / cd8 + t cells , natural killer cells , macrophages , and b cells ( fig 4a )  . 
the t - pll cells from the patient case were clustered into a unique island composed of 95.3% total peripheral cells and few nonmalignant cell types ( fig 4a )  . 
 the cd45lo / population showed increased cd27 ( tnfrsf7 ) , cd44 ( h - cam ) , ccr4 , and ccr7 and reduced cd43 ( leukosialin ) compared with preor post - treatment cd45 + cells ( figs 4c through 4d )  . cd45 is a receptor tyrosine phosphatase encoded by the ptprc gene that negatively regulates jak - stat and t - cell receptor signaling.34 , 35 cd45 downregulation coincident with clinical relapse on ruxolitinib implied that it may be a mechanism for ruxolitinib resistance . 
the jak1 mutation was not detectable by sanger sequencing , but the jak3 mutation was clonal and present in cd45hi , cd45intermediate , and cd45 cells ( figs 5a and 5b )  . 
whole - transcriptome analysis on preand post - treatment samples found that ptprc mrna abundance was reduced significantly in the relapsed sample by 1.95 - fold ( p = 3.18e74 ; fig 5d ) , which approximates the 50% reduction in protein levels observed by flow cytometry . 
 jak1 and jak3 were probed by western blot analysis of whole - cell lysates and showed lower protein abundance in the relapsed sample compared with lysates before ruxolitinib treatment ( fig 5c )  . next , the tyrosine phosphatase activity was analyzed in lysates prepared from t - pll cells pre and post - ruxolitinib / relapse therapy . 
immunodepletion with a specific antibody against cd45 reduced total tyrosine phosphatase activity to 20% to 22% of normal , which confirmed that cd45 was the major enzyme to contribute to this enzyme activity in t - pll cells ( fig 5e )  . 
 ( a ) dot plots show the immunophenotype of the t - pll cells at presentation as analyzed by flow cytometry ; t - pll cells were interpreted as tdt cd1 cd3 + cd5 + cd7 + cd4 +  . 
 ( g ) plot of the total leukocytes for the patient ; y - axis shows cells number ( 103 ) ; gray brackets show the normal range of peripheral leukocyte number . 
dark blue arrows , time points of physical exams that show a palpable spleen 4 cm below costal margin before ruxolitinib therapy ; spleen mass was not palpable after treatment . 
 ( h ) bar graphs of t - pll cells treated in vitro with varying concentrations of ruxolitinib ( left panel ) or tofacitinib ( right panel ) in molar ( m ) quantities ; the y - axis shows cell viability . 
 peripheral - blood samples from a healthy donor and the patient with t - pll , before ruxolitinib ( pretreatment ) and at relapse ( post - treatment ) were analyzed by mass cytometry after staining for 28 cell surface markers . 
 ( a ) visne analysis performed on the data to allow grouping of peripheral leukocytes into distinct islands that correspond to ( b ) cell lineages ; iridium ( dna intercalator ) - positive ( ir + ) events show those cells that were intact . 
 ( a ) the visne map shows cell density for all ir + ( nucleic dna intercalator ) cells from a healthy donor and in pretreatment and post - treatment / relapse cells . 
 ( a - c ) flow cytometry dot plots show ( a ) staining patterns of t - cell prolymphocytic leukemia ( t - pll ) cells before ( pre - rx ) and after ( post - rx ) ruxolitinib treatment / relapse for forward scatter ( fsc ) and side scatter ( ssc ) , 7 - aminoactinomycin d ( 7 - aad ) , and anti - cd45 . 
three distinct populations were noted on the basis of cd45 expression ; ( b ) cells were flow sorted , extracted for genomic dna , subjected to polymerase chain reaction for relevant exons , and sequenced . 
left panel , rpkm for t - pll , reads per kilobase of gene per million reads ; right panel , rpkm normalized to pre - rx reads ( set at 100% )  . 
 ( e ) bar graphs show measured in vitro phosphatase activity from cytosolic lysates prepared from t - pll cells before ( blue ) and after ( gold ) ruxolitinib . 
the third set of assays was done after incubation with anti - cd45 / protein a / g ; values were normalized to cytosolic lysates before immunodepletion ( set at 100% ) ; error bars show standard error of the mean from quadruplicates . 
 time of disease relapse after treatment with combination cyclophosphamide , doxorubicin , vincristine , and prednisone chemotherapy ( data supplement )  . enhanced phosphorylations downstream of jak1 / jak3 at relapse cd45 has been shown to directly dephosphorylate jak1 and jak3 , which suggests that its loss of function should show increased activity of jak3 or jak1 . 
to assess whether t - pll cells had increased sensitivity to cytokine stimulation in addition to increased basal signaling , we stimulated each sample with 20 ng / ml of cytokine for 15 minutes . 
increased phosphorylation of stat5 was seen after in vitro stimulation with il - 2 , il - 4 , il - 7 , il - 21 , and interferon gamma , but not with il - 9 , in both preand post - ruxolitinib / relapsetreated samples compared with healthy t cells ( fig 6d )  . 
a comparison between preand post - ruxolitinib / relapse t - pll cells showed similar p - stat5 levels at baseline and after stimulation by cytokines ( fig 6d )  . 
for example , there was an il - 2induced 1.49 - fold change in p - stat5 for pre - ruxolitinib samples and 1.44 - fold ( comparison of arcsine transformed raw values ) change for post - ruxolitinib / relapse samples . 
to understand the effects of cd45 expression , we gated on cd45hi , cd45lo , and cd45 post - ruxolitinib / relapse t - pll cells and analyzed p - stat5 and p - stat6 basally and in response to stimuli . 
 cd45hi had the lowest p - stat5 response to il - 2 ( 0.23 - fold ) , followed by cd45lo ( 0.61 - fold ) and cd45 ( 1.24 - fold ; fig 6d ) ; this pattern was seen for all common gamma chain cytokines compared with control ( p - stat6 ; figs 6d and 6e )  . 
in summary , t - pll cells were hyper responsive to common gamma chain cytokines , and cd45 expression was negatively correlated with p - stat5 at relapse . discussion in this study , diverse t - cell neoplasms were profiled by targeted next - generation sequencing of the exomes from approximately 400 known tumor suppressors and oncogenes . 
the cohort was composed of occurrences submitted to foundation medicine as a result of relapsed or resistant disease , so the observed genetic alterations may be specific to advanced - stage disease or therapeutic resistance . 
nevertheless , the mutation frequencies for jak3 ( 13% of occurrences ) and for jak1 ( 8.7% ) were consistent with genomic profiling studies focused on specific disease subtypes ( ie , t - all , atll , t - pll , and ctcl15 - 19 ; less often , aitl and ptcl ) .38 , 39 the jak mutations in this study were mutually exclusive with stat3 and stat5 gene alterations , as expected , because stat3 and stat5 proteins are downstream of il2rg ( common gamma chain ) / jak1 / jak3restricted cytokines . 
interestingly , recent data in cell lines and mouse models suggest that jak1 enzyme activity is required for mutant jak3 effects.40 - 42 however , as in the index case , the mutations were co - occurring but not present in the same cell ; allele frequencies approached 50% for jak1 and jak3 mutations in the same tumor . most important , the jak1 and jak3 mutations were functionally significant , because they induced constitutive phosphorylations of downstream stat5 proteins . 
p - stat3 was not observed in the t - pll cells ( data not shown ) , although it is an important downstream substrate in other t - cell neoplasms , such as alcl.43 thus , signaling patterns downstream of jak1 / jak3 may be unique to disease subtype . 
stat1 and stat5 phosphorylations in t - pll could be inhibited by the specific jak inhibitors ruxolitinib and tofacitinib.44 in the index case , treatment with ruxolitinib induced an impressive clinical response . 
intracellular signaling responses , monitored by using phospho - flow cytometry , of peripheral - blood mononuclear cells ( pbmcs ) from healthy donors , and from the patient with t - pll before ( pretreatment ) and after ( post - treatment ) relapse experienced during ruxolitinib treatment . 
 ( d ) graphs show p - stat5 and p - stat6 for health donor t cells , pretreatment t - pll , and post - treatment t - pll unstimulated or after 15 minutes of cytokine stimulation at 20 ng / ml . ( e ) similar graphs of cytokine - stimulated p - stat5 and p - stat6 for post - treatment t - pll cells with cd45hi , cd45lo , or cd45neg gating . 
furthermore , this oral drug worked when intensive parenteral therapies had failed to control the disease . this study showed two cell - intrinsic mechanisms to account for resistance to ruxolitinib : expansion of the mutant jak3 t - pll clone and downregulation of cd45 . 
in in vitro studies , the ic50 of ruxolitinib for jak1 is 3.3 nm ; for jak2 , it is 2.8 nm45 ; and for jak3 , it is 428 nm.45 this diminished potency against jak3 probably accounted for the expansion of the mutant jak3 clone from 10% before ruxolitinib to 56% at relapse . 
the t - pll cells showed cross - resistance to tofacitinib , which has a nanomolar ic50 for jak3.46 , 47 the downregulation of cd45 protein appears to be an additional resistance mechanism at relapse . 
the expression pattern of cd45 in a clonal t - pll population resembles position effect variegation , an epigenetic phenomenon.48 , 49 because the primary leukemia samples were consumed , we were unable to directly transduce ptprc cdna to test if jak inhibitor sensitivity could be restored . 
 reddy , xueyan chen administrative support : siraj ali , utpal dav financial support : utpal dav data analysis and interpretation : allison greenplate , kai wang , rati m . 
irish , utpal dav m511i mutation that had similarly downregulated cd45 after disease relapse during chop chemotherapy , which suggests that downregulation of the cd45 protein may play a role in chemotherapy resistance . 
notably , porcu et al50 discovered deletion , missense , and nonsense mutations in ptprc in t - allevidence that supports a tumor suppressor role for ptprc in this disease . 
furthermore , porcu et al50 also showed concordant loss of function in ptprc and gain of function in jak1 or il7r , which suggests that these two hits cooperate in t - all pathogenesis . 
our studies on the index case are similar to these findings , because we also observed an inverse correlation between cd45 levels and p - stat5 , albeit in t - pll . 
our studies do suggest that ptprc may be a tumor suppressor in more mature t - cell neoplasms in addition to precursor t - all and that its loss of function may be an important resistance mechanism to ruxolitinib . 
finally , the data presented in this study support the design of larger phase i / ii clinical trials to test ruxolitinib on its own or in combination with cytotoxic therapies in t - cell neoplasms . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome stuff in non - neoplastic disease ( i ) phil j . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center yu shyr consulting or advisory role : aduro biotech , janssen research and development , novartis , roche , genentech yan guo no relationship to disclose nishitha m . 
reddy consulting or advisory role : celgene , abbvie , gilead sciences , bristol - myers squibb lina kozhaya no relationship to disclose derya unutmaz no relationship to disclose xueyan chen no relationship to disclose jonathan m . 
irish research funding : janssen ( inst ) , incyte ( inst ) , pharmacyclics ( inst ) patents , royalties , other intellectual property : methods and compositions for risk stratification , us patents ( us 7 , 393 , 656 , us 7 , 939 , 278 , us 8 , 206 , 939 , us 8 , 309 , 316 , us 8 , 394 , 599 ) other relationship : cytobank utpal dav no relationship to disclose acknowledgment we thank stephen brandt , md , scott hiebert , phd , carlos arteaga , md , and justin balko , phd , for helpful discussions and kevin weller , phd , for his expert advice . the content is solely the responsibility of the authors and does not represent the official views of the national institutes of health . affiliations allison greenplate , rati m . 
miller , foundation medicine , cambridge , ma ; kai wang , origimed , shanghai , china ; lina kozhaya and derva unutmaz , jackson laboratory , farmington , ct ; xueyan chen , university of washington medical center , seattle , wa ; and utpal p . 
coustan - smith e , mullighan cg , onciu m , et al : early t - cell precursor leukemia : a subtype of very high - risk acute lymphoblastic leukemia . 
patrick k , wade r , goulden n , et al : outcome for children and young people with early t - cell precursor acute lymphoblastic leukemia treated on a contemporary protocol , ukall 2003 . 
chiaretti s , li x , gentleman r , et al : gene expression profile of adult t - cell acute lymphocytic leukemia identifies distinct subsets of patients with different response to therapy and survival . 
weisenburger dd , savage kj , harris nl , et al : peripheral t - cell lymphoma , not otherwise specified : a report of 340 cases from the international peripheral t - cell lymphoma project . 
parrilla castellar er , jaffe es , said jw , et al : alk - negative anaplastic large - cell lymphoma is a genetically heterogeneous disease with widely disparate clinical outcomes . 
wood bl , winter ss , dunsmore kp , et al : t - lymphoblastic leukemia ( t - all ) shows excellent outcome , lack of significance of the early thymic precursor ( etp ) immunophenotype , and validation of the prognostic value of end - induction minimal residual disease ( mrd ) in childrens oncology group ( cog ) study aall0434 . 
boucheix c , david b , sebban c , et al : immunophenotype of adult acute lymphoblastic leukemia , clinical parameters , and outcome : an analysis of a prospective trial including 562 tested patients ( lala87 )  . 
koretzky ga , picus j , schultz t , et al : tyrosine phosphatase cd45 is required for t - cell antigen receptor and cd2 - mediated activation of a protein tyrosine kinase and interleukin 2 production . 
irish jm , myklebust jh , alizadeh aa , et al : b - cell signaling networks reveal a negative prognostic human lymphoma cell subset that emerges during tumor progression . 
vallois d , dobay mpd , morin rd , et al : activating mutations in genes related to tcr signaling in angioimmunoblastic and other follicular helper t - cell - derived lymphomas . 
boddicker rl , razidlo gl , dasari s , et al : integrated mate - pair and rna sequencing identifies novel , targetable gene fusions in peripheral t - cell lymphoma . 
degryse s , de bock ce , cox l , et al : jak3 mutants transform hematopoietic cells through jak1 activation , causing t - cell acute lymphoblastic leukemia in a mouse model . 
losdyck e , hornakova t , springuel l , et al : distinct acute lymphoblastic leukemia ( all ) associated janus kinase 3 ( jak3 ) mutants exhibit different cytokine - receptor requirements and jak inhibitor specificities . 
flanagan me , blumenkopf ta , brissette wh , et al : discovery of cp - 690 , 550 : a potent and selective janus kinase ( jak ) inhibitor for the treatment of autoimmune diseases and organ transplant rejection . 
quints - cardama a , vaddi k , liu p , et al : preclinical characterization of the selective jak1 / 2 inhibitor incb018424 : therapeutic implications for the treatment of myeloproliferative neoplasms . 
 detection of somatic structural variants enables quantification and characterization of circulating tumor dna in children with solid tumors objective liquid biopsies are being rapidly used in adult cancers as new biomarkers of disease . 
therefore , we developed a next - generation sequencing approach to detect and quantify ctdna in the blood of patients with the most common pediatric solid tumors . methods detection of ctdna requires assays sensitive to somatic events typically observed in the cancer type being studied . 
we adapted an ultralow passage whole - genome sequencing approach to capture copy number variants and a hybrid capture sequencing assay to detect translocations in liquid biopsy samples from pediatric patients . results copy number changes seen by ultralow passage whole - genome sequencing enabled detection of ctdna in patients with osteosarcoma , neuroblastoma , alveolar rhabdomyosarcoma , and wilms tumor . 
we also found that disease - specific genomic biomarkers of prognosis were detectable in ctdna . conclusion this study demonstrates that liquid biopsy approaches that detect somatic structural variants are well suited to pediatric solid tumors . 
we show that children with the most common solid tumor malignancies have detectable levels of ctdna , which may be used to track disease response and identify genomic subclassifiers of disease . 
2018 by american society of clinical oncology introduction cancer remains one of the most common childhood causes of disease - related death in developed countries.1 patients with pediatric solid tumor malignancies are commonly treated with regimens that combine intensive chemotherapy , surgery , and radiation therapy.2 this approach has led to tremendous improvements in outcome , with overall cure rates for pediatric solid tumors now > 80%.3 however , these cures come at the cost of exposing patients to a high risk of long - term toxicities resulting in significant morbidity.4 in some diseases , such as wilms tumor , efforts to de - escalate therapy have resulted in stable cure rates for low - risk patients accompanied by reduced treatment toxicity.5 , 6 in other diseases , such as ewing sarcoma , a lack of prognostic biomarkers limit the ability to risk stratify therapy.7 , 8 in both cases , the development of new and more precise assays for risk stratification could improve outcomes by facilitating patient - specific treatment modifications . kelly klega alma imamovic - tuco gavin ha andrea n . 
crompton author affiliations and support information ( if applicable ) appear at the end of this article . the contents are solely the responsibility of the authors and do not necessarily represent the official views of the national institutes of health or other funding agencies . corresponding author : brian d . 
numerous studies have now demonstrated that circulating tumor dna ( ctdna ) levels in adults with cancer correlate with disease burden and track with treatment responses over time.9 - 14 the development of ctdna assays rely on identification and quantification of somatic mutations.9 , 15 many ctdna assays have been developed to detect highly recurrent hot - spot mutations that frequently drive adult malignancies.9 , 12 , 13 , 16 - 18 however , recent comprehensive sequencing efforts in pediatric cancers show that pediatric solid tumors are rarely driven by highly recurrent single - nucleotide variants.19 instead , structural variants , including chromosomal copy number changes and dna translocations , are common somatic events in these tumor types.20 - 26 to determine whether patients with childhood solid tumor malignancies express detectable levels of ctdna , we adapted two next - generation sequencing strategies to detect and quantify structural variants in the plasma of these patients . 
 we applied these assays to five of the most common types of pediatric solid tumors , excluding cns tumors , to quantify ctdna levels , identify genomic subtypes , and confirm the feasibility of using ctdna assays to track disease response to therapy . methods patients and tissue samples patients at the dana - farber cancer institute and boston childrens hospital were consented to an institutional review boardapproved protocol . 
patients were included if an initial peripheral blood , pleural effusion , or bone marrow sample was collected within 3 days from the start of chemotherapy and before a surgical resection . 
additional details are available in the data supplement . sequencing library preparation , sequencing alignment , and ultralow passage whole - genome sequencing coverage for all experiments , sequencing library preparation and sequencing data alignment were performed using standard techniques . 
additional details are available in the data supplement . translocation - specific sarcoma sequencing assay development and sequencing to detect pediatric sarcoma - specific translocations in cell - free dna , we developed a unique hybrid capture sequencing assay . 
first , we reviewed the literature to identify the genomic introns involved in oncogenic translocations in the ewsr1 , fus , cic , ccnb3 , pax3 , pax7 , and tp53 genes.20 , 21 , 25 - 33 second , we used the sureselect advanced design wizard ( agilent technologies , santa clara , ca ) to create capture probes targeting these regions and the coding regions of tp53 and stag2 with the following design options : sense strand , 3 tiling density , least stringent masking , balanced boosting , and region extensions of 10 bases from the 3 and 5 ends ( data supplement )  . 
the average measured coverage at enrichment sites for all samples tested by transs - seq was 655 ( range , 31 to 1 , 464 )  . sequencing analysis ulp - wgs analysis was performed using the ichorcna algorithm ( dinstitute / ichorcna ) , with manual curation of results.34 in brief , ulp - wgs uses relative sequencing coverage of whole - genome data and computational correction of sequencing bias to detect segmental copy number changes . 
 wild - type reads detected in each sample , we developed a custom algorithm designed to realign all sequencing reads to either the reference human genome or the patient - specific translocation positive reference sequence ( vanallenlab / peds_ctdna )  . 
the algorithm then reported the number of reads aligned at the patient - specific translocation breakpoint and the number of wild - type reads at the equivalent genomic base - pair location within the human reference genome . 
because each cancer genome contains one translocated and one wild - type allele , whereas germline genomes contain two wild - type alleles , we used the following formula to calculate the percentage of ctdna , where t equals the number of translocation reads and w equals the number of wild - type reads : % ctdna = t / { [ ( w - t ) / 2 ] + t }  . cell lines and digital droplet polymerase chain reaction the ew8 ewing sarcoma cell line dilution experiments , digital droplet polymerase chain reaction ( ddpcr ) methods , and ddpcr primers are listed in the data supplement . highest values originating from patients with neuroblastoma ( fig 1a )  . 
ulp - wgs was performed for each sample to detect and quantify ctdna by measuring segmental copy number changes as recently described.34 ctdna was detected in 50% of pretreatment plasma samples from patients with osteosarcoma , neuroblastoma , wilms tumor , and alveolar rhabdomyosarcoma . 
in patients with detectable ctdna , the pattern of segmental chromosomal copy number changes in cellfree dna matched the copy number pattern observed in the tumor biopsy from the same patient ( figs 1c and 1d ; data supplement )  . 
in four of the seven patients with ewing sarcoma with no detectable ctdna , ulp - wgs analysis of tumor biopsy dna material demonstrated no discernable segmental copy number changes ( fig 2 )  . 
this finding is consistent with previous reports that ewing sarcoma tumors have few highly recurrent somatic events other than the ewsr1 / ets translocations and suggests that an alternative method for detection of ctdna is necessary for this disease.21 , 26 results patients and samples a liquid biopsy sample was collected before the initiation of therapy from 45 pediatric patients with cancer with a confirmed diagnosis of ewing sarcoma ( n = 11 ) , osteosarcoma ( n = 10 ) , neuroblastoma ( n = 10 ) , wilms tumor ( n = 8 ) , or alveolar rhabdomyosarcoma ( n = 7 )  . 
dna from tumor biopsy material from patients with neuroblastoma and wilms tumor were not readily available . circulating tumor dna is detectable in patients with pediatric solid tumor malignancies total cell - free dna levels ranged from 2 ng to 3.5 g of dna per 1 ml of plasma , with the translocation detection outperforms copy number detection for ewing sarcoma to detect ctdna in translocation - positive tumors , we developed a novel hybrid - capture assay , termed transs - seq , designed to sequence intronic regions involved in genomic rearrangements in pediatric sarcomas . 
first , we confirmed that the assay could detect the expected translocations in a panel of ewing and ewing - like sarcomas and alveolar rhabdomyosarcomas ( data supplement )  . 
ddpcr in these samples confirmed the ability to detect and quantify the ew8 - specific ewsr1 / fli translocation across the range of dilutions ( fig 3a ; data supplement )  . 
 ( a ) quantity of cell - free dna extracted per ml of plasma or body fluid in patients with osteosarcoma ( ost ) , alveolar rhabdomyosarcoma ( arms ) , ewing sarcoma ( ews ) , wilms tumor ( wilms ) , and neuroblastoma ( nb )  . 
the color for each data point corresponds to the relative copy number change from baseline , with blue equal to two copies of the genomic location , green equal to copy number loss , and red equal to copy number gains . 
the same pattern of copy number changes is observed in dna sequenced from a tumor biopsy ( top ) and a pretreatment blood sample ( bottom ) in ( c ) a patient with osteosarcoma and ( d ) alveolar rhabdomyosarcoma . and detected ew8 dna at a concentration of 1.56% ( figs 3b and 3c ; data supplement )  . identical to the breakpoint observed from the tumor biopsy sample . transs - seq was then applied to cell - free dna samples from patients with ewing sarcoma and alveolar rhabdomyosarcoma . 
for five patients with ewing sarcoma and three patients with alveolar rhabdomyosarcoma , dna from tumor biopsy samples was also profiled by transs - seq ( data supplement )  . 
in all cases , the unique genomic breakpoint in the ctdna was previous studies in ewing sarcoma have used ddpcr assays that amplify patient - specific ews / ets translocations to measure ctdna levels in patients.36 - 38 to compare transs - seq with this previously validated approach , patient specific polymerase chain reaction primers were developed for a subset of ewing sarcoma and alveolar rhabdomyosarcoma samples ( data supplement )  . 
 mrd0006 ewing sarcoma mrd0019 ewing sarcoma 108765 14 16 18 20 23 x 108765 14 16 18 20 23 x 14 16 18 20 23 x 108765 14 16 18 20 23 x chromosome mrd0023 ewing sarcoma chromosome mrd0046 ewing sarcoma chromosome chromosome mrd0007 ewing sarcoma 108765 chromosome mrd0041 ewing sarcoma 108765 chromosome mrd0047 ewing sarcoma 14 16 18 20 23 x 108765 14 16 18 20 23 x 14 16 18 20 23 x 108765 chromosome fig 2 . 
genome - wide copy number plots from seven ewing sarcoma tumor biopsy samples detected by ultralow passage whole - genome sequencing in patients for which circulating tumor dna could not be detected from peripheral blood . 
in three of the four patients with ewing sarcoma for which no copy number change could be detected by ulp - wgs in the tumor ( mrd0006 , mrd0041 , mrd0047 ) , transsseq was able to detect an ewsr1 - fusion in the tumor and cell - free dna ( data supplement )  . 
in the fourth patient ( mrd0007 ) , transs - seq detected an ewsr1 / fli fusion in the tumor but not in cell - free dna ( data supplement )  . 
however , four patients with tumor necrosis < 70% ( mrd0031 , mrd0036 , mrd0040 , mrd0054 ) had detectable ctdna in at least one sample collected after initiation of chemotherapy ( fig 4d ; data supplement )  . 
 finally , in patients whose ctdna levels became undetectable with therapy but then experienced a clinical relapse or progression , ctdna was again detectable before the initiation of relapsed therapy ( fig 4b ; data supplement )  . genomic markers of poor outcome are detectable in ctdna we also examined whether disease - specific genomic markers of prognosis could be detected in ctdna . 
recent studies demonstrate that mutations in stag2 and tp53 may be associated with a worse outcome in ewing sarcoma.21 , 26 a frame - shift mutation in stag2 was detected by ctdna from one patient ( mrd0023 ) , and a mutation in tp53 was detected in another patient ( mrd0003 ; data supplement )  . 
in alveolar rhabdomyosarcoma , studies have demonstrated that patients with pax3 / foxo1 have a worse prognosis than patients with pax7 / foxo1 translocation.41 the foxo1 fluorescent in situ hybridization probe , which is used in the diagnostic work - up of alveolar rhabdomyosarcoma , confirms a foxo1 rearrangement but not the fusion partner . 
in osteosarcoma , copy number gains of chromosome arm 8q are associated with a poor outcome.42 - 44 ulp - wgs detected copy number gains in 8q in seven of nine osteosarcoma samples with detectable ctdna ( fig 1c ; data supplement )  . 
amplification of mycn is a well - established marker of poor prognosis in neuroblastoma.45 , 46 mycn amplification was detectable in the ctdna of two patients by ulp - wgs ( fig 5a ; data supplement )  . 
finally , in wilms tumor , copy number gains of 1q were associated with poor prognosis in favorable histology tumors.47 ulp - wgs detected 1q gain in copy number change but ulp - wgs was unable to detect ctdna from the same patient ( mrd0019 , mrd0023 , mrd0046 ) , transsseq detected low levels of ctdna , suggesting that transs - seq may have greater sensitivity for ctdna than ulp - wgs in ewing sarcoma ( data supplement )  . ctdna levels track with disease burden in pediatric solid tumors when comparing ctdna levels across cancer types , neuroblastoma demonstrated a significantly higher percentage of ctdna ( median , 55% ; range , 13% to 98% ) than other cancer types ( data supplement )  . 
in patients with newly diagnosed ewing sarcoma and alveolar rhabdomyosarcoma , ctdna levels declined rapidly after initiation of chemotherapy , often becoming undetectable by the start of the second cycle ( figs 4a and 4b ; data supplement )  . 
in osteosarcoma , studies have shown that a high percentage of tumor necrosis observed in the primary tumor after neoadjuvant chemotherapy is associated with a better prognosis.39 , 40 in five patients with newly diagnosed osteosarcoma , the percentage of tumor necrosis was available . 
the translocation - specific sarcoma sequencing assay ( transs - seq ) detects circulating tumor dna ( ctdna ) in ewing sarcoma ( ews ) and alveolar rhabdomyosarcoma ( arms )  . 
 samples are plotted on the x - axis by the percentage of ew8 by experimental dilution and on the y - axis by the percentage of ew8 dna detected by digital droplet polymerase chain reaction ( ddpcr )  . 
 ( d ) percentage of ctdna levels in cell - free dna samples from patients with ewing sarcoma and arms ( same samples as in figure 1b ) determined by transsseq . 
 percentage of ctdna levels from serial cell - free dna samples collected from four patients with ( a ) ewing sarcoma , ( b ) alveolar rhabdomyosarcoma , ( c - d ) osteosarcoma . 
blue dots indicate peripheral blood samples , and the red dot ( b ) indicates a bone marrow sample collected simultaneously with a blood sample . mrd0019 ewing sarcoma mrd0045 alveolar rhabdomyosarcoma bone marrow clinical course clinical course mrd0061 osteosarcoma mrd0036 osteosarcoma clinical course clinical course had detectable levels of ctdna . 
patients with neuroblastoma had the highest levels of ctdna , including two patients with > 1 g of cell - free dna per ml of plasma , which was nearly 100% composed of tumor dna . 
however , one obvious limitation to the use of ulp - wgs was in tumor types with low rates of copy number alterations , such as ewing sarcoma . recent liquid biopsy studies in ewing sarcoma have used the development of patient - specific ddpcr assays.36 - 38 although this approach has proven to be highly sensitive and quantitative , the development of each assay requires genomic profiling of large amounts of tumor biopsy material to establish the patient - specific oncogenic translocation . 
one recent study used a combination of ddpcr and hybrid capture sequencing to detect ewsr1 translocations in ewing sarcoma and desmoplastic small roundcell tumors.38 results showed that it is feasible to detect ewsr1 translocations directly from the plasma of these patients without first sequencing the tumor sample . 
despite the larger genomic region targeted for hybrid capture , the transs - seq assay detected ctdna in 10 of 11 pretreatment samples obtained from ewing sarcoma , similar to rates observed by other groups . 
we also demonstrated that quantification of ctdna levels was similar using either transs - seq or ddpcr . in this study , changes in ctdna levels were observed during a patients clinical course and corresponded to changes in disease burden . 
with next - generation sequencing becoming increasingly available for clinical decision making , we anticipate that our ctdna assays could also be adapted to clinical laboratory testing if they demonstrate significant improvements to risk stratification for pediatric solid tumors . 
 ( a ) sequencing coverage ( read counts ) across the mycn gene ( top ) and c - myc gene ( bottom ) from four cell - free dna samples from patients with neuroblastoma . 
therefore , prospective studies should be designed to obtain frequent samples throughout treatment so that the time points most predictive of outcome can be appropriately identified . finally , our study demonstrates that next generation sequencing of ctdna can detect existing genomic biomarkers of outcome and may provide another modality for genomic profiling of tumors in patients . 
furthermore , it remains unclear whether these genomic biomarkers are primarily clonal or heterogeneous events within a tumor or across tumors and whether the clonality of these genomic events changes in patients who relapse after therapy . 
recent studies demonstrate that ctdna can detect intratumor and multitumor heterogeneity and detect complex patterns of treatment resistance.52 - 55 with the emergence of new sequencing modifications that improve sensitivity and decrease sequencing errors , we believe that ctdna profiling by next - generation sequencing approaches will improve our understanding of tumor heterogeneity and patterns of somatic evolution in pediatric solid tumors.12 , 16 in addition , the assays described in this study could facilitate broader profiling of ctdna , such as deep whole - exome sequencing , by providing a mechanism to screen samples for the presence of sufficiently abundant ctdna , allowing selection of samples most likely to yield informative data . in summary , our study demonstrates that patients with pediatric solid tumors have detectable levels of ctdna , which can be measured with next generation sequencing approaches that do not require profiling of tumor biopsy material or patient - specific assays . 
disease - specific genomic hallmarks of pediatric solid tumors can also be identified in liquid biopsy samples , and ctdna levels correlate with disease burden and response to therapy over time . 
crompton manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors anwesha nag no relationship to disclose eliezer van allen stock and other ownership interests : syapse , tango therapeutics , genome medical consulting or advisory role : syapse , roche , third rock ventures , takeda , novartis , genome medical , invitae speakers ' bureau : illumina research funding : bristol - myers squibb , novartis elizabeth mullen no relationship to disclose steven g . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . katherine janeway no relationship to disclose matthew meyerson stock and other ownership interests : origimed consulting or advisory role : origimed research funding : bayer ( inst ) patents , royalties , other intellectual property : patent on egfr mutations for lung cancer diagnosis aaron r . 
crompton employment : mersana ( i ) , shire ( i ) stock and other ownership interests : mersana ( i ) , shire ( i ) acknowledgment we thank the boston childrens hospital biorepository for processing a portion of the blood samples . 
pediatr blood cancer 60 : 1083 - 1094 , 2013 kelly klega no relationship to disclose alma imamovic - tuco no relationship to disclose gavin ha no relationship to disclose andrea n . 
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yung tk , chan kc , mok ts , et al : single - molecule detection of epidermal growth factor receptor mutations in plasma by microfluidics digital pcr in non - small cell lung cancer patients . 
shern jf , chen l , chmielecki j , et al : comprehensive genomic analysis of rhabdomyosarcoma reveals a landscape of alterations affecting a common genetic axis in fusion - positive and fusionnegative tumors . 
tirode f , surdez d , ma x , et al : genomic landscape of ewing sarcoma defines an aggressive subtype with co - association of stag2 and tp53 mutations . 
kawamura - saito m , yamazaki y , kaneko k , et al : fusion between cic and dux4 up - regulates pea3 family genes in ewing - like sarcomas with t ( 4 ; 19 ) ( q35 ; q13 ) translocation . 
ng tl , osullivan mj , pallen cj , et al : ewing sarcoma with novel translocation t ( 2 ; 16 ) producing an in - frame fusion of fus and fev . 
sugita s , arai y , tonooka a , et al : a novel cic - foxo4 gene fusion in undifferentiated small round cell sarcoma : a genetically distinct variant of ewing - like sarcoma . 
yoshimoto m , graham c , chilton - macneill s , et al : detailed cytogenetic and array analysis of pediatric primitive sarcomas reveals a recurrent cic - dux4 fusion gene event . 
shukla nn , patel ja , magnan h , et al : plasma dna - based molecular diagnosis , prognostication , and monitoring of patients with ewsr1 fusion - positive sarcomas . 
meyers pa , schwartz cl , krailo m , et al : osteosarcoma : a randomized , prospective trial of the addition of ifosfamide and / or muramyl tripeptide to cisplatin , doxorubicin , and high - dose methotrexate . 
sorensen ph , lynch jc , qualman sj , et al : pax3 - fkhr and pax7 - fkhr gene fusions are prognostic indicators in alveolar rhabdomyosarcoma : a report from the childrens oncology group . 
tarkkanen m , elomaa i , blomqvist c , et al : dna sequence copy number increase at 8q : a potential new prognostic marker in high - grade osteosarcoma . 
gratias ej , dome js , jennings lj , et al : association of chromosome 1q gain with inferior survival in favorable - histology wilms tumor : a report from the childrens oncology group . 
lecomte t , berger a , zinzindohou f , et al : detection of free - circulating tumor - associated dna in plasma of colorectal cancer patients and its association with prognosis . 
tie j , wang y , tomasetti c , et al : circulating tumor dna analysis detects minimal residual disease and predicts recurrence in patients with stage ii colon cancer . 
vora a , goulden n , mitchell c , et al : augmented post - remission therapy for a minimal residual disease - defined high - risk subgroup of children and young people with clinical standard - risk and intermediate - risk acute lymphoblastic leukaemia ( ukall 2003 ) : a randomised controlled trial . 
de mattos - arruda l , weigelt b , cortes j , et al : capturing intra - tumor genetic heterogeneity by de novo mutation profiling of circulating cell - free tumor dna : a proof - of - principle . 
thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . 
 clinical value of rna sequencing based classifiers for prediction of the five conventional breast cancer biomarkers : a report from the population - based multicenter sweden cancerome analysis networkbreast initiative purpose in early breast cancer ( bc ) , five conventional biomarkersestrogen receptor ( er ) , progesterone receptor ( pgr ) , human epidermal growth factor receptor 2 ( her2 ) , ki67 , and nottingham histologic grade ( nhg ) are used to determine prognosis and treatment . 
we aimed to develop classifiers for these biomarkers that were based on tumor mrna sequencing ( rna - seq ) , compare classification performance , and test whether such predictors could add value for risk stratification . methods in total , 3 , 678 patients with bc were studied . 
patients with discordant classifications , predicted as hormone responsive by histopathology but non hormone responsive by mgc , had significantly inferior overall survival compared with patients who had concordant results . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license christian brueffer johan vallonchristersson dorthe grabau anna ehinger jari hkkinen cecilia hegardt janne malina yilun chen pr - ola bendahl jonas manjer martin malmberg christer larsson niklas loman lisa rydn ke borg lao h . 
immunohistochemistry ( ihc ) is the principal method for er , pgr , her2 , and ki67 measurement , and in situ hybridization ( ish ) methods are used to refine her2 ihc . 
 accuracy and reproducibility are concerns , with up to 20% false - positive or false - negative er / pgr ihc determinations.3 varying discordance has been reported for her2 ihc and fluorescent ish ( fish ) .4 - 7 accordingly , consensus guidelines emphasize standardization and validation of analytic performance.1 , 2 , 8 lack of standardization has slowed the entrance of ki67 into clinical routines.9 for example , ki67 status was only moderately concordant in an interlaboratory reproducibility analysis.10 thresholds for ki67 positivity are evolving ; cutoffs between 20% and 29% were recommended by the 2015 st gallen / vienna panel for laboratories with a quality assurance program.11 swedish quality assurance program guidelines recommend that each laboratory calibrate a cutoff yearly such that one third of 100 consecutive occurrences are ki67 - high . 
in 2010 , toward implementation of molecular profiling in the clinical routine , we launched the sweden cancerome analysis network breast initiative ( scan - b ; clinicaltrials.gov identifier : nct02306096 ) , an ongoing population - based multicenter observational study covering a wide geography of sweden that prospectively invites all patients with bc to participate.17 to date , approximately 85% of the eligible catchment population are included , more than 11 , 000 patients have enrolled , and blood and fresh tumor tissues are sampled for molecular research . 
thus , for each bc , it will be possible to report a multitude of biomarker tests simultaneously on the basis of its rna - sequencing data and within a clinically actionable time frame . herein , we aimed to validate the scan - b multicenter infrastructure and provide molecular analyses of clinical value by developing rnaseqderived classifiers for the conventional histopathologic bc biomarkers er , pgr , her2 , ki67 , and nhg . 
for this purpose , both single gene classifiers ( sgcs ) and multigene classifiers ( mgcs ) were developed by using a training cohort , the prediction accuracy was compared against current clinical practice across a large independent prospective cohort , and the classifier predictions and their discrepancies to histopathology were evaluated with respect to patient survival . methods patients the study ( fig 1 ) was approved by the regional ethical review board of lund at lund university and the swedish data inspection group . 
 diagnostic reading diagnostic stains : er , pgr , her2 , nhg two independent readings histopathology performance evaluation training set ( n = 405 ) five biomarkers : er , pgr , her2 , nhg , ki67 new stains : er , pgr , her2 , ki67 three independent readings rna sequencing train sgc / mgc consensus pathology scores independent validation set ( n = 3 , 273 ) rna sequencing apply trained sgc / mgc classifier performance evaluation and survival analysis five biomarkers : er , pgr , her2 , nhg , ki67 diagnostic stains : er , pgr , her2 , nhg , ki67 diagnostic reading fig 1 . 
study design flow diagraer , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; ki67 , proliferation antigen ki67 ; mgc , multigene classifier ; nhg , nottingham histologic grade ; pgr , progesterone receptor ; sgc , single - gene classifier . and er - negative tumors ( training cohort ; data supplement )  . 
for classifier testing , an independent , prospective , and population - based modern cohort of 3 , 273 patients with early bc was assembled from the ongoing scan - b study17 ( validation cohort ; appendix fig a1 ; data supplement )  . histopathology for the training cohort , all biomarkers with the exception of ki67 were evaluated at time of diagnosis . 
in addition , new formalin - fixed paraffin - embedded slides were analyzed for er , pgr , and ki67 ihc and for her2 silver ish , all performed at a central laboratory ( helsingborg hospital )  . 
the diagnostic slides and newly stained slides were each scored in total by three pathologists independently by using 1% or greater tumor cell staining threshold for hormone receptor positivity , standard her2 herceptest ( agilent / dako , santa clara , ca ) and ish criteria ( roche / ventana , tucson , az ) , greater than 20% positive nuclei for ki67high status , and the nhg scoring system ( data supplement )  . 
the biologic functional annotation clusters of each mgc signature were evaluated with the david bioinformatics resource.20 statistical analysis histopathology evaluations and single - gene and multigene predictions were compared with agreement statistics21 ( defined in the data supplement ) and balanced statisticscohens and matthews correlation coefficient ( mcc ) and were interpreted according to viera and garrett.22 the and mcc values were comparable ( data supplement ) , so we focused on  . 
 multivariable cox models included the variables age at diagnosis , lymph node status , tumor size , er , pgr , her2 , and nhg as covariates , as relevant ( data supplement )  . 
as expected with minimization of technical and heterogeneity factors , within - slide concordances were slightly better than betweenslide concordances ( data supplement )  . classifier training whole - transcriptome expression profiles were generated for the 405 training samples using rna - seq . 
for the sgcs , optimal thresholds were determined for esr1 ( which encodes the er protein ) , pgr ( pgr ) , erbb2 ( her2 ) , and mki67 ( ki67 ) ( data supplement )  . 
the constituent biologic themes for each mgc classifier were investigated with functional annotation clustering ( data supplement )  . performance on independent data to evaluate the classifiers , we tested them on rna - seq data generated for 3 , 273 independent tumors from the prospective population - based multicenter scan - b study ( n = 136 tumors were analyzed in technical replicates )  . 
for rna - seq replicates , 534 ( 98.2% ) of 544 sgc classifications and 675 ( 99.3% ) of 680 mgc classifications were concordant ( data supplement )  . 
within a biomarker staining group ( left - most column headings ) , all comparisons presented are the reference evaluation ( the diagnostic reading made in the clinical routine , or reader 1 in the case of ki67 ) versus each specified reader number . 
 abbreviations : er , estrogen receptor ; h&e , hematoxylin and eosin ; her2 , human epidermal growth factor receptor 2 ; ihc , immunohistochemistry ; nhg , nottingham histologic grade ; pgr , progesterone receptor ; sish , silver in situ hybridization . survival analysis to evaluate the possible clinical utility of our classifiers , we analyzed our classifier predictions within the validation cohort with respect to overall survival . 
kaplan - meier analysis revealed comparable patient stratification for both diagnostic histopathology and sgcs for the five biomarkers across the entire validation cohort , whereas the mgcs had a noticeably richer stratification , particularly for the hormone receptors and the hormone - responsive group , defined by er positivity and pgr positivity ( appendix figs a4 and a5 )  . 
after adjusting for important covariates in multivariable cox analyses , the mgc prediction for hormone nonresponsiveness was a significant stratifier among patients with histopathologic hormone - responsive disease who were treated with endocrine therapy , as were the mgc predictions discordant for her2 - negative or ki67 - high status in patients who received chemotherapy with or without trastuzumab and / or endocrine therapy . 
previously , several gene expressionbased approaches for determination of known treatment - predictive biomarkers have been developed16 , 23 - 26 ; however , they are not widely used clinically in most countries . 
 ( a ) forest plots of concordance statistics for histopathologic evaluation in the training set ( blue square markers ) , and single - gene classifiers ( sgcs ; gold circles ) and multigene classifiers ( mgcs ; gray diamonds ) in the validation cohort , which plots overall agreement with 95% cis , specific agreements ( positive and negative agreements for estrogen receptor [ er ] , progesterone receptor [ pgr ] , human epidermal growth factor receptor 2 [ her2 ] , and ki67 ) and nottingham histologic grade ( nhg ) category agreements ( grade [ g ] 1 , g2 , and g3 ) , and values with 95% cis . 
scan - b , sweden cancerome analysis networkbreast . demonstrated that accurate classifiers for er , pgr , her2 , ki67 and nhg can be built with rna - seq data , can provide a valuable complement to traditional histopathology , and represent the first of many potential clinical reports that can be delivered from a single rna - seq measurement . 
in the future , we foresee the development , validation , and clinical implementation of a multitude of signatures , classifiers , and mutational profiles within the scan - b population - based infrastructure and rna - seq platform.17 , 18 we also aim to use rna - seq analyses in the performance of interventional clinical trials.29 the quality of machine - learned classifiers is crucially dependent on the quality of the labels on which they have been trained . 
matched against routine histopathologic evaluation , repeated er , pgr , and her2 readings showed good concordance , whereas ki67 and nhg had notably lower concordance between pathologists ( table 1 )  . 
 ( a ) histopathologically hormone responsive ( defined as estrogen receptor [ er ] positive and progesterone receptor [ pgr ] positive ) group stratified by mgc hormone responsive classification ( concordant [ blue curve ] or discordant [ gold curve ] to histopathology ) within the subgroup of patients who received ( left ) no adjuvant systemic therapy , ( middle ) endocrine therapy alone , or ( right ) chemotherapy with or without trastuzumab or endocrine therapy . 
 it is unlikely that a classifier would perform better than the quality of training labels ; therefore , it is not surprising that our classifiers had the worst performance for ki67 and nhg . 
moreover , because we benchmarked our biomarker predictions in the validation cohort to the clinical diagnostic histopathology results that contained this inherent variability , we could not expect our classifiers to have higher accuracy than what is achievable within histopathology . generally , sgcs performed comparably to clinical diagnostic pathology . 
earlier work on mrna - based classifiers for er , pgr , and her2 has been performed with microarrays , quantitative reverse - transcriptase polymerase chain reaction , and , recently , with rna - seq and mainly has been restricted to signatures of either one16 , 31 or few23 , 24 , 26 , 32 , 33 genes . 
in each kaplan - meier plot , the histopathology to mgc concordant tumor cases are plotted in blue , the discordant tumor cases are plotted in gold , the log - rank p value is given , and the hazard ratio ( hr ) for discordant - versus - concordant result is given with a 95% ci and after multivariable ( mv ) cox regression adjustment . 
covariables included in the mv analysis were age at diagnosis , lymph node status , tumor size , and the variables denoted by the following symbols : , er , pgr , and nhg ; , er , pgr , her2 , and nhg ; , her2 and nhg ; # , er , pgr , and her2 . discrepancies between rna - seqbased classifications and histopathology may be a result of staining and reader variations , as discussed in this paper . 
 the consequence is that a mismatch between mrna biomarker prediction and histopathology may be influenced by various mechanisms active between these layers , for example rna silencing / interference / translation , protein stability and epitope availability , or tumor heterogeneity . despite these possible explanations for discrepancies , when benchmarked against patient outcome , our classifiers exemplified enhanced stratification of patients with significant differences in overall survival ( fig 3 ; appendix figs a4 and a5 )  . 
the fact that mgcs performed best overall suggests that a multigene signature captures the biologic signaling upand downstream of the biomarker in question in a more consequential way than the expression of the single gene or protein alone . 
another approach is to use clinical outcome as the training labels to develop new prognostic / predictive signatures.13 , 34 the scan - b material is excellently suited to evaluate previously published signatures ; as we accrue longer follow - up , we aim to develop rna - seq signatures trained on clinical outcomes . ki67 has been introduced relatively recently in international guidelines.11 to our knowledge , this study is the first to develop a validated predictor for ki67 status . 
the lower concordance between our ki67 predictions compared with the clinical reference is related to the relatively larger ki67 interrater disagreement seen within our consensus pathology evaluation , which is likely a consequence of the continuous nature of ki67 expression and of the spectrum of proliferation activity and pathways in bc . nhg is distinct from the other biomarkers . 
moreover , nhg prediction is a three - class proble even for pathologists , nhg can be difficult to determine , as evidenced by the moderate and oa results within clinical pathology , in line with the literature.12 most misclassified tumor cases in this study were histologically grade 1 ( g1 ) or grade 3 that were misclassified as grade 2 ( g2 ) by our predictor . 
all histologic g1 occurrences were misclassified , which may have been a result of the imbalanced composition of the training set for nhg ( 48 of 405 samples consensus - scored g1 ) , or may have occurred because g1 is not a discrete entity but rather the lower end of an underlying continuous scale . 
this approach has been suggested by others as a viable gene for expressionbased alternative to nhg translation into a clinical setting35 , 36 and essentially is what our nhg predictor has become . an important question when building classifiers is how many genes to use . 
when compared with clinical pathology , sgcs have slightly better concordance than mgcs for er and her2 , whereas the sgc and mgc performances were comparable for pgr and ki67 . 
mgcs may be more robust than sgcs , because they are able to classify tumors correctly even when the main gene that underlies a biomarker is poorly measured in a particular analysis . 
when clinical outcome was considered , the survival analyses indicated that our mgcs generally contained greater potential clinical utility than sgcs to complement histopathology . in summary , we have performed a systematic pathologic evaluation of 405 bc tumors , which resulted in consensus scores for the five conventional bc biomarkers and estimated a well - controlled bestcase scenario for the inherent uncertainty within clinical histopathology . 
classifiers based on the expression of single genes performed slightly better than mgcs for concordance to histopathology , but mgcs performed significantly better for stratification of patients into groups with clinically meaningful differences in survival , in particular for histopathologic hormone - responsive bcs . 
in conclusion , rna - seqbased classifiers may be suitable complementary diagnostics for bc , in particular for difficult diagnoses in which the classifier can add an additional vote toward the therapeutic choice . 
saal collection and assembly of data : christian brueffer , johan vallon - christersson , dorthe grabau , anna ehinger , jari hkkinen , cecilia hegardt , janne malina , jonas manjer , christer larsson , niklas loman , lisa rydn , ke borg , lao h . 
saal data analysis and interpretation : christian brueffer , johan vallon - christersson , dorthe grabau , anna ehinger , jari hkkinen , yilun chen , pr - ola bendahl , jonas manjer , martin malmberg , lisa rydn , ke borg , lao h . 
saal manuscript writing : all authors final approval of manuscript : all authors jonas manjer no relationship to disclose martin malmberg no relationship to disclose christer larsson honoraria : lilly ( i ) research funding : diamyd medical ab ( i ) travel , accommodations , expenses : lilly ( i ) niklas loman honoraria : astrazeneca consulting or advisory role : amgen lisa rydn research funding : roche ke borg honoraria : roche , astrazeneca travel , accommodations , expenses : roche , astrazeneca agree to be accountable for all aspects of the work : all authors lao h . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . christian brueffer employment : saga diagnostics ab johan vallon - christersson no relationship to disclose dorthe grabau no relationship to disclose anna ehinger no relationship to disclose jari hkkinen no relationship to disclose cecilia hegardt no relationship to disclose janne malina employment : unilabs honoraria : astrazeneca yilun chen no relationship to disclose pr - ola bendahl no relationship to disclose stock and other ownership interests : saga diagnostics patents , royalties , other intellectual property : patent filed for methods related to ultrasensitive quantification of nucleotide sequence variants . acknowledgment we thank the patients who were part of this study and the scan - b study . 
we also thank karin annersten , minerva li , inger remse , ralph schulz , jeanette valcich , cecilia wahlstrm , olle mnsson , nicklas nordborg , anna karlsson , christel reuterswrd , frida rosengren , and ingrid wilson of the scan - b laboratory and the division of oncology and pathology , lund university , for handling samples , genomic analyses , and database and administrative support , as well as cristina ciornei - karlsson for retrieving pathology slides and patient reports , daniel filipazzi and anders kvist for help with computing infrastructure , and johan staaf for help with classifier development . 
we thank the south sweden breast cancer group and all scan - b collaborators at hallands hospital halmstad , helsingborg hospital , blekinge county hospital , central hospital kristianstad , skne university hospital lund / malm , central hospital vxj , for inclusion of patients and sampling of tissue for this study , and we thank the swedish national breast cancer registry and regional cancer center south for clinical data . 
 this work is dedicated to the memory of dorthe grabau , who sadly passed away during the writing of this paper . affiliations christian brueffer , johan vallon - christersson , anna ehinger , jari hkkinen , cecilia hegardt , yilun chen , pr - ola bendahl , jonas manjer , christer larsson , niklas loman , lisa rydn , ke borg , and lao h . 
 support supported by the berta kamprad foundation and funded in part by the swedish foundation for strategic research , swedish research council , swedish cancer society , knut and alice wallenberg foundation , vinnova , governmental funding of clinical research within national health service , scientific committee of blekinge county council , crafoord foundation , lund university medical faculty , gunnar nilsson cancer foundation , skne university hospital foundation , biocare research program , king gustav vth jubilee foundation , maggie stephens foundation , royal physiographic society in lund , and the krapperup foundation . references netw 12 : 542 - 590 , 2014 1 . 
hammond meh , hayes df , dowsett m , et al : american society of clinical oncology / college of american pathologists guideline recommendations for immunohistochemical testing of estrogen and progesterone receptors in breast cancer . 
press mf , sauter g , bernstein l , et al : diagnostic evaluation of her - 2 as a molecular target : an assessment of accuracy and reproducibility of laboratory testing in large , prospective , randomized clinical trials . 
perez ea , suman vj , davidson ne , et al : her2 testing by local , central , and reference laboratories in specimens from the north central cancer treatment group n9831 intergroup adjuvant trial . 
rydn l , haglund m , bendahl p - o , et al : reproducibility of human epidermal growth factor receptor 2 analysis in primary breast cancer : a national survey performed at pathology departments in sweden . 
ekholm m , grabau d , bendahl p - o , et al : highly reproducible results of breast cancer biomarkers when analysed in accordance with national guidelines : a swedish survey with central re - assessment . 
wolff ac , hammond meh , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
saal lh , johansson p , holm k , et al : poor prognosis in carcinoma is associated with a gene expression signature of aberrant pten tumor suppressor pathway activity . 
roepman p , horlings hm , krijgsman o , et al : microarray - based determination of estrogen receptor , progesterone receptor , and her2 receptor status in breast cancer . 
saal lh , vallon - christersson j , hkkinen j , et al : the sweden cancerome analysis network breast ( scan - b ) initiative : a large - scale multicenter infrastructure towards implementation of breast cancer genomic analyses in the clinical routine . 
hkkinen j , nordborg n , mnsson o , et al : implementation of an open source software solution for laboratory information management and automated rnaseq data analysis in a large - scale cancer genomics initiative using base with extension package reggie . 
kun y , how lc , hoon tp , et al : classifying the estrogen receptor status of breast cancers by expression profiles reveals a poor prognosis subpopulation exhibiting high expression of the erbb2 receptor . 
viale g , slaets l , bogaerts j , et al : high concordance of protein ( by ihc ) , gene ( by fish ; her2 only ) , and microarray readout ( by targetprint ) of er , pgr , and her2 : results from the eortc 10041 / big 03 - 04 mindact trial . 
wilson tr , xiao y , spoerke jm , et al : development of a robust rna - based classifier to accurately determine er , pr , and her2 status in breast cancer clinical samples . 
cieslik m , chugh r , wu ym , et al : the use of exome capture rna - seq for highly degraded rna with application to clinical cancer sequencing . 
 appendix all patients with breast cancer in the south sweden health care region diagnosed between september 1 , 2010 , and march 31 , 2015 who underwent operation for invasive primary * breast cancer ( n = 5 , 892 ) not enrolled ( n = 791 ) patients enrolled in scan - b ( n = 5 , 101 : 87% ) no tumor tissue for study ( n = 1 , 205 ) or tumor tissue obtained after neoadjuvant therapy or previous biopsy ( n = 49 ) enrolled patients with tumor biopsy sample for analysis ( n = 3 , 847 : 75% ) validation cohort with quality controlled rna - seq data ( n = 3 , 273 : 85% ) insufficient or poor quality rna and rna - seq not performed or failed ( n = 464 ) ; rna - seq data failed qc ( n = 110 ) fig a1 . 
for estrogen receptor ( er ) , progesterone receptor ( pgr ) , human epidermal growth factor receptor 2 ( her2 ) , and ki67 clinical histopathology diagnostic results ( y - axis ) , the single - gene classifier ( sgc ) gene expression ( x - axis ) ( a ) or the transformed multigene classifier ( mgc ) score ( x - axis ) ( b ) is plotted for the validation cohort ( circles )  . 
transformed multigene classifier ( mgc ) score ( x - axis ) versus single gene classifier ( sgc ) gene expression ( y - axis ) in the 3 , 273 samples of the independent validation cohort ( circles ) for ( a ) estrogen receptor ( er ) , ( b ) progesterone receptor ( pgr ) , ( c ) human epidermal growth factor receptor 2 ( her2 ) , and ( d ) ki67 . 
vertical dashed lines are drawn at the mgc score threshold of 0 to distinguish the classes , and horizontal dotted lines are drawn at the sgc gene expression thresholds determined from the training cohort . 
kaplan - meier overall survival estimates for histopathology , single - gene classifiers ( sgcs ) , and multigene classifiers ( mgcs ) within the validation cohort ( neg , classified as negative ; pos , classified as positive ; grade [ g ] 1 , g2 , or g3 )  . 
the biomarker is indicated at the far left , and the number of tumor cases with complete data across pathology , sgc , and mgc for a given biomarker is shown below each biomarker name . 
in columns are plotted the kaplan - meier survival curves for each classification : ( left ) pathology , ( middle ) sgc , and ( right column ) mgc . 
the log - rank p value is displayed , and horizontal dashed lines are drawn to aid identification of kaplan - meier estimates with the poorest outcome classification group within each row . 
at risk : concordant hormone nonresponsive concordant hormone responsive path hormone nonresponsive / mgc hormone responsive path hormone responsive / mgc hormone nonresponsive log - rank p < .001 concordant hormone nonresponsive concordant hormone responsive pathology hormone nonresponsive / mgc hormone responsive pathology hormone responsive / mgc hormone nonresponsive time ( years ) 2 , 310 2 , 302 2 , 262 1 , 946 1 , 413 fig a5 . 
kaplan - meier overall survival estimates for groups defined by pathology ( path ) versus multigene classifiers ( mgcs ) within the validation cohort ; the log - rank p value is given . 
survival curves , number of samples classied as tmb high , and predicted neoantigens were used to evaluate the differences between thresholds . results the distribution of tmb varied dramatically among cancer types . 
2019 by american society of clinical oncology introduction immunotherapy ; immunotherapy , especially checkpoint inhibition , has been added recently as a successful treatment option for some patients with cancer . 
it is based on the presence of neoantigens eliciting a response from t cells by recognizing these antigens as foreign and inltrating the tumor microenvironment.1 , 2 however , only a subset of patients respond to checkpoint inhibitor therefore , predictive biomarkers are critical to guide the selection of patients for these therapies . 
although high - level programmed death - ligand 1 expression , microsatellite instability , and mismatch - repair deciency have been deemed including tumor clinically relevant , other markers , mutational burden ( tmb ) , interferon gamma prole , and human leukocyte antigen ( hla ) genotype , have also exhibited promising results.3 tmb is commonly dened as the total number of somatic mutations in a tumor genome , divided by the number of bases sequenced in megabases ( mb ) .4 , 5 previously , patients with higher tmb ( tmb high ) demonstrated increased response to immunotherapy compared with patients with lower tmb ( tmb low ) , especially in nonsmallcell lung cancer.6 , 7 however , no consensus has been established to dene a standard threshold for tmb high . 
last , previous studies have adopted panel target sequencing with small regions of genomic dna , possibly excluding neoantigen candidates.8 therefore , exploring the tmb distribution with more extensive sequencing platforms , such as whole exome sequencing ( wes ) , can provide a more comprehensive view of tmb . 
 fernandez et al context threshold ? key objective can a cancer - specic tumor mutational burden ( tmb ) provide more useful information compared with a xed pan - cancer knowledge generated a cancer - specic tmb threshold can dynamically adjust to identify dramatically more patients as tmb high compared with a restrictive pan - cancer threshold . 
the additional patients do not have a signicantly different outcome compared with the other tmb - high patients . relevance when interpreting a patients tmb , the overall tmb seen in the specic cancer type should be taken into consideration to give the tmb context . reect tmb in each cancer type , the wcm threshold uses interquartile range ( iqr ) : mean ( tmb ) + 1.25 iqr ( tmb ) applied within each cancer , meaning each cancer type will have its own threshold reective of the distribution of mutations within that cancer type . 
predicted neoantigens for tcga samples were obtained through the cancer immunome atlas.23 tmb calculation tmb was calculated as the total number of nonsynonymous mutated bases in the tumor genome divided by the mb of the genome covered . 
the wcm advanced cohort was sequenced using our exact - 1 wes haloplex pipeline using tumor - normal pairs , 24 which covers 37 mb of the genome . samples were collected under a protocol approved by the institutional review board of weill cornell medical college , and written informed consent was obtained . 
because tmb is divided by the total size of genome sequenced to help adjust for technical batch effects , the size of sequenced regions was determined for each tcga cohort according to their respective publications.11 - 22 samples with purity of less than 50% according to absolute ( tcga ) or clonality estimate in tumors ( exact - 1 ; weill cornell medine clinical genomics lab , new york , ny ) were removed.25 , 26 germline variants and variants appearing in the exome aggregation consortium database with a frequency of at least 1% were removed to lter them out.27 variants with a variant allele frequency ( vaf ) of less than 10% were ltered out after correcting vaf for tumor purity by dividing vaf by purity . 
a summary of ltering steps can be seen in the data supplement . mutational signatures mutational signatures were determined using the deconstructsigs r package.28 for each sample , a matrix containing the frequency a mutation appears within a trinucleotide context was generated . 
this matrix was compared with the signatures published previously in the catalogue of somatic mutations in cancer , 29 resulting in signature contributions . statistical methods the wilcoxon rank sum test was used to compare sample distributions . 
for example , the tmb for prostate cancer in tcga ranged from 0.03 mutations / mb to 14.13 distribution of tmb for tcga samples cancer type distribution of tmb for wcm advanced samples threshold chalmers et al threshold chalmers et al cancer type fig 1 . 
however , the tmb for bladder cancer in tcga ranged from 0.04 mutations / mb to 99.68 mutations / mb , with a mean of 6.92 mutations / mb ( n = 375 )  . because of the higher frequency of metastatic samples in the wcm advanced cohort , we sought to understand how the distribution of tmb changes between primary and metastatic samples . 
the chalmers et al threshold is a constant cutoff of 20 mutations / mb for all cancer types , 4 whereas our custom wcm threshold is a formula of mean ( tmb ) + 1.25 iqr ( tmb ) , adapted from a study by zehir et al.5 the wcm threshold was applied per cancer to account for the variation in tmb among cancer types . data for patients treated with immunotherapy were not available for either cohort ; however , tcga survival outcomes were investigated to understand the differences in survival between tmb high and tmb low using both thresholds . 
tmb - high patients showed signicantly improved survival compared with tmb - low patients for blca using both the wcm threshold ( log - rank p value = .0014 ) and the chalmers et al threshold ( log - rank p value = .009 ; data supplement )  . 
lusc showed improved survival for tmb - high patients compared with tmb - low patients when using the wcm cutoff ( log - rank p value = .036 ) but not when using the chalmers et al cutoff ( log - rank p value = .11 ; data supplement )  . 
ucec also showed signicantly improved survival for tmb - high patients compared with tmb - low patients when using chalmers et al ( log - rank p value = .023 ) but did not reach signicance when using wcm ( log - rank p value = .055 ; data supplement )  . 
to further compare the performances of the two thresholds , timedependent roc curves were created at the 5 - year time point ( fig 2d ; data supplement )  . 
to explore the difference between the patients selected by the thresholds , we split the samples into three groups : tmb high , wcm - tmb high , and tmb low . 
the wcm - tmbhigh group contained samples classied as tmb high by wcm and tmb low by chalmers et al ( when chalmers et al had more tmb high classications [ ucec ] than wcm , we used chalmers - tmb high [ chm - tmb high ] )  . 
the tmb - low group contained samples classied as tmb low by both methods ( fig 2a )  . the wcm - tmbhigh group did not attain signicantly improved survival compared with the tmb - low group for blca ( log - rank p value = .072 ; fig 2b )  . 
the chalmers et al threshold did not classify any patients with kirc as tmb high . although the survival trends were not signicantly different between the cutoffs , the number of samples classied as tmb high differed between thresholds . 
out of 14 tcga cancer types investigated , eight cancers had a statistically larger tmb - high group for wcm compared with chalmers et al ( blca [ fold change = 1.9 ] , brca [ fold change = 6.7 ] , gbm [ fold change = 2.7 ] , kirc [ no high by chalmers ] , lgg [ fold change = 13.0 ] , ov [ fold change = 5.67 ] , prad [ no high by chalmers ] , and thca [ no high by chalmers ] ) ; ve cancers had no statistically signicant change in the number of tmb - high classications ( coad , kich , luad , lusc , and read ) ; and only ucec had a large number of tmb high classied by chalmers et al compared with wcm ( 2 test with yatess continuity correction ; p value , .05 ; fig 3a )  . 
predicted neoantigens from the cancer immunome atlas compared the tmbhigh , the wcm - tmbhigh , and the tmb - low groups for tcga samples ( fig 4a ) .23 the tmb - low group had signicantly fewer neoantigens than both the tmb - high ( wilcoxon p value , 2.3e - 16 ) and wcm - tmbhigh ( wilcoxon p value = 2.1e - 14 ) group . 
kaplan - meier survival curves comparing the tmb classications between the weill cornell medicine ( wcm ) threshold and the chalmers et al threshold for ( b ) blca and ( c ) kirc . 
for kirc , the chalmers et al threshold was too high to classify any samples as tmb high , resulting in only two groups : wcm - tmb high and tmb low . 
 ( d ) time - dependent receiver operating characteristic ( roc ) curve comparing the true positive ( tpr ) and false positive ( fpr ) rates for blca using both the chalmers et al threshold and the wcm threshold shows the area under the curve ( auc ) for both cutoffs at 5 years from diagnosis . 
because of the observed variation in tmb among cancer types , neoantigens were also compared between the tmb groups for each cancer ( figs 4b and 4c ; data supplement )  . 
prostate adenocarcinoma ( prad ) and kidney renal clear cell carcinoma ( kirc ) are excluded from the plot because the chalmers et al threshold did not classify any samples as tmb high . 
blue bars represent cancer types with a higher or equal number of tmb - high classications for the weill cornell medicine ( wcm ) threshold than the chalmers et al threshold . 
overall , the tmb - high and wcm - tmbhigh groups showed increased neoantigen counts compared with the tmb - low group . finally , mutational signatures were compared among tmb groups . 
distribution of predicted neoantigens for tmb high ( blue ) , tmb high weill cornell medicine ( wcm ; red ) , and tmb low ( teal ) for the cancer genome atlas ( tcga ) shown for ( a ) all cancers pooled together , ( b ) lung adenocarcinoma ( luad ) , and ( c ) bladder urothelial carcinoma ( blca )  . 
 ( a ) violin plots showing the distribution of the contribution of signature 10 ( defective polymerase - ) in tumor mutational burden ( tmb ) high , chalmers ( chm ) - tmb high , and tmb low . 
 ( b ) pca showing the signature contributions for uterine corpus endemetrial carcinoma ( ucec ) with tmb - high samples in blue , wcm - tmbhigh samples in red , and tmb - low samples in teal . 
only signatures 2 , 4 , 6 , 10 , 13 , 15 , 20 , 21 , and 26 were considered , to focus on signatures with the most relevant interpretations . 
for example , the chalmers et al cutoff of 20 mutations / mb is higher than the maximum tmb seen within tcga prostate cancer ( 14.13 mutations / mb ) ; however , using a lower threshold might be too lenient for tcga bladder cancer ( maximum tmb of 99.68 mutations / mb )  . 
the dramatic difference in tmb among cancer types led us to explore a tmb threshold applied in a cancer - specic manner . to a cancer - specic when comparing a pan - cancer threshold , we found we were able to maintain differences in survival trends between tmb high and tmb low , often while including more patients in the tmb - high group by using the cancer - specic threshold . 
using a tmb threshold that has a larger number of tmb - high classications while not having signicantly different survival trends than a more stringent threshold can potentially open treatment options to patients if they can be shown to respond well . 
hr , hazard ratio ; os , overall survival ; wcm , weill cornell medicine . seen in recent publications suggests that tmb alone is not a critical predictor of survival for nonimmunotherapy treatment response.6 , 37 , 38 differences in tmb distribution between the tcga and wcm advanced cohorts could be a result of biologic or technical differences . 
tcga contains primary tumor samples , and wcm advanced contains mostly metastatic tumor samples . when comparing different cohorts of patients , many technical differences can inuence tmb , making a static threshold potentially less accurate . 
after sequencing , the exact - 1 pipeline and tcga pipeline use different mutation callers and apply different quality lters . in addition , when comparing tmb among studies , it is important to understand the variants that were considered . 
 fernandez et al calculating tmb.6 , 38 , 39 targeted panels cover different genes and sizes of the genome and at a higher sequencing depth than wes , inuencing the estimated distribution of tmb . 
the panel must cover at least 2 mb of the genome to have high sensitivity and specicity when measuring tmb.8 a static threshold would not be able to adjust to the differing levels of tmb resulting from different panels . 
however , a dynamic threshold would be able to adjust for technical differences . the cancer - specic threshold adjusted for the variation in tmb ; however , the pan - cancer threshold classied more patients as tmb high for ucec . 
mutational signatures for these samples showed a cluster of patients with pole deciency , which led to a large number of mutations and a tmb distribution with a large iqr , 22 causing the cancerspecic threshold to be strict in this case . the survival analyses in this study were limited by a lack of patients undergoing immunotherapy treatment . 
in addition , the number of predicted neoantigens was compared per cancer , showing that a cancer - specic threshold identies patients with a higher number of neoantigens compared with tmb - low patients . moreover , tmb might depict only one factor in the success of immunotherapy . 
a recent study has shown that patients with melanoma and nonsmall - cell lung cancer with heterozygous hla class i exhibit improved survival compared with patients who are homozygous.40 because of the limitation of tcga data , we could not examine the role of hla class i in the current study . 
fernandez employment : celgene travel , accommodations , expenses : foundation medicine himisha beltran consulting or advisory role : janssen oncology , genzyme , glaxosmithkline , abbvie , astellas pharma , astrazeneca research funding : janssen ( inst ) , abbvie / stemcentrx ( inst ) , eli lilly ( inst ) travel , accommodations , expenses : janssen oncology bishoy m . 
faltas honoraria : digital science press publications research funding : eli lilly juan miguel mosquera research funding : personal genome diagnostics travel , accommodations , expenses : personal genome diagnostics david m . 
hoffmann la roche ag , novartis , astellas pharma research funding : eli lilly , janssen , millenium pharmaceuticals , sano patents , royalties , other intellectual property : us patent ( 7 , 767 , 393 and 7 , 229 , 774 ) , expression prole of prostate cancer , 2007 ; us patent ( 7 , 332 , 290 ) , detection of amacr cancer markers in urine , 2008 ; us patent ( 7 , 718 , 369 ) , recurrent gene fusions in prostate cancer , 2010 ; us patent ( 7 , 803 , 552 and 7 , 666 , 595 ) , biomarkers for predicting prostate cancer progression , 2010 ; us patent ( 7 , 981 , 609 b2 ) , methods for identifying and using snp panels , 2011 ; us patent ( 8 , 106 , 037 b2 ) , identication and treatment of estrogen responsive pca , 2012 ; us patent ( 9 , 090 , 899 b2 ) , methods of diagnosing and treating prostate cancer characterized by ndrg1 - erg fusion , 2015 ; us patent ( 9 , 458 , 213 b2 ) , compositions and methods for diagnosing prostate cancer based on detection of slc45a3 - elk4 fusion transcript , 2016 ; us patent ( 9 , 568 , 483 b2 ) , molecular subtyping , prognosis and treatment of prostate cancer , 2017 ; us patent ( 9 , 678 , 077 b2 ) , erg / tff3 / hmwck triple immunostain for detection of prostate cancer , 2017 ; us patent ( 61 , 408 , 341 ) , exploration of novel gene fusion in prostate cancer by rna - seq travel , accommodations , expenses : f . 
shah consulting or advisory role : astellas pharma , eli lilly japan research funding : gilead sciences ( inst ) , merck ( inst ) , boston biomedical ( inst ) , oncolys biopharma ( inst ) , bristol - myers squibb ( inst ) wei song employment : genentech ( i ) employment : cytokinetics ( i ) honoraria : foundation medicine , loxo consulting or advisory role : foundation medicine , loxo no other potential conicts of interest were reported . acknowledgment we thank juan sebastian andrade martinez for his previous work with the wcm advanced cohort and bhavneet bhinder for her advice on predicted neoantigens . references 2018 topalian sl , weiner gj , pardoll dm : cancer immunotherapy comes of age . 
j clin oncol 29 : 4828 - 4836 , 2011 topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of anti - pd - 1 antibody in cancer . 
n engl j med 366 : 2443 - 2454 , 2012 tray n , weber js , adams s : predictive biomarkers for checkpoint immunotherapy : current status and challenges for clinical application . 
cancer immunol res 6 : 1122 - 1128 , 2018 chalmers zr , connelly cf , fabrizio d , et al : analysis of 100 , 000 human cancer genomes reveals the landscape of tumor mutational burden . 
genome med 9 : 34 , 2017 zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
n engl j med 378 : 2093 - 2104 , rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
lancet 387 : 1909 - 1920 , 2016 buchhalter i , rempel e , endris v , et al : size matters : dissecting key parameters for panel - based tumor mutational burden analysis . 
plimack er , dunbrack rl , brennan ta , et al : defects in dna repair genes predict response to neoadjuvant cisplatin - based chemotherapy in muscle - invasive bladder cancer . 
biometrics 56 : 337 - 344 , 2000 johnson db , frampton gm , rioth mj , et al : targeted next generation sequencing identies markers of response to pd - 1 blockade . 
rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
 no evidence of increased risk of breast cancer in women with lynch syndrome identied by multigene panel testing jessica stoll , ms , cgc1 ; eric rosenthal , scm , phd2 ; shelly cummings , ms , cgc2 ; jamie willmott , ms , cgc2 ; ryan bernhisel , mstat2 ; and sonia s . 
kupfer , md1 purpose prior estimates of breast cancer risk in women with lynch syndrome ( ls ) range from population risk to 18 - fold increased risk with reported differences by gene . 
standardized incidence ratios ( sirs ) and 95% cis of breast cancer were calculated compared with age - matched incidence in the general us female population and with women negative for pvs stratied by the test indication . results in total , 0.8% of women ( 30 , 362 of 441 , 966 women ) carried mmr gene pvs . 
women with pvs in pms2 and msh6 were tested more frequently for hboc , whereas those with pvs in mlh1 and msh2 / epcam were tested more frequently for ls . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction breast cancer risk in lynch syndrome ( ls ) has been debated , with published data indicating anywhere from no increased risk1 - 4 up to 18 - fold increased risk for women with a pathogenic variant ( pv ) in a mismatch repair ( mmr ) gene.5 - 9 a recent laboratorybased study reported a 2to 3 - fold increased incidence of breast cancer in women with pvs in msh6 and pms2 compared with the general us female population , but not in mlh1 or msh2 carriers.10 these authors used us female population data from the seer registry ; however , comparing cancer histories in a population heavily weighted toward women being assessed for hereditary breast and ovarian cancer ( hboc ) to cancer histories in the general population could result in ascertainment bias.11 - 13 specically , this approach likely increases the proportion of the sample with a personal diagnosis of breast cancer , resulting in elevated breast cancer rates regardless of mmr gene status . 
this ascertainment bias might be less evident for women with pvs in the higher penetrance mmr genes ( ie , mlh1 , msh2 , and epcam ) who are more likely to be ascertained for testing on the basis of personal or family history of early - onset colorectal or endometrial cancer or other ls - associated cancers . therefore , to properly estimate cancer risk , women with pvs should be compared with pv - negative women within the same testing population . quantifying breast cancer risk in women with ls has signicant implications for screening and risk reduction , especially for patients with ls caused by pvs in msh6 and pms2 , which are more prevalent than previously thought . 
 stoll et al context key objective using a large , laboratory - based database , we determined whether women with lynch syndrome ( ls ) are at increased risk of breast cancer compared with the general population and to a population undergoing genetic testing . knowledge generated women with ls are not at increased risk of breast cancer . 
these ndings are in line with results from the prospective ls database but contrast with other laboratory - based studies . relevance these ndings support average - risk breast cancer screening in women with ls . ascertained for suspicion of hboc and / or ls but were not found to have a pv by multigene panel testing . methods study population women tested with a single commercial laboratorys ( myriad genetic laboratories , salt lake city , ut ) multigene panel between september 2013 and november 2018 were included unless they resided in a state prohibiting use of deidentied genetic or clinical information for research . 
clinical and demographic data for participants were obtained from test request forms submitted by ordering health care providers . ls - associated cancers included colorectal , endometrial , ovarian , pancreatic , stomach , gastric , ureter , brain , small intestine , and biliary tract cancers . 
hboc - associated cancers included breast , ovarian , prostate , and pancreatic cancers . testing criteria individuals met providers indicated on the test requisition forms whether testing was ordered for suspicion of ls or hboc . 
for hboc , 2013 national comprehensive cancer network ( nccn ) guidelines were used , 14 but the contribution of prostate cancer was excluded because gleason score or metastatic disease information was not collected reliably . these exclusions were not expected to substantially inuence results but may have resulted in an underestimate of the number of women meeting hboc criteria . 
to directly evaluate rates against the recent publication that established a 2to 3fold elevated breast cancer incidence for msh6 and pms2 , 10 the us female population from the seer registry17 was used as one comparator group . 
to compensate for the ascertainment bias expected in a population selected for testing on the basis of suspicion of hereditary cancer risk , we also calculated the sirs using the following 3 additional comparator populations : women who tested negative for any pv who were ascertained for suspicion of hboc or ls ; women who were ascertained for hboc only ; and women who were ascertained for ls only . 
all analyses were performed using sas software ( sas institute , cary , nc )  . results demographic and clinical characteristics in total , 441 , 996 women met inclusion criteria ( appendix table a1 )  . 
among these , 3 , 362 women ( 0.8% ) were found to carry a single pv in an mmr gene ( mlh1 , msh2 , msh6 , pms2 , or epcam ) , and 438 , 634 women ( 99.2% ) were negative for pvs in any of the other genes included on the panel . 
epcam deletions were identied in only 11 women and therefore were included with msh2 for all analyses . demographic and clinical characteristics for women with mmr gene pv and all women tested are listed in table 1 . for women with an mmr gene pv , median age at testing was 47 years , and 56.8% of women reported white or caucasian ancestry . 
demographic and clinical characteristics of women with mmr gene pvs and all women undergoing multigene panel testing all women tested ( n = 441 , 996 ) women with mmr gene pv ( n = 3 , 362 ) characteristic age at testing , yearsa mean ( sd ) range mean ( sd ) range age at bc diagnosis , yearsb self - reported ancestry , no . 
similar differences in mutation spectrum were found for women meeting nccn testing criteria for ls versus hboc ( fig 1 )  . the majority of mlh1 and msh2 / epcam mutation carriers were ascertained for clinical suspicion of ls , whereas msh6 and pms2 mutation carriers were more commonly ascertained for suspicion of hboc ( fig 2 )  . phenotypic spectrum the majority of women with pvs in mlh1 and msh2 / epcam were affected by cancer , whereas most pms2 carriers were unaffected . 
for msh2 / epcam carriers , endometrial and colorectal cancers were the most common cancers reported ( n = 162 [ 24.8% ] and n = 150 [ 23.0% ] , respectively )  . 
carriers of mlh1 and msh2 / epcam pvs had lower rates of breast cancer , whereas there was no difference in sirs for msh6 or pms2 carriers compared with seer population breast cancer rates ( table 2 )  . table 3 lists sirs for women with mmr gene pvs compared with women with negative panel testing . 
when all women ascertained for hboc or ls were analyzed , breast cancer rates were lower in women with pvs in mmr genes . specically , breast cancer rates ranged from 22% to 50% lower than expected among the various mmr genes . 
similarly , when compared with women ascertained for suspicion of ls , breast cancer rates also did not differ between women with mmr gene pvs compared with pv - negative women . 
distribution of pathogenic variants ( pvs ) by mismatch repair gene on the basis of ascertainment for testing indicated by ordering provider and testing criteria met ( mlh1 , n = 462 ; msh2 / epcam , n = 653 ; msh6 , n = 985 ; pms2 , n = 1 , 262 )  . 
prevalence of mismatch repair pathogenic variants by ascertainment for lynch syndrome ( ls ) and hereditary breast and ovarian cancer syndrome ( hboc ) testing as indicated by ordering provider ( mlh1 , n = 462 ; msh2 / epcam , n = 653 ; msh6 , n = 985 ; pms2 , n = 1 , 262 )  . discussion data from multigene panel testing in ls have called into question the unresolved issue of whether breast cancer risk is increased in ls . 
although there is a wealth of existing literature on breast cancer in ls , data from these studies are conicting , with risk estimates ranging from no increased risk1 - 4 up to 18 - fold increased risk.5 - 9 recent studies report an increased breast cancer risk in women with pvs in msh6 and pms2 , but not in mlh1 and msh2 / epcam , 10 or an increased risk of breast cancer exclusive to msh6.19 in the present laboratory - based study , including a large sample of msh6 and pms2 pv carriers , previously published data showing an increased breast cancer risk in women with pvs in msh6 and / or pms2 were not replicated when the same methodology was used.10 moreover , the rate of breast cancer was found to be lower than expected among mlh1 and msh2 / epcam carriers . 
findings from the current study are in line with a recent report from the prospective ls database.20 the ndings in the current study likely differ from previous studies showing increased breast cancer risk in ls for several reasons . 
first , the current study includes the largest number of mmr gene pv carriers reported to date , including large numbers of msh6 and pms2 carriers , thereby increasing precision in breast cancer risk estimates compared with more moderately sized studies . 
moreover , this sample included a large proportion of women unaffected by cancer , which appropriately shifts the breast cancer estimates closer to those of the general us female population . colon endometrial breast ovarian other * unaffected mlh1 msh2 / epcam msh6 pms2 no mutation fig 3 . 
in these analyses , no difference in breast cancer incidence was found among women with or without mmr gene pvs whether they were ascertained for suspicion of hboc or ls . 
these results support current guidelines to follow average - risk breast cancer screening recommendations in all women with ls.22 consistent with ndings from other laboratory and population - based studies , these data demonstrate that pvs in msh6 and pms2 account for a much higher proportion of ls than previously estimated.10 , 23 also similar to previous studies , 23 , 24 this study found that the current ls testing criteria perform reasonably well for women with pvs in mlh1 and msh2 but miss close to half of women with pvs in msh6 and pms2 . 
 no increased breast cancer risk in lynch syndrome these results suggest that current clinical criteria are insufcient for identication of the full spectrum of patients with ls who would benet from appropriate surveillance.25 one limitation inherent to utilization of a laboratory - based testing population is that clinical information was limited to that which was included on the test requisition form as provided by ordering clinicians and therefore may not be wholly inclusive of individuals personal and family histories . 
however , we obtained essentially the same ndings through comparisons between different populations within this study , suggesting that underor overreporting of cancer history in any of these populations did not affect the ndings . 
although the study was designed specically to address ascertainment bias , the population included only women undergoing genetic testing for clinical suspicion of a hereditary cancer syndrome and may not be representative of the more general population with ls . however , this was at least in part mitigated by the fact that the comparator population was from the same testing population to ensure that any population differences between women with and without pvs were valid . in the largest study of mmr gene pv carriers identied by a multigene panel through a commercial laboratory , there was no evidence of increased breast cancer risk in women with pvs in mmr genes compared with the general us female population or with woman undergoing multigene panel testing . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . jessica stoll consulting or advisory role : invitae travel , accommodations , expenses : invitae eric rosenthal employment : myriad genetic laboratories stock and other ownership interests : myriad genetic laboratories shelly cummings employment : myriad genetics stock and other ownership interests : myriad genetics travel , accommodations , expenses : myriad genetics jamie willmott employment : myriad genetics stock and other ownership interests : myriad genetics research funding : myriad genetics travel , accommodations , expenses : myriad genetics ryan bernhisel employment : myriad genetics sonia s . 
kupfer honoraria : advance medical no other potential conicts of interest were reported . references baglietto l , lindor nm , dowty jg , et al : risks of lynch syndrome cancers for msh6 mutation carriers . 
j natl cancer inst 102 : 193 - 201 , 2010 pande m , wei c , chen j , et al : cancer spectrum in dna mismatch repair gene mutation carriers : results from a hospital based lynch syndrome registry . 
mller p , sepp al a tt , bernstein i , et al : cancer risk and survival in path_mmr carriers by gene and gender up to 75 years of age : a report from the prospective lynch syndrome database . 
gut 67 : 1306 - 1316 , 2018 therkildsen c , ladelund s , smith - hansen l , et al : towards geneand gender - based risk estimates in lynch syndrome ; age - specic incidences for 13 extracolorectal cancer types . 
 stoll et al oliveira ferreira f , napoli ferreira cc , rossi bm , et al : frequency of extra - colonic tumors in hereditary nonpolyposis colorectal cancer ( hnpcc ) and familial colorectal cancer ( fcc ) brazilian families : an analysis by a brazilian hereditary colorectal cancer institutional registry . 
fam cancer 3 : 41 - 47 , 2004 scott rj , mcphillips m , meldrum cj , et al : hereditary nonpolyposis colorectal cancer in 95 families : differences and similarities between mutation - positive and mutation - negative kindreds . 
win ak , young jp , lindor nm , et al : colorectal and other cancer risks for carriers and noncarriers from families with a dna mismatch repair gene mutation : a prospective cohort study . 
j clin oncol 30 : 958 - 964 , 2012 goldberg m , bell k , aronson m , et al : association between the lynch syndrome gene msh2 and breast cancer susceptibility in a canadian familial cancer registry . 
harkness ef , barrow e , newton k , et al : lynch syndrome caused by mlh1 mutations is associated with an increased risk of breast cancer : a cohort study . j med genet 52 : 553 - 556 , 2015 genet med 20 : 1167 - 1174 , 2018 10 . 
2018 : is breast cancer truly caused by msh6 and pms2 variants or is it simply due to a high prevalence of these variants in the population ? genet med 21 : 256 - 257 , 2019 12 . 
evans dg , woodward er , lalloo f , et al : are women with pathogenic variants in pms2 and msh6 really at high lifetime risk of breast cancer ? genet med , 2018 13 . 
dominguez - valentin m , sampson jr , sepp al a tt , et al : cancer risks by gene , age , and gender in 6350 carriers of pathogenic mismatch repair variants : findings from the prospective lynch syndrome database . 
giardiello fm , allen ji , axilbund je , et al : guidelines on genetic evaluation and management of lynch syndrome : a consensus statement by the us multisociety task force on colorectal cancer . 
klein , md2 purpose to assess the association between the oncotype dx genomic prostate score ( gps ) result and longterm oncological outcomes following radical prostatectomy ( rp )  . methods we evaluated the association of the gps result assayed from the index lesion from rp tissue with the risk of distant metastases ( dm ) and prostate cancerspecic mortality ( pcsm ) over the 20 years following rp in a stratied cohort sample of 428 patients from 2 , 641 treated between 1987 and 2004 . 
exploratory analysis using presurgical parameters and the gps test as prognostic variables was performed to assess the additional value of the gps test on 20 - year risk of dm and pcsm . 
model discrimination was measured using the area under the receiver operating characteristic curve . results the gps test appears to be independently associated with both 20 - year risk of dm and pcsm with a low false discovery rate . 
accuracy of models including clinical risk factors alone appeared to improve when including the gps test in assessing risk of both end points . conclusion the results suggest that the gps test provides information on the risk for the meaningful long - term outcomes of dm and pcsm . jco precis oncol 5 : 442 - 449 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction long - term cancer outcomes are an important consideration when deciding between active surveillance ( as ) and immediate treatment for newly diagnosed prostate cancer . 
multiple prospective as studies that predominantly include patients at the lowest risk of progression have demonstrated a low risk of distant metastasis ( dm ) and prostate cancerspecic mortality ( pcsm ) with extended follow - up.1 , 2 however , these excellent outcomes with as require strict selection criteria and stringent follow - up with frequent repeat prostate biopsies . 
based on these studies , the current use of as for newly diagnosed men is increasing and now includes expanded selection criteria , including younger men with longer life expectancy and those with biopsy - dened pathologic features that fall outside eligibility criteria of older studies.3 it is long - term as outunknown whether the excellent comes observed for low - risk disease can be maintained in this expanded group using only traditional clinical variables and existing surveillance strategies . for example , although both pivot and protect showed no statistically signicant difference in pcsm between observation and immediate treatment intermediate - risk patients with up to a 12.7 - year followup , 4 , 5 the condence intervals for the hazard ratio ( hr ) do not exclude substantial benet of radical prostatectomy ( rp )  . 
furthermore , the long - term results of scandinavian prostate cancer group trial 4 demonstrated an 11.7% absolute risk reduction in pcsm with rp , corresponding to a relative risk of 0.55 , compared with conservative management.6 with up to a 29 - year follow - up , the results of this study are more reective of the lifetime risk of cancer recurrence and death in men with intermediateor high - risk features . 
 gps assay associated with long - term prostate cancer outcomes context key objective localized prostate cancer has an extended natural history , making immediate treatment decisions difcult without the understanding of long - term cancer risks . 
we sought to evaluate the association between the genomic prostate score ( gps ) test and long - term prostate cancer outcomes : distant metastasis and prostate cancerspecic mortality following radical prostatectomy . knowledge generated the gps test appeared to be associated with both distant metastasis and prostate cancerspecic mortality at a 20 - year followup in both univariable and multivariable models , where model discrimination was improved when the gps results were included . relevance the use of the gps test can provide risk assessment of long - term prostate cancer outcomes , beyond clinical factors alone , for patients with localized prostate cancer . traditionally used clinical information in assessing risk of adverse pathology ( ap ) at rp.7 , 8 van den eeden et al9 established the association of the gps test with risk of dm and pcsm over 10 years . 
in this report , we sought to evaluate whether the gps test is also associated with 20 - year risk of dm and pcsm and whether its use improves risk assessment for these end points compared with clinical variables alone . methods using a stratied cohort sampling design , so that a weighted analysis of the study cohort is representative of all patients ( n = 2 , 641 ) who underwent rp between 1987 and 2004 at our institution , we selected 501 patients for inclusion . 
among the remaining 441 patients , the nal analysis cohort comprised the 428 patients with evaluable primary gleason pattern in prostatectomy tissue ( fig 1 )  . all patients were selected from our prospective institutional review board ( irb ) approved database that includes clinical staging , pathology from biopsy and rp , and followup information . 
follow - up and outcome data were obtained through subsequent clinic visits , telephone calls , and semiannual follow - up letters obtained through august 1 , 2019 , approximately 10 years after the previously reported cutoff.7 multiple data reviews and quality checks were performed to ensure delity of the data set . high grade at rp was dened as grade group 3 or above ( gleason score 4 + 3 or higher )  . 
the time to event in patients who died without an event or who were alive without an event at the end of follow - up was considered censored in these analyses . 
each patient was weighted using the inverse sampling fraction in his stratulin and weis robust variance estimate was used.12 in the multivariable analysis , the gps result , preoperative prostatespecic antigen ( psa ) , clinical stage , and biopsy grade were used as covariables . 
the hr for continuous gps results was reported per 20 - gps unit increase , which approximated the difference between the average gps value in the highest 25% and the average gps value in the lowest 25% of patients based on the gps value distribution from previous studies.7 , 13 preoperative psa value was included in the model as log2 ( psa value )  . 
characteristics of the patients in the cohort sample biopsy gleason grade , % brooks et al 61 ( 6 ) 62 ( 57 - 66 ) mean ( sd ) median ( iqr ) race , % white black / afro - caribbean asian / hispanic / others year of surgery , % surgical gleason grade results clinical tumor stage , % pathologic tumor stage % 3 + 4 3 + 5 4 + 3 4 + 5 5 , 5 + 4 low / very low intermediate high 1987 - 1989 1990 - 1994 1995 - 1999 2000 - 2004  . 
summary statistics and percentages are estimated using cohort sampling weights so they estimate the distribution of characteristics in the full cohort of 2 , 641 patients from which the cohort sample ( n = 428 ) was drawn . abbreviations : aua , american urological association ; psa , prostate - specic antigen . for overoptimism of effect estimates involving the gps test . therefore , all estimates using the gps test as a covariable were corrected for regression to the mean ( rm ) 14 and false discovery rates ( fdrs ) were reported rather than p values ( data supplement )  . 
applying the rm correction for gps test , the absolute risk estimates were computed as the weighted average of the absolute risk estimates over the study population patient age for each ap status , with cis derived using the delta method . 
receiver operating characteristic ( roc ) curve estimates were based on these absolute risk estimates , correcting for bias 444 2021 by american society of clinical oncology inherent in roc curves ( data supplement ) , with and without the gps results as a covariable . 
differences between models in the roc area under the curve ( auc ) were tested for signicance using the bootstrap . the overall cohort consisted of predominantly american urological association ( aua ) lowand intermediate - risk patients with prostate cancer , 55% and 35% , respectively ( table 1 )  . 
the distribution of gps results , accounting for the stratied cohort sampling weighting , in the overall population and by biopsy gleason grade is shown in figure 2 . the gps result appeared to be highly associated with both dm and pcsm at 20 years of follow - up . 
 gps assay associated with long - term prostate cancer outcomes total cohort 2 , 641 patients with prostatectomy 19872004 501 patients selected 127 with clinical recurrence 374 without clinical recurrence 441 patients evaluable for clinical / pathology / gene expression 428 patients with evaluable primary gleason pattern in prostatectomy tissue 51 excluded for insufficient tumor 7 did not meet inclusion criteria 2 outlier gene profile fig 1 . 
of 2 , 641 patients who underwent rp between 1987 and 2004 , a cohort of 501 patients was selected using a 1 : 3 sampling design , which included all 127 patients who did and 374 patients who did not have a clinical recurrence . 
rm - corrected estimates of the 20 - year absolute risk of dm and pcsm as a function of gps result among aua low - risk patients and favorable intermediaterisk patients have functional form similar to the estimates for the overall population , with a large increase in risk for the gps result  . 
the number of events in this subgroup was insufcient for multivariable analysis . discussion previous validation studies have clearly shown the gps test and other prostate biopsybased gene expression proles to predict the presence of ap ( grade group 3 or higher or extraprostatic disease ) in rp specimens or serial needle biopsies in men on as or post - rp.7 , 8 , 15 although ap on biopsy or rp is prognostic regarding risk of recurrence , dm , and pcsm , 16 its use as a surrogate end point for these outcomes in men considering starting or staying on surveillance has been questioned with no clear short - term alternative.17 in this study , we sought to assess whether the gps result , based on pathologic evaluation of the index lesion on rp , in the original discovery cohort of this biomarker appeared to be associated with the more clinically meaningful outcomes of dm and pcsm at long - term followup . 
absolute risks of these outcomes , considering death from causes other than prostate cancer as a competing risk , showed a lowslope relationship with the gps result from 1 to 29 , with an inection point evident at a score 30 , above which the risk of dm or pcsm increased substantially , reaching an absolute risk of 38% for dm and 13% for pcsm at a score of 60 ( fig 3 )  . 
furthermore , we found that including the gps results in models assessing risk of dm and pcsm at 20 years improved discrimination compared with using clinical variables alone ( tables 2 and 3 ; fig 4a and 4b )  . 
other commercially available gene expression proles have reported similar ndings , albeit at earlier time points.18 - 21 treatment because key drivers of biological progression in patients on as are yet to be elucidated , an open question is what aspect of tumor biology commercially available gene expression proles may be measuring . 
detailed pathological analysis of the canary - pass study , a large , well - characterized as cohort , identied the presence of cribriform or stromagenic histology as the strongest predictor of cancer recurrence after in men who progressed to requiring therapy.22 the presence of cribriform glands has been shown in other studies to be associated with higher rates of biochemical recurrence after rp or radiation , as well as both dm and pcsm , 23 , 24 likely driven by the observation that these glands exhibit genomic features characteristic of aggressive disease.25 in a recent study of 194 men with national comprehensive cancer network very low - , low - , or intermediate - risk disease considering as , we observed that only those with the gps results above 29 had cribriform histology present on biopsy ( falzarano et al , manuscript submitted for publication )  . 
gps , genomic prostate score . observed that a gps result 29 was associated with grade reclassication on subsequent biopsy in a cohort of lowand intermediate - risk men on as , whereas in an underpowered study using a cohort of lower - risk men whose mean gps results were 21 , no association with grade progression was observed.17 together , these table 2 . 
however , a number of published observations support a role for decision making in men with higher scores : ( 1 ) multiple biopsy - based studies have validated that higher gps scores are associated with traditional histologic measures of ap ( dened as grade group 3 or extraprostatic disease , both of which are associated with worse outcomes ) 7 - 9 ; ( 2 ) the association of higher gps scores with histologic variants ( cribriform [ falzarano et al , manuscript submitted for publication ] and stromagenic26 histology ) shown to be associated with higher rates of recurrence in an as cohort ; 22 and ( 3 ) long - term data from the current study that link higher gps scores to the risk of meaningful clinical end points ( dm and pcsm )  . 
rm - corrected estimates with 95% condence intervals of the 20 - year absolute risk of distant metastasis ( a ) and prostate cancerspecic mortality ( b ) as a function of the gps result . 
 a 100% brooks et al 100% gps grade stage spline ( psa ) grade stage spline ( psa ) reference gps grade stage spline ( psa ) grade stage spline ( psa ) reference 0% 10% 20% 30% 40% 50% 60% 70% 80% 90% 100% 0% 10% 20% 30% 40% 50% 60% 70% 80% 90% 100% fig 4 . 
model - based rm - corrected , bias - corrected roc curve for dm ( a ) and pcsm ( b ) within 20 years of surgery with covariables : the gps result , high stage , high grade , and log2 psa . 
auc , area under the curve ; dm , distant metastases ; fpr , false positive rate ; gps , genomic prostate score ; pcsm , prostate cancerspecic mortality ; psa , prostate - specic antigen ; rm , regression to the mean ; roc , receiver operating characteristic ; tpr , true positive rate . strengths of this study include that the data were sourced from a prospectively maintained patient registry with locked baseline clinical , pathologic , and gene expression information ; centralized expert pathology review ; 20 - year followup , the longest reported in any similar study ; and independent verication of the statistical analysis . 
there are two limitations : ( 1 ) changes in standardized biopsy grading and stage migration since initial patient enrollment , although we note that all rp specimens were reviewed by an expert gu pathologist after the majority of substantive changes in prostate cancer grading occurred and ( 2 ) that this should be considered an exploratory analysis since the gps test was developed in this cohort . 
although the study by van den eeden et al9 largely replicates the results of this analysis , we believe that further validation in other cohorts is important to rmly establish our conclusions . in conclusion , with long - term follow - up , the gps test appears to be associated with both dm and pcsm and improves the accuracy of models containing clinical variables alone . 
these ndings suggest that genomic changes in the tumor tissue , quantied by the gps test , provide additional biological insight into the long - term risk of dm and pcsm . this information may be valuable to those considering as . prospective studies should be pursued to validate these results . affiliations 1scott department of urology , baylor college of medicine , houston , tx 2glickman urological and kidney institute , cleveland clinic , cleveland , 3department of anatomic pathology , university of alabama at birmingham , birmingham , al 4department of quantitative health sciences , cleveland clinic , cleveland , oh 5genomic health inc , an exact sciences corporation , redwood city , ca administrative support : tamer aboushwareb , eric a . 
 gps assay associated with long - term prostate cancer outcomes patents , royalties , other intellectual property : patent co - inventor on 17gene prostate assay with genomic health , inc conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . michael crager employment : exact sciences stock and other ownership interests : exact sciences travel , accommodations , expenses : genomic health ruixiao lu employment : genomic health , exact sciences stock and other ownership interests : genomic health , exact sciences consulting or advisory role : mission bio john abran employment : exact sciences stock and other ownership interests : exact sciences tamer aboushwareb employment : exact sciences stock and other ownership interests : exact sciences eric a . 
klein consulting or advisory role : grail no other potential conicts of interest were reported . references 2016 klotz l , vesprini d , sethukavalan p , et al : long - term follow - up of a large active surveillance cohort of patients with prostate cancer . 
j clin oncol 33 : 272 - 277 , 2015 tosoian jj , mamawala m , epstein ji , et al : intermediate and longer - term outcomes from a prospective active - surveillance program for favorable - risk prostate cancer . 
mahal ar , butler s , franco i , et al : conservative management of low - risk prostate cancer among young versus older men in the united states : trends and outcomes from a novel national database . 
n engl j med 377 : 132 - 142 , 2017 bill - axelson a , holmberg l , garmo h , et al : radical prostatectomy or watchful waiting in prostate cancer29 - year follow - up . 
n engl j med 379 : 2319 - 2329 , 2018 klein ea , cooperberg mr , magi - galluzzi c , et al : a 17 - gene assay to predict prostate cancer aggressiveness in the context of gleason grade heterogeneity , tumor multifocality , and biopsy undersampling . 
eur urol 66 : 550 - 560 , 2014 cullen j , rosner il , brand tc , et al : a biopsy - based 17 - gene genomic prostate score predicts recurrence after radical prostatectomy and adverse surgical pathology in a racially diverse population of men with clinically lowand intermediate - risk prostate cancer . 
eur urol 68 : 123 - 131 , 2015 van den eeden sk , lu r , zhang n , et al : a biopsy - based 17 - gene genomic prostate score as a predictor of metastases and prostate cancer death in surgically treated men with clinically localized disease . 
lin dw , zheng y , mckenney jk , et al : 17 - gene genomic prostate score test results in the canary prostate active surveillance study ( pass ) cohort . 
spratt de , youse k , deheshi s , et al : individual patient - level meta - analysis of the performance of the decipher genomic classier in high - risk men after prostatectomy to predict development of metastatic disease . 
klein ea , youse k , haddad z , et al : a genomic classier improves prediction of metastatic disease within 5 years after surgery in node - negative high - risk prostate cancer patients managed by radical prostatectomy without adjuvant therapy . 
cooperberg mr , davicioni e , crisan a , et al : combined value of validated clinical and genomic risk stratication tools for predicting prostate cancer mortality in a high - risk prostatectomy cohort . 
canter dj , freedland s , rajamani s , et al : analysis of the prognostic utility of the cell cycle progression ( ccp ) score generated from needle biopsy in men treated with denitive therapy . 
mckenney jk , wei w , hawley s , et al : histologic grading of prostatic adenocarcinoma can be further optimized : analysis of the relative prognostic strength of individual architectural patterns in 1275 patients from the canary retrospective cohort . 
kweldam cf , wildhagen mf , steyerberg ew , et al : cribriform growth is highly predictive for postoperative metastasis and disease - specic death in gleason score 7 prostate cancer . 
greenland ny , cowan je , chan e , et al : prostate biopsy histopathologic features correlate with a commercial gene expression assays reclassication of patient eur j cancer 66 : 26 - 33 , 2016 alterations . 
kornberg z , cooperberg mr , cowan je , et al : a 17 - gene genomic prostate score as a predictor of adverse pathology in men on active surveillance . 
 c clinical response to antiprogrammed death 1 after response and subsequent progression on antiprogrammed death ligand 1 therapy introduction immune checkpoint inhibitors are rapidly becoming a cornerstone in the treatment of nonsmall cell lung cancer ( nsclc )  . 
the programmed death 1 ( pd - 1 ) receptor and its two ligands , programmed death ligand 1 ( pd - l1 ; b7h1 ) and ligand 2 ( pd - l2 ; b7 - dc ) , negatively regulate t - cell activation , and expression of pd - l1 by tumor cells is an important mechanism of immune evasion.1 - 3 multiple agents have been developed to disrupt tumor - associated immune evasion by targeting either pd - 1 or pdl1 . 
nivolumab and pembrolizumab , both anti pd - 1 agents approved for advanced nsclc progressing after chemotherapy , confer an overall survival benefit and produce response rates in 16% to 23% of unselected patients with nsclc.4 - 6 food and drug administration approval was also recently extended to pembrolizumab in the first - line setting for patients with metastatic nsclc expressing pd - l1.7 atezolizumab , an antipd - l1 agent , has also demonstrated an overall survival benefit and has been approved for use in the second - line setting.8 the growing supply of treatment options has led to new questions of optimal sequencing and choice of therapy . 
in particular , the utility of serial treatment with immune checkpoint inhibitors has not been established . agents targeting pd - l1 block the interaction of pd - l1 expressed on tumor cells and tumorinfiltrating immune cells with pd - 1 and b7.1 expressed on t cells . 
studies of these agents , including atezolizumab , avelumab , and durvalumab , have demonstrated similar response rates and clinical benefit.9 - 14 although the effects of antipd - l1 are predicted to be similar to antipd - 1 , it has been speculated that the variation in mechanism may lead to distinct antitumor and toxicity profiles compared with the antipd - 1 agents.15 however , these agents have not been directly compared . 
he had been diagnosed approximately 2 years earlier with nsclc metastatic to bilateral cervical lymph nodes and bilateral adrenal glands . molecular testing showed that his tumor was egfr and kras wild type and alk translocation negative . 
before this evaluation , he received four lines of therapy , including platinum doublet chemotherapy , single - agent docetaxel , palliative chemoradiation with weekly carboplatin and paclitaxel , and erlotinib . he was enrolled in a phase i clinical trial of an antipd - l1 monoclonal antibody given in 21 - day cycles . 
he experienced only mild ( grade 1 ) rash and hypothyroidishe received a total of 16 cycles of antipd - l1 therapy before treatment was stopped per study protocol . the patient was followed with serial cross - sectional imaging and demonstrated continued pr on imaging for 16 months after therapy completion . 
after seven cycles of treatment , he was noted to have progression of disease in his right axilla and a new retropharyngeal ( rp ) mass . biopsy of the rp mass showed poorly differentiated carcinoma consistent with recurrent nsclc and similar to his initial biopsy . 
 chest , abdomen , and pelvis show a metastatic lesion within the right adrenal gland ( arrow ) before initiation of antiprogrammed death ligand 1 ( pd - l1 ) therapy ( panel a1 ) , which regressed after 16 cycles of treatment with antipd - l1 therapy ( panel a2 )  . 
repeat computed tomography imaging demonstrated progressive disease in the right adrenal gland before initiation of antipd - 1 therapy ( panel a3 ) , with subsequent improvement after 9 months of antipd1 therapy ( panel a4 )  . 
ccrt , concurrent radiotherapy ; lns , lymph nodes ; na , not available . palliative radiation therapy ( 30 gy in 10 fractions ) to both his right axilla and rp space . 
two weeks after radiation therapy , repeat imaging demonstrated stability of the rp mass , decrease in the size of the right axillary lymph node , and enlarging adrenal masses . 
imaging of the face after 6 weeks showed a pr in the rp space , and body imaging after 8 weeks of treatment showed a pr in both the right axilla and right adrenal gland ( fig 1a )  . 
he tolerated treatment well , with no immune - related adverse events for 24 cycles , after which he was noted to have progression limited to his right axilla , with a core biopsy confirming nsclc . 
unfortunately , he died several days after this procedure at an outside facility ; the cause of death was unclear . statement of informed consent all human investigations were performed after approval by a local human investigations committee and in accord with an assurance filed with and approved by the department of health and human services , and all data were anonymized to protect the identities of participants involved in the research . 
informed consent from the patient for such research was obtained . longitudinal assessment of pd - l1 and pd - l2 expression biopsy samples were obtained at the time of diagnosis ( biopsy 1 ) , before repeat treatment with antipd - l1 ( biopsy 2 ) , before treatment with anti - pd - 1 ( biopsy 3 ) , and after progression anti pd - 1 therapy ( biopsy 4 ; fig 1b )  . 
however , tissue for this first sample was extremely limited , and possible pd - l1 positivity could not be ruled out because of the size of the tissue specimen , particularly because subsequent specimens from the patient demonstrated a highly heterogeneous pattern of pd - l1 expression with rare positive stromal cells , whereas pd - l2 staining was robust throughout the tumor . 
after his initial disease progression while receiving antipd - l1 therapy , repeat biopsy demonstrated no tumor pd - l1 staining ( with limited stromal pd - l1 positivity ) , and pd - l2 remained strongly positive ( 70% ; fig 1c )  . 
similar results were demonstrated in biopsy 3 before starting pd - 1 therapy and biopsy 4 after progression on this final line of treatment , with strong pd - l2 expression in tumor , moderate pd - l1 staining in stroma , and absence of pd - l1 expression in tumor . 
representative immunohistochemistry samples from each time point are shown in figure 2 . targeted next - generation sequencing genomic testing using a hybrid capture - based next - generation sequencing platform assessing exons from 315 genes ( foundationone ) of the patients tumor at the time of progression while taking nivolumab ( biopsy 4 ) identified seven potentially functional alterations , including rictor amplification , arid1a t2030fs * 3 , arid2 q904 * , kdm5c e656 * , slit2 g498 * , tet2 e1851 * , and tp53 r280i . 
thirty - three variants of unknown significance were identified , and a total mutation burden of 53 mutations / megabase was estimated , placing this patient in the top 7% of all tumor specimens tested by this method.16 thus , the response observed in this high mutation - load patient was consistent with clinical observations.17 no alterations were identified in jak1 , jak2 , cd274 , pdcd1lg2 , pten , myc , or ctnnb1 in this patient , which were previously reported mechanisms of t - cell exclusion and / or resistance to antipd - 1 therapy.18 - 21 next - generation sequencing data were only available on the final biopsy specimen ; thus , changes in mutation burden over time cannot be assessed . gene expression analysis sufficient tissue for expression analysis ( nanostring pancancer immune profiling panel ) was available for two of the four biopsy time points : post - therapy a , which was sampled before beginning the second treatment course of antipd - l1 , and post - therapy b , sampled at disease progression on antipd - l1 , before radiation therapy followed by nivolumab . 
comparison of the expression of immune genes between these two samples demonstrated substantial downregulation of cd274 ( pd - l1 ) mrna and upregulation of several immunosuppressive genes , including il6 and ptgs2 ( cyclooxygenase - 2 ; fig 3a )  . 
it could be hypothesized that distinct immune checkpoints ( eg , pd - l1 v pd - l2 ) could divergently mediate therapeutic resistance to checkpoint inhibitors and support preclinical studies testing this hypothesis . this patients tumor was pd - l1 negative at diagnosis , with some positivity in the stroma , on the basis of our limited sample , but strongly pd - l2 positive . this finding suggests that the significance of pd - l2 positivity in response to pd - l1 or pd - 1 targeted therapies may be a useful subject of study . 
 ( a ) rna collected from archival although these studies used different clones for detection.27 , 28 using our own methods for detection of pd - l2 in a tissue microarray cohort of 43 patients with nsclc , we found that this patient was consistently among the top 5% of pd - l2 expressers . 
 tissue blocks were analyzed by nanostring pancancer immune profiling ( 730 immune - related genes )  . normalized data were compared between the post - therapy a ( preresistance ) and posttherapy b ( postresistance ) specimens for log2 fold change . 
 ( b ) genes involved in the interferon - gamma signaling reactome ( reactome.org ; accession : m965 ) were selected from the pancancer immune profiling gene set and plotted by fold change . this analysis demonstrated a general decrease in interferon - gamma signaling within the tumor microenvironment at disease progression on antiprogrammed death ligand 1 ( pd - l1 )  . 
pdl1 interacts with programmed death 1 ( pd1 ) and b7 - 1 ( cd80 ) to promote immune effector cell suppression , whereas pd - l2 can bind pd - 1 and rgmb , promoting effector suppression and respiratory tolerance in lung - resident macrophages , respectively.22 , 23 apcs , antigen - presenting cells ; cox2 , cyclooxygenase - 2 . be associated with earlier stage of disease ( stage i v all others ) , but not with gender or smoking status ( appendix fig a1 )  . during the second treatment with antipd - l1 , which was accompanied by short - term stable disease and subsequent progression , we observed maintenance of high pd - l2 expression and downregulation of pd - l1 mrna expression accompanied by simultaneous decrease of interferongamma response signatures . 
we also observed upregulation of immunosuppressive genes , such as cyclooxygenase - 2 ( recently shown to be important in mediating antipd - 1 responsiveness29 ) and interleukin - 6 , which was shown to decrease after initial treatment with pd - l1 targeted therapy.30 thus , the changes in gene expression within the tumor microenvironment in this patient were consistent with previous studies . importantly , there were multiple intervening therapies in this patient during the approximately 20month period after the initial pretreatment biopsy , limiting the inferences that can be made during the initial therapy with antipd - l1 . 
balko , leora horn manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors despite his prior treatments with palliative radiation ; however , he did receive an additional course of palliative radiation after his third biopsy and preceding his antipd - 1 therapy , and a role for radiation in sensitizing his tumor to anti - pd - 1 therapy cannot be ruled out . although anecdotal , this case report demonstrates an important clinical finding : patients who become resistant to antipd - l1 may still benefit from pd - 1 targeted therapies , possibly due to a switch from dependency on pd - l1 to pd - l2 for maintenance of immunosuppression . however , the presence of consistently high pd - l2 staining argues against a direct mechanism of pd - l2mediated de novo resistance to antipd - l1 therapy . 
moreover , pd - l2 mrna did not seem to be upregulated or changed during acquisition of resistance to antipd - l1 therapy . however , the ratio of pd - l2 to pd - l1 mrna increased substantially from 3.6 - fold to 14.6 - fold during this period and may be a useful metric to test experimentally in the future for association with resistance to antipd - l1 treatment . 
although more investigation is needed in the context of preclinical studies and clinical trials , this report supports investigations of sequencing antipd - l1 and antipd - 1 therapies to elucidate mechanisms of cross - resistance and derive maximal patient benefit from these agents . 
johnson consulting or advisory role : bristol - myers squibb , genoptix , merck research funding : incyte patents , royalties , other intellectual property : intellectual property and patents pending surrounding use of mhc - ii and response to immune therapy leora horn honoraria : biodesix consulting or advisory role : bristol - myers squibb , merck , bayer , xcovery , genentech , boehringer ingelheim , eli lilly , abbvie , astrazeneca research funding : astrazeneca ( inst ) other relationship : bristol - myers squibb justin m . 
balko research funding : incyte patents , royalties , other intellectual property : patent on use of hla - dr / mhc expression to predict response to immunotherapies references 677 - 704 , 2008 1 . 
mu cy , huang ja , chen y , et al : high expression of pd - l1 in lung cancer may contribute to poor prognosis and tumor cells immune escape through suppressing tumor infiltrating dendritic cells maturation . 
borghaei h , paz - ares l , horn l , et al : nivolumab versus docetaxel in advanced nonsquamous nonsmall - cell lung 2018 - 2028 , 2015 cancer . 
rittmeyer a , barlesi f , waterkamp d , et al : atezolizumab versus docetaxel in patients with previously treated nonsmall - cell lung cancer ( oak ) : a phase 3 , open - label , multicentre randomised controlled trial . 
brahmer jr , tykodi ss , chow lq , et al : safety and activity of anti - pd - l1 antibody in patients with advanced cancer . n engl j med 366 : 2455 - 2465 , 2012 10 . 
brahmer jr , rizvi na , luzky j , et al : clinical activity and biomarkers of medi4736 , an anti - pd - l1 antibody , in patients with nsclc . 
rizvi n , brahmer j , ignatius s , et al : safety and clinical activity of medi4736 , an anti - programmed cell death - ligand 1 ( pd - l1 ) antibody , in patients with nonsmall - cell lung cancer ( nsclc )  . 
spira ai , park k , mazi`eres j , et al : efficacy , safety and predictive biomarker results from a randomized phase ii study comparing mpdl3280a vs docetaxel in 2l / 3l nsclc ( poplar )  . 
spigel dr , chaft je , gettinger sn , et al : clinical activity and safety from a phase ii study ( fir ) of mpdl3280a ( antipdl1 ) in pd - l1selected patients with nonsmall - cell lung cancer ( nsclc )  . 
kelly k , patel mr , infante jr , et al : avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in patients with metastatic or locally advanced solid tumors : assessment of safety and tolerability in a phase i , open - label expansion study . 
xiao y , yu s , zhu b , et al : rgmb is a novel binding partner for pd - l2 and its engagement with pd - l2 promotes respiratory tolerance . 
he j , hu y , hu m , et al : development of pd - 1 / pd - l1 pathway in tumor immune microenvironment and treatment for nonsmall - cell lung cancer . 
yearley j , gibson c , yu n , et al : pd - l2 expression in human tumors : relevance to anti - pd - 1 therapy in cancer . presented at european society for medical oncology annual meeting , vienna , austria , september 25 - 29 , 2015 27 . 
calles a , liao x , sholl lm , et al : expression of pd - 1 and its ligands , pd - l1 and pd - l2 , in smokers and never smokers with kras - mutant lung cancer . 
kim my , koh j , kim s , et al : clinicopathological analysis of pd - l1 and pd - l2 expression in pulmonary squamous cell carcinoma : comparison with tumor - infiltrating t cells and the status of oncogenic drivers . 
postow ma , callahan mk , barker ca , et al : immunologic correlates of the abscopal effect in a patient with melanoma . 2035 - 2036 , 2012 n engl j med 366 : 925 - 931 , 2012 34 . 
programmed death ligand 2 ( pd - l2 ) expression across 43 patients with nonsmall cell lung cancer ( nsclc )  . ( a ) a tissue microarray series of 43 patients with nsclc was stained for pd - l2 expression and analyzed by histoscore ( h - score ; % of cells staining positive 3 intensity [ 0 - 3 + ] )  . 
 c clinical observation of improved outcomes of patients with brca 1 / 2 breast cancer treated with everolimus prior to dna - damaging therapy introduction the mammalian target of rapamycin ( mtor ) pathway comprises mtor complexes 1 and 2 ( mtorc1 / 2 ) and is primarily responsible for maintaining cellular growth and proliferation . 
although it is known to act as a catalyst toward anabolic synthesis , mtorc1 also is responsible for mitigating cellular catabolic processes , namely autophagy.1 mtorc2 complements mtorc1 in anabolic processes.2 phosphoinositide 3 - kinase ( pi3k ) and phosphatase and tensin homolog ( pten ) genetic mutations frequently are found in many tumor types , including breast cancer.3 these genes are important in regulating the downstream activation of the mtor pathway . 
many drugs have been developed to target the mtor pathway , including the mtorc1 inhibitor ( mtori ) everolimus.2 , 4 poly ( adp - ribose ) polymerase ( parp ) is a family of enzymes that repairs damaged dna . 
treatment with a parp inhibitor ( parpi ) prevents dna repair in cancer cells during homologous recombination ( hr ) events in patients with brca1 / 2 mutations , which leads to cell death through synthetic lethality.5 brca1 / 2 germline mutations are found in approximately 5% of unselected breast cancers , with higher prevalence in high - risk cohorts.6 activation of the pi3k / mtor pathway is important in decreasing the effect of brca1 / 2 mutations by stabilizing hr.7 ibrahim et al8 showed that when pi3k is inhibited , hr is impaired , which results in sensitization of brca wild - type triple - negative breast cancer cells to parpis . 
the details of the cohort are listed in table 1 . our analysis revealed that six patients among the 14 treated in brocade had experienced exceptional responses to treatment ; these six had been treated with the mtori everolimus before commencing study therapy . 
the patient with the second - best response had a documented pten deletion and nearly the same pfs at 29.2 months but did not receive veliparib with her carboplatin doublet . discussion most of the preclinical data of the role of the pik3ca / mtor pathway in dna damage sensitivity was carried out with concurrent therapeutic combinations . 
 these adaptive changes can persist over time , which allows one to use a treatment to sensitize a patients tumors to a subsequent therapy.14 , 15 the observed difference in pfs between eve + and eve patients raises the possibility that prior mtori exposure may render brca1 / 2 mutated breast cancer more susceptible to subsequent dna - damaging therapy . the interaction between activating pik3ca mutations or pten deletions and this sensitizing effect by mtori cannot be fully evaluated in this limited case series . 
however , it seems that the presence of these genomic abnormalities did not preclude those patients from deriving a significant benefit from subsequent dna - damaging therapy . in addition to the usual limitations and biases of case series , our analysis was limited by the heterogeneity of patient characteristics , prior treatments received , and study treatment assigned . 
this precludes us from specifically concluding how much of the observed clinical benefit in the eve + group was a result of improving the activity of the cytotoxic chemotherapy or the veliparib ( if given )  . 
in addition , veliparib did not significantly increase the median pfs of the experimental arm compared with the control arm in the overall study , so the effect of the treatment assignment may be minor in explaining the difference between the eve + and eve arms . 
the pfs of these two patients was similar to the main study population , so including them in the analysis with the other estrogen receptor positive patients is unlikely to change the main analysis . 
future studies in patients with brca1 / 2 mutations also should examine sequential treatment strategies by administering pi3kcai / mtori agents for one to two cycles as a sensitizing therapy before switching to a parpi or dna - damaging cytotoxic chemotherapy . 
han research funding : abbvie ( inst ) , prescient therapeutics ( inst ) , tapimmune ( inst ) , seattle genetics ( inst ) , g1 therapeutics ( inst ) , bristol - myers squibb ( inst ) , pfizer ( inst ) , novartis ( inst ) hatem h . 
lee moffitt cancer center and research institute , tampa , fl . presented at the 2017 annual meeting of the american society of clinical oncology , chicago , il , june 2 - 6 , 2017 . prior presentation references 10 : 18 , 2018 2012 150 , 2009 2017 1 . 
ibrahim yh , garca - garca c , serra v , et al : pi3k inhibition impairs brca1 / 2 expression and sensitizes brca - proficient triple - negative breast cancer to parp inhibition . 
mo w , liu q , lin cc , et al : mtor inhibitors suppress homologous recombination repair and synergize with parp inhibitors via regulating suv39h1 in brca - proficient triple - negative breast cancer . 
juvekar a , burga ln , hu h , et al : combining a pi3k inhibitor with a parp inhibitor provides an effective therapy for brca1 - related breast cancer . 
beuvink i , boulay a , fumagalli s , et al : the mtor inhibitor rad001 sensitizes tumor cells to dna - damaged induced apoptosis through inhibition of p21 translation . 
oreilly t , mcsheehy pmj , wartmann m , et al : evaluation of the mtor inhibitor , everolimus , in combination with cytotoxic antitumor agents using human tumor models in vitro and in vivo . 
han hs , diras v , robson m , et al : veliparib with temozolomide or carboplatin / paclitaxel versus placebo with carboplatin / paclitaxel in patients with brca1 / 2 locally recurrent / metastatic breast cancer : randomized phase ii study . 
miller , md4 purpose next - generation sequencing ( ngs ) of tumor and germline dna is foundational for precision oncology , with rapidly expanding diagnostic , prognostic , and therapeutic implications . 
although few question the importance of ngs in modern oncology care , the process of gathering primary molecular data , integrating it into electronic health records , and optimally using it as part of a clinical workow remains far from seamless . numerous challenges persist around data standards and interoperability , and clinicians frequently face difculties in managing the growing amount of genomic knowledge required to care for patients and keep up to date . methods this review provides a descriptive analysis of genomic data workows for ngs data in clinical oncology and issues that arise from the inconsistent use of standards for sharing data across systems . 
questions about their provenance and timeliness of updating remapotentially useful standards for sharing genomic data , such as hl7 fhir and mcode , remain primarily in the research and / or development stage . 
2019 by american society of clinical oncology introduction next - generation sequencing ( ngs ) of tumor and inherited ( germline ) genomes has revolutionized and rened cancer treatment during the past two decades and is now vital for evaluating therapeutic opportunities in many solid and hematologic malignancies.1 currently , ngs panels including sets of genes are the most widespread method of rapidly identifying sequence variation in patients with cancer . 
ngs panels provide information for a variety of purposes , cluding diagnostics ( eg , determination of sarcoma subtype ) , hereditary risk assessment ( eg , lynch syndrome ) , prognosis ( eg , kras mutations in lung adenocarcinoma ) , and treatment selection ( eg , biomarkers for immunotherapy responsiveness , such as tumor mutational burden and microsatellite instability ; therapeutic selection for clinically actionable alterations , such as braf v600e in melanoma ; and biomarkers of resistance , such as loss of b2m for immunotherapy ) .2 , 3 as a metric of the signicance of ngs in oncology care , 29 of the 43 national comprehensive cancer network clinical practice guidelines denote specic sequence - based biomarkers important for clinical care ( table 1 )  . 
of these 29 guidelines for treatment of cancer by site , 12 include both somatic and germline biomarkers , 16 include somatic only , and one includes germline only . recently , there has been an increased focus on performing ngs on matched normal samples ( either adjacent tissue or blood ) to compare with tumor biopsies . 
 conway et al context key objective the amount of molecular knowledge required for patient care is exploding , but the minimal adoption of genomic data standards in electronic health records compounds the challenges facing oncologists . 
using examples from asco cancerlinq , this review covers the current status of next - generation sequencing , describes relevant data standards , highlights the pilot of the genomic smart - on - fhir application , and provides a call to action for laboratories and electronic health record vendors to ensure that the chain of data custody for structured genomic content remains unbroken and reaches the clinician . knowledge generated several genomic knowledge bases for variant interpretation are available to support clinicians . 
nonetheless , transmitting nextgeneration sequencing results via pdf hinders the use of decision support tools intended for clinical care , including trial selection , and blocks the downstream reuse of genomic data . relevance the consistent use of evolving standards ( eg , hl7 fhir and mcode ) should improve genomic data interoperability and care quality . 
however , the full integration of genotype and phenotype will require an innovative and socially driven commitment by all oncologic ecosystem participants , beginning with sequencing laboratories , to better leverage technologic solutions . also embedded in guidelines and reimbursement for certain treatments ( eg , poly [ adp - ribose ] polymerase inhibitors for ovarian cancer )  . 
multiple molecularly targeted agents have now been incorporated into standard patient management and reected in numerous guidelines . clinical quality measures the 2019 merit - based incentive payment system ( mips ) of the centers for medicare and medicaid services quality payment program contains 24 general oncology measures , two of which involve genetic testing ( kras and nras in patients with colorectal cancer ) .14 in addition , a number of clinical quality measures in the asco quality oncology practice initiative reference ngs testing , including nonsmall - cell lung cancer ( nsclc ) measures evaluating the use and turnaround time of molecular testing in patients with adenocarcinoma histology.15 as clinical quality measurement evolves from clinicianfocused process measures to more patient - centric outcome measures , it is reasonable to expect that more measures will incorporate results from ngs panels and potentially circulating tumor - free dna testing to foster appropriate diagnostic testing and therapy selection that affect patient outcomes . molecular testing has become essential to oncology care.12 survey data from 2017 showed that more than 75% of oncologists used ngs tests to guide cancer treatment . 
inclusion of genetic testing in nccn cancer site guidelines s , g , b , or n cancer subtype details cancer site acute lymphoblastic leukemia ( adult and aya ) acute lymphoblastic leukemia ( pediatric ) acute myeloid leukemia aids - related kaposi sarcoma anal carcinoma bladder cancer bladder cancer upper tract tumors urothelial carcinoma of the prostate primary carcinoma of the urethra ewing sarcoma family of tumors giant cell tumor of the bone bone chondrosarcoma chordoma osteosarcoma breast cancer cns cancer cervical cancer lymphoma chronic myeloid leukemia colon / rectal cancer colon cancer rectal cancer chronic lymphocytic leukemia / small lymphocytic esophageal and esophagogastric junction cancers gastric cancer gestational trophoblastic neoplasia hairy cell leukemia head and neck cancers hepatobiliary cancers hodgkin lymphoma kidney cancer malignant pleural mesothelioma melanoma cutaneous melanoma uveal melanoma multiple myeloma / other plasma cell neoplasms multiple myeloma systemic light chain amyloidosis waldenstr om macroglobulinemia / lymphoplasmacytic lymphoma myelodysplastic syndromes myeloproliferative neoplasms ( continued on following page ) efciently assess eligibility criteria . 
barriers include insufcient clinician knowledge , training , and condence regarding the use of ngs results.20 , 21 although many clinicians may take laboratorybased interpretations at face value , numerous knowledge bases have been created to aid oncologists and clinical researchers in the curation and interpretation of ngs data . these were developed largely because of the recognition that institutional ( local ) knowledge based on a limited sampling of the cancer population , including that possessed by testing laboratories , would not be sufcient to type , capture the genomic diversity of any cancer common or rare . 
perhaps a surprise to clinicians , many commonly tested genes , such as brca1 and brca2 , show considerable disagreement by interpreting laboratories about the pathogenicity of genetic variants.22 one of the earliest resources to address this issue was mycancergenome , 23 created at vanderbilt university in 2009 . 
since that time , there have been numerous entrants into an increasingly crowded eld , with the most well - known publicly available resources for variant interpretation being civic , 24 oncokb , 25and clinvar , 26 the latter of which is the rst fda - recognized public genetic variant database , housing clingen expert - curated data.27 each of these efforts was developed in relative isolation and with slightly different goals , leading to a divergence of data models , evidentiary models , and user experiences . 
the variant interpretation in cancer consortium , a driver project of the global alliance for genomics and health , 28 was founded with the mission statement to help unify and harmonize the disparate interpretation in cancer data sources . 
inclusion of genetic testing in nccn cancer site guidelines ( continued ) cancer site neuroendocrine and adrenal tumors s , g , b , or n cancer subtype details neuroendocrine tumors of the gi tract , lung , and thymus ( carcinoid tumors ) neuroendocrine tumors of the pancreas adrenal gland tumors pheochromocytoma / paraganglioma men1 men2 non - hodgkins lymphomas chronic lymphocytic leukemia / small lymphocytic lymphoma b - cell lymphomas primary cutaneous b - cell lymphomas t - cell lymphomas nonmelanoma skin cancers basal cell skin cancer dermatobrosarcoma protuberans merkel cell carcinoma squamous cell skin cancer nonsmall - cell lung cancer occult primary ( cancer of unknown primary ) ovarian cancer epithelial ovarian cancer ( including fallopian tube cancer and primary peritoneal cancer ) pancreatic adenocarcinoma penile cancer prostate cancer small - cell lung cancer soft tissue sarcoma systemic mastocytosis testicular cancer thyroid carcinoma uterine neoplasms endometrial carcinoma uterine sarcoma vulvar cancer thymomas and thymic carcinomas note . 
categorization of national comprehensive cancer network ( nccn ) guideline44 by cancer site showing whether the guideline recommends somatic testing ( s ) , germline testing ( g ) , both ( b ) , or neither ( n )  . 
genetic testing refers to short variations , structural sequence variations , cytogenetic analyses , and mismatch repair assays . abbreviations : aya , adolescent or young adult ; men1 , multiple endocrine neoplasia type 1 ; men2 , multiple endocrine neoplasia type 2 . several challenges associated with knowledge bases must be considered . 
although the aforementioned knowledge bases are free to users , they 4 2019 by american society of clinical oncology are generally not integrated into the clinical workow.30 the second is trustworthiness and culpability . 
can the assertions made by knowledge bases be trusted ? if advice is erroneous , the primary responsibility clearly lies with the managing clinician , but can knowledge bases also be held culpable ? furthermore , advice can become outdated ; this must be expected to some degree , given the exponential growth of the eld and the lag between the announcement of trial results , publication of ndings , fda labeling , and revision of variant interpretations ; however , poor recency of data in knowledge bases will diminish trust . 
many knowledge bases spend much effort on attractive so - called skins and search abilities , but the degree to which clinicians nd these interfaces useful has not been extensively studied . technological challenges of data integration : opportunities with fhir and mcode integration of ngs results into the clinical workow via tackle several ehr interfaces must technologic challenges . interpreted genomic results are in particular , generally reported in pdf format , which cannot support electronic search , clinical decision support ( cds ) , or secondary use.31 moreover , the lack of a common data model for genomic testing impedes all use cases by hampering data storage and interoperability between ehr systems and / or data warehouses , thereby hindering the use of cds tools intended to assist clinicians in caring for their patients . these issues have prompted the emergence of initiatives aimed at improving genomic data standards and facilitating genomic data interoperability . 
the top section shows total count of prognostic or predictive assertions related to this gene - variant combination , the breakdown by data source ( ve are shown ) , and the breakdown by assertion type per association for molecular pathology ( amp ) / asco / college of american pathologists ( cap ) guidelines.46 the middle section cross - references drugs and diseases with the gene of interest ( rst column ) , as well as potentially related genes ( adjacent columns ) , which are automatically determined ; heatmap colors indicate the quantity of evidence for a drug - gene or diseasegene correlation . 
the vicc meta - knowledgebase user guide is available online.47 auspices of sync for genes.36 these reports were generated from proprietary pipelines used for the fmi foundationone and foundationact ngs panels . 
although customers typically receive a pdf of the ndings and interpretations , fmi also sends xml les , based on a custom internal standard used to generate the pdfs , upon request . 
these xml les include more detailed information than that presented in the pdf , some of which is for research use only , and can be parsed to generate information relevant for fhir resources and elements ( eg , variant allele fraction , sequencing depth and functional effect for mutations , absolute copy number and copy - number ratio for copy - number events , number of supporting read pairs and identity of both genes involved for rearrangements , and genomic location for all alterations )  . 
briey , clinical elds such as patient , sample , and physician information could be mapped to patient , specimen , and physician fhir resources , respectively . genomic elds such as alterations ( eg , braf p.v600e , amplication , rearrangement ) , therapies , and clinical trials were mapped to elements of the observation genetics resource , with more detailed genetic information ( eg , chromosome , start position , end position , variant allele frequency , coverage , and variant type ) mapped to the molecular sequence resource . 
the entire fmi report was represented as a diagnostic report resource , which included references to the patient , physician , specimen , observation genetics , and molecular sequence resources . 
the modular design ( fig 2 ) was architected with four major goals : assist in clinical interpretation of variants within context , provide links to external resources , facilitate point - of - care physician - patient conversations , and demonstrate that smart - on - fhir technology can be used for a clinicogenomic use case . 
cancerlinq aggregates structured and unstructured data from ehrs and other sources via direct feeds and processes the data in a series of cloud - based databases where it normalized and deidentied for secondary reuse.40 database the cancerlinq database , now representing more than 1.5 million patients , contains vast amounts of detailed longitudinal clinical data , such as demographics , diagnoses , laboratory results , and medications . 
however , a signicant volume of the data is not computable , because many critical concepts ( cancer staging , biomarkers , disease progression , and adverse events ) reside primarily in text notes and other unstructured documents and not in discrete elds . 
smart ( sustainable medical apps , reusable technology ) precision cancer medicine ( pcm ) architecture diagrathe application is designed to be modular and extensible , particularly in the ability to add presentation modules and interfaces to external data sources . 
unique text strings are shown for two well - known egfr gene variations abstracted during curation of unstructured genomic reports that were obtained from electronic health records of practices participating in cancerlinq . 
although natural language processing technology itself has not yet demonstrated sufcient precision or recall to be used as a standalone solution , it has been successfully embedded in the curation workbench used by the data abstractors , where it functions to surface putative data elements from unstructured text that can then be conrmed or disregarded . curation of genomic data from ngs panels in cancerlinq as noted , ngs panels are typically brought into the ehr as pdfs or scanned faxes and therefore are not computable . however , since 2017 , cancerlinq has been extracting high - value genomic information via user interfaceassisted data abstraction . 
cancerlinq has also obtained and processed structured genomic reports in xml format and is evaluating automated processes to scan and extract data from reports with standardized formats . the magnitude of the genomic data gap in native ehrs is considerable and shows how poorly precision oncology is supported . 
similarly , for advanced nsclc , 85.3% of curated patient records had epidermal growth factor receptor tests , but structured epidermal growth factor receptor data were found in native ehrs for only 1.7% of all records for patients with advanced nsclc . it is worth noting that although cancerlinq has developed various technical solutions to structuring genomic data as it is housed in ehrs , all ngs data are originally generated as structured data by molecular diagnostics laboratories . 
the data capture of the various chemistries that underlie ngs sequencing , as well as the components of bioinformatic pipelines ( sequence aligners , variant callers ) and even clinical report production , comprises machine - readable , structured genomic data . 
the technical solutions cancerlinq has painstakingly developed would not be necessary at all if the originally structured data were provided . a stark example of how data quality is diminished when optical character recognition , needed to parse genomic reports , is applied , particularly to scanned images ( eg , faxed reports ) and tables , is listed in table 2 . 
 conway et al of national comprehensive cancer network guidelines as well as payment incentives ( eg , mips ) and quality programs ( eg , quality oncology practice initiative )  . 
clinical trial eligibility in oncology increasingly incorporates genomic biomarkers , and the fda has been modernizing its policies and review processes for cancer , resulting in an avalanche of new agents and approved indications for targeted therapies.41 there is no dearth of cds tools to help translate patient data into quality care , nor is there a lack of technical solutions to transmit , harmonize , curate , store , or otherwise manage data . 
these problems are not primarily technical , and solving them requires a will to action , with social incentives and disincentives . for example , ngs test results that are natively structured are sent to ordering physicians and stored in their ehrs , but in a manner that requires costly and data - lossy curation to restructure back into usable information . 
considering that the genomic results are reimbursed through federal and private insurers , but the reporting format impedes their utility to clinicians , we call for all molecular diagnostic laboratories to provide structured data as part of routine reporting at the request of ordering physicians and their practices . 
this would help laboratories meet the denition of interoperability by the 21st century cures act34 to facilitate health information exchange without special effort on the part of the user while avoiding the act 's prohibition of information blocking . it is notable that on the basis of curated records , structured brca1 or brca2 gene test results are extremely underrepresented among the 10 ehrs used by the more than 50 cancerlinq practices . 
it is possible to integrate genomic and clinical data from apis externally to native ehrs , but greater cooperation is needed from vendors to export clinical data for cds use and to provide a seamless experience for the clinician , whose attention is tethered to the ehr . adoption of data standards , including hl7 fhir and mcode , by all the entities that generate , transmit , and receive health information would also facilitate the implementation of precision oncology . 
the endless customizability of ehrs is at odds with health information technology interoperability and suboptimally supports automated quality measure reporting as required by mips.42 , 43 the dearth of coding for cancer staging , laboratory data , and medications within ehrs could be rectied by adopting widely used standard vocabularies , which would facilitate the computable representation of patients oncology records as envisioned by mcode . 
miller , md , cancerlinq , american society of clinical oncology , 2318 mill rd , suite 800 , alexandria , va 22314 ; e - mail : robert.miller@asco.org. support supported by award no . 
 ngs data challenges and solutions references freedman an , klabunde cn , wiant k , et al : use of next - generation sequencing tests to guide cancer treatment : results from a nationally representative survey of oncologists in the united states . 
mol oncol 8 : 859 - 873 , 2014 kamps r , brando rd , bosch bj , et al : next - generation sequencing in oncology : genetic diagnosis , risk prediction and cancer classication . 
int j mol sci 18 : e308 , 2017 jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
sci transl med 7 : 283ra53 , 2015 cibulskis k , lawrence ms , carter sl , et al : sensitive detection of somatic point mutations in impure and heterogeneous cancer samples . 
nat biotechnol 31 : 213 - 219 , 2013 carter sl , cibulskis k , helman e , et al : absolute quantication of somatic dna alterations in human cancer . 
nat biotechnol 30 : 413 - 421 , 2012 robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . j clin oncol 33 : 3660 - 3667 , 2015 karow j : tumor - only sequencing may misguide therapy but many labs omit matched control . 
may - misguide - therapy - many - labs - omit - matched - control damodaran s , berger mf , roychowdhury s : clinical tumor sequencing : opportunities and challenges for precision cancer medicine . 
saigi m , alburquerque - bejar jj , sanchez - cespedes m : determinants of immunological evasion and immunocheckpoint inhibition response in non - small cell patterns of carcinoma evolution . 
gao p , zhang r , li j : comprehensive elaboration of database resources utilized in next - generation sequencing - based tumor somatic mutation detection . biochim biophys acta rev cancer . 
j clin oncol 32 : 1317 - 1323 , 2014 johnson l - m , valdez jm , quinn ea , et al : integrating next - generation sequencing into pediatric oncology practice : an assessment of physician condence and understanding of clinical genomics . 
lawler m , siu ll , rehm hl , et al : all the worlds a stage : facilitating discovery science and improved cancer care through the global alliance for genomics and 29 . 
hughes ks , ambinder ep , hess gp , et al : identifying health information technology needs of oncologists to facilitate the adoption of genomic medicine : recommendations from the 2016 american society of clinical oncology omics and precision oncology workshop . 
li m , datto m , duncavage e : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
 during this period , because of a strong family history of breast cancer ( her mother and maternal aunt were diagnosed at age 50 years ) , the patient was referred for genetic counseling and germline testing . 
tumor next - generation sequencing of her resected brain metastasis detected the following genomic events : deleterious tp53 mutation , pi3k3ca exon 20 hotspot mutation , atm deletion mutation ( same as germ line dna sequencing ) and heterozygous atm loss , fgfr1 amplification ( validated by fluorescent in situ hybridization ; 10 gene copies ) , myc amplification , and ccnd1 amplification . 
the primary recommendation of the mtb was recruitment into the expansion cohort of a clinical trial with a poly ( adp - ribose ) polymerase ( parp ) inhibitor available on site . 
table 1 summarizes the existing knowledge in three large public databasesclinical interpretations of variants in cancer ( civic ) , 1 cancer genome interpreter ( cgi ) , 2 and oncokb3on driver genomic events considered predictive biomarkers for targeted therapies in cancer ( atm loss or mutation , pik3ca h1047r mutation , and fgfr1 amplification )  . 
the information is organized according to the level of evidence supporting each gene variantdrug - disease association , ranging from results of preclinical experiments to case reports and from early to late clinical trials . 
each database provided unique and relevant interpretations for single genomic events , and the collective information was helpful when making a therapeutic decision , such as with pik3ca mutations matched to pi3k pathway inhibitors and fgfr1 amplifications matched to fgfr inhibitors in breast cancer . 
of note , some biomarker - drug interactions were described only in different tumor types , including parp inhibitors in the setting of atm loss or mutation in prostate cancer . 
summary of existing knowledge in three public databases with genomic biomarkers for cancer drugs gene alteration atm loss or mutation database predictive association civic response drug evidence level disease pmid case study prostate cancer 26510020 conference ( abstract number ) sensitivity temozolomide preclinical melanoma , glioblastoma 23960094 response early trials prostate cancer 26510020 olaparib ( parp inhibitor ) olaparib ( parp inhibitor ) response vx - 970 ( atr inhibitor ) case report colorectal cancer ena 2015 ( a48 ) response cisplatin early trials bladder cancer 26238431 sensitivity temozolomide preclinical oncokb response olaparib ( parp inhibitor ) compelling biologic evidence pik3ca civic sensitivity preclinical breast cancer h1047r mutation melanoma , glioblastoma 23960094 prostate cancer 26510020 20453058 , 21558396 sensitivity preclinical her2 - positive breast cancer 22294718 resistance trastuzumab case study her2 - positive breast cancer 21594665 response early trials breast cancer 28331003 , 27672108 asco 2015 ( 2500 ) response oncokb response late trials her2 - positive breast cancer 27091708 compelling clinical evidence breast cancer 27672108 asco 2015 ( 2501 ) fgfr1 civic response amplification clinical , case study breast cancer 23658459 , 27179038 no response bgj398 ( fgfr inhibitor ) lucitanib ( multikinase fgfr inhibitor ) response early trials breast cancer 25193991 clinical breast cancer 27870574 oncokb response azd4547 ( fgfr inhibitor ) compelling clinical evidence lung cancer asco 2014 ( 8015 ) note . 
civic , cgi , and oncokb databases were accessed on august 10 , 2017 . abbreviations : cgi , cancer genome interpreter ; civic , clinical interpretations of variants in cancer ; ena , aacr - nci - eortc ; her2 , human epithelial growth factor receptor 2 ; parp , poly ( adp - ribose ) polymerase ; pmid , pubmed identification number . pictilisib ( pi3k inhibitor ) , ch5132799 ( pi3k inhibitor ) azd5363 ( akt inhibitor ) + trastuzumab / lapatinib taselisib ( pi3k inhibitor ) , copanlisib ( pi3k inhibitor ) , azd5363 ( akt inhibitor ) everolimus + trastuzumab + chemotherapy copanlisib ( pi3k inhibitor ) , mln1117 ( pi3k inhibitor ) , others dovitinib ( fgfr inhibitor ) , azd4547 ( fgfr inhibitor ) and consistent across databases . 
both cgi and oncokb present compelling clinical evidence that pik3ca mutations in breast cancer may be targetable with potent and selective pi3k alpha inhibitors , with response rates up to 30% . 
regarding fgfr1 amplifications , antitumor activity of fgfr inhibitors varied depending on the drug being investigated , and response rates were on average lower than those reported for selective pi3k alpha inhibitors in pik3ca - mutated breast cancer . 
 despite the limited preclinical and early clinical data on parp inhibitor activity in an atm loss or mutation setting , mtb members prioritized this therapy in a clinical trial setting because of the biologic evidence of complete atm deficiency ( germ line pathogenic atm mutation plus loss of wild - type atm allele in tumor dna sequencing ) coupled with the patients clinical history of longterm response to platinum - based chemotherapy . 
there are emerging retrospective data on increased efficacy of pd1 / pdl1 blockade in tumors with gene alterations in the dna damage repair pathway , 8 and prospective trials are being designed ( eg , nct03040791 and nct03236935 )  . 
mayer ia , abramson vg , formisano l , et al : a phase ib study of alpelisib ( byl719 ) , a pi3kspecific inhibitor , with letrozole in er + / her2metastatic breast cancer . 
goyal l , saha sk , liu ly , et al : polyclonal secondary fgfr2 mutations drive acquired resistance to fgfr inhibition in patients with fgfr2 fusion - positive cholangiocarcinoma . 
teo m , seier k , ostrovnaya i , et al : dna damage repair and response ( ddr ) gene alterations ( alt ) and response to pd1 / pdl1 blockade in platinum - treated metastatic urothelial carcinoma ( muc )  . 
 acquired ctnnb1 mutation drives immune checkpoint inhibitoracquired resistance in a microsatellite instabilityhigh gastroesophageal adenocarcinoma with brain metastases introduction the landscape of advanced gastric and esophageal adenocarcinomas continues to evolve , partly owing to improved molecular characterization identifying genomically defined subgroups that may benefit from matched therapies.1 - 3 the keynote - 059 and attraction - 2 trials have demonstrated efficacy for the antiprogrammed death - 1 ( pd - 1 ) antibodies pembrolizumab and nivolumab in gastroesophageal adenocarcinomas ( geas ) after two or more prior lines of therapy.3 , 4 the keynote - 059 study population included seven known patients with microsatellite instabilityhigh ( msi - h ) tumors , among whom the response rate was 57% . 
outside of msi - h tumors , changes in neoantigen landscape , acquired jak1 mutations , mhc - i loss , beta - 2microglobulin mutations affecting antigen presentation , and expression of alternate checkpoints have been shown to mediate acquired resistance to immune checkpoint blockade.9 - 12 with the tumor agnostic approval of pembrolizumab for msi - h tumors in 2017 , a better understanding of acquired resistance is increasingly important . 
 standard - of - care human epidermal growth factor receptor 2 immunohistochemical testing was negative , and he received first - line fluorouracil and oxaliplatin with palliative radiotherapy to a painful bone metastasis with a best response of stable disease . 
at the time of first - line progression , his liver biopsy was screened for microsatellite instability , found to be msi - h , and he was enrolled in a clinical trial of ipilimumab 1 mg / kg and nivolumab 3 mg / kg ( table 1 )  . 
after complete radiographic response of distant disease lasting 18 months , he received palliative radiotherapy ( 0.414 gy ) concurrent with nivolumab every 2 weeks for endoscopically improved , but residual , disease and remained in the trial . 
genomic alterations with preclinical and / or clinical evidence supporting resistance to immune checkpoint inhibitors are shown in bold . abbreviations : gej , gastroesophageal junction ; msi - h , microsatellite instabilityhigh ; mut , mutation ; tmb , tumor mutation burden ; wt , wild type . the resection specimen revealed persistence of an 8.5 - cm segment of poorly differentiated gej adenocarcinoma positive for lymphovascular invasion . all lymph nodes were negative , and evidence of significant treatment effect was seen ( tumor regression grade 2 ) , overall staged as ypt3ypn0 with negative margins . 
the surgical specimen was subjected to hybrid - capture comprehensive genomic profiling using a commercial assay ( foundationone , foundation medicine , cambridge , ma ) , which confirmed msi - h ( table 1 )  . 
during the treatment time encompassing stereotactic brain radiotherapy and nivolumab , washout biopsy samples were taken from a stable subcutaneous scalp metastasis , and an intramuscular rectus femoris lesion reappeared on restaging imaging ( table 1 )  . 
in an effort to explore putative resistance mechanisms after excellent durable response to ipilimumab and nivolumab , the samples were all subjected to the same hybrid - capture comprehensive genomic profiling assay ( table 1 ; fig 1 )  . 
after stereotactic brain radiotherapy , the patient went on to enroll in a third - line trial of paclitaxel in combination with the anti - dkk1 monoclonal antibody dkn - 01 ( clinicaltrials . gov identifier : nct02013154 ) and achieved stable disease lasting 4 months , ultimately , with progression in the brain and extracranial sites concurrently . 
clonal divergence and acquired ctnnb1 in a patient with microsatellite instabilityhigh ( msi - h ) gastroesophageal junction adenocarcinoma with disease progression while receiving ipilimumab in combination with nivolumab after a durable response . 
however , the sampled site of cns progression contained private alterations known or suspected to mediate immuno oncology resistance not seen at other disease sites ( fig 1 )  . 
the ctnnb1 t41a and d32y mutations are known ( t41a ) or predicted ( d32y ) stabilizing mutations that lead to t - cell exclusion and resistance to antiprogrammed death - ligand 1 therapies in preclinical models.17 although less well studied , the d32y mutation should increase stability owing to proximity to the cki and gsk3b phosphorylation sites and is a part of the recognition motif for b - trcp ( e3 ligase for b - catenin )  . 
the additional ctnnb1 n387k is not well characterized functionally , although there is some evidence for it leading to increased b - catenin activity in liver cancer.18 stabilizing or gain - of - function ctnnb1 alterations are recurrent in gea and other tumor types and may be associated with a worse outcome , although clinical immunotherapy - specific outcome data are lacking ( fig 3 ) .2 , 19 , 20 it is also possible that the blood - brain barrier may have reduced the efficacy of checkpoint blockade , allowing for the tissue - specific development of the ctnnb1 alterations we observed . 
however , because our methods are limited to dna - based assessment , we cannot exclude nongenomic mediators of acquired resistance that are known to exist.24 overall , our patient may add early support to the possibility of tissue - contextspecific acquired resistance under selective pressure of immune checkpoint inhibitors , although we cannot draw significant conclusions from a single patient . 
in an analogy to oncogene - driven gea , intertumoral heterogeneity may emerge as an acquired resistance mechanism in msi - driven gea.2 in fact , a recent correlative article from a phase ii trial of pembrolizumab in advanced gea identified intratumoral msi heterogeneity in a patient refractory to therapy.6 if further validated , our observation may have implications beyond gea and inform rational , and perhaps individualized , salvage strategies for msi - h tumors progressing while the patient is taking checkpoint inhibitor therapy . 
klempner stock and other ownership interests : tp therapeutics speakers ' bureau : foundation medicine research funding : leap therapeutics ( inst ) , astellas pharma ( inst ) travel , accommodations , expenses : eli lilly alexa b . 
ali employment : foundation medicine leadership : incysus stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health on microbiome stuff in non - neoplastic disease ( i ) charlotte d . 
kubicky consulting or advisory role : bristol - myers squibb , eisai , array biopharma , loxo , bayer , arqule , blueprint medicines , novartis speakers ' bureau : bristol - myers squibb , eisai consulting or advisory role : eli lilly , boston biomedical , astellas pharma matthew h . 
fuchs cs , doi t , jang rw , et al : safety and efficacy of pembrolizumab monotherapy in patients with previously treated advanced gastric and gastroesophageal junction cancer : phase 2 clinical keynote - 059 trial . 
kang yk , boku n , satoh t , et al : nivolumab in patients with advanced gastric or gastrooesophageal junction cancer refractory to , or intolerant of , at least two previous chemotherapy regimens ( ono - 4538 - 12 , attraction - 2 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
janjigian yy , bendell j , calvo e , et al : checkmate - 032 study : efficacy and safety of nivolumab and nivolumab plus ipilimumab in patients with metastatic esophagogastric cancer . 
overman mj , lonardi s , wong kym , et al : durable clinical benefit with nivolumab plus instability - high metastatic in dna mismatch repair - deficient / microsatellite ipilimumab colorectal cancer . 
shitara k , zgrolu m , bang yj , et al : pembrolizumab versus paclitaxel for previously treated , advanced gastric or gastro - oesophageal junction cancer ( keynote - 061 ) : a randomised , openlabel , controlled , phase 3 trial . 
smyth ec , wotherspoon a , peckitt c , et al : mismatch repair deficiency , microsatellite instability , and survival : an exploratory analysis of the medical research council adjuvant gastric infusional chemotherapy ( magic ) trial . 
 o multi - institutional , prospective clinical utility study evaluating the impact of the 92 - gene assay ( cancertype id ) on final diagnosis and treatment planning in patients with metastatic cancer with an unknown or unclear diagnosis purpose metastatic cancers of unknown primary or with unclear diagnoses pose diagnostic and management challenges , often leading to poor outcomes . 
the current study assessed the clinical impact of the 92 - gene assay on diagnostic and treatment decisions for patients with unknown or uncertain diagnoses . methods patients in this prospective , multi - institutional , decision - impact study included those for whom the 92 - gene assay was ordered as part of routine care . 
the key study objective of clinical impact was calculated on the basis of changes in final diagnosis and treatment after testing . results data collection included 444 patients , 107 physicians ( 73 oncologists and 34 pathologists ) , and 28 sites . 
 physicians reported that the 92 - gene assay was used broadly for diagnostic dilemmas that ranged from single suspected tumor type ( 29% ) to a differential diagnosis of two or more suspected tumor types ( 30% ) or cancers of unknown primary ( 41% )  . 
integration of 92 - gene assay results led to a change in the recommended treatment in 47% of patients . conclusion findings from this clinical utility study demonstrate that the 92 - gene assay led to a change in treatment decisions in every other patient case . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction metastatic cancers that are initially characterized as unknown primary ( cup ) , or with other features that may lead to diagnostic uncertainty with respect to tumor type diagnosis , can prolong the clinicopathologic workup and result in delays in the initiation of treatment , additional costs , and relatively poor patient outcomes.1 - 3 sachdev p . 
schnabel fadi braiteh author affiliations and support information ( if applicable ) appear at the end of this article . licensed under the creative commons attribution 4.0 license corresponding author : sachdev p . 
numerous diagnostic and treatment strategies , such as enhanced pathologic techniques , molecular classification of tumor type and subtype , comprehensive mutational profiling , and novel combination regimens of cytotoxics plus biolo gics , have been proposed without universal consensus.4 - 10 investigational approaches to personalize the systemic treatment of metastatic cancer solely on the basis of the patients somatic genomic alterations , disregarding histologic context , have had mixed and disappointing results.11 - 14 results from several recent phase ii studies that evaluated targeted agents for specific genomic alterations across a variety of tumor types have provided evidence that mutations are not targetable in similar manners across tumor types.11 , 12 thus , the clinical utility of this approach is unclear . 
 whereas driver mutations matter , the integration of tumor type and subtype remains critical when considering the efficacy of a targeted therapy aimed at a putative driver mutation.15 given that empirical chemotherapy approaches are associated with poor prognosis in patients with cup or uncertain diagnoses , it might be more effective to refocus on methods with which to identify patient tumor type and subtype to guide therapy.1 , 16 gene expression profilingbased molecular classification of tumors might prove efficacious by helping to identify the primary tumor type and histologic subtype for patients with unknown or uncertain diagnoses . 
the primary objective was to assess clinical impact on the basis of changes in diagnostic and treatment decisions after the incorporation of 92 - gene assay results . methods study design observational in nature , the current study was prospectively defined to evaluate multidisciplinary clinical utility in patients for whom physicians ordered the 92 - gene assay as a clinical workup tool to help identify or narrow the tumor type and subtype diagnosis . 
prespecified objectives were to examine the diagnostic and clinical utility of the 92 - gene assay in oncology and pathology practice to characterize indications of use , and to evaluate its potential integration and impact on patient management by comparing changes in diagnosis and treatment selection after testing . data collection physicians were required to complete standard ized , discipline - specific questionnairespathology and oncologyafter receiving a 92 - gene assay test report . 
 the pathology ecrf consisted of 11 multiple choice questions and four questions that required written responses ( biopsy quality , number and types of immunohistochemistry [ ihc ] performed , and 92 - gene assay result )  . 
the medical oncologist ecrf consisted of 11 multiple choice questions and five questions that required written responses ( time between biopsy and treatment , clinical diagnosis for first - line treatment , name of first - line treatment , other diagnostic or clinical considerations for choosing first - line therapy , and 92 - gene assay result )  . 
 rna quality determined to be quantity not sufficient , in which a molecular prediction could not be determined , physicians completed quantity not sufficient ecrfs that consisted of four multiple choice questions and two questions that required written response ( biopsy quality and number of ihc performed )  . 
ecrf forms are included in the data supplement . physicians were instructed on the web portal and ecrf via a standardized training progra for the pathology questionnaire ( data supplement : pathology ecrf question 7 and oncology ecrf question 8 , respectively ) , physicians were instructed to align terminology with the 50 tumor types and subtypes classified by the 92 - gene assay . 
the testing laboratory was blinded to the working clinical diagnosis from the ecrf . 92 - gene assay the 92 - gene assay was performed as previously described.17 , 20 in brief , the assayreal - time rt pcrwas performed on isolated total rna from tumor cells that were enriched by either microdissection or laser microdissection . 
a prespecified computational algorithm generated probabilities for primary tumor type and subtype on the basis of the degree of similarity of the submitted sample to a reference database of gene expression information from more than 2 , 000 tumors of known tumor type . 
the test report provided a prediction of the main tumor type and subtype on the basis of the highest relative probability and any additional tumor types that cannot be ruled out . 
the report also provided a list of tumor types that could be excluded with 95% confidence . statistical analysis statistical considerations of study size were based on an anticipated treatment recommendation change rate of 35% , targeting a sample size of at least 156 patients to ensure a 95% two - sided ci width of 15% . 
the primary objective of the study was to measure the clinical impact of the 92 - gene assay results on the basis of changes in patient treatment , the narrowing of treatment options , or the elimination of a treatment option ( a , b , or c on question 15 of the oncology questionnaire in the data supplement )  . 
patients were considered eligible for a targeted agent if the physician responded a , " " b , " or c in question 15 and there was a us food and drug administrationapproved targeted therapy that was recommended by the national comprehensive cancer network for the molecular diagnosis provided by the 92 - gene assay . results patient enrollment began in february 2013 and closed october 2014 after enrolling 444 patients with 107 physicians73 medical oncologists and 34 pathologistsfrom 28 sites21 oncology sites and seven pathology sitesacross the united states . 
of the 444 patients enrolled , 397 had sufficient rna for analysis , which corresponded to an overall analytical success rate of 89% , taking into account samples that were determined to have insufficient tissue on pathology review before testing . 
a patient flow diagram is shown in figure 1 . biopsy and tumor characteristics the most common metastatic biopsy sites included the liver ( 23% ) , lymph nodes ( 17% ) , and lung ( 14% ; fig 2a )  . 
patient flow diagram showing the disposition of 92 - gene assay testing . patients submitted for testing ( n = 444 ) not reportable insufficient tissue or rna ( n = 47 ) reportable results ( n = 397 ) resulted to oncologist ( n = 271 ) resulted to pathologist ( n = 126 ) 92 - gene assay results ( n = 271 ) 92 - gene assay results ( n = 126 ) indeterminate ( n = 12 ) indeterminate ( n = 6 ) molecular diagnosis ( n = 259 ) molecular diagnosis ( n = 120 ) excluded did not receive anticancer therapy performance deaths patient choice other ( n = 56 ) ( n = 16 ) ( n = 8 ) ( n = 7 ) ( n = 25 ) patient received anticancer therapy ( n = 203 ) diagnostic testing and preassay diagnosis factors that contributed to an oncologists decision to order the 92 - gene assay were multidisciplinary and included the following : no primary site of origin after clinical review and imaging ( 42% ) , a pathology report that indicated a differential diagnosis ( 21% ) or that indicated an unknown primary site ( 20% ) , and distinguishing between new cancer versus recurrence ( 16% )  . 
 data that were collected to better characterize the sequence of diagnostic testing demonstrated that 72% of physicians responded that patients had pathology and ihc studies performed before the 92 - gene assay , 14% of samples were submitted for pathology and ihc evaluation and the 92 - gene assay concurrently , and approximately 14% of samples were submitted without an indication of the diagnostic sequence . 
the most common imaging tests were computed tomography scans ( 86% ) , fusion positron emission tomography / computed tomography scans ( 57% ) , magnetic resonance imaging ( 29% ) , ultrasound ( 28% ) , regular film radiographs ( 11% ) , or mammogram ( 11% ; data not shown )  . for pathologists , inconclusive ihc ( 50% ) was the most common reason for ordering the 92 - gene assay . 
the mean number of ihc stains performed before the molecular assay was ordered was 10 ( median , nine ; range , zero to 23 ; data not shown )  . 92 - gene assay results and impact on diagnosis of the 397 patients with sufficient tissue and rna for a reportable result , the 92 - gene assay provided a molecular - based tumor type and histologic subtype diagnosis in 379 patients ( 95.5% ) , whereas 4.5% had an indeterminate molecular diagnosis ( fig 1 )  . 
 ( * ) other indicates biopsy sites with fewer than three cases , encompassing uterus , gallbladder , gastroesophageal junction , spine , spleen , thyroid , and salivary gland . 
fna , fine - needle aspiration . liver lymph node lung peritoneal cavity or omentum soft tissue bone / marrow pleural cavity / pleura colon brain rectum skin breast bladder stomach pelvic mass retroperitoneum pericardial cavity adrenal gland pancreas mediastinum esophagus ovary duodenum other * core excision endoscopic other percentage percentage types . 
the most common diagnoses were pancreaticobiliary ( 21.9% ) , squamous cell carcinoma ( 10.1% ) , lung adenocarcinoma ( 9.3% ) , and intestinal ( 8.6% ) type tumors ( fig 3 )  . working diagnoses before the 92 - gene assay were assessed in the medical oncology subset ( n = 271 )  . 
preassay working diagnoses were reported as a single suspected site in 79 patients ( 29% ) , a differential diagnosis of two or more suspected sites in 80 patients ( 30% ) , and cup in 112 patients ( 41% ; fig 4a )  . 
comparison of the 92 - gene assay molecular diagnoses with preassay working diagnoses demonstrated that the assay provided a tumor type diagnosis that was not initially suspected in a large proportion of patients ( fig 4b )  . 
in patients with a single suspected primary site ( n = 79 ) , the 92 - gene assay confirmed the suspected diagnosis in 60% of patients but provided a tumor type result that was not initially suspected in 39% of patients . 
in patients with a differential diagnosis ( n = 80 ) , the 92 - gene assay narrowed the diagnosis in 66% of patients and provided a tumor type result that was not initially suspected in 27% of patients . 
in patients for whom the pathology report indicated cup site ( n = 112 ) , the assay provided a molecular tumor type prediction in 97% of patients . impact on treatment planning of the 271 oncologist - submitted cases , 203 patients ( 75% ) received anticancer treatment after the 92 - gene assay results were made available . 
the most common reasons for patients not receiving treatment were a rapid deterioration in the patients performance status ( 29% ) , patient death ( 14% ) , and a patient declination of treatment ( 13% ; fig 1 )  . 
molecular cancer classification predictions from submitted cases using the 92 - gene assay ( n = 397 )  . pancreaticobiliary squamous cell carcinoma lung adenocarcinoma intestine gastroesophageal adenocarcinoma urinary bladder neuroendocrine ovary breast adenocarcinoma liver hepatocellular carcinoma sarcoma head and neck salivary gland carcinoma prostate adenocarcinoma endometrial adenocarcinoma cervix adenocarcinoma melanoma kidney mesothelioma germ cell thyroid brain indeterminate skin basal cell carcinoma percentage ( fig 5a )  . 
the assay resulted in similar changes in treatment recommendations in all three scenarios of the original working diagnosis48% of cases with a single suspected primary ( n = 79 ) , 49% of differential diagnoses with two or more primaries ( n = 80 ) , and 42% of cases with an unknown primary site ( n = 112 )  . subset analysis within the most commonly predicted tumor type classesthose with 20 casesdemonstrated that physicians changed their recommended treatment in 58% of gi cancers ( n = 81 ) , 54% of gynecologic and breast cancers ( n = 28 ) , and 44% of lung cancers ( n = 27 ; fig 5b )  . 
mutational biomarker testing was most commonly ordered after the 92 - gene assay rendered a diagnosis of lung ( 81% ) or colorectal cancer ( 67% )  . discussion results from this large , multisite study have demonstrated that the 92 - gene assay was used across a spectrum of diagnostic uncertainty , beyond cups , and included cases with differential diagnoses and those with a suspected diagnosis for confirmatory testing . 
in addition , the assay provided a diagnosis that was not initially suspected in a substantial proportion of patients who had either a single suspected diagnosis or differential diagnosis before testing with the 92 - gene assay . 
 this clinical impact was more pronounced in gi and gynecologic and breast tumor types , which suggests that the 92 - gene assay may have additional utility in particular metastatic presentations in which standard approaches may be limited . 
 distribution of 92 - gene assay diagnostic results within the preassay working diagnosis classifications . differential diagnosis ( 30% ) unknown primary ( 41% ) single suspected site ( 29% ) indeterminate indeterminate indeterminate provided new diagnosis provided new diagnosis confirmed suspected diagnosis confirmed suspected diagnosis provided new diagnosis single suspected site differential diagnosis unknown primary approaches , what is both the current and future relevance of establishing the tumor type or cellular context of a metastatic cancer ? recent results from a number of basket trials have demonstrated that knowledge of tumor type and cellular context remains fundamental for the interpretation of potentially targetable dna mutations and the recommendation of treatment approaches in metastatic cancer . 
whereas molecularly targeted agents have been demonstrated to be effective in tumors that harbor a matching molecular alteration , a growing understanding of the importance of molecular heterogeneity and cellular context is emerging . 
for example , the efficacy of the targeted braf inhibitor , vemurafenib , has been shown to be mixed across a diverse set of nonmelanoma cancers with a braf v600 mutation11 and is well known to have poor efficacy in braf - mutated colorectal cancers.11 , 13 similarly , early results from the mypathway basket trial have demonstrated variable response rates in patients with identical mutations across different tumor types.14 finally , in a phase ii study in which patients with a specific molecular alteration were randomly assigned to receive treatment with a molecularly targeted agent or physicians choice of treatment , there was no difference in median progression - free survival between the two treatment groups.12 these data suggest that the effectiveness of targeting putative driver mutations with molecularly targeted agents may be dependent on the specific cellular context or tumor type . 
 no , treatment regimen was not changed ( 53% ) yes , treatment regimen was changed ( 47% ) gi cancers gynecological and breast cancers lung cancers treatment regimen was not changed ( 42% ) yes , treatment regimen was changed ( 58% ) treatment regimen was not changed ( 46% ) yes , treatment regimen was changed ( 54% ) treatment regimen was not changed ( 56% ) yes , treatment regimen was changed ( 44% ) fig 5 . 
 ( b ) impact of the 92 - gene assay on treatment decisions within tumor type subgroups that received therapy : gi cancers ( n = 81 ) , gynecologic and breast cancers ( n = 28 ) , and lung cancers ( n = 27 )  . breast adenocarcinoma , and lung adenocarcinoma.23 - 25 results presented here reinforce the continued relevance of tumor type diagnosis in optimizing treatment strategies that can potentially affect patient outcomes . 
with regard to pancreaticobiliary tumors , the 92 - gene assay also reports additional subtyping into gallbladder adenocarcinoma , pancreatic adenocarcinoma , or cholangiocarcinoma , which may inform treatment decisions for surgery type , neoadjuvant chemotherapy , or site - directed and targetable agents . 
in addition , a significant proportion of tumor types predicted by the 92 - gene assay , including lung adenocarcinoma , lung squamous , colorectal , gastroesophageal , urinary bladder , and neuroendocrine tumors , have not only specific chemotherapy approaches , but also us food and drug administrationapproved molecularly targeted therapies or immunotherapies . 
 decision making , with similar overall results , which supports the clinical utility of the assay.34 , 35 strengths of this study include the large number of patients and contributing physicians , which contributed to the generalizability of the study results . 
first , this was an observational study and no data on outcomes were collected ; however , previous studies have demonstrated that the use of the 92 - gene assay improved survival in patients with cup who were treated on the basis of assay results.16 , 34 although multiple aspects of the study design were prespecified and carefully planned , such as study physicians independently completing questionnaires , a blinded design such that the testing laboratory did not have knowledge of working diagnoses , and a preplanned statistical analysis , bias is an inherent feature of observational studies . 
this aspect of the cross - functional integration of molecular diagnostic results warrants investigation in future studies . this study demonstrated that the 92 - gene assay affected diagnosis and treatment selection in a significant proportion of patients , which supports the clinical utility of the assay as a standardized molecular approach to help streamline additional diagnostic testing in patients with metastatic cancer with unknown or uncertain diagnoses . 
schnabel data analysis and interpretation : all authors manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors lauren e . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : biotheranostics brock e . 
 fadi braiteh stock and other ownership interests : bristol - myers squibb , insys therapeutics , agios , clovis oncology , tesaro honoraria : genentech , insys therapeutics , bristol - myers squibb , amgen , boehringer ingelheim , astrazeneca , bayer , celgene , ipsen , incyte , taiho pharmaceutical , lexicon , ariad pharmaceuticals , eli lilly , abbott nutrition , heron consulting or advisory role : amgen , bristol - myers squibb , clovis oncology , boehringer ingelheim , ipsen , insys therapeutics , ambry genetics , genentech , eli lilly , incyte , bayer , sanofi , regeneron , astrazeneca , merck , celgene , lexicon , pfizer , merrimack pharmaceuticals speakers ' bureau : amgen , bristol - myers squibb , genentech , merck , pfizer , eli lilly , ipsen , insys therapeutics , incyte , boehringer ingelheim , astrazeneca , celgene , taiho pharmaceutical , merrimack pharmaceuticals , biotheranostics travel , accommodations , expenses : genentech , bristolmyers squibb , amgen , celgene , clovis oncology , tesaro , ipsen , insys therapeutics , incyte , heron , astrazeneca , medimmune , novartis , boehringer ingelheim , lexicon , taiho pharmaceutical , bayer , bayer , onyx pharmaceuticals , exelixis , regeneron , sanofi , merrimack pharmaceuticals , pfizer research funding : biotheranostics acknowledgment we thank andrea c . 
grschel s , bommer m , hutter b , et al : integration of genomics and histology revises diagnosis and enables effective therapy of refractory cancer of unknown primary with pdl1 amplification . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors based on molecular profiles : early results from mypathway , an open - label , phase iia umbrella basket study . 
hainsworth jd , rubin ms , spigel dr , et al : molecular gene expression profiling to predict the tissue of origin and direct site - specific therapy in patients with carcinoma of unknown primary site : a prospective trial of the sarah cannon research institute . 
weiss lm , chu p , schroeder be , et al : blinded comparator study of immunohistochemical analysis versus a 92 - gene cancer classifier in the diagnosis of the primary site in metastatic tumors . 
kim b , schroeder b , schnabel ca , et al : physician - reported clinical utility of the 92 - gene molecular classifier in tumors with uncertain diagnosis following standard clinicopathologic evaluation . 
ahmed ka , caudell jj , el - haddad g , et al : radiosensitivity differences between liver metastases based on primary histology suggest implications for clinical outcomes after stereotactic body radiation therapy  . 
spetzler d , xiao n , burnett k , et al : multi - platform molecular profiling of 1 , 180 patients increases median overall survival and influences treatment decision in 53% of cases . 
nystrom sj , hornberger jc , varadhachary gr , et al : clinical utility of gene - expression profiling for tumor - site origin in patients with metastatic or poorly differentiated cancer : impact on diagnosis , treatment , and survival . 
raghav k , mhadgut h , mcquade jl , et al : cancer of unknown primary in adolescents and young adults : clinicopathological features , prognostic factors and survival outcomes . 
hainsworth jd , schnabel ca , erlander mg , et al : a retrospective study of treatment outcomes in patients with carcinoma of unknown primary site and a colorectal cancer molecular profile . 
j nat cancer inst 105 : 782 - 790 , 2013 appendix we thank the following principal investigators of the clinical study sites who participated in the study : paul adams , md ( genesys hurley cancer institute ) , solhail akbani , md ( baptist hospitals of southeast texas ) , stephen anthony , do ( evergreen hematology - oncology ) , andrew j . 
brenner , md ( the university of texas health science center at san antonio ) , david campbell , md ( grass valley hematology - oncology medical group ) , arvind chaudhry , md , phd ( medical oncology associates ) , william gilles , md ( dignity health ) , h . 
oxnard , md1 noninvasive genotyping of plasma cell - free dna is being integrated into cancer care at an astonishing rate , as its potential to radically increase access to personalized cancer care is increasingly recognized.1 whereas next - generation sequencing ( ngs ) of tumor has been commoditized and democratized ( with many academic hospitals offering their own clinical laboratory improvement amendmentscertied tests ) , plasma ngs is primarily sent out for testing at commercial laboratories . 
however , although these tests are ordered and reported en masse , the causes of falsepositive or false - negative plasma ngs results have only gradually become apparent ( fig 1 )  . false - negative results have long been recognized as common with blood - based assays . 
we and others identied that assay sensitivity is closely related to clinical factors such as stage and metastatic spread , tumor dna in cases suggesting limited shed of missed by plasma ngs.2 , 3 false positives have also been described with many plasma genotyping assays and are routinely attributed to tumor heterogeneity.4 although heterogeneity is clearly a source of tumor / plasma discordance in cancers that have developed drug resistance , 5 , 6 many false positives can be attributed to dna shed from normal cells , including germline variants or noncancerous somatic variants such as clonal hematopoiesis ( ch ) .7 - 9 the latter is particularly challenging because ch can involve cancer - associated genes ( eg , tp53 , jak2 , kras )  . 
yet when such mutations are identied in plasma , they may not reect true tumor genotype . what is least understood is how technical factors related to assay performance contribute to false - positive and false - negative results . 
probe design and specics of library generation are often considered proprietary and are only minimally described in the few analytical validation studies that have been published . this is the context motivating the publication by stetson et al10 in jco precision oncology . 
the authors sent aliquots of plasma to four commercial clinical laboratory improvement amendmentscertied laboratories for plasma ngs and compared this to ngs performed on matched tumor and normal tissue at foundation medicine . 
the vendors were blinded to tumor ngs results but knew that their plasma ngs results would be compared with orthogonal tissue results , as well as with plasma results from other laboratories . 
following bioinformatic analysis and variant calling , binary alignment map les were provided by the vendors to the authors for independent , unblinded , post - hoc sequence analysis . with this design , the authors were not only able to address many of the pitfalls that plagued prior vendor comparison studies , 11 , 12 but they could also investigate interassay technical factors . 
more precisely , stetson et al10 were able to account for known germline variants , investigate mutation - calling biases , and examine whether false negatives were as the result of stochastic sample biases or thresholding nuances of the vendors bioinformatic lter . the results should give pause . 
positive predictive value ( ppv ) against tissue ranged from 36% to 80% . however , results improved when limited to mutations called at an allelic fraction ( af ) greater than 1% , with three vendors achieving a ppv of 100% for these higher af calls . 
note that variants detected at less than 1% af are routinely reported by each vendor , and such sensitivity is advertised as a unique strength of plasma ngs assays . false - positive variants tended to be novel with no reports in somatic variant databases , and these were often related to vendor - specic mutational biases . false negatives were attributed to bioinformatic ltering of suspected germline variants and limitations from high signal - to - noise ratio . 
taken together , these results point to recurrent contributions from technical differences in the bioinformatic pipelines of the assays , assay sensitivity , or plain error . the current study is far from perfect and leaves room for improvement . 
the study cohort consisted primarily of early - stage cancers ( 21 of 24 patients had stage i and ii cancers ) , which are not the intended population for plasma ngs . 
beyond these established biologic factors , technical factors may be an underappreciated source of erroneous plasma ngs . technical factors tett chnical factor tumor dna shed tumor heterogeneity ( particularly at resistance ) tett chnical factors technical factors white blood cell dna ( clonal hematopoiesis , germline variants ) finally , reference truth was extrapolated across four different assays . 
furthermore , this analysis does not broach the challenges of reporting plasma ngs results . one could imagine that a forward - thinking laboratory might recognize the limitations of plasma ngs in its reporting , noting the risk of false positives for low af or ch - associated variants , as well as the risk of false negatives when low tumor shed is apparent . as the use of plasma ngs becomes increasingly widespread in cancer care , there remains a clear need for concordance studies such as this one . 
 editorial policy , please refer to or ascopubs.org / po / authorcenter . patents , royalties , other intellectual property : patent pending on noninvasive blood - based monitoring of genomic alterations in cancer ( inst ) cloud p . 
paweletz honoraria : astrazeneca korea , bio - rad consulting or advisory role : dropworks research funding : guardant health , astrazeneca travel , accommodations , expenses : astrazeneca korea geoffrey r . 
oxnard honoraria : chugai pharma , bio - rad , sysmex , guardant health consulting or advisory role : astrazeneca , inivata , sysmex , takeda , loxo oncology , ignyta , dropworks , grail no other potential conicts of interest were reported . references aggarwal c , thompson jc , black ta , et al : clinical implications of plasma - based genotyping with the delivery of personalized therapy in metastatic non - small cell lung cancer . 
jama oncol 2 : 1014 - 1022 , 2016 bettegowda c , sausen m , leary rj , et al : detection of circulating tumor dna in earlyand late - stage human malignancies . 
sci transl med 6 : 224ra24 , 2014 forshew t , murtaza m , parkinson c , et al : noninvasive identication and monitoring of cancer mutations by targeted deep sequencing of plasma dna . 
sci transl med 4 : 136ra68 , 2012 oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - smallcell lung cancer . 
clin cancer res 24 : 4437 - 4443 , 2018 oxnard gr , hu y , mileham kf , et al : assessment of resistance mechanisms and clinical implications in patients with egfr t790m - positive lung cancer and acquired resistance to osimertinib . 
hu y , alden rs , odegaard ji , et al : discrimination of germline egfr t790m mutations in plasma cell - free dna allows study of prevalence across 31 , 414 cancer patients . 
clin cancer res 23 : 7351 - 7359 , 2017 slavin tp , banks kc , chudova d , et al : identication of incidental germline mutations in patients with advanced solid tumors who underwent cell - free circulating tumor dna sequencing . 
stetson d , ahmed a , nuttall brb , et al : orthogonal comparison of four plasma ngs tests with tumor suggests technical factors are a major source of assay discordance . 
paweletz cp , sacher ag , raymond ck , et al : bias - corrected targeted next - generation sequencing for rapid , multiplexed detection of actionable alterations in cell - free dna from advanced lung cancer patients . 
guibert n , hu y , feeney n , et al : amplicon - based next - generation sequencing of plasma cell - free dna for detection of driver and resistance mutations in advanced non - small cell lung cancer . 
 mutational landscape in resected periampullary adenocarcinoma : relationship with morphology and clinical outcome sebastian lundgren , md1 ; soe olsson hau , md1 ; jacob elebro , md , phd1 ; margareta heby , md , phd1 ; emelie karnevi , phd1 ; bj orn nodin , phd1 ; jakob eberhard , md , phd1 ; karolina holm , phd1 ; johan staaf , phd1 ; g oran b . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction periampullary adenocarcinoma is a collective term for tumors arising in the area surrounding the ampulla of vater , including the head of the pancreas , the duodenum , and the common bile duct . 
a morphologic classication into intestinal type ( i - type ) and pancreatobiliary type ( pb - type ) has been shown to provide better prognostic information than anatomic origin , with the former having a more favorable clinical outcome.1 - 3 although a plethora of mutations has been documented in pancreatic cancer , 4 - 7 the mutational landscape of other periampullary cancers has been less studied . 
no targeted therapies have proven to be efcient , and adjuvant chemotherapy therefore remains standard of care after resection of these tumors . hence , there is evident need for additional studies on the distribution and clinical signicance of the mutational landscape in the full range of periampullary including pancreatic cancer , adenocarcinomas , enable a better patient stratication and identify potential responders to targeted therapies . 
 lundgren et al context ( cid : 129 ) to what extent does morphology inuence the mutational landscape in periampullary adenocarcinomas , and can we nd novel prognostic and predictive biomarkers that differ by morphology , so as to better characterize this heterogeneous group of tumors in a clinical context ? ( cid : 129 ) the results presented here demonstrate that the distribution and prognostic impact of mutations in key genes indeed differ according to morphology and that emphasis on morphology rather than anatomy is of importance . 
approval for the study was obtained from the ethics committee of lund university ( reference number 445 / 07 ) , whereby the committee waived the need for consent other than the option to opt ; out . next - generation sequencing tissue cores of 1 - mm diameter were taken from tumor cellenriched formalin - xed parafn - embedded tissue . dna extraction was performed using the qiagen generead ( qiagen , hilden , germany ) kit for formalin - xed parafnembedded tissue according to the manufacturers instructions . 
forty - one ( 39.8% ) were classied as i - type and 62 ( 60.2% ) as pb - type . a panel of 70 cancer - associated genes was put together for this study and characterized using illumina truseq custom amplicon assay ( illumina , san diego , ca ) with a miseq instrument according to manufacturers instructions . 
detected mutations were screened against the cosmic and exac databases , to lter single - nucleotide polymorphisms commonly reported in different populations . immunohistochemical analysis of brahma - related gene 1 protein expression immunohistochemical analysis of brahma - related gene 1 ( brg1 ) protein expression , 4 - m tissue microarray sections were automatically pretreated in the pt - link system ( dako , glostrup , denmark ) and stained in an automated immunostainer ( autostainer plus , dako ) using the dako envision flex + detection system , peroxidase / dab , rabbit / mouse with the monoclonal anti - brg1 antibody clone g - 7 ( santa cruz biotechnology , dallas , tx ) , diluted 1 : 25 . brg1 was expressed in the tumor cell nuclei and present in the majority of tumor cells in positive cases . 
kaplanmeier analysis log - rank test was applied to illustrate any difference in 5 - year overall survival ( os ) , and cox regression proportional hazard models were used to estimate hazard ratios ( hrs ) for death within 5 years in both univariable and multivariable analysis . 
multivariable cox regression included adjustment for age ( continuous ) , t - stage ( t1 or t2 v t3 or t4 ) , n - stage ( negative v positive nodal status ) , grade ( well to moderate v poor ) , morphology ( i - type v pb - type ) in the entire cohort , adjuvant chemotherapy ( none v any ) , invasion into vascular and lymphatic structures , and perineural growth . 
the proportional hazard ( ph ) assumption was tested using cox regression with a timedependent covariate analysis , whereby the ph assumption was considered to be satised when the factor time interaction was nonsignicant . 
the ph assumption was also evaluated graphically using log - minus - log plots . in the entire cohort , three cases were excluded in the survival analyses : one patient with a pb - type tumor who was lost to follow - up because of emigration , and two patients with i - type tumors who died as a result of complications from the initial surgical treatment . 
to estimate the interaction treatment and selected bioeffect between adjuvant markers , the following interaction variable was constructed : any adjuvant treatment ( + / ) biomarker ( + / )  . 
all data generated or analyzed during this study are included in this published article ( data supplement )  . results distribution of mutations according to morphologic type there were no signicant differences in the distribution of clinicopathological characteristics between cases with known and unknown mutational status ( data supplement )  . the frequency of mutations according to morphologic type is shown in figure 1 and further outlined in the data supplement . 
the frequency of mutations according to anatomic origin is shown in the data supplement . prognostic impact of the most frequent mutations kaplan - meier analyses demonstrate a signicantly prolonged os for patients with i - type compared with patients with pb - type tumors ( data supplement )  . 
when stratifying for anatomic origin , the survival curves cluster into two groups concordant with morphology ( data supplement )  . of the nine most frequently mutated genes outlined above , only apc , erbb3 , kras , and smarca4 were shown to confer a prognostic value , depending on the context . 
apc mutation was not prognostic in i - type tumors ( data not shown ) , and erbb3 mutation was not prognostic in analyses stratied for morphology ( data not shown )  . kras mutation was the strongest predictor of survival , as visualized in figure 2 . 
when stratifying for ampullary origin , kras mutation remained a prognostic factor in i - type tumors ( p = 0.033 ; fig 2d ) but was not prognostic in pb - type tumors ( fig 2e )  . 
 intestinal type pancreatobiliary type tp53 kras rnf43 smad4 erbb3 smarca4 cdkn2a lundgren et al tp53 kras rnf43 smad4 smarca4 cdkn2a erbb3 genetic alteration no alterations truncating mutation in - frame mutation missense mutation fig 1 . 
the genetic alterations were classied as either truncating , missense , or in - frame mutations . mutation did not differ according to adjuvant chemotherapy in i - type tumors ( data not shown )  . 
in the entire cohort , high brg1 expression was an adverse prognostic factor in patients not receiving adjuvant chemotherapy but was not prognostic in patients receiving adjuvant chemotherapy ( data not shown )  . 
the mutational burden of the analyzed genes did not differ signicantly between i - type and pb - type tumors ( p = .577 ) and was not prognostic in the whole cohort or stratied for morphologic type . discussion morphology is emerging as an important prognostic factor in periampullary adenocarcinoma , 1 , 2 and to our knowledge , this is the rst study to comprehensively map common cancer - associated mutations in the full range of periampullary adenocarcinoma , with particular reference to morphology . 
these ndings are in line with a study on 112 cancers of ampullary origin , demonstrating that the mutational spectrum in i - type tumors resembles that of colorectal cancer , and the mutational spectrum in pb - type tumors resembles that of pancreatic cancer.12 in the current study , mutations in apc but not in cdkn2a were found to be prognostic . 
given that no pb - type tumors harbored apc mutations , it is plausible to assume that the link between these mutations and a favorable outcome in the entire cohort is mainly due to their association with i - type morphology . 
the same line of reasoning applies to the association between erbb3 mutations , being more prevalent in i - type tumors , and a prolonged survival in the entire cohort . 
adding to this , there was no signicant association between her3 expression and erbb3 mutational status , and the clinical utility of assessment of erbb3 mutation status for prognostication purposes needs additional validation . kras mutation was found to signify a signicantly shorter survival in patients with i - type tumors , also when adjusted for established clinical factors , whereas patients with kras wild - type i - type tumors could indeed be classied as long - term survivors . 
as of yet , epidermal growth factor receptor ( egfr ) inhibition has not shown clinical efcacy in pancreatic cancer , 15 but no study has investigated the efcacy of egfr inhibitors in periampullary adenocarcinoma in relation to morphology . although none of the patients in this study had received egfr - inhibiting treatment , the ndings indicate that some ras wild - type periampullary cancers of i - type may indeed benet from such treatment . 
 mutational spectrum and morphology in periampullary cancer kras wt kras mut p = .033 kras wt kras mut p = .018 time since diagnosis ( months ) time since diagnosis ( months ) 2 . 
kaplan - meier curves visualize differences in 5 - year overall survival for patients with kras - mutated ( mut ) and wild - type ( wt ) tumors in ( a ) the entire cohort , intestinal - type tumors , ( c ) pancreatobiliary - type tumors , ( d ) intestinal - type amtumors , and ( e ) pullary pancreatobiliary - type pullary tumors . kras wt kras mut p = .680 kras wt kras mut p = .033 time since diagnosis ( months ) time since diagnosis ( months ) no . 
 lundgren et al smarca4 wt smarca4 mut p = .050 smarca4 wt smarca4 mut p = .803 time since diagnosis ( months ) time since diagnosis ( months ) score 0 score 2 score 3 brg1 low brg1 hight p = .061 brg1 low brg1 high p = .037 time since diagnosis ( months ) time since diagnosis ( months ) no . 
relationship of smarca4 mutation status and brahma - related gene 1 ( brg1 ) protein expression with overall survival according to adjuvant chemotherapy in patients with pancreatobiliary ( pb ) - type tumors . 
 ( a , b ) kaplanmeier curves visualizing differences in 5 - year overall survival in patients with pb - type tumors according to smarca4 mutation status ( a ) without adjuvant chemotherapy , and ( b ) with adjuvant chemotherapy . ( c ) sample immunohistochemical images of brg - 1 expression . 
 ( d , e ) kaplan - meier analyses visualizing differences in 5 - year overall survival in patients with pb - type tumors according to low and high brg1 expression ( d ) without adjuvant chemotherapy , and ( e ) with adjuvant chemotherapy . 
 mutational spectrum and morphology in periampullary cancer despite the lack of a signicant interaction between smarca4 mutation and adjuvant treatment , this observation led us to further explore the expression and prognostic value of brg1 , the protein encoded by smarca4 , in tumors from the full study cohort . 
brg1 was found to be an adverse factor in patients who did not receive adjuvant chemotherapy and , in addition , there was a signicant interaction with adjuvant chemotherapy in pbtype tumors . 
one study on pancreatic cancer ( n = 68 ) failed to demonstrate an association between brg1 expression and gemcitabine response or survival , 17 but the nding of a potential predictive role for smarca4 / brg1 in the current study merits further validation in additional patient cohorts . to our knowledge , this is the rst study to map the prevalence and prognostic signicance of mutations in common cancer - associated genes in the full spectrum of periampullary adenocarcinoma . 
in particular , kras mutation status may be a suitable biomarker for prognostication in patients with i - type tumors , and smarca4 / brg1 expression may add value in the prediction of response to adjuvant chemotherapy treatment in patients with pbtype tumors . 
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diagn pathol 9 : 80 , 2014 elebro j , heby m , warfvinge cf , et al : expression and prognostic signicance of human epidermal growth factor receptors 1 , 2 and 3 in periampullary adenocarcinoma . 
philip pa , benedetti j , corless cl , et al : phase iii study comparing gemcitabine plus cetuximab versus gemcitabine in patients with advanced pancreatic adenocarcinoma : southwest oncology group - directed intergroup trial s0205 . 
 c signicant and durable clinical response to sorafenib and radiation therapy for a patient with stage iv hepatocellular carcinoma and lrrk2 mutation linlin yang , md1 ; patrick wald , md1 ; sameek roychowdhury , md , phd1 ; anne m . 
the level was elevated to alpha fetoprotein ( afp ) 57 , 400 ng / ml , and ct - guided biopsy of the large hepatic lesion revealed stage iv hcc . 
because of radiographic concern for disease progression and invasion into the transverse colon , sorafenib was discontinued and radiation therapy was in addition , started 1 week after sorafenib was discontinued . 
the two large masses were irradiated to a dose of 40 gy in 16 fractions using a conformal radiation plan ( fig 1d )  . repeat ct scans 1 month later showed a large decrease in the size of not only the two radiated extrahepatic lesions but also the unirradiated hepatic lesions , and it was decided to restart the patient on maintenance sorafenib ( 200 mg twice daily ) 6 weeks after radiation . 
on the basis of this impressive response , sorafenib doses were held , and the patient underwent laparoscopic partial left hepatectomy of segment 4b with removal of additional primary liver and extrahepatic omental masses . 
at abdominal masses showed no residual 3 weeks after surgery , sorafenib was restarted at 200 mg twice daily but was discontinued after 2 more months because of sorafenib - related pulmonary toxicity . 
after this exceptional response , we performed next - generation sequencing of whole blood lymphocytes and tumor dna from the diagnostic biopsy specimen ( table 1 ) , which revealed mutations in lrrk2 ( k1316n ) , lrp1b ( v4250a , y4256c ) , tp53 ( v157insa , a nonframeshift insertion of three base pairs : cgc ) , and notch3 ( g501s )  . 
 yang et al started sorafenib 400 mg twice a day sorefenib stopped and rt delivered started maintenance sorafenib 200 mg twice a day surgery sorafenib 200 mg twice a day sorafenib discontinued 9 10 11 12 14 47 52 time ( months ) 180000 160000 140000 120000 100000 80000 60000 40000 20000 fig 1 . 
 ( right ) disappearance of intrahepatic lesions noted in fig 1b . lrrk2 we turned our attention to lrrk2 , a gene that has been linked to the pathogenesis of parkinson disease with known roles in the antioxidant response.2 , 3 ionizing radiation generates reactive oxygen species ( ros ) , which are critical for the ability of radiation to promote tumor cell kill through dna damage . 
the degree of ros generation correlates with serum levels of advanced oxidation protein products and clinical effectiveness in sorafenib - treated patients with hcc.4 because ros are in the response to both radiation and sorafenib , critical through promotion of dna damage , we hypothesized that this mutation in lrrk2 could alter the response to both therapies . 
we observed adequate transfected wild - type ( wt ) and k1316n expression of leucine - rich repeat kinase 2 ( lrrk2 ) protein in multiple cell lines ( appendix fig a3 for rna and protein ; primer sequences intable a1 )  . 
we also tested genetic silencing of lrrk2 with small interfering rna ( sirna ) and found that lrrk2 depletion likewise sensitized hcc cells to sorafenib ( figs 2c and 2d )  . 
in addition , we found that expression of the lrrk2 k1316n mutation in both hela and hepg2 cells resulted in notable radiation sensitization in radiation clonogenic assays , whereas wt lrrk2 had no radiosensitizing effects ( figs 2e and 2f )  . because of the previously identied role of lrrk2 in ros , we assessed whether wt lrrk2 or the k1316n mutant altered levels of ros in cancer cells . 
 ( a , b ) overexpression of lrrk2 k1316n signicantly increases sorafenib sensitivity on hcc cells . ( c , d ) genetic silencing of lrrk2 with sirna sensitizes hcc cells to sorafenib treatment . 
sorafenib sensitivity on hcc cells was determined by alamarblue assay ( thermofisher , waltham , ma ) 72 hours after transfection , whereas radiation sensitivity was determined by clonogenic assay . 
similarly , we found that lrrk2 k1316n greatly increased hydrogen peroxide ( h2o2 ) levels , another known mediator of ros damage , and this increase was reversed by treatment of cells with ebselen , an h2o2 scavenger ( figs 3d , 3e , and 3f )  . 
finally , the addition of the superoxide scavenger tiron greatly attenuated the radiation sensitivity induced by lrrk2 k1316n in radiation clonogenic assays ( figs 4a and 4b )  . discussion in this case of a patient with an exceptional response to sorafenib and radiation , we identied a novel lrrk2 k1316n mutation that induced sorafenib and radiation sensitivity in various hcc cell lines , consistent with our clinical observations . 
 ( * ) signicant difference from corresponding tiron or ebselen treatment group ; ( ) signicant difference from empty vector ; ( ) signicant difference from lrrk2 wild type ( wt )  . 
hepg2 and hela cells transfected with wild - type ( wt ) lrrk2 and lrrk2 k1316n were preincubated with dmso or tiron ( 1 mm ) and then exposed to 4 gy of radiation . 
thus , we hypothesize that this lrrk2 mutation increases lrrk2 kinase activity and enhances sorafenib and radiation - induced apoptotic cell death signaling via increased p53 and p21 activity . our in vitro data suggest that this lrrk2 k1316n mutation like other canonical lrrk2 mutations increases ros , observed in parkinson disease . 
thus , another potential hypothesis to explain the radiosensitivity of disease in this patient is that increased lrrk2 kinase activity in lrrk2 mutants may render cells more susceptible to oxidative stress imparted by radiotherapy through creation of ros , such as oxygen free radicals.6 multiple publications show that lrrk2 mutations induce synergistic or additive cell killing in the presence of oxidative stress.7 , 8 taken together , the presence of increased oxidative stress imparted by an activating lrrk2 mutation could prime tumor cells to increased radiation - mediated cell death . the near - complete pathologic response and more than 4 - year disease - free interval since completion of all therapy are remarkable results from a low to moderate dose of radiation and a drug that rarely induces complete response ( 0% in the sharp trial )  . 
it is also interesting to note the dramatic radiographic responses seen in lesions that were not directly radiated , which suggests an abscopal effect from the combination of sorafenib and radiotherapy . 
certainly , we cannot overlook that the dramatic responses observed may have been due in part to the development of an antitumor immune response , which has been previously attributed to both sorafenib and radiation.9 , 10 indeed , the radiologic progression initially noted after sorafenib started may be related to pseudoprogression and development of an early immune response or apoptosis / necrosis of the tumor , despite the observation of the most dramatic clinical and radiographic response with postradiation sorafenib . in conclusion , these data support a role for a novel , previously unidentied lrrk2 mutation that promotes sorafenib and radiation sensitivity through an ros - dependent mechanism . in addition , the combination of radiation and sorafenib also may have induced an antitumor immune response . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . patrick wald employment : riverside radiation oncology sameek roychowdhury stock and other ownership interests : johnson & johnson ( i ) consulting or advisory role : incyte , abbvie , qed therapeutics research funding : takeda , ignyte anne m . 
noonan consulting or advisory role : helsinn healthcare no other potential conicts of interest were reported . references llovet jm , ricci s , mazzaferro v , et al : sorafenib in advanced hepatocellular carcinoma . 
n engl j med 359 : 378 - 390 , 2008 goldwurm s , di fonzo a , simons ej , et al : the g6055a ( g2019s ) mutation in lrrk2 is frequent in both early and late onset parkinsons disease and originates from a common ancestor . 
j med genet 42 : e65 , 2005 loefer da , klaver ac , coffey mp , et al : increased oxidative stress markers in cerebrospinal uid from healthy subjects with parkinsons diseaseassociated lrrk2 gene mutations . 
front aging neurosci 9 : 89 , 2017 coriat r , nicco c , ch ereau c , et al : sorafenib - induced hepatocellular carcinoma cell death depends on reactive oxygen species production in vitro and in vivo . mol cancer ther 11 : 2284 - 2293 , 2012 5 . 
ho dh , kim h , kim j , et al : leucine - rich repeat kinase 2 ( lrrk2 ) phosphorylates p53 and induces p21 ( waf1 / cip1 ) expression . 
gene 532 : 18 - 23 , 2013 yang d , li t , liu z , et al : lrrk2 kinase activity mediates toxic interactions between genetic mutation and oxidative stress in a drosophila model : suppression by curcumneurobiol dis 47 : 385 - 392 , 2012 8 . 
ho v , lim ts , lee j , et al : tlr3 agonist and sorafenib combinatorial therapy promotes immune activation and controls hepatocellular carcinoma progression . oncotarget 6 : 27252 - 27266 , 2015 10 . 
stable post - operative changes are seen , and there is no evidence of disease . 1 / 30 / 14 : afp decrease to 26 , 343 ng / ml but radiographic progression seen . sorafenib radiation surveillance 2 / 17 / 14 - 3 / 10 / 14 : received 40 gy in 16 fractions . 4 / 21 / 14 - 6 / 20 / 14 : sorafenib restarted at 200 mg twice daily . 
quantitative polymerase chain reaction ( qpcr ) analysis ( a ) and western blot ( b ) conrmed overexpression of wild - type ( wt ) lrrk2 and lrrk2 - k1316n ( mutant ) on four cell lines 72 hours after transfection . 
 telomerase is a prognostic marker of poor outcome and a therapeutic target in neuroblastoma andrea roderwieser , phd1 , 2 ; frederik sand , md1 ; esther walter , md1 ; janina fischer , md1 ; judith gecht , dmedsci1 ; christoph bartenhagen , phd1 , 2 ; sandra ackermann , phd1 , 2 ; felix otte1 ; anne welte1 , 2 ; yvonne kahlert1 , 2 ; daniela lieberz , phd1 ; falk hertwig , phd3 ; h . 
christian reinhardt , md2 , 4 ; thorsten simon , md1 ; martin peifer , phd2 ; monika ortmann , md2 ; reinhard b uttner , md2 ; barbara hero , md1 ; roderick j . 
osullivan , phd5 ; frank berthold , md1 ; and matthias fischer , md1 , 2 purpose telomere maintenance is a hallmark of high - risk neuroblastoma ; however , the contribution of telomerase and alternative lengthening of telomeres ( alt ) to clinical phenotypes has remained unclear . 
the presence of activated telomerase ( ie , tert rearrangements , mycn amplication , or high tert expression without these alterations ) was associated with poorest overall survival and was an independent prognostic marker in multivariable analyses . 
we also found that the telomerase - interacting compound 6 - thio - 2 ( cid : 1 ) - deoxyguanosine effectively inhibited viability and proliferation of neuroblastoma cells bearing activated telomerase . 
 roderwieser et al context key objective to determine the prognostic value of telomerase activation in primary neuroblastoma and to evaluate telomerase as a therapeutic target in preclinical neuroblastoma models . knowledge generated alterations associated with telomerase activation ( ie , tert rearrangements , mycn amplication , or elevated tert expression levels in the absence of these alterations ) occur in approximately one - third of primary neuroblastomas . 
the telomerase - interacting compound 6 - thio - 2 ( cid : 1 ) - deoxyguanosine efciently inhibits growth of telomerase - positive neuroblastoma cell lines in vitro and in vivo . relevance telomerase activation predicts adverse outcomes in primary neuroblastoma and may thus contribute to improving risk estimation for patients with neuroblastoma . 
preclinical studies establish telomerase as a promising therapeutic target in telomerase - positive neuroblastoma , suggesting that telomerase - interacting compounds should be evaluated in clinical trials . represent a therapeutic target in affected patients.9 in line with this notion , studies have reported on high levels of telomerase activity in unfavorable neuroblastoma phenotypes in a limited number of patients.10 - 12 by contrast , inactivating atrx mutations along with activation of the alternative lengthening of telomeres ( alt ) pathway and low tert mrna levels have been identied in a separate high - risk subgroup lacking mycn and tert alterations.6 , 13 in addition , we recently demonstrated that telomere maintenance mechanisms , in general , are a hallmark of high - risk neuroblastoma.14 it has remained unclear , however , whether telomerase and alt activation delineate distinct clinical subgroups and whether activated telomerase is a suitable therapeutic target in neuroblastoma . here , we set out to assess the prognostic value of biomarkers indicating telomerase or alt activation in patients with neuroblastoma and to examine the potential relevance of telomerase as a molecular target in this malignancy . 
to this end , we determined the genomic status of tert and mycn , characteristics of alt as well as tert expression levels in large cohorts of pretreatment neuroblastomas , and examined their association with prognostic markers and patient outcome . we also assessed growth characteristics of neuroblastoma cell lines on treatment with different telomeraseinteracting compounds in vitro and in vivo . 
we found that tert rearrangements occurred exclusively in patients age 18 months or older at diagnosis ( n = 46 of 254 [ 18.1% ] ; fig 1b ) , and they were not associated with being older than 5 years at diagnosis ( n = 11 of 66 [ 16.7% ] ; appendix fig a2a )  . 
tert rearrangements were predominantly detected in stage 4 disease and mycnnonamplied tumors ( n = 41 of 218 [ 18.8% ] and n = 41 of 361 [ 11.4% ] , respectively ; fig 1b ) , and were also associated with genomic losses at chromosome 1p and 11q ( appendix fig a2a )  . 
in addition , the presence of tert rearrangements was strongly associated with high - risk disease according to the international neuroblastoma risk stratication system17 ( n = 41 of 220 [ 18.6% ] ; fig 1b )  . outcome of patients whose tumors harbored tert rearrangements was poor in terms of event - free survival ( efs ) and overall survival ( os ) , and similar to that of patients whose tumors carried mycn amplication ( fig 1c )  . 
the prognostic relevance of tert rearrangements was substantiated by multivariable analyses , in which the presence of such alterations predicted adverse os independently of the established variables stage , age , and mycn and 1p status , which are currently used for patient risk assessment in germany18 ( p = .050 ; fig 1d , data supplement )  . 
we also validated that tert rearrangements and mycn amplication were strongly associated with elevated tert mrna levels in neuroblastoma in a large cohort of 379 neuroblastoma tumors14 ( fig 1e )  . alt denes an unfavorable patient subgroup that differs from patients with telomerase - positive neuroblastoma activation of the alt pathway has been suggested to be a marker of poor outcome in neuroblastoma13 ; however , its overall prevalence and its association with patient characteristics and courses have largely remained unclear . therefore , we assessed apbs , a hallmark of alt - positive tumors , in 273 of 457 neuroblastomas ( fig 2a ; table 1 ; appendix fig a1 ; data supplement )  . 
apbs were observed mainly in tumors of patients age 18 months or older at diagnosis ( n = 47 of 159 [ 29.6% ] ; fig 2b ) and occurred in approximately half of the patients who were older than 5 years at diagnosis ( n = 18 of 38 [ 47.4% ] ; appendix fig a2b )  . 
in addition , genomic alterations of atrx were identied in eight of 109 evaluable cases ( 7.3% ) , all of which were apb positive , whereas no atrx mutations were found in 12 additional apb - positive cases that ( 11.0% ; data supplement )  . 
as expected , 14 apbs were associated with low tert expression levels and increased telomere length ratios , which is in line with alt activation ( appendix fig a3a and a3b )  . telomerase and alt activation discriminate subgroups of patients with neuroblastoma with distinct outcome in our previous studies , we had observed that a small number of neuroblastomas harbored elevated tert expression levels and increased telomerase activity despite lacking genomic alterations of tert and mycn.14 therefore , we had dened a tert expression threshold that identied tert and mycn wild - type tumors whose tert mrna levels were comparable to those of tumors bearing tert or mycn alterations , referred to as tert hi14 . 
in the current study , we applied this threshold to the cohort for which information on genomic tert and mycn alterations and alt and tert expression was available ( n = 223 )  . 
the tert hi cohort consisted of 10 tumors ( 4.5% ; appendix fig a3a ) , which all were derived from patients age 18 months or older and mainly from stage 4 disease ( data supplement )  . 
outcome of these patients was as poor as that of patients with neuroblastomas bearing tert rearrangements and worse than that of patients with mycnamplied or alt - positive tumors ( appendix fig a4 )  . furthermore , we found three tumors positive for alt showing high tert expression levels ; it remains unclear , therefore , whether these tumors depend on alt or telomerase activation . together , our ndings suggest that telomerase activation , resulting from tert rearrangements , mycn amplication , or alternative events , may constitute a mechanistically dened clinical subgroup in neuroblastoma . 
telomerase activation was strongly associated with stage 4 , age older than 18 months at diagnosis , loss of 1p , and high - risk disease ( fig 3a )  . 
by contrast , absence of both telomerase activation and alt ( ie , absence of telomere maintenance mechanisms ) was predominantly associated with age younger than 18 months at diagnosis , stages 1 to 3 and 4s , and nonhigh - risk disease ( appendix fig a5 )  . 
tert mrna levels were slightly higher in tumors with complete response compared with tumors with partial response or stable disease ( appendix fig a6a )  . this nding was probably mainly due to better responses of mycn - amplied tumors ; however , the data might also suggest that alt - positive tumors are more indolent in response to induction therapy than tumors with telomerase activation ( appendix fig a6b )  . 
additional studies on larger patient cohorts are needed to address this question denitely . efs of patients whose tumors bore telomerase activation was similar to that of patients with alt - positive tumors and signicantly worse than that of patients whose tumors lacked telomere maintenance mechanisms ( fig 3b )  . 
by contrast , os of patients with telomerasepositive neuroblastomas was poorer than that of patients with alt - positive and telomere maintenancenegative tumors ( fig 3b )  . in multivariable analysis based on efs , both telomerase activation and alt were independent prognostic markers in addition to age , whereas only telomerase and age were independent prognostic markers in multivariable analysis based on fig 1 . 
 ( d ) multivariable cox regression analysis of patients with neuroblastoma ( n = 457 ) for os considering the following variables : age , stage , mycn status , 1p status , and tert status . 
 ( a ) detection of alt - associated pml nuclear bodies ( apbs ) indicating alt by combined telomere uorescent in situ hybridization and direct pml immunouorescence in tumor cells of sample nbc - 16 . 
 ( a ) frequencies of telomerase activation ( ie , mycn amplication , tert rearrangements , or tert hi ) in patient subgroups dened by stage ( blue , stage 4 ; red , stages 1 to 3 , 4s ) , age ( blue , 18 months or older ; red , younger than 18 months ) , risk group ( blue , hr ; red , nhr ) , 1p status and 11q status ( blue , deletion or imbalance [ del / im ] ; red , normal )  . 
 ( c ) multivariable cox regression analysis of neuroblastoma patients ( n = 223 ) for efs and os considering the following variables : age , stage , 1p status , telomerase activation , and alt . 
growth characteristics and dna damage signaling analysis of neuroblastoma cell lines with 6 - thio - 2 ( cid : 1 ) deoxyguanosine ( 6 - thio - dg ) treatment . 
 clinical relevance of telomerase activation in neuroblastoma telomerase is a therapeutic target in telomerase - activated neuroblastoma because telomerase activation denes a large group of high - risk neuroblastomas with poor outcome , we evaluated its potential value as therapeutic target in vitro and in vivo . 
to this end , the growth inhibitory effect of three different telomerase - interacting compounds ( 6 - thio - dg , 19 bibr - 1532 , 20 , 21 and costunolide22 ) was assessed in lines bearing tert rearhuman neuroblastoma cell rangements or mycn amplication , as well as altpositive cell lines and normal human bj broblasts as control . 
using two different assays , we found that cell viability upon treatment with 6 - thio - dg was impaired more effectively in telomerase - positive than in altlines and bj cells ( fig 4a - 4d ; appendix positive cell fig a7 )  . 
bibr - 1532 and costunolide treatment also reduced cell viability at lower concentrations in cell lines bearing telomerase activation than in alt - positive cell lines , using trypan blue exclusion assay ( appendix fig a8 ) ; however , this result was not conrmed for bibr1532 using a luminescent cell viability assay ( appendix fig a9 )  . 
moreover , growth inhibitory effects of these two compounds occurred in bj cells at similar or even lower concentrations in comparison with telomerase - positive cell lines , suggesting poor on - target specicity ( appendix fig a7 )  . 6 - thio - dg has been reported as a potent cytotoxic drug in telomerase - positive tumors that acts via telomere dysfunction leading to induction of apoptosis , reduction of proliferation , and senescence.19 , 23 - 25 therefore , we assessed the effect of 6 - thio - dg on apoptosis in telomeraselines . 
we obpositive and - negative neuroblastoma cell served a strong increase in apoptotic cells in cell line clb - ga , which harbors a tert rearrangement ( fig 4e and 4f ) , whereas the effect was less pronounced in the mycnamplied cell line imr - 32 ( fig 4g and 4h )  . 
by contrast , 6 - thio - dg treatment did not induce apoptosis in the altpositive cell line sk - n - fi ( fig 4i and 4j )  . 
this nding was supported by strong upregulation of cleaved caspase 7 in clb - ga , 25 whereas upregulation was weaker in imr - 32 cells and lacking in sk - n - fi ( fig 4k )  . 
we also examined levels of p21waf1 / cip1 as a marker of cell cycle arrest and found a strong and concentration - dependent p21waf1 / cip1 increase on 6 - thio - dg treatment in both telomerasepositive cell lines but not in alt - positive neuroblastoma cells ( fig 4k )  . line clb - ga , results from in vitro experiments suggested that 6thio - dg may represent a promising compound for the treatment of telomerase - positive neuroblastoma . 
to this end , the tert rearrangement - positive cell the two mycn - amplied cell lines be ( 2 ) c and imr - 32 , the tert hi cell line sh - sy5y , and the alt - positive cell line sk - n - fi were injected subcutaneously in immunodecient arthymic nude mice . 
growth of clb - ga and sh - sy5y cells was strongly impaired upon 6 - thio - dg treatment as compared with control animals , resulting in signicantly improved os of the treated mice ( fig 5a and 5b )  . 
in be ( 2 ) c xenografts , 6 - thio - dgtreated mice had signicantly better os , though the effect on tumor growth was moderate ( fig 5a and 5b )  . 
by contrast , 6 - thio - dg treatment had no effects on tumor growth or survival in imr - 32 and sk - n - fi xenograft models ( fig 5a and 5b )  . discussion in this study , we demonstrated that telomerase is activated in a large group of patients with high - risk neuroblastoma with poor outcome , who may thus potentially lines treated with fig 4 . 
because of limited compound effects , a growth inhibition curve could not be calculated for the alternative lengthening of telomeres ( alt ) - positive cell line chla - 90 . 
all experiments were performed in triplicate in at least two independent experiments . ( c ) cell viability determined by celltiter - glo assay ( promega , madison , wi ) in neuroblastoma cell lines treated with various concentrations of 6 - thio - dg . 
 ( k ) protein expression levels of p21waf1 / cip1 and cleaved caspase 7 after treatment with various concentrations of 6 - thio - dg for 48 hours , as determined by western blot analysis ; - actin was used as loading control . 
overall , approximately 10% and 20% of untreated tumors harbored tert rearrangements and mycn amplication , respectively , both of which have been shown to induce tert expression.6 , 26 in addition , tert mrna levels were elevated in approximately 4% of untreated tumors that lacked genomic aberrations of tert or mycn . 
all three alterations occurred mutually exclusively and were associated with similarly poor patient outcome . moreover , we have shown previously that enzymatic activity of telomerase is elevated in tumors of these subgroups.6 , 14 thus , neuroblastoma with tert or mycn alterations or high tert expression in the absence of these alterations may be considered as a single clinical subgroup that is dened by telomerase activation . 
telomerase activation was also a strong prognostic marker thus emphasizing its potential value for neuroblastoma risk assessment.10 in multivariable analyses , in addition , we found that alt occurs in approximately one - sixth of primary neuroblastomas . 
this nding is in line with those of a previous report suggesting that alt activation may be associated with a more indolent but eventually deadly course of the disease.13 in fact , we observed that os of patients with alt - positive tumors plateaued at 10 years , whereas that of patients with telomerase - positive tumors remained stable after 5 years ( fig 3b )  . 
together , our ndings indicate that telomerase and alt activation are strong and independent prognostic markers in neuroblastoma ( fig 3c ) and suggest these alterations may be considered for patient risk assessment formation on telomere maintenance with additional molecular data , such as copy number alterations , gene expression proles , or ras and p53 pathway gene mutations , 14 , 27 , 28 may rene clinico - genetic classication of neuroblastoma in future studies , ultimately allowing precise risk estimation and treatment in clinical practice . integration of stratication of patients solely on the basis of a dened set of biomarkers . in addition , we demonstrated that telomerase represents a potential therapeutic target in patients with telomerasepositive neuroblastoma , who have poor outcome with current treatment protocols . 
treatment of neuroblastoma cell lines with 6 - thio - dg impaired cell viability at signicantly lower concentrations in telomerase - activated than in altpositive cell lines and normal human broblasts , suggesting on - target specicity of this compound.19 , 23 - 25 , 29 , 30 the cytotoxic effect of 6 - thio - dg was obviously associated with induction of apoptosis and , potentially , with induction of cell cycle arrest . 
in neuroblastoma xenografts , 6 - thio - dg strongly impaired tumor growth of tert rearrangement - positive and tert hi neuroblastoma cells , whereas the inhibitory effect on mycn - amplied neuroblastoma was less pronounced . 
although the reason for these differences remains unclear , the broad effect of mycn on one may speculate that oncogenic pathways8 , 31 , 32 may counteract inhibition of single downstream molecules , such as telomerase . 
the distinct inhibitory effects may also be due to incorporation of a higher fraction of 6 - thio - dg into the genomic dna in mycn - amplied xenografts , related to different growth characteristics of these tumors , at least in the ultrafast growing sk - n - be ( 2 ) c xenografts . 
it has been demonstrated that 6 - thio - dg is incorporated into telomeres and genomic dna , whereas the toxic effects of 6 - thio - dg are elicited primarily by incorporation into telomeres.19 thus , higher doses of 6 - thio - dg might be required for efcient growth inhibition in very - fast - growing neuroblastomas . 
this suggestion is supported by the observation that 6 - thio - dg increased the probability of animal survival signicantly in mycn - amplied sk - n - be ( 2 ) c xenografts , whereas no growth inhibitory effects were observed in mycn - amplied imr - 32 tumors ( fig 5 )  . 
christian reinhardt , matthias fischer financial support : matthias fischer administrative support : reinhard b uttner , matthias fischer provision of study material or patients : janina fischer , h . 
osullivan , frank berthold , matthias fischer collection and assembly of data : andrea roderwieser , frederik sand , janina fischer , felix otte , anne welte , thorsten simon , monika ortmann , reinhard b uttner , barbara hero , frank berthold , matthias fischer data analysis and interpretation : andrea roderwieser , esther walter , janina fischer , judith gecht , christoph bartenhagen , sandra ackermann , yvonne kahlert , daniela lieberz , falk hertwig , martin peifer , reinhard b uttner , barbara hero , roderick j . 
christian reinhardt consulting or advisory role : abbvie , astrazeneca , vertex , merck research funding : gilead sciences thorsten simon consulting or advisory role : eusa pharma ( inst ) , merck ( inst ) reinhard b uttner stock and other ownership interests : targos molecular pathology , tamp honoraria : astrazeneca , abbvie , bayer , bristol - myers squibb , boehringer ingelheim , merck serono , msd , novartis , qiagen , pzer , roche research funding : roche ( inst ) frank berthold consulting or advisory role : ymabs pharmaceuticals , united therapeutics matthias fischer consulting or advisory role : novartis honoraria : janssen - cilag no other potential conicts of interest were reported . acknowledgment we thank the patients and their parents for making available the tumor specimens analyzed in this study . 
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 appendix roderwieser et al neuroblastoma cohort tert cohort ( n = 457 ) analysis of tert rearrangements alt cohort ( n = 273 ) telomerase cohort ( n = 223 ) analysis of tert rearrangements and apbs analysis of tert rearrangements , apbs , and gene expression fig a1 . 
a cohort of 457 patients with neuroblastoma was analyzed for the presence of tert rearrangements . for 273 of these 457 patients , activation of the alternative lengthening of telomeres ( alt ) pathway was examined . 
 ( a ) frequencies of tert rearrangements ( tert - ra ) in patient subgroups dened by age ( blue , 5 years or older ; red , younger than 5 years ) , and chromosome 1p and 11q copy number status ( blue , deletion or imbalance [ del / im ] ; red , normal )  . 
tumors were categorized according to the presence of tert rearrangements , mycn amplication , alternative lengthening of telomeres ( alt ) , elevated tert expression in the absence of tert or mycn alterations ( tert hi ) , or lack of telomere maintenance mechanisms ( others )  . patients whose tumors were both alt positive and tert hi were excluded from analysis . 
 ( b ) telomere length ratios of tumors and matched normal controls ( computed from whole genome sequencing and whole exome sequencing data14 ) in tumor subgroups dened by tert rearrangements , mycn amplication , alt , or lack of these alterations ( others )  . 
frequencies of absence of telomere maintenance mechanisms in patient subgroups dened by age ( blue , 18 months or older ; red , younger than 18 months ) , stage ( blue , stage 4 ; red , stages 1 to 3 , 4s ) , and risk group ( blue , hr ; red , nhr )  . 
 ( a ) association of tert expression levels as determined by microarrays in neuroblastomas ( n = 83 ) according to residual / stable disease or complete response of metastases at the end of induction therapy . 
 ( b ) frequencies of tert rearrangements ( blue , tert - ra ; red , tert - wt ) , mycn amplication ( blue , mycn amplied ; red , nma ) , and alt activation ( blue , alt pos ; red , alt neg ) in patients with residual / stable disease at the end of induction therapy . 
relative cell viability determined by celltiter - glo assay in human normal bj broblasts treated with various concentrations of 6 - thio - 2 ( cid : 1 ) deoxyguanosine ( 6 - thio - dg ) , bibr - 1532 , and costunolide . 
 mutational signature and transcriptomic classification analyses as the decisive diagnostic tools for a cancer of unknown primary roger olofsson bagge akif demir joakim karlsson babak alaei - mahabadi purpose cancer of unknown primary is a group of metastatic tumors in which the standard diagnostic workup fails to identify the site of origin of the tumor . 
the potential impact of precision oncology on this group of patients is large , because actionable driver mutations and a correct diagnosis could provide treatment options otherwise not available for patients with these fatal cancers . 
nilsson , phd , goteborgs universitet sahlgrenska akademin , sahlgrenska cancer center , medicinaregatan ( continued ) patients and methods here we describe a patient whose tumor was misdiagnosed at least three times . 
next - generation sequencing , a patient - derived xenograft mouse model , and bioinformatics were used to identify an actionable mutation , predict resistance development to the targeted therapy , and correctly diagnose the origin of the tumor . 
transcriptomic classification was benchmarked using the cancer genome atlas ( tcga )  . results despite the lack of a known primary tumor site and the absence of diagnostic immunohistochemical markers , the origin of the patients tumor was established using the novel bioinformatic workflow . 
2018 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license : introduction massively parallel sequencing of tumor dna and rna offers new possibilities to identify actionable mutations and enables precision medicine in the clinic.1 , 2 identification of a high mutational load ( eg , resulting from carcinogen exposure or dna repair defects3 ) can also provide information on increased responsiveness to immunotherapies , such as antiprogrammed death 1 antibodies.4 trials such as the nci - match ( national cancer institute molecular analysis for therapy choice ) trial , the tapur ( targeted agent and profiling utilization registry ) study , and the nct - master ( molecularly aided stratification for tumor eradication ) study5 , 6 include next - generation sequencing ( ngs ) to identify actionable mutations and will generate new data to inform future trial designs or best clinical practice . 
because their prognosis is poor , 7 patients may benefit significantly from extended genomic analysis not only for identification of targeted treatments but also for identification of the primary site of the tumor.8 , 9 targeted therapies directed against a particular driver mutation can act differently in different tumor types10 ; therefore , it may be beneficial to identify both the actionable mutation and the primary tumor site . here we describe an unusual case of a patient seeking a second opinion while receiving therapy with pembrolizumab for a presumed lung cancer . 
however , a subsequent fluorescent in situ hybridization analysis failed to confirm the alk positivity , and re - evaluation of the original specimen suggested instead a largecell neuroendocrine carcinoma of the lung . at the patients request , the cell block sections were re - examined in may 2016 at the sahlgrenska university hospital in sweden . 
cytologic and immunohistochemical ( ihc ) examination of the original specimen suggested a malignant neuroendocrine neoplasm ( nen ) , possibly a malignant paraganglioma ( pgl ) with differential diagnoses being gangliocytic neuroblastoma , malignant melanoma , merkel cell carcinoma , carcinoid , and small - cell lung cancer ( fig 1 )  . 
 analysis of an extirpated subcutaneous metastasis revealed that the tumor was positive for the neuroendocrine markers tyrosine hydroxylase ( th ) , chromogranin a , synaptophysin ( syn ) , neu - n , and cd99 , as well as for the neural crest markers sox10 and s100 . 
in contrast , the tumor was negative for cytokeratins as well as the melanoma markers tyrosinase , hmb45 ( pmel ) , and melan - a ( fig 1 ; appendix figs a1 to a3 )  . 
a patient - derived xenograft ( pdx ) mouse model was generated as previously described11 from the subcutaneous metastasis , and the xenograft was also positive for th , syn , sox10 , and s100 ( fig 1 )  . 
taken together , these analyses argue for a nen of unknown primary , which accounts for > 10% of these diagnoses.12 urinary dopamine levels were transiently elevated ( approximately three times the upper limit of normal ) , but repeated measurements of plasma metanephrines ( including metoxytyramine ) were negative , arguing against a primary pgl . 
ngs and multiplex ligation dependent probe amplification analyses of genes previously associated with hereditary pgl were all negative , 13 , 14 and there was no family history of pgl . 
array comparative genomic hybridization and whole - genome sequencing analyses of the metastasis revealed an aneuploid tumor with copy number alterations preferentially affecting whole chromosomes and chromosome arms , including gain of 1q , 2 , 7 , 8 , 9p24.3 - p23 , 9q , 13 , 15 , 16 , 20 , and 21 and loss of 1p , 9p23 - p13.2 ( homozygous loss of cdkn2a ) , 10 , and 18 ( fig 2a and 2b ; appendix table a1 ; data supplement )  . 
morphologic and immunohistochemical characteristics of the cell block from the ( a - f ) second opinion endobronchial ultrasound - guided aspiration , ( g - l ) subcutaneous metastatic lesion , and ( m - r ) patient - derived xenograft model . 
 [ 18f ] fluorodeoxyglucosepositron emission tomography / ct examination at sahlgrenska university hospital ( fig 3a ) showed progression , and the patient had clinical symptoms of stridor and shortness of breath . 
both were negative , ruling out the use of metaiodobenzylguanidineor peptide receptormediated radionuclide therapy . after a multidisciplinary conference in august 2016 , the patient started with the braf inhibitor ( brafi ) dabrafenib ( based on the v600e mutation )  . 
a rapid partial response was observed , with shrinkage of the subcutaneous metastases , disappearance of clinical symptoms including the stridor , and metabolic response on [ 18f ] fluorodeoxyglucosepositron emission tomography / ct after evaluation at 8 weeks ( fig 3a )  . 
unfortunately , he rapidly deteriorated ; a ct brain scan revealed massive progression of the brain metastases , and the patient died shortly thereafter . in the pdx model generated from the subcutaneous metastasis , treatment with the brafi dabrafenib alone or in combination with the meki trametinib was tested . 
notably , there was no effect of the brafi alone , whereas in two of three mice , the combination treatment led to markedly slower disease progression , which correlated with a reduction of phosphorylation of the mek target erk ( fig 3b )  . 
the lack of complete inhibition of erk phosphorylation could be explained by extended analyses of the genome sequencing of the subcutaneous metastasis , which revealed p124l and f53l mutations in map2k1 ( encoding mek1 ; fig 2d )  . 
these mutations have previously been associated with resistance to brafi in melanoma.17 comprehensive immunoprofiling to establish the correct diagnosis to diagnose this unusual case of presumed nen , additional morphologic and ihc analyses were performed ( appendix table a2 ; appendix figs a1 to a3 )  . 
analyses of all specimens , including the brain metastasis , showed that the tumor had partly epithelioid and partly elongated cells , with moderate nuclear pleomorphism but no prominent nucleoli , squamous differentiation , or gland formation . 
 ( a ) somatic copy number variants ( cnvs ) , single - nucleotide variants ( snvs ) , expressed fusion genes ( thick green lines ) , and somatic structural variants revealed by whole genome sequencing and ( b ) array comparative genomic hybridization . 
 ( c ) somatic variants detected with whole - genome and rna sequencing in braf ( v600e ) and ( d ) map2k1 ( p124l and f53l )  . carcinoma , malignant pgl , neuroblastic tumor , or malignant melanoma could be entertained . 
although such cells may be lost in malignant forms , and these may also have a more diffuse growth pattern , the extent of atypia and necrosis and the complete lack of nesting and sustentacular cell pattern would be unusual . 
a neuroblastic tumor would be unusual at the patients age and with this dissemination pattern , and the lack of ganglion cell differentiation and nb84 expression is not compatible with this diagnosis . 
lack of such differentiation may occur in undifferentiated neuroblastoma , but the patients tumor did not show the typical small blue round - cell tumor pattern characteristic of this entity . 
neural and neuroendocrine differentiation , as exemplified by focal reactivity for syn , chromogranin - a , and th , has been noted in melanoma18 but has always been accompanied by at least one of the melanoma markers hmb45 , tyrosinase , or melan - a . 
 ( a ) tumor load in patient visualized on [ 18f ] fluorodeoxyglucose ( [ 18f ] fdg ) positron emission tomography / computed tomography at baseline ( top panels ) and after 3 months of treatment with the braf inhibitor dabrafenib ( bottom panels )  . 
 ( b ) patient - derived xenograft ( pdx ) model in nonobese severe combined immune - deficient interleukin - 2 chain receptor knockout mice ( nog mice )  . 
mutational signatures have emerged as powerful tools to determine the somatic mutational processes underlying the development of tumors.19 , 20 by calculating the frequencies of base substitutions across the genome , we observed a dominance of c > t transitions that preferentially occurred in dipyrimidine trinucleotide contexts ( fig 4a ) and that were biased toward the untranscribed strand ( poisson test , false discovery rate < 0.05 ) in both the skin and brain metastases . 
this pattern closely matched a known mutational signature from the catalogue of somatic mutations in cancer ( signature 7 ) associated with ultraviolet radiation ( uv ) induced damage ( fig 4a ) , which is only found in cancers originating from sun - exposed areas.19 , 20 a decomposition of the mutational spectrum into known mutational signatures , using the mutationalpatterns r package , 21 yielded an estimated 80% contribution from signature 7 in both samples . 
these results strongly indicate that the primary tumor had originated from the skin . the classic melanoma markers tyr , pmel , and mlana and the merkel cell carcinoma marker cytokeratin 20 were all negative , both by ihc analyses and by rna sequencing ( rna - seq )  . 
therefore , we instead compared the transcriptome of the present tumor with that of 9 , 583 other tumors from 32 cancer types sequenced by the cancer genome atlas ( tcga ) consortiunotably , for both the skin and brain metastases , the strongest correlating samples were melanomas ( fig 4b )  . 
dct and sox10 were also elevated in xenografts from brafi - treated mice , which correlated with suppression of the neuroendocrine markers chgb , th , and eno2 ( appendix fig a4 ; data supplement )  . 
taken together , our findings of an uv - induced mutational signature , braf / map2k1 / cdkn2a mutations , the dissemination pattern , the expression of s100 and sox10 , and the correlation with the transcriptome profiles of tcga melanomas strongly indicated that the present tumors represented metastases from an unknown primary melanoma with neuroendocrine differentiation . pan - cancer transcriptome - based classification can predict the cellular origin of a tumor to investigate how transcriptome - based classification performance generalizes beyond the present case , we performed leave - one - out cross validation of k nearest neighbor classification on the pan - cancer data set , varying the number of nearest neighbors ( k ) considered , in terms of spearman correlation , from one to 50 ( appendix )  . 
however , certain cancers were more difficult to predict than others ; for example , rectal and colon adenocarcinomas were difficult to distinguish , as were squamous carcinoma of the lung , squamous carcinoma of the head and neck , and bladder cancer , which share molecular characteristics22 ( fig 5a )  . an additional evaluation was performed on an independent set of previously published data11 and unpublished rna - seq data of melanoma pdxs , uveal melanoma metastases , and one lung adenocarcinoma , yielding an overall accuracy of 0.84 ( appendix fig a5c )  . 
 ( a ) trinucleotide substitution frequencies observed in exonic regions of whole - genome sequencing data from the skin ( top ) and brain metastases ( middle ) , as well as the ultraviolet radiation ( uv ) - associated reference signature from catalogue of somatic mutations in cancer ( bottom )  . 
acc , adrenocortical carcinoma ; blca , bladder urothelial carcinoma ; brca , breast invasive carcinoma ; cesc , cervical squamous cell carcinoma and endocervical adenocarcinoma ; chol , cholangiocarcinoma ; coad , colon adenocarcinoma ; dlbc , lymphoid neoplasm diffuse large b - cell lymphoma ; esca , esophageal carcinoma ; gbm , glioblastoma multiforme ; hnsc , head and neck squamous cell carcinoma ; kich , kidney chromophobe ; kirc , kidney renal clear cell carcinoma ; kirp , kidney renal papillary cell carcinoma ; lgg , brain lower - grade glioma ; lihc , liver hepatocellular carcinoma ; luad , lung adenocarcinoma ; lusc , lung squamous cell carcinoma ; meso , mesothelioma ; ov , ovarian serous cystadenocarcinoma ; paad , pancreatic adenocarcinoma ; pcpg , pheochromocytoma and paraganglioma ; prad , prostate adenocarcinoma ; read , rectum adenocarcinoma ; sarc , sarcoma ; skcm , skin cutaneous melanoma ; stad , stomach adenocarcinoma ; tgct , testicular germ cell tumor ; thca , thyroid carcinoma ; thym , thymoma ; ucs , uterine carcinosarcoma ; ucec , uterine corpus endometrial carcinoma ; uvm , uveal melanoma . uveal melanomas were misclassified according to the organs where metastases were sampled , suggesting that normal tissue contamination could influence transcriptome - based predictions . 
 notably , however , both the skin and brain metastases of the present case were predicted to be melanoma by this classifier . ultraviolet radiation signature identifies incorrectly labeled tcga lung tumors to further study the utility of uv signature analysis in detecting misdiagnosed tumors , we investigated all squamous lung cancer samples in tcga . 
transcriptome - based analyses predicted one to be head and neck squamous cell carcinoma and the others to be lung squamous carcinomas ( fig 5a ; appendix fig a6a )  . 
melanoma could be ruled out by a lack of decisive melanoma markers and common driver mutations , as well as by high expression of the squamous / basal marker tp6325 ( appendix fig a6b )  . 
 although these samples still shared many catalogue of somatic mutations in cancer mutations with skin melanomas ( appendix fig a6c ) , this is likely explained by spuriously shared mutations with highly mutated tumors in general . 
 ( a ) t - distributed stochastic neighbor embedding ( tsne ) projection of the pan - cancer data set , together with the main case skin and brain metastasis samples , as well as the independent data set used for additional validation of the transcriptome - based classifier . 
notably , skin squamous and basal cell carcinomas are absent from tcga and therefore cannot be excluded as possible diagnoses for either of the three lung squamous cancers in tcga with an uv signature . 
the uv signature is a biomarker that can indicate an origin from a sun - exposed site . discussion here we demonstrate the application of mutational signature analysis and transcriptomic profiling as an adjunct in the diagnosis of a cup with neuroendocrine differentiation . 
although the tumor had a braf mutation , the morphology was ambiguous and atypical for malignant melanoma.27 at least three hospitals had misdiagnosed the tumor , because the following features did not support a melanoma diagnosis : the tumor in the thoracic region was believed to be the primary , and the patient had never had a skin lesion removed ; classic melanocyte markers were negative , whereas the tumor was positive for several neuroendocrine markers ; and s100 and sox10 were expressed , but these markers may also be expressed in nen . 
indeed , the possibility of a diagnosis of melanoma was confirmed by a specialist in nen pathology ( r.r.d.k. ) who was blinded to the genome analyses . we benchmarked the performance of transcriptome based cancer type classification according to our method using tcga data and found high accuracy in general . 
 although beyond the scope of our study to investigate , we expect that other signatures associated with site - specific carcinogen exposure , such as tobacco smoke , could also be found informative when deciphering the primary origin of tumors . current knowledge indicates that skin melanocytes may have two developmental origins : directly from the neural crest or via schwann cell progenitors ( scps ) migrating along nerves in the developing embryo.28 interestingly , scps also generate the chromaffin cells of the adrenal gland.29 it is therefore tempting to speculate that coexpression of the neuroendocrine markers th , chromogranin a , and syn in the present tumor was the result of a transformation event involving an scp - generated sox10 - positive / mitf - positive / dct - positive melanoblast . 
 ( d ) estimated contributions of the uv signature in samples from tcga head and neck squamous cell carcinoma ( hnsc ) cohort , with site of origin noted according to available clinical metadata . 
given the approval of targeted therapies and immunotherapies for melanoma and lung cancer , a change of diagnosis could have real clinical impact within a short timeframe . despite the incorrect diagnosis , we would argue that the treatments our patient received included those used in the clinical management of malignant melanoma , such as dabrafenib and pembrolizumab . 
one might argue that he should have received the dabrafenib and trametinib combination treatment upfront given the mapk1 mutation , 17 but at that time , this mutation was unknown to the clinician , and the diagnosis was pgl , meaning that dabrafenib was already off label . 
possibly , a recently postulated triple combination targeting braf , mek , and erk would have been beneficial in this case.30 in summary , this is to our knowledge the first case study where mutational signature analysis has been used as a decisive adjunct to routine histopathology to ascertain the diagnosis of metastatic deposits from a cup . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . roger olofsson bagge consulting or advisory role : amgen consulting or advisory role : bristol - myers squibb speakers bureau : roche joakim karlsson no relationship to disclose babak alaei - mahabadi no relationship to disclose berglind o . 
nilsson stock and other ownership interests : exocure ventures , oxcia travel , accommodations , expenses : merck sharp & dohme sweden acknowledgment this research would not have been possible without the cooperation of the patient and his close relatives , to whom we extend our sincere gratitude . 
sequence data generated for this study has been deposited at the european genome - phenome archive , which is hosted by the ebi and the crg under accession number egas00001003026 . 
wagle n , berger mf , davis mj , et al : high - throughput detection of actionable genomic alterations in clinical tumor samples by targeted , massively parallel sequencing . 
stadler zk , battaglin f , middha s , et al : reliable detection of mismatch repair deficiency in colorectal cancers using mutational load in next - generation sequencing panels . 
golfinopoulos v , pentheroudakis g , salanti g , et al : comparative survival with diverse chemotherapy regimens for cancer of unknown primary site : multiple - treatments meta - analysis . 
dasari a , shen c , halperin d , et al : trends in the incidence , prevalence , and survival outcomes in patients with neuroendocrine tumors in the united states . 
muth a , abel f , jansson s , et al : prevalence of germline mutations in patients with pheochromocytoma or abdominal paraganglioma and sporadic presentation : a population - based study in western sweden . 
hoadley ka , yau c , wolf dm , et al : multiplatform analysis of 12 cancer types reveals molecular classification within and across tissues of origcell 158 : 929 - 944 , 2014 23 . 
adameyko i , lallemend f , aquino jb , et al : schwann cell precursors from nerve innervation are a cellular origin of melanocytes in skcell 139 : 366 - 379 , 2009 29 . 
 appendix patient the patient received oral and written information and signed the informed consent according to the ethical approval at the regional ethical review board ( #289 - 12 )  . 
the patient and his relatives have approved the publication of this case report . immunohistochemical staining of tumor tissues biopsies from patient tumor and patient - derived xenograft ( pdx ) tumor were fixed in neutral buffered formalin and embedded in paraffsections ( 3 to 5 microns ) were placed on positively charged glass slides and subjected to antigen retrieval using envision flex target retrieval solution ( high power of hydrogen ; agilent technologies , santa clara , ca )  . 
the following primary antibodies were used : anti - alk ( clone alk1 ; dako ) , antibeta - catenin ( bd610154 ; becton dickinson , franklin lakes , nj ) , anti - cd56 ( clone 123c3 ; dako ) , anti - cd99 ( clone epr3097y ; epitomics , burlingame , ca ) , antichromogranin a ( clone lk2h10 ; millipore , burlington , ma ) , anti - cdx2 ( ab76541 ; abcam , cambridge , united kingdom ) , anticytokeratin 8 / 18 ( ncl - 5d3 ; leica , wetzlar , germany ) , anticytokeratin 20 ( clone ks20.8 ; dako ) , antihigh molecular weight cytokeratin ( clone ae1 / 3 ; dako ) , anti - hmb45 ( m0634 ; dako ) , anti - ki67 ( clone mib - 1 ; dako ) , antimelan a ( clone a103 ; dako ) , anti - nb84 ( ncl - nb84 ; leica ) , anti neu - n ( mab377 ; millipore ) , anti - nfp ( m0762 ; dako ) , anti - pax8 ( 10336 - 1 - ap ; proteintech , chicago , il ) , anti - s100 ( catalog no ir504 ; dako ) , anti - sox10 ( clone ep268 ; epitomics ) , antisynaptophysin ( clone dak - synap ; dako ) , anti - ttf1 ( clone spt24 ; novocastra , wetzlar , germany ) , and antityrosine hydroxylase ( clone 1b5 ; novocastra )  . extraction of dna and rna from tumor snap - frozen tumor pieces were homogenized using bullet blender ( next advance , troy , ny )  . 
dna and rna were extracted using the allprep dna / rna kit ( qiagen , hilden , germany )  . dna sequencingbased variant calling raw dna sequencing reads were aligned to the hg19 reference genome with bwa ( version 0.7.12 ; options mem and - m ; li h , et al : bioinformatics 25 : 1754 - 1760 , 2009 )  . 
the resulting bam files were recalibrated and indels were jointly realigned for the tumor and normal samples with gatk ( version 3.3.0 ; mckenna a , et al : genome res 20 : 1297 - 1303 , 2010 )  . 
variant calling was performed with gatk haplotypecaller on the tumor and normal sample separately and with mutect ( version 1.1.5 ; cibulskis k , et al : nat biotechnol 31 : 213 - 219 , 2013 ) on both samples paired . rna sequencingbased variant calling raw rna sequencing reads were aligned to the hg19 reference genome with star ( verison 2.5.2b ; dobin a , et al : bioinformatics 29 : 15 - 21 , 2013 ) in two passes , with the parameter sjdboverhang 125 . 
variant calling was subsequently performed using gatk haplotypecaller with the options - dontusesoftclippedbases , - stand_call_conf 20.0 , and - stand_emit_conf 20.0. variant filtering to obtain a sensitive set of whole - genome sequencing variant calls that included indels , the union of the gatk tumor and mutect somatic calls was first constructed . 
before the set operations , the variant vcf files were left normalized using bcftools ( two steps : options norm - m - both in the first , and norm f human_g1k_v37.fasta in the second ; the reference fasta file was obtained from the gatk resource bundle )  . 
subsequently , the sets were annotated with annovar ( wang k , et al : nucleic acids res 38 : e164 , 2010 ) to identify and discard all variants present with 1% frequency in either the 1000 genomes database ( version august 2015 ; 1000g2015aug_all ) or esp6500 ( esp6500siv2_all ) or listed in a version of dbsnp 138 , from which flagged somatic and clinically associated variants had been removed ( snp138nonflagged )  . 
 mutational signature analysis variants detected by whole - genome sequencing , as described under dna sequencingbased variant calling , were annotated using annovar ( as described ) , after which all variants that were either nonexonic or present in the snp138nonflagged , esp6500siv2_all , or 1000g2015aug_all databases were removed . 
the principle behind the fitting algorithm is to find the nonnegative linear combination of the predefined mutational signatures that best explains all mutations in a given sample , which is done by solving a nonnegative least squares optimization problem.21 this allowed the estimation of the relative contributions of the known mutational signatures in a given sample . 
p values were adjusted using the benjamini - hochberg method . for mutational signature analysis of the cancer genoma atlas ( tcga ) tumors , annotated somatic mutation calls ( mutect2 ) in vcf format on the basis if whole - exome sequencing data were downloaded for 561 lung squamous cell carcinoma ( lusc ) and 528 head and neck squamous cell carcinoma tumors from the genomic data commons portal ( gov / ; accessed on november 24 , 2017 , and february 26 , 2018 , respectively )  . 
gene read counts were derived with htseq - count ( parameters : - m intersection - strict - s no ; anders s , et al : bioinformatics 31 : 166 - 169 , 2015 )  . 
reads per kilobase per million normalized values were calculated , taking into account the max mature transcript length of each gene and using robust size factors as previously described for the deseq method ( anders s , et al : genome biol 11 : r106 , 2010 )  . 
 implementation and cross - validation of transcriptome - based cancer type classification to classify a sample using the k - nearest neighbor approach , spearman correlation coefficients were first calculated between the sample of interest and all samples in the tcga pan - cancer data set . 
leave - one - out cross - validation was performed by in turn excluding each sample from the tcga data set and classifying it using correlations to the remaining samples . 
the final classifier was then subjected to additional validation on an independent data set composed of 30 skin melanoma pdxs , 13 uveal melanoma metastases ( four skin and nine liver ) , and one lung adenocarcinoma primary tumor sample , all preprocessed and normalized as described for the main case samples . 
only mutations in cancer gene census genes listed in the catalogue of somatic mutations in cancer and annotated as missense_mutation , nonsense_mutation , nonstop_mutation , in_frame_ins , in_frame_del , frame_ shift_ins , or frame_shift_del and found in any of the three lusc samples were included . 
for additional removal of germ line variants , we first used the somatic call function with the - f parameter where the discord files were generated from seven normal genomes ( unpublished data ) and then removed events in which both breakpoints overlapped with known population variants the database of genomic variants database ( macdonald jr , et al : nucleic acids res 42 : d986 - d992 , 2014 )  . array - based comparative genomic hybridization genomic dna was extracted from fresh - frozen tumor tissues of the subcutaneous and brain metastases as previously described ( persson f , et al : oncogene 27 : 3072 - 3080 , 2008 )  . 
array comparative genomic hybridization ( cgh ) analysis was performed using the human genome cgh microarray 244k oligonucleotide arrays ( g4411b ; agilent technologies ) as recommended by the manufacturer . 
slides were scanned using an agilent high - resolution c microarray scanner , followed by data extraction and normalization using feature extraction ( version 12.0.1.1 ; agilent technologies ) with linear normalization ( protocol cgh_1200_jun14 )  . 
 generation of a pdx model a 3 3 3 mm piece of a biopsy of a subcutaneous metastasis of the patient was transplanted into the flank of immunocompromised , nonobese severe combined immune - deficient interleukin - 2 chain receptor knockout mice ( nog mice ; taconic , copenhagen , denmark ) to form xenografts . 
when the first pdx tumor reached 150 mm3 , it was passaged to new mice ( passage 2 ) , which subsequently were passaged to 10 mice , where tumor finally grew in eight mice ( passage 3 )  . 
these mice were treated 5 days per week for a minimum of 3 weeks with either vehicle or trametinib 0.3 mg / kg twice per day ( selleck chem , houston , tx )  . 
all animal experiments were performed in accordance with eu directive 2010 / 63 ( regional animal ethics committee of gothenburg approval #36 - 2014 )  . rna sequencing analysis of drug - treated pdx models rna sequencing reads were aligned to a combined human ( hg19 ) and mouse ( mm10 ) reference genome using star , with default settings . 
read counts were then binned to genes using the htseq ( version 0.6.0 ; zhao m , et al : nucleic acids res 44 : d1023 - d1031 , 2016 ) command htseq - count ( parameters - s reverse and - m intersection - strict ) , as well as the human reference genome annotation gencode ( version 17 )  . 
differential expression analysis was carried out using deseq2 ( cancer genome atlas network : nature 517 : 576 - 582 , 2015 ) , with the parameter alpha = 0.05 , considering vehicle - treated and untreated mice both as controls relative to the dabrafeniband trametinib - treated samples . 
enrichment analyses were carried out using msiddb ( love mi , et al : genome biol 15 : 550 , 2014 ) , using gene ontology biological process gene sets ( anders s , et al : bioinformatics 31 : 166 - 169 , 2015 ) , considering genes with an absolute log2 fold change > 2 and adjusted p values < .01. 
differential expression analysis of ( a ) dabrafenib - treated mice compared with vehicle and untreated controls and ( b ) dabrafenib and trametinib combinationtreated mice compared with vehicle and untreated controls . 
 ( a ) classification error ( defined as 1 - accuracy ) per cancer type obtained during leave - one - out cross - validation of the k - nearest neighbor classification approach on the cancer genome atlas data set , with spearman correlation coefficients calculated using all coding genes as the measure of similarity between samples . 
 ( c ) performance with k = 6 on an independent validation set , using unrelated skin melanoma patient - derived xenograft models , uveal melanoma skin and liver metastasis samples , and one lung adenocarcinoma primary tumor . 
 ( a ) tcga cancer types ranked by mean spearman correlation of the top six most strongly correlating samples in each cohort : tcga - 21 - 1079 ( top ) , tcga - 90 - a4ed ( middle ) , and tcga - 18 - 3409 ( bottom )  . 
 ( b ) expression of selected marker genes relevant when considering a melanoma diagnosis : tcga - 21 - 1079 ( top ) , tcga - 90 - a4ed ( middle ) , and tcga - 18 - 3409 ( bottom )  . 
 ( c ) frequency of each driver gene mutation found in the ultraviolet radiationassociated lusc tumors , in each of the different tcga cancer types , relative to the total number of samples in each cohort . 
2 , 3 we used our recently reported in silico tool ( dpyd - varifier ) 7 to predict that p.t132a would be deleterious to function , which was subsequently validated using ex vivo and in vitro approaches . 
these methodologies permitted us to determine an activity score for the patient that was used to calculate a safe adjusted dose of fu for adjuvant therapy . this study was approved by the mayo clinic institutional review board . 
dpyd - varifier was used to predict the function of p.t132a.7 the effect of p.t132a on dpd activity was measured in vitro as previously described.5 - 7 total rna was isolated from the patients blood sample using the paxgene blood rna kit ( preanalytix , hombrechtikon , switzerland ) , and cdna was reverse transcribed using oligo ( dt ) 15 primers ( thermo fisher scientific , waltham , ma )  . 
the full - length dpyd open reading frame was amplified ( primers : 5 - gtttgtcactggcagactcg - 3 , 5 - ttcacagcaactgtttcacaaa - 3 ) using q5 high fidelity dna polymerase ( new england biolabs , ipswich , ma )  . 
the polymerase chain reaction ( pcr ) product was cloned into the pjet1.2 vector , and 20 cloned constructs were sequenced at the mayo clinic gene analysis shared resource to determine the cis or trans conformation of the variants . 
peripheral blood mononuclear cells ( pbmcs ) were isolated and assessed ex vivo for dpd activity as previously described.9 , 10 additional pcr and quantitative pcr reactions were performed with primers specific to canonically ( e13 / 14 : 5 - ctcttgataaggacattgtgacaaa - 3 , 5 - tttgcagctcttgcgatgc - 3 ) and alternatively spliced dpyd ( e13 / 15 : 5 - ctcttgataagattgtgattgctagc - 3 , 5 - tttgcagctcttgcgatgc - 3 )  . 
 patient presentation ( bowel function alteration and red blood cell per rectum ) colonoscopy pathology staging ct scan 1st cycle began toxicity symptoms dose reduction 2nd cycle radiotherapy only radiotherapy completed 1st cycle began ( reduced mfolfox6 ) 46 - hour infusion 2nd cycle 4th cycle ( dose increased ) 5th cycle ( initial dose ) 8th cycle 10th cycle in silico prediction , ex vivo , and in vitro dpd assay , clonal rna sequencing dpyd sequencing ( mayo medical lab ) blood sample collection surgical resection diagnostic tests neoadjuvant cape + radio variants testing adjuvant mfolfox6 30 34 543 635 no . 
a 32 - year - old male with a history of gastroesophageal reflux and hyperlipidemia presented with altered bowel function and bright red blood per rectu colonoscopy revealed a polyp in the cecum and a mass approximately 10 cm within the rectosigmoid colon . 
a staging computed tomography scan of the chest , abdomen , and pelvis showed no evidence of distal metastases , which suggested stage iii disease . the patient was treated shortly after diagnosis with neoadjuvant therapy that consisted of capecitabine ( 825 mg m2 for 5 days each week ) and radiotherapy ( 50.4 gy in 28 fractions )  . 
 during hospitalization , absolute neutrophil count decreased to 700 cells / l ( normal reference range , 1 , 500 to 8 , 000 cells / l ) , which prompted discontinuation of therapy late in the second week of treatment . 
one and a half months after surgery , the patient was scheduled to begin modified infusional fu , leucovorin , and oxaliplatin ( mfolfox6 ) adjuvant therapy . because of the severe toxicity during the initial neoadjuvant therapy , genetic testing was ordered . 
dpd activity in the patients pbmcs was reduced by 64% ( 92.4 pmol fu min1 mg1 ) compared with previously reported reference values obtained from individuals who do not carry a deleterious dpyd variant10 ( 254.0 pmol fu min1 mg1 ; fig 2a )  . 
to determine whether allelic imbalance of dpyd was occurring , allele - specific pcr primers e13 / 14 and e13 / 15 were used to amplify canonical and alternatively spliced dpyd ( fig 2b , top )  . 
 ( a ) dihydropyrimidine dehydrogenase ( dpd ) enzyme activity was measured in peripheral blood mononuclear cells isolated from the patient and was compared with reference values previously published by our laboratory for peripheral blood mononuclear cells from individuals who do not carry known deleterious variants in dpyd ( noncarriers ) and those heterozygous for * 2a ( * 2a / wild type [ wt ] ) .10 ( b ) polymerase chain reaction primers were designed as indicated ( arrows ) to amplify across the exon 13 / 14 and 13 / 15 junctions to detect the presence of alternative splicing in the patient and a heterozygous carrier of * 2a . 
this level of reduction is similar to that observed for the well - studied p.d949v variant5 , 7 ; thus , the dpd activity score would be expected to be similar . 
finally , the decision was made to administer two additional cycles of therapy that did not contain oxaliplatin because of accumulating grade 1 neuropathy ( fig 1 , gold box )  . 
the patient has completed the 10th cycle of adjuvant therapy and has responded well to the treatment with no severe toxicity and no physical evidence of cancer progression . discussion this report outlines the effective management of toxicity in a patient with rectal cancer treated with an fu - based regimen using a precision oncology approach . 
to date , genetic testing of dpyd variants is not mandated in the united states , and complete dpd deficiency is only listed as a contraindication to fu treatment.11 many studies have increasingly performed functional characterizations of dpyd variants , 3 , 5 - 7 , 9 , 10 , 12 , 13 and the clinical pharmacogenetics implementation consortium has published activity - based fu dosing guidelines for many of the reported dpyd variants.8 however , a paucity of information exists with respect to fu dose adjustments in compound heterozygous variant carriers . in this case report , dpyd genotype and variant function data were used to provide guidance for adjuvant fu dosing in a patient who carries a complex dpyd genotype that includes a novel variant of unknown significance . 
the 38% reduction in in vitro dpd function attributed to p.t132a also is consistent with the approximately 36% activity measured in the patients pbmcs because the p.t132a variant in the patients genome is present in a compound complex heterozygous state ( trans ) with dpyd * 2a . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . shikshya shrestha no relationship to disclose colbren ( scout ) trogstad - isaacson no relationship to disclose timothy j . 
lee am , shi q , pavey e , et al : dpyd variants as predictors of 5 - fluorouracil toxicity in adjuvant colon cancer treatment ( ncctg n0147 )  . 
meulendijks d , henricks lm , sonke gs , et al : clinical relevance of dpyd variants c.1679t > g , c.1236g > a / hapb3 , and c.1601g > a as predictors of severe fluoropyrimidine - associated toxicity : a systematic review and meta - analysis of individual patient data . 
offer sm , wegner nj , fossum c , et al : phenotypic profiling of dpyd variations relevant to 5 - fluorouracil sensitivity using real - time cellular analysis and in vitro measurement of enzyme activity . 
lee am , shi q , alberts sr , et al : association between dpyd c.1129 - 5923 c > g / hapb3 and severe toxicity to 5 - fluorouracil - based chemotherapy in stage iii colon cancer patients : ncctg n0147 ( alliance )  . 
 o crizotinib and surgery for long - term disease control in children and adolescents with alk - positive inammatory myobroblastic tumors toby trahair , mbbs , phd1 , 2 , 3 ; andrew j . 
we retrospectively analyzed the outcome of patients with ap - imt treated with crizotinib to document response , toxicity , survival , and features associated with relapse . methods the cohort comprised eight patients with ap - imt treated with crizotinib and surgery . 
both harbored ranbp2 - alk fusions and responded to alternative alk inhibitors ; one ultimately died as a result of progressive disease , whereas the other remains alive on treatment . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction inammatory myobroblastic tumors ( imts ) are rare and predominantly arise in the abdomen , pelvis , and chest . 
approximately 40% to 60% of imts express anaplastic lymphoma kinase ( alk ) and have associated alk gene rearrangements.1 - 4 multiple alk fusion partners have been identied , including , but limited to , cars , 5 tpm3 , tpm4 , 2 , 6 cltc , 7 , 8 ranbp2 , 9 sec31l1 , 10 ppfib1 , 11 fn1 , 12 igfbp5 , thbs1 , 13 dctn1 , rrbp1 , tfg , 6 and eml4.14 cryptic translocations that involve ros , etv6 , and ntrk also have been identied in alk - negative imt.15 - 18 currently , a poor understanding exists of how the alk fusion partner inuences the clinical behavior of imt , in cases of epithelioid inammatory myoexcept broblastic sarcoma ( eims ) , a clinically aggressive tumor associated with a high mortality before the introduction of alk inhibitors ( alkis ) .19 , 20 eims is characterized by perinuclear or nuclear membrane alk staining6 , 19 , 21 ; cd30 expression19 , 20 , 22 , 23 ; and characteristic alk fusion partners , namely ranbp2 , 19 , 20 , 23 rrbp1 , 6 and eml4.14 surgery remains central to imt therapy . 
surgical resection with clear margins results in excellent outcomes.24 , 25 although incomplete resection is associated with recurrence , favorable outcomes have been reported with adjuvant chemotherapy.24 - 26 alkis have been shown to be safe and effective in alkrearranged tumors , including imts , 27 - 30 but no randomized data have compared alki treatment and chemotherapy . 
some authors continue to advocate surgery and adjuvant chemotherapy.25 to better dene the utility of alki treatment in alk - positive imt ( ap - imt ) , we analyzed the outcome of a cohort of eight patients with ap - imts treated with crizotinib . 
 trahair et al context key objective to document the long - term outcome of a cohort of children and teenagers diagnosed with widespread , multifocal , alk - positive inammatory myobroblastic tumors ( ap - imts ) treated in a crizotinib compassionate use access program . knowledge generated crizotinib and surgery are effective for widespread ap - imts in most patients who are able to stop treatment safely . 
disease control in the aggressive imt variant ranbp2 - alk rearranged epithelioid inammatory myobroblastic sarcoma was suboptimal , with early , on - treatment relapses . relevance many patients with ap - imt have excellent outcomes with crizotinib and surgery , which conrms that crizotinib should be considered as rst - line therapy for patients with widespread or unresectable disease . 
the poorer outcomes in patients with ranbp2 - alkrearranged epithelioid inammatory myobroblastic sarcoma suggests that specic patient subgroups , dened by pathology and alk translocation partner , could benet from intensied or combination therapy . methods participants and treatment the cohort comprised eight patients diagnosed with apimt from 2009 onward and who were treated with crizotinib . 
patients were treated at four childrens cancer including sydney childrens hospital ( n = 5 ) , centers , queensland childrens hospital ( n = 1 ) , princess margaret hospital ( n = 1 ) , and starship childrens hospital ( n = 1 )  . the cohort includes all patients diagnosed with ap - imt from 2009 onward . 
alk locus rearrangement was detected using uorescence in situ hybridization ( fish ) with a dual - color break - apart probe ( vysis ; abbott laboratories , abbott park , il )  . crizotinib was provided by pzer ( new york , ny ) using a noncommercial supply management system for alkrearranged malignancies . 
eligibility criteria for patients the pzer with ap - imt were based on version 6.0 of named - patient early - access guidance dated november 1 , 2011 , and included a diagnosis of an ap - imt , adequate organ function , stable neurologic disease , and no clinical or laboratory evidence of signicant cardiorespiratory disease.31 for ap - imt , demonstration of alk positivity by ihc alone was sufcient . 
crizotinib was used at the pediatric maximum tolerated dose ( 280 mg / m2 / dose twice a day orally ) .28 , 29 a treatment cycle was dened as 28 days , and crizotinib was continued at physician discretion while there was evidence of clinical benet . 
guidelines for safety monitoring ; lifestyle recommendations , including contraception ; management of adverse events ( aes ) ; dose modication for toxicity and ae reporting ; grading ; and attribution were as recommended in the pzer crizotinib named - patient earlyaccess reference guide.32 briey , recommended clinical monitoring for safety included monthly blood tests , including a full blood count and liver function tests , for the rst 3 months then repeated as clinically indicated . 
it was recommended that aes be identied throughout the entire course of treatment with grading , causality , and reporting to the pzer drug safety unit within 24 hours of identifying each ae . 
disease staging and treatment response were determined locally by clinical examination and laboratory assessment combined with anatomic ( computed tomography [ ct ] , magnetic resonance imaging , and / or ultrasound ) and functional ( positron emission tomography [ pet ] / ct scan ) imaging . 
single diameter measurements were used to quantify treatment response on the basis of response evaluation criteria in solid tumors ( recist ) version 1.1.33 a complete response ( cr ) was dened as disappearance of all lesions , partial response ( pr ) as a 30% or greater reduction in the diameters of all lesions with no new lesions , progressive disease ( pd ) as a 20% or greater increase in the diameters of all lesions or the appearance of new sites of disease , and stable disease as no evidence of signicant change in all lesions to qualify as pd , pr , or cr . outcomes and toxicity were analyzed retrospectively . toxicity guidelines data were graded according to the common terminology criteria for adverse events ( version 4 )  . 
the primary outcomes of interest were progressionfree survival ( pfs ) and overall survival ( os ) since the commencement of crizotinib , the incidence of severe treatment - related toxicities ( dened as grade 3 ) , and features associated with treatment failure . 
pfs and os were determined by kaplan - meier method using medcalc version 18 ( medcalc , ostend , belgium ) statistical software . the study was approved by the sydney childrens hospital network human research ethics committee ( lnr / 14 / schn / 90 )  . 
 crizotinib and surgery for alk - positive imts the declaration of helsinki , and informed consent was obtained from the patients parents or legal guardians . results clinical and pathologic features molecular analyses tumor samples from the ve patients treated at sydney childrens hospital were subjected to rna extraction for rna capture sequencing to identify alk fusion partners.34 sequencing libraries were prepared from 1 g of patient rna using the kapa stranded rna - seq library preparation kit ( roche , basel , switzerland )  . capture was performed according to manufacturers instructions using custom biotinylated probes complementary to the coding regions of genes associated with chromosomal translocations in imt . 
captured libraries were sequenced to standard depth with 125 - base pair paired - end sequencing using the hiseq 2500 kit v4 ( illumina , san diego , ca )  . 
three patients with alk nuclear membrane staining were found to have ranbp2 - alk translocations , whereas two patients with diffuse cytoplasmic alk staining were found to have sec31a - alk and cltc - alk fusions ( fig 1 ; table 1 )  . outcome after treatment with crizotinib and surgery the median time from diagnosis to commencing crizotinib was 19 days ( range , 5 to 1 , 504 days ; table 2 )  . 
histopathology of the resected alk - positive epithelioid inammatory myobroblastic sarcoma tumor from patient 2 that demonstrates ( a ) epithelioid / rhabdoid tumor cells , ( b ) prominent perinuclear / nuclear membrane alk staining on immunohistochemistry , ( c ) cd30 + tumor cells on immunohistochemistry , and ( d ) conrmation of an alk translocation by uorescence in situ hybridization using a dual - color break - apart probe ( vysis ; abbott laboratories , abbott park , il )  . 
the photograph demonstrates the alk translocation ( the split red and green signals in the lower portion of the image ) and one normal alk locus signal ( red and green signals adjacent to each other in upper portion of the image ) in a patient tumor cell . 
 ( e ) schematic representation of sec31a - , cltc - , and ranbp2 - alk fusions identied in ve patients from sydney childrens hospital by rna capture sequencing . long - term naproxen before developing progressive hepatic dysfunction . 
three patients were critically unwell and commenced crizotinib treatment in the intensive care unit ( table 2 )  . all patients had a clinical response to crizotinib ( table 2 )  . in three patients , surgery was performed at the point of maximal tumor shrinkage to achieve a cr . 
analysis of resected tumors showed extensive treatment - induced changes characterized by brous , hyalinized nodules , a patchy inammatory inltrate with foamy macrophages , and scattered foci of dystrophic calcication . 
in patient 4 , plump spindle - shaped cells weakly staining for alk - 1 in a nuclear membrane / perinuclear pattern were identied in the resected residual tumor ( fig 2 )  . 
patient 1 , who had multifocal abdominal and hepatic disease , had no evidence of tumor shrinkage on ct scan but had a complete metabolic response to crizotinib on uorodeoxyglucose pet scan and normalization of abnormal liver function tests . the eight patients , both with ranbp2 - alk two of rearranged tumors , experienced disease relapse within the rst year of crizotinib treatment despite initial crs with crizotinib ( table 2 ; fig 3 )  . 
treatment and outcome of alk - positive inammatory myobroblastic tumor cohort best response duration of crizotinib therapy patient clinical status at commencement of crizotinib crizotinib alone after surgery , years pfs , years total , years additional therapy and current treatment duration off crizotinib , years outcome after crizotinib surgery crizotinib surgery off treatment relapse crizotinib ceritinib ongoing pleural and off treatment alive ceased ceased ceased ceased ceased ceased off treatment alive off treatment alive relapse ceritinib vinorelbine , methotrexate , nsaid off treatment alive ceased ongoing current status alive alive dead alive time from diagnosis to crizotinib , days 1 , 504 ascites , pleural effusions icu admission pericardial effusions with tamponade icu admission massive ascites , abdominal compartment syndrome , liver and renal impairment icu admission abbreviations : cr , complete response ; icu , intensive care unit ; na , not applicable ; ned , no evidence of disease ; nsaid , nonsteroidal anti - inammatory drug ; pd , progressive disease ; pfs , progression - free survival ; pr , partial response ; sd , stable disease . with intermittent granulocyte colony - stimulating factor ( 5 g / kg subcutaneous injection once or twice per week ) without crizotinib dose reduction . 
crizotinib adverse effects contributed to decisions to cease treatment in two patients . patient 3 , who had preexisting mild , chronic dermatitis , experienced multiple episodes of cellulitis , and patient 4 experienced multiple fractures ( fig 3 )  . 
both patients remain well , off crizotinib , and in continuing cr . clinical outcome after recurrence on crizotinib despite initial crs , two patients with ranbp2 - alk eims experienced on - treatment disease recurrence after 4 and 10 months of crizotinib . 
at recurrence , there were bilateral pleural effusions , largevolume ascites , multiple intra - abdominal peritoneal masses , and several lesions that indented the capsular surface of the liver . 
there was a signicant tumor response within 2 weeks of the dose increase , which was sustained at most disease sites and accompanied by resolution of pleural effusions , ascites , and peritoneal nodules . 
 ( d ) alk immunohistochemistry of resected residual tumor demonstrates frequent spindle - shaped cells with weak nuclear membrane / perinuclear alk staining . achieved a partial tumor response of 2 months.39 , 40 after progression on ceritinib , the patient was commenced on low - dose chemotherapy ( vinorelbine , methotrexate , and ketorolac ) , 41 which resulted in a complete metabolic response on uorodeoxyglucose pet scan , but with progressive calcication and no objective shrinkage on ct scan and magnetic resonance imaging . 
the tumor progressed after 6 months , and the patient died 23 months after the initial diagnosis . discussion imts are rare tumors in children , teenagers , and adults commonly characterized by alk gene rearrangement15 - 18 , 42 that are targetable with alkis.19 , 27 - 30 here , we present the clinical features , treatment , and outcome of a cohort of patients with ap - imts treated with crizotinib at the pediatric maximum tolerated dose.28 , 29 there are limitations to this study , being a retrospective analysis of outcome and toxicity in a compassionate access cohort . 
eligibility was based on a standardized guideline , which included demonstration of alk positivity on ihc , adequate organ function , and the absence of alternative treatment options as judged by the clinician . 
the access program provided guidance on safety monitoring and a requirement that clinicians identify , report , grade , and attribute causality for aes within 24 hours of their identication . 
 ( a ) kaplan - meier analysis of overall survival ( os ) and progression - free survival ( pfs ) since commencement of crizotinib treatment . ( b ) swimmer plot analysis of individual patient outcomes since diagnosis , including treatment received and episodes of disease progression , surgery , cellulitis , and fractures . 
although ranbp2 - alkrearranged eims has previously been identied as an aggressive ap - imt subtype , 19 , 22 we also observed life - threatening complications associated with a cltc - alkrearranged imt . 
early consideration of an alk rearrangement in the appropriate clinical context , particularly when patients present with extensive disease , is important for rapid diagnosis and timely initiation of alki treatment . 
this study demonstrates that crizotinib is tolerable and effective in patients with life - threatening complications , with three patients treated in the intensive care setting because of malignant effusions and one patient with associated hepatic impairment . 
despite this , oral crizotinib was well tolerated and resulted in rapid clinical responses . the phase i / ii crizotinib trial conducted by the us childrens oncology group ( cog ) demonstrated high response rates ( cr , 36% ; pr , 50% ) with a favorable toxicity prole in children and teenagers with ap - imts.28 , 29 a lower objective response rate ( 50% ) was observed in an adult crizotinib trial for ap - imt.30 our response data are concordant with the cog study , with all patients experiencing a clinical response . 
factors that underlie differences in responses between pediatric and adult patients are not clear ; however , the maximum tolerated dose in children ( 280 mg / m2 ) 28 is higher than the adult dose of 250 mg ( approximately equivalent to 140 mg / m2 ) .30 at steady state , the pediatric dose ( 280 mg / m2 ) results in a 2.5 - fold higher plasma area under the curve compared with the adult dose of 250 mg , 43 which suggests that the response of apimt to crizotinib may be partly due to plasma crizotinib levels . 
of note , ve ( 62.5% ) of the eight patients ceased crizotinib without experiencing relapse or pd , which indicates that possible to cease crizotinib in ap - imt without rapid disease recurrence as has been reported in alcl.44 the toxicity prole observed was in line with the cog clinical trial.28 , 29 the most notable ongoing toxicity during crizotinib treatment was moderate to severe neutropenia , which was managed by intermittent granulocyte colony - stimulating factor . 
recurrent toxicity contributed to the decision to cease crizotinib in two patients , one because of multiple fractures ( n = 3 ) and one because of multiple episodes of cellulitis ( n = 4 )  . 
cd30 - directed therapy using brentuximab vedotin is effective in relapsed hodgkin lymphoma and alcl , 62 , 63 in patients with cd30 + a strategy that may be useful ranbp2 - alk eims . in summary , with acknowledgment of the limitations of our retrospective cohort study , the outcomes indicate that crizotinib and surgery are effective in long - term disease control for the majority of patients with ap - imt . 
walker , james blackburn , draga barbaric data analysis and interpretation : toby trahair , chelsea mayoh , andrew c . wood , santosh valvi , james blackburn , erin e . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . toby trahair stock and other ownership interests : csl andrew c . 
wood patents , royalties , other intellectual property : pat055863 - us - pct , inventor assigned to genomics institute of the novartis research foundation involving combination inhibition of alk tim r . 
mercer speakers bureau : oxford nanopore patents , royalties , other intellectual property : inventor of two patents related to synthetic rna and dna controls for next - generation sequencing karen l . 
mackenzie research funding : komipharm ( inst ) no other potential conicts of interest were reported . acknowledgment we thank our surgical colleagues for the surgical care of these patients , including susan adams , bruce currie , and guy henry from sydney childrens hospital ; japinder khosa from perth childrens hospital ; and craig mcbride from lady cilento childrens hospital , brisbane . 
we acknowledge the pathologists martin weber and ella sugo , anatomical pathology , south eastern pathology service ; mary suter , cytogenetics laboratory , sydpath , st vincents hospital ; and the technical assistance of lisa morgan , emily mould , carol wadham , and angela xie at the childrens cancer institute . references grifn ca , hawkins al , dvorak c , et al : recurrent involvement of 2p23 in inammatory myobroblastic tumors . 
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j pathol 241 : 316 - 323 , 2017 bridge ja , kanamori m , ma z , et al : fusion of the alk gene to the clathrin heavy chain gene , cltc , in inammatory myobroblastic tumor . 
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takeuchi k , soda m , togashi y , et al : pulmonary inammatory myobroblastic tumor expressing a novel fusion , ppfibp1 - alk : reappraisal of anti - alk immunohistochemistry as a tool for novel alk fusion identication . 
am j surg pathol 41 : 773 - 780 , 2017 jiang q , tong hx , hou yy , et al : identication of eml4 - alk as an alternative fusion gene in epithelioid inammatory myobroblastic sarcoma . 
antonescu cr , suurmeijer aj , zhang l , et al : molecular characterization of inammatory myobroblastic tumors with frequent alk and ros1 gene fusions and rare novel ret rearrangement . 
mario - enrquez a , wang wl , roy a , et al : epithelioid inammatory myobroblastic sarcoma : an aggressive intra - abdominal variant of inammatory myobroblastic tumor with nuclear membrane or perinuclear alk . 
yu l , liu j , lao iw , et al : epithelioid inammatory myobroblastic sarcoma : a clinicopathological , immunohistochemical and molecular cytogenetic analysis of ve additional cases and review of the literature . 
kimbara s , takeda k , fukushima h , et al : a case report of epithelioid inammatory myobroblastic sarcoma with ranbp2 - alk fusion gene treated with the alk inhibitor , crizotinib . 
zhou j , jiang g , zhang d , et al : epithelioid inammatory myobroblastic sarcoma with recurrence after extensive resection : signicant clinicopathologic characteristics of a rare aggressive soft tissue neoplasint j clin exp pathol 8 : 5803 - 5807 , 2015 23 . 
moss e yp , lim ms , voss sd , et al : safety and activity of crizotinib for paediatric patients with refractory solid tumours or anaplastic large - cell lymphoma : a childrens oncology group phase 1 consortium study . 
moss e yp , voss sd , lim ms , et al : targeting alk with crizotinib in pediatric anaplastic large cell lymphoma and inammatory myobroblastic tumor : a childrens oncology group study . 
sch offski p , suiarsky j , gelderblom h , et al : crizotinib in patients with advanced , inoperable inammatory myobroblastic tumours with and without anaplastic lymphoma kinase gene alterations ( european organisation for research and treatment of cancer 90101 create ) : a multicentre , single - drug , prospective , non - randomised phase 2 trial . 
davis mp , van dongen s , abreu - goodger c , et al : kraken : a set of tools for quality control and analysis of high - throughput sequence data . 
nicorici d , satalan m , edgren h , et al : fusioncatcher a tool for nding somatic fusion genes in paired - end rna - sequencing data , 2014 . 
geoerger b , schulte j , zwaan cm , et al : phase i study of ceritinib in pediatric patients ( pts ) with malignancies harboring a genetic alteration in alk ( alk plus ) : safety , pharmacokinetic ( pk ) , and efcacy results . 
chang w , brohl as , patidar r , et al : multidimensional clinomics for precision therapy of children and adolescent young adults with relapsed and refractory cancer : a report from the center for cancer research . 
bertocchini a , lo zupone c , callea f , et al : unresectable multifocal omental and peritoneal inammatory myobroblastic tumor in a child : revisiting the role of adjuvant therapy . 
balis fm , thompson pa , mosse yp , et al : first - dose and steady - state pharmacokinetics of orally administered crizotinib in children with solid tumors : a report on advl0912 from the childrens oncology group phase 1 / pilot consortiucancer chemother pharmacol 79 : 181 - 187 , 2017 44 . 
thorne - nuzzo t , williams c , catallini a , et al : a sensitive alk immunohistochemistry companion diagnostic test identies patients eligible for treatment with j thorac oncol 9 : 295 - 306 , 2014 crizotinib . 
maesako y , izumi k , okamori s , et al : inv ( 2 ) ( p23q13 ) / ran - binding protein 2 ( ranbp2 ) - alk fusion gene in myeloid leukemia that developed in an elderly 49 . 
touriol c , greenland c , lamant l , et al : further demonstration of the diversity of chromosomal changes involving 2p23 in alk - positive lymphoma : 2 cases expressing alk kinase fused to cltcl ( clathrin chain polypeptide - like )  . 
tokuda k , eguchi - ishimae m , yagi c , et al : cltc - alk fusion as a primary event in congenital blastic plasmacytoid dendritic cell neoplasgenes chro53 . 
chikatsu n , kojima h , suzukawa k , et al : alk + , cd30 - , cd20large b - cell lymphoma containing anaplastic lymphoma kinase ( alk ) fused to clathrin heavy chain gene ( cltc )  . 
de paepe p , baens m , van krieken h , et al : alk activation by the cltc - alk fusion is a recurrent event in large b - cell lymphoma . 
mcmanus dt , catherwood ma , carey pd , et al : alk - positive diffuse large b - cell lymphoma of the stomach associated with a clathrin - alk rearrangement . 
cerchietti l , damm - welk c , vater i , et al : inhibition of anaplastic lymphoma kinase ( alk ) activity provides a therapeutic approach for cltc - alk - positive human diffuse large b cell lymphomas . 
van roosbroeck k , cools j , dierickx d , et al : alk - positive large b - cell lymphomas with cryptic sec31a - alk and npm1 - alk fusions . 
pro b , advani r , brice p , et al : brentuximab vedotin ( sgn - 35 ) in patients with relapsed or refractory systemic anaplastic large - cell lymphoma : results of a phase ii study . 
 heterogeneity and coexistence of t790m and t790 wild - type resistant subclones drive mixed response to third - generation epidermal growth factor receptor inhibitors in lung cancer zofia piotrowska mehlika hazarrethinam coleen rizzo brandon nadres emily e . 
contributed equally to this work . ( continued ) purpose third - generation epidermal growth factor receptor ( egfr ) inhibitors like nazartinib are active against egfr mutationpositive lung cancers with t790m mediated acquired resistance to initial anti - egfr treatment , but some patients have mixed responses . methods multiple serial tumor and liquid biopsies were obtained from two patients before , during , and after treatment with nazartinib . 
next - generation sequencing and droplet digital polymerase chain reaction were performed to assess heterogeneity and clonal dynamics . results we observed the simultaneous emergence of t790m - dependent and - independent clones in both patients . 
serial plasma droplet digital polymerase chain reaction illustrated shifts in relative clonal abundance in response to various systemic therapies , confirming a molecular basis for the clinical mixed radiographic responses observed . conclusion heterogeneous responses to treatment targeting a solitary resistance mechanism can be explained by coexistent tumor subclones harboring distinct genetic signatures . 
2018 by american society of clinical oncology introduction epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitors ( tkis ) are effective therapies against advanced egfr - mutant lung cancer , but outcomes are limited by acquired resistance.1 egfr t790m accounts for 50% to 60% of resistance to erlotinib , gefitinib , and afatinib , whereas other mechanisms , including bypass pathway activation ( eg , met or errb2 amplification , mutations in braf and pik3ca ) and lineage shifts ( eg , small - cell transformation , epithelial - to - mesenchymal transition ) , are less commonly observed.2 , 3 third - generation egfr inhibitors yield responses in 40% to 60% of t790m - positive tumors , and osimertinib is us food and drug administration approved in this setting.4 other third - generation tkis , including nazartinib ( egf816 ; novartis , cambridge , ma ) , 5 are in development . 
however , tumors can harbor extensive molecular heterogeneity , potentially affecting response to subsequent therapies.6 we present two cases of egfr - mutant lung cancer treated with nazartinib after developing t790m . 
sequist , department of medicine , massachusetts general hospital , 32 fruit st , yawkey 7b , boston , ma 02114 ; e - mail : lvsequist@ partners.org. methods patients patients were treated with nazartinib in a phase i / ii trial ( clinicaltrials.gov identifier : nct02108964 ) at massachusetts general hospital ( mgh ; patient 1 : 200 mg daily , patient 2 : 150 mg daily )  . 
patients provided informed consent under an institutional review board approved protocol allowing next - generation sequencing ( ngs ) and exploratory research on their biopsies . clinical genotype assessments tissue biopsies were genotyped at mgh with three clinical laboratory improvement amendments ( clia ) - certified assays : snapshot version 4 , a multiplex polymerase chain reaction ( pcr ) allele - specific assay for somatic mutations in 23 cancer - related genes ( appendix table a1 ; snapshot ; applied biosystems7 ) ; a pcr sizing assay for in - frame egfr insertions or deletions ; and snapshot ngs , an anchored multiplex pcr assessing 39 ( v1 ) or 91 ( v2 ) genes ( appendix table a1 )  . 
foundation medicines foundationone ngs ( cambridge , ma ) assesses the entire coding sequence of 315 genes and select introns of 28 genes.8 tissue met amplification was assessed at mgh with a clia - certified dual - color fluorescence in situ hybridization ( fish ) assay using the 07q001b550 c - met probe ( chromosome 7q31 met , leica biosystems , wetzlar , germany ) and a copy number probe ( cep7 ; abbott - vysis , lake bluff , il )  . 
the remaining plasma samples were analyzed by droplet digital pcr ( ddpcr )  . plasma ctdna isolation and ddpcr ctdna was extracted from plasma using the qiaamp circulating nucleic acid kit ( qiagen , hilden , germany ) per manufacturers instructions . 
pcr reactions were performed using 10 l final volume containing 5 l lightcycler 480 sybr green i qpcr master mix , 2x ( roche , basel , switzerland ) and line - 1 ( 12.5 mol ) forward and reverse primers . 
droplets were analyzed with the qx200 droplet reader ( bio - rad ) for fluorescent measurement of fam and hex probes . quantasoft software ( bio - rad ) was used to obtain fractional abundance and copy number variations of mutant dna alleles in wild - type / normal background . 
 fractional abundance was calculated as ( nmut / [ nmut + nwt ] ) 100 , where nmut is number of mutant events and nwt is number of wt events per reaction . 
positive and negative droplet counts were used to calculate the concentration of target and reference dna sequences as previously described.10 normal control dna ( human genomic dna [ promega , madison , wi ] ) , and no dna template controls were included . 
 results patient 1 a 68 - year - old never - smoking woman presented with progressive neurologic symptoms and was found to have a lung mass with multiple brain , pulmonary , lymph node , and hepatic metastases . 
 a trans - bronchial biopsy confirmed lung adenocarcinoma and multiplexed , allele - specific pcr ( snapshot version 4 ) identified an egfr exon 19 deletion ( del19 )  . 
a symptomatic brain metastasis was resected , and erlotinib 150 mg daily was initiated with good response in all sites of disease . the cancer progressed after 9 months of erlotinib , and biopsy of a growing liver metastasis ( fig 1b ; day 35 ) was analyzed via targeted ngs ( snapshot ngs - v1 ) , revealing both the original egfr del19 and acquired egfr t790m . 
 hence , she began a clinical trial of nazartinib ( clinicaltrials.gov identifier : nct02108964 ; fig 1a , days 1 to 392 ) and achieved a partial response.11 after 11 months on nazartinib , she developed a solitary progressing liver metastasis in a location distinct from her prior lesion ( fig 1b , day 332 )  . 
in addition , a braf v600e mutation , not present on the preor post erlotinib biopsy samples , was detected as the likely nazartinib - resistant mechanism within this lesion . 
shortly after the ablation , further progression was noted within the thorax ( day 388 )  . ctdna analysis provides a noninvasive means of monitoring the genomic evolution of cancer during treatment . 
in this patient , multiple plasma samples were taken for ctdna analyses , including ngs ( guardant360 ; guardant health , redwood city , ca ) and ddpcr ( fig 1d )  . 
on nazartinib initiation , ddpcr revealed a sharp decline in both egfr del19 ( fig 1d , days 0 to 100 , gray line ) , and t790m ( red line ) , suggesting effective inhibition of the dominant egfr del19 / t790m subclone . 
by day 100 , the mutant allele fraction ( maf ) of del19 began to increase again , this time without rebound of t790m , suggesting outgrowth of a distinct t790wt subclone . 
the increase in egfr del19 was coincident with emergence of a previously undetected braf v600e mutation ( ddpcr ; blue line ) , consistent with the egfr del19 / t790wt / braf v600e subclone detected in the contemporaneous biopsy of the progressing liver metastasis . 
interestingly , ablation of the liver metastasis ( fig 1c , day 351 ) caused braf v600e levels to drop below detection in ctdna , corresponding with radiographic regression , and suggesting this subclone was likely unique to the ablated metastasis . meanwhile , egfr t790m ( fig 1d , red line ) reappeared around day 200 , accompanying a continued increase in total del19 , emergence of egfr c797s ( ddpcr ; gold line ) , and clinical progression of disease in the thorax . 
c797s drives resistance to third - generation egfr tkis by disrupting the key cysteine residue at the drug - binding site.12 - 15 although tissue biopsy was not obtained , we hypothesize based on increasing plasma levels of t790m and c797s that an egfr del19 / t790m / c797s clone may have been driving disease progression in the thorax . 
consistent with this , guardant360 ngs ctdna analysis on day 402 revealed egfr del19 ( maf 4.5% ) , t790m ( 1.1% ) , and c797s ( 0.6% ) in cis configuration without detectable braf v600e ( fig 1c , day 402 ; appendix figs a1a and a1b )  . although several novel treatment strategies for egfr c797s are being studied , 16 , 17 there are currently no targeted therapies against t790m / c797s available in the clinic . 
thus , the patient discontinued nazartinib and started carboplatin / pemetrexed chemotherapy ( fig 1a , days 400 to 547 ) with an initial brief response , followed by disease progression in the liver and thorax 5 months later ( fig 1b , day 547 )  . 
a repeat plasma sample ( guardant360 ngs ) demonstrated increasing maf of egfr del19 ( 44.8% ) and t790m ( 12.3% ) , whereas egfr c797s ( 0.5% ) remained stable ( fig 1c , day 555 ; appendix fig a1c )  . 
the pattern of ddpcr detected ctdna clones during carboplatin / pemetrexed chemotherapy ( fig 1d , days 400 to 547 ) suggests there are ( at least ) two subclones present . 
plasma g360 ngs day 555 ( maf ) egfr del19 egfr del19 egfr del19 ( 4.5% ) egfr del19 ( 44.8% ) egfr t790m egfr t790m ( 1.1% ) egfr t790m ( 12.3% ) egfr c797s ( 0.6% ) egfr c797s ( 0.5% ) braf v600e tp53 r333 * tp53 r333 * ddr2 r806 * ddr2 r806 * apc h1172h ( 0.4% ) , hnf1a t196t ( 0.2% ) rit1 e94k ( 0.4% ) , raf1 d457h ( 0.2% ) , tp53 c238y ( 0.2% ) , pik3ca i211v ( 0.1% ) nazartinib carboplatin + pemetrexed osi + doce * ablation of t790 wt , braf v600e liver lesion egfr del19 braf v600e egfr t790m egfr c797s time ( days ) fig 1 . 
 ( c ) results of clinical genotyping on days 35 , 351 ( tissue biopsies tested by snapshot next - generation sequencing [ ngs ] panel ) , and days 402 and 555 ( liquid biopsies , guardant360 )  . 
on day 548 , treatment was switched to docetaxel plus osimertinib ( fig 1a ) , which yielded a response in the thorax but progression in other sites , including the liver . 
interestingly , the high t790m levels quantified through ddpcr before reintroduction of a t790m specific inhib itor ( this time , osimertinib ) may provide a molecular predictor of the retreatment effect sometimes observed clinically , as in this patient.19 in summary , this case highlights the complexity and heterogeneity of resistance in egfr - mutant lung cancer and provides insight into clonal evolution via complementary longitudinal ctdna and tumor analyses . 
here , nazartinib resistance was attributed to two genetically distinct subclones , one braf v600e / egfr t790wt , the second egfr t790m / c797s , each of which followed a distinct trajectory in response to systemic and local therapies . patient 2 a 48 - year - old never - smoking woman presented with flank pain and was found to have a lung mass with metastases to mediastinal lymph nodes , ovary , liver , adrenal gland , and bones , and several small brain metastases . 
ngs ( foundationone ) showed egfr del19 , tp53 r273c , and the emergence of t790m ( fig 2c , day 29 , core 1 ) , prompting treatment with nazartinib . 
 interestingly , parallel ngs ( snapshot ngs - v1 ) of a second core from the same liver biopsy demonstrated egfr del19 without t790m , but met amplification was detected by fish ( abnormal signal clusters , unquantifiable ; fig 2c , day 29 , core 2 )  . after 2 months receiving nazartinib ( fig 2a , days 1 to 57 ) , a mixed response was observed , with progression of multiple liver metastases but reduction in mediastinal lymph nodes and lung mass ( fig 2b , day 54 )  . 
biopsy of the progressive hepatic metastasis on day 60 ( fig 2c ) analyzed by ngs ( snapshot ngs - v1 ) revealed egfr del19 without t790m , tp53 r273c , and high - level met amplification by fish ( abnormal signal clusters , unquantifiable )  . 
 on the basis of met amplification observed within the liver and ctdna , nazartinib was discontinued and combination therapy initiated ( fig 2a , days 70 to 100 ) with erlotinib ( 100 mg daily ) and crizotinib ( 250 mg daily ) , a regimen effective in another patient with egfr - mutant , met - amplified cancer.20 scans 1 month later showed reduction in the met - amplified liver metastasis that previously underwent biopsy but marked disease progression elsewhere ( fig 2b , day 100 )  . 
as expected , egfr del19 and t790m declined on nazartinib initiation ( fig 2d , days 1 to 25 , gray and red lines ) , but we observed a coincident increase in normalized met copy number ( ddpcr ; fig 2d , blue line )  . 
taken together with the biopsy and radiographic findings , the increasing met signal likely corresponds to a clone residing within the hepatic metastases , whereas the decline in t790m may arise from a nazartinib - sensitive clone within the thorax . 
humerus biopsy day 68 egfr del19 egfr del19 egfr del19 ( 2.4% ) egfr del19 egfr del19 egfr del19 egfr t790m egfr t790m ( 1.1% ) tp53 r273c tp53 r273c tp53 r273c ( 2.3% ) tp53 r273c tp53 r273c met amp met amp met amp tert p702p ( 1.4% ) , ccnd1 e122k ( 0.4% ) nazartinib erlotinib / crizotinib 1000 egfr del19 egfr t790m met copy # time ( days ) fig 2 . 
 ( c ) results of tissue genotyping with snapshot next - generation sequencing ( ngs ) panel on days 29 , 60 , 61 , and 68 and guardant360 plasma test ( mutant allele frequencies [ mafs ] in parentheses ) on day 57 . 
 discussion these two egfr - mutant lung cancer cases with serial tissue and plasma biopsies present a unique opportunity to study clonal evolution in depth during diverse molecularly targeted therapies . 
 our findings illustrate the critical role heterogeneity plays in resistance to targeted therapies and the clinical challenge posed by genetically distinct subpopulations that respond differentially to treatment . heterogeneity in the context of egfr resistance has been documented in both autopsy and ctdna - based studies.14 , 21 , 22 we previously described an afatinib - resistant pleural effusion , which was t790m positive on clinical testing , but single - cell cloning revealed both t790m mutant and t790wt subclones . 
in a cohort of such patients , either subpopulation could spawn the dominant driver of subsequent resistance to third - generation egfr tkis.6 recently , blakely et al23 demonstrated increasing heterogeneity of an egfr - mutant cancer across multiple lines of therapy through whole - exome sequencing of serial biopsies and autopsy specimens . 
the two cases reported here build on these observations and reveal that one can clinically document coexistent , genetically distinct subpopulations differentially responding as predicted by their genotype in real time to therapies . 
 indeed , chabon et al14 also demonstrated that coexistence of t790m and met amplification within ctdna predicted poorer outcomes than t790m alone on a third - generation tki.14 in contrast , patient 1 had only t790m detected on erlotinib progression and enjoyed a durable response to nazartinib . 
her ultimate nazartinib resistance was driven initially by a t790wt / braf - mutant clone localized to a solitary liver metastasis that was transiently eradicated from ctdna by directed ablation and , subsequently , by a t790m / c797s subclone . 
 although egfr c797s has previously been described in osimertinib , olmutinib , and rociletinib resistance , 12 - 15 to our knowledge this is the first report of c797s emergent after nazartinib . 
 broader efforts may be required moving forward to more fully characterize resistance . locally ablative therapies ( lat ) to treat sites of oligoprogression are often used to prolong disease control among patients with egfrand alk - positive disease.26 in patient 1 , microwave ablation of an oligoprogressive egfr del19 / braf v600e - mutant liver metastasis caused the corresponding ctdna signal to fall below detectable levels , suggesting local therapy can effectively eradicate a focally restricted resistant clone and lending biologic rationale to the use of lat . 
in this patient , ablation did not provide sufficient overall disease control , likely because of the egfr del19 / t790m / c797s subclone already detectable in plasma at the time of ablation , which emerged clinically shortly thereafter . 
sometimes , as in patient 1 , plasma identifies resistance mechanisms not detected in tissue ( here , egfr c797s ) , although its utility is limited in patients with low levels of ctdna . 
here , we used a broad ngs - based ctdna panel at key points of disease progression and ddpcr , which is generally more sensitive and cost - effective than serial ngs , to retrospectively quantify known genetic variants in plasma samples banked during treatment . 
although this strategy was well suited to our longitudinal analysis , in practice providers must select the most appropriate test on the basis of gene coverage , turnaround time , and cost . ultimately , our cases illustrate the critical role of cancer heterogeneity in targeted therapy acquired resistance and provide a glimpse of a future where real - time information gleaned from tracking resistant clones during treatment could be clinically meaningful . 
currently , t790m status is used to determine whether a patient should be treated with second - line osimertinib , 1 but our data suggest that looking beyond t790m might have relevance ; incorporating broader tissue and plasma panels into routine testing may identify other clones influencing the success of subsequent therapies . 
future clinical trials should incorporate longitudinal ctdnaand tissue - based assessments during therapy to develop a more complete understanding of dynamic evolution under the pressure of treatment and which clones survive and drive resistance . 
iafrate stock and other ownership interests : archer biosciences consulting or advisory role : debiopharm group , chugai pharmaceutical , roche research funding : blueprint medicines patents , royalties , other intellectual property : archerdx exclusive license to anchored multiplexpcr technology dora dias - santagata no relationship to disclose ignaty leshchiner no relationship to disclose nicholas a . 
engelman employment : novartis stock and other ownership interests : loxo oncology , agios pharmaceuticals , kura oncology , gatekeeper pharmaceuticals , novartis consulting or advisory role : novartis , agios pharmaceuticals , loxo oncology , clovis oncology , ventana medical systems , g1 therapeutics , sanofi , chugai pharmaceutical , warp drive bio , asana biosciences , emd serono , synta , allostery , genentech , aveo / biodesix , merck , cell signaling technology , endo pharmaceuticals , astrazeneca , glaxosmithkline , amgen , bristol - myers squibb , cancer progress research funding : novartis , jounce therapeutics , sanofi , araxes pharma , astrazeneca , amgen ( inst ) patents , royalties , other intellectual property : i am a co - inventor on a patent application that has been licensed to ventana / roche other relationship : third rock ventures aaron n . 
corcoran consulting or advisory role : avidity nanomedicines , taiho pharmaceutical , merrimack , genentech , n - of - one , astex pharmaceuticals , amgen , bristol - myers squibb , roche , shire , fog pharma , loxo oncology , roivant sciences , warp drive bio research funding : astrazeneca , sanofi stock and other ownership interests : guardant health lecia v . 
lanman employment : guardant health , veracyte leadership : guardant health , biolase stock and other ownership interests : guardant health , biolase research funding : guardant health consulting or advisory role : astrazeneca , genentech , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , merck ( inst ) , pfizer ( inst ) , guardant health ( inst ) , incyte ( inst ) susan moody employment : novartis institutes for biomedical research stock and other ownership interests : novartis consulting or advisory role : dominion diagnostics ( i ) travel , accommodations , expenses : dominion diagnostics ( i ) other relationship : acadia healthcare ( i ) affiliations zofia piotrowska , mehlika hazar - rethinam , coleen rizzo , brandon nadres , emily e . 
 coyne memorial fund ( l.v.s. ) , uniting against lung cancer ( z.p. ) , the lungevity foundation ( z.p. ) , a damon runyon clinical investigator award ( r.b.c. ) , and national institutes of health / national cancer institute grants no . 
yu ha , arcila me , rekhtman n , et al : analysis of tumor specimens at the time of acquired resistance to egfr - tki therapy in 155 patients with egfr - mutant lung cancers . 
tan ds - w , yang jc - h , leighl nb , et al : updated results of a phase 1 study of egf816 , a thirdgeneration , mutant - selective egfr tyrosine kinase inhibitor ( tki ) , in advanced non - small cell lung cancer ( nsclc ) harboring t790m . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a thirdgeneration egfr inhibitor . 
dias - santagata d , akhavanfard s , david ss , et al : rapid targeted mutational analysis of human tumours : a clinical platform to guide personalized cancer medicine . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
yu ha , tian sk , drilon ae , et al : acquired resistance of egfr - mutant lung cancer to a t790m - specific egfr inhibitor : emergence of a third mutation ( c797s ) in the egfr tyrosine kinase domajama oncol 1 : 982 - 984 , 2015 13 . 
thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . 
song hn , jung ks , yoo kh , et al : acquired c797s mutation upon treatment with a t790mspecific third - generation egfr inhibitor ( hm61713 ) in non - small cell lung cancer . 
uchibori k , inase n , araki m , et al : brigatinib combined with anti - egfr antibody overcomes osimertinib resistance in egfr - mutated non - small - cell lung cancer . 
chang gc , tseng ch , hsu kh , et al : predictive factors for egfr - tyrosine kinase inhibitor retreatment in patients with egfr - mutated non - small - cell lung cancera multicenter retrospective sequence study . 
gainor jf , niederst mj , lennerz jk , et al : dramatic response to combination erlotinib and crizotinib in a patient with advanced , egfr - mutant lung cancer harboring de novo met amplification . 
suda k , murakami i , katayama t , et al : reciprocal and complementary role of met amplification and egfr t790m mutation in acquired resistance to kinase inhibitors in lung cancer . 
blakely cm , watkins tbk , wu w , et al : evolution and clinical impact of co - occurring genetic alterations in advanced - stage egfr - mutant lung cancers . 
ohashi k , sequist lv , arcila me , et al : lung cancers with acquired resistance to egfr inhibitors occasionally harbor braf gene mutations but lack mutations in kras , nras , or mek1 . 
weickhardt aj , scheier b , burke jm , et al : local ablative therapy of oligoprogressive disease prolongs disease control by tyrosine kinase inhibitors in oncogene - addicted non - small - cell lung cancer . 
 ( a ) results of next - generation sequencing of circulating tumor dna ( ctdna ) by guardant360 for patient 1 , day 402 ( progression on nazartinib )  . 
 ( c ) results of subsequent ctdna analysis on day 555 ( progression on carboplatin / pemetrexed ) with an overall increase in the mutant allele fraction of egfr del19 and t790 , whereas egfr c797s declined slightly . 
we sought to examine a large genomic data set to comprehensively characterize non - v600 braf alterations in lung cancer . patients and methods a total of 23 , 396 patients with lung cancer provided data to assay with comprehensive genomic profiling . 
data were reviewed for predicted pathogenic braf base substitutions , short insertions and deletions , copy number changes , and rearrangements . results adenocarcinomas represented 65% of the occurrences ; nsclc not otherwise specified ( nos ) , 15% ; squamous cell carcinoma , 12% ; and small - cell lung carcinoma , 5% . 
braf was altered in 4.5% ( 1 , 048 of 23 , 396 ) of all tumors ; 37.4% ( n = 397 ) were braf v600e , 38% were braf non - v600e activating mutations , and 18% were braf inactivating . 
2018 by american society of clinical oncology introduction the rapid development of genotype - directed management of metastatic nonsmall - cell lung carcinoma ( nsclc ) has emerged as the paradigm for precision oncology . 
ali , md , phd , 150 second st , foundation medicine , cambridge , ma 02139 ; e - mail : siraj@ foundationmedicine.com. within lung cancers , small series have described other oncogenic braf point mutations in exons 11 and 15.9 - 12 however , because of the small sample size of prior studies and the focused sequencing methodologies that can miss important classes of genomic alterations , such as rearrangements , a complete landscape of braf alterations in lung cancers is lacking.13 - 15 given the therapeutic action ability of diverse braf alterations , we hypothesized that analysis by comprehensive genomic profiling ( cgp ) would refine the braf landscape and identify additional subsets of patients who may be candidates for targeted therapy . 
the hybrid capture next - generation sequencingbased assay used identifies genomic alterations in 186 , 236 , or 315 genes : base substitutions , insertions / deletions , copy number alterations , and gene fusions via intron baiting for 14 , 19 , and 31 genes , as previously described.16 dna was extracted from 40 - micron scrolls of formalin - fixed paraffin - embedded tissue , and cgp was performed on hybridization captured , adaptor ligationbased libraries to a mean coverage depth of greater than 500 . 
before sequencing , all patient cases were reviewed by a board - certified pathologist to establish adequacy of submitted material but not to confirm or overturn the submitted histologic diagnosis . 
testing was performed in a clinical laboratory improvement amendmentscertified , college of american pathologistsaccredited reference laboratory ( foundation medicine , cambridge , ma )  . ordinal relationships were examined with the mann - whitney u test ; categoric relationships were examined with the pearson 2 test , and the yates continuity correction was applied when applicable . 
literature review defined kinase - activating base substitutions in braf as follows : g464a , g464e , g464v , g466a , f468c , g469a , g469r , g469s , g469v , v471f , n581s , e586k , f595l , l597q , l597r , l597s , l597v , and k601e . 
base substitutions that inactivate braf kinase activity were defined as follows : g466e , g466r , g466v , g469e , d594a , d594e , d594g , d594h , d594n , d594v , d594y , g596r , t599i . results the histologic breakdown and basic clinicopathologic features are listed in table 1 . 
 there were differences among histologic subtypes : 5.5% of adenocarcinomas and 1% ( 42 of 3 , 948 ) of squamous and small - cell tumors harbored braf alterations ( table 2 )  . 
of the 10 sclcs with braf alterations , nine were kinase activating , one was v600e , and two were g469v ( fig 1a )  . overall , non - v600e activating mutations accounted for 37.9% ( 402 of 1 , 061 ) of all braf alterations . 
within non - v600e mutations ( n = 402 ) , codon 469 ( g469 ) alterations represented 34% ( 135 of 402 ) , and g469a was the most common alteration ( 23% ; 94 of 402 ; table 2 )  . 
 frequency of point mutation within braf protein ( n = 1 , 048 ) ras - binding domain protein kinase domain v600 , 400 g469 , 171 g466 , 105 g464 , 38 k483 , 7 n581 , 67 d594 , 77 k601 , 63 g596 , 31 l597 , 16 amino acid residue tmb level ( mutations / mb ) low ( < 6 ) intermediate ( 6 and < 20 ) high ( 20 ) braf setd2 tp53 stk11 kras pik3ca keap1 smad4 rictor variant type point mutation / indel deletion fusion / rearrangement amp and fusion / rearrangement braf v600e amplification truncation amp and point mutation / indel other multiple number of samples : 1 , 047 fig 1 . 
intragenic distribution of braf point mutations and co - occurrence of braf alterations with alterations of other cancer - related genes within braf in a series of 23 , 396 patient cases with lung cancer . 
braf f595l and g596d were found once each and may have affected kinase activity.17 additional kinase - inactivating mutations included changes at position g466 in the p - loop in 54% ( 104 of 193 ) , as follows : g466v ( 35.2% ; 68 of 193 ) , g466e ( 5.7% ; 11 of 193 ) , and g466r ( 3.1% ; six of 193 )  . 
nearly half ( 44% ) of setd2 alterations in the braf v600e occurrences were loss of heterozygosity ( loh ) , which was more frequent than the occurrence of loh ( 22% ) across a large set of setd2 altered nsclc tumors ( data not shown )  . 
this assessment included any known / likely kras variant . small activating insertions and deletions of braf were rare ( 2% ; 23 of 1 , 061 tumors ) and were predominantly in adenocarcinoma ( 91% ; 21 of 23 tumors )  . 
such deletions were l485_ n486 > f , l485_n486 > y ( n = 2 ) , n486_p490del ( n = 3 ) , v487_p492 > a ( n = 2 ) , t488_p492del , and a489_q493del ( n = 3 ) , which are all adjacent or within the alpha c - helix , as previously described.14 , 15 other oncogenic braf deletions were g593_a598del , t599_v600 > m , v600_w604 > r , and v600_w604 > e ( n = 1 each )  . 
 oncogenic braf deletions and insertions were largely mutually exclusive from other national comprehensive cancer networkdesignated nsclc oncogenic alterations except for one tumor that harbored both t599_v600inst and erbb2 amplification , quantitatively estimated as seven copies ( table 2 )  . rearrangements that consisted of n - terminal deletions ( ntds ) , exonic deletions , kinase domain duplications ( kdds ) , and fusions of braf were identified at a frequency of 4.3% ( 46 of 1 , 061 braf alterations ; fig 2 )  . 
kdd events occurred in 0.76% ( eight of 1 , 048 tumors ) and appended exons that coded for the full kinase domain of braf to the 3 - prime end of the wildtype gene . 
one tumor had a breakpoint in intron 7 , appended to exons 7 through 18 ; two tumors had a breakpoint in intron 8 ; four tumors had breakpoints in intron 9 ; and one tumor had a breakpoint in intron 10 ( fig 2 )  . 
predicted fusions of braf were found in 2.9% ( 30 of 1 , 048 ) of tumors , which provided an overall frequency of 2.8% ( 30 of 1 , 061 ) of all braf alterations . 
 twenty - six tumors had identifiable fusion partners of braf , and the following recurrent fusions occurred twice each : armc10 , dock4 , and trim24 ; three tumors harbored snd1braf . 
fusions that involved agap3 , agk , ap3b1 , btfl34 , eps15 , eys , ghr , grm8 , lmo7 , mkrn1 , nup214 , parp12 , ptpn13 , stat3 , trim4 , trio , and zc3hav4 occurred once each ( fig 2 )  . paired samples were available for a small subset of tumors ( n = 16 )  . 
among seven braf v600e adenocarcinomas , five had new mutations in ras family members , including four mutations in kras , and one in nras ( table 3 )  . 
patients with chronologically separated specimens were assayed by comprehensive genomic profiling , and genomic alterations present in the latter specimen are highlighted in this table . abbreviation : tmb , tumor mutational burden . * original braf alteration for each was braf v600e . discussion here , we present , to our knowledge , the largest assessment of braf alterations and expand upon the understanding of activating genomic braf aberrations across lung cancers . 
pathologic activation of the ras / raf / mek / erk ( mapk ) pathway is observed across multiple tumor types , and braf alterations in lung cancer can be targeted by mek inhibitors or pan - raf inhibitors . 
preclinical data suggest that mapk pathway activation that results from braf activating ( including non - v600e ) alterations may be sensitive to targeting downstream signaling nodes mek and erk.18 our data suggest that non - v600e braf alterations are recurrent in nsclc and warrant additional clinical exploration . raf proteins ( including braf ) have similar structures , which contain three conserved regions ( cr1 , cr2 , and cr3 ) .19 cr1 contains ras - binding and cysteine - rich domains ( called rbd and crd , respectively ) , that bind ras . 
 cr2 is a serine - threoninerich domain , which functions as an inhibitory domain upon binding of the 14 - 3 - 3 regulatory prote cr3 encompasses the kinase domain , which includes sites for binding of atp ( the p - loop ) and braf substrates mek1 and mek2 . 
in this large patient subset , use of the multikinase inhibi tors sorafenib , and the closely structurally related compound regorafenib , which have activity against c - raf , an obligate physiologic heterodimerization partner for braf , may be a more rational approach . 
indeed , sorafenib activity in in two nsclc tumors with activating mutations , g469a and g469v , was demonstrated recently.17 , 20 orthogonal support from translational studies demonstrated decreased signaling activity , with a dimerization - impaired form of braf g469a ( r509h ) compared with wildtype braf g469a , in contrast with only a slight ( 7% ) reduction for the analogous dimerization impaired form of braf v600e ( r509h ) , which is consistent with the operation of the r509h form as a promoter.21 we hypothesize that response to single - agent braf inhibitors in g469 alterations would be limited by paradoxical activation of raf / mek / erk signaling caused by the current approved braf inhibitors ( vemurafenib , dabrafenib ) , and we expect that newer pan - raf inhibitors , such as plx8394 , may have broader utility against both v600 and non - v600 mutant forms of braf in nsclc.22 across cancers , the mutagenic processes most frequently observed in each anatomic tumor type exhibit some well - described variation.23 in this series , we identified recurrent braf mutations at g464 , g466 , and particularly g469 , which typically are not observed in melanoma.24 this observation hints at different underlying carcinogenic processes between melanoma ( ultraviolet lightinduced dna damage ) and lung cancer ( often smoking - induced damage )  . 
in preclinical studies of deletion in the alpha c - helix of braf , single to multiple amino acids deletions have been modeled with some gain in braf kinase activity less than that of the 486 through 490 deletion , but this insertion of f / y was not modeled . 
this change may mimic the poorly characterized l747p mutation in egfr or the conserved exon 19 insertion , which also results in l747p mutation.26 , 27 it remains to be understood how l485_n486 > f / y activates braf and any associated sensitivity to a pan - raf inhibitor . 
larger series with treatment data will be needed to address a possible role for how tissue and / or the genomic context of a given braf alteration would affect clinical responsiveness . 
for example , in this data set , 0.7% of lung carcinoma tumors harbored focal braf amplification , which by itself is not known to serve as an oncogenic driver , but more than half of these co - occurred with braf non - v600e point mutations without other oncogenic driver alterations ( data not shown )  . 
stk11 alterations in particular may be functionally related to braf alterations , as was shown in melanoma cells in which braf v600e suppressed lkb1 function , which allowed activation of ampk.28 , 29 such interaction has not been described for non - v600e braf mutants , but it is conceivable that stk11 mutations on one allele , coupled with inactivation of residual wild - type stk11 protein by a mutated braf protein , may abrogate stk11 function . we observed a diversity of braf rearrangements , including ntds , kdds , and braf fusions , in this series . 
previously , variably sized deletions of exons 2 through 9 or less in braf ( ntd - braf ) were described only in preclinical models of vemurafenib - resistant melanoma and lung cancer.30 , 31 to our knowledge , this is the first report of ntd - braf in lung cancer samples ( none , to our knowledge , with prior raf - directed therapy ) , and it suggests that mechanisms other than splicing at the rna level can underlie ntd . 
across the series , braf fusions lack the ras - binding auto inhibitory domain found in the n - terminal half of braf , akin to braf ntds , and the n - terminal fusion partner often harbors a con stitutive dimerization or oligomerization motif . 
 not needed for braf fusion activity , although is required.40 , 41 kinase some dimerization fusions may emerge as resistance mechanisms to targeted therapy , such as epidermal growth factor receptor inhibitors.42 , 43 limited clinical histories were available for patient cases in the series , but , for one tumor with egfr exon 19 deletion ( t790m negative ) , a trim24 - braf fusion was observed with erlotinib resistance , which suggests that the braf fusion may drive resistance . 
 resistance to small molecule inhibitors is universal , and the landscape of braf - mutant lung cancers treated with braf inhibition is not known.44 among a small subset of tumors with paired samples and clinical data , genomic alterations not present in the pretreatment specimen existed in the post - treatment specimens and may correlate with acquired resistance ( table 3 )  . 
we observed a braf fusion upon resistance to vemurafenib , which mimicked a recent description of a fusion - based resistance to vemurafenib in melanoma.45 in a second tumor , loss of map2k4 and biallelic inactivation of smarca4 was seen at progression . 
several tumors also had activating kras / nras mutations upon progression . overall , we report the largest series , to our knowledge , to examine all classes of braf alterations in lung cancers . 
although limited by disease heterogeneity , incomplete clinical annotation , and no independent confirmation of histology , the series identifies multiple non - v600 aberrations that tend to be mutually exclusive with other oncogenic drivers in lung cancer . 
 whether non - v600 identifies a good prognostic group , as in colorectal cancer , is of interest but is not answerable from our data.46 likewise , it is unclear whether non - v600e alterations are responsive to existing therapies ; clinical trials are needed . 
trabucco employment : foundation medicine research funding : foundation medicine travel , accommodations , expenses : foundation medicine jon chung employment : foundation medicine stock and other ownership interests : foundation medicine mark rosenzweig employment : foundation medicine stock and other ownership interests : foundation medicine kai wang no relationship to disclose vamsidhar velcheti honoraria : novartis , foundation medicine , merck , bristolmyers squibb , genentech , roche consulting or advisory role : clovis oncology , genentech , bristol - myers squibb , merck , celgene , foundation medicine , astrazeneca , medimmune , genoptix , amgen , takeda research funding : genentech ( inst ) , trovagene ( inst ) , eisai ( inst ) , oncoplex diagnostics ( inst ) , alkermes ( inst ) , nantomics ( inst ) , genoptix ( inst ) , altor bioscience ( inst ) , merck ( inst ) , bristol - myers squibb ( inst ) , atreca ( inst ) , heat biologics ( inst ) , leap therapeutics ( inst ) travel , accommodations , expenses : astrazeneca / medimmune , eisai , foundation medicine , merck garrett m . 
frampton employment : foundation medicine stock and other ownership interests : foundation medicine nir peled consulting or advisory role : astrazeneca , boehringer ingelheim , bristol - myers squibb , lilly , msd , novartis , pfizer , roche speakers ' bureau : astrazeneca , boehringer ingelheim , bristol - myers squibb , lilly , msd , novartis , pfizer , roche molly murray employment : foundation medicine young kwang chae consulting or advisory role : foundation medicine , boehringer ingelheim , biodesix , counsyl , astrazeneca , guardant health speakers ' bureau : merck , genentech , roche travel , accommodations , expenses : hanmi lee a . 
albacker employment : foundation medicine stock and other ownership interests : foundation medicine hatim husain consulting or advisory role : astrazeneca , abbvie , foundation medicine speakers ' bureau : astrazeneca , merck , bristol - myers squibb research funding : pfizer ( inst ) travel , accommodations , expenses : astrazeneca , merck , bristol - myers squibb , foundation medicine , abbvie james suh employment : foundation medicine stock and other ownership interests : foundation medicine sherri millis employment : foundation medicine venkataprasanth reddy employment : foundation medicine stock and other ownership interests : foundation medicine travel , accommodations , expenses : foundation medicine julia elvin employment : foundation medicine stock and other ownership interests : foundation medicine ryan j . 
 consulting or advisory role : revolution medicine , array biopharma , novartis , astrazeneca stock and other ownership interests : foundation medicine speakers ' bureau : novartis research funding : ignyta , revolution medicine vincent miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis patents , royalties , other intellectual property : i hold two patents for digital imaging that may be licensed to ibris and inspirata travel , accommodations , expenses : inspirata alexa schrock employment : foundation medicine sai - hong ou honoraria : pfizer , roche pharma ag , genentech , roche , ariad , takeda , novartis , astrazeneca , foundation medicine consulting or advisory role : pfizer , roche , genentech , novartis , astrazeneca , takeda , ariad , foundation medicine speakers ' bureau : genentech , astrazeneca , takeda , ariad research funding : pfizer ( inst ) , roche pharma ag ( inst ) , astrazeneca ( inst ) , medimmune ( inst ) , clovis oncology ( inst ) , ariad ( inst ) , ignyta ( inst ) , peregrine pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , astellas pharma ( inst ) , chugai pharma ( inst ) siraj ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiomes in non - neoplastic disease ( i ) affiliations yuri sheikine , vancouver general hospital , vancouver , british columbia , canada ; dean pavlick , sally e . 
 klempner , the angeles clinic and research institute and cedars - sinai medical center , los angeles ; hatim husain , university of california san diego , san diego ; trever g . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as first - line treatment for european patients with advanced egfr mutationpositive nonsmall - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) - mutant metastatic nonsmall - cell lung cancer : an open - label , multicentre phase 2 trial . 
planchard d , kim tm , mazieres j , et al : dabrafenib in patients with braf ( v600e ) - positive advanced non - small - cell lung cancer : a single - arm , multicentre , open - label , phase 2 trial . 
villaruz lc , socinski ma , abberbock s , et al : clinicopathologic features and outcomes of patients with lung adenocarcinomas harboring braf mutations in the lung cancer mutation consortiucancer 121 : 448 - 456 , 2015 13 . 
chen sh , zhang y , van horn rd , et al : oncogenic braf deletions that function as homodimers and are sensitive to inhibition by raf dimer inhibitor ly3009120 . 
kordes m , rring m , heining c , et al : cooperation of braf ( f595l ) and mutant hras in histiocytic sarcoma provides new insights into oncogenic braf signaling . 
rring m , herr r , fiala gj , et al : distinct requirement for an intact dimer interface in wildtype , v600e , and kinase - dead b - raf signaling . 
okimoto ra , lin l , olivas v , et al : preclinical efficacy of a raf inhibitor that evades paradoxical mapk pathway activation in protein kinase braf - mutant lung cancer . 
lee lh , gasilina a , roychoudhury j , et al : real - time genomic profiling of histiocytoses identifies early - kinase domain braf alterations while improving treatment outcomes . 
allen jm , schrock ab , erlich rl , et al : genomic profiling of circulating tumor dna in relapsed egfr - mutated lung adenocarcinoma reveals an acquired fgfr3 - tacc3 fusion . 
klempner sj , bazhenova la , braiteh fs , et al : emergence of ret rearrangement co - existing with activated egfr mutation in egfr - mutated nsclc patients who had progressed on first or second - generation egfr tki . 
kulkarni a , al - hraishawi h , simhadri s , et al : braf fusion as a novel mechanism of acquired resistance to vemurafenib in braf v600e mutant melanoma . 
carl barrett , phd1 ; and jeeyun lee , md3 purpose some gastric cancers harbor met gene amplications that can be targeted by selective met inhibitors to achieve tumor responses , but resistance eventually develops . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction gastric cancer is the fth most common cancer worldwide and the third leading cause of cancerrelated death.1 gastric cancer is a heterogenous disease , the drivers of which remain unclear , making it difcult to treat these patients . 
pembrolizumab was approved for treating gi malignancies with mismatch repair deciencies and for third - line programmed death ligand 1positive gastric cancer based on its recently observed promising antitumor activity.2 , 3 however , it remains urgent to identify a subset of patients with gastric cancer who may benet from molecularly targeted agents . 
one such potential target is met amplication , which is observed in approximately 5% of patients with gastric cancer.3 - 9 savolitinib ( azd6094 , hmpl - 504 , volitinib ) is a potent small - molecule met kinase inhibitor that inhibits met inhibitory concentration kinase at a half - maximal ( ic50 ) of 4 nm and met phosphorylation in tumor cells . savolitinib was found to inhibit cell growth in vitro against tumors with met gene amplication in the absence of hepatocyte growth factor stimulation , with ic50 generally , 10 nm . 
 met inhibitor in met - amplied gastric cancer context key objective we evaluated the mechanisms of acquired resistance to savolitinib in 3 patients with met - amplied gastric cancer who showed a clinical response and then cancer progression using tumor and circulating tumor dna ( ctdna ) sequencing . knowledge generated ctdna is a powerful tool for identifying potential genomic aberrations that emerge during therapy to confer resistance to targeted therapies . 
using a next - generation sequencing 100 - gene panel , we identied the target mechanisms of resistance met d1228v / n / h and y1230c mutations or high copy number met gene amplications that emerge when resistance to savolitinib develops in patients with met - amplied gastric cancer . relevance we demonstrated the utility of ctdna in gastric cancer and conrmed this approach using baseline tumor tissue or rebiopsy . we identied various met mutations previously unidentied in gastric cancer upon progression to savolitinib , as well as met amplications as drivers of savolitinib resistance during monotherapy treatment of patients with met - amplied gastric cancer . circulating tumor dna ( ctdna ) from baseline until progression every 2 cycles to evaluate the tumor biology during treatment with targeted agents . 
the human investigations were performed after approval by a local human investigations committee ( institutional review board ) and in accordance with an assurance led with and approved by the health authority in korea . 
this prospective open - label trial was designed as a single - arm phase ii study at an academic cancer center ( clinicaltrials.gov identier : nct02449551 )  . treatment was administered as follows : savolitinib 800 mg once a day until disease progression or unacceptable toxicity . 
tumor tissue and plasma ctdna samples from 3 patients enrolled in the viktory trial were obtained before treatment , during therapy , and at the time of progression . next - generation sequencing a targeted next - generation sequencing 100 - gene panel was used to analyze matched tumor dna at baseline and progression and longitudinal ctdna to determine the mechanisms of acquired resistance to savolitinib ( az translational genomics labs , boston , ma )  . 
genes included in this panel are provided in appendix figure a1a . sequencing libraries were prepared using the kapa biosystems hyperprep kit ( wilmington , ma ) and roche nimblegen hybridization capture reagents ( basel , switzerland )  . 
raw sequencing data were processed using the bcbio framework.12 the quality of sequencing data was assessed using the multiqc report.13 fastq les were aligned to the reference genome hg38 using bwa mem aligner , 14 yielding a median depth of coverage of 2 , 000 ( range , 1 , 300 - 6 , 600 ) in plasma samples and 1 , 200 ( range , 1 , 100 - 1 , 400 ) in tissue samples . 
variants were called using vardict15 and classied into the following 3 tiers from high to low based on the likelihood of the variant contributing to cancer - relevant processes : known , likely , and unknown.15 copy number analysis of sequencing data were performed using the copy number caller seq2c.16 all plasma samples were analyzed together as a plasma cohort , whereas tissue samples were processed together as a tissue cohort . 
mapping and sequencing statistics for formalin - xed parafn - embedded tumor tissue ( fig a1b ) and ctdna from frozen plasma ( fig a1c ) indicated that  . 90% and 96% of the 100 genes were sequenced with 500 coverage in tumor and ctdna , respectively , providing a quality data set for analysis . et immunohistochemistry and met fluorescent in situ hybridization met immunohistochemistry ( ihc ) was performed using the rabbit monoclonal primary antibody , confirm antitotal met ( sp44 ; ventana medical systems , tucson , az ) according to the manufacturers protocol . 
 frigault et al performed using dual - color dna - specic met / cep7 probes ( abnova , walnut , ca ) , as described previously.5 , 8 results we analyzed the rst 3 patients enrolled in the savolitinib trial , which enrolls patients with gastric cancer with met amplication in the salvage setting . 
patients were screened for the presence of met amplication by tumor sequencing as part of the viktory trial and are conrmed wild type for met.11 the viktory trial screened 715 patients with genomic sequencing , and the incidence of met amplication was 3.5% ( 25 of 715 patients )  . 
in this study , we tested the feasibility of using a 100 - gene panel in patients with met - amplied gastric cancer serially from baseline until disease progression using both matched biopsies and ctdna . 
the patient had microsatellite - stable and her2 - negative gastric cancer ( fig 1a ) and experienced rapid progression after 5 cycles of capecitabine plus oxaliplatin ( initially stable disease ) to extensive dissemination in the lymph nodes ( fig 1b )  . 
the patient responded dramatically to 2 cycles of savolitinib ( fig 1b , middle panel ) , which was concordant with the decrease in the allele frequency of tp53 p190l ( 7% ) , met 1.4 copy number , and myc 3.4 copy number in the ctdna . 
notably , although the patient maintained a radiologic and clinical partial response ( pr ) to savolitinib , low frequencies of met d1228h ( 5% ) , met d1228n ( 5% ) , met d1228v ( 35% ) , and met y1230c ( 3% ) were newly detected . 
met d1228n is a resistant mutation to crizotinib in lung cancer.17 in addition , met d1228v has been shown to induce resistance to type 1 met tyrosine kinase inhibitors in lung cancer.18 finally , met y1230c is associated with resistance to crizotinib in nonsmall - cell lung cancer.19 the high concordance for the copy number level between ctdna 100 - gene sequencing and tumor rebiopsy specimen sequencing supports the usefulness of copy number evaluation from longitudinal plasma ctdna ( appendix fig a2 )  . 
at disease progression , the patient had mostly experienced progression to bone and bone marrow metastases rather than previous lymph nodes , suggesting the emergence of an aggressive clone that spread to the bone and bone marrow at progression . 
our data suggest that , rather than met amplications , met mutations drove the rapid progression observed in this patient ( fig 1c )  . the second patient was a 74 - year - old woman who was diagnosed with gastric cancer with extensive liver metastases at presentation and enrolled in the viktory trial at diagnosis . 
after 4 cycles of savolitinib , with her pr conrmed radiologically , the met copy number was 2.7 and showed a slight increase from diploid , and a tp53 g245d ( 2% ) variant began to emerge as detected in the ctdna . 
after 6 months ( 7 cycles of savolitinib ) , the patient developed radiologic progression . interestingly , in contrast to the newly emerging mutations conferring resistance to savolitinib in patient 1 ( fig 1 ) , the second patient developed a high level of met amplication of 13 copies and cdk6 copy number of 3.9 at progression ( fig 2a )  . 
although both genes are proximal to one another on chromosome 7 , they are not part of the same amplicon because the trap and pik3cg gene loci are between met and cdk6 , and they remained at a normal copy number in both the ctdna and tumor samples at progression ( fig 2b , top panel )  . 
high concordance was observed between the ctdna and tumor tissue dna ( liver metastasis ) with a reincrease in met amplication and cdk6 amplication that was not detected at pr . 
in addition , the ctdna sample at progression indicated that the tp53 g245d substitution containing the clone had expanded , as suggested by an increase from a 2% allele fraction ( at the third follow - up ) to a 22% allele fraction ( at progression )  . 
this was conrmed in the progression rebiopsy , where the same tp53 g245d substitution that was not detected in normal dna had subsequently increased to an 82% allele fraction ( fig 2b , bottom panel )  . the third patient was a 31 - year - old woman who underwent total gastrectomy for gastric cancer in 2013 . 
pathology , clinical assessment , and circulating tumor dna ( ctdna ) monitoring for patient 1 ( b5 - 002 ) identies met d1228 and y1230 mutations as mechanism of resistance to savolitinib . 
 ( a ) hematoxylin and eosin ( he ) , met immunohistochemistry ( ihc ) , and met uorescence in situ hybridization ( fish ; left to right ) from baseline tumor tissue . 
 ( b ) tumor assessment by radiologic assessment at baseline before savolitinib treatment , after 2 cycles at time of partial response ( pr ) , and after 4 cycles at time of progressive disease ( pd )  . 
clinical assessment and circulating tumor dna ( ctdna ) monitoring for patient 2 ( b5 - 001 ) identify on - target high - level met amplication ( amp ) as mechanism of resistance to savolitinib . 
 ( a ) radiologic assessment of tumor at baseline before savolitinib treatment ( follow - up [ fu ] 1 ) ; after 2 cycles ( fu2 ) and 4 cycles ( fu3 ) , both at time of partial response ( pr ) ; and after 7 cycles at time of progressive disease ( pd )  . 
 ( b ) copy number prole of ctdna plasma ( top ) and tumor tissue or normal dna at progression ( bottom ) , where each sample is represented by a different color at baseline ( fu1 ) , after 2 cycles ( fu2 ) and 4 cycles ( fu3 ) , and after 7 cycles at time of progression . patient was administered postoperative chemoradiation therapy with a ts - 1 plus oxaliplatin regimen and developed recurrent metastases to both ovaries 18 months later . 
 ( a ) hematoxylin and eosin ( he ) , met immunohistochemistry ( ihc ) , and met uorescence in situ hybridization ( fish ; left to right ) from baseline tumor tissue . 
 ( b ) tumor assessment by radiologic assessment at baseline before savolitinib treatment , after 2 cycles at time of partial response ( pr ) , and after 8 cycles at time of progressive disease ( pd )  . 
 frigault et al discussion the aim of this exploratory study was to determine whether relapses on savolitinib in patients with gastric cancer after an initial pr resulted from the development of on - target or bypass mechanisms of resistance . 
furthermore , we established the utility of ctdna from plasma as a matrix for monitoring changes in dna alterations during the course of treatment of gastric cancer and demonstrated the concordance of genomic alterations in ctdna to tumor biopsy both before treatment with a targeted therapy and at the time of progression . 
the efcacy of the trial will be reported once the trial completes recruitment ; here , we focused on the utility of ctdna sequencing to identify potential resistance mechanisms in gastric cancer after met inhibition . 
we identied the following two potential mechanisms of acquired resistance at progression following a dramatic response to savolitinib in met - amplied gastric cancer : newly developed met mutations previously only described in lung cancer and an increase in the met copy number at resistance , which decreased during the clinical response but increased again at disease progression . in the rst patient , newly emerging met d1228h ( 31% ) , met d1228n ( 12% ) , met d1228v ( 1% ) , and met y1230c ( 1% ) mutations were detected with the sudden onset of disease progression to multiple bones and the bone marrow . 
this patient died of rapid progression immediately after developing resistance to savolitinib therapy . mutations in met , including at positions d1228 and y1230 , are among the reported mechanisms of acquired resistance in preclinical models21 , 22 and have been reported to confer clinical resistance to met inhibition in lung cancer.17 , 19 the cocrystal structure of the met kinase domain and met kinase inhibitor revealed an important binding interaction of the met inhibitor and y1230 and explains the abrogation of compound binding with the emergence of mutations at this residue . 
in addition , d1228 is engaged in interactions with other residues to maintain the activation loop in a conformation that enables the critical interaction between y1230 and the met inhibitor.21 these results demonstrate that the on - target resistance mutations emerge in met - amplied gastric cancer treated with a selective met kinase inhibitor . 
therefore , upregulation of met ( in a savolitinib - responsive tumor ) similar to her2 ( in a lapatinib - responsive tumor ) may confer resistance via epithelial to mesenchymal transition and by promoting a metastatic phenotype.26 , 27 an on - target met copy number gain as a mechanism of resistance has been reported in lung cancer , where one met exon 14skipping patient became a responder to a met inhibitor in the clinic ; however , at the time of progression , the exon 14 met allele was amplied , but not the wild - type allele of met , 28 suggesting that highlevel amplication of the met gene is a mechanism of resistance to met inhibitors across indications . in 2 of 3 patients studied , ctdna was detectable in the circulation , harboring somatic alterations in the met pathway that changed over time and were conrmed by rebiopsy at recurrence . 
our data agree with this hypothesis ; in the rst patient , tp53 p190l changed from a fraction of 44% at baseline to 7% during pr and then back to 13% at disease progression , which was further conrmed in tumor tissue with a 17% allele fraction harboring the same mutation in tp53 . 
 met inhibitor in met - amplied gastric cancer contained no detectable ctdna tp53 until after 4 cycles , at which point a g245d amino acid substitution was detectable at a 2% allele fraction and increased to 22% at progression . 
the same alteration was identied by rebiopsy at an 82% allele fraction . in 1 of 3 patients studied , no mutations in any of the 100 genes on the high - coverage deep - sequencing gene panel were detected , and therefore , this patients tumors may not be shedding ctdna into circulation . 
this patient demonstrates the limitations of the use of ctdna to the 57% - 87% of patients with gastric cancer who are shedding ctdna from their tumor into circulation.30 , 31 this patient highlights that tumor collection at the time of progression will still be important for identifying resistance mechanisms to targeted treatments in nonshedders and to understand tumor heterogeneity . in summary , ctdna is a powerful tool for identifying potential genomic aberrations that emerge during therapy to confer resistance to targeted therapies . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . aleksandra markovets employment : astrazeneca stock and other ownership interests : astrazeneca barrett nuttall employment : astrazeneca , cvs health ( i ) stock and other ownership interests : astrazeneca , cvs health ( i ) travel , accommodations , expenses : astrazeneca , cvs health ( i ) se hoon park honoraria : merck sharp & dohme , sano - aventis consulting or advisory role : eli lilly , janssen oncology research funding : kura oncology , ono pharmaceutical esha a . 
gangolli employment : clovis oncology stock and other ownership interests : astrazeneca , clovis oncology , novartis , merck , bristol - myers squibb , jounce therapeutics , unum therapeutics , incyte , alcon , guardant health , titan medical travel , accommodations , expenses : clovis oncology peter g.s. 
nat rev dis primers 3 : 17036 , 2017 fuchs c , doi t , jang r , et al : keynote - 059 cohort 1 : efcacy and safety of pembrolizumab ( pembro ) monotherapy in patients with previously treated advanced gastric cancer . 
n engl j med 372 : 2509 - 2520 , 2015 lee j , ou sh , lee jm , et al : gastrointestinal malignancies harbor actionable met exon 14 deletions . 
mod pathol 26 : 1632 - 1641 , 2013 lee j , kim km , kang wk , et al : innovative personalized medicine in gastric cancer : time to move forward . 
nature 513 : 202 - 209 , 2014 lee j , seo jw , jun hj , et al : impact of met amplication on gastric cancer : possible roles as a novel prognostic marker and a potential therapeutic target . 
oncol rep 25 : 1517 - 1524 , 2011 ahn s , brant r , sharpe a , et al : correlation between mek signature and ras gene alteration in advanced gastric cancer . 
ou si , young l , schrock ab , et al : emergence of preexisting met y1230c mutation as a resistance mechanism to crizotinib in nsclc with met exon 14 skipping . 
kim st , banks kc , pectasides e , et al : impact of genomic alterations on lapatinib treatment outcome and cell - free genomic landscape during her2 therapy in her2 + gastric cancer patients . 
tiedt r , degenkolbe e , furet p , et al : a drug resistance screen using a selective met inhibitor reveals a spectrum of mutations that partially overlap with activating mutations found in cancer patients . 
kim dc , park kr , jeong yj , et al : resistance to the c - met inhibitor krc - 108 induces the epithelial transition of gastric cancer cells . 
oliveras - ferraros c , corominas - faja b , cuf s , et al : epithelial - to - mesenchymal transition ( emt ) confers primary resistance to trastuzumab ( herceptin )  . 
shi j , li f , yao x , et al : the her4 - yap1 axis promotes trastuzumab resistance in her2 - positive gastric cancer by inducing epithelial and mesenchymal transition . 
awad mm , bahcall m , sholl lm , et al : mechanisms of acquired resistance to met tyrosine kinase inhibitors ( tkis ) in met exon 14 ( metex14 ) mutant non - small cell lung cancer ( nsclc )  . 
 ( b ) sequencing and mapping statistics of tissue samples and ( c ) plasma circulating tumor dna ( ctdna ) describing number of sequenced reads , percentage of aligned reads , percentage of duplicated reads , percentage of reads mapped on targets ( + 200 base pairs ) , percentage of usable reads , average depth of coverage , gc content ( percentage of nitrogenous bases that are either guanine or cytosine ) , average insert size , and percentage of targeted bases with given coverage . 
 next - generation sequencing reveals potentially actionable alterations in the majority of patients with lymphoid malignancies purpose next - generation sequencing ( ngs ) identifies potentially targetable alterations by us food and drug administration ( fda ) approved drugs and / or by available experimental agents that may not have otherwise been contemplated . 
many targeted drugs have been developed for diverse solid cancers ; a smaller number of genomically targeted drugs have been approved for lymphoid malignancies . materials and methods we analyzed ngs results from 60 patients with various lymphoid malignancies and found 224 alterations ( median per patient , three alterations )  . results forty - nine patients ( 82% ) had potentially actionable alterations with the use of fdaapproved drugs and / or experimental therapies ; only 11 patients ( 18% ) had no theoretically actionable alterations . 
only three patients ( 5% ) had an alteration for which an approved drug in the disease is available ( on label ) ; 45 patients ( 75% ) had an alteration for which an approved drug is available for another disease ( off label )  . 
of note , 19 ( 32% ) of 60 patients had intermediate to high tumor mutational burden , which may predict response to certain immunotherapy agents . conclusion ngs identifies alterations that may be pharmacologically tractable in most patients with lymphoid malignancies , albeit with drugs that have usually been developed in the context of solid tumors . 
goodman michael choi matthew wieduwilt carolyn mulroney caitlin costello garrett frampton vincent miller razelle kurzrock author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : aaron m . 
goodman , md , moores cancer center , university of california san diego , 3855 health science dr , la jolla , ca 92093 ; e - mail : a1goodman@ucsd.edu. introduction the lymphoid malignancies have diverse biologic and clinical behavior and typically are treated with multiagent chemotherapy . 
many therapeutic regimens for b - cell non - hodgkin lymphomas and leukemias also incorporate the anti - cd20 monoclonal antibody rituximab , which has improved patient outcomes.1 treatment of metastatic solid tumors , like lymphoid malignancies , has also relied heavily on the use of cytotoxic chemotherapy . however , over the past decade , the treatment paradigm for metastatic solid tumors has shifted away from chemotherapy toward matching oncogenic driver mutations with targeted therapy ( precision medicine ) .2 - 4 for example , in patients with braf - mutated metastatic melanoma , the braf inhibitor vemurafenib markedly increases overall survival compared with chemotherapy.5 numerous targeted therapies are now approved by the us food and drug administration ( fda ) for patients with metastatic solid tumors across a wide array of histologies ( data supplement )  . 
the first example of targeted therapeutic efficacy is the hematologic disorder chronic myelogenous leukemia , which has been transformed by the use of agents that affect bcr - abl kinase activity . despite the rapid success in development , approval , and use of small - moleculetargeted agents in patients with solid malignancies , a paucity of such therapies approved for use in lymphoid malignancies remains ( data supplement )  . 
 small - moleculetargeted therapeutics are not an available option . the rapid technological advances in nextgeneration sequencing ( ngs ) have allowed oncologists to sequence tumor exomes in a clinically meaningful period of time.6 - 8 some studies have shown that patients with solid malignancies treated with matched therapy have improved outcomes , 9 and meta - analyses in approximately 85 , 000 patients have supported this finding.10 - 12 the targeting of alterations such as braf can result in responses across a wide variety of cancers , including lymphoid malignancies ( eg , hairy cell leukemia ) .13 , 14 although not all malignancies that harbor braf mutations will respond equally well to braf inhibition , the strategy of crosscancer basket trials has been established as highly worthwhile . ngs accurately identifies substitutions , indels , copy number alterations , and gene fusions in hematologic malignancies.15 in this report , we use this technology to analyze the genomic alterations in a cohort of 60 patients with various lymphoid malignancies to estimate the frequency of theoretically actionable alterations . 
this study was performed and consents obtained in accordance with university of california san diego institutional review board guidelines . tumor samples from tissue ( table 1 ) or peripheral blood were collected from 60 patients and submitted for ngs to foundation medicine , a laboratory improvement amendments clinical certified laboratory for ngs . 
the foundationone heme panel was used , which is a hybrid capturebased ngs test.16 the methods used in this assay have been described in detail in previous reports.7 , 15 the foundationone heme assay simultaneously detects all genomic alterations , including base pair substitutions , indels , copy number alterations , and select gene rearrangements , in 405 cancer - related genes . 
for tumor mutational burden ( tmb ) , the number of somatic mutations detected on ngs are quantified , and that value was extrapolated to the whole exome by using a validated algorithm described in detail in earlier publications.17 , 18 alterations with known and likely effects on functional status are not counted . definition of actionable alteration an alteration was defined as potentially actionable if its protein product is a component of a molecularly defined pathway for which there is at least one available fda - approved drug or investigational drug that may affect the function of the protein product of the alteration or the immediate downstream effectors of the protein product or that differentially recognizes the protein in tumor versus normal cells . 
the protein products of genomic alterations were considered to be functional the genomic alterations have been previously identified as relevant to cancer in the cosmic database , 19 which catalogs recurrent somatic alterations in cancer . 
novel base substitution , indel , and rearrangement alterations that result in truncations and homozygous copy number deletions that occur in tumor suppressor genes were considered to have likely functional implications . 
novel genomic alterations that occur at the same position as known alterations as well as alterations with conflicting evidence with regard to implication for function were subject to review by an internal panel of subject matter experts to determine functional status of the relevant protein product on the basis of all available evidence , including , but not limited to , the exac , dbsnp , and clinvar databases.20 - 22 data and statistical analyses patient characteristics were obtained through electronic medical record review . 
descriptive statistics were used , including medians , ranges , and frequencies . results patient characteristics sixty patients ( 35 men [ 58% ] and 25 women [ 42% ] ) with lymphoid malignancies were identified ( table 1 )  . 
the most common malignancy in the cohort was chronic lymphocytic leukemia ( cll ; 32% ) , followed by acute lymphoblastic leukemia ( all ; 20% ) , multiple myeloma ( 18% ) , diffuse large b - cell lymphoma ( dlbcl ; 10% ) , follicular lymphoma ( 8% ) , and other lymphoid neoplasms ( 5% )  . 
however , the actual alteration in nras differed between the two patients ( nras g13d v nras q61r )  . the median number of alterations detected per patient was three ( range , zero to 14 )  . 
as demonstrated in figure 1b , seven patients ( 12% ) had no reportable alterations , 10 ( 17% ) had one alteration , and 43 ( 71% ) had two or more alterations . 
the maximum number of alterations identified was 14 , which was observed in two patients ( 3% ) , one with cll , the other with dlbcl . of note , all patients with dlbcl had five or more alterations . actionable alterations potentially actionable alterations were identified in all disease subtypes ( table 2 )  . 
all disease subtypes , except marginal zone lymphoma , had alterations targetable by fda - approved drugs . forty - nine patients ( 82% ) had potentially actionable alterations with fda - approved drugs and / or experimental therapies ( clinical trials ) , whereas 11 patients ( 18% ) had no theoretically actionable alterations . depicted in figure 2 is the number of patients with potentially fda actionable alterations per disease group . 
only three patients had an alteration for which an approved drug in the disease is available ( on label ) , whereas 45 patients ( 75% ) had an alteration for which an approved drug is available in another disease ( off label )  . 
eleven patients had no targetable alterations ; these patients included seven with no detected genomic alterations . two patients with b - cell all ( b - all ) and one with waldenstr om macroglobulinemia had alterations targetable with on - labelapproved drugs ( fig 3 )  . 
high tmb was seen in five patients ( 8% ) , intermediate in 14 ( 23% ) , and low in 40 ( 67% )  . tmb was not available for one patient ( 2% )  . intermediate to high tmb was noted across almost all histologies ( except for marginal zone lymphoma , natural killer / t - cell lymphoma , and cutaneous t - cell lymphoma )  . 
three patients with multiple myeloma had an intermediate level of tmb . discussion this study demonstrates that in the majority of patients ( 82% ) with lymphoid malignancies whose disease was interrogated by ngs , alterations were found that might be pharmacologically tractable , a percentage similar to the 77% reported by he et al15 for diverse hematologic malignancies . 
another study reported that 70% of patients with various solid tumors had an alteration that was theoretically actionable with an approved drug.24 this finding is similar for lymphoid malignancies , with 75% of the current study patients having an alteration potentially actionable by an approved drug . 
table 3 lists therapeutics with their corresponding targets that were identified in the patient cohort . one of the major obstacles to performing comprehensive genomic profiling of clinical specimens is the necessity for an adequate tumor sample . 
unlike solid malignancies where invasive biopsy is almost always required to obtain a tissue sample , comprehensive genomic profiling of lymphoid malignancies often can be performed with the use of peripheral blood and / or bone marrow . in this cohort , 54% of patients had specimens obtained from blood and / or bone marrow . tumors can acquire new mutations as they progress , which underscores the importance of obtaining new tissue when available for sequencing at the time of therapeutic decision making . 
 other not actionable , 2 mm not actionable , 2 other actionable , actionable , actionable , cll not actionable , fl not actionable , 2 actionable , 3 actionable , dlbcl actionable , fig 2 . 
in one study , 42% of patients did not have metastatic disease at the time of their biopsy.24 lymphoid malignancies are more amenable to repeat biopsy , with more than one half of the current cohort having tissue available from the blood and / or bone marrow . 
this accessibility facilitates repeat ngs to guide therapy . over the past decade , 26 orally administered targeted therapies have been fda approved for the treatment of 13 different solid malignancies ( data supplement )  . 
over the same period , only five orally administered targeted therapies have been approved for the treatment of lymphoid malignancies ( philadelphia chromosomepositive all , cll , follicular lymphoma , mantle cell lymphoma , and waldenstr om macroglobulinemia )  . the current data demonstrate that 45 patients ( 75% ) had an alteration that theoretically could have been targeted with an approved , albeit offlabel , drug , whereas only three patients ( 5% ) had an alteration for which an approved on - label drug was available . 
in a similar study in patients with solid malignancies , 20% had an alteration targeted by on - label agents , whereas 67% had an alteration targetable by off - label use.24 ( of note , the study used the same definitions for actionability as were used in this analysis . ) currently , a paucity of orally administered targeted therapy is available for onlabel use in lymphoid malignancies . 
however , as our findings suggest , the majority of cases likely will have potentially targetable alterations . the mutational landscape for numerous lymphomas has now been well characterized by several whole - exome sequencing studies.46 , 47 for example , mll2 , crebbp , and tp53 alterations in dlbcl , as described by pasqualucci et al , 46 were some of the most common recurrent mutations in the current cohort of patients with dlbcl . 
this alteration was also the most common ( 12% ) in a cohort of patients with cll sequenced by puente et al.47 furthermore , 82% of our patients had alterations that were pharmacologically tractable , similar to the 77% reported by he et al15 in diverse hematologic malignancies . 
these similar findings in other cohorts provide further support of the generalizability of our findings to other large cohorts of lymphoid malignancies . myd88 , an adapter protein used by toll - like receptors , was shown to be mutated ( myd88 l265p ) in  . 
90% of patients with waldenstr om macroglobulinemia ( lymphoplasmacytic lymphoma ) .48 this mutation not only is relatively specific for the disease but also predicts clinical presentation and survival.49 myd88 signaling is important in lymphomagenesis and signals through btk.50 in a phase ii trial , ibrutinib produced an overall response rate of 91% in a group of previously treated patients with waldenstr om macroglobulinemia , which led to its fda approval.37 furthermore , response rates to ibrutinib were significantly higher in patients with myd88 mutations versus wild - type myd88.51 in the current cohort , myd88 l265p mutation was found in the one patient with waldenstr om macroglobulinemia . 
however , myd88 alterations were also identified in one patient with dlbcl ( myd88 l265p ) , one with follicular lymphoma ( myd88 s219c ) , and one with primary cns lymphoma ( myd88 l265p )  . 
myd88 mutations have been discerned in marginal zone b - cell lymphoma , 52 cll , 53 dlbcl , 54 and primary cns lymphoma.55 preliminary data from a phase i trial of single - agent ibrutnib in four patients with cns lymphoma demonstrated responses in two of the three patients evaluated . 
in a phase i trial of 17 patients with relapsed mantle cell lymphoma treated with single - agent palbociclib , five ( 18% ) achieved progression - free survival of  . 
1 year , with one complete and two partial responses.58 the high percentage of cdkn2a / b alterations in the current study population gives further rationale for designing trials with cdk inhibitors in lymphoid malignancies . activating mutations in braf were found in three patients with cll ( two with braf g469a and one with braf v600e ) and one patient with multiple myeloma ( braf v600e )  . 
these mutations are potentially targetable by the braf inhibitors vemurafenib and dabrafenib and the mek inhibitors trametinib and cobimetinib.5 , 27 braf alterations have been identified as a driver mutation and as a biomarker for sensitivity to braf inhibition in both hairy cell leukemia and erdheim - chester disease.59 - 61 braf alterations have been found in approximately 3% of patients with cll.62 in the current study , two patients had mutations that led to an alanine substitution for a glycine at position 469 . 
ngs readily identified philadelphia chromosomelike b - all and can assist in selecting patients for clinical trials of targeted agents aimed at improving the poor outcome of these patients.15 higher neoantigen burden , which may be largely predicted by tmb , has been associated with higher objective response rates and progressionin patients treated with pd - 1 free survival blockade.67 , 68 melanoma , lung cancer , and renal cell carcinoma , all of which are highly responsive to pd - 1 blockade , have been shown to have a high degree of mutational burden from wholegenome and - exome sequencing studies.69 in the current cohort , tmb ranged from one or fewer to 140 ( data supplement )  . 
intermediate to high tmb was noted across almost all histologies ( except for marginal zone lymphoma , natural killer / t - cell lymphoma , and cutaneous t - cell lymphoma )  . 
the majority of the patients had cll , multiple myeloma , and all , whereas other nonhodgkin lymphomas were less well represented . although the majority of patients had actionable mutations theoretically targeted by fda - approved drugs , in practice , insurance approval for off - label drug use often is difficult to obtain.73 in addition , no standard definition exists for a targetable alteration , and the level of evidence needed to support this is a matter of debate . 
the number of actionable alterations discussed in this article may be overestimated , but even so , these patients should still be directed toward clinical trials that target these alterations so that the responsiveness or lack thereof can be determined . 
numerous additional clinical trials with a standardized definition of what constitutes a targetable alteration are needed to determine the extent to which patients respond when an alteration is theoretically druggable . 
currently , a number of such trials are ongoing ( clinicaltrials.gov identifiers nct02534675 , nct00851032 , and nct02465060 )  . in conclusion , we found that most patients with lymphoid malignancies have unique and complex molecular portfolios . 
goodman administrative support : caitlin costello , razelle kurzrock provision of study materials or patients : michael choi , matthew wieduwilt , carolyn mulroney , caitlin costello collection and assembly of data : aaron m . 
 novartis , merck , roche / genetech , genentech mypath , foundation medicine , pfizer , guardant health , merck serono patents , royalties , other intellectual property : four patents travel , accommodations , expenses : win , emd serono , gateway research advisory committee , icrp , win 2015 , caris centers of excellence , aacr , association of american cancer institutes , emd serono & quintiles , global biomarkers consortium , guardant health , global source ventures / novena therapeutics , ascpt , meyers consulting , fda - ocra , genentech , orbimed / global source ventures , sylvester cancer center , journal of precision medicine , curematch , lynx group , mayo clinic cancer center , kaiser permanente , pancan , cedars - sinai , medimmune / jk associates medical communications group affiliations aaron m . 
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 radiogenomics analysis of intratumor heterogeneity in a patient with high - grade serous ovarian cancer britta weigelt , phd1 ; hebert alberto vargas , md1 ; pier selenica1 ; felipe c . 
reis - filho , md , phd1 ; and evis sala , md , phd1 , 3 introduction the overall survival of patients with high - grade serous ovarian cancer ( hgsoc ) has not improved during the past 20 years.1 studies have revealed that genomic intratumor heterogeneity correlates with poor survival2 , 3 and specic patterns of malignant cell spread in hgsoc.4 the physical distribution of malignant clones across the peritoneal cavity may be nonrandom , because some sites harbor genetically diverse clones.5 these region - specic properties may invasion and expansion , modulate malignant cell thereby shaping evolutionary selection.3 , 6 our understanding of genomic heterogeneity in hgsoc is limited to single biopsies ; little is known about individual spatial and temporal variation across various tumor sites.2 - 5 hence , developing imaging methods for guiding tissue sampling to physiologically and metabolically distinct tumor habitats is desirable . 
such approaches will be vital for new clinical trials , especially those combining immunologic and genomically targeted therapies . here we use lesion - specic three - dimensional ( 3d ) molds for phenotypic image - guided tumor sampling to ensure spatial colocation of imaging , histology , and genomic data , critical for understanding tumor biology . phenotypic imaging maps of heterogeneity ( ie , imaging habitats ) of two hgsoc sites were obtained by combining perfusion , diffusion , and metabolic maps derived from multiparametric imaging . 
four days before primary cytoreductive surgery the patient underwent same - day multiparametric magnetic resonance imaging ( mpmri ; discovery mr750 3t mri system , ge healthcare , chicago , il ) of the abdomen and pelvis and 18f - uorodeoxyglucose ( fdg ) positron emission tomography ( pet ) / computed tomography ( ct ; discovery pet / ct system , ge healthcare )  . 
details of image acquisition , analysis , and mr - pet / ct coregistration are described in the appendix and in appendix table a1 . cluster - guided specimen sampling imaging habitats were identied using k - means clustering of the standardized uptake value ( suv ) , diffusion coefcient ( d ) , perfusion fraction ( f ) , and transfer constant ( dynamic contrast - enhanced parameter ktrans ) voxels , with the number of clusters ( k ) being xed to k = 3.7 custom - made 3d molds of the lesions were printed using a 3d printer ( makerbot replicator 2 ; makerbot , brooklyn , ny ) on the basis of manual segmentation of the right ovarian tumor and metastatic implant on the axial t2 - weighted mri ( appendix )  . 
tissue samples of each imaging cluster were obtained , cut in half , and formalin - xed and parafn - embedded for histopathologic analysis or snap - frozen for genomic analysis ( fig 1a )  . histologic review and immunohistochemistry the three right ovarian mass hgsoc imaging - based habitats ( labeled blue , yellow , or green ) and the omental implant ( blue ) were reviewed by two pathologists blinded to the habitat assignment . 
 ( a ) phenotypically distinct areas of a highgrade serous ovarian cancer ( hgsoc ) were identied by k - means clustering of imaging features derived from magnetic resonance imaging ( mri ) and positron emission tomography ( pet ) / computed tomography . 
the distinct imaging habitats ( labeled blue , yellow , and green ) were sampled from the surgically removed primary hgsoc and metastatic implant using a three - dimensional ( 3d ) mold . 
half of each imaging - based tissue area was formalin - xed parafnembedded for histopathologic review and immunohistochemical analysis , and the other half was ash - frozen for whole - exome sequencing analysis . 
 ( b ) micrographs of representative hematoxylin and eosin ( h and e ) stained sections of the imaging - based hgsoc areas ( top row ) , and immunohistochemical analysis of cd31 , ki - 67 , ca - ix , and hif - 1 . 
 ( c ) imaging features associated with the distinct color areas as dened by k - means clustering of standardized uptake values ( suv ) , diffusion coefcient ( d ) , dynamic contrast - enhanced dce parameter ( ktrans ) , and water volume fraction owing through microvessels ( f ) are plotted on top , and the histopathologic features of the distinct imaging - based tumor areas are shown at the bottocolor - coding according to the legend . dw , diffusion - weighted ; fdg , 18f - uorodeoxyglucose ; til , tumor - inltrating lymphocyte . nonsynonymous somatic mutations ( 74% ) not detected in all tumor areas by wes were independently validated using a custom hybrid - capture targeted massively parallel sequencing assay . 
the clusters were labeled blue ( lowest ktrans , highest suv , highest f ) , yellow ( highest d , lowest f ) , or green ( lowest d , highest ktrans , lowest suv )  . 
the right ovarian cancer contained all three distinct imagingbased clusters , whereas the omental metastatic implant was entirely composed of one cluster ( blue ; fig 1a ) , suggestive of phenotypic imaging heterogeneity in the primary hgsoc . tissue from the distinct imaging - based clusters for immunohistochemical and genetic analyses was obtained through a custom - made 3d mold ( fig 1a )  . imaging - based clusters are underpinned by distinct growth patterns and expression of hypoxia - related markers phenotypic imaging - based clusters were associated with distinct histopathologic growth patterns . 
 ( d ) unsupervised hierarchical clustering of the somatic mutations ( left ) and of the gene copy number alterations ( right ) identied not to be shared by all four imaging - based hgsoc areas using wards algorithm and euclidean distance . left , genes affected by mutations are shown in black ; right , amplication , gain , loss , and deletion are shown in dark red , red , blue , and dark blue , respectively . 
the values on the edges of the clustering are derived from pvclust analysis to assess the stability of the clusters ; both the approximatelyunbiased and bootstrap - probability p values were 100% . 
 weigelt et al signature 1 signature 3 other signatures mutant wild type somatic mutations copy number alterations amplification no change deletion gain loss ovary green ovary yellow ovary blue omentum blue ovary green ovary yellow ovary blue omentum blue 7q11 amp 2q11 amp ovary yellow ovary green tp53 pot1 16p12 amp 6p21 amp ovary blue fig 2 . 
the expression levels and patterns of the hypoxia - marker hif - 1 and its downstream target ca - ix correlated with the distinct areas dened by multiparametric imaging ( fig 1c )  . 
consistent with the imaging ndings , which demonstrated that the ovary blue and omentum blue areas displayed the highest f , an mri marker of tissue vascularity , cd31 immunohistochemical assessment revealed a higher density of tumor neovascularization ( 4 + ) in the ovary blue and omentum blue areas than in the ovary green and ovary yellow areas ( 2 + ; fig 1c )  . 
furthermore , distinct patterns and levels of ca - ix expression were observed among these areas , with ovary yellow and green having h - scores of 80 , compared with 230 and 195 in ovary blue and omentum blue , respectively . 
for hif - 1 , a reverse pattern was found , with ovary yellow and ovary green areas displaying high levels of hif - 1 expression ( h - scores , 115 ) compared with ovary blue and omentum blue ( h - scores , 75 and 60 , respectively ; figs 1b and 1c )  . imaging - based clusters are underpinned by distinct repertoires of genetic alterations high - depth wes of microdissected tumor and normal samples revealed 50 nonsynonymous somatic mutations , including a tp53 p.p47tfs * 5 frameshift mutation , which were shared among all four imaging - based tumor areas ( fig 2 )  . 
twenty - eight nonsynonymous somatic mutations were shared exclusively between ovary blue and omentum blue , and 46 between the ovary green and ovary yellow components ( fig 2a )  . 
although all imaging habitats displayed genomics features of homologous recombination dna repair deciency ( dominant mutational signature 3 , high large - scale transition scores ; fig 2c ) , hierarchical clustering of the 146 nonsynonymous somatic mutations or the 718 gene copy number alterations not shared among all four imagingbased areas revealed that both at the mutational and gene copy number levels , ovary blue and omentum blue clustered together and were distinct from ovary yellow and ovary green ( fig 2d )  . 
several somatic mutations found to be subclonal in ovary blue , including mutations affecting auts2 , eif2ak4 , and trim41 , became clonal in omentum blue ( fig 2a ) , and a subset of genes affected by copy number losses in ovary blue became homozygously deleted in omentum blue ( eg , chromosome 18q23 ; fig 2d )  . discussion several studies have demonstrated that hgsocs display spatial and temporal genetic heterogeneity , 2 - 6 , 22 with tumors composed of genetically distinct clones and exhibiting distinct evolutionary trajectories and mechanisms of therapy resistance.4 , 23 , 24 our observations support the contention that phenotypic and genetic analysis of single biopsy or single tumor samples may not provide a sufciently accurate representation of hgsoc heterogeneity.4 this proof - of - principle study suggests that multiparametric imaging assessment may provide a noninvasive surrogate for intratumor genetic heterogeneity and may guide precise tissue sampling . 
given the evidence supporting the impact of intratumor genetic heterogeneity on tumors metastatic ability and resistance to therapeutic interventions , 25 the results of this proof - of - principle observation provide the basis for studies to dene the type of sampling required for the assessment of preand posttreatment hgsocs . 
it should be noted , however , that multiparametric imaging for tumor heterogeneity and tumor evolution assessment requires not only manual segmentation of the imaging data but also standardization of the image acquisition protocols across different imaging platforms . targeted therapy and immunotherapy are being progressively applied earlier in the treatment of patients with cancer , and certain agents are anticipated to become part of front - line therapy . 
minimally invasive methods for disease monitoring in the form of circulating cell - free plasma dna hold great promise in the assessment of genetic heterogeneity within a patient.26 - 28 our imaging habitatbased method would constitute a noninvasive and complementary approach to such endeavors , given that it may allow for the sampling of selected image habitats without having to analyze every section of every tumor , an impossible task particularly in the metastatic and recurrent settings . 
for more information about asco 's conict of interest policy , please refer to or po.ascopubs.org / site / ifc . britta weigelt consulting or advisory role : genentech ( i ) , invicro ( i ) , ventana medical systems ( i ) , volitionrx ( i ) , paige.ai ( i ) , goldman sachs ( i ) felipe c . 
 weigelt et al niamh conlon employment : abbvie ( i ) stock and other ownership interests : merck ( i ) alexandra snyder employment : adaptive biotechnologies , merck stock and other ownership interests : merck consulting or advisory role : driver group research funding : bristol - myers squibb travel , accommodations , expenses : genentech , bristol - myers squibb robert a . 
assignee : the regents of the university of california august 18 , 2015 ( inst ) ; application : compositions and methods for the diagnosis and treatment of ovarian cancers that are associated with reduced smarca4 gene expression or protein function ( inst ) ; royalties from published books : cambridge university press and springer publishing dennis s . 
chi leadership : csurgeries stock and other ownership interests : bovie medical , verthermia , intuitive surgical , transenterix consulting or advisory role : bovie medical , verthemia ginger j . 
reis - filho consulting or advisory role : genentech , invicro , ventana medical systems , volitionrx , paige.ai , goldman sachs evis sala honoraria : siemens healthineers speakers ' bureau : siemens healthineers travel , accommodations , expenses : siemens healthineers no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
ca cancer j clin 68 : 7 - 30 , 2018 schwarz rf , ng ck , cooke sl , et al : spatial and temporal heterogeneity in high - grade serous ovarian cancer : a phylogenetic analysis . 
cell 173 : 1755 - 1769.e22 , 2018 bashashati a , ha g , tone a , et al : distinct evolutionary trajectories of primary high - grade serous ovarian cancers revealed through spatial mutational proling . j pathol 231 : 21 - 34 , 2013 5 . 
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dowsett m , nielsen to , ahern r , et al : assessment of ki67 in breast cancer : recommendations from the international ki67 in breast cancer working group . int j gynecol pathol 34 : 437 - 444 , 2015 working group 2014 . 
detre s , saclani jotti g , dowsett m : a quickscore method for immunohistochemical semiquantitation : validation for oestrogen receptor in breast carcinomas . j clin pathol 48 : 876 - 878 , 1995 110 : 1030 - 1034 , 2018 15 . 
schultheis am , ng ck , de filippo mr , et al : massively parallel sequencing - based clonality analysis of synchronous endometrioid endometrial and ovarian cancer res 72 : 5454 - 5462 , 2012 carcinomas . 
the examination was performed on a 3t magnetic resonance imaging ( mri ) whole - body scanner unit ( discovery mr750 ; ge healthcare , chicago , il ) using a dedicated multichannel torso phased - array coil as the receive coil . the standard protocol included the following sequences acquired in two - dimensional t2 - weighted fast spin - echo , t1an axial plane : weighted gradient - echo . 
single - shot incoherent motion intravoxel ( ivim ) based diffusion - weighted images were obtained using echoplanar imaging with a pair of motion - probing gradients along three orthogonal axes , using a chemical shift selective fat - saturation technique . 
dynamic contrast - enhanced ( dce ) images were acquired before and after the intravenous injection of gadopentetate dimeglumine ( magnevist ; berlex laboratories , montville , nj ; 0.1 mmol per kilogram of body weight at a rate of 2 ml / s ) using an automatic injector ( medrad , bayer , pittsburgh , pa )  . 
the patient was scanned on a dedicated positron emission tomography ( pet ) / computed tomography ( ct ) system ( discovery 690 ; ge healthcare , chicago , il )  . 
a standard - of - care acquisition protocol was applied with an intravenous injection of approximately 400 to 455 mbq 18f - uorodeoxyglucose after at least 6 hours of fasting and documentation of blood glucose less than 200 mg / dl followed by a 60 - minute uptake period . 
subsequently , a low - dose , attenuation - correction ct scan ( 120 to 140 kv , approximately 80 ma ) was acquired with the patient in the supine position , followed by acquisition of pet emission images of the whole body ( 3 minutes per bed position , ve to six bed positions )  . imaging analysis and mr - pet coregistration . 
using anatomic landmarks available on axial t2 - weighted mr images and on the axial pet and low - dose ct images , the tumor regions outlined on mri were coregistered with pet . 
this was achieved by calculating the mean location ( corresponding to the center of mass of the tumor ) on the mri image ( t2w ) and the corresponding mean location on the pet / ct image . 
rigid registration was selected to ensure that the geometry ( and the voxel count ) of the region of interest ( roi ) for each slice was maintained between mri and pet . 
the translational matrix was applied to the roi for each slice to determine the displacement of the roi . the ivim biexponential model proposed by le bihan et al ( le bihan d , et al : radiology 168 : 497 - 505 , 1988 ; le bihan d , et al : radiology 161 : 401 - 407 , 1986 ; le bihan d , et al : magn reson med 10 : 324 - 337 , 1989 ) was used to estimate the diffusion parameters for each lesion outlined , including diffusion coefcient ( d ) and the volume fraction of the water owing through the microvessels ( f )  . 
the segmented analysis procedure ( callot v , et al : magn reson med 50 : 531 - 540 , 2003 ; yao l , et al : acad radiol 7 : 27 - 32 , 2000 ) was used to estimate ivim parameters on a voxel - wise basis . 
pharmacokinetic analysis of the dce data were carried out using a one - compartment tofts model ( tofts ps : j magn reson imaging 7 : 91 - 101 , 1997 )  . 
for each outlined lesion , voxel - wise estimates of the volume transfer constant between the blood plasma and the extravascular extracellular space ( ktrans [ min1 ] ) was calculated . 
arterial input function was calculated using a biexponent model as previously described ( weinmann hj , et al : physiol chem phys med nmr 16 : 167 - 172 , 1984 ; priest an , et al : magn reson med 63 : 1044 - 1049 , 2010 )  . gaussian smoothing was applied to all raw mr images before processing with variance of half a voxel , to smooth the parameters . 
for voxels that had estimated parameters that exceeded the bounds set by the tting curve , the values were set to nan ( not - a - number )  . 
once all voxels were tted , the voxels with nan value were replaced by an average of the surrounding voxels so that each voxel had an estimated parameter for the purpose of clustering . the standardized uptake values ( suv ) of the voxels contained within each lesion on 18f - uorodeoxyglucose pet was calculated based on the standard expression given by kinahan et al ( kinahan pe , et al : transl oncol 2 : 223 - 230 , 2009 )  . three - dimensional printing methodology . 
custom made threedimensional ( 3d ) molds were printed based on manual segmentation of the ovarian primary tumor and metastatic implants on the preoperative axial t2 - weighted mr images . 
the 3d model was then compared with the mr images and manually adjusted to resolve any discrepancies using meshlab ( meshlab , visual computing labisti - cnr ) , an extensible mesh processing system , aimed at editing and rendering unstructured 3d triangular meshes . 
the nal 3d models of each lesion were imported into openscad ( openscad , the openscad developers ) , 3d cad modeling software , which was used to create an internal cavity that exactly shaped each lesion according to the mri shape and contour . 
the slits for slicing each lesion were designed into the molds at 5 - mm intervals , which corresponded to the slice thickness and locations of the axial t2w fast relaxation fast spin echo mr images . 
 graft - versus - host diseasefree antitumoral signature after allogeneic donor lymphocyte injection identied by proteomics and systems biology xiaowen liu , phd1 , 2 ; zongliang yue , ms3 ; yimou cao , ms1 ; lauren taylor , md2 ; qing zhang , ms4 ; sung w . 
chen , phd3 ; huanmei wu , phd1 ; and sophie paczesny , md , phd2 purpose as a tumor immunotherapy , allogeneic hematopoietic cell transplantation with subsequent donor lymphocyte injection ( dli ) aims to induce the graft - versus - tumor ( gvt ) effect but often also leads to acute graftversus - host disease ( gvhd )  . 
our novel six - step systems biology analysis involved removing common proteins and gvhd - specic proteins , creating a protein - protein interaction network , calculating relevance and penalty scores , and visualizing candidate biomarkers in gene networks . 
we then performed a second proteomics experiment in a validation set of patients who experienced gvt without acute gvhd after dli for comparison with the proteome of patients before dli . 
an independent experiment with single - cell proling in tumor antigenactivated t cells from a patient with posthematopoietic cell transplantation relapse was performed . results the approach provided a list of 46 proteins in the training set , and 30 proteins in the validation set were associated with gvt without gvhd . 
finally , the single - cell proling in activated t cells found 43 of the 61 genes . novel markers , such as rpl23 , ilf2 , cd58 , and crtam , were identied and could be extended to other antitumoral responses . conclusion our multiomic analysis provides , to our knowledge , the rst human plasma signature for gvt without gvhd . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction allogeneic hematopoietic cell transplantation ( hct ) is one of the most effective forms of tumor immunotherapy available to date . 
the lymphocytes in the donor graft recognize and eliminate residual tumoral cells through the graft - versus - tumor ( gvt ) effect , and thus , donor lymphocyte injection ( dli ) often is used at the time of relapse post - hct to induce gvt . 
despite the correlation of gvt indirect evidence for a gvt reaction and gvhd , separate from gvhd has been reported in large cohorts of hct patients or when dli is administered to induce remission in hct patients who have experienced a relapse.1 , 2 gvt activity can be increased by targeted therapy , as has been shown with sorafenib in flt3 internal tandem duplicationmutant leukemia cells.3 the gvt effect is mediated by minor histocompatibility antigens ( mihags ) on recipient leukemic cells that are recognized by donor cd4 + and cd8 + t cells.4 mihags can mediate gvt without inducing gvhd if they are only expressed by the recipient hematopoietic cells ( ie , minor h antigen [ ha ] - 1 , ha - 2 , bcl2a1 , and hb - 1 ) .5 , 6 nonhistocompatibility antigen proteins expressed by tumor cells , called tumor - associated antigens ( survivin , wilms tumor 1 , proteinase 3 ) also can mediate gvt activity.7 cytokines ( ie , interleukin - 15 [ il - 15 ] ) 3 ; checkpoint proteins , such as pd - 1 / pd - l18 ; and t - cell trafcking modulators9 are other possible mediators of gvt . our study aim was to develop a proteomic signature to identify gvt without gvhd after allogeneic dli . 
we attempted to do so through plasma proteomics and systems biology analyses of patients in relapse after hct who received donor lymphocytes as immunotherapy . knowledge generated our novel six - step systems biology analysis involved the removal of common proteins and gvhd - specic proteins , creation of a protein - protein interaction network , calculation of relevance and penalty scores , and visualization of candidate biomarkers in gene networks to dene a unique , biologically relevant 61 - protein signature of gvhd - free gvt . 
forty - three of the 61 genes also were found in an independent experiment using massive single - cell proling of tumor antigenactivated t cells from a patient who experienced post - hct relapse . relevance this multiomic analysis provides the rst human plasma signature for gvhd - free gvt to our knowledge . 
risk stratication on the basis of the gvt without gvhd protein signature would allow for customized treatment plans after hct . of 61 proteins that are signicantly expressed in the plasma of hct patients who received dli for tumor relapse . 
the methodology for this study is described in the data supplement . results plasma proteomics of gvhd - free gvt in a training set our initial approach to identifying gvt - specic biomarkers was to undertake a proteomics analysis . 
we reasoned that the best setting to observe a gvt effect without any effect of chemotherapy or preparative conditioning regimen would be after dli is given for relapse of malignant disease . 
our rst proteomics experiment ( ipas01 ) was designed to distinguish proteomes that predict gvhd - free gvt from those that predict gvt with gvhd after dli in a training set . 
we compared a pool of plasma samples taken approximately 30 days after dli from ve patients without relapse and without gvhd ( gvt - positive , gvhd - negative ) labeled with the heavy isotope and compared them with a pool of plasma samples at matched time points from 11 patients without relapse but with concomitant gvhd ( gvt - positive , gvhd - positive ) labeled with the light isotope ( fig 1 )  . 
no signicant differences between groups were observed for patient age , disease status ( all but one with morphologic relapse , and only one patient did not receive chemotherapy ) , dli donor type , and dli dose , and all patients were off immunosuppression . 
 gvhd - free antitumoral signature after donor lymphocyte injection gvt - positive , and gvhd - positive post - dli ( ipas - 01 ) gvt - positive , and gvhd - negative pre - dli ( ipas - 02 ) gvt - positive , and gvhd - negative post - dli ( ipas - 01 and - 02 ) isotopic labeling light isotopic labeling heavy immunodepletion six most abundant proteins acrylamide alkylation samples mixed fig 1 . 
the intact - protein analysis system ( ipas ) compared graft - versus ( gvt ) positive and graft - versus - host disease tumor ( gvhd ) negative postdonor lymphocyte injection ( dli ; heavy isotope ) with gvt - positive and gvhd - positive postdli ( light isotope ) samples in a training set ( ipas - 01 ) , and gvt - positive and gvhd - negative post - dli ( heavy isotope ) with gvt - positive and gvhd - negative pre - dli ( light isotope ) samples in a validation set ( ipas - 02 )  . anion - exchange chromatography ( n = 8 ) reversed - phase chromatography ( n = 60 ) liquid chromatography - ms / ms software tool ( data supplement )  . 
after this data processing , the ipas - 01 experiment provided a list of 46 proteins associated with a gvt signature without gvhd post - dli in the training set ( table 1 )  . 
although we started with ipas proteins with a heavy / light ratio greater than 1.2 , the systems biology process may have resulted in a nal score of less than 1 ; however , because all these proteins are gvt specic , they all are included in the nal gvhd - free gvt signature . 
the rst node is centered around cd8 ( cd8a ) and includes cd58 , il1a , ly75 , fas , and gpnmb and a secondary node centered around raf1 and containing guk1 , ephb4 , and cxcl12 . 
our data with the cd8a - centered node strongly suggest that gvt is majorly mediated by cd8 t cells and gvhd less so , which provides an opportunity to separate gvt and gvhd by manipulating these two t - cell subsets differently . 
as a proof of concept , we performed the experiment without applying these proteins to show that their nal scores have not been signicantly changed by the use of penalty scores ( table 1 ; data supplement )  . plasma proteomics of gvhd - free gvt in a validation set our second proteomics experiment ( ipas - 02 ) used a validation set that was designed to compare a pool of samples from ve gvt - positive , gvhd - negative ( labeled with the heavy isotope ) patients with a pool of samples from the same patients taken before dli when the patients were in relapse and thus gvt negative ( labeled with the light isotope ; fig 1 )  . 
a major cluster is constituted by centromere protein m ( cenpm ) , nup160 , wapal , dhx37 , stx7 , and il enhancer binding factor 2 ( ilf2 ) , which are all proteins implicated in the activation of cytotoxic t cells consistent with a gvt response ( table 2 )  . 
for example , cenpm ( also called pane1 ) is a known mihag expressed on b - lymphoid cells that is highly relevant to gvt - mediated post - dli.12 the protein encoded by ilf2 is a transcription factor needed for t - cell expression of il - 2.13 the second cluster is similar to the one found in ipas - 01 centered on map3k6 and dbnl . final 61 - protein gvhd - free gvt signature after dli the next step was to combine the proteins found in the training and validation sets . 
combined analysis of the two ipas experiments yielded 61 proteins : 49 with a nal combined score of greater than 1 and 12 with a nal combined score of less than 1 , all specic to gvt without gvhd ( table 1 )  . 
these include one similar to that seen in ipas - 01 centered on cd8a , one similar to that seen in ipas - 02 centered on cenpm - wapal and also containing dhx37 , and one found in both experiments and centered on map3k6 and dbnl . 
this additional cluster is centered around cse1l , which is a ras - related nuclear protein with a potential role in ras / raf / mapk signaling in t cells . 
some potential important novel markers , such as cytotoxic and regulatory t - cell molecule ( crtam ) , which has been shown to determine the cd4 + cytotoxic t - lymphocyte lineage , 14 are not part of a cluster . 
 ( a ) intact - protein analysis system ( ipas ) - 01 : geneterrain visualization shown in 2d for the graftversus - tumor ( gvt ) signature obtained by comparing gvt - positive , graft - versus - host disease ( gvhd ) negative with gvt - positive , gvhd - positive postdonor lymphocyte injection ( dli ) samples . 
a mean reads number of 381 , 079 per cell and median gene number of 1 , 091 per cell were analyzed for an average of 1 , 436 cells per condition . 
among the 61 genes identied in the proteomic gvhd - free gvt signature , 11 were more highly expressed in prame - specic t cells compared with cmvspecic t cells or nonreactive t cells . 
the expression prole of four representative gvt markers in the single - cell rna sequencing analysis of prame - specic t cells ( rpl23 , ilf2 , cd58 , and crtam ) is shown in figure 3 . 
rpl23 is a component of the 60s ribosomal subunit and has been shown to link the oncogenic ras signaling to p53 - mediated tumor suppression.15 t - cell responses to rpl23 also are increased in autoimmune diseases , 16 which suggests a role for the ras / raf / mapk pathway in t cells that is currently underexplored . 
the cd58 / cd2 axis is the primary costimulatory pathway for cd8 + t cells that lack cd28 , which suggests an alternate activation mechanism during gvt for exhausted t cells.17 crtam is upregulated in cd4 + and cd8 + t cells and encodes a type 1 transmembrane protein with v and c1 - like immunoglobulin domains.18 it has been shown to negatively regulate zeb1 ( zinc nger e - boxbinding homeobox 1 ) in t cells19 and to determine the cd4 + cytotoxic t - lymphocyte lineage , 14 and it might determine the cd8 + cytotoxic t - lymphocyte lineage as well . 
expression prole of four representative graft - versus - tumor ( gvt ) markers in single - cell rna sequencing analysis of prameand cytomegalovirus ( cmv ) pp65specic t cells . 
one systems biology novelty of our approach was the performance of a one - layer extension on ppi data using interactions one node away from the gene in the original list that are called outer genes . 
a strength of our approach is that we ltered out nonrelevant proteins using a penalty score , which led to a more - specic list of candidate proteins and avoided contaminants . 
this study favored a large - scale proteomics approach as opposed to a hypothesis - driven candidate approach.21 we have shown that for gvhd markers , this method is efcient in discovering new candidate markers.10 , 11 compared with our previous studies , we experimentally removed the gvhd proteins by assigning them the light isotope . 
of note , this approach showed that the proteins identied and their ratio have not been inuenced much by the implementation of penalty scores . in an independent experiment with single - cell proling of t cells from a patient with relapse after hct that were activated in vitro , 43 of the 61 proteomic genes also were found in activated t cells , which suggests that the proteins identied are biologically relevant in different antitumoral responses . the biology of the gvt markers not yet described is as follows . 
the function of trpc4ap ( transient receptor potential cation channel subfamily c member 4associated protein ) has been shown to be involved in the ubiquitination of e3 ligase skp222 and the activation of c - jun nh ( 2 ) terminal kinase and transcription factor ap - 1.23 guanylate kinase 1 ( guk1 ) is an enzyme that catalyzes the transfer of a phosphate group from atp to guanosine monophosphate ( gmp ) to form guanosine diphosphate ( gdp ) and is believed to be a good target for cancer chemotherapy.24 its expression on tumor - specic t cells was not previously reported . 
pin1 ( peptidylprolyl cis / trans isomerase , nimainteracting 1 ) catalyzes the cis / trans isomerization of peptidyl - prolyl peptide bonds and thus catalytically regulates the postphosphorylation conformation of its substrates and is involved in the regulation of t - cell biology . 
in particular , its implication has been shown in systemic lupus erythematosus and t - cell acute lymphoblastic leukemia progression.25 - 27 wapl cohesin release factor has been shown to restrict chromatin loop extension.28 of note , it was part of a microrna - mrna network in allogeneic t - cell responses.29 fermitin family member 3 ( fermt3 ) a member of the kindlins that mediates ppi involved in integrin activation . 
mutations in this gene cause the auadhesion deciency tosomal leukocyte syndrome - 3.30 its role in t cells has not been studied . cd160 is another surface protein tightly expressed on peripheral cytotoxic cd8 t lymphocytes and natural killer cells , 31 and soluble cd160 enhances cd8 + t cells , which results in increased interferon - , il - 2 , and tumor necrosis recessive factorsecretion as well as cytolysis against tumor cells in vitro and in vivo.32 not surprisingly , serglycin ( srgn ) , which serves as a mediator of granule - mediated apoptosis through the macromolecular complex of granzymes and perforin and determines the secretory granule repertoire of cytotoxic t lymphocytes , 33 was also upregulated in this study . 
the fas cell surface death receptor ( fas ) that plays a critical role in the activation of the death - inducing signaling complex with fas - associated death domain protein and triggers a downstream caspase cascade that leads to apoptosis34 also was upregulated . the chemokine cxcl12 has been proposed to be able to distinguish immune cells that induce gvt going to the bone marrow from immune cells that induce gvhd.35 it is one of the rare proteins for which the nal score was modied more than twice by the penalty score but is still included overall as a gvt proteseveral of the tripartite motif ( trim ) members encode for mihags.21 although trim42 , 22 , and 37 are located on chromosomes 3 , 11 , and 17 , respectively , trim39 is on chromosome 6 in the major histocompatability class i region and , in our study , showed global expression on activated t cells . 
raf1 is the cellular homolog of viral raf proto - oncogene ( v - raf ) and is also a map3k that functions downstream of the ras family of membrane - associated gtpases to which it binds directly . 
cse1l is a ras - related nuclear protein that binds strongly to nuclear localization signal - free importin - , and this complex is then released in the cytoplasm by the combined action of ranbp1 and rangap1 . 
one particular protein of nont - cell origin , il - 1 , was found to be elevated in the plasma of patients with gvt response and may play a signicant role in antitumor effects . 
of note , il - 1engineered tumor cells rarely develop into tumors , and if they do , the tumors are quickly destroyed through a mechanism that involves cd8 + t cells and natural killer cells , and il - 1 tumor immunoediting microenvironment.36 although our approach identied several proteins for gvhd - free gvt , there are limitations in this study . 
third , the systems biology pipeline relies on knowledge from the published domain , which makes the application of this method to diseases that have not been well studied , such as gvt , difcult . 
chen travel , accommodations , expenses : wuxi apptec sophie paczesny patents , royalties , other intellectual property : inventor on a patent entitled methods of detection of graft - versus - host disease ( us 20130115232a1 , wo 2013066369a3 ) no other potential conicts of interest were reported . acknowledgment the raw mass spectrometry data are publicly available at massive ( massive.ucsd.edu ) with the identication number msv000081057 . 
we thank gregory yanik , md , for providing the patient samples through a university of michigan - indiana university material transfer agreement . references ringd en o , labopin m , gorin nc , et al : is there a graft - versus - leukaemia effect in the absence of graft - versus - host disease in patients undergoing bone marrow transplantation for acute leukaemia ? br j haematol 111 : 1130 - 1137 , 2000 bar m , sandmaier bm , inamoto y , et al : donor lymphocyte infusion for relapsed hematological malignancies after allogeneic hematopoietic cell transplantation : prognostic relevance of the initial cd3 + t cell dose . 
mathew nr , baumgartner f , braun l , et al : sorafenib promotes graft - versus - leukemia activity in mice and humans through il - 15 production in flt3 - itdmutant leukemia cells . 
blood 91 : 2197 - 2207 , 1998 bleakley m , otterud be , richardt jl , et al : leukemia - associated minor histocompatibility antigen discovery using t - cell clones isolated by in vitro stimulation of naive cd8 + t cells . 
blood 115 : 4923 - 4933 , 2010 dossa rg , cunningham t , sommermeyer d , et al : development of t - cell immunotherapy for hematopoietic stem cell transplantation recipients at risk of leukemia relapse . 
leuk lymphoma 45 : 2229 - 2237 , 2004 koestner w , hapke m , herbst j , et al : pd - l1 blockade effectively restores strong graft - versus - leukemia effects without graft - versus - host disease after delayed adoptive transfer of t - cell receptor gene - engineered allogeneic cd8 + t cells . 
blood 117 : 1030 - 1041 , 2011 kim ym , sachs t , asavaroengchai w , et al : graft - versus - host disease can be separated from graft - versus - lymphoma effects by control of lymphocyte trafcking with fty720 . 
vander lugt mt , braun tm , hanash s , et al : st2 as a marker for risk of therapy - resistant graft - versus - host disease and death . 
brickner ag , evans am , mito jk , et al : the pane1 gene encodes a novel human minor histocompatibility antigen that is selectively expressed in b - lymphoid 13 . 
kao pn , chen l , brock g , et al : cloning and expression of cyclosporin aand fk506 - sensitive nuclear factor of activated t - cells : nf45 and nf90 . 
cancer res 76 : 5030 - 5039 , 2016 ito y , hashimoto m , hirota k , et al : detection of t cell responses to a ubiquitous cellular protein in autoimmune disease . 
leitner j , herndler - brandstetter d , zlabinger gj , et al : cd58 / cd2 is the primary costimulatory pathway in human cd28 - cd8 + t cells . 
yeh jh , sidhu ss , chan ac : regulation of a late phase of t cell polarity and effector functions by crtacell 132 : 846 - 859 , 2008 19 . 
bachireddy p , hainz u , rooney m , et al : reversal of in situ t - cell exhaustion during effective human antileukemia responses to donor lymphocyte infusion . blood 123 : 1412 - 1421 , 2014 21 . 
tissue antigens 81 : 183 - 193 , 2013 jamal a , swarnalatha m , sultana s , et al : the g1 phase e3 ubiquitin ligase truss that gets deregulated in human cancers is a novel substrate of the s - phase e3 ubiquitin ligase skp2 . 
soond sm , terry jl , riches dw : truss , a tumor necrosis factor receptor - 1 - interacting protein , activates c - jun nh ( 2 ) - terminal kinase and transcription factor ap - 1 . 
ruppert r , moser m , sperandio m , et al : kindlin - 3 - mediated integrin adhesion is dispensable for quiescent but essential for activated hematopoietic stem cells . j exp med 212 : 1415 - 1432 , 2015 31 . 
kotsiou e , davies jk : new ways to separate graft - versus - host disease and graft - versus - tumour effects after allogeneic haematopoietic stem cell transplantation . br j haematol 160 : 133 - 145 , 2013 36 . 
 o integrative molecular analysis of patients with advanced and metastatic cancer verena sailer , md1 ; kenneth wa eng , ms1 ; tuo zhang , phd1 ; rohan bareja , ms1 ; david j . 
pisapia , md1 ; alexandros sigaras , ms1 ; bhavneet bhinder , ms1 ; alessandro romanel , phd2 ; david wilkes , phd1 ; evan sticca , ms1 ; joanna cyrta , md1 ; rema rao , md1 ; sheena sahota , md1 ; chantal pauli , md1 ; shaham beg , md1 ; samaneh motanagh , md1 ; myriam kossai , md1 ; jacqueline fontugne , md1 ; loredana puca , phd1 ; hanna rennert , phd1 ; jenny zhaoying xiang , md1 ; noah greco , mba1 ; rob kim1 ; theresa y . 
in patients with more than one sequenced tumor sample ( n = 146 ) , 84.62% of actionable mutations were concordant . conclusion integrative analysis may uncover informative alterations for an advanced pan - cancer patient population . 
2019 by american society of clinical oncology introduction genomic proling is widely used in cancer care to identify actionable alterations for individual patients within the context of precision medicine ( pm ) .1 however , only 2% to 11% of those patients with sequencing performed receive a genomically matched therapy , which may be a result of the availability and accessibility of clinical trials , 2 - 6 patient factors and comorbidities , disease state or alternative options , or patient preference.5 despite these drawbacks , pm studies continue to provide insights into the molecular underpinnings of cancer . 
we and others have shown that performing whole - exome sequencing ( wes ) and rna sequencing is feasible in a clinical setting and may provide relevant information beyond targeted gene panels in certain settings.3 , 7 , 8 sequencing matched tumor and normal ( germline ) dna has the additional benet of uncovering unforeseen hereditary conditions , including cancer risk mutations . 
in particular , germline dna repair defects ( drds ) are more common than previously anticipated across adult advanced cancer populations.9 - 11 robinson et al12 published their met500 cohort with wes and rna sequencing data from 500 patients with metastatic disease of varied tumor primary and biopsy sites . 
our study , obtained from our own cohort of 759 samples from 515 patients with advanced and metastatic cancer , complements this data set as it adds wes data from approximately the same number of patients . 
 sailer et al context key objective we assessed whether developing a multidimensional precision oncology program is feasible and informative for patients with cancer with advanced disease . knowledge generated we established a comprehensive clinical genomics program for this patient group . 
the rate of clinically relevant alterations across 515 patients with advanced solid tumors was 39% by whole - exome sequencing , which was improved by 16% by adding rna sequencing . 
germline dna was obtained from blood samples ( circulating mononuclear cells ) , buccal swabs , or benign tissue as described previously.3 part of the data presented in this manuscript have already been published.3 , 13 , 15 wes was performed on each patients tumor / matched germline dna pair using previously described protocols.3 we used a clinical - grade wes testexome cancer test version 1approved by new york state department of health ( id# 43032 ) and described in detail in rennert et al.16 this approach allows for assessment of more than 21 , 000 genes through the development and implementation of computational approaches for tumor mutational burden and neoepitope analysis , as well as integration with other data , including rna sequencing , to improve the identication of clinically relevant and actionable alterations . 
to evaluate the concordance of tier 1 and tier 2 alterations between multiple samples from the same patient and to gain high - delity results , a cutoff of 20% for variant allele frequency was used . 
in addition , we developed patientderived organoids from fresh tissues using previously described protocols , 4 , 17 and we used cell lines to functionally validate outlier targetable alterations . wes alterations were categorized on the basis of on their actionability and clinical or biologic relevance.3 alterations in 49 actionable or clinically signicant genes were reported within category 1 , alterations in 508 known cancer - associated genes within category 2 , and somatic alterations of unknown signicance within category 3.3 we developed an open - access , dynamic , web - based pm knowledge base as an interactive online tool where variants are carefully interpreted in the context of tumor type.18 wes results were conveyed to the referring physician in the form of an exome cancer test version 1 report.3 selected cases are presented at a regular , continuing medical education accredited pm tumor board , which discusses sequencing results in the context of a patients history , available literature , and treatment options , including active clinical trials . pathogenic germline ndings were reported to the referring physician if they occurred in any of the genes deemed reportable by the american college of medical genetics and genomics ( acmg ) , 19 and these patients were referred for genetic counseling and results were conrmed by targeted testing in a clinical laboratory improvement amendments / clinical laboratory evaluation programcertied laboratory . study cohort demographic data were obtained through electronic health record search . 
 precision oncology for patients with advanced disease primary site ( 515 patients ) biopsy / resection site ( 759 samples ) breast ( 13 ) pancreas ( 18 ) kidney ( 46 ) soft tissue ( 8 ) brain ( 98 ) lung ( 16 ) hematologic malignancies ( 24 ) colon and / or rectum ( 41 ) bladder ( 57 ) prostate ( 105 ) primary recurrent metastatic brain ( 150 ) liver ( 64 ) bla d d er ( 69 ) b o n e ( 71 ) ly m p h n o d e ( 85 ) c olo n ( 18 ) l u n g ( 44 ) kid n ey ( 26 ) prostate ( 33 ) sample characteristic metastatic primary recurrent 34 - year - old female , er - positive breast carcinoma , mastectomy , brca1 / 2 germline negative chest wall recurrence , er / pr / her2 unknown , excision and radiotherapy no cancer detected metastatic disease seven systemic therapies precision medicine consent liver biopsy , akt1 mutation detected by wes cdk4 / 6 inhibitor ( palbociclib ) liver progress + 3 years + 20 years + 3 years + 1 year + 1 year + 1 year fig 1 . 
the most common somatic alterations were found in tp53 ( 33% ) , cdkn2a ( 11% ) , apc ( 10% ) , kmt2d ( 8% ) , pten ( 8% ) , and brca2 ( 7% ; fig 2 )  . multiple samples three hundred eighty - two spatially and temporally heterogeneous samples from 146 patients underwent wes . 
of these , 185 ( 48.4% ) were metastatic , 153 ( 40.1% ) were primary , and 44 ( 11.5% ) were recurrent tumor samples . most samples were paired primary and metastatic tumors , and concordance of alterations between primary and metastatic samples in clinically informative genes is shown in figure 3 . 
paired primarymetastatic tumor samples from 59 patients were the most frequent combination . spatially and / or temporally heterogeneous metastases and primary tumors from 35 and 29 patients , respectively , also underwent sequencing . 
 ( e ) different kras mutations in two morphologically similar lung cancer samples from the same patient , thus conrming two separate primary tumors . this cohort ( data supplement )  . 
the most frequently mutated genes were chek2 ( 11 patients ) , brca2 ( nine patients ) , brca1 ( nine patients ) , msh6 ( nine patients ) , and atm ( four patients ; fig 2 )  . 
in likely pathogenic variants in 38 addition , 44 additional patients in msh6 ( 14 cases ) ; apc ( seven cases ) ; chek2 ( ve cases ) ; pole , pms2 , msh2 brca1 , and atm ( three cases each ) ; and tp53 , cdh1 , and brip1 ( one case each ) were discovered in our cohort . the prevalence of drd in our cohort of patients with metastatic prostate cancer was 14.3% , with brca2 mutations being the most frequent variants ( data supplement )  . pathogenic germline drds were found in 9.2% of patients with primary brain tumors . 
we did not identify pathogenic mutations involving mismatch repair genes , which have been described in primary brain tumor patients , in particular as biallelic losses.25 chek2 was altered in four cases , including one medulloblastoma . 
 ( b ) high frequency of germline mutations in breast , prostate , and lung tumors is observed . germline drd defects , 12 had received platinum - based chemotherapy with follow - up available . 
an additional targetable ncoa4ret fusion , which has been described in papillary thyroid cancer , nonsmall - cell lung cancer , and colorectal cancer , was found in a brain metastasis of a patient with unknown primary.28 rna sequencing rna sequencing was performed when sufcient fresh frozen tumor tissue was available after wes . 
of these 89 patients , 50 did not harbor a targetable genomic alteration identied by wes , resulting in an increase in the rate of actionable alteration detection of approximately 15% . 
we conrmed the drug sensitivity of select outlier genes using cell line experiments compared with randomly selected drugs ( fig 5 )  . nine novel fusions in a variety of cancer types were detected . 
a novel rbm47 - cdk12 gene fusion was found in a prostate cancer bone metastasis , which was conrmed organoids part of the program was the development of patient - derived organoids from patient biopsies for high - throughput drug screening.4 altogether 60 organoids were developed from 98 patients with an overall success rate of 61% . 
a pathogenic msh6 mutation was detected in a 26 - year - old patient with metastatic breast carcinoma who had undergone previous outside testing for brca1 / 2 germline mutations with a negative result . 
other potentially signicant variants in drd genes , such as palb2 , would have been missed as well.30 this case underlines the importance of multigene panel or wes testing in patients not only with suspected hereditary cancer but also in those , especially young patients , with metastatic disease to detect underrecognized germline alterations.31 tumor evolution and clonality . 
a deleterious effect has been predicted for this variant.33 in a previously published analysis of 13 uterine carcinosarcomas analyzed by targeted sequencing , eight cases demonstrated 100% identical mutations in both the carcinoma and sarcoma part.34 in contrast , we observed an early divergence with only the one pten mutation of 54 nonsynonymous shared mutations . 
this case again demonstrates the importance of using next - generation sequencing to correctly identify synchronous primary tumors.39 another patient with metastatic neuroblastoma was conrmed to have an activating alk mutation ( r1275q ) in both primary tumor and bone marrow metastasis . 
the patient has had stable disease for 13 months on therapy with sequential alk inhibitors40 ( fig 3 )  . discussion we have established a pm program for patients with advanced cancer using tumor / normal wes and integrative molecular proling to detect genomic and other actionable alterations , improve clinical decision making , and study tumor evolution in a pan - cancer cohort . 
the patient population in our study is distinct from several reported studies in that our focus was on the evaluation of advanced tumors.41 , 42 the majority of patients ( 70.8% ) presented the time of with metastatic or recurrent disease at enrollment . whereas publicly accessible molecular data for several tumor types are available , both for primary and metastatic cancers , 43 , 44 these specimens are rarely matchedthat is , obtained from the same patient.45 our cohort of patients with locally advanced and metastatic cancer allowed for the collection of multiple matched , often primary and metastatic samples , resulting in a unique feature of this cohort : genomic data from spatially and / or temporally heterogeneous , matched tissue samples were available in 146 patients . 
of clinical importance is the nding that almost 85% of category 1 alterations were shared between multiple samples from the same patient . these results are in concordance with published data in specic cancer types . 
in one study , when comparing actionable mutations between presurgery biopsies and resected specimen in patients with nonsmall - cell lung cancer , the concordance rate was found to be 79%.46 similar ndings have been reported for primary and recurrent breast cancer , with 86.6% of mutations and 85.5% of scnas being concordant.47 our data conrm that it may reasonable to select the most accessible location or even archival material from the primary tumor for molecular analysis for certain cancer types.48 , 49 new research indicates that pathogenic germline mutations are more frequently found in patients with advanced cancer , 9 , 12 and our data conrm this . 
germline mutations that involve the dna repair pathway , found in 10.7% of our patients , are predictive of response to parp inhibitors and platinum - based therapy and have important familial plications for cancer screening.50 family history was indicative of a heritable component in only one half of these patients . 
this fusion might result in the loss of cdk12 activity , which has recently been described to delineate a distinct immunogenic subtype of metastatic castrationresistant prostate cancer.51 in our study , wes was prioritized over rna sequencing whenever tissue availability was of concern . 
biopsies in our study were usually performed for diagnostic purposes in the context of clinical care , hence the lower availability of fresh frozen tissue for additional rna sequencing . targeted sequencing of cancer - related genes offers several advantages over wes , including deeper coverage , quicker turnaround time , lower cost , and fewer requirements for an elaborate computational pipeline . 
here , we show that wes and rna sequencing may provide an additional and information in certain settings , complimentary layer of particularly for patients with advanced cancer who experience progression after standard therapies . 
wes also considers the rapidly expanding spectrum of actionable alterations , including alterations for which targeted treatment may not be available at the time of analysis , but for which clinical trials might be planned . 
in addition , whereas targeted nextgeneration sequencing testing of somatic dna are sometimes ordered as part of clinical care , using germline dna as normal control for wes necessitates securing informed consent . implementing - omic data into clinical care requires an interdisciplinary teagenomic data and its interpretation in the context of tumor type and primary site must be easily accessible to enable clinicians to integrate the data into everyday patient care . 
 precision oncology for patients with advanced disease one limitation of our study is the lack of uniformity of the cohort in terms of tumor type and therapy , which prevents us from making generalized statements about treatment response . 
this data set also reports on a large number of matched temporally and spatially heterogeneous samples , highlighting the concordance of actionable alterations in different samples . as other pm trials have shown , uncovering genomic alterations may not be sufcient in identifying actionable alterations . 
contributed equally to this work and share senior authorship . support supported by the englander institute for precision medicine of weill cornell medicine and new york presbyterian , the translational research program of the department of pathology and laboratory medicine at weill cornell medicine . 
macdonald , eleni andreopoulou , olivier elemento , himisha beltran provision of study materials or patients : noah greco , rob kim , bishoy m . faltas , eleni andreopoulou , linda t . 
pisapia , david wilkes , joanna cyrta , sheena sahota , chantal pauli , shaham beg , samaneh motanagh , myriam kossai , jacqueline fontugne , jenny zhaoying xiang , noah greco , rob kim , theresa y . 
pisapia , alexandros sigaras , bhavneet bhinder , alessandro romanel , david wilkes , evan sticca , rema rao , shaham beg , loredana puca , rob kim , mirjam blattner - johnson , eleni andreopoulou , linda t . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . alexandros sigaras employment : weill cornell medical college loredana puca employment : petra pharma corporation bishoy m . 
faltas honoraria : digital science press publications research funding : eli lilly david rickman research funding : janssen oncology eleni andreopoulou honoraria : astrazeneca , sirtex , svb leerink , abbvie , eisai , nanostring technologies consulting or advisory role : astrazeneca , sirtex , svb leerink , abbvie , eisai , nanostring technologies speakers bureau : r - pharm us travel , accommodations , expenses : astrazeneca , sirtex , svb leerink , abbvie , eisai , nanostring technologies kevin holcomb research funding : fujirebio diagnostics expert testimony : johnson & johnson linda t . 
vahdat honoraria : polyphor , r - pharm , athenex , seattle genetics , osmol therapeutics consulting or advisory role : berg pharma speakers bureau : eisai research funding : polyphor ( inst ) , immunomedics ( inst ) , seattle genetics ( inst ) patents , royalties , other intellectual property : patent pending on the application for bmd progenitor cells ( inst ) douglas s . 
 sailer et al koen van besien stock and other ownership interests : hemogenyx consulting or advisory role : hemogenyx , actinium pharmaceuticals , cellectis , tessa therapeutics research funding : miltenyi biotec , actinium pharmaceuticals , juno therapeutics , fate therapeutics christopher e . 
ocean consulting or advisory role : celgene , tyme speakers bureau : daiichi sankyo travel , accommodations , expenses : daiichi sankyo ana molina honoraria : american society of clinical oncology consulting or advisory role : eisai , exelixis , novartis , janssen oncology manish a . 
shah consulting or advisory role : astellas pharma , eli lilly research funding : gilead sciences ( inst ) , merck ( inst ) , boston biomedical ( inst ) , oncolys biopharma ( inst ) , bristol - myers squibb ( inst ) david m . 
nanus consulting or advisory role : genentech research funding : novartis ( inst ) , boehringer ingelheim ( inst ) , zenith epigenetics ( inst ) qiulu pan employment : caris life sciences stock and other ownership interests : caris life sciences francesca demichelis patents , royalties , other intellectual property : co - inventor on a patent led by the university of michigan and brigham and womens hospital covering the diagnostic and therapeutic elds for ets fusions in prostate cancer , diagnostic eld licensed to gen - probe scott t . 
tagawa consulting or advisory role : medivation , astellas pharma , dendreon , janssen oncology , bayer , genentech , endocyte , immunomedics , karyopharm therapeutics , abbvie , tolmar , qed , amgen , sano , pzer research funding : eli lilly ( inst ) , sano ( inst ) , janssen oncology ( inst ) , astellas pharma ( inst ) , progenics ( inst ) , millennium pharmaceuticals ( inst ) , amgen ( inst ) , bristol - myers squibb ( inst ) , dendreon ( inst ) , rexahn pharmaceuticals ( inst ) , bayer ( inst ) , genentech ( inst ) , newlink genetics ( inst ) , inovio pharmaceuticals ( inst ) , astrazeneca ( inst ) , immunomedics ( inst ) , novartis ( inst ) , aveo ( inst ) , boehringer ingelheim ( inst ) , merck ( inst ) , stem centrx ( inst ) , karyopharm therapeutics ( inst ) , abbvie ( inst ) , medivation ( inst ) , endocyte ( inst ) , exelixis ( inst ) , clovis oncology ( inst ) travel , accommodations , expenses : sano , immunomedics , amgen wei song employment : genentech ( i ) , cytokinetics ( i ) honoraria : foundation medicine , loxo consulting or advisory role : foundation medicine , loxo juan miguel mosquera research funding : personal genome diagnostics travel , accommodations , expenses : personal genome diagnostics mark a . 
nature 537 : s63 , 2016 beltran h , eng k , mosquera jm , et al : whole - exome sequencing of metastatic cancer and biomarkers of treatment response . 
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 impact of the spop mutant subtype on the interpretation of clinical parameters in prostate cancer purpose molecular characterization of prostate cancer , including the cancer genome atlas , has revealed distinct subtypes with underlying genomic alterations . 
one of these core subtypes , spop ( speckle - type poz protein ) mutant prostate cancer , has previously only been identifiable via dna sequencing , which has made the impact on prognosis and routinely used risk stratification parameters unclear . methods we have developed a novel gene expression signature , classifier ( subclass predictor based on transcriptional data ) , and decision tree to predict the spop mutant subclass from rna gene expression data and classify common prostate cancer molecular subtypes . 
we then validated and further interrogated the association of prostate cancer molecular subtypes with pathologic and clinical outcomes in retrospective and prospective cohorts of 8 , 158 patients . results the subclass predictor based on transcriptional data model showed high sensitivity and specificity in multiple cohorts across both rna sequencing and microarray gene expression platforms . 
we found that the spop mutant subclass was associated with lower frequency of positive margins , extraprostatic extension , and seminal vesicle invasion at prostatectomy ; however , spop mutant cancers were associated with higher pretreatment serum prostate - specific antigen ( psa )  . 
despite high pretreatment psa , the spop mutant subtype was associated with a favorable prognosis with improved metastasis - free survival , particularly in patients with high - risk preoperative psa levels . conclusion using a novel gene expression model and a decision tree algorithm to define prostate cancer molecular subclasses , we found that the spop mutant subclass is associated with higher preoperative psa , less adverse pathologic features , and favorable prognosis . 
2018 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license : introduction prostate cancer is a clinically and molecularly heterogeneous disease.1 - 4 current risk stratification guidelines , such as those from the national comprehensive cancer network , 5 the american urological association / american society for therapeutic radiology and oncology , 6 and the european association of urologyeuropean society for radiotherapyoncologyinternational society of geriatric oncology7 use clinical and pathologic parameters , including the level of prostate - specific antigen ( psa ) , to guide management decisions for clinically localized disease . 
psa is also used in a number of other clinical scenarios in prostate cancer , including initial diagnosis , monitoring for recurrence after primary therapy , and monitoring disease burden and treatment response for metastatic disease . the emerging next - generation dna and rna sequencing data point toward distinct molecular subclasses of prostate cancer , 2 - 4 , 8 , 9 but their clinical impact remains unclear . 
 genome atlas ( tcga ) study identified seven core prostate cancer subtypes , which were defined by underlying genomic alterations.4 one key molecular subclass , which represents approximately 10% of prostate cancers , harbors recurrent missense mutations in the e3 ubiquitin ligase component spop.2 - 4 , 10 - 13 to date , identification of spop mutations has required mutational analysis using genomic ( dna ) sequencing . 
in contrast , gene expression ( rna ) data are widely available from a variety of prostate cancer cohorts , often with the long follow - up necessary to define prognostic impact.14 - 21 here , we reported the first development and validation of the subclass predictor based on transcriptional data ( scapt ) model , which we used to define key prostate cancer molecular subclasses , including spop mutant cancer , using gene expression data . 
we used the scapt model to predict the molecular subclass from a retrospective cohort that included 1 , 626 patient samples and a prospective cohort that included 6 , 532 samples using genome - wide microarray gene expression data from a clinically available prognostic assay ( decipher ; genomedx biosciences , vancouver , bc , canada ) , and we explored the clinicopathologic and prognostic associations of key molecular subclasses of prostate cancer . methods prostate cancer tumor samples and microarray data we used a total of 8 , 559 radical prostatectomy ( rp ) tumor expression profiles for training , testing , and validation . 
for training and testing , we used rna sequencing expression and dna mutation data from tcga prostate cancer project ( n = 333 ) 4 and the weill cornell medicine ( wcm ) sequencing ( n = 68 ) cohort . 
for validation , expression profiles of retrospective ( n = 1 , 626 ) and prospective ( n = 6 , 532 ) cohorts were derived from the decipher genomics resource information database ( grid ) registry ( clinicaltrials.gov identifier : nct02609269 )  . 
 the retrospective grid cohort was pooled from seven published microarray studies : cleveland clinic , 22 erasmus mc , 23 johns hopkins , 15 memorial sloan kettering cancer center , 1 mayo clinic ( mayo i and mayo ii ) , 20 , 24 and thomas jefferson university.21 the prospective grid cohort was from clinical use of the decipher test . 
dna and rna from the tcga and wcm cohorts were extracted from fresh frozen rp tumor tissue , as previously described.4 rna from the grid cohorts was extracted from routine formalin - fixed , paraffin - embedded rp tumor tissues , amplified , and hybridized to human exon 1.0 st microarrays ( thermo fisher scientific , waltham , ma ) .24 , 25 spop mutant transcriptional signature we developed the spop mutant transcriptional signature , which includes 212 genes differentially expressed between spop mutant and wild - type samples from tcga prostate cancer rna sequencing data4 ( fig 1 )  . 
the overlap between two methods was significant ( p < 2.2 1016 ) , which confirmed similar results when applying these methods . scapt development on the basis of spop mutant transcriptional signature and the support vector machine model to predict tumors in the spop mutant subclass in the absence of dna sequencing datathat is , microarray data setswe developed the scapt model on the basis of the support vector machine ( svm ) model.28 - 30 given a set of training data marked with two categories , svm builds a model that assigns testing data into one category or the other , which makes it a nonprobabilistic binary linear classifier ( fig 2a )  . 
 ( a ) spop mutant transcriptional signature that included 212 differentially expressed genes between spop mutant and wild - type samples from the cancer genome atlas ( tcga ) non - ets fusion rna sequencing ( rna - seq ) data . 
 ( b ) significant enrichment of spop mutant case from 68 weill cornell medicine ( wcm ) prostate cancer samples with spop mutant transcriptional signature on the basis of hierarchical clustering . 
erg , erg - fusion position ; ets : other ets fusion positive ; fdr , false - discovery rate . z - scores of spop mutant signature from tcga cohort . 
 by performing 10 - fold cross - validation on the tcga training data set , we found costcost of constraints violationequal to 0.04 to yield the model with the highest sensitivity and specificity . 
next , using a decision tree and previously developed microarray - based classifiers for the erg - positive and ets - positive subtypes , 25 we classified the remaining cases in each cohort . 
high accuracy and confidence of spop mutant ( spopmut ) subclass prediction on weill cornell medicine ( wcm ) and gene expression omnibus ( geo ) data set by the scapt ( subclass predictor based on transcriptional data ) model . 
data from taylor et al , 1 erho et al , 24 and kelin et al.22 wt , wild type . spopwt spopmut support vectors large margin spop other taylor et al ( n = 150 ) erho et al ( n = 545 ) klein et al ( n = 182 ) prediction : spopmut sensitivity , 89% ; specificity , 95% spopwt spop wild type combined cohort to test the statistical association between spop mutant status and clinical variables , including age , race , preoperative psa , gleason score , lymph node invasion , surgical margin status , extracapsular extension , and seminal vesicle invasion . 
we evaluated the associations between spop mutant status and patient outcomes , including biochemical recurrence , metastasis , and prostate cancerspecific mortality , on the basis of kaplan - meier analysis . 
as spop mutations are mutually exclusive with erg and other ets rearrangements , 13 we excluded prostate cancer samples with ets fusions to define spop mutantspecific gene expression effects ( fig 1a )  . 
among those 212 genes , we found that upregulated genes from the spop mutant subgroup were enriched in transport vesicle membrane and oxidoreductase activity , but that there was no significant enriched function in downregulated genes from the spop mutant subgroup ( data supplement )  . 
in this independent cohort , we found significant enrichment ( p < 1.9103 ) of spop mutant tumors in one subcluster based on unsupervised clustering ( fig 1b and data supplement )  . 
we next used the spop mutant transcriptional signature in a locked svm modelthat is , with fixed parameters on the basis of the training step using the tcga cohort ( see methods ) to generate scores for each sample in the wcm cohort . 
the spop mutant prediction and its impacts on clinical and prognostic outcomes from retrospective ( n = 1 , 626 ) and prospective grid ( n = 6 , 532 ) cohorts . 
 ( a ) the pie chart of predicted molecular subclasses from the retrospective cohort with 1 , 626 samples , on the basis of the scapt ( subclass predictor based on transcriptional data ) model and decision tree . 
 ( c ) the pie chart of predicted molecular subclasses from the prospective grid cohort with 6 , 532 samples , on the basis of the scapt model and decision tree . 
erg , erg - fusion position ; ets , other ets fusion positive ; or , odds ratio ; psa , prostate - specific antigen . the grid microarray expression data , which do not have spop mutation annotation from dna analysis . 
between 9% and 15% of samples in the cohorts were predicted as spop mutant subclass , which is consistent with the known prevalence of spop mutations at the genomic level in previous prostate cancer studies3 , 4 , 10 , 12 ( fig 2b )  . 
overall , these results demonstrated that the scapt model predicted spop mutant subclass on the basis of the transcriptional data with high accuracy and confidence . molecular subtyping of 8 , 158 patients using the scapt and decision tree we applied the scapt model and decision tree to 8 , 158 patients from retrospective and prospective grid cohorts . 
among the retrospective cohort with 1 , 626 rp specimens , we predicted 9% ( range , 2% to 13% ) of samples to be spop mutant subclass ( data supplement )  . 
among the prospective cohort with 6 , 532 rp specimens , we predicted 8% of cases to be spop mutant subclass , 41% as erg positive , 12% as ets positive , 39% as other subtype , and 1% as conflict cases ( fig 3c )  . 
 the percentage of each molecular subclass was consistent with that reported in previous prostate cancer studies , 1 - 4 , 14 , 25 which supports the validity of our approach . spop mutant subclass associated with favorable pathology at rp we used binominal univariable analysis to compare clinical and pathologic characteristics between spop mutant and wild - type subclasses ( figs 3b and 3d )  . 
spop mutant subclass was less likely to harbor adverse pathologic features , such as positive surgical margins , extraprostatic extension , and seminal vesicle invasion , compared with wild - type subclass in both retrospective and prospective cohorts ( figs 3b and 3d )  . 
these data suggest that the spop mutant subclass was associated with more favorable pathologic outcomes at rp , but expresses higher levels of psa and was associated with tumors from older men , whereas the opposite was true in the erg - positive subclass of prostate cancer . consistent association between spop mutation and higher psa in multiple cohorts the inverse association of psa and prognosis in specific prostate cancer subtypes has potential clinical implications . 
to independently validate the association of spop mutant status and higher preoperative psa , we examined multiple distinct rp cohorts ( grid , tcga , taylor , and wcm )  . 
we observed a similar trend of higher preoperative psa in spop mutant cases , and the spop mutant subclass was more enriched in the higher psa subgroups ( psa > 10 ; fig 4a )  . 
on univariable analysis across cohorts , spop mutant status was significantly associated with higher preoperative psa ( fig 4b ) , whereas erg fusion status was significantly associated with lower preoperative psa ( fig 4c )  . spop mutation is associated with favorable clinical outcomes after rp on kaplan - meier analysis , the spop mutant subclass had the highest biochemical - free , metastasis - free , and lowest prostate cancer specific mortality compared with erg - positive , ets - positive , and other subtypes in the retrospective grid cohort ( fig 5b and data supplement )  . 
whereas long - term outcomes were not available for the prospective grid cohort , we evaluated the association with metastasis risk using the decipher score , a validated metric for prostate cancer metastatic potential.22 , 24 , 37 , 38 we found fewer spop mutant tumors in the decipher high - risk score ( > 0.6 ) group compared with the lowand average - risk groups ( data supplement ) , which again is consistent with a favorable prognosis subtype . 
together , these data support that spop mutant prostate cancer had favorable prognosis after rp , despite its association with higher preoperative psa . favorable prognosis in high - risk psa subgroup in the spop mutant subclass pretreatment psa level is a standard component of risk stratification for prostate cancer , with a psa level > 20 ng / ml considered to be high risk by a number of risk assessment methods.39 - 41 consistent with this , higher psa was associated with worse metastasis - free survival and prostate cancerspecific mortality in the retrospective cohorts ( fig 5a ) ; however , spop mutant status had a dramatic effect on prognosis within the subgroup of patients with high psa . 
 among patients with a psa level > 20 ng / ml , spop mutant tumors were associated with better clinical outcomes , which were comparable to the lowest psa subgroup ( psa < 10 ng / ml ; fig 5d )  . 
 ( a ) enrichment of spopmut cases among higher psa subgroups from prospective grid , the cancer genome atlas ( tcga ) , taylor , and weill cornell medicine ( wcm ) cohorts . 
 ( a ) clinical outcome difference between lower , average , and higher psa groups via kaplan - meier analyses for metastasis ( met ) and prostate cancerspecific mortality ( pcsm ) free survival rates . 
 society of geriatric oncology guidelines for clinically localized prostate cancer5 - 7 classify patients with a pretreatment psa level of > 20 as high risk , even in the absence of other adverse prognostic features . 
this results in increased treatment burden , and it is recommended that patients classified as high risk who opt for radiotherapy undergo 2 to 3 years of concurrent androgen - deprivation therapy compared with a duration of 4 to 6 months for patients with intermediate risk disease . 
knowledge of the molecular subtype of prostate cancer and its impact on psa level could therefore improve risk stratification , sparing unnecessary treatment burden and directing higher - intensity therapy to patients who are truly at higher risk ; however , whether molecular subtype will actually add clinical value to the current risk stratification toolsor if it adds additional information compared with such tests as decipherremains unclear . 
additional studies will be necessary to optimally deploy these strategies clinically , but it is clear that molecular subtyping should be considered in future clinical trial designs . recent advances in technology have increased our understanding of molecular subclasses of prostate cancer , but clinical and biologic differences among the key erg - positive , ets - positive , and spop mutant subclasses remain poorly understood . 
biologically , prostate cancer cells that harbor mutant spop may produce more psa on a per - cell basis as a result of enhanced androgen transcription , essentially leading to higher psa from fewer cancer cells , whereas the opposite may be true from erg - positive tumors . 
these hypotheses need to be rigorously tested in future functional and clinical studies . as a result of the retrospective nature of the cohorts and small sample size of case cohort studies , survival analysis was inevitably affected by baseline risk . 
although the favorable prognosis was consistent with improved clinical outcomes in the spop mutant subclass , these survival results need to be independently validated in additional clinical trials to be generalizable . in conclusion , we have developed the scapt model to predict spop mutant subclass purely on the basis of transcriptional data with high confidence and accuracy . 
we believe this work not only builds a prediction model for spop mutant prostate cancers and expands the data types usable for the interrogation of clinical outcomes , but it also reinforces the concept that molecular subtyping of prostate cancer can alter the interpretation of the current standard of care risk stratification methods . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . deli liu no relationship to disclose mandeep takhar employment : genomedx mohammed alshalalfa employment : genomedx nicholas erho employment : genomedx jonathan shoag no relationship to disclose travel , accommodations , expenses : genomedx robert b . 
rubin research funding : eli lilly , janssen pharmaceuticals bruce trock consulting or advisory role : genomedx consulting or advisory role : myriad genetics research funding : myriad genetics , mdxhealth eric a . 
den consulting or advisory role : genomedx speakers ' bureau : bayer research funding : medivation , astellas pharma , genomedx travel , accommodations , expenses : genomedx scott a . 
tomlins leadership : strata oncology stock and other ownership interests : strata oncology consulting or advisory role : abbvie , janssen pharmaceuticals , astellas pharma , medivation , strata oncology , sanofi , almac diagnostics research funding : astellas pharma ( inst ) , medivation ( inst ) , genomedx ( inst ) patents , royalties , other intellectual property : coauthor on a patent issued to the university of michigan on ets gene fusions in prostate cancer travel , accommodations , expenses : strata oncology daniel e . 
spratt no relationship to disclose elai davicioni employment : genomedx leadership : genomedx stock and other ownership interests : genomedx patents , royalties , other intellectual property : cancer diagnostics using biomarkers 20140066323 travel , accommodations , expenses : genomedx andrea sboner no relationship to disclose christopher e . 
barbieri patents , royalties , other intellectual property : coinventor on a patent application filed regarding spop mutations in prostate cancer by weill cornell medicine travel , accommodations , expenses : genomedx acknowledgment ashley e . 
ross stock and other ownership interests : genomedx honoraria : healthtronics consulting or advisory role : healthtronics research funding : metamark genetics we thank the patients with prostate cancer and families who contributed to this research . 
barbieri , newyork - presbyterian hospital , new york , ny ; mandeep takhar , mohammed alshalalfa , nicholas erho , and elai davicioni , genomedx bioscience , vancouver , british columbia , canada ; robert b . 
johnson mh , ross ae , alshalalfa m , et al : spink1 defines a molecular subtype of prostate cancer in men with more rapid progression in an at risk , natural history radical prostatectomy cohort . 
ross ae , johnson mh , yousefi k , et al : tissue - based genomics augments post - prostatectomy risk stratification in a natural history cohort of intermediateand high - risk men . 
nguyen pl , haddad z , ross ae , et al : ability of a genomic classifier to predict metastasis and prostate cancer - specific mortality after radiation or surgery based on needle biopsy specimens . 
spratt de , yousefi k , deheshi s , et al : individual patient - level meta - analysis of the performance of the decipher genomic classifier in high - risk men after prostatectomy to predict development of metastatic disease . 
karnes rj , bergstralh ej , davicioni e , et al : validation of a genomic classifier that predicts metastasis following radical prostatectomy in an at - risk patient population . 
klein ea , yousefi k , haddad z , et al : a genomic classifier improves prediction of metastatic disease within 5 years after surgery in node - negative high - risk prostate cancer patients managed by radical prostatectomy without adjuvant therapy . 
boormans jl , korsten h , ziel - van der made aj , et al : identification of tdrd1 as a direct target gene of erg in primary prostate cancer . 
bennett kp , campbell c : support vector machines : hype or hallelujah ? sigkdd explor 2 : 113 , 2000 technol 2 : 1 - 27 , 2011 30 . 
fine sw , gopalan a , leversha ma , et al : tmprss2 - erg gene fusion is associated with low gleason scores and not with high - grade morphological features . 
zhou ck , young d , yeboah ed , et al : tmprss2 : erg gene fusions in prostate cancer of west african men and a meta - analysis of racial differences . 
schaefer g , mosquera jm , ramoner r , et al : distinct erg rearrangement prevalence in prostate cancer : higher frequency in young age and in low psa prostate cancer . 
font - tello a , juanpere n , de muga s , et al : association of erg and tmprss2 - erg with grade , stage , and prognosis of prostate cancer is dependent on their expression levels . 
marrone m , potosky al , penson d , et al : a 22 gene - expression assay , decipher ( genomedx biosciences ) to predict five - year risk of metastatic prostate cancer in men treated with radical prostatectomy . 
cooperberg mr , pasta dj , elkin ep , et al : the university of california , san francisco cancer of the prostate risk assessment score : a straightforward and reliable preoperative predictor of disease recurrence after radical prostatectomy . 
damico av , whittington r , malkowicz sb , et al : biochemical outcome after radical prostatectomy , external beam radiation therapy , or interstitial radiation therapy for clinically localized prostate cancer . 
 c intratumoral cd3 + and cd8 + t - cell densities in patients with dna mismatch repairdecient metastatic colorectal cancer receiving programmed cell death - 1 blockade sakti chakrabarti , md1 ; lucas j . 
sinicrope , md1 introduction the programmed cell death - 1 ( pd - 1 ) pathway represses type 1 t - helper cell cytotoxic immune responses and is upregulated in many tumors and in their microenvironment . 
blockade of this pathway with antibodies to pd - 1 has led to robust clinical responses in patients with many tumor types , including a subset of metastatic colorectal cancers ( mcrcs ) with decient dna mismatch repair ( dmmr ) .1 the clinical benet of pd - 1 blockade by pembrolizumab in dmmr mcrc was rst reported in a phase ii study in which the objective response rate ( orr ) and immunerelated progression - free survival rate at 20 weeks were 40% ( four of 10 patients ) and 78% ( seven of nine patients ) , respectively.2 expansion of this cohort to 40 patients indicated an orr of 52%.1 among dmmr tumors , mechanisms underlying responsiveness or resistance to pd - 1 blockade remain unknown , 1 and a predictive biomarker has not been identied within this tumor subtype . colorectal cancers ( crcs ) with dmmr have high microsatellite instability ( msi - h ) and are associated with a high mutational burden , neoantigen load , and typically a dense lymphocytic inltrate.3 in a recent report , the densities of cd3 + and cd8 + t cells were found to be signicantly more heterogeneous in dmmr versus procient mismatch repair ( pmmr ) colon cancers and were shown to prognostically stratify patients with both dmmr and pmmr tumors.4 , 5 on the basis of these data , we hypothesized that the responsiveness of dmmr mcrcs to immunotherapy may be related to the extent of inltration . 
tumor response was assessed by radiographic studies using response evaluation criteria in solid tumors ( recist ) version 1.1.6 the study was approved by the institutional review board of mayo clinic . informed consent was obtained from all patients before collection of data and tumor specimens for analysis . tumors were analyzed for mmr protein ( mlh1 , msh2 , msh6 , and pms2 ) expression by immunohistochemistry ( ihc ) or using a polymerase chain reactionbased assay for msi.7 in archival primary colorectal tumor tissues , cd3 + and cd8 + t - lymphocyte staining was performed by ihc ( ventana medical systems , tucson , az ) , and t - cell densities were determined in tumor core ( ct ) and invasive margin ( im ) by automated image analysis ( appendix fig a1 )  . 
analyses of cd3 + and cd8 + density scores and programmed death ligand 1 ( pd - l1 ) expression were performed by investigators blinded to clinical characteristics and patient outcomes . 
density values for cd3 + and cd8 + t cells , calculated by dividing the cell count by the area ( square millimeters ) within ct or im compartments , were used to calculate a density score ( 0 to 100 ) for each marker by compartment ( cd3 + im , cd3 + ct , cd8 + im , and cd8 + ct ) , as previously described.5 pd - l1 protein expression in tumor cells and in tumor - inltrating immune cells was determined by ihc using ventana pd - l1 ( sp263 ) rabbit monoclonal antibody and was graded according to the percentage of tumor cells with membranous pdl1 expression or as the percentage of positive immune cells in the inammatory inltrate.8 patient and tumor characteristics , details of prior treatment , and pembrolizumab response data are listed in table 1 . 
box plots illustrating the distribution of cd3 + and cd8 + t - cell density ( score range , 0 to 100 ) at the tumor core ( ct ) and the invasive margin ( im ) among the responders and nonresponders . 
responders are dened as patients with complete responses ( crs ) and partial responses ( prs ) ; nonresponders are dened as those with stable disease ( sd ) or progressive disease ( pd )  . regimens received was one ( range , one to four regimens ; one regimen in seven patients , two regimens in three patients , and four regimens in two patients )  . 
median follow - up time of the study cohort since initiation of pembrolizumab was 19.5 months ( range , 9 to 41 months ) in all patients , 21 months ( range , 16 to 24 months ) in nonresponders , and 16 months ( range , 9 to 41 months ) in responders . patient radiographic response data were as follows : two complete responses ( crs ) , ve partial responses ( prs ) , four patients with stable disease , and one patient with progressive disease . 
among pembrolizumab - treated patients who had a cr or pr ( n = 7 ) , the median time to response was 12 weeks ( range , 6 to 40 weeks )  . to examine the relationship between t - cell density scores and treatment response , patients were divided into responders ( cr and pr , n = 7 ) and nonresponders ( stable disease and progressive disease , n = 5 ) to pembrolizumab . median values and ranges of cd3 + and cd8 + t - cell density scores at the ct ( cd3 + ct and cd8 + ct ) and im ( cd3 + im and cd8 + im ) in each response category are provided in figure 1 and table 2 . 
all median t - cell density scores were higher in responders than in nonresponders , with score for cd3 + ct ( 74 v 52 , differences that were greatest respectively ) and cd8 + ct ( 88 v 37 , respectively ) , as shown in figure 1 . 
all median t - cell density scores were higher in the patient group in whom disease control was achieved for more than 12 months ( n = 8 ) , with the greatest score difference seen for cd8 + ct ( 88 v 36 for patients with disease control for more than 12 months v less than 12 months , respectively )  . median tumor cell pd - l1 expression was 2% ( range , 1% to 40% ) among responders and 1% ( range , 0% to 60% ) among nonresponders . 
median pd - l1 expression in intratumoral immune cells was 5% for both responders ( range , 2% to 25% ) and nonresponders ( range , 1% to 10% )  . 
of the ve nonresponding patients , one patients tumor underwent testing for a jak2 mutation , which was not detected . discussion the ability to distinguish high versus low immunogenic tumors could enable selection of patients who are more likely to benet from immunotherapy . 
we used an automated analysis of cd3 + and cd8 + tumor - inltrating lymphocyte density quantitation that was initially reported in stage ii colon cancers and found to be signicantly prognostic independent of mmr status.9 more recently , we validated this platform in nearly 600 stage iii colon cancers from a clinical trial of folfox - based adjuvant chemotherapy where cd3 + and cd8 + t - cell densities were shown to prognostically stratify patients with both dmmr and pmmr colon cancers.5 we found that both cd3 + and cd8 + t - cell density scores in ct and im were higher in patients with dmmr tumors who beneted from pembrolizumab , both in terms of objective response rate and duration of disease control . despite variability observed in our small patient cohort , median density scores of t - cell markers were higher in responders versus nonresponders and in those in whom disease control was achieved for more than versus less than 12 months . 
conversely , these response data suggest that lower t - cell densities are associated with immunotherapy resistance in dmmr tumors and are consistent with the reported nding that lower t - cell densities are associated with worse survival in patients with dmmr stage iii colon cancers receiving cytotoxic chemotherapy.5 our data are consistent with the ndings that increased intratumoral cd8 + t cells can predict response to immunotherapy in patients with metastatic melanoma10 and in patients with head and neck cancers.11 median follow - up of 21 months among nonresponders exceeded the median follow - up time of 12.5 months that was reported in the largest published series of patients with dmmr mcrcs treated with pd - 1 blockade.1 in that study , the mean time to the best radiographic response was 7 months , 1 suggesting that our study follow - up time was of sufcient duration to detect response outcomes . studies have shown higher expression of tumor pd - l1 protein in dmmr versus pmmr crcs , 3 and our analysis of the cancer genome atlas database revealed higher pd - l1 mrna levels in dmmr versus pmmr primary colon cancers ( unpublished data )  . 
in the current study of patients with dmmr and msi - h crcs , we found similar median levels of pd - l1 expression on tumor cells and on inltrating immune cells in responders versus nonresponders . studies of crc , expression of pd - l1 has not been shown to be a predictive biomarker , in contrast to data in patients with nonsmall - cell lung cancer . 
furthermore , a phase ii study of patients with dmmr mcrcs treated with pembrolizumab found that the expression of pd - l1 was not signicantly associated with progression - free survival or overall survival.2 insight into responses to antipd - 1 blockade in dmmr colon cancers is suggested by functional analysis in a responding patient in which rapid in vivo expansion of neoantigen - specic t - cell clones that were reactive to mutant neopeptides were found in the tumor.1 immune inltration may reect the tumors clonal evolution during treatment . 
potential causes of immunotherapy resistance include 2 - microglobulin and jak1 / 2 mutations , 12 and in our study , only one of ve nonresponders was tested for a jak2 mutation , which was not detected . 
other potential biomarkers in dmmr tumors such as the elimination of neoepitopes and differences in t - cell clonal diversity and tumor microenvironment proles warrant additional study . it is important to recognize that dmmr and msi - h are predictive biomarkers for responsiveness to immune checkpoint inhibitors . 
tumor mutation burden ( tmb ) may be a promising biomarker and has been studied in relationship to a t - cellinamed gene expression prole across 22 tumor types.13 although tmb and t - cell gene expression signature were poorly correlated , their combination jointly predicted responders to pembrolizumab , suggesting that features of neoantigenicity and t - cell activation.13 using tmb as a biomarker for immunotherapy responsiveness has important limitations in that not all mutations generate neoantigens , the correlation of tmb with neoantigen load is variable , and an established cutoff point remains unresolved.14 they may capture distinct in summary , we observed that higher cd3 + and cd8 + t - cell densities were associated with higher objective response rates and duration of disease control in patients with dmmr mcrc treated with pembrolizumab . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . andrea muranyi employment : roche stock and other ownership interests : roche patents , royalties , other intellectual property : roche travel , accommodations , expenses : roche june clements employment : ventana medical systems stock and other ownership interests : ventana medical systems research funding : ventana medical systems shalini singh employment : ventana medical systems stock and other ownership interests : ventana medical systems patents , royalties , other intellectual property : method of identifying treatment - responsive nonsmall - cell lung cancer using alk as a marker ( inst ) joleen m . 
hubbard consulting or advisory role : bayer ( inst ) research funding : boston biomedical ( inst ) , senhwa biosciences ( inst ) , bayer ( inst ) , merck ( inst ) , taiho pharmaceutical ( inst ) , treosbio ( inst ) , effector therapeutics ( inst ) robert r . 
mcwilliams consulting or advisory role : merrimack ( inst ) , zeno pharmaceuticals , newlink genetics ( inst ) research funding : prism biolab ( inst ) , genentech ( inst ) , novartis ( inst ) , newlink genetics ( inst ) , eli lilly ( inst ) , aduro biotech ( inst ) , pzer ( inst ) , sano ( inst ) , merck ( inst ) , bristol - myers squibb ( inst ) kandavel shanmugam employment : ventana medical systems stock and other ownership interests : roche patents , royalties , other intellectual property : patents ( inst ) travel , accommodations , expenses : ventana medical systems frank a . 
sinicrope stock and other ownership interests : illumina honoraria : imedex , american society of clinical oncology consulting or advisory role : roche ( inst ) , bristol - myers squibb ( inst ) , ventana medical systems ( inst ) , haliodx ( inst ) research funding : ventana medical systems ( inst ) travel , accommodations , expenses : ventana medical systems no other potential conicts of interest were reported . references le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 le dt , uram jn , wang h , et al : pd - 1 blockade in tumors with mismatch - repair deciency . 
n engl j med 372 : 2509 - 2520 , 2015 llosa nj , cruise m , tam a , et al : the vigorous immune microenvironment of microsatellite instable colon cancer is balanced by multiple counter - inhibitory checkpoints . 
cancer discov 5 : 43 - 51 , 2015 pag `es f , mlecnik b , marliot f , et al : international validation of the consensus immunoscore for the classication of colon cancer : a prognostic and accuracy study . 
lancet 391 : 2128 - 2139 , 2018 yoon hh , shi q , heying en , et al : intertumoral heterogeneity of cd3 + and cd8 + t - cell densities in the microenvironment of dna mismatch - repair - decient colon cancers : implications for prognosis . 
eur j cancer 45 : 228 - 247 , 2009 sinicrope fa , mahoney mr , smyrk tc , et al : prognostic impact of decient dna mismatch repair in patients with stage iii colon cancer from a randomized trial of folfox - based adjuvant chemotherapy . 
j clin oncol 31 : 3664 - 3672 , 2013 el jabbour t , ross js , sheehan ce , et al : pd - l1 protein expression in tumour cells and immune cells in mismatch repair protein - decient and - procient colorectal cancer : the foundation study using the sp142 antibody and whole section immunohistochemistry . 
j clin pathol 71 : 46 - 51 , 2018 gibbs ph , hutchinson r , tran b , et al : immune prole and survival outcomes in stage 2 colon cancer . 
partlov a s , bou cek j , kloudov a k , et al : distinct patterns of intratumoral immune cell inltrates in patients with hpv - associated compared to non - virally induced head and neck squamous cell carcinoma . 
 ( a ) hematoxylin and eosin ( he ) stained whole - tissue sections were manually annotated to outline the entire tumor region ( red line ) and demarcate the invasive margin ( orange line )  . 
 ( b and c ) annotations were transferred onto adjacent cd3 + and cd8 + ihc images with an algorithm outlining the invasive margin ( im ; green line ) and core of the tumor ( ct ; red line )  . 
the cfdna next - generation sequencing ( ngs ) analysis was performed at guardant health ( guardant360 ; redwood city , ca ) , a clinical laboratory improvement amendmentscertified , college of american pathologistsaccredited , new york state department of healthapproved laboratory . 
the exons of 73 cancer genes were captured using biotinylated custom bait oligonucleotides ( agilent , santa clara , ca ) , resulting in a capture footprint of 148 , 000 base pairs ( 78 kb )  . 
he received adjuvant androgen deprivation therapy and radiation therapy ( 70 gy in 35 fractions ) and developed biochemical recurrence 1 year later , when he was treated with bicalutamide . 
germline testing confirmed a heterozygous brca2 c.5946delt mutation in the patient , which was inherited from his father , who had died as a result of colon cancer at age 81 years . after liver biopsy , the patient was treated with olaparib ( 400 mg twice per day ) , resulting in rapid reduction of psa from 821 to 300 ng / ml and improvement of lymphadenopathy and liver lesions . 
 in addition to multiple brca2 mutations , ctdna analyses revealed the following alterations : tp53 f113fs ; gata3 d336d ; arid1a s1755t ; myc p72a ; and amplification of myc , kras , ccnd2 , and braf . because the biallelic reversion of both germline and truncal somatic brca1 / 2 alterations contrasted the generally accepted model of monoallelic reversion of germline brca1 / 2 mutations , we attempted to estimate the relative prevalence of germline versus somatic brca1 / 2 reversion events in patients with mcrpc using a large genomic database including comprehensive ctdna results from more than 40 , 000 patients with a variety of solid tumors . 
a third case of reversion was identified , but the patient had no previous exposure to platinum - based chemotherapy or parp inhibitors . discussion we report a case of acquired resistance to olaparib in brca2 germlinepositive mcrpc resulting from multiple acquired brca2 reversion mutations of both the germline mutation and a second - hit somatic mutation on the opposite allele . 
this case is similar to one recently reported by goodall et al , 22 in which acquired reversion mutations restored the open reading frame of not only the primary germline mutation but also the secondary loss - of - function mutation . 
 although previous studies in ovarian cancer have established that reversion of the germline allele is necessary and sufficient to restore normal brca protein function , this case suggests functional comparability of the variants despite their origin ( ie , somatic or germline )  . 
this observation challenges the established model of brca1 / 2 reversion as restricted to germline mutations and suggests that the germline or somatic origin of the allele may not play a critical biologic role in this mechanism of resistance . furthermore , this case is a powerful illustration of convergent evolution of multiple brca2 reversion mutations arising in different clones of the metastatic lesion or within multiple metastases ( fig 2 ) , as has been described.23 other studies of acquired resistance have compared ctdna with tissue - based testing on biopsies from multiple metastatic lesions in the same patient . 
these studies have shown that a single tissue biopsy often does not capture the full spectrum of acquired resistance mutations , whereas ctdna may provide a more global summary of tumor heterogeneity , as seen in this case.24 , 25 ctdna analyses also enable monitoring and early detection of mutations driving treatment resistance to parp inhibitors , with meaningful clinical implications . once a brca1 / 2 mutation is detected , longitudinal monitoring with ctdna can be relevant for early detection of reversion brca1 / 2 mutations to predict resistance to parp inhibitors , as illustrated by the case presented here . 
in women with platinum - resistant ovarian cancer , presence of brca reversion mutations was a more accurate predictor of response to subsequent platinum or parp inhibitor therapy than duration of response to previous lines of platinum therapy.26 another study identified reversion of germline brca1 / 2 mutations in high - grade serous ovarian carcinoma using ctdna and was able to predict treatment responses.27 there are limited data on the prevalence of brca reversion mutations and rates of resistance to platinum or parp inhibitors in mcrpc . 
circulating tumor dna profiling of a patient experiencing disease progression during treatment with a poly ( adp - ribose ) polymerase inhibitor , showing a known germline frameshift mutation and somatic second - hit frameshift mutation , as well as 11 additional frameshift mutations . 
phe2000fs time platinum - resistant ovarian cancer range from 25% to 70% , but these are based on small series.18 , 26 analysis of genomic data from large databases may be one way to overcome this limitation . 
although genomic testing on tissue before parp inhibitor therapy was performed for the index case , this information was not available for the additional patient cases showing evidence of reversion mutation . 
all patients underwent cfdna analysis at the time of clinical progression , suggesting that they had developed platinum or parp inhibitor resistance , but the duration of their response during therapy or presence of reversion mutations before exposure is unknown . 
 with regard to the retrospective cohort analysis , our brca2 germline mutation rate was lower than that previously described in the literature.28 possible explanations for this include exclusion of putative germline missense and nonsense mutations in the analysis and overly restrictive germline maf thresholds resulting in exclusion of putative germline mutations in patients with more severe allele imbalance . 
lastly , one patient case with evidence of a reversion mutation had no prior exposure to parp inhibitors or platinu review of the patients treatment history revealed treatment with taxane - based chemotherapy , radium - 223 , and mitoxantrone . 
at the time of relapse , a bone marrow biopsy was performed , and a patient - derived cell line showed loss of the fanconi anemia phenotype because of monoallelic reversion of the brca2 mutation and restoration of wild - type brca2 function . 
the authors suggest that dna intercalating agents such as mitoxantrone may have the ability to induce reversion mutations and lead to resistance . compared with biopsy , cfdna analyses allow easier monitoring and potentially earlier detection of mutations that result in treatment resistance . 
cfdna analysis , which allows detection of both somatic and germline mutations in a single test , is well suited to distinguish whether a somatic brca mutation represents a second - hit loss of function or a reversion of the germline brca mutation . 
giles manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors sahithi pamarthy no relationship to disclose vinay sagar no relationship to disclose stephen fairclough employment : guardant health stock and other ownership interests : guardant health research funding : guardant health patents , royalties , other intellectual property : guardant health travel , accommodations , expenses : guardant health justin odegaard employment : guardant health stock and other ownership interests : guardant health richard b . 
 alice fan stock and other ownership interests : molecular decisions consulting or advisory role : verily research funding : calithera biosciences patents , royalties , other intellectual property : stanford patent has been licensed young kwang chae consulting or advisory role : foundation medicine , boehringer ingelheim , biodesix , counsyl , astrazeneca , guardant health , speakers bureau : merck , genentech / roche travel , accommodations , expenses : hanmi massimo cristofanilli honoraria : domp farmaceutici , pfizer consulting or advisory role : domp farmaceutici , newomics , vortex biosciences maha h . 
hussain honoraria : onclive , sanofi research funding : genentech ( inst ) , pfizer ( inst ) , pcctc ( inst ) , astrazeneca ( inst ) patents , royalties , other intellectual property : title : systems and methods for tissue imaging , 3676 our file , serial no . 
giles employment : actuate leadership : actuate honoraria : novartis consulting or advisory role : novartis travel , accommodations , expenses : medimmune , novartis , foundation medicine affiliations benedito a . 
cleton - jansen am , collins n , lakhani sr , et al : loss of heterozygosity in sporadic breast tumours at the brca2 locus on chromosome 13q12 - q13 . 
collins n , mcmanus r , wooster r , et al : consistent loss of the wild type allele in breast cancers from a family linked to the brca2 gene on chromosome 13q12 - 13 . 
tutt an , lord cj , mccabe n , et al : exploiting the dna repair defect in brca mutant cells in the design of new therapeutic strategies for cancer . 
bouwman p , jonkers j : molecular pathways : how can brca - mutated tumors become resistant to parp inhibitors ? clin cancer res 20 : 540 - 547 , 2014 13 . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
epstein ji , egevad l , amin mb , et al : the 2014 international society of urological pathology ( isup ) consensus conference on gleason grading of prostatic carcinoma : definition of grading patterns and proposal for a new grading systeam j surg pathol 40 : 244 - 252 , 2016 22 . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
de mattos - arruda l , weigelt b , cortes j , et al : capturing intra - tumor genetic heterogeneity by de novo mutation profiling of circulating cell - free tumor dna : a proof - of - principle . 
christie el , fereday s , doig k , et al : reversion of brca1 / 2 germline mutations detected in circulating tumor dna from patients with high - grade serous ovarian cancer . 
ikeda h , matsushita m , waisfisz q , et al : genetic reversion in an acute myelogenous leukemia cell line from a fanconi anemia patient with biallelic mutations in brca2 . 
 long - term complete response of an androgen receptorpositive triple - negative metastatic breast cancer to abiraterone acetate introduction several gene expression array studies have identified a new breast cancer subtype characterized by the expression of the androgen receptor ( ar ) , absence of the estrogen receptor ( er ) , and paradoxical expression of many genes that are typically expressed in er - positive luminal tumors.1 - 3 two thirds of this tumor subtype are human epidermal growth factor receptor 2 ( her2 ) positive . 
these ar - positive and triple - negative tumors have been identified as a stable subtype in two series of tnbcs.4 , 5 of note , ar is also expressed in approximately 75% of er - positive / her2 - negative breast cancers.6 however , clinical and preclinical data suggest that ars act as a tumor suppressor gene in er - positive tumors and as an oncogene in er - negative tumors.7 in both retrospective series8 and prospective clinical trials , 9 - 11 the following immunohistochemistry ( ihc ) definition is classically used to identify this breast cancer subtype : ar positive and er , progesterone receptor ( pr ) negative , and her2 negative . 
there is no universal consensus on defining ar positivity to date , although the accepted definition of ar positivity is 10% . preclinical in vitro2 , 12 - 14 and in vivo14 , 15 data suggest that androgens are involved in the development and growth of the mda - mb - 453 cell line , which is used as an in vitro model for the ar - positive tnbc subtype.2 consequently , in three prospective clinical trials , either competitive antagonists of the ar ( bicalutamide or enzalutamide ) or androgen synthesis suppressor , cyp17 inhibitor ( abiraterone acetate , aa ) , were evaluated in ar - positive tnbcs . 
 she received neoadjuvant chemotherapy ( three cycles of fluorouracil , epirubicin , and cyclophosphamide followed by three cycles of docetaxel ) followed by mastectomy and axillary lymph node dissection ( level 1 and 2 )  . 
 the arrows show the index masses with changes with therapies . multiple sclerosis and administered interferon at a dose of 30 g per week . in november 2007 , the patient was diagnosed with an ipsilateral axillary lymph node relapse without distant metastasis . 
no further treatment was proposed . in july 2013 , she presented with a 4 - cm left axillary mass with skin involvement ( fig 1a ) and two supraclavicular 1 - cm lymph nodes ; a core biopsy of the axillary mass confirmed tnbc , with a proliferation index ( ki - 67 ) of 15% . 
on the computed tomography scan ( figs 1b and 1c ) , in addition to the axillary mass , several chest soft tissue masses were observed ; no visceral or bone metastasis was observed . 
the patient was included in the ucbg 2012 - 1 trial and received experimental treatment with 1 , 000 mg of aa and 10 mg of prednisone administered orally , daily . 
ten months after the treatment initiation , clinical and computed tomography scan evaluations showed that the patient achieved a cr ( on the basis of the response evaluation criteria in solid tumors criteria )  . 
after 4 years , the patient is still receiving the treatment with aa and low - dose prednisone , with a prolonged cr ( figs 1d - 1f )  . 
concomitantly , she has been receiving interferon treatment for multiple sclerosis . further ihc analyses later performed on the 2006 mastectomy and the 2007 axillary relapse showed that 100% of cells were ar positive . 
 furthermore , ihc analyses on additional markers in the 2013 axillary relapse confirmed a pronounced apocrine feature with marked forkhead box a1 and gross cystic disease fluid protein 15 expression . 
ongoing clinical trials on ar - positive triple negative breast cancer in metastatic setting single agent combination antiandrogen ar antagonist enzalutamide ( phase iii , clinicaltrials.gov identifier : nct02929576 , withdrawn ) bicalutamide v chemotherapy ( phase iii / first line , clinicaltrials . gov identifier : nct03055312 , recruiting ) darolutamide v chemotherapy ( randomized phase ii , first and second line , clinicaltrials.gov identifier : nct03383679 , recruiting ) bicalutamide plus cdk4 / 6 inhibitor ribociclib ( phase i / ii , clinicaltrials.gov identifier : nct03090165 , recruiting ) bicalutamide plus cdk4 / 6 inhibitor palbociclib ( phase i / ii , clinicaltrials.gov identifier : nct02605486 , recruiting ) enzalutamide plus pi3k inhibitor alpelisib ( phase i , clinicaltrials.gov identifier : nct03207529 , not yet recruiting ) or plus pi3k inhibitor taselisib ( phase i / ii , clinicaltrials.gov identifier : nct02457910 , recruiting ) cyp17a1 inhibitors orteronel ( tak - 700 ; phase ii , clinicaltrials.gov identifier : nct01990209 , recruiting ) seviteronel ( phase i / ii , clinicaltrials.gov identifier : nct02580448 , recruiting ) selective ar modulator cr1447 ( phase ii , clinicaltrials.gov identifier : nct02067741 , recruiting ) enobosarm plus pembrolizumab ( phase ii , clinicaltrials.gov identifier : nct02971761 , recruiting ) enobosarm ( phase ii , clinicaltrials.gov identifier : nct02368691 , terminated ) abbreviations : ar , androgen receptor ; cdk , cyclin - dependent kinase ; her2 , human epidermal growth factor receptor 2 ; pi3k , phosphatidylinositol 3 - kinase . from a clinicians perspective , the cbrs at 6 months ( 19% to 29% ) observed in this breast cancer subtype in the three prospective trials testing ar antagonist or androgen synthesis inhibitor are modest but clinically relevant . 
patients with ar - positive tnbcs seem to be older compared with the whole tnbc population.9 - 11 , 17 they also tend to relapse after a long interval after the primary tumor treatment . 
in our opinion , in ar - positive tnbcs , treatment choice between antiandrogens and chemotherapy could take into account different factors , including disease - free interval , tumor burden , and the need for rapid disease / symptom control , similar to luminal erand / or pr - positive tumors . 
of note , it is important to remember that progression - free survival for first - line chemotherapy is merely 4 to 6 months.18 , 19 from a researchers perspective , cbrs at 6 months with antiandrogens in this tumor subtype are much lower than those observed with anti - aromatase inhibitors used as single agents in luminal erand / or pr - positive cancers . 
in the latter group , the historical cbrs range from 49% to 59% for first - line and from 24% to 37% for second - line treatments , respectively.20 hence , there is a need to improve these results in ar - positive tnbcs , and we briefly outline four key areas that could be improved . first , ihc is probably not ideal to identify this breast cancer subtype . 
of note , in the enzalutamide trial , 10 patients with low ar ( 1% to 9% ) were included in an exploratory cohort , and some of these patients responded . 
in two large series of tnbcs analyzed by gene expression array , 11% and 17% of tumors were ar positive.4 , 5 in a tnbc series analyzed by ihc , 22% to 35% of patients were ar positive.8 it is difficult to explain this difference . 
hence , there is a need to better identify this subtype in clinical practice , for example , by using rna signatures with a selected number of transcripts.5 second , predictors of antiandrogen treatment sensitivity in this breast cancer subtype should be developed . 
new preclinical models are needed ; the reliability of the mda - mb - 453 cell line has been in question because of genomic alterations , such as ar mutation.22 , 23 this ar q865h mutation in its ligand - binding domain is reported to decrease sensitivity to dihydrotestosterone , limiting its use to test antiandrogen therapy.22 a new patient - derived xenograft model of molecular apocrine tumors , directly derived from patients , could be a solution.24 finally , we need better drugs and combinations . 
 however , both enzalutamide and abiraterone have shown to improve the sensitivity of tnbc cell lines toward immune - mediated lysis , providing potential rationale for combination of immunotherapy with antiandrogen therapy.25 in conclusion , we believe that this patients case is important for clinicians . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . thomas grellety consulting or advisory role : novartis herv bonnefoi consulting or advisory role : abbvie , astellas pharma , bayer healthcare pharmaceuticals , innocrin pharmaceuticals , puma biotechnology research funding : bayer ( inst ) travel , accommodations , expenses : roche , pfizer acknowledgment we thank ravi nookala , phd , of institut bergoni for the medical writing service . affiliations thomas grellety and herv bonnefoi , institut bergoni unicancer , universit bordeaux , institut national de la sant et de la recherche mdicale u1218 , institut national de la sant et de la recherche mdicale cic1401 ; and thomas grellety , gaetan macgrogan , camille chakiba , michele kind , and herv bonnefoi , institut bergoni , bordeaux , france . support supported by the fondation pour la lutte contre le cancer pour les recherches medico - biologiques , site de recherche intgre sur le cancer - bordeaux recherche intgre oncologie , and groupement interrgional de recherche clinique et dinnovation sud - ouest outre - mer grant no . 
vera - badillo fe , templeton aj , de gouveia p , et al : androgen receptor expression and outcomes in early breast cancer : a systematic review and meta - analysis . 
hickey te , robinson jl , carroll js , et al : minireview : the androgen receptor in breast tissues : growth inhibitor , tumor suppressor , oncogene ? mol endocrinol 26 : 1252 - 1267 , 2012 8 . 
gucalp a , tolaney s , isakoff sj , et al : phase ii trial of bicalutamide in patients with androgen receptor - positive , estrogen receptor - negative metastatic breast cancer . 
traina ta , miller k , yardley da , et al : results from a phase 2 study of enzalutamide ( enza ) , an androgen receptor ( ar ) inhibitor , in advanced ar + triple - negative breast cancer . 
bonnefoi h , grellety t , tredan o , et al : a phase ii trial of abiraterone acetate plus prednisone in patients with triple - negative androgen receptor positive locally advanced or metastatic breast cancer ( ucbg 12 - 1 )  . 
lehmann bd , bauer ja , schafer jm , et al : pik3ca mutations in androgen receptor - positive triple negative breast cancer confer sensitivity to the combination of pi3k and androgen receptor inhibitors . 
arce - salinas c , riesco - martinez mc , hanna w , et al : complete response of metastatic androgen receptor - positive breast cancer to bicalutamide : case report and review of the literature . 
oshaughnessy j , schwartzberg l , danso ma , et al : phase iii study of iniparib plus gemcitabine and carboplatin versus gemcitabine and carboplatin in patients with metastatic triple - negative breast cancer . 
miles dw , diras v , corts j , et al : first - line bevacizumab in combination with chemotherapy for her2 - negative metastatic breast cancer : pooled and subgroup analyses of data from 2447 patients . 
moore nl , buchanan g , harris jm , et al : an androgen receptor mutation in the mda - mb - 453 cell line model of molecular apocrine breast cancer compromises receptor activity . 
vranic s , gatalica z , wang zy : update on the molecular profile of the mda - mb - 453 cell line as a model for apocrine breast carcinoma studies . 
lumbar spine magnetic resonance imaging ( mri ) demonstrated multiple bone lesions , and computed tomography scans revealed a 4 - cm right - sided hilar lung mass , regional thoracic lymphadenopathy , multiple hepatic metastases , a left - sided adrenal metastasis , and several osseous lesions ( fig 1a )  . 
biopsies of the subcarinal lymph node and the left - side adrenal lesion were performed , which confirmed adenocarcinoma of lung origin ( figs 2a and 2b )  . the patient was treated with radiation therapy to the painful vertebral metastasis and stereotactic radiosurgery to two brain lesions . 
200 genes ( foundationone ; foundation medicine , cambridge , ma ) revealed an egfr exon 19 deletion ( del19 ) mutation , a tp53 v173l mutation , an egfr amplification , and an rb1 loss of exons 18 and 19 . oral erlotinib 150 mg daily was initiated in may 2015 , and uniform disease response was evident on restaging scans in july 2015 ( fig 1b )  . 
however , in october 2015 , repeat imaging showed significant growth in a single liver lesion and a new 2.6 - cm lesion in the spleen , with continued response elsewhere , including the brain ( fig 1c )  . repeat biopsy of the enlarging liver lesion in november 2015 revealed nests of highly atypical cells with finely dispersed chromatin , inconspicuous nucleoli , and abundant mitoses ( figs 2c to 2e )  . immunohistochemical stains were positive for synaptophysin and chromogranin and negative for thyroid transcription factor 1 and napsin a . 
the overall features were consistent with small - cell lung cancer ( sclc ) transformation.4 ngs that consisted of targeted hotspot evaluation in 39 genes ( snapshot ngs ; massachusetts general hospital , boston , ma ) confirmed the presence of the original egfr del19 and tp53 mutations and showed additional mutations in pik3ca ( g545l ) , pik3ca ( g726l ) , erbb3 ( g337a ) , and fbxw7 ( l8p )  . 
a patientderived xenograft generated from this biopsy specimen lacked rb protein expression but retained minimal egfr expression and demonstrated activation of the mitogen - activated protein kinase and akt pathways ( fig 3c ) , likely as a result of the presence of an activating pik3ca mutation . the patient was treated with carboplatin and etoposide chemotherapy and ongoing erlotinib . 
scans after four cycles of chemotherapy showed a mixed response with slight regression in the previously biopsied ( sclc - transformed ) liver metastasis , stable brain metastases , and multiple new distinct sites of hepatic progression ( fig 1d )  . 
 ( a to e ) selected radiographic images of the liver illustrate involvement with cancer . treatments and key biopsy ( bx ) results ( tissue or liquid ) are indicated underneath each image in chronologic order . 
of note , the guardant360 assay can detect rb1 inactivating mutations but not allelic losses . we interpreted the emergence of an egfr t790m positive clone as the most likely resistance mechanism within the growing liver nodules . 
the patient discontinued chemotherapy , and the t790m - specific tki osimertinib7 was administered in march 2016 . restaging in june 2016 ( performed with mri because of renal dysfunction ) revealed that the hepatic lesions that had most recently progressed on chemotherapy ( presumed t790m positive ) had stabilized , but the liver lesion biopsied in 2015 ( sclc histology at that time ) had again enlarged with no other sites of systemic or intracranial progression ( fig 1e )  . 
a repeat plasma guardant360 test in june 2016 confirmed that egfr t790m was now undetectable , but increases were found in the mafs of pik3ca e726k ( 50.9% ) , pik3ca e545k ( 54.3% ) , tp53 v173l ( 54.8% ) , and egfr del19 ( 45.5% ; fig 4 )  . 
 ( a ) hematoxylin and eosin ( h&e ) stain and ( b ) thyroid transcription factor 1 ( ttf - 1 ) immunostain of fine - needle aspiration of a subcarinal lymph node at diagnosis show adenocarcinoma with diffuse ttf - 1 expression consistent with a lung primary . 
 ( c ) h&e stain and ( d ) synaptophysin ( syn ) and ( e ) ttf - 1 immunostains of a liver core biopsy at the time of acquired resistance to erlotinib demonstrate small - cell lung cancer with solid nests of highly atypical epithelial cells with finely dispersed chromatin , inconspicuous nucleoli , and brisk mitotic activity . 
 ( a ) summary of all evaluable probes across all chromosomes ( red , genomic gains ; blue , genomic losses ) shows diffuse losses across chromosome 13 , including the rb1 gene locus . 
 ( b ) a magnified view of four specific genes on chromosome 13 shows that all examined loci of rb1 are lost , with only blue signals and complete absence of red signals . 
 ( c ) tissue obtained from the november 2015 liver biopsy ( which shows sclc ) wasusedtogenerateapatient - derivedxenograft ( pdx ) inannsgmouseandsubsequentlypassagedthroughadditionalnsgmice.thepdxtumordemonstrated sclc histologic features consistent with the patient biopsy sample ( not shown )  . 
a western blot demonstrates relative protein levels of egfr , p - akt ( s473 ) , p - erk , rb , p16 , and actin ( loading control ) among pdx tumors ( mgh1529 ; two tumors shown ) with control lung adenocarcinoma ( adenoca ) and sclc samples for comparison . genetic characteristics of the various cell lines ( rb1 , p16 , and egfr exon 19 deletion [ del19 ] mutations [ mut ] ) are shown above the western blot . 
however , one resistant clone with sclc morphology emerged clinically in october 2015 , and genotyping confirmed an additional private pik3ca e545l mutation , which often is seen in sclc - transformed egfr mutant clones.4 during chemotherapy , we believe that the sclc clone diminished , whereas another clone that harbored an acquired egfr t790m mutation and perhaps two other distinct pik3ca mutations ( e545k and e726k ) emerged as observed in plasma ctdna in march 2016 . although a tissue biopsy specimen could not be obtained at that time , on the basis of our prior observation that sclc and adenocarcinoma populations can oscillate in response to specific treatment4 and that t790m is rarely seen in sclc - transformed tissue biopsy specimens , we hypothesize that the t790m - positive clone detected in plasma maintained an adenocarcinoma phenotype . 
the t790m clone was no longer detectable by june 2016 after treatment with osimertinib , but one or more other clones became dominant with increasing mafs , and subsequently , the disease became refractory to therapy ( fig 4 )  . 
this elevation in ctdna and subsequent clinical decline mirror data that demonstrated the correlation of increased mafs and decreased overall survival.9 - 11 in addition , the patient had a tumor with baseline rb1 mutation that was expected to lead to loss of function and is believed to play an essential role in the histologic transformation to sclc among egfr mutant cancers . 
we previously demonstrated that rb1 is universally lost in sclc - transformed cancers , although not sufficiently for transformation.12 recent work has demonstrated that baseline rb1 loss among egfr mutant tumors is a strong predictor for subsequent sclc transformation.13 as the clinical use of ngs panels increases and baseline inactivating rb1 mutations are more frequently detected , more data to understand the implications will be required , including a better understanding of the critical steps that lead to the lineage shift , so that we can develop more - effective treatment strategies.14 finally , this case report illustrates the potential utility of longitudinal molecular profiling during targeted therapy . 
at present , two mutationspecific food and drug administrationapproved plasma tests may be used to select egfr tkis.15 , 16 clinical practice is rapidly evolving , but on the basis of current evidence , it is reasonable to offer plasma genotyping upon progression with frontline egfr tkis to evaluate for t790m . 
 testing is negative for t790m , reflexive tissue biopsy should be performed because approximately 30% of ctdna test results will be false negative.17 the exact role of liquid biopsies for serial monitoring requires more rigorous evaluation , but a key appeal is that tumor biopsy findings may underestimate the full spectrum of resistant clones present at the time of progression.6 , 18 , 19 in practice , we commonly see the type of mixed radiographic response as observed in this patient with regression of some sites but continued growth in others . 
heterogeneity among distinct cancer subclones may explain such disparate responses , and longitudinal plasma testing might be a valuable adjunct to tissue biopsies to understand the dynamic evolution of various clones . for example , although tissue biopsy may offer critical information about the histology and molecular alterations of a specific progressing lesion , it may lack information about other sites of disease . 
conversely , ctdna genotyping could paint a more - complete picture of the competing resistance clones within a patient , although precise determination of which molecular alterations coexist within one clone or in one anatomic site are not currently possible . 
indeed , other studies have demonstrated that multiple resistance mechanisms can be detected within plasma , 18 and we and others have observed that longitudinal ctdna analyses can track the rise and fall of distinct subclones.6 , 20 in summary , this case report illustrates that the relative magnitude of resistant subclones can fluctuate in response to therapy , that liquid biopsies hold great potential to detect and monitor distinct genetic subpopulations within a patient , and that the presence of a baseline rb1 mutation in an egfr mutant cancer and subsequent sclc transformation raises important questions about monitoring such patients . 
for those with egfr mutant lung cancers , both tissue and liquid biopsy specimens can yield critical information to elucidate dominant clones that drive cancer growth at various time points . 
mooradian no relationship to disclose zofia piotrowska consulting or advisory role : boehringer ingelheim , astrazeneca , ariad pharmaceuticals , takeda pharmaceuticals , superdimension research funding : guardant health ( inst ) benjamin j . 
drapkin no relationship to disclose dora dias - santagata no relationship to disclose nicolas marcoux honoraria : bristol - myers squibb konstantinos arnaoutakis honoraria : foundation medicine , precision advisors , ariad pharmaceuticals consulting or advisory role : foundation medicine , precision advisors , ariad pharmaceuticals rebecca j . 
nagy employment : guardant health stock and other ownership interests : guardant health richard lanman employment : guardant health , veracyte leadership : guardant health stock and other ownership interests : guardant health , veracyte research funding : guardant health anthony j . 
farago honoraria : foundation medicine consulting or advisory role : pharmamar , merrimack , takeda pharmaceuticals , abbvie , intervention insights research funding : pharmamar ( inst ) , abbvie ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , loxo ( inst ) , ignyta ( inst ) travel , accommodations , expenses : pharmamar , abbvie , stemcentrx mari mino - kenudson consulting or advisory role : merrimack , h3 biomedicine , acd pharmaceuticals , roche , genentech aaron n . 
sequist honoraria : astrazeneca consulting or advisory role : astrazeneca , genentech , roche , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , pfizer ( inst ) affiliations meghan j . 
sequist lv , yang jc , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as first - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
yu ha , arcila me , rekhtman n , et al : analysis of tumor specimens at the time of acquired resistance to egfr - tki therapy in 155 patients with egfr - mutant lung cancers . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a third - generation egfr inhibitor . 
cancer discov 5 : 713 - 722 , 2015 janne pa , yang jc , kim dw , et al : azd9291 in egfr inhibitor - resistant non - small - cell lung cancer . 
schwaederle mc , patel sp , husain h , et al : utility of genomic assessment of blood - derived circulating tumor dna ( ctdna ) in patients with advanced lung adenocarcinoma . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
suda k , murakami i , sakai k , et al : small cell lung cancer transformation and t790m mutation : complimentary roles in acquired resistance to kinase inhibitors in lung cancer . 
 systematic assessment of tumor purity and its clinical implications syed haider , phd1 , 2 ; svitlana tyekucheva , phd3 , 4 ; davide prandi , phd5 ; natalie s . 
laird , phd10 ; chris sander11 , 12 ; wenyi wang , phd13 ; francesca demichelis , phd5 , 14 ; massimo loda , md15 , 16 ; and paul c . 
as molecular proles are frequently generated using bulk tissue sections , they represent an admixture of multiple cell types ( including immune , stromal , and cancer cells ) interacting with each other . 
bulk mrna and microrna proles were subject to in silico deconvolution to estimate cancer cellspecic mrna and microrna proles . results we present a systematic comparison of 10 tumor purity estimation methods on a cohort of 333 prostate tumors . 
limited concordance between dnaand mrna - derived purity estimates remained a general pan - cancer phenomenon when tested in an additional 4 , 497 tumors spanning 12 cancer types . conclusion the choice of tumor purity estimation method may have a profound impact on the interpretation of genomic assays . 
taken together , these data highlight the need for improved assessment of tumor purity and quantitation of its inuences on the molecular hallmarks of cancers . jco precis oncol 4 : 995 - 1005 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the tumor microenvironment represents an admixture of multiple cell types and complex interactions between bona de cancer cells and surrounding stromal and immune cells.1 because a majority of highthroughput experiments are performed on bulk tissue samples , the resulting signal is usually confounded by nonmalignant tumor - adjacent cells ( tacs )  . variable tumor content and variable tac composition can impinge upon interpretations of molecular data and subsequent clinical decisions.2 - 4 to delineate true residual signal representing individual cell populations , it is crucial to accurately estimate tumor purity . 
tumor purity represents the fraction of cancer cells in a tumor and can be estimated either by expert pathologists reviewing tumor sections5 or in silico ( using epigenomic , genomic , or transcriptomic proles ) .6 pathologic estimates can be inconsistent5 and pragmatically may not always represent the region of tumor that is subject to molecular proling . 
although in silico estimates could circumvent these problems , it remains unclear to what extent these estimates vary across purity calling methods and with the underlying type of biomolecule ( eg , dna v rna )  . 
previous studies have quantied the pan - cancer purity landscape2 , 7 and compared a panel of tools for estimating tumor purity.6 however , systematic benchmarking of in silico tumor purity against matched pathologic estimates and its association with multimodal clinico - genomic proles remains to be elucidated . 
herein , we present systematic benchmarking of 10 purity estimation methods using dna , mrna , and microrna ( mirna ) proles in a 333patient clinically - coherent cohort8 with matched multiobserver pathologic estimates of purity . 
to determine the context specicity of these algorithms , we compared tumor purity estimates from multiobserver pathology to those from multiple algorithms working on different biomolecules ( eg , dna , rna )  . knowledge generated tumor purity estimates from in silico tools varied signicantly from pathology estimates . 
we recommend parameterizing genomic analyses with tumor purity estimated from the matched molecular analyte being analyzed . relevance tumor purity is a key criterion for sample inclusion in clinico - genomic studies and subsequent interpretation of molecular results . 
computational tools often require purity estimates ; we show that these are inuenced by the selected purity estimator . both molecularly driven clinical trials , as well as therapeutic and theranostic decisions , may be affected by these choices . quantify how molecular correlates of tumor purity can skew clinico - genomic interpretations as the result of variable estimates of cancer cell fraction . 
integer infers purity , ploidy , and subclonality from paired tumor and normal samples using the following principles : ( 1 ) models the relationship between the observed allelic frequencies and the underlying copy number changes , and the possible existences and impacts of multiple subclones that may often mislead inferences if not explicitly modeled ; ( 2 ) simultaneous statistic inference on the basis of both copy number changes and major allelic frequencies ; ( 3 ) restoration of information lost as a result of the guanine - cytosine content and actual sizes of each library insert and other specic biases of each genomic location ; ( 4 ) avoid making inferences when the signal - to - noise ratio is not ideal because of technical artifacts ; ( 5 ) an explicit modeling of whole - genome duplication events and whole - chromosome duplication events , which are common in cancer genomics and have huge impacts on the accurate inference of purity and ploidy ; the cancer genome atlas pan - cancer purity estimates were generated using processed rna - seq data ( for isopure ) downloaded from ( download version 2015 ) and snp6 array level - 1 data ( for ascat ) downloaded from gdc data portal . consensus pathology , dna , and mrna purity estimates multiobserver pathology reviews yielded purity ranges , 8 which were further collapsed into single - point estimates using the median value of purity range in deciles . 
dna ( absolute , ascat , clonet , integer , oncosnp ) and mrna ( demix and isopure - r ) based purity estimates were aggregated using median dna and mrna estimates , respectively . availability of data and materials all processed data are available either in the data supplement or uploaded to as speciﬁed in the data supplement . 
 haider et al ethics approval and consent to participate tissue contributing sites followed appropriate consent documentation and approved submission of cases to the cancer genome atlas , as detailed in the original publication.8 results prostate cancer presents complex intraand interpatient heterogeneity . 
it is an ideal model to study heterogeneity because of frequent surgical management via radical prostatectomy of the whole gland , allowing spatio - genomic studies.9 , 10 we collated pathologic , molecular , and clinical data sets from the cancer genome atlas ( tcga ) prostate marker study , which comprised 333 patients.8 purity estimates from multiple pathologists were consolidated , resulting in point estimates as previously described8 ( see methods )  . 
for a subset of cases , both top and bottom tissue block slides ( with sections acquired for molecular analysis in between these ) were assessed by multiple pathologists , demonstrating moderate correlation between pathologists ( top sections : pearsons r = 0.64 , p = 6.23 107 ; bottom sections : pearsons r = 0.53 , p = 8.93 103 ; data supplement fig 1a - b )  . 
a similar trend was observed between the pathology estimates of top and bottom sections ( pearsons r = 0.59 , p = 2.03 1012 ; data supplement fig 1c ) , highlighting potential inuence of spatial heterogeneity . 
in silico estimates of tumor purity were generated using nine methods11 - 18 that leverage dna ( methylation or copy number data ) , mrna , or mirna proles ( data supplement tables 1 and 2 ; methods )  . 
of note , leuc estimates on the basis of dna methylation data were right skewed , with a median purity of 0.9 ( leuc - other = 0.33 , p = 1.44 1095 , wilcoxon rank sum test )  . 
interestingly , all these methods were based on dna proles ( genomic or epigenomic ) , suggesting intrinsic limitations in estimating tumor purity from dna - based assays in this setting . 
these limitations could be explained by the dna prole itself , because samples with failed purity estimates exhibited quiet genomes with low numbers of somatic single nucleotide variants ( snvs ; data supplement fig 2a - b )  . 
pathology calls did not show clear evidence of low purity ; however , rnabased methods predicted a trend toward low purity for a subset of samples ( data supplement fig 2c )  . 
however , it is probable that some may also represent quiet cancer genomes , which are now increasingly recognized as a real phenomenon , particularly in prostate cancer.8 , 19 inspection of the complete sample set revealed no association with histologic heterogeneity ( rationalized as gleason score10 ; fig 1b , data supplement fig 3a - b )  . 
hence , we preclude spatial heterogeneity as the primary factor underlying this lack of concordance . these data highlight that variation and error proles among the intraplatform estimates are probably correlated and suffer from similar intrinsic limitations , independent of the specic algorithm used . 
therefore , we created consensus dna and mrna purity estimates using the median for each class of methods , hereafter referred to as dna and mrna estimates ( see methods )  . 
the differences between pathology estimates and either dna or mrna estimates were strongly correlated ( pearsons r = 0.81 , p = 4.68 1079 ; fig 2 ) , with 29.13% of cases demonstrating agreement ( within 15% purity of each other )  . 
 ( a ) distribution of tcga prostate tumor purity estimates ( n = 333 ) using in silico methods and consolidated multiobserver pathology reviews ; ( b ) patient - wise purity estimates grouped by gleason score . 
data from integer were available for 107 samples using the low - pass dna sequencing data ; ( c ) pearson correlation between purity estimates inferred using in silico methods and pathology reviews . 
of the dnaand mrna - based estimates , only two samples displayed discordant directions of effect relative to pathologic estimates ( purple and yellow dots in fig 2 ) , highlighting overall similarity in error proles of the underlying biomolecules . next , we assessed whether the key transcriptional and genomic biomarkers that underpin prostate cancer biology are dependent on tumor purity . 
to further delineate the relationship between tumor purity and somatic mutations , we stratied purity estimates by the mutation status of a panel of recurrently altered genes in prostate cancer.8 tumor purity determined by at least one prole was associated with six genes , including erg fusions and spop , foxa1 , and tp53 point mutations ( false discovery rate [ fdr ] adjusted p , .25 , wilcoxon rank sum test ; fig 3d , data supplement table 3 )  . 
for these six genes , tumor purity was moderately higher in mutant samples . to characterize this association between driver gene status and tumor purity , we evaluated the associations between tumor purity and the variant allele frequency ( vaf ) in samples carrying mutations ( fig 3e )  . 
however , pathology estimates of tumor purity were unable to accurately capture the vaf of these recurrently altered genes . next , we evaluated whether pathology , dna , mrna , and mirna purity estimates vary in their associations with individual genes or mirnas and to what extent these can be overcome by using in silico deconvolution.15 each of the four consensus purity estimators was individually correlated with ve molecular proles ( bulk / nave and deconvolved mrna abundance , bulk / nave and deconvolved mirna abundance , and bulk copy number data ; deconvolved proles were generated using isopure )  . 
nave mrna and mirna proles exhibited the greatest proportion of features correlated with tumor purity , which diminished after in silico deconvolution , highlighting potentially confounding tacs . with the exception of nave mirna proles , purity estimates were inversely correlated with molecular proles regardless of the underlying purity estimation prole ( data supplement fig 5a - f )  . 
these data suggest that the presence of genomic and transcriptomic correlates of tumor purity are likely to confound biologic and clinical interpretations . because dnaand mrna - based assays are most commonly used in cancer genomics , we asked if the purity estimates from these two analytes are comparable in other cancers . 
given the strong intra - analyte correlation ( fig 1c ) , we considered a representative dna - based method ( ascat ) and an mrna - based method ( isopure ) to estimate tumor purity for an additional 12 cancer types ( 4 , 497 tumor samples ) from tcga project ( fig 4b , prostate cancer data discussed above is shown for reference only )  . overall , all cancer types showed an average purity of at least 0.56. 
these data further underscore the importance of using analyte - matched purity estimates for bioinformatics analysis and subsequent interpretation . discussion herein , we provide evidence that tumor purity estimates manifest intrinsic properties of the underlying information used for purity estimation and exhibit only modest interprole concordance . 
however , interpathologist variation observed in our study , as well as previous studies , suggests that there are probably some inaccuracies in these estimates because of their subjectivity / qualitative nature.5 , 21 these discrepancies may also be a result of the lack of full spatial heterogeneity of the pathologic slide . 
genomic correlates of tumor purity as summarized using androgen receptor ( ar ) signature score ( a ) , percent genome altered ( [ pga ] , b ) , and mutation burden ( c )  . 
statistical tests were performed for genes with more than three mutant samples . therefore , idh1 , rb1 , akt1 , and chd1 ( displayed with x ) were deemed inappropriate for statistical testing . 
 ( a ) correlation between purity estimates derived using pathology , dna , mrna , and microrna ( mirna ) proles and molecular proles ( mrna.naive = bulk mrna abundance , mrna.isopure = deconvolved mrna abundance , mirna.naive = bulk mirna abundance , mirna.isopure = deconvolved mirna abundance , and cna = bulk copy number data ; deconvolved rna proles were generated using isopure )  . 
each feature ( genes for mrna and copy number aberration [ cna ] proles , mirnas for mirna proles ) was correlated with tumor purity estimators ( pathology , dna , rna , mirna ) separately . 
 ( b ) distribution of tumor purity estimates across 13 tcga tumor types ( 4 , 830 tumors ) using an in silico dna - based ( ascat ) and mrna - based ( isopure ) method . 
for clinico - genomic sequencing studies requiring a minimum purity threshold for inclusion in the study , an alternative to pathology estimates is to infer purity directly from the analyte by performing low - pass dna sequencing to lter low - purity samples.22 in addition to poor concordance between pathology and dna / rna - based tumor purity in prostate cancer , our pan - cancer data reported herein suggest that the purity estimates from dna and mrna proles also show limited concordance . 
the concordance between purity estimators also varies depending upon the tumor type and patterns of somatic changes it exhibits ( eg , dna - based methods rely on the presence of copy number aberrations )  . 
furthermore , previous studies have reported varying levels of concordance in purity estimates inferred from dnaand rna - based methods.2 , 23 for instance , aran et al2 show much stronger concordance between estimate24 ( rna - based purity estimator ) and absolute13 ( dna - based purity estimator ) compared with the rnaand dna - based methods in our study . 
because purity estimates vary across methods , consensus estimates on the basis of matched analyte type may further improve purity estimates and may also overcome missing values and normalize outlier estimates . 
after condent purity estimates have been created , one way to account for these is to adjust bioinformatics and statistical analyses for tumor purity , as stressed in previous studies.2 , 7 , 15 because bulk tumor proles are heterogeneous compositions of tumor cells and tacs featuring complex interplay , it is crucial to interpret the clinico - genomic proles in the context of the underlying heterogeneity.25 many in silico deconvolution techniques have been developed to estimate relative abundance of different cell types , 24 , 26 , 27 as well as techniques that transcriptomic11 , 12 , 15 , 18 , 23 and explicitly generate residual genomic14 proles of tumor - only and stromal - only cells . 
herein , we recommend researchers to consider deconvolution of bulk proles into individual component proles ( e.g. , cancer and stromal proles ) to improve sensitivity and specicity of downstream analyses.4 , 15 affiliations 1ontario institute for cancer research , toronto , ontario , canada 2the breast cancer now toby robins research centre , the institute of cancer research , london , united kingdom 3department of data sciences , dana - farber cancer institute , boston , 4department of biostatistics , harvard t.h. 
boutros provision of study material or patients : massimo loda collection and assembly of data : syed haider , svitlana tyekucheva , davide prandi , andrew wei xu , peter w . 
park honoraria : pzer consulting or advisory role : neuroinammation newco patents , royalties , other intellectual property : patent on mutational signature - based detection of homologous recombination deciency peter w . 
laird consulting or advisory role : progenity , anchordx patents , royalties , other intellectual property : received royalties annually through 2018 for inventions licensed to epigenomics ag by usc travel , accommodations , expenses : anchordx wenyi wang stock and other ownership interests : genomic health francesca demichelis patents , royalties , other intellectual property : co - inventor on a patent led by the university of michigan and the brigham and womens hospital covering the diagnostic and therapeutic elds for ets fusions in prostate cancer . 
boutros consulting or advisory role : biosymetrics patents , royalties , other intellectual property : holds patents on multiple biomarkers no other potential conicts of interest were reported . acknowledgment the results published herein are based , in part , upon data generated by tcga pilot project established by the national cancer institute and the national human genome research institute . 
nature 501 : 346 - 354 , 2013 fox ns , haider s , harris al , et al : landscape of transcriptomic interactions between breast cancer and its microenvironment . 
nat commun 10 : 3116 , 2019 smits aj , kummer ja , de bruin pc , et al : the estimation of tumor cell percentage for molecular testing by pathologists is not accurate . 
mod pathol 27 : 168 - 174 , 2014 yadav vk , de s : an assessment of computational methods for estimating purity and clonality using genomic data derived from heterogeneous tumor tissue samples . 
brief bioinform 16 : 232 - 241 , 2015 zheng x , zhang n , wu hj , et al : estimating and accounting for tumor purity in the analysis of dna methylation data from cancer studies . 
wang l , sebra rp , sfakianos jp , et al : a reference prole - free deconvolution method to infer cancer cell - intrinsic subtypes and tumor - type - specic stromal 24 . 
miller , md3 ; and razelle kurzrock , md2 , 5 purpose high - grade neuroendocrine cervical cancer ( hgnecc ) is an uncommon malignancy with limited therapeutic options ; treatment is patterned after the histologically similar small - cell lung cancer ( sclc )  . 
these results were subsequently compared with a cohort of 1 , 800 sclcs . results the median age of patients with hgnecc was 40.5 years ; 83 patients ( 85.6% ) harbored high - risk human papillomavirus ( hpv )  . 
overall , 294 genomic alterations ( gas ) were identied ( median , 2 gas / sample ; average , 3.0 gas / sample , range , 0 - 25 gas / sample ) in 109 distinct genes . 
seventy - one patients ( 73% ) had 1 alteration that was theoretically druggable . comparing hgnecc with sclc , signicant differences in tmb , microsatellite instability , hpv - positive status , and in pik3ca , myc , pten , tp53 , arid1a , and rb1 alteration rates were found . conclusion this large cohort of patients with hgnecc demonstrated a genomic landscape distinct from sclc , calling into question the biologic and therapeutic relevance of the histologic similarities between the entities . furthermore , 73% of hgnecc tumors had potentially actionable alterations , suggesting novel treatment strategies for this aggressive malignancy . jco precis oncol 4 : 972 - 987 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the treatment of solid malignancies has evolved and is perhaps best exemplied by the approach to non small - cell lung cancer , for which molecular characterization and use of targeted agents have emerged as standard therapeutic paradigms . 
recently , the cancer genome atlas ( tcga ) completed and published the integrated genomic and molecular characterization of cervical cancer.1 in addition to data previously released for both ovarian ( high - grade serous ) and endometrial ( endometrioid and serous ) cancers , this publication completed the molecular and genomic evaluation of the most common gynecologic malignancies.2 , 3 traditionally , cervical cancer clinical trials have excluded less common histologies such as high - grade neuroendocrine cervical carcinoma ( hgnecc )  . 
despite the low incidence of hgnecc ( , 2% of all cervical cancers ) the oncologic impact is signicant because these tumors exhibit more aggressive clinical characteristics.4 , 5 unfortunately , the 5 - year overall survival rate for patients with early - stage disease is only a 36% , and those with metastatic spread face an even more dismal prognosis . 
given these poor outcomes , patients with hgnecc represent an area of unmet clinical need . developing therapeutic options for patients with rare tumors is challenging , relying on international collaboration , as well as small case series or retrospective reports rather than prospective clinical trials . 
 genomic landscape of high - grade neuroendocrine cervix cancer context key objective to dene the molecular landscape of high - grade neuroendocrine cervical cancer in a large cohort of patients . knowledge generated high - grade neuroendocrine cervical cancer appears molecularly distinct from the histologically similar small - cell lung cancer . up to 73% of patients samples harbored potentially actionable alterations , informing novel treatment strategies . relevance continued understanding of the molecular underpinnings of high - grade neuroendocrine cervical carcinoma will be critical to driving drug discovery for this disease . approved by the food and drug administration ( fda ) specically for hgnecc.8 recently , 2 reports of exceptional responses to immune checkpoint inhibition in patients with recurrent hgnecc were published.9 , 10 to better understand these responses and to identify molecular aberrations underlying this uncommon malignancy , we examined the genomic landscape of hgnecc . 
the submitting physicians provided specication of a poorly differentiated , neuroendocrine tumor type of cervical origin , which was then independently reviewed by a gynecologic pathologist ( j.e. ) to conrm high - grade neuroendocrine pathologic features in the pathology report and / or the representative sample of tumor submitted for sequencing ( grade 3 cytomorphologic features , some component of small - cell or large - cell carcinoma histology , and / or positivity for neuroendocrine markers )  . 
ngs data were generated by foundationone ( foundation medicine ; cambridge , ma )  . the study was performed in accordance with university of california , san diego , institutional review board guidelines for a de - identied database . 
the test sequences the entire coding region of 182 or , more recently , 236 or 315 cancer - related genes plus up to 47 introns of up to 19 genes often rearranged or altered in cancer to an average depth of coverage of  . 
500.11 the pathologic diagnosis of each case was conrmed on routine hematoxylinand eosin - stained slides and all samples forwarded for dna extraction contained a minimum of 20% tumor nuclear area . 
microsatellite instability ( msi ) status was evaluable in 75 hgnecc and 1 , 573 sclc cases . the sequencing methods used for comprehensive genomic proling have been validated and reported previously ( appendix ) .12 , 13 the optimized loci used to evaluate msi status were selected from a total set of 1 , 897 that have adequate coverage on all versions of the assay . 
there was no need to extend beyond the rst principal component , because it explained approximately 50% of the total data variance , whereas none of the other principal components explained  . 
msi - low calls are not made because there was no gold - standard test set , but we presume such samples would signicantly overlap with the msiambiguous category reported here . 
the cutoff of 20 coding mutations / mb is approximately equal to 400 nonsynonymous mutations per exome.15 human papillomavirus detection in addition , the presence of high - risk human papillomavirus ( hpv ) was examined in submitted specimens , as previously reported.16 hybrid - capture reagents included baits designed to capture unique regions of select viral genomes including hpv - 16 and - 18 . 
a total hpv - 16 / 18 aligned read count of 5 reads per million was considered a positive hpv status , and , 5 reads per million was considered hpv not detected.16 end points and statistical methods descriptive statistics were used to summarize the baseline patient characteristics . 
all statistical tests were carried out using graphpad prism , version 6.0 ( graphpad software , san diego , ca )  . results characterization of gas in hgnecc the median age of the cohort was 40.5 years ( range , 25 - 77 years )  . 
the most frequently reported number of gas per sample was 2 , with a range of 0 - 25 ( average , 3.0 gas / sample ; fig 2 )  . 
5% of samples are depicted . variants of unknown signicance excluded . genomics in hpv - positive versus - negative patients when examining distribution of gas on the basis of hpv detection status , a signicant difference was identied in the frequency of several gas , including pik3ca , tp53 , pten , arid1a , and rb1 , all of which were more frequent in the hpv - negative subgroup ( table 1 )  . 
two of the 3 cases were both msi - h and tmb - h and harbored the highest numbers of identiable gas in the cohort.17 , 18 the third case , with a nonsense mutation near the 3 ( cid : 3 ) end of the coding sequence ( msh2 r929 * ) , was mss and tmb - l . the 2 msh - 2mutant msi - h cases were both of small - cell histology and accounted for all msi - h cases out of the 75 no . 
furthermore , a total of 40 patient samples ( 41.2% ) harbored mutations in the pi3k / akt / mtor pathway ; mutations in pik3ca were identied in 47.5% of these samples ( n = 19 ) , and pten mutations were reported in 35% ( n = 14 )  . 
the small - cell subset of hgnecc samples showed analogous gene mutation differences from sclc . discussion neuroendocrine carcinoma is an uncommon but aggressive variant accounting for approximately 1.5% of all newly diagnosed cervical cancers.20 the great majority of these lesions are high - grade largeor small - cell subtypes , with only rare reports of well - differentiated cervical carcinoid tumors.20 the treatment of patients with hgnecc remains table 2 . 
 eskander et al clinically challenging , with limited response rates to chemotherapy ; however , anecdotal reports of exceptional responders have been described.9 , 10 the paradigm for management of hgnecc has been informed by the treatment of the more commonly diagnosed ( and histologically similar ) sclc , which accounts for approximately 15% of all lung cancer cases . 
in prior studies , whole - genome sequencing of 110 sclc specimens identied essentially ubiquitous tp53 and rb1 inactivating mutations , with biallelic losses of each gene respectively in 100% and 93% of cases without chromothripsis.21 in an effort to better dene the molecular landscape of hgnecc , we evaluated the comprehensive genomic proling of 97 patient samples . 
at least 1 characterized alteration was identied in 88 patient samples ( 90.7% ) and of these , 72 had a potentially pharmacologically tractable alteration . interestingly , the frequency and distribution of gas identied in this cohort of patients are similar and distinct from mutational patterns described in the more common hpvrelated cervical cancer histologies.1 as detailed in tcgas integrated genomic characterization of cervical cancer ( ie , squamous , adenocarcinoma , and adenosquamous histologies ) , mutations in the pik3ca gene were the most frequently identied aberration , occurring in 26% of samples , approximating the nearly 20% rate in our cohort . in addition , signicantly mutated genes reported by the tcga , identied in similar proportions in this patient cohort , included arid1a ( 7% in tcga and 9.3% in our cohort ) and kras ( 6% in tcga and 8.2% in our cohort )  . 
these molecular differences may be reective of the varying histologies or , potentially , the differential highrisk hpv detection rates ( 85.6% in our cohort v 95% in the tcga ) .1 importantly , the high - risk hpv rate in our cohort should be interpreted with caution because the assay used has not undergone formal concordance study with gold standard tests such as hybrid capture and can detect only hpv 16 / 18 . our own , much larger cohort of sclc samples ( n = 1 , 800 ) recapitulates prior studies and had a strikingly different molecular portfolio when compared with hgnecc samples . 
msi - h status was also more common in the hgnecc cohort whereas tmb - i / tmb - h was more common in sclc ( despite the lack of msi - h status )  . 
the use of everolimus , or an alternate mtor or pik3ca inhibitor , may be considered in such circumstances , although the utility of a pik3ca mutation in predicting response to single - agent everolimus in the presence of multiple gas remains limited.26 , 27 although less frequently identied , alterations in the hrd pathway were detected in 9.3% of patient samples , potentially supporting use of a poly - adp ribose polymerase inhibitor . 
the identication of both tmb - h ( n = 2 ) and gas in mismatch repair genes ( n = 3 ) may also inform the use of immune checkpoint inhibition.28 in may 2017 , the fda approved pembrolizumab for the treatment of mismatch repairdecient or msi - h solid tumors that progressed after prior therapy . 
more recently , the fda accepted and granted priority review to a supplemental biologics license application for pembrolizumab for the treatment of adult and pediatric patients with unresectable or metastatic solid tumors with tissue tmb - h whose disease has progressed after prior treatment and who have no satisfactory alternative treatment options , supported by data from the phase ii keynote - 158 trial . 
notably , there are 2 published case reports of patients with recurrent , treatment - refractory hgnecc with exceptional and durable responses to checkpoint inhibition ; 1 of these tumors was from our current hgnecc cohort and had a mismatch repair defect and the other lacked correlative genomic testing.9 , 10 last , the identication of arid1a ( 9.3% ) and smarca4 ( 4.1% ) mutations may predict sensitivity to an alternate therapeutic strategy.29 homeostasis requires balanced arid1a and ezh2 activity , facilitated via chromatinmediated gene expression . 
 genomic landscape of high - grade neuroendocrine cervix cancer aberrations were identied in patients with msi - h lesions , possibly reecting that the smarca4 may be a passenger mutation resulting from the underlying msi . 
furthermore , of the 4 cases with smarca4 alterations , 1 was hpv - 18 positive and another was p16 positive by immunohistochemical assessment . despite the large sample size and robust genomic data , this study has limitations . 
95% of the identied high - risk hpv strains.30 this report highlights the potential therapeutic utility of genomic testing in patients with this uncommon disease.27 interest , despite the histologic similarity between hgnecc and sclc , which has led to the latter being used as a model for treating the former , the molecular portfolio of these 2 entities is strikingly different . 
therefore , plausible that patients with hgnecc may benet from alternative therapeutic strategies . it is not anticipated that traditional prospective trials will accrue sufcient patient numbers in this disease setting , and novel study designs , including umbrella , basket , and platform trials , should be considered given the presence of actionable targets . 
interestingly , the rst reported cohort of the dart trial ( clinicaltrials.gov identier : nct02834013 ) 31 was the neuroendocrine cohort , with a 44% overall response rate in those with high - grade disease . 
eskander consulting or advisory role : pzer , clovis oncology , astrazeneca / medimmune , tesaro , merck speakers bureau : clovis oncology , astrazeneca / medimmune , roche travel , accommodations , expenses : clovis oncology , astrazeneca / medimmune , roche , merck , pzer julia elvin employment : foundation medicine stock and other ownership interests : hoffman - laroche laurie gay employment : foundation medicine , invitae stock and other ownership interests : foundation medicine , naveris , invitae consulting or advisory role : invitae , naveris jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : celsius therapeutics research funding : foundation medicine vincent a . 
 eskander et al leadership : foundation medicine , revolution medicines stock and other ownership interests : foundation medicine , mirati therapeutics , revolution medicines patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center razelle kurzrock leadership : curematch , curemetrix stock and other ownership interests : curematch , idbydna , soluventis honoraria : roche , eusa pharma , neogenomics laboratories , biocom , neomed therapeutics , advanced therapeutics , lek , aacr , chugai pharma usa , wiley consulting or advisory role : actuate therapeutics , loxo , xbiotech , neomed , roche , gaido , soluventis , pzer , merck speakers bureau : roche , guardant health ( inst ) research funding : sequenom ( inst ) , merck serono ( inst ) , genentech ( inst ) , pzer ( inst ) , foundation medicine ( inst ) , incyte ( inst ) , konica minolta ( inst ) , grifols ( inst ) , omniseq ( inst ) , debiopharm group ( inst ) , boerhinger ingelheim ( inst ) travel , accommodations , expenses : roche , eusa pharma , neogenomics laboratories , biocom , neomed therapeutics , advanced therapeutics , lek , aacr , chugai pharma usa , wiley no other potential conicts of interest were reported . references cancer genome atlas research network : integrated genomic and molecular characterization of cervical cancer . 
nature 497 : 67 - 73 , 2013 [ erratum : nature 500 : 242 , 2013 ] cancer genome atlas research network : integrated genomic analyses of ovarian carcinoma . 
nature 474 : 609 - 615 , 2011 [ erratum : nature 490 : 298 , 2012 ] gardner gj , reidy - lagunes d , gehrig pa : neuroendocrine tumors of the gynecologic tract : a society of gynecologic oncology ( sgo ) clinical document . gynecol oncol 122 : 190 - 198 , 2011 satoh t , takei y , et al : gynecologic cancer intergroup ( gcig ) consensus review for small cell carcinoma of the cervix . 
int j gynecol cancer 24 : s102 - s108 , 2014 ( 9 suppl 3 ) fukuoka m , masuda n , furuse k , et al : a randomized trial in inoperable non - small - cell lung cancer : vindesine and cisplatin versus mitomycin , vindesine , and cisplatin versus etoposide and cisplatin alternating with vindesine and mitomycj clin oncol 9 : 606 - 613 , 1991 kubota k , hida t , ishikura s , et al : etoposide and cisplatin versus irinotecan and cisplatin in patients with limited - stage small - cell lung cancer treated with etoposide and cisplatin plus concurrent accelerated hyperfractionated thoracic radiotherapy ( jcog0202 ) : a randomised phase 3 study . 
lancet oncol 15 : 106 - 113 , 2014 ishikawa m , kasamatsu t , tsuda h , et al : prognostic factors and optimal therapy for stages i - ii neuroendocrine carcinomas of the uterine cervix : a multi - center retrospective study . 
gynecol oncol 148 : 139 - 146 , 2018 paraghamian se , longoria tc , eskander rn : metastatic small cell neuroendocrine carcinoma of the cervix treated with the pd - 1 inhibitor , nivolumab : a case report . 
sharabi a , kim ss , kato s , et al : exceptional response to nivolumab and stereotactic body radiation therapy ( sbrt ) in neuroendocrine cervical carcinoma with high tumor mutational burden : management considerations from the center for personalized cancer therapy at uc san diego moores cancer center . oncologist 22 : 631 - 637 , 2017 11 . 
ross js , fakih m , ali sm , et al : targeting her2 in colorectal cancer : the landscape of amplication and short variant mutations in erbb2 and erbb3 . 
genome med 9 : 34 , 2017 johnson db , frampton gm , rioth mj , et al : targeted next generation sequencing identies markers of response to pd - 1 blockade . 
chae yk , pan ap , davis aa , et al : path toward precision oncology : review of targeted therapy studies and tools to aid in dening actionability of a molecular lesion and patient management support . 
kato s , kurasaki k , ikeda s , et al : rare tumor clinic : the university of california san diego moores cancer center experience with a precision therapy 25 . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecularp : results from mypathway , an openlabel , phase iia multiple basket study . 
j clin oncol 36 : 536 - 542 , 2018 janku f , hong ds , fu s , et al : assessing pik3ca and pten in early - phase trials with pi3k / akt / mtor inhibitors . 
alejo m , alemany l , clavero o , et al : contribution of human papillomavirus in neuroendocrine tumors from a series of 10 , 575 invasive cervical cancer cases . pract 4 : 17 , 2017 papillomavirus res 5 : 134 - 142 , 2018 31 . 
patel sp , othus m , chae yk , et al : a phase ii basket trial of dual anti - ctla - 4 and anti - pd - 1 blockade in rare tumors ( dart ) s1609 : the neuroendocrine cohort . presented at the american association for cancer research annual meeting , atlanta , ga , march 29 - april 3 , 2019 ( abstr ct039 )  . 
briey , after pathologic review to conrm sufcient tumor nuclei ( minimum , 20% ) and mitigate pathologic inconsistencies , at least 50 ng of dna was extracted from 40 tumor samples provided as formalin - xed , parafnmicrons of embedded tissue blocks . 
the samples were assayed using adaptorligation and hybrid - capture next - generation sequencing ( foundationone ) for all coding exons from 182 ( version 1 ) , 287 ( version 2 ) , or 315 ( version 3 ) cancer - related genes plus selected introns from 14 ( version 1 ) , 19 ( version 2 ) , or 28 ( version 3 ) genes frequently rearranged in cancer . sequencing of captured libraries was performed using hisequation 2500 / 4000 ( illumina , san diego , ca ) to a mean exon coverage depth of  . 
500 , and resultant sequences were analyzed using both an algorithmic pipeline and manual curation for base substitutions , small insertions or deletions ( indels ) , copy number alterations ( focal amplications and homozygous deletions ) , and selected gene fusions , as previously described.13 clinically relevant genomic alterations were dened as alterations targetable by anticancer drugs currently available on the market or in registered clinical trials . 
germline variants documented in the dbsnp database ( dbsnp142 ; nlm.nih.gov / snp / ) , with 2 counts in the exac database ( broadinstitute.org / ) , or recurrent variants of unknown signicance that were predicted by an internally developed algorithm to be germline were removed , with the exception of known driver germline events.12 known , conrmed somatic alterations deposited in the catalog of somatic mutations in cancer ( version 62 ) were highlighted as biologically signicant , as were inactivating events in tumor suppressor genes . 
 o majority of b2m - mutant and - decient colorectal carcinomas achieve clinical benet from immune checkpoint inhibitor therapy and are microsatellite instability - high sumit middha , phd1 ; rona yaeger , md1 ; jinru shia , md1 ; zsoa k . 
hechtman , md1 purpose microsatellite instability - high ( msi - h ) colorectal carcinomas ( crcs ) show high rates of response to immune checkpoint inhibitors ( ios )  . 
all b2m - mutant crcs were assessed for expression of b2m , major histocompatibility complex class i , and programmed death - 1 ligand ( pd - l1 ) via immunohistochemistry and average cd3 + and cd8 + tumor - inltrating lymphocyte counts against a control group of msi - h b2m wild - type crcs . results fifty - nine ( 3.4% ) of 1 , 751 patients with crc harbored b2m mutations , with 84% ( 77 of 92 ) of the mutations predicted to be truncating . 
b2m mutation status was not associated with major histocompatibility complex class i expression , kras or braf mutation , tumor - inltrating lymphocyte level , or pd - l1 expression after adjustment for msi status . 
of 13 patients with b2m - mutant crc who received programmed death - 1 or pd - l1 ios , 11 ( 85% ) achieved clinical benet , dened as stable disease or partial response using response evaluation criteria in solid tumors criteria . conclusion b2m mutations occur in approximately 24% of msi - h crcs and are usually associated with loss of b2m expression . 
 middha et al context do b2m - mutant and decient colorectal carcinomas ( crcs ) respond to immune checkpoint inhibitors ? we found that b2m mutations are enriched in microsatellite instability - high crc , that these mutations commonly occur at coding microsatellite loci , and that these b2m mutations are truncating and associated with loss of b2m expression . 
of 13 patients with b2m - mutant crc and available recist data , six achieved stable disease , ve achieved partial response , and one experienced pseudoprogression . b2m mutations are not predictive of primary resistance to immune checkpoint inhibition in crc . administrationcleared , next - generation sequencing assay that interrogates  . 
presence of loss of heterozygosity ( loh ) was assessed via allelespecic copy - number analysis using the fraction and allelespecic copy number estimates from tumor sequencing ( facets ) algorithm14 and , in cases of low tumor content , via comparison of b2m mutation variant allele frequency against median variant allele frequency . 
clinical parameters , clinical response to immune checkpoint inhibitor therapy all patients with crc with msk - impact data and b2m mutations who underwent therapy with immune checkinhibitors ( ios ; durvalumab , nivolumab , or pempoint brolizumab ) before july 2018 were assessed for b2m expression ( ihc ) , response , stable disease ( sd ) , and progressive disease ( pd )  . 
formal response evaluation criteria in solid tumors ( recist ) scores were assessed via radiologic data as follows : complete response ( cr ) , disappearance of all target lesions , conrmed at 4 weeks ; partial response ( pr ) , 30% decrease , conrmed at 4 weeks ; pd , 20% increase over smallest sum observed ; and sd , meeting none of the other criteria . patients were deemed to have experienced clinical benet from ios if recist results were sd , pr , or cr . ihc staining for b2m using a polyclonal antibody with concentration of 1 : 6 , 000 ( catalog #a0072 ; dako , santa clara , ca ) , mhc class i using a monoclonal antibody with concentration of 1 : 200 ( catalog #14 - 9958 ; e - bioscience , carlsbad , ca ) , cd3 using a monoclonal antibody with concentration of 1 : 200 ( catalog #ncl - l - cd3 - 565 ; leica , lincolnshire , il ) , cd8 using a monoclonal antibody with concentration of 1 : 100 ( catalog #m7103 ; dako ) , and pd - l1 using a monoclonal antibody with concentration of 1 : 100 ( catalog #13684 ; cell signaling , danvers , ma ) was performed on all crcs with b2m mutations with available tissue as well as a set of 26 randomly selected wild - type ( wt ) crcs with in - house resection specimens and mskimpact testing ( performed between january 1 , 2014 , and october 31 , 2017 ) that were matched to the b2m - mutant group for prevalence of msi status . 
complete loss of b2m on ihc ( 0% of tumor cells with b2m expression ) was interpreted as loss of b2m expression . statistical analyses associations were assessed using pearsons 2 test with simulated p value based on 2 , 000 replicates for low count data . 
a cox proportional hazards model was tted to the data to calculate survival using the covariates of b2m mutation status , age at diagnosis , pathologic stage , msi status , proximal versus distal status , and kras , nras , braf , and pik3ca mutation status . 
these were each assessed through both univariable and multivariable cox regressions . r survival and survminer software packages were used to perform this analysis ( r foundation , vienna , austria )  . results molecular findings we rst sought to determine the spectrum of b2m mutations in a cohort of patients with crc ( n = 1 , 751 ) with msk - impact data ( appendix fig a1 )  . 
next , we classied the samples on the basis of whether they were microsatellite stable ( mss ) or unstable ( msi - h ) on the basis of genomic data . 
a medullary carcinoma of the colon shows immune - cell expression of programmed death - 1 ligand at the tumor - stroma interface , loss of b2m expression in tumor cells , retention of strong diffuse mhc class i expression in tumor cells ,  . 
twelve samples showed either loh or copy - neutral loh along with a clonal mutation , suggesting biallelic loss . b2m expression , mhc class i expression , and til level to evaluate the functional outcome of b2m mutations , we examined protein expression in samples with available tissue ( figs 1b and 1c ; appendix table a2 )  . 
because pdl1 status has been used as a predictive marker of ios and linked to expression of mhc class 1 , we performed pd - l1 ihc in available b2m - mutant and wt patient cases . 
thirtytwo ( 73% ) of 44 b2m - mutant and 13 ( 50% ) of 26 b2m wt crcs were positive for pd - l1 expression ( immune cells in tumor - stroma interface )  . 
average median cd3 + count per hpf was 22.3 in b2m - mutant and 37.3 in b2m wt crcs , whereas average median cd8 + count per hpf was 15.1 and 49 for b2m - mutant and b2m wt crcs , respectively . 
in comparison with b2m wt crcs matched for msi status , b2m - mutant crcs tended to have lower average levels of cd3 and cd8 per patient case ( fig 2a ) , these differences did not reach statistical significance . 
age , stage , and kras , nras , and braf status were associated with os , whereas pik3ca mutation status , msi status , and proximal versus distal location were not associated with os ( fig 2b ; appendix table a2 )  . response to immunotherapy because b2m mutations were identied as a possible resistance mechanism for checkpoint inhibition , we identied 13 ( msi - h , n = 11 ; mss , n = 2 ) patients with crc with b2m mutations who subsequently received io therapy , and we evaluated their response to treatment . 
 ( a ) box plot graphs of average cd3 ( left ) and cd8 ( right ) counts in b2m - mutant vs wild - type ( wt ) colorectal carcinoma ( crc ) show that median average cd3 and cd8 trend toward higher values in b2m wt carcinoma . ( b ) multivariable model showing the clinical variables associated with os of patients with crc in our cohort . 
analysis of their tumor response by recist criteria demonstrated pr in ve patients , sd in six patients , and pd in one patient , likely pseudoprogression ( fig 3a ; appendix table a3 )  . 
this response rate is in line with recent publications of ios in msi - h crc.8 , 9 of the two patients with mss tumors , one had an ultramutated pole hotspot mutated tumor and experienced tumor growth with io treatment but was able to continue treatment for 1 year , likely to be pseudoprogbecause growth was thought ression , and the other patient had sd during treatment with a combination of io treatment and targeted therapy ( after progression with targeted therapy alone )  . 
the association of b2m mutations with complete loss of expression on whole sections of pole s459f best response pseudoprogression partial response stable disease treatment stopped ongoing 40% 80% msi status io therapy b2m expression fig 3 . 
immune checkinhibitor ( io ) repoint sponse in b2m - mutant colorectal cancer ( crc )  . waterfall plot of io response in b2m - mutant crc ( colored by microsatellite instability [ msi ] status , type of b2m mutation , and type of io received )  . 
indeed , in the 42 b2m - mutant crcs analyzed by facets , 60% had evidence of either two clonal b2m mutations or one clonal b2m mutation and loh ( appendix table a1 )  . 
it is possible that the remaining b2m - mutant crcs have epigenetic modications as a mechanism of b2m silencing . unlike previous studies , 3 we found that b2m protein loss is not correlated with loss of mhc class i expression . 
we show that b2m mutation and loss do not correlate with mhc class i loss of expression , although the effect of b2m loss on the functional competence of mhc class i is known to be deleterious.16 limitations to our study include the retrospective analysis and relatively small number of patients treated with ios , as well as limitations in molecular testing for epigenetic issues and allele specicity of b2m mutations . most importantly , our study shows that b2m mutation and loss in immunotherapy - naive crc do not predict primary resistance to ios . 
we saw that most patients had some degree of regression with treatment ; larger , prospective studies are needed to clarify if the response rate and duration of response vary by b2m mutation status . however , our data indicate that patients with crc whose tumors harbor b2m mutations should not be excluded from io treatment . 
the clinical benet demonstrated in patients with b2m - decient crc who received ios may have resulted from the fact that despite b2m loss , there was still evidence of functional neoantigen recognition , as indicated by the high number of tils ( median , 22.3 per hpf ) still present in b2m - decient msi - h crc . 
 middha et al leonard saltz consulting or advisory role : mcneil ( i ) research funding : taiho pharmaceutical neil segal consulting or advisory role : bristol - myers squibb , pzer , astrazeneca / medimmune , imugene , roche / genentech , pieris pharmaceuticals , synlogic , aduro biotech , kyn therapeutics , boehringer ingelheim , merck , puretech , horizon pharma , emd serono , gritstone oncology , chugai pharma , trm oncology , ifm therapeutics , psioxus therapeutics research funding : medimmune , bristol - myers squibb , pzer , roche / genentech , merck , incyte marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso rfp advisory committee , takeda pharmaceuticals , bristol - myers squibb , bayer healthcare pharmaceuticals , merck ( i ) research funding : loxo ( inst ) , helsinn therapeutics ahmet zehir no relationship to disclose jaclyn f . 
hechtman honoraria : medscape consulting or advisory role : navigant consulting , axiom biotechnologies research funding : bayer no other potential conicts of interest were reported . references roberts ad , ordway dj , orme im : listeria monocytogenes infection in beta 2 microglobulin - decient mice . 
infect immun 61 : 1113 - 1116 , 1993 schaible ue , collins hl , priem f , et al : correction of the iron overload defect in beta - 2 - microglobulin knockout mice by lactoferrin abolishes their increased susceptibility to tuberculosis . 
j exp med 196 : 1507 - 1513 , 2002 sade - feldman m , jiao yj , chen jh , et al : resistance to checkpoint blockade therapy through inactivation of antigen presentation . 
nat commun 8 : 1136 , 2017 janikovits j , m uller m , krzykalla j , et al : high numbers of pdcd1 ( pd - 1 ) - positive t cells and b2m mutations in microsatellite - unstable colorectal cancer . oncoimmunology 7 : e1390640 , 2017 grasso cs , giannakis m , wells dk , et al : genetic mechanisms of immune evasion in colorectal cancer . 
cancer discov 8 : 730 - 749 , 2018 le dt , uram jn , wang h , et al : pd - 1 blockade in tumors with mismatch - repair deciency . 
n engl j med 372 : 2509 - 2520 , 2015 riaz n , havel jj , makarov v , et al : tumor and microenvironment evolution during immunotherapy with nivolumab . 
cell 171 : 934 - 949.e16 , 2017 le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - decient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
clendenning m , huang a , jayasekara h , et al : somatic mutations of the coding microsatellites within the beta - 2 - microglobulin gene in mismatch repairdecient colorectal cancers and adenomas . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
consort diagramutation and immunohistochemistry analyses included data from 1 , 751 patients with colorectal cancer ( crc ) with memorial sloan kettering integrated mutation proling of actionable cancer targets testing . 
 comparative rna - sequencing analysis benefits a pediatric patient with relapsed cancer clinical detection of sequence and structural variants in known cancer genes points to viable treatment options for a minority of children with cancer.1 to increase the number of children who benefit from genomic profiling , gene expression information must be considered alongside mutations.2 , 3 although high expression has been used to nominate drug targets for pediatric cancers , 4 , 5 its utility has not been evaluated in a systematic way.6 we describe a child with a rare sarcoma that was profiled with whole - genome and rna sequencing ( rna - seq ) techniques . 
although the tumor did not harbor dna mutations targetable by available therapies , incorporation of gene expression information derived from rna - seq analysis led to a therapy that produced a significant clinical response . 
histology revealed a mitotically active , epithelioid - to - spindled cell tumor in patternless sheets , interrupted by thick fibrous bands and foci of necrosis ( figs 1c to 1d )  . 
focal immunohistochemical positivity was observed for pan - cytokeratin ( ae1 / ae3 ) and synaptophys the tumor was negative for glial fibrillary acidic protein ( gfap ) , wilms tumor 1 ( wt1 ) , myo - d1 , myogenin , smooth muscle actin , nonphosphorylated and phosphorylated neurofilament protein , cd34 , cd31 , hmb - 45 , s - 100 , leukocyte common antigen , and baf47 / ini - 1 ( retained nuclear positivity )  . 
a diagnosis of desmoplastic small round cell tumor ( dsrct ) was favored initially.7 because ewsr1 breakapart fluorescence in situ hybridization confirmed an ewsr rearrangement but concomitant wt1 breakapart fluorescence in situ hybridization was negative , the molecular criterion for dsrct was not met , and a final diagnosis of poorly differentiated sarcoma , not otherwise specified , was rendered . 
the patient received six cycles of induction chemotherapyifosfamide , carboplatin , and etoposidefollowed by autologous stem - cell transplantation with a high - dose preparative regimen of carboplatin , thiotepa , and etoposide as well as 54 gy of focal radiation to the location of the original tumor . 
we compared the rna - seqderived tumor gene expression profile of patient 1 with similarly derived profiles of 10 , 668 samples that represented 38 pediatric and adult tumor types studied by the the cancer genome atlas ( tcga ) and therapeutically actionable research to generate effective treatments ( target ) .11 , 12 rna - seq reads from different laboratories were reanalyzed with a single computational pipeline to reduce batch effects.13 we searched for tumors in this homogeneously processed compendium in which expression profiles were similar to those of patient 1 by using tumormap.14 the tumor gene expression profile for patient 1 resembled lung cancers ( fig 2a ) , the site of the metastasis . 
lung adenocarcinoma ( luad ) samples formed four groups in the tumormap ( fig 2b ) and the sarcoma of patient 1 clustered with the 354 luad tumors of the terminal respiratory unit and proximal - inflammatory molecular subtype ( fig 2c ) , associated with the activation of receptor tyrosine kinases ( rtk ) .15 to define the transcriptional programs that drove placement of the patients tumor with the lung cancers , we conducted gene set enrichment analysis16 with genes differentially expressed between the luad cluster that contained the tumor of patient 1 ( n = 354 ) and the remaining samples in the compendium ( n = 10 , 314 ) ; we also repeated this analysis and compared the cluster for patient 1 with the remaining luad samples ( n = 529 )  . 
both analyses revealed the overexpression of members of the il6 / jak / stat3 signaling pathway ( appendix fig a2 ) , which suggests that the activation of shared signaling programs likely contributed to the tumor transcriptional phenotype of patient 1 in addition to the site of the metastatic sample . 
we next searched for genes that were significantly overexpressed in the patients tumor compared with the whole compendium and compared with only the sarcomas by using outlier statistics3 , 17 ( data supplement )  . 
consolidating the fusion - based and the rtk - based mechanisms of il6 / jak / stat3 activation , we reconstructed a candidate pathway driving patient 1s cancer ( fig 3 , appendix fig a4 )  . 
a decision was made to use ruxolitinib given ( 1 ) the over - expression of atf1 target genes , ( 2 ) the over - expression of jak1 , and ( 3 ) the available pediatric dosing information.20 in addition , ruxolitinib was favored over crizotinib because it targets downstream of both ewsr1 - atf1 and the over expressed rtks , whereas crizotinib only targets the rtks . 
t2 - weighted coronal sequence revealed a large , primarily hyperintense tumor that arises from the ventral aspect of the left tentorium , invaginating into the superior aspect of the cerebellum and causing diffuse edema there ( b ) preoperative mri . 
 higher magnification depicts epithelioid tumor cells ( eg , long arrow ) and a mitotic figure ( short arrow ) ; many of the tumor cells exhibit somewhat vacuolated cytoplasm ( h&e ; 400 magnification )  . 
diffuse membranous immunostaining is appreciated for ( g ) epithelial membrane antigen ( ema ) , and ( h ) cd99 ( all photomicrographs taken at 200 magnification )  . lethargy , was mostly bed - ridden , and had a lansky play - performance score21 of 60 ( fig 4 )  . 
the patient tolerated this therapy without significant toxicity and had stabilization of the previously rapidly growing lung nodules by recist , 22 and his lansky score improved to 90 to 100 for 5 months . 
 a patient 1 's tumor rna - seq prole in the context of 38 tumor types lung adenocarcinoma lung adenocarcinoma molecular subtypes : proximal proliferative proximal - inammatory terminal respiratory unit patient 1 patient 1 cluster patient 1 lung adenocarcinoma lung squamous cell carcinoma acute lymphoblastic leukemia acute myeloid leukemia adrenocortical cancer bladder urothelial carcinoma brain lower grade glioma breast invasive carcinoma cholangiocarcinoma cervical & endocervical cancer colon adenocarcinoma diffuse large b - cell lymphoma esophageal carcinoma pathology test data , multiple tumor types glioblastoma multiforme head & neck squamous cell carcinoma kidney chromophobe kindney clear cell carcinoma kidney papillary cell carcinoma liver hepatocellular carcinoma lung adenocarcinoma lung squamous cell carcinoma mesothelioma neuroblastoma ovarian serous cystadenocarcinoma pancreatic adenocarcinoma pheochromocytoma & paraganglioma prostate adenocarcinoma rhabdoid tumor rectum adenocarcinoma sarcoma skin cutaneous melanoma stomach adenocarcinoma testicular germ cell tumor thymoma thyroid carcinoma uterine carcinosarcoma uterine corpus endometrioid carcinoma uveal melanoma wilms tumor fig 2 . 
 ( c ) a zoomed - in view of the cluster for patient 1 and the surrounding area that contains luad tumors , now colored according to luad molecular subtypes ( proximal proliferative , blue ; proximal inflammatory , green ; terminal repiratory unit , red )  . 
the family requested that ruxolitinib be restarted for quality of life , and the patient again showed dramatic improvement in clinical status and an unexpected prolonged period of stable disease until dose reduction because of myelosuppression was required . 
 ( a ) candidate pathway that drove tumorigenesis in patient 1 was reconstructed on the basis of outlier analysis , differential expression analysis compared with normal tissues , copy number information , and literature mining ( appendix methods )  . 
all gene expression outliers depicted in the figure ( gene names written in red font ) were significant in all three comparisons : patient 1 versus all cancers , patient 1 versus lung adenocarcinomas , and patient 1 versus sarcomas . 
 ( b ) the tumor in patient 1 expresses jak1 at a strikingly higher level than those seen in all 10 , 668 tumors , which are represented by 38 tumor types studied by the tcga11 and target ( denoted pancan ) , 12 including lung adenocarcinomas ( luads ) and sarcomas ( sarcs )  . 
 ( c ) jak1 is an attractive molecular target for patient 1s tumor because it is downstream of the ewsr1 - atf1 fusion and the activate receptor tyrosine kinases ( rtks )  . 
previous functional studies implicated stat3 as an oncogene in sarcomas25 ; the current case report builds on this work and prompts investigation into the potential clinical utility of targeting this pathway . 
of note was the patients marked and rapid clinical response to treatment , which suggests that response may have been related to the modulation of cytokine expression by the medication . 
ultimately , a randomized clinical trial is necessary to assess the benefit of molecular approaches compared with the standard of care . the case also highlights tumor heterogeneity : although the majority of the metastases remained stable , one lesion rapidly became resistant . 
during treatment , the patients status improved significantly according to both body weight and lansky play performance score , which reached normal levels ; thus , the ruxi dose was increased to 60 mg twice per day at day 29 . 
 ruxi was restarted at day 348 , and a response again was noted according to both body weight and lansky performance score . ruxi at 60 mg twice daily ruxi at 40 mg twice daily ruxi stopped ; progression lansky weight ruxi stopped ruxi at 40 mg twice daily time ( days ) a serial molecular analysis of the heterogeneous lesions could inform the mechanisms of resistance ; however , it was not pursued because of the familys wishes . 
rod rassekh no relationship to disclose yaoqing shen no relationship to disclose martin jones no relationship to disclose chris dunham no relationship to disclose stephen yip no relationship to disclose sreeja leelakumari no relationship to disclose jing zhu no relationship to disclose duncan mccoll no relationship to disclose teresa swatloski no relationship to disclose sofie r . 
mungall no relationship to disclose david haussler no relationship to disclose janessa laskin honoraria : boehringer ingelheim , roche canada , astrazeneca , pfizer research funding : astrazeneca ( inst ) , roche canada ( inst ) steven j.m. 
stuart stock and other ownership interests : five3 genomics patents , royalties , other intellectual property : pending patent on creb1 inhibition for treatment of metastatic prostate cancer colleen jantzen no relationship to disclose we thank the patients family and all of our patient families for their support . 
we thank the bc cancer foundation , alex 's lemonade stand foundation for childhood cancer research , the team finn foundation , the california initiative to advance precision medicine , unravel pediatric cancer , team g childhood cancer foundation , and the st baldricks foundation . 
we thank poul sorensen , md , phd , for his assistance with the fluorescence in situ studies and charles vaske , phd , for manuscript review . affiliations yulia newton , jingchun zhu , duncan mccoll , teresa swatloski , sofie salama , david haussler , joshua m . 
stuart , and olena morozova , university of california santa cruz genomics institute ; sofie salama and david haussler , howard hughes medical institute , university of california , santa cruz , ca ; s . 
lee , and colleen jantzen , british columbia childrens hospital and british columbia children 's hospital research institute ; stephen yip , tony ng , and janessa laskin , british columbia cancer ; and yaoqing shen , martin jones , sreeja leelakumari , yussanne ma , richard moore , andrew j . 
marra , canada 's michael smith genome sciences centre , british columbia cancer , vancouver , british columbia , canada . supported by the bc cancer foundation , an alex 's lemonade stand foundation for childhood cancer innovation grant , the team finn foundation , the california initiative to advance precision medicine , unravel pediatric cancer , the team g . 
is supported by the canada research chairs program and the cihr ( fdn - 143288 )  . presented at the american association for cancer research advances in pediatric cancer research conference , november 9 - 12 , 2015 , fort lauderdale , fl . support prior presentation references 1 . 
laskin j , jones s , aparicio s , et al : lessons learned from the application of whole - genome analysis to the treatment of patients with advanced cancers . 
le rhun e , chamberlain mc , zairi f , et al : patterns of response to crizotinib in recurrent glioblastoma according to alk and met molecular profile in two patients . 
xu j , gong b , wu l , et al : comprehensive assessments of rna - seq by the seqc consortium : fda - led efforts advance precision medicine . 
neder l , scheithauer bw , turel ke , et al : desmoplastic small round cell tumor of the central nervous system : report of two cases and review of the literature . 
loh ml , tasian sk , rabin kr , et al : a phase 1 dosing study of ruxolitinib in children with relapsed or refractory solid tumors , leukemias , or myeloproliferative neoplasms : a childrens oncology group phase 1 consortium study ( advl1011 )  . 
 appendix online methods reference compendium we obtained the cancer genome atlas ( tcga ) 11 and therapeutically applicable research to generate effective treatments ( target ) 12 rna sequencing fragments per kilobase of transcript per million mapped reads ( fpkm12 ; trapnell c , et al : natl biotechnol 28 : 511 - 515 , 2010 ) gene expression data from the public data hub in the university of california santa cruz xena browser ( vivian j , et al : nat biotechnol 35 : 314 - 316 , 2017 ; goldman m , et al : nucleic acids res 43 : d812 - d817 , 2015 )  . 
the tcga and target data sets were processed with the same rna - seq pipeline ( star2 [ dobin a , et al : bioinformatics 29 : 15 - 21 , 2013 ] and rsem [ li b , et al : bmc bioinformatics 12 : 323 , 2011 ] ) by the university of california santa cruz genomics institute.13 we extracted tumor samples from these data sets and combined them into a single cohort that contained multiple adult and pediatric tumor types ( n = 10 , 668 )  . 
the expression of 18 , 357 protein - coding genes was measured ( data supplement )  . gene expression outlier analysis gene - level reads per kilobase of transcript per million mapped reads ( rpkm ) expression measurements for patient 1 's tumor were generated according to the previously published method.3 we used these data to compute fpkms by dividing each value by two . 
we proceeded to quantile normalize the expression values , using theoretical exponential distribution ( rate parameter = 1 ) as a background distribution ( bolstad bm , et al : bioinformatics 19 : 185 - 193 , 2003 )  . 
we then performed gene expression outlier analysis3 , 17 to identify transcripts significantly enriched in the patient 's tumor compared with 10 , 668 cancer samples in the reference compendium ( pan - cancer outlier analysis )  . 
we also performed the same analysis using only the 529 lung adenocarcinoma ( luad ) tumors as a reference ( luad - only outlier analysis ) and using 262 sarcoma tumors as a reference ( sarcoma - only outlier analysis )  . 
we analyzed the outlier genes for enrichment of specific pathways and signaling networks that could be targeted by available therapies using msigdb ( liberzon a et al : bioinformatics 27 : 1739 - 1740 , 2011 )  . the pan - cancer outlier analysis of the tumor in patient 1 compared with the reference compendium ( n = 10 , 668 ) revealed 906 genes significantly overexpressed in the patients tumor . 
the luad - only outlier analysis3 , 17 ( n = 529 ) revealed 1 , 176 up - outlier genes , and the same analysis against sarcomas ( n = 262 ) revealed 1 , 196 genes . 
we used the drug gene interaction database ( dgidb ; wagner ah , et al : nucleic acids res 44 : d1036 - d1044 , 2016 ) to identify genes whose protein products could be targeted by clinically available inhibitors . 
samples that cluster together exhibit similar gene expression profiles . we first computed pairwise spearman correlations ( brown gw : arch pediatr adolesc med 146 : 682 , 1992 ) between rnaseqderived gene expression profiles of all tumor pairs in our reference cohort ( n = 10 , 668 ) , including the tumor in patient 1 ( n = 10 , 669 )  . 
this produced a square correlation matrix with 10 , 669 columns and 10 , 669 rows . the tumormap method seeks to project high - dimensional genomic observations onto a two - dimensional plane while preserving original sample - to - sample distances . 
openord treats the similarities as spring constants and searches for a configuration among the samples that produces an arrangement to minimize the spring tension of the system as much as possible . 
 furthermore , to avoid overlapping and crowding samples in the dense graph components , openord ( x , y ) coordinates are snapped to their nearest hexagon to arrange all of the samples on a tiling of regular hexagons . 
the api provides the ability to interactively navigate , zoom , and explore various annotations of locations on the map , analogous to google maps and google earth applications . we applied the tumormap method to the reference cohort of 10 , 668 tumors together with the tumor of patient 1 by using transcriptional profiles of 18 , 357 genes ( data supplement )  . 
of note , the reference compendium contained 262 heterogeneous sarcomas from the tcga11 cohort . statistical robustness of tumormap placement the tumormap method belongs to the family of nearest neighbor classification methods . 
specifically , we wanted to assess whether the local neighborhood of patient 1 remains stable when only subsets of genes are used to compute pairwise similarities between samples . we subsampled , without replacement , gene expression features at 80% of the original gene features . 
we computed a local neighborhood specificity ( lnspecificity ) score as follows : lnspecificity = 1 __ * i = 1 n = 1000 s true s i _______ , | s i | where s is a set of nearest neighbors for either true or subsampled computation and |s| is the nearest neighbor set cardinality . this score represents average overlap , as a fraction , of the true local neighborhood and the perturbed local neighborhoods across all subsampling iterations . 
the sp score of patient 1 was 0.885 , which indicated that 88.5% of the top neighbors were consistently the same across 1 , 000 perturbations to the gene expression profiles , from which the tumormap visualization was computed . identification of genes associated with the patient 1 cluster in tumormap we identified genes differentially expressed between the luad cluster containing patient 1 and the 10 , 668 tumor samples in the compendium by using the linear model for microarray analysis method ( ritchie me , et al : mucleic acids res 43 : e47 , 2015 )  . 
the gene set enrichment analysis ( gsea ) 16 of the resulting list of genes revealed that il6 / jak / stat3 signaling pathway annotation was significantly enriched among these genes ( false discovery rate q value , 1.787e4 with 39 genes in the leading edge )  . we also identified differentially expressed genes between the luad cluster containing patient 1 and the remaining luad tumors in the compendium ( data supplement )  . 
the gsea analysis16 of this gene list revealed that members of the il6 / jak / stat3 signaling pathway were still driving the creation of the luad cluster containing patient 1 's tumor ( false discovery rate q value , 0 with 36 genes in the leading edge )  . identification of druggable targets we used the dgidb ( liberzon a et al : bioinformatics 27 : 1739 - 1740 , 2011 ; wagner ah , et al : nucleic acids res 44 : d1036 - d1044 , 2016 ) resource to search for drug targets among the genes that were upregulated in patient 1 by gene expression outlier analysis . 
for each sample in the cohort as well as for patient 1 , we ranked genes relative to the expression of all genes within that sample ( ie , the highest expressed gene was ranked as 1 )  . 
the percentiles are displayed in figure 3 for 12 genes that can be targeted by known cancer drugs , according to dgidb analysis ( liberzon a et al : bioinformatics 27 : 1739 - 1740 , 2011 ; wagner ah , et al : nucleic acids res 44 : d1036 - d1044 , 2016 )  . differential expression analysis relative to normal tissues for all of the genes in the reconstructed candidate driver pathway that are targetable by cancer drugs ( fig 3 ) we computed the fold change between the expression in patient 1 's tumor and in normal cells . 
for each gene , we mean - aggregated normal expression into a single value and computed log change of the expression of that gene in patient 1 compared with the aggregated normal value . histologic techniques and immunohistochemistry the tumor tissue was routinely fixed in 10% buffered formalin and then was processed in an automated fashion . 
all primary antibodies were either diluted or received as a ready to use prediluted solution from the relevant vendor . fluorescence in situ hybridization fluorescence in situ hybridization analysis was performed on formalin - fixed paraffin - embedded tumor tissue . 
antibodies and vendors primary antibody ki67 vimentin epithelial membrane antigen pan - cytokeratin ( ae1 / ae3 ) neuron specific enolase desmin synaptophysin cd99 myo - d1 myogenin s - 100 cd34 cd31 hmb - 45 leukocyte common antigen baf - 47 / ini - 1 abbreviation : rtu , ready to use . 
two forms of the fusion were identified ; the ewsr1 - atf1 form had higher expression than the reciprocal atf1ewsr1 forbzip , basic leucine zipper domain , which mediates sequence specific dna binding properties and the leucine zipper that is required to hold together ( dimerize ) two dna binding regions ; pkid , phosphorylated kinase - inducible - domain ; rrm , rna recognition motif ; zf , zn - finger in ran binding protein and others . 
all gene expression outliers depicted in this figure were significant in all three comparisons : patient 1 versus all cancers , patient 1 versus lung adenocarcinomas , and patient 1 versus sarcomas . 
romero - cordoba et al we appreciate the commentary and analysis by romero - cordoba et al1 in their response to our recent article in jco precision oncology.2 our research groups pursue the common goal of elucidating immunologic differences between breast cancers that could inform future immunotherapy strategies . 
all immune metrics , including counts of tumor inltrating lymphocytes and other immune cells , as well as immune gene signatures , represent a continuum and display substantial variations across samples . nevertheless , it is possible to dene more versus less immune - rich cancers by any of these metrics , and for some types of analyses , such dichotomization is necessary , even using an arbitrary threshold . our study focused on the question of whether immune - rich estrogen receptor ( er ) positive and triple - negative ( tn ) breast cancers ( bcs ) have similar or different immune microenvironments . 
to perform this comparison across multiple types of molecular data , we had to dene a shared denition of immunerichness ; we used the 75th percentile of a total tumor inltrating lymphocyte gene expression score , which encompasses the expression of 11 immune cell populations , calculated across all samples as the threshold . 
we were delighted to see that this admittedly arbitrary denition of immune - richness corresponded reasonably well with the tnbc immune classication developed by romero - cordoba et al3 : 62% of our immune - rich cancers were classied as ima ( t cell - inamed ) and 21% as imc ( immune warm )  . 
several tnbc classications have been proposed using this method.3 - 6 despite the high and mostly positive correlation in immune gene expression in breast cancer tissues , the different classication schemas yield discordant results in a substantial minority of cases , partly because of different design principles and partly because of methodology . 
however , which classication schema or molecular marker is most useful in the clinic is yet to be determined in clinical trials . the clear majority of immune biomarker studies in breast cancer focus on tnbc because of the higher prevalence of tumor inltrating lymphocytes in this subtype . 
we hope that our article draws attention to immunotherapy opportunities in er - positive cancers , because in absolute numbers , there are more immune - rich er - positive cancers than immune - rich tnbcs . 
omeara t , marczyk m , qing t , et al : immunological differences between immune - rich estrogen receptor - positive and immune - rich triple - negative breast cancers . 
prado - v azquez g , g amez - pozo a , trilla - fuertes l , et al : a novel approach to triple - negative breast cancer molecular classication reveals a luminal immune - positive subgroup with good prognoses . 
j ez equel p , loussouarn d , gu erin - charbonnel c , et al : gene - expression molecular subtyping of triple - negative breast cancer tumours : importance of immune response . 
sohal , md , mph1 a 53 - year - old woman with no signicant medical history presented to her primary care physician with fatigue and anorexia in may 2016 . 
she subsequently underwent a liver biopsy in september 2016 , and the pathology was consistent with adenocarcinoma ( strongly and diffusely positive for ck7 , with weak , patchy expression for ck20 ; programmed death ligand 1 , 2% )  . 
she was diagnosed with cancer of unknown primary , despite extensive workup revealing caudal - type homeobox 2 , thyroid transcription factor 1 , napsin a , gata - 3 , arginase , receptor 2 , and human epidermal growth factor mammaglobin negativity on immunohistochemical staining and no lesions on esophagogastroduodenoscopy or repeat colonoscopy ; however , the pathology was thought to be suggestive of a biliary origin . she received three doses of uorouracil and oxaliplathowever , she deteriorated clinically . 
genomic sequencing performed on her initial biopsied tissue ( foundationone ; foundation medicine , cambridge , ma ) was notable for mutations in braf v600e , apc , and cdkn2a ( table 1 )  . 
her case was reviewed at our genomics tumor board in december 2016 , and the recommendation was made to trial ( nci - match [ national pursue either a clinical cancer institute molecular analysis for therapy choice ; clinicaltrials.gov identier : nct02465060 ] or mypathway [ clinicaltrials.gov identier : nct02091141 ] ; each trial , the vemurafenib arm was open and available at the time ) or off - label treatment with dabrafenib and trametinib based on the asco 2016 update.1 at our institution , if two outside experts agree with the scientic data presented , off - label therapy can be approved on a case - by - case basis . given that she was not a clinical trial candidate because of the high bilirubin , off - label treatment with dabrafenib and trametinib was started in december 2016 . 
it is important to note that hepatic dysfunction , although closely monitored , is not a contraindication to initiating treatment with dabrafenib and trametinib . although serum alt elevations can occur in approximately 35% to 42% of patients receiving combination therapy , elevations greater than ve times the upper limit of normal occur in only 4% of such patients . 
in addition , there have been no instances of clinically apparent acute liver injury or hepatic failure in prelicensure studies , and there have been no published reports of clinically apparent hepatotoxicity with either drug.2 our patient was noted to experience clear clinical benet , with her total bilirubin and ast normalizing within just 2.5 months of treatment initiation and the remainder of her liver function enzymes continuing to downtrend . 
she had remarkable disease response , with radiographic ( fig 1 ) and clinical improvement until may 2018 ( a duration of almost 18 months ) , at which point there was concern about radiographic progression . 
cisplatin and gemcitabine were considered but not agreed to by the patient and family because of prior potential failure of oxaliplatin . her other option was to pursue a phase i clinical trial at an outside institution . 
her case was again discussed at the genomics tumor board in july 2018 , at which time there was deemed to be no targetable therapeutic option beyond the braf alteration , for which she had already been treated . 
interestingly , her second biopsy did identify some additional , albeit nontherapeutic , alterations not seen on the rst : rictor amplication and mtap loss of exons 6 to 8 . 
in a study analyzing these alterations in melanoma cell lines , it was found that v600e - mutant braf inhibits mammalian target of rapamycin complex 2induced phosphorylation of akt ser473 in the presence of pten . 
therapeutic implications of genomic sequencing , november 2016 sadaps and sohal fda - approved therapies genomic alterations detected * patients tumor type another tumor type potential clinical trials braf v600e none cobimetinib dabrafenib regorafenib nct01827384 nct01531361 ( phase i , targeting braf ) nct02034110 ( phase ii , targeting braf , mek ) trametinib nct02465060 ( phase ii , nci - match ) vemurafenib nct02693535 ( phase ii , tapur study ) apc r856c cdkn2a / b : cdkn2a loss exon 1 and cdkn2b loss none none none none none none abbreviations : fda , us food and drug administration ; nci - match , national cancer institute molecular analysis for therapy choice ; tapur , targeted agent and proling utilization registry . * variants of unknown signicance , 10 ; microsatellite stable ; low tumor mutational burden , 4 . discovered rictor amplication contributed to the development of braf inhibitor resistance . cleveland clinic to allow publication of this case have been obtained . per the request of the patient and her family and preliminary data extrapolated from the keynote 022 phase ii trial ( clinicaltrials.gov identier : nct02130466 ) , pembrolizumab ( via compassionate use ) was added to her regimen of dabrafenib plus trametinib starting in august 2018 . 
although high tumor mutational burden ( tmb ) has been demonstrated to be a useful biomarker in predicting immunotherapy responsiveness , 4 , 5 most studies ( eg , mypathway ) have used much higher tmb cutoffs , generally of at least 16 or more mutations per megabase , which far exceeds the tmb score obtained for our patient in either of her next - generation sequencing reports . 
she died in january 2019 , secondary to septic shock with multiorgan failure . because the patient died , consent could not be obtained ; however , no identifying personal health information has been disclosed . 
patients who receive standard - of - care gemcitabine and cisplatin chemotherapy have an overall survival ( os ) benet of 3.6 months when compared with gemcitabine monotherapy.6 even then , most patients develop treatment resistance within a few months , and median os remains less than 1 year . 
outcomes for second - line therapies have not been promising , with median progression - free survival of only a few months.7 - 13 recent advances in precision medicine have allowed for the identication of potentially targetable mutations in the effort to improve therapeutic outcomes in this population . promising targets identied in cholangiocarcinoma thus far include idh 1 / 2 , fgfr , her2 , and , the focus of our patient case , braf mutations.14 braf encodes protein kinases that function downstream of ras as part of the mitogenactivated protein kinase signaling cascade , which promotes cell proliferation , survival , and transformation . 
therapeutic implications of repeat genomic sequencing , june 2018 fda - approved therapies genomic alterations detected * patients tumor type another tumor type potential clinical trials braf v600e none cobimetinib dabrafenib regorafenib trametinib vemurafenib nct02091141 ( phase ii , mypathway ) nct02070549 ( phase i , targeting mek ) nct01989585 ( phase i / ii ) nct02428712 ( phase i / ii , targeting braf / craf ) nct02693535 ( phase ii , tapur study ) nct02034110 ( phase ii , targeting braf , mek ) apc r856c cdkn2a / b : cdkn2a loss exon 1 and cdkn2b loss riktor amplication none none none none none none none none nct02795156 ( phase ii ) nct02466802 ( phase i ) nct02097225 ( phase i ) nct01531361 ( phase i ) nct02576444 ( phase ii ) nct02142803 ( phase i ) nct03065062 ( phase i ) nct02159989 ( phase i ) nct02719691 ( phase i ) nct02583542 ( phase i / ii ) mtap loss of exons 6 to 8 none none none abbreviations : fda , us food and drug administration ; tapur , targeted agent and proling utilization registry . * variants of unknown signicance , 10 ; microsatellite stable ; low tumor mutational burden , 1 . and hyperactivate its downstream signaling.15 braf mutations are reported in up to 22% of biliary tract cancers , among which it is most commonly seen in intrahepatic cholangiocarcinoma . 
braf mutations have typically been associated with poor prognosis in patients with cholangiocarcinoma , including worse os , higher tumor grade , and chemotherapy resistance.16 there have been a few case reports on the use of dabrafenib and trametinib in cholangiocarcinoma , describing remarkable clinical and radiographic responses in patients who experienced progression during standard - of - care chemotherapy and who continued to do well 5 to 9 months out.17 , 18 most recently , a phase ii international clinical trial of dabrafenib plus trametinib in braf - mutated rare gi cancers was reported as a late - breaking presentation at the 30th european organisation for research and treatment of cancernational cancer instituteamerican association for cancer research symposium on molecular targets and cancer therapeutics . 
sohal honoraria : foundation medicine consulting or advisory role : perthera research funding : novartis ( inst ) , celgene ( inst ) , oncomed ( inst ) , bayer healthcare pharmaceuticals ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) , loxo ( inst ) travel , accommodations , expenses : foundation medicine no other potential conicts of interest were reported . references flaherty k , davies ma , grob jj , et al : genomic analysis and 3 - y efcacy and safety update of combi - d : a phase iii study of dabrafenib ( d ) + trametinib ( t ) vs d monotherapy in patients with unresectable or metastatic braf v600e / k - mutant cutaneous melanoma . 
plos one 7 : e42598 , 2012 chan ta , yarchoan m , jaffee e , et al : development of tumor mutation burden as an immunotherapy biomarker : utility for the oncology clinic . 
ann oncol 30 : 44 - 56 , 2019 legrand f , gandara d , mariathasan s , et al : association of high tissue tmb and atezolizumab efcacy across multiple tumor types . 
j clin oncol 36 , 2018 ( suppl ; abstr 12000 ) valle j , wasan h , palmer dh , et al : cisplatin plus gemcitabine versus gemcitabine for biliary tract cancer . 
croitoru a , gramaticu i , dinu i , et al : fluoropyrimidines plus cisplatin versus gemcitabine / gemcitabine plus cisplatin in locally advanced and metastatic biliary tract carcinomaa retrospective study . 
fornaro l , vivaldi c , cereda s , et al : second - line chemotherapy in advanced biliary cancer progressed to rst - line platinum - gemcitabine combination : a multicenter survey and pooled analysis with published data . 
brugnara s , sicher m , bonandini em , et al : treatment with combined dabrafenib and trametinib in brafv600e - mutated metastatic malignant melanoma : a case of long - term complete response after treatment cessation . 
loaiza - bonilla a , clayton e , furth e , et al : dramatic response to dabrafenib and trametinib combination in a braf v600e - mutated cholangiocarcinoma : implementation of a molecular tumour board and next - generation sequencing for personalized medicine . 
presented at the 30th eortc - nci - aacr symposium on molecular targets and cancer therapeutics , dublin , ireland , november 13 - 16 , 2018 ( abstr 2 ) 20 . 
 c profound immunotherapy response in mismatch repair - deficient breast cancer introduction because most patients with cancer do not benefit from immunotherapies such as anti - pd1 , the identification of biomarkers to select patients for immunotherapy is crucial . 
mismatch repair deficiency ( dmmr ) is strongly associated with responsiveness to anti - pd11 in gi and endometrial cancers and can be readily detected using immunohistochemistry ( mlh1 , msh2 , mhs6 , and pms2 ) and / or polymerase chain reaction ( pcr ) for microsatellite instability ( msi )  . 
the response rate to anti - pd1 in dmmr colorectal cancers was no less than 40% , and was even 70% in other gi and endometrial dmmr cancers , whereas it was 0% in mmr - proficient colorectal cancer.1 although not routinely tested , dmmr can be found in other cancer types outside gi and endometrial cancers , in a frequency of approximately 2% to 3%.2 breast cancer is an example of a tumor type in which dmmr is rare ( frequency is 0% to 1% ) .3 responses to checkpoint blockade in breast cancer are relatively infrequent ( 5% to 19% ) 4 but can be durable , illustrating the urgent need for predictive biomarkers to select those few patients who could benefit from immunotherapy . 
three years before , she received treatment for a triple negative breast carcinoma ( tnbc )  . morphology , immunohistochemistry , and cancer gene - panel sequencing of the lung and stomach and the archived breast biopsy findings confirmed the diagnosis of lung and stomach metastases from the former tnbc ( appendix )  . immunohistochemistry findings showed loss of mlh1 and pms2 , and somatic hypermethylation of the mlh1 promotor was found . 
however , focal pd - l1 expression was observed on the tils . short - term response was seen with palliative carboplatin , yet , after six cycles , progression was observed . 
in addition , a partial response of all other lesions was observed as determined by response evaluation criteria in solid tumors ( recist ) 1.1.5 after 12 cycles , this response is still ongoing . in this case , extensive revision of three seemingly separate lesions led to the identification of this rare dmmr breast cancer . 
we would like to bring this case to the attention of colleagues to make a case for msi testing in patients with metastatic cancer beyond the typical lynch - associated cancers . 
linn jolanda van dieren all authors : netherlands cancer institute , amsterdam , netherlands . the dutch cancer society provided funding for the setup and data management of the clinical trial in which the patient in this report is participating , as well as translational fellowships to m.k. 
 ( a ) a deep 5 - cm ulcerative tumor located at the lesser curvature of the stomach . ( b ) disappearance of the tumor after three cycles of nivolumab . 
horlings , jolanda van dieren collection and assembly of data : marleen kok , hugo m . horlings , petur snaebjornsson , myriam chalabi , sabine c . linn , jolanda van dieren data analysis and interpretation : marleen kok , hugo m . horlings , petur snaebjornsson , ton n . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . marleen kok research funding : bristol - myers squibb ( inst ) travel , accommodations , expenses : roche hugo m . 
horlings no relationship to disclose petur snaebjornsson no relationship to disclose references 2509 - 2520 , 2015 myriam chalabi research funding : bristol - myers squibb ( inst ) travel , accommodations , expenses : roche / genentech ton n . 
schumacher employment : kite pharma stock and other ownership interests : kite pharma , neon therapeutics , aimm therapeutics honoraria : neon therapeutics , aimm therapeutics research funding : merck , bristol - myers squibb christian u . 
blank consulting or advisory role : genentech ( inst ) , msd oncology ( inst ) , bristol - myers squibb ( inst ) , novartis ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , astrazeneca ( inst ) , eli lilly ( inst ) research funding : bristol - myers squibb ( inst ) , novartis ( inst ) travel , accommodations , expenses : pfizer , roche sabine c . 
linn consulting or advisory role : astrazeneca ( inst ) , ibm ( inst ) , bayer ( inst ) research funding : genentech ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) patents , royalties , other intellectual property : named inventor on a patent for a brca1ness gene expression classifier in breast cancer ( inst ) travel , accommodations , expenses : roche jolanda van dieren no relationship to disclose 1 . 
hall mj , gowen k , sanford em , et al : evaluation of microsatellite instability ( msi ) status in 11 , 573 diverse solid tumors using comprehensive genomic profiling ( cgp )  . 
subsequently , microsatellite instability ( msi ) was assessed by a pentaplex polymerase chain reaction - based assay using fluorescently labeled primers of five mononucleotide repeat targets ( bat25 , bat26 , nr24 , nr21 , nr27 ) , followed by fragment analysis . 
promoter methylation status of mmr genes was assessed by multiplex ligation - dependent probe amplification ( mlpa , me011 - b2 kit ; mrc holland , amsterdam , netherlands )  . 
in brief , paraffin sections were cut at 4 mm , heated at 75c for 28 minutes , and deparaffinized in the instrument with ez prep solution ( roche )  . 
two pathologists scored pd - l1 staining based on the percentage of positive tumor and / or immune cells . assessment of tumor - infiltrating lymphocytes tumor - infiltrating lymphocytes ( tils ) were evaluated according to the guidelines of the international tils working group for invasive breast carcinoma ( luen sj , et al : lancet oncol 18 : 52 - 62 , 2017 ; salgado r , et al : ann oncol 26 : 259 - 271 , 2015 )  . 
dmmr / microsatellite high ( msi - h ) breast cancers were among the responding tumors that led to the recent us food and drug administration accelerated approval of pembrolizumab for any patient with a dmmr / msi - h metastatic solid tumor.2 the authors conclude that they would like to make a case for msi testing in patients with metastatic cancer beyond typical lynch - associated cancers.1 i also propose the study of whether patients now identified with dmmr breast cancers might harbor germline mismatch repair ( mmr ) - mutated genes and , therefore , would be molecularly defined as lynch syndrome family members . the us food and drug administration accelerated approval and suggestion by kok et al represent an opportunity to clarify whether breast cancer should be considered a lynch - associated cancer . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . steven sorscher honoraria : celgene , pfizer , puma biotechnology speakers bureau : celgene , pfizer , puma biotechnology travel , accommodations , expenses : celgene , pfizer , puma biotechnology 1 . 
 e beyond the androgen receptor : targeting actionable drivers of prostate cancer see accompanying article doi : more than 70 years ago , huggins et al1 exploited the exquisite and unique dependence of prostate cancer ( pc ) on androgenic hormones for survival and growth using a treatment strategy that foreshadowed the clinical benefits underlying the application of precision oncology . 
today , variations of androgen receptor ( ar ) pathway targeting remain the cornerstone of the initial management of men with metastatic pc , usually with gratifying responsesalthough unfortunately few cures . 
however , the advent and application of technologies capable of deep assessments of the full spectrum of molecular aberrations that underlie the development and progression of malignant neoplasms now forecast the near - term potential of new therapeutic approaches poised to change the near - exclusive reliance on ardirected interventions as initial treatment for advanced pc . studies using whole - exome sequencing and comprehensive rna sequencing , supported through the cancer genome atlas2 and stand up to cancer / prostate cancer foundation3 initiatives , have profiled hundreds of localized and castration - resistant metastatic pcs ( crpcs ) , resulting in the identification of numerous recurrent driver aberrations that comprise signaling programs and pathways for which there are pharmacologic inhibitors . 
lacking in these previous studies was an assessment of untreated metastatic tumors . in the article accompanying this editorial , abida et al4 have taken the first step in filling this knowledge gap . using a predefined gene panel , abida et al4 evaluated mutations and copy losses in key oncogenes and tumor suppressors across a spectrum of localized pc , untreated metastatic disease , and crpc . 
the tumor assays were conducted in a clinical laboratory improvement amendments environment using real - world clinical samples , which demonstrates the feasibility of molecular profiling to guide therapeutics , even in challenging situations such as evaluating bone metastases . overall , a high frequency of potentially actionable alterations were identified that included components of the phosphatidylinositol 3 - kinase ( pi3k ) pathway ( 24% ) , mitogen - activated protein kinase pathway ( 5% ) , and b - catenin program ( 15% )  . this study also confirmed previous reports that aberrations in genes involved in dna repair are common , particularly those involved in the process of homologous recombination repair.5 overall , 22% of tumors had somatic aberrations in a dna repair gene , and 19% were found to have a putative deleterious germ line mutation . 
this pc subtype is notable for therapeutics such as poly ( adp - ribose ) polymerase inhibitors and platinum - based chemotherapy that could exploit a dna repair vulnerability.6 , 7 however , it is important to recognize that it is currently unclear whether each gene comprising the dna repair machinery will exhibit enhanced responses to these agents , nor is it clear whether each type of aberration within a particular dna repair gene will confer congruent outcomes with respect to treatment response . 
preclinical studies using functional readouts of dna repair proficiency and clinical trials coupled with careful assessments of each dna damage response gene aberration will be required to confirm predictive associations . overall , there was substantial heterogeneity in the composition of putative cancer drivers between individuals , a finding that supports avoiding a onesize - fits - all approach to therapy . 
 number of matched tumors from the same patient demonstrated consistent truncal aberrations in tumor suppressors such as tp53 and brca2 and amplification of ar across each tumor evaluated . these results indicate that sampling a single metastatic site provides a reasonable assessment of the major molecular alterations that may influence treatment decisions . 
however , analyses of tumors across intervals of time and treatment indicated that molecular evolution does occur , with higher mutation counts in tumors sampled at later time points . consequently , it is not clear whether sampling a primary tumor or a metastatic tumor early in the course of disease will accurately reflect driver or resistance mechanisms that are operating later in the course of cancer progression . a distinguishing feature of the abida et al4 study involves the acquisition and assessment of metastatic tumors that had not been exposed to ar - directed therapy or other systemic treatment . comparing the features of these metastases with those of localized tumors serves to identify drivers of the metastatic process , and comparing their molecular composition with that of tumors withstanding ar - directed therapy serves to identify mechanisms contributing to treatment resistance . in the first comparison , it is notable that aberrations in ar did not occur , emphasizing that ar mutation and copy - number gain , frequent events in crpc , occur in response to pressures exerted by ar pathway inhibition and rarely or never arise as de novo drivers of pc . 
in addition to ar , the frequency of aberrations in tp53 , rb1 , pten , and atm was significantly increased in crpc compared with metastatic noncastrate disease , indicating potential roles in mediating castration resistance . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . interactions with the ar or ar program or if they promote pc growth through mechanisms that bypass ar requirements . 
although enriched in crpc , a substantial number of treatment - nave tumors did exhibit mutations or structural alterations in these genes , suggesting that cotargeting the aberrant pathways concurrently with the ar may serve to circumvent predestined pathways of resistance . that drug combinations current therapy for metastatic pc generally follows a paradigm of sequentially deploying a given therapeutic such as androgen deprivation to the point of resistance , switching to another agent such as abiraterone or enzalutamide , and treating again to resistance , until options are exhausted . 
nelson consulting or advisory role : janssen oncology , astellas pharma , genentech acknowledgment supported by national institutes of health grants no . p30ca15704 and p50ca097186 , us department of defense grant no . 
cancer genome atlas research network : the molecular taxonomy of primary prostate cancer . arch surg 43 : 209 - 223 , 1941 cell 163 : 1011 - 1025 , 2015 3 . 
mateo j , carreira s , sandhu s , et al : dna - repair defects and olaparib in metastatic prostate cancer . n engl j med 373 : 1697 - 1708 , 2015 7 . 
schweizer mt , zhou xc , wang h , et al : the influence of prior abiraterone treatment on the clinical activity of docetaxel in men with metastatic castration - resistant prostate cancer . 
smith mr , saad f , rathkopf de , et al : clinical outcomes from androgen signaling - directed therapy after treatment with abiraterone acetate and prednisone in patients with metastatic castration - resistant prostate cancer : post hoc analysis of cou - aa - 302 . 
30 years ago with the identication of the reciprocal translocation , t ( 11 ; 22 ) ( q24 ; q12 ) , otherwise known as ews - fl1.1 , 2 in the time since , multiple other fusion partners with ews have been identied that t a similar ewing sarcoma phenotype.3 , 4 when ews fusions are not identied , tumors with histologic features of ewing sarcoma have been labeled as primitive neuroectodermal tumors . 
in 2012 , pierron et al5 identied a subset of ewing - like tumors harboring paracentric inversion on the short arm of chromosome x , resulting in the fusion of the bcor and ccnb3 genes.5 since that discovery , several small case series have further elucidated the clinical , morphologic , and genomic differences that make this diagnosis distinct from other round cell sarcomas , most notably ewing sarcoma.6 - 8 though distinct from ewing sarcoma , most bcorccnb3fused sarcomas ( bcs ) are treated with upfront compressed chemotherapy with vincristine , doxorubicin , cyclophosphamide , ifosfamide , and etoposide plus local control with surgery and / or radiation . bcs shares similar event - free and overall survival rates with the standard ews - fli1fused ewing sarcoma using this treatment strategy.6 - 8 despite the growing knowledge base related to bcs , little is known about potential drug targets related to this disease entity , especially with regard to treatment of disease recurrence . 
we highlight the treatment of a young patient who had multiply - relapsed disease with the us food and drug administrationapproved cyclindependent kinase 4 / 6 ( cdk4 / 6 ) inhibitor palbociclib ; the tumor harbored a bcor - ccnb3 fusion and a germline variant in cdkn2b , and treatment resulted in a complete response and no evidence of disease 25 months into therapy . case history our male patient initially presented in 2010 at 1 year of age with a xed mass on his back . 
a core needle biopsy was performed , which revealed a malignant , small , round , blue cell tumor along with small amounts of benign brofatty tissue and skeletal muscle . 
immunohistochemical stains were positive for cd99 , fli1 , and vimentin and were negative for nse , synaptophysin , myf4 , gaf , cd45rb , and tdt consistent with a primitive neuroectodermal tumor . 
the patient started chemotherapy per childrens oncology group protocol aews0031 , regimen b2 , with ifosfamide , etoposide , vincristine , doxorubicin , and cyclophosphamide . gross total resection was not feasible at the time per neurosurgery , and the patient received 57.6 gy of proton beam radiation in october 2010 . 
2 years but then developed multiple local recurrences without metastases from 2013 to 2017 and underwent numerous surgeries , along with multiple different early - phase childrens oncology group therapeutic studies , as outlined in the timeline in figure 1a . 
after the most recent recurrence in october 2016 , the patient was referred to our pediatric cancer precision genomics prograbecause of the ndings outlined here in the results , we chose to start palbociclib in february 2017 . 
 diagnosis radiation debulking surgeries ( n = 4 ) case report molecular tumor analysis debulking surgery debulking surgery april 2010 2010 july 2013 2014 2015 2016 june 2016 2016 2016 2017 march 2019 initial therapy aews0031 arm b : vincristine , doxorubicin , cyclophosphamide , ifosfamide , etoposide cog phase i advl1212 : crizotinib , cyclophosphamide , topotecan phase ii advl1322 : pazopanib phase i advl1315 : axitinib metronomic therapy molecular - guided therapy palbociclib initial diagnosis before palbociclib 2 cycles of palbociclib 3 cycles of palbociclib 2 years of palbociclib fig 1 . 
there was concern for progression after 2 cycles of palbociclib , but there was a 2 - month lag between the before palbociclib scan and actually starting drug , so interval progression likely occurred in this timeframe . 
ned , no evidence of disease . results whole - genome sequencing , rna sequencing ( rna - seq ) analysis , germline exome sequencing , and protein evaluation were performed at the clinical laboratory improvement amendment ( clia ) approved laboratory , nantomics ( culver city , ca )  . 
the mutational burden of the tumor was relatively low at 75 , 046 somatic mutations , with only 88 somatic mutations mapping to protein coding regions ( circos plot in fig 2a )  . 
additionally , an undescribed somatic mutation in the smo gene ( smo n476s ) was identied in the tumor , and germline sequencing revealed a cdkn2b n41d missense variant , which was heterozygous in both the germline and tumor genomes of this patient . 
rna - seq was also performed by nantomics , and mrna transcripts were ranked by abundance , which could be associated with increased pathway activity and sensitivity to a targeted drug . 
with the exception of the destruction box in ccnb3 , all functional domains from each encoded protein remain intact in the bcor - ccnb3 fusion prote ( c ) the cdk4 / 6 pathway is a gene regulatory program controlled by multiple tiers of protein kinases and transcriptional regulators . increases in cyclin - d or cdk4 or 6 protein can lead to phosphorylation of the rb1 - e2f tumor suppressor complex . 
upon phosphorylation of rb1 , the e2f1 - 3 transcription factors are released from the complex and are able to bind to the promoters of target genes , driving activation of transcription . 
in the several case series describing bcs , the median age of diagnosis is in the teenage years , with the youngest patient recorded at age 2.5 - 8 , 11 again , because of the age of presentation , one could be concerned about an inherited cancer syndrome . 
this congenital tumor also harbored a smarcb1 / ini1 gene deletion common to malignant rhabdoid tumor , epithelioid sarcomas , and epithelioid malignant peripheral nerve sheath tumor that also , table 1 . 
overexpression of relevant tumor - promoting pathways gene status gene function ccnd1 ccnd2 cdk4 e2f1 e2f2 e2f3 cdc25a cdc25c cdc25b top2a bub1 bub1b overexpressed activating cyclin for cdk4 and cdk6 overexpressed activating cyclin for cdk4 and cdk6 overexpressed rb1 protein kinase overexpressed rb1 - regulated transcription factor overexpressed rb1 - regulated transcription factor overexpressed rb1 - regulated transcription factor overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene note . 
the expression status for a gene was classied as overexpressed if its tpm exceeded the genes upper 5th percentile.30 abbreviations : cdk , cyclin - dependent kinase ; e2f , e2 transcription factor ; rb1 , retinoblastoma gene ; tpms , transcripts per million . when found germline , is known to cause rhabdoid tumor predisposition syndrome.12 - 16 in the case reported by alfaro - cervello et al , 12 ini1 germline analysis was not performed . 
our patient also harbored a germline heterozygous missense variant , cdkn2b n41d . is unclear what role this germline cdkn2b n41d variant could play in sarcomagenesis , as cancer risks associated with cdkn2a / b gene variants include melanoma , pancreatic cancer , and astrocytomas.17 , 18 there is a recent short report from jouenne et al19 that found an increased risk of soft tissue sarcoma development with germline loss of cdkn2a , though no data exist conrming this risk with cdkn2b variants . 
sunita et al20 showed that the specic cdkn2b n41d variant , which encodes p15 ( ink4b ) , is unable to bind to the cdk6 protein , leading to loss of function of cdkn2b , which could lead to dysregulated control of s - phase entry . 
though this variants contribution to tumorigenesis is intriguing , ckdn2b was normally expressed in our patients tumor , and there are no data suggesting that this impaired binding to cdk6 leads to mrna overexpression along multiple levels of the cdk4 / 6 pathway . despite discovering alterations of several key regulators of the cdk4 / 6 pathway in this tumor , none have been proven to serve as clinical biomarker for sensitivity to cdk4 / 6 inhibitors.21 in a preclinical ewing sarcoma orthotopic xenograft model with cdkn2a deletion , palbociclib was able to greatly suppress growth despite doxorubicin resistance of this model.22 in other sarcoma subtypes , palbociclib reduced tumor burden in murine preclinical models.23 - 25 clinically , there is phase ii evidence of palbociclibs efcacy in adults with liposarcoma26 , 27 and leiomyosarcoma.28 despite growing evidence in these sarcomas , there are no published data testing cdk4 / 6 inhibitors in bcs . 
for our patient with bcs , the expression status for a gene was classied as overexpressed if its tpm exceeded the genes upper 5th percentile of per - gene rna - seq by expectation - maximization ( rsem ) transcript - per - million ( tpm ) values for a collection of rna sequencing ( rna - seq ) datasets from the cancer genome atlas normal samples . 
in the study by pierron et al , 5 10 bcs tumors were analyzed for certain mrna expression ; overexpression was determined as described in pierron manuscript methods . abbreviations : bcs , bcor - ccnb3fused sarcomas ; nd , not disclosed . pathway , and ( 3 ) the presence of a germline cdkn2b variant . 
ferguson , md , ms , 705 riley hospital dr , ri 4340 , indianapolis , in 46202 ; twitter : @rileychildrens ; e - mail : micjferg@iu.edu. support supported by grant no . 
cancer genet cytogenet 21 : 185 - 208 , 1986 turc - carel c , aurias a , mugneret f , et al : chromosomes in ewings sarcoma : i . 
an evaluation of 85 cases of remarkable consistency of t ( 11 ; 22 ) ( q24 ; q12 )  . cancer genet cytogenet 32 : 229 - 238 , 1988 ginsberg jp , de alava e , ladanyi m , et al : ews - fli1 and ews - erg gene fusions are associated with similar clinical phenotypes in ewings sarcoma . 
j clin oncol 17 : 1809 - 1814 , 1999 shing dc , mcmullan dj , roberts p , et al : fus / erg gene fusions in ewings tumors . 
cancer res 63 : 4568 - 4576 , 2003 pierron g , tirode f , lucchesi c , et al : a new subtype of bone sarcoma dened by bcor - ccnb3 gene fusion . 
nat genet 44 : 461 - 466 , 2012 peters tl , kumar v , polikepahad s , et al : bcor - ccnb3 fusions are frequent in undifferentiated sarcomas of male children . 
mod pathol 28 : 575 - 586 , 2015 puls f , niblett a , marland g , et al : bcor - ccnb3 ( ewing - like ) sarcoma : a clinicopathologic analysis of 10 cases , in comparison with conventional ewing sarcoma . 
am j surg pathol 38 : 1307 - 1318 , 2014 kao , yc , owosho aa , sung ys , et al : bcor - ccnb3 fusionpositive sarcomas : a clinicopathologic and molecular analysis of 36 cases with comparison to morphologic spectrum and clinical behavior of other round cell sarcomas . 
riggi n , suv `a ml , suv `a d , et al : ews - fli - 1 expression triggers a ewings sarcoma initiation program in primary human mesenchymal stem cells . 
matsuyama a , shiba e , umekita y , et al : clinicopathologic diversity of undifferentiated sarcoma with bcor - ccnb3 fusion : analysis of 11 cases with a reappraisal of the utility of immunohistochemistry for bcor and ccnb3 . 
chan ak , han sj , choy w , et al : familial melanoma - astrocytoma syndrome : synchronous diffuse astrocytoma and pleomorphic xanthoastrocytoma in a patient with germline cdkn2a / b deletion and a signicant family history . 
campa d , pastore m , gentiluomo m , et al : functional single nucleotide polymorphisms within the cyclin - dependent kinase inhibitor 2a / 2b region affect pancreatic cancer risk . 
oncotarget 7 : 57011 - 57020 , 2016 jouenne f , chauvot de beauchene i , bollaert e , et al : germline cdkn2a / p16ink4a mutations contribute to genetic determinism of sarcoma . 
agarwal sk , mateo cm , marx sj : rare germline mutations in cyclin - dependent kinase inhibitor genes in multiple endocrine neoplasia type 1 and related states . j clin endocrinol metab 94 : 1826 - 1834 , 2009 21 . 
murakami t , singh as , kiyuna t , et al : effective molecular targeting of cdk4 / 6 and igf - 1r in a rare fus - erg fusion cdkn2a - deletion doxorubicin - resistant ewings sarcoma patient - derived orthotopic xenograft ( pdox ) nude - mouse model . 
perez m , muoz - galv an s , jim enez - garca mp , et al : efcacy of cdk4 inhibition against sarcomas depends on their levels of cdk4 and p16ink4 mrna . oncotarget 6 : 40557 - 40574 , 2015 24 . 
vlenterie m , hillebrandt - roeffen mh , schaars ew , et al : targeting cyclin - dependent kinases in synovial sarcoma : palbociclib as a potential treatment for synovial sarcoma patients . 
b ohm mj , marienfeld r , j ager d , et al : analysis of the cdk4 / 6 cell cycle pathway in leiomyosarcomas as a potential target for inhibition by palbociclib . 
dickson ma , tap wd , keohan ml , et al : phase ii trial of the cdk4 inhibitor pd0332991 in patients with advanced cdk4 - amplied well - differentiated or dedifferentiated liposarcoma . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
elvin ja , gay lm , ort r , et al : clinical benet in response to palbociclib treatment in refractory uterine leiomyosarcomas with a common cdkn2a alteration . oncologist 22 : 416 - 421 , 2017 1072 - 1074 , 2015 29 . 
we developed and validated a genome - wide dna methylationbased classifier to differentiate between osteosarcoma , ewing sarcoma , and synovial sarcoma . methods dna methylation status of 482 , 421 cpg sites in 10 ewing sarcoma , 11 synovial sarcoma , and 15 osteosarcoma samples were determined using the illumina infinium humanmethylation450 array . 
this classifier was validated on data drawn from the cancer genome atlas synovial sarcoma , target - osteosarcoma , and a recently published series of ewing sarcoma . results methylation profiling revealed three distinct patterns , each enriched with a single sarcoma subtype . 
within the validation cohorts , all samples from the cancer genome atlas were accurately classified as synovial sarcoma ( 10 of 10 ; sensitivity and specificity , 100% ) , all but one sample from target - osteosarcoma were classified as osteosarcoma ( 85 of 86 ; sensitivity , 98% ; specificity , 100% ) , and 14 of 15 ewing sarcoma samples were classified correctly ( sensitivity , 93% ; specificity , 100% )  . 
two additional clinical samples that were difficult to classify by morphology and molecular methods were classified as osteosarcoma ; one had been suspected of being a synovial sarcoma and the other of being ewing sarcoma on initial diagnosis . conclusion osteosarcoma , synovial sarcoma , and ewing sarcoma have distinct epigenetic profiles . 
ewing sarcoma ( ews ) , synovial sarcoma ( ss ) , and osteosarcoma ( os ) are among the most common malignant solid tumors in children.1 although these tumors can occur in similar anatomic locations , optimal management and treatment strategies differ substantially depending on the tumor type.2 , 3 accurate diagnosis is thus paramount for clinical management , but can be challenging . histologically , ews is mainly composed of small round blue cells4 but occasionally consists of larger , more pleomorphic cells , making the diagnosis of ews based solely on histopathological analysis unreliable.5 the discovery of the ewsr1 - fli1 fusion detected by fluorescent in situ hybridization ( fish ) has significantly improved diagnostic accuracy , but the fusion is only present in approximately 85% of samples that are histologically consistent with ews.6 in the remainder of cases , most tumors harbor a fusion of the ewsr1 gene with a different member of the e - 26 transformation specific family of transcription factors.7 , 8 , 9 , 10 , 11 ss typically has a biphasic appearance consisting of epithelioid and fibroblast - like spindle cell components ; however , a monophasic spindle cell s . 
morphologic variants include spindle - cell os ( resembling fibrosarcoma or monophasic synovial sarcoma ) , high - grade pleomorphic os ( resembling undifferentiated pleomorphic sarcoma ) , or small round blue cell os ( resembling classic ews ) .12 the presence of osteoid deposition is helpful in the histologic diagnosis , but this deposition may not be present in very poorly differentiated specimens or small biopsy specimens . 
a wide range of copy number changes , most frequently including chromosomes 6p , 8q , 13q , and 17p , have been observed.15 - 18 additionally , the presence of the ewsr1 - fli1 translocation in a rare subset of small - cell os further complicates diagnostics.19 - 22 previous work has demonstrated the feasibility of classifying small round cell tumors using machinelearning techniques and artificial neural networks trained on gene expression data , 23 or support vector machinebased classifiers to distinguish between sarcoma subtypes with variable sensitivity and specificity ( range , 50% to 100% ) .24 a new approach to aid the diagnosis of solid tumors is based on the molecular signatures of genomewide dna methylation profiles . 
this technique has been pioneered as a powerful diagnostic tool in pediatric brain tumors and has been shown to be superior for risk stratification compared with standard histopathology.25 - 27 for the purposes of classification alone , the advantage of methylation is resolution . 
there is also an advantage of decreased noise , because methylation is more invariant to formalin fixation , time to fixation , cold ischemia time , temperature out of the body , immune status of the host , and several other factors that affect gene expression . 
integrative dna - methylation analysis has been examined as a tool to classify high - grade soft - tissue sarcoma , including ss , but not os or ews.28 the aim of the current study was to determine if methylation profiling can be used to accurately distinguish among ss , os , and ews . methods tissue collection and dna extraction eighty tissue samples from patients newly diagnosed with os , ews , and ss were obtained from the archives of the departments of pathology at the new york university langone medical center ( nyulmc ) , memorial sloan kettering cancer center , and montefiore medical center . 
oss were diagnosed on the basis of histologic features and , where available , absence of fusions characteristic of ews and ss . to develop the classifier , we selected histopathologically classic ( os , ss , ews ) and molecularly confirmed ( ss , ews ) reference samples . 
for the ith probe , the m value was calculated as a log2 transform of a ratio of the b value . mi log2 = 1 2 b a one - way analysis of variance via empirical bayes method ( r package limma ) was conducted to select for the most differentially methylated probes among the different sarcoma subtypes . 
more than 8 , 556 probes were found to be significantly differentially methylated ; however , many were very highly correlated ( data supplement ) ; thus , we selected the top 400 probes with the greatest median absolute deviation in b values ( data supplement )  . the random forest algorithm was used for classification . 
the number of trees was set at 400 with a number of variables tried at each node of 305 ( tuned to reduce out - of - bag error ) and minimum node size of 1 . validation samples we validated our classifier using the cancer genome atlas ( tcga ) , target - osteosarcoma ( target - os ; from childrens oncology group and the hospital for sick children , toronto , canada ) , and ews samples from a recently published series . 
raw signal intensity data ( idat ) files from tcga sss ( n = 10 ) were downloaded from the legacy archives of the genomic data commons.32 similarly , idat files and normalized gene quantification from mrna sequencing belonging to the discovery cohort of target - os ( n = 86 ) were accessed through the target data matrix ( matrix )  . 
idat files from huertas - martinez et al ( institut dinvestigacio biomedica de bellvitge [ idibell ] ) were obtained from the corresponding author.33 genomic pathway analysis information probes in the classifier were annotated using the ( version 1.2 ; humanmethylation450 manifest illumina )  . 
genomic including dna sequence and coordinates of gene coding regions were obtained from the university of california santa cruz genome browser database.34 we accessed 113 probes corresponding to enhancers and gene coding regions , using the molecular signatures database , a gene - set based pathway analysis . 
in total , we interrogated the overlap of classifier genes with 4 , 729 curated gene sets , which include known chemical and genetic perturbations ( n = 3 , 500 ) , gene sets derived from the kegg ( n = 186 ) , biocarta ( n = 217 ) , and reactome ( n = 674 ) pathways , and canonical pathways curated by domain experts ( n = 1 , 329 ) .35 data access idat files of the training set have been deposited in gene expression omnibus , accession number gse97529 . 
sample location included the appendicular ( 11 of 36 ; 31% ) and axial skeleton ( 23 of 36 ; 64% ) ; biopsy sites of two samples ( 5% ) were unknown . sarcomas showed distinct patterns of methylation unsupervised hierarchical clustering using the 400 most differentially methylated probes among the training set demonstrated three distinct molecular phenotypes corresponding to the pathologic diagnoses ( fig 1a )  . 
patient characteristics of the training set ( n = 36 ) sample histology primary tumor location translocation or fusion lateral side of the right knee mediastinal lymph node orbit ( secondary os ) lymph node left talus tibia back femur epidural tibia femur mandible femur femur right tibia right knee neck left knee right neck left foot thigh chest wall foot shoulder abdomen thigh foot right distal femur left tibia right femur right shoulder left pelvis left humerus left shoulder wall ewsr1 - fli1 ewsr1 - fli1 ewsr1 - fli1 ewsr1 - fli1 ewsr1 - fli1 ewsr1 - fli1 ewsr1 - fli1 ewsr1 - fli1 ewsr1 - fli1 x : 18 x : 18 x : 18 syt rearrangement syt rearrangement syt rearrangement abbreviations : ews , ewing sarcoma ; n / a , not applicable ; os , osteosarcoma ; ss , synovial sarcoma . with known genetic probes of interest . 
the closest probe to fli1 is 5 mb away ( cg13153466 ) , corresponding to the promoter region of asam , a coxsackieand adenovirus - receptorlike membrane protein . no probes lie near the cytogenetic band 18q11.2 belonging to the syt translocation partner of synovial sarcoma ; the closest four probes in chromosome 18 lie in a 0.1 - mb strip at 18q23 , notably hypomethylated in ss . 
the gray arrow indicates the sample from the targetosteosarcoma ( targetos ) dataset ( target40 - pasefs ) that demonstrated hypermethylation in several cpg islands uncharacteristic of other osteosarcomas . accurate methylation - based classification of bone sarcomas when the classifier was applied to the training cohort , all samples were accurately classified with a minimum margin score of 0.2 , thus confirming internal validity ( table 3 )  . 
within the validation cohorts , all samples ( 10 of 10 ) from tcga were accurately classified as ss , 14 of 15 ews samples were accurately classified as ews , and all tumors from target - os ( 85 of 86 ) were classified as os except one sample , which was classified as ews ( table 4 )  . 
a single case from the ews validation set that classified as a ss did not have rna data available for confirmatory studies . the discrepant os sample , target - 40pasefs ( highlighted by the arrow in fig 1a and displayed in fig 1b ) , was submitted from an 18 - year - old white man who was enrolled and treated in childrens oncology group clinical trial aost0331 . 
 ( b ) multidimensional scaling plot of random forest classifier samples demonstrates this target - os sample ( red triangle ) was classified as ewing sarcoma ( ews )  . 
 ( c ) rna sequence analysis of the sample target - os sample identified as ews by methylation classifier . the target - 40pasefs sample shows overexpression of ewsr1 and etv1 . 
rna expression data are consistent with the methylation sarcoma classifier diagnosis of ews . have been misclassified as ews at the time of original diagnosis , we investigated ewsr1 , fli1 , erg , and etv1 mrna transcript counts , available in the target - os dataset , to examine the common gene products of oncogenic ews fusions . 
although the expression of fli1 was similar to other samples in the cohort , we noted a striking overexpression of etv1 ( n = 70 transcripts per kilobase million ) and ewsr1 ( n = 200 transcripts per kilobase million ) compared with the other os samples in the dataset ( fig 1c )  . 
we hypothesized that the tumor harbored a ewsr1 / etv1 rearrangement consistent with ews ; however , after manually curating the transcript sequence reads , there was no evidence of an etv1 fusion , suggesting an alternative mechanism leading to etv1 upregulation . clinical application to illustrate the clinical utility of our classifier , we present two challenging clinical cases . 
the first is that of a 16 - year - old girl with a past medical history of rhabdomyosarcoma of the right orbit initially diagnosed in 2007 and treated with chemotherapy and radiation therapy . 
immunohistochemical stains were positive for vimentin , cd56 , and desmin , but tumor cells were negative for myogenin , myo - d1 , s - 100 , cam 5.2 , ae 1 / 3 , bcl - 2 , cd99 , cd34 , and ema . 
fish testing using a dual - color breakapart probe showed a rearrangement involving ss18 ( syt ; 88.0% of cells ; data not shown ) , raising the concern that the tumor may represent ss . 
however , satb2 was positive by immunohistochemistry , suggesting osteoblastic differentiation.36 ssx1 and ssx2 , the usual fusion partners for syt in synovial sarcoma , had no abnormalities . we performed methylation profiling on the 2016 recurrence sample . 
moreover , it indicates robustness of a methylation - based sarcoma classifier not only in de novo but also in radiation - induced os . the second difficult case was a 2 - year - old girl who had a mass involving t7 - 9 of the thoracic spine with radiographic evidence of pulmonary metastases . 
she received intensive multiagent chemotherapy and involved field radiation therapy to the spine . three years later at the age of 5 , she presented with recurrent disease , including a left - sided pleural mass and hilar adenopathy . 
pathology revealed viable disease with similar morphologic findings as her initial disease . at the age of 15 , the patient presented with headache , pupillary asymmetry , and slurred speech . 
targeted dna ( msk - impact37 ) and rna ( archer fusionplex ; archerdx , boulder , co ) were nondiagnostic but revealed a genomically unstable tumor with numerous mutations , which would be unusual for translocation - driven sarcomas such as ews . quantitative predictive probabilities derived from the random forest model were used to classify this sample , with a predicted probability of 48% os , 32% ss , and 20% ews . 
in the scenario in which os and ews compose the differential diagnosis , os was the most likely and ews the least likely grouping ( fig 2f )  . discussion in sarcomas lacking pathognomonic gene fusions , diagnostic differentiation can be extremely challenging , even with the help of modern diagnostic tools including immunohistochemistry and cytogenetics.38 - 41 additionally , tumor heterogeneity and sampling errors can significantly confound the diagnosis . 
ancillary cytogenetic studies such as fish can assist in differentiating between morphologically similar tumor specimens45 ; however , these tests frequently fail to identify a pathognomonic genetic abnormality and can occasionally produce false - positive results . the humanmethylation450 array is a rapid and cost - effective method for genome - wide quantitative profiling of the methylation of cpg loci.29 to explore the utility of dna - based methylation profiling in patients with sarcoma , we used a similar approach that has been shown to be highly accurate and reproducible in subclassifying other histologically similar tumors ( ie pediatric brain tumors ) .46 using random forest modeling , we developed a classifier that we successfully validated using ss and os samples from two publicly available datasets and an ews validation set obtained from a recently published series.33 in our training set , our classifier correctly identified all 36 samples as the tumor type determined by a combination of clinical , histologic , and table 3 . 
when applied to our validation cohorts ( tcga and target - os ) , all 10 ss samples and 85 of 86 of the os samples ( 99% ) were correctly classified . 
our analysis shows that the case target - 40pasefs may represent a tumor that is biologically related to ews , 47 as indicated by overexpression of ewsr1 and etv1 , illustrating the power and usefulness of methylation - based profiling for discovery . our study highlights the epigenetic heterogeneity present in ews despite a single recurrent oncogenic fusion driver . 
contingency table for validation set * pathology diagnosis random forest classification , validation set data ( n = 110 ) , no . abbreviations : ews , ewing sarcoma ; os , osteosarcoma ; ss , synovial sarcoma . * within the validation set , all patients were correctly classified within the the cancer genome atlas ( ss ) , huertas - martinez et al ( ews ) , and target - osteosarcoma ( target - os ) cohorts , with the exception of one sample from target - os ( target - 40 - pasefs ) that is classified as a es and one es sample from the huertas - martinez et al cohort that is classified as an ss . single test , thereby expediting the diagnosis . 
on the basis of positive fluorescent in situ hybridization analysis , the tumor was initially diagnosed as a synovial sarcoma ; however , multidimensional scaling plot of the classifier including the patients tumor ( red triangle ) ( c ) shows that the tumor classifies with osteosarcoma . 
 study comparing the performance and costeffectiveness of our methylation classifier and traditional immunohistochemical and fish testing could represent a fruitful avenue of research . in summary , we developed and validated a dna methylationbased classifier that accurately differentiated three of the most common subtypes of bone sarcomas . 
meyers stock and other ownership interests : amgen , bayer , e.i. dupont , henry schein , jazz pharmaceuticals , mednax , novartis , procter & gamble , sigma - aldrich honoraria : france foundation ( i ) consulting or advisory role : boehringer ingelheim ( i ) speakers bureau : france foundation ( i ) travel , accommodations , expenses : takeda , intermune ( i ) david j . 
pisapia no relationship to disclose richard gorlick stock and other ownership interests : oncolytics consulting or advisory role : oncolytics marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / boehringer ingelheim afatinib targeted therapy advisory committee , national comprehensive cancer network / astrazeneca tagrisso request for proposal advisory committee research funding : loxo ( inst ) kristen thomas no relationship to disclose matija snuderl stock and other ownership interests : arca biopharma , bluebird bio , cellceutix , epizyme , geron , isis pharmaceuticals , sevion therapeutics , acceleron pharma , catalyst pharmaceutical travel , accommodations , expenses : silicon biosystems matthias a . 
pisapia , weill cornell medical college , new york ; and richard gorlick , albert einstein college of medicine , bronx , ny . supported in part by kids of new york university langone and the friedberg charitable foundation and through the nih / nci cancer center support grant no . 
werier j , yao x , caudrelier jm , et al : a systematic review of optimal treatment strategies for localized ewings sarcoma of bone after neo - adjuvant chemotherapy . 
surg oncol 25 : 16 - 23 , 2016 isakoff ms , bielack ss , meltzer p , et al : osteosarcoma : current treatment and a collaborative pathway to success . j clin oncol 33 : 3029 - 3035 , 2015 4 . 
sorensen ph , lessnick sl , lopez - terrada d , et al : a second ewings sarcoma translocation , t ( 21 ; 22 ) , fuses the ews gene to another ets - family transcription factor , erg . 
nat genet 6 : 146 - 151 , 1994 jeon is , davis jn , braun bs , et al : a variant ewings sarcoma translocation ( 7 ; 22 ) fuses the ews gene to the ets gene etv1 . 
kaneko y , yoshida k , handa m , et al : fusion of an ets - family gene , eiaf , to ews by t ( 17 ; 22 ) ( q12 ; q12 ) chromosome translocation in an undifferentiated sarcoma of infancy . 
peter m , couturier j , pacquement h , et al : a new member of the ets family fused to ews in ewing tumors . oncogene 14 : 1159 - 1164 , 1997 12 . 
goldblum jr , folpe al , weiss sharon w : general considerations , in goldblum jr , folpe al , weiss sharon w , eds : enzinger and weisss soft tissue tumors . 
yen cc , chen wm , chen th , et al : identification of chromosomal aberrations associated with disease progression and a novel 3q13.31 deletion involving lsamp gene in osteosarcoma . 
kresse sh , ohnstad ho , paulsen eb , et al : lsamp , a novel candidate tumor suppressor gene in human osteosarcomas , identified by array comparative genomic hybridization . 
dragoescu e , jackson - cook c , domson g , et al : small cell osteosarcoma with ewing sarcoma breakpoint region 1 gene rearrangement detected by interphase fluorescence in situ hybridization . 
hill da , osullivan mj , zhu x , et al : practical application of molecular genetic testing as an aid to the surgical pathologic diagnosis of sarcomas : a prospective study . 
sturm d , orr ba , toprak uh , et al : new brain tumor entities emerge from molecular classification of cns - pnets . cell 164 : 1060 - 1072 , 2016 26 . 
hovestadt v , remke m , kool m , et al : robust molecular subgrouping and copy - number profiling of medulloblastoma from small amounts of archival tumour material using high - density dna methylation arrays . 
huertas - martnez j , court f , rello - varona s , et al : dna methylation profiling identifies ptrf / cavin - 1 as a novel tumor suppressor in ewing sarcoma when co - expressed with caveolin - 1 . 
raney bj , dreszer tr , barber gp , et al : track data hubs enable visualization of user - defined genome - wide annotations on the ucsc genome browser . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
kilpatrick se , ward wg , chauvenet ar , et al : the role of fine - needle aspiration biopsy in the initial diagnosis of pediatric bone and soft tissue tumors : an institutional experience . 
bridge rs , rajaram v , dehner lp , et al : molecular diagnosis of ewing sarcoma / primitive neuroectodermal tumor in routinely processed tissue : a comparison of two fish strategies and rt - pcr in malignant round cell tumors . 
 ntrk alterations in pediatric highrisk malignancies identied through european clinical sequencing programs constitute promising drug targets over the last 2 years , two neurotrophic - tropomyosin receptor tyrosine kinase ( ntrk ) inhibitors have been approved for a tissue - agnostic indication in adults and children , namely , larotrectinib and entrectinib both in the united states and europe . 
although ntrkfusionpositive malignancies are rare , patients with tumors harboring this alteration may greatly benet from those innovative targeted therapies . molecular characterization platforms have been set up in europe over the last 5 years to identify targetable alterations in tumors of individual pediatric patients and to guide therapeutic prioritization . 
mappyacts , coordinated in france ( molecular proling for pediatric and young adult cancer treatment stratication ; clinicaltrials.gov identier : nct02613962 ) , and in ( individualized form , coordinated in germany therapy for relapsed malignancies in childhood ; eudract number : 2018 - 000127 - 14 ) , are the largest european efforts , offering real - time clinical sequencing to relapsed or refractory or very high - risk pediatric patients from 13 european countries.1 - 3 they are part of the innovative therapies for children with cancer ( itcc ) precision medicine and new drug development program , matching patients tumor molecular proles to new drugs in early clinical trials . alterations of the ntrk 1 - 3 were recently investigated in approximately 3 , 500 pediatric tumor samples across tumor types , with fusions involving these genes being detected in 0.34% of samples and amplication , mutation , and mrna overexpression occurring less frequently.4 although ntrk fusions are druggable by selective ( eg , larotrectinib and entrectinib ) and less specic small molecules , 4 - 11 reports on response of nonfusion ntrk alterations to ntrk inhibitors ( ntrki ) are lacking to date.4 since its initiation in january 2016 until july 2020 , approximately 690 patients with relapsed , refractory , or very high - risk pediatric cancer have been screened through mappyacts , whereas approximately 1 , 100 patients were screened through the inform registry from february 2015 until july 2020 . 
apart in mappyacts patients inform who were included because of being very high risk at rst diagnosis , all other tumor samples were obtained at relapse or progression ( table 1 )  . ntrk fusions were the most frequent alterations ( n = 25 ) , with ntrk1 , 2 , 3 being involved in 9 / 25 , 8 / 25 , and 8 / 25 patients , respectively . 
even for previously not described fusions , the similar structure to known ntrk fusions , with conservation of the tyrosine kinase domain , supports the hypothesis of an activation of the tyrosine kinase domain of ntrk . single nucleotide variants ( snvs ) were detected in 14 tumors ( 3 ntrk1 , 7 ntrk2 , and 4 ntrk3 ) , with six snvs being located in the kinase domain of the respective protein , one snv each in the immunoglobulin i - set domain and the leucine - rich domain , respectively , and the remaining six snvs falling outside of annotated functional domains . two cases harbored a focal amplication of ntrk1 genomic locus . a total of 17 patients with tumors harboring an ntrk fusion were treated with the specic ntrki larotrectinib . 
of these , four patients from germany , four patients from sweden , four patients from france , and one patient from poland were enrolled in an early phase clinical trial . 
complete resection of the tumor , stabilization with conventional therapy , missing availability of the drug ( before the initiation of pediatric trials ) , and loss to follow - up were stated as reasons not to treat with ntrki . 
one patient with ntrk1 amplication as nonfusion ntrk alteration received larotrectinib in a clinical trial setting . through this pan - european initiative , we demonstrate the feasibility and value of next - generation sequencing to identify children and adolescents with an ntrk tumor alteration - harboring malignancy ( across all types ) who may be eligible for ntrki therapy . addition , it allows the capture of all potential ntrk fusion partners and novel snvs in functionally relevant domains of ntrk . 
the current development of additional pediatric sequencing programs ( ie , smpaeds in the united kingdom , ither in the netherlands , and the danish program ) as part of the itcc strategy will provide an expanded access to targeted agents for children and adolescents across europe . elke pfaff , md hopp childrens cancer center heidelberg ( kitz ) , heidelberg , germany ; pediatric glioma research group , german cancer research center ( dkfz ) , heidelberg , germany ; department of pediatric oncology , hematology and immunology , heidelberg university hospital , heidelberg , germany tiphaine adam de beaumais , md clinical research department , gustave roussy cancer center , villejuif , france antonin marchais , phd bioinformatics and inserm u1015 , gustave roussy cancer center , university paris - saclay , villejuif , france cornelis m . 
van tilburg , md hopp childrens cancer center heidelberg ( kitz ) , heidelberg , germany ; department of pediatric oncology , hematology and immunology , heidelberg university hospital , heidelberg , germany ; clinical cooperation unit pediatric oncology , german cancer research center ( dkfz ) , heidelberg , germany german cancer consortium ( dktk ) , germany ; kitz clinical trial unit , hopp childrens cancer center heidelberg ( kitz ) , german cancer research center ( dkfz ) and heidelberg university hospital , heidelberg , germany mirjam blattner - johnson , phd hopp childrens cancer center heidelberg ( kitz ) , heidelberg , germany ; pediatric glioma research group , german cancer research center ( dkfz ) , heidelberg , germany uta dirksen , md german cancer consortium ( dktk ) , partner essen , germany ; university hospital essen , pediatrics iii , hematology and oncology , west german cancer centre , essen , germany ingrid ra , md , phd department of pediatric oncology and hematology , karolinska university hospital , solna , sweden ; skane university hospital , lund , sweden birgit geoerger , md , phd department of pediatric and adolescent oncology , gustave roussy cancer center , inserm u1015 , university parissaclay , villejuif , france gudrun schleiermacher , md equipe siric rtop recherche translationelle en oncologie p ediatrique , institut curie , paris , france ; siredo : care , innovation and research for children , adolescents and young adults with cancer , institut curie , paris , france stefan m . 
 correspondence hematology and immunology , heidelberg university hospital , heidelberg , germany ; division of pediatric neurooncology , german cancer consortium ( dktk ) and german cancer research center ( dkfz ) , heidelberg , germany data analysis and interpretation : elke pfaff , antonin marchais , ingrid ra , birgit geoerger , gudrun schleiermacher , stefan m . 
the inform project is nancially supported by the german consortium for translational cancer research ( dktk ) , german cancer aid , the german childhood cancer foundation , the german cancer research center ( dkfz ) , bild e.v. 
pster provision of study materials or patients : elke pfaff , uta dirksen , ingrid ra , birgit geoerger , olaf witt collection and assembly of data : elke pfaff , tiphaine adam de beaumais , antonin marchais , cornelis m . 
van tilburg consulting or advisory role : novartis , bayer uta dirksen consulting or advisory role : lilly , ipsen ingrid ra consulting or advisory role : bayer birgit geoerger consulting or advisory role : roche or genentech , merck kgaa , boehringer ingelheim , bayer , azd , novartis gudrun schleiermacher honoraria : bristol - myers squibb research funding : bristol - myers squibb , pzer , msdavenir , roche travel , accommodations , expenses : roche stefan m . 
pster research funding : lilly , bayer , roche , pharmamar , pzer patents , royalties , other intellectual property : patent on utilizing dna methylation proling for tumor classication olaf witt consulting or advisory role : novartis , astrazeneca , janssen research & development , bristol - myers squibb , roche , bayer , dayonetx research funding : biomed valley discoveries david t.w. 
worst bc , van tilburg cm , balasubramanian gp , et al : next - generation personalised medicine for high - risk paediatric cancer patients : the inform pilot study . 
harttrampf ac , lacroix l , deloger m , et al : molecular screening for cancer treatment optimization ( moscato - 01 ) in pediatric patients : a singleinstitutional prospective molecular stratication trial . 
 correspondence berlanga p , pierron g , lacroix l , et al : can pediatric and adolescent patients with recurrent tumors benet from a precision medicine program ? the european mappyacts experience . 
j clin oncol 37 , 2019 ( suppl ; abstr 10018 ) okamura r , boichard a , kato s , et al : analysis of ntrk alterations in pan - cancer adult and pediatric malignancies : implications for ntrk - targeted therapeutics . 
cancer discov 7 : 400 - 409 , 2017 laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
lancet oncol 19 : 705 - 714 , 2018 konicek bw , capen ar , credille km , et al : merestinib ( ly2801653 ) inhibits neurotrophic receptor kinase ( ntrk ) and suppresses growth of ntrk fusion bearing tumors . 
oncotarget 9 : 13796 - 13806 , 2018 van tilburg cm , dubois sg , albert cm , et al : larotrectinib efcacy and safety in pediatric trk fusion cancer patients . 
j clin oncol 37 , 2019 ( suppl ; abstr 10010 ) robinson gw , gajjar aj , gauvain km , et al : phase 1 / 1b trial to assess the activity of entrectinib in children and adolescents with recurrent or refractory solid tumors including central nervous system ( cns ) tumors . 
hong ds , dubois sg , kummar s , et al : larotrectinib in patients with trkfusionpositive solid tumours : a pooled analysis of three phase 1 / 2 clinical trials . 
robson , md10 purpose screening and prevention decisions for women at increased risk of developing breast cancer depend on genetic and clinical factors to estimate risk and select appropriate interventions . 
a combined risk score ( crs ) of an 86single - nucleotide polymorphism polygenic risk score and the tyrer - cuzick v7.02 clinical risk estimator was generated with attenuation for confounding by family history . 
calibration and discriminatory accuracy of the crs were evaluated in two independent validation cohorts of women of european ancestry ( n = 1 , 615 and n = 518 )  . 
risk stratication with a 20% risk threshold was compared between crs and tyrer - cuzick in an independent clinical cohort ( n = 32 , 576 )  . results simulation studies conrmed that the fixed - stratied method produced accurate risk estimation across patients with different family history . 
in an analysis with both crs and tyrer - cuzick as predictors of breast cancer , crs added signicant discrimination independent of that captured by tyrer - cuzick ( p , 1011 in validation 1 ; p , 107 in validation 2 )  . 
in an independent cohort , 18% of women shifted breast cancer risk categories from their tyrer - cuzickbased risk compared with risk estimates by crs . conclusion integrating clinical and polygenic factors into a risk model offers more effective risk stratication and supports a personalized genomic approach to breast cancer screening and prevention . jco precis oncol 5 : 307 - 316 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction mammography and adjuvant treatment of early - stage disease are widely used for the mitigation of morbidity and mortality in invasive breast cancer.1 effective prevention requires the identication of higher - risk individuals , which has typically involved family history evaluation , assessment of clinical and lifestyle factors , and testing for the presence of pathogenic variants ( pvs ) in a limited number of highor moderate - risk breast cancer genes.2 although guidelines for pv carriers have long recommended enhanced screening and discussion of surgical prevention measures , they do not adequately address the increased risk for unaffected pv - negative women with a strong family history of breast cancer . 
we examined confounding and interaction between an 86 - snp polygenic risk score and each clinical factor in the tyrer - cuzick model to inform the development of a combined clinical and polygenic risk score . 
20% lifetime risk of developing breast cancer . improved risk stratication from the combined risk score can help target the use of more intense screening strategies for unaffected women with truly elevated risk based on clinical and genetic factors . here , we describe the development and validation of a strategy for integrating a snp score with a validated clinical risk model , with attenuation for correlated effects . 
clinical testing cohort data were subdivided according to successive time intervals to ensure the independence of development and validation activities ( fig 1 ) ; this included two development sets ( development 1 and 2 ) , one validation set ( validation 1 ) , and one clinical performance population . 
genetic testing for all patients was performed at a clinical laboratory improvement amendments - approved and college of american pathology - approved laboratory ( myriad genetics , inc . , salt lake city , ut ) by next - generation sequencing.34 hybridization probes for the 86 snps in the prs were included in the sequencing panel.33 women were eligible if they were of age 18 - 84 years , of european ancestry ( ashkenazi and non - ashkenazi ; selfreported ) , and negative for likely pvs or pvs in 11 breast cancerrelated genes ( brca1 , brca2 , tp53 , pten , stk11 , cdh1 , palb2 , chek2 , atm , nbn , and bard1 )  . patients were excluded as unaffected controls if they reported a history of ductal carcinoma in situ , lobular carcinoma in situ , hyperplasia , or unspecied breast disease . women were excluded from the clinical testing cohort if they were submitted from states that disallow the research use of samples after completion of genetic testing . 
all studies were conducted with institutional review board ( irb ) oversight ( quorum review irb #31713 , 32556 , 32608 )  . development 1 included women from the clinical testing cohort unaffected by cancer of any type accrued between june 1 , 2017 and august 11 , 2017 ( n = 5 , 489 )  . 
development 2 ( n = 141 , 160 ) included 112 , 232 women unaffected by breast cancer and 28 , 928 breast cancer cases from the clinical testing cohort accrued between august 11 , 2017 and january 11 , 2019 . 
clinical characteristics of this set were previously reported.33 validation 1 consisted of women in the clinical testing cohort accrued between june 1 , 2017 and august 10 , 2017 ( n = 1 , 615 )  . 
controls included unaffected women submitted for genetic testing because of possible hereditary nonpolyposis colorectal cancer syndrome as these patients have a breast cancer family history consistent with that of general population controls . for validation 2 , a consecutive series of women who presented to four breast cancer screening centers ( elizabeth wende breast care , the breast center of nwa , bethesda health , and cuda women 's health center / cape cod healthcare ) were prospectively recruited between february 6 , 2017 and november 11 , 2017 ( n = 518 )  . 
 integrating clinical and polygenic factors to predict cancer risk cohort description noisulcni noisulcxe accrual findings development n = 5 , 489 clinical testing cohort : 18 - 84 years old , european ancestry , pv - negative , from states that allow research use of data or samples post - testing history of breast cancer , dcis , lcis , hyperplasia , or unspecified breast disease ; eligible for validation set 1 development n = 141 , 160 clinical testing cohort : same inclusion criteria as development set 1 controls could not have a history of dcis , lcis , hyperplasia , or unspecified breast disease validation 1 clinical testing cohort : same basic inclusion or exclusion criteria as development set 2 cases : breast cancer diagnosis , submitted for testing due to suspicion of hboc within 1 year of diagnosis controls : unaffected women submitted for testing due to suspicion of hnpcc prospectively acquired case - control study enrolled from imaging centers cases : pathologically confirmed first diagnosis of invasive breast cancer 12 mos . preenrollment or incident breast cancer 6 mos . 
for each factor , we conducted a simple linear regression with prs as the dependent variable and the clinical factor as the independent variable . from these models , we examined regression coefcients , p values based on f - statistics , and pearson correlation coefcients . design of the combined risk score . 
to calculate absolute risk incorporating tyrer - cuzick and prs , we developed a fixed - stratied method ( data supplement ) to attenuate prs after xing the effects of confounded factors from the tyrer - cuzick model and to constrain risk separately within strata of the confounders . 
absolute risk for a woman in strata k was calculated as follows : ( cid : 3 ) exp { prs + ck } , ( cid : 1 ) 1 tc where represents the per - unit log ( or ) of the prs from a multivariable logistic regression model with the effect of breast cancer family history xed . 
the combined risk score ( crs ) was validated in two independent studies ( table 1 ) : a clinical testing set ( validation 1 ; n = 1 , 615 ) and the prospective case - control cohort ( validation 2 ; n = 518 )  . 
exploratory analyses tested calibration of the crs by comparing average absolute risk estimates with those from the tyrer - cuzick model ; with proper calibration , we expected to observe the same average risk for tyrer - cuzick as for the crs among unaffected controls . 
these analyses were conducted separately for rlr and 5 - year risk of developing breast cancer . weighted logistic regression was used with weights for unaffected controls calculated such that average tyrercuzick rlr matched general population rates ( data supplement )  . performance of the 86 - snp prs . 
in contrast , for women with family history , the fixed - stratied method matched risks from multivariable co - estimation , whereas the unadjusted model overestimated risk ( data supplement )  . clinical validations validation 1 included 988 ( 61% ) breast cancer cases and 627 ( 39% ) unaffected controls ( table 1 )  . 
overall , 362 ( 22% ) patients reported breast cancer in 1 rst - degree relative and 620 ( 38% ) in 1 second - degree relative . the prospectively collected case - control validation 2 included 256 ( 49% ) breast cancer cases and 262 ( 51% ) unaffected controls ( table 1 )  . 
nearly one third ( 29% ) of patients reported breast cancer in a rst - degree relative and 204 ( 39% ) patients in 1 second - degree relative . in both validations , rlr and 5 - year risk estimates of the crs and tyrer - cuzick were signicantly associated with breast cancer ( table 2 and fig 2 )  . 
in a model with both risk predictors , the crs added signicant discrimination independent of that captured by tyrer - cuzick for both rlr ( p , 1011 in validation 1 ; p , 107 in validation 2 ) and 5year risk ( p , 1011 in validation 1 ; p , 107 in validation 2 ; data supplement )  . although all patients in validation 2 provided complete tyrer - cuzick risk factor questionnaires , data on tyrercuzick variables were incomplete for some patients in validation 1 . 
analyses were repeated in the subset of patients with complete information for all tyrer - cuzick risk factors with results similar to those from the full data set ( data supplement )  . calibration of the crs was examined by comparing average risk estimates with those from tyrer - cuzick in the control samples from either validation . 
 hughes et al average remaining lifetime risk in validation cohort 1 ( n = 627 ) average 5 - year risk in validation cohort 1 ( n = 627 ) crs mean ( 95% ci ) tyrercuzick mean ( 95% ci ) fig 3 . 
estimates for average remaining lifetime ( a and c ) and 5 - year risk ( b and d ) for unaffected controls in validation 1 ( a - b ) and validation 2 ( c - d )  . patients were grouped into 5 - year age bins , and average risks were evaluated according to crs and tyrer - cuzick . 95% cis are also reported . 
addition of the 86 - snp score signicantly improved discrimination relative to the tyrer - cuzick model for predicting risk of breast cancer , and the crs model showed excellent calibration across age groups . 
20% - 25% lifetime risk of breast cancer to improve early - stage cancer detection.36 in a clinical testing population , we showed that for 33% of pv - negative women , the crs - estimated risk was  . 
distribution of crs risk estimates in unaffected women . remaining lifetime risk ( rlr ) in a population of unaffected women ( clinical performance population , n = 32 , 576 ; excluded women with ductal carcinoma in situ , lobular carcinoma in situ , hyperplasia , or unspecied breast disease ) according to crs with thresholds at 20% ( increased ) and 50% ( high ) rlr . 
blue squares indicate patients with discordance between the scores ( eg , the tyrer - cuzick model produced a score that indicated a patient had low rlr , but the same patient was determined to have increased rlr by the crs model )  . 
crs , combined risk score . performance integrating clinical and polygenic factors to predict cancer risk increased risk ( crs > 20% ) 33.1% high risk ( crs > 50% ) 0.6% 3000 2500 2000 1500 1000 rlr according to crs ( % ) remaining lifetime risk according to tyrer - cuzick ( 20% ) increased ( > 20% ) crs total 56.5% n = 18 , 398 10.5% n = 3 , 407 67.0% n = 21 , 805 8.0% n = 2 , 619 25.0% n = 8 , 152 33.0% n = 10 , 771 64.5% n = 21 , 017 35.5% n = 11 , 559 100% n = 32 , 576 tyrer - cuzick or crs - based risk discordant increased risk ( > 20% ) high risk ( > 50% ) tyrer - cuzick remaining lifetime risk ( % ) women ( 8% ) who would have been categorized as , 20% using tyrer - cuzickestimated risk alone . combinations of prss with the tyrer - cuzick model have been presented previously , generally without attenuation for confounding . 
an 88 - snp score was added to tyrercuzick under the assumption of independence in a nested case - control study.25 although the snp score added disit had poor crimination to the tyrer - cuzick prediction , calibration . 
first , previous examinations of confounding often evaluated the correlations between a prs and a model rather than individual clinical factors.21 , 25 , 26 this approach might have obscured associations between prs and clinical factors with a stronger genetic component . 
second , genetic overlap is more likely with a larger prs since casting a wider for cancer - associated snps is more likely to also the genetic component of capture a larger fraction of clinical risk . 
1 rst - degree relative or those with second - degree relatives . limitations of the present study include a potential ascertainment bias in the clinical testing population cohorts . qualication for genetic testing is often based on family history . 
it has been previously shown that this potential bias can be avoided by accounting for family history in a multivariable model.38 , 39 consequently , all analyses presented here were conducted by multivariable co - estimation . 
in support of this approach , results from validation 1 ( clinical testing samples ) were similar to results obtained in validation 2 , for which participants were prospectively collected and were unaffected by potential bias due to selection for hereditary cancer testing . 
evaluation of the crs in a prospectively collected , unselected populationbased sample is being pursued.40 future work to expand assessment tools such as tyrer - cuzick and the prs for non - european ancestries will be required to apply these tools to other ancestry populations . 
however , subanalysis of validation 1 in women with complete tyrer - cuzick information showed similar results as the whole data set , indicating that missing information did not substantially affect the analysis . this crs model is suitable for reporting age - specic risk of developing breast cancer for unaffected women of european descent with or without signicant family history . 
it is currently the only tyrer - cuzickbased model fully adjusted for the shared risk between snps and family history and is therefore less likely to overestimate risk in women with a family history of breast cancer . 
lanchbury data analysis and interpretation : elisha hughes , placede tshiaba , susanne wagner , eric rosenthal , benjamin roa , shannon gallagher , stephanie meek , wade hedegard , susan m . 
 integrating clinical and polygenic factors to predict cancer risk benjamin roa employment : myriad genetics leadership : myriad genetics stock and other ownership interests : myriad genetics research funding : myriad genetics patents , royalties , other intellectual property : intellectual property held by employer myriad genetics travel , accommodations , expenses : myriad genetics shannon gallagher employment : myriad genetics stock and other ownership interests : myriad genetics stephanie meek employment : myriad genetics stock and other ownership interests : myriad genetics kathryn dalton speakers bureau : myriad genetics danna f . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca , clovis oncology judy garber consulting or advisory role : novartis , gtx , helix biopharma , konica minolta , aleta biotherapeutics , h3 biomedicine , kronos bio research funding : novartis , ambry genetics , invitae , myriad genetics other relationship : susan g . 
lanchbury employment : myriad genetics leadership : myriad genetics stock and other ownership interests : myriad genetics patents , royalties , other intellectual property : i am an inventor on multiple patents led by myriad genetics travel , accommodations , expenses : myriad genetics alexander gutin employment : myriad genetics stock and other ownership interests : myriad genetics , gilead sciences mark e . 
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jco precis oncol 4 : 585 - 592 , 2020 judkins t , leclair b , bowles k , et al : development and analytical validation of a 25 - gene next generation sequencing panel that includes the brca1 and brca2 genes to assess hereditary cancer risk . 
newberg , phd3 ; meagan montesion , phd3 ; and peter mu - hsin chang , md , phd1 , 2 introduction salivary gland tumors comprise a rare group of neoplasms that arise from salivary ducts , most of which are benign.1 the parotid gland is the most frequently involved site and comprises more than 80% of salivary tumors.2 of the parotid tumors , approximately 75% are benign , whereas the remaining 25% are malignant.3 the most frequent subtype of malignant salivary gland cancer is mucoepidermoid carcinoma , followed by adenoid cystic carcinoma.4 salivary gland tumors have been linked to exposure to high ultraviolet radiation.5 salivary gland cancer has a poor prognosis ( 5 - year overall survival , 50% ) and a high propensity for recurrence.6 the mainstay of treatment of salivary gland cancers is surgery in patients with early and locally advanced disease.7 in metastatic or recurrent disease , consensus is lacking on the optimal regimen for systemic chemotherapy.8 the low prevalence of this disease precludes large - scale randomized trials , and current clinical data are mostly derived from small clinical studies . 
current data , although dated , support cisplatin , anthracyclines , uorouracil , and cyclophosphamide as active agents against salivary gland cancer.9 - 11 in general , response to chemotherapy is limited ( a review of response to chemotherapy was published by laurie and licitra , 12 with response rates mostly ranging from 10% to 30% ) , and chemotherapy is mostly for palliative control.8 , 12 experts have urged a coordinated effort for clinical trials to further elucidate the role of chemotherapy in this patient group , 12 but this proves to be difcult , owing to the rarity of this cancer . the success of epidermal growth factor receptor ( egfr ) inhibitors in head and neck cancers13 and lung cancers14 has sparked hope for the possibility of use in salivary gland tumors because egfr is sometimes upregulated in this disease group.15 however , attempts to use egfr inhibitors , such as getinib and cetuximab , have largely been disappointing , with limited response.16 , 17 multiple mechanisms have been proposed for the lack of response to egfr inhibition in salivary gland cancers.18 to gain additional insight into the egfr expression pattern in salivary gland cancers , the dna and protein status of more than 800 tumor samples were analyzed for egfr gene alteration and protein levels in a retrospective study.19 the study revealed a high frequency of egfr low prevalence of egfr gene protein expression , mutation , and , more interestingly , no occurrence of egfr gene amplication . this is signicantly different from studies of head and neck squamous cell carcinomas , in which the prevalence of egfr amplication has been reported to be 17%20 and was linked to worse clinical outcome . 
interestingly , studies in colorectal cancer have shown that egfr gene amplication is linked to better outcomes and response to cetuximab.21 , 22 conversely , egfr amplication is proposed as an intrinsic resistance mechanism in lung cancer , 23 although other studies report conicting results , demonstrating egfr amplication associated with better outcomes with tyrosine kinase inhibitors ( tkis ) in patients with advanced nonsmall - cell lung cancer.24 therefore , the exact role of egfr amplication in response to egfr inhibition therapy remains to be claried . in this case report , we describe an unusual patient with a salivary gland cancer , refractory to initial chemotherapy agents but demonstrating signicant response to afatinib , an egfr and human epidermal growth factor receptor 2 tki . 
 ( c ) a computed tomography scan was performed 3 months after starting afatinib , showing marked decrease in size of the tumor ( right )  . pathology studies conrmed the diagnosis of high - grade salivary ductal carcinoma with inltration to the nontumor portion of the parotid gland . 
copy number ( cn ) plot ( top ) and minor allele frequency plot ( bottom ) showing marked increase in copy number of epidermal growth factor receptor . after discussion with the patient , the decision was made to initiate a therapeutic regimen of the egfr inhibitor afatinib ( 40 mg , every other day )  . 
written informed consent for publication of this case report was obtained from the patient . discussion afatinib is a tki that irreversibly inhibits the human egfr and human epidermal growth factor receptor 2 kinases.26 it has proven clinical activity and is approved for treatment of nonsmall - cell lung cancer with mutant egfr27 ( as shown in the lux - lung 3 and lux - lung 6 trials )  . 
interestingly , afatinib showed signicant activity against tumors harboring the deletion of exon 19 in egfr , while lacking activity against the common l858r point mutation , 27 , 28 highlighting the differences in biology between different egfr mutation types.29 afatinib was shown to be effective in advanced head and neck cancers , with benet progression - free survival30 , 31 ; however , little data exist for afatinib in salivary gland cancers . although some subtypes of salivary gland tumors exhibit egfr overexpression , 15 it is generally established that egfr inhibitors such as cetuximab are ineffective against salivary gland tumors . 
mechanistically , egfr amplication has been linked to higher spatial density of the receptor and thus linked to heightened dimerization and signaling.32 interestingly , as described in a recent case report , a patient with triple - negative breast cancer with egfr amplication was also successfully treated with cetuximab.33 a recent study retrospectively investigated a subgroup of esophageal cancers with egfr amplication.34 although previous studies have failed to demonstrate efcacy of egfr inhibition in esophageal cancers , 35 this study demonstrated a high response rate ( objective response rate , 58% ; disease control rate , 100% ) in this patient population.34 the ndings in our case report are in line with the aforementioned studies , highlighting the prognostic value of egfr amplication with treatment with egfr inhibitors . 
our patient is unique in that egfr amplication is extremely rare in salivary gland tumors , 19 compared with higher prevalence in triple - negative breast cancer ( up to 92% ) 36 or in esophageal cancer ( 7% ) .37 these reports that egfr amplication may indicate a favorsuggest able response to egfr inhibitors , regardless of the tumor site . 
this highlights the importance of genetic proling of individual tumors to determine personalized treatment of patients . in conclusion , we report a patient with a high copy number of egfr who demonstrated good response to egfr inhibition therapy . 
newberg employment : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : im on a patent stemming from research in my graduate school days related to identifying location biomarkers using imaging techniques . 
head neck surg 8 : 177 - 184 , 1986 liu y , li h , qin l , et al : prognostic factors in malignant sublingual salivary gland tumors . 
j oral maxillofac surg 75 : 1542 - 1548 , 2017 spitz mr , sider jg , newell gr , et al : incidence of salivary gland cancer in the united states relative to ultraviolet radiation exposure . 
head neck surg 10 : 305 - 308 , 1988 johnston ml , huang sh , waldron jn , et al : salivary duct carcinoma : treatment , outcomes , and patterns of failure . 
head neck 38 : e820 - e826 , 2016 ( suppl 1 ) lewis ag , tong t , maghami e : diagnosis and management of malignant salivary gland tumors of the parotid gland . 
otolaryngol clin north am 49 : 343 - 380 , 2016 aleri s , granata r , bergamini c , et al : systemic therapy in metastatic salivary gland carcinomas : a pathology - driven paradigm ? oral oncol 66 : 58 - 63 , 2017 licitra l , cavina r , grandi c , et al : cisplatin , doxorubicin and cyclophosphamide in advanced salivary gland carcinoma . 
proc natl sci counc repub china b 25 : 90 - 96 , 2001 jakob ja , kies ms , glisson bs , et al : phase ii study of getinib in patients with advanced salivary gland cancers . 
chen z , chen j , gu y , et al : aberrantly activated areg - egfr signaling is required for the growth and survival of crtc1 - maml2 fusion - positive mucoepidermoid carcinoma cells . 
temam s , kawaguchi h , el - naggar ak , et al : epidermal growth factor receptor copy number alterations correlate with poor clinical outcome in patients with head and neck squamous cancer . 
hirsch fr , herbst rs , olsen c , et al : increased egfr gene copy number detected by uorescent in situ hybridization predicts outcome in non - small - cell lung cancer patients treated with cetuximab and chemotherapy . 
nukaga s , yasuda h , tsuchihara k , et al : amplication of egfr wild - type alleles in non - small cell lung cancer cells confers acquired resistance to mutationselective egfr tyrosine kinase inhibitors . 
cappuzzo f , hirsch fr , rossi e , et al : epidermal growth factor receptor gene and protein and getinib sensitivity in non - small - cell lung cancer . 
sk alov a a , vanecek t , sima r , et al : mammary analogue secretory carcinoma of salivary glands , containing the etv6 - ntrk3 fusion gene : a hitherto undescribed salivary gland tumor entity . 
solca f , dahl g , zoephel a , et al : target binding properties and cellular activity of afatinib ( bibw 2992 ) , an irreversible erbb family blocker . 
yang jc , wu yl , schuler m , et al : afatinib versus cisplatin - based chemotherapy for egfr mutation - positive lung adenocarcinoma ( lux - lung 3 and lux - lung 6 ) : analysis of overall survival data from two randomised , phase 3 trials . 
kato t , yoshioka h , okamoto i , et al : afatinib versus cisplatin plus pemetrexed in japanese patients with advanced non - small cell lung cancer harboring activating egfr mutations : subgroup analysis of lux - lung 3 . 
kaneda t , yoshioka h , tamiya m , et al : differential efcacy of cisplatin plus pemetrexed between l858r and del - 19 in advanced egfr - mutant non - squamous non - small cell lung cancer . 
machiels jp , haddad ri , fayette j , et al : afatinib versus methotrexate as second - line treatment in patients with recurrent or metastatic squamous - cell carcinoma of the head and neck progressing on or after platinum - based therapy ( lux - head & neck 1 ) : an open - label , randomised phase 3 trial . 
clement pm , gauler t , machiels jp , et al : afatinib versus methotrexate in older patients with second - line recurrent and / or metastatic head and neck squamous cell carcinoma : subgroup analysis of the lux - head & neck 1 trial . 
suntharalingam m , winter k , ilson d , et al : effect of the addition of cetuximab to paclitaxel , cisplatin , and radiation therapy for patients with esophageal cancer : the nrg oncology rtog 0436 phase 3 randomized clinical trial . 
 c dramatic response to sequential braf inhibition in braf v600emutant metastatic lung adenocarcinoma introduction lung [ aq1 ] [ aq2 ] cancer is the leading cause of cancer related death.1 targeted therapy directed toward molecular pathways that drive nonsmall - cell lung cancer ( nsclc ) has dramatically improved treatment options . 
some of the oncogenic drivers identified in lung adenocarcinoma involve the ras - raf - mitogen - activated protein kinase ( mapk ) kinase ( mek ) - extracellular regulated kinase ( erk ) pathway ( mapk - erk pathway ) .2 braf is a key protein in mapk - erk signaling . 
 mutations in braf [ aq3 ] are present in 1% to 3% of nsclc and lead to constitutive activation of the mapk - erk pathway , promoting cancer cell proliferation and survival . 
several other mutations of braf have been identified and are grouped as non - v600e mutations.3 patients with nsclc harboring braf v600e mutations are sensitive to braf inhibitors ( brafis ) alone or in combination with mek inhibitors ( mekis ) .4 - 6 after initial response , patients typically experience relapse as a result of various resistance mechanisms . 
imaging revealed a left - side hilar lung mass , enlarged mediastinal lymph nodes , vertebral body sclerotic lesions , small bilateral pleural effusions , and a pericardial effusion consistent with metastatic disease . 
the repeat biopsy specimen was sent for massively parallel dna sequencing using the illumina hiseq2000 platform ( foundation medicine , cambridge , ma ) to characterize base substitutions , short insertions and deletions , copy number alterations , and selected fusions across 287 cancer - related genes . 
several tumor mutations , including braf v600e , mapk1 ( r306h ) , smad4 ( r361c ) , and setd2 ( splice site 65_71 + 13del20 ) , were identified . 
 a through lymphangitic spread ( fig 2 ) that required oxygen supplementation at 5 l / min and showed malignant involvement of the right - side iliopsoas muscle , which caused significant pa after palliative radiation to the right - side pelvic mass for pain control , he began a combination of dabrafenib 150 mg twice daily and trametinib 2 mg daily . 
at the same time , the patient became oxygen independent , and functional status improved , which allowed him to fulfill his desire to travel to his home country to visit family . more than 5 months later , after dose reduction for grade 3 fatigue , his lung mass again increased in size . 
by that point , he had survived 3.5 years since diagnosis of nsclc with a response duration of 12 months on braf targeted therapy . discussion in this era of personalized medicine , targeted therapies against braf v600e and mek have changed the standard of care in the treatment of braf - mutated metastatic melanoma . 
two brafis , dabrafenib and vemurafenib , with or without mekis , trametinib and cobimetinib , are approved for braf v600emutant metastatic melanoma.7 , 8 such targeted medications also have clinical activity in braf v600emutant nsclc.4 - 6 , 9 , 10 in a retrospective analysis of the european euraf cohort , 35 patients with braf - mutant nsclc treated with brafis were identified . 
after first - line therapy with brafis , overall survival ( os ) was 25.3 months in patients with braf v600emutant nsclc ( n = 29 ) and 11.8 months in patients with nonv600e braf mutations ( n = 6 ) .9 response to chest before and after initiation of vemurafenib , at 2 weeks , and at 3 months demonstrated a significant decrease in the size of the rightside upper - lobe mass [ aq4 ] and improvement of the air space disease , with an overall decrease in tumor volume of greater than 90% ( fig 1 )  . 
the dosage of vemurafenib was reduced twice for grade 3 fatigue , recurrent grade 2 skin rash , and transaminitis . after maintaining response for 7 months on vemurafenib , the patients tumor burden escalated fig 1 . 
computed tomography scans of chest demonstrating response to combination dabrafenib and trametinib treatment brafis also was documented in a phase ii basket trial of vemurafenib in braf v600mutant positive nonmelanoma cancers with an overall response rate ( orr ) of 42% in 20 patients with nsclc.10 in a prospective multicenter phase ii clinical trial , planchard et al5 evaluated the safety and efficacy of dabrafenib trametinib in nsclc . 
previously treated patients ( n = 78 ) and treatment - nave patients ( n = 6 ) responded to dabrafenib alone with a median progression - free survival ( pfs ) of 5.5 months , a median os of 12.7 months , and an orr of 33% . 
testing for braf is recommended as part of the initial molecular analysis in patients with lung cancer of adenocarcinoma histology and is considered in some patients with squamous subtype.11 all patients with braf v600emutant nsclc eventually progress after brafis with or without mekis . 
resistance mechanisms are not as well characterized in nsclc compared with braf v600emutant melanoma.12 secondary resistance mechanisms in melanoma include ras mutations , braf splice variants , braf v600 amplifications , mek1 / 2 mutations , and non - mapk pathway alterations.13 in nsclc , lin et al14 described two classes of resistance patterns to vemurafenib using a preclinical model of hcc364 braf v600emutant lung cancer cells . 
in contrast , expression of c - junmediated egfr ligands that promote continued egfr signaling represents another class.14 plx9394 , a novel brafi , evades resistance caused by alternatively spliced truncated braf v600e , but subsequent resistance occurs through egfr - mediated ras - mammalian target of rapamycin signaling.15 in the clinical setting , kras , tp53 , and cdkn2a mutations were acquired in one patient after progression on dabrafenib.16 currently , there is no standard therapy for patients with braf v600emutant nsclc after progression on brafis . 
in a phase i / ii study , the combination of brafi and meki was evaluated in patients with braf v600mutant metastatic melanoma who had disease progression on a single - agent brafi . 
one of these patients had a partial response to dabrafenib monotherapy after prior treatment with vemurafenib.9 another case report showed a similar response ; a patient who progressed on vemurafenib achieved a 3 - month clinical benefit with single - agent dabrafenib.18 our patient attained clinical response for an additional 5 months with an alternative brafi , dabrafenib , combined with the meki trametinib after progression on vemurafenib . 
two prior case studies described the benefit of combination treatment after progression on initial brafi monotherapy.19 , 20 similar to our patient , schmid et al19 reported on a patient who responded to combination dabrafenib and trametinib for 6 months after progression on vemurafenib . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . sushma jonna no relationship to disclose affiliations all authors : georgetown university , washington , dc . clinical trials or have already progressed on other lines of therapy . 
chen d , zhang lq , huang jf , et al : braf mutations in patients with non - small cell lung cancer : a systematic review and meta - analysis . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) - mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
planchard d , kim tm , mazieres j , et al : dabrafenib in patients with braf ( v600e ) - positive advanced non - small - cell lung cancer : a single - arm , multicentre , open - label , phase 2 trial . 
planchard d , smit ef , groen hjm , et al : dabrafenib plus trametinib in patients with previously untreated brafv600e - mutant metastatic non - small - cell lung cancer : an open - label , phase 2 trial . 
lindeman ni , cagle pt , aisner dl , et al : updated molecular testing guideline for the selection of lung cancer patients for treatment with targeted tyrosine kinase inhibitors : guideline from the college of american pathologists , the international association for the study of lung cancer , and the association for molecular pathology . 
johnson db , menzies am , zimmer l , et al : acquired braf inhibitor resistance : a multicenter meta - analysis of the spectrum and frequencies , clinical behaviour , and phenotypic associations of resistance mechanisms . 
okimoto ra , lin l , olivas v , et al : preclinical efficacy of a raf inhibitor that evades paradoxical mapk pathway activation in protein kinase braf - mutant lung cancer . 
rudin cm , hong k , streit m : molecular characterization of acquired resistance to the braf inhibitor dabrafenib in a patient with braf - mutant non - small - cell lung cancer . 
johnson db , flaherty kt , weber js , et al : combined braf ( dabrafenib ) and mek inhibition ( trametinib ) in patients with brafv600 - mutant melanoma experiencing progression with single - agent braf inhibitor . 
schmid s , siano m , joerger m , et al : response to dabrafenib after progression on vemurafenib in a patient with advanced braf v600e - mutant bronchial adenocarcinoma . 
 outcomes of chemotherapy for microsatellite instablehigh metastatic colorectal cancers purpose microsatellite instable - high ( msi - h ) colorectal cancers ( crcs ) are known to carry better survival in the local disease stage even without treatment . 
the influence of types of treatment on survival of msi - h metastatic crcs ( mcrcs ) is still unclear and is evaluated in this study . materials and methods patients with msi - h mcrc treated with first - line chemotherapy , with or without bevacizumab , identified in the israeli population - based molecular epidemiology of colorectal cancer ( mecc ) study , were diagnosed between 1998 and 2013 and followed up until may 2017 ; msi status was determined by comparing 10 markers in tumor and normal tissue . 
dates of metastases and death and treatment details were extracted from oncology records . results among 590 patients treated for mcrc , 106 ( 18% ) had msi - h tumors . 
although treatment advances with modern protocols including antivascular endothelial growth factor and antiepidermal growth factor receptor ( egfr ) monoclonal antibodies1 - 3 prolonged median overall survival ( os ) of patients with crc to > 2 years , mcrc , unfortunately , is still an incurable disease in most cases . k - ras proto - oncogene ( kras ) or n - ras proto oncogene ( nras ) mutation ; the presence of a braf v600e mutation has a detrimental effect on overall survival ; the presence of human epidermal growth factor receptor 2 ( her2 ) in mcrc tumors suggests the possibility of benefit from anti - her2 biologic treatment ; and , more recently , microsatellite instable ( msi ) high tumors have been identified as candidates for immunotherapy.4 - 7 molecular heterogeneity in metastatic crcs influences treatment and outcome . 
anti - egfr agents are less effective in the presence of a loss of genomic stability is identified as an early step in colon cancer tumorigenesis and has pathologic , phenotypic , and clinical consequences.8 - 11 stephen b . 
 molecular analysis enables better understanding and separation of colorectal tumors now identified as carrying differences in clinical outcome.12 , 13 under this classification , tumors defined as consensus molecular subtype - 1 ( cms1 ) are characterized as microsatellite instable ( msi - h ) and hypermutated tumors.14 the clinical importance and exclusiveness of msi - h crcs have formerly been established.15 - 18 msi - h tumors have significantly better prognosis at early local stages of disease and rarely metastasize . 
cases identified in the mecc study were approached for risk - factors interview and contributed a venous blood sample after signing a consent form approved by carmel medical center in israel and the university of southern california in the united states . 
dna was extracted from both the peripheral blood and the tissue sample and was routinely studied for msi status , kras and braf mutations , as well as known founder mutations in mmr genes , mostly in ashkenazi jews . 
clinical follow - up included identification of treatment modalities used during the whole follow - up period and identification of changes in disease status , including identification of new metastases . 
details of treatments , as well as date of identification of metastases ( at diagnosis or during disease progression ) , were extracted from the medical files of the patients , which were extracted by experienced senior physicians . for this study , mecc cases that presented with metastatic disease at diagnosis or developed metastases during follow - up were sought . 
in addition to cases from the mecc population - based series , we recruited into the study other mcrc cases that were evaluated in our laboratory on the basis of their clinical presentation or suspicion of lynch syndrome to increase the size of the case series . 
detailed treatment options were grouped into three categories : fu or capecitabine only , combination chemotherapy ( oxaliplatin - based or irinotecan - based in combination with fluoropyrimidine ) , and combination chemotherapy with bevacizumab . 
 metastases with information on treatment details , and have available tissue and germline dna to analyze msi and braf status . laboratory assay dna was extracted using a commercial dna extraction kit . 
five loci of mononucleotide repeats ( bat25 , bat26 , bat40 , - catenin , and tgfbrii ) and five of dinucleotide repeats ( d2s123 , d5s346 , d10s197 , d17s250 , and d18s58 ) were amplified and tested . 
those include the five original bethesda panel markers and five additional monoand dinucleotide markers.33 results for each marker were registered as stable , unstable , equivocal , or suspected as loss of heterozygosity . 
most msi - h cases were also validated by immunohistochemistry tests of the mmr genes . mutations in codon 600 of braf were identified by direct sequencing of exon 15 of the braf gene . 
similarly , kras mutations in exon 12 , 13 , and 61 were identified using a taqman - based single - nucleotide polymorphism genotyping assay on the abi prism 7900ht sequence detection system ( applied biosystems ) in a 96 - well format . until the recorded date of death ( of any cause ) or the last date of available follow - up . 
overall survival was estimated with the use of kaplanmeier method and presented using medians and 2 - year and 5 - year survival probabilities . differences in os were summarized using hazard ratios ( hrs ) , estimated using cox proportional hazard modeling . 
the predictive effect of msi status on treatment effects was assessed using cox proportional hazard models with terms for treatment , msi status , and their interaction results patient population the study population consisted of 106 msi - h mcrc ( met / msi - h ) cases for which first - line chemotherapy - based treatment was identified . 
the metastatic msi - h group had mean age at treatment of 63 15 years , 54% female , 86% with jewish ethnicity , and 48% presenting at stage iv at diagnosis . 
generally , the met / mss group had comparable sex and ethnicity ( jewish / non - jewish ) distribution , as well as frequency of presenting at stage iv at diagnosis . 
this distribution reflects that fact that the patients with met / msi - h were younger at diagnosis ( proportion of patients younger than 50 years : 25% in met / msi - h group and only 10% in met / mss group )  . 
overall survival was calculated from the start date of first treatment of the first identified metastasis ( either at time of crc diagnosis or at time of disease progression ) and treatments for metastatic disease common first - line treatment chemotherapy for the metastatic disease in the msi - h group included fu + leucovorin ( lcv ) or capecitabine only in 21% ( n = 22 ) , combination chemotherapy protocols ( irinotecan based or oxaliplatin based ) in 33% ( n = 35 ) , and combination chemotherapy ( irinotecan based or oxaliplatin based ) and bevacizumab in 46% ( n = 49 ) of cases . 
demographic and disease characteristics of study participants with metastatic colorectal cancer by microsatellite instability status ( n = 590 ) characteristic metastatic msi - h ( n = 106 ) metastatic mss ( n = 484 ) age younger than 50 years at diagnosis female sex jewish ethnicity braf mutation positive stage iv at diagnosis right colon primary tumor location 26 ( 25 ) 57 ( 54 ) 88 * ( 86 ) 19 ( 18 ) 45 ( 48 ) 39 ( 38 ) note . 
 figure 1 presents frequency of the three classes across period years . second - line treatment was given to 55% of the patients treated before 2003 , 63% of those treated in 2003 to 2006 , and 68% of patients treated in 2007 and after . 
no difference in number of treatment lines was noticed between cases with msi - h and cases with mss tumors , probably reflecting the fact that in those years the treating oncologists were unaware of the msi status at time of treatment . in addition , in the msi - h population , the baseline characteristics of patients in the different treatment regimen were comparable ( data not shown )  . 
figure 4 presents os by treatment group , separately for patients with met / mss ( fig 4a ) and patients with met / msi - h ( fig 4b ) , in the homogenous population of braf - wt cases . 
 a sensitivity analysis adjusting for study period revealed similar results . prognostic effect of msi status in the braf - wt population the prognostic role of msi status in the metastatic disease setting was assessed in the population of patients who were indicated to receive an fu - only regimen as having the smallest or even no treatment effect , according to the literature . 
overall survival of patients with microsatellite instable , brafwild type metastatic colorectal cancer by treatment groups in the in the molecular epidemiology of colorectal cancer study , northern israel ( n = 87 )  . 
the mecc study reported here has recruited and collected materials over a time span of 17 years from close to 6 , 000 cases of crc and served as the source for the 590 cases who were diagnosed with , or later developed , metastases and for whom detailed treatment information was available . 
all cases participating in the final analysis were evaluated for their msi status , which was performed in only approximately two thirds of all cases recruited into mecc , with enrichment for suggestive phenotypes . in accordance with other published literature , cases with msi - high mcrc in our study were younger at diagnosis and had a higher proportion of braf mutations , 33 , 34 with a similar proportion of right - sided tumors . 
although msi - h tumors are described as having a much better prognosis than mss tumors for early - stage disease , the proportion of tumors diagnosed with metastases at the time of diagnosis was similar between msi - h cases and mss cases . 
the leading randomized controlled trials evaluating the effect of various chemotherapy regimens in mcrc were not randomized by msi status , and most have not provided subgroup analyses of the results according to their msi status . our study has three major findings . 
we verified that the survival of patients with mcrc indeed improved with the introduction of new chemotherapies but showed that the improvement in survival was limited to the met / mss , braf - wt cases and was not evident in the met / msi - h , braf - wt group of patients . 
we were unable to have a comparison with an observation - only group , and no future studies are likely to include such an arour observational data found no difference in os among metastatic msi - h cases between cases treated with a basic fu + lcv regimen only , compared with cases treated with any ( oxaliplatin or irinotecan ) combination chemotherapy with or without bevacizumab , whereas a significant os improvement was found with advanced chemotherapy in met / mss cases . 
similarly , we did not have any cases that were treated with immune checkpoint inhibitors at the time interval of the current analysis . few reports evaluated the effect of chemotherapy in met / msi - h cases . 
although early studies reported a positive effect of high - dose fu + lcv in patients with met / msi - h in comparison with patients with met / mss , 35 , 36 more recent studies of fu , in combination with irinotecan or oxaliplatin , did not show benefit.16 , 31 , 34 , 37 one study31 showed a trend toward benefit of oxaliplatin - based treatment in cases of msi - h mcrc . 
our data do not have enough power to evaluate specific therapeutic regimens . we chose to exclude from our study all metastatic cases that were not treated at all , because of the inability to assess the causes for no treatment and biases that could stem from it . 
comparison of os results in met / mss and met / msi - h groups supports biologic differences , with a baseline survival advantage for the msi - h group . 
effect of combination treatment on overall survival of patients with metastatic , brafwild type colorectal cancer by microsatellite instability status in the molecular epidemiology of colorectal cancer study , northern israel . 
 published data on the effect of braf mutation on prognosis in patients with met / msi - h were published on a group of crc stages ii to iv , 38 potentially underrepresenting the few cases with stage iv disease . 
extremely poor outcomes in this patient group support the use of the folfoxiri ( oxaliplatin , irinotecan , fluorouracil , leucovorin ) protocol in the unselected group of braf - mutated cases . 
given the much higher prevalence of braf mutations in the msi - h cases , 11 , 26 , 39 it is important to study the outcomes of folfoxiri in this subgroup of patients with met / msi - h . our study is limited by the relatively modest sample size of patients with msi - h mcrc . 
 advantages of our population - based sampling of incident cases with long - term follow - up include generalizability to community practice in a large and well - defined population . 
the representative , observational nature of the data from a large health system , in combination with molecular evaluation of all tumor tissues , offers a framework for understanding clinical practice over nearly two decades in a universally insured group of patients in a single country . msi status is becoming a cornerstone of individualized decision making with regard to a variety of potential oncological interventions , and this trend is likely to continue with the introduction of immunotherapy.40 , 41 routine mutational profiling of mcrc and specifically msi testing and other assays that designate deficient mismatch repair have already been recommended.39 , 42 , 43 the failure of conventional advanced treatments to improve survival in the meaningful subset of met / msi - h cases emphasizes the need to evaluate the role of the newly introduced immunotherapy as a first - line treatment in these cases with msi - h / braf - wt mcrc . in conclusion , therapeutic approaches to mcrc have changed dramatically during the past two decades , with increasing reliance on the molecular features of tumors to inform treatment decisions . 
gruber stock and other ownership interests : teva pharmaceuticals provision of study material or patients : flavio lejbkowicz collection and assembly of data : all authors data analysis and interpretation : katerina shulman , ofra barnett - griness , joel k . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . katerina shulman no relationship to disclose vered friedman no relationship to disclose joel k . 
gruber employment : brogent technologies leadership : brogent technologies stock and other ownership interests : brogent technologies , fulgent therapeutics consulting or advisory role : myriad genetics , fulgent therapeutics research funding : myriad genetics ( inst ) flavio lejbkowicz no relationship to disclose gad rennert no relationship to disclose affiliations katerina shulman , hillel yaffe medical center , hadera ; katerina shulman , ofra barnett - griness , vered friedman , flavio lejbkowicz , and gad rennert , carmel medical center , and technion , haifa , israel ; joel k . 
zhou sw , huang yy , wei y , et al : no survival benefit from adding cetuximab or panitumumab to oxaliplatin - based chemotherapy in the first - line treatment of metastatic colorectal cancer in kras wild type patients : a meta - analysis . 
chan dl , pavlakis n , shapiro j , et al : does the chemotherapy backbone impact on the efficacy of targeted agents in metastatic colorectal cancer ? a systematic review and meta - analysis of the literature . 
siena s , sartore - bianchi a , di nicolantonio f , et al : biomarkers predicting clinical outcome of epidermal growth factor receptor - targeted therapy in metastatic colorectal cancer . 
tol j , dijkstra jr , klomp m , et al : markers for egfr pathway activation as predictor of outcome in metastatic colorectal cancer patients treated with or without cetuximab . 
mller ci , schulmann k , reinacher - schick a , et al : predictive and prognostic value of microsatellite instability in patients with advanced colorectal cancer treated with a fluoropyrimidine and oxaliplatin containing first - line chemotherapy . 
sargent dj , marsoni s , monges g , et al : defective mismatch repair as a predictive marker for lack of efficacy of fluorouracil - based adjuvant therapy in colon cancer . 
weitzel jn , blazer kr , macdonald dj , et al : genetics , genomics , and cancer risk assessment : state of the art and future directions in the era of personalized medicine . 
webber em , kauffman tl , oconnor e , et al : systematic review of the predictive effect of msi status in colorectal cancer patients undergoing 5fu - based chemotherapy . 
des guetz g , schischmanoff o , nicolas p , et al : does microsatellite instability predict the efficacy of adjuvant chemotherapy in colorectal cancer ? a systematic review with meta - analysis . 
ribic cm , sargent dj , moore mj , et al : tumor microsatellite - instability status as a predictor of benefit from fluorouracil - based adjuvant chemotherapy for colon cancer . 
cremolini c , loupakis f , masi g , et al : folfoxiri or folfoxiri plus bevacizumab as first - line treatment of metastatic colorectal cancer : a propensity score - adjusted analysis from two randomized clinical trials . 
van cutsem e , khne c - h , lng i , et al : cetuximab plus irinotecan , fluorouracil , and leucovorin as first - line treatment for metastatic colorectal cancer : updated analysis of overall survival according to tumor kras and braf mutation status . 
peeters m , price tj , cervantes a , et al : randomized phase iii study of panitumumab with fluorouracil , leucovorin , and irinotecan ( folfiri ) compared with folfiri alone as secondline treatment in patients with metastatic colorectal cancer . 
tran b , kopetz s , tie j , et al : impact of braf mutation and microsatellite instability on the pattern of metastatic spread and prognosis in metastatic colorectal cancer . 
goldstein j , tran b , ensor j , et al : multicenter retrospective analysis of metastatic colorectal cancer ( crc ) with high - level microsatellite instability ( msi - h )  . 
liang j - t , huang k - c , lai h - s , et al : high - frequency microsatellite instability predicts better chemosensitivity to high - dose 5 - fluorouracil plus leucovorin chemotherapy for stage iv sporadic colorectal cancer after palliative bowel resection . 
brueckl wm , moesch c , brabletz t , et al : relationship between microsatellite instability , response and survival in palliative patients with colorectal cancer undergoing first - line chemotherapy . 
kim je , hong ys , ryu m - h , et al : association between deficient mismatch repair system and efficacy to irinotecan - containing chemotherapy in metastatic colon cancer . 
overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - deficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
dunne pd , oreilly pg , coleman hg , et al : stratified analysis reveals chemokine - like factor ( cklf ) as a potential prognostic marker in the msi - immune consensus molecular subtype cms1 of colorectal cancer . 
the aim of our study was to investigate whether ctdna can be used for response monitoring in neuroblastoma . methods one hundred forty - nine plasma samples from 56 patients were analyzed by quantitative polymerase chain reaction ( qpcr ) for total cell free dna ( cfdna ; albumin and - actin ) and ctdna ( hypermethylated rassf1a )  . 
ctdna results were compared with mrna - based minimal residual disease ( qpcr ) in bone marrow ( bm ) and blood and clinical patient characteristics . results ctdna was detected at diagnosis in all patients with high - risk and stage m neuroblastoma and in 3 of 7 patients with localized disease . 
the discrepancies indicated either low - level bm inltration ( ctdna negative / mrna positive ) or primary tumor / soft tissue lesions with no bm involvement ( ctdna positive / mrna negative )  . conclusion ctdna can be used for monitoring disease in patients with neuroblastoma . 
it is likely that ctdna can originate from both primary tumor and metastases and may be of special interest for disease monitoring in patients who experience relapse in other organs than bm . jco precis oncol 4 : 291 - 306 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction neuroblastoma is the most common extracranial solid tumor of childhood . in approximately 50% , patients present with high - risk ( hr ) disease and are treated with intensive multimodality treatment protocols that encompass induction therapy , primary tumor surgery , myeloablative chemotherapy with autologous stem - cell rescue , local irradiation , and anti - gd2based immunotherapy1 ( appendix fig a1 )  . 
despite this intensive therapy , in approximately one half of hr patients , the tumor will relapse and result in a fatal outcome.2 assessment of treatment response is based on the international neuroblastoma response criteria . 
meta - iodobenzylguanidine ( mibg ) scintigraphy , imaging ( magnetic resonance imaging / positron emission tomography scans ) , and bone marrow ( bm ) examinations by histology or ( immuno ) cytology are combined to assess the extent of disease.3 because the median age at diagnosis is 18.8 months , 4 response evaluation that is based on imaging and bm testing often must be performed under general anesthesia . 
 van zogchel et al context key objective can hypermethylated rassf1a be used as a circulating tumor dna ( ctdna ) marker for minimal residual disease detection in neuroblastoma ? knowledge generated when testing cell free dna , we were able to detect tumor - derived hypermethylated rassf1a in all patients with stage m disease at diagnosis . 
comparison between ctdna and bloodor bone marrow ( bm ) derived mrna revealed that discrepancies were found when bm inltration was low or when there were primary tumor lesions without bm involvement . relevance ctdna is an interesting source for monitoring disease in patients with neuroblastoma . 
our data indicate that testing of both ctdna and mrna increases the sensitivity of molecular disease monitoring . several studies have shown the feasibility of detecting mutations or tumor - specic translocations in the ctdna by high - depth targeted sequencing or mutation - specic pcr to monitor disease in various types of adult cancer.13 - 19 however , neuroblastoma tumors , like many pediatric tumors , lack recurrent mutations and translocations . 
broader analysis , such as whole - exome sequencing ( wes ) and shallow whole - genome sequencing ( swgs ) , to detect tumor - specic mutations or copy number alterations have been performed successfully using cfdna of patients with neuroblastoma at diagnosis and relapse.20 - 26 nevertheless , these techniques are only informative when the ctdna content is approximately 10%27 and are , therefore , less suited for the detection of mrd , when the tumor burden is low . in contrast to the copy number alterations and tumorspecic mutations , a methylation - specic qpcr assay could potentially be a more general and sensitive ctdna marker . 
hypermethylated rassf1a ( rassf1am ) can be detected in bm with a similar sensitivity as mrna and has shown added value in mrna - negative bm.28 in addition , rassf1am already has been described as a prognostic ctdna marker at diagnosis.29 the aim of this study was to investigate the feasibility of using ctdna ( rassf1am in plasma ) to monitor treatment response in patients with hr / stage m neuroblastoma . 
we retrospectively performed qpcr for rassf1am on cfdna from stored remains of previously collected plasma samples of patients with localized or metastatic neuroblastoma at diagnosis and for patients with hr / stage m neuroblastoma during treatment and at relapse . 
to test the additional value of ctdna monitoring , we compared it with other techniques for disease monitoring : mibg scans , urinary catecholamines , immunocytology , and rt - qpcr rna - based mrd detection in bm and peripheral blood ( pb )  . methods between 2013 and 2016 , from all consecutively diagnosed patients who were included in this study ( n = 56 ) , 149 pb samples for mrna and cfdna and 105 bm samples for mrna were tested . 
pediatric pb control samples were collected from the amsterdam umc ( appendix table a1 )  . sample collection , dna isolation , bisulte conversion , and real - time qpcr methods for sample collection , dna isolation , bisulte conversion , and real - time qpcr for rassf1am28 and mrna markers31 can be found in the appendix and appendix table a2 . data analysis total cfdna was quantied by qpcr for albumin ( alb ) or - actin ( actb )  . 
all statistical analyses were performed with spss version 23 ( ibm corporation , chicago , il ) or graphpad prism 8 ( graphpad software , la jolla , ca ) software . results patients and samples from 48 patients with hr and / or stage m and 8 patients with non - hr neuroblastoma , 149 samples were tested in this study ( fig 1 )  . 
six of the 149 patient samples and 12 of 73 healthy control samples were not included for rassf1am qpcr because too much dna had been lost during bisulte conversion ( fig 1 )  . 
flowchart of samples tested for total cell free dna ( cfdna ) , number of samples excluded after too much dna had been lost after bisulte conversion , and number of samples tested for circulating tumor dna ( ctdna ) by hypermethylated rassf1a ( rassf1am )  . 
the percentage of ctdna of total cfdna , calculated with the equation [ rassf1am / ( rassf1am + unmethylated rassf1a ) 100 ] , was 94% ( range , 82% - 98% ) in the 14 diagnostic samples from patients with stage m disease . 
compared with the individual mrna markers , rassf1am was more often positive , but the combined mrna markers identied the same positive samples as rassf1am ( appendix table a4 )  . in 93 matched bm mrna and ctdna ( pb ) samples , double - negative or double - positive results were found in 77% ( fig 3b )  . 
in contrast to pb , the bm mrna panel identied more positive samples than ctdna , and the individual markers phox2b and th correlated best with rassf1am ( appendix table a4 )  . discrepant findings between ctdna and pb or bm mrna mrd discrepant results between ctdna and mrna were detected in 27 pb and 21 bm samples , respectively , and listed in table 3 and appendix table a4 . 
from 3 of 5 bm mrna - negative / ctdnapositive samples , cryopreserved bm cells were available and tested all negative for rassf1ain some patients ( n850 , n865 , n732 ) , the high levels of ctdna probably correlated with the large primary or local relapse tumors , and these patients had no or very little bm inltration . in the ctdna - negative samples , in general , the cfdna levels were lower , with a median of 6.1 ng / ml for the bm mrna - positive / ctdna - negative and 1.52 ng / ml for the pb mrna - positive / ctdna - negative samples . 
from 15 of negative samples , cryopreserved cells were available and tested for rassf1am ; of the 5 positive samples , 4 were not in the quantitative range , which indicated low levels of bm inltration . in the samples from patients n777 , n798 , n2011 , n2014 , and n802 , no ctdna was detected . 
begin induction indicates until 2 courses of induction therapy ; mid - induction indicates after 3 - 5 courses of induction chemotherapy , unless additional courses were given after 6 courses , and samples before last course were also included at this time point ; end induction indicates at the end of induction therapy ; surveillance indicates during follow - up or at relapse suspicion ; and event indicates relapse or progression . 
of samples diagnosis samples localized and stage ms stage m follow - up samples beginning of induction therapy mid - induction therapy end of induction therapy postconsolidation surveillance progression relapse / refractory disease relapse therapy note . 
positive indicates that rassf1am circulating tumor dna was detected and quantied , and negative indicates that no rassf1am circulating tumor dna was detected . abbreviations : pnq , positive not quantiable ; rafssf1am , hypermethylated rafssf1a . complete remission at that time . 
patient n802 was treated for an isolated cns relapse . in the samples from patients n2012 , n2013 , n2016 , n2024 , n2029 , and n2031 , no ctdna was detected , while low amounts of mrna were detected in the bm . in the case of restricted , minimal bm disease , mrna detection was more sensitive than ctdna ( appendix table a4 )  . 
however , in some patients , a primary tumor was still present ( median , 50 mm ) while ctdna was negative ( table 3 )  . discussion ctdna in plasma is a powerful source for the detection of tumor - derived aberrations in a minimally invasive setting . many ctdna studies in adults for the detection of mrd are based on detection of tumor - specic mutations by targeted sequencing or digital droplet pcr ( ddpcr ) .12 , 16 , 17 because recurrent mutations are not common in neuroblastoma , 32 tumor - specic aberrations need to be characterized before they can be used as an mrd marker . 
however , temporospatial heterogeneity has been reported in neuroblastoma by several studies , 20 , 26 which raises the question of whether we should only use the small part of the tumor that is derived from the biopsy to design tumor - specic mrd markers . 
first , it is a sensitive marker , with a sensitivity of 1 tumor cell in 105 mononuclear cells.28 second , rassf1am qpcr can be used in all patients with stage m neuroblastoma because it has been shown that rassf1a is hypermethylated in all previously tested stage m neuroblastoma tumors.28 third , detection of rassf1am is less costly compared with wes and even swgs ( approximately 40and 10 - fold less expensive , respectively )  . 
hypermethylation of rassf1a has been described in several types of cancer and in physiologic circumstances in placental cells.33 rassf1a is not methylated in normal hematologic cells.28 , 33 , 34 however , in 2 of 61 samples from healthy individuals , we detected very low , nonquantiable levels of rassf1ain diagnosis or relapse other diagnosis or relapse other n = 11 n = 12 n = 23 n = 16 n = 12 n = 124 positive negative positive negative n = 66 n = 12 n = 4 n = 36 n = 4 n = 1 negative ctdna ( rassf1am ) positive negative ctdna ( rassf1am ) positive fig 3 . 
 van zogchel et al addition , in other studies , infrequent detection of rassf1am has been observed in plasma samples from healthy control participants.35 , 36 therefore , when detecting verylow levels of rassf1am in patients with neuroblastoma ( indicated as pnq range ) , results should be analyzed with caution . it has been shown that neuroblastoma tumors shed high amounts of ctdna in the plasma.25 , 26 , 37 in the current study , we found a median cfdna concentration of 73.1 ng / ml at diagnosis for patients with stage m disease . 
however , the levels we found are lower compared with previously published studies.25 , 26 , 37 this inconsistency may be due to differences in isolation of cfdna because we did not use a circulating nucleic acid kit or to differences in quantication methods . 
we found the majority of the cfdna ( 94% at diagnosis ) to be tumor derived in patients with stage m or hr disease , which is also supported by previous research.26 , 37 we tested 143 samples from 54 patients with neuroblastoma and detected ctdna in 57 samples . 
ctdna was detected at diagnosis in all 14 patients with stage m and 4 of 8 patients with localized and stage ms neuroblastoma . misawa et al29 described detection of rassf1am at diagnosis in the serum of 17 of 68 patients ( all stages ) and in 11 of 18 patients with stage m disease . 
there are two likely causes for the increased ctdna detection in our study . first , we used plasma , whereas misawa et al tested serum , which is known to be more contaminated by genomic dna originated from leukocytes during ex vivo clotting.38 second , misawa et al used conventional pcr , which is less sensitive than qpcr . 
our group has previously described that hypermethylation of rassf1a is variable in tumors of patients with stage ms ( median , 65% ) and localized ( median , 30% ) disease28 ; therefore , the level of ctdna can be slightly underestimated in these patients when using rassf1am as marker . we compared the performance of ctdna with pb and bm mrna in 128 and 93 samples , respectively . 
most patients in whom we detected relatively high levels of ctdna compared with pb or bm mrnas still had considerable tumor volumes or negative or low mibg scores ( data not shown ) ; therefore , it is likely that the ctdna in these patients originated from the primary tumor . 
two of these patients were in complete remission but in the other 15 patients , considerable tumor volumes were detected on imaging or urine catecholamines were still positive , which indicate the need to optimize pre - analytic sample handling and prospective study of cfdna kinetics in well - characterized patient cohorts with available paired ( nuclear ) imaging and bm assessment . while the detection of ctdna is very promising for future mrd studies , the current study has some limitations . stored remains were used , which resulted in missing samples and paired clinical data . 
for detection and quantication of low levels of ctdna in the plasma , dna extraction methods can be optimized with an isolation method specic for cfdna , and ddpcr39 may be a more suited technique compared with qpcr.40 moreover , large amounts of cfdna ( up to 96% ) could be destroyed during bisulte conversion41 ; therefore , we are investigating alternative methylation - specic ddpcr methods . 
previous studies showed that rassf1a was the most frequent hypermethylated tumor suppressor gene in neuroblastoma as well as identied other hypermethylated tumor suppressor genes , and inclusion of these genes as mrd markers might increase the sensitivity.42 , 43 in this study , we used rassf1am as a ctdna marker . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . no potential conicts of interest were reported . references pinto nr , applebaum ma , volchenboum sl , et al : advances in risk classication and treatment strategies for neuroblastoma . 
j clin oncol 33 : 3008 - 3017 , 2015 park jr , kreissman sg , london wb , et al : effect of tandem autologous stem cell transplant vs single transplant on event - free survival in patients with high - risk neuroblastoma : a randomized clinical trial . 
jama 322 : 746 - 755 , 2019 park jr , bagatell r , cohn sl , et al : revisions to the international neuroblastoma response criteria : a consensus statement from the national cancer institute clinical trials planning meeting . 
j clin oncol 35 : 2580 - 2587 , 2017 london wb , castleberry rp , matthay kk , et al : evidence for an age cutoff greater than 365 days for neuroblastoma risk group stratication in the childrens oncology group . 
j clin oncol 23 : 6459 - 6465 , 2005 viprey vf , gregory wm , corrias mv , et al : neuroblastoma mrnas predict outcome in children with stage 4 neuroblastoma : a european hr - nbl1 / siopen study . 
j clin oncol 32 : 1074 - 1083 , 2014 cheung nk , ostrovnaya i , kuk d , et al : bone marrow minimal residual disease was an early response marker and a consistent independent predictor of survival after anti - gd2 immunotherapy . 
j clin oncol 33 : 755 - 763 , 2015 kreissman sg , seeger rc , matthay kk , et al : purged versus non - purged peripheral blood stem - cell transplantation for high - risk neuroblastoma ( cog a3973 ) : a randomised phase 3 trial . 
lancet oncol 14 : 999 - 1008 , 2013 burchill sa , beiske k , shimada h , et al : recommendations for the standardization of bone marrow disease assessment and reporting in children with neuroblastoma on behalf of the international neuroblastoma response criteria bone marrow working group . 
cancer 123 : 1095 - 1105 , 2017 stutterheim j , zappeij - kannegieter l , versteeg r , et al : the prognostic value of fast molecular response of marrow disease in patients aged over 1 year with stage 4 neuroblastoma . 
gormally e , caboux e , vineis p , et al : circulating free dna in plasma or serum as biomarker of carcinogenesis : practical aspects and biological signicance . mutat res 635 : 105 - 117 , 2007 2017 12 . 
mcbride dj , orpana ak , sotiriou c , et al : use of cancer - specic genomic rearrangements to quantify disease burden in plasma from patients with solid tumors . genes chromosomes cancer 49 : 1062 - 1069 , 2010 16 . 
tsao sc , weiss j , hudson c , et al : monitoring response to therapy in melanoma by quantifying circulating tumour dna with droplet digital pcr for braf and 18 . 
van roy n , van der linden m , menten b , et al : shallow whole genome sequencing on circulating cell - free dna allows reliable noninvasive copy - number proling in neuroblastoma patients . 
chicard m , colmet - daage l , clement n , et al : whole - exome sequencing of cell - free dna reveals temporo - spatial heterogeneity and identies treatmentresistant clones in neuroblastoma . 
yanik ga , parisi mt , shulkin bl , et al : semiquantitative mibg scoring as a prognostic indicator in patients with stage 4 neuroblastoma : a report from the 31 . 
stutterheim j , gerritsen a , zappeij - kannegieter l , et al : detecting minimal residual disease in neuroblastoma : the superiority of a panel of real - time quantitative 32 . 
chan kc , ding c , gerovassili a , et al : hypermethylated rassf1a in maternal plasma : a universal fetal dna marker that improves the reliability of noninvasive prenatal diagnosis . 
scheffer pg , de haas m , van der schoot ce : the controversy about controls for fetal blood group genotyping by cell - free fetal dna in maternal plasma . 
white he , dent cl , hall vj , et al : evaluation of a novel assay for detection of the fetal marker rassf1a : facilitating improved diagnostic reliability of noninvasive opin hematol 18 : 467 - 473 , 2011 prenatal diagnosis . 
wong fc , sun k , jiang p , et al : cell - free dna in maternal plasma and serum : a comparison of quantity , quality and tissue origin using genomic and epigenomic approaches . 
 circulating tumor dna in neuroblastoma appendix sample collection clinical samples were collected in edta tubes and processed within 24 hours , and 2 ml peripheral blood ( pb ) or 0.5 ml bone marrow ( bm ) was transferred to paxgene blood rna tubes ( qiagen , venlo , the netherlands ) and stored at 20c . 
mononuclear cells were isolated from the remaining bm sample by ficoll density centrifugation and cryopreserved in 10% dimethyl sulfoxide . dna isolation and bisulte conversion dependent on the available plasma volume , dna was extracted by using the qiaamp dna mini blood kit ( qiagen ) for 200 l plasma , or the magna pure 96 isolation robot ( roche , basel , switzerland ) for 500 - 1 , 000 l plasma and eluted in h2o . 
converted dna samples were used directly or stored at 20c . real - time quantitative polymerase chain reaction real - time quantitative polymerase chain reaction ( qpcr ) was performed as previously described ( van wezel em , et al : j mol diagn 17 : 43 - 52 , 2015 )  . 
primer and probe sequences have been described previously28 ( scheffer pg , et al : bjog 118 : 1340 - 1348 , 2011 ) and are listed in appendix table a2 . 
qpcr for alb , actb , and unmethylated rassf1a was performed in duplicate ; hypermethylated rassf1a was tested in triplicate . pb and bm mrna reverse transcriptase qpcr total rna from whole blood and bm samples was extracted using the paxgene blood rna kit ( qiagen ) according to the manufacturers instructions . 
cdna was synthesized and reverse transcriptase ( rt ) qpcr , with a maximum of 50 cycles was performed for - glucuronidase ( gusb ) , paired ctdna in neuroblastoma like homeobox 2b ( phox2b ) , tyrosine hydroxylase ( th ) , dopa decarboxylase ( ddc ) , growth - associated protein 43 ( gap43 ) , cholinergic receptor nicotinic - 3 ( chrna3 ) , and dopamine - hydroxylase ( dbh ) , as has been described previously.31 expression was normalized to gusb expression using the following equation : [ normalized threshold cycle ( ct ) = ( ctgusb ctmarker ) ]  . 
samples were scored for positivity according to previously published thresholds9 , 31 ( stutterheim j , et al : j clin oncol 26 : 5443 - 5449 , 2008 )  . 
oncogenic met activation results from a hijacking of various aspects of the canonical met pathway otherwise normally active in development and wound healing.2 the canonical pathway consists of hgf ligand - induced dimerization , tyrosine kinase domain activation , and the subsequent activation of a downstream signaling cascade resulting in the met - driven oncophenotype . 
shouldnt a targeted therapy be directed toward a susceptible cancer cell that harbors the target ? but what was the biomarker to reliably signify that a tumor was truly met dependent and would derive substantial benet from anti - met therapy ? the leading biomarker candidate was , and still is , met amplication , which has severalfold higher protein expression as observed by mass spectrometry compared with nonamplied tumors.8 although rare , amounting to only approximately 5% of gea ( the highest incidence of any cancer ) , met amplication has been the most consistent and reliable biomarker both of overall poor prognosis and predictive benet from agents targeting the receptor.3 , 4 , 12 - 14 however , other potential predictive biomarkers have also been proposed , including met tyrosine kinase phosphorylation ( difcult to measure ) , 15 met activating mutation or fusion ( rare ) , met exon 14 skipping or deletion ( mostly lung cancer ) , 16 high hgf tumor and / or serum levels ( not consistently demonstrated ) , and met overexpression ( in the absence of met amplication ) .17 focus on the latter overexpression ensued , likely because this was generally than the more stringent genomic more prevalent denition of amplication , making this more expedient and lucrative to study . 
what exactly is the denition of met overexpression ? met expression by immunohistochemistry ( ihc ) has many descriptions , including cellular distribution ( membranous , cytoplasmic , and / or nuclear staining ) , extensity ( the percentage of tumor cells actually staining ) , and intensity ( the semiquantied staining strength from 0 to 3 + )  . 
 catenacci death ligand 1 ( pd - l1 ) , various alterations in the scoring criteria can change a tumor from met negative to met positive , or vice versa , and dramatically alter positivity incidence with slight scoring modications . 
benet in the met - high population ( 64% incidence in that study ) hinged on a small retrospective subgroup of 47 and 21 patients receiving rilotumumab and placebo , respectively.18 unfortunately , the competition to be rst to market and , therefore , the rush to initiate phase iii studies with rilotumumab in rilomet - 1 ( international phase iii multicenter , randomized , double - blind , placebocontrolled trial of rilotumumab plus epirubicin , cisplatin , and capecitabine as first - line therapy in patients with advanced met - positive gastric or gastroesophageal junction adenocarcinoma ) and onartuzumab in metgastric ( fluorouracil , leucovorin , and oxaliplatin with or without onartuzumab in her2 - negative , met - positive gastroesophageal adenocarcinoma ) , without more attention to these issues , resulted in a fundamental lack of biomarker understanding . 
because the questions were unasked , the answers were unknown . importantly , thus , the market - based engines steamed on ahead with the following two bits of data : one patient who responded to an lbab monotherapy5 and one retrospective small subgroup analysis of a phase ii randomized study.18 unfortunately , ultimately both lbab phase iii studies were negative.10 , 11 regrettably , neither study successfully enriched for a population who would benet from met lbabs . 
notably , for the rilotumumab studies , the initial antibody prototype assay and , the actual scoring system used in the phase ii study were changed for the prospective phase iii study to ofcially codevelop a companion diagnostic assay . the assay in rilomet - 1 likely inadequately selected any optimal patient population for treatment , with most patients ( 81% ) screened considered positive for met expression using the lax criteria of greater than or equal to 1 + intensity at 25% or greater extensity staining ( hardly selecting ) and most patients having low - level expression.11 prospectively testing formalin - xed parafn - embedded ( ffpe ) freshly cut samples from recently diagnosed patients in rilomet - 1 compared with a retrospective batched archival ffpe analysis in the phase ii study may also have contributed to the incidence discrepancy between the studies , because ihc sensitivity is decreased with older ffpe samples and , when still positive in light of this , would represent those indeed , true benet randomized phase ii samples likely having the highest levels of expression to begin with . 
conversely , the metgastric study had only the slightly more stringent criteria of positivity for eligibility of greater than or equal to 1 + intensity at 50% or greater extensity staining ( ie , more cells needed to be expressing at least low - level amounts of protein )  . 
notably , in this latter underpowered subgroup analysis , the hr for overall survival was 0.64 in favor of onartuzumab ( p = .062 ) , and the median survival increased from 9.7 months to 11 months with onartuzumab.10 could this have been statistically signicant with the originally intended number of patients ? because the question was unasked ( study terminated early ) , the answer is unknown . 
in the end , the optimal met biomarker assay , scoring , and positivity criteria of expression for lbabs , if any , remain undened . nevertheless , even if we could rewind and do things differently with this hindsight ( could we perform prospective , adequately accrued , randomized phase ii and / or iii studies with only the highest ihc criteria amounting to approximately 20% to 30% of all patients with gea ? ) , the marginal absolute benets that could be realistically achieved with lbab in an optimal expressing subgroup , as exemplied by the metgastric subgroup analysis hr of 0.64 , lend pause to question whether this would really provide signicant clinical improvement . 
yet , frustratingly , met amplication , now serving as a driver oncogene in this scenario , is the biomarker subset to likely derive the most benet from targeted met receptor inhibitors . 
in comparison , pd - l1 checkpoint blockade monotherapies , despite the hysteria , ultimately demonstrated an approximate 10% response rate in the third - line or higher setting in gea all - comers , with a median progression - free survival time of 2 months , and only a 13.3% response rate ( 19 of 143 patients ) in the subset of pd - l1positive , microsatellite stable ( mss ) selected patients , with a median dor of less than 8 months ( only ve patients , or ve [ 28% ] of 19 responders or ve [ 3% ] of 143 pd - l1positive / mss patients , had dor greater than 12 months ) .25 yet on the basis of these results , pembrolizumab was recently successfully pursued for accelerated approval for the entire pd - l1positive / mss subset by the us food and drug administration.25 , 26 similar clinical outcomes are consistently reported in patients with met - amplied gea ( with comparable incidence of responses lasting greater than 12 months )  . 
in the face of being an uncommon genomic event , this discussion still matters for patients with gea with tumors harboring met amplication . this amg337 example , along with other met inhibitors , has well - elucidated reasons for perceived failure . 
these include underappreciating the general poor prognosis of met - amplied tumors in single - arm , late - line studies , intrapatient heterogeneity with regions harboring and not harboring met amplication , and the presence of concurrent genomic aberrations in some met - amplied cells . all of these factors could lead to relatively quick progression on monotherapy either outright or shortly after an initial response in most , but importantly not all , responding patients . 
however , the ideal randomized and combination therapy studies have been elusive to date because of the infeasibility of classic clinical study designs and the requirement of extraordinarily high numbers of patients screened to identify the met - amplied subset , with the consequent abandonment of additional investigation by pharma because of this apparently high - risk and low - yield scenario . 
with met , supportive evidence abounds that there are patients who derive benet from met inhibitors , particularly those with met - amplied tumors , yet to date , no met - specic inhibitor is approved by the us food and drug administration in any met - specic indication for any tumor . 
lack of progress can be attributed to a number of issues including inadequate validation of biomarker cut - offs , along with the inherent hurdles to developing drugs in lowincidence biomarker populations , coupled with complex intrapatient heterogeneous biology rendering monotherapy in late - line therapy less likely to impress , 34 and certainly so for accelerated approval paths . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . daniel catenacci honoraria : genentech , eli lilly , amgen , oncoplex diagnostics , foundation medicine , taiho pharmaceutical , genmab , nantomics , guardant health , merck , bristol - myers squibb , gritstone oncology , five prime therapeutics , astellas pharma consulting or advisory role : genentech , amgen , merck , eli lilly , taiho pharmaceutical , bristol - myers squibb , astellas pharma speakers ' bureau : guardant health , foundation medicine , genentech , eli lilly , merck references giordano s , di renzo mf , ferracini r , et al : p145 , a protein with associated tyrosine kinase activity in a human gastric carcinoma cell line . 
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clin cancer res 20 : 1666 - 1675 , 2014 catenacci dv , liao wl , thyparambil s , et al : absolute quantitation of met using mass spectrometry for clinical application : assay precision , stability , and correlation with met gene amplication in ffpe tumor tissue . 
plos one 9 : e100586 , 2014 shah ma , wainberg za , catenacci dv , et al : phase ii study evaluating 2 dosing schedules of oral foretinib ( gsk1363089 ) , cmet / vegfr2 inhibitor , in patients with metastatic gastric cancer . 
shah ma , bang yj , lordick f , et al : effect of uorouracil , leucovorin , and oxaliplatin with or without onartuzumab in her2 - negative , met - positive gastroesophageal adenocarcinoma : the metgastric randomized clinical trial . 
catenacci dvt , tebbutt nc , davidenko i , et al : rilotumumab plus epirubicin , cisplatin , and capecitabine as rst - line therapy in advanced met - positive gastric or gastro - oesophageal junction cancer ( rilomet - 1 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
smolen ga , sordella r , muir b , et al : amplication of met may identify a subset of cancers with extreme sensitivity to the selective tyrosine kinase inhibitor pha665752 . 
j clin oncol 29 : 4803 - 4810 , 2011 jardim dlf , tang c , gagliato ddm , et al : analysis of 1 , 115 patients tested for met amplication and therapy response in the md anderson phase i clinic . 
awad mm , oxnard gr , jackman dm , et al : met exon 14 mutations in non - small - cell lung cancer are associated with advanced age and stage - dependent met genomic amplication and c - met overexpression . 
neoplasia 7 : 75 - 84 , 2005 iveson t , donehower rc , davidenko i , et al : rilotumumab in combination with epirubicin , cisplatin , and capecitabine as rst - line treatment for gastric or oesophagogastric junction adenocarcinoma : an open - label , dose de - escalation phase 1b study and a double - blind , randomised phase 2 study . 
shah ma , cho jy , tan ib , et al : a randomized phase ii study of folfox with or without the met inhibitor onartuzumab in advanced adenocarcinoma of the stomach and gastroesophageal junction . 
wilke h , muro k , van cutsem e , et al : ramucirumab plus paclitaxel versus placebo plus paclitaxel in patients with previously treated advanced gastric or gastrooesophageal junction adenocarcinoma ( rainbow ) : a double - blind , randomised phase 3 trial . 
kwak el , lorusso p , hamid o , et al : clinical activity of amg 337 , an oral met kinase inhibitor , in adult patients ( pts ) with met - amplied gastroesophageal junction ( gej ) , gastric ( g ) , or esophageal ( e ) cancer . 
hong ds , lorusso pm , hamid o , et al : phase 1 study of amg 337 , a highly selective small - molecule met inhibitor , in patients with advanced solid tumors . 
van cutsem e , karaszewska b , kang yk , et al : a multicenter phase 2 study of amg 337 in patients with met - amplied gastric / gastroesophageal junction / esophageal adenocarcinoma and other solid tumors . 
fuchs cs , doi t , jang rw , et al : safety and efcacy of pembrolizumab monotherapy in patients with previously treated advanced gastric and gastroesophageal junction cancer : phase 2 clinical keynote - 059 trial . 
catenacci dvt , park h , uronis he , et al : margetuximab ( m ) plus pembrolizumab ( p ) in erbb2 - amplied pd - l1 + gastroesophageal adenocarcinoma ( gea ) post trastuzumab ( t )  . 
lancet oncol 16 : 1276 - 1278 , 2015 joshi ss , maron sb , lomnicki s , et al : personalized antibodies for gastroesophageal adenocarcinoma ( pangea ) : a phase ii precision medicine trial ( nct02213289 )  . 
j natl cancer inst 97 : 249 - 250 , 2005 jardim dl , groves es , breitfeld pp , et al : factors associated with failure of oncology drugs in late - stage clinical development : a systematic review . 
hamid o , gajewski tf , frankel ae , et al : epacadostat plus pembrolizumab in patients with advanced melanoma : phase 1 and 2 efcacy and safety results from echo - 202 / keynote - 037 . 
long gv , dummer r , hamid o , et al : epacadostat ( e ) plus pembrolizumab ( p ) versus pembrolizumab alone in patients ( pts ) with unresectable or metastatic melanoma : results of the phase 3 echo - 301 / keynote - 252 study . 
gene amplication , or increased gene dosage , leads to increased messenger rna expression , which leads to exponential increase in the amount of met protein receptor ( green ) expression at the membrane . 
 c sustained exceptional response to poly ( adp - ribose ) polymerase inhibition plus temozolomide in metastatic melanoma with dna repair deficiency introduction the median overall survival ( os ) of patients with melanoma with brain metastases was 4.7 months in a retrospective series from 1986 to 2004.1 in historical series of such patients , median os was 7.5 months for those diagnosed between 2000 and 2008 , 8.5 months for those diagnosed between 2009 and 2010 , and 22.5 months for those diagnosed from 2011 on.1 - 5 the availability of newer systemic therapies , such as braf inhibitors and immunotherapy , in patients with melanoma and brain metastases are directly attributable to the increased length in survival.2 - 5 better understanding of the biology of advanced melanoma could help researchers to identify targetable aberrations in the relapsed refractory setting , and integrative clinical sequencing may allow us to exploit additional therapeutic modalities . 
the tumor was ulcerated with an involved marg he had a wide local excision and left - side axillary dissection that showed residual melanoma to a depth of 12 mm , clear margins , and zero of 14 lymph nodes positive for melanoma . 
after work - up , he was found to be eligible and was treated with high - dose interleukin - 2 and received a first cycle ( 11 of a planned 14 doses ) and a second cycle ( eight of a planned 14 doses )  . 
the patient was then treated in a double - blind randomized controlled clinical trial with temozolomide 200 mg / m2 plus placebo or combined with either 20 or 40 mg abt - 888 ( veliparib ) , a parp inhibitor . 
the patient remained on treatment , continuing with temozolomide 150 mg / m2 once per day for days 1 to 5 of a 28 - day cycle and veliparib 40 mg twice per day on days 1 to 7 . 
his metastases did not progress , and he continues to live without treatment , with follow - up ct and mri scans revealing no progression ( fig 1 )  . given the exceptional response , the patient was followed through the indiana university health precision genomics biobank , and his archived brain tissue underwent whole - exome sequencing ( nantomics , culver city , ca )  . 
information at the gene level ( oncogene or tumor suppressor , driver of tumorigenesis , etc ) and specific to the mutation ( activating or disruptive , conservation score , location within recurrently mutated hotspot , etc ) is used . 
gene type is obtained using data from the catalog of somatic mutations in cancer cancer gene census.8 driver status is obtained from a pan - cancer publication across 15 and more the cancer genome atlas cancer types , and clusters of mutations are discovered using oncodriveclust.9 best - fit parameters for tumor ploidy are found by gradient descent . 
in the joint log likelihood calculation , a set of common allelic states are used to determine the expected relative coverage and majority allele fraction values for each state , given tumor ploidy . on the basis of this analysis , somatic tumor changes revealed a single copy number loss of brca2 , atm , chek1 , atr , fancm , and rad21 , which indicates dna repair deficiencies ( fig 2 )  . 
pathway analysis was performed using ingenuity pathway analysis.15 bard1 , brca1 - associated ring domain 1 ; fanc , fanconi anemia complementation group ; nhej1 , nonhomologous end - joining factor 1 ; plk1 , polo - like kinase 1 ; rb , retinoblastoma ; rx , treatment ; xrcc1 , x - ray repair cross - complementing group 1 . 
in addition , a germline recq1 i46r dna mutation was observed and is predicted to be possibly damaging through polyphen - 2.11 recql ( also known as recq1 ) helicases are a family of dna unwinding enzymes involved in the maintenance of chromosome stability and play a role in cellular response to oxidative dna damage.12 , 13 recent data have suggested that recql deficiency results in decreased homologous recombination and hyperactivation of parp.13 viziteu et al14 demonstrated that recql deficiency in myeloma cell lines displays sensitivity to parp inhibitors . 
there was an increase in the presence of other pathogenic alterations , which included braf g469r , cdh1 p429s , apc q1090 * , nf1 q803 * , and tp53 r248w . 
moving inward from the outside : intrachromosomal structural variants ( lines ) , overall copy number ( grey ) , majority and minority allele fractions ( light red and blue , respectively ) , single nucleotide variants and small indels ( colored dots ) , and interchromosomal structural variants . 
 ( b ) a total of 8 , 040 somatic variants were identified in this patient sample and categorized according to each variants annotation and supporting data as described in the case report . 
additional findings are presented in the circular genome and tumor mutation burden plots shown in figure 3 , and mutations are included in the data supplement . discussion our patient was treated in a randomized , controlled , double - blind , phase ii study of temozolomide combined with placebo or veliparib ( clinicaltrials.gov identifier : nct00804908 )  . 
 the randomization was 1 : 1 : 1 , and results were published by middleton et al.16 this report is the first to our knowledge of a patient treated successfully with chemotherapy and a parp inhibitor who had observed somatic losses in homologous recombination pathways with a recql germline mutation and who had an loh of 42.4%. 
 recently , the ariel2 trial was completed with the parp inhibitor rucaparib ; participants had relapsed , platinum - sensitive , high - grade ovarian carcinoma with brca mutations and an loh with a cutoff of 14%.18 the investigators observed a higher progression - free survival benefit in patients with high loh treated with parp inhibition . 
the investigators also suggested that patients with ovarian cancer who are brca wild type but with a high loh may derive benefit from parp inhibitor therapy as a future research hypothesis . in addition to the potential implications from high loh , evaluation of hrd or dna repair deficiency in melanoma registered with cbioportal reveals an overall incidence of dna repair mutations in 41% of samples , including 5% brca1 , 10% brca2 , 10% atm , 2.9% recql , and less than 10% for other fig 4 . 
although we cannot pinpoint the exact aberrations associated with sensitivity to therapy , we believe that the single - loss combinations in dna repair pathways and loh play the most important role to parp sensitivity . reported here is an extraordinary case of response to parp inhibition that may have been kismet on the basis of the plethora of aberrations in dna repair , germline recql , and loh of 42.4%. 
hypothesis - generating points from this report include the evaluation of the role of monoallelic and biallelic dna repair dysfunction , loh , or novel biomarkers or algorithms associated with hrd because this patient would not have been expected to derive such a continued benefit . 
logan consulting or advisory role : prometheus laboratories research funding : abbott laboratories ( inst ) , abraxis bioscience ( inst ) , acceleron pharma ( inst ) , amgen ( inst ) , argos therapeutics ( inst ) , astrazeneca ( inst ) , aveo pharmaceuticals ( inst ) , biovex ( inst ) , bristol - myers squibb ( inst ) , eisai ( inst ) , eli lilly ( inst ) , glaxosmithkline ( inst ) , roche ( inst ) , immatics biotechnologies ( inst ) , merck ( inst ) , novartis ( inst ) , pfizer ( inst ) , synta pharmaceuticals ( inst ) , threshold pharmaceuticals ( inst ) , millennium pharmaceuticals ( inst ) , tracon pharmaceuticals ( inst ) , cerulean pharma ( inst ) , emd serono ( inst ) , prometheus laboratories ( inst ) , macrogenics ( inst ) , peloton therapeutics ( inst ) , iovance biotherapeutics ( inst ) , medimmune ( inst ) , dynavax technologies ( inst ) affiliations all authors : indiana university school of medicine and iu simon cancer center , indianapolis , in . support supported by indiana university health with assistance from the indiana clinical and translational sciences institute and funded in part by national center for advancing translational sciences , clinical and translational sciences award ul1tr001108 . 
sloot s , chen ya , zhao x , et al : improved survival of patients with melanoma brain metastases in the era of targeted braf and immune checkpoint therapies . 
long gv , trefzer u , davies ma , et al : dabrafenib in patients with val600glu or val600lys braf - mutant melanoma metastatic to the brain ( break - mb ) : a multicentre , open - label , phase 2 trial . 
goldberg sb , gettinger sn , mahajan a , et al : pembrolizumab for patients with melanoma or non - small - cell lung cancer and untreated brain metastases : early analysis of a non - randomised , open - label , phase 2 trial . 
telli ml , hellyer j , audeh w , et al : homologous recombination deficiency ( hrd ) status predicts response to standard neoadjuvant chemotherapy in patients with triple - negative or brca1 / 2 mutation - associated breast cancer . 
hu h , huff cd , moore b , et al : vaast 2.0 : improved variant classification and disease - gene identification using a conservation - controlled amino acid substitution matrix . 
middleton mr , friedlander p , hamid o , et al : randomized phase ii study evaluating veliparib ( abt - 888 ) with temozolomide in patients with metastatic melanoma . 
middleton mr , grob jj , aaronson n , et al : randomized phase iii study of temozolomide versus dacarbazine in the treatment of patients with advanced metastatic malignant melanoma . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
 molecular and clinical characterization of a claudin - low subtype of gastric cancer purpose claudin - low molecular subtypes have been identified in breast and bladder cancers and are characterized by low expression of claudins , enrichment for epithelial - to - mesenchymal transition ( emt ) , and tumor - initiating cell ( tic ) features . 
we evaluated whether the claudin - low subtype also exists in gastric cancer . materials and methods four hundred fifteen tumors from the cancer genome atlas ( tcga ) gastric cancer mrna data set were clustered on the claudin , emt , and tic gene sets to identify claudin - low tumors . 
compared with gs subtype , claudin - low subtype had significant activation in rho family of gtpases signaling , which appears to play a key role in its emt and tic properties . 
in the acrg data set , 28 of 300 samples were classified as claudinlow tumors by the 24 - gene predictor and were phenotypically similar to the initially derived claudinlow tumors . 
2017 by american society of clinical oncology introduction claudin - low tumors have been identified as a molecular subtype originally in breast cancer and more recently in bladder cancer on the basis of gene expression profiling.1 , 2 these distinct tumors are characterized by the low expression of tight - junction claudins , enrichment for epithelial - to - mesenchymal transition ( emt ) markers , and tumor - initiating cell ( tic ) features.1 , 2 clinically , claudin - low tumors , which lack luminal differentiation marker expression , are associated with poor prognosis compared with luminal tumors.1 , 3 similar to breast , bladder , and other types of cancer , gastric cancer is a heterogeneous disease and arises from multiple genetic and epigenetic aberrations . 
to better understand the biology that drives gastric cancer , molecular evaluation of gastric cancer has been performed and has led to the identification of key dysregulated pathways and the development of molecular classifications.4 gene expressionbased classifiers were reported by the asian cancer research group ( acrg ) 5 and by lei et al.6 the acrg divided gastric cancer tumors into four subtypes ( microsatellite unstable [ msi ] , emt , and tumor protein 53 active and inactive ) , and lei et al classified gastric cancer tumors into three subtypes ( proliferative , metabolic , and mesenchymal )  . on the basis of an integrative analysis of molecular profiling data , the cancer genome atlas ( tcga ) proposed the following four molecular subtypes of gastric cancer tumors : epstein - barr virus ( ebv ) positive , msi , chromosomally unstable ( cin ) , and genomically stable ( gs ) .7 this classification system first categorizes tumors by ascopubs.org / journal / po jco precision oncology tomohiro f . 
vincent author affiliations appear at the end of this article . supported by the university cancer research fund of the lineberger comprehensive cancer center at the university of north carolina at chapel hill and the university of north carolina at chapel hill oncology clinical translational research training program ( 5k12ca120780 )  . presented at the asco 2017 gastrointestinal cancers symposium , san francisco , ca , january 1921 , 2017 . corresponding author : benjamin g . 
however , gs subtype was found to have some notable features , including enrichment of lauren diffuse histologic type and alterations in the genes associated with cell adhesion and motility , such as cdh1 and rhoa mutations and cldn18 - arhgap fusions . 
missing values were imputed using the k - nearest neighbor imputation method , and gene expression values were median centered across each gene . results gene expression signatures tight - junction claudin , emt , and tic gene signatures were used in the classification of a claudin - low subtype . 
the set of claudins used was identified by herschkowitz et al.9 the bidirectional pan - cancer emt signature was derived by tan et al.10 the gastric cancerspecific tic signature was derived from the publicly available gene expression omnibus gene expression data set ( gse53276 )  . 
proliferation and immune gene signatures were derived by hippo et al11 and iglesia et al , 12 respectively . identification of a claudin - low subtype data were clustered on the claudin , emt , and tic gene sets using average linkage clustering with a centered correlation similarity metric on the cluster 3.0 platform ( stanford university , stanford , ca )  . 
sigclust2 r software ( statistical significance of clustering 2 ) was run on the node to perform a gaussian distribution analysis , which expands to the entire gene set for each increasing node . 
the data supplement contains additional details on methods . identification of a claudin - low subtype in gastric cancer from adjacent clusters of we performed unsupervised hierarchical clustering on 415 gastric cancer samples from tcga data set using gene signatures representative of biologic characteristics known to define the claudin - low subtype of breast and bladder cancers.1 , 2 this unsupervised hierarchical clustering with these gene signatures revealed a distinct cluster that had characteristics of claudin - low tumors ( fig 1a , highlighted in red )  . 
to ensure that the set of tumors within the presumed claudin - low cluster were homogeneous and distinct tumors , we performed a gaussian distribution analysis ( data supplement )  . 
this method identified a conserved node of 46 tumors ( 11.1% ) that had consensus enrichment for claudin - low features , and these tumors , therefore , were defined as claudin - low subtype . 
classification of the nonclaudin - low tumors ( n = 369 ) was as follows : ebv , 31 tumors ; msi , 79 tumors ; cin , 218 tumors ; and gs , 41 tumors . 
because the claudin - low tumors were identified originally in breast cancer , we applied the previously defined breast cancerspecific claudin - low classifier to tcga gastric cancer samples and found a significant enrichment ( p , .001 , fishers exact test ) of the breast cancerdefined claudin - low tumors within the gastric claudin - low cluster ( data supplement )  . 
this finding further supports the notion that claudin - low tumors exhibit features of previously defined claudin - low tumors . gene expression signature analysis relative to tic and stem - cell features , breast cancer claudin - low tumors express low levels of proliferation genes and are likely slowercycling tumors.1 , 3 we examined proliferation gene expression of gastric cancer by subtype using a previously reported gastric cancerspecific proliferation signature.11 expression of the proliferation - associated genes in the claudinlow subtype was lowest among all the subtypes ( figs 2a and 2b )  . 
despite the apparent similarity to gs subtype , the claudin - low subtype expressed significantly lower levels of proliferation genes than gs subtype ( p , .001 , bonferronicorrected pairwise t test )  . 
 another notable feature of the claudin - low subtype of breast and bladder cancers is high expression of immune cell genes , including t and b cells.1 , 2 to characterize the immune response in gastric claudin - low tumors , we evaluated gene signatures associated with immune cells by molecular subtype using previously defined signatures that correspond to tumor - infiltrating immune cells.12 heat maps of immune signature expression across the 415 samples in order by subtype showed generally high expression in ebv , claudin - low , and gs ( fig 3a )  . 
on the basis of the z scores of the gene signature , expression of all immune signatures other than the b - cell signature was highest in the ebv subtype ( data supplement )  . to assess the level of active immunosuppression , we examined the expression of a previously defined panel of immune checkpoint molecules ( immunosuppression signature ) 2 and found that it was also highest in the ebv subtype ( fig 3b ; data supplement )  . 
this observation is in line with the previous report by strong et al.13 wherein ebvpositive gastric carcinoma samples expressed high levels of the cytotoxic t - cell and natural killer cell inhibitor indoleamine - 2 , 3 - dioxygenase 1 , which leads to the induction of immune tolerance to tumors despite the elevated immune cell infiltration . 
similar to the previous analysis of bladder cancer , a clear correlation existed between the immune signatures and the immunosuppression signature across all gastric cancer subtypes2 ( data supplement )  . the prognostic impact of tumor - immune infiltrates , especially tumor - infiltrating lymphocytes ( tils ) , has been reported in multiple tumor types.14 , 15 for instance , the presence of cd8 + tils was associated with favorable survival outcomes.16 - 18 some studies evaluated the prognostic relevance of tils in gastric cancer , but the results were not consistent across them.19 - 21 we performed cox proportional hazards regression modeling for each immune gene signature , including immunosuppression signature , across all tumors and within each subtype . 
none of the signatures were prognostic in tcga gastric cancer samples ( data not shown )  . we explored potential mechanisms of immune response by examining predicted neoantigen burden and levels of cytokines and chemokines among subtypes . 
 ( a ) heat map of supervised clustering of gastric cancer subtypes across previously identified proliferationassociated genes ( n = 415 )  . ( b ) box plot of proliferation gene signature z scores across gastric cancer subtypes ( n = 415 )  . significance was determined by one - way analysis of variance ( anova )  . 
 ( b ) box plot of immune suppression gene signature z scores across gastric cancer subtypes ( n = 415 )  . significance was determined by one - way analysis of variance ( anova )  . 
 ( c ) and ( d ) box plots show the number of predicted neoantigens with a half - maximal inhibitory concentration , 150 nm by tumor molecular subtype . significance was determined by kruskalwallis exact test ( n = 357 )  . ( e ) box plot of cytokine and chemokine signature z scores across gastric cancer subtypes ( n = 415 )  . significance was determined by one - way anova . 
cin , chromosomally unstable ; ebv , epstein - barr virus ; gs , genomically stable ; igg , immunoglobulin g ; mac th1 , macrophageassociated t helper 1 ; msi , microsatellite unstable . difference in immune infiltration among subtypes because the predicted neoantigen burdens of ebv , claudin - low , and gs subtypes were lower than that of cin subtype and relatively similar to one another ( fig 3d )  . we next examined the relative expression of a previously defined panel of cytokines and chemokines by subtype2 and observed a strong correlation between this expression signature and multiple immune signatures , including immunosuppression signature ( data supplement )  . 
overall , claudin - low tumors appeared to have a high level of immune infiltration but lacked active immunosuppression within the tumor microenvironment . pathway analysis given that claudin - low tumors were primarily found in gs subtype , we performed ingenuity pathway analysis ( ipa ) and gene set enrichment analysis to understand the gene expression patterns that differentiate claudin - low tumors from nonclaudin - low gs tumors . 
ipa revealed that claudin - low subtype had significant activation in rho family of gtpases signaling and significant inactivation in rho guanine nucleotide dissociation inhibitor ( gdi ) signaling compared with gs subtype ( fig 4 )  . 
rhoa ( a member of the rho family of gtpases ) signaling has been reported to promote cancer stem - celllike phenotype in diffuse - type gastric cancer.22 in addition , claudinlow subtype had higher levels of actin cytoskeleton and integrin signaling relative to signaling levels in gs subtype . 
these observations are in keeping with the tic and emt phenotypes , which are defining characteristics of claudin - low tumors . mutation and copy number alteration analysis we next examined somatic mutations and copy number alterations using tcga data set to compare genomic events of claudin - low subtype with those of nonclaudin - low gs subtype ( data supplement )  . 
tcga network reported rhoa and cdh1 mutations , and cldn18 - arhgap fusions were enriched in gs subtype.7 we did not observe significant differences in the frequency of these genomic events between the two subtypes ( data supplement )  . 
nonclaudin - low tumors ( n = 272 ) were classified into the following subtypes : ebv , 17 tumors ; msi , 63 tumors ; cin , 162 tumors ; and gs , 30 tumors . 
we found that claudin - low subtype in the acrg data set was phenotypically similar to the initially derived claudin - low subtype in the discovery tcga data set as measured by expression of the claudin , emt , and tic gene signatures ( data supplement )  . 
bar graph of the most significantly activated ( gold ) or inactivated ( blue ) signaling pathways in claudin - low subtype ( n = 46 ) compared with gs subtype ( n = 41 )  . significance was determined using ipa software . 
to further compare prognosis for claudin - low subtype with gs subtype , with adjustment for potential confounders ( age and pathologic stage ) , we performed cox proportional hazards regression modeling by setting gs type as a reference group ( table 1 )  . 
in addition , we assessed a prognostic value of claudin - low subtype in patients with stage iii cancer because it was the largest subgroup with the most equal distribution of subtypes . 
similar hrs from the two independent data sets suggest that claudin - low subtype of gastric cancer has a poor prognosis as a result of its unique biologic features . tcga overall survival by subtype acrg overall survival by subtype claudin fig 5 . 
prognosis of claudin - low tumors in ( a ) the cancer genome atlas ( tcga ) and ( b ) the asian cancer research group ( acrg ) data sets . unadjusted kaplan - meier plots show overall survival of gastric cancer by molecular subtype . significance was determined by log - rank test ( n = 415 in tcga cohort ; n = 300 in the acrg cohort )  . 
thus , we especially focused on comparing molecular and clinical features of claudin - low tumors with those of nonclaudin - low gs tumors . claudin - low gastric cancer was defined by low expression levels of tight - junction claudins , high levels of emt , and enrichment for tic signatures . 
in addition , compared with gs subtype , claudin - low subtype had the lower expression of proliferation signature , significant activation in rho family of gtpases signaling , and enrichment of cell motility and adhesion - associated pathways . furthermore , the claudin - low subtype conferred significantly worse prognosis than the gs subtype , which had comparable survival to the cin and ebv subtypes . 
these observations support the claim that claudin - low subtype is distinct from gs subtype and warrants additional validation in prospective studies . we report a 24 - gene classifier that accurately classifies gastric cancer into claudin - low and non claudin - low subtypes . 
we applied this classifier to the acrg data set and identified 28 claudin - low tumors that were phenotypically similar to the initially derived claudin - low subtype in the discovery data set . 
adjusted for age and pathologic stage ( n = 415 in tcga cohort ; n = 300 in the acrg cohort )  . abbreviations : acrg , asian cancer research group ; cin , chromosomally unstable ; ebv , epsteinbarr virus ; gs , genomically stable ; msi , microsatellite unstable ; tcga , the cancer genome atlas . are also characterized by low expression of claudins and enrichment for tic signatures . 
the combined expression of emt and cancer stem - cell makers was reported to be associated with aggressive clinical features , such as vascular invasion and metastasis , and prognostic of poorer disease - free and overall survival in a study of 276 patients with gastric cancer.25 moreover , emt and / or stem - celllike biologic processes have been linked to resistance to chemotherapy and radiation.26 - 28 the mechanisms of therapeutic resistance include relative quiescence , expression of atp - binding cassette transporters , an active dna - repair capacity , and a resistance to apoptosis.29 recent work by yoon et al22 demonstrated a role of rhoa , a member of the rho family of gtpases , in gastric cancer stem - like cells ( cscs ) for the maintenance of emt phenotypes and chemotherapy resistance . 
furthermore , rhoa pathway inhibition reversed chemoresistance in diffuse gastric cscs resistant to fluorouracil and cisplatof note , our ipa revealed that , compared with gs subtype , the most significantly activated and inactivated pathway in claudin - low subtype were rho family of gtpases signaling and rhogdi signaling , respectively . 
gdis are regulators of rho gtpases and prevent activation of gtpases by acting as molecular chaperones.30 all things considered , dysregulated rho gtpase signaling appears to play a key role in the biology of gastric claudinlow tumors and contributes to the poor prognosis . 
sanoff research funding : bayer ag ( inst ) , novartis ( inst ) , merck ( inst ) , precision biologics ( inst ) , immunomedics ( inst ) references 1 . 
sabatier r , finetti p , guille a , et al : claudin - low breast cancers : clinical , pathological , molecular and prognostic jci insight 1 : e85902 , 2016 characterization . 
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ryu hs , park dj , kim hh , et al : combination of epithelial - mesenchymal transition and cancer stem cell - like phenotypes has independent prognostic value in gastric cancer . 
takaishi s , okumura t , tu s , et al : identification of gastric cancer stem cells using the cell surface marker cd44 . stem cells 27 : 1006 - 1020 , 2009 27 . 
miller , md3 ; and razelle kurzrock , md2 , 5 purpose high - grade neuroendocrine cervical cancer ( hgnecc ) is an uncommon malignancy with limited therapeutic options ; treatment is patterned after the histologically similar small - cell lung cancer ( sclc )  . 
these results were subsequently compared with a cohort of 1 , 800 sclcs . results the median age of patients with hgnecc was 40.5 years ; 83 patients ( 85.6% ) harbored high - risk human papillomavirus ( hpv )  . 
overall , 294 genomic alterations ( gas ) were identied ( median , 2 gas / sample ; average , 3.0 gas / sample , range , 0 - 25 gas / sample ) in 109 distinct genes . 
seventy - one patients ( 73% ) had 1 alteration that was theoretically druggable . comparing hgnecc with sclc , signicant differences in tmb , microsatellite instability , hpv - positive status , and in pik3ca , myc , pten , tp53 , arid1a , and rb1 alteration rates were found . conclusion this large cohort of patients with hgnecc demonstrated a genomic landscape distinct from sclc , calling into question the biologic and therapeutic relevance of the histologic similarities between the entities . furthermore , 73% of hgnecc tumors had potentially actionable alterations , suggesting novel treatment strategies for this aggressive malignancy . jco precis oncol 4 : 972 - 987 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the treatment of solid malignancies has evolved and is perhaps best exemplied by the approach to non small - cell lung cancer , for which molecular characterization and use of targeted agents have emerged as standard therapeutic paradigms . 
recently , the cancer genome atlas ( tcga ) completed and published the integrated genomic and molecular characterization of cervical cancer.1 in addition to data previously released for both ovarian ( high - grade serous ) and endometrial ( endometrioid and serous ) cancers , this publication completed the molecular and genomic evaluation of the most common gynecologic malignancies.2 , 3 traditionally , cervical cancer clinical trials have excluded less common histologies such as high - grade neuroendocrine cervical carcinoma ( hgnecc )  . 
despite the low incidence of hgnecc ( , 2% of all cervical cancers ) the oncologic impact is signicant because these tumors exhibit more aggressive clinical characteristics.4 , 5 unfortunately , the 5 - year overall survival rate for patients with early - stage disease is only a 36% , and those with metastatic spread face an even more dismal prognosis . 
given these poor outcomes , patients with hgnecc represent an area of unmet clinical need . developing therapeutic options for patients with rare tumors is challenging , relying on international collaboration , as well as small case series or retrospective reports rather than prospective clinical trials . 
 genomic landscape of high - grade neuroendocrine cervix cancer context key objective to dene the molecular landscape of high - grade neuroendocrine cervical cancer in a large cohort of patients . knowledge generated high - grade neuroendocrine cervical cancer appears molecularly distinct from the histologically similar small - cell lung cancer . up to 73% of patients samples harbored potentially actionable alterations , informing novel treatment strategies . relevance continued understanding of the molecular underpinnings of high - grade neuroendocrine cervical carcinoma will be critical to driving drug discovery for this disease . approved by the food and drug administration ( fda ) specically for hgnecc.8 recently , 2 reports of exceptional responses to immune checkpoint inhibition in patients with recurrent hgnecc were published.9 , 10 to better understand these responses and to identify molecular aberrations underlying this uncommon malignancy , we examined the genomic landscape of hgnecc . 
the submitting physicians provided specication of a poorly differentiated , neuroendocrine tumor type of cervical origin , which was then independently reviewed by a gynecologic pathologist ( j.e. ) to conrm high - grade neuroendocrine pathologic features in the pathology report and / or the representative sample of tumor submitted for sequencing ( grade 3 cytomorphologic features , some component of small - cell or large - cell carcinoma histology , and / or positivity for neuroendocrine markers )  . 
ngs data were generated by foundationone ( foundation medicine ; cambridge , ma )  . the study was performed in accordance with university of california , san diego , institutional review board guidelines for a de - identied database . 
the test sequences the entire coding region of 182 or , more recently , 236 or 315 cancer - related genes plus up to 47 introns of up to 19 genes often rearranged or altered in cancer to an average depth of coverage of  . 
500.11 the pathologic diagnosis of each case was conrmed on routine hematoxylinand eosin - stained slides and all samples forwarded for dna extraction contained a minimum of 20% tumor nuclear area . 
microsatellite instability ( msi ) status was evaluable in 75 hgnecc and 1 , 573 sclc cases . the sequencing methods used for comprehensive genomic proling have been validated and reported previously ( appendix ) .12 , 13 the optimized loci used to evaluate msi status were selected from a total set of 1 , 897 that have adequate coverage on all versions of the assay . 
there was no need to extend beyond the rst principal component , because it explained approximately 50% of the total data variance , whereas none of the other principal components explained  . 
msi - low calls are not made because there was no gold - standard test set , but we presume such samples would signicantly overlap with the msiambiguous category reported here . 
the cutoff of 20 coding mutations / mb is approximately equal to 400 nonsynonymous mutations per exome.15 human papillomavirus detection in addition , the presence of high - risk human papillomavirus ( hpv ) was examined in submitted specimens , as previously reported.16 hybrid - capture reagents included baits designed to capture unique regions of select viral genomes including hpv - 16 and - 18 . 
a total hpv - 16 / 18 aligned read count of 5 reads per million was considered a positive hpv status , and , 5 reads per million was considered hpv not detected.16 end points and statistical methods descriptive statistics were used to summarize the baseline patient characteristics . 
all statistical tests were carried out using graphpad prism , version 6.0 ( graphpad software , san diego , ca )  . results characterization of gas in hgnecc the median age of the cohort was 40.5 years ( range , 25 - 77 years )  . 
the most frequently reported number of gas per sample was 2 , with a range of 0 - 25 ( average , 3.0 gas / sample ; fig 2 )  . 
5% of samples are depicted . variants of unknown signicance excluded . genomics in hpv - positive versus - negative patients when examining distribution of gas on the basis of hpv detection status , a signicant difference was identied in the frequency of several gas , including pik3ca , tp53 , pten , arid1a , and rb1 , all of which were more frequent in the hpv - negative subgroup ( table 1 )  . 
two of the 3 cases were both msi - h and tmb - h and harbored the highest numbers of identiable gas in the cohort.17 , 18 the third case , with a nonsense mutation near the 3 ( cid : 3 ) end of the coding sequence ( msh2 r929 * ) , was mss and tmb - l . the 2 msh - 2mutant msi - h cases were both of small - cell histology and accounted for all msi - h cases out of the 75 no . 
furthermore , a total of 40 patient samples ( 41.2% ) harbored mutations in the pi3k / akt / mtor pathway ; mutations in pik3ca were identied in 47.5% of these samples ( n = 19 ) , and pten mutations were reported in 35% ( n = 14 )  . 
the small - cell subset of hgnecc samples showed analogous gene mutation differences from sclc . discussion neuroendocrine carcinoma is an uncommon but aggressive variant accounting for approximately 1.5% of all newly diagnosed cervical cancers.20 the great majority of these lesions are high - grade largeor small - cell subtypes , with only rare reports of well - differentiated cervical carcinoid tumors.20 the treatment of patients with hgnecc remains table 2 . 
 eskander et al clinically challenging , with limited response rates to chemotherapy ; however , anecdotal reports of exceptional responders have been described.9 , 10 the paradigm for management of hgnecc has been informed by the treatment of the more commonly diagnosed ( and histologically similar ) sclc , which accounts for approximately 15% of all lung cancer cases . 
in prior studies , whole - genome sequencing of 110 sclc specimens identied essentially ubiquitous tp53 and rb1 inactivating mutations , with biallelic losses of each gene respectively in 100% and 93% of cases without chromothripsis.21 in an effort to better dene the molecular landscape of hgnecc , we evaluated the comprehensive genomic proling of 97 patient samples . 
at least 1 characterized alteration was identied in 88 patient samples ( 90.7% ) and of these , 72 had a potentially pharmacologically tractable alteration . interestingly , the frequency and distribution of gas identied in this cohort of patients are similar and distinct from mutational patterns described in the more common hpvrelated cervical cancer histologies.1 as detailed in tcgas integrated genomic characterization of cervical cancer ( ie , squamous , adenocarcinoma , and adenosquamous histologies ) , mutations in the pik3ca gene were the most frequently identied aberration , occurring in 26% of samples , approximating the nearly 20% rate in our cohort . in addition , signicantly mutated genes reported by the tcga , identied in similar proportions in this patient cohort , included arid1a ( 7% in tcga and 9.3% in our cohort ) and kras ( 6% in tcga and 8.2% in our cohort )  . 
these molecular differences may be reective of the varying histologies or , potentially , the differential highrisk hpv detection rates ( 85.6% in our cohort v 95% in the tcga ) .1 importantly , the high - risk hpv rate in our cohort should be interpreted with caution because the assay used has not undergone formal concordance study with gold standard tests such as hybrid capture and can detect only hpv 16 / 18 . our own , much larger cohort of sclc samples ( n = 1 , 800 ) recapitulates prior studies and had a strikingly different molecular portfolio when compared with hgnecc samples . 
msi - h status was also more common in the hgnecc cohort whereas tmb - i / tmb - h was more common in sclc ( despite the lack of msi - h status )  . 
the use of everolimus , or an alternate mtor or pik3ca inhibitor , may be considered in such circumstances , although the utility of a pik3ca mutation in predicting response to single - agent everolimus in the presence of multiple gas remains limited.26 , 27 although less frequently identied , alterations in the hrd pathway were detected in 9.3% of patient samples , potentially supporting use of a poly - adp ribose polymerase inhibitor . 
the identication of both tmb - h ( n = 2 ) and gas in mismatch repair genes ( n = 3 ) may also inform the use of immune checkpoint inhibition.28 in may 2017 , the fda approved pembrolizumab for the treatment of mismatch repairdecient or msi - h solid tumors that progressed after prior therapy . 
more recently , the fda accepted and granted priority review to a supplemental biologics license application for pembrolizumab for the treatment of adult and pediatric patients with unresectable or metastatic solid tumors with tissue tmb - h whose disease has progressed after prior treatment and who have no satisfactory alternative treatment options , supported by data from the phase ii keynote - 158 trial . 
notably , there are 2 published case reports of patients with recurrent , treatment - refractory hgnecc with exceptional and durable responses to checkpoint inhibition ; 1 of these tumors was from our current hgnecc cohort and had a mismatch repair defect and the other lacked correlative genomic testing.9 , 10 last , the identication of arid1a ( 9.3% ) and smarca4 ( 4.1% ) mutations may predict sensitivity to an alternate therapeutic strategy.29 homeostasis requires balanced arid1a and ezh2 activity , facilitated via chromatinmediated gene expression . 
 genomic landscape of high - grade neuroendocrine cervix cancer aberrations were identied in patients with msi - h lesions , possibly reecting that the smarca4 may be a passenger mutation resulting from the underlying msi . 
furthermore , of the 4 cases with smarca4 alterations , 1 was hpv - 18 positive and another was p16 positive by immunohistochemical assessment . despite the large sample size and robust genomic data , this study has limitations . 
95% of the identied high - risk hpv strains.30 this report highlights the potential therapeutic utility of genomic testing in patients with this uncommon disease.27 interest , despite the histologic similarity between hgnecc and sclc , which has led to the latter being used as a model for treating the former , the molecular portfolio of these 2 entities is strikingly different . 
therefore , plausible that patients with hgnecc may benet from alternative therapeutic strategies . it is not anticipated that traditional prospective trials will accrue sufcient patient numbers in this disease setting , and novel study designs , including umbrella , basket , and platform trials , should be considered given the presence of actionable targets . 
interestingly , the rst reported cohort of the dart trial ( clinicaltrials.gov identier : nct02834013 ) 31 was the neuroendocrine cohort , with a 44% overall response rate in those with high - grade disease . 
eskander consulting or advisory role : pzer , clovis oncology , astrazeneca / medimmune , tesaro , merck speakers bureau : clovis oncology , astrazeneca / medimmune , roche travel , accommodations , expenses : clovis oncology , astrazeneca / medimmune , roche , merck , pzer julia elvin employment : foundation medicine stock and other ownership interests : hoffman - laroche laurie gay employment : foundation medicine , invitae stock and other ownership interests : foundation medicine , naveris , invitae consulting or advisory role : invitae , naveris jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : celsius therapeutics research funding : foundation medicine vincent a . 
 eskander et al leadership : foundation medicine , revolution medicines stock and other ownership interests : foundation medicine , mirati therapeutics , revolution medicines patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center razelle kurzrock leadership : curematch , curemetrix stock and other ownership interests : curematch , idbydna , soluventis honoraria : roche , eusa pharma , neogenomics laboratories , biocom , neomed therapeutics , advanced therapeutics , lek , aacr , chugai pharma usa , wiley consulting or advisory role : actuate therapeutics , loxo , xbiotech , neomed , roche , gaido , soluventis , pzer , merck speakers bureau : roche , guardant health ( inst ) research funding : sequenom ( inst ) , merck serono ( inst ) , genentech ( inst ) , pzer ( inst ) , foundation medicine ( inst ) , incyte ( inst ) , konica minolta ( inst ) , grifols ( inst ) , omniseq ( inst ) , debiopharm group ( inst ) , boerhinger ingelheim ( inst ) travel , accommodations , expenses : roche , eusa pharma , neogenomics laboratories , biocom , neomed therapeutics , advanced therapeutics , lek , aacr , chugai pharma usa , wiley no other potential conicts of interest were reported . references cancer genome atlas research network : integrated genomic and molecular characterization of cervical cancer . 
nature 497 : 67 - 73 , 2013 [ erratum : nature 500 : 242 , 2013 ] cancer genome atlas research network : integrated genomic analyses of ovarian carcinoma . 
nature 474 : 609 - 615 , 2011 [ erratum : nature 490 : 298 , 2012 ] gardner gj , reidy - lagunes d , gehrig pa : neuroendocrine tumors of the gynecologic tract : a society of gynecologic oncology ( sgo ) clinical document . gynecol oncol 122 : 190 - 198 , 2011 satoh t , takei y , et al : gynecologic cancer intergroup ( gcig ) consensus review for small cell carcinoma of the cervix . 
int j gynecol cancer 24 : s102 - s108 , 2014 ( 9 suppl 3 ) fukuoka m , masuda n , furuse k , et al : a randomized trial in inoperable non - small - cell lung cancer : vindesine and cisplatin versus mitomycin , vindesine , and cisplatin versus etoposide and cisplatin alternating with vindesine and mitomycj clin oncol 9 : 606 - 613 , 1991 kubota k , hida t , ishikura s , et al : etoposide and cisplatin versus irinotecan and cisplatin in patients with limited - stage small - cell lung cancer treated with etoposide and cisplatin plus concurrent accelerated hyperfractionated thoracic radiotherapy ( jcog0202 ) : a randomised phase 3 study . 
lancet oncol 15 : 106 - 113 , 2014 ishikawa m , kasamatsu t , tsuda h , et al : prognostic factors and optimal therapy for stages i - ii neuroendocrine carcinomas of the uterine cervix : a multi - center retrospective study . 
gynecol oncol 148 : 139 - 146 , 2018 paraghamian se , longoria tc , eskander rn : metastatic small cell neuroendocrine carcinoma of the cervix treated with the pd - 1 inhibitor , nivolumab : a case report . 
sharabi a , kim ss , kato s , et al : exceptional response to nivolumab and stereotactic body radiation therapy ( sbrt ) in neuroendocrine cervical carcinoma with high tumor mutational burden : management considerations from the center for personalized cancer therapy at uc san diego moores cancer center . oncologist 22 : 631 - 637 , 2017 11 . 
ross js , fakih m , ali sm , et al : targeting her2 in colorectal cancer : the landscape of amplication and short variant mutations in erbb2 and erbb3 . 
genome med 9 : 34 , 2017 johnson db , frampton gm , rioth mj , et al : targeted next generation sequencing identies markers of response to pd - 1 blockade . 
chae yk , pan ap , davis aa , et al : path toward precision oncology : review of targeted therapy studies and tools to aid in dening actionability of a molecular lesion and patient management support . 
kato s , kurasaki k , ikeda s , et al : rare tumor clinic : the university of california san diego moores cancer center experience with a precision therapy 25 . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecularp : results from mypathway , an openlabel , phase iia multiple basket study . 
j clin oncol 36 : 536 - 542 , 2018 janku f , hong ds , fu s , et al : assessing pik3ca and pten in early - phase trials with pi3k / akt / mtor inhibitors . 
alejo m , alemany l , clavero o , et al : contribution of human papillomavirus in neuroendocrine tumors from a series of 10 , 575 invasive cervical cancer cases . pract 4 : 17 , 2017 papillomavirus res 5 : 134 - 142 , 2018 31 . 
patel sp , othus m , chae yk , et al : a phase ii basket trial of dual anti - ctla - 4 and anti - pd - 1 blockade in rare tumors ( dart ) s1609 : the neuroendocrine cohort . presented at the american association for cancer research annual meeting , atlanta , ga , march 29 - april 3 , 2019 ( abstr ct039 )  . 
briey , after pathologic review to conrm sufcient tumor nuclei ( minimum , 20% ) and mitigate pathologic inconsistencies , at least 50 ng of dna was extracted from 40 tumor samples provided as formalin - xed , parafnmicrons of embedded tissue blocks . 
the samples were assayed using adaptorligation and hybrid - capture next - generation sequencing ( foundationone ) for all coding exons from 182 ( version 1 ) , 287 ( version 2 ) , or 315 ( version 3 ) cancer - related genes plus selected introns from 14 ( version 1 ) , 19 ( version 2 ) , or 28 ( version 3 ) genes frequently rearranged in cancer . sequencing of captured libraries was performed using hisequation 2500 / 4000 ( illumina , san diego , ca ) to a mean exon coverage depth of  . 
500 , and resultant sequences were analyzed using both an algorithmic pipeline and manual curation for base substitutions , small insertions or deletions ( indels ) , copy number alterations ( focal amplications and homozygous deletions ) , and selected gene fusions , as previously described.13 clinically relevant genomic alterations were dened as alterations targetable by anticancer drugs currently available on the market or in registered clinical trials . 
germline variants documented in the dbsnp database ( dbsnp142 ; nlm.nih.gov / snp / ) , with 2 counts in the exac database ( broadinstitute.org / ) , or recurrent variants of unknown signicance that were predicted by an internally developed algorithm to be germline were removed , with the exception of known driver germline events.12 known , conrmed somatic alterations deposited in the catalog of somatic mutations in cancer ( version 62 ) were highlighted as biologically signicant , as were inactivating events in tumor suppressor genes . 
all four patients received selpercatinib ( capsule or liquid formulation ) orally in continuous 28 - day cycles at a starting dose of 90 mg / m2 twice per day . this dose was intended to deliver exposure equivalent to the recommended adult phase ii dose of 160 mg twice per day . 
one patient was enrolled to the 80 - mg cohort of trial ( clinicaltrials.gov identier : nct03157128 ) and underwent intrapatient dose escalation to 160 mg per protocol . the ongoing selpercatinib phase i / ii pharmacokinetic analysis serial blood samples were collected for pharmacokinetic analyses . 
molecular analysis showed that the tumor harbored an ret exon 6 deletion ( d378_ g685.e ) , and the patient was treated sequentially with four multitargeted kinase inhibitors : vandetanib , sunitinib , cabozantinib , and lenvatinib , which were each discontinued because of either adverse events or lack of efcacy . 
a 7 - year - old boy with neonatal hypotonia , abdominal pain , hollow feet , and unexplained laryngeal spasms was referred for diagnostic exome sequencing of genomic dna ( sureselect xt clinical research exome , agilent , santa clara , ca )  . 
this revealed a constitutional de novo ret m918t mutation , a pathogenic variant associated with men2b that confers the highest risk of early onset mtc.16 the patient was subsequently diagnosed with an mtc and underwent thyroidectomy with tracheostomy followed by vandetanib therapy , which was discontinued because of the onset of grade 3 colitis . selpercatinib was subsequently initiated at 90 mg twice per day . 
magnetic resonance imaging demonstrated new lung nodules indicative of metastatic disease . an rna - based next - generation sequencing ( ngs ) fusion assay ( solid fusion assay v2 ; archerdx , boulder , co ) indicated that the tumor harbored an myh10 - ret gene fusion . 
the patient was started on vandetanib and achieved a partial tumor response by response evaluation criteria in solid tumors ( recist ) 1.1.22 however , after 4 months of treatment , she developed disease progression at the primary site . 
repeat imaging after 6 months of treatment showed complete resolution of the paraspinal mass and a 50% decrease in the size of the retroperitoneal , pelvic , and lumbosacral mass ( fig 2a - d )  . 
during repair of congenital bilateral inguinal hernias , a 2 - month - old girl was found to have a right renal mass , and she underwent a right nephrectomy . 
patient 1 : magnetic resonance imaging scans of ( a ) right lateral and ( b ) left anterior liver metastatic lesions at baseline and after 22 months of treatment with selpercatinib of ( c ) right lateral and ( d ) left anterior in a heavily pretreated patient with ret - mutated medullary thyroid cancer . 
patient 3 : ( a , c ) computed tomography ( ct ) scans of the abdomen at baseline and ( b , d ) after 6 months of treatment with selpercatinib , revealing multiple paraspinal retroperitoneal and pelvic lesions in a patient with infantile myobroma / hemangiopericytoma harboring an myh10 - ret fusion . 
a partial response was observed after one cycle of selpercatinib ; after six cycles , the paraspinal lesion had completely resolved , and the patient regained lower extremity neurologic function . 
patient 4 : ct scans at baseline of ( e ) the lungs and ( g ) brain and after 8 months of treatment with selpercatinib of ( f ) the lungs and ( h ) brain in a patient with an specc1l - ret fusionpositive congenital mesoblastic nephroma and infantile brosarcoma . 
patient 5 : ct scans ( i , k ) at baseline and ( j , l ) after 2 months of treatment with selpercatinib of the left foot in a patient with an ncoa4 - ret fusionpositive lipobromatosis . 
abdominal ultrasound and chest x - ray identied a mass in the left kidney and a large left lower lung mass ; computed tomography imaging conrmed these lesions and identied additional , multiple small lung lesions . 
biopsy of a lung mass revealed high - grade spindle cell sarcoma consistent with an infantile brosarcoma ; pathology review of the original right nephrectomy specimen conrmed the initial diagnosis of mesoblastic nephroma . 
the patient received additional chemotherapy with cyclophosphamide and topotecan , but treatment was complicated by febrile neutropenia and enterococcus faecalis ventriculitis . dna - based ngs ( using memorial sloan kettering integrated mutation proling of actionable cancer targets [ msk - impact ] ) of the tumor from the renal and lung masses identied the same specc1l - ret gene fusion , and the patient initiated treatment with selpercatinib . after two cycles , a partial response was observed with a 41% tumor reduction , ( fig 2e - h )  . 
a selpercatinib concentration of 4.5 ng / ml was achieved in cerebrospinal uid at a dose level of 48 mg twice per day ( 90 mg / m2 per dose )  . upon detection and resection of an isolated metastasis at the right posterior temporal occipital junction , the dose of selpercatinib was increased to 94 mg ( 180 mg / m2 ) twice per day , raising the concentration of the drug to 16 ng / ml in the cerebrospinal uid . 
 selpercatinib in pediatric ret - altered cancer libretto - 001 ( 160 mg , day 8 ) patient 3 patient 4 patient 5 6 , 000 4 , 000 2 , 000 time ( hours ) fig 3 . 
plasma samples from three patients revealed that adequate plasma concentrations of selpercatinib were achieved ( greater than ret wild - type concentration that inhibits 90% [ ic90 ] ) , which were within the range seen in adult patients treated with the recommended dose of 160 mg in the libretto - 001 trial . 
the gray area represents the 95% cis for the median plasma concentrations observed in patients treated in the libretto - 001 trial ( red circles )  . fusion , which was conrmed by whole genome and transcriptome analysis . 
selpercatinib was initiated , and imaging after 2 months revealed a partial response by recist 1.1 , with a 59% reduction in tumor volume and resolution of tumor inltration of the metatarsals ( fig 2i - l )  . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . sandya govinda raju employment : loxo oncology dahlia henry employment : loxo oncology stock and other ownership interests : loxo oncology , allergan , axovant sciences , palatin technologies steve smith consulting or advisory role : various , loxo oncology patents , royalties , other intellectual property : various patents and applications travel , accommodations , expenses : various s . 
cox employment : bayer , loxo oncology , merck kgaa , amgen , day one biopharmaceuticals stock and other ownership interests : loxo oncology , bayer , merck kgaa , amgen , day one biopharmaceuticals patents , royalties , other intellectual property : us patent 62 / 318 , 041 issued to loxo oncology ( inst ) julia glade bender consulting or advisory role : abbvie ( inst ) research funding : celgene ( inst ) , merck ( inst ) , pzer ( inst ) , amgen ( inst ) , ignyta ( inst ) , bristol - myers squibb ( inst ) , eisai ( inst ) , novartis ( inst ) , eli lilly ( inst ) , loxo oncology ( inst ) , genentech ( inst ) travel , accommodations , expenses : novartis , amgen , merck , bayer , genentech uncompensated relationships : springworks therapeutics , bristol - myers squibb a . 
lindsay frazier stock and other ownership interests : decibel therapeutics consulting or advisory role : decibel therapeutics peter anderson stock and other ownership interests : healios consulting or advisory role : enlivity patents , royalties , other intellectual property : patent for glutamine and trehalose compositions ; priority date 13 september 2013 ; app 14 / 470 , 545 , led august 27 , 2014 ; patent 61 / 878 , 084 issued december 26 , 2017 other relationship : enlivity alberto s . 
pappo honoraria : bayer , roche consulting or advisory role : merck , loxo oncology / bayer , eusa pharma no other potential conicts of interest were reported . acknowledgments we thank the patients and their families and contributing clinical staff across all sites . 
medical writing services were provided by jim heighway of cancer communications and consultancy , knutsford , united kingdom , and were funded by loxo oncology , stamford , ct . references kato s , subbiah v , marchlik e , et al : ret aberrations in diverse cancers : next - generation sequencing of 4 , 871 patients . 
clin cancer res 23 : 1988 - 1997 , 2017 ceccherini i , pasini b , pacini f , et al : somatic in frame deletions not involving juxtamembranous cysteine residues strongly activate the ret proto - oncogene . oncogene 14 : 2609 - 2612 , 1997 prescott jd , zeiger ma : the ret oncogene in papillary thyroid carcinoma . 
nat commun 9 : 4821 , 2018 ferrara r , auger n , auclin e , et al : clinical and translational implications of ret rearrangements in non - small cell lung cancer . 
j thorac oncol 13 : 27 - 45 , 2018 cordioli mi , moraes l , bastos au , et al : fusion oncogenes are the main genetic events found in sporadic papillary thyroid carcinomas from children . 
thyroid 27 : 182 - 188 , 2017 fenton cl , lukes y , nicholson d , et al : the ret / ptc mutations are common in sporadic papillary thyroid carcinoma of children and young adults . 
j clin endocrinol metab 85 : 1170 - 1175 , 2000 prasad ml , vyas m , horne mj , et al : ntrk fusion oncogenes in pediatric papillary thyroid carcinoma in northeast united states . 
cancer 122 : 1097 - 1107 , 2016 vanden borre p , schrock ab , anderson pm , et al : pediatric , adolescent , and young adult thyroid carcinoma harbors frequent and diverse targetable genomic alterations , including kinase fusions . 
carvalho d , mackay a , bjerke l , et al : the prognostic role of intragenic copy number breakpoints and identication of novel fusion genes in paediatric high 11 . 
al - ibraheemi a , folpe al , perez - atayde ar , et al : aberrant receptor tyrosine kinase signaling in lipobromatosis : a clinicopathological and molecular genetic grade glioma . 
antonescu cr , suurmeijer aj , zhang l , et al : molecular characterization of inammatory myobroblastic tumors with frequent alk and ros1 gene fusions and rare novel ret rearrangement . 
elisei r , cosci b , romei c , et al : prognostic signicance of somatic ret oncogene mutations in sporadic medullary thyroid cancer : a 10 - year follow - up study . j clin endocrinol metab 93 : 682 - 687 , 2008 16 . 
latteyer s , klein - hitpass l , khandanpour c , et al : a 6 - base pair in frame germline deletion in exon 7 of ret leads to increased ret phosphorylation , erk activation , and men2a . 
wirth lj , kohno t , udagawa h , et al : emergence and targeting of acquired and hereditary resistance to multikinase ret inhibition in patients with ret - altered 20 . 
drilon ae , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
antonescu cr , dickson bc , swanson d , et al : spindle cell tumors with ret gene fusions exhibit a morphologic spectrum akin to tumors with ntrk gene 26 . 
wells sa jr , robinson bg , gagel rf , et al : vandetanib in patients with locally advanced or metastatic medullary thyroid cancer : a randomized , double - blind 28 . 
schlumberger m , jarzab b , cabanillas me , et al : a phase ii trial of the multitargeted tyrosine kinase inhibitor lenvatinib ( e7080 ) in advanced medullary thyroid 30 . 
gautschi o , milia j , filleron t , et al : targeting ret in patients with ret - rearranged lung cancers : results from the global , multicenter ret registry . 
yoh k , seto t , satouchi m , et al : vandetanib in patients with previously treated ret - rearranged advanced non - small - cell lung cancer ( luret ) : an open - label , multicentre phase 2 trial . 
kasi , mbbs , md , ms1 ; judong yang , md , ms2 ; phani keerthi surapaneni , mbbs1 ; tanios bekaii - saab , md3 ; daniel h . 
borad , md3 purpose recent advances in molecular diagnostic technologies have allowed for the evaluation of solid tumor malignancies via noninvasive blood sampling , including circulating tumor dna ( ctdna ) proling . 
after excluding variants of unknown signicance , therapeutically relevant alterations were observed in 76 patients ( 55% ) , including braf mutations , erbb2 amplications , fgfr2 fusions , fgfr2 mutations , and idh1 mutations seen in 21% of patients . 
a different spectrum of alterations was observed in patients with early - onset btc ( younger than age 50 years ) compared with older patients ( older than age 50 years )  . conclusion data on ctdna in btc is currently limited . 
intact circulating tumor cells and cell - free dna ( cfdna ) from both leukocytes and tumors ( circulating tumor dna [ ctdna ] ) can now be isolated and analyzed using advanced sequencing methods . 
ctdna has been shown to carry tumor - specic genetic or epigenetic alterations , such as point mutations , copy number variations , chromosomal rearrangements , and dna methylation patterns.1 - 4 the testing approaches in this eld are two dominant polymerase chain reaction ( pcr ) based ( digital pcr ) and next - generation sequencing ( ngs )  . 
ngs approaches have the ability to investigate a larger these number of genes simultaneously ; however , techniques have historically been limited by the need for high sensitivity and specicity and the cost associated with sequencing . 
this approach allows for agnostic analysis of large portions of the genome and can identify multiple mutations with increased sensitivity.5 evaluation of ctdna is particularly attractive as it enables the assessment of patient - specic tumoral genetic / epigenetic alterations while allowing for serial monitoring of tumor genomes in a noninvasive , convenient , and accurate manner . 
 mody et al biliary tract cancers ( btcs ) are an uncommon malignancy arising from epithelial cells that line the biliary tree and have a rapidly fatal course , with 5 - year survival rates of less than 10%.1 , 2 although relatively rare in western countries , btcs are more prevalent in southeast asia.3 in the united states , btcs account for approximately 2% of all new cancer diagnoses and have been rising in incidence during the past few decades.4 - 10 patients with cholangiocarcinoma stand to gain immensely from the use of ctdna given that diagnosis currently is more often made at advanced stages of disease ; recurrences are common , despite the pursuit of potentially curable treatments , such as surgery in a subset of patients ; biopsies are not always obtained or often yield suboptimal quantities of tumor cells for tissue - based genomic proling ; and multiple genomic alterations , which are potential therapeutic targets , are known to occur in btcs . 
genetic alterations that have been identied include activating kras mutations , tp53 mutations / deletions , idh1 and idh2 mutations , fgfr2 gene fusions , cdkn2a / b mutations / deletions , and , less commonly , ntrk gene fusions and alterations in erbb2 ( her2 ) , met , braf , nras , and pik3ca.6 , 7 therefore , the purpose of the current study was to examine the results of ctdna testing from a large cohort of patients with btc at a national cancer institute comprehensive cancer center , acquired in the course of clinical practice , and to characterize the mutational landscape of btcs using this technology . 
data analysis from this patient cohort was reviewed and approved by the mayo clinic institutional review board . demographic information and the date of blood collection were available for all patients . 
additional patient information was collected from the mayo clinic electronic medical record and included conrmation of btc diagnosis ; risk factors , including history of hepatitis a , b , or c , nonviral chronic liver disease , diabetes , obesity , or primary sclerosing cholangitis ; and pertinent clinical information , such as treatment status at the time of ctdna testing and history of liver - directed therapy . comprehensive genomic testing in plasma cfdna was extracted from whole blood collected in 10 - ml streck tubes . 
samples were shipped to a clinical laboratory improvement actcertied , college of american pathologistsaccredited laboratory ( guardant health )  . after double ultracentrifugation , 5 to 30 ng cfdna was isolated for digital sequencing . cfdna fragments , both leukocyte and tumor derived , were simultaneously sequenced . 
analytical sensitivity allowed for the detection of one to two mutant fragments in a 10 - ml blood sample ( 0.1% limit of detection ) with analytic specicity of more than 99.9999%. twelve copy number alterations were reported as the absolute gene copy number in plasma . 
as most cfdna is leukocyte derived , the gene copy number is generally 2.0. tumor - derived dna shed into the bloodstream raises this value , but , because of the relative proportions of tumorderived versus leukocyte - derived cfdna , is typically a minor contributor . 
in the 68 - gene panel , eight genes were retired from the single - nucleotide variation gene set , whereas coverage of gene amplications expanded from three to 16 genes , and the addition of detection of fusions in four genes and insertions or deletion of bases ( indels ) in one gene was made . 
the 70 - gene panel included all national comprehensive cancer network somatic genomic targets , cluding complete or critical exon coverage in 30 and 40 genes , respectively , amplications in 14 genes , fusions in six genes , and indels in three genes . 
the majority of samples in this study ( n = 122 ) were tested using the 73 - gene panel . to determine if an alteration was therapeutically relevant , we dened therapeutically relevant as any gene alteration with an oncokb level of evidence of 1 , 2a , 2b , 3a , 3b , or r1.8 oncokb is a precision oncology knowledge base that contains information about the effects and treatment implications of specic cancer gene alterations.8 oncokb contains detailed information about specic alterations in 477 cancer genes compiled from various sources , cluding guidelines from the us food and drug administration ( fda ) , national comprehensive cancer network , asco , clinicaltrials.gov , and the scientic literature . 
level 4 includes those variants that are considered predictive of response to targeted agents on the basis of compelling biologic , nonclinical evidence . by these standards , a gene is considered therapeutically relevant if there is supporting evidence that the gene is a driver of tumorigenesis , and wherein actionability of the gene can refer to either sensitivity and / or resistance to a drug ( s )  . 
in addition , there must be a clinically available agent , including clinical trials , that targets the gene / protein for a specic agent , and there must be at least preclinical evidence that supports its role in targeting the specic gene / protein . on the basis of the aforementioned criteria , the following genes were considered actionable : akt1 , alk , araf , atm , braf , brca1 , brca1 , ccnd1 , ccnd2 , cdk4 , cdk6 , cdkn2a , ctnnb1 , egfr , erbb2 , esr1 , fgfr1 , fgfr2 , gnas , idh1 , idh2 , jak2 , kras , met , map2k1 , mlh1 , mtor , myc , ntrk1 , ntrk3 , pdgfra , pik3ca , raf1 , ptpn11 , stk11 , tsc1 , and vhl . 
finally , variants found in actionable genes that did not alter the amino acid sequencethat is , synonymous mutationsand / or those that lacked any supporting functional evidence of pathogenicity were excluded . statistical analysis the distribution of each continuous variable is summarized by its mean , standard deviation , and range . 
the relationship between gene types with regard to mutation and amplication , as well as synonymous and targetable status , was evaluated using spearmans rank correlation and was displayed in the correlation matrix in which nonsignicant correlations are marked with a blank in the graph . 
a small subset of patients had underlying chronic liver disease , such as primary sclerosing cholangitis ( 8% ) or other chronic liver disease ( 6% )  . landscape of alterations among a total of 138 ctdna samples , 105 ( 76% ) of these included one or more alterations when variants of unknown signicance were excluded . 
tp53 and kras were the two most common alterations in all subtypes of disease , followed by fgfr2 in 7% ( intrahepatic subtype ) , arid1a ( extrahepatic subtype ) and cdk6 , apc , and smad4 ( gallbladder subtype )  . 
in the more prevalent of the subtypes ( intrahepatic ) in our sampleaside from fgfr2pik3ca and idh1 were fairly commonly altered . a different spectrum of alterations was observed in patients with early - onset btc ( younger than age 50 years ) compared with older patients ( older than age 50 years ) , although overall the differences were not statistically signicant ( p = .55 ; fig 3 )  . 
other alterations which were more common in younger patients included pik3ca , met , and braf . therapeutically relevant alterations after excluding variants of unknown signicance , therapeutically relevant alterations were seen in 55% ( n = 76 ) of the total cohort of samples . 
several risk factors for btc have been described , with most etiologies resulting in long - standing inammation.9 , 12 the only standard systemic therapy for the disease is gemcitabine and cisplatthere is no standard second - line therapy that has been shown to unequivocally improve survival for patients who experience disease progression on gemcitabine / cisplatin.13 btcs are traditionally classied by location as intrahepatic , extrahepatic , and gallbladder on the basis of their presumed site of origin within the biliary duct systethis 4 2019 by american society of clinical oncology mody et al 65 ( 28 - 87 ) 85 ( 69 ) 22 ( 18 ) 16 ( 13 ) 60 ( 48 ) 63 ( 52 ) 42 ( 35 ) 38 ( 30 ) 43 ( 35 ) 21 ( 17 ) 14 ( 12 ) 10 ( 8 ) 2 ( 1 ) 6 ( 5 ) 15 ( 11 ) 30 ( 22 ) 26 ( 19 ) 19 ( 14 ) 48 ( 35 ) anatomic classication has been effective in differentiating btcs with regard to epidemiology , etiology , clinical presentation , and treatment.9 early diagnosis is ideal given that surgical resection or liver transplantationfor perihilar tumorsoffers the best chance at cure ; however , majority of patients are diagnosed with advanced - stage disease precluding surgical management . 
of particular importance , pathologic tissue - based conrmation of btc can be challenging given that clinical yield is often suboptimal and insufcient , especially for dna extraction to enable genomic proling . 
this is primarily a result of the more desmoplastic nature of many btc tumors . with the availability of next - generation genomic proling in recent years , a number of genomic subtypes of btc have been described , many of which are dened by therapeutically targetable genomic alterations.7 , 14 - 18 for example , fgfr fusion rearrangements and idh1 and idh2 mutations have emerged as signicant driver mutation genomic subtypes . 
at present , several targeted drugs are in clinical development , with encouraging results thus far . for the above reasons , the potential for use of ctdna in the management of btc is of particular interest . 
investigations of the use of ctdna in cca have previously been hampered by the rarity of the disease , the relatively incomplete understanding of the genetics of this cancer , and the lack of a validated and widely used ctdna assay . 
this has now changed with recent increased focus on the disease ; recent characterization of the btc genome by several studies , including that from the cancer genome atlas ; and also with the availability of a number of commercially available ctdna assays in clinical practice.14 , 15 , 19 thus far , data on ctdna in cholangiocarcinoma have been sparse . 
andersen and jakobsen20 have demonstrated the early feasibility of a ctdna assay in btc , using a multiplex digital pcr assay to screen for 31 mutations in kras , nras , braf , and pik3ca . 
the authors then performed the assay on serum from ve patients with btc with known tumor mutations and six patients who were known to be wild type for the assayed mutations . 
the assay correctly identied the ve known mutations , whereas none of the six wild - type samples had mutations identied in cfdna . goyal and colleagues21 demonstrated the usefulness of ctdna in serial monitoring of disease and for the detection of resistance mechanisms in the setting of targeted therapy . among 32 patients enrolled in a phase ii study of the fgfr inhibitor bgj398 , nine patients ( 28% ) had fgfr2 fusions detected and four patients were enrolled in the trial . 
pivotal trials exploring inhibitors of fgfr and idh in the management of btc specically are ongoing ( clinicaltrials.gov identiers : nct02924376 , nct03230318 , nct02052778 , and nct02989857 )  . other data have highlighted the application of erbb2 and braf targeted therapies in the disease.22 - 27 for these reasons , it is critically important to identify therapeutically relevant alterations in patients with cholangiocarcinoma . we demonstrate , for the rst time to our knowledge , the ability to detect a broad array of therapeutically relevant alterations using ctdna testing at a signicant rate ( 55% ) in patients with btc . 
whereas the oncokb system is an extensive , comprehensive , and curated precision oncology knowledge base that is capable of supporting precision oncology treatment decisions , should be noted that universally accepted denitions of actionable alterations are not currently available.8 more practically , a total of 21% of patients in our cohort were cohort ; fig 3 . 
 circulating tumor dna in biliary tract cancer identied as having actionable alterations in braf , erbb2 , fgfr2 , and idh1 , for which there are dedicated clinical trials available for patients with btc or for which currently available data exist on the treatment of patients with btc with existing targeted therapies . limitations , our study does have other including the moderate sample size , its retrospective nature , and the fact that patients are derived from a single institution . 
we also have limited clinical data as a result of the retrospective nature of the study . ctdna in btc has been an underexplored area , but our study for the rst time to our knowledge demonstrates the true feasibility of ctdna testing in this disease . 
we believe there is a rationale for ctdna to be incorporated in cholangiocarcinoma trials going forward so as to further explore the technology as a means for identifying patients with actionable genomic alterations , as a biomarker of response , and for serial monitoring of disease and detection of resistance mechanisms , as well as for prognostic purposes . 
borad manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors policy , please refer to or ascopubs.org / po / authorcenter . kabir mody consulting or advisory role : celgene , genentech , merrimack pharmaceuticals , eisai , astrazeneca , vicus therapeutics research funding : fibrogen , senhwa biosciences , ariad pharmaceuticals , tracon pharma , medimmune , agios , arqule , taiho pharmaceutical pashtoon m . 
kasi consulting or advisory role : taiho pharmaceutical ( inst ) , ipsen ( inst ) , bristol - myers squibb ( inst ) , advanced accelerator applications ( inst ) , array biopharma ( inst ) , celgene ( inst ) tanios bekaii - saab consulting or advisory role : amgen ( inst ) , glenmark , ipsen ( inst ) , eli lilly ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , bayer ( inst ) , celgene ( inst ) , genentech ( inst ) , abbvie , incyte ( inst ) , imugene , immuneering other relationship : exelixis , merck , sillajen , armo biosciences daniel h . 
ahn consulting or advisory role : celltrion ( i ) , merrimack pharmaceuticals , astellas pharma , eisai , cardinal health , paradigm , lexicon amit mahipal research funding : taiho pharmaceutical jason s . 
nat med 20 : 548 - 554 , 2014 sia d , hoshida y , villanueva a , et al : integrative molecular analysis of intrahepatic cholangiocarcinoma reveals 2 classes that have different outcomes . gastroenterology 144 : 829 - 840 , 2013 valle jw , lamarca a , goyal l , et al : new horizons for precision medicine in biliary tract cancers . 
shaib yh , davila ja , mcglynn k , et al : rising incidence of intrahepatic cholangiocarcinoma in the united states : a true increase ? j hepatol 40 : 472 - 477 , 2004 11 . 
chan - on w , kuwahara k , kobayashi n , et al : cholangiocarcinomas associated with long - term inammation express the activation - induced cytidine deaminase and germinal center - associated nuclear protein involved in immunoglobulin v - region diversication . 
j gastrointest oncol 7 : 797 - 803 , 2016 javle m , bekaii - saab t , jain a , et al : biliary cancer : utility of next - generation sequencing for clinical management . 
goyal l , saha sk , liu ly , et al : polyclonal secondary fgfr2 mutations drive acquired resistance to fgfr inhibition in patients with fgfr2 fusion - positive cholangiocarcinoma . 
j clin oncol 33 , 2017 ( suppl ; abstr e15137 ) javle m , churi c , kang hc , et al : her2 / neu - directed therapy for biliary tract cancer . 
kocsis j , aroksz all asi a , andr as c , et al : combined dabrafenib and trametinib treatment in a case of chemotherapy - refractory extrahepatic braf v600e mutant cholangiocarcinoma : dramatic clinical and radiological response with a confusing synchronic new liver lesion . 
loaiza - bonilla a , clayton e , furth e , et al : dramatic response to dabrafenib and trametinib combination in a braf v600e - mutated cholangiocarcinoma : implementation of a molecular tumour board and next - generation sequencing for personalized medicine . 
golan t , raitses - gurevich m , kelley rk , et al : overall survival and clinical characteristics of brca - associated cholangiocarcinoma : a multicenter retrospective a brief review . 
 circulating tumor dna predicts the response and prognosis in patients with early breast cancer receiving neoadjuvant chemotherapy shunying li , phd1 , 2 ; hongna lai , phd1 , 2 ; jieqiong liu , md1 , 2 ; yujie liu , phd1 , 2 ; liang jin , md1 , 2 ; yudong li , phd1 , 2 ; fengtao liu , md1 , 2 ; yuhua gong , ms3 ; yanfang guan , phd3 ; xin yi , phd3 ; qianfeng shi , md1 , 2 ; zijie cai , md1 , 2 ; qian li , md1 , 2 ; ying li , md1 ; mengdi zhu , md1 , 2 ; jingru wang , md1 , 2 ; yaping yang , md1 , 2 ; wei wei , md4 ; dong yin , phd1 , 2 ; erwei song , md , phd1 , 2 ; and qiang liu , md , phd1 , 2 purpose many patients with breast cancer still relapse after curative treatment . 
serial plasma samples before , during , and after nac and paired tumor biopsies were harvested and subjected to deep targeted sequencing using a large next - generation sequencing panel that covers 1 , 021 cancerrelated genes . results positive baseline ctdna was detected in 21 of 44 patients before nac . 
more importantly , positive baseline ctdna is signicantly associated with worse disease - free survival ( p = .011 ) and overall survival ( p = .004 ) in patients with early breast cancer , especially in estrogen receptornegative patients . conclusion our study demonstrated that ctdna can be used to predict tumor response to nac and prognosis in early breast cancer , providing information to tailor an individuals therapeutic regimen . jco precis oncol 4 : 244 - 257 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction breast cancer is the most commonly diagnosed cancer and the leading cause of cancer death in women worldwide.1 although early breast cancer is a curable disease , up to 40% of such patients still relapse after surgery.2 it is believed that breast cancer is a systemic disease and that clinically undetectable micrometastases often happened before the diagnosis.3 , 4 how to distinguish patients with early breast cancer with high relapse risk from those with low risk remains a critical and challenging clinical question . neoadjuvant chemotherapy ( nac ) is often used in patients with locally advanced or triple - negative / her2positive early breast cancer before surgery to decrease tumor size and enable breast - conserving surgery . 
the current consensus to monitor response to nac is clinical examination backed up by radiologic and sonographic measures.5 however , these measures are quite subjective and have poor interand intraobserver reproducibility.6 moreover , given the heterogeneity of cancer , a reliable method to examine the overall response from local , regional , and micrometastatic lesions in patients with early breast cancer is still lacking . circulating tumor dnas ( ctdnas ) are mutated gene fragments that are exclusively shed by cancer cells into blood , 7 which can be detected by digital polymerase chain reaction ( dpcr ) 8 or sequencing . 
 ctdna predicts prognosis in breast cancer context key objective can the presence and dynamic change of circulating tumor dna ( ctdna ) predict the tumor response and prognosis in patients with breast cancer receiving neoadjuvant chemotherapy ( nac ) ? knowledge generated using a next - generation sequencing panel of 1 , 021 genes , positive baseline ctdna was identied in 21 of 44 patients with early breast cancer before nac . 
positive ctdna before nac was associated with signicantly worse disease - free survival and overall survival , especially in estrogen receptor ( er ) negative patients . relevance our study demonstrates that ctdna has signicant value to complement imaging to monitor tumor response and predict prognosis in patients with early breast cancer , providing information to tailor an individuals therapeutic regimen . 
the high relapse rate in er - negative patients with positive ctdna indicates that it may be necessary to escalate treatment in these high - risk patients . patients with early breast cancer after surgery , ctdna by dpcr predicted metastasis at 7.9 - 11 months earlier than clinical relapse.11 , 12 a few studies also explored the role of ctdna in patients with breast cancer who received nac . 
it was reported that ctdna change during nac was correlated with tumor response13 - 15 or relapse , 16 , 17 although two of them only used dpcr to detect a single gene ( metrassf1a14 or tp5316 ) , and the other study only correlated the ctdna disappearance after the rst cycle of nac with two patients who achieved pathologic complete response.13 advances in next - generation sequencing ( ngs ) 18 technology have enabled the rapid identication and broad coverage of tumor - specic genomic alterations in cell - free dna ( cfdna ) of individual patients.19 - 21 the ngs assay provides an opportunity to screen more genes at a single time point and avoid missing mutations absent in biopsy because of intratumor heterogenicity . 
for patient cohort , sample collection and processing , and ngs sequencing and data analysis , please see the data supplement . statistical analysis the primary end point of this study was to evaluate the clinical value of the presence and dynamic change of ctdna to predict the tumor response and prognosis in patients with breast cancer treated with neoadjuvant chemotherapy . 
all statistical analyses were performed with graphpad prism version 6.0 or r version 3.4.1. results clinicopathological features of patients a total of 52 patients with early breast cancer who received nac were prospectively enrolled in the study since 2013 . eight patients were excluded from further study because of insufcient cfdna in plasma before nac ( fig 1 )  . the clinicopathological features of the 44 patients in the study are listed in table 1 and the data supplement . 
after surgery , the patients were followed up every 6 months . during the follow - up ( median , 46 months ; range , 11 - 68 months ) , 11 patients ( 25% ) had distant metastasis , and 9 of them died of metastatic breast cancer . baseline mutated dnas in plasma and tumor all baseline plasma samples , matched blood cells , and 32 paired tumor biopsy samples underwent parallel targeted ngs to screen for point mutations and structural variants , using the ngs panel of 1 , 021 cancer - related genes that covers a region of 1.1 mb ( data supplement ) .24 after deduplication , the median depths of unique coverage were 984 for primary tumor and 1 , 225 for plasma dna . 
the analysts were blinded to clinical and follow - up information during the analysis of sequencing data . among the 44 patients , 21 patients were found to have positive baseline ctdna . 
a total of 72 mutations in 46 genes were found in these 21 samples , with 1 - 8 ( median , 3 ) mutations per sample ( data supplement )  . 
tp53 ( 20 / 32 ) , pi3kca ( 13 / 32 ) , nf1 ( 5 / 32 ) , and gata3 ( 4 / 32 ) were the most frequently mutated genes in tumor ( fig 2c )  . in the 32 patients with both tumor and plasma sequencing data , 14 had concordant / partially concordant mutations in plasma and tumor , 16 patients had mutations only in tumor with negative ctdna , and the other two patients ( p034 and p036 ) had completely different mutations in tumor and plasma ( fig 2b )  . 
in the 16 patients with positive ctdna , 14 ( 87.5% ) of them had one or more mutations conrmed independently in tumor sequencing data , indicating that most positive ctdna represents tumor - specic mutations in the primary tumors . 
among the 33 concordant mutations found in both tumor and plasma of the 14 patients , tp53 ( 12 / 14 ) and pik3ca ( 4 / 14 ) mutations were the most frequent ( fig 2d )  . changes of ctdna and tumor response during nac the current gold standard to monitor tumor response during nac is ultrasound or magnetic resonance imaging , although it is subjective and sometimes falls behind the histologic changes . 
to explore whether ctdna surpasses imaging in monitoring or predicting overall tumor response , all plasma samples collected during nac in the 20 patients ( 1 patient was excluded because of insufcient cfdna in subsequent plasma samples ) with positive baseline ctdna were sequenced and compared with baseline data to track the dynamic changes of ctdna during nac ( data supplement )  . in this study , tumor response was dened as cr / pr / sd / pd using recist1.1 criteria when the imaging data of local / regional tumor before surgery was compared with that before nac . 
of the 20 assessable patients , 11 did not respond to nac ( including a patient with pd ) , and 9 responded to nac ( response rate , 45% )  . however , patient 038 ( p038 ) , who was dened as pr according to imaging , had an increasing ctdna amount ( clonal variant allele frequency [ vaf ] ) during all cycles of nac , 25 and a persisting high ctdna even after surgery , although she did not have any clinical metastasis before surgery . 
follow - up showed that she had multiple distant metastases ( liver , lung , and bone ) at 21 months and died at 46 months after surgery ( appendix fig a2 )  . 
the increase of ctdna in this case indicated the early micrometastases undetected by imaging did not respond to nac well , although the primary tumor did , suggesting that ctdna is better than imaging of local tumor to monitor the overall response to nac . next we did a longitudinal analysis of ctdna changes during nac and correlated it with local tumor response . p038 was excluded from this analysis because of discrepant tumor and ctdna data . 
the ctdna amount ( clonal vaf ) in baseline plasma was set as 100% , and those in subsequent plasma from the same patient were normalized it was found that patients who to the baseline value . responded to nac had more decreasing ctdna than patients who did not respond to nac ( fig 3a )  . 
the difference was signicant after the second cycle ( p = .03 ) and all cycles of nac ( p = .02 ) but was not statistically signicant after the rst cycle of nac ( p = .290 ; figs 3b - 3d )  . next , we constructed roc22 curves to compare the efcacy of ctdna amount ( clonal vaf ) and ultrasound to predict the response to nac ( fig 4 )  . 
it was found that clonal vaf after 2 cycles , clonal vaf before surgery , and ultrasound after 2 cycles were all predictive of the response to nac before surgery . 
the optimal criteria of clonal vaf in predicting the response to nac , as determined by the roc plots , are 40% drop in clonal vaf after 2 cycles and 60% drop in clonal vaf before surgery , respectively . 
the optimal criterion of ultrasound after 2 cycles was 20% decrease in the longest diameter of tumor in our study . concordant mutations between tumor and plasma were also identied in two patients with smaller tumor and negative lymph nodes ( t2n0m0 )  . 
the er - negative patients with negative baseline ctdna had 100% dfs and os , whereas those with positive baseline ctdna had a dfs / os of only approximately 36% . among the 20 patients with positive baseline ctdna ( one patient ruled out due to lack of subsequent samples ) , 6 of them turned negative and 14 remained positive for the ctdna before surgery . 
six out of 8 ( 75% ) er - negative patients with persistent positive ctdna relapsed , whereas only 1 out of 3 ( 33% ) such patients with negative ctdna before surgery relapsed , although the difference was not statistically signicant because of small sample size ( appendix figure a4 )  . discussion in this study , we used targeted deep sequencing of cfdna with a panel of 1 , 021 cancer - related genes to screen for mutated ctdna in patients with early breast cancer and found that 21 out of 44 patients had positive ctdna . 
more importantly , positive ctdna before nac is signicantly associated with worse prognosis in patients with early breast cancer , with the signicance mainly derived from er - negative patients . many patients with early breast cancer still relapse after surgery because of clinically undetectable micrometastases . 
current imaging methods are not sensitive enough to detect micrometastatic lesions ; even the most sensitive positron emission tomographycomputed tomography has the resolution limit at 4 mm.26 recently , ctdna has been suggested to be an ideal tumor biomarker because of its specicity , stability , and sensitivity . 
it is shown to be better than traditional biomarkers and imaging in predicting the relapse or progression in both early and metastatic cancer.9 , 11 , 12 , 27 - 29 however , the best method to measure ctdna is uncertadpcr is cheaper and easier , but it only measures one or few known mutations . 
to our knowledge , this study used the largest ngs panel so far to look for ctdna in patients with early breast cancer . using the large 1 , 021 - gene panel , somatic mutations were found in all the tumor biopsies . 
more importantly , positive ctdna was found in 47% of patients with early breast cancer and 73% of er - negative patients , which was consistent with previous reports.12 , 16 , 17 , 30 , 31 the majority of the ctdna was conrmed in tumor mutation data , suggesting that ctdna can be used to detect tumor - specic fig 2 . 
 ( c , d ) clonal vaf in no - response patients was signicantly higher than that in response patient after ( c ) 2 , and ( d ) all cycles of nac . 
in the 21 patients with positive baseline ctdna , 16 patients had paired plasma and tumor biopsy samples for ngs analysis , and 14 / 16 had at least one mutation conrmed in primary tumors . 
with the high specicity , at 98.72% , the discrepancy between the mutations in plasma and the mutations in tumor may be explained by the small tumor biopsy specimen not representing the whole primary tumor or micrometastasis . 
but this study also identied 24% ( 5 / 21 ) of patients with positive ctdna who had mutations other than tp53 and pi3kca . interestingly , our data showed that dynamic change of ctdna can be used to monitor and predict the response to nac in early breast cancer . 
kaplan - meier curve compares the disease - free survival ( dfs ) and overall survival ( os ) in patients with breast cancer with positive or negative baseline circulating tumor dna ( ctdna )  . 
nbc , negative baseline ctdna ; pbc , positive baseline ctdna . the change of ctdna level after 2 cycles of nac predicted local tumor response to nac better than ultrasound , although this was not statistically signicant . 
interestingly , none of the four er - negative patients with negative baseline ctdna relapsed during the follow - up , which was strikingly different from the high relapse rate in er - negative patients with positive baseline ctdna . 
other limitations of this study include limited sample size and suboptimal nac cycles , which hinder further subgroup analysis . in conclusion , our study demonstrates the feasibility and validity of ctdna in patients with early breast cancer receiving nac . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . yuhua gong employment : geneplus - beijing yanfang guan employment : geneplus - beijing xin yi employment : geneplus - beijing qiang liu consulting or advisory role : novartis , astrazeneca speakers bureau : pzer , roche , novartis , astrazeneca , eisai no other potential conicts of interest were reported . references bray f , ferlay j , soerjomataram i , et al : global cancer statistics 2018 : globocan estimates of incidence and mortality worldwide for 36 cancers in 185 countries . 
ca cancer j clin 68 : 394 - 424 , 2018 early breast cancer trialists collaborative group ( ebctcg ) , davies c , godwin j , et al : relevance of breast cancer hormone receptors and other factors to the efcacy of adjuvant tamoxifen : patient - level meta - analysis of randomised trials . 
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cancer res 72 : 5145 - 5149 , 2012 ; discussion 5150 schwarzenbach h , hoon ds , pantel k : cell - free nucleic acids as biomarkers in cancer patients . 
nat rev cancer 11 : 426 - 437 , 2011 bernard - tessier a , jeannot e , guenat d , et al : clinical validity of hpv circulating tumor dna in advanced anal carcinoma : an ancillary study to the epitopeshpv02 trial . 
clin cancer res25 : 2109 - 2115 , 2019 dawson sj , tsui dw , murtaza m , et al : analysis of circulating tumor dna to monitor metastatic breast cancer . 
schiavon g , hrebien s , garcia - murillas i , et al : analysis of esr1 mutation in circulating tumor dna demonstrates evolution during therapy for metastatic breast 11 . 
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robin x , turck n , hainard a , et al : proc : an open - source package for r and s + to analyze and compare roc curves . 
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 li et al et * 4 2 weeks after surgery no liver metastasis after surgery liver metastasis after 1 cycle b aselin e after 2 cycles b efore surg ery after 3 cycles after surg ery cycles 24 months fig a2 . 
et * 4 , 4 cycles of epirubicin and docetaxel . p031 ( t2n0m0 ) p041 ( t2n0m0 ) tuba3c tp53 raf1 pik3ca notch2 tsc2 tp53 gab2 dnmt3a brd3 fig a3 . 
although targeted therapies , including vandetanib and cabozantinib , are used to treat mtc , resistance ( both intrinsic and acquired ) to these therapeutic approaches warrants a need to better understand the broad - spectrum anomalies that govern this phenomenon , especially in patients with aggressive disease . 
using whole - exome sequencing ( wes ) and shallow whole - genome sequencing ( swgs ) of the primary tumor , adjacent normal bone marrow tissues , and blood , we identified three germline single nucleotide polymorphisms ( snps ) within the ret proto - oncogene that remained undetected using routine hospital genetic testing procedures . 
supported by findings from both wes and swgs , we report on the occurrence of a chromothripsis - like pattern in thyroid cancer , which involved shattering of chromosome 4 leading to complete abrogation of normal chromosomal function , along with dramatic widespread copy - number aberrations across both primary tumor and bone marrow samples . a 36 - year - old man with a body mass index ( bmi ) of 45 presented with a 4 - week history of chest pain , dyspnea , and 22 kg of unintentional weight loss ( overview of the patients clinical course is presented in the data supplement )  . 
the working diagnosis was carcinoma of unknown primary . a bone marrow biopsy was performed , and immunohistochemical ( ihc ) staining revealed round and polygonal malignant cells arranged in nests and cord - like patterns with round to oval nuclei containing coarse granular chromatin patterns adjacent to areas of extensive tumor necrosis ( fig 1a1 )  . focal staining was positive for calcitonin ( fig 1a2 ) , chromogranin ( data supplement ) , thyroid transcription factor 1 ( data supplement ) , and synaptophysin ( data supplement ) , but it was negative for cd45 ( data supplement )  . 
a diagnosis of mtc was established . these results led to a thyroid ultrasound , which showed a 4 - cm hypoechoic nodule at the lower pole of the left lobe and a 1.4 - cm hypervascular echogenic focus inferomedially to it ( fig 1b )  . 
ihc of the primary tumor revealed pleomorphic polygonal and ascopubs.org / journal / po jco precision oncology sudipto das deirdre kelly bruce moran kathleen han niall mulligan ciara barrett patrick g . 
radiologic detection of primary tumor and immunohistochemical analysis of primary thyroid and bone marrow sample . ( a ) bone marrow biopsy sample stained with ( 1 ) hematoxylin and eosin staining showed infiltration of the marrow space by a proliferation of pleomorphic round to oval cells with scant eosinophilic cytoplasm and inconspicuous nucleoli . 
 ( 2 ) positive staining of the bone marrow biopsy observed for calciton ( b ) thyroid ultrasound shows a 1.4 - cm hyperechoic nodule at the lower pole of the left lobe of thyroid ( as indicated by the red arrow ) , suggestive of a primary thyroid malignancy . 
 ( d ) primary tumor sample stained with ( 1 ) hematoxylin and eosin shows that the primary tumor consisted primarily of pleomorphic polygonal and spindle cells arranged in nests separated by fibrous strand . 
serum calcitonin was 5 , 000 ng / l ( normal range , , 10 ng / l ) , and carcinoembryonic antigen was 200 mg / l ( normal range , , 5 mg / l )  . routine germline ret mutation testing in exons 10 , 11 , 13 , 14 , and 16 was negative . 
the patient died on day 31 from multiorgan failure . postmortem examination showed metastatic mtc , with complete replacement of the left lobe of the thyroid involving para - esophageal tracheal lymph nodes and the pleural surface of both lungs extending into the parenchyma . 
after receiving written informed consent from the patients family for research activities to be carried out postmortem , dna extracted from the primary tumor , adjacent normal bone marrow tissue , and blood was used to carry out wes and swgs ( data supplement )  . results chromothripsis - like pattern in genomic data . we revealed a dramatic landscape , concordant between wes and swgs ( fig 2a ) , of wideranging copy - number aberrations ( cnas ) across the primary tumor , two distinct regions of bone marrow , which showed clear tumor cell infiltration ( bm - mets1 , bm - mets2 ) , and adjacent normal tissue . 
by using the blood sample as a baseline , losses ranging from regions of several megabases to entire chromosomes were evident across all tumor samples ( fig 2a ; data supplement ) with a single gain occurring on the q arm of chromosome 1 . 
genome - wide copy - number aberrations and identification of chromothripsis - like pattern across adjacent normal tissue , blood , primary tumor , and bone marrow samples showing somatic mutations from whole - exome sequencing ( wes )  . 
 ( a ) absolute copy - number aberrations ( y - axis : 1 , loss ; 3 , gain ) across chromosomes 1 to 21 ( x - axis , denoted by blue lines , centromere denoted by dashed pink line ) compared by using data from wes and shallow wholegenome sequencing across all sample types . 
 ( b ) the copy - number aberration profile for chromosome 4 across the all samples demonstrating the chromothripsis - like pattern event generated for a 30 - kb bin using the wes data . 
ctlp is a catastrophic event involving tens to hundreds of chromosomal rearrangements up to the whole - chromosome level , which can contribute to development of a highly unstable and aggressive disease.1 - 7 the ctlp observed in this patient led to generation of approximately 30 to 40 segments with a typical oscillation of cna between two states ( loss and normal copy number ) .7 although we did carry out genomic analysis of the other metastatic lesions , including the para - esophageal , para - tracheal , and lung metastases , they were not included in the detailed genomic assessment described in this study because of unacceptable sequencing data quality . germline mutations in ret and somatic mutations in disease - associated genes . 
germline mutation analysis using wes from blood and adjacent normal tissue did not reveal any ret variants that are currently used diagnostically ( confirming the posthumous germline ret mutation profiling )  . 
however , we identified three annotated snps within ret ( rs1800861 , rs2742241 , and rs2742243 ) that were fixed with a mutant allele frequency of 1 across all samples including blood and normal tissue . we were able to validate these orthogonally across all samples by using sanger sequencing ( data supplement )  . 
the rs1800861 ( l769l , exon 13 leuctt / leuctg ) variant has previously been reported as a predisposing factor for development of aggressive mtc.8 , 9 of the other two mutations , rs2742243 ( c / t variant ) has been associated with papillary thyroid carcinoma10 and rs2742241 ( g / a variant ) has not been shown to be associated with thyroid cancer . furthermore , our somatic mutational analysis identified 109 somatic mutations , 70% of which occurred in only one of the samples ( fig 2c ; data supplement )  . 
among the nonsynonymous variants of note in disease - associated are missense mutations genes , including gse1 , cldn12 , and trim28 , which have been previously implicated as playing a role in disease processes such as metastasis , migration , and proliferation across various cancer types11 - 15 and may have had a role as potential drivers of disease progression in this patient . 
the differences in mutational patterns between the two bone marrow samples suggest marked genetic heterogeneity between tumor deposits in the same tissue . discussion the patients high bmi made palpation of a neck mass impossible , and the lack of an abnormality on routine imaging in addition to the development of dic and deteriorating respiratory status made this an extremely difficult clinical and diagnostic case . 
remarkably , it was the analysis of the bone marrow that led to the diagnosis of mtc , which further exemplified the severity of the disease in this patient showing complete infiltration of the bone marrow , potentially contributing to a total bone marrow collapse and resulting in development of dic.16 , 17 posthumously , routine clinical germline ret mutation testing did not identify any mutations within this gene . we sought to determine why this young man developed such an aggressive mtc and if it could be explained by the interplay of genomic events . our results support the hypothesis of a catastrophic event such as the evident ctlp , along with widespread copy - number alterations that may be regarded as contributing factors toward the observed phenotype.4 , 5 , 18 although ctlp has been detected in 2% to 3% of all cancers , 1 , 3 , 7 , 19 - 21 to the best of our knowledge , this is the first report to demonstrate ctlp in any form of thyroid cancer . in addition to de novo events that have an impact on cancer phenotype , known genetic alterations can often predispose patients to aggressive disease development . 
variants in the ret protooncogene are commonly associated with mtc and are used as a primary diagnostic test to identify familial and sporadic cases.22 - 25 these tests encompass well - established hot spots within ret and have largely been proven effective in detecting patients with conventional mtc . 
however , unusual patients such as this one require detailed analysis of such genes with the intent of identifying rare mutations that might either explain the atypical phenotype or allow it to be molecularly diagnosed . 
the germline ret l769l variant , previously associated with increased risk of aggressive mtc , 8 , 10 , 22 as well as the other two mutations discovered here , which have not previously been reported in mtc , could have an additive effect on increased risk of development of an aggressive phenotype . 
 ret snps were shown to have increased risk for lymph node and distant metastases at diagnosis ( odds ratio , 5.84 ) and also for developing metastases earlier.8 importantly , our results exemplify how the inclusion of more variants in clinical assays may be of use , especially in diagnostically challenging patients . although identification of mutations in individual disease - associated loci , as observed through the somatic mutation analysis , allows us to generate an appropriate hypothesis surrounding the events that could have led to the development of metastasis , the genetic heterogeneity observed across all resection samples of this patient underpin why , in the clinical setting , targeting specific mutational events therapeutically is rarely effective . 
however , it is also important to note that the study reported here describes a single patient with a rare and atypical mtc . multifactorial genomic events , including germline and somatic mutations in functionally important genes together with widespread cna ( including ctlp ) supports the need for pragmatic treatment approaches using combinations of targeted agents and possibly even immunotherapeutic approaches.26 - 28 within the context of this study and in patients who have disease of a similar nature , it is tempting to speculate that the presence of ctlp would likely lead to generation of multiple neoantigens , suggesting a potential benefit of immunotherapy.26 however , it is noteworthy that such immunotherapeutic strategies to date have not been used for patients with mtc . 
although mutational load may be inferred from routine panel - based genetic testing when only a few hot spot mutations are screened , such as in mtc , it is unlikely that candidates for immunotherapy will be identified , suggesting that a deeper examination of the genome may provide better diagnostic and therapeutic information . in conclusion , our results provide a critical insight into potential drivers of an aggressive phenotype of mtc and , in parallel , present a vital opportunity to identify effective therapeutic strategies based on the evident abnormalities in a given patient . 
kelly collection and assembly of data : sudipto das , deirdre kelly , bruce moran , kathleen han , niall mulligan , ciara barrett , peter mcmahon , hendrik f . 
relationships are self - held unless noted . deirdre kelly no relationship to disclose bruce moran no relationship to disclose kathleen han no relationship to disclose niall mulligan no relationship to disclose ciara barrett no relationship to disclose patrick g . 
van essen no relationship to disclose kate connor no relationship to disclose diether lambrechts no relationship to disclose bauke ylstra no relationship to disclose consulting or advisory role : carrick therapeutics research funding : carrick therapeutics travel , accommodations , expenses : oncomark darran p . 
gallagher employment : oncomark leadership : oncomark stock and other ownership interests : oncomark acknowledgment we thank lisa dwane , brian mooney , and camille hurley for their technical assistance on the study and the family of the patient for consenting to the study . affiliations sudipto das , deirdre kelly , bruce moran , kathleen han , niall mulligan , ciara barrett , peter mcmahon , john mccaffrey , kate connor , william m . 
oconnor , royal college of surgeons in ireland ; deirdre kelly , kathleen han , niall mulligan , ciara barrett , peter mcmahon , john mccaffrey , and catherine m . 
van essen and bauke ylstra , vrije universiteit medical center , amsterdam , the netherlands ; and diether lambrechts , vesailus research center , vlaams instituut voor biotechnologie , katholieke universiteit , leuven , belgium . supported by funding from the mater foundation , by postdoctoral fellowship crf13das from the irish cancer society ( s.d. ) , by grant no . 
cai h , kumar n , bagheri hc , et al : chromothripsis - like patterns are recurring but heterogeneously distributed features in a survey of 22 , 347 cancer genome screens . 
sromek m , czetwerty nska m , skasko e , et al : the frequency of selected polymorphic variants of the ret gene in patients with medullary thyroid carcinoma and in the general population of central poland . 
liao s , song w , liu y , et al : familial multinodular goiter syndrome with papillary thyroid carcinomas : mutational analysis of the associated genes in 5 cases from 1 chinese family . 
wei c , cheng j , zhou b , et al : tripartite motif containing 28 ( trim28 ) promotes breast cancer metastasis by stabilizing twist1 protesci rep 6 : 29822 , 2016 15 . 
yang y , cheon s , jung mk , et al : interleukin - 18 enhances breast cancer cell migration via down - regulation of claudin - 12 and induction of the p38 mapk pathway . 
forment jv , kaidi a , jackson sp : chromothripsis and cancer : causes and consequences of chromosome shattering . j gen intern med 21 : c6 - c8 , 2006 study . 
ye l , santarpia l , cote gj , et al : high resolution array - comparative genomic hybridization profiling reveals deoxyribonucleic acid copy number alterations associated with medullary thyroid carcinoma . 
 parental perspectives on whole - exome sequencing in pediatric cancer : a typology of perceived utility purpose to explore how parents of pediatric patients with cancer perceived the utility of clinical tumor and germline whole - exome sequencing ( wes ) results . patients and methods we conducted longitudinal interviews with parents of a diverse pediatric cancer population before disclosure of wes results ( n = 64 ) , then 1 to 8 months ( n = 33 ) after disclosure . 
2017 by american society of clinical oncology introduction genomic sequencing ( gs ) technologies including whole - exome sequencing ( wes ) and wholegenome sequencing are increasingly being used in cancer clinical research and care.1 - 5 these technologies are typically valued for their potential to allow evidence - based changes to patients treatment . 
this is particularly true in the context of pediatric practice , in which ethical reservations about the impact of gs information have limited its use in generating direct clinical benefits.6 however , recent policy and position statements have criticized these narrow definitions of utility and argue that testing and disclosure provide value for families and society in addition to individual patients and may be appropriate in a wider set of cases.7 - 10 many have argued for a more comprehensive and empirically informed understanding of the utility of gs and have urged that perspectives of individuals receiving sequencing results should be incorporated into the development of clinical practice and coverage guidelines.11 - 14 the hypothetical interest of parents in receiving gs results for their children with conditions other than cancer has been reported.15 - 17 two studies have described the perceptions of parents of children with rare diseases18 and autism spectrum disorders19 regarding gs ; these parents found the information useful for reproductive and financial planning19 as well as for finding a conclusive diagnosis and helping with the coping process.18 recent studies have found that adults undergoing sequencing reported finding value in increased self - awareness , 20 , 21 satisfaction of curiosity , 20 legitimation of their condition , 21 and support from others.21 to the best of our knowledge , no research has evaluated how parents of pediatric patients with cancer who have received their childs gs results conceptualize the utility of the information . 
the basic3 study enrolled 287 pediatric patients ; the consent process and reporting components of the trial as well as the initial germline and tumor exome results have been described.22 , 23 the study includes providing clinical wes of blood samples for all patients and tumor samples when available ( 80% of patients enrolled ) ; results were reported in the medical record . 
the study was approved by the institutional review board of baylor college of medicine . tumor and germline wes results were disclosed to parents by the patients primary oncologist and a study genetic counselor . 
it was explicitly stated in both the informed consent document and consent session that it was unlikely that wes information would provide immediate clinical benefit to patients in terms of current treatment and that the tumor wes results in particular might be more clinically useful if the tumor recurred . 
parents were given a copy of their childs wes report ( s ) in addition to a counseling letter summarizing findings from the germline wes report in lay language . we conducted semistructured interviews with one parent of basic3 study patients in either english or spanish as preferred by the parent . 
to ensure that we would have sufficient participation throughout the longitudinal project , we oversampled for predisclosure interviews ( n = 64 )  . these were conducted with parents after consent and enrollment in the study but before disclosure of wes results ( predisclosure )  . 
interviews lasted an average of 50 minutes and were conducted at a time and location convenient for the parent , most frequently at the time of one of their childs clinical appointments . 
all potentially identifying information was removed , and parents were referred to only by their study identification number , noted in brackets after each quotation . we calculated descriptive statistics for parents demographic characteristics , evaluating differences between interview participants and overall study participants sex and race / ethnicity by using x2 tests . 
all p values were two - sided and with statistical significance set at p , .05. results our study enrolled a highly diverse set of families . demographic information from all parents who completed predisclosure interviews are provided in table 1 . 
 families enrolled in basic3 study ( n = 287 ) not interviewed for predisclosure enrolled after predisclosure goal met scheduling conflicts , unable to be contacted , and / or disclosed before predisclosure interview ineligible due to tumor unavailability declined predisclosure interview withdrawal ( n = 223 ) ( n = 102 ) ( n = 80 ) ( n = 35 ) ( n = 1 ) ( n = 5 ) completed predisclosure interview ( n = 64 ) not disclosed scheduling conflicts and / or unable to be contacted ( n = 3 ) ( n = 3 ) received wes results disclosure ( n = 61 ) not interviewed for postdisclosure scheduling conflicts and / or unable to be contacted patient death before postdisclosure interview declined postdisclosure interview ( n = 28 ) ( n = 19 ) ( n = 8 ) ( n = 1 ) completed postdisclosure interview ( n = 33 ) fig 1 . 
representative quotes illustrating each dimension are included in table 3 . although the focus of this article is the range of ways in which parents found participation in the basic3 study valuable , it is worth noting that parents described few concerns about having gs information . clinical utility parents were informed as part of the consent process that participation in the study was highly unlikely to change their childs treatment plan . even so , in predisclosure interviews some parents expressed hope that their childrens wes results might provide clinical benefits for their children either in the short term or in the future , including tailored treatments and information about the need for additional genetic testing or surveillance . as expected , only a minority ( 33% of those interviewed postdisclosure ) of tumor reports included somatic mutations categorized by the laboratory as being of proven or potential clinical relevance.23 even when such a mutation was found , the information was not used immediately because the child was undergoing standard treatment . 
however , some parents , including both those whose child was found to have a tumor mutation and those who received a negative report , believed that it could be used to personalize treatment in the future if the tumor returned . before and after disclosure , parents were clear that germline genomic information was valuable not only for their child with cancer . 
they hoped that the tumor or germline wes reports would offer an answer to a question bothering them . of the 33 families interviewed postdisclosure , only 11 had received information identifying a potentially clinically relevant mutation in the childs tumor , and one had received information about a cancer - related germline mutation . that most parents did not get information explaining their childs cancer caused disappointment among some participants whereas others were grateful for any findings that were returned . some parents looking to explain their childs cancer articulated in predisclosure interviews that they hoped the results would offer exculpatory information . 
they felt that a better understanding of the cancers source would remove the guilt associated with worrying that they had passed the disease on or that they had done something to cause it . 
relief from guilt associated with the possibility of passing on a cancer gene was also identified by parents as a source of utility after receiving genomic information about tumor mutations . there were parents who stated that the information offered them peace of mind after they had received a negative result . 
all demographics were self - reported at the time of enrollment in the larger basic3 study . abbreviation : na , not applicable . * non - hispanic or latino , other category includes asian ( 4 ) , black or african american ( 8 ) , two or more races ( 2 ) , declined or na ( 9 )  . participation in the basic3 study . 
interestingly , many parents discussed the psychological impact of genomic information on themselves rather than on the patient or other family members . one of the strongest themes emerging from our analysis was that parents felt the need to know why table 2 . 
parents descriptions of utility of tumor and germline wes before ( pre ) or after ( post ) disclosure findings patient id post post medically actionable finding post tumor mutation finding description clinical utility tailored treatment of patient thats what my hope is , is that of course any genetic information that they find would be helpful to do that , just to find what would be the most effective therapy for him . but , if for some reason , ( knocks on table ) [ the tumor ] came back , they could use that basic3 study and figure out from the genetics of his tumor what to do , and he would essentially have his own regimen and treatment plan or whatever . additional testing for patient it will just help us in the future with her , and itll help me in the future if i decide to have another baby . 
so we know what to look for , we know the signs , we know what to do with her to help prevent things returning or prevent more disease and illness . testing or surveillance for others it showed us some of the mutations that we really need to look at their possible representation and thats what we did . 
we dont know when its going to show so we will keep informing next generations and making sure that they check this . i really wanted to know if it was genetic , just for the fact if i needed to get my daughter [ the patients sibling ] testedbut when they said that it wasnt , then that made me reallythat i didnt need to get her a whole body scanned for anything . ( laughs ) so that was my real reason for doing it is to make sure she didnt need to be checked . psychological utility understanding cause of cancer they possibly could figure out why this happens too . 
parents descriptions of utility of tumor and germline wes ( continued ) description before ( pre ) or after ( post ) disclosure post findings patient id of course , the study doesnt point out what caused it exactly or why that was . 
yeah , that was the only disappointment , but otherwise i guess whatever the information we have so far is not bad . curiosity i want to know everything there is to know about [ child ] and us . 
it really justits just really interesting to find out these things relief from guilt how did it develop ? i dont know like , is it that something that we carried ? is it something i did while i was pregnant ? what caused it ? mainly thats what we want to know . as long as theres nothing that we did that caused itor nothing that we couldve possibly ever have done to cause iti suppose that [ would be ] a relief . you know it was a relief to know that its just something that his body just grew on its own and didnti didnt pass downso justi dont know , just a reliefsomething off your shoulders . peace of mind i guess peace of mind at some level for her thatyou knowtheres not an inherited mutation . 
parents descriptions of utility of tumor and germline wes ( continued ) before ( pre ) or after ( post ) disclosure findings patient id post post post description pragmatic utility reproductive considerations she also has a gene that if her future partner has the same kind ofif they carry the same kind of gene together , their kids mightwell , well tell her when she grow up . 
she might go to the doctors to find out whats going on . so now its like , if we ever do plan on having more children , its kind of like , we have to go get our genetics testing done first before we even think about having a baby , and then while imwhenever i do get pregnantthen we have to get the genetic testing while the babys still inside of me . 
so its likeits a lot to think about . future planning butfor me , the benefits are just like mainly her future stuff and knowing that we could have another child that has cancer...id rather know than not know and it just pop up and surprise us like it did with her . 
if i know its coming , you cani can better handle myself like , okay , thats fine , well be prepared , well handle it just like we handled this one , except now we know what to expect . abbreviations : id , identification ( number ) ; nf , no medically actionable , cancer - related , or tumor mutation findings ; wes , whole - exome sequencing . finally , several parents identified the value of being able to plan for the future and the possibility of additional health problems . 
although few of the parents in our postdisclosure cohort ( three [ 9% ] of 33 ) received results indicating that their family was at increased genetic risk for other cancers or diseases , many reported being grateful for any information that could prevent them from being surprised by a similar occurrence again , consistent with results in the predisclosure interviews.25 discussion the results of this qualitative analysis demonstrate that parents perception of the value of wes information in the context of childhood cancer extends well beyond a narrow definition of clinical utility focused on diagnosis , prognosis , and therapeutic management . 
our diverse cohort of parents described other dimensions of utility , including the psychological and pragmatic value of having this information . existing literature typically classifies any utility that is not grounded in a change of medical management as personal utility . 
 clinical decision making at the time of the disclosure was found in our analysis and in other work.21 with respect to psychological utility , our results mirror those suggesting that parents and patients place enormous value on establishing a causal explanation for a disease or condition.19 , 21 similarly , our data support a finding that parents of children with serious diseases seek confirmation that the disease was not the fault of the parents.18 as other studies have shown , 19 , 20 our participants reported that having genomic information may be valuable in and of itself , even if it does not lead to any significant changes in their lives or experiences . 
the possibility that this information could have an impact on reproductive decision making was identified as important for many parents in other contexts as well.19 available literature on pediatric gs has not described the extent to which utility for individuals other than the patient is considered by those making decisions about wes , although this is clearly a theme in adult contexts . 
finally , our study has described parents perceptions in the unique context of decision making about wes in pediatric cancer . the experiences and perspectives of the parents interviewed offer evidence to buttress emerging critiques of a narrow view of utility . 
our data support the view of botkin et al13 that , softer outcomes , such as psychological impacts , behavior changes , and social impacts , are particularly important in the assessment of many genetic tests and illustrate the importance of recognizing a wide range of utility . 
the finding that parents of pediatric patients with cancer perceive the value of genomic information so broadly has several significant ethical implications for whether and how wes is integrated into clinical practice . first , a few of the responses given by parents suggest that their perceived value of wes information may be disproportionate to its clinical implications . 
despite being told that it was unlikely that the wes results would change or improve their childs medical care in the short term , many parents still cited hopes of tailored treatment . 
in addition , the peace of mind that parents described having after getting a negative germline report may reflect an overestimation of the familys risk reduction estimate , even though the disclosure and counseling letter notes that wes does not identify all cancer susceptibility findings . although it is not novel to note concerns about the accuracy of decision makers understanding of complex genomic data , the question of how to ethically account for parents possibly exaggerated perceptions of the utility of a negative report ( there are no reliable data on how exaggerated this might be ) seems particularly salient in the context of pediatric cancer . second , the data demonstrate that parents put significant weight on the perceived benefits of wes information for themselves , their other children , and other family members . 
the nature of genetic and genomic technologies is that they have implications for individuals beyond the index patient , an aspect that parents seemed acutely aware of and that shaped their experience with wes . this finding raises questions about the degree to which utility for nonpatients should have an impact on sequencing recommendations , health care coverage , and disclosures . third , it is uncertain which of these varied types of utility should be used to justify a recommendation for genomic sequencing of a patient and his or her family . 
although it is clear that clinical utility could justify the use of this technology by thirdparty payers , it has not been generally accepted that the possibility of finding psychological or pragmatic utility offer the same grounding for a testing recommendation . 
consideration should be given to whether these types of utility are sufficient justification for wes or whether they ought to be given second - tier status . finally , the insights offered by this study raise questions about the nature of the informed consent process in the clinical and research settings for gs that is used with parents of children with serious diseases . 
current practice is to identify and clearly communicate possible psychological and social risks ( such as anxiety or loss of insurance ) , but corresponding possible benefits ( such as peace of mind or reproductive planning ) are not typically discussed ; instead , the focus is usually on narrow definitions of potential medical benefits . 
our results suggest that this differential treatment of the different types of risks and benefit may not be coherent and that both may be of great importance to decision makers . 
 experience , which suggests that additional work is required to ensure that all of the appropriate risks and benefits are discussed with parents who are consenting to genomic trials or testing . our study had several limitations . 
first , this interview - based analysis used open - ended questions and so was not designed to assess the prevalenceofvariousperspectiveson genomic information . accurate characterization of the frequency of various responses would require a methodology that included greater numbers of participants and more discrete response options . 
second , because parents understanding of their childs wes results was not directly evaluated , we were not able to characterize parents comprehension of the information they were given at disclosure or the degree to which their understanding of utility was shaped by various elements of the study ( ie , the consent process , education and counseling , and the information contained in the tumor and germline reports )  . finally , because our study was conducted with parents of pediatric patients with cancer , our findings might be limited to this population and may not be generalizable to other pediatric patient populations . longitudinal interviews with a diverse cohort of parents of pediatric patients with cancer identified a broad range of anticipated and experienced utility through the integration of wes into their childrens medical care . 
parents cited possible clinical utility for the patient , themselves , and for their other family members , and also described psychological and pragmatic benefits for these parties as well . 
mcguire no relationship to disclose acknowledgments the authors thank robin raesz - martinez , study coordinator , sarah scollon and katie bergstrom , study genetic counselors , and uma ramamurthy and her team at the baylor college of medicine institute for clinical and translational research and especially thank the oncologists and parents who participated in this study . janet malek , jill o . 
worthey ea , mayer an , syverson gd , et al : making a definitive diagnosis : successful clinical application of whole exome sequencing in a child with intractable inflammatory bowel disease . 
yang y , muzny dm , reid jg , et al : clinical whole - exome sequencing for the diagnosis of mendelian disorders . n engl j med 369 : 1502 - 1511 , 2013 4 . 
american college of medical genetics and genomics ( acmg ) board of directors : clinical utility of genetic and genomic services : a position statement of the american college of medical genetics and genomics . 
botkin jr , belmont jw , berg js , et al : points to consider : ethical , legal , and psychosocial implications of genetic testing in children and adolescents . 
waisbren se , back dk , liu c , et al : parents are interested in newborn genomic testing during the early postpartum genomics 18 : 151 - 159 , 2015 period . 
mccullough lb , slashinski mj , mcguire al , et al : is whole - exome sequencing an ethically disruptive technology ? perspectives of pediatric oncologists and parents of pediatric patients with solid tumors . 
to inform targeted treatment strategies , 3 , 476 clinically advanced prostate tumors were analyzed by cgp for genomic alterations ( gas ) and signatures of genomic instability . methods prostate cancer samples ( 1 , 660 primary site and 1 , 816 metastatic site tumors from unmatched patients ) were prospectively analyzed by cgp ( foundationone assay ; foundation medicine , cambridge , ma ) for gas and genomic signatures ( genome - wide loss of heterozygosity [ gloh ] , microsatellite instability [ msi ] status , tumor mutational burden [ tmb ] )  . results frequently altered genes were tp53 ( 44% ) , pten ( 32% ) , tmprss2 - erg ( 31% ) , and ar ( 23% )  . 
potentially targetable gas were frequently identied in dna repair , phosphatidylinositol 3 - kinase , and ras / raf / mek pathways . dna repair pathway gas included homologous recombination repair ( 23% ) , fanconi anemia ( 5% ) , cdk12 ( 6% ) , and mismatch repair ( 4% ) gas . 
metastatic site tumors were enriched for the 11q13 amplicon ( ccnd1 / fgf19 / fgf4 / fgf3 ) and gas in ar , lyn , myc , ncor1 , pik3cb , and rb1 compared with primary tumors . conclusion routine clinical cgp in the real - world setting identied gas that are investigational biomarkers for targeted therapies in 57% of cases . 
2019 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction genomic alterations ( gas ) that drive prostate cancer have been elucidated by proling primary tumors.1 , 2 comprehensive genomic proling ( cgp ) is increasingly used for routine clinical management of patients with prostate cancer , 3 with accumulating evidence associating gas with responses to therapy . 
 chung et al context key objective in this study , we use real - world data from routine prospective clinical genomic proling to evaluate genomic alterations ( gas ) and genomic signatures in primary and metastatic prostate cancer . knowledge generated we evaluated the landscape of gas in prostate cancer and identied those that are enriched in metastatic site tumors . approximately 3% of cases had high microsatellite instability and / or high tumor mutational burden status . 
genomic signatures , including microsatellite instability , tumor mutational burden , and genome - wide loss of heterozygosity , may further rene biomarker development for poly ( adp - ribose ) polymerase inhibitors and immunotherapies . samples using a validated assay16 ( foundationone ; foundation medicine , cambridge , ma ; appendix table a1 )  . 
the pathologic diagnosis of each case was conrmed on routine hematoxylin and eosinstained slides . results were analyzed for gas and gene signatures ( tmb , msi , genome - wide loss of heterozygosity [ gloh ] )  . 
germline / somatic mutation calls were predicted without a matched normal ; in validation testing of 480 tumor - only sequencing calls against matched normal samples , accuracy was 95% for somatic and 99% for germline calls.17 enrichment was dened as the difference in ga frequency between metastatic and primary sites . 
activating braf or raf1 fusions / rearrangements were observed in 1.2% of cases ( 35 braf and seven raf1 ; appendix fig a2 )  . the pi3k / akt / mammalian target of rapamycin ( mtor ) pathway was frequently altered ( 40.8% ; figs 1b and 1c )  . as expected , pten gas were frequent , and we observed in pik3ca , activating mutations and amplications pik3cb , akt1 / 2 / 3 , mtor , and rictor and loss - offunction alterations in pik3r1 / 2 and tsc1 / 2 . 
ras / raf / mek pathway alterations ( 5.7% ; figs 1b and 1f ) included oncogenic braf mutations ( appendix fig a2 ) , braf / raf1 rearrangements , activating mutations in raf1 / araf , kras / nras / hras and map2k1 / 2 , and nf1 loss - of - function alterations . 
 chung et al cdk12 ga ( p , .001 ) , and braf rearrangements / mutations ( p , .001 ; fig 1b )  . to compare primary and metastatic site tumors , we assessed relative enrichment in gas ( fig 1g ; appendix table a3 )  . 
predicted germline mutations were identied in 57.8% of brca2 - , 25.0% of brca1 - , 35.8% of atm - , 80.0% of chek2 - , 52.2% of fanca - , 42.3% of msh2 - , 20.0% of msh6 - , 25.0% of mlh1 - , and 44.4% of pms2 - mutated cases ; only 9.2% of cdk12 - mutated cases harbored a predicted germline mutation ( fig 2c )  . genomic signatures : gloh in addition to gas in individual dna repair genes , genomic signatures represent the phenotypic readout of deleterious dna repair and are potential predictive biomarkers . 
we evaluated the association between gloh and dna repair gas ( fig 2d )  . consistent with the established relationship between brca1 / 2 and hrd , 21 brca1 / 2 - altered cases ( both predicted germline and somatic mutations ) were more frequently gloh - h compared with the overall data set ( fig 2d )  . to evaluate the potential relevance of non - brca1 / 2 dna repair genes as biomarkers for parp inhibition , we assessed their association with gloh . 
gloh - h frequency was comparable between the overall data set and cases with non - brca1 / 2 dna repair gas , although cases with homozygous deletions in non - brca1 / 2 hrr pathway or fa / icl pathway genes were more frequently gloh - h ( appendix fig a4b )  . 
 ( b ) frequency of major pathway alterations , including ets fusions , braf rearrangements / mutations , spop / cul3 mutations , cdk12 gas , idh1 / 2 mutations , ar gas , phosphatidylinositol 3 - kinase ( pi3k ) pathway gas , homologous recombination gas , g1 / s - cell cycle gas , wnt pathway gas , fanconi anemia / interstrand crosslink repair ( fa / icl ) repair pathway gas , ras / raf / mek pathway gas ( other than braf ) , mismatch repair gas , and pole mutations ( see figs 1c to 1f for details )  . 
 ( c to f ) gas identied in each pathway , including the ( c ) pi3k / akt / mammalian target of rapamycin ( mtor ) pathway , ( d ) g1 / s - cell cycle pathway , ( e ) wnt pathway , and ( f ) ras / raf / mek pathway ( nf1 mutation , rearrangement , or copy number loss ; braf or raf1 mutations or rearrangements ; araf , k / n / h - ras , or map2k1 / 2 mutations were included ) ; percent of altered cases is indicated . 
genes that were enriched ( difference between primary site v metastatic site frequency ) by at least 2% are indicated ( all p , .05 by fishers exact test [ two - tailed ] ) , with genes enriched at least twofold indicated in red ( all p , .001 by fishers exact test [ two - tailed ] )  . 
msi status was assessable for 3 , 326 cases , and overall , 87 of 3 , 326 of cases ( 2.6% ) were msi - h ( 2.0% primary site , 3.1% metastatic site tumors )  . 
for the remaining cases , tmb - h phenotype was not attributed to msi - h or pole . landscape of ets fusions and ar gas in total , 1 , 236 ets fusions were detected ( one sample harbored two ets fusions ; fig 1b )  . 
tmprss2 - erg comprised the majority ( 87.7% ) of ets fusions ( fig 3a ) , with the remaining consisting of etv1 ( 8.5% ) , etv4 ( 2.6% ) , and etv5 ( 1.2% ) with diverse fusion partners , including several not previously described ( fig 3b )  . 
we also identied breakpoints that juxtaposed tmprss2 with the intergenic region upstream of erg ( 0.1 to 75 kb upstream ; fig 3c ) ; similar upstream intergenic breakpoints were observed for tmprss2 fusions with etv4 ( 10 of 32 cases ) and etv5 ( two of 15 cases )  . ar gas are associated with castration - resistant disease and were most enriched in metastatic site tumors ( 39.7% of metastatic site and 3.7% of primary site tumors ; fig 1g )  . 
five hundred fty - ve of 557 cnas were amplications ( median copy number , 24 ; range , six to 366 ) ; two homozygous deletions that encompass exons 5 to 7 or exons 5 to 8 are likely activating.27 ar missense mutations were observed in 6.9% of cases ( 1.3% primary site and 11.9% metastatic site ) , and most were ligandbinding domain antiandrogen resistance mutations ( fig 4b ) .28 finally , ar rearrangements were observed in 1.3% of cases ( 0.4% primary site and 2.2% metastatic site ) ; however , because the sequencing strategy was not explicitly designed to detect ar rearrangements and does not fully cover ar intronic regions , the true frequency of ar rearrangements is difcult to establish . 
gas that co - occur with targetable gas ( fig 1b ) and their impact on response to therapy warrant consideration in biomarker - driven trials . msi - h and tmb - h have been associated with immunotherapy benet , 10 , 24 , 25 and gloh - h has been associated with parp inhibitor benet21 ; therefore , assessment of signatures of genomic instability potentially expands the population of patients addressable with immunotherapy or targeted therapy . we identied a subset of tmprss2 rearrangements fused to upstream intergenic regions of erg , etv4 , or etv5 as well as novel ets fusion partners . 
 cgp of primary and metastatic prostate tumors etv4 ( 32 ; 2.6% ) etv5 ( 15 ; 1.2% ) etv1 ( 105 ; 8.5% ) tmprss2 - erg ( 1 , 084 ; 87.7% ) etv1 etv4 etv5 intron 4 ( n = 38 ) erg gene ( nm_004449 chr21 : 40033704 - 39751950 ) intron 3 ( n = 940 ) intron 1 ( n = 58 ) upstream ( 108 bp - 75 kbp ) ( n = 39 ) intron 2 ( n = 9 ) erg exon 1 genomic coordinates : chr21 : 40020000 40040000 40060000 40080000 40100000 40120000 fig 3 . 
consistent with distinct molecular subsets of prostate cancer , 1 , 8 ets fusions were mutually exclusive with spop / cul3 , cdk12 mutations , or braf rearrangements / mutations that may potentially comprise a clinically relevant genomic subset.30 , 31 diverse ar gas can mediate androgen axis inhibitor resistance28 , 29 and were strongly enriched in metastatic site tumors . 
ar rearrangements that disrupted the ligand - binding domain can mediate resistance to current ar inhibitors.29 development of novel ar inhibitors that target the diverse spectrum of ar alterations is needed . 
 ( a ) ar genomic alterations ( gas ) were identied in 721 cases , including amplication ( red ) , mutation ( green ) , and rearrangements ( purple )  . 
of note , 11q13 amplication is associated with endocrine resistance in breast cancer and potentially targetable by broblast growth factor receptor inhibitors32 - 34 and , therefore , warrants investigation in prostate cancer . 
second , cdkn2a gas were enriched in metastatic site tumors ( 1.9 - fold ) , and although not previously described in primary versus metastatic studies , 1 - 3 acquired cdkn2a alterations were described in enzalutamide - resistant tumors.15 metastatic enrichment of cell cycle gas suggests that cdk4 / 6 inhibitors could be explored . 
 cgp of primary and metastatic prostate tumors certain hrr genes , mmr genes , or msi status ; identication of such dna repair ga by tumor sequencing warrants follow - up germline testing and genetic counseling . 
however , compared with a recent study , 3 we identify similar relative proportions of germline / somatic mutations for frequently mutated hrr genes ( brca2 , atm , chek2 )  . 
furthermore , another study of prostate cancer similarly identied germline mutations for many of the dna repair genes evaluated here.37 we also describe potential cdk12 germline mutations ( four of 12 were rs138292741 )  . 
although not identied in one recent study of cdk12 in prostate cancer , 8 germline truncating cdk12 mutations were described in other studies , cluding prostate cancer , 38 - 40 and in germline databases.40 although preclinical studies have identied non - brca1 / 2 hrr genes , their association with hrd phenotype in clinical samples is unclear . 
identication of gloh - h cases lacking dna repair gas ( appendix fig a4a ) may have clinical value , but further investigation in parp inhibitor trials is required to assess the clinical utility of gloh as a biomarker in prostate cancer . similarly , dna repair gas were associated with msi - h or tmb - h genomic signatures that are associated with benet from immunotherapy ( fig 2 ; appendix fig a5 )  . 
a subset of msi / tmb - h cases do not harbor corresponding dna repair gas potentially because gas may occur in genes involved in dna repair that have not yet been discovered , complex rearrangements with intronic breakpoints may be challenging to detect , or genomic instability can occur through mechanisms such as gene silencing or extrinsic dna damage . limitations of this study should be acknowledged . 
furthermore , because samples were collected for routine clinical testing , primary samples in this cohort may be biased toward patients who have received prior treatment or developed metastatic disease that resulted in a distinct genomic landscape from untreated primary tumors . 
chung employment : foundation medicine ninad dewal employment : foundation medicine stock and other ownership interests : foundation medicine ethan sokol employment : foundation medicine paul mathew honoraria : exelixis patents , royalties , other intellectual property : patent pending on new therapeutic invention travel , accommodations , expenses : exelixis robert whitehead employment : unitedhealthcare , cancer treatment centers of america sherri z . 
pal honoraria : novartis , medivation , astellas pharma consulting or advisory role : pzer , novartis , aveo , myriad pharmaceuticals , genentech , exelixis , bristol - myers squibb , astellas pharma , ipsen , eisai research funding : medivation richard j . 
lee consulting or advisory role : janssen pharmaceuticals , exelixis research funding : janssen pharmaceuticals andrea necchi employment : bayer ag ( i ) stock and other ownership interests : bayer ag ( i ) honoraria : roche , merck , astrazeneca , janssen pharmaceuticals , foundation medicine consulting or advisory role : merck sharp & dohme , roche , bayer ag , astrazeneca , clovis oncology , janssen pharmaceuticals , incyte , seattle genetics , astellas pharma , bristol - myers squibb , rainier therapeutics research funding : merck sharp & dohme ( inst ) , astrazeneca ( inst ) travel , accommodations , expenses : roche , merck sharp & dohme , astrazeneca , janssen pharmaceuticals other relationship : bayer ag ( i ) jeffrey p . 
gregg consulting or advisory role : astrazeneca , bristol - myers squibb , roche , foundation medicine speakers bureau : astrazeneca , foundation medicine , bristol - myers squibb primo lara jr honoraria : pzer consulting or advisory role : exelixis , pzer , astrazeneca , bayer ag , genentech , roche , janssen pharmaceuticals , bristol - myers squibb , abbvie , turnstone bio , foundation medicine , merck , cellmax life , nektar research funding : millennium pharmaceuticals ( inst ) , polaris ( inst ) , glaxosmithkline ( inst ) , genentech ( inst ) , aragon pharmaceuticals ( inst ) , janssen pharmaceuticals ( inst ) , heat biologics ( inst ) , tracon pharma ( inst ) , merck ( inst ) , pharmacyclics ( inst ) , incyte ( inst ) emmanuel s . 
antonarakis honoraria : sano , dendreon , medivation , janssen pharmaceuticals , essa , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , medivation , janssen pharmaceuticals , essa , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen pharmaceuticals ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : co - inventor of a biomarker technology that has been licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation vincent a . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : revolution medicines patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center jeffrey s . 
 cgp of primary and metastatic prostate tumors research funding : bayer ag ( inst ) , bristol - myers squibb ( inst ) , glaxosmithkline ( inst ) , medivation ( inst ) , takeda pharmaceuticals ( inst ) , novartis ( inst ) , pzer ( inst ) , bn immunotherapeutics ( inst ) , tracon pharma ( inst ) , rexahn pharmaceuticals ( inst ) , amgen ( inst ) , astrazeneca ( inst ) , active biotech ( inst ) , bavarian nordic ( inst ) , calithera biosciences ( inst ) , celldex ( inst ) , eisai ( inst ) , genentech ( inst ) , immunomedics ( inst ) , janssen pharmaceuticals ( inst ) , merck ( inst ) , newlink genetics ( inst ) , prometheus ( inst ) , sano ( inst ) no other potential conicts of interest were reported . references abeshouse a , ahn j , akbani r , et al : the molecular taxonomy of primary prostate cancer . 
nat genet 50 : 645 - 651 , 2018 abida w , armenia j , gopalan a , et al : prospective genomic proling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making . 
n engl j med 373 : 1697 - 1708 , 2015 de bono js , de giorgi u , massard c , et al : pten loss as a predictive biomarker for the akt inhibitor ipatasertib combined with abiraterone acetate in patients with metastatic castration - resistant prostate cancer ( mcrpc )  . 
mateo j , ganji g , lemech c , et al : a rst - time - in - human study of gsk2636771 , a phosphoinositide 3 kinase beta - selective inhibitor , in patients with advanced 8 . 
clin cancer res 23 : 5981 - 5992 , 2017 2018 lee l , ali s , genega e , et al : aggressive - variant microsatellite - stable pole mutant prostate cancer with high mutation burden and durable response to immune checkpoint inhibitor therapy . 
cell 161 : 1215 - 1228 , 2015 [ erratum : cell 162 : 454 , 2015 ] joseph jd , lu n , qian j , et al : a clinically relevant androgen receptor mutation confers resistance to second - generation antiandrogens enzalutamide and arn509 . 
han gc , hwang j , wankowicz sam , et al : genomic resistance patterns to second - generation androgen blockade in paired tumor biopsies of metastatic castration - resistant prostate cancer . 
mateo j , chakravarty d , dienstmann r , et al : a framework to rank genomic alterations as targets for cancer precision medicine : the esmo scale for clinical actionability of molecular targets ( escat )  . 
bajrami i , frankum jr , konde a , et al : genome - wide proling of genetic synthetic lethality identies cdk12 as a novel determinant of parp1 / 2 inhibitor sensitivity . 
blazek d , kohoutek j , bartholomeeusen k , et al : the cyclin k / cdk12 complex maintains genomic stability via regulation of expression of dna damage response 21 . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
coleman rl , oza am , lorusso d , et al : rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
carbone dp , reck m , paz - ares l , et al : first - line nivolumab in stage iv or recurrent non - small - cell lung cancer . 
giltnane jm , hutchinson ke , stricker tp , et al : genomic proling of er + breast cancers after short - term estrogen suppression reveals alterations associated with endocrine resistance . 
luen sj , asher r , lee ck , et al : association of somatic driver alterations with prognosis in postmenopausal , hormone receptor - positive , her2 - negative early breast cancer : a secondary analysis of the big 1 - 98 randomized clinical trial . 
soria j - c , debraud f , bahleda r , et al : phase i / iia study evaluating the safety , efcacy , pharmacokinetics , and pharmacodynamics of lucitanib in advanced solid tumors . 
brovkina oi , shigapova l , chudakova da , et al : the ethnic - specic spectrum of germline nucleotide variants in dna damage response and repair genes in hereditary breast and ovarian cancer patients of tatar descent . 
popova t , mani e e , boeva v , et al : ovarian cancers harboring inactivating mutations in cdk12 display a distinct genomic instability pattern characterized by large tandem duplications . 
abida w , bryce ah , vogelzang nj , et al : preliminary results from triton2 : a phase ii study of rucaparib in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) associated with homologous recombination repair ( hrr ) gene alterations . 
clarke n , wiechno p , alekseev b , et al : olaparib combined with abiraterone in patients with metastatic castration - resistant prostate cancer : a randomised , double - blind , placebo - controlled , phase 2 trial . 
 cgp of primary and metastatic prostate tumors appendix methods approval for this study , including a waiver of informed consent and health insurance portability and accountability act waiver of authorization , was obtained from the western institutional review board ( protocol 20152817 )  . 
comprehensive genomic proling ( cgp ) results were reported clinically by prospective sequencing of tissue samples from 3 , 476 unique patients with prostate cancer ( august 2014 to february 2018 ) using a validated hybrid capture - based cgp assay ( foundationone [ baitset version t7 was used during this period ] ) 16 in a clinical laboratory improvement amendmentscertied , college of american pathologistsaccredited , new york stateapproved laboratory ( foundation medicine , cambridge , ma )  . 
for patients with multiple submitted samples , only a single sample was included , and the sample with the highest sequencing quality metrics was included . age and site of specimen collection were abstracted from the accompanying pathology reports , clinical notes , and requisition forms submitted by the treating physician . 
specimens included 1 , 660 primary site tumors and 1 , 816 metastatic site tumors ( appendix fig a1 )  . the pathologic diagnosis of each case was conrmed on routine hematoxylin and eosinstained slides , and all samples forwarded for dna extraction contained a minimum of 20% tumor nuclei . 
cgp was performed on hybridization - captured , adaptor ligation - based libraries to a median coverage depth of 743 for 395 cancer - related genes plus select introns from 31 genes frequently rearranged in cancer ( appendix table a1 )  . 
for ets fusions , targeted regions were tmprss2 ( introns 1 to 3 ) , erg ( all exons ) , etv1 ( introns 3 to 4 ) , etv4 ( intron 8 ) , and etv5 ( introns 6 to 7 )  . insertions / deresults were analyzed for base substitutions , short letions , rearrangements , and copy number alterations ( amplication and homozygous deletion )  . 
genomic alterations ( gas ) were called as reportable if the specic variant was present in the catalog of somatic mutations in cancer database ( forbes et al : nucleic acids res 45 : d777 - d783 , 2017 ) , if the variant has been characterized as pathogenic , or if the variant had likely functional status ( disruptive alterations in tumor suppressor genes ) ; all other variants were classied as variants of unknown signicance . to compare relative enrichments in primary site and metastatic site tumors , genes altered at a 2% or greater frequency were assessed for enrichment . 
enrichment was dened as the difference in frequency of gene alteration between metastatic site and primary site samples . to determine microsatellite instability status , 114 intronic homopolymer repeat loci on the foundationone panel were analyzed for length variability and compiled into an overall microsatellite instability score through principal components analysis ( chalmers et al : genome med 9 : 34 , 2017 )  . 
tumor mutational burden was calculated as the number of somatic base substitutions or insertions / deletions per megabase of the coding region target territory of the test ( 1.1 mb ) after ltering to remove known somatic and deleterious mutations and extrapolating that value to the exome or genome as a whole ( chalmers et al : genome med 9 : 34 , 2017 )  . 
tumor mutational burden was categorized as low ( fewer than six mutations / mb ) , intermediate ( six to 20 mutations / mb ) , or high ( 20 mutations / mb or more ; chalmers et al : genome med 9 : 34 , 2017 )  . 
germline , somatic , and zygosity statuses for mutations were determined without matched normal tissue as previously described17 ; in validation testing of 480 germline / somatic calls from tumor - only sequencing with matched normal reference samples , accuracy was 95% for somatic calls and 99% for germline calls . 
biallelic inactivation was dened as mutations under loss of heterozygosity ( loh ) as determined by zygosity status.17 percent genome - wide loh ( gloh ) was used as a marker of homologous recombination deciency and calculated as described , and a gloh score of 14% or greater was dened as gloh - high.21 potentially targetable gas were dened as those that have been associated with response to targeted therapy in prostate cancer , homologous recombination repair gas that have been associated with responses to poly ( adp - ribose ) polymerase inhibitors , or gas associated with response to targeted therapy in multiple other tumor types and were ranked according to modied european society for medical oncology scale for clinical actionability of molecular targets criteria.18 ln ( unk ) ln ( d ) ln ( l ) liver bone lung other prostate ( n = 1 , 660 ) metastasis ( n = 1 , 816 ) neuroendocrine ( 4% ) undifferentiated ( 3% ) acinar ( 93% ) fig a1 . 
for fusion , exons ( e ) are annotated with the last exon included in the 5 ( cid : 3 ) partner and the rst exon included in the 3 ( cid : 3 ) partner . 
in addition , braf rearrangements at intron 9 ( n = 6 ) and intron 7 ( n = 1 ) and raf1 rearrangement at intron 7 with no clear fusion partner were identied ( data not shown )  . 
 ( a ) genome - wide loss of heterozygosity ( gloh ) score was assessable for 2 , 624 cases , and cases with 14% or more gloh were designated loh - high ( loh - h )  . 
loh - h cases were assessed for the presence ( green ) or absence ( yellow ) of a genomic alteration ( ga ) in the homologous recombination repair ( hrr ) or fanconi anemia / interstrand crosslink repair ( fa / icl ) pathway . 
 ( b ) genes were grouped together into hrr pathway ( excluding non - brca1 / 2 ) or fa / icl pathway ( fanc ) ; genes were categorized as in figure 2a . 
 ( a ) microsatellite instability ( msi ) status was assessable for 3 , 326 cases , and each case was designated as msi - high ( msi - h ) , msi - low ( msi - l ) , or microsatellite stable ( mss )  . 
the percent tmb - high ( tmb - h ) or tmb of 10 or more mutations ( mut ) / mb cases in primary site and metastatic site tumors is indicated . 
 m is there room for personalized medicine in small - cell lung cancer ( sclc ) ? remarkable activity of pazopanib in refractory fgfr1 - amplied ed - sclc alessandro russo , md1 , 2 ; david arias ron , md3 ; marika rasschaert , md3 ; hans prenen , md , phd3 ; ranee mehra , md1 ; katherine scilla , md1 ; patrick pauwels , phd3 ; and christian rolfo , md , phd , mba , drhc1 , 3 introduction small - cell lung cancer ( sclc ) is a malignant neuroendocrine tumor that represents almost 15% of total lung cancers , characterized by distinct clinicopathologic , biologic , and therapeutic features.1 in contrast to the impressive progress made in non - sclc ( nsclc ) , 2 , 3 treatment of sclc remained relatively unchanged for more than 30 years . 
only recently the advent of immune checkpoint inhibitors introduced novel options in the therapeutic armamentarium of sclc.4 - 7 despite accelerated approval of these agents , several relevant questions remain unanswered . 
unfortunately , for the vast majority of patients survival rates are still quite disappointing . during the last several years , different studies have shed light on the genetic background of sclc , and a new model of sclc subtypes has been proposed.8 sclcs have a mean mutation rate of 7.4 nonsynonymous mutations per million base pairs , and alterations in tumor - suppressor genes are the most frequent ndings , 9 with mutations in rb1 ( 91% ) and tp53 ( 98% ) being nearly ubiquitous.10 alterations in the notch family genes are detected in 25% of sclcs10 and have a crucial role in sclc tumorigenesis , disease progression , and chemoresistance.11 recently , delta - like protein 3 ( dll3 ) , a notch inhibitory ligand , has emerged as a potential target in sclc , and the dll3 - targeted antibody - drug conjugate rovalpituzumab tesirine is under active clinical development.11 unfortunately , most of the genome alterations found in sclc are not easily therapeutically tractable . interestingly , broblast growth factor receptor 1 ( fgfr1 ) amplications have been reported in a small subgroup of patients ( 5%7% ) 10 , 12 - 14 and might represent a potentially exploitable therapeutic target . preclinical data have shown in vitro and in vivo activity of the fgfr inhibitor pd173074 on sclc growth.15 multiple fgfr inhibitors have been developed , and different nonselective agents have been evaluated in unselected patients with sclc with relatively modest activity.16 , 17 to date , the role of these agents has not been evaluated in fgfr - amplied sclc . the development of new diagnostic methods , cluding liquid biopsy and next - generation sequencing ( ngs ) , offers novel opportunities to identify potentially exploitable genetic alterations in this tumor type . 
to our knowledge , we present for the rst time a case of a heavily pretreated patient with advanced sclc with an fgfr1 amplication who experienced a durable and remarkable response to third - line pazopanib . informed consent for use of the radiology images was obtained by the patient presented . case report a 49 - year - old woman without relevant medical antecedents was diagnosed in august 2015 with ct3 n3 m0 sclc . 
at that time , she presented with nodules in the same lung lobe ( stage iiib according to tnm , 8th edition ) , and with symptomatic superior vena cava ( svc ) syndrome , including dyspnea , cyanosis , fatigue , and weight loss . 
at that time , additional local treatment with radiation was not possible , and there was a decline in clinical condition ( eastern cooperative oncology group performance status 2 )  . treatment with carboplatin - etoposide was initiated but did not result in a clinical response after two cycles , as the computed tomography ( ct ) scan in october 2016 showed additional progression of disease . 
hence , she started second - line topotecan , but after 10 weeks new lung progression was found in imaging studies . in january 2017 , the patient was referred to the phase iearly clinical trials unit of the university of antwerp . a liquid biopsy with a 73 - gene ngs plasma test ( guardant360 ; guardanthealth , redwood city , ca ) was performed to determine the existence of somatic alterations and targetable mutations . 
on the basis of these results and the absence of clinically approved drugs at that time , off - label pazopanib 800 mg / d was started on february 20 , 2017 after notication of the local ethical committee . pazopanib is a tyrosine kinase inhibitor with highly selective activity against vascular endothelial growth factor receptors ( vegfr - 1 , - 2 , and - 3 ; ic50 , 10 - 47 nm ) , platelet - derived growth factor receptors ( pdgfrand - ; ic50 , 84 nm ) , c - kit ( ic50 , 74 nm ) , and fgfr - 1 , - 2 , and - 319 ( ic50 , 140 nm ) , and it is currently approved for the treatment of metastatic renal cell cancer and soft - tissue sarcoma . after 2 months of treatment , in april 2017 a ct scan evaluation showed a partial response according to recist to perform real - time monitoring of the disease , in may a second liquid biopsy was carried out , demonstrating a molecular response to the treatment with a spectacular decrease of molecular tumor burden , with fgfr1 amplication undetectable in plasma cfdna ( fig 2 ) , as well as myc and raf1 amplications . in june 2017 , the patient developed dyspnea and chest pain , with right - sided crackles on auscultation . 
a chest x - ray showed a possible growth in the right upper quadrant with right - sided bronchus obliteration and lateral expansion of lung mass , in addition to enlargement of a right apical nodule . 
cdbca - vp16 , carboplatin - etoposide ; cddpvp16 , cisplatin - etoposide ; cfdna , cell - free dna ; ecog ps2 , eastern cooperative oncology group performance status 2 ; ld - sclc , limited disease smallcell lung cancer ; nd , not detectable ; ngs , next - generation sequencing ; pd , progressive disease ; rt , radiotherapy ; svcs , superior vena cava syndrome . nonetheless , we performed a uorodeoxyglucosepositron emission tomography ( fdg - pet ) scan in july 2017 for a better interpretation of previous results and noted a consolidation in the right hemithorax compatible with a necrotic process and not with tumor progression ( fig 3a ) , further conrming the decision of maintaining treatment with pazopanib at the same dose . in september 2017 , a new liquid biopsy analysis was repeated , showing an increase of amount of cfdna , with a total of eight somatic alterations detected and reappearance of fgfr1 amplication . 
an fdg - pet scan ( fig 3b ) and a ct scan documented progression of disease in both the thorax and abdomen , with enlargement of the primary tumor , mediastinal adenopathy , mesenteric lesions , and a left adrenal gland nodule . 
 ( a ) fdgpet scan in july 2017 shows an increase in size of the consolidation process in the right thorax half , with current conuent intense ring - shaped tracer stacking ( presumably component central necrosis / cysteous transformation )  . 
 ( b ) fdg - pet scan in february 2018 documenting progression of disease in both the thorax and the abdomen . inhibitor either in clinical trial or as compassionate use . unfortunately , treatment was poorly tolerated , and in april 2018 radiotherapy to the mediastinum was performed because of re - emergence of svc syndrome . 
the patient ultimately died in july 2018 as a result of clinical deterioration and further disease progression . discussion the fgfr family comprises four transmembrane tyrosine kinase members ( fgfr 1 - 4 ) and a fth member without tyrosine kinase domain ( fgfr - 5 ) that has been recently identied . 
the main pathways include ras / mapk , dagpkc , and pi3k / akt / mtor , which result in nuclear activation of genomic compounds related to cell growth , differentiation , proliferation , motility , angiogenesis , and apoptosis20 ( appendix fig a1 )  . in clinical practice , interest in fgfr as a potential targetable pathway in several tumor types is based on evidence of uncontrolled oncogenesis , tumor progression , and development of resistance as a result of aberrant fgfr - fgf signaling axis . 
genetic aberrations of fgfr members have been reported in multiple solid tumors.21 - 23 interestingly , fgfr1 amplications ( 8q12 locus ) have been described in different cancers , 24 , 25 including 5% - 7% of sclc , 10 , 12 - 14 and fgfr blockade has demonstrated preclinical in vivo and in vitro activity in sclc , 15 with increased sensitivity in cell lines with higher copies of fgfr1.14 moreover , fgfr1 amplication has been correlated with poorer outcomes after platinum - etoposide chemotherapy.26 these data suggest that fgfr1 could represent a valuable target for sclc . 
multiple selective and nonselective fgfr inhibitors have been developed to date ( appendix fig a1 ) , and in april 2019 the us food and drug administration granted accelerated approval of erdatinib for the treatment of bladder cancer with fgfr3 or fgfr2 alterations . 
 remarkable activity of pazopanib in fgfr - amplied sclc reported a sustained and remarkable response to pazopanib in a heavily pretreated patient with ed - sclc relines and with svc fractory to two previous treatment syndrome . 
interestingly , plasma ngs results predicted radiographic disease progression a few months in advance , further conrming the utility of serial liquid biopsies in oncogene - driven tumors treated with targeted inhibitors . these results are quite impressive and suggest that an appropriate selection strategy might improve the outcome of patients with ed - sclc , who have been traditionally considered to have low responses to targeted therapy strategies . 
ctcs are prognostic factors for survival in both limited29 and ed - sclc , 30 , 31 and their decline during treatment has been correlated with response to chemotherapy31 , 32 and also pazopanib.33 some studies have also shown the utility of molecular analysis of ctcs to depict the genomic proles and evolutionary history of sclc.34 therapeutic decision - making process and might pave the way for the development of targeted therapies through rationally designed clinical trials . 
furthermore , liquid biopsy can also allow real - time monitoring of patients treated with targeted therapies , predicting disease progression in advance compared with conventional radiographic methods , 35 , 36 as reported in our case . 
no data were reported in fgfr - amplied tumors . emergence of cdk6 amplication and raf1 amplication at progression suggests the involvement of these abnormalities in the development of resistance to pazopanib . interestingly , activation of erk1 / 2 has been associated with lines , 37 pazopanib resistance in synovial sarcoma cell suggesting that activation of alternative downstream signaling pathways such as ras / raf / erk / mek might represent an escape strategy to fgfr blockage in sclc . 
furthermore , multiple cdk4 / 6 inhibitors are under active evaluation in sclc in combination with chemotherapy , and alterations of cell cycle regulation genes can represent a potential target . in the present case , the use of a commercially available 73 - gene plasma ngs in our case demonstrates the utility of this diagnostic tool also in patients with sclc to select the best therapeutic strategy and might provide a useful minimally invasive source for tumor genotyping in a disease that is classically associated with small histologic tumor samples . 
the biomolecular information derived by these tests can guide the in conclusion , we reported here for the rst time a dramatic and sustained response to a nonselective fgfr inhibitor in a refractory , heavily pretreated ed - sclc harboring an fgfr1 amplication through a plasma ngs test . 
fgfr1 amplication can represent a novel therapeutic target in sclc , and clinical evaluation of novel selective fgfr inhibitors in this selected population is awaited . affiliations 1university of maryland medical center greenebaum comprehensive cancer center , baltimore , md 2a.o. 
 russo et al ranee mehra stock and other ownership interests : glaxosmithkline ( i ) consulting or advisory role : genentech , bayer research funding : astra zeneca patrick pauwels consulting or advisory role : astra zeneca , boehringer ingelheim , bristolmyers squibb belgium ( inst ) , msd oncology ( inst ) , roche molecular diagnostics , pzer ( inst ) , bayer ( inst ) research funding : pzer ( inst ) , roche molecular diagnostics ( inst ) christian rolfo consulting or advisory role : mylan speakers bureau : novartis , msd , guardanthealth travel , accommodations , expenses : ialsc , astrazeneca research funding : novartis , sano , grant from antwerp university hospital , belgium no other potential conicts of interest were reported . acknowledgment we thank amelie lyssens for her assistance in the material supply . references gazdar af , bunn pa , minna jd : small - cell lung cancer : what we know , what we need to know and the path forward . 
nat rev cancer 17 : 725 - 737 , 2017 [ erratum : nat rev cancer 17 : 765 , 2017 ] corrales l , scilla k , caglevic c , et al : immunotherapy in lung cancer : a new age in cancer treatment , in naing a and hajjar j ( eds ) : immunotherapy . 
cham , switzerland , springer international publishing , 2018 , pp 65 - 95 russo a , franchina t , ricciardi grr , et al : a decade of egfr inhibition in egfr - mutated non small cell lung cancer ( nsclc ) : old successes and future perspectives . 
n engl j med 379 : 2220 - 2229 , 2018 antonia sj , l opez - martin ja , bendell j , et al : nivolumab alone and nivolumab plus ipilimumab in recurrent small - cell lung cancer ( checkmate 032 ) : a multicentre , open - label , phase 1 / 2 trial . 
cancer cell 33 : 853 - 861.e4 , 2018 [ erratum : cancer cell 35 : 329 , 2019 ] chung hc , lopez - martin ja , kao sc - h , et al : phase 2 study of pembrolizumab in advanced small - cell lung cancer ( sclc ) : keynote - 158 . 
j clin oncol 36 , 2018 ( suppl 15 ; abstr 8506 ) rudin cm , poirier jt , byers la , et al : molecular subtypes of small cell lung cancer : a synthesis of human and mouse model data . 
nat rev cancer 19 : 289 - 297 , 2019 [ erratum : nat rev cancer 19 : 415 , 2019 ] sabari jk , lok bh , laird jh , et al : unravelling the biology of sclc : implications for therapy . 
schultheis am , bos m , schmitz k , et al : fibroblast growth factor receptor 1 ( fgfr1 ) amplication is a potential therapeutic target in small - cell lung cancer . 
pardo oe , latigo j , jeffery re , et al : the broblast growth factor receptor inhibitor pd173074 blocks small cell lung cancer growth in vitro and in vivo . 
koinis f , agelaki s , karavassilis v , et al : second - line pazopanib in patients with relapsed and refractory small - cell lung cancer : a multicentre phase ii study of the hellenic oncology research group . 
nat rev cancer 17 : 318 - 332 , 2017 jiang t , gao g , fan g , et al : fgfr1 amplication in lung squamous cell carcinoma : a systematic review with meta - analysis . 
park js , lee j - s , kim ey , et al : the frequency and impact of fgfr1 amplication on clinical outcomes in korean patients with small cell lung cancer . 
sun j - m , lee kh , kim b - s , et al : pazopanib maintenance after rst - line etoposide and platinum chemotherapy in patients with extensive disease small - cell lung cancer : a multicentre , randomised , placebo - controlled phase ii study ( kcsg - lu12 - 07 )  . 
rolfo c , mack pc , scagliotti gv , et al : liquid biopsy for advanced non - small cell lung cancer ( nsclc ) : a statement paper from the iaslc . 
tay ry , fern andez - guti errez f , foy v , et al : prognostic value of circulating tumour cells in limited - stage small - cell lung cancer : analysis of the concurrent oncedaily versus twice - daily radiotherapy ( convert ) randomised controlled trial . 
hou j - m , krebs mg , lancashire l , et al : clinical signicance and molecular characteristics of circulating tumor cells and circulating tumor microemboli in patients with small - cell lung cancer . 
hou j - m , greystoke a , lancashire l , et al : evaluation of circulating tumor cells and serological cell death biomarkers in small cell lung cancer patients undergoing chemotherapy . 
messaritakis i , politaki e , plataki m , et al : heterogeneity of circulating tumor cells ( ctcs ) in patients with recurrent small cell lung cancer ( sclc ) treated with 34 . 
su z , wang z , ni x , et al : inferring the evolution and progression of small - cell lung cancer by single - cell sequencing of circulating tumor cells . 
oxnard gr , paweletz cp , kuang y , et al : noninvasive detection of response and resistance in egfr - mutant lung cancer using quantitative next - generation genotyping of cell - free plasma dna . 
clin cancer res 20 : 1698 - 1705 , 2014 iwama e , sakai k , azuma k , et al : monitoring of somatic mutations in circulating cell - free dna by digital pcr and next - generation sequencing during afatinib treatment in patients with lung adenocarcinoma positive for egfr activating mutations . 
each one of the four members of the fgfr family presents an intracellular region , which involves a juxtamembrane domain that acts as a binding side for phosphotyrosinebinding domains , a transmembrane domain that allows ligand - dependent activation as a result of the stabilization of receptor conformation , and an extracellular ligand binding domain including three immunoglobulin domains that act as binding points for fgfr ligands ( olsen et al : proc natl acad sci usa 101 : 935 - 940 , 2004 )  . 
the fgf family is composed of almost 22 ligands that have been identied in humans , and each one is recognized by a specic fgfr member ( beenken et al : nat rev drug discov 8 : 235 - 253 , 2009 )  . 
although from their analysis , her2 exon 20 mutations emerge as the most clearly actionable driver in nsclc , the authors themselves pinpoint ambiguous functional roles of individual her2 aberrations ( ie , activating mutations , amplication , and overexpression ) , as well as their reciprocal associations . therefore , her2 biology may be different in lung cancer compared with breast or gastric cancers , possibly because of specic microenvironmental and tumor - host interactions . as pointed out by the authors , a substantial heterogeneity exists in therapeutic approaches and clinical results of her2 - targeting strategies in this context . this is well exemplied by two clinical nsclc cases harboring different her2 alterations ( her2 mutation and all three her2 aberrationsmutation , amplication , and protein overexpression , respectively ) we discuss herein . case 1 a 44 - year - old woman , never - smoker , presented with stage ivb lung adenocarcinoma ( egfr - wt , alk and ros1 nonrearranged , pd - l1 1% )  . 
she was then treated with two courses of atezolizumab , resulting in clinico - radiologic hyperprogression.2 next - generation sequencing ( ngs ) based molecular proling revealed a her2 exon 20 insertion ( p.a775_ g776insyvma ) ; neither gene amplication nor protein expression was detected . 
she then received whole - brain radiotherapy ( rt ) for an isolated brain progression and was subsequently enrolled in a clinical trial of poziotinib ; treatment was poorly tolerated , and diffuse extracranial progression rapidly ensued . 
rechallenge with trastuzumab and vinorelbine obtained no clinical benet , and she went on to receive gemcitabine single agent and subsequently best supportive care on further clinicoradiologic disease progression . case 2 a 48 - year - old woman , never - smoker , presented with stage iib lung adenocarcinoma in 2011 , when she underwent left inferior lobectomy and medilymphadenectomy followed by adjuvant astinal cisplatin / vinorelbine . 
in 2018 , disease recurred in multiple metastatic sites ; right supraclavicular lymph node rebiopsy showed egfr - wt , alk and ros1 nonrearranged , and pd - l1 1% , and she received rstline platinum - based chemotherapy with partial response , followed by stereotactic body rt on residual tumor sites ; multisite disease progression was observed 2 months after treatment completion . 
she was then started on trastuzumab emtansine ( tdm - 1 ) in march 2020 , experiencing dramatic clinical benet with disappearance of all disease - related symptoms , in particular dyspnea , and performance status improvement ( from 2 to 0 , according to eastern cooperative oncology group ) ; treatment is currently ongoing . the two cases presented highlight the inherent complexity of her2 biology in nsclc and the difculties in reliably predicting the clinical outcome of specic her2 - targeted interventions . 
in case 1 , a clinically meaningful response to trastuzumab - based treatment was observed , in line with other reports , 3 - 5 even in the presence of an isolated exon 20 mutation not accompanied by gene amplication and in the absence of protein expression by immunohistochemistry . 
intrigued by the relatively unexpected response , occurring after hyperprogression to pd - l1 blockade , we analyzed fcriiia polymorphisms and found that the patient carried a valine / valine ( v / v ) variant , which has been correlated to better response to trastuzumab - based treatment in breast cancer.6 in line with the presence of a polymorphism potentially fostering antibody - dependent cell - mediated cythe patients peripheral blood totoxicity ( adcc ) , mononuclear cells displayed a marked and specic trastuzumab - dependent cytotoxic activity toward her2 - overexpressing targets in vitro ( fig 1 )  . 
on the other hand , such a mechanism did not prove relevant in case 2 , in which no response to trastuzumab - based treatment was observed , despite gene amplication and protein overexpression accompanying exon 20 insertion . 
 ( a ) computed tomographic imaging of primary lesion at baseline ( showing atezolizumab progression , left ) and at rst assessment during trastuzumab - based therapy ( right )  . 
 ( b ) mcf7 target cells , expressing ( mcf7 - her2 ) or not expressing ( mcf7 - evector ) her2 antigen , were rst stained with carboxyuorescein succinimidyl ester ( cfse ) 5 mm and celltrace 5 mm , respectively . 
mixed targets ( ratio 1 : 1 ) were incubated for 18 hours at different ratios ( 2 : 1 , 4 : 1 , 8 : 1 , 12 : 1 ) with peripheral blood mononuclear cells ( pbmcs ) isolated from peripheral blood of the patient in the presence of rituximab ( 10 mg / ml ) or trastuzumab ( 10 mg / ml )  . 
tumor cellspecic lysis by pbmcs was analyzed by ow cytometry ( representative plot of 8 : 1 ratio on the left ) and quantied as percentage of lysis ( right ) using the formula : ( 1 ( % mcf7 - her2 or mcf7 - evector + trastuzumab / tot target ) / ( %mcf7 - her2 or mcf7 - evector + rituximab / tot target ) 100 )  . 
fitc , uorescein isothiocyanate ; v450 - ct , v450 cell trace . overall , her2 aberrations in nsclc convey important prognostic10 and potentially predictive information ; however , prospective studies should be designed not only according to patients stratication for specic her2 aberration ( s ) or combinations but also it is mandatory to evaluate the patients immunologic features , especially for antibody - based treatments . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . zhao j , xia y : targeting her2 alterations in nonsmall - cell lung cancer : a comprehensive review . 
jco precis oncol 4 : 411 - 425 , 2020 kato s , goodman a , walavalkar v , et al : hyperprogressors after immunotherapy : analysis of genomic alterations associated with accelerated growth rate . 
clin cancer res 23 : 4242 - 4250 , 2017 chuang jc , stehr h , liang y , et al : erbb2 - mutated metastatic non - small cell lung cancer : response and resistance to targeted therapies . 
mazi `eres j , barlesi f , filleron t , et al : lung cancer patients with her2 mutations treated with chemotherapy and her2 - targeted drugs : results from the european euher2 cohort . 
mazi `eres j , peters s , lepage b , et al : lung cancer that harbors an her2 mutation : epidemiologic characteristics and therapeutic perspectives . j clin oncol 31 : 1997 - 2003 , 2013 6 . 
musolino a , naldi n , bortesi b , et al : immunoglobulin g fragment c receptor polymorphisms and clinical efcacy of trastuzumab - based therapy in patients with her - 2 / neu - positive metastatic breast cancer . 
j clin oncol 26 : 1789 - 1796 , 2008 li b , ofn m , hembrough t , et al : p1.13 - 43 molecular and imaging predictors of response to ado - trastuzumab emtansine in patients with her2 mutant lung cancers : an exploratory phase 2 trial . 
j thorac oncol 13 : s599 , 2018 li bt , shen r , buonocore d , et al : ado - trastuzumab emtansine for patients with her2 - mutant lung cancers : results from a phase ii basket trial . 
j clin oncol 36 : 2532 - 2537 , 2018 peters s , stahel r , bubendorf l , et al : trastuzumab emtansine ( t - dm1 ) in patients with previously treated her2 - overexpressing metastatic non - small cell lung cancer : efcacy , safety , and biomarkers . 
milella m , nuzzo c , bria e , et al : egfr molecular proling in advanced nsclc : a prospective phase ii study in molecularly / clinically selected patients pretreated with chemotherapy . 
 cd33_pgx6_score predicts gemtuzumab ozogamicin response in childhood acute myeloid leukemia : a report from the childrens oncology group lata chauhan , phd1 ; miyoung shin , phd1 ; yi - cheng wang , ms2 ; michael loken , phd3 ; jessica pollard , md4 , 5 ; richard aplenc , md , msce6 ; betsy a . 
lamba , phd1 purpose the us food and drug administration recently announced reapproval of gemtuzumab ozogamicin ( go ) for treatment of cd33 - positive acute myeloid leukemia ( aml ) , thus opening up opportunities to develop strategies for effective use of go . 
we further developed a composite cd33 pharmacogenetics ( pgx ) score using six cd33 snps ( cd33_pgx6_score ) for association with clinical outcome . results four cd33 snps were associated with cell surface cd33 levels and clinical response in the go versus no - go arms . 
 chauhan et al context key objective the key objective of this study was to identify and establish the clinical impact of cd33 genetics on treatment response to gemtuzumab , a recently approved cd33 - directed immunotherapeutic agent in patients with acute myeloid leukemia . knowledge generated our results identied multiple cd33 single nucleotide polymorphisms ( snps ) of prognostic signicance that were associated with gemtuzumab clinical response . 
patients with a cd33_pgx6_score of 0 or higher had higher cd33 expression levels compared with patients with a score of less than 0 and demonstrated improved disease - free survival and reduced risk of relapse when given gemtuzumab . 
no improvement from gemtuzumab was observed in patients with a cd33_pgx6_ score of less than 0 . relevance our results hold promise for developing strategies to personalize the use of cd33 - directed agents such as gemtuzumab using cd33 genetics . 
in addition , cd33 expression levels have been correlated with disease characteristics such as presence of flt3 internal tandem duplications ( itds ) , npm1 mutations , and high - risk group features.20 , 21 recently , we reported a splicing single nucleotide polymorphism ( snp ) in cd33 rs12459419 ( c.t ) , resulting in a shorter isoform of cd33 that lacks exon 2 ( cd33 - d2 ) .22 lack of exon 2 results in loss of the igv domain within the cd33 protethis is clinically relevant , because the igv domain is recognized by go and other cd33 antibodies used in clinical immunophenotyping of aml specimens . 
our results showed signicant association of rs12459419 with diagnostic leukemic cell surface cd33 intensity ( determined using igv targeting p67.6 antibody ) , as well as differential response in go versus no - go treatment arms.22 specically , patients with at least one copy of the variant t allele ( ct / tt genotypes ) derived no benet from addition of go . 
in contrast , patients with homozygous cc genotype showed signicantly better survival ( event - free survival [ efs ] and disease - free survival [ dfs ] ) as well as lower risk of relapse with the addition of go to standard chemotherapy.22 in contrast to these results , an investigation in the united kingdom mrc adult aml cohorts showed consistent association of the splicing snp with cd33 cell surface intensity but no association with clinical outcome.23 this was most likely a result of the inclusion of multiple go random assignments and varying go doses in these studies23 or the presence of other cd33 snps . 
these observations and an anticipated increase in the use of go as a result of its recent approval prompted us to evaluate the prognostic role of other snps within cd33 in the context of the go - based randomized cog aaml0531 trial . 
details of the study design , treatment regimen , and clinical outcome have been reported previously.17 overall , 1 , 022 patients with de novo aml ( age , 0 to 29 years ) were randomly assigned to either standard ve - course chemotherapy ( no - go arm ; n = 511 ) or the same chemotherapy plus two doses of go 3 mg / m2 ( go arm ; n = 511 ) during induction 1 and intensication 2 . as described previously , low - risk features included t ( 8 ; 21 ) , inv ( 16 ) , or t ( 16 ; 16 ) ; high - risk features included monosomy 7 , monosomy 5 / 5q deletion , or persistent disease at end of induction 1 . 
patients not classied as low or high risk were categorized as intermediate risk and received hematopoietic stem - cell transplantation if suitable donor was available.17 , 21 specimens from patients who consented for biology studies were used in this study . 
the institutional review boards of all participating institutions approved the clinical protocol , and the cog myeloid disease biology committee approved this research study . genotyping of cd33 snps on the basis of our previous ndings , 24 , 25 we selected cd33 snps with potential functional or clinical relevance that occurred with the minimum allele frequency of greater than 0.10 in either white or black patients . 
genotype data on rs12459419 ( ala14 val ) splicing were already available in this cohort.22 all cd33 snps had a call rate of greater than 0.98 , and all but rs1803254 were in accordance with the hardy - weinberg equilibriuin addition , we genotyped a novel 4base pair ( bp ) ccgg deletion variation ( rs201074739 ) that creates a premature termination codon and thus loss of cd33 using a polymerase chain reactionrestriction fragment length polymorphismbased recent data suggest method ( data supplement )  . 
for cd33 snps rs12459419 , rs1803254 , rs35112940 , rs6136475 , and rs201074739 , with variant alleles associated with lower leukemic cell surface cd33 intensity and inferior response by treatment arms , the genotype score was 0 for wild - type ( wt ) / wt genotype , 1 for wt / variant genotype , and 2 for variant / variant genotype ( for rs201074739 , none of the patients were the variant allele )  . 
for cd33 snp homozygous for rs2455069 , with variant allele associated with high cd33 cell surface intensity and superior response by treatment arms , the genotype score was 0 for wt / wt genotype , 1 for wt / variant genotype , and 2 for variant / variant genotype . composite cd33_pgx6_score = ( individual genotype scores of six snps [ rs12459419 , rs1803254 , rs35112940 , rs201074739 , rs61736475 , and rs2455069 ] )  . 
 chauhan et al statistical analyses genotype and clinical data were available for 938 patients . clinical outcome data for patients enrolled in cog aaml0531 were current as of september 30 , 2014 . 
the median follow - up time for eligible patients with de novo aml who were alive at last contact and included in our analysis was 1 , 856 days ( range , 4 to 2 , 829 days )  . 
the kaplan - meier method was used to estimate overall survival ( os ; dened as time from study entry to death ) , efs ( dened as time from study entry until failure to achieve cr during induction , relapse , or death ) , and dfs ( dened as time from end of course 1 for patients in cr until relapse or death ) .28 relapse risk ( rr ) was calculated by cumulative incidence methods dened as time from the end of induction 1 for patients in cr to relapse or death , where deaths without a relapse were considered competing events . 
cox proportional hazards models were used to estimate the hazard ratios ( hrs ) for os and efs.29 the 2 test was used to test the signicance of observed differences in proportions , and fishers exact test was used when data were sparse . 
in contrast , for missense snp rs2455069 , the presence of the variant g allele was associated with higher cd33 levels ( p , .001 ; table 1 and data supplement )  . 
no difference in distribution within arms , in risk groups , or by flt3 - itd status was observed ( data supplement ) for these snps , indicating the effect of these snps on cd33 cell surface intensity might not be associated with risk group characteristics . 
rs201074739 and rs61736475 occurred with a low frequency , and thus analysis within each group was limited by small sample size within genotype groups . in a subset of patients ( n = 496 ) , we had mrna levels of total cd33 available from the rna sequencing data . 
as shown in the data supplement , variant alleles for 3 ( cid : 1 ) utr rs1803254 ( p = .010 ) and the rs201074739 - ccgg deletion that results in a premature termination codon ( p = .003 ) were associated with low cd33 mrna expression . association of cd33 snps with clinical outcome by treatment arm ( no - go v go ) survival estimates and rr indicated differences in treatment arm by cd33 snps ( table 2 )  . 
although limited by numbers , we observed that presence of variant alleles for rs1803254 ( c allele ) , rs35112940 ( a allele ) , rs201074739 ( ccgg deletion ) , and rs61736475 ( c allele ) within the 12459419 cc genotype resulted in no signicant outcome benet from adding go to treatment ( data supplement )  . 
presence of the wt / reference genotype for these snps in conjunction with the wt / reference cc genotype for rs12459419 resulted in significant improvement in outcome with the addition of go . 
 cd33_pgx and gemtuzumab response in aml across all genotype groups , which was expected given that the variant allele is associated with higher cd33 expression . development of composite cd33_pgx6_score and its association with cd33 expression and benet from go on the basis of the results for individual cd33 snps as well as our previous ndings regarding rs12459419 splicing snp , 22 we developed a composite cd33_pgx6_score for each patient by taking into account the directional genotype scores of six snps ( rs12459419 , rs1803254 , rs2455069 , rs35112940 , rs61736475 , and rs201074739 ) , as described in patients and methods . 
a higher snp score was associated with higher cd33 cell surface expression , and as the score decreased , it was predictive of lower cd33 levels ( p , .001 ; fig 3a )  . 
signicant benet of adding go , compared with the standard no - go arm , was observed only for the score categories of 0 and greater than 1 ( p , .05 ) , and no difference in outcome was observed for the 3 to 4 and 2 to 1 categories . 
given this observation and that a score of 0 indicated reference allele for each genotype , we dichotomized patients into those with a cd33_pgx6_score of 0 or higher and those with scores less than 0 ( presence of least one detrimental allele )  . 
the cd33_pgx6_score was created for each patient using genotype information for the following six single nucleotide polymorphisms ( snps ) : rs12459419 , rs1803254 , rs35112940 , rs2455069 , rs61736475 , and rs201074739 . 
genotype scores are as follows : wild type ( wt ) / wt = 0 , wt / variant ( var ) = 1 , and var / var = 2 for rs12459419 , rs1803254 , rs35112940 , rs61736475 , and rs201074739 and wt / var = 1 and var / var = 2 for rs2455069 . 
association of dichotomized cd33 - pgx6_score ( rs12459419 , rs35112940 , rs1803254 , rs2455069 , rs61736475 , and rs201074739 ) with clinical outcome by go versus no - go arms in all patients and by risk group no - go no . 
association of dichotomized cd33 - pgx6_score ( rs12459419 , rs35112940 , rs1803254 , rs2455069 , rs61736475 , and rs201074739 ) with clinical outcome by go versus no - go arms in all patients and by risk group ( continued ) no - go no . 
success of go has resulted in development of multiple new cd33 - directed therapeutics that are currently at different stages of development and investigation , such as fc - engineered unconjugated antibodies ( bi 836858 [ mab 33.1 ] ) , antibody - drug conjugates ( sgncd33a [ vadastuximab talirine ] , imgn779 , and ave9633 ) , radioimmunoconjugates ( actinium - 225 lintuzumab ) , biand trispecic antibodies ( amg330 , amg673 , amv564 , and 161533 trike fusion protein ) , and chimeric antigen receptormodied immune effector cells.30 thus , timely to dene pharmacogenetic determinants of go response . we recently reported that the cd33 splicing polymorphism rs12459419 c.t regulates production of an alternatively spliced isoform of cd33 lacking exon 2 and , hence , the igv domain of cd33.22 our previous results demonstrated that rs12459419 was a signicant predictor of cell surface cd33 intensities as well as clinical response . 
association of dichotomized cd33_pgx6_score ( rs12459419 , rs35112940 , rs1803254 , rs2455069 , rs61736475 , and rs201074739 ) with clinical outcome by go versus no - go arms in patients with aml patients by race no - go no . 
our results show that the rs1803254 , rs2455069 , rs201074739 , and rs35112940 snps in cd33 are signicantly associated with cell surface cd33 expression as well as outcome by treatment arm ( go v no - go ) within the context of the cog in the 3 ( cid : 1 ) utr aaml0531 trial . 
the novel variant rs201074739 is a 4 - bp deletion in exon 3 that changes the reading frame , creating a premature regulates cd33 transcript termination codon and thus nonfunctional truncated cd33 protethe transcript with premature termination is degraded by the cellular nonsense - mediated decay pathway , 26 consistent with the observed association of this variant with cd33 mrna levels . rs35112940arg304gly and rs61736475 - ser305pro occur close to the itim motif of cd33 and thus might inuence cd33 function . 
our results demonstrate the clinical impact of these snps , warranting additional investigation in independent clinical cohorts as well as in - depth molecular these snps for impact on cd33 characterization of mrna , protein stability , cd33 trafcking and signaling , and efcacy of other cd33 - directed therapies . given that a patient with aml can inherit different genotype combinations for snps ( as shown in cd33 onco - print ; data supplement ) , it is important to evaluate the association of genotype combinations for the most inuential snps in relation to cd33 cell surface levels and go clinical response . 
a cd33_pgx6_score of 0 or higher was associated with signicantly higher cd33 expression , better efs and dfs , and lower rr in the go arm compared with the nogo arin patients with a score of less than 0 , cd33 expression was low , and the addition of go did not provide any clinical benet . 
in addition , as shown in figure 3b , there is overlap in the cd33 expression levels between the scores , indicating that the cd33 expression may not be the sole determinant of response . 
in fact , our previous data show that patients heterozygous ( ct ) for the splicing snp rs12459419 , despite having intermediate levels of cd33 , did not benet from the addition of go , implying co - occurrence of the short isoform with the full - length isoform compromising the efcacy . 
furthermore , as indicated earlier , the presence of the coding or splicing variations can affect cd33 intracellular trafcking , localization , internalization rates of the go - cd33 complex , recycling , and signaling as the mechanisms underlying the observed impact on response . 
pollard et al21 showed that patients classied as low cd33 expressers ( quartile 1 ) on the basis of cd33 cell surface levels do not derive benet from go , whereas patients classied as high cd33 expressers ( quartiles 2 to 4 ) show signicant improvement with go . 
we investigated the interaction of snps within high cd33 expressers ( quartiles 2 to 4 , as per pollard et al21 ) and observed that , despite being in a high cd33 expression category , the presence of a detrimental variant allele for cd33 snp compromises benet from adding go to chemotherapy ( data not shown )  . 
our results show that in black patients with a cd33_pgx6_score of less than 0 , 54.5% of patients have the cc genotype , compared with only 6% of white patients with the cc genotype for the rs12459419 splicing group . 
given that the cd33_pgx6_score considers multiple cd33 snps in addition to the splicing snp , it is more likely to identify patients who are less likely to benet from go or other cd33 - directed therapies across different ethnic groups . 
the novel snp rs201074739 , a 4 - bp ccgg deletion that results in truncated protein , never occurs in patients in the rs12459419 tt genotype group ( data supplement ) but has been observed in patients with the cc and ct genotypes for rs12459419 , indicating its contribution to lower cd33 levels and perhaps response within the rs12459419 cc and ct genotype groups . given the anticipated increase in go use with its recent approval and several new cd33 - directed therapies in the pipeline , development of the cd33_pgx6_score is timely and critical to establish its ability and clinical utility to personalize go treatment in aml . 
our future work is targeted toward validating the cd33 score in other clinical cohorts ( united kingdom trials ) and an upcoming study from cog that plans to incorporate go - containing regithe cd33_pgx6_score holds mens . 
lamba provision of study material or patients : richard aplenc collection and assembly of data : lata chauhan , yi - cheng wang , michael loken , jessica pollard , richard aplenc , betsy a . 
alonzo , soheil meshinchi , jatinder k . lamba manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors michael loken employment : hematologics , hematologics ( i ) leadership : hematologics , hematologics ( i ) stock and other ownership interests : hematologics , hematologics ( i ) consulting or advisory role : newlink genetics richard aplenc honoraria : sigma - tau expert testimony : wiggin and dana travel , accommodations , expenses : sigma - tau irwin d . 
16 / 091 , 720 entitled biomarkers of anti - leukemic therapy no other potential conicts of interest were reported . acknowledgment we thank the childrens oncology group acute myeloid leukemia reference laboratory for providing specimens for the study . 
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leukemia 27 : 843 - 851 , 2013 burnett ak , hills rk , hunter ae , et al : the addition of gemtuzumab ozogamicin to low - dose ara - c improves remission rate but does not signicantly prolong survival in older patients with acute myeloid leukaemia : results from the lrf aml14 and ncri aml16 pick - a - winner comparison . 
burnett ak , hills rk , milligan d , et al : identication of patients with acute myeloblastic leukemia who benet from the addition of gemtuzumab ozogamicin : results of the mrc aml15 trial . 
castaigne s , pautas c , terr e c , et al : effect of gemtuzumab ozogamicin on survival of adult patients with de - novo acute myeloid leukaemia ( alfa - 0701 ) : a randomised , open - label , phase 3 study . 
delaunay j , recher c , pigneux a , et al : addition of gemtuzumab ozogamycin to chemotherapy improves event - free survival but not overall survival of aml patients with intermediate cytogenetics not eligible for allogeneic transplantation : results of the goelams aml . 
hills rk , castaigne s , appelbaum fr , et al : addition of gemtuzumab ozogamicin to induction chemotherapy in adult patients with acute myeloid leukaemia : a meta - analysis of individual patient data from randomised controlled trials . 
cooper tm , franklin j , gerbing rb , et al : aaml03p1 , a pilot study of the safety of gemtuzumab ozogamicin in combination with chemotherapy for newly diagnosed childhood acute myeloid leukemia : a report from the childrens oncology group . 
gamis as , alonzo ta , meshinchi s , et al : gemtuzumab ozogamicin in children and adolescents with de novo acute myeloid leukemia improves event - free survival by reducing relapse risk : results from the randomized phase iii childrens oncology group trial aaml0531 . 
 cd33_pgx and gemtuzumab response in aml jen ey , ko cw , lee je , et al : fda approval : gemtuzumab ozogamicin for the treatment of adults with newly diagnosed cd33 - positive acute myeloid leukemia . clin cancer res 24 : 3242 - 3246 , 2018 19 . 
norsworthy kj , ko cw , lee je , et al : fda approval summary : mylotarg for treatment of patients with relapsed or refractory cd33 - positive acute myeloid leukemia . 
pollard ja , alonzo ta , loken m , et al : correlation of cd33 expression level with disease characteristics and response to gemtuzumab ozogamicin containing chemotherapy in childhood aml . 
pollard ja , loken m , gerbing rb , et al : cd33 expression and its association with gemtuzumab ozogamicin response : results from the randomized phase iii childrens oncology group trial aaml0531 . 
lamba jk , chauhan l , shin m , et al : cd33 splicing polymorphism determines gemtuzumab ozogamicin response in de novo acute myeloid leukemia : report from randomized phase iii childrens oncology group trial aaml0531 . 
mortland l , alonzo ta , walter rb , et al : clinical signicance of cd33 nonsynonymous single - nucleotide polymorphisms in pediatric patients with acute myeloid leukemia treated with gemtuzumab - ozogamicin - containing chemotherapy . 
papageorgiou i , loken mr , brodersen le , et al : ccgg deletion ( rs201074739 ) in cd33 results in premature termination codon and complete loss of cd33 expression : another key variant with potential impact on response to cd33 - directed agents . 
 eleven month progressionfree survival on vemurafenib monotherapy in a patient with recurrent and metastatic braf v600emutated glioblastoma who grade 4 introduction glioblastoma multiforme ( gbm ) accounts for 3% to 4% of all cancer - related deaths , despite having an average incidence rate of 3.19 / 100 , 000 population.1 , 2 prognosis for gbm remains poor , with standard - of - care therapy providing only a 16to 20 - month median overall survival.3 , 4 braf kinase inhibitors have transformed melanoma treatment and have successfully been used in other tumor types containing the braf v600e mutation.5 - 8 there are several reports of improved survival with the use of braf - directed therapy in braf - positive gbm , although the efficacy of braf inhibitors in nonmelanoma cancers has not been systematically explored . 
a basket study of 122 patients with braf v600e mutations in various nonmelanoma cancer types found three out of six patients with gbm experienced tumor regression with vemurafenib.8 a pediatric case series presented three pediatric patients with braf v600e - mutant high - grade gliomas treated with vemurafenib , including a patient with clinical and neurologic improvement 20 months after starting treatment.9 robinson et al10 reported a case of complete clinical regression of a braf v600emutant pediatric gbm treated with braf inhibitor therapy . 
the patient underwent a craniotomy with resection , and pathology demonstrated glioblastoma , who grade 4 , isocitrate dehydrogenase ( idh - 1 ; wild - type immunohistochemistry and by sequencing )  . 
further analysis showed a tert mutation and wildtype for both atrx and egfr . immediate postoperative imaging showed residual enhancement superior to the resection cavity , treated with gamma knife radiosurgery . 
subsequent treatment consisted of fractionated intensitymodulated radiation therapy of 60 gy at 2 gy per fraction with concurrent daily temozolomide 75 mg / m2 , followed by monthly cycles of maintenance temozolomide . 
her treatment was then switched to bevacizumab monotherapy . eleven months postsurgery , or 4 months after switching to bevacizumab monotherapy , she was found to have a right hemispheric focus of duralbased enhancement concerning for local recurrence and underwent repeat gamma knife radiosurgery . 
within 2 months of starting vemurafenib , she was weaned off all opioid medications , dexamethasone , baclofen , and gabapentshe reported a significant improvement in her quality of life and was once again able to work with physical therapy to improve her chronic left - sided weakness . 
five months after starting vemurafenib , her brain and spine mri demonstrated significant improvement in intracranial leptomeningeal disease and in the nodular leptomeningeal enhancement along the conus medullaris and multiple nerve roots of the cauda equina . 
eleven months after starting vemurafenib monotherapy , the patient reported feeling well overall and had achieved stable disease on brain and spine mri ( fig 3 )  . she denied any headaches , visual changes , back pain or neuropathy , or gi or genitourinary symptoms . 
she was rated 80% on the karnofsky performance status scale . discussion this case report is consistent with several others in showing significantly improved survival with the use of braf kinase inhibitors in braf v600e positive gbm . 
no epithelioid or rhabdoid morphology was identified . spine , which demonstrated drop metastases throughout the thoracic and lumbosacral spine , specifically on the posterior cord from t10 - 12 , anterior to the conus medullaris , and throughout the cauda equina . 
an mri of the spine 1 month later showed a significant increase in the number and size of the abnormal cord enhancement lesions . one month after being diagnosed with metastatic recurrent glioblastoma , the patient was referred to our clinic , and we recommended addition of carboplatin area under the curve 4 intravenously monthly to her regimen of bevacizumab 10 mg / kg intravenously every 2 weeks . 
at the time of vemurafenib approval 2 months later and before starting the braf inhibitor , neuraxis imaging demonstrated development of leptomeningeal enhancement around the lobe resection cavity and initial right parietal considerable progression of metastatic spinal cord disease . 
 plasma concentration ratio for dabrafenib was 10 - fold higher compared with vemurafenib.17 in the dabrafenib plus trametinib versus vemurafenib alone in unresectable or metastatic braf v600e / k cutaneous melanoma ( combi - v ) trial , patients with braf - mutated metastatic melanomas who were treated with the combination of dabrafenib and mek inhibitor trametinib had significantly longer pfs than those treated with vemurafenib monotherapy.18 furthermore , dabrafenib appears to be less nephrotoxic than vemurafenib.19 nonmelanoma tumorspecific studies of braf inhibitors are difficult to conduct because of the relative rarity of these tumors and the low frequencies of braf mutations . 
these limitations also extend to basket trials of braf inhibitors , such as the national cancer institutemolecular analysis for therapy choice ( nci - match ; eay131 - h protocol ) evaluating dabrafenib and trametinib in patients with braf v600e or v600k mutations . 
despite these limitations , case reports of exceptional responders to targeted therapies such as ours support the value of genetics - guided therapy for activating braf mutations and driver mutations in general in gbm and other rare cancers , underscoring the need to systematically investigate these targeted drugs . the case reports can also be of value in supporting current off - label therapy of these rare mutations in tumor types not listed in the us food and drug administrationapproved indications . 
this microscopic image shows an immunohistochemical study for braf v600e . the tumor cells and their processes are positive for the mutated form of the protein . although there is a therapeutic potential of braf inhibitors in gbm , the experience with these drugs in melanoma treatment suggests that resistance will surely emerge in tumors responsive to this therapy . several mechanisms mediating resistance to braf inhibitors through mitogen - activated protein kinase ( mapk ) reactivation have been described , and coadministration of braf inhibitors with selective mapk inhibitors has led to significant improvement in progression - free survival in melanoma.15 coadministration with alternative survival pathway inhibitors , such as vascular endothelial growth factor and phosphatidylinositol 3 - kinase inhibitors , may also need to be evaluated.16 it could be further argued that dabrafenib might be the preferred braf kinase inhibitor . 
tran honoraria : novocure , monteris medical consulting or advisory role : novocure research funding : novocure , merck , novartis , tocagen , northwest biotherapeutics , vbl therapeutics , stemline therapeutics patents , royalties , other intellectual property : a molecular cell diary system , chemotherapeutic methods to target differentiated tumor cells , generep and nscore : method and apparatus for improved determination of node influence in a network , core master regulators of glioblastoma stem cells , conversion of glioblastoma multiforme cells into regulatory immune cells , novel targets that prevent cancer cells from evading the immune system and synergize with current immunotherapies travel , accommodations , expenses : novocure , monteris medical , novartis , tocagen , vbl therapeutics ashley p . 
 ( b ) the same regions are denoted by arrows on follow - up imaging performed 8 months later , showing improvement in metastatic disease and near - complete resolution of some lesions . references med 6 : 1359 - 1370 , 2014 1 . 
stupp r , mason wp , van den bent mj , et al : radiotherapy plus concomitant and adjuvant temozolomide for epidemiol biomarkers prev 23 : 1985 - 1996 , 2014 glioblastoma . 
stupp r , taillibert s , kanner aa , et al : maintenance therapy with tumor - treating fields plus temozolomide vs temozolomide alone for glioblastoma : a randomized clinical trial . 
myall nj , neal jw , cho - phan cd , et al : long - term survival of a patient with nonsmall - cell lung cancer harboring a v600e mutation in the braf oncogene . 
hyman dm , puzanov i , subbiah v , et al : vemurafenib in multiple nonmelanoma cancers with braf v600 mutations . n engl j med 373 : 726 - 736 , 2015 9 . 
schindler g , capper d , meyer j , et al : analysis of braf v600e mutation in 1 , 320 nervous system tumors reveals high mutation frequencies in pleomorphic xanthoastrocytoma , ganglioglioma and extra - cerebellar pilocytic astrocytoma . acta neuropathol 121 : 397 - 405 , 2011 14 . 
jang s , atkins mb : which drug , and when , for patients with braf - mutant melanoma ? lancet oncol 14 : e60 - e69 , 2013 17 . 
kieran mw , cohen kj , doz f , et al : complete radiographic responses in pediatric patients with brafv600 - positive tumors including high - grade gliomas : preliminary results of an ongoing phase 1 / 2a safety and pharmacokinetics ( pk ) study of dabrafenib . 
grob jj , amonkar mm , karaszewska b , et al : comparison of dabrafenib and trametinib combination therapy with vemurafenib monotherapy on health - related quality of life in patients with unresectable or metastatic cutaneous braf val600 - mutation - positive melanoma ( combi - v ) : results of a phase 3 , open - label , randomised trial . 
 o evaluation of the her / pi3k / akt family signaling network as a predictive biomarker of pathologic complete response for patients with breast cancer treated with neratinib in the i - spy 2 trial purpose in the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) , the panerythroblastic oncogene b inhibitor neratinib was available to all hormone receptor ( hr ) / human epidermal growth factor receptor 2 ( her2 ) subtypes and graduated in the hr - negative / her2 - positive signature . 
we hypothesized that neratinib response may be predicted by baseline her2 epidermal growth factor receptor ( egfr ) signaling activation / phosphorylation levels independent of total levels of her2 or egfr proteins . materials and methods complete experimental and response data were available for between 130 and 193 patients . 
in qualifying analyses , which used logistic regression and treatment interaction analysis , 18 protein / phosphoprotein , 10 mrna , and 12 dna biomarkers that related to her family signaling were evaluated . 
 exploratory analysis of her family signaling in patients with triple - negative ( tn ) disease found that activation of egfr y1173 ( p = .005 ) and her2 y1248 ( pher2 ) ( p = .019 ) were positively associated with pathologic complete response . 
exploratory analysis in this pegfr / pher2activated tn subgroup identified elevated levels of estrogen receptor ( p < .006 ) in these patients . conclusion activation of her family phosphoproteins associates with response to neratinib , but only egfr y1173 and stmn1 appear to add value to the graduating signature . 
 introduction the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ; clinicaltrials.gov identifier : nct01042379 ) is a phase ii , adaptive neoadjuvant therapy trial in which the primary goal was to determine the predictive probabilities of phase iii trial success for various targeted therapeutics . 
patients with locally advanced , high - risk breast cancer had their diseases assigned to one of eight subtypes on the basis of hormone receptor ( hr ) , human epidermal growth factor receptor 2 ( her2 ) , and mammaprint - based high1 / ( ultra ) high2 risk statuses.1 - 3 neratinib , a pan - erythroblastic oncogene b ( erbb ) inhibitor , was available to patients with all tumor subtypes in the i - spy 2 trial , and the agent availability was graduated in the hr negative / her2 - positive signature.4 neratinib has shown activity against her2 - positive metastatic breast cancer , and there is also evidence for activity against her2 - negative tumor cells in vitro.5 , 6 because neratinib was available to all patients in the trial , this study provided an opportunity to test the efficacy of the drug in patients with her2 - negative tumors . cell linebased preclinical studies have implicated alterations in her / akt / mtor family genes on the dna , mrna , or protein level as predictive of neratinib response.7 - 11 however , recent her2 therapybased clinical trials in which her family biomarkers at the total protein and / or mrna level were analyzed for response prediction found that none provided predictive value compared with the conventional , us food and drug administrationapproved immunohistochemistry ( ihc ) / fluorescence in situ hybridizationbased her2 / estrogen receptor ( er ) testing methods.12 - 14 previous work with the i - spy 1 trial cohort revealed that her2 phosphorylation was highly concordant with her2 expression.15 that study identified a subpopulation of patients who had her2 negative disease by standard testing yet had her2 phosphorylation levels similar to patients with her2 - positive disease . 
the her2 activation seen in these patients in the her2 - negative subtype appeared coincident with epidermal growth factor receptor ( egfr ) activation . on the basis of the mechanism of action of neratinib as a potent her family kinase inhibitor combined with observations of i - spy 1 trial results , we postulated that her2 and egfr activation / phosphorylation may be predictive of neratinib response independent of total her2 status in the i - spy 2 trial ; this hypothesis was motivation for an exploratory analysis within the her2 - negative and triple - negative ( tn ) subpopulation . 
our analysis of her / phosphoinositide - 3 - kinase ( pi3k ) / akt signaling family components in pretreatment samples from the neratinib and concurrent control arms of the i - spy 2 trial was performed at a unique multiomic level . 
we report results from the following : ( 1 ) assessment of selected mutation / copy number alterations by exome sequencing , ( 2 ) mrna expression levels by expression microarrays , and ( 3 ) analysis of protein / phosphoprotein levels by reverse phase protein arrays ( rppas ) as specific biomarkers of neratinib response . 
rppa analysis assessed the ability of 18 protein / phosphoproteins that comprise the known drug targets of neratinib ( egfr , her2 ) and downstream effector molecules , such as shc transforming protein 1 ( shc ) and mammalian target of rapamycin ( mtor ) / ak thyoma ( akt ) signaling components to predict complete pathologic response ( pcr ) to neratinib . 
 patients randomly assigned to the experimental arm were treated with neratinib in addition to standard chemotherapy ( neratinib + t > ac ) .4 in patients with her2 - positive disease , neratinib was administered in place of trastuzumab ( appendix fig a1 )  . 
consort diagram that outlines the number of patients included in the neratinib and control arms of the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) and those included in the subsequent analyses . 
cnv , copy number variation ; rppa , reverse phase protein array . primary efficacy analysis cohort neratinib concurrent control pretreatment expression data available neratinib concurrent control ( n = 193 ) ( n = 115 ) ( n = 78 ) ( n = 193 ) ( n = 115 ) ( n = 78 ) withdrew consent for use of tissue ( n = 2 ) pretreatment samples available for additional biomarker assessment ( n = 191 ) neratinib concurrent control ( n = 115 ) ( n = 76 ) insufficient material ( n = 23 ) insufficient material ( n = 61 ) rppa data available ( n = 168 ) neratinib ( n = 106 ) concurrent control ( n = 62 ) somatic mutation and cnv data available neratinib concurrent control ( n = 168 ) ( n = 78 ) ( n = 52 ) expression by using agilent 44k expression arrays ( agendia , irvine , ca ) , signaling protein activation by rppa , and dna sequencing ( approximately 2 , 000 - gene mini - cancer genome ; utrecht , the netherlands )  . 
details of sample preparation and data processing are provided in the data supplement . in our prespecified analysis plan , 16 logistic regression was used to assess association with pcr in the control and neratinib treated populations individually . 
relative biomarker performance between arms ( biomarker - by - treatment interaction ) was assessed with a logistic model ( pcr approximately equaled treatment + biomarker + [ treatment biomarker ] )  . 
 if a continuous biomarker did not follow a normal distribution , we applied a nonparametric method that discretized the score by using a series of cut points , and we applied logistic modeling for the dichotomized biomarker at each cut point ; significance was assessed by permutation testing . 
for significant biomarkers , bayesian logistic regression analysis was performed , as previously described , with the following model : pcr hr + her2 + biomarker + treatment + ( treatment hr ) + ( treatment her2 ) + ( treatment biomarker ) .16 in additional analyses , parametric t tests ( for normally distributed data ) or nonparametric wilcoxon rank sum tests ( for non - normally distributed data ) were used to assess association of protein end points with pcr in the control and neratinib - treated populations individually . 
hr , hormone receptor ; tn , triple negative . curves were generated for end points associated with pcr in the neratinib - treated arm of the trial to identify potential cut points for biomarker positivity rates within selected patient subtypes . 16 patients with mutated pik3ca achieved pcr in the neratinib arm compared with 24 ( 39% ) of 62 patients with wild - type pik3ca . 
however , pik3ca mutation status did not show a significant biomarker - by - treatment interaction . results evaluation of her family gene point mutations and dna amplification / loss as predictors of neratinib sensitivity we evaluated somatic mutations and copy number variations ( cnvs ) in 12 her family linked signaling pathway genesegf , egfr , her2 , nrg1 , igf1r , pik3ca , akt1 , pten , stmn1 , and mtorby targeting exome sequencing across all evaluable patients . 
 consistent with publications that link pik3ca mutation with resistance to neratinib and other her2 - targeted agents , 14 , 17 - 19 only two ( 13% ) of association of her family gene expression with response to neratinib we evaluated 10 predefined her family signaling genes as expression biomarkers of neratinib response in all evaluable patients ( appendix table a1 )  . 
her2 expression was significantly associated with sensitivity to neratinib combination therapy ( and in the her2 - positive subpopulation ) , and igf1r , to resistance ; neither gene was associated with response in the control arm of the trial ( appendix tables a1 and a2 )  . 
within the her2 negative subset , stmn1 was associated with response to neratinib ( p = .0023 ) and not control , and this result showed a significant biomarker - by - treatment interaction ( p = .0036 ; fig 3a ; appendix table a3 )  . 
 2 neratinib arm : her2 control arm : her2 hr + her2 no pcr no pcr her2 subset stmn1 - low stmn1 - high unselected her2 her2 / stmn1 - high pcr probability pcr probability fig 3 . 
 ( d ) bayesian estimated pcr probability distributions in ( left ) the unselected her2 - negative subset and ( right ) the her2 - negative / stmn1 - high subset in the control ( blue ) and neratinib ( gold ) arms . of patients with her2 - negative disease ( 29 of 106 patients ) had stmn1 - high status ( fig 3b - c )  . 
by using bayesian modeling , the estimated pcr rate of patients with her2 negative / stmn1 - high status in the treatment arm was 57% compared with 17% in the control arm ( fig 3d ) ; the predictive probability of phase iii success in this subset was 97% . her family protein signaling activation as predictors of neratinib sensitivity we evaluated 18 her family signaling proteins / phosphoproteins as biomarkers of neratinib response by using rppa data from pretreatment , laser capture microdissection ( lcm ) purified tumor epithelia across all evaluable patients in the neratinib and concurrent control arms . 
six of the 18 her family biomarkers tested ( egfr y1068 , egfr y1173 , egfr y992 , her2 total , her2 y1248 , and shc y317 ) were associated with pcr in neratinib - treated patients but not in concurrent control - arm patients in the trial ( table 1 )  . 
we dichotomized patients by their egfr y1173 intensity values into high and low groups ( optimal cut point of 4 , 501 , which maximized the significance of the biomarker - by - treatment interaction term ) , and we evaluated the distribution of pcr rates ( table 2 )  . 
bold indicates p < 0.05. the predictive probability of phase iii success ( appendix table a4 )  . comparison of her family gene expression , protein , phosphoprotein , and mutation data unsupervised clustering revealed that total protein levels of her - family genes clustered with its gene expression level , whereas phosphoprotein levels were more highly correlated to one another than to their respective gene or total protein expression levels ( fig 4 )  . 
pik3ca mutations ( 28 of 130 patients ) were not associated with altered levels of pik3ca expression of protein / phosphoprotein ; however , they were associated with lower levels of stmn1 and egfr gene expression and higher levels of the phosphoproteins pten s380 and akt s473 ( data not shown )  . exploratory analysis of her family signaling in patients with tn disease although neratinib graduated in the hr negative / her2 - positive signature , this signature was characterized by ihc / f luorescence in situ hybridizationbased analysis of total her2 expression and did not measure her2 or egfr phosphorylation . 
pcr rates for egfr y1173 and her2 y1248 biomarker high / low groups by hr / her2 subtype in neratinib - treated and control groups subtype neratinib ( n = 106 ) control ( n = 62 ) egfr y1173 ( riu > 4501 cutoff ) egfr y1173 high egfr y1173 low egfr y1173 high egfr y1173 low no . 
two - way plots of egfr y1173 and her2 y1248 for neratinib treated and concurrent controls demonstrated that nine ( 82% ) of 11 patients with tn disease who exhibited elevated phospho - egfr ( pegfr ) and phospho - her2 ( pher2 ) levels experienced a pcr in response to neratinib treatment compared with four ( 36% ) of 11 with tn disease among the concurrent controls ( table 2 ; fig 5a - b )  . 
bayesian evaluation of egfr y1173 and her2 y1248 as biomarkers for neratinib response in the tn population revealed a comparable probability of success in a phase iii trial to that of the graduated hr negative / her2 - positive population ( fig 5c ; appendix tables a4 and a5 )  . 
in this pegfr / pher2 - high group of tn tumors , 16 ( 76% ) of 21 patients had erlevels greater than the median value for the tn population compared with 11 ( 37% ) of 30 patients in the rest of the tn population ( fig 5d )  . 
in the neratinib - treated population alone , 11 ( 35% ) of 31 patients had pegfr / pher2 - high status , and nine ( 82% ) of 11 patients had total er levels greater than the tn population median . discussion as precision cancer medicine evolves into concomitant processes of discovery , validation , and development of biomarkers predictive of therapeutic response alongside the clinical assessment of drug efficacy , there is increasing emphasis on identification of predictive biomarker candidates as early as possible . 
the subset of biomarkers represented include phosphoproteins associated with response to neratinib , and their associated mrna and total protein levels ( scaled to a median of 0 and standard deviation of 1 )  . 
 egfr , epidermal growth factor receptor ; erbb , erythroblastic oncogene b ; her2 , human epidermal growth factor receptor 2 ; hr , hormone receptor ; na , not available ; shc , shc transforming protein ; tn , triple negative . neratinib arm control arm treatment receptor subtype pten loss pik3ca mut egf mut her2 mut egfr total egfr mrna stmn1 mrna erbb3 total erbb3 mrna egfr y1068 egfr y1173 her2 y1248 shc y317 egfr y992 erbb3 y1289 her2 total her2 mrna no pcr no pcr treatment receptor subtype mutation status heatmap color key neratinib control hr / her2 + hr + / her2 + hr + / her2 mutated wild type 3 2 1 0 1 2 3 value proteomic / phosphoproteomic biomarkers were measured in all pretreatment biopsy samples . 
given that her2 total protein levels do not strictly correlate with her2 phosphorylation in the her2 - negative setting , 15 and given that the phosphorylation status of her2 protein ( compared with total her2 ) provides significant information on breast cancer survival , 23 - 27 we postulated that phosphorylation levels of the neratinib drug targets her2 and egfr in pretreatment biopsy specimens would correlate with pcr in both her2 - positive and her2 negative tumors . our data revealed that coactivation of her2 and egfr correlated with pcr in both her2 positive and tn tumors . 
the pcr rate in the pegfr / pher2 - high tn population , according to an optimal cut point for both markers , was 82% ( nine of 11 patients ) in the treatment arm , compared with 36% ( four of 11 patients ) with pcr in the control ar although these data are exploratory , this pcr rate was higher than the 55% of patients who had a complete response observed in the graduated hr negative / her2 - positive arm for neratinib.4 in keeping with these results , in which phosphorylated egfr levels rather than total egfr were predictive for pcr , phosphorylated egfr has been shown to be a potential predictive marker for anti - egfr therapies in other tumors , such as nonsmall - cell lung cancer.28 , 29 also , our expression analysis produced only one predictive biomarker for neratinib sensitivity , stmn1 , a gene implicated in her2 pathway signaling and chemotherapy sensitivity in non - her2 amplified cell lines.30 - 33 although our data indicate that phosphorylation levels of her2 and egfr correlate with pcr in neratinib - treated patients with breast cancer , a number of caveats in the study limit generalizability . 
the adaptive design of the trial allowed for efficient and quick graduation ( or termination ) of agent / marker combinations on the basis of their estimated likelihood of phase iii success . 
analysis of epidermal growth factor receptor ( egfr ) y1173 and human epidermal growth factor receptor 2 ( her2 ) y1248 as biomarkers for neratinib response in patients with triple - negative ( tn ) disease enrolled in the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 )  . 
 ( a ) and ( b ) two - way plots of egfr y1173 and her2 y1248 intensities for tn ( a ) control group and ( b ) neratinib - treated patients . 
other studies with her family inhibitors have shown that neratinib , in combination with insulin - like growth factor receptor ( igfr ) inhibitors had antiproliferative effects in her2 non - overexpressing breast cancer cell lines , and pilot clinical studies of lapatinib treatment in various metastatic cancers showed a correlation of pher2 with lapatinib response.37 , 38 what is the basis for her2 and egfr activation in the tn subpopulation ? the frequency of her2 and egfr mutations in the neratinib cohort is too small ( n = 4 and 3 , respectively ) to be a contributing factor . 
in the absence of genomic alterations related to her family signaling when her activation is seen , a logical postulate is that the process is mediated by ligand - driven events . 
recently , it has been shown that neuregulin 1 ( nrg1 or heregulin ) and her2 phosphorylation coincidentally occurred in a subset of her2 - negative tumors and that inhibition of egfr or her2 or both receptors reduced breast cancer stem cell survival and self - renewal.39 although we evaluated nrg1 in our study and did not find any correlation with pcr or her2 activation status ( table 1 ) , we did explore the possibilities of other ligand - driven events underpinning the her2 and egfr activation observed in tn tumors , namely estrogen signaling . 
estrogen can exert nongenomic activity called membrane - initiated steroid signaling through binding with er at low concentrations40 ; er may exist in a signalsome complex with a variety of receptor tyrosine kinases , such as igfr , 41 egfr , 42 , 43 or her2 , 44 , 45 and lead to activation of egfr , her2 , and igfr121 in the absence of gene transcription . 
 we found that erlevels in the tn cohort were higher in pegfr / pher2 - high tumors than in tumors that were not her2 / egfr activated ( fig 5 )  . 
this result could provide a potential explanation for the paradoxical finding of her2 / egfr activation in tn cancers in the absence of her2 genomic alterations and must be confirmed in independent study sets . the lcm - rppa workflow used in this study provides a powerful and unique approach to quantitatively measure the activated signaling architecture of a large number of cancer - related pathways , including the her family , from microscopic quantities of tissue . 
this technology and workflow is especially well suited for clinical sample assessment.46 , 47 past studies have revealed the need for lcm to accurately assess phosphorylated and total protein levels , and to facilitate biomarker evaluation in the context of high and low tumor cell content.48 moreover , unlike ihc - based approaches that can be adversely effected by choice of antigen retrieval method , the rppa technique utilizes fully denatured protein in which phospho - epitopes are fully linearized and recognized by the cognate primary antibody . patients with tn breast cancer have a paucity of targeted therapeutic options available . 
given the pcr rate observed and biomarker positive prevalence we found in the tn setting , we believe these data provide a strong molecular rationale to consider prospective validation of the findings in patients with tn disease who received neratinib . 
to our knowledge , this study is the first of its kind to quantitatively assess activated her family signaling in the context of clinical response to her - directed therapies in a tn population . 
 the biomarker findings , although prespecified , ultimately are based on small numbers of patients and must be confirmed with larger patient populations in independent clinical studies to validate fig 5 . 
wulfkuhle honoraria : dava oncology patents , royalties and other intellectual property : coinventor on filed george mason universityassigned patents related to phosphorylated her2 and egfr response predictors for her family directed therapeutics . 
gallagher no relationship to disclose lamorna brown - swigart no relationship to disclose gillian hirst no relationship to disclose laura esserman consulting or advisory role : blue cross blue shield association research funding : merck travel , accommodations , expenses : blue cross blue shield association donald berry employment : berry consultants leadership : berry consultants stock and other ownership interests : berry consultants consulting or advisory role : berry consultants travel , accommodations , expenses : berry consultants minetta liu research funding : eisai ( inst ) , seattle genetics ( inst ) , novartis ( inst ) , roche ( inst ) , genentech ( inst ) , grail ( inst ) , merck ( inst ) , janssen diagnostics ( inst ) travel , accommodations , expenses : grail , mreck , celgene , agena bioscience , menarini silicon biosystems , cynvenio biosystems john w . 
park stock and other ownership interests : merrimack consulting or advisory role : genentech ( inst ) speakers ' bureau : genentech , pfizer , agendia ( i ) lodewyk f.a. 
petricoin iii leadership : perthera , ceres nanosciences stock and other ownership interests : perthera , ceres nanosciences , avant diagnostics consulting or advisory role : perthera , ceres nanosciences , azgen , avant diagnostics research funding : ceres nanosciences ( inst ) , glaxosmithkline ( inst ) , abbvie ( inst ) , symphony evolution ( inst ) patents , royalties , other intellectual property : national institutes of health patents licensing fee distribution / royalty . 
6 - 10 , 2016 , and the annual meeting of the american society for clinical oncology , chicago , il , may 29 - june 2 , 2015 . support prior presentation references 1 . 
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baselga j , corts j , im sa , et al : biomarker analyses in cleopatra : a phase iii , placebocontrolled study of pertuzumab in human epidermal growth factor receptor 2 - positive , first - line metastatic breast cancer . 
wolf dm , yau c , sanil a , et al : dna repair deficiency biomarkers and the 70 - gene ultra - highrisk signature as predictors of veliparib / carboplatin response in the i - spy 2 breast cancer trial . 
loibl s , majewski i , guarneri v , et al : pik3ca mutations are associated with reduced pathological complete response rates in primary her2 - positive breast cancer : pooled analysis of 967 patients from five prospective trials investigating lapatinib and trastuzumab . 
lopez s , cocco e , black j , et al : dual her2 / pik3ca targeting overcomes single - agent acquired resistance in her2 - amplified uterine serous carcinoma cell lines in vitro and in vivo . 
lee av , guler bl , sun x , et al : oestrogen receptor is a critical component required for insulinlike growth factor ( igf ) - mediated signalling and growth in mcf - 7 cells . 
lee av , cui x , oesterreich s : cross - talk among estrogen receptor , epidermal growth factor , and insulin - like growth factor signaling in breast cancer . 
thor ad , liu s , edgerton s , et al : activation ( tyrosine phosphorylation ) of erbb - 2 ( her - 2 / neu ) : a study of incidence and correlation with outcome in breast cancer . 
cicenas j , urban p , kng w , et al : phosphorylation of tyrosine 1248 - erbb2 measured by chemiluminescence - linked immunoassay is an independent predictor of poor prognosis in primary breast cancer patients . 
frogne t , laenkholm av , lyng mb , et al : determination of her2 phosphorylation at tyrosine 1221 / 1222 improves prediction of poor survival for breast cancer patients with hormone receptorpositive tumors . 
digiovanna mp , stern df , edgerton sm , et al : relationship of epidermal growth factor receptor expression to erbb - 2 signaling activity and prognosis in breast cancer patients . 
hudelist g , kstler wj , czerwenka k , et al : her - 2 / neu and egfr tyrosine kinase activation predict the efficacy of trastuzumab - based therapy in patients with metastatic breast cancer . 
wang f , wang s , wang z , et al : phosphorylated egfr expression may predict outcome of egfr - tkis therapy for the advanced nsclc patients with wild - type egfr . 
saal lh , johansson p , holm k , et al : poor prognosis in carcinoma is associated with a gene expression signature of aberrant pten tumor suppressor pathway activity . 
drury sc , detre s , leary a , et al : changes in breast cancer biomarkers in the igf1r / pi3k pathway in recurrent breast cancer after tamoxifen treatment . 
zhu hw , jiang d , xie zy , et al : effects of stathmin 1 silencing by sirna on sensitivity of esophageal cancer cells eca - 109 to paclitaxel . 
chakraborty a , hatzis c , digiovanna mp : co - targeting the her and igf / insulin receptor axis in breast cancer , with triple targeting with endocrine therapy for hormone - sensitive disease . 
lee cy , lin y , bratman sv , et al : neuregulin autocrine signaling promotes self - renewal of breast tumor - initiating cells by triggering her2 / her3 activation . 
arpino g , wiechmann l , osborne ck , et al : crosstalk between the estrogen receptor and the her tyrosine kinase receptor family : molecular mechanism and clinical implications for endocrine therapy resistance . 
song rx , barnes cj , zhang z , et al : the role of shc and insulin - like growth factor 1 receptor in mediating the translocation of estrogen receptor to the plasma membrane . 
pietras rj , arboleda j , reese dm , et al : her - 2 tyrosine kinase pathway targets estrogen receptor and promotes hormone - independent growth in human breast cancer cells . 
akbani r , becker kf , carragher n , et al : realizing the promise of reverse phase protein arrays for clinical , translational , and basic research : a workshop report : the rppa ( reverse phase protein array ) society . 
i - spy2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) schema for patients in the control and experimental therapy arms . 
 o undetectable ras - mutant clones in plasma : possible implication for anti - egfr therapy and prognosis in patients with ras - mutant metastatic colorectal cancer mohamed bouchahda , md1 - 4 ; raphael saffroy , phd5 ; abdoulaye karabou e , md2 , 6 ; jocelyne hamelin , phd5 ; pasquale innominato , md , phd2 , 7 , 8 ; faouzi saliba , md , phd9 ; francis l evi , md , phd1 , 2 , 8 ; nelly bosselut , md5 ; and antoinette lemoine , pharmd , phd5 purpose combining cetuximab with chemotherapy provides clinical benet to 60% of the patients with ras wild - type ( ras - wt ) metastatic colorectal cancer ( mcrc )  . 
the patients with raswt ctdna received cetuximab + uorouracil , leucovorin , and irinotecan ( folfiri ) , whereas those with ras - mt ctdna were treated with the oncologists choice of therapy . results of 16 registered patients , 11 were male and ve female . 
they were age 48 to 81 years , and they had unresectable metastatic adenocarcinoma from the colon ( n = 11 ) or rectum ( n = 5 ) , with a median of two metastatic sites . 
in the patients with wt ctdna , objective tumor response rate was 50.0% , including one complete response and four partial responses after a median number of 6 courses of cetuximab + folfiri ( range , 1 to 16 courses )  . 
this was particularly the case for the combination of cetuximab with uorouracil , leucovorin , and irinotecan ( folfiri ) or uorouracil , leucovorin , and oxaliplatin ( folfox ) .1 , 2 however , several studies have shown that the survival of those patients with tumor ras mutations ( ras - mt ) was shorter than for those with ras - wild - type ( ras - wt ) tumors.3 , 4 since 2014 , it has been recommended that only patients with ras - wt mcrc should receive an anti - egfr targeted agent.5 ras mutations have been found in 30% to 50% of patients with mcrc , 6 - 9 which makes these patients ineligible for egfr - targeted therapies . recent studies have demonstrated that the analysis of circulating tumor dna ( ctdna ) in blood samples , through its ability to recapitulate tumor heterogeneity , is a remarkable surrogate of tumor biopsy for detecting mutations.10 - 12 this technique has the advantage of being less invasive than a tissue biopsy and can be easily repeated over time . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue context key objective to determine whether the lack of ras mutation in a liquid biopsy supports the administration of an antiepidermal growth factor receptor ( egfr ) antibody , despite earlier documentation of a pathogenic ras mutation in the primary colorectal cancer ( crc )  . knowledge generated nearly half the patients in this pilot study received cetuximab - based chemotherapy , because no ras mutation was detected in the liquid biopsy , despite such mutations having been found in the primary tumor . 
the progression - free survival and the overall survival of these heavily pretreated patients largely exceeded those in patients whose liquid biopsy revealed ras mutation and who received chemotherapy only . relevance tracking the gain or loss of ras - mutated cancer clones through liquid biopsies along the course of crc disease may have a profound impact on its therapeutic management . 
this is achieved through enabling the administration of anti - egfr that was initially rejected on the basis of previous molecular testing of tissue . in the characterization of the dynamics of acquired resistance to anti - egfr therapies.13 to date , studies with liquid biopsy have been selectively focused on the early detection of the appearance of ras - mt clones in tumor deposits by analyzing ctdna in blood samples from patients with ras - wt primary crc13 as biomarkers of an increasing resistance to anti - egfr agents . 
indeed , no specication in the european marketing authorisation for cetuximab mentions that tumor ras testing should be determined on solid tumor tissue in order to allow for anti - egfr administration . 
this is also the case for the recommendations by the french high health authority regarding cetuximab use . all consecutive patients treated between august 2017 and february 2019 at one of three participating centers in france were screened for inclusion in this pilot study . 
inclusion required histologic or cytologic proof of colorectal adenocarcinoma , with a kirsten rat sarcoma viral oncogene homolog ( kras ) or neuroblastoma rat sarcoma viral oncogene homolog ( nras ) mutation ( nras - mt ) from a tissue biopsy . 
the massarray ultraseek procedure involves a 3 - step process consisting of the initial polyinactivation of unincorporated merase chain reaction , nucleotides by shrimp alkaline phosphatase , and a singlebase primer extension according to the manufacturers protocol . 
the products were then nano - dispensed onto a matrix - loaded silicon chip ( spectrochipii , agena bioscience ) , and the mutations were detected by matrixassisted laser desorption - ionizationtime of ight mass spectrometry . 
for our study , the sensitivity for the detection of clinically relevant ras gene mutations in ctdna was 88% for patients with crc liver metastases , in good agreement with bettegowda et al.16 we currently use these highly sensitive mass spectrometry ctdna analyses for monitoring treatment of patients with nonsmall - cell lung cancer or breast cancer in routine oncology practice . study treatment all patients had ras - mt tissue biopsies . 
the study population was divided in two groups according to the results of the ctdna mutational analysis : group 1 included the patients with ras - mt also found in plasma ; group 2 included the patients with ras - wt ctdna . 
the sum of the largest diameters of the target lesions was computed on the inclusion imaging and used as baseline for the quantication of tumor downsizing and response categorization according to recist . 
response was classied as complete response , partial response , stable , or progressive disease.15 statistical consideration this pilot exploratory study included consecutive patients , and no sample size was dened a priori . 
the durations of progression - free survival ( pfs ) and overall survival ( os ) were measured from inclusion until the date of progression or death , respectively , or that of last follow up , with the database locked on may 25 , 2019 . 
all analyses were performed with intentto - treat using spss v18.0 software ( spss , chicago , il )  . results patients sixteen patients with unresectable mcrc and ras - mt in a cancer tissue were registered at one of three centers in initial ras mutational status was dethis pilot study . termined in the resected primary tumor for 11 patients ( 69% ) or in a tumor biopsy for 5 patients ( 31% )  . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue two or more chemotherapy regimens for metastatic disease . two groups of patients were identied according to the results of ctdna mutational analysis at inclusion . 
group 1 received the investigators choice of chemotherapy regimens , which included bevacizumab + folfox for three patients , aibercept + folfiri for three patients , and regorafenib for one patient . 
baseline characteristics were similar in the 2 groups ( table 1 )  . safety data for the nine patients with ctdna ras - wt ( group 2 ) overall , the cetuximab + folfiri regimen was well tolerated . 
the main grade 1 or 2 clinical toxicities were fatigue , diarrhea , nausea or vomiting , mucositis , acneiform rash , and alopecia ( 6 [ 67% ] of 9 for all )  . 
this fourth - line protocol was well tolerated , with the most severe toxicities being grade 2 leukopenia , neutropenia , fatigue , and acneiform rash . discussion the patients in this study had advanced and chemotherapy - resistant metastatic disease , without any imbalance in apparent overall tumor burden that could reasonably inuence the liquid biopsy results . 
thus , no evidence supports the possibility that the differences in detection of ctdna ras mutation would be related to between - patient variations in tumor burden . the identication of a mutation in kras or nras from a cancer tissue biopsy precludes the use of anti - egfr treatment in association with chemotherapy against mcrc , based on consistent evidence.5 our group rst reported the occurrence of acquired kras mutations along the progression of colorectal metastases in patients treated with cetuximab . 
we then hypothesized that the late acquisition of kras mutations could represent a possible mechanism of secondary resistance to anti - egfr antibodies.18 however , the assumption of persisting ras - mt genotype for patients who received chemotherapy has not been challenged before now because of the expected evolutionary advantage of ras - mt clones.19 yet in this pilot study , we found that nearly half the patients with mcrc displayed no detectable ras - mt in ctdna , although their cancer tissue genotyping had demonstrated ras - mt . 
this nding raised several questions . first , is there a concordance between the ras mutational status of tumor tissues and that of ctdna ? several studies have highlighted discrepant results in ras mutational status for 10% - 15% of the patients tested , depending on the method used.11 , 14 , 20 vidal et al explained such plasmaversus - tissue ras discrepancies with spiral and temporal heterogeneity in ras - mt tumor clones within the tumor tissue.11 according to thierry et al , 20 such discrepancies could relate to the use of biopsies . 
other discrepancies that seemed to affect concordance were long intervals between assessments of the ras status in tumor tissue and that in the blood sample , resection of the tumor at the time of blood draw , tissue analyzed . grasselli et al14 ascribed the discrepancies in ras status to differences in technical sensitivity of the methods used for analysis or to heterogeneity . tumor site , and type of second , is there a change in ras status over time and / or during treatment ? this question does not yet have a clear answer . 
we were the rst to report 1 case of acquired kras mutation in metastases after progression under combined anti - egfr and doublet chemotherapy in 12 patients with kras - wt mcrc.18 other authors have highlighted the concurrent detection of sensitive and resistant clones to anti - egfr antibodies within tumor deposits from different locations in the same patient.21 - 24 this multiclonality could explain the dissociated antitumor responses that are frequently encountered in clinical practice . 
such tumor heterogeneity assumes the existence of wt clones sensitive to anti - egfr treatment alongside resistant mutant clones . interestingly , the team of raimondi et al25 recently reported the disappearance of ras - mt clones in ctdna after tumor progression while receiving bevacizumab and chemotherapy in 4 patients with ras - mt mcrc . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue feb 19 , 2019 before cetux + folfiri may 29 , 2019 after 6 courses sept 19 , 2019 after 12 courses target lesion target lesion target lesion fig 4 . 
case report illustrating exceptional efcacy of cetuximab + uorouracil , leucovorin , and irinotecan ( cetux + folfiri ) as fourth - line chemotherapy received by a 72 - year - old patient with kras mutation in tumor tissue but kras wild - type in liquid biopsy , upon inclusion in the study . 
indeed , the observed median pfs and os in these patients were similar to those reported for patients with ras - wt tumor tissue who received this combination as rst - line treatment for mcrc . 
our internal steering committee proposed to stop the pilot study , once the information was adequate for designing a randomized trial for testing the hypothesis further on the basis of an apparent three - fold increase in the median pfs of the experimental treatment compared with cetuximab - free chemotherapy . the intriguing and encouraging results of this exploratory trial need to be conrmed in randomized clinical trials . such validation steps are particularly relevant because all our patients with ras - wt ctdna received cetuximab ; thus , we cannot differentiate between a prognostic and a predictive role of ras - wt ctdna for outcomes of patients receiving cetuximab - based chemotherapy . 
 bouchahda et al than prognostic of an aggressive tumor biology.34 such consideration would further support the hypothesis of an added benet from cetuximab in this subgroup of patients . yet recent evidence suggests that the proportion of ras - mt in ctdna was a prognostic indicator for both os and pfs in patients with mcrc.35 this nding raised the question of a potential divide on the clinical signicance between tumor and ctdna genotyping , which this study cannot respond to . 
the fact that orrs exceeded 40% and were similar in both treatment groups suggested that all the patients included in the study were not completely resistant to chemotherapy and that those with ras - mt in the liquid biopsy could have a worse prognosis , as proposed by elz et al.35 however , single - agent cetuximab achieved only a 10% orr in patients with chemotherapy refractory mcrc , 36 despite prolonging pfs by 4 months . 
taken together , the literature results support a much greater value for pfs prolongation compared with orr as an efcacy end point , which supports the hypothesis that the liquid biopsy results have a predictive value . the lack of a prespecied sample size and the low number of patients in each group constitute the main limitations of our pilot salvage study . 
the three - fold increase in median pfs in the absence of any apparent bias does suggest that antiegfrbased chemotherapy could represent a promising option for nearly half the patients with initially documented ras - mt on tumor tissue at a later stage of their disease . our study was in line with the chronos study ( clinicaltrials.gov identier : nct03227926 ) , 37 whose design is based on the concept that crc genome adapts dynamically to intermittent anti - egfr drug schedules . 
a follow - up on our study would involve a randomized clinical trial in which eligible patients with ras - mt on solid tumor tissue undergo ras mutational status assessment in ctdna upon progression on chemotherapy . 
 anti - egfr therapy for ctdna ras - wt despite ras - mt in tumor tissue references venook ap , niedzwiecki d , lenz hj , et al : effect of rst - line chemotherapy combined with cetuximab or bevacizumab on overall survival in patients with kras wild - type advanced or metastatic colorectal cancer : a randomized clinical trial . 
jama 317 : 2392 - 2401 , 2017 tejpar s , stintzing s , ciardiello f , et al : prognostic and predictive relevance of primary tumor location in patients with ras wild - type metastatic colorectal cancer : retrospective analyses of the crystal and fire - 3 trials . 
modest dp , ricard i , heinemann v , et al : outcome according to kras - , nrasand braf - mutation as well as kras mutation variants : pooled analysis of ve randomized trials in metastatic colorectal cancer by the aio colorectal cancer study group . 
ann oncol 27 : 1746 - 1753 , 2016 de roock w , claes b , bernasconi d , et al : effects of kras , braf , nras , and pik3ca mutations on the efcacy of cetuximab plus chemotherapy in chemotherapy - refractory metastatic colorectal cancer : a retrospective consortium analysis . 
lancet oncol 11 : 753 - 762 , 2010 van cutsem e , cervantes a , nordlinger b , et al : metastatic colorectal cancer : esmo clinical practice guidelines for diagnosis , treatment and follow - up . 
ann oncol 25 : iii1 - iii9 , 2014 douillard jy , oliner ks , siena s , et al : panitumumab - folfox4 treatment and ras mutations in colorectal cancer . 
heinemann v , von weikersthal lf , decker t , et al : folfiri plus cetuximab versus folfiri plus bevacizumab as rst - line treatment for patients with metastatic colorectal cancer ( fire - 3 ) : a randomised , open - label , phase 3 trial . 
lancet oncol 15 : 1065 - 1075 , 2014 van cutsem e , lenz hj , k ohne ch , et al : fluorouracil , leucovorin , and irinotecan plus cetuximab treatment and ras mutations in colorectal cancer . 
j clin oncol 33 : 692 - 700 , 2015 peeters m , kafatos g , taylor a , et al : prevalence of ras mutations and individual variation patterns among patients with metastatic colorectal cancer : a pooled analysis of randomised controlled trials . 
vidal j , muinelo l , dalmases a , et al : plasma ctdna ras mutation analysis for the diagnosis and treatment monitoring of metastatic colorectal cancer patients . ann oncol 28 : 1325 - 1332 , 2017 12 . 
grasselli j , elez e , carat `u g , et al : concordance of bloodand tumor - based detection of ras mutations to guide anti - egfr therapy in metastatic colorectal cancer . 
bouchahda m , macarulla t , liedo g , et al : feasibility of cetuximab given with a simplied schedule every 2 weeks in advanced colorectal cancer : a multicenter , retrospective analysis . 
lacina l , coma m , dvor ankov a b , et al : evolution of cancer progression in the context of darwinisanticancer res 39 : 1 - 16 , 2019 20 . 
thierry ar , el messaoudi s , mollevi c , et al : clinical utility of circulating dna analysis for rapid detection of actionable mutations to select metastatic colorectal patients for anti - egfr treatment . 
raimondi c , nicolazzo c , belardinilli f , et al : transient disappearance of ras mutant clones in plasma : a counterintuitive clinical use of egfr inhibitors in ras mutant metastatic colorectal cancer . 
zhou m , yu p , hou k , et al : effect of ras status on anti - egfr monoclonal antibodies + 5 - fu infusion - based chemotherapy in rst - line treatment of metastatic colorectal cancer : a meta - analysis . 
giantonio bj , catalano pj , meropol nj , et al : bevacizumab in combination with oxaliplatin , uorouracil , and leucovorin ( folfox4 ) for previously treated metastatic colorectal cancer : results from the eastern cooperative oncology group study e3200 . 
van cutsem e , tabernero j , lakomy r , et al : addition of aibercept to uorouracil , leucovorin , and irinotecan improves survival in a phase iii randomized trial in patients with metastatic colorectal cancer previously treated with an oxaliplatin - based regimen . 
tabernero j , yoshino t , cohn al , et al : ramucirumab versus placebo in combination with second - line folfiri in patients with metastatic colorectal carcinoma that progressed during or after rst - line therapy with bevacizumab , oxaliplatin , and a uoropyrimidine ( raise ) : a randomised , double - blind , multicentre , phase 3 study . 
sobrero af , maurel j , fehrenbacher l , et al : epic : phase iii trial of cetuximab plus irinotecan after uoropyrimidine and oxaliplatin failure in patients with metastatic colorectal cancer . 
peeters m , oliner ks , price tj , et al : analysis of kras / nras mutations in a phase iii study of panitumumab with folfiri compared with folfiri alone as second - line treatment for metastatic colorectal cancer . 
de stefano a , rosanova m , malapelle u , et al : discordance in ras mutations between primary colon tumor and metastases : a real event or a matter of methodology ? int j biol markers 32 : e474 - e477 , 2017 34 . 
elez e , chianese c , sanz - garca e , et al : impact of circulating tumor dna mutant allele fraction on prognosis in ras - mutant metastatic colorectal cancer . 
siena s , bardelli a , sartore - bianchi a , et al : exploiting clonal evolution and liquid biopsy to overcome resistance to anti - egfr treatment in metastatic colorectal cancer : the chronos trial . 
lolkema1 introduction the vhl gene is a tumor suppressor gene located at chromosome 3p25 , 1 and its protein has multiple functions linked to multiple effector proteins.2 aberrations in the vhl gene are associated with sporadic clear cell renal cell carcinomas ( ccrccs ) , sporadic hemangioblastomas , pheochromocytomas , pancreatic islet cell tumors , endolymphatic sac tumors , and benign cysts affecting various organs.3 germline inthe vhl gene causes the autosomal activation of dominant von hippel - lindau ( vhl ) syndrome . 
vhl is rarely mutated outside of the context of rcc or vhl syndromeassociated malignancies.4 biallelic vhl inactivation caused by genetic and epigenetic alterations ( including dna methylation , histone modications , and coincidental loss of genes localized adjacent to the vhl chromosome locus ) has been described.2 in both hereditary and sporadic tumors , vhl mutations are heterogeneous.5 the encoded vhl protein ( pvhl ) plays an important role in ubiquitination and proteosomal degradation of hypoxia inducible factor - 1 ( hif - 1 )  . 
our aim was to investigate the ( epi ) genetic background of this patients disease and to determine whether the identied vhl mutation could be a driving mutation in this patients fdcs . methods case report in 2013 , a 29 - year - old female patient presented with a large abdominally located mass and multiple hepatic lesions . 
a histologic biopsy from a liver lesion showed an epithelioid and spindle cell malignant neoplasm with scattered lymphocytes . immunohistochemistry ( ihc ) results matched the pattern of fdcs with exfollicular dendritic cell markers cd21 , pression of cd23 , and cd359 ( fig 1a - c )  . 
on the basis of radiologic diagnosis , the pattern did not t an rcc . this was further supported by a negative paired box gene 8 ( pax8 ) ihc result ( fig 1d )  . the clinical course of our patients disease is outlined in figure 2 . 
the second - line treatment was pazopanib , which resulted in unexpected stable disease for 22 months . rendering additional the patient participated in the dutch national center for personalized cancer treatment ( cpct ) - 02 program , 10 tumor sampling for whole - genome sequencing ( wgs ) analysis before and after treatment with pazopanib . 
wgs was performed on the illumina hiseq x platform with 100 ng dna as input using standard protocols ( pairedend 2 150 base pairs ; illumina , san diego , ca )  . within the framework of cpct - 02 , all germline variants are ltered , which guarantees that only somatic variants are reported . 
hif - 1 ihc showed positive nuclear staining ( e ) , and glucose transporter 1 ( glut1 ) ihc showed positive staining ( f )  . results genomic landscape the identied c.119delc vhl frameshift mutation led to a truncated pvhl ( p.pro40fs ; fig 4 )  . 
both biopsies showed genome - wide aberrations , with large chromosomal copy number alterations , structural rearrangements , and mutations in a broad spectrum of loci ( fig 5 )  . 
the patient received eight cycles of chop ( cyclophosphamide , doxorubicin , vincristine , prednisone ) , which resulted 6 months later ( t6 ) in metabolic complete remission ( cr )  . 
after that ( t36 ) , the patient showed pd and participated in a phase 1 trial with immunotherapy ( cd40 agonistic monoclonal antibody ) in combination with vanucizumab ( anti - angiopoietin - 2 and anti - vegf [ vascular endothelial growth factor ] ) for 11 months . 
both results provide circumstantial evidence for functional loss of pvhl.7 , 10 discussion our analysis revealed a unique patient with fdcs harboring a somatic functional vhl aberration , which is the rst description of a vhl mutation in sarcoma.14 because fdcs is a rare mesenchymal neoplasm with a largely unknown and rather complex genetic landscape15 and is unknown for harboring vhl aberrations , we veried specic ihcbased markers to conrm the diagnosis and to reject metastatic rcc ( mrcc ) as an alternative diagnosis . 
the positive hif - 1 ihc result may indicate a functional loss of pvhl ; in this patient , it was a consequence of mutation and potential methylation - derived changes leading to biallelic vhl gene inactivation . 
although most evidence in fdcs has been found for the involvement of the ras / raf signaling pathway , 16 , 17 we did not identify mitogen - activated protein kinase ( mapk ) alterations in our patient . 
a mutant allele - specic imbalance as a consequence of allele - specic amplication has been described.18 , 19 however , this seems to be a more common aspect with activating mutations . 
recurrent vhl locus amplications have not been described in ccrcc ; therefore , it does not seem to be a common aberration . however , these reports did not specically investigate post - tyrosine kinase samples.2 , 20 , 21 numerous nonspecic chromosomal translocations were present in the pretreatment biopsy , with a remarkable decline in the number of structural variants ( svs ) following treatment with pazopanib . 
treatment of cancer may have an inuence on involved processes and subsequently on patterns and frequency of svs.22 alterations in the number of svs between time points in a patients malignancy may also be a consequence of tumor evolution and selective survival of subclonal populations as a result of the selective pressure of treatment , similar to variable somatic alterations that cause the emergence of drug resistance.23 the changes in the genomic landscape between the two biopsies obtained in our patient could be associated with the observed disease response during treatment with pazopanib.24 moreover , the fact that the mutated vhl gene has been amplied in our patients disease over time emphasizes its importance and potential as a driver mutation . upregulated vegf is associated with the hif pathway . 
pazopanib , a multikinase inhibitor with activity against the vegf receptor and platelet - derived growth factor and receptors , is effective in the treatment of mrcc25 and metastatic sarcoma.26 during treatment with pazopanib , our patient had stable disease for 22 months . 
in march 2016 , progressive disease was revealed on a conventional ct scan ( a ) and on a positron emission tomography scan ( b ) before the start of treatment with pazopanib . 
untranslated regions ( utr ) and exonic regions are depicted by rectangular boxes ( colored dark blue and dark gold , respectively ) , and intronic regions are depicted by black lines . 
 ( c ) protein sequences of wild - type ( wt ) pvhl and mutant pvhl , colored by protein domains ; ( gxeex ) 8 is shown in light blue , - domain in light gold , and - domain in red . 
 ( the vhl gene model is on the basis of ensembl transcript nm_000551.2 and the protein model is on the basis of the uniprotkb p40337 entry . ) red asterisk indicates stop codon . 
moreover , saygin et al27 performed a pooled analysis of data from 462 patients with fdcs , showing a median survival for patients with metastatic disease of 9 months ( range , 0.25 to 72 months ) and a 2 - year survival rate of 15.8% ; these results suggest that the long pfs is not the result of better prognostic features of fdcs . 
the relatively long pfs during our patients last treatment , which consisted of the combination of a cd40 agonistic monoclonal antibody and an antiangiopoietin - 2 and anti - vegf bispecic monoclonal antibody , could possibly be explained by the effect of the latter drug ( vanucizumab )  . 
these data imply that the vhl mutation in our patient may predict a biologic behavior more similar to mrcc than to a metastatic sarcoma in response to treatment with pazopanib . 
these ndings are not sufcient to make an argument for vegf - targeted therapies in fdcs , because this is the rst case of a vhl - mutated fdcs as far as we know . indirect evidence for pvhl functional although hif stabilization and glut1 accumulation are , at the most , loss , a limitation of this case report is the absence of methylation analysis looking further into epigenetic silencing of the vhl gene . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . florence atra travel , accommodations , expenses : abbvie , astellas pharma paul j . 
van diest consulting or advisory role : panterhei ( inst ) patents , royalties , other intellectual property : ddx3 as a biomarker for cancer and methods related thereto ( inst ) geert j.l.h. 
we thank hartwig medical foundation for providing wholegenome sequencing data and for performing analysis of these data . moreover , this patient was entered into the center for personalized cancer treatment ( cpct ) - 02 study . 
medicine ( baltimore ) 76 : 381 - 391 , 1997 lawrence ms , stojanov p , mermel ch , et al : discovery and saturation analysis of cancer genes across 21 tumour types . 
annu rev pathol 10 : 263 - 289 , 2015 greijer ae , van der groep p , kemming d , et al : up - regulation of gene expression by hypoxia is mediated predominantly by hypoxia - inducible factor 1 ( hif - 1 )  . j pathol 206 : 291 - 304 , 2005 lymphoproliferative disorders associated with immune deciencies and histiocytic and dendritic cell neoplasms , in wahed a and dasgupta a : hematology and coagulation : a comprehensive review for board preparation , certication and clinical practice . 
center for personalized cancer treatment : development of a platform for next - generation dna sequencing based personalized treatment for cancer patients : protocol to obtain biopsies from patients with locally advanced or metastatic cancer ( cpct 02 biopsy protocol )  . 
chen x , schulz - trieglaff o , shaw r , et al : manta : rapid detection of structural variants and indels for germline and cancer sequencing applications . bioinformatics 32 : 1220 - 1222 , 2016 iliopoulos o , levy ap , jiang c , et al : negative regulation of hypoxia - inducible genes by the von hippel - lindau proteproc natl acad sci usa 93 : 10595 - 10599 , 1996 14 . 
soh j , okumura n , lockwood ww , et al : oncogene mutations , copy number gains and mutant allele specic imbalance ( masi ) frequently occur together in tumor cells . 
beroukhim r , brunet jp , di napoli a , et al : patterns of gene expression and copy - number alterations in von - hippel lindau disease - associated and sporadic clear cell carcinoma of the kidney . 
van allen em , wagle n , stojanov p , et al : whole - exome sequencing and clinical interpretation of formalin - xed , parafn - embedded tumor samples to guide amsterdam , netherlands , elsevier , 2013 , pp 39 - 71 precision cancer medicine . 
borad mj , champion md , egan jb , et al : integrated genomic characterization reveals novel , therapeutically relevant drug targets in fgfr and egfr pathways in sporadic intrahepatic cholangiocarcinoma . 
j pathol 221 : 125 - 138 , 2010 van der graaf wt , blay jy , chawla sp , et al : pazopanib for metastatic soft - tissue sarcoma ( palette ) : a randomised , double - blind , placebo - controlled phase 3 trial . 
morgan , md1 , 2 purpose using nonenrichment - based , potentially more sensitive epic sciences circulating tumor cell ( ctc ) platform , we sought to detect and characterize ctcs in untreated , high - risk localized prostate cancer and to evaluate their clinical implication . methods between 2012 and 2015 , blood samples were prospectively collected from patients with national comprehensive cancer network high - risk localized prostate cancer undergoing either radiotherapy ( xrt ) plus androgen deprivation therapy or radical prostatectomy ( rp ) with curative intent . 
samples were analyzed with the epic sciences platform with 4 ( cid : 1 ) , 6 - diamidino - 2 - phenylindole , cd45 , cytokeratin ( ck ) , and androgen receptor ( ar ) n - terminal staining . 
bcr occurred more frequently in the rp group than xrt ( 15 of 26 v one of 19 ) , with most patients in the xrt group continuing to receive androgen deprivation therapy . 
2019 by american society of clinical oncology introduction the existence of disseminated tumor cells detectable in the blood or bone marrow of men with clinically localized prostate cancer has long been known.1 - 4 yet , molecular characterization of these cells in the localized setting has remained elusive because of the extremely low ratio of tumor to normal cells in circulation . 
with recent advances in molecular imaging , we now know that many men with clinically localized disease have positron emission tomographyvisible metastatic disease , 5 - 9 yet these modalities are expensive and may only detect lesions consisting of at least several million tumor cells . 
additional methods of detecting otherwise occult , disseminated disease are still needed , because these may inform primary treatment decisions such as the use of systemic therapy . circulating tumor cells ( ctcs ) may provide an approach for identifying men with micrometastatic disease at the time of diagnosis . 
 salami et al context key objective to determine if circulating tumor cells ( ctcs ) can predict treatment response in high - risk localized prostate cancer . knowledge generated phenotypic and genomic features of ctcs may predict biochemical recurrence in high - risk localized prostate cancer . 
individual ctcs can be sequenced in this setting , conrming their tumor origin . relevance detection and characterization of ctcs may facilitate identication of patients with high - risk prostate cancer who could benet from multimodal therapy . in the advanced prostate cancer setting , the identication and characterization of ctcs is now poised to help guide appropriate treatment selection , because detection of the ar - v7 splice variant in ctcs predicts resistance to second - generation antiandrogens in men with metastatic castration - resistant prostate cancer ( mcrpc ) .10 - 12 previous efforts to reliably detect and analyze ctcs in localized prostate cancer , however , have not led to clinically useful assays because of the low clinical sensitivity and challenges associated with characterizing the individual detected ctcs.13 - 23 in men with mcrpc , a high - throughput digital imaging approach has been shown to increase the sensitivity of ctc detection while also providing additional molecular and morphologic granularity at the single - cell level.24 - 26 this same approach may offer one avenue to improving the sensitivity and clinical implications of ctc detection in the localized disease setting . 
adt , androgen deprivation therapy ; ctc , circulating tumor cell ; rp , radical prostatectomy ; xrt , radiation therapy . methods cohort description after institutional review board approval , we conducted a prospective study of 49 patients ( fig 1 ) with untreated national comprehensive cancer network ( nccn ) dened high - risk prostate cancer.27 these men had at least one of the following : grade group 4 or 5 disease , prostate - specic antigen ( psa ) greater than 20 , and / or clinical stage t2c or greater . 
all patients completed bone scans and computerized tomography ( ct ) scans of the abdomen and pelvis demonstrating no evidence of metastatic disease before undergoing local therapy ( either radiotherapy [ xrt ] plus androgen deprivation therapy [ adt ] or radical prostatectomy [ rp ] ) with curative intent . 
the samples were analyzed with the epic sciences ctc platform ( epic sciences , san diego , ca ) , which uses an enrichment - free approach to ctc detection , with all nucleated cells analyzed on a glass slide using digital pathology . 
 ( % ) unless otherwise noted . abbreviations : bcr , biochemical recurrence , bmi , body mass index ; n / a , not applicable ; psa , prostate - specic antigen ; rp , radical prostatectomy . subtypes inclusive of ck - negative ctcs , ctc clusters , and apoptotic ctcs ( fragmented nuclei ) .28 additional parameters included cell size , shape , nuclear area , and presence of macronucleoli , along with ar expression , uniformity , and cellular localization . 
ctc phenotypic heterogeneity was quantied using the shannon index , as previously described.29 samples from four patients failed quality control testing , leaving a nal analyzable cohort size of 45 patients ( fig 1 )  . single - cell whole - genome sequencing and copy number variation analysis single ctc copy number variation ( cnv ) analysis based on low - pass whole - genome sequencing was performed as previously described.30 , 31 briey , individual ctcs were isolated from the slides , dropped into eppendorf tubes , and whole - genome amplied using seqplex enhanced dna amplication kit from sigma ( sigma aldrich , st louis , mo )  . 
amplied dna was used for library construction using nebnext ultra dna library prep kit for illumina ( new england biolabs , ipswich , ma ) and 2 150 pairedend sequencing was performed using illumina nextsequation 500 sequencer . 
dna cnvs were determined using an existing , standardized single - cell cnv analysis pipeline.30 data collection and statistical analyses we tracked relevant demographic , clinical , and pathologic data for each patient and entered all data into a secure electronic health insurance portability and accountability actcompliant database . 
a diversity of ctc subtypes was detected , including arpositive cells , ck - positive cells , ck - negative ctcs , 28 and clusters of ctcs ( fig 2a )  . 
ctcs with detectable ar expression were observed in 24.4% ( 11 of 45 ) of the cohort . compared with patients who underwent xrt , those who underwent rp had a higher rate of bcr ( 15 of 26 v one of 19 ; p , .001 ) , although most patients in the xrt group continued receiving adt . 
 ( b ) comparison of total ctc / ml of blood , presence of androgen receptor ( ar ) positive ctcs , ctc phenotypic heterogeneity or shannon index ( si ) , metastases , and bcr for each patient . 
 ( c ) association of bcr and development of radical metastases after prostatectomy to total ctc / ml , ar - positive ctc / ml , and ctc phenotypic heterogeneity . 
all of the patients who underwent rp and xrt who experienced metastasis ( to bone , regional lymph nodes , and abdominal viscera ) during follow - up were preceded by bcr . 
patients experiencing bcr had signicantly greater numbers of arpositive ctcs , and patients developing metastases had signicantly more total ctcs and ar - positive ctcs ( figs 2b and 2c )  . single - cell sequencing and morphology analysis of all detected ctcs was performed on patient 252 , who had the highest ctc count in the rp group ( 4.7 ctcs / ml of blood )  . 
single - cell sequencing results identied genomic aberrations consistent with malignant origin in six ( 46% ) of the 13 ctcs sequenced ( fig 3b )  . moreover , heterogeneous genomic proles were observed in these six ctcs . 
pten loss was detected in this ctc akin to those ctcs found in patients with mcrpc previously analyzed with similar methodology.24 , 29 two ctcs had 12p loss and 22q loss ( prole b ) ; both of these alterations have been reported in this study , we detected ctcs in more than two - thirds of patients , demonstrating the feasibility of detecting and characterizing ctc morphology and genomics in men with localized prostate cancer . 
oncologic end points were not evaluable in this time frame for patients who underwent radiotherapy , because most of these patients continued to receive adt . various liquid biopsy approaches have been interrogated in the past for risk stratifying patients with apparent clinically localized prostate cancer with varying success . 
for example , reverse transcriptase polymerase chain reaction assay for psa , 34 - 36 an indirect approach to detect psaexpressing cells in circulation , demonstrated no signicant advantage in preoperative staging of prostate cancer . similarly , recent approaches to identifying prostate cancer ctcs have widely varied in their capacity to detect ctcs in men with localized disease.13 - 23 , 37 , 38 thus , unlike in metastatic disease , where ctc number is associated with survival , the clinical or prognostic relevance of ctc detection in localized prostate cancer remains unclear . 
this stands in contrast to other tumor types , where the detection of ctcs in localized disease is considered prognostic.39 , 40 there are a number of existing , tissue - based molecular markers for risk stratication in prostate cancer ; therefore , a key question is whether the molecular information obtained through analysis of ctcs could have any clinical relevance beyond tissue - based approaches.41 - 44 yet , prostate cancer is characterized by tumor multifocality as well as intraand interfocal genomic and transcriptomic heterogeneity , which may affect the clinical performance of tests assessing a single tumor focus.45 - 49 similarly , metastatic prostate cancer , ctcs are diverse in their phenotypic appearance and genomic makeup.29 a liquid biopsy approach may provide one avenue for addressing tumor heterogeneity and biopsy under - sampling by allowing a broader sample of potentially clinically signicant tumor cells . in line with this hypothesis , we observed signicant phenotypic diversity within the same patient and from patient to patient in our cohort of men with untreated high - risk localized prostate cancer . 
this molecular information could allow for clinical utility related to risk stratication and prediction of treatment response . the role for molecular diagnostics in localized prostate cancer continues to evolve and now also includes advanced molecular imaging techniques.5 - 9 the ultimate goal is the prediction and / or identication of early metastatic disease to guide improved treatment and long - term oncologic outcomes . 
compared with men who underwent radical prostatectomy , we observed a relatively lower rate of bcr in men who received radiation therapy , likely due to the effect of adt in this subgroup . 
furthermore , the phenotypic and genomic make - up of ctcs may provide additional prognostic and predictive information . to our knowledge , the current study is the rst to characterize ctcs at the combined protein and whole - genome single - cell level in localized prostate cancer . 
before routine clinical implementation , larger studies with longer follow - up are needed to validate our ndings and further investigate the association between ctc proles and the likelihood of subsequent metastasis . 
third , we did not measure ctcs intraor postoperatively to account for the impact of surgery on ctc count or evaluate the clearance of ctcs after surgery . in this study , we demonstrate that ctcs are not only detectable but also can be further proled in men with localized high - risk prostate cancer . 
the association of ctc subtypes , including those with high ar protein expression , with bcr and metastases suggests that characterization of ctcs may provide useful information for risk stratication and the need for multimodal therapy . 
palapattu stock and other ownership interests : nantkwest consulting or advisory role : janssen scientic affairs research funding : minomic patents , royalties , other intellectual property : implantable nanotechnology for long - term testosterone delivery functionalized ducial marker for drug delivery brent k . 
 salami et al ryon graf employment : epic sciences research funding : epic sciences travel , accommodations , expenses : epic sciences jessica louw employment : epic sciences , epic sciences ( i ) , navican genomics stock and other ownership interests : navican genomics travel , accommodations , expenses : navican genomics adam jendrisak employment : epic sciences stock and other ownership interests : epic sciences research funding : epic sciences lyndsey dugan employment : navican genomics , human longevity stock and other ownership interests : navican genomics consulting or advisory role : human longevity ( inst ) , chromacode yipeng wang employment : epic sciences stock and other ownership interests : epic sciences scott a . 
tomlins employment : strata oncology leadership : strata oncology stock and other ownership interests : strata oncology consulting or advisory role : abbvie , janssen , astellas medivation , strata oncology , sano , almac diagnostics research funding : astellas medivation ( inst ) , genomedx ( inst ) patents , royalties , other intellectual property : i am a coauthor on a patent issued to the university of michigan on ets gene fusions in prostate cancer . 
the diagnostic eld of use has been licensed to hologic / genprobe , who has sublicensed some rights to ventana medical systems / roche . travel , accommodations , expenses : strata oncology ryan dittamore employment : epic sciences leadership : epic sciences stock and other ownership interests : epic sciences patents , royalties , other intellectual property : patents pending felix y . 
feng leadership : pfs genomics stock and other ownership interests : pfs genomics consulting or advisory role : dendreon , emd serono , janssen oncology , ferring pharmaceuticals , sano , bayer , blue earth diagnostics , celgene , medivation / astellas research funding : zenith epigenetics patents , royalties , other intellectual property : i helped develop a molecular signature to predict radiation resistance in breast cancer , and this signature was patented by the university of michigan , my employer . 
morgan consulting or advisory role : myriad genetics , terumobct research funding : myriad genetics ( inst ) , mdxhealth ( inst ) , genomedx ( inst ) no other potential conicts of interest were reported . references ch ery l , lam hm , coleman i , et al : characterization of single disseminated prostate cancer cells reveals tumor cell heterogeneity and identies dormancy associated pathways . 
oncotarget 5 : 9939 - 9951 , 2014 todenh ofer t , hennenlotter j , faber f , et al : signicance of apoptotic and non - apoptotic disseminated tumor cells in the bone marrow of patients with clinically localized prostate cancer . 
prostate 75 : 637 - 645 , 2015 lilleby w , stensvold a , mills ig , et al : disseminated tumor cells and their prognostic signicance in nonmetastatic prostate cancer patients . 
morgan tm , lange ph , porter mp , et al : disseminated tumor cells in prostate cancer patients after radical prostatectomy and without evidence of disease predicts biochemical recurrence . 
oncotarget 8 : 84180 - 84192 , 2017 selns km , kr uger - stokke b , elschot m , et al : 18f - fluciclovine pet / mri for preoperative lymph node staging in high - risk prostate cancer patients . 
eur radiol 28 : 3151 - 3159 , 2018 bauman g , martin p , thiessen jd , et al : [ 18f ] - dcfpyl positron emission tomography / magnetic resonance imaging for localization of dominant intraprostatic foci : first experience . 
eur urol focus 4 : 702 - 706 , 2016 schmuck s , von klot ca , henkenberens c , et al : initial experience with volumetric 68ga - psma i&t pet / ct for assessment of whole - body tumor burden as a quantitative imaging biomarker in patients with prostate cancer . 
scher hi , graf rp , schreiber na , et al : nuclear - specic ar - v7 protein localization is necessary to guide treatment selection in metastatic castration - resistant prostate cancer . 
scher hi , graf rp , schreiber na , et al : assessment of the validity of nuclear - localized androgen receptor splice variant 7 in circulating tumor cells as a predictive biomarker for castration - resistant prostate cancer . 
scher hi , lu d , schreiber na , et al : association of ar - v7 on circulating tumor cells as a treatment - specic biomarker with outcomes and survival in castration13 . 
meyer cp , pantel k , tennstedt p , et al : limited prognostic value of preoperative circulating tumor cells for early biochemical recurrence in patients with localized resistant prostate cancer . 
shao c , liao cp , hu p , et al : detection of live circulating tumor cells by a class of near - infrared heptamethine carbocyanine dyes in patients with localized and metastatic prostate cancer . 
davis jw , nakanishi h , kumar vs , et al : circulating tumor cells in peripheral blood samples from patients with increased serum prostate specic antigen : initial results in early prostate cancer . 
kauffman ec , lee mj , alarcon sv , et al : lack of impact of robotic assisted laparoscopic radical prostatectomy on intraoperative levels of prostate cancer 100 : 608 - 610 , 2009 circulating tumor cells . 
punnoose ea , ferraldeschi r , szafer - glusman e , et al : pten loss in circulating tumour cells correlates with pten loss in fresh tumour tissue from castrationresistant prostate cancer patients . 
werner sl , graf rp , landers m , et al : analytical validation and capabilities of the epic ctc platform : enrichment - free circulating tumour cell detection and characterization . 
scher hi , graf rp , schreiber na , et al : phenotypic heterogeneity of circulating tumor cells informs clinical decisions between ar signaling inhibitors and taxanes in metastatic prostate cancer . 
anantharaman a , friedlander t , lu d , et al : programmed death - ligand 1 ( pd - l1 ) characterization of circulating tumor cells ( ctcs ) in muscle invasive and variation analysis . 
urology 43 : 765 - 775 , 1994 ignatoff jm , oefelein mg , watkin w , et al : prostate specic antigen reverse transcriptase - polymerase chain reaction assay in preoperative staging of prostate cancer . 
shariat sf , gottenger e , nguyen c , et al : preoperative blood reverse transcriptase - pcr assays for prostate - specic antigen and human glandular kallikrein for prediction of prostate cancer progression after radical prostatectomy . 
helo p , cronin am , danila dc , et al : circulating prostate tumor cells detected by reverse transcription - pcr in men with localized or castration - refractory prostate cancer : concordance with cellsearch assay and association with bone metastases and with survival . 
erho n , crisan a , vergara ia , et al : discovery and validation of a prostate cancer genomic classier that predicts early metastasis following radical prostatectomy . dju066 , 2014 118 : 3072 - 3077 , 2006 plos one 8 : e66855 , 2013 42 . 
cuzick j , swanson gp , fisher g , et al : prognostic value of an rna expression signature derived from cell cycle proliferation genes in patients with prostate cancer : a retrospective study . 
cuzick j , berney dm , fisher g , et al : prognostic value of a cell cycle progression signature for prostate cancer death in a conservatively managed needle biopsy cohort . 
klein ea , cooperberg mr , magi - galluzzi c , et al : a 17 - gene assay to predict prostate cancer aggressiveness in the context of gleason grade heterogeneity , tumor multifocality , and biopsy undersampling . 
 bayesian adaptive design for finding the maximum tolerated sequence of doses in multicycle dose - finding clinical trials purpose statistical designs for traditional phase i dose - finding trials consider dose limiting toxicity in the first cycle of treatment . 
 therefore , it is desirable to identify the maximum tolerated sequence of three doses across three cycles of treatment . methods motivated by a three - cycle dose - finding clinical trial for a rare cancer with a jak inhibitor , we proposed and implemented a simple bayesian adaptive dose - cycle finding ( basyc ) design that allows intercycle and intrapatient dose modification . 
because of the patient - specific dosing strategy over cycles , the basyc design is suited as a method in precision oncology . results basyc is simple and transparent because its algorithm can be summarized as two tabulated decision rules before the trial starts , allowing physicians to visually examine these rules . 
2018 by american society of clinical oncology introduction phase i oncology clinical trials are typically first - in - human studies characterized by a small number of patients with a goal of determining the maximum tolerated dose of an experimental drug . 
numerous dose - finding designs have been developed , such as the 3 + 3 design , 1 the continual reassessment method , 2 and the modified toxicity probability interval ( mtpi ; mtpi - 2 ) methods , 3 - 5 as recently reviewed by sverdlov et al.6 most of the dose - finding trials consider dlt within the first cycle of treatment as the primary outcome and do not allow multicycle intrapatient dose modification . 
 for example , a new developmental drug may be considered as an additional treatment in chemotherapy that includes other standard drugs over multiple cycles . our work was motivated by and applied to such a trial at the university of chicago for a rare form of leukemia . 
in this trial , a janus kinase inhibitor , ruxolitinib , was added to a three cycle us food and drug administration ( fda ) approved chemotherapy backbone that includes cycle - specific drugs ( table 1 )  . 
scheme of the dose - cycle finding clinical trial induction ( course 1 ) four - drug bfmbased regimen consolidation ( course 2 ) cyclophosphamide vincristine dexamethasome pegylated asparaginase cytarabine mercaptopurine methotrexate ( it ) interim maintenance ( course 3 ) delayed intensification ( course 4 ) methotrexate ( iv ) vincristine pegylated asparaginase methotrexate ( it ) doxorubicin cyclophosphamide vincristine dexamethasome pegylated asparaginase cytarabine thioguanine methotrexate ( it ) maintenance ( course 5 ) vincristine dexamethasone mercaptopurine methotrexate ( po ) methotrexate ( it ) screening ruxolitinib ruxolitinib ruxolitinib 4 weeks 4 - week treatment , 4 - week washout 4 - week treatment , 4 - week washout 4 - week treatment , 4 - week washout monitoring 2 - 3 years note . 
the chemotherapy backbone is based on the c10403 regimen.7 ruxolitinib is added to courses 2 to 4 as a three - cycle treatment , with potentially varying doses across cycles . abbreviations : bfm , berlin - frankfurt - munster ; it , intrathecally ; iv , intravenously ; po , orally . dose - finding study , which aimed to identify the maximum tolerated sequence ( mts ) of ruxolitinib dose levels across three cycles . 
the mts is defined as the highest sequence of three doses at which the probability of toxicity per cycle ( tpc ) is no more than or close to a prespecified target response rate pt , given that the probability of toxicity at each cycle is also no more than or close to pt . 
three doses of ruxolitinib were considered for each of the three cycles ; therefore , there were a total of 27 possible dose - cycle combinations for three cycles of treatment . the complication of the trial was the intrapatient dose modifications over cycles . 
such approaches usually work well when the sample size of the trial is sufficiently large , as seen in the dynamic treatment regimen methods , 8 reinforcement learning , 9 and sequential multiple assignment randomized trials.10 these approaches aim to better reflect the intrinsically multistage , adaptive structure of medical decisions , in both trial design and analysis of the trial data . 
the first is lee et al , 17 who proposed an innovative phase i / ii design to adaptively and dynamically optimize a patients dose in each of two cycles of therapy based on the joint binary cycle - specific efficacy and toxicity outcomes . 
 begin treatment end of treatment cycle 1 cycle 2 cycle 3 patient enrollment ith cohort trial end mts selection first cohort dar - 1 select dose level ( cid : 143 ) treat cohort at di and collect data stop ? treat at stop ? exit trial dar - 2b treat at stop ? nth cohort exit trial patients without dlts dar - 2a patients with dlts patients without dlts patients with dlts patients without dlts patients with dlts dar - 2a dar - 2b dar - 2a dar - 2b treat at treat at treat at treat at exit trial fig 1 . 
basyc consists of decisions to determine the dose in each cycle for the enrolled patients and to select the maximum tolerated sequence ( mts ) when the trial is completed . 
in each cycle , the dose allocation rule ( dar ) selects the doses for treating patients , in which dar - 1 selects the dose for cycle 1 and dar - 2 selects the dose for subsequent cycles . 
dar - 2 is composed of two subcases : dar - 2a and dar - 2b , which are applied to the two subcohortspatients without dose - limiting toxicities ( dlts ) and patients with dlts , respectively . 
for example , a patient might exit the trial after one cycle of treatment ( potentially because of toxicity [ indicated by stop ] ) based on the dcr applied in cycle 1 . 
figure 1 illustrates the general scheme of the basyc design for the motivating trial with three doses and three cycles of treatment . dcr and dar the basic concept of the dcr is that if the probability of toxicity of the lowest dose in the next cycle is considered lower than the target rate pt , the cohort can move to the next cycle for additional treatment ( ie , the decision is a go )  . 
technical details of the dcr are given in the appendix . if the dcr is a go for a cohort , the cohort will enter the next cycle for additional treatment . 
first , the dar always assigns the first cohort patients at the lowest dose level in all the cycles of treatment , which is a default rule to ensure the safety of the lowest dose in all three cycles . 
in this case , dar - 1 follows the same decision rule as in the mtpi - 2 design.5 specifically , the dose level is decided based on the observed toxicity data from previously enrolled patients treated at the most recent dose in the first cycle . 
this ad hoc rule is needed to protect patient safety . the two subcohorts undergo the dcr and dar separately hereafter until all three cycles of treatment are completed or until they exit the trial . 
motivated by the mtpi - 2 design , 5 dose allocation is presented in the form of dose escalation , stay , or de - escalation to give the candidate dose level at the next cycle relevant to the dose level of the cycle we currently consider . 
 this table is applied to the dose at which the current cohort is treated and the dose at which the previous cohort is most recently treated in the next cycle . 
the two tables can be generated and predetermined before the trial starts for examination by physicians . in the dar , we used the mtpi - 2 design as the backbone for decision making . 
the default values of 1 and 2 are 0.05. dose - finding algorithm to begin a trial , the basyc design treats the first cohort of patients at the lowest dose level in all three cycles . 
then , after the toxicity outcomes from the first cycle are observed , the dcr decides whether the cohort will go to the next cycle , and the dar decides which dose level to use if the dcr decision is go . 
this process is repeated until all cohorts finish all cycles of treatment unless the trial is terminated early because of excessive toxicity ( safety rules are given in the appendix )  . 
as a default rule , the cohort at a given cycle must wait for the cohort at the next cycle to complete follow - up before it can enter the next cycle . we demonstrate in table 2 how the basyc design guides the motivating dose - cycle trial with three doses and three cycles . 
specifically , once the current cohort completes the first cycle of treatment with observed outcome data , the next cohort can be enrolled and assigned a dose level in the first cycle . 
for example , in table 2 , in week 24 , after cohort 3 completed the first - cycle treatment at dose level 2 , the next cohort ( cohort 4 ) was enrolled and treated at dose level 1 as its first - cycle therapy . 
each column number represents the number of patients treated , and each row number represents the number of patients experiencing toxicity , at a given dose where the decision is applied . 
 ( a ) go ( g ) / no - go ( ng ) decisions according to the dose continuous rule ( dcr ) , in which the letters in blue and red represent g and ng decisions , respectively . 
 ( b ) dose allocation decisions according to the dose allocation rule ( dar ) , in which the letters in blue , gold , green , and red represent dose escalation ( e ) , staying at the current dose ( s ) , dose de - escalation ( d ) , and dose de - escalation and exclusion ( du ) because of toxicity , respectively . 
this table is applied to the dose at which the current cohort is treated and the dose at which the previous cohort is treated in the next cycle . mts selection at the end of the trial , among all the candidate sequences of dose - cycle combinations , a sequence of three doses for three cycles would be selected as the mts . 
we provided the true toxicity probabilities of the three dose levels in the first cycle and assumed that the toxicity probability would increase by 10% per cycle at the same dose level . 
for each scenario , 10 , 000 simulated trials are conducted on computer . operating characteristics the simulation results for scenarios 1 to 6 are summarized in table 3 , with four sections per scenario . 
recall that the mts is defined as the highest sequence of three safe doses with the true probability of tpc ( calculated as the average of the three true toxicity probabilities corresponding to the three dose levels ) closest to pt and falling in the ei ( pt 1 , pt + 2 )  . 
if a scenario has no dose sequence falling in the ei , the highest sequence of three safe doses with the true probability of tpc less than pt is considered the true mts . 
no practical methods are available , and the two existing designs17 , 18 in the literature are either highly complex or tailored for specific trials . perhaps the most attractive feature of the basyc design is its simplicity and transparency , as shown in figure 2 . 
we can see that escalation and de - escalation will never happen if the true toxicity probability of a dose is located in the higher interval ( pt + 2 , 1 ) and the lower interval ( 0 , pt + 1 ) , respectively . in this report , we implemented basyc for a realworld trial with three dose levels for three cycles of treatment . 
for example , a total of 53 = 125 sequences are available for trials with five dose levels and three cycles . basyc uses independent beta / binomial models as the working model to estimate the toxicity probability of each dose in each cycle based on all patients data at that dose / cycle . 
 alternatively , one could consider a dependent model , such as the markov model in fernandes et al , 18 to estimate the toxicity probabilities . in basyc , we focused on the dose - cycle trials with binary outcomes . 
with larger sample sizes , one can adopt dose - insertion methods23 , 24 to allow insertion of new doses when necessary . an mts with fixed dose levels at the end of the trial . 
for example , one may not allow a higher dose level than that in mts for any cycle of the treatment in the policy . lastly , a formal personalized dosing policy would follow the spirit of lee et al17 and use model - based inference on multiple cycles . 
stock w , luger sm , advani as , et al : favorable outcomes for older adolescents and young adults ( aya ) with acute lymphoblastic leukemia ( all ) : early results of us intergroup trial c10403 . 
doussau a , asselain b , le deley mc , et al : dose - finding designs in pediatric phase i clinical trials : comparison by simulations in a realistic timeline framework . 
doussau a , thibaut r , paoletti x : dose - finding design using mixed - effect proportional odds model for longitudinal graded toxicity data in phase i oncology clinical trials . 
guo w , ni y , ji y : teams : toxicityand efficacy - based dose insertion design with adaptive model selection for phase i / ii dose - escalation trials in oncology . 
 appendix notation suppose under consideration is a total of i candidate dose levels and j treatment cycles , indexed by i = 1 , 2 , , i ; j = 1 , 2 , , j . 
let k index the cohort , k = 1 , 2 , , k , where k is the maximum number of cohorts that will be recruited to the trial . during dose - cycle finding ( not for maximum tolerated sequence [ mts ] selection ) , we use simple and independent beta priors across doses and cycles and an independent binomial likelihood as a working model for the estimation of pij . 
the application in bayesian adaptive dose - cycle finding ( basyc ) is detailed here . dose continuation rule for cohort k that has been treated at dose i in cycle j , the dose continuation rule ( dcr ) for cohort continuation ( whether the cohort can continue treatment at cycle ( j + 1 ) ) is described as follows : if cohort k has finished the last cycle of therapy ( ie , j = j ) , cohort k exits the trial . if cohort k has not finished all cycles of therapy ( ie , j < j ) , and if pr { p1 , j + 1 > pt|data } > , where is a prespecified cutoff probability and often set to be close to 1 ( eg , = 0.95 ) , stop cohort k for any additional treatment , and patients in cohort k exit the trial . 
 otherwise , continue this cohort k to the next cycle ( j + 1 )  . this algorithm states that when the probability that toxicity of the lowest dose level ( dose level 1 ) in cycle ( j + 1 ) is higher than the target pt does not exceed a large value , cohort continuation is allowed . 
let x1 , j + 1 and n1 , j + 1 be the cumulative number of patients ( across all the previous and current cohorts ) with dose - limiting toxicity ( dlt ) events and treated at dose level 1 at cycle ( j + 1 ) , respectively . 
this beta distribution is used to calculate the posterior probability . dose allocation rule if cohort k in cycle j can proceed to the next cycle , the dose assigned to the next cycle ( j + 1 ) is dependent on the cumulative data from both the current cycle j and the next cycle ( j + 1 )  . 
such data accumulate all the toxicity outcomes from previously treated cohorts at this dose . then , consider a cohort of patients that has just completed treatment in the first cycle at a dose level . 
 here , the previous cohort refers to the cohort of patients enrolled just before the current cohort , and the toxicity data or the data ( also hereinafter ) refer to the data from all enrolled patients treated at the corresponding dose . 
specifically , given data1 and dose1 , the mtpi - 2 design will output a candidate dose level i1 , and given data2 and dose2 , mtpi - 2 will output another candidate dose i2 . 
specifically , given the dose ( dose1 ) in cycle 1 and the candidate dose i2 that mtpi - 2 gives based on data2 and dose2 from cycle 2 , dar - 2b selects the dose i = min { max { dose1 1 , 1 } , i2 } , the minimum of the dose 1 level lower than the current dose in cycle 1 , and i2 as the final dose for treating the cohort in cycle 2 . note that because of the cohort split , the previously enrolled subcohorts may have been treated in cycle 2 at two dose levels , say dose21 and dose22 . 
the outcome data from both subcohorts , denoted as data21 and data22 , will be used to inform the cycle 2 dose for the subsequent cohort that will start from the first cycle . 
in particular , for each of the data21 and data22 , the mtpi - 2 design will give two candidate doses i21 and i22 as the potential dose for the subsequent cohort in cycle 2 . 
then , the minimum of i21 and i22 will be provided as the candidate dose , denoted as i2 = min { i21 , i22 } , for the subsequent cohort as the cycle 2 candidate dose . 
the same principle is applied to decide the dose level in cycle 3 if needed . walkthrough of the hypothetic trial table 2 summarizes how the basyc design guides the motivating dose - cycle trial with three doses and three cycles . 
at this point , cohort 2 is enrolled and assigned to the next higher dose , dose 2 ( d2 ) , according to the dar decision , because cohort 1 has not exhibited any toxicity . 
at week 16 , cohort 1 completes treatment at d1 in cycle 2 with 0 toxicity outcome , and cohort 2 completes treatment at d2 in cycle 1 with 1 dlt outcome . 
the single patient with dlt , patient 4 , is de - escalated to d1 , and the remaining two patients without dlts , patients 5 and 6 , stay at d2 . 
this process continues for subsequent cohorts and cycles at weeks 24 , 32 , and so on , until all 15 patients ( or five cohorts ) have completed treatment at week 56 . safety rule applied in basyc for safety , the basyc design applies two additional safety rules throughout the entire trial : rule 1 ( early termination ) : for any cycle , if the toxicity probability of the lowest dose is higher than the target pt with a large probabilitythat is , if j * { 1 , 2 , , j } such that pr { p1j * > pt|data } > , where is close to 1 ( say = = 0.95 ) terminate the trial early . rule 2 ( dose exclusion ) : if the toxicity probability of dose i in cycle j is higher than the target pt with a large probability , pr { pij > pt|data } > , exclude doses i and the higher doses from cycle j and higher cyclesthat is , doses { i , i + 1 , , i } will never be used in the trial in cycles { j , j + 1 , , j } again . the posterior probabilities in both rules are calculated based on the simple beta / binomial calculation proposed in the mtpi design.3 details are provided in appendix under dose continuation rule . mts definition and selection after the enrollment and dose - cycle finding are completed , in the mts selection , we use a frequentist and nonparametric probability model to make inference . 
specifically , we essentially want to estimate the toxicity per cycle ( tpc ) qs , which is the average of the three toxicities of the doses in a sequence s ( described under definition of mts )  . 
we then construct an unbiased estimate of tpc qs ( described under estimation of qs ) and order - transform them based on isotonic regression ( described under mts selection )  . 
for each sequence s , we define the cumulative dose level as the sum of the dose levels across three cycles ( ie , d * s = ds1 + ds2 + ds3 )  . 
for each sequence s , denote pdsj , j the probability of toxicity for the dose in cycle j of sequence s , j = 1 , 2 , 3 . 
a sequence s is unacceptable if the toxicity probability of each dose in each cycle is higher than pt with a large probability , defined as j = 1 , 2 , 3 , pr { pdsj , j > pt|data } > , where dsj denotes dose levels { 1 , 2 , 3 } and is close to 1 , say = 0.95. 
the posterior probability pr { pdsj , j > pt|data } is based on a simple beta / binomial hierarchic model , similar to the calculation under dose continuation rule . 
 among all the safe sequences that satisfy the condition above , we want to select the highest sequence with overall qs close to pt , subject to the toxicity probability of the same dose level nondecreasing across cycles . 
however , the problem with that approach is that because of random chance , a sequence with a higher order ( and therefore higher toxicity ) might have a smaller qs than a lower - ordered sequence . 
for example , it is possible that the toxicity data for sequence 1 , 1 , 1 include only one toxicity event in all three cycles , whereas the data for sequence 2 , 1 , 1 include no toxicity event . 
however , sequence 2 , 1 , 1 is in theory a more toxic sequence , because it uses dose level 2 in cycle 2 instead of dose level 1 . 
therefore , selecting the sequence based on the distance of |qs pt| is not valid , because we would select 1 , 1 , 1 as the mts , not 2 , 1 , 1 in this case . to address this issue , we propose an isotonic transformation and calculate transformed qs values using the pool adjacent violator algorithm ( pava ) 20 just like in the mtpi design3 , 4 and mtpi - 2 design.5 here , we still use the sequence - specific data for the isotonic transformation . 
when there is a tie between m sequences , there are m ! possible simple orderings among thethen , assuming with probability 1 / m ! that one of the orderings , say ordering w , is true , we apply pava to the following ordering w of qs , w = 1 , 2 , , m !  . 
then , finally , the sequence dl * * that has nonincreasing dose levels across three cycles and the largest frequency f l * is selected as the estimated mts . 
therefore , the dose levels of the mts cannot be increasing , or else the lower dose in the early cycle can always be replaced by the higher dose in the later cycle . 
these results show that basyc is strong in protecting patient safety . scenario 2 presents a similar pattern of dose - toxicity relationship to scenario 1 , except that the toxicity probability of dose level 2 is now below pt = 30% . 
this suggests that the basyc design is nimble and can reach high dose - cycle combinations even with small sample sizes . scenario 4 presents an opposite case to scenario 3 , because all the doses are overly toxic with toxicity probabilities above pt . 
this scenario demonstrates the ability of the basyc design to stop the trial quickly in case of excessive toxicity in all dose sequences . scenarios 5 and 6 reflect situations where there is a leap in toxicity probabilities across the three doses . 
oxnard , md1 noninvasive genotyping of plasma cell - free dna is being integrated into cancer care at an astonishing rate , as its potential to radically increase access to personalized cancer care is increasingly recognized.1 whereas next - generation sequencing ( ngs ) of tumor has been commoditized and democratized ( with many academic hospitals offering their own clinical laboratory improvement amendmentscertied tests ) , plasma ngs is primarily sent out for testing at commercial laboratories . 
however , although these tests are ordered and reported en masse , the causes of falsepositive or false - negative plasma ngs results have only gradually become apparent ( fig 1 )  . false - negative results have long been recognized as common with blood - based assays . 
we and others identied that assay sensitivity is closely related to clinical factors such as stage and metastatic spread , tumor dna in cases suggesting limited shed of missed by plasma ngs.2 , 3 false positives have also been described with many plasma genotyping assays and are routinely attributed to tumor heterogeneity.4 although heterogeneity is clearly a source of tumor / plasma discordance in cancers that have developed drug resistance , 5 , 6 many false positives can be attributed to dna shed from normal cells , including germline variants or noncancerous somatic variants such as clonal hematopoiesis ( ch ) .7 - 9 the latter is particularly challenging because ch can involve cancer - associated genes ( eg , tp53 , jak2 , kras )  . 
yet when such mutations are identied in plasma , they may not reect true tumor genotype . what is least understood is how technical factors related to assay performance contribute to false - positive and false - negative results . 
probe design and specics of library generation are often considered proprietary and are only minimally described in the few analytical validation studies that have been published . this is the context motivating the publication by stetson et al10 in jco precision oncology . 
the authors sent aliquots of plasma to four commercial clinical laboratory improvement amendmentscertied laboratories for plasma ngs and compared this to ngs performed on matched tumor and normal tissue at foundation medicine . 
the vendors were blinded to tumor ngs results but knew that their plasma ngs results would be compared with orthogonal tissue results , as well as with plasma results from other laboratories . 
following bioinformatic analysis and variant calling , binary alignment map les were provided by the vendors to the authors for independent , unblinded , post - hoc sequence analysis . with this design , the authors were not only able to address many of the pitfalls that plagued prior vendor comparison studies , 11 , 12 but they could also investigate interassay technical factors . 
more precisely , stetson et al10 were able to account for known germline variants , investigate mutation - calling biases , and examine whether false negatives were as the result of stochastic sample biases or thresholding nuances of the vendors bioinformatic lter . the results should give pause . 
positive predictive value ( ppv ) against tissue ranged from 36% to 80% . however , results improved when limited to mutations called at an allelic fraction ( af ) greater than 1% , with three vendors achieving a ppv of 100% for these higher af calls . 
note that variants detected at less than 1% af are routinely reported by each vendor , and such sensitivity is advertised as a unique strength of plasma ngs assays . false - positive variants tended to be novel with no reports in somatic variant databases , and these were often related to vendor - specic mutational biases . false negatives were attributed to bioinformatic ltering of suspected germline variants and limitations from high signal - to - noise ratio . 
taken together , these results point to recurrent contributions from technical differences in the bioinformatic pipelines of the assays , assay sensitivity , or plain error . the current study is far from perfect and leaves room for improvement . 
the study cohort consisted primarily of early - stage cancers ( 21 of 24 patients had stage i and ii cancers ) , which are not the intended population for plasma ngs . 
beyond these established biologic factors , technical factors may be an underappreciated source of erroneous plasma ngs . technical factors tett chnical factor tumor dna shed tumor heterogeneity ( particularly at resistance ) tett chnical factors technical factors white blood cell dna ( clonal hematopoiesis , germline variants ) finally , reference truth was extrapolated across four different assays . 
furthermore , this analysis does not broach the challenges of reporting plasma ngs results . one could imagine that a forward - thinking laboratory might recognize the limitations of plasma ngs in its reporting , noting the risk of false positives for low af or ch - associated variants , as well as the risk of false negatives when low tumor shed is apparent . as the use of plasma ngs becomes increasingly widespread in cancer care , there remains a clear need for concordance studies such as this one . 
 editorial policy , please refer to or ascopubs.org / po / authorcenter . patents , royalties , other intellectual property : patent pending on noninvasive blood - based monitoring of genomic alterations in cancer ( inst ) cloud p . 
paweletz honoraria : astrazeneca korea , bio - rad consulting or advisory role : dropworks research funding : guardant health , astrazeneca travel , accommodations , expenses : astrazeneca korea geoffrey r . 
oxnard honoraria : chugai pharma , bio - rad , sysmex , guardant health consulting or advisory role : astrazeneca , inivata , sysmex , takeda , loxo oncology , ignyta , dropworks , grail no other potential conicts of interest were reported . references aggarwal c , thompson jc , black ta , et al : clinical implications of plasma - based genotyping with the delivery of personalized therapy in metastatic non - small cell lung cancer . 
jama oncol 2 : 1014 - 1022 , 2016 bettegowda c , sausen m , leary rj , et al : detection of circulating tumor dna in earlyand late - stage human malignancies . 
sci transl med 6 : 224ra24 , 2014 forshew t , murtaza m , parkinson c , et al : noninvasive identication and monitoring of cancer mutations by targeted deep sequencing of plasma dna . 
sci transl med 4 : 136ra68 , 2012 oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - smallcell lung cancer . 
clin cancer res 24 : 4437 - 4443 , 2018 oxnard gr , hu y , mileham kf , et al : assessment of resistance mechanisms and clinical implications in patients with egfr t790m - positive lung cancer and acquired resistance to osimertinib . 
hu y , alden rs , odegaard ji , et al : discrimination of germline egfr t790m mutations in plasma cell - free dna allows study of prevalence across 31 , 414 cancer patients . 
clin cancer res 23 : 7351 - 7359 , 2017 slavin tp , banks kc , chudova d , et al : identication of incidental germline mutations in patients with advanced solid tumors who underwent cell - free circulating tumor dna sequencing . 
stetson d , ahmed a , nuttall brb , et al : orthogonal comparison of four plasma ngs tests with tumor suggests technical factors are a major source of assay discordance . 
paweletz cp , sacher ag , raymond ck , et al : bias - corrected targeted next - generation sequencing for rapid , multiplexed detection of actionable alterations in cell - free dna from advanced lung cancer patients . 
guibert n , hu y , feeney n , et al : amplicon - based next - generation sequencing of plasma cell - free dna for detection of driver and resistance mutations in advanced non - small cell lung cancer . 
rna - seq allows the use of a method called the percent splicing index to quantify allelic expression by mapping rna - seq reads from alternate or aberrant transcripts relative to reference ( normal ) transcripts as described by schafer et al.7 we have recently published data demonstrating that the variant brca2 c.426 - 12_426 - 8delgtttt not only results in partial skipping of exon 5 ( brca2 r.426_475del ) , but this splicing event was also seen in 20 of 345 control patients.8 laboratories should proceed with caution when weighting functional evidence in variant curation , because interpretation of these results can be complex . 
in this specic case , the rna - seq results and the new clinical data prompted reassessment and resulted in reclassication of this brca2 variant . the article by nix et al6 highlights the need for laboratories to increase collaboration , particularly when siloed clinical information can shed light onto discrepant classications . 
submission of a classication and its justication to dynamic databases such as clinvar is a critical step in this process , 9 because data sharing among clinical diagnostic laboratories improves the resolution of variant interpretation differences.10 in summary , we believe that innovation , such as introduction of rna - seq to hereditary cancer clinical genetic testing as well as participation in multi - institutional efforts designed to increase transparency between laboratories , is of utmost importance for advancing variant classication that will ultimately benet patients . rachid karam , md , phd ; holly laduca , ms ; marcy e . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . rachid karam employment : ambry genetics research funding : ambry genetics travel , accommodations , expenses : ambry genetics holly laduca employment : ambry genetics stock and other ownership interests : ambry genetics marcy e . 
richardson employment : ambry genetics tina pesaran employment : ambry genetics stock and other ownership interests : ambry genetics travel , accommodations , expenses : ambry genetics elizabeth chao employment : ambry genetics no other potential conicts of interest were reported . references cummings bb , marshall jl , tukiainen t , et al : improving genetic diagnosis in mendelian disease with transcriptome sequencing . 
sci transl med 9 : eaal5209 , 2017 fr esard l , smail c , ferraro nm , et al : identication of rare - disease genes using blood transcriptome sequencing and large control cohorts . 
nat med 25 : 911 - 919 , 2019 gonorazky hd , naumenko s , ramani ak , et al : expanding the boundaries of rna sequencing as a diagnostic tool for rare mendelian disease . 
am j hum genet 104 : 466 - 483 , 2019 lee h , huang ay , wang l - k , et al : diagnostic utility of transcriptome sequencing for rare mendelian diseases . 
genet med 22 : 490 - 499 , 2020 karam r , conner b , laduca h , et al : assessment of diagnostic outcomes of rna genetic testing for hereditary cancer . 
nix p , mundt e , manley s , et al : functional rna studies are a useful tool in variant classication but must be used with caution : a case study of one brca2 variant . 
jco precis oncol 4 : 730 - 735 , 2020 schafer s , miao k , benson cc , et al : alternative splicing signatures in rnaseq data : percent spliced in ( psi )  . 
curr protoc hum genet 87 : 11.16.111.16.14 , 2015 landrith t , li b , cass aa , et al : splicing prole by capture rna - seq identies pathogenic germline variants in tumor suppressor genes . 
considering that the codon of asparagine is aac or aat , we wondered if the adenine base editor ( abe ) , which induces at to gc conversion at specific site , could be used to reduce pd - 1 suppression by changing the glycosylated residue in car - t cells . 
our study suggested that the single base editors can be used to augment car - t cell therapy . keywords : glycosylation , single base editing , car - t cell , pd - 1 to the editor , chimeric antigen receptor t ( car - t ) cells are not satisfying in treating solid tumors [ 1 ]  . 
crispr / cas9 can downregulate pd - 1 [ 2 ] but also potentially leads to carcinogenesis , because success of such tools relies on suppressing dna damage response [ 3 ]  . 
as n - linked glycosylation is restricted on asparagine coded by aac or aat , adenine base editors ( abe ) can convert at to gc base pair [ 5 ] , and may be used to diminish such glycosylation . 
the delivery of grna using lentivirus is efficient [ 6 ] , so we constructed lentiviral vectors simultaneously expressing mesothelin - directed car and grna targeting non - specific sites ( scramble ) or n74 of pdcd1 ( grna ) , under 2 independent promoters ( additional file 1 : figure s1a )  . 
2h ( cid : 150 ) ( additional files 3 and 4 )  . single base editing can modulate the stability and function of target protein by changing a single residue [ 8 ]  . 
compared with crispr / cas9 , abe has narrower editing window and much less frequent off - target events [ 9 ] , representing a safer and more precise approach for gene editing . 
abe - mediated point mutation can downregulate the inhibitory pd - 1 , therefore providing an alternative approach to augment t cell immunotherapy . authors contributions yz and fl devised the project and supervised the experiments . 
all authors read and approved the final manuscript . funding this work received funds from the national key research and development program ( 2018yfc1313400 , 2016yfc1303501 ) ; national natural science foundation of china ( 81771781 , u1804281 )  . availability of data and materials all supporting data are included in the manuscript and supplemental files . additional data are available upon reasonable request to corresponding author . ethics approval and consent to participate all experiment procedures were followed the protocol approved by institute committee on ethics . 
and all animal experiments were performed in accordance with the ethics approval obtained from the first affiliated hospital of zhengzhou university animal ethics committee . consent for publication not applicable competing interests the authors declare that they have no competing interests . author details 1biotherapy center , the first affiliated hospital of zhengzhou university , zhengzhou 450052 , henan , china . 
3school of life sciences , zhengzhou university , zhengzhou 450052 , henan , china . 4henan key laboratory for tumor immunology and biotherapy , zhengzhou 450052 , henan , china . received : 3 november 2019 accepted : 13 november 2019 supplementary information supplementary information accompanies this paper at 1186 / s13045 - 019 - 0831 - 5 . next - generation sequencing directs therapy and delineates a clonal relationship in mast cell sarcoma and acute myeloid leukemia timothy j . 
collins jr , md1 a 61 - year - old man was diagnosed with acute myeloid leukemia ( aml ) associated with trisomy 8 cytogenetic abnormality and flt3 itd mutation . 
post - transplantation , he showed no morphologic or ow cytometric evidence of disease and his bone marrow chimerism was more than 95% donor cells at several timepoints post - transplantation , including 24 months after the transplant . 
he received tacrolimus post - transplantation and developed mild chronic graft - versus - host disease that was limited to the skthe patient remained on tacrolimus . twenty - nine months after transplantation , he presented with abdominal pacomputed tomography scan of the abdomen and pelvis revealed a known , unchanged ventral abdominal hernia , but also showed a new lytic lesion on the inferior pubic ramus that was concerning for a new malignancy ( fig 1a )  . 
flow cytometry of the lesion demonstrated a predominance of cd117bright positive , cd34 - negative myeloid cells suspected to be mast cells that did not aberrantly express cd2 or cd25 ( fig 3 )  . 
these cells showed atypical expression of fcri ( cd64 ) , which is seen upon mast cell activation . immunohistochemical analysis demonstrated that the cells were positive for cd117 and weakly positive for mast cell tryptase and negative for cd2 , cd25 , and cd34 ( fig 4 )  . 
altogether , supportive of a diagnosis of mast cell sarcoma ( mcs )  . the tumor next - generation sequencing ( foundationone heme panel ; foundation medicine , cambridge , ma ) on the biopsy was signicant for kit y503_f504insay , idh2 r140q , and srsf2 p95h mutations , but was negative for flt3 mutations . 
the particular kit mutation detected has been reported to be responsive to imatinib.1 - 4 the idh2 mutation has not previously been identied in mast cell neoplasms.5 the patient was treated with imatinib 400 mg per day in addition to radiation to the sacrum and pubic ramus4 , 500 cgy in 25 fractions . 
he remains without evidence of aml recurrence 71 months after hematopoietic sct . the original diagnosis of aml and subsequent bone marrow evaluations were reviewed in light of the development of mcs . 
cytogenetic studies revealed 47xy , + 8 [ 13 ] / 46 , xy [ 7 ] and uorescence in situ hybridization was positive for an extra signal for runx1t1 ( 8q22 ) in 59 of 200 interphase cells . 
sanger sequencing on dna from a saliva sample demonstrated wild - type germline idh2 and srsf2 . identical idh2 and srsf2 mutations implied a clonal relationship between the mcs and aml ( fig 5 )  . 
 brown et al context and mast cell sarcoma ? can tools , such as next - generation sequencing ( ngs ) , delineate a clonal relationship in a patient with acute myeloid leukemia we identied a probable clonal relatedness between the two neoplasms , with both sharing identical idh2 and srsf2 mutations . 
this report provides anecdotal evidence of a clonal relationship between acute myeloid leukemia and mast cell sarcoma that is developmentally feasible and describes a unique scenario in which ngs was effective at directing therapy . 
clinicians should consider performing ngs in patients with two neoplasms , particularly if a progenitor cell is feasible , as well as in patients with mast cell disorders and a neoplasm . the clonal progenitor that harbored the idh2 and srsf2 mutations persisted . 
shared mutations between aml and mcs support the existence of a preleukemic clonal progenitor that developed into aml initially and later into mcs . mcs was rst described in 1986 and is one of many diseases arising from the spectrum of mastocytosis.11 - 13 it typically presents as a solitary mass that may arise anywhere in the body and has intensely avid uorodeoxyglucose uptake on petcomputed tomography scan.9 - 11 , 14 - 20 diagnosis depends on the synthesis of pathologic and immunophenotypic that are features in a patient with an aggressive , initially sarcoma - like tumor.16 , 17 although initially localized , these tumors typically metastasize fig 1 . 
 ( a ) computed tomography ( ct ) scan of the abdomen and pelvis obtained for evaluation of abdominal pain incidentally revealed a destructive lesion of the left inferior pubic ramus that measured approximately 3 cm 2 cm , worrisome for malignancy . 
survival ranges from 2 months to 8 years , with a median survival of 6 months.10 , 12 , 15 , 16 , 18 - 21 cells are usually more atypical than those observed in systemic mastocytosis , with an epithelioid appearance with abundant granular cytoplasm and bilobed or multilobed nucleoli.15 , 22 mcs can be misdiagnosed on initial pathologic review given its rarity and resemblance to other tumor types , including lymphomas . 
these cells often lose markers that are characteristic for mast cells , which further complicates the diagnosis.20 , 23 evaluation of markers that are helpful to establish the diagnosis include cd2 , cd25 , cd30 , cd33 , cd34 , cd45 , cd117 , and mast cell tryptase.12 , 18 absence of cd117 positivity should call into question the diagnosis of a mast cell disorder . 
mast cell tryptase is highly specic for mast cell lineage , but may only show variable positivity in mcs.12 , 23 other immunohistochemical markers that overlap with melanoma , lymphomas , or other histiocytic processes have been reported.12 in the absence of another concurrent myeloid neoplasm , serum tryptase elevation strongly supports the diagnosis of a mast cell disorder.12 , 23 mcs have possessed kit mutations in eight of 15 cases that have reported on kit mutation testing , including the present case.10 , 11 , 19 , 20 cells with kit mutations fig 2 . 
flow cytometry of pubic ramus lesion detected a population of medium - sized to large cells , which accounted for approximately 60% of the total events , with high orthogonal light scatter indicative of high granularity / internal complexity ( red , abnormal cells ; blue , lymphocytes )  . 
abnormal cells were cd15 negative , cd117 bright positive , cd7 equivocal , cd13 + , cd2 , cd25 , cd36 , and cd64 + ( variable intensity )  . 
by immunohistochemistry , tumor cells were positive for cd117 and mast cell tryptase ( weakly ; top ) but negative for cd2 and cd25 ( bottom )  . cd25 remain cd117 bright on immunohistochemistry and are unaffected by changes induced by these mutations.24 kit mutations do not affect the ow cytometric detection of cd117 . therapy of mcs is poorly dened but typically involves surgery and radiation to localized lesions ; chemotherapy is usually ineffective.19 , 20 we would suggest that all patients with suspected mcs have kit sequenced . 
results of next - generation sequencing on both mcs and aml mutated allele genomic alteration frequency , % detected fda - approved therapy for patients tumor kit ( y503_ f504insay ) idh2 ( r140q ) srsf2 ( p95h ) flt3 ( s451f ) idh2 ( r140q ) ptpn11 d61h - subclonal n308dsubclonal srsf2 ( p95h ) imatinib none * none none none none enasidenib ( 2017 ) common myeloid progenitor cell idh2 srsf2 idh2 srsf2 flt3 ptpn11 mast cell idh2 srsf2 note . 
enasidenib was approved by the fda in 2017 , several years after the patient had aml . abbreviations : aml , acute myeloid leukemia ; fda , us food and drug administration ; mcs , mast cell sarcoma . * although enasidenib is not fda approved for mcs , it is conceivable that the drug , which targets mutant idh2 , may have activity in this patients case . and thus remains sensitive to imatinib.28 mcs with d816v mutations may be sensitive to other tyrosine kinase inhibitors , including avapritinib , which selectively targets the d816v mutation and is well tolerated.29 , 30 of interest , the idh2 mutation in our patients case is shared between aml and mcs , which suggests that it was present in a lessdifferentiated common progenitor cell . 
collins jr employment : university of texas southwestern medical centersimmons cancer center honoraria : optumhealth research funding : agios , arog , bristol - myers squibb , celgene no other potential conicts of interest were reported . references 2011 guo t , hajdu m , agaram np , et al : mechanisms of sunitinib resistance in gastrointestinal stromal tumors harboring kitay502 - 3ins mutation : an in vitro mutagenesis screen for drug resistance . 
br j haematol 173 : 323 - 326 , 2016 cancer genome atlas research network ; ley tj , miller c , et al : genomic and epigenomic landscapes of adult de novo acute myeloid leukemia . 
cell 168 : 1041 - 1052.e18 , 2017 yamashita a , saito t , akaike k , et al : mast cell sarcoma of the sternum , clonally related to an antecedent germ cell tumor with a novel d579del kit mutation . virchows arch 470 : 583 - 588 , 2017 10 . 
georgin - lavialle s , aguilar c , guieze r , et al : mast cell sarcoma : a rare and aggressive entityreport of two cases and review of the literature . 
krauth mt , f odinger m , rebuzzi l , et al : aggressive systemic mastocytosis with sarcoma - like growth in the skeleton , leukemic progression , and partial loss of mast cell differentiation antigens . 
verstovsek s , tefferi a , cortes j , et al : phase ii study of dasatinib in philadelphia chromosome - negative acute and chronic myeloid diseases , including systemic j cancer 42 : 1093 - 1103 , 2006 mastocytosis . 
brunner am , neuberg ds , wander sa , et al : isocitrate dehydrogenase 1 and 2 mutations , 2 - hydroxyglutarate levels , and response to standard chemotherapy for patients with newly diagnosed acute myeloid leukemia . 
schuurhuis gj , heuser m , freeman s , et al : minimal / measurable residual disease in aml : a consensus document from the european leukemianet mrd working party . 
leach , ms , lgc1 ; jessica marquard , ms , lgc1 ; manmeet ahluwalia , md1 ; hetty carraway , md , mba1 ; petros grivas , md , phd2 ; davendra p.s. 
recent data sets indicate that the incidence of hereditary cancer may be as high as 17.5% in patients with cancer , and a notable subset is missed if screening is solely by family history and current syndrome - based testing guidelines . identication of germline variants has implications for both patients and their families . 
we aimed to summarize genes linked to hereditary cancer and the somatic and germline panels that include such genes . methods germline predisposition genes were chosen if commercially available for testing . 
penetrance was dened as low , moderate , or high according to whether the gene conferred a 0% to 20% , 20% to 50% , or 50% to 100% lifetime risk of developing the cancer or , when percentages were not available , was estimated on the basis of existing literature descriptions . results we identied a total of 89 genes linked to hereditary cancer predisposition , and we summarized these genes alphabetically and by organ systewe considered four germline and six somatic commercially available panel tests and quantied the coverage of germline genes across thecomparison between the number of genes that had germline importance and the number of genes included in somatic testing showed that many but not all germline genes are tested by frequently used somatic panels . conclusion the inclusion of cancer - predisposing genes in somatic variant testing panels makes incidental germline ndings likely . 
2019 by american society of clinical oncology introduction cancer is a genetically driven disease triggered by the accumulation of variants in genes responsible for regulation of cell growth , invasion , survival , and migration . 
most cancers are sporadic and result from acquired genetic changes known as somatic variants , which are caused by stochastic events that accumulate over time as well as by specic environmental factors , such as smoking and ultraviolet radiation , among others.1 precision oncology currently consists of an effort to understand the acquired genetic variants that underlie each patients cancer , which thus allows the opportunity to tailor therapy to a patients individual tumor biology.2 although tumor testing previously involved sequencing of individual genes or short hotspot fragments of dna , recent advances in next - generation sequencing ( ngs ) technology have enabled much more frequent and precise identication of pathogenic variants.2 , 3 such sequencing platforms are rapidly becoming faster and cheaper , which makes them as available and as popular as many other clinical testing tools.4 , 5 germline variants occur in germ cells , which are responsible for reproduction . 
although somatic variants occur in a single cell and are passed down only to that cells offspring , germline variants exist in all somatic cells and can inuence cancer susceptibility by affecting multiple cellular processes ( eg , cancer clone growth , somatic variant acquisition rates , and carcinogen metabolism ) .1 discovery and understanding of germline variants are of major clinical importance to the patient diagnosed with a hereditary cancer ; the identication of an inherited genetic variant often has therapeutic and prognostic value for a patient undergoing therapy . 
 akras et al showing promise in the context of both somatic and germline variants in brca and other homologous repair genes and represent a breakthrough niche in precision oncology.7 therapeutic consequences of other germline ndings are also expanding ; this is best highlighted by the recent nding that lynch syndromerelated cancers are exquisitely sensitive to programmed cell death - 1 inhibition.8 finally , a germline nding is clinically important in that members of the patients broader family who also carry inherited pathogenic variants will be at an increased risk of cancer as well.9 targeted surveillance is important for all carriers of germline pathogenic variants , whether they are cancer survivors or asymptomatic relatives ; the vast majority of inherited cancer predisposition syndromes increase the risk of multiple cancers , and targeted surveillance for the discrete subset of cancers associated with that particular gene should be undertaken . 
in addition , data support that gene - specic , directed cancer surveillance programs can be life - saving for carriers.10 , 11 thus , identication of pathogenic variants in the germline is critical for the improvement of health outcomes in cancer treatment and prevention . previously , it had been estimated that a small minority of cancers ( 5% to 10% ) are a result of inherited germline pathogenic variants.9 emerging data sets in the post - ngs era indicate that the incidence of hereditary cancer may be as high as 17.5% in patients who carry a diagnosis of cancer and even higher in specic histologic types , such as ovarian cancer and urothelial carcinoma.12 - 14 multiple studies have shown that somatic tumor dna sequencing may lead to incidental ndings of hereditary risk.15 , 16 this realization magnies the potential impact of somatic testing and prompts the need for a re - evaluation of companion germline diagnostic methodology . 
in this review , we provide a summary of genes related to hereditary cancer and assess the comprehensiveness of somatic and germline panels that test them . genes with germline implications table 1 catalogs cancer predisposition genes organized by tumor type ; each row lists all associated germline genes for a given tumor type . 
as an alternate reference , table 2 lists cancer predisposition genes in alphabetical order ; each row lists associated cancers and the estimated penetrance of these cancers for that particular gene . 
the dual table organization allows an oncologist to use either the clinical presentation or the results of somatic genetic testing as a screening tool to understand if a patients family history or somatic genetic testing result , respectively , may represent a germline variant . reviewed genes were chosen on the basis of their identication as cancer - susceptibility genes for which commercial germline testing is available from the four major germline testingfocused companies in the united states . 
for each cancer predisposition gene in table 2 , associated cancers are broadly categorized by the estimated penetrance categories ( high , medium , and low penetrance ) for that gene . 
penetrance was dened as low , moderate , or high , according to a 0% to 20% , 20% to 50% , or 50% to 100% lifetime chance of developing that particular cancer or , when percentages were unavailable , an estimate based on descriptions in the existing literature.17 it is important to note that different studies may declare varying penetrance rates for a gene , so we aimed to reect the ndings of the literature at large . as seen in table 2 , cancer - associated genes have greatly varying penetrance rates for different phenotypes ( ie , different types of cancer )  . 
for example , pathogenic variants in lynch syndrome genes ( ie , epcam , mlh1 , msh2 , msh6 , pms2 ) are not highly penetrant for pancreatic cancer but are for colorectal cancer . 
these differences in penetrance also underscore the importance of gene - based , rather than syndromic or histology - based , interpretations , given the unique physiology that underlies specic variants . in addition , several germline variants confer an increased risk only if they are biallelic ( ie , both alleles of the gene carry pathogenic variants )  . 
if genes are not marked as such , they can be assumed to confer risk when monoallelic ( ie , only one allele is altered )  . in the appropriate scenario , these tables can be used to guide genetic testing and counseling ; however , they should the current clinical be used with an understanding of limitations of such data . 
cancer subtypes and associated hereditary genes that confer risk ( continued ) cancer type associated germline genes skin ( scc ) small bowel ( ac ) thyroid acd , blm , cdkn2a , fancc , recql4 , terc , tert , tp53 apc , bmpr1a , epcam , mlh1 , msh2 , msh6 , mutyh , pms2 , smad4 , stk11 apc ( ptc ) , hras , mutyh , pten ( ftc , ptc ) , ret ( mtc ) , wrn ( ftc , ptc ) abbreviations : ac , adenocarcinoma ; acc , adrenocorticocarcinoma ; all , acute lympocytic leukemia ; aml , acute myeloid leukemia ; bcc , basal cell carcinoma ; cel , chronic eosinophilic leukemia ; cll , chronic lymphocytic leukemia ; cmml , chronic myelomonocytic leukemia ; eoc , epithelial ovarian cancer ; erms , embryonal rhabdomyosarcoma ; ftc , follicular thyroid cancer ; gbm , glioblastoma multiforme ; gist , gi stromal tumor ; hb , hepatoblastoma ; hcc , hepatocellular carcinoma ; lam , lymphangioleiomyomatosis ; mds , myelodysplastic syndrome ; mel , melanoma ; mtc , medullary thyroid cancer ; nb , nephroblastoma ; nsclc , nonsmall - cell lung cancer ; pnet , pancreatic neuroendocrine tumors ; ppb , pleuropulmonary blastoma ; ptc , papillary thyroid cancer ; rcc , renal cell carcinoma ; scc , squamous cell carcinoma ; sccoht , small - cell carcinoma of the ovary , hypercalcemic type ; scst , sex cord stromal tumors ; sctat , sex cord tumors with annular tubules ; seb , sebaceous gland carcinoma ; sega , supependymal giant cell astrocytoma ; tcc , transitional cell carcinoma ; t - pll , t - cell prolymphocytic leukemia . clinical benet to the patient . 
testing relatives can help identify those at an increased risk of developing similar cancers ; however , a challenge to counseling still exists , because these variants lack the cohesive screening guidelines of their high - penetrance counterparts , and they may require a more individualized plan . 
differences between the number of genes currently tested in widely available germline panels , even compared with the number of genes linked to cancer predisposition as listed in table 2 , underscore the rapidly shifting understanding of clinically pertinent germline genes and the wide differences in opinion about what constitutes a clinically useful gene list . variants noted as rare ( labeled - r in table 2 ) are included for a more comprehensive guide to known germline - related malignancies . 
given the young age at which cancers develop in these patients or the other profound organ dysfunction associated with the respective syndromes , germline variants in such genes are unlikely to be carried through generations . furthermore , these syndromes often have clearly associated features that readily identify them clinically , and genetic testing only conrms a suspected diagnosis . 
one such example is wrn , the gene implicated in werner syndrome ; individuals with this disease display severe growth retardation , lipodystrophy , and progeria that would be obvious on examination . 
although familial inheritance of these genes has on occasion been described , such cases should be regarded as the rare exception rather than the rule . currently available somatic variant panels somatic variant panels test many more genes than their germline counterparts do . 
some prominent somatic tests are caris molecular intelligence ( caris life sciences , irving , tx ) , foundationone cdx ( foundation medicine , cambridge , ma ) , genpath onkosight ( genpath oncology , elmwood park , nj ) , msk - impact ( memorial sloan kettering cancer center , new york city , ny ) , omniseq comprehensive ( omniseq corporation , buffalo , ny ) , and tempus xt ( tempus labs , chicago , il )  . 
table 4 lists the number of genes in these somatic panels and the number of genes in each panel with germline implications ( according to table 2 ) at the time of publication . 
in general , a notable number of genes with germline implications are sequenced within common somatic panels . importantly , however , no somatic panel covers all known genes of germline importance , and sizeable numbers of cancer - susceptibility genes are excluded . currently available germline variant panels discussion several companies offer panels that test genes linked to hereditary cancer for various body systems . 
well - established companies with longer commercial track records include ambry genetics ( aliso viejo , ca ) , genedx ( gaithersburg , md ) , invitae ( san francisco , ca ) , and myriad genetics ( salt lake city , ut )  . 
criteria for inclusion of a company in this summary were a primary focus in commercial clinical laboratory improvement amendmentscertied germline testing and exclusion of direct - to - consumer testing or testing several cancer - related genes hold germline implications , and these genes are not uniformly included in currently available germline panel tests ( table 3 )  . 
given the state of current germline testing guidelines , which are syndrome based , and available commercial germline panels , which increasingly are organ - system based , a degree of disconnect between what is clinically relevant and what is offered with germline panels is to be expected . 
our group found that tumor sequencing had a notable number of potential germline variants and that referrals based on somatic variant sequencing could reveal otherwise unknown germline variants.22 within the 315 - gene panel used for the initial 222 - patient cohort , 41 genes ( 13% ) were classied as genes known to cause cancer susceptibility when mutated in the germline . 
coverage of genes within comprehensive or body systemspecic panel offerings from each major germline testing company ambry cancer type genedx invitae myriad * breast / gynecologic colorectal melanoma pancreatic prostate renal frequently somatically mutated in tumors , including tp53 , apc , and cdkn2a , were excluded , 91 patients ( 41% ) had a potential germline variant . 
twenty - three patients ( 10% ) were evaluated by genetics professionals ; three genetics referrals resulted directly from somatic testing results , which ultimately yielded one previously unknown germline variant . 
with formal integration of medical genetics into somatic testing review by the genomics tumor board at our institution , the overall percentage of referrals to genetics increased from 15% to 33% , and 41% of those referrals were the direct result of a somatic test review.23 in another study , speare et al24 reviewed 74 germline tests that followed identication of somatic variants in the tumor specimens of 54 patients and found that 10 variants ( 13.5% ) were conrmed in the germline . 
last , schrader et al25 surveyed germline variants in 187 genes that overlapped with a concurrent 341 - gene tumor somatic panel and identied pathogenic germline variants in 246 ( 15.7% ) of 1 , 566 patients . 
moreover , of the 198 individuals with variants in genes specically associated with increased cancer risk , only 81 of these germline changes ( 40.9% ) were concordant with the tumor type . 
that is , more than half of the patients who had pathogenic germline variants likely would not have had a recommendation for germline testing of that particular gene on the basis of their cancer type alone . 
in our own data , a high proportion of patients who were discovered by somatic tumor testing alone to carry a germline pathogenic variant ( ve of seven patients , or 71.4% ) did not meet any guidelinebased genetic testing criteria.23 together , these data demonstrate that somatic variant sequencing can inform germline testing and act as a screening tool for inherited germline carrier status , which suggests an additional clinical purpose for somatic variant testing separate from the intended goal of screening for possible targeted therapies . * myriad myrisk simultaneously tests 28 genes linked to hereditary cancers in various body systems . 
although some of these tests ask for blood or saliva samples and can test germline variants , they are primarily advertised as panels used to test tumor samples for somatic variants . abbreviation : mskcc , memorial sloan kettering cancer center . in a 1 , 000 - patient cohort with tumor and normal dna sequenced with a 202 - gene panel , meric - bernstam et al20 reported 43 patients ( 4.3% ) with potentially germline variants . 
more than half of these germline variantpositive individuals ( 101 patients ) would not have met guideline - based criteria for clinical germline testing . these studies add credence to the idea that the identication of germline variants from somatic testing can benet patients who would not otherwise have been identied by means of striking personal or family histories and would likely identify inherited cancer susceptibility in additional patients that targeted germline panel or syndrome testing alone may miss . although somatic variant testing can unearth germline variants that traditional means of screening have not , it is important to point out that some common types of germline variants are not picked up with the current technology used for somatic sequencing . 
large rearrangements , inversions , promoter variants , and pseudogene differentiation are not consistently addressed with current somatic sequencing . thus , a germline variant that involves a large rearrangement of brca or is within pms2 , which is notoriously difcult to distinguish from its pseudogene , may be missed these genes or misinterpreted despite the inclusion of within the somatic test panel.26 , 27 despite technical differences between germline and somatic testing , somatic sequencing still has promise as a clinically useful , but not independently adequate , tool for the screening of inherited cancer predisposition . 
somatic tumor sequencing may be considered additive to a proper family history and of particular utility in screening the subset of patients whose family or tumor histology would not otherwise meet traditional germline genetic testing criteria . tables 3 and 4 demonstrate the complexity of current offerings in germline and somatic variant testing . 
even within the category of commercial germline testing , the composition of clinically relevant genes within panels designed for the same organ ( eg , breast ) varies widely from company to company . 
these tables underscore the difculty of interpreting exactly which genes are clinically relevant , whether in a germline or somatic setting , and in some ways reect the issues of offering tests in a eld with a rapidly expanding knowledge base . 
correspondingly , one of the largest challenges in the writing of this review was the expansive and rapidly changing nature of both genes and tumors , which require multidisciplinary expertise and multiple revisions to interpret emerging data . although these tables are designed as a foundational primer specically for the oncologist and should serve well as a quick reference in clinic , the involvement of genetic counselors whenever available in the interpretation of germline implications of somatic testing and the orders for follow - up germline testing is recommended . in conclusion , although family history remains the most reliable screening tool for inherited cancer predisposition syndromes , several studies suggest that a clinically notable subset of germline carriers would be missed by family history alone . because limited family history or an incomplete gene penetrance can result in ambiguity , family historybased germline testing alone may be inadequate to completely assess a patients , and the familys , hereditary cancer risk . 
the plethora of cancer susceptibility genes tested in widespread somatic testing tumor panels makes incidental germline ndings likely , and numerous studies have conrmed that somatic testing can be a useful , but not fully adequate , screen for germline variants . 
sohal , pauline funchain collection and assembly of data : zade akras , brandon bungo , brandie h . leach , jessica marquard , manmeet ahluwalia , hetty carraway , davendra p.s. 
leach consulting or advisory role : invitae speakers ' bureau : myriad genetics references manmeet ahluwalia stock and other ownership interests : mimivax honoraria : prime oncology , elsevier , itamar medical ( i ) consulting or advisory role : monteris medical , astrazeneca , bristol - myers squibb , abbvie , cbt pharmaceuticals , kadmon , vbi vaccines research funding : novartis , tracon pharma , novocure , spectrum pharmaceuticals , lilly , imclone , boehringer ingelheim , astrazeneca hetty carraway consulting or advisory role : amgen , agios , myriad genetics , celgene speakers ' bureau : baxalta , celgene , novartis , jazz pharmaceuticals research funding : celgene travel , accommodations , expenses : celgene , agios , jazz pharmaceuticals , novartis , baxalta petros grivas consulting or advisory role : genentech , merck , bristol - myers squibb , astrazeneca , biocept , clovis oncology , emd serono , seattle genetics , foundation medicine , driver , pzer , qed therapeutics , heron speakers ' bureau : genentech , bristol - myers squibb research funding : mirati therapeutics ( inst ) , genentech ( inst ) , roche ( inst ) , merck ( inst ) , oncogenex ( inst ) , bayer ( inst ) , pzer ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) davendra p.s. 
sohal honoraria : foundation medicine consulting or advisory role : perthera research funding : novartis ( inst ) , celgene ( inst ) , oncomed ( inst ) , bayer ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) travel , accommodations , expenses : foundation medicine pauline funchain consulting or advisory role : eisai no other potential conicts of interest were reported stratton mr : exploring the genomes of cancer cells : progress and promise . 
science 331 : 1553 - 1558 , 2011 friedman aa , letai a , fisher de , et al : precision medicine for cancer with next - generation functional diagnostics . 
nat rev cancer 15 : 747 - 756 , 2015 kamps r , brando rd , bosch bj , et al : next - generation sequencing in oncology : genetic diagnosis , risk prediction and cancer classication . 
nature 470 : 204 - 213 , 2011 biesecker lg : opportunities and challenges for the integration of massively parallel genomic sequencing into clinical practice : lessons from the clinseq project . genet med 14 : 393 - 398 , 2012 castro e , goh c , leongamornlert d , et al : effect of brca mutations on metastatic relapse and cause - specic survival after radical treatment for localised prostate cancer . 
n engl j med 373 : 1697 - 1708 , 2015 le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 lu kh , wood me , daniels m , et al : american society of clinical oncology expert statement : collection and use of a cancer family history for oncology providers . j clin oncol 32 : 833 - 840 , 2014 10 . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
carlo mi , zhang l , mandelker d , et al : cancer predisposing germline mutations in patients ( pts ) with urothelial cancer ( uc ) of the renal pelvis ( r - p ) , ureter ( u ) and bladder ( b )  . 
catenacci dvt , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 16 . 
cheon jy , mozersky j , cook - deegan r : variants of uncertain signicance in brca : a harbinger of ethical and policy issues to come ? genome med 6 : 121 , 2014 19 . 
meric - bernstam f , brusco l , daniels m , et al : incidental germline variants in 1 , 000 advanced cancers on a prospective somatic genomic proling protocol . 
pearlman r , frankel wl , swanson b , et al : prevalence and spectrum of germline cancer susceptibility gene mutations among patients with early - onset oncol 27 : 795 - 800 , 2016 colorectal cancer . 
klek s , heald b , milinovich a , et al : genetic counseling ( gc ) and germline ( gl ) testing rates after adoption of an integrated clinical cancer genetics ( ccg ) approach to genomics tumor board ( gtb )  . 
this study aimed to describe the hr pathway mutations and hrd status and determine their association with treatment response and outcome in patients with pdac . patients and methods we performed a retrospective analysis of tumor samples from patients treated at indiana university for locally advanced or metastatic pdac . 
patients were included if they received gemcitabine plus nanoparticle albumin - bound paclitaxel ( control ) or fluorouracil , oxaliplatin , leucovorin , and irinotecan ( folfirinox ) and had adequate follow - up to assess survival and response to therapy . 
tumor analysis generated a three - biomarker hrd score and mutation data for 44 genes . results ninety - one samples met inclusion criteria , and 78 samples ( formalin - fixed paraffinembedded , n = 15 ; fine - needle aspiration , n = 63 ) generated mutation data . 
hrd analysis was successful for 57 samples ( hrd score : median , 18 ; range , 5 to 61 ) ; the primary cause of failure was low tumor cellularity . 
2018 by american society of clinical oncology introduction pancreatic ductal adenocarcinoma ( pdac ) is the fourth leading cause of cancer - related mortality in the united states.1 most patients present with advanced disease where palliative chemotherapy is minimally effective with high rates of toxicity , and the lack of meaningful benefit associated with targeted therapy continues to be a challenge.2 gemcitabine plus nanoparticle albumin - bound ( nab ) paclitaxel ( g + nab - p ) and fluorouracil , oxaliplatin , leucovorin , and irinotecan ( folfirinox ) are commonly used first - line treatment regimens for advanced disease , with objective response rates of 23% to 31% and median overall survival ( os ) times of , 1 year.3 , 4 kras and tp53 mutations remain the most common molecular abnormalities in pdac , 5 in the absence of effective therapy targeting these mutations . 
genomic analysis has revealed the presence of low - frequency , potentially actionable mutations in patients with pdac6 ; 15% of patients with pdac may carry a mutation in the safi shahda kirsten m . 
therefore , a score of 42 was not chosen as a cutoff in this study ; instead , we decided to evaluate the range of scores and correlate outcome based on hrd scores greater than and less than the median , without intending to establish the median as the cutoff . data collection data were retrieved from a retrospective database ( under a separate irb - approved protocol ) of patients who were diagnosed with pdac and who were partially or completely observed at our institution . 
the data were housed in an oncore ( forte research systems , madison , wi ) database per institutional guidelines . determination of radiographic response and outcome the principal investigator reviewed all images of eligible patients and analyzed response to therapy per response evaluation criteria in solid tumors ( recist ) v1.1. 
median follow - up time for the 16 patients without progression was 9 months ( 11 months for the six patients without progression who were alive at end of study )  . 
pfs and os were calculated from the time of initiating second - line therapy . tissue samples the direct smears prepared from the pancreatic fine - needle aspirates ( fna ) were screened by a cytopathologist ( a.a.i. ) to assure adequacy for molecular testing . 
 formalin - fixed paraffin - embedded ( ffpe ) cell blocks were prepared in a subset of the fnas . the hematoxylin and eosinstained sections cut from those blocks were also examined by a cytopathologist ( a.a.i. ) , and the block was considered acceptable for molecular testing if the estimated tumor cellularity was at least 20% . 
either the entire paraffin cell block or sections cut from the block ( one 4to 5 - mm hematoxylin and eosin slide followed by five consecutive 10 - mm unstained slides ) were submitted for analysis . tissue processing and dna extraction ffpe blocks and fna smears from pretreatment samples were retrieved . 
mutations identified were only included in the analysis if they were classified as deleterious or suspected deleterious on the basis of previously described criteria.21 to calculate the hrd score for samples analyzed by custom hybridization sequencing assay , reads covering snp positions were used to generate allelic imbalance profiles as described previously.14 hrd score was defined as the unweighted sum of loh , tai , and lst scores ( hrd = loh + tai + lst )  . statistical analysis clinical characteristics were compared between treatment groups using nonparametric methods ( wilcoxon rank sum or fishers exact test )  . 
response was coded as a binary variable ( complete response [ cr ] + partial response [ pr ] v stable disease [ sd ] + progressive disease [ pd ] or cr + pr v pd , unless otherwise noted ) , and logistic regression analysis was used to test association with clinical and molecular variables . 
hrd score was dichotomized at the median of 18 ( score , or > 18 ) , and median survival times were estimated using kaplan - meier curves compared by log - rank tests . 
all p values are two - sided , with significance set at p = .05. study approval and ethical considerations this was a retrospective analysis , and at the time of analysis , most patients had died as a result of the advanced nature of their illness . 
patients received care at the discretion of their treating oncologist , with genetic counseling and testing as deemed appropriate . results study population ninety - one patients met inclusion criteria , of whom seven had inadequate tissue for analysis after a second screening process by a pathologist from myriad genetics , 14 had ffpe tissue , and 70 had fna ( fig 1 )  . patients characteristics and treatment patient characteristics are listed in table 1 . 
summary of sample screening and number of samples used in the final analysis . hrd , homologous recombination deficiency . tumor samples ( n = 91 ) final clinical data merged with molecular results ( n = 84 ) inadequate tissue for molecular analysis ( n = 7 ) mutation screen and hrd score failed ( n = 6 ) mutation screen passed ( n = 78 ) brca1 / 2 mutation ( n = 6 ) brca1 / 2 wild type ( n = 72 ) hrd score failed ( n = 1 ) hrd score passed ( n = 5 ) hrd score failed ( n = 20 ) hrd score passed ( n = 52 ) mutant with no hrd score ( n = 1 ) mutants with hrd score ( n = 5 ) wild type with no hrd score ( n = 20 ) wild type with hrd score ( n = 52 ) 5 to 61 , with a median score of 18 . 
six brca1 / 2 mutants were detected in this cohort , and hrd score analysis was successful in five of six patients , with scores ranging from 13 to 61 and a median score of 44 . 
loss of the second allele of the mutant locus via either loh or a second deleterious mutation was observed in three of the six mutant samples , with hrd scores of 43 , 52 , and 53 , respectively . 
in comparison , the median hrd score observed in brca1 / 2 mutation carriers with breast or ovarian tumors was 65 , suggesting that the distribution of hrd scores may differ between pdac and these other tumor types , consistent with our preclinical observations . description of brca mutation functionality and pathogenicity six patients harbored brca mutations , four brca1 mutations and two brca2 mutations . individual mutations and hrd scores associated with those mutations are listed in table 2 . association of hrd with response to folfirinox for the purpose of this study we explored the following two scenarios , which were disease response defined as cr + pr versus sd + pd or cr + pr versus pd ( fig 2 )  . 
the composite variables that were assessed were any pathogenic mutation regardless of the status of the second allele and any brca1 / 2 mutation regardless of the status of the second allele against response , pfs , and os . 
in a subgroup analysis of metastatic status , with or without adjusting for treatment , hrd score was not significant for any of the outcomes ; however , the sample size was not large enough to test whether hrd behaves differently in these two groups . discussion this is the first study to our knowledge to evaluate the relationship between hr gene mutations , hrd score , and response to chemotherapy in patients with pdac . 
higher hrd score was correlated with brca1 / 2 mutations but was not associated with the presence of other hr brca1 mutation brca2 mutation brca1 / 2 wild type brca1 mutation brca2 mutation brca1 / 2 wild type fig 2 . 
 ( a ) complete response ( cr ) or partial response ( pr ) versus stable disease or progressive disease ( pd ) , and ( b ) cr or pr versus pd . 
distribution of homologous recombination deficiency ( hrd ) scores across samples of locally advanced ( la ) and metastatic pancreatic ductal adenocarcinoma ( pdac )  . max , maximum ; min , minimum ; qu , quartile ; sd , standard deviation . time from start of metastatic therapy ( months ) pathway mutations . 
one possible explanation for the absence of an elevated hrd score despite the presence of an hr pathway mutation is the retained functional allele in the affected genes . although conducted retrospectively , our study demonstrates the feasibility of performing genomic analysis on fna samples available from patients with pdac . 
on the contrary , however , this study also highlights the challenge of conducting correlative studies in patients with pdac ; most patients with pancreatic malignancies are diagnosed based on endoscopic ultrasound - guided fna only.22 in addition , high nontumor content , likely as a result of abundant desmoplastic stroma , often led to low dna content and thus a high assay failure rate . interestingly , we experienced a higher failure rate associated with core needle biopsy samples as opposed to fna samples , as a result of higher levels of nontumor dna content , even after macrodissection . 
 despite the low incidence of dna repair deficiency in pdac , it continues to represent an attractive target for drug development.23 several clinical trials using single agents or drug combinations are ongoing . 
in addition , patients with pdac tend to have a higher symptom burden and experience rapid progression after first - line therapy , frequently prohibiting second - line therapy.3 , 4 therefore , the optimal timing for testing such methods to select patients for subsequent therapies will likely be early in the disease process to inform secondline therapy.24 although our study does not address the presence of heterogeneity between the primary and metastatic lesions , some literature exists regarding hrd heterogeneity in other tumor types . for example , a study of patients with triplenegative breast cancer compared hr score in three different areas from the same primary tumor.25 overall , there was no significant difference among these samples , and the authors concluded that heterogeneity for hrd metrics was small and did not influence hrd score or status from three samples in the same tumor . whether hrd is more common in metastatic sites remains unknown in pdac ; however , a higher rate of germline mutations associated with dna repair genes ( without examining hrd score ) was found in metastatic prostate cancer when compared with localized disease.26 this study has limitations . 
it is a single - institution , nonrandomized , retrospective study comparing two commonly used chemotherapy regimens and including patients who had locally advanced and metastatic disease , which may carry different biology and represent a challenge in assessing response to therapy in locally advanced pdac . 
we had a relatively high assay failure rate in both fna and ffpe , although it was higher in the ffpe samples . in conclusion , this study did not demonstrate a correlation between hrd score and radiographic response to platinum - based therapy in patients with pdac . 
although hr gene mutations or hrd score may represent targets for drug development in pdac , larger prospective studies may be needed to evaluate the utility of these markers and their correlation with response to dna - damaging agents . 
for more information about ascos conflict of interest policy , please refer to or ascopubs.org / po / author - center . safi shahda consulting or advisory role : merrimack , bayer research funding : myriad genetics kirsten m . 
timms employment : myriad genetics stock and other ownership interests : myriad genetics patents , royalties , other intellectual property : austria ( e840080 , 3012329 ) , china pr ( zl 201280070358.0 ) , denmark , european patent convention , finland , france , great britain , ireland , the netherlands , spain , sweden , and switzerland ( 2582847 , 3012329 ) , germany ( 602011031723.7 , 3012329 ) , italy ( 502016000131029 , 3012329 ) , japan ( 6117194 ) , new zealand ( 625468 ) , united states ( 9 , 574 , 229 ; 9 , 279 , 156 ; 9 , 388 , 427 ) travel , accommodations , expenses : myriad genetics ashley a . 
 milan radovich no relationship to disclose sulfikar ibrahim no relationship to disclose brian allen employment : myriad genetics , grail stock and other ownership interests : myriad genetics , grail bert h . 
oneil , indiana university school of medicine , indianapolis ; ashley a . ibrahim and sulfikar ibrahim , indiana university health ball memorial hospital , muncie , in ; and kirsten m . 
moore mj , goldstein d , hamm j , et al : erlotinib plus gemcitabine compared with gemcitabine alone in patients with advanced pancreatic cancer : a phase iii trial of the national cancer institute of canada clinical trials group . j clin oncol 25 : 1960 - 1966 , 2007 3 . 
von hoff dd , ervin t , arena fp , et al : increased survival in pancreatic cancer with nab - paclitaxel plus gemcitabine . med 364 : 1817 - 1825 , 2011 n engl j med 369 : 1691 - 1703 , 2013 jones s , zhang x , parsons dw , et al : core signaling pathways in human pancreatic cancers revealed by global genomic analyses . 
risch ha , mclaughlin jr , cole de , et al : population brca1 and brca2 mutation frequencies and cancer penetrances : a kin - cohort study in ontario , canada . 
yang d , khan s , sun y , et al : association of brca1 and brca2 mutations with survival , chemotherapy sensitivity , and gene mutator phenotype in patients with ovarian cancer . 
mccabe n , turner nc , lord cj , et al : deficiency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deficiency among breast cancer subtypes . 
telli ml , timms km , reid j , et al : homologous recombination deficiency score predicts response to platinumcontaining neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
mills gb , timms km , reid je , et al : homologous recombination deficiency score shows superior association with outcome compared with its individual score components in platinum - treated serous ovarian cancer . 
 alk testing trends and patterns among community practices in the united states purpose targeted therapy of alk in patients with metastatic nonsquamous nonsmall - cell lung cancer ( nsclc ) and alk rearrangements improves outcomes compared with chemotherapy . 
logistic regression was used to examine the association between demographic and clinical characteristics and testing for alk rearrangements . results of 31 , 483 patients analyzed from the database , 16 , 726 patients ( 53.1% ) were tested for alk rearrangements . 
median ( interquartile range ) time from laboratory receipt of sample to first alk test result was 7 ( 7 ) days ; median time from advanced diagnosis to first alk test result was 25 ( 29 ) days . 
patients who were older , male , had a history of smoking , lived in non - western us regions , and who had recurrent disease or squamous histology were less likely to be tested for alk . 
2018 by american society of clinical oncology introduction recent advances in molecular genetics have increased the opportunity for precision medicine in metastatic nonsquamous nonsmall - cell lung cancer ( nsclc )  . 
for instance , translocation of the anaplastic lymphoma kinase ( alk ) gene is found in approximately 2% to 8% of all patients with nsclc and occurs primarily in patients who are never - smokers or light ex - smokers with adenocarcinoma histology.1 - 4 in addition to representing a distinct molecular nsclc subtype , alk rearrangements are indicative of tumor cell susceptibility to alk inhibitors.5 targeted inhibition of alk in patients with alk rearrangements can decrease tumor burden and significantly increase progression - free survival compared with chemotherapy.3 , 6 the first alk inhibitor , crizotinib , along with the vysis alk break apart fish probe kit , was given accelerated approval by the us food and drug administration ( fda ) in 2011 . 
since then , other firstand second - generation alk inhibitors have been approved , including ceritinib in 2014 and alectinib in 2015 . the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology ( cap / iaslc / amp ) molecular testing and national comprehensive cancer network ( nccn ) peter b . 
 nsclc treatment guidelines recommend testing for alk , egfr , and ros1 in lung adenocarcinomas and in nsclc where an adenocarcinoma component cannot be excluded , regardless of clinical characteristics.1 , 7 , 8 fluorescent in situ hybridization ( fish ) or immunohistochemistry ( ihc ) are assays recommended by cap / iaslc / amp guidelines for the detection of alk rearrangements before selection of targeted therapy.8 in addition to fish , the alk ( d5f3 ) cdx assay ( ventana medical systems , tucson , az ) and foundationone cdx ( foundation medicine , cambridge , ma ) are ihc and next - generation sequencing ( ngs ) assays , respectively , that are fda approved to identify patients eligible for alk inhibitor treatment . 
alk rearrangements could also be detected using polymerase chain reaction , but no fda - approved assay is available to date , and this method is not currently recommended in guidelines.8 numerous challenges associated with molecular testing of malignancies may affect adoption of molecular testing guidelines and performance of alk testing in clinical practice . 
a major challenge in molecular testing is inadequate tissue samples.9 , 10 for example , in a study that examined the workflow of molecular testing for 157 lung cancer specimens , successful testing of all molecular targets could not be completed for 19% of specimens.11 additional challenges may include tumor heterogeneity , complex results that require multidisciplinary input , education and training of laboratory and staff , availability of assays , and patient affordability.9 , 10 in a retrospective analysis of 814 patients in new jersey and maryland with nonsquamous nsclc who were identified using the cota database ( cota , new york , ny ) , which extracts and organizes data from electronic health records , only 65% underwent alk testing , indicating limited integration of molecular testing recommendations into clinical practice.12 given the clinical benefit of alk inhibitor therapy in patients with nsclc with alk rearrangements , evaluation of alk testing using large , real - world , geographically diverse data sources is warranted . 
the objective of this study was to assess real - world alk testing patterns among community practices in the united states in patients with advanced nsclc from january 2011 through may 2017 . methods study overview and database description this was a retrospective analysis using the flatiron health electronic health record ( ehr ) derived database , a longitudinal , demographically and geographically diverse database.13 the database includes > 265 cancer clinics ( approximately 800 sites of care ) representing more than 2 million active us patients with cancer available for analysis . 
the current analysis was limited to data from community practices and included 34 , 911 patients diagnosed with advanced nsclc ( stage iiib or iv by american joint committee on cancer 7th edition ) from january 2011 through may 2017 . 
insurance information was categorized into commercial ( including those with dual medicare or medicaid coverage ) , medicare ( including dual medicaid coverage ) , medicaid , and other / unknown . 
 ( % ) unless otherwise noted . abbreviations : alk , anaplastic lymphoma kinase ; iqr , interquartile range , q3 - q1 ; nos , not otherwise specified ; nsclc , nonsmall - cell lung cancer . date specimens were received by the laboratory to the test report date . data analysis statistical analyses were primarily descriptive , with frequencies calculated for categorical data and means , medians , interquartile ranges ( iqrs ) , and standard deviations ( sds ) calculated for continuous data . 
odds ratios ( ors ) and 95% cis were calculated by logistic regression to examine the association between demographic and clinical characteristics and testing for alk rearrangements . results patient characteristics overall , 34 , 911 patients with advanced nsclc were identified from the flatiron health ehr - derived database from january 2011 through may 2017 ; 31 , 483 met the selection criteria and were included in the analysis . 
most of the samples used for alk testing were tissue ( 93.7% ; 15 , 664 of 16 , 726 ) ; 2.6% ( 439 of 16 , 726 ) were blood , and the rest were unknown . 
of the total 21 , 639 patients with nonsquamous histology , 66.9% ( 14 , 478 of 21 , 639 ) were tested for alk , and of the 7 , 923 patients with squamous histology , 18.5% ( 1 , 466 of 7 , 923 ) were tested for alk . 
 among the patients who had nonsquamous histology and who were not tested for alk , 87.2% ( 6 , 025 of 6 , 913 ) had a history of smoking , and among those with a squamous histology and who were either tested or not tested for alk , 91.5% ( 1 , 320 of 1 , 443 ) and 95.6% ( 5 , 992 of 6 , 268 ) , respectively , had a history of smoking . 
overall , 16 , 726 of 31 , 483 ( 53.1% ) patients were tested for alk , with 633 of 16 , 726 ( 3.8% ) patients positive for alk ( 581 of 14 , 478 [ 4.0% ] nonsquamous histology , 24 of 1 , 466 [ 1.6% ] squamous histology , and 28 of 782 [ 3.6% ] not otherwise specified histology )  . alk testing patterns alk testing rates by year of advanced diagnosis steadily increased over time from an average of 32.4% ( 1 , 093 of 3 , 371 ) in 2011 to 62.1% ( 3 , 526 of 5 , 680 ) in 2016 for all patients with advanced nsclc , from 41.1% ( 935 of 2 , 273 ) in 2011 to 75.1% ( 2 , 947 of 3 , 924 ) in 2016 for patients with nonsquamous histology , and from 12.1% ( 101 of 832 ) in 2011 to 26.5% ( 372 of 1 , 403 ) in 2016 for patients with squamous histology ( fig 1a )  . 
with test 2012 2014 year 178 201 245 368 395 471 483 446 525 595 593 625 665 765 717 746 728 801 891 820 860 805 787 702 631 2015 2013 2016 2017 squamous , no . 
 age , years 55 - 64 v < 55 65 - 74 v < 55 75 - 84 v < 55 85 + v < 55 female v male race asian v white black or african american v white other race v white missing v white hispanic v non - hispanic ethnicity histology nos v non squamous squamous v non squamous disease type recurrent v de novo unknown v de novo smoking status history of smoking v no history unknown history v no history insurance medicaid v commercial medicare v commercial other v commercial region midwest v west northeast v west south v west missing v west fig 2 . 
the overall median ( iqr ) turnaround time from the date samples were received by the laboratory to the test report date was 7 ( 7 ) days and ranged from 6 days for fish to 12 days for ngs ( table 2 )  . 
the overall median ( iqr ) time from advanced diagnosis date to first alk test result date was 25 ( 29 ) days ( table 2 ) and differed by type of test and insurance type . 
 median ( iqr ) times from advanced diagnosis to first alk test result for fish were 20 ( 19 ) , 22 ( 31 ) , and 23 ( 27 ) days for commercial insurance , medicaid , and medicare , respectively , and for ngs were 37 ( 34 ) , 58 ( 159 ) , and 41 ( 105 ) days , respectively ( table 2 )  . 
on the basis of tests conducted by foundation medicine ( cambridge , ma ) laboratory , the overall agreement between ngs and fish was 97.6% ( 360 of 369 )  . 
the percentage of tests positive by ngs that were initially negative by fish was 1.9% ( 7 of 369 )  . treatment before alk test results among patients tested for alk who had valid tissue collection and test result dates , 21.5% ( 3 , 290 of 15 , 320 ) initiated therapy before receiving their first alk test results . 
percentage of patients initiating treatment before first anaplastic lymphoma kinase ( alk ) test result . discussion this retrospective analysis of patients with advanced nsclc treated at community practices between january 2011 and may 2017 found that 53.1% of all patients , 66.9% of patients with nonsquamous histology , and 18.5% of patients with squamous histology were tested for alk rearrangements . 
cap / iaslc / amp and nccn guidelines recommend alk testing be conducted for patients with nsclc that has an adenocarcinoma component.7 , 8 however , alk testing may also be considered for patients with nsclc who have mixed histology , who are of young age , or who are without a history of tobacco exposure.7 , 8 the current analysis confirms and extends the findings of a retrospective analysis of 814 patients with nonsquamous nsclc treated in community centers in the united states , which found an overall 65% alk testing rate for the years 2013 to 2015.12 alk testing rates increased over time , reaching 75% in 2016 in patients with nonsquamous histology , indicating improvement in adherence to alk testing recommendations as well as physician recognition of the clinical benefits of alk targeted therapy . 
 the reasons for lack of testing were not captured in the flatiron health database , although possible reasons may include evolution of best practices and guidelines across the study period , patient disease severity , and insufficient tissue ( as was observed in 16% to 21% of patients in other nsclc studies ) .4 , 14 , 15 blood - based assays could address the issue of insufficient tissue , and research in this field is emerging.16 patients with squamous histology were less likely to be alk tested , which is consistent with guidelines that state there is no evidence to recommend alk testing in patients with typical squamous histology who do not have other clinical features to prompt alk testing.7 , 8 in the current analysis , testing rates increased over time in patients with squamous histology , and , overall , 1.6% had an alk rearrangement . 
the increased testing rate for patients with squamous histology may be due to a general increase in the perceived benefit of alk inhibitors for alk - positive nsclc by physicians or to the release of cap / iaslc / amp and nccn guidelines that suggest selectively testing patients with squamous histology , such as patients who are never - smokers or former light smokers.1 , 17 the likelihood of alk testing decreased as age increased . 
patients with alk - positive disease in clinical studies tended to be younger , nonsmokers , and have adenocarcinoma , perhaps increasing the likelihood that these patients would have been tested for alk positivity despite guidelines recommending that all patients with nonsquamous disease be tested . 
in addition , the current analysis suggests there may also be socioeconomic barriers to alk testing ; medicaid patients were 40% less likely to be tested than patients with commercial insurance . 
collectively , these results suggest that additional education on alk testing in the community oncology setting is warranted . in our study , fish was the most commonly ordered genomic testing method , which was not unexpected , given that fish was the only recommended and fda - approved assay during the majority of the time period for our study . 
 updated 2018 cap / iaslc / amp and nccn guidelines now recommend fish or ihc for alk testing.7 , 8 with the rapidly changing landscape of fda - approved assays , such as the 2017 approval of the foundationone cdx ngs assay , the distribution of assays used will likely continue to evolve . 
indeed , in our study we observed a trend of declining use of fish and an increase in the use of ngs and , to a lesser extent , ihc . 
there is a trend in clinical practice to use ngs as the primary testing method to identify all targetable alterations.18 , 19 turnaround times for laboratory receipt of sample to test results were consistently less than 2 weeks across different test types , including ngs . 
the reasons for this variation are unknown ; however , potential reasons for longer times for some patients may include the ordering process for biomarker testing , sample shipment to the laboratory , and sample processing . 
for example , a previous study in metastatic colon cancer found that testing performed at a nonlocal or noncancer centeraffiliated laboratory was associated with greater likelihood of a testing delay.20 the current study was conducted in the community setting , and the majority of biomarker testing was done in commercial laboratories , which may be one of the possible explanations for the observed variance in times . 
in addition , the 14 - day rule may also have contributed to the variation in times for some medicare patients , because testing may have been delayed to avoid reimbursement complexities . numerically , ngs had a longer time from advanced diagnosis to alk test result for both medicare and medicaid patients . 
given that turnaround times for ngs were similar across insurance types and only accounted for a minor portion of the time from advanced diagnosis to alk test result , this may imply that delays in ordering ngs , which was not an approved test during the study period , may have existed . 
additional research is needed to determine if this trend will continue in the future , particularly given the 2017 simultaneous fda approval of ngs tests for tumor profiling and centers for medicare & medicaid services approval of coverage for fda - approved ngs tests , which may substantially improve the ability to provide more timely access to ngs testing.21 , 22 the lack of alk testing or delay in results may have serious clinical implications , given the efficacy of alk inhibitors in patients with alk rearrangements.3 , 6 , 23 , 24 in a head - to - head comparison , a second - generation alk inhibitor ( alectinib ) exhibited a median progression - free survival of 34.8 months , compared with 10.9 months with a first - generation alk inhibitor ( crizotinib ) .24 , 25 delays in alk testing may potentially lead to delayed treatment , 15 and , as is seen in other cancers , delays in treatment may lead to poorer outcomes.26 , 27 although additional research is needed to assess the impact of delays on outcomes , specifically in alk - positive nsclc , alk testing is needed to help facilitate timely treatment with an efficacious alk inhibitor . day - level granularity of biomarker testing ordered date is not always available in ehr data , which has limited our ability to interpret and determine reasons for observed delays in testing . 
 last , this study focused on community practices in the united states , and hence the results of this study may not be generalizable to all clinical practices . the results of the current analysis indicate that the frequency of alk testing in patients with advanced nsclc treated in community centers in the united states has increased over time . 
 however , certain subgroups of patients , such as patients receiving medicaid , were less likely to be tested , suggesting that additional education on genomic testing and investigation into socioeconomic barriers is warranted . 
 laura chu employment : genentech stock and other ownership interests : roche ravindra gupta employment : genentech katja schulze employment : genentech stock and other ownership interests : genentech matthew a . 
gubens consulting or advisory role : bristol - myers squibb , ariad pharmaceuticals , genentech , astrazeneca , abbvie , novartis , mersana therapeutics research funding : celgene ( inst ) , merck ( inst ) , novartis ( inst ) , genentech ( inst ) , oncomed ( inst ) acknowledgment medical writing and editorial assistance was provided by erin p . 
illei , johns hopkins university school of medicine , baltimore , md ; william wong , laura chu , ravindra gupta , and katja schulze , genentech , south san francisco ; matthew a . 
gubens , university of california , san francisco , ca ; and ning wu , pro unlimited , boca raton , fl . support supported by genentech , south san francisco , ca . prior presentation presented in part at the international association for the study of lung cancer 18th world conference on lung cancer , yokohama , japan , october 15 - 18 , 2017 . 
lindeman ni , cagle pt , beasley mb , et al : molecular testing guideline for selection of lung cancer patients for egfr and alk tyrosine kinase inhibitors : guideline from the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology . 
korpanty gj , graham dm , vincent md , et al : biomarkers that currently affect clinical practice in lung cancer : egfr , alk , met , ros - 1 , and kras . 
lindeman ni , cagle pt , aisner dl , et al : updated molecular testing guideline for the selection of lung cancer patients for treatment with targeted tyrosine kinase inhibitors : guideline from the college of american pathologists , the international association for the study of lung cancer , and the association for molecular pathology . 
distasio m , chen y , rangachari d , et al : molecular testing turnaround time for non - small cell lung cancer in routine clinicalpractice confirms feasibility of cap / iaslc / amp guideline recommendations : a single - center analysis . 
mayo - de - las - casas c , garzn ibez m , jordana - ariza n , et al : an update on liquid biopsy analysis for diagnostic and monitoring applications in non - small cell lung cancer . 
suh jh , johnson a , albacker l , et al : comprehensive genomic profiling facilitates implementation of the national comprehensive cancer network guidelines for lung cancer biomarker testing and identifies patients who may benefit from enrollment in mechanism - driven clinical trials . 
jensen ts , chin j , baldwin j , et al : proposed decision memo for next generation sequencing ( ngs ) for medicare beneficiaries with advanced cancer ( cag - 00450n )  . 
soria jc , tan dsw , chiari r , et al : first - line ceritinib versus platinum - based chemotherapy in advanced alk - rearranged non - small - cell lung cancer ( ascend - 4 ) : a randomised , open - label , phase 3 study . 
garcia , md3 ; amir momeni - boroujeni , md1 ; qi gao , mls1 ; jeeyeon baik , ba1 ; dory londono , bs1 ; ryma benayed , phd1 ; allison sigler , ma1 ; michael haddadin , md2 ; alexander v . 
goldberg , md , phd2 ; yanming zhang , md1 ; wenbin xiao , md , phd1 ; and caleb ho , md1 introduction ighcytokine receptorlike factor 2 ( crlf2 ) rearrangement is the most common mechanism of overexpression of crlf2 in precursor b - cell acute lymphoblastic leukemia ( b - all ) ; however , p2ry8 - crlf2 rearrangement or alternative alterations leading to crlf2 overexpression have also been observed , which are associated with increased relapse rate and progression.1 although many myeloid neoplasms , particularly acute myeloid leukemia ( aml ) , are associated with various recurrent genetic rearrangements and fusions , 2 alterations leading to crlf2 overexpression are exceedingly rare in aml . 
one patient with myelodysplastic syndrome with excess blasts - 1 ( mds - eb1 ) with crlf2 overexpression via multiple copies of an isodicentric y chromosome , without evidence of crlf2 rearrangement , has been reported.3 to our knowledge , we report the rst patient with aml arising from an mds , with a p2ry8 - crlf2 fusion , which responded to a myeloid regimen in a clinical trial of hypomethylating agent and immune checkpoint blockade combination therapy . 
at mskcc , karyotype analysis of the aml bone marrow aspirate specimen showed a normal male karyotype , and fish analysis was negative for the presence of kmt2a ( mll ) , evi1 , and cbfb translocations , and tp53 deletion . 
a targeted nextgeneration sequencing ( nsg ) panel ( msk - impact heme panel ; mskcc , new york , ny ) was performed on the bone marrow specimen obtained at the time of the aml diagnoses , which showed the alterations including mutations in asxl1 , listed in table 1 , kmt2d , runx1 , sf3b1 , tet2 , phf6 , rad21 , and xbp1 . 
evaluation of this bone marrow sample using an anchored multiplex polymerase chain reaction based , targeted rna sequencing assay for detection of fusions ( archer fusionplex , archerdx , boulder , co ) revealed the presence of a fusion between exon 1 of p2ry8 and exon 1 of crlf2 ( fig 1c )  . 
cell sorting , molecular characterization , and immunostaining characterized the myeloid origin of this fusion and subsequent signaling effects . relevance this patient was treated with the novel combination of decitabine and ipilimumab with an outstanding response . 
immune cell inltrates in the bone marrow with treatment suggests the response was related to the immune checkpoint inhibition . additional study of p2ry8 - crlf2 fusions and response to immunotherapy is warranted and could have implications for fusion discovery in novel disease contexts . sorting to isolate the leukemic blasts , myelomonocytic cells , lymphocytes . 
fish using the crlf2 breakand normal apart probe revealed the crlf2 rearrangement in a subset of the myeloid blasts ( 27.5% ) and myelomonocytic cells ( 19.5% ) but not in b cells ( fig 2 )  . fish evaluation of the prior bone marrow biopsy with mdseb1 was also performed , which showed the presence of the p2ry8 - crlf2 rearrangement in 10% of the cells ( appendix fig a1c )  . 
oncoscan array ( thermofisher , waltham , ma ) of the mds - eb1 biopsy did not reveal any unbalanced genomic changes or copy - neutral loss of heterozygosity ( data not shown ) , consistent with the normal fish study observed by the outside institution a year prior . 
targeted ngs sequencing ( msk - impact heme panel ) of the mds - eb1 bone marrow specimen also showed overlapping mutations with the aml bone marrow sample ( table 1 ) , but with acquisition of new mutations ( phf6 , rad21 , xbp1 ) in the aml sample , suggesting a myeloid primed hematopoietic stem cell / progenitor origin and clonal evolution with expansion of the clone with the p2ry8 - crlf2 rearrangement , likely due to acquisition of a loss - of - function mutation in phf6 , which led to downregulation of genes involved in normal b - cell development.4 total rna sequencing of the aml bone marrow specimen further conrmed the presence of the p2ry8 - crlf2 fusion along with overexpression of crlf2 ( fig 3a )  . 
principal component analysis comparing our patient with cohorts of aml or b - all from the target study5 showed that the patients neoplasm clustered with other patients with aml , conrming the myeloid differentiation of the blasts ( fig 3b )  . gene ontology analysis showed transcriptome - wide increases in cytokine - related signaling pathway genes potentially related to the p2ry8 - crlf2 fusion , as well as genes involved in regulating hematopoietic progenitor cell differentiation and the spliceosome ( fig 3c )  . because it is known that stat5 is activated by p2ry8crlf2 fusion in b - all , we performed immunohistochemistry ( ihc ) using phosphorylation - specic antibodies that showed increased stat5 phosphorylation and partial erk phosphorylation but not stat3 phosphorylation ( fig 4a )  . 
gene expression and ihc were largely correlated ; however , the results are interpreted in the context of the importance of signaling in leukemia overall , and these are not necessarily specic for p2ry8 - crlf2 fusion . cell sorting myeloid blasts monocytes 27.5% ( 55 / 200 ) 19.5% ( 22 / 113 ) bone marrow aspirate fluorescence in - situ hybridization 0% ( 0 / 174 ) b lymphocytes crlf2 fusion positive fig 2 . 
 ( b ) principal component analysis plot showing 2 strongest principal components ( pc1 on x - axis and pc2 on y - axis ) from publicly available data from aml ( green dots ) and b - all ( red dots ) patient samples compared with our patient with p2ry8 - crlf2 fusion ( blue dot )  . 
he was consented and enrolled in a study regimen consisting of standard - dose decitabine plus investigational administration of the cytotoxic t - lymphocyte associated protein - 4 ( ctla - 4 ) antagonist , ipilimumab ( clinicaltrials.gov identier : nct02890329 )  . 
after 2 cycles of combination therapy , he achieved complete remission with incomplete count recovery and shortly thereafter a full complete remission ( table 2 ) with negative measurable residual disease ( mrd ) status by a ow cytometric assay with a detection limit of 1 in 2 , 500 cells . 
this was accompanied by a robust molecular response with undetectable levels of the previously detected phf6 , runx1 , tet2 , and rad21 mutations , and a marked reduction in the variant allele frequencies for the mutations asxl1 ( 0.4% ) and sf3b1 ( 1.4% ) , likely representing mrd below the detection limit of ow cytometry . 
ihc was performed on the checkpoint molecules including programmed death ( pd ) - 1 , pd - ligand 1 ( pd - l1 ) and pd - l2 ( fig 4b )  . 
 ( c ) using multiplex immunouorescence microscopy , with digital image analysis , we found that the patients bone marrow was highly enriched with cd8 plus granzyme b ( gzmb ) plus t cells . 
we further identied a population of cd3 + cd4 + t cells at baseline . discussion crlf2 is the protein product of a synonymous gene located in the par1 on the short arm of the x chromosome and the y chromosome . 
it forms a heterodimer with interleukin 7 receptor alpha and is involved in lymphoid signaling pathways . activation of this receptor leads to activation of janus family tyrosine kinases and stat5 . 
deregulated expression of this gene has been described as the characteristic alteration in philadelphia chromosomelike b - all in adolescent and adult patients.7 , 8 russell et al9 showed that this subgroup of b - all has either a translocation juxtaposing the crlf2 to the igh gene on chromosome 14 ( t ( x ; 14 ) ( p22 ; q32 ) or t ( y ; 14 ) ( p11 ; q32 ) ) or a deletion of par1 region , resulting in overexpression of the crlf2 gene . 
this has been observed in down syndromerelated all as well as nondown syndrome all , supporting the cooperation of crlf2 events with other genetic alterations in progression of disease.11 however , irrespective of the clone size , presence of this rearrangement is associated with a higher relapse rate.12 there have been suggestions that the increased relapse rate may be due to other concurrent alterations , such as ikzf1 deletion.13 however , other studies have shown the rearrangement as well as the crlf2 overexpression to be independent predictors of worse outcome in b - all.14 , 15 until now , only one patient with myeloid neoplasm with crlf2 overexpression has been reported . 
however , this patient was associated with multiple copies of an isodicentric y chromosome and not associated with p2ry8crlf2 rearrangement.3 to our knowledge , our patient represents the rst p2ry8 - crlf2 rearrangement myeloid neoplasms , which in our patient was an aml arising from the underlying mds . 
the ow - sorted fish the p2ry8 - crlf2 was not analysis has shown that present in the b lymphocytes of this patient but only in the myeloid - lineage cells ( myeloid blasts and myelomonocytic cells )  . 
in addition , based on the results from total rna sequencing , our patients neoplasm clustered with other patients with aml , providing additional evidence for the myeloid differentiation of the blasts . 
furthermore , the alterations observed in this patient , including the p2ry8affiliations 1department of pathology , memorial sloan kettering cancer center , new york , ny 2leukemia service , department of medicine , memorial sloan kettering cancer center , new york , ny 3department of medical oncology , dana - farber cancer institute , boston , 4department of pathology , brigham and womens hospital , boston , ma crlf2 rearrangement , were present at the mds stage , suggesting a stem cell origin with selective pressure leading to development of aml . phf6 mutations are rare in de novo aml but relatively common in aml - mrc and exceedingly rare in b - all.16 , 17 phf6 and dnmt3a are the most common mutations in mixed phenotype acute leukemias ( mpal ) with t - lineage differentiation.18 phf6 is a critical component in lineage determination of precursor cells , especially between t and b lineages , and it is believed that a functioning phf6 is required for b - cell differentiation leading to selective abundance of this mutation in t - all and mpal with t - lineage differentiation.18 , 19 this notion is further supported by the observation that phf6 suppression leads to impaired tumor progression in b - all.4 it has also been shown that pax5 - decient pro - b cells can undergo myeloid - lineage differentiation in the presence of transcription factors , such as gata or cebpa.20 in our patient , the immunophenotype and rna expression data unequivocally point toward myeloid differentiation . 
although it is difcult to ascertain the functional consequences of the p2ry8 - crlf2 rearrangement and the acquired phf6 mutation at the time of aml transformation , we hypothesize that the two may interact in a way that led to the development of aml instead of b - all . remarkably , this patient with aml - mrc and phf6 , runx1 , tet2 , and rad21 mutations had an mrdnegative complete response by ow cytometry after just 4 cycles of combination decitabine with ipilimumab . 
although the complete results from clinical trials of these agents are needed to evaluate the efcacy and safety of this this patients exceptional response could combination , suggest the unique molecular characteristics of his tumor the p2ry8 - crlf2 may have been important , namely , fusion . 
recent evidence in head and neck cancers with oncogenic chromosomal rearrangements suggests that gene fusions may be a source of immunogenic neoantigens and stimulate t - cell responses that could be unleashed after immune checkpoint blockade.21 this patients t cells were positive for pd - 1 , suggesting a relation to the response to ctla - 4 blockade . 
garcia , wenbin xiao , caleb ho administrative support : jeeyeon baik , allison sigler collection and assembly of data : umut aypar , justin taylor , jacqueline s . garcia , amir momeni - boroujeni , qi gao , dory londono , ryma benayed , michael haddadin , alexander v . 
goldberg , yanming zhang , wenbin xiao , caleb ho data analysis and interpretation : umut aypar , justin taylor , jacqueline s . garcia , amir momeni - boroujeni , alexander v . 
garcia consulting or advisory role : abbvie research funding : abbvie ( inst ) , pzer ( inst ) , genentech ( inst ) , eli lilly ( inst ) maria e . 
arcila honoraria : invivoscribe , biocartis references mikhail roshal honoraria : celgene consulting or advisory role : agios , auron research funding : agios , roche , boehringer ingelheim ana lako employment : bristol - myers squibb scott j . 
rodig honoraria : perkin elmer , bristol - myers squibb consulting or advisory role : bristol - myers squibb research funding : bristol - myers squibb , merck , afmed therapeutics , kite pharma patents , royalties , other intellectual property : patent pending for use of antigalectin - 1 antibodies for diagnostic use travel , accommodations , expenses : roche , bristol - myers squibb aaron d . 
goldberg honoraria : dava oncology consulting or advisory role : abbvie , celgene , daiichi sankyo research funding : abbvie ( inst ) , adc therapeutics ( inst ) , pzer ( inst ) , arog ( inst ) travel , accommodations , expenses : arog open payments link : 1195852 / summary wenbin xiao research funding : stemline therapeutics ( inst ) caleb ho honoraria : invivoscribe travel , accommodations , expenses : invivoscribe no other potential conicts of interest were reported . acknowledgment we acknowledge the members of the memorial sloan kettering cancer center diagnostic molecular laboratory , cytogenetics laboratory , ow cytometry laboratory , and immunohistochemical stain laboratory for their support in performing the relevant assays . schm ah j , fedders b , panzer - gr umayer r , et al : molecular characterization of acute lymphoblastic leukemia with high crlf2 gene expression in childhood . pediatr blood cancer 64 : e26539 , 2017 arber da , orazi a , hasserjian r , et al : the 2016 revision to the world health organization classication of myeloid neoplasms and acute leukemia . 
meacham ce , lawton ln , soto - feliciano ym , et al : a genome - scale in vivo loss - of - function screen identies phf6 as a lineage - specic regulator of leukemia cell therapeutic target . 
nature 555 : 371 - 376 , 2018 patel ss , weirather jl , lipschitz m , et al : the microenvironmental niche in classic hodgkin lymphoma is enriched for ctla - 4 - positive t cells that are pd - 1negative . 
curr opin pharmacol 8 : 249 - 254 , 2008 vesely c , frech c , eckert c , et al : genomic and transcriptional landscape of p2ry8 - crlf2 - positive childhood acute lymphoblastic leukemia . 
leukemia 31 : 1491 - 1501 , 2017 russell lj , capasso m , vater i , et al : deregulated expression of cytokine receptor gene , crlf2 , is involved in lymphoid transformation in b - cell precursor acute lymphoblastic leukemia . 
potter n , jones l , blair h , et al : single - cell analysis identies crlf2 rearrangements as both early and late events in down syndrome and non - down syndrome leukemia . 
morak m , attarbaschi a , fischer s , et al : small sizes and indolent evolutionary dynamics challenge the potential role of p2ry8 - crlf2 - harboring clones as main relapse - driving force in childhood all . 
dou h , chen x , huang y , et al : prognostic signicance of p2ry8 - crlf2 and crlf2 overexpression may vary across risk subgroups of childhood b - cell acute lymphoblastic leukemia . 
fang q , zhao x , li q , et al : ikzf1 alterations and expression of crlf2 predict prognosis in adult chinese patients with b - cell precursor acute lymphoblastic leukemia . 
xiao w , bharadwaj m , levine m , et al : phf6 and dnmt3a mutations are enriched in distinct subgroups of mixed phenotype acute leukemia with t - lineage differentiation . 
presence of the p2ry8 - crlf2 fusion in earlier bone marrow biopsy with myelodysplastic syndrome ( mds )  . ( a ) photomicrographs of the bone marrow biopsy showing mds with excess blast - 1 ( mds - eb1 )  . 
 molecular characterization and clinical outcomes of primary gleason pattern 5 prostate cancer after radical prostatectomy pedro isaacsson velho , md1 ; david lim , ms1 ; hao wang , phd1 ; jong chul park , md1 ; harsimar b . 
lotan , md1 purpose very high - risk prostate cancer ( pc ) is associated with poor response to local and systemic treatments ; however , few cases have been molecularly proled . 
clinicopathologic and genomic parameters were correlated with biochemical relapse , metastasis - free survival , time to castration resistance , and overall survival using cox proportional hazards models . results of patients with somatic sequencing data and clinical follow - up , 34% had dna repair gene mutations , including 22% ( 11 of 49 ) with homologous recombination and 12% ( six of 49 ) with mismatch repair gene alterations . 
these data are retrospective and hypothesis generating . conclusion potentially actionable homologous recombination and mismatch repair alterations are observed in a signicant proportion of patients with very high - risk pc at the time of radical prostatectomy . 
2019 by american society of clinical oncology introduction the national comprehensive cancer network very high - risk prostate cancer ( pc ) subset includes patients with t3b to t4 disease or more than four biopsy cores with gleason score 8 to 10 ( grade group 4 / 5 ) or those presenting with gleason score 5 + 5 = 10 or 5 + 4 = 9 ( primary gleason pattern 5 [ pg5 ] ; grade group 5 ) .1 these patients have the poorest oncologic outcomes , with higher relapse rates , frequent development of distant metastasis , poor response to systemic treatments , and short survival.2 - 4 previous studies have suggested that the proportion of gleason pattern 5 tumor on biopsy or surgical specimen denes a subset with independent prognostic implications and distinct outcomes after local and systemic treatments.5 - 8 although we have a wealth of data substantiating the poor prognosis of patients with predominant or pg5 , the molecular we know surprisingly little about alterations in these poorly differentiated tumors . among the 333 primary prostate tumors proled for the cancer genome atlas ( tcga ) , only eight patient cases ( 2% ) had pg5.9 because the prevalence of targetable alterations is relatively increased in other aggressive histologic subtypes of pc , 10 - 12 it is critically important to ll in these gaps in our molecular characterization of this disease . evolving data on metastatic castration - resistant pc ( mcrpc ) have demonstrated that druggable genomic alterations are not uncommon . 
 isaacsson velho et al context key objective we performed an integrated clinical and genomic analysis of prostate tumors with primary gleason pattern 5 at radical prostatectomy to identify potentially actionable alterations . knowledge generated in this very high - risk patient subset , adverse pathologic ndings and common molecular alterations , such as tp53 mutation , pten loss , and erg expression , were associated with poor outcomes . 
importantly , one third of patients had pathogenic mutations in dna repair genes , including in the homologous repair and mismatch repair pathways . relevance these data support the notion that aggressive subsets of primary prostate cancer are enriched for actionable genomic alterations and could inform the design of prospective clinical trials in this population . ( pd - 1 ) inhibitors.18 yet how these results in mcrpc might translate into treatment for clinically localized disease remains unclear . 
several clinical trials evaluating perioperative therapies in patients with high - risk localized including androgen - deprivation therapy ( adt ) , 19 antiandrogens , 20 and docetaxel , 21 have failed to demonstrate relevant benet . 
however , the utility of neoadjuvant and / or adjuvant parp and pd - 1 inhibitors has not yet been studied , in large part because of the relative rarity of these alterations in primary pc cohorts . here , we assembled a consecutive cohort of clinically localized prostate tumors with pg5 and long - term clinical follow - up after radical prostatectomy ( rp )  . 
to maximize duration of oncologic follow - up with the most recent pathologic specimens possible to preserve dna quality , we queried the pathology database for consecutive rps with pg5 from 2005 to 2015 and identied 60 patient cases with available tissue and clinical follow - up ( appendix fig a1 )  . immunohistochemistry tissue microarrays were constructed as previously reported.11 immunostaining for erg , pten , and p53 status was performed using previously reported and genetically validated rabbit monoclonal antibodies and staining and scoring protocols.22 - 26 punches from regions with the highest percentage of gleason pattern 5 tumor . 
dna was extracted from formalin - xed parafn - embedded material as previously described.11 next - generation tumor sequencing targeted next - generation deep sequencing to evaluate 262 cancer - related genes at a 500 average depth was performed using uw - oncoplex ( university of washington , seattle , wa ) as previously described.27 reported alterations were limited to those deemed pathogenic or likely pathogenic in the clinvar database . 
germline mutations were inferred by expert molecular pathologist review through cross - referencing against the clinvar database and by variant allele fraction in the context of tumor content , ploidy , and loss of heterozygosity status.28 , 29 two patients ( two of 49 ) did not have tumor dna available for uwoncoplex but had prior somatic sequencing performed using a clinical platform for clinical care purposes ( pgdx ; foundation medicine , cambridge , ma , and baltimore , md ) and were included in the analysis . 
patient cases in which tumor purity and / or dna quality was not high enough to exclude false - negative results are listed in the data supplement . germline sequencing altogether , 55% patient cases ( 27 of 49 ) underwent germline sequencing ( data supplement )  . 
 ( % ) a conrmatory test , 31 and metastasis - free survival ( mfs ) , dened as the time from rp to the rst detection of distant metastasis on imaging or death resulting from any cause , whichever occurred rst . 
time to castration resistance ( tcr ) , dened as the time from adt to two consecutive elevations in psa at least 4 weeks apart , and overall survival ( os ) , dened as the time from rp to death , were also assessed . 
univariable and multivariable cox proportional hazards models were used to estimate hazard ratios ( hrs ) and corresponding 95% cis and test for the association of the variables with clinical outcomes . 
because this study was hypothesis generating , we did not perform corrections for multiple comparisons . results baseline characteristics demographic , clinical , and pathologic characteristics of the pg5 cohort ( n = 60 ) at rp are listed in table 1 . 
at surgery , most patients had pathologic evidence of locally advanced disease , including nonorgan - conned ( pt3 / t4 ) tumors ( 54 [ 90% ] of 60 ) , seminal vesicle invasion ( svi ) ( 35 [ 58% ] of 60 ) , positive lymph nodes ( 16 [ 27% ] of 60 ) , and positive surgical margins ( 28 [ 47% ] of 60 )  . 
of the 37 patients who received either salvage or adjuvant radiation therapy , 27 ( 73% ) also received adjuvant adt . also , of the 16 patients who had positive lymph nodes ( pn + ) , 11 ( 69% ) received adjuvant adt . prevalence of gene mutations overall , 81.7% ( 49 of 60 ) of patients had available sequencing data on somatic genomic alterations ( data supplement ) , and 35% ( 17 of 49 ) of these had at least one pathogenic mutation in a gene involved in dna repair ( table 2 ; data supplement )  . 
overall , 55% ( 27 of 49 ) had germline sequencing results available , including six patients with presumed germline homologous recombination alterations on the basis of somatic sequencing , all of which were conrmed on germline sequencing ( brca2 , n = 3 ; brca1 , chek2 , and palb2 , n = 1 each )  . 
in addition to these alterations in homologous recombination genes , mmr deciency was found in 12% ( six of 49 ) of patients ( all in msh2 and included in our previous immunohistochemistry [ ihc ] study11 )  . other mutations common in pc were also identied ( data supplement )  . 
of 57 patients who had tumors evaluated by ihc , 51% ( 29 of 57 ) had pten protein loss . foxa1 mutations were seen in 12% ( six of 49 ) of patients , and spop mutations were seen in 8% ( four of 49 ) of patients . 
several pathologic characteristics were associated with increased risk of bcr on univariable analysis , including svi ( appendix table a1 ; appendix fig a2a ) and presence of ductal or intraductal histology ( appendix table a1 ; appendix fig a2b )  . 
multivariable models were t separately for each genomic alteration , adjusting for ductal or intraductal histology and svi ; however , none of the genomic alterations remained signicantly associated with bcr ( appendix table a2 )  . overall , 43% ( 26 of 60 ) of the cohort developed metastasis , with a median mfs of 86.4 months ( 95% ci , 40.7 months to not reached )  . 
visceral disease was seen in 31% of patients who developed metastasis , with liver ( 23% ) and lung ( 19% ) the most common sites . among clinicopathologic factors on univariable analysis , presence of svi ( table 3 ; fig 1a ) and ductal or intraductal histology ( table 3 ; fig 1b ) , along with patient age , psa , and nodal status , were both associated with increased risk of metastasis ( fig 1b )  . 
kaplan - meier analysis of metastasis - free survival in primary gleason pattern 5 cohort by ( a ) seminal vesicle invasion ( svi ) status , ( b ) ductal or intraductal ( doi ) histology status , ( c ) tp53 mutation status , and ( d ) pten protein status using immunohistochemistry . 
we chose a subset of patients with established unfavorable clinical outcomes who were diagnosed before evidence of metastatic disease and received the same initial local treatment to minimize potential biases associated with extent of disease . 
almost all patients had nonorganconned disease , more than half had svi , and a quarter had node - positive disease , demonstrating the aggressive behavior of these poorly differentiated tumors . the prevalence of genomic abnormalities in the dna repair pathway in clinically localized pg5 seems to be comparable to or perhaps even higher than that in patients with mcrpc . pritchard et al13 showed that 12% of patients with mcrpc table 5 . 
abnormalities in homologous recombination and mmr genes could have potential therapeutic implications for the treatment of all stages of pc , including the design of adjuvant and neoadjuvant trials in the pg5 population . 
in addition , our ndings have important implications for the families of patients with very high - risk disease , given that 82% of patients with homologous recombination mutations in this study had apparent underlying germline mutations . 
these ndings clearly support the recent national comprehensive cancer network guidelines , which recommend genetic testing in all patients with high - risk or very high - risk pc . our results show that there are pathologic and molecular features that are useful for risk stratication after rp . 
patients with svi or ductal or intraductal histology have more than four times greater risk of metastasis , and tp53 mutation , pten loss , and erg expression were associated with increased risk of biochemical failure and metastasis . 
notably , our study validates current clinicopathologic variables used for risk stratication and suggests that pathologic ndings after rp may be more signicant for risk prediction than molecular alterations in multivariable models . 
however , where full pathologic data are not available ( eg , in patients who do not undergo rp ) , molecular alterations could be of added value . future studies should evaluate prospectively the utility of tp53 mutation and pten loss in well - designed biomarkerdriven clinical trials cohorts , particularly in the biopsy setting . in addition , although we believe that our data are unique and informative , these results should be viewed as preliminary because of relatively the small numbers and multiplicity of clinical , pathologic , and molecular data points , which limit the power of the observations with regard to outcomes . 
it is likely that a prospective evaluation with additional numbers and follow - up time will allow for a more precise study of the prognostic signicance of clinicopathologic and molecular parameters in this group of patients . the pivotal role of adt in pc with gleason scores 9 to 10 has been called into question in recent years.8 a recent large retrospective study of patients undergoing external - beam radiation therapy in combination with adt compared outcomes of patients with gleason score 8 versus 9 to 10 , suggesting that those in the higher gleason group may derive less benet than patients with gleason score 8.8 recent studies have shown that the addition of either docetaxel21 , 32 or abiraterone33 , 34 improves os in the locally advanced or metastatic hormone - sensitive setting , with higher benet among high - risk patients , including those with high disease burden , 32 t3 to t4 disease , 21 , 34 psa greater than 40 ng / ml , 21 , 34 and gleason score 8 to 10.21 , 33 , 34 our data suggest that compared with lower - grade tumors , pg5 tumors may be less dependent on androgens and potentially more dependent on alternative oncogenic drivers , including defects in dna repair pathways . limitations of the study include the fact that it was retrospective , and clinical follow - up and dna sequencing were available only for a subset of patients , although the clinicopathologic parameters of patients with and without follow - up and sequencing were not signicantly different ( appendix fig a1 )  . 
also , the quality of the archival dna and tumor purity were not uniformly high , and false negatives at sequencing could not be excluded in all patient cases , suggesting that our results may actually underestimate the prevalence of dna repair alterations among pg5 tumors . 
 isaacsson velho et al in conclusion , we performed the rst integrated clinical and genomic analysis to our knowledge of pg5 prostate tumors at rp , a subset that has not been well represented in other sequencing efforts . 
clinical outcomes and response to conventional treatment are worse compared with lower - risk groups , and adverse pathologic ndings and common molecular alterations such as tp53 mutation , pten loss , and erg expression are associated with poor outcomes . 
the relatively high incidence of hrd and mmr deciency observed herein could inform the design of multimodal clinical trials employing parp inhibitors or pd - 1 / pd - 1 ligand monoclonal antibodies in very high - risk patients with clinically localized disease . 
contributed equally to this work . support supported by the patrick walsh research fund ; by national cancer institute ( nci ) , national institutes of health , prostate specialized program of research excellence grant no . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . travel , accommodations , expenses : astrazeneca , astellas pharma , pzer , merck serono , merck michael a . 
carducci consulting or advisory role : astellas pharma , abbvie , roche / genentech , pzer , foundation medicine research funding : bristol - myers squibb ( inst ) , pzer ( inst ) , astrazeneca ( inst ) , gilead sciences ( inst ) , emd serono ( inst ) , effector therapeutics ( inst ) samuel r . 
antonarakis honoraria : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : coinventor of biomarker technology licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation mario a . 
eisenberger leadership : veru stock and other ownership interests : veru honoraria : sano , pzer consulting or advisory role : astellas pharma , ipsen , bayer healthcare pharmaceuticals , sano , pzer research funding : sano , tokai pharmaceuticals , genentech travel , accommodations , expenses : bayer healthcare pharmaceuticals , astellas pharma , sano , pzer , veru pedro isaacsson velho honoraria : bayer healthcare pharmaceuticals speakers bureau : astrazeneca , pzer , bristol - myers squibb research funding : bristol - myers squibb , pzer ( inst ) expert testimony : bayer healthcare pharmaceuticals tamara l . 
prostate cancer 2018 : 151 epstein ji , zelefsky mj , sjoberg dd , et al : a contemporary prostate cancer grading system : a validated alternative to the gleason score . 
eur urol 69 : 428 - 435 , 2016 sundi d , tosoian jj , nyame ya , et al : outcomes of very high - risk prostate cancer after radical prostatectomy : validation study from 3 centers . 
cancer 125 : 391397 , 2019 sundi d , wang vm , pierorazio pm , et al : very - high - risk localized prostate cancer : denition and outcomes . 
prostate cancer prostatic dis 17 : 57 - 63 , 2014 ellis cl , partin aw , han m , et al : adenocarcinoma of the prostate with gleason score 9 - 10 on core biopsy : correlation with ndings at radical prostatectomy and prognosis . 
j urol 190 : 2068 - 2073 , 2013 cheng l , davidson dd , lin h , et al : percentage of gleason pattern 4 and 5 predicts survival after radical prostatectomy . 
cancer 110 : 1967 - 1972 , 2007 tilki d , chen mh , wu j , et al : surgery vs radiotherapy in the management of biopsy gleason score 9 - 10 prostate cancer and the risk of mortality . 
marshall ch , fu w , wang h , et al : prevalence of dna repair gene mutations in localized prostate cancer according to clinical and pathologic features : association of gleason score and tumor stage . 
clin cancer res 23 : 6863 - 6874 , 2017 isaacsson velho p , silberstein jl , markowski mc , et al : intraductal / ductal histology and lymphovascular invasion are associated with germline dna - repair gene mutations in prostate cancer . 
powell ij , tangen cm , miller gj , et al : neoadjuvant therapy before radical prostatectomy for clinical t3 / t4 carcinoma of the prostate : 5 - year followup , phase ii southwest oncology group study 9109 . 
vale cl , burdett s , rydzewska lhm , et al : addition of docetaxel or bisphosphonates to standard of care in men with localised or metastatic , hormone - sensitive prostate cancer : a systematic review and meta - analyses of aggregate data . 
tosoian jj , almutairi f , morais cl , et al : prevalence and prognostic signicance of pten loss in african - american and european - american men undergoing 23 . 
lotan tl , wei w , ludkovski o , et al : analytic validation of a clinical - grade pten immunohistochemistry assay in prostate cancer by comparison with pten radical prostatectomy . 
maughan bl , guedes lb , boucher k , et al : p53 status in the primary tumor predicts efcacy of subsequent abiraterone and enzalutamide in castration - resistant prostate cancer . 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
na r , zheng sl , han m , et al : germline mutations in atm and brca1 / 2 distinguish risk for lethal and indolent prostate cancer and are associated with early age 31 . 
cookson ms , aus g , burnett al , et al : variation in the denition of biochemical recurrence in patients treated for localized prostate cancer : the american urological association prostate guidelines for localized prostate cancer update panel report and recommendations for a standard in the reporting of surgical outcomes . 
n engl j med 377 : 352 - 360 , 2017 james nd , de bono js , spears mr , et al : abiraterone for prostate cancer not previously treated with hormone therapy . 
pathology database query for consecutive radical prostatectomies ( rps ) with primary gleason score 5 ( pg5 ) from 2005 to 2015 , where 60 patient cases were identied with available tissue and clinical follow - up . 
 c significant tumor response to the poly ( adp - ribose ) polymerase inhibitor olaparib in heavily pretreated patient with ovarian carcinosarcoma harboring a germline rad51d mutation introduction brca1 and brca2 are the best - known examples of proteins that contribute to repair of double - strand dna breaks via the homologous recombination repair ( hrr ) pathway . the rad51 paralogs rad51b , rad51c , and rad51d are proteins that are also involved in the hrr pathway . 
parp inhibitors are rationally designed drugs that inhibit parp1 by trapping the inactivated enzyme onto the single - strand break , generating a potential block for cellular dna replication.5 - 7 trapped parp - dna complexes can lead to the stalling and / or collapse of replication forks , resulting in the generation of more deleterious double - strand breaks.8 in cells unable to carry out hrr because of brca mutation , the added genotoxic stress of inhibition of single - strand repair is cytotoxic and referred to as synthetic lethality.5 , 7 in vitro and mice studies support the use of parp inhibition , not only in the presence of brca mutation but also in malignancy with other genetic defects that affect hrr , such as rad51 deletion.9 given the rarity of rad51 mutations , there is limited clinical evidence in this context . we describe a heavily pretreated patient with ovarian carcinosarcoma , with known germline rad51d mutation , that exhibited a remarkable and durable response to parp inhibitor therapy . 
subsequently the patient experienced remissions of varying degrees and durations , with additional lines of therapy including paclitaxel , cisplatin , ifosfamide , and doxorubictwo years before presentation of this case report , the patient was enrolled in a phase i clinical trial using a novel pd - 1 inhibitor . 
 a writing , the patient continues to take olaparib , with no evidence of disease regrowth . discussion synthetic lethality is a term used to describe the combination of two defects that do not affect cell viability when each occurs individually but are cytotoxic when they occur simultaneously in a single cell.7 , 10 parp inhibitors have been used to exploit synthetic lethality in brca1and brca2 - mutant ovarian , breast , prostate , and other cancers . 
 however , hrr deficiency extends beyond cancers harboring brca1 / 2 mutations , and the term brcaness has been coined to describe the clinical and biologic features of such tumors . 
 this not only includes similar histomorphological features such as basal - like phenotype in breast cancers or high - grade serous morphology in ovarian cancers , but also similar immunophenotypic profile ( eg , triple - negative breast cancers ) , drug sensitivity ( eg , to platinum agents and parp inhibitors ) , as well as prognosis.11 - 13 the brcaness phenotype is seen in tumors with loss - of - function mutations involving other hrr pathway genes , including atm , atr , bard1 , brip1 , mre11a , palb2 , rad50 , rad51d , rad54 , nbs1 , chek1 , and chek2 , as well as components of the fanconi anemia repair pathway.13 , 14 in vitro and mice studies have demonstrated efficacy of parp inhibitors against cancer cells with defects in rad51 . 
separate studies by shah et al , cruz et al , and wang et al found that breast or ovarian cancer cells with absent or low levels of rad51 were sensitive to parp inhibitors.15 - 17 another study observed that parp inhibitor sensitivity was increased by 1 , 000 - fold in cells that are rad51 knockdown.14 cruz et al and wang et al additionally demonstrated that the presence of rad51 conferred resistance to parp inhibitors in these cells.16 , 17 in their experiments on triple - negative breast cancer cells , wang et al postulated that it may be possible to expand the sensitivity of triple - negative breast cancer to parp inhibitors by targeting rad51.17 other studies found increased sensitivity to parp inhibition when rad51 inhibitors were coadministered.10 , 18 interestingly , falchi et al found the addition of a brca2 - rad51 disruptor to parp inhibition to be synergistic , rather than merely additive , which is probably a consequence of fig 1 . 
 ( a ) baseline computed tomography ( ct ) scan of pelvis , demonstrating heterogeneous mass ( arrowhead ) , ( b ) ct scan after 8 weeks on olaparib , showing excellent partial response in pelvic mass ( arrowhead ) , and ( c ) ct scan after 16 weeks on olaparib , showing additional disease response ( arrowhead )  . disease response for 16 months , followed by rapid and significant tumor regrowth ( fig 1a )  . the patient had previously been determined to have a germline mutation in rad51d , evidenced by a heterozygous variant c.263 + 1g > a . 
 this mutation has previously been described in ovarian cancer.4 with the possibility of defective hrr in the patients tumor as the result of loss of the remaining functional rad51d allele , a therapeutic trial of olaparib was initiated . 
we are not aware of other case reports that have demonstrated disease response to parp inhibitors in tumors with an underlying rad51d mutation . our clinical experience is consistent with preclinical models and adds to the current limited clinical evidence of benefit of parp inhibition in the context of rad51 mutations . 
chandran no relationship to disclose ian kennedy no relationship to disclose the simultaneous inhibition of two dna - repair mechanisms.10 a 2016 phase ii study ( ariel2 ; a study of rucaparib in patients with platinum - sensitive , relapsed , high - grade epithelial ovarian , fallopian tube , or primary peritoneal cancer ) used the parp inhibitor rucaparib in recurrent , platinum - sensitive , high - grade ovarian carcinoma . 
 of 206 patients , there were seven with rad51 mutations : one patient with rad51b mutation with stable disease , who was receiving rucaparib ; four patients with rad51c mutations ( three partial responses and one patient with stable disease ) ; and two patients with rad51d mutation , both with stable disease.19 using baseline and postprogression biopsy samples from the same study , kondrashova et al reported that in five of six patients with rad51c and rad51d truncation mutations that subsequently developed resistance to rucaparib , there were one or more secondary mutations restoring the open reading frame . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
song h , dicks e , ramus sj , et al : contribution of germline mutations in the rad51b , rad51c , and rad51d genes to ovarian cancer in the population . 
tan dsp , rothermundt c , thomas k , et al : brcaness syndrome in ovarian cancer : a casecontrol study describing the clinical features and outcome of patients with epithelial ovarian cancer associated with brca1 and brca2 mutations . 
mccabe n , turner nc , lord cj , et al : deficiency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
shah mm , dobbin zc , nowsheen s , et al : an ex vivo assay of xrt - induced rad51 foci formation predicts response to parp - inhibition in ovarian cancer . 
cruz c , castroviejo - bermejo m , gutirrez - enrquez s , et al : rad51 foci as a functional biomarker of homologous recombination repair and parp inhibitor resistance in germline brca - mutated breast cancer . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
tan author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license corresponding author : david s.p. 
indeed , hrd - related genetic aberrations may confer a similar clinical phenotype to gboc , 7 , 8 including improved responses and longer progression - free survival ( pfs ) in patients receiving maintenance parpi treatment.9 - 11 few effective treatment options exist for patients with recurrent hgsoc ( rhgsoc ) , especially in the context of malignant bowel obstruction , where the use of bevacizumab is associated with a higher risk of bowel perforation.12 we present the case of a patient with a germline pathogenic rad51c mutation who received salvage treatment for terminal malignant bowel obstruction with sixth - line carboplatin and pegylated liposomal doxorubicin ( pld ) , followed by maintenance olaparib . a 57 - year - old chinese woman was referred to our institution after hgsoc relapse . 
she first received the hgsoc diagnosis at 53 years of age , with no family history of breast or ovarian cancer , and had received initial treatment elsewhere ( table 1 )  . 
at first relapse of hgsoc ( after a 28 - month pfi ) , she received carboplatin plus pld every 4 weeks for six cycles , followed by secondary debulking . 
she received four cycles of carboplatin every 3 weeks with dose - dense paclitaxel once per week , followed by two cycles of cisplatin substituted for carboplatin , owing to grade 2 carboplatin hypersensitivity . 
complete response was achieved with a nadir ca - 125 concentration of 90 u / ml . three months later , however , the patients ca - 125 level rose to 571 u / ml , at which point she transferred care to our institution . 
clinical presentation and treatment summary treatment received at another institution presentation and treatment date may 2010 july 2010 july - nov 2010 mar 2013 apr - june 2013 july 2013 sept - nov 2013 june 2014 july - nov 2014 jan 2015 feb 2015 apr - june 2015 june 2015 june - nov 2015 feb - june 2016 june 2016 july - oct 2016 nov 2014 ca - 125 level nadir of 90 u / ml . complete response determined from repeated ct scan . transfer of care to our institution genetic testing performed using invitae panel . hgsoc diagnosed at another institution . 
 switched to cisplatin ( 75 mg / m2 ) and paclitaxel ( 175 mg / m2 ) every 3 weeks for two more cycles in view of grade 2 hypersensitivity to carboplatin . biochemical recurrence ; ttp : 3 months ; ca - 125 level : 571 u / ml . 
no measurable disease seen on ct scan . genetic testing showed pathogenic grad51c mutation . symptomatic hgsoc relapse ; pfi now 5 months ; ca - 125 level : 3 , 145 u / ml . 
intestinal obstruction resolved with conservative management . switched to fourth - line carboplatin ( auc 5 ) with desensitization protocol and gemcitabine ( 1 , 000 mg / m2 , days 1 and 8 ) every 3 weeks . carboplatin ( auc 5 ) treatment continued with desensitization protocol and gemcitabine ( 1 , 000 mg / m2 , days 1 and 8 ) every 3 weeks ; total of eight cycles with partial response . 
ct scan shows residual 3.6 - cm pelvic implant . ct scans showed new ascites and increasing size of peritoneal implant . patient enrolled in phase i study of low - dose whole abdominal radiation therapy ( 60 cgy fractions , 2 d / wk , twice on each of those days ) , in combination with weekly paclitaxel ( 80 mg / m2 )  . 
pfs while receiving olaparib treatment : 7 months . underwent surgical exploration and defunctioning jejunostomy . july 2017 multiple levels of malignant small - bowel obstruction developed . patient referred to hospice care . 
she joined a phase i trial of kpt330 ( clinicaltrials.gov identifier : nct02078349 ) , but her disease progressed after 2 months , and she had an intestinal obstruction from worsening peritoneal metastases . 
after eight cycles , sustained partial response ( pr ) was achieved according to gynecologic cancer intergroup criteria.14 the ca - 125 concentration improved from 7 , 550 u / ml to 368 u / ml . 
the patient was given a chemotherapy holiday . unfortunately , after another short ttp of 2 months , there was symptomatic disease progression , and the patient was enrolled in a phase ii clinical trial of low - dose , whole - abdomen radiation combined with weekly paclitaxel treatment . 
this approach was based on the knowledge that genomic hrd could enable prediction of response to dna - damaging agents such as carboplatin and topoisomerase iia inhibitors.15 the patient chose carboplatin plus pld every 4 weeks , and her disease responded according to gynecologic cancer intergroup criteria . 
the patient was experiencing grade 2 fatigue and , in view of emerging data at that time on the efficacy of parpis in tumors with hrd , 16 a complete break from treatment , versus off - label maintenance therapy with olaparib capsules , was discussed . 
 she chose the latter option . because of financial constraints , the patient was prescribed olaparib capsules 200 mg twice daily ( rather than the 400 - mg twice - daily standard dosing ) , but her disease continued to respond , with a reduction in ca - 125 level from 1 , 405 u / ml to a nadir of 44.7 u / ml ( fig 2 )  . 
after 6 months of olaparib treatment , scans confirmed pr by response evaluation criteria in solid tumors ( recist ) , version 1.1 , with improved ascites and resolution of a perihepatic peritoneal deposit ( fig 1 )  . unfortunately , the patients disease relapsed a month later with small - bowel obstruction and required parenteral nutrition . 
 ( a and b ) june 2016 ( preplatinum rechallenge ) : left lung lesion ( curved arrow ) , ascites , and peritoneal thickening ( double arrow )  . 
 ( e and f ) april 2017 resolution of ascites and of the deposit at the hepatic hilum after 6 months of olaparib treatment ( originally seen in ( d ) , arrow )  . many to be a preterminal event.17 retrospective data show limited responses from chemotherapy.17 yet , this patient responded remarkably to sixthline carboplatin plus pld and , per the recent us food and drug administration approval for maintenance parpis , derived significant benefit from olaparib , even at an off - label dose of 200 mg twice daily . 
notably , biologically effective inhibition of parp by olaparib capsules has been demonstrated even at 100 mg twice daily.18 to our knowledge , this report is the first to describe the clinical effect of this specific grad51c variant on treatment selection and patient outcome in rhgsoc . the cancer genome atlas project showed approximately 30% of hgsoc cases harbor nonbrca1 / 2 mutation - related hrd . 
 more recently , olaparib , 7 - 9 niraparib , 10 and rucaparib16 were approved for use in patients who have received at least two prior treatments of platinum - based chemotherapy and are platinum responsive . 
of note , all patients eligible for the landmark phase iii trials , 9 - 11 leading to approval of parpi for this indication , had experienced a ttp after penultimate platinum exposure of 6 months , which was not the case in our patient . efficacy data on resensitization to platinum based chemotherapy and thresholds constituting an effective pfi are ambiguous . 
dramatic reduction of ca - 125 level from 17 , 256 u / ml to 867.7 u / ml was noted after the patient commenced receiving carboplatin plus pld treatment . 
analyses revealed a frameshift - truncating mutation of tp53bp1 , which is associated with olaparib resistance.33 reversion mutations in rad51c have also been described in acquired rucaparib resistance.34 unfortunately , at the time of disease progression , surgeons were unable to obtain an adequate tumor sample for analysis of resistance mechanisms in the patient in the current report . in conclusion , patients with ovarian cancer with grad51c mutations may benefit from similar treatment paradigms as brca1 / 2 - mut disease . 
 darwin tay no relationship to disclose valerie heong consulting or advisory role : roche ; astrazeneca patents , royalties , other intellectual property : royalties received for drug venetoclax travel , accommodations , expenses : astrazeneca soo chin lee honoraria : roche ; astrazeneca ; pfizer ; novartis consulting or advisory role : pfizer ; novartis ; astrazeneca ; roche ; eisai research funding : eisai ; taiho pharmaceutical ; bayer ; aslan pharmaceuticals expert testimony : novartis travel , accommodations , expenses : roche ; novartis ; pfizer ; act genomics yee liang thian no relationship to disclose pei yi ong no relationship to disclose samuel g.w. 
jeyasekharan honoraria : msd oncology yi wan lim no relationship to disclose siew eng lim no relationship to disclose research funding : astrazeneca ; perkin elmer travel , accommodations , expenses : perkin elmer joseph ng no relationship to disclose jeffrey j.h. 
tan honoraria : astrazeneca ; roche consulting or advisory role : astrazeneca ; roche research funding : astrazeneca ( inst ) ; karyopharm therapeutics ( inst ) ; bayer ( inst ) travel , accommodations , expenses : merck sharp & dohme ; merck serono ; astrazeneca ; bayer ; roche affiliations natalie y.l. 
alsop k , fereday s , meldrum c , et al : brca mutation frequency and patterns of treatment response in brca mutation - positive women with ovarian cancer : a report from the australian ovarian cancer study group . 
song h , dicks e , ramus sj , et al : contribution of germline mutations in the rad51b , rad51c , and rad51d genes to ovarian cancer in the population . 
swisher em , harrell mi , lin k , et al : brca1 and rad51c promoter hypermethylation confer sensitivity to the parp inhibitor rucaparib in patients with relapsed , platinum - sensitive ovarian carcinoma in ariel2 part 1 . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
pujade - lauraine e , ledermann ja , selle f , et al : olaparib tablets as maintenance therapy in patients with platinum - sensitive , relapsed ovarian cancer and a brca1 / 2 mutation ( solo2 / engot - ov21 ) : a double - blind , randomised , placebo - controlled , phase 3 trial . 
coleman rl , oza am , lorusso d , et al : rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebocontrolled , phase 3 trial . 
rustin gj , vergote i , eisenhauer e , et al : definitions for response and progression in ovarian cancer clinical trials incorporating recist 1.1 and ca 125 agreed by the gynecological cancer intergroup ( gcig )  . 
tan ds , kaye sb : chemotherapy for patients with brca1 and brca2 - mutated ovarian cancer : same or different ? am soc clin oncol educ book 35 : 114 - 121 , 2015 16 . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
kaye sb , lubinski j , matulonis u , et al : phase ii , open - label , randomized , multicenter study comparing the efficacy and safety of olaparib , a poly ( adp - ribose ) polymerase inhibitor , and pegylated liposomal doxorubicin in patients with brca1 or brca2 mutations and recurrent ovarian cancer . 
gayarre j , martn - gimeno p , osorio a , et al : characterisation of the novel deleterious rad51c p.arg312trp variant and prioritisation criteria for functional analysis of rad51c missense changes . 
hatanaka a , yamazoe m , sale je , et al : similar effects of brca2 truncation and rad51 paralog deficiency on immunoglobulin v gene diversification in dt40 cells support an early role for rad51 paralogs in homologous recombination . 
yokoyama h , sarai n , kagawa w , et al : preferential binding to branched dna strands and strand - annealing activity of the human rad51b , rad51c , rad51d and xrcc2 protein complex . 
somyajit k , mishra a , jameei a , et al : enhanced non - homologous end joining contributes toward synthetic lethality of pathological rad51c mutants with poly ( adp - ribose ) polymerase . 
ghiringhelli f , richard c , chevrier s , et al : efficiency of olaparib in colorectal cancer patients with an alteration of the homologous repair proteworld j gastroenterol 22 : 10680 - 10686 , 2016 33 . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
others have an intermediate phenotype and are classified as glomus tumors of uncertain malignant potential ( gt - ump ) .3 herein , we present a case of an 18 - year - old patient with two glomus tumors involving the lateral and posterior cords of the right brachial plexus . 
physical examination demonstrated no neurologic deficit . imaging mr imaging of the right upper extremity demonstrated two distinct brachial plexus lesions , one emanating from the distal aspect of the lateral cord and the other from the posterior cord ( fig 1 )  . 
after extensive discussion with the neurosurgeon , the patient opted for surgical exploration with open biopsy and possible removal of the infraclavicular tumors to provide a histologic diagnosis and guidance on further management . intraoperative findings open exploration of the right infraclavicular brachial plexus was performed . 
these were gently mobilized but did not stimulate and were divided , allowing the lesion to be removed en bloc and sent for histopathological analysis . in the posterior cord region , the axillary nerve was clearly enlarged with tumor . 
 ( a ) on coronal fluid - sensitive magnetic resonance sequence through the chest , the right brachial plexus demonstrates asymmetric hyperintensity and thickening of the c5 , c6 , c7 , and t1 nerve roots and upper trunk ( not shown ) in addition to two discrete masses arising from the distal brachial plexus involving the posterior ( short arrow ) and lateral ( long arrow ) cords . 
 ( c ) on diffusion weighted imaging with apparent diffusion coefficient mapping , there is qualitative and quantitative restricted diffusion ( apparent diffusion coefficient [ adc ] values range from 0.6 to 1 103 mm2 / s in the larger mass and 0.9 to 1 103 mm2 / s in the smaller mass )  . 
on frozen section , this tumor appeared relatively benign , but given its widespread involvement with the axillary nerve , further aggressive dissection of the remaining tumor was deferred to avoid morbid neurologic deficits . histopathology and molecular analysis histopathologic analysis revealed a well circumscribed proliferation of relatively monomorphic cells with round nuclei and abundant eosinophilic cytoplasm ( figs 2a and 2b )  . 
mart1 was faint , caldesmon was focal , cd34 highlighted blood vessels , ini - 1 expression was intact , and ki - 67 proliferation index was mild to moderate . 
these findings together led to the diagnosis of malignant glomus tumor per current criteria.3 molecular genetic analysis using polymerase chain reactionbased sequencing of braf exon 15 revealed the braf v600e mutation at a mutant allele frequency of 40% . 
 to support this finding , we performed immunohistochemical analysis using antibodies directed against phosphoextracellular signal - regulated kinase ( erk ) ; this revealed variable immunostaining , with both cytoplasmic and nuclear immunoreactivity . 
in addition to isolated braf testing , a conventional cytogenetic analysis of the tumor revealed a normal 46 xx karyotype in all cells examined . therapeutic management management of this patients malignant tumor was discussed at the johns hopkins hospital multidisciplinary sarcoma tumor board . 
 ( a ) low - power view of glomus tumor associated with peripheral nerve fascicles , hematoxylin and eosin sta ( b ) tumor cells had ample eosinophilic cytoplasm and evident mitotic activity . 
mr imaging and 18f - fluorodeoxy - d - glucose positron emission tomographycomputed tomography obtained 2 weeks after the addition of trametinib demonstrated interval decrease in tumor size ( table 1 )  . 
 mr imaging at 3 and 6 months after initiating raf inhibitor therapy showed continued decrease in tumor size ( figs 3 and 4 ) and at 9 months showed no further change in size or imaging characteristics relative to most recent prior imaging . 
she experiences no pain , and the extremity function is normal . discussion the ras - raf - mek - erk signaling pathway is a frequent site of oncogenic mutations , with approximately 30% of human cancer harboring at least one mutation that results in its dysregulation . 
activating braf mutations are found in approximately 7% of cancers , roughly half of malignant melanomas , 5 and in other tumors , including colorectal , ovarian , papillary thyroid , and nonsmall - cell lung cancers , gliomas , and histiocytic disorders.6 - 12 the most common mutation , v600e , results in constitutive activation of the erk pathway . small molecule inhibitors of raf kinase were first studied in clinical trials of patients with melanoma . 
to determine whether the benefit of targeted raf inhibition would extend to nonmelanoma tumors with braf v600e , a phase ii basket trial explored the use of vemurafenib in patients selected for this mutation . 
this study demonstrated modest antitumor activity , although not all tumors with braf mutation responded , thus enforcing that a single driver oncogene may be associated with a nonuniform response to targeted therapy.16 braf mutations also occur rarely in a wide spectrum of cancers , including 1.4% of soft tissue sarcomas.17 a single patient with braf - mutated clear cell sarcoma was treated in the vemurafenib basket trial and sustained a partial response.16 the role of raf inhibitors in other sarcomas , however , has not been explored . glomus tumors are mesenchymal neoplasms that are rare and generally benign.18 they can occur as solitary or multiple soft tissue tumors and are most commonly located on the digits , supporting early hypotheses about their origin in the temperature - sensing glomus body . 
in a targeted sequencing analysis , three of 28 glomus tumors were found to harbor braf v600e mutations and a single tumor mutation in kras.19 a single case of a glomus tumor of the median nerve was found by next - generation sequencing to harbor a braf v600e mutation.20 this patient , and those in the retrospective analysis of 28 cases , was treated surgically without consideration for systemic therapy . 
finally , in a collection of 102 glomus tumors ( 56% benign , 15% gt - ump , and 29% malignant ) braf v600e mutation was detected in six tumors ( 6% ) , all of which were classified as either malignant glomus tumor or gt - ump ( and 0 of 57 benign glomus tumors harbored braf mutations ) .21 these data , although reflective of an overall small sample size , are suggestive of braf mutation as a predictor of more aggressive clinical behavior . 
 interestingly , glomus tumor has previously been associated with neurofibromatosis type 1 , 22 suggesting a shared terminal event in activation of erk signaling in these tumors . our patients response to targeted braf inhibition is an extraordinary one and highlights promise for future use in sarcomas with this mutation . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . andrea cuviello no relationship to disclose aviad zick research funding : merck ( inst ) , eli lilly ( inst ) shivani ahlawat no relationship to disclose fausto j . 
folpe al , fanburg - smith jc , miettinen m , et al : atypical and malignant glomus tumors : analysis of 52 cases , with a proposal for the reclassification of glomus tumors . 
kimura et , nikiforova mn , zhu z , et al : high prevalence of braf mutations in thyroid cancer : genetic evidence for constitutive activation of the ret / ptc - ras - braf signaling pathway in papillary thyroid carcinoma . 
mcarthur ga , chapman pb , robert c , et al : safety and efficacy of vemurafenib in braf ( v600e ) and braf ( v600k ) mutation - positive melanoma ( brim - 3 ) : extended follow - up of a phase 3 , randomised , open - label study . 
hauschild a , grob jj , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
dahlin lb , scherman p , besjakov j , et al : intraneural glomus tumor of uncertain malignant potential and with braf mutation in the median nerve an unusual case . 
karamzadeh dashti n , bahrami a , lee sj , et al : braf v600e mutations occur in a subset of glomus tumors , and are associated with malignant histologic characteristics . 
dahlin lb , mller g , anagnostaki l , et al : glomus tumours in the long finger and in the thumb of a young patient with neurofibromatosis - 1 ( nf - 1 )  . 
voss ( continued ) purpose with prospective clinical sequencing of tumors emerging as a mainstay in cancer care , an urgent need exists for a clinical support tool that distills the clinical implications associated with specific mutation events into a standardized and easily interpretable format . 
to this end , we developed oncokb , an expert - guided precision oncology knowledge base . methods oncokb annotates the biologic and oncogenic effects and prognostic and predictive significance of somatic molecular alterations . 
potential treatment implications are stratified by the level of evidence that a specific molecular alteration is predictive of drug response on the basis of us food and drug administration labeling , national comprehensive cancer network guidelines , disease - focused expert group recommendations , and scientific literature . results to date , > 3 , 000 unique mutations , fusions , and copy number alterations in 418 cancerassociated genes have been annotated . 
with the shift from single analyte tests and small hotspot panels to larger gene panels and whole - exome and - genome platforms , interpretation of the clinical significance of the increasing number of genomic alterations identified in individual tumors has become a challenge . 
a smaller subset are known or suspected functionally significant mutations with no clear therapeutic implications , and the smallest subset consists of known driver mutations that are clinically actionable . the information that discriminates whether an alteration is clinically actionable can reside in various silos , including us food and drug administration ( fda ) labeling , national comprehensive cancer network ( nccn ) guidelines , conference proceedings , disease - focused expert group recommendations , and the scientific literature . 
therefore , an urgent need exists for a clinical support tool that distills this information into a standardized and easily interpretable format that democratizes its access to clinicians of all knowledge levels and at all centers . 
to address these limitations , we describe oncokb , a comprehensive precision oncology knowledge base that offers oncologists detailed , evidence - based information about individual somatic mutations and structural alterations present in patient tumors to support optimal treatment decisions . 
oncokb content is supervised by a dedicated panel of physicians and cancer biologists who review and edit biomarker - associated investigational therapeutic strategies ( data supplement )  . through continual dialogue with the scientific and medical community , oncokb integrates clinical best practices as defined by institutionwide , multidisciplinary disease management teams ( fig 1 )  . 
oncokb communicates information on the biomarker - guided use of fdaapproved therapies and investigational agents under evaluation in clinical trials and highlights negative clinical results to discourage off - label use of expensive targeted therapies shown to be ineffective in specific mutational contexts . methods oncokb includes biologic , clinical , and therapeutic information curated from multiple unstructured information resources , including guidelines and recommendations derived from fda labeling , nccn guidelines , other diseasespecific expert and advocacy group recommendations , and the medical literature ( fig 1 )  . with recognition that clinical implications vary substantially on the basis of specific alterations within a gene and tumor context , information in oncokb is hierarchically organized by gene , alteration , tumor type , and clinical implication ( fig 1 )  . 
oncokb information is publicly available through an interactive web site19 and incorporated into the cbioportal for cancer genomics , 20 - 22 where patient genomic alterations are annotated with information from oncokb and their biologic effects and clinical implications are summarized , which facilitates cancer researcher and clinician interpretation of complex genomic data ( fig 1 )  . 
3 , 000 alterations in 418 cancer - associated genes ( table 1 )  . levels of evidence to communicate the clinical utility of individual mutant alleles consistently , a level of evidence classification system was developed ( fig 2 ) that takes into account the site of tumor origin by recognizing that the effects of targeted inhibitors vary by tumor lineage , even in cancers that share the same mutant allele ( fig 3 )  . 
potentially actionable alterations in a specific cancer type are assigned to one of four levels that are based on the strength of evidence that the mutation is a predictive biomarker of drug sensitivity to fdaapproved or investigational agents for a specific indication . 
level 1 includes genes for which specific alterations have been recognized by the fda as predictive of response to an fda - approved drug in a particular disease context ( data supplement )  . examples include braf v600e and either vemurafenib or dabrafenib as monotherapy or in combination with the mek inhibitors cobimetinib or trametinib in melanoma ; egfr l858r and erlotinib , afatinib , or gefitinib in nonsmall - cell lung cancer ( nsclc ) ; and mutations in exons 9 and 11 of kit and imatinib , sunitinib , and regorafenib in gi stromal tumors . 
in total , 82 alterations in 12 genes are considered level 1 ( data supplement )  . in recognition that some alterations in what would be considered a level 1 gene are intrinsically resistant to currently available fda - approved drugs or fall outside explicit fda approval , oncokb assigns individual alterations to a level of evidence as opposed to the entire gene . 
 variant databases gene alteration tumor type clinical implications incorporation of feedback onc kb oncokb.org web site statistical recurrence treatment guidelines akt1 scientific literature data sources breast cancer ovarian cancer lung cancer e17k e40k l52r q79k amplification prevalence prognosis nccn guidelines standard therapy clinical genomics annotation committee oncokb api cbioportal msk clinical reports investigational therapy curation review variant curation oncokb access fig 1 . 
data sources : alterations are identified by their recurrence18 from public variant databases ( cbioportal , cosmic [ catalogue of somatic mutations in cancer ] , the memorial sloan kettering [ msk ] impact internal clinical sequencing cohort ) , and by prior knowledge available in the literature . biologic and clinical therapeutic implications of alterations are curated from several public resources , including disease - specific treatment guidelines ; abstracts from major conference proceedings , such as asco , european society of medical oncology , and american association for cancer research ; and the scientific literature through pubmed . 
level 2a includes alterations that are not fda - recognized biomarkers but are considered standard care predictive biomarkers of response to an fda - approved therapy in specific cancer types . 
these alterations are highlighted in expert panel guidelines , such as the nccn compendium and asco clinical practice guidelines . several level 2a associations involve rare cancer types ( eg , braf v600e mutant histiocytosis ) or small subpopulations of common cancers ( eg , braf v600e mutant lung cancer ) , and therefore , accrual to a prospective randomized phase iii clinical study may not be feasible . 
because the total number of patients affected often is small , an application for an fda indication may never be filed , but disease experts consider the biomarker - drug association as a standard off - label use . 
in total , 11 genes with 85 alterations are currently considered level 2a ( data supplement )  . as an example , met exon 14 alterations are present in approximately 3% of nsclc27 and represent a distinct , molecularly defined subpopulation of lung adenocarcinomas that are mutually exclusive with tumors that harbor activating mutations in egfr and kras and fusions of alk , ros1 , and ret.28 - 30 an adequately powered randomized trial that compares the met inhibitor crizotinib with other standard approaches , such as chemotherapy and immunotherapy , has not yet been performed partly because of the rarity of these alterations . 
however , durable complete or partial responses to crizotinib and cabozantinib in patients with met exon 14altered lung cancers have been reported.27 , 31 although widely available as a result of its fda approval for use in alk fusionpositive nsclc , crizotinib is not explicitly fda approved in the setting of met exon 14altered nsclc . 
because the nccn guidelines consider off - label prescription of crizotinib a standard treatment approach for patients with lung cancer with met exon 14 alterations , 32 they are classified as level 2a ( fig 2 )  . 
although vemurafenib is not fda approved for use in patients with these specific braf v600e mutant indications , the off - label use of vemurafenib is a well - supported treatment option included in the nccn guidelines on the basis of compelling clinical data33 - 35 ( fig 3 )  . level 2b includes alterations that are standard predictive biomarkers of drug sensitivity in other tumor types but for which data in the tumor in question are either lacking or negative to date . 
for example , braf v600e mutations have been identified in several cancer types , including urothelial carcinomas and germ cell tumors , 36 , 37 for which no clinical response data are reported in the literature . 
in these tumors , the use of raf inhibitors in patients with braf mutant tumors remains investigational , and braf v600e is therefore classified as level 2b36 ( fig 3 )  . 
in patients with braf v600e mutant colorectal cancer , braf inhibitors , such as vemurafenib , have been tested with disappointing results.38 such negative data are referenced in oncokb and argue against the use of raf inhibitor monotherapy in patients with braf v600e colorectal cancers . 
level 3a includes mutations that are candidate predictive biomarkers of drug response on the basis of off - label use of fdaapproved drugs or investigational agents not yet fda approved for any indication . 
for the former , the evidence that supports the predictive value of the alteration is not considered sufficient to warrant a change in standard clinical practice , and disease experts would consider the use of the fda - approved drug in this context to be investigational . 
 into oncokb in real time . oncokb access : oncokb data are available for public use through an interactive web site19 and the cbioportal for cancer genomics22 and are used internally to annotate msk clinical reports . 
api , application program interface ; nccn , national comprehensive cancer network . activity has been reported , and the mutation - drug association is classified as level 3b in all other tumor types . 
fifty - five alterations in 25 genes are considered level 3 ( data supplement )  . a representative example of a level 3 alteration is akt1 e17k ( fig 3 )  . 
promising clinical activity consistent with preclinical studies of this compound has been reported with the investigational panakt inhibitor azd5363 in patients with akt1 e17k mutant breast , lung , cervical squamous , and endometrial cancers.40 - 42 on the basis of these emerging clinical data , akt1 e17k is classified as a level 3a mutation in breast , cervical , endometrial , ovarian , and lung cancers . 
a more complex example of level 3 alterations are erbb2 missense mutations that are present in a minority of a broad range of human cancers43 and that often arise in patients without erbb2 amplification or human epidermal growth factor receptor 2 ( her2 ) protein overexpression.44 these erbb2 mutants demonstrate varying degrees of sensitivity to her2 - selective kinase inhibitors , such as lapatinib and neratinib44 ( fig 3 )  . 
level 4 alterations are candidate predictive biomarkers of response to either fdaapproved or investigational agents on the basis of compelling laboratory data and an absence of substantiating compelling clinical data . 
although anecdotal responses to targeted agents may have been demonstrated in individual patients whose tumor harbored a level 4 alteration , the data are not sufficiently robust to indicate that the presence of the mutation is associated with significantly greater activity than tumors that lack the alteration . 
for example , although studies in mouseand patient - derived xenograft models have suggested that mammalian target of rapamycin or akt - targeted inhibitors may be effective in pten - null tumors , 46 the clinical data that support pten loss as a predictive biomarker of response to phosphatidylinositol 3 - kinase , akt , or mammalian target of rapamycin inhibitors in patients are limited and conflicting.47 - 52 therefore , classification of loss - of - function pten alterations as a level 4 alteration indicates that patients with pten - deficient tumors would be rational candidates for a clinical trial of investigational phosphatidylinositol 3 - kinase pathway inhibitors alone or in combination with other agents , but that the use of such agents outside the context of a clinical trial is not yet supported by the sum of the clinical data . 
additional examples of level 4 alterations include nf1 inactivating alterations , which may be predictive of response to mek1 / 2 inhibitors , 53 and egfr exon 20 insertions in lung adenocarcinomas that respond poorly to erlotinib54 , 55 but which may be sensitive to ap32788 , an investigational inhibitor of egfr and her256 ( fig 3 )  . 
because oncokb levels are dynamic , mutations currently classified as level 4 may be reclassified as level 3 or higher if additional compelling clinical data emerge . levels of resistance ( levels r1 to r3 )  . 
oncokb classifies mutations that have been shown to confer resistance to specific targeted therapies into one of three levels on the basis of the strength of the evidence that the mutation is predictive of treatment resistance ( fig 2 )  . 
level r1 includes mutational events for which there is sufficient evidence to recommend routine testing for the mutation to identify , with a high likelihood , patients who will not respond to a standard therapy . identification of r1 mutations , therefore , would lead to a recommendation that the associated therapy be withheld in patients whose tumors harbor the mutation . 
by definition , level r1 mutations predict for resistance to fda - approved drugs , and testing for such mutations is typically recommended by expert guidelines , such as those published by the nccn . 
level r1 alterations include activating ras mutations in colorectal cancer , which predict for resistance to the egfr - targeted monoclonal antibodies cetuximab and panitumumab57 , 57a ; egfr t790m mutations in nsclc , which predict for intrinsic and acquired resistance to the egfr tyrosine kinase inhibitors ( tkis ) erlotinib , afatinib , and gefitinib58 ; and pdgfra d842v , which predicts for oncokb annotation metric no . 
 level level level level level level level level level fda - recognized biomarker predictive of response to an fdaapproved drug in this indication standard care biomarker predictive of response to an fdaapproved drug in this indication * standard care biomarker predictive of response to an fdaapproved drug in another indication but not standard care for this indication compelling clinical evidence supports the biomarker as being predictive of response to a drug in this indication , but neither biomarker nor drug is standard care compelling clinical evidence supports the biomarker as being predictive of response to a drug in another indication , but neither biomarker nor drug is standard care compelling biologic evidence supports the biomarker as being predictive of response to a drug , but neither biomarker nor drug is standard care standard care biomarker predictive of resistance to an fda - approved drug in this indication compelling clinical evidence supports the biomarker as being predictive of resistance to a drug , but neither biomarker nor drug is standard care compelling biologic evidence supports the biomarker as being predictive of resistance to a drug , but neither biomarker nor drug is standard care standard therapeutic implications * includes biomarkers that are recommended as standard care by the nccn or other expert panels but not necessarily fda recognized for a particular indication investigational therapeutic implications possibly directed to clinical trials hypothetical therapeutic implications on the basis of preliminary , nonclinical data standard therapeutic implications hypothetical therapeutic implications on the basis of preliminary , nonclinical data fig 2 . 
standard therapeutic implications include food and drug administration ( fda ) recognized biomarkers that are predictive of response to an fda - approved drug in a specific indication ( level 1 ) and standard care biomarkers that are predictive of response to an fda - approved drug in a specific indication ( level 2a )  . 
investigational therapeutic implications include fda - approved biomarkers predictive of response to an fdaapproved drug detected in an off - label indication ( level 2b ) , fdaor nonfda - recognized biomarkers that are predictive of response to novel targeted agents that have shown promising results in clinical trials ( level 3a ) , and nonfdarecognized biomarkers that are predictive of response to novel targeted agents on the basis of compelling biologic data ( level 4 )  . 
nccn , national comprehensive cancer network . resistance to imatinib in patients with gi stromal tumors.59 alterations classified as levels r2 and r3 have hypothetical therapeutic implications and include alterations that are predictive of drug resistance on the basis of clinical and biologic data , respectively , but their use in guiding treatment decisions is considered investigational ( fig 2 )  . 
for example , although multiple strategies to reverse the oncogenic effects of tp53 loss have been explored in laboratory studies and early - phase clinical trials , 61 , 62 the agents tested do not directly target tp53 , their activity is typically not restricted to tp53 mutant models , and clinical trials that test these agents either have been aborted because of lack of efficacy or do not use tp53 status as a selection criterion.63 thus , although genomic alterations in tp53 are typically oncogenic , oncokb does not consider them therapeutically actionable . 
90% of alterations in oncokb have curated biologic effects and are classified as oncogenic but are not associated with actionability . actionable alterations across cancer types although targeted inhibitors have been shown to improve clinical outcomes in melanoma and lung cancer among others , 64 the broader clinical utility of large panel or whole - exome testing remains undefined . 
implicit in the designation of a level of evidence for each branch is whether the biomarker is food and drug administration ( fda ) recognized standard care or investigational and whether it is predictive of response to a drug that is fda approved or currently being tested in clinical trials . 
90% of samples harbored at least one known oncogenic mutation , only 41% had one or more alterations for which compelling clinical data currently exist to justify the use of a standard or an investigational agent ( levels 1 to 3b ) ( fig 4a )  . 
level 1 and 2a alterations were most common in melanoma ( 44% ) , ovarian cancer ( 21% , which includes 65 of 312 samples that have either germline or somatic brca1or brca2 - inactivating mutations ) , soft tissue sarcomas ( 19% on the basis of cdk4 amplifications , which predict response to palbociclib in welldifferentiated and dedifferentiated liposarcomas but not in other soft tissue sarcomas ) , nsclc ( 14% ) , esophagogastric cancer ( 13% ) , and breast cancer ( 12% )  . 
however , whereas 44% of melanomas had mutations that predict for clinical benefit with standard therapies in patients with melanoma , the majority of actionable alterations in lgg were associated with only investigational implications , with the most common mutation being idh1 r132c ( 77% of lgg samples ) , a level 3b alteration that is based on promising clinical data with the idh1 inhibitor ag - 120 in patients with acute myeloid leukemia ( figs 4a and 4b )  . 
in total , just over 10% of all samples had a level 3a mutation as their highest actionable alteration , a cohort of patients for which enrollment in a clinical trial would represent a compelling treatment option after standard treatments . 
in addition , approximately 15% of samples had level 3b alterations as their highest actionable event , ie , alterations for which promising clinical data have been observed in an investigational setting in another cancer type . on average , there were approximately three oncogenic mutations per sample , and the number of known oncogenic mutations per sample in tumor types was independent of overall mutation burden ( fig 4c )  . 
for example , although renal cell cancers had , on average , one oncogenic mutation per sample , these mutations were typically inactivating in tumor suppressors , such as vhl and pbrm1 , which are not clinically actionable at this time . 
in contrast , although thyroid cancers also on average had approximately one oncogenic mutation per sample ( fig 4c ) , these alterations were typically actionable , such as ret fusions and braf and nras mutations . 
frequencies of level of evidence 1 to 3 assignments in the cancer genome atlas cohorts . patient samples from 19 cancer types ( the cancer genome atlas ) are classified by the alteration that carries the highest level of evidence . 
 ( a ) inset pie chart : fraction of samples across all cancer types that carry a mutation considered actionable according to the levels of evidence , oncogenic but not actionable , or variants of unknown significance ( vus )  . 
cell color as shown in the key for the inset pie chart ( a )  . columns indicate sample tumor type , rows indicate gene alteration present in sample , and numbers indicate the percentage of samples per tumor type that harbor an alteration in each gene . 
 ( c ) each patient sample was classified by the number of oncogenic alterations or the number of actionable alterations . shown is the mean number of actionable ( black ) , oncogenic ( dark gray ) , or total ( gray ) mutations per sample per tumor type . 
 ( d ) each tumor type was evaluated for the percentage of samples that carry zero , one , two , three , or four or more actionable mutations per sample ( indicated in shades of blue )  . 
 mutations ( 31% , 25% , and 22% , respectively ) , which is consistent with data that demonstrate that these tumor types are driven by multiple oncogenic mutations in nonredundant pathways65 - 68 ( fig 4d ) and may explain why targeted monotherapies have shown disappointing results to date in some of these cancer types.69 , 70 discussion since the introduction of imatinib for chronic myeloid leukemia more than a decade ago , 71 , 72 a growing number of drugs that target specific genetic alterations required for tumor initiation and progression have been shown to significantly improve outcomes in molecularly defined populations of patients with cancer.64 , 73 - 74a although tumor genetic testing is now part of routine patient care in an increasing number of tumor types , interpretation of variants remains an important challenge , and in major academic cancer centers , a significant proportion of physicians report low confidence in their ability to make optimal treatment recommendations on the basis of genomic information.75 although multiple classification systems exist for the annotation of germline variants , 76 , 77 efforts to define the clinical utility of somatic alterations have been limited to established biomarkers , 78 - 80 and prior efforts often have classified actionability as a binary variable that results in the grouping of biomarkers that are fda recognized with those that are nonactionable but oncogenic . 
to this end , we assigned each mutation to one of four levels that are based on available clinical and laboratory data that support the use of the mutation as a predictive biomarker . 
standard therapeutic implications are classified as either level 1 or 2a to recognize that not all mutation - drug associations used in standard practice have been recognized by the fda . 
moreover , there are cases where off - label use of an fda - approved drug is explicitly not warranted because of existing data that argue against the use of a targeted agent in a specific cancer type . 
for example , although the braf inhibitor vemurafenib is a standard treatment option for patients with braf v600e mutant melanoma or nsclc , robust clinical reports from multiple independent centers demonstrated that patients with braf v600e mutant colorectal cancer do not respond to raf inhibitors , at least as monotherapy.38 , 84 similarly , although erbb2 amplification predicts for the clinical utility of her2 - targeted therapies in breast and esophagogastric cancers , the clinical activity of trastuzumab in erbb2 - amplified lung cancers has been disappointing.85 braf v600e and erbb2 amplification are , therefore , level 2b when detected in colorectal cancers . 
 individual mutant alleles within a single gene may be functionally distinct , with different predictive value and , therefore , individual therapeutic implications , which complicates the development of clinical decision support tools , particularly in the context of often - vague fda labeling and expert guidelines , such as those provided by the nccn , that may not define at a granular level whether specific mutations within a gene are predictive of drug response . 
to address this complexity , oncokb groups mutations in level 1 genes , such as egfr and kit , according to whether they are biologically active , whether there are preclinical data to suggest that the allele is sensitive or resistant to the matched targeted agents , and whether there are clinical data to suggest clinical sensitivity or intrinsic resistance to the approved targeted therapy . 
the challenge of rare drug - sensitive variants in level 1 genes also highlights the need for consortia efforts , such as the american association for cancer research project genie ( genomics evidence neoplasia information exchange ) , which should allow for the collection of clinical response data for rare alleles to help to guide the treatment of patients with these less common mutations . although new laboratory and clinical data are continually generated , fda labels and professional guidelines are updated at irregular intervals . 
for example , although explicit fda approval of crizotinib in ros1 - rearranged nsclc did not occur until march 2016 , offlabel use of crizotinib in patients with ros1 fusion - positive lung cancers has been considered standard of care by several expert groups for some time.86 - 88 as another example , whereas kras was initially considered a level 3a alteration in nsclc on the basis of promising data from the randomized phase ii study that supplemented standard chemotherapy with a mek inhibitor , 89 the subsequent phase iii trial showed no survival benefit with this combination , 90 which is consistent with negative data associated with mek inhibitor use in kras mutant pancreatic and colorectal cancers.91 , 92 nonetheless , anecdotal clinical and compelling preclinical data support the use of kras as a predictive biomarker of sensitivity to novel mek and erk inhibitors alone or in combination with other agents.93 - 97 oncokb thus recognizes and reassigns the level of evidence of mutational events , if appropriate , on the basis of newer , moredefinitive , and negative randomized clinical data , which take precedence over prior preliminary clinical findings . to incorporate new clinical and research findings , we have made the oncokb annotation available publically through an interactive web site19 and through the cbioportal for cancer genomics.22 both systems include a comment feature to facilitate crowdsourcing curation of this knowledge base . 
user suggestions are evaluated by the scientific team and incorporated into oncokb through periodic updates . oncokb is also an active member in efforts to promote harmonization of variant annotation across existent knowledge bases and is participating in both clingen and the global alliance for genomic health through the variant interpretation cancer consortium . in the future , we will curate information about mutational signatures , such as overall mutation burden and the possible link to immunotherapy , mutational clonality , and the impact on drug sensitivity of co - occurrence of specific oncogenic and actionable mutations . 
rudolph , ederlinda paraiso collection and assembly of data : debyani chakravarty , jianjiong gao , sarah phillips , ritika kundra , hongxin zhang , tara soumerai , moriah h . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . debyani chakravarty no relationship to disclose jianjiong gao no relationship to disclose sarah phillips no relationship to disclose ritika kundra no relationship to disclose hongxin zhang no relationship to disclose jiaojiao wang no relationship to disclose julia e . 
chang no relationship to disclose rona yaeger consulting or advisory role : glaxosmithkline , advaxis sarat chandarlapaty honoraria : chugai pharmaceutical , foresite capital , astrazeneca , sermonix pharmaceuticals , macrogenics , agendia research funding : eli lilly ( inst ) , novartis ( inst ) travel , accommodations , expenses : chugai pharmaceutical , macrogenics , astrazeneca tiffany a . 
traina consulting or advisory role : genentech , roche , eisai , mundipharma , medivation , pfizer , astrazeneca , bayer ag , immunomedics , merck research funding : medivation , eisai , pfizer , novartis , myriad genetics , innocrin pharmaceuticals , astrazeneca paul k . 
paik honoraria : celgene , bristol - myers squibb , eli lilly , ariad pharmaceuticals consulting or advisory role : celgene , eli lilly , ariad pharmaceuticals , bristol - myers squibb , celgene research funding : celgene , emd serono travel , accommodations , expenses : emd serono alan l . 
ho consulting or advisory role : oncology consortium , bristol - myers squibb , eisai , genzyme , merck , novartis , sun pharmaceutical industries , kura oncology speakers bureau : medscape , omniprex america , eli lilly , genentech , roche , astrazeneca , bayer ag , kura oncology , kolltan pharmaceuticals , eisai , astrazeneca travel , accommodations , expenses : janssen pharmaceuticals , merck , kura oncology feras m . 
hantash employment : quest diagnostics stock and other ownership interests : quest diagnostics patents , royalties , other intellectual property : patents on molecular methods , but not related to manuscript andrew grupe employment : quest diagnostics stock and other ownership interests : quest diagnostics patents , royalties , other intellectual property : patents or patent applications travel , accommodations , expenses : quest diagnostics shrujal s . 
danila honoraria : astellas pharma , angle , bayer ag , janssen pharmaceuticals consulting or advisory role : angle , bayer ag research funding : prostate cancer foundation , genentech , janssen pharmaceuticals ( inst ) patents , royalties , other intellectual property : gene expression profile associated with prostate cancer travel , accommodations , expenses : cambridge healthtech institute , prostate cancer foundation , angle , bayer ag , american austrian foundation open medical institute , global technology community , janssen pharmaceuticals , oncology education mrinal gounder honoraria : amgen , daiichi sankyo , karyopharm therapeutics , tracon pharmaceuticals , amgen consulting or advisory role : daiichi sankyo , karyopharm therapeutics , epizyme speakers bureau : amgen travel , accommodations , expenses : amgen travel , accommodations , expenses : daiichi sankyo , karyopharm therapeutics james j . 
harding no relationship to disclose dana rathkopf consulting or advisory role : janssen pharmaceuticals research funding : janssen pharmaceuticals ( inst ) , medivation ( inst ) , celgene ( inst ) , takeda pharmaceuticals ( inst ) , millennium pharmaceuticals ( inst ) , ferring pharmaceuticals ( inst ) , novartis ( inst ) , taiho pharmaceutical ( inst ) , astrazeneca ( inst ) , genentech ( inst ) , roche ( inst ) , tracon pharmaceuticals ( inst ) alexander n . 
shoushtari consulting or advisory role : vaccinex , castle biosciences , immunocore research funding : bristol - myers squibb , immunocore travel , accommodations , expenses : bristol - myers squibb neerav shukla no relationship to disclose martin h . 
voss honoraria : novartis consulting or advisory role : novartis , calithera biosciences , natera , glaxosmithkline , exelixis , pfizer , alexion pharmaceuticals research funding : pfizer , bristol - myers squibb , genentech , roche travel , accommodations , expenses : novartis , takeda pharmaceuticals matthew d . 
hellmann consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca , medimmune , novartis , janssen pharmaceuticals research funding : bristol - myers squibb , genentech , roche ederlinda paraiso no relationship to disclose ahmet zehir no relationship to disclose gopa iyer no relationship to disclose yelena y . 
levine stock and other ownership interests : critical outcome technologies consulting or advisory role : clovis oncology , mtrap , biodesix , tesaro maeve lowery consulting or advisory role : agios , celgene antonio omuro consulting or advisory role : stemline therapeutics , juno therapeutics , bristol - myers squibb , oxigene , alexion pharmaceuticals , astrazeneca , inovio pharmaceuticals , merck michael a . 
postow honoraria : bristol - myers squibb , merck consulting or advisory role : amgen , bristol - myers squibb , novartis research funding : bristol - myers squibb ( inst ) , novartis ( inst ) , array biopharma ( inst ) , infinity pharmaceuticals ( inst ) travel , accommodations , expenses : bristol - myers squibb leonard b . 
riely consulting or advisory role : novartis , genentech research funding : novartis ( inst ) , roche ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , infinity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) patents , royalties , other intellectual property : patent application submitted that covers pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : novartis marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network , boehringer ingelheim , astrazeneca research funding : loxo oncology ( inst ) david m . 
 jos e baselga leadership : infinity pharmaceuticals , varian medical systems , grail , foghorn stock or other ownership : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , varian medical systems , tango , foghorn , aura biomedical , apogen , northern biologics honoraria : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , northern biologics consulting or advisory role : eli lilly , novartis , grail patents , royalties , other intellectual property : combination therapy using pdk1 and pi3k inhibitors . 
may 16 travel , accommodations , expenses : roche / genentech paul sabbatini research funding : bristol - myers squibb ( inst ) , ludwig institute for cancer research ( inst ) david b . 
solit honoraria : loxo oncology , pfizer consulting or advisory role : pfizer , loxo oncology nikolaus schultz no relationship to disclose acknowledgment we thank the following individuals for serving as oncokb curators : andrew intlekofer , eric smith , piro lito , jaclyn hechtman , dmitriy zamarin , wassim abida , mythili koneru , weiyi toy , pedram razavi , philip iaquinta , byron lee , martin dalin , matthew jones , elizabeth adams , karuna ganesh , olga guryanova , carolyn jackson , william terry , yu chen , ping chi , eduard reznik , aphrothiti hanrahan , sevin turcan , philip watson , neeman mohibullah , elena goldberg , aaron viny , emily foley , samuel kaffenberger , andrew winer , connie batlevi , helen won , lindsay saunders , kinisha gala , philip jonsson , fiona brown , eneda toska , i~nigo landalopez , and tripti shrestha - bhattarai . affiliations debyani chakravarty , jianjiong gao , sarah phillips , ritika kundra , hongxin zhang , jiaojiao wang , julia e . 
j am med inform assoc 10.1093 / jamia / ocw148 [ epub ahead of print on october 27 , 2016 ] institute of precision medicine : welcome to the precision medicine knowledgebase . 
kim kb , kefford r , pavlick ac , et al : phase ii study of the mek1 / mek2 inhibitor trametinib in patients with metastatic braf - mutant cutaneous melanoma previously treated with or without a braf inhibitor . 
paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
ma pc , jagadeeswaran r , jagadeesh s , et al : functional expression and mutations of c - met and its therapeutic inhibition with su11274 and small interfering rna in non - small cell lung cancer . 
ma pc , kijima t , maulik g , et al : c - met mutational analysis in small cell lung cancer : novel juxtamembrane domain mutations regulating cytoskeletal functions . 
frampton gm , ali sm , rosenzweig m , et al : activation of met via diverse exon 14 splicing alterations occurs in multiple tumor types and confers clinical sensitivity to met inhibitors . 
planchard d , besse b , groen hj , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
davies br , greenwood h , dudley p , et al : preclinical pharmacology of azd5363 , an inhibitor of akt : pharmacodynamics , antitumor activity , and correlation of monotherapy activity with genetic background . 
hyman dm , smyth l , bedard pl , et al : abstract b109 : azd5363 , a catalytic pan - akt inhibitor , in akt1 e17k mutation positive advanced solid tumors . 
hyman d , piha - paul s , rod on j , et al : abstract pd5 - 05 : neratinib for erbb2 mutant , her2 non - amplified , metastatic breast cancer : preliminary analysis from a multicenter , open - label , multi - histology phase ii basket trial . cancer res 76 : pd5 - 05 , 2016 46 . 
lin j , sampath d , nannini ma , et al : targeting activated akt with gdc - 0068 , a novel selective akt inhibitor that is efficacious in multiple tumor models . 
clin cancer res 19 : 1760 - 1772 , 2013 de bono js , de giorgi u , massard c , et al : pten loss as a predictive biomarker for the akt inhibitor ipatasertib combined with abiraterone acetate in patients with metastatic castration - resistant prostate cancer ( mcrpc )  . 
ma cx , luo j , naughton m , et al : a phase i trial of bkm120 ( buparlisib ) in combination with fulvestrant in postmenopausal women with estrogen receptor - positive metastatic breast cancer . 
rodon j , bra~na i , siu ll , et al : phase i dose - escalation and - expansion study of buparlisib ( bkm120 ) , an oral panclass i pi3k inhibitor , in patients with advanced solid tumors . 
yang l , clarke mj , carlson bl , et al : pten loss does not predict for response to rad001 ( everolimus ) in a glioblastoma orthotopic xenograft test panel . 
naidoo j , sima cs , rodriguez k , et al : epidermal growth factor receptor exon 20 insertions in advanced lung adenocarcinomas : clinical outcomes and response to erlotinib . 
yasuda h , park e , yun ch , et al : structural , biochemical , and clinical characterization of epidermal growth factor receptor ( egfr ) exon 20 insertion mutations in lung cancer . 
gonzalvez f , zhu x , huang w - s , et al : abstract 2644 : ap32788 , a potent , selective inhibitor of egfr and her2 oncogenic mutants , including exon 20 insertions , in preclinical models . 
druker bj , sawyers cl , kantarjian h , et al : activity of a specific inhibitor of the bcr - abl tyrosine kinase in the blast crisis of chronic myeloid leukemia and acute lymphoblastic leukemia with the philadelphia chromosome . n engl j med 344 : 1038 - 1042 , 2001 72 . 
druker bj , talpaz m , resta dj , et al : efficacy and safety of a specific inhibitor of the bcr - abl tyrosine kinase in chronic myeloid leukemia . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
macarthur dg , manolio ta , dimmock dp , et al : guidelines for investigating causality of sequence variants in oncol 32 : 1317 - 1323 , 2014 human disease . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
simon rm , paik s , hayes df : use of archived specimens in evaluation of prognostic and predictive biomarkers . j natl cancer inst 101 : 1446 - 1452 , 2009 81 . 
conti rm , bernstein ac , villaflor vm , et al : prevalence of off - label use and spending in 2010 among patentprotected chemotherapies in a population - based cohort of medical oncologists . 
langer cj , stephenson p , thor a , et al : trastuzumab in the treatment of advanced non - small - cell lung cancer : is there a role ? focus on eastern cooperative oncology group study 2598 . 
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cell 131 : 1190 - 1203 , 2007 janne pa , shaw at , pereira jr , et al : selumetinib plus docetaxel for kras - mutant advanced non - small - cell lung cancer : a randomised , multicentre , placebo - controlled , phase 2 study . 
clin lung cancer 17 : e1 - e4 , 2016 infante jr , fecher la , falchook gs , et al : safety , pharmacokinetic , pharmacodynamic , and efficacy data for the oral mek inhibitor trametinib : a phase 1 dose - escalation trial . 
rinehart j , adjei aa , lorusso pm , et al : multicenter phase ii study of the oral mek inhibitor , ci - 1040 , in patients with advanced non - small - cell lung , breast , colon , and pancreatic cancer . 
hu - lieskovan s , mok s , homet moreno b , et al : improved antitumor activity of immunotherapy with braf and mek inhibitors in braf ( v600e ) melanoma . 
kakavand h , wilmott js , menzies am , et al : pd - l1 expression and tumor - infiltrating lymphocytes define different subsets of mapk inhibitor - treated melanoma patients . 
loi s , dushyanthen s , beavis pa , et al : ras / mapk activation is associated with reduced tumor - infiltrating lymphocytes in triple - negative breast cancer : therapeutic cooperation between mek and pd - 1 / pd - l1 immune checkpoint inhibitors . 
yoon yk , kim hp , han sw , et al : kras mutant lung cancer cells are differentially responsive to mek inhibitor due to akt or stat3 activation : implication for combinatorial approach . 
 precision oncology and the universal health coverage system in japan hiromichi ebi , md , phd1 , 2 , 3 and hideaki bando , md , phd4 although precision oncology is transforming clinical management of patients with cancer , many hospitals face challenges to effectively implement precision oncology . 
the most promising development is that tests to prole the genomes of select cancers are now fully covered by the national health insurance systein may 2019 , two gene panels were approved with reimbursement : foundationone cdx cancer genomic prole and oncoguide ncc oncopanel system , the latter of which was developed in japan . 
to make better use of scarce resources , the reimbursement is restricted to patients with solid tumors that have progressed on standard chemotherapy , rare tumors , or tumors of unknown primary . 
in addition , japans national cancer center launched a center for cancer genomics and advanced therapeutics ( c - cat ) that collects genomic information and clinical characteristics of patients who received genomic proling tests . 
the centralized system under the national health insurance system could be a double - edged sword . although tight regulation may make it hard to keep up with the rapid development of precision oncology , a federated ecosystem for sharing clinical and genomic data will be a precious asset and allow for shared access to data . 
high - cost medical expense benet also denes maximum out - of - pocket payment month according to household income of the patient . for example , the maximum is roughly $800 for a household income of approximately $34 , 000$70 , 000 . 
although for - prot insurance companies have voluntary health insurance programs , holding this type of insurance does not exempt an individual from mandatory enrollment in the universal health coverage scheme . 
the role of voluntary health insurance is supplemental and complements social health insurance benet packages . prices for all drugs and devices reimbursed by the universal health coverage system are the ofcial price set by the government ( japanese ministry of health , labor , and welfare [ mhlw ] )  . 
if a physician uses an unapproved device or off - label drug , any costs related to the patient , including but not limited to blood tests and physician fees , are not reimbursed . 
therefore , any cancer genomic proling tests must be examined and approved by the pharmaceuticals and medical devices agency ( pmda ) and mhlw before insurance reimbursement is set by the government , unless all the cost is to be paid by the patients . 
 ebi et al context key objective to summarize the framework of precision oncology recently arranged in japan . knowledge generated the japanese government designated core , hub , and liaison hospitals for cancer genomic medicine . 
also , reimbursement applies only to patients who nished standard chemotherapy , as a way to restrict potentially unnecessary investigations . relevance each country must design a precision oncology initiative under their distinct social care systejapan is an example of a centralized precision oncology under a universal health care coverage system . for clinical trials , even when gene proling testing identies actionable alterations . the japanese mhlw has a structured system to promote the development of drugs and devices under governmental regulations . 
although system a is designed for intervention with approved drugs / devices or minimally invasive intervention with unapproved drugs / devices , system b is designed for unapproved drugs or medical technologies . 
the patientrequested therapy system is also expected to be used as the japanese version of what the united states has hailed as the compassionate use prograto start off - label drug treatment using patient - requested therapy systems , it is necessary to pass several review processes equivalent to clinical trials , and the cost of the unapproved medical care should be fully paid by the patients . 
second , similar to the breakthrough therapy designation by the us food and drug administration , mhlw has the sakigake program , an accelerated inspection scheme for rapid authorization of unapproved drugs and devices . 
beginning around 2010 , pan - cancer genome screening started in japan by using researchuse only next - generation sequencing ( ngs ) panels.2 to promote genome - based clinical trials , the nationwide genome screening consortium for lung cancer was launched in february 2013 . 
the group , lc - scrum - japan , originally aimed to identify patients harboring ros1 and ret fusions originally discovered in japan.3 in february 2014 , gi - screen - japan multicenter screening project also started for gi cancer . 
the project began to screen for braf , nras , and pik3ca mutations in patients with metastatic colorectal cancer , using multiplex polymerase chain reaction ( pcr ) and luminex ( xmap ) technology.4 in february 2015 , these two groups merged into scrumjapan and started to use oncomine comprehensive assays as a screening platform.5 with the advent of plasma - based genome screening , scrum - japan subsequently started plasma - based ngs using guardant 360 . 
the screening and associated clinical trials have been research based , funded by government agencies through grant mechanisms ( the japan agency for medical research and development or the national cancer center research and development fund ) as well as by pharmaceutical companies . 
therefore , patients were not required to pay screening costs for any of these studies . from february 2013 to december 2018 , 6 , 860 and 6 , 391 patients were enrolled in lc - scrum - japan and gi - screenjapan , respectively . 
on the basis of this screening platform , 28 umbrella and 20 basket - type genome - based studies have been conducted.6 one of the notable accomplishments was a clinical trial of vandetanib , for patients with ret - rearranged nonsmall - cell lung cancer ( nsclc ) identied by the screening . 
 precision oncology in japan results of clinical trials conducted by lc - scrum japan led to the approval of crizotinib for the treatment of ros1translocated nsclc and the combination of trametinib and dabrafenib for use in patients with braf v600e - mutant nsclc . 
scrum - japan also contributed to the approval of in vitro diagnostic testing by pmda including simultaneous detection of ras and braf mutations in colorectal cancer , 8 oncomine dx target test cdx ngs panel for egfr and braf mutations and ros1 and alk translocations in nsclc , pcr - based microsatellite instability testing for solid tumors , 9 and plasma - based ras mutation testing for colorectal cancer.10 another notable genome screening is the top - gear ( trial of oncopanel for gene proling to estimate both adverse events and response ) project , which is a prospective cohort study conducted by japans national cancer center ( ncc ) to investigate the feasibility and utility of an ngsbased panel customized for japanese patients with cancer ( ncc oncopanel ) .11 this work was carried out within the context of the sakigake program and clinical utility was investigated within the advanced medical care b system . during the second stage of the top - gear project , 187 patients with advanced solid tumors obtained the gene proling data , and 25 ( 13.3% ) of them have received molecular - targeted therapy on the basis of their genome alterations.12 the achievements of this project led to governmental approval for the oncoguide ncc oncopanel system . some other medical university hospitals are also developing their own genome screening systems . 
these tests are performed under the advanced medical care b systekyoto university hospital ( oncoprime ) 13 , 14 and keio university hospital ( plessision - rapid ) offer their screening service outside of the national health care systerecently , keio university hospital started a whole - exon sequencing service ( plessision - exome )  . 
importantly , the report also concluded that cancer genome medicine should be accomplished under a universal health coverage systeafter the report , the japanese government designated 11 hospitals throughout japan to serve as core hospitals for cancer genomic medicine . 
the eligibility to be designed as a hub hospital is based on their ability to organize their resources and infrastructure akin to the core hospitals , which have their own molecular tumor board ( mtb ) and organic capabilities to run clinical trials . in addition , core hospitals have more responsibilities to train fellows and clinical coordinators and to be involved in translational research . 
liaison hospitals , on the other hand , are dependent on core and hub hospitals for their sequencing , reports , and mtb ( fig 1 )  . from the academia side , three major japanese cancerrelated societies ( the japanese society of medical oncology [ jsmo ] , the japanese society of clinical oncology [ jsco ] , and the japanese cancer association [ jca ] ) issued consensus clinical practice guidelines for ngs - based cancer tests in october 2017.18 the guideline dened the evidence level of each genomic alteration suitable for the japanese medical care system in harmony with classications of evidence levels set by regulators in the united states and european union ( eu ) .19 in june 2018 , japans national cancer center founded the center for cancer genomics and advanced therapeutics ( c - cat ) to coordinate an integrated network of core , hub , and liaison hospitals . 
c - cat is expected to aggregate and deploy cancer genomic medicine information to advance the quality of health care offered under the universal health coverage system and to devise new modalities of health care ( fig 2 )  . 
first , the center has been constructing a cancer knowledge database ( ckdb ) optimized for japan to assist in decision making by mtbs . c - cat will collect and share updated information on clinical trials , promoting and improving matching between patients genomic data and clinical trials . 
oncoguide ncc oncopanel system is a 114 - gene ngs panel for tumor and germline analysis developed by japans ncc and health instrument maker sysmex corp , and foundationone cdx cancer genomic prole ( foundation medicine ) sequences 324 genes and also can detect microsatellite instability . oncoguide ncc oncopanel system was approved as a device combining the oncoguide ncc oncopanel kit and the oncoguide ncc oncopanel analyzing systein contrast , although foundation medicine had to be reviewed 11 core hospitals 34 hub hospitals 122 liaison hospitals their quality for sample analysis by pmda for the approval , pmda could not perform assessment as an in vitro diagnostic because the analysis was done in the united states . 
first , physicians submit tumor samples for foundationone cdx analysis to foundation medicine , and foundation medicine performs sequencing and reports the variant calls in an xml le , uploaded to a portal site created by chugai , a subsidiary of roche . 
because this step is not subject to reimbursement , and to set up a procedure suitable for reimbursement , physicians need to download the xml le from the portal site and then send it back to foundation medicine . 
in addition , the japanese act on the protection information denes genomic sequence as of personal personal information that was amended in response to the general data protection regulation enacted by the eu . 
on comply with the law , written consent consent , samples are sent to third parties outside of japan to analyze personal information and sequence data . after approval by pmda , the mhlw granted the use of these two gene panel analyses and set the ofcial price of reimbursement at the end of may 2019 . 
the second reimbursement is 480 , 000 , applied after the physician explains the results to patients following train personnel for precision medicine play central role in running clinical trials based on molecular profiling translational research run molecular tumor board run clinical trials based on molecular profiling provide patients with genomic testing interpretation is supported by core and hub hospitals refer patients to core and hub hospitals for clinical trial fig 1 . 
the test is approved for patients with solid tumors that have progressed on standard chemotherapy , with rare tumors , or with cancers of unknown primary . foundationone cdx is also approved for the use of companion diagnostic tests , such as those for the detection of egfr , ras , and braf mutations during standard care . for these companion dihowever , agnostic tests is much cheaper . 
furthermore , the results obtained outside of companion diagnostics will not be taken the reimbursement into consideration for decision making about treatment even when the test analyzes a number of genes . 
if a physician uses a test result during standard care , the difference for companion between the amount of reimbursement diagnostics and the actual cost paid to foundation medicine will be a decit for the hospital . 
if the physician wants to use the test results when the patient experiences progression while receiving standard therapy , additional reimbursement can be submitted as a fee for mtb ( 480 , 000 )  . 
 precision oncology in japan patient dies during standard care or fails to follow - up , it is unlikely that genome proling would be used during standard therapy in japan under current reimbursement rules . although only a few hospitals run these genome panels inhouse , most hospitals outsource these genomic proling tests to a clinical testing company . 
laboratories in core and hub hospitals are required to be certied by independent organizations such as iso15189 to handle patient samples . clinical testing companies also have clinical laboratory improvement amendments certication . 
formalin - xed and parafn - embedded samples ( and also blood samples in case of oncoguide ncc oncopanel system ) are prepared in each hospital and sent to the company . 
turnaround time in general is 16 to 22 days . to fulll its function as a data repository and to facilitate access to clinical data , a requirement of test granted by the government is that physicians need to submit detailed clinical data from patients with cancer to c - cat , including diagnostics , treatment , and outcomes information , as well as the raw bam or fastq and vcf or xml les ( fig 2 ; in japan , each hospital has an appendix table a1 )  . electronic platform that contains individual health records for patients . 
test results are usually reported in pdf les that are incorporated into electronic medical records , making it difcult for physicians to match patients with ongoing clinical trials or to identify patients who are eligible for new drugs when they become available . thus , a central data repository at c - cat will make it easier to identify candidates for clinical trials in a timely manner . using the submitted data , c - cat also issues their own report . 
ckdb1 is further divided into four databases : marker database listing genomic abnormalities such as egfr mutation or brca1 germline mutation ; drug database listing approved drugs or drugs under clinical trials in and outside of japan and their targets ; evidence database curated from biologic , clinical , and therapeutic information in multiple public information resources , including civic ( clinical interpretation of variants in cancer ) , brca exchange , clinvar , and cosmic ( catalogue of somatic mutations in cancer ) ; and a clinical trial database generated from clinicaltrials.gov as well as several japanese clinical trial registries . 
for instance , a patient with a druggable mutation needs to be treated by the appropriate drug , even as an off - label indication in the absence of a clinical trial or current approval . 
patient - requested therapy system , a japanese compassionate use program , has to be initiated by the request from a patient to the government with required documentation from physician . because the preparation of documents is a heavy burden for physicians , the system has not been widely adopted . also , as mentioned above , the cost of the drug has to be fully paid by the patient . 
to enable large basket / umbrella trials , a core facility supporting the protocol creation , drug distribution , monitoring , and audit will be needed , similar to the cancer therapy evaluation program in the united states . the other big challenge facing japanese precision oncology is the timing of reimbursements for genome proling tests . 
in addition , it was difcult to grant the use of cancer genomic proling during standard care because clear evidence for the benet of testing did not exist when consensus clinical practice guidelines for ngs - based cancer testing were published . 
for example , french clinical trials suggested the use of molecularly targeted agents outside established indications do not improve progression - free survival for heavily pretreated patients with cancer when compared with oncologists preferred treatment regimen.20 however , patients who experienced progression while receiving standard chemotherapy tend to have poor performance status and may not have enough time to wait for the results of genomic testing ; even in the very best case scenarios , their tumors will continue to grow and their health worsen each day that they are required to wait . 
currently , uncovered genome screening services are the only option for patients without rare tumors and before disease progression with standard therapy . quality and sustainability of mtbs are also challenging . 
however , a problem that arises is that it is challenging to demand this level of participation of physicians , given their limited availibility.21 overall , the cost for precision oncology is a heavy burden for hospitals . 
to put this into global perspective , memorial sloan kettering cancer center has already achieved clinical sequencing of 10 , 000 patients in the united states.22 furthermore , the united kingdom nished sequencing for  . 
in september 2019 , the mhlv unveiled a project with the goal of sequencing whole genomes from 100 , 000 patients with cancer over 3 years , a number chosen by referring to the united kingdoms sequencing achievements . 
although details of the project have not emerged yet , it is expected to result in the analyses of fresh frozen samples in collaboration with biobanks at core and hub hospitals . 
as the primary aim is to accelerate the development of new diagnostics and treatments , the project should be research based and funded by the japanese government and private sources . 
although the primary purpose of this initiative in precision oncology is to harness articial telligence ( ai ) for improved genomic analyses and drug target identication , the use of ai could connect genomic data with other prioritized areas in this initiative , such as pathology and radiology . 
the relatively homogenous genetic background of the japanese population and the detailed clinical outcomes collected by c - cat will be an advantage when harnessing the power of genomic data to develop new therapies . 
also , the genomic and clinical data would be integrated with other japanese databases , such as the medical genomics japan variant database and the japanese multi omics reference panel.23 conclusion in conclusion , precision oncology covered by the health insurance system has just begun in japan . 
on the other hand , although the japanese health care system has so far achieved excellent health outcomes with a relatively low cost , 24 the centralized structure under the national health insurance system with its inherent tight regulation may cause difculty in keeping up with the rapid development of precision oncology . 
in the united kingdom , genomics england was founded as a subsidiary limited company , as it was the most effective way to ensure the project running as quickly as possible . 
in the united states , for instance , protocols and treatment decisions surrounding personalized medicine are largely decided by the institutions treating the patients , with governing bodies like the national cancer institute playing ancillary roles and the ability to pay for patient care largely dictated by individuals private insurance policies . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . hiromichi ebi honoraria : taiho pharmaceutical , astrazeneca consulting or advisory role : merck serono , eli lilly , astellas pharma hideaki bando honoraria : taiho pharmaceutical , lilly japan , takeda , chugai pharma , sano , yakult honsha research funding : astrazeneca , sysmex no other potential conicts of interest were reported . acknowledgment we thank anthony faber , md ( vcu massey cancer center ) , for critical reading of the manuscript . references 48 : 559 - 564 , 2018 sakamoto h , rahman m , nomura s , et al : japan health system review . 
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li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular proling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
nucleic acids res 46 : d551 - d557 , 2018 ikegami n , yoo bk , hashimoto h , et al : japanese universal health coverage : evolution , achievements , and challenges . 
anthony blau rebecca boddicker ron bose seruga bostjan theresa boyle priscilla brastianos james brigarolas thomas brown mark burkard john burn jaume capdevila richard carvajal daniel catenacci jamie chaft marjan champine chang chan james chen mark chiang elena gabriela chiorean david chism atish choudhury james cleary eric collisson howard colman ryan corcoran brian crompton daniel crona william dahut adil daud michael davies kurtis davies francesca demichelis jennifer diamond adam dicker max diehn robert doebele alexander drilon steven dubois suhendan ekmekcioglu aymen elfiky leif ellisen anna farago phillip febbo sara federico michael feldman emmanouil fokas james ford william foulkes terence friedlander shirish gadgeel vijayakrishna gadi judy garber michael gatza thomas george giuseppe giaccone marios giannakis hannah gilmore bert glader ramaswamy govindan lipika goyal stacy gray joshua gruber matthew gubens michael hall heather hampel sigurdis haraldsdottir andrew harris derrick haslem eric haura florette hazard yijing he andrew hendifar daniel hertz cinta hierro kim hirshfield david hsu franklin huang willy hugo hatim husain a . 
 steven isakoff gopa iyer katherine janeway yelena janjigian filip janku randy jensen rinath jeselsohn neil johnson hossein khiabanian samuel klempner todd knepper wendy kohlmann takashi kohno scott kopetz carl koschmann vessela kristensen ian krop shivaani kummar marc ladanyi albert lai aly - khan lalani josh lauring alexander lazar dung le christophe le tourneau sarah leary sooyoun lee benjamin levy mark lewis jessica lin geoffrey lindeman jeffrey lipton stephen liu roger lo tamara lotan christine lovly ying lu david lum patrick ma subha madhavan luke maese roberta maestro david mangum juan martin - liberal renato martins clinton mason joaquin mateo david mcconkey bruno medeiros alexander menzies rodney miles c . 
chung , phd1 purpose brca1 or brca2 loss of function results in homologous recombination deciency ( hrd ) , which is targetable by poly ( adp - ribose ) polymerase ( parp ) inhibitors and other dna - damaging agents . 
in cancers associated with germline brca1 / 2 alterations ( brca1 / 2 - associated cancers : breast , ovarian , pancreatic , prostate ) , brca1 / 2 alterations result in hrd and are biomarkers for parp inhibitor use . 
across cancer types , biallelic brca1 / 2 alteration was associated with increased gloh versus monoallelic or wild - type brca1 / 2 ; predicted germline or somatic mutations were both associated with elevated gloh . conclusion biallelic brca1 / 2 alterations were associated with elevated gloh in diverse cancer types , including those not traditionally associated with brca1 / 2 cancer syndromes . 
biomarker development for parp inhibitors should integrate methods to distinguish biallelic from monoallelic brca1 / 2 status , and biallelic brca1 / 2 alteration should be broadly evaluated across cancer types as a biomarker for underlying hrd and parp inhibitor sensitivity . jco precis oncol 4 : 442 - 465 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction brca1 and brca2 encode critical components of the homologous recombination ( hr ) dna repair pathway that maintains genomic stability.1 germline brca1 / 2 ( gbrca1 / 2 ) alterations are associated with elevated risk for breast , ovarian , pancreatic , and prostate cancer ( brca1 / 2 - associated cancers ) , 2 , 3 and tumors that arise in brca1 / 2 mutation carriers have often lost the wild - type allele.4 synthetic lethal interactions between brca1 / 2 loss of function and poly ( adp - ribose ) polymerase inhibitors ( parpi ) underlie development and regulatory approval of parpi targeted therapy for ovarian , breast , and pancreatic cancer.1 , 5 companion diagnostic testing for gbrca1 / 2 and somatic brca1 / 2 ( sbrca1 / 2 ) alteration1 can guide parpi therapy selection . brca1 or brca2 loss - of - function results in hr deciency ( hrd ) and accumulation of chromosomal rearrangements and copy number alterations . 
 pan - cancer analysis of biallelic brca1 / 2 context key objective brca1 / 2 loss - of - function alterations result in homologous recombination deciency ( hrd ) and are biomarkers for poly ( adpribose ) polymerase ( parp ) inhibitor sensitivity in breast , ovarian , prostate , and pancreatic cancer . 
to determine the relevance of brca1 / 2 alterations across cancer types , we evaluated the pan - cancer landscape of brca1 / 2 alterations and their association with the genome - wide loss - of - heterozygosity ( gloh ) marker of hrd . knowledge generated the fraction of brca1 / 2 alterations that were biallelic differed by cancer type and predicted germline / somatic status . 
brca1 / 2 alterations were most frequently biallelic in breast , ovarian , prostate , and pancreatic cancer ; in other cancer types , 44% of brca1 / 2 alterations were biallelic . 
percent gloh was calculated as a signature of hrd as previously described.9 , 10 see the appendix for full methods . results to assess the prevalence of brca1 / 2 genomic alterations across cancer types , we examined cgp results from 234 , 154 tumors sequenced as part of routine clinical care . overall , brca1 / 2 alterations were observed in 4.7% of cases ( brca1 , 2.1% ; brca2 , 2.7% ; fig 1a ; appendix fig a1 )  . 
brca1 and brca2 alterations were most frequent in ovarian ( 10.5% ) and prostate cancer ( 9.6% ) , respectively ; unlike brca2 , brca1 alterations were infrequent in prostate cancer . brca1 / 2 homozygous deletions were infrequent except in prostate cancer , where brca2 deletions were observed at a 2.6% frequency and accounted for 25% of brca1 / 2altered cases . 
brca1 / 2 mutations were distributed throughout the length of each gene , and most were truncating events ( appendix fig a2 )  . germline / somatic status for brca1 / 2 short variant mutations was predicted using validated computational methods.18 we also evaluated performance of germline / somatic predictions in this study . 
fraction ( % ) of ( b ) brca1 or ( c ) brca2 mutations predicted to be germline v somatic was determined for each cancer type . see the data supplement for detailed data . computational methods correctly identied 21 ( 91% ) as predicted germline variants . 
second , because cell - free dna ( cfdna ) sequencing can often distinguish germline from somatic variants , 19 we evaluated 52 brca1 / 2 germline / somatic predictions from tissue samples and evaluated patientmatched cfdna ngs results . 
as expected , the majority of mutations were predicted to be germline in brca1 / 2 - associated cancers ( brca1 , 58.1% ; brca2 , 56.8% ) , but predicted sbrca1 / 2 mutations comprised an appreciable proportion of brca1 / 2 mutations . 
 ( a ) fraction of brca1 / 2 - altered cases with biallelic or monoallelic alteration was determined . brca1 / 2 - altered cases were evaluated for class of alteration identied and classied as biallelic ( multiple brca1 or multiple brca2 alterations in the same sample , homozygous deletion , biallelic short variant mutation [ loss of heterozygosity of the wild - type allele ] ) , monoallelic ( heterozygous mutation ) , or unknown ( zygosity status could not be determined )  . 
a lower - bound estimate was established by assessing biallelic cases as a fraction of all brca1 / 2 - altered cases , including those with unknown biallelic / monoallelic status ( see data supplement )  . 
for cases where biallelic / monoallelic status could be determined , we estimated the fraction of brca1 / 2 - altered cases with biallelic alteration ( biallelic fraction )  . 
although biallelic fraction was lower in nonbrca1 / 2 - associated cancers ( p , .0001 , fishers exact test ) , biallelic alterations nonetheless comprised 43.6% of brca1 / 2 - altered cases : biallelic fraction was  . 
1% frequency in at least 13 cancer types . in prostate cancer , predicted gbrca1 / 2 and sbrca1 / 2 mutations were separately assessed for biallelic fraction ( fig 3 ; appendix fig a5 )  . 
for brca1 / 2associated cancers , both predicted gbrca1 / 2 ( 90.8% ) and sbrca1 / 2 ( 81.2% ) mutations were frequently biallelic , whereas in nonbrca1 / 2 - associated cancers , fewer predicted gbrca1 / 2 ( 46.4% ) and sbrca1 / 2 ( 25.4% ) mutations were biallelic . 
in ovarian and breast cancer , the majority of brca1 and brca2 mutations were biallelic , both for predicted germline and the majority of somatic mutations . brca2 ( gbrca2 , 87.6% ; sbrca2 , 75.0% ) mutations were biallelic , but brca1 ( gbrca1 , 40.0% ; sbrca1 , 22.2% ) mutations were less frequently biallelic . 
cases with 16% gloh were classied as gloh - high on the basis of the cutoff established in the ariel3 trial of rucaparib in ovarian cancer.10 biallelic brca1 / 2 alterations were associated with gloh - high across every cancer type examined . 
the fraction of cases that were gloh - high was signicantly increased for biallelic brca1 / 2 - altered compared with wild - type cases ( fig 4a , appendix fig a6a ) , whereas the fraction of monoallelic brca1 / 2 cases that were gloh - high was similar to wild type . 
signicant association of biallelic but not monoallelic alterations with gloh - high was observed both for brca1 and for brca2 when assessed individually ( figs 4b and 4c )  . 
in some cancer types , significant but modest elevation in tumor mutational burden ( tmb ) was observed for biallelic brca1 / 2 - mutated cases ( predicted germline or somatic ) versus wild type ; however , the association with tmb was not consistent across cancer types ( appendix fig a7 )  . 
monoallelic sbrca1 / 2 - mutated ( but not gbrca1 / 2 ) cases were commonly associated with elevated tmb versus wild type , and such mutations may be a consequence of increased mutation rate . although biallelic brca1 / 2 status was consistently associated with gloh - high , the magnitude was variable for each cancer type , with the greatest association observed in pancreatic ( or , 22.5 ) , biliary ( or , 21.5 ) , endometrial ( or , 17.2 ) , unknown primary ( or , 16.1 ) , and ovarian ( or , 14.9 ) cancer ( fig 4a )  . 
more than 75% of cases with biallelic brca1 / 2 alterations were gloh - high for ovarian , breast , pancreatic , unknown primary , and endometrial cancer , whereas fewer than half were gloh - high for prostate and colorectal cancer . 
25% of brca1 / 2 wildtype cases were gloh - high for ovarian , breast , lung , and gastric / esophageal cancer . the 16% gloh - high cutoff was clinically validated in ovarian cancer9 , 10 and requires optimization for other cancer types . 
consistent with the ndings using a gloh cutoff - based approach , gloh scores were higher in brca1 / 2 biallelic versus wild - type cases across all cancer types evaluated ; increased gloh score was also observed when biallelic brca1 and brca2 were evaluated independently . hrd signatures ( including gloh - high ) may identify additional brca1 / 2 wild - type tumors potentially suitable for parpi.9 , 10 , 20 overall , 19.3% of cases were gloh - high compared with 3.2% of cases with biallelic brca1 / 2 alteration , and for most cancer types , the frequency of gloh - high was greater than biallelic brca1 / 2 alterations ( data supplement ) ; distribution of gloh scores varied between cancer types . 
to inform rational cancer typespecic gloh - high cutoffs , we assessed the performance of different gloh - high thresholds to classify biallelic brca1 / 2 compared with wild - type cases . 
plotting sensitivity to detect cases with biallelic brca1 / 2 alteration and specicity ( percentage of brca1 / 2 wild - type cases negative for the glohhigh biomarker ) , we identied a cutoff that maximized the combined sensitivity and specicity score ( fig 6 )  . 
the identied cutoff for ovarian cancer was 15.1% , which was consistent with the 14% and 16% cutoffs identied in clinical trials.9 , 10 discussion the development of parpi for brca1 / 2 altered ovarian , breast , and pancreatic cancer1 , 5 is predicated on synthetic lethality interactions between brca1 / 2 loss of function and parpi / trapping . 
emerging clinical trial data suggest that brca1 / 2 alteration may also be predictive of parpi response in prostate cancer.1 , 11 - 13 although responses to parpi have been documented in other cancer types , 14 , 21 - 23 the relevance of brca1 / 2 alterations in nonbrca1 / 2associated cancers remains unclear.4 to understand the landscape and phenotypic consequence of brca1 / 2 alterations , we assessed our data set of 234 , 154 cancer specimens sequenced using a clinicalgrade cgp assay . 
brca1 / 2 alterations were frequent in brca1 / 2 - associated cancers but also observed in a signicant fraction ( 3% ) of nonbrca1 / 2 - associated cancers . 
predicted germline mutations comprised the majority of brca1 / 2 mutations in brca1 / 2 - associated cancers ; however , it is notable that 43% were predicted somatic ( of which 81% were biallelic ) given data that support sbrca1 / 2 alteration as a biomarker for parpi in ovarian and prostate cancer.1 , 11 - 13 brca1 / 2 alterations were assessed for biallelic versus monoallelic status to distinguish likely loss of function from biologically neutral alterations . 
of note , although monoallelic alteration in brca1 / 2 mutation carriers may have a subtle haploinsufcient phenotype , 24 it does not lead to severe hrd or sensitivity to platinum - based chemotherapy.25 consistent with the established role of brca1 / 2 in the pathogenesis of brca1 / 2 - associated cancers , 90% of brca1 / 2 - altered cases were biallelic with high biallelic fraction both for predicted gbrca1 / 2 and sbrca1 / 2 . 
differences in brca1 and brca2 biallelic fraction were observed : brca2 was more frequently biallelic in prostate and small - cell lung cancer , and brca1 was more frequently biallelic in endometrial cancer , esophageal scc , colorectal cancer , and melanoma . 
the frequency of ( a ) brca1 / 2 , ( b ) brca1 , or ( c ) brca2 biallelic , monoallelic , and wild - type cases that were gloh - high was compared across cancer types . 
50 biallelic brca1 / 2 - altered samples were assessed individually , and all other cancer types were grouped together and analyzed as a single group ( other )  . 
association between brca1 / 2 biallelic alteration and genome - wide loss of heterozygosity ( gloh ) score as a continuous variable . gloh score was assessed in ( a ) brca1 / 2 , ( b ) brca1 , and ( c ) brca2 biallelic v wild - type cases across cancer types . 
boxes span the rst and third quartiles , and the median is denoted by the horizontal line in the box ; whiskers indicate maximum and minimum values within 1.5 the interquartile range ; black dots indicate outlier events . 
 100 sokol et al ovarian prostate breast endometrial pancreatic bladder / uc gastric / esophageal adenocarcinoma biliary tract colorectal nsclc % gloh sensitivity specificity % gloh % gloh fig 6 . 
 pan - cancer analysis of biallelic brca1 / 2 differences suggest that brca1 and brca2 may have tissue specicities outside breast and ovarian different cancer . to determine whether brca1 / 2 alterations lead to hrd in both brca1 / 2 - associated and nonbrca1 / 2 - associated cancers , we evaluated gloh in brca1 / 2 - altered versus type evaluated , wild - type cases . 
monoallelic alterations may be found in sporadic cancers from gbrca1 / 2 carriers or as somatic passenger mutations . distinguishing biallelic from monoallelic status may be an important consideration for rening brca1 / 2 alteration as a predictive biomarker for parpi . 
in brca1 / 2 - associated cancers , brca1 / 2 alteration status alone has proven sufcient as a predictive biomarker , 1 likely explained by the majority of brca1 / 2 alterations in this context being biallelic . 
nevertheless , parpi trials in prostate cancer have incorporated brca1 / 2 biallelic status into biomarker development , 13 and our nding of signicantly lower biallelic fraction for brca1 ( v brca2 ) in prostate cancer suggests that integrating biallelic status could rene predictive biomarkers in this setting . the lack of parpi clinical activity in nonbrca1 / 2 - associated cancers reported previously could be explained by grouped analysis of biallelic and monoallelic brca1 / 2 alterations.4 because of lower rates of biallelic alteration in nonbrca1 / 2 - associated cancers , parpi clinical trials will likely require patient selection strategies that incorporate methods to discriminate biallelic from monoallelic brca1 / 2 alterations . our ndings are consistent with a recent study that demonstrated an elevated hrd composite score in biallelic but not heterozygous brca1 / 2 cases relative to wild type in an aggregate set of nonbrca1 / 2 - associated cancers.4 a strength of the current study was that the large data set size enabled analysis of biallelic brca1 / 2 separately from monoallelic alterations , independent assessment of brca1 and brca2 , and evaluation of nonbrca1 / 2 - associated cancers as individual cancer types rather than in aggregate , which may have enabled identication of associations between biallelic brca1 / 2 alterations and an hrd signature across cancer types not previously described.4 if brca1 / 2 biallelic alterations functionally result in hrd , they should represent a targetable vulnerability to parpi and platinum - based chemotherapy , irrespective of whether they are drivers of disease pathogenesis or bystander passenger alterations.26 our data demonstrate that biallelic brca1 / 2 alteration in nonbrca1 / 2 - associated cancers are associated with the gloh - high signature of hrd and , therefore , warrant investigation in parpi trials . 
although biallelic brca1 / 2 alterations occur at low prevalence in nonbrca1 / 2 - associated cancers , basket trials that led to the tumor - agnostic approvals of ntrk inhibitors for ntrk fusion - positive tumors and pembrolizumab for microsatellite instabilityhigh tumors27 demonstrate feasibility of therapeutic development for rare pan - cancer biomarkers . 
clinical trials such as the tapur study ( clinicaltrials.gov identier : nct02693535 ) that treatment arm for brca1 / 2 - altered includes a parpi cancers will inform parpi development in nonbrca1 / 2associated cancers , and analyses may benet from consideration of monoallelic versus biallelic status . although gloh - high is associated with clinical benet from rucaparib in ovarian cancer , 9 , 10 understanding of the gloh biomarker in other cancer types is required . 
evaluation of sensitivity and specicity of varying gloh thresholds to distinguish biallelic brca1 / 2 - altered and wild - type cases may inform development of disease - specic gloh - high cutoffs . 
in future studies , analysis of brca1 / 2 wild - type , gloh - high cases may be a discovery tool for characterizing brca1 / 2 vuss and for prioritizing candidate non - brca1 / 2 hr pathway gene biomarkers.9 although detection of gloh - high in brca1 / 2 wild - type cases potentially expands the patient population addressable by parpi , the utility of gloh - high requires validation in prospective trials for nonovarian cancers . limitations of this study should be acknowledged . 
first , we focus on gloh as a biomarker for hrd ; other hrd markers were not evaluated , including telomeric allelic imbalance ( tai ) , large - scale transition ( lst ) , mychoice hrd ( combination loh / tai / lst score ; myriad genetics , salt lake city , ut ) , signature 3 , and hrdetect.7 , 8 , 28 - 33 in parpi trials , hrd biomarkers have focused on approaches that are compatible with targeted ngs assays ( gloh , mychoice hrd ) , which are used in routine clinical practice.1 , 9 , 10 in contrast , signature 3 and hrdetect signatures have been evaluated in the research setting using whole - exome or whole - genome sequencing ; novel methods may enable future clinical assessment of signature 3 with targeted assays.34 second , germline / somatic status predictions using tumor - only sequencing and computational methods are less denitive compared with matched normal sequencing used in other studies.4 , 18 third , using brca1 / 2 biallelic versus wild - type status to rene gloh - high cutoffs is confounded by some brca1 / 2 wild - type gloh - high cases that are hrd because of brca1 / 2 alteration independent mechanisms , such as brca1 / 2 methylation or alteration in other hr genes . 
 sokol et al in the future ; however , we focused on brca1 / 2 because other hr pathway genes have not been consistently predictive of clinical response to parpi , 11 - 13 , 36 and robust clinical evidence supporting predictive biomarker genes beyond brca1 / 2 is lacking . 
finally , clinical outcomes data that associate parpi response with biallelic brca1 / 2 alteration and gloh were not available and require evaluation in clinical trials . we demonstrate that biallelic brca1 / 2 alterations are associated with elevated gloh across all cancer types evaluated and may therefore represent a therapeutic vulnerability targetable by parpi . 
ali , shridar ganesan , jon h . chung financial support : brian alexander administrative support : brian alexander provision of study material or patients : hossein khiabanian , primo n . 
gregg consulting or advisory role : astrazeneca , bristol - myers squibb , roche , foundation medicine , luminex speakers bureau : astrazeneca , foundation medicine , bristol - myers squibb primo n . 
 pan - cancer analysis of biallelic brca1 / 2 research funding : merck sharp & dohme ( inst ) , astrazeneca ( inst ) , ipsen ( inst ) travel , accommodations , expenses : roche , merck sharp & dohme , astrazeneca , janssen pharmaceuticals , rainier therapeutics other relationship : bayer ag ( i ) vincent a . 
miller employment : foundation medicine leadership : foundation medicine , revolution medicines stock and other ownership interests : foundation medicine , mirati therapeutics , revolution medicines patents , royalties , other intellectual property : periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center brian alexander employment : foundation medicine leadership : foundation medicine stock and other ownership interests : roche research funding : eli lilly ( inst ) , puma ( inst ) , celgene ( inst ) open payments link : 854258 / summary siraj m . 
ali employment : foundation medicine , eqrx , eqrx ( i ) leadership : incysus stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences consulting or advisory role : revolution medicines , azitra ( i ) , princepx tx ( i ) patents , royalties , other intellectual property : patents through foundation medicine , patents through seres health on microbiome stuff in nonneoplastic disease ( i ) shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis , roche , foghorn therapeutics , foundation medicine , merck sharp & dohme patents , royalties , other intellectual property : two patents for digital imaging that may be licensed to ibris and inspirata travel , accommodations , expenses : inspirata other relationship : national cancer institute / national institutes of health jon h . 
chung employment : foundation medicine stock and other ownership interests : foundation medicine no other potential conicts of interest were reported . references 105 : 812 - 822 , 2013 1 . 
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j natl cancer inst 110 : 704 - 713 , 2018 swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
coleman rl , oza am , lorusso d , et al : rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
abida w , bryce ah , vogelzang nj , et al : preliminary results from triton2 : a phase ii study of rucaparib in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) associated with homologous recombination repair ( hrr ) gene alterations . 
smith mr , sandhu sk , kelly wk , et al : phase ii study of niraparib in patients with metastatic castration - resistant prostate cancer ( mcrpc ) and biallelic dnarepair gene defects ( drd ) : preliminary results of galahad . 
sandhu sk , schelman wr , wilding g , et al : the poly ( adp - ribose ) polymerase inhibitor niraparib ( mk4827 ) in brca mutation carriers and patients with sporadic cancer : a phase 1 dose - escalation trial . 
slavin tp , banks kc , chudova d , et al : identication of incidental germline mutations in patients with advanced solid tumors who underwent cell - free circulating tumor dna sequencing . 
moore kn , secord aa , geller ma , et al : niraparib monotherapy for late - line treatment of ovarian cancer ( quadra ) : a multicentre , open - label , single - arm , 21 . 
necchi a , raggi d , giannatempo p , et al : exceptional response to olaparib in brca2 - altered urothelial carcinoma after pd - l1 inhibitor and chemotherapy 22 . 
hierro c , matos i , martin - liberal j , et al : agnostic - histology approval of new drugs in oncology : are we already there ? clin cancer res 25 : 3210 - 3219 , 2019 28 . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deciency among breast cancer 31 . 
telli ml , timms km , reid j , et al : homologous recombination deciency ( hrd ) score predicts response to platinum - containing neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
marshall ch , sokolova ao , mcnatty al , et al : differential response to olaparib treatment among men with metastatic castration - resistant prostate cancer harboring brca1 or brca2 versus atm mutations . 
 pan - cancer analysis of biallelic brca1 / 2 appendix supplementary methods approval for this study , including a waiver of informed consent and health insurance portability and accountability act waiver of authorization , was obtained from the western institutional review board ( irb ; protocol #20152817 )  . 
cgp results included in this study were from tumor tissue specimens ( n = 234 , 154 ) submitted as part of routine clinical care ( december 2013 - march 2019 ) ; for patient characteristics , see the data supplement . 
in validation testing of 480 tumor - only sequencing calls against matched normal specimens , accuracy was 95% for somatic and 99% for germline calls ( sun jx , et al : plos comput biol 14 : e1005965 , 2018 ) ; in assessment of zygosity calls , signicant enrichment in mutations with loss of heterozygosity ( loh ) was observed for tumor suppressor genes ( sun jx , et al : plos comput biol 14 : e1005965 , 2018 )  . 
to evaluate performance of germline / somatic computational predictions in this series , we compared predictions against a subset of cases with available results from patient - matched germline testing or cell - free dna ( cfdna ) ngs that were performed as previously described ( clark ta , et al : j mol diagnostics 20 : 686 - 702 , 2018 ; khiabanian h , et al : jco precis oncol 2 : 1 - 15 , 2018 ) ; brca1 / 2 genetic testing on a subset of patients at the rutgers cancer institute of new jersey were analyzed under the auspices of an irb - approved protocol . 
germline - like af was dened as mutations observed in cfdna at 40% - 60% af ( except for cfdna samples with high circulating tumor dna fraction [  . 20% ] that were excluded from the analysis as ambiguous )  . 
brca1 / 2 alterations were categorized as biallelic , monoallelic , or unknown . biallelic alterations were mutations with loh of the wild - type allele , as determined by zygosity status ( sun jx , et al : plos comput biol 14 : e1005965 , 2018 ) ; homozygous deletion ; or 2 brca1 or 2 brca2 alterations in a sample . 
percent genome - wide loh ( gloh ) was calculated as a signature of hrd as previously described ( coleman rl , et al : lancet 390 : 1949 - 1961 , 2017 ; swisher em , et al : lancet oncol 18 : 75 - 87 , 2017 )  . 
this prole was segmented and interpreted using afs of sequenced snps to estimate copy number ( ci ) and minor allele count ( mi ) at each segment ( i )  . 
two types of loh segments were excluded from the calculation of percent gloh : loh segments that spanned 90% of a whole chromosome or chromosome arm because these loh events usually arise through non - hrd mechanisms ( eg , mitotic nondisjunction ) and regions in which loh inference was ambiguous . 
for each tumor , the percent gloh was computed as 100 the total length of nonexcluded loh regions ( xi ) divided by the total length of nonexcluded regions of the genome . 
 sokol et al brca1 / 2 short variant homozygous deletion rearrangement multiple brca1 brca2 short variant homozygous deletion rearrangement multiple brca1 brca2 breast cancer ovarian cancer breast cancer ovarian cancer fig a1 . 
growth factor receptor 2 ( her2 ) status was determined on the basis of the presence or absence of a copy number amplication ; triple - negative breast cancer ( tnbc ) was dened as er - negative , her2 - negative samples . 
 somatic af germline af cfdna germline af cfdna somatic af 5 10 15 20 25 30 35 40 45 50 55 60 65 70 75 80 85 90 95 brca1 / 2 variant allele frequency ( % ) predicted germline ( n = 22 ) predicted somatic ( n = 30 ) cfdna gbrca sbrca predicted germline predicted somatic sokol et al predicted germline predicted somatic breast cancer ovarian cancer fig a3 . 
 ( a and b ) comparison of tissue - based germline / somatic predictions to brca1 / 2 allele frequencies ( afs ) in patient - matched cell - free dna ( cfdna )  . 
mutations with germline af were dened as those identied in cfdna at 40% - 60% af , except for cases with high circulating tumor dna fraction ( 20% ) that were excluded from the analysis as ambiguous af . 
 ( c - e ) predicted germline / somatic status calls were made for each brca1 or brca2 short variant mutation . for mutations yielding a successful call , frequency of predicted germline v somatic mutation was determined for ( c ) brca1 / 2 across cancer types , ( d ) brca1 / 2 ( grouped and individually ) overall ( n = 5 , 845 ) for brca1 / 2 - associated cancers ( breast , ovarian , pancreatic , prostate ; n = 3 , 061 ) and nonbrca1 / 2 - associated cancers ( n = 2 , 784 ) , and ( e ) brca1 / 2 for the subset of ovarian and breast cancer cases where molecular / histologic subtype information was available . 
relative fraction of brca1 / 2 - altered cases with biallelic or monoallelic alteration was determined for ( a ) brca1 across cancer types and ( b ) brca2 across cancer types . 
 ( c ) brca1 / 2 ; ( d ) brca1 ; ( e ) brca2 for overall , brca1 / 2 - associated cancers , and nonbrca1 / 2 - associated cancers ; and ( f ) brca1 / 2 for the subset of ovarian and breast cancer cases where molecular / histologic subtype information was available . 
 ( a ) brca1 / 2 mutations ( grouped ) with a germline ( gbrca1 / 2 ) or somatic ( sbrca1 / 2 ) prediction were evaluated for biallelic / monoallelic status for all cancers , brca1 / 2 - associated cancers ( as a group and as individual cancer types ) , and nonbrca1 / 2 - associated cancers ( see data supplement )  . 
cases with somatic brca1 / 2 ( sbrca1 / 2 ) or germline brca1 / 2 ( gbrca1 / 2 ) biallelic mutation , monoallelic mutation , or wild - type ( wt ) brca1 / 2 were plotted against tumor mutational burden ( tmb in mutations / mb ; log10 score )  . 
box and whisker plot where the box spans the rst and third quartiles , the median is denoted by the horizontal line in the box , and whiskers indicate maximum and minimum values within 1.5 the interquartile range ( see data supplement )  . 
 ( a ) the frequency of brca1 / 2 biallelic , monoallelic , and wild - type cases that were high genome - wide loss of heterozygosity ( gloh - high ) was compared in the subset of ovarian and breast cancer cases where molecular / histologic subtype information was available ( see data supplement )  . 
 ( b ) frequency of predicted germline brca1 / 2 ( gbrca1 / 2 ) biallelic , monoallelic , and wild - type cases that were gloh - high ( see data supplement )  . 
 ( c ) frequency of predicted somatic brca1 / 2 ( sbrca1 / 2 ) biallelic , monoallelic , and wild - type cases that were gloh - high ( see data supplement )  . 
egfr tyrosine kinase inhibitors ( tkis ) markedly increase progression - free survival in advanced disease.17 , 18 this discovery opened a new era of precision medicine leading to accelerated development and subsequent approval of drugs for several actionable genomic alterations in nsclc . 
while the molecular proling of nsclc is considered a standard of care in the advanced setting , the utility of molecular testing and targeted therapies in the adjuvant setting in early - stage nsclc has yet to be established . 
the br19 trial compared getinib versus placebo in a similar population.21 the trial closed prematurely after results of another trial showed detrimental effect of getinib after chemoradiation in stage iii nsclc.23 however , egfrmutant nsclc accounted for only 4% ( n = 15 ) of the patients . 
patients with resected stage ib - iiia ( american joint committee on cancer [ ajcc ] 7th edition ) adenocarcinoma with sensitizing egfr mutation were randomly assigned 1 : 1 to adjuvant osimertinib at the standard dose of 80 mg / d or matching placebo . 
random assignment was stratied by stage ( ib v ii v iiia ) , type of egfr mutation ( exon 19 del v l858r ) , and race ( asian v non - asian ) , but not based on receipt of adjuvant chemotherapy . 
patients received assigned treatment for a planned 3 - year duration or until disease recurrence , completion they met predetermined criteria for discontinuation . treatment , or if six - hundred eighty - two patients were randomly assigned to osimertinib ( n = 339 ) or placebo ( n = 343 )  . 
the published data are an unplanned interim analysis with the dfs data being only 33% mature ( 11% in osimertinib and 55% in placebo ) at the data cutoff date of january 17 , 2020 . 
similarly , dfs in the overall population ( including stage ib ) was also signicantly longer with a consistent benet seen across all predened subgroups ( age , smoking , race , stage , and type of egfr mutation )  . 
first , positron emission tomography - computed tomography ( pet - ct ) scan and brain mri were not mandated at screening in the study protocol.27 in the united states , pet - ct scan and brain mri are considered the standard of care for the complete staging of early - stage nsclc.28 data on proportion of patients with complete staging information ( pet - ct and brain mri ) in either arm are not available . 
in the adura trial , the median dfs and 2 - year dfs rate in the placebo arm are signicantly lower than those reported in historical trials , suggesting that suboptimal staging at baseline could have contributed to higher proportion of patients being understaged.29 , 30 compared to control arm , osimertinib showed an 82% reduction in risk for cns recurrence or death . 
however , this should be interpreted with caution , given limited follow - up and patients with occult intracranial metastatic disease missed on brain ct scans who get osimertinib are at an advantage because of potent cns activity . 
data regarding the recurrence rates adjusted by country or region of enrollment may be important as petct and brain mri are not readily available worldwide in resource - limited settings . second , about 40% of the patients did not get adjuvant chemotherapy . 
to accurately assess the benet of adjuvant osimertinib , adjuvant chemotherapy should have been offered to all patients in the control arm and not just left to the discretion of the attending physician . 
 commentary enrollment , port was considered a valid treatment option for resected stage iiia n2 disease . in retrospect , not allowing port and not mandating standard of care adjuvant chemotherapy with proven os benet among participants in the placebo arm may be more of an ethical consideration for patients and investigators rather than a confounding variable . 
in the adjuvant setting , in an asymptomatic context , daily treatment with osimertinib for up to 3 years can lead to considerable toxicity , especially if we consider that some patients have been already cured with surgery with or without adjuvant chemotherapy . in addition to some of the limitations mentioned above , several important aspects related to study outcomes remain to be dened . 
in the adjuvant setting , it is not known whether the 2 - year dfs superiority with egfr directed therapy will translate into an os benet with osimertinib . data from adjuvant / ctong 1104 trial suggest that the substantial dfs benet did not translate into os , a goldstandard measure of patient impact in the adjuvant setting . although pfs may be a reasonable surrogate for os in the metastatic setting , higher level of evidence is needed before advocating for dfs as a proxy for os benet in patients receiving adjuvant cancer therapies . 
unlike adaura , the alchemist trial is testing adjuvant egfrand alkdirected therapy using os as the primary end point . furthermore , it has been suggested that targeted therapies as cytostatic agents suppress micrometastatic disease progression , thereby delaying recurrence but not eliminating the disease completely . 
despite multiple studies across solid tumors , to our knowledge , imatinib is the only tki that has shown improved os when given in the adjuvant setting of high - risk gi stromal malignancies , 31 a disease with completely different molecular background compared with lung adenocarcinomas . 
of note , in the osimertinib arm of the adaura trial , about 15% of the patients who stopped the drug at 3 years experienced dfs event in the 6 - 9 months after drug discontinuation . 
this might suggest that recurrence - free survival is directly related to the length of drug exposure , and therefore adjuvant osimertinib might only delay recurrence and not cure the disease . 
in adaura , at the data cutoff , approximately 46% of patients in the placebo arm experienced disease reto know the post - protocol currence . treatment patterns , specically the proportion of patients in the placebo arm who received osimertinib at progression . if this percentage is lower than expected , then the dfs benet seen in adaura might only reect the suboptimal treatment of control arm upon progression . 
if similar it will be critical os can be achieved in the placebo arm with osimertinib treatment on recurrence , one can speculate that osimertinib has minimal effect on the natural history of the disease and is only delaying the inevitable relapsed disease . 
one can anticipate that having a nonngsbased molecular testing at the time of initial detection of the egfr mutation will make it hard to tease out the acquired , potentially actionable mechanisms of resistance at the dfs event . 
furthermore , development of acquired resistance mechanisms at relapse on osimertinib in the adjuvant setting could result in these patients missing the window of opportunity to receive osimertinib in the metastatic setting . robust biomarkers to predict durable clinical benet to adjuvant therapy are lacking . 
thus , it might not be as cost - effective to justify the use of osimertinib in the absence of an os benet , an issue that is contentious but is an important consideration from a societal healthcare perspective . 
furthermore , a proportion of patients who are probably cured of lung cancer with surgery alone may have unnecessary exposure to osimertinib and its toxicities with added hospitalizations . lowand middle - income countries might be affected the most because of lack of access to testing and drugs , as well as prohibitive costs . 
assessment of the quality of life ( qol ) while on therapy and beyond will also be a crucial parameter to consider the overall benet of treatment . in conclusion , os is the most important and clinically meaningful end point in the adjuvant setting . 
given the lack of evidence to demonstrate dfs as a validated surrogate end point with targeted therapy in the adjuvant setting , mature os data are recommended before a denitive statement on adjuvant osimertinib in egfr - mutant nsclc . we also worry that wide adoption of adura in the community might lead to lower use of adjuvant chemotherapy in favor of osimertinib . 
with the idmc decision to unblind and terminate the study early based on the perceived dfs benet , we might never know whether adjuvant osimertinib leads to a superior os versus treatment with osimertinib upon rst evidence of relapse . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . sonam puri consulting or advisory role : astrazeneca rodrigo dienstmann consulting or advisory role : roche , boehringer ingelheim speakers bureau : roche , ipsen , sano , msd oncology , servier , amgen research funding : merck no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2020 . 
ca cancer j clin 70 : 7 - 30 , 2020 besse b , le chevalier t : developments in the treatment of early nsclc : when to use chemotherapy . 
ann thorac surg 83 : 409 - 418 , 2007 pignon jp , tribodet h , scagliotti gv , et al : lung adjuvant cisplatin evaluation : a pooled analysis by the lace collaborative group . 
j clin oncol 26 : 3552 - 3559 , 2008 kris mg , gaspar le , chaft je , et al : adjuvant systemic therapy and adjuvant radiation therapy for stage i to iiia completely resected non - small - cell lung cancers : american society of clinical oncology / cancer care ontario clinical practice guideline update . 
j clin oncol 35 : 2960 - 2974 , 2017 arriagada r , auperin a , burdett s , et al : adjuvant chemotherapy , with or without postoperative radiotherapy , in operable non - small - cell lung cancer : two metaanalyses of individual patient data . 
lancet 375 : 1267 - 1277 , 2010 strauss gm , herndon je , maddaus ma , et al : adjuvant paclitaxel plus carboplatin compared with observation in stage ib non - small - cell lung cancer : calgb 9633 with the cancer and leukemia group b , radiation therapy oncology group , and north central cancer treatment group study groups . 
j clin oncol 26 : 5043 - 5051 , 2008 burdett s , rydzewska l , tierney jf , et al : a closer look at the effects of postoperative radiotherapy by stage and nodal status : updated results of an individual participant data meta - analysis in non - small - cell lung cancer . 
lung cancer 80 : 350 - 352 , 2013 burdett s , stewart l : postoperative radiotherapy in non - small - cell lung cancer : update of an individual patient data meta - analysis . 
robinson cg , patel ap , bradley jd , et al : postoperative radiotherapy for pathologic n2 non - small - cell lung cancer treated with adjuvant chemotherapy : a review of the national cancer data base . 
mikell jl , gillespie tw , hall wa , et al : postoperative radiotherapy is associated with better survival in non - small cell lung cancer with involved n2 lymph nodes : results of an analysis of the national cancer data base . 
corso cd , rutter ce , wilson ld , et al : re - evaluation of the role of postoperative radiotherapy and the impact of radiation dose for non - small - cell lung cancer using the national cancer database . 
fukuoka m , wu yl , thongprasert s , et al : biomarker analyses and nal overall survival results from a phase iii , randomized , open - label , rst - line study of getinib versus carboplatin / paclitaxel in clinically selected patients with advanced non - small - cell lung cancer in asia ( ipass ) , j clin oncol 29 : 2866 - 2874 , 2011 inoue a , kobayashi k , maemondo m , et al : updated overall survival results from a randomized phase iii trial comparing getinib with carboplatin - paclitaxel for chemo - nave non - small cell lung cancer with sensitive egfr gene mutations ( nej002 )  . 
zhong wz , wang q , mao wm , et al : getinib versus vinorelbine plus cisplatin as adjuvant treatment for stage ii - iiia ( n1 - n2 ) egfr - mutant nsclc ( adjuvant / ctong1104 ) : a randomised , open - label , phase 3 study . 
kelly k , altorki nk , eberhardt wee , et al : adjuvant erlotinib versus placebo in patients with stage ib - iiia nonsmall - cell lung cancer ( radiant ) : a randomized , double - blind , phase iii trial . 
wu yl , zhong w , wang q , et al : ctong1104 : adjuvant getinib versus chemotherapy for resected n1 - n2 nsclc with egfr mutationnal overall survival analysis of the randomized phase iii trial 1 analysis of the randomized phase iii trial . 
douillard jy , rosell r , de lena m , et al : adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ib - iiia non - small - cell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
arriagada r , de radiomedic - ina i , santiago c , et al : cisplatin - based adjuvant chemotherapy in patients with completely resected nonsmall - cell lung cancer . n engl j med 350 : 351 - 360 , 2004 joensuu h , eriksson m , sundby hall k , et al : survival outcomes associated with 3 years vs 1 year of adjuvant imatinib for patients with high - risk gastrointestinal stromal tumors : an analysis of a randomized clinical trial after 10 - year follow - up . 
abbosh c , frankell a , garnett a , et al : phylogenetic tracking and minimal residual disease detection using ctdna in early - stage nsclc : a lung tracerx study . cancer res 80 , 2020 ( suppl ; abstr ct023 ) 36 . 
li n , ou w , ye x , et al : pemetrexed - carboplatin adjuvant chemotherapy with or without getinib in resected stage iiia - n2 non - small cell lung cancer harbouring egfr mutations : a randomized , phase ii study . 
zhong wz , chen kn , chen c , et al : erlotinib versus gemcitabine plus cisplatin as neoadjuvant treatment of stage iiia - n2 egfr - mutant non - small - cell lung cancer ( emerging - ctong 1103 ) : a randomized phase ii study . 
pennell na , neal jw , chaft je , et al : select : a phase ii trial of adjuvant erlotinib in patients with resected epidermal growth factor receptor - mutant non - smallcell lung cancer . 
precursors and carcinomas were immunohistochemically compared and analyzed for mutations , gene amplications , microsatellite instability , and tumor mutational burden using an next - generation sequencing panel containing 523 cancer - related genes . 
in addition , presence of fusion genes was analyzed using a panel of 55 genes . results sixty percent of neuroendocrine cases ( 6 / 10 ) presented with a precursor lesion , either intracholecystic papillary neoplasm ( n = 3 ) or biliary intraepithelial neoplasia ( n = 3 )  . 
moreover , nearly half of the ne gbcs carried at least one potentially actionable molecular alteration , highlighting the importance of molecular testing in this highly lethal cancer . jco precis oncol 5 : 473 - 484 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction neuroendocrine neoplasms ( nens ) can arise from almost any anatomical site including , but not limited to , the lung , the prostate , and throughout the gi and hepatobiliary tract . 
two major categories of nens have been described : well - differentiated neuroendocrine tumors ( nets ) and poorly differentiated neuroendocrine carcinomas ( necs ) , the latter being high grade by denition.1 morphologically , necs are classied as either pure small - cell or large - cell nec , and they might also be present together with an adenocarcinoma ( ac ) component . 
they nonneuroendocrine neoplasms ( minens ) when both the neuroendocrine component ( generally nec ) and the non - neuroendocrine component ( generally ac ) comprise at least 30% of the neoplasm.2 regardless of the anatomical site , necs and minens are highly aggressive tumors and carry a dismal prognosis . neuroendocrine as mixed classied necs can either arise de novo or during progression of an epithelial neoplasm , for example , because of a therapy resistance mechanism.3 the molecular features of necs have been best described in lung , pancreas , and prostate , but the cell of origin of necs has been a matter of controversy , specically in tumors with a mixed phenotype ( ie , minens )  . 
this study was approved by the radboud university medical center medical ethics committee ( 2018 - 4126 )  . histopathologic review formalin - xed parafn - embedded ( ffpe ) blocks were selected on the basis of pathology reports and histopathologic review . 
histologic typing and grading , including description of a precursor lesion ( either bilin or icpn ) , was performed using the who histologic classication of tumors of the gallbladder ( fth edition ) .2 t classication was performed using the american joint committee on cancer tumor - node - metastasis classication system ( eighth edition ) .12 additionally , presence of vascular , lymphatic , and perineural invasion was assessed . immunohistochemistry immunohistochemistry ( ihc ) was performed on 4 - mm whole - slide ffpe sections semiautomated using the lab vision autostainer ( immunologic , duiven , the netherlands ) for muc2 , muc5ac , muc6 , and ttf - 1 essentially as described before13 or fully automated using tissue - tek genie ( sakura finetek , torrance , ca ) for chromogranin a , cd56 , ck7 , ck20 , ki - 67 , ema ( muc1 ) , p53 , and synaptophysin with ready - to - use reagents . 
discrepancies in scoring were reevaluated until agreement . nucleic acid extraction for molecular analyses , dna and rna were isolated from ffpe - derived tumor tissue and the precancerous lesion if available . 
dna was isolated , quantied , and precipitated manually as described before.14 after precipitation , the nal concentration was determined using the qubit high sensitivity kit ( thermo fisher scientic , waltham , ma )  . rna was isolated using the reliaprep ffpe total rna miniprep system ( promega , madison , wi ) according to the manufacturers protocol , omitting the dnase treatment step . 
 histologic and molecular features of ne gallbladder cancer subsequently , 60 ng of either dna or rna was used as input for the library preparation . library preparation dna and rna library preparations were performed separately using the hybrid capture - based trusight oncology ( tso ) 500 dna and rna library preparation kits , respectively ( illumina , san diego , ca ) according to the manufacturers protocol essentially as described before.15 the tso500 dna assay targets 523 cancer - related genes for assessment of singleand multiple - nucleotide variants , gene amplications , tumor mutational burden ( tmb ) , and microsatellite instability ( msi ) , whereas the rna kit targets 55 genes for fusion gene analyses ( data supplement )  . 
in short , dna samples were fragmented , and rna samples were used for rstand second - strand cdna synthesis . next , samples underwent end - repair and a - tailing , followed by unique molecular identier ligation and barcoding . two target capture and purication steps , allowing for maximal target enrichment , were followed by polymerase chain reaction amplication and purication . 
libraries were quantied and normalized for uniform library representation . sequencing and data analysis sequencing was performed on a nextseq 500 system ( illumina ) , with 10 dna libraries on a nextseq high - output cassette or 16 rna libraries on a nextseq mid - output cassette . 
the number of gene copies in the tumor cells was estimated on the basis of the relative coverage corrected for the percentage of neoplastic cells in the sample . variant annotation was performed as described before via an in - housedeveloped pipeline.17 variants were ltered by exclusion of ( 1 ) variants outside exons and splice site regions ( 8 / + 8 ) except those in the tert promoter region , ( 2 ) synonymous variants , unless present in a splice site region , ( 3 ) variants present with a frequency of  . 
0.1% in the exac ( version 0.2 ) database , ( 4 ) variants with a variant allele frequency ( vaf ) of , 5% , and ( 5 ) variants with , 5 variant reads . 
remaining variants were manually inspected and curated and classied into ve classes on the basis of their level of evidence for pathogenicity , largely on the basis of american college of medical genetics / association for molecular pathology guidelines18 , 19 : class 1 , not pathogenic ; class 2 , unlikely pathogenic ; class 3 , possibly pathogenic ; class 4 , likely pathogenic ; and class 5 , pathogenic . 
potential effects on splicing were evaluated on the basis of the majority vote of splicesitefinder - like , maxentscan , nnsplice , and genesplicer ( all available from alamut visual version 2.13 [ sophia genetics , lausanne , switzerland ] )  . 
details on classes and their interpretation are provided in figure a1 , online only . variant - specic level 1 , 2 , 3 , or 4 evidence for actionability across all tumor types was derived from oncokb.21 level 1 and 2 biomarkers are dened as fda - recognized or standard care biomarkers , respectively , that are predictive of response to fda - approved drugs in specic tumor types . for level 3a biomarkers , there is compelling clinical evidence of drug response in a specic indication , and level 3b alterations are predictive of response to an fdaapproved or investigational drug in another indication . level 4 alterations comprise alterations for which there is compelling biological evidence that predicts response to a drug . 
seven cases ( 70% ) were pure high - grade net or nec , whereas three tumors ( 30% ) showed both ac and nec features and were classied as minens . 
data on type of systemic therapy are not available . tumors ( 50% ) were large - cell nec , four cases ( 40% ) were small - cell nec , and one case ( 10% ) was a net grade 3 , hereafter collectively referred to as ne gbc . 
in 90% of cases , at least one tumor component ( either nec or , if present , ac ) showed angioinvasion ; lymphatic invasion and perineural invasion were observed in 80% and 30% of cases , respectively . neuroendocrine expression with synaptophysin , chromogranin a , and cd56 conrmed neuroendocrine histology and was absent in the precancerous lesions ( table 2 and fig 1 )  . 
tumor characteristics case diagnosis ptnm ( m location ) icpn ( mixed type ) with nec ( sc ) t2anx bilin with nec ( sc ) t3nx nec ( sc ) t3n2m1 ( liver ) icpn ( intestinal type ) with nec ( lc ) t3n1 icpn ( biliary type ) with minen ( lc ) t2an1 bilin with minen t3nx ( lc ) nec ( lc ) nec ( lc ) t2nx t3nxm1 ( peritoneum ) 476 2021 by american society of clinical oncology abbreviations : + ,  . 
neuroendocrine marker expression with synaptophysin was positive in the nec and negative in the icpn and ac ( chromogranin a and cd56 were comparable ; table 2 ) , whereas epithelial marker expression ( ck 7 ) was positive in the icpn and ac and negative in the nec ( ck20 - negative in all three ; table 2 )  . 
since tp53 is frequently altered in necs of other anatomical origin , case 5 served as an exemplary case for which p53 ihc was performed next to a molecular screening , which was done for all cases . 
both the ac and nec components showed aberrant p53 expression , whereas the icpn component showed predominantly a normal p53 expression with only a small region with overexpression ( fig 1 )  . 
 de bitter et al molecular characteristics discussion for each case , dna and rna were isolated from the precursor lesion , the nec component and , if available , the ac component . 
quality control parameters of dna and rna libraries including reference values are listed in the data supplement . for case 1 , both the nec and icpn components did not meet quality control for msi , tmb , and cnv assessment . all likely pathogenic and pathogenic singleand multiplenucleotide variants ( classes 4 and 5 ) were considered potentially clinically relevant and are listed in figure 2 and the data supplement . 
a variety of other genes harbored potentially clinically relevant mutations in individual cases . mutations in tp53 were shared among the different precursor , ac , and nec components in all but one case ( case 8 ) , where two different mutations were observed in the ac versus the nec . 
interestingly , the icpn of case 5 did share the same tp53 mutation with the invasive tumor components , albeit with a low vaf ( 8.7% ) , reecting the limited region with p53 overexpression ( fig 1 )  . 
three cases ( 30% ) harbored potentially actionable variants ( level 1 ) in atm , brca2 , and rad54l , albeit with a low vaf for the atm variant of case 4 . in six cases , gene amplications were observed in a variety of genes including potentially actionable amplications of erbb2 ( level 1 ) and mdm2 ( level 3a ) , the latter being in a case without a tp53 mutation ( fig 2 )  . 
whereas the majority of mutations were shared among different precancerous , ac , and nec components , for gene amplications this was for a cnne1 amplication that not observed , except was shared between the ac and nec , but not the icpn , of case 5 . a fusion involving fgfr3 and tacc3 genes was observed in all three components of case 5 ( fig 2 )  . 
despite these phenotypical differences , the shared tp53 mutation in the different components in ve of six cases strongly suggests a common origin for neuroendocrine and epithelial components of ne gbc . 
in addition , 50% of the cases also had cholelithiasis , which is a well - known risk factor for pure gallbladder ac , 26 and may further reinforce the concept of a common origother studies of digestive system necs also support the lineage transformation hypothesis with molecular analyses.5 , 27 , 28 nearly all cases had multiple pathogenic or likely pathogenic mutations in a variety of genes with tp53 , ctnnb1 , rb1 , and atm being the most frequently involved . 
our ndings are largely in line with observations in lung , prostate , and pancreatic necs , where tp53 and rb1 are altered in roughly 80% of cases.3 interestingly , also pure gallbladder ac is molecularly highly heterogeneous with tp53 as the most frequently mutated gene ( 47.1% - 59% of cases ) .29 however , large - scale molecular data remain scarce and are mainly derived from endemic regions , which could hamper the extrapolation of ndings to nonendemic regions . gene amplications ( n = 6 cases ) were observed in a subset of cases and were in all but one case not shared between the different components . 
this suggests that , in contrast to mutations that are shared between the precursor and invasive components , oncogenic amplications typically occur as a later event in carcinogenesis , which has been observed before in esophageal ac.30 in case 5 , a ccne1 amplication was shared between the ac and nec , but not the icpn . 
potentially clinically relevant mutations ( class 4 and class 5 ) , gene amplications , fusion genes , microsatellite status , and total tumor mutational burden , identied by tso500 . 
another limitation of this study is the limited information on used therapeutic regimens , such as the type and outcome of adjuvant systemic therapy received by three of the patients , because of the retrospective anonymized nature of this study . in conclusion , we provide a comprehensive histopathologic and molecular overview of a very rare and understudied tumor type . 
ligtenberg employment : synthon ( i ) honoraria : astrazeneca ( inst ) , msd ( inst ) consulting or advisory role : astrazeneca ( inst ) , bayer ( inst ) , bristol - myers squibb ( inst ) , janssen ( inst ) , merck sharp and dohme ( inst ) , novartis ( inst ) , roche ( inst ) , lilly ( inst ) research funding : astrazeneca ( inst ) , bristol - myers squibb ( inst ) no other potential conicts of interest were reported . acknowledgment we would like to thank mandy hermsen , lisa plettenburg , and chinook ophelders for technical assistance ; palga and the ncr for providing data ; and pathology laboratories ( pathan , gelre hospitals , olvg , meander medical center , and martini hospital ) for providing tumor tissue . references rindi g , klimstra ds , abedi - ardekani b , et al : a common classication framework for neuroendocrine neoplasms : an international agency for research on cancer ( iarc ) and world health organization ( who ) expert consensus proposal . 
mod pathol 31 : 1770 - 1786 , 2018 klimstra ds , lam ak , paradis v , et al : tumours of the gallbladder and extrahepatic bile ducts , in who classication of tumours , 5th edition : digestive system tumours . 
am j surg pathol 11 : 71 - 86 , 1987 ( suppl 1 ) furlan d , cerutti r , genasetti a , et al : microallelotyping denes the monoclonal or the polyclonal origin of mixed and collision endocrine - exocrine tumors of the gut . 
world j surg 29 : 92 - 101 , 2005 yao jc , hassan m , phan a , et al : one hundred years after carcinoid : epidemiology of and prognostic factors for neuroendocrine tumors in 35 , 825 cases in the united states . 
j clin oncol 26 : 3063 - 3072 , 2008 sciarra a , missiaglia e , trimech m , et al : gallbladder mixed neuroendocrine - non - neuroendocrine neoplasm ( minen ) arising in intracholecystic papillary neoplasm : clinicopathologic and molecular analysis of a case and review of the literature . 
meguro y , fukushima n , koizumi m , et al : a case of mixed adenoneuroendocrine carcinoma of the gallbladder arising from an intracystic papillary neoplasm associated with pancreaticobiliary maljunction . 
acosta am , hamedani fs , kajdacsy - balla a , et al : primary mixed adenoneuroendocrine carcinoma of the gallbladder in a 55 - year - old female patient : a case report and review of the literature . 
de bitter tjj , van der linden rla , van vliet s , et al : colorectal metastasis to the gallbladder mimicking a primary gallbladder malignancy : histopathological and molecular characteristics . 
eijkelenboom a , kamping ej , kastner - van raaij aw , et al : reliable next - generation sequencing of formalin - xed , parafn - embedded tissue using single 15 . 
kroeze li , de voer rm , kamping ej , et al : evaluation of a hybrid capture - based pan - cancer panel for analysis of treatment stratifying oncogenic aberrations and molecule tags . 
eijkelenboom a , tops bbj , van den berg a , et al : recommendations for the clinical interpretation and reporting of copy number gains using gene panel ngs analysis in routine diagnostics . 
neveling k , feenstra i , gilissen c , et al : a post - hoc comparison of the utility of sanger sequencing and exome sequencing for the diagnosis of heterogeneous diseases . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
scardoni m , vittoria e , volante m , et al : mixed adenoneuroendocrine carcinomas of the gastrointestinal tract : targeted next - generation sequencing suggests a monoclonal origin of the two components . 
voss mh , hierro c , heist rs , et al : a phase i , open - label , multicenter , dose - escalation study of the oral selective fgfr inhibitor debio 1347 in patients with advanced solid tumors harboring fgfr gene alterations . 
chung , phd1 purpose brca1 or brca2 loss of function results in homologous recombination deciency ( hrd ) , which is targetable by poly ( adp - ribose ) polymerase ( parp ) inhibitors and other dna - damaging agents . 
in cancers associated with germline brca1 / 2 alterations ( brca1 / 2 - associated cancers : breast , ovarian , pancreatic , prostate ) , brca1 / 2 alterations result in hrd and are biomarkers for parp inhibitor use . 
across cancer types , biallelic brca1 / 2 alteration was associated with increased gloh versus monoallelic or wild - type brca1 / 2 ; predicted germline or somatic mutations were both associated with elevated gloh . conclusion biallelic brca1 / 2 alterations were associated with elevated gloh in diverse cancer types , including those not traditionally associated with brca1 / 2 cancer syndromes . 
biomarker development for parp inhibitors should integrate methods to distinguish biallelic from monoallelic brca1 / 2 status , and biallelic brca1 / 2 alteration should be broadly evaluated across cancer types as a biomarker for underlying hrd and parp inhibitor sensitivity . jco precis oncol 4 : 442 - 465 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction brca1 and brca2 encode critical components of the homologous recombination ( hr ) dna repair pathway that maintains genomic stability.1 germline brca1 / 2 ( gbrca1 / 2 ) alterations are associated with elevated risk for breast , ovarian , pancreatic , and prostate cancer ( brca1 / 2 - associated cancers ) , 2 , 3 and tumors that arise in brca1 / 2 mutation carriers have often lost the wild - type allele.4 synthetic lethal interactions between brca1 / 2 loss of function and poly ( adp - ribose ) polymerase inhibitors ( parpi ) underlie development and regulatory approval of parpi targeted therapy for ovarian , breast , and pancreatic cancer.1 , 5 companion diagnostic testing for gbrca1 / 2 and somatic brca1 / 2 ( sbrca1 / 2 ) alteration1 can guide parpi therapy selection . brca1 or brca2 loss - of - function results in hr deciency ( hrd ) and accumulation of chromosomal rearrangements and copy number alterations . 
 pan - cancer analysis of biallelic brca1 / 2 context key objective brca1 / 2 loss - of - function alterations result in homologous recombination deciency ( hrd ) and are biomarkers for poly ( adpribose ) polymerase ( parp ) inhibitor sensitivity in breast , ovarian , prostate , and pancreatic cancer . 
to determine the relevance of brca1 / 2 alterations across cancer types , we evaluated the pan - cancer landscape of brca1 / 2 alterations and their association with the genome - wide loss - of - heterozygosity ( gloh ) marker of hrd . knowledge generated the fraction of brca1 / 2 alterations that were biallelic differed by cancer type and predicted germline / somatic status . 
brca1 / 2 alterations were most frequently biallelic in breast , ovarian , prostate , and pancreatic cancer ; in other cancer types , 44% of brca1 / 2 alterations were biallelic . 
percent gloh was calculated as a signature of hrd as previously described.9 , 10 see the appendix for full methods . results to assess the prevalence of brca1 / 2 genomic alterations across cancer types , we examined cgp results from 234 , 154 tumors sequenced as part of routine clinical care . overall , brca1 / 2 alterations were observed in 4.7% of cases ( brca1 , 2.1% ; brca2 , 2.7% ; fig 1a ; appendix fig a1 )  . 
brca1 and brca2 alterations were most frequent in ovarian ( 10.5% ) and prostate cancer ( 9.6% ) , respectively ; unlike brca2 , brca1 alterations were infrequent in prostate cancer . brca1 / 2 homozygous deletions were infrequent except in prostate cancer , where brca2 deletions were observed at a 2.6% frequency and accounted for 25% of brca1 / 2altered cases . 
brca1 / 2 mutations were distributed throughout the length of each gene , and most were truncating events ( appendix fig a2 )  . germline / somatic status for brca1 / 2 short variant mutations was predicted using validated computational methods.18 we also evaluated performance of germline / somatic predictions in this study . 
fraction ( % ) of ( b ) brca1 or ( c ) brca2 mutations predicted to be germline v somatic was determined for each cancer type . see the data supplement for detailed data . computational methods correctly identied 21 ( 91% ) as predicted germline variants . 
second , because cell - free dna ( cfdna ) sequencing can often distinguish germline from somatic variants , 19 we evaluated 52 brca1 / 2 germline / somatic predictions from tissue samples and evaluated patientmatched cfdna ngs results . 
as expected , the majority of mutations were predicted to be germline in brca1 / 2 - associated cancers ( brca1 , 58.1% ; brca2 , 56.8% ) , but predicted sbrca1 / 2 mutations comprised an appreciable proportion of brca1 / 2 mutations . 
 ( a ) fraction of brca1 / 2 - altered cases with biallelic or monoallelic alteration was determined . brca1 / 2 - altered cases were evaluated for class of alteration identied and classied as biallelic ( multiple brca1 or multiple brca2 alterations in the same sample , homozygous deletion , biallelic short variant mutation [ loss of heterozygosity of the wild - type allele ] ) , monoallelic ( heterozygous mutation ) , or unknown ( zygosity status could not be determined )  . 
a lower - bound estimate was established by assessing biallelic cases as a fraction of all brca1 / 2 - altered cases , including those with unknown biallelic / monoallelic status ( see data supplement )  . 
for cases where biallelic / monoallelic status could be determined , we estimated the fraction of brca1 / 2 - altered cases with biallelic alteration ( biallelic fraction )  . 
although biallelic fraction was lower in nonbrca1 / 2 - associated cancers ( p , .0001 , fishers exact test ) , biallelic alterations nonetheless comprised 43.6% of brca1 / 2 - altered cases : biallelic fraction was  . 
1% frequency in at least 13 cancer types . in prostate cancer , predicted gbrca1 / 2 and sbrca1 / 2 mutations were separately assessed for biallelic fraction ( fig 3 ; appendix fig a5 )  . 
for brca1 / 2associated cancers , both predicted gbrca1 / 2 ( 90.8% ) and sbrca1 / 2 ( 81.2% ) mutations were frequently biallelic , whereas in nonbrca1 / 2 - associated cancers , fewer predicted gbrca1 / 2 ( 46.4% ) and sbrca1 / 2 ( 25.4% ) mutations were biallelic . 
in ovarian and breast cancer , the majority of brca1 and brca2 mutations were biallelic , both for predicted germline and the majority of somatic mutations . brca2 ( gbrca2 , 87.6% ; sbrca2 , 75.0% ) mutations were biallelic , but brca1 ( gbrca1 , 40.0% ; sbrca1 , 22.2% ) mutations were less frequently biallelic . 
cases with 16% gloh were classied as gloh - high on the basis of the cutoff established in the ariel3 trial of rucaparib in ovarian cancer.10 biallelic brca1 / 2 alterations were associated with gloh - high across every cancer type examined . 
the fraction of cases that were gloh - high was signicantly increased for biallelic brca1 / 2 - altered compared with wild - type cases ( fig 4a , appendix fig a6a ) , whereas the fraction of monoallelic brca1 / 2 cases that were gloh - high was similar to wild type . 
signicant association of biallelic but not monoallelic alterations with gloh - high was observed both for brca1 and for brca2 when assessed individually ( figs 4b and 4c )  . 
in some cancer types , significant but modest elevation in tumor mutational burden ( tmb ) was observed for biallelic brca1 / 2 - mutated cases ( predicted germline or somatic ) versus wild type ; however , the association with tmb was not consistent across cancer types ( appendix fig a7 )  . 
monoallelic sbrca1 / 2 - mutated ( but not gbrca1 / 2 ) cases were commonly associated with elevated tmb versus wild type , and such mutations may be a consequence of increased mutation rate . although biallelic brca1 / 2 status was consistently associated with gloh - high , the magnitude was variable for each cancer type , with the greatest association observed in pancreatic ( or , 22.5 ) , biliary ( or , 21.5 ) , endometrial ( or , 17.2 ) , unknown primary ( or , 16.1 ) , and ovarian ( or , 14.9 ) cancer ( fig 4a )  . 
more than 75% of cases with biallelic brca1 / 2 alterations were gloh - high for ovarian , breast , pancreatic , unknown primary , and endometrial cancer , whereas fewer than half were gloh - high for prostate and colorectal cancer . 
25% of brca1 / 2 wildtype cases were gloh - high for ovarian , breast , lung , and gastric / esophageal cancer . the 16% gloh - high cutoff was clinically validated in ovarian cancer9 , 10 and requires optimization for other cancer types . 
consistent with the ndings using a gloh cutoff - based approach , gloh scores were higher in brca1 / 2 biallelic versus wild - type cases across all cancer types evaluated ; increased gloh score was also observed when biallelic brca1 and brca2 were evaluated independently . hrd signatures ( including gloh - high ) may identify additional brca1 / 2 wild - type tumors potentially suitable for parpi.9 , 10 , 20 overall , 19.3% of cases were gloh - high compared with 3.2% of cases with biallelic brca1 / 2 alteration , and for most cancer types , the frequency of gloh - high was greater than biallelic brca1 / 2 alterations ( data supplement ) ; distribution of gloh scores varied between cancer types . 
to inform rational cancer typespecic gloh - high cutoffs , we assessed the performance of different gloh - high thresholds to classify biallelic brca1 / 2 compared with wild - type cases . 
plotting sensitivity to detect cases with biallelic brca1 / 2 alteration and specicity ( percentage of brca1 / 2 wild - type cases negative for the glohhigh biomarker ) , we identied a cutoff that maximized the combined sensitivity and specicity score ( fig 6 )  . 
the identied cutoff for ovarian cancer was 15.1% , which was consistent with the 14% and 16% cutoffs identied in clinical trials.9 , 10 discussion the development of parpi for brca1 / 2 altered ovarian , breast , and pancreatic cancer1 , 5 is predicated on synthetic lethality interactions between brca1 / 2 loss of function and parpi / trapping . 
emerging clinical trial data suggest that brca1 / 2 alteration may also be predictive of parpi response in prostate cancer.1 , 11 - 13 although responses to parpi have been documented in other cancer types , 14 , 21 - 23 the relevance of brca1 / 2 alterations in nonbrca1 / 2associated cancers remains unclear.4 to understand the landscape and phenotypic consequence of brca1 / 2 alterations , we assessed our data set of 234 , 154 cancer specimens sequenced using a clinicalgrade cgp assay . 
brca1 / 2 alterations were frequent in brca1 / 2 - associated cancers but also observed in a signicant fraction ( 3% ) of nonbrca1 / 2 - associated cancers . 
predicted germline mutations comprised the majority of brca1 / 2 mutations in brca1 / 2 - associated cancers ; however , it is notable that 43% were predicted somatic ( of which 81% were biallelic ) given data that support sbrca1 / 2 alteration as a biomarker for parpi in ovarian and prostate cancer.1 , 11 - 13 brca1 / 2 alterations were assessed for biallelic versus monoallelic status to distinguish likely loss of function from biologically neutral alterations . 
of note , although monoallelic alteration in brca1 / 2 mutation carriers may have a subtle haploinsufcient phenotype , 24 it does not lead to severe hrd or sensitivity to platinum - based chemotherapy.25 consistent with the established role of brca1 / 2 in the pathogenesis of brca1 / 2 - associated cancers , 90% of brca1 / 2 - altered cases were biallelic with high biallelic fraction both for predicted gbrca1 / 2 and sbrca1 / 2 . 
differences in brca1 and brca2 biallelic fraction were observed : brca2 was more frequently biallelic in prostate and small - cell lung cancer , and brca1 was more frequently biallelic in endometrial cancer , esophageal scc , colorectal cancer , and melanoma . 
the frequency of ( a ) brca1 / 2 , ( b ) brca1 , or ( c ) brca2 biallelic , monoallelic , and wild - type cases that were gloh - high was compared across cancer types . 
50 biallelic brca1 / 2 - altered samples were assessed individually , and all other cancer types were grouped together and analyzed as a single group ( other )  . 
association between brca1 / 2 biallelic alteration and genome - wide loss of heterozygosity ( gloh ) score as a continuous variable . gloh score was assessed in ( a ) brca1 / 2 , ( b ) brca1 , and ( c ) brca2 biallelic v wild - type cases across cancer types . 
boxes span the rst and third quartiles , and the median is denoted by the horizontal line in the box ; whiskers indicate maximum and minimum values within 1.5 the interquartile range ; black dots indicate outlier events . 
 100 sokol et al ovarian prostate breast endometrial pancreatic bladder / uc gastric / esophageal adenocarcinoma biliary tract colorectal nsclc % gloh sensitivity specificity % gloh % gloh fig 6 . 
 pan - cancer analysis of biallelic brca1 / 2 differences suggest that brca1 and brca2 may have tissue specicities outside breast and ovarian different cancer . to determine whether brca1 / 2 alterations lead to hrd in both brca1 / 2 - associated and nonbrca1 / 2 - associated cancers , we evaluated gloh in brca1 / 2 - altered versus type evaluated , wild - type cases . 
monoallelic alterations may be found in sporadic cancers from gbrca1 / 2 carriers or as somatic passenger mutations . distinguishing biallelic from monoallelic status may be an important consideration for rening brca1 / 2 alteration as a predictive biomarker for parpi . 
in brca1 / 2 - associated cancers , brca1 / 2 alteration status alone has proven sufcient as a predictive biomarker , 1 likely explained by the majority of brca1 / 2 alterations in this context being biallelic . 
nevertheless , parpi trials in prostate cancer have incorporated brca1 / 2 biallelic status into biomarker development , 13 and our nding of signicantly lower biallelic fraction for brca1 ( v brca2 ) in prostate cancer suggests that integrating biallelic status could rene predictive biomarkers in this setting . the lack of parpi clinical activity in nonbrca1 / 2 - associated cancers reported previously could be explained by grouped analysis of biallelic and monoallelic brca1 / 2 alterations.4 because of lower rates of biallelic alteration in nonbrca1 / 2 - associated cancers , parpi clinical trials will likely require patient selection strategies that incorporate methods to discriminate biallelic from monoallelic brca1 / 2 alterations . our ndings are consistent with a recent study that demonstrated an elevated hrd composite score in biallelic but not heterozygous brca1 / 2 cases relative to wild type in an aggregate set of nonbrca1 / 2 - associated cancers.4 a strength of the current study was that the large data set size enabled analysis of biallelic brca1 / 2 separately from monoallelic alterations , independent assessment of brca1 and brca2 , and evaluation of nonbrca1 / 2 - associated cancers as individual cancer types rather than in aggregate , which may have enabled identication of associations between biallelic brca1 / 2 alterations and an hrd signature across cancer types not previously described.4 if brca1 / 2 biallelic alterations functionally result in hrd , they should represent a targetable vulnerability to parpi and platinum - based chemotherapy , irrespective of whether they are drivers of disease pathogenesis or bystander passenger alterations.26 our data demonstrate that biallelic brca1 / 2 alteration in nonbrca1 / 2 - associated cancers are associated with the gloh - high signature of hrd and , therefore , warrant investigation in parpi trials . 
although biallelic brca1 / 2 alterations occur at low prevalence in nonbrca1 / 2 - associated cancers , basket trials that led to the tumor - agnostic approvals of ntrk inhibitors for ntrk fusion - positive tumors and pembrolizumab for microsatellite instabilityhigh tumors27 demonstrate feasibility of therapeutic development for rare pan - cancer biomarkers . 
clinical trials such as the tapur study ( clinicaltrials.gov identier : nct02693535 ) that treatment arm for brca1 / 2 - altered includes a parpi cancers will inform parpi development in nonbrca1 / 2associated cancers , and analyses may benet from consideration of monoallelic versus biallelic status . although gloh - high is associated with clinical benet from rucaparib in ovarian cancer , 9 , 10 understanding of the gloh biomarker in other cancer types is required . 
evaluation of sensitivity and specicity of varying gloh thresholds to distinguish biallelic brca1 / 2 - altered and wild - type cases may inform development of disease - specic gloh - high cutoffs . 
in future studies , analysis of brca1 / 2 wild - type , gloh - high cases may be a discovery tool for characterizing brca1 / 2 vuss and for prioritizing candidate non - brca1 / 2 hr pathway gene biomarkers.9 although detection of gloh - high in brca1 / 2 wild - type cases potentially expands the patient population addressable by parpi , the utility of gloh - high requires validation in prospective trials for nonovarian cancers . limitations of this study should be acknowledged . 
first , we focus on gloh as a biomarker for hrd ; other hrd markers were not evaluated , including telomeric allelic imbalance ( tai ) , large - scale transition ( lst ) , mychoice hrd ( combination loh / tai / lst score ; myriad genetics , salt lake city , ut ) , signature 3 , and hrdetect.7 , 8 , 28 - 33 in parpi trials , hrd biomarkers have focused on approaches that are compatible with targeted ngs assays ( gloh , mychoice hrd ) , which are used in routine clinical practice.1 , 9 , 10 in contrast , signature 3 and hrdetect signatures have been evaluated in the research setting using whole - exome or whole - genome sequencing ; novel methods may enable future clinical assessment of signature 3 with targeted assays.34 second , germline / somatic status predictions using tumor - only sequencing and computational methods are less denitive compared with matched normal sequencing used in other studies.4 , 18 third , using brca1 / 2 biallelic versus wild - type status to rene gloh - high cutoffs is confounded by some brca1 / 2 wild - type gloh - high cases that are hrd because of brca1 / 2 alteration independent mechanisms , such as brca1 / 2 methylation or alteration in other hr genes . 
 sokol et al in the future ; however , we focused on brca1 / 2 because other hr pathway genes have not been consistently predictive of clinical response to parpi , 11 - 13 , 36 and robust clinical evidence supporting predictive biomarker genes beyond brca1 / 2 is lacking . 
finally , clinical outcomes data that associate parpi response with biallelic brca1 / 2 alteration and gloh were not available and require evaluation in clinical trials . we demonstrate that biallelic brca1 / 2 alterations are associated with elevated gloh across all cancer types evaluated and may therefore represent a therapeutic vulnerability targetable by parpi . 
ali , shridar ganesan , jon h . chung financial support : brian alexander administrative support : brian alexander provision of study material or patients : hossein khiabanian , primo n . 
gregg consulting or advisory role : astrazeneca , bristol - myers squibb , roche , foundation medicine , luminex speakers bureau : astrazeneca , foundation medicine , bristol - myers squibb primo n . 
 pan - cancer analysis of biallelic brca1 / 2 research funding : merck sharp & dohme ( inst ) , astrazeneca ( inst ) , ipsen ( inst ) travel , accommodations , expenses : roche , merck sharp & dohme , astrazeneca , janssen pharmaceuticals , rainier therapeutics other relationship : bayer ag ( i ) vincent a . 
miller employment : foundation medicine leadership : foundation medicine , revolution medicines stock and other ownership interests : foundation medicine , mirati therapeutics , revolution medicines patents , royalties , other intellectual property : periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center brian alexander employment : foundation medicine leadership : foundation medicine stock and other ownership interests : roche research funding : eli lilly ( inst ) , puma ( inst ) , celgene ( inst ) open payments link : 854258 / summary siraj m . 
ali employment : foundation medicine , eqrx , eqrx ( i ) leadership : incysus stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences consulting or advisory role : revolution medicines , azitra ( i ) , princepx tx ( i ) patents , royalties , other intellectual property : patents through foundation medicine , patents through seres health on microbiome stuff in nonneoplastic disease ( i ) shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis , roche , foghorn therapeutics , foundation medicine , merck sharp & dohme patents , royalties , other intellectual property : two patents for digital imaging that may be licensed to ibris and inspirata travel , accommodations , expenses : inspirata other relationship : national cancer institute / national institutes of health jon h . 
chung employment : foundation medicine stock and other ownership interests : foundation medicine no other potential conicts of interest were reported . references 105 : 812 - 822 , 2013 1 . 
nature 571 : 576 - 579 , 2019 [ erratum : nature 577 : e1 , 2020 ] golan t , hammel p , reni m , et al : maintenance olaparib for germline brca - mutated metastatic pancreatic cancer . 
nature 534 : 47 - 54 , 2016 [ erratum : nature 566 : e1 , 2019 ] davies h , glodzik d , morganella s , et al : hrdetect is a predictor of brca1 and brca2 deciency based on mutational signatures . 
j natl cancer inst 110 : 704 - 713 , 2018 swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
coleman rl , oza am , lorusso d , et al : rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
abida w , bryce ah , vogelzang nj , et al : preliminary results from triton2 : a phase ii study of rucaparib in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) associated with homologous recombination repair ( hrr ) gene alterations . 
smith mr , sandhu sk , kelly wk , et al : phase ii study of niraparib in patients with metastatic castration - resistant prostate cancer ( mcrpc ) and biallelic dnarepair gene defects ( drd ) : preliminary results of galahad . 
sandhu sk , schelman wr , wilding g , et al : the poly ( adp - ribose ) polymerase inhibitor niraparib ( mk4827 ) in brca mutation carriers and patients with sporadic cancer : a phase 1 dose - escalation trial . 
slavin tp , banks kc , chudova d , et al : identication of incidental germline mutations in patients with advanced solid tumors who underwent cell - free circulating tumor dna sequencing . 
moore kn , secord aa , geller ma , et al : niraparib monotherapy for late - line treatment of ovarian cancer ( quadra ) : a multicentre , open - label , single - arm , 21 . 
necchi a , raggi d , giannatempo p , et al : exceptional response to olaparib in brca2 - altered urothelial carcinoma after pd - l1 inhibitor and chemotherapy 22 . 
hierro c , matos i , martin - liberal j , et al : agnostic - histology approval of new drugs in oncology : are we already there ? clin cancer res 25 : 3210 - 3219 , 2019 28 . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deciency among breast cancer 31 . 
telli ml , timms km , reid j , et al : homologous recombination deciency ( hrd ) score predicts response to platinum - containing neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
marshall ch , sokolova ao , mcnatty al , et al : differential response to olaparib treatment among men with metastatic castration - resistant prostate cancer harboring brca1 or brca2 versus atm mutations . 
 pan - cancer analysis of biallelic brca1 / 2 appendix supplementary methods approval for this study , including a waiver of informed consent and health insurance portability and accountability act waiver of authorization , was obtained from the western institutional review board ( irb ; protocol #20152817 )  . 
cgp results included in this study were from tumor tissue specimens ( n = 234 , 154 ) submitted as part of routine clinical care ( december 2013 - march 2019 ) ; for patient characteristics , see the data supplement . 
in validation testing of 480 tumor - only sequencing calls against matched normal specimens , accuracy was 95% for somatic and 99% for germline calls ( sun jx , et al : plos comput biol 14 : e1005965 , 2018 ) ; in assessment of zygosity calls , signicant enrichment in mutations with loss of heterozygosity ( loh ) was observed for tumor suppressor genes ( sun jx , et al : plos comput biol 14 : e1005965 , 2018 )  . 
to evaluate performance of germline / somatic computational predictions in this series , we compared predictions against a subset of cases with available results from patient - matched germline testing or cell - free dna ( cfdna ) ngs that were performed as previously described ( clark ta , et al : j mol diagnostics 20 : 686 - 702 , 2018 ; khiabanian h , et al : jco precis oncol 2 : 1 - 15 , 2018 ) ; brca1 / 2 genetic testing on a subset of patients at the rutgers cancer institute of new jersey were analyzed under the auspices of an irb - approved protocol . 
germline - like af was dened as mutations observed in cfdna at 40% - 60% af ( except for cfdna samples with high circulating tumor dna fraction [  . 20% ] that were excluded from the analysis as ambiguous )  . 
brca1 / 2 alterations were categorized as biallelic , monoallelic , or unknown . biallelic alterations were mutations with loh of the wild - type allele , as determined by zygosity status ( sun jx , et al : plos comput biol 14 : e1005965 , 2018 ) ; homozygous deletion ; or 2 brca1 or 2 brca2 alterations in a sample . 
percent genome - wide loh ( gloh ) was calculated as a signature of hrd as previously described ( coleman rl , et al : lancet 390 : 1949 - 1961 , 2017 ; swisher em , et al : lancet oncol 18 : 75 - 87 , 2017 )  . 
this prole was segmented and interpreted using afs of sequenced snps to estimate copy number ( ci ) and minor allele count ( mi ) at each segment ( i )  . 
two types of loh segments were excluded from the calculation of percent gloh : loh segments that spanned 90% of a whole chromosome or chromosome arm because these loh events usually arise through non - hrd mechanisms ( eg , mitotic nondisjunction ) and regions in which loh inference was ambiguous . 
for each tumor , the percent gloh was computed as 100 the total length of nonexcluded loh regions ( xi ) divided by the total length of nonexcluded regions of the genome . 
 sokol et al brca1 / 2 short variant homozygous deletion rearrangement multiple brca1 brca2 short variant homozygous deletion rearrangement multiple brca1 brca2 breast cancer ovarian cancer breast cancer ovarian cancer fig a1 . 
growth factor receptor 2 ( her2 ) status was determined on the basis of the presence or absence of a copy number amplication ; triple - negative breast cancer ( tnbc ) was dened as er - negative , her2 - negative samples . 
 somatic af germline af cfdna germline af cfdna somatic af 5 10 15 20 25 30 35 40 45 50 55 60 65 70 75 80 85 90 95 brca1 / 2 variant allele frequency ( % ) predicted germline ( n = 22 ) predicted somatic ( n = 30 ) cfdna gbrca sbrca predicted germline predicted somatic sokol et al predicted germline predicted somatic breast cancer ovarian cancer fig a3 . 
 ( a and b ) comparison of tissue - based germline / somatic predictions to brca1 / 2 allele frequencies ( afs ) in patient - matched cell - free dna ( cfdna )  . 
mutations with germline af were dened as those identied in cfdna at 40% - 60% af , except for cases with high circulating tumor dna fraction ( 20% ) that were excluded from the analysis as ambiguous af . 
 ( c - e ) predicted germline / somatic status calls were made for each brca1 or brca2 short variant mutation . for mutations yielding a successful call , frequency of predicted germline v somatic mutation was determined for ( c ) brca1 / 2 across cancer types , ( d ) brca1 / 2 ( grouped and individually ) overall ( n = 5 , 845 ) for brca1 / 2 - associated cancers ( breast , ovarian , pancreatic , prostate ; n = 3 , 061 ) and nonbrca1 / 2 - associated cancers ( n = 2 , 784 ) , and ( e ) brca1 / 2 for the subset of ovarian and breast cancer cases where molecular / histologic subtype information was available . 
relative fraction of brca1 / 2 - altered cases with biallelic or monoallelic alteration was determined for ( a ) brca1 across cancer types and ( b ) brca2 across cancer types . 
 ( c ) brca1 / 2 ; ( d ) brca1 ; ( e ) brca2 for overall , brca1 / 2 - associated cancers , and nonbrca1 / 2 - associated cancers ; and ( f ) brca1 / 2 for the subset of ovarian and breast cancer cases where molecular / histologic subtype information was available . 
 ( a ) brca1 / 2 mutations ( grouped ) with a germline ( gbrca1 / 2 ) or somatic ( sbrca1 / 2 ) prediction were evaluated for biallelic / monoallelic status for all cancers , brca1 / 2 - associated cancers ( as a group and as individual cancer types ) , and nonbrca1 / 2 - associated cancers ( see data supplement )  . 
cases with somatic brca1 / 2 ( sbrca1 / 2 ) or germline brca1 / 2 ( gbrca1 / 2 ) biallelic mutation , monoallelic mutation , or wild - type ( wt ) brca1 / 2 were plotted against tumor mutational burden ( tmb in mutations / mb ; log10 score )  . 
box and whisker plot where the box spans the rst and third quartiles , the median is denoted by the horizontal line in the box , and whiskers indicate maximum and minimum values within 1.5 the interquartile range ( see data supplement )  . 
 ( a ) the frequency of brca1 / 2 biallelic , monoallelic , and wild - type cases that were high genome - wide loss of heterozygosity ( gloh - high ) was compared in the subset of ovarian and breast cancer cases where molecular / histologic subtype information was available ( see data supplement )  . 
 ( b ) frequency of predicted germline brca1 / 2 ( gbrca1 / 2 ) biallelic , monoallelic , and wild - type cases that were gloh - high ( see data supplement )  . 
 ( c ) frequency of predicted somatic brca1 / 2 ( sbrca1 / 2 ) biallelic , monoallelic , and wild - type cases that were gloh - high ( see data supplement )  . 
our real - time tumor sequencing program , which makes precision treatment decisions for patients with cancer , produces matched germline information , providing a unique opportunity to efficiently implement pharmacogenetics and benefit patients . methods the germline genetic database from the michigan oncology sequencing ( mi - oncoseq ) program was searched for 21 clinically actionable polymorphisms in five cancer - relevant genes : tpmt , dpyd , cyp2c19 , cyp3a5 , and ugt1a1 . 
the medical records of mi - oncoseq patients with actionable phenotypes were searched for receipt of relevant drugs and to determine whether having genetic information at the time of treatment would have led to a treatment recommendation . results all nine variants in tpmt , dpyd , and cyp2c19 that were detected in mi - oncoseq were confirmed by external genotyping . 
on the basis of retrospective assessment of 115 adult and pediatric patient records , 4.3% ( n = 5 ) had a potentially clinically actionable phenotype for tpmt , dpyd , or cyp2c19 and received a relevant medication . 
 after accounting for differences in adult and pediatric recommendations , three of these patients could have received a treatment recommendation at the time of prescribing . conclusion germline genotype determinations for tpmt , dpyd , and cyp2c19 can be used to make evidence - based treatment recommendations in mi - oncoseq patients . 
 although the proportion of patients for whom recommendations can be made is small , this added value to mi - oncoseq and patient care comes at no additional genotyping cost . 
2018 by american society of clinical oncology introduction the genomes of patients ( germline ) and their tumors ( somatic ) each provide useful information to guide precision medicine in oncology . 
vali dated pharmacogenetic associations exist for several germline polymorphisms with com monly used cancer treatments , including thiopu rines ( tpmt ) , 1 fluorouracil ( fu ) / capecitabine ( dpyd ) , 2 irinotecan ( ugt1a1 ) , 3 and tacrolimus ( cyp3a5 ) .4 additionally , there are several known associations with supportive care agents com monly used in patients during treatment , such fungal prophylaxis with voriconazole ( cyp2c19 ) 5 and antiemetic treatment with ondansetron ( cyp2d6 ) .6 despite their established clinical validity , few of these associations have been implemented into clinical practice . 
st jude childrens research hospital has led the way , implementing pre emptive pharmacogenetic testing to guide per sonalized treatment of several genedrug pairs.7 the experiences of early adopters has identified formidable challenges to implementing phar macogenetics into clinical practice , 8 , 9 which require substantial investment and expertise.10 , 11 daniel l . 
mody arul chinnaiyan author affiliations and support information ( if applicable ) appear at the end of this article . the content is solely the responsibility of the authors and does not necessarily represent the official views of the national institutes of health . corresponding author : daniel l . 
although there is debate about the necessity and feasibility of demon strating clinical utility for pharmacogenetic implementation , 12 , 13 the lack of uptake indicates that health systems are not willing to incur the costs of pharmacogenetic implementation for unproven clinical benefit . 
however , available germline genetic information should be con sidered when making treatment decisions.14 in anticipation of a time when genetic informa tion is available for many patients , perhaps as a result of the proliferation of directtoconsumer genotyping , 15 the pharmacogenetic community has developed evidencebased pharmacogenetic treatment guidelines.3 , 16 in oncology , there has been a tremendous expan sion in the availability of genetic information as a result of the proliferation of tumor sequenc ing programs that use somatic genetic informa tion to personalize selection of targeted cancer treatments.17 although some programs analyze only the somatic genome , others have found that matched germline analysis improves quality control18 and enables simultaneous assessment of familial predisposition to cancer.19 this cre ates a unique situation in which germline genetic information for clinically relevant pharmaco genes is freely available.20 however , the oppor tunity to use these data in clinical practice has not yet been capitalized upon . the michigan oncology sequencing ( mi oncoseq ) program at the university of michi gan comprehensive cancer center ( umccc ) performs targeted sequencing of somatic and matched germline dna , in addition to somatic wholetranscriptome analysis . 
21 the targeted sequencing panel includes approximately 100 pharmacogenes that could be used to provide evidencebased pharmacogenetic treatment rec ommendations , if the accuracy of the germline genetic determinations are verified . 
detailed study information including inclusion and exclusion criteria , data analysis and processing , and return of results has been pre viously published.2123 briefly , patients treated at umccc with refractory tumors are invited to participate in a research protocol in which they provide tumor and blood samples for matched genetic sequencing , among other somatic anal yses . 
 since the initiation of mioncoseq , the dna sequencing platform has transitioned from wholeexome sequencing to a targeted exon sequencing panel , and sequencing methods have been previously described in detail.21 , 23 this tar geted panel sequences primarily exonic regions of approximately 1 , 700 genes , including approx imately 100 pharmacogenes selected based on curation within pharmgkb ( appendix table a1 )  . 
these five genes were selected based on their relevance to cancer treatment or sup portive care , likelihood of clinician interest in prospective implementation of the genedrug pairs , and existence of evidencebased treatment guidelines from the clinical pharmacogenet ics implementation consortium ( cpic ) 16 or the dutch pharmacogenetics working group ( dpwg ) .3 the polymorphisms in each gene were selected based on the validated variant lists within each guideline . 
note that ugt1a1 * 28 ( rs8175347 ) and * 80 ( rs887829 ) were both included to represent the ugt1a1 * 28 geno type , because they are highly linked , and * 80 is often substituted for * 28 as a result of its relative ease of genotyping.24 the mioncoseq germ line genetic database was screened to identify all variant calls at any of these polymorphisms for all patients sequenced on onco1700_v4 , and variant calls were compiled in a single data set for further analysis . confirmatory genotyping genotype determinations from onco1700 were manually screened for potentially unreliable calls by assessing standard sequencing quality con trol parameters , including read depth . 
in the second stage , polymor phisms with > five but < 30 occurrences were selected , by prioritizing patients who also car ried a variant at one of the common snp posi tions . 
finally , as many samples as necessary were selected that carried these common variants so that each variant was represented in five samples . selected samples were sent for college of american pathologistsaccredited , clinical lab oratory improvement amendmentsapproved genotyping at genelex laboratories ( seat tle , wa )  . 
genotypes were obtained using a laboratorydeveloped , multiplex polymerase chain reactionbased test followed by single base primer extension for variant detection by mass spectrometry ( massarray analyzer 4 system ; agena bioscience , san diego , ca )  . 
percent concordance for each snp was calculated as the number of concordant genotypes divided by the total number of samples compared . retrospective analysis of clinically actionable phenotypes patient genotypes were translated to activity phenotypes based on the appropriate cpic26 or dpwg3 guidelines ( appendix table a2 )  . 
genotype data for ugt1a1 * 28 ( * 80 ) and cyp3a5 * 3 was only available for the 25 samples sent for confirma tory genotyping ; therefore , these patients and genotypes were included in assessments of clin ical usefulness . 
medical record screening was performed using an automated screening tool ( emerse27 ) that searches the text of notes in michart , the version of epic used at mich igan medicine . 
text used to screen the medical records included all generic and brand drug names and commonly used acronyms ( eg , fu for fluourouracil )  . a pharmacy student , in consultation with a phar macist with oncology pharmacogenomic expertise , manually reviewed the electronic medical record for each patient who had an actionable pheno type and received the relevant drug to determine whether a treatment modification would have been recommended had this genetic information been available to the clinician before treatment initia tion . 
these patients represent the diversity of the mioncoseq cohort , including adult ( n = 82 ; 71% ) and pediatric patients ( n = 33 ; 29% ) who were evenly divided between male ( n = 58 ; 50% ) and female sex ( n = 57 ; 50% ) , were primarily white ( n = 97 ; 84% ) , and had a variety of solid ( n = 80 ; 70% ) and liquid tumor types ( n = 35 ; 30% )  . no genotype determinations for cyp3a5 * 3 , ugt1a1 * 28 , or ugt1a1 * 80 were made by onco1700 because of low read depth ( cyp3a5 * 3 and ugt1a1 * 80 ) or sequence repeat misalign ment ( ugt1a1 * 28 ) ; therefore , these polymor phisms were excluded from genotype concordance analyses . 
across the 18 remaining snps , a total of 139 variant calls were made in these 115 samples , and nine unique snps were detected in at least one patient ( table 1 )  . 
the frequency of actionable phenotypes was highest for cyp2c19 ( 43.5% ) , followed by cyp3a5 ( 20% ) , ugt1a1 ( 20% ) , and tpmt ( 13% ) , and lowest for dpyd ( 3.5% ) , as expected . the electronic medical record for each patient carrying an actionable phenotype was screened for relevant drugs . 
one patient with cyp2c19 rapid metabolizer phenotype never received voriconazole ; two patients with cyp2c19 rapid metabolizer phenotype received voriconazole treatment , but they were pediatric patients , so no dose adjustment is recommended per cpic guidelines5 ; and one patient with ugt1a1 poor metabolizer phenotype treated with irinotecan received a standard pediatric dose ( 49 mg / m2 ) , which is below the recommended threshold for dose adjustment based on dpwg guidelines.3 three patients with actionable phenotypes who received the relevant drug , in whom a treatment recommendation could have been made , were identified . 
one patients dose was held after 5 days because of neutro penia ( absolute neutrophil count [ anc ] , 200 ) , and the second patients dose was reduced to 70% of the standard dose after 7 days because of neutropenia ( anc , 500 )  . 
 are many challenges to pharmacogenetic imple mentation , 10 but perhaps the primary challenge is the current lack of evidence of clinical util ity to justify the upfront cost of establishing a pharmacogenetic service.31 , 32 in anticipation of a future in which genomic information is more readily available , cpic and other groups have published evidencebased treatment recommen dations for patients with known genotypes.3 , 16 there is a unique opportunity to integrate evidencebased pharmacogenetic treatment into tumor sequencing programs that analyze germline genetic information , 20 such as the mioncoseq program at umccc.21 the objective of this analysis was to confirm the accuracy of germ line genotype determinations produced during mioncoseq sequencing and then to retrospec tively assess the clinical usefulness of integrating pharmacogenetics into mioncoseq . attempted confirmatory genotyping of 21 clin ically actionable snps in five cancerrelevant pharmacogenes confirmed genotyping accu racy for common and uncommon variants in three genes ( tpmt , dpyd , and cyp2c19 ) but revealed an inability to genotype common vari ants in cyp3a5 and ugt1a1 . 
this finding is easily explained by the targeted exonic coverage of onco1700 and the location of these polymor phisms at a splice site ( cyyp3a5 * 3 , rs776746 ) and in the promoter region ( ugt1a1 * 28 , rs8175347 )  . 
other variants that were not detected are extremely rare , and several have not been found in white patients . prior studies have estimated that > 90% of the population has an actionable phenotype of at least one candidate gene33 , 34 ; however , this is only relevant if the patient is treated with the drug of interest and the guidelines apply to the patient . 
 in our cohort , 4% ( five of 115 ) of patients had a potentially actionable phenotype in cyp2c19 , tpmt , or dpyd and received the relevant drug , and in 2.6% ( three of 115 ) of patients , a guideline based treatment recommendation could have been made . manual review of these three patients identified several interesting findings . 
despite tpmt gen otype information available at the time of treat ment , two patients with heterozygous genotypes initiated treatment at standard mercaptopurine doses , per the childrens oncology group protocols on which they were enrolled . 
cpic recommends a preemptive 30% to 70% dose decrease with enhanced monitoring and titration based on tolerability.1 although germline tpmt determination from mioncoseq would not have changed these patients treatment in any way , it would have prevented external genetic testing , resulting in cost savings to the health systethe third patient carried a dpyd geno type that confers risk of severe toxicity with fu , which was not known at the time of treatment . 
 cpic guidelines recommend a preemptive dose reduction of 50% with monitoring and titra tion.2 although it is impossible to attribute tox icity to any single factor , it is interesting that two patients experienced toxicity requiring a reactive dose reduction , which may have been prevented if care had been based on cpic guidelines . the 2% to 4% absolute increase in the propor tion of patients with clinically actionable findings from germline pharmacogenetics represents a minimal estimate , because the emerse screen ing tool does not automatically screen prescrib ing data , and there is some chance that a patient with an actionable phenotype received a relevant medication that was never mentioned in a clini cal note . 
regardless , this represents a meaning ful increase in the clinically actionable findings from our tumor sequencing program.35 in addi tion to its usefulness for quality control , 18 , 36 matched germline analysis identifies validated cancer predisposition variants in an estimated 15% of patients.19 several tumor sequencing programs , including mioncoseq , 21 use their matched germline dna for this purpose.37 , 38 our results represent a critical first step toward integration of germline pharmacogenetics into mioncoseq . although several programs have reported that pharmacogenetics is considered in their deci sion making , 39 , 40 we are not aware of any detailed reports of the integration of pharmacogenetics into these programs . 
 used to inform irinotecan treatment decisions3 or how the incidental finding of gilberts syn drome would be conveyed to the patient.42 , 43 generalization of our estimate of the proportion of patients who could benefit from pharmacog enetic implementation in other tumor sequenc ing programs is challenging for several reasons . 
 first , there are differences in the frequencies of clinically actionable alleles or phenotypes among racial cohorts.44 additionally , institutional differ ences in the distribution of tumors that are treated and sent for sequencing could dramatically affect this estimate . 
 pharmacogenetic integration would be most ben eficial in programs that sequence tumors early in treatment , particularly at institutions that treat many pediatric patients with all . the proportion of patients who would benefit from pharmacogenetic implementation could be increased in several ways . 
mody , arul chinnaiyan substantial upfront investment to build and maintain clinical decision support within the electronic health record , hire or train individu als with pharmacogenetic expertise , and provide clinician and patient education . 
pharmacoge netic implementation within tumor sequencing programs that analyze matched germline dna is particularly efficient because there is no geno typing cost and the bioinformatic workflow to detect actionable germline phenotypes can be integrated into the existing infrastructure . 
additional work is necessary to develop infrastructure to embed active clini cal decision support into the electronic health record so that actionable phenotypes can be stored and used indefinitely.7 , 11 in conclusion , onco1700 produces reliable germline pharmacogenetic information for three clinically relevant pharmacogenes ( tpmt , dpyd , and cyp2c19 )  . 
elliott ls , henderson jc , neradilek mb , et al : clinical impact of pharmacogenetic profiling with a clinical decision support tool in polypharmacy home health patients : a prospective pilot randomized controlled trial . 
caudle ke , dunnenberger hm , freimuth rr , et al : standardizing terms for clinical pharmacogenetic test results : consensus terms from the clinical pharmacogenetics implementation consortium ( cpic )  . 
hanauer da , mei q , law j , et al : supporting information retrieval from electronic health records : a report of university of michigans nineyear experience in developing and using the electronic medical record search engine ( emerse )  . 
luzum ja , pakyz re , elsey ar , et al : the pharmacogenomics research network translational pharmacogenetics program : outcomes and metrics of pharmacogenetic implementations across diverse healthcare systems . 
ji y , skierka jm , blommel jh , et al : preemptive pharmacogenomic testing for precision medicine : a comprehensive analysis of five actionable pharmacogenomic genes using nextgeneration dna sequencing and a customized cyp2d6 genotyping cascade . 
stockley tl , oza am , berman hk , et al : molecular profiling of advanced solid tumors and patient outcomes with genotypematched clinical trials : the princess margaret impact / compact trial . 
crews kr , gaedigk a , dunnenberger hm , et al : clinical pharmacogenetics implementation consortium ( cpic ) guidelines for codeine therapy in the context of cytochrome p450 2d6 ( cyp2d6 ) genotype . 
hicks jk , bishop jr , sangkuhl k , et al : clinical pharmacogenetics implementation consortium ( cpic ) guideline for cyp2d6 and cyp2c19 genotypes and dosing of selective serotonin reuptake inhibitors . 
 retrospective survival analysis of patients with resected pancreatic ductal adenocarcinoma and a germline brca or palb2 mutation shun yu , md1 , 2 ; parul agarwal , md1 ; ronac mamtani , md1 , 2 ; heather symecko , mph2 ; kelsey spielman , ms2 ; mark ohara , md1 , 2 ; peter j . 
reiss , md1 , 2 purpose germline mutations in the homologous recombination genes brca1 , brca2 , and palb2 confer an increased risk for pancreatic ductal adenocarcinoma ( pdac )  . 
2019 by american society of clinical oncology introduction ( pdac ) adenocarcinoma pancreatic ductal a highly lethal cancer with a 5 - year overall survival rate of 9% in unselected patients , despite multimodality treatment that includes surgery , chemotherapy , and radiation.1 for patients who have undergone curative intent surgery for early - stage the perioperative therapeutic landscape pdac , is shifting ; several recent studies demonstrated improved overall survival ( os ) using specic combinations of chemotherapy and radiation in the neoadjuvant and adjuvant settings.2 - 4 however , treatment of resected pancreatic cancer has yet to be tailored to subsets of patients according to the underlying mechanism of tumor development . 
pdac that develops in the setting of a germline mutation in brca1 , brca2 , or palb2 , for example , may represent a biologically unique group that would benet from tailored perioperative management . tumors that develop in the setting of pathogenic germline mutations in the dna - repair genes brca1 , brca2 , or palb2 are well understood to have heightened sensitivity to therapies that induce doublestranded dna breaks.5 - 7 as a result of ineffective homologous recombination , the tumor cells are unable to repair the dna damage caused by such treatments , which include platinum chemotherapies , 8 and cell death results . we and others have shown with retrospective data that patients with advanced pdac and a germline mutation in brca1 , brca2 , or palb2 have improved os when exposed to platinum - based therapies , such as oxaliplatin and cisplatin.9 , 10 most recently , yurgelun et al11 published an analysis that included seven germline brca mutation carriers who had undergone resection for pdac . 
 yu et al context key objective to examine whether platinum - based chemotherapy improved outcomes for patients with surgically resected pancreatic ductal adenocarcinoma and pathogenic germline mutations in brca1 , brca2 , or palb2 . knowledge generated platinum - based chemotherapy may be associated with increased survival for patients with early - stage pancreatic ductal adenocarcinoma who have pathogenic germline brca1 , brca2 , or palb2 mutations . 
this was especially true for patients who received platinum therapy in the perioperative setting . relevance these results suggest that platinum - based perioperative chemotherapy may be preferable for patients with pancreatic cancer who have germline mutations in brca1 , brca2 , or palb2 . 
therefore , awareness of such a mutation in the early - stage disease setting may be of value . was noted that this group of patients had signicantly longer os than noncarriers overall , and this difference seemed to be enhanced when oxaliplatin therapy was delivered in the recurrent disease setting.11 collectively , these ndings are consistent with literature about other brca mutation associated cancers , such as ovarian and breast cancer.12 - 16 data to describe the effect of perioperative platinum on early - stage pdac caused by a mutation in brca or palb2 are sparse . 
patients were identied one of two ways : enrollment in the university of pennsylvania basser center for brca registry or identication via the penn medicine patient electronic medical record ( emr )  . 
the emr was mined using pennseek ( university of pennsylvania , philadelphia , pa ) , which allows for targeted keyword searches of unstructured or semistructured medical documents . notably , patients who were in the mutation - positive group were identied in both the basser registry and the emr , whereas those in the mutation - negative group were identied solely from the emr . 
data were collected and extracted using the emr , paper records , and the social security death index . patients diagnosed with nonmetastatic pdac who had resection between undergone curative intent surgical january 1 , 1995 , and march 31 , 2018 , were included . those in the mutation - positive group were dened as patients with a known pathogenic germline mutation in brca1 , brca2 , or palb2 . 
collected data included demographics ; clinical history ; personal history of prior malignancies ; family history of cancers ; pathology results at time of resection ; germline and somatic sequencing results ; and treatments related to pdac , including surgical interventions , radiation , and systemic chemotherapy . 
each patient in the mutation - positive group was matched with two patients in the mutation - negative group by stage at diagnosis , age at diagnosis , year of diagnosis , and sex . 
the institutional review board at the university of pennsylvania approved this study . os was dened as the time from the date of diagnosis of pdac to the date of death for any cause . 
the os for patients exposed to platinumbased treatments ( including cisplatin , oxaliplatin , or carboplatin ) during the course of the disease was compared with the os for patients who had not been exposed to such treatment . 
whenever possible , specic regimen details were recorded . time to progression time to progression ( ttp ) was dened as the time from the date of surgical resection to the documented date of recurrence or death . 
 survival of patients with pdac and brca or palb2 mutation platinum - based treatments in the perioperative period was compared with the ttp for patients who had not been exposed to such treatment . statistical analysis univariable analysis was performed using fishers exact test for dichotomous variables and the t test and wilcoxon rank sum test for normal and nonnormal continuous variables , respectively . 
survival curves by mutation carrier status were estimated using the kaplan - meier method and were compared using the log - rank test . in subgroup analyses , separate cox regression models examined the following a priori subgroups : patients who received no platinum therapy , patients who received platinum therapy in any setting ( adjuvant , neoadjuvant , palliative ) , and patients who received platinum only in the perioperative setting ( adjuvant or neoadjuvant )  . each patient in the mutation - positive group was matched to two patients in the mutation - negative group using a greedymatch algorithm18 without replacement on the basis of four patient factors : pathologic stage at resection , if available , or clinical stage if the former was unavailable ; age at diagnosis ; year of diagnosis ; and sex . 
during matching , stage at diagnosis was given the most weight , followed by age at diagnosis and year of diagnosis , and then followed by sex . each patient in the mutation - positive group was successfully matched to two eligible patients in the mutationnegative group . all analyzed variables were 100% complete with the exceptions of family history ( missing in 11% ) , node status ( missing in 7% ) , margin status ( missing in 11% ) , timing of germline testing ( missing in 8% ) , time to progression ( missing in 6% ) , and use of platinum therapy ( missing in 7% )  . 
all statistical analyses were performed using sas 9.4 ( sas institute , cary nc )  . results patient characteristics overall , 32 patients with pdac were identied for the mutation - positive group ( table 1 ) , and the mutational breakdown was as follows : brca1 ( n = 6 ) , brca2 ( n = 23 ) , brca1 and brca2 ( n = 1 ) , and palb2 ( n = 2 )  . 
the mean age of patients in the mutationnegative group was 60 years ( range , 44 to 85 years )  . data points were missing in both groups of patients . 
to mitigate possible bias as a result of missing data , we performed a sensitivity analysis to compare those who had missing data with those who had no missing data . 
we found no statistically signicant differences in patient age , sex , stage at diagnosis , receipt of platinum therapy , receipt of perioperative platinum therapy , ttp , or os between these groups . personal and family history of cancer fourteen patients ( 44% ) in the mutation - positive group had a personal history of a prior malignancy . 
details of these results can be found in appendix table a1 . clinical and treatment characteristics of patients all patients underwent curative - intent surgical resection ( table 2 )  . 
of these , three patients in the mutation - positive group and 10 in the mutation - negative group received perioperative infusional 5 - uorouracil , irinotecan and oxaliplatin ( folfirinox ) , whereas the remaining patients received other platinum - containing regimens . 
 ( % ) unless otherwise indicated . abbreviations : dcis , ductal carcinoma in situ ; iqr , interquartile range ; r0 , negative margin ; r1 , microscopically positive margins ; r2 , macroscopically positive margins ; sd , standard deviation . group received palliative platinum chemotherapy upon recurrence . node and margin status nodal disease was detected in 18 patients ( 72% ) in the mutation - positive group and in 50 patients ( 78% ) in the mutation - negative group ( p = .58 ; table 1 )  . 
several subgroup analyses were performed . those in the mutation - positive group had signicantly longer median os ( mos ) than those in the mutation - negative group first , patients in both groups who received platinum therapy at any time during treatment course were evaluated . 
of patients mutation negative mutation positive time ( months ) no platinum perioperative platinum + censored log - rank p = .3722 + censored log - rank p = .0193 mutation negative mutation positive mutation negative mutation positive time ( months ) no . 
 full cohort no platinum + censored log - rank p = .2557 + censored log - rank p = .5427 mutation negative mutation positive mutation negative mutation positive time ( months ) time ( months ) no . 
of patients mutation negative mutation positive platinum in any setting perioperative platinum + censored log - rank p = .0685 mutation negative mutation positive + censored log - rank p = .2134 mutation negative mutation positive yu et al no . 
time to progression of patients by mutation - positive and mutation - negative statuses : ( a ) full cohort ; ( b ) patients who received any platinum therapy ( neoadjuvant , adjuvant , or palliative ) ; ( c ) patients who received no platinum therapy ; and ( d ) patients who received platinum in the neoadjuvant or adjuvant setting . nding in the advanced cancer setting . 
however , we also observed an improvement in mos when both groups receive perioperative ( neoadjuvant , adjuvant , or both ) platinum therapya nding that , to our knowledge , has not previously been described . 
after analysis was adjusted for margin and nodal status , the mos was not reached for patients in the mutation - positive group who received perioperative platinum ( median follow - up , 22.8 months ) , whereas patients in the mutation - negative group had an mos of 23.1 months in the same setting . 
furthermore , we observed prolonged ttp for patients in the mutationpositive group who received perioperative platinum therapy compared with those who did not ; again , the median ttp was not reached in patients who received perioperative platinum therapy . chemotherapy in the curative - intent setting . 
prospective studies are required to conrm this observation . one of the key strengths of this study is that the cohort of patients with brca1 , brca2 , or palb2 mutations was matched to a cohort without these mutations according to age at diagnosis , year of diagnosis , sex , and disease stage . in addition , the multivariable model accounted for several additional variables that might have inuenced patient outcomes : nodal status at resection , margin positivity , and resectability at diagnosis . 
the resectability variable allowed control of the analysis for patients who had locally advanced disease at the time of diagnosis and who might , therefore , have inherently different outcomes compared with those whose disease was resectable at presentation . when patients in both groups did not receive perioperative platinum - based therapy , there was no signicant difference in mos . 
although the number of patients enrolled in the study was small , the results suggest that patients who are positive for mutations benet preferentially from platinum - based this study has several important limitations that should be highlighted . 
because of the small number of patients in the mutation - positive group enrolled in the study , we included all patients for whom we had survival data . third , there is the risk of a potential survival bias as a result of the timing of germline testing . 
of the 24 patients in the mutation - positive group for whom we had dates of germline testing , six had testing before the diagnosis of pdac , and the remaining 19 patients had testing at a median of 10.5 months after diagnosis ; 10 of these patients were tested in the perioperative period , and nine were tested after disease recurrence . 
we are unable to account for this bias in this retrospective study because of the small number of tested patients in the mutationnegative group , which highlights the need for prospective studies . finally , the mutation - negative group may have inadvertently contained patients who were brca or palb2 carriers . 
however , this would have plausibly biased results toward the null hypothesis . these ndings are hypothesis generating only , but they may have several potential implications within the current neoadjuvant and adjuvant therapy treatment landscape . we observed a trend toward improved ttp and a signicantly longer mos in patients in the mutation - positive group who were treated with platinum chemotherapy in the perioperative setting . 
importantly , recent data from hu et al19 demonstrate that a substantial portion of patients who are positive for mutations do not have the classic clinical features associated with genetic syndromes , such as a positive family history or personal history of cancer . therefore , using an all - comer approach of early testing for patients with pdac seems rational and may improve outcomes for those who carry a pathogenic homologous recombination mutation . second , recent data from conroy et al3 have shown a substantial os benet in patients with resected pdac when adjuvant modied folfirinox , compared with gemcitabine therapy , is used.3 however , because of its substantial toxicities , folfirinox must be reserved for patients who have a robust performance status . 
at this time , patients who have undergone curative - intent surgery but who are not well enough to receive folfirinox do not have a dened course , and many are likely to receive nonplatinum treatments , such as gemcitabine plus capecitabine2 or gemcitabine plus nab - paclitaxel . 
given the nding that platinum - based perioperative therapy may preferentially benet patients who have a positive mutation status , chemotherapy combinations , such as cisplatin plus gemcitabine or infusional uorouracil , leucovorin , and oxaliplatin , might be preferable for these patients if folfirinox cannot be used . in conclusion , we present a small cohort study in which we observed an os benet when patients with resected pdac and a brca or palb2 mutation received platinum therapy in the perioperative setting . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . ronac mamtani consulting or advisory role : genentech , roche mark o ' hara consulting or advisory role : karyopharm therapeutics travel , accommodations , expenses : astrazeneca / medimmune peter j . 
o ' dwyer consulting or advisory role : genentech , bristol - myers squibb , boehringer ingelheim research funding : bristol - myers squibb , pzer , novartis , genentech , mirati therapeutics , celgene , glaxosmithkline , bbi healthcare , merck , pharmacyclics , bayer , five prime therapeutics , forty seven , amgen susan m . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) kim a . 
reiss research funding : lilly ( inst ) , clovis oncology ( inst ) , bristol - myers squibb ( inst ) , tesaro ( inst ) no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
neoptolemos jp , palmer dh , ghaneh p , et al : comparison of adjuvant gemcitabine and capecitabine with gemcitabine monotherapy in patients with resected pancreatic cancer ( espac - 4 ) : a multicentre , open - label , randomised , phase 3 trial . 
j clin oncol 36 , 2018 ( suppl ; abstr lba4001 ) van tienhoven g , versteijne e , suker m , et al : preoperative chemoradiotherapy versus immediate surgery for resectable and borderline resectable pancreatic cancer ( preopanc - 1 ) : a randomized , controlled , multicenter phase iii trial . 
genet med 17 : 569 - 577 , 2015 dann rb , deloia ja , timms km , et al : brca1 / 2 mutations and expression : response to platinum chemotherapy in patients with advanced stage epithelial ovarian cancer . 
mol cell 7 : 263 - 272 , 2001 golan t , kanji zs , epelbaum r , et al : overall survival and clinical characteristics of pancreatic cancer in brca mutation carriers . 
yurgelun mb , chittenden ab , morales - oyarvide v , et al : germline cancer susceptibility gene variants , somatic second hits , and survival outcomes in patients with resected pancreatic cancer . 
genet med 21 : 213 - 223 , 2018 isakoff sj , mayer el , he l , et al : tbcrc009 : a multicenter phase ii clinical trial of platinum monotherapy with biomarker assessment in metastatic triplenegative breast cancer . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
 ( % ) variable timing of germline testing before diagnosis during perioperative period at recurrence somatic brca testing ( controls only ) germline testing results ( controls only ) negative variant of uncertain signicance non - brca pathogenic mutation note . 
one is the growing recognition that complex diseases such as cancer are multifactorial and may be attributed to harmful changes on multiple - omics levels and on the pathway level . 
when individual genes in an important pathway have relatively weak signals , it can be challenging to detect them on their own , but the aggregated signal in the pathway can be considerably stronger and hence easier to detect with the same sample size . 
to address these challenges , there is a growing body of literature on knowledge - guided statistical learning methods for analysis of high - dimensional - omics data that can incorporate biological knowledge such as functional genomics and functional proteomics . 
2019 by american society of clinical oncology introduction rapid advances in technologies have led to generation of high - dimensional - omics data , such as genomics , transcriptomics , and metabolomics data , in many biomedical studies . 
they have been used to build prediction models for disease risk or progression and for adaptive response to treatment , uncover molecular signatures associated with a disease that provide insights about disease mechanism , and identify potential therapeutic targets . 
in particular , they achieve simultaneous variable selection and model estimation and can be used to analyze data where the sample size is less than the number of - omics features . 
for example , when expression levels of individual genes in an important pathway associated with cancer risk have relatively weak signals , it can be challenging to detect them on their own , but the aggregated signal in the pathway can be considerably stronger and hence easier to detect with the same sample size . 
the vast majority of existing statistical learning methods are entirely data driven and fail to incorporate biological knowledge such as functional genomics and functional proteomics that can be represented by a graph ( table 1 )  . extensive research in the past has yielded everfunctions of deepening knowledge of biological genes and gene products , which have been shown to function through pathways and networks . 
 zhao , chang , and long context key objective to review advances in knowledge - guided statistical learning methods for analysis of - omics data and spur wider and more frequent applications of such methods in basic , translational , and clinical research toward the goal of advancing precision oncology . knowledge generated the knowledge - guided analysis strategy offers a number of advantages . 
the strategy can also facilitate the integration of multimodal - omics data through the incorporation of biological knowledge about the functional relationship between different modalities . relevance knowledge - guided statistical learning methods can be used to construct accurate models for predicting cancer risk , prognosis , and response ; uncover molecular signatures that are predictive of cancer risk , disease progression , or patient response to treatment , which can inform novel targets for therapeutic development ; and identify cancer subtypes related to molecular differences , which offers insights about optimizing treatment strategy for each subtype , an important step toward precision oncology . associated with disease risk or progression . 
in addition , a two - step approach , 22 conducting clustering analysis followed by annotating clusters by a gene set enrichment analysis , has been shown to improve power in clustering analysis of gene expression data . 
similar biological knowledge is also available for other types of - omics data , and table 1 lists representative databases for such biological knowledge . recent methodologic research23 - 25 has also provided strong evidence about the advantages of knowledgeguided statistical learning methods that can incorporate the aforementioned biological knowledge , compared with statistical learning methods that do not use such biological knowledge . 
knowledge - guided statistical learning methods enable selection of important pathways instead of individual - omics features and improve power in uncovering important features , particularly those with weak signals . 
in addition , such a strategy can also facilitate the integration of multimodal - omics data through the incorporation of biological knowledge about the functional relationship between different modalities ( eg , expression quantitative trait loci and metabolomic quantitative trait loci )  . 
as such , this knowledge - guided data - driven approach is particularly powerful and useful for analysis of - omics data in complex diseases such as cancer . knowledge - guided statistical learning methods have wide applications in precision medicine , including precision oncology . 
the knowledge - guided supervised learning methods can be used to construct prediction models for disease risk and prognosis , which can then be used to identify higher risk groups more accurately and tailor interventions to individual patients.26 they can also be used to uncover molecular signatures that are predictive of disease risk , disease progression , or patient response to treatment , which can inform novel targets for therapeutic development . 
the knowledge - guided unsupervised learning methods , such as biclustering , can be used to identify disease subgroups and important pathways associated with each subgroup.27 identication of subgroups related to molecular differences offers insights about optimizing treatment strategy for each subgroup and is an important step toward developing a precision medicine approach for complex diseases such as cancer . in this review , we survey advances in knowledge - guided statistical learning methods for analysis of highdimensional - omics data in precision medicine , many of which have been applied to analysis of cancer data . 
representative databases for various types of biological knowledge database full name knowledge kyoto encyclopedia of genes and genomes2 metabolic pathways reactome pathway database3 metabolic and signaling pathways mummichog mummichog4 metacyc metabolic pathways from all domains of life6 invitrogen ipath invitrogen ipath7 metabolomic pathway metabolic pathways metabolic pathways ingenuity pathways knowledge base8 gene regulatory and signaling pathways biocyc pathway / genome database collection9 metabolic pathways transpath transpath10 gene regulatory and signaling pathways cell signaling technology pathway11 signaling pathways targetscan12 mirbase : the microrna database13 gene - microrna regulatory network gene - microrna regulatory network probabilistic identication of combinations of target sites14 gene - microrna regulatory network mirdb15 microrna data integration portal16 gene - microrna regulatory network gene - microrna regulatory network biological general repository for interaction datasets17 protein and genetic interactions kegg reactome ipkb biocyc targetscan mirbase pictar mirdb mirdip biogrid consensuspathdb consensuspathdb18 integrative database for molecular interactions and certain clinical outcomes . 
depending on the type of clinical outcomes , methods have been proposed to handle binary data ( eg , the disease status ) , continuous data ( eg , time to death ) , categorical data ( eg , cancer subtypes ) , and censored data ( eg , time to cancer recurrence )  . 
through this learning procedure , we can identify important genomic features that are highly associated with clinical end points , build a prediction rule that will be crucial for future clinical practice , or even achieve both simultaneously . 
correspondingly , prior biological or structure knowledge is supposed to be incorporated within feature selection or the prediction process to rene the model for a more accurate and interpretable result . x : - omics predictors yi = xi + ei biological knowledge g = < v , e > penalty for ( frequentist ) prior for ( bayesian ) fig 1 . 
knowledge - guided linear regression model where y is the clinical outcome of interest and x is the set of high - dimensional - omics features or predictors , and g = , v , e . 
is the graph containing the biological knowledge about - omics predictors with v denoting the set of nodes ( ie , - omics features ) and e denoting the set of edges . 
to incorporate g = , v , e . , a penalty for is used in a frequentist framework , and a prior distribution for is used in a bayesian framework . for ease of illustration , we introduce a few notations without loss of generality . 
suppose a study recruits n patients with an outcome of interest ( eg , disease status ) and p predictors ( ie , confounders and genomics features ) collected for each patient . 
the existing biological knowledge ( eg , pathway information , gene - gene network ) among predictors is represented as a direct or indirect graph among genomics features , denoted as g . 
figure 1 provides an example of a knowledge - guided linear regression model in both the frequentist and bayesian frameworks . the main distinction between the frequentist and bayesian approaches is their view on probability . short , frequentist approaches try to solve the exact value of probability on the basis of the event they observed , whereas bayesian methods do not assume there is xed probability of the event but treat this probability itself also as randoin terms of model tting , frequentist models do not assign prior distribution for the unknown parameters and eventually end up with a point estimate for them , whereas bayesian models need such a prespecied prior and produce a posterior distribution for each parameter . 
 zhao , chang , and long results in their differences in how to incorporate biological knowledge , computation , and interpretation of analysis results . frequentist approach the majority of knowledge - guided frequentist methods for analysis of high - dimensional - omics data are based on a regression framework to study the association between - omics features x and an outcome of interest y [ ie , y f ( x , ) ] , with being the set of p unknown regression coefcients to be estimated . 
to induce the regression coefcients , sparsity or shrinkage for a penalty function , p ( ) , is often introduced , leading to the so - called penalized regression . in the case where biological knowledge among predictors x is available and can be represented by a graph g , we can also use p ( ) to incorporate such biological knowledge ( fig 1 )  . 
specically , when there is an edge between features i and j in g , a common strategy is to induce similar shrinkage effects between their corresponding parameters i and j . the work of li and li23 represents one of the earliest attempts to incorporate gene network information into feature selection for cancer genomics application . 
to incorporate the pathway information in kegg , they proposed a network - constrained penalty on the the following two assumptions : rst , genes basis of connected by an edge have similar functions and , therefore , are expected to have smoothed regression parameters ; and second , the connected genes have higher probability to be selected or not selected simultaneously . 
the penalty itself consists of an l1 - norm to achieve global sparsity as the usual penalization procedure does , as well as a quadratic form on the network laplacian matrix to induce smoothness across the biological graph . 
using this method , they identied gene subnetworks that were highly correlated with survival time of patients with glioblastoma ( see fig 2 in the article by li and li23 ) , and some of these subnetworks were not identied by other existing learning methods that did not use pathway information . 
although some of the subnetworks were supported by previously published work , some have not been reported in the literature , and these novel gene signatures can inform the molecular underpinnings of glioblastoma prognosis or even novel targets for therapeutic development . after li and li , 23 a number of extensions have been proposed . 
to handle binary outcome , zhang et al28 adopted the network - constrained penalty under a logistic regression model that was used to predict a specic breast cancer subtype on the basis of gene expression data from the cancer genome atlas ( tcga ) consortium while incorporating protein - protein interactions . 
their method was applied to a breast cancer study to identify genes and subnetworks that are predictive of survival while incorporating biologic network from kegg . besides extensions to handle different outcome types , pan et al24 proposed a new penalty on the basis of lrnorit reduces the computational costs with a smaller number of tuning parameters and allows two connected genes to both upand downregulate one anothers expression while maintaining the grouping effect . 
a few subsequent extensions include those by kim et al30 to modify the penalty by removing the constraint of a similar magnitude of the connected biomarkers , which is biologically more meaningful , and tian et al31 to use a multinomial logit model for cancer subtype prediction . overall , these works focus on incorporating individuallevel relationships between - omics biomarkers under the assumption that connected biomarkers are more likely to affect clinical outcome in a coordinated way . more recently , for analysis of gene and microrna biomarkers , zhao et al26 proposed a hierarchical group penalty , which incorporates pathway membership , gene network , and microrna - gene regulatory network information into a semiparametric accelerated failure time model to predict prostate cancer recurrence after surgery . 
compared with previous works , hierarchical group penalty further allows a group - level sparsity ( ie , genes in the same pathway are also more likely to be associated or not associated with clinical outcome at the same time )  . 
zhao et al26 were among the rst to include both group - level membership and within - group connectivity and induce sparsity at both the pathway level and gene level . 
the article by zhao et al26 treats the unknown component of the biological graph as missing data and proposes a multiple - imputation approach for handling missing edges in the graph . 
 knowledge - guided statistical learning methods for - omics data for both methods , similar to the regression setting , biological knowledge represented by graph is incorporated into the model using penalty functions , where the sparsity and grouping effects are also expected . 
the knowledgeguided svm has been used to predict clinical outcome of patients with glioblastoma using genomic biomarkers.32 bayesian approach although frequentist models are traditionally considered canonical , bayesian approaches have attracted increasing interest in recent years as a result of their ease in incorporating prior information and quantifying uncertainty . as such , they have played an important role in the development of knowledge - guided supervised learning methods . when analyzing high - dimensional - omics data , prior distributions that lead to variable selection or shrinkage are used in a bayesian model to improve prediction and identify important features . 
there is an extensive body of literature on bayesian variable selection.34 different from variable selection achieved through a penalty in a frequentist paradigm , bayesian variable selection can be achieved in two ways , namely , selection on the basis of a point - mass mixture prior or regularization through a shrinkage prior . the former35 directly includes or excludes a predictor in the model by introducing a binary selection indicator . 
the downside with a shrinkage prior is that it does not directly provide results on feature selection ; in addition , a subsequent truncation step , often ad hoc , is required to obtain the nal set of selected predictors . similar to existing frequentist methods , the majority of knowledge - guided bayesian supervised learning methods are developed for regression models . 
as an extension of the work by li and zhang , 37 stingo et al39 proposed a bayesian hierarchical variable selection regression model incorporating both pathway membership and gene network information with application to breast cancer microarray data . 
zhe et al40 tackled the following limitation of the method from stingo et al39 : all the pathways that a selected gene belongs to are also selected , which is overly restrictive and may not always be meaningful . 
to remove this restriction as well as reduce the computation , they proposed a bayesian joint pathway and gene selection model that uses a graph laplacian matrix to encode biological knowledge and a variational bayesian algorithm for model estimation . 
the analyses of a gene expression data set using their method yielded a more accurate prediction model for survival time in palymphoma than several tients with diffuse large b - cell existing learning methods that did not use biological information . beyond genomics , zhang et al41 analyzed molecular inversion probe data to identify genes and probes that are associated with clinically relevant subtypes of breast cancer . 
their method uses information on biological grouping of gene and probe - within - gene levels to dene a hierarchical selection procedure through a point - mass mixture prior for gene selection and a shrinkage prior for probe selection . 
as the dimension of - omics data increases , there is a growing interest in using bayesian shrinkage priors for knowledge - guided variable selection and prediction as a result of potential computational savings . 
rockova and lesaffre42 developed a bayesian model for hierarchical feature selection at the pathway level and gene level on the basis of bayesian lasso.36 subsequently , chang et al25 developed a novel adaptive structured shrinkage prior to incorporate biological knowledge in a bayesian regression model . 
in general , with the computational advantage of the bayesian shrinkage prior , this research direction is expected to become even more active for analysis of large - scale - omics data . besides regression , knowledge - guided bayesian methods have also been developed for discriminant analysis44 and svm45 for analysis of high - dimensional genomics data . 
unsupervised learning methods are typically used as a data mining approach to help explore and visualize large - scale data ; see chapter 14 in hastie et al.1 the existing knowledge - guided unsupervised learning methods have been focused in two areas , namely , clustering analysis and dimension reduction , for which either a frequentist or a bayesian approach can be used . clustering analysis the goal of clustering analysis is to group patients on the basis of their similarities in , for example , genomic features . in terms of application to cancer - omics , clustering analysis has been widely used to uncover cancer subtypes , which is essential to understand tumor heterogeneity and optimize prevention and treatment strategy accordingly . 
they mainly used the number of edges connected with each gene to dene weights in the clustering procedure . recently , more advanced integrative clustering methods have been proposed to jointly analyze multimodality cancer - omics data while incorporating biological information . 
their method is able to jointly handle different data types ( continuous and discrete ) , which is well suited to analyze multiomics data sets in cancer , including gene expression , copy number , rna sequencing , and single nucleotide polymorphisto incorporate biological knowledge , a bayesian adaptive structured shrinkage prior is placed on the factor loading matrix , which encourages the - omics features connected in a graph to have zero or nonzero loading simultaneously in the same factor . 
to reduce heavy computation , they developed an efcient variational expectation - maximization algorithm for estimation , making their method scalable to the analysis of high - dimensional - omics data . dimension reduction dimension reduction methods can be used to project highdimensional - omics features into a lower dimension space either to better understand or visualize the data structure or to facilitate assessing dependence between two sets of ( cid : 129 ) ( cid : 129 ) ( cid : 129 ) subtypes identified in wz prior for z : ( zli ) exp ( |zli| ) prior for w : ( wjl ) exp ( |wjl| ) prior for : l l ~ ln ( , g ) biological knowledge : g = < v , e > insights on subtypes and molecular signatures prediction ( cid : 129 ) ( cid : 129 ) ( cid : 129 ) ( cid : 129 ) ( cid : 129 ) ( cid : 129 ) fig 2 . 
this method was used to conduct biclustering analysis of gene expression data , dna methylation data , and dna copy number data from a glioblastoma data set from the cancer genome atlas . 
li et al27 incorporated biological knowledge into the sparse principal component analysis , a popular dimension reduction tool for high - dimensional data , to identify genes associated with glioblastoma cancer subtypes . 
they extended and investigated two networkbased penalties , the grouped penalty by pan et al24 and the fused lasso penalty by tibshirani et al.50 the resulting sparse principal component analysis algorithm is able to incorporate biological network information in the principal component loadings and achieve more accurate and biologically meaningful dimension reduction . 
similarly , biologic knowledge has also been incorporated into the canonical correlation analysis51 and the coinertia analysis ( cia ) 52 for assessing dependence between two - omics data sets . 
applied to analysis of gene expression data and protein abundance data in the nci - 60 cell line data set , the knowledge - guided cia52 method was able to project the high - dimensional - omics feature to a lower dimensional space in which the 10 different types of cancers were clearly separated ( see fig 1 in article by min et al52 )  . 
of note , both canonical correlation analysis and cia are popular multivariate statistical methods for integrative analysis and have become popular in analysis of multimodality - omics data in cancer studies . in addition , liu et al53 developed a knowledge - guided approach to use expression data and coexpression network information to improve de novo discovery of driver pathways in cancer on the basis of mutation data . 
analyses of three cancer data sets using their method revealed new driver pathways that were not uncovered by other methods including , particularly , driver genes with less frequent mutations that are much more difcult to detect . 
these new driver pathways may offer insights about cancer biology and inform novel targets for screening and for therapeutic development . discussion statistical learning methods have been proven powerful for analysis of high - dimensional - omics data in modern biomedical research but have some important limitations . 
to address these limitations , the knowledge - guided strategy , as reviewed here , has drawn increasing interest in recent years and has been shown to yield biologically more interpretable and meaningful results . 
software tools for many of the methods reviewed earlier have been made publicly available ( table 2 )  . knowledge - guided statistical although substantial progress has been made in the delearning velopment methods , there is still much room for additional methodologic developments and improvements . 
one area for future research is to assess robustness of knowledgeguided methods to mis - specication of biological knowledge , because in practice , biological knowledge represented by a graph g is known to be incomplete and include table 2 . 
existing work27 has demonstrated that some knowledge - guided supervised learning methods are fairly robust to mis - specied biological knowledge g , but more research is needed for other types of statistical learning methods . 
to further enhance robustness , it is also of signicant interest to combine knowledge - guided methods with learning biological knowledge graphs from observed data , for which there is little research besides that by zhao et al.26 in addition , most of the existing knowledge - guided bayesian methods may not be scalable to analysis of big - omics data that can have hundreds of thousands or even millions of features , and more research on efcient computation algorithms is needed . although knowledge - guided statistical learning methods have drawn growing interest in methodologic communities , this review will they have not been widely used by cancer researchers , and the ndings from the methods publications reviewed in this article largely remain to be validated in subsequent studies . 
our hope is that raise the awareness and spur wider and more frequent applications of knowledge - guided methods in basic , transto advance lational , and clinical precision medicine , particularly for complex diseases such as cancer . 
nucleic acids res 28 : 27 - 30 , 2000 croft d , okelly g , wu g , et al : reactome : a database of reactions , pathways and biological processes . 
subramanian a , tamayo p , mootha vk , et al : gene set enrichment analysis : a knowledge - based approach for interpreting genome - wide expression proles . proc natl acad sci usa 102 : 15545 - 15550 , 2005 23 . 
zhao y , chung m , johnson ba , et al : hierarchical feature selection incorporating known and novel biological information : identifying genomic features related to prostate cancer recurrence . 
stingo fc , chen ya , tadesse mg , et al : incorporating biological information into linear models : a bayesian approach to the selection of pathways and genes . ann appl stat 5 : 1978 - 2002 , 2011 40 . 
polley , phd1 and ying kuen cheung , phd2 applications in early - phase cancer trials have motivated the development of many statistical designs since the late 1980s , including dose - nding methods , futility screening , treatment selection , and early stopping rules . these methods are often proposed to address the conventional cytotoxic therapeutics for neoplastic diseases and cancer . 
recent advances in precision medicine have motivated novel trial designs , most notably the idea of master protocol ( eg , platform trial , basket trial , umbrella trial , n - of - 1 trial ) , for the evaluation of molecularly targeted cancer therapies . 
in this article , we review the concepts and methodology of early - phase cancer trial designs with a focus on dose nding and treatment screening and put these methods in the context of platform trials of molecularly targeted cancer therapies . 
tumors once thought to be of the same histologic type may now be considered heterogeneous and differentiated on the basis of genomic biomarkers and may be treated differently according to the biomarker expression prole . 
because the subject subgroups dened by specic genetic abnormalities of the tumors may only represent a small fraction of the disease population , the concept of precision oncology trials for targeted therapies has created enormous challenges in recruiting patients with rare genomic subtypes . 
this recruitment challenge , coupled with the need to test multiple targeted therapies in relatively small molecularly dened patient subgroups in an efcient manner , has led to the rethinking of cancer drug development paradigto meet these challenges , the concept of master protocols has been introduced to increase the speed of oncologic therapy development and evaluation . 
the main goal of constructing a master protocol is to enable sharing of operational infrastructure and key design elements across substudies so as to achieve better coordination and efciency than can be achieved in single trials designed and conducted independently in biomarker - dened subpopulations.1 - 5 a platform trial is a randomized trial in a single histology that involves multiple treatments and multiple biomarkers under a master protocol . 
instead , rather than presuming we know which therapy is appropriate for which biomarker stratum , randomization is used for treatment assignment within each biomarker stratutable 1 gives a schema of biomarker - based inclusion criteria in a hypothetical platform trial . 
 polley and cheung context key objective this article provides a critical review of early - phase cancer trial statistical methods and discusses their practicality under the novel platform trial paradigm for evaluating molecularly targeted therapies . knowledge generated although many trial design principles for cytotoxic agents still hold relevance for molecularly targeted therapies , new design and analysis issues , including delayed toxicities and efcacy - tolerability trade - offs , should be considered when designing studies involving these agents . 
early - phase platform trials facilitate efciency gains by allowing within - trial information sharing of safety and efcacy data . relevance this article provides a practical guide for early - phase platform trial designs in the era of precision medicine . 
novel statistical methods continue to be needed to harness the information garnered in these new - generation trial designs to help expedite oncologic drug development and approval . for neoadjuvant therapeutic response with imaging and molecular treatment of analysis 2 ( i - spy2 ) trial women with locally advanced breast cancer.8 , 9 methodologic innovations in a platform trial may include midtrial outcome - adaptive randomization to favor treatments with higher response rates within the respective biomarkerdened stratum.10 , 11 the treatment effects of various experimental therapies are often estimated according to a bayesian hierarchical model by borrowing outcome information across molecularly dened biomarker subgroups.10 , 11 at the same time , bayesian decision rules may be incorporated to determine when and whether therapies with low probabilities of success should be discontinued and therapies with high probabilities of future success should advance to subsequent conrmatory studies ; in this way , novel therapies may be added or dropped in a perpetual manner.10 , 12 , 13 because of the need for midtrial adaptations , platform trials often use short - term end points , such as absence of disease progression at 8 weeks ( as in battle ) or pathologically conrmed complete response ( as in i - spy2 )  . 
although the bayesian inferential structure provides a convenient and efcient framework for analysis , it does not protect the type i error rate against multiple comparisons in the conventional sense . 
as such , phase ii platform trials are generally regarded as exploratory , and positive ndings from these trials will require independent conrmation for the promising drug - biomarker stratum in subsequent phase iii trials . cancer trial designs have been well established for cytotoxic agents . 
specically , phase i trials are dose - nding studies that examine safety of the drug and estimate the maximum - tolerated dose ( mtd ) , 14 and phase ii trials are designed to screen new drugs on the basis of pilot efcacy such as clinical response.15 , 16 the general objective of early - phase cancer trials is to identify and recommend a promising dose regimen of a new agent for conrmatory investigation in multicenter phase iii randomized clinical trials . 
the rationale for using toxicity as a surrogate for efcacy can be traced back to the suggestion of using nitrogen mustards in the treatment of neoplastic diseases in the 1960s.18 the most commonly used statistical design for a phase i oncology dose - nding trial is the 3 + 3 design . 
this is a rulebased design in which the number of dose levels is xed in advance and the dose escalation or de - escalation decision is based on the number of dlts that patients experience at a given dose . 
the 3 + 3 design has received extensive examinations and has been demonstrated to produce poor statistical properties , including treating many patients at doses that are below the biologically active level and imprecise estimation of dlt probability because of the relatively small number ( three to six ) of patients treated at each dose cohort.19 - 21 to address the deciencies of the 3 + 3 design , many dosending designs have been proposed since the 1990s that purport to improve statistical accuracy and trial efciency in the context of chemotherapy trials.22 the most prominent work among these is an adaptive design known as the continual reassessment method ( crm ) .23 , 24 the crm uses a mathematical model to relate the dose levels to the probability of dlt . 
after the rst patient has been treated at the dose determined by the initial dose - toxicity curve , the toxicity information is combined statistically with the initial curve , and an updated dose - toxicity curve is estimated using a bayesian methodology . 
the crm has been shown to improve the precision in estimating the mtd and to increase the number of patients assigned to the selected mtd when compared with the standard 3 + 3 method.25 - 27 the latter property has important ethical implications because traditional methods will likely treat many patients at low and , hence , inefcacious the crm fullls the therapeutic doses . purpose of phase i cancer trials , which are often the last resort of the patients who have exhausted other alternative treatment options . 
during its early inception , the crm drew some criticisms particularly with regard to the possibility of exposing patients to doses that are likely to cause dlt.28 , 29 to address these concerns , several trials used a hybrid approach that combined the model - based crm with a rulebased initial dose - escalation plan ( clinicaltrial.gov identiers : nct03141203 , nct03733990 , and nct03028766 ) .28 - 31 in this regard , once an mtd is identied , a new chemotherapy will be studied in phase ii trials , which are proof - of - concept studies looking for early indication of antitumor activity . 
this objective is often achieved with a single - arm trial design using clinical response as an end point , with the possibility of stopping a trial early as a result of futility.16 , 23 , 32 , 33 for instance , to have 80% statistical power to reject a 25% response rate in favor of a 45% response rate of a new drug at 5% signicance , a single - arm , xed - sample size trial will need to enroll 36 patients and seek to observe 14 responses in the enrolled patients . 
alternatively , a simon two - stage design16 will rst enroll 17 patients and then enroll an additional 24 patients ( ie , a total of 41 patients ) only if there are at least six responses in the rst 17 patients . 
because of the provision for futility stopping , the simon design will , on average , treat fewer patients with inefcacious drugs , thus allocating resources to the more promising ones . 
however , to demonstrate promise of a new drug , an adaptive design with futility stopping will always require a larger maximum sample size than a xed trial ( as in the example just provided )  . 
a participant with a given biomarker is eligible for random assignment to a drug and dose among those marked by a checkmark , which indicates that the drug is a candidate for the biomarker and that the dose does not exceed the maximum - tolerated dose . 
these noncytotoxic agents tend to induce long - lasting mild toxicities , and hence , the assumption of acute toxicities may not apply.35 for some agents , prolonged administration may be required to achieve desirable therapeutic benet , thus increasing the likelihood of late - onset or cumulative toxicities that may manifest many months after the initiation of treatment . 
therefore , for phase i trials of targeted therapies , it is critical to identify the mtd with respect to a longer observation window , so as to ensure future investigations are limited to a tolerated dose range . the 3 + 3 design and crm - type designs dictate that accrual of new patients be suspended until all enrolled patients have been fully evaluated for dlt . 
when delayed toxicities are anticipated , the trial length may be prohibitively long because of the need for frequent accrual suspension and the lengthy dlt observation window.36 , 37 a dose - nding design that does not require suspension of patient accrual while waiting for dlt information on previously treated patients to mature is the time - to - event continual reassessment method ( titecrm ) .38 the dose allocation scheme of the tite - crm follows closely the original crm paradigm but additionally leverages the time - to - toxicity and partial follow - up information in all enrolled patients when estimating the mtd . 
since its introduction , the tite - crm design has been successfully implemented in trials at major academic cancer centers , 39 - 48 as well as us national cancer institutesponsored cooperative groups trials such as radiation therapy oncology group 0813 trial ( clinicaltrials.gov identier : nct00750269 )  . in situations where patients become available to a trial at a rapid rate , the tite - crm could accrue many patients at a given dose level before anyone has been observed for a meaningfully long period . 
therefore , it may be useful to impose a waiting window between cohorts of patients , so as to allow adequate follow - up before adaptation is made.49 - 51 tolerability and efcacy trade - off for molecularly targeted agents and immunotherapies , it may not be adequate to only consider toxicity and tolerability in a dose - nding trial . 
second , a higher dose of a new compound may be less efcacious than a lower dose52 or may see limited benets on the basis of considerations of pharmacokinetic properties.53 hence , the mtd may not be an ideal recommended phase ii dose , although it is still useful to dene the upper safety limit by the mtd . 
third , dlts may not be observed with these agents , and mtd may not be determined at the conclusion of dose escalation.54 , 55 these are the scenarios where both toxicity and activity end points should be used to guide dose recommendations.54 , 55 yan et al56 proposed an adaptive bayesian phase i / ii efftox design that guides dose selection on the basis of the tradeoffs between the probabilities of treatment toxicity and efcacy . 
paoletti and postel - vinay55 discussed the ideal setting for the efftox design and contended that such design is best suited when a homogeneous disease population is well - dened for drug sensitivity and an early biomarker for efcacy is available . 
houede et al57 model clinical utilities on the basis of both toxicity and clinical response in a combination therapy trial , which aims to choose the optimal dose pair of a chemotherapy and a biologic agent . finally , li et al58 proposed an approach to identify the best drug at an efcacious and safe dose for a given biomarker subtype in an early - phase platform trial . 
as cancer trials increasingly focus on combination therapies , it is critical to leverage efcacy information as well as toxicity in dosing decisions . treatment screening in a randomized platform trial in a single - arm , proof - of - concept trial , the interpretation of the results and conclusion of the trial depend on the specication of what would constitute a poor ( null ) response rate on the basis of historical data or a priori clinical experience . 
although response dened by tumor shrinkage is an indicator of activity for cytotoxic drugs , progression - free survival ( pfs ) may be more appropriate for early indication of efcacy of a targeted therapy whose mechanism does not necessarily shrink tumors . 
pfs is a less specic end point than tumor shrinkage because untreated patients may survive without progression for a period of time , whereas patients not treated with chemotherapy are unlikely to experience response . 
furthermore , as precision medicine challenges the fundamental assumption of tumor homogeneity , the appropriate null response rate may vary with biomarker expression . in a platform trial where several drugs are considered for a biomarker subtype ( table 1 ) , drug screening can be based on randomized comparison and ranking , thereby eliminating some subjectivity in choosing a null response rate . 
others have proposed adaptive screening strategies such as a two - stage design , 60 , 61 whereby the rst screening stage aims to select a promising drug among several for additional evaluation , and continuous monitoring using the sequential probability ratio test.62 these innovative adaptive designs have been shown to increase the nal dose selection accuracy while treating more patients with better drugs during the trial and can accommodate situations where there is a concurrent standard therapy . 
indeed , the infrastructure developed under a master protocol , in conjunction with the use of these innovative adaptive designs , facilitates unbiased randomized comparisons of potential drug candidates in a platform trial in a timely and efcient manner . pooling information across subtypes in a platform trial in an early - phase platform trial , where a drug may be given to patients across biomarker subtypes , the safety prole of the drug can be evaluated using pooled information across subgroups . 
specically , it is often reasonable to assume there is a common mtd for all biomarker subtypes when the biomarker is agnostic to adverse reactions to the drug.58 the concept of combining toxicity information from different diseases is not new , because phase i cancer trials of chemotherapy are often conducted in patients with heterogeneous malignancies ( eg , solid tumors )  . 
however , implementing this concept in the context of a platform trial provides much needed relevant safety information of the drug in patients with rare biomarker subtypes . when assessing a drugs efcacy in a given biomarker subtype , a statistically unbiased approach is to consider the observed response or pfs rate using only data of patients with that subtype . 
this analytical approach may make it difcult to understand the drugs effect in rare biomarker subtypes . is that a potential advantage of running a platform trial a targeted therapys efcacy for a given biomarker can potentially be analyzed based on its efcacy in other subtypes of the same histology , when the drug is hypothesized to work through a common molecular mechanism in all subtypes . 
 polley and cheung this analysis adds another level in the hierarchy of bayesian analysis , it is called hierarchical bayesian modeling ( hbm )  . several authors have examined and proposed the use of hbm in platform trials.58 , 63 , 64 it has been noted that borrowing information using hbm can be counterproductive when the drugs effects vary across biomarker subtypes.63 this is conceivable when a drug has nonspecic anticancer activity that is not specic to the molecule . 
although ongoing work has been suggested to model multiple sources of exchangeable drug effects in conjunction with hbm , 64 it is critical to evaluate the clinical situations as to whether there is a strong reason for expecting a common drug effect across subgroups . discussion there are many potential efciency gains associated with a platform trial.2 , 5 first , the use of a common genomic screening platform to identify patients eligible for the trial often results in shorter recruitment time and lower screen failure rate . 
second , the use of centralized governance bodies under a master protocol ( eg , the scientic review committee , institutional review board , or data and safety monitoring committee ) can ensure streamlined and efcient oversight for all substudies . 
for example , the trial innovation network represents a collaborative national network that aims to enhance operational efciency by leveraging the resources and expertise of the clinical and translational science award.65 third , the speed of drug development and evaluation is improved by the common infrastructure that allows opening or closure of substudies of new agents and biomarkers more expeditiously . other related trial designs for biomarker - based cancer drug development under the broad denition of a master protocol include basket trials and umbrella trials.1 , 3 , 4 a basket trial evaluates a targeted therapy on multiple disease subtypes ; specically , each basket evaluates the therapeutic effect of a targeted therapy for several cancer types that have a common molecular biomarker or genetic alteration . 
basket trials are typically nonrandomized ; on the basis of a prespecied genetic alteration , patients are assigned to a regimen that is expected to be active for their tumor . 
these biomarker - dening strata may be single - arm phase ii or phase ii / iii trials that randomly assign patients to either the matched targeted therapy or some standard therapy ( or placebo )  . 
an example of an umbrella trial is the adjuvant lung cancer enrichment marker identication and sequencing trial ( alchemist ) for early - stage nonsmall - cell lung cancer.66 although these novel trials provide a platform to answer clinical questions that traditional clinical trial design may not afford , it is important to appreciate that these gains are accompanied by increased logistical challenges and coordination efforts.67 for example , a platform trial requires tremendous resources and time commitment to establish the common trial infrastructure . 
often , a platform trial would involve multiple agents developed by different industry partners ; the contract negotiation with multiple stakeholders in terms of data sharing or coordination across substudies will likely pose additional communication the assay platform used to screen challenges . 
finally , patients for eligibility and assignment to substudies will also need to be cleared with an investigational device exemption by the us food and drug administration , further adding regulatory complexities . despite these challenges , the opportunities afforded by the new - generation platform trials are enormous . 
from a study design perspective , as we have illustrated , a single platform trial under a master protocol can facilitate information sharing of safety and efcacy data across disease subtypes in the statistical analysis.58 to date , most existing statistical methods have been proposed that deal with safety and efcacy questions independently ( eg , crm for safety dose nding , hbm for efcacy evaluation )  . 
 early - phase platform trials manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors inst = my institution . 
semin oncol 42 : 724 - 730 , 2015 renfro la , sargent dj : statistical controversies in clinical research : basket trials , umbrella trials , and other master protocolsa review and examples . 
n engl j med 377 : 62 - 70 , 2017 kim es , herbst rs , wistuba ii , et al : the battle trial : personalizing therapy for lung cancer . 
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cancer prev res ( phila ) 5 : 1144 - 1154 , 2012 jakubowiak aj , grifth ka , reece de , et al : lenalidomide , bortezomib , pegylated liposomal doxorubicin , and dexamethasone in newly diagnosed multiple myeloma : a phase 1 / 2 multiple myeloma research consortium trial . 
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polley my : practical modications to the time - to - event continual reassessment method for phase i cancer trials with fast patient accrual and late - onset toxicities . stat med 30 : 2130 - 2143 , 2011 52 . 
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houede n , thall pf , nguyen h , et al : utility - based optimization of combination therapy using ordinal toxicity and efcacy in phase i / ii trials . 
 harnessing clinical sequencing data for survival stratication of patients with metastatic lung adenocarcinomas ronglai shen , phd1 ; axel martin , ms1 ; ai ni , phd1 ; matthew hellmann , md1 ; kathryn c . 
we sought to extend the use of broad - panel sequencing results to survival stratication and clinical outcome prediction . methods by using sequencing results from a cohort of 1 , 054 patients with advanced lung adenocarcinomas , we developed oncocast , a machine learning tool for survival risk stratication and biomarker identication . results with oncocast , we stratied this patient cohort into four risk groups on the basis of tumor genomic prole . 
2019 by american society of clinical oncology introduction with the growth of precision medicine programs driven by genomic testing as well as recent us food and drug administration clearance of next - generation sequencing ( ngs ) platforms for clinical use , there has been rapid growth in the availability of broad - panel sequencing data for patients with cancer . 
zehir et al1 delineated the molecular landscape of 10 , 000 metastatic cancers in a pretreated real - world cohort sequenced by the memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) platform , a hybridization capture - based ngs panel that can detect mutations and copy number alterations in 341 or more cancer - associated genes.2 this study showed that 37% of patients harbored at least one therapeutically actionable alteration , and 11% were matched to genome - directed clinical trials . in patients with lung adenocarcinoma , tumor genotyping is now an essential step in routine clinical decision making . 
to determine treatment , patients with lung adenocarcinomas are currently categorized on the basis of the presence of mutated driver oncogenes ( eg , egfr , alk , ros1 , and braf )  . 
a multiinstitutional study characterized genetic aberrations across 10 genes in 733 tumor samples and identied an oncogenic driver in 64% of the patients.3 by using broad - panel sequencing , jordan et al4 reported on a single - institution experience of 860 patients with metastatic lung adenocarcinoma . 
more than 37% of patients received a matched therapy , and the use of matched therapy was strongly inuenced by the level of pre - existent clinical evidence that the mutation identied predicts the drug response . although the focus of tumor genotyping has been on ascertaining mutations that identify therapeutic targets , there is considerable unexplained variability in clinical outcomes , even within specic molecular subsets of patients with metastatic cancer . 
 shen et al death - ligand 1 ( pd - 1 / pd - l1 ) inhibitors.5 however , additional markers are needed to predict durable benet and long - term survival among these patients . 
some studies have explored the effects of single co - occurring alterations on outcome in patients with egfr - mutant and kras - mutant lung adenocarcinoma , and they observed that the presence or absence of pairs of co - occurring events could be used to identify those patients with a poor prognosis most in need of novel therapeutic approaches.3 , 6 - 8 however , a systematic approach is needed to additionally improve our understanding of survival and treatment outcome of patients . thus , we developed oncocast , a computational tool for survival stratication , and applied it to a large clinical series of patients with metastatic lung adenocarcinomas to improve the understanding of heterogeneity in clinical outcome for these patients and the mutation and comutational patterns that underlie such heterogeneity . 
such real - world evidence can supplement information from randomized clinical trials in that the results are more generalizable to patients treated outside randomized clinical trials , and the larger sample sizes of real - world data sets allow subset analysis that clinical trials are not powered for . 
the open - source computational pipeline that we have developed can facilitate the application of statistical and machine learning approaches for clinico - genomics analysis of precision medicine data sets . methods the oncocast method is described in the data supplement . 
electronic medical records were used to identify patient clinical factors as well as survival outcomes as previously described.4 overall survival ( os ) was dened as the time from date of diagnosis of advanced disease ( stage iv or recurrent cancer ) until date of death or last follow - up . 
however , a fraction ( 21% ) of the tumors were sampled and sequenced more than 6 months from the date of metastatic disease , with 16% sequenced at more than 1 year and 8% sequenced at more than 2 years , which represents older samples used for sequencing analysis . 
those patients with older samples which had been taken at initial diagnosis of from their initial advanced lung cancer were immortal sampling time to the time of referral for msk - impact sequencing . 
this interval can be long for a small fraction of patients ( 8% with a delayed interval of more than 2 years , as mentioned earlier ) , which introduces survival bias . 
details of lefttruncation analysis are described in the data supplement . the most frequently mutated genes were tp53 ( 55.1% ) , kras ( 30% ) , egfr ( 29.4% ) , stk11 ( 17.7% ) , and keap1 ( 17.7% ; data supplement )  . 
among the frequently comutated gene pairs , stk11 and keap1 were comutated in 10% of the tumors , and kras and stk11 were comutated in 9% of the tumors ( data supplement )  . prognostic relevance and clonality of cancer genes to dene the prognostic signicance of msk - impact panel genes that were sequenced , we developed oncocast , a machine learning tool for survival risk stratication and biomarker identication by implementing a lassopenalized proportional hazards regression for deriving prediction rules for os and feature selection ( data supplement )  . 
oncocast uses an ensemble learning strategy by repeatedly splitting the cohort into training and test sets that generate an ensemble of classiers with varying selection of genes and gene combinations ( data supplement )  . the median number of prognostic genes selected was 19 ( range , 4 - 67 genes ) , with a total of 169 cancer genes selected at least once by the ensemble learner . 
the relative prognostic importance of each gene was measured by how often it was selected ( fraction of the models containing the gene ) and its average regression coefcients , which determined the corresponding weights for individual genes in the scoring rule . 
circle size is proportional to mutation frequency . targeted and immunotherapies than subclonal events.9 - 11 we thus used the high depth of coverage afforded by our sequencing data ( mean coverage , 758 ) to determine the clonality of the gene alterations found to be associated with prognosis in the analysis we outlined earlier . 
 shen et al oncocast : an integrated prognostic scoring system based on ngs tumor proling in addition , improvement . oncocast aggregates prognostic effects across the sequenced cancer genes to derive a genomic risk score for each patient ( scaled from 0 to 10 ) , with a higher score indicating a greater likelihood of shorter survival . 
there was a difference of more than 6 units in average risk score between the highand low - risk groups . the oncocast classication substantially outperformed all of the individual genes as a predictor of os ( fig 3b )  . 
oncocast risk score remained a highly signicant predictor after adjusting for clinical variables and treatment types as potential confounding factors in a multivariable cox regression model ( data supplement )  . to conrm the validity of the oncocast survival stratication , we applied it to a separate data set of patients with mostly early - stage nonsmall - cell lung cancer obtained from the cancer genome atlas lung adenocarcinoma analysis . 
stk11 is a tumor suppressor gene that encodes for the serine / threonine kinase lkb1 that functions as a negative regulator of mammalian target of rapamycin ( mtor ) signaling . 
to examine the status of the other allele in such cases , we performed allele - specic cna using the fraction and allele - specic copy number estimates from tumor sequencing ( facets ) algorithm.15 strikingly , more than 90% of stk11 mutant tumors had evidence of biallelic inactivation through loss of heterogeneity ( loh ) of chromosome 19p ( data supplement )  . 
the majority of keap1 mutations were missense , and the mutant copy was frequently duplicated ( present as copy - neutral loh and uniparental gains ) as reected in the average total copy number . we also explored whether other tumor characteristics such as tumor mutational signature or intratumor heterogeneity were prognostic and associated with oncocast risk score . previously dened smoking - associated and apolipoprotein b mrna editing enzyme , catalytic polypeptide - like ( apobec ) signatures were the most prevalent mutational signatures in this cohort . 
however , mutation burden did not provide additional prognostic value beyond oncocast risk score in a multivariable cox model ( data supplement )  . clonal diversity was calculated for each tumor by summarizing the cancer cell fraction for all somatic mutations using the shannon index . 
 ( a ) kaplan - meier plot of survival curves for the four risk subgroups ( low , intermediate - low [ int - low ] , intermediate - high [ int - high ] , and high )  . 
the average risk score ( avg rs ) , median overall survival ( os ) , and 1 - year and 3 - year survival probabilities are reported for each group . 
 ( b ) forest plot of hazard ratios ( hrs ) for age , sex , smoking status , and individual driver gene alterations compared with the oncocast integrated scoring approach . genotypes associated with risk groups to better understand the association between targetable cancer driver mutations and oncocast risk score , we explored the distribution of genotypes within four major risk categories ( fig 5 )  . 
the dening characteristic for the patients in the low - risk group without egfr , alk , ret , and ros1 alterations was an absence of any of the poor prognostic gene alterations . 
this suggests that stk11 and keap1 comutation denes a cohort of patients with resected lung adenocarcinoma at higher risk of disease progression and cancerspecic mortality . survival stratication in specic treatment subsets we then sought to demonstrate the ability of the oncocast technique to explore tumor genomic predictor outcomes in last to death or the subset of patients with mutated driver oncogenes treated with kinase inhibitors . 
the model , oncocast - tr ( targeted therapies model ) , was derived using the genomic proles and survival outcomes from the start of therapy for the 387 patients who received targeted therapies ( egfr , alk , ros )  . 
tp53 is strongly associated with worse survival outcome ( fig 6c ) , with 96% of patients in the tr2 group harboring concurrent tp53 mutations and 0% concurrent tp53 mutations in the tr1 group . 
arid1a also showed association with poor survival with 11 ( 78% ) of 14 arid1a mutations in tr2 . interactive tool for visualizing and exploring mutation pattern and survival to facilitate clinical translation and research use of the data , we created an interactive web application ( data that allows for visualization of mutation supplement ) ros1 fusion , 6% ret fusion , low - intermediate tp53 , egfr , smarca4 , 2% tp53 , ret fusion , 1% tp53 , alk fusion , 1% tp53 , ros1 fusion , 2% tp53 , smarca4 , 3% egfr , 40% tp53 , kras , tp53 , egfr , tp53 , egfr , alk fusion , other , 30% kras , 17% tp53 , 24% high - intermediate keap1 , 2% stk11 , 5% tp53 , kras , stk11 , 6% tp53 , kras , keap1 , 6% tp53 , keap1 , kras , keap1 , kras , stk11 , stk11 , keap1 , smarca4 , 7% tp53 , kras , stk11 , keap1 , 8% stk11 , keap1 , 8% high tp53 , stk11 , keap1 , smarca4 , 6% kras , stk11 , keap1 , 28% tp53 , stk11 , keap1 , 25% tp53 , stk11 , 10% kras , stk11 , keap1 , smarca4 , 16% fig 5 . 
 ( c ) gene importance plot for the oncocast - tr model . patterns and individualized prediction of os to be generated on the basis of a user - dened mutational prole and clinical characteristics . 
along with a patients clinical prole , the application outputs the predicted survival probabilities and 95% cis . although the tool was built using the largest metastatic lung adenocarcinoma cohort to date , it was designed to be dynamically updated as new data are incorporated into the model . discussion tumors from patients with lung adenocarcinoma have a high frequency of actionable oncogenic drivers.16 , 17 the introduction of targeted therapy has transformed the clinical care of patients with lung adenocarcinoma by incorporating tumor genotyping into therapeutic decision making . 
by using an ensemble learning approach , we demonstrated the prognostic utility of data from a large panel ngs assay interrogating 341 cancer - associated genes in 1 , 054 patients with metastatic lung adenocarcinoma treated with currently available therapies . 
we show that it is a practical approach to molecular stratication in metastatic lung adenocarcinoma and provides the ability to identify biomarkers that predict survival outcome . overlaying the oncocast risk score with the tumor genomic landscape revealed novel biologic and clinical insights . 
the major prognostic genes associated with poor survival included stk11 , keap1 , tp53 , kras , and smarca4 . remarkably , comutations of both stk11 and keap1 dened an exceptionally high - risk prole with a short median os of 7.3 months and an increase of more than 6 units in risk score compared with a low - risk group , corresponding to an hr of 4.6. 
some of the favorable prognostic genes may reect the availability of effective targeted therapies in the case of egfr , alk , and ros1 . however , in patients with these targetable oncogenes , there is heterogeneity in the additional mutations their tumors harbor . 
for example , our model revealed that mutations in tp53 and arid1a dene a high - risk subgroup with shorter survival in the tyrosine kinase inhibitortreated patient cohort . is novel in that conversely , some of the unfavorable prognostic genes may reect negative associations with treatment responses ( eg , the recent observation that stk11 inactivation is associated with poor responses to immunotherapy18 )  . 
mutations in keap1 are associated with chemotherapy resistance and poor survival . some studies have suggested that targeting nrf2 may enhance chemotherapy sensitization.19 , 20 mtor is a kinase downstream of lkb1 ( stk11 ) , and mtor inhibitors have been proposed as a potential therapeutic approach in stk11 - mutant tumors.21 smarca4 was also identied as a major driver of a poor prognosis factor in metastatic lung adenocarcinoma in our study . 
 shen et al complexes that regulate genomic instability and dna repair . smarca4 was mutated in 9.4% of lung adenocarcinomas in the msk - impact cohort , with 42% of the mutations being truncating and residing in regions of loh . 
with increasing sample sizes , we will be poised to identify outcome associations with rare alterations , and we will be better able to explain the heterogeneity in clinical outcomes for patients with advanced lung adenocarcinoma . in addition , the oncocast risk score described here provides a valuable tool for more accurately determining the prognosis of patients enrolled in clinical trials or included in real - world data sets . 
although conventional clinical factors such as age , sex , and performance status have long been used , our data indicate that we can signicantly improve the description of patient populations by incorporating the genomic risk scores in our understanding to allow better comparisons of groups of patients enrolled in clinical trials or included in real - world data sets . with the growth of precision medicine programs driven by genomic testing as well as recent us food and drug administration clearance of ngs platforms for clinical use , there will be a rapid growth in the availability of broad sequencing data for patients with a variety of cancers and growing integration with clinical data through institutional databases and electronic health records . 
riely manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors matthew hellmann stock and other ownership interests : shattuck labs honoraria : astrazeneca , bristol - myers squibb consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca / medimmune , novartis , janssen , nektar therapeutics , syndax pharmaceuticals , mirati therapeutics , shattuck labs research funding : bristol - myers squibb ( inst ) patents , royalties , other intellectual property : a patent has been led by memorial sloan kettering ( pct / us2015 / 062208 ) for the use of tumor mutation burden for prediction of immunotherapy efcacy , which is licensed to personal genome diagnostics ( inst ) travel , accommodations , expenses : astrazeneca , bristol - myers squibb kathryn c . 
rudin consulting or advisory role : bristol - myers squibb , abbvie , seattle genetics , harpoon therapeutics , genentech , astrazeneca , ascentage pharma , bicycle therapeutics , celgene , daiichi sankyo , ipsen , loxo oncology , pharmamar , elucida oncology research funding : abbvie / stemcentrx ( inst ) , viralytics ( inst ) , merck ( inst ) , daiichi sankyo ( inst ) michael f . 
solit stock and other ownership interests : loxo oncology consulting or advisory role : pzer , loxo oncology , illumina , intezyne technologies , vivideon therapeutics travel , accommodations , expenses : merck maria arcila consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe technologies , raindance technologies marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso request for proposal advisory committee , takeda pharmaceuticals , bristol - myers squibb , bayer ag , merck ( i ) research funding : loxo oncology ( inst ) , helsinn therapeutics gregory j . 
riely research funding : novartis ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pzer ( inst ) , innity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : merck sharp & dohme no other potential conicts of interest were reported . references zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
nat med 23 : 703 - 713 , 2017 cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
j mol diagn 17 : 251 - 264 , 2015 kris mg , johnson be , berry ld , et al : using multiplexed assays of oncogenic drivers in lung cancers to select targeted drugs . 
jama 311 : 1998 - 2006 , 2014 jordan ej , kim hr , arcila me , et al : prospective comprehensive molecular characterization of lung adenocarcinomas for efcient patient matching to approved and emerging therapies . 
hellmann md , nathanson t , rizvi h , et al : genomic features of response to combination immunotherapy in patients with advanced non - small - cell lung cancer . cancer cell 33 : 843 - 852.e4 , 2018 arbour kc , jordan e , kim hr , et al : effects of co - occurring genomic alterations on outcomes in patients with kras - mutant non - small cell lung cancer . 
clin cancer res 24 : 334 - 340 , 2018 yu ha , suzawa k , jordan e , et al : concurrent alterations in egfr - mutant lung cancers associated with resistance to egfr kinase inhibitors and characterization of mtor as a mediator of resistance . 
clin cancer res 24 : 3108 - 3118 , 2018 yu ha , sima cs , shen r , et al : prognostic impact of kras mutation subtypes in 677 patients with metastatic lung adenocarcinomas . 
j thorac oncol 10 : 431 - 437 , 2015 de bruin ec , mcgranahan n , mitter r , et al : spatial and temporal diversity in genomic instability processes denes lung cancer evolution . 
rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
azzoli cg , temin s , giaccone g : 2011 focused update of 2009 american society of clinical oncology clinical practice guideline update on chemotherapy for stage iv non - small - cell lung cancer . 
directors challenge consortium for the molecular classication of lung adenocarcinoma , shedden k , taylor jm , et al : gene expression - based survival prediction in lung adenocarcinoma : a multi - site , blinded validation study . 
ren d , villeneuve nf , jiang t , et al : brusatol enhances the efcacy of chemotherapy by inhibiting the nrf2 - mediated defense mechanisproc natl acad sci u 21 . 
tagal v , wei s , zhang w , et al : smarca4 - inactivating mutations increase sensitivity to aurora kinase a inhibitor vx - 680 in non - small cell lung cancers . 
 impact of genetic ancestry on outcomes in ecog - acrin - 5103 purpose racial disparity in breast cancer outcomes exists between african american and white women in the united states . 
we have evaluated the impact of genetically determined ancestry on disparity in efficacy and therapy - induced toxicity for patients with breast cancer in the context of a randomized , phase iii adjuvant trial . methods this study compared outcomes between 386 patients of african ancestry ( aa ) and 2 , 473 patients of european ancestry ( ea ) in a randomized , phase iii breast cancer trial , ecogacrin - 5103 . 
the primary efficacy end point , invasive diseasefree survival ( dfs ) , and clinically significant toxicities were compared , including anthracycline - induced congestive heart failure , taxane - induced peripheral neuropathy ( tipn ) , and bevacizumab - induced hypertension . results overall , aas had significantly inferior dfs ( p = .002 ; hazard ratio , 1.5 ) compared with eas . 
2017 by american society of clinical oncology introduction african american patients with breast cancer have inferior efficacy outcomes compared with other races.1 , 2 the reason for this imbalance is multifactorial and includes higher stage , higher grade , more triple - negative breast cancer ( tnbc ) , and poorer responsiveness to chemotherapy.3 , 4 these clinical imbalances have previously been attributed to both socioeconomic factors and a different underlying biology of the tumor.2 , 5 patients of african ancestry ( aa ) also experience more adverse drug reactions , including an increase in clinically important toxicities for chemotherapeutic agents . 
although less well characterized , these toxicity disparities are also likely multifactorial and include inherited genetic variation and comorbidities , among other factors.6 - 10 much of the prior work has been based on selfreported race . 
 node - negative breast cancer to intravenous doxorubicin and cyclophosphamide ( ac ) every 2 or 3 weeks ( at discretion of treating physician ) for four cycles followed by 12 weeks of paclitaxel ( 80 mg / m2 once per week ) alone ( arm a ) or to the same chemotherapy with either concurrent bevacizumab ( arm b ) or concurrent plus sequential bevacizumab ( arm c ) ; figure 1a . 
patients with estrogen receptor ( er ) positive disease were ln positive , had a tumor > 5 cm or a tumor measuring 1 to 5 cm , with a recurrence score > 11 . genome - wide association study germline dna from whole blood and companion clinical outcome data were available in 3 , 126 patients . 
if arm c significantly improved dfs relative to arm a , then in the second step , a comparison of arm b with arm a was performed.14 in this correlative study , dfs and overall survival ( os ) were evaluated using kaplan - meier methodology . 
the differences in outcomes between aas and eas were compared with the application of cox proportionalhazards models using either univariate or multivariate analysis , which were corrected with significant covariates . 
to identify the best regression model , a forward and a backward stepwise selection procedure were performed separately to evaluate variable associations , and the akaike information criterion was used to determine the inclusion of potential confounders such as race , menopausal status , age , weight , height , side of cancer involvement , er status , histologic grade , nuclear grade , ln status , type of surgery , types of ac schedule , and dose reductions in ac or paclitaxel . both procedures returned the same model with six predictors , which are listed in the data supplement . dfs was the primary end point of the parent trial ; it was defined as invasive dfs and calculated from the date of random assignment to the date of first treatment failure ( invasive ipsilateral , local / regional invasive , distant recurrence , invasive contralateral breast cancer , invasive nonbreast second primary , or death from any cause [ whichever occurred first ] )  . cases with incomplete follow - up , without a documented invasive dfs event ( including those who developed squamous or basal cell skin cancers or in situ carcinomas of any site as their only event ) were censored at the date of last disease evaluation . 
we previously published biomarker data on each of these toxicities.15 , 17 , 18 in the present study , we sought to compare the frequency of all toxicities between aas and eas and to assess the impact of race on dose modifications . 
statistical analysis was performed using r ( version 3.3.0 ) and the x2 test . odds ratio ( or ) was used to evaluate the significance and magnitude of the differences in the toxicity frequency between aas and eas . chf cases for this study included individuals who had centrally reviewed , cardiologist - adjudicated chf . 
to be selected for inclusion in ecogacrin - 5103 , patients must have had no history of clinically significant cardiovascular disease . cardiovascular health was monitored at the start and during the trial by multigated angiograms or echocardiograms . 
cardiac events included chf , decrease in left ventricle ejection fraction , acute coronary syndrome , supraventricular tachycardia , and myocardial dysfunction diagnosed by a cardiologist . tipn cases for this study were defined as those experiencing either grades 2 to 4 or grades 3 to 4 tipn as assessed by ctcae . 
to serve as a tipn case , the patient must have received at least one dose of paclitaxel , and the neuropathy event must have occurred during treatment or within 3 months of the last dose of therapy . hypertension cases for this study were defined as those experiencing a systolic blood pressure ( sbp )  . 
blood pressure values were collected as part of standard clinical assessment before administration of therapy throughout the conduct of the trial . results genotyped group from ecog - acrin5103 and genetic ancestry a total of 3 , 394 germline dna samples from patients were collected as part of the planned correlative protocol within ecog - acrin5103 ( fig 1b )  . 
the outcomes of the entire genotyped cohort ( all ancestries combined ) used in this correlative study were almost identical to the parent trial4 ( data supplement )  . demographic data and disease comparisons table 1 summarizes the important demographic comparisons between aas and eas . 
we assessed for the differences in the parent trial stratification factors as well as other known outcome predictors , including age , hormone receptor status ( er positive v tnbc ) , ln status , height , weight , type of surgery , and tumor grade . 
there were no significant differences overall in ln status . genetic ancestry as a predictor of efficacy in ecog - acrin - 5103 dfs was the primary efficacy end point of the parent trial . 
an imbalance in associated comorbidities or environmental factors cannot be excluded as a contributing cause , and unfortunately , those data were not collected in ecog - acrin - 5103 . 
dose reductions in paclitaxel also negatively affected dfs for all ancestries ( p = .02 ; data supplement ) ; however , having a dose modification in paclitaxel did not affect dfs for eas , but it did significantly cause an inferior dfs for aas ( fig 4 )  . the difference may have been explained by more severe dose reductions in aas . 
the outcomes for the subgroup genotyped , however , were similar to the parent population , thus minimizing the concern for subgroup bias . we also compared the results of the genetic ancestry with self - reported race , and there was no significant difference in the conclusion . 
work in other disease phenotypes , however , has demonstrated that use of self - reported race as a surrogate for genetic ancestry was not perfect.25 - 27 prior work has demonstrated that  . 
9% of patients cannot supply , or choose not to supply , ancestry information.28 thus , the real impact of accurately self - reported race is probably larger than the 9% that was observed , as the result of misclassification alone . 
although genotype may provide more insight toward underlying biologic diversity , selfreported race still likely represents a reasonable surrogate for genotypic variation in the routine clinical setting for consideration of metabolism and drug toxicity . we previously evaluated genetic markers to predict some of the most clinically important toxicities in ecog - acrin - 5103 : bevacizumabinduced hypertension ( using various definitions ) , tipn , and cardiologist - adjudicated anthracyclineinduced chf.15 , 17 , 18 in this study we compared the likelihood of each of these clinically relevant toxicities between aas and eas . 
these data support prior work from a single - institution retrospective analysis as well as data in pediatric populations that revealed higher likelihood of anthracycline - induced chf in aas . 
similarly , a prior single - institution retrospective analysis demonstrated higher risk of tipn for aas.8 - 10 because aas experience greater toxicity , it is highly unlikely that the imbalance in efficacy is a result of exposure as the result of pharmacokinetic considerations , as the end organs are clearly being affected . 
as expected , all ancestries that had dose reductions in the ac portion of the chemotherapy had inferior dfs ; this difference , however , was present for both eas and aas . 
the significant difference in dfs as the result of paclitaxel dose modifications for aas may have been because of the markedly more severe dose reductions ; this was evidencedby alower meannormalizeddosein thosewho had dose reductions ( p = .03 ) , in large part because table 2 . 
this study did not evaluate socioeconomic factors , which are known to be important variables in outcomes.5 however , in the context of a randomized phase iii trial , many of these inequities are minimized . in conclusion , this study highlights the need to better understand the biologic differences in normal breast biology , tumor biology , and the inherited genetic differences between women of aa and ea . 
it also highlights the need to better personalize counseling when discussing the risk - to - benefit ratio for aas , for whom the disease - specific outcomes are inferior and drug - specific toxicities are higher . 
ecog - 1199 previously demonstrated that the dosing of docetaxel every 3 weeks was as effective but had fewer dose reductions for aas in a similar clinical setting.20 future trials should investigate whether another taxane with less risk of tipn , such as docetaxel , might be more effective for aas in the adjuvant breast cancer setting . 
sparano stock and other ownership interests : metastat consulting or advisory role : genentech , novartis , astrazeneca , celgene , eli lilly , celldex , pfizer , prescient therapeutics , juno therapeutics , merrimack research funding : prescient therapeutics ( inst ) , deciphera ( inst ) , genentech ( inst ) , merck ( inst ) , novartis ( inst ) , merrimack ( inst ) george w . 
sledge jr leadership : syndax stock and other ownership interests : syndax honoraria : symphogen consulting or advisory role : symphogen , coherus biosciences , radius health , peregrine pharmaceuticals , taiho pharmaceutical research funding : genentech ( inst ) travel , accommodations , expenses : nektar , radius health , taiho pharmaceutical kathy d . 
miller consulting or advisory role : nektar , tesaro , merck research funding : genentech ( inst ) , merrimack ( inst ) , entremed ( inst ) , taiho pharmaceutical ( inst ) , macrogenics ( inst ) , medivation ( inst ) , novartis ( inst ) , seattle genetics ( inst ) affiliations support bryan p . 
schneider , fei shen , guanglong jiang , milan radovich , lang li , laura gardner , dongbing lai , tatiana foroud , and kathy d . miller , indiana university school of medicine , indianapolis , in ; anne oneill , dana farber cancer instituteecog - acrin biostatistics center , boston , ma ; joseph a . 
keenan t , moy b , mroz ea , et al : comparison of the genomic landscape between primary breast cancer in african american versus white women and the association of racial differences with tumor recurrence . 
desantis c , jemal a , ward e : disparities in breast cancer prognostic factors by race , insurance status , and education . jama 295 : 2492 - 2502 , 2006 cancer causes control 21 : 1445 - 1450 , 2010 americans . 
kidd rs , curry tb , gallagher s , et al : identification of a null allele of cyp2c9 in an african - american exhibiting toxicity to phenytopharmacogenetics 11 : 803 - 808 , 2001 8 . 
bhatnagar b , gilmore s , goloubeva o , et al : chemotherapy dose reduction due to chemotherapy induced peripheral neuropathy in breast cancer patients receiving chemotherapy in the neoadjuvant or adjuvant settings : a single - center experience . 
cobb rj , thomas cs , laster pirtle wn , et al : self - identified race , socially assigned skin tone , and adult physiological dysregulation : assessing multiple dimensions of race in health disparities research . 
miller k , oneill am , dang ct , et al : bevacizumab ( bv ) in the adjuvant treatment of her2 - negative breast cancer : final results from eastern cooperative oncology group e5103 . 
schneider bp , li l , radovich m , et al : genome - wide association studies for taxane - induced peripheral neuropathy in ecog - 5103 and ecog - 1199 . 
killelea bk , yang vq , wang sy , et al : racial differences in the use and outcome of neoadjuvant chemotherapy for breast cancer : results from the national cancer data base . 
halder i , shriver m , thomas m , et al : a panel of ancestry informative markers for estimating individual biogeographical ancestry and admixture from four continents : utility and applications . 
louwers yv , lao o , fauser bc , et al : the impact of self - reported ethnicity versus genetic ancestry on phenotypic characteristics of polycystic ovary syndrome ( pcos )  . 
 c distinct dicer1 hotspot mutations identify bilateral tumors as separate events introduction dicer1 syndrome1 predisposes to a variety of cancers , including pleuropulmonary blastoma ( ppb ) , 2 ovarian sertoli - leydig cell tumor ( slct ) , 3 embryonal rhabdomyosarcoma , 4 and kidney tumors.5 - 8 in dicer1 syndrome , most patients bear a germline null mutation in dicer1 , and the tumors uniformly bear a second - hit missense substitution at one of five hotspot positions ( 1705e , 1709d , 1809g , 1810d , and 1813e )  . a wide range of clinical phenotypes can be seen in dicer1 syndrome5 , 9 ; some patients are asymptomatic , whereas others develop multiple tumors . 
in the classic cases , patients with a germline null mutation develop different somatic hotspot mutations in each tumor.7 , 10 - 16 however , in some patients , multiple tumors arise from germline mosaicism of the hotspot mutation , with subsequent somatic loss of the wild - type allele.17 - 19 here we report a patient with dicer1 syndrome who developed four tumor types at six anatomic sites over the course of 12 years . 
because we found no other mutations to explain her particularly severe clinical course , we speculate that her subsequent tumors were a product of the intense chemotherapy and radiation regimens she received . methods informed consent was obtained from the patient and her guardian before collection of tumor specimens . 
when needed , pcr products were subcloned into pcr2.1topo ( thermo - fisher scientific , waltham , ma ) before sequencing . for tp53 sequencing , coding regions were amplified using the accel - amplicon comprehensive tp53 panel ( swift biosciences , ann arbor , mi )  . 
reads were trimmed using trimmomatic21 in the galaxy project and were aligned to human genome grch38 using bwa - mem22 ; 88% mapped to the tp53 locus , producing a mean depth of 13 , 367x in targeted regions . 
variants were called using the freebayes algorithm v0.9.20 using frequency - based pooled calling instead of simple diploid calling , which allowed the algorithm to detect subclonal mutations.23 results clinical presentation the patient ( cmcw11 ) presented originally at 5 years of age with a left kidney mass . 
she was treated with 10 months of combination chemotherapy ( vincristine , doxorubicin , cyclophosphamide , irinotecan , and etoposide ) targeted at both anaplastic wilms tumor and sarcoma , together with 2 , 100 cgy whole - abdomen irradiation given in 14 fractions over 19 days . when the patient was 10 years old , a new mass arose in her remaining kidney , with a histology similar to her prior tumor , and she was diagnosed with relapsed wilms tumor ( fig 1b )  . 
 on completion , she underwent right radical nephrectomy and started hemodialysis . this patients kidney tumors were diagnosed initially as wilms tumor , but in retrospect their unique histologic features are more consistent with anaplastic sarcoma of the kidney . 
this entity was first described in 2007 , after our patients kidney tumor first arose.24 biallelic dicer1 mutations have been seen in both wilms tumor and anaplastic sarcoma of the kidney , which may represent neoplastic degeneration from cystic nephroma.6 - 8 at 12 years of age , the patient developed multiple nodules throughout her thyroid . 
thyroidectomy revealed follicular adenomas ( fig 1c )  . at 13 years of age , a mass arising from her bladder was diagnosed as embryonal rhabdomyosarcoma with focal cartilaginous differentiation ( fig 1d )  . 
sanger sequencing chromatograms demonstrating the patients ( a ) dicer1 germline frameshift mutation and ( b ) rnase iiib hotspot mutations in her ovarian sertoli - leydig cell tumors ( slcts ) ; ( c ) left ( l ) kidney tumor ; and ( d ) right ( r ) kidney tumor . 
since that time , she has been observed for > 2 years , with no further disease . dicer1 mutations we performed whole - exome sequencing on the patients first kidney tumor and germline dna as table 1 . 
her tumor bore an additional somatic hotspot mutation ( c.5425g > a ; p.g1809r ; fig 2 and table 1 )  . we then sequenced the rnase iii domains of dicer1 in archival specimens from her other tumors . 
to sequence strands separately , we subcloned the pcr amplicon spanning this mutation and found that both single - nucleotide variants occurred on the same strand , making the tumor heterozygous for a single somatic hotspot mutation ( appendix fig a1 )  . 
contrary to our clinical suspicion at the time , her contralateral kidney tumor was , in fact , a second primary . we also sequenced dicer1 from her thyroid follicular adenoma and bladder rhabdomyosarcoma . 
bladder rhabdomyosarcomas have been associated previously with dicer1 syndrome , although specific discussion of their histologic features was not reported.4 her two ovarian tumors were detected at the same time , and it was unclear whether they represented distinct primary tumors or metastatic spread . 
her initial renal tumor bore a p.v274l variant , as we described previously.20 however , her remaining tumors had no additional somatic tp53 variants and did not undergo loss of heterozygosity at tp53 . discussion clinically , the discovery of a second tumor with similar histology can raise the question of whether it is a recurrence or a new primary tumor . 
had we known that her second kidney tumor was , in fact , metachronous , she might have avoided the increased toxicity of chemotherapy regimens designed for relapsed or refractory tumors . 
in fact , the cartilaginous elements of her bladder tumor led us to question whether it could instead represent a distant recurrence of her renal sarcoma , although its distinct dicer1 mutation proved its independence . thus , this case highlights a powerful but often overlooked application of clinical tumor sequencing : better understanding of the biology behind tumor formation . 
as sequencing costs fall , clinicians should be cognizant that tumor sequencing can help distinguish between new primary tumors and recurrences . in this case , sequencing at initial diagnosis would have also had the added benefit of alerting clinicians to her potential dicer1 status . 
in the case of dicer1 syndrome , because second hit mutations occur at such stereotyped positions , sequencing separate tumors could even occur by simple sanger sequencing rather than by next - generation sequencing . 
in patients with dicer1 syndrome , dedicated tests may be developed for identifying these stereotyped mutations , perhaps including circulating tumor dna assays as a noninvasive screening method . this is one of the most severe cases in the literature of multiple distinct somatic dicer1 mutations arising in a patient . 
shukla no relationship to disclose jason wang no relationship to disclose veena rajaram no relationship to disclose gordan vujanic no relationship to disclose tamra slone no relationship to disclose dinesh rakheja no relationship to disclose james f . 
slade i , bacchelli c , davies h , et al : dicer1 syndrome : clarifying the diagnosis , clinical features and management implications of a pleiotropic tumour predisposition syndrome . 
schultz ka , pacheco mc , yang j , et al : ovarian sex cord - stromal tumors , pleuropulmonary blastoma and dicer1 mutations : a report from the international pleuropulmonary blastoma registry . 
schultz ka , harris a , messinger y , et al : ovarian tumors related to intronic mutations in dicer1 : a report from the international ovarian and testicular stromal tumor registry . 
durieux e , descotes f , mauduit c , et al : the co - occurrence of an ovarian sertoli - leydig cell tumor with a thyroid carcinoma is highly suggestive of a dicer1 syndrome . 
klein s , lee h , ghahremani s , et al : expanding the phenotype of mutations in dicer1 : mosaic missense mutations in the rnase iiib domain of dicer1 cause glow syndrome . 
brenneman m , field a , yang j , et al : temporal order of rnase iiib and loss - of - function mutations during development determines phenotype in dicer1 syndrome : a unique variant of the two - hit tumor suppression model . 
vujani gm , kelsey a , perlman ej , et al : anaplastic sarcoma of the kidney : a clinicopathologic study of 20 cases of a new entity with polyphenotypic features . 
pugh tj , yu w , yang j , et al : exome sequencing of pleuropulmonary blastoma reveals frequent biallelic loss of tp53 and two hits in dicer1 resulting in retention of 5p - derived mirna hairpin loop sequences . 
 o plasma androgen receptor copy number status at emergence of metastatic castration - resistant prostate cancer : a pooled multicohort analysis anuradha jayaram , md1 ; anna wingate , msc1 ; daniel wetterskog , phd1 ; vincenza conteduca , md , phd2 ; daniel khalaf , md3 ; mansour taghavi azar sharabiani , phd4 ; fabio calabr `o , md5 ; lorraine barwell , md6 ; susan feyerabend , md7 ; enrique grande , md8 ; alberto martinez - carrasco , msc9 ; albert font , md , phd10 ; alfredo berruti , md11 ; cora n . 
sternberg , md12 ; rob jones , ma , md , phd6 ; florence lefresne , md13 ; marjolein lahaye , msc13 ; shibu thomas , phd14 ; shilpy joshi , phd15 ; dong shen , md , phd14 ; deborah ricci , phd14 ; michael gormley , phd14 ; axel s . 
wyatt , md , phd3 ; and gerhardt attard , md , phd1 purpose increases in androgen receptor ( ar ) copy number ( cn ) can be detected in plasma dna when patients develop metastatic castration - resistant prostate cancer . 
2019 by american society of clinical oncology introduction standard of care treatment at development of metastatic castration - resistant prostate cancer ( mcrpc ) is inhibition of androgen receptor ( ar ) signaling with either abiraterone acetate administered with prednisone ( aap ; 5 mg twice a day ) or enzalutamide . 
 jayaram et al context key objective several studies have assessed plasma dna , including the androgen receptor ( ar ) , as a biomarker for patient stratication . variable plasma ar copy number ( cn ) parameters have been used , making it challenging to interpret differences in associations with outcome observed across multiple analyses . 
the pcr2023 cohort ( clinicaltrials.gov identier : nct01867710 ) was an international , multi - institutional , open - label , parallel - arm , phase ii study of abiraterone acetate in asymptomatic or minimally symptomatic , chemotherapy - nave patients with mcrpc.13 patients were randomly assigned 1 : 1 : 1 : 1 to abiraterone acetate and one of four different glucocorticoid regimens ( prednisone 5 mg twice a day or once a day or 2.5 mg twice a day or dexamethasone 0.5 mg once a day ) to evaluate tolerability . 
the nal cohort , the british columbia ( bc ) cohort , was from a randomized phase ii trial of aap versus enzalutamide ( clinicaltrials.gov identier : nct02125357 ) that was sponsored and conducted by the bc cancer agency.12 for the biomarker analyses from all four studies , only patients with histologically conrmed prostate adenocarcinoma and no neuroendocrine differentiation ; progressive disease despite castrate levels of serum testosterone ( , 50 ng / dl ) ; ongoing medical or prior surgical castration ; and no prior treatment with chemotherapy , aap , or enzalutamide were included . 
all four studies obtained institutional review board and ethics committee approval and were conducted in accordance with the declaration of helsinki and the good clinical practice guidelines of the international conference on harmonization . 
psa levels in cohort a and the premiere and bc cohorts were measured as previously described.10 disease was evaluated radiographically using computed tomography scans of the chest , pcr2023 cohort a pcr2023 patients randomly assigned ( n = 164 ) baseline plasma samples ( n = 151 ) samples without long dna fragments ( n = 98 ) samples with long dna fragments ( n = 53 ) samples optimal for final analysis ( n = 135 ) samples without long dna fragments after size selection ( n = 37 ) samples with long dna fragments after size selection ( n = 16 ) patients on enzalutamide excluded ( n = 2 ) ar copy number ar copy number premiere british columbia crossover study ar copy number ar copy number samples optimal for final analysis ( n = 133 ) ar copy number density maximum log - likelihood density copy number cut point of 1.92 relative hr cumulative relative hr 1.92 cutoff based on maximum log - likelihood ar copy number ar copy number fig 1 . 
 ( b ) ar copy number ( cn ) distribution across the four clinical cohorts ( pcr2023 , cohort a , premiere , and british colombia crossover study ) included in the pooled analysis ( n = 501 )  . 
serum lactate dehydrogenase ( ldh ) and alkaline phosphatase ( alp ) were measured at screening or on day 1 of cycle 1 . outcomes plasma samples were collected prospectively in all four studies with the primary aim of studying associations between plasma dna aberrations and clinical outcome as secondary exploratory objectives . 
for full denitions of outcome measures , see the data supplement . for exploratory analysis of the association between ar status at development of mcrpc and time on adt , the outcome measure of time from start of uninterrupted adt to start of aap , abiraterone acetate plus dexamethasone ( aad ) , or enzalutamide was used . 
the association of clinically relevant baseline factors ( previously shown to be associated with prognosis15 - 17 for os and progression - free survival [ pfs ] ) was examined using univariable and multivariable cox regression models that were performed with stepwise variable selection to identify the prognostic factors for os and pfs . 
all tests were two sided , and an error of 5% was considered signicant . results clinical cohorts and plasma ar status between june 2013 and october 2014 , 164 patients were recruited onto the pcr2023 study at 22 centers in ve countries . 
visual inspection showed that the cut point region overlapped with the turning point of decreasing local hr identied via the maximum log - likelihood statistics approach.14 at increasing cns , the decreasing trend became so prominent that it reached a plateau close to an hr of 1 ( fig 1d )  . 
the clinical prognostic factors selected have been previously demonstrated to be strong independent predictors of os and pfs for ar - targeted therapies.15 , 17 - 20 using stepwise backward elimination , plasma ar gain ; high alp , ldh , and psa ; and the presence of bone and visceral metastases were all dependently associated with poorer os ( table 2 )  . 
for cohort a and the premiere cohort , 69.2% ( 36 of 52 patients ) and 60% ( 56 of 94 patients ) of patients were stage m0 at diagnosis , respectively , whereas in the bc cohort , only men who had metastatic disease detected on computed tomography of the chest , abdomen , and pelvis or whole - body bone scan at start of continuous adt were included . 
the median times from start of adt to second - generation hormone treatment of cohort a and the premiere and bc cohorts were 91 , 165 , and 64 weeks , respectively . 
 plasma ar in mcrpc pcr2023 cohort a time receiving adt ( weeks ) 4 , 096 time receiving adt ( weeks ) 4 , 096 premiere british columbia crossover study time receiving adt ( weeks ) 4 , 096 time receiving adt ( weeks ) 4 , 096 fig 3 . 
in addition , to account for differences in frequency of psa and imaging measurements , end points , follow - up times , and treatment , the mfp was stratied by trial . 
 jayaram et al second - generation ar - targeting agents when the response to adt was shorter than 12 months.23 - 25 rapidly expands after treatment resistance . initiation , leading to to appropriately interrogate our main aim , we focused our genomic analysis solely on ar . 
in an exploratory analysis in two similar but nonrandomized cohorts , we reported that the outcome of patients with mcrpc at a similar stage as patients in our study population but who were treated with taxane chemotherapy was worse in patients with higher circulating dna but not those with plasma ar gain.30 randomized studies are required to investigate whether ar gain can be used for treatment selection . 
 plasma ar in mcrpc daniel khalaf consulting or advisory role : bayer fabio calabr `o consulting or advisory role : pzer susan feyerabend consulting or advisory role : janssen - cilag a grant from astellas to support the conduct of the trial . 
wyatt , gerhardt attard provision of study materials or patients : vincenza conteduca , lorraine barwell , susan feyerabend , enrique grande , albert font , alfredo berruti , cora n . 
wyatt , gerhardt attard collection and assembly of data : anuradha jayaram , anna wingate , daniel wetterskog , vincenza conteduca , lorraine barwell , susan feyerabend , alberto martinez - carrasco , albert font , alfredo berruti , cora n . sternberg , rob jones , dong shen , deborah ricci , michael gormley , axel s . 
wyatt , gerhardt attard data analysis and interpretation : anuradha jayaram , anna wingate , daniel wetterskog , daniel khalaf , mansour taghavi azar sharabiani , fabio calabr `o , susan feyerabend , enrique grande , cora n . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . anna wingate research funding : janssen ( inst ) travel , accommodations , expenses : janssen vincenza conteduca consulting or advisory role : bayer , astellas pharma , janssen - cilag , sano travel , accommodations , expenses : bayer , astellas pharma , janssencilag , sano enrique grande honoraria : pzer , bristol - myers squibb , ipsen , roche , eisai , eusa pharma , msd , genzyme , adacap , novartis , pierre fabre , lexicon , celgene , janssen - cilag , astellas pharma consulting or advisory role : msd , pzer , ipsen research funding : mtem / threshold ( inst ) , roche , pzer ( inst ) , astrazeneca ( inst ) , ipsen ( inst ) travel , accommodations , expenses : bristol - myers squibb , genentech , pzer , janssen - cilag alfredo berruti consulting or advisory role : janssen - cilag , astellas pharma speakers bureau : janssen - cilag research funding : astellas pharma ( inst ) , janssen - cilag ( inst ) travel , accommodations , expenses : janssen - cilag , sano cora n . 
 jayaram et al shibu thomas employment : janssen research & development leadership : janssen research & development stock and other ownership interests : janssen research & development research funding : janssen oncology patents , royalties , other intellectual property : four patents ( inst ) travel , accommodations , expenses : janssen research & development kim n . 
chi honoraria : sano , janssen , astellas pharma , bayer consulting or advisory role : essa , astellas pharma , janssen , sano , amgen , bayer , astrazeneca , roche research funding : janssen ( inst ) , astellas pharma ( inst ) , bayer ( inst ) , sano ( inst ) , tokai pharmaceuticals ( inst ) , eli lilly / imclone ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , roche ( inst ) dong shen employment : janssen research & development stock and other ownership interests : janssen research & development deborah ricci employment : janssen stock and other ownership interests : janssen patents , royalties , other intellectual property : janssen ( inst ) travel , accommodations , expenses : janssen michael gormley employment : janssen research & development stock and other ownership interests : johnson & johnson patents , royalties , other intellectual property : i have several patents pending where i am listed as the inventor of things that have been developed in the course of my work at janssen research and development ( inst ) travel , accommodations , expenses : janssen research & development axel s . 
merseburger honoraria : janssen - cilag , astellas pharma , ipsen , roche , bristol - myers squibb , eisai , takeda , pzer , novartis consulting or advisory role : msd oncology , bristol - myers squibb , janssen - cilag , astellas pharma , ipsen speakers bureau : ipsen research funding : novartis ( inst ) , astrazeneca ( inst ) , janssen - cilag ( inst ) , bristol - myers squibb ( inst ) , clovis oncology ( inst ) travel , accommodations , expenses : janssen - cilag , astellas pharma , ipsen bertrand tombal honoraria : amgen , astellas pharma , bayer , ferring , sano , janssen , pzer , myovant sciences consulting or advisory role : astellas pharma , bayer , ferring , janssen , takeda , steba biotech , sano speakers bureau : amgen , janssen research funding : ferring ( inst ) travel , accommodations , expenses : amgen , astellas pharma , bayer , ferring , janssen , sano ugo de giorgi consulting or advisory role : pzer , janssen , astellas pharma , sano , bristol - myers squibb , bayer , ipsen , merck research funding : sano ( inst ) , astrazeneca ( inst ) , roche ( inst ) travel , accommodations , expenses : bristol - myers squibb , ipsen , janssen , pzer enrique gonzalez - billalabeitia travel , accommodations , expenses : bristol - myers squibb , pzer , bristolmyers squibb , janssen - cilag , astellas pharma , sano , roche , pzer alexander w . 
wyatt consulting or advisory role : genzyme speakers bureau : janssen research funding : janssen gerhardt attard honoraria : janssen , astellas pharma , janssen ( i ) consulting or advisory role : janssen - cilag , veridex , ventana medical systems , astellas pharma , medivation , novartis , millennium , abbott laboratories , essa , bayer , pzer speakers bureau : janssen , astellas pharma , takeda , sano , ventana medical systems research funding : janssen ( inst ) , arno therapeutics ( inst ) , innocrin pharma ( inst ) patents , royalties , other intellectual property : i am on the institute of cancer research rewards to inventors list of abiraterone acetate travel , accommodations , expenses : janssen , astellas pharma , medivation , ventana medical systems , abbott laboratories , bayer , essa , janssen ( i ) , astellas pharma ( i ) , pzer other relationship : institute of cancer research no other potential conicts of interest were reported . acknowledgment we thank the study participants and study centers . 
we acknowledge all the staff at the spanish oncology genitourinary group for their support in running the premiere trial and apoyo a la investigacion clinica en espana for data management . references beer tm , armstrong aj , rathkopf de , et al : enzalutamide in metastatic prostate cancer before chemotherapy . 
n engl j med 371 : 424 - 433 , 2014 ryan cj , smith mr , de bono js , et al : abiraterone in metastatic prostate cancer without previous chemotherapy . 
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nat genet 50 : 645 - 651 , 2018 kumar a , coleman i , morrissey c , et al : substantial interindividual and limited intraindividual genomic diversity among tumors from men with metastatic prostate cancer . 
nat med 22 : 369 - 378 , 2016 kallio hml , hieta r , latonen l , et al : constitutively active androgen receptor splice variants ar - v3 , ar - v7 and ar - v9 are co - expressed in castration - resistant prostate cancer metastases . 
conteduca v , wetterskog d , sharabiani mta , et al : androgen receptor gene status in plasma dna associates with worse outcome on enzalutamide or abiraterone for castration - resistant prostate cancer : a multi - institution correlative biomarker study . 
annala m , vandekerkhove g , khalaf d , et al : circulating tumor dna genomics correlate with resistance to abiraterone and enzalutamide in prostate cancer . cancer discov 8 : 444 - 457 , 2018 13 . 
attard g , merseburger as , arlt w , et al : assessment of the safety of glucocorticoid regimens in combination with abiraterone acetate for metastatic castrationresistant prostate cancer : a randomized , open - label phase 2 study . 
halabi s , lin cy , kelly wk , et al : updated prognostic model for predicting overall survival in rst - line chemotherapy for patients with metastatic castrationresistant prostate cancer . 
chi kn , kheoh t , ryan cj , et al : a prognostic index model for predicting overall survival in patients with metastatic castration - resistant prostate cancer treated with abiraterone acetate after docetaxel . 
rathkopf de , smith mr , de bono js , et al : updated interim efcacy analysis and long - term safety of abiraterone acetate in metastatic castration - resistant prostate cancer patients without prior chemotherapy ( cou - aa - 302 )  . 
ryan cj , smith mr , fizazi k , et al : abiraterone acetate plus prednisone versus placebo plus prednisone in chemotherapy - naive men with metastatic castrationresistant prostate cancer ( cou - aa - 302 ) : final overall survival analysis of a randomised , double - blind , placebo - controlled phase 3 study . 
armstrong aj , lin p , higano cs , et al : development and validation of a prognostic model for overall survival in chemotherapy - nave men with metastatic castration - resistant prostate cancer . 
de laere b , oeyen s , mayrhofer m , et al : tp53 outperforms other androgen receptor biomarkers to predict abiraterone or enzalutamide outcome in metastatic castration - resistant prostate cancer . 
de laere b , van dam pj , whitington t , et al : comprehensive proling of the androgen receptor in liquid biopsies from castration - resistant prostate cancer reveals novel intra - ar structural variation and splice variant expression patterns . 
loriot y , eymard jc , patrikidou a , et al : prior long response to androgen deprivation predicts response to next - generation androgen receptor axis targeted drugs in castration resistant prostate cancer . 
bellmunt j , kheoh t , yu mk , et al : prior endocrine therapy impact on abiraterone acetate clinical efcacy in metastatic castration - resistant prostate cancer : post - hoc analysis of randomised phase 3 studies . 
hung j , taylor ar , divine gw , et al : the effect of time to castration resistance on outcomes with abiraterone and enzalutamide in metastatic prostate cancer . clin genitourin cancer 14 : 381 - 388 , 2016 26 . 
wang l , dehm sm , hillman dw , et al : a prospective genome - wide study of prostate cancer metastases reveals association of wnt pathway activation and increased cell cycle proliferation with primary resistance to abiraterone acetate - prednisone . 
antonarakis es , lu c , luber b , et al : clinical signicance of androgen receptor splice variant - 7 mrna detection in circulating tumor cells of men with metastatic castration - resistant prostate cancer treated with rstand second - line abiraterone and enzalutamide . 
scher hi , graf rp , schreiber na , et al : assessment of the validity of nuclear - localized androgen receptor splice variant 7 in circulating tumor cells as a predictive biomarker for castration - resistant prostate cancer . 
torquato s , pallavajjala a , goldstein a , et al : genetic alterations detected in cell - free dna are associated with enzalutamide and abiraterone resistance in castration - resistant prostate cancer . 
baseline characteristics of pcr2023 cohort by ar status abiraterone chemotherapy naive ( n = 133 ) ar normal ( n = 111 , 83.5% ) ar gain ( n = 22 , 16.5% ) characteristic median age , years ( range ) median pretreatment psa , mg / l ( range ) median pretreatment ldh , uln ( range ) median pretreatment alp , uln ( range ) site of metastases , no . 
malignant cells have a high proliferative fraction and typically express b - cell lymphoma 2 ( bcl2 ) , interferon regulatory factor 4 ( irf4 ) , and b - cell lymphoma 6 ( bcl6 ) on immunohistochemistry . gene expression proling is associated with constitutive nuclear factor ( nf ) - b pathway activation and up - regulation of apoptosis - inhibiting genes , similar to ndings in abc dlbcl . 
mutations of myd88 , resulting in constitutive nf - b activation , are reported in pbdlbcl - lt in up to 69% of cases6 , 7 and are associated with a worse clinical outcome.7 apoptosis gene expression proling in pcdlbcl - lt has shown not only high expression levels of antiapoptotic genes but also concomitant downstream inhibition of the intrinsic apoptosis pathway , as reported in chemotherapy - refractory nodal abc dlbcl.8 , 9 treatment of relapsed / refractory pcdlbcl - lt remains a signicant challenge , with many patients succumbing to uncontrolled disease.3 current therapeutic options , including access to clinical trials , are limited because of both the rarity of disease and the often frail , comorbid patient population . 
small case series of patients with myd88 - mutated pcdlbcl - lt have demonstrated responses to inhibition of b cell receptor ( bcr ) signaling via bruton 's tyrosine kinase ( btk ) inhibition , although responses are of short duration ( 4 to 40 weeks ) and associated with rapid emergence of resistance - conferring mutations.10 , 11 the efcacy of the specic bcl2 inhibitor venetoclax in pcdlbcl - lt remains unexplored . 
this study was approved by the university hospitals of leicester nhs trust ( uk ; 06 / q2501 / 122 )  . research and development written informed consent was obtained for publication purposes . expression of cd20 , cd79a , paired box 5 ( pax5 ) , bcl2 , bcl6 , irf4 , and cd10 , with a ki67 fraction of 90% ( figs 1a - 1d )  . 
 ( a ) hematoxylin and eosin staining , ( b ) interferon regulatory factor 4 ( irf4 ) , ( c ) b - cell lymphoma 2 ( bcl2 ) , and ( d ) ki67 expression . 
in 2010 , he relapsed again with left leg cutaneous involvement only , adjacent to the previously treated sites , and received additional treatment with four cycles of r - chop and radiotherapy ( 40 gy in 15 fractions ) , again attaining clinical response . 
two additional relapses in the left leg with progressively shorter disease - free intervals were treated with radiotherapy alone in 2011 and 2012 ( 4 gy , single fraction )  . 
subsequently , in 2016 , an additional relapse , treated with rituximab , gemcitabine , cyclophosphamide , vincristine , and prednisolone , was refractory to chemotherapy . because of high expression of bcl2 and the development of chemorefractory disease , in january 2017 we obtained venetoclax through the uk abbvie compassionate access scheme . 
repeat staging by ct and 18f - labeled uorodeoxyglucosepositron emission tomography / ct scans conrmed that disease remained localized to the left lower leg , as shown in figure 1e . 
the dose of venetoclax was escalated to 1 , 200 mg because of published data in dlbcl and follicular lymphoma conrming safety and tolerability of this dose.12 however , 1 , 200 mg was not tolerated because of persistent grade 2 diarrhea and grade 2 fatigue , and thus 800 mg was adopted as a maintenance dose . 
biopsy after 2 weeks of treatment showed a complete histologic and immunohistochemical response , although ighv polymerase chain reaction showed persistence of clonal b cells ( data not shown )  . 
treatment with venetoclax was stopped 1 month after demonstration of metabolic remission . however , within 4 weeks of stopping venetoclax , disease recurred , once again conned to the left lower leg , but at different anatomic sites . 
an additional biopsy was performed , which conrmed relapsed disease and showed persistent high - level bcl2 expression ( data not shown )  . venetoclax was recommenced at a dose of 400 / 800 mg on alternate days , with only mild gastrointestinal ( gi ) toxicity ( grade 1 common terminology criteria for adverse events )  . eighteen months later , with continued daily venetoclax , his disease remains in complete remission . whole - exome dna sequencing was performed only on the last relapse sample because of a lack of suitable material from prior biopsies . 
call thresholds were a minimum of 10 variant reads , depth 25 reads , variant allele frequency 10% , scale - invariant feature transform score less than 0.35 , polyphen greater than 0.7. 
potential genetic drivers of this malignancy included previously described arid1a and notch2 mutations ( table 1 ) , as well as biallelic deletion of rb1 and cdkn2a and monoallelic loss of tp53 ( fig 2 )  . 
 ( a , b ) somatic copy number analysis of the tumor biopsy was carried out using varscan and sequenza programs against patient germline dna . frequency of copy number ( log2 ratio ) obtained by pairwise comparison of read depths along the sequenced exome . 
dyer honoraria : roche pharma ag , abbvie , sandoz speakers ' bureau : roche research funding : roche ( inst ) , gilead sciences ( inst ) , astex pharmaceuticals ( inst ) , bioinvent ( inst ) travel , accommodations , expenses : abbvie no other potential conicts of interest were reported . references sokol l , naghashpour m , glass lf : primary cutaneous b - cell lymphomas : recent advances in diagnosis and management . 
blood 105 : 3768 - 3785 , 2005 grange f , beylot - barry m , courville p , et al : primary cutaneous diffuse large b - cell lymphoma , leg type : clinicopathologic features and prognostic analysis in 60 cases . 
arch dermatol 143 : 1144 - 1150 , 2007 vermeer mh , geelen fa , van haselen cw , et al : primary cutaneous large b - cell lymphomas of the legs . 
arch dermatol 132 : 1304 - 1308 , 1996 senff nj , noordijk em , kim yh , et al : european organization for research and treatment of cancer and international society for cutaneous lymphoma consensus recommendations for the management of cutaneous b - cell lymphomas . 
 successful treatment with single - agent venetoclax pham - ledard a , cappellen d , martinez f , et al : myd88 somatic mutation is a genetic feature of primary cutaneous diffuse large b - cell lymphoma , leg type . j invest dermatol 132 : 2118 - 2120 , 2012 pham - ledard a , beylot - barry m , barbe c , et al : high frequency and clinical prognostic value of myd88 l265p mutation in primary cutaneous diffuse large b - cell lymphoma , leg - type . 
jama dermatol 150 : 1173 - 1179 , 2014 cillessen sa , hess cj , hooijberg e , et al : inhibition of the intrinsic apoptosis pathway downstream of caspase - 9 activation causes chemotherapy resistance in diffuse large b - cell lymphoma . 
clin cancer res 13 : 7012 - 7021 , 2007 van galen jc , hoefnagel jj , vermeer mh , et al : proling of apoptosis genes identies distinct types of primary cutaneous large b cell lymphoma . 
fox lc , yannakou ck , ryland g , et al : molecular mechanisms of disease progression in primary cutaneous diffuse large b - cell lymphoma , leg type during 11 . 
davids ms , roberts aw , seymour jf , et al : phase i rst - in - human study of venetoclax in patients with relapsed or refractory non - hodgkin lymphoma . 
li l , pongtornpipat p , tiutan t , et al : synergistic induction of apoptosis in high - risk dlbcl by bcl2 inhibition with abt - 199 combined with pharmacologic loss 14 . 
paulli m , lucioni m , maf a , et al : primary cutaneous diffuse large b - cell lymphoma ( pcdlbcl ) , leg - type and other : an update on morphology and treatment . 
 prospective longitudinal ctdna workow reveals clinically actionable alterations in ovarian cancer jaana oikkonen , phd1 ; kaiyang zhang , msc1 ; liina salminen , md2 ; ingrid schulman1 ; kari lavikka1 ; noora andersson , phd1 ; erika ojanper a1 ; sakari hietanen , md , phd2 ; seija gr enman , md , phd2 ; rainer lehtonen , phd1 ; kaisa huhtinen , phd3 ; olli carp en , md , phd1 , 3 , 4 ; johanna hynninen , md , phd2 ; anniina f arkkil a , md , phd1 , 4 , 5 ; and sampsa hautaniemi , d tech1 purpose circulating tumor dna ( ctdna ) detection is a minimally invasive technique that offers dynamic molecular snapshots of genomic alterations in cancer . 
although ctdna markers can be used for early detection of cancers or for monitoring treatment efcacy , the value of ctdna in guiding treatment decisions in solid cancers is controversial . 
we applied the workow to a prospective cohort consisting of 78 ctdna samples from 12 patients with high - grade serous ovarian cancer before , during , and after treatment . these longitudinal data sets were analyzed using our open - access ctdna - tailored bioinformatics analysis pipeline and in - house translational oncology knowledgebase to detect clinically actionable genomic alterations . 
the alterations were ranked according to the european society for medical oncology scale for clinical actionability of molecular targets . results our results show good concordance of mutations and copy number alterations in ctdna and tumor samples , and alterations associated with clinically available drugs were detected in seven patients ( 58% )  . treatment of one chemoresistant patient was changed on the basis of detection of erbb2 amplication , and this ctdna - guided decision was followed by signicant tumor shrinkage and complete normalization of the cancer antigen 125 tumor marker . conclusion our results demonstrate a proof of concept for using ctdna to guide clinical decisions . 
analysis of circulating tumor dna ( ctdna ) is an approach with the potential of overcoming all three obstacles.1 indeed , ctdna sampling is a clinically attractive , minimally invasive technique that is based on the observation that tumor cells leak dna to the bloodstream , where it can be captured by genomic assays . 
 oikkonen et al context key objective the aim of the study was to identify the clinical usefulness of circulating tumor dna ( ctdna ) in the treatment of high - grade serous ovarian cancer ( hgsoc ) and to provide a clinical workow for reliable detection of ctdna alterations . knowledge generated we show that longitudinal ctdna sampling can be used to detect response to platinum - taxane primary therapy after the rst cycles of chemotherapy and to identify clinically applicable mutations and copy number alterations . 
in one patient with chemoresistant hgsoc , ctdna - guided treatment including trastuzumab was administered during tumor progression and yielded tumor shrinkage . relevance the early detection of poor - responding patients allows the design of alternative treatment strategies in hgsoc . 
especially for platinum - resistant patients who have limited treatment options , rapid discovery of resistant cell populations can provide an early opportunity to interfere with the development of recurrence . 
this is a substantial improvement in the management of recurrent solid cancers , where tumors are not usually sampled either because of the risk of potential intervention complications or simply because the sample could be insufcient or not representative of the disease . ctdna analysistailored bioinformatics pipelines , and a translational oncology knowledgebase to identify clinically actionable mutations and copy number alterations ( cnas )  . 
we demonstrate the usefulness of this approach in high - grade serous ovarian cancer ( hgsoc ) , which is the most common and aggressive form of epithelial ovarian cancer , with a 5 - year survival rate of 43%.7 the current standard - of - care therapy for advanced hgsoc consists of cytoreductive surgery and platinum - paclitaxel chemotherapy.8 although the initial response to standard - of - care therapy is usually good , nearly all patients eventually relapse and have limited treatment options . 
the samples were stored at 80c as 1 to 2 ml aliquots frozen less than 2 hours after collection to avoid lysis of the white blood cells.1 cell - free dna ( cfdna ) was extracted from plasma samples and subjected to 1000 targeted illumina hi - seq sequencing at bgi ( bgi europe a / s , copenhagen , denmark ) using the oseq solid cancer panel with more than 500 clinically actionable genes ( data supplement )  . dna was isolated from 21 liquid ln2 snap - frozen tumor tissue and ascites samples ( data supplement ) , as well as from whole blood ( germline ) buffy coat samples , and was sequenced using the oseq panel with coverage of 200 . mutation and copy number detection mutation detection was performed in the computational ecosystem anduril10 using the ctdna data analysis pipeline , which is based on best practices for sequencing data analysis ( data supplement )  . 
filtering steps included detection of likely spurious mutations by identifying clusters of variants shared between patients but not known in cancer , 12 and functionally irrelevant variants by a combined annotation dependent depletion13 score of less than 15 . 
to estimate the change in mutational proles , we identied the largest proportion of signicantly decreased variants during treatment compared with the pretreatment sample ( p , .01 , fishers exact test )  . 
because of varying numbers of mutations in the pretreatment samples , the proportion of signicantly decreased variants was corrected for mutation counts . pathway analysis was performed for genes with a nondecreasing mutation frequency ( p , .01 , fishers exact test ; data supplement ) using the consensuspathdb15 algoriththe consensuspathdb integrates data from 32 databases and allows comprehensive over - representation analysis for mutations . immunohistochemistry and in situ hybridization potentially clinically actionable alterations were validated through immunohistochemistry ( ihc ) and in situ hybridization for alterations classied as most prominent ( escat , the european society for medical oncology scale for clinical actionability of molecular targets ) 16 and shown to exist in patients tumor tissue ( data supplement )  . results ctdna panel reliably captures mutations and cnas we collected 78 longitudinal ctdna samples and 21 tumor tissue samples from 12 unselected patients with hgsoc ( data supplement )  . 
we applied a sequencing panel of more than 500 genes , followed by variant and cna calling , ltering , and prioritization of clinically relevant aberrations as shown in fig 1a and the data supplement . 
altogether , 265 mutations in 185 genes ( data supplement ) and cna aberrations in 113 genes ( data supplement ) passed our calling and ltering criteria . the median concordance of mutations detected from plasma to tumor tissue samples from the same patient was 79% ( fig 1b ; data supplement )  . 
 oikkonen et al 12 patients with hgsoc variant and cna calling targeted sequencing mutation discovery filtering plasma , sampled longitudinally cancer gene panel cna detection germline dna tumor tissue validation clinical application interpretation prioritization early response monitoring vaf dynamics drug relevance translational oncology knowledgebase tumor burden and mutational composition during therapy plasma only shared tissue only patient 12 months 12 months fig 1 . 
pfi , platinum - free interval . ctdna mutation proles reect long - term treatment response and reveal targetable pathways in patients with aggressive hgsoc ctdna allows several ways to monitor treatment response . for hgsoc , parkinson et al4 suggested the use of tp53 measured from ctdna in disease monitoring . 
we observed that , consistent with their results , tp53 vaf was below 0.5% in all except one patient during primary chemotherapy and was increased in all patients at disease progression ( fig 2 )  . 
these results suggest that the changes in vafs detected from ctdna samples can be used for the early identication of patients with poor response to chemotherapy . we hypothesized that genes whose mutation vafs remained stable or increased during treatment in poor responders could reveal pathways crucial for chemoresistance . 
pathways enriched in the poor - responding patients in comparison with the good - responding patients included transcription , p53 , and chromatin regulatory pathways and dna double - strand break repair pathways ( data supplement )  . 
these alterations are predicted to cause sensitivity to cdk2 / 425 and / or cdk4 / 6 inhibitors.26 regardless of the presence of hr - deciencyconferring alterations , this patient , who had no residual tumor after surgery , progressed 8.9 months after the last platinum cycle . ctdna identies actionable mutations in patients with hgsoc we prioritized and interpreted all 265 mutations and 113 cnas using the translational oncology knowledgebase , which integrates information from 11 databases and 14 scientic articles ( data supplement )  . 
the knowledgebaseprioritized mutations and cnas revealed four major targetable processes : mammalian target of rapamycin ( mtor ; patients eoc429 , eoc49 ) , dna repair ( patients eoc429 , eoc677 , and eoc1067 ) , epidermal growth factor receptor ( egfr ; patients eoc587 , eoc736 , and eoc568 ) , and cyclin dependent kinases ( cdks ; patient eoc1067 )  . the highest allele frequency mutations matching tumor content were detected in pten ( patient eoc49 ) and nf1 ( patient eoc429 ) , which cause overactivation of the mtor pathway.20 , 22 patients with the activated mtor pathway have been shown to be responsive to phosphatidylinositol 3 - kinase / mtor inhibitors.22 we validated overactivity of the mtor pathway in the two patients with ihc from tumor tissue samples ( fig 3 ; data supplement )  . 
in patient eoc49 , pten mutation vaf in omentum ( 8% and 6% for pretreatment and interval samples , respectively ) and plasma matched the pattern of tp53 mutation , indicating that tumor cells and presents an early event in tumor evolution ( data supplement )  . 
pten was detected in a follow - up sample at 8 months after primary treatment with vaf of 0.1% , conrming its persistence during therapy . the pten mutation exists in all we observed mutations and cnas in genes associated with dna repair in three patients . 
in patient eoc677 , we detected mutations in brca2 and stag2 , which potentially confer homologous recombination ( hr ) dna repair deciency and sensitivity to poly - adp ribose polymerase ( parp ) inhibitors . however , the frequencies of these mutations were low in the tumor tissues ( 0.2% for brca2 and 3.1% for stag2 ) , suggesting subclonal events . 
in patient eoc429 , we detected a germline deletion in rad51c from plasma , which has been shown to confer hr deciency and parp inhibitor sensitivity , 21 and , consistent with this , the patient had a prolonged response to platinum - based chemotherapy . 
we also detected a somatic deletion of fanca in patient three patients had mutations or cnas associated with sensitivity to drugs targeting the epidermal growth factor receptor ( egfr ) pathway . 
patient eoc568 had an erbb4 mutation , which is predicted to confer sensitivity to egfr inhibitors.27 patient eoc587 had a mapk mutation and a simultaneous mapk1 amplication , which are associated with resistance to the egfr targeting therapies.28 , 29 we detected a high copycount erbb2 amplication in the ctdna in patient eoc736 . the erbb2 locus is amplied in 3% to 11% of hgsocs30 , 31 and is a predictive biomarker for trastuzumab . 
the erbb2 amplication was validated in primary omentum tissue using snp genotypebased cna detection and in the tumor tissue sample from interval debulking surgery with in situ hybridization and ihc ( figs 4a and 4b )  . patient eoc736 was treated with nact , and she participated in a clinical trial after primary treatment , receiving maintenance bevacizumab and olaparib or placebo ( fig 4c )  . 
although she had a clinical and radiologic complete response to primary therapy , tp53 vaf remained detectable throughout the treatment , which , on the basis of our ndings , indicates a poor response to platinum taxane ( data supplement )  . 
this patient also suffered from severe paclitaxel - induced neuropathy after primary treatment , and therefore , pegylated liposomal doxorubicin ( pld ) was started at the rst relapse instead of dose - dense paclitaxel therapy . 
pld was discontinued after four cycles because of constantly rising ca125 ( from 193 to 769 ) and progression in lymph nodes as evidenced by a computed tomography scan . the erbb2 amplication detected in on the basis of ctdna , treatment of patient eoc736 was changed to trastuzumab 600 mg subcutaneously once every 3 weeks , combined with reduced doses of carboplatin ( auc4 ) and dose - dense paclitaxel ( 80 mg / m2 on days 1 and 8 )  . 
the patient responded to this combination well , and a biochemical complete response ( ca - 125 value reduced from 840 iu / ml to 19 iu / ml ) was achieved after only three treatment cycles ( fig 4c )  . 
pathogenic mutation in nf1 was detected in circulating tumor dna ( ctdna ) , leading to functionally overactive mammalian target of rapamycin ( mtor ) signaling in the tumor tissue . 
 ( a ) mutational frequencies in a good - responding patient ( eoc429 ) during primary treatment and follow - up . variant allele frequency ( vaf ) values are normalized for the frequency level to show relative changes in the levels . 
 ( b ) mtor pathway activation was detected in primary tumor tissue with higher staining for phosphorylated mtor ( pmtor ) and e4 - bp1 compared with normal ovarian tissue . 
scale bar , 100 m ( c ) in addition to having a complete response on the basis of recist 1.1 , the response to primary therapy was good , as indicated by cancer antigen 125 ( ca - 125 ) values that stayed low during treatment and follow - up . 
cadd , combined annotation dependent depletion ; hgsoc , high - grade serous ovarian cancer ; pte , primary treatment end ; 4e - bp , 4e - binding protein . sequencing of more than 500 genes from liquid biopsies , a ctdna data analysis pipeline , and a translational oncology knowledgebase to enable longitudinal analysis of ctdna during therapy and guide personalized cancer treatment decisions . 
the ctdna analysis pipeline and translational oncology knowledgebase are open - source and available with documentation ( data supplement )  . we detected high ctdnatumor congruence , which , together with the absence of alterations from the blood cells used as germline samples and comprehensive ltering of mutations through clustering , maximizes the likelihood that the reported alterations originated from tumor and not from other sources , such as clonal hematopoiesis.1 indeed , our ltering approach using longitudinal samples removed false - positive alterations in all patients . 
rara was within the amplied region in plasma but not in primary omentu ( b ) erbb2 protein was overexpressed in cancer tissue ( arrowheads ) in immunohistochemistry ( ihc ) and the erbb2 gene was amplied in dna in situ hybridization ( ish ) analysis ( scale bars , 20 mm )  . 
the most informative comparisons for predicting treatment outcome are samples at the preoperative stage , after two cycles of chemotherapy , and after debulking surgery , because they provide information on treatment response and on persisting tumor subclones we identied potentially clinically applicable mutations or cnas in more than one half of the patients with hgsoc . these included two patients with mtor pathwayactivating mutations that were validated . 
both patients had a good response to the platinum - based rst - line therapy , but in the case of relapse they could most likely benet from mtor inhibitors alone or in combination with chemotherapy.22 in patient eoc429 , we identied alterations conferring both mtor pathway activation and hr deciency , which suggests potential benet from combination treatment with , for example , mtor inhibition and parp inhibition . 
in addition , two patients had more than one concurrent , potentially targetable alteration . patient eoc1067 progressed after 9 months of platinum - based therapy despite the fanca deletion conferring hr deciency , potentially because of the contribution of the cdk alterations on cell - cycle regulation and tumor progression.32 on the basis of the concurrent ckdn1b and ckdn2b deletions , this patient could potentially benet from a combination targeting both pathways , for instance , parp inhibitor and cdk4 / 6 inhibitor . these results indicate that longitudinal ctdna sampling can detect and monitor a relapse at an early stage and identify potentially effective drug combinations . we identied a high - condence erbb2 amplication in the ctdna of a patient with platinum - resistant hgsoc and used this information to change the patients treatment to include trastuzumab with reduced doses of platinum and paclitaxel . 
thus , rapid response to the ctdna - guided treatment , detected by complete normalization of ca - 125 values within 2 months after starting the combination treatment , was surprising . 
earlier studies that have combined erbb2 inhibitors with platinum and paclitaxel report similar encouraging responses for relapsed patients with advanced hgsoc.31 although the number of patients in these studies and our study remains small because of the low number of patients with erbb2 - amplied hgsoc , these results warrant testing erbb2 amplication from relapsed hgsoc patients with advanced disease . ctdna sampling and sequencing with a large panel offers several benets to physicians . 
for a detailed description of the disclosure categories , or for more information about ascos conict of interest policy , please refer to or po.ascopubs.org / site / ifc sakari hietanen consulting or advisory role : tesaro , astrazeneca travel , accommodations , expenses : roche pharma ag olli carp en stock and other ownership interests : orion corporation honoraria : merck kgaa , roche pharma ag sampsa hautaniemi stock and other ownership interests : nanostring technologies no other potential conicts of interest were reported . acknowledgment we thank the patients who participated in this study , dr tuulia vallius and dr zoltan maliga for critical review of the manuscript , ma tiia pelkonen for proof reading , and the csc - it center for science ltd . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
j clin oncol 36 : 1631 - 1641 , 2018 khan kh , cunningham d , werner b , et al : longitudinal liquid biopsy and mathematical modeling of clonal evolution forecast time to treatment failure in the prospect - c phase ii colorectal cancer clinical trial . 
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science359 : 926 - 930 , 2018 parkinson ca , gale d , piskorz am , et al : exploratory analysis of tp53 mutations in circulating tumour dna as biomarkers of treatment response for patients with relapsed high - grade serous ovarian carcinoma : a retrospective study . 
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wright aa , bohlke k , armstrong dk , et al : neoadjuvant chemotherapy for newly diagnosed , advanced ovarian cancer : society of gynecologic oncology and american society of clinical oncology clinical practice guideline . 
mateo j , chakravarty d , dienstmann r , et al : a framework to rank genomic alterations as targets for cancer precision medicine : the esmo scale for clinical actionability of molecular targets ( escat )  . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
cen l , carlson bl , schroeder ma , et al : p16 - cdk4 - rb axis controls sensitivity to a cyclin - dependent kinase inhibitor pd0332991 in glioblastoma xenograft cells . biol 19 : 1371 - 1378 , 2017 2013 2015 27 . 
 precision medicine across the cancer continuum : implementation and implications for cancer disparities advances in health care , including genomic technologies and reduction in the cost of dna sequencing , create new opportunities and implications for individualized health care regarding the potential for specific treatments based on a persons genetic makeup . 
precision oncology discoveries and implementation can be extended across the cancer continuum , from individualized screening recommendations to targeted treatments based on a persons risk profile encompassing genetic , environmental , and / or behavioral factors.4 although the concept of precision medicine may not be entirely new , its visibility has increased considerably with initiatives such as the all of us precision medicine research program5 supported by the us governments investment of $70 million . summarized by collins and varmus , 6 the goal of this initiative is to lay the groundwork for ultimately developing treatment strategies based on the specific characteristics of an individuals tumor , with eventual application to other chronic diseases . 
importantly , the all of us research program includes a focus on patient engagement , which will be critical to its success in reaching goals such as the recruitment of 1 million americans to provide the level and types of data necessary to understand the clinical impact of precision medicine . with the implementation of precision medicine comes a concomitant need for ethically responsible and effective communication strategies to clearly convey this benefit to patients . 
a recent study examined communication between genetic counselors and patients and reported a mismatch ( eg , too much information , not the right kind of information ) between the information provided by the counselors and the understanding and preferences of the audience.7 there is confusion among clinicians about how to use genomic data at the point of care8 ; thus , with greater implementation of precision medicine approaches will come a need for clinician training about how best to apply these approaches and communicate their potential benefits ( and risks ) to patients.4 at present , it is not clear how well the clinical and public health communities are prepared to communicate about precision medicine to patients , particularly those with limited resources , education , or health literacy . 
holt , university of maryland , college park ; arif hussain , robert wachbroit , and jessica scott , university of maryland , baltimore , md . corresponding author : cheryl l . 
 recent studies3 , 9 have suggested an important role for implementation science , and chambers et al9 extended this to include the role of the learning health care system , a concept advocated by the institute of medicine , in successfully implementing precision medicine . 
implementation science can provide theories , methods , and guidance for examining issues such as the role of context ( eg , diverse array of health care systems ) in implementing precision medicine , identification of influences on evidence - based practice usage , and implementation strategies . 
implementation issues will likely arise around the recommendation of wearable devices and ecological momentary assessment , 10 which , again , will benefit from community engagement and a multidisciplinary approach to implementation . a 2015 commentary by riley et al10 recommends involvement of behavioral and social sciences because of the potential impact of behavioral and environmental factors in determining responsiveness to treatment . 
it is likely that as precision medicine is implemented on a population scale , disciplines such as economics , health services research , behavioral medicine , communication , public health , and psychology will become increasingly relevant . we believe it is critical to take a patient - centered perspective on precision medicine in particular , because it involves different treatments for different people , which , for minorities and the poor , could amplify feelings of mistrust in the medical system and could result in adverse medical outcomes . 
similar to the confusion that was created when the us preventive service task force made changes in recommendations to cancer screening guidelines , 11 the complexity of precision medicine has the potential to significantly magnify medical mistrust . 
continuous patient engagement involves actively listening to and incorporating patient perspectives through all phases of research , including selecting and prioritizing research topics and questions , identifying appropriate outcomes , weighing in on data collection methods , and helping interpret and disseminate results.12 in the context of precision oncology and disparities , patient engagement may involve the inclusion of individuals from under - represented groups on research advisory boards so that they can help prioritize cancers they think impact their communities most , provide input on acceptable ways to communicate precision oncology - based treatment strategies , and ensure patient representation and recruitment in clinical trials while minimizing risk and maximizing benefit . advances in precision medicine are likely to benefit the medically underserved last and could increase existing health disparities.3 , 4 this may be particularly true in circumstances where precision medicine relies on clinical samples and / or data from electronic medical records , because people with no regular source of care could be excluded.13 there are several pathways by which the implementation of precision oncology could widen cancer disparities . 
first , to the extent that discoveries in precision oncology are based on a majority population ( eg , white people ) , findings may not generalize to minorities ( eg , african americans , hispanic / latino , and asian americans ) ; thus , these groups may not reap as much benefit . 
second , there are likely to be geographic ( eg , urban , rural ) , demographic ( eg , race , ethnicity , age , sex ) , and socioeconomic ( eg , income , education , neighborhood context ) differences in the trajectory at which precision oncology approaches become available to patients . 
this is illustrated in a report of a sample of rural and appalachian physicians in which 66% indicated that accessing a genetic counselor was somewhat or extremely difficult.14 it was reported that most patients living in a rural area would have to travel to an academic medical center to access genetic counseling services , creating a financial and psychological burden.15 third , there could be a gradient among patients most likely to be served by or willing to participate in precision oncology , starting with early adopters , the most affluent and insured , followed by the poor and people without health insurance at the other end of the spectrum . paradoxically , the poor suffer the greatest burden of cancer disparities and may be most in need of precision approaches to cancer screening and treatment , but this group is more likely to be left behind . 
among the several factors that are particularly pertinent to the poor in terms of increasing their cancer risk are an unhealthy diet beginning in childhood , 16 living in areas considered food deserts or areas with greater environmental exposures to carcinogens resulting in chronic stress and allostatic load , 16 and greater tobacco use.17 the poor are more likely to be negatively affected by factors such as housing segregation , 18 and health care access has recently become uncertain with possible changes to the affordable care act . 
given these challenges , it is apparent that the poor and those in rural areas would be among the last to have access to and reap the potential benefits of precision oncology . responsibilities of patients , insofar as they have a responsibility for their own care , by obligating them to undergo genetic tests and to inform health professionals of their results when appropriate . we have several suggestions for the field of precision oncology to move forward in consideration of cancer disparities . 
as an initial step , we need to gain a better understanding of what precision medicine and precision oncology mean to different stakeholders such as clinicians and patients . through stakeholder engagement , including a patient - centered approach , diverse voices should be considered at both the provider and the recipient levels . 
knowledge and acceptability should be determined as precursors to implementation . we currently know almost nothing about what people in the community know , particularly medically underserved people or those low in health literacy , nor do we know how they feel about precision medicine and how they will respond to its ever - growing application in clinical settings.4 similarly , we know little about the perspective of cancer clinicians and cancer researchers on precision oncology and how this may influence educating patients and guiding treatments , particularly in underserved patient populations . precision medicine promises to identify therapies and drugs that are tailored to the individual patients genetic makeup or their tumor and other patient - specific factors . 
because much of this promise relies on information obtained from the genetic testing or sequencing of the individual patient , many of the ethical issues raised by genetic testing ( eg , concerns about misuse of genetic information ) carry over to the implementation of precision medicine . 
does the advent of precision medicine mean that no physician should treat a patient with certain drugs ( eg , clopidogrel ) without first a genetic analysis indicating whether the patient is a good metabolizer of that drug ? precision medicine may involve a different configuration of physician and patient responsibilities . 
for example , precision medicine may shape the responsibilities of clinicians toward their patients by obligating them to know the results from genetic tests before treatment and to work closely with genetic counselors to inform patients of their vulnerabilities and treatment options . 
indeed , there could be some things that certain patients may not want to know about ( eg , genetic risk for cancer ; predisposition to disease )  . this could also include nonmedical information such as a discovery of nonpaternity . 
although there might be a predisposition among physicians not to disclose information that the patient does not want to know , this can challenge the professionals responsibilities and obligations , especially if the information is clinically actionable . in summary , we recommend that those in the field of precision oncology make a concerted effort to consider cancer disparities , not only by including diverse participant / patient groups but also by pursuing research questions that consider diversity . 
for instance , such questions might include the examination of targeted therapies for triple negative breast cancer in black women and advancing research on biologic explanations for why black men are more likely to die of prostate cancer than white men . 
in the face of large epidemiologic trials suggesting little benefit from prostate cancer screening , there remains a challenging question about what black men can do about prostate cancer mortality , especially if they have a family history . culturally appropriate strategies and messaging will need to be developed and evaluated to communicate about precision medicine with patients , and providers will need training and increased knowledge to be able to effectively integrate precision medicine into their practices . 
we recommend community and patient engagement as part of future precision oncology research in these areas to gain important perspectives relevant to the diverse patient populations that otherwise could be missed . 
holt no relationship to disclose arif hussain consulting or advisory role : novartis , astrazeneca , bayer , bristol - myers squibb research funding : sotio , merck , bayer , agensys , clovis oncology , cerulean pharma robert wachbroit no relationship to disclose jessica scott no relationship to disclose references 1 . 
n engl j med 372 : 793 - 795 , 2015 joseph g , pasick rj , schillinger d , et al : information mismatch : cancer risk counseling with diverse underserved patients . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental findings : results from the canseq study . 
chambers da , feero wg , khoury mj : convergence of implementation science , precision medicine , and the learning health care system : a new model for biomedical research . 
riley wt , nilsen wj , manolio ta , et al : news from the nih : potential contributions of the behavioral and social sciences to the precision medicine initiative . 
gehlert s : precision behavioral medicine in cancer , personalization across the cancer care continuu37th annual meeting and scientific sessions , pre - conference workshop , washington , dc , 2016 14 . 
 immunological differences between immune - rich estrogen receptorpositive and immune - rich triple - negative breast cancers tess omeara , ba1 ; michal marczyk , phd1 , 2 ; tao qing , phd1 ; vesal yaghoobi , md3 ; kim blenman , ms , phd1 ; kimberly cole , md3 ; vasiliki pelekanou , md , phd3 , 4 ; david l . 
we compared expression of immune cell markers , immune function metagenes , and immuno - oncology therapeutic targets among immune - rich subtypes . results relative fractions of resting mast cells ( tcga padj = .009 ; metabric padj = 4.09e - 15 ) , cd8 + t cells ( tcga padj = .015 ; metabric padj = 0.390 ) , and m2 - like macrophages ( tcga padj = 4.68e - 05 ; metabric padj = .435 ) were higher in immune - rich er - positive bcs , but m0 - like macrophages ( tcga padj = 0.015 ; metabric padj = .004 ) and m1 - like macrophages ( tcga padj = 9.39e - 08 ; metabric padj = 6.24e - 11 ) were higher in immune - rich tnbcs . 
ninety - one immune - related genes ( eg , cxcl14 , csf3r , tgf - b3 , lrrc32 / garp , tgfb - r2 ) and a transforming growth factor ( tgf - ) response metagene were signicantly overexpressed in immune - rich er - positive bcs , whereas 41 immune - related genes ( eg , ifng , pd - l1 , ctla4 , magea4 ) were overexpressed in immune - rich tnbcs in both discovery and validation data sets . 
tgfpathway member genes correlated negatively with expression of immune activation markers ( ifng , granzyme - b , perforin ) and positively with m2 - like macrophages ( il4 , il10 , and mmp9 ) and regulatory t - cell ( foxp3 ) markers in both subtypes . conclusion different immunotherapy strategies may be optimal in immune - rich er - positive bc and tnbc . drugs targeting the tgfpathway and m2 - like macrophages are promising strategies in immune - rich erpositive bcs to augment antitumor immunity . jco precis oncol 4 : 767 - 779 . 
 omeara et al context key objective does the immune microenvironment of immune - rich estrogen receptorpositive breast cancer ( er - positive bc ) differ from the immune microenvironment of immune - rich triple - negative bc ( tnbc ) ? knowledge generated relative fractions of mast cells and m2 - like macrophages are higher in the immune microenvironment of immune - rich erpositive bc , whereas fractions of m0 - like and m1 - like macrophages are higher in immune - rich tnbc . 
her2 - positive patients were excluded , and only er - positive / her2 - negative ( herein designated er - positive ; tcga , n = 627 ; metabric , n = 1 , 186 ) and er - negative / her2 - negative ( herein designated tnbc ; tcga , n = 191 ; metabric , n = 279 ) patients were included in this analysis . 
we obtained formalin - xed parafn - embedded tissues from 63 tnbcs and 53 erpositive , treatment - nave , stage i to iii bcs from yale pathology tissue archives , matched by distribution of histologic grade , for quantitative immunouorescence ( qif ) and automated quantitative analysis ( aqua )  . assessment of immune cell content and selection of immune - rich patients a gene expression signature score developed by danaher et al19 was used to score each tcga and metabric patient for total tils . 
the total til gene signature score is the average of scores representing 11 immune cell subpopulations ( cd45 , macrophages , cd8 + t cells , t cells , cytotoxic cells , exhausted cd8 + cells , th1 cells , b cells , neutrophils , natural killer [ nk ] cells , cd56dim nk cells )  . log2 + 1 - transformed expression was used to calculate total til gene signature scores from tcga ( rna - seq ) and metabric ( microarray ) data . 
the til metagene score distribution was plotted for the pooled er - positive bc and tnbc patients , and patients with scores in the top 25th percentile of the distribution were dened as immune - rich . for 156 basal - like cancers in tcga ( er - positive bc , n = 21 ; tnbc , n = 135 ) , histologic til counts were also available.20 , 21 for these patients , we assessed the correlation between histologic til count and til gene expression score . 
we also assessed correlations between til gene signature score and pam50 subtype , tumor mutation burden ( tmb ) , and ki - 67 expression level in the tcga data when this information was available ( er - positive bc , n = 191 ; tnbc , n = 697 )  . 
pam50 subtypes and tmb categories were obtained from a previous publication , and ki - 67 categories were dened as greater than or less than the median log2 + 1 - transformed ki - 67 expression across tcga patients.22 survival analysis progression - free survival ( pfs ) and overall survival ( os ) times were available for 807 tcga patients ( er - positive bcs , n = 189 ; tnbcs , n = 618 ) .23 pfs and os were compared by er subtype within immune - rich patients ( erpositive bcs , n = 114 ; tnbcs , n = 84 ) and within nonimmune - rich patients ( er - positive bcs , n = 504 ; tnbcs , n = 105 ) using the survival and survminer r packages.24 assessment of immune cell subpopulations cibersort , an analytical tool that uses support vector regression , was used to estimate the relative proportions of 9 aggregated immune cell populations and 22 subpopulations in immune - rich er - positive bcs and immunerich tnbcs.25 , 26 the average relative fraction and standard error of the mean of each immune cell population were compared by subtype . 
 immunological differences between immune - rich er - positive bcs and tnbcs calculated gene expression signature scores of overall macrophages , m1 - like macrophages , m2 - like macrophages , and the transforming growth factor ( tgf - ) signaling response were obtained from previous publications and were compared between patients with erpositive bcs and those with tnbcs.27 - 29 slopes of linear regression curves between total tils and metagene expression signatures were compared by using a t test based on standard error in the linear regression models.30 formalinxed parafn - embedded tissue microarrays were stained for the nuclear marker 4 ( cid : 1 ) , 6 - diamidino - 2 - phenylindole and the pan - macrophage marker cd68 , and multiplexed qif and aqua were used to quantify expression levels in yale er - positive bc and tnbc patients as previously described.31 differential gene expression analysis the deseq2 ( tcga , rna - seq data ) and limma ( metabric , microarray data ) r packages were used for differential gene expression analysis of 779 immunerelated genes ( nanostring pancancer io 360 panel , nanostring technologies , seattle , wa ) and 137 currently available immuno - oncology drug target genes between immune - rich er - positive bcs and immune - rich tnbcs.32 - 34 availability of rna expression data for each member gene in tcga and metabric databases is summarized in the data supplement . 
genes with false discovery rate padj , .05 were considered signicantly differentially expressed for a broad investigation of differentially regulated immune pathways . statistical analysis all statistical analyses were performed in r v 3.5.0. 
in tcga , the 75th percentile til metagene score was 5.92 , and it categorized 119 er - positive bcs ( 19% ) and 89 tnbcs ( 45% ) as being immune rich . 
the total til gene signature scores correlated moderately but signicantly with histologic til scores in tcga ( r = 0.44 ; p = 1.18e - 08 ; fig 2a ) when these data were available . 
in tcga , there was no statistically signicant difference between the distribution of pam50 subtypes or ki - 67 expression levels between immune - rich and nonimmune - rich er - positive bcs . 
patients with immune - rich er - positive bcs had signicantly higher tmb than patients with nonimmune - rich er - positive bcs ; this difference was not seen among patients with tnbcs . 
for a subset of tcga patients with available survival formation ( n = 804 ) , pfs and os were compared by subtype ( data supplement )  . immune - rich patients had similar pfs and os regardless of er status . 
in contrast , among the nonimmune - rich cancers , os was signicantly longer in patients with er - positive bcs than in patients with tnbcs ( p = .043 ) , as expected . immune cell subpopulations in the tumor microenvironment of immune - rich er - positive bcs and immune - rich tnbcs by using cibersort , we found higher relative fractions of t cells ( padj = .009 ) and mast cells ( padj = .0005 ) in patients with immune - rich er - positive bcs compared with those who had immune - rich tnbcs ( fig 3a ) in tcga . in patients with immune - rich tnbcs , the relative fractions of macrophages ( padj = .026 ) and nk cells ( padj = .0007 ) were higher relative to those in patients with immune - rich er - positive bcs . 
the higher relative fractions of t cells ( padj = .005 ) and mast cells ( padj = 1.73e - 20 ) in immunerich er - positive bcs and the higher relative fraction of macrophages ( padj = 1.22e - 06 ) in immune - rich tnbcs were also observed in metabric ( fig 3b )  . 
qif also showed higher overall expression of the pan - macrophage marker cd68 in tnbc tissues relative to tissue from erpositive bcs from yale pathology archives ( p = .011 ; fig 3c )  . next , we examined differences among 22 immune cell subpopulations . in immune - rich er - positive tumors in tcga , the relative fractions of cd8 + t cells ( padj = .015 ) and resting mast cells ( tcga padj = .009 ) were higher relative to those in immune - rich tnbc tumors in both data sets ( fig 3d )  . 
in contrast , the relative fractions of m0 - like macrophages ( padj = .015 ) and m1 - like macrophages ( padj = 9.39e - 08 ) were signicantly higher in patients with immune - rich tnbcs compared with those with immunerich er - positive bcs . 
 ( a - b ) gene signature scores were calculated for 11 immune cell subpopulations for patients with er - positive bcs and tnbcs in ( a ) the cancer genome atlas ( tcga ) and ( b ) molecular taxonomy of breast cancer international consortium ( metabric ) databases , as described by danaher et al.19 the x - axis indicates immune cell subpopulations plus the total tumor - inltrating lymphocyte ( til ) population . 
immune - rich erpositive bcs had higher m2 - like macrophage ( p = .012 ) and tgfresponse ( p = 0.035 ) metagene expression scores ( fig 4a )  . 
the subtype - specic differences in m1 - like macrophage ( p = 1.85e - 04 ) and tgfresponse ( p = .029 ) metagene scores signicantly increased with higher total til gene signature scores , whereas the differences in overall macrophage ( p = .786 ) and m2 - like macrophage ( p = .097 ) scores between cancer subtypes were not specic to immune - rich patients ( fig 4b )  . 
 ( a ) for a subset of basal - like patients from the cancer genome atlas ( tcga ) with previously published histologic til scores ( n = 156 ) according to danaher et al , 19 the total til gene signature scores ( x - axis ) were correlated with histologic stromal til counts ( y - axis )  . 
 ( b - d ) for all patients with er - positive bcs ( n = 697 ) and tnbcs ( n = 191 ) in tcga , patients were classied as immune cell high ( danaher et l19 total til gene signature score in the top 25th percentile ) or low ( danaher total til gene signature scores in the bottom 75th percentile ) , represented on the x - axis . 
distributions of ( b ) pam50 subtypes , ( c ) ki - 67 expression categories and ( d ) tumor mutation burden ( tmb ) categories were compared between patients with immune - rich high and low er - positive bcs and tnbcs separately . 
pam50 and tmb categories were obtained from previous publications , and ki - 67 categories were dened as greater than ( high ) or less than ( low ) the median ki - 67 expression level across all patients . differential expression of immune - related genes and immuno - oncology drug target genes between immune - rich er - positive bcs and immune - rich tnbcs at the individual gene level , 132 of 754 immune - related genes were signicantly overexpressed in tcga immunerich er - positive bcs . 
ninety - one of these immune - related genes , including mast cell genes ms4a2 and cpa3 and therapeutic targets cxcl14 , cx3cr1 , and potential csf3r , were also upregulated in metabric patients with immune - rich er - positive bcs ( data supplement )  . immune - rich tnbcs , 303 immune - related genes were overexpressed compared with immune - rich er - positive bcs in tcga , and 218 of these were validated in metabric . 
sixteen of 136 available therapeutic target genes were overexpressed in tcga patients with immune - rich er - positive bcs , and 12 of these , including 3 members of the tgfsignaling pathway ( tgf - 3 , lrrc32 / garp , and tgf - r2 ) , were also overexpressed in metabric patients with immune - rich er - positive bcs ( table 1 ; data supplement )  . 
for patients from ( a ) the cancer genome atlas ( tcga ) and ( b ) molecular taxonomy of breast cancer international consortium ( metabric ) databases , 9 aggregate immune cell populations are listed on the x - axis , and the average fraction of each immune cell population for a certain subtype is quantied on the y - axis . 
 ( c ) quantitative immunouorescence ( qif ) signal was compared between estrogen receptorpositive breast cancer ( er - positive bc ; , n = 53 ) and triple - negative bc ( tnbc ; n = 63 ) formalin - xed parafn - embedded tumor microarray tissues . 
subtype is shown on the x - axis , and cd68 qif signal in the total 4 ( cid : 1 ) , 6 - diamidino - 2 - phenylindole ( dapi ) compartment is quantied on the y - axis . 
for ( d ) tcga and ( e ) metabric patients , 22 immune cell populations derived by cibersort are listed on the x - axis , and the average fraction of each immune cell population for a certain subtype is quantied on the y - axis . 
false discovery rate padj values are provided for tcga ( er - positive bcs , n = 119 ; tnbcs , n = 86 ) and metabric ( er - positive bcs , n = 225 ; tnbcs , n = 140 ) patients . 
comparison of macrophage population and transforming growth factor ( tgf - ) response metagene expression scores between patients with immune - rich estrogen receptorpositive breast cancers ( er - positive bcs ) and those with triple - negative bcs ( tnbcs ) in the cancer genome atlas ( tcga )  . 
 ( a ) metagene expression scores for overall macrophages , m1 - like macrophages , m2 - like macrophages , and tgfresponse were compared between immune - rich er - positive bc ( red , n = 119 ) and immune - rich tnbc ( blue , n = 86 ) patients in tcga . 
 ( b ) for all patients with er - positive bcs ( n = 697 ) and tnbcs ( n = 191 ) in tcga , gene expression signature scores for overall macrophages , m1 - like macrophages , m2 - like macrophages , and tgfresponse ( y - axis ) were plotted against total til gene signature scores ( x - axis )  . 
linear regression lines for each subtype with 95% cis are shown in red ( er - positive bc ) or blue ( tnbc )  . and the cancer - testis antigen , magea4 , were also overexpressed in immune - rich tnbcs in metabric . correlation between tgfpathway expression and other immune - related genes tgfis a pleotropic cytokine that can stimulate regulatory induce m2 - like macrophage polarization , and t cells , suppress effector t cells , nk cells , and dendritic cells . furthermore , tgfsignaling has been linked to an immune - excluded phenotype in cancer . 
we therefore examined correlations between the differentially expressed tgfpathway members ( tgf - 3 , lrrc32 , and tgfr2 ) and the expression levels of the 53 immuno - oncology drug target genes that were differentially expressed in both data sets ( 12 upregulated in immune - rich er - positive bcs , 41 upregulated in immune - rich tnbcs ) across immunerich tnbcs and er - positive bcs . in both tcga and metabric , expression of the tgfpathway members correlated positively with each other and negatively with most immune activation markers ( fig 5a - b ; data supplement )  . 
similar correlation patterns were seen between tgfpathway members and immune activation marker expression when only immune - rich er - positive bcs were analyzed ( fig 5c - d )  . 
we also noted a positive correlation between expression of tgf - 1 and the m2 - like macrophage markers il4 ( r = 0.24 ) , il10 ( r = 0.38 ) , and mmp9 ( r = 0.43 ) as well as the regulatory t - cell marker foxp3 ( r = 0.42 ) in the tcga data . discussion in this report , we used a gene expression signature of total tils to identify patients with immune - rich er - positive bcs and tnbcs in 2 publicly available databases to compare the tumor immune microenvironment of these subtypes . the patients with immune - rich er - positive bcs had signicantly higher tmb than patients with nonimmune - rich er - positive bcs , but no difference in tmb was seen between immune - rich and nonimmune - rich tnbcs . 
for ( a ) the cancer genome atlas ( tcga ) and ( b ) molecular taxonomy of breast cancer international consortium ( metabric ) patients , correlation matrices display the pearson correlation coefcients between expression levels of 53 immuno - oncology drug targets across patients with immune - rich estrogen receptorpositive breast cancers ( er - positive bcs ) and triple - negative bcs ( tnbcs )  . 
for tcga , the number of patients with immune - rich er - positive bcs was 119 , and for tnbcs , it was 86 ; for metabric , the number of patients with immune - rich er - positive bcs was 225 , and for tnbcs , it was 140 . 
for ( c ) tcga and ( d ) metabric patients , correlation matrices display the pearson correlation coefcients between expression levels of 53 immuno - oncology drug targets in patients with immune - rich er - positive bc alone . 
the number of patients with immune - rich er - positive bcs in tcga was 119 , and in metabric , it was 225 . results are consistent with previous reports.11 , 36 approximately 70% of the immune - rich er - positive bcs we identied were luminal a molecular subtype , and the pam50 subtype distribution and ki - 67 expression were similar between immune - rich and nonimmune - rich er - positive bcs . an os difference was detected between patients with nonimmune - rich er - positive bcs relative to nonimmunerich tnbcs , but no similar statistically signicant difference was seen between patients with immune - rich er - positive bcs and immune - rich tnbcs ( both groups had excellent long - term survival )  . 
by using deconvolution methods , we observed differences in the relative fractions of immune cell subpopulations between immune - rich er - positive bcs and immune - rich tnbcs . immune - rich er - positive bcs had higher relative fractions of m2 - like macrophages , cd8 + t cells , and resting mast cell populations , whereas immunerich tnbcs had overall higher macrophage content and higher m0 - like and m1 - like macrophage populations . 
higher overall cd68 protein expression in tnbcs was also conrmed by immunohistochemistry . interestingly , immune - rich er - positive bcs had higher expression of a tgfsignaling metagene and showed coordinated overexpression of tgf - 3 , tgf - r2 , and lrrc32 compared with immune - rich tnbcs . 
the tgfpathway is activated by ligands tgf - 1 , tgf - 2 , and tgf3 that bind to membrane - bound serine / threonine protein receptor kinases composed of subunits tgf - r1 and tgfr2 . 
although the tgfligand isoforms are more than 75% similar in amino acid structure , tgf - r2 has increased afnity for tgf - 1 and tgf - 3 relative to tgf2.37 lrrc32 encodes the garp protein that tethers tgfligands to the cell membrane to prime its activation.38 the simultaneous upregulation of the ligand , receptor , and signaling components suggests a functional role for the tgfpathway in immune - rich er - positive bcs . the immune - attenuating function of tgfsignaling in the tumor microenvironment has been extensively studied in vitro and in vivo . 
in early in tumorigenesis , tgfacts as a tumor suppressor , inducing apoptosis in premalignant cells and inhibiting proliferation.39 after tumor formation , tgfpromotes cancer progression through suppressing the host antitumor immune response.40 among other roles , tgfinhibits cd8 + effector t - cell function , inhibits the th1 helper t - cell phenotype , activates foxp3 - positive regulatory t cells , drives m2 - like macrophage polarization , and excludes immune cells from the tumor compartment.41 - 45 the distinct roles of the different tgfisoforms in cancer remain undened . 
among the 3 isoforms , tgf - 3 is the most potent stimulator of neovascularization in models of wound healing and the most potent inhibitor of granulocyte - macrophage colonystimulating factormediated hematopoiesis in the bone marrow . 
tgf - 1 and tgf - 3 are equally potent stimulators of extracellular matrix collagen deposition in models of pulmonary brosis.46 overall , high tgfsignaling is also associated with lesser response to immune checkpoint inhibitors.41 , 42 on an expression level , we found higher relative fractions of cd8 + t cells in immune - rich er - positive bcs as well as higher tgfsignaling ; these cd8 + t cells in immune - rich er - positive patients may therefore lack robust effector cytotoxic function or be excluded from the tumor compartment by augmented tgfsignaling . tgfcan be released by cancer cells as well as by m2 - like macrophages in a positive feedback loop to attenuate antitumor immunity.47 in several studies , the presence of m2 - like macrophages in bc was associated with poor prognosis , and reprogramming of macrophages toward the m1 - like phenotype has been shown to increase responsiveness to immune checkpoint therapy in experimental models.48 , 49 a recent study found that a macrophage - dependent autochthonous mouse model of luminal btype bc , inhibition of class iia histone deacetylase ( hdac ) by tmp195 induces the recruitment and differentiation of antitumor - type macrophages , reduces tumor burden and metastases , and enhances the durability of tumor reduction when combined with chemotherapy regimens or t - cell checkpoint blockade.50 this observation in an animal model of bc is consistent with our ndings in human tissues . 
our analyses also showed that expression of tgfpathway members correlated negatively with the expression of many immune activation markers including interferon ( ifn - ) , granzymes , and perforin , but correlated positively with m2 - like macrophage markers il4 , il10 , mmp9 , and regulatory t - cell marker foxp3 . 
although m2 - like macrophages in the tumor microenvironment may be the source of tgfsignaling , high levels of apolipoprotein b mrna editing enzyme , catalytic polypeptide - likeassociated mutational signatures that have been previously identied in patients with immunerich er - positive bcs may also contribute to upregulation of the tgfpathway in tumor cells and downstream recruitment of m2 - like macrophages.36 deconvolution of the leukocyte compartment also revealed a higher relative fraction of mast cells in immune - rich erpositive bcs ; this was corroborated by overexpression of the mast cell markers cpa3 and ms4a2 in patients with immune - rich er - positive bcs compared with those who have immune - rich tnbcs . 
how these cells inuence antitumor immunity is unknown , but high mast cell inltration in bc has been associated with er expression and favorable prognosis in earlier studies.51 , 52 in summary , our analysis of gene expression data is consistent with a more attenuated immune microenvironment mediated by increased tgfsignaling and m - 2 macrophage presence in immune - rich er - positive bcs . 
in this subset of er - positive bcs , we observed high relative fractions of cd8 + t cells , mast cells , and m2 - like macrophages with lower expression of granzyme - b , perforin , and ifn -  . 
in addition , practical assays that can distinguish patients with immune - rich and tgf - - high from patients with tgf - - low er - positive bcs are needed before these results can be applied in the clinic . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . vasiliki pelekanou employment : sano david l . 
rimm stock and other ownership interests : pixel gear honoraria : amgen , bristol myers squibb , ventana medical systems consulting or advisory role : perkin elmer , bristol myers squibb , astrazeneca , agendia , ultivue , merck , daiichi sankyo , glaxosmithkline , konica minolta , nanostring technologies , nextcure , cell signaling technology , roche , paige , cepheid , sano research funding : cepheid ( inst ) , perkin elmer ( inst ) , astrazeneca / medimmune ( inst ) , nextcure ( inst ) , eli lilly ( inst ) , nanostring technologies ( inst ) , navigate biopharma ( inst ) , ultivue ( inst ) , konica minolta ( inst ) , amgen ( inst ) patents , royalties , other intellectual property : rarecyte circulating tumor cells ; quantitative immunouorescence ( aqua ) ( inst ) travel , accommodations , expenses : ventana medical systems , nextcure , bristol - myers squibb lajos pusztai consulting or advisory role : h3 biomedicine , merck , novartis , seattle genetics , syndax pharmaceuticals , athenex , astrazeneca , genentech , bristol myers squibb , clovis oncology , immunomedics , eisai , almac diagnostics research funding : merck ( inst ) , genentech ( inst ) , seattle genetics ( inst ) , astrazeneca ( inst ) travel , accommodations , expenses : astrazeneca uncompensated relationships : nanostring technologies open payments link : 110878 / summary no other potential conicts of interest were reported . references bianchini g , qi y , alvarez rh , et al : molecular anatomy of breast cancer stroma and its prognostic value in estrogen receptor - positive and - negative cancers . j clin oncol 28 : 4316 - 4323 , 2010 karn t , pusztai l , holtrich u , et al : homogeneous datasets of triple negative breast cancers enable the identication of novel prognostic and predictive signatures . 
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 use of a targeted exome next - generation sequencing panel offers therapeutic opportunity and clinical benet in a subset of patients with advanced cancers scott kopetz , md , phd1 ; kenna r . 
jack lee , md1 ; jiexin zhang , ms1 ; beate litzenburger , phd1 ; vijaykumar holla , phd1 ; walter kinyua , ms1 ; emily broaddus1 ; molly s . 
broaddus , md , phd1 purpose smaller hotspot - based next - generation sequencing ( ngs ) panels have emerged to support standard of care therapy for patients with cancer . 
survival and the impact of matched therapy use were determined by kaplan - meier estimate , log - rank test , and cox proportional hazards regression . results the larger ngs panel identied at least one alteration in an actionable gene not previously identied in the smaller sequencing panel in 214 ( 41% ) of 521 of enrolled patients . 
with current clinical molecular diagnostics , sequencing is faster , uses less tumor dna , and costs less when genes are multiplexed into small next - generation sequencing ( ngs ) panels . 
historically , the focus was often on the identication of mutations found in hotspotsareas of the genome where known drivers are frequently mutated , many of which can be mapped to therapeutic intervention . 
these panels typically emphasize genes that are recommended by cancer treatment guidelines . an emerging utility of ngs is the screening of other types of cancers for mutations in clinically actionable genes that can be targeted therapeutically . 
such treatment approaches are associated with improved in retrospective analyses screening , 1 prosurvival spective trials , 2 - 4 and meta - analyses , 5 - 7 but this approach is not universally embraced.8 , 9 an important issue in these studies is the low number of patients who benet from this approach . 
 kopetz et al context key objective can additional actionable information be identied by expanding sequencing coverage to the full exome of hundreds of genes beyond hotspot analysis and , secondarily , does that additional information affect patient outcomes ? knowledge generated only a small number of genes have alterations that are specically listed in a us food and drug administrationapproved indication that would match a patient with cancer to a specic actionable agentfor example , braf v600e to vemurafenib . 
limited access to targeted therapy trials is an issue , as some trials enroll only certain tumor types or are only active in a few geographic sites . in patients with advanced cancer that is refractory to standard treatment , any benet gained from the detection of mutations in clinically actionable genes beyond those detected using focused hotspot sequencing panels remains unknown . 
hotspot - focused ngs panels fail to robustly identify copy number alterations or mutations that are found outside commonly altered loci , which would represent an advantage of larger ngs initiative was to panels . 
enrollment criteria included the following : adult patient with pathologic documentation of a single solid tumor malignancy ; completed frontline treatment and any standard treatments that extended life by at least 3 months ; eastern cooperative oncology group performance status of 0 or 1 ; no active brain metastases ; and completed tumor testing using a smaller sequencing panel and either disease progression on a matched therapy that targeted a previously identied actionable nding or no clinically actionable mutations detected . molecular assays and decision support that consisted of hotspot mutation testing was primarily performed on archival formalin - xed , parafn - embedded primary and metastatic cancers acquired during the course of routine clinical care using a 46or 50 - gene ngs panel described previously10 ( actionable genes summarized in the data supplement )  . 
subsequent testing used a larger ngs the entire coding regions of panel 409 cancer - related genes with methodologies previously detailed11 ( actionable genes and details of larger ngs panel provided in the data supplement )  . 
the protocol did not provide for image - guided biopsies of the most recent metastasis for testing ; median time since tissue acquisition to ngs was 467 days ( appendix fig a1 )  . relevant germline ndings were reported to the referring oncologist.12 for comparisons with protocol patients , the cancer genome atlas ( tcga ) datagene mutations and gene amplicationsfor the same 409 genes from 316 ovarian high - grade serous carcinomas , 212 colorectal adenocarcinomas , and 230 lung adenocarcinomas were extracted using cbioportal.org. 
for patients with colorectal cancer , mismatch repair was assessed as part of routine clinical care.13 somatic mutations and amplications that were reported for each patient were reviewed by the precision oncology decision support team.14 , 15 this involved annotation for function and potential clinical trial matching for actionability . 
characteristics for patients enrolled and tested in the prospective protocol characteristic female male performance status missing race asian black white hispanic other unknown tumor type bladder breast colorectal endometrial hawaiian / pacic islander gastric / gastroesophageal junction germ cell tumor head and neck lung neuroendocrine others ovarian prostate renal sarcoma thyroid age , years 20 20 - 30 30 - 40 40 - 50 50 - 60 60 - 70  . 
for the smaller 46and 50 - gene ngs panel , 34 and 38 genes , respectively , were considered actionable , whereas for the larger 409 - gene ngs panel , 96 genes were actionable ( data supplement )  . statistical analysis study sample size was dictated by the capacity of the clinical laboratory improvement amendmentscertied clinical molecular diagnostics laboratory that performed the 409 - gene ngs panel , estimated to be 25 cases per week . with a target of 600 patients , it was determined a priori that the rate of identication of alterations in actionable genes could be estimated with a standard error of no more than 0.02. 
we used fishers exact test to assess whether the gene mutation frequency was signicantly different between protocol patients with colorectal adenocarcinoma , lung adenocarcinoma , or ovarian high - grade serous carcinoma and corresponding tcga data sets . 
the probability of overall survival was determined by kaplan - meier estimate , and we used a log - rank test to assess the statistical signicance of the difference between patient groups . 
to evaluate the effect of clinical variables on overall survival , we performed multivariable survival analysis using a cox proportional hazards regression model that included variables that were signicant ( p , .05 ) in a univariable analysis . results characteristics of the patient population enrolled in the protocol a total of 675 patients were enrolled , with large - panel testing completed in 569 patients . 
five hundred twenty - one patients who received at least 6 months of follow - up or who died within 6 months were included in the analysis ( appendix fig a2 )  . colorectal cancer , sarcoma , head and neck cancer , ovarian cancer , and breast cancer were the most frequently represented cancers in the cohort ( table 1 ) , but the protocol enrolled patients with a broad spectrum of cancer types . sequencing results once material was received by the molecular diagnostics laboratory , a median of 13 days passed before the molecular reports were nalized and entered into the electronic medical record ( appendix fig a3 )  . 
of the 521 patients who were tested with the 409 - gene ngs assay , 214 ( 41% ) had at least one tumor alteration in an actionable gene that was not identied in a prior assay using a smaller ngs panel ( figs 1a and 1b )  . full 409 - gene ngs assay results are summarized for all patients in the data supplement . 
not counting the sequencing results from the smaller panel , the mean number of alterations detected in actionable genes in the 409 - gene panel was 1.0 ( range , 0 to 66 ; fig 1c )  . 
after the application of decision support , 201 ( 41% ) of 495 alterations in actionable genes were considered to affect the function of the gene and were deemed actionable ( mean per patient , 0.4 ; range , 0 to 5 ; fig 1d )  . 
the rate of detection of an alteration in an actionable gene with additional testing was dependent on tumor type , with low rates observed in thyroid and ovarian cancers ( fig 2a )  . 
alterations in a variety of actionable genes from the 409 - gene panel were identied , with the most common mutations in genes nf1 , mdm2 , atm , kdr , notch2 , erbb2 , mtor , and pten ( fig 2b )  . matching tested patients to targeted therapy of the 214 patients who had alterations in actionable genes in the large ngs platform that were not detected in the previous small - panel ngs testing , 40 ( 19% ) were matched gender race male female unknown other hispanic hawaiian / pacific islander white black asian disease site others thyroid sarcoma renal ovarian lung colorectal breast age , years > q3 : 65 - 85 q2 - q3 : 56 - 65 q1 - q2 : 46 - 56 < q1 : 18 - 46 fig 1 . 
on average , only one alteration in an actionable gene per tumor was detected . ( d ) on average , only 0.4 actionable alterationsmutation or amplication in an actionable gene that is known or has inferred biologic functionwere detected per tumor . 
 ( a ) stacked bar chart shows the percent of cases for each broad class of tumor type listed with 0 , 1 , 2 , or 3 or more alterations in actionable genes not detected in the smaller testing panel . data are shown for tumor types in which at least 10 patient tumors were sequenced . 
these patients had mutations in actionable genes that were classied as actionable , potentially actionable , or a variant of unknown signicance but the oncologist chose a therapy that was not a match to the gene alterations treating with matched therapy found . 
reasons for not protocols were similar to those from a previously reported patient population18 and included declining performance status , a desire to seek treatment closer to home , or an oncologist who did not consider the gene mutation clinically actionable or the targeted therapy sufciently active in the given tumor type ( data supplement )  . decision support decision support was critical as alterations were detected in a number of actionable genes that were less familiar to oncologists , and the availability of matching clinical trials varied during the study period . 
given the hypermutated nature of this patients tumor , it was felt that none of the mutations would act as a driver or represented a good target for matched therapy ; thus , they were not annotated ( fig 3a )  . 
not counting the sequencing results from the smaller panel , nearly 70% of tumor alterations were identied in patients with tumors that were found to be in the top quartile of overall tumor mutation burden . 
 kopetz et al ( n = 201 ; 41% ) yes : inferred ( n = 35 ; 17% ) potentially ( n = 81 ; 40% ) yes : literature based ( n = 85 ; 42% ) ( n = 66 ; 13% ) ( n = 11 ; 2% ) unknown ( n = 21 ; 44% ) all gene alterations ( n = 2 , 673 ) bottom quartile 3rd quartile 2nd quartile top quartile alterations in actionable genes ( n = 495 ) actionable alterations ( n = 201 ) bottom quartile 3rd quartile bottom quartile 2nd quartile top quartile 3rd quartile top quartile 2nd quartile fig 3 . 
forty - four percent of the alterations found in actionable genes were variants of unknown signicance ( unknown ) , and 13% were not annotated because they were all from one hypermutated patient ( na )  . 
of the alterations with known function , 2% are known to be benign or not actionable ( no ) , with the remainder having some annotated function on the basis of the existing literature . 
presence of clinically actionable alterations was not related to high overall tumor mutation burden . application of decision support , the number of actionable alterations was poorly correlated with mutation burden , as less than 50% of actionable alterations in actionable genes are in the top quartile of mutation load ( fig 3b )  . 
thus , tumor mutation burden was not a good predictor of the presence of a clinically actionable alteration . patient outcomes neither the number of overall gene alterations in the tumor , nor the presence of alterations in actionable genes signicantly inuenced patient survival ( figs 4a and 4b )  . 
survival was assessed by manual curation of the medical record along with the date when a patient was last known to be alive as documented by a physician note or date of death provided by obituary , tumor registry , or reported by a family member . 
this study is limited by the lack of randomization ; however , comparison of matched and unmatched patients helps to minimize concerns related to comorbidities or declining performance status as an explanation for the differences in outcomes observed in figures 4c and 4d , as all patients in this analysis received another line of therapy , including participation in clinical trials . two patients were found to have deleterious germline mutations that were not previously known to the patient or oncologistpatient management was not altered in either case . 
 ( a - d ) kaplan - meier plots for overall survival by ( a ) total number of alterations ( actionable and nonactionable ) detected , ( b ) whether the patient had a tumor with an alteration in an actionable gene , ( c ) type of therapy and absence of alterations in actionable genes , and ( d ) whether the patient had a tumor with an alteration in an actionable gene on the 409 - genes next - generation sequencing panel received matched treatment . 
only treatment with matched targeted therapy ( c and d ) was associated with signicantly improved survival ( p = .017 compared with patients treated with nonmatched therapy )  . 
tcga did not select for patients with advanced cancers ; therefore , we compared mutation frequencies in our cohort with those of the tcga for colorectal adenocarcinoma , lung adenocarcinoma , and ovarian high - grade serous carcinoma.19 - 21 these three cancers were examined because of their relatively homogeneous histology and sufcient representation in the study . 
for colorectal cancer , kras mutation frequency was higher in our patient population , which was consistent with their resistance to epidermal growth factor receptordirected therapy22 ( data supplement )  . 
protocol patients also had a signicantly higher incidence of tp53 mutations ( 72% v 52% ; p = .004 ; data not shown )  . only 3% of protocol colorectal cancers were microsatellite instabilityhigh compared with 13% in tcga . 
at risk : wild type 507 439 315 197 112 508 440 318 198 113 508 439 319 199 114 time ( months ) time ( months ) time ( months ) mutation mutation mutation no . 
 ( a - j ) kaplan - meier plots for overall survival for nine actionable genes commonly altered in clinical protocol patients ( a - i ) and for the most common cancer types represented in the protocol ( j )  . 
only two clinically actionable genescdkn2a and cdkn2bhad lower frequencies of alteration in protocol patients with lung adenocarcinoma ( data supplement )  . discussion survival for the overall cohort was poor in this institutionwide prospective protocol that enrolled patients with advanced solid tumor malignancies refractory to treatment . for 41% of these patients , we identied an alteration in a clinically actionable gene that was not detected by previous small - panel testing . 
the overall utility of singleas opposed to sequential smallpanel , then large - panel testinglarge - panel ngs testing combined with decision support can be estimated by combining the 11% enrollment in clinical trials from our prior 46and 50 - gene panel study18 with the 8% derived from the incremental addition of the large - panel testing in this study . 
as metastases can accumulate mutations over time , this represents another potential reason for limited patient benet . with increasing gene targets and matched drugs , it is becoming increasingly difcult for an individual physician to reasonably interpret the molecular ndings from larger ngs panels . 
the importance of decision support a comprehensive precision medicine strategy is highlighted by the fact that less than one half of actionable alterations in actionable genes had been reported previously in the literature . 
over time , at least some of these variants of undetermined signicance may be found to be activating mutations after they are examined in functional assays . examples of variants that have been reclassied as activating mutations in a functional genomics platform26 include pdgfra k385m , pik3ca e110del , and ret d627n . 
the reliability of quality decision support is crucial as patients with advanced cancers have a nite lifespan . patients with advanced cancers that are refractory to standard therapy may have mutational frequencies of individual genes that differ from published frequencies derived from unselected patients . 
this was apparent in patients with colorectal cancer and ovarian high - grade serous carcinoma in whom frequencies likely reected a bias toward more clinically aggressive or treatment - resistant tumor biology . frontline treatment of ovarian cancer is for example , platinum - based chemotherapy ; is possible that , by selecting for patients with platinum - resistance , the protocol also selected for patients with ovarian cancers with therapydriven alterations in the molecular landscape . 
the phenomenon is supported by the comparison of survival populations from stage - matched patients in tcga and clinical trials , where patient survival from clinical trials was substantially lower.27 patients with advanced cancers may have higher incidences of mutations associated with other forms of treatment resistance , such as egfr t790m and esr1 mutations.28 the potentially unique molecular features in patients with advanced , chemotherapy - resistant cancers may represent one factor that contributes to the the matched targeted therapy low success rate of approach . treatment directed against actionable genes remains suboptimal . 
pathways that were previously thought to be universally targetable have proven to be difcult to treat , such as the phosphatidylinositol 3 - kinase / akt pathway , 29 or subject to variation in results by tumor type , such as braf30 or her2 / 3 mutations.31 , 32 in protocol patients , we were unable to ascertain any strong individual signals of activity for particular alterations in specic tumor types in part because of insufcient numbers of patients . in conclusion , these results demonstrate the utility of largepanel ngs testing when combined with decision support . the derived benet is realized in only a small subset of patients . 
future efforts should emphasize high - quality and timely decision support and minimize barriers to patient enrollment , with the ultimate goal of broadly delivering precision medicine to patients with solid tumor malignancies . 
broaddus , md , phd , department of pathology , unit 85 , university of texas md anderson cancer center , 1515 holcombe blvd , houston , tx 77030 ; twitter : @mdandersonnews ; e - mail : rbroaddus@ mdanderson.org. support supported , in part , by undesignated donor funds from the md anderson annual funds program provided by the provosts ofce , khalifa bin zayed al nahyan foundation , cancer prevention research institute of texas grant no . 
for more information about asco 's conict of interest policy , please refer to or po.ascopubs.org / site / ifc . scott kopetz stock and other ownership interests : molecularmatch , navire consulting or advisory role : roche , genentech , emd serono , merck , karyopharm therapeutics , amal therapeutics , navire pharma , symphogen , holy stone , biocartis , amgen , novartis research funding : amgen ( inst ) , sano ( inst ) , biocartis ( inst ) , guardant health ( inst ) , array biopharma ( inst ) , genentech ( inst ) , emd serono ( inst ) , medimmune ( inst ) , novartis ( inst ) j . 
jack lee consulting or advisory role : abbvie kopetz et al beate litzenburger employment : qiagen funda meric - bernstam honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pzer , effector therapeutics , abbvie , boehringer ingelheim ( i ) , guardant health ( inst ) no other potential conicts of interest were reported . references tsimberidou am , iskander ng , hong ds , et al : personalized medicine in a phase i clinical trials program : the md anderson cancer center initiative . 
massard c , michiels s , fert e c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . 
cancer discov 7 : 586 - 595 , 2017 radovich m , kiel pj , nance sm , et al : clinical benet of a precision medicine - based approach for guiding treatment of refractory cancers . 
cancer res 76 : 3690 - 3701 , 2016 jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
j natl cancer inst 107 : djv253 , 2015 schwaederle m , zhao m , lee jj , et al : impact of precision medicine in diverse cancers : a meta - analysis of phase ii clinical trials . 
j clin oncol 33 : 3817 - 3825 , 2015 schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
singh rr , patel kp , routbort mj , et al : clinical validation of a next - generation sequencing screen for mutational hotspots in 46 cancer - related genes . 
singh rr , patel kp , routbort mj , et al : clinical massively parallel next - generation sequencing analysis of 409 cancer - related genes for mutations and copy number variations in solid tumours . 
bartley an , luthra r , saraiya ds , et al : identication of cancer patients with lynch syndrome : clinically signicant discordances and problems in tissue - based mismatch repair testing . 
cancer prev res ( phila ) 5 : 320 - 327 , 2012 johnson a , zeng j , bailey am , et al : the right drugs at the right time for the right patient : the md anderson precision oncology decision support platfordrug discov today 20 : 1433 - 1438 , 2015 15 . 
liang h , cheung lw , li j , et al : whole - exome sequencing combined with functional genomics reveals novel candidate driver cancer genes in endometrial cancer . genome res 22 : 2120 - 2129 , 2012 33 : 2753 - 2762 , 2015 18 . 
andr e f , bachelot t , commo f , et al : comparative genomic hybridisation array and dna sequencing to direct treatment of metastatic breast cancer : a multicentre , prospective trial ( safir01 / unicancer )  . 
hyman dm , piha - paul sa , rodon j , et al : neratinib for erbb2 mutant , her2 non - amplied , metastatic breast cancer : preliminary analysis from a multicenter , open - label , multi - histology phase ii basket trial . 
 t clinical benet of larger ngs panels assessed for eligibility ( n = 675 ) excluded ( n = 101 ) died before testing declined to return to the institution for treatment insufficient tissue for testing ngs testing ( n = 574 ) final analysis ( n = 521 ) excluded ( n = 53 ) no death within 6 months follow - up < 6 months cms46 / 50 testing ( n = 507 ) without cms46 / 50 ( n = 14 ) no actionable gene found ( n = 371 ) actionable gene found , then progression ( n = 78 ) actionable gene found , no progression ( n = 58 ) cms400 testing ( n = 507 ) no actionable genes in cms400 that are not identified in cms46 / 50 ( n = 301 ) no actionable gene identified in cms400 ( n = 6 ) cms400 testing ( n = 14 ) 1 actionable gene in cms400 not identified in cms46 / 50 ( n = 206 ) no additional actionable gene identified in cms400 ( n = 307 ) 1 actionable gene identified in cms400 ( n = 8 ) 1 actionable gene in cms400 not in previous panel ( n = 214 ) matched therapy ( n = 40 ) nonmatched therapy ( n = 108 ) no therapy ( n = 66 ) fig a2 . 
summary of the turnaround time ( in days ) for large panel next - generation sequencing testing to be nalized once tissue was received by the clinical molecular diagnostics lab . 
polley , phd1 and ying kuen cheung , phd2 applications in early - phase cancer trials have motivated the development of many statistical designs since the late 1980s , including dose - nding methods , futility screening , treatment selection , and early stopping rules . these methods are often proposed to address the conventional cytotoxic therapeutics for neoplastic diseases and cancer . 
recent advances in precision medicine have motivated novel trial designs , most notably the idea of master protocol ( eg , platform trial , basket trial , umbrella trial , n - of - 1 trial ) , for the evaluation of molecularly targeted cancer therapies . 
in this article , we review the concepts and methodology of early - phase cancer trial designs with a focus on dose nding and treatment screening and put these methods in the context of platform trials of molecularly targeted cancer therapies . 
tumors once thought to be of the same histologic type may now be considered heterogeneous and differentiated on the basis of genomic biomarkers and may be treated differently according to the biomarker expression prole . 
because the subject subgroups dened by specic genetic abnormalities of the tumors may only represent a small fraction of the disease population , the concept of precision oncology trials for targeted therapies has created enormous challenges in recruiting patients with rare genomic subtypes . 
this recruitment challenge , coupled with the need to test multiple targeted therapies in relatively small molecularly dened patient subgroups in an efcient manner , has led to the rethinking of cancer drug development paradigto meet these challenges , the concept of master protocols has been introduced to increase the speed of oncologic therapy development and evaluation . 
the main goal of constructing a master protocol is to enable sharing of operational infrastructure and key design elements across substudies so as to achieve better coordination and efciency than can be achieved in single trials designed and conducted independently in biomarker - dened subpopulations.1 - 5 a platform trial is a randomized trial in a single histology that involves multiple treatments and multiple biomarkers under a master protocol . 
instead , rather than presuming we know which therapy is appropriate for which biomarker stratum , randomization is used for treatment assignment within each biomarker stratutable 1 gives a schema of biomarker - based inclusion criteria in a hypothetical platform trial . 
 polley and cheung context key objective this article provides a critical review of early - phase cancer trial statistical methods and discusses their practicality under the novel platform trial paradigm for evaluating molecularly targeted therapies . knowledge generated although many trial design principles for cytotoxic agents still hold relevance for molecularly targeted therapies , new design and analysis issues , including delayed toxicities and efcacy - tolerability trade - offs , should be considered when designing studies involving these agents . 
early - phase platform trials facilitate efciency gains by allowing within - trial information sharing of safety and efcacy data . relevance this article provides a practical guide for early - phase platform trial designs in the era of precision medicine . 
novel statistical methods continue to be needed to harness the information garnered in these new - generation trial designs to help expedite oncologic drug development and approval . for neoadjuvant therapeutic response with imaging and molecular treatment of analysis 2 ( i - spy2 ) trial women with locally advanced breast cancer.8 , 9 methodologic innovations in a platform trial may include midtrial outcome - adaptive randomization to favor treatments with higher response rates within the respective biomarkerdened stratum.10 , 11 the treatment effects of various experimental therapies are often estimated according to a bayesian hierarchical model by borrowing outcome information across molecularly dened biomarker subgroups.10 , 11 at the same time , bayesian decision rules may be incorporated to determine when and whether therapies with low probabilities of success should be discontinued and therapies with high probabilities of future success should advance to subsequent conrmatory studies ; in this way , novel therapies may be added or dropped in a perpetual manner.10 , 12 , 13 because of the need for midtrial adaptations , platform trials often use short - term end points , such as absence of disease progression at 8 weeks ( as in battle ) or pathologically conrmed complete response ( as in i - spy2 )  . 
although the bayesian inferential structure provides a convenient and efcient framework for analysis , it does not protect the type i error rate against multiple comparisons in the conventional sense . 
as such , phase ii platform trials are generally regarded as exploratory , and positive ndings from these trials will require independent conrmation for the promising drug - biomarker stratum in subsequent phase iii trials . cancer trial designs have been well established for cytotoxic agents . 
specically , phase i trials are dose - nding studies that examine safety of the drug and estimate the maximum - tolerated dose ( mtd ) , 14 and phase ii trials are designed to screen new drugs on the basis of pilot efcacy such as clinical response.15 , 16 the general objective of early - phase cancer trials is to identify and recommend a promising dose regimen of a new agent for conrmatory investigation in multicenter phase iii randomized clinical trials . 
the rationale for using toxicity as a surrogate for efcacy can be traced back to the suggestion of using nitrogen mustards in the treatment of neoplastic diseases in the 1960s.18 the most commonly used statistical design for a phase i oncology dose - nding trial is the 3 + 3 design . 
this is a rulebased design in which the number of dose levels is xed in advance and the dose escalation or de - escalation decision is based on the number of dlts that patients experience at a given dose . 
the 3 + 3 design has received extensive examinations and has been demonstrated to produce poor statistical properties , including treating many patients at doses that are below the biologically active level and imprecise estimation of dlt probability because of the relatively small number ( three to six ) of patients treated at each dose cohort.19 - 21 to address the deciencies of the 3 + 3 design , many dosending designs have been proposed since the 1990s that purport to improve statistical accuracy and trial efciency in the context of chemotherapy trials.22 the most prominent work among these is an adaptive design known as the continual reassessment method ( crm ) .23 , 24 the crm uses a mathematical model to relate the dose levels to the probability of dlt . 
after the rst patient has been treated at the dose determined by the initial dose - toxicity curve , the toxicity information is combined statistically with the initial curve , and an updated dose - toxicity curve is estimated using a bayesian methodology . 
the crm has been shown to improve the precision in estimating the mtd and to increase the number of patients assigned to the selected mtd when compared with the standard 3 + 3 method.25 - 27 the latter property has important ethical implications because traditional methods will likely treat many patients at low and , hence , inefcacious the crm fullls the therapeutic doses . purpose of phase i cancer trials , which are often the last resort of the patients who have exhausted other alternative treatment options . 
during its early inception , the crm drew some criticisms particularly with regard to the possibility of exposing patients to doses that are likely to cause dlt.28 , 29 to address these concerns , several trials used a hybrid approach that combined the model - based crm with a rulebased initial dose - escalation plan ( clinicaltrial.gov identiers : nct03141203 , nct03733990 , and nct03028766 ) .28 - 31 in this regard , once an mtd is identied , a new chemotherapy will be studied in phase ii trials , which are proof - of - concept studies looking for early indication of antitumor activity . 
this objective is often achieved with a single - arm trial design using clinical response as an end point , with the possibility of stopping a trial early as a result of futility.16 , 23 , 32 , 33 for instance , to have 80% statistical power to reject a 25% response rate in favor of a 45% response rate of a new drug at 5% signicance , a single - arm , xed - sample size trial will need to enroll 36 patients and seek to observe 14 responses in the enrolled patients . 
alternatively , a simon two - stage design16 will rst enroll 17 patients and then enroll an additional 24 patients ( ie , a total of 41 patients ) only if there are at least six responses in the rst 17 patients . 
because of the provision for futility stopping , the simon design will , on average , treat fewer patients with inefcacious drugs , thus allocating resources to the more promising ones . 
however , to demonstrate promise of a new drug , an adaptive design with futility stopping will always require a larger maximum sample size than a xed trial ( as in the example just provided )  . 
a participant with a given biomarker is eligible for random assignment to a drug and dose among those marked by a checkmark , which indicates that the drug is a candidate for the biomarker and that the dose does not exceed the maximum - tolerated dose . 
these noncytotoxic agents tend to induce long - lasting mild toxicities , and hence , the assumption of acute toxicities may not apply.35 for some agents , prolonged administration may be required to achieve desirable therapeutic benet , thus increasing the likelihood of late - onset or cumulative toxicities that may manifest many months after the initiation of treatment . 
therefore , for phase i trials of targeted therapies , it is critical to identify the mtd with respect to a longer observation window , so as to ensure future investigations are limited to a tolerated dose range . the 3 + 3 design and crm - type designs dictate that accrual of new patients be suspended until all enrolled patients have been fully evaluated for dlt . 
when delayed toxicities are anticipated , the trial length may be prohibitively long because of the need for frequent accrual suspension and the lengthy dlt observation window.36 , 37 a dose - nding design that does not require suspension of patient accrual while waiting for dlt information on previously treated patients to mature is the time - to - event continual reassessment method ( titecrm ) .38 the dose allocation scheme of the tite - crm follows closely the original crm paradigm but additionally leverages the time - to - toxicity and partial follow - up information in all enrolled patients when estimating the mtd . 
since its introduction , the tite - crm design has been successfully implemented in trials at major academic cancer centers , 39 - 48 as well as us national cancer institutesponsored cooperative groups trials such as radiation therapy oncology group 0813 trial ( clinicaltrials.gov identier : nct00750269 )  . in situations where patients become available to a trial at a rapid rate , the tite - crm could accrue many patients at a given dose level before anyone has been observed for a meaningfully long period . 
therefore , it may be useful to impose a waiting window between cohorts of patients , so as to allow adequate follow - up before adaptation is made.49 - 51 tolerability and efcacy trade - off for molecularly targeted agents and immunotherapies , it may not be adequate to only consider toxicity and tolerability in a dose - nding trial . 
second , a higher dose of a new compound may be less efcacious than a lower dose52 or may see limited benets on the basis of considerations of pharmacokinetic properties.53 hence , the mtd may not be an ideal recommended phase ii dose , although it is still useful to dene the upper safety limit by the mtd . 
third , dlts may not be observed with these agents , and mtd may not be determined at the conclusion of dose escalation.54 , 55 these are the scenarios where both toxicity and activity end points should be used to guide dose recommendations.54 , 55 yan et al56 proposed an adaptive bayesian phase i / ii efftox design that guides dose selection on the basis of the tradeoffs between the probabilities of treatment toxicity and efcacy . 
paoletti and postel - vinay55 discussed the ideal setting for the efftox design and contended that such design is best suited when a homogeneous disease population is well - dened for drug sensitivity and an early biomarker for efcacy is available . 
houede et al57 model clinical utilities on the basis of both toxicity and clinical response in a combination therapy trial , which aims to choose the optimal dose pair of a chemotherapy and a biologic agent . finally , li et al58 proposed an approach to identify the best drug at an efcacious and safe dose for a given biomarker subtype in an early - phase platform trial . 
as cancer trials increasingly focus on combination therapies , it is critical to leverage efcacy information as well as toxicity in dosing decisions . treatment screening in a randomized platform trial in a single - arm , proof - of - concept trial , the interpretation of the results and conclusion of the trial depend on the specication of what would constitute a poor ( null ) response rate on the basis of historical data or a priori clinical experience . 
although response dened by tumor shrinkage is an indicator of activity for cytotoxic drugs , progression - free survival ( pfs ) may be more appropriate for early indication of efcacy of a targeted therapy whose mechanism does not necessarily shrink tumors . 
pfs is a less specic end point than tumor shrinkage because untreated patients may survive without progression for a period of time , whereas patients not treated with chemotherapy are unlikely to experience response . 
furthermore , as precision medicine challenges the fundamental assumption of tumor homogeneity , the appropriate null response rate may vary with biomarker expression . in a platform trial where several drugs are considered for a biomarker subtype ( table 1 ) , drug screening can be based on randomized comparison and ranking , thereby eliminating some subjectivity in choosing a null response rate . 
others have proposed adaptive screening strategies such as a two - stage design , 60 , 61 whereby the rst screening stage aims to select a promising drug among several for additional evaluation , and continuous monitoring using the sequential probability ratio test.62 these innovative adaptive designs have been shown to increase the nal dose selection accuracy while treating more patients with better drugs during the trial and can accommodate situations where there is a concurrent standard therapy . 
indeed , the infrastructure developed under a master protocol , in conjunction with the use of these innovative adaptive designs , facilitates unbiased randomized comparisons of potential drug candidates in a platform trial in a timely and efcient manner . pooling information across subtypes in a platform trial in an early - phase platform trial , where a drug may be given to patients across biomarker subtypes , the safety prole of the drug can be evaluated using pooled information across subgroups . 
specically , it is often reasonable to assume there is a common mtd for all biomarker subtypes when the biomarker is agnostic to adverse reactions to the drug.58 the concept of combining toxicity information from different diseases is not new , because phase i cancer trials of chemotherapy are often conducted in patients with heterogeneous malignancies ( eg , solid tumors )  . 
however , implementing this concept in the context of a platform trial provides much needed relevant safety information of the drug in patients with rare biomarker subtypes . when assessing a drugs efcacy in a given biomarker subtype , a statistically unbiased approach is to consider the observed response or pfs rate using only data of patients with that subtype . 
this analytical approach may make it difcult to understand the drugs effect in rare biomarker subtypes . is that a potential advantage of running a platform trial a targeted therapys efcacy for a given biomarker can potentially be analyzed based on its efcacy in other subtypes of the same histology , when the drug is hypothesized to work through a common molecular mechanism in all subtypes . 
 polley and cheung this analysis adds another level in the hierarchy of bayesian analysis , it is called hierarchical bayesian modeling ( hbm )  . several authors have examined and proposed the use of hbm in platform trials.58 , 63 , 64 it has been noted that borrowing information using hbm can be counterproductive when the drugs effects vary across biomarker subtypes.63 this is conceivable when a drug has nonspecic anticancer activity that is not specic to the molecule . 
although ongoing work has been suggested to model multiple sources of exchangeable drug effects in conjunction with hbm , 64 it is critical to evaluate the clinical situations as to whether there is a strong reason for expecting a common drug effect across subgroups . discussion there are many potential efciency gains associated with a platform trial.2 , 5 first , the use of a common genomic screening platform to identify patients eligible for the trial often results in shorter recruitment time and lower screen failure rate . 
second , the use of centralized governance bodies under a master protocol ( eg , the scientic review committee , institutional review board , or data and safety monitoring committee ) can ensure streamlined and efcient oversight for all substudies . 
for example , the trial innovation network represents a collaborative national network that aims to enhance operational efciency by leveraging the resources and expertise of the clinical and translational science award.65 third , the speed of drug development and evaluation is improved by the common infrastructure that allows opening or closure of substudies of new agents and biomarkers more expeditiously . other related trial designs for biomarker - based cancer drug development under the broad denition of a master protocol include basket trials and umbrella trials.1 , 3 , 4 a basket trial evaluates a targeted therapy on multiple disease subtypes ; specically , each basket evaluates the therapeutic effect of a targeted therapy for several cancer types that have a common molecular biomarker or genetic alteration . 
basket trials are typically nonrandomized ; on the basis of a prespecied genetic alteration , patients are assigned to a regimen that is expected to be active for their tumor . 
these biomarker - dening strata may be single - arm phase ii or phase ii / iii trials that randomly assign patients to either the matched targeted therapy or some standard therapy ( or placebo )  . 
an example of an umbrella trial is the adjuvant lung cancer enrichment marker identication and sequencing trial ( alchemist ) for early - stage nonsmall - cell lung cancer.66 although these novel trials provide a platform to answer clinical questions that traditional clinical trial design may not afford , it is important to appreciate that these gains are accompanied by increased logistical challenges and coordination efforts.67 for example , a platform trial requires tremendous resources and time commitment to establish the common trial infrastructure . 
often , a platform trial would involve multiple agents developed by different industry partners ; the contract negotiation with multiple stakeholders in terms of data sharing or coordination across substudies will likely pose additional communication the assay platform used to screen challenges . 
finally , patients for eligibility and assignment to substudies will also need to be cleared with an investigational device exemption by the us food and drug administration , further adding regulatory complexities . despite these challenges , the opportunities afforded by the new - generation platform trials are enormous . 
from a study design perspective , as we have illustrated , a single platform trial under a master protocol can facilitate information sharing of safety and efcacy data across disease subtypes in the statistical analysis.58 to date , most existing statistical methods have been proposed that deal with safety and efcacy questions independently ( eg , crm for safety dose nding , hbm for efcacy evaluation )  . 
 early - phase platform trials manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors inst = my institution . 
semin oncol 42 : 724 - 730 , 2015 renfro la , sargent dj : statistical controversies in clinical research : basket trials , umbrella trials , and other master protocolsa review and examples . 
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triplenegative breast cancer ( tnbc ) is dened by the lack of expression of estrogen receptor ( er ) , progesterone receptor , and human epidermal growth factor receptor 2 ( her2 ) .1 , 2 this subtype represents 15% to 20% of all breast cancers and is associated with the worst outcome of all subtypes , with greater tendency to distant recurrence in general and visceral metastasis in particular , including brain metastasis.3 , 4 to date , chemotherapy remains the standard of care for tnbc.5 molecular stratication of tnbc will have treatment implications.6 for example , approximately 40% of tnbc patients have expression of programmed death - ligand 1 ( pd - l1 ) protein in immune cells , and this biomarker predicts survival benet from anti - pd - l1 therapy in combination with chemotherapy in the rst - line metastatic setting.7 in addition , approximately 10% of patients with tnbc harbor a germline brca1 / 2 mutation , which confers sensitivity to platinum and / or poly ( adpribose ) polymerase ( parp ) inhibitors.2 , 8 parp is involved in the repair of dna single - strand breaks via the base excision pathway . 
parp inhibitors such as olaparib or talazoparib lead to an accumulation of double - strand dna breaks , resulting in the activation of homologous recombination repair , which can compensate for the lack of activity of the base excision pathway and repair the dna damage.9 however , patients with defects in the homologous recombination dna repair pathway cannot repair dna damages caused by parp inhibitors , and the tumor cell eventually dies ( a term known as synthetic lethality )  . the patient is a 46 - year - old woman diagnosed in december 2015 with stage iib ( ct3cn1 ) moderately differentiated invasive papillary carcinoma with marked tumoral inltrating lymphocytes10 ( 60% ) and the presence of vascular invasion . 
she had a mastectomy and lymphadenectomy in june 2016 . analysis of the surgical specimen revealed extensive invasive residual disease ( ypt2ypn1 ) with a tnbc images of vascular inphenotype and abundant vasion . 
she then underwent adjuvant radiation to the breast and started adjuvant endocrine therapy with tamoxifen ( clinical decision based on baseline er positivity )  . in august 2017 , a positron emission tomography scan revealed multiple pathologic deposits in the bone , lung , and mediastinum and a prepectoral lesion . 
biopsy of the lesion conrmed recurrence of the disease ( gata3 positivity ) and a tnbc phenotype with a ki - 67 of 70% and androgen receptornegative and tumor inltrating lymphocytes around 10% ( fig 1 )  . 
no germline mutation was detected . here , we describe a heavily pretreated patient with tnbc brain metastasis and a brca1 somatic mutation with a remarkable and durable response to parp inhibitor therapy . 
to our knowledge , this is the rst case report to demonstrate disease response to parp inhibition in a tnbc without a germline brca1 or brca2 mutation . the patient was treated with carboplatin and gemcitabine for six cycles , and she achieved a partial response ( fig 2 )  . 
 ( a ) the tumor ( hematoxylin and eosin stain ) was composed of neoplastic inltrative nests with scattered stromal tumor - inltrating lymphocytes with many images of ( b ) lymphovascular invasion ( cd31 )  . 
 ( g ) the tumor had a high proliferation index ( ki - 67 ) , and ( h ) programmed death - ligand 1 ( pd - l1 ) was negative in both the neoplasm and the stromal cells . emergency department with progressively worsening headache . 
a brain magnetic resonance imaging scan showed multiple metastases , the largest being found in the right frontal lobe with surrounding edema ( fig 3a )  . the patient consented to participate in a research project in which tumor proling at the dna and rna level was performed with results discussed at a molecular tumor board . the prepectoral lesion was used for all the molecular analyses . 
the results revealed somatic mutations in brca1 ( s1253fs * 10 9435_9436delgt ) and tp53 ( s37fs * 6 * ) , a low tumor mutational burden ( four mutations per megabase ) , and a stable microsatellite status . 
at the rna level , an ncounter - based breast cancer 360 panel was performed.11 this assay includes 752 breast cancerrelated genes and 23 signatures , the tumor inammation signature , 12 the pam50 subtype predictor , 13 and the tnbctype classications14 , 15 ( fig 4 )  . 
results revealed a pam50 basal - like subtype with the following features : high expression of brca - ness and dna scar signatures , high expression of proliferationrelated genes , low expression of androgen receptorand estrogen - regulated genes , low expression of cd8 t cells and pd - l1 , high expression of immunosuppressive genes or signatures such as transforming growth factorand regulatory t - cell signatures , and a tnbctype mesenchymal subtype . on the basis of these results , off - label use of olaparib 300 mg twice per day was indicated . 
consideration was given to introducing corticosteroids or delivering whole - brain radiotherapy ( wbrt ) , but after discussion with the patient , a clinical decision was made to start olaparib under close observation and without the addition of either radiotherapy or corticosteroids . 
after 2 weeks of treatment , neurologic symptoms improved , and a restaging magnetic resonance imaging scan at week 8 demonstrated a signicant reduction in the size of the brain lesions and disappearance of associated cerebral edema ( fig 3b )  . 
brca proteins play a critical role in the homologous recombination dna repair pathway.16 in the presence of a brca germline mutation , one allele is affected , and the occurrence of a genetic alteration in the other allele ( eg , through methylation or loss of heterozygosity ) leads to a nonfunctional brca and the appearance of breast cancer , among other cancers.9 to date , two phase iii clinical trials have shown that parp inhibition with olaparib17 or talazoparib18 is superior to standard chemotherapy in terms of progression - free survival in her2 - negative advanced breast cancer harboring a brca germline mutation . 
 short title neoadjuvant doxorubicin + cyclophosphamide followed by paclitaxel radiation completed sep 2016 ; adjuvant tamoxifen carboplatin + gemcitabine with clinical response ; treatment stopped for toxicities palliative radiotherapy for bone metastasis ; progression on capecitabine + vinorelbine olaparib initiated dec 2015 jul 2016 aug 2017 feb 2018 may 2018 diagnosed with stage iib ( ct3n1 ) ; er , 50% ; pr , 0% ; her2 - ki - 67 , 80% right mastectomy and alnd ; ypt2n1 ; tnbc ; ki - 67 , 40% metastatic disease , bone , lymph node , subcutaneous tissue ; tnbc reappearance of pain and progression of bone metastases brain metastases fig 2 . 
alnd , axillary lymph node dissection ; er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; pr , progesterone receptor ; tnbc , triple - negative breast cancer ; yp , pathologic staging after neoadjuvant therapy . patients with germline brca1 / 2 - mutated advanced breast cancer . 
brain magnetic resonance imaging before and after olaparib monotherapy . images before olaparib therapy show a cortical enhancing lesion on gadolinum - enhanced t1 - weighted imaging in the inferior frontal gyrus with perilesional edema visualized on uid - attenuated inversion recovery ( flair ) sequencing , as well as diffuse dural enhancement in the right hemisphere . 
selected signature scores are shown with the tumor inammation signature ( tis ) and pam50 signatures at the core ; the other signature scores are shown as bars around the riscores range from 0 to 1 mapped to quantiles of the population with invasive breast carcinoma in the cancer genome atlas ( tcga )  . 
apm , antigen processing machinery ; ar , androgen receptor ; brca - ness , brcaness signature ; cldl - ness , claudin - low subtype signature ; diffrn , differentiation ; dna scar , dna scar signature ; er , estrogen receptor ; her2 - e , her2 - enriched ; inm chmkn , inammatory chemokines ; pd - 1 , programmed cell death protein 1 ; pdl1 , programmed death - ligand 1 ; pgr , progesterone receptor ; tigit , t cell immunoreceptor and ig and itims domains ; treg , regulatory t cell . somatic mutations may also arise in genes involved in homologous recombination . 
early - phase clinical trials of parp inhibitors in metastatic tnbc and germline brca1 / 2 wild - type her2 - negative breast cancer with specic somatic genomic alterations such as brca1 / 2 mutations are underway ( eg , nct02401347 ; phase ii talazoparib in brca1 + brca2 wild - type & triple - neg / her2 - negative breast cancer / solid tumors and nct03330847 ; to assess safety and efcacy of agents targeting dna damage repair with olaparib versus olaparib monotherapy )  . the long - lasting response of breast cancer brain metastasis to olaparib in the absence of any other treatment is worth discussing . 
first , this suggests that olaparib , which had not previously been thought to cross the blood - brain barrier , 28 is able to get to the site of the tumor . 
concordant with this , other case reports with olaparib monotherapy have described regression of brain metastasis.29 , 30 second , olaparib , and other highly effective targeted systemic therapies , allow the delay of wbrt.31 - 35 this is important because wbrt can have a negative impact on quality of life and long - term neurocognitive functioning.36 thus , strategies to avoid , delay , or abrogate the effects of wbrt using systemic targeted therapies should be prioritized . in summary , comprehensive genomic alteration testing may provide novel clinical strategies for personalized therapy in advanced tnbc with improvement in overall survival and quality of life . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . tom as pascual consulting or advisory role : genentech research funding : genentech ( inst ) , msd oncology ( inst ) consulting or advisory role : bristol - myers squibb , diaceutics research funding : novartis travel , accommodations , expenses : pzer , boehringer ingelheim , menarini , msd , takeda pharmaceuticals , thermo fisher scientic maria vidal consulting or advisory role : novartis / pzer speakers bureau : novartis / pzer , genentech , eisai travel , accommodations , expenses : pzer montserrat muoz consulting or advisory role : eli lilly speakers bureau : roche travel , accommodations , expenses : roche , eli lilly aleix prat employment : novartis ( i ) honoraria : pzer , novartis , roche , msd oncology , eli lilly , daiichi sankyo consulting or advisory role : nanostring technologies ( inst ) , amgen , roche , novartis , pzer , bristol - myers squibb research funding : roche ( inst ) , novartis ( inst ) patents , royalties , other intellectual property : pct / ep2016 / 080056 : her2 as a predictor of response to dual her2 blockade in the absence of cytotoxic therapy travel , accommodations , expenses : daiichi sankyo other relationship : oncolytics biotech no other potential conicts of interest were reported . cristina teixid o honoraria : msd , pzer references bauer kr , brown m , cress rd , et al : descriptive analysis of estrogen receptor ( er ) - negative , progesterone receptor ( pr ) - negative , and her2 - negative invasive breast cancer , the so - called triple - negative phenotype : a population - based study from the california cancer registry . 
nature 490 : 61 - 70 , 2012 carey la , perou cm , livasy ca , et al : race , breast cancer subtypes , and survival in the carolina breast cancer study . 
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clin cancer res 13 : 4429 - 4434 , 2007 cardoso f , senkus e , costa a , et al : 4th eso - esmo international consensus guidelines for advanced breast cancer ( abc 4 )  . 
ann oncol 29 : 1634 - 1657 , 2018 prat a , adamo b , cheang mc , et al : molecular characterization of basal - like and non - basal - like triple - negative breast cancer . 
oncologist 18 : 123 - 133 , 2013 schmid p , adams s , rugo hs , et al : atezolizumab and nab - paclitaxel in advanced triple - negative breast cancer . 
n engl j med 379 : 2108 - 2121 , 2018 ahn sg , kim sj , kim c , et al : molecular classication of triple - negative breast cancer . 
j breast cancer 19 : 223 - 230 , 2016 ashworth a : a synthetic lethal therapeutic approach : poly ( adp ) ribose polymerase inhibitors for the treatment of cancers decient in dna double - strand break repair . 
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lehmann bd , jovanovi c b , chen x , et al : renement of triple - negative breast cancer molecular subtypes : implications for neoadjuvant chemotherapy j clin invest 121 : 2750 - 2767 , 2011 selection . 
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 o prospective genomic profiling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making see accompanying editorial doi : purpose a long natural history and a predominant osseous pattern of metastatic spread are impediments to the adoption of precision medicine in patients with prostate cancer . 
to establish the feasibility of clinical genomic profiling in this disease , we performed targeted deep sequencing of tumor and normal dna from patients with locoregional , metastatic noncastrate , and metastatic castration - resistant prostate cancer . patients and methods patients consented to genomic analysis of their tumor and germline dna . a hybridization capture - based clinical assay was used to identify single - nucleotide variations , small insertions and deletions , copy number alterations , and structural rearrangements in more than 300 cancer - related genes in tumors and matched normal blood . results we successfully sequenced 504 tumors from 451 patients with prostate cancer . 
twenty - seven percent of patients harbored a germline or a somatic alteration in a dna damage repair gene that may predict for response to poly ( adp - ribose ) polymerase inhibition . 
in contrast , comparative analysis across disease states revealed that apc alterations were enriched in metastatic tumors , whereas atm alterations were specifically enriched in castration - resistant prostate cancer . conclusion through genomic profiling of prostate tumors that represent the disease clinical spectrum , we identified a high frequency of potentially actionable alterations and possible drivers of disease initiation , metastasis , and castration resistance . 
2017 by american society of clinical oncology wassim abida joshua armenia anuradha gopalan ryan brennan michael walsh david barron daniel danila dana rathkopf michael morris susan slovin brigit mclaughlin kristen curtis david m . 
although molecular profiling is not yet considered a standard - of - care for patients with this disease , new evidence points to enhanced treatment response in specific molecular contexts , paving the way for therapy selection on the basis of tumor molecular characteristics . 
all tumors were reviewed by pathologists who specialize in genitourinary oncology for confirmation of malignant histology of prostatic origin . sequencing and analysis we used the msk - impact assay as previously described10 , 11 ( fig 1a )  . 
the assay was performed in a clinical laboratory improvement amendments certified laboratory and designed to robustly identify single - nucleotide variations , small insertions and deletions ( indels ) , somatic copy number alterations , and structural rearrangements in more than 300 cancerrelated genes in formalin - fixed and paraffinembedded tumors and matched normal blood . somatic variant analysis was performed as described , 10 , 11 with germline variants identified in matched blood samples filtered out in the somatic analysis process . 
somatic findings were reported in the electronic medical record and anonymized and uploaded to cbioportal for visualization and analysis.12 - 14 clonality of mutations was estimated as cancer cell fraction15 and implemented in the facets algorithm.16 beginning in may 2015 , patients were given the option to consent to analysis of germline variants that were identified via sequencing of normal blood samples . 
germline analysis of 76 known cancer - predisposing genes was performed as previously described.16a additional methods are provided in the data supplement . results targeted dna sequencing of tumornormal pairs from patients with prostate cancer using the msk - impact assay , we successfully profiled 504 tumors from 451 patients with prostate cancer who presented to the clinic ( fig 1a and data supplement )  . 
in total , 348 patients ( 77% ) had metastatic prostate cancer , 53 ( 12% ) had biochemical recurrence after definitive therapy , and 50 ( 11% ) had locoregional disease ( fig 1b )  . 
metastatic tumors that were successfully profiled were obtained from lymph node ( 45% ) , bone ( 22% ) , liver ( 14% ) , lung ( 5% ) , and other soft tissue sites ( 14% ; fig 1c )  . 
unlike the tcga and su2c - pcf studies , tumors that were profiled represented all three prostate cancer clinical states : locoregional , metastatic noncastrate , and metastatic castration resistant . we began with 746 biopsy / surgical samples to successfully sequence the 504 tumors reported above , with an overall success rate of 68% ( appendix fig a1 )  . 
 a tumor pathology review matched normal extraction library construction target gene capture somatic analysis ( snvs , indels , cnvs , fusions ) germline analysis ( with specific consent ) tumor report in emr genetics report in emr metastatic tumor site other soft tissue lung liver bone patient disease state ( highest known ; n = 451 patients ) locoregional biochemically recurrent metastatic sample type prostate metastasis disease state at time of tumor tissue collection ( n = 504 tumors ) locoregional locoregional locoregional metastatic noncastrate metastatic castration resistant fig 1 . 
their disease state at the time of tissue collection for the 504 tumors that were profiled is represented at bottotumors that were profiled represented all three prostate cancer clinical disease states : locoregional , metastatic noncastrate , and metastatic castration resistant . 
cnv , copy number variation ; emr , electronic medical record , msk - impact , memorial sloan kettering - integrated mutation profiling of actionable cancer targets ; snv , single - nucleotide variation . states and are shown in fig 2 , grouped in pathways that are potentially clinically actionable . prospectively acquired primary tcga tumors ( appendix fig a3 )  . overall , the frequency of alterations in genes of interest in prostate cancer was similar for mcrpc tumors that were profiled in the msk - impact and su2c - pcf mcrpc data sets4 ( appendix fig a2 ) but demonstrated now in a clinical practice setting . 
however , notable differences were observed when comparing primary localized tumors in the msk - impact data set with those that were profiled in the prospective tcga study , including a higher frequency of alterations in tp53 and foxa1 in msk - impact tumors ( appendix fig a3 )  . 
this is most likely a result of the more aggressive nature of the primary localized tumors in the msk - impact cohort , which were predominantly obtained from patients who subsequently developed biochemically recurrent and metastatic disease ( fig 1b ) relative to the in total , 24% of patients carried somatic alterations in the pi3k / akt pathway , including in pten , pik3ca , pik3cb , pik3r1 , akt1 , and akt3 ( appendix fig a4 )  . 
alterations in commonly affected genes in prostate cancer ( eg , ar , pten , tp53 , foxa1 ) are shown in addition to genes in potentially actionable or biologically relevant pathways . 
mapk , mitogen - activated protein kinase ; msk - impact , memorial sloan ketteringintegrated mutation profiling of actionable cancer targets ; pi3k , phosphatidylinositol - 3kinase . homologous recombination , including brca2 , brca1 , atm , fanca , rad50 , palb2 , and cdk1217 - 21 ( fig 3a and appendix fig a7 )  . a recent multi - institutional study identified a high frequency of ddr gene alterations in the germline of patients with advanced prostate cancer.22 of patients in our data set , 221 underwent formal germline analysis , the first 124 of whom were included in the previously reported study.22 of these 221 patients , 42 ( 19% of total ) had a known or likely pathogenic germline mutation in brca2 ( 9% of total ) , chek2 ( 4% ) , atm ( 2% ) , brca1 ( 1% ) , fh ( 1% ) , and pms2 , nbn , palb2 , and brip1 ( , 1% each ; fig 3b and appendix table a1 )  . 
whereas germline ddr gene alterations may predict for response to parp inhibition or platinum agents , somatic - only alterations in these genes without a germline event may still predict for drug response.9 of the 221 patients who underwent germline analysis , 27% demonstrated alterations in brca2 , brca1 , atm , or chek2 , either in the germline or somatically ( fig 3c )  . 
of note , germline analysis alone accounted for approximately one half of these patients only , which suggests that both germline and somatic analysis should be performed to identify patients with ddr gene deficiency . in total , 3% of patients had tumors with somatic alterations in mismatch repair ( mmr ) genes msh2 , mlh1 , pms2 , or msh6 . 
these tumors accounted for the majority of samples with the highest mutation counts on msk - impact profiling ( fig 3d ) , which were confirmed to be enriched for previously described mmr and microsatellite instability signatures23 , 24 ( appendix fig a8 )  . 
identification of mmr - deficient prostate cancers may have immediate clinical applicability , given recent data that suggest sensitivity of such tumors to immune checkpoint blockade in colorectal cancer and other malignancies.25 - 27 overall , 36% of patients were found to have a potentially actionable alteration by using the oncokb annotation platform27a ( appendix fig a9 )  . this platform does not include non - brca / atm germline alterations , missense alterations of unknown significance , and genes whose clinical significance is less clear , including cdk12 and fanca . 
as genomic alterations undergofurther characterization and new trials and drug targets emerge , the frequency of alterations that are defined as actionable may increase . comparative analysis of somatic alterations across disease states a unique aspect of this data set is that it includes genetic profiles of tumors that represent all three clinical states : locoregional , metastatic noncastrate , and metastatic castration resistant . 
consistent with previous studies , 3 , 4 we identified recurrent areas of copy number loss that involved chromosomes 6q , 8p , 13q , and 16q , and areas of copy number gain that involved chromosomes 1q , 3q , 7 , 8q , and x ( fig 4 )  . 
 displayed the highest burden of copy number alterations , whereas those that represented locoregional disease displayed the lowest ( fig 4 and appendix fig a10 )  . aiming to identify possible genomic drivers of disease progression , we performed a selective enrichment analysis to identify genes that were more frequently altered in mcrpc compared with locoregional disease ( fig 5a )  . 
ar amplification / mutation was the most enriched alteration in mcrpc , as shown in previous studies.3 , 4 other genes that were more commonly altered in mcrpc included tp53 , rb1 , pten , apc , atm , fanca , and cdk12 . we performed a similar analysis that compared alterations in mcrpc with metastatic noncastrate prostate cancer ( fig 5b )  . 
the high enrichment of alterations in ar in mcrpc relative to both locoregional and metastatic non - castrate disease serves as a positive control , consistent with the known role of ar as a driver of castration resistance.28 - 31 beyond frequent amplification of the gene , ar antiandrogen resistance mutations were identified in tumors from patients with mcrpc ( appendix fig a11 ) , including an f877l enzalutamide / arn509 resistance mutation32 , 33 that was found in the tumor of a patient who experienced progression after 4 years of treatment on arn509 . 
four locoregional tumors were found to have mutations in ar , including an h875y mutation that is known to confer resistance to flutamide29 , 34 in a prostatectomy 16 17 18 19 20 21 22 disease state : locoregional metastatic noncastrate metastatic castration resistant sample type : prostate metastasis scna fig 4 . 
represented here are regions of amplification ( red ) or deletion ( blue ) with chromosomes listed horizontally ( top ) in the msk - impact , su2c - pcf ( metastatic castration - resistant prostate cancer [ crpc ] ) , and tcga ( primary localized prostate cancer ) data sets . 
msk - impact tumors are sorted by disease state at time of tissue acquisition , from locoregional ( bottom , gray ) to metastatic crpc ( top , blue )  . 
the level of enrichment is represented as difference in frequency between the two indicated classes ( x - axis ) and its significance ( p value , y - axis )  . 
amp , amplification ; homdel , homozygous deletion ; mut , mutation . sample from a patient who was treatment - nave but who had received dutasteride for benign prostate enlargement . in addition to ar , we again identified enrichment of alterations in tp53 , rb1 , pten , and atm in mcrpc compared with metastatic noncastrate disease . 
enrichment of these genes in mcrpc relative to both earlier disease states implicates them in the development of castration resistance , a finding that is of particular interest for atm , a gene that is involved in ddr . 
fanca and cdk12 , two other dna repair genes , did not show statistically significant mcrpc compared with metastatic noncastrate disease as they did versus locoregional disease , enrichment although there is a trend that suggests a role in castration resistance as well ( fig 5d )  . 
when analysis was limited to metastatic tumors or lymph nodes only , similar trends for enrichment were observed , although statistical significance was not always reached because of smaller sample size ( appendix fig a12 )  . only two genes were enriched in metastatic noncastrate versus locoregional disease : apc and , to a lesser extent , arid5a ( fig 5c )  . 
these findings will require functional validation in the laboratory . matched samples identify clonal alterations in prostate cancer in total , 44 patients had more than one tumor site profiled by msk - impact , including 16 with a matched primary localized tumor and a subsequent metastatic tumor . 
tumors from the same patient that were acquired at a later time point typically had a higher mutation count ( fig 6a )  . given the high frequency of tp53 alterations that were observed in primary localized tumors in this data set and prior reports of aggressive behavior of prostate tumors that harbor tp53 alterations , 36 - 37a we sought to determine whether tp53 alterations were present in tumors early in their evolution or whether they were acquired later at disease progression . 
tp53 mutations were clonal , including in cases in which both a primary localized tumor and a later metastasis were available ( cancer cell fraction > 0.9 in the later metastasis )  . 
likewise , we found that somatic alterations in brca2 were present in matched tumors , which again suggested that somatic brca2 loss of function alterations occur early in tumorigenesis for affected patients . conversely , alterations in ar did not occur early in matched samples ( fig 6b , patients p - 0003597 and p - 0004910 ) , which is consistent with treatment - related changes that promote castration resistance . 
of note , other potentially actionable alterations may arise later in disease evolution , as was the case for patient p - 0002149 ( fig 6b ) , who acquired an activating pik3ca e545k mutation ( appendix fig a4b ) in a recurrent tumor nearly 3 years after his radical prostatectomy . to confirm the above findings , we performed phylogenetic analysis on cases in which several matched tumors were available from the same patient ( fig 6c )  . 
for patient p - 0003511 , ar amplification was truncal castration - resistant tumors , which is consistent with its well - characterized role in castration resistance.28 as the number of patients with prostate cancer who are profiled longitudinally throughout their clinical care increases , such findings may provide insight into clonal driver events that promote disease progression and site - specific metastasis . discussion unlike previous prostate cancer genomic studies , we profiled tumors that represent the clinical spectrum of the disease , from locoregional to metastatic noncastrate and metastatic castrationresistant prostate cancer , which enabled comparisons of genomic landscape across disease states using a single assay . 
whereas locoregional tumors in this data set typically represented more aggressive disease than tcga , patients with such tumors are those in greatest need of new treatment approaches and profiling of their tumors may have particular clinical relevance . an increase in copy number alterations and mutation frequency was evident in mcrpc compared with earlier disease states , as was an increased frequency of alterations in ar , tp53 , rb1 , and pten . 
spop mutations , however , were more frequent in the earlier disease states , which suggested better outcomes for patients with spop - mutant tumors , possibly through increased sensitivity to adt . 
in this analysis , apc and atm emerged as candidate genes of interest that may independently contribute to metastasis and castration resistance , respectively , pending functional validation in the laboratory . 
these genes , like atm , are involved in ddr , alluding to a possible role for dna repair defects in the development of castration resistance . we also found that tp53 alterations are early clonal events in matched tumor samples from individual patients . 
a notable exception ( * ) involves a bladder metastasis and a bone metastasis acquired 5 months later , where the patient had received salvage radiation to the pelvis , possibly explaining the higher mutation count in the earlier bladder tumor . 
 ( b ) somatic alterations in tp53 ( red ) , brca2 ( blue ) , ar ( gold ) , and pik3ca ( green ) in matched tumors in the data set , including localized primaries and later metastases ( green box ) and other matched tumors from the same patients . 
crpc , castration - resistant prostate cancer . available , it will be possible to validate this finding , guiding more aggressive treatment approaches early on for these patients . overall , we identified potentially actionable alterations , including hotspot activating alterations in genes that are known drug targets , consistent with findings of the su2c mcrpc study , but this time in a prospective clinical practice setting . 
these findings have immediate therapeutic relevance , given the recently reported sensitivity of these tumors to parp inhibition9 or immune checkpoint blockade.25 the higher frequency of dna repair alterations that were identified via integrative germline and somatic analyses strongly argues for performing both germline and somatic genomic analyses in all patients with advanced prostate cancer who will require systemic treatment , irrespective of screening on the basis of family history . in summary , this study shows that a large genomic data set that represents the clinical spectrum of prostate cancer can provide mechanistic insight into possible genomic drivers of disease initiation , metastasis , and drug resistance . 
our ability to profile metastatic tumors allowed us to detect the evolution of potential driver alterations in matched tumors from individual patients , identifying alterations in tp53 and brca2 as early events that may confer a more aggressive phenotype . 
scher provision of study materials or patients : wassim abida , joshua armenia , daniel danila , michael morris , susan slovin , marc ladanyi , liying zhang , victor e . 
scher collection and assembly of data : wassim abida , joshua armenia , ryan brennan , michael walsh , david barron , daniel danila , michael morris , susan slovin , brigit mclaughlin , kristen curtis , david m . 
scher data analysis and interpretation : wassim abida , joshua armenia , anuradha gopalan , michael walsh , daniel danila , dana rathkopf , michael morris , susan slovin , jeremy c . 
robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , abbvie ( inst ) , myriad genetics ( inst ) , biomarin ( inst ) , medivation ( inst ) , tesaro ( inst ) travel , accommodations , expenses : astrazeneca vijai joseph stock and other ownership interests : juno therapeutics daniel danila honoraria : astellas scientific , medical affairs , angle , bayer , xian - janssen pharmaceutical consulting or advisory role : angle , bayer research funding : prostate cancer foundation , genentech , janssen research & development ( inst ) patents , royalties , other intellectual property : gene expression profile associated with prostate cancer travel , accommodations , expenses : cambridge healthtech institute , prostate cancer foundation , angle , bayer , american austrian open medical institute , global technology community , xian - janssen pharmaceutical , oncology education dana rathkopf consulting or advisory role : janssen oncology research funding : janssen oncology ( inst ) , medivation ( inst ) , celgene ( inst ) , takeda ( inst ) , millennium pharmaceuticals ( inst ) , ferring ( inst ) , novartis ( inst ) , taiho pharmaceutical ( inst ) , astrazeneca ( inst ) , genentech ( inst ) , tracon pharma ( inst ) michael morris consulting or advisory role : astellas pharma , bayer , endocyte research funding : bayer ( inst ) , sanofi ( inst ) , endocyte ( inst ) , progenics ( inst ) travel , accommodations , expenses : bayer , endocyte susan slovin consulting or advisory role : bayer brigit mclaughlin no relationship to disclose kristen curtis no relationship to disclose david m . 
durack stock and other ownership interests : adient medical consulting or advisory role : adient medical patents , royalties , other intellectual property : patent disclosures , provisionals submitted for instrument to analyze biopsy specimens ( unrelated to the small renal masses topic )  . patent holder for device related to x - ray imaging data collection ( unrelated to small renal masses topic ) , july 2008 . other relationship : society of interventional radiology foundation stephen b . 
solomon leadership : devicor medical products stock and other ownership interests : johnson & johnson , progenics , aspire bariatrics consulting or advisory role : ge healthcare , angiodynamics , medtronic research funding : ge healthcare ( inst ) , angiodynamics ( inst ) patents , royalties , other intellectual property : ge healthcare - patents pending ( inst ) , aspire bariatrics ahmet zehir no relationship to disclose aijazuddin syed no relationship to disclose jianjiong gao no relationship to disclose debyani chakravarty no relationship to disclose hebert alberto vargas no relationship to disclose kenneth offit no relationship to disclose mark t.a. 
kantoff stock and other ownership interests : bellicum pharmaceuticals , metamark genetics , placon , druggablity technologies , tarveda consulting or advisory role : bavarian nordic , janssen , millennium pharmaceuticals , morphosys , pfizer , astellas pharma , bellicum pharmaceuticals , bind biosciences , endocyte , metamark genetics , medivation , merck , mtg therapeutics , oncocellmdx , oncogenex , sotio , sanofi , tokai pharmaceuticals , bayer , genentech , cristal therapeutics , ipsen , omnitura , gtx , tarveda , druggablity technologies , progenity research funding : medivation ( inst ) , sanofi ( inst ) , oncogenex ( inst ) , aragon pharmaceuticals ( inst ) , amgen ( inst ) , astellas pharma ( inst ) , bayer ( inst ) , bavarian nordic ( inst ) , dendreon ( inst ) , exelixis ( inst ) , janssen ( inst ) patents , royalties , other intellectual property : method for predicting the risk of prostate cancer morbidity and mortality , predicting and treating prostate cancer , methods for predicting likelihood of responding to treatment , chromosome copy number gain as a biomarker of urothelial carcinoma lethality , drug combinations to treat cancer , somatic ercc2 mutations correlate with cisplatin sensitivity in muscle - invasive urothelial carcinoma ( patent ) , up - to - date royalties , wolters - kluwer royalties expert testimony : sanofi , janssen travel , accommodations , expenses : sanofi , janssen , bind biosciences , bavarian nordic , millennium pharmaceuticals david b . 
sawyers leadership : novartis stock and other ownership interests : novartis , agios , blueprint medicines , beigene , oric pharmaceuticals consulting or advisory role : novartis , blueprint medicines , agios , beigene , oric pharmaceuticals patents , royalties , other intellectual property : xtandi nikolaus schultz no relationship to disclose howard i . 
grasso cs , wu ym , robinson dr , et al : the mutational landscape of lethal castration - resistant prostate cancer . 11 - 22 , 2010 nature 487 : 239 - 243 , 2012 7 . 
hyman dm , solit db , arcila me , et al : precision medicine at memorial sloan kettering cancer center : clinical next - generation sequencing enabling next - generation targeted therapy trials . 
cheng dt , mitchell t , zehir a , et al : msk - impact : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
joshi pm , sutor sl , huntoon cj , et al : ovarian cancer - associated mutations disable catalytic activity of cdk12 , a kinase that promotes homologous recombination repair and resistance to cisplatin and poly ( adp - ribose ) polymerase inhibitors . 
bajrami i , frankum jr , konde a , et al : genome - wide profiling of genetic synthetic lethality identifies cdk12 as a novel determinant of parp1 / 2 inhibitor sensitivity . 
mccabe n , turner nc , lord cj , et al : deficiency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
mskimpact versus su2cpcf dataset comparison . frequencies of alterations in select genes in metastatic crpc tumors from the msk - impact dataset ( orange ) versus the su2cpcf dataset ( red )  . 
mmr / msi mutation signatures in hypermutated tumors . k - means clustering of mutations / mb ( mut / mb ) across all 504 tumors identified two distinct clusters : cluster1 with mutations / mb10 . 
actionable alterations are ranked by level of evidence ( level 2b : standard of care biomarker predictive of response to an fda - approved drug in another indication , but not standard of care for this indication ; level 3a : compelling clinical evidence supports the biomarker as being predictive of response to a drug in this indication , but neither biomarker nor drug are standard of care ; level 3b : compelling clinical evidence supports the biomarker as being predictive of response to a drug in another indication , but neither biomarker nor drug are standard of care ; level 4 : compelling biological evidence supports the biomarker as being predictive of response to a drug , but neither biomarker nor drug are standard of care )  . 
variants were considered pathogenic or likely pathogenic per american college of medical genetics and genomics guidelines . somatic second hit is reported in column two for patients with germline dna damage repair gene mutations . 
of interest , several of the patients who harbored a germline brca2 c.5946delt ashkenazi founder mutation did not have a detectable somatic second hit in this gene , suggesting a nonclassical pathogenic mechanism for this mutation . 
in this article , we cover topics related to the analysis of prognostic factors , centering on factors that are both relevant at the time of diagnosis or initial treatment and during treatment . 
we then review the state - of - the art methods for dynamic prediction and compare the strengths and limitations of these methods . although static models will continue to play an important role in oncology , developing and validating dynamic models of clinical outcomes need to take a higher priority . 
2019 by american society of clinical oncology introduction the identication of prognostic factors and building of risk assessment prognostic models will continue to play a major role in 21st century medicine in patient management and decision making.1 prognostic factors in oncology associate host and tumor variables treatment.2 with clinical outcomes independent of gospodarowicz et al3 classied factors as either tumor related , host , or environmental . 
tumor - related factors are variables related to the tumor and reveal the tumor biology and pathology , such as size of tumor , lymph node involvement , presence of metastasis , and molecular markers ( overexpression of pten gene , presence of androgen receptor variant ar - v7 )  . 
finally , environmental factors are external to the patient , such as access to health care.3 prognostic models are increasingly used in the design , conduct , and analysis of clinical trials . for example , trials of prostate cancer , randomization was stratied by the predicted survival probability determined by the prognostic model of overall survival.4 - 7 in the tailorx trial , oncotype dx , a 21 - gene score that predicts the likelihood of in several recurrence , is used to classify women with breast cancer by their risk group of recurrence.8 prognostic factors also have been used for enriching the patient population in trials with targeted therapies . 
for example , in the toga trial , patients with human epireceptor 2positive gastric dermal growth factor cancer were randomly assigned to either trastuzumab plus chemotherapy or chemotherapy alone.9 in this article , we cover topics that are related to the analysis of prognostic factors , centering on factors that are relevant both at the time of diagnosis or initial treatment and during treatment or follow - up . 
we make a distinction between static and dynamic predictive models and provide a review of the state - of - the - art methods for dynamic predictive models to promote them for future use . knowledge generated to date , most risk assessment models in oncology have been based on static prognostic models . 
in patients with advanced cancer , the disease has substantially evolved race , age , performance status , body mass index , host factors tumor factors psa , ldh , alkaline phosphatase , p53 , etc clinical outcomes overall survival progression - free survival objective response rate prediction window all available information up to t timeline study baseline landmark time horizon time fig 1 . 
 developing and validating risk assessment models and has a heterogeneous presentation within the patient.10 the interand intrapatient variability should be taken into account in statistical modeling.11 , 12 dynamic prediction incorporates time - dependent covariates so that risk prediction would be continually updated with new observations to reect the patients prognosis . we dene terminology that is typically used in dynamic risk prediction . 
standard variable selection approaches , such as forward selection , backward selection , and so forth , with logistic regression for binary end points , 13 and proportional hazards regression for timeto - event end points , 14 have been applied . 
criticism for the stepwise variable selection has been well documented.15 , 16 of note , classication trees , such as recursive partitioning for both binary and time - to - event end points , 17 - 20 frequently have been used.2 , 21 - 26 we concentrate on penalized methods that t and shrink p predictors and in doing so , reduce the variance of the coefcient estimates.27 thus , these methods would improve the accuracy of the model.28 the least absolute shrinkage and selection operator ( lasso ) and adaptive lasso ( alasso ) have been widely used to develop prognostic models of clinical outcomes.29 , 30 we will briey describe ridge regression and penalized methods . 
ridge regression minimizes the residual sum of squares function , but a caveat is that it does not reduce all the coefcients exactly to 0.28 let yi be the response , xij the jth covariate value ( j = 1 , 2 , , p ) corresponding to the ith individual , j the regression coefcient jth covariate , and a tuning parameter . 
similar to ridge regression , the rst term in lasso is the residual sum of squares , and lasso minimizes this function subject to the l1 penalty ( eq 1 ) : ( cid : 1 ) i ( cid : 1 ) 1 yi ( cid : 1 ) j ( cid : 1 ) 1 j xij ( cid : 2 ) + ( cid : 1 ) ( cid : 2 ) j ( cid : 2 ) ( cid : 2 )  . j ( cid : 1 ) 1 a large tuning parameter causes the coefcient estimates to be equal to 0 , thus the lasso will have the sparsity property.28 lasso is an improvement over ridge regression , although it has the main limitation of tending to select too many unimportant variables , and it performs poorly in situations when p  . 
the alasso enjoys the oracle property.30 , 34 elastic net regression uses a combination of l1 penalty and ridge l2 penalty and is a compromise between lasso and ridge regression . 
n is that it retains more than n variables in the model.35 hastie et al28 provided a thorough comparison of these shrinkage techniques . we applied lasso and alasso from calgb 90401 , a phase iii clinical trial in advanced prostate cancer , with the overall goal of building a model of overall survival.5 we had 22 variables that were common between calgb 90401 and the enthuse trial ( external data set ) .36 because of missing data in the covariates , we used methods to impute them as described by white and royston.37 the regressions estimates from the cox proportional hazards model , lasso , and alasso , are listed in table 1 . 
we considered lasso and alasso and applied both the akaike information criterion and the bayesian information criterion to choose the optimal model of overall survival . lasso and alasso selected eight and nine variables , respectively ( table 1 )  . 
figure 2 shows the solution lactate depath for alasso , and we observe that hydrogenase ( ldh ) greater than the upper limit of normal and eastern cooperative oncology group ( ecog ) performance status were selected early in the l1 path compared with the other variables . 
this is followed by visceral disease , alkaline phosphatase , albumin , hemoglobin , pain , bone metastases , and then psa ( the bayesian information criterion stopped at psa )  . 
the nal model selected the following prognostic factors : ldh greater than the upper limit of normal , ecog performance status , metastatic site ( presence of visceral disease , presence of bone metastases ) , psa , alkaline phosphatase , albumin , hemoglobin , and analgesic opioid use . we have focused on variable selection when the number of predictors is small relative to the sample size . 
in recent years , a few statistical studies extended the penalized method for the joint modeling of longitudinal data and survival outcomes.42 , 43 the general idea is to postulate the joint likelihood linking the two submodels through latent random variables and to add shrinkage operators to select xed and random effects . 
while these methods have not been implemented in oncology , the 4 2019 by american society of clinical oncology heterogeneity of treatment effect ( hte ) is another important area to consider when building prognostic models . hte is the nonrandom , explainable variability in the direction and magnitude of treatment effects for individuals within a population.44 there are different sources for hte , and hte may arise from an underlying causal mechanism , artifacts , measurements , or methods.45 , 46 one main goal of hte analyses is to predict whether a patient might benet from a treatment . 
when we turned to our prognostic model of overall survival in prostate cancer , we computed a risk score from the estimated regression coefcients and the predicted survival at 24 months using the baseline cumulative hazard . 
we observe that patient 2 had a worse predicted survival probability at 24 months than patient 1 . another important task in static predictive modeling is to construct prognostic risk groups , which can be formed on the basis of their quantiles from the estimated linear predictor . 
t , we can update the risk prediction by calculating i * ( ut ( cid : 5 ) )  . there are two general dynamic risk prediction frameworks : joint modeling and landmark analysis . 
joint modeling comprises two linked submodels , one for the longitudinal process and one for the time - to - event data , and both depend on a common set of latent random variables.54 , 55 in particular , the longitudinal data usually are modeled by a linear mixed - effects model . 
the cox regression coefcient quanties the association between the latent longitudinal process and the hazard rate at time t . the longitudinal process and the event time process are assumed to be independent given the latent random effects , and the joint likelihood can be derived . 
the model can be estimated either using a frequentist approach that attains maximum likelihood through an expectationmaximization algorithm54 , 56 - 58 or a bayesian approach that uses markov chain monte carlo to obtain posterior means.59 - 61 while assuming that the parameters are readily estimated from the observed data , the conditional probability i * ( ut ) can be computed . 
a monte carlo estimate of i * ( ut ) can be obtained by sampling the random effects and the parameters from the corresponding distributions.62 on the other hand , landmarking63 - 66 consists of a series of related cox regression models , where each one is dened at a distinct landmark time t.63 - 66 for each pair of { u , t } , a separate model is tted to the individuals who remain in the study and have not yet experienced the event of interest . 
joint modeling models the dual distribution of the longitudinal process and the failure times and hence satises the consistency conditions for dynamic prediction.68 moreover , it exploits the full information of collected data and takes into account the measurement error of the longitudinal data . 
joint modeling also takes a considerable amount of effort to estimate the parameters , and the computational cost is high because it involves complicated joint distribution and numerical integration . landmarking circumvents the aforementioned model assumptions and computational burden , but it is not a comprehensive probability model of in contrast , the longitudinal process and failure times and , as such , does not satisfy the consistency conditions . 
another major shortcoming is that landmarking only considers the patients at risk at the landmark time and does not fully explore the information . several articles have focused on the comparison of joint modeling and landmarking . 
ferrer et al71 compared the two approaches in the case of model misspecication , and they aimed for predicting competing risks of prostate cancer from psa history . dynamic risk prediction ( joint modeling ) relies on model assumptions , and hence , its performance suffers from model misspecication . 
we have previously explored whether psa decline at different landmark times is prognostic for overall survival in patients with advanced prostate cancer.79 fontein et al80 developed a dynamic model for predicting overall survival in patients with breast cancer . 
other applications of dynamic models have been implemented to prostate cancer82 - 85 and colorectal cancer.86 we demonstrated the application of dynamic risk prediction using the datatop study , 87 a clinical trial that examined the benets of deprenyl and - tocopherol in slowing the progression of parkinson disease ( pd ) .88 multiple longitudinal biomarkers were collected in the datatop study , including unied pd rating scale total score , modied hoehn and yahr scale , and schwab and england activities of daily living . 
 developing and validating risk assessment models trajectories ( fig 3a ) and risk of functional disability ( fig 3b )  . patient 169 , who had more severe disease with earlier development of functional disability , and patient 718 , who had less severe disease , were selected to illustrate the patient - specic predictions at clinically relevant future time points conditional on their available longitudinal measurements . 
 ( a ) predicted unied parkinson disease rating scale ( updrs ) trajectories and ( b ) predicted conditional failure probabilities for patient 169 ( top rows ) and patient 718 ( bottom rows )  . 
 halabi , li , and luo joint modeling , our major interest was to predict probability of functional disability after visits at time t given the patients longitudinal proles and event - free status up to time t . 
overtting occurs when a high predictive accuracy is estimated from a model that has been applied to the training set but has low accuracy when assessed in an independent data set.90 a good example of overtting is provided in halabi and owzar.2 the validation of a prognostic model is considered a critical step after a risk assessment model has been built . 
there are two types of validation : external and internal.16 , 89 , 90 external validation , where the frozen model from the training data is applied to an independent data set , is the most rigorous approach . 
of note , other types of resampling methods , such as cross - validation , bootstrapping , and bootstrapping using 0.632 + , are considered appropriate approaches to model validation.32 , 53 , 91 , 92 investigators plot assessment of the models performance usually is conducted by examining the calibration and discriminative ability of the model . 
using data from two phase iii clinical trials , we evaluated the overall survival model for calibration at different landmarks.36 , 93 figure 4a shows that the predicted survival probabilities at 18 months in the enthuse 33 trial were close to the proportion of patients who survived 18 months . 
the rst two points ( circles ) show that the model overpredicted the proportion of patients who survived 12 months , whereas the third and fth data points show that the model underpredicted the proportion of patients who survived 12 months . discrimination describes the ability of a prognostic model to distinguish between patients with and without the outcome of interest.16 several metrics are used to report the performance of a model . 
these models are anticipated to be implemented in both the design and the conduct of future trials . although static models will continue to play an important role in oncology , developing and validating dynamic models of clinical outcomes need to take a higher priority . 
one of the limitations is that modelers may be constrained by the lack of access to the longitudinal biomarker data ; therefore , the next generation of risk assessments are highly recommended to take into consideration the longitudinal biomarker data and outcomes so that predictions are updated . in summary , risk assessment will remain an important research task in precision oncology . 
calibration of the overall survival model for observed and predicted survival probability at ( a ) 18 months and ( b ) 12 months . pertinent to patient outcomes , dene the primary end point a priori , justify the sample size , and describe the appropriate methods for variable selection and model assessment . 
lastly , they should be validated using external data sets if available . an understanding of the longitudinal relationship between host and tumor - related factors and their impact on clinical outcomes is critical . 
we expect to see an upsurge in dynamic risk assessments in oncology , and as such , the american joint committee on cancer and the transparent reporting of a multivariable prediction model for individual prognosis or diagnosis guidelines should be extended to dynamic predictive modeling . 
regardless of whether static or dynamic modeling is the primary objective , we envision that this review will bridge gaps in knowledge and motivate investigators to take risk assessment as a discipline by itself . 
 halabi , li , and luo references osullivan b , brierley j , gospodarowicz m : prognosis and classication of cancer , in osullivan b , brierley jd , dcruz ak , et al : uicc manual of clinical oncology ( ed 9 )  . 
halabi s , lin cy , kelly wk , et al : updated prognostic model for predicting overall survival in rst - line chemotherapy for patients with metastatic castrationresistant prostate cancer . 
j clin oncol 32 : 671 - 677 , 2014 kelly wk , halabi s , carducci m , et al : randomized , double - blind , placebo - controlled phase iii trial comparing docetaxel and prednisone with or without bevacizumab in men with metastatic castration - resistant prostate cancer : calgb 90401 . 
morris mj , heller g , bryce ah , et al : alliance a031201 : a phase iii trial of enzalutamide ( enz ) versus enzalutamide , abiraterone , and prednisone ( enz / aap ) for metastatic castration resistant prostate cancer ( mcrpc )  . 
j clin oncol 37 , 2019 ( suppl ; abstr 5008 ) sparano ja , gray rj , makower df , et al : adjuvant chemotherapy guided by a 21 - gene expression assay in breast cancer . 
n engl j med 379 : 111 - 121 , 2018 bang yj , van cutsem e , feyereislova a , et al : trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of her2 - positive advanced gastric or gastro - oesophageal junction cancer ( toga ) : a phase 3 , open - label , randomised controlled trial . 
miller kd , oneill a , gradishar w , et al : double - blind phase iii trial of adjuvant chemotherapy with and without bevacizumab in patients with lymph nodepositive and high - risk lymph node - negative breast cancer ( e5103 )  . 
rudloff u , jacks lm , goldberg ji , et al : nomogram for predicting the risk of local recurrence after breast - conserving surgery for ductal carcinoma in situ . 
fizazi k , higano cs , nelson jb , et al : phase iii , randomized , placebo - controlled study of docetaxel in combination with zibotentan in patients with metastatic castration - resistant prostate cancer . 
halabi sp , pi l : statistical considerations for developing and validating prognostic models of clinical outcomes , in kelly do , kevin w , halabi s ( eds ) : oncology clinical trials : successful design , conduct , and analysis ( ed 2 )  . 
gabler nb , duan n , liao d , et al : dealing with heterogeneity of treatment effects : is the literature up to the challenge ? trials 10 : 43 , 2009 46 . 
dane a , spencer a , rosenkranz g , et al : subgroup analysis and interpretation for phase 3 conrmatory trials : white paper of the efspi / psi working group on 51 . 
kattan mw , hess kr , amin mb , et al : american joint committee on cancer acceptance criteria for inclusion of risk models for individualized prognosis in the practice of precision medicine . 
rizopoulos d , hateld la , carlin bp , et al : combining dynamic predictions from joint models for longitudinal and time - to - event data using bayesian model averaging . 
yao f , m uller hg , clifford aj , et al : shrinkage estimation for functional principal component scores with application to the population kinetics of plasma folate . biometrics 59 : 676 - 685 , 2003 74 . 
yan f , lin x , li r , et al : functional principal components analysis on moving time windows of longitudinal data : dynamic prediction of times to event . 
halabi s , conaway mr , small ej , et al : serum prostate specic antigen as a predictor of survival in prostate cancer patients treated with second - line hormonal 80 . 
proust - lima c , taylor jm : development and validation of a dynamic prognostic tool for prostate cancer recurrence using repeated measures of posttreatment psa : a joint modeling approach . 
s `ene m , taylor jm , dignam jj , et al : individualized dynamic prediction of prostate cancer recurrence with and without the initiation of a second treatment : development and validation . 
kr ol a , ferrer l , pignon jp , et al : joint model for left - censored longitudinal data , recurrent events and terminal event : predictive abilities of tumor burden for cancer evolution with application to the ffcd 2000 - 05 trial . 
moons kg , altman dg , reitsma jb , et al : transparent reporting of a multivariable prediction model for individual prognosis or diagnosis ( tripod ) : explanation checklist . 
petrylak dp , vogelzang nj , budnik n , et al : docetaxel and prednisone with or without lenalidomide in chemotherapy - naive patients with metastatic castrationresistant prostate cancer ( mainsail ) : a randomised , double - blind , placebo - controlled phase 3 trial . 
halabi s , pi l , lin c - y : developing and validating prognostic models of clinical outcomes , in halabi s , michiels s ( eds ) : textbook of clinical oncology : a statistical perspective . 
giannetta , md1 ; gianluca tomasello , md1 ; stefano stabile , phd1 ; valentina motta , phd1 ; spyridon alexiadis , md1 ; francesco scaglione , md , phd1 , 2 ; angelo vanzulli , md1 , 2 ; massimo torre , md1 ; emanuela bonoldi , md1 ; silvio m . 
veronese , phd1 ; salvatore siena , md1 , 2 ; and andrea sartore - bianchi , md1 , 2 introduction epidermal growth factor receptor ( egfr ) gene mutations are strong oncogenic drivers in a subset of nonsmall - cell lung cancer ( nsclc )  . 
their inhibition with specic tyrosine kinase inhibitors ( tkis ) represents a successful example of precision medicine.1 nevertheless , disease progression almost invariably occurs after 9 - 14 months of treatment with either getinib , erlotinib , or afatinib ( rstand second - generation tkis ) 2 - 4 and after 19 months with osimertinib ( a thirdgeneration tki ) 5 because of the development of acquired therapeutic resistance . several mechanisms of tki resistance have been reported , with different mechanisms for rst - , second - , 6 and third - generation tkis.7 the acquisition of t790m mutation in exon 20 of egfr represents the most frequent mechanism ( more than 50% of patients ) of disease progression with getinib , erlotinib , or afatinib , which can be overcome by osimertinib and other thirdgeneration inhibitors . 
however , a frequent cause of third - generation tki resistance is the development of mutations at the egfr c797 codon , because they prevent binding to the egfr active site.8 , 9 in these patients , preclinical studies have shown that c797s mutation can be found in the same ( in cis ) or different ( in trans ) t790m - mutated alleles , or in other patients the t790m mutation can be lost.10 in clinical practice , resistant mechanisms to different tkis can be detected on disease progression through tissue rebiopsy . 
the isolation and analysis of circulating tumor dna ( ctdna ) through liquid biopsy is also recommended and widely used for identication of acquired resistance mutations of egfr.11 however , not only target - dependent resistance mechanisms can occur . 
after 9 months , the patient experienced disease progression in the liver ( data supplement ) , and a liquid biopsy revealed the acquisition of egfr t790m mutation ( fig 1b ; table 1 )  . 
almost 12 months later , dyspnea worsened , with evidence of increased right pleural effusion and disease progression in the lung , lymph nodes , and liver ( data supplement )  . a new liquid biopsy identied persistence of t790m plus the acquisition of c797s in trans conformation ( table 1 ; fig 1 - c )  . 
synopsis of therapeutic history and histologic and molecular analysis of the present patient showing tumor evolution toward small - cell lung cancer ( sclc ) transformation and accumulation of epidermal growth factor receptor ( egfr ) genetic abnormalities . 
in the case of sclc transformation , a favorable response to etoposide and platinum can be expected25 ; therefore , a rebiopsy should be performed when a histologic transformation is suspected ( eg , aggressive progression )  . in this case report , which describes a representative patient , different subclones harboring distinct resistance mechanisms coexisted . 
the initial ratio of t790m / activating mutation was below the threshold of 0.05 and , according to the ndings of chabon et al , 24 the response to osimertinib was limited to a stable disease by recist criteria . 
this ratio deeply decreased ( table 1 ) at progression after 12 months of therapy with osimertinib when c797s appeared concomitantly with a small - cell transformation , after a total of 20 months of treatment with tkis . 
at this time point , we observed a reduction of t790m / del19 ratio in ctdna , which was similar to the c797s / del19 ratio ( table 1 )  . 
 pizzutilo et al in conclusion , our case report underlines the importance of monitoring the evolution of tissue rebiopsy for identifying heterogeneous resistance mechanisms , especially in patients with aggressive progression , the disease and of to better dene potential treatment modications . 
pizzutilo , calogero lauricella , giulio cerea , massimo torre , salvatore siena , andrea sartore - bianchi financial support : salvatore siena provision of study materials or patients : elio g . 
giannetta , stefano stabile , valentina motta , spyridon alexiadis , angelo vanzulli , emanuela bonoldi , silvio m . veronese , salvatore siena , andrea sartore - bianchi data analysis and interpretation : elio g . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . angelo vanzulli travel , accommodations , expenses : bracco diagnostics , ge healthcare emanuela bonoldi consulting or advisory role : bayer silvio m . 
mitsudomi t , morita s , yatabe y , et al : getinib versus cisplatin plus docetaxel in patients with non - small - cell lung cancer harbouring mutations of the epidermal growth factor receptor ( wjtog3405 ) : an open label , randomised phase 3 trial . 
lancet oncol 11 : 121 - 128 , 2010 rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutationpositive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
lancet oncol 13 : 239 - 246 , 2012 sequist lv , yang jc - h , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
j clin oncol 31 : 3327 - 3334 , 2013 soria j - c , ohe y , vansteenkiste j , et al : osimertinib in untreated egfr - mutated advanced non - small - cell lung cancer . 
 case report thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . nat med 21 : 560 - 562 , 2015 10 . 
niederst mj , hu h , mulvey he , et al : the allelic context of the c797s mutation acquired upon treatment with third - generation egfr inhibitors impacts sensitivity to subsequent treatment strategies . 
rolfo c , mack pc , scagliotti gv , et al : liquid biopsy for advanced non - small cell lung cancer ( nsclc ) : a statement paper from the iaslc . 
tan dsw , yom ss , tsao ms , et al : the international association for the study of lung cancer consensus statement on optimizing management of egfr mutation - positive non - small cell lung cancer : status in 2016 . 
j thorac oncol 11 : 946 - 963 , 2016 jukna a , montanari g , mengoli mc , et al : squamous cell carcinoma transformation concurrent with secondary t790m mutation in resistant egfr - mutated adenocarcinomas . 
yu ha , arcila me , rekhtman n , et al : analysis of tumor specimens at the time of acquired resistance to egfr - tki therapy in 155 patients with egfr - mutant 75ra26 , 2011 lung cancers . 
oxnard gr , hu y , mileham kf , et al : assessment of resistance mechanisms and clinical implications in patients with egfr t790m - positive lung cancer and acquired resistance to osimertinib . 
yang z , yang n , ou q , et al : investigating novel resistance mechanisms to third - generation egfr tyrosine kinase inhibitor osimertinib in non - small cell lung cancer patients . 
leone a : c797s and t790m egfr mutations in non - small cell lung cancer : in trans or in separate clones ? j thorac oncol 13 : e21 - e22 , 2018 19 . 
wang z , yang j - j , huang j , et al : lung adenocarcinoma harboring egfr t790m and in trans c797s responds to combination therapy of rstand thirdgeneration egfr tkis and shifts allelic conguration at resistance . 
zhou z , zhao y , shen s et al : durable clinical response of lung adenocarcinoma harboring egfr 19del / t790m / in trans - c797s to combination therapy of rstand third - generation egfr tkis . 
minari r , bordi p , del re m , et al : primary resistance to osimertinib due to sclc transformation : issue of t790m determination on liquid re - biopsy . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a third - generation egfr inhibitor . 
marcoux n , gettinger sn , okane g , et al : egfr - mutant adenocarcinomas that transform to small - cell lung cancer and other neuroendocrine carcinomas : clinical outcomes . 
they demonstrated that one or a number of molecular alterations could commonly be identied in the circulating dna of these patients . their key nding was that 55% of these patients demonstrated therapeutically relevant alterations in their ctdna.1 because these alterations would be unexpected in patients without an underlying malignancy , their comprehensive work suggests another tool to aid in the often difcult task of diagnosing btc . the authors comment that of particular importance , pathologic tissue - based conrmation of btc can be challenging given that clinical yield is often suboptimal and insufcient1 in fact , despite using endoscopic retrograde cholangiopancreatography with brushings ( including forceps biopsies ) , endoscopic retrograde cholangiopancreatography with endoscopy , percutaneous cholangioscopy , and cholangioscopy with spyglass , diagnosing btc in patients suspected to have btc remains particularly challenging . 
for example , in 2018 , a worldwide study revealed that 8% to 22% of patents turned out to have benign disease on microscopic examination of resected specimens.2 mody and cleary3 recently reviewed the potential usefulness of evaluating circulating dna in diagnosing hepatocellular carcinoma and other cancers . 
rizvi et al4 and wasenang et al5 reviewed the evidence and presented data that differentially methylated circulating cellfree dna regions might aid in distinguishing malignant from nonmalignant causes of signs and symptoms in patients where btc is included as part of the differential diagnosis . 
a case of molecularly diagnosed cholangiocarcinoma on the basis of clinical suspicion and after multiple failed attempts at a tissue diagnosis has also been described.7 if btc is suspected , the lack of ctdna consistent with btc could result from the patients having only a small tumor volume and shedding of insufcient mutated dna to be identied . 
however , if the circulating dna included one or more of the molecular alterations described in the study by mody et al1 and in reports by others , it is almost certainly reasonable to conclude that there is an underlying btc in a clinical setting consistent with the patient harboring a btc and no other apparent malignancy . 
aside from being derived from a different tumor of origin , only a couple of the alterations they described would be potentially unrelated to a nonmalignant source , although , for example , identication of circulating brcamutated dna might imply a germline mutation without an underlying related malignancy , and circulating mutated tp53 might be related to clonal hematopoietic cells of indeterminate potential.8 an expert panel of the american society of clinical oncology and the college of american pathologists concluded that , in general , the evidence is currently lacking to support the use of cell - free dna evaluation for early - stage cancer diagnosis.9 however , btc in particular is often difcult to diagnose , even at a locally advanced stage . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . steven sorscher honoraria : celgene , pzer , puma speakers bureau : celgene , pzer , puma travel , accommodations , expenses : celgene , pzer , puma references 1 . 
wasenang w , chaiyarit p , proungvitaya s , et al : serum cell - free dna methylation of opcml and hoxd9 as a biomarker that may aid in differential diagnosis between cholangiocarcinoma and other biliary diseases . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
j clin oncol 36 : 1631 - 1641 , 2018 jaiswal s , fontanillas p , flannick j , et al : age - related clonal hematopoiesis associated with adverse outcomes . 
the other two articles are case reports of breast and gastroesophageal cancer with mismatch repair deficiency ( dmmr ) where immunotherapy resulted in remarkable responses . these articles are highly relevant because the us food and drug administration ( fda ) approved pembrolizumab in may 2017 for the treatment of all unresectable or metastatic cancer with msi / dmmr irrespective of tissue origit was the first time that any therapy had been approved for cancers that share a specific genetic feature irrespective of site of origfurthermore , in late july , nivolumab was approved for msi / dmmr metastatic colorectal cancer . 
the fda approvals are based on studies showing disease control rates of 70% to 90% in patients with colorectal cancer and noncolorectal msi / dmmr cancers , most of whom with disease that was refractory to standard chemotherapy upon entering these trials.1 - 3 these trials had not reached median progression - free survival1 , 2 or overall survival1 - 3 at the time of publication , indicating that the responses are durable . msi is defined as a difference in length of microsatellites ( dna nucleotide repeats ) when comparing tumor dna with normal dna from the same individual . 
deficiency in the mmr system , a dna repair system in charge of correcting errors during dna replication , causes a distinct accumulation of errors in microsatellites , as well as a hypermutated phenotype . 
the mmr system is most commonly inactivated in tumors by either somatic inactivation via methylation of the mlh1 gene , 4 germline mutations in the mmr genes ( mlh1 , msh2 , msh6 , and pms2 [ lynch syndrome ] ) , 5 or , more rarely , somatic mmr mutations.6 , 7 dmmr can be detected by two widely implemented methods : immunohistochemistry ( tumor is stained for the four mmr proteins ) and msi testing via polymerase chain reaction ( pcr )  . 
these two methods have a high concordance.8 traditionally , msi testing has been done via pcr focusing on five predefined microsatellites ( monoor dinucleotide microsatellites ) , which were initially chosen during a meeting in bethesda in 1997.9 , 10 with the advent of ngs with targeted gene sequencing or whole exome / genome sequencing , myriad microsatellites can now be investigated simultaneously with computational tools . 
at least four different computational tools have been developed : msings , 11 msisensor , 12 mantis , 13 and mosaic.14 so how common is msi / dmmr in cancer ? it is well known that the highest msi / dmmr incidences are observed in endometrial cancer ( 20% to 30% ) , 15 - 17 colorectal cancer ( 12% to 15% ) , 18 , 19 and gastric cancer ( 15% to 20% ) , 20 although rates may be lower when focusing on metastatic disease ( 4% to 5% in colorectal cancer in populationbased studies ) .21 , 22 bonneville et al23 examined msi with mantis software in 11 , 139 tumors ( 39 cancer types ) , mostly derived from the cancer genome atlas , using whole exome sequencing data ( including 2 , 530 microsatellites )  . 
the study by middha et al24 describes lower rates of msi compared with bonneville et al , 23 but it is probably as a result of the more advanced stages examined in the study by middha et al . 
both studies looked at mutational burden and found that msi tumors have a significantly higher mutational burden compared with microsatellite stable ( mss ) tumors . do msi cases found via msi - ngs always signify tumors with dmmr ? or could they have other etiologies causing msi ? mantis had previously been validated against samples with msi by pcr in colorectal cancer , endometrial cancer , gastric cancer , esophageal cancer , and prostate cancer , as well as uterine carcinomasarcoma.13 in the study by bonneville et al , 23 the investigators examined ngs data of the mmr genes and found mmr mutations in some cases , but do not have data on mlh1 hypermethylation , which is the most common reason for msi . 
in the study by middha et al , 24 the msi status was validated in 138 colorectal and endometrial cancer cases by performing mmr immunohistochemistry and conventional msi by pcr . 
they found a high concordance between the methods ( 99.4% ) , and msi by ngs seems slightly more sensitive than msi by pcr because they discovered three msi cases by msisensor that scored as msi - low or mss on pcr but were dmmr on immunohistochemistry . 
furthermore , they investigated 456 other cancer cases that scored low ( 3 to 10 ) on msisensor and found that only 3.5% were discordant ( msi by pcr ) , reflecting the fact that most cases with low msi are not truly dmmr.10 ideally , validation would be done for every tumor type to ensure that msi is detected across a range of different cancers and truly represents dmmr . 
in the study by middha et al , 24 one case with a pole mutation was msh6 deficient and msi ; all other pole - mutated cases were mss by msisensor and had normal mmr immunohistochemistry , suggesting that msi in pole - mutated cases is secondary to mutations in mmr genes . other studies have described similar findings.6 , 25 the case reports are great examples of how tumors that are not typically associated with msi status can respond dramatically to immunotherapy . 
in the study by kok et al , 26 a 69 - year - old patient with metastatic breast cancer responded to nivolumab , with complete resolution of a malignant gastric ulcer after three cycles and an ongoing response after 12 cycles of nivolumab . 
in the study by klempner et al , 27 an 85 - yearold patient with stage iii gastroesophageal adenocarcinoma , deemed not a surgical candidate , had a complete response to pembrolizumab , with an ongoing response for 8 months . 
because mlh1 - hypermethylated tumors are more commonly observed in older patients , 16 , 20 , 28 a patients age should not deter physicians from investigating msi / dmmr . with the fdas recent approval of immunotherapy in msi / dmmr advanced cancers , and the finding of this molecular signature across a broad range of tumor types , screening all metastatic cancer cases for msi should become standard practice . 
companies and / or institutions who offer multiple gene sequencing panels should strongly consider integrating msi analysis into their existing ngs protocols and include this as part of their reporting . 
some panels are already reporting this , such as the foundation one platform . it is unclear how many of the msi cases found in the studies by bonneville et al23 and middha et al24 were caused by lynch syndrome . 
in prior studies , 10% to 15% of msi / dmmr colorectal cancer cases and 10% of msi / dmmr endometrial cancer cases were caused by lynch syndrome.21 , 22 , 29 lynch syndrome can increase the risk of many of the malignancies found to be msi in the studies presented in jco precision oncology ; thus it is important for physicians to refer patients with msi / dmmr cancers to the genetics clinic ( the exception being mlh1 / pms2 - absent cancers that test positive for mlh1 hypermethylation , because most of these cases are somatic )  . 
overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - deficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
kane mf , loda m , gaida gm , et al : methylation of the hmlh1 promoter correlates with lack of expression of hmlh1 in sporadic colon tumors and mismatch repair - defective human tumor cell lines . 
haraldsdottir s , hampel h , tomsic j , et al : colon and endometrial cancers with mismatch repair deficiency can arise from somatic , rather than germline , mutations . 
bartley an , luthra r , saraiya ds , et al : identification of cancer patients with lynch syndrome : clinically significant discordances and problems in tissue - based mismatch repair testing . 
boland cr , thibodeau sn , hamilton sr , et al : a national cancer institute workshop on microsatellite instability for cancer detection and familial predisposition : development of international criteria for the determination of microsatellite instability in colorectal cancer . 
billingsley cc , cohn de , mutch dg , et al : polymerase e ( pole ) mutations in endometrial cancer : clinical outcomes and implications for lynch syndrome testing . 
 sunitinib in the treatment of thymoma and associated autoimmune neutropenia introduction autoimmune disorders such as myasthenia gravis or pure red cell aplasia ( prca ) are frequent in patients with thymoma . 
thymoma - associated neutropenias , however , are rare ; to the best of our knowledge , only 17 patients have been described.1 - 16 for these patients , the diagnosis of neutropenia occurred simultaneously with that of thymoma or , less often , during the disease course , 2 , 4 - 8 , 10 - 16 and was frequently associated with myasthenia gravis , hypogammaglobulinemia , or anemia.2 - 12 , 14 - 16 granulopoiesis has been described as being completely or almost completely absent or as being arrested at the promyelocyte stage.2 - 7 , 9 , 10 , 12 - 16 bone marrow ( bm ) lymphocytosis is frequent and predominantly the result of t - cell infiltration.2 , 6 , 7 , 10 , 13 in one patient , a monoclonal rearrangement of the t - cell receptor ( tcr ) beta chain was found.8 thymoma - associated neutropenia is likely of autoimmune etiology ( ie , autoimmune neutropenia [ ain ] )  . 
antinuclear antibodies were present4 , 10 - 12 , 14 or not6 , 12 , 15 ; antineutrophil cytoplasmic antibodies were positive in one article , 11 with a decrease in titer upon neutrophil recovery . 
antigranulocyte antibodies were not detected5 , 9 , 12 or present10 ; in the latter case , the antibodies did not react with common human neutrophil antigens.10 studies consistently showed decreased granulocyte - macrophage colony formation in the bm of patients or controls in the presence of patients serum , 5 - 7 , 9 , 10 , 12 whereas formation was not affected by control sera or patients lymphocytes or thymoma cells.5 , 7 , 10 the inhibitory activity of the patients serum was present in the immunoglobulin g fraction.5 , 9 , 10 the treatment of thymoma - associated ain resembles that of prca17 and comprises the use of immunosuppressants ( eg , corticosteroids , 5 , 7 - 13 cyclosporine , 13 - 15 azathioprine , 9 cyclophosphamide , 5 , 10 , 12 mycophenolate , 14 or alemtuzumab14 ) , intravenous immunoglobulins , granulocyte colony - stimulating factor , plasmapheresis , and / or thymectomy.5 , 7 , 9 - 15 neutrophil response varied widely among the patients described . the tyrosine kinase inhibitor sunitinib has recently been shown to be effective against thymic carcinoma and , less frequently , type b thymoma in a phase ii trial and in retrospective analyses.18 , 19 sunitinib inhibits the receptors for the plateletderived growth factor receptor , vascular endothelial growth factor receptor ( vegfr ) , and stem cell factor ( kit ) , as well as other kinases . 
the patient provided written informed consent for the research use of the clinical data and biomaterial in accordance with the declaration of helsinki , as approved by the local ethics committee ( university of freiburg )  . the patient , a 33 - year - old man , was diagnosed with thymoma b2 in masaoka stage iva ( table 1 )  . he received three courses of cisplatin , doxorubicin , and cyclophosphamide ( pac ) chemotherapy followed by total thymectomy and resection of adjacent structures , leaving only microscopic tumor residues . 
shortly thereafter , computed tomography scans revealed new lesions in the right cardiophrenic angle and mediastinuthe patient then agreed to receive radiotherapy . radiotherapy was interrupted after 20 gy because of neutropenia and anemia . 
the neutrophils spontaneously rapidly recovered , but the anemia persisted until corticosteroid therapy was started . after recovery of the blood counts and stopping corticosteroids , and in the light of new lesions , radiotherapy was reinitiated but again stopped heiko becker konrad auman rainer claus nikolas von bubnoff ulrich j . 
diagnosed with thymoma b2 in masaoka stage iva . biopsy negative for variants ( non - synonymous and allele frequency > 10% ) in braf exon 15 ; egfr exons 18 , 19 , 20 , 21 ; kras exons 2 , 3 , 4 ; kit exons 9 , 11 , 13 , 17 ; nras exons 2 , 3 ; pdgfra exon 18 ; pi3kca exons 9 , 20 . 
bold font indicates days being on sunitinib treatment ( v being off treatment )  . abbreviations : gat , granulocyte agglutination test ; gift , granulocyte immunofluorescence test ; nd , not determined . * the interval between the end of cycle 2 and the start of cycle 3 was prolonged by 4 weeks because of patients personal reasons ; during this interval , granulocyte colony - stimulating factor was prophylactically applied once per week . computed tomography scan : progressive disease ; discontinuation of sunitinib treatment after 20 gy because of neutropenia , this time not coinciding with anemia . during the following treatment break , the blood counts completely recovered , but the thymoma lesions slowly progressed , which was associated with increased pain and deterioration of the patients general condition . 
at the same time , the patient developed a severe neutropenia ; the lowest wbc count at presentation was 1.290 3 109 / l with bands accounting for 8% , segmented cells 12% , basophils 2% , monocytes 15% , and lymphocytes 62% . 
immunoglobulin g was decreased ( 420 mg / dl ) ; c - reactive protein and c3d levels were increased , and procalcitonin was repeatedly normal . the patient had not received any thymoma - specific systemic therapy or radiotherapy for approximately fig 1 . 
the patient had taken valproic acid for epilepsy since adolescence . bm examination showed hypoplasia and a marked left shift of the granulopoiesis with almost complete absence of mature granulocytes ( fig 1 ) , which was associated with hyperplasia of the erythropoiesis and megakaryopoiesis , and an interstitial t - cell infiltration ( cd1a , predominantly terminal deoxynucleotidyl transferasenegative )  . in the blood , the cd4 : cd8 and tcr alpha / beta : gamma / delta cell ratios were slightly decreased ( table 2 )  . 
although a low cd4 : cd8 ratio as a result of the relative increase of cd8 + cells has been inconsistently described in patients with thymoma , 24 , 25 our patient had normal cd8 + cell counts . 
no clonal tcr gamma rearrangement was detected . in the search for granulocyte autoantibodies , we performed granulocyte agglutination ( gat ) and granulocyte immunofluorescence tests ( gifts ; table 1 )  . 
in enzyme immunoassays , no reactions were observed against hla class i antigens or human neutrophil antigens cd16b , cd11a , cd11b / cd18 , and cd177 . the neutropenia repeatedly displayed prompt but short - lasting responses to granulocyte colony - stimulating factor application . 
this decision was based on the efficacy of sunitinib against thymoma , 18 , 19 our reluctance to apply chemotherapy during neutropenia , and consideration of the immunomodulatory effect of sunitinib.21 - 23 we decided to use sunitinib at a dose of 25 mg / day because adverse effects were common at higher doses in patients with thymoma18 and in 6 - week cycles ( 4 weeks of treatment followed by 2 weeks without treatment )  . sunitinib treatment was associated with a rapid increase in neutrophil counts and decrease in inflammation parameters and granulocyte antibodies ( table 1 )  . 
moreover , the computed tomography scan showed stable disease . because adverse effects had been minimal during cycle 1 , we increased the dose to 37.5 mg / day in cycle 2 , which resulted in mucositis , sinus arrhythmia , and decreased left ventricular contractility , all of which improved during treatment break . 
from cycle 3 on , we kept the sunitinib dose at 25 mg / day and used an alternative application schedule ( ie , 3 - week cycles consisting of 2 weeks of treatment and 1 week without treatment , in accordance with a current trial [ nct01621568 ; sunitinib for advanced thymus cancer following earlier treatment ] )  . 
subsequent treatments included paclitaxel and gemcitabine . at the last follow - up , approximately 4 months after sunitinib was stopped , the patient remained without neutropenia and no granulocyte antibodies were detected . the rationale for the initial trials of sunitinib in patients with thymoma was the expression and mutation profile of distinct signaling molecules . in retrospective analyses of the thymoma biopsy from the diagnosis , immunohistochemistry showed weak expression of vegfr1 and vegfr2 and no expression of kit . 
in miseq ( illumina , san diego , ca ) - based sequencing of thymoma cells microdissected on the basis of their morphology , no variants were identified in the genes analyzed ( table 1 )  . sunitinib alters the ctla4 expression on cd8 + t cells and pd1 expression on regulatory t cells in patients with thymoma , and low ctla4 and decrease of pd1 are associated with shorter survival among patients with thymoma who are treated with sunitinib.18 although we have no data on pd1 or ctla4 , immunohistochemistry showed moderate to high pd - l1 expression on the thymoma cells . discussion the patient was diagnosed with thymoma b2 in masaoka stage iva ; he developed prca under radiotherapy , which resolved with corticosteroid treatment , and ain under progression of the thymoma , which resolved with sunitinib treatment . although we cannot exclude with certainty another cause for the ain besides the thymoma , the causative relationship is supported by the simultaneous occurrence of the ain and the progression of the thymoma and by the previous reports describing the development of ain in patients with thymoma.1 - 16 considering that the etiology of thymomaassociated ain is a matter of debate , we here demonstrate a clear association between neutrophil counts and the detection of autoantibodies against granulocytes that were present at diagnosis and disappeared under treatment . one may speculate that the neutropenic episodes under radiotherapy that were once associated with prca may have been temporary occurrences of the ain . 
however , bm findings ( ie , hypoplastic erythropoiesis , maturing granulopoiesis ) and the rapid and stable wbc recovery without immunosuppressive therapy suggest that these neutropenic episodes were indeed related to radiotoxicity . to the best of our knowledge , this is the first description of a thymoma - associated autoimmune disorder that resolved under sunitinib . 
in the study by thomas et al , 18 two patients developed prca or hypogammaglobulinemia while receiving sunitinib ; three patients had autoimmune disorders before receiving sunitinib and not during treatment , but it was not specified whether these disorders were present when sunitinib therapy was started ( as opposed to earlier ) and then improved under therapy . because our report is based on clinical observations , we cannot exclude that the neutropenia only coincidentally improved during sunitinib treatment . 
sachs no relationship to disclose konrad aumann research funding : novartis ( inst ) travel , accommodations , expenses : novartis rainer claus honoraria : janssen oncology , roche , novartis consulting or advisory role : roche , janssen oncology speakers bureau : janssen oncology travel , accommodations , expenses : janssen oncology , abbvie , roche nikolas von bubnoff honoraria : novartis , bristol - myers squibb consulting or advisory role : novartis research funding : novartis travel , accommodations , expenses : novartis cornelius f . 
waller consulting or advisory role : mylan , teva , boehringer ingelheim , bristol - myers squibb , astrazeneca , msd , roche travel , accommodations , expenses : bristol - myers squibb acknowledgment we thank ingrid bartsch for flow cytometry analyses and the molecular tumor board ( medical center , university of freiburg , germany ) for the thorough and elaborate discussion of the case . 
schweiz med wochenschr 97 : 1606 - 1611 , 1967 jacobson bm , castleman b : case 1 - 1971anemia , granulocytopenia and terminal sepsis in a 70 - year - old woman . n engl j med 284 : 39 - 47 , 1971 4 . 
nagashima s , yamato h , saito k , et al : cd8 + agranular lymphocyte proliferative disorder with t - cell receptor betachain gene rearrangement associated with thymoma and neutropenia [ in japanese ]  . 
mathieson pw , oneill jh , durrant st , et al : antibody - mediated pure neutrophil aplasia , recurrent myasthenia gravis and previous thymoma : case report and literature review . 
kobayashi m , hasegawa t , iwabuchi s , et al : the effect of thymectomy on myasthenia gravis , thrombocytopenia , and granulocytopenia associated with thymoma : report of a case . 
hirokawa m , sawada k , fujishima n , et al : long - term response and outcome following immunosuppressive therapy in thymoma - associated pure red cell aplasia : a nationwide cohort study in japan by the prca collaborative study group . 
thomas a , rajan a , berman a , et al : sunitinib in patients with chemotherapy - refractory thymoma and thymic carcinoma : an open - label phase 2 trial . 
finke jh , rini b , ireland j , et al : sunitinib reverses type - 1 immune suppression and decreases t - regulatory cells in renal cell carcinoma patients . 
ozao - choy j , ma g , kao j , et al : the novel role of tyrosine kinase inhibitor in the reversal of immune suppression and modulation of tumor microenvironment for immune - based cancer therapies . 
gu y , zhao w , meng f , et al : sunitinib impairs the proliferation and function of human peripheral t cell and prevents t - cell - mediated immune response in mice . 
hoffacker v , schultz a , tiesinga jj , et al : thymomas alter the t - cell subset composition in the blood : a potential mechanism for thymoma - associated autoimmune disease . 
faden , md1 , 2 ; roberto gomez - casal , ms3 ; diego alvarado , phd4 ; and umamaheswar duvvuri , md , phd3 introduction the epidermal growth factor receptor / human epidermal growth factor receptor ( her ) family plays a critical role in the growth of numerous human cancers . multiple therapeutics targeted to members of the her family have been developed , including the epidermal growth factor receptortargeting monoclonal antibody cetuximab , which is fda approved for treatment of head and neck squamous cell carcinoma ( hnscc )  . her3 / erbb3 is expressed in most solid tumors , including hnscc , and has been shown to correlate with a poor prognosis.1 , 2 phosphorylation of erbb3 ( perbb3 ) affects numerous pathways , including activation of the pi3k / akt pathway , driving cell survival and growth . 
for this reason , blocking erbb3 activity could be an effective strategy to decrease tumor growth and resistance to other tyrosine kinase inhibitors.3 - 5 cdx - 3379 is a human immunoglobulin g1 lambda monoclonal antibody that binds erbb3 and inhibits its activity by multiple mechanisms . 
after pathologic conrmation by biopsy , informed consent was obtained , the patient was enrolled in nct02473731 and given two 1 , 000 mg intravenous doses of cdx - 3379 . 
a signiresponse was noted within the rst cant clinical 48 hours after administration of the rst dose , with concomitant reduction in pain from 8 of 10 to 2 of 10 . on examination before surgical extirpation , the primary tumor was found to have a nearly complete response , demonstrating a 92% reduction in greatest dimension . 
tumor and germline dna underwent whole exome sequencing ( wes ) library construction with the illumina truseq kit ( san diego , ca ) , with exonic regions captured using agilent sureselect v4 ( santa clara , ca )  . 
rna underwent library preparation with the illumina truseq rna access kit followed by pairedend ( 2 76 ) sequencing on an illumina nextseq 500 , with average coverage of 45 million reads per sample . primary processing of sequence data was performed using illumina casava software v1.8. 
somatic mutations and copy number variants ( cnvs ) were identied by variantdx as previously described.10 all nonsynonymous coding variants , splice site variants , indels , and cnvs above or below 2.0 were considered potentially deleterious . 
after adapter trimming with cutadapt v1.5 , reads were mapped to the human reference genome grch37 / 38 using hisat2 v2.0.4 , and gene expression was quantitated using htseq v0.9. 
differential gene expression was performed using edger v3.20.9. quantitative real - time polymerase chain reaction total rna was isolated from human hnscc cell lines ( te6 , kyse510 , te9 , fadu , pecapj34 , cal33 , scc4 , bhy , osc19 , scc25 ) using the qiagen rneasy kit . 
 faden et al real - time polymerase chain reaction ( pcr ) was performed using the bio - rad iq sybr green supermix and applied biosystems 7900ht fast real - time pcr systethe following primers were used to detect fzd3 mrna : 5 ( cid : 2 ) - gcttccacagtgacacaagg - 3 ( cid : 2 ) and 5 ( cid : 2 ) - accatacactgccagccata - 3 ( cid : 2 )  . to detect erbb3 mrna , the following primers were used : 5 ( cid : 2 ) - actctccatatcccttcctctc - 3 ( cid : 2 ) and 5 ( cid : 2 ) - gtttcctccctttcctctct - 3 ( cid : 2 )  . pcr amplications were run in triplicate for each cell line . comparative quantication of gene expression was performed using the ct method , and values were referenced to gapdh mrna expression . erbb3 phosphorylation erbb3 phosphorylation was measured by veratag assay ( san francisco , ca ) on ffpe tissue.6 colony - formation assays five thousand cells per well were seeded in six - well plates and allowed to attach overnight . 
the area covered by stained cells was measured using imagej . statistical analysis was performed using graphpad prism 7 . perbb3 was assessed by veratag assay to examine changes in activated erbb3 pretreatment to post - treatment , revealing a 69% decrease from 0.45 to less than 0.14 ( lower limit of quantitation of the assay ) , demonstrating successful blockage of erbb3 activation by cdx - 3379 . 
we hypothesized that loss of somatic alterations from pretreatment to post - treatment , in combination with a signicant reduction in clinical tumor volume , could represent selective killing of clones more sensitive to cdx - 3379 and thus give insight terrogating the list of alterations that were present in the tumor pretreatment but not post - treatment ( on the basis of known mechanisms of action of each gene ) identied amplication of fzd3 ( frizzled class receptor 3 ) , a receptor in the wnt signaling pathway , as a possible candidate conferring sensitivity to cdx - 3379 ( table 1 )  . 
rna - seq demonstrated a 2.5 - foldhigher expression of fzd3 pretreatment versus post - treatment ( p , 4.5e - 13 ) , consistent with the 3.0 amplication identied on wes in the pre ( fig 1a )  . 
six percent ( 28 of 496 ) of hnsccs in tcga possess an fzd3 alteration that could result in an increase in downstream wnt signaling , consistent with the case reported here ( one amplication and 27 mrna upregulations )  . 
patients with hnsccs from tcga that possess an fzd3 alteration have poorer overall survival , suggesting that alterations in this gene may be important in the biology of a subset of hnsccs ( fig 1b )  . tumor to explore the possibility that fzd3 plays a role in sensitivity to erbb3 inhibition , we examined fzd3 mrna expression lines , by quantitative real - time pcr in 10 hnscc cell nding high variability among cell lines ( fig 1c )  . 
to test the hypothesis that increased fzd3 expression could render cells more sensitive to cdx - 3379 , akin to the pretreatment tumor , we performed colony - formation assays with table 1 . 
the role of wnt signaling pathways in cancer is well established.11 fzd upregulation has been identied in numerous cancers , correlates with poor outcomes , and is an active area of investigation for targeted therapeutics.11 , 12 fzd3 , in particular , is believed to play a role in both the canonical and noncanonical wnt pathways and has been found to be upregulated in lung , esophageal , and colon cancers.13 - 15 here , we report fzd3 gene amplication and overexpression in pretreatment but not post - treatment tumor from an exceptional responder to cdx - 3379 . 
review of fzd3 in hnsccs from tcga supports the potential biologic importance of alterations in this gene . we further demonstrate that fzd3 expression levels correlate with sensitivity to cdx - 3379 and that activation of fzd3 by its ligand wnt3a further potentiates the effects of cdx - 3379 . 
the mechanism by which fzd3 confers sensitivity to erbb3 inhibition is unclear ; however , the wnt and erbb pathways have been reported to closely interact and collude in tumorigenesis.16 , 17 it remains to be seen whether this is by convergence on a common downstream molecule , such as - catenin , 18 or via effects on different target genes . 
in breast cancer , wnt overexpression activates signaling via erbb.19 , 20 interestingly , we identied a tight correlation between erbb3 and fzd3 mrna expression levels in hnscc cell lines , suggesting a similar relationship and highlighting the interconnected nature of these singling pathways . 
images of a representative colony formation ( top ) with quantication of stained area represented in bar graph ( middle ) and culture additives ( bottom ) p , .001 for all comparisons by one - way analysis of variance . 
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a major barrier is that many conventional designs are inadequate for modern drug development , yet most novel adaptive designs are difcult to understand , require complicated statistical modeling , demand complex computation , and need expensive infrastructure for implementation . 
the objective of this article is to introduce and review a class of novel adaptive designs , known as model - assisted designs , to remove this barrier and increase the use of novel adaptive designs . 
model - assisted designs enjoy superior performance comparable to more complicated , model - based adaptive designs , but their decision rule can be pretabulated and included in the protocolthus implemented as simply as the conventional designs . 
we review state - of - the - art model - assisted designs for phase i clinical trials for single - agent , drug - combination and late - onset toxicity scenarios . 
as a result , conventional designs ( eg , the 3 + 3 design ) are still dominantly used despite relatively poor performance . there is an urgent need to increase the adoption of novel adaptive designs . the objective of this article is to introduce and review a class of novel phase i and ii designs , known as model - assisted designs , 10 - 12 to overcome this quandary of simplicity versus performance . 
model - assisted designs yield superior performance compared with the conventional algorithm - based designs and are comparable to more complicated ( model - based ) designs . with the model - assisted designs , the decision rule can be pretabulated and included in the protocol and , thus , implemented in as simple a way as the conventional designs . 
 yuan et al context key objective is there any novel adaptive design that is simple to implement ? knowledge generated this article introduces and reviews a class of novel phase i and ii designs , known as model - assisted designs , to provide a stateof - the - art approach to overcome the quandary of simplicity versus performance that hinders the adoption of novel adaptive designs . 
model - assisted designs yield superior performance compared with more complicated model - based designs , but the decision rule can be pretabulated and included in the protocol and , thus , implemented in as simple a way as the conventional designs . relevance model - assisted designs are easy to implement and have great potential to improve the efciency and success rate of earlyphase trials . estimate the dlt rate , and has a greater tendency to underdose patients ( ie , it treats patients at the doses lower than the mtd )  . 
despite decades of advocacy by statisticians , the use of the crm , however , is still limited because of statistical and computational complexity of the design.8 , 9 for appropriate use , the crm requires specialized expertise to choose and calibrate the dose - toxicity model and to re - estimate the model at each decision of dose escalation / de - escalation . 
examples of model - assisted designs include the modied toxicity probability interval ( mtpi ) design23 and its variation , mtpi - 224 ; bayesian optimal interval ( boin ) design25 , 26 ; and keyboard design22 ( fig 1 )  . 
given the data observed at current dose , mtpi makes the decision of dose escalation and de - escalation on the basis of the unit probability mass ( upm ) of the three intervals . 
the upm of an interval is dened as the posterior probability that p is within the interval divided by the length of the interval , calculated according to a statistical model known as the beta - binomial model . 
comparison of design characteristics among algorithm - based , model - based , and model - assisted phase i designs algorithm based model assisted model based design characteristic transparency and simplicity in the protocol dose escalation / de - escalation rule can be predetermined and included avoids computation - intensive , repeated estimation of the dose - toxicity curve model to make interim decisions flexibility size targets any prespecied dlt rate allows decision making when the cohort size deviates from the planned no . 
6 sample size can be calibrated to ensure good operating characteristics performance identies the mtd accurately allocates a high percentage of patients to the mtd provides good overdose control abbreviations : dlt , dose - limiting toxicity ; mtd , maximum - tolerated dose . the dose stays at the current dose . 
one deciency of mtpi is that it overly downweighs the overdosing probability , because the overdosing interval is typically wider than the proper dosing interval , which leads to a high risk of overdose of patients ( ie , treatment of a high percentage of patients at doses greater than the mtd ) .22 the keyboard design addresses the overdosing issue of mtpi by dening a series of equal - width dosing intervals ( or keys ) to represent the potential locations of p.22 the proper dosing interval is called the target key . 
the design makes the decision of dose escalation and de - escalation by examining the relative position between the target key and the strongest key , in which the strongest key is dened as the interval that the true dlt is most likely located . 
if the strongest key is on the left ( or right ) side of the target key , the observed data suggest that the current dose is most likely underdosing ( or overdosing ) ; thus , the design escalates ( or de - escalate ) the dose ; otherwise , the dose stays at the current dose . 
the keyboard design outperforms the mtpi with substantially lower risk of overdosing patients and better accuracy to identify the mtd.11 , 22 the variation of the mtpi ( ie , mtpi - 224 ) adopts the same dose escalation / de - escalation rule as the keyboard design but is less transparent . 
the mtpi - 2 relies on complicated procedures , such as occams razor and model selection . compared with the mtpi / mtpi - 2 and keyboard designs , the boin design is more straightforward and transparent ( fig 1 )  . 
let p denote the observed dlt rate at the current dose , dened as the number of patients experiencing dlt at the current dose divided by the total number of dltevaluable patients treated at the current dose . the boin design makes dose escalation / de - escalation recommendations simply by comparing p with prespecied dose escalation ( e ) and de - escalation ( d ) boundaries , as illustrated in figure 2 and described as follows : 1 . 
repeat step 2 until the prespecied maximum sample size is reached or the number of patients treated on a single level reaches a certain number ( eg , 12 )  . 
at that point , select the mtd as the dose at which the dlt estimate is closest to the target.25 , 26 figure 2 provides the default , optimal dose escalation and deescalation boundaries ( e , d ) for commonly used target dlt rates ,  . 
for patient safety , boin imposes an overdose control rule : if the observed data indicate that there is more than a 95% chance that the current dose is higher than and at least three patients have been treated , the current and higher doses are eliminated from the trial . 
to determine the next dose , the modied toxicity probability interval design calculates and compares the values of the three unit probability masses ( upms ) , whereas the keyboard design compares the location of the strongest key with respect to the target key . 
bayesian optimal interval compares the observed dlt rate at the current dose with the optimized dose escalation boundary , e , and de - escalation boundary , d . the simple and intuitive structure of boin gives it several unique advantages . 
because boin guarantees deescalation of the dose when the observed toxicity rate p is higher than the de - escalation boundary d , it is particularly easy for clinicians and regulatory agents to assess the safety of a trial with boin . 
for example , given a target dlt rate of = 0.25 , we know a priori that a phase i trial using boin guarantees de - escalation of the dose if the observed dlt rate is higher than 0.298. 
suppose that , for a phase i trial with a new compound , the regulatory agency mandates that the dose must be de - escalated if the observed toxicity rate is higher than 0.25. 
we can easily fulll that requirement by setting the target dlt rate at = 0.21 , such that boin guarantees de - escalation of the dose if the p 0.25. 
such exibility and observed toxicity rate of transparency are the important advantages of boin compared with the other model - assisted designs , such as mtpi / mtpi - 2 and keyboard designs . because model - assisted designs are built upon rigorous statistical theory , like model - based designs , they also enjoy the same exibility as the model - based designs . 
in addition , unlike the 3 + 3 design , for which the dose escalation and de - escalation decisions can be made only when we have three or six evaluable patients , boin allows decision making with incomplete cohorts in the face of dropouts as a result of dlt inevaluability . 
boin design has been used for various treatment agents , including chemotherapy ( clinicaltrials . gov identier : nct02942264 ) , radiotherapy ( clinicaltrials.gov identier : nct03114462 ) , checkpoint inhibitor ( clinicaltrials . gov identier : nct03600155 ) , monoclonal antibody ( clinicaltrials.gov identier : nct03577704 ) , oncolytic virus ( clinicaltrials.gov identier : nct02705196 ) , and t - cell immunotherapy ( clinicaltrials.gov identier : nct03318900 )  . boin also has also been used in nononcology trials , such as stem cell therapy for stroke patients with stroke.35 we used an ongoing national cancer institute phase i to ii trial ( clinicaltrials.gov identier : nct02942264 ) to illustrate the design . 
one of the trials objectives of was to identify the mtd of tg02 , a pyrimidine - based multikinase inhibitor combined with temozolomide in adult patients with recurrent anaplastic astrocytoma or glioblastoma . because of lack of effective treatments for this patient population , the target dlt rate was set at a relatively high value of 0.35. 
according to the toxicity prole of tg02 in other patients with cancer , the principal vestigator chose 200 mg of tg02 as the starting dose . according to the boin design , the dose will be escalated if the observed dlt rate at the current dose is lower than e = 0.276 , and it will be deescalated if the observed dlt rate is greater than d = 0.419 ( fig 2 )  . 
for example , if the dlt takes up to 8 weeks to evaluate and the accrual rate is one patient per week , on average , then ve new patients could be accrued while investigators wait to evaluate the previous three patients outcomes . 
the question is this : how can new patients receive timely treatment when the previous patients outcomes are pending ? a few model - based designs have been proposed to address this logistic issue , including the time - to - event crm ( titecrm ) 38 and data - argumentation crm ( da - crm ) .39 these designs support continuous accrual and yield superior performance in nding the mtd.39 , 40 however , like the crm , they are statistically and computationally complex and require repeated model tting after each cohort , which limits their use . model - assisted designs , including time - to - event boin ( tite - boin ) 29 and time - to - event keyboard ( tite - keyboard ) designs , 41 provide a well - performing and yet easy - toimplement approach to address late - onset toxicity . 
table 2 shows the tite - boin decision rule with a cohort size of three patients , which can be generated easily using the software described in the software section . 
during the trial , at the current dose , we counted the number of patients , the number of patients who experienced dlt , and the number of pending patients and their standard total follow - up times ( stft ) ; we then used the table to make the dose escalation / de - escalation decision . 
to illustrate the use of the tite - boin decision table , suppose that three patients have been treated at the current dose : one had a dlt , one had no dlt , and one has dlt data pending . 
according to table 2 , if the stft of the pending patient is greater than 0.88 , we treat the next cohort at the same dose ; otherwise , we de - escalate the dose . 
suppose that the next cohort of three patients is treated at the same dose and that , among the six treated patients , one patient had a dlt , two had no dlt , and three have dlt data pending . 
unlike single - agent trials with a string of ordered doses , combinations in the dose matrix are only partially ordered in toxicity , and multiple mtds ( ie , the mtd contour ) may exist in the dose matrix ( appendix fig a1 )  . 
numerous designs have been proposed to nd an mtd or the mtd contour for combination trials.28 , 42 - 52 almost all are model - based designs using a strategy similar to that of a crm : devise a model to describe the dose - toxicity surface and then , on the basis of accumulating data , continuously update the model estimate to select a dose for the new patient . 
because of their statistical and computational complexity , despite good performance , these model - based designs are rarely used for conducting trials . model - assisted designs provide a simple and robust approach to phase i combination trials.43 one example is the boin combination design , 28 which makes the decision of dose escalation / de - escalation according to the same rule as the single - agent boin design described in the modelassisted designs section , and thereby inherits the singleagent designs simplicity and good performance . 
the only difference is that , in combination trials , when we decide to escalate or de - escalate the dose , there is more than one neighboring dose to which we can move . 
dose escalation and de - escalation rule for tite - boin with a target dlt rate of 0.3 and a cohort size of three patients , with up to nine patients treated at a dose no . 
for example , simons optimal ( or minimax ) two - stage design53 could be classied as a model - assisted design in the sense that it is derived from a statistical model ( ie , a binomial model for response ) , but its go / no - go decision rule can be predetermined when the design parameters are specied . 
simons optimal two - stage designs are appropriate for the simple setting in which the end point is binary and quickly ascertainable , and these designs allow only one interim look . phase ii trials sometimes are more complicated and have more than one end point . 
table 3 provides four trial examples with different types of end points ( eg , ordinal end point and coprimary end points ) .54 - 56 in addition , multiple interim looks are useful to improve the exibility and efcacy of the trial , especially in basket and platform trials.57 - 59 the bayesian optimal phase ii ( bop2 ) design60 provides a simple , exible , and efcient model - assisted design to allow multiple interims and handle different types of phase ii trials under a unied framework . the key feature of bop2 is that , although the end points in the four examples are clinically different , they all can be represented using a variable y with k distinct categories , statistically known as a multinomial random variable . 
as an example , consider a treatment that is deemed ineffective if the objective response rate ( orr ) is , in which is a threshold prespecied by clinicians ( eg , = 20% )  . 
at each interim , the go / no - go decision is made according to the following bayesian stopping criteria : stop the trial if pr ( orr | data )  . 
given the response rate deemed ineffective ( ie , the null hypothesis ) and the response rate deemed desirable ( ie , the alternative hypothesis ) , the value of cn is chosen such that the type i error rate is controlled at a prespecied level and the statistical power is maximized . 
 ( see zhou et al60 for details . ) similar bayesian stopping criteria can be applied to other types of end points to determine whether the treatment promising.60 in the equation , as a model - assisted design , one important advantage of the bop2 design is that its stopping boundary can be enumerated and included in the trial protocol before the onset of the trial . 
when they conduct the trial , clinicians simply count the number of relevant events and make the go / no - go decision according to whether that count exceeds the boundary or not . 
if the end point requires a long time to be scored , clinicians may have to suspend the accrual and wait for the interim data mature to make interim decisions . 
use the design decision table to conduct the trial and make adaptive decisions ( eg , dose escalation / stay / deescalation or go / no - go )  . discussion one major barrier for the adaptation of novel adaptive designs is that these designs often are complicated to implement . 
model - assisted designs offer the superior performance compared with the more complicated , model - based adaptive designs but , once designed , can be implemented in as simple a way as the conventional designs . 
the approach establishes a new kiss principle : keep it simple and smart ! as in all trial designs , the design parameters for modelassisted designs must be carefully chosen to reect the clinical setting and the study objective . 
for the boin design , the target dlt rate can vary with the type of phase i studies . the maximum sample size must be realistic and attainable . for the bop2 design , the choice of using a binary end point or coprimary end point , and their null and target rates , depends on which disease type is studied and how effective the standard of care is . 
the number of interim analyses should account for both design efciency and the logistic complexity . the choice of designs parameters should be validated and carefully calibrated through extensive computer simulation to ensure that the design has desirable operating characteristics under a variety of scenarios . 
jack lee consulting or advisory role : abbvie no other potential conicts of interest were reported . references kessel m : the problems with todays pharmaceutical business : an outsiders view . 
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 o bayesian adaptive design for finding the maximum tolerated sequence of doses in multicycle dose - finding clinical trials purpose statistical designs for traditional phase i dose - finding trials consider dose limiting toxicity in the first cycle of treatment . 
 therefore , it is desirable to identify the maximum tolerated sequence of three doses across three cycles of treatment . methods motivated by a three - cycle dose - finding clinical trial for a rare cancer with a jak inhibitor , we proposed and implemented a simple bayesian adaptive dose - cycle finding ( basyc ) design that allows intercycle and intrapatient dose modification . 
because of the patient - specific dosing strategy over cycles , the basyc design is suited as a method in precision oncology . results basyc is simple and transparent because its algorithm can be summarized as two tabulated decision rules before the trial starts , allowing physicians to visually examine these rules . 
2018 by american society of clinical oncology introduction phase i oncology clinical trials are typically first - in - human studies characterized by a small number of patients with a goal of determining the maximum tolerated dose of an experimental drug . 
numerous dose - finding designs have been developed , such as the 3 + 3 design , 1 the continual reassessment method , 2 and the modified toxicity probability interval ( mtpi ; mtpi - 2 ) methods , 3 - 5 as recently reviewed by sverdlov et al.6 most of the dose - finding trials consider dlt within the first cycle of treatment as the primary outcome and do not allow multicycle intrapatient dose modification . 
 for example , a new developmental drug may be considered as an additional treatment in chemotherapy that includes other standard drugs over multiple cycles . our work was motivated by and applied to such a trial at the university of chicago for a rare form of leukemia . 
in this trial , a janus kinase inhibitor , ruxolitinib , was added to a three cycle us food and drug administration ( fda ) approved chemotherapy backbone that includes cycle - specific drugs ( table 1 )  . 
scheme of the dose - cycle finding clinical trial induction ( course 1 ) four - drug bfmbased regimen consolidation ( course 2 ) cyclophosphamide vincristine dexamethasome pegylated asparaginase cytarabine mercaptopurine methotrexate ( it ) interim maintenance ( course 3 ) delayed intensification ( course 4 ) methotrexate ( iv ) vincristine pegylated asparaginase methotrexate ( it ) doxorubicin cyclophosphamide vincristine dexamethasome pegylated asparaginase cytarabine thioguanine methotrexate ( it ) maintenance ( course 5 ) vincristine dexamethasone mercaptopurine methotrexate ( po ) methotrexate ( it ) screening ruxolitinib ruxolitinib ruxolitinib 4 weeks 4 - week treatment , 4 - week washout 4 - week treatment , 4 - week washout 4 - week treatment , 4 - week washout monitoring 2 - 3 years note . 
the chemotherapy backbone is based on the c10403 regimen.7 ruxolitinib is added to courses 2 to 4 as a three - cycle treatment , with potentially varying doses across cycles . abbreviations : bfm , berlin - frankfurt - munster ; it , intrathecally ; iv , intravenously ; po , orally . dose - finding study , which aimed to identify the maximum tolerated sequence ( mts ) of ruxolitinib dose levels across three cycles . 
the mts is defined as the highest sequence of three doses at which the probability of toxicity per cycle ( tpc ) is no more than or close to a prespecified target response rate pt , given that the probability of toxicity at each cycle is also no more than or close to pt . 
three doses of ruxolitinib were considered for each of the three cycles ; therefore , there were a total of 27 possible dose - cycle combinations for three cycles of treatment . the complication of the trial was the intrapatient dose modifications over cycles . 
such approaches usually work well when the sample size of the trial is sufficiently large , as seen in the dynamic treatment regimen methods , 8 reinforcement learning , 9 and sequential multiple assignment randomized trials.10 these approaches aim to better reflect the intrinsically multistage , adaptive structure of medical decisions , in both trial design and analysis of the trial data . 
the first is lee et al , 17 who proposed an innovative phase i / ii design to adaptively and dynamically optimize a patients dose in each of two cycles of therapy based on the joint binary cycle - specific efficacy and toxicity outcomes . 
 begin treatment end of treatment cycle 1 cycle 2 cycle 3 patient enrollment ith cohort trial end mts selection first cohort dar - 1 select dose level ( cid : 143 ) treat cohort at di and collect data stop ? treat at stop ? exit trial dar - 2b treat at stop ? nth cohort exit trial patients without dlts dar - 2a patients with dlts patients without dlts patients with dlts patients without dlts patients with dlts dar - 2a dar - 2b dar - 2a dar - 2b treat at treat at treat at treat at exit trial fig 1 . 
basyc consists of decisions to determine the dose in each cycle for the enrolled patients and to select the maximum tolerated sequence ( mts ) when the trial is completed . 
in each cycle , the dose allocation rule ( dar ) selects the doses for treating patients , in which dar - 1 selects the dose for cycle 1 and dar - 2 selects the dose for subsequent cycles . 
dar - 2 is composed of two subcases : dar - 2a and dar - 2b , which are applied to the two subcohortspatients without dose - limiting toxicities ( dlts ) and patients with dlts , respectively . 
for example , a patient might exit the trial after one cycle of treatment ( potentially because of toxicity [ indicated by stop ] ) based on the dcr applied in cycle 1 . 
figure 1 illustrates the general scheme of the basyc design for the motivating trial with three doses and three cycles of treatment . dcr and dar the basic concept of the dcr is that if the probability of toxicity of the lowest dose in the next cycle is considered lower than the target rate pt , the cohort can move to the next cycle for additional treatment ( ie , the decision is a go )  . 
technical details of the dcr are given in the appendix . if the dcr is a go for a cohort , the cohort will enter the next cycle for additional treatment . 
first , the dar always assigns the first cohort patients at the lowest dose level in all the cycles of treatment , which is a default rule to ensure the safety of the lowest dose in all three cycles . 
in this case , dar - 1 follows the same decision rule as in the mtpi - 2 design.5 specifically , the dose level is decided based on the observed toxicity data from previously enrolled patients treated at the most recent dose in the first cycle . 
this ad hoc rule is needed to protect patient safety . the two subcohorts undergo the dcr and dar separately hereafter until all three cycles of treatment are completed or until they exit the trial . 
motivated by the mtpi - 2 design , 5 dose allocation is presented in the form of dose escalation , stay , or de - escalation to give the candidate dose level at the next cycle relevant to the dose level of the cycle we currently consider . 
 this table is applied to the dose at which the current cohort is treated and the dose at which the previous cohort is most recently treated in the next cycle . 
the two tables can be generated and predetermined before the trial starts for examination by physicians . in the dar , we used the mtpi - 2 design as the backbone for decision making . 
the default values of 1 and 2 are 0.05. dose - finding algorithm to begin a trial , the basyc design treats the first cohort of patients at the lowest dose level in all three cycles . 
then , after the toxicity outcomes from the first cycle are observed , the dcr decides whether the cohort will go to the next cycle , and the dar decides which dose level to use if the dcr decision is go . 
this process is repeated until all cohorts finish all cycles of treatment unless the trial is terminated early because of excessive toxicity ( safety rules are given in the appendix )  . 
as a default rule , the cohort at a given cycle must wait for the cohort at the next cycle to complete follow - up before it can enter the next cycle . we demonstrate in table 2 how the basyc design guides the motivating dose - cycle trial with three doses and three cycles . 
specifically , once the current cohort completes the first cycle of treatment with observed outcome data , the next cohort can be enrolled and assigned a dose level in the first cycle . 
for example , in table 2 , in week 24 , after cohort 3 completed the first - cycle treatment at dose level 2 , the next cohort ( cohort 4 ) was enrolled and treated at dose level 1 as its first - cycle therapy . 
each column number represents the number of patients treated , and each row number represents the number of patients experiencing toxicity , at a given dose where the decision is applied . 
 ( a ) go ( g ) / no - go ( ng ) decisions according to the dose continuous rule ( dcr ) , in which the letters in blue and red represent g and ng decisions , respectively . 
 ( b ) dose allocation decisions according to the dose allocation rule ( dar ) , in which the letters in blue , gold , green , and red represent dose escalation ( e ) , staying at the current dose ( s ) , dose de - escalation ( d ) , and dose de - escalation and exclusion ( du ) because of toxicity , respectively . 
this table is applied to the dose at which the current cohort is treated and the dose at which the previous cohort is treated in the next cycle . mts selection at the end of the trial , among all the candidate sequences of dose - cycle combinations , a sequence of three doses for three cycles would be selected as the mts . 
we provided the true toxicity probabilities of the three dose levels in the first cycle and assumed that the toxicity probability would increase by 10% per cycle at the same dose level . 
for each scenario , 10 , 000 simulated trials are conducted on computer . operating characteristics the simulation results for scenarios 1 to 6 are summarized in table 3 , with four sections per scenario . 
recall that the mts is defined as the highest sequence of three safe doses with the true probability of tpc ( calculated as the average of the three true toxicity probabilities corresponding to the three dose levels ) closest to pt and falling in the ei ( pt 1 , pt + 2 )  . 
if a scenario has no dose sequence falling in the ei , the highest sequence of three safe doses with the true probability of tpc less than pt is considered the true mts . 
no practical methods are available , and the two existing designs17 , 18 in the literature are either highly complex or tailored for specific trials . perhaps the most attractive feature of the basyc design is its simplicity and transparency , as shown in figure 2 . 
we can see that escalation and de - escalation will never happen if the true toxicity probability of a dose is located in the higher interval ( pt + 2 , 1 ) and the lower interval ( 0 , pt + 1 ) , respectively . in this report , we implemented basyc for a realworld trial with three dose levels for three cycles of treatment . 
for example , a total of 53 = 125 sequences are available for trials with five dose levels and three cycles . basyc uses independent beta / binomial models as the working model to estimate the toxicity probability of each dose in each cycle based on all patients data at that dose / cycle . 
 alternatively , one could consider a dependent model , such as the markov model in fernandes et al , 18 to estimate the toxicity probabilities . in basyc , we focused on the dose - cycle trials with binary outcomes . 
with larger sample sizes , one can adopt dose - insertion methods23 , 24 to allow insertion of new doses when necessary . an mts with fixed dose levels at the end of the trial . 
for example , one may not allow a higher dose level than that in mts for any cycle of the treatment in the policy . lastly , a formal personalized dosing policy would follow the spirit of lee et al17 and use model - based inference on multiple cycles . 
stock w , luger sm , advani as , et al : favorable outcomes for older adolescents and young adults ( aya ) with acute lymphoblastic leukemia ( all ) : early results of us intergroup trial c10403 . 
doussau a , asselain b , le deley mc , et al : dose - finding designs in pediatric phase i clinical trials : comparison by simulations in a realistic timeline framework . 
doussau a , thibaut r , paoletti x : dose - finding design using mixed - effect proportional odds model for longitudinal graded toxicity data in phase i oncology clinical trials . 
guo w , ni y , ji y : teams : toxicityand efficacy - based dose insertion design with adaptive model selection for phase i / ii dose - escalation trials in oncology . 
 appendix notation suppose under consideration is a total of i candidate dose levels and j treatment cycles , indexed by i = 1 , 2 , , i ; j = 1 , 2 , , j . 
let k index the cohort , k = 1 , 2 , , k , where k is the maximum number of cohorts that will be recruited to the trial . during dose - cycle finding ( not for maximum tolerated sequence [ mts ] selection ) , we use simple and independent beta priors across doses and cycles and an independent binomial likelihood as a working model for the estimation of pij . 
the application in bayesian adaptive dose - cycle finding ( basyc ) is detailed here . dose continuation rule for cohort k that has been treated at dose i in cycle j , the dose continuation rule ( dcr ) for cohort continuation ( whether the cohort can continue treatment at cycle ( j + 1 ) ) is described as follows : if cohort k has finished the last cycle of therapy ( ie , j = j ) , cohort k exits the trial . if cohort k has not finished all cycles of therapy ( ie , j < j ) , and if pr { p1 , j + 1 > pt|data } > , where is a prespecified cutoff probability and often set to be close to 1 ( eg , = 0.95 ) , stop cohort k for any additional treatment , and patients in cohort k exit the trial . 
 otherwise , continue this cohort k to the next cycle ( j + 1 )  . this algorithm states that when the probability that toxicity of the lowest dose level ( dose level 1 ) in cycle ( j + 1 ) is higher than the target pt does not exceed a large value , cohort continuation is allowed . 
let x1 , j + 1 and n1 , j + 1 be the cumulative number of patients ( across all the previous and current cohorts ) with dose - limiting toxicity ( dlt ) events and treated at dose level 1 at cycle ( j + 1 ) , respectively . 
this beta distribution is used to calculate the posterior probability . dose allocation rule if cohort k in cycle j can proceed to the next cycle , the dose assigned to the next cycle ( j + 1 ) is dependent on the cumulative data from both the current cycle j and the next cycle ( j + 1 )  . 
such data accumulate all the toxicity outcomes from previously treated cohorts at this dose . then , consider a cohort of patients that has just completed treatment in the first cycle at a dose level . 
 here , the previous cohort refers to the cohort of patients enrolled just before the current cohort , and the toxicity data or the data ( also hereinafter ) refer to the data from all enrolled patients treated at the corresponding dose . 
specifically , given data1 and dose1 , the mtpi - 2 design will output a candidate dose level i1 , and given data2 and dose2 , mtpi - 2 will output another candidate dose i2 . 
specifically , given the dose ( dose1 ) in cycle 1 and the candidate dose i2 that mtpi - 2 gives based on data2 and dose2 from cycle 2 , dar - 2b selects the dose i = min { max { dose1 1 , 1 } , i2 } , the minimum of the dose 1 level lower than the current dose in cycle 1 , and i2 as the final dose for treating the cohort in cycle 2 . note that because of the cohort split , the previously enrolled subcohorts may have been treated in cycle 2 at two dose levels , say dose21 and dose22 . 
the outcome data from both subcohorts , denoted as data21 and data22 , will be used to inform the cycle 2 dose for the subsequent cohort that will start from the first cycle . 
in particular , for each of the data21 and data22 , the mtpi - 2 design will give two candidate doses i21 and i22 as the potential dose for the subsequent cohort in cycle 2 . 
then , the minimum of i21 and i22 will be provided as the candidate dose , denoted as i2 = min { i21 , i22 } , for the subsequent cohort as the cycle 2 candidate dose . 
the same principle is applied to decide the dose level in cycle 3 if needed . walkthrough of the hypothetic trial table 2 summarizes how the basyc design guides the motivating dose - cycle trial with three doses and three cycles . 
at this point , cohort 2 is enrolled and assigned to the next higher dose , dose 2 ( d2 ) , according to the dar decision , because cohort 1 has not exhibited any toxicity . 
at week 16 , cohort 1 completes treatment at d1 in cycle 2 with 0 toxicity outcome , and cohort 2 completes treatment at d2 in cycle 1 with 1 dlt outcome . 
the single patient with dlt , patient 4 , is de - escalated to d1 , and the remaining two patients without dlts , patients 5 and 6 , stay at d2 . 
this process continues for subsequent cohorts and cycles at weeks 24 , 32 , and so on , until all 15 patients ( or five cohorts ) have completed treatment at week 56 . safety rule applied in basyc for safety , the basyc design applies two additional safety rules throughout the entire trial : rule 1 ( early termination ) : for any cycle , if the toxicity probability of the lowest dose is higher than the target pt with a large probabilitythat is , if j * { 1 , 2 , , j } such that pr { p1j * > pt|data } > , where is close to 1 ( say = = 0.95 ) terminate the trial early . rule 2 ( dose exclusion ) : if the toxicity probability of dose i in cycle j is higher than the target pt with a large probability , pr { pij > pt|data } > , exclude doses i and the higher doses from cycle j and higher cyclesthat is , doses { i , i + 1 , , i } will never be used in the trial in cycles { j , j + 1 , , j } again . the posterior probabilities in both rules are calculated based on the simple beta / binomial calculation proposed in the mtpi design.3 details are provided in appendix under dose continuation rule . mts definition and selection after the enrollment and dose - cycle finding are completed , in the mts selection , we use a frequentist and nonparametric probability model to make inference . 
specifically , we essentially want to estimate the toxicity per cycle ( tpc ) qs , which is the average of the three toxicities of the doses in a sequence s ( described under definition of mts )  . 
we then construct an unbiased estimate of tpc qs ( described under estimation of qs ) and order - transform them based on isotonic regression ( described under mts selection )  . 
for each sequence s , we define the cumulative dose level as the sum of the dose levels across three cycles ( ie , d * s = ds1 + ds2 + ds3 )  . 
for each sequence s , denote pdsj , j the probability of toxicity for the dose in cycle j of sequence s , j = 1 , 2 , 3 . 
a sequence s is unacceptable if the toxicity probability of each dose in each cycle is higher than pt with a large probability , defined as j = 1 , 2 , 3 , pr { pdsj , j > pt|data } > , where dsj denotes dose levels { 1 , 2 , 3 } and is close to 1 , say = 0.95. 
the posterior probability pr { pdsj , j > pt|data } is based on a simple beta / binomial hierarchic model , similar to the calculation under dose continuation rule . 
 among all the safe sequences that satisfy the condition above , we want to select the highest sequence with overall qs close to pt , subject to the toxicity probability of the same dose level nondecreasing across cycles . 
however , the problem with that approach is that because of random chance , a sequence with a higher order ( and therefore higher toxicity ) might have a smaller qs than a lower - ordered sequence . 
for example , it is possible that the toxicity data for sequence 1 , 1 , 1 include only one toxicity event in all three cycles , whereas the data for sequence 2 , 1 , 1 include no toxicity event . 
however , sequence 2 , 1 , 1 is in theory a more toxic sequence , because it uses dose level 2 in cycle 2 instead of dose level 1 . 
therefore , selecting the sequence based on the distance of |qs pt| is not valid , because we would select 1 , 1 , 1 as the mts , not 2 , 1 , 1 in this case . to address this issue , we propose an isotonic transformation and calculate transformed qs values using the pool adjacent violator algorithm ( pava ) 20 just like in the mtpi design3 , 4 and mtpi - 2 design.5 here , we still use the sequence - specific data for the isotonic transformation . 
when there is a tie between m sequences , there are m ! possible simple orderings among thethen , assuming with probability 1 / m ! that one of the orderings , say ordering w , is true , we apply pava to the following ordering w of qs , w = 1 , 2 , , m !  . 
then , finally , the sequence dl * * that has nonincreasing dose levels across three cycles and the largest frequency f l * is selected as the estimated mts . 
therefore , the dose levels of the mts cannot be increasing , or else the lower dose in the early cycle can always be replaced by the higher dose in the later cycle . 
these results show that basyc is strong in protecting patient safety . scenario 2 presents a similar pattern of dose - toxicity relationship to scenario 1 , except that the toxicity probability of dose level 2 is now below pt = 30% . 
this suggests that the basyc design is nimble and can reach high dose - cycle combinations even with small sample sizes . scenario 4 presents an opposite case to scenario 3 , because all the doses are overly toxic with toxicity probabilities above pt . 
this scenario demonstrates the ability of the basyc design to stop the trial quickly in case of excessive toxicity in all dose sequences . scenarios 5 and 6 reflect situations where there is a leap in toxicity probabilities across the three doses . 
 acquired met exon 14 alteration drives secondary resistance to epidermal growth factor receptor tyrosine kinase inhibitor in egfr - mutated lung cancer ken suzawa , md , phd1 ; michael ofn , md1 ; adam j . 
in this study , we used targeted ngs with memorial sloan kettering integrated mutation proling of actionable cancer targets ( msk - impact ) , 12 immunohistochemistry , cell - free dna testing , and uorescence in situ hybridization to evaluate acquired resistance mediated by metex14 . 
furthermore , we used in vitro functional studies to establish metex14 as a novel mechanism of acquired resistance to egfr tkis . we used msk - impact , a large - panel ngs assay , to detect mutations , copy - number alterations , and select gene fusions involving up to 468 cancer - associated genes.12 metex14 was introduced into pc9 and h1975 cells as follows . 
briey , full - length metex14 was polymerase chain reaction amplied and subcloned into plenti - cmv - blast lentiviral vector ( plasmid 17451 ; addgene , cambridge , ma )  . 
the patient restarted erlotinib ( 100 mg daily ) with clinical and radiologic response for 12.5 months , at which time computed tomography revealed an increase in the dominant right upper lobe mass . 
 ( b - d ) representative images showing ( b ) baseline scan ( at time of progression during osimertinib monotherapy ) , ( c ) response to crizotinib monotherapy , and ( d ) response to combined crizotinib and osimertinib therapy . 
 ( * ) the patient initially received 1.4 months of combination osimertinib and savolitinib in a clinical trial , but treatment was changed to monotherapy with osimertinib because of intolerable toxicity . 
 ( ) as of 10 months of ongoing treatment with osimertinib and crizotinib . l858r mutation , no evidence of egfr t790m , and a new metex14 ( c.2899g.a ) alteration and met amplication ( fold change , 2.5 ; fig 1a ; appendix table a1 )  . 
therapy was changed to osimertinib with savolitinib daily ( clinicaltrials . gov identier : nct02143466 ) for 1.4 months , after which savolitinib was stopped because of toxicity and single - agent osimertinib 80 mg daily was continued . 
the patient continued to receive combination therapy with durable clinical and radiographic benet for more than 9 months . to dene the role of metex14 in mediating resistance to egfr tkis , we generated two isogenic egfr - mutant nonsmall - cell lung cancer ( nsclc ) cell models using pc9 ( exon 19 deletion ) and h1975 cells ( l858r and t790m ) by transduction with lentiviral vectors driving expression of metex14 ( fig 2a )  . 
western blot analysis showed that phosphorylation of egfr and its downstream effectors akt and erk was inhibited by osimertinib in pc9 cells transduced with empty plasmids ( pc9 empty ) , but phosphorylation of egfr , metex14 , and downstream effectors remained unaffected by osimertinib treatment in pc9 metex14 cells ( fig 2b )  . 
each condition was assayed in triplicate determinations ; data were normalized for cell number by measuring cell viability and shown relative to the control group ( mean 6 standard deviation )  . 
combination treatment with epidermal growth factor receptor ( egfr ) and met inhibitors is effective against met exon 14 skipping alteration ( metex14 ) induced drug resistance in egfr - mutant nonsmall - cell lung cancer cells . 
 ( c ) cells were treated with osimertinib ( 1 mm ) , crizotinib ( 1 mm ) , or a combination of the two agents for 3 hours , and lysates were subjected to immunoblotting . 
 ( e ) caspase 3 / 7 activity was analyzed in pc9 metex14 cells that were treated with osimertinib ( 1 mm ) , crizotinib ( 200 nm ) , or a combination of osimertinib ( 1 mm ) and crizotinib ( 200 nm ) for 48 hours . 
each condition was assayed in triplicate determinations , and data were normalized for cell number by measuring cell viability and are shown relative to the control group ( mean 6 standard deviation )  . 
pc9 metex14 cells showed a reduction in osimertinib - induced caspase 3 / 7 activation compared with pc9 - empty cells ( p , .001 ; fig 2d )  . 
together , these results indicate that metex14 induces resistance to osimertinib in egfr - mutant nsclc cells . investigated whether metex14 - mediated rewe next sistance to egfr tkis could be overcome by combination therapy with egfr and met inhibitors . 
as expected , crizotinib inhibited metex14 phosphorylation in pc9 metex14 cells ; however , phosphorylation of egfr , akt , and erk remained largely unchanged ( fig 3a ) , suggesting that egfr is still signaling effectively in pc9 metex14 cells . similarly , crizotinib was ineffective at modulating growth of egfr - mutated cell lines , with or without metex14 expression ( fig 3b )  . 
in agreement with these results , inhibition of egfr and met caused signicantly dual higher activation of caspase 3 / 7 ( fig 3e )  . discussion our study highlights the importance of serial and diverse molecular analyses , including ngs , to evaluate acquired alterations in the post - tki setting . 
although the patient did not respond to met - targeted therapy alone , the patient continued to have a durable clinical response to combination osimertinib and crizotinib , with stable disease by recist criteria and without notable toxicity . 
crizotinib restored sensitivity to egfr tkis ; however , crizotinib alone was not enough to suppress growth . two previous reports have demonstrated co - occurrence of egfr and metex14 mutations . 
in the rst report , three ( 0.2% ) of 1 , 590 patients with nsclc harbored concomitant egfr and metex14 mutations , one of whom received combination treatment with met ( volitinib ) and egfrtargeted therapies ( getinib ) , yielding a partial response.16 the second report noted one patient case of sarcomatoid carcinoma with egfr and metex14 alterations.17 in our msk - impact testing experience of 866 patient cases of egfr - mutant lung adenocarcinomas ( as of october 15 , 2018 ) , only two patients showed this combination of alterations : the patient described here , with acquired resistance , and a patient separate primaries at diagnosis . in whom the alterations were present the clinical benet of the combination of metand egfrtargeted therapies in patients with nsclc with acquired met amplicationmediated resistance to egfr tkis has trials , with varying tolerability been explored in clinical dependent upon the agents being combined.18 our ndings provide a rationale for future clinical evaluation of this combination approach , given its tolerability and efcacy in this case , for patients with egfr and metex14 mutations . furthermore , given the recent reports of secondary - site mutations in the met kinase domain , such as d1228n / v and y1230c , as mechanisms of acquired resistance to crizotinib in patients with metex14 , 19 it is plausible that these secondary met mutations will also emerge as mechanisms of resistance to the combination of osimertinib and crizotinib . we found that expression of metex14 upregulated phosphorylation of egfr itself , presumably via crossphosphorylation , because met is known to interact with egfr and drive the activity of egfr , 20 which resulted in blunting of the inhibition of egfr phosphorylation by egfr tkis . 
yu , romel somwar , marc ladanyi data analysis and interpretation : ken suzawa , michael ofn , adam j . schoenfeld , igor odintsov , daniel lu , alexander drilon , helena a . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter michael ofn consulting or advisory role : pharmamar travel , accommodations , expenses : bristol - myers squibb , merck sharp & dohme maria e . 
rudin consulting or advisory role : bristol - myers squibb , abbvie , seattle genetics , harpoon therapeutics , genentech / roche , astrazeneca , ascentage pharma , bicycle therapeutics , celgene , daiichi sankyo , ipsen , loxo , pharmamar , elucida oncology , bridge medicines research funding : abbvie / stemcentrx ( inst ) , viralytics ( inst ) , merck ( inst ) , daiichi sankyo ( inst ) alexander drilon honoraria : medscape , onclive , peervoice , physicians education resources , targeted oncology , more health , research to practice , foundation medicine , peerview consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pzer , blueprint medicines , genentech / roche , helsinn therapeutics , beigene , hengrui therapeutics , exelixis , bayer healthcare pharmaceuticals , tyra biosciences , verastem , takeda / ariad / millennium pharmaceuticals , bergenbio , more health patents , royalties , other intellectual property : wolters kluwer ( royalties for pocket oncology ) other relationship : merck , glaxosmithkline , teva pharmaceuticals industries , taiho pharmaceutical helena a . 
yu consulting or advisory role : astrazeneca , eli lilly research funding : clovis oncology ( inst ) , astrazeneca ( inst ) , astellas pharma ( inst ) , eli lilly ( inst ) , novartis ( inst ) , pzer ( inst ) , daiichi sankyo ( inst ) travel , accommodations , expenses : eli lilly other relationship : astellas pharma gregory j . 
 acquired met exon 14 alteration and resistance to egfr tkis references yu ha , suzawa k , jordan e , et al : concurrent alterations in egfr - mutant lung cancers associated with resistance to egfr kinase inhibitors and characterization of mtor as a mediator of resistance . 
clin cancer res 24 : 3108 - 3118 , 2018 ofn m , somwar r , rekhtman n , et al : acquired alk and ret gene fusions as mechanisms of resistance to osimertinib in egfr - mutant lung cancers . 
jama oncol 4 : 1527 - 1534 , 2018 bean j , brennan c , shih jy , et al : met amplication occurs with or without t790m mutations in egfr mutant lung tumors with acquired resistance to getinib or erlotinib . 
proc natl acad sci usa 104 : 20932 - 20937 , 2007 onozato r , kosaka t , kuwano h , et al : activation of met by gene amplication or by splice mutations deleting the juxtamembrane domain in primary resected lung cancers . 
j thorac oncol 4 : 5 - 11 , 2009 kong - beltran m , seshagiri s , zha j , et al : somatic mutations lead to an oncogenic deletion of met in lung cancer . 
cancer res 66 : 283 - 289 , 2006 paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
cancer discov 5 : 842 - 849 , 2015 drilon ae , camidge dr , ou s - hi , et al : efcacy and safety of crizotinib in patients ( pts ) with advanced met exon 14 - altered non - small cell lung cancer ( nsclc )  . 34 , 2016 ( suppl ; abstr 108 ) drilon a , ou s - h , clark j , et al : antitumor activity and safety of crizotinib in patients with met exon 14 - altered advanced non - small cell lung cancer . 
felip e , horn l , patel jd , et al : tepotinib in patients with advanced non - small cell lung cancer ( nsclc ) harboring met exon 14 - skipping mutations : phase ii trial . 
wolf j , han j , nishio m , et al : geometry mono - 1 : phase ii , multicenter study of met inhibitor capmatinib ( inc280 ) in egfr wt , met - dysregulated advanced nsclc . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
pennell na , neal jw , chaft je , et al : select : a phase ii trial of adjuvant erlotinib in patients with resected epidermal growth factor receptormutant nonsmallcharacteristics . 
borsu l , intrieri j , thampi l , et al : clinical application of picodroplet digital pcr technology for rapid detection of egfr t790m in next - generation sequencing libraries and dna from limited tumor samples . 
ou si , govindan r , eaton kd , et al : phase i results from a study of crizotinib in combination with erlotinib in patients with advanced nonsquamous non - small cell lung cancer . 
in cohort b , the orr and disease control rate were 75% and 75% . conclusion capmatinib in combination with erlotinib demonstrated safety proles consistent with prior studies . we observed efcacy in specic patient populations . 
early studies evaluated onartuzumab ( an anti - met monoclonal antibody ) in combination the phase iii with erlotinib in recurrent nsclc.16 , 17 in the phase ii study , patients with met 2 + or 3 + by immunohistochemistry ( ihc ) demonstrated a signicant improvement in survival end points compared with low met expression . 
despite this , trial was negative.18 tivantinib , a non - atp competitive small molecule met inhibitor , was evaluated in combination with erlotinib in a phase ii trial of unselected pretreated patients . 
the combination did not meet its overall efcacy goal ; however , a planned subset analysis showed a trend toward prolonged progression - free survival ( pfs ) in patients with met amplication.19 this lack of efcacy may be due to the lack of specicity of tivantinib for the met pathway compared with other met inhibitors.20 capmatinib ( inc280 ) is a highly potent and selective oral met inhibitor that has recently been approved for the treatment of tumors with met exon 14 mutations.21 in the phase i study , antitumor activity was observed in pretreated patients with egfr wild - type ( wt ) tumors with met dysregulation . 
because of overlapping signaling pathways , we sought to determine whether the combination of capmatinib with erlotinib would be safe and demonstrate an efcacy signal in patients with egfror metaltered tumors . knowledge generated we demonstrated that the combination of capmatinib and erlotinib is safe . 
however , it restored sensitivity to erlotinib and promoted apoptosis in nsclc models rendered erlotinib resistant by hgf.23 on the basis of the data available during trial development , we propose that the combination of capmatinib plus erlotinib would be safe and show efcacy in patients with egfr - mutated tumors experiencing disease progression on erlotinib due to met activating bypass pathways . 
the initial phase of the study was a dose escalation to determine the maximum tolerated dose ( mtd ) of capmatinib plus erlotinib ; there was no intrapatient dose escalation . 
patients in cohort a must have an egfr activating mutation and a biopsy at the time of progression that shows evidence of met positivity . treatment capmatinib capsules were administered orally every 12 hours of a 28 - day cycle at 100 - 600 mg . 
a dose - limiting toxicity ( dlt ) was dened as per the study protocol ( data supplement )  . pk blood samples were collected for patients in the doseescalation cohort on cycle 1 , day 15 ; cycle 2 , days 1 and 15 ; and cycles 3 and 4 , day 1 . 
analysis of hgf levels was conducted in duplicate by enzyme - linked immunosorbent assay ( r&d systems , minneapolis , mn ; cat dhg00 ) as per the manufacturers instructions . statistical methods all patients who had at least one dose of study therapy were included in the analyses . 
twelve and ve patients were enrolled in cohorts a and b , respectively ( fig 1 )  . patient demographics and disease characteristics patient demographics and disease characteristics are listed in table 1 . 
in the doseescalation cohort and cohort a , 67% ( patients 1 and 313 ) and 92% ( all except patient 29 ) had prior treatment with at least one egfr tki . 
swimmers plot demonstrating the cohort , met , and epidermal growth factor receptor ( egfr ) status of each patient and corresponding response status and progression - free survival of each patient . 
patient 30 was found to have an egfr t790m mutation on a biopsy sample taken after egfr tyrosine kinase inhibitor ( tki ) treatment ; however , on immediate pretreatment biopsy this mutation was not detected . 
a waterfall plot of best response for all evaluable patients is shown in figure 3 . the aes that were possibly , probably , or denitely attributed to the study drugs are shown in table 2 for all dose levels . 
the most common aes of any grade were acneiform rash ( 62.9% ) , fatigue ( 51% ) , nausea ( 45.7% ) , diarrhea , lower extremity edema , vomiting , and hypoalbuminemia ( 37% each )  . 
in patients who received the recommended phase ii dose ( rp2d ) , the most common aes were acneiform rash ( 65% ) , fatigue and nausea ( both 60% ) , vomiting ( 55% ) , and hypoalbuminemia and edema ( both 50% ) ; additional aes are detailed in appendix table a1 . there were no grade 5 toxicities related to the drug combination . dlt and mtd in dose level 5 , one patient developed grade 3 neutropenia possibly related to treatment . 
dose level 6 served as the expansion of dose level 5 , given that 600 - mg capsules were previously shown to be pharmacokinetically equivalent to 400 - mg tablets . 
six patients received dose modications of capmatinib due to nausea ( 2 ) , alt abnormalities ( 1 ) , edema ( 1 ) , low neutrophil count ( 1 ) , and elevated amylase ( 1 )  . 
five patients received dose modications of erlotinib due to paronychia ( 2 ) , acneiform rash ( 1 ) , creatinine increase ( 1 ) , and diarrhea ( 1 )  . 
four patients received dose modications of both drugs for lipase elevation ( 1 ) , creatinine increase ( 1 ) , lymphopenia ( 1 ) , and lung inammation / pneumonitis ( 1 )  . the pk properties of erlotinib and capmatinib were examined during dose escalation on cycle 1 , day 15 at multiple time points after drug administration . 
the same 400mg dose of capmatinib in the tablet formulation demonstrates a higher drug exposure with greater variation ( appendix table a2 ) compared with the capsule formulation , 182 2021 by american society of clinical oncology although it was not statistically signicant . in addition , erlotinib showed a dose - dependent change of systemic drug exposure ( 150 mg v 100 mg ; appendix fig a1b and appendix table a2 ) ; coadministration with capmatinib did not have signicant impact on erlotinib pk ( appendix table a2 )  . 
overall , the range of erlotinib exposures during dose escalation was similar to previously published results.28 efcacy across all evaluable patients , the orr was 31% ( 8 / 26 ; fig 3 )  . 
among patients with pr or cr , the responses were prolonged , from patient 24 , who discontinued study after apart 3 months because of pneumonia / pneumonitis ; vestigators could not rule out possible drug - related pneumonitis , and thus the patient was discontinued from study . two responders were treatment nave ( 20 and 24 ) ; the remainder had at least one prior regimen ( table 1 )  . dose - escalation cohort fifteen of the 18 patients in the dose - escalation cohort were evaluable . 
two patients ( patients 21 and 23 ) withdrew from the study by individual choice , one patient ( patient 33 ) developed new brain metastasis and withdrew , and one patient ( patient 30 ) had a prolonged hospitalization for a cerebrovascular event deemed unrelated to study drugs . 
efcacy data across dose - escalation cohort dose level median cycles ( range ) 2 ( 2 - 4 ) 5 ( 4 - 16 ) 2 ( 1 - 7 ) 2 ( 2 - 8 ) 4 ( 1 - 10 ) 4 ( 4 - 29 ) inc280 , mg twice a day erlotinib , mg once daily evaluable patients complete response partial response stable disease progressive disease overall response rate abbreviation : inc280 , capmatinib . 1 ( 33% ) 3 ( 100% ) disease control rate 2 ( 67% ) 2 ( 67% ) 1 ( 33% ) 2 ( 67% ) 1 ( 33% ) five egfr - wt patients were enrolled in cohort b ; one patient ( patient 25 ) was not evaluable because of death during cycle 1 deemed unrelated to the study drugs . 
efcacy data across dose - expansion cohorts dosing and response groups cohort a median cycles ( range ) 2 ( 1 - 33 ) 3 ( 1 - 45 ) inc280 , mg twice daily erlotinib , mg once daily evaluable patients complete response partial response stable disease progressive disease overall response rate , % disease control rate , % cohort b abbreviations : inc280 , capmatinib ; ne , not evaluable . at the recommended phase ii dosing , responses were seen in patients with met amplication by ngs and / or 3 + ihc expression and those with met exon 14 mutations , but not in patients with 2 + ihc expression . 
a study in chinese patients with getinib plus capmatinib also reported that 2 + ihc expression was not predictive of response unless it was accompanied by a gene copy number of 5.29 the met / cen7 ratios were not fully reported in this study , but a ratio  . 
serial blood hgf levels were measured to evaluate baseline levels and treatment - related changes in patients over time ; however , no overt correlations with baseline hgf levels and treatment outcomes were observed ( data not shown )  . the patient population with the greatest potential to benet from the combination treatment was cohort a , which enrolled egfr - positive patients who had experienced progression on egfr tkis . 
additional evaluation of an egfr - tki plus a met - tki to overcome this common resistance mechanism is warranted . affiliations 1helen diller family comprehensive cancer center , university of california , san francisco , ca 2university of california davis comprehensive cancer center , sacramento , ca 3mount sinai tisch cancer institute , new york , ny subject matter of this manuscript . 
mccoach honoraria : novartis , genentech , guardant health consulting or advisory role : astrazeneca speakers bureau : novartis research funding : novartis , revolution medicine travel , accommodations , expenses : loxo , eli lilly , takeda pharmaceuticals aiming yu stock and other ownership interests : johnson & johnson patents , royalties , other intellectual property : patents : ( 1 ) yu am , wang wp , chen qx , li mm . 
gandara honoraria : astrazeneca consulting or advisory role : astrazeneca ( i ) , guardant health ( i ) , oncocyte ( i ) , amgen , io biotech ( i ) , merck , roche / genentech , boehringer ingelheim , inivata , novartis research funding : roche / genentech ( i ) , merck ( i ) , amgen ( i ) travel , accommodations , expenses : boehringer ingelheim jonathan w . 
lara consulting or advisory role : janssen research funding : aragon pharmaceuticals ( i ) , janssen biotech ( i ) , tracon pharma ( i ) , merck ( i ) , pharmacyclics ( i ) , incyte ( i ) , taiho pharmaceutical ( i ) matthew gubens consulting or advisory role : bristol myers squibb , roche / genentech , astrazeneca , heron , boehringer ingelheim , takeda pharmaceuticals , beyondspring pharmaceuticals , inivata research funding : celgene ( i ) , merck ( i ) , novartis ( i ) , roche / genentech ( i ) , oncomed ( i ) philip c . 
mack honoraria : guardant health consulting or advisory role : astrazeneca , guardant health , amgen research funding : boehringer ingelheim consulting or advisory role : roche / genentech , regeneron , abbvie , emd serono , merck , pzer , astrazeneca , novartis , symphogen , inivata , bristol myers squibb , takeda pharmaceuticals , eli lilly , amgen , genmab , targeted oncology , genentech research funding : emd serono ( i ) , genentech ( i ) , abbvie ( i ) , five prime therapeutics ( i ) , regeneron ( i ) , astellas pharma ( i ) , tizona therapeutics , ( i ) eli lilly ( i ) , novartis ( i ) , amgen ( i ) patents , royalties , other intellectual property : author royalties for uptodate , an evidence - based , peer - reviewed information resource , available via the web , desktop , and pda travel , accommodations , expenses : astrazeneca , roche / genentech , merck , regeneron , eli lilly , abbvie , emd serono no potential conicts of interest were reported . acknowledgment we thank patients and their families for participation in this study . karen kelly honoraria : merck references finocchiaro g , toschi l , gianoncelli l , et al : prognostic and predictive value of met deregulation in non - small cell lung cancer . 
ann transl med 3 : 83 , 2015 go h , jeon yk , park hj , et al : high met gene copy number leads to shorter survival in patients with non - small cell lung cancer . 
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science 316 : 1039 - 1043 , 2007 bean j , brennan c , shih jy , et al : met amplication occurs with or without t790m mutations in egfr mutant lung tumors with acquired resistance to getinib or erlotinib . 
proc natl acad sci usa 104 : 20932 - 20937 , 2007 cappuzzo f , j anne pa , skokan m , et al : met increased gene copy number and primary resistance to getinib therapy in non - small - cell lung cancer patients . ann oncol 20 : 298 - 304 , 2009 piotrowska z , thress ks , mooradian m , et al : met amplication ( amp ) as a resistance mechanism to osimertinib . 
le x , puri s , negrao mv , et al : landscape of egfr - dependent and - independent resistance mechanisms to osimertinib and continuation therapy beyond progression in egfr - mutant nsclc . 
drilon a , cappuzzo f , ou si , et al : targeting met in lung cancer : will expectations nally be met ? j thorac oncol 12 : 15 - 26 , 2017 15 . 
spigel dr , ervin tj , ramlau ra , et al : randomized phase ii trial of onartuzumab in combination with erlotinib in patients with advanced non - small - cell lung 18 . 
spigel dr , edelman mj , obyrne k , et al : results from the phase iii randomized trial of onartuzumab plus erlotinib versus erlotinib in previously treated stage iiib or iv non - small - cell lung cancer : metlung . 
sequist lv , von pawel j , garmey eg , et al : randomized phase ii study of erlotinib plus tivantinib versus erlotinib plus placebo in previously treated non - smallcell lung cancer . 
calles a , kwiatkowski n , cammarata bk , et al : tivantinib ( arq 197 ) efcacy is independent of met inhibition in non - small - cell lung cancer cell lines . 
liu x , wang q , yang g , et al : a novel kinase inhibitor , incb28060 , blocks c - met - dependent signaling , neoplastic activities , and cross - talk with egfr and her22 . 
bang y - j , su w - c , nam d - h , et al : phase i study of the safety and efcacy of inc280 in patients with advanced met - dependent solid tumors . 
lara ms , holland ws , chinn d , et al : preclinical evaluation of met inhibitor inc - 280 with or without the epidermal growth factor receptor inhibitor erlotinib in non - small - cell lung cancer . 
paik pk , drilon a , fan pd , et al : correction : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
cancer discov 5 : 842 - 849 , 2015 jorge se , schulman s , freed ja , et al : responses to the multitargeted met / alk / ros1 inhibitor crizotinib and co - occurring mutations in lung adenocarcinomas with met amplication or met exon 14 skipping mutation . 
fukudo m , ikemi y , togashi y , et al : population pharmacokinetics / pharmacodynamics of erlotinib and pharmacogenomic analysis of plasma and cerebrospinal uid drug concentrations in japanese patients with non - small cell lung cancer . 
wu yl , zhang l , kim dw , et al : phase ib / ii study of capmatinib ( inc280 ) plus getinib after failure of epidermal growth factor receptor ( egfr ) inhibitor therapy in patients with egfr - mutated , met factor - dysregulated non - small - cell lung cancer . 
wolf j , overbeck tr , han j , et al : capmatinib in patients with high - level met - amplied advanced nonsmall cell lung cancer ( nsclc ) : results from the phase 2 geometry mono - 1 study . 
camidge dr , otterson ga , clark jw , et al : crizotinib in patients ( pts ) with met - amplied non - small cell lung cancer ( nsclc ) : updated safety and efcacy ndings from a phase 1 trial . 
caparica r , yen ct , coudry r , et al : responses to crizotinib can occur in high - level met - amplied non - small cell lung cancer independent of met exon 14 33 . 
wolf j , seto t , han j , et al : results of the geometry mono - 1 phase ii study for evaluation of the met inhibitor capmatinib ( inc280 ) in patients with metex14 mutated advanced non - small cell lung cancer . 
yu h , ahn m , kim s , et al : ct032 tatton phase ib expansion cohort : osimertinib plus savolitinib for patients ( pts ) with egfr - mutant , met - amplied nsclc after progression on prior rst / second - generation epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitor ( tki )  . 
sequist l , lee js , han j , et al : ct033 tatton phase ib expansion cohort : osimertinib plus savolitinib for patients ( pts ) with egfr - mutant , met - amplied nsclc after progression on prior third - generation epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitor ( tki )  . 
treatment - related adverse events by cohort and dose level ( continued ) dose level 1 dose level 2 dose level 3 dose level 4 dose level 5 dose level 6 expansion adverse event gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 total gastroesophageal reux disease oral mucositis hyponatremia stroke proteinuria back pain peripheral sensory neuropathy abbreviations : gr , grade ; inr , international normalized ratio ; sae , signicant adverse event . 
 response of a metastatic breast carcinoma with a previously uncharacterized erbb2 g776v mutation to human epidermal growth factor receptor 2targeted therapy introduction we present a case of a patient with advanced estrogen receptor / progesterone receptorpositive , her2 - negative ( by fluorescent in situ hybridization ) breast cancer , refractory to estrogen receptortargeted therapy . 
in vitro experiments showed that erbb2 g776v is an oncogenic driver , and further largescale analysis of genomic profiles of breast carcinomas suggested the existence of a distinct subtype of her2 - negative breast cancer driven by a combination of activating erbb2 kinase domain mutations and inactivating map3k1 alterations . 
these observations suggest that patients with breast cancer who have relapsed / refractory disease can benefit from cancer genomic profiling to identify unanticipated opportunities for targeted therapy , including the use of combinatorial therapies with anti - her2 agents for those cases with erbb2 mutations . management of estrogen receptor ( er ) / progesterone receptor ( pr ) - positive breast cancer refractory to endocrine therapy presents a clinical challenge , although recent studies demonstrating the acquisition of esr1 mutations1 - 5 or alterations in the pi3k / mtor pathway6 - 8 have identified mechanisms of such resistance . 
in addition , unlike the breast cancer described in this case report , where the tumor was her2 negative , a small subset of er - positive breast cancers are also her2 positive and have been dubbed triple - positive cases ; in the absence of her2 - targeted therapy , these have a poor prognosis and worse response to endocrine therapy relative to er - positive breast cancers in general , 9 - 11 but they have been reported to respond to anti - her2 agents.11 , 12 recently , several lines of investigation have demonstrated that mutations in the her2 gene ( erbb2 ) are oncogenic drivers in breast carcinoma , as evidenced by patient responses to her2 - targeted therapy . 
erbb2 mutations such as s310f , l755s , v777l , and l869q have been shown to be strong drivers associated with clinical sensitivity to her2 - targeted agents.13 - 16 in addition , erbb2 mutations have been reported to be prevalent in invasive lobular breast carcinoma , which is typically er / pr positive , her2 negative , and cdh1 mutant.17 - 19 we report on a patient with advanced breast cancer harboring a previously uncharacterized erbb2 g776v variant , who derived clinical benefit from treatment with trastuzumab plus pertuzumab ( tp ) regimens . 
furthermore , breast carcinomas with erbb2 kinase domain ( kd ) mutations are marked by cosegregation with map3k1 alterations , and the majority of breast cancer cases with the g776v mutation are er positive , which are not general features of her2 - positive or erbb2 - mutant breast cancer and , thus , may denote a distinct class of breast carcinoma driven by erbb2 kd alterations . methods comprehensive genomic profiling dna was extracted from 40 microns of formalinfixed paraffin - embedded sections , and comprehensive yakov chudnovsky runjun d . 
 genomic profiling was performed in a clinical laboratory improvement amendments certified , college of american pathologistsaccredited reference laboratory ( foundation medicine ) on hybridization - captured , adaptor ligationbased libraries to a mean coverage depth of  . 
the construct was then shuttled into the pcfg5 retroviral vector ( which includes a zeocyn resistance marker and ires - gfp sequence ) using the in - fusion hd cloning system kit ( clonetech laboratories , mountain view , ca ) , and verified using sanger sequencing . retroviral particles were produced using fnx amphotrophic packaging cells . 
cells were selected under 10 mg / ml zeocin for 3 weeks . agar colony - formation assays , wells were seeded with 7 , 000 cells and grown for 2 weeks before imaging . 
codons 23652 were defined as the extracellular domain ( ecd ) , and codons 720987 were defined as the kd.22 the p value was calculated using logistic regression , and p values were corrected for multiple testing using the falsediscovery rate23 method to generate q values . the odds ratio ( or ) for each variant type is calculated from the logistic regression coefficient ; an or  . 
1.0 indicates more frequent co - occurrence than expected by chance , whereas an pr , 1.0 indicates less frequent co - occurrence than expected by chance . results case description for western blots , cells were serum starved for 6 hours before lysate harvesting . 
lysates were probed using the following antibodies : her2 ( monoclonal , ab - 17 ) from thermo fisher scientific ( waltham , ma ) , phospho - her2 ( py1248 ) from emd millipore ( billerica , ma ) , p44 / 42 mapk and phospho p44 / 42 mapk from cell signaling technologies ( danvers , ma )  . 
in july 2003 , the patient presented with a t2 n0 m0 , er - positive , pr - positive , her2negative ( nonamplified by fluorescent in situ hybridization , 2 + by immunohistochemistry ) invasive ductal carcinoma of the left breast . 
in december 2005 , she developed metastasis to the sternum and lung , and was initially treated with ovarian suppression and zoledronate . she received radiation therapy to the sternal lesions in december 2008 and again in may 2012 . 
additional antiestrogen therapies used included letrozole ( january 2009 to january 2011 and again from february 2012 to may 2013 ) and fulvestrant ( february 2011 to january 2012 )  . in early 2013 , positron emission tomographycomputed tomography ( pet - ct ) scans showed increasing activity in the lung lesions , and the patient underwent a video - assisted thoracoscopic surgery procedure in may 2013 . 
the ca15 - 3 tumor marker level decreased with capecitabine ( down from 391 to 85 u / ml , but then rising to 213 u / ml ) and also with estradiol ( decreasing further to 74 u / ml , but then rising to 132 u / ml ; fig 1 )  . 
trastuzumab , pertuzumab , and exemestane were started in october to november 2014 , and the patient responded well to this , with marked improvement on pet - ct scan and decrease in ca15 - 3 level to 43 u / ml . 
however , by february 2015 , the ca15 - 3 level rose to 58 u / ml and the patients treatment was changed to nabpaclitaxel , trastuzumab , and pertuzumab . 
the ca15 - 3 level decreased to a nadir of 31 u / ml ( normal range for ca15 - 3 is 0 to 31 u / ml ) , the pet - ct scan showed no areas of increased uptake , and the patient remained on this regimen for a total of seven cycles . 
in december 2015 , pet - ct showed new uptake in her lung nodules , and the patient enrolled in an unrelated clinical trial . preclinical characterization of her2 ( erbb2 ) g776v the her2 g776v mutant was stably overexpressed in nih 3t3 cells by retroviral transduction . capecitabine estradiol trastuzumab pertuzumab exemestane nabpaclitaxel trastuzumab pertuzumab maintanence trastuzumab date ascopubs.org / journal / po jco precision oncology 3 fig 1 . 
immunoblotting showed that these cell lines expressed elevated levels of active phosphorylated mapk ( similar to cells expressing her2 v777l ) , but nonelevated levels of phosphorylated her2 , which may be an artifact of the overexpression system ( fig 2a )  . 
we also assayed these cell lines for colony formation in soft agar . we found that cells expressing her2 g776v formed colonies at a rate similar to that of the her2 v777l mutant ( figs 2b and 2c )  . 
together , these results suggest that g776v is an activating mutation , causing increased signaling through the her2 / mapk pathway and allowing for anchorage - independent growth of nih 3t3 cells . genomic co - occurrence of map3k1 alterations with erbb2 alterations among the 10 , 790 breast carcinoma cases that have undergone cgp in our laboratory , 1 , 329 ( 12.3% ) have been found to harbor alterations in erbb2 , including 1 , 041 cases ( 9.6% ) with erbb2 amplification , 229 cases ( 2.1% ) with erbb2 short variants ( substitutions or inframe insertions or deletions ) , and 59 ( 0.5% ) with both ( table 1 )  . 
to identify additional genomic variants that may cooperate with erbb2 mutations in the pathogenesis of her2 - negative breast cancer , we calculated the co - occurrence of alterations in each of 345 genes profiled at foundation medicine with various alterations in erbb2 ( data supplement )  . 
as discussed , cdh1 alterations have been reported to co - occur with erbb2 mutations in the context of invasive lobular breast carcinoma.17 - 19 tbx3 has also been reported to be enriched for mutations in lobular breast carcinoma , 25 as well in neuroendocrine breast cancer , 26 but its role in breast cancer is not entirely clear : it has been suggested to be a tumor suppressor27 , 28 and an oncogene29 , 30 in different studies . 
we chose to further examine the tumor suppressor gene map3k1 , which was mutated in the patient described in this case report . alterations in map3k1 co - occur with erbb2 short variants significantly more frequently than expected by chance in breast cancer cases profiled in our laboratory , but erbb2 alterations , in general , are not significantly enriched for cooccurrence with map3k1 variants ( table 1 )  . furthermore , although activating mutations in erbb2 are found in both the ecd and the kd , 21 only kd mutations , and not ecd mutations , are significantly enriched for co - occurrence with map3k1 alterations ( table 1 )  . 
map3k1 alterations have been identified in 513 ( 4.8% ) of the 10 , 790 breast carcinoma cases profiled at foundation medicine and at a similar frequency range of 0% to 8% of breast cancers in several large - scale sequencing studies.27 , 31 - 33 map3k1 inactivation via mutation or copy number loss has been reported to be particularly prevalent in the luminal a subtype of breast cancer , which is distinct from the subtype that is characterized by erbb2 amplification.33 , 34 consistent with this , among the breast carcinoma cases profiled using our hybrid capture based assay , erbb2 copy number alterations co - occur with map3k1 variants significantly less frequently than expected by chance ( table 1 )  . 
notably , although subtype data were not available for the breast cancer cases profiled in our laboratory , logistic regression g776va v777l her2 wt parental ascopubs.org / journal / po jco precision oncology fig 2 . 
 ( a ) western blot showing expression of active phosphorylated and total her2 and mapk in untransduced ( parental ) nih 3t3 cells and those transduced with wt human her2 or the indicated mutants . 
g776va and g776vb are duplicate cell lines that were transduced independently . ( b ) representative images and ( c ) quantification of soft - agar colony formation ( anchorage - independent growth ) by untransduced ( parental ) nih 3t3 cells and those transduced with wt human her2 or the indicated mutants . 
 analysis to control for alteration status of the genes reported to be most frequently mutated in luminal a breast cancer ( ie , tp53 , pik3ca , gata3 , and cdh1 ) 33 retained significant enrichment of cooccurrence of map3k1 alterations with all erbb2 short variants and with erbb2 kd short variants ( table 2 )  . 
this indicates that the co - occurrence of erbb2 and map3k1 variants in a subset of breast carcinoma cases is independent of the status of luminal aassociated genes and cannot be attributed solely to these cases belonging to the luminal a subtype . 
these findings suggest that there may be a particular subtype of her2 - negative , predominantly er - positive breast cancer driven by a combination of activating erbb2 kinase domain mutations and inactivating map3k1 alterations . discussion this is the first demonstration of clinical response to tp regimens ( tp plus exemestane followed by tp plus nab - paclitaxel ) in a patient with a her2 kinase domain mutation ( erbb2 g776v ) and expands our knowledge of treatment options for patients with metastatic breast cancer containing erbb2 mutations . 
although it cannot be excluded that the clinical benefit was due to the exemestane or nab - paclitaxel , these findings are consistent with four previous studies that have reported responses of patients with erbb2 - mutant ( s310f , l755s , v777l , l869q ) breast cancer to antiher2 agents including antibodies and tyrosine kinase inhibitors , with a cytotoxic chemotherapy backbone in three of the four cases.13 - 16 in addition , studies in cultured cells and animal xenograft models have shown that multiple erbb2 mutations associated with erbb2 amplification - negative breast cancer are activating , oncogenic , and sensitive to the irreversible pan - her inhibitor neratinib and , in some cases , to the reversible pan - her inhibitor lapatinib and the anti - her2 antibody trastuzumab.21 the effects of the g776v mutation on her2 functions had not previously been characterized in published studies , although one study reported that this alteration is untargetable.35 however , including the substitution similar alterations , g776s36 and the compound substitution and insertion g776vinsc , 37 - 39 have been shown to be activating . 
 her2 - targeted agents have shown high rates of clinical benefit in her2 - positive breast cancers and are approved for both er - negative and erpositive patients.11 , 12 the clinical data for her2negative breast carcinoma cases driven by erbb2 mutations are considerably more limited . 
a recent large - scale study of nonamplification genomic alterations in erbb2 in breast cancer18 reported three patients who responded to anti - her2 therapy , two with er - positive tumors and one with triple - negative cancer.13 - 15 , 18 consistent with this , the patient we report here had er - positive cancer , and additional analysis showed that 80% ( four of five ) of breast cancers profiled at foundation medicine and found to carry the erbb2 g776v mutation were er positive . 
the previous study reported that several genes are frequently coaltered with erbb2 in erbb2 - nonamplified breast cancers , particularly the tumor suppressor tp53 and the oncogene pik3ca.18 here , we show that erbb2 - nonamplified breast carcinomas driven by erbb2 kinase domain mutations specifically are significantly enriched for co - alteration with the tumor suppressor map3k1 . 
although frequent alteration of map3k1 in the luminal / erpositive breast cancer subtype has been reported , 33 the current study provides evidence of association between erbb2 and map3k1 mutations independent of subtype and suggests that activating mutations in the erbb2 kinase domain may cooperate with inactivation of map3k1 to promote cancer progression . 
additional work will also be needed to elucidate the effects of er status on the clinical efficacy of her2 - targeted agents in erbb2 - mutated breast cancer . in this patients case , the clinical decision to use tp - based regimens was based on prior reports of similar erbb2 mutations in breast cancer or nsclc.36 - 42 , 46 , 48 the preclinical experiments reported here confirmed that erbb2 g776v is an activating mutation , and the patient had a good clinical outcome on tp - based therapy . 
this study adds to a body of evidence supporting the use of her2 - targeted therapy in patients with metastatic breast cancer with erbb2 mutations , although given that the tp - based regimens in this case included exemestane or nab - paclitaxel that may have significantly contributed to the clinical benefit , caution must be exercised in applying these findings to the treatment of other patients . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . yakov chudnovsky employment : foundation medicine stock and other ownership interests : foundation medicine travel , accommodations , expenses : foundation medicine runjun d . 
schrock employment : foundation medicine stock and other ownership interests : foundation medicine caitlin connelly employment : foundation medicine kyle gowen employment : foundation medicine stock and other ownership interests : foundation medicine travel , accommodations , expenses : foundation medicine garrett m . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan - kettering cancer center jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine honoraria : pfizer , emd merck serono research funding : foundation medicine siraj m . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health related to microbiome in non - neoplastic disease ( inst ) ron bose honoraria : genentech , novartis consulting or advisory role : genentech affiliations yakov chudnovsky , alexa b . 
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schiavon g , hrebien s , garcia - murillas i , et al : analysis of esr1 mutation in circulating tumor dna demonstrates evolution during therapy for metastatic breast cancer . 
tokunaga e , kimura y , oki e , et al : akt is frequently activated in her2 / neu - positive breast cancers and associated with poor prognosis among hormone - treated patients . 
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ali sm , alpaugh rk , downing sr , et al : response of an erbb2 - mutated inflammatory breast carcinoma to human epidermal growth factor receptor 2 - targeted therapy . 
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chumsri s , weidler j , ali s , et al : prolonged response to trastuzumab in a patient with her2 - nonamplified breast cancer with elevated her2 dimerization harboring an erbb2 s310f mutation . 
grellety t , soubeyran i , robert j , et al : a clinical case of invasive lobular breast carcinoma with erbb2 and cdh1 mutations presenting a dramatic response to anti - her2 - directed therapy . 
ross js , wang k , sheehan ce , et al : relapsed classic e - cadherin ( cdh1 ) - mutated invasive lobular breast cancer shows a high frequency of her2 ( erbb2 ) gene mutations . 
ross js , gay lm , wang k , et al : nonamplification erbb2 genomic alterations in 5605 cases of recurrent and metastatic breast cancer : an emerging opportunity for anti - her2 targeted therapies . 
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minami y , shimamura t , shah k , et al : the major lung cancer - derived mutants of erbb2 are oncogenic and are associated with sensitivity to the irreversible egfr / erbb2 inhibitor hki - 272 . 
shimamura t , ji h , minami y , et al : non - small - cell lung cancer and ba / f3 transformed cells harboring the erbb2 g776insv_g / c mutation are sensitive to the dual - specific epidermal growth factor receptor and erbb2 inhibitor hki - 272 . 
suzuki t , fujii a , ohya j , et al : antitumor activity of a dual epidermal growth factor receptor and erbb2 kinase inhibitor mp - 412 ( av - 412 ) in mouse xenograft models . 
wang se , narasanna a , perez - torres m , et al : her2 kinase domain mutation results in constitutive phosphorylation and activation of her2 and egfr and resistance to egfr tyrosine kinase inhibitors . 
buttitta f , barassi f , fresu g , et al : mutational analysis of the her2 gene in lung tumors from caucasian patients : mutations are mainly present in adenocarcinomas with bronchioloalveolar features . 
arcila me , chaft je , nafa k , et al : prevalence , clinicopathologic associations , and molecular spectrum of erbb2 ( her2 ) tyrosine kinase mutations in lung adenocarcinomas . 
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de gr`eve j , moran t , graas mp , et al : phase ii study of afatinib , an irreversible erbb family blocker , in demographically and genotypically defined lung adenocarcinoma . 
kris mg , camidge dr , giaccone g , et al : targeting her2 aberrations as actionable drivers in lung cancers : phase ii trial of the pan - her tyrosine kinase inhibitor dacomitinib in patients with her2 - mutant or amplified tumors . 
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bryce purpose genomic testing has increased the quantity of information available to oncologists . unfortunately , many identified sequence alterations are variants of unknown significance ( vuss ) , which thus limit the clinicians ability to use these findings to inform treatment . 
we applied a combination of in silico prediction and molecular modeling tools and laboratory techniques to rapidly define actionable vuss . materials and methods exome sequencing was conducted on 308 tumors from various origins . most single nucleotide alterations within gene coding regions were vuss . 
a subset of receptor tyrosine kinase vuss was characterized by laboratory comparison of each vus versus its wild - type counterpart in terms of expression and signaling activity . results the study identified 4 , 327 point mutations of which 3 , 833 were vuss . 
three vuss ( fgfr2 f276c , fgfr4 r78h , and kdr g539r ) showed increased basal or ligand - stimulated erk phosphorylation compared with their wild - type counterparts , which suggests that they support transformation . 
for example , braf v600e is well accepted as a therapeutic target in metastatic melanoma.7 however , a current challenge in genomic oncology care is the evaluation of the potential therapeutic significance of large numbers of uncharacterized , nonsynonymous sequence alterations referred to as variants of unknown significance ( vuss ) in potentially oncogenic proteins . when novel vuss are identified , the clinical team must try to draw conclusions about whether the variant is a driver mutation or has no significance for cancer pathogenesis . 
although some recurrent mutations within oncogenic proteins have been characterized as having an effect on protein function and thus , the promotion of transformation , novel vuss identified through clinical genomic testing often are lacking functional information . the definition of the therapeutic value of vuss is a current unmet need.8 we demonstrate how in silico analysis and experimental laboratory studies can rapidly determine the potential therapeutic value of a vus . 
by using bioinformatic analysis of exome sequencing results , a large number of potentially deleterious vuss that are therapeutically targetable were identified with a high frequency of occurrence in kinases . 
the mayo clinic irb approved the in vitro functional studies of somatic mutations identified in tumors of patients enrolled in the cim oncology service ( irb 15 - 003386 )  . 
redcap ( research electronic data capture ) hosted at the mayo clinic was used to collect and store clinical follow - up data.10 results vuss are the most common findings in tumor exome sequencing analysis targeted and exome sequencing were performed on heterogeneous solid ( 57% ) and hematologic ( 43% ) malignancies ( data supplement )  . 
vuss , which constitute mutations that are functionally uncharacterized or previously unreported in the cosmic ( catalogue of somatic mutations in cancer ) database , 11 comprised the majority ( 89% ) of the point mutations observed in this cohort ( fig 1a )  . 
obstacles to clinical use of these data resulted from large numbers of vuss identified in each patient , uncertainty whether identified vuss are potential drivers of transformation , and whether encoded proteins were therapeutically targetable . to begin to address these difficulties , vuss were filtered into a subgroup of 905 in genes that encode proteins therapeutically targetable by food and drug administrationapproved drugs or by investigational agents available through clinical trials . 
protein class analysis demonstrated that rtks and serine / threonine kinases represent the largest therapeutically targetable functional classes , with mutations in both hematologic and solid tumors ( fig 1b )  . these 905 therapeutically targetable vuss were then evaluated in silico , and those determined to be benign by two prediction tools were removed , which left 522 potentially deleterious , therapeutically targetable vuss in 226 patients ( data supplement ) or 12% of the total variants detected ( fig 1a )  . 
the distribution of protein classes represented in this deleterious , therapeutically targetable subgroup ( fig 1c ) was similar to that of the therapeutically targetable vus group ( fig 1b )  . 
 a significant findings , 11% targetable , deleterious , vuss , 12% other vuss , receptor tyrosine kinase serine / threonine kinase notch receptor dna endonuclease endocytosis nonreceptor tyrosine kinase tumor suppressor pi3k family ubiquitin ligase apoptotic regulator growth inhibition receptor tyrosine kinase serine / threonine kinase notch receptor endocytosis nonreceptor tyrosine kinase dna endonuclease pi3k family histone deacetylase tumor suppressor hormone receptor fgf receptor ubiquitin ligase growth inhibition hematologic solid no . 
 ( a ) frequency of significant findings and uncharacterized / unreported variants of unknown significance ( vuss ) in 4 , 327 point mutations reported in 308 patient tumors , including solid and hematologic malignancies . 
 ( b ) frequency of the most commonly observed protein classes in 905 therapeutically targetable vuss . with pymol software ( schrodinger , new york , ny ; data supplement ) , which predicted potentially altered function on the basis of their location within the proteins kinase domain ( data supplement )  . in silico and functional characterization of rtk vuss identified a subset of new targetable mutations ten rtk vuss from varied solid and hematologic malignancies ( data supplement ) and in reinterest were selected for gions of functional additional evaluation by in vitro testing . 
in addition , sequence alignment across species demonstrated that the wt residue that corresponded to each of the 10 vuss was completely conserved among diverse species , including mouse , rat , bovine , and human proteins . 
biochemical studies of r78h demonstrated no significant differences from wt fgfr4 in overall expression levels when expressed in kmch - 1 cholangiocarcinoma cells ( figs 2b and 2c )  . 
cellular localization of wt and r78h fgfr4 was also similar and exhibited mainly a plasma membrane distribution with intracellular labeling of probable golgi membranes ( fig 2e )  . however , r78h fgfr4 exhibited a small , but significantly elevated fgf2 - stimulated phosphoerk ( perk ) level compared with wt ( figs 2b and 2d )  . two kdr vuss , g55e and g539r , are located in the extracellular domain in proximity to amino acids that form disulfide bonds ( c53 and c530 ) ; thus , these amino acid substitutions may potentially affect neighboring disulfide bonds . 
 ( c ) frequency of the most commonly observed protein classes in 522 therapeutically targetable , potentially deleterious vuss . cells that expressed g55e kdr ( figs 3a and 3c )  . kdr variants and wt exhibited a similar punctate distribution by immunofluorescence ( fig 3d )  . vuss g251e , v484m , and t643m of pdgfra and variants v258l and v316m of pdgfrb were investigated . 
all variants fall in the extracellular domain of their respective receptor except t643m , which occurs within the pdgfrb kinase domav258l was predicted to be functionally benign but was of interest for in vitro study because of its ig3 location . 
pdgfr vuss were generally similar to their wt counterparts in terms of expression , distribution of polypeptide species on western blots , pdgf - stimulated perk levels , and cellular localization ( data supplement ) , except that pdgfra v484m was significantly lower in expression and pdgfstimulated perk levels than wt ( data supplement ) and pdgfrb v316m was significantly lower in expression than wt ( data supplement )  . f276c mutant is a new , constitutively active form of fgfr2 although predicted in silico to be benign , fgfr2 k41e , identified in an acute myeloid leukemia , was selected for additional study because of its location in the extracellular ig1 of fgfr2 and its unknown effect on ligand binding in nearby ig2 and ig3 ( data supplement )  . 
the fgfr2 f276c mutation identified here from a cholangiocarcinoma was also in a single cholangiocarcinoma in the cosmic database but has not been characterized.11 , 12 f276c is located in an extracellular , ig - like c2 - type 3 domain13 where ligand binding occurs.14 a different amino acid substitution at the same residue , f276v , has been reported in crouzon syndrome.15 modeling of wt and f276c fgfr2 showed that the extracellular receptor of fgfr2 contains an intrinsic disulfide bond between c278 and c342 in ig3 ( fig 4a , shown in gold )  . 
these data suggest that the f276c variant is functionally altered relative to the wt form . when fgfr2 proteins were expressed in kmch - 1 cells , immunofluorescence microscopy showed that the wt and k41e fgfr2 proteins were localized mainly to the cell surface and occurred on intracellular structures , likely endosomes and the golgi apparatus ( fig 4c )  . 
in contrast , the f276c variant exhibited an endoplasmic reticulumlike appearance and bright golgi - like intracellular structures in most cells , with only a minority of cells showing an obvious plasma membrane distribution ( fig 4c )  . 
each protein was expressed as an approximately 130 - kda polypeptide as detected by western blot ( fig 4d )  . however , the f276c variant was expressed at a higher level and the k41e variant at a lower level compared with wt ( fig 4d ) , although cells were transfected with equal amounts of dna for the different fgfr2 constructs . functional characteristics of fgfr2 proteins were assessed by studying perk signaling . 
because the f276c fgfr2 variant is expressed at higher levels than wt when equal amounts of dna were used , a lower ratio of f276c construct dna was used for transfection in the following experiments so that resulting levels of wt and f276c fgfr2 proteins were comparable ( figs 4e and 4f ) : kmch - 1 cells transfected with fgfr2 constructs were treated for 16 hours in serum - free media with fgf2 , lysed , and analyzed by western blot . 
the expression of wt or k41e fgfr2 in the absence of fgf2 increased perk levels beyond control levels , and treatment with fgf2 led to approximately fivefold increases in perk compared with control for both wt and k41e . 
however , expression of f276c fgfr2 significantly increased the perk level in the absence of fgf2 compared with wt fgfr2 , with little increase upon treatment with fgf2 ( figs 4e and 4g )  . 
in summary , f276c fgfr2 has high expression , altered cellular distribution , and increased constitutive activity compared with wt . finally , the sensitivity of wt and f276c fgfr2 activities to treatment with the fgfr inhibitor bgj398 were compared . 
at concentrations between 0 and 100 nm , erk phosphorylation was similarly partially inhibited by bgj398 in cells that expressed wt or f276c , and both fgfr2 forms were completely inhibited by bgj398 at 200 nm ( figs 5a and 5b )  . 
right panel : after 1 day , the cells were incubated with and without 20 ng / ml fgf2 in 0.1% bovine serum albumin / dmem for 16 hours at 37c . 
values are mean 6 se normalized to wt ( + fgf2 ) levels . bracket indicates groups within treatment types ( 2fgf or + fgf ) among fgfr4 - transfected samples that were significantly different ( p , .05 ) from each other in twotailed t tests . 
 ( e ) hucct - 1 cells were transfected with flag - tagged wt and r78h fgfr4 for 2 days and then processed for immunofluorescence by using an anti - flag antibody . 
he was originally treated in a clinical trial with gemcitabine , cisplatin , and silmitasertib , which resulted in a partial response . he remained on this treatment of 10 months , at which time his disease progressed and he was switched to capecitabine and oxaliplattwo months later , the disease became refractory to that regimen . 
after 1 day , the cells were serum starved in 0.1% bovine serum albumin / dmem overnight and then incubated with and without 25 ng / ml vascular endothelial growth factor ( vegf ) for 10 min at 37c . 
cell samples were then lysed and subjected to western blot analysis for flag - kdr , phospho - erk ( perk ) , total erk , and vinculequal amounts of total protein were loaded per lane . 
g55e expression of full - length receptor ( approximately 200 kda ) was decreased compared with wt , with the appearance of approximately 70to 80 - kda fragments , which suggested decreased stability / increased degradation of the g55e forperk was barely detectable in g55e samples and not increased by vegf treatment . 
brackets indicate groups within treatment types ( 2vegf or + vegf ) among kdr - expressing samples that were significantly different ( p , .05 ) from one another in two - tailed t tests . 
 ( d ) hucct - 1 cells were transfected with flag - tagged wt and variants of unknown significance kdr for 2 days and then processed for immunofluorescence with an anti - flag antibody . 
on the basis of this finding , the patient started on bgj398 ( clinicaltrials.gov identifier : nct02150967 ) , achieved a partial response to therapy after 2 months ( figs 5c and 5d ) , and maintained the response for an additional 4 months , at which time new lesions developed that led to discontinuation of bgj398 . 
as a result of our in vitro studies of f276c , a mechanism of action has now been correlated with this observed clinical response of the tumor to bgj398 . discussion the volume of new data from individual and group sequencing efforts ( eg , the cancer genome atlas ) has rapidly expanded the understanding of the incidence and frequency of mutations in disparate cancers . 
few mutations have extensive preclinical and clinical evidence that support the effectiveness of targeted therapies , and genomic testing often reveals that tumors have numerous vuss , including variant sequences for which no functional data are available . mutations that have not been functionally characterized present a significant and growing challenge to the treating physician . 
the extracellular receptor of fgfr2 contains an intrinsic disulfide bond between c278 and c342 in the immunoglobulin - like domain 3 ( ig3 ; shown in gold )  . residue f276 is highlighted in gray and is proximal to the disulfide bridge . 
the fgfr2 f276c variant ( highlighted in red ) may lead to the introduction of aberrant disulfide bonds that could alter the activation state of the prote ( b ) sequence alignment shows that residue f276 is highly conserved among the fgfr2 family from zebrafish to humans ( sequence alignment performed by using clustal omega [ embl - ebi , wellcome genome campus , uk ] ; uniprotkb entry numbers are shown )  . 
 ( c ) hucct - 1 cholangiocarcinoma cells transfected with the wt , k41e , and f276c fgfr2 forms for 2 days were fixed , permeabilized , and processed for immunofluorescence by using the flag antibody . 
kmch - 1 cells were transfected with fgfr2 forms by using a 3.5 / 5 ratio of f276c / wt and k41e dna to adjust expression of the f276c protein to similar levels as the wt forafter 1 day , cells were switched to serum - free medium with or without 20 ng / ml fgf2 and incubated an additional 16 hours at 37c before lysis . 
lysates were analyzed by western blot for expression of fgfr2 - flag , phospho - erk ( perk ) , total erk , and vincul ( f ) quantitation of fgfr2 levels in western blots as in ( e )  . 
brackets indicate groups within treatment types ( 2fgf or + fgf ) among fgfr2 - expressing samples that were significantly different ( p , .05 ) from one another in two - tailed t tests . 
 ( a ) kmch - 1 cells were transfected with f276c and wild type ( wt ) by using a 3.5 / 5 dna ratio , respectively , to normalize expression levels . 
values are mean 6 se and expressed as percent inhibition of perk signal compared with cells with no bgj398 . response of fgfr2 f276ccontaining tumor to bgj398 in ( c ) september 2015 ( pretreatment , with magnetic resonance imaging showing a 30.1mm tumor diameter [ red line ] ) and ( d ) october 2015 ( postinitiation of treatment , with pan - fgfr inhibitor bgj398 magnetic resonance imaging showing tumor shrinkage to an 18.2 - mm diameter [ red line ] )  . fgfr2flag perk fgfr2flag perk f276c bgj398 ( nm ) 50 100 200 f276c bgj398 ( nm ) becomes how to quickly assess the potentially deleterious effect of vuss that occur in therapeutically targetable genes . 
with multiple uncharacterized / unreported mutations returned for each patient , a method of prioritizing which variants to study in depth is necessary . we addressed this problem by developing an approach that uses an in silico filtering process to prioritize mutations of the highest biologic and clinical interest . 
of these 10 variants , seven were found to be altered in expression or activity relative to the wt protein , and three of these ( fgfr2 f276c , fgfr4 r78h , and kdr g539r ) demonstrated greater activity than their wt counterparts ( table 1 ) , which suggests that these mutations play a role in promoting oncogenesis . 
in contrast , four vuss ( fgfr4 k41e , kdr g55e , pdgfra v484m , and pdgfrb v316m ) exhibited reduced expression compared with their wt counterparts , and thus were unlikely to be involved in oncogenesis in the tumors where they occurred . 
these findings not only support the strength of our in silico analysis in predicting whether vuss are functionally altered but also point to the inability to distinguish among activating , deactivating , and destabilizing mutations . optimization of appropriate cellular models is important in methods development for functional evaluation of vuss . 
for more understanding of the functional significance of vuss , these studies should be followed by experiments that use cell types that match the vus tumor of origin and evaluate end points such as cell growth and viability . fgfr2 f276c was identified as a vus of potential interest because of the presence of several factors , including prediction of a deleterious effect by two algorithms , 3d modeling that suggests an increase in activity on the basis of its location in the ligand - binding ig3 , and proximity to a key disulfide bond . 
dashes ( ) indicate no change versus wild - type protein . abbreviation : vus , variant of unknown significance . * increases or decreases in activity ( phospho - erk levels ) indicate changes seen versus wild type upon stimulation with ligand , except for fgfr2 f276c , which exhibited increased constitutive activity . constitutive receptor dimerization and activation , which lead to a variety of skeletal and craniosynostosis disorders ( eg , crouzon and pfeiffer syndromes ) .16 - 18 our molecular modeling combined with the demonstration that f276c fgfr2 is more highly expressed and constitutively active than the wt receptor suggests that this mutation alters disulfide bonds , which alters receptor dimerization and activity similarly to the fgfr2 mutations seen in craniosynostosis syndromes . 
by using in vitro studies , we show that the f276c fgfr2 variant is sensitive to bgj398 , a panfgfr inhibitor , which was also reflected clinically in the response of a patients tumor when treated with bgj398 as part of a clinical trial ( fig 5 )  . 
however , additional studies , such as the testing of bgj398 effectiveness in impeding growth of organoids or xenografts that express wt versus f276c , are needed to confirm that fgfr2 f276c is actionable . the ability to identify potentially actionable vuss from numerous vuss for each patient tumor would simplify therapeutic choices . 
in silico analysis requires only hours to conduct and as demonstrated here , can yield a subset of vuss that encode therapeutically targetable proteins likely to be altered in function by their variant sequence . in vitro functional studies are more time consuming and may not fit practically within a patients progression timeline , but they may yield moredefinitive findings . 
gawryletz no relationship to disclose sikander ailawadhi consulting or advisory role : amgen , takeda pharmaceuticals , novartis research funding : pharmacyclics ( inst ) travel , accommodations , expenses : amgen , takeda pharmaceuticals , novartis stephen m . 
ansell honoraria : webmd , research to practice research funding : bristol - myers squibb ( inst ) , celldex therapeutics ( inst ) , seattle genetics ( inst ) , merck ( inst ) , affimed ( inst ) , trillium therapeutics ( inst ) kelly k . 
halfdanarson consulting or advisory role : lexicon ( inst ) , ipsen ( inst ) , merrimack ( inst ) research funding : esanex ( inst ) , ipsen ( inst ) , boston biomedical ( inst ) thai h . 
 research funding : merck , bristol - meyers squibb , roche ( inst ) , genentech ( inst ) , x4p pharmaceuticals ( inst ) , amgen ( inst ) prashant kapoor consulting or advisory role : sanofi ( inst ) research funding : amgen ( inst ) , takeda pharmaceuticals ( inst ) aaron s . 
mansfield consulting or advisory role : trovagene ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) travel , accommodations , expenses : bristol - myers squibb nathalie meurice no relationship to disclose amulya a . 
nowakowski consulting or advisory role : celgene ( inst ) , morphosys ( inst ) , genentech ( inst ) research funding : celgene ( inst ) animesh pardanani no relationship to disclose sameer a . 
feldman consulting or advisory role : infinity pharmaceuticals patents , royalties , other intellectual property : inventor of technology for which the mayo clinic holds an unlicensed patent or has submitted a patent application ( inst ) ramesh k . 
ramanathan honoraria : taiho pharmaceutical , cerulean pharma , pharmacyclics , insys therapeutics , novocure consulting or advisory role : cerulean pharma , novocure , insys therapeutics , pharmacyclics research funding : abbvie ( inst ) , celgene ( inst ) , merck ( inst ) , schering plough ( inst ) , merrimack ( inst ) , boston biomedical ( inst ) , berg ( inst ) , superlab far east ( inst ) steven i . 
robinson travel , accommodations , expenses : tricon pharmaceuticals raoul tibes research funding : novartis ( inst ) , merck ( inst ) , seattle genetics ( inst ) , boehringer ingelheim ( inst ) , astellas pharma ( inst ) , astex pharmaceuticals ( inst ) heidi d . 
mcwilliams consulting or advisory role : merrimack ( inst ) research funding : prism biolab ( inst ) , genentech ( inst ) , novartis ( inst ) , newlink genetics ( inst ) , eli lilly ( inst ) , aduro biotech ( inst ) , pfizer ( inst ) , sanofi ( inst ) travel , accommodations , expenses : astrazeneca mrinal m . 
wieben patents , royalties , other intellectual property : champions oncologylicensed ip - targeted therapy with abiraterone acetate ( $0 received ) , wuxi appteclicensed ip - breast cancer xenografts ( $12 , 737 to mayo clinic ; inst ) , affymetrix - licensed ip on several variants in drug processing enzymes ( $0 in past 2 years ) , life technologieslicensed ip on several variants in drug processing enzymes ( $0 in past 2 years ) tammy m . 
kennedy patents , royalties , other intellectual property : patent on unrelated work ( us patent 9 , 458 , 189 ) for ligation of stapled polypeptides issued october 4 , 2016 eric w . 
borad stock and other ownership interests : glaxosmithkline , gilead sciences consulting or advisory role : g1 therapeutics , td2 , fujifilm ( inst ) , agios ( inst ) , insys therapeutics ( inst ) , novartis ( inst ) , arqule ( inst ) , celegene ( inst ) , inspyr therapeutics , halozyme therapeutics ( inst ) research funding : boston biomedical ( inst ) , mirna therapeutics ( inst ) , senhwa biosciences ( inst ) , medimmune ( inst ) , bioline ( inst ) , agios ( inst ) , halozyme therapeutics ( inst ) , celgene ( inst ) , threshold pharmaceuticals ( inst ) , toray ( inst ) , dicerna pharmaceuticals ( inst ) , sillajen ( inst ) , eisai ( inst ) , taiho pharmaceuticals ( inst ) , emd serono ( inst ) , isis pharmaceuticals ( inst ) , incyte ( inst ) , sun biopharma ( inst ) , ariad pharmaceuticals ( inst ) , imclone systems ( inst ) travel , accommodations , expenses : arqule , celgene , astrazeneca aminah jatoi research funding : entera health , boston biologics martin e . 
kennedy , university of georgia , athens , ga . supported by the mayo clinic center for individualized medicine . presented at the science of team science 2016 conference , phoenix , az , may 16 - 19 , 2016 . support prior presentation references 35 : 49 - 62 , 2016 1 . 
horak p , fr ohling s , glimm h : integrating next - generation sequencing into clinical oncology : strategies , promises onco targets ther 9 : 7355 - 7365 , 2016 and pitfalls . 
harris pa , taylor r , thielke r , et al : research electronic data capture ( redcap ) a metadata - driven methodology and workflow process for providing translational research informatics support . 
steinberger d , vriend g , mulliken jb , et al : the mutations in fgfr2 - associated craniosynostoses are clustered in five structural elements of immunoglobulin - like domain iii of the receptor . 
lajeunie e , heuertz s , el ghouzzi v , et al : mutation screening in patients with syndromic craniosynostoses indicates that a limited number of recurrent fgfr2 mutations accounts for severe forms of pfeiffer syndrome . 
ratisoontorn c , fan gf , mcentee k , et al : activating ( p253r , c278f ) and dominant negative mutations of fgfr2 : differential effects on calvarial bone cell proliferation , differentiation , and mineralization . 
connor claire bascuana jamil asselah nathaniel bouganim vronique poulin jacques jolivet petro vafiadis philippe le guillaume martel frdric lemay annie beaudoin khashayar rafatzand prosanto chaudhury jeffrey barkun peter metrakos victoria marcus atilla omeroglu george chong mohammad r . 
foulkes steven gallinger george zogopoulos ( continued ) purpose we investigated the translational value of reflex testing for germline mutations in four homology - directed dna repair predisposition genes ( brca1 , brca2 , palb2 , and atm ) in consecutive patients with pancreatic adenocarcinoma . methods one hundred fifty patients with french - canadian ( fc ) ancestry were evaluated for founder mutations , and 114 patients were subsequently assessed by full gene sequencing and multiplex ligation - dependent probe amplification for nonfounder mutations . 
2018 by american society of clinical oncology introduction pancreatic adenocarcinoma ( pac ) remains a lethal malignancy.1 - 3 although novel combinations of systemic therapies have been evaluated in pac over the past decade , 4 , 5 these efforts have not resulted in marked improvements in patient survival . 
these clinical failures , together with the projection that pac will be the second leading cause of cancer death by 2030 , 6 highlight the urgent need for both early detection and precision therapy strategies for pac . genomic subtypes of pac have been described and may inform therapies . 
in this large , two - center study , we assessed whether reflex genetic testing of brca1 , brca2 , palb2 , and atm should be offered to all or select patients with incident pac . methods study participants two case series were evaluated . 
the fc study participants included consecutively enrolled patients with a clinical diagnosis of pac and self - reported fc ancestry ( one or more grandparents ) enrolled in the quebec pancreas cancer study ( qpcs ) 30 between april 2012 and june 2017 . 
 the montreal - toronto ( mt ) study participants included patients , unselected for ancestry or family history , with a clinical diagnosis of pac who were consecutively enrolled in the qpcs or ontario pancreas cancer study31 between august 2014 and december 2015 . 
dna from circulating lymphocytes , saliva , and / or tissue specimens was obtained from participants and their relatives for germline genetic testing , segregation , and / or somatic studies ( data supplement )  . 
ethics approval was obtained for both studies . clinical variables and family history data were extracted from the qpcs and ontario pancreas cancer study registries.30 , 31 eligibility for clinical genetic testing was assessed using the national comprehensive cancer network ( nccn ) brca - related breast and / or ovarian cancer syndrome testing criteria v2.2016.32 for the nccn criteria , a second primary cancer in the proband was considered equivalent to a cancer in a close blood relative , and all prostate cancers were assumed to have a gleason score < 7 , because these were unavailable . fc founder mutation screening screening for the 20 fc founder mutations ( 11 brca1 , eight brca2 , and one palb2 ; listed with historical names in data supplement ) 21 - 26 was performed on a rolling basis . 
screening was performed by polymerase chain reaction and bead - based fluorescent detection on the luminex 200 platform26 , 33 or by sanger sequencing ( primers listed in data supplement )  . full gene sequencing in the fc study , full gene sequencing of brca1 , brca2 , palb2 , and atm was performed after founder mutation testing ( data supplement )  . 
pathogenic mutation prevalence french - canadian study ( n = 150 ) montreal - toronto study ( n = 236 ) founder panel testing ( n = 150 ) full gene testing ( n = 114 * ) ashkenazi jewish ( n = 30 ) nonfounder ( n = 206 ) no . 
these vus were assessed for pathogenicity using in silico prediction algorithms ( data supplement )  . multiplex ligation - dependent probe amplification patients with pac with fc ancestry have not previously been characterized for mutations in these four genes . 
therefore , fc study participants were evaluated for large insertions / deletions or rearrangements in brca1 , brca2 , palb2 , and atm by multiplex ligation - dependent probe amplification ( mlpa ; data supplement )  . statistical analysis categorical and continuous patient variables were compared using fishers exact test or t test , respectively . 
for the os analyses , atm carriers were included in the noncarrier group , because it remains uncertain whether these patients exhibit similar genomic and therapeutic profiles as brca1 , brca2 , and palb2 carriers . 
fc patients who underwent founder testing only were not considered in statistical analyses , because nonfounder mutations could not be excluded . results mutation carriers if samples were available , pathogenic variants and vus predicted pathogenic were assessed for segregation in relatives affected with pac or associated cancers and for loss - of - heterozygosity ( loh ) or somatic silencing of the wild - type allele in the tumors ( data supplement )  . one hundred seventy - four patients underwent reflex fc founder mutation testing during the study period . 
notably , an fc patient who was excluded from our analyses because of a final pathologic diagnosis of ampullary carcinoma was found to carry an atm mutation ( table 2 )  . 
considering these results , mlpa was performed only for brca1 and brca2 for the subsequent 24 samples , because large alterations are more common in these genes , 39 - 42 with no mutations identified . two - hundred ninety - one patients were enrolled during the mt study period . 
 table 2 shows mutation details as well as clinical and family history variables for the individual carriers . the results from segregation and somatic silencing analyses of mutation and vus carriers are described in the data supplement . 
the pedigrees of the palb2 mutation carriers demonstrate cosegregation of the germline mutation with pac in family fc - 2 ( fig 1a ) and a pac phenocopy in family fc - 58 ( fig 1b )  . 
the pedigrees for the remaining fc study carriers are shown in the data supplement . clinicopathologic characteristics , including responses to chemotherapy of all carriers , are shown in table 2 , with additional mutation details in the data supplement . 
a family history ( one or more firstor second - degree relatives ) of pac ( p = .03 ) , breast cancer ( p = .02 ) , or prostate cancer ( p = .009 ) were each significantly associated with carrier status . 
a previous study of patients with incident pac reported a brca1 and brca2 mutation prevalence of 4.6%.13 this observation was driven by a 12.1% founder mutation prevalence among aj patients , whereas the prevalence among non - aj patients was 3.7%.13 hu et al14 reported a similar prevalence of 3.1% among 96 unselected patients with pac without aj ancestry . 
moreover , one of the two rare nonfounder mutations identified did not originate from the fc branch of the patients pedigree , whereas the second nonfounder mutation was identified in an adopted patient where paternal ancestry could not be confirmed . 
although we did not identify any brca1 mutations , pathogenic mutations in brca1 are less common than in brca2 in pac , and our study is not sufficiently powered to exclude a contribution of brca1 mutations.13 , 47 , 48 considering the low cost of targeted mutation screening , we recommend founder mutation testing include all 20 fc founder mutations . in the fc study case series , two carriers had the palb2 c.2323c > t ( p.gln775 * ) fc founder mutation . 
the observation of cosegregation with disease , as well as loh of the wild - type allele in the tumors of affected carriers in family fc - 2 , provides further support of a causal role for this palb2 mutation in pac . among patients with pac with fc ancestry , a single pathogenic atm mutation was identified ( 0.9% ; 95% ci , 0% to 5.3% ) , which has only been previously reported as a somatic variant.50 an additional germline atm mutation , with loh in the tumor , was identified in an fc patient with a final diagnosis of ampullary carcinoma . 
a recent genomic study of ampullary carcinomas described mutations in atm ; however , it was not indicated whether these mutations originated in the germline.51 no atm mutations were identified among the patients reporting aj ancestry . 
consistent with these findings are reports showing absence of large genomic changes in brca1 , brca2 , and / or palb2 in families with breast / ovarian cancer with fc ancestry , 22 , 42 , 52 , 53 aj ancestry , 54 and ethnically diverse families.13 , 41 , 55 , 56 large genomic changes in atm are also rare.57 collectively , these studies suggest that mlpa analyses for these four genes in patients with incident pac should not be necessary . in recent years , numerous studies have demonstrated that brca1and brca2 - deficient pac tumors are sensitive to platinum - based chemotherapies or parpis.7 , 9 - 11 although less well established , similar findings in palb2 - deficient tumors treated with dna damaging agents have been reported.58 , 59 here , we report two patients with germline palb2 mutations treated with platinum - based chemotherapy . 
much less is known about the clinical behavior of patients with pac with atm mutations , and the genomes of atm - deficient pac tumors infrequently exhibit the genomic hallmarks associated with hdr deficiency.7 , 8 although there is some evidence that atm - deficient breast and prostate cancers have sensitivity to olaparib ( a parpi ) , 60 , 61 the chemotherapeutic sensitivities to platinum - based agents and parpis in atm deficient pac remains unknown . 
although this was not an intent - to - treat study , the carrier status of participants may have influenced chemotherapy choices as well as decisions to include surgical and ablative approaches to manage advanced disease . 
because these treatment decisions were not uniform , and in the absence of intent - to - treat clinical trial data , it is not possible to fully assess the benefit of platinum therapy in carriers . increased numbers of mutation - associated neoantigens8 and favorable responses to immunotherapy.62 although genetic studies have reported the prevalence of germline mutations in these genes among patients with incident pac to be low ( 0% to 2% ) , 14 , 16 these studies have not considered large genomic changes ( eg , exon deletions ) , which are prevalent in patients with lynch syndrome.63 considering the promise of immunotherapy , genetic studies to fully assess the prevalence of mismatch repair germline mutations in pac are merited . although our study was focused on hdr genes , additional genetic subtypes of pac may be amenable to precision oncology strategies . 
the genomes of pac tumors with deficiency in one or more of the dna mismatch repair genes ( mlh1 , msh2 , msh6 , and pms2 ) exhibit finally , although age at diagnosis and family history have not consistently been shown to be predictors of brca1 or brca2 carrier status in pac , 13 , 64 significant associations were observed in our study . 
nearly one in six patients with pac diagnosed at age 50 years or younger were found carriers noncarriers p = .068 carriers noncarriers p = .049 * 1 , 000 2 , 000 2 , 500 3 , 000 1 , 500 2 , 000 1 , 500 time ( days ) 1 , 000 time ( days ) no . 
kaplan - meier survival curves for ( a ) all - stages ( 0 - iv ) carriers versus noncarriers , ( b ) late - stage ( iii / iv ) carriers versus noncarriers , and ( c ) late - stage ( iii / iv ) carriers treated with platinum versus noncarriers . 
we found that patients with pac meeting family history criteria of two or more firstor second - degree relatives with pancreas , breast , ovarian , or prostate cancer on the same side of the family , or one such relative and a second primary of one of these cancer types , identified carriers with similar sensitivity and specificity to the nccn guidelines . 
in the interim , in view of existing health care systems and considering our observed founder mutation frequencies , we recommend reflex founder mutation testing of patients with incident pac with fc or aj ancestry and reflex full - gene sequencing for these four hdr genes in patients without founder ancestry or who test negative for founder mutations who are diagnosed at age 50 years or younger or who meet our described family history criteria . 
 foulkes provision of study material or patients : adeline cuggia , ayelet borgida , spring holter , claire bascuana , jamil asselah , nathaniel bouganim , vronique poulin , jacques jolivet , petro vafiadis , philippe le , guillaume martel , frdric lemay , annie beaudoin , khashayar rafatzand , prosanto chaudhury , jeffrey barkun , peter metrakos , william d . 
connor , claire bascuana , jamil asselah , nathaniel bouganim , vronique poulin , jacques jolivet , petro vafiadis , philippe le , guillaume martel , annie beaudoin , prosanto chaudhury , jeffrey barkun , peter metrakos , george chong , mohammad r . 
smith no relationship to disclose cavin wong no relationship to disclose adeline cuggia no relationship to disclose ayelet borgida no relationship to disclose spring holter no relationship to disclose anita hall no relationship to disclose ashton a . 
 jamil asselah consulting or advisory role : roche canada research funding : celgene nathaniel bouganim no relationship to disclose vronique poulin honoraria : amgen jacques jolivet no relationship to disclose petro vafiadis no relationship to disclose philippe le no relationship to disclose guillaume martel stock and other ownership interests : abbott laboratories honoraria : sanofi canada travel , accommodations , expenses : baxter frdric lemay honoraria : esperas pharma consulting or advisory role : esperas pharma prosanto chaudhury honoraria : novartis , ipsen , astellas pharma consulting or advisory role : ipsen travel , accommodations , expenses : novartis jeffrey barkun travel , accommodations , expenses : baxter canada peter metrakos honoraria : novartis , ipsen , astellas pharma consulting or advisory role : ipsen , novartis speakers ' bureau : amgen travel , accommodations , expenses : novartis , ipsen victoria marcus no relationship to disclose atilla omeroglu no relationship to disclose george chong no relationship to disclose mohammad r . 
foulkes no relationship to disclose steven gallinger no relationship to disclose annie beaudoin honoraria : amgen , novartis , roche canada consulting or advisory role : amgen , novartis travel , accommodations , expenses : novartis , roche canada khashayar rafatzand no relationship to disclose george zogopoulos consulting or advisory role : astellas pharma , baxalta , ipsen research funding : diazon pharmaceuticals patents , royalties , other intellectual property : tc - ptp inhibitors as apc activators for immunotherapy travel , accommodations , expenses : baxalta affiliations alyssa l . 
foulkes , and george zogopoulos , research institute of the mcgill university health centre ; jamil asselah , nathaniel bouganim , khashayar rafatzand , prosanto chaudhury , jeffrey barkun , peter metrakos , victoria marcus , atilla omeroglu , william d . 
rahib l , smith bd , aizenberg r , et al : projecting cancer incidence and deaths to 2030 : the unexpected burden of thyroid , liver , and pancreas cancers in the united states . 
andrei a - z , hall a , smith al , et al : increased in vitro and in vivo sensitivity of brca2 - associated pancreatic cancer to the poly ( adp - ribose ) polymerase - 1 / 2 inhibitor bmn 673 . 
lowery ma , kelsen dp , stadler zk , et al : an emerging entity : pancreatic adenocarcinoma associated with a known brca mutation : clinical descriptors , treatment implications , and future directions . 
cavallone l , arcand sl , maugard cm , et al : comprehensive brca1 and brca2 mutation analyses and review of french canadian families with at least three cases of breast cancer . 
cote s , arcand sl , royer r , et al : the brca2 c.9004g > a ( e2002k ) [ corrected ] variant is likely pathogenic and recurs in breast and / or ovarian cancer families of french canadian descent . 
tischkowitz m , sabbaghian n , hamel n , et al : contribution of the palb2 c.2323c > t [ p.q775x ] founder mutation in well - defined breast and / or ovarian cancer families and unselected ovarian cancer cases of french canadian descent . 
ghadirian p , robidoux a , nassif e , et al : screening for brca1 and brca2 mutations among french - canadian breast cancer cases attending an outpatient clinic in montreal . 
belanger mh , dolman l , arcand sl , et al : a targeted analysis identifies a high frequency of brca1 and brca2 mutation carriers in women with ovarian cancer from a founder population . 
oros kk , ghadirian p , greenwood cmt , et al : significant proportion of breast and / or ovarian cancer families of french canadian descent harbor 1 of 5 brca1 and brca2 mutations . 
borgida ae , ashamalla s , al - sukhni w , et al : management of pancreatic adenocarcinoma in ontario , canada : a population - based study using novel case ascertainment . 
higgs je , harkness ef , bowers nl , et al : the brca2 polymorphic stop codon : stuff or nonsense ? j med genet 52 : 642 - 645 , 2015 35 . 
cavalieri s , funaro a , pappi p , et al : large genomic mutations within the atm gene detected by mlpa , including a duplication of 41 kb from exon 4 to 20 . 
ameziane n , van den ouweland amw , adank ma , et al : lack of large genomic deletions in brip1 , palb2 , and fancd2 genes in brca1 / 2 negative familial breast cancer . 
foulkes wd , ghadirian p , akbari mr , et al : identification of a novel truncating palb2 mutation and analysis of its contribution to early - onset breast cancer in french - canadian women . 
kwong a , ng eko , wong clp , et al : identification of brca1 / 2 founder mutations in southern chinese breast cancer patients using gene sequencing and high resolution dna melting analysis . 
martin dc , mark bl , triggs - raine bl , et al : evaluation of the risk for tay - sachs disease in individuals of french canadian ancestry living in new england . 
moisan a - m , fortin j , dumont m , et al : no evidence of brca1 / 2 genomic rearrangements in high - risk french - canadian breast / ovarian cancer families . 
gunard f , pedneault cs - l , ouellette g , et al : evaluation of the contribution of the three breast cancer susceptibility genes chek2 , stk11 , and palb2 in non - brca1 / 2 french canadian families with high risk of breast cancer . 
pylks k , erkko h , nikkil j , et al : analysis of large deletions in brca1 , brca2 and palb2 genes in finnish breast and ovarian cancer families . 
rouleau e , jesson b , briaux a , et al : rare germline large rearrangements in the brca1 / 2 genes and eight candidate genes in 472 patients with breast cancer predisposition . 
villarroel mc , rajeshkumar nv , garrido - laguna i , et al : personalizing cancer treatment in the age of global genomic analyses : palb2 gene mutations and the response to dna damaging agents in pancreatic cancer . 
 circulating human papillomavirus dna as a biomarker of response in patients with locally advanced cervical cancer treated with definitive chemoradiation purpose to determine whether plasma human papillomavirus ( hpv ) dna predates clinical recurrence and compare its accuracy with 3 - month fluorodeoxyglucose positron emission tomography ( fdg - pet ) in locally advanced cervical cancer . methods this prospective multicenter study accrued 23 women with stage ib to iva cervical cancer planned for definitive chemoradiation therapy ( crt )  . 
all patients underwent routine staging investigations , including thoracic , abdominal , and pelvic computed tomography scan and pelvic magnetic resonance imaging , and were treated with definitive standard external beam radiotherapy ( 45 in 1.8 - gy daily fractions ) to the pelvis with or without inclusion of para aortic lymph nodes , weekly cisplatin chemotherapy ( 40 mg / m2 ) , and brachytherapy . 
all patients were examined routinely every 3 months during the first 2 years after crt and every 6 months thereafter . hpv genotyping was performed by qpcr ( sacace biotechnologies , como , italy ) using genomic dna isolated from baseline cervical swabs . 
at each time point , 20 ml of edta blood was collected at each center and then promptly transported on ice to the central laboratory where plasma was immediately separated and stored at 80c . 
after purification of cfdna from 5 to 10 ml of plasma ( circulating nucleic acid kit ; qiagen , hilden , germany ) , total cfdna concentration was determined using qubit fluorometric quantitation ( thermo fisher scientific , waltham , ma )  . 
absolute quantification of hpv genotype - specific dna was performed on 10 ng of cfdna by dpcr using the qx200 droplet digital pcr system ( bio - rad laboratories , hercules , ca )  . 
each 20 - l reaction contained a final concentration of 900 nm of each primer , 250 nm of each taqman probe , and 1 droplet dpcr master mix ( ddpcr supermix for probes ; bio - rad )  . 
multiplexed taqman assays ( primers and probes from bio - rad ) targeted the e6 and e7 open reading frames from the hpv genotype detected from the baseline swab for each patient . 
 before their use on cfdna , each dpcr assay was evaluated for technical performance using negative controls ( fragmented human genomic dna supplied in the sacace biotechnologies hpv genotyping kit ) and positive controls ( fragmented genomic dna from genotype - matched cervical cancer tissue )  . 
flow of patients by plasma human papillomavirus ( hpv ) and fluorodeoxyglucose positron emission tomography ( pet ) results at the end of or 3 months after chemoradiation therapy ( crt )  . 
given that the e6 and e7 values were highly correlated ( pearsons correlation coefficient , 0.997 ) , their average value was used for all analyses . tumor response on the 3 - month fdg - pet was defined per previous studies into three categories : complete metabolic response , partial metabolic response , and progressive disease.5 consistent with the conventional definitions used to categorize 3 - month fdg - pet in patients with cervical cancer who underwent definitive radiotherapy , 5 the latter two categories were considered a positive test . 
pfs was measured from the date of diagnosis and defined as the time to disease progression / relapse ( biopsy proven relapse or progression of disease on serial imaging ) 5 , 6 or death . 
as of the cutoff date for this analysis ( january 16 , 2018 ) , median follow - up from the date of diagnosis for patients without relapse was 24 months ( range , 18 to 31 months )  . 
currently , at least six active phase iii studies are evaluating this question worldwide ( clinicaltrials.gov identifiers : nct02853604 , nct01414608 , nct00980954 , nct02036164 , nct03468010 , and nct02703961 )  . 
thus , many patients will be subjected needlessly to additional toxicities of these investigational agents , and real benefits may be missed as a result of the inclusion of lower - risk patients . 
representative example of a patient with stage iib cervical cancer who had a false - positive fluorodeoxyglucose positron emission tomography scan ( maximum standardized uptake value , 4.6 ) at approximately 3 months after chemoradiation therapy ( crt ) , with no definite residual disease on subsequent imaging or clinical examination to date ( 25 months after crt )  . 
although the specificity of fdg - pet might have improved with repeated or later ( ie , > 3 months post - treatment ) assessment , the added cost and delay in diagnosing recurrent disease would be major drawbacks of this approach . 
we anticipate that this approach would result in more - successful adjuvant trials , thus enabling personalized and adaptive treatment regimens . strengths of the current study include the prospective design and serial analysis of plasma hpv dna . 
this study may not be applicable to modern cohorts because it was conducted before concurrent cisplatin chemotherapy became standard of care and included patients with small - cell carcinoma ( rare histology with more - aggressive behavior )  . 
this may be explained by more - modern radiation techniques that are leading to improved locoregional control.21 , 22 our follow - up time was limited , although the majority of recurrences in cervical cancer occur within 2 years . 
 bratman administrative support : kathy han provision of materials or patients : kathy han , eric leung , lisa barbera , jennifer croke , anthony fyles , robert wolfson , scott v . 
bratman data analysis and interpretation : kathy han , eric leung , lisa barbera , anthony fyles , ur metser , michael milosevic , melania pintilie , zhen zhao , scott v . 
di grappa no relationship to disclose anthony fyles no relationship to disclose ur metser no relationship to disclose michael milosevic no relationship to disclose melania pintilie no relationship to disclose robert wolfson no relationship to disclose zhen zhao no relationship to disclose kathy han no relationship to disclose eric leung no relationship to disclose scott v . 
 affiliations kathy han , eric leung , lisa barbera , elizabeth barnes , jennifer croke , anthony fyles , ur metser , michael milosevic , robert wolfson , and scott v . 
bratman , princess margaret cancer centre , university health network ; and eric leung , lisa barbera , elizabeth barnes , and robert wolfson , odette cancer centre , sunnybrook health sciences centre , toronto , ontario , canada . supported by the university of toronto department of radiation oncology collaborative seed grant . 
is supported by the princess margaret cancer foundation 's gattuso - slaight personalized cancer medicine fund . presented at the american society of radiation oncology annual meeting , san diego , ca , september 24 - 27 , 2017 , and the canadian association of radiation oncology annual meeting , toronto , ontario , canada , september 13 - 16 , 2017 . support prior presentation references 1 . 
chemoradiotherapy for cervical cancer meta - analysis collaboration : reducing uncertainties about the effects of chemoradiotherapy for cervical cancer : a systematic review and meta - analysis of individual patient data from 18 randomized trials . 
rose pg , java j , whitney cw , et al : nomograms predicting progression - free survival , overall survival , and pelvic recurrence in locally advanced cervical cancer developed from an analysis of identifiable prognostic factors in patients from nrg oncology / gynecologic oncology group randomized trials of chemoradiotherapy . 
schwarz jk , siegel ba , dehdashti f , et al : metabolic response on post - therapy fdg - pet predicts patterns of failure after radiotherapy for cervical cancer . 
ho cm , yang ss , chien ty , et al : detection and quantitation of human papillomavirus type 16 , 18 and 52 dna in the peripheral blood of cervical cancer patients . 
wang wy , twu cw , lin wy , et al : plasma epstein - barr virus dna screening followed by 18f - fluoro - 2 - deoxy - d - glucose positron emission tomography in detecting posttreatment failures of nasopharyngeal carcinoma . 
jeannot e , becette v , campitelli m , et al : circulating human papillomavirus dna detected using droplet digital pcr in the serum of patients diagnosed with early stage human papillomavirusassociated invasive carcinoma . 
sturdza a , ptter r , fokdal lu , et al : image guided brachytherapy in locally advanced cervical cancer : improved pelvic control and survival in retroembrace , a multicenter cohort study . 
charra - brunaud c , harter v , delannes m , et al : impact of 3d image - based pdr brachytherapy on outcome of patients treated for cervix carcinoma in france : results of the french stic prospective study . 
 functional rna studies are a useful tool in variant classication but must be used with caution : a case study of one brca2 variant paola nix , phd1 ; erin mundt , ms1 ; susan manley , ms / cgc , mba1 ; bradford coffee , phd1 ; and benjamin roa , phd1 the use of genetic testing to evaluate hereditary cancer risk is increasing , because it can inform clinical management and cancer treatment decisions . 
a germline pathogenic variant in one of these genes is associated with an increased risk of cancer and therefore merits altered including increased surveilmedical management , lance and the option of risk - reducing surgeries.1 in addition , the identication of a pathogenic brca1 or brca2 variant may affect treatment decisions and clinician recommendations for women with breast and / or ovarian cancer.1 - 4 given these clinical implications , laboratories accurately that classify variants as part of hereditary cancer genetic testing . is essential although established guidelines from the american college of medical genetics ( acmg ) and association for molecular pathology ( amp ) provide a framework to help with variant classication , 5 there may be challenges interpreting the available evidence for some variants.6 , 7 this includes some sequence variants that have the potential to affect mrna splicing . 
a notable fraction of disease - causing variants in cancer predisposition genes affect splicing.8 - 10 many of these occur at the 5 ( cid : 1 ) and 3 ( cid : 1 ) exon - intron boundaries , and the potential impact on splicing is well established , based on the expected sequence at the canonical splice donor and acceptor ( 6 1 , 2 splice sites ) .5 however , sequence variants located beyond these canonical splice sites may also alter mrna processing . 
pathogenicity for these variants is more difcult to assess , and additional functional evidence is often required to determine the actual impact of the variants on splicing . clinical laboratories commonly use functional rna studies to aid in the classication of variants that may affect splicing . 
although these studies can provide useful evidence about the pathogenicity of such variants , there are important caveats to consider , and care must be taken in both how the studies are performed and how the data are interpreted.11 , 12 one important consideration when using rna analysis to classify variants that may affect splicing is that the observation of a splice defect alone may not be sufcient evidence for classication . 
aberrant splicing may result either in no normal transcript produced by the variant allele ( complete splice defect ) or in some residual normal transcript produced by the variant allele.13 these partial , or leaky , splice defects may result in enough functional transcript being produced to support normal protein function . 
therefore , it is essential to quantify any aberrant splice product and determine whether the variant allele produces any normal transcript when using rna analysis in variant classication . functional rna studies often involve reverse transcription polymerase chain reaction ( rt - pcr ) analysis of rna extracted from a patient blood sample or lymphoblastoid cell line . 
one method to distinguish variant - specic transcripts is to use informative single nucleotide in the same pcr polymorphisms ( snps ) present amplicon as the putative spliceogenic variant being tested ( ie , tag snps )  . 
in the case of a heterozygous variant carrier , these tag snps can differentiate the transcripts produced by the normal allele versus the variant allele , especially when the variant allele is located in the intron and not present in the processed mrna . 
rt - pcr products representing these transcripts can be cloned into a vector system or used directly as templates for sequencing analysis . laboratories that do not require rna analysis to include allele - specic transcript quantication for variant classication , either as part of their own studies or from published studies , may misclassify splice - related variants and potentially report false - positive results . 
in addition , care must be taken in assigning pathogenicity if a variant allele has been shown to produce functional transcript , because it may be unclear whether the amount transcript could support normal protein function . 
 commentary splice variants causing brca2 exon 3 skipping , a variant allele may express up to 20% aberrant product yet not be associated with even a moderate risk of cancer . case study of brca2 c.426 - 12_426 - 8del one example of a splice variant with a complex interpretation is brca2 c.426 - 12_426 - 8delan intronic variant resulting in the deletion of ve nucleotides from the dna sequence adjacent to the splice acceptor site of exon 5 . 
published functional studies support this prediction , with studies by zhang et al in 200916 and sanz et al in 201017 demonstrating that this variant causes skipping of exon 5 , which is out of frame . 
however , both studies also noted that the variant allele produces full - length transcript , indicating a partial splice defect . the variant recently published rna analyses from one clinical testing laboratory showed that brca2 c.426 - 12_426 - 8del caused aberrant splicing , resulting in the deletion of exon 5.18 , 19 there was no allele - specic quantication of however , normal transcripts to determine how much , if any , was produced from the variant allele . 
still , the authors concluded that this variant could be classied as likely pathogenic in accordance with acmg / amp guidelines5 on the basis of rna studies demonstrating abnormal splicing from ( evidence category ps3 ) , absence of population controls ( evidence category pm2 ) , and in silico splicing models predicting a weakening of the native site ( evidence category pp3 ) .18 conversely , our laboratory initially classied brca2 c.42612_426 - 8del as a vus on the basis of the evidence available at the time ( fig 1 )  . 
this evidence included the 2 previously published functional studies showing that the variant allele produced some normal transcript.16 , 17 these functional data alone are not sufcient to determine whether the variant is associated with increased cancer risk , because there is uncertainty in how much normal transcript must be expressed by the variant allele to support normal brca2 function . 
although population databases and in silico modeling can provide useful evidence for classication , these tools also must be considered carefully . benign variants also can be rare ( eg , absent from population controls ) , and in silico splicing models cannot discriminate between a full or partial splice defect . 
as a result , this body of evidence was not sufcient for our laboratory to classify brca2 c.42612_426 - 8del as likely pathogenic . our laboratory was later able to reclassify brca2 c.42612_426 - 8del from vus to benign using additional clinical evidence . 
this included evidence from a validated history weighting algorithm ( hwa ) that scores a variant on the basis of the personal and family histories of multiple individuals who carry the specic variant of interest.20 the variant - specic score is compared with matched pathogenic controls ( individuals with known pathogenic variants in brca2 ) and matched benign controls ( individuals with only benign variants in brca2 and other breast and ovarian cancer - risk genes ; appendix fig a1 )  . 
in this case , the hwa called brca2 c.426 - 12_426 - 8del benign , indicating that carriers did not have a personal or family in brca2 history consistent with a pathogenic variant ( appendix fig a1 )  . in addition , co - occurrence of a vus with known pathogenic variants in the same gene can provide evidence that a variant is benign on the basis of associated clinical phenotypes . 
this provides additional evidence that time of brca2 c.426 - 12_426 - 8del hwa and co - occurrence data are consistent with a benign classication and suggest the variant allele does produce enough functional transcript to support normal brca2 function . 
the recent uptake in laboratories performing their own functional rna studies for variant classication can lead to denitive , actionable ndings for more patients ; however , it is critical that rna analysis be held to a high standard to ensure that variant classications also retain a high level of accuracy . to this end , there are several important considerations in the classication of variants in cancer predisposition genes that may affect splicing . 
snp , single - nucleotide polymorphism . some functional transcript , additional clinical evidence may be needed to determine whether the variant is pathogenic . the importance of this additional clinical evidence is exemplied by brca2 c.426 - 12_426 - 8del . 
karam et al18 came to the conclusion that the variant was likely pathogenic on the basis of rna analysis that identied aberrant splicing , in combination with population frequency and in silico modeling data ; however , the rna analysis performed in that study did not elucidate whether the transcript . 
the variant allele produced any functional previously published rna analyses were considered insufcient for a pathogenic classication by our laboratory because of evidence that the variant allele does produce some normal transcript . 
previous studies have highlighted the complex situation that discordant classications create for patients and providers regarding patient management and the potential for discordant test results for family members tested at different laboratories.6 , 7 second , classications made without careful consideration of rna analysis performed by the laboratory or from published studies may result in a false - positive test result . 
professional societies provide recommendations for the medical management of patients with a pathogenic variant in brca2 , including consideration of risk - reducing surgical interventions and eligibility for cancer drug therapies.1 - 4 the example of brca2 c.426 - 12_426 - 8del highlights the need for caution when interpreting functional evidence from rna analysis for variants that may affect splicing to avoid potential mismanagement and inappropriate medical intervention . in this case , variant classication made without full the partial splice defect consideration of resulted in a classication of likely pathogenic for a variant that our laboratory classied as benign when assessed with additional clinical evidence . acmg / amp guidelines provide useful guidance for variant classication5 but do not inform on every caveat or complexity that may be encountered during variant classication . given the severity of the potential clinical consequences of incorrectly classifying a benign variant as pathogenic , additional guidance for interpreting rna sequencing data may be necessary to enhance accurate classication of splicerelated variants . 
this could involve a stepwise process until sufcient data ( from functional rna studies and other sources ) are obtained to accurately perform variant classication ( fig 1 )  . 
for example , the rna transcripts observed in a patient who carries a sequence variant should be compared with the range of full - length and alternative transcripts that naturally occur in normal controls . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . erin mundt employment : myriad genetics stock and other ownership interests : myriad genetics susan manley employment : myriad genetics stock and other ownership interests : myriad genetics bradford coffee employment : myriad genetic laboratories stock and other ownership interests : myriad genetics benjamin roa employment : myriad genetics leadership : myriad genetics stock and other ownership interests : myriad genetics research funding : myriad genetics patents , royalties , other intellectual property : intellectual property held by employer myriad genetics ( inst ) travel , accommodations , expenses : myriad genetics no other potential conicts of interest were reported . acknowledgment we thank krystal brown , phd , and stephanie meek , phd , for their assistance in preparing the manuscript . references daly mb , pilarski r , berry mp et al : nccn clinical practice guidelines in oncology : genetic / familial high - risk assessment : breast , ovarian , and pancreatic ( version 1.2020 ) , nccn clinical practice guidelines in oncology , 2020 . 
 nix et al armstrong d , plaxe s , alvarex r , et al : nccn clinical practice guidelines in oncology : ovarian cancer including fallopian tube cancer and primary peritoneal cancer , version 4.2017. 
curr oncol 25 : s151 - s160 , 2018 richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
genet med 17 : 405 - 424 , 2015 gradishar w , johnson k , brown k , et al : clinical variant classication : a comparison of public databases and a commercial testing laboratory . 
oncologist 22 : 797 - 803 , 2017 balmaa j , digiovanni l , gaddam p , et al : conicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
j clin oncol 34 : 4071 - 4078 , 2016 rhine cl , cygan kj , soemedi r , et al : hereditary cancer genes are highly susceptible to splicing mutations . 
whiley pj , de la hoya m , thomassen m , et al : comparison of mrna splicing assay protocols across multiple laboratories : recommendations for best practice in 12 . 
brnich se , abou tayoun an , couch fj , et al : recommendations for application of the functional evidence ps3 / bs3 criterion using the acmg / amp sequence standardized clinical testing . 
gelli e , colombo m , pinto am , et al : usefulness and limitations of comprehensive characterization of mrna splicing proles in the denition of the clinical relevance of brca1 / 2 variants of uncertain signicance . 
sanz dj , acedo a , infante m , et al : a high proportion of dna variants ofbrca1 and brca2 is associated with aberrant splicing in breast / ovarian cancer patients . 
pruss d , morris b , hughes e , et al : development and validation of a new algorithm for the reclassication of genetic variants identied in the brca1 and brca2 genes . 
the new era of precision medicine complicates communication even further as a result of our increasing reliance on genomic data and the varying psychological responses to genomic - based treatments and their expected outcomes . 
however , many of the communication issues are actually similar to perennial long - standing communication issues in oncology , which center on providing hope when breaking bad news and ensuring that adequate informed consent to treatments is obtained . 
we highlight these new communication issues that focus on clinical and ethical questions ( ie , informed consent , shared decision making , patient autonomy , and uncertainty in oncologic treatments ) and provide guidance on working with each scenario . 
in this article , we address common reactions of patients to genomic information and provide thoughtful communication suggestions using a shared decision making framework to help patients cope with the inherent distress - provoking uncertainties in oncology practice . introduction the practice of oncology depends on adequate communication between patients and clinicians . although the science of cancer medicine is advancing exponentially , information technology advances are seriously impeding the critical component of face - to - face communication . 
the key communication issues in oncology are always twofold : the delivery of emotionally charged bad news while sustaining hope in the presence of a lifethreatening prognosis and ensuring that patients understand the information that is provided.1 the advent of precision medicine now complicates the discussion of these issues in oncology in significant ways.2 , 3 although there is a growing emphasis on providing humanistic care in oncology ( eg , palliative care initiatives ) , the increasingly complicated science and public hype , coupled with limited time to talk with patients in busy oncology clinics , significantly threaten this goal . 
science and technology have yet again raced ahead of the human element , which depends on communication to foster those critical elements of mutual respect and trust . the application of genomic medicine is now accessible for the majority of oncology patients because the cost of genomic sequencing has decreased 1 millionfold from a decade ago.4 - 6 the development of molecular diagnostic , prognostic , and predictive biomarkers continues to change the landscape of clinical oncology.7 furthermore , technologic advances facilitate the use of largescale databases that store genomic data , such as ascos cancerlinq and ibm watson.8 - 11 also , research trial design in precision oncology is evolving from the randomized controlled trial to designs that harness these large data - collection initiatives and evaluate responses to drugs across multiple cancer subtypes ( ie , basket trial design ) .12 , 13 at the same time that genomic science and technology have created new research and clinical treatment paradigms , social media and drug direct - to - consumer marketing in the united states has brought information to the public with remarkable speed and fervor.14 , 15 although there are advantages to patients being informed consumers , handling this complex information without any interpretation of its meaning is not helpful.16 this breadth and rapidity of information adds an additional strain to the already complicated communication that occurs between clinicians and their patients.17 direct - to - consumer marketing is new and often amplifies drug benefits beyond reality . 
mcfarland , memorial sloan kettering cancer center , west harrison ; and elizabeth blackler , smita banerjee , and jimmie holland , memorial sloan kettering cancer center , new york , corresponding author : daniel c . 
 understand the implications for the overall cancer experience , eg , their satisfaction or dissatisfaction with their oncology care , or how this information influences patients treatment choices.15 its implications may be greatest when considering the delicate end - of - life conversations that are critical to quality oncology care.18 therefore , it is critical that we understand patients experiences in this new technologic age of genomic medicine . 
the shared decision making ( sdm ) model of communication promotes patient activation and engagement in health care and is an optimal model to guide communication tasks in the precision medicine era.19 , 20 the sdm model describes how clinician and patient jointly participate in making a health decision , having discussed the options and their benefits and harms , as well as having considered the patients values , preferences , and circumstances . 
it respects patient autonomy and leads to improved patient satisfaction when patients are faced with clinical options for which there is not a clearly correct choice , as is frequently encountered in the context of precision oncology.21 - 24 in this article , we highlight the psychological , social , and ethical issues that are part of our new treatments , and we provide communication suggestions on the basis of sdm . 
patients emotional reactions should be considered before , during , and after sdm to ensure effective communication . i won the lottery : the lucky biology club member jane was a 58 - year - old teacher who was diagnosed with stage iv adenocarcinoma of the lung that harbored an epidermal growth factor receptor mutation . her cancer responded well to erlotinib . 
after 15 months , her cancer began to grow as it became increasingly resistant to erlotinib , and chemotherapy was required to treat it . jane became extremely angry and frustrated that her cancer had progressed and found it hard to appreciate the benefit that the drug provided in light of its failure . she remained in shock and disbelief and had a difficult time accepting the need to adjust her treatment to the new situation . the lucky biology club members have driver actionable mutations such as epidermal growth factor receptor , anaplastic lymphoma kinase , ros1 , and brafv600e . 
subsequently , discussions about health care proxies , financial planning , and wills are often delayed . in terms of discussion , it is important to acknowledge the implications of disease biology and to corroborate and correct the information that they have from other sources . 
using sdm principles , the clinician could initiate a discussion of options by saying , there are some specific treatment options for you , on the basis of your cancers genomic make - up . 
however , the clinician must also discuss the framework for treatment and prognosis : although the cancer is still not curable , the mutation indicates that we have some additional treatment options . 
the clinician may say , given this news , it seems like a good time to talk about what to do next or we are in a different place now . 
is it okay if we talk more about the other options and next steps ? addressing the underlying emotions and acknowledging fear are important tools that should be dealt with before focusing on sdm . 
sdm can help provide clinical decision transparency and ameliorate disappointments with limited treatment effectiveness . i failed the test : the unlucky biology club member sarah was a 73 - year - old patient with newly diagnosed nonsmall - cell lung cancer who had no actionable mutation . 
at her first visit , she was clutching an article from the new york times and yelling , i want the serial killer ! she had come to memorial sloan kettering cancer center in hopes of enrolling in a clinical trial with first - line immunotherapy . when she did not meet trial entry criteria because of her pd - l1 status , she became enraged at being denied the opportunity that she had heard and read about . 
the article she held on to described how immunotherapy unleashes a so - called serial killer that ravages all cancer cells in the body , which is understandably what she wanted.29 sarah had delayed seeking cancer treatment in hopes of having the right mutation to enroll in a clinical trial . 
the unlucky biology club members feel that their tumor biology has conspired against them ; they are angered by the treatment options that are available for others but not for thethey feel that it is not fair that other patients with the same cancer are treated with more desirable targeted therapies . 
this may resonate with failures in their life before having cancer . it is crucial to validate their emotions of anger , fear , frustration , and worry by saying , i cant imagine what it has been like for you to hear this news ; i can see this is very upsetting . 
is it okay if we talk a bit more about what this means ? in this scenario , it is important to educate and reorient the patient who has been stuck on one idea as a result of their limited information . 
as part of sdm , the clinician should provide information on benefit and risk , such as , this information helps us plan the very best treatment for you . clinicians should be careful about comparing patients and especially about providing unsolicited information . this is an opportunity to re - establish / realign with the patients goals . 
given what you know about your illness , whats most important to you ? or , as you think about the future , are there situations or things that you want to make sure you accomplish or avoid ? explain that treatment options can be re - evaluated and tailored to the patients wishes . 
it also sends a positive message that although one opportunity for treatment did not work out , the team provides realistic hope and direction , despite a disappointment . a new drug has just come out : a novel treatment michael was a 47 - year - old patient with sinonasal undifferentiated carcinoma , a rare form of head and neck cancer . 
although the drug had never been tested with his specific head and neck cancer , sinonasal undifferentiated carcinoma , his clinicians believed that he had to be informed about the new treatment because he was young and otherwise healthy and , if it worked , would possibly provide a durable response . 
he did not want to complicate or disrupt the decision to accept hospice care , yet he felt ethically bound to offer a treatment for which michael had become eligible . this case highlights an ethical dilemma associated with the interface of advancing science and clinical care . 
it illustrates how the emergence of rapidly changing oncology treatments begets new levels of uncertainty in the cancer experience ( eg , no specific data for a cancer subtype , even though pembrolizumab had been approved for head and neck cancers )  . 
clinicians are taught to provide answers , which can be frustrating when new data become available and raise new questions and more uncertainty ( eg , does the drug work in this cancer subtype ? )  . 
medical training teaches clinicians how to handle uncertainty , but it does not teach them how to share its presence in a constructive way for patients.30 a full discussion was undertaken with the patient about the absence of data , the ethical reason for informing him of the new agent , and the inherent complications of considering another new treatment . 
he decided to stay with his decision to begin hospice care . it is important to discuss patients emotions about clinical uncertainty and the various treatment options , framed in the context of their current clinical situation : i realize this is all very complicated ; let me try to explain these options in the setting of your illness . 
also , it is important to frequently determine their level of understanding ( facilitates deliberation ) : can you tell me , in your words , what you understand ? also , it is helpful to review the patients clinical information together as a background to discussing the uncertainty . in situations of greatest clinical uncertainty , it is important to assure the patient that you are available for further discussion of their concerns and questions . 
a partnering statement , conveying the sense of were in this together and i will continue to work with you , is helpful to demonstrate a personal commitment to providing the best care possible despite the clinical uncertainty . 
patients who feel that they are in a partnership with their clinicians are better able to trust them and tolerate clinical uncertainty.31 i know i can beat it : the denier don was a 68 - year - old patient with progressive metastatic colon cancer who had received all conventional lines of cancer treatment . 
don said that he was the exception , frequently finding ways to explain how the negative clinical facts did not apply to hihe made many references to newly available targeted therapies that he believed could be used to treat his cancer . hope is a critical component of coping , especially in a time of great need . 
these offers are often made in the face of overwhelming disease biology . for most advanced cancers , precision oncology finds driver mutations in only a minority of cases , and the goal of most early trial design is still safety and not necessarily efficacy . 
these are difficult concepts to explain to patients who will probably only hear that there is hope . typically , educating the denier will require revisiting the topic several times to try to arrive at a shared understanding of the actual situation : you may be eligible for a trial if your cancer has a certain mutation ; however , taking the drug in this basket trial may not extend your life . 
when the patients condition worsens , the education may have to become more pointed : scans dont always reflect what is going on in terms of tumor growth and a change in functional status is an indication that the cancer is progressing . 
i hear you saying that what is most important to you is and i understand that you want to make sure to avoid the following this demonstrates that they have been heard , ensures that the goal of hope is not being taken away , and helps the patient to evaluate options . 
it is also important to keep in mind that the denier fluctuates in their level of denial and may partially accept the reality of the situation . patients often maintain two levels of awareness and acknowledgment of the situation . 
one is cognitive : i know how ill i athe other is emotional : i simply cant believe i could die . both exist simultaneously in many patients , which accounts for these day - to - day attitudinal changes . an ongoing positive clinician - patient relationship allows these feelings to emerge , and a more realistic discussion can occur about end - of - life planning , for example . 
often , a patients underlying fear will ameliorate in the context of working closely together . i have done my research : the overly or misinformed patient barbara was a 49 - year - old well - educated professional with nonsmall - cell lung cancer metastatic to brain and bone . 
barbara had strong opinions about the new treatment choices for lung cancer and was unwilling to consider therapies that were more appropriate for her type of disease . this case illustrates the complexity of precision oncology and the level of sophisticated genomic knowledge that is required to have a fully informed conversation with a patient . 
she explained the difference between inherited dna mutations , for which olaparib could be used in the presence of an inherited brca2 mutation in ovarian cancer , and the more common somatic mutations present in noninherited cancers such as her brca2 - mutated nonsmall - cell lung cancer . 
in this situation , correcting misinformation and misunderstanding is essential : there are many exciting cancer treatments , but whats important is that we find the right one for you . some patients want all available information and want to actively participate in their treatment decision . 
also , uncovering each patients major concerns is critical : what information would be most helpful for me to know about you ? then , it is important to acknowledge the patients concerns : this must be very upsetting for you . 
this acknowledges the importance of alliance.32 a request for a specific cancer treatment may be driven by an attempt to reach a goal , which may be modifiable in certain cases . 
it is crucial to demonstrate that you clearly understand their request : i hear you saying that whats most important is to continue treating your cancer to ensure you can reach your goal . case continued : a rebiopsy after progression revealed a her2 mutation that made her eligible for a basket trial . the oncologist invited another discussion of her tumor dna mutations and informed her that a newly found her2 mutation would qualify her for a basket trial . 
the previous genomics discussion on inherited and somatic mutations helped her understand that she would be treated with a group of patients with different cancers , who would all have the same somatic tumor dna mutation , to assess safety and perhaps efficacy in accordance with the trial objectives . she understood alternative treatment options and was offered a decision delay to facilitate deliberation and decision making . 
so far , the literature remains limited.7 , 33 , 34 patients acknowledge the promise of precision medicine but also consistently raise concerns about the discovery of incidental findings , information overload , complications from additional biopsies with delay in definitive cancer treatment , and the lack of a clear benefit.35 the risk of ineffective communication is that patients misunderstand the nature and seriousness of their diseases , which may lead to more aggressive and futile cancer treatments at the end of life or to increased fear and anxiety , while increasing stress and burnout in members of the medical team.36 on the other hand , effective communication enhances shared decision making , decreases patient distress , and increases patient satisfaction and trust in the medical team.25 shared decision making is the communication style that is preferred by most patients.37 patients make choices that are guided by the clinicians information and recommendations . 
patients may also have preferences on a spectrum of communication styles that can range from paternalistic ( ie , the patient is a passive recipient of their care ) to the clinician who is a nondirective information provider or educator ( ie , the patient is given choices and decides on management according to his / her preferences ) .30 it can be helpful to simply ask how the patient and family would like to make decisions , and the clinician can discuss this spectrum to gain clarification . 
discussing therapeutic uncertainty is often a difficult task for clinicians and leads to clinician behaviors of not disclosing all of the information , not talking about it , or oversimplifying the information.30 understandably , this can leave patients with a distorted account of their clinical situation . 
they may make sense of the situation by prescribing to alternative introducing so - called explanations or hopes , extramedical values , or seeking other remedies ( eg , alternative treatments ) when presented with clinical uncertainty.30 the idea of effective disclosure has been proposed as a potential goal in discussing uncertainty with patients . 
this idea supposes that patients can tolerate a certain amount of uncertainty and that extra vigilance is required by the clinician to ensure that they are given the tools and information they need to engage in decision making.30 effectively , extra care is taken in those situations of greater uncertainty to provide information and to ensure that the patient understands . 
this protects autonomy and increases patient trust in the long run . also , addressing underlying emotions , hopes , and fears is an effective way to ensure good communication and informed consent . 
a conversation analysis found that patients who are more assertive draw more empathy from their oncologists , whereas passive patients elicited much less emotional reciprocation from the oncologists.39 clinicians may use open - ended questions , such as , id like to switch gears and check in to see how you are feeling about all of this technical information ? or more closed - ended questions , such as , many patients may feel overwhelmed by all of the scientific information weve discussed ; im wondering if that is true for you ? in addition , checking understanding and emotional reactions enhances the clinician - patient relationship and is key in the setting of uncertainty . directly focusing on the therapeutic aspects of the relationshipby assessing communication preference , checking understanding , and searching for underlying emotional issuesdevelops rapport and may bolster patients resilience in the face of clinical uncertainty . 
the clinician may say something such as : im wondering if there is anything that might be difficult for you to discuss with me ? is there anything that i might be able to do to make this better for you ? or i have a sense that you are someone who likes x , y , and z ; please help me understand if i am correct . 
realigning goals may be accomplished by saying something such as : it is my goal to provide you with the best information for us to make a decision that works for you ; please let me know if that is also your goal or if youd like to focus on additional issues . this human connection dimension of medical care is needed to withstand the uncertainty . 
clinicians frequently underestimate the therapeutic power of their relationships with patients.40 a strong therapeutic bond is fundamental , not simply useful.41 patients have varying abilities to trust , hope , and have faith in their clinicians . 
the relationship is strengthened by focusing on agreed - upon common goals and tasks.32 it is always appropriate to discuss the nuts and bolts of the therapeutic relationship , especially when the clinician perceives that it may not be firmly established or upon entering areas of clinical uncertainty that are inherent in the precision medicine era . summary precision medicine presents a new era of communication in oncology . 
this article has presented some of the common patient reactions to precision medicine and basic communication issues in oncology . communication can be used to enhance rapport , trust , and support . 
zachariae r , pedersen cg , jensen ab , et al : association of perceived physician communication style with patient satisfaction , distress , cancer - related self - efficacy , and perceived control over the disease . 
blanchette ps , spreafico a , miller fa , et al : genomic testing in cancer : patient knowledge , attitudes , and expectations . cancer 120 : 3066 - 3073 , 2014 35 . 
politi mc , studts jl , hayslip jw : shared decision making in oncology practice : what do oncologists need to know ? oncologist 17 : 91 - 100 , 2012 38 . 
kenny da , veldhuijzen w , weijden tv , et al : interpersonal perception in the context of doctor - patient relationships : a dyadic analysis of doctor - patient communication . 
differences in the relative fractions of immune cell subpopulations between immune - rich er - positive and tnbcs3 suggested disparate immunotherapy strategies in the two immune - rich subsets . concerning the study of tnbc immune microenvironment , we recently observed the existence of at least three immune - clusters ( im ) in tnbcs by computing transcriptional - based deconvolution algorithms.4 ima , considered hot or t cell - inamed , shows greater enrichment of cytotoxic t cells , inferred by deconvolutions tools or by histologic til counts , and accounts for approximately 30% of the tnbcs analyzed . 
finally , imc was described as warm tumors , because intrinsic immune activities are effectively mounted , but tumors are able to escape and suppress such responses , as indicated by the greater abundance of tregs and the lower expression of pdl - 1 and pd - 1 compared with ima . 
on the basis of our ndings , we would like to comment that besides the heterogeneity of tnbcs in terms of immune - cell inltration , the immune - rich subtype represents immune - related transcriptional heterogeneity , with signicant implications for potential immunotherapeutic strategies . consistent with the genomic characterization of immune - cell inltration obtained in our tnbc cohort , the incidence of immune - enriched ima in tcga and metabric data sets does not exceed 30% ( fig 1a ) , supporting the reproducibility of our immune clusters , especially for hot tumors . 
 ( a ) proportion of immuno - clusters ( im ) previously reported in romero et al4 with the ital - mex , molecular taxonomy of breast cancer international consortium ( metabric ) , and the cancer genome atlas ( tcga ) datasets . 
 ( b ) donut plot of the percentage of immuno - clusters among tumors classied as immune - rich or non - immune - rich from the tcga and metbric cohorts . 
by applying cluster analysis of our immune clusters to tcga and metabric data sets , we found that immune - rich tnbcs ( high til metagene described by omeara et al1 ) are composed mainly of ima ( n = 160 , 62% ) , followed by imc ( n = 54 , 21% ; fig 1b ) , with cases categorized as imb ( n = 44 , 17% ) also present . 
when considering the distribution of high til metagenes ( top 25th percentile ) applied by omeara et al1 in our cohort ( ital - mex , n = 158 ) and classied according to immune - related clusters , we conrmed that immune - rich cases ( ima ) are almost exclusively integrated by high til metagene tumors ( n = 41 , 94% )  . however , we also observed that a relevant percentage of high til cases are also distributed among imc ( n = 17 , 32% ) and less represented in the cold imb immune cluster ( n = 11 , 18% ; fig 1c )  . 
omeara t , marczyk m , qing t , et al : immunological differences between immune - rich estrogen receptor - positive and immune - rich triple - negative breast cancers . 
 a rationale and design of the targeted agent and profiling utilization registry study purpose case reports and small prospective trials suggest that administering targeted therapies to patients with advanced cancer and an identified genomic target may be associated with clinical benefit . 
the targeted agent and profiling utilization registry ( tapur ) study , a phase ii prospective , nonrandomized , multibasket pragmatic clinical trial , aims to identify signals of drug activity when us food and drug administration approved drugs are matched to prespecified genomic targets in patients with advanced cancer , outside of approved indications . methods patients eligible to participate in tapur are age 12 years and have advanced measurable or evaluable solid tumors , multiple myeloma , or b - cell non - hodgkin lymphoma . 
secondary end points include safety , progression - free survival , and overall survival . results more than 1 , 000 participants have thus far been registered , and more than 800 have been treated with a tapur study drug . 
two study cohorts have permanently closed to enrollment because of lack of antitumor activity , and 12 have expanded to the second stage of enrollment after promising preliminary activity . conclusion the tapur study will describe the efficacy and toxicity of the targeted drugs used outside of their approved indications when matched to a somatic genomic variant . evidence is building through reports of clinical trials , case reports , and clinical anecdotes to suggest that patient outcomes may be improved when a targeted agent is matched to a genomic alteration present in a patients tumor.1 - 6 clinical reports to date suggest that 30% to 80% of advanced solid tumors harbor potentially actionable genomic variants.7 - 10 in a meta - analysis of 570 phase ii studies of new anticancer agents , schwaederle et al11 examined response rate ( rr ) , progression - free survival ( pfs ) , and overall survival ( os ) for 32 , 149 patients who received a personalized treatment strategy versus those who did not . 
 of the md anderson cancer center experience of genomic profiling of patients with solid tumors with advanced disease , the impact ( initiative for molecular profiling and advanced cancer therapy ) study . 
the moscato - 01 ( molecular screening for cancer treatment optimization ; clinicaltrials.gov identifier : nct01566019 ) trial enrolled patients with treatment - resistant progressive metastatic cancers with lesions accessible to biopsy to perform genomic profiling.14 this study compared pfs using therapy based on genomic assessment with pfs for the most recent therapy during which the patient had experienced disease progression . 
le tourneau et al17 published the results of a randomized phase ii trial comparing therapy on the basis of tumor molecular profiling versus physician choice of therapy in patients with refractory cancer . 
this article will describe the rationale and design of the targeted agent and profiling utilization registry ( tapur ) study , a large pragmatic precision medicine basket trial with the overarching goal of describing the efficacy and toxicity of targeted anticancer drugs used outside of their approved indications for treatment of patients with advanced cancer based on a tumor genomic profile . methods objectives the primary objective of tapur is to evaluate the antitumor activity of commercially available targeted anticancer drugs used outside of their fda - approved indications for treatment of patients with advanced solid tumors , multiple myeloma , or b - cell non - hodgkin lymphoma with a genomic alteration known to be a drug target . 
secondary objectives include determination of pfs , os , and safety . design the tapur study is a phase ii prospective , nonrandomized , open - label clinical trial that aims to define signals of drug activity . 
list of available tapur study treatments for adults and pediatric patients study drug population to which available adults and children age 12 - 17 years adults only adults and children age 12 - 17 years adults and children age 16 - 17 years adults and children age 13 - 17 years adults and children age 12 - 17 years adults and children age 16 - 17 years adults only adults and children age 12 - 17 years adults and children age 12 - 17 years adults and children age 12 - 17 years nivolumab + ipilimumab adults only pembrolizumab adults and children age 12 - 17 years axitinib bosutinib cetuximab crizotinib dasatinib erlotinib olaparib palbociclib regorafenib sunitinib temsirolimus trastuzumab + pertuzumab adults only vemurafenib + cobimetinib adults only vismodegib adults and children age 12 - 17 years note . 
the study includes participants as young as 12 years of age with a tumor harboring a genomic alteration known to be a target of or to predict sensitivity to at least one of the 16 therapeutic options available in the study ( table 1 )  . 
eligible participants must have a tumor genomic variant identified on a test performed in a laboratory that has certification under the clinical laboratory improvement amendments and accreditation by the college of american pathologists . 
patients are matched to at least one of the available study treatments through a set of protocol - defined genomic matching rules or after review of a participant case by the tapur molecular tumor board ( mtb )  . 
the study uses simons optimal two - stage design for cohort analysis . tapur was designed independently by asco staff and volunteer leaders , with input from patient advocates , community - based investigators , the initial collaborating pharmaceutical companies , and the asco cancer research committee . 
the study was registered on clinicaltrials.gov ( nct02693535 ) before study launch . a data and safety monitoring board ( dsmb ) , consisting of a group of independent experts not involved in the conduct of tapur , meets biannually to monitor the study data and outcomes . 
 their primary functions include assessing the safety and efficacy of study treatments , safeguarding the interests and safety of trial participants , and ensuring that study results are both credible and reported to the medical community in a timely manner . 
for expanded cohorts , it will review all final cohort analyses and make recommendations regarding release of the cohort data . study population and recruitment the pragmatic approach of tapur allows for broad eligibility criteria , including eastern cooperative oncology group performance status of 0 to 2 , age 12 years , prior malignancies or positive hiv status , and previously treated but clinically stable brain metastases . 
tapur inclusion and exclusion criteria comport fully with recently published recommendations by asco and friends of cancer research for broadening eligibility criteria for cancer clinical trials.23 participating sites include both academic and community centers . study treatment decision once a potential participant is identified , the clinical site obtains informed consent and registers the participant in the tapur electronic data capture ( edc ) platform as shown in figure 1 . 
if a study drug is identified and the drug - specific inclusion and exclusion criteria are met , the clinical site completes the drug specific informed consent process and enrolls the participant in the study . 
 a screening consent general eligibility criteria met registration treatment 1 treatment 2 , continued tapur matching to study drug ( s ) based on genomic criteria ( or approved by mtb ) treatment decision by treating physician target variant 1 target variant 2 screening continued drug - specific eligibility criteria met tumor type 1 tumor type 2 tumor type 1 tumor type 2 enrolled and placed into cohorts enrollment cohort 1 cohort 2 cohort 3 cohort 4 fig 1 . 
the mtb , composed of clinical oncologists , molecular pathologists , and patient advocates , reviews the genomic test results , pathology reports , and clinical histories of submitted patient cases and identifies potential treatment matches among the study treatments . 
of the patient cases reviewed by the mtb , approximately 65% resulted in identification of a study drug option . permitted at the discretion of the treating physician in accordance with the recommended dose modifications contained in the approved prescribing information . 
management of aes is performed according to institutional standards of care , informed by the package insert . tumor measurements and radiologic evaluations and evaluation of clinical disease status are performed every 8 weeks after initiation of treatment for the first 16 weeks , and then every 12 weeks if the treatment continues , and at the end of study treatment , if possible . 
study treatment is continued until progressive disease is documented . after progression of disease during any study treatment , participants may be reassessed to determine eligibility for treatment with another study drug after a minimum of 30 days has elapsed from the last dose of the previous drug and any aes have resolved to grade 2 or stabilized . 
all general and drug - specific eligibility criteria must be reconfirmed , and the participant must sign a new drug - specific consent form . treatment schedule and interval of evaluations ae and sae criteria study treatments are administered according to the recommended starting dose and schedule described in the package insert of each drug . 
events not resolved at the end of study treatment require follow - up every 30 days until the event resolves to ctcae grade 2 . tapur requires reporting of ctcae grade 3 to 4 aes that are possibly , probably , or definitely related to the study treatment , whether expected or not . 
all saes , regardless of grade , relatedness to study drug , or expectedness , must also be reported , including all deaths . end points the primary end point is objective response at 8 weeks or sd documented at 16 weeks . 
tapur study milestones date milestone march 14 , 2016 study launch at 37 clinical site locations with 14 study drugs first participant registered ( consented ) first participant enrolled ; two additional drugs added for total of 16 study drugs additional drug added for total of 17 study drugs 100th participant registered november 2016 100th participant enrolled march 2016 april 2016 may 2016 august 2016 april 2017 june 2017 august 2017 september 2017 november 2017 december 2017 february 2018 march 2018 33 clinical sites added for total of 70 locations 500th participant registered additional therapy added for 19 study drugs first cohort reaches stage one 500th participant enrolled 1 , 000th participant registered 10th cohort reaches stage one 43 clinical sites added for total of 113 locations abbreviation : tapur , targeted agent and profiling utilization registry . the basis of the presence , absence , or unequivocal progression of the lesions . 
participants who have no tumor evaluation beyond baseline and are alive with no signs of progressive disease at the time of leaving the study will be replaced in their cohort with another participant . secondary end points include grade 3 to 5 aes and saes , pfs , response duration , and os . 
the null hypothesis is that the probability of objective response or sd of at least 16 weeks duration is 15% , versus the alternative hypothesis that it is at least 35% . 
after 28 participants in the cohort have been observed for the primary outcome , if seven or more participants achieve objective response or sd of at least 16 weeks duration , the null hypothesis will be rejected , and we will declare that the study drug is active in the cohort of participants defined by tumor type and genomic alteration . 
this design has a 54% chance of early stopping if the null hypothesis is true . estimates of the rr and 95% ci will be presented for each cohort upon closure ( at either stage one or stage two ) .24 the kaplan - meier method will be used to estimate the duration of response , pfs , and os distributions . results table 3 summarizes key study milestones . 
figure 2 also shows the distribution of genomic targets by tumor type ( fig 2b ) and study drug ( fig 2c ) , highlighting the heterogeneity of genomic targets and tumor types , resulting in 336 unique cohorts at the time of this writing . 
targeted agent and profiling utilization registry ( tapur ) study registration , enrollment , and cohort creation by ( a ) month , ( continued on next page ) many cancers that are driven by specific molecular alterations that can be targeted with drugs that inhibit aberrant signaling pathways in tumor cells . 
thus , the targeting of bcr - abl alterations in chronic myeloid leukemia , flt3 alterations in acute myeloid leukemia , egfr mutations and alk translocations in nonsmallcell lung cancer , braf mutations in melanoma and nonsmall - cell lung cancer , and human epidermal growth factor receptor 2 overexpression in breast and gastric cancers , among others , represent examples of the successful application of precision medicine approaches in clinical oncology that have extended the lives of many patients.1 , 25 - 30 interest in precision medicine has been further fueled by reported responses ranging from modest to exceptional when targeted treatments are selected based on large - scale genomic tumor profiling.5 the widespread availability of commercial next generation sequencing tests presents opportunities for patients who have exhausted standard treatment options to pursue treatments with investigational agents or approved drugs prescribed outside of their labeled indications . the tapur study stemmed from the recognition that the rapid dissemination of genomic profiling provides an opportunity to learn from the application of precision cancer medicine in practice while at the same time providing a framework for clinical decision support for clinical oncologists who are struggling to interpret the complex genomic data they now confront in practice . 
 b vegfr3 ( flt4 ) mutation , amplification , or overexpression vegfr1 ( flt1 ) mutation , amplification , or overexpression smo mutation lck mutation prkdc mutation pold1 mutation msh2 mutation vegfr3 ( flt4 ) mutation or amplification ewsr1nrya3 fusion cdk12 mutation ccnd3 bcr - abl mutation alk fusion or mutation msi high status egfr mutation rictor amplification vegfr1 ( flt1 ) mutation or amplification csf1r mutation or amplification vegfr2 ( kdr ) mutation , amplification , or overexpression vhl mutation or amplification ptch1 deletion or inactivating mutation mlh1 mutation tsc2 mutation pdgfra mutation or amplification palb2 mutation stk11 mutation vegfr2 ( kdr ) mutation or amplification ret mutation or amplification pdgfr ? mutation or amplification kit mutation atm mutation tsc1 mutation pole mutation fgfr3 mutation or amplification cdk6 amplification raf1 mutation or amplification pten mutation kit mutation or amplification braf mutation or amplification akt1 mutation flt3 mutation or amplification brca1 / brca2 mutation met amplification or mutation pik3ca mutation mtor mutation fgfr2 mutation or amplification ccnd1 amplification fgfr1 mutation or amplification cdk4 amplification atm mutation or deletion braf_v600e / d / k / r mutation erbb2 / erbb3 mutation , amplification , or overexpression kras , nras , and braf wild type ( all must be wild type ) germline or somatic brca1 / brca2 inactivating mutations high tumor mutational burden cdkn2a loss or mutation total fig 2 . 
 ( a ) april 2018 registration , enrollment , and cohort creation in progress at the time of this report ; ( b , c ) the number in each box indicates the number of patients . 
 c vegfr3 ( flt4 ) mutation , amplification , or overexpression vegfr1 ( flt1 ) mutation , amplification , or overexpression smo mutation lck mutation prkdc mutation pold1 mutation msh2 mutation vegfr3 ( flt4 ) mutation or amplification ewsr1nrya3 fusion cdk12 mutation ccnd3 bcr - abl mutation alk fusion or mutation msi high status egfr mutation rictor amplification vegfr1 ( flt1 ) mutation or amplification csf1r mutation or amplification vegfr2 ( kdr ) mutation , amplification , or overexpression vhl mutation or amplification ptch1 deletion or inactivating mutation mlh1 mutation tsc2 mutation pdgfra mutation or amplification palb2 mutation stk11 mutation vegfr2 ( kdr ) mutation or amplification ret mutation or amplification pdgfr ? mutation or amplification kit mutation atm mutation tsc1 mutation pole mutation fgfr3 mutation or amplification cdk6 amplification raf1 mutation or amplification pten mutation kit mutation or amplification braf mutation or amplification akt1 mutation flt3 mutation or amplification brca1 / brca2 mutation met amplification or mutation pik3ca mutation mtor mutation fgfr2 mutation or amplification ccnd1 amplification fgfr1 mutation or amplification cdk4 amplification atm mutation or deletion braf_v600e / d / k / r mutation erbb2 / erbb3 mutation , amplification , or overexpression kras , nras and braf wild type ( all must be wild type ) germline or somatic brca1 / brca2 inactivating mutations high tumor mutational burden cdkn2a loss or mutation total fig 2 . 
 ( continued ) ( c ) ibrance ( pfizer , new york , ny ) , lynparza ( astrazeneca , wilmington , de ) , sutent ( pfizer ) , keytruda ( merck , kenilworth , nj ) , torisel ( pfizer ) , erbitux ( eli lilly , indianapolis , in ) , perjeta ( genentech , south san francisco , ca ) , herceptin ( genentech ) , cotellic ( genentech ) , zelboraf ( genentech ) , opdivo ( bristol - myers squibb , new york , ny ) , yervoy ( bristol - myers squibb ) , stivarga ( bayer , whippany , nj ) , xalkori ( pfizer ) , sprycel ( bristol - myers squibb ) , erivedge ( genentech ) , inlyta ( pfizer ) , bosulif ( pfizer ) , and tarceva ( genentech )  . 
tapur study initial cohort expansions and closures study drug tumor type variant ovarian cancer kras , nras , and braf wild type colorectal cancer braf_v600e / d / k / r mutation breast cancer colorectal cancer germline or somatic brca1 / brca2 inactivating mutations atm mutation or deletion head and neck cancer soft tissue sarcoma malignant neoplasm of bronchus and lung cdkn2a loss or mutation cdk4 amplification cdkn2a loss or mutation breast cancer colorectal cancer uterine cancer high tumor mutational burden high tumor mutational burden high tumor mutational burden colorectal cancer erbb2 / erbb3 mutation , amplification , or overexpression expansion to stage two cetuximab cobimetinib + vemurafenib olaparib palbociclib pembrolizumab pertuzumab + trastuzumab sunitinib closed at stage one palbociclib breast cancer fgfr1 mutation or amplification pancreatic cancer malignant neoplasm of gallbladder and bile ducts cdkn2a loss or mutation abbreviation : tapur , targeted agent and profiling utilization registry . data collection , and discretion left to the treating physician regarding choice of which tumor biospecimen to interrogate and which genomic profiling test to use . 
however , tapur uses standard treatment response and toxicity criteria for assessment of efficacy and toxicity outcomes , structured data collection , protocol - specified evaluation times , and a standard simons twostage statistical design to assess the primary end point as well as an independent dsmb to provide recommendations on cohort expansion and closure . 
importantly , the study also provides educational opportunities and clinical decision support tools to treating physicians in the form of protocol - specified genomic matching rules and access to an mtb to assist in interpretation of genomic test reports . although study results are not yet available , preliminary information about the status of certain cohorts suggests that the study can provide meaningful information . 
 enrollment rates when the frequency of genomic targets was not well defined for many tumor types , identifying clinical launch sites that routinely used genomic profiling , arranging for drug distribution , and building an experienced clinical trial management team to operate the study . 
mangat no relationship to disclose susan halabi consulting or advisory role : tokai pharmaceuticals consulting or advisory role : eisai , bayer healthcare pharmaceuticals travel , accommodations , expenses : bayer healthcare pharmaceuticals suanna s . 
bruinooge no relationship to disclose elizabeth garrett - mayer stock and other ownership interests : abbott laboratories , abbvie consulting or advisory role : tactical therapeutics , okava pharmaceuticals ajjai alva consulting or advisory role : eisai , astrazeneca , genentech / roche speakers bureau : astrazeneca research funding : genentech ( inst ) , novartis ( inst ) , bristol - myers squibb ( inst ) , bind biosciences ( inst ) , acerta pharma ( inst ) , merck sharp & dohme ( inst ) , prometheus laboratories ( inst ) , covance ( inst ) , mirati therapeutics ( inst ) , united biosource ( inst ) , ariad pharmaceuticals ( inst ) , astrazeneca ( inst ) , pfizer ( inst ) , genentech / roche ( inst ) , hoosier cancer research network ( inst ) , bayer healthcare pharmaceuticals ( inst ) katherine a . 
stella no relationship to disclose emile voest consulting or advisory role : interna , biogeneration ventures research funding : novartis ( inst ) , glaxosmithkline ( inst ) , genentech / roche ( inst ) , pfizer ( inst ) , astrazeneca ( inst ) , eisai ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) kathleen j . 
kim honoraria : celgene , eli lilly , astrazeneca , boehringer ingelheim consulting or advisory role : eli lilly , celgene , astrazeneca , boehringer ingelheim travel , accommodations , expenses : eli lilly , celgene , astrazeneca , boehringer ingelheim richard l . 
kim , carolinas healthcare systems levine cancer institute , charlotte , nc ; ajjai alva , university of michigan ; jane perlmutter , gemini group , ann arbor ; philip j . 
janeway , data - farber / boston childrens cancer and blood disorders center , boston , ma ; emile voest , netherlands cancer institute , amsterdam , the netherlands ; and navin pinto , seattle childrens hospital , seattle , wa . 
wagle n , grabiner bc , van allen em , et al : activating mtor mutations in a patient with an extraordinary response on a phase i trial of everolimus and pazopanib . 
cobain ef , robinson dr , wu y - m , et al : clinical impact of high - throughput sequencing in patients with advanced cancer : lessons learned from the michigan oncology sequencing center . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
massard c , michiels s , fert c , et al : high - throughput genomics and clinical outcome in hardto - treat advanced cancers : results of the moscato 01 trial . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , openlabel , proof - of - concept , randomised , controlled phase 2 trial . 
cheson bd , fisher ri , barrington sf , et al : recommendations for initial evaluation , staging , and response assessment of hodgkin and non - hodgkin lymphoma : the lugano classification . 
barrington sf , mikhaeel ng , kostakoglu l , et al : role of imaging in the staging and response assessment of lymphoma : consensus of the international conference on malignant lymphomas imaging working group . 
kim es , bruinooge ss , roberts s , et al : broadening eligibility criteria to make clinical trials more representative : american society of clinical oncology and friends of cancer research joint research statement . 
druker bj , talpaz m , resta dj , et al : efficacy and safety of a specific inhibitor of the bcr - abl tyrosine kinase in chronic myeloid leukemia . 
slamon dj , leyland - jones b , shak s , et al : use of chemotherapy plus a monoclonal antibody against her2 for metastatic breast cancer that overexpresses her2 . 
bang yj , van cutsem e , feyereislova a , et al : trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of her2 - positive advanced gastric or gastrooesophageal junction cancer ( toga ) : a phase 3 , open - label , randomised controlled trial . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecular profiles : results from mypathway , an open - label , phase iia multiple basket study . 
butler , mph ; kuo guo , ms ; molly holoubek , ccrn ; samiha islam ; linda miller , msn , rn , ocn ; shamika ranasinghe , ms ; brittany m . 
 drug - related pneumonitis in the era of precision cancer therapy drug - related pneumonitis as a result of novel cancer therapy provides new challenges for providers of cancer care in the era of precision medicine . 
here , we provide a detailed review of drug - related pneumonitis that develops during precision cancer therapies using immune - checkpoint inhibitors and molecular targeting agents , and we summarize the emerging data that have been obtained by recent investigations to provide a state - of - the - art overview for clinicians involved in cancer care . we focus on immune - checkpoint inhibitorrelated pneumonitis , which is an immune - related adverse event of growing interest and increasing clinical significance in current oncology practice that has rapidly expanding access to these agents . 
clinical characteristics , radiographic spectrum , and risk factors and outcome of pneumonitis are described for each class of agents , and current treatment guidelines and monitoring recommendations are discussed . 
with recent advances in precision cancer therapy using molecular targeting agents and immune - checkpoint inhibitors ( icis ) , pneumonitis in patients who are treated with novel anticancer agents is increasingly recognized as a significant clinical challenge . 
in addition , rapidly expanding access to icis , such as programmed death 1 ( pd - 1 ) and programmed death - ligand 1 ( pd - l1 ) inhibitors has brought new and emerging challenges . 
recent studies of pneumonitis in patients who are treated with these novel agents have provided important new knowledge and insight that are relevant to cancer care providers across disciplines . this review focuses on drug - related pneumonitis during precision cancer therapies , including icis and molecular targeting agents , and provides an overview for clinicians who are involved in the care of patients with cancer . 
the spectrum of radiographic manifestations of pneumonitis is presented in the context of patient management . we also provide up - to - date guidelines and recommendations for the treatment and monitoring of pneumonitis during these therapies . 
 been made to characterize the radiographic patterns of pneumonitis caused by various therapeutic agents.1 , 2 several recent reports have indicated that the radiographic patterns of drug - related pneumonitis may be categorized according to patterns that correspond to american thoracic society / european respiratory society ( ats / ers ) classifications of idiopathic interstitial pneumonias and related disorders , 3 which are based on ct findings and their extent and distributions on imaging.2 , 4 - 8 in these studies of pneumonitis that developed during treatment with molecular targeting agents and icis , the commonly noted radiographic patterns of pneumonitis included cryptogenic organizing pneumonia ( cop ) pattern , nonspecific interstitial pneumonia ( nsip ) pattern , hypersensitivity pneumonitis ( hp ) pattern , and acute interstitial pneumonia ( aip ) / acute respiratory distress syndrome ( ards ) pattern2 , 4 - 10 ( table 1 )  . 
radiographic patterns of pneumonitis have been shown to correlate with the toxicity grades assessed by the common terminology criteria for adverse events.5 recent advances in precision cancer therapy have brought the new and emerging challenges of pneumonitis as a result of treatment with novel agents . 
regulatory approvals for these agents have recently been granted , including nivolumab for melanoma , nonsmall - cell lung cancer ( nsclc ) , renal cell carcinoma ( rcc ) , and hodgkin lymphoma ; pembrolizumab for melanoma , nsclc , hodgkin lymphoma , and squamous cell head and neck cancer ; and atezolizumab for urothelial carcinoma and nsclc . 
combination therapy of nivolumab and ipilimumab , a cytotoxic t - lymphocyte - associated protein 4 inhibitor , has also been approved for treatment of advanced melanoma and is actively investigated in nsclc and other malignancies . as a result , these agents are rapidly expanding their treatment roles in clinical oncology practice , and more agents are in the drug development and testing pipeline . immune - checkpoint inhibition of these agents is associated with a unique set of toxicities that are known as immune - related adverseevents ( iraes ) .11 - 14 among a variety of iraes that can affect organs from head to toe , ici - related pneumonitis is a clinically significant and potentially life - threatening irae and is therefore recognized as an event of special interest . phase i trials of pd - 1 inhibitors have resulted in pneumonitis - related deaths in patients with advanced solid tumors , including nsclc , melanoma , and colorectal cancer.15 - 18 in a report of long - term safety in a nsclc cohort that was treated in a phase i trial , pneumonitis occurred in 7% ( 9 of 129 patients ) , with three pneumonitisrelated deaths.15 in a phase ii trial of nivolumab in squamous nsclc , pneumonitis was one of the most common iraes , occurring in 5% of patients ( 6 of 117 patients ) , including four patients with grade 3 pneumonitis.19 more recent data suggest that pneumonitis can be an even more significant issue in patients who are treated with combination therapies . 
radiographic pattern was associated with clinical severity of pneumonitis represented by toxicity grades , where aip / ards pattern had the highest grade , followed by cop pattern , whereas nsip pattern and hp pattern had lower grade ( median grade : 3 , 2 , 1 , 1 ) .5 results indicate that the radiographic patternbased approach , in addition to early and accurate diagnosis , may help guide patient management and follow - up in the setting of pneumonitis . 
another recent study of pd - 1 / pd - l1 inhibitor - related pneumonitis has also reported the diverse radiographic and pathologic features of the entity , 25 further indicating the importance of a standardized common language to describe the findings of ici - related pneumonitis.10 treatment , clinical course , and management guidelines treatment of ici - related pneumonitis consists mainly of holding back on the use icis and administering corticosteroids ; however , some cases may be refractory to corticosteroids and require additional treatment . 
 ( d ) aip / ards pattern is characterized by diffuse or multifocal ggos or consolidations , along with lung volume loss and traction bronchiectasis . ( n = 12 ) or as intravenous therapy ( n = 5 )  . 
although the cause of death was solely attributed to pneumonitis in one patient alone , the serious outcome in 12% ( 5 of 43 ) of patients again emphasizes the clinical significance of the entity.25 twelve patients were retreated with icis after complete clinical resolution of initial pneumonitis , and three patients experienced recurrent pneumonitis , which again resolved by drug holding ( n = 1 ) or oral corticosteroids ( n = 2 ) as in the course of their initial pneumonitis treatment.25 a recently published guideline of pneumonitis management is in agreement with the observations in these reports.31 the guideline recommends oral corticosteroid treatment , including prednisone 1 to 2 mg / kg / d or methylprednisolone 0.5 to 1 mg / kg / d in mild to moderate cases . 
in mild to moderate cases , bronchoscopy is recommended to exclude infectious etiologies before starting immunosuppression.31 in severe cases , hospitalization is necessary , with treatment to include high - dose corticosteroids , such as methylprednisolone 2 to 4 mg / kg / d , and additional immunosuppression , including mycophenolate mofetil , cyclophosphamide ; infliximab can be administered if necessary.31 although limited to a small percentage of patients , an additional unique phenomenon of pneumonitis flare has been reported where ici - related pneumonitis recurs after the termination of corticosteroid taper and in the absence of ici retreatment after the initial episode of pneumonitis has been successfully treated ( fig 2 )  . 
this was first reported in a patient with nsclc who was treated with commercial nivolumab and who experienced pneumonitis.6 the patient was successfully treated with corticosteroids for the initial pneumonitis ; however , the patient experienced another episode of pneumonitis after completing corticosteroid taper without resuming pd - 1 inhibitor therapy or starting any other therapy , indicating a pneumonitis flare.6 although similar to the initial presentation both clinically and radiographically , flare pneumonitis tends to be more severe and extensive than the initial episode . 
such a phenomenon has not been described in the setting of pneumonitis related to other anticancer agents and this that indicates the clinical course of icirelated pneumonitis may be more complex than other drug - related pneumonitis in some patients . in a series of 20 patients with ici - related pneumonitis , one patient with lymphoma experienced two episodes of pneumonitis flare in which pneumonitis came back with similar but more extensive radiographic presentations compared with the initial episode after completion of corticosteroid taper without pd - 1 retreatment5 ( fig 2 )  . 
this observation further confirms the phenomenon , which is likely unique to iraes and may involve autoimmune mechanisms . unmet clinical needs that require additional investigations although several recent reports provide important knowledge and observations of ici - related pneumonitis , significant knowledge gaps still exist for this emerging entity . 
because early and accurate diagnosis is key for this mostly treatable conditionwith good response to corticosteroids in the majority of the casesadditional studies are needed to identify risk factors and early markers for pneumonitis to improve diagnostic accuracy . treatment and clinical management guidelines need to be further optimized as the immuneoncology community accumulates the experience of this entity . 
pneumonitis with a cryptogenic organizing pneumonia ( cop ) pattern in a 33 - year - old female with hodgkin lymphoma who was treated with nivolumab and ipilimumab combination therapy , with a recurrence during retreatment ( 2a ; ah ) and two episodes of pneumonitis flare after completion of corticosteroid taper ( 2b ; ah )  . 
reprinted with permission from nishino et al.5 2a : ( a and b ) computed tomography ( ct ) scan of the chest at 1.4 months of therapy demonstrated ground - glass and reticular opacities and consolidations with multifocal distribution , which are indicative of a cop pattern of pneumonitis ( arrowheads )  . 
 ( 2b : a and b ) the patient completed 2 months of corticosteroid taper , and after 1 month , experienced another episode of pneumonitis with a similar radiographic pattern , without nivolumab retreatment or other systemic therapy , which indicated a pneumonitis flare . 
 ( 2b : e and f ) the 2.7 - month course of corticosteroid taper was completed , and after 2 weeks , the patient again developed a pneumonitis flare with a similar radiographic pattern as prior episodes . 
findings included lymphocyte - predominant interstitial pneumonitis ( arrowhead , 2b [ g ] , hematoxylin and eosin stain , 3200 ) with rare eosinophils ( arrow , 2b [ g ] ) , and areas of organizing pneumonia with fibroblast plugs and foamy macrophages filling the airspaces ( asterisks , 2b [ h ] , hematoxylin and eosin stain , 3200 )  . 
the patient started another course of prednisone taper with subsequent clinical improvement and is schedule for a follow - up ct scan . in addition , awareness of pneumonitis related to icis other than pd - 1 / pd - l1 inhibitors is becoming increasingly important . 
everolimus is approved for the treatment of several cancers , including advanced rcc , advanced pancreatic neuroendocrine tumors ( nets ) , subependymal giant cell astrocytomas , and advanced hormone receptorpositive , human epireceptor 2negative dermal growth factor breast cancer ( in combination with exemestane )  . 
temsirolimus is approved for the treatment of advanced rcc . drug - related pneumonitis is a recognized class effect toxicity of mtor inhibitors and has been described in detail in the context of advanced rcc treatment . 
in a study by maroto et al , 34 among 178 patients with rcc who were treated with singleagent temsirolimus , 52 ( 29% ) had radiographically identified drug - related pneumonitis . 
of these , 16 patients ( 31% ) had respiratory symptoms at the time of the onset of radiographically detected pneumonitis , whereas others ( 36 of 52 ; 69% ) were asymptomatic and thus may not be clinically diagnosed for pneumonitis . 
the estimated cumulative probability of radiologically identified drug - related pneumonitis was 21% ( 95% ci , 15% to 29% ) at 8 weeks , 31% ( 95% ci , 24% to 40% ) at 16 weeks , and 45% ( 95% ci , 36% to 57% ) at 13 months.34 another study of 46 patients with rcc who were treated with temsirolimus or everolimus reported that 14 patients ( 30% ) developed drug - related pneumonitis.35 median time of the onset of radiologic manifestations of pneumonitis was 56 days ( range , 31 to 214 days )  . 
these 14 patients more frequently achieved stable disease than did others , which indicates a possibility of pneumonitis as a treatment benefit marker.35 reports of mtor inhibitorrelated pneumonitis in tumors other than rcc indicate a somewhat different incidence of pneumonitis according to tumor types . 
radiographic patterns of mtor inhibitorrelated pneumonitis have been characterized in patients with wm and in those with advanced net.7 , 8 in both cohorts , the most common findings were bilateral ground - glass opacities ( ggos ) and reticular opacities , sometimes with consolidations , in a peripheral and lower distribution . 
cop pattern was the leading pattern observed in the majority of cases ( 70% in wm and 57% in net ) , followed by nsip pattern ( 30% in wm and 36% in net ) , whereas one patient in the net cohort demonstrated the hp pattern.7 , 8 similar imaging manifestations are noted in other cohorts with mtor inhibitor related pneumonitis.34 , 35 recognition of the characteristic radiographic patterns of pneumonitis during mtor inhibitor therapy helps with the early detection and accurate diagnosis of this entity . clinical management of mtor inhibitorrelated pneumonitis mostly depends on the severity of clinical symptoms . 
egfr - tki therapy should be discontinued , and systemic corticosteroids are usually administered.49 although egfr - tkirelated pneumonitis has mostly been a specific concern among the japanese population and has often had a low clinical impact in other populations , a recent observation from a trial of a novel ici and third - generation egfr - tki , osimertinib , raises a new concern in the setting of combination therapy . 
 agents may limit , in part , the destructive remodeling of the lung and impair the lungs ability to respond to injury.37 , 49 , 52 these possible mechanisms are also likely modified by various host and environmental factors , which further complicates the issue.52 likewise , risk factors for pneumonitis need to be defined , especially for ici - related pneumonitis , to allow for optimal patient selection with regard to treatment safety . 
the risk of recurrent pneumonitis after reintroduction of therapy is another important debate for these agents , as they may be the only available or effective therapy for patients with advanced cancers.5 , 37 the impact of radiotherapy on pneumonitis is a major topic , given a number of ongoing combination therapy trials that use ici and radiotherapy.53 in some studies of patients with advanced nsclc who were treated with egfr - tkis , prior thoracic irradiation and concomitant radiotherapy have been noted as risk factors for pneumonitis.49 , 54 although the exact effect of radiotherapy on ici - related pneumonitis awaits additional data , prior chest radiation has influenced the radiographic appearance of pd - 1 pneumonitis in patients with lymphoma , which indicates a need for caution in treatment monitoring.30 prior reports have often focused on radiation to the chest ; however , radiotherapy in the extrathoracic sites may require more attention given the concept of abscopal effects , which are increasingly discussed in the context of ici and radiation treatment.53 in the clinical setting , drug - related pneumonitis is ultimately a diagnosis of clinical correlation and exclusion , and there is no specific test for the entity.55 among various lung conditions that can affect patients with advanced cancer who undergo systemic therapy , infection is an important differential diagnosis that should be excluded before starting corticosteroid therapy . 
fiberoptic bronchoscopy is helpful for this purpose as it allows for targeted and deep sampling of specimens for microbiology , cytology , and histology via bronchoalveolar lavage and transbronchial biopsy.55 a minority of patients may present with respiratory distress in the absence of radiographic confirmation , thereby leading to delays in appropriate management . 
of note , some of the findings of pneumonitis , such as ggos , are not adequately evaluated on chest radiographs , and thus diagnostic chest ct scans are needed to sensitively detect and fully characterize the lung abnormalities in the setting of suspected pneumonitis . in conclusion , knowledge of drug - related pneumonitis has increasingly emerged in recent investigations , providing important clues for accurate diagnosis , patient management , and monitoring . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . mizuki nishino honoraria : bayer yakuhin consulting or advisory role : bristol - myers squibb , worldcare clinical , toshiba medical systems research funding : merck ( inst ) drug - related pneumonitis in the era of precision cancer therapy the following represents disclosure information provided by authors of this manuscript . 
stephen hodi employment : dana - farber cancer institute consulting or advisory role : merck sharp & dohme , novartis , genentech , amgen , emd serono research funding : bristol - myers squibb ( inst ) , merck sharp & dohme ( inst ) , genentech ( inst ) , novartis ( inst ) patents , royalties , other intellectual property : patent pending as per institutional policy , patent pending royalties received on mica - related disorders application to institution per institutional policy travel , accommodations , expenses : novartis , bristol - myers squibb other relationship : bristol - myers squibb , genentech nikhil h . 
travis wd , costabel u , hansell dm , et al : an official american thoracic society / european respiratory society statement : update of the international multidisciplinary classification of the idiopathic interstitial pneumonias . 
nishino m , chambers es , chong cr , et al : anti - pd - 1 inhibitor - related pneumonitis in nonsmall - cell lung cancer . cancer immunol res 4 : 289 - 293 , 2016 7 . 
nishino m , brais lk , brooks nv , et al : drug - related pneumonitis during mammalian target of rapamycin inhibitor therapy in patients with neuroendocrine tumors : a radiographic pattern - based approach . 
nishino m , boswell en , hatabu h , et al : drug - related pneumonitis during mammalian target of rapamycin inhibitor therapy : radiographic pattern - based approach in waldenstr om macroglobulinemia as a paradigoncologist 20 : 1077 - 1083 , 2015 9 . 
nishino m , tirumani sh , ramaiya nh , et al : cancer immunotherapy and immune - related response assessment : the role of radiologists in the new arena of cancer treatment . 
weber js , dummer r , de pril v , et al : patterns of onset and resolution of immune - related adverse events of special interest with ipilimumab : detailed safety analysis from a phase 3 trial in patients with advanced melanoma . 
gettinger sn , horn l , gandhi l , et al : overall survival and long - term safety of nivolumab ( anti - programmed death 1 antibody , bms - 936558 , ono - 4538 ) in patients with previously treated advanced nonsmall - cell lung cancer . 
rizvi na , mazi`eres j , planchard d , et al : activity and safety of nivolumab , an anti - pd - 1 immune checkpoint inhibitor , for patients with advanced , refractory squamous nonsmall - cell lung cancer ( checkmate 063 ) : a phase 2 , single - arm trial . 
rizvi na , hellmann md , brahmer jr , et al : nivolumab in combination with platinum - based doublet chemotherapy for first - line treatment of advanced nonsmall - cell lung cancer . 
nishino m , giobbie - hurder a , hatabu h , et al : incidence of programmed cell death 1 inhibitor - related pneumonitis in patients with advanced cancer : a systematic review and meta - analysis . 
fehrenbacher l , spira a , ballinger m , et al : atezolizumab versus docetaxel for patients with previously treated nonsmall - cell lung cancer ( poplar ) : a multicentre , open - label , phase 2 randomised controlled trial . 
rittmeyer a , barlesi f , waterkamp d , et al : atezolizumab versus docetaxel in patients with previously treated nonsmall - cell lung cancer ( oak ) : a phase 3 , open - label , multicentre randomised controlled trial . 
antonia s , goldberg sb , balmanoukian a , et al : safety and antitumour activity of durvalumab plus tremelimumab in nonsmall cell lung cancer : a multicentre , phase 1b study . 
ghobrial im , gertz m , laplant b , et al : phase ii trial of the oral mammalian target of rapamycin inhibitor everolimus in relapsed or refractory waldenstr om macroglobulinemia . 
dabydeen da , jagannathan jp , ramaiya n , et al : pneumonitis associated with mtor inhibitors therapy in patients with metastatic renal cell carcinoma : incidence , radiographic findings and correlation with clinical outcome . 
soria jc , shepherd fa , douillard jy , et al : efficacy of everolimus ( rad001 ) in patients with advanced nsclc previously treated with chemotherapy alone or with chemotherapy and egfr inhibitors . 
janne pa , gurubhagavatula s , yeap by , et al : outcomes of patients with advanced nonsmall cell lung cancer treated with gefitinib ( zd1839 , iressa ) on an expanded access study . 
lynch tj , bell dw , sordella r , et al : activating mutations in the epidermal growth factor receptor underlying responsiveness of nonsmall - cell lung cancer to gefitinib . 
burotto m , manasanch ee , wilkerson j , et al : gefitinib and erlotinib in metastatic nonsmall cell lung cancer : a metaanalysis of toxicity and efficacy of randomized clinical trials . 
kudoh s , kato h , nishiwaki y , et al : interstitial lung disease in japanese patients with lung cancer : a cohort and nested case - control study . 
gemma a , kudoh s , ando m , et al : final safety and efficacy of erlotinib in the phase 4 polarstar surveillance study of 10 708 japanese patients with nonsmall - cell lung cancer . 
ding pn , lord sj , gebski v , et al : risk of treatment - related toxicities from egfr tyrosine kinase inhibitors : a metaanalysis of clinical trials of gefitinib , erlotinib , and afatinib in advanced egfr - mutated nonsmall cell lung cancer . j thorac oncol 12 : 633 - 643 , 2017 49 . 
min jh , lee hy , lim h , et al : drug - induced interstitial lung disease in tyrosine kinase inhibitor therapy for nonsmall cell lung cancer : a review on current insight . 
ahn m , yang j , yu h , et al : osimertinib combined with durvalumab in egfr - mutant nonsmall cell lung cancer : results from the tatton phase ib trial . 
hotta k , kiura k , tabata m , et al : interstitial lung disease in japanese patients with nonsmall cell lung cancer receiving gefitinib : an analysis of risk factors and treatment outcomes in okayama lung cancer study group . 
we completely agree with the authors that better ways of selecting patients with melanoma for snb are required , because approximately 80% of patients who currently have an snb are found to be sn negative . 
improved methods of identifying those at low risk of being sn positive are needed so that they are not unnecessarily subjected to the procedure , while those at higher risk are not excluded . bellomo et al1 propose that using their gene expression prole ( gep ) test will achieve greater accuracy , but we are not convinced that this is correct . 
first , we have several concerns about the statistical methodology used in their study to support the claim that a combination of two clinicopathologic ( cp ) features and an eight - gene test ( a cp - gep model ) improves the accuracy of selecting patients for snb . and second , we have evidence that prognostic estimates of sn status equivalent to or better than those provided by the cp - gep model of bellomo et al1 can be achieved using readily available cp parameters only . one of our statistical concerns is that the study had a relatively small sample size of patients who underwent snb ( n = 754 ) and only 128 were sn positive . the small sample size used for model development may explain why there was no apparent improvement in performance when more complex cp models were used compared with the use of breslow thickness and age only . another statistical concern is that the model reported by bellomo et al1 was assessed only by internal crossvalidation , and external validation was not performed . this is important , because there is a high probability that external validation using an unrelated data set will demonstrate a reduced discrimination ( c statistic ) compared with the development set because models tend to overt the data set on which they were developed.2 the apparent gain in discrimination achieved by the cp - gep model relative to the memorial sloan kettering cancer center ( mskcc ) nomogram ( from 77% to 82% ) is therefore likely to be is externally validated . reduced when the model furthermore , the c statistics had considerable overlap , and there is no evidence that there was a statistically signicant improvement . the 95% cis of in addition , the reported snb reduction rate reported by bellomo et al1 is based upon a negative predictive value ( npv ) threshold of 95% . 
however , the npv of any test decreases as the prevalence of the condition increases ; thus , in practice , it cannot be xed.3 therefore , it would be more informative for both clinicians and patients to indicate the rate reductions of snb with individual risk thresholds rather than the npv . the above statistical concerns , regardless of question of whether the gep test improved prognostic accuracy remains . 
it should be noted that the c statistic obtained by using the mskcc nomogram was considerably higher in the report by bellomo et al1 than in both our study and the original mskcc study , 5 which probably reects selection bias in their study sample that excluded thick tumors . 
the 5% absolute improvement in the c statistic reported in their study combining cp parameters ( two only ) and molecular risk factors ( an eight - gene test ) is less than the 6.2% achieved by our new model , which used cp parameters only . for all of the above reasons , we are not convinced that the addition of gep to cp parameters improves the reliability of sn - positivity estimates . 
scolyer , phd melanoma institute australia and faculty of medicine and health , the university of sydney , sydney , and department of tissue oncology and diagnostic pathology , royal prince alfred hospital and nsw health pathology , camperdown , nsw , australia john f . 
scolyer employment : royal prince alfred hospital consulting or advisory role : bristol myers squibb , glaxosmithkline , merck sharp & dohme , neracare , novartis amgen , myriad genetics , qbiotics research funding : the ainsworth foundation ( inst ) , national health and medical research council travel , accommodations , expenses : bristol myers squibb , novartis john f . 
bellomo d , arias - mejias sm , ramana c , et al : model combining tumor molecular and clinicopathologic risk factors predicts sentinel lymph node metastasis in primary cutaneous melanoma . 
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wong sl , kattan mw , mcmasters km , et al : a nomogram that predicts the presence of sentinel node metastasis in melanoma with better discrimination than the american joint committee on cancer staging systeann surg oncol 12 : 282 - 288 , 2005 6 . 
scolyer ra , judge mj , evans a , et al : data set for pathology reporting of cutaneous invasive melanoma : recommendations from the international collaboration on cancer reporting ( iccr )  . 
 impact of the spop mutant subtype on the interpretation of clinical parameters in prostate cancer purpose molecular characterization of prostate cancer , including the cancer genome atlas , has revealed distinct subtypes with underlying genomic alterations . 
one of these core subtypes , spop ( speckle - type poz protein ) mutant prostate cancer , has previously only been identifiable via dna sequencing , which has made the impact on prognosis and routinely used risk stratification parameters unclear . methods we have developed a novel gene expression signature , classifier ( subclass predictor based on transcriptional data ) , and decision tree to predict the spop mutant subclass from rna gene expression data and classify common prostate cancer molecular subtypes . 
we then validated and further interrogated the association of prostate cancer molecular subtypes with pathologic and clinical outcomes in retrospective and prospective cohorts of 8 , 158 patients . results the subclass predictor based on transcriptional data model showed high sensitivity and specificity in multiple cohorts across both rna sequencing and microarray gene expression platforms . 
we found that the spop mutant subclass was associated with lower frequency of positive margins , extraprostatic extension , and seminal vesicle invasion at prostatectomy ; however , spop mutant cancers were associated with higher pretreatment serum prostate - specific antigen ( psa )  . 
despite high pretreatment psa , the spop mutant subtype was associated with a favorable prognosis with improved metastasis - free survival , particularly in patients with high - risk preoperative psa levels . conclusion using a novel gene expression model and a decision tree algorithm to define prostate cancer molecular subclasses , we found that the spop mutant subclass is associated with higher preoperative psa , less adverse pathologic features , and favorable prognosis . 
2018 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license : introduction prostate cancer is a clinically and molecularly heterogeneous disease.1 - 4 current risk stratification guidelines , such as those from the national comprehensive cancer network , 5 the american urological association / american society for therapeutic radiology and oncology , 6 and the european association of urologyeuropean society for radiotherapyoncologyinternational society of geriatric oncology7 use clinical and pathologic parameters , including the level of prostate - specific antigen ( psa ) , to guide management decisions for clinically localized disease . 
psa is also used in a number of other clinical scenarios in prostate cancer , including initial diagnosis , monitoring for recurrence after primary therapy , and monitoring disease burden and treatment response for metastatic disease . the emerging next - generation dna and rna sequencing data point toward distinct molecular subclasses of prostate cancer , 2 - 4 , 8 , 9 but their clinical impact remains unclear . 
 genome atlas ( tcga ) study identified seven core prostate cancer subtypes , which were defined by underlying genomic alterations.4 one key molecular subclass , which represents approximately 10% of prostate cancers , harbors recurrent missense mutations in the e3 ubiquitin ligase component spop.2 - 4 , 10 - 13 to date , identification of spop mutations has required mutational analysis using genomic ( dna ) sequencing . 
in contrast , gene expression ( rna ) data are widely available from a variety of prostate cancer cohorts , often with the long follow - up necessary to define prognostic impact.14 - 21 here , we reported the first development and validation of the subclass predictor based on transcriptional data ( scapt ) model , which we used to define key prostate cancer molecular subclasses , including spop mutant cancer , using gene expression data . 
we used the scapt model to predict the molecular subclass from a retrospective cohort that included 1 , 626 patient samples and a prospective cohort that included 6 , 532 samples using genome - wide microarray gene expression data from a clinically available prognostic assay ( decipher ; genomedx biosciences , vancouver , bc , canada ) , and we explored the clinicopathologic and prognostic associations of key molecular subclasses of prostate cancer . methods prostate cancer tumor samples and microarray data we used a total of 8 , 559 radical prostatectomy ( rp ) tumor expression profiles for training , testing , and validation . 
for training and testing , we used rna sequencing expression and dna mutation data from tcga prostate cancer project ( n = 333 ) 4 and the weill cornell medicine ( wcm ) sequencing ( n = 68 ) cohort . 
for validation , expression profiles of retrospective ( n = 1 , 626 ) and prospective ( n = 6 , 532 ) cohorts were derived from the decipher genomics resource information database ( grid ) registry ( clinicaltrials.gov identifier : nct02609269 )  . 
 the retrospective grid cohort was pooled from seven published microarray studies : cleveland clinic , 22 erasmus mc , 23 johns hopkins , 15 memorial sloan kettering cancer center , 1 mayo clinic ( mayo i and mayo ii ) , 20 , 24 and thomas jefferson university.21 the prospective grid cohort was from clinical use of the decipher test . 
dna and rna from the tcga and wcm cohorts were extracted from fresh frozen rp tumor tissue , as previously described.4 rna from the grid cohorts was extracted from routine formalin - fixed , paraffin - embedded rp tumor tissues , amplified , and hybridized to human exon 1.0 st microarrays ( thermo fisher scientific , waltham , ma ) .24 , 25 spop mutant transcriptional signature we developed the spop mutant transcriptional signature , which includes 212 genes differentially expressed between spop mutant and wild - type samples from tcga prostate cancer rna sequencing data4 ( fig 1 )  . 
the overlap between two methods was significant ( p < 2.2 1016 ) , which confirmed similar results when applying these methods . scapt development on the basis of spop mutant transcriptional signature and the support vector machine model to predict tumors in the spop mutant subclass in the absence of dna sequencing datathat is , microarray data setswe developed the scapt model on the basis of the support vector machine ( svm ) model.28 - 30 given a set of training data marked with two categories , svm builds a model that assigns testing data into one category or the other , which makes it a nonprobabilistic binary linear classifier ( fig 2a )  . 
 ( a ) spop mutant transcriptional signature that included 212 differentially expressed genes between spop mutant and wild - type samples from the cancer genome atlas ( tcga ) non - ets fusion rna sequencing ( rna - seq ) data . 
 ( b ) significant enrichment of spop mutant case from 68 weill cornell medicine ( wcm ) prostate cancer samples with spop mutant transcriptional signature on the basis of hierarchical clustering . 
erg , erg - fusion position ; ets : other ets fusion positive ; fdr , false - discovery rate . z - scores of spop mutant signature from tcga cohort . 
 by performing 10 - fold cross - validation on the tcga training data set , we found costcost of constraints violationequal to 0.04 to yield the model with the highest sensitivity and specificity . 
next , using a decision tree and previously developed microarray - based classifiers for the erg - positive and ets - positive subtypes , 25 we classified the remaining cases in each cohort . 
high accuracy and confidence of spop mutant ( spopmut ) subclass prediction on weill cornell medicine ( wcm ) and gene expression omnibus ( geo ) data set by the scapt ( subclass predictor based on transcriptional data ) model . 
data from taylor et al , 1 erho et al , 24 and kelin et al.22 wt , wild type . spopwt spopmut support vectors large margin spop other taylor et al ( n = 150 ) erho et al ( n = 545 ) klein et al ( n = 182 ) prediction : spopmut sensitivity , 89% ; specificity , 95% spopwt spop wild type combined cohort to test the statistical association between spop mutant status and clinical variables , including age , race , preoperative psa , gleason score , lymph node invasion , surgical margin status , extracapsular extension , and seminal vesicle invasion . 
we evaluated the associations between spop mutant status and patient outcomes , including biochemical recurrence , metastasis , and prostate cancerspecific mortality , on the basis of kaplan - meier analysis . 
as spop mutations are mutually exclusive with erg and other ets rearrangements , 13 we excluded prostate cancer samples with ets fusions to define spop mutantspecific gene expression effects ( fig 1a )  . 
among those 212 genes , we found that upregulated genes from the spop mutant subgroup were enriched in transport vesicle membrane and oxidoreductase activity , but that there was no significant enriched function in downregulated genes from the spop mutant subgroup ( data supplement )  . 
in this independent cohort , we found significant enrichment ( p < 1.9103 ) of spop mutant tumors in one subcluster based on unsupervised clustering ( fig 1b and data supplement )  . 
we next used the spop mutant transcriptional signature in a locked svm modelthat is , with fixed parameters on the basis of the training step using the tcga cohort ( see methods ) to generate scores for each sample in the wcm cohort . 
the spop mutant prediction and its impacts on clinical and prognostic outcomes from retrospective ( n = 1 , 626 ) and prospective grid ( n = 6 , 532 ) cohorts . 
 ( a ) the pie chart of predicted molecular subclasses from the retrospective cohort with 1 , 626 samples , on the basis of the scapt ( subclass predictor based on transcriptional data ) model and decision tree . 
 ( c ) the pie chart of predicted molecular subclasses from the prospective grid cohort with 6 , 532 samples , on the basis of the scapt model and decision tree . 
erg , erg - fusion position ; ets , other ets fusion positive ; or , odds ratio ; psa , prostate - specific antigen . the grid microarray expression data , which do not have spop mutation annotation from dna analysis . 
between 9% and 15% of samples in the cohorts were predicted as spop mutant subclass , which is consistent with the known prevalence of spop mutations at the genomic level in previous prostate cancer studies3 , 4 , 10 , 12 ( fig 2b )  . 
overall , these results demonstrated that the scapt model predicted spop mutant subclass on the basis of the transcriptional data with high accuracy and confidence . molecular subtyping of 8 , 158 patients using the scapt and decision tree we applied the scapt model and decision tree to 8 , 158 patients from retrospective and prospective grid cohorts . 
among the retrospective cohort with 1 , 626 rp specimens , we predicted 9% ( range , 2% to 13% ) of samples to be spop mutant subclass ( data supplement )  . 
among the prospective cohort with 6 , 532 rp specimens , we predicted 8% of cases to be spop mutant subclass , 41% as erg positive , 12% as ets positive , 39% as other subtype , and 1% as conflict cases ( fig 3c )  . 
 the percentage of each molecular subclass was consistent with that reported in previous prostate cancer studies , 1 - 4 , 14 , 25 which supports the validity of our approach . spop mutant subclass associated with favorable pathology at rp we used binominal univariable analysis to compare clinical and pathologic characteristics between spop mutant and wild - type subclasses ( figs 3b and 3d )  . 
spop mutant subclass was less likely to harbor adverse pathologic features , such as positive surgical margins , extraprostatic extension , and seminal vesicle invasion , compared with wild - type subclass in both retrospective and prospective cohorts ( figs 3b and 3d )  . 
these data suggest that the spop mutant subclass was associated with more favorable pathologic outcomes at rp , but expresses higher levels of psa and was associated with tumors from older men , whereas the opposite was true in the erg - positive subclass of prostate cancer . consistent association between spop mutation and higher psa in multiple cohorts the inverse association of psa and prognosis in specific prostate cancer subtypes has potential clinical implications . 
to independently validate the association of spop mutant status and higher preoperative psa , we examined multiple distinct rp cohorts ( grid , tcga , taylor , and wcm )  . 
we observed a similar trend of higher preoperative psa in spop mutant cases , and the spop mutant subclass was more enriched in the higher psa subgroups ( psa > 10 ; fig 4a )  . 
on univariable analysis across cohorts , spop mutant status was significantly associated with higher preoperative psa ( fig 4b ) , whereas erg fusion status was significantly associated with lower preoperative psa ( fig 4c )  . spop mutation is associated with favorable clinical outcomes after rp on kaplan - meier analysis , the spop mutant subclass had the highest biochemical - free , metastasis - free , and lowest prostate cancer specific mortality compared with erg - positive , ets - positive , and other subtypes in the retrospective grid cohort ( fig 5b and data supplement )  . 
whereas long - term outcomes were not available for the prospective grid cohort , we evaluated the association with metastasis risk using the decipher score , a validated metric for prostate cancer metastatic potential.22 , 24 , 37 , 38 we found fewer spop mutant tumors in the decipher high - risk score ( > 0.6 ) group compared with the lowand average - risk groups ( data supplement ) , which again is consistent with a favorable prognosis subtype . 
together , these data support that spop mutant prostate cancer had favorable prognosis after rp , despite its association with higher preoperative psa . favorable prognosis in high - risk psa subgroup in the spop mutant subclass pretreatment psa level is a standard component of risk stratification for prostate cancer , with a psa level > 20 ng / ml considered to be high risk by a number of risk assessment methods.39 - 41 consistent with this , higher psa was associated with worse metastasis - free survival and prostate cancerspecific mortality in the retrospective cohorts ( fig 5a ) ; however , spop mutant status had a dramatic effect on prognosis within the subgroup of patients with high psa . 
 among patients with a psa level > 20 ng / ml , spop mutant tumors were associated with better clinical outcomes , which were comparable to the lowest psa subgroup ( psa < 10 ng / ml ; fig 5d )  . 
 ( a ) enrichment of spopmut cases among higher psa subgroups from prospective grid , the cancer genome atlas ( tcga ) , taylor , and weill cornell medicine ( wcm ) cohorts . 
 ( a ) clinical outcome difference between lower , average , and higher psa groups via kaplan - meier analyses for metastasis ( met ) and prostate cancerspecific mortality ( pcsm ) free survival rates . 
 society of geriatric oncology guidelines for clinically localized prostate cancer5 - 7 classify patients with a pretreatment psa level of > 20 as high risk , even in the absence of other adverse prognostic features . 
this results in increased treatment burden , and it is recommended that patients classified as high risk who opt for radiotherapy undergo 2 to 3 years of concurrent androgen - deprivation therapy compared with a duration of 4 to 6 months for patients with intermediate risk disease . 
knowledge of the molecular subtype of prostate cancer and its impact on psa level could therefore improve risk stratification , sparing unnecessary treatment burden and directing higher - intensity therapy to patients who are truly at higher risk ; however , whether molecular subtype will actually add clinical value to the current risk stratification toolsor if it adds additional information compared with such tests as decipherremains unclear . 
additional studies will be necessary to optimally deploy these strategies clinically , but it is clear that molecular subtyping should be considered in future clinical trial designs . recent advances in technology have increased our understanding of molecular subclasses of prostate cancer , but clinical and biologic differences among the key erg - positive , ets - positive , and spop mutant subclasses remain poorly understood . 
biologically , prostate cancer cells that harbor mutant spop may produce more psa on a per - cell basis as a result of enhanced androgen transcription , essentially leading to higher psa from fewer cancer cells , whereas the opposite may be true from erg - positive tumors . 
these hypotheses need to be rigorously tested in future functional and clinical studies . as a result of the retrospective nature of the cohorts and small sample size of case cohort studies , survival analysis was inevitably affected by baseline risk . 
although the favorable prognosis was consistent with improved clinical outcomes in the spop mutant subclass , these survival results need to be independently validated in additional clinical trials to be generalizable . in conclusion , we have developed the scapt model to predict spop mutant subclass purely on the basis of transcriptional data with high confidence and accuracy . 
we believe this work not only builds a prediction model for spop mutant prostate cancers and expands the data types usable for the interrogation of clinical outcomes , but it also reinforces the concept that molecular subtyping of prostate cancer can alter the interpretation of the current standard of care risk stratification methods . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . deli liu no relationship to disclose mandeep takhar employment : genomedx mohammed alshalalfa employment : genomedx nicholas erho employment : genomedx jonathan shoag no relationship to disclose travel , accommodations , expenses : genomedx robert b . 
rubin research funding : eli lilly , janssen pharmaceuticals bruce trock consulting or advisory role : genomedx consulting or advisory role : myriad genetics research funding : myriad genetics , mdxhealth eric a . 
den consulting or advisory role : genomedx speakers ' bureau : bayer research funding : medivation , astellas pharma , genomedx travel , accommodations , expenses : genomedx scott a . 
tomlins leadership : strata oncology stock and other ownership interests : strata oncology consulting or advisory role : abbvie , janssen pharmaceuticals , astellas pharma , medivation , strata oncology , sanofi , almac diagnostics research funding : astellas pharma ( inst ) , medivation ( inst ) , genomedx ( inst ) patents , royalties , other intellectual property : coauthor on a patent issued to the university of michigan on ets gene fusions in prostate cancer travel , accommodations , expenses : strata oncology daniel e . 
spratt no relationship to disclose elai davicioni employment : genomedx leadership : genomedx stock and other ownership interests : genomedx patents , royalties , other intellectual property : cancer diagnostics using biomarkers 20140066323 travel , accommodations , expenses : genomedx andrea sboner no relationship to disclose christopher e . 
barbieri patents , royalties , other intellectual property : coinventor on a patent application filed regarding spop mutations in prostate cancer by weill cornell medicine travel , accommodations , expenses : genomedx acknowledgment ashley e . 
ross stock and other ownership interests : genomedx honoraria : healthtronics consulting or advisory role : healthtronics research funding : metamark genetics we thank the patients with prostate cancer and families who contributed to this research . 
barbieri , newyork - presbyterian hospital , new york , ny ; mandeep takhar , mohammed alshalalfa , nicholas erho , and elai davicioni , genomedx bioscience , vancouver , british columbia , canada ; robert b . 
johnson mh , ross ae , alshalalfa m , et al : spink1 defines a molecular subtype of prostate cancer in men with more rapid progression in an at risk , natural history radical prostatectomy cohort . 
ross ae , johnson mh , yousefi k , et al : tissue - based genomics augments post - prostatectomy risk stratification in a natural history cohort of intermediateand high - risk men . 
nguyen pl , haddad z , ross ae , et al : ability of a genomic classifier to predict metastasis and prostate cancer - specific mortality after radiation or surgery based on needle biopsy specimens . 
spratt de , yousefi k , deheshi s , et al : individual patient - level meta - analysis of the performance of the decipher genomic classifier in high - risk men after prostatectomy to predict development of metastatic disease . 
karnes rj , bergstralh ej , davicioni e , et al : validation of a genomic classifier that predicts metastasis following radical prostatectomy in an at - risk patient population . 
klein ea , yousefi k , haddad z , et al : a genomic classifier improves prediction of metastatic disease within 5 years after surgery in node - negative high - risk prostate cancer patients managed by radical prostatectomy without adjuvant therapy . 
boormans jl , korsten h , ziel - van der made aj , et al : identification of tdrd1 as a direct target gene of erg in primary prostate cancer . 
bennett kp , campbell c : support vector machines : hype or hallelujah ? sigkdd explor 2 : 113 , 2000 technol 2 : 1 - 27 , 2011 30 . 
fine sw , gopalan a , leversha ma , et al : tmprss2 - erg gene fusion is associated with low gleason scores and not with high - grade morphological features . 
zhou ck , young d , yeboah ed , et al : tmprss2 : erg gene fusions in prostate cancer of west african men and a meta - analysis of racial differences . 
schaefer g , mosquera jm , ramoner r , et al : distinct erg rearrangement prevalence in prostate cancer : higher frequency in young age and in low psa prostate cancer . 
font - tello a , juanpere n , de muga s , et al : association of erg and tmprss2 - erg with grade , stage , and prognosis of prostate cancer is dependent on their expression levels . 
marrone m , potosky al , penson d , et al : a 22 gene - expression assay , decipher ( genomedx biosciences ) to predict five - year risk of metastatic prostate cancer in men treated with radical prostatectomy . 
cooperberg mr , pasta dj , elkin ep , et al : the university of california , san francisco cancer of the prostate risk assessment score : a straightforward and reliable preoperative predictor of disease recurrence after radical prostatectomy . 
damico av , whittington r , malkowicz sb , et al : biochemical outcome after radical prostatectomy , external beam radiation therapy , or interstitial radiation therapy for clinically localized prostate cancer . 
 high - content biopsies facilitate molecular analyses and do not increase complication rates in patients with advanced solid tumors purpose precision oncology relies on frequent pathologic , molecular , and genomic assessments of tumor tissue to guide treatment selection , evaluate pharmacodynamic effects of novel agents , and determine drug resistance mechanisms . 
it remains unknown how the need for serial biopsies with large numbers of tumor cores relates to tissue yields and biopsy complication rates . materials and methods in this study , we performed a retrospective analysis of 199 focal liver biopsies performed in 143 patients in the setting of oncologic research protocols ( research biopsy group ) over a 4 - year period at a single - intervention oncology service . 
practice patterns and complication rates were compared with those related to 1 , 522 consecutive biopsies performed in 1 , 154 patients in whom two cores were obtained for standard clinical management of patients ( standard biopsy )  . results in the research biopsy group , 1 , 100 tissue cores ( average , 5.5 cores per procedure ) were harvested and distributed to trial sponsors , internal research laboratories , and pathology services . 
in the standard biopsy control group , major complications were observed in 1.4% of procedures ( 22 of 1 , 522 ) and minor complications in 0.2% ( three of 1 , 522 )  . 
2017 by american society of clinical oncology introduction precision oncology aims to adapt treatment decisions based on the molecular characteristics of an individual tumor , thereby increasing the chance for a successful clinical outcome.1 tumors are increasingly being classified into subsets based on molecular profile with corresponding tailored treatment . 
there are substantial data demonstrating metastatic tissue can harbor unique genomic alterations compared with the primary tumor , and heterogeneity can also be seen among different metastatic sites in the same patient.2 , 3 it is generally accepted that the use of genomics and biomarkers substantially increases the success rate of clinical trials while lowering their cost.4 despite the rapid emergence of liquid biopsies ( eg , circulating tumor dna , 5 exosomes , circulating tumor cells ) , image - guided , minimally invasive biopsies remain the gold standard in procuring sufficient malignant tissue for molecular analysis . there are several reasons for sampling increasing amounts of tissue more frequently : the realization that tumors can adapt rapidly to therapeutic pressures and that molecular analysis of progression site biopsy , rather than primary specimen , is crucial to identify mechanisms of resistance ; the nathan e . 
 increasing use of immunotherapy trials where treatment response assessment can be difficult by imaging ( eg , pseudoprogression ) ; the emergence of more sophisticated analytic models , including patient - derived tumor cell lines and xenografts , requiring additional tissue ; the fact that a single biopsy core ( 10 mm3 ) maximally contains 30 million cells but often much fewer because of stroma and other factors ; and as a precautionary method to ensure that genomic analysis is indeed possible , because results can help with potential selection of matched targeted therapy . 
for example , in a large recent federal trial of personalized cancer medicine , 13% of tumor biopsy samples could not be used for genomic analysis.6 a recent trend in image - guided biopsies has therefore been to collect more cores ( four to 10 cores ) than necessary for traditional pathology workup ( eg , one to two cores )  . additional cores can be harvested with the use of coaxial systems that allow repeat 18 - gauge samples to be obtained through a hollow needle placed under image guidance . 
with such an approach , consecutive tissue fragments can then be used for immunohistochemistry , fluorescence in situ hybridization analysis , genomic analysis , protein and phosphoprotein biomarker testing , and establishment of patient - derived models , including cell lines , organoids , and mouse xenografts.7 these multicore biopsies , which we herein term highcontent biopsies ( hcbx ) , are thus attractive in initiating and evaluating genotype - centric drug trials and may be critically important for comprehensive genomic and proteomic analyses . 
with increased core sampling , a critical question remains : is there an increased complication rate associated with more extensive tissue harvesting ? data on the safety of research biopsies are limited , 8 , 9 in part because such data are typically not reported in clinical trials , and there is no standard consensus for the reporting of adverse events.10 the technical success rates of obtaining adequate cores after repeat sampling are largely unpublished , although anecdotal reports describe potential reduction in sample quality after repeat sampling.11 furthermore , performing biopsies within research protocols requires more complex logistics , with dedicated personnel and workflows . the main goal of this study was to evaluate if the increased number of cores obtained for research biopsies was associated with increased complication rates or decreased sample quality . 
to address these questions , we performed a retrospective analysis of focal tumor biopsies in the liver performed in the setting of specific oncologic research protocols at a single institution over a 4 - year period . 
practice patterns and complication rates were compared with those of 1 , 522 consecutive biopsies performed in 1 , 154 patients for standard clinical management during the same time period . 
of these , 199 biopsies were performed in 143 patients in the setting of oncologic research protocols ( research biopsy group ) ; 1 , 522 were performed in 1 , 154 patients for standard clinical management ( standard biopsy group )  . in the standard biopsy group , patients were referred from their oncologists directly to the interventional oncology service . 
these cores were placed in formalin and sent to pathology for standard processing : hematoxylin and eosin staining , immunohistochemistry as needed , and , more recently , molecular testing ( snapshot or foundation medicine [ fm ] , as discussed in pathology analysis ) when requested by referring oncologists . for research biopsies , however , a dedicated staff research coordinator was responsible for coordinating the entire process : arranging for the biopsy scheduling , determining and discussing the number of cores needed with the interventional radiologist , and collecting the samples and distributing them to their appropriate destinations . 
this was performed according to a standard operating procedure ( sop ) associated with each research study in which these patients were enrolled and was prospectively logged in an institutional database . 
for research biopsies , a dedicated staff member ( biopsy coordinator ) is responsible for coordinating the entire process : arranging for the scheduling , discussing the number of cores , and collecting the samples and distributing them to their appropriate destinations . the most common workflow involves obtaining five cores : in formalin for pathology , including mutational analyses ; fixed in formalin for 6 to 24 hours and subsequently transferred to ethanol , to be sent to trial sponsor ; in fetal bovine serum ( fbs ) , for development of patientderived models and drug testing ; in formalin for intrainstitutional research laboratories ; and snap frozen for tissue bank . prior imaging coaxial biopsy research / clinical trial biopsy > 5 cores formalin formalin formalin snap frozen patient 1 - 2 cores analysis of : size location growth approach routine pathology tissue type ihc mutations analysis of : tissue type pathway analysis mutations drug response oncologist interventional radiologist biopsy coordinator the fourth in formalin for intra - institutional research laboratories ; and the fifth , which was snap frozen ( fig 1 )  . 
patients in the research group were consented for additional risk of bleeding and other complications . image - guided biopsy procedures all procedures were performed using 18 - gauge coaxial , semiautomatic needle biopsy cutting needles ( bard mission ; bard biopsy systems , tempe , az ) under imaging guidance . 
50 , 000 / ml and an international normalized ratio of prothrombin time , 1.5 for all patients undergoing liver biopsy . in the research biopsies , 54.3% of the procedures were performed using ultrasound guidance ( supersonic imagine , aix - en - provence , france ; hitachi aloka medical , tokyo , japan ) , and 45.7% were performed using computed tomography guidance ( general electrics , fairfield , ct )  . 
a total of 193 procedures were performed using moderate sedation ( intravenous use of fentanyl and midazolam ) , three biopsies were performed with general anesthesia or monitored anesthesia care , and three procedures were performed with local anesthetic only ( lidocaine )  . complication rates were determined by review of medical notes and imaging studies obtained up to 30 days after the procedure ( research biopsies ) and of a prospectively maintained departmental database ( research and standard biopsies ; hi - iq ; conexsys , lincoln , ri )  . 
complications were classified as major ( including all patients who required more therapy other than clinical support , required hospitalization , or experienced an unplanned increase in the level of care , permanent adverse sequelae , or death ) or minor ( others ) .13 we did not record intraprocedural pain scores , because a majority of patients received conscious sedation in a patient - focused manner and by different care providers . 
all patient cases with negative results were reviewed , and clinical and imaging follow - up was used to determine whether they were true or false negatives . pathology analysis a negative biopsy was defined as 0% tumor cells . when rare tumor cells were present , they were noted , and the diagnosis was positive for malignancy . 
this was performed in house with polymerase chain reaction ( pcr ) based assay ( pcr - snapshot14 ) or targeted nextgeneration sequencing ( ngs ) tumor genotyping assay ( ngs - snapshot ) .15 selected samples were sent to fm for a different comprehensive genomic profiling using ngs.16 statistical analysis descriptive statistics were used to summarize results . 
table 1 summarizes patient demographics . because of heterogeneity among the clinical trial protocols , the mean number of cores obtained in the research cohort varied ( fig 3a )  . 
for a majority of procedures ( n = 186 of 199 ; hcbx ) , a larger number of cores ( range , four to 10 ; mean , 5.7 cores ) was obtained . 
in a smaller characteristic age , years mean range male female cancer type breast lung colorectal other primary stage * complication minor major 57.9 28 - 84 60 ( 30.2 ) 139 ( 69.8 ) 68 ( 34.2 ) 55 ( 27.6 ) 26 ( 13.1 ) 50 ( 25.1 ) 1 ( 0.5 ) 5 ( 2.5 ) 3 ( 1.5 ) 190 ( 95.5 ) 2 ( 1.0 ) 1 ( 0.5 ) * patient cases of stage i to iii disease correspond to cases of intrahepatic cholangiocarcinoma or hepatocellular carcinoma ; patient cases of stage iv disease represent all other neoplasms . number of procedures ( n = 13 of 199 ) , fewer cores ( range , two to three ; mean , 2.8 cores ) were sufficient to satisfy trial requirements and / or research needs . sample processing and analysis the 1 , 100 cores were distributed to their appropriate destination by the research biopsy coordinator according to the sop of each study ( fig 3b ) ; 229 cores ( from 127 procedures ) were sent to trial sponsors , 121 cores ( from 110 procedures ) were sent for development of patient - derived cell lines , 466 cores ( from 192 procedures ) were sent to other in - house research laboratories for various studies , and 284 cores ( from 174 procedures ) were sent to standard pathology . 
among the procedures from which samples were sent to standard pathology ( n = 174 ) , molecular analysis was attempted on 73 : multiplex pcr - based snapshot in 13 , ngs - based snapshot in 39 , and foundationone in 19 ; two samples had insufficient tissue for molecular analysis . the success rates of different analyses for research biopsies are summarized in figure 3c . 
 ( a ) distribution of number of cores per biopsy ( median , five ; mean , 5.5 6 standard deviation , 1.5 ; range , two to 10 cores )  . 
of these , four were shown to be true negatives ( ie , no evidence of metastasis or persistent local response after treatment on followup ) and were excluded from the analyses of success for the different tests . 
of the evaluated parameters ( table 2 ) , none were clearly associated with either satisfactory or nondiagnostic samples . the complication rates in the standard biopsy cohort were similar , with major complications observed in 1.4% of procedures ( 22 of 1 , 522 )  . the major complications were hematomas requiring transfusion or intervention ( n = 15 ) , pneumothorax requiring chest tube ( n = 1 ) , hemobilia requiring endoscopic retrograde cholangiopancreatogram ( n = 1 ) , infection requiring admittance ( n = 1 ) and / or percutaneous drainage ( n = 1 ) , and death ( n = 3 ; all secondary to bleeding )  . 
the minor complication rate was 1.0% ( n = 2 ; both were hematomas managed conservatively : one patient with metastatic breast cancer [ seven cores ] and one with colorectal cancer [ five cores ] )  . image - guided biopsies have long played an important role in the management of cancer . 
these findings are not entirely unexpected , because we used a coaxial biopsy technique that allows for multiple cores to be harvested through a single coaxial needle , therefore minimizing the number of capsular punctures probably a factor for decreasing the risk of complications in biopsies.24 one evident finding of our study is the progressive increase of research biopsies over the study period . this is consistent with the increasing popularity of molecularly targeted trials , as well as the realization that hcbx are technically feasible and safe . 
it has already been reported that genetic analysis is contingent on sufficient material.6 accordingly , different methods of molecular analysis in our data had results that ranged from 79% ( fm ) to 100% ( pcr - based snapshot )  . although ngs can more efficiently detect a wider range of molecular aberrations , more material is needed compared with older pcrbased techniques . to streamline research biopsies and accommodate larger numbers of procedures , we implemented a specific workflow with dedicated staff for efficient communication among clinicians , researchers , trial sponsors , and interventional radiologists , as well as collection and distribution of samples . 
although we did not measure the exact length of time required for the procedures in this study , we had previously determined that additional core sampling only required a few minutes longer , unless the coaxial needle had to be repositioned because of poor sample material ( eg , necrotic core , cystic tumor , fragmented specimen )  . 
interestingly , in our experience , the order in which cores were harvested was not associated with lower success rates for pathology , contrary to prior published reports.11 the samples sent for cell - line creation had a lower success rate . 
although this may have been related to the sample volume , it may also have resulted from other variables beyond our control ( amount of tumoral cells required for successful cell - line creation , timing , distance , or personnel , among others )  . 
interestingly , however , within the samples that were used for cell - line creation , the number of cores was not associated with cellline creation success rate . our study was designed to answer simple questions : how successful are hcbx , and what is their complication rate ? this is of timely interest ; data on the safety of research biopsies are limited , because they are often not reported in clinical trials.10 as such , our study focused on so - called all comers in a large oncologic interventional care setting rather than on specific subsets of patients , biopsy sites , or operators . 
 3% pi3k - akt signaling pathway fgfr1 / 2 / 3 / 4 and fgf familiy mapk / ras signaling pathway cyclin - dependent kinase related tp53 egfr esr1 other negative fig 4 . 
the genomic abnormalities detected in our study were similar to those found in several large studies17 and reflect the study population involving breast , lung , and colorectal cancer and cholangiocarcinoma trials at our institution . 
mapk , mitogen - activated protein kinase ; pi3k , phosphatidylinositol 3 - kinase . thoracic lesions , and similar studies may be warranted for those cohorts . our study has several limitations . 
medical records were reviewed for complications exclusively in the research biopsy group , although this would , if anything , overestimate the relative risk of complications compared with that of standard biopsies . 
only data on liver biopsies were reviewed , and therefore , additional studies are required to verify if the conclusions apply to other organs frequently biopsied , such as lungs , lymph nodes , and bones . 
vadvala , aditya bardia , jeffrey engelman , peter r . mueller , dejan juric , ralph weissleder financial support : dejan juric , ralph weissleder administrative support : dejan juric , ralph weissleder provision of study material or patients : laura spring , dejan juric collection and assembly of data : nathan e . 
frenk , laura spring , alona muzikansky , mari mino - kenudson , amy ly , aditya bardia , dianne finkelstein , dejan juric , ralph weissleder manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors the field of blood - based biomarkers in oncology for disease monitoring and molecular analysis is rapidly evolving . 
liquid biopsies can be used to detect circulating extracellular vesicles25 or tumor cells within a blood specimen , providing a tool to monitor cancer noninvasively.26 similarly , a number of technologies have also been developed to identify and track tumor - specific mutations via circulating free dna in the blood and urine.5 as these technologies are further developed and validated , they might replace some of the tissue biopsies in certain research and clinical settings . however , tissue biopsies allow for sampling of specific lesions and evaluation of tissue architecture and the tumor microenvironment , including proteins , phosphoproteins , and varied cytokines . image - guided biopsies will therefore continue to remain important for phenotyping tumor responses , identifying tumor heterogeneity , identifying therapeutic resistance , and characterizing host responses in the era of immunotherapy and targeted therapies . 
additional advances in image - guided tumor sampling , including lower computed tomography doses , shorter image acquisition times , and systems for acquiring , processing , and analyzing smaller samples may further expand the use of hcbx . 
mueller consulting or advisory role : cook medical patents , royalties , other intellectual property : royalties from cook ( percutaneous catheters ) dejan juric consulting or advisory role : novartis , emd serono , eisai ralph weissleder consulting or advisory role : moderna therapeutics , alivio therapeutics , tarveda therapeutics , lumicell , t2 biosystems , bioanalytix acknowledgment we thank all members of the division of interventional and abdominal radiology who contributed to the review of cases and / or performing of biopsies , in particular steven dawson , md , ashraf thabet , md , ronald arellano , md , suvranu ganguli , md , avinash kambadakone , md , michael zalis , md , and omar zurkiya , md , phd . 
j clin oncol 31 : 1904 - 1911 , 2013 juric d , castel p , griffith m , et al : convergent loss of pten leads to clinical resistance to a pi ( 3 ) ka inhibitor . 
friedman aa , letai a , fisher de , et al : precision medicine for cancer with next - generation functional diagnostics . nat rev cancer 15 : 747 - 756 , 2015 8 . 
el - osta h , hong d , wheler j , et al : outcomes of research biopsies in phase i clinical trials : the md anderson cancer center experience . 
hopper kd , grenko rt , tenhave tr , et al : percutaneous biopsy of the liver and kidney by using coaxial technique : adequacy of the specimen obtained with three different needles in vitro . 
dias - santagata d , akhavanfard s , david ss , et al : rapid targeted mutational analysis of human tumours : a clinical platform to guide personalized cancer medicine . 
giorgio a , tarantino l , de stefano g , et al : complications after interventional sonography of focal liver lesions : a 22 - year single - center experience . 
babaei jandaghi a , lebady m , zamani aa , et al : a randomised clinical trial to compare coaxial and noncoaxial techniques in percutaneous core needle biopsy of renal parenchyma . 
im h , shao h , park yi , et al : label - free detection and molecular profiling of exosomes with a nano - plasmonic sensor . nat biotechnol 32 : 490 - 495 , 2014 26 . 
mody , md , ms2 introduction somatic mutations in b - cell lymphoma 6 ( bcl6 ) corepressor ( bcor ) are reported in solid and hematologic malignancies in adults and children . 
bcor mediates transcriptional repression through epigenetic modication believed to cause oncogenesis through both overexpression or loss of tumor suppressor function.1 it is found to affect multiple diverse downstream gene targets and plays a role in development and function across many tissue lineages , especially the cns.2 , 3 in pediatric malignancies , bcor - ccnb3 fusion is prominent in undifferentiated round cell sarcoma ( uds ) , which , until recently , was treated similarly to ewing sarcoma ( ews )  . 
now considered its own genetic entity , bcor - ccnb3 fusions are typically identied in uds using transcriptome sequencing ( rna - seq ) and are present in up to 14% of uds cases.4 , 5 internal tandem duplications in bcor are found in pediatric cns neuroepithelial tumors and clear cell sarcoma of the kidney , 6 , 7 and mutations are reported in rhabdomyosarcoma and diffuse intrinsic pontine glioma ( dipg ) .8 , 9 however , uncertainty remains regarding the genomic landscape and signicance of bcor alterations in pediatric malignancies . in this article , we describe bcor alterations identied in our integrative clinical sequencing ( ics ) cohort in patients with sarcoma and high - grade glioma ( hgg ) these alterations in and explore the landscape of publicly available databases . 
furthermore , we examine their histopathologic features and co - occurring genomic aberrations and propose prospective targeted treatment strategies . methods pediatric and young adult patients ( , 26 years ) described were consented and enrolled in a prospective , institutional review boardapproved ( hum# : ics trial pediatricmichigan oncology 00056496 ) sequencing ( peds - mioncoseq ) at c.s. 
details of the sequencing procedures and bioinformatics analyses have been previously described.10 briey , somatic mutations , copy number variants / alterations , insertions and deletions , gene fusions , and gene expression are analyzed.11 , 12 investigation of clinical relevance of somatic variants uses an integrated approach incorporating technical considerations , variant and patient - specic information , and published data . st judes pediatric cancer data portal ( pecan ) was used ( accessed january 2019 ) to explore bcor alterations in a larger cohort of pediatric patients . 
the pecan database is a pediatric cancer genome repository containing whole - genome sequencing , wholeexome sequencing , and rna - seq data on more than 4 , 300 patients . 
 mankuzhy et al of the 86 sarcoma cases sequenced at the time of this report , 18 osteosarcomas and ve malignant peripheral nerve sheath tumors did not contain bcor alterations . twenty - seven of the remaining 63 cases contained clinically relevant diagnostic fusions , one ( 3.7% ) of which ( pax3 - foxo1positive alveolar rhabdomyosarcoma ) also had a bcor alteration . 
of the 15 patients with dipg sequenced , three ( 20% ) harbored mutations in bcor . pathologic evaluation of the bcor - mutant sarcoma cases showed both round - cell ( ewing - like ) morphology and the recently recognized variant with spindle - cell sarcoma morphology.17 figure 1 shows noncohesive sheets of malignant round to ovoid cells , with primitive - appearing chromatin , high mitotic activity , and necrosis . 
there were interlacing short fascicles with whorled pattern and foci of somewhat epithelioid congurations around larger vessels , mimicking synovial sarcoma and malignant peripheral nerve sheath tumor . mitotic gures were also identied . 
vimentin immunostain was diffusely strongly positive , and cd99 was negative . review of the pecan data set revealed 16 patients with tumors harboring nonsynonymous bcor alterations , ranging in age from 2 to 21 years ( table 2 )  . 
of the nine hggs , six contained concurrent gfr alterations , including two egfr and four platelet - derived growth factor receptor a mutations . the frequency of bcor mutations of primary adult cancers in tcga was 15 of 393 ( 3.8% ) in sarcoma and two of 273 ( 0.7% ) in hgg , particularly gbm . 
in the mi - oncoseq data set with advanced or refractory adult patients , sarcoma had a bcor mutation frequency of three of 199 ( 1.5% ) and gbm one of 49 ( 2% )  . discussion through integrative analysis of a cohort of high - risk pediatric malignancies and review of other large genomic databases , our study further describes the frequency and distribution of bcor alterations in pediatric sarcoma and high - grade glial malignancies . 
we recognized a higher overall prevalence of bcor alterations in these pediatric malignancy subtypes compared with their adult counterparts , both in primary cases ( tcga ) and refractory / advanced cases ( mi - oncoseq )  . 
this could be explained by bcors role in embryonic stem - cell differentiation , hematopoiesis , and regulation of vertebrate laterality and germline bcor mutations causing lenz microphthalmia and oculofaciocardiodental syndromes , which display fig 1 . 
 ( d ) cd99 immunostain ( 20 ) is negative . phenotypically overlapping skeletal , cns , and ocular effects , supporting its pleotropic developmental function.1 , 3 , 18 our study shows relatively high prevalence of bcor alterations in pediatric hgg ( 17% ) and in pediatric sarcomas , which are negative for fusions and other pathognomonic molecular alterations ( 11% ) , emphasizing the need for ics analysis to better dene molecular subtypes of these cases . 
our study also conrms earlier observations of bcor alterations in fusion - positive and - negative alveolar rhabdomyosarcoma.19 , 20 however , our ics cohort did not detect any bcor alterations in classic ewsr1 - rearranged ews or osteosarcoma , as seen in pecan . previous research has suggested that the prognostic signicance of bcor alterations could be tissue and diagnosis specic , with bcor - mutant leukemia being associated with a worse prognosis and no survival difference detected when comparing bcor - ccnb3 and ews.4 , 21 , 22 however , because of our cohorts small sample size and a lack of availability of outcomes data in larger data sets , additional investigation is needed to truly dene prognostic signicance of bcor alterations , specically in hgg . a novel nding in our cohort is the high frequency ( 57% ) of concurrent bcor and gfr alterations . 
gfrs are typically expressed on cell surfaces and play important roles in cell growth , survival , angiogenesis , and metastasis.23 the concurrent gfr mutations seen in our cohort are all known to be gain - of - function mutations resulting in constitutive activation of the gfr pathway and increased cell proliferation.24 - 27 bcl6 depletion results in downregulation of kinases in the receptor tyrosine kinase pathway , suggesting a potential link between bcl6 and related proteins such as bcor with receptor tyrosine kinase signaling that could be further explored to determine the signicance of these mutations.28 the bcl6 / bcor previous research has suggested that complex could serve as a potential therapeutic target . reported downstream targets of bcor activity include bcl6 targets , hoxa cluster genes , notch homolog 1 targets , and sonic hedgehog effectors such as gli1 and gli2.2 , 29 - 31 bcor can interact with specic histone deacetylase of both class i and ii , which increases the repression of transcriptional activity.32 the effect of histone deacetylase inhibitors on tumors with bcor mutations warrants additional investigation to assess the biologic relevance of these interactions , particularly in patients with dipg who also harbor histone mutations . 
 bcor alterations in pediatric solid tumors molecular and genomic characterization of tumors can complement histology - based classications of human cancers.35 recognizing which alterations are clinically meaningful and developing effective targeted treatment strategies can further contribute to dening this new cancer routine genomic proling can taxonomy . identify potential drivers of oncogenesis and possible targetable aberrations that can stimulate development of novel investigations of therapeutic approaches and additional in addition , molecular mechanisms of cancer . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . chandan kumar patents , royalties , other intellectual property : royalty for um agr #3199.101 recurrent gene fusions in prostate cancer licensed to gen - probe , inc . no other potential conicts of interest were reported . references hum mol genet 16 : 1773 - 1782 , 2007 1 . 
hilton en , manson fdc , urquhart je , et al : left - sided embryonic expression of the bcl - 6 corepressor , bcor , is required for vertebrate laterality determination . gearhart md , corcoran cm , wamstad ja , et al : polycomb group and scf ubiquitin ligases are found in a novel bcor complex that is recruited to bcl6 targets . mol cell biol 26 : 6880 - 6889 , 2006 3 . 
plos one 3 : e2814 , 2008 kao yc , owosho aa , sung ys , et al : bcor - ccnb3 fusion positive sarcomas : a clinicopathologic and molecular analysis of 36 cases with comparison to morphologic spectrum and clinical behavior of other round cell sarcomas . 
am j surg pathol 42 : 604 - 615 , 2018 peters tl , kumar v , polikepahad s , et al : bcor - ccnb3 fusions are frequent in undifferentiated sarcomas of male children . 
mod pathol 28 : 575 - 586 , 2015 argani p , kao y - c , zhang l , et al : primary renal sarcomas with bcor - ccnb3 gene fusion : a report of 2 cases showing histologic overlap with clear cell sarcoma of kidney , suggesting further link between bcor - related sarcomas of the kidney and soft tissues . 
am j surg pathol 41 : 1702 - 1712 , 2017 sturm d , orr ba , toprak uh , et al : new brain tumor entities emerge from molecular classication of cns - pnets . 
cell 164 : 1060 - 1072 , 2016 cramer sl , miller al , pressey jg , et al : pediatric anaplastic embryonal rhabdomyosarcoma : targeted therapy guided by genetic analysis and a patient - derived xenograft study . 
mackay a , burford a , carvalho d , et al : integrated molecular meta - analysis of 1 , 000 pediatric high - grade and diffuse intrinsic pontine glioma . 
tirode f , surdez d , ma x , et al : genomic landscape of ewing sarcoma denes an aggressive subtype with co - association of stag2 and tp53 mutations . 
 mankuzhy et al juckett lt , lin di , madison r , et al : a pan - cancer landscape analysis reveals a subset of endometrial stromal and pediatric tumors dened by internal tandem duplications of bcor . 
li w - s , liao i - c , wen m - c , et al : bcor - ccnb3 - positive soft tissue sarcoma with round - cell and spindle - cell histology : a series of four cases highlighting the pitfall of mimicking poorly differentiated synovial sarcoma . 
shern jf , chen l , chmielecki j , et al : comprehensive genomic analysis of rhabdomyosarcoma reveals a landscape of alterations affecting a common genetic axis in fusion - positive and fusion - negative tumors . 
puls f , niblett a , marland g , et al : bcor - ccnb3 ( ewing - like ) sarcoma : a clinicopathologic analysis of 10 cases , in comparison with conventional ewing sarcoma . 
bellus ga , spector eb , speiser pw , et al : distinct missense mutations of the fgfr3 lys650 codon modulate receptor kinase activation and the severity of the skeletal dysplasia phenotype . 
de gunst mm , gallegos - ruiz mi , giaccone g , et al : functional analysis of cancer - associated egfr mutants using a cellular assay with yfp - tagged egfr 28 . 
proc natl acad sci usa 114 : 3981 - 3986 , 2017 [ erratum : proc intracellular domamol cancer 6 : 56 , 2007 natl acad sci usa 114 : e4317 , 2017 ] 29 . 
tiberi l , bonnefont j , van den ameele j , et al : a bcl6 / bcor / sirt1 complex triggers neurogenesis and suppresses medulloblastoma by repressing sonic hedgehog signaling . 
schnidar h , eberl m , klingler s , et al : epidermal growth factor receptor signaling synergizes with hedgehog / gli in oncogenic transformation via activation of the mek / erk / jun pathway . 
wei , md1 cdk12 is a kinase that regulates several key cellular processes , including transcription and maintenance of genomic stability.1 the prevalence of cdk12 alterations is higher in metastatic castration - resistant prostate cancer ( mcrpc ; 7% ) compared with primary prostate cancer ( 1% ) , which indicates an association with an aggressive phenotype.2 in the articles accompanying this editorial in jco precision oncology , schweizer et al3 and antonarakis et al4 report on the clinical features and outcomes of patients with cdk12 - altered prostate cancer in two independent retrospective multicenter series . 
in both studies , the source of tumor dna included primary prostate , metastatic sites , and circulating tumor dna sequenced for cdk12 alteration status through a variety of commercial and inhouse sequencing platforms . schweizer et al3 identied 52 patients who harbored cdk12 mutations , and antonarakis et al4 identied 60 . in both studies , there was a roughly even split incidence of monoallelic or biallelic cdk12 inactivation . because of limitations in the diverse sequencing platforms used , neither series required biallelic mutations . 
in the schweizer series , median time from initiation of androgen deprivation therapy ( adt ) to development of crpc was 1.4 years , and in the antonarakis series , median progression - free survival ( pfs ) after initiation of adt was 12.3 months , which indicates short responses to primary adt . 
median overall survival ( os ) from time of metastasis was 3.9 years in the schweizer series , and median os from initiation of adt was 40.8 months in the antonarakis data set , which suggests poor prognosis . 
in the schweizer cohort , the unconrmed 50% prostate - specic antigen decline ( psa50 ) response rate to rst - line abiraterone and enzalutamide for crpc was approximately 70% ; however , median pfs was short at approximately 9 months . 
first , antonarakis et al required a conrmatory psa at least 4 weeks after the initial psa50 response , which was not required in the schweizer series and likely contributed to the lower psa response rate in the antonarakis study . 
de novo metastatic presentation is a poor prognostic factor that likely contributed to the shorter pfs with rst - line abiraterone and enzalutamide in the antonarakis study . these data are consistent with another recently published retrospective series by reimers et al5 that included 46 patients with advanced prostate cancer with cdk12 mutations . 
of note , the patients with cdk12 loss - of - function alterations had worse clinical outcomes compared with those with other mutations , including atm , brca1 / 2 , and tp53 . 
taken together , all three studies have consistently shown that cdk12 alterations portend aggressive clinical features and relative resistance to second - generation androgen signaling inhibitors . while the antonarakis and schweizer series represent the largest cdk12 - altered cohorts to date , they are both limited by their retrospective nature . 
clinical assessments were variable and not standardized , and there were no comparisons of cdk12 alteration with other genomically dened cohorts ( as in the reimers et al5 study )  . 
regardless , the authors should be commended for assembling these large data sets that help to inform on the prognostic implications of cdk12 - mutated prostate cancer . furthermore , these series include the largest cohort to date of outcomes in cdk12 - mutated prostate cancer after immune checkpoint blockade , shedding light on its predictive potential . 
two phase iii , randomized , placebocontrolled trials of ipilimumab in the postdocetaxel and predocetaxel mcrpc settings failed to meet their primary end point of os.6 , 7 pembrolizumab alone in mcrpc leads to low rates of either psa or radiographic response.8 while the prevalence of mismatch repair ( mmr ) deciency in crpc is low ( , 5% ) , 9 deciencies in mmr proteins are associated with higher psa and objective responses to pd - 1 / pd - l1 inhibitors.10 the response rate to pd - 1 / pd - l1 inhibitors in crpc is higher than the prevalence of mmr deciency , and some patients achieve responses without harboring mmr - decient tumors , which suggests that there are other currently undetermined biomarkers of clinical benet . cdk12 biallelic inactivating mutations lead to the formation of ftd , which results in increased prevalence of gene fusions , elevated antigen load , and inltration of t cells into the tumor microenvironment.2 these ndings suggest that tumors that harbor cdk12 loss may be immunogenic and susceptible to immunotherapy . in a small cohort of 4 pretreated patients with cdk12 - mutant mcrpc treated with an anti - pd - 1 immune checkpoint inhibitor , 2 experienced a marked psa decline.2 this suggests the potential of cdk12 as a predictive biomarker for immunotherapy , a hypothesis that can be scrutinized further with new data from the schweizer and antonarakis series . in the antonarakis series , 9 heavily pretreated men with mcrpc received a pd - 1 inhibitor , of whom 3 ( 33% ) achieved a conrmed psa50 response . 
in the schweizer series , 19 patients received diverse immunotherapy regimens , including pembrolizumab , atezolizumab , nivolumab and ipilimumab , durvalumab and tremelimumab , and atezolizumab and radium - 223 . 
objective responses were not assessed in this series . heterogeneity in patient population , prior therapies , and treatment regimens likely account for the differences in clinical outcomes to immune checkpoint inhibitors observed in these two studies . 
furthermore , the rate of objective responses and duration of disease control remain unclear . ultimately , prospective data are needed to further dene the role of cdk12 as a potential biomarker to predict response and benet to immune checkpoint inhibitors in advanced prostate cancer . 
toward this end , multiple prospective clinical trials are currently under way to explore outcomes to immune checkpoint inhibition in patients with prostate cancer who harbor cdk12 alterations or other dna damage repair defects ( table 1 )  . 
of note , these studies are prospectively enriching for genomic alterations of interest and cover a spectrum of disease states , including biochemically recurrent prostate cancer , metastatic hormone - sensitive prostate cancer , and mcrpc . 
for example , cdk12 loss is associated with amplication of cell cycle genes ccn1 and cdk4 , which suggests that cdk12 - mutated tumors may be susceptible to cdk4 / 6 inhibition.11 the combination of atezolizumab and abemaciclib is being studied in cdk12 - altered mcrpc ( clinicaltrials.gov identier : nct04272645 )  . optimal patient selection using clinical and genomic / molecular characteristics along with effective combination strategies are likely to move the needle for immunotherapy strategies in prostate cancer . 
despite the limitations of retrospective analysis , these data with rich clinical annotation suggest that patients with prostate cancer with cdk12 mutations have a poor prognosis and that novel therapies are needed . 
wei honoraria : onclive research funding : bristol - myers squibb travel , accommodations , expenses : corvus pharmaceuticals no other potential conicts of interest were reported . references blazek d , kohoutek j , bartholomeeusen k , et al : the cyclin k / cdk12 complex maintains genomic stability via regulation of expression of dna damage response genes . 
cell 173 : 1770 - 1782.e14 , 2018 schweizer mt , ha g , gulati r , et al : cdk12 - mutated prostate cancer : clinical outcomes with standard therapies and immune checkpoint blockade . 
eur urol 77 : 333 - 341 , 2020 kwon ed , drake cg , scher hi , et al : ipilimumab versus placebo after radiotherapy in patients with metastatic castration - resistant prostate cancer that had progressed after docetaxel chemotherapy ( ca184 - 043 ) : a multicentre , randomised , double - blind , phase 3 trial . 
lancet oncol 15 : 700 - 712 , 2014 beer tm , kwon ed , drake cg , et al : randomized , double - blind , phase iii trial of ipilimumab versus placebo in asymptomatic or minimally symptomatic patients with metastatic chemotherapy - naive castration - resistant prostate cancer . 
j clin oncol 38 : 395 - 405 , 2020 abida w , cheng ml , armenia j , et al : analysis of the prevalence of microsatellite instability in prostate cancer and response to immune checkpoint blockade . jama oncol 5 : 471 - 478 , 2019 10 . 
agarwal n , loriot y , mcgregor ba , et al : cabozantinib ( c ) in combination with atezolizumab ( a ) in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) : results of cohort 6 of the cosmic - 021 study . 
 acquired alk and ret gene fusions as mechanisms of resistance to osimertinib in egfr - mutant lung cancers introduction approximately 20% of patients with metastatic lung adenocarcinoma have somatic activating mutations in the epidermal growth factor receptor ( egfr ) gene , egfr . 
1 patients with egfr - mutant lung adenocarcinomas have a 70% response rate to first - line egfrtyrosine kinase inhibitor ( tki ) therapy ( ie , erlotinib , gefitinib , or afatinib ) .2 egfr t790m is the dominant resistance mechanism to earlier - generation egfr - tkis.3 osimertinib is approved by the us food and drug administration for the treatment of egfr - mutant lung cancers that have an acquired egfr t790m after failure of a previous egfr - tki4 and now is approved in the first - line setting as well.5 response to osimertinib eventually is followed by progression with known resistance mechanisms , including small - cell transformation3 , 6 ; acquired egfr mutations , including g796 / c797 , l792 and l718 / g7197 ; and non - egfr mediated resistance , including alterations / amplification in met , her2 , braf , mek , kras , and pik3ca . 
ngs with archerdx and msk - impact confirmed an acquired eml4 - alk fusion ( eml4 exons 1 through 6 fused with alk exons 20 through 29 ; c.667 + 516 : eml4_c.3173 - 415 : alkinv ) in addition to the egfr exon19del and t790m mutations . 
the patient started combination treatment with osimertinib 80 mg daily and crizotinib 200 mg twice daily , remained on treatment with stable disease ( by recist version 1.1 ) , and continued to receive clinical benefit from treatment , with no report of toxicity . 
the preosimertinib biopsy was a fine - needle aspiration ( fna ) and was partially fragmented on staining , whereas the acquired resistance ( ar ) sample was a core - needle biopsy . 
the pretreatment egfr exon19del staining was performed with epidermal growth factor receptor ( egfr ) e746 ; the post - treatment ihc stained more diffusely for egfr exon19del , likely related to the egfr amplification ( fold change : 3.0 ) noted on next - generation sequencing with msk - impact . 
 the ihc data suggest the presence of the alk rearrangement and egfr mutation within the same cell ( however , this cannot be confirmed by targeted next - generation sequencing because of technical limitations )  . 
 case 2 a 68 - year - old woman , who was never a smoker , presented with a 9 - cm right apical lung mass , right hilar lymphadenopathy , and a left temporal lobe mass ( staging t4n1m1b )  . 
 ( of note , no alk rearrangement was detected on ngs or fish . ) the patient started treatment with osimertinib and had an initial disease response , but oligoprogression occurred in the lung after 6 months . 
 ( a ) osimertinib and crizotinib in patient case 1 after one cycle ( 28 days ) of treatment ; image shows overall stable disease ( 0% best response )  . 
 ( b ) osimertinib and alectinib in patient case 2 after one cycle ( 28 days ) of treatment ; image shows regression of the dominant right upper lobe mass ( 25% reduction )  . precombination targeted therapy postcombination targeted therapy precombination targeted therapy postcombination targeted therapy l858r and t790m mutations as well as the new eml4 - alk rearrangement ( eml4 exons 1 through 2 fused to alk exons 20 through 29 ; c.208 + 4890 : eml4_c.3173 - 373 : alkinv ; fig 3b ; appendix table a2 )  . 
the patient started treatment with alectinib 300 mg twice daily and osimertinib 80 mg daily ; the first interval scan showed a decrease in the dominant right lung mass ( 25% reduction by recist version 1.1 ) as well as ongoing clinical benefit and no report of toxicity at the last follow - up . 
a right lung biopsy showed the known egfr l747s and l858r mutations as well as a new ncoa4 - ret fusion on msk - impact ; the fusion was confirmed by archerdx . 
 ( * ) treatment ongoing as of april 1 , 2018 . which showed that the fusion partner did not influence ret activity in cell lines.19 , 20 each condition was assayed in triplicate in at least two independent experiments . 
the pc9 cells were used to assess the effect of ret fusions on sensitivity of growth and apoptosis ( caspase 3 / 7 activity ) in the presence of osimertinib and cabozantinib . 
however , erk1 / 2 phosphorylation was not sensitive to osimertinib treatment in pc9 - pcx4.1ccdc6 - ret cells but was diminished with cabozantinib treatment ( fig 4b )  . 
these results suggest that ret rearrangements can cause bypass activation of growth - promoting pathways in cells that express oncogenic egfr . growth of pc9 cells that stably expressed ccdc6 - ret or kif5b - ret rearrangements was at least 10 - fold less sensitive to osimertinib than pc9 - pcx4.1empty cells were ( 50% inhibitory concentrations described in fig 4e )  . 
expression of ret fusions in pc9 cells prevented osimertinib - induced activation of caspase 3 / 7 , similar to the effect on growth rate ( fig 4f [ left panel ] )  . 
treatment of control - group pc9 cells or pc9 - ret cells with cabozantinib did not lead to activation of caspase 3 / 7 ( fig 4f [ left panel ] )  . 
these results suggest that ret rearrangements can induce resistance to osimertinib in cells that have egfr mutations and that response to osimertinib is restored when it is used in combination with cabozantinib . in conclusion , osimertinib is now a first - line treatment for metastatic egfr - mutant lung cancers.5 although potential resistance mechanisms to osimertinib have been identified , these have primarily been observed after later - line osimertinib in the setting of egfr t790m mutations and have focused on ctdna.9 - 11 many alterations identified as potential resistance mechanisms are seen concurrently with egfr in pretreatment samples , including amplifications of met and her2 as well as pik3ca mutations , which makes the comparison with pretreatment tissue critical to identify truly acquired alterations.13 as ngs becomes standard of care , it is feasible and fruitful to molecularly profile tumors broadly before treatment and at progression to identify acquired alterations that mediate resistance . it remains unclear whether mechanisms of resistance to first - line osimertinib will differ from mechanisms of resistance to later - line osimertinib or earlier - generation egfr - tkis . 
osimertinib is a potent mutant - egfr inhibitor that inhibits egfr t790m , so there is a potential to see novel on - target21 , 22 and off - target23 - 25 resistance mechanisms . 
this is corroborated by the low frequency ( 15% to 25% ) of egfr c797s and other acquired egfr alterations after osimertinib use compared with 60% frequency of acquired egfr t790m after use of earlier generation egfr - tkis.9 , 13 , 22 we may see new acquired alterations not previously seen or seen rarely with earlier - generation egfr - tkis . 
 moreover , although cabozantinib can inhibit growth of egfrand ret - mutant / rearranged cell lines , a combination of osimertinib and cabozantinib induced apoptosis . at our institution , among 174 patients with egfr - mutant lung cancer in whom ngs was performed on tumor tissue after progression developed during treatment with erlotinib or afatinib , we found no alk or ret fusions . 
it is unknown whether this potential enrichment of acquired fusions is related to the more potent egfr inhibition of osimertinib or to the later - line setting after multiple lines of egfr inhibition . 
pc9 cells were infected with lentivirus that harbored an empty plasmid ( pcx4.1 - empty ) or pcx4.1 with either ccdc6 - ret or kif5b - ret complementary dna ( cdna ) , and cells that expressed the plasmids were selected to generate stable cell lines . 
 ( a ) cell extracts were immunoblotted ( indicated by ib ) for ( left panel ) total ret ( left panel ) or ( right panel ) phosphorylated ret . 
 ( b ) cell lines were treated with either osimertinib 0.05 m or cabozantinib or 0.25 m for 1 h ; cell extracts were prepared and then immunoblotted for the indicated proteins . 
 ( c ) cells were treated with increasing concentrations ( as indicated on the figure ) of ( left panel ) osimertinib or ( right panel ) cabozantinib for 96 h , and then growth was determined . 
 ( f ) cells were treated with the indicated concentrations of ( left panel ) osimertinib or ( right panel ) cabozantinib for 48 hours , and then caspase 3 / 7 enzymatic activity determined . 
 ( g ) pc9 cells that expressed either pcx4.1 - empty vector or pcx4.1ccdc6 - ret were treated with the indicated concentrations of cabozantinib in the presence of osimertinib 0.1 m for 48 h , and then caspase 3 / 7 enzymatic activity was determined . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . michael offin no relationship to disclose romel somwar research funding : helsinn healthcare travel , accommodations , expenses : helsinn healthcare natasha rekhtman no relationship to disclose ryma benayed no relationship to disclose jason c . 
li consulting or advisory role : roche , biosceptre international , thermofisher scientific , mersana , guardant health research funding : roche ( inst ) , genentech ( inst ) , illumina ( inst ) , biomed valley discoveries ( inst ) , astrazeneca ( inst ) , grail ( inst ) gregory j . 
riely research funding : novartis ( inst ) , roche ( inst ) , genentech ( inst ) , millenium ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , infinity pharmaceuticals ( inst ) , ariad ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : merck sharp & dohme charles m . 
kris consulting or advisory role : astrazeneca , regeneron william travis speakers ' bureau : genentech alexander drilon consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pfizer , blueprint medicines , genentech , roche , takeda , helsinn therapeutics , beigene maria e . 
arcila consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe , raindance technologies marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network , boehringer ingelheim , astrazeneca ( tagrisso rfp advisory committee ) research funding : loxo ( inst ) helena a . 
jui , the chinese university of hong kong , sha tin new town , hong kong special administrative region , china . supported in part by the national cancer institute of the national institutes of health grants no . 
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national cancer institute : osimertinib and necitumumab in treating patients with egfr - mutant stage iv or recurrent nonsmall - cell lung cancer who have progressed on a previous egfr tyrosine kinase inhibitor ( nct02496663 )  . 
okamoto k , kodama k , takase k , et al : antitumor activities of the targeted multi - tyrosine kinase inhibitor lenvatinib ( e7080 ) against ret gene fusiondriven tumor models . 
arai s , kita k , tanimoto a , et al : in vitro and in vivo anti - tumor activity of alectinib in tumor cells with ncoa4 - ret . 
klempner sj , mehta p , schrock ab , et al : cis - oriented solvent - front egfr g796s mutation in tissue and ctdna in a patient progressing on osimertinib : a case report and review of the literature . 
ou si , horn l , cruz m , et al : emergence of fgfr3 - tacc3 fusions as a potential bypass resistance mechanism to egfr tyrosine kinase inhibitors in egfr - mutated nsclc patients . 
detailed molecular and immunohistochemical characterization of patient case 1 presented timing of molecular test diagnosis type of molecular test result tissue pcra impactb 15base pair egfr exon 19 deletion detected egfr exon19 p.e746_a750del ; tp53 exon10 p.r337l ; atr exon41 p.d2331y detected erlotinib progression cfdnac egfr t790m detected ( 0.79% ) d tissue pcrc egfr t790m detected ( 15.15% ) d alk : negative ; egfr exon 19 deletion : positive osimertinib + necitumumab ihce alk : positive ; egfr exon 19 deletion : positive progression impactb ihce impactb archerdxf fishg egfr exon19 p.e746_a750del ; egfr exon20 p.t790m ; kmt2c exon38 p.d2690n ; rad51b exon7 p.l209v detected no alk fusion detected no evidence of alk rearrangement . 
the single base extension product is detected by tandem mass - spectrometry on a sequenom massarray spectrometer ( sequenom , san diego , ca )  . bmsk - impact ( integrated mutation profiling of actionable cancer targets ) was used to identify specific mutations in 468 genes . cdigital pcr of cfdna and / or tissue amplification of part of egfr exon 20 in the presence of fluorescent probes specific to the wild - type and mutant alleles . dratio of mutant allele / ( mutant + wild - type allele )  . eimmunohistochemistry ( ihc ) for pertinent proteins performed with the following clones : egfr - exon19del ( egfr - e746 ) : clone 6b6 ; alk : clone d5f3 . farcher fusionplex custom solid panel ( archer fusionplex , boulder , co ) uses the anchored multiplex pcr used to detect gene fusions in tumor samples consisting of 62 cancer - related genes previously reported to be involved in chromosomal rearrangements . 
the single base extension product is detected by tandem mass - spectrometry on a sequenom massarray spectrometer . carcher fusionplex custom solid panel uses the anchored multiplex pcr used to detect gene fusions in tumor samples consisting of 62 cancer - related genes previously reported to be involved in chromosomal rearrangements . 
 lynch syndrome and breast cancer risk : weighing the data wendy kohlmann , ms , cgc1 as we continue to expand our understanding of the genotype - phenotype correlations in lynch syndrome ( ls ) , we must be cautious in the design of studies and interpretation of ndings to responsibly serve our patients with ls with as accurate information as possible . 
although pathogenic variants ( pvs ) in the mismatch repair ( mmr ) genes mlh1 , msh2 / epcam , msh6 , and pms2 are all associated with ls , each gene is associated with a unique risk prole . 
mlh1 and msh2 have been associated with the highest risk for ls - associated cancers , whereas risk for colorectal cancer is signicantly lower for msh6 and pms2 pv carriers.1 in studies of high - risk colorectal cancer cohorts , msh6 and pms2 pvs are less commonly identied than mlh1 and msh2 , but use of clinical multigene panel testing is expanding the identication of carriers of pvs in these genes , often in individuals and families lacking the classic pattern of cancers associated with ls.2 , 3 the large data sets being generated by genetic testing laboratories can be assets for research and can allow for gene - specic risk analysis . however , analytical caution needs to be taken to account for the biases that arise from patient selection for clinical genetic testing , and family history and clinical data provided to commercial laboratories may be incorrect or inaccurate . in the article accompanying this editorial , stoll et al2 add data from a large cohort of mmr carriers and demonstrate a successful strategy for using commercial laboratory data to assess associations between pvs and cancer risk . 
however , to account for the study population having a more signicant cancer history than the general population , pv carriers were also compared with other subpopulations within the laboratory cohort , including women who were negative for a pv in any cancer predisposition gene when testing was performed for evaluation for hereditary breast or ovarian cancer ( hboc ) and / or ls , evaluation for hboc only , and evaluation for ls only . no excess in breast cancer risk was noted when compared with seer or any laboratory comparison group for any of the mmr genes . in the cohort in the study by stoll et al , 2 pvs in msh6 and pms2 were more common in women undergoing genetic testing for the indication of hboc than in women being tested as a result of suspicion of ls . other studies of clinical testing populations have also found a predominance of msh6 and pms2 pvs in individuals meeting hboc guidelines rather than ls.4 however , this pattern does not conrm that these genetic variants increased the risk for breast cancer . this distribution of pvs in laboratory cohorts likely reects that , other than msh6 - associated endometrial cancer risk , pvs in msh6 and pms2 confer only a modest risk for colorectal and other lsassociated cancers . 
stoll et al2 have provided a systematic examination of a large laboratory cohort using the proper comparison groups to put the frequency of msh6 and pms2 pvs by testing criteria into context and have provided strong evidence against the association of breast cancer with any of the mmr genes . before widespread panel testing , most analyses of breast cancer risk and ls had come from small studies.5 data from studies with larger samples are now becoming available . 
signicant breast cancer history may be a result of other factors , and genetic testing of other affected family members may be warranted to determine whether there is an additional pv segregating in the family and contributing to that cancer risk . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . wendy kohlmann employment : biofire diagnostics ( i ) no other potential conicts of interest were reported . references dominguez - valentin m , sampson jr , sepp al a tt , et al : cancer risks by gene , age , and gender in 6350 carriers of pathogenic mismatch repair variants : findings from the prospective lynch syndrome database . 
cancer epidemiol biomarkers prev 26 : 404 - 412 , 2017 espenschied cr , laduca h , li s , et al : multigene panel testing provides a new prospective on lynch syndrome . 
mller p , sepp al a tt , bernstein i , et al : cancer risk and survival in path_mmr carriers by gene and gender up to 75 years of age : a report from the prospective lynch syndrome database . 
gut 67 : 1306 - 1316 , 2018 ten broeke sw , van der klift hm , tops cmj , et al : cancer risks for pms2 - associated lynch syndrome . 
j clin oncol 36 : 2961 - 2968 , 2018 slavin tp , maxwell kn , lilyquist j , et al : the contribution of pathogenic variants in breast cancer susceptibility genes to familial breast cancer risk . 
npj breast cancer 3 : 22 , 2017 therkildsen c , ladelund s , smith - hansen l , et al : towards geneand gender - based risk estimates in lynch syndrome ; age - specic incidences for 13 extracolorectal cancer types . 
evans dg , woodward er , lalloo f , et al : are women with pathogenic variants in pms2 and msh6 really at high lifetime risk of breast cancer ? genet med 13 . 
2018 : is breast cancer truly caused by msh6 and pms2 variants or is it simply due to a high prevalence of these variants in the population ? genet med 21 : 256 - 257 , 2019 14 . 
 c treatment of patients with lobular breast cancer harboring human epidermal growth factor receptor 2 mutation with her2 - directed therapy introduction human epidermal growth factor receptor 2 ( her2 ) is a tyrosine kinase encoded by the erbb2 gene . 
mutations in cdh1 have been reported in 62% to 100% of cases of invasive lobular carcinoma , and many investigators consider a mutation in cdh1 to represent a genomic alteration characteristic of lobular carcinoma.5 mutations in erbb2 have been reported in six of 22 ( 27% ) cdh1 - mutated lobular carcinomas.5 the presence of activating somatic mutations in erbb2 could provide a rationale for her2 targeted therapy , 4 , 6 and there have now been several case reports of successful treatment of patients with such mutations with her2 targeted therapy.7 - 10 we initially identified a patient with progressive metastatic lobular carcinoma resistant to chemotherapy and hormonal regimens , whose liver metastasis harbored both cdh1 and erbb2 mutations . 
on the basis of the presence of the erbb2 mutation , we elected to treat the patient with her2 - targeted therapy , and she has achieved significant and durable responses to three consecutive her2 - targeted therapies during a 2.5year period of time , despite the lack of erbb2 amplification . after our experience with this patient , we then reviewed all of our patients with metastatic lobular carcinoma of the breast for whom next generation sequencing had been obtained . 
on the basis of reports that erbb2 exon 20 insertion has been shown to confer sensitivity to trastuzumab and tyrosine kinase inhibitors , we elected to treat the patient with dual her2 blockade with the combination of trastuzumab and pertuzumab.2 , 3 treatment was continued for 8 months , with major subjective clinical improvement , which included better appetite and resolution of abdominal pa clinical response was confirmed by ct scan on april 4 , 2016 showing a significant decrease in hepatic lesions , which has been maintained ( fig 2 )  . 
by july 2017 , the carcinoembryonic antigen , ca19 - 9 , and alkaline phosphatase increased aga ado - trastuzumab emtansine was discontinued , and she was started on third - line anti - her2directed therapy with lapatinib and capecitabine in july 2017 . she once again demonstrated significant response in all four tumor markers as well as her liver enzymes ( figs 3 and 4 )  . 
 only one of the five was also her2 amplified and had received prior her2 - directed therapy . all five patients have received her2 - targeted therapy for their metastatic disease , and four have achieved clinical responses as defined by response evaluation criteria in solid tumors ( recist ; tables 1 and 2 )  . 
liver biopsy showing infiltrating cords and nests of tumor cells ( july 2011 )  . in december 2010 , tumor markers were noted to be elevated , and a magnetic resonance imaging scan of the abdomen demonstrated hepatic metastases . 
 subsequent positron emission tomography / computed tomography ( ct ) scan showed progression of her liver lesions , and an ultrasound guided biopsy of the liver in july 2011 confirmed metastatic lobular carcinoma ( fig 1 )  . 
as with the primary tumor , the tumor specimen from liver biopsy was estrogen receptor and progesterone receptor positive and her2 negative by ihc . during the next 2 years she was treated with several chemotherapy regimens , including carboplatin and gemcitabine , capecitabine , and eribul she experienced progression on these regimens after initial responses of approximately 6 months , and progression of liver metastases was seen in august of 2014 . eribulin was then discontinued and she was started on tamoxifen , followed by exemestane and everolimus . 
her disease did not respond to these treatments , and she presented to cancer treatment centers of america at midwestern regional medical center for a second opinion in march of 2015 with extensive hepatic and bone metastases . 
comprehensive metabolic panel : alkaline phosphatase , ast , and alt . has received only two cycles of treatment , and it is too early to evaluate for radiologic response , although her tumor markers have fallen significantly . discussion we have identified erbb2 mutations in five of 16 patients ( 31% ) with cdh1 - mutated metastatic lobular carcinoma , an incidence similar to that previously reported.5 our experience suggests that such patients may well respond favorably to her2 - targeted therapy despite the absence trastuzumab and pertuzumab of her2 amplification . 
if the prevalence of erbb2 mutations is confirmed in larger studies , it would indicate that a significant number of patients with metastatic lobular carcinoma are likely to benefit from her2 - targeted therapy . 
this , together with the fact that one patient ( patient 3 ) had received no systemic treatment before biopsy , suggests that erbb2 mutation may be an intrinsic characteristic of lobular carcinoma of the breast and does not necessarily arise from prior systemic therapy . there is currently considerable interest in the possibility that patients with her2 - mutated breast cancer can be successfully treated with drugs already approved by the us food and drug administration for her2 - amplified disease . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . speakers ' bureau : astrazeneca , pfizer , r - pharm us , agendia bradford a . 
ali employment : foundation medicine leadership : incyte stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health on microbiome in non - neoplastic disease ( i ) ankur r . 
parikh consulting or advisory role : foundation medicine maurie markman employment : cancer treatment centers of america consulting or advisory role : amgen , celgene , crititech , pfizer , myriad genetics , merck , clovis oncology dennis l . 
 expert testimony : actavis , acorn research , apotex , emcure pharmaceuticals , dr reddy 's laboratories , fresenius kabi , hikma pharmaceuticals , hospira , pharma international , sagent pharmaceuticals , strides arcolab , sun pharma , wockhardt jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine references stock and other ownership interests : foundation medicine research funding : foundation medicine arun kadamkulam syriac no relationship to disclose sara j . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
ross js , slodkowska ea , symmans wf , et al : the her - 2 receptor and breast cancer : ten years of targeted anti - her - 2 therapy and personalized medicine . 
ross js , wang k , sheehan ce , et al : relapsed classic e - cadherin ( cdh1 ) - mutated invasive lobular breast cancer shows a high frequency of her2 ( erbb2 ) gene mutations . 
ali sm , alpaugh rk , downing sr , et al : response of an erbb2 - mutated inflammatory breast carcinoma to human epidermal growth factor receptor 2 - targeted therapy . 
chumsri s , weidler j , ali s , et al : prolonged response to trastuzumab in a patient with her2nonamplified breast cancer with elevated her2 dimerization harboring an erbb2 s310f mutation . 
ben - baruch ne , bose r , kavuri sm , et al : her2 - mutated breast cancer responds to treatment with single - agent neratinib , a second - generation her2 / egfr tyrosine kinase inhibitor . 
shih j , bashir b , gustafson ks , et al : cancer signature investigation : erbb2 ( her2 ) - activating mutation and amplification - positive breast carcinoma mimicking lung primary . 
hyman dm , piha - paul sa , rodon j , et al : neratinib in her2 or her3 mutant solid tumors : summit , a global , multi - histology , open - label , phase 2 basket study . 
 use of cabozantinib in a patient with egfr - mutated nonsmall - cell lung cancer harboring acquired ccdc6 - ret fusion young kwang chae , md , mph , mba1 ; pedro viveiros , md1 ; caio t . 
nine months after initiation of therapy , however , the patient displayed growth of the known right lung lesion as well as a new subcentimeter nodule in the right lower lobe . 
genomic proling with ctdna next - generation sequencing ( ngs ; guardant health , redwood city , ca ) identied an egfr t790m mutation with a variant allele frequency of 0.2% ( fig 1b ) the patient was then started on osimertinib . 
ct scans after 7 months showed a new right - sided pleural effusion , with an associated dense consolidation that was considered to represent either atelectasis or therapy - related pneumonitis . 
repeat ctdna ngs no longer detected the t790m mutation but presented new mutations in pik3ca ( g118d , 0.7% ) and tp53 ( h193l , 0.4% ) as well as a ccdc6 - ret rearrangement with a frequency of 0.1% ( fig 1c )  . 
instead , she opted to continue osimertinib with the addition of bevacizumab . fourteen months from the start of osimertinib , the patient had recurrent malignant effusions with possible pleural - based metastases concerning for disease progression . 
the tumor response mapping illustrates the mutant allele percentage ( percent cell - free dna [ cfdna ] ) of observed somatic variants at each sample submission time point . the somatic alteration burden value refers to the maximum percentage cfdna detected at each time point and has been used to illustrate how tumor progeny is responding to the selective pressure of treatment . 
three months after cabozantinib initiation , ct imaging still could not visualize her primary tumor but demonstrated decreased burden of bilateral pulmonary nodules as well as a discrete increase in pre - existent liver metastases . 
the patient reported marked improvement of dyspnea and pain as well as increased activity tolerance . discussion we report emergence of ccdc6 - ret rearrangement in the setting of osimertinib use in a patient with egfr t790mmutated nsclc . 
the c797s egfr mutation is detected in ctdna in nearly 40% of these patients and has been implicated in osimertinib resistance.9 - 12 other less commonly reported mutations include met , erbb2 ( human epidermal growth factor receptor ) , braf , egfr ( l718q ) , kras , and g12s.6 , 13 - 16 many of these occurred with the loss of egfr t790m mutation , suggesting that t790m - positive clones were suppressed , but t790m wild - type cells with other driver mutations were able to mediate resistance.6 epithelial - mesenchymal transition transformation have also been changes and small - cell reported in some cases of resistance . 
nonetheless , approximately 15% to 20% of the cases , the mechanism of acquired resistance to egfr tkis is yet to be discovered . in this patient , we identied an uncommon acquired ccdc6 - ret rearrangement that is also found in approximately 1% to 2% of nsclcs at primary diagnosis.17 this rearrangement raises interest as a result of its possible role in resistance , emerging under the selective pressure of treatment . 
fusion of the ret tyrosine kinase domain with an upstream coiled - coil domain has been shown to promote self - dimerization , resulting in constitutive signaling via prosurvival and proliferative pathways.18 ccdc6 - ret rearrangements accounted for 23% of genetic alterations in a recent international registry of ret - rearranged lung cancers.19 at the initial diagnosis , de novo ret rearrangements have been considered to be mutually exclusive with other common driver mutations , such as those in egfr , braf , kras , and alk.17 trials assessing clinical and pathologic characteristics of these de novo ret rearrangement suggest increased frequency in nonsmokers and patients with poorly differentiated adenocarcinomas , solid subtype , younger age , asian origin , or small tumors ( 3 cm or smaller ) with n2 disease.17 , 20 , 21 germline gain - of - function mutations in ret predispose carriers to multiple endocrine neoplasia type 2 , whereas somatic gain - of - function ret mutations have been commonly reported in sporadic medullary thyroid cancer and papillary thyroid cancer.22 , 23 several commercially available multikinase inhibitors , such as vandetanib , cabozantinib , sorafenib , sunitinib , lenvatinib , and ponatinib , have shown activity against ret kinase ( table 1 )  . 
one example is loxo - 292 , which had a good toxicity prole and showed activity against retmutated or including those with previous resistance to multikinase inhibitors ( table 2 )  . translocated tumors , cabozantinib is recommended by the national comprehensive cancer network for treatment of medullary thyroid and clear cell renal cancers . 
its use in ret - mutated tumors is approved by the us food and drug administration and has been reported in a phase ii clinical trial of patients with nsclc.24 in this trial , an overall response rate of 28% was reported with a favorable safety prole . 
this dose has comparable plasma exposure ( area under the plasma concentration - time curve ) as the us food and drug administrationapproved dose of 140 mg per day used for the treatment of patients with metastatic medullary thyroid carcinoma.19 , 24 , 38 after 3 months of cabozantinib use in our patient , there was a reduction in ctdna level of ccdc6 - ret rearrangement and signicant improvement in reported symptoms . 
ctdna has been useful in demonstrating molecular response without the need for tissue biopsies and is a convenient way to assess for driver mutations and molecular response.39 absolute levels of ctdna have also been signicantly correlated with tumor volume measured by ct and positron emission tomographyct imaging.40 , 41 however , it has so far been used as an exploratory measure of response . 
clinical and imaging data remain sovereign . it is still unclear whether the presence of a rare yet targetable mutation represents a putative resistance mechanisfor this patient , the ret rearrangement was possibly not the only mechanism of acquired resistance . loss of t790m coincided with the emergence of several mutations in oncogenic drivers , although none have been proven to be associated with osimertinib resistance . 
furthermore , retrospective data sets can complement clinical trial results , as exemplied in a recently published global registry of retdirected treatment outcomes.19 in conclusion , we report a case of acquired ccdc6 - ret rearrangement in a patient with egfr - mutated nsclc . treatment with the ret inhibitor cabozantinib led to signicant clinical improvement and associated reduction in levels of ccdc6 - ret detected from ctdna . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . young kwang chae consulting or advisory role : foundation medicine , boehringer ingelheim , biodesix , counsyl , astrazeneca , guardant health , takeda , genentech , immuneoncia , hanmi speakers ' bureau : genentech , merck , astrazeneca , eli lilly research funding : abbvie , bristol - myers squibb , lexent bio , freenome , biodesix travel , accommodations , expenses : hanmi wade t . 
iams travel , accommodations , expenses : emd serono no other potential conicts of interest were reported . references diaz la jr , bardelli a : liquid biopsies : genotyping circulating tumor dna . 
j clin oncol 32 : 579 - 586 , 2014 pao w , chmielecki j : rational , biologically based treatment of egfr - mutant non - small - cell lung cancer . 
nat rev cancer 10 : 760 - 774 , 2010 kosaka t , yatabe y , endoh h , et al : analysis of epidermal growth factor receptor gene mutation in patients with non - small cell lung cancer and acquired resistance to getinib . 
clin cancer res 12 : 5764 - 5769 , 2006 j anne pa , yang jc , kim dw , et al : azd9291 in egfr inhibitor - resistant non - small - cell lung cancer . 
n engl j med 372 : 1689 - 1699 , 2015 soria jc , ohe y , vansteenkiste j , et al : osimertinib in untreated egfr - mutated advanced non - small - cell lung cancer . 
n engl j med 378 : 113 - 125 , 2018 planchard d , loriot y , andr e f , et al : egfr - independent mechanisms of acquired resistance to azd9291 in egfr t790m - positive nsclc patients . 
j clin oncol 31 : 3639 - 3646 , 2013 choueiri tk , escudier b , powles t , et al : cabozantinib versus everolimus in advanced renal - cell carcinoma . 
 cabozantinib in patient with nsclc with acquired ccdc6 - ret fusion 82 : 294 - 298 , 2013 e121 - e123 , 2016 2012 35 : 1403 - 1410 , 2017 2014 10 . 
yu ha , tian sk , drilon ae , et al : acquired resistance of egfr - mutant lung cancer to a t790m - specic egfr inhibitor : emergence of a third mutation ( c797s ) in the egfr tyrosine kinase domajama oncol 1 : 982 - 984 , 2015 12 . 
niederst mj , hu h , mulvey he , et al : the allelic context of the c797s mutation acquired upon treatment with third - generation egfr inhibitors impacts sensitivity to subsequent treatment strategies . 
klempner sj , bazhenova la , braiteh fs , et al : emergence of ret rearrangement co - existing with activated egfr mutation in egfr - mutated nsclc patients who had progressed on rstor second - generation egfr tki . 
sun j - m , ahn m - j , choi y - l , et al : clinical implications of t790m mutation in patients with acquired resistance to egfr tyrosine kinase inhibitors . 
gautschi o , milia j , filleron t , et al : targeting ret in patients with ret - rearranged lung cancers : results from the global , multicenter ret registry . 
lin c , wang s , xie w , et al : the ret fusion gene and its correlation with demographic and clinicopathological features of non - small cell lung cancer : a metaanalysis . 
yeganeh mz , sheikholeslami s , dehbashi behbahani g , et al : skewed mutational spectrum of ret proto - oncogene exon 10 in iranian patients with medullary thyroid carcinoma . 
yakes fm , chen j , tan j , et al : cabozantinib ( xl184 ) , a novel met and vegfr2 inhibitor , simultaneously suppresses metastasis , angiogenesis , and tumor growth . 
wells sa jr , robinson bg , gagel rf , et al : vandetanib in patients with locally advanced or metastatic medullary thyroid cancer : a randomized , double - blind phase iii trial . 
motzer rj , hutson te , glen h , et al : lenvatinib , everolimus , and the combination in patients with metastatic renal cell carcinoma : a randomised , phase 2 , open - label , multicentre trial . 
cortes je , kim dw , pinilla - ibarz j , et al : ponatinib efcacy and safety in philadelphia chromosome - positive leukemia : final 5 - year results of the phase 2 pace trial . 
drilon ae , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase oncol 36 , 2018 ( suppl 15 ; abstr 102 ) 2 , single - arm trial . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
nat med 20 : 548 - 554 , 2014 imamura f , uchida j , kukita y , et al : monitoring of treatment responses and clonal evolution of tumor cells by circulating tumor dna of heterogeneous mutant egfr genes in lung cancer . 
this article describes medical oncologists condence with genomic testing and the association between genomic condence and test use . methods we used data from the 2017 national survey of precision medicine in cancer treatment to characterize oncologists condence with genomic testing . 
genomic condence was examined separately by type of test user : next - generation sequencing ( ngs ) only , gene expression ( ge ) only , both ngs and ge , or nonuser . predictors of genomic condence were examined with multinomial logistic regression . 
the association between genomic condence and test use was examined with multivariable linear regression . results more than 75% of genomic test users were either moderately or very condent about using results from multimarker tumor panel tests to guide patient care . 
condence with using multimarker tumor panel tests was highest among both ngs and ge test users , with 60.1% very condent in using test results , and lowest among ngs - only test users , with 38.2% very condent in using test results . 
oncologists were most condent in using single - gene tests and least condent in using whole - genome or - exome sequencing to guide patient care . genomic condence was positively associated with self - reported test use . 
in adjusted models , training in genomics , larger patient volume , and treating patients with solid tumors predicted higher genomic condence . onsite pathology services and receipt of electronic medical record alerts for genomic testing predicted lower genomic condence . conclusion oncologists condence varies by testing platform , patient volume , genomic training , and practice infrastructure . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction the landscape of cancer care has changed dramatically over the past decade as therapies are increasingly personalized to the molecular characteristics of a patients tumor.1 whereas genomic testing in oncology started with testing for single mutations in specic genes , advances in molecular proling has spurred the development and now widespread use of multimarker tumor panels.2 , 3 these panels assess different types of genomic alterations commonly detected through nextgeneration sequencing ( ngs ) and gene expression ( ge ) proles . 
such testing can identify therapeutic targets that can be treated with particular anticancer agents and determine when individuals are at higher risk for recurrence and may need therapy.3 , 4 although not standard practice as of yet , whole - genome or whole - exome sequencing is a newer technology that shows promise in informing patient care.4 the rapid proliferation of genomic testing has outpaced the development of practice guidelines on their appropriate use.5 , 6 multimarker tumor panel tests generate vast data about the biology of a patients tumor . 
in cases where the tumor can be successfully sequenced , an actionable target is identied for 39%90% of patients , a wide range that varies by patient population and the size of the panel test.7 - 10 although testing reports typically highlight multimarker panel potentially benecial therapies and relevant clinical trials , individual providers must navigate the process of communicating results to their patients and selecting an appropriate targeted therapy . 
furthermore , multimarker panel testing frequently identies variants of unknown signicance or germline variants , which can further complicate interpretation and care management.11 - 13 very few studies have examined providers attitudes about genomic testing . 
 oncologist condence in genomic testing context key objective this article provides unique data about oncologists in the united states and their condence in using results from commercially available multimarker tumor panel tests to guide decisions about patient treatment and management . knowledge generated oncologists who used both next - generation sequencing ( ngs ) and gene expression tests reported the highest condence in using multimarker tumor panel results to guide patient care ; oncologists who only used ngs tests had the lowest condence . 
oncologists with higher condence were more likely to report using results from multimarker tumor panels to inform patient care . relevance these ndings underscore the importance of genomic training and suggest other providerand practice - level factors that can be leveraged to build oncologists condence in using genomic testing . providers lack condence in using new genomic tests , which could limit the extent to which new tests are appropriately applied in practice.5 , 6 , 14 , 15 for example , providers report less condence in using multimarker tumor panels compared with single - gene tests , which are well established for certain patient populations.6 in addition , providers vary in their understanding of how to interpret and act upon results from whole - genome sequencing , which is not available outside of clinical trials.16 given the potential of precision oncology , there is a need to better understand oncologists attitudes and experiences with genomic testing and to identify factors that foster genomic testing condence . this article builds upon previous studies by describing oncologists condence with genomic testing and the association between condence and genomic test use over the past 12 months . 
oncologists condence in using multimarker tumor panels was rst examined in relation to their condence in using single - gene somatic tests and whole - genome or - exome sequencing . 
oncologists condence was then further characterized by exploring the individualand practice - level characteristics associated with condence and assessing whether their condence was associated with their use of multimarker tumor panels in practice . methods data and study population this study uses data from the national survey of precision medicine in cancer treatment , a nationally representative study of how oncologists use genomic testing in practice . eligible providers were identied from the american medical association physician masterle and selected using multistage probability sampling . 
additional information about the study design and methods have been published elsewhere.17 the survey is available upon request . measures the national survey of precision medicine in cancer treatment collected detailed data about oncologists condence in using genomic testing ; their genomic test use ; and demographics , specialty , and practice characteristics . 
condence was assessed for genomic tests for individual genes or chromosomal alterations ( referred to as single - gene tests ) , commercially available multimarker tumor panel tests , and whole - genome or - exome sequencing . 
response options were very condent , moderately condent , a little condent , or not at all condent . type of genomic test user was determined on the basis of oncologists reported use of 18 specic multimarker tumor panels in the past 12 months . 
the multimarker tumor panel tests included commercially available ge tests ( eg , oncotype dx breast ; genomic health , redwood city , ca ) , commercially available ngs tests ( eg , foundationone ; foundation medicine , cambridge , ma ) , and noncommercial panels performed at an academic medical center . 
training in genomics was also captured and dened as any formal training ( eg , instruction during residency / fellowship , professional lectures or seminars , symposiums , conferences , continuing medical education ) in the use of genomic testing . practice setting information was assessed with questions about the number of unique patients with cancer treated per month . 
responses were categorized as academic medical center or medical school and nonacademic setting . infrastructure to support precision medicine was assessed with a series of questions about whether the respondents primary practice had the following genomic testing services : onsite pathology , internal policies or protocols for use of genomic and biomarker testing , an electronic medical record ( emr ) that alerts when a genomic test is recommended , or a genomic / molecular tumor board . 
response options were categorized as yes and no or do not know . analysis weighted percentages were calculated to describe the sample and provider condence in using single - gene tests , multimarker tumor panel tests , and whole - genome or - exome sequencing . 
two sets of models were examined : one that adjusted for type of genomic test user and a second that simultaneously adjusted for type of genomic test user and the other physician and practice characteristics in the model . 
results are presented as odds ratios and adjusted percentages , also referred to as predicted margins.19 multivariable linear regression was then used to assess whether condence was associated with the percentage of patients for whom multimarker panel test results guided patient care in the past 12 months . 
multivariable models adjusted for years since graduation , sex , race , census region , specialty , training in genomics , practice setting , patient volume , and infrastructure for precision medicine . 
results are presented as adjusted percentages.19 all analyses were conducted using sudaan release 11.0 statistical software ( rti international , research triangle park , nc ) and weighted to account for the complex sampling approach and survey nonresponse . results sample characteristics the sample comprised 1 , 281 oncologists ( table 1 )  . 
participants reported a range of institutional resources to support precision medicine , with onsite pathology and internal policies or protocols for use of genomic and biomarker testing reported most frequently . genomic test use was reported by 95.4% of the sample , with 58.6% using both ngs and ge tests , 26.4% using only ngs tests , and 10.3% using only ge tests . condence using genomic tests in practice condence using multimarker tumor panel tests to guide decisions about patient treatment and management was highest among ngs and ge users , with 60.1% very condent and 35.6% moderately condent in using test results . 
even among oncologists who did not use multimarker tumor panel tests in the past 12 months , 27.1% were very condent and 37.8% were moderately condent in using test results ( fig 1b )  . in contrast to multimarker tumor panel tests , oncologists were more condent in using somatic single - gene tests and less condent in using whole - genome or - exome sequencing ( figs 1a and 1c )  . 
30 female male race white asian other region midwest northeast south west specialty solid and hematologic malignancies hematologic malignancies only solid tumors only training in genomics practice setting practice afliation academic medical center or medical school other practice settingb no . 
percentages may not sum to 100 because of missing data . bother settings include a medical center not afliated with a medical school , community hospital , ofce - based practice , health maintenance organization or integrated health care system , and other . guide decisions about patient treatment and management . in the fully adjusted models ( table 2 ) and in models that only adjusted for the type of genomic test user ( appendix table a1 ) , oncologists with training in genomics had higher condence than those who did not . 
likewise , oncologists who treated 100 patients per month had higher condence than those who treated , 49 patients per month . compared with oncologists who treated both solid and hematologic malignancies , those who only treated solid tumors were more condent , whereas those who treated only hematologic malignancies were less condent in using results of multimarker panel tests to guide patient care . oncologists who practice in institutions with onsite pathology or emr alerts for recommended genomic tests had lower condence than those who practice in institutions without onsite pathology or emr alerts . 
for example , ngs and ge users who were very condent used multimarker panel test results to inform care for 30.97% of their patients ( who had received testing ) compared with 18.44% among ngs and ge users who were not at all or a little condent . 
oncologists condence in using results from ( a ) single - gene tests , ( b ) commercially available multimarker somatic panels , and ( c ) whole - genome or - exome sequencing to guide decisions about patient treatment and management ( n = 1 , 281 )  . 
on the basis of 2 tests for independence , overall differences in condence among 4 types of genomic test users were statistically signicant at p , .001 for single - gene tests , multimarker tumor panels , and whole - genome or - exome sequencing . discussion the current study adds to the literature on provider attitudes about genomic testing . 
most ge panel tests are used to inform the treatment of patients with breast cancer , and there are clear guidelines for test results.20 , 21 for users of other multimarker tumor panel tests , the application of test results to patient management is guideline endorsed for a limited set of clinical indications . testing and the interpretation of tumor panel tests to inform care is more complicated than using single - gene tests . 
at the time the survey was conducted , there were only consensus recommendations for multimarker tumor panel testing in treating nonsmall - cell lung cancer.23 despite this , providers condence using multimarker tumor panel tests was relatively high , with  . 75% of genomic test users reporting that they were either moderately or very condent in using results to guide patient care . 
these ndings are consistent with other studies of provider condence.15 , 24 - 26 oncologists condence also varied by test type , which is consistent with previous research.6 single - gene tests have been used for several decades as companion diagnostics to targeted therapies ; thus , clinical appropriateness and utility are well prescribed.22 even among genomic test nonusers , more than half reported being very condent in using single - gene tests to guide patient care . 
presented are adjusted percentages from multivariable linear regression models that were adjusted for years since graduation , sex , race , census region , specialty , training in genomics , practice setting , and infrastructure for precision medicine . 
historically , providers who treat patients with a hematologic malignancy have technologies ( eg , ow cytometry for relied on different immunophenotyping ) or single - gene somatic tests to identify relevant targeted therapies.27 in contrast , use of multimarker tumor panel tests has been more common in the treatment of solid tumors.23 the importance of experience was also highlighted in our ndings that providers who treat  . 
100 patients per month had higher condence than providers who treat , 50 . providers in high - volume clinics have more opportunity to encounter patients for whom multimarker tumor panel tests are warranted . 
indeed , patient volume has been associated with better treatment outcomes in other settings.28 providers in lower - volume clinics may benet from additional resources , including clinical decision support , to strengthen evidence - based use of genomic testing in treatment planning.29 our ndings underscore the importance of genomic training to increase provider condence in using multimarker panel tests to guide patient care . 
training was dened broadly and included any instruction during residency or fellowship , professional lectures , conferences , or continuing medical education in the use of genomic testing . additional research should identify the specic competencies needed by different types of oncologists and be tailored to support providers who demonstrate relatively low condence in using genomic testing in practice . 
several categories of training could be pursued , including revision of the curricula of medical and nursing schools to provide training in genomics ; advanced training of physicians and other practitioners in genomics ; and continuing medical education to help practicing clinicians to stay up to date on advances in the eld.30 , 31 strategies such as case - based learning , clinical decision - support tools , administrative support for prior authorization , and clinical trial matching may be helpful in strengthening provider condence around genomic testing at the point of care and supporting successful implementation of precision medicine programs.29 genomic testing services available in an oncologists primary practice were either not associated with provider condence or , paradoxically , associated with lower condence . 
oncologists who reported that their practice had onsite pathology spent a lower percentage of time in delivering patient care ( data not shown ) , which could have inuenced their condence in using genomic test results to guide treatment decisions . 
oncologists in settings with onsite pathology could also have been more likely to have a research focus outside of genomics , although that is not something we can explore with our data . in addition , it is possible that other features of the practice setting or availability of appropriate training were more important drivers of provider condence . 
this work should address both the knowledge and the skills to use genomic testing appropriately and to act on test results as well as system - level resources to support precision oncology . our study results should be considered in light of a few limitations . 
first , providers were asked generally about their condence in using genomic test results to guide patient care ; we do not know how condence with a particular testing approach may vary on the basis of specic patient subgroups or clinical scenarios . 
however , participants are representative of practicing oncologists in the united states in terms of age , sex , and geographic location , and all analyses were weighted to adjust estimates for survey nonresponse . 
de moor , phd , mph , healthcare delivery research program , division of cancer control and population sciences , national cancer institute , 9609 medical center dr , room 3e438 , rockville , md 20850 ; e - mail : demoorjs@mail.nih.gov. support supported by the national cancer institute ( nci ) , national human genome research institute , and american cancer society through nci contract no . 
gray stock and other ownership interests : magenta therapeutics ( i ) consulting or advisory role : grail industries , magenta therapeutics ( i ) expert testimony : riley and associates no other potential conicts of interest were reported . references kalia m : biomarkers for personalized oncology : recent advances and future challenges . 
morganti s , tarantino p , ferraro e , et al : complexity of genome sequencing and reporting : next generation sequencing ( ngs ) technologies and implementation of precision medicine in real life . 
crit rev oncol hematol 133 : 171 - 182 , 2019 el - deiry ws , goldberg rm , lenz hj , et al : the current state of molecular testing in the treatment of patients with solid tumors , 2019 . 
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genet test mol biomarkers 19 : 657 - 665 , 2015 tan o , shrestha r , cunich m , et al : application of next - generation sequencing to improve cancer management : a review of the clinical effectiveness and costeffectiveness . 
j clin oncol serv res 9 : 131 , 2009 33 : 2753 - 2762 , 2015 johnson db , dahlman kh , knol j , et al : enabling a genetically informed approach to cancer medicine : a retrospective evaluation of the impact of comprehensive tumor proling using a targeted next - generation sequencing panel . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
freedman an , klabunde cn , wiant k , et al : use of next - generation sequencing tests to guide cancer treatment : results from a nationally representative survey of oncologists in the united states . 
duffy mj , harbeck n , nap m , et al : clinical use of biomarkers in breast cancer : updated guidelines from the european group on tumor markers ( egtm )  . 
godin g , b elanger - gravel a , eccles m , et al : healthcare professionals intentions and behaviours : a systematic review of studies based on social cognitive theories . 
implement sci 3 : 36 , 2008 johnson lm , valdez jm , quinn ea , et al : integrating next - generation sequencing into pediatric oncology practice : an assessment of physician condence and understanding of clinical genomics . 
allegretti m , fabi a , buglioni s , et al : tearing down the walls : fda approves next generation sequencing ( ngs ) assays for actionable cancer genomic 33 . 
pennell na , mutebi a , zhou z - y , et al : economic impact of next - generation sequencing versus single - gene testing to detect genomic alterations in metastatic nonsmall - cell lung cancer using a decision analytic model . 
unadjusted models of provider and practice characteristics associated with condence in using genomic test results to guide patient management not at all or a little condent moderately condent very condent moderately v not at all or a little condent very condent v not at all or a little condent total wtd % 95% ci wtd % 95% ci wtd % 95% ci 95% ci 95% ci overall p characteristic provider years since graduation 10 11 - 20 21 - 30  . 
unadjusted multinomial logistic regression models controlled for type of genomic test use , which was dened according to the multimarker somatic panel tests each oncologist used in the past 12 months . 
lum , md1 ; shirley zhu , md , mph1 ; sujay vennam1 ; erna forg o , md1 ; sushama varma , ms1 ; kristen ganjoo , md1 ; trevor hastie , phd3 ; rafck bowen , phd1 ; maria debiec - rychter , md , phd2 ; and matt van de rijn , md , phd1 purpose the preoperative distinction between uterine leiomyoma ( lm ) and leiomyosarcoma ( lms ) is difcult , which may result in dissemination of an unexpected malignancy during surgery for a presumed benign lesion . an assay based on circulating tumor dna ( ctdna ) could help in the preoperative distinction between lm and lms . 
we also proled 36 lm tumor specimens by exome sequencing to develop a panel for targeted detection of point mutations in ctdna of patients with lm . results we identied tumor - derived cnas in the plasma dna of 50% ( six of 12 ) of patients with lm . 
we identied only two recurrently mutated genes in lm tumors ( med12 and acly )  . conclusion our results show that lms do shed dna into the circulation , which provides an opportunity for the development of ctdna - based testing to distinguish lm from lms . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction uterine leiomyomas ( lms ) are common benign smooth muscle tumors that may present with symptoms similar to those associated with uterine leiomyosarcoma ( lms ) , a rare malignant tumor with a poor prognosis.1 with the exception of endometrial lesions , most uterine masses are not biopsied before surgery , and the preoperative distinction between benign and malignant uterine smooth muscle tumors relies primarily on clinical evaluation and imaging . 
as a result , patients may undergo surgery without a denitive distinction between the two entities . it is estimated that one in nine women in the united states will undergo a hysterectomy for benign gynein their lifetime.2 cologic indications , such as lm , power morcellation used to be performed in many in 2014 the us food and drug such cases , until administration discouraged the use of power morcellation for the removal of the uterus or uterine masses , after reporting that this procedure may lead to inadvertent retroperitoneal spread of an unsuspected malignancy in one in 305 patients.3 however , intraabdominal manual morcellation is still performed in patients with large masses diagnosed as lm , and although this is less aggressive than power morcellation , it still carries a risk for dissemination of an unexpected lms . 
risk factors that may favor the diagnosis of lms over lm include postmenopausal status , tamoxifen use , history of retinoblastoma , pelvic irradiation , hereditary leiomyomatosis , and renal cell cancer syndrome , 4 but these factors do not always correlate with a diagnosis of lms . also , the new emerging magnetic resonance imaging techniques present unsatisfactory positive predictive values for the distinction between lm and lms.4 therefore , there is a high need for improved methods for preoperative discrimination between benign lm and malignant tumors . 
in an attempt to improve the distinction between lm and lms , nagai et al5 developed a revised preoperative sarcoma score ( rpress ) based on patients age , serum lactate dehydrogenase ( ldh ) levels , and endometrial cytology ndings . 
 przybyl et al context key objective we sought to explore the feasibility of distinguishing between uterine leiomyoma and leiomyosarcoma based on the analysis of tumor - specic aberrations in circulating tumor dna ( ctdna )  . 
for this purpose , in the current study we aimed to determine whether uterine leiomyomas shed dna into the circulation . knowledge generated we demonstrate that it is feasible to detect ctdna derived from leiomyomas . 
in the limited number of cases analyzed to date , we show that these benign tumors do not carry alterations in tumor suppressor genes that can be detected in the ctdna of most patients with leiomyosarcoma . relevance our ndings are a rst and necessary step toward developing a blood test that , together with clinical and imaging information , ultimately could help clinicians to better evaluate the risk of leiomyosarcoma in a patient presenting with a uterine mass . was developed in a group of 63 patients with lm and lms but has not yet been validated in an independent study . we recently demonstrated that tumor - associated genetic aberrations can be detected in the circulating tumor dna ( ctdna ) of patients with lms.6 in that study , we used two technologies to detect different classes of genomic aberrations in plasma dna : cancer personalized proling by deep sequencing ( capp - seq ) for the analysis of point mutations , 7 , 8 and a genome - wide interrogation of copy number alterations ( cnas ) by shallow whole - genome sequencing.9 , 10 using these two approaches , we were able to detect ctdna in six of seven patients with lms with  . 
the study was approved by the stanford university institutional review board ( irb - 31067 )  . proling plasma cell - free dna cell - free dna was extracted from plasma using qiaamp circulating nucleic acid kit ( qiagen )  . 
sequencing libraries were prepared with the truseq chip preparation kit ( illumina , foster city , ca ) and sequenced using hiseq 2500 instrument ( illumina ) ( data supplement )  . plasma ldh measurement plasma ldh levels were measured on a roche cobas 8000 ( roche , indianapolis , in ) automated platform ( data supplement )  . proling tumor specimens genomic dna extracted from 12 archival lm tumor specimens and germline dna extracted from patient - matched blood leukocytes were used for genome - wide copy number proling with the oncoscan ffpe assay ( thermo fisher scientic / affymetrix , santa clara , ca )  . thirty - six archival lm tumor specimens and normal patientmatched counterpart tissues or peripheral blood leukocytes were used for whole - exome sequencing using the seqcap ez human exome v3.0 library ( roche ) on hiseq 4000 instrument ( illumina ) ( data supplement )  . results tumor - derived copy number aberrations can be detected in plasma dna of patients with lm to explore the possibility of developing a blood - based test for the distinction between lm and lms , we rst determined whether lm can shed dna in the blood . 
we calculated genome - wide segmented z - scores in plasma cell - free dna , and we intersected each genomic region of cnas identied in the eight lm tumor specimens with the segments identied in plasma dna of the matching patients . 
of the 33 cnas detected in the eight tumor specimens , 30 cnas had the same type of copy number alteration in tumor and plasma dna ( ie , matching dna copy number gain or loss ; data supplement )  . 
1.5 in cell - free dna , we found 11 tumor - derived cnas in the plasma dna of six patients with lm ( correlation between log2 ratio in the tumor and z - score in the plasma determined by linear regression was r2 = 0.74 ; p value = .0007 ; table 3 ; appendix fig a1 )  . 
selected large dna cnas identied in lm tumor specimens were not detected in plasma specimens , which is most likely the result of the limit of detection of our method and / or the effect of stochastic sampling of blood specimens . 
we have previously demonstrated that it is possible to detect tumorderived cnas in cell - free dna among patients with lms using the same technology as applied to the patients with lm in the current study.6 we sought to verify whether the aberrations found in ctdna of patients with lm in the present report are specic to these benign tumors or whether the same aberrations could be found also in lms tumor specimens . 
for this purpose , we reanalyzed the previously generated genomic proles of 22 tumors from seven patients with lms using exactly the same criteria as were used for the lm tumor specimens . 
our results show that 10 of 11 genomic aberrations found in the ctdna of patients with lm were also present in the tumor dna of patients with lms analyzed in our previous study , 6 with a median of four aberrations per lms tumor sample ( range , 1 - 8 )  . 
these results demonstrate that the majority of cnas found in lm tumors are not specic for this entity ; therefore , proling these cnas in plasma dna may not be useful to distinguish between lm and lms . 
on the other hand , cnas found in lm specimens did not affect any of the frequently deleted tumor suppressor genes in lms ( eg , tp53 , rb1 , atrx , pten , atm , or cdkn2a )  . 
therefore , the detection of cnas in these tumor suppressor genes in ctdna may favor a diagnosis of lms . patient age and levels of ldh do not allow for distinction between lm and lms previous studies have proposed that ldh level measurements and patient age may be helpful in the distinction between lm and lms.5 , 11 we evaluated the ldh levels in plasma specimens of nine of 12 patients with lm proled for the presence of ctdna and eight untreated patients with uterine lms . 
in the rpress algorithm , the cutoff of serum ldh levels indicative of lms was set at 279 u / l.5 in our group of patients , the sensitivity and specicity values of this test were found to be only 50% and 89% , respectively . 
the mean age of the patients with lm and lms was 48 and 54 years , respectively ( t test two - tailed p value = .19 ; fig 2b )  . 
this performance was poorer than the ndings reported in the rpress study , where the sensitivity , specicity , positive predictive value , and negative predictive value were 93% , 65% , 45% , and 97% , respectively.5 low mutation burden in lm previous genomic studies of lm have identied med12 as the most frequently mutated gene in these lesions , but these studies did not report on other recurrent somatic mutations in these tumors.12 - 14 however , med12 mutations have been reported also in a subset of lms tumors , and therefore these mutations cannot be used for a molecular distinction between lm and lms.15 to investigate whether lm tumors might have recurrently mutated genes other than med12 , we performed whole - exome sequencing on 36 pairs of matched tumor and normal dna specimens from patients with lm . 
mutations in exon 2 of med12 were identied in 39% ( 14 of 36 ) of lm tumor specimens , and the acly gene was mutated in 6% ( two of 36 ) of lm tumor specimens ( data supplement )  . 
mutations in these two genes were present in 15 of 36 patients , with a median of one mutation per tumor ( range , 0 - 2 across all 36 tumors )  . 
all med12 mutations identied in our study were previously reported in the cosmic database ( cosmic v84 ; accessed on november 12 , 2018 ) .16 our results show that recurrent mutations other than in the med12 gene rarely occur in lm . 
importantly , we did not detect in any lm case any of the mutations in tumor suppressor genes that are frequently mutated in lms , such as tp53 , rb1 , pten , atrx , atm , and arid1a.6 this indicates that mutations in these driver genes may be highly specic to malignant tumors such as lms . 
because lms do not carry mutations in these tumor suppressor genes , we propose that detection of these mutations in plasma dna of patients with uncertain diagnosis , using the capp - seq lms - specic panel developed in our previous study , may favor the diagnosis of lms . discussion the clinical utility of ctdna proling has been widely demonstrated in malignant tumors that harbor highly recurrent mutations.7 , 8 , 17 , 18 currently , the two most frequently used sequencing - based approaches for ctdna monitoring include deep targeted sequencing for ultrasensitive quantitative analysis of point mutations , such as capp - seq , and shallow whole - genome sequencing for the detection of cnas . 
histologic appearance of representative leiomyoma ( lm ) cases with ( a ) no detectable dna copy number alterations , ( b ) 20 dna copy number alterations , and ( c ) six dna copy number alterations . 
however , it is not practical to design an lm - specic capture panel for detection of point mutations by deep targeted sequencing of ctdna , because we identied only two recurrently mutated genes in a low percentage of 36 lm tumors . we assume that an approximately two - fold increase of coverage may result in improving the reliability of the calls , by reducing the number of false - positive calls and increasing the number of true - positive calls.22 moreover , most of the patients included in our study had multifocal disease , and we expect that proling all nodules from these patients would reveal a wider spectrum of cnas and thus allow for the detection of overlapping aberrations between plasma and tumor dna in a higher percentage of patients with lm . although ctdna released from malignant tumors has been well characterized in multiple types of cancer , ctdna derived from benign lesions has not been extensively studied . an incidental nding of lm - derived dna in the circulatory system has been reported in pregnant women undergoing noninvasive prenatal testing ( nipt )  . 
dharajiya et al19 reported unexpectedly abnormal nipt proles in 55 of 450 , 000 pregnant women tested for fetal aneuploidy ; 20 of these 55 women were known to have had lm at the time of nipt . 
but the genomic prole of a matching tumor was examined only in a single patient from this group to conrm levels of cell - free dna were indeed that the abnormal derived from this lm.19 although these incidental ndings indicated that lm can shed dna into the circulatory system , the overall sensitivity of shallow whole - genome sequencing for the detection of lm - derived ctdna has not been investigated . 
in the current study , by prospective analysis of plasma and tumor samples of 12 patients with lm , we found ctdna in 50% of these patients , which is a comparable detection rate to the current sensitivity of ctdna detection in many stage i cancers.20 , 21 importantly , the nipt assays used for detecting fetal abnormalities usually focus solely on screening for monosomy or trisomy of chromosomes 13 , 18 , and / or 21 . 
in the current study , instead of focusing only on selected chromosomes , we performed a genome - wide analysis in which we aimed to detect not only chromosome - wide aberrations but also small focal aberrations . 
we performed shallow whole - genome sequencing at approximately 0.1 genomewide coverage ; however , we expect that deeper sequencing would allow for the detection of ctdna in a higher percentage of patients with lm . 
on the basis of previously published studies , it must be noted that the development of a reliable assay for the distinction between lm and lms is challenged by the great difference in prevalence of these two entities . 
 circulating tumor dna in leiomyoma predictive value for any positive result indicating lms would be only 2% , while the negative predictive value of a negative result would be 99.99%. 
on the basis of the genomic proles of lm and lms , we propose that it may be more practical to apply an assay that would rule out the diagnosis of lm . 
this could be possible by applying capp - seq for detection of mutations in tumor suppressor genes that are frequently mutated in lms but have never been reported in lm . 
regardless , given the statistical considerations on the prevalence of lm and lms , validation of such assay in the clinical setting may be challenging and would require a very large prospective study . in summary , we demonstrate in the current study that a substantial portion of lms do shed dna into the circulatory systethese ndings provide an opportunity to develop a noninvasive test for distinction between lm and lms on the basis of ctdna in plasma . 
lyon , iarc , 2014 , in kurman rj , carcangiu ml , herrington cs , et al ( eds ) : who classication of tumours of female reproductive organs . 
nagai t , takai y , akahori t , et al : highly improved accuracy of the revised preoperative sarcoma score ( rpress ) in the decision of performing surgery for patients presenting with a uterine mass . 
nat biotechnol 34 : 547 - 555 , 2016 1 : 814 - 819 , 2015 334 : 252 - 255 , 2011 bayindir b , dehaspe l , brison n , et al : noninvasive prenatal testing using a novel analysis pipeline to screen for all autosomal fetal aneuploidies improves pregnancy management . 
goto a , takeuchi s , sugimura k , et al : usefulness of gd - dtpa contrast - enhanced dynamic mri and serum determination of ldh and its isozymes in the differential diagnosis of leiomyosarcoma from degenerated leiomyoma of the uterus . 
m akinen n , mehine m , tolvanen j , et al : med12 , the mediator complex subunit 12 gene , is mutated at high frequency in uterine leiomyomas . 
wan r , wang z , lee jj , et al : comprehensive analysis of the discordance of egfr mutation status between tumor tissues and matched circulating tumor dna in advanced non - small cell lung cancer . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
sci transl med van beek dm : detection of copy number variation using shallow whole genome sequencing data to replace array - comparative genomic hybridization analysis [ masters thesis ]  . 
heitzer e , ulz p , belic j , et al : tumor - associated copy number changes in the circulation of patients with prostate cancer identied through whole - genome 27 . 
karczewski kj , francioli lc , tiao g , et al : variation across 141 , 456 human exomes and genomes reveals the spectrum of loss - of - function intolerance across 37 . 
correlation between log2 ratio in tumor dna and z - score in cell - free dna for 11 tumor - derived copy number alterations detected in plasma of leiomyoma patients . 
although from their analysis , her2 exon 20 mutations emerge as the most clearly actionable driver in nsclc , the authors themselves pinpoint ambiguous functional roles of individual her2 aberrations ( ie , activating mutations , amplication , and overexpression ) , as well as their reciprocal associations . therefore , her2 biology may be different in lung cancer compared with breast or gastric cancers , possibly because of specic microenvironmental and tumor - host interactions . as pointed out by the authors , a substantial heterogeneity exists in therapeutic approaches and clinical results of her2 - targeting strategies in this context . this is well exemplied by two clinical nsclc cases harboring different her2 alterations ( her2 mutation and all three her2 aberrationsmutation , amplication , and protein overexpression , respectively ) we discuss herein . case 1 a 44 - year - old woman , never - smoker , presented with stage ivb lung adenocarcinoma ( egfr - wt , alk and ros1 nonrearranged , pd - l1 1% )  . 
she was then treated with two courses of atezolizumab , resulting in clinico - radiologic hyperprogression.2 next - generation sequencing ( ngs ) based molecular proling revealed a her2 exon 20 insertion ( p.a775_ g776insyvma ) ; neither gene amplication nor protein expression was detected . 
she then received whole - brain radiotherapy ( rt ) for an isolated brain progression and was subsequently enrolled in a clinical trial of poziotinib ; treatment was poorly tolerated , and diffuse extracranial progression rapidly ensued . 
rechallenge with trastuzumab and vinorelbine obtained no clinical benet , and she went on to receive gemcitabine single agent and subsequently best supportive care on further clinicoradiologic disease progression . case 2 a 48 - year - old woman , never - smoker , presented with stage iib lung adenocarcinoma in 2011 , when she underwent left inferior lobectomy and medilymphadenectomy followed by adjuvant astinal cisplatin / vinorelbine . 
in 2018 , disease recurred in multiple metastatic sites ; right supraclavicular lymph node rebiopsy showed egfr - wt , alk and ros1 nonrearranged , and pd - l1 1% , and she received rstline platinum - based chemotherapy with partial response , followed by stereotactic body rt on residual tumor sites ; multisite disease progression was observed 2 months after treatment completion . 
she was then started on trastuzumab emtansine ( tdm - 1 ) in march 2020 , experiencing dramatic clinical benet with disappearance of all disease - related symptoms , in particular dyspnea , and performance status improvement ( from 2 to 0 , according to eastern cooperative oncology group ) ; treatment is currently ongoing . the two cases presented highlight the inherent complexity of her2 biology in nsclc and the difculties in reliably predicting the clinical outcome of specic her2 - targeted interventions . 
in case 1 , a clinically meaningful response to trastuzumab - based treatment was observed , in line with other reports , 3 - 5 even in the presence of an isolated exon 20 mutation not accompanied by gene amplication and in the absence of protein expression by immunohistochemistry . 
intrigued by the relatively unexpected response , occurring after hyperprogression to pd - l1 blockade , we analyzed fcriiia polymorphisms and found that the patient carried a valine / valine ( v / v ) variant , which has been correlated to better response to trastuzumab - based treatment in breast cancer.6 in line with the presence of a polymorphism potentially fostering antibody - dependent cell - mediated cythe patients peripheral blood totoxicity ( adcc ) , mononuclear cells displayed a marked and specic trastuzumab - dependent cytotoxic activity toward her2 - overexpressing targets in vitro ( fig 1 )  . 
on the other hand , such a mechanism did not prove relevant in case 2 , in which no response to trastuzumab - based treatment was observed , despite gene amplication and protein overexpression accompanying exon 20 insertion . 
 ( a ) computed tomographic imaging of primary lesion at baseline ( showing atezolizumab progression , left ) and at rst assessment during trastuzumab - based therapy ( right )  . 
 ( b ) mcf7 target cells , expressing ( mcf7 - her2 ) or not expressing ( mcf7 - evector ) her2 antigen , were rst stained with carboxyuorescein succinimidyl ester ( cfse ) 5 mm and celltrace 5 mm , respectively . 
mixed targets ( ratio 1 : 1 ) were incubated for 18 hours at different ratios ( 2 : 1 , 4 : 1 , 8 : 1 , 12 : 1 ) with peripheral blood mononuclear cells ( pbmcs ) isolated from peripheral blood of the patient in the presence of rituximab ( 10 mg / ml ) or trastuzumab ( 10 mg / ml )  . 
tumor cellspecic lysis by pbmcs was analyzed by ow cytometry ( representative plot of 8 : 1 ratio on the left ) and quantied as percentage of lysis ( right ) using the formula : ( 1 ( % mcf7 - her2 or mcf7 - evector + trastuzumab / tot target ) / ( %mcf7 - her2 or mcf7 - evector + rituximab / tot target ) 100 )  . 
fitc , uorescein isothiocyanate ; v450 - ct , v450 cell trace . overall , her2 aberrations in nsclc convey important prognostic10 and potentially predictive information ; however , prospective studies should be designed not only according to patients stratication for specic her2 aberration ( s ) or combinations but also it is mandatory to evaluate the patients immunologic features , especially for antibody - based treatments . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . zhao j , xia y : targeting her2 alterations in nonsmall - cell lung cancer : a comprehensive review . 
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mazi `eres j , peters s , lepage b , et al : lung cancer that harbors an her2 mutation : epidemiologic characteristics and therapeutic perspectives . j clin oncol 31 : 1997 - 2003 , 2013 6 . 
musolino a , naldi n , bortesi b , et al : immunoglobulin g fragment c receptor polymorphisms and clinical efcacy of trastuzumab - based therapy in patients with her - 2 / neu - positive metastatic breast cancer . 
j clin oncol 26 : 1789 - 1796 , 2008 li b , ofn m , hembrough t , et al : p1.13 - 43 molecular and imaging predictors of response to ado - trastuzumab emtansine in patients with her2 mutant lung cancers : an exploratory phase 2 trial . 
j thorac oncol 13 : s599 , 2018 li bt , shen r , buonocore d , et al : ado - trastuzumab emtansine for patients with her2 - mutant lung cancers : results from a phase ii basket trial . 
j clin oncol 36 : 2532 - 2537 , 2018 peters s , stahel r , bubendorf l , et al : trastuzumab emtansine ( t - dm1 ) in patients with previously treated her2 - overexpressing metastatic non - small cell lung cancer : efcacy , safety , and biomarkers . 
milella m , nuzzo c , bria e , et al : egfr molecular proling in advanced nsclc : a prospective phase ii study in molecularly / clinically selected patients pretreated with chemotherapy . 
responses to avelumab were observed regardless of pd - l1 expression , the presence or absence of tumor - inltrating therapy , and lymphocytes , multiple prior lines of somatic or germline origin of mmrd , which suggests that baseline clinical and pathologic characteristics could not predict response . 
ten of the 12 tumors were determined to be mmrd by oncopanel on the basis of mutational signature analysis using two independent algorithms , 4 , 5 which was consistent with the ihc determination . 
the remaining 2 tumors were determined to be mmrp by oncopanel and microsatellite stable using polymerase chain reactionthat is , both oncopanel and polymerase chain reaction were discordant with ihcand none of them responded to avelumab . 
 ( b ) frequency of common jak1 and b2m mutations found in our data set are compared with the frequency in the mismatch repairdecient ( mmrd ) endometrial cancers ( ecs ) from the cancer genome atlas ( tcga )  . 
fs , frameshift ; fsdel , frameshift deletion ; fsins , frameshift insertion ; nr , nonresponder ; or , objective response ; r , responder ; recur , recurrent . 
therefore , these 2 tumors were more likely to be mmrp and were excluded from the analysis . of the remaining 10 patients ( table 1 ) with tumors determined to be mmrd using both ihc and oncopanel , 3 exhibited an objective response to avelumab ( responders ) , whereas 7 did not ( nonresponders )  . 
all 7 nonresponders harbored either jak1 ( 6 tumors ) or b2m mutations ( 1 tumor ) , while only 1 of the 3 responders harbored a jak1 mutation ( fisher exact test , two - sided p = .067 ; fig 1a )  . 
in addition , of the 7 nonresponders , 4 harbored two mutations of jak1 ( 3 tumors ) or b2m ( 1 tumor ) , possibly reecting biallelic inactivation of these genes . 
all jak1 mutations were frameshift ( deletions or insertions ) , with the exception of two missense mutations that occurred together with frameshift mutations : a missense mutation q750r on the pseudokinase domain ( exon 16 ) and a missense mutation l1071p toward the end of the kinase domain ( exon 23 )  . 
frameshift jak1 mutations involved the hotspot position k860 / p861 ( deletions in 5 tumors and insertion in 1 tumor ) and the hotspot position p430 / l431 ( insertions in 2 tumors )  . 
 ( a ) number of indels , deletions , insertions , and tumor mutational burden , dened as the number of nonsynonymous mutations per mb for responders ( r ) and nonresponders ( nr ) in our data set . 
 ( b ) same as panel a comparing patients with endometrial cancer ( ec ) in the cancer genome atlas ( tcga ) data set with and without frameshift jak1 mutations . 
furthermore , in another data set ( msk - imp ) , which included 29 patients with recurrent mmrd ecs ( dened by ihc ) , 6 the overall frameshift jak1 mutations was 51.7% cidence of signicantly higher than that in the tcga data set , but comparable with that in our data set ( fig 1c )  . 
nonresponders had a signicantly higher number of total deletion mutations compared with responders ( p = .03 ) , but the number of total insertion mutations was not different ( fig 2a )  . 
 ( a ) exposure ( left ) and fraction ( right ) , dened as the exposure divided by the total number of single - nucleotide variants of signatures 20 . 
bottom : blue and red boxes and points indicate cases with and without frameshift ( fs ) jak1 mutations in whole - exome sequencing data from the cancer genome atlas ( tcga )  . 
to calculate the fraction , the exposure of each mmrd signature is divided by the sum of exposures of all mmrd signatures ( the contribution of the non - mmrd signatures is not shown as they did not vary signicantly across data sets )  . 
konstantinopoulos , md , phd , dana - farber cancer institute , 450 brookline ave , boston , ma 02115 ; e - mail : panagiotis_ konstantinopoulos@dfci.harvard.edu. support supported by the ludwig center at harvard and by a fund in memory of bina sareen . 
gulhan patents , royalties , other intellectual property : a provisional patent application is being drafted for an algorithm developed by the author for which a coversheet provisional has been led on september 24 , 2018 , titled computational method to identify mutational signatures from sequencing data ( inst ) joyce f . 
liu consulting or advisory role : tesaro , mersana , clovis oncology , genentech , glaxosmithkline research funding : genentech ( inst ) , astrazeneca ( inst ) , boston biomedical ( inst ) , atara biotherapeutics ( inst ) , acetylon ( inst ) , bristolmyers squibb ( inst ) , agenus ( inst ) , cytomx therapeutics ( inst ) , regeneron ( inst ) , tesaro ( inst ) , clovis oncology ( inst ) , surface oncology ( inst ) , 2x oncology ( inst ) , vigeo therapeutics ( inst ) , aravive ( inst ) , arch oncology ( inst ) travel , accommodations , expenses : astrazeneca , merck uncompensated relationships : merck , astrazeneca ursula a . 
konstantinopoulos consulting or advisory role : merck , vertex , astrazeneca , pzer , emd serono , tesaro , bayer research funding : pzer ( inst ) , eli lilly ( inst ) , tesaro ( inst ) , merck serono ( inst ) , astrazeneca ( inst ) , merck ( inst ) , bayer ( inst ) no other potential conicts of interest were reported . references aghajanian c , sill mw , darcy km , et al : phase ii trial of bevacizumab in recurrent or persistent endometrial cancer : a gynecologic oncology group study . 
j clin oncol 29 : 2259 - 2265 , 2011 alvarez ea , brady we , walker jl , et al : phase ii trial of combination bevacizumab and temsirolimus in the treatment of recurrent or persistent endometrial carcinoma : a gynecologic oncology group study . 
gynecol oncol 129 : 22 - 27 , 2013 konstantinopoulos pa , luo w , liu jf , et al : phase ii study of avelumab in patients with mismatch repair decient and mismatch repair procient recurrent / persistent endometrial cancer . 
j mol diagn 19 : 84 - 91 , 2017 gulhan dc , lee jj , melloni gem , et al : detecting the mutational signature of homologous recombination deciency in clinical samples . 
nat genet 51 : 912 - 919 , 2019 soumerai te , donoghue mta , bandlamudi c , et al : clinical utility of prospective molecular characterization in advanced endometrial cancer . 
clin cancer res 24 : 5939 - 5947 , 2018 alexandrov lb , nik - zainal s , wedge dc , et al : signatures of mutational processes in human cancer . 
gao j , shi lz , zhao h , et al : loss of ifn - gamma pathway genes in tumor cells as a mechanism of resistance to anti - ctla - 4 therapy . 
albacker la , wu j , smith p , et al : loss of function jak1 mutations occur at high frequency in cancers with microsatellite instability and are suggestive of 15 . 
howitt be , shukla sa , sholl lm , et al : association of polymerase e - mutated and microsatellite - instable endometrial cancers with neoantigen load , number of tumor - inltrating lymphocytes , and expression of pd - 1 and pd - l1 . 
 returning individual genetic research results to research participants : uptake and outcomes among patients with breast cancer purpose understanding the outcomes of returning individual genetic research results to participants is critical because some genetic variants are found to be associated with health outcomes and have become available for clinical testing . materials and methods brca1 / 2 - negative women with early - onset breast cancer , multiple primary cancers , or a family history of breast cancer who participated in a gene discovery cancer registry were offered the opportunity to learn their individual genetic research results of 24 breast cancer susceptibility genes with a genetic counselor after predisclosure genetic counseling . 
outcomes included uptake of research results , knowledge , informed choice , psychosocial adjustment , uncertainty , satisfaction , and uptake of clinical confirmation testing . results four hundred two potential participants were contacted . 
sixty - four percent of participants had clinical confirmation testing when recommended , including all participants with a mutation in a high - penetrance gene . conclusion uptake of genetic research results may be lower than anticipated by hypothetical reports and small select studies . 
2018 by american society of clinical oncology introduction as large studies with banked dna are increasingly used in genetic sequencing studies , there has been increasing debate over the obligation to share individual research results with research participants.1 - 7 over time , genetic variants identified in research may be found to be associated with health outcomes and may become available in clinical practice.8 , 9 arguments against returning research results include a blurring of the distinction between research and clinical care , misunderstanding , the right not to know , and costs.3 , 7 , 10 - 17 others argue that results should be returned based on the principles of beneficence , autonomy , reciprocity , and respect for persons.6 , 18 - 25 there remains no consensus on how and which results should be returned.1 - 7 , 26 - 28 numerous studies have reported high interest in receiving research results , even if the patients knew there was nothing they could do about the results.29 - 35 although some argue that only actionable results from a laboratory certified by angela r . 
 the clinical laboratory improvement amendments ( clia ) should be returned , 3 , 36 , 37 others argue that research results should be offered to patients more broadly , allowing patients to make decisions about which results they would like to receive , with recommendations for clia confirmation for results that could change clinical care.6 , 20 , 21 , 38 - 41 in the few studies reporting uptake of research results ( as opposed to hypothetical interest ) , uptake varied considerably ( 17% to > 80% ) in cohorts with cancer.42 - 48 most studies returned results with recommendations to have confirmatory clia testing , but none report on uptake of confirmatory testing , 42 - 44 , 48 , 49 and the majority of these studies were small , with select populations and limited outcomes.42 - 45 , 50 - 52 in the returning genetic research panel results for breast cancer susceptibility ( respect ) study , we sought to evaluate uptake of research results in patients with breast cancer who participated in the research registry , factors associated with uptake of results , and participant cognitive and affective outcomes . 
five hundred two samples from brca1 / 2 - negative women with breast cancer and with a diagnosis at < 40 years of age , multiple primary cancers , or at least three firstor second - degree relatives with breast cancer were selected for sequencing of 24 breast cancer susceptibility genes ( cdh1 , cdkn2a , mlh2 , msh2 , epcam , msh6 , mutyh homozygous , pms2 , pten , stk11 , tp53 , atm , bap1 , bard1 , bmpr1a , brip1 , chek2 , mre11a , mutyh heterozygous , nbn , palb2 , rad50 , rad51c , and rad51d ) for related research.53 sequencing was by either targeted or whole - exome hybrid capture methodologies , as described.53 - 55 all potential participants were checked against a death index and were confirmed to have permission for recontact . 
the letter explained that everyone whose research sample had been tested was being invited to participate in the study ( ie , that the invitation was not an indication of a positive result )  . 
this was the only method provided to participants to receive their research results . predisclosure and result disclosure genetic counseling predisclosure genetic counseling sessions using the tiered - binned model were conducted by genetic counselors ( n = 5 ) via phone or in person.56 , 57 genetic counselors were blinded to the results at predisclosure and completed counseling checklists for all sessions . 
genetic counselors shared the need for clinical confirmation when applicable and any clinical genetic testing consistent with current clinical practice . confirmatory testing in a clia - certified laboratory participants with a deleterious or likely deleterious research result in any gene and a variant of uncertain significance ( vus ) in a high penetrance gene were recommended to have clinical confirmation of the research finding . 
 assessed for eligibility ( n = 582 ) contacted by letter for ror ( n = 402 ) excluded ineligible deceased no permission to recontact ( n = 180 ) ( n = 35 ) * ( n = 64 ) ( n = 81 ) ineligible no response mailing returned called but not reached discussed ror but never enrolled declined ( n = 16 ) ( n = 194 ) ( n = 14 ) ( n = 180 ) ( n = 62 ) ( n = 23 ) interested in ror and consented completed t0 survey ( n = 107 ) ( n = 93 ) received predisclosure genetic counseling ( n = 91 by phone ; n = 1 in person ) completed t1 survey ( n = 86 ) declined receipt of results ( n = 9 ) || received genetic research result ( n = 81 by phone ; n = 2 in person ) deleterious / likely deleterious results vus results no findings ( n = 13 ) # ( n = 16 ) ( n = 54 ) completed t2 survey ( after disclosure ; n = 70 ) fig 1 . 
study flow diagra ( * ) seven patients were men , 12 had clinical multigene panel testing ( mgpt ) , five had return of results ( ror ) before returning genetic research panel results for breast cancer susceptibility ( respect ) study , and research charts were not available for 11 . 
 ( ) reasons for declining included concerns about research or time burdens , not being interested in genetic information , only wanting actionable results , preferring clinical testing , and concerns about uncertainty or distress . 
 ( ) three participants reported concerns about distress , three reported concerns about uncertainty , three reported a preference for clinical testing , three reported that they were not ready , and one was not ready at the time because of relative in hospice . 
we adjusted for individuals within the same family using cluster - corrected standard errors.73 in regression models , we excluded 26 of 372 participants who had missing data for continuous variables , race , or proband status . we used paired t tests for psychosocial responses between the first and second survey rounds . 
because only seven pairs of individuals within a same family had longitudinal data ( 7 2 = 14 individuals ) , we did not account for familial correlation in longitudinal analyses . 
we assumed exchangeable correlation matrices for generalized estimating equations . we did not find significant differences when comparing baseline response means between those who completed the first two surveys and those who completed all three surveys ( p > .28 in all cases )  . 
 similarly , we did not find significant differences in the second set of survey responses when comparing the same two groups ( p > .075 in all cases )  . 
a positive attitude about genetic testing was defined by a sum score at or greater than the midpoint of the scale.71 , 72 a more informed choice is defined by adequate knowledge and a testing decision concordant with attitudes about genetic testing . 
all other categories are considered less informed . results participant characteristics all of the 402 potential participants contacted had a history of breast cancer ; the mean age at diagnosis was 40.2 years old ( table 1 )  . 
 in a multiple logistic regression analysis , nonresponders were more likely to be older at the time of their first cancer diagnosis , to not have been seen in the clinical program ( eg , participated in research only ) , and to be nonwhite ( table 2 )  . 
variables included in the models were as follows : race ( nonwhite v white ) , married ( yes , no , or missing ) , children ( yes , no , or missing ) , seen in clinical cancer risk program ( yes , no , or missing ) , age at time of survey , number of fdrs or sdrs with breast cancer , number of fdrs or sdrs with any cancer , age at first diagnosis , and time since sample received . 
three hundred forty - six potential participants had complete data . abbreviations : fdr , first - degree relative ; or , odds ratio ; respect , returning genetic research panel results for breast cancer susceptibility ; sdr , second - degree relative . declined participation ( eg , communicated that they did not want to participate ) or passively declined participation ( eg , never responded after multiple contacts ) after learning about the study were more likely to have been younger age at cancer diagnosis and to have had a greater number of relatives with cancer ( table 2 )  . 
in a multiple logistic regression analysis , those who consented were more likely to be younger at the time of contact , married , and white ( table 2 )  . 
nine participants who had predisclosure counseling chose not to receive their results . informed decision making eighty - nine percent of participants ( 74 of 83 participants ) who had predisclosure counseling and completed relevant measures were classified as making an informed choice as defined by the mmic ( table 3 )  . 
making an informed choice was not associated with any demographic characteristics but was associated with a 2.0 - point change - score increase in research knowledge ( t test , p = .048 ) and marginally statistically significant 3.0 - point change score in total knowledge ( t test , p = .095 ) compared with participants who did not make an informed choice . patient - reported outcomes with receipt of genetic research results knowledge increased significantly after predisclosure counseling and receipt of results ( table 4 )  . 
frequency of making an informed choice using the tiered - binned predisclosure genetic counseling model adequate knowledge of genetic testing positive attitudes toward testing proceeded with receipt of research results all participants ( n = 83 ) , no . 
 ( % ) 74 ( 89 ) category informed choices category 1 category 2 category 3 category 4 category 5 category 6 category 7 category 8 less informed choices 9 ( 11 ) note . 
 anxiety declined significantly for participants with a positive and negative result , but cancer worry only declined significantly for those with a negative result . clinical confirmation testing and changes in medical management sixty - four percent of participants ( 14 of 22 participants ) had the recommended clinical confirmation testing ( fig 2 ) , and all recommended confirmation testing was covered by insurance , although one patient had a small out - of - pocket cost . 
clinical testing ( 14 samples with variants where confirmation testing was recommended and three samples where participants elected to have clinical testing to confirm a vus in a moderate - penetrance gene ) identified 16 of 17 variants identified by the research laboratory ( 94% ; appendix table a2 )  . 
for two samples , the research classification was vus and the clinical result by the commercial laboratory was benign , although other clinical laboratories also classify the variant as vus ( thus , discordant when compared with the call by the specific clinical laboratory used but not discordant with results in clinvar ) .75 for two samples , the research classification was likely deleterious , and the clinical result was reported as a vus . 
finally , clinical testing identified three additional variants that were not reported on research testing because they were considered likely benign by the research laboratory . discussion to our knowledge , this is the largest study offering a range of research genetic cancer susceptibility results ( eg , actionable mutations as well as no identified mutations , genes of variable clinical utility ) to research participants and collecting comprehensive outcomes as well as uptake of confirmatory testing in a commercial clia laboratory . 
although hypothetical query and some published studies have suggested high interest in receiving genetic research results , 29 , 30 , 48 , 76 in this study , we contacted > 400 research participants and only a small subset elected to receive research results . 
nonetheless , patient - reported outcomes for those who elected to receive results were favorable , with no significant increase in distress or uncertainty , even among subgroups receiving a positive or vus result . 
we found increases in understanding of the limitations of research testing and that the majority of participants made informed decisions about receiving individual genetic research results . of note , in our study , we were not able to reach 50% of research participants . 
although some studies have reported higher contact rates , 43 , 48 our rate is consistent with that in the kathleen cuningham foundation consortium for research into familial breast cancer cohort , where 62% of participants did not acknowledge receipt of an invitation to receive results.46 these data highlight that it may be more difficult than anticipated to reach research participants in some cohorts . 
 disparities in uptake and highlighting the need to better understand how to clearly communicate the opportunity to receive research results among diverse populations . in addition , 22% of research participants contacted actively or passively declined . 
these data are consistent with other studies reporting that some participants are not interested in receiving research results.49 , 76 , 79 , 80 until further data are available , researchers and institutional review boards considering return of results should anticipate that there will be a subset of participants who will not be interested in receiving results . although uptake was lower than anticipated in our study , the majority of participants who spoke with a genetic counselor elected to receive their research results , and most met criteria for making an informed choice with favorable patient - reported outcomes . 
our findings are consistent with the favorable patient - reported outcomes reported in the colon cancer family registry , 47 , 48 and our study included additional knowledge measures , patients with a wide range of results , and greater sociodemographic diversity . 
many studies have suggested that research participants and the lay public report interest in receiving genetic research results even when there is unclear utility or uncertainty.29 - 32 our findings support the premise that providing participants with a choice to receive a wide range of results may not be associated with negative psychosocial outcomes . 
outcomes could differ with different approaches , and providing results with a genetic provider for all research all ( 14 of 22 participants ) high - penetrance d / ld research result ( 3 of 3 participants ) moderate - penetrance d / ld research result ( 6 of 10 participants ) high - penetrance vus ( 5 of 9 participants ) participants will be challenge given the limited number of genetic counselors.81 importantly , all participants with a deleterious or likely deleterious finding in a high - penetrance gene proceeded with confirmation testing , and for the most part , this testing was covered by insurance . 
 however , returning only results obtained in a clia - certified research laboratory would deny some individuals critical medically actionable information that could be relevant to their health if subsequently confirmed in a clinical laboratory . 
 for a small number of participants , the return of results and confirmation in a clinical laboratory did change their medical management and , even more frequently , could have medical implications for their relatives . 
equally important , all 92 participants who had predisclosure counseling were candidates for clinical testing ( eg , they were all reasonable candidates for clinical multigene panel testing ) , but only 32% proceeded with some clinical testing . 
longitudinal data and further data will be needed to understand whether declining available clinical testing is based on informed preferences or potential misunderstandings or reliance on research results . although this study is , to our knowledge , the largest report of patient - reported outcomes in a sociodemographically diverse population receiving a wide range of genetic panel research results , we acknowledge several limitations . 
in addition , participants who did not respond could have had higher baseline distress , and these results may not reflect outcomes for all individuals who are contacted to receive research results . 
maxwell no relationship to disclose laura digiovanni employment : carevive research funding : carevive ( inst ) amanda brandt no relationship to disclose danielle mckenna no relationship to disclose jessica long employment : depuy synthes companies ( i ) stock and other ownership interests : depuy synthes companies ( i ) travel , accommodations , expenses : depuy synthes companies ( i ) jacquelyn powers employment : carevive systems honoraria : cureconnect consulting or advisory role : carevive systems travel , accommodations , expenses : hospital of the university of pennsylvania jill e . 
domchek honoraria : astrazeneca , clovis oncology research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , abbvie ( inst ) , pharmamar ( inst ) the pennsylvania department of health specifically disclaims responsibility for any analyses , interpretations , or conclusions . 
wallace se , kent a : population biobanks and returning individual research results : mission impossible or new directions ? hum genet 130 : 393 - 401 , 2011 5 . 
jarvik gp , amendola lm , berg js , et al : return of genomic results to research participants : the floor , the ceiling , and the choices in between . 
daly mb , pilarski r , berry m , et al : nccn guidelines insights : genetic / familial high - risk assessment : breast and ovarian , version 2.2017. 
berg js , amendola lm , eng c , et al : processes and preliminary outputs for identification of actionable genes as incidental findings in genomic sequence data in the clinical sequencing exploratory research consortiugenet med 15 : 860 - 867 , 2013 12 . 
fernandez cv , santor d , weijer c , et al : the return of research results to participants : pilot questionnaire of adolescents and parents of children with cancer . 
bollinger jm , scott j , dvoskin r , et al : public preferences regarding the return of individual genetic research results : findings from a qualitative focus group study . 
fullerton sm , wolf wa , brothers kb , et al : return of individual research results from genome - wide association studies : experience of the electronic medical records and genomics ( emerge ) network . 
wakefield ce , thorne h , kirk j , et al : improving mutation notification when new genetic information is identified in research : a trial of two strategies in familial breast cancer . 
keogh la , fisher d , sheinfeld gorin s , et al : how do researchers manage genetic results in practice ? the experience of the multinational colon cancer family registry . 
cacioppo cn , chandler ae , towne mc , et al : expectation versus reality : the impact of utility on emotional outcomes after returning individualized genetic research results in pediatric rare disease research , a qualitative interview study . 
maxwell kn , hart sn , vijai j , et al : evaluation of acmg - guideline - based variant classification of cancer susceptibility and non - cancer - associated genes in families affected by breast cancer . 
maxwell kn , wubbenhorst b , d ' andrea k , et al : prevalence of mutations in a panel of breast cancer susceptibility genes in brca1 / 2 - negative patients with early - onset breast cancer . 
bradbury ar , patrick - miller l , long j , et al : development of a tiered and binned genetic counseling model for informed consent in the era of multiplex testing for cancer susceptibility . 
lerman c , narod s , schulman k , et al : brca1 testing in families with hereditary breast - ovarian cancer : a prospective study of patient decision making and outcomes . 
kelly k , leventhal h , marvin m , et al : cancer genetics knowledge and beliefs and receipt of results in ashkenazi jewish individuals receiving counseling for brca1 / 2 mutations . 
pieterse ah , van dulmen am , beemer fa , et al : cancer genetic counseling : communication and counselees post - visit satisfaction , cognitions , anxiety , and needs fulfillment . 
cella d , hughes c , peterman a , et al : a brief assessment of concerns associated with genetic testing for cancer : the multidimensional impact of cancer risk assessment ( micra ) questionnaire . 
o ' neill sc , white db , sanderson sc , et al : the feasibility of online genetic testing for lung cancer susceptibility : uptake of a web - based protocol and decision outcomes . 
fiallos k , applegate c , mathews dj , et al : choices for return of primary and secondary genomic research results of 790 members of families with mendelian disease . 
wakefield ce , ratnayake p , meiser b , et al : for all my familys sake , i should go and find out : an australian report on genetic counseling and testing uptake in individuals at high risk of breast and / or ovarian cancer . 
crook a , plunkett l , forrest le , et al : connecting patients , researchers and clinical genetics services : the experiences of participants in the australian ovarian cancer study ( aocs )  . 
keogh la , southey mc , maskiell j , et al : uptake of offer to receive genetic information about brca1 and brca2 mutations in an australian population - based study . 
ultrasound imaging identied a hypoechoic nodule in the right breast ; right axillary lymph node ne - needle aspiration biopsy performed at previous hospital on day 13 revealed invasive carcinoma with a focal micropapillary pattern ( fig 1 )  . immunostaining of estrogen receptor ( er ) and progesterone receptor ( pgr ) was evaluated by using the allred score and the allred scores were positive ( proportion score [ ps ] 1 ( , 1% ) , intensity score [ is ] 2 ) and negative ( ps 0 , is 0 ) , respectively.12 , 13 the tumor was human epidermal growth factor 2 ( her2 ) negative ( immunohistochemistry [ ihc ] 0 )  . 
given these results , she was diagnosed with stage iv breast cancer . targeted next - generation sequencing ( ngs ) analysis using the foundationone companion diagnostic panel ( foundation medicine , cambridge , ma ) was performed on the right axillary lymph node specimen . 
the result of ngs was reported on day 58 , and the ngs identied a ccdc6 - ret fusion ( c1 ; r12 ) with no other reported genomic alterations known to contribute to human breast tumorigenesis , including none in brca1 or brca2 . 
consistent with local standard - of - care guidelines , she received treatment with tamoxifen plus goserelin from day 14 to day 91 , but these were discontinued due to progression in the right breast and new lesions detected in the left lower lung . 
rebiopsy of the right breast tumor revealed the following results : er allred score 2 ( ps 1 [ , 1% ] , is 1 ) , pgr allred score 2 ( ps 1 , is 1 ) , her2 ihc 2 + , her2 uorescence in situ hybridization negative ( her2 / her2 / cep ( centromere ) 17 = 0.9 ) , and programmed death ligand 1 ( sp142 ) expression on tumor - inltrating immune cells of 1% - 4% . 
on day 126 , she was started on treatment with selpercatinib at the recommended phase 2 dose of 160 mg twice daily in the libretto - 001 study after providing written informed consent from the patient to publish information and images . 
 case report sorafenib and vandetanib , multikinase inhibitors with preclinical inhibitory activity against ret , have been used to treat unselected patients with breast cancer , but minimal clinical activity was observed.14 , 15 a patient with ncoa4 - retpositive breast cancer experienced a partial response to the multikinase inhibitor cabozantinib in combination with trastuzumab and exemestane although the cabozantinib dose was reduced for toxicity , the total time on treatment was short , and the relative contribution of each agent to the overall antitumor activity was not known.8 in addition , although cabozantinib has preclinical inhibitory activity against ret , its much stronger inhibition of other kinases ( eg , vegfr2 ) likely accounts for its clinical activity.16 , 17 in contrast , in the current case , the highly selective and potent ret inhibitor selpercatinib demonstrated a durable singleagent response in a patient with ret fusionpositive breast cancer . to our knowledge , this is the rst report of a breast cancer patient with a complete and sustained response to selective , ret - targeted therapy and adds to the diversity of ret fusionpositive tumor types that may benet from selective ret inhibition . 
rothenberg , kazuhiko nakagawa financial support : elizabeth olek administrative support : elizabeth olek provision of study materials or patients : elizabeth olek collection and assembly of data : satomi watanabe , tomoyuki otani , takeshi yoshida , kazuko sakai , elizabeth olek , s . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . masayuki takeda honoraria : astrazeneca kk , chugai pharma , bristol - myers squibb , novartis , ono pharmaceutical kazuko sakai honoraria : roche diagnostics , bio - rad , astrazeneca , chugai pharma elizabeth olek employment : loxo oncology inc stock and other ownership interests : loxo oncology , inc travel , accommodations , expenses : loxo oncology , inc s . 
michael rothenberg employment : loxo , pzer stock and other ownership interests : loxo , pzer jennifer kherani employment : loxo oncology at lilly , ajax health , aisling capital , summus global leadership : ajax health and aisling capital stock and other ownership interests : ajax health and aisling capital consulting or advisory role : ajax health and aisling capital travel , accommodations , expenses : ajax health and aisling capital , loxo pearl p . 
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allison kh , hammond meh , dowsett m , et al : estrogen and progesterone receptor testing in breast cancer : american society of clinical oncology / college of american pathologists guideline update . 
miller kd , trigo jm , wheeler c , et al : a multicenter phase ii trial of zd6474 , a vascular endothelial growth factor receptor - 2 and epidermal growth factor receptor tyrosine kinase inhibitor , in patients with previously treated metastatic breast cancer . 
drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 17 . 
schlumberger m , elisei r , m uller s , et al : overall survival analysis of exam , a phase iii trial of cabozantinib in patients with radiographically progressive 2 , single - arm trial . 
konat e , phd1 ; biswajit das , phd3 ; chris karlovich , phd3 ; chih - jian lih , phd3 ; eric polley , phd9 ; richard simon , dsc1 ; ming - chung li , phd1 ; richard piekarz , md , phd1 ; and james h . 
although patients and physicians were blinded to the sequencing and random assignment results , a higher pretreatment dropout rate was observed in the control arm ( 22% ) compared with the experimental arm ( 6% ; p = .038 ) , suggesting that some patients may have had prior tumor mutation proling performed that led to a lack of participation in the control arm . conclusion further investigation , better annotation of predictive biomarkers , and the development of more effective agents are necessary to inform treatment decisions in an era of precision cancer medicine . 
increasing prevalence of tumor mutation proling and preference for targeted therapy make it difcult to use a randomized phase ii design to evaluate targeted therapy efcacy in an advanced disease setting . jco precis oncol 5 : 133 - 144 . 
to explore this , we conducted a randomized , histology - agnostic clinical to examine whether patients with advanced , refractory cancer who had a tumor mutation in a gene in one of three signaling pathways ( dna repair , pi3k , or ras / raf / mek ) were more likely to derive clinical benet if treated with regimens targeting that pathway ( the experimental arm ) than if they were treated with regimens that did not ( the control arm )  . 
 chen et al context key objective a molecular aberration in a patients tumor is expected to render the tumor susceptible to a drug targeting that aberration , but randomized , controlled , blinded phase ii trials conrming the efcacy of this precision medicine approach are both sparse and challenging to design . knowledge generated efcacy in patients with study - dened actionable mutations in the dna repair , ras / raf / mek , or akt / pi3k / mtor pathways either did not achieve the target objective response rate ( trametinib or adavosertib with carboplatin ) or indicated futility despite accrual challenges ( everolimus or veliparib with temozolomide )  . 
patients randomly assigned to the nontargeted control arm had a higher pretreatment dropout rate than the experimental arm , suggesting a preference for targeted therapy based on prestudy genetic proling . relevance the prevalence of genetic data makes it challenging to randomly assign patients to a nontargeted control arbetter geneand variant - specic biomarkers that predict response to drugs are needed for patients with cancer . patients were required to have measurable disease , be willing to undergo tumor biopsy to establish presence of a study - dened actionable mutation of interest ( amoi ) , and have tumor amenable to interventional radiologyguided percutaneous biopsy with a 16to 18 - gauge neeindicated and dle ; excisional biopsy was allowed if evaluable . 
patients who had prior treatment with any of the investigational agents were eligible to participate but were not assigned that same agent . agent - specic eligibility criteria are included in the data supplement . this trial was conducted under a national cancer institute ( nci ) - sponsored investigational new drug application with institutional review board approval . 
protocol design and conduct followed all applicable regulations , guidances , and local policies ( clinicaltrials.gov identier : nct01827384 )  . the investigators obtained informed consent from each participant . trial design this was a multihistology , multicenter , randomized phase ii study of four investigational drug regimens demonstrated to inhibit the dna repair pathway , ras / raf / mek pathway , or akt / pi3k / mtor pathway . 
eligible patients with an amoi detected were randomly assigned 2 : 1 to receive the recommended phase ii dose of either ( 1 ) a predened targeted regimen based on mutation status ( experimental arm ) or ( 2 ) a regimen , chosen from the four study regimens , that did not target their amois ( control arm )  . 
the specic study amois ( data supplement ) were selected on the basis of published functional evidence or implications for protein translation and pathway function ; they were detected in patient samples via a clinical laboratory improvement amendments ( clia ) sequencing assay developed and validated by the molecular characterization laboratory at the frederick national laboratory for cancer research , as previously described.5 patient eligibility determination and randomized treatment assignment were performed with the genemed informatics system as described.6 if more than one amoi was detected for a patient randomly assigned to the experimental arm , the targeted treatment was based on the selection of higher allele frequency ; if allele frequencies were within 15% , the patient was assigned to the targeted treatment cohort with the fewest patients enrolled ( with the option to receive the other treatment regimen upon disease progression )  . 
if a patient randomly assigned to the control arm had multiple nontargeted treatment options , their regimen was chosen based on the proportions of treatment assignments on the experimental arm , so as to balance the two arms with respect to proportions receiving each of the four regimens . for the purpose of assessing the primary end point of this trial , only response to the rst regimen was used . 
adverse events ( aes ) were graded according to nci common toxicity criteria version 4.0 until march 31 , 2018 , when version 5.0 was implemented ; all aes were mapped to version 5.0 before the nal analysis . 
 random assignment and clinical outcome on the nci - mpact trial study agents veliparib ( abt - 888 ; nsc 737664 ) , adavosertib ( azd1775 ; nsc 751084 ) , trametinib ( nsc 763093 ) , and everolimus ( nsc 733504 ) were supplied by the division of cancer treatment and diagnosis , nci , under collaborative research and development agreements with abbvie ( north chicago , il ) , astrazeneca ( cambridge , united kingdom ) , glaxosmithkline ( brentford , united kingdom ) , and novartis ( basel , switzerland ) , respectively . 
study drugs were administered at the recommended phase ii doses and schedules ( data supplement )  . statistical study design the accrual ceiling for each regimen cohort of the experimental arm was set at 30 patients to discriminate between tumor response rates of 20% versus 5% . 
the design included n = 198 enrolled n = 5 did not have biopsy n = 193 had biopsy collected n = 13 insufficient tumor or dna n = 1 declined to participate detceted ioma on dah 17 = n detceted ioma na dah 801 = n n = 7 had no targeted regimen n = 5 had no control regimen but were offered treatment n = 64 randomly assigned to targeted arm n = 32 randomly assigned to control arm n = 10 assigned everolimus n = 25 assigned trametinib n = 3 assigned veliparib plus tmz n = 10 assigned everolimus n = 10 assigned trametinib n = 2 assigned veliparib plus tmz n = 26 assigned adavosertib plus carboplatin n = 10 assigned adavosertib plus carboplatin n = 7 clinically excluded n = 4 died n = 4 declined to participate n = 7 clinically excluded n = 1 died n = 7 declined to participate n = 6 received adavosertib plus carboplatin n = 8 received everolimus n = 20 received trametinib n = 3 received veliparib plus tmz n = 3 received everolimus n = 6 received trametinib n = 2 received veliparib plus tmz n = 8 off treatment : n = 2 death ( pd ) n = 4 pd n = 1 toxicity n = 1 withdrew n = 20 off treatment : n = 19 pd n = 1 withdrew n = 3 off treatment : n = 3 pd n = 3 off treatment : n = 3 pd n = 6 off treatment : n = 5 pd n = 1 withdrew n = 2 off treatment : n = 1 pd n = 1 withdrew n = 6 off treatment : n = 5 pd n = 1 toxicity n = 18 received adavosertib plus carboplatin n = 18 off treatment : n = 13 pd n = 1 intercurrent illness n = 3 toxicity n = 1 withdrew fig 1 . 
seven patients had an amoi but could not be randomly assigned because they were ineligible for the targeted treatment ( six patients : pancreatic cancer with an ras mutation ; one patient : unknown reason )  . 
 chen et al an interim futility analysis ; if no objective responses were observed among the initial 12 patients in each experimental cohort , the cohort was to be terminated early ( with 54% likelihood under the null hypothesis ) , with 93% condence that the response rate would be lower than the target 20% rate . 
this design yields at least 84% power to detect a true objective response rate of at least 20% and at least 0.94 probability of a negative result if the true objective response rate was no more than 5% . 
four - month progression - free survival ( pfs ) , dened as the time from random assignment to progression or death from any cause ( whichever comes rst ) , was evaluated as a secondary end point using kaplan - meier estimates and cis calculated using greenwoods formula . 
twelve or more instances of 4 - month pfs ( at least 40% ) among the 30 patients in an experimental cohort was to be considered promising ; this would occur with 90% likelihood if the true 4 - month pfs rate is 50% ( median pfs of 4 months ) and with 5% likelihood if the true 4 - month pfs rate is 25% ( median pfs of 2 months )  . results enrollment and treatment assignment one hundred ninety - eight patients who met study eligibility criteria were enrolled from january 2014 to april 2018 ( fig 1 , table 1 , data supplement ) , 108 ( 55% ) of whom underwent a tumor biopsy procedure and ultimately had a study - actionable mutation detected ( fig 2a )  . 
patient characteristics characteristic patients enrolled median age , years ( range ) sex ( female / male ) median number of prior lines of therapy ( range ) a patients with karnofsky performance status ( % ) dna repair pi3k ras / raf / mek patients with an amoi in a targeted pathwayb number 60 ( 23 - 83 ) 109 / 89 4 ( 1 - 12 ) abbreviations : amoi , actionable mutation of interest . areported for patients who received at least one dose of study agent on nci - mpact . breported for all patients with an amoi detected on nci - mpact . 
patients with an amoi in more than one pathway are counted here for each affected pathway . 136 2021 by american society of clinical oncology the genes with highest frequency of study amois were tp53 and kras ( 56% and 46% of patients with an amoi , respectively ) ( fig 2c , data supplement )  . 
all patients assigned to the two dna repair pathway cohorts of the experimental arm had a tp53 mutation and 75% of patients assigned to the trametinib experimental cohort had a kras mutation . 
the majority of amois were nonsynonymous single - nucleotide variants ( data supplement )  . toxicity thirty ( 45% ) of the 66 patients who received at least one dose of study agent ( s ) experienced an ae of grade 3 or greater that was considered at least possibly related to study treatment ( data supplement )  . 
seven patients died within 30 days of their last dose of study drugs but none of the on - study deaths were considered related or likely related to the study treatments . treatment compliance interim analysis revealed unanticipated differences in compliance for patients who were assigned to targeted versus nontargeted therapy ( fig 3a )  . 
the overall percentage of patients assigned to the control arm who never initiated treatment was 47% ( 15 / 32 ) , signicantly higher than the rate for patients assigned to the experimental arm ( 23% ; 15 / 64 ; p = .034 , two - sided , by fishers exact test )  . 
evaluation of the reasons why patients came off study , as documented in the clinical database , reveals that a signicantly higher percentage of the patients randomly assigned to the control arm chose not to start treatment ( 22% [ 7 / 32 ] ) compared with the percentage of patients in the experimental arm who chose not to start treatment ( 6% [ 4 / 64 ] ; p = .038 , two - sided , by fishers exact test )  . interim futility analysis accrual to the veliparib plus tmz and everolimus cohorts was slow such that accrual did not reach the 12 - patient threshold for interim analysis of the primary end point , objective response rate ; no responses were measured on either regimen ( fig 3b )  . 
slow accrual to the veliparib plus tmz arm was because of the fact that every dna repair pathway amoi detected on study was within tp53 ; on the basis of preclinical evidence that loss - of - function mutations in tp53 affect regulation of cell cycle progression , patients who were randomly assigned to the experimental arm with these mutations were assigned adavosertib plus carboplatin as their rst - line study treatment if eligible , not veliparib plus tmz . 
pfs events were experienced by 12 / 17 randomly assigned and treated patients in the control arm ; among the patients randomly assigned to the experimental cohorts , pfs events were documented in 6 of 8 treated with everolimus , 20 of 20 treated with trametinib , 13 of 18 treated with adavosertib plus carboplatin , and 3 of 3 treated with veliparib plus tmz . 
caution must be used in comparing the individual experimental cohorts to the control arm as the restriction of an experimental cohort to a particular target may be prognostic of better ( or worse ) pfs . 
 ( a ) nci - mpact treatment compliance rates : the percent of randomly assigned patients who initiated their assigned study treatment or did not start treatment because of death , clinical exclusion that developed after enrollment , or patient choice . 
 ( b ) the proportions of randomly assigned and treated patients who experienced objective response ( complete response or conrmed partial response ) are presented by arm or targeted treatment cohort . 
none of the three patients in the experimental veliparib plus tmz cohort were progressionfree at 4 months ( ci not provided because of small sample size )  . two patients experienced sustained stable disease ( sd ) for a noteworthy 24 cycles of targeted treatment ( fig 5 )  . one patient with endometrial cancer and pik3ca h1047l and pten r130 * amois received everolimus and experienced sd for 24 cycles before progressing . 
the other patient , a 52 - year - old woman with low - grade ovarian cancer with an nras q61r amoi , experienced sd for 27 cycles of trametinib treatment before her disease progressed . 
in the experimental adavosertib plus carboplatin cohort , one patient with endometrial carcinoma and tp53 r213 * and pik3ca c420r amois had an unconrmed pr before coming off treatment because of toxicity . 
none of the patients who crossed over at disease progression from the control arm to a targeted treatment or from one targeted treatment to another experienced clinical benet on the crossover regimen ( data supplement )  . discussion highly effective , tailored therapy targeting specic genetic aberrations is a primary goal of precision medicine.1 , 2 reports of exceptional responders , retrospective studies , and several nonrandomized trials indicate clinical benet for genome - driven treatments , prompting optimism and discussion about the appropriate evidence framework for precision oncology.3 , 8 - 24 the results of our study , which was important considerdesigned in 2012 , highlight several ations for randomized precision oncology studies in the advanced disease setting that have evolved since then.25 - 28 with the greater prevalence of genetic tests and emphasis on precision medicine , it may be very challenging to randomly assign patients to a nontargeted control arour data suggest that some patients and physicians may have had prior tumor mutation prole knowledge and , when randomly assigned to the control arm , appeared to show a bias favoring the presumed precision medicine approach , declining to participate in the study . 
the low dropout rate on the similarly designed shiva trial may be explained by having the patients randomly assigned to a physicians choice control arm ; results from the shiva trial also did not demonstrate the superiority of molecularly targeted agents over the control treatment.25 the results of the winther and coppo trials , two nonrandomized studies , describe clinical benet for a small number of patients with personalized treatment but the pfs - based end point was not met in either study.29 , 30 our results are similar in that the two statistically evaluable experimental cohorts indicate that neither trametinib nor adavosertib plus carboplatin was more effective than standard therapy at achieving objective response when assigned to target nci - mpact - dened amois in ras / raf / mek or dna repair pathways ( eg , kras gain of function or tp53 loss of function mutations , respectively )  . 
 random assignment and clinical outcome on the nci - mpact trial experimental arm control arm 120 - day rate median 120 - day rate median 100 150 200 250 300 350 100 150 200 250 300 350 days since random assignment days since random assignment number at risk number at risk everolimus experimental cohort trametinib experimental cohort 120 - day rate median 120 - day rate median 100 150 200 250 300 350 days since random assignment number at risk 100 150 200 250 300 350 days since random assignmentt number at risk ( b ) control arm , fig 4 . 
 chen et al x age at dx prior disease category cycles best response werdhtiw yticixot withdrew toxicity illness toxicity werdhtiw female genitourinary genitourinary lower gi breast lower gi female genitourinary gender female male female male female female female male female female male male female female female female male female male male female female male male female female female female female male female male male female female female female female male male male female female male female female female male male male female male female male male male male female female female female elamef genitourinary head and neck genitourinary sarcoma genitourinary lower gi lower gi lower gi lung upper gi genitourinary neuroendocrine lower gi genitourinary lower gi lower gi lower gi lower gi lower gi breast sarcoma lower gi genitourinary gi upper head and neck breast lower gi melanoma lower gi breast sarcoma lower gi lower gi genitourinary genitourinary lower gi lung lower gi lower gi lower gi lower gi lower gi breast lower gi lower gi lung lower gi lower gi lower gi lower gi lower gi lower gi female genitourinary lower gi melanoma melanoma lung genitourinary female genitourinary fig 5 . 
each patients detected nci - mpact amois are listed and color - coded to indicate the level of evidence that the mutation is susceptible to the assigned nci - mpact treatment ( based on the information in the oncokb and civic precision oncology knowledge bases at the time of writing )  . 
where available , the results of whole exome sequencing are presented as the number of genetic alterations detected that are annotated in oncokb as either oncogenic ( # oncogenic mutations ) or as oncogenic and actionable with available therapeutic agents ( # oncokb mutations )  . 
 random assignment and clinical outcome on the nci - mpact trial medicine approach , the lack of signicant response on the experimental arm argues for need of better therapies and further validation . 
extensive genetic sequencing and clinical trials evaluating broader aspects of pathway alterations may reveal additional information about actionable sensitivity markers . the targeted treatment assignments in nci - mpact were made based on molecular aberrations that were expected to confer therapeutic sensitivity at the level of a signaling pathway . 
since the trials initiation , the cancer research community has been engaged in an ongoing effort identify geneand variant - specic biomarkers that predict response to drugs.31 - 37 retrospective review of two precision oncology knowledge bases , oncokb and civic , suggests that there is little curated evidence to support many of the amoi - drug associations targeted in the ncimpact trial , which is consistent with the lack of clinical activity . 
for example , tp53 mutations , which were detected in every nci - mpact patient randomly assigned to a targeted dna repair inhibitor cohort , are understood to be oncogenic but have remained largely undruggable.38 the experimental trametinib cohort is the exception in that for each ras / mek / erk pathway amoi that was detected , there is evidence curated in oncokb or civic suggesting effective inhibition by trametinib . 
notably , all three patients who were treated with trametinib to target an nras q61r mutation experienced clinical benet , in line with published clinical evidence of mek inhibitor activity in patients carrying an nras q61 mutation.39 most of the patients treated in the experimental trametinib arm carried an amoi in kras . 
although there is preclinical support for treating kras amois with an mek inhibitor , the results of that approach were modest in this study , perhaps because of reported mechanisms of kras mutant resistance to atpnoncompetitive mek inhibitors.40 - 42 the presence of a therapy - targeted amoi furthermore , in a patient tumor does not indicate whether the amoi is a driver or passenger mutation.43 , 44 in nci - mpact , the most frequently detected amoisthose in tp53 and kraswere detected in all four treatment cohorts and might have contributed to disease progression in cases where treatment was assigned to target an amoi in a different pathway ( eg , akt / pi3k / mtor pathway )  . 
treatment assignment in such cases was made based on the amoi with the highest allele frequency but there is precedent for subclonal molecular alterations driving disease progression.45 - 48 two of the three patients who tolerated everolimus treatment and had amois conned to only the pi3k pathway experienced prolonged sd ( 10 cycles )  . it is important to note that we were able to achieve a successful biopsy collection rate of  . 
90%.49 even with a turnaround time of 10 days for sequencing results , 5 19 biopsied patients ( 10% ) progressed to the point of ineligibility or death before treatment initiation , reecting the advanced disease status of this patient population . 
biopsy sampling could not have identied spatially or temporally isolated tumor subclones that may have been driving tumor growth or conferring resistance in these patients , 43 , 44 , 50 , 51 challenges that can be explored further in preclinical studies as can the presence of putative driver mutations in other signaling pathways . we are completing the analysis of a preclinical study performed in parallel with the nci - mpact trial using xenograft models derived from the tumors of cancer patients to overcome the hurdles inherent to clinical investigations of molecularly targeted treatment response ( manuscript in preparation )  . 
our preliminary data suggest that functional in vivo evidence of activity in molecularly dened models should be the basis on which to evaluate clinical benet of targeted agents in specied patient subgroups . 
chen , md , national cancer institute , 31 center drive , room 3a44 , bethesda , md 20814 ; twitter : @ncitreatment ; e - mail : chenali@ mail.nih.gov. support this project has been funded in whole or in part with federal funds from the national cancer institute , national institutes of health , under contract no . 
mickey williams , richard piekarz , james h . doroshow provision of study materials or patients : shivaani kummar , geraldine osullivan coyne , funda meric - bernstam , stephen leong , chris karlovich collection and assembly of data : alice p . 
konat e , biswajit das , chris karlovich , chih - jian lih , eric polley , richard simon , ming - chung li , richard piekarz , james h . 
mickey williams research funding : illumina patents , royalties , other intellectual property : i was a co - inventor of the dlbcl cell of origin patent recently led by the nih kanwal p . 
trends mol med 23 : 874 - 898 , 2017 tate jg , bamford s , jubb hc , et al : cosmic : the catalogue of somatic mutations in cancer . 
nucleic acids res 47 : d941 - d947 , 2019 lih c - j , sims dj , harrington rd , et al : analytical validation and application of a targeted next - generation sequencing mutation - detection assay for use in treatment assignment in the nci - mpact trial . 
j mol diagn 18 : 51 - 67 , 2016 zhao y , polley ec , li m - c , et al : genemed : an informatics hub for the coordination of next - generation sequencing studies that support precision oncology clinical trials . 
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blood 100 : 1965 - 1971 , 2002 sawyers cl , hochhaus a , feldman e , et al : imatinib induces hematologic and cytogenetic responses in patients with chronic myelogenous leukemia in myeloid blast crisis : results of a phase ii study . 
obrien sg , guilhot f , larson ra , et al : imatinib compared with interferon and low - dose cytarabine for newly diagnosed chronic - phase chronic myeloid leukemia . 
fukuoka m , wu yl , thongprasert s , et al : biomarker analyses and nal overall survival results from a phase iii , randomized , open - label , rst - line study of getinib versus carboplatin / paclitaxel in clinically selected patients with advanced non - small - cell lung cancer in asia ( ipass )  . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutationpositive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
hauschild a , grob jj , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . lancet 380 : 358 - 365 , 2012 16 . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
massard c , michiels s , ferte c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . cancer discov 7 : 586 - 595 , 2017 19 . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecular proles : results from mypathway , an open - label , phase iia multiple basket study . 
freidlin b , allegra cj , korn el : moving molecular proling to routine clinical practice : a way forward ? j natl cancer inst 112 : 773 - 778 , 2019 25 . 
le tourneau c , delord j - p , gonalves a , et al : molecularly targeted therapy based on tumour molecular proling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
herbst rs , gandara dr , hirsch fr , et al : lung master protocol ( lung - map ) - a biomarker - driven protocol for accelerating development of therapies for squamous cell lung cancer : swog s1400 . 
goncalves a , bachelot t , lusque a , et al : high - throughput genome analysis and therapeutic decision for patients with her2 - negative metastatic breast cancer : first feasibility and molecular results of the randomized phase ii study safir02 breast ( ucbg - 0105 / 1304 )  . 
tuxen iv , rohrberg ks , oestrup o , et al : copenhagen prospective personalized oncology ( coppo ) clinical utility of using molecular proling to select patients to phase i trials . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
dummer r , schadendorf d , ascierto pa , et al : binimetinib versus dacarbazine in patients with advanced nras - mutant melanoma ( nemo ) : a multicentre , open - label , randomised , phase 3 trial . 
ferry - galow kv , datta v , makhlouf hr , et al : what can be done to improve research biopsy quality in oncology clinical trials ? j oncol pract 14 : e722 - e728 , 2018 50 . 
 c deep response to anti - pd - 1 therapy of metastatic neurobromatosis type 1 - associated malignant peripheral nerve sheath tumor with cd274 / pd - l1 amplication berna c . 
ozdemir , md , phd1 , 2 ; pierre bohanes , md3 ; bettina bisig , md , phd1 ; edoardo missiaglia , phd1 ; petros tsantoulis , md , phd4 ; george coukos , md , phd1 , 5 , 6 ; michael montemurro , md1 ; krisztian homicsko , md , phd1 , 5 , 6 ; and olivier michielin , md , phd1 , 5 , 6 introduction malignant peripheral nerve sheath tumors ( mpnsts ) , also known as neurobrosarcomas , are a rare type of highly aggressive soft tissue sarcomas originating from peripheral nerve branches or sheaths . 
more than 50% of these tumors are found in individuals with neurobromatosis type 1 , evolve from benign neurobromas , and are associated with worse outcome than are sporadic tumors.1 patients with metastatic mpnst have a 3 - year survival of only 14%.2 surgery in combination with adjuvant chemotherapy and radiotherapy is the current standard of care.3 although complete resection is potentially curative , local or distant relapse frequently occurs.4 mpnsts are resistant to chemotherapy through different mechanisms , including the upregulation of drug efux transporters.5 radiotherapy can improve local control but does not increase patient survival.3 overall , treatment options are limited for recurrent or metastatic disease . molecular proling of mpnsts identied frequent mutations in the mapk pathway ( nf1 , rassf9 ) ; loss tumor suppressor genes , such as tp53 and cdkn2a ; and alterations in core components of the polycomb repressive complex 2 ( prc2 ) : eed and suz12.6 , 7 still , with some notable exceptions , targeted therapies are generally not successful in the treatment of mpnst.8 , 9 typically , mpnsts present with low programmed death ligand - 1 ( pd - l1 ) expression9 but with relatively high numbers of inltrating cytotoxic t cells and low abundance of immunosuppressive regulatory t cells.10 this immune phenotype would be suggestive of possible benet from immune checkpoint inhibition . 
after multidisciplinary evaluation , a second revision surgery with re - excision of the stump of the left peroneal nerve was realized by the end of october 2015 and showed negative surgical margins . in march 2016 , 5 months after the re - excision , computed tomography ( ct ) showed multiple pulmonary metastases , and a positron emission tomography - ct scan conrmed the absence of extrapulmonary disease . 
after three cycles of doxorubicin chemotherapy ( 75 mg / m2 ) , a partial response was achieved with signicant decrease of the voluminous paramediastinal pulmonary metastasis and stability of the other pulmonary nodules , per response evaluation criteria in solid tumors ( recist ) 1.1. 
we performed a comprehensive molecular analysis of a pulmonary metastasis specimen ( estimated to contain 50% tumor cells ; fig 1a ) and matched constitutional dna , using an inhouse , 400 - gene , next - generation sequencing panel . this is a capture - based panel developed at our institution , aimed at detecting clinically actionable somatic genomic alterations in 394 common cancer - associated genes ( data supplement )  . 
tumor mutation burden , dened as the number of nonsynonymous somatic mutations ( excluding splice variants ) divided by the size of the coding sequence covered by the panel , ( ie , 1.48 megabase ) , was 3.4 per megabase , within the range of previous descriptions.6 besides the known germline mutation of the nf1 gene , we observed a second somatic hit represented by the frameshift variant arg1136hisfs * 2 , interpreted as a loss - offunction mutation , as expected in mpnsts developed in the setting of neurobromatosis type 1 . 
among other alterations , a tp53 loss - of - function variant and a cdkn2a deletion were also identied , in line with published genomic data.6 furthermore , we detected an amplication of the including the cd274 / chromosomal region 9p23 - p24 , pd - l1 locus , in the context of a near - triploid genome . cd274 / pd - l1 locus amplication was conrmed by uorescence in situ hybridization analysis ( fig 1b ) and appeared to be associated with pd - l1 protein overexpression in almost 100% of tumor cells ( fig 1c )  . 
we could not detect any ny - eso - 1 expression ( fig 1g )  . on the basis of these ndings , the molecular tumor board recommended anti - pd - 1 therapy . 
therefore , it was decided to deliver treatments concomitantly.12 the patient began treatment with nivolumab 3 mg / kg intravenously every 2 weeks and received radiotherapy to the bilateral anterior pleural metastases at a dose of 39 gy ( 13 sessions at 3 gy ) at the beginning of july 2017 ( fig 2 )  . two months after starting nivolumab , a ct scan demonstrated a decrease in the size of all pleural and pulmonary lesions without any new lesions . 
 ( a ) microscopic examination of a pulmonary metastasis showed a spindle cell proliferation with marked pleomorphism , consistent with a high - grade mpnst ( hematoxylin - and - eosin stain ; original magnication , 200 )  . 
this was a laboratory - developed break - apart fish probe exploring rearrangements and copy number gains of cd274 / pd - l1 locus at 9p24.1 ; an average of nine red - green fusion signals per nucleus were observed , representing nonrearranged cd274 / pd - l1 loci . 
in contrast , a mean of only three blue signals per nucleus were present , corresponding to a centromeric control probe on chromosome 9 ( original magnication , 630 )  . 
 ( c ) by immunohistochemistry , almost 100% of tumor cells strongly expressed pd - l1 at their cell membrane ( pd - l1 , clone sp263 ; original magnication , 100 ) and ( d ) numerous tumor - inltrating t cells were present ( cd3 , clone 2gv6 ; original magnication , 100 )  . 
 ( e ) the vast majority of these were cd8 positive ( cd8 , clone c8 / 144b ; original magnication , 100 ) , whereas ( f ) foxp3 - expressing regulatory t cells represented less than 10% ( foxp3 , clone 236a / e7 ; original magnication , 100 )  . 
all upstream or downstream nonsense variants are also reported to be pathogenic or likely pathogenic . this variant has not been observed in the general population or in the consulted databases . 53% decrease of the target lesions according to recist 1.1 at 9 months remained stable at 12 and 15 months of nivolumab therapy ( fig 2 ) an increase of a pulmonary micronodule from 5 to 7 mm and the appearance of three small , aspecic micronodules were noted after 12 months of therapy . 
importantly , the radiologic improvement translated into improved general health status , with an increase in appetite and weight , a reduction of fatigue , and a decrease in opioid use for pleural pathe patients general condition improved rapidly , from eastern cooperative oncology group performance status 3 to 1 , 12 months from the start of the immunotherapy . 
a case of complete response to pembrolizumab in combination with procarbazine was reported in a patient with mpnst harboring 90% pd - l1 expression.13 , 14 to our knowledge , this is the rst report of a deep and prolonged response to nivolumab and radiotherapy in mpnst with cd274 / pd - l1 amplication . 
most notably , cd274 / pd - l1 amplication is found in 97% of patients with classic hodgkin lymphoma and is characterized by exceptionally high response rates of 70% to anti - pd - 1 therapy.14 , 15 however , cd274 / pd - l1 amplication has been detected across more than 100 different solid tumor types at varying frequencies , 16 , 17 including in triple - negative breast cancer ( 29% ) , 17 squamous cell carcinomas of the oral cavity ( 19% ) , 18 nonsmall - cell lung cancer ( 5% ) , 19 and colon cancer ( 3% ) .17 in a recent analysis of the cancer genome atlas sarcoma data set , cd274 / pd - l1 copy number gains were detected in 11% of the mpnst samples . 
in agreement with other studies , pd - l1 expression correlated with copy number gains of the corresponding genomic locus.12 cd274 / pd - l1 amplication in hodgkin lymphoma and nonsmall - cell lung cancer has been associated with poor prognosis15 , 20 and predicts response to anti - pd - 1 therapy.21 , 22 as in the patient in this case report , amplication of table 2 . 
13 jak2 , cd274 , ptprd cdkn2a , cdkn2b , fancg all genes in the region all genes in the region hnf1a , ncor2 , pole all genes in the region all genes in the region all genes in the region amplication deletion amplication amplication amplication deletion amplication deletion * only copy number gains of ve or more copies and deletions are reported in this table . 
computed tomography scans show the bilateral pleural metastases in june 2017 , before starting nivolumab therapy or radiotherapy and after 5 , 9 , 12 , and 15 months of nivolumab therapy , respectively . 
the irradiated pleural metastases are indicated by red arrows ; the nonirradiated lesions are indicated by blue arrows . the 9p24 locus typically involves both cd274 / pd - l1 and jak2 , with the 9p24 locus amplication situated 300 kb distally of cd274 / pd - l1 . 
jak2 activation causes increased pd - l1 transcription via the increased signal transducer and activator of transcription ( stat ) protein secretion22 and is associated with response to anti - pd - 1 therapies . 
in line with this , preclinical models have shown that loss of function mutations in the jak / stat pathway are correlated with impaired response to interferon receptor 1 and 2 signaling and could represent a mechanism of resistance to anti - pd - 1 therapies.23 - 25 it is difcult to estimate the contribution of radiotherapy to the exceptional response of the patient in this report . 
radiotherapy might potentiate the effect of immune checkpoint inhibitors through induction of immunogenic cell death with an increase in the number or diversity of tumorassociated antigens and improved inltration of immune cells , and by consequence , could partially overcome the immune suppressive tumor microenvironment , a phenomenon known as the abscopal effect.25 although we cannot exclude the presence of an abscopal effect , we currently have no direct supporting evidence . 
clinical trials testing different sequences and types of immunotherapy in combination with radiotherapy are ongoing and will help determine the extent of the abscopal effect.26 a major issue in immuno - oncology is the lack of predictive biomarkers . 
our report suggests that pd - 1 targeting alone or in combination with radiotherapy could be an effective strategy in mpnsts harboring amplication of cd274 / pd - l1 and could be an option for patients whose disease progresses after standard therapies . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . pierre bohanes honoraria : merck serono , eli lilly , abbvie , sano travel , accommodations , expenses : amgen , boehringer ingelheim , bristol - myers squibb , eli lilly petros tsantoulis honoraria : roche , pzer travel , accommodations , expenses : amgen george coukos consulting or advisory role : roche , astrazeneca , bristol - myers squibb speakers ' bureau : roche research funding : bristol - myers squibb ( inst ) , celgene ( inst ) , boehringer ingelheim ( inst ) , roche ( inst ) , iovance kite pharma ( inst ) , nextcure ( inst ) , geneostx ( inst ) , sano / aventis ( inst ) patents , royalties , other intellectual property : patents in the domain of antibodies and vaccines targeting the tumor vasculature as well as technologies related to t - cell expansion and engineering for t - cell therapy . 
receives royalties from the university of pennsylvania . krisztian homicsko consulting or advisory role : amgen , bristol - myers squibb , roche travel , accommodations , expenses : msd oncology olivier michielin consulting or advisory role : bristol - myers squibb , msd , novartis , roche , amgen research funding : msd , bristol - myers squibb expert testimony : bristol - myers squibb travel , accommodations , expenses : bristol - myers squibb , msd no other potential conicts of interest were reported . acknowledgment the patient has provided informed consent for the publication of this case report . we thank dr abderrahim zouhair , clinique de la source , lausanne , for providing the images of the irradiation elds . 
we also thank the fasma and philanthropia foundations that are supporting the romand network of oncology and our institutional molecular tumor board . references kolberg m , hland m , agesen th , et al : survival meta - analyses for .1800 malignant peripheral nerve sheath tumor patients with and without neurobromatosis type 1 . 
j neurosurg 126 : 319 - 329 , 2017 kahn j , gillespie a , tsokos m , et al : radiation therapy in management of sporadic and neurobromatosis type 1 - associated malignant peripheral nerve sheath tumors . 
front oncol 4 : 324 , 2014 zehou o , fabre e , zelek l , et al : chemotherapy for the treatment of malignant peripheral nerve sheath tumors in neurobromatosis 1 : a 10 - year institutional review . 
orphanet j rare dis 8 : 127 , 2013 peacock j.d. , cherba d , kampfschulte k , et al : molecular - guided therapy predictions reveal drug resistance phenotypes and treatment alternatives in malignant peripheral nerve sheath tumors . 
j transl med 11 : 213 , 2013 brohl a.s. , kahen e , yoder sj , et al : the genomic landscape of malignant peripheral nerve sheath tumors : diverse drivers of ras pathway activation . 
sci rep 7 : 14992 , 2017 lee w , teckie s , wiesner t , et al : prc2 is recurrently inactivated through eed or suz12 loss in malignant peripheral nerve sheath tumors . 
curr treat options oncol 16 : 328 , 2015 shurell e , singh as , crompton jg , et al : characterizing the immune microenvironment of malignant peripheral nerve sheath tumor by pd - l1 expression and presence of cd8 + tumor inltrating lymphocytes . 
budczies j , mechtersheimer g , denkert c , et al : pd - l1 ( cd274 ) copy number gain , expression , and immune cell inltration as candidate predictors for response to immune checkpoint inhibitors in soft - tissue sarcoma . 
payandeh , ms , sadeghi , m , sadeghi , e : complete response to pembrolizumab in a patient with malignant peripheral nerve sheath tumor : the rst case 14 . 
armand p , engert a , younes a , et al : nivolumab for relapsed / refractory classic hodgkin lymphoma after failure of autologous hematopoietic cell transplantation : extended follow - up of the multicohort single - arm phase ii checkmate 205 trial . 
straub m , drecoll e , pfarr n , et al : cd274 / pd - l1 gene amplication and pd - l1 protein expression are common events in squamous cell carcinoma of the oral oncol 4 : 1237 - 1244 , 2018 cancer . 
n engl j med 372 : 311 - 319 , 2015 ikeda s , goodman am , cohen pr , et al : metastatic basal cell carcinoma with amplication of pd - l1 : exceptional response to anti - pd1 therapy . 
luo n , formisano l , gonzalez - ericsson pi , et al : melanoma response to anti - pd - l1 immunotherapy requires jak1 signaling , but not jak2 . 
 first report of clinical response to venetoclax in early t - cell precursor acute lymphoblastic leukemia introduction early t - cell precursor acute lymphoblastic leukemia ( etp - all ) is a recently recognized , highrisk subgroup of all characterized by early differentiation arrest and distinct genetic and transcriptional features . 
etp - all represents 10% to 30% of t - cell all ( t - all ) cases in adults and 10% to 15% of cases in children , exhibits inferior response rates to chemotherapy , and is characterized by high relapse rates with dismal outcomes in the relapsed / refractory setting.1 recent insights into the biology of etpall using bh3 profiling have revealed bcl - 2 dependence2 with exquisite in vitro sensitivity to the bcl - 2selective antagonist venetoclax.3 herein , we report a patient with refractory etp - all and another with t - all and some features suggestive of the etp subtype who had excellent responses to venetoclax given in combination with cytotoxic chemotherapy . 
both patients received venetoclax off - label and provided written informed consent after receiving counseling about the unapproved nature of this treatment , the rationale for its use , and possible adverse effects from the medication . patient 1 a 71 - year - old woman was diagnosed with etpall in april 2017 with 80% bone marrow blasts . 
she received two cycles of hyperfractionated cyclophosphamide , vincristine , doxorubicin and dexamethasone ( hyper - cvad ) alternating with high - dose methotrexate and cytarabine and was refractory to treatment . 
 negative markers included cd1a , cd2 , surface cd3 , cd8 , cd14 , cd15 , cd19 , cd22 , cd25 , cd36 , cd41 , myeloperoxidase , and terminal deoxynucleotidyl transferase ( tdt )  . 
 a third cycle of mini - cvd was then administered , but venetoclax was held on day 31 of cycle yazan numan mansour alfayez abhishek maiti yesid alvarado elias j . 
at the time of writing , she remains in morphologic remission with progressively declining levels of mrd in the bone marrow ( 0.02% on cycle 3 day 44 ; 0.01% on cycle 3 day 78 )  . 
filgrastim was initiated on cycle 3 day 84 enabling resumption of venetoclax ( without chemotherapy ) on cycle 3 day 93 . patient 2 a 75 - year - old man was referred to our center with an outside diagnosis of refractory secondary acute myeloid leukemia ( aml )  . 
the patient had initially been diagnosed with myelodysplastic syndrome ( mds ) in june 2016 and treated with azacitidine for six cycles before it was discontinued , reportedly because of pancytopenia . 
initial bone marrow examination at our center in october 2017 showed 85% blasts with a phenotype consistent with t - all ( positive for cytoplasmic cd3 , cd5 , cd7 , cd10 ( partial ) , cd13 , cd34 , cd38 ( dim ) , cd56 ( dim ) , cd117 ( dim ) , and hla - dr and negative for cd1a , cd2 , surface cd3 , cd4 , cd8 , cd14 , cd15 , cd19 , cd22 , cd25 , cd33 , cd36 , cd41 , cd64 , cd123 , myeloperoxidase , and tdt )  . 
the blasts lacked cd1a and cd8 expression , while co expressing the myeloid markers cd13 , cd117 ( dim ) , and cd34 , consistent with etp - all ; however , cd5 expression was strong , which argued against etp - all . 
we reviewed his previous bone marrow slides performed at the outside facility ( august 2017 ) , which showed an acute leukemia ( 70% blasts ) without good evidence for a myeloid immunophenotype and dysplastic granulocytes . 
 flow cytometry performed at the outside facility had shown expression of cd5 ( moderate ) , cd7 ( bright ) , cd10 ( partial ) , cd11b ( partial ) , cd13 ( variable ) , cd33 ( variable ) , cd34 ( moderate ) , cd38 ( moderate ) , cd45 ( dim ) , cd56 ( partial ) , cd117 ( variable ) , cd123 ( partial ) , and hla - dr ( partial ) , and karyotyping had revealed monosomy 7 , trisomy 1 , and der ( 1 ; 22 ) ( q10 ; q10 )  . 
the reported immunophenotype of the blasts ( 7% ) was positive for cd34 , cd117 , hla - dr , cd13 , cd33 ( partial ) , cd38 , cd7 , myeloperoxidase , and cytoplasmic cd3 ( subset ) , and negative for cd2 , cd3 , cd4 , cd10 , cd11b , cd14 , cd15 , cd16 , cd19 , cd56 , cd64 , cd123 , and tdt . 
routinely stained sections of bone marrow core biopsy specimens obtained from patients with ( a ) t - cell acute lymphoblastic leukemia and ( c ) early t - cell precursor acute lymphoblastic leukemia demonstrate sheets of medium - sized blasts . 
immunohistochemical studies performed with anti - bcl - 2 antibody ( clone 100 / d5 , leica / novocastra , buffalo grove , il ) on formalin fixed , paraffin - embedded tissue of bone marrow core biopsy specimen of ( b ) the patient with t - cell acute lymphoblastic leukemia demonstrate that blasts show variable bcl - 2 expression . 
mutational analysis disclosed the known srsf2 mutation and tet2 variants , and a new mpl variant of uncertain orig the response , however , was transient , with a repeat bone marrow examination 4 weeks later showing persistent t - all with 10% blasts , background mds , and del ( 20q ) on karyotyping . 
the patient then received a third cycle of mini - cvd with venetoclax , and a follow - up bone marrow examination 4 weeks later was markedly hypocellular with no morphologic evidence of acute leukemia , but flow cytometry showed persistent mrd ( t - all ) at 1.2%. 
unfortunately , approximately 3 weeks afterward , he was found to have relapsed with 62% bone marrow blasts ; flow cytometry revealed 18.8% aberrant t lymphoblasts with no appreciable change in immunophenotype , whereas karyotyping and fluorescent in situ hybridization again showed del ( 20q ) and monosomy 7 . 
serial ngs was not performed . clonal selection and survival advantage mediated by antiapoptotic bcl - 2 family proteins have a central role in lymphoblast biology.5 , 6 abt - 263 ( navitoclax ) , the clinical equivalent of the prototypical bh3 - mimetic abt - 737 , 7 targeted both bcl - xl and bcl - 2 ; however , severe thrombocytopenia as a result of bcl - xl inhibition in megakaryocytes limited its application in the clinic.8 - 10 venetoclax ( formerly abt - 199 ) is a bcl - 2selective bh3 - mimetic that spares platelets while inducing apoptosis of tumor cells.6 by using bh3 profiling in patient - derived tumor xenograft models , chonghaile et al3 demonstrated that t - all cells are , in general , dependent on bcl - xl for survival . 
other investigators have reported similar findings and shown synergism between venetoclax and cytotoxic chemotherapy against t - all cell lines and primary samples.11 , 12 to our knowledge , we report the first clinical response of etp - all ( case 1 ) , which has been durable thus far , to venetoclax administered in combination with low - intensity chemotherapy . 
trajectory of circulating leukocyte count ( 103 / l ) and blast percentage from start of treatment for patient 1 with corresponding serum phosphate ( mg / dl ) and plasma uric acid levels ( mg / dl ) , and absolute blast count ( 103 / l )  . 
 this is in line with the preclinical data showing particular susceptibility of the etp subtype to bcl - 2 inhibition , with greater dependence on bcl - xl exhibited by other , more mature subtypes of t - all . 
given these preclinical data and such anecdotal clinical responses , as well as preclinical evidence of efficacy of venetoclax against mixed lineage leukemiarearranged b - cell all ( b - all ) , 13 a phase ib clinical trial ( clinicaltrials.gov identifier : nct03319901 ) testing the combination of venetoclax and minicvd in previously untreated adults with all ( both band t - all , including etp - all ) has been initiated at dana - farber cancer institute and md anderson cancer center . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . yazan numan no relationship to disclose mansour alfayez no relationship to disclose abhishek maiti research funding : celgene ( inst ) yesid alvarado no relationship to disclose elias j . 
jain n , lamb av , obrien s , et al : early t - cell precursor acute lymphoblastic leukemia / lymphoma ( etp - all / lbl ) in adolescents and adults : a high - risk subtype . 
chonghaile tn , roderick je , glenfield c , et al : maturation stage of t - cell acute lymphoblastic leukemia determines bcl - 2 versus bcl - xl dependence and sensitivity to abt - 199 . 
kantarjian h , ravandi f , short nj , et al : inotuzumab ozogamicin in combination with lowintensity chemotherapy for older patients with philadelphia chromosome - negative acute lymphoblastic leukaemia : a single - arm , phase 2 study . 
souers aj , leverson jd , boghaert er , et al : abt - 199 , a potent and selective bcl - 2 inhibitor , achieves antitumor activity while sparing platelets . 
roberts aw , advani rh , kahl bs , et al : phase 1 study of the safety , pharmacokinetics , and antitumour activity of the bcl2 inhibitor navitoclax in combination with rituximab in patients with relapsed or refractory cd20 + lymphoid malignancies . 
roberts aw , seymour jf , brown jr , et al : substantial susceptibility of chronic lymphocytic leukemia to bcl2 inhibition : results of a phase i study of navitoclax in patients with relapsed or refractory disease . 
wilson wh , oconnor oa , czuczman ms , et al : navitoclax , a targeted high - affinity inhibitor of bcl - 2 , in lymphoid malignancies : a phase 1 dose - escalation study of safety , pharmacokinetics , pharmacodynamics , and antitumour activity . 
anderson nm , harrold i , mansour mr , et al : bcl2 - specific inhibitor abt - 199 synergizes strongly with cytarabine against the early immature loucy cell line but not more - differentiated t - all cell lines . 
peirs s , matthijssens f , goossens s , et al : abt - 199 mediated inhibition of bcl - 2 as a novel therapeutic strategy in t - cell acute lymphoblastic leukemia . 
 economic impact of next - generation sequencing versus single - gene testing to detect genomic alterations in metastatic nonsmall - cell lung cancer using a decision analytic model nathan a . 
pennell , md , phd1 ; alex mutebi , phd2 ; zheng - yi zhou , phd3 ; marie louise ricculli , msc3 ; wenxi tang , ms3 ; helen wang3 ; annie guerin , msc4 ; tom arnhart , pharmd , ms2 ; anand dalal , phd2 ; medha sasane , phd2 ; kevin y . 
model outcomes for each strategy were time - to - test results , the proportion of patients identied harboring alterations with or without us food and drug administrationapproved therapies , and total testing costs . 
a budget impact analysis assessed the economic effects of increasing the proportion of ngs - tested patients . results in a hypothetical 1 , 000 , 000 - member health plan , 2 , 066 medicare - insured patients and 156 commercially insured patients were estimated to have mnsclc and to be eligible for testing . 
2019 by american society of clinical oncology lung cancer ( nsclc ) , introduction nonsmall - cell the most common type of lung cancer , 1 can be classied on the basis of the presence of genomic alterations in driver oncogenes , 2 , 3 such as egfr , alk , ros1 , kras , braf , met , her2 , ret , and ntrk1.2 - 4 in the united states , several theratarget egfr , alk , ros1 , and braf pies that v600e alterations5 - 7 have been approved by the us food and drug administration ( fda ) therapy for patients with metaacross lines of static nsclc ( mnsclc )  . 
other targeted therapies are in clinical including those trial phase , against met , her2 , ntrk1 , and ret alterations identier : nct01639508 ; ( clinicaltrials.gov nct02414139 ; nct02716116 ; nct01336634 ; nct02097810 )  . improve treatment targeted therapies have been demonstrated to signicantly response and progression - free survival7 - 9 ; therefore , it is important to identify patients with specic genomic alterations to individualize treatment and optimize outcomes.2 , 9 currently , a number of testing strategies are available with which to identify genomic alterations in nsclc . 
 pennell et al context key objective to determine the least costly strategy for testing for all recommended molecular abnormalities in patients with nonsmall - cell lung cancer ( nsclc ) at diagnosis . knowledge generated upfront next - generation sequencing ( ngs ) testing for all relevant molecular targets in nsclc is less costly than performing single - gene testing , no matter what testing strategy is used . 
upfront ngs testing also results in the largest number of patients with targetable genetic alterations being identied in the shortest period of time . relevance as more clinically relevant genetic targets in nsclc emerge that require routine testing at diagnosis , it is vital to identify the molecular testing strategy that is timeliest , spares the most tissue , and is most cost efcient , as this must be done in every new patient . 
our model illustrates that moving from sequential single - gene tests or even panels of tests to broader ngs testing for patients with advanced nsclc is already the best strategy in these three areas and will only become more relevant as the list of tests grows . 
stakeholders should consider moving to ngs as the preferred method for biomarker testing . single - gene tests for less common alterations.10 sequences of single - gene tests can also be used without hotspot panel , typically testing for the most common alterations rst and less common alterations last.10 in either case , running a sequence of single - gene tests can be time consuming and may require a relatively large tissue sample , which is not always available as nsclc is often detected at an advanced stage and only small biopsy samples are usually attainable.11 - 13 as a result , one or more rebiopsies may be needed to complete the sequence . 
in recent years , next - generation sequencing ( ngs ) has emerged as a reliable strategy to simultaneously test for multiple alterations using a single tissue sample14 ; however , only a small percentage of patients with nsclc currently receive ngs , 15 as a number of practical barriers hinder its wider adoption , including limited patient access , a lack of awareness and communication within medical care teams about the benets of ngs , limited coverage , and low reimbursement rates.16 , 17 in addition , given the relatively recent development of ngs , there is a need to better understand the economic implications of using ngs versus other testing strategies in real - world clinical practice . therefore , a decision analytic model was developed to estimate the difference in testing costs and time - to - test results between ngs and commonly used single - gene testing strategies among patients with mnsclc from the perspective of the centers for medicare & medicaid services ( cms ) and a us commercial payer . 
in addition , the budget impact of increasing ngs testing was assessed from the perspective of both cms and a us commercial payer . methods model overview a decision analytic model was developed in microsoft excel 2016 from the perspective of cms and a us commercial payer for patients with newly diagnosed mnsclc who were eligible for genomic testing to determine mnsclc alteration status and inform treatment selection . 
alterations included in the model involved the programmed cell death protein 1 and its ligand programmed death protein 1 ligand ( pd - l1 ) , as well as genes egfr , alk , ros1 , braf , kras , met , her2 , ret , and ntrk1 . 
four genomic testing strategies were considered . upfront ngs : at mnsclc diagnosis , patients received a panel that tested simultaneously for all alterations with and without fda - approved therapies ( egfr , alk , ros1 , braf , met , her2 , ret , and ntrk1 )  . sequential testing : patients received a sequence of singlegene tests for alterations with fda - approved therapies ( egfr , alk , ros1 , and braf )  . 
negative test results for all four alterations were followed by either a sequence of single - gene tests or ngs to test for alterations without fda - approved therapies ( met , her2 , ret , and ntrk1 )  . 
single - gene tests were assumed to be ordered in sequence , one at a time , after receiving negative results for each previous test . exclusionary testing : patients rst received a test for kras because kras is the most common mutation in lung adenocarcinoma , and as the genetic alterations of interest are mutually exclusive , a positive test would prevent the need for additional testing . 
negative results were followed by either a sequence of single - gene tests or ngs to test for alterations without fda - approved therapies ( met , her2 , ret , and ntrk1 )  . all four testing strategies included pd - l1 and routine immunohistochemistry testing , which were assumed not to time because they were conducted sitake additional multaneously with the rst test in sequential and exclusionary testing and at the same time as the hotspot panel and ngs . 
appropriate therapyeither targeted therapy or nontargeted therapy ( eg , chemotherapy and immunotherapy ) was selected on the basis of the test results , that is , a conrmed alteration with or without fdaapproved therapies or no known alteration . 
patients who received rst - line nontargeted therapy and who tested negative for alterations with fda - approved therapies were assumed to continue testing with ngs or single - gene tests for alterations without fda - approved therapies , provided that enough tissue sample remained . 
a proportion of patients with alterations without fda - approved therapies were assumed to receive a benet from participating in clinical trials of agents under development . model inputs epidemiology and population inputs . 
for cms , the diagnosis of metastatic nsclc ( biopsy performed ) sequential exclusionary hotspot panel positive for tested alteration negative for tested alteration positive for tested alteration negative for tested mutation negative for tested mutation negative for tested mutation positive for tested alteration exclusionary mutation ( kras positive ) appropriate therapy appropriate therapy appropriate therapy appropriate therapy appropriate therapy enough tissue / no need for rebiospy insufficient tissue / need rebiopsy negative for tested mutation positive for tested alteration successful rebiopsy no rebiopsy / failed rebiopsy continue testing until appropriate treatment appropriate treatment appropriate treatment continue testing until appropriate treatment legend : continue testing for next alteration until the decision is made for appropriate treatment . is there sufficient v insufficient tissue and need for rebiopsy to continue testing ? fig 1 . 
sequential testing : sequence of single - gene tests for egfr , alk , ros1 , and braf , followed by either a sequence of single - gene tests or ngs for met , her2 , ret , and ntrk1 . 
hotspot panel : panel testing simultaneously for egfr , alk , ros1 , and braf , followed by either a sequence of single - gene tests or ngs for met , her2 , ret , and ntrk1 . 
epidemiology , population , and testing cost inputs variable commercial payer source patient population in the health care plan , no . 1 , 000 , 000 1 , 000 , 000 assumption adults in the population of interest , % * cms : kaiser family foundation18 ; commercial : us census bureau19 no . 
unit costs for all genomic alteration testing were based on the 2017 clinical lab fee schedule23 for the medicare - insured population and from dalal et al15 for the commercially insured population using two us administrative claims databases ( table 1 )  . 
single - gene tests for kras , egfr , her2 , and braf were assumed to be performed using real - time polymerase chain reaction . pd - l1 tests were assumed to be performed using immunohistochemistry or uorescence in situ hybridization . for each testing strategy , the per - patient cost of sequential , exclusionary , and hotspot panel testing was considered to be the sum of the cost of each individual test for pd - l1 and alterations with or without fdaapproved therapiesegfr , alk , ros1 , braf , met , her2 , ret , ntrk1 , and krasmultiplied by the proportion of patients who received each test , which was determined by the results for the preceding testing and rebiopsy failure rate ( table 2 )  . 
the difference between the plan - total testing costs of a certain strategy and those of ngs was considered as the cost savings associated with ngs versus the strategy in question . 
as a result of insufcient tissue sample , 8% of patients were assumed to require rebiopsy to continue testing.22 of these patients , only 30% were assumed to be actually rebiopsied , with 15% experiencing failure with rebiopsy.28 on the basis of on handorf et al , 28 rebiopsy cost was $415.30 for medicare - insured patients and $1 , 399.80 for commercially insured patients . 
one half of patients who tested negative for alterations with fda - approved therapies and who received nontargeted therapy were assumed to continue testing for alterations without fda - approved therapies . 
of these patients , 75% were assumed to continue testing with ngs and 25% with one of the other testing strategies . model outputs model results for ngs were compared with those for sequential , exclusionary , and hotspot panel testing in terms of differences in the estimated total cost associated with testing , calculated separately for cms and the commercial payer ; time - to - test results that accounted for the time associated with test turnaround and rebiopsy , assumed to be the same for cms and the commercial payer ; and the proportion of patients identied by each testing strategy as harboring alterations with or without fda - approved therapies . budget impact analysis we conducted a budget impact analysis to assess the effects of increasing upfront ngs testing in cms and commercial plans . 
total cost and cost difference versus ngs medicare - insured patients ( n = 2 , 066 ) commercially insured patients ( n = 156 ) testing strategy sequential exclusionary hotspot panel total cost 2 , 190 , 499 3 , 721 , 368 3 , 584 , 177 4 , 331 , 295 note . 
costs are given in 2017 us dollars . abbreviation : ngs , next - generation sequencing . cost difference v ngs total cost cost difference v ngs 1 , 530 , 869 1 , 393 , 678 2 , 140 , 795 620 , 369 747 , 771 624 , 178 871 , 211 127 , 402 3 , 809 250 , 842 the other parameters at their base - case values . 
on the basis of commercial payer for the 156 commercially insured patients , ngs rates , remained the least expensive testing option , with cost savings of $3 , 809 versus exclusionary testing , $127 , 402 versus sequential testing , and $250 , 842 versus hotspot panel testing . time to receive test results the cumulative time to receiving full test results and initiating treatment , incorporating both testing time and time for rebiopsy , is a critical element in molecular testing . 
proportion of patients identied with alterations with or without fda - approved therapies patients identied with alterations with fda - approved therapies ( medicare insured , n = 446 ; commercially insured , n = 34 ) patients identied , % difference v ngs , % difference in no . 
the only exception was ngs versus exclusionary testing for commercial payersranging from $19 , 943 to $27 , 562likely because of the relatively small base - case cost savings results ( $3 , 809 )  . 
results were most sensitive to scenarios in which test unit costs and the proportion of patients tested for alterations without fdaapproved therapies were varied . discussion several testing strategies for the detection of genomic alterations in nsclc exist in clinical practice ; however , scant evidence is available on the comparative economic implications of using these strategies in patients with mnsclc . 
accordingly , an economic model was developed to estimate the time - to - test results ; the proportion of patients identied as harboring alterations with or without fda - approved therapies ; and testing costs associated with upfront ngs , sequential , exclusionary , and hotspot panel testing among patients with mnsclc . model results demonstrate that ngs was associated with the same ( as hotspot panel ) or shorter ( v exclusionary and sequential testing ) time - to - test results and lower testing costs than sequential , exclusionary , and hotspot panel testing . both ngs and hotspot panel testing had the shortest time - totest results ( 2 weeks ) , indicating that these two testing strategies may yield the shortest time to initiation of appropriate therapy among the four strategies considered here . of note , although the unit cost of ngs was higher than that of individual single - gene tests , the overall cost , which included testing and rebiopsy cost , to test for a broad range of alterations was the lowest for ngs . 
although no treatment is yet approved for these alterations , it is important to identify these patients to give them the opportunity to participate in clinical trials of investigational therapies . although prior studies have discussed the cost effectiveness and benets of various testing strategies in patients with nsclc , 31 - 34 the current study is , to our knowledge , the rst to quantify the economic impact of using ngs versus other testing strategies to detect a comprehensive list of alterationsegfr , alk , ros1 , braf , met , her2 , ret , ntrk1 , and krasin patients with mnsclc in the united states . 
from a clinical standpoint , the timely identication of genomic alterations in patients with mnsclc is key to initiating the most appropriate treatment course on the basis of either targeted therapy , if available , or nontargeted therapy . 
as the results of the current study indicate , upfront ngs seems to be the cheapest broad molecular testing strategy for genomic alterations in terms of both time - to - test results and testing costs . 
furthermore , unlike other testing strategies , ngs allows for the simultaneous screening of both common and less common alterations , which is important because less common alterations are less likely to be tested when using sequential testing strategies . 
in a retrospective review of genomic testing patterns in patients with nonsquamous mnsclc , only 63 of 814 patients were reported to have undergone testing for all seven alterations recommended by national comprehensive cancer network for patients with mnsclc , namely egfr , alk , ros1 , braf , met , ret , and her2.17 using ngs may increase the number of patients tested for including both common and less common alterations , those recommended by the national comprehensive cancer network , thereby providing more information to physicians and patients with which to make informed and timely treatment decisions . 
future studies should also assess the clinical implications of our nding that , as a result of longer time - totest results , patients using sequential and / or exclusionary testing are able to initiate targeted therapy nearly 3 weeks later than patients using ngs or hotspot panel testing . 
it is worth noting that , whereas this study suggests that ngs is a more efcient testing strategy than sequential , exclusionary , and hotspot panel testing , several barriers to wider adoption of ngs in clinical practice remain , including limited coverage and reimbursement.17 however , this may change over time given that the lower total testing costs and shorter initiationof ngs , together with a reduced need for rebiopsy , may reduce medical costs substantially and improve outcomes , beneting patients and payers alike . resultsand thus treatment time - to - test this study has some limitations . 
first , as the study is based on a modeling approach using a decision tree and budget impact inputs and assumptionssome of framework , the model which were based on expert opinionmay contain uncertainty or may have limited generalizability . 
last , the model included only testing costs and not therapy costs and benets , the inclusion of which would allow for an estimate of a wider spectrum of costs . in conclusion , for both cms and commercial payers , upfront ngs testing was associated with the same ( as ( v exclusionary and hotspot panel testing ) or shorter sequential testing ) time to the initiation of appropriate treatment , as well as substantial cost savings compared with all other testing strategies in patients with newly diagnosed mnsclc . 
pennell , alex mutebi , zheng - yi zhou , marie louise ricculli , wenxi tang , helen wang , annie guerin , tom arnhart , anand dalal , kevin y . 
pennell , alex mutebi , zheng - yi zhou , marie louise ricculli , wenxi tang , helen wang , annie guerin , tom arnhart , anand dalal , medha sasane , kevin y . 
pennell consulting or advisory role : astrazeneca , eli lilly , regeneron , cota healthcare , merck research funding : genentech ( inst ) , celgene ( inst ) , astrazeneca ( inst ) , pzer ( inst ) , merck ( inst ) , loxo ( inst ) , altor bioscience ( inst ) , spectrum pharmaceuticals ( inst ) , bristol - myers squibb ( inst ) tom arnhart employment : novartis , alexion pharmaceuticals stock and other ownership interests : alexion pharmaceuticals anand dalal employment : novartis stock and other ownership interests : novartis medha sasane employment : sano , novartis ( i ) stock and other ownership interests : sano , novartis ( i ) kevin y . 
wu employment : novartis , astrazeneca stock and other ownership interests : novartis , astrazeneca , gilead sciences , intercept pharmaceuticals , merck , organovo , takeda , seattle genetics , tg therapeutics kenneth w . 
transl respir med 1 : 6 , 2013 kohno t , nakaoku t , tsuta k , et al : beyond alk - ret , ros1 and other oncogene fusions in lung cancer . 
expert rev mol diagn 16 : 737 - 749 , 2016 barlesi f , mazieres j , merlio jp , et al : routine molecular proling of patients with advanced non - small - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
lancet 387 : 1415 - 1426 , 2016 kris mg , johnson be , berry ld , et al : using multiplexed assays of oncogenic drivers in lung cancers to select targeted drugs . 
dalal aa , guerin a , mutebi a , et al : economic analysis of braf gene mutation testing in real world practice using claims data : costs of single gene versus panel tests in patients with lung cancer . 
levy bp , chioda md , herndon d , et al : molecular testing for treatment of metastatic non - small cell lung cancer : how to implement evidence - based recommendations . 
yang p , allen ms , aubry mc , et al : clinical features of 5 , 628 primary lung cancer patients : experience at mayo clinic from 1997 to 2003 . 
reck m , rodrguez - abreu d , robinson ag , et al : pembrolizumab versus chemotherapy for pd - l1 - positive non - small - cell lung cancer . 
chen d , zhang lq , huang jf , et al : braf mutations in patients with non - small cell lung cancer : a systematic review and meta - analysis . 
meng d , yuan m , li x , et al : prognostic value of k - ras mutations in patients with non - small cell lung cancer : a systematic review with meta - analysis . 
handorf ea , mcelligott s , vachani a , et al : cost effectiveness of personalized therapy for rst - line treatment of stage iv and recurrent incurable adenocarcinoma 29 . 
vanderlaan pa , yamaguchi n , folch e , et al : success and failure rates of tumor genotyping techniques in routine pathological samples with non - small - cell lung 5 : 293 - 305 , 2011 22 : 2616 - 2624 , 2011 cancer 18 : 651 - 659 , 2017 snapshot / 2005 prevalence / canques.html 375 : 1823 - 1833 , 2016 2014 cancer 81 : 1 - 10 , 2013 of the lung . 
as noted in a recent article by black et al2 in jco precision oncology , many laboratories , including ours , have included analysis of the upstream promoter region in routine pten analysis as a result of early literature that identified variants in this region in individuals with phts component cancers , with some variants reported to have a possible impact on translation.3 , 4 our laboratory , however , does not currently classify any pten promoter variant as pathogenic or likely pathogenic . 
thus , we also question the clinical utility of including this region in clinical diagnostic testing and offer our laboratorys experience in support of the proposal that analysis of the full pten promoter region may not be beneficial as a component of hereditary cancer panel testing . 
 this study was approved by the western institutional review board , puyallup , washington ( wirb 20162523 )  . to review briefly , black et al2 assessed cancer risks in individuals who underwent multigene hereditary cancer panel testing at their clinical diagnostic laboratory and identified no increased risk for cancer overall or for the major phts component cancers ( breast , colon , endometrial , thyroid , and renal ) in those with pten promoter variants of uncertain significance ( vus ) compared with those with wild - type pten . 
no statistically significant difference was observed in the frequency of pten promoter vus among those with breast , endometrial , thyroid , renal , or colorectal cancer compared with individuals with no personal history of cancer ( table 1 )  . 
within this cohort , individuals with vus in the minimum promoter region did not seem to have increased prevalence of phts component cancers compared with those with promoter vus outside this region ( table 2 )  . 
of note , variants in the minimum promoter region were found at a lower frequency in those with cancers of interest compared with individuals without cancer ; however , the power of these analyses was limited by sample size . as noted by black et al , 2 additional functional and clinical data are needed to better understand the impact of ultra - rare variants . 
the three promoter variants reported by teresi et al4 as leading to decreased promoter activity ( c . - 862g > t , c . - 854c > g , and c . - 765g > a ) by using the current reference sequence were either absent or present in only one of approximately 30 , 000 alleles in the genome aggregation database.6 furthermore , none of these variants were observed in our cancer panel cohort . 
pten promoter variant prevalence comparisons for core pten - associated cancers individuals with cancer individuals without cancer carrier * negative carrier * negative cancer type female breast endometrial thyroid colorectal renal breast and endometrial breast and thyroid or endometrial 37 , 648 1 , 308 3 , 082 breast and / or thyroid and / 44 , 352 note . 
mester manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors immediate family member , inst = my institution . 
zhou x - p , waite ka , pilarski r , et al : germline pten promoter mutations and deletions in cowden / bannayan - riley - ruvalcaba syndrome result in aberrant pten protein and dysregulation of the phosphoinositol - 3 - kinase / akt pathway . 
bekelman , md2 , 4 , 6 , 7 the senseless killings of george floyd , ahmaud arbery , breonna taylor , and countless others have led to a national reckoning on institutional racism . medicine , race has long been used as a heuristic , or mental shortcut , used by clinicians to process information and make decisions within the time and cognitive constraints of our healthcare system.1 however , using race as a heuristic in medical decision making has the potential to accentuate cognitive biases and lead to deviations from rational decision making , even among the most well - intentioned of clinicians.2 furthermore , it is well recognized that race is a social , not a biological , construct ; as a result , the broad race categories used in medicine are heterogeneously dened and may be incongruent with genetic ancestry , particularly among minority patients.3 , 4 because cancer is inherently a disease of genetic aberration , using these race categories to make decisions in oncology may lead to the delivery of ineffective , or even detrimental , patient care . the rapid advancement of precision oncology , the use of molecular and genetic testing to tailor cancer therapies to individual patients , has uniquely positioned the eld of oncology to move beyond racebased medicine . 
since the discovery of the rst targeted therapy , imatinib , in the 1990s , over 80 targeted agents have been approved by the us food and drug administration for the treatment of numerous solid organ and hematologic malignancies.5 , 6 some of these precision oncology applications correlate with patient race . 
for instance , epidermal growth factor receptor ( egfr ) mutations in nonsmall - cell lung cancer are found in over 60% of patients of asian descent and strongly predict sensitivity to egfr tyrosine kinase inhibitors.7 , 8 similarly , several founder mutations in brca1 / 2 have been observed in multiple ethnic groups , including patients with ashkenazi jewish ancestry , and can be used to predict sensitivity to poly ( adp - ribose ) polymerase inhibitors in patients with breast , ovarian , prostate , and pancreatic cancers.9 - 14 fortunately , the tools of precision oncology enable the administration of agents such as egfr and poly ( adpribose ) polymerase inhibitors to be guided by genetic testing rather than race or ancestry . however , differential use of precision oncology has the potential to widen the very racial disparities that the eld seeks to eliminate.15 indeed , multiple studies have demonstrated decreased rates of genetic counseling , germline and somatic genetic testing , targeted therapy administration , genomic database participation , and clinical trial enrollment among minorities compared with white patients.16 - 22 there are many barriers to achieving the promise of precision oncology , including lack of access to and payment for testing , targeted treatment , and counseling . 
additionally , one major challenge is simply a lack of awareness among minority patients and clinicians.23 the rapid advancement of precision oncology has made it difcult for many clinicians to have the time and expertise to select appropriate genetic testing , interpret and apply test results , and educate patients on their implications.24 this challenge may be especially pertinent among minority - serving physicians , who have been shown to be less likely to refer to genetics and order germline testing for diseases such as breast and colorectal cancer.25 the resultant use of race as a heuristic in the setting of these time and cognitive constraints may lead to decisions that are inuenced by implicit bias , unconscious stereotypes , or attitudes toward people that inuence ones actions and behaviors . 
much like the general population , physicians have been found to have implicit bias with a preference for white over black patients and to associate race with their assessments of patient intelligence , risk - taking behavior , and adherence to medical advice.26 - 29 in turn , these perceptions have been linked to poorer communication , biased treatment recommendations , and unequal access to quality healthcare for minority patients.30 , 31 in this paper , we propose three strategies to advance health equity in precision oncology ( table 1 )  . 
ehr - based strategies to advance health equity in precision oncology ehr strategy key features default orders preselected ehr orders that are automatically applied unless a clinician actively modies them behavioral economics principle nudge decision making by taking advantage of individual status quo bias , or the tendency to favor the current state of affairs automated patient dashboards programs that harness the automation and computing power of the ehr to identify candidate patients for a given diagnostic or therapeutic intervention minimize choice overload by searching through a clinicians full patient panel to identify the subset that is eligible for precision oncology care clinician - directed clinical integration of standardized clinical pathways into the ehr for minimize choice overload by simplifying and facilitating use at the point of care complex clinical decision making use of electronic patient portals to send educational materials prime patients to initiate conversations with their clinicians about precision oncology and communicate normative feedback on its uptake among other patients about precision oncology note . 
we propose that behavioral economic principles should be leveraged to promote health equity in precision oncology as well . to steer the ehr offers a scalable , cost - effective approach to harnessing behavioral economic principles to advance health equity in precision oncology . 
defaultspreselected choices that are applied unless an individual actively changes themare powerful tools that take advantage of the status quo bias to nudge decision making while minimizing cognitive effort and preserving choice . 
this approach has been shown to optimize cancer care delivery by increasing high - value medication prescribing and reducing unnecessary daily imaging during palliative radiotherapy.36 , 37 in the precision oncology space , default orders in the ehr can be used to make direct referrals to genetics for patients who meet guideline criteria on the basis of factors such as tumor type and age , clinical characteristics that can be easily identied in the ehr . 
 advancing health equity in precision oncology decision altogether.47 - 49 the ehr is well equipped to solve the problem of choice overload through automated patient dashboards , which can efciently search through all the patients cared for by a given clinician or at a particular practice to identify a more limited pool of individuals who are eligible for a given intervention . 
this approach has been leveraged by multiple clinical trial matching programs to match patient and tumor characteristics from the ehr to study eligibility criteria , thereby enabling oncologists to identify study opportunities for individual patients . 
these programs have been effective in facilitating increased clinical trial participation not only within academic institutions but also at community oncology practices , sites that are more likely to serve minority and underserved populations.50 , 51 similar automated patient dashboards should be leveraged to identify candidate patients for other precision oncology opportunities that remain underutilized by minorities , such as genetics referrals , germline and somatic testing , targeted therapy administration , and genomic database participation . 
because this strategy matches patients to precision oncology care using the automation and computing power of the ehr rather than the heuristics of human decision making , it is likely to be more effective than individual clinicians in advancing health equity . clinical decision support systems decision support also mitigates choice overload by guiding individuals toward more desirable decisions while preserving their freedom of choice . 
in precision oncology , clinical pathways have emerged as a decision support strategy for clinicians to handle the elds ever - expanding scope and complexity.52 however , these pathways are ineffective unless they are seamlessly integrated into routine clinical practice to maximize their usefulness . 
embedding clinical decision support systems into the ehr has been shown to facilitate decision making in other areas of cancer diagnosis , treatment , and supportive care , 53 and it has been associated with decreased racial disparities in the management such as hypertension.39 this approach should also be leveraged to standardize precision oncology care for all patients , regardless of race . of nononcologic conditions perhaps an even more compelling clinician decision aid is a patients own request for a given medical intervention . 
priming , the use of subtle stimuli to activate thoughts and ideas , 54 is a powerful tool that can be directly used by patients to support clinicians in overcoming the use of race as a heuristic . 
first , we recognize that our proposed strategies do not fully combat the lack of access , nancial language barriers , and challenges , health literacy or longstanding history of mistrust in the healthcare system that have also impeded the adoption of precision oncology among minority patients . 
to be successful , ehr - based strategies informed by the principles of behavioral economics must be implemented as part of a broader , multifaceted approach that addresses all these challenges . second , the application of behavioral economics in medicine is still in its nascency , so there is a paucity of data on the impact of choice architecture redesign on subgroups within the population . 
future studies should incorporate the emerging concept of precision nudging to tailor behavioral economics interventions to specic patient populations as a strategy to ensure equal effectiveness for all . finally , the implementation of ehr - based strategies may require initial investment of nancial and human resources that is not feasible at all institutions . 
as implementation efforts get underway , we must monitor for and address any signs of differential uptake so that our proposed strategies do not inadvertently widen existing inequities in care . in conclusion , in this article , we present three ehr - based strategies that leverage the principles of behavioral economics to nudge oncologists away from the use of race as a heuristic in their decision making . 
 lau - min et al 4abramson cancer center , perelman school of medicine , university of pennsylvania , philadelphia , pa 5division of translational medicine and human genetics , department of medicine , perelman school of medicine , university of pennsylvania , philadelphia , pa 6department of radiation oncology , perelman school of medicine , university of pennsylvania , philadelphia , pa 7department of medical ethics and health policy , perelman school of medicine , university of pennsylvania , philadelphia , pa otherwise noted . 
guerra leadership : freenome , guardant health , genentech stock and other ownership interests : crispr therapeutics , beam therapeutics , intellia therapeutics , editas medicine honoraria : lundbeck ( i ) consulting or advisory role : bristol - myers squibb ( i ) speakers bureau : janssen , pzer ( i ) research funding : bristol - myers squibb ( inst ) travel , accommodations , expenses : lundbeck , janssen ( i ) uncompensated relationships : tapestry networks justin e . 
bekelman honoraria : unitedhealthcare , national comprehensive cancer network , cvs health , optum , american journal of managed care research funding : pzer , united health group , north carolina blue cross blue shield , embedded healthcare no other potential conicts of interest were reported . acknowledgment we thank mitesh patel , md , mba , and callie scott , msc , both at the university of pennsylvania , for their helpful comments during the writing of this manuscript . 
new york , farrar , straus and giroux , 2011 zhang f , finkelstein j : inconsistency in race and ethnic classication in pharmacogenetics studies and its potential clinical implications . 
therapies - for - cancer / shi y , au js , thongprasert s , et al : a prospective , molecular epidemiology study of egfr mutations in asian patients with advanced non - small - cell lung cancer of adenocarcinoma histology ( pioneer )  . 
j thorac oncol 9 : 154 - 162 , 2014 soria j - c , ohe y , vansteenkiste j , et al : osimertinib in untreated egfr - mutated advanced nonsmall - cell lung cancer . 
n engl j med 378 : 113 - 125 , 2018 robson m , im s - a , senkus e , et al : olaparib for metastatic breast cancer in patients with a germline brca mutation . 
binder kar , mick r , ohara m , et al : abstract ct234 : a phase ii , single arm study of maintenance rucaparib in patients with platinum - sensitive advanced pancreatic cancer and a pathogenic germline or somatic mutation in brca1 , brca2 or palb2 . 
presley cj , soulos pr , chiang ac , et al : disparities in next generation sequencing in a population - based community cohort of patients with advanced non - small cell lung cancer . 
kwiatkowski k , coe k , bailar jc , et al : inclusion of minorities and women in cancer clinical trials , a decade later : have we improved ? cancer 119 : 2956 - 2963 , 22 . 
j health care poor underserved 20 : 896 - 913 , 2009 van ryn m , burke j : the effect of patient race and socio - economic status on physicians perceptions of patients . 
cooper la , roter dl , carson ka , et al : the associations of clinicians implicit attitudes about race with medical visit communication and patient ratings of interpersonal care . 
sharma s , guttmann d , small ds , et al : effect of introducing a default order in the electronic medical record on unnecessary daily imaging during palliative radiotherapy for adults with cancer . 
grebe ta , khushf g , chen m , et al : the interface of genomic information with the electronic health record : a points to consider statement of the american college of medical genetics and genomics ( acmg )  . 
lau - min ks , asher sb , chen j , et al : real - world integration of genomic data into the electronic health record : the pennchart genomics initiative . 
cheema pk , menjak ib , winterton - perks z , et al : impact of reex egfr / alk testing on time to treatment of patients with advanced nonsquamous nonsmallmayo clinic proc 95 : 476 - 487 , 2020 cell lung cancer . 
new york , ecco , 2004 iyengar ss , lepper mr : when choice is demotivating : can one desire too much of a good thing ? j personal soc psychol 79 : 995 - 1006 , 2000 jacoby j : perspectives on information overload . 
 balancing raf , mek , and egfr inhibitor doses to achieve clinical responses and modulate toxicity in braf v600e colorectal cancer introduction recent years have seen dramatic clinical advances in targeting the erk pathway with the us food and drug administration approval of several selective inhibitors of raf and mek.1 - 5 clinical trials of these agents indicate that near - complete inhibition of pathway signaling is necessary to effectively inhibit tumor growth.6 targeted approaches have been most successful in braf v600e tumors because of the relatively wide therapeutic index of raf inhibitors ( vemurafenib and dabrafenib ) , which inhibit signaling in cells with braf v600 mutants but cause paradoxical activation of erk signaling in normal cells that are wild type for raf kinases . 
combining these agents ( with raf and mek inhibitors for braf v600e melanoma or lung cancer and with raf , mek , and epidermal growth factor receptor [ egfr ] inhibitors for braf v600e colorectal cancer ) to profoundly inhibit erk signaling has led to improved antitumor activity.7 combination therapy has also been shown to offset the toxicities caused by raf inhibitors , such as the development of keratoacanthoma and squamous cell carcinoma , resulting from paradoxical erk activation with these agents . the role of raf inhibitors in offsetting mek inhibitor toxicity and the need for dose intensity to modulate opposing toxicities is less clear . 
in the phase iii trial of trametinib in melanoma , grade 3 or 4 acneiform dermatitis occurred in 8% of trametinib - treated patients , whereas in the phase iii trial of the combination of dabrafenib and trametinib , no patient had grade 3 or 4 acneiform dermatitis.8 , 9 combinations of raf and egfr inhibitors have also had a lower incidence of acneiform rash than seen with egfr inhibitors alone.7 , 10 , 11 this is also likely because of the opposite effects of raf and egfr inhibitors on mek activation in normal cells . 
we now report the course of a patient with braf v600e colorectal cancer treated with dabrafenib , trametinib , and panitumumab in a phase ii clinical trial and characterize the effect on toxicities of different dose levels of these agents in this patient . 
she received 6 months of adjuvant folfox ( folinic acid , fluorouracil , and oxaliplatin ) chemotherapy , and imaging 3 months after completion of adjuvant therapy showed recurrent disease with peritoneal carcinomatosis ( primarily omental caking ) and ascites . 
she then provided written informed consent to participate in a clinical trial for patients with braf v600e colorectal cancer and was started on the combination of dabrafenib ( 150 mg orally twice daily ) , trametinib ( 2 mg orally once daily ) , and panitumumab ( 6 mg / kg intravenously every 2 weeks ) , all at the full us food and drug administration approved single - agent doses ( fig 1a ) , with prophylactic doxycycline ( 28 - day cycles )  . 
during the first cycle , she developed grade 2 neutropenia that was attributed to dabrafenib ; therefore , the dose of this drug was decreased one dose level to 100 mg orally twice daily . 
despite these modifications , during the fourth cycle , the rash became grade 3 ; skin cultures were positive for methicillin - sensitive staphylococcus aureus , and she was treated with sulfamethoxazole and trimethopri given the lack of response of the rash to medical treatment , with sponsor approval , the dose of dabrafenib was escalated to 100 mg orally twice daily during the fifth cycle , which was followed by clinical improvement of skin toxicity to grade 1 . 
in terms of clinical efficacy , her disease was difficult to measure on imaging , but response evaluation criteria in solid tumors review was consistent with stable disease on the computed tomography evaluations at the 6 - , 12 - , and 18 - week assessments . 
the patient died as a result of disease progression 1 month after stopping the study treatment . discussion this case shows the opposing effects of raf inhibitors and egfr and mek inhibitors on skin and the importance of raf inhibitor dose - intensity for clinical efficacy and for offsetting toxicity in combination regimens with other erk pathway inhibitors . 
as the dose of dabrafenib was reduced , skin toxicity resulting from the egfr and mek inhibitors became more pronounced , and when the dabrafenib dose was raised , the toxicity improved , confirming that dabrafenib was modulating skin toxicity resulting from the egfr and mek inhibitors . 
differences in raf signaling underlie the differing effects of raf inhibitors seen in normal and tumor tissues ; in normal tissues , raf signals as homoand heterodimers activated by ras , whereas braf v600 mutants , which lead to high erk activation and feedback suppression of upstream signaling and ras , signal uniquely as constitutively activated monomers . 
in braf v600mutant tumors , this leads to suppression of activated monomers , and in tissues with wildtype raf kinases ( functioning as dimers ) , this leads to transactivation of raf dimers.12 , 13 thus , clinical efficacy and the modulation of toxicity in combination regimens are linked ; inhibition of braf v600e monomers and paradoxical activation of erk occur at the same doses . 
the absence of clinically appreciable opposing effects to egfr or mek inhibitors in normal tissues , as occurred in this case , thus suggests inadequate occupation of the first site of raf dimers in normal tissues as well as of braf v600e monomers.14 this case shows the fine balance of the raf inhibitor dose in the clinical range for treatment efficacy and adverse effects . 
when the raf inhibitor was reduced to a dose level of 50% of the recommended dose , toxicities from unopposed erk inhibition resulting from the mek and egfr inhibitors became problematic , and the tumor began progressing through treatment . 
also shown is inferred phosphorylated erk ( p - erk ) level in skin with inflection point from mild to severe erk inhibition occurring at the dabrafenib dose of 75 mg orally twice daily . 
 ( b ) grade 2 acneiform rash , paronychia , and splinter hemorrhages . raf inhibitor dose can rapidly improve toxicity but may not overcome resistance that has developed to treatment . 
although tumor progression in this case was likely multifactorial , incomplete inhibition of braf v600e at a lower dose of dabrafenib and the likely higher threshold to reestablish erk suppression after incomplete pathway inhibition may have contributed to the short duration of clinical benefit of approximately 4 months . 
 mario lacouture consulting or advisory role : novartis , novocure , legacy healthcare services , janssen research & development , adgero biopharmaceuticals , galderma , amryt pharmaceuticals , lindi , debiopharm group , merck , legacy healthcare services , helsinn healthcare , celldex , menlo therapeutics , johnson & johnson , roche research funding : veloce , us biotest jonathan hersch no relationship to disclose rona yaeger research funding : array biopharma , glaxosmithkline , novartis travel , accommodations , expenses : array biopharma affiliation all authors : memorial sloan - kettering cancer center , new york , ny . support references supported by the byrne fund ( r.y. ) and national institutes of health memorial sloan kettering cancer center core grant no . 
long gv , stroyakovskiy d , gogas h , et al : dabrafenib and trametinib versus dabrafenib and placebo for val600 braf - mutant melanoma : a multicentre , double - blind , phase 3 randomised controlled trial . 
planchard d , smit ef , groen hjm , et al : dabrafenib plus trametinib in patients with previously untreated brafv600e - mutant metastatic non - small - cell lung cancer : an open - label , phase 2 trial . 
van geel rmjm , tabernero j , elez e , et al : a phase ib dose - escalation study of encorafenib and cetuximab with or without alpelisib in metastatic braf - mutant colorectal cancer . 
yaeger r , yao z , hyman dm , et al : mechanisms of acquired resistance to braf v600e inhibition in colon cancers converge on raf dimerization and are sensitive to its inhibition . 
 dramatic response to crizotinib in a patient with lung cancer positive for an hla - drb1 - met gene fusion introduction nonsmall - cell lung cancer ( nsclc ) is a disease in which tumor growth is commonly driven by alterations along the receptor tyrosine kinase ras - rafmitogen - activated protein kinase pathway . 
the patient declined adjuvant chemotherapy . eighteen months after diagnosis , surveillance imaging with a fluorodeoxyglucose positron emission tomography / computed tomography ( ct ) scan demonstrated new lesions within the right and left lower lung lobe , as well as a pericardiac nodule and an enlarged precarinal lymph node . 
this sample was negative for alk and ros1 rearrangements . there was insufficient sample for additional molecular testing . treatment with carboplatin and pemetrexed was commenced for four cycles , followed by continuation maintenance pemetrexed with stable disease as best response . 
at her second opinion appointment , tissue from the patients second lung resection was subjected to additional molecular analysis . methods anchored multiplex polymerase chain reaction total nucleic acid was extracted from formalinfixed , paraffin - embedded processed material from the resection sample by using the agencourt kurtis d . 
 ( a ) schematic of the detected fusion with breakpoints between exons indicated ( transcript fusion breakpoints map to the following genomic coordinates [ hg19 ] : hla - drb1 , chromosome 6 : 32548024 ; met , chromosome 7 : 116414935 ; top )  . 
this rnabased assay allows for fusion gene detection without a priori knowledge of the fusion partner.18 the assay detected a previously undescribed fusion of hla - drb1 exon 5 ( nm_002124 ) to met exon 15 ( nm_000245 ) , which was predicted to be in - frame and to preserve the met kinase domain ( fig 1a )  . this finding was confirmed on a separate extraction and repeat analysis of the resection sample . 
whereas the 59 fusion partner is novel , previously described fusions to met , including fusions to c8orf34 , baiap2l1 , tfg , and clip2 , have also been reported to occur at exon 15.13 , 14 a reverse transcriptase polymerase chain reaction assay , followed by sanger sequencing of the product confirmed the existence of this fusion transcript ( fig 1a )  . expression of any fusion gene relies on the activity of the promoter of the 59 partner . 
although this does not directly demonstrate activity of the hladrb1 promoteras other b - subunit genes can also form the heterodimer in this protein complexit suggests the general expression of the gene class , which tends to be coordinately expressed . 
the observation of high hla class ii ( dr ) expression is in accordance with a previous study that demonstrated robust major histocompatibility class ii expression specifically in lung adenocarcinoma.19 to demonstrate the activation of hgfr - mediated signaling in the sample , we performed a pla.20 pla measures the formation of protein complexes , in this case , between hgfr and the adaptor gab1 , which occurs upon hgfr activation . 
this assay demonstrated hgfr - gab1 complex formation at levels similar to samples that were positive for met exon 14 skipping , which suggests that hgfr is activated ( fig 2 )  . of importance , the sample was found to be negative for other known oncogenic drivers of lung cancer , including alk and ros1 fusions , as well as met exon 14 skipping . 
any of these three aberrations would be expected to confer sensitivity to crizotinib ; however , if present in this sample , they would have been detected by the amp - based assay . 
lack of alk rearrangement was confirmed by immunohistochemistry . met amplification may also promote sensitivity to crizotinib ; however , met fluorescent in situ hybridization did not reveal an increase in met copy number . 
an ngs - based mutational assay ( illumina trusight tumor 26 ) that covers commonly mutated regions in 26 genes , including egfr , kras , and braf , revealed no nonsynonymous coding mutations . the patient began treatment with off - label oral crizotinib 250 mg twice daily . 
after 6 weeks of therapy , repeat ct showed complete resolution of the previously observed left upper lobe perihilar and right lower lobe lung nodules with no new lesions ( fig 3 )  . 
the patient experienced grade 1 fatigue , grade 1 dysgeusia , grade 2 anorexia , grade 1 visual disturbance , grade 1 transaminitis , grade 1 creatinine increase , grade 1 hyponatremia , and grade 3 hypokalemia ( grade 1 hypokalemia at baseline )  . 
this robust response remains at 8 months on therapy . discussion in this study , we described the discovery of a novel fusion gene that involves met in a tumor sample from a patient with nsclc who was negative for fig 2 . 
 ( a ) met - gab1 proximity ligation assay ( pla ) analysis of formalinfixed , paraffin - embedded samples from the hladrb1 - met patient , two different met exon 14 ( ex14 ) skippingpositive patients , and an alk rearrangementpositive patient ( negative control )  . scale bar is 50 microns . ( b ) quantification of pla analysis displayed as the average number of dots per nucleus . 
the hla - drb1 - met sample displayed a significantly higher pla score than did the alk sample , as determined by analysis of variance followed by bonferronis post hoc analysis . 
contrastenhanced computed tomography scans of the chest of the patient ( a ) before and ( b ) approximately 6 weeks and ( c ) 3 months after starting crizotinib 250 mg twice daily . 
arrows highlight lung lesions before and after therapy . shown are four of 14 lesions ; the remaining 10 lesions had regressed by 6 weeks , with an ongoing response at 3 months . other known oncogenic drivers , and , in particular , other known targets of crizotinib . 
the patient demonstrated a dramatic response to off - label treatment with crizotinib , a us food and drug administrationapproved small - molecule tyrosine kinase inhibitor with activity against hgfr . this finding suggests that the met fusion gene product serves as an oncogenic driver in the patients tumor . 
future studies are needed to determine the specific mechanism of action of this novel fusion gene , although overexpression of the met kinase domain may be sufficient to activate hgfr - mediated signaling . 
it is also tempting to speculate that , as the fusion occurred to met exon 15 , the lack of the ubiquitination motif that is found in exon 14 results in impaired degradationsimilar to the met exon 14 skipping isoform.21 for clinical purposes , it is now imperative to know the driver oncogene status of patients with nsclc . 
until recently , test a small number of genes to guide clinical decision making , and this could be achieved by using single - gene assays.22 however , the recent it was sufficient rapid expansion in the number of characterized driver oncogenes , the increase in the number of approved therapies , and the large number of clinical studies now available that are testing drugs that target these novel oncogenes necessitates the evaluation of multiple genes simultaneously . ngs - based assays are well suited to meet this requirement because of the ability to sequence in massively parallel fashion . 
the ability of this assay to detect fusions without prior knowledge of the fusion partner was critical in this case , as fusion of met to hla - drb1 has not been reported previously . in conclusion , we provide evidence that met fusions may be another class of actionable alteration in nsclc . 
doebele honoraria : pfizer , astrazeneca , ariad pharmaceuticals , guardant health consulting or advisory role : pfizer , oncomed , trovagene , ignyta , green peptide , astrazeneca research funding : mirati therapeutics ( inst ) , abbott molecular , loxo oncology ( inst ) , ignyta ( inst ) patents , royalties , other intellectual property : licensing fees from abbott molecular for patent pct / us2013 / 057495 , licensing fees for biologic material from ariad pharmaceuticals ( inst ) , licensing fees for biologic materials from gvkbio , licensing fees for biologic materials from loxo oncology ( inst ) travel , accommodations , expenses : ignyta , ariad pharmaceuticals dara l . 
drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 2 , single - arm trial . 
tabernero j , bahleda r , dienstmann r , et al : phase i dose - escalation study of jnj - 42756493 , an oral pan - fibroblast growth factor receptor inhibitor , in patients with advanced solid tumors . 
zou hy , li q , lee jh , et al : an orally available small - molecule inhibitor of c - met , pf - 2341066 , exhibits cytoreductive antitumor efficacy through antiproliferative and antiangiogenic mechanisms . 
ou sh , kwak el , siwak - tapp c , et al : activity of crizotinib ( pf02341066 ) , a dual mesenchymal - epithelial transition ( met ) and anaplastic lymphoma kinase ( alk ) inhibitor , in a non - small cell lung cancer patient with de novo met amplification . 
frampton gm , ali sm , rosenzweig m , et al : activation of met via diverse exon 14 splicing alterations occurs in multiple tumor types and confers clinical sensitivity to met inhibitors . 
paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
awad mm : impaired c - met receptor degradation mediated by met exon 14 mutations in non - small - cell lung cancer . j clin oncol 34 : 879 - 881 , 2016 22 . 
lindeman ni , cagle pt , beasley mb , et al : molecular testing guideline for selection of lung cancer patients for egfr and alk tyrosine kinase inhibitors : guideline from the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology . 
 immunological differences between immune - rich estrogen receptorpositive and immune - rich triple - negative breast cancers tess omeara , ba1 ; michal marczyk , phd1 , 2 ; tao qing , phd1 ; vesal yaghoobi , md3 ; kim blenman , ms , phd1 ; kimberly cole , md3 ; vasiliki pelekanou , md , phd3 , 4 ; david l . 
we compared expression of immune cell markers , immune function metagenes , and immuno - oncology therapeutic targets among immune - rich subtypes . results relative fractions of resting mast cells ( tcga padj = .009 ; metabric padj = 4.09e - 15 ) , cd8 + t cells ( tcga padj = .015 ; metabric padj = 0.390 ) , and m2 - like macrophages ( tcga padj = 4.68e - 05 ; metabric padj = .435 ) were higher in immune - rich er - positive bcs , but m0 - like macrophages ( tcga padj = 0.015 ; metabric padj = .004 ) and m1 - like macrophages ( tcga padj = 9.39e - 08 ; metabric padj = 6.24e - 11 ) were higher in immune - rich tnbcs . 
ninety - one immune - related genes ( eg , cxcl14 , csf3r , tgf - b3 , lrrc32 / garp , tgfb - r2 ) and a transforming growth factor ( tgf - ) response metagene were signicantly overexpressed in immune - rich er - positive bcs , whereas 41 immune - related genes ( eg , ifng , pd - l1 , ctla4 , magea4 ) were overexpressed in immune - rich tnbcs in both discovery and validation data sets . 
tgfpathway member genes correlated negatively with expression of immune activation markers ( ifng , granzyme - b , perforin ) and positively with m2 - like macrophages ( il4 , il10 , and mmp9 ) and regulatory t - cell ( foxp3 ) markers in both subtypes . conclusion different immunotherapy strategies may be optimal in immune - rich er - positive bc and tnbc . drugs targeting the tgfpathway and m2 - like macrophages are promising strategies in immune - rich erpositive bcs to augment antitumor immunity . jco precis oncol 4 : 767 - 779 . 
 omeara et al context key objective does the immune microenvironment of immune - rich estrogen receptorpositive breast cancer ( er - positive bc ) differ from the immune microenvironment of immune - rich triple - negative bc ( tnbc ) ? knowledge generated relative fractions of mast cells and m2 - like macrophages are higher in the immune microenvironment of immune - rich erpositive bc , whereas fractions of m0 - like and m1 - like macrophages are higher in immune - rich tnbc . 
her2 - positive patients were excluded , and only er - positive / her2 - negative ( herein designated er - positive ; tcga , n = 627 ; metabric , n = 1 , 186 ) and er - negative / her2 - negative ( herein designated tnbc ; tcga , n = 191 ; metabric , n = 279 ) patients were included in this analysis . 
we obtained formalin - xed parafn - embedded tissues from 63 tnbcs and 53 erpositive , treatment - nave , stage i to iii bcs from yale pathology tissue archives , matched by distribution of histologic grade , for quantitative immunouorescence ( qif ) and automated quantitative analysis ( aqua )  . assessment of immune cell content and selection of immune - rich patients a gene expression signature score developed by danaher et al19 was used to score each tcga and metabric patient for total tils . 
the total til gene signature score is the average of scores representing 11 immune cell subpopulations ( cd45 , macrophages , cd8 + t cells , t cells , cytotoxic cells , exhausted cd8 + cells , th1 cells , b cells , neutrophils , natural killer [ nk ] cells , cd56dim nk cells )  . log2 + 1 - transformed expression was used to calculate total til gene signature scores from tcga ( rna - seq ) and metabric ( microarray ) data . 
the til metagene score distribution was plotted for the pooled er - positive bc and tnbc patients , and patients with scores in the top 25th percentile of the distribution were dened as immune - rich . for 156 basal - like cancers in tcga ( er - positive bc , n = 21 ; tnbc , n = 135 ) , histologic til counts were also available.20 , 21 for these patients , we assessed the correlation between histologic til count and til gene expression score . 
we also assessed correlations between til gene signature score and pam50 subtype , tumor mutation burden ( tmb ) , and ki - 67 expression level in the tcga data when this information was available ( er - positive bc , n = 191 ; tnbc , n = 697 )  . 
pam50 subtypes and tmb categories were obtained from a previous publication , and ki - 67 categories were dened as greater than or less than the median log2 + 1 - transformed ki - 67 expression across tcga patients.22 survival analysis progression - free survival ( pfs ) and overall survival ( os ) times were available for 807 tcga patients ( er - positive bcs , n = 189 ; tnbcs , n = 618 ) .23 pfs and os were compared by er subtype within immune - rich patients ( erpositive bcs , n = 114 ; tnbcs , n = 84 ) and within nonimmune - rich patients ( er - positive bcs , n = 504 ; tnbcs , n = 105 ) using the survival and survminer r packages.24 assessment of immune cell subpopulations cibersort , an analytical tool that uses support vector regression , was used to estimate the relative proportions of 9 aggregated immune cell populations and 22 subpopulations in immune - rich er - positive bcs and immunerich tnbcs.25 , 26 the average relative fraction and standard error of the mean of each immune cell population were compared by subtype . 
 immunological differences between immune - rich er - positive bcs and tnbcs calculated gene expression signature scores of overall macrophages , m1 - like macrophages , m2 - like macrophages , and the transforming growth factor ( tgf - ) signaling response were obtained from previous publications and were compared between patients with erpositive bcs and those with tnbcs.27 - 29 slopes of linear regression curves between total tils and metagene expression signatures were compared by using a t test based on standard error in the linear regression models.30 formalinxed parafn - embedded tissue microarrays were stained for the nuclear marker 4 ( cid : 1 ) , 6 - diamidino - 2 - phenylindole and the pan - macrophage marker cd68 , and multiplexed qif and aqua were used to quantify expression levels in yale er - positive bc and tnbc patients as previously described.31 differential gene expression analysis the deseq2 ( tcga , rna - seq data ) and limma ( metabric , microarray data ) r packages were used for differential gene expression analysis of 779 immunerelated genes ( nanostring pancancer io 360 panel , nanostring technologies , seattle , wa ) and 137 currently available immuno - oncology drug target genes between immune - rich er - positive bcs and immune - rich tnbcs.32 - 34 availability of rna expression data for each member gene in tcga and metabric databases is summarized in the data supplement . 
genes with false discovery rate padj , .05 were considered signicantly differentially expressed for a broad investigation of differentially regulated immune pathways . statistical analysis all statistical analyses were performed in r v 3.5.0. 
in tcga , the 75th percentile til metagene score was 5.92 , and it categorized 119 er - positive bcs ( 19% ) and 89 tnbcs ( 45% ) as being immune rich . 
the total til gene signature scores correlated moderately but signicantly with histologic til scores in tcga ( r = 0.44 ; p = 1.18e - 08 ; fig 2a ) when these data were available . 
in tcga , there was no statistically signicant difference between the distribution of pam50 subtypes or ki - 67 expression levels between immune - rich and nonimmune - rich er - positive bcs . 
patients with immune - rich er - positive bcs had signicantly higher tmb than patients with nonimmune - rich er - positive bcs ; this difference was not seen among patients with tnbcs . 
for a subset of tcga patients with available survival formation ( n = 804 ) , pfs and os were compared by subtype ( data supplement )  . immune - rich patients had similar pfs and os regardless of er status . 
in contrast , among the nonimmune - rich cancers , os was signicantly longer in patients with er - positive bcs than in patients with tnbcs ( p = .043 ) , as expected . immune cell subpopulations in the tumor microenvironment of immune - rich er - positive bcs and immune - rich tnbcs by using cibersort , we found higher relative fractions of t cells ( padj = .009 ) and mast cells ( padj = .0005 ) in patients with immune - rich er - positive bcs compared with those who had immune - rich tnbcs ( fig 3a ) in tcga . in patients with immune - rich tnbcs , the relative fractions of macrophages ( padj = .026 ) and nk cells ( padj = .0007 ) were higher relative to those in patients with immune - rich er - positive bcs . 
the higher relative fractions of t cells ( padj = .005 ) and mast cells ( padj = 1.73e - 20 ) in immunerich er - positive bcs and the higher relative fraction of macrophages ( padj = 1.22e - 06 ) in immune - rich tnbcs were also observed in metabric ( fig 3b )  . 
qif also showed higher overall expression of the pan - macrophage marker cd68 in tnbc tissues relative to tissue from erpositive bcs from yale pathology archives ( p = .011 ; fig 3c )  . next , we examined differences among 22 immune cell subpopulations . in immune - rich er - positive tumors in tcga , the relative fractions of cd8 + t cells ( padj = .015 ) and resting mast cells ( tcga padj = .009 ) were higher relative to those in immune - rich tnbc tumors in both data sets ( fig 3d )  . 
in contrast , the relative fractions of m0 - like macrophages ( padj = .015 ) and m1 - like macrophages ( padj = 9.39e - 08 ) were signicantly higher in patients with immune - rich tnbcs compared with those with immunerich er - positive bcs . 
 ( a - b ) gene signature scores were calculated for 11 immune cell subpopulations for patients with er - positive bcs and tnbcs in ( a ) the cancer genome atlas ( tcga ) and ( b ) molecular taxonomy of breast cancer international consortium ( metabric ) databases , as described by danaher et al.19 the x - axis indicates immune cell subpopulations plus the total tumor - inltrating lymphocyte ( til ) population . 
immune - rich erpositive bcs had higher m2 - like macrophage ( p = .012 ) and tgfresponse ( p = 0.035 ) metagene expression scores ( fig 4a )  . 
the subtype - specic differences in m1 - like macrophage ( p = 1.85e - 04 ) and tgfresponse ( p = .029 ) metagene scores signicantly increased with higher total til gene signature scores , whereas the differences in overall macrophage ( p = .786 ) and m2 - like macrophage ( p = .097 ) scores between cancer subtypes were not specic to immune - rich patients ( fig 4b )  . 
 ( a ) for a subset of basal - like patients from the cancer genome atlas ( tcga ) with previously published histologic til scores ( n = 156 ) according to danaher et al , 19 the total til gene signature scores ( x - axis ) were correlated with histologic stromal til counts ( y - axis )  . 
 ( b - d ) for all patients with er - positive bcs ( n = 697 ) and tnbcs ( n = 191 ) in tcga , patients were classied as immune cell high ( danaher et l19 total til gene signature score in the top 25th percentile ) or low ( danaher total til gene signature scores in the bottom 75th percentile ) , represented on the x - axis . 
distributions of ( b ) pam50 subtypes , ( c ) ki - 67 expression categories and ( d ) tumor mutation burden ( tmb ) categories were compared between patients with immune - rich high and low er - positive bcs and tnbcs separately . 
pam50 and tmb categories were obtained from previous publications , and ki - 67 categories were dened as greater than ( high ) or less than ( low ) the median ki - 67 expression level across all patients . differential expression of immune - related genes and immuno - oncology drug target genes between immune - rich er - positive bcs and immune - rich tnbcs at the individual gene level , 132 of 754 immune - related genes were signicantly overexpressed in tcga immunerich er - positive bcs . 
ninety - one of these immune - related genes , including mast cell genes ms4a2 and cpa3 and therapeutic targets cxcl14 , cx3cr1 , and potential csf3r , were also upregulated in metabric patients with immune - rich er - positive bcs ( data supplement )  . immune - rich tnbcs , 303 immune - related genes were overexpressed compared with immune - rich er - positive bcs in tcga , and 218 of these were validated in metabric . 
sixteen of 136 available therapeutic target genes were overexpressed in tcga patients with immune - rich er - positive bcs , and 12 of these , including 3 members of the tgfsignaling pathway ( tgf - 3 , lrrc32 / garp , and tgf - r2 ) , were also overexpressed in metabric patients with immune - rich er - positive bcs ( table 1 ; data supplement )  . 
for patients from ( a ) the cancer genome atlas ( tcga ) and ( b ) molecular taxonomy of breast cancer international consortium ( metabric ) databases , 9 aggregate immune cell populations are listed on the x - axis , and the average fraction of each immune cell population for a certain subtype is quantied on the y - axis . 
 ( c ) quantitative immunouorescence ( qif ) signal was compared between estrogen receptorpositive breast cancer ( er - positive bc ; , n = 53 ) and triple - negative bc ( tnbc ; n = 63 ) formalin - xed parafn - embedded tumor microarray tissues . 
subtype is shown on the x - axis , and cd68 qif signal in the total 4 ( cid : 1 ) , 6 - diamidino - 2 - phenylindole ( dapi ) compartment is quantied on the y - axis . 
for ( d ) tcga and ( e ) metabric patients , 22 immune cell populations derived by cibersort are listed on the x - axis , and the average fraction of each immune cell population for a certain subtype is quantied on the y - axis . 
false discovery rate padj values are provided for tcga ( er - positive bcs , n = 119 ; tnbcs , n = 86 ) and metabric ( er - positive bcs , n = 225 ; tnbcs , n = 140 ) patients . 
comparison of macrophage population and transforming growth factor ( tgf - ) response metagene expression scores between patients with immune - rich estrogen receptorpositive breast cancers ( er - positive bcs ) and those with triple - negative bcs ( tnbcs ) in the cancer genome atlas ( tcga )  . 
 ( a ) metagene expression scores for overall macrophages , m1 - like macrophages , m2 - like macrophages , and tgfresponse were compared between immune - rich er - positive bc ( red , n = 119 ) and immune - rich tnbc ( blue , n = 86 ) patients in tcga . 
 ( b ) for all patients with er - positive bcs ( n = 697 ) and tnbcs ( n = 191 ) in tcga , gene expression signature scores for overall macrophages , m1 - like macrophages , m2 - like macrophages , and tgfresponse ( y - axis ) were plotted against total til gene signature scores ( x - axis )  . 
linear regression lines for each subtype with 95% cis are shown in red ( er - positive bc ) or blue ( tnbc )  . and the cancer - testis antigen , magea4 , were also overexpressed in immune - rich tnbcs in metabric . correlation between tgfpathway expression and other immune - related genes tgfis a pleotropic cytokine that can stimulate regulatory induce m2 - like macrophage polarization , and t cells , suppress effector t cells , nk cells , and dendritic cells . furthermore , tgfsignaling has been linked to an immune - excluded phenotype in cancer . 
we therefore examined correlations between the differentially expressed tgfpathway members ( tgf - 3 , lrrc32 , and tgfr2 ) and the expression levels of the 53 immuno - oncology drug target genes that were differentially expressed in both data sets ( 12 upregulated in immune - rich er - positive bcs , 41 upregulated in immune - rich tnbcs ) across immunerich tnbcs and er - positive bcs . in both tcga and metabric , expression of the tgfpathway members correlated positively with each other and negatively with most immune activation markers ( fig 5a - b ; data supplement )  . 
similar correlation patterns were seen between tgfpathway members and immune activation marker expression when only immune - rich er - positive bcs were analyzed ( fig 5c - d )  . 
we also noted a positive correlation between expression of tgf - 1 and the m2 - like macrophage markers il4 ( r = 0.24 ) , il10 ( r = 0.38 ) , and mmp9 ( r = 0.43 ) as well as the regulatory t - cell marker foxp3 ( r = 0.42 ) in the tcga data . discussion in this report , we used a gene expression signature of total tils to identify patients with immune - rich er - positive bcs and tnbcs in 2 publicly available databases to compare the tumor immune microenvironment of these subtypes . the patients with immune - rich er - positive bcs had signicantly higher tmb than patients with nonimmune - rich er - positive bcs , but no difference in tmb was seen between immune - rich and nonimmune - rich tnbcs . 
for ( a ) the cancer genome atlas ( tcga ) and ( b ) molecular taxonomy of breast cancer international consortium ( metabric ) patients , correlation matrices display the pearson correlation coefcients between expression levels of 53 immuno - oncology drug targets across patients with immune - rich estrogen receptorpositive breast cancers ( er - positive bcs ) and triple - negative bcs ( tnbcs )  . 
for tcga , the number of patients with immune - rich er - positive bcs was 119 , and for tnbcs , it was 86 ; for metabric , the number of patients with immune - rich er - positive bcs was 225 , and for tnbcs , it was 140 . 
for ( c ) tcga and ( d ) metabric patients , correlation matrices display the pearson correlation coefcients between expression levels of 53 immuno - oncology drug targets in patients with immune - rich er - positive bc alone . 
the number of patients with immune - rich er - positive bcs in tcga was 119 , and in metabric , it was 225 . results are consistent with previous reports.11 , 36 approximately 70% of the immune - rich er - positive bcs we identied were luminal a molecular subtype , and the pam50 subtype distribution and ki - 67 expression were similar between immune - rich and nonimmune - rich er - positive bcs . an os difference was detected between patients with nonimmune - rich er - positive bcs relative to nonimmunerich tnbcs , but no similar statistically signicant difference was seen between patients with immune - rich er - positive bcs and immune - rich tnbcs ( both groups had excellent long - term survival )  . 
by using deconvolution methods , we observed differences in the relative fractions of immune cell subpopulations between immune - rich er - positive bcs and immune - rich tnbcs . immune - rich er - positive bcs had higher relative fractions of m2 - like macrophages , cd8 + t cells , and resting mast cell populations , whereas immunerich tnbcs had overall higher macrophage content and higher m0 - like and m1 - like macrophage populations . 
higher overall cd68 protein expression in tnbcs was also conrmed by immunohistochemistry . interestingly , immune - rich er - positive bcs had higher expression of a tgfsignaling metagene and showed coordinated overexpression of tgf - 3 , tgf - r2 , and lrrc32 compared with immune - rich tnbcs . 
the tgfpathway is activated by ligands tgf - 1 , tgf - 2 , and tgf3 that bind to membrane - bound serine / threonine protein receptor kinases composed of subunits tgf - r1 and tgfr2 . 
although the tgfligand isoforms are more than 75% similar in amino acid structure , tgf - r2 has increased afnity for tgf - 1 and tgf - 3 relative to tgf2.37 lrrc32 encodes the garp protein that tethers tgfligands to the cell membrane to prime its activation.38 the simultaneous upregulation of the ligand , receptor , and signaling components suggests a functional role for the tgfpathway in immune - rich er - positive bcs . the immune - attenuating function of tgfsignaling in the tumor microenvironment has been extensively studied in vitro and in vivo . 
in early in tumorigenesis , tgfacts as a tumor suppressor , inducing apoptosis in premalignant cells and inhibiting proliferation.39 after tumor formation , tgfpromotes cancer progression through suppressing the host antitumor immune response.40 among other roles , tgfinhibits cd8 + effector t - cell function , inhibits the th1 helper t - cell phenotype , activates foxp3 - positive regulatory t cells , drives m2 - like macrophage polarization , and excludes immune cells from the tumor compartment.41 - 45 the distinct roles of the different tgfisoforms in cancer remain undened . 
among the 3 isoforms , tgf - 3 is the most potent stimulator of neovascularization in models of wound healing and the most potent inhibitor of granulocyte - macrophage colonystimulating factormediated hematopoiesis in the bone marrow . 
tgf - 1 and tgf - 3 are equally potent stimulators of extracellular matrix collagen deposition in models of pulmonary brosis.46 overall , high tgfsignaling is also associated with lesser response to immune checkpoint inhibitors.41 , 42 on an expression level , we found higher relative fractions of cd8 + t cells in immune - rich er - positive bcs as well as higher tgfsignaling ; these cd8 + t cells in immune - rich er - positive patients may therefore lack robust effector cytotoxic function or be excluded from the tumor compartment by augmented tgfsignaling . tgfcan be released by cancer cells as well as by m2 - like macrophages in a positive feedback loop to attenuate antitumor immunity.47 in several studies , the presence of m2 - like macrophages in bc was associated with poor prognosis , and reprogramming of macrophages toward the m1 - like phenotype has been shown to increase responsiveness to immune checkpoint therapy in experimental models.48 , 49 a recent study found that a macrophage - dependent autochthonous mouse model of luminal btype bc , inhibition of class iia histone deacetylase ( hdac ) by tmp195 induces the recruitment and differentiation of antitumor - type macrophages , reduces tumor burden and metastases , and enhances the durability of tumor reduction when combined with chemotherapy regimens or t - cell checkpoint blockade.50 this observation in an animal model of bc is consistent with our ndings in human tissues . 
our analyses also showed that expression of tgfpathway members correlated negatively with the expression of many immune activation markers including interferon ( ifn - ) , granzymes , and perforin , but correlated positively with m2 - like macrophage markers il4 , il10 , mmp9 , and regulatory t - cell marker foxp3 . 
although m2 - like macrophages in the tumor microenvironment may be the source of tgfsignaling , high levels of apolipoprotein b mrna editing enzyme , catalytic polypeptide - likeassociated mutational signatures that have been previously identied in patients with immunerich er - positive bcs may also contribute to upregulation of the tgfpathway in tumor cells and downstream recruitment of m2 - like macrophages.36 deconvolution of the leukocyte compartment also revealed a higher relative fraction of mast cells in immune - rich erpositive bcs ; this was corroborated by overexpression of the mast cell markers cpa3 and ms4a2 in patients with immune - rich er - positive bcs compared with those who have immune - rich tnbcs . 
how these cells inuence antitumor immunity is unknown , but high mast cell inltration in bc has been associated with er expression and favorable prognosis in earlier studies.51 , 52 in summary , our analysis of gene expression data is consistent with a more attenuated immune microenvironment mediated by increased tgfsignaling and m - 2 macrophage presence in immune - rich er - positive bcs . 
in this subset of er - positive bcs , we observed high relative fractions of cd8 + t cells , mast cells , and m2 - like macrophages with lower expression of granzyme - b , perforin , and ifn -  . 
in addition , practical assays that can distinguish patients with immune - rich and tgf - - high from patients with tgf - - low er - positive bcs are needed before these results can be applied in the clinic . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . vasiliki pelekanou employment : sano david l . 
rimm stock and other ownership interests : pixel gear honoraria : amgen , bristol myers squibb , ventana medical systems consulting or advisory role : perkin elmer , bristol myers squibb , astrazeneca , agendia , ultivue , merck , daiichi sankyo , glaxosmithkline , konica minolta , nanostring technologies , nextcure , cell signaling technology , roche , paige , cepheid , sano research funding : cepheid ( inst ) , perkin elmer ( inst ) , astrazeneca / medimmune ( inst ) , nextcure ( inst ) , eli lilly ( inst ) , nanostring technologies ( inst ) , navigate biopharma ( inst ) , ultivue ( inst ) , konica minolta ( inst ) , amgen ( inst ) patents , royalties , other intellectual property : rarecyte circulating tumor cells ; quantitative immunouorescence ( aqua ) ( inst ) travel , accommodations , expenses : ventana medical systems , nextcure , bristol - myers squibb lajos pusztai consulting or advisory role : h3 biomedicine , merck , novartis , seattle genetics , syndax pharmaceuticals , athenex , astrazeneca , genentech , bristol myers squibb , clovis oncology , immunomedics , eisai , almac diagnostics research funding : merck ( inst ) , genentech ( inst ) , seattle genetics ( inst ) , astrazeneca ( inst ) travel , accommodations , expenses : astrazeneca uncompensated relationships : nanostring technologies open payments link : 110878 / summary no other potential conicts of interest were reported . references bianchini g , qi y , alvarez rh , et al : molecular anatomy of breast cancer stroma and its prognostic value in estrogen receptor - positive and - negative cancers . j clin oncol 28 : 4316 - 4323 , 2010 karn t , pusztai l , holtrich u , et al : homogeneous datasets of triple negative breast cancers enable the identication of novel prognostic and predictive signatures . 
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cancer immunol res 3 : 326 - 332 , 2015 loi s , giobbe - hurder a , gombos a , et al : phase ib / ii study evaluating safety and efcacy of pembrolizumab and trastuzumab in patients with trastuzumabresistant her2 - positive metastatic breast cancer : results from the panacea ( ibcsg 45 - 13 / big 4 - 13 / keynote - 014 ) study . 
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tolaney sm , barroso - sousa r , keenan t , et al : randomized phase ii study of eribulin mesylate ( e ) with or without pembrolizumab ( p ) for hormone receptorpositive ( hr + ) metastatic breast cancer ( mbc )  . 
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statistics / breast - cancer - facts - and - gures / breast - cancer - facts - and - gures - 2017 - 2018.pdf van maaren mc , de munck l , strobbe lja , et al : ten - year recurrence rates for breast cancer subtypes in the netherlands : a large population - based study . 
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 novel alk fusion , ppfibp1 - alk , in pancreatic ductal adenocarcinoma responsive to alectinib and lorlatinib arjan gower , md , ms1 ; barry golestany , md2 ; jun gong , md3 ; aatur d . 
singhi , md , phd4 ; and andrew eugene hendifar , md , mph3 introduction pancreatic cancer is the seventh leading cause of cancer death among men and women worldwide , with  . 
430 , 000 deaths in 2018.1 despite advances in surgical techniques , radiation , and systemic treatment in the past few decades , overall survival for pancreatic cancer is extremely poor , with a 5 - year survival rate of 9%.2 current systemic treatment regimens for metastatic pancreatic cancer include folfirinox ( uorouracil , folic acid , oxaliplatin , and irinotecan ) , gemcitabine plus nab - paclitaxel , and liposomal irinotecan with uorouracil.3 - 6 approximately 88% - 95% of pancreatic adenocarcinomas harbor kras driver mutations . 
in row 1 , the circled hepatic lesion in the right lobe of the liver at baseline ( a ) before alectinib decreased in size ( b ) 2 months after alectinib . 
the patient experienced progression during alectinib treatment after 5 months and experienced progression during uorouracil , folic acid , oxaliplatin , and irinotecan treatment shortly thereafter . fluorescence in situ hybridization ( fish ) was negative . 
it has been shown that fish may have different sensitivities of detecting alk compared with next - generation sequencing or immunohistochemistry.27 of note , molecular proling was negative for kras , microsatellite instability , nf1 and p53 inactivating mutations , and cdkn2a / b loss . proling was positive for brca2 c.8007a.g ( silent ) and cdkn1b 407a.g , both of unknown clinical signicance . patient was started on folfirinox with radiographic response . 
however , because of the adverse effects of chemotherapy , including nausea and neuropathy , the patient was switched to alectinib 600 mg twice daily , given her alk fusion status . 
subsequent cell - free plasma ( guardant360 ; guardant health , redwood city , ca ) showed newly acquired alk mutations g1202r and v1180l in addition to the ppfibp1 - alk translocation . 
the patients disease has been stable on lorlatinib on 2 - month follow - up imaging , and she continues to be treated with lorlatinib ( figs 2 and 3 )  . discussion currently , there are no fda - approved targeted therapies for pancreatic cancer , and standard chemotherapy ( folfirinox ) for metastatic pancreatic cancer is quite toxic , with a median overall survival of approximately 11 months.3 to our knowledge , we present the seventh case of alk - positive metastatic pancreatic cancer with a novel ppfibp1 - alk fusion gene and the rst patient to be treated with alectinib as rst - line targeted therapy . 
the patient ultimately acquired alectinib - resistant alk mutations g1202r and v1180l ; however , the disease has been stable on the third - generation alk inhibitor lorlatinib . alk translocation in pancreatic cancer was rst described in 2017 , and there have been only 6 documented cases of alk - positive pancreatic adenocarcinoma through literature review ( table 1 )  . 
although the prevalence of the alk fusion gene is rare , at 0.16% , the prevalence increases to 1.3%.among patients , 50 years old12 the majority of alk fusion partners seen in nsclc includes eml4 , but other partners include strn , kcnq , klc1 , kif5b , ppm1b , and tgf genes.28 ppfibp1 - alk gene fusion was rst described in 2011 in a patient with pulmonary inammatory myobroblastic tumor29 and subsequently was described in epithelioid brous histiocytoma , 30 but it has never been described in nsclc or pancreatic cancer . 
of the 6 patients with alk - positive pancreatic cancer , 4 patients had eml4alk translocation , 1 patient had strn - alk , and 1 patient had a dctn1 - alk translocation ( table 1 )  . 
 case report 3 / 19 4 / 19 5 / 19 7 / 19 9 / 19 12 / 19 1 / 20 3 / 20 3w pain + bloating ; us , pet / ct : liver lesions folfirinox #2 - 6 ; dose reduction due to adverse effects ct imaging : stable disease biopsy with acquired resistance mutations ; progression on folfirinox #7 - 8 ; start lorlatinib biopsy : pancreatic adenocarcinoma ; folfirinox #1 ct imaging : stable disease ; start alectinib ct imaging : progressive disease ct imaging : stable disease inferior r hepatic lobe posterior r hepatic lobe folfirinox alectinib lorlatinib folfirinox 3 / 1 / 19 5 / 1 / 19 7 / 1 / 19 9 / 1 / 19 11 / 1 / 19 1 / 1 / 20 3 / 1 / 20 date fig 2 . 
# , dose number ; 3w , 3 - week ; ct , computed tomography ; folfirinox , uorouracil , folic acid , oxaliplatin , and irinotecan ; pet , positron emission tomography ; r , right ; us , ultrasound . and proliferative capabilities , ultimately leading to activation of different signaling pathways.28 in nsclc , alk fusion is an oncogenic driver that is generally mutually exclusive of kras mutation16 ; however , there are reports of concomitant kras and alk fusion double alteration that may confer worse prognosis.31 all 7 patients with alk - positive pancreatic cancer were kras wild type , suggesting , albeit in a small sample size , that alk translocation drives oncogenesis and that these 2 oncogenic drivers are mutually exclusive . 
this case demonstrates the rst time , to our knowledge , that alectinib has been used as the rst targeted therapy , and the development of known alectinib - resistant alk mutations suggests that alk - positive pancreatic cancer acquires resistance in a fashion similar to that of nsclc . there is a clear unmet medical need for novel therapeutic approaches in pancreatic cancer . 
a recent study in metastatic pancreatic cancer with germ - line brca mutations ( 7% prevalence ) regardless of kras mutation status showed increased pfs with the poly adp ribose polymerase inhibitor olaparib after rst - line platinum - based chemotherapy.4 in a recent phase ii basket study , 2 of 9 patients who had pancreatic cancer with her2 amplication / overexpression experienced responses to her2 - targeted therapies trastuzumab plus pertuzumab . 
additionally , a patient who had pancreatic cancer and braf gene fusion ( cux1 - braf ) had a partial response to the braf - targeted therapy vemurafenib.32 last , 3 patients who had pancreatic cancer with ntrk1 and ros1 gene fusions experienced responses to entrectinib , a targeted inhibitor of these genes.33 these studies are additional proof of concept that targeted therapies can be used successfully when paired with the right genomic alteration and that alk inhibitors may be of substantial clinical benet in the right patient . 
in row 1 , the circled hepatic lesion after disease progression on uorouracil , folic acid , oxaliplatin , and irinotecan ( a ) before lorlatinib was stable in size ( b ) 2 months after lorlatinib treatment . 
the patient currently continues to be treated with lorlatinib . 38% of kras wild - type tumors have genomic alterations that could activate the mapk signaling cascade.9 identication of molecular alterations in patients with kras wild - type status that may drive oncogenesis will help guide therapeutic intervention in a small but clinically relevant population . alk translocations are rare in pancreatic cancer . 
this is , to the rst report of ppfibp1 - alk rearour knowledge , rangement in pancreatic or nsclc , the rst reported patient with pancreatic cancer to be treated with alectinib as the rst targeted therapy , and the rst patient to be treated with lorlatinib after acquired resistance to alectinib with stabilization of disease . 
all 7 occurrences of alk - positive pancreatic cancer have been kras wild type ; given that 6 of the 7 patients were , age 50 years , there may be clinical benet to screen young patients with pancreatic cancer who are kras negative for the alk gene fusion , as they may benet from alk inhibitors , which may lead to improved overall survival . 
clinical characteristics of patients with alk - positive pancreatic cancer patient case age ( years ) alk rearrangement exon 13 eml4 - exon 20 alk ( 1 ) crizotinib ; ( 2 ) ceritinib ; ( 3 ) alectinib alk inhibitor ( in order of treatment ) ( 1 ) crizotinib ( 1 ) crizotinib unknown none ( 1 ) crizotinib ; ( 2 ) alectinib duration of survival ( months ) unknown unknown ppfibp1 - alk ( 1 ) alectinib ; ( 2 ) lorlatinib exon 6 eml4 - exon 20 alk exon 3 strn - exon 20 alk exon 6 eml4 - exon 20 alk exon 6 eml4 - exon 20 alk dctn1 - alk note . 
singhi , andrew eugene hendifar collection and assembly of data : arjan gower , barry golestany , andrew eugene hendifar data analysis and interpretation : arjan gower , jun gong , aatur d . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / authors / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . jun gong honoraria : amgen , astellas pharma , clinical congress consultants , qed therapeutics , exelixis , elsevier consulting or advisory role : amgen , astellas pharma , clinical congress consultants , qed therapeutics , exelixis , elsevier aatur d . 
singhi honoraria : foundation medicine andrew eugene hendifar consulting or advisory role : novartis , ipsen , perthera , celgene , abbvie research funding : ipsen travel , accommodations , expenses : halozyme no other potential conicts of interest were reported . references bray f , ferlay j , soerjomataram i , et al : global cancer statistics 2018 : globocan estimates of incidence and mortality worldwide for 36 cancers in 185 countries . 
ca cancer j clin 69 : 7 - 34 , 2019 conroy t , desseigne f , ychou m , et al : folfirinox versus gemcitabine for metastatic pancreatic cancer . 
n engl j med 364 : 1817 - 1825 , 2011 golan t , hammel p , reni m , et al : maintenance olaparib for germline brca - mutated metastatic pancreatic cancer . 
n engl j med 381 : 317 - 327 , 2019 von hoff dd , ervin t , arena fp , et al : increased survival in pancreatic cancer with nab - paclitaxel plus gemcitabine . 
wang - gillam a , li cp , bodoky g , et al : nanoliposomal irinotecan with uorouracil and folinic acid in metastatic pancreatic cancer after previous gemcitabinebased therapy ( napoli - 1 ) : a global , randomised , open - label , phase 3 trial . 
lancet 387 : 545 - 557 , 2016 biankin av , waddell n , kassahn ks , et al : pancreatic cancer genomes reveal aberrations in axon guidance pathway genes . 
nature 518 : 495 - 501 , 2015 singhi ad , george b , greenbowe jr , et al : real - time targeted genome prole analysis of pancreatic ductal adenocarcinomas identies genetic alterations that might be targeted with existing drugs or used as biomarkers . 
lin e , li l , guan y , et al : exon array proling detects eml4 - alk fusion in breast , colorectal , and nonsmall - cell lung cancers . 
kelly lm , barila g , liu p , et al : identication of the transforming strn - alk fusion as a potential therapeutic target in the aggressive forms of thyroid cancer . 
no e j , lovejoy a , ignatius ou , s - h , et al : alk mutation status before and after alectinib treatment in locally advanced or metastatic alk - positive nsclc : pooled analysis of two prospective trials . 
solomon bj , besse b , bauer tm , et al : lorlatinib in patients with alk - positive nonsmall - cell lung cancer : results from a global phase 2 study . 
zou hy , friboulet l , kodack dp , et al : pf - 06463922 , an alk / ros1 inhibitor , overcomes resistance to rst and second generation alk inhibitors in preclinical 27 . 
lin c , shi x , yang s , et al : comparison of alk detection by fish , ihc , and ngs to predict benet from crizotinib in advanced nonsmall - cell lung cancer . 
takeuchi k , soda m , togashi y , et al : pulmonary inammatory myobroblastic tumor expressing a novel fusion , ppfibp1 - alk : reappraisal of anti - alk immunohistochemistry as a tool for novel alk fusion identication . 
ulivi p , chiadini e , dazzi c , et al : nonsquamous , nonsmall - cell lung cancer patients who carry a double mutation of egfr , eml4 - alk or kras : frequency , clinical - pathological characteristics , and response to therapy . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecular proles : results from mypathway , an open - label , phase iia multiple basket study . 
 c clinical response to antiprogrammed death 1 after response and subsequent progression on antiprogrammed death ligand 1 therapy introduction immune checkpoint inhibitors are rapidly becoming a cornerstone in the treatment of nonsmall cell lung cancer ( nsclc )  . 
the programmed death 1 ( pd - 1 ) receptor and its two ligands , programmed death ligand 1 ( pd - l1 ; b7h1 ) and ligand 2 ( pd - l2 ; b7 - dc ) , negatively regulate t - cell activation , and expression of pd - l1 by tumor cells is an important mechanism of immune evasion.1 - 3 multiple agents have been developed to disrupt tumor - associated immune evasion by targeting either pd - 1 or pdl1 . 
nivolumab and pembrolizumab , both anti pd - 1 agents approved for advanced nsclc progressing after chemotherapy , confer an overall survival benefit and produce response rates in 16% to 23% of unselected patients with nsclc.4 - 6 food and drug administration approval was also recently extended to pembrolizumab in the first - line setting for patients with metastatic nsclc expressing pd - l1.7 atezolizumab , an antipd - l1 agent , has also demonstrated an overall survival benefit and has been approved for use in the second - line setting.8 the growing supply of treatment options has led to new questions of optimal sequencing and choice of therapy . 
in particular , the utility of serial treatment with immune checkpoint inhibitors has not been established . agents targeting pd - l1 block the interaction of pd - l1 expressed on tumor cells and tumorinfiltrating immune cells with pd - 1 and b7.1 expressed on t cells . 
studies of these agents , including atezolizumab , avelumab , and durvalumab , have demonstrated similar response rates and clinical benefit.9 - 14 although the effects of antipd - l1 are predicted to be similar to antipd - 1 , it has been speculated that the variation in mechanism may lead to distinct antitumor and toxicity profiles compared with the antipd - 1 agents.15 however , these agents have not been directly compared . 
he had been diagnosed approximately 2 years earlier with nsclc metastatic to bilateral cervical lymph nodes and bilateral adrenal glands . molecular testing showed that his tumor was egfr and kras wild type and alk translocation negative . 
before this evaluation , he received four lines of therapy , including platinum doublet chemotherapy , single - agent docetaxel , palliative chemoradiation with weekly carboplatin and paclitaxel , and erlotinib . he was enrolled in a phase i clinical trial of an antipd - l1 monoclonal antibody given in 21 - day cycles . 
he experienced only mild ( grade 1 ) rash and hypothyroidishe received a total of 16 cycles of antipd - l1 therapy before treatment was stopped per study protocol . the patient was followed with serial cross - sectional imaging and demonstrated continued pr on imaging for 16 months after therapy completion . 
after seven cycles of treatment , he was noted to have progression of disease in his right axilla and a new retropharyngeal ( rp ) mass . biopsy of the rp mass showed poorly differentiated carcinoma consistent with recurrent nsclc and similar to his initial biopsy . 
 chest , abdomen , and pelvis show a metastatic lesion within the right adrenal gland ( arrow ) before initiation of antiprogrammed death ligand 1 ( pd - l1 ) therapy ( panel a1 ) , which regressed after 16 cycles of treatment with antipd - l1 therapy ( panel a2 )  . 
repeat computed tomography imaging demonstrated progressive disease in the right adrenal gland before initiation of antipd - 1 therapy ( panel a3 ) , with subsequent improvement after 9 months of antipd1 therapy ( panel a4 )  . 
ccrt , concurrent radiotherapy ; lns , lymph nodes ; na , not available . palliative radiation therapy ( 30 gy in 10 fractions ) to both his right axilla and rp space . 
two weeks after radiation therapy , repeat imaging demonstrated stability of the rp mass , decrease in the size of the right axillary lymph node , and enlarging adrenal masses . 
imaging of the face after 6 weeks showed a pr in the rp space , and body imaging after 8 weeks of treatment showed a pr in both the right axilla and right adrenal gland ( fig 1a )  . 
he tolerated treatment well , with no immune - related adverse events for 24 cycles , after which he was noted to have progression limited to his right axilla , with a core biopsy confirming nsclc . 
unfortunately , he died several days after this procedure at an outside facility ; the cause of death was unclear . statement of informed consent all human investigations were performed after approval by a local human investigations committee and in accord with an assurance filed with and approved by the department of health and human services , and all data were anonymized to protect the identities of participants involved in the research . 
informed consent from the patient for such research was obtained . longitudinal assessment of pd - l1 and pd - l2 expression biopsy samples were obtained at the time of diagnosis ( biopsy 1 ) , before repeat treatment with antipd - l1 ( biopsy 2 ) , before treatment with anti - pd - 1 ( biopsy 3 ) , and after progression anti pd - 1 therapy ( biopsy 4 ; fig 1b )  . 
however , tissue for this first sample was extremely limited , and possible pd - l1 positivity could not be ruled out because of the size of the tissue specimen , particularly because subsequent specimens from the patient demonstrated a highly heterogeneous pattern of pd - l1 expression with rare positive stromal cells , whereas pd - l2 staining was robust throughout the tumor . 
after his initial disease progression while receiving antipd - l1 therapy , repeat biopsy demonstrated no tumor pd - l1 staining ( with limited stromal pd - l1 positivity ) , and pd - l2 remained strongly positive ( 70% ; fig 1c )  . 
similar results were demonstrated in biopsy 3 before starting pd - 1 therapy and biopsy 4 after progression on this final line of treatment , with strong pd - l2 expression in tumor , moderate pd - l1 staining in stroma , and absence of pd - l1 expression in tumor . 
representative immunohistochemistry samples from each time point are shown in figure 2 . targeted next - generation sequencing genomic testing using a hybrid capture - based next - generation sequencing platform assessing exons from 315 genes ( foundationone ) of the patients tumor at the time of progression while taking nivolumab ( biopsy 4 ) identified seven potentially functional alterations , including rictor amplification , arid1a t2030fs * 3 , arid2 q904 * , kdm5c e656 * , slit2 g498 * , tet2 e1851 * , and tp53 r280i . 
thirty - three variants of unknown significance were identified , and a total mutation burden of 53 mutations / megabase was estimated , placing this patient in the top 7% of all tumor specimens tested by this method.16 thus , the response observed in this high mutation - load patient was consistent with clinical observations.17 no alterations were identified in jak1 , jak2 , cd274 , pdcd1lg2 , pten , myc , or ctnnb1 in this patient , which were previously reported mechanisms of t - cell exclusion and / or resistance to antipd - 1 therapy.18 - 21 next - generation sequencing data were only available on the final biopsy specimen ; thus , changes in mutation burden over time cannot be assessed . gene expression analysis sufficient tissue for expression analysis ( nanostring pancancer immune profiling panel ) was available for two of the four biopsy time points : post - therapy a , which was sampled before beginning the second treatment course of antipd - l1 , and post - therapy b , sampled at disease progression on antipd - l1 , before radiation therapy followed by nivolumab . 
comparison of the expression of immune genes between these two samples demonstrated substantial downregulation of cd274 ( pd - l1 ) mrna and upregulation of several immunosuppressive genes , including il6 and ptgs2 ( cyclooxygenase - 2 ; fig 3a )  . 
it could be hypothesized that distinct immune checkpoints ( eg , pd - l1 v pd - l2 ) could divergently mediate therapeutic resistance to checkpoint inhibitors and support preclinical studies testing this hypothesis . this patients tumor was pd - l1 negative at diagnosis , with some positivity in the stroma , on the basis of our limited sample , but strongly pd - l2 positive . this finding suggests that the significance of pd - l2 positivity in response to pd - l1 or pd - 1 targeted therapies may be a useful subject of study . 
 ( a ) rna collected from archival although these studies used different clones for detection.27 , 28 using our own methods for detection of pd - l2 in a tissue microarray cohort of 43 patients with nsclc , we found that this patient was consistently among the top 5% of pd - l2 expressers . 
 tissue blocks were analyzed by nanostring pancancer immune profiling ( 730 immune - related genes )  . normalized data were compared between the post - therapy a ( preresistance ) and posttherapy b ( postresistance ) specimens for log2 fold change . 
 ( b ) genes involved in the interferon - gamma signaling reactome ( reactome.org ; accession : m965 ) were selected from the pancancer immune profiling gene set and plotted by fold change . this analysis demonstrated a general decrease in interferon - gamma signaling within the tumor microenvironment at disease progression on antiprogrammed death ligand 1 ( pd - l1 )  . 
pdl1 interacts with programmed death 1 ( pd1 ) and b7 - 1 ( cd80 ) to promote immune effector cell suppression , whereas pd - l2 can bind pd - 1 and rgmb , promoting effector suppression and respiratory tolerance in lung - resident macrophages , respectively.22 , 23 apcs , antigen - presenting cells ; cox2 , cyclooxygenase - 2 . be associated with earlier stage of disease ( stage i v all others ) , but not with gender or smoking status ( appendix fig a1 )  . during the second treatment with antipd - l1 , which was accompanied by short - term stable disease and subsequent progression , we observed maintenance of high pd - l2 expression and downregulation of pd - l1 mrna expression accompanied by simultaneous decrease of interferongamma response signatures . 
we also observed upregulation of immunosuppressive genes , such as cyclooxygenase - 2 ( recently shown to be important in mediating antipd - 1 responsiveness29 ) and interleukin - 6 , which was shown to decrease after initial treatment with pd - l1 targeted therapy.30 thus , the changes in gene expression within the tumor microenvironment in this patient were consistent with previous studies . importantly , there were multiple intervening therapies in this patient during the approximately 20month period after the initial pretreatment biopsy , limiting the inferences that can be made during the initial therapy with antipd - l1 . 
balko , leora horn manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors despite his prior treatments with palliative radiation ; however , he did receive an additional course of palliative radiation after his third biopsy and preceding his antipd - 1 therapy , and a role for radiation in sensitizing his tumor to anti - pd - 1 therapy cannot be ruled out . although anecdotal , this case report demonstrates an important clinical finding : patients who become resistant to antipd - l1 may still benefit from pd - 1 targeted therapies , possibly due to a switch from dependency on pd - l1 to pd - l2 for maintenance of immunosuppression . however , the presence of consistently high pd - l2 staining argues against a direct mechanism of pd - l2mediated de novo resistance to antipd - l1 therapy . 
moreover , pd - l2 mrna did not seem to be upregulated or changed during acquisition of resistance to antipd - l1 therapy . however , the ratio of pd - l2 to pd - l1 mrna increased substantially from 3.6 - fold to 14.6 - fold during this period and may be a useful metric to test experimentally in the future for association with resistance to antipd - l1 treatment . 
although more investigation is needed in the context of preclinical studies and clinical trials , this report supports investigations of sequencing antipd - l1 and antipd - 1 therapies to elucidate mechanisms of cross - resistance and derive maximal patient benefit from these agents . 
johnson consulting or advisory role : bristol - myers squibb , genoptix , merck research funding : incyte patents , royalties , other intellectual property : intellectual property and patents pending surrounding use of mhc - ii and response to immune therapy leora horn honoraria : biodesix consulting or advisory role : bristol - myers squibb , merck , bayer , xcovery , genentech , boehringer ingelheim , eli lilly , abbvie , astrazeneca research funding : astrazeneca ( inst ) other relationship : bristol - myers squibb justin m . 
balko research funding : incyte patents , royalties , other intellectual property : patent on use of hla - dr / mhc expression to predict response to immunotherapies references 677 - 704 , 2008 1 . 
mu cy , huang ja , chen y , et al : high expression of pd - l1 in lung cancer may contribute to poor prognosis and tumor cells immune escape through suppressing tumor infiltrating dendritic cells maturation . 
borghaei h , paz - ares l , horn l , et al : nivolumab versus docetaxel in advanced nonsquamous nonsmall - cell lung 2018 - 2028 , 2015 cancer . 
rittmeyer a , barlesi f , waterkamp d , et al : atezolizumab versus docetaxel in patients with previously treated nonsmall - cell lung cancer ( oak ) : a phase 3 , open - label , multicentre randomised controlled trial . 
brahmer jr , tykodi ss , chow lq , et al : safety and activity of anti - pd - l1 antibody in patients with advanced cancer . n engl j med 366 : 2455 - 2465 , 2012 10 . 
brahmer jr , rizvi na , luzky j , et al : clinical activity and biomarkers of medi4736 , an anti - pd - l1 antibody , in patients with nsclc . 
rizvi n , brahmer j , ignatius s , et al : safety and clinical activity of medi4736 , an anti - programmed cell death - ligand 1 ( pd - l1 ) antibody , in patients with nonsmall - cell lung cancer ( nsclc )  . 
spira ai , park k , mazi`eres j , et al : efficacy , safety and predictive biomarker results from a randomized phase ii study comparing mpdl3280a vs docetaxel in 2l / 3l nsclc ( poplar )  . 
spigel dr , chaft je , gettinger sn , et al : clinical activity and safety from a phase ii study ( fir ) of mpdl3280a ( antipdl1 ) in pd - l1selected patients with nonsmall - cell lung cancer ( nsclc )  . 
kelly k , patel mr , infante jr , et al : avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in patients with metastatic or locally advanced solid tumors : assessment of safety and tolerability in a phase i , open - label expansion study . 
xiao y , yu s , zhu b , et al : rgmb is a novel binding partner for pd - l2 and its engagement with pd - l2 promotes respiratory tolerance . 
he j , hu y , hu m , et al : development of pd - 1 / pd - l1 pathway in tumor immune microenvironment and treatment for nonsmall - cell lung cancer . 
yearley j , gibson c , yu n , et al : pd - l2 expression in human tumors : relevance to anti - pd - 1 therapy in cancer . presented at european society for medical oncology annual meeting , vienna , austria , september 25 - 29 , 2015 27 . 
calles a , liao x , sholl lm , et al : expression of pd - 1 and its ligands , pd - l1 and pd - l2 , in smokers and never smokers with kras - mutant lung cancer . 
kim my , koh j , kim s , et al : clinicopathological analysis of pd - l1 and pd - l2 expression in pulmonary squamous cell carcinoma : comparison with tumor - infiltrating t cells and the status of oncogenic drivers . 
postow ma , callahan mk , barker ca , et al : immunologic correlates of the abscopal effect in a patient with melanoma . 2035 - 2036 , 2012 n engl j med 366 : 925 - 931 , 2012 34 . 
programmed death ligand 2 ( pd - l2 ) expression across 43 patients with nonsmall cell lung cancer ( nsclc )  . ( a ) a tissue microarray series of 43 patients with nsclc was stained for pd - l2 expression and analyzed by histoscore ( h - score ; % of cells staining positive 3 intensity [ 0 - 3 + ] )  . 
laetsch author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license clinical trial information : nct02637687 . corresponding author : theodore w . 
in normal development , these genes regulate the growth , differentiation , and survival of neurons.14 , 15 gene fusions that involve one of these genes ( trk fusions ) have been described in a range of pediatric and adult cancers.16 - 25 in these fusions , the 3 region of the ntrk gene , which includes the kinase domain , is joined downstream of the promoter and 5 region of an unrelated gene . 
most reported fusions in extra cranial solid tumors to date have involved either ntrk1 or ntrk3 , with ntrk2 fusions more common in primary cns tumors.26 larotrectinib is the first highly selective inhibitor of all three trk kinases to enter clinical development . 
after two cycles of chemotherapy , disease progression continued , and an aortic pseudo aneurysm developed within the mass , which led to displacement of the inferior vena cava and ureteral impingement ( fig 1b )  . 
 ( e ) after 14 months of larotrectinib treatment . the patient was subsequently referred to our institution , where surgical intervention to debulk the tumor and repair the pseudo - aneurysm was offered . 
histologically , the tumor consisted of sheets of epithelioid cells with large eccentrically placed nucleus , occasional nucleoli , and abundant eosinophilic cytoplasm , mimicking rhabdoid cells ( fig 3 )  . 
immunohistochemically , the cells showed retained ini - 1 nuclear positivity and scattered cells positive for s - 100 protein and cd34 . postoperatively , gross residual tumor remained in the vertebral bodies . 
next generation sequencing ( ngs ) of her tumor was performed using foundationoneheme ( foundation medicine , cambridge , ma ) , a combined dna and rna sequencing hybrid capture - based assay that has been validated for clinical use without requirement for an orthogonal confirmatory assay.28 sequencing revealed a novel strn - ntrk2 fusion in which the kinase domain of ntrk2 is joined in frame to strn ( figs 3e and 3f )  . 
copy number loss of cdkn2b also was identified . two months after surgery , after informed consent , the patient was enrolled in the pediatric phase i trial of larotrectinib.29 she was treated with dose level 1 ( 100 - mg adult equivalent dose by simcyp modeling [ simcyp , sheffield , uk ] ) and received larotrectinib 75 mg twice a day continuously on the basis of her age and body surface area . 
pharmacokinetic assessment after the first dose of larotrectinib revealed an estimated 24 - hour area under the plasma concentration time curve ( auc0 - 24 ) of 2 , 980 ng h / ml , which was less than the protocol - specified threshold of 3 , 500 ng h / ml that would allow intrapatient dose escalation . 
pharmacokinetics at this dose demonstrated an estimated auc0 - 24 of 3 , 830 ng h / ml . at the time of initiation of larotrectinib , the patients lansky play - performance score ( lps ) was 60 . 
by 14 days after initiation of larotrectinib , the patient was noticeably less fatigued ( lps of 70 ) , the ascites had resolved by physical examination , and her back pain had resolved ( fig 4 )  . 
 ( d ) excised tumor specimen , including the aortic bifurcation . ureter position of vertebral bodies 2 , demonstrated resolution of pet avidity of all tumors , resolution of ascites , and significant reduction in the size of the residual pulmonary metastases and retroperitoneal tumors consistent with a partial response by response evaluation criteria in solid tumors ( recist ) version 1.1 ( figs 1d and 1e )  . 
five months after starting larotrectinib , the patient underwent uncomplicated closure of her colostomy and removal of her denver shunt . despite heavy pretreatment , the patient has tolerated larotrectinib well , with the only drug related adverse events consisting of mild ( common terminology criteria for adverse events [ version 4 ] grade 1 ) fatigue and intermittent grade 1 to 2 cytopenias . 
her response continues to deepen with complete resolution of her pulmonary metastasis and only residual pet - negative tissue at the site of tumor invasion of the vertebral bodies after 22 months of larotrectinib therapy as of february 2018 . 
 currently , the patients lps is 90 , and she has returned to school . discussion we describe a patient in whom tumor sequencing led to the identification of a novel ntrk2 fusion in a chemotherapy - refractory , metastatic , unresectable , undifferentiated sarcoma and successful treatment with larotrectinib . 
the identification of an ntrk2 fusion is consistent with other reports of oncogenic fusions in this histology.13 , 30 - 39 a wide range of tumors that harbor trk fusions has been reported to respond to larotrectinib.27 the activity of larotrectinib is striking in children , with a 93% confirmed objective response rate and all patients with trk fusions experiencing tumor regression.29 this patients tumor harbored a fusion of ntrk2 , and she was the sole patient in the initial 55 - patient data set to have a fusion of this gene.27 other rare ntrk2 fusions have been described in gliomas , specifically with vcl , agbl4 , qki , and nacc2 , 20 , 40 but to our knowledge , this report is the first of an ntrk2 fusion in a pediatric extracranial solid tumor . 
 ( b ) hematoxylin and eosin stain that shows epithelioid / rhabdoid cells with eccentric , pleomorphic nuclei ; occasional nucleoli and abundant eosinophilic cytoplasm ; and a single mitosis . 
 ( f ) rna sequencing reads that support the strn - ntrk2 fusion . ntrk3 suggests that these sarcomas should be evaluated for fusions of all three ntrk genes.41 strn on chromosome 2p22.2 encodes striatin , a ubiquitously expressed calmodulin - binding protein thyroid cancer , it is a common 5 fusion partner for alk also located on 2p.42 however , strn has not previously been reported as an ntrk fusion partner , which is consistent with the broad diversity of 5 fusion partners seen in trk fusion - positive cancers27 and is an important consideration when designing testing strategies for trk fusions . 
tests such as reverse transcriptase polymerase chain reaction only detect known fusion partners and are likely to miss tumors with uncommon or unique ntrk fusion genes , which can respond to trk inhibition . 
testing that uses hybrid capturebased ngs has the potential to detect a diversity of ntrk fusion partners , but careful attention must be paid to the initial substrate ( dna v rna ) , the target enrichment strategy ( hybrid capture v amplicon v anchored multiplex polymerase chain reaction ) , and the detailed probe design . the profound clinical response seen in this strn - ntrk2 fusion patient to larotrectinib establishes that the trk fusion is the key driver for this patients tumor . 
in the latter , despite high initial response rates , nearly all patients treated with vemurafenib or dabrafenib experience disease progression within 12 to 18 months of starting therapy.43 , 44 durable responses also have been observed in patients with fusions that involve ntrk1 and ntrk3 treated with larotrectinib.27 in conclusion , ngs of the undifferentiated sarcoma in our patient was critical in identifying a highly actionable kinase fusion ( strn - ntrk2 ) , which resulted in a profound and durable clinical response on matched treatment . 
laetsch manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors veena rajaram no relationship to disclose dean c . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center lee a . 
cox employment : bayer ag , loxo oncology , merck , amgen stock and other ownership interests : loxo oncology , bayer ag , merck , amgen patents , royalties , other intellectual property : us patent 62 / 318 , 041 issued to loxo oncology ( inst ) theodore w . 
laetsch , the university of texas southwestern medical center ; tara pavlock , alison patterson , anne post , caitlyn ambrose , veena rajaram , andrew martin , steve megison , and theodore w . 
ferrari a , sultan i , huang tt , et al : soft tissue sarcoma across the age spectrum : a populationbased study from the surveillance epidemiology and end results database . 
pappo as , devidas m , jenkins j , et al : phase ii trial of neoadjuvant vincristine , ifosfamide , and doxorubicin with granulocyte colony - stimulating factor support in children and adolescents with advanced - stage nonrhabdomyosarcomatous soft tissue sarcomas : a pediatric oncology group study . 
antonescu cr , suurmeijer aj , zhang l , et al : molecular characterization of inflammatory myofibroblastic tumors with frequent alk and ros1 gene fusions and rare novel ret rearrangement . 
simon mp , pedeutour f , sirvent n , et al : deregulation of the platelet - derived growth factor b - chain gene via fusion with collagen gene col1a1 in dermatofibrosarcoma protuberans and giant - cell fibroblastoma . 
moss yp , voss sd , lim ms , et al : targeting alk with crizotinib in pediatric anaplastic large cell lymphoma and inflammatory myofibroblastic tumor : a childrens oncology group study . 
laetsch tw , roy a , xu l , et al : undifferentiated sarcomas in children harbor clinically - relevant oncogenic fusions and gene copy - number alterations : a report from the childrens oncology group . 
bourgeois jm , knezevich sr , mathers ja , et al : molecular detection of the etv6 - ntrk3 gene fusion differentiates congenital fibrosarcoma from other childhood spindle cell tumors . 
knezevich sr , garnett mj , pysher tj , et al : etv6 - ntrk3 gene fusions and trisomy 11 establish a histogenetic link between mesoblastic nephroma and congenital fibrosarcoma . 
el demellawy d , cundiff ca , nasr a , et al : congenital mesoblastic nephroma : a study of 19 cases using immunohistochemistry and etv6 - ntrk3 fusion gene rearrangement . 
laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
italiano a , sung ys , zhang l , et al : high prevalence of cic fusion with double - homeobox ( dux4 ) transcription factors in ewsr1 - negative undifferentiated small blue round cell sarcomas . 
yamada y , kuda m , kohashi k , et al : histological and immunohistochemical characteristics of undifferentiated small round cell sarcomas associated with cic - dux4 and bcor - ccnb3 fusion genes . 
li ws , liao ic , wen mc , et al : bcor - ccnb3 - positive soft tissue sarcoma with round - cell and spindle - cell histology : a series of four cases highlighting the pitfall of mimicking poorly differentiated synovial sarcoma . 
omeara e , stack d , phelan s , et al : identification of an mll4 - gps2 fusion as an oncogenic driver of undifferentiated spindle cell sarcoma in a child . 
kao yc , sung ys , zhang l , et al : recurrent bcor internal tandem duplication and ywhaenutm2b fusions in soft tissue undifferentiated round cell sarcoma of infancy : overlapping genetic features with clear cell sarcoma of kidney . 
sugita s , arai y , aoyama t , et al : nutm2a - cic fusion small round cell sarcoma : a genetically distinct variant of cic - rearranged sarcoma . 
kelly lm , barila g , liu p , et al : identification of the transforming strn - alk fusion as a potential therapeutic target in the aggressive forms of thyroid cancer . 
hauschild a , grob jj , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
 o tmprss2 - erg fusions unexpectedly identified in men initially diagnosed with nonprostatic malignancies purpose tmprss2 - erg gene fusions are frequently found in prostate cancer and are pathognomonic for prostatic origin a series of cancer cases assayed with comprehensive genomic profiling ( cgp ) in the course of clinical care , we reviewed the frequency of tmprss2 - erg fusions in patient tumors of various histologic subtypes . methods frequency of tmprss2 - erg fusions was determined in cgps from 64 , 263 cancer cases submitted to foundation medicine to assess genomic alterations suggesting benefit from targeted therapy . 
genomic results are presented from an index case of prostate cancer that underwent evolution from adenocarcinoma to pure squamous cell carcinoma . results tmprss2 - erg fusions were identified for 0.86% of male patients ( 250 of 29 , 030 ) and not found for female patients ( none of 35 , 233 )  . 
the index case is a patient with a large , left retrovesical mass diagnosed as squamous carcinoma by morphologic examination and a history of gleason score 9 prostate cancer with prior prostatectomy and salvage radiation therapy . 
a phylogenetic tree demonstrating clonal and histopathologic evolution of prostate cancer in the index patient was constructed . conclusion in this large cgp dataset , tmprss2 - erg fusion was seen in approximately 30% of prostate cancers regardless of histologic type ; on occasion , the fusion was detected in advanced cancers not initially carrying a diagnosis of prostate carcinoma . 
2017 by american society of clinical oncology introduction chromosomal translocations involving tmprss2 , an androgen - regulated gene encoding a transmembrane serine protease , and members of the ets transcription factor family including erg are frequently observed in prostate cancer.1 specifically , tmprss2 - erg fusions occur in approximately half of all prostate cancers and are believed to be a critical player in prostate carcinogenesis.2 tmprss2 - erg is involved in the promotion of cell migration , invasion , and tumor progression.1 , 3 the prognostic and predictive value of tmprss2erg fusions is still under active investigation ; however , some studies have suggested an association of the fusion gene with higher recurrence risk and possibly even increased risk of prostate cancerrelated death.4 - 6 clinically , tmprss2 - erg fusions can be detected in formalin - fixed paraffin - embedded tumor specimens through comprehensive genomic profiling ( cgp ) assays that use next - generation sequencing technology . 
the wide availability of this technology enables practicing clinicians to readily ascertain the presence of gene fusion events , such as those between tmprss2 and erg , in patient tumors . 
however , the presence of this fusion in a case where prostate cancer was not the diagnosis may dramatically alter the therapeutic approach . here , we review a large database of patients with advanced cancers who underwent cgp in the course of clinical care to ascertain the frequency of tmprss2 - erg in both prostate cancer and in patients with diagnoses of nonprostate cancer . 
an index case was identified to highlight the clinical impact of this approach . methods the methods used for this analysis have been previously described.7 in brief , formalin - fixed , paraffin - embedded slides or blocks from tumor samples were subjected to cgp in a clinical laboratory improvement amendmentscertified , college of american pathologistsaccredited , new york stateregulated reference laboratory ( foundation medicine )  . 
60 , 000 cancer cases submitted to foundation medicine by december 31 , 2015 , were used to determine the frequency of tmprss2 - erg fusions across histologic subtypes . genomic profiles for an index case of prostate cancer with histologic evolution from prostatic adenocarcinoma to pure squamous cell carcinoma were identified and described . 
an evolutionary tree was inferred using the neighbor - joining method , with the branch lengths being proportional to the number of genomic alterations acquired on the corresponding branch.8 the evolutionary analysis was conducted in mega7 ( net / home ) .9 approval for this study , including a waiver of informed consent and a health insurance portability and accountability act waiver of authorization , was obtained from the western institutional review board ( protocol no . 20152817 ) results the tmprss2 - erg fusion gene was detected exclusively in tumor samples obtained from male patients . 
other tumor types , for which tmprss2 - erg was not found , accounted for most of the samples ( n = 59 , 114 ) in the overall dataset ( table 2 )  . 
in the 2 , 139 patients with carcinoma of unknown primary , 28 ( 1.3% ) had tmprss2erg identified in their tumors and six of those were of the squamous cell subtype . 
he was noted to have a stage pt2 n0 mx tumor ; final histopathologic analysis identified his tumor to be of higher grade ( gleason score 9 [ 4 + 5 ] )  . 
by november 2009 , the patient was found to have a persistently detectable prostate - specific antigen ( psa ) level of 0.2 ng / ml , which increased to 0.3 ng / ml by january 2010 . 
the patient subsequently underwent salvage external beam radiation tomotherapy ( 64.8 gy 3 36 fractions ) to the prostatic fossa . despite radiation , his psa level continued to slowly rise over the next few years . in june 2011 , the patient underwent a liver biopsy for a slowly enlarging liver nodule that had been observed over the past 6 years . 
to palliate urinary and rectal obstruction from the enlarging pelvic mass , the patient underwent radical cystectomy with ileal conduit urinary diversion , low anterior resection with diverting colostomy , and small - bowel resection in september 2015 . 
tumor types for samples in the dataset ( n = 59 , 114 ) percentage of all samples tumor type lung adenocarcinoma colon adenocarcinoma breast invasive ductal carcinoma breast carcinoma ( nos ) unknown primary adenocarcinoma brain glioblastoma lung non - small cell lung carcinoma ( nos ) pancreas ductal adenocarcinoma ovary serous carcinoma lung squamous cell carcinoma abbreviation : nos , not otherwise specified . pelvic mass was confirmed to be pure squamous cell cancer . 
all three carcinoma specimens shared the tmprss2 - erg fusion , loss of pten exons 5 through 9 , the tp53 missense mutation v147g , and variants of unknown significance in the genes pdgfrb ( r177c ) and prkdc ( s1660y )  . 
in addition , the primary prostatic adenocarcinoma tumor ( june 2009 ) carried high - level amplifications of the genes foxp1 and tbx3 , whereas the squamous cell carcinoma specimen ( july 2015 ) and the prostatic adenocarcinoma metastasis ( september 2015 ) , which were both from the bladder , had homozygous loss of the adjacent genes cdkn2a and cdkn2b in common . 
the adenocarcinoma metastasis also harbored a subclonal nfe2l2 mutation ( w8c ) , and the squamous cell carcinoma carried a distinct variant of unknown significance ( cic g133c )  . 
no reportable genomic alterations were identified in the benign carcinoid specimen ; all its variants were of unknown significance , shared with the other specimens , and had variant allele frequencies consistent with germline status . 
in summary , comprehensive genomic analysis identified truncal prostatic adenocarcinoma drivers in the squamous cell carcinoma , including the unexpected tmprss2 - erg fusion event , and thus indicated that the squamous cell carcinoma had arisen from a prostatic adenocarcinoma . discussion prostate cancer is a highly heterogeneous malignancy on the genomic level . 
nevertheless , morphologic evaluation of prostate cancer overwhelmingly identifies this tumor type to be adenocarcinoma , albeit of varying grades within the same tumor ( intrapatient ) or across different patients tumors ( interpatient )  . 
here , we have reported an index case of prostate cancer with variant histology , specifically squamous cell carcinoma that was realized by the identification of tmprss2erg fusion in both the squamous ( divergent histology ) and in the primary prostatic adenocarcinoma specimen . 
histopathologic sections of the index patients tumors . ( a ) micrographs of hematoxylinand - eosin stained typical carcinoid biopsy specimen and the corresponding synaptophysin stain . ( b ) micrographs of representative sections of the patients metachronous squamous cell cancer in a metastatic pelvic mass . ( c ) metastatic prostatic adenocarcinoma obtained from a regional lymph node . 
 ( d ) metastatic prostatic adenocarcinoma adherent to small bowel . we observed tmprss2 - erg fusions in approximately 30% of prostate cancers , which were predominantly adenocarcinoma , but the frequency of fusion - positive cases held true across histologic prostate tumor types . 
tmprss2 - erg fusion was also detected in patients with advanced cancer who had a diagnosis of nonprostate tumors as defined by the treating teain addition to the index case of squamous carcinoma presented in this report , five additional patients who had squamous cell cancer were found to harbor tmprss2 - erg , a finding with likely therapeutic implications . 
in the absence of genomic information , a histologic phenotype not known to be associated with prostate cancer , such as squamous cell carcinoma , would trigger a different treatment algorithm , such as cytotoxic platinum - based chemotherapy . 
 squamous cell carcinoma ( pelvic mass ) cic g133c nfe2l1 w8c cdkn2a / b loss adenocarcinoma ( metastatic deposit ) adenocarcinoma , prostate ( primary tumor ) foxp1 amplification tbx3 amplification tmprss2 - erg fusion pten loss exons 5 - 9 tp53 v147g prkdc s1660y pdgfrb r177c carcinoid , liver ( benign specimen ) fig 2 . 
the evolutionary tree was inferred using the neighbor - joining method , 8 with the branch lengths being proportional to the number of genomic alterations acquired on the corresponding branch . evolutionary analyses were conducted in mega7.9 xenograft mouse models of tmprss - erg expression nonadenocarcinoma . primary squamous cell carcinoma of the prostate has been reported in the literature , but it is exceedingly rare.11 such cases may represent transformation of a prostatic adenocarcinoma primary , as in this index case . 
lara jr honoraria : pfizer consulting or advisory role : exelixis , pfizer , novartis , astrazeneca , bayer , roche , celgene , janssen , bristol - myers squibb , abbvie , turnstone bio research funding : millennium ( inst ) , polaris ( inst ) , glaxosmithkline ( inst ) , genentech ( inst ) , aragon established the correct clinical diagnosis and later revealed the pattern of clonal evolution and selection . most importantly , the finding of tmprss2 - erg in the squamous cell tumor provided support for the use of androgen deprivation therapy for the patient . there are important limitations to this analysis . our report focuses solely on tmprss2 - erg fusions . 
although this event represents the vast majority of ets rearrangements , tmprss2 can be rearranged with other biologically relevant partner genes that were not specifically studied here and that could be similarly pathognomonic for a prostatic origin of advanced cancer in men . 
elvin employment : foundation medicine stock and other ownership interests : foundation medicine mamta parikh no relationship to disclose ralph de vere white stock and other ownership interests : pfizer regina gandour - edwards no relationship to disclose christopher p . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan - kettering cancer center siraj m . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome in non - neoplastic disease ( i ) primo n . 
p30 ca093373 to the university of california davis comprehensive cancer center . presented in part at the asco annual meeting , chicago , il , june 3 - 7 , 2016 . affiliations support prior presentation references 1 . 
wirth , md1 ; takashi kohno , phd2 ; hibiki udagawa , md , phd3 ; shingo matsumoto , md , phd3 ; genichiro ishii , md , phd3 ; kevin ebata , phd4 ; brian b . 
michael rothenberg , md , phd4 ; and koichi goto , md , phd3 introduction the ret receptor tyrosine kinase is oncogenically activated by ret gene fusions in 1% to 2% of nonsmall - cell lung cancers ( nsclc ) and by ret gene mutations in most medullary thyroid cancers ( mtc ) .1 although multikinase inhibitors ( mkis ) with nonspecic anti - ret activity are approved for the treatment of mtc irrespective of ret mutation status , their investigational use for patients with ret fusion - positive nsclc has been limited by substantial off - target adverse effects that lead to dose reductions and inadequate ret - specic inhibition.2 - 7 as a result , tumor responses to mkis have been infrequent and short lived , and a comprehensive molecular understanding of mki response and resistance is lacking . in contrast to the mkis , loxo - 292 is a highly selective , small molecule ret tyrosine kinase inhibitor ( tki ) with nanomolar potency against diverse ret alterations , favorable pharmacokinetic ( pk ) properties , and signicant cns penetration.8 in an ongoing , phase i / ii identier : study of loxo - 292 ( clinicaltrials.gov nct03157128 ) , conrmed partial responses ( prs ) were achieved in most ret - altered patients across different tumor histologies and diverse ret gene fusions and mutations . 
a 42 - yearold woman with nsclc had received nine prior systemic therapy regimens , including approved chemotherapy , immunotherapy , and investigational tkis , before the identication of a kif5b - ret fusion in a sample from a recurrent pleural fusion ( fig 1a , data supplement )  . 
she received alectinib and additional chemotherapy and then vandetanib ( fig 1a ) .6 she experienced a conrmed pr by response evaluation criteria in solid tumors ( recist ) 1.1 with vandetanib treatment , with improvement in multiple lung and pleural - based lesions . 
targeted ret gene sequencing of a biopsy specimen from a progressing right lung lesion identied a ret valine - to - leucine ( v804l ) gatekeeper mutation absent from a pretreatment tumor sample ( fig 1a , data supplement )  . v804l allele frequency in the progression sample was 15% by next - generation sequencing ( 120 of 799 reads ) compared with 0% in the pretreatment sample ( 0 of 847 reads ; data supplement )  . the patient received additional systemic chemotherapy with pemetrexed and amrubicin but experienced continued disease progression . 
after providing written informed consent , she started treatment with loxo292 in the phase i portion of the phase i / ii clinical trial at the recommended phase ii dose of 160 mg twice a day . 
 ( a ) various treatments the patient received for metastatic , kif5b - ret fusion - positive nonsmall - cell lung cancer are shown , together with the levels of carcinoembryonic antigen ( cea ; red diamonds ) and the sum of target lesions by response evaluation criteria in solid tumors ( recist ) 1.1 ( blue squares ) over time during treatment . 
the estimated levels of ret target inhibition at the 50% inhibitory concentration ( ic50 ) and 90% inhibitory concentration ( ic90 ) for kif5b - ret and kif5b - ret - v804l were modeled using actual patient human pharmacokinetic parameters ( data supplement )  . 
 ( c ) computed tomographic images of the patients metastatic lung and liver disease before and at the indicated times after initiating treatment with vandetanib ( left three pairs of panels ) or loxo - 292 ( right two pairs of panels )  . 
consistent with this , she experienced a rapid clinical and biochemical response to loxo - 292 , with decreased shortness of breath and reduction in serum carcinoembryonic antigen ( fig 1a )  . repeat imaging after 8 weeks of treatment demonstrated a 48% decrease in measurable tumor burden by recist 1.1 that was maintained after 16 weeks , indicating a conrmed pr ( figs 1a and 1c )  . 
the patient has received loxo - 292 for more than 11 months , is still receiving treatment , and is tolerating therapy well , without dose interruption , and with all treatment - emergent adverse events grade 1 or 2 . case 2 : hereditary ret v804m mtc . 
a 50 - year - old man with hereditary ret v804m multiple endocrine neoplasia 2a and mtc developed primary disease progression despite previous treatment with three anti - ret mkis ( fig 2a )  . before treatment with loxo - 292 , he was highly symptomatic , with abdominal pain from tumor inltration of the liver and severe tumor - related diarrhea . 
consistent with this , serum carcinoembryonic antigen and calcitonin levels decreased rapidly , together with resolution of diarrhea , abdominal distension , and abdominal parepeat imaging after 8 weeks of treatment indicated a complete response by recist 1.1 , which was conrmed after 12 weeks of treatment , with complete resolution of target lymph node lesions and nontarget liver memediastinal tastases and normalization of serum tumor markers ( figs 2c and 2d )  . 
the patients dose was increased to 160 mg twice a day as allowed by the protocol , with doseproportional increases in exposure and continuous more than ic90 ret v804m target coverage ( fig 2b ) , continued complete response , and continued normalization of tumor markers ( fig 2c )  . 
the patient experienced three adverse events : transient grade 3 altered mental status ( sedation ) , judged by the investigator to be related to concomitant treatment with anxiolytic medications and unrelated to loxo - 292 ; grade 1 constipation ; and grade 2 nausea . 
he remains in complete response and is still receiving treatment at more than 20 months after the start of loxo - 292 . loxo - 292 but not anti - ret mkis maintain inhibitory activity against ret gatekeeper mutations preclinically . 
in contrast to mkis , loxo - 292 is predicted to better accommodate the bulky leucine and methionine side chains in the gatekeeper residues without any steric interactions ( fig 3b )  . to determine the impact of ret kinase domain resistance mutations on inhibitor activity , loxo - 292 , vandetanib , and cabozantinib were tested in vitro against the puried wildtype and mutant ret kinase domains ( fig 3c )  . 
at physiologic ( 1 mm ) atp concentration , loxo - 292 had potent inhibitory activity against wild - type ret , ret v804l , and ret v804m kinases . the anti - ret mkis , in contrast , vandetanib and cabozantinib , displayed signicantly reduced activity against ret v804l / m compared with wildtype ret . 
these data demonstrate that loxo - 292 , but not the mkis vandetanib or cabozantinib , maintain potent inhibitory activity against ret gatekeeper mutations . discussion selective tkis targeting actionable kinase alterations have transformed the treatment landscape for several human cancers . 
although acquired resistance to tkis is universal , a detailed molecular understanding of resistance has led to the development of next - generation tkis that have extended disease control and clinical benet in resistant patients.16 , 17 in several instances , initial treatment with the next - generation inhibitor has led to more durable treatment responses than treatment with the rstgeneration tki and has become standard upfront systemic therapy.18 , 19 loxo - 292 combines features of both rstand nextgeneration tkis used to treat other single kinase - driven cancers . 
it is highly potent against and selective for diverse founder activating ret alterations in human cancers , and in preclinical experiments , it overcomes ret v804 gatekeeper mutations , which have been identied in rare patients with acquired resistance to anti - ret mkis . 
for both patients , inhibiintegration of preclinical ret target tory activity with the actual exposures safely achieved at the recommended phase ii dose of 160 mg twice a day allowed more than ic90 calculated target coverage of both wild - type and gatekeeper - mutated ret in patients ( figs 1b and 2b )  . 
 ( b ) pharmacokinetic analysis at steady state after 8 days of treatment with loxo - 292 at a dose of 80 mg , 120 mg , and 160 mg twice a day . 
the estimated levels of ret target inhibition at the 50% inhibitory concentration ( ic50 ) and 90% inhibitory concentration ( ic90 ) for wild - type ( wt ) ret and ret v804m were modeled as in fig 1b . 
the red arrows indicate diffuse inltration of the liver by tumor . lenvat , lenvatinib ; rt , radiation treatment ; vande , vandetanib . treatment with loxo - 292 after the prior mkis has signicantly extended the period of durable clinical and biochemical response and disease control . 
 wirth et al hibiki udagawa honoraria : astrazeneca , chugai pharmaceutical , bristol - myers squibb , ono pharmaceutical , msd , taiho pharmaceutical , amco , abbvie , boehringer ingelheim , daiichi sankyo consulting or advisory role : abbvie , boehringer ingelheim research funding : msd , abbvie , daiichi sankyo , amgen shingo matsumoto honoraria : pzer , novartis , chugai pharma , astrazeneca research funding : chugai pharma ( inst ) , novartis ( inst ) , lilly ( inst ) , merck serono ( inst ) , merck sharp & dohme ( inst ) kevin ebata employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology brian b . 
tuch employment : loxo oncology stock and other ownership interests : loxo oncology consulting or advisory role : kezar life sciences patents , royalties , other intellectual property : biomarkers for ntrk inhibition ; biomarkers for proteasome inhibition edward y . 
zhu employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology michele nguyen employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology steve smith consulting or advisory role : loxo oncology , various patents , royalties , other intellectual property : various patents and applications travel , accommodations , expenses : various lauren m . 
burkard employment : array biopharma , university of colorado hospital ( i ) stock and other ownership interests : array biopharma , pzer , pzer ( i ) james f . 
blake employment : array biopharma stock and other ownership interests : array biopharma patents , royalties , other intellectual property : i am listed as a co - author on approximately 46 patents ( inst ) kevin r . 
brandhuber employment : loxo oncology stock and other ownership interests : loxo oncology , array biopharma travel , accommodations , expenses : loxo oncology steve andrews employment : loxo oncology leadership : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology s . 
michael rothenberg employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology koichi goto honoraria : bristol - myers squibb , astrazeneca , pzer , chugai pharmaceutical , taiho pharmaceutical , ono pharmaceutical , novartis , eli lilly , boehringer ingelheim , quintiles , merck serono , life technologies , msd , abbvie , riken genesis , nippon kayaku , takeda pharmaceuticals , otsuka pharmaceutical , srl diagnostics consulting or advisory role : otsuka pharmaceutical research funding : msd , astrazeneca , taiho pharmaceutical , chugai pharmaceutical , boehringer ingelheim , ono pharmaceutical , sumitomo dainippon , takeda pharmaceuticals , novartis , daiichi sankyo , kyowa hakko kirin , astellas pharma , eisai , eli lilly , pzer , riken genesis , bristol - myers squibb , merck serono , ignyta , life technologies , research triangle institute d / b / a rti health solutions , janssen , xcoo , loxo oncology no other potential conicts of interest were reported . references ji jh , oh yl , hong m , et al : identication of driving alk fusion genes and genomic landscape of medullary thyroid cancer . 
wells sa jr , robinson bg , gagel rf , et al : vandetanib in patients with locally advanced or metastatic medullary thyroid cancer : a randomized , double - blind phase iii trial . 
j clin oncol 30 : 134 - 141 , 2012 drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 2 , single - arm trial . 
lancet oncol 17 : 1653 - 1660 , 2016 lin jj , kennedy e , sequist lv , et al : clinical activity of alectinib in advanced ret - rearranged non - small cell lung cancer . 
j thorac oncol 11 : 2027 - 2032 , 2016 yoh k , seto t , satouchi m , et al : vandetanib in patients with previously treated ret - rearranged advanced non - small - cell lung cancer ( luret ) : an open - label , multicentre phase 2 trial . 
lancet respir med , 5 : 42 - 50 , 2017 lee sh , lee jk , ahn mj , et al : vandetanib in pretreated patients with advanced non - small cell lung cancer - harboring ret rearrangement : a phase ii clinical trial . 
ann oncol 28 : 292 - 297 , 2017 brandhuber bb , haas j , tuch bb , et al : ena - 0490 the development of loxo - 292 , a potent , kdr / vegfr2 - sparing ret kinase inhibitor for treating patients with ret - dependent cancers . 
aacr - nci - eortc international conference on molecular targets and cancer therapeutics , munich , germany , november 29 - december 2 , 2016 oxnard gr , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer : an update from asco 2018 . 
wirth lj , cabanillas me , sherman ej , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret - altered thyroid cancers : an update from asco 2018 . 
drilon ae , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
yang , m , cai j , guo s , et al : rapid conversion to resistance , of a colon pdw with ret - fusion , by ponatinib treatment could potentially be attributed to the introduction of the gate keeper mutation , v804m . 
dagogo - jack i , stevens se , lin jj , et al : emergence of a ret v804m gatekeeper mutation during treatment with vandetanib in ret - rearranged nsclc . j thorac oncol 13 : e226 - e227 , 2018 15 . 
nat commun 9 : 625 , 2018 j anne pa , yang jc , kim dw , et al : azd9291 in egfr inhibitor - resistant non - small - cell lung cancer . 
ou sh , ahn js , de petris l , et al : alectinib in crizotinib - refractory alk - rearranged non - small - cell lung cancer : a phase ii gobal study . 
pao w , miller va , politi ka , et al : acquired resistance of lung adenocarcinomas to getinib or erlotinib is associated with a second mutation in the egfr kinase 2016 293 : 876 - 880 , 2001 domaplos med 2 : e73 , 2005 22 . 
katayama r , khan tm , benes c , et al : therapeutic strategies to overcome crizotinib resistance in non - small cell lung cancers harboring the fusion oncogene eml4 - alk . 
tumor biopsies taken prior to neoadjuvant treatment were analyzed by reverse - phase protein arrays ( rppa ) for expression levels of 210 bc - relevant ( phospho - ) proteins . 
similarly , the mrna virp score was validated ( p , .001 ) in an independent phase ii clinical trial ( promix )  . conclusion our virp score , integrating the expression of nine proteins and validated on mrna data both internally and in an independent clinical trial , may be used to increase the likelihood of benet from treatment with bevacizumab combined with chemotherapy in patients with her2 - negative bc . jco precis oncol 5 : 286 - 306 . 
2021 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction treatment of solid tumors using antiangiogenic therapy has been explored for several decades.1 , 2 discovery of vascular endothelial growth factor a ( vegf - a ) as a major culprit in tumor angiogenesis led to the development of bevacizumab , a recombinant humanized monoclonal antibody targeting vegf - a.3 addition of bevacizumab to various chemotherapy regimens has proven highly benecial in patients with several types of advanced solid tumors resulting in a signicant improvement in overall survival ( os ) and / or progression - free survival ( pfs )  . despite good response to bevacizumab therapy in many individual patients with breast cancer ( bc ) , randomly selected treatment populations do not demonstrate improved os.4 , 5 thus , the clinical use of bevacizumab in bc is limited and currently only approved in europe . 
regardless of this , activity is observed in subsets of patients pointing to the urgent need for novel biomarkers to select subpopulations in which adequate clinical benet can be achieved.6 , 7 one of the most obvious and biological plausible biomarkers was the plasma vegf - a level , and although promising in some studies , evidence from the latter meridian trial did not support its use for identifying patients with benet from added bevacizumab.8 other biomarkers at various molecular levels have been investigated such as soluble carbonic anhydrase ix , 9 brca1 / 2 mutations , 10 and dna methylation signatures.11 however , tissue protein expression and protein signatures have not previously been explored , although data at the proteomic level in general have proven highly valuable in drug response prediction models.12 in this study , we sought to establish protein expression features predicting the response to treatment with bevacizumab in combination with chemotherapy . 
 protein signature predicts response to chemotherapy plus bevacizumab context key objective the use of antivascular endothelial growth factor ( vegf ) targeted therapies in combination with chemotherapy in breast cancer ( bc ) is limited because of the lack of a predictive biomarker . 
in this study , protein expression in pretreatment tumor biopsies was used to develop a predictor for patients with large bcs . knowledge generated a nine - protein response predictor was established by lasso regression trained by a continuous response evaluation . 
the protein signature was validated using corresponding mrna expression in the same patient cohort as well as in an independent patient cohort . relevance our study supports using this protein signature as a predictive marker for vegf inhibition in combination with chemotherapy , and represents a novel opportunity for rational use of this therapy in patients with bc . samples collected from patients with bc prior to neotreatment ( nat ) with chemotherapy ( ctx ) or adjuvant chemotherapy in combination with bevacizumab ( bev plus ctx ) , and analyzed expression against treatment effect on tumor size and clinical outcomes . 
patients with human epidermal growth factor receptor 2 ( her2 ) negative , previously untreated , breast carcinomas with size 2.5 cm were included , and 67 and 71 patients randomly assigned to treatment with ctx or bev plus ctx , respectively . 
one hundred nine samples collected prior to treatment were available for protein analysis on rppa in the ctx treatment arm ( n = 55 ) and in the bev plus ctx treatment arm ( n = 54 ) ( appendix fig a1 )  . 
clinicopathologic characteristics of patients , including adverse events , have previously been described.13 in brief , the primary end point of the clinical study , pcr , was dened as pathologic stage ypt0 and ypn0 after end of therapy . 
in the subset of patients with available protein proles ( n = 109 ) , pcr rates were overall higher in the bev plus ctx ( 26 % ) compared with the ctx ( 13 % ) treatment arm , although not signicantly ( p = .094 ) ( appendix fig a2 )  . 
relative tumor size in percent after 24 weeks of nat was calculated as tumor size at the time of surgery ( longest diameter on histopathologic specimen ) relative to tumor size at week 0 ( mri if available or ultrasound or mammography )  . 
tumor cell content in samples was assessed by use of ascat15 as previously reported.16 the study was approved by the institutional protocol review board , the regional ethics committee , the norwegian medicines agency , performed in accordance with the declaration of helsinki , and informed consent was obtained . 
we further used an external cohort with similar treatment characteristics ( promix trial , clinicaltrials.gov identier : nct00957125 ) , with mrna expression data available , 17 for validation of the virp score . reverse phase protein arrays ( rppa ) proling of 210 cancer - relevant proteins of which 54 were in a phosphorylated state ( appendix table a1 ) were performed by the rppa18 core facility at md anderson cancer center ( houston , tx )  . 
tumor protein lysates were serially diluted two - fold for 5 dilutions ( from undiluted to 1 : 16 dilution ) , probed with antibodies , and visualized by dab colorimetric reaction . 
for development of the virp score , the continuous response parameter relative tumor size was used as outcome , whereas the other clinically used response parameters pcr and rcb were used for evaluation of predictive performance . 
relative importance of each model variable was assessed using the r - package relaimpo23 with metrics lmg . virp scores based on mrna data in the neoava and promix study were computed using the intercept and beta - coefcients determined from the protein data in the neoava study . 
the corresponding surrogate mrna scores were determined using quantile - normalized and probeaveraged mrna expressions from the genes corresponding to the proteins in the original protein signature , including the phosphoproteins . results protein prole of tumors before treatment using unsupervised hierarchical clustering on the expression of the 210 proteins in all 109 tumors collected prior to treatment , they cluster into groups signicantly related to tumor shrinkage and to pam50 subtypes , with most estrogen receptor ( er ) - negative patients ( 17 of 21 ) localizing in a separate subcluster ( appendix fig a4 )  . univariate spearman correlation analysis of protein expressions related to relative tumor size visualized by the nonvariable - dependent rst principal component demonstrated a positive yet limited relationship between the two treatment arms , with expression of almost half of proteins ( n = 103 ) being inversely correlated with response . 
the number of proteins signicantly ( p , .05 unadjusted ) related to response was higher in the ctx treatment arm ( n = 54 ) than in the bev plus ctx arm ( n = 38 ) , with only ten in common and of which two had rho - values with opposite signs ( appendix fig a5 and appendix table a2 )  . development of a protein signature score predicting response to treatment with bev plus ctx addition of bevacizumab to standard treatment with chemotherapy demonstrated benet compared with chemotherapy alone , although not signicant ( appendix fig a2 )  . to develop a signature predicting response to treatment with bev plus ctx , protein expression in biopsies taken prior to treatment were used from patients with available relative tumor size after nat ( n = 54 )  . 
low - variance proteins are likely to have low predictive value , thus a certain level of variance in expression should be present in order for clinical markers to be applicable . 
we thus reduced the original panel of 210 proteins by plotting the variance in expression and demonstrated a mixed distribution ( appendix fig a3 ) where only members belonging mainly to the proteins with higher variance ( n = 114 ; appendix table a3 ) were considered for use in the adaptive lasso regression model . 
a second iterative round of lasso on this subset of ten proteins gave the nal intercept and beta coefcients , of which one was shrunk to zero giving a nal signature of nine proteins with corresponding beta coefcients . 
 protein signature predicts response to chemotherapy plus bevacizumab the virp score for each patient was calculated as the sum of the intercept and beta coefcient weighted expression of the nine proteins . 
in univariate analysis , only the virp score , both as a continuous value and dichotomized ( low v high ) , was signicantly associated with pcr ( table 2 )  . 
no signicant association was found for tumor stage , pam50 subtypes , age , pgr , tp53 mutation , and nodal or er status . we next sought to establish and evaluate the corresponding mrna expression score as a surrogate to the virp protein score . 
by taking the corresponding genes from the virp ( including the parent protein for the phosphoprotein antibodies ) and using the predened lasso intercept and beta coefcients , the mrna score for the neoava patients ( mrna virp scores ) was calculated . 
this demonstrated a signicant increase , approximately doubling , in the percentage of both pcr responders ( p = .009 ) and low rcb ( p = .022 ) in the virp score selected patient population . 
use of the virp score for selecting patients to bev plus ctx demonstrated a clear benet with an increased response both by pcr ( p , .001 ) and rcb ( p , .001 ) compared with standard ctx treatment ( fig 3 )  . discussion we have dened a protein signature score named virp for use in large her2 - negative primary bcs that identies good responders to nat with chemotherapy plus bevacizumab . 
use of the virp score for selection to bev plus ctx therapy signicantly enriches for patients responding 290 2021 by american society of clinical oncology to treatment ( pcr or rcb - low )  . 
importantly , the robustness of the virp score was conrmed through validation in an independent clinical cohort ( promix )  . the lasso regression method was used to select proteins for the virp score . 
however , in silico evaluation the virp proteins under stimulus of bevacizumab treatment links them to response on relevant biological processes ( appendix fig a7 )  . ranking the relative importance of each protein in the virp signature is interesting with respect to , for example , the potential to use each or selected proteins as biomarkers separately . 
it appears that the syk protein is of high importance ( appendix fig a8 ) , which also coincides with being the only protein in the signature differently expressed ( p = .002 ) in pcr versus non - pcr patients . 
the syk protein is enriched in immune cells , but also expressed in breast epithelium and endothelial cells where it plays a role in angiogenesis.26 when passing from protein to mrna expression , functional dimension of activating or deactivating phosphorylations is lost . 
this potentially inuences the performance of the mrna virp score when used as surrogate for the original protein score , and could partly explain the observed drop in auc for the roc analysis between the protein and mrna data sets in the neoava trial ( fig 2a and appendix fig a6a )  . 
spearman correlation between expression of all 210 assessed proteins and mrnas showed that of the nine proteins in the signature , the four with the lowest correlation were phosphorylated or extracellularly localized proteins . 
however , the signature members had a signicantly ( p = .039 ) higher correlation compared with all proteins in the original data set ( appendix fig a9 )  . 
although the neoava protein data set is too small to draw conclusions , a previous observation of nearly 10 , 000 proteins in bc showed that established prognostic mrna - centered signatures ( ie , pam50 - ror , oncotype dx , and mammaprint ) in general had higher protein - mrna correlation than average for the human genome.27 we propose that because of the closer relation proteins have to phenotype , biomarker signatures being developed to identify features with clinical , and thus phenotypical impact , will represent genes with high expressional and translational penetrance . in the neoava clinical trial , patient subgroups were divided based on er expression ( using 1% positivity as cutoff ) , and better response ( as assessed by pcr and rcb ) was in general observed for the er - negative group , whereas only the er - positive group had signicant benet of added in univariate analysis , er bevacizumab . 
this is also consistent with the discrepancy seen in large studies regarding the benet of added bevacizumab in the er - positive or er - negative subpopulations of patients.28 - 30 the relative higher number of proteins signicantly correlated with tumor size after treatment in the ctx arm ( n = 54 ) suggested that a similar protein signature predicting response to chemotherapy alone might be developed . however , use of adaptive lasso regression only returned a signature of two proteins with low predictive performance , and not represented in the bev plus ctx virp signature . use of the virp score developed for bev plus ctx treatment applied on the ctx patients did demonstrate a signicantly lower score in the limited number of patients with pcr ( n = 7 ) , but not when assessed for the low - rcb patients ( n = 14 )  . 
this does not exclude the possibility that the proteins in the virp signature also reect sensitivity to the baseline chemotherapy when combined with bevacizumab . bulk tumor samples may have variable tumor cell content , which might inuence the readout of mrna or proteinbased molecular signatures.31 inuence of tumor cell content ( median of 42% ) on the virp signature , or on its individual proteins , did not demonstrate any signicant associations in the bev plus ctx - treated patients ( appendix fig a11 )  . 
furthermore , the virp score should be related to the mechanism of action of the anti - vegf therapy , which involves normal tissue constituents and in particular endothelial cells and vessels.32 thus , a composite tissue is likely required for the score to function . 
 ( a ) fraction of patients obtaining pcr when treated with standard ctx in all neoava patients ( n = 55 ) or bev plus ctx in all neoava patients ( n = 54 ) and selected based on virp score ( n = 22 )  . 
 ( b ) fraction of patients obtaining low rcb ( 0 and i ) when treated with standard ctx in all neoava patients ( n = 55 ) or bev plus ctx in all neoava patients ( n = 54 ) and selected based on virp score ( n = 22 )  . 
pcr , pathologic complete response ; rcb , residual cancer burden ; virp , vegf inhibition response predictor . 100% 100% random population ctx treatment ( low = 14 high = 41 ) random population bev plus ctx treatment ( low = 20 high = 34 ) virp selected population bev plus ctx treatment ( low = 15 high = 7 ) from treatment with bevacizumab in combination with chemotherapy.34 the virp score is predicting responses , but further studies are warranted to assess for impact on survival . although the discovered virp signature was established for patients treated with bev plus ctx in a neoadjuvant setting , it recapitulates biology related to treatment response and could have the potential to also predict response to bev plus ctx therapy in the metastatic setting . 
additionally , studies are initiated to investigate whether the virp signature recapitulates common response biology shared by other solid cancer types for which bevacizumab in combination with chemotherapy is commonly used.35 affiliations 1department of tumor biology , institute for cancer research , division of cancer medicine , oslo university hospital , the norwegian radium hospital , oslo , norway 2department of genetics , institute for cancer research , division of cancer medicine , oslo university hospital , the norwegian radium hospital , oslo , norway 3department of informaticsbiomedical informatics , university of oslo , oslo , norway 4k.g. 
mills , olav engebraaten provision of study materials or patients : ingrid hedenfalk , elin borgen , niklas loman , thomas hatschek , anne - lise brresen - dale , bjrn naume , gordon b . 
mills , olav engebraaten manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors thomas hatschek consulting or advisory role : roche , pzer , pierre fabre research funding : roche , pzer travel , accommodations , expenses : roche anne - lise brresen - dale employment : arctic pharma as , pubgene stock and other ownership interests : arctic pharma as gordon b . 
mills stock and other ownership interests : catena , signalchem , tarveda therapeutics , immunomet honoraria : nuevolution : astrazeneca , tarveda therapeutics , tesaro , symphogen , pdx pharmacy , immunomet , lilly consulting or advisory role : astrazeneca , signalchem , tarveda therapeutics , symphogen , takeda / millennium , pdx pharmacy , immunomet , lilly , turbine , ion pharma , zentalis research funding : adelson medical research foundation , astrazeneca , nanostring technologies , breast cancer research foundation , karus therapeutics , pzer , prospect creek foundation , tarveda therapeutics , ions pharmaceuticals , immunomet patents , royalties , other intellectual property : hrd assay to myriad genetics , dsp technology patent with nanostring travel , accommodations , expenses : astrazeneca , pzer , symphogen , chrysalis biomedical advisors , immunomet , michigan primary care consortium gunhild m . 
mlandsmo patents , royalties , other intellectual property : patent application submitted for a nine - protein / gene panel predicting response to anti vegf therapies in combination with chemotherapy olav engebraaten patents , royalties , other intellectual property : patent application pending for a biomarker for antibody drug conjugates , patent application submitted for a nine - protein / gene panel predicting response to anti vegf therapies in combination with chemotherapy no other potential conicts of interest were reported . references folkman j : anti - angiogenesis : new concept for therapy of solid tumors . 
 haugen et al roviello g , bachelot t , hudis ca , et al : the role of bevacizumab in solid tumours : a literature based meta - analysis of randomised trials . 
maru d , venook ap , ellis lm : predictive biomarkers for bevacizumab : are we there yet ? clin cancer res 19 : 2824 - 2827 , 2013 gampenrieder sp , westphal t , greil r : antiangiogenic therapy in breast cancer . 
miles d , cameron d , bondarenko i , et al : bevacizumab plus paclitaxel versus placebo plus paclitaxel as rst - line therapy for her2 - negative metastatic breast cancer ( meridian ) : a double - blind placebo - controlled randomised phase iii trial with prospective biomarker evaluation . 
eur j cancer 70 : 146 - 155 , 2017 janning m , m uller v , vettorazzi e , et al : evaluation of soluble carbonic anhydrase ix as predictive marker for efcacy of bevacizumab : a biomarker analysis from the geparquinto phase iii neoadjuvant breast cancer trial . 
fasching pa , loibl s , hu c , et al : brca1 / 2 mutations and bevacizumab in the neoadjuvant treatment of breast cancer : response and prognosis results in patients with triple - negative breast cancer from the geparquinto study . 
ali m , khan sa , wennerberg k , et al : global proteomics proling improves drug sensitivity prediction : results from a multi - omics , pan - cancer modeling 13 . 
silwal - pandit l , nord s , von der lippe gythfeldt h , et al : the longitudinal transcriptional response to neoadjuvant chemotherapy with and without bevacizumab 8 : 2278 - 2288 , 2018 approach . 
h oglander ek , nord s , wedge dc , et al : time series analysis of neoadjuvant chemotherapy and bevacizumab - treated breast carcinomas reveals a systemic shift in genomic aberrations . 
lu y , ling s , hegde am , et al : using reverse - phase protein arrays as pharmacodynamic assays for functional proteomics , biomarker discovery , and drug development in cancer . 
robin x , turck n , hainard a , et al : proc : an open - source package for r and s + to analyze and compare roc curves . 
loibl s , denkert c : how much information do we really need after neoadjuvant therapy for breast cancer ? j clin oncol 35 : 1029 - 1030 , 2017 25 . 
kazerounian s , duquette m , reyes ma , et al : priming of the vascular endothelial growth factor signaling pathway by thrombospondin - 1 , cd36 , and spleen subtype . 
nat commun 10 : 1600 , 2019 von minckwitz g , eidtmann h , rezai m , et al : neoadjuvant chemotherapy and bevacizumab for her2 - negative breast cancer . 
earl hm , hiller l , dunn ja , et al : efcacy of neoadjuvant bevacizumab added to docetaxel followed by uorouracil , epirubicin , and cyclophosphamide , for women with her2 - negative early breast cancer ( artemis ) : an open - label , randomised , phase 3 trial . 
garcia j , hurwitz hi , sandler ab , et al : bevacizumab ( avastin ( r ) ) in cancer treatment : a review of 15 years of clinical experience and future outlook . 
robert nj , di eras v , glaspy j , et al : ribbon - 1 : randomized , double - blind , placebo - controlled , phase iii trial of chemotherapy with or without bevacizumab for rst - line treatment of human epidermal growth factor receptor 2 - negative , locally recurrent or metastatic breast cancer . 
delaloge s , p erol d , courtinard c , et al : paclitaxel plus bevacizumab or paclitaxel as rst - line treatment for her2 - negative metastatic breast cancer in a multicenter national observational study . 
 protein signature predicts response to chemotherapy plus bevacizumab appendix patients assigned to treatment with chemotherapy with or without bevacizumab ( n = 138 ) patients randomly assigned to chemotherapy ( ctx ) ( n = 67 ) patients randomly assigned to chemotherapy and bevacizumab ( bev plus ctx ) ( n = 71 ) ineligible ( n = 1 ) ineligible ( n = 2 ) discontinued treatment ( n = 2 ) patients included in primary endpoint analysis ( n = 66 ) patients included in primary endpoint analysis ( n = 66 ) start of treatment ( n = 55 ) start of treatment ( n = 54 ) fig a1 . 
mixed distribution of protein expression variances ( solid green and blue lines ) ; only proteins with variance above intersection ( red line ) were selected for input in lasso regression to determine the virp ( appendix table a3 )  . 
 protein signature predicts response to chemotherapy plus bevacizumab relative tumor size ( p = .003 ) bevacizumab ( p = .815 ) pam50 ( p < .001 ) bevacizumab relative tumor size pam50 basal her2 luma lumb normal 150% fig a4 . 
rho - values derived from the spearman correlation of protein expression to relative tumor size for patients receiving the bev plus ctx combination ( x - axis ) and ctx treatment only ( y - axis ) with rst principal component of relation between the treatment arms ( stitched red line )  . 
in silico simulation with ingenuity pathway analysis ( version 47547484 , qiagen ) was used to predict biologic effects ( lower row ) affected by the virp member proteins ( second bottom row ) when inuenced by bevacizumab treatment ( top row ) through a set of intermediate proteins ( second top row )  . 
 ( c ) virp scores in rcb low ( 0 and i ) and high ( ii and iii ) patients . ( d ) fraction of patients obtaining pcr when treated with standard ctx in all neoava patients ( n = 55 ) or selected based on virp score ( n = 17 )  . 
 ( e ) fraction of patients obtaining low rcb ( 0 and i ) when treated with standard ctx in all neoava patients ( n = 55 ) or selected based on virp score ( n = 17 )  . 
 tissue / site - agnostic study of ribociclib for tumors with cyclin dcdk4 / 6 pathway genomic alterations : a phase ii , open - label , single - arm basket study julio peguero , md1 ; davendra p . 
grilley - olson , md6 ; vivek subbiah , md7 ; lincoln nadauld , md , phd8 ; das purkayastha , phd9 ; erica stealey , ms9 ; alejandro d . 
kang , phd9 ; and joseph paul eder , md10 purpose as part of the novartis signature program , this study evaluated the efcacy of ribociclib ( selective cyclin - dependent kinase 4 / 6 [ cdk4 / 6 ] inhibitor ) in patients with cyclin dcdk4 / 6 pathwayaberrant tumors . methods this was a phase ii , single - arm , signal - seeking study in patients with advanced malignancies that had progressed on or after standard treatment . 
clinical benet ( dened as the proportion of patients with response or stable disease at 16 weeks ) was the primary end point . results from 61 centers in the united states , 106 patients ( median age , 62.5 years ) were enrolled across multiple malignancies . 
in patients with solid tumors , the clinical benet rate was 18.1% ( n = 19 of 105 ) and the overall response rate was 2.9% ( n = 3 of 105 ) ; three partial responses occurred in patients with adenocarcinoma ( unknown primary ) , soft tissue sarcoma , and urothelial carcinoma . 
2019 by american society of clinical oncology introduction cyclin - dependent kinases 4 and 6 ( cdk4 / 6 ) , in conjunction with their protein regulator cyclin d1 ( encoded by ccnd1 ) , phosphorylate the retinoblastoma ( rb ) protein and regulate g1 cell - cycle progression . 
the p16 ( cdkn2a ) and p15 ( cdkn2b ) tumor suppressors and negaproteins are critical tive regulators of this pathway , mediating cellular senescence.1 , 2 arf ( p19 ) plays an important role in the p53 / mouse double minute 2 homolog ( mdm2 ) - dependent checkpoint ; arf expression leads to activation and stabilization of p53 by promoting mdm2 degradation.3 , 4 pathway alteration can result including from multiple mechanisms , rb mutation or loss , increased signaling through cdk4 and cdk6 amplication , cyclin d1 overexpression , and loss of inhibitors.1 cdk pathway alterations contribute to tumor proliferation and genomic instability , and have been linked to poorer clinical outcomes in multiple cancers . 
cdk4 / 6 and cdkn2a / b abnormalities were reported in 22.8% of patients with various cancers who underwent molecular proling by targeted next - generation sequencing.2 ribociclib is a selective cdk4 / 6 inhibitor that induces dose - dependent rb dephosphorylation , reducing cell proliferation via g1 arrest . 
ribociclib is approved in combination with an aromatase inhibitor as initial endocrine - based therapy for postmenopausal women with hormone receptorpositive / human epidermal growth factor receptor 2 ( her2 ) - negative advanced or metastatic breast cancer . 
 peguero et al context key objective to determine if tumor cyclin dcyclin - dependent kinase 4 / 6 ( cdk4 / 6 ) pathway alterations are an effective signal of efcacy for treatment with ribociclib , a selective cdk4 / 6 inhibitor . knowledge generated in this phase ii , signal - seeking study , 105 patients with heavily pretreated cyclin dcdk4 / 6 pathwayaberrant solid tumors received ribociclib treatment . 
although the primary end point of the study was not met , the clinical benet rate was 18.1% , with partial responses observed in three patients with single gene amplications in the cyclin dcdk4 / 6 pathway . relevance a deeper understanding of the molecular context of tumors is required to accurately match patients to ribociclib , either as a monotherapy or in combination with agents that target interconnected signaling pathways . we present ndings from a signal - seeking study that assessed ribociclib as part of the novartis signature program ( clinicaltrials.gov identier : nct02187783 ) , comprising a series of signal - nding basket protocols in which different single - agent targeted therapies were investigated in a tissueor site - agnostic indication , mutation - specic manner.6 , 7 in this study , patients preidentied as having cdk4 / 6 pathwayaberrant tumors were matched to ribociclib monotherapy . methods study design this was a phase ii , open - label , singletreatment arm , basket study in patients with solid tumors or hematologic malignancies with cdk4 / 6 pathway alterations and whose disease had progressed on or after standard treatment . patients received ribociclib 600 mg , once daily , on a 3week - on / 1 - week - off schedule until disease progression ( by investigator assessment ) , unacceptable toxicity , death , or discontinuation from study treatment ( eg , consent withdrawal , starting a new antineoplastic therapy , investigator decision )  . 
ribociclib dose was reduced to 400 mg , and then to 200 mg if an additional dose reduction was required ; ribociclib dose could not be reescalated . the primary end point was the clinical benet rate assoinvestigator asciated with ribociclib treatment by local sessment , dened as the proportion of patients achieving a complete response ( cr ) , partial response ( pr ) , or stable disease ( sd ) at 16 weeks or later by response evaluation criteria in solid tumors 1.1. 
patients who discontinued treatment before week 16 for reasons other than progressive disease ( pd ) were considered nonevaluable ; patients who had pd before week 16 were considered to have no clinical benet . 
overall response rate ( orr ; ie , cr or pr ) by local investigator assessment was the key secondary end point . patient eligibility criteria patients at least 18 years old with solid tumors or hematologic malignancies with cdk4 / 6 mutations or amplications , cyclin - d1 / d3 gene amplications , or p16 gene mutations or loss were enrolled . 
patients had at least one prior treatment of their recurrent , metastatic , and / or locally advanced disease and had no remaining standard therapy options expected to result in durable response . 
because of overlapping disease - oriented studies , the following tumor types were excluded : breast cancer ( except triple negative ) , liposarcoma , teratoma , castrate - resistant prostate cancer , melanoma , and mantle cell lymphoma . 
all patients gave written informed consent before treatment , according to federal and local stitutional guidelines . genomic proling gene aberrations were assessed in a local clinical laboratory improvement amendmentscertied laboratory before patient consent . 
once a patient was identied , vestigators contacted novartis study enrollment consideration.8 post hoc broad molecular proling using a next - generation dna sequencing panel of more than 280 cancerassociated genes9 was performed centrally on pretreatment tumor biopsy specimens from all patients . 
 mutation - specic , tissue / site - agnostic study of ribociclib statistical analysis tumor cohorts were formed when four or more patients with a particular tumor type were enrolled . 
the number of patients enrolled per tumor type was based on a patientsparing , adaptive design , allowing early closure of nonresponding groups and / or groups with early success . clinical benet was evaluated using a bayesian adaptive statistical design that allowed dynamic borrowing of information across cohorts on the basis of their degree of similarity.8 the statistical design used a hierarchical model that allowed dynamic borrowing of information between groups . 
this design allowed analyses with small sample sizes for each cohort . at least 10 patients were required to evaluate early futility , and at least 15 to evaluate early success and make a go or no - go decision for each tumor type cohort . 
if there was an 80% or greater probability that the response rate exceeded the historical rate , the group was considered a success . orr , pr , or cr on the basis of local investigator assessment were summarized , and 95% exact cis using the clopperpearson method were also reported.8 correlation between a specic genomic ( somatic ) dna prole , based laboratory analysis , and clinical benet was on central explored . 
in addition , ribociclib safety and tolerability were reported . results patients in total , 106 patients from 61 centers in the united states were enrolled across multiple malignancies between august 25 , 2014 , and may 4 , 2015 . 
of the 105 patients with solid tumors , 19 ( 18.1% ) achieved clinical benet ( primary end point ) ; the orr ( key secondary end point ) was 2.9% ( three prs ; table 2 )  . 
the rst patient , a 59 - year - old man with poorly differentiated adenocarcinoma of unknown primary with cdk6 amplication , achieved a pr ( 100% reduction in target lesions ) after the fourth cycle of ribociclib and was continuing therapy at last data cutoff with a duration of response of + 796 days . 
the second patient , a 25year - old man with poorly differentiated , round blue cell soft tissue sarcoma not otherwise specied with cdk4 amplication , had a pr ( 100% reduction ) after two cycles of ribociclib , with a duration of response of 330 days . 
the third patient , a 53 - year - old man with urothelial carcinoma of the bladder with ccnd1 amplication , also experienced a pr ( 37.5% reduction ) after two cycles of ribociclib , with a duration of response of 254 days . 
his bladder cancer had not responded to either rst - line cisplatin plus gemcitabine combination or apatorsen ( ogx - 427 ) an experimental antisense inhibitor targeting heat shock protein 27 . 
one patient with papillary serous ovarian carcinoma with cdk6 mutation ( not conrmed by central review ) experienced a tumor burden reduction of at least 30% , without subsequent conrmation , and had sd for 239 days . 
 ( % ) unless otherwise indicated . abbreviations : ecog , eastern cooperative oncology group ; ps , performance status . * gastroesophageal junction ( n = 4 ) , head and neck nonsquamous cell carcinoma ( n = 4 ) , unknown primary site ( n = 4 ) , uterus ( n = 4 ) , esophagus ( n = 3 ) , ovarian ( n = 3 ) , skin nonmelanoma ( n = 3 ) , cholangiocarcinoma ( n = 2 ) , colorectal ( n = 2 ) , renal cell carcinoma ( n = 2 ) , liver ( n = 2 ) , neuroendocrine ( n = 2 )  . 
other histologies ( n = 10 ) only included one each . based on local molecular proling . a patient can be counted in multiple categories ; therefore , the overall count can be  . 
100. 4 2019 by american society of clinical oncology there was no association between any specic genomic ( somatic ) dna prole and clinical benet per central analysis ( fig 3 )  . 
however , 18 of 19 patients ( 94.7% ) with clinical benet had tumors with a single hit in the cyclin d - cdk4 / 6 pathway and one patient with clinical benet had multiple mutational events ; patients with a pr had tumors with cdk4 / 6 or ccnd1 amplication . 
in total , 86 patients had a single cyclin dcdk4 / 6 pathway mutation and 10 patients had multiple pathway mutations ; central mutation analysis was not available in nine patients . 
the most common aes suspected to be related to the study drug included fatigue ( 31.1% ) , neutropenia ( 30.2% ; decreased neutrophils , 15.1% ) , and nausea ( 29.2% ; table 3 )  . 
of these , fatigue and nausea were typically mild . the most common grade 3 / 4 ae suspected to be related to the study drug was neutropenia ( 18.9% ; n = 20 ; decreased neutrophils , 7.5% , n = 8 ) ; only one incident of febrile neutropenia ( grade 3 ) occurred , but it was effectively managed with supportive care and antibiotics . 
 mutation - specic , tissue / site - agnostic study of ribociclib screened ( n = 176 ) enrolled ( n = 106 ) excluded * unacceptable laboratory value unacceptable test result unacceptable medical history intercurrent medical event did not meet diagnostic / severity criteria use of excluded medications patient withdrew consent other ( n = 70 ) ( n = 22 ) ( n = 15 ) ( n = 6 ) ( n = 6 ) ( n = 7 ) ( n = 8 ) ( n = 2 ) ( n = 10 ) still receiving study drug ( n = 1 ) discontinued disease progression patient / guardian decision adverse event death protocol deviation physician decision ( n = 105 ) ( n = 80 ) ( n = 9 ) ( n = 8 ) ( n = 3 ) ( n = 3 ) ( n = 2 ) consented for survival follow - up ( n = 89 ) death lost to follow - up ( n = 58 ) ( n = 31 ) fig 1 . 
as such , more patients have been identied with potentially actionable pathway activation , raising the hope of personalized medicine through targeted drug treatment.10 , 11 the design of basket trials enables molecularly driven enrollment and treatment assignment , with simultaneous testing of a single targeted agent in tumors of different histologies that harbor genetic alterations in the targeted pathway.12 - 14 the signature program was built on this approach and included eight agentspecic , signal - seeking phase ii basket trials of various targeted therapies in a histology - agnostic , mutation - specic manner , matching patients with potentially actionable mutations to the corresponding agent . 
the aim of the signature program was to support or refute the hypothesis that driver mutations determine therapeutic response to treatment in a histology - agnostic manner . this tissueor site - agnostic approach was recently evaluated in patients with solid tumors and led to the us food and drug administration granting accelerated approval to pembrolizumab for the rst tissueor site - agnostic indication.15 indeed , the prospects for the tissueor siteagnostic approach in oncology have never looked brighter , as the successful stories of larotrectinib and entrectinib continue to unfold.16 moreover , the food and drug administration has also recently granted marketing approval to several diagnostics based on next - generation sequencing : the praxis extended ras panel ( illumina , san diego , ca ) , the oncomine dx target test ( thermo fisher scientic , waltham , ma ) , and the foundationone cdx ( foundation medicine , cambridge , ma ) .17 - 19 these tests , and others under clinical investigation , could identify which patients with pathway - aberrant tumors may benet from targeted treatment options . 
thus , the aim for the present ribociclib signal - seeking study was to match patients with cdk4 / 6 pathway - aberrant tumors with the selective cdk4 / 6 inhibitor ribociclib . the primary end point of the study was the rate of clinical benet associated with ribociclib monotherapy , based on local investigator assessment . 
prs were observed in three patients , and 16 patients had sd for 16 weeks or longer . two patients with pr had the maximum percentage reduction from baseline in target lesions ( 100% )  . 
unlike the mutations affecting rb activation , cdkn2a mutation or loss concomitantly decreases the critical function of the p53 - stabilizing effect of the arf protein on the ubiquitin ligase mdm2 , mimicking many mutations in tp53 . 
other selective cdk4 / 6 inhibitors , palbociclib and abemaciclib , have shown low - rate monotherapy activity outside of breast cancer.20 - 23 similarly , a few extraordinary long - term responses have been observed with these agents in tumors with ccnd1cdk4 / 6 amplications . 
these observations may be partly due to the molecular context of the tumor . cyclin dcdk4 / 6 pathway activity is regulated by a number of mitogenic signals , including epidermal growth factors , signaling through the her2 and estrogen receptors , and the phosphoinositide 3 - kinase ( pi3k ) akt pathway.24 studies have suggested that response to targeted therapy may be affected by the presence of tumor mutations in related signaling pathways . 
 mutation - specic , tissue / site - agnostic study of ribociclib chromosome head and neck nonsquamous - cell carinoma head and neck squamous - cell carinoma adrenals bladder breast , triple negative cervix cholangiocarcinoma chordoma colorectal esophagus gallbladder ducts gastroesophageal junction gist kidneys liver lung , nonsmall - cell nonadenocarcinoma lung , nonsmall - cell adenocarcinoma lung , nonsmall - cell squamous lymphoma mesothelioma neuroendocrine ovarian pancreas penile prostate salivary gland sarcoma skin , nonmelanoma thyroid unknown primary uterus shrinkage mutation amplication loss rearrangement short variant fig 3 . 
the most common grade 3 / 4 aes suspected to be related to ribociclib was neutropenia ( 18.9% ) and decreased neutrophils ( 7.5% ) ; only one incident of febrile neutropenia ( grade 3 ) was reported , which was effectively managed with supportive care and antibiotics . 
no deaths due to aes were suspected to be related to study drug per the investigator . one study limitation was the restriction of cohorts by tumor type rather than molecular subtype . 
a second limitation was the exclusion of the most obvious indications for single - agent cdk4 / 6 inhibition : hormone - sensitive breast cancer , liposarcoma , teratoma , castrate - resistant prostate cancer , melanoma , and mantle cell lymphoma . 
this exclusion was due to overlapping disease - oriented studies in these indications , which already were in place by the time this tissueor site - agnostic study started . in conclusion , although no tumor - type cohort graduation was observed , preliminary activity was seen in tumors with single - hit ccnd1cdk4 / 6 amplications . 
these ndings investigation and suggest that in the warrant additional absence of ccnd1cdk4 / 6 amplications or in patients with multiple mutational events , cdk4 / 6 inhibition may require combination with other agents that provide additive or synergistic effects . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . julio peguero employment : oncology consultants leadership : oncology consultants davendra p . 
sohal honoraria : foundation medicine consulting or advisory role : perthera , ability pharma research funding : novartis ( inst ) , celgene ( inst ) , oncomed ( inst ) , bayer ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) , loxo ( inst ) bert h . 
oneil employment : eli lilly consulting or advisory role : bristol - myers squibb , merck karen kelly honoraria : merck consulting or advisory role : astrazeneca , roche , eli lilly , regeneron , abbvie , janssen , emd serono , merck , pzer , astrazeneca research funding : emd serono ( inst ) , genentech ( inst ) , abbvie ( inst ) , five prime therapeutics ( inst ) , regeneron ( inst ) patents , royalties , other intellectual property : author royalties for uptodate travel , accommodations , expenses : astrazeneca , roche , merck , regeneron , eli lilly , abbvie , emd serono , merck juneko e . 
grilley - olson consulting or advisory role : bayer , chimerix research funding : nanocarrier ( inst ) , genentech ( inst ) , seattle genetics ( inst ) , medimmune ( inst ) , pzer ( inst ) vivek subbiah consulting or advisory role : medimmune research funding : novartis ( inst ) , glaxosmithkline ( inst ) , nanocarrier ( inst ) , northwest biotherapeutics ( inst ) , roche ( inst ) , berg pharma ( inst ) , bayer ( inst ) , incyte ( inst ) , fujilm ( inst ) , pharmamar ( inst ) , d3 oncology solutions ( inst ) , pzer ( inst ) , amgen ( inst ) , abbvie ( inst ) , multivir ( inst ) , blueprint medicines ( inst ) , loxo ( inst ) , vegenics ( inst ) , takeda ( inst ) , alfasigma ( inst ) , agensys ( inst ) , idera ( inst ) , boston biomedical ( inst ) , inhibrx ( inst ) , exelixis ( inst ) travel , accommodations , expenses : pharmamar , bayer lincoln nadauld stock and other ownership interests : toma biosciences , citizen corporation consulting or advisory role : roche speakers bureau : genentech patents , royalties , other intellectual property : navican travel , accommodations , expenses : roche , chugai pharma das purkayastha employment : novartis pharmaceuticals erica stealey employment : novartis stock and other ownership interests : novartis alejandro d . 
clin cancer res 21 : 2905 - 2910 , 2015 kato s , schwaederle m , daniels ga , et al : cyclin - dependent kinase pathway aberrations in diverse malignancies : clinical and molecular characteristics . 
cell cycle 14 : 1252 - 1259 , 2015 zhang y , xiong y , yarbrough wg : arf promotes mdm2 degradation and stabilizes p53 : arf - ink4a locus deletion impairs both the rb and p53 tumor suppression pathways . 
cell 92 : 725 - 734 , 1998 ozenne p , eymin b , brambilla e , et al : the arf tumor suppressor : structure , functions and status in cancer . 
n engl j med 375 : 1738 - 1748 , 2016 kang bp , slosberg e , snodgrass s , et al : the signature program : bringing the protocol to the patient . 
n engl j med 377 : 62 - 70 , 2017 slosberg ed , kang bp , peguero j , et al : signature program : a platform of basket trials . 
oncotarget 9 : 21383 - 21395 , 2018 frampton gm , fichtenholtz a , otto ga , et al : development and validation of a clinical cancer genomic proling test based on massively parallel dna sequencing . 
lopez - chavez a , thomas a , rajan a , et al : molecular proling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
patnaik a , rosen ls , tolaney sm , et al : efcacy and safety of abemaciclib , an inhibitor of cdk4 and cdk6 , for patients with breast cancer , non - small cell lung cancer , and other solid tumors . 
goldman jw , shi p , reck m , et al : treatment rationale and study design for the juniper study : a randomized phase iii study of abemaciclib with best supportive care versus erlotinib with best supportive care in patients with stage iv non - small - cell lung cancer with a detectable kras mutation whose disease has progressed after platinum - based chemotherapy . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
edelman mj , redman mw , albain ks , et al : a phase ii study of palbociclib ( p ) for previously treated cell cycle gene alteration positive patients ( pts ) with stage iv squamous cell lung cancer ( scc ) : lung - map sub - study swog s1400c . 
ther adv med oncol 10 : 1 - 15 , 2018 janku f , hong ds , fu s , et al : assessing pik3ca and pten in early - phase trials with pi3k / akt / mtor inhibitors . 
kim s , tiedt r , loo a , et al : the potent and selective cyclin - dependent kinases 4 and 6 inhibitor ribociclib ( lee011 ) is a versatile combination partner in preclinical cancer models . 
 circulating cell - free tumor dna in the management of double primary tumors introduction synchronous lung and colorectal cancer ( crc ) occurrence in one individual is a rare event.1 - 3 the genomics of both malignancies have been extensively studied and found to be distinct . 
 broad molecular profiling in advanced non small - cell lung cancer is widely accepted and routinely used in selecting targeted therapy , because response rates ( rrs ) to single targeted agents are twoto three - fold higher than those to cytotoxic chemotherapy.4 - 11 in advanced crc , potentially targeted alterations are mostly detected in the braf gene ; however , the rr in crc is typically worse than in nonsmall - cell lung cancer ( rr range in crc , 10% to 15% )  . 
 in addition , in crc , expanded testing of the kras and nras genes is used as a negative predictor of antiepidermal growth factor receptor ( egfr ) antibody treatment.12 circulating cell - free tumor dna ( ctdna ) sequencing is a blood - based test , also known as liquid biopsy , which is currently widely used for tumor genomic profiling.13 in contrast to tissue biopsy , ctdna sequencing is a noninvasive approach and thus especially valuable where the tumor tissue obtained is insufficient for molecular testing . 
most importantly , liquid biopsy may provide a global summary of intraand intertumor heterogeneity.14 guardant 360 ( guardant health , redwood city , ca ) is a liquid biopsy test based on digital sequencing technology . 
 the clinical sensitivity and specificity of this test are comparable to those of tissue - based next - generation sequencing ( ngs ; analytic specificity of > 99.9999% at the per - nucleotide level ) .15 absolute variant allele fractions , including egfr and braf single - nucleotide variants , have been shown to tightly correlate with a well - validated orthogonal digital droplet polymerase chain reactionbased plasma analysis.16 we present a case of a patient with synchronous lung and colorectal cancers driven by two different oncogenic drivers ( egfr l858r and braf v600e for the lung and colorectal tumors , respectively )  . 
whereas the incidence of the abovementioned molecular aberrations in these tumor types ranges from 10% to 20% , 17 - 19 it is rare to discover both in the same individual . 
biopsy of the colonic mass confirmed a cdx2 - positive adenocarcinoma compatible with primary colonic orig positron emission tomographycomputed tomography scan showed the abovementioned tumor in the right colon and also demonstrated metastatic disease in the bones and a speculated right upper lobe ( rul ) lesion with an atelectatic component compatible with a second primary lung tumor ( fig 1a )  . 
a biopsy of both the rul lesion and the t9 lytic mass confirmed the diagnosis of metastatic lung adenocarcinoma in both tumor specimens ; tumor cells were positive for ttf1 and ck7 and negative for cdx2 and ck20 . because the rul lesion and the vertebral metastasis had insufficient tumor tissue for elizabeth dudnik tal twito iris faull addie dvir lior soussan - gutman ofer purim richard b . 
 ( a ) positron emission tomographycomputed tomography scan demonstrating metastatic disease in the spiculated right upper lobe ( rul ) lesion with an atelectatic component compatible with a second primary lung tumor . 
targeted ngs of the ctdna identified two driver mutations : egfr l858r at 2.4% mutant allele fraction ( maf ) and braf v600e mutation at 0.9% maf ( fig 2a )  . 
after the ctdna analysis , the tumor specimen obtained from the bone lesion was reviewed , and polymerase chain reaction analysis for egfr ( amoydx egfr 29 mutations detection ce - ivd kit ; xiamen , peoples republic of china ) was performed , confirming the presence of egfr l858r mutation in the bone metastasis . 
the origin of the braf v600e clone at that point remained unclear . when the patient was about to start treatment with anti - egfr therapy , she was diagnosed with acute large - bowel obstruction and underwent extended right hemicolectomy , which revealed moderately differentiated colonic adenocarcinoma infiltrating the pericolic fat with three involved regional lymph nodes and positive surgical margins ( pt3n2r1 )  . 
soon thereafter , the patient developed a large pericardial effusion , and pericardial window was performed , revealing no viable tumor in the pericardial tissue specimen . erlotinib was initiated , resulting in a significant shrinkage of the rul mass ; however , new liver metastases developed ( fig 1b )  . 
this time , braf testing as well as kras and nras testing was performed ( amoydx ce - ivd kit ) , revealing that the tumor was kras wild type and nras wild type and harbored a braf v600e mutation . after the diagnosis of metastatic crc , in march 2016 , capecitabine was added to erlotinib . 
although not known as driver mutations , these mutations are more common in crc than in lung cancer , and their mafs increased from the initial test to that performed after the patient received egfr inhibitors ( fig 2b )  . after the second ctdna testing , the treatment was switched to a combination of vemurafenib and erlotinib.20 - 22 however , the treatment was poorly tolerated ( severe diarrhea ) and was therefore discontinued after 1 month . 
previous genetic studies of crc have identified somatic mutations in four main candidate pathways : tgf - , wnt , p53 , and rtk - ras , all of which were identified as important contributors to crc development.29 among them , mutations in the smad4 , apc , fbxw7 , and braf genes were identified as recurrent mutations in patients with crc.29 - 31 in contrast , apc was suggested to be a gatekeeper , which regulates epithelial cells to develop into adenoma and even carcinoma cells.32 notably , not only did liquid biopsy detect both tumor driver mutations at the time of initial diagnosis , it also reflected the progression of the second primary colon tumor , early in the course of the disease , even before its growth was shown in imaging . 
a rise in the maf of braf v600e , a driver mutation , as well as other crc - associated mutations ( smad4 , apc , fbxw7 ) , alongside a drop in the maf of the egfr l858r mutation , suggested that the new retroperitoneal lesions were related to the crc . 
this finding is consistent with other reports showing how ctdna allele fractions serve as early indicators of response versus progression in earlyand late - stage crc.33 , 34 later on , liquid biopsy allowed simultaneous response monitoring of both tumors . 
however , it should be emphasized that for clinical application of monitoring with serial testing , the assay used must be validated not only for detecting mutations but also for accurate quantitation of variant allele fractions . 
our patient did not benefit from the braf inhibitor , possibly because single - agent braf inhibitor yields poor results in patients with crc with braf mutations.12 therefore , inhibition of multiple pathways and immunotherapy should have been considered.35 although tumor mutational burden was not assessed here , analysis of blood - derived ctdna demonstrated high mutation in november 2015 as well as in june 2016 ( fig 2 )  . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . elizabeth dudnik consulting or advisory role : boehringer ingelheim speakers bureau : boehringer ingelheim , roche , astrazeneca , pfizer , merck sharp & dohme , bristol - myers squibb , novartis research funding : boehringer ingelheim ofer purim no relationship to disclose richard b . 
lanman employment : guardant health , veracyte leadership : guardant health , biolase stock and other ownership interests : guardant health , biolase research funding : guardant health affiliations elizabeth dudnik and ofer purim , davidoff cancer center , rabin medical center , petach tikva ; tal twito , addie dvir , and lior soussan - gutman , teva pharmaceuticals industries , shoam , israel ; and iris faull and richard b . 
yun hr , yi lj , cho yk , et al : double primary malignancy in colorectal cancer patients : msi is the useful marker for predicting double primary tumors . 
chiang jm , yeh cy , changehien cr , et al : clinical features of second other - site primary cancers among sporadic colorectal cancer patients : a hospital - based study of 3 , 722 cases . 
zhou c , wu yl , chen g , et al : erlotinib versus chemotherapy as first - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
sequist lv , yang jc , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
mazires j , barlesi f , filleron t , et al : lung cancer patients with her2 mutations treated with chemotherapy and her2 - targeted drugs : results from the european euher2 cohort . 
paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
sarfaty m , moore a , neiman v , et al : ret fusion lung carcinoma : response to therapy and clinical features in a case series of 14 patients . 
prez - callejo d , romero a , provencio m , et al : liquid biopsy based biomarkers in non - small cell lung cancer for diagnosis and treatment monitoring . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
ulrich bc , nagy rj , odegaard ji , et al : cross - platform detection and quantification of actionable mutations in cell - free dna shows high concordance and correlation between next - generation sequencing and droplet digital pcr . 
pao w , miller va : epidermal growth factor receptor mutations , small - molecule kinase inhibitors , and non - small - cell lung cancer : current knowledge and future directions . 
sanz - garcia e , martinez am , elez e , et al : survival determinants with matched targeted therapies in braf mutant metastatic colorectal cancer ( mcrc )  . 
barlesi f , mazieres j , merlio jp , et al : routine molecular profiling of patients with advanced nonsmall - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
ohashi k , sequist lv , arcila me , et al : lung cancers with acquired resistance to egfr inhibitors occasionally harbor braf gene mutations but lack mutations in kras , nras , or mek1 . 
blakely cm , watkins tbk , wu w , et al : evolution and clinical impact of co - occurring genetic alterations in advanced - stage egfr - mutant lung cancers . 
kim st , lee ws , lanman rb , et al : prospective blinded study of somatic mutation detection in cell - free dna utilizing a targeted 54 - gene next generation sequencing panel in metastatic solid tumor patients . 
tie j , wang y , tomasetti c , et al : circulating tumor dna analysis detects minimal residual disease and predicts recurrence in patients with stage ii colon cancer . 
we hypothesized that patients with pdac with germline brca1 , brca2 , or palb2 mutations may benefit preferentially from platinum - based chemotherapy . materials and methods twenty - nine individuals with deleterious germline mutations in brca1 , brca2 , or palb2 and a diagnosis of advanced pdac ( mut - positive ) were matched 2 : 1 to patients who were noncarrier or untested ( control ) by age at diagnosis , year of diagnosis , stage , and sex . 
patients were identified via one of two available databases at the university of pennsylvania : the basser center for brca registry or the university of pennsylvania electronic medical patient record . 
2018 by american society of clinical oncology introduction pancreatic ductal adenocarcinoma ( pdac ) is an increasingly prevalent and often rapidly fatal malignancy.1 - 3 even with the relatively recent introduction of gemcitabine plus paclitaxel4 and folinic acid , fluorouracil , irinotecan , and oxaliplatin ( folfirinox ) 5 chemotherapy regimens , the median overall survival for patients with inoperable disease remains abysmal at , 1 year . 
 clinically , breast and ovarian cancers associated with brca1 and brca2 mutations have heightened sensitivity to platinum - based chemotherapies and to parp inhibitors.16 - 22 these observations suggest that patients with pdac due to brca1 , brca2 , or palb2 germline mutations with resulting hrd might also benefit from similar therapeutic strategies . early data have suggested that patients with advanced pdac and a germline brca1 / 2 mutation who received platinum treatment had higher tumor response rates and improved overall survival compared with those who did not receive platinum.23 however , because of their high toxicity , platinum - based therapies such as folfirinox are often reserved for the younger , healthier patients . 
therefore , without an age - matched control group , it is unclear whether the inherent bias to select platinum - based treatment in healthier patients might have affected these results . we performed a retrospective cohort study of patients with unresectable pdac . 
these were matched 2 : 1 with patients who either had not been tested or were known not to have a germline deleterious mutation ( referred to collectively as control ) by age at diagnosis , year of diagnosis , stage at diagnosis , and sex . 
patients were identified one of two ways : enrollment in the university of pennsylvania basser center for brca registry or identification via the university of pennsylvania patient electronic medical record ( emr )  . 
the emr was mined using pennseek , which allows for targeted keyword searches of unstructured or semistructured medical documents . notably , patients who were mut - positive were identified in both the basser registry and the emr . 
data were collected and extracted using the emr , paper records , and patient and family reports , and online using the social security death index . patients diagnosed with either locally advanced or metastatic pdac between january 1 , 1995 , and december 31 , 2016 , were included . 
cases were defined as patients with a known pathogenic germline brca1 , brca2 , or palb2 mutation . controls were either confirmed mutation noncarriers or those who had not been tested . 
collected data included demographics , clinical history , personal history of prior malignancies , family history of cancers , and treatments related to pdac , including surgical interventions , radiation , and systemic chemotherapy . 
the institutional review board at the university of pennsylvania approved this study . overall survival overall survival ( os ) was defined as the time from the date of diagnosis of pdac to the date of death from any cause . 
the os for patients exposed to platinum - based treatments ( including cisplatin , oxaliplatin , or carboplatin and with at least one confirmed dose ) during the course of their disease were compared with the os for patients who had not been exposed to such treatment . 
whenever possible , specific regimen details were recorded . statistical analysis univariate analysis was performed using fishers exact test for dichotomous variables and students t test or wilcoxon rank sum test for normal and nonnormal continuous variables , respectively . hazard ratios ( hrs ) and 95% cis were calculated using the cox proportional hazards model . 
survival curves were compared using the log - rank test . each patient who was mut - positive was matched to two control patients using a greedy - match algorithm24 without replacement on the basis of four patient factors : stage at diagnosis , age at diagnosis , year of diagnosis , and sex . 
all statistical analyses were performed using sas 9.4 ( sas institute , cary , nc )  . results patients and tumor characteristics overall , 29 patients who were mut - positive were identified with the following mutational breakdown : brca1 ( n = 12 ) , brca2 ( n = 15 ) , and palb2 ( n = 2 )  . 
the median age of control patients was 63.5 years ( range , 38 to 82 years )  . demographics are summarized in table 1 . clinical and treatment characteristics of patients of the 87 patients , four mut - positive patients ( 13.8% ) and 12 control patients ( 20.7% ) received no systemic treatment of any kind . 
for patients who were mut - positive and who did receive systemic therapy , 18 of 25 cases ( 72.0% ) received platinum - based therapy during their treatment course : 12 ( 48.0% ) received oxaliplatin , three ( 12.0% ) received cisplatin , two ( 8.0% ) received both oxaliplatin and cisplatin , and the exact regimen was unknown for one patient . among control patients , 28 of 46 ( 60.8% ) received platinum - based therapy : 27 ( 96.4% ) received oxaliplatin , one received cisplatin ( 3.5% ) , and the regimen was unknown for one patient . 
among patients who were mut - positive and for whom this information was known , six ( 33% ) received a parp inhibitor and 12 ( 67% ) did not . 
the median os for patients who were mut - positive and had received platinumbased treatment was undefined ( at a median follow - up of 20.1 months ) , and the median os for control patients was 15.5 months ( fig 1 ; table 2 )  . 
 ( % ) unless otherwise noted . abbreviations ; fhx , family history ; folfirinox , folinic acid , fluorouracil , irinotecan , oxaliplatin ; folfox , folinic acid , fluorouracil , oxaliplatin ; iqr , interquartile range . mutations ( control ) when both receive platinumbased treatment . 
in mut - positive patients , the median os was not yet reached at median follow - up of 20.1 months , and the 1 - year os was 94% . however , when patients who are mut - positive and control patients who did not receive platinum therapy were compared , there was no os difference between groups . 
 ( a - c ) kaplanmeier survival curves demonstrating the overall survival for ( a ) the full cohort , ( b ) patients treated with platinum , and ( c ) patients treated without platinu ( d ) breakdown of hazard ratios for the full cohort of patients . this may suggest that mutational status is predictive of benefit to platinum - based therapies . in mut - positive patients treated with platinum therapy , the regimens were split nearly evenly between folfirinox ( folinic acid , fluorouracil , irinotecan and oxaliplatin ) , folfox ( folinic acid , fluorouracil andoxaliplatin ) , andcisplatin / gemcitabine.subgroup analysis comparing oxaliplatin to cisplatin did not demonstrate a difference between regimens , with curves clearly overlapping . 
it is possible that receiving a platinum agent , regardless of which one , is beneficial to patients with pdac who carry a germline brca1 , brca2 , or palb2 mutation . 
however , because cisplatin and oxaliplatin differ in their mechanisms of action and therefore trigger different dna repair pathways , it is also reasonable to hypothesize that there is a therapeutic difference between these agents in patients with an hrd . 
whether an oxaliplatin - based treatment or a cisplatin - based regimen is superior for this population is an area of active research . one of the key strengths of our study is the fact that we were able to fully match our cohort of patients with and without brca1 , brca2 , or palb2 mutations on age at diagnosis , year of diagnosis , sex , and stage . 
in our subgroup analysis of those who received platinum - based therapy , there continued to be no significant differences between mut - positive and control patients regarding these variables . 
golan et al23 reported an os benefit in patients with pdac with brca mutations who had received platinum , but because this study did not include a comparison with patients who did not carry mutations , it was unclear if the observed benefit was due to patient selection bias ( such as age ) or carrier status . 
our data suggest that patients with brca1 , brca2 , or palb2 mutations and pdac may be more likely to respond to platinum , similar to other cancer types , such as breast and ovarian . our study has several important limitations . 
patients in the registry were less likely to have received all their treatment at the university of pennsylvania , meaning that control patients were more uniformly treated at our single - institution academic center . 
however , we were able to collect treatment data for the vast majority of patients . second , because testing for germline brca1 / 2 and palb2 mutations in patients with pdac has only recently been offered as a standard part of clinical practice , our control group may have inadvertently contained patients who were carriers table 3 . 
comparison of baseline variables for patients receiving and not receiving platinum therapy subgroup controls cases year of diagnosis , median ( iqr ) 2014 ( 2010 - 2015 ) 2014 ( 2011 - 2015 ) patients who received platinum age at diagnosis , mean ( sd ) stage at diagnosis stage iii stage iv patients who received no platinum age at diagnosis , mean ( sd ) males males stage at diagnosis stage iii stage iv 57 ( 10 ) 17 ( 61 ) 7 ( 25 ) 21 ( 75 ) 67 ( 9 ) 15 ( 50 ) 3 ( 10 ) 27 ( 90 ) note . 
 ( % ) unless otherwise noted . abbreviations : iqr , interquartile range ; sd , standard deviation . 61 ( 9 ) 8 ( 44 ) 2 ( 11 ) 16 ( 89 ) 65 ( 14 ) 7 ( 64 ) 3 ( 27 ) 8 ( 73 ) year of diagnosis , median ( iqr ) 2013 ( 2009 - 2015 ) 2006 ( 2002 - 2014 ) .053 of brca or other homologous recombination deficiencies . 
however , if patients with germline brca1 , brca2 , or palb2 mutations had unintentionally been included in our control group , this would have plausibly biased toward the null hypothesis . a third limitation is potential survival bias due to the timing of brca or palb2 testing . 
it is possible that patients who survive their pdac diagnosis longer are more likely to undergo genetic testing . prospective cohorts are needed to overcome potential survival bias . our findings have several implications . 
given that patients who are mut - positive may have a substantial survival benefit when treated with platinumbased therapy , it might be beneficial for such patients to be selected for this treatment strategy up front when presenting with inoperable pdac . second , on the basis of our data , efforts should be made to maximize the identification of brca1 , brca2 , and palb2 mutation carriers either by expanding up - front germline testing or by confirming germline status when somatic sequencing identifies a mutation . 
although clinical clues , such as ashkenazi ancestry , a family history of brcaassociated malignancies , or a personal history of other cancers , can be helpful and in themselves may predict for response to platinum agents , 25 not all of the patients in our small cohort had these features . perhaps most importantly , our findings provide further evidence that pdac in patients with germline brca1 , brca2 , or palb2 mutations may represent a fundamentally biologically different group compared with sporadic pdac , suggesting that clinical trial and drug development strategies for this cohort should perhaps be different than for the general population of patients with pdac . indeed , clinical trials using parp inhibitors for patients with pdac and a brca1 , brca2 , or palb2 mutation are currently underway ( clinicaltrials.gov identifiers : nct03140670 and nct02184195 )  . it is unknown whether our observation would extend to patients with somatic alterations in brca1 , brca2 , or palb2 and whether allelespecific loss of heterozygosity would be required to observe the same biologic effect . 
at risk case control 17 time ( months ) in conclusion , we present a small cohort study in which we observe a substantial survival benefit when patients with advanced pdac and a brca or palb2 mutation are treated with platinumbased therapy . 
rahib l , smith bd , aizenberg r , et al : projecting cancer incidence and deaths to 2030 : the unexpected burden of thyroid , liver , and pancreas cancers in the united states . 
murphy km , brune ka , griffin c , et al : evaluation of candidate genes map2k4 , madh4 , acvr1b , and brca2 in familial pancreatic cancer : deleterious brca2 mutations in 17% . 
blanco a , de la hoya m , osorio a , et al : analysis of palb2 gene in brca1 / brca2 negative spanish hereditary breast / ovarian cancer families with pancreatic cancer cases . 
dann rb , deloia ja , timms km , et al : brca1 / 2 mutations and expression : response to platinum chemotherapy in patients with advanced stage epithelial ovarian cancer . 
isakoff sj , mayer el , he l , et al : tbcrc009 : a multicenter phase ii clinical trial of platinum monotherapy with biomarker assessment in metastatic triple - negative breast cancer . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
robson m , im sa , senkus e , et al : olaparib for metastatic breast cancer in patients with a germline brca mutation . oncol 28 : 1145 - 1153 , 2010 n engl j med 377 : 523 - 533 , 2017 23 . 
 contribution of inherited dna - repair gene mutations to hormone - sensitive and castrate - resistant metastatic prostate cancer and implications for clinical outcome siddhartha yadav , md1 ; steven n . 
couch , phd1 ; and manish kohli , md1 purpose to compare the prevalence of germline mutations in metastatic hormone - sensitive prostate cancer ( mhspc ) and metastatic castrate - resistant prostate cancer ( mcrpc ) and assess the impact of mutations on progression to castration resistance and overall survival . methods targeted sequencing of germline dna from 704 men ( 221 at the time of mhspc and 483 at the time of mcrpc ) enrolled in two advanced prostate cancer registries at mayo clinic between 2003 and 2013 was performed for 21 predisposition genes . 
mutations in atm , brca2 , chek2 , fancm , and tp53 were signicantly enriched ( odds ratio greater than 2.0 ) in the metastatic cohorts compared with reference controls . 
2019 by american society of clinical oncology introduction prostate cancer is a leading cause of cancer in men in the united states and worldwide.1 , 2 approximately 30% of patients experience a relapse with advanced disease after curative - intent local therapy for prostate cancer , 3 , 4 and between 5% and 7% of patients are diagnosed initially with advanced stage . 
however , the majority of patients with metastatic hormonesensitive prostate cancer ( mhspc ) eventually stop responding to adt and progress to metastatic castrate - resistant prostate cancer ( mcrpc )  . 
several factors have been implicated in the progression from mhspc to mcrpc , 5 - 8 but the role of mutations in cancer predisposition genes has not been adequately explored . inherited mutations in cancer predisposition genes , such as brca1 / 2 and other dna repair genes , are detected in approximately 4% of patients with localized prostate cancer and less than 1% of the general population.9 in comparison , 7% to 17% of men with mcrpc carry deleterious germline mutations in cancer predisposition genes , 9 - 13 which suggests a contributory role of these mutations in the progression from localized prostate cancer to mcrpc . 
however , the frequency of germline mutations in patients with mhspc is not known , and whether mutation carrier status can predict rapid progression from hormonal sensitivity to castration resistance is unclear . novel drug combinations with adt in patients with mhspc already have demonstrated efcacy in slowing progression to mcrpc and death , 14 - 16 but currently , interventions are not based on the presence of specic genomic aberrations or mutations . 
 yadav et al context key objective to compare the prevalence of germline mutations in metastatic hormone - sensitive prostate cancer ( mhspc ) and metastatic castrate - resistant prostate cancer ( mcrpc ) and assess the impact of mutations on progression to castration resistance and overall survival . knowledge generated in this analysis of 704 patients with metastatic prostate cancer enrolled in a prospective registry , germline mutations were observed in 9.4% of men , 11.8% of men with mhspc , and 8.3% of men with mcrpc . 
no signicant difference was found in time to progression from the hormonesensitive state to the castrate - resistant state or in overall survival between mutation carriers and noncarriers . relevance these ndings have signicant implications for informing prognosis and designing future clinical trials with targeted agents in patients with mhspc and mcrpc . mcrpc state , the targeting of mutations in dna repair genes with poly ( adp - ribose ) polymerase ( parp ) inhibitors , such as olaparib or platinum - based chemotherapy , 17 - 19 has demonstrated clinical benet . 
because the inuence of dna repair gene defects in mhspc on disease progression has not been determined , the use of parp inhibitors or carboplatin in this subcohort has not been explored . 
in this study , we undertook a comprehensive assessment to study the contributions of dna repair gene defects in mhspc and mcrpc and the implications for clinical outcomes . methods patient selection patients with advanced prostate cancer were derived from two prospective registries at mayo clinic . 
a second registry enrolled patients with mhspc and mcrpc between september 2009 and january 2013 . details of both cohorts have been published previously.20 - 23 a total of 826 patients with either mhspc or mcrpc enrolled in either registry were evaluated for inclusion in this study . 
patients without a germline dna sample or available clinical data were excluded from germline sequencing . patients were stratied into mhspc or mcrpc enrollment cohorts on the basis of hormone sensitivity or castration resistance at the time of enrollment . 
mhspc was dened as the development of metastasis as seen on bone imaging scans or computed tomography scans of the abdomen and pelvis , with or without a rising prostate - specic antigen ( psa ) , and no previous adt in the past 2 years . 
mcrpc was dened as the occurrence of either two serial psa rises during continuous adt measured at least 1 week apart with an absolute psa level greater than 2 ng / ml or detection of imaging - based progressive metastasis , whichever came rst . 
high volume of metastasis was dened as the presence of visceral metastases or four or more bone lesions with one or more beyond the vertebral bodies and pelvis per the e3805 study.14 data on initial diagnosis of localized cancer , including date of diagnosis , t stage , n stage , and gleason score , were collected by review of medical records the time of enrollment . 
for the mcrpc cohort , formation on date of mhspc diagnosis , psa and alkaline phosphatase ( alp ) levels , and volume of disease at mhspc diagnosis were collected by medical record review at the time of enrollment . 
this study was approved by the institutional review board at mayo clinic . sequencing and bioinformatics analysis germline dna from peripheral blood mononuclear cells was enriched for the coding regions and consensus splice sites of 21 cancer predisposition genes ( atm , bard1 , brca1 , brca2 , brip1 , chek2 , fancc , fancm , mre11a , mlh1 , msh2 , msh6 , nbn , palb2 , pten , rad50 , rad51c , rad51d , stk11 , tp53 , and xrcc2 ) using a custom ampliconbased qiaseq panel ( qiagen , hilden , germany )  . pooled libraries ( n = 728 ) were subjected to paired - end 150 - base pair sequencing in a single lane of a hiseq 4000 ( illumina , san diego , ca ) , which corresponds to a median coverage of 200 . 
 germline mutations and outcomes in metastatic prostate cancer detected with patterncnv version 1.1.3.27 annotations were provided through the bior toolkit , 28 which leverages dbnsfp version 3.0 , 29 clinvar , 30 clinical annotation of variants , 31 and population frequencies from genome aggregation database ( gnomad ) 32 and exome aggregation consortium33 nonthe cancer genome atlas controls . 
mutations were viewed with vcf - miner.34 interpretation of variants the pathogenicity of germline variants was determined using a framework consistent with established american college of medical genetics and genomics and association for molecular pathology guidelines.35 only patients with likely pathogenic or pathogenic mutations were classied as mutation carriers . 
in case - control association analysis , mutation frequencies by gene were compared with mutation frequencies for non - finnish whites in gnomad.32 large genomic rearrangements in all genes and gnomad lter non - pass variants were excluded from case - control association studies . 
odds ratios ( ors ) and 95% cis for the strength of association with prostate cancer were estimated by fishers exact test . gene - specic mutation enrichment in the mhspc enrollment cohorts relative to the mcrpc cohort were assessed by logistic regression adjusted for age at mhspc diagnosis and reported as ors with 95% cis . 
multivariable analysis for time to progression to mcrpc and overall survival was performed using a cox proportional hazards regression model that included age , initial presentation , gleason score , t and n stage at initial diagnosis , psa and alp level at mhspc diagnosis , volume of metastasis , and mutation status as covariates . 
seventeen patients who did not receive adt despite a diagnosis of metastatic prostate cancer were excluded from analysis of progression from hormone - sensitive stage to castration resistance but were included in the overall survival analysis . all tests were two - sided , and p , .05 was considered to indicate statistical signicance . local versus advanced disease at results of 728 samples subjected to germline sequencing , 17 failed coverage , and six were identied as duplicates ; one patient was excluded because of a diagnosis of neuroendocrine prostate cancer ( data supplement )  . 
the median duration of follow - up from mhspc diagnosis was 71 months for the entire cohort , 53 months for the mhspc cohort , and 77 months for the mcrpc cohort . 
atm , brca2 , chek2 , fancm , and tp53 mutations were signicantly enriched in patients with prostate cancer relative to controls , with ors ranging from 2.8 for chek2 to 15.9 for tp53 ( table 2 )  . 
for the entire cohort , the median time to progression from mhspc to mcrpc was 23.1 months for mutation carriers and 32.5 months for noncarriers ( p = .96 ; fig 1a )  . 
when the mhspc and mcrpc cohorts were analyzed separately , a signicant difference in the rate of progression from mhspc to mcrpc was not observed between mutation carriers and noncarriers in either cohort ( figs 1b and 1c )  . in univariable cox proportional hazards regression analysis , older age at diagnosis of mhspc , metastatic disease at initial presentation , gleason score greater than 7 , higher psa level , elevated alp level , and high volume of metastatic disease were signicant predictors of mhspc to mcrpc progression ( table 3 )  . 
in multivariable cox proportional hazards regression analysis , older age at diagnosis , gleason score greater than 7 , elevated alp level , and high volume of metastasis remained signicant predictors of progression to castration resistance ( table 3 )  . 
on further analysis by enrollment cohort , mutation status was not associated with progression to castration resistance in multivariable models of the mhspc or mcrpc cohorts ( data supplement )  . impact of germline mutations on overall survival ( 87.0% ) from the mcrpc enrollment cohort . 
no difference in overall survival was found from diagnosis of mhspc between patients with and without mutations ( median , 66 v 84 months ; p = .14 ; fig 2a )  . 
on further subset analysis by enrollment cohort , mutation status was not associated with overall survival in multivariable analysis of the mhspc or mcrpc cohorts ( data supplement )  . discussion this study showed that more than 10% of patients in the mhspc state of advanced prostate cancer harbor a germline mutation in one of the predisposition genes associated with the cellular response to dna damage and that the frequency of germline mutations is not signicantly different between patients with mhspc and mcrpc . 
comparison of the rate of progression from metastatic hormone - sensitive prostate cancer ( mhspc ) to metastatic castrate - resistant prostate cancer ( mcrpc ) between mutation carriers and noncarriers . 
this variant also has been noted to be more frequent in patients with lethal prostate cancer compared with low - risk prostate cancer.38 whether other variants in chek2 confer similar prostate cancer risk is unclear . 
for instance , in the study by pritchard et al , more than 50% of patients had a rst - degree relative with cancer , whereas in the study by castro et al , those with brca2 mutations had the greatest association with a family history of cancer . 
although to our knowledge the current study is the largest in terms of sample size among all reported studies , we did not evaluate family history of cancer , which is a limitation when comparing participating populations across different studies . 
 yadav et al with the general population in this study . in a similar comparison , pritchard et al9 found that six genes ( atm , brca1 , brca2 , chek2 , gen1 , and rad51d ) were signicantly enriched in mcrpc . 
fancm is considered a member of the fanconi anemia ( fa ) family of dna repair genes ( online mendelian inheritance in man 609644 ) , a component of the upstream fa pathway that mediates the assembly of the fa core complex , and a regulator of the s - phase checkpoint upon interstrand crosslink - induced dna damage.41 fancm has been associated with an increased risk of breast cancer.42 - 45 in the current study , three of the seven mutations noted in fancm were due to the deletion of exon 8 , which has not been reported previously to be associated with prostate cancer risk , and hence , needs to be validated in future studies . 
the association between germline tp53 mutations and prostate cancer risk is also a novel nding of this study but needs to be interpreted with caution because of the small number of mutation carriers and the potential for ageand / or therapy - related clonal hematopoiesis events , which can be seen in up to one quarter of tp53 mutation carriers.46 we did not attempt to conrm the mendelian inheritance of these tp53 mutations through analysis of dna from secondary tissue sources , 46 which is a limitation of this and other germline tp53 studies . 
based on the results of our study , additional studies should investigate associations between germline tp53 mutations and risk of prostate cancer while also accounting for clonal hematopoiesis events . germline mutation carriers with localized prostate cancer have been reported to have a higher rate of progression to metastatic disease and an overall poorer prognosis.47 - 52 this is also supported by signicant enrichment of mutation carriers among patients with metastatic prostate cancer compared with patients with localized prostate cancer.9 although mutation carriers are more likely to progress from localized prostate cancer to metastatic prostate cancer , our results suggest the rate of progression to castration resistance or death is not affected by mutation carrier status . 
the biologic mechanisms of metastasis and androgen resistance are distinct from each other.53 , 54 genomic analysis of metastatic prostate tumors has demonstrated that mutation or amplication of the androgen receptor gene is the most enriched alteration in mcrpc compared with mhspc tumors , and mutations in dna repair genes are less common.55 that in recent years , several clinical trials evaluated the addition therapeutic agents to adt in early mhspc of other stage , 14 , 15 , 56 - 58 with the goal of slowing down progression to mcrpc and improving overall survival . 
at present , targeted therapies for patients with dna repair defects , such as parp inhibitors , have been studied only in the mcrpc stage.17 our study suggests that future clinical trials with early addition of parp inhibitors or similar drugs to adt in the mhspc stage may be feasible . 
these somatic alterations in dna repair genes can arise during different stages of disease progression as a result of acquired resistance to therapy or as part of tumor evolution59 even in the absence of germline mutations . 
our study did not evaluate somatic mutations in dna repair genes in corresponding tumor material , but such patients are known to respond to parp inhibitors.17 in addition , parp inhibitors may potentially replace adt in a select group of patients with mhspc because of superior adverse effect proles , as is being evaluated in an ongoing phase ii clinical trial of parp inhibitors instead of adt in patients with mhspc.60 because this study was performed using prospective registries from a single institution , it has several strengths compared with similar prior studies . 
in addition , we did not account for treatment effect , although the majority of patients were enrolled before the publication of studies that established preferential use of docetaxel14 or abiraterone in the mhspc setting15 , 58 and were unlikely to receive these treatments outside a clinical trial . 
however , patients may have received these treatments at progression to castration resistance , which can potentially affect the overall survival analysis . finally , we did not take into account somatic mutations in dna repair genes , which can independently affect outcomes . this study demonstrated that approximately 10% of patients with metastatic prostate cancer harbor germline mutations in cancer predisposition genes , and it identied mutations in ve genes ( atm , brca2 , chek2 , fancm , and tp53 ) that are enriched in patients with advanced prostate cancer . 
couch consulting or advisory role : astrazeneca research funding : grail travel , accommodations , expenses : grail , qiagen other relationship : ambry genetics no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
ca cancer j clin 68 : 7 - 30 , 2018 ferlay j , soerjomataram i , dikshit r , et al : cancer incidence and mortality worldwide : sources , methods and major patterns in globocan 2012 . 
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prostate 74 : 820 - 828 , 2014 karantanos t , corn pg , thompson tc : prostate cancer progression after androgen deprivation therapy : mechanisms of castrate resistance and novel therapeutic approaches . 
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prostate 74 : 225 - 234 , 2014 keto cj , aronson wj , terris mk , et al : obesity is associated with castration - resistant disease and metastasis in men treated with androgen deprivation therapy after radical prostatectomy : results from the search database . 
bju int 110 : 492 - 498 , 2012 pritchard cc , mateo j , walsh mf , et al : inherited dna - repair gene mutations in men with metastatic prostate cancer . 
antonarakis es , lu c , luber b , et al : germline dna - repair gene mutations and outcomes in men with metastatic castration - resistant prostate cancer receiving rst - line abiraterone and enzalutamide . 
pomerantz mm , spis ak s , jia l , et al : the association between germline brca2 variants and sensitivity to platinum - based chemotherapy among men with metastatic prostate cancer . 
liu x , wu c , li c , et al : dbnsfp v3.0 : a one - stop database of functional predictions and annotations for human nonsynonymous and splice - site snvs . 
m unz m , ruark e , renwick a , et al : csn and cava : variant annotation tools for rapid , robust next - generation sequencing analysis in the clinical setting . genome med 7 : 76 , 2015 32 . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
castro e , romero - laorden n , del pozo a , et al : prorepair - b : a prospective cohort study of the impact of germline dna repair mutations on the outcomes of patients with metastatic castration - resistant prostate cancer . 
n aslund - koch c , nordestgaard bg , bojesen se : increased risk for other cancers in addition to breast cancer for chek2 * 1100delc heterozygotes estimated from the copenhagen general population study . 
peterlongo p , catucci i , colombo m , et al : fancm c.5791c.t nonsense mutation ( rs144567652 ) induces exon skipping , affects dna repair activity and is a familial breast cancer risk factor . 
neidhardt g , hauke j , ramser j , et al : association between loss - of - function mutations within the fancm gene and early - onset familial breast cancer . 
kiiski ji , tervasm aki a , pelttari lm , et al : fancm mutation c.5791c.t is a risk factor for triple - negative breast cancer in the finnish population . 
na r , zheng sl , han m , et al : germline mutations in atm and brca1 / 2 distinguish risk for lethal and indolent prostate cancer and are associated with early age at death . 
castro e , goh c , olmos d , et al : germline brca mutations are associated with higher risk of nodal involvement , distant metastasis , and poor survival outcomes 51 . 
castro e , goh c , leongamornlert d , et al : effect of brca mutations on metastatic relapse and cause - specic survival after radical treatment for localised in prostate cancer . 
abida w , armenia j , gopalan a , et al : prospective genomic proling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making . 
kyriakopoulos ce , chen yh , carducci ma , et al : chemohormonal therapy in metastatic hormone - sensitive prostate cancer : long - term survival analysis of the randomized phase iii e3805 chaarted trial . 
tombal b , borre m , rathenborg p , et al : enzalutamide monotherapy in hormone - naive prostate cancer : primary analysis of an open - label , single - arm , phase 2 study . 
lancet oncol 15 : 592 - 600 , 2014 james nd , de bono js , spears mr , et al : abiraterone for prostate cancer not previously treated with hormone therapy . 
markowski mc , wang h , sullivan r , et al : phase ii trial of rucaparib ( without adt ) in patients with metastatic hormone - sensitive prostate cancer harboring germline dna repair gene mutations ( triumph )  . 
 integrative molecular analysis of patients with advanced and metastatic cancer verena sailer , md1 ; kenneth wa eng , ms1 ; tuo zhang , phd1 ; rohan bareja , ms1 ; david j . 
pisapia , md1 ; alexandros sigaras , ms1 ; bhavneet bhinder , ms1 ; alessandro romanel , phd2 ; david wilkes , phd1 ; evan sticca , ms1 ; joanna cyrta , md1 ; rema rao , md1 ; sheena sahota , md1 ; chantal pauli , md1 ; shaham beg , md1 ; samaneh motanagh , md1 ; myriam kossai , md1 ; jacqueline fontugne , md1 ; loredana puca , phd1 ; hanna rennert , phd1 ; jenny zhaoying xiang , md1 ; noah greco , mba1 ; rob kim1 ; theresa y . 
in patients with more than one sequenced tumor sample ( n = 146 ) , 84.62% of actionable mutations were concordant . conclusion integrative analysis may uncover informative alterations for an advanced pan - cancer patient population . 
2019 by american society of clinical oncology introduction genomic proling is widely used in cancer care to identify actionable alterations for individual patients within the context of precision medicine ( pm ) .1 however , only 2% to 11% of those patients with sequencing performed receive a genomically matched therapy , which may be a result of the availability and accessibility of clinical trials , 2 - 6 patient factors and comorbidities , disease state or alternative options , or patient preference.5 despite these drawbacks , pm studies continue to provide insights into the molecular underpinnings of cancer . 
we and others have shown that performing whole - exome sequencing ( wes ) and rna sequencing is feasible in a clinical setting and may provide relevant information beyond targeted gene panels in certain settings.3 , 7 , 8 sequencing matched tumor and normal ( germline ) dna has the additional benet of uncovering unforeseen hereditary conditions , including cancer risk mutations . 
in particular , germline dna repair defects ( drds ) are more common than previously anticipated across adult advanced cancer populations.9 - 11 robinson et al12 published their met500 cohort with wes and rna sequencing data from 500 patients with metastatic disease of varied tumor primary and biopsy sites . 
our study , obtained from our own cohort of 759 samples from 515 patients with advanced and metastatic cancer , complements this data set as it adds wes data from approximately the same number of patients . 
 sailer et al context key objective we assessed whether developing a multidimensional precision oncology program is feasible and informative for patients with cancer with advanced disease . knowledge generated we established a comprehensive clinical genomics program for this patient group . 
the rate of clinically relevant alterations across 515 patients with advanced solid tumors was 39% by whole - exome sequencing , which was improved by 16% by adding rna sequencing . 
germline dna was obtained from blood samples ( circulating mononuclear cells ) , buccal swabs , or benign tissue as described previously.3 part of the data presented in this manuscript have already been published.3 , 13 , 15 wes was performed on each patients tumor / matched germline dna pair using previously described protocols.3 we used a clinical - grade wes testexome cancer test version 1approved by new york state department of health ( id# 43032 ) and described in detail in rennert et al.16 this approach allows for assessment of more than 21 , 000 genes through the development and implementation of computational approaches for tumor mutational burden and neoepitope analysis , as well as integration with other data , including rna sequencing , to improve the identication of clinically relevant and actionable alterations . 
to evaluate the concordance of tier 1 and tier 2 alterations between multiple samples from the same patient and to gain high - delity results , a cutoff of 20% for variant allele frequency was used . 
in addition , we developed patientderived organoids from fresh tissues using previously described protocols , 4 , 17 and we used cell lines to functionally validate outlier targetable alterations . wes alterations were categorized on the basis of on their actionability and clinical or biologic relevance.3 alterations in 49 actionable or clinically signicant genes were reported within category 1 , alterations in 508 known cancer - associated genes within category 2 , and somatic alterations of unknown signicance within category 3.3 we developed an open - access , dynamic , web - based pm knowledge base as an interactive online tool where variants are carefully interpreted in the context of tumor type.18 wes results were conveyed to the referring physician in the form of an exome cancer test version 1 report.3 selected cases are presented at a regular , continuing medical education accredited pm tumor board , which discusses sequencing results in the context of a patients history , available literature , and treatment options , including active clinical trials . pathogenic germline ndings were reported to the referring physician if they occurred in any of the genes deemed reportable by the american college of medical genetics and genomics ( acmg ) , 19 and these patients were referred for genetic counseling and results were conrmed by targeted testing in a clinical laboratory improvement amendments / clinical laboratory evaluation programcertied laboratory . study cohort demographic data were obtained through electronic health record search . 
 precision oncology for patients with advanced disease primary site ( 515 patients ) biopsy / resection site ( 759 samples ) breast ( 13 ) pancreas ( 18 ) kidney ( 46 ) soft tissue ( 8 ) brain ( 98 ) lung ( 16 ) hematologic malignancies ( 24 ) colon and / or rectum ( 41 ) bladder ( 57 ) prostate ( 105 ) primary recurrent metastatic brain ( 150 ) liver ( 64 ) bla d d er ( 69 ) b o n e ( 71 ) ly m p h n o d e ( 85 ) c olo n ( 18 ) l u n g ( 44 ) kid n ey ( 26 ) prostate ( 33 ) sample characteristic metastatic primary recurrent 34 - year - old female , er - positive breast carcinoma , mastectomy , brca1 / 2 germline negative chest wall recurrence , er / pr / her2 unknown , excision and radiotherapy no cancer detected metastatic disease seven systemic therapies precision medicine consent liver biopsy , akt1 mutation detected by wes cdk4 / 6 inhibitor ( palbociclib ) liver progress + 3 years + 20 years + 3 years + 1 year + 1 year + 1 year fig 1 . 
the most common somatic alterations were found in tp53 ( 33% ) , cdkn2a ( 11% ) , apc ( 10% ) , kmt2d ( 8% ) , pten ( 8% ) , and brca2 ( 7% ; fig 2 )  . multiple samples three hundred eighty - two spatially and temporally heterogeneous samples from 146 patients underwent wes . 
of these , 185 ( 48.4% ) were metastatic , 153 ( 40.1% ) were primary , and 44 ( 11.5% ) were recurrent tumor samples . most samples were paired primary and metastatic tumors , and concordance of alterations between primary and metastatic samples in clinically informative genes is shown in figure 3 . 
paired primarymetastatic tumor samples from 59 patients were the most frequent combination . spatially and / or temporally heterogeneous metastases and primary tumors from 35 and 29 patients , respectively , also underwent sequencing . 
 ( e ) different kras mutations in two morphologically similar lung cancer samples from the same patient , thus conrming two separate primary tumors . this cohort ( data supplement )  . 
the most frequently mutated genes were chek2 ( 11 patients ) , brca2 ( nine patients ) , brca1 ( nine patients ) , msh6 ( nine patients ) , and atm ( four patients ; fig 2 )  . 
in likely pathogenic variants in 38 addition , 44 additional patients in msh6 ( 14 cases ) ; apc ( seven cases ) ; chek2 ( ve cases ) ; pole , pms2 , msh2 brca1 , and atm ( three cases each ) ; and tp53 , cdh1 , and brip1 ( one case each ) were discovered in our cohort . the prevalence of drd in our cohort of patients with metastatic prostate cancer was 14.3% , with brca2 mutations being the most frequent variants ( data supplement )  . pathogenic germline drds were found in 9.2% of patients with primary brain tumors . 
we did not identify pathogenic mutations involving mismatch repair genes , which have been described in primary brain tumor patients , in particular as biallelic losses.25 chek2 was altered in four cases , including one medulloblastoma . 
 ( b ) high frequency of germline mutations in breast , prostate , and lung tumors is observed . germline drd defects , 12 had received platinum - based chemotherapy with follow - up available . 
an additional targetable ncoa4ret fusion , which has been described in papillary thyroid cancer , nonsmall - cell lung cancer , and colorectal cancer , was found in a brain metastasis of a patient with unknown primary.28 rna sequencing rna sequencing was performed when sufcient fresh frozen tumor tissue was available after wes . 
of these 89 patients , 50 did not harbor a targetable genomic alteration identied by wes , resulting in an increase in the rate of actionable alteration detection of approximately 15% . 
we conrmed the drug sensitivity of select outlier genes using cell line experiments compared with randomly selected drugs ( fig 5 )  . nine novel fusions in a variety of cancer types were detected . 
a novel rbm47 - cdk12 gene fusion was found in a prostate cancer bone metastasis , which was conrmed organoids part of the program was the development of patient - derived organoids from patient biopsies for high - throughput drug screening.4 altogether 60 organoids were developed from 98 patients with an overall success rate of 61% . 
a pathogenic msh6 mutation was detected in a 26 - year - old patient with metastatic breast carcinoma who had undergone previous outside testing for brca1 / 2 germline mutations with a negative result . 
other potentially signicant variants in drd genes , such as palb2 , would have been missed as well.30 this case underlines the importance of multigene panel or wes testing in patients not only with suspected hereditary cancer but also in those , especially young patients , with metastatic disease to detect underrecognized germline alterations.31 tumor evolution and clonality . 
a deleterious effect has been predicted for this variant.33 in a previously published analysis of 13 uterine carcinosarcomas analyzed by targeted sequencing , eight cases demonstrated 100% identical mutations in both the carcinoma and sarcoma part.34 in contrast , we observed an early divergence with only the one pten mutation of 54 nonsynonymous shared mutations . 
this case again demonstrates the importance of using next - generation sequencing to correctly identify synchronous primary tumors.39 another patient with metastatic neuroblastoma was conrmed to have an activating alk mutation ( r1275q ) in both primary tumor and bone marrow metastasis . 
the patient has had stable disease for 13 months on therapy with sequential alk inhibitors40 ( fig 3 )  . discussion we have established a pm program for patients with advanced cancer using tumor / normal wes and integrative molecular proling to detect genomic and other actionable alterations , improve clinical decision making , and study tumor evolution in a pan - cancer cohort . 
the patient population in our study is distinct from several reported studies in that our focus was on the evaluation of advanced tumors.41 , 42 the majority of patients ( 70.8% ) presented the time of with metastatic or recurrent disease at enrollment . whereas publicly accessible molecular data for several tumor types are available , both for primary and metastatic cancers , 43 , 44 these specimens are rarely matchedthat is , obtained from the same patient.45 our cohort of patients with locally advanced and metastatic cancer allowed for the collection of multiple matched , often primary and metastatic samples , resulting in a unique feature of this cohort : genomic data from spatially and / or temporally heterogeneous , matched tissue samples were available in 146 patients . 
of clinical importance is the nding that almost 85% of category 1 alterations were shared between multiple samples from the same patient . these results are in concordance with published data in specic cancer types . 
in one study , when comparing actionable mutations between presurgery biopsies and resected specimen in patients with nonsmall - cell lung cancer , the concordance rate was found to be 79%.46 similar ndings have been reported for primary and recurrent breast cancer , with 86.6% of mutations and 85.5% of scnas being concordant.47 our data conrm that it may reasonable to select the most accessible location or even archival material from the primary tumor for molecular analysis for certain cancer types.48 , 49 new research indicates that pathogenic germline mutations are more frequently found in patients with advanced cancer , 9 , 12 and our data conrm this . 
germline mutations that involve the dna repair pathway , found in 10.7% of our patients , are predictive of response to parp inhibitors and platinum - based therapy and have important familial plications for cancer screening.50 family history was indicative of a heritable component in only one half of these patients . 
this fusion might result in the loss of cdk12 activity , which has recently been described to delineate a distinct immunogenic subtype of metastatic castrationresistant prostate cancer.51 in our study , wes was prioritized over rna sequencing whenever tissue availability was of concern . 
biopsies in our study were usually performed for diagnostic purposes in the context of clinical care , hence the lower availability of fresh frozen tissue for additional rna sequencing . targeted sequencing of cancer - related genes offers several advantages over wes , including deeper coverage , quicker turnaround time , lower cost , and fewer requirements for an elaborate computational pipeline . 
here , we show that wes and rna sequencing may provide an additional and information in certain settings , complimentary layer of particularly for patients with advanced cancer who experience progression after standard therapies . 
wes also considers the rapidly expanding spectrum of actionable alterations , including alterations for which targeted treatment may not be available at the time of analysis , but for which clinical trials might be planned . 
in addition , whereas targeted nextgeneration sequencing testing of somatic dna are sometimes ordered as part of clinical care , using germline dna as normal control for wes necessitates securing informed consent . implementing - omic data into clinical care requires an interdisciplinary teagenomic data and its interpretation in the context of tumor type and primary site must be easily accessible to enable clinicians to integrate the data into everyday patient care . 
 precision oncology for patients with advanced disease one limitation of our study is the lack of uniformity of the cohort in terms of tumor type and therapy , which prevents us from making generalized statements about treatment response . 
this data set also reports on a large number of matched temporally and spatially heterogeneous samples , highlighting the concordance of actionable alterations in different samples . as other pm trials have shown , uncovering genomic alterations may not be sufcient in identifying actionable alterations . 
contributed equally to this work and share senior authorship . support supported by the englander institute for precision medicine of weill cornell medicine and new york presbyterian , the translational research program of the department of pathology and laboratory medicine at weill cornell medicine . 
macdonald , eleni andreopoulou , olivier elemento , himisha beltran provision of study materials or patients : noah greco , rob kim , bishoy m . faltas , eleni andreopoulou , linda t . 
pisapia , david wilkes , joanna cyrta , sheena sahota , chantal pauli , shaham beg , samaneh motanagh , myriam kossai , jacqueline fontugne , jenny zhaoying xiang , noah greco , rob kim , theresa y . 
pisapia , alexandros sigaras , bhavneet bhinder , alessandro romanel , david wilkes , evan sticca , rema rao , shaham beg , loredana puca , rob kim , mirjam blattner - johnson , eleni andreopoulou , linda t . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . alexandros sigaras employment : weill cornell medical college loredana puca employment : petra pharma corporation bishoy m . 
faltas honoraria : digital science press publications research funding : eli lilly david rickman research funding : janssen oncology eleni andreopoulou honoraria : astrazeneca , sirtex , svb leerink , abbvie , eisai , nanostring technologies consulting or advisory role : astrazeneca , sirtex , svb leerink , abbvie , eisai , nanostring technologies speakers bureau : r - pharm us travel , accommodations , expenses : astrazeneca , sirtex , svb leerink , abbvie , eisai , nanostring technologies kevin holcomb research funding : fujirebio diagnostics expert testimony : johnson & johnson linda t . 
vahdat honoraria : polyphor , r - pharm , athenex , seattle genetics , osmol therapeutics consulting or advisory role : berg pharma speakers bureau : eisai research funding : polyphor ( inst ) , immunomedics ( inst ) , seattle genetics ( inst ) patents , royalties , other intellectual property : patent pending on the application for bmd progenitor cells ( inst ) douglas s . 
 sailer et al koen van besien stock and other ownership interests : hemogenyx consulting or advisory role : hemogenyx , actinium pharmaceuticals , cellectis , tessa therapeutics research funding : miltenyi biotec , actinium pharmaceuticals , juno therapeutics , fate therapeutics christopher e . 
ocean consulting or advisory role : celgene , tyme speakers bureau : daiichi sankyo travel , accommodations , expenses : daiichi sankyo ana molina honoraria : american society of clinical oncology consulting or advisory role : eisai , exelixis , novartis , janssen oncology manish a . 
shah consulting or advisory role : astellas pharma , eli lilly research funding : gilead sciences ( inst ) , merck ( inst ) , boston biomedical ( inst ) , oncolys biopharma ( inst ) , bristol - myers squibb ( inst ) david m . 
nanus consulting or advisory role : genentech research funding : novartis ( inst ) , boehringer ingelheim ( inst ) , zenith epigenetics ( inst ) qiulu pan employment : caris life sciences stock and other ownership interests : caris life sciences francesca demichelis patents , royalties , other intellectual property : co - inventor on a patent led by the university of michigan and brigham and womens hospital covering the diagnostic and therapeutic elds for ets fusions in prostate cancer , diagnostic eld licensed to gen - probe scott t . 
tagawa consulting or advisory role : medivation , astellas pharma , dendreon , janssen oncology , bayer , genentech , endocyte , immunomedics , karyopharm therapeutics , abbvie , tolmar , qed , amgen , sano , pzer research funding : eli lilly ( inst ) , sano ( inst ) , janssen oncology ( inst ) , astellas pharma ( inst ) , progenics ( inst ) , millennium pharmaceuticals ( inst ) , amgen ( inst ) , bristol - myers squibb ( inst ) , dendreon ( inst ) , rexahn pharmaceuticals ( inst ) , bayer ( inst ) , genentech ( inst ) , newlink genetics ( inst ) , inovio pharmaceuticals ( inst ) , astrazeneca ( inst ) , immunomedics ( inst ) , novartis ( inst ) , aveo ( inst ) , boehringer ingelheim ( inst ) , merck ( inst ) , stem centrx ( inst ) , karyopharm therapeutics ( inst ) , abbvie ( inst ) , medivation ( inst ) , endocyte ( inst ) , exelixis ( inst ) , clovis oncology ( inst ) travel , accommodations , expenses : sano , immunomedics , amgen wei song employment : genentech ( i ) , cytokinetics ( i ) honoraria : foundation medicine , loxo consulting or advisory role : foundation medicine , loxo juan miguel mosquera research funding : personal genome diagnostics travel , accommodations , expenses : personal genome diagnostics mark a . 
nature 537 : s63 , 2016 beltran h , eng k , mosquera jm , et al : whole - exome sequencing of metastatic cancer and biomarkers of treatment response . 
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cell 163 : 1011 - 1025 , 2015 isaka m , serizawa m , kenmotsu h , et al : comparison of clinically relevant mutation proles between preoperative biopsy and corresponding surgically resected specimens in japanese patients with non - small - cell lung cancer by amplicon - based massively parallel sequencing . 
kang hj , hwangbo b , lee js , et al : comparison of epidermal growth factor receptor mutations between metastatic lymph node diagnosed by ebus - tbna and primary tumor in non - small cell lung cancer . 
 response to selective ret inhibition with loxo - 292 in a patient with ret fusion - positive lung cancer with leptomeningeal metastases robin guo , md1 ; mark schreyer , ms1 ; jason c . 
hyman , md1 , 4 ; and alexander drilon1 , 4 introduction the development of leptomeningeal metastases is a poor prognostic factor in patients with advanced cancers.1 - 3 in nonsmall - cell lung cancers ( nsclcs ) , median overall survival of patients from the diagnosis of leptomeningeal disease is 1 to 2 months without treatment and up to 8 months with systemic therapy.4 - 6 furthermore , patients with leptomeningeal disease have historically had limited access to novel therapies in clinical trials . 
recent efforts from many groups , including the european society for medical oncology and the us food and drug administration ( fda ) , have encouraged the inclusion of patients with leptomeningeal metastases in clinical trials , in addition to promoting standardization of intracranial response assessments.7 - 9 these efforts are crucial given that many investigational agents have substantial cns activity and may improve outcomes in driver - positive cancers with leptomeningeal involvement.5 , 10 ret fusions are actionable oncogenic drivers that are identied in 1% to 2% of nsclcs.11 , 12 to date , chemotherapy and / or immunotherapy remain the only approved systemic therapies for these cancers . 
although these agents were found to be active in these patients , outcomes are modest a subset of compared with targeted therapies in other driverpositive lung cancers , and intracranial activity is poor.13 , 14 selective ret inhibitors currently in development , such as loxo - 292 and blu - 667 , have improved outcomes for patients with ret fusion - positive cancers because of increased potency and less offtarget toxicity.15 , 16 in september of 2018 , loxo - 292 received breakthrough therapy designation from the fda for treatment of patients with metastatic ret fusion - positive nsclcs ( as well as ret fusion - positive thyroid cancers and ret - mutant medullary thyroid cancer )  . 
in addition , conrmed intracranial responses and durable disease control have been achieved in patients with brain metastases in an ongoing phase i / ii trial of loxo - 292 for patients with ret fusion - positive cancers.15 its activity in leptomeningeal disease , however , has not previously been characterized . 
computed and positron - emission tomography imaging revealed a hypermetabolic 4.8lobe mass , mediastinal and hilar cm right adenopathy , and osseous metastases involving l1 , the sacrum , and the left anterolateral sixth rib . 
magnetic resonance imaging ( mri ) of the brain showed three subcentimeter enhancing foci in the right precentral lobe . gyrus , right parietal endobronchial biopsy of an r4 lymph node revealed adenocarcinoma with signet ring cell features ( fig 1a )  . tumor cells were positive for ttf - 1 and negative for p40 by immunohistochemistry . 
broad , hybrid capture based next - generation sequencing using the memorial sloan kettering integrated mutation proling of actionable cancer targetsmsk - impactand illumina hiseq 2500 ( illumina , san diego , ca ) 17 identied an eml4 - ret fusion ( fig 1b ) in addition to a tp53 p.p142tfs * 5 frameshift mutation . 
this eml4 - ret fusion was conrmed using a targeted rna - based anchored multiplex polymerase chain reaction archer fusion assay ( archer , boulder , co )  . with identication of the ret fusion , the patient was treated with the investigational anti - ret multikinase inhibitor rxdx - 105.18 , 19 although a conrmed partial response was initially achieved ( a near - complete response in her brain metastases ) , her course was marked by isolated asymptomatic intracranial progression requiring multiple radiation treatments . 
 guo et al eml4 ( nm_019063.3 ) ret ( nm_020630.4 ) 8 9 10 1112 13 14 15 16 1718 1912 13 1415 1617 18 ence eml4 ( + ) nm_019063.3|exon : 19 ret ( + ) nm_020630.4|exon : 12 fig 1 . 
 ( a ) a hematoxylin and eosinstained section from a cell block of a ne - needle aspiration specimen from a lower paratracheal lymph node conrmed a diagnosis of lung adenocarcinoma . 
clusters of malignant epithelial cells with signet - ring cell morphology ( eccentrically placed nuclei , focally prominent nucleoli , and abundant amount of cytoplasm containing grayish - blue mucin ) are shown . 
 ( b ) an in - frame ret fusion containing the ret tyrosine kinase domain was identied in extracted dna from this sample by broad , hybrid capturebased next - generation sequencing using the memorial sloan kettering integrated mutation proling of actionable cancer targetsmsk - impact and illumina hiseq 2500 ( illumina , san diego , ca )  . exon 19 of the 5 ( cid : 1 ) upstream gene partner eml4 was fused to exon 12 of 3 ( cid : 1 ) ret . 
this eml4 - ret fusion was conrmed using an rna - based anchored multiplex polymerase chain reaction ( archer , illumina miseq [ archer , boulder , co ] )  . four months later , the patient developed symptomatic progression of brain metastases and new leptomeningeal disease . 
she presented with left facial , tongue , and upper extremity tingling and worsening neck pathese symptoms were deemed to be secondary to leptomeningeal disease that was identied radiologically in the right hemisphere , predominantly in the right parietal lobe ( fig 2a ; top panel ) , recognizing that nonradiologically apparent disease was likely present in other areas.8 multiple brain metastases had also increased ( largest measuring 2.7 cm in the right frontal lobe ; fig 2a ; bottom panel )  . 
a cant lumbar puncture was recommended , but the patient declined ; a brain biopsy to potentially determine the mechanism of resistance to rxdx - 105 was not deemed safe . extracranial imaging again showed no evidence of disease . given that the patient was highly symptomatic with progressive symptoms , a single - patient use protocol of loxo - 292 was approved by the fda and institutional review board . 
magnetic resonance imaging axial brain images are shown ( a ) at baseline , ( b ) 5 weeks , and ( c ) 21 weeks after the initiation of loxo - 292 therapy in a patient with an eml4ret fusion - positive lung cancer . 
a representative right superior medial and right lower frontal intraparenchymal metastasis ( green arrows ) regressed with loxo - 292 therapy , along with several other metastases followed on serial intracranial response by recist ( response evaluation criteria in solid tumors ) v1.1 and a complete response in leptomeningeal disease by response assessment in neuro - oncology were achieved . 
a conrmed partial patient provided written informed consent before enrollment , and loxo - 292 was administered orally at 160 mg twice daily . this dose was selected based on preliminary safety and efcacy results from an ongoing phase i / ii trial of the drug ( clinicaltrials.gov identier : nct03157128 )  . imaging assessments ( mri of the brain and computed tomography of the chest , abdomen , and pelvis ) were performed every 8 weeks . response was assessed by recist ( response evaluation criteria in solid tumors ) version 1.1.20 response of leptomeningeal metastases was assessed in accordance with response assessment in neuro - oncology criteria.8 additional volumetric three - dimensional imaging was performed on subsequent scans ( sloan kettering advanced imaging lab , sail ; figs 3b and 3c )  . a clinical response to therapy was achieved within the rst week of therapy , with improvement and subsequent resolution of the patients neurologic symptoms . 
in addition , loxo - 292 therapy achieved complete resolution of leptomeningeal in neuroenhancement , with a response assessment oncology leptomeningeal score dropping from 1 at baseline to 0 at 8 weeks . 
volumetric assessment revealed a continued decrease in the total volume of signicant intracranial disease ( leptomeningeal and parenchymal ) , with a maximal shrinkage of 65% ( from 20.1 cm3 at baseline to 7 cm3 ) at 5 months ( fig 3c )  . the patient continues to receive therapy with loxo - 292 at 10.8 months , with ongoing radiologic disease control and no neurologic symptoms . 
volumetric three - dimensional magnetic resonance imaging analyses were performed on serial imaging performed at ( a ) baseline , ( b ) 5 weeks , and ( c ) 21 weeks . 
maximal volumetric disease regression of 65% was achieved at 21 weeks in the graph of total volume over time on loxo - 292 therapy as shown in the bottom panel . 
in nsclcs with leptomeningeal metastases , there is no consensus on the use of wholebrain radiotherapy , because it has not been shown to consistently improve survival.1 , 3 although systemic chemotherapy with more contemporary regimens ( including pemetrexed and / or bevacizumab ) and intrathecal chemotherapy have been shown to improve outcomes in select series , the development of new agents with higher response rates and more durable disease control continues to represent an unmet need for many patients.4 , 6 this report represents the rst description , to our knowledge , of leptomeningeal metastases responding to any systemic therapy in a patient with a ret fusion - positive cancer . 
a brisk and durable ongoing response to loxo - 292 was achieved in a patient with a ret fusion - positive lung cancer who had notable disease progression while 4 2019 by american society of clinical oncology receiving a prior multikinase inhibitor and multiple prior stereotactic radiosurgery treatments . 
in preliminary data from trial ( clinicaltrials.gov identier : an ongoing phase i / ii nct03157128 ) , all four patients with untreated measurable parenchymal metastases had conrmed intracranial responses to therapy accompanied by overall disease control.15 durable intracranial and extracranial disease control was likewise established in several other patients with untreated nonmeasurable brain metastases before loxo - 292 therapy . the activity of loxo - 292 in the cns can be attributed to several factors . 
the drug is active preclinically , with oral dosing in an orthotopic mouse model of a ret fusionpositive patient - derived tumor implanted into the brain.21 , 22 its potency and selectivity for ret are also likely contributory . 
using a highly active agent in the cns is crucial in ret fusion - positive lung cancers , because close to 25% of patients present with intracranial disease at baseline , whereas the lifetime prevalence of brain metastases approaches 50%.14 in addition , loxo - 292 was designed to target potential resistance mechanisms that can emerge from prior multikinase inhibitor use , such as ret v804m / l gatekeeper substitutions . 
 response to loxo - 292 in ret - rearranged leptomeningeal disease fusions are also identied in papillary thyroid , anaplastic thyroid , colorectal , pancreatic , and breast cancers ; spitzoid neoplasms ; and chronic myeloproliferative neoplasms.11 somatic and germline - activating ret mutations are likewise actionable drivers of oncogenesis that are identied in medullary thyroid cancers and potentially other malignancies.33 although the frequency at which intracranial metastases present is lower for many of these other cancers compared with nsclcs , metastatic disease in the cns can occur in some cases.34 in conclusion , selective ret inhibition with loxo - 292 achieved a clinically meaningful and conrmed response in a patient with a ret fusion - positive lung cancer with leptomeningeal disease and heavily pretreated brain metastases . 
although additional conrmation of this activity will help elucidate overall intracranial disease outcomes , this report underscores the potential of selective ret inhibition as a means of treating and preventing the occurrence of disease in the cns in patients with ret - dependent cancers of any histology . affiliations 1memorial sloan kettering cancer center , new york , ny 2loxo oncology , stamford , ct 3new york university langone medical center , new york , ny 4weill cornell medical college , new york , ny s . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . dahlia henry employment : loxo stock and other ownership interests : loxo , allergan , axovant sciences , palatin technologies mark g . 
kris consulting or advisory role : astrazeneca , regeneron , pzer travel , accommodations , expenses : astrazeneca , genentech other relationship : memorial sloan kettering cancer center robert j . 
young stock and other ownership interests : agios , alexion pharmaceuticals , biogen , celgene , gilead sciences , karyopharm therapeutics , spark therapeutics , regeneron , stemline therapeutics , vertex consulting or advisory role : agios , puma biotechnology , nordicneurolab , icon clinical research research funding : agios ( inst ) david m . 
future oncol 14 : 391 - 407 , 2018 omuro am , kris mg , miller va , et al : high incidence of disease recurrence in the brain and leptomeninges in patients with nonsmall cell lung carcinoma after response to getinib . 
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j thorac oncol 11 : 1962 - 1969 , 2016 park jh , kim yj , lee jo , et al : clinical outcomes of leptomeningeal metastasis in patients with non - small cell lung cancer in the modern chemotherapy era . lung cancer 76 : 387 - 392 , 2012 kim es , bruinooge ss , roberts s , et al : broadening eligibility criteria to make clinical trials more representative : american society of clinical oncology and friends of cancer research joint research statement . 
neuro - oncol 19 : 484 - 492 , 2017 le rhun e , weller m , brandsma d , et al : eano executive board and esmo guidelines committee : eano - esmo clinical practice guidelines for diagnosis , treatment and follow - up of patients with leptomeningeal metastasis from solid tumours . 
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drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 14 . 
oxnard gr , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer : an update from asco 2018 . 
subbiah v , taylor m , lin j , et al : highly potent and selective ret inhibitor , blu - 667 , achieves proof of concept in a phase i study of advanced , ret - altered solid tumors . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
drilon ae , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
yang jc - h , cho bc , kim d - w , et al : osimertinib for patients ( pts ) with leptomeningeal metastases ( lm ) from egfr - mutant nonsmall cell lung cancer ( nsclc ) : updated results from the bloom study . 
reungwetwattana t , nakagawa k , cho bc , et al : cns response to osimertinib versus standard epidermal growth factor receptor tyrosine kinase inhibitors in patients with untreated egfr - mutated advanced nonsmall - cell lung cancer . 
wu yl , ahn mj , garassino mc , et al : cns efcacy of osimertinib in patients with t790m - positive advanced nonsmall - cell lung cancer : data from a randomized 28 . 
costa db , shaw at , ou sh , et al : clinical experience with crizotinib in patients with advanced alk - rearranged nonsmall - cell lung cancer and brain phase iii trial ( aura3 )  . 
gadgeel s , peters s , mok t , et al : alectinib versus crizotinib in treatment - naive anaplastic lymphoma kinase - positive ( alk + ) non - small - cell lung cancer : cns efcacy results from the alex study . 
shaw at , kim tm , crin `o l , et al : ceritinib versus chemotherapy in patients with alk - rearranged non - small - cell lung cancer previously given chemotherapy and crizotinib ( ascend - 5 ) : a randomised , controlled , open - label , phase 3 trial . 
camidge dr , kim dw , tiseo m , et al : exploratory analysis of brigatinib activity in patients with anaplastic lymphoma kinase - positive nonsmall - cell lung cancer and brain metastases in two clinical trials . 
solomon bj , besse b , bauer tm , et al : lorlatinib in patients with alk - positive non - small - cell lung cancer : results from a global phase 2 study . 
 total number of alterations in liquid biopsies is an independent predictor of survival in patients with advanced cancers peter vu , md1 ; yulian khagi , md1 ; paul riviere , bs1 ; aaron goodman , md2 ; and razelle kurzrock , md1 purpose studies have demonstrated an association between quantity of circulating tumor dna ( ctdna ) and poorer survival . 
our ndings suggest that the total number of alterations in plasma may be an indicator of more aggressive tumor biology and therefore poorer survival . jco precis oncol 4 : 192 - 201 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction five - year survival rates are incredibly variable among cancer types , ranging from more than 90% in prostate cancer to less than 8% in pancreas cancer , and depend heavily on clinical and pathologic stage.1 although repeat tissue biopsies during the course of treatment or at the time of progression may provide clinically important information , such biopsies are not routinely performed because they can be technically difcult , time consuming , medically invasive , and lead to complications . 
however , liquid biopsies , or cell - free dna ( cfdna ) obtained from blood plasma that contains fragments of circulating tumor dna ( ctdna ) shed from tumor cells into the bloodstream , can identify new actionable alterations and be performed repeatedly with minimal procedural risk.2 - 5 ctdna can then be analyzed using technologies such as digital polymerase chain reaction to detect specic known somatic variants ( eg , egfr t790m ) or next - generation sequencing ( ngs ) that uses massive parallel sequencing to detect up to thousands of somatic and germline alterations in a single run.6 in addition , genomic alterations found on liquid biopsies are often concordant with alterations found on tissue biopsy when obtained within close proximity to one another.7 - 9 a number of studies have demonstrated that there is an association between higher amounts of cfdna or ctdna and poorer survival , perhaps because percent ctdna ( %ctdna ) correlates with tumor burden.10 , 11 for the most part , these reports dichotomized the level of cfdna or ctdna at a cut - point ( often but not always at approximately 5% or 10% ctdna ) .10 , 12 - 18 in the case of surgical candidates , the cut - points may be lower . 
eligible patients included those who had solid tumor malignancies , never received immunotherapy treatment , and were evaluable for clinical correlations , including overall survival ( os ) from ctdna collection date . 
immunotherapytreated patients were omitted because a correlation with blood or tissue tumor mutational burden has been associated with better immunotherapy response and might therefore alter the survival curve.19 , 20 patients with amplications only in ctdna were omitted because the %ctdna for amplications could not be determined . 
in addition to os evaluation , patients data were also collected and analyzed for %ctdna ; the alteration with the highest allele fraction was calculated from all alterations , including variants of unknown signicance ( vuss ) , total number of vuss , and total number of alterations ( which included vuss )  . 
all values for the total number of ctdna alterations and the number of vuss were corrected for the length ( kilobase pairs [ kbp ] ) of dna sequenced based on the date sequencing was performed and multiplied by 100 ( appendix table a1 )  . 
all data were analyzed from the time of ctdna collection from plasma ( two 10 - ml blood tubes )  . this ctdna assay has a sensitivity and specicity of  . 
hazard ratios ( hrs ) for survival were calculated by comparing os above and below cutoffs and performed from the time of ctdna collection ; dichotomization for each variable ( ie , total number of alterations , total number of vuss , %ctdna ) was performed at the median . 
multivariate analyses were conducted using the wald 2 test from a cox proportional hazards model that included all variables with p .05 in univariate analyses ( ie , sex , age , total number of alterations , %ctdna ) , with the exception of vuss because these alterations are already encompassed within the total number of alterations variable . 
associations between %ctdna and total number of alterations were determined using spearmans rank - order correlation . bootstrapping using random sampling with replacement ( n = 1 , 000 bootstrap samples ) and multiple logistic regression analysis were performed , permitting the data of the sample study to be used as a surrogate for a larger population to validate the model . 
intermediate to high %ctdna was dichotomized at 5% because it had been found to be signicant in prior studies.10 the %ctdna for each patient was calculated using the alteration with the highest allele fraction , including variants of unknown signicance validation cohort , as was the case in our study.22 statistical analyses were carried out using prism version 7.0 ( graphpad , san diego , ca ) and r version 3.5 ( r foundation for statistical computing , vienna , austria )  . results patient characteristics this study included 418 patients who had ngs performed on plasma - derived ctdna and did not receive immunotherapy treatment . 
after correcting for the kbp length of dna sequenced for each sample , the median total number of ctdna alterations ( including vuss ) per patient was 1.46 ( range , 0 - 78.8 ) ; the median total number of vus alterations per patient was 0.66 ( range , 0 - 64.2 ) ; and the median %ctdna was 0.4% ( range , 0% - 80.3% ; table 1 )  . 
 total number of alterations in liquid biopsies is prognostic regression model showed that age , sex , and the total number of alterations were independently prognostic for survival ( table 1 )  . 
among these characteristics , only total number of alterations was signicantly associated with survival ( p , .0001 ; table 1 )  . discussion liquid biopsies have been incorporated into clinical practice as a means to obtain noninvasive molecular proling to identify specic oncogenic driver mutations or other alterations that can guide treatment selection . 
in this study , we evaluated the relationship between the total number of alterations and the %ctdna detected by liquid biopsy and survival outcomes in 418 patients with advanced cancers . 
in addition , we intentionally excluded patients who subsequently received immunotherapy treatment , because several studies have suggested that the use of immune checkpoint inhibitors may alter the survival curve in patients with increased tumor mutational burden.19 , 20 , 23 we demonstrate that both the total number of alterations and the %ctdna have prognostic value and correlate with one another , but only an intermediate to high ( 1.46 ) total number of alterations / kbp ( and not high %ctdna ) was independently associated with worse survival outcomes in multivariate analysis in patients with gi tumors ( table 2 ) , as well as in patients with a diverse group of advanced cancers ( table 1 )  . 
it is also plausible that the higher number of alterations and accompanying aggressive biology results in a higher tumor burden that yields a higher %ctdna ( rather than vice versa )  . a strength of our study is that we used sequencing technology that allows for the detection of %ctdna at a low level with high sensitivity and high specicity.21 , 24 in comparison , some prior studies have used low - depth sequencing , which is less capable of detecting ctdna . 
as a result , these studies were only able to conclude that the presence of ctdna was associated with worse outcomes compared with the absence of detectable ctdna.14 , 18 , 25 , 26 indeed , yang et al27 proposed that the presence or absence of ctdna should be added to the tnm staging classication of tumors because it has diagnostic , therapeutic , and prognostic value . 
when greater depth of ctdna sequencing was used , prior studies have reported that %ctdna is correlated with worse survival and also with increased tumor volume.10 , 11 , 14 we also demonstrated that %ctdna correlates with survival measured from the time of blood draw ( fig 1 ) , which suggests that the association between %ctdna and outcomes may be more reective of tumor burden . limitations to our ndings , given the there are several retrospective nature of the analysis . 
although our study used a relatively large sample of 418 patients , we included a diverse group of advanced cancers and , therefore , our ndings may not be applicable to certain tumor types . despite this , the variety of tumor types in our study may make our ndings more generalizable across advanced total no . 
in addition , 112 patients in this study had no detectable %ctdna , which may be due to low disease burden or due to limitations of the ctdna sequencing technique . 
it should also be noted that there was a different number of subgroups in the analysis of %ctdna and number of ctdna alterations ; hence , the conclusion that the total number of alterations and %ctdna have prognostic value and correlate with one another but that only the total number of alterations was independently associated with survival outcomes will need to be further examined and validated . 
also , we do not know whether this patient population is comparable with those who were not analyzed for ctdna because physicians chose not to perform the analysis or with patients who were lost to follow - up early and hence were inevaluable . 
finally , patients had a diverse array of prior treatments , some of which could have confounded the results ; patients treated with immunotherapy were excluded because cancers with higher mutational burden / number appear to do better on this modality . in conclusion , to our knowledge , this is the rst demonstration that the total number of alterations and %ctdna are highly correlated and have prognostic value . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . support supported in part by the joan and irwin jacobs fund and by national cancer institute grant no . 
 total number of alterations in liquid biopsies is prognostic aaron goodman consulting or advisory role : mitsubishi tanabe pharma , gerson lehrman group , jazz pharmaceuticals , speakers bureau : seattle genetics razelle kurzrock leadership : curematch stock and other ownership interests : curematch , idbydna , soluventis , actuate therapeutics , loxo , xbiotech , neo - med , roche , gaido , soluventis , pzer , merck speakers bureau : roche research funding : guardant health ( inst ) , sequenom ( inst ) , merck serono ( inst ) , genentech ( inst ) , pzer ( inst ) , foundation medicine ( inst ) , incyte ( inst ) , konica minolta ( inst ) , grifols ( inst ) , omniseq ( inst ) , debiopharm group ( inst ) , boerhinger ingelheim ( inst ) no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
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ai b , liu h , huang y , et al : circulating cell - free dna as a prognostic and predictive biomarker in non - small cell lung cancer . 
baumgartner jm , raymond vm , lanman rb , et al : preoperative circulating tumor dna in patients with peritoneal carcinomatosis is an independent predictor of progression - free survival . 
mehrotra m , singh rr , loghavi s , et al : detection of somatic mutations in cell - free dna in plasma and correlation with overall survival in patients with solid 17 . 
stover dg , parsons ha , ha g , et al : association of cell - free dna tumor fraction and somatic copy number alterations with survival in metastatic triple - negative 19 . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free 22 . 
j clin oncol 36 : 543 - 553 , 2018 ther 16 : 2598 - 2608 , 2017 cancer res 23 : 5729 - 5736 , 2017 circulating tumor dna . 
lecomte t , berger a , zinzindohou e f , et al : detection of free - circulating tumor - associated dna in plasma of colorectal cancer patients and its association with 27 . 
yang m , forbes me , bitting rl , et al : incorporating blood - based liquid biopsy information into cancer staging : time for a tnmb system ? ann oncol prognosis . 
intermediate to high %ctdna was dichotomized at 5% because it had been found to be signicant in prior studies.10 the %ctdna for each patient was calculated using the alteration with the highest allele fraction , including variants of unknown signicance . time ( months ) fig a2 . 
 clinical application of circulating tumor cells and circulating tumor dna in uveal melanoma purpose to evaluate the feasibility of using circulating tumor cells ( ctcs ) and circulating tumor dna ( ctdna ) for the management of uveal melanoma ( um )  . patients and methods low - coverage whole - genome sequencing was used to determine somatic chromosomal copy number alterations ( scnas ) in primary um tumors , ctdna , and whole - genome amplified ctcs . 
ctcs were immunocaptured using an antimelanoma associated chondroitin sulfate antibody conjugated to magnetic beads and immunostained for melanoma antigen recognised by t cells 1 ( mart1 ) / glycoprotein 100 ( gp100 ) / s100 calcium - binding protein ( s100 )  . 
ctdna was quantified using droplet digital polymerase chain reaction assay for mutations in the gnaq , gna11 , plc4 , and cysltr2 genes . results scna analysis of ctcs and ctdna isolated from a patient with metastatic um showed good concordance with the enucleated primary tumor . 
in a cohort of 30 patients with primary um , ctcs were detected in 58% of patients ( one to 37 ctcs per 8 ml of blood ) , whereas only 26% of patients had detectable ctdna ( 1.6 to 29 copies / ml )  . 
however , the frequent detection of ctcs in patients with early - stage um supports a model in which ctcs can be used to derive tumor - specific scna relevant for prognosis . 
monitoring of ctdna after treatment of the primary tumor allowed detection of metastatic disease earlier than 18f - labeled fluorodeoxyglucose positron emission tomography in two patients . conclusion the presence of ctcs in localized um can be used to ascertain prognostic scna , whereas ctdna can be used to monitor patients for early signs of metastatic disease . 
2018 by american society of clinical oncology introduction uveal melanoma ( um ) is the most common intraocular malignancy.1 despite successful control of the primary tumor within the eye , metastatic disease ultimately develops in up to 50% of patients , predominantly in the liver . 
currently , there are limited therapeutic options for metastatic um , and as a result there is a high mortality rate.2 extensive analysis of primary ums has defined molecular features of the tumor cells that predict , with a high degree of accuracy , a patients risk for development of metastases . 
biomarkers of poor prognosis include histopathological features of the tumor ; somatic copy number alterations ( scnas ) , such as loss of chromosome 3 , 6q , and 8q3 , 4 ; bap1 mutations5 , 6 ; and the differential expression of marker genes that include well - characterized cancer - associated factors.7 , 8 other features , such as gain in 6p and mutations in eif1ax and sf3b1 , are associated with better prognosis.4 , 6 given that metastasis in um arises from hematogenous dissemination , investigation of circulating tumor cells ( ctcs ) and circulating tumor dna ( ctdna ) could provide a unique opportunity for genetic analysis of the patients tumor through a simple and safe blood test . 
previous research has indicated that ctcs harbor genetic profiles representative of the primary tumor9 and can be used to detect tumor - specific mutations in other cancers.9 - 14 in um , amplification aaron beasley timothy isaacs muhammad a . 
gray , phd , school of medical and health sciences , edith cowan university , 270 joondalup dr , joondalup , wa 6027 , australia ; e - mail : e.gray@ecu. 
 of dna from a single ctc has been reported , with comparative genomic hybridization array showing copy number abnormalities associated with poor prognosis.15 a recent study described the detection of loss in chromosome 3 in ctcs using a modified fluorescence in situ hybridization technique as a method to aid prognostication of um patients likely to metastasize.16 an additional blood - based marker , commonly used to evaluate tumor burden and tumor - specific genetic features , is ctdna.17 , 18 the high proportion of recurrent hot spot mutations in um enables the opportune detection of ctdna using droplet digital polymerase chain reaction ( pcr )  . 
ums carry mutually exclusive activating mutations in gnaq , gna11 , plc4 , and cysltr2 , encompassing more than 90% of um patients.4 , 19 - 22 bidard et al18 detected ctdna in 84% of patients with um with metastatic disease and found ctdna levels to be an independent prognostic factor for both progression - free survival and overall survival.18 however , the presence and prognostic significance of ctdna in patients with primary um without detectable metastatic disease has yet to be evaluated . given that um harbors distinct scnas that correlate with poor prognosis ( l1p , l3 , l6q , g8q ) and good prognosis ( g6p ) , 4 their detection in ctcs may offer a minimally invasive method for prognostication . 
furthermore , because ctdna is highly correlated with tumor volume , 18 it may offer a minimally invasive method for detection of metastatic disease . here , we evaluated the viability of ctc and ctdna as suitable biomarkers to derive prognostic information in um . 
the blood of patients with primary um was analyzed for both the number of ctcs immunomagnetically captured using melanoma - associated chondroitin sulfate proteoglycan ( mcsp ) and the level of plasma ctdna . 
finally , we showed that ctdna monitoring allowed early detection of metastatic disease in two patients with um . western australia , were enrolled in the study between march 2014 and november 2016 . 
um was diagnosed by clinical and ultrasound examination performed by a specialist ophthalmologist to evaluate the size and location of the intraocular tumor , including the presence of ciliary body involvement . 
for ctc quantification , blood was collected in vacutainer k2 edta tubes ( bd biosciences , franklin lakes , nj ) , stored at 4c , and processed within 24 hours . 
 plasma was isolated by double centrifugation at 1 , 600 g for 10 minutes and stored at 80c . ctc capture , quantification , and lowpass whole - genome sequencing ctc isolation was adapted from a previously described protocol , 23 detailed in the data supplement . 
one hundred nanograms of whole - genome amplified ( wga ) dna ( data supplement ) was used to construct 200 - bp sequencing libraries using an neb next ultra fragment library kit ( new england biosciences , ipswich , ma ) and barcoded using the ion xpress barcode adapters 1 - 96 kit ( life technologies , carlsbad , ca )  . 
somatic mutations and scnas were analyzed using ion reporter 4.6 ( life technologies )  . ctdna quantification cell - free dna ( cfdna ) was extracted from 1 to 5 ml of plasma using a qiaamp circulating nucleic acid kit ( qiagen , hilden , germany ) according to the manufacturers instructions and stored at 80c . 
comparison between the genetic profile of the primary tumor , cell - free dna ( cfdna ) , two circulating tumor cells ( ctcs ) , and a single peripheral blood mononuclear cell ( pbmc ) in a patient with metastatic uveal melanoma . 
cells were stained with a combination of antibodies against the melanoma markers melanoma antigen recognised by t cells 1 ( mart1 ) / glycoprotein 100 ( gp100 ) / s100 calcium - binding protein ( s100 ; green ) , cd45 ( red ) , and 4 ' , 6 diamidino - 2 - phenylindole ( dapi ; blue ) , taken at 200 magnification . 
 ( c ) whole - genome sequencing somatic chromosomal copy number alteration profile of primary formalin - fixed paraffin - embedded tumor , cfdna , two ctcs , and a single pbmc . 
 tumor volume was calculated using a formula previously described.24 the numbers of captured ctcs in patients with and without monosomy of chromosome 3 were compared using a nonparametric mann - whitney u test . 
statistical analyses were performed using graphpad prism version 5.0 ( graphpad software , la jolla , ca )  . results analysis of somatic copy number alterations in ctcs from a patient with um with metastatic disease ctcs were isolated from peripheral venous blood of a patient with metastatic um ( patient 640 )  . 
in march 2017 , the patient was diagnosed with metastatic um , with bone marrow activity in the spine , pelvis , ribs , and both femora ( fig 1a )  . 
the accuracy and reliability of this wga method for the analysis of single um for assessment of scna were first demonstrated using individual cells from three um cell lines ( data supplement )  . two ctcs and a pbmc provided suitable wgadna material for whole - genome sequencing . 
multiplex ligand dependent probe amplification ( mlpa ) analysis of the primary tumor confirmed the chromosomal gains of 6p and 8p / 8q and the lack of evidence for scnas of 1p and 3p / 3q ( data supplement )  . 
 the two isolated ctcs also showed overlapping chromosomal gains and losses in comparison with the primary tumor , despite the primary tumor being removed 2 years earlier ( fig 1c )  . 
additional alterations found in ctcs comprised a gain in 6q in both cells , a gain of chromosome 22 in ctc1 , and a loss of chromosome 10 in ctc2 . 
the pbmc analyzed did not harbor any scnas ( fig 1c ) , same as multiple pbmcs used as negative controls in the validation experiments ( data supplement )  . 
the gna11 q209l mutation was detectable in dna derived from the primary tumor and in wga ctcs . sequencing of cfdna from the same blood sample from which ctcs were isolated also showed similar chromosome gains , with trends toward gains in some chromosomal alterations found in the primary tissue ; however , these did not reach the threshold to be called a true gain ( fig 1c )  . 
 droplet digital pcr targeting the gna11 q209l mutation in the cfdna indicated the presence of 15 , 460 copies / ml of mutant dna in plasma , with a 20.2% frequency abundance relative to normal dna . 
thus , despite the significant abundance of ctdna , this compartment is not as sensitive as ctcs for the analysis of scnas . these results illustrate that tumor - associated scna can be ascertained through genetic analysis of ctcs , providing important prognostic information . 
ctcs were identified by positive staining for melanoma antigen recognised by t cells 1 ( mart1 ) / glycoprotein 100 ( gp100 ) / s100 calcium - binding protein ( s100 ) and negative staining for cd45 ( fig 2a )  . 
a total of 15 of 26 ( 58% ) individuals with assessable results had at least one ctc in 8 ml of blood , with a range of one to 37 ctcs detected , and 14 ( 54% ) patients had two or more detectable ctcs . 
screening for all of these mutations was necessary in our study , because for most patients fine - needle aspirate biopsies were either not performed or provided limited amounts of dna that was used for mlpa testing and , therefore , we were unable to determine the tumors driver mutations before testing for ctdna . 
instead , all patient blood samples were tested for these mutations , because they have been reported to occur in > 90% of ums.19 , 20 , 22 we detected ctdna in eight of the 30 patients tested ( 23% ; range , 1.6 to 29 copies ) ; two patients had a gnaq q209l mutation , two had a gna11 q209l mutation , one had a gna11 q209p mutation , one had a gna11 r183c mutation , one had a plc4 d630y mutation , and one had a cysltr2 l129q mutation . 
green fluorescence ( af488 , mel ) indicates staining with a combination of antibodies against the melanoma markers mart1 / gp100 / s100 ; red fluorescence ( phycoerythrin [ pe ] ) indicates cd45 positivity ; and blue fluorescence ( 4 ' , 6 - diamidino - 2 - phenylindole , dapi ) indicates the presence of a nucleus . 
no correlation was found between ctc , ctdna , and tumor size . detectable mutations , ctdna levels were correlated with tumor size ( largest basal / apical diameter / volume ; figs 2g - 2i )  . ctdna for detection of metastatic um we also analyzed ctdna in eight patients with metastatic um . 
 retrospective analysis of longitudinal samples collected from two patients indicated that detection of ctdna preceded radiologic recognition of liver metastases . patient 656 had an enucleation 3 months before enrollment and a history of low - grade lymphoproliferative disorder and pulmonary embolis pathology of the enucleated tumor confirmed a choroidal melanoma , with callender classification mixed and no angiolymphatic invasion . 
a positron emission tomography ( pet ) scan 4 weeks before enrollment showed mildly fluorodeoxyglucose ( fdg ) - avid bilateral pelvic and inguinofemoral lymphadenopathy consistent with her history of a low - grade lymphoproliferative disorder . 
characteristics of patients with confirmed metastatic disease patient baseline ctdna ( copies / ml ) ctdna mutation primary um location ( eye ) gna11 q209l 5 , 745 3 , 300 15 , 160 gnaq q209l gna11 q209l gna11 q209l gna11 q209l gna11 q209l note . 
 ( c ) plasma ctdna levels in longitudinally collected samples from patient 433 with um , before and after the development of overt metastatic disease as shown by fluorodeoxyglucose positron emission tomography imaging of the liver . 
however , ctdna levels significantly increased to 1 , 380 copies / ml by week 96 , with the concurrent imaging indicating new extensive metastases to the left lobe of the liver and new bone metastases . 
these results illustrate that for um , ctdna can be used to track disease burden and has the potential to provide a complementary measure in addition to imaging . discussion our results provide the proof of concept for using blood - based biomarkers for prognostication and routine monitoring of patients with um . 
these preliminary findings warrant additional clinical studies to validate the use of these two biomarkers for the management of um . previously , scna profiles of the primary tumor have been shown to accurately identify patients with um at risk for developing metastatic disease.4 , 25 although fine - needle aspirate biopsies are performed worldwide , genetic testing of um primary tumors can be hampered by patients declining biopsy because of the perceived invasiveness of the procedure and the preferred use of sight - conserving therapies . 
nevertheless , up to 50% of patients with um will develop metastatic tumors after either short or long latency periods.26 thus , development of pre - emptive adjuvant therapies may be an important strategy for improving survival . 
in this context , the provision of a blood test for the identification of prognostic scna from ctcs would allow identification of patients at risk , aiding triaging of patients for clinical trials and more frequent systemic surveillance for metastatic disease . most ctc studies in um have been limited to ctc quantification . 
however , they have failed to find significant association between the levels of ctcs and disease prognosis.27 , 28 similarly , we found that most patients have detectable ctcs irrespective of the predicted propensity of their tumor to metastasize , indicating that the presence of these ctcs may not be associated with metastatic disease risk . 
however , our ctc detection was restricted to the detection of mcsp - expressing cells , and thus we cannot exclude that ctcs expressing other cell surface markers may also provide prognostic information , as shown in some studies.28 , 29 nevertheless , the opportunity to examine the genomic features in ctcs may offer a more accurate indication of patient metastatic risk , in comparison with simple quantification of ctcs . 
on the basis of the results presented here , methodologies to enhance ctc capture16 , 28 are needed for the optimal implementation of ctcs as a viable alternate source of tumor genetic material from which prognosis can be derived for most patients . sequencing of the matching cfdna revealed several large chromosomal gains , but because of the high abundance of normal cfdna , we could only detect trends toward chromosomal amplifications found in the ctcs and primary tumor . 
 patient 640 ( fig 1 ) had a high disease volume , with 15 , 460 copies / ml of gna11 q209l ctdna with a fractional abundance of 20% , whereas by contrast the highest ctdna level in our primary um study was found to be 29 copies / ml , with a fractional abundance of < 1% ; therefore , sequencing of patients with localized disease for scna profiles may prove ineffective . 
 previous studies investigating scna in cfdna similarly required the presence of a large fraction of ctdna present to obtain results similar to the tissue of origin.30 thus , although ctdna is much easier to isolate , analysis of scna in ctcs should prove to be a more effective means of analyzing prognostic scna . we also showed that ctdna is not commonly detectable in blood of patients with localized um . 
our findings in this study indicate that the low levels of detectable ctdna in patients with primary disease are not suitable for screening of patients at a high risk of developing metastasis . 
however , given the high proportion of hotspot mutations in um , 4 ctdna analysis may be a feasible minimally invasive method of monitoring metastatic disease burden and disease progression , as we have exemplified here . in conclusion , our study underscores the potential clinical use of liquid biopsy for um . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . aaron beasley no relationship to disclose muhammad a . 
khattak honoraria : msd oncology , novartis , merck serono consulting or advisory role : bristol - myers squibb , merck serono speakers ' bureau : merck serono , msd oncology , novartis research funding : msd oncology travel , accommodations , expenses : msd oncology , amgen , merck serono fred k . 
pereira no relationship to disclose kyle yau no relationship to disclose jacqueline bentel no relationship to disclose tersia vermeulen no relationship to disclose leslie calapre no relationship to disclose michael millward consulting or advisory role : roche , bristol - myers squibb , astrazeneca , merck sharp & dohme , novartis , boehringer ingelheim travel , accommodations , expenses : roche , merck sharp & dohme , bristol - myers squibb , astrazeneca elin s . 
gray research funding : merck sharp & dohme patents , royalties , other intellectual property : provisional patent on a blood test to detect melanoma based on auto - antibody detection travel , accommodations , expenses : bio - rad laboratories timothy isaacs travel , accommodations , expenses : pfizer melanie r . 
we also thank pauline zaenker , ashleigh mcevoy , and danielle bartlett for their phlebotomy services , william cunningham , md , and rian vijoen , md , for assisting with patient recruitment at royal perth hospital , and karen shakespeare for gathering the clinical data . affiliations aaron beasley , muhammad a . 
khattak , jaqueline bentel , and tersia vermeulen fiona stanley hospital , murdoch , western australia , australia . support supported by an edith cowan university postgraduate scholarship and a cancer council western australia honours scholarship ( a.b. ) ; a fellowship from the cancer research trust ( e.s.g. ) ; raine medical research foundation priming grant , ophthalmic research institute of australia grant , and western australia cancer council grant no . 
heitzer e , auer m , gasch c , et al : complex tumor genomes inferred from single circulating tumor cells by array - cgh and next - generation sequencing . 
gasch c , bauernhofer t , pichler m , et al : heterogeneity of epidermal growth factor receptor status and mutations of kras / pik3ca in circulating tumor cells of patients with colorectal cancer . 
carter l , rothwell dg , mesquita b , et al : molecular analysis of circulating tumor cells identifies distinct copy - number profiles in patients with chemosensitive and chemorefractory small - cell lung cancer . 
dago ae , stepansky a , carlsson a , et al : rapid phenotypic and genomic change in response to therapeutic pressure in prostate cancer inferred by high content analysis of single circulating tumor cells . 
suesskind d , ulmer a , schiebel u , et al : circulating melanoma cells in peripheral blood of patients with uveal melanoma before and after different therapies and association with prognostic parameters : a pilot study . 
 addition of chemotherapy is associated with decreased survival in early - stage ( t1 - 2n0m0 ) glottic squamous cell carcinoma treated with definitive radiotherapy purpose the role of chemoradiation ( crt ) in treating patients with early - stage glottic squamous cell carcinoma ( scc ) , especially for t2n0m0 glottic scc with impaired vocal cord mobility , remains unexplored . 
we sought to evaluate the impact of crt on survival in early - stage glottic scc by using the seer database . patients and methods we included patients with localized ( t1 - 4n0m0 ) glottic scc ( n = 4 , 743 ) diagnosed between 2004 and 2014 and treated with definitive radiotherapy ( rt ) alone , crt , or laryngectomy alone in the seer database . 
disease - specific mortality ( dsm ) was evaluated via multivariable regression using a competing risk model that accounts for other - cause mortality as a competing risk event for dsm . 
2019 by american society of clinical oncology introduction definitive treatment with radiotherapy ( rt ) for t1 - 2n0m0 squamous cell carcinomas ( scc ) of the glottis remains a standard of care in the united states and can help to preserve voice quality . 
several studies have shown lc rates for t1 and t2 glottic cancer treated with transoral laser microsurgery to range from 77% to 92% and 66% to 88% , respectively , 1 - 5 whereas open surgical procedures for glottic scc demonstrated a lc rate of 86% to 98%.2 , 6 - 10 the lc rate for early - stage glottic cancer treated with definitive rt depends significantly on t stage , with studies showing lc rates of 82% to 94% for t1 disease11 - 17 and 61% to 80% for t2 disease.11 - 13 , 15 - 19 the decreased lc for t2 glottic cancers treated with rt alone was thought to be attributed to a subset of patients with impaired vocal cord chenyang wang amar u . 
 the radiation therapy oncology group 9111 trial established concurrent crt as the standard treatment of t3 glottic cancer.28 the lc benefit associated with crt in the setting of t3 glottic cancer has raised the question of whether the subset of patients with t2 glottic cancer with impaired vocal cord mobility should be treated with crt as well , given the suboptimal outcomes with rt alone . 
seer routinely collects data on patient demographics , primary tumor site , morphology , stage at diagnosis , first course of treatment , and follow up for vital status . for this study , we selected patients diagnosed with n0m0 scc of the glottic larynx diagnosed from january 1 , 2004 , to december 31 , 2014 , who underwent definitive rt , crt , or subtotal or total laryngectomy . 
we excluded patients who had non - scc histology , unknown tumor grade , unknown race , unknown surgical status , unknown t stage , more than one primary malignancy , no active follow - up , or age younger than 18 years . 
this study was reviewed and approved by the institutional review board of the university of california , los angeles . statistical analysis extracted variables included age at diagnosis , sex , race , year of diagnosis , t stage , and tumor grade . 
analysis of variance , kruskal - wallis rank sum tests , and 2 tests were used to characterize differences in variables of interest between different treatment cohorts for continuous , ordinal , and categorical variables , respectively . 
 follow - up time was calculated via the reverse kaplan - meier method described by schemper and smith , 30 in which alive at last follow - up was designated the event of interest while death from any cause was censored . 
seer determines death and cause of death via algorithms to process death certificates , taking into account causes of deaths in conjunction with tumor sequence , site of original cancer diagnosis , and comorbidities . 
 to account for other - cause mortality ( ocm ) as a competing risk for dsm , multivariable regression analyses on the basis of the competing risk model as described by fine and gray31 were applied to the survival analysis while adjusting for age , year of diagnosis , sex , race , t stage , definitive treatment modality , and tumor grade . 
for t2n0 disease , an additional subset analysis was carried out on the basis of vocal cord impairment status to investigate whether patients with t2n0 disease with vocal cord impairment selectively benefit from crt . 
the validity of proportional hazards assumption was evaluated via schoenfeld residuals . to adjust for covariables and determine whether the addition of chemotherapy to rt affected dsm in patients with t1 - 4n0m0 glottic scc , we adopted propensity score matching ( psm ) via a nearest neighbor approach to balance patient characteristics including age , year of diagnosis , sex , race , and tumor grade between the rt and crt cohorts for each t stage . 
propensity score , first defined by rosenbaum and rubin32 as the probability of treatment assignment on the basis of a set of observed baseline patient characteristics , provides the means to retrospectively balance distribution of patient characteristics and thereby minimize effects of unmeasured confounders on treatment outcomes . 
the cumulative incidences of dsm and ocm after psm were plotted to illustrate the difference between rt and crt cohorts for each t stage , and their distributions were evaluated via a k - sample test described by gray.33 all statistical analyses were carried out using r version 3.4.1 ( r foundation for statistical computing , vienna , austria ) with two - sided testing and a statistical significance threshold of p = .05. results patient characteristics patient characteristics , stratified by definite treatment modality consisting of rt , crt , and subtotal or total laryngectomy , are listed in table 1 . 
patients who underwent rt alone tended to be older , with a median age of 66 years , compared with patients who underwent crt and surgery , who had median ages of 62 and 63 years , respectively . 
these patients were also more likely to present with higher tumor grade . multivariable regression for dsm and the results of the multivariable regression for dsm according to the competing risk model , accounting for ocm as a competing risk , are listed in table 2 . 
 plots of schoenfeld residuals versus failure times are shown in appendix figure a2 . subgroup multivariable regression for dsm using a competing risk model stratified by t stage the results of subgroup multivariable regression for dsm stratified by t stage are listed in table 3 . 
more recent year of diagnosis was not associated with any significant difference in dsm . cumulative incidence of dsm and ocm for rt and crt after psm patient characteristics stratified by definitive treatment modality before and after psm are listed in appendix tables a1 and a2 , respectively . 
a recent phase ii trial of concurrent crt with a fluoropyrimidine agent for t2n0m0 scc of the larynx ( 70% ) , oropharynx ( 16% ) , and hypopharynx ( 14% ) demonstrated a 3 - year lc rate of 89.0% and a 3 - year overall survival rate of 97.2%.29 another study by bhateja et al25 demonstrated superior lc in patients receiving crt for t2b - 3n0 - 2 glottic cancers compared with patients receiving rt alone for t2n0m0 glottic cancer with impaired vocal cord mobility ( t2bn0 ) , suggesting a potential therapeutic benefit of crt in this setting . 
in this study , 51.6% of the t2bn0 patients treated with rt alone received altered fractionation ( > 2.1 gy per fraction or twice - a - day fractionation ) compared with 38.5% of patients in the crt cohort . 
of note , the crt cohort contained only one patient with t2bn0 and one patient with t2bn1 ; therefore , it is difficult to assess the impact of crt on patients with t2bn0 disease . 
in accordance with the results from bhateja et al , 25 our study also demonstrated that patients with t3n0 glottic scc had decreased dsm with crt compared with rt alone . 
cumulative incidence plots of disease specific mortality ( dsm ) and other - cause mortality ( ocm ) for glottic squamous cell carcinoma at each t stage after propensity score matching . 
to our knowledge , our data from this study are the first to question the utility of chemotherapy in addition to rt for t2bn0 glottic scc . one possible hypothesis for the increase in dsm for patients with t1 - 2n0 glottic scc treated with crt may be treatment prolongation as a result of increased toxicity . 
rt treatment time prolongation past 40 days has been shown to correlate with decreased lc from 95% to 100% to 79% to 84%.13 , 34 additional factors that can contribute to the observed survival detriment in crt may be lower total rt dose and dose per fraction as a result of the higher combined toxicity with chemotherapy , because it has been established that total rt dose less than 65 gy results in decreased lc.2 , 10 , 13 , 14 , 35 furthermore , a randomized prospective study has shown that 2.25 gy per fraction , as compared with 2 gy per fraction , results in significantly improved lc.36 meanwhile , the survival benefit associated with chemotherapy in locally advanced glottic scc may be attributed to improved lc secondary to chemotherapy sensitization and / or additional regional and distant control , which could compensate for the decrease in lc associated with potential treatment prolongation . this study had several important limitations inherent to the seer database , including lack of information on radiation dose , treating physician experience , the type of treatment institution , and sequence of chemotherapy relative to rt , which prevented us from distinguishing between concurrent versus induction chemotherapy . 
however , given the relatively rare use of induction chemotherapy in the modern era for t1 - 2n0 glottic scc , it is reasonable to assume that the patients in the crt cohort of this study predominantly received concurrent crt . 
steinberg honoraria : viewray consulting or advisory role : viewray research funding : viewray , accuray travel , accommodations , expenses : viewray robert chin travel , accommodations , expenses : varian medical systems , brainlab affiliations chenyang wang , amar u . 
spector jg , sessions dg , chao ksc , et al : stage i ( t1 n0 m0 ) squamous cell carcinoma of the laryngeal glottis : therapeutic results and voice preservation . 
laccourreye o , muscatello l , laccourreye l , et al : supracricoid partial laryngectomy with cricohyoidoepiglottopexy for early glottic carcinoma classified as t1 - t2n0 invading the anterior commissure . 
marshak g , brenner b , shvero j , et al : prognostic factors for local control of early glottic cancer : the rabin medical center retrospective study on 207 patients . 
le q - tx , fu kk , kroll s , et al : influence of fraction size , total dose , and overall time on local control of t1t2 glottic carcinoma . 
cellai e , frata p , magrini sm , et al : radical radiotherapy for early glottic cancer : results in a series of 1087 patients from two italian radiation oncology centersi . 
warde p , osullivan b , bristow rg , et al : t1 / t2 glottic cancer managed by external beam radiotherapy : the influence of pretreatment hemoglobin on local control . 
mendenhall wm , parsons jt , million rr , et al : t1t2 squamous cell carcinoma of the glottic larynx treated with radiation therapy : relationship of dose - fractionation factors to local control and complications . 
frata p , cellai e , magrini sm , et al : radical radiotherapy for early glottic cancer : results in a series of 1087 patients from two italian radiation oncology centersii . 
garden as , forster k , wong p - f , et al : results of radiotherapy for t2n0 glottic carcinoma : does the 2 stand for twice - daily treatment ? int j radiat oncol biol phys 55 : 322 - 328 , 2003 20 . 
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hoang , md1 , 2 ; rui yang , md1 , 2 ; daniel weiser , md2 ; jonathan morris , md3 ; richard gorlick , md4 ; jonathan b . 
we have identied a single patient who was initially diagnosed with a benign osteoblastoma and subsequently presented years later with a high - grade osteosarcoma in the same anatomic region . 
a biopsy sample of the mass demonstrated conventional - type osteoblastoma with focal epithelioid features for which the patient underwent intralesional curettage ( fig 2 )  . subsequent imaging demonstrated a persistent abnormal signal in the sacrum , and a plan of continued surveillance was agreed upon . 
over the ensuing 4 - year imaging failed to demonstrate appreciable period , radiographic change , and the patients clinical course remained stable . five years later , the patient returned with increasing paimaging demonstrated an increase in the size of the mass , and an urgent open sacral biopsy was performed ( fig 3 )  . 
staging studies performed at that time were negative for distant disease . neoadjuvant chemotherapy was started in accordance with childrens oncology group protocol aost0331 ; however , because of severe pain , patient required semi - urgent surgical intervention and did not complete planned neoadjuvant treatment . 
the decision was made to manage conservatively , and as of july 2019 , surveillance demonstrated no evidence of disease . methods including the osteoblastoma , patient consent and institutional review board approval were obtained before study initiation . 
sequencing and data analysis were performed by novogene technology ( beijing , china ) to evaluate for structural variants , copy number variation , single nucleotide variants , and insertions / deletions . 
germline - matched comparison from each tumor was undertaken to evaluate for somatic changes . to evaluate for pathogenic variants , somatic analysis on small variants focused on changes that would elicit a coding or splice site change and were not common polymorphisms ( allele frequency , 0.01 in 1 , 000 genomes and exac databases )  . 
furthermore , we evaluated whether any variants were found in cancer mutational hotspots ( recurrence of more than ve in cosmic [ catalog of somatic mutations in cancer ] ) or were a truncating variant in a known tumor suppressor gene ( cancer gene census )  . 
 geller et al context key objective does genomic analysis of a patient who was initially diagnosed with a benign osteoblastoma and subsequently presented years later with a high - grade osteosarcoma in the same anatomic region demonstrate evidence of malignant transformation ? knowledge generated there was near - zero overlap in the somatic small variants , somatic copy number variation pattern , and predicted structural variants in the osteoblastoma compared with the osteosarcoma . 
findings from this study argue against malignant transformation as an evolving or stepwise process and conversely support two distinct neoplasms with dissimilar genetic makeups . relevance this study performed an in - depth genetic characterization of two distinct tumors that historically have been believed to be along the same spectrum of disease . 
in addition , a germline mutation in brip1 was discovered , which lends itself to additional investigation . pathogenic or likely pathogenic for a cancer predisposition syndrome . results whole - genome sequencing resulted in high - quality data , which generated an average 63 million reads per tumor , with more than 98% usable on the basis of quality metrics . 
after ltering and duplicate removal , mapping to hg19 resulted in an average sequencing depth of 29 and 32 for the benign and malignant tumors , respectively , and at least 4 coverage in more than 99% of the genome . somatic variant analysis revealed approximately 98 , 000 and 141 , 000 high - condence small variants in the benign and malignant tumor , respectively , which corresponded to somatic mutational burdens of 33 and 47 mutations / megabase ( mb )  . 
in the osteosarcoma , a single variant recurrent in cosmic of unclear oncologic signicance , znf429 p.n426k , was found as well as truncating mutations in two tumor suppressor genes , daxx and ncor1 . structural and copy number variation analysis revealed signicant alterations in both tumors . 
a striking number of somatic inversion events were found in both tumors ( approximately 1 , 750 per tumor ) , particularly compared with other structural changes , such as translocations , deletions , or tandem duplications ( each approximately 10 to 30 per tumor )  . 
 ( a ) a 2015 hematoxylin and eosinstained low - power ( 10 ) micrograph demonstrates ndings consistent with high - grade osteosarcoma , including high cellularity , multiple foci of tumor necrosis , and osteoid formation . 
 ( b ) a 2015 hematoxylin and eosinstained high - power ( 40 ) micrograph that demonstrates pleiomorphic and bizarre cellular features . overlap in the predicted structural variants in the osteoblastoma compared with the osteosarcoma . germline analysis using the methods described identied a single pathogenic germline mutation , brip1 r798x , identied with high condence in all three samples . 
a summary of genomic ndings is listed in table 1 . discussion the notion that osteoblastoma can undergo malignant transformation to osteosarcoma dates back to an original report in 1967.1 since then , 24 cases have appeared in the literature , none of which investigated the transformation event on a genomic level1 - 20 ( table 2 )  . 
given the lack of objective genetic data and short time to transformation in some cases , there is a distinct possibility that some of these reports represent coincidence or diagnostic error . a few prior reports have attempted to document malignant transformation through a limited analysis of sequential biopsies samples.4 , 18 , 21 however , these tumors were characterized only in terms of ploidy , thereby limiting understanding of the transformation process.4 , 18 , 21 although these reports suggested that transformation is associated with an increase in dna content , only one patients tumor showed an observable change in dna content over time . moreover , in the current study , we have demonstrated the benign and malignant tumors to have distinct genomic proles with almost no overlap in somatic changes . 
whether these tumors are driven in part by an unrecognized anatomic predisposition remains speculative . we also identied a germline mutation in the brip1 tumor suppressor gene , a member of the recq helicase family associated with brca1.22 , 23 brip1 mutations are associated with a predisposition to breast cancer , ovarian cancer , and fanconi anemia , 22 , 24 , 25 and brip1 is known to play a critical role in dna repair , with knockdown leading to chromosomal instability.26 of note in our patient , both the benign and the malignant tumors exhibited a higher - thantypical somatic mutation rate compared with most pediatric malignancies27 as well as a high number of structural variants with a preponderance of inversion events , which suggests a functional role of this germline nding . 
we have speculated that these changes may have accumulated because of brip1 partial dysfunction that led to chromoinstability and impaired dna crosslink repair.26 somal admittedly , denitive conclusions cannot be drawn on the basis of a single patient , and additional investigation seems warranted . although osteoblastoma infrequently has been associated with mutations involving rb , tp53 , fos , fosb , d - jun , and mdm2 , the genetic landscape of this tumor is still largely unknown.28 - 31 the osteoblastoma in this report is similar to previous reports in that we observed many structural table 1 . 
many osteosarcomas demonstrate chromosomal abnormalities that commonly involve tumor suppressor genes or dna helicases.32 , 33 however , osteosarcoma generally is recognized as exhibiting tremendous genetic complexity with no clearly identiable genetic driver . this heterogeneity may stem from chromothripsis , 34 - 36 markers of which have been described in 2% to 3% of all cancers and up to 33% of osteosarcomas . 
although the current case did not exhibit evidence of chromothripsis , it demonstrates an otherwise typical genomic prole for osteosarcoma with a high degree of chromosomal instability , increased ploidy , and truncating point mutations in several tumor suppressor genes . in some cases , in conclusion , although malignant transformation of osteoblastoma to osteosarcoma historically has been accepted , review of the literature has revealed a paucity of convincing evidence , and controversy has persisted . 
to our knowledge , this study is the rst to report an in - depth genetic characterization of two distinct tumors within the same patient and the same anatomic location . 
findings from this study argue against malignant transformation as an evolving or stepwise process and conversely supports two distinct neoplasms with dissimilar genetic makeups . this report also has uncovered a germline truncating mutation in brip1 in this patient , which raises the question of whether this serves as an underlying predisposition for both tumors . 
geller , md , monteore greene medical arts pavilion , 3400 bainbridge ave , bronx , ny 10467 ; e - mail : dgeller@monteore.org. support supported by clinical and translational science awards catalytic seed grant ul1 tr001073 ( d.s.g. ) from the national center for advancing translational sciences , a component of the national institutes of health . the content is solely the responsibility of the authors and does not necessarily represent the ofcial views of the national institutes of health . 
j bone joint surg am 57 : 424 - 426 , 1975 stutch r : osteoblastomaa benign entity ? orthopaed rev 4 : 27 , 1975 grace j , mccarthy s , stankovic r , et al : malignant transformation of osteoblastoma : study using image analysis microdensitometry . 
 genomic analysis does not support malignant transformation kunze e , enderle a , radig k , et al : aggressive osteoblastoma with focal malignant transformation and development of pulmonary metastases . 
sun x , brieo - enrquez ma , cornelius a , et al : fancj ( brip1 ) loss - of - function allele results in spermatogonial cell depletion during embryogenesis and altered processing of crossover sites during meiotic prophase i in mice . 
weber - lassalle n , hauke j , ramser j , et al : brip1 loss - of - function mutations confer high risk for familial ovarian cancer , but not familial breast cancer . 
radig k , schneider - stock r , mittler u , et al : genetic instability in osteoblastic tumors of the skeletal systepathol res pract 194 : 669 - 677 , 1998 31 . 
lorenz s , bary t , sun j , et al : unscrambling the genomic chaos of osteosarcoma reveals extensive transcript fusion , recurrent rearrangements and frequent novel tp53 aberrations . 
however , the clinical application of these targeted drugs and diagnostics often remains unclear . however , this approach is not newdoctors have been trying to provide personalized care with high precision for centuries . 
for example , during the last 150 years , virchow developed microscopic pathology , roentgen introduced radiographic imaging , and bloom and richardson proposed a tumor grading scale ; all represented major leaps forward in personalized medicine that we still apply.1a - 1e more recent examples include tests for estrogen receptor in breast cancer to guide endocrine therapy and evaluation of the cd20 antigen on b - cell lymphomas to guide the use of anti - cd20 monoclonal antibodies . so , whats new ? we have new and exciting tools that rival those giants on whose shoulders we stand . 
however , to deliver personalized medicine as precisely as possible , we need high levels of evidence that use of these new therapies and diagnostic tests does , in fact , improve patient care . we agree with the skeptics in oncology who question the benefit of precision oncology , but we maintain that the answer is not to declare it all hype and walk away but to continue to learn how best to use it . 
rather than hope for luck , clinicians should continue to use the scientific method to make evidence - based decisions . in may 2013 , journal of clinical oncology published a special series on precision oncology . the success of this special series led asco to recognize both the plethora of research that is occurring in this field and the need to disseminate this information effectively to the oncology community . 
the special issue of jco featured articles that outlined the current and emerging technologies for tumor genomic profiling , 1f ways to build personalized medicine infrastructure at major cancer centers , 2 and various applications of genomic profiling for different cancer diagnoses . 
it will also provide researchers and clinicians with a reliable source of high - quality precision oncology research , reviews , and commentary essential to real - world cancer care . 
in addition to original clinical research , the journal will publish articles about key care delivery issues , such as value , quality , and cost - effectiveness , and about ethical , legal , and social considerations to inform clinical practice and shape this rapidly evolving field . we are thrilled to have james m . 
ford is a professor of medicine ( oncology ) , pediatrics ( medical genetics ) , and genetics and is the director of the stanford cancer genetics clinic and the cancer genomics program at the stanford cancer institute . 
hayes , university of michigan comprehensive cancer center , ann arbor , mi ; and julie vose , university of nebraska medical center , omaha , ne corresponding author : daniel f . 
 genetic targets for personalized targeted therapies in breast and gastrointestinal cancer as well as in examination of the role of dna repair in the treatment and prevention of cancer in families and populations . 
with the commencement of the targeted agent and profiling utilization registry ( tapur ) study , asco aims to describe both the safety and the efficacy of targeted anticancer drugs to catalog genomic profiling tests and to learn about the utility of registry data . 
in addition , with the launch by asco of cancerlinq , oncologists will have access to a massive database of treatment options and results of those treatments from millions of patient records . 
vose consulting or advisory role : bio connections research funding : celgene ( inst ) , genentech ( inst ) , incyte ( inst ) , janssen biotech ( inst ) , acerta pharma ( inst ) , kite pharma ( inst ) , seattle genetics ( inst ) , novartis ( inst ) , amgen ( inst ) , bristol - myers squibb ( inst ) , allos therapeutics ( inst ) references 1a . 
hammond me , hayes df , dowsett m , et al : american society of clinical oncology / college of american pathologists guideline recommendations for immunohistochemical testing of estrogen and progesterone receptors in breast cancer . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
tbt reimbursement within the united states in the current regulatory environment is not tied to premarket evidence of clinical utility , resulting in a vicious cycle wherein low - level evidence of utility leads to poor reimbursement , thereby impeding investment in developing new , clinically valuable tbts supported by high - level evidence . 
precise one - to - one mapping of reimbursement to cost savings or cost effectiveness is precluded by an absence of formal cost - effectiveness analyses for many emerging tbts , and for more established tbts , it has become clear that such analyses may yield wildly variable , subjective estimates . 
to address these challenges , we propose a system of tiered reimbursement that rewards development of high - quality tbts within specic use contexts , supported by strong evidence of analytic validity and clinical utility . 
we propose three use contexts of tbts , each dened by its inuence on treatment decisions relative to the current standard of careopt - out , opt - in , and the use of appropriate , alternative , effective therapies ( opt - alt )  . 
the true clinical utility of a tbt is often difcult to determine , initiating a vicious cycle in which tbts are often undervalued and poorly reimbursed because of a lack of high - level evidence of clinical utility.1 an inconsistent regulatory and reimbursement environment results in an unfavorable return on investment in the research and development ( r&d ) needed to generate the high levels of evidence ( loes ) necessary to demonstrate the clinical utility of tbts.1 indeed , despite increasing recognition of the benets of personalized medicine , medicare coverage of many emerging tbts is being signicantly reduced or denied , 2 resulting in decreased investment in tbt r&d.3 reimbursement of tbts to date has been driven primarily by a combination of commodity and labor pricing ( ie , reagent and technical costs ) , market forces , and perceived clinical value . 
this is not an effective strategy to support long - term investment in high - quality tbts . we propose that objective and transparent tiers of tbt value be created based on high loes of analytic validity ( ie , accurate and reproducible measurement of a specic analyte ) and clinical utility ( ie , improves patient outcomes ) that meet minimal specied thresholds and address unmet medical needs.4 , 5 our proposal would potentially result in redistribution of health care dollars currently spent on needless or ineffective therapies while ensuring that patients who require and are likely to benet from treatment strategies receive theit will create pathways by which tbt manufacturers could receive guaranteed minimum rates of reimbursement ( fig 1 ) and thereby increase the likelihood that tbt developers obtain a return on r&d investment . 
we propose an alternative , value - based reimbursement which clinical utility can be assessed within specic use contexts , undergo formal review , and then provide a new value - based , tiered reimbursement rate . 
note that the use of appropriate , alternative , effective therapies ( opt - alt ) context includes both the initial treatment and the monitoring paradigms . fda , us food and drug administration ; icers , cost - effectiveness ratios ; qaly , quality - adjusted life - year . dinan et al proposed valuation status quo / conventional pricing holder of tbt seeks higher , value - based reimbursement value - based application to set new reimbursement cost - saving tbts opt - out evidence to reduce treatment % treatment reduction treatment cost pricing : function of costs saved cost - effective tbts evidence of beneficial treatment treatment outcomes ( qalys ) treatment costs pricing : function of icers opt - in opt - alt approved : new value - based reimbursement set formal review by fda or other regulatory body loes of robustness in the assay itself and that its use improves patient outcomes compared with not using it , respectively.4 - 6 we propose three major contexts of use for which a tbt might have clinical utility , and therefore value , designated as optout , opt - in , and the use of appropriate , alternative , effective therapies ( opt - alt ; table 1 )  . 
each of these terms refers to the clinical decision that might be made based on the results of the tbt compared with the decision made as standard of care ( soc ) without tbt results . 
these categories can be applied to the various use contexts considered for the tbt , including assessment of cancer risk / susceptibility , screening , differential diagnosis , prognosis , prediction , and monitoring.7 similar to therapeutics , the performance and therefore value of a tbt will vary within certain subpopulations of patients , underlying the need to specify the target population when assessing value within a specic use context . 
opt - out tbts have value and the potential to be directly cost saving by reducing the use of unnecessary or ineffective yet toxic and costly therapies , either by indicating that the patient does not need additional therapy ( prognosis ) or that the therapy under consideration is unlikely to work ( prediction ; table 1 )  . perhaps the most well - known example of opt - out tbts with high analytic validity and clinical utility are genomic tests used to determine whether adjuvant chemotherapy should be given to patients with estrogen receptorpositive , human epidermal growth factor receptor 2negative , and least ve node - negative breast cancer . 
there are at commercially available tbts in this category.8 , 9 the 21 - gene recurrence score ( rs ; oncotype dx ; genomic health , redwood city , ca ) is the most well studied and provides an illuminating case study . 
before introduction of the 21 - gene rs , adjuvant chemotherapy was recommended for 50% or more of patients with estrogen receptorpositive , human epidermal growth factor 2negative , node - negative breast cancer.10 the 21 - gene rs , which has high analytic validity , 11 identies a large percentage of this group of patients for whom adjuvant chemotherapy has little or no chance of improving cancer - related outcomes , and its use is now recommended for all women in this category.8 , 12 cost - effectiveness analyses of the 21 - gene rs have varied widely and involve complex and unavoidably subjective modeling that depends on assumptions made about management strategy , impact of treatment , time horizon , inputs.13 accepted patient population , and other model estimates of the impact of the 21 - gene rs assay suggest overall absolute reductions in chemotherapy of 7% to 14% in the roughly 50 , 000 women who are newly diagnosed every year in whom testing would be recommended ( table 2 )  . 
assuming an average total adjuvant chemotherapy cost of $80 , 000 ( including modern drugs and supportive care treatments ) , 14 annual chemotherapy cost savings for women in this category would be between $280 million to $560 million per year , signicantly outpacing the roughly $175 million spent on the test for these same women ( assuming $3 , 500 per test )  . 
in this case , the value of the tbt is generated by turning a minimally effective or is indicated , and unacceptable therapy into one that therefore acceptable , because of an altered risk - benet that justies or renes treatment . 
an opt - in tbt will typically increase costs , but still has value because it may result in improved long - term clinical outcomes . an example of an opt - in tbt is provided by analysis of germline susceptibility genes , such as brca1 or brca2 , or associated genes ( table 2 )  . 
in this case , the presence of a deleterious inherited germline mutation in the brca1 or brca2 ( or related ) gene substantially increases the odds of developing and dying as a result of breast and / or ovarian cancer . 
however , the risk of developing these cancers and the odds of mortality are reduced by as much as 90% and 35% to 75% with prophylactic mastectomy and salpingooophorectomy , respectively.15 , 16 in this case , these otherwise unacceptable interventions become appropriate because of the increased chances of long - term survival as a result of the intervention in a high - risk population ( table 2 )  . 
therefore , although such tests may be relatively expensive , their value in terms of lives saved , decreased long - term medical costs , and increased economic productivity and quality of life often outweigh the immediate costs of the tests and associated downstream medical expenditures . 
this tradeoff between added costs and increased quality of life is often measured through economic metrics , such as incremental costeffectiveness ratios , which are expressed in units of cost ( dollars ) per 1 year of full quality of life , or quality - adjusted life - years ( qalys )  . 
for example , the brca test listed in table 2 , when applied to the target population , saves on average 1 qaly for every $4 , 300 spent ( $4 , 300 / qaly ) .17 opt - alt tbt the opt - alt tbt paradigm is a subcategory of opt - in . 
in this case , the value of the tbt is to help select a strategy from two or more available choices that is most likely to benet the patient , thus enhancing the precision of his or her management . 
opt - alt tbts improve outcomes via the use of appropriate , alternative , effective therapies . an example of an opt - alt tbt is illustrated by somatic mutation testing in metastatic lung adenocarcinoma to drive the use of therapies directed against genomic abnormalities ( table 2 ; opt - alt : initial rx )  . 
these abnormalities occur in various genes , including egfr , kras , alk , ros1 , erbb2 , braf , ret , and ntrk1 , which are found collectively in more than 20% of patients with metastatic nonsmall - cell lung cancer using tbts on the basis of nextthese abnormalities is generation sequencing . 
each of linked to a specic therapy that targets the genomic abnormality ( eg , erlotinib and other tyrosine kinase inhibitors ) , 18 and approximately one quarter of these patients will benet from these agents . 
in contrast , chemotherapy , which has roughly the same likelihood of benet but is associated with substantially higher toxicities , remains an soc for many of the remaining patients.19 although the clinical value in terms of quality and quantity of life is established , it is a difcult and somewhat subjective exercise to determine the true economic value of these tests , which depend heavily on the relative benets of each of the drugs in each of the many settings in which they may be used across different populations . opt - out / monitoring or opt - in / monitoring tbt in an opt - in / monitoring scenario , a patient a variation on the opt - out , opt - in , or opt - alt schema is the monitoring paradigm ( table 1 )  . 
value arises from avoiding the toxicity and cost of continuing an ineffective therapy . clinically free of apparent disease , but the tbt results indicate an impending future cancer - related event which early intervention may be more effective than waiting until the event becomes clinically evident . 
an additional variant of the opt - alt / monitoring paradigm occurs if serial tbts are used as surrogates of more expensive or inconvenient , but strongly indicated , monitoring strategies . 
in this case , the patients cancer - related outcome may not be improved by the tbt per se , but the tbt helps the patient avoid other diagnostic studies , such as radiographic imaging . 
one should note that a given tbt can fall into one or more of these use context categories , depending on the disease to which the tbt is applied and the clinical scenario . as noted , the opt / monitoring paradigm has three possibilities : opt - out / monitoring , opt - in / monitoring , or opt - alt / monitoring . 
for solid malignancies , liquid biopsies include tumor - associated proteins ( eg , carcinoembryonic antigen [ cea ] / colorectal cancer ; ca125 / ovarian cancer ; prostate - specic antigen [ psa ] / prostate cancer , and muc1 , identied by ca15 - 3 or ca27.29 / breast cancer ) , circulating tumor cells , and cell - free tumor dna . opt - out / monitoring and opt - alt / monitoring tbts might be used in many settings , and their economic value may differ in each . 
introducing earlier treatment of such patients may result in higher overall survival rates , as with patients with isolated colorectal metastases detected by an increasing cea level , 22 or may not , as in patients with ovarian and breast cancers monitored with ca125 or ca15 - 3 , respectively.23 , 24 we consider serial cea for patients with a history of colorectal cancer to have high clinical utility , and we would place this tbt for this indication in tier 1 , suggesting that reimbursement should be based on more than just commodity pricing . 
in contrast , monitoring the latter two tbts has been shown in prospective randomized clinical trials to not result in longer overall survival . we would place these markers in tier 3 , or tier x , because their clinical and economic value is not clear ( table 3 )  . 
in contrast , results of a prospective , randomized clinical trial have demonstrated that identication and treatment of hepatic oligometastases in patients with stage ii to iii colorectal cancer results in a small but denite chance of cure22 and would therefore be placed in tier 1 ( table 2 )  . 
however , the development of high - level evidence of tbts in high - risk subsets might expand their indications in the future , thus offering an incentive for biotech companies to invest in generating high - level evidence demonstrating the clinically utility of tbts . in the metastatic setting , an increasing circulating tbt either directly indicates failure of the current therapy or suggests the need for more invasive imaging to determine whether the disease is progressing . 
in this case , such tbts provide both opt - out and opt - alt information because the soc is usually to change from the apparently inactive treatment to a second or later - line treatment ( opt - alt ) or to discontinue treatment altogether ( opt - out )  . 
although few , if any , prospective randomized clinical trials exist to demonstrate the clinical utility of these markers in this use context , in general , the opt - alt paradigm is considered to be sufcient to place these tbts ( at least the circulating proteins ) in tier 2 or 3 , and they are used routinely.25 our model would suggest that reimbursement for these tbts should be commensurate with their value in managing patient care . having dened the tbt use contexts and their relative value possibilities , we propose a semiquantitative , hierarchal , tiered - based approach to help determine a reimbursement structure for tbts ( table 3 )  . 
tiers dene tbts ranging from high analytic validity and clinical utility ( tier 1 ) to less accurate analytic validity or lower evidence of clinical utility ( tiers 2 and 3 ) and tbts without conrmed clinical value ( tier x )  . 
in each case , assessment of a tbt is dependent on its specic use context as an optout , opt - in , opt - alt , or opt / monitoring tbt ( table 1 )  . 
these savings could be redistributed within the health care systeone option would be to simply use the savings , especially those generated by opt - out tbts , to reduce the cost of care . 
we maintain that this approach is unattractive , because it is likely to stie innovation for new tbts , reduce the quality of data regarding a tbts clinical utility , and further enhance the existing vicious cycle.1 rather , we argue that the value of generating high - quality tbts should instigate a redistribution of health care spending directly ( in the case of opt - out tbts ) from therapeutics to diagnostics or indirectly ( in the case of opt - in tbts ) , on the basis of the case that immediate costs should be borne by society to obtain long - term cost effectiveness . 
such redistribution of nancial resources would then stimulate greater investment into diagnostics to support r&d and reward innovation and entrepreneurship . our tiered approach provides a clear and achievable opportunity for companies to develop high - quality tbts with a guarantee for a commensurate return on investment . 
rather , tbt proposes a strategy to redistribute third - party reimbursement from unnecessary or ineffective therapies to support tbts with high clinical utility to provide a baseline assurance of reimbursement and return on investment for entities investing in tbt development . 
importantly , tbts in tiers with poor evidence ( tier 3 ) or those that are purely informative with unclear implications for management ( tier x ) cannot be expected to recoup health care resources , and we argue that such tbts should receive little , if any , third - party reimbursement . although our system does not directly reward a tbt for having slightly better performance than another for a similar indication , it does so indirectly . 
therefore , a static determination of cost effectiveness for a tbt is unrealistic . in the example of the 21 - gene rs , the cost of adjuvant chemotherapy has increased dramatically in breast cancer , in part as a result of routine hematopoietic growth factor for dose - dense treatment.14 another issue is support whether tbts should be entered into clinical practice before high loes are available , with reimbursement on the basis of a coverage - with - evidence - development approach , which has been piloted by the centers for medicare and medicaid and its afliates.27 in this case , rather than insistence on either prospective clinical trials or prospectiveretrospective4 , 5 studies , the third party payer is willing to cover the use of a tbt , with the proviso that the user or manufacturer generates evidence supporting at least clinical validity if not utility for the assay . 
this strategy represents an intriguing but special circumstance outside of our model . a key limitation of our proposed system is that there will be justiable differences in opinions regarding the relative analytic validity , meaningfulness of different clinical end points , magnitude of outcomes , and strategies to generate loes for clinical utility . 
nonetheless , this formulation is a rst conceptual and quantitative step toward what would eventually be a rened , objective , and quantitative method to assign value to emerging tbts using a practical tiered reimbursement scheme , helping to break the vicious cycle of tumor biomarker value . finally , a consideration of the proposed system would not be complete without acknowledging the critical importance of practical barriers to implementation . 
although an indepth discussion of all barriers is beyond the scope of this article , it is worth noting that efforts to implement this proposed system will require input and approval from the involved stakeholders , 1 which include the life sciences industry , private third - party payers , government and regulatory agencies , health care systems , providers and larger medical associations , and patients and patient advocacy groups . 
however , the ultimate success of this system will require large - scale adoption to provide incentives sufcient to power the proposed virtuous cycle of investment in high - quality tbt development . in conclusion , we have proposed an objective , systematic , and semiquantitative approach to guide researchers , funders , test manufacturers , clinicians , patients , and health care systems to invest health care dollars into tbt r&d . 
by providing a tiered categorical solution with clear minimum reimbursement levels , we hope to provide assurance to investors of a solid potential for return on investment via r&d into high - quality clinically useful tbts . 
by increasing entry into the market for high - quality tbts , we argue that market forces will drive real - time selection of the most clinically local useful tbt available for a given clinical context , treatment practices , and population characteristics . 
lyman consulting or advisory role : g1 therapeutics , halozyme , partners healthcare , amgen , pzer , agendia , helsinn therapeutics , celldex ( i ) , janssen ( i ) , genomic health , mylan , samsung bioepis , spectrum pharmaceuticals research funding : amgen richard l . 
schilsky research funding : astrazeneca ( inst ) , bayer ( inst ) , bristol - myers squibb ( inst ) , genentech ( inst ) , eli lilly ( inst ) , merck ( inst ) , pzer ( inst ) , boehringer ingelheim ( inst ) travel , accommodations , expenses : varian daniel f . 
hayes stock and other ownership interests : oncimmune , inbiomotion consulting or advisory role : cepheid , freenome , cellworks , cvs caremark breast cancer expert panel , agendia research funding : astrazeneca ( inst ) , puma biotechnology ( inst ) , pzer ( inst ) , eli lilly ( inst ) , merrimack ( inst ) , menarini silicon biosystems ( inst ) patents , royalties , other intellectual property : royalties from licensed technology ; diagnosis and treatment of breast cancer . 
hayes is designated as inventor / co - inventor ; title : a method for predicting progression - free and overall survival at each follow - up time point during therapy of patients with metastatic breast cancer using circulating tumor cells . 
cancer - tests / #530d572f5955 teutsch sm , bradley la , palomaki ge , et al : the evaluation of genomic applications in practice and prevention ( egapp ) initiative : methods of the egapp working group . 
harris ln , ismaila n , mcshane lm , et al : use of biomarkers to guide decisions on adjuvant systemic therapy for women with early - stage invasive breast cancer : american society of clinical oncology clinical practice guideline . 
j clin oncol 34 : 1134 - 1150 , 2016 krop i , ismaila n , andre f , et al : use of biomarkers to guide decisions on adjuvant systemic therapy for women with early - stage invasive breast cancer : american society of clinical oncology clinical practice guideline focused update . 
cronin m , sangli c , liu ml , et al : analytical validation of the oncotype dx genomic diagnostic test for recurrence prognosis and therapeutic response prediction in node - negative , estrogen receptor - positive breast cancer . 
wang sy , dang w , richman i , et al : cost - effectiveness analyses of the 21 - gene assay in breast cancer : systematic review and critical appraisal . 
balmaa j , sanz j , bonll x , et al : genetic counseling program in familial breast cancer : analysis of its effectiveness , cost and cost - effectiveness ratio . 
lindeman ni , cagle pt , beasley mb , et al : molecular testing guideline for selection of lung cancer patients for egfr and alk tyrosine kinase inhibitors : guideline from the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
rustin gj , van der burg me : a randomized trial in ovarian cancer ( oc ) of early treatment of relapse based on ca125 level alone versus delayed treatment based on conventional clinical indicators ( mrc ov05 / eortc 55955 trials )  . 
van poznak c , somereld mr , bast rc , et al : use of biomarkers to guide decisions on systemic therapy for women with metastatic breast cancer : american society of clinical oncology clinical practice guideline . 
reed sd , dinan ma , schulman ka , et al : cost - effectiveness of the 21 - gene recurrence score assay in the context of multifactorial decision making to guide chemotherapy for early - stage breast cancer . 
eiermann w , rezai m , k ummel s , et al : the 21 - gene recurrence score assay impacts adjuvant therapy recommendations for er - positive , node - negative and node - positive early breast cancer resulting in a risk - adapted change in chemotherapy use . 
pilon d , queener m , lefebvre p , et al : cost per median overall survival month associated with abiraterone acetate and enzalutamide for treatment of patients with metastatic castration - resistant prostate cancer . 
schremser k , rogowski wh , adler - reichel s , et al : cost - effectiveness of an individualized rst - line treatment strategy offering erlotinib based on egfr mutation testing in advanced lung adenocarcinoma patients in germany . 
 plasma cell - free dna testing of patients with egfr mutant nonsmall - cell lung cancer : droplet digital pcr versus next - generation sequencing compared with tissue - based results christi m.j. 
aerts , md , phd1 ; and hendrikus jan dubbink , phd , 1 on behalf of erasmus mc cancer institute purpose to compare the results of plasma cell - free dna ( cfdna ) droplet digital pcr ( ddpcr ) and nextgeneration sequencing ( ngs ) on detection of epidermal growth factor receptor ( egfr ) primary activating mutations and p.t790m with results of tissue analysis in patients with egfr mutated nonsmall - cell lung cancer . methods all patients with egfr mutated nonsmall cell lung cancer for which a pathology and a plasma specimen were available upon progression between november 2016 and july 2018 were selected . 
for the detection of p.t790m , this was 75% ( = 0.49 ) for ddpcr as well as for ngs . conclusion mutual agreement is high between ngs and ddpcr in cfdna on the level of a specic mutation , with comparable ratio results . 
plasma testing of egfr primary activating mutations and p.t790m shows high concordance with pathology results , for ngs as well as for ddpcr , depending on the extent of the panel used . 
2019 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction among cancer deaths worldwide , nonsmall - cell lung cancer ( nsclc ) is the leading cause.1 the survival of metastasized disease is poor as illustrated by a 1 - year survival rate of 23% in the netherlands between 2010 and 2015.2 the choice of palliative systemic treatment currently depends on histologic subtype , programmed cell death ligand 1 ( pd - l1 ) expression , and the presence of specic genetic aberrations ( also known as driver mutations ) for which specic targeted therapies are available.3 today , is common practice to perform molecular analysis on a tissue biopsy specimen at the time of diagnosis.3 for nonsquamous nsclc , targeted therapies have been developed and registered for treating nsclc on the basis of the presence of genetic alterations in an expanding number of genes . 
 steendam et al context key objective to compare plasma cell - free dna mutation testing by droplet digital polymerase chain reaction ( ddpcr ) and next - generation sequencing ( ngs ) with their concordance with tissue testing . knowledge generated ddpcr and ngs yield comparable results , with similar sensitivity for the mutations that can be detected by both methods , and the concordance with tissue - based results is high . 
discordant cases tend to show intrathoracic and / or cns progression . the extent of mutations that can be discovered by ngs in one step is larger . relevance when searching for a resistance mechanism , ngs analysis of cell - free dna in plasma offers a more comprehensive view than ddpcr , with comparable precision at a single mutation level . 
when no mutations are detected in plasma , tissue - based investigation remains desirable . average to rst - generation tyrosine kinase inhibitors ( tkis ) .6 all patients , however , ultimately develop resistance to treatment with tkis and show progression of disease at some point . 
there are two main mechanisms of acquired resistance : pharmacologic ( eg , problems with compliance , dose reductions , reduced absorption or increased metainadequate cns penetration ) and biologic ( eg , bolism , altered drug target , bypass tracks , phenotypic change , downstream signaling pathways ) .7 the gatekeeper mutation p.t790m in egfr exon 20 is the most common resistance mechanism to rstand secondgeneration tkis ( erlotinib , getinib , and afatinib ) nsclc with an activating egfr mutation and occurs in more than 50% of patients.7 because the availability of osimertinib , a drug that overcomes the p.t790m resistance mechanism that shows high response rates and a substantial median pfs of 8 months , the detection of this gatekeeper mutation has been of utmost importance.8 , 9 in addition , there are other known resistance mechanisms for which targeted therapies are available in research or off - label settings . 
real - time pcr slightly im ( eg , cobas [ roche , basel , proves the detection limit switzerland ] , therascreen [ qiagen , valencia , ca ] ) , but a major improvement in sensitivity was achieved by the development of digital platforms that target specic mutations like droplet digital pcr ( ddpcr ) and beads , emulsion , amplication , and magnetics digital pcr.13 this requires a modest amount of time and cfdna to obtain reliable results . 
a lot of effort was invested in optimizing ngs for use on cfdna , with adjusted amplicon sizes for amplication of smaller dna fragments and application of molecular barcodes to recognize the needle in the haystack in low concentrations of ctdna in the total amount of cfdna.14 for optimal results , it is advised to use as much cfdna in the panel as possible . 
depending on the platform used , the lead time requires several working days , which is comparable to ngs on tissue specimens . this study compares the results of ddpcr ( bio - rad laboratories , hercules , ca ) and ngs ( ion torrent , thermo fisher scientic , waltham , ma ) for detection of primary activating and resistance p.t790m egfr mutations in plasma - derived cfdna . 
outcomes are compared with ngs results of conventional tissue biopsy or cytology . methods we included all patients with egfr mutated nsclc with progression on current therapy for which a tissue specimen ( histology / cytology ) was available in the same time frame and line of treatment as plasma analysis . 
we prospectively collected all data on requested plasma analyses . cfdna isolation blood was collected in 10 - ml cellsave preservative tubes ( cellsearch , menarini silicon biosystems , castel maggiore , italy ) and centrifuged for 20 minutes at 1 , 600 g . 
the dna was eluted in 50 l of buffer . ddpcr analysis the actual analysis of egfr activating ( exon 19 deletions and p.l858r ) and resistance ( p.t790m ) mutations was performed using ddpcr mutation assays ( bio - rad laboratories ) as previously described.15 ngs on pathology specimens and cfdna dna was isolated from formalin - xed parafn - embedded tissues enriched for neoplastic cells by manual microdissection as previously described.16 ngs analysis was performed by semiconductor sequencing with the ion s5 system ( thermo fisher scientic ) with the suppliers materials and protocols . 
library preparation was performed with 1 to 10 ng of tissue dna and 4 to 50 ng of cfdna , depending on the amount of tissue or cfdna available . libraries of tissue dna were prepared with a custom - made primer panel that encompassed , among others , egfr exons 18 to 21 , kras exons 2 to 4 , erbb2 exons 19 to 21 , braf exons 11 and 15 , and the entire coding region of tp53 using the ampliseq library kit 2.0 - 384 lv ( thermo fisher scientic ) ; cfdna library preparation was performed using the oncomine lung cfdna assay ( thermo fisher scientic )  . 
templates were prepared using the ion 520 & ion 530 kit - chef and sequenced with the ion s5 sequencing kit on an ion 530 chip ( thermo fisher scientic )  . sequence data were analyzed with variant caller version 5.6.0.4 ( thermo fisher scientic )  . 
results are reported as allele ratios ( mutated alleles / [ mutated + wild - type alleles ] 100% ) in the case of at least three positive droplets ( ddpcr ) or three unique molecules ( ngs )  . statistical analysis ratios of ddpcr and ngs for p.t790m as well as for the primary activating mutation when applicable . results between november 2016 and july 2018 , 162 patients underwent cfdna analysis on plasma collected in 10 - ml cellsave preservative tubes . 
we selected all 36 patients with egfr mutated nsclc with progression on current treatment of which a histology or cytology specimen was available in the same time frame and line of treatment . the population are listed in baseline characteristics of table 1 . results of plasma analyses agreement between ddpcr and ngs was 94% ( = 0.89 ) for egfr p.t790m detection in plasma and 86% ( = 0.63 ) for detection of the primary activating egfr mutation . 
table 2 lists results of plasma and tissue analyses for all patients . in six patients ( 16.7% ) , the primary activating mutation was a less common variant that was not present in the current ddpcr panel . 
at the level of p.t790m detection , better agreement was shown , with only one patient in whom p.t790m was detected by ngs but not by ddpcr . comparison with tissue results for ngs , concordance for the primary activating egfr mutation with tissue specimens was 83% ( 30 of 36 conrmed results )  . 
cohens was calculated to evaluate the agreement between ddpcr or ngs and tissue - based results for p.t790m detection and between ddpcr and ngs on cfdna for the primary activating mutation as well as for p.t790m. intraclass correlation coefcients were calculated for the in six patients ( 16.7% ) , all with intrathoracic progression , no mutations were detected in cfdna ( mutation - negative plasma ) , whereas the tissue analysis showed the presence of egfr p.t790m in three ( 50% ) of these patients . 
 ( % ) 66 ( 45 - 85 ) activating egfr mutation exon 21 p.l858r exon 21 other lines of therapy mean before pa specimen ( range ) smoking status male female never former current unknown pack - years 1 - 15 15 - 30  . 
one patient showed stable disease as best response to osimertinib , another died before subsequent therapy could be initiated , and the clinical course of the third patient remained unknown because he was treated elsewhere . discussion this study compared two accurate and promising techniques for detection of targetable genetic aberrations in nsclc in the same plasma samples and conrms the high concordance of cfdna with tumor tissue analysis as published earlier.13 , 17 we did not calculate negative predictive value or positive predictive value because we did not consider the tissue analysis as the gold standard ; it is tumor heterogeneity might a known phenomenon that result in a mutation - negative biopsy specimen while a mutation can be present in another ( metastasized ) region . our ndings support this because three patients had p.t790m detected in plasma but not in tissue . 
we do not believe that they had false - positive ndings but , rather , that the biopsy specimen did not represent the whole spectrum of genetic aberrations of the disease . ddpcr is considered a highly sensitive pcr platform that , next to high concordance with tissue - based results , also offers high sensitivity and specicity compared with earlier pcr assays ( taqman pcr with peptide nucleic acid ; therascreen ; cobas ; and beads , emulsion , amplication , and magnetics digital pcr ) .12 , 18 ngs has proven its qualities in molecular analysis of tissue and has promising evolving capabilities for mutation analysis of cfdna.19 - 21 both techniques yield results as a percent of the total ( ratio ) , which is considered a benet over methods that merely indicate positive or negative . the moderate agreement between cfdna and tissuebased results on p.t790m detection is partly the result of mutation - negative plasma samples . 
correlation between the ratio of mutant versus total cell - free dna of next - generation sequencing ( ngs ) and droplet digital polymerase chain reaction ( ddpcr ) results . 
the mutation - negative plasma subset has a substantial negative effect on the concordance between cfdna and tissue biopsy results . on the other hand , the three patients ( 8.3% ) in whom p.t790m was detected in cfdna but not in tumor tissue also contribute to the limitation of agreement . 
these three patients might represent the concept of tumor heterogeneity , where the location of the biopsy does not represent the full spectrum of genetic aberrations of the disease.24 , 26 the p.t790m - positive cells might represent a subclone of limited extent , or another ( not yet detected ) alternative resistance mechanism might be of greater inuence ( illustrated by the patient with a pik3ca mutation in the pathology specimen )  . 
the patients who showed p.t790m in tissue analysis but not in plasma all had intrathoracic and / or cns progression , which again supports the theory that those sites are associated with a lesser rate of shedding of tumor dna into blood.25 the concordance between ngs and ddpcr in cfdna of a specic genetic aberration that is targetable for ddpcr , like p.t790m , is higher than for the broader and heterogeneous group of activating egfr mutations because not all activating egfr mutations were present in the current ddpcr panel and , thus , will be missed . 
in such cases , it is unclear whether plasma is false negative for p.t790m because of limited sensitivity of ddpcr or true negative because of absence of ctdna , as the primary activating egfr mutation also could not be detected . by the food and drug administration and european medicines agency is a fact , the expectation is that in the near future , most patients will be treated with osimertinib upfront , and p.t790m detection will be of lesser importance . 
however , mechanisms of acquired resistance on rst - line osimertinib presented at the european society for medical oncology 2018 congress showed a shift toward more mesenchymal - epithelial transition factor amplications ( 14% ) ; some secondary egfr mutations , like p.c797s ( 7% ) ; and human epidermal growth factor receptor 2 amplications ( 2% ) .28 in this light , a broader approach to investigate the resistance mechanism upon progression seems desirable . in practice , frequently , only a limited amount of material for dna investigation is available , and this is also the case for blood samples . 
an advantage is the fast lead time because ddpcr can generate a quick answer for the clinician ( ie , within 1 working day when needed )  . ngs can explore a broad spectrum of genetic aberrations in a single run , and the possibilities to detect translocations and amplications are expanding quickly . 
thus , with the expanding knowledge of resistance mechanisms and possible targeted treatments ( in development ) for these , the detection of a broad set of genetic aberrations seems desirable . 
for example , a braf v600e mutation can appear next to the primary activating egfr mutation for which a dabrafenib and trametinib combination can be added to the current treatment . 
on the other hand , ngs is more time consuming and still much more expensive than ddpcr . both plasma - based approaches are limited by the fact that some resistance mechanisms need a tissue - based diagnosis ( eg , transformation to small - cell lung cancer )  . because osimertinib showed improved pfs when used in rst - line treatment in the azd9291 versus getinib or erlotinib in patients with locally advanced or metastatic nsclc ( flaura ) trial27 and registration for this indication in conclusion , our study demonstrates that results of egfr mutation detection in cfdna by ngs and ddpcr are comparable , with a high agreement when the ratio of egfr mutant alleles to wild - type alleles is compared . 
steendam research funding : astrazeneca ( inst ) travel , accommodations , expenses : roche , boehringer ingelheim , eli lilly cor van der leest honoraria : roche , boehringer ingelheim , bristol - myers squibb , abbvie consulting or advisory role : roche , abbvie , boehringer ingelheim , bristol - myers squibb jan h . 
aerts stock and other ownership interests : amphera consulting or advisory role : eli lilly , boehringer ingelheim , msd oncology , roche , bristol - myers squibb , amphera , astrazeneca , takeda pharmaceuticals patents , royalties , other intellectual property : dendritic cellbased immunotherapy ( inst ) , proteomics in nsclc ( inst ) hendrikus jan dubbink consulting or advisory role : pzer , personal genome diagnostics , eli lilly , astrazeneca , pzer , janssen pharmaceuticals research funding : astrazeneca no other potential conicts of interest were reported . acknowledgment we thank nadine van donk for her extensive efforts and support in obtaining the ddpcr results at the department of clinical chemistry , erasmus mc rotterdam . references bray f , ferlay j , soerjomataram i , et al : global cancer statistics 2018 : globocan estimates of incidence and mortality worldwide for 36 cancers in 185 countries . 
novello s , barlesi f , califano r , et al : metastatic non - small - cell lung cancer : esmo clinical practice guidelines for diagnosis , treatment and follow - up . 
ann oncol 27 : v1 - v27 , 2016 barlesi f , mazieres j , merlio jp , et al : routine molecular proling of patients with advanced non - small - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
midha a , dearden s , mccormack r : egfr mutation incidence in non - small - cell lung cancer of adenocarcinoma histology : a systematic review and global map by ethnicity ( mutmapii )  . 
ann oncol 29 : i3 - i9 , 2018 camidge dr , pao w , sequist lv : acquired resistance to tkis in solid tumours : learning from lung cancer . 
nat rev clin oncol 11 : 473 - 481 , 2014 yang jc , ahn mj , kim dw , et al : osimertinib in pretreated t790m - positive advanced non - small - cell lung cancer : aura study phase ii extension component . j clin oncol 35 : 1288 - 1296 , 2017 9 . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american 11 . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - smallpathologists joint review . 
rolfo c , mack pc , scagliotti gv , et al : liquid biopsy for advanced non - small cell lung cancer ( nsclc ) : a statement paper from the iaslc . 
oncotarget 8 : 13611 - 13619 , 2017 van lier mg , wagner a , van leerdam me , et al : a review on the molecular diagnostics of lynch syndrome : a central role for the pathology laboratory . 
mok t , wu yl , lee js , et al : detection and dynamic changes of egfr mutations from circulating tumor dna as a predictor of survival outcomes in nsclc patients treated with rst - line intercalated erlotinib and chemotherapy . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
hou h , yang x , zhang j , et al : discovery of targetable genetic alterations in advanced non - small cell lung cancer using a next - generation sequencing - based circulating tumor dna assay . 
veldore vh , choughule a , routhu t , et al : validation of liquid biopsy : plasma cell - free dna testing in clinical management of advanced non - small cell lung cancer . 
karachaliou n , mayo - de las casas c , queralt c , et al : association of egfr l858r mutation in circulating free dna with survival in the eurtac trial . 
seki y , fujiwara y , kohno t , et al : circulating cell - free plasma tumour dna shows a higher incidence of egfr mutations in patients with extrathoracic disease progression . 
 clinically integrated sequencing alters therapy in children and young adults with high - risk glial brain tumors carl koschmann yi - mi wu chandan kumarsinha robert lonigro pankaj vats katayoon kasaian marcin cieslik xuhong cao bailey anderson kevin frank lili zhao john r . 
the goal of this study was to evaluate the feasibility , utility , and clinical impact of integrative clinical sequencing and genetic counseling in children and young adults with high - risk brain tumors . patients and methods fifty - two children and young adults with brain tumors designated by the treating neuro - oncologist to be high risk ( > 25% chance for treatment failure ; mean age , 10.2 years ; range , 0 to 39 years ) were enrolled in a prospective , observational , consecutive case series , in which participants underwent integrative clinical exome ( tumor and germline dna ) and transcriptome ( tumor rna ) sequencing and genetic counseling . 
results were discussed in a multi - institutional brain tumor precision medicine teleconference . results sequencing revealed a potentially actionable germline or tumor alteration in 25 ( 63% ) of 40 tumors with adequate tissue , of which 21 ( 53% ) resulted in an impact on treatment or change of diagnosis . 
seventeen of 20 patients ( 85% ) with glial tumors were found to have a potentially actionable result , which resulted in change of therapy in 14 ( 70% ) patients . 
 none of the sponsors played a role in the design ; data collection , management , analysis , and interpretation of the data ; preparation , review , or approval of the manuscript ; and decision to submit the manuscript for publication . corresponding author : rajen mody , md , ms , michigan medicine , d4207 medical professional building , po box 5718 , ann arbor mi , 48109 ; e - mail : rmody@ umich.edu. novel effective therapies that are based , ideally , on the unique biology of each tumor . in contrast to adult tumors , recent surveys of pediatric tumors have shown that most are driven by relatively few mutational events , many of which may be targetable with personalized clinically available agents.2 , 10 although precision medicine is an exciting potential therapeutic avenue for younger patients with brain tumors , this approach requires substantial optimization to successfully improve outcomes for children with these aggressive tumors . 
our group has successfully shown the feasibility and potential clinical utility of integrative clinical sequencing in the practice of precision oncology in pediatric and adult patients with relapsed and refractory disease , 11 , 12 and other pediatric groups have recently reported similar findings.13 , 14 two recent studies have reported targeted dna sequencing in pediatric patients with brain tumors.15 , 16 however , to our knowledge , no studies have been primarily designed to study the role of dna and rna sequencing of children and adolescents with high - risk brain tumors , with a focus on their treatment and follow - up . we therefore launched a clinical sequencing study to better understand the role of personalized genomic characterization and precision oncology in the management of these patients . 
 we performed clinically integrated tumor ( dna / rna ) and germline ( dna ) sequencing and genetic counseling for a prospective cohort of children and young adults with high - risk brain tumors . 
the pediatric mioncoseq study was approved by the institutional review board of the university of michigan medical school , and all patients or their parents or legal guardians provided informed consent ( written assent if > 10 years )  . 
 clinically integrated sequencing was performed according to previous published methodology ( data supplement ) .11 , 12 , 17 our study began using a whole - exome gene panel , as previously described . 
partway through the study of our cohort , the mioncoseq sequencing laboratory ( michigan center for translational pathology ) adjusted their panel from whole exome to a panel of 1 , 700 genes ( oncoseq1700 ) that covered all cancer consensus genes and fusion partners seen in their initially sequenced cohort ( > 1 , 000 tumors )  . 
the michigan center for translational pathology prospectively performed paired whole exome and 1 , 700 gene panel on a prospective cohort of tumors and confirmed no notable difference in reporting of cancer consensus gene alterations to clinicians . as previously described , 11 potentially actionable findings were defined as any genomic finding that could lead to a change in patient management by providing a targetable tumor molecular aberration , a change in diagnosis or risk stratification ( leading to an immediate potential therapeutic application ) , or a change in patient or family counseling by identifying cancer - related germline findings . 
for medulloblastoma , sonic hedgehog ( shh ) was the only subgroup designation considered actionable by itself . brain tumor precision medicine conference tumor sequencing results were reviewed in a multi - institutional brain tumor precision medicine teleconference held at the university of michigan and attended by seattle childrens hospital , university of california , san francisco , baylor , colorado childrens hospital , lurie childrens , childrens national , and childrens hospital of michigan . 
 opinion and to generate discussion of clinical trial availability . for discussion of targeted agents to be considered for patients , special attention was paid to likelihood of their penetration of bbb . 
for all agents ( available on or off trial ) , the university of michigan cns targeted agent prediction ( cns - tap ) rating system was developed , with seven criteria to score utility of the agent , including targeted pathway / relevance to sequencing results , preclinical data , pediatric phase i data , clinical data in cns tumors , active clinical trials for which patient is eligible , cns / bbb penetration , and relevant formulation ( pill v suspension ; see data supplement for sample checkbox evaluation of everolimus for a pik3ca mutation in a patient with diffuse intrinsic pontine glioma [ dipg ] )  . 
for patients with multiple targetable lesions , preference was given to lesions with higher variant allele fraction in tumor , when known . results feasibility of clinically integrated sequencing for children and young adults with brain tumors we screened 52 patients and enrolled 50 patients with high - risk primary brain tumors ( mean age , 10.2 years ; median age , 9.0 years ; range , 1 to 39 years ) between january 2014 and march 2017 ( fig 1 )  . 
patients were referred with a wide variety of brain tumor diagnoses , as long as their treating neuro - oncologist denoted high - risk status ( > 25% risk of progression or treatment failure )  . eighteen patients ( 36% ) had relapsed or refractory tumors ( of which we sequenced the original tumor in 12 cases ) , and 13 patients ( 26% ) had metastatic tumors at the time of enrollment ( table 1 )  . 
thirty - two patients were enrolled at the time of their original diagnoses , when they presented with either a high - risk neoplasm or a possible diagnosis that met criteria for highrisk neoplasm after pathology review . 
for all patients , tissue was obtained by standard - of - care diagnostic or therapeutic surgical procedures done either at the time of enrollment or at the time of an earlier procedure . 
of the 50 enrolled patients , 40 ( 80% ) had adequate tumor specimen for dna / rna sequencing , including 20 ( 50% ) glial tumors , 15 ( 38% ) embryonal tumors , and five ( 13% ) other tumors . 
patients with frozen tumor samples had a median time to results of 49 days . twenty - six tumors ( 65% ) underwent dna sequencing with a panel of 1 , 700 cancer - related genes ( oncoseq1700 ) , rather than whole - exome sequencing . 
rates of actionable findings were similar between both methodologies . clinical utility of integrated sequencing for children and young adults with brain tumors sequencing revealed a potentially actionable germline or tumor alteration in 25 ( 63% ) tumors , including five germline and 22 somatic tumor alterations ( two patients with both a distinct germline and tumor alteration ; table 1 )  . 
 this included 18 patients ( 45% ) who underwent a change in therapy on the basis of sequencing results and three patients ( 8% ) who received new genetic counseling for germline finding and future cancer risk . 
during the course of this study , none of these patients were found to have additional malignancies , although three of five of these patients ( and the sibling of one of these patients ) remain on annual surveillance programs for additional associated malignancies ( data supplement )  . we graded the actionable potential of the somatic mutations into category i to iv ( table a1 ) as described previously.13 category i included somatic mutations of established clinical utility ; category ii : mutations of potential utility ; category iii : other consensus cancer gene mutations ; and category iv : other genes . 
 total patients screened ( n = 52 ) enrolled patients ( n = 50 ) agreed to receive incidental genetic findings ( n = 48 ) patients with inadequate tissue , no further analysis done ( n = 8 ) patients with adequate quality and quantity of tissue ( n = 40 ) patients with incidental genetic findings returned ( n = 38 ) glial tumors ( n = 20 ) embryonal tumors ( n = 15 ) other cns tumor ( n = 5 ) ( n = 8 ) medulloblastoma ( n = 10 ) clival chordoma ( n = 1 ) anaplastic oligodendroglioma ( n = 2 ) rhabdomyosarcoma ( n = 1 ) choroid plexus tumor ( n = 2 ) pilocytic astrocytoma ( n = 2 ) pineoblastoma ( n = 1 ) meningioma ( n = 2 ) ependymoma ( n = 2 ) dipg ( n = 4 ) other glial ( n = 2 ) at / rt ( n = 2 ) etmr ( n = 1 ) fig 1 . 
children and their families were offered enrollment if they had a diagnosis of a primary brain tumor believed to have at least a 25% chance of treatment failure by their treating oncologist . 
at / rt , atypical teratoid / rhabdoid tumor ; dipg , diffuse intrinsic pontine glioma ; etmr , embryonal tumor with multilayered rosettes ; gbm , glioblastoma multiforme . actionable mutations per tumor ( range , 0 to 8 ; median , 2 )  . 
glial tumors showed more grade i to iii mutations per tumor ( average , 3.0 ; range , 0 to 8 ; median , 3 ) than embryonal tumors ( average , 1.6 ; range , 0 to 5 ; median , 1 ; data supplement )  . most targeted therapeutic interventions included use of tyrosine kinase inhibitors , histone deactylase inhibitors , or mechanistic target of rapamycin inhibitors . 
fifteen patients ( 38% ) underwent precision medicinebased therapy with agents selected through the cns - tap program , including 10 patients who also underwent radiation and one patient who underwent surgery and radiation ( data supplement )  . 
our group was heterogeneous in terms of tumor type , time of enrollment ( diagnosis or relapse ) , and whether targeted therapy was given in isolation or was followed by radiation therapy , thus limiting our ability to analyze whether targeted treatments improved treatment outcomes . 
 ( % ) 40 mean age , years median age , years histology glial tumors embyronal other metastatic local at diagnosis clinical characteristics at relapse or progression tissue used for sequencing original diagnostic material sample obtained at relapse ffpe frozen tissue feasibility adequate tissue ffpe adequate no . 
 germline finding 40 of 50 ( 80 ) therapy / diagnostic finding 26 of 36 ( 72 ) any actionable finding frozen tissue adequate 14 of 15 ( 96 ) action taken note : data presented as no . 
the most frequent reasons cited by clinicians or families of the five patients ( of 22 ) for not pursuing treatment on the basis of potentially actionable findings included selecting a nontargeted salvage chemotherapy regimen ( n = 3 ) or pursuing no therapy in the absence of clear clinical or radiologic progression ( n = 1 )  . 
 for one patient with a recurrent medulloblastoma and shh pathway upregulation , consideration of therapy with a targeted shh inhibitor , such as vismodegib , was considered , but no clinical trial was available , and the provider and family decided not to pursue off - trial use of the agent . actionable findings sequencing was of highest utility in glial tumors . 
he was treated with adjuvant temozolomide and lomustine ( ccnu ) , but magnetic resonance imaging obtained before third cycle ( including magnetic resonance spectroscopy ) was consistent with tumor progression before third cycle . 
sequencing of his tumor revealed h3f3a k27m mutation , tp53 mutation and copy loss , and cdk4 amplification and outlier expression ( all category iii ; figs 2a to 2c )  . 
 ( d ) magnetic resonance imaging of the brain ( t1 with contrast ) showed increase in size in enhancing mass after three cycles of adjuvant lomustine ( ccnu ) / temozolomide . 
tp53 , tumor protein 53 ; xrt , radiation . exception of mild hyperbilirubinemia and count suppression . as another example , a 1 - year old girl presented with a recurrent posterior fossa glioblastoma multiforme . 
she originally underwent a gross total resection at 8 months of age , multiagent chemotherapy according to children 's cancer group protocol 99703 , 20 and then focal radiation therapy with concomitant temozolomide ( after initial relapse )  . 
sequencing of her initial tumor revealed significant focal amplification of pdgfb ( 19 copies ; data supplement ) , outlier expression of pdgfb and pdgfra ( data supplement ) , and somatic mutations in setd2 , with the loss - of - function mutation in setd2 comprising 42% of the sequenced tumor fraction . 
 unfortunately , she developed additional progression and changed to a phase i trial . embryonal tumors were found to have potentially actionable results in five of 15 patients ( 33% )  . 
only two of these patients ( 13% ) underwent a change in their therapy on the basis of sequencing results ( table a1 ) both cases involved clarification or revision of the original diagnosis . thirty - eight ( 95% ) participating patients received germline sequencing results . 
 dna damage cell cycle epigenetic transcription signaling kinase cell cycle transcription tumor suppressor genes oncogenes signaling medulloblastoma subgroups glial ( n = 21 ) embryonal ( n = 15 ) gbm ( n = 8 ) dipg ( n = 4 ) other ( n = 9 ) medulloblastoma ( n = 10 ) at / rt ( n = 2 ) other ( n = 3 ) other cns tumors ( n = 5 ) fig 3 . 
 activating dna lesions ( mutation , amplification , or fusion ) were seen in 19 tumors ( 48% ) , most frequently in the mitogen - activated protein kinase signaling and mechanistic target of rapamycin / phosphoinositide 3 - kinase pathways . 
tumor suppressor mutations or deletions ( germline and / or somatic ) were seen in 32 tumors ( 80% ) , most frequently in dna damage or apoptotic signaling pathways . 
at / rt , atypical teratoid / rhabdoid tumor ; dipg , diffuse intrinsic pontine glioma ; gbm , glioblastoma multiforme ; snv , somatic nucleotide variant . deleterious germline snv somatic mutation deletion activating overexpression somatic mutation amplification germline and somatic snv amplification and overexpression other gene fusion present subtype present deletion and germline snv deletion and somatic snv are listed in table a1 . 
all patients with a new actionable pathogenic germline variant were seen in a cancer genetics clinic for counseling and additional testing in family members . molecular landscape of brain tumors in cohort tumor dna and rna sequencing allowed us to explore the molecular landscape of a diverse group of high - risk brain tumors from children and young adults . 
activating alterations ( mutation , amplification , or fusion ) in platelet - derived growth factor receptor ( pdgfr ) or fibroblast growth factor receptor ( fgfr ) pathways was seen in nine ( 45% ) of 20 glial tumors ( fig 3 ) , which is higher than previously published in any of these tumor subtypes.21 - 23 in addition , we saw potential tumor - driving rna fusions in eight ( 20% ) tumors , including novel fusions in three tumors ( lrp6 - etv6 fusion in a pediatric glioblastoma [ po - 3089 ] , an fgfr3 - phgdh fusion in a thalamic anaplastic oligodendroglioma [ po3124 ] , and an elf4 - smarca fusion in a bithalamic pediatric glioblastoma [ po - 3195 ] )  . 
the location of the fgfr3 breakpoint in this fusion is similar to that of reported fgfr3 - tacc3 fusions in adult glioblastoma multiforme.24 of note , overexpression of phosphoglycerate dehydrogenase has been shown to be a negative prognostic funding in adult glioma , possibly related to increase in glioma invasion and proliferation.25 sequencing allowed for medulloblastoma molecular group analysis in nine of 10 medulloblastomas with tissue suitable for rna library formation , by comparison with established groups of highly expressed genes in each group.26 our population of medulloblastomas was from all four groups but was enriched for group 4 tumors ( table a1 ; data supplement )  . 
one tumor ( po - 3063 ) had expression and copy number attributes of three subgroups ( wnt , shh , and group 3 )  . discussion younger patients with brain tumor diagnoses die as a result of their disease more commonly than those with any other tumor type.1 in an effort to tackle this problem , we sought to study a comprehensive integration of precision medicine into the management of this patient population . 
 a few recent studies have assessed the utility of sequencing pediatric cancers , 11 , 13 , 14 including targeted dna sequencing at diagnosis in pediatric patients with brain tumors.15 to our knowledge , our study is the first to report on the feasibility of integrating dna and rna sequencing into the clinical management of children and young adults with high - risk brain tumors at both diagnosis and relapse , along with their treatment and response . 
sequencing revealed a potentially actionable germline or somatic alteration in two thirds of brain tumors , of which one third resulted in an impact on treatment or change of diagnosis . our results demonstrate the utility of combining tumor exome dna and rna sequencing with germline dna sequencing in pediatric brain tumors . 
the brain tumors in our cohort harbored driving tumor mutations not previously known for their tumor type or seen only in a small number ( < 5% ) of tumors . 
in addition , this series supports the use of rna - seq , which identified fusions in 20% of tumors , allowed us study gene expression levels , and also helped us with identification of medulloblastoma subgroups . 
germline sequencing revealed germline cancer predisposition alterations in 13% of tumors , which is consistent with previous studies of pediatric malignancies that have included germline sequencing.11 , 13 our median turnaround time was suboptimal . 
future efforts for molecular profiling will be clinically more relevant if available within 1 to 2 weeks , and novel platforms have been able to bring the time down to days.27 the brain tumors in our younger patient cohort were found to have relatively few somatic mutational events , as compared with mutational surveys of adult brain tumors , which are more heavily mutated.28 , 29 as seen in previous surveys of pediatric cancer , 2 , 12 the somatic mutations that were present in our tumors , especially in our gliomas , were frequently targetable with personalized clinically available agents . 
of note , 14 of 17 ( 83% ) of our patients who underwent therapy changes on the basis of sequencing had a high - grade glial tumor , whereas only one of 23 ( 4% ) of our patients who did not undergo therapy change had a high - grade glial tumor . 
 although no formal survey was performed on this topic , multiple families expressed comfort with pursuing a targeted therapy without a formal second opinion because of the attendance and input from clinicians from multiple other childrens hospitals around the country . pediatric and young adult patients with gbm and dipg highlight the unique opportunities and drawbacks of precision medicine in this patient population . 
however , all of these tumors harbored multiple consensus cancer gene alterations ( category i to iii ) , with an average of 3.8 per tumor , and one with eight consensus cancer gene alterations . 
the selected targeted therapy may have led to the evolution of resistant subclonal tumor cell populations in tumors that progressed.30 recent studies have shown a variable degree of heterogeneity within pediatric and adult high - grade gliomas , which could account for treatment failure with the use of a single agent.31 , 32 current and future clinical trials will approach some of these issues by starting with multiple agents targeting nonredundant pathways.30 the timing of the biopsy is also likely important , because gliomas have also been shown to develop numerous mutations in response to cytotoxic chemotherapy and radiation.9 as a limitation of our study , a minority of our patients with progressive tumors underwent biopsy or resection at progression . 
nevertheless , targeted therapies chosen for some of these patients in our study contributed to potential clinical benefit ( although response attribution is uncertain because of previous irradiation in many cases )  . 
none of the patients receiving targeted therapy had grade 3 or 4 adverse events , cytopenia requiring transfusion , or admission for fever and neutropenia . the cns - tap tool provided a useful framework for selection of targeted agents on the basis of previously published data and the likelihood of bbb penetration . 
we are also developing a prospective trial , which will compare cns - tapselected therapy to clinician choice , as well as measuring outcomes for a more homogenous cohort prospectively compared with historical controls . 
these studies will be crucial to our understanding of the true value of targeted therapy for children with brain tumors . in summary , selection of personalized agents on the basis of integrative clinical sequencing of high - risk brain tumors of children and young adults is feasible and frequently results in change of management . 
maher , karin muraszko , patricia robertson collection and assembly of data : carl koschmann , yi - mi wu , marcin cieslik , xuhong cao , bailey anderson , kevin frank , andrew h . 
chinnaiyan , rajen mody data analysis and interpretation : carl koschmann , chandan kumar - sinha , robert lonigro , pankaj vats , katayoon kasaian , bailey anderson , kevin frank , lili zhao , john r . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . carl koschmann no relationship to disclose yi - mi wu no relationship to disclose chandan kumar - sinha no relationship to disclose robert lonigro no relationship to disclose pankaj vats no relationship to disclose katayoon kasaian no relationship to disclose marcin cieslik no relationship to disclose xuhong cao no relationship to disclose bailey anderson no relationship to disclose kevin frank no relationship to disclose lili zhao no relationship to disclose john r . 
 bernard marini speakers ' bureau : genentech / abbvie , shire jessica everett no relationship to disclose brendan mullan no relationship to disclose sandra camelo - piragua no relationship to disclose sriram venneti no relationship to disclose paul mckeever no relationship to disclose kathryn mcfadden no relationship to disclose andrew p . 
maher no relationship to disclose hugh garton no relationship to disclose karin muraszko no relationship to disclose patricia robertson no relationship to disclose dan robinson no relationship to disclose arul m . 
chinnaiyan consulting or advisory role : tempus rajen mody no relationship to disclose acknowledgment we thank the patients and families who participated in this study for their generosity and kindness . 
we also thank steven pipe , valerie opipari , maria castro , pedro lowenstein , becky sigler , coral grothe , lilly pritula , justin flees , javed siddiqui , christine brennan , erica rabban , terrence barrette , christine betts , karen giles , pallavi mohapatra , and xiaoxuan dong for their administrative or academic guidance ; none of them received compensation beyond their salaries at the university of michigan . 
we also thank participants and presenters in the university of michigan brain tumor precision medicine conference . affiliations carl koschmann , yi - mi wu , chandan kumar - sinha , robert lonigro , pankaj vats , katayoon kasaian , marcin cieslik , xuhong cao , kevin frank , lili zhao , andrew h . 
zureick , jessica everett , bailey anderson , brendan mullan , bernard marini , sandra camelo - piragua , sriram venneti , paul mckeever , kathryn mcfadden , andrew p . 
harris mh , dubois sg , glade bender jl , et al : multicenter feasibility study of tumor molecular profiling to inform therapeutic decisions in advanced pediatric solid tumors : the individualized cancer therapy ( icat ) study . 
ramkissoon sh , bandopadhayay p , hwang j , et al : clinical targeted exome - based sequencing in combination with genome - wide copy number profiling : precision medicine analysis of 203 pediatric brain tumors . 
kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identifies pathogenic germline mutations , and directs targeted therapy . 
thorarinsdottir hk , rood b , kamani n , et al : outcome for children < 4 years of age with malignant central nervous system tumors treated with high - dose chemotherapy and autologous stem cell rescue . 
to our knowledge , there are no previous reports of basal cell carcinoma of the prostate occurring in association with a germline brca2 mutation , as in the patient reported here ; however , brca2 mutations , which are a recognized risk factor for prostate adenocarcinoma , are increasingly recognized as a driver for more aggressive disease5 and as a potential therapeutic target . 
olaparib , a poly ( adp ribose ) polymerase ( parp ) inhibitor , has shown high response rates in patients with prostate cancer and defects in homologous repair.6 unfortunately , many patients receiving treatment with parp inhibitors may develop reversion mutations that restore brca function and reduce sensitivity to parp inhibition or confer resistance . 
to our knowledge , there are no reports of the successful treatment of patients with metastatic prostate cancer after brca reversion mutations . in this article , we present a patient with a germline brca2 mutation who developed de novo metastatic basal cell carcinoma of the prostate and experienced a complete clinical response with olaparib . 
 after a mixed response , the patient underwent metastasectomy and subsequently had minimal to no evidence of disease while continuing to receive olaparib maintenance . in january 2016 , a 77 - year - old man with a normal psa presented with urinary obstruction . 
a computed tomography ( ct ) scan confirmed dozens of soft tissue nodules in all lobes of both lungs , suggestive of metastatic disease , as well as an enlarged prostate with a hypodense lesion in the left lobe causing mass effect on the urethra , suggestive of malignancy . 
tumor cells stained diffusely positive for bcl2 and ttf1 ; focally positive for ck903 , ck20 , p63 , and ar ; and negative for ck7 , napsin a , chromogranin , synaptophysin , psa , erg , nkx3.1 , uroplakin , gata3 , and s100 . 
overall , the immunophenotype and morphology were compatible with basal cell carcinoma of the prostate , basaloid variant ( fig 1 )  . the patients lung metastases continued to grow rapidly , he was no longer ambulatory , and he joseph e . 
bhatt author affiliations and support information ( if applicable ) appear at the end of this article . the content is solely the responsibility of the authors and does not necessarily represent the official views of harvard catalyst , harvard university , and its affiliated academic health care centers or the national institutes of health . corresponding author : joseph e . 
 ( a ) x100 , ( b ) x400 , ( c ) x200 , and ( d ) x400 ; prostate biopsies demonstrated a high - grade carcinoma with basaloid morphology : monotonous cells with high nuclear to - cytoplasmic ratio , arranged in solid nests , with peripheral palisading , frequent comedonecrosis . 
we met him for an initial visit at this time , and targeted sequencing of his tumor was performed by foundationone ( foundation medicine , cambridge , ma ) , revealing a mutation in brca2 : s1982fs * 22 , also known as 6174delt , present at 70% allele frequency . 
after 2 months of treatment , he developed progressive macrocytic anemia , which is a known adverse effect of olaparib , and his dose was reduced to 300 mg twice daily . 
three months after initiating treatment , a ct scan of the torso revealed a dramatic response , with the innumerable pulmonary nodules and masses decreased in size and quantity throughout the lungs ( fig 2c ) and shrinkage of the hypodense lesion in the prostate . eight months after beginning treatment , the patient continued receiving olaparib , which was further dose reduced to 200 mg twice daily for anemia . 
the second mutation restored the open reading frame presumably restoring brca2 function , thereby mediating resistance to olaparib . because of frequent complicated urinary tract infections , we wished to avoid cytotoxic chemotherapy , and we continued giving olaparib while adding atezolizumab and androgen deprivation therapy ( adt ) with leuprolide acetate . 
we did not treat with adt initially because of what we thought would be a low likelihood of response for this type of tumor on the basis of the limited case series available , 8 but we added it at this point because of limited low - toxicity options . 
imaging again showed a mixed response : the four new lung nodules seen on the previous scan had disappeared , other nodules were stable to smaller , but the largest right subpleural nodule and one additional nodule continued to grow and cavitate . 
 the two growing lung nodules were resected , and the patient continues to receive olaparib monotherapy , now 28 months after diagnosis , with his most recent scan showing only a single 1.4 - cm nodule that continues to shrink . discussion we present a patient who was successfully treated for a rare disease that has no standard of care . 
the patient is notable for rationally selected targeted therapy with parp inhibition in a new tumor subtype and for further success in treatment after the development of a brca2 reversion mutation that seemed to confer resistance . 
parp inhibition is showing increasing promise across tumor types that harbor defects in homologous recombination , and mechanisms and patterns of resistance are being elucidated.9 in prostate cancer , the first case series6 reporting the successful treatment of tumors harboring defects in homologous repair with olaparib showed a response in 88% of patients with dna repair defects . 
long - term data are still evolving and have not yet been reported in this setting , but a recent abstract10 suggests that , at least in combination with adt , olaparib results in a median pfs of approximately 13 months in patients with metastatic prostate cancer . 
at the time of progression , various mechanisms of resistance have been reported , including brca2 reversion mutations , as in this patient , 11 which may be polyclonal , suggesting that these reversion mutations may be relatively common under the evolutionary pressure of parp inhibition . in the patient presented here , we elected to add atezolizumab in the hope that there could be a synergistic effect with parp inhibition . 
 preclinical rationale for this approach is based on cell culture and xenograft models where parp inhibitors upregulate pd - l1 expression , thereby attenuating anticancer immunity , and pd - l1 inhibitors resensitize tumors to t - cell killing , increasing therapeutic efficacy.12 clinical trials investigating these combinations are ongoing.13 , 14 after adding atezolizumab , this patient experienced a mixed response , and with only two lung nodules remaining , we elected to proceed with a metastasectomy . 
if reversion mutations are indeed common under the evolutionary pressure of parp inhibition , we hypothesize that the patient remains disease free , at least in part , as a result of continued efficacy of immune checkpoint blockade . 
in conclusion , to our knowledge , this is the first report of the successful treatment of basal cell prostate cancer with a parp inhibitor , and more importantly , the first report of the successful treatment of a brca2 - mutated tumor after a reversion mutation . 
 bhatt collection and assembly of data : all authors data analysis and interpretation : all authors manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors relationships may not relate to the subject matter of this manuscript . 
simper nb , jones cl , maclennan gt , et al : basal cell carcinoma of the prostate is an aggressive tumor with frequent loss of pten expression and overexpression of egfr . 
chang k , dai b , kong y , et al : basal cell carcinoma of the prostate : clinicopathologic analysis of three cases and a review of the literature . 
banda k , swisher em , wu d , et al : somatic reversion of germline brca2 mutation confers resistance to poly ( adp - ribose ) polymerase inhibitor therapy . 
clarke n , wiechno pj , alekseev b , et al : olaparib combined with abiraterone in patients ( pts ) with metastatic castration - resistant prostate cancer ( mcrpc ) : a randomized phase ii trial . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
karzai f , madan ra , owens h , et al : a phase 2 study of olaparib and durvalumab in metastatic castrate - resistant prostate cancer ( mcrpc ) in an unselected population . 
friedlander m , meniawy t , markman b , et al : a phase 1b study of the anti - pd - 1 monoclonal antibody bgb - a317 ( a317 ) in combination with the parp inhibitor bgb - 290 ( 290 ) in advanced solid tumors . 
suarez , md1 introduction genomic sequencing of colorectal cancers reveals that 16% have a very high tumor mutation burden ( tmb ) .1 three quarters of such tumors display microsatellite instability ( msi ) associated with silencing or somatic mutation of mismatch repair ( mmr ) genes . 
among advanced colorectal cancers , prevalence of pole mutations remains unknown , but only 3.5% are defective in mmr.2 pole proofreading and mmr act in concert to correct replication errors . because mmr - decient tumors often respond to therapy , 3 - 5 pole - mutated tuimmune checkpoint mors might also respond . 
pathology revealed moderately differentiated adenocarcinoma with two involved lymph nodes , classied as stage iiic disease ( pt4bn1b according to the american joint committee on cancer staging system , eighth edition )  . 
after adjuvant chemotherapy with uorouracil and oxaliplatin , computerized tomography ( ct ) scan showed no evidence of disease . three years later , biopsy of an enlarging left supraclavicular lymph node revealed a kras - mutated mss adenocarcinoma with abundant extracellular mucin and a lack of programmed death ligand 1 ( pd - l1 ) tumor cell expression by both e1l3n and sp263 antibody clones . 
the tumor - inltrating lymphocytes ( tils ) could not be assessed , because this was a lymph node metastasis and the primary tumor was unavailable . the patient received uorouracil and irinotecan plus bevacizumab . 
treatment was complicated by a small bowel stula , which required discontinuation of bevacizumab , partial small bowel resection , takedown of an enterorectal stula , and placement of a permanent rectal tube . after a 3 - month recovery from surgical complications , imaging showed new pulmonary metastases . 
the enlarging left supraclavicular nodal mass led to horner syndrome with ptosis and near syncope , which required palliative radiation . the left supraclavicular lymph node specimen obtained 3 years after surgery displayed approximately 20% tumor purity by histology . 
genomic proling with the stanford solid tumor actionable mutation panel , a hybrid capturebased next - generation sequencing assay , revealed an ultra - high tmb relative to colorectal carcinomas analyzed on the same panel ( fig 1b )  . additional testing demonstrated intact expression of mmr proteins as well as mss by polymerase chain reaction . 
the boxplot shows the median , interquartile range , and standard deviation for the tmb in 82 microsatellite - stable ( mss ) colorectal cancers ( crcs ) detected by the stanford solid tumor actionable mutation panel at the time of patient testing . 
the gray dots indicate tmb for those pole - mutated tumors reported to have responded to programmed death 1 ( pd - 1 ) blockade : two crcs and two endometrial cancers ( ecs )  . 
the box plots show the tmb for a survey of 859 tumors with likely driver mutations in mismatch repair genes that would produce microsatellite instability ( msi ) and 102 tumors with known or likely functional pole mutations ( adapted from chalmers et al16 )  . 
on the basis of the ultra - high tmb , estimated at 200 mutations / mb ( fig 1c ) , our molecular tumor board recommended immunotherapy with an immune checkpoint inhibitor . pembrolizumab was obtained for compassionate use . treatment led to a transient increase in the carcinoembryonic antigen ( cea ) from 2 , 742 ng / ml to a peak of 3 , 727 ng / ml followed by a decline to a plateau of 57 to 83 ng / ml which was maintained through 25 months of treatment and an additional 3 months of follow - up ( fig 2a )  . this was associated with resolution of pain and normalization of performance status from eastern cooperative oncology group status of 2 to 0 . 
bars above the graph indicate periods of treatment with uorouracil and irinotecan ( folfiri ) , uorouracil and oxaliplatin ( folfox ) , regorafenib , triuridine ( tfd ) and tipiracil ( tpi ) , radiation therapy ( xrt ) to the left supraclavicular mass , and the programmed death 1 ( pd - 1 ) inhibitor pembrolizumab . 
the delayed response was consistent with slow clearance of mucin after tumor cell death . the patient experienced a brief episode of localized herpes zoster and later a brief episode of asymptomatic grade 1 transaminitis . 
each episode was addressed by withholding one cycle of pembrolizumab , and each quickly resolved without sequelae . discussion in recent years , immune checkpoint blockade has emerged as a safe and effective treatment of many solid tumors . 
in particular , tumors with high level of msi and mismatch repair deciency have shown dramatic responses to treatment with inhibitors.4 , 5 similarly , accumulating immune checkpoint evidence suggests that tmb alone , independent of mmr status , correlates with response to immune checkpoint blockade for some tumor types.3 , 6 - 9 hence , mss tumors with an ultra - mutated phenotype as a result of mutations in pole or pold110 , 11 represent an intriguing subset of tumors that may also respond to immune checkpoint inhibitors . the case presented here adds to the few reports of polemutated tumors that responded to pd - 1 checkpoint blockade . 
by contrast , the responsive tumors were inconsistent in pd - l1 expression ( fig 1d )  . unlike patients in the other cases , the patient in this report began treatment with the greatest extent of disease and enjoyed the longest sustained response ( which continued beyond 28 months )  . 
radiologic density of tumors failed to change signicantly for 8 months before nally disappearing at 28 months . the dramatic response in this patient shows the potential benet of evaluating mss tumors for pole and possibly pold1 mutations . 
however , it is important to realize that some pole or pold1 mutations , particularly previously uncharacterized mutations , may prove to be passenger alterations with no effect on tmb.10 a prospective analysis of 80 , 853 patients with advanced solid tumors revealed known genomic alterations in pole in only 259 patients ( 0.3% ) , with a median tmb of 31 mutations / mb.17 the most common mutation was p.r446q ( n = 77 ) , which is uncharacterized , associated with low tmb ( less than ve mutations / mb ) , and predominantly germline . 
the two nextmost - common mutations , p.p286r ( n = 41 ) and p.v411l ( n = 29 ) , are both functional , associated with high tmb ( greater than 20 mutations / mb ) , predominantly somatic , and enriched in colorectal cancer and endometrial carcinoma . 
these were the mutations present in the four polemutant tumors that have responded to pd - 1 checkpoint blockade in this and other published reports ( fig 1d )  . however , not all pole - mutated tumors respond to checkpoint blockade . 
two colorectal cancers with the p.p286r mutation showed progressive and stable disease after 1 and more than 10 months of follow - up.15 both cases showed low levels of cd8 + tils . 
lo employment : genentech , roche stock and other ownership interests : genentech , roche gilbert chu patents , royalties , other intellectual property : rapid small volume detection of blood ammonia , patent no . 
nature 487 : 330 - 337 , 2012 koopman m , kortman ga , mekenkamp l , et al : decient mismatch repair system in patients with sporadic advanced colorectal cancer . 
br j cancer 100 : 266 - 273 , 2009 rizvi na , hellmann md , snyder a , et al : mutational landscape determines sensitivity to pd - 1 blockade in nonsmall - cell lung cancer . 
science 348 : 124 - 128 , 2015 le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 le dt , uram jn , wang h , et al : pd - 1 blockade in tumors with mismatch - repair deciency . 
n engl j med 372 : 2509 - 2520 , 2015 snyder a , makarov v , merghoub t , et al : genetic basis for clinical response to ctla - 4 blockade in melanoma . 
n engl j med 371 : 2189 - 2199 , 2014 goodman am , kato s , bazhenova l , et al : tumor mutational burden as an independent predictor of response to immunotherapy in diverse cancers . 
mol cancer ther 16 : 2598 - 2608 , 2017 . kowanetz m , zou w , shames d , et al : oa20.01 : tumor mutation burden ( tmb ) is associated with improved efcacy of atezolizumab in 1l and 2l + nsclc patients . 
santin ad , bellone s , buza n , et al : regression of chemotherapy - resistant polymerase ( pole ) ultra - mutated and msh6 hyper - mutated endometrial tumors with nivolumab . 
wang c , gong j , tu ty , et al : immune proling of microsatellite instability - high and polymerase ( pole ) mutated metastatic colorectal tumors identies predictors of response to antipd - 1 therapy . 
schrock ab , fabrizio d , he y , et al : analysis of pole mutation and tumor mutational burden ( tmb ) across 80 , 853 tumors : implications for immune checkpoint inhibitors ( icpis )  . 
gaba author affiliations and support information ( if applicable ) appear at the end of this article . authors disclosures of potential conflicts of interest and contributions are found at the end of this article . corresponding author : steven f . 
powell , sanford cancer center , 1309 w 17th st , suite 101 , sioux falls , sd 57104 ; e - mail : steven.powell@sanfordhealth.org. introduction precision oncology ( po ) is a growing treatment approach in the era of next - generation sequencing ( ngs ) and matched therapies . 
our program developed a virtual molecular tumor board ( mtb ) strategy to help guide po care . materials and methods over 18 months , eligible adult patients with advanced , incurable solid tumor malignancies were enrolled in a molecular profiling ( mp ) study using the foundation medicine ngs panel . 
results were reviewed through a weekly , videoconferenced mtb conducted across our largely rural integrated health systerecommendations from the mtb were used to identify actionable alterations ( aas )  . 
secondary outcomes included the frequency of aas , genomic matched treatments , genomic matched clinical trial enrollment , and clinical outcomes . results a total of 120 participants with a variety of advanced tumor types were enrolled . 
2018 by american society of clinical oncology introduction the emergence of next - generation sequencing ( ngs ) and genomic matched treatments ( gmts ) has spawned the field of precision oncology ( po ) .1 now that ngs has moved from academic centers to routine clinical practice , 2 po is rapidly becoming a part of standard cancer care . 
 variability in clinician understanding , tumor tissue requirements , cost concerns , limited availability of gmts , and lack of infrastructure to support testing are barriers to ngs testing in clinical practice.6 effective cancer care delivery mechanisms are needed to understand the impact of po . community oncology centers represent a major venue for the growth of po . 
nearly 85% of patients with cancer are diagnosed and treated at community - based cancer centers.7 although ngs testing is now available to providers in these settings , assistance in interpretation and access to therapies can vary . 
 although collaborative academic - community mtbs are emerging , 10 this practice has not been widely used in the community , a setting that offers many challenges for po care delivery . access to therapies is perhaps the most significant challenge in po . 
 academic centers with large clinical trial portfolios demonstrate genomic - matched clinical trial ( gmct ) enrollment rates for 3% to 11% of participants with an actionable alteration ( aa ) .11 , 12 gmcts often enroll rare patient cohorts , and implementation at a community site can be challenging . 
highlighting this access issue is the fact that only approximately 2% to 5% of patients with cancer enroll in trials as part of standard cancer care.13 furthermore , for off label drug use , relevant evidence - based guidelines are limited and variability in insurance coverage exists , which can limit drug access for food and drug administration ( fda ) approved agents . 
 although newer clinical trial models , such as the national cancer institutemolecular analysis for therapy choice ( nci - match ) trial14 and asco targeted agent and profiling utilization registry ( tapur ) 15 study , seek to improve access , po therapy is often limited to major cancer centers.16 , 17 as commercial cancer ngs panels are becoming widely available to cancer providers , our cancer program sought to determine the best approach to deliver po care . 
we developed a centralized mtb with video conferencing to all oncology sites in our largely rural community cancer progra as part of this program , we developed a prospective observational study to determine the impact of this approach in this setting . 
 eligibility criteria included patients with incurable , solid tumor malignancies who were 18 years of age ; experienced disease progression while receiving one or more prior lines of therapy or had no standard first - line treatment options available ; had a recent tissue biopsy ( 14 weeks ) available for molecular testing ; had an eastern cooperative oncology group performance status of 1 ; and had adequate organ and bone marrow function for active cancer therapy . 
patients were excluded if they had primary brain cancer , had a concurrent uncontrolled malignancy , had symptomatic or untreated cns metastases , had uncontrolled concurrent illness , were pregnant or breastfeeding , or were of childbearing potential not using adequate contraception . participants who were interested in molecular profiling ( mp ) were approached for consent ( prescreening phase )  . 
if a participant did not have tumor tissue available for testing , a new biopsy was allowed if this was felt to be clinically appropriate by the enrolling investigator . study objectives the primary objective of the study was to determine the feasibility of mp in patients with advanced cancer in the community setting . 
secondary objectives included evaluation of patient and tumor characteristics , frequency of molecular alterations , influence of mp on treatment decisions , and patient outcomes . molecular profiling mp was performed in a clinical laboratory improvement amendmentscertified , new york stateaccredited , and college of american pathologistsaccredited laboratory ( foundation medicine [ fm ] , cambridge ma )  . 
technical descriptions and validation of genomic profiling assays have been extensively described in previous publications.18 - 20 in brief , at least 50 ng dna were extracted from 40 m formalin - fixed , paraffin - embedded tissue sections with at least 20% tumor cells . 
adaptor - ligated dna underwent hybrid capture for all coding exons of 236 , 315 , or 405 cancer - related genes plus select introns from 19 , 28 , or 31 genes frequently rearranged in cancer.18 - 20 captured libraries were sequenced to a median exon coverage depth of 528 ( hiseq ; illumina , san diego , ca )  . 
resultant sequences were analyzed for short variants ( base substitutions , insertions / deletions ) , copy number alterations ( focal amplifications and homozygous deletions ) , rearrangements , and select gene fusions . 
for the purposes of this study , treatment was recommended for an aa only if the gene variant had been previously reported as actionable in the peer - reviewed literature , either from clinical or preclinical data . 
variants of undetermined significance were included in treatment decisions , but first reviewed by genetics professionals to determine whether there was strong evidence of functionality in the peer reviewed literature . 
participants who did not have an aa and / or those who were treated with non - gmts were classified as being treated as standard of care ( soc )  . 
any participant with a variant with potential germline implications was offered a referral to a genetic counselor . clinical outcomes assessment all participants enrolled in the study were followed for clinical outcomes on the basis of their mp . 
 for participants treated with an fda - approved on - label or off - label drug , new baseline tumor assessments were required within 30 days before starting recommended treatment . 
after the initial 16 weeks , tumor assessments were performed per routine clinical practice and continued until disease progression or discontinuation because of toxicity . statistical analysis sample size was not calculated but set at 120 participants with testing performed . 
patients considered evaluable for response included those who received at least two treatment cycles ( or a minimum of 6 weeks of therapy ) and underwent at least one in - study disease assessment or experienced clinical disease progression . 
kaplan - meier curves were created in r software with the survival package . results patient and tumor characteristics a total of 144 participants were screened from june 2014 to december 2015 , with 120 eligible for enrollment . 
race distribution predominantly consisted of white ( n = 114 ; 95% ) participants ; however , two latino , two asian , one native american , and one african american participant were also included . 
 case presentation provider or designee review of mp results moderator mtb discussion medical oncology genetics specialists oncology subspecialists clinical research ancillary staff treatment recommendation on - label drug off - label drug clinical trials standard of care documentation direct to provider electronic medical record fig 1 . 
the sanford mtb encompasses a large , rural geographic area ( covering > 200 , 000 square miles ) , with cancer centers in fargo , nd ; sioux falls , sd ; bemidji , mn ; and bismarck , nd . 
in addition to the physician moderator and presenting provider , the mtb discussion included practicing medical oncologists , board - certified genetics specialists ( clinical genetics , molecular genetics , cytogenetics , and genetic counselors ) , oncology subspecialists ( radiology , pathology , interventional radiology , and surgery ) , clinical research , and ancillary staff ( nursing , pharmacy , and patient advocates )  . 
colorectal ( n = 20 ; 16.7% ) , nonsmall - cell lung ( n = 20 ; 16.7% ) , and breast ( n = 15 ; 12.5% ) cancers represented the most common disease types enrolled . 
rare tumors , representing one patient each , included bladder , germ cell , duodenal , neuroblastoma , salivary , and cutaneous squamous cell cancers . molecular pathway alterations of the 120 participants who had mp performed , 109 completed testing . 
genomic matched treatment categories treatment categories fda - approved on - label drug ( companion biomarker approved ) treatment is fda approved for the identified aa in the same tumor type and is a validated companion biomarker example : erlotinib for egfr mutated nonsmall - cell lung cancer fda - approved on - label drug ( biomarker relevant , but not approved ) treatment is fda approved for the tumor type and directed at an aa predictive of response , but not validated as a companion biomarker example : everolimus for i3k - activated breast cancer fda - approved off - label treatment is directed at an aa and is fda approved for use for another indication example : vemurafenib for braf v600e mutated nonsmall - cell lung cancer genomic matched clinical trial treatment is matched to an aa that is a required for enrollment in a clinical trial example : bgj398 ( fgfr inhibitor ) for fgfr1 mutated adenoid cystic carcinoma abbreviations : aa , actionable alteration ; egfr , endothelial growth factor receptor ; fda , food and drug administration . there was an average of 4.7 genomic alterations per patient , ranging from one to 15 genomic alterations each . 
on the basis of mtb review , an aa was identified , and treatment was recommended for 63 of the 109 of patients ( 58% ) who completed testing with the fm panel . influence on treatment decisions the consort diagram in figure 2 outlines the pathway from mp to treatment assignment . 
for those who did not pursue treatment , enrollment in hospice ( n = 10 ) because of declining clinical status or standard chemotherapy ( n = 7 ) because of patient or provider preference were the most commonly chosen treatment options . 
only six participants who sought targeted therapy were denied access either by clinical trial screen failure or lack of off - label access . treatment outcomes of the 39 participants treated with gmt , the overall response rate was 12.8% ( n = 5 ) , all of which were partial responses ( prs )  . 
a total of 14 patients ( 35.9% ) had a best response of stable disease ( sd ) , and 13 ( 33.3% ) had progressive disease ( pd )  . 
 figure 3 demonstrates the kaplan - meier curves with pfs and os data from each of these two groups . discussion implementation of an easily accessible , multidisciplinary team approach to ngs testing and review resulted in a high rate of gmt in our patient population . 
 ( * ) 31% of trials ( n = 5 ) identified as an exact genomic matched clinical trial ( gmct ) match on the foundation medicine ( fm ) report . 
because of rapid changes in genomic biomarkers , relevant data , and emerging treatment options , access to these clinical trials is critical in determining the efficacy of this approach . outlined in figure 2 , our mtb was able to identify additional participants who might have benefited from gmcts beyond what was listed as an exact molecular match on the fm report . 
by using this care delivery model , we were able to enroll 14.7% of those with aas on gmcts , the majority of whom were at our centers . until recently , access to gmcts has been largely limited to major academic centers . 
md anderson has the largest series of patients in this setting , showing gmct match rates of 11% for those with an aas.12 these major academic centers often have large phase i programs and a number of relevant clinical trials . 
however , in the community , these trials are often not as easily accessible because of physician , organizational , and patient factors.22 these challenges can be magnified further with po trials because they seek to enroll unique cohorts that require specialized screening through ngs tests . 
treatment options were available through novel umbrella / basket clinical trials ( novartis signature program , 23 - 28 genentech mypathway trial29 ) and with a limited number of off - label drug options . 
improving patient access to gmcts in the community has the potential to rapidly propel this field forward . as part of this study , our group not only learned how to implement this process in our multicenter health system , but also how to adapt the program to emerging trends in po . 
since the end of our study , the pd - 1 antibody pembrolizumab was subsequently approved by the fda for any solid tumor with msi - h status.31 through our genomic tumor board review of genomic results and emerging efficacy data in msi - h tumors , we were able to identify patients who may benefit from pd - 1 inhibitors.32 two patients in this study with msi - h tumors on the basis of msh6 and mlh1 loss were identified and had exceptional , durable responses to therapy . 
this scenario highlights the fact that a multidisciplinary approach , such as described here , can provide continuous education to clinicians on rapidly emerging data on genomic biomarkers and targeted therapies . 
as such , we have now developed a subsequent program to integrate additional biomarker tests , such as programmed death ligand - 1 expression , into our mtb review process . one limitation of our study was the heterogenous patient population and the heavily pretreated , advanced stage of diseases we included . 
although several rare tumors were allowed to proceed with testing and treatment with no prior therapy , the majority of participants were being evaluated for third - line or greater therapy . 
gemma , genetic exploration of the molecular basis of malignancy in adults . treatment gmct treatment gmct time ( days ) time ( days ) previous analyses of po - guided care have suggested improved pfs data in those treated with gmt compared with soc.34 although we did not directly compare outcomes with soc , we did find similar outcomes for those treated with gmt , regardless of gmct enrollment . 
despite this , our group strongly favors enrollment in gmcts to increase the knowledge base of relevant aas and outcomes of gmt . finally , it is important to consider the number of participants ( 16% ) who had treatment recommended but declined and enrolled in hospice before they could pursue therapy . 
as the cost of ngs testing decreases and use becomes more widespread , it is important to consider its role early in diagnosis to help define future therapeutic strategies for patients . 
as we learn more effective ways to deliver po care , we can develop evidence - based guidelines around the timing of testing , appropriate disease types , and treatment selection . overall , this study demonstrates the feasibility of a po care delivery model in a largely rural community oncology syste by developing a systematic process to provide ngs testing and review results , we achieved a high rate of gmt . 
powell research funding : merck sharp & dohme ( inst ) , novartis ( inst ) , genentech / roche ( inst ) , incyte ( inst ) , bristol - myers squibb ( inst ) , pfizer ( inst ) , vyriad ( inst ) elie g . 
chung employment : foundation medicine stock and other ownership interests : foundation medicine rachel anhorn employment : foundation medicine , pfizer stock and other ownership interests : foundation medicine anu g . 
tafe lj , gorlov ip , de abreu fb , et al : implementation of a molecular tumor board : the impact on treatment decisions for 35 patients evaluated at dartmouth - hitchcock medical center . 
lynam eb , leaw j , wiener mb : a patient focused solution for enrolling clinical trials in rare and selective cancer indications : a landscape of haystacks and needles . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
 economic impact of next - generation sequencing versus single - gene testing to detect genomic alterations in metastatic nonsmall - cell lung cancer using a decision analytic model nathan a . 
pennell , md , phd1 ; alex mutebi , phd2 ; zheng - yi zhou , phd3 ; marie louise ricculli , msc3 ; wenxi tang , ms3 ; helen wang3 ; annie guerin , msc4 ; tom arnhart , pharmd , ms2 ; anand dalal , phd2 ; medha sasane , phd2 ; kevin y . 
model outcomes for each strategy were time - to - test results , the proportion of patients identied harboring alterations with or without us food and drug administrationapproved therapies , and total testing costs . 
a budget impact analysis assessed the economic effects of increasing the proportion of ngs - tested patients . results in a hypothetical 1 , 000 , 000 - member health plan , 2 , 066 medicare - insured patients and 156 commercially insured patients were estimated to have mnsclc and to be eligible for testing . 
2019 by american society of clinical oncology lung cancer ( nsclc ) , introduction nonsmall - cell the most common type of lung cancer , 1 can be classied on the basis of the presence of genomic alterations in driver oncogenes , 2 , 3 such as egfr , alk , ros1 , kras , braf , met , her2 , ret , and ntrk1.2 - 4 in the united states , several theratarget egfr , alk , ros1 , and braf pies that v600e alterations5 - 7 have been approved by the us food and drug administration ( fda ) therapy for patients with metaacross lines of static nsclc ( mnsclc )  . 
other targeted therapies are in clinical including those trial phase , against met , her2 , ntrk1 , and ret alterations identier : nct01639508 ; ( clinicaltrials.gov nct02414139 ; nct02716116 ; nct01336634 ; nct02097810 )  . improve treatment targeted therapies have been demonstrated to signicantly response and progression - free survival7 - 9 ; therefore , it is important to identify patients with specic genomic alterations to individualize treatment and optimize outcomes.2 , 9 currently , a number of testing strategies are available with which to identify genomic alterations in nsclc . 
 pennell et al context key objective to determine the least costly strategy for testing for all recommended molecular abnormalities in patients with nonsmall - cell lung cancer ( nsclc ) at diagnosis . knowledge generated upfront next - generation sequencing ( ngs ) testing for all relevant molecular targets in nsclc is less costly than performing single - gene testing , no matter what testing strategy is used . 
upfront ngs testing also results in the largest number of patients with targetable genetic alterations being identied in the shortest period of time . relevance as more clinically relevant genetic targets in nsclc emerge that require routine testing at diagnosis , it is vital to identify the molecular testing strategy that is timeliest , spares the most tissue , and is most cost efcient , as this must be done in every new patient . 
our model illustrates that moving from sequential single - gene tests or even panels of tests to broader ngs testing for patients with advanced nsclc is already the best strategy in these three areas and will only become more relevant as the list of tests grows . 
stakeholders should consider moving to ngs as the preferred method for biomarker testing . single - gene tests for less common alterations.10 sequences of single - gene tests can also be used without hotspot panel , typically testing for the most common alterations rst and less common alterations last.10 in either case , running a sequence of single - gene tests can be time consuming and may require a relatively large tissue sample , which is not always available as nsclc is often detected at an advanced stage and only small biopsy samples are usually attainable.11 - 13 as a result , one or more rebiopsies may be needed to complete the sequence . 
in recent years , next - generation sequencing ( ngs ) has emerged as a reliable strategy to simultaneously test for multiple alterations using a single tissue sample14 ; however , only a small percentage of patients with nsclc currently receive ngs , 15 as a number of practical barriers hinder its wider adoption , including limited patient access , a lack of awareness and communication within medical care teams about the benets of ngs , limited coverage , and low reimbursement rates.16 , 17 in addition , given the relatively recent development of ngs , there is a need to better understand the economic implications of using ngs versus other testing strategies in real - world clinical practice . therefore , a decision analytic model was developed to estimate the difference in testing costs and time - to - test results between ngs and commonly used single - gene testing strategies among patients with mnsclc from the perspective of the centers for medicare & medicaid services ( cms ) and a us commercial payer . 
in addition , the budget impact of increasing ngs testing was assessed from the perspective of both cms and a us commercial payer . methods model overview a decision analytic model was developed in microsoft excel 2016 from the perspective of cms and a us commercial payer for patients with newly diagnosed mnsclc who were eligible for genomic testing to determine mnsclc alteration status and inform treatment selection . 
alterations included in the model involved the programmed cell death protein 1 and its ligand programmed death protein 1 ligand ( pd - l1 ) , as well as genes egfr , alk , ros1 , braf , kras , met , her2 , ret , and ntrk1 . 
four genomic testing strategies were considered . upfront ngs : at mnsclc diagnosis , patients received a panel that tested simultaneously for all alterations with and without fda - approved therapies ( egfr , alk , ros1 , braf , met , her2 , ret , and ntrk1 )  . sequential testing : patients received a sequence of singlegene tests for alterations with fda - approved therapies ( egfr , alk , ros1 , and braf )  . 
negative test results for all four alterations were followed by either a sequence of single - gene tests or ngs to test for alterations without fda - approved therapies ( met , her2 , ret , and ntrk1 )  . 
single - gene tests were assumed to be ordered in sequence , one at a time , after receiving negative results for each previous test . exclusionary testing : patients rst received a test for kras because kras is the most common mutation in lung adenocarcinoma , and as the genetic alterations of interest are mutually exclusive , a positive test would prevent the need for additional testing . 
negative results were followed by either a sequence of single - gene tests or ngs to test for alterations without fda - approved therapies ( met , her2 , ret , and ntrk1 )  . all four testing strategies included pd - l1 and routine immunohistochemistry testing , which were assumed not to time because they were conducted sitake additional multaneously with the rst test in sequential and exclusionary testing and at the same time as the hotspot panel and ngs . 
appropriate therapyeither targeted therapy or nontargeted therapy ( eg , chemotherapy and immunotherapy ) was selected on the basis of the test results , that is , a conrmed alteration with or without fdaapproved therapies or no known alteration . 
patients who received rst - line nontargeted therapy and who tested negative for alterations with fda - approved therapies were assumed to continue testing with ngs or single - gene tests for alterations without fda - approved therapies , provided that enough tissue sample remained . 
a proportion of patients with alterations without fda - approved therapies were assumed to receive a benet from participating in clinical trials of agents under development . model inputs epidemiology and population inputs . 
for cms , the diagnosis of metastatic nsclc ( biopsy performed ) sequential exclusionary hotspot panel positive for tested alteration negative for tested alteration positive for tested alteration negative for tested mutation negative for tested mutation negative for tested mutation positive for tested alteration exclusionary mutation ( kras positive ) appropriate therapy appropriate therapy appropriate therapy appropriate therapy appropriate therapy enough tissue / no need for rebiospy insufficient tissue / need rebiopsy negative for tested mutation positive for tested alteration successful rebiopsy no rebiopsy / failed rebiopsy continue testing until appropriate treatment appropriate treatment appropriate treatment continue testing until appropriate treatment legend : continue testing for next alteration until the decision is made for appropriate treatment . is there sufficient v insufficient tissue and need for rebiopsy to continue testing ? fig 1 . 
sequential testing : sequence of single - gene tests for egfr , alk , ros1 , and braf , followed by either a sequence of single - gene tests or ngs for met , her2 , ret , and ntrk1 . 
hotspot panel : panel testing simultaneously for egfr , alk , ros1 , and braf , followed by either a sequence of single - gene tests or ngs for met , her2 , ret , and ntrk1 . 
epidemiology , population , and testing cost inputs variable commercial payer source patient population in the health care plan , no . 1 , 000 , 000 1 , 000 , 000 assumption adults in the population of interest , % * cms : kaiser family foundation18 ; commercial : us census bureau19 no . 
unit costs for all genomic alteration testing were based on the 2017 clinical lab fee schedule23 for the medicare - insured population and from dalal et al15 for the commercially insured population using two us administrative claims databases ( table 1 )  . 
single - gene tests for kras , egfr , her2 , and braf were assumed to be performed using real - time polymerase chain reaction . pd - l1 tests were assumed to be performed using immunohistochemistry or uorescence in situ hybridization . for each testing strategy , the per - patient cost of sequential , exclusionary , and hotspot panel testing was considered to be the sum of the cost of each individual test for pd - l1 and alterations with or without fdaapproved therapiesegfr , alk , ros1 , braf , met , her2 , ret , ntrk1 , and krasmultiplied by the proportion of patients who received each test , which was determined by the results for the preceding testing and rebiopsy failure rate ( table 2 )  . 
the difference between the plan - total testing costs of a certain strategy and those of ngs was considered as the cost savings associated with ngs versus the strategy in question . 
as a result of insufcient tissue sample , 8% of patients were assumed to require rebiopsy to continue testing.22 of these patients , only 30% were assumed to be actually rebiopsied , with 15% experiencing failure with rebiopsy.28 on the basis of on handorf et al , 28 rebiopsy cost was $415.30 for medicare - insured patients and $1 , 399.80 for commercially insured patients . 
one half of patients who tested negative for alterations with fda - approved therapies and who received nontargeted therapy were assumed to continue testing for alterations without fda - approved therapies . 
of these patients , 75% were assumed to continue testing with ngs and 25% with one of the other testing strategies . model outputs model results for ngs were compared with those for sequential , exclusionary , and hotspot panel testing in terms of differences in the estimated total cost associated with testing , calculated separately for cms and the commercial payer ; time - to - test results that accounted for the time associated with test turnaround and rebiopsy , assumed to be the same for cms and the commercial payer ; and the proportion of patients identied by each testing strategy as harboring alterations with or without fda - approved therapies . budget impact analysis we conducted a budget impact analysis to assess the effects of increasing upfront ngs testing in cms and commercial plans . 
total cost and cost difference versus ngs medicare - insured patients ( n = 2 , 066 ) commercially insured patients ( n = 156 ) testing strategy sequential exclusionary hotspot panel total cost 2 , 190 , 499 3 , 721 , 368 3 , 584 , 177 4 , 331 , 295 note . 
costs are given in 2017 us dollars . abbreviation : ngs , next - generation sequencing . cost difference v ngs total cost cost difference v ngs 1 , 530 , 869 1 , 393 , 678 2 , 140 , 795 620 , 369 747 , 771 624 , 178 871 , 211 127 , 402 3 , 809 250 , 842 the other parameters at their base - case values . 
on the basis of commercial payer for the 156 commercially insured patients , ngs rates , remained the least expensive testing option , with cost savings of $3 , 809 versus exclusionary testing , $127 , 402 versus sequential testing , and $250 , 842 versus hotspot panel testing . time to receive test results the cumulative time to receiving full test results and initiating treatment , incorporating both testing time and time for rebiopsy , is a critical element in molecular testing . 
proportion of patients identied with alterations with or without fda - approved therapies patients identied with alterations with fda - approved therapies ( medicare insured , n = 446 ; commercially insured , n = 34 ) patients identied , % difference v ngs , % difference in no . 
the only exception was ngs versus exclusionary testing for commercial payersranging from $19 , 943 to $27 , 562likely because of the relatively small base - case cost savings results ( $3 , 809 )  . 
results were most sensitive to scenarios in which test unit costs and the proportion of patients tested for alterations without fdaapproved therapies were varied . discussion several testing strategies for the detection of genomic alterations in nsclc exist in clinical practice ; however , scant evidence is available on the comparative economic implications of using these strategies in patients with mnsclc . 
accordingly , an economic model was developed to estimate the time - to - test results ; the proportion of patients identied as harboring alterations with or without fda - approved therapies ; and testing costs associated with upfront ngs , sequential , exclusionary , and hotspot panel testing among patients with mnsclc . model results demonstrate that ngs was associated with the same ( as hotspot panel ) or shorter ( v exclusionary and sequential testing ) time - to - test results and lower testing costs than sequential , exclusionary , and hotspot panel testing . both ngs and hotspot panel testing had the shortest time - totest results ( 2 weeks ) , indicating that these two testing strategies may yield the shortest time to initiation of appropriate therapy among the four strategies considered here . of note , although the unit cost of ngs was higher than that of individual single - gene tests , the overall cost , which included testing and rebiopsy cost , to test for a broad range of alterations was the lowest for ngs . 
although no treatment is yet approved for these alterations , it is important to identify these patients to give them the opportunity to participate in clinical trials of investigational therapies . although prior studies have discussed the cost effectiveness and benets of various testing strategies in patients with nsclc , 31 - 34 the current study is , to our knowledge , the rst to quantify the economic impact of using ngs versus other testing strategies to detect a comprehensive list of alterationsegfr , alk , ros1 , braf , met , her2 , ret , ntrk1 , and krasin patients with mnsclc in the united states . 
from a clinical standpoint , the timely identication of genomic alterations in patients with mnsclc is key to initiating the most appropriate treatment course on the basis of either targeted therapy , if available , or nontargeted therapy . 
as the results of the current study indicate , upfront ngs seems to be the cheapest broad molecular testing strategy for genomic alterations in terms of both time - to - test results and testing costs . 
furthermore , unlike other testing strategies , ngs allows for the simultaneous screening of both common and less common alterations , which is important because less common alterations are less likely to be tested when using sequential testing strategies . 
in a retrospective review of genomic testing patterns in patients with nonsquamous mnsclc , only 63 of 814 patients were reported to have undergone testing for all seven alterations recommended by national comprehensive cancer network for patients with mnsclc , namely egfr , alk , ros1 , braf , met , ret , and her2.17 using ngs may increase the number of patients tested for including both common and less common alterations , those recommended by the national comprehensive cancer network , thereby providing more information to physicians and patients with which to make informed and timely treatment decisions . 
future studies should also assess the clinical implications of our nding that , as a result of longer time - totest results , patients using sequential and / or exclusionary testing are able to initiate targeted therapy nearly 3 weeks later than patients using ngs or hotspot panel testing . 
it is worth noting that , whereas this study suggests that ngs is a more efcient testing strategy than sequential , exclusionary , and hotspot panel testing , several barriers to wider adoption of ngs in clinical practice remain , including limited coverage and reimbursement.17 however , this may change over time given that the lower total testing costs and shorter initiationof ngs , together with a reduced need for rebiopsy , may reduce medical costs substantially and improve outcomes , beneting patients and payers alike . resultsand thus treatment time - to - test this study has some limitations . 
first , as the study is based on a modeling approach using a decision tree and budget impact inputs and assumptionssome of framework , the model which were based on expert opinionmay contain uncertainty or may have limited generalizability . 
last , the model included only testing costs and not therapy costs and benets , the inclusion of which would allow for an estimate of a wider spectrum of costs . in conclusion , for both cms and commercial payers , upfront ngs testing was associated with the same ( as ( v exclusionary and hotspot panel testing ) or shorter sequential testing ) time to the initiation of appropriate treatment , as well as substantial cost savings compared with all other testing strategies in patients with newly diagnosed mnsclc . 
pennell , alex mutebi , zheng - yi zhou , marie louise ricculli , wenxi tang , helen wang , annie guerin , tom arnhart , anand dalal , kevin y . 
pennell , alex mutebi , zheng - yi zhou , marie louise ricculli , wenxi tang , helen wang , annie guerin , tom arnhart , anand dalal , medha sasane , kevin y . 
pennell consulting or advisory role : astrazeneca , eli lilly , regeneron , cota healthcare , merck research funding : genentech ( inst ) , celgene ( inst ) , astrazeneca ( inst ) , pzer ( inst ) , merck ( inst ) , loxo ( inst ) , altor bioscience ( inst ) , spectrum pharmaceuticals ( inst ) , bristol - myers squibb ( inst ) tom arnhart employment : novartis , alexion pharmaceuticals stock and other ownership interests : alexion pharmaceuticals anand dalal employment : novartis stock and other ownership interests : novartis medha sasane employment : sano , novartis ( i ) stock and other ownership interests : sano , novartis ( i ) kevin y . 
wu employment : novartis , astrazeneca stock and other ownership interests : novartis , astrazeneca , gilead sciences , intercept pharmaceuticals , merck , organovo , takeda , seattle genetics , tg therapeutics kenneth w . 
transl respir med 1 : 6 , 2013 kohno t , nakaoku t , tsuta k , et al : beyond alk - ret , ros1 and other oncogene fusions in lung cancer . 
expert rev mol diagn 16 : 737 - 749 , 2016 barlesi f , mazieres j , merlio jp , et al : routine molecular proling of patients with advanced non - small - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
lancet 387 : 1415 - 1426 , 2016 kris mg , johnson be , berry ld , et al : using multiplexed assays of oncogenic drivers in lung cancers to select targeted drugs . 
dalal aa , guerin a , mutebi a , et al : economic analysis of braf gene mutation testing in real world practice using claims data : costs of single gene versus panel tests in patients with lung cancer . 
levy bp , chioda md , herndon d , et al : molecular testing for treatment of metastatic non - small cell lung cancer : how to implement evidence - based recommendations . 
yang p , allen ms , aubry mc , et al : clinical features of 5 , 628 primary lung cancer patients : experience at mayo clinic from 1997 to 2003 . 
reck m , rodrguez - abreu d , robinson ag , et al : pembrolizumab versus chemotherapy for pd - l1 - positive non - small - cell lung cancer . 
chen d , zhang lq , huang jf , et al : braf mutations in patients with non - small cell lung cancer : a systematic review and meta - analysis . 
meng d , yuan m , li x , et al : prognostic value of k - ras mutations in patients with non - small cell lung cancer : a systematic review with meta - analysis . 
handorf ea , mcelligott s , vachani a , et al : cost effectiveness of personalized therapy for rst - line treatment of stage iv and recurrent incurable adenocarcinoma 29 . 
vanderlaan pa , yamaguchi n , folch e , et al : success and failure rates of tumor genotyping techniques in routine pathological samples with non - small - cell lung 5 : 293 - 305 , 2011 22 : 2616 - 2624 , 2011 cancer 18 : 651 - 659 , 2017 snapshot / 2005 prevalence / canques.html 375 : 1823 - 1833 , 2016 2014 cancer 81 : 1 - 10 , 2013 of the lung . 
 clinical utility of gene expression classifiers in men with newly diagnosed prostate cancer purpose tissue - based gene expression classifiers ( gecs ) may assist with management decisions in patients with newly diagnosed prostate cancer . 
we sought to assess the current use of gec tests and determine how the test results are associated with primary disease management . methods in this observational study , patients diagnosed with localized prostate cancer were tracked through the michigan urological surgery improvement collaborative registry . 
practice patterns , predictors of gec use , and effect of gec results on disease management were investigated . results of 3 , 966 newly diagnosed patients , 747 ( 18.8% ) underwent gec testing . 
this results in an estimate that , for every nine men with favorable risk of cancer who undergo gec testing , one additional patient may have their disease initially managed with as . 
although active surveillance ( as ) is now recognized as a preferred treatment option for patients with low - risk prostate cancer , more than one third of patients will experience disease progression that requires treatment.1 - 3 men with favorable intermediate risk prostate cancer are rarely entered onto as , yet growing data suggest that some may be safely treated with as to avoid immediate radical therapy.4 multiple new tissue biomarkers have surfaced to aid in risk stratification of newly diagnosed patients , with a goal of improving prognostic accuracy compared with routine clinicopathologic variables . 
on the basis of multiple retrospective development and validation studies , there are now three widely available tissue - based gene expression classifiers ( gecs ) for use in this setting : prolaris ( myriad genetics , salt lake city , ut ) , oncotype dx prostate ( genomic health , redwood city , ca ) , and decipher prostate biopsy ( genomedx , vancouver , canada ) .5 - 12 these tools are now included in the national comprehensive cancer network ( nccn ) jonathan c . 
 guidelines as options to aid in decision making for men with newly diagnosed localized prostate cancer , although other national guidelines caution against their routine use.13 , 14 each of these tests are rna - based prognostic biomarkers that analyze a distinct multigene panel that predicts oncologic end points , which range from the likelihood of harboring unrecognized high - grade disease to death as a result of prostate cancer at 10 years . 
 although published data have demonstrated the prognostic utility of these tests compared with clinicopathologic data alone , 7 , 9 , 11 , 12 there is limited understanding of how these tools influence treatment decisions in the contemporary setting . one unique aspect of these tests is the continuous scale used to report risk , whether for near - term adverse pathology end points or more distant survival end points . 
this is in contrast to breast cancer , for which analogous tests have become incorporated into guidelines as a result of multiple prospective trials that validate discrete cut points for management decisions.15 - 17 because the emergence of multiple gec tests each with various measurement scales , thresholds , outcomes , and reporting toolsis recent , it is unclear how these tests affect real - world management decisions . to address this complex issue in localized prostate cancer , we sought to perform a prospective clinical utility study by tracking the use of gecs in patients with newly diagnosed prostate cancer and comparing treatment decisions according to gec result . 
to capture gec use and subsequent management across a broad cohort of patients , this study was performed through the michigan urological surgery improvement collaborative ( music ) , a consortium of more than 90% of urology practices in the state of michigan . 
we hypothesized that gec use would be highly variable and that results would correlate closely with subsequent treatment decisions , specifically that rates of as would be higher in gec - defined low - risk patients . methods study population within music . 
in each participating practice , trained abstractors prospectively enter a standardized set of demographic and pathologic data for every patient with a new prostate cancer diagnosis into an electronic clinical registry . 
abstractors also enter data related to treatmentradical prostatectomy , radiotherapy , or other ( primary androgen deprivation therapy , high - intensity focused ultrasound , cryotherapy , or other ablative technologies ) and follow - up data . 
each site obtains regulatory exemption from local institutional review boards to participate in music , and funding is provided by blue cross blue shield of michigan . in this analysis , we included all men who were newly diagnosed with clinically localized prostate cancer between january and september 2017 . 
subsequent treatment decisions ( as , prostatectomy , or radiotherapy ) were tracked until the analytic data set was locked on april 1 , 2018 . clinical and pathologic variable definitions data elements collected included age , ethnicity , prostate - specific antigen ( psa ) level , number of positive cores from biopsy , primary and secondary gleason patterns , prostate volume , clinical t stage , body mass index ( bmi ) , and comorbidity scores . 
prostate magnetic resonance imaging ( mri ) was categorized according to maximum prostate imaging and reporting data system ( pirads ) version 2 score as reassuring ( pirads 1 to 3 ) or nonreassuring ( pirads 4 to 5 )  . 
using standard clinicopathologic parameters , patients were categorized according to the favorable - risk prostate cancer stratification that has been widely disseminated in the music consortium as a way to identify patients who may be most appropriate for as.18 favorable - risk prostate cancer was defined by a biopsy gleason score of 6 or low - volume , gleason 3 + 4 = 7 disease ( defined as three or fewer cores positive and no core with > 50% cancer volume )  . 
 accordance with published data and test reports for each of these assays.19 a summary of the three assays and cut points used to define gec low - risk disease are listed below : decipher biopsy ( genomedx biosciences ) : microarray platform , with score composed of 22 rna biomarkers reported on a scale of 0 to 1 . 
threshold for low versus high risk is 0.45. oncotype dx prostate ( genomic health ) : quantitative real - time polymerase chain reaction platform , with score composed of 17 genes and reported on a scale of 0 to 100 . 
 threshold for low versus high risk is the probability of adverse surgical pathology greater than 20% . prolaris ( myriad genetics ) : quantitative real - time polymerase chain reaction platform , with score composed of 46 genes and reported on a scale of 1 to 10 . 
threshold for low versus high risk is 10 - year mortality risk of 3% or greater . for patients who had more than one test performed ( n = 13 ) , only the initial test was included in the analysis . end points the primary study outcome was gec testing status ( did not undergo gec testing v underwent gec testing with result below threshold v underwent gec testing with result above threshold )  . 
patients whose data were lost to follow - up , deceased , or switched practices for follow - up care were excluded from the evaluation of treatment because music no longer collected treatment information . 
patients who were still missing treatment data at the time of analysis because of a lag in data entry were also excluded . statistical analyses patient characteristics were compared between those who did and did not undergo gec testing using 2 tests for the overall cohort as well as for patients with favorable - risk prostate cancer . 
the proportion of patients with a test result above the threshold was then summarized by the type of the test used ( prolaris v oncotype dx v decipher )  . 
the primary management strategy was then compared across three groups defined by the performance and result of the gec test : no test , gec test below the threshold , and gec test above the threshold . 
the model included the performance and result of the gec test ( above or below the threshold ) as the primary predictor ( with no test as the reference group )  . 
the model also adjusted for patient and practice - level characteristics , including patient age , ethnicity , psa level , biopsy gleason score , clinical t stage , comorbidity , bmi , practice size , and practice type ( academic v private )  . 
among this subgroup , patients who underwent a gec test were more likely to be african american and to have a higher biopsy gleason score ( 3 + 4 v 6 ) , fewer positive cores , and nccn intermediaterather than low - risk cancer ( p < .05 for each ; appendix table a1 )  . 
seven practices ordered a gec test on more than 50% of patients with newly diagnosed prostate cancer . among the 747 patients who underwent gec testing , 439 ( 59% ) were tested with prolaris , 81 ( 11% ) with oncotypedx , and 227 ( 30% ) with decipher . 
gec testing was performed in 367 ( 17.6% ) of 2 , 080 patients with unfavorable risk ; 61 of these men ( 16.6% ) had a low - risk result , and 17 ( 27.9% ) elected as for initial management . of the 1 , 487 patients with favorable - risk disease but with treatment data , 320 ( 22% ) underwent gec testing . 
only 30 patients with favorable - risk disease underwent both mri and gec testing ; this represented 16% of patients who underwent mri and 9% of patients who underwent gec testing ( appendix table a2 )  . 
gec testing and use of as appeared to be independent of each other at a provider level , which indicated the absence of any provider - specific effect ( correlation coefficient r = 0.16 ; appendix fig a2 )  . with 63% of patients with favorable - risk prostate cancer harboring gec low - risk disease in this cohort ( 203 of 320 who underwent gec testing ) , these data suggest that , for every nine patients with favorable - risk disease who undergo testing , one patient will receive as who would have otherwise undergone primary therapy . 
 conversely , 117 ( 37% ) of 320 gec - tested patients with favorable - risk prostate cancer were considered molecularly high risk , and 46 ( 39% ) of these 117 patients selected initial definitive management compared with 337 ( 29% ) of 1 , 167 untested patients . 
patient and practice characteristics stratified by gec testing ( continued ) characteristic all patients ( n = 3 , 966 ) gec test performed ( n = 747 ) gec test not performed ( n = 3 , 219 ) practice size , no . 
more granular clinical tools to quantify risk , including the cancer of the prostate risk assessment25 score and memorial sloan kettering cancer center26 nomograms , can be affected greatly by variability among pathologists and are still somewhat limited in their prognostic accuracy.27 , 28 emerging tools , such as multiparametric mri ( mpmri ) , may improve the initial detection of more aggressive tumors , but variability in the performance and interpretation of mpmri may limit its generalizability for now.29 gec testing provides an additional objective tool for risk stratification . 
prospective data suggest that up to 67% of patients may be reclassified into different risk categories when genomic risk is considered in addition to conventional clinicopathologic parameters of risk.11 despite this , limited data describe the use of gec testing in this setting , and the effect of these tools on clinical decision making has not been well established . 87 112 152 243 133 165 practice ascopubs.org / journal / po jco precision oncology fig 1 . 
practice - level rate of genomic test after diagnosis : rate of gene expression classifier ( gec ) testing in newly diagnosed men with prostate cancer at each practice ( practices are numbered 1 through 44 )  . 
 the overall rates and rates within patient subgroups are presented separately . overall ( n = 747 ) patients with favorable risk ( n = 336 ) patients with unfavorable risk ( n = 411 ) patients with gleason score 3 + 4 = 7 ( n = 296 ) patients with gleason score 3 + 3 = 6 ( n = 215 ) a number of unique findings are presented in this study , because this is the first study , to our knowledge , to report on a prospective observational cohort of patients with and without gec testing . 
approximately 20% of patients diagnosed during the study period underwent a gec test , and there was wide variation in testing patterns across different urology practices in the state of michigan . 
fitting with the current approval details for each test , which are primarily for men with favorable - risk disease , these tests were more likely to be obtained in the setting of clinically less aggressive disease . 
patients were more likely to undergo testing if seen at a larger urology practice ( with more than 10 providers ) , which may relate to incorporation of gec testing into clinical care pathways at some of these practices . the analysis of the primary end point , clinical utility of gec testing in favorable - risk prostate cancer , provides key information about how these tests affect treatment decisions . 
this is one of the key measures used by the molecular diagnostic services program developed by palmetoto gba to determine medicare coverage , and prospective data that compare tested and untested patients . 
multivariable logistic regression model to assess variables associated with active surveillance among patients with favorable - risk prostate cancer variable gec ( ref : no test ) below threshold above threshold race ( ref : white ) african american biopsy gleason grade ( ref : 6 ) clinical t stage ( ref : ct1 ) ct2 or higher charlson comorbidity index ( ref : 0 ) practice size , no . 
the model also included random intercepts for practices . abbreviations : bmi , body mass index ; gec , gene expression classifier ; or , odds ratio ; psa , prostate - specific antigen ; ref , reference . underwent as instead of surgery or radiation for every nine patients tested and that one additional patient underwent primary therapy rather than as for every 26 patients tested . 
in the unfavorable - risk group , utility was less apparent : 17% of tested patients had gec low risk disease , and only 28% of these men received as . finally , it is important to note that meaningful differences existed among the three tests . 
 although we did not have sufficient data to compare test results for patients with more than one gec assay performed , we found substantial variability in the likelihood of gec highversus gec low - risk disease , depending on the test performed . 
for example , in the subgroup with a gleason score of 3 + 3 = 6 , 13.7% of patients tested with prolaris had results that were considered above the threshold , whereas 58.3% were above the threshold as reported by decipher . 
 importantly , although most of these test - specific thresholds have not been validated , they are included in test reports provided to patients and providers.30 this issue highlights the challenges of applying thresholds to tests developed and validated for assessment along a continuum of risk and also emphasizes the need for research to compare the predictive accuracy of each of these tests . 
although that was not the case in this cohort , additional study about appropriate and consistent thresholds for these tests is paramount . it is important note key limitations to this study . 
 some patients could have undergone gec testing outside of a music urology practice , such as by a radiation oncologist , and this would only be captured in the registry if the test results were provided to the primary urologist . 
an example of such a trial is the ongoing genomics in michigan impacting observation or radiation ( g - minor ) trial in the postprostatectomy setting.31 however , in the absence of a similar trial in patients with newly diagnosed disease , prospective observational data can provide critical insights into how these tests are guiding clinical decisions . these limitations notwithstanding , strengths of this study include prospective data collection on nearly 4 , 000 consecutively enrolled patients with newly diagnosed prostate cancer . 
although other studies have sought to evaluate treatment decisions related to gec testing , none included concurrently diagnosed patients without testing , which is vital to understand the clinical utility of these tests.32 - 35 in conclusion , these data indicate that gec testing has clinical utility in the favorable - risk setting , and testing of patients with favorable - risk disease is more common in men with higher psa levels and higher - grade disease who may not typically be considered as candidates . 
gec testing also is being performed in patients with intermediate - risk and high - risk unfavorable disease , for whom the clinical implications are less apparent , and there is marked variability in how gec tests are being used . 
spratt no relationship to disclose speakers ' bureau : myriad genetics , genomic health , genomedx , mdxhealth , strand diagnostics research funding : myriad genetics ( inst ) , genomic health ( inst ) , genomedx ( inst ) , mdxhealth ( inst ) , neogenomics laboratories ( inst ) frank n . 
morgan consulting or advisory role : myriad genetics , terumobct research funding : myriad genetics ( inst ) , mdxhealth ( inst ) , genomedx ( inst ) affiliations jonathan c . 
morgan , university of michigan , ann arbor ; and kirk wojno , comprehensive urology , royal oak , mi . supported by blue cross blue shield of michigan ; the department of defense physician research training award no . 
bokhorst lp , valdagni r , rannikko a , et al : a decade of active surveillance in the prias study : an update and evaluation of the criteria used to recommend a switch to active treatment . 
newcomb lf , thompson im , jr , boyer hd , et al : outcomes of active surveillance for clinically localized prostate cancer in the prospective , multi - institutional canary pass cohort . 
tosoian jj , mamawala m , epstein ji , et al : intermediate and longer - term outcomes from a prospective active - surveillance program for favorable - risk prostate cancer . 
cuzick j , stone s , fisher g , et al : validation of an rna cell cycle progression score for predicting death from prostate cancer in a conservatively managed needle biopsy cohort . 
cuzick j , swanson gp , fisher g , et al : prognostic value of an rna expression signature derived from cell cycle proliferation genes in patients with prostate cancer : a retrospective study . 
van den eeden sk , lu r , zhang n , et al : a biopsy - based 17 - gene genomic prostate score as a predictor of metastases and prostate cancer death in surgically treated men with clinically localized disease . 
klein ea , cooperberg mr , magi - galluzzi c , et al : a 17 - gene assay to predict prostate cancer aggressiveness in the context of gleason grade heterogeneity , tumor multifocality , and biopsy undersampling . 
spratt de , zhang j , santiago - jimnez m , et al : development and validation of a novel integrated clinical - genomic risk group classification for localized prostate cancer . 
spratt de , yousefi k , deheshi s , et al : individual patient - level meta - analysis of the performance of the decipher genomic classifier in high - risk men after prostatectomy to predict development of metastatic disease . 
barcenas ch , sinha ak , raghavendra as , et al : outcomes after chemotherapy in early - stage breast cancer ( ebc ) patients who underwent a 21 - gene expression assay . 
reese ac , pierorazio pm , han m , et al : contemporary evaluation of the national comprehensive cancer network prostate cancer risk classification systeurology 80 : 10751079 , 2012 25 . 
cooperberg mr , pasta dj , elkin ep , et al : the university of california , san francisco , cancer of the prostate risk assessment score : a straightforward and reliable preoperative predictor of disease recurrence after radical prostatectomy . 
morgan tm , miller dc , dunn r , et al : prospective randomized trial of genomic classifier impact on treatment decisions in patients at high risk of recurrence following radical prostatectomy ( g - minor )  . 
dallera ma , maddala t , polychronopoulos l , et al : utility of the oncotype dx prostate cancer assay in clinical practice for treatment selection in men newly diagnosed with prostate cancer : a retrospective chart review analysis . 
eure g , germany r , given r , et al : use of a 17 - gene prognostic assay in contemporary urologic practice : results of an interim analysis in an observational cohort . 
rev urol 18 : 123 - 132 , 2016 appendix for number needed to test calculations , we assumed that the distribution of test results in untested patients would reflect the distribution of test results in tested patients . 
we first asked the following : of the 1 , 167 patients with favorable risk of cancer without a gene expression classifier ( gec ) test , how many patients with a gec test result below threshold would likely be reallocated to active surveillance ( as ) if they had undergone gec testing ? we calculated this as ( 203 / 320 ) 1 , 167 = 740 , which means that approximately 740 patients with low - risk gec exist of the 1 , 167 untested men . 
similarly , we assumed that , of the 667 untested patients with favorable risk of cancer who initially received as in this cohort , ( 203 / 320 ) 667 , or 429 of these men , are truly gec low risk . 
thus , use of a gec test should shift 562 429 , or 133 , patients with low - risk gec to as and result in a number needed to test of 1 , 167 / 133 , or 8.8 patients with favorable risk of cancer to shift one patient to as . conversely , of the 1 , 167 patients with favorable risk of cancer without a gec test , we asked how many patients with a gec test result above the threshold would likely be reallocated to definitive treatment if they had undergone gec testing . 
we assumed that ( 117 / 320 ) 1 , 167 , or 427 , would be gec high risk , using the same approach as for low risk , and that 427 39.3% , or 168 patients , would undergo primary therapy . 
summary of primary management in patients with favorable - risk disease according to the performance and result of prostate mri and gec testing test result total active surveillance definitive treatment no treatment no mri no gec test gec test < threshold gec test > threshold reassuring mri no gec test gec test < threshold gec test > threshold nonreassuring mri no gec test gec test < threshold gec test > threshold 564 ( 56.6 ) 144 ( 77 ) 46 ( 45.1 ) 77 ( 78.6 ) 9 ( 69.2 ) 5 ( 71.4 ) 34 ( 55.7 ) 0 ( 0 ) 3 ( 37.5 ) 299 ( 30 ) 27 ( 14.4 ) 41 ( 40.2 ) 14 ( 14.3 ) 2 ( 15.4 ) 2 ( 28.6 ) 17 ( 27.9 ) 2 ( 100 ) 3 ( 37.5 ) 134 ( 13.4 ) 16 ( 8.6 ) 15 ( 14.7 ) 7 ( 7.1 ) 2 ( 15.4 ) 0 ( 0 ) 10 ( 16.4 ) 0 ( 0 ) 2 ( 25 ) note . 
by law , we are the custodians of diagnostic tissues , and as such , we must comply with legal regulations covering the preservation and use of these tissues.1 as representatives of our hospitals and specialty , we want to be helpful collaborators in providing the diagnostic tissues necessary for the care of oncology patients . 
and as patient advocates , because of our legal role as custodians of these tissues , many of us harbor serious concerns about the current informed consent processes and standard practices for tissue handling during clinical trials and translational research . 
the vast majority of tissue - based assays used in the clinic ( including dna sequencing , rna and fusion protein identication by in situ hybridization , and immunohistochemistry to detect protein expression ) can be performed on formalinxed , parafn - embedded ( ffpe ) tissues . 
simultaneously , there is less diagnostic tissue available on each patient because of smaller biopsies acquired as part of lessinvasive sampling techniques , including small - caliber core biopsies or ne - needle aspiration ( fna ) cell blocks , earlier identication of small tumors , and successful neoadjuvant lead to marked tumor response . treatments that conservative estimates from our clinical practice suggest that up to 50% of tissue in diagnostic biopsies is used during routine standard - of - care testing , with more being used for challenging cases ( unpublished data )  . 
typical clinical scenarios from our practices illustrate the potential tensions between the availability of tissue after standard - of - care testing ( the supply ) and subsequent demands for tissues for research . 
their eligibility for these trials inevitably will lead to a request by the investigators for tissue submission ( usually 10 to 15 but sometimes 25 unstained slides or the entire parafn block ) , often as a condition of enrollment . 
pathologists are the caretakers of all tissues removed during clinical care , 1 and there are federal , state , and sometimes local laws governing how pathologists must treat those tissues . 
 mccall and dry of american pathologists ( cap ) require that pathologists store archival parafn tissues in a retrievable manner for a minimal time , which includes rules prohibiting exhaustion of the tissue during storage . 
these laws were intended to protect a patients ability to access the tissue for subsequent diagnostic testing , transfer of care , or medicolegal inquiries . as noted , many patients have only limited amounts of tissue available after standard - of - care testing . 
it is not uncommon for a pathologist to examine a block of tissue and realize that submitting the material desired by one clinical trial will completely exhaust the remaining biopsy sample . 
if they refuse to fulll the request , the patient will not qualify for the study , which will upset the patient and oncologist and will deny the patient a therapy with the potential to extend their survival and / or improve their quality of life . local trial enrollment , pathologists , when confronted with a request for limited biopsy tissue as a condition of stitutional review boards , and hospital legal counsel in the united states struggle with a catch - 22 situation : national institutes of healthsponsored clinical trials require submission of research tissue , whereas the centers for medicare and medicaid services ( another federal agency ) reimburse testing only in clia - certied laboratories ( that must adhere to tissue retention guidelines )  . 
clia requires that parafn blocks be retained for 2 years , and cap ( which has clia - deemed status and is the accrediting body for many us pathology laboratories ) requires that pathology laboratories retain parafn blocks for 10 years.4 , 5 state laws may have different retention requirements , and laboratories must comply with the most stringent applicable requirement . 
if a patient were appropriately informed , would that patient elect to provide two slides for biomarker research or trial eligibility and not provide 15 slides for downstream , unnamed correlative science ? as caretakers of the parafn archival tissues , pathologists take special care to avoid exhausting diagnostic biopsy samples in any retrospective translational research project . should correlative science performed as part of a clinical trial be different ? are clinical trial sponsors using ( for research or clinical purposes ) all the tissue they are collecting on enrolled patients ? and what about the submitted tissues from patients who are found to be ineligible for the study ? recent cancer clinical trials have reported accrual rates of 14% to 46%.7 , 8 patients are risking their existing tissues for an uncertain or even low chance of participation , without fully understanding the risks of tissue exhaustion or the trial needs for eligibility testing versus correlative science ( appendix )  . should the pathologist make executive decisions in these cases regarding the most judicious use of the remaining tissue ? as seasoned pathologists , we recall a time in which these individual patient scenarios would be discussed directly with oncologists ; however , the ever - increasing volume of patients , the remarkable number of available clinical trials , the practice of patients seeking second ( and third and fourth ) opinions far from home , and other pressures on general medical practice are making these conversations increasingly difcult to have . there are ethical and practical concerns here . 
patients may believe that the available clinical trial provides their only hope of benet from additional therapy . however , from prior experience , oncologists and pathologists know that the patient may not respond to the rst clinical trial agent and may want to enroll in a second clinical trial . 
 precision pathology in precision medicine mimicked metastatic disease or had developed a second cancer that had metastasized ( or that presents multifocally , such as multiple myeloma ) whereas the original cancer was controlled . 
without diagnostic conrmation of the tissues procured for research , these patients have a small but real risk of receiving the wrong treatment , which could shorten in misleading data and untheir life span and result necessary expense for the study sponsor . recommendations fortunately , we believe that there are multiple approaches available to address these concerns . 
working together , regulators , pathology departments , investigators , and clinical trial sponsors can improve how we prioritize limited tissue samples and how we inform patients of the risks and benets of using remnant clinical diagnostic samples for research . although we do not recommend major changes to clia or cap tissue retention regulations , we do feel a minor change is needed , namely explicit authorization to exhaust clinical diagnostic tissues if required for clinical trial enrollment ; we do not recommend similar authorization for unnamed correlative science as part of a clinical trial . 
we believe the minor modications we propose would continue to protect patients terests , while clarifying and permitting tissue exhaustion in exceptional circumstances . future diagnostic and medicolegal we also recommend changes to informed consent clinical trials . 
patients need to understand what materials are required for study enrollment , what materials are requested for possible future correlative science , benets and risks of providing materials for future correlative science , and their risks if their diagnostic tissues are exhausted in the process of getting tissues for study enrollment or future correlative science . 
such truly informed consent would fulll the intention of the common rule for protecting human research subjects9 and could make it easier for pathologists , institutional review boards , and legal counsel to approve exceptions to laws and regulations governing conservation of diagnostic tissues . for sponsors who receive more limited correlative science tissues , scientic review committees could prioritize the use of the material . 
other sources of cancer biologic materials , such as cell - free dna ( cfdna ) in peripheral blood could be considered , because cfdna may be most representative of the mutational prole of aggressive , metastatic tumor clones . 
in fact , the fda approved cfdna assays to direct treatment in egfr - mutated nonsmall - cell lung cancer.10 when possible , clinical trial sponsors should design studies so that research - only biopsies can be taken at the same time as routine clinical diagnostic biopsies . 
research - only biopsies performed under specic study consent do not fall under state , clia , or cap custodianship requirements , allowing entire parafn blocks to be submitted directly to the sponsor . finally , we urge sponsors to obtain diagnostic conrmation before enrolling patients into clinical trials . 
the incidence of such errors is unknown and is worthy of study . new approaches in pathology pathology departments also can make important changes . they can and should make it easier for clinical trial sponsors to obtain additional tissue sections to facilitate correlative science . 
this would encourage sponsors to reduce their upfront minimum acceptable requirements . this also could be accomplished by using consent language that gives the pathology department permission to send additional unstained slides or ( in case the patient dies ) a representative block or blocks for additional correlative science to the sponsor . 
sponsors could leverage virtual biobank technology to keep track of the samples potentially available to them for correlative science . pathology departments should review and update their protocols for processing small biopsy and cytology samples to maximize their potential downstream utility . 
one clear best practice emerging from recent studies is the separation of multiple biopsy cores into individual parafn blocks.11 - 14 this saves tissue for research and facilitates retention of representative diagnostic material per cap and clia regulations . 
although this prevents wasting tissue , it does require workows that may not be compatible with busy clinical histology laboratories and may be more suitable for research laboratories and biorepositories . 
 mccall and dry laboratories are reimbursed for interrupting clinical workows for high - priority assessments ( intraoperative consultations , cytologic adequacies ) , and research pathologists and laboratories should also be appropriately reimbursed for these activities . for downstream molecular during the biopsy procedure , cytopathologists or cytotechnologists can perform an immediate adequacy assessment in the procedural suite ( so - called rapid on - site evaluation [ rose ] )  . 
because feedback is immediate , rose increases the likelihood that research - only procedures will be successful in obtaining diagnostic tissue sufcient testing.15 during clinical and diagnostic biopsy procedures , rose is generally performed with simple designations such as diagnostic or nondiagnostic . 
in the era of precision pathology , varying degrees of diagnosis may be desired : enough for denitive diagnosis , enough for denitive diagnosis plus standard - of - care ancillary testing , or enough for denitive diagnosis plus standard - of - care ancillary testing and submission of tissue for clinical trial research . 
upfront planning and budgeting by sponsors of rose for research - only biopsies will ensure the availability of specialized cytotechnologists or cytopathologists and will increase the probability that the sponsor obtains sufcient malignant tissues for study . 
if the cytopathologist cannot be on site , telecytopathology has been successful and may decrease costs.16 , 17 in summary , pathologists want to support research and want to help their patients enroll in clinical trials . 
but we are concerned that current practices could result in morbidity for our patients in the form of additional biopsy procedures , may not meet with patient expectations of tissue availability after the clinical trial , and may explicitly violate federal regulations , state laws , and the standards of laboratory accrediting bodies . 
mccall other relationship : college of american pathologists no other potential conicts of interest were reported . references dry s , grody ww , papagni p : stuck between a scalpel and a rock , or molecular pathology and legal - ethical issues in use of tissues for clinical care and research : what must a pathologist know ? am j clin pathol 137 : 346 - 355 , 2012 sepulveda ar , hamilton sr , allegra cj , et al : molecular biomarkers for the evaluation of colorectal cancer : guideline from the american society for clinical pathology , college of american pathologists , association for molecular pathology , and the american society of clinical oncology . 
j clin oncol 35 : 1453 - 1486 , 2017 lindeman ni , cagle pt , aisner dl , et al : updated molecular testing guideline for the selection of lung cancer patients for treatment with targeted tyrosine kinase inhibitors : guideline from the college of american pathologists , the international association for the study of lung cancer , and the association for molecular pathology . 
amaria rn , prieto pa , tetzlaff mt , et al : neoadjuvant plus adjuvant dabrafenib and trametinib versus standard of care in patients with high - risk , surgically resectable melanoma : a single - centre , open - label , randomised , phase 2 trial . 
lozano md , echeveste ji , abengozar m , et al : cytology smears in the era of molecular biomarkers in non - small cell lung cancer : doing more with less . 
aisner dl , rumery md , merrick dt , et al : do more with less : tips and techniques for maximizing small biopsy and cytology specimens for molecular and ancillary testingthe university of colorado experience . 
harada s , agosto - arroyo e , levesque ja , et al : poor cell block adequacy rate for molecular testing improved with the addition of diff - quik - stained smears : need for better cell block processing . 
khurana kk , graber b , wang d , et al : telecytopathology for on - site adequacy evaluation decreases the nondiagnostic rate in endoscopic ultrasound - guided ne - needle aspiration of pancreatic lesions . 
identifying sufciently expanded short nucleotide repeat sequences in the tumor compared with non - neoplastic tissue is diagnostic for microsatellite instability ( whether it is the result of sporadic or inherited causes )  . however , if a clinical trial sponsor is already aware of a tumor mutation that has a hereditary cancer association , submitting non - neoplastic tissue to the sponsor could conrm a sporadic versus a hereditary origit should be noted that some commercial providers of highthroughput next - generation sequencing assays have elected to neither simultaneously test non - neoplastic germ line tissue nor provide interpretation of a possible inherited mutation within their reported results on the basis of increased mutant allele fraction . 
 window - of - opportunity study of valproic acid in breast cancer testing a gene expression biomarker purpose the anticancer activity of valproic acid ( vpa ) is attributed to the inhibition of histone deacetylase . 
we previously published the genomically derived sensitivity signature for vpa ( gdssvpa ) , a gene expression biomarker that predicts breast cancer sensitivity to vpa in vitro and in vivo . we conducted a window - of - opportunity study that examined the tolerability of vpa and the ability of the gdss - vpa to predict biologic changes in breast tumors after treatment with vpa . patients and methods eligible women had untreated breast cancer with breast tumors larger than 1.5 cafter a biopsy , women were given vpa for 7 to 12 days , increasing from 30 mg / kg / d orally divided into two doses per day to a maximum of 50 mg / kg / d . 
fifty percent of women ( three of six ) with triple - negative breast cancer had a ki - 67 reduction of at least 10% compared with 17% of other women . 
treatment individualization has been accomplished to a limited extent with the use of hormone receptor testing to determine a patients eligibility for antiestrogen therapy and human epidermal growth factor receptor 2 ( her2 ) testing to determine eligibility for anti - her2 therapies . however , with the ability to analyze tumors on the basis of their genomic profiles , further individualization may be possible for additional cancer therapies . inhibitors have histone deacetylase ( hdac ) shown promise in breast cancer in vitro , although this promise has not yet translated to clinical benefit . 
 effects , including increasing the expression of tumor suppression genes , 2 increasing the expression of cell cycle regulators , 3 increasing the expression of mediators of apoptosis , 4 - 7 decreasing proteasomemediated degradation of tumor suppressor genes , 8 decreasing oncoprotein levels via loss of hsp90mediated protection , 9 - 11 decreasing mitotic stability , 12 and decreasing angiogenesis.13 , 14 hdac inhibitors potentiate the apoptotic effect of anthracyclines on breast cancer cell lines.15 valproic acid ( vpa ) is an antiepileptic discovered in 1882 , which has been used clinically since 1962 . vpa inhibits class i and class iia hdacs.16 , 17 in vitro and in vivo studies show that vpa at clinically relevant concentrations inhibits the proliferation of breast cancer cell lines and xenografts.18 - 21 vpa has been used in breast cancer in combination with chemotherapy in three small trials22 - 24 in which response rates ranged from 33% to 70% , but the relative contribution of vpa and other drugs could not be determined . 
we previously published a gene expression signature that predicted the sensitivity of breast cancer to vpa in vitro and in vivo.21 we refer to this signature as the genomically derived sensitivity signature for vpa ( gdss - vpa )  . before committing to phase i and ii studies , it is important to establish the biologic effect of a drug and get preliminary data on potential biomarkers . in window - of - opportunity studies , women with newly diagnosed breast cancer receive a drug between the diagnostic breast biopsy and planned surgical resection or the start of neoadjuvant therapy . 
the primary objectives were to determine safety and tolerability of vpa , whether vpa levels correlate with histone acetylation in peripheral blood mononuclear cells ( pbmcs ) during treatment , and whether either vpa levels or histone acetylation in pbmcs predicts histone acetylation in tumor samples after treatment . 
key secondary objectives were to assess the sensitivity and specificity of the gdss - vpa to predict histologically measured antitumor activity of vpa in breast cancer , to assess the sensitivity and specificity of the gdss - vpa to predict antitumor activity of vpa in breast cancer as measured by dce - mri scanning , and to determine whether women have dose - limiting toxicities during or after treatment with vpa over 7 to 12 days . eligibility women with any stage of breast cancer who had received no prior treatment were potentially eligible for the trial . 
adult women were eligible if they had eastern cooperative oncology group performance status of 0 to 2 , a biopsy - proven invasive adenocarcinoma of the breast 1.5 cm or larger by clinical examination or imaging , were able to provide consent , and either were scheduled for breast surgery or were willing to have an endof - study biopsy . 
exclusion criteria included pregnancy ; need for immediate chemotherapy ; hypersensitivity to vpa or its components ; peanut allergy ( because some vpa formulations contain peanut oil ) ; inadequate bone marrow , kidney , or liver function ( greater than grade 1 by common terminology criteria for adverse events v3 ) ; were immunocompromised as a result of medications or hiv ; used other antiepileptics or medications that interact with vpa ; had inborn errors of metabolism ; had a history of pancreatitis ; were on a ketogenic diet ; were unable to have an mri scan ; or had a tumor that was unlikely to yield adequate tissue for genomic studies . conduct of the study women were enrolled between the biopsy that diagnosed their breast cancer and the start of therapy for the breast cancer , and all provided informed consent . 
estrogen receptor ( er ) , progesterone receptor ( pr ) , and her2 were assessed by using standard diagnostic methods.29 , 30 the percent of invasive cancer cells that expressed ki - 67 in samples before and after treatment with vpa was determined manually by a certified expert pathologist ( r.e.f. ) , who used an eyeball estimate . 
if no intolerable grade 2 or higher adverse effects ( aes ) were present , the dose was increased every 3 days by 10 mg / kg / d to a maximum of 50 mg / kg / d . 
dce - mri , dynamic contrast - enhanced magnetic resonance imaging ; pbmc , peripheral blood mononuclear cell ; vpa , valproic acid . screened ( n = 39 ) enrolled ( n = 31 ) completed vpa ( n = 29 ) screen failed no tumor on biopsy unable to isolate rna infection unwilling to do rebiopsy could not have mri withdrew consent ( n = 8 ) ( n = 1 ) ( n = 2 ) ( n = 1 ) ( n = 1 ) ( n = 2 ) ( n = 1 ) withdrawn change in diagnosis withdrew consent ( n = 2 ) ( n = 1 ) ( n = 1 ) missing some data post treatment mri : ( n = 4 ; 3 could not complete , and 1 technical problem ) pbmc histone acetylation : ( n = 4 ; insufficient pbmcs collected ) evaluable for ( n = 31 ) tolerability ( n = 29 ) ki - 67 pbmc histone acetylation ( n = 25 ) ( n = 25 ) dce - mri ( 7 days ) of vpa had been given or after 24 doses ( 12 days ) of vpa had been given . once the patient had received the highest tolerated dose of vpa treatment for at least four doses , a dce - mri scan was performed followed by either surgical excision of the tumor per standard of care or a repeat core biopsy . 
pbmcs were frozen , and histone acetylation was assessed by using western blot ( acetyl - h3 antibody #9649s and beta - actin antibody #3700s ; cell signaling technology , danvers , ma )  . the gdss - vpa was calculated by using rna from the pretreatment and post - treatment specimens as previously described.21 parameters for the gene expression signature were locked before the trial . 
cognitive effects were assessed by using the short portable mental status questionnaire ( spmsq ) .31 statistical analysis a sample size of 33 patients was planned to give a power of 80% to detect a correlation of 0.5 between the vpa level on the day of surgery and change in tumor or peripheral blood histone acetylation from day 0 to the day of surgery at a twosided a = .025. 
accuracy of predictions was determined by using area under the receiver operating characteristic ( roc ) curves calculated by using the proc r package.32 cis for roc curves were calculated by using the method of delong.33 thirty - three patients would result in a precision for estimating the specificity of the gdss - vpa of 6 14% if the specificity were 0.8 and 6 17% if the specificity were 0.6. 
 results patient characteristics between june 2010 and august 2014 , 39 patients were screened , 31 were enrolled , and 29 were treated with vpa ( fig 1 )  . 
all patients completed the study . safety and tolerability of the 31 women who started vpa treatment , 16 ( 51.6% ) completed the 50 mg / kg / d dose . 
characteristics of participants in vast characteristic median age , years ( range ) tumor size 54 ( 31 - 73 ) tumor grade er - positive / her2 - negative er - positive / her2 - positive er - negative / her2 - positive triple - negative study . 
all aes resolved quickly upon stopping vpa . pharmacodynamics most women ( 68% ) had increased pbmc histone 3 ( h3 ) acetylation after treatment with vpa ( fig 2a )  . 
there seemed to be a threshold effect at 100 mg / ml of vpa , because no women with vpa levels below this level had a doubling of pbmc h3 acetylation . 
however , change in histone acetylation was inconsistent ; three of eight women with serum vpa levels above 200 mg / ml had less than a doubling of h3 acetylation . 
h3 acetylation in tumors could not be assessed because of technical issues . we assessed the change in gene expression from before to after vpa treatment in breast tumors by using the gdss - vpa , which was designed by comparing gene expression patterns in breast cancer cells before and after in vitro treatment with vpa.21 the gene expression pattern in the posttreatment samples was significantly more like that seen in cells treated in vitro with vpa ( mean difference , 0.2063 on a scale of 0 to 1 , with 0 being the most like untreated cells and 1 being the most like vpa - treated cells ; p , .001 by paired t test )  . 
thirty - one percent of the women with er - positive / her2 - negative breast cancer had a decrease in ki - 67 of at least 10% , and 50% of women with triple - negative breast cancer ( tnbc ) had a decrease in ki - 67 of 10% or greater with vpa treatment . 
there was no detectable difference in age , grade , tumor size , baseline ki - 67 , final vpa level , or tumor subtype between the four responding women and the rest of the group , with the exception of the lack of her2 - positve tumors among the responders . 
in particular , of the four women with tumors whose ki - 67 decreased by 20% or more , two tumors were er - positive / pr - positive and two were triplenegative , two were grade 3 and two were grade 2 . in addition to using gdss - vpa as an indicator of exposure to vpa , we tested its ability as a biomarker on the pretreatment tumor rna to predict sensitivity to vpa . 
with the optimal cutoff chosen post hoc on the basis of the roc curves , the gdss - vpa had a sensitivity of 75% and a specificity of 64% for predicting a decrease in ki - 67 of at least 20% . 
 ( a ) scatter plot comparing serum valproic acid ( vpa ) level on the last day of treatment and the change in peripheral blood mononuclear cell histone 3 acetylation . 
the change in histone 3 acetylation is calculated as the ratio of the normalized expression of acetylated histone 3 by western blot on the final day of treatment to that before treatment . 
one tumor , which had a decrease from 60% to 40% in ki - 67 , was grade 3 on the pretreatment biopsy and grade 2 on the posttreatment lumpectomy , and one tumor was grade 2 on the pretreatment biopsy and grade 3 on the post - treatment lumpectomy . 
window - ofopportunity studies in breast cancer have been completed in the united kingdom , sweden , and canada.25 , 26 , 37 - 41 in the united states , windowof - opportunity studies have been conducted but have been more challenging.42 - 46 despite the lack of evidence of harm from short delays in definitive therapy , women in the united states are often reluctant to wait more than 2 weeks between seeing a surgeon and having surgery.41 the vast trial enrolled 94% of the goal population over 4 years . 
without treatment , the absolute change in ki - 67 between biopsy and surgery averages 2% to 4%.47 by contrast , large changes in ki - 67 were seen in some women in our trial , particularly women with tnbc . 
this contrasts with in vitro and in silico data from our group and from others.21 , 48 the reason for this lack of sensitivity may be related to the differences in expression of the various hdacs among breast cancer subtypes.49 , 50 our results complement another recent windowof - opportunity study of hdac inhibitors in breast cancer . 
other ongoing studies are combining hdac inhibitors with chemotherapy ( nct02632071 , nct02393794 ) , endocrine therapy ( nct02820961 , nct02115282 , nct02395627 ) , or immunotherapy ( nct02708680 , nct02453620 , nct02395627 )  . 
 ( a ) hematoxylin and eosin stain from biopsies before ( left ) and after ( right ) treatment with valproic acid ( vpa ) showing fibrosis typical of a post - treatment effect . 
like any biomarker , gdss - vpa was not perfect . discrepant response to drug and biomarker prediction could be the result of tumor heterogeneity , subtherapeutic vpa levels , deficiencies in the signature , or insufficient time of treatment ; our sample size was too small for a multivariable analysis . vpa faces significant challenges as an anti breast cancer agent . 
although by traditional measures it is well tolerated with no grade 4 toxicities , many of the grade 2 toxicities , including dizziness , sleepiness , and cognitive slowing , are intolerable over long periods of time and are difficult to ameliorate with standard supportive care . 
 ( a ) scatter plot comparing genomically derived sensitivity signature for valproic acid ( gdss - vpa ) prediction to the change in ki - 67 from the pretreatment tumor to the post - treatment tumor . the prediction ranges from 0 ( predicted most resistant ) to 1 ( predicted most sensitive )  . 
 ( b ) receiver operating characteristic curve for the gdss - vpa predictor for predicting a decrease in ki - 67 of 20% . finally , the nonlinear relationship between vpa serum levels and pbmc histone acetylation changes suggests pharmacogenetic effects that may make vpa ineffective in some people . therefore , other hdac inhibitors may be more appropriate for future studies . weaknesses of our study include the small sample size and the inability to assess histone acetylation changes in tumors . 
conclusions about the relationship between tumor subtype and sensitivity to vpa are hypothesis generating only . finally , the short time period of treatment may not have been long enough to see the full effect of treatment . we were able to complete a window - ofopportunity trial of vpa in breast cancer and to test a gene expression biomarker of sensitivity to vpa . 
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kim hr , kim ej , yang sh , et al : trichostatin a induces apoptosis in lung cancer cells via simultaneous activation of the death receptor - mediated and mitochondrial pathway ? exp mol med 38 : 616 - 624 , 2006 6 . 
zhang xd , gillespie sk , borrow jm , et al : the histone deacetylase inhibitor suberic bishydroxamate regulates the expression of multiple apoptotic mediators and induces mitochondria - dependent apoptosis of melanoma cells . 
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zhou q , agoston at , atadja p , et al : inhibition of histone deacetylases promotes ubiquitin - dependent proteasomal degradation of dna methyltransferase 1 in human breast cancer cells . 
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bali p , pranpat m , bradner j , et al : inhibition of histone deacetylase 6 acetylates and disrupts the chaperone function of heat shock protein 90 : a novel basis for antileukemia activity of histone deacetylase inhibitors . 
phiel cj , zhang f , huang ey , et al : histone deacetylase is a direct target of valproic acid , a potent anticonvulsant , mood stabilizer , and teratogen . 
hodges - gallagher l , valentine cd , bader se , et al : inhibition of histone deacetylase enhances the anti - proliferative action of antiestrogens on breast cancer cells and blocks tamoxifen - induced proliferation of uterine cells . 
candelaria m , gallardo - rinc on d , arce c , et al : a phase ii study of epigenetic therapy with hydralazine and magnesium valproate to overcome chemotherapy resistance in refractory solid tumors . 
arce c , perez - plasencia c , gonzalez - fierro a , et al : a proof - of - principle study of epigenetic therapy added to neoadjuvant doxorubicin cyclophosphamide for locally advanced breast cancer . 
m unster p , marchion d , bicaku e , et al : phase i trial of histone deacetylase inhibition by valproic acid followed by the topoisomerase ii inhibitor epirubicin in advanced solid tumors : a clinical and translational study . 
hadad sm , coates p , jordan lb , et al : evidence for biological effects of metformin in operable breast cancer : biomarker analysis in a pre - operative window of opportunity randomized trial . 
klintman m , dowsett m : early surrogate markers of treatment activity : where are we now ? j natl cancer inst monogr 2015 ( 51 ) : 24 - 28 , 2015 28 . 
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wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
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mehta s , hughes np , buffa fm , et al : assessing early therapeutic response to bevacizumab in primary breast cancer using magnetic resonance imaging and gene expression profiles . 
singletary se , atkinson en , hoque a , et al : phase ii clinical trial of n ( 4 - hydroxyphenyl ) retinamide and tamoxifen administration before definitive surgery for breast neoplasia . 
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curigliano g , g omez pardo p , meric - bernstam f , et al : ribociclib plus letrozole in early breast cancer : a presurgical , window - of - opportunity study . 
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gandini s , guerrieri - gonzaga a , pruneri g , et al : association of molecular subtypes with ki - 67 changes in untreated breast cancer patients undergoing pre - surgical trials . 
mawatari t , ninomiya i , inokuchi m , et al : valproic acid inhibits proliferation of her2 - expressing breast cancer cells by inducing cell cycle arrest and apoptosis through hsp70 acetylation . 
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m uller bm , jana l , kasajima a , et al : differential expression of histone deacetylases hdac1 , 2 and 3 in human breast cancer : overexpression of hdac2 and hdac3 is associated with clinicopathological indicators of disease progression . 
 decision - making preferences about secondary germline findings that arise from tumor genomic profiling among patients with advanced cancers purpose in patients with advanced cancers , tumor genomic profiling ( tgp ) can reveal secondary germline findings ( sgfs ) with regard to inherited disease risks . 
this study examined the process by which patients with advanced cancers would decide about whether to learn these sgfs and their preferences about specific challenging decision scenarios , including whether patients should be required to receive sgfs and whether sgfs should be returned to the family after a patients death . patients and methods we conducted qualitative semistructured interviews with 40 patients with advanced breast , bladder , colorectal , or lung cancer who had undergone tgp . 
data were collected on participants perspectives about the hypothetical decision to learn their sgfs , including their anticipated approach to the decision - making process , and their preferences about challenging decision scenarios . 
data were evaluated by thematic content analysis . results we identified themes with regard to participants preferred degree of decisional autonomy , perceived vital role of doctors , information needs , and anticipated process of deliberation . 
most participants stated that patients should be able to make a choice about receiving actionable sgfs , and a majority stated that sgfs should be available to family after a patients death . conclusion these results provide insight into sgf decision - making processes of patients with advanced cancers , which can allow clinicians to provide patients with optimal decision support in this context . 
these germline variants are considered secondary findings when actively sought by researchers or clinicians ( or incidental findings when not ) because they arise outside the original purpose of tgp.1 , 2 secondary germline findings ( sgfs ) that indicate risks for various health conditions are likely to be detected in a sizable minority of patients who receive tgp ; for example , presumed pathogenic germline variants have been observed jada g . 
this decision is likely to be challenging , particularly for patients with advanced cancers who are currently the primary users of tgp ( because of its utility for identifying eligibility for clinical trials of novel therapeutics5 , 6 )  . 
these individuals must choose whether to learn information about their future disease risks and potential shared familial risks while facing a poor prognosis and the psychosocial challenges of a terminal diagnosis.7 although patients with varying stages of cancer have reported interest in receiving such information from tgp in real8 and hypothetical9 - 11 settings , how patients decide whether to learn sgfs is unclear . 
understanding the decision - making processes of patients with advanced cancers would allow clinicians to anticipate patient informational and decision support needs in this context . the current study describes processes by which patients with advanced cancers decide whether to learn sgfs that arise from tgp . 
we analyzed qualitative data collected through an investigation of attitudes about sgfs among patients who received tgp at our institution.12 these patients were informed about the possible incidental discovery of germline variants during tgp consent conducted by their primary medical oncologists ; however , because our institution did not routinely conduct secondary analyses at the time of this study , none of the patients had made a definitive decision about learning their sgfs . 
 we also assessed preferences with regard to specific challenging decision scenarios , including whether patients should be required to receive sgfs and whether sgfs should be returned to the family after a patients death . study methods are described in detail elsewhere.12 in brief , we recruited 40 adults with advanced breast , bladder , colorectal , or lung cancer who had undergone tgp with an institutional somatic sequencing panel ( msk - impact [ memorial sloan kettering - integrated mutation profiling of actionable targets ] 13 , 14 )  . 
 the memorial sloan kettering cancer center institutional review board approved this study . individual semistructured interviews15 - 18 were conducted with participants in person or by telephone on the basis of participant preference . 
we categorized participant responses into four key themes and relevant subthemes ( indicated by italicized text ) ; illustrative quotes appear in table 2 . theme 1 : degree of decisional autonomy as participants considered how they would decide whether to learn sgfs , a spectrum emerged with regard to participants preferred degree of decisional control and autonomy from close others . 
influential factors for this perspective included a view that the decision was my choice because it involved highly personal information fundamentally related to my body and a desire to avoid burdening others , particularly family , with potentially distressing information . a second group of participants preferred that close others play a consultative role in the decision making process . 
these participants anticipated communicating with close others about the option to learn sgfs and would consider their advice and opinions but would ultimately make the final decision on their own . 
some in this group noted that their familys views were highly valued but would not be determinants in their decision making . finally , a smaller group preferred that close others serve as active partners in decision making . 
others explained that their family members should be actively involved in this decision because sgfs may have direct health - related implications for them . participants who anticipated the involvement of others in their decision making also described their process of selecting close others for communication about the option of learning sgfs . 
decision - making process and preferences regarding secondary germline findings and illustrative participant quotes participant quote theme theme 1 : degree of decisional autonomy patient as an autonomous decision maker well , i think that would be up to me to decide , so i wouldnt be asking my family what they think about doing that . 
 ( f / cc ) close others play a well , id like their input , but ultimately , i make the decisions for what...kind of consultative role in the decision - making process treatment....i would make the final decision . 
 ( f / brc ) close others serve as active partners in decision making process of selecting close others for communication i would expect my wife to be involved....i trust her knowledge and judgment in these matters . 
i dont think my husband could deal with it , so i dont want him burdened with it , and i dont think my step - kids have enough...skin in the game , so to speak , that they should actually be involved in making the decision and i guess i feel similarly about sisters and brother that thats too distant . 
 ( f / cc ) theme 2 : vital role of doctors nature and quality of the doctor - patient relationship primary source of relevant and valuable information theme 3 : information needs clinical benefit meaning tainty testing procedure believe me , its been a rough road , and so like i said , my oncologist and i , we have a good understanding . 
he was the one that put me in the tumor profiling and also on this new research , and anything he decides with me , im okay with it because we have that doctor - patient trust . 
i mean , you know , if they tell me to go get this test , i go get that test....i do it because i think its in the interest of my health.you know , you would have to make a strong argument for that case , but if he was insistent , i would do it . 
 ( m / blc ) i think from a personal standpoint i would ask...how realistic do you think , or how probable do you think , something that came up as high risk is likely to happen , or is there anything i can do to prevent it ? i mean , its more so in the latter that i would care about more if theres anything i can do to prevent it , to minimize the risk . 
is it certain mutations , is it only certain diseases that were talking about , or...is it kind of open ended ? ...i guess i would want to learn more and hear more about the science of what the mutations might mean . 
 ( m / cc ) degree of scientific uncerwhat im trying to have connection with is that if this testing were predictive of something , they would be more interested than if [ with ] this testing , nobody understood or knew how to interpret the results . 
so i guess it would be depending [ on ] how far along the continuum we are in being able to use this information [ that ] would make a difference . 
 ( m / lc ) yes , and if its nothing invasive and they wont...poke me anymore and they wont do anything to me , its fine with me....i would like to know . 
decision - making process and preferences regarding secondary germline findings and illustrative participant quotes ( continued ) theme participant quote who will have access who would have that information , would health care providers...have to have access to that or insurance providers have to have access to that information ? ( f / brc ) yes , what are the possible ramifications , like everything ? like the question that i have now , like what havent i thought of that could be a possible ramification of knowing ? yeah . 
 ( f / brc ) negative implications or harms theme 4 : process of deliberation ing process deliberative decision - makthe only potential benefit i see is if it discovers something that could be dealt with and prevent serious illness or genetic problems in the future . 
 ( m / cc ) take time to decide i think i would want to think about it and talk about it a little more before i made that quick decision , yeah . 
but i dont think its something that we would shy away fro ( m / lc ) well , i think i would research mutations first and find out a little about it before i answered him , but my nature is to go ahead and find out as much information as i can . 
 ( f / blc ) no need to engage in i would say , great , where do i sign ? when i first got diagnosed , i offered to extensive deliberation have my dna sequenced , and the doctor said , why would you bother ? theres only 30 markers , and weve already looked at theso yeah , to me , it was like a no - brainer and required no thought . 
so for me , its really once i understand what exactly ill be getting out of the study or what benefit it can provide , thats enough of what i need to make a decision on . 
i wouldnt want to procrastinate...it would be my decision....id discuss with family members...my husband and my sister , but...it would be my decision ultimately , and id really want to make it quickly . 
the interviewer described secondary germline findings as follows : i mentioned that with tumor genomic profiling , sometimes the lab will also look for mutations in the genes in your normal cells . 
 abbreviations : blc , bladder cancer ; brc , breast cancer ; cc , colorectal cancer ; f , female ; lc , lung cancer ; m , male . theme 2 : vital role of doctors participants perceived their doctors ( ie , oncologists ) as a vital influence on their decision making . 
for example , several participants reported great trust in their doctors on the basis of a foundation of past experiences and certainty that their doctors will act in their best interests . 
several participants anticipated that their doctors would possess expertise with regard to a range of issues relevant to sgfs and thus could help them to acquire all essential information . theme 3 : information needs participants described a typology of information that they would require to make an educated decision about learning sgfs , including an explanation of whether sgfs would provide a clinical benefit to the patient , his or her family , or other cancer patients and whether these benefits would outweigh possible harms ; assistance in interpreting the meaning of sgfs , such as the degree of certainty of the results and meaning of specific mutations ; degree of scientific uncertainty of sgfs and confidence in their applicability to health decisions ; description of the testing procedure in terms of the invasiveness of sample acquisition ; information about who will have access to the findings ( eg , insurers , health care providers ) ; and negative implications or harms of learning sgfs for the patient and family , including unanticipated consequences . 
many participants stated that they would ask questions about these issues to feel adequately informed , yet a minority doubted that they would have any specific questions if presented with this decision primarily because of placing a high innate value on sgfs . theme 4 : process of deliberation two preferences emerged among participants with regard to the necessity to engage in an extensive decision - making process . 
 ( a detailed description of these perceived benefits and harms is provided elsewhere.12 ) participants described procedural aspects of their deliberation and expressed a preference to take time to decide , during which they would consider the option on their own and seek out information about the value of sgfs . 
furthermore , a few participants expressed a preference to conduct independent research to learn more about receiving sgfs and the meaning of potential mutations . a minority of the sample articulated no need to engage in an extensive deliberation to determine their interest in sgfs . 
 finally , some described a sense of urgency about learning sgfs and stated the necessity to gain and act upon this information quickly to benefit their current health directly . preferences with regard to decision scenarios during the interview , participants were presented with challenging scenarios and asked to describe their preferences for how clinicians should handle these situations . 
first , in response to the debate about the disclosure of sgfs , 26 - 29 we asked participants whether findings about diseases that have effective medical interventions or medication adverse effects ( ie , actionable sgfs ) should always be returned to patients . 
most participants ( 28 [ 70% ] of 40 ) stated that patients should be able to choose whether to receive this information , whereas a minority ( 12 [ 30% ] of 40 ) stated that such information should always be disclosed to patients . participants also were asked to decide whether they believed that if actionable sgfs were detected after a patients death , then these findings should be made available to a patients family or significant other . 
a subset of participants ( 16 [ 69.5% ] of 23 ) also expressed a belief that patients should be required to provide consent for this disclosure before their death , such as at the time of agreeing to tgp , whereas fewer ( seven [ 30.5% ] of 23 ) deemed patient consent unnecessary . 
preferences with regard to specific decision scenarios that involve secondary germline findings and illustrative participant quotes participant quote question should actionable secondary germline findings * always be returned to patients ? yes ( 30% ) yes , i agree with that because they may not want to know , but theyre still going to be affected by it . 
because at least theyd have the opportunity to know...whats going on with thethey may not want to know , and it may be painful , but i think that they should be told . 
i think of a very close friend that was diagnosed with cancer , and he was in his 20s , and he survived , but when i learned that i had cancer , i reached out to him , and he said that at his lowest point he begged , i dont want to know any more information . 
and that was part of the healing for him , so i always think about that because that was a poignant point that he made , and i think its so personal . 
 ( f / brc ) should actionable secondary germline findings be made available to a patients family or significant other if a patient has died ? yes ( 90% ) unsure ( 5% ) no ( 5% ) should nonactionable secondary germline findings be made available to a patients family or significant other if a patient has died ? yes . 
well , if it in any way could...impact the timing of treatment or care for someone else in the family , they should....i would want them to know about it....i guess at the end of the day that you should get consent from the patient...as to what youre going to do with anything...you take from the ( m / lc ) you got a coin ; you wanna flip a coin ? because the problem that comes to me is that my family is very tight , and it wouldnt be a problem with my family , but you always have a family that [ is ] ...on the outs , so to speak , and if you tell one , you got to tell all . 
 ( m / lc ) thats a good question because im thinking that if the spouse , for example , were told after the person passed away that we had discovered this , i guess the first reaction would be , how come we didnt discover it earlier while the person was still alive and there may have been time for some kind of treatment ? so it might cause some kind of anger . 
preferences with regard to specific decision scenarios that involve secondary germline findings and illustrative participant quotes ( continued ) question unsure ( 2.5% ) no ( 15% ) participant quote i can project how i might think in the future , but its hard for me to say at this time in a practical way how i would feel about , you know , releasing . 
if they want the information they should go and get it...and i think that if they get it just because it was available for me , like as part of my estate , heres her genetic testing , and again , ill use my brother because he has the kids . 
if...he sees in black and white that theres an indicator that we have a genei have a gene so that becomes a family gene - - so hes now gotten a worry he didnt ask for in his life . 
 abbreviations : blc , bladder cancer ; brc , breast cancer ; cc , colorectal cancer ; f , female ; lc , lung cancer ; m , male . * in the interview , actionable secondary germline findings were described as follows : there are different ways to think about the many kinds of mutations or disease risks that you could theoretically learn about . 
when doctors know that someone has one of these mutations , they can recommend ways to help prevent a disease from developing or help find it earlier when it is more likely to be treatable . 
the doctors may also change the kinds of medications that they prescribe . in the interview , nonactionable secondary germline findings were described as follows : it is also possible that the lab will find mutations for conditions that do not have recommended or effective medical interventions . 
 but when two carriers of the same recessive mutation have a child , then the child could have the disease . unsure about whether actionable sgfs should be available to a patients family after death ( two [ 5% ] of 40 ) or stated that such information should not be made available ( two [ 5% ] of 40 )  . 
 preferences against disclosure were due to concerns about negative emotional implications of such information for families . participants were similarly asked to decide whether they believed that sgfs about diseases without effective medical interventions or that indicate one is a healthy carrier for recessive diseases ( ie , nonactionable sgfs ) should be made available to a patients family after a patients death . 
most participants who provided an opinion regarding consent reported that patients should be required to consent to the disclosure of this information to their families ( 11 [ 92% ] of 12 )  . 
fewer ( six [ 15% ] of 40 ) stated that nonactionable sgfs should not be made available to family after a patients death because of concerns about negative emotional reactions and the limited ability to intervene with such diseases . 
 finally , when comparing the preferences of participants with regard to the return of actionable versus nonactionable sgfs to family after a patients death , 22.5% ( nine of 40 ) were discordant in their preferences across these scenarios . discussion this study clarifies the decision - making processes of patients with advanced cancer with regard to sgfs from tgp . 
however , consistent with other medical decision contexts , 30 - 34 variability existed in participants preferences for involving others , including spouses / partners , children , and siblings , in their decision making . 
consequently , when presenting the option of learning sgfs , clinicians must allow patients to solicit input from close others and help to navigate challenges inherent in decision making with multiple individuals.35 additional research should investigate how such interpersonal influences shape , hinder , or support patients sgfs decision making . participants anticipated that their doctors ( ie , oncologists ) would be the primary source of guidance for this decision . 
participants also anticipated that they would have extensive questions about the benefits , harms , interpretation , and process of obtaining sgfs and would expect their oncologists to provide answers . 
however , research has demonstrated that this may not be feasible because many oncologists have limited experience with germline testing and express concerns about their ability to address challenges presented by sgfs.8 several approaches may help to bridge this gap between patient expectations and oncologist preparedness , including oncologist - targeted communication training , novel patient education materials , and referral to genetic counselors to address patient questions . 
future research should evaluate which of these approaches are most effective at achieving the delicate balance between meeting patients information needs and practical challenges of cancer care delivery ( eg , time demands , workforce limitations )  . 
research should also examine how various models of patient education ( eg , oncologist led , genetics professional led ) influence patient sgfs decisions and how patients weigh the opinions of various care providers in this context . many participants anticipated a preference to undergo a thoughtful deliberation about the prospect of learning sgfs . 
research suggests that the adoption of a more intuitive decision - making approach can yield similar outcomes to deliberative decision making , 36 although both approaches have benefits and drawbacks.37 of note , some participants preferences for a quick decision were motivated by beliefs that sgfs would provide clinical utility or necessitate urgent action for them to reap health benefits . 
accordingly , clinicians must ensure that all patients , including those immediately enthusiastic or accepting of sgfs , accurately understand the limitations of this risk information . these results also provide insight into preferences of patients with advanced cancers with regard to challenging scenarios that involve the return of sgfs . 
consistent with american college of medical genetics and genomics recommendations4 and expert opinion , 38 most participants stated that patients should choose whether they want to receive actionable sgfs from tgp . 
participants generally were more supportive of the return of actionable sgfs to family after a patients death than nonactionable sgfs ; although , in both instances , a majority supported the sharing of this information with family largely because of perceived family health benefits . 
the qualitative design enabled an in - depth analysis of the decision - making preferences of a sample of patients with advanced cancers diverse in diagnosis , sex , and health status . 
however , the majority was well - educated ( 85% reporting at least some college ) ; decision - making preferences and processes of these individuals may differ from those with less formal education . 
additional limitations are that this sample was racially and ethnically homogenous , recruited from one institution , and assessed at a time when the decision about learning sgfs was hypothetical in nature ; thus , the findings may not be generalizable to the broader population of patients with advanced cancers treated in other care settings who are navigating this decision in real time . 
recommendations for developing precision oncology programs with regard to how to manage and support patient decision making about secondary germline findings from tumor genomic profiling develop educational materials about tumor genomic profiling ( tgp ) and secondary germline findings ( sgfs ) that can be easily disseminated to and understood by close others ( eg , siblings , children , spouses / partners ) who may play a role in a patients decision making . ensure that individuals who lead education and consent discussions about the return of sgfs are prepared to help patients with varying preferences for decisional autonomy from their close others . patients attribute high trust and expertise to their oncologists ; therefore , prepare oncologists to serve as a primary resource who can provide balanced advice to patients about sgf decisions . create patient educational materials that provide clear information about the potential benefits and harms of sgfs . 
 distinguish between potential outcomes of sgfs for patients ( with a consideration of their cancer stage and prognosis ) and their families . ensure that patients understand that the decision to undergo tgp is separate from the decision about return of sgfs and that varying potential benefits and harms of each choice exist . structure education and consent discussions about tgp and the return of sgfs to be temporally flexible and , therefore , capable of accommodating patients preferences to take time to deliberate , seek additional input from close others , and conduct independent research . give patients a choice about the return of actionable sgfs . 
either opt - in or opt - out models of germline variant management could allow such patient choice , but each has unique implications for resources to support informed patient decision making and subsequent uptake of sgfs . require patients to make decisions about the management of actionable and nonactionable sgfs in the event of their death at the time of consenting to tgp and the return of sgfs . in conclusion , this study provides important insight into how patients with advanced cancers approach the decision to learn sgfs and informs how developing precision oncology programs can manage the reporting of germline variants from tgp ( table 4 )  . 
patient preferences for involvement in this decision can be accommodated in both opt - in and opt - out models , although these models likely will differ in the resources necessary to support patient deliberation and in the number of patients who select to receive sgfs.42 , 43 although most patients likely will want to retain decisional control in this context , some will desire time and space to include family and other influential figures in their decision making . 
whereas the tgp decision may be time sensitive because of treatment implications , patients may benefit from efforts to ensure that the decision to receive sgfs can be pursued on a different temporal schedule that aligns with their preferences for information seeking and deliberation . 
thus , educational and communication interventions targeted to patients , their families , and oncologists are needed to provide clear information that contextualizes the meaning of sgfs in the advanced cancer setting , assist the weighing of benefits and harms , and allow patients to explore and express their preferences about specific categories of sgfs and management of this information in the event of their death . 
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kaphingst ka , ivanovich j , biesecker bb , et al : preferences for return of incidental findings from genome sequencing among women diagnosed with breast cancer at a young age . 
 o predicting expected absolute chemotherapy treatment benet in women with early - stage breast cancer using endopredict , an integrated 12 - gene clinicomolecular assay hatem soliman , md1 ; darl d . 
flake ii , phd2 ; anthony magliocco , md1 ; mark robson , md3 ; lee schwartzberg , md4 ; priyanka sharma , md5 ; krystal brown , phd2 ; saskia wehnelt2 ; ralf kronenwett , md , phd6 ; alexander gutin , phd2 ; johnathan lancaster , md , phd2 ; jack cuzick , phd7 ; and william gradishar , md8 purpose previous studies have shown endopredict ( epclin ) , a test that integrates 12 - gene expression data with nodal status and tumor size , to be predictive for risk of distant recurrence in women with estrogen receptorpositive , human epidermal growth factor receptor 2negative early - stage breast cancer . 
here , we modeled expected absolute chemotherapy benet on the basis of epclin test results . methods the effect of chemotherapy was modeled using previously validated 10 - year risk of distant recurrence as a function of epclin score for patients treated without chemotherapy . 
the early breast cancer trialists collaborative group performed a meta - analysis of more than 100 clinical trials in more than 100 , 000 women to evaluate the benet of adjuvant chemotherapy.6 although the in individual benet trials varied considerably , 3 this meta - analysis demonstrated an average 30% relative reduction in distant recurrence among women who received chemotherapy compared with those who did not.6 for many patients with er - positive disease , the risk of distant recurrence is sufciently low that et alone is adequate . 
in these patients , the adverse effects associated with chemotherapy may outweigh any benet provided by a reduced risk of disease recurrence . historically , identication of these low - risk patients has relied on clinicopathologic parameters , such as nodal status , tumor size , and tumor grade . 
 soliman et al context key objective can an integrated , 12 - gene , clinicomolecular assay predict absolute benet from chemotherapy for women with estrogen receptor ( er ) positive , human epidermal growth factor receptor 2 ( her2 ) negative breast cancer ? knowledge generated in this model , patients with low 12 - gene scores showed no difference in recurrence - free survival with or without chemotherapy , whereas those with high 12 - gene scores showed a marked increase in recurrence - free survival with the addition of chemotherapy . 
overall , this study suggests that the 12 - gene clinicomolecular score is able to predict absolute benet of chemotherapy for women with er - positive , her2 - negative breast cancer . relevance accurate risk assessment is critical for determining appropriate treatment of women with breast cancer . 
breast cancer prognostic assays like the 12 - gene clinicomolecular score have been shown to provide more information about risk than standard clinical information alone in predicting recurrence - free survival in the absence of treatment . 
these new data support the ability of the 12 - gene clinicomolecular score to also predict absolute benet from chemotherapy to help to guide chemotherapy decisions for women with er - positive , her2 - negative breast cancer . are inadequate to guide adjuvant chemotherapy decisions reliably.7 thus , when risk is dened using clinicopathologic features alone , a subset of truly low - risk patients receives unnecessary chemotherapy , whereas others at high risk forgo chemotherapy and experience avoidable disease recurrence . to address this clinical dilemma , multigene expression prognostic assays have been developed for patients with er - positive , human epidermal growth factor receptor 2 ( her2 ) negative early - stage breast cancer . 
several such assays are clinically available , with variable performance according to nodal status , and early ( 0 to 5 years ) versus late ( 5 or more years ) recurrence.8 - 11 these assays better quantify residual risk of recurrence after surgery and et than clinicopathologic features alone , which enables physicians to tailor the use of adjuvant therapies ( et alone v et + c ) more accurately . 
to this end , evidence - based practice guidelines now indicate that prognostic assays are appropriate tools to help guide decision making.12 - 14 one such test is endopredict ( myriad genetics , salt lake city , ut ) , which integrates a 12 - gene molecular score with nodal status and tumor size into a combined clinicomolecular score ( epclin )  . 
previous studies have validated that epclin accurately predicts the risk of distant metastases in patients with er - positive , her2 - negative breast cancers.11 , 15 - 18 although this information can reliably identify patients at sufciently low risk so that chemotherapy may be avoided safely , the ability of epclin to predict benet from the addition of chemotherapy has yet to be fully dened . 
ideal approaches to evaluate this are limited because archival samples from previous randomized trials of et 6 c in appropriate patients largely have been exhausted.3 , 5 a prospective trial of epclin that includes an arm randomized to receive no chemotherapy would now be unethical , given the established benet of chemotherapy for patients with high - risk disease . 
alternative study designs , therefore , are required to explore the scope of epclins ability to predict adjuvant chemotherapy benet for patients with er - positive , her2 - negative earlystage breast cancer . so far , classic factors that inuence breast cancer prognosis have not shown an interaction between the relative effect of adjuvant chemotherapy on absolute risk of recurrence.19 furthermore , the absolute benet of chemotherapy depends on the patients baseline risk of developing recurrent disease.19 as such , as we evaluate a biomarker , it is helpful to understand the principal drivers of its chemopredictive ability . 
one possibility is that chemopredictive ability is driven by high prognostic accuracy , that is , the ability of the biomarker to differentiate those patients at highest versus lowest absolute risk of recurrence and , thus , those latter patients for whom chemotherapy cannot yield any clinically meaningful benet . 
alternatively , it is possible that a biomarkers chemopredictive ability is driven by differences in relative chemotherapy benet between higher versus lower biomarker - dened patient groups ( ie , interaction between the biomarker score and relative chemotherapy benet )  . in the current study , we describe a modeling study that uses epclin score , absolute risk of recurrence , and reduction of this risk associated with the addition of chemotherapy to estimate the differences in absolute risk for distant recurrence across epclin scores . 
we demonstrate that for a molecular marker such as epclin , patients with the highest baseline absolute risk for recurrence experience the greatest absolute benet from chemotherapy . furthermore , we establish that the key factor in any biomarkers chemopredictive capacity is the ability to predict accurately the baseline absolute risk of recurrence . 
through this modeling , we estimate the differences in absolute risk of distant recurrence across epclin scores and examine the impact of different amounts of statistical interaction between epclin and chemotherapy on these estimates . methods gene expression assay the 12 - gene mrna expression assay has been previously described in detail.20 - 22 in brief , the expression of three proliferation - related target genes ( birc5 , dhcr7 , ube2c ) , ve hormone receptorrelated target genes ( azgp1 , il6st , mgp , rbbp8 , stc2 ) , and three normalization genes ( calm2 , oaz1 , rpl37a ) were measured by reversetranscription quantitative polymerase chain reaction . 
a 12gene molecular score was calculated as the linear combination of the normalized target gene expression.11 , 22 the clinicomolecular score epclin was calculated by combining the 12 - gene molecular score with tumor size and the number of positive lymph nodes and was reported as a numerical score from 1 to 6.11 , 22 tumors with an epclin score of less than 3.3 are considered low risk for distant recurrence and tumors with scores of 3.3 or greater are considered high risk for distant recurrence.11 , 17 , 18 statistical methods the ability of epclin to provide an estimate of expected chemotherapy benet was modeled , as shown in figure 1 . the primary component was the prognostic value of epclin to predict the rate of distant recurrence in the rst 10 years of follow - up . 
 soliman et al 10 - year distant recurrence in patients treated with et + c ( treated ) was estimated by introducing a relative chemotherapy benet for a particular epclin score , hrtreatment , to the untreated risk according to a proportional hazards model ( fig 1b ) , as in equation 1 : rtreated ( cid : 1 ) 1 1 runtreated ( cid : 1 ) ( cid : 3 ) hrtreatment mathematically , the dependence of the relative chemotherapy benet on the risk of distant recurrence was modeled using a main effect for chemotherapy and an interaction between treatment status and the prognostic signature.23 interactions were modeled as a linear dependence of the logarithm of hr for treatment on epclin score according to equation 2 : ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 1 ) hrtreatment ( cid : 1 ) ( cid : 1 ) ln hroverall ( cid : 1 ) epclin epclinavg in this equation , represents the interaction strength and denes how strongly the relative chemotherapy benet for a patient depends on epclin score , epclinavg is the mean epclin score in the population , and hroverall is the hazard ratio for the chemotherapy benet in the population . 
with the maximum value of determined for an interaction giving no chemotherapy benet at epclinmin , weaker interactions were modeled using a percentage of the maximum value of ( fig 1b )  . finally , the absolute benet ab from chemotherapy for treated patients was determined according to equation 3 ( fig 1c ) : december 8 , 2017 , who received valid test results . formalin - xed parafn - embedded breast resections of treatment - nave er - positive , her2 - negative breast tissue were tested . 
these scores also were used to calculate epclinavg . results we examined the impact of different magnitudes of treatment effect and interaction strengths on the estimated 10 - year risk of distant recurrence ( table 1 )  . 
maximal interaction strength ( max = 0.159 ) was rst determined by assuming that a patients relative chemotherapy benet is 0 at the lowest possible epclin score and maintaining the hroverall of treatment at 0.7. 
the corresponding hrtreatment as a function of epclin score is shown in figure 2 . hrtreatment is 1 for a patient with an epclin score of 1 and 0.45 for a patient with the maximum observed epclin score of 6 . 
the risk of distant recurrence in the treated arm also was evaluated in a conservative scenario that assumed no interaction between chemotherapy benet and epclin score ( ie , 0% interaction strength , constant hrtreatment )  . 
in this scenario , the relative chemotherapy benet was equal to the overall chemotherapy benet ( = 0 ; hrtreatment = 0.7 ; fig 2 )  . after max was determined , risk of distant recurrence was calculated for scenarios with a variety of interaction strengths between epclin and chemotherapy . 
figure 3a shows the relationship between epclin score and predicted risk of distant recurrence by 10 years for untreated and treated patients under interaction strength ( 0% , 50% , and 100% )  . 
absolute chemotherapy benet for patients with low and high epclin scores assuming different overall relative chemotherapy benet ( 20% , 30% , or 40% ) for different relative interaction strengths ( 0% , 50% , or 100% ) absolute chemotherapy benet ( % ) 20% relative chemotherapy benet low epclin high epclin 0% relative interaction ( no interaction ) 50% relative interaction ab ( cid : 1 ) runtreated rtreated 100% relative interaction ( maximal ) 30% relative chemotherapy benet low epclin high epclin absolute chemotherapy benet for the low - risk category was calculated as a mean absolute chemotherapy benet for all low - risk patients , and the same went for the high - risk category . 
 predicting chemotherapy benet in early - stage breast cancer ln ( hrtreatment ) = ln ( hroverall ) ( epclin epclinavg ) 0% interaction strength ( = 0 ) 100% interaction strength ( = 0.159 ) epclin score fig 2 . 
patient benet from chemotherapy ( hrtreatment ) according to epclin score at no interaction ( 0% ) and maximal interaction ( 100% )  . recurrence is low for low epclin scores , which results in small absolute chemotherapy benet . 
for example , the expected absolute benet of chemotherapy treatment for a patient with low epclin scores ranged from 0.3% ( epclin = 1 ) to 2.9% ( epclin = 3.3 ) for 0% interaction strength and from 0% to 3.0% for 100% interaction strength . 
similar results were obtained when overall relative chemotherapy benet was modeled to be lower ( 20% ; fig 3b ) or higher ( 40% ; table 1 ; fig 3c )  . the various risk estimates across all scenarios of interaction strength were applied to a clinical cohort of patients with er - positive , her2 - negative breast resections and representative epclin scores ( n = 2 , 185 )  . 
the full epclin distribution is shown in figure 4 . overall , 1 , 275 samples ( 58% ) were low risk , and 910 ( 42% ) were high risk . 
risk of distant recurrence as a function of epclin score for different interaction strengths under different assumptions about overall relative chemotherapy benet : ( a ) 30% , ( b ) 20% , and ( c ) 40% . 
epclin scores in pretreatment estrogen receptorpositive , human epidermal growth factor receptor 2negative breast resection tissue ( n = 2 , 185 )  . the absolute chemotherapy benet in lowand high - risk patients was calculated as a function of interaction strength ( fig 5 )  . 
indeed , even with the strongest interaction , the absolute chemotherapy benet for a 30% relative benet in high - risk patients is 7.3% , which is not dramatically different from the 5.3% benet modeled in the patients with high ( 3.3 ) epclin score patients with low ( < 3.3 ) epclin score 40% overall benefit 30% overall benefit 20% overall benefit case of no interaction ( table 1 )  . 
similarly , in low - risk patients , the absolute benet is 1.5% when we assume the strongest interaction , which is close to a 1.8% benet in the case of no interaction . discussion previous studies have demonstrated that epclin accurately identies patients at low risk for distant recurrence 10 years after surgery , with improved prognostic performance compared with clinical features alone or other molecular tests.11 , 15 - 18 for these low - risk patients , it is clear that the addition of adjuvant chemotherapy likely will not yield any clinically meaningful risk reduction . 
here , we evaluated the capacity of epclin to identify patients with er - positive , her2 - negative earlystage breast cancer who may benet most from adding adjuvant chemotherapy to et . 
thus , we evaluated the impact by modeling across a range of potential chemotherapy effects sizes and interaction strengths with epclin . to minimize potential error associated with individual trial values , the absolute benet of chemotherapy in women with various epclin scores was modeled using wellestablished estimates of the average relative benet of adjuvant chemotherapy . 
this risk is particularly noteworthy in interventions in early - stage breast studies of adjuvant cancer because event rates may be low and distant recurrence may manifest many years or even decades after the initial diagnosis and treatment . 
as a result , the absolute predicted chemotherapy benet in low - risk patients was small and largely unaffected by average chemotherapy effect or interaction strength , whereas the toxicity of therapy remains the same . 
this association is irrespective of interaction strength between epclin and predicted chemotherapy benet , and the impact of any interaction on absolute benet is much smaller than the ability to accurately estimate absolute risk . as is typical of modeling studies , this study is not without limitations . 
of note , the approximately 30% reduction in distant recurrence was selected on the basis of its association with chemotherapy regimens that are more consistent with modern patterns of care in contrast to more historic regimens . other aspects of the statistical model are also limitations of the study . 
it is assumed that the relative benet of chemotherapy linearly depends on epclin score ( eq 2 ) , which is the simplest mathematical implementation of dependence . linear dependence also was used to demonstrate interaction between chemotherapy and a prognostic score.8 in statistical analysis , the most common implementation of interaction between variables has the same functional forin addition , only positive interaction between chemotherapy benet and epclin score was included in this analysis because it is expected that high expression of the proliferation - related genes in epclin is associated with higher rather than lower relative chemotherapy benet . 
conversely , high expression of the hormone receptorrelated genes is expected to be associated with smaller relative chemotherapy benet because er - negative tumors have a much stronger response to chemotherapy than er - positive tumors . 
this again corresponds to a positive interaction because the hormone receptorrelated genes contribute negatively to the epclin score . in summary , this modeling analysis demonstrates that epclin is able to predict which patients will gain maximum absolute benet from chemotherapy . 
in addition , these data indicate that the predicted absolute impact of chemotherapy on distant recurrence depends much more on the prognostic ability of the biomarker to predict an individual womans risk of recurrence accurately . 
endopredict has been shown in multiple studies to predict risk of distant recurrence accurately in women with er - positive , her2 - negative early - stage breast cancer who receive 5 years of et , with an accuracy similar to the other best breast prognostic tests and substantially better than the 21 - gene recurrence score ( oncotype dx ; genomic health , redwood city , ca ) .18 , 24 this modeling indicates identied a substantial proportion of that endopredict women whose risk of breast cancer recurrence was so low that the addition of adjuvant chemotherapy would not produce a clinically meaningful benet on recurrence risk . conversely , patients with high epclin scores were predicted to experience the greatest benet from chemotherapy regardless of the simulated interaction strength between epclin and predicted chemotherapy benet . 
flake , anthony magliocco , mark robson , lee schwartzberg , priyanka sharma , ralf kronenwett , alexander gutin , johnathan lancaster , jack cuzick , william gradishar collection and assembly of data : darl d . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . hatem soliman consulting or advisory role : celgene , astrazeneca , eli lilly , novartis , pzer , puma biotechnology research funding : amgen ( inst ) travel , accommodations , expenses : astrazeneca , eli lilly darl d . 
flake employment : myriad genetics stock and other ownership interests : myriad genetics patents , royalties , other intellectual property : multiple patents related to the development of tests at myriad genetics anthony magliocco stock and other ownership interests : protean biodiagnostics , the genomic cancer institute , proscia honoraria : bristol - myers squibb , merck , illumina , leica consulting or advisory role : bristol - myers squibb , merck , proscia , roche , illumina speakers bureau : bristol - myers squibb research funding : biotheranostics , roche , genentech patents , royalties , other intellectual property : various patents pending as co - inventor through moftt cancer center travel , accommodations , expenses : menarini silicon biosystems , illumina , bristol - myers squibb , merck , ventana medical systems mark robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca , merck , pzer , daiichi sankyo research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca , pzer lee schwartzberg stock and other ownership interests : vector oncology honoraria : pzer , amgen , nanostring technologies , novartis , napo , taiho pharmaceutical , genentech , e.r. 
squibb and sons , helsinn therapeutics , genomic health , myriad genetics , astrazeneca consulting or advisory role : bristol - myers squibb , pzer , helsinn therapeutics , caris life sciences , spectrum pharmaceuticals , tesaro , genomic health , astrazeneca , e.r. 
squibb and sons , amgen , f . hoffmann - la roche , genentech , eli lilly , novartis , merck , biocept , abbvie , biotheranostics , athenex , coherus biosciences speakers bureau : coherus biosciences , puma biotechnology research funding : amgen ( inst ) , glaxosmithkline ( inst ) , spectrum pharmaceuticals ( inst ) , medivation ( inst ) , bayer ag ( inst ) , genentech ( inst ) , pzer ( inst ) , tesaro ( inst ) , sano ( inst ) , e.r. 
n engl j med 319 : 1681 - 1692 , 1988 early breast cancer trialists collaborative group : tamoxifen for early breast cancer : an overview of the randomised trials . 
lancet 351 : 1451 - 1467 , 1998 early breast cancer trialists collaborative group ( ebctcg ) : effects of chemotherapy and hormonal therapy for early breast cancer on recurrence and 15 - year survival : an overview of the randomised trials . 
lancet 365 : 1687 - 1717 , 2005 peto r , davies c , godwin j , et al : comparisons between different polychemotherapy regimens for early breast cancer : meta - analyses of long - term outcome among 100 , 000 women in 123 randomised trials . 
curr treat options oncol 16 : 23 , 2015 paik s , tang g , shak s , et al : gene expression and benet of chemotherapy in women with node - negative , estrogen receptor - positive breast cancer . 
j clin oncol 24 : 3726 - 3734 , 2006 van de vijver mj , he yd , vant veer lj , et al : a gene - expression signature as a predictor of survival in breast cancer . 
gnant m , filipits m , greil r , et al : predicting distant recurrence in receptor - positive breast cancer patients with limited clinicopathological risk : using the pam50 risk of recurrence score in 1478 postmenopausal patients of the abcsg - 8 trial treated with adjuvant endocrine therapy alone . 
filipits m , rudas m , jakesz r , et al : a new molecular predictor of distant recurrence in er - positive , her2 - negative breast cancer adds independent information to conventional clinical risk factors . 
coates as , winer ep , goldhirsch a , et al : tailoring therapies - - improving the management of early breast cancer : st gallen international expert consensus on the primary therapy of early breast cancer 2015 . 
harris ln , ismaila n , mcshane lm , et al : use of biomarkers to guide decisions on adjuvant systemic therapy for women with early - stage invasive breast cancer : american society of clinical oncology clinical practice guideline . 
dubsky p , filipits m , jakesz r , et al : endopredict improves the prognostic classication derived from common clinical guidelines in er - positive , her2 - negative 17 . 
martin m , brase jc , calvo l , et al : clinical validation of the endopredict test in node - positive , chemotherapy - treated er + / her2breast cancer patients : results early breast cancer . 
buus r , sestak i , kronenwett r , et al : comparison of endopredict and epclin with oncotype dx recurrence score for prediction of risk of distant recurrence after endocrine therapy . 
warf mb , rajamani s , krappmann k , et al : analytical validation of a 12 - gene molecular test for the prediction of distant recurrence in breast cancer . 
sestak i , buus r , cuzick j , et al : comparison of the performance of 6 prognostic signatures for estrogen receptor - positive breast cancer : a secondary analysis of a randomized clinical trial . 
 applying precision oncology principles in radiation oncology radiation therapy is a critical component in the curative management of many solid tumor types , and advances in radiation delivery techniques during the past decade have led to improved disease control and quality of life for patients . 
during the same period , remarkable advances have also been made in understanding the genomic landscape of tumors ; however , treatment decisions in radiation oncology continue to depend primarily on clinical and histopathologic characteristics rather than on the genetic features of the tumor or the patient . 
with the development of novel genomic techniques and their increasing use in clinical practice , radiation oncology is uniquely positioned to leverage these advances to identify novel biomarkers that could inform radiation dose , field , and the use of concurrent systemic agents . 
2018 by american society of clinical oncology introduction radiation plays a central role in cancer management , and it is estimated that more than half of all patients with cancer will receive radiation therapy during their treatment course.1 radiation is used in a variety of clinical contexts , including in the definitive management of several solid tumor types as well as in palliation of symptoms associated with advanced disease.2 many of the changes in radiation oncology in recent decades have been driven by advances in imaging and dosimetry that have resulted in the ability to deliver higher radiation doses to tumor while minimizing the dose to surrounding normal tissue.3 in contrast , advances in understanding tumor biology and genetics have affected radiation oncology practice less to date , particularly when compared with other oncology specialties.4 , 5 currently , genomic biomarkers are rarely used to inform the use of radiation therapy . 
instead , clinical - pathologic factors , such as tumor size , histology , lymph node involvement , and surgical margin status , continue to drive radiation oncology standards of practice . 
thus , although radiation is a precision treatment modality in a spatial and anatomic sense , the potential to incorporate tumor genomic features as a precision tool in radiation oncology has not yet been realized . 
efforts by radiobiologists to understand and model these differences have driven current clinical strategies , such as dose fractionation ( ie , delivering a fractional dose of radiation each day over several weeks ) , that exploit differences in the radiation sensitivity of tumor and normal cells . 
the development of massively parallel sequencing and other high - throughput techniques has led to an explosion in available tumor genomic data , which provide a unique opportunity to map the landscape of radiation response across tumor types . 
nevertheless , defining the underlying genomic determinants of differential radiation response remains challenging for several reasons . historically , the tumoricidal effects of radiation were believed to be mediated primarily through dna damage , but accumulating evidence suggests that radiation has numerous effects on the sophia c . 
 tumor and microenvironment that vary on the basis of anatomic site , tumor histology , radiation dose and fractionation , and the use of concurrent therapies.6 , 7 therefore , the molecular underpinnings of radiation response may vary within and among tumor types and may be strongly dependent on clinical and treatment factors . when delivered in the neoadjuvant or definitive settings , radiation is often combined with cytotoxic chemotherapy , and separating the effects of each agent on tumor response is difficult . 
conversely , when radiation is used in the adjuvant setting , no measurable tumor is present , and response is defined by lack of tumor recurrence over months or years , which can be affected by factors beyond tumor cell radiosensitivity . finally , although comprehensive genomic profiling of thousands of tumors has been performed through efforts such as the cancer genome atlas , these studies often pool cases that represent diverse clinical settings and disease states , and detailed treatment and response data are often not available . 
furthermore , even when an association between a specific genomic event and treatment response is observed , rigorous experimental work is required to validate the association and establish causality . experimental systems to study radiation sensitivity many of the tenets of radiobiology were developed and validated using radiosensitivity assays , including in vitro approaches such as clonogenic cell survival and in vivo approaches using transplantable tumor systems.8 although these assays have been invaluable in establishing the mechanisms of radiation - mediated cell killing and the properties of dose fractionation , the assays are often time consuming , technically challenging , and difficult to scale . 
therefore , one of the most important challenges currently facing the field is the development of efficient and reliable techniques that faithfully recapitulate the effects of radiation to yield insights at both the cellular and tissue levels . in an attempt to comprehensively characterize associations between genomic features and radiation sensitivity , yard et al9 profiled radiation sensitivity across 533 genomically annotated cell lines representing 26 tumor types using a validated high - throughput assay . 
perhaps one of the most surprising findings from this study was the large variation in radiation sensitivity observed within and among lineages : many tumor types exhibited a greater than five - fold difference in survival between the mostand least - sensitive cell lines . 
conversely , mutations in several dna repair genes , such as brca1 , mlh1 , and atr , were associated with high point mutation frequency , low levels of aneuploidy , and radiation sensitivity . 
 whole - transcriptome gene expression profiling revealed that upregulation of pathways involved in dna damage response , cell cycle , and chromatin organization were associated with radiation sensitivity , whereas increased expression of genes in pathways involved in cellular signaling ( janus kinase - signal transducers and activators of transcription [ jak / stat ] and phosphatidylinositol 3 - kinase [ pi3k ] pathways ) , stem - cell state , and inflammation were associated with radiation resistance . 
this study is one of the largest efforts to date to investigate the association of tumor genomic features with radiation sensitivity and highlights the potential to leverage large data sets to study cellular radiation response . many other groups have studied gene expression patterns in an attempt to define transcriptional signatures of radiation response . 
several studies have identified an association between increased clonogenic survival of primary tumor cells irradiated ex vivo and worse clinical outcomes after radiation - based treatment.17 , 18 in addition , immunohistochemical ( ihc ) readouts of dna repair functionsuch as formation of functional dna repair foci after ex vivo tumor irradiationhave been described as a potential biomarker for predicting radiosensitivity.19 genetic changes that are unique to the experimental system.21 given the expanding role of numerous genomic and experimental platforms for tumor profiling , an important challenge will be developing tools for integrating multi - omic tumor data to derive clinically relevant insights . 
it is likely that the most powerful clinical insights will be achieved by combining analyses of large genomic data sets with functional data derived from experimental systems ( fig 1 )  . candidate clinical radiation biomarkers finally , recent efforts have focused on developing platforms for establishing patient - derived organoid and xenograft models that can serve as a living biobank to test drugs or other therapy combinations.20 the goal of these approaches is to identify personalized treatment approaches in a time frame that can be useful for individual patients . 
organoid and xenograft systems likely reflect more elements of relevant tumor biology than two - dimensional cell culture systems ; however , these systems are often more expensive and time consuming to develop and may select for dna repair pathway alterations have been studied extensively as potential biomarkers of radiation sensitivity , and several clinically relevant associations between dna repair deficiency and tumor biology have been described ( fig 2 )  . 
5 - fu , 5 - fluorouracil ; ai , aromatase inhibitor ; ar , androgen receptor ; bet , bromodomain and extra - terminal domain ; dna - pkcs , dna - dependent protein kinase catalytic subunit ; dnmt , dna methytransferase ; egfr , epidermal growth factor receptor ; er / pr , estrogen receptor / progesterone receptor ; fgfr , fibroblast growth factor receptor ; hdac , histone deacetylase ; her2 , human epidermal growth factor receptor 2 ; hif1 , hypoxia - inducible factor 1 ; lhrh , luteinizing hormonereleasing hormone ; msi , microsatellite instability ; parp , poly ( adp ) ribose polymerase ; pd - 1 , programmed cell death1 ; pd - l1 , programmed cell deathligand 1 ; serd , selective estrogen receptor degrader ; serm , selective estrogen receptor modulator ; tmb , tumor mutational burden ; vegf , vascular endothelial growth factor . properties and predicts response to conventional chemotherapy and immune checkpoint blockade25 , 26 ; however , msi is not currently a biomarker that directly affects radiation decision making . 
somatic mutations in the nucleotide excision repair gene ercc2 are associated with improved response to cisplatin - based chemotherapy and chemoradiotherapy in muscle invasive bladder cancer.27 , 28 deleterious germline and somatic mutations in homologous recombination ( hr ) genes such as brca1 , brca2 , palb2 , and atm occur across tumor sites . 
although the rates are highest in breast and ovarian cancers , a subset of other tumors also have hr gene alterations or have mutational patterns suggestive of functional hr loss.29 because hr is a primary repair mechanism for radiation - induced dna double strand breaks ( dsbs ) , it has been hypothesized that hr - deficient tumors may have heightened radiation sensitivity . 
however , defining the clinical role of hr gene alterations as a radiation biomarker has been challenging for several reasons.30 radiation is not part of the standard treatment of ovarian cancer and is typically used in the adjuvant setting in breast cancer , making it more challenging to assess treatment response than in settings where radiation is used to treat gross disease . 
 carriers treated with lumpectomy and adjuvant radiation for localized breast cancer have reported higher rates of ipsilateral breast event rates ( tumor recurrence and / or second primary tumors ) among brca1 / 2 carriers , whereas others have found no difference.32 - 34 the rate of contralateral breast cancer is significantly higher in brca1 / 2 carriers than in noncarriers , 35 and the role of germline brca1 / 2 status in driving clinical management ( including prophylactic mastectomy and oophorectomy ) is an active area of investigation with important medical and socioeconomic implications . homologous recombination deficiency was also recently identified as a relatively common feature of metastatic prostate tumors , 36 and germline hr alterations are surprisingly frequent among men with metastatic disease.37 hr - deficient prostate cancers have aggressive clinical behavior and respond to poly ( adp ribose ) polymerase ( parp ) inhibitors38 , 39 ; however , it is not known if hr alterations predict improved response to definitive radiation for men with localized prostate cancer . 
similarly , the prognostic and predictive implications of hr pathway alterations in other tumor types in which radiation is used in the first - line settingsuch as gastric and pancreatic cancershave not yet been defined . 
 in pancreatic cancer , patients with a family history of breast , ovarian , or pancreatic cancer had significantly improved survival after platinum - based chemotherapy compared with patients with sporadic disease , suggesting that germline brca1 / 2 - mediated hr deficiency may contribute to treatment response.40 - 42 somatic mutations in the dsb checkpoint kinase ataxia telangiesctasia mutated ( atm ) have been associated with durable responses to radiation for recurrent or metastatic lesions , 43and increased ihc staining of the dsb nuclease mre11 is associated with improved outcomes after radiotherapy in muscle - invasive bladder cancer.44 , 45 in addition to dna repair pathway alterations , numerous other tumor genomic features have been correlated with clinical radiation response ( fig 2 )  . 
activating kras mutations are associated with resistance to radiation as well as to numerous conventional and targeted systemic agents.46 , 47 oncogene activation can result in increased oxidative stress in tumor cells , and mutations in keap1 , or the keap1 - binding region of nfe2l2 ( which encodes nuclear factor erythroid 2 - related factor 2 [ nrf2 ] ) , can result in stabilization of nrf2 and transcriptional upregulation of oxidative stress response genes . 
keap1 mutations are associated with radiation resistance in cell lines and have been shown to drive tumor formation and radiation resistance in a mouse model of lung squamous cell cancer.48 , 49 keap1 mutations are enriched in patients with lung cancer who develop local recurrence after radiation , consistent with a role in mediating radiation resistance.48 the advent of next - generation sequencing techniques has allowed genomic analyses to be performed from small amounts of formalin - fixed paraffin - embedded tumor tissue.50 in addition to characterizing features of primary ( pretreatment ) tumors , these techniques can also be applied to post - treatment residual or recurrent tumors to provide a window into mechanisms of radiation - induced tumor evolution . 
 sequencing of preand post - chemoradiotherapy rectal tumors suggest enrichment of tp53 or co - occurring kras / tp53 mutations in poorly responding tumors , 51 , 52 and enrichment of kras / tp53 mutations were also noted in liver metastases that recurred after proton - based stereotactic radiotherapy.53 analysis of preand post - treatment anal cancer showed enrichment or emergence of mutations in known cancer genes , such as tp53 , pik3ca , and fbxw7.54 interestingly , in both the rectal and anal tumor cohorts , numerous subclonal mutations were gained or lost through treatment , but there was no change in overall mutational burden . 
 finally , there is immense interest in the use of minimally invasive techniques , such as circulating tumor dna ( ctdna ) and circulating tumor cell ( ctc ) analyses , to monitor disease status and treatment response . 
it is already clear that many of the common genomic features of tumors have important prognostic implicationsthat is , the genomic event is associated with better ( or worse ) clinical outcomes independent of the type of treatment . 
however , to advance precision radiation oncology , it will also be critical to identify genomic features that , although perhaps not strongly prognostic , are predictive of favorable response to radiation . 
however , despite the lack of mutation - based biomarkers , several gene expression signatures have been validated as prognostic and predictive tools in a variety of radiation settings . one of first gene expression signatures to be widely used in clinical practice was the oncotypedx test , which measures expression of a panel of genes involved in estrogen receptor signaling and cell proliferation.61 although the assay was initially validated to predict benefit of adjuvant chemotherapy in estrogen receptor positive breast cancer , it has now been studied in other contexts and can be used to estimate risk of locoregional recurrence after radiation for invasive cancer62 or ductal carcinoma in situ.63 similar approaches have also been used in the post - mastectomy setting.64 clinical trials are ongoing to investigate if transcriptional signatures can be used to prospectively identify women at low risk of locoregional recurrence for whom post - lumpectomy radiation can be omitted ( clinicaltrials.gov identifier : nct02653755 ) .65 gene expressionbased assays are also being used to inform management of prostate cancer . 
lin et al77 showed that higher pretreatment plasma ebv titers ( > 1 , 500 copies / ml ) were associated with worse outcomes after chemotherapy and radiation in patients with stage iii and iv npc . 
historically , patients with medulloblastoma were defined as standard risk or high risk on the basis of clinical features , and chemotherapy and radiation decisions were driven by clinical risk group . 
however , elegant work by several groups has identified four consensus molecular subtypes of medulloblastoma with distinct biology and clinical behavior.78 patients with tumors harboring mutations in the wingless - type mmtv1 integration site ( wnt ) pathway ( such as ctnnb1 ) have extremely good prognosis , patients with group 3 tumors have extremely poor prognosis , and patients with group 4 tumors or tumors with alterations in the sonic hedgehog ( shh ) pathway ( such as ptch1 , gli3 , mycn ) have intermediate prognoses . 
for example , the childrens oncology group is examining the role of reduced - dose craniospinal irradiation ( csi ) and chemotherapy for wntdriven medulloblastoma ( clinicaltrials.gov identifier : nct02724579 )  . 
similarly , st judes hospital is evaluating different radiation and drug combinations across molecular subtypes ( clinicaltrials.gov identifier : nct01878617 ) : patients with low - risk wnt pathway mutations will receive dose - reduced csi , and patients with shh alterations will receive an shh inhibitor ( vismodegib ) after four cycles of standard chemotherapy . 
if successful , these studies have the potential to maximize cure rates while minimizing the known acute and late toxicities of chemotherapy and csi in pediatric patients . in current practice , the prescribed radiation dose is defined by tumor histology , with doses reduced when necessary to avoid exceeding normal ( nontumor ) tissue tolerance . 
instead , normal ( nontumor ) radiation dose limits are typically selected to limit the rate and severity of toxicity to an acceptably low level ( often 5% )  . 
therefore , prospectively identifying the patients at highest risk for normal tissue toxicity could inform mitigation strategies such as dose de - escalation or aggressive supportive care in the most sensitive patients and , conversely , could allow for dose escalation in the majority of the population who are at lower risk for normal tissue toxicity.86 many preclinical and retrospective clinical studies have attempted to identify germline factors that affect radiation sensitivity.87 , 88 candidate gene approaches focusing on genes involved in dna damage signaling and repair have identified associations between specific germline alleles in dna repair genes and increased normal tissue sensitivity to radiation , but many of these associations have failed to validate in larger cohorts.89 genome - wide association studies have also identified associations between specific single nucleotide polymorphisms and radiation sensitivity . 
although some of these alleles occur in genes known to play a role in cancer biology or tissue injury , many exist in noncoding regions of the genome and / or have no obvious role in damage - related cell signaling . 
therefore , additional work will be needed to validate these associations and uncover the relevant biology . in addition to defining predictive biomarkers of radiation toxicity , efforts have also focused on developing functional assays to profile and predict normal tissue toxicity . 
for example , increased radiation - induced apoptosis of circulating cd8 + t lymphocytes from patients undergoing breast radiotherapy was associated with increased risk of late breast fibrosis.90 ideally , genetic and functional data reflecting the sensitivity of both the tumor and normal tissue to radiation would be used to personalize radiation dose for individual patients . one of the most feared and life - threatening late toxicities of radiation is radiation - induced second malignancy ( smn )  . 
smns typically develop in normal tissues adjacent to the treated tumor and have unique genomic features and aggressive clinical behavior.91 - 93 the risk of developing an smn depends on multiple factors , including age at radiation , anatomic site , and radiation dose . 
 germline mutations in known cancer genes such as tp53 and rb1 can increase the risk of smn after radiation.94 however , accurately predicting smn risk is challenging in part because radiation - induced tumors often take years to develop ; therefore , patients who present with an smn were often treated using techniques that no longer reflect the standard of care . 
radiosurgery ( rs ) - based treatments are now commonly used in many disease settings and are capable of precisely delivering high doses of radiation in just a single fraction or over a small number of treatments.95 rs - based approaches minimize toxicity by using advanced delivery techniques to reduce normal tissue radiation exposure and can also increase patient convenience by decreasing the number of treatment visits . currently , the decision to pursue rs - based treatment is dependent on clinical factors such as tumor size and location . 
for example , the classic radiobiology tenets of sublethal damage repair and cell cycle redistribution between fractionated radiation treatments are likely less relevant in rs - based therapy.96 rs doses may increase the extent of dna damage or create dna lesions that are more difficult to repair than those created by conventional doses . 
 however , the contribution of each of these factors has not been firmly established , and much of the observed efficacy of rs treatments may be due simply to the ability to deliver a higher biologically relevant dose.99 , 100 tumor genomic features that affect the dose dependent radiation response have the potential to serve as biomarkers to inform selection of the dose and fractionation scheme . 
specifically , rs - based dose escalation may be particularly beneficial in specific populations of cells , such as hypoxic cells or cancer stem cells , that are traditionally considered to be radioresistant . 
in addition , the potential to induce systemic immune responses using rs is of substantial interest in the setting of combined immune checkpoint blockade . radiotherapy with charged particles ( such as protons or carbon ions ) is becoming increasingly common in some developed countries . 
charged particles have distinct physical properties that make them attractive for treatment of specific tumor types.101 in addition to their unique physical properties that can be exploited to minimize dose to normal tissues , charged particles may induce tumor cell death via distinct mechanisms . 
for example , charged particles may be less dependent on oxidative intermediates to create lethal dna damage and may therefore be more effective for hypoxic tumors.102 in addition , emerging evidence suggests that charged particles may elicit a host immune response that is distinct from the immune response elicited by conventional ( photon - based ) radiation , 103 and studies reporting associations between specific genomic features and response to particle therapy are now emerging.53 radiomics and molecular imaging imaging - based analyses are a particularly promising tool for precision radiotherapy because they are noninvasive and can be used longitudinally to assess tumor response during and after treatment . 
radiomics is an emerging field of study that aims to characterize and quantify imaging properties of tumors and correlate these features with available genomic or clinical data to define new image - based biomarkers.104 quantifying novel anatomic and functional features of tumors can provide relevant clinical insights , and examples of the potential utility of radiomics based analyses are now being reported . 
in one large study , computed tomographybased imaging features such as tumor shape , contrast , and texture had independent prognostic power in several cohorts of lung and head and neck cancers.105 radiomics features also correlate with genomic properties ; for example , arterial phase imaging traits were associated with a doxorubicin resistance transcriptional program in hepatocellular carcinoma.106 functional imaging studies also have the potential to be rich sources of radiomics data . 
positron emission tomography ( pet ) tracer uptake ( as measured by standard uptake value ) has been studied as a potential prognostic and predictive biomarker in several tumor types , 107 and more complex metrics that incorporate both anatomic and functional outputs are now being explored . advanced imaging techniques allow improved visualization of both tumor and normal tissue , and many of these imaging modalities are now routinely integrated into radiation oncology practice . 
daily imaging with either two - dimensional ( x - rays ) or three - dimensional ( computed tomography ) techniques is used to ensure set - up reproducibility and minimize the effect of interfraction changes in anatomy ( such as bowel or bladder filling )  . 
intrafraction motion can also be managed using techniques that account for positional uncertainty in the planning phase or directly track the position of an implantable beacon and adjust the radiation field in real time . in addition to techniques for ensuring reproducible patient position and accounting for slight variations in anatomy , advanced imaging modalities ( such as magnetic resonance imaging or pet ) can also be used to measure tumor response during the treatment course . 
 adaptive planningupdating the radiation plan during the treatment course on the basis of tumor responsehas the potential to maximize dose delivery to areas of persistent tumor while sparing normal tissue in areas where tumor has regressed.108 - 110 for example , an attractive property of particle therapy is the potential to use pet techniques to monitor in vivo dosimetry . 
 pet imaging can be used to detect positron emissions created from inelastic nuclear collisions of protons with elements in tissues , thereby creating a radiation dose distribution from proton111 , 112 or carbon ion113 radiation . 
 for adaptive radiation planning on the basis of delivered dose to the target and adjacent normal tissue.114 prospective studies are being conducted in multiple disease settings to study the impact of adaptive on - treatment planning on outcome and toxicity . 
early results from single - arm studies suggest that dose escalation using adaptive radiation techniques can be performed safely and are associated with promising local control rates115 - 117 ; however , results from randomized trials ( such as clinicaltrials.gov identifier : nct01507428 ) will be required to confirm that shrinking the radiation fields does not compromise disease control by sparing regions that appear normal on imaging but harbor residual microscopic disease . identifying and targeting tumor hypoxia many tumors contain hypoxic regions , and hypoxic conditions are known to induce tumor cell radioresistance.118 a direct measure of tumor hypoxia can be performed using an oxygenation probe , but this method is invasive and cannot readily distinguish between viable hypoxic regions of the tumor and dead / necrotic tumor . 
 noninvasive functional imagingbased methods are also available , such as 18f - fluoromisonidazole pet imaging , which uses a hypoxia - sensitive chemical probe . measures of hypoxia can also be estimated from harvested tumor specimens . 
for example , increased ihc levels of hypoxia - inducible factor 1 ( hif1 ) have been associated with worse outcomes after radiotherapy in several clinical contexts , 119 and in a randomized trial for muscle invasive bladder cancer , only tumors with high hif1 staining benefitted from the addition of the antihypoxia agents carbogen and nicotinamide to radiation.120 gene expression signatures have also been used to identify tumor hypoxia . 
the rationale for combining radiation with chemotherapy was outlined by steel124 and others in the 1970s , and despite preceding the advent of modern molecular cancer biology , this contextual framework remains relevant to understanding the interplay of radiation with chemotherapy and targeted agents . systemic agents have the potential to interact with radiation to produce additive , synergistic , or antagonistic effects , and the net biologic response is dependent on both tumor and host genomic features ( fig 2 )  . 
despite the widespread use of concurrent chemoradiotherapy regimens , the molecular features that drive response and / or toxicity with these combinations remain poorly understood , and treatment decisions continue to be driven primarily by clinical factors , such as patient age , performance status , and tumor histology , rather than by tumor genomic features . 
 however , given the proven efficacy of combined chemoradiotherapy approaches , future efforts should focus not only on discovering novel targets and therapies but also on defining reliable genomic biomarkers that predict response to existing cytotoxic regimens . molecularly targeted therapies have transformed the management of diseases such as chronic myelogenous leukemia and nonsmall - cell lung cancer . 
as with conventional chemotherapy , there are several potential therapeutic advantages to combining targeted agents with radiation ( table 1 ) .125 , 126 in the primary tumor , targeted agents may radiosensitize tumor cells , resulting in improved local control and / or allowing for radiation dose de - escalation . 
the sequence of therapies is an important factor that may affect the interactions between radiation and targeted agents at the cellular and systemic levels , and the best outcomes will be achieved when the correct combination is provided in the correct genomic context with the correct timing ( fig 2 )  . given that dna damage is a major mechanism of radiation - induced cell killing , there has been significant interest in combining targeted inhibitors of dna repair with radiation.127 , 128 as large genomic studies continue to define the landscape of dna repair pathway deficiencies across tumor types , it will be critical to match dna repair inhibitors with the tumor genomic contexts in which maximum benefit can be achieved when combined with radiation . 
inhibitors of parp are the most clinically advanced dna repair directed agents and are now approved for the treatment of hr - deficient tumors , such as those with brca1 / 2 mutations.129 preclinical evidence suggests that parp inhibition may synergize with radiation to kill tumor cells , and clinical trials combining parp inhibitors with radiation are now open . 
it is unknown whether adding parp inhibition to radiation will primarily benefit hr - deficient tumorsthe setting in which the largest parp inhibitor monotherapy effect has been observedor whether parp inhibition might best be used to sensitize hr - proficient tumors to radiation - induced dna damage . 
in addition to parp inhibitors , combination trials of radiation plus inhibitors of numerous different kinases that are involved in orchestrating the cellular response to dna damage ( including atm , atr , chek1 / 2 , wee1 , and prkdc [ dna - pkcs ] ) are also underway ( table 1 )  . inhibition of receptor tyrosine kinaseswith either antibodies or small moleculesrepresents one of the most well - developed and successful targeted therapeutic strategies to date , and inhibitors of several families of receptor tyrosine kinases are us food and drug administration approved . 
 repair genes such as prkdc ( encoding dnapkcs ) to promote radioresistance , 145 - 147 and this ar - mediated radioresistance can be countered with adt . the androgen receptor is also found in a subset of breast tumors , and increased ar transcript levels are associated with radioresistance and increased risk of local recurrence.148 , 149 in preclinical systems , blocking ar signaling with enzalutamide led to increased levels of dna damage and cell death after radiation , and adt and radiation cooperate to decrease cell growth in orthotopic breast cancer models.9 interestingly , although the interactions between radiation and estrogen signaling in breast cancer have been extensively studied , there is no standard for sequencing of antiestrogen therapy and radiation in the breast - conserving or post - mastectomy setting.150 radiation is also being investigated in combination with modulators of intracellular signaling pathways . 
for example , activating pik3ca mutations are common in head and neck squamous cell cancers , and increased activity of the pik3 / akt serine / threonine kinase ( akt ) / mammalian target of rapamycin ( mtor ) signaling pathway drives cellular growth , proliferation , and a radioresistant phenotype . 
 accordingly , depletion or pharmacologic inhibition of pi3k impairs dna repair and confers radiosensitivity in cell lines with activating pik3ca mutations.151 , 152 numerous drugs targeting epigenetic processes are also being tested in combination with radiation . 
 for example , the histone deacetylase inhibitor vorinostat has shown radiosensitizing effects in preclinical studies.153 , 154 a clinical trial combining vorinostat with temozolomide and radiation in newly diagnosed glioblastoma multiforme showed the combination to be safe ; however , the primary efficacy end point was not met.155 , 156 as the portfolio of targeted therapies continues to expand , and as targeted agents become approved for first - line use in more settings , significant work will be needed to understand the interactions of these agents with radiation . 
the identification of reliable predictive biomarkers for both the targeted agent and radiation will be critical to ensuring that combinations are applied in the most rational way to maximize benefit . combining radiation with immunotherapy inhibitors the discovery and clinical development of therapies that modulate the host immune response has transformed oncology practice , and immune checkpoint ( anticytotoxic t - cell lymphocyte - 4 [ ctla - 4 ] , anti - programmed cell death 1 [ pd1 ] , and antiprogrammed death ligand 1 [ pd - l1 ] ) are now approved in numerous clinical settings . 
given the widespread incorporation of these agents , there is intense interest in combining immunotherapies with radiation , and the topic has been addressed comprehensively in several recent reviews.157 - 159 the interaction between the immune system and radiation has been appreciated for decades160 , 161 ; however , the tumor and host genomic features governing the interplay between immune directed therapies and radiation are incompletely understood . 
remarkable case reports of an abscopal effect , in which radiation drives regression of lesions outside the radiation field , have become more common in the era of immune checkpoint inhibitors , 162 , 163 but the mechanisms remain unclear , and it is currently impossible to predict which patients may experience a systemic response to localized radiation . 
it is likely that tumor and host genomic features as well as clinical factors such as radiation field size , dose , and fractionation pattern play a role . in preclinical models , radiation has been shown to have both immune - stimulating and immune suppressive effects . 
advances in imaging and dosimetry have allowed radiation to become remarkably precise in its physical delivery ; however , recent advances in cancer biology and genomics must now be translated into clinical radiation oncology practice to further maximize the therapeutic potential of radiation . many oncology centers are now performing routine genomic analysis of primary tumor specimens from patients . 
although these assays often identify genomic features that are known to be prognostic , translating these findings into actionable treatment decisions at the point of care remains a significant challenge ( fig 3 ) .169 the recent advent of noninvasive biomarkers such as circulating tumor dna and circulating tumor cellswill likely become integral techniques in monitoring disease response and identifying resistance mechanisms . incorporating genomic biomarkers to shift radiation oncology practice represents a unique challenge . 
radiation has complex , dose - dependent cellular effects and is often combined with systemic agents ; therefore , defining reliable signatures of radiation response will require unraveling intricate interactions among signals and effectors . 
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rieckmann t , tribius s , grob tj , et al : hnscc cell lines positive for hpv and p16 possess higher cellular radiosensitivity due to an impaired dsb repair capacity . 
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 genomic characterization of erbb2 - driven biliary cancer and a case of response to ado - trastuzumab emtansine sebastian mondaca , md1 ; pedram razavi , md , phd1 , 2 ; chongrui xu , md , phd1 ; michael ofn , md1 ; mackenzie myers , ms1 ; maurizio scaltriti , phd1 ; jaclyn f . 
abou - alfa , md , mba1 , 2 purpose biliary tract cancers ( btcs ) , which include intrahepatic cholangiocarcinoma ( icc ) , extrahepatic cholangiocarcinoma ( ehc ) , and gallbladder cancer ( gbc ) , have limited treatment options . 
twenty - eight patients ( 5.4% ) had erbb2 alterations , including 2.7% with erbb2 gene amplication , 2.3% with erbb2 mutation , and 0.4% with concurrent amplication and mutation . 
frequent co - altered genes in this cohort were tp53 ( 54% ) , pik3ca ( 21% ) , and cdkn2a ( 18% ) ; kras amplication / mutation was found in 7% of patients . 
2019 by american society of clinical oncology introduction biliary tract cancer ( btc ) comprises three clinically and molecularly distinct entities , intrahepatic cholangiocarcinoma ( icc ) , extrahepatic cholangiocarcinoma ( ehc ) , and gallbladder cancer ( gbc )  . 
genomic proling of btcs with next - generation sequencing ( ngs ) platforms has shown that the three clinical subtypes have signicant molecular differences.5 whereas all three have a high prevalence of tp53 and cdkn2a mutations , genomic alterations in fgfr2 and idh1 are mostly limited to icc ( approximately 20% each )  . 
 mondaca et al context key objective to describe the landscape of erbb2 genomic alterations in biliary tract cancer and illustrate a case of a patient who responded to antihuman epidermal growth factor receptor 2 ( her2 ) targeted therapy . knowledge generated erbb2 amplication or mutations were identied in 28 ( 5.4% ) of 517 patients with biliary tract cancer . 
erbb2 - driven biliary tract tumors had higher concurrent alterations of tp53 and pik3ca , while kras alterations seemed to be less common . one patient with erbb2 - amplied extrahepatic cholangiocarcinoma had a partial response to the her2 - targeted antibodydrug conjugate ado - trastuzumab emtansine . relevance potentially targetable erbb2 amplication and mutation are present in a signicant group of biliary tract tumors , particularly in gallbladder cancer . 
this study supports prospective testing for erbb2 alterations to develop novel anti - her2 strategies in this population . rst - line chemotherapy compared with patients with erbb2 wild type . on the basis of demonstrated improved os in pivotal phase iii trials , drugs that target her2 are standard treatment in her2 - overexpressed breast and gastric cancers.9 , 10 given the low incidence of btcs , the clinical characterization of relevant molecular subgroups , such as erbb2 - amplied or erbb2 - mutant btcs , has been limited , and the clinical experience with anti - her2 agents in this group has been largely anecdotal . 
a recent basket trial showed objective response in four ( 36% ) of 11 patients with erbb2amplied or erbb2 - mutant btc treated with the combination of the anti - her2 antibodies trastuzumab and pertuzumab.11 the aim of the current study was to comprehensively describe the clinical and molecular characteristics of erbb2 - amplied or erbb2 - mutant btcs identied within the context of a prospective tumor proling initiative at memorial sloan kettering ( msk ) cancer center . we also report a durable response to the her2 - targeted antibody - drug conjugate ado - trastuzumab emtansine ( t - dm1 ) in a patient with erbb2 - amplied btc enrolled in a basket trial ( clinicaltrials.gov identier : nct02675829 )  . methods patients demographic data and treatment histories were collected for all patients with erbb2 - altered btc who consented for prospective tumor genomic proling using the us food and drug administrationauthorized msk - impact assay between february 2014 and june 2018 . 
informed consent for tumor proling and clinical data collection was obtained under the genomic proling in cancer patients protocol ( clinicaltrials.gov identier : nct01775072 ) , which was approved by the msk institutional review board . data collection clinical data were extracted from electronic medical records . variables collected were demographic characteristics ( age , sex , race ) , eastern cooperative oncology group performance status , tumor type ( icc , ehc , gbc ) , metastatic sites , systemic treatments received , and clinical outcomes . 
all tumors were prospectively reviewed to conrm histology and to estimate tumor purity . molecular proling and genomic analysis memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) was performed as previously described in a clinical laboratory improvement amendmentscertied laboratory.12 , 13 msk - impact sequences at high coverage all exons and selected intronic and noncoding regions of up to 468 cancer - associated genes . 
baseline characteristics characteristic illustrative case one patient with metastatic erbb2 - amplied ehc was treated with t - dm1 in a basket trial at msk for patients with her2 - amplied or her2 - mutant cancers in the cohort of other solid tumors . 
methods and partial results of this trial have been presented previously , 15 , 16 but to our knowledge , this would be the rst publication about the patient with btc from the basket trial . 
this study was approved by the msk institutional review board , and all patients signed informed consent in accordance with the precepts of the declaration of helsinki . results patients and molecular prole during the period considered in this study , 517 patients with btc underwent msk - impact testing . 
in the subset of patients with btc with erbb2 - amplied or erbb2 - mutant tumors , the median age at diagnosis was 64 years ( range , 27 - 82 years ) , and the most frequent stage of presentation was stage iv ( 50% )  . 
the most frequently mutated domain of her2 was the extracellular domain ( 32% ) , and all mutations in this region arose at the s310 codon ( fig 1 )  . missense mutations represented the most common alteration in the mutated group ( 94% )  . 
of patients age , years median ( range ) male female race white asian black unknown primary tumor stage at diagnosis genomic alteration erbb2 amplication erbb2 mutation erbb2 amplication / mutation first sites of metastasis liver lung bone peritoneum other btc , no . 
the patient then received adjuvant gemcitabine , but within 3 months of initiation of systemic chemotherapy , imaging showed progression of disease in the posterior mediastinum , liver , and peritoneua biopsy specimen of the table 3 . 
aa , amino acid ; furin - like , furin - like cysteine - rich region ; gf_recept - iv , growth factor receptor domain iv ; pkinase_tyr , protein tyrosine kinase domain ; recep_l , receptor l domain . mediastinal metastasis conrmed recurrence ; immunohistochemistry revealed 3 + her2 protein overexpression . the patient was then treated with t - dm1 3.6 mg / kg once every 21 days in a basket trial and achieved a conrmed partial response after 12 weeks of treatment ( fig 3 )  . 
despite ongoing treatment with t - dm1 , the patients disease progressed after 8.6 months with the development of a new 2.2 - cm ( short - axis ) retrocaval lymph node . 
cancer antigen 19 - 9 was 10 , 700 u / ml before starting t - dm1 and decreased to 73 u / ml after achieving a conrmed partial response , with cancer antigen 19 - 9 remaining stable at the time of disease progression ( 62 u / ml )  . 
however , with the development of a new site of disease , t - dm1 was discontinued . discussion this study reports that potentially targetable erbb2 amplication or mutation was present in 5.4% of a cohort of 517 patients with btc who underwent prospective tumor molecular characterization at our institution . 
a similar gradient was described in a previous study that reported 16% , 11% , and 3% of erbb2 amplication in gbc , ehc , and icc , respectively.5 we also found that msi - high tumors were more frequent in the erbb2 - altered cohort compared with tumors without these alterations . 
similar ndings have been described in erbb2 - mutant colon cancer17 ; however , it is not clear whether this represents a biologically meaningful association or passenger erbb2 mutations are more frequent in tumors with an increased tumor mutational burden . 
erbb2activating mutations have been previously described to be present in 1% to 8% of btcs ; the potential therapeutic signicance of these mutations is an active area of research.5 as an example , 20 patients with her2 - mutant btc were enrolled in a basket trial of the pan - her tyrosine kinase inhibitor neratinib ( clinicaltrials.gov identier : nct01953926 ) , with two ( 10% ) achieving a partial response.18 this trial the clinical activity of found that neratinib varied as a function of tumor site , with the most promising clinical activity observed in her2 - mutant breast cancer ( 32% ) but no recist responses in several other cancer types , including bladder and colon cancers.19 the likelihood of clinical response to neratinib also varied as a function of mutation type . 
in another basket study , the response rate of patients with her2 - mutant nonsmall - cell lung cancer to t - dm1 was 44%.15 it remains unknown whether her2targeted antibody drug conjugates would have similar activity in her2 - mutant btc . we report here a patient with erbb2 - amplied btc who achieved a partial response to the her2 - targeted antibodydrug conjugate t - dm1 . 
 mutation count mutation spectrum msi type cancer type sample type erbb2 egfr erbb3 erbb4 fgfr2 pik3ca akt1 tsc2 tp53 mdm2 smad4 arid1a arid1b arid2 kmt2c kras cdkn2a idh1 bap1 mondaca et al stable indeterminate instable primary metastatic female male 100% genomic alterations missense mutation ( putative driver ) missense mutation ( unknown significance ) truncating mutation in - frame mutation fusion amplification deletion no alterations fig 2 . 
ehc , extrahepatic cholangiocarcinoma ; gbc , gallbladder cancer ; icc , intrahepatic cholangiocarcinoma ; msi , microsatellite instability . basket trials , conduct of dedicated trials that include an erbb2 - altered btc cohort has been more challenging . currently , a phase ii trial in china is evaluating the combination of gemcitabine plus oxaliplatin and trastuzumab in erbb2 - amplied btc ( clinicaltrials.gov identier : nct02836847 )  . 
her2 overexpression by immunohistochemistry and uorescence in situ hybridization has been pivotal for the approval of her2 - targeted therapies in breast and gastric cancers.9 , 10 however , tissuebased ngs analyses can identify both mutation and amplication along with other potential actionable targets . given the good correlation for amplication among these methods14 and the increasing clinical use of ngs , we believe that this approach represents an appropriate inclusion criterion in clinical trials . 
first , the cohort represents a selected population treated at a single academic cancer center that favors clinical trial enrollment ; hence , the patients with btc studied may have had different characteristics compared with those being treated in a community setting . 
 erbb2 amplication and mutation in biliary tract cancer baseline 3 months 8.6 months 30% present 80% present new retrocaval ln target lesions ( liver ) nontarget lesions new lesions 10 , 000 8 , 000 6 , 000 4 , 000 2 , 000 months fig 3 . 
ca , cancer antigen ; ln , lymph node . reported treatment is greater than 1.3 times the pfs on the prior line of therapy , the reported treatment can be considered benecial.26 in the case presented here , the patient progressed within 3 months after starting adjuvant chemotherapy and had a pfs of 8.6 months on rst - line t - dm1 , which supports a clinically meaningful benet . 
abou - alfa , md , memorial sloan kettering cancer center , 300 e 66th st , new york , ny 10065 ; twitter : @gaboualfa , @sloan_ kettering ; e - mail : abou - alg@mskcc.org. support supported by national institutes of health memorial sloan kettering cancer center core grant no . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . sebastian mondaca consulting or advisory role : foundation medicine pedram razavi consulting or advisory role : novartis research funding : grail ( inst ) , illumina ( inst ) chongrui xu honoraria : astrazeneca , boehringer ingelheim , eli lilly , msd , novartis , pzer , roche consulting or advisory role : boehringer ingelheim , pzer travel , accommodations , expenses : astrazeneca , boehringer ingelheim , eli lilly , novartis , pzer , roche , bristol - myers squibb , msd michael ofn consulting or advisory role : pharmamar , novartis , targeted oncology travel , accommodations , expenses : bristol - myers squibb , merck sharp & dohme maurizio scaltriti stock and other ownership interests : loxo oncology honoraria : menarini , adc therapeutics consulting or advisory role : menarini research funding : menarini ( inst ) , immunomedics ( inst ) , targimmune therapeutics ( inst ) , puma biotechnology ( inst ) , daiichi sankyo ( inst ) patents , royalties , other intellectual property : pi3k inhibitors and uses thereof , us provisional application no . 
62 / 742 , 163 , inventors : maurizio scaltriti , dan heller , jos e baselga , yosef shamay , carles monterrubio , amaia arruabarrena ( inst ) ; methods for detecting her2 dimerization in patients with her2 mutant lung cancers and predicting responsiveness to ado - trastuzumab emtansine therapy , sk2018038 - 01 , inventors : maurizio scaltriti , bob t . 
solit stock and other ownership interests : loxo oncology consulting or advisory role : pzer , loxo oncology , illumina , intezyne technologies , vivideon therapeutics , eli lilly travel , accommodations , expenses : merck kgaa bob t . 
li consulting or advisory role : roche , biosceptre international , thermo fisher scientic , mersana , guardant health , hengrui therapeutics research funding : roche ( inst ) , genentech ( inst ) , illumina ( inst ) , biomed valley discoveries ( inst ) , astrazeneca ( inst ) , grail ( inst ) , daiichi sankyo ( inst ) , hengrui therapeutics ( inst ) , guardant health ( inst ) , amgen ( inst ) ghassan k . 
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identication and monitoring the molecular mechanisms of acquired resistance to cetuximab or panitumumab in crc is important to anticipate the failure of anti - egfr antibodies and design strategies for additional treatments . several mechanisms of acquired resistance to antiegfr have been described in metastatic crc ( mcrc )  . 
 maurel et al context key objective the key objective was to evaluate the predictive and prognostic value of ras and braf mutation dynamics in plasma from patients with metastatic colorectal cancer treated with antiepidermal growth factor receptor ( anti - egfr ) therapy within two clinical trials ( posiba and pulse )  . knowledge generated baseline mutant ras / braf circulating tumor ( ct ) dna was a negative predictive marker of response to anti - egfr therapy , as well as a poor prognostic factor . 
the emergence of ctdna ras / braf mutations had limited relevance to the time to progression to anti - egfr therapy but conferred poor prognosis . relevance this work conrms the clinical utility of ctdna for ras / braf molecular testing to guide treatment decisions in patients with metastatic colorectal cancer ; however , clinical impact of ras / braf dynamics deserves further characterization . of ras , braf , or egfr mutations that drive acquired resistance in approximately 50% of patients.5 , 6 the use of circulating tumor ( ct ) dna for genotyping the tumor ( liquid biopsy ) offers clear advantages compared with repeated tumor tissue biopsies , including the minimally invasive method and no need for a tumor lesion accessible to biopsy . 
our objective was to determine the role of ctdna ras and braf mutations at the time of progression to anti - egfr therapy . methods study design and patient population the pulse and posiba studies were both prospective biomarker - design trials . 
patients were recruited into the pulse trial from november 2010 to april 2013 in 24 spanish centers and treated with infusional uorouracil , leucovorin , and oxaliplatin ( folfox ) - 6 plus panitumumab ( 6 mg / kg )  . 
patients were recruited into the posiba trial from july 2011 to may 2015 in 28 spanish centers and treated with folfox6 or uorouracil , leucovorin , and irinotecan ( folfiri ; at the investigators choice ) plus biweekly cetuximab ( 500 mg / m2 )  . in both trials , cytotoxic drugs were administered for 6 months , and anti - egfr monotherapy was continued until pd or unacceptable toxicity occurred . 
extended ras mutational analysis ( including kras / nras exons 2 , 3 , and 4 ) started in october 2013 in the pulse trial and in october 2015 in the posiba trial after protocol amendments . 
competitive allele - specic taqman pcr ( castpcr ; thermo fisher scientic , waltham , ma ) and an ultrasensitive sequencing technique ( digital polymerase chain reaction [ pcr ] ) were used to reanalyze tissue ras determination in patients with discrepancies between basal liquid biopsy ( mutation ) and formalin - xed parafn - embedded ( ffpe ) specimens ( wt )  . ctdna ras and braf mutational analysis this was an exploratory translational study with a primary objective of investigating measurement of ras and braf v600 - mutant ctdna in patients treated in the posiba and pulse trials using the idylla ctras and ctbraf mutation assay ( biocartis , jersey city , nj )  . 
plasma samples were collected basally , and serum samples were collected every 2 months in the pulse trial and every 3 months in the posiba trial , until pd was detected according to response evaluation criteria in solid tumors ( recist ) v1.1. 
two blood samples were analyzed for each patient for this study : a baseline plasma sample and a serum sample collected at the time of the last available determination . integrated ctdna purication and allele - specic quantitative pcr followed by automated data analysis was performed using the idylla ctkras and ctnras mutation assays to detect ras exon 2 , 3 , and 4 mutations and braf v600 mutations using 0.5 to 1 ml of plasma or serum per assay . 
the investigators who performed plasma genotyping were blinded to the clinical patient information . statistical analysis imaging was performed every 8 weeks in the pulse trial and every 12 weeks in the posiba trials and response was based on recist v1.1 as assessed by the investigators . progression - free survival ( pfs ) was dened as time from enrollment to disease progression ( recist criteria ) , death , or end of follow - up , whichever came rst . 
concordance was assessed using the kappa statistic and the characteristics of the diagnostic test using the sensitivity , specicity , and positive and negative predictive values by collapsing ras plus braf versus wt . 
statistical analysis was performed with spss statistics 22 ( spss , chicago , il ) and sas 9.4 software ( sas institute , cary , nc )  . results patient characteristics and concordance of baseline ras and braf mutation determination in plasma versus tissue the study ow chart is presented in figure 1 . 
kaplan - meier estimates of ( a ) progression - free survival and ( b ) overall survival , on the basis of ( c ) solid and ( d ) liquid biopsies . 
blood extraction was performed in group 1 ( between blood extraction and pd ) with a median ( p25 to p75 ) of + 7 days ( 1 to + 23 days ) and in group 2 with a median of 157 days ( 76 to 330 days ) , with the date of progression as the index date . the emergence of ras / braf mutations in ctdna was observed in 15 patients after initiation of therapy ( 11% ; appendix table a3 , online only )  . 
however , one of 11 patients ( 9% ) with acquired mutations in ctdna received anti - egfr compounds after disease progression compared with 22 of 79 ( 27.8% ) of those who remained free of mutations , potentially contributing to improved os . discussion our study indicates that ras and braf testing in baseline if not better , pfs and os ctdna results in a similar , discrimination compared with tissue testing in patients treated with rst - line chemotherapy plus anti - egfr therapy . 
 maurel et al 20116 20601 10019 10129 10140 10039 10027 10149 23209 10090 10153 20804 10131 10082 20401 10004 10159 20602 10006 10182 20306 10124 10115 21119 10122 22008 10167 22901 20611 10174 10126 10189 10147 22001 mutational status ( os bar ) : negativitzation no change overall response rate ( pfs bar ) : metastasectomy end of treatment liquid biopsy 1 , 000 1 , 200 1 , 400 time ( days ) fig 4 . 
progression - free survival ( pfs ) and overall survival ( os ) in patients with mutant ras and braf on basal liquid biopsy ( n = 34 )  . 
in a recent study with 43 patients , oncobeam demonstrated 72.1% concordance with tissue results , whereas idylla demonstrated 46.5% concordance with kras tissue results.15 finally , we observed that the subgroup of patients who had ras or braf mutations on tissue and wt on ctdna was enriched with patients with low tumor burden ( ldh , 1 uln )  . 
our results analyzing plasma samples at baseline and serum samples at progression differ with the analysis from the aspecct third - line phase iii panitumumab study , which showed that patients with emergent ras mutations at progression had similar pfs and os versus patients whose status remained wt at progression.19 in our study , patients with ras and braf with acquired mutations that were initially 2 wt showed signicantly poorer survival than those patients who remained wt at progression ; also , patients with disappearance of mutations showed better os . 
we have to note that patients in our study had been treated in rst - line therapy ( compared with third line in the aspecct trial ) and , therefore , second - line egfr therapies in truly sensitive patients ( those with liquid biopsies that remain wt ) would affect survival . 
moreover , we could not rule out that at pd , in patients with a poor prognosis ( identied by a high level of ldh at disease progression ) , we would have more chance to detect acquired mutations in ctdna . 
our study addresses most of the potential limitations from previous analyses , such as low number of patients , treatment heterogeneity ( including type of treatment and mixed rst , second , and third lines ) , and lack of a control group ( analysis of ras and braf in samples of patients without progression or before pd )  . 
 clinical impact of circulating tumor ras and braf mutations with rst - line therapy with currently accepted schedules of chemotherapy ( folfox and folfiri ) and approved antiegfr compounds ( cetuximab and panitumumab ) to establish differences between both groups ( 14% and 8% , respectively ; p = .47 ) , and global mutation acquisition was observed in only 11% of patients . 
this suggests that other mechanisms beyond ras and braf acquired mutations will probably play an important role , not only in the subset of patients without acquired ras and braf mutations , but also in the group of patients with acquired ras and braf mutations . 
n engl j med 360 : 1408 - 1417 , 2009 van cutsem e , lenz hj , k ohne ch , et al : fluorouracil , leucovorin , and irinotecan plus cetuximab treatment and ras mutations in colorectal cancer . 
j clin oncol 33 : 692 - 700 , 2015 douillard jy , siena s , cassidy j , et al : randomized , phase iii trial of panitumumab with infusional uorouracil , leucovorin , and oxaliplatin ( folfox4 ) versus folfox4 alone as rst - line treatment in patients with previously untreated metastatic colorectal cancer : the prime study . 
j clin oncol 28 : 4697 - 4705 , 2010 douillard jy , oliner ks , siena s , et al : panitumumab - folfox4 treatment and ras mutations in colorectal cancer . 
montagut c , dalmases a , bellosillo b , et al : identication of a mutation in the extracellular domain of the epidermal growth factor receptor conferring cetuximab resistance in colorectal cancer . 
montagut c , argil es g , ciardiello f , et al : efcacy of sym004 in patients with metastatic colorectal cancer with acquired resistance to anti - egfr therapy and molecularly selected by circulating tumor dna analyses : a phase 2 randomized clinical trial . 
jama oncol 4 : e175245 , 2018 pietrantonio f , vernieri c , siravegna g , et al : heterogeneity of acquired resistance to anti - egfr monoclonal antibodies in patients with metastatic colorectal cancer . 
clin cancer res 23 : 2414 - 2422 , 2017 diaz la jr , williams rt , wu j , et al : the molecular evolution of acquired resistance to targeted egfr blockade in colorectal cancers . 
siena s , sartore - bianchi a , garcia - carbonero r , et al : dynamic molecular analysis and clinical correlates of tumor evolution within a phase ii trial of panitumumab - based therapy in metastatic colorectal cancer . 
normanno n , esposito abate r , lambiase m , et al : ras testing of liquid biopsy correlates with the outcome of metastatic colorectal cancer patients treated with rst - line folfiri plus cetuximab in the capri - goim trial . 
grasselli j , elez e , carat `u g , et al : concordance of bloodand tumor - based detection of ras mutations to guide anti - egfr therapy in metastatic colorectal cancer . 
ann oncol 29 : 1211 - 1219 , 2018 jacobs b , claes b , pomella v , et al : analytical and clinical validation of the idylla ( cid : 1 ) ctkras and ctnras - braf liquid biopsy tests identies mcrc patient groups with high and low ctdna shedding . 
ras and braf mutational status in baseline plasma sample and secondary extraction serum sample : characteristics of patients with ctdna ras / braf mutation in baseline and second liquid biopsy plasma liquid biopsy ( basal ) serum liquid biopsy ( secondary ) , no . ras mutated braf mutated patient primary side basal liquid biopsy site of metastasis response surgery of second liquid metastasis biopsy maurel et al mutated braf mutated 2 wt total rectum kras ( a146p / t / v ) plus nras ( g13r / v ) liver left colon nras ( g13r / v ) liver , lung sigmoid kras ( g12d ) liver , lung sigmoid nras ( g13r / v ) liver , peritoneum sigmoid kras ( g12v ) node right side kras ( a146p / t / v ) local relapse sigmoid kras ( k117n ) liver , lung left colon kras ( g12v ) peritoneum rectum kras ( g12r ) liver , lung rectum kras ( k117n ) liver , lung right side braf ( v600e / d ) liver , peritoneum rectum nras ( q61h ) rectum braf ( v600e / d ) right side braf ( v600e / d ) kras ( g12d ) liver liver liver liver rectum kras ( a146p / t / v ) liver , node , suprarenal  . 
ras and braf mutational status in baseline plasma sample and secondary extraction serum sample : characteristics of patients with ctdna ras / braf mutation in baseline and second liquid biopsy ( continued ) serum liquid biopsy ( secondary ) , no . 22008 10122 10115 10006 20602 10004 10082 10153 22001 10189 10174 21119 10131 10090 rectum nras ( g61k ) liver , lung sigmoid nras ( g61r ) liver , lung right side kras ( a59t / e / g ) liver rectum kras ( a146p / t / v ) liver , lung left colon nras ( g61h ) liver , node , peritoneum  . 
 o palbociclib in patients with pancreatic and biliary cancer with cdkn2a alterations : results from the targeted agent and proling utilization registry study tareq al baghdadi , md1 ; susan halabi , phd2 ; elizabeth garrett - mayer , phd3 ; pam k . 
schilsky , md3 purpose the targeted agent and proling utilization registry ( tapur ) study identies signals of antitumor activity of commercially available targeted agents in patients with advanced cancers that harbor genomic alterations known as drug targets . 
in this article , data from two cohorts of patients with pancreatic and biliary cancers with cdkn2a loss or mutation treated with palbociclib are reported . methods eligible patients age 12 years and older with advanced measurable or evaluable solid tumors are provided treatment according to protocol - specied genomic matching rules . 
secondary end points include safety , progression - free survival ( pfs ) , and overall survival ( os )  . results between july 2016 and november 2017 , 12 and 10 patients with pancreatic and biliary cancer , respectively , with cdkn2a loss or mutation were treated with palbociclib . 
despite recent advances , outcomes remain poor with a median overall survival ( os ) of less than 12 months in stage iv biliary and pancreatic cancers , 1 - 4 and new therapies are urgently needed . cyclin - dependent kinase ( cdk ) inhibitor 2a ( cdkn2a ) encodes p16ink4a , which plays an important role in cell - cycle regulation through inhibition of cdk4 / 6 . cdkn2a loss or mutation is found in a wide array of malignancies and may lead to increased cdk activity.5 in a report of the mutational landscape of advanced pancreatic cancer , 46.5% of tumors harbored alterations in cdkn2a.6 palbociclib is an orally available selective cdk inhibitor approved for the treatment of hormone receptorpositive , human epidermal growth factor receptor 2 ( her2 ) negative breast cancer in combination with endocrine therapy . the targeted agent and proling utilization registry ( tapur ) study is a prospective , phase ii , pragmatic basket trial designed to identify signals of antitumor activity of commercially available targeted agents in patients with advanced cancers that harbor genomic alterations known to be drug targets . 
this study examined whether patients with advanced biliary and pancreatic cancer with cdkn2a loss or mutation would be responsive to palbociclib , an oral cyclin - dependent kinase inhibitor . knowledge generated the results demonstrated that palbociclib monotherapy has no meaningful clinical activity in patients with cdkn2a mutated or deleted advanced pancreatic or biliary adenocarcinoma . relevance off - label prescribing of palbociclib for the treatment of patients with pancreatic and biliary tract cancers with cdkn2a loss or mutation is not recommended . 
these patients should be offered participation in clinical trials of new treatment approaches . methods trial design the rationale and study design have been reported previously in detail.7 patients with advanced cancer and no standard treatment options are eligible if they have a tumor that harbors a genomic alteration known to be a target of or to predict sensitivity to one of the available study drugs . the primary study end point is antitumor activity , dened as objective response ( or ) at 8 weeks or later or stable disease ( sd ) at 16 weeks or later from the time of enrollment . secondary end points include progression - free survival ( pfs ) , os , and toxicity . 
patients are matched to one of according to prespecied protocol matching rules on the basis of genomic testing performed by laboratories selected by clinical sites that have certication under the clinical laboratory improvement amendments and accreditation from the college of american pathologists . 
treating physicians may choose to consult with the tapur molecular tumor board for appropriate targeted treatment options where none or multiple treatment matches surface within the tapur matching rules or if the treating physician would like to propose a treatment match outside the matching rules . 
radiographic assessment and clinical evaluation for response evaluation are performed at 8 and 16 weeks after initiation of treatment ; then every 12 weeks while the patient remains in the study ; and then at the end of study treatment , where possible . 
patients are placed in multiple parallel cohorts dened by study drug , genomic alteration , and tumor type . each cohort has the same optimal simon two - stage design , with a total possible cohort size of 28 patients . 
the design requires 10 patients to be enrolled in a cohort in stage i and if fewer than two patients have or or sd of at least 16 weeks duration , the cohort is permanently closed . 
if at least seven patients in the total cohort have a response of at least 16 weeks duration , the null hypothesis is rejected , and it is concluded that a signal of activity has been identied . patients eligible patients are required to meet both protocoland drugspecic inclusion and exclusion criteria . 
protocol - specic eligibility criteria include advanced measurable or evaluable solid tumors per recist version 1.1 ; eastern cooperative oncology group ( ecog ) performance status ( ps ) of 0 , 1 , or 2 ; and a protocol - specied genomic target identied by a test performed in a laboratory that has clinical laboratory improvement amendments certication and college of american pathologists accreditation . 
 palbociclib in pancreatic / biliary cancer with cdkn2a alterations addition , to match to palbociclib , patients must have a cancer type other than breast and not have received food or drugs within 7 days before the start of study treatment that are known to be cyp3a4 inhibitors or inducers . 
detailed inclusion and exclusion criteria for tapur have been previously reported.7 patients treated with palbociclib received standard doses ( 125 mg orally daily for 21 days followed by 7 days off treatment to complete a 28 - day cycle ) until disease progression . 
all patients were tested for alterations using next - generation sequencing ( ngs ) platforms , with more than half the patients determined to have cdkn2a loss ( table 1 )  . patients in both cohorts continued treatment with palbociclib until disease progression , and no patients withdrew from the study . trial oversight the tapur study protocol was reviewed and approved by a central institutional review board and , in some cases , by the local institutional review board at participating sites . patients provide written consent before any screening activities or data collection . 
the tapur study was designed by asco staff with input from asco volunteer members and the participating pharmaceutical companies . the tapur data and safety monitoring board ( dsmb ) is an independent board appointed by asco and meets biannually to monitor the study and review the safety and efcacy ndings . 
in the case of the cohorts reported herein , the dsmb reviewed the safety and efcacy data and determined that both cohorts should permanently close at the end of stage i enrollment and that the ndings be released . study end points the primary end point is or , dened as complete or partial response at or before 16 weeks , or sd at 16 weeks or later as reported per recist version 1.1. 
 al baghdadi et al results patients with pancreatic cancer twelve patients with pancreatic cancer and cdkn2a loss or mutation treated with palbociclib were enrolled in the study across seven sites from july 25 , 2016 , to april 28 , 2017 . 
the median age was 62 years ( range , 52 to 70 years ) ; 67% of patients were male ; and 10 patients were white , one black , and one other . 
other common genomic alterations noted in this cohort were mutations in braf , fgfr1 , frs2 , kras , and tp53 , with kras mutations being the most commonly reported in 10 of 12 patients . two patients who were enrolled and received treatment were subsequently found to be ineligible because they had not met the eligibility requirement for a hemoglobin level of 9.0 g / dl or greater at the time of enrollment . 
of the 10 eligible patients , nine experienced progression at or before 8 weeks ; the remaining patient had tumor progression at 16 weeks . all patients were included in the analysis for safety , pfs , and os . 
no other grade 3 or higher adverse event or serious adverse event was observed as at least possibly related to palbociclib . patients with biliary cancer ten patients with biliary cancer with cdkn2a loss or mutation treated with palbociclib were enrolled in the study across six sites from august 9 , 2016 , to november 11 , 2017 . 
other genomic alterations noted in this cohort included arid1a , atm , braf , fgfr2 , fh , kras , nras , pik3ca , and vhl . all 10 patients experienced progression at or before 10 weeks . 
four patients experienced grade 3 or 4 adverse events of thrombocytopenia at least possibly related to palbociclib . discussion this phase ii study in patients with advanced pancreatic or biliary cancers with cdkn2a loss or mutation treated with single - agent palbociclib demonstrated no clinical activity . the toxicity is similar to previous reports of monotherapy with palbociclib . cdkn2a is a tumor suppressor gene frequently altered by mutations , deletions , and epigenetic silencing . 
of patients loss mutation loss cdkn2a / 2b homozygous loss p16ink4a a4_p11del , p16ink4a l16fs * 9 , loss exons 2 - 3 splice site 151 - 2a.g p16ink4a r58 * and p14arf p72l p16ink4a a36fs * 17 , p16ink4a n71fs * 49 and p14arf q85fs * 50 + splice site 151 - 1g.c truncation exon 2 foundationone mi - oncoseq foundationone foundationone foundationone foundationone foundationone foundationone abbreviations : mi - oncoseq , michigan oncology sequencing project ; ngs , next - generation sequencing . cdkn2a mutations / deletions occur frequently in pancreatic adenocarcinoma.11 moreover , alterations that abrogate the rb / p16 tumor suppressor pathway are seen in virtually all pancreatic carcinomas.12 cdkn2a mutations occur in a minority of cholangiocarcinomas and are associated with a poor prognosis.13 , 14 prior studies of multiple rb - positive tumors have shown that most are sensitive to some degree to cdk4 / 6 inhibition.15 - 18 preclinical studies assessing the impact of cdk4 / 6 inhibition on pancreatic cancer cell lines and xenograft models showed conicting data . 
for example , one study showed that palbociclib inhibited the growth of pancreatic cancer cell lines but resulted in upregulation of the expression of genes that promote invasion and metastasis.19 another showed that established pancreatic cell lines displayed a relatively weak response to palbociclib , but palbociclib had potent activity in patient - derived xenografts.20 palbociclib is approved for the treatment of patients with advanced hormone receptorpositive , her2 - negative breast cancer in combination with an aromatase inhibitor or fulvestrant.21 , 22 palbociclib showed promising activity in patients with liposarcoma23 and cdkn2a - mutated nonsmallcell lung cancer.24 however , palbociclib was not effective in lung cancer25 or unselected patients with squamous cell urothelial cancer.26 prior studies have suggested several mechanisms of resistance to cdk4 / 6 inhibitors in human cancer cell lines and xenograft models , including cdk4 amplication , rb loss , and cyclin e1 amplication.27 - 31 the potential for prior exposure to systemic chemotherapy to induce resistance to palbociclib through these or other mechanisms has not been explored but might have contributed to the lack of efcacy of palbociclib in this trial . 
it is conceivable , therefore , that the use of palbociclib alone or in combination earlier in the treatment course could be benecial . the association of cdkn2a mutations / deletions with clinical activity of cdk4 / 6 inhibitors is undetermined . 
in patients with hormone receptorpositive , her2 - negative breast cancer , cdkn2a mutations do not predict activity of either palbociclib or ribociclib.32 , 33 a report revealed that cdkn2a mutant cancers show only intermediate sensitivity to cdk4 / 6 inhibition with abemaciclib , whereas genetic events that activate d - type cyclins were associated with high sensitivity.30 the effects of combining other targeted agents with palbociclib in pancreatic adenocarcinoma cell lines have been explored . 
the addition of a mek inhibitor31 and a mammalian target of rapamycin inhibitor30 , 34 was synergistic . the latter may relate to metabolic reprogramming of pancreatic cancer cells by cdk4 / 6 inhibition , which results in increased oxidative phosphorylation , increased consumption of glucose and glutamine , and activation of mammalian target of rapamycin pathway.34 these and other novel combinations hopefully will allow successful treatment of pancreatic adenocarcinoma and other malignancies on the basis of a sound understanding of mechanisms that underlie cancer cell resistance . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . tareq al baghdadi stock and other ownership interests : array biopharma , astrazeneca , biogin , bristol - myers squibb , merck , portola pharmaceuticals , spectrum pharmaceuticals , tracon pharma , celgene , seattle genetics , sunesis pharmaceuticals honoraria : cardinal health , medscape consulting or advisory role : celgene , bristol - myers squibb , heron therapeutics travel , accommodations , expenses : cardinal health , celgene , bristolmyers squibb , heron therapeutics susan halabi consulting or advisory role : eisai , ferring pharmaceuticals vaibhav sahai consulting or advisory role : celgene , halozyme , newlink genetics , ipsen , incyte research funding : celgene ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) , clovis oncology ( inst ) , debiopharm group ( inst ) , fibrogen ( inst ) , halozyme ( inst ) , medimmune ( inst ) , rafael pharmaceuticals ( inst ) , ipsen ( inst ) ricardo h . 
alvarez employment : cancer treatment centers of america leadership : cancer treatment centers of america consulting or advisory role : eisai , puma biotechnology , r - pharma , pzer speakers bureau : eisai , pzer other relationship : eisai , puma biotechnology , pzer edward s . 
kim honoraria : astrazeneca , boehringer ingelheim , pzer , merck , takeda pharmaceuticals , roche , genentech consulting or advisory role : astrazeneca , boehringer ingelheim , pzer , merck , takeda pharmaceuticals , roche , genentech research funding : boehringer ingelheim , merck , ignyta , genentech , roche travel , accommodations , expenses : astrazeneca , boehringer ingelheim , takeda pharmaceuticals , genentech , roche , pzer , merck kathleen j . 
schilsky research funding : astrazeneca ( inst ) , bayer ag ( inst ) , bristol - myers squibb ( inst ) , genentech ( inst ) , roche ( inst ) , eli lilly ( inst ) , merck ( inst ) , pzer ( inst ) , boehringer ingelheim ( inst ) , varian ( inst ) no other potential conicts of interest were reported . references conroy t , desseigne f , ychou m , et al : folfirinox versus gemcitabine for metastatic pancreatic cancer . 
n engl j med 364 : 1817 - 1825 , 2011 von hoff d.d. , ervin t , arena fp , et al : increased survival in pancreatic cancer with nab - paclitaxel plus gemcitabine . 
n engl j med 369 : 1691 - 1703 , 2013 valle j , wasan h , palmer dh , et al : cisplatin plus gemcitabine versus gemcitabine for biliary tract cancer . 
n engl j med 362 : 1273 - 1281 , 2010 sahai v , catalano pj , zalupski mm , et al : nab - paclitaxel and gemcitabine as rst - line treatment of advanced or metastatic cholangiocarcinoma : a phase 2 clinical trial . 
witkiewicz ak , knudsen ke , dicker ap , et al : the meaning of p16 ( ink4a ) expression in tumors : functional signicance , clinical associations and future developments . 
cell cycle 10 : 2497 - 2503 , 2011 aguirre aj , nowak ja , camarda nd , et al : real - time genomic characterization of advanced pancreatic cancer to enable precision medicine . 
fry dw , harvey pj , keller pr , et al : specic inhibition of cyclin - dependent kinase 4 / 6 by pd 0332991 and associated antitumor activity in human tumor 16 . 
finn rs , dering j , conklin d , et al : pd 0332991 , a selective cyclin d kinase 4 / 6 inhibitor , preferentially inhibits proliferation of luminal estrogen receptor - positive human breast cancer cell lines in vitro . 
baughn lb , di liberto m , wu k , et al : a novel orally active small molecule potently induces g1 arrest in primary myeloma cells and prevents tumor growth by specic inhibition of cyclin - dependent kinase 4 / 6 . 
young rj , waldeck k , martin c , et al : loss of cdkn2a expression is a frequent event in primary invasive melanoma and correlates with sensitivity to the cdk4 / 6 inhibitor pd0332991 in melanoma cell lines . 
cristofanilli m , turner nc , bondarenko i , et al : fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment of hormone - receptor - positive , her2negative metastatic breast cancer that progressed on previous endocrine therapy ( paloma - 3 ) : final analysis of the multicentre , double - blind , phase 3 randomised controlled trial . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
gopalan pk , pinder mc , chiappori a , et al : a phase ii clinical trial of the cdk 4 / 6 inhibitor palbociclib ( pd 0332991 ) in previously treated , advanced non - small cell lung cancer ( nsclc ) patients with inactivated cdkn2a . 
edelman mj , redman mw , albain ks , et al : a phase ii study of palbociclib ( p ) for previously treated cell cycle gene alteration positive patients ( pts ) with stage iv squamous cell lung cancer ( scc ) : lung - map sub - study swog s1400c . 
rose tl , chism dd , alva as , et al : phase ii trial of palbociclib in patients with metastatic urothelial cancer after failure of rst - line chemotherapy . 
herrera abreu mt , asghar u , elliot r , et al : pi3 kinase / mtor inhibition increases sensitivity of er positive breast cancers to cdk4 / 6 inhibition by blocking cell cycle re - entry driven by cyclind1 and inducing apoptosis . 
gong x , litcheld lm , webster y , et al : genomic aberrations that activate d - type cyclins are associated with enhanced sensitivity to the cdk4 and cdk6 31 . 
finn rs , crown jp , lang i , et al : the cyclin - dependent kinase 4 / 6 inhibitor palbociclib in combination with letrozole versus letrozole alone as rst - line treatment of oestrogen receptor - positive , her2 - negative , advanced breast cancer ( paloma - 1 / trio - 18 ) : a randomised phase 2 study . 
andre f , stemmer sm , campone m , et al : ribociclib + letrozole for rst - line treatment of hormone receptor - positive ( hr + ) , human epidermal growth factor receptor 2 - negative ( her2 - ) advanced breast cancer ( abc ) : efcacy by baseline tumor markers . 
 genomic and proteomic alterations in desmoplastic small round bluecell tumors purpose desmoplastic small round blue - cell tumors ( dsrcts ) are sarcomas that contain the t ( 11 ; 22 ) ( p13 ; q12 ) translocation ews - wt1 fusion protebecause this is a rare tumor type , prospective clinical trials in dsrct are challenging . 
patients are treated in a manner similar to those with ewing sarcoma ; however , differences in prognosis and clinical presentation suggest fundamental differences in biology and potentially different therapeutic implications . 
 methods thirty - five dsrct tumors were assessed using next - generation sequencing , protein expression ( immunohistochemistry ) , and gene amplification ( chromogenic in situ hybridization or fluorescence in situ hybridization )  . 
independent analysis by rna sequencing confirmed higher ar expression from an independent data set of ews - wt1 fusionpositive dsrcts compared with ewing sarcoma and a pan - cancer analysis . 
dsrcts had somatic mutations that were identified in tp53 and foxo3 , averaged five mutations per megabase , and no programmed death - ligand 1 expression was detected in any dsrct samples . 
2018 by american society of clinical oncology ajaz bulbul john paul shen joanne xiu pablo tamayo hatim husain author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : hatim husain , md , university of california san diego , 3855 health sciences #3011 , la jolla , ca 92093 ; e - mail : hhusain@ucsd.edu. introduction desmoplastic small round blue - cell tumors ( dsrcts ) originate from a cell with multilineage potential and are defined by a molecular hallmark with ews - wt1 reciprocal translocation.1 dsrcts are rare , highly aggressive mesenchymal tumors , with only 200 to 450 affected patients with the disease described to date.1 , 2 ewing sarcoma and dsrcts are treated in a similar manner in the clinic ; however , dsrcts have been represented in limited numbers in sarcoma studies . 
the clinical presentations of these diseases are different , with important comparisons being the site of disease presentation and poor prognosis in dsrct groups . despite aggressive therapy , median survival ranges from 17 to 25 months , 2 , 3 and the 5 - year survival rate remains around 15%3 with higher survival reported among those who underwent removal of at least 90% of the tumor with an absence of extraperitoneal metastasis.4 almost all of these tumors contain the t ( 11 ; 22 ) ( p13 ; q12 ) translocation that fuses ews with wt1 leading to production of a chimeric protein with transcriptional regulatory activity . 
 and pelvic cavity of young adult men in 88% to 97% of cases , 2 , 5 whereas ewing sarcoma commonly occurs in the axial skeleton.7 despite similar histologic morphology , differences in disease presentation and prognosis likely reflect the impact of different biologic factors , including differences in the transcriptional effects of the ews - wt1 fusion relative to the ews - fli1 fusion observed in ewing sarcoma . although there is no standard clinical management strategy for dsrct , treatment usually includes neoadjuvant high - dose cyclophosphamide , doxorubicin , and vincristine , alternating with ifosfamide and etoposide chemotherapy combined with aggressively attempted r0 resection.4 , 8 , 9 recent accelerated us food and drug administration ( fda ) approval in october 2016 of the compound olaratumab , a platelet - derived growth factor receptor a inhibitor , was based on a highly significant improvement in overall survival of 26.5 months in soft tissue sarcomas of histologic subtypes for which an anthracycline containing regimen may be appropriate . 
however , only one patient in the phase ii olaratumab study had round blue - cell sarcoma , and that patient was negative for the ews translocation.10 patients with dsrcts are poorly represented in clinical trials as a result of the rare nature of the disease . 
a list of ongoing clinical trials in this disease is provided in the data supplement . the aim of the current study was to understand the molecular characteristics of dsrcts by analyzing 35 patients with molecularly and immunohistochemically profiled tumors and to compare these with ewing sarcoma to explore therapeutic options and potential oncogenic vulnerabilities for this extremely rare and aggressive cancer type . 
dna from formalin fixed , paraffin - embedded samples was sequenced using the nextseq ( 592 genes selected on the basis of the cosmic database ; agilent sure select xt ; illumina , san diego , ca ) and miseq ( 47 genes ; truseq ) , to evaluate mutation and gene amplification . 
the full list of markers surveyed is available.11 twenty - four tumors were sequenced with the 45 - gene panel , and 11 tumors were sequenced with the 592 - gene panel . 
additional data for ar and epidermal growth factor receptor ( egfr ) ihc in other tumors , including prostate cancer , lung cancer , breast cancer , kidney cancer , endometrial cancer , and glioblastoma , were obtained from a larger cohort of 127 , 000 pan - cancer tumor samples analyzed . we used 2 tests for comparison , and statistical significance was determined as p < .05. 
 ( a ) enrichment scores ( single - sample gene set enrichment analysis ) of selected transcriptional signatures across alveolar rhabdomyosarcoma , desmoplastic small round blue cell tumors , ewing sarcoma , and synovial sarcoma . 
desmoplastic small round blue - cell tumor ( dsrct ) sarcomas are clearly overenriched in androgen receptor ( ar ) , epidermal growth factor receptor ( egfr ) , and ews - wt1 ( kts positive / negative ) signatures compared with those of other sarcomas . 
arms , alveolar rhabdomyosarcoma ; es , ewing sarcoma ; ss , synovial sarcoma . the degree to which the genes in a particular gene set are coordinately upregulated or downregulated within each sample . 
in this manner , ssgsea projects a single sample gene expression profile from the space of single genes onto the space of gene sets . the signature for ar is the hallmark_ androgen_response gene set from the molecular signatures database hallmark subcollection.13 the egfr signature corresponds to the egfr_up.v1_up / dn gene sets from the molecular signatures database subcollection c6.14 the ews - wt1 ( kts positive / negative ) signatures were generated from the geo data set gse53301.15 the ews - fli1 signature was made from the 20 genes listed in figure 1 from mendiola et al.16 transcriptional data sets the multiple sarcoma data set shown in figure 1a is a subset of the data set from filion et al.17 sarcoma samples in figure 1b are the dsrct subset from filion et al.17 prostate samples , shown in figure 1b , consisted of 22 primary prostate cancer samples from the geo data set gse32269.18 endometrial samples are 30 samples from the endometrial cancer data set from raeder et al.19 glioblastoma multiforme samples consisted of a subset of 30 samples from the glioblastoma multiforme data set from verhaak et al.20 results demographic data from the 35 patients whose tumors underwent clinical molecular testing are provided in the data supplement . 
 ( a ) thirty - five desmoplastic small round blue - cell tumors ( dsrcts ) went through molecular profiling using a commercial , multiplatform profiling service ( caris life sciences )  . 
specific tests performed included sequencing ( next - generation sequencing [ seq ] ) , protein expression ( immunohistochemistry [ ihc ] ) , and gene amplification ( chromogenic in situ hybridization or fluorescence in situ hybridization [ ish ] )  . 
 patients with ewing sarcoma had lung and bone involvement , which is consistent with the known distribution pattern of these tumors.21 in the 35 dsrcts , increased expression of top2a was observed in 63% of cases , topo1 in 63% , pten in 62% , ar in 59% , and egfr in 42% of tumors . 
increased expression of tubb3 was observed in 56% of tumors , mgmt in 55% , ts in 52% , rrm1 in 43% , and ercc1 in 24% ( fig 2a )  . 
comparing dsrcts with ewing sarcoma tumors , we found that both ar ( 59% v 3% ; p = 1.7e10 ) and tubb3 ( 56% v 29% ; p = .03 ) were expressed in significantly more dsrcts ( fig 2b )  . 
a full list of all of the patients with ihc staining is provided in the data supplement , which includes a description of staining thresholds . given that both the ar and egfr pathways can be effectively targeted with fda - approved drugs , we sought to further evaluate the activity of these pathways in dsrcts . 
we obtained gene expression profiles for 28 dsrcts as well as profiles for ewing sarcoma , alveolar rhabdomyosarcomas , and synovial sarcoma for comparison with other primitive sarcomas.17 performing ssgsea , we found that the majority of dsrcts was enriched for the ar signature , which indicated that these tumors coordinately upregulated genes that are known to be highly expressed when the ar pathway is activated ( fig 1a )  . 
as expected , ewing sarcoma tumors were enriched for the ews - fli1 signature , and dsrcts were enriched for the ews - wt1 signature , which is consistent with the translocation event pathognomonic for each tumor . to evaluate the significance of ar pathway activation in dsrcts , we made comparisons with tumors that are known to be driven by the ar pathway . 
compared with 59% ar expression in dsrct , ihc results indicated that ar expression was most frequent in prostate cancer ( 94% [ n = 1 , 340 tumors ] ) ; however , dsrct was greater than any other tumor type , including breast cancer ( 50% [ n = 1 , 962 tumors ] ) , kidney cancer ( 30% [ n = 40 tumors ] ) , and the pan - cancer analysis , which demonstrated < 30% expression ( n = 127 , 000 )  . 
a pan - cancer analysis of egfr expression demonstrated a percentage of expression ( 53% [ n > 20 , 000 ] ) that was similar to the 42% observed in dsrct . 
furthermore , tubb3 expression ( 51% [ n = 66 , 000 ] ) and top2a ( 69% [ n = 77 , 000 ] ) was similar to that observed in dsrct . pd - l1 expression ( sp142 ) was not detected in tumors tested ( zero of four ) , whereas programmed death 1 ( pd - 1 ) staining on tumor infiltrating lymphocytes ( tils ) was found in 25% of tumors tested ( two of eight )  . 
pd - l1 expression on tumor cells in ewing sarcoma was absent ( zero of 10 ) , and pd - 1 expression on tils was observed in 32% ( six of 19 ) of ewing sarcoma tumors ( fig 2 )  . 
tumor mutational load was calculated in 11 ewing sarcoma tumors , and mean tumor mutational load was five mutations per megabase ( range , three to eight mutations )  . next - generation sequencing revealed a synonymous tp53 g245g mutation and a foxo3 mutation ( l382fs ) in dscrt , whereas six tp53 mutations ( 13% ) , two apc mutations ( l1129s and i1307k ) , one brca1 ( c.301 + 1g > a ) , and one ctnnb1 ( t41a ) mutation were identified in ewing sarcoma . 
there was no copy number amplification identified in dsrct samples for cmet , her2 ( human epidermal growth factor receptor 2 ) , and egfr with in situ hybridization ( data supplement )  . discussion our understanding of the biology of dsrcts and their distinction from other sarcomas is evolving . 
 apart from the canonical ews - wt1 fusion , some major differences between dsrct and ewing sarcoma reflect those between ar and egfr expression . significantly higher ar expression in dsrcts compared with ewing sarcoma tumors suggest the possibility of a mechanistic link between ews - wt1 activation and androgen receptor expression . 
various ews - wt1 proteins regulate the promoter activity of egr - 1 , a zinc finger transcription factor that contributes to ar pathway activation.25 , 26 egr - 1 knockdown by small interfering rna inhibited activity of the ar signaling pathway.27 evidence for ar activation in dsrcts was observed by ihc as well as the coordinate regulation of the ar - responsive transcriptome . 
the degree of ar enrichment in dsrcts was higher than that of many other tumors , and additional work is needed to understand the clinical sensitivity of these tumors to ar inhibition . fda - approved novel ar inhibitors , including enzalutamide , and cyp17a1 inhibitors , including abiraterone , will need to be explored and provide a potential opportunity for continued drug expansion in this space . 
the three patients who had benefit from complete androgen blockade ( cab ) had normal testosterone levels before cab , whereas the three who did not experience a response had baseline castrate levels of testosterone.28 in vitro studies that evaluated the functional status of ar using western blot analysis and the stimulation of growth by dihydrotestosterone in mtt calorimetric assays in 27 patient tumors suggested that ar in dsrcts is functional , and inhibition of basal and testosterone - stimulated growth by flutamide could be achieved.28 a phase ib study in prostate cancer has combined treatment with enzalutamide and docetaxel chemotherapy and has resulted in a 50% decline from baseline in prostate - specific antigen in 19 of 20 patients , and a phase ii study is ongoing in prostate cancer ( clinicaltrials.gov identifier : nct02685267 ) .29 given the poor outcomes found with conventional therapy , the role of combinatorial therapy with ar inhibitors alone or in combination with chemotherapy in dsrtc deserves additional clinical investigation . tumor mutational load may affect response rates to immunotherapy in melanoma and nonsmallcell lung cancers.30 unfortunately , single - agent antipd - 1 antibodies , to date , have had limited efficacy across sarcomas , and an ongoing phase ii study ( sarc028 ) is evaluating the role of pembrolizumab across various sarcoma histologies ( clinicaltrials.gov identifier : nct02301039 ) .31 none of the patients in our cohort had identifiable tumoral pd - l1 expression by sp142 antibody testing , and the significance of pd - 1 positive tils is unclear at this time . in conclusion , there are distinguishing molecular characteristics between dsrcts and ewing sarcoma . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ajaz bulbul consulting or advisory role : pfizer , astrazeneca travel , accommodations , expenses : pfizer , astrazeneca joanne xiu employment : caris life sciences pablo tamayo no relationship to disclose hatim husain consulting or advisory role : astrazeneca , abbvie , foundation medicine speakers ' bureau : astrazeneca , merck , bristol - myers squibb research funding : pfizer ( inst ) travel , accommodations , expenses : astrazeneca , merck , bristol - myers squibb , foundation medicine , abbvie affiliations ajaz bulbul , john paul shen , pablo tamayo , and hatim husain , university of california san diego , la jolla , ca ; and joanne xiu , caris life sciences , phoenix , az . funded by university of california san diego moores cancer center institutional funds and national institutes of health grants no . 
honor c , amroun k , vilcot l , et al : abdominal desmoplastic small round cell tumor : multimodal treatment combining chemotherapy , surgery , and radiotherapy is the best option . 
tap wd , jones rl , van tine ba , et al : olaratumab and doxorubicin versus doxorubicin alone for treatment of soft - tissue sarcoma : an open - label phase 1b and randomised phase 2 trial . 
creighton cj , hilger am , murthy s , et al : activation of mitogen - activated protein kinase in estrogen receptor alpha - positive breast cancer cells in vitro induces an in vivo molecular phenotype of estrogen receptor alpha - negative human breast tumors . 
mendiola m , carrillo j , garca e , et al : the orphan nuclear receptor dax1 is up - regulated by the ews / fli1 oncoprotein and is highly expressed in ewing tumors . 
raeder mb , birkeland e , trovik j , et al : integrated genomic analysis of the 8q24 amplification in endometrial cancers identifies atad2 as essential to myc - dependent cancers . 
verhaak rg , hoadley ka , purdom e , et al : integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
gerald wl , rosai j , ladanyi m : characterization of the genomic breakpoint and chimeric transcripts in the ews - wt1 gene fusion of desmoplastic small round cell tumor . 
sukhatme vp , cao xm , chang lc , et al : a zinc finger - encoding gene coregulated with c - fos during growth and differentiation , and after cellular depolarization . 
fine rl , shah ss , moulton ta , et al : androgen and c - kit receptors in desmoplastic small round cell tumors resistant to chemotherapy : novel targets for therapy . 
morris mj , rathkopf de , novotny w , et al : phase ib study of enzalutamide in combination with docetaxel in men with metastatic castration - resistant prostate cancer . 
burgess ma , crowley j , reinke dk , et al : sarc 028 : a phase ii study of the anti - pd1 antibody pembrolizumab ( p ) in patients ( pts ) with advanced sarcomas . 
 eleven month progressionfree survival on vemurafenib monotherapy in a patient with recurrent and metastatic braf v600emutated glioblastoma who grade 4 introduction glioblastoma multiforme ( gbm ) accounts for 3% to 4% of all cancer - related deaths , despite having an average incidence rate of 3.19 / 100 , 000 population.1 , 2 prognosis for gbm remains poor , with standard - of - care therapy providing only a 16to 20 - month median overall survival.3 , 4 braf kinase inhibitors have transformed melanoma treatment and have successfully been used in other tumor types containing the braf v600e mutation.5 - 8 there are several reports of improved survival with the use of braf - directed therapy in braf - positive gbm , although the efficacy of braf inhibitors in nonmelanoma cancers has not been systematically explored . 
a basket study of 122 patients with braf v600e mutations in various nonmelanoma cancer types found three out of six patients with gbm experienced tumor regression with vemurafenib.8 a pediatric case series presented three pediatric patients with braf v600e - mutant high - grade gliomas treated with vemurafenib , including a patient with clinical and neurologic improvement 20 months after starting treatment.9 robinson et al10 reported a case of complete clinical regression of a braf v600emutant pediatric gbm treated with braf inhibitor therapy . 
the patient underwent a craniotomy with resection , and pathology demonstrated glioblastoma , who grade 4 , isocitrate dehydrogenase ( idh - 1 ; wild - type immunohistochemistry and by sequencing )  . 
further analysis showed a tert mutation and wildtype for both atrx and egfr . immediate postoperative imaging showed residual enhancement superior to the resection cavity , treated with gamma knife radiosurgery . 
subsequent treatment consisted of fractionated intensitymodulated radiation therapy of 60 gy at 2 gy per fraction with concurrent daily temozolomide 75 mg / m2 , followed by monthly cycles of maintenance temozolomide . 
her treatment was then switched to bevacizumab monotherapy . eleven months postsurgery , or 4 months after switching to bevacizumab monotherapy , she was found to have a right hemispheric focus of duralbased enhancement concerning for local recurrence and underwent repeat gamma knife radiosurgery . 
within 2 months of starting vemurafenib , she was weaned off all opioid medications , dexamethasone , baclofen , and gabapentshe reported a significant improvement in her quality of life and was once again able to work with physical therapy to improve her chronic left - sided weakness . 
five months after starting vemurafenib , her brain and spine mri demonstrated significant improvement in intracranial leptomeningeal disease and in the nodular leptomeningeal enhancement along the conus medullaris and multiple nerve roots of the cauda equina . 
eleven months after starting vemurafenib monotherapy , the patient reported feeling well overall and had achieved stable disease on brain and spine mri ( fig 3 )  . she denied any headaches , visual changes , back pain or neuropathy , or gi or genitourinary symptoms . 
she was rated 80% on the karnofsky performance status scale . discussion this case report is consistent with several others in showing significantly improved survival with the use of braf kinase inhibitors in braf v600e positive gbm . 
no epithelioid or rhabdoid morphology was identified . spine , which demonstrated drop metastases throughout the thoracic and lumbosacral spine , specifically on the posterior cord from t10 - 12 , anterior to the conus medullaris , and throughout the cauda equina . 
an mri of the spine 1 month later showed a significant increase in the number and size of the abnormal cord enhancement lesions . one month after being diagnosed with metastatic recurrent glioblastoma , the patient was referred to our clinic , and we recommended addition of carboplatin area under the curve 4 intravenously monthly to her regimen of bevacizumab 10 mg / kg intravenously every 2 weeks . 
at the time of vemurafenib approval 2 months later and before starting the braf inhibitor , neuraxis imaging demonstrated development of leptomeningeal enhancement around the lobe resection cavity and initial right parietal considerable progression of metastatic spinal cord disease . 
 plasma concentration ratio for dabrafenib was 10 - fold higher compared with vemurafenib.17 in the dabrafenib plus trametinib versus vemurafenib alone in unresectable or metastatic braf v600e / k cutaneous melanoma ( combi - v ) trial , patients with braf - mutated metastatic melanomas who were treated with the combination of dabrafenib and mek inhibitor trametinib had significantly longer pfs than those treated with vemurafenib monotherapy.18 furthermore , dabrafenib appears to be less nephrotoxic than vemurafenib.19 nonmelanoma tumorspecific studies of braf inhibitors are difficult to conduct because of the relative rarity of these tumors and the low frequencies of braf mutations . 
these limitations also extend to basket trials of braf inhibitors , such as the national cancer institutemolecular analysis for therapy choice ( nci - match ; eay131 - h protocol ) evaluating dabrafenib and trametinib in patients with braf v600e or v600k mutations . 
despite these limitations , case reports of exceptional responders to targeted therapies such as ours support the value of genetics - guided therapy for activating braf mutations and driver mutations in general in gbm and other rare cancers , underscoring the need to systematically investigate these targeted drugs . the case reports can also be of value in supporting current off - label therapy of these rare mutations in tumor types not listed in the us food and drug administrationapproved indications . 
this microscopic image shows an immunohistochemical study for braf v600e . the tumor cells and their processes are positive for the mutated form of the protein . although there is a therapeutic potential of braf inhibitors in gbm , the experience with these drugs in melanoma treatment suggests that resistance will surely emerge in tumors responsive to this therapy . several mechanisms mediating resistance to braf inhibitors through mitogen - activated protein kinase ( mapk ) reactivation have been described , and coadministration of braf inhibitors with selective mapk inhibitors has led to significant improvement in progression - free survival in melanoma.15 coadministration with alternative survival pathway inhibitors , such as vascular endothelial growth factor and phosphatidylinositol 3 - kinase inhibitors , may also need to be evaluated.16 it could be further argued that dabrafenib might be the preferred braf kinase inhibitor . 
tran honoraria : novocure , monteris medical consulting or advisory role : novocure research funding : novocure , merck , novartis , tocagen , northwest biotherapeutics , vbl therapeutics , stemline therapeutics patents , royalties , other intellectual property : a molecular cell diary system , chemotherapeutic methods to target differentiated tumor cells , generep and nscore : method and apparatus for improved determination of node influence in a network , core master regulators of glioblastoma stem cells , conversion of glioblastoma multiforme cells into regulatory immune cells , novel targets that prevent cancer cells from evading the immune system and synergize with current immunotherapies travel , accommodations , expenses : novocure , monteris medical , novartis , tocagen , vbl therapeutics ashley p . 
 ( b ) the same regions are denoted by arrows on follow - up imaging performed 8 months later , showing improvement in metastatic disease and near - complete resolution of some lesions . references med 6 : 1359 - 1370 , 2014 1 . 
stupp r , mason wp , van den bent mj , et al : radiotherapy plus concomitant and adjuvant temozolomide for epidemiol biomarkers prev 23 : 1985 - 1996 , 2014 glioblastoma . 
stupp r , taillibert s , kanner aa , et al : maintenance therapy with tumor - treating fields plus temozolomide vs temozolomide alone for glioblastoma : a randomized clinical trial . 
myall nj , neal jw , cho - phan cd , et al : long - term survival of a patient with nonsmall - cell lung cancer harboring a v600e mutation in the braf oncogene . 
hyman dm , puzanov i , subbiah v , et al : vemurafenib in multiple nonmelanoma cancers with braf v600 mutations . n engl j med 373 : 726 - 736 , 2015 9 . 
schindler g , capper d , meyer j , et al : analysis of braf v600e mutation in 1 , 320 nervous system tumors reveals high mutation frequencies in pleomorphic xanthoastrocytoma , ganglioglioma and extra - cerebellar pilocytic astrocytoma . acta neuropathol 121 : 397 - 405 , 2011 14 . 
jang s , atkins mb : which drug , and when , for patients with braf - mutant melanoma ? lancet oncol 14 : e60 - e69 , 2013 17 . 
kieran mw , cohen kj , doz f , et al : complete radiographic responses in pediatric patients with brafv600 - positive tumors including high - grade gliomas : preliminary results of an ongoing phase 1 / 2a safety and pharmacokinetics ( pk ) study of dabrafenib . 
grob jj , amonkar mm , karaszewska b , et al : comparison of dabrafenib and trametinib combination therapy with vemurafenib monotherapy on health - related quality of life in patients with unresectable or metastatic cutaneous braf val600 - mutation - positive melanoma ( combi - v ) : results of a phase 3 , open - label , randomised trial . 
morphology and ow cytometry phenotype of the bone marrow and peripheral blood were consistent with a diagnosis of t - cell acute lymphoblastic leukemia ( t - all )  . 
targeted next - generation sequencing ( ngs ) based mutational proling ( foundation medicine , cambridge , ma ) of the bone marrow specimen demonstrated the following pathogenic molecular events : mtorc1483y , mtort1977k , nrasg12d , ptenr234 * ( 29base pair frameshift , subclonal ) , loss of p16ink4a , loss of exons 2 and 3 from p14arf , and phf6r116 * ( asterisk denotes a nonsense mutation )  . 
written informed consent for the study described herein was obtained from the patient . induction chemotherapy using a pediatric - type approach was initiated per the cancer and leukemia group b 10403 protocol.1 the patient achieved complete cytomorphologic remission as demonstrated on the day 28 bone marrow assessment . 
bone marrow biopsy performed on day 32 demonstrated continued morphologic and cytogenetic remission with full donor chimerism . at a clinic visit 11 days after discharge , the patient complained of progressive dyspnea and cough . 
there was no morphologic evidence of t - all in the biopsy sample . fluorescence in situ hybridization studies performed on tissue touch imprints with representative neoplastic hs cells demonstrated a male karyotype and were positive for the tcr , myc , and tcr rearrangements detected at t - all diagnosis ( figs 1e and 1f )  . molecular studies performed on hs parafn tissue blocks were also positive for tcr gene rearrangements , as described earlier . diagnostic t - all and hs lung biopsy specimens were submitted for ngs to foundation medicine , a clinical laboratory improvement amendmentscertied laboratory service . 
foundationone heme ( foundation medicine ) is a combination dnaand rna - sequencing assay using a hybrid - capture ngs technology with the capability to detect base substitutions , insertions and deletions , copy number variants , and select fusions from a panel of more than 400 protein - coding genes , 250 rna transcripts , and 30 selected introns thought to play a role in hematologic malignancies . 
positive immunohistochemistry for ( c ) cd163 and ( d ) cd68 conrms histiocytic lineage . ( e ) fluorescence in situ hybridization studies performed on tissue touch imprints show ghost outline for the large neoplastic histiocytes . 
 ( f ) breakapart probes ( cytocell , tarrytown , ny ) identied recurrent rearrangements of the myc locus at 8q24 and the tcr locus at 7q34 in 112 of 200 cells analyzed , identical to those present at the time of t - cell actute lymphoblastic leukemia diagnosis . 
tmb is reported to be low if a level of 5 mutations per megabase ( muts / mb ) or lower is detected , intermediate if a level of 6 to 19 muts / mb is detected , and high if a level of 20 muts / mb or greater is detected . 
the biopsy sample tested negative for brafv600e mutation.2 the patient was treated with a chemotherapy regimen of ifosfamide , carboplatin , and etoposide.3 bone marrow assessment before therapy initiation showed full donor chimerism and was negative for t - all and hs . 
cycle 2 was started on day 20 , with the positron emission tomographyct scan at this time demonstrating intensively positron emission tomographyavid lesions throughout both lungs ( fig 2a )  . 
therefore , we chose to treat the patient with ipilimumab because he presented with predominantly extramedullary relapsed disease and did not respond to a standard chemotherapeutic regimen aimed at hs . 
in a 2016 series of 28 patients with relapsed hematologic malignancies after allogeneic transplantation , ipilimumab was particularly active in patients with acute leukemia with extramedullary relapse.4 in addition , recent analysis of tmb across the spectrum of histiocytic neoplasms by goyal et al5 found that hs harbors a higher tmb than the other tumor types examined and that patients with hs would likely benet from further investigation into treatment with checkpoint inhibitor therapies . 
repeat imaging after one dose of ipilimumab showed substantial reduction of disease burden ( fig 2b ) , but shortly thereafter , the patient presented with a total - body rash that was ultimately proven to be grade 4 cutaneous graft - versus - host disease ( gvhd )  . although ngs - based mutational proling of the hs specimen had not revealed immediately targetable molecular lesions , mutations in nras may portend sensitivity to map kinase pathway inhibitors through activation of downstream signaling.6 a previous report of a patient with atypical chronic myeloid leukemia containing nrasg12d exhibited a durable response to trametinib7 ( a mek inhibitor )  . 
gounder et al8 have also reported on the successful use of trametinib in a patient presenting with hs ( and previous follicular lymphoma ) harboring an activating mutation in map2k1 . 
a recent analysis of the us national cancer institute seer database uncovered 159 reported patients with hs in the period between 2000 and 2014.9 although hs can arise sporadically , a considerable proportion of hss occur in patients with previous or synchronous hematopoietic malignancies and have been found to harbor identical bor t - cell receptor rearrangements as those observed in the associated tumors . 
 ( a ) maximumintensity coronal and fused axial projections from positron emission tomography ( pet ) and computed tomography ( ct ) after one cycle of ifosfamide , carboplatin , and etoposide chemotherapy show progressive disease burden with several pet - avid foci and malignant rightsided pleural effusion . 
in the case of this patient , such explanations would include dedifferentiation of t - all to an uncommitted stem cell that subsequently differentiates in a myeloid - biased fashion ; residual neoplastic cells responding to intrinsic or extrinsic inuences with changes in transcription factor levels , cytokine signaling , or epigenetic modication that mediate transdifferentiation to hs ; and the presence of a shared clonal precursor giving rise to both tumors ( appendix fig a2 )  . because we conducted longitudinal ngs - based analysis , the patients clinical course can be understood by deconstructing the molecular evidence available . 
two of the seven molecular lesions identied in our patients diagnostic t - all bone marrow specimen , specically the loss of p16ink4a and loss of exons 2 and 3 from p14arf , were not present in the post - transplantation hs specimen , which was resequenced by ngs using the same assay . 
consistent with a previous report by brunner et al12 of hs arising in the context of this makes hypotheses based on transdifferentiation or dedifferentiation or redifferentiation mechanisms improbable , because such genomic losses are considered irreversible . follicular lymphoma , the cdkn2a gene encodes for tumor suppressor proteins p16ink4a and p14arf through use of different open reading frames and alternative splice isoforms . 
specically , using a mouse model , they demonstrated that normal ink4a / arf and pten tumor suppressor function is required to preserve homeostasis in hematopoietic compartments and constrain emergence of hs . 
mutational proling of our patients hs specimen did not reveal genetic deletions in the cdkn2a locus , which had been detected in the diagnostic t - all sample , as might be suspected by the ndings of carrasco et al.13 however , their analysis of human hss revealed that alternative mechanisms , such as hypermethylation of the p16ink4a and p14arf promoters , might also develop , mediating loss of tumor suppressor function and subsequent development of hs in cooperation with pten inactivation . ngs - based mutational proling from the t - all diagnostic specimen and the specimen of the hs that presented after transplantation was also notable for the presence of phf6116 *  . 
recent analysis has uncovered that phf6 mutations are early events in t - all leukemogenesis and that phf6 loss propagates transcriptional networks associated with leukemia stem - cell activity.14 this allows for the construction of a disease progression model whereby enhanced expression of phf6116 * promoted the divergence of t - all from a bipotential neoplastic progenitor population that also gave rise to hs . 
given the acquisition of additional genetic events in the t - all genome , it is possible that our patients t - all branched from the malignant precursor later than the hs but clinically presented rst.15 because establishing the diagnosis of hs is difcult , a history of lymphoid neoplasm should warrant suspicion on the part of the clinician . 
although much of the literature on the disease is limited to case reports , hs is an exceedingly rare neoplasm with a rapid clinical course and no standard treatment options . 
grifths , md , department of medicine , roswell park comprehensive cancer center , elm and carlton sts , buffalo , ny ; twitter : @roswellpark ; e - mail : elizabeth.grifths@roswellpark.org. sheila sait speakers bureau : celgene relationships are self - held unless noted . 
grifths honoraria : novartis , abbvie consulting or advisory role : celgene , boston scientic , persimmune , new link genetics , otsuka , alexion pharmaceuticals , partner therapeutics research funding : genentech ( inst ) , celgene ( inst ) , astex pharmaceuticals ( inst ) , apellis pharmaceuticals ( inst ) , astex pharmaceuticals ( inst ) , celldex therapeutics ( inst ) no other potential conicts of interest were reported . acknowledgment we thank eunice wang , md ; james thompson , md ; evelena ontiveros , md , phd ; philip mccarthy , md ; and maureen ross , md , phd , for providing clinical care and wish to dedicate this article to the memory of the patient described herein . references advani as , sanford b , luger s , et al : frontline - treatment of acute lymphoblastic leukemia ( all ) in older adolescents and young adults ( aya ) using a pediatric regimen is feasible : toxicity results of the prospective us intergroup trial c10403 ( alliance )  . 
moskowitz ch , bertino jr , glassman jr , et al : ifosfamide , carboplatin , and etoposide : a highly effective cytoreduction and peripheral - blood progenitor - cell mobilization regimen for transplant - eligible patients with non - hodgkins lymphoma . 
j clin oncol 17 : 3776 - 3785 , 1999 davids ms , kim ht , bachireddy p , et al : ipilimumab for patients with relapse after allogeneic transplantation . 
hematol oncol clin north am 31 : 705 - 719 , 2017 khanna v , pierce st , dao kh , et al : durable disease control with mek inhibition in a patient with nras - mutated atypical chronic myeloid leukemia . 
n engl j med 378 : 1945 - 1947 , 2018 kommalapati a , tella sh , durkin m , et al : histiocytic sarcoma : a population - based analysis of incidence , demographic disparities , and long - term outcomes . blood 131 : 265 - 268 , 2018 10 . 
feldman al , arber da , pittaluga s , et al : clonally related follicular lymphomas and histiocytic / dendritic cell sarcomas : evidence for transdifferentiation of the follicular lymphoma clone . 
huang w , qiu t , zeng l , et al : high frequency of clonal ig and t - cell receptor gene rearrangements in histiocytic and dendritic cell neoplasms . 
carrasco dr , fenton t , sukhdeo k , et al : the pten and ink4a / arf tumor suppressors maintain myelolymphoid homeostasis and cooperate to constrain histiocytic sarcoma development in humans . 
wendorff aa , quinn sa , rashkovan m , et al : phf6 loss enhances hsc self - renewal driving tumor initiation and leukemia stem cell activity in t - all . 
computed tomography ( ct ) scan at the time of presentation to oncology care demonstrates ( a ) a 20 15 cm mass within the anterior mediastinum and ( b ) splenomegaly . 
 roloff et al common progenitor leukemogenesis hs oncogenesis nras g12d pten r234fs phf6 r116 * mtor c1483y , t1977k cdkn2a ( p16 ink4a loss ) p14 arf ( loss of exons 2 - 3 ) tcell acute lymphoblastic leukemia transdifferentiation mtor c1483y , t1977k cdkn2a ( p16 ink4a loss ) p14arf ( loss of exons 2 - 3 ) nras g12d pten r234fs phf6 r116 * histiocytic sarcoma fig a2 . 
the schematic depicts potential routes for stepwise oncogenesis of t - cell acute lymphoblastic leukemia ( t - all ) and histiocytic sarcoma ( hs ) from a common malignant precursor cell . 
shared mutational composition in nras , pten , and phf6 likely arose in the progenitor cell , whereas the acquisition of mutations in mtor and cdkn2a ( p16ink4a / p14arf losses ) occurred privately in t - all . 
possible transdifferentiation events showing the development of hs from t - all and vice versa are also depicted but are unlikely given the irreversibility of genomic losses in p16ink4a and p14arf ( dashed line )  . 
 prospective genomic profiling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making see accompanying editorial doi : purpose a long natural history and a predominant osseous pattern of metastatic spread are impediments to the adoption of precision medicine in patients with prostate cancer . 
to establish the feasibility of clinical genomic profiling in this disease , we performed targeted deep sequencing of tumor and normal dna from patients with locoregional , metastatic noncastrate , and metastatic castration - resistant prostate cancer . patients and methods patients consented to genomic analysis of their tumor and germline dna . a hybridization capture - based clinical assay was used to identify single - nucleotide variations , small insertions and deletions , copy number alterations , and structural rearrangements in more than 300 cancer - related genes in tumors and matched normal blood . results we successfully sequenced 504 tumors from 451 patients with prostate cancer . 
twenty - seven percent of patients harbored a germline or a somatic alteration in a dna damage repair gene that may predict for response to poly ( adp - ribose ) polymerase inhibition . 
in contrast , comparative analysis across disease states revealed that apc alterations were enriched in metastatic tumors , whereas atm alterations were specifically enriched in castration - resistant prostate cancer . conclusion through genomic profiling of prostate tumors that represent the disease clinical spectrum , we identified a high frequency of potentially actionable alterations and possible drivers of disease initiation , metastasis , and castration resistance . 
2017 by american society of clinical oncology wassim abida joshua armenia anuradha gopalan ryan brennan michael walsh david barron daniel danila dana rathkopf michael morris susan slovin brigit mclaughlin kristen curtis david m . 
although molecular profiling is not yet considered a standard - of - care for patients with this disease , new evidence points to enhanced treatment response in specific molecular contexts , paving the way for therapy selection on the basis of tumor molecular characteristics . 
all tumors were reviewed by pathologists who specialize in genitourinary oncology for confirmation of malignant histology of prostatic origin . sequencing and analysis we used the msk - impact assay as previously described10 , 11 ( fig 1a )  . 
the assay was performed in a clinical laboratory improvement amendments certified laboratory and designed to robustly identify single - nucleotide variations , small insertions and deletions ( indels ) , somatic copy number alterations , and structural rearrangements in more than 300 cancerrelated genes in formalin - fixed and paraffinembedded tumors and matched normal blood . somatic variant analysis was performed as described , 10 , 11 with germline variants identified in matched blood samples filtered out in the somatic analysis process . 
somatic findings were reported in the electronic medical record and anonymized and uploaded to cbioportal for visualization and analysis.12 - 14 clonality of mutations was estimated as cancer cell fraction15 and implemented in the facets algorithm.16 beginning in may 2015 , patients were given the option to consent to analysis of germline variants that were identified via sequencing of normal blood samples . 
germline analysis of 76 known cancer - predisposing genes was performed as previously described.16a additional methods are provided in the data supplement . results targeted dna sequencing of tumornormal pairs from patients with prostate cancer using the msk - impact assay , we successfully profiled 504 tumors from 451 patients with prostate cancer who presented to the clinic ( fig 1a and data supplement )  . 
in total , 348 patients ( 77% ) had metastatic prostate cancer , 53 ( 12% ) had biochemical recurrence after definitive therapy , and 50 ( 11% ) had locoregional disease ( fig 1b )  . 
metastatic tumors that were successfully profiled were obtained from lymph node ( 45% ) , bone ( 22% ) , liver ( 14% ) , lung ( 5% ) , and other soft tissue sites ( 14% ; fig 1c )  . 
unlike the tcga and su2c - pcf studies , tumors that were profiled represented all three prostate cancer clinical states : locoregional , metastatic noncastrate , and metastatic castration resistant . we began with 746 biopsy / surgical samples to successfully sequence the 504 tumors reported above , with an overall success rate of 68% ( appendix fig a1 )  . 
 a tumor pathology review matched normal extraction library construction target gene capture somatic analysis ( snvs , indels , cnvs , fusions ) germline analysis ( with specific consent ) tumor report in emr genetics report in emr metastatic tumor site other soft tissue lung liver bone patient disease state ( highest known ; n = 451 patients ) locoregional biochemically recurrent metastatic sample type prostate metastasis disease state at time of tumor tissue collection ( n = 504 tumors ) locoregional locoregional locoregional metastatic noncastrate metastatic castration resistant fig 1 . 
their disease state at the time of tissue collection for the 504 tumors that were profiled is represented at bottotumors that were profiled represented all three prostate cancer clinical disease states : locoregional , metastatic noncastrate , and metastatic castration resistant . 
cnv , copy number variation ; emr , electronic medical record , msk - impact , memorial sloan kettering - integrated mutation profiling of actionable cancer targets ; snv , single - nucleotide variation . states and are shown in fig 2 , grouped in pathways that are potentially clinically actionable . prospectively acquired primary tcga tumors ( appendix fig a3 )  . overall , the frequency of alterations in genes of interest in prostate cancer was similar for mcrpc tumors that were profiled in the msk - impact and su2c - pcf mcrpc data sets4 ( appendix fig a2 ) but demonstrated now in a clinical practice setting . 
however , notable differences were observed when comparing primary localized tumors in the msk - impact data set with those that were profiled in the prospective tcga study , including a higher frequency of alterations in tp53 and foxa1 in msk - impact tumors ( appendix fig a3 )  . 
this is most likely a result of the more aggressive nature of the primary localized tumors in the msk - impact cohort , which were predominantly obtained from patients who subsequently developed biochemically recurrent and metastatic disease ( fig 1b ) relative to the in total , 24% of patients carried somatic alterations in the pi3k / akt pathway , including in pten , pik3ca , pik3cb , pik3r1 , akt1 , and akt3 ( appendix fig a4 )  . 
alterations in commonly affected genes in prostate cancer ( eg , ar , pten , tp53 , foxa1 ) are shown in addition to genes in potentially actionable or biologically relevant pathways . 
mapk , mitogen - activated protein kinase ; msk - impact , memorial sloan ketteringintegrated mutation profiling of actionable cancer targets ; pi3k , phosphatidylinositol - 3kinase . homologous recombination , including brca2 , brca1 , atm , fanca , rad50 , palb2 , and cdk1217 - 21 ( fig 3a and appendix fig a7 )  . a recent multi - institutional study identified a high frequency of ddr gene alterations in the germline of patients with advanced prostate cancer.22 of patients in our data set , 221 underwent formal germline analysis , the first 124 of whom were included in the previously reported study.22 of these 221 patients , 42 ( 19% of total ) had a known or likely pathogenic germline mutation in brca2 ( 9% of total ) , chek2 ( 4% ) , atm ( 2% ) , brca1 ( 1% ) , fh ( 1% ) , and pms2 , nbn , palb2 , and brip1 ( , 1% each ; fig 3b and appendix table a1 )  . 
whereas germline ddr gene alterations may predict for response to parp inhibition or platinum agents , somatic - only alterations in these genes without a germline event may still predict for drug response.9 of the 221 patients who underwent germline analysis , 27% demonstrated alterations in brca2 , brca1 , atm , or chek2 , either in the germline or somatically ( fig 3c )  . 
of note , germline analysis alone accounted for approximately one half of these patients only , which suggests that both germline and somatic analysis should be performed to identify patients with ddr gene deficiency . in total , 3% of patients had tumors with somatic alterations in mismatch repair ( mmr ) genes msh2 , mlh1 , pms2 , or msh6 . 
these tumors accounted for the majority of samples with the highest mutation counts on msk - impact profiling ( fig 3d ) , which were confirmed to be enriched for previously described mmr and microsatellite instability signatures23 , 24 ( appendix fig a8 )  . 
identification of mmr - deficient prostate cancers may have immediate clinical applicability , given recent data that suggest sensitivity of such tumors to immune checkpoint blockade in colorectal cancer and other malignancies.25 - 27 overall , 36% of patients were found to have a potentially actionable alteration by using the oncokb annotation platform27a ( appendix fig a9 )  . this platform does not include non - brca / atm germline alterations , missense alterations of unknown significance , and genes whose clinical significance is less clear , including cdk12 and fanca . 
as genomic alterations undergofurther characterization and new trials and drug targets emerge , the frequency of alterations that are defined as actionable may increase . comparative analysis of somatic alterations across disease states a unique aspect of this data set is that it includes genetic profiles of tumors that represent all three clinical states : locoregional , metastatic noncastrate , and metastatic castration resistant . 
consistent with previous studies , 3 , 4 we identified recurrent areas of copy number loss that involved chromosomes 6q , 8p , 13q , and 16q , and areas of copy number gain that involved chromosomes 1q , 3q , 7 , 8q , and x ( fig 4 )  . 
 displayed the highest burden of copy number alterations , whereas those that represented locoregional disease displayed the lowest ( fig 4 and appendix fig a10 )  . aiming to identify possible genomic drivers of disease progression , we performed a selective enrichment analysis to identify genes that were more frequently altered in mcrpc compared with locoregional disease ( fig 5a )  . 
ar amplification / mutation was the most enriched alteration in mcrpc , as shown in previous studies.3 , 4 other genes that were more commonly altered in mcrpc included tp53 , rb1 , pten , apc , atm , fanca , and cdk12 . we performed a similar analysis that compared alterations in mcrpc with metastatic noncastrate prostate cancer ( fig 5b )  . 
the high enrichment of alterations in ar in mcrpc relative to both locoregional and metastatic non - castrate disease serves as a positive control , consistent with the known role of ar as a driver of castration resistance.28 - 31 beyond frequent amplification of the gene , ar antiandrogen resistance mutations were identified in tumors from patients with mcrpc ( appendix fig a11 ) , including an f877l enzalutamide / arn509 resistance mutation32 , 33 that was found in the tumor of a patient who experienced progression after 4 years of treatment on arn509 . 
four locoregional tumors were found to have mutations in ar , including an h875y mutation that is known to confer resistance to flutamide29 , 34 in a prostatectomy 16 17 18 19 20 21 22 disease state : locoregional metastatic noncastrate metastatic castration resistant sample type : prostate metastasis scna fig 4 . 
represented here are regions of amplification ( red ) or deletion ( blue ) with chromosomes listed horizontally ( top ) in the msk - impact , su2c - pcf ( metastatic castration - resistant prostate cancer [ crpc ] ) , and tcga ( primary localized prostate cancer ) data sets . 
msk - impact tumors are sorted by disease state at time of tissue acquisition , from locoregional ( bottom , gray ) to metastatic crpc ( top , blue )  . 
the level of enrichment is represented as difference in frequency between the two indicated classes ( x - axis ) and its significance ( p value , y - axis )  . 
amp , amplification ; homdel , homozygous deletion ; mut , mutation . sample from a patient who was treatment - nave but who had received dutasteride for benign prostate enlargement . in addition to ar , we again identified enrichment of alterations in tp53 , rb1 , pten , and atm in mcrpc compared with metastatic noncastrate disease . 
enrichment of these genes in mcrpc relative to both earlier disease states implicates them in the development of castration resistance , a finding that is of particular interest for atm , a gene that is involved in ddr . 
fanca and cdk12 , two other dna repair genes , did not show statistically significant mcrpc compared with metastatic noncastrate disease as they did versus locoregional disease , enrichment although there is a trend that suggests a role in castration resistance as well ( fig 5d )  . 
when analysis was limited to metastatic tumors or lymph nodes only , similar trends for enrichment were observed , although statistical significance was not always reached because of smaller sample size ( appendix fig a12 )  . only two genes were enriched in metastatic noncastrate versus locoregional disease : apc and , to a lesser extent , arid5a ( fig 5c )  . 
these findings will require functional validation in the laboratory . matched samples identify clonal alterations in prostate cancer in total , 44 patients had more than one tumor site profiled by msk - impact , including 16 with a matched primary localized tumor and a subsequent metastatic tumor . 
tumors from the same patient that were acquired at a later time point typically had a higher mutation count ( fig 6a )  . given the high frequency of tp53 alterations that were observed in primary localized tumors in this data set and prior reports of aggressive behavior of prostate tumors that harbor tp53 alterations , 36 - 37a we sought to determine whether tp53 alterations were present in tumors early in their evolution or whether they were acquired later at disease progression . 
tp53 mutations were clonal , including in cases in which both a primary localized tumor and a later metastasis were available ( cancer cell fraction > 0.9 in the later metastasis )  . 
likewise , we found that somatic alterations in brca2 were present in matched tumors , which again suggested that somatic brca2 loss of function alterations occur early in tumorigenesis for affected patients . conversely , alterations in ar did not occur early in matched samples ( fig 6b , patients p - 0003597 and p - 0004910 ) , which is consistent with treatment - related changes that promote castration resistance . 
of note , other potentially actionable alterations may arise later in disease evolution , as was the case for patient p - 0002149 ( fig 6b ) , who acquired an activating pik3ca e545k mutation ( appendix fig a4b ) in a recurrent tumor nearly 3 years after his radical prostatectomy . to confirm the above findings , we performed phylogenetic analysis on cases in which several matched tumors were available from the same patient ( fig 6c )  . 
for patient p - 0003511 , ar amplification was truncal castration - resistant tumors , which is consistent with its well - characterized role in castration resistance.28 as the number of patients with prostate cancer who are profiled longitudinally throughout their clinical care increases , such findings may provide insight into clonal driver events that promote disease progression and site - specific metastasis . discussion unlike previous prostate cancer genomic studies , we profiled tumors that represent the clinical spectrum of the disease , from locoregional to metastatic noncastrate and metastatic castrationresistant prostate cancer , which enabled comparisons of genomic landscape across disease states using a single assay . 
whereas locoregional tumors in this data set typically represented more aggressive disease than tcga , patients with such tumors are those in greatest need of new treatment approaches and profiling of their tumors may have particular clinical relevance . an increase in copy number alterations and mutation frequency was evident in mcrpc compared with earlier disease states , as was an increased frequency of alterations in ar , tp53 , rb1 , and pten . 
spop mutations , however , were more frequent in the earlier disease states , which suggested better outcomes for patients with spop - mutant tumors , possibly through increased sensitivity to adt . 
in this analysis , apc and atm emerged as candidate genes of interest that may independently contribute to metastasis and castration resistance , respectively , pending functional validation in the laboratory . 
these genes , like atm , are involved in ddr , alluding to a possible role for dna repair defects in the development of castration resistance . we also found that tp53 alterations are early clonal events in matched tumor samples from individual patients . 
a notable exception ( * ) involves a bladder metastasis and a bone metastasis acquired 5 months later , where the patient had received salvage radiation to the pelvis , possibly explaining the higher mutation count in the earlier bladder tumor . 
 ( b ) somatic alterations in tp53 ( red ) , brca2 ( blue ) , ar ( gold ) , and pik3ca ( green ) in matched tumors in the data set , including localized primaries and later metastases ( green box ) and other matched tumors from the same patients . 
crpc , castration - resistant prostate cancer . available , it will be possible to validate this finding , guiding more aggressive treatment approaches early on for these patients . overall , we identified potentially actionable alterations , including hotspot activating alterations in genes that are known drug targets , consistent with findings of the su2c mcrpc study , but this time in a prospective clinical practice setting . 
these findings have immediate therapeutic relevance , given the recently reported sensitivity of these tumors to parp inhibition9 or immune checkpoint blockade.25 the higher frequency of dna repair alterations that were identified via integrative germline and somatic analyses strongly argues for performing both germline and somatic genomic analyses in all patients with advanced prostate cancer who will require systemic treatment , irrespective of screening on the basis of family history . in summary , this study shows that a large genomic data set that represents the clinical spectrum of prostate cancer can provide mechanistic insight into possible genomic drivers of disease initiation , metastasis , and drug resistance . 
our ability to profile metastatic tumors allowed us to detect the evolution of potential driver alterations in matched tumors from individual patients , identifying alterations in tp53 and brca2 as early events that may confer a more aggressive phenotype . 
scher provision of study materials or patients : wassim abida , joshua armenia , daniel danila , michael morris , susan slovin , marc ladanyi , liying zhang , victor e . 
scher collection and assembly of data : wassim abida , joshua armenia , ryan brennan , michael walsh , david barron , daniel danila , michael morris , susan slovin , brigit mclaughlin , kristen curtis , david m . 
scher data analysis and interpretation : wassim abida , joshua armenia , anuradha gopalan , michael walsh , daniel danila , dana rathkopf , michael morris , susan slovin , jeremy c . 
robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , abbvie ( inst ) , myriad genetics ( inst ) , biomarin ( inst ) , medivation ( inst ) , tesaro ( inst ) travel , accommodations , expenses : astrazeneca vijai joseph stock and other ownership interests : juno therapeutics daniel danila honoraria : astellas scientific , medical affairs , angle , bayer , xian - janssen pharmaceutical consulting or advisory role : angle , bayer research funding : prostate cancer foundation , genentech , janssen research & development ( inst ) patents , royalties , other intellectual property : gene expression profile associated with prostate cancer travel , accommodations , expenses : cambridge healthtech institute , prostate cancer foundation , angle , bayer , american austrian open medical institute , global technology community , xian - janssen pharmaceutical , oncology education dana rathkopf consulting or advisory role : janssen oncology research funding : janssen oncology ( inst ) , medivation ( inst ) , celgene ( inst ) , takeda ( inst ) , millennium pharmaceuticals ( inst ) , ferring ( inst ) , novartis ( inst ) , taiho pharmaceutical ( inst ) , astrazeneca ( inst ) , genentech ( inst ) , tracon pharma ( inst ) michael morris consulting or advisory role : astellas pharma , bayer , endocyte research funding : bayer ( inst ) , sanofi ( inst ) , endocyte ( inst ) , progenics ( inst ) travel , accommodations , expenses : bayer , endocyte susan slovin consulting or advisory role : bayer brigit mclaughlin no relationship to disclose kristen curtis no relationship to disclose david m . 
durack stock and other ownership interests : adient medical consulting or advisory role : adient medical patents , royalties , other intellectual property : patent disclosures , provisionals submitted for instrument to analyze biopsy specimens ( unrelated to the small renal masses topic )  . patent holder for device related to x - ray imaging data collection ( unrelated to small renal masses topic ) , july 2008 . other relationship : society of interventional radiology foundation stephen b . 
solomon leadership : devicor medical products stock and other ownership interests : johnson & johnson , progenics , aspire bariatrics consulting or advisory role : ge healthcare , angiodynamics , medtronic research funding : ge healthcare ( inst ) , angiodynamics ( inst ) patents , royalties , other intellectual property : ge healthcare - patents pending ( inst ) , aspire bariatrics ahmet zehir no relationship to disclose aijazuddin syed no relationship to disclose jianjiong gao no relationship to disclose debyani chakravarty no relationship to disclose hebert alberto vargas no relationship to disclose kenneth offit no relationship to disclose mark t.a. 
kantoff stock and other ownership interests : bellicum pharmaceuticals , metamark genetics , placon , druggablity technologies , tarveda consulting or advisory role : bavarian nordic , janssen , millennium pharmaceuticals , morphosys , pfizer , astellas pharma , bellicum pharmaceuticals , bind biosciences , endocyte , metamark genetics , medivation , merck , mtg therapeutics , oncocellmdx , oncogenex , sotio , sanofi , tokai pharmaceuticals , bayer , genentech , cristal therapeutics , ipsen , omnitura , gtx , tarveda , druggablity technologies , progenity research funding : medivation ( inst ) , sanofi ( inst ) , oncogenex ( inst ) , aragon pharmaceuticals ( inst ) , amgen ( inst ) , astellas pharma ( inst ) , bayer ( inst ) , bavarian nordic ( inst ) , dendreon ( inst ) , exelixis ( inst ) , janssen ( inst ) patents , royalties , other intellectual property : method for predicting the risk of prostate cancer morbidity and mortality , predicting and treating prostate cancer , methods for predicting likelihood of responding to treatment , chromosome copy number gain as a biomarker of urothelial carcinoma lethality , drug combinations to treat cancer , somatic ercc2 mutations correlate with cisplatin sensitivity in muscle - invasive urothelial carcinoma ( patent ) , up - to - date royalties , wolters - kluwer royalties expert testimony : sanofi , janssen travel , accommodations , expenses : sanofi , janssen , bind biosciences , bavarian nordic , millennium pharmaceuticals david b . 
sawyers leadership : novartis stock and other ownership interests : novartis , agios , blueprint medicines , beigene , oric pharmaceuticals consulting or advisory role : novartis , blueprint medicines , agios , beigene , oric pharmaceuticals patents , royalties , other intellectual property : xtandi nikolaus schultz no relationship to disclose howard i . 
grasso cs , wu ym , robinson dr , et al : the mutational landscape of lethal castration - resistant prostate cancer . 11 - 22 , 2010 nature 487 : 239 - 243 , 2012 7 . 
hyman dm , solit db , arcila me , et al : precision medicine at memorial sloan kettering cancer center : clinical next - generation sequencing enabling next - generation targeted therapy trials . 
cheng dt , mitchell t , zehir a , et al : msk - impact : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
joshi pm , sutor sl , huntoon cj , et al : ovarian cancer - associated mutations disable catalytic activity of cdk12 , a kinase that promotes homologous recombination repair and resistance to cisplatin and poly ( adp - ribose ) polymerase inhibitors . 
bajrami i , frankum jr , konde a , et al : genome - wide profiling of genetic synthetic lethality identifies cdk12 as a novel determinant of parp1 / 2 inhibitor sensitivity . 
mccabe n , turner nc , lord cj , et al : deficiency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
mskimpact versus su2cpcf dataset comparison . frequencies of alterations in select genes in metastatic crpc tumors from the msk - impact dataset ( orange ) versus the su2cpcf dataset ( red )  . 
mmr / msi mutation signatures in hypermutated tumors . k - means clustering of mutations / mb ( mut / mb ) across all 504 tumors identified two distinct clusters : cluster1 with mutations / mb10 . 
actionable alterations are ranked by level of evidence ( level 2b : standard of care biomarker predictive of response to an fda - approved drug in another indication , but not standard of care for this indication ; level 3a : compelling clinical evidence supports the biomarker as being predictive of response to a drug in this indication , but neither biomarker nor drug are standard of care ; level 3b : compelling clinical evidence supports the biomarker as being predictive of response to a drug in another indication , but neither biomarker nor drug are standard of care ; level 4 : compelling biological evidence supports the biomarker as being predictive of response to a drug , but neither biomarker nor drug are standard of care )  . 
variants were considered pathogenic or likely pathogenic per american college of medical genetics and genomics guidelines . somatic second hit is reported in column two for patients with germline dna damage repair gene mutations . 
of interest , several of the patients who harbored a germline brca2 c.5946delt ashkenazi founder mutation did not have a detectable somatic second hit in this gene , suggesting a nonclassical pathogenic mechanism for this mutation . 
 c acral lentiginous melanoma harboring a ros1 gene fusion with clinical response to entrectinib purpose ros1 gene fusions demonstrate oncogenic activity , and patients with nonsmall - cell lung cancer ( nsclc ) harboring a ros1 fusion benefit from the use of a ros1 inhibitor ; however , clinical response to ros1 inhibitors remains largely uncharacterized outside of nsclc . 
ros1 fusions have been identified in multiple tumor types but have not been reported in cutaneous melanoma . patients and methods tumors from 22 patients with acral lentiginous melanoma ( alm ) were analyzed with targeted rna sequencing to detect fusions in ros1 , ntrk1 , ntrk2 , ntrk3 , and alk genes . 
the patient underwent a dramatic and durable response to entrectinib , with a recist ( version 1.1 ) partial response of 238% at 3 months and 255% at 11 months . 
ohara ii seed grant program , an american cancer society institutional research grant to university of colorado cancer center , the amy davis foundation , and the moore family foundation . the university of colorado molecular tumor board ( at which patient case was discussed ) is supported in part by the colorado center for personalized medicine . clinical trial information : nct02097810 . corresponding author : kasey l . 
cdna was synthesized using the verso cdna kit ( thermo fisher scientific , waltham , ma ) , followed by pcr amplification using gotaq ( promega , madison , wi ) and gopcros1specific primers ( sense , 59 - agagcttgaggcaaacaa - 39 ; antisense , 59 - ccactgctgttccttcataca - 39 )  . 
purified pcr products were sequenced using the bigdye terminator cycle sequencing ready reaction kit ( version 3.1 ; applied biosystems , foster city , ca )  . clinical trial startrk - 1 ( studies of tumor alterations responsive to targeting receptor kinases ) is an ongoing multicenter phase i / iia open - label study of oral entrectinib ( rxdx - 101 ) in patients with locally advanced or metastatic cancer who have a confirmed ros1 , ntrk1 , ntrk2 , ntrk3 , or alk fusion . 
a fusion containing exons 1 to 4 of the gopc gene and exons 36 to 42 of the ros1 gene was detected in one patient ( table 1 ; fig 1a )  . 
expression of the gopc - ros1 fusion transcript was confirmed using reverse - transcriptase pcr followed by sanger sequencing ( fig 1b ) , and ihc of the tumor sample confirmed ros1 protein expression ( fig 1c )  . the patient with the gopc - ros1 fusion is a 46 - year - old man who was initially diagnosed with alm in 2010 . 
the patient then underwent amputation of the fifth toe with left groin sentinel lymph node biopsy followed by amputation of the fourth left toe and resection of a satellite nodule . 
because of high - risk disease , the patient underwent complete left inguinal lymph node dissection and received adjuvant biochemotherapy with cisplatin , vinblastine , dacarbazine , aldesleukin , and interferon alfa - 2b . approximately 1 year later , a recurrence was detected in the surgical scar , and this was reresected , followed later by recurrent in - transit metastases . mutation testing showed the tumor was wild type for braf and kit genes . 
 table 1 demographic and clinical characteristics of patients with aml in rna sequencing screen patient case no . age ( years ) stage location fusion detected * tissue left thumbnail bed sole , left foot plantar surface , right foot plantar surface , left foot right heel left heel left thumbnail right heel left thumb sole , left foot right heel right heel subcutaneous subcutaneous lymph node lymph node brain brain brain brain brain brain gopc - ros1 abbreviation : aml , acral lentiginous melanoma . * indicates no fusions were detected . patient with ros1 fusion responds to treatment with entrectinib given the ros1 fusion and the potential for response to targeted treatment , treatment options included off - label crizotinib , which is effective in ros1 - positive nsclc tumors , or a phase i clinical trial of the cns - penetrant ros1 / trk / alk inhibitor entrectinib . 
the patient was found eligible for this trial and provided written informed consent . at baseline , the patient had several palpable masses in the left leg , ranging from approximately 1 to 4 cm ( figs 2a to 2c ) , as well as a 12 - mm nodal mass in the paratracheal lymph node and a small right subpleural pulmonary nodule ( data not shown )  . the patient initiated entrectinib 600 mg orally once per day , and after 2 weeks , four of the five main lesions on the left leg were no longer palpable . 
staining was scored on a scale from 0 to 2 + , and all samples scored a 0 , except for two samples from one patient , which were scored 1 + and corresponded to the study patient described here ( table 2 )  . 
 ( b ) dna sequencing chromatogram of real - time polymerase chain reaction product confirms a gopc - ros1 fusion and validates the gopc exon 4 and ros1 exon 36 breakpoints . 
 ( c ) immunohistochemistry images ( magnification , 103 ) show tumor - specific staining for ros1 ( left ) in the patient tumor sample . he , hematoxylin and eosin . fig 2 target lesion responses to entrectinib at baseline ( column one ) , 3 months ( column two ) , and 11 months ( column three )  . ( a ) anterior proximal shin subcutaneous nodule ( yellow arrow )  . 
i = immediate family member , inst = my institution . for other cancer types where ros1 fusions have been detected , such as nsclc , but lower than frequencies reported for spitzoid neoplasms and spitzoid melanomas.8 , 17 we did not find any ros1 expressionpositive cases in 30 superficial spreading or nodular melanoma cases , consistent with the previous study conducted on 374 cutaneous melanomas.10 we also did not find any ros1 expressionpositive cases in the 18 mucosal melanomas ; however , the number of patients needed to estimate the true frequency likely needs to be much larger . 
although we found the overall ros1 fusion frequency to be 1.3% across all melanoma subtypes , the dramatic treatment response described in this report should prompt additional screening and studies of ros1 fusions in patients with melanoma . although entrectinib has shown activity against ros1 fusion tumors in nsclc , 18 this is the first report to our knowledge of entrectinib response against a ros1 fusion outside of lung cancer . entrectinib has previously demonstrated antitumor response in patients with tumors that are positive for alk or ntrk1 - 3 gene fusions in indications outside of nsclc , such as colorectal cancer , 19 , 20 astrocytoma , 18 and mammary analog secretory carcinoma.21 altogether , the tumor response observed in this patient with ros1 - positive melanoma is adding toagrowingbodyofliteraturesuggestinggenefusions in ros1 , ntrk1 - 3 , and alk may be generally responsive to their respective tyrosine kinase inhibitors , irrespective of the tumor histology context.18 , 22 - 24 published online on po.ascopubs.org on march 2 , 2017 . relationships may not relate to the subject matter of this manuscript . 
charest a , lane k , mcmahon k , et al : fusion of fig to the receptor tyrosine kinase ros in a glioblastoma with an interstitial del ( 6 ) ( q21q21 )  . 
birch ah , arcand sl , oros kk , et al : chromosome 3 anomalies investigated by genome wide snp analysis of benign , low malignant potential and low grade ovarian serous tumours . 
murphy da , ely ha , shoemaker r , et al : detecting gene rearrangements in patient populations through a 2 - step diagnostic test comprised of rapid ihc enrichment followed by sensitive next - generation sequencing . 
drilon a , de braud fg , siena s , et al : entrectinib , an oral pan - trk , ros1 , and alk inhibitor in tki - nave patients with advanced solid tumors harboring gene rearrangements : updated phase i results . 
sartore - bianchi a , ardini e , bosotti r , et al : sensitivity to entrectinib associated with a novel lmna - ntrk1 gene fusion in metastatic colorectal cancer . 
drilon a , li g , dogan s , et al : what hides behind the masc : clinical response and acquired resistance to entrectinib after etv6 - ntrk3 identification in a mammary analogue secretory carcinoma ( masc )  . 
hong ds , farago af , brose ms , et al : clinical safety and activity from a phase i study of loxo - 101 , a selective trka / b / c inhibitor , in solid - tumor patients with ntrk gene fusions . 
vassal g , faivre l , geoerger b , et al : crizotinib in children and adolescents with advanced ros1 , met , or alk - rearranged cancer : results of the acse phase ii trial . 
approximately 20% to 25% metastasize to distant sites and are generally associated with poor response to treatment.1 outcomes with systemic chemotherapy have historically been poor.2 with improved understanding of molecular biology of these tumors , we are beginning to identify promising potential therapeutic targets . in particular , the human epidermal growth factor receptor 2 / neu ( her2 / neu ) oncogene , one of the tyrosine kinase receptors , is overexpressed in salivary duct carcinomas ( 44% ) , salivary gland adenocarcinomas ( 21% ) , and adenoid cystic carcinomas ( 2% ) , among other subtypes.3 trastuzumab , a monoclonal antibody that binds to the extracellular domain of her2 / neu , inhibits the proliferation of tumor cells that overexpress her2 / neu.4 patients with her2 / neu - overexpressing sgns are often treated with trastuzumab - containing regimens with encouraging results , but disease progression is inevitable , even with a favorable initial response . 
the antibody - drug conjugate adotrastuzumab emtansine ( t - dm1 ) is currently approved for treating her2 - positive metastatic breast cancer that has progressed on therapy with trastuzumab . this antibody - drug conjugate selectively directs the cytotoxic drug emtansine to tumor cells with her2 / neu expression , thereby minimizing systemic toxicities.5 results favorable given the seen with adotrastuzumab emtansine in patients with breast cancer , it is logical to consider administering it to patients with sgns that overexpress her2 / neu after they have progressed on trastuzumab with or without chemotherapy . 
sequential her2 / neu - directed therapy has been successfully used with sustained clinical benet , albeit in a single patient.6 here we report on the clinical outcomes of seven patients with metastatic sgns who were treated at our institution with adotrastuzumab emtansine ( table 1 ) , and we summarize the clinical course and response to therapy of one patient . a 45 - year - old man presented with a painless right neck mass in late 2013 . 
fine - needle aspiration revealed a high - grade carcinoma and positron emission tomography / ct ( pet / ct ) showed multiple uorodeoxyglucose ( fdg ) - avid lymph nodes in the right cervical region . 
surgical pathology revealed a 3.9 - cm high - grade salivary duct carcinoma that was positive for androgen receptor ( ar ) and her2 / neu ( 3 + ) by immunohistochemistry ( ihc ) staining . 
because of the high - risk features of extracapsular nodal extension and close margins , he received adjuvant chemotherapy with cisplatin and radiation therapy once per week in october 2014 . 
 ( c ) restaging scan in june 2018 after ado - trastuzumab emtansine shows a complete metabolic response of previously noted metastatic lymphadenopathy . currently a void in the therapeutic guidelines for managing this disease . 
standard treatment of sgns involves surgical resection with or without adjuvant radiation therapy . locoregional recurrence and metastases are common , at which time palliative chemotherapy is considered , but response rates are generally poor , and the duration of response is brief without a clear favorable impact on survival . 
given the aggressive nature of these tumors and the limited treatment options upon relapse and metastasis , there has been an increased interest in developing targeted therapies . two such targets , the ar and her2 / neu receptor tyrosine kinase , are currently used in clinical practice with variable results.7 a relatively large retrospective case series has reported favorable outcomes using androgen deprivation therapy in ar - positive sgns with good tolerability and an overall survival benet.8 the success of her2 / neu - directed therapy in breast cancer has resulted in multiple case reports that show benet from using trastuzumab - based regimens in treating sgns.4 , 9 despite initial success with targeted therapy , however , progression is inevitable . mechanisms of resistance have not been extensively explored . 
therefore , it seems reasonable to consider the use of ado - trastuzumab emtansine upon progression on trastuzumab , drawing on its demonstrated activity and clinical benet in the analogous clinical scenario in patients with advanced her2 / neu - positive breast cancer.10 by contrast to the previous reports , we describe one of the largest single - institution experiences with her2 / neutargeted therapy in patients with metastatic sgns . 
most of our patients ( n = 6 of 7 ) experienced progression after trastuzumab , which highlights the role of sequential her2 / neu therapy described by almquist et al.6 all of our patients tumors demonstrated her2 / neu overexpression , and most had a high degree of her2 / neu receptor positivity . in our retrospective case series , there was variability in the methods for her2 / neu testing that reect the natural evolution of institutional testing practices . 
nevertheless , clinical benet was seen regardless of the method of testing diagnosed with high - grade right parotid salivary carcinoma solitary liver metastasis retroperitoneal lymph node metastases progression of retroperitoneal lymph node metastases surgical resection with modied radical neck dissection left hepatic lobectomy cisplatin and rt bicalutamide and leuprolide carboplatin and paclitaxel ado - trastuzumab emtansine trastuzumab and pertuzumab maintenance time ( months ) fig 2 . 
 swed , cohen , and aggarwal ( ihc , uorescence in situ hybridization , or next - generation sequencing ) , conrming the role of a her2 / neu - targeted approach . 
for example , the patient discussed here initially experienced a complete metabolic and radiographic response and derived a sustained clinical benet with a progression - free survival of 29 months that is ongoing . progression - free survival in all of our patients ranged from 6 to 29 months , and overall survival ranged from 9 to 33 months . 
all of the patients experienced varying degrees of neuropathy , which proved to be dose - limiting in patient 2 . thrombocytopenia was another adverse effect of therapy , which led to interruption of therapy in one patient . 
cohen honoraria : bristol - myers squibb consulting or advisory role : heat biologics , takeda pharmaceuticals , cerulean pharma , kolltan pharmaceuticals , zymeworks , pzer research funding : heat biologics ( inst ) , macrogenics ( inst ) , merck ( inst ) , takeda pharmaceuticals ( inst ) , cleave biosciences ( inst ) , celldex ( inst ) travel , accommodations , expenses : heat biologics takeda pharmaceuticals , kolltan pharmaceuticals , cerulean pharma , zymeworks , bristol - myers squibb , pzer charu aggarwal consulting or advisory role : genentech , bristol - myers squibb , eli lilly , celgene , medimmune research funding : genentech ( inst ) , incyte ( inst ) , macrogenics ( inst ) , merck sharp & dohme ( inst ) , astrazeneca / medimmune ( inst ) no other potential conicts of interest were reported . references bradley pj : distant metastases from salivary glands cancer . 
otolaryngol head neck surg 154 : 1041 - 1046 , 2016 alotaibi am , alqarni ma , alnobi a , et al : human epidermal growth factor receptor 2 ( her2 / neu ) in salivary gland carcinomas : a review of literature . 
j clin diagn res 9 : ze04 - ze08 , 2015 limaye sa , posner mr , krane jf , et al : trastuzumab for the treatment of salivary duct carcinoma . 
oncologist 18 : 294 - 300 , 2013 girish s , gupta m , wang b , et al : clinical pharmacology of trastuzumab emtansine ( t - dm1 ) : an antibody - drug conjugate in development for the treatment of her2 - positive cancer . 
cancer chemother pharmacol 69 : 1229 - 1240 , 2012 almquist d , umakanthan jm , ganti ak : sequential her2 - targeted therapy in salivary ductal carcinoma with her2 / neu overexpression and a concomitant erbb2 mutation . 
head neck pathol 12 : 95 - 104 , 2018 boon e , van boxtel w , buter j , et al : androgen deprivation therapy for androgen receptor - positive advanced salivary duct carcinoma : a nationwide case series of 35 patients in the netherlands . 
head neck 40 : 605 - 613 , 2018 van boxtel w , boon e , weijs wlj , et al : combination of docetaxel , trastuzumab and pertuzumab or treatment with trastuzumab - emtansine for metastatic salivary duct carcinoma . 
baron jm , boster bl , barnett cm : ado - trastuzumab emtansine ( t - dm1 ) : a novel antibody - drug conjugate for the treatment of her2 - positive metastatic breast cancer . 
vitanza , md1 , 3 ; and bonnie cole , md1 , 4 introduction xeroderma pigmentosum ( xp ) is a rare autosomal recessive disorder caused by a nucleotide excision repair decit , resulting in sensitivity to uv radiation.1 individuals with xp are 10 , 000 times more likely to develop cutaneous squamous cell carcinoma ( scc ) , with initial presentation at a median age of 9 years.2 metastatic skin cancer is the leading cause of death ( 34% ) , with a median survival of 32 years.2 few options for effective systemic therapy of advanced cutaneous scc are available , 3 , 4 and there is no standard therapy for patients with xp who have developed metastatic skin malignancies.5 there is a critical need for effective therapy for advanced skin cancers , and patients with xp represent a unique need because they have the potential to suffer catastrophic adverse effects from standard chemotherapeutic agents.6 immune checkpoint blockade has demonstrated efcacy in tumors characterized by high mutational burincluding scc.7 , 8 therefore , cutaneous scc is den , a good candidate for additional investigation of response to checkpoint inhibitors.9 - 13 a recent phase i / ii clinical trial demonstrated partial response in 41% of patients receiving the programmed cell death 1 ( pd - 1 ) inhibitor cemiplimab.14 case reports in patients with xp and advanced scc describe response with pd - 1 inhibitors , including pembrolizumab.5 , 15 - 17 however , these reports do not provide a molecular mechanistic rationale for the use of pd - 1 inhibitors specic to this patient population , nor do they provide support for the use of these agents for long - term disease management . 
we report stable disease for 2 years in response to pembrolizumab in a patient with xp and metastatic cutaneous scc , along with molecular ndings to support the use of pd - 1 inhibitors in patients with xp . 
extensive perineural spread along the right inferior alveolar nerve and right third through sixth in addition to lepcranial nerves was observed , tomeningeal spread into the right aspect of the posterior fossa ( figs 1a to 1d )  . biopsies of sites concerning for malignant skin lesions were performed , including separate left lower eyelid , right conjunctiva and cornea , and right preauricular masses ; all were diagnostic of scc . 
perineural spread of squamous cell carcinoma ( a to d ) at time of diagnosis and ( e to h ) after therapy , shown by contrast - enhanced t1 - weighted magnetic resonance imaging . 
 ( a ) axial image through face at level of parotid gland shows asymmetric nodular enhancement throughout right parotid gland , as well as more anterior nodular supercial enhancing tissue ( arrow )  . 
 ( b ) axial , ( c ) coronal , and ( d ) sagittal images through head at level of cavernous sinus and right pterygopalatine fossa show extensive abnormal enhancing tissue within cavernous sinus , extending anteriorly into the right orbital apex , as well as posteriorly toward posterior fossa ( arrowheads )  . 
 ( e and f ) five months after initiation of therapy , imaging shows dramatic reduction in tumor burden , both ( e , arrow ) in supercial tissues of face and ( f , arrowheads ) within cavernous sinus and orbital apex . 
 ( g and h ) thirteen months after initiation of therapy , disease burden had diminished further , both ( g , arrow ) in supercial tissues of the face and ( h , arrowheads ) within the cavernous sinus and orbital apex . were also tested and did not show any unexpected mutations ( data supplement )  . 
both tumors showed a signicant strand bias ( p , .001 ) , concordant with the transcription - coupled repair function of the nucleotide excision repair complex ( fig 2b )  . 
on the basis of encouraging reported results in msi - high malignancies to immune checkpoint blockade , pembrolizumab ( 2 mg / kg intravenously every 3 weeks ) was initiated 1 month after diagnosis , using the recent us food and drug administration indication for msi - high malignancies to support insurance approval . after ve cycles of pembrolizumab , follow - up imaging demonstrated a considerable decrease in tumor bulk and resolution of leptomeningeal disease along the right pons and cerebellum ( figs 1e to 1h )  . 
the patient experienced resolution of the chronic cough and reported substantial improvement in the facial pain ( initially the pain required scheduled opioid medications , but they have now been discontinued without pain )  . 
mutation prole analysis of the corneal and conjunctival primary tumors , along with their parotid lymph node metastases ( met ) , was performed on identied somatic single nucleotide variants.19 ( a ) all four tumors show mutation patterns consistent with base excision repair deciency ( catalogue of somatic mutations in cancer mutation signature 7 )  . 
 ( b ) analysis of mutation signatures based on the transcribed gene strand shows a strong bias of c.t mutations on the untranscribed strand ( 1 , 683 v 348 mutations on the transcribed strand ) , consistent with the transcription - coupled nature of the nucleotide excision repair pathway . 
 ( c ) comparison and set overlap of somatic variants identied in four sequenced samples reveals two unrelated primary tumors ( corneal and conjunctival ) , each with unique metastases to the parotid lymph nodes . 
 steineck et al on clinical examutational analyses demonstrated that the ocular lesions had different mutations but a similar mutational burden compared with her metastatic tumor ( data supplement )  . 
mutations implicated in pd - 1 resistance , including wnt , were not identied in analysis of the patients tumors.21 - 23 topical uorouracil , which is efcacious in cutaneous scc associated with xp , was initiated in the affected eye , and no additional tumor progression was noted after 1 month of local treatment . discussion we report the case of a pediatric patient with xp who demonstrated long - term partial response of advanced cutaneous scc to pembrolizumab with development of no clinically signicant adverse effects . 
acknowledges the potential limitation of pd - 1 inhibitors for the treatment of scc involving immune - privileged sites , such as the cornea . xp represents a decit in dna nucleotide excision repair , resulting in sensitivity to uv radiation . 
loss of xpc ( or xpe ) is consistent with decient global genomic repair ( ggr ) but relatively preserved transcription - coupled repair ( tcr ) ; this contrasts with loss of xpa , xpb , or xpd , which results in a ggr - negative / tcr - negative phenotype.24 , 25 the tcrnegative / ggr - positive mutational signature of xpc is demonstrated in this patient with a greater burden of c.t mutations on the untranscribed strand ( fig 2b )  . 
the novel report of our patients mutational signature enriches our understanding of xp and further supports the potential efcacy of immune checkpoint blockade with pd - 1 inhibitors in the treatment of advanced scc among patients with xp . 
in addition , we were able to use molecular methods to demonstrate the coincidental development of two independent primary lesions with two paired metastatic lesions to better understand the origin of this patients metastatic disease . this report describes long - term sustained stable disease , including response of signicant burden of disease in the cns . 
of the existing published reports using pd - 1 inhibitors in patients with xp , the longest reported time to follow - up was 18 months , 16 with other studies describing therapy for no more than 1 year.5 , 15 , 17 our patients sustained response supports the use of pd - 1 inhibitors for long - term disease management in this setting . 
moreover , pd - 1 inhibitors have the potential to do this with minimal adverse effects , providing a quality - oflife benet , which is an important consideration for individuals with advanced cancer . our patients right corneal lesion demonstrated discordant poor response . 
the cornea is immune privileged26 and does not have t - cell immunosurveillance , potentially limiting the ability of immune checkpoint blockade to treat malignancies in the cornea and other immune - privileged sites , such as the testis . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . niklas krumm stock and other ownership interests : reference genomics andrew w . 
stacey honoraria : immunocore travel , accommodations , expenses : immunocore no other potential conicts of interest were reported . references kraemer kh , digiovanna jj : xeroderma pigmentosum , in adam mp , ardinger hh , pagon ra , et al ( eds ) : genereviews . 
seattle , wa , university of washington , 2003 bradford pt , goldstein am , tamura d , et al : cancer and neurologic degeneration in xeroderma pigmentosum : long term follow - up characterises the role of dna repair . 
maubec e , petrow p , scheer - senyarich i , et al : phase ii study of cetuximab as rst - line single - drug therapy in patients with unresectable squamous cell carcinoma of the skj clin oncol 29 : 3419 - 3426 , 2011 deinlein t , lax sf , schwarz t , et al : rapid response of metastatic cutaneous squamous cell carcinoma to pembrolizumab in a patient with xeroderma pigmentosum : case report and review of the literature . 
eur j cancer 83 : 99 - 102 , 2017 sumiyoshi m , soda h , sadanaga n , et al : alert regarding cisplatin - induced severe adverse events in cancer patients with xeroderma pigmentosuintern med 56 : 979 - 982 , 2017 7 . 
science 351 : 1463 - 1469 , 2016 rizvi na , hellmann md , snyder a , et al : cancer immunology : mutational landscape determines sensitivity to pd - 1 blockade in non - small cell lung cancer . science 348 : 124 - 128 , 2015 bauml j , seiwert ty , pster dg , et al : pembrolizumab for platinumand cetuximab - refractory head and neck cancer : results from a single - arm , phase ii study . j clin oncol 35 : 1542 - 1549 , 2017 10 . 
chang al , kim j , luciano r , et al : a case report of unresectable cutaneous squamous cell carcinoma responsive to pembrolizumab , a programmed cell death protein 1 inhibitor . 
stevenson ml , wang cq , abikhair m , et al : expression of programmed cell death ligand in cutaneous squamous cell carcinoma and treatment of locally advanced disease with pembrolizumab . 
salomon g , maza a , boulinguez s , et al : efcacy of anti - programmed cell death - 1 immunotherapy for skin carcinomas and melanoma metastases in a patient with xeroderma pigmentosubr j dermatol 178 : 1199 - 1203 , 2018 17 . 
hauschild a , eichstaedt j , m obus l , et al : regression of melanoma metastases and multiple non - melanoma skin cancers in xeroderma pigmentosum by the pd1 - antibody pembrolizumab . 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . 
kruizinga r , scherer - rath m , schilderman jb , et al : the life in sight application study ( lisa ) : design of a randomized controlled trial to assess the role of an assisted structured reection on life events and ultimate life goals to improve quality of life of cancer patients . 
adra n , einhorn lh , althouse sk , et al : phase ii trial of pembrolizumab in patients with platinum refractory germ - cell tumors : a hoosier cancer research network study gu14 - 206 . 
 steineck et al appendix molecular methods tumor and germline samples were processed , sequenced , and analyzed using the university of washington laboratory medicine uwoncoplex cancer gene panel ( university of washington , seattle , wa ) .18 single nucleotide variants and indels in targeted regions were called from aligned bam les using the genome analysis toolkit ( broad institute , cambridge , ma ) and the variant detection in massively parallel sequencing datavarscan . 
in this study , metex14 ( c.2899g.a ) was detected by targeted next - generation sequencing with memorial sloan kettering integrated mutation proling of actionable cancer targets ( msk - impact ) in a case of advanced lung adenocarcinoma driven by egfr l858r mutation , after 12.5 months of frontline egfrtyrosine kinase inhibitor ( tki ) treatment . 
interestingly , metex14 co - occurred with met amplication and egfr t790m at the time of progression , as revealed by digital polymerase chain reaction on cell - free dna ( but not conrmed on tumor tissue )  . 
earlier , we described a patient whose primary resection sample tested positive for both egfr l858r and metex14 ( c3028 + 1g.t ) , but not for met amplication , as assessed by next - generation sequencing.2 in the current study , although the patient did not respond to met - targeted therapy alone , a combination of crizotinib ( met - tki ) and osimertinib ( third - generation egfr - tki ) led to durable disease control.1 however , we believe that additional key points should be discussed in more detail . 
targeted sequencing did not assess unknown potential mechanisms of resistance . it would have been interesting to learn which other pathways were abnormally activated in this tumor , such as fas or components of the nf - b pathway that specically enhanced cell death induced by rstgeneration egfr - tki erlotinib and caused acquired resistance to third - generation egfr - tki rociletinib in egfr - mutant lung cancer cells.3 , 4 met amplication should be further investigated . 
two recent studies reported a response to a combination of osimertinib and crizotinib in patients with nonsmallcell lung cancer ( nsclc ) harboring egfr l858r , while a rebiopsy showed met amplication after disease progression on erlotinib.5 , 6 similarly , a dramatic response was achieved using crizotinib and erlotinib in a case of met amplication emerging in the setting of egfr l858r mutation , suggesting the potential role of erlotinib and crizotinib combination , 5 which was not tested in vitro . 
in this model , crizotinib monotherapy was unable to modulate cell growth and switch off the egfr downstream signaling . although the drugs were used at a low concentration and no analysis was performed to assess pharmacointeractions , 7 crizotinib restored sensitivity to logical osimertinib in both pc9 and h1975 metex14 models . mechanistically , it was shown that the combination inhibited activation of egfr , met , as well as downstream akt and erk.1 these ndings underline the effectiveness of different tki combinations in inhibition of multiple signaling cascades to overcome cancer cell resistance.8 in particular , met signaling plays a crucial role in driving egfr - tki resistance in oncogene - addicted nsclc , and met inhibition can be a successful strategy to recover sensitivity in cases of met aberrations . 
despite the striking clinical activity of the combination in the current study , there is often a large gap between preclinical evaluations of tki combinations and clinical outcome.9 thus , the identication of predictive biomarkers for response could be useful for proper selection of patients who would likely benet from the therapeutic combination . 
we recently identied p - her3 and p - pras40 as potential candidates to assess the synergy between erlotinib and crizotinib in vitro.10 erlotinib and crizotinib showed remarkable synergy in the ludlu squamous - cell lung cancer ( scc ) cell line , which does not harbor egfrsensitizing mutations , met amplication , or metex14 . interestingly , other investigated scc cell lines ( h1703 and skmes - 1 ) , which were also wild - type for egfr and met , reacted differently ( but still additive ) , suggesting a role for the differential expression of p - her3 and p - pras40 expression in this synergy . 
because we observed a synergistic effect of the combination treatment of erlotinib and crizotinib only in scc cells that showed concordant expression of p - her3 and p - pras40 , we assume that p - her3 and p - pras40 may be candidate biomarkers for effective egfr + met blockade in patients with scc.10 taking into account our ndings , other components of the egfr and met pathways , including p - her3 and p - pras40 , should be investigated in tissues obtained from patients receiving a combination of egfr - tki and met - tki . in conclusion , we are indebted to suzawa et al1 for their elegant study . 
 correspondence alessandro leonetti , md amsterdam umc , vu university medical center , cancer center amsterdam , amsterdam , the netherlands , and university hospital of parma , parma , italy marcello tiseo , md , phd university hospital of parma and university of parma , parma , italy christian rolfo , md , phd , mba university of maryland greenebaum comprehensive cancer center , baltimore , md nele van der steen , phd amsterdam umc , vu university medical center , cancer center amsterdam , amsterdam , the netherlands , and center for oncological research ( core ) , university of antwerp , wilrijk , belgium godefridus j . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . marcello tiseo consulting or advisory role : astrazeneca , bristol - myers squibb , msd , boehringer ingelheim , takeda research funding : astrazeneca christian rolfo consulting or advisory role : mylan speakers bureau : novartis , msd , boehringer ingelheim , guardant health travel , accommodations , expenses : astrazeneca godefridus j . 
peters consulting or advisory role : taiho pharmaceutical , clear creek bio , ellipses pharma research funding : rexahn pharmaceuticals ( inst ) travel , accommodations , expenses : rexahn pharmaceuticals , taiho pharmaceutical no other potential conicts of interest were reported . references suzawa k , ofn m , schoenfeld aj , et al : acquired met exon 14 alteration drives secondary resistance to epidermal growth factor receptor tyrosine kinase inhibitor in egfr - mutated lung cancer . 
clin lung cancer 19 : 35 - 41 , 2018 bivona tg , hieronymus h , parker j , et al : fas and nf - b signalling modulate dependence of lung cancers on mutant egfr . 
nature 471 : 523 - 526 , 2011 galvani e , sun j , leon lg , et al : nf - b drives acquired resistance to a novel mutant - selective egfr inhibitor . 
oncotarget 6 : 42717 - 42732 , 2015 giroux - leprieur e , dumenil c , chinet t : combination of crizotinib and osimertinib or erlotinib might overcome met - mediated resistance to egfr tyrosine kinase inhibitor in egfr - mutated adenocarcinoma . 
j thorac oncol 13 : e232 - e234 , 2018 zhu vw , schrock ab , ali sm , et al : differential response to a combination of full - dose osimertinib and crizotinib in a patient with egfr - mutant nonlung cancer and emergent met amplication . 
lung cancer small cell ( auckl ) 10 : 21 - 26 , 2019 bijnsdorp iv , giovannetti e , peters gj : analysis of drug interactions . methods mol biol 731 : 421 - 434 , 2011 tong cws , wu wkk , loong hhf , et al : drug combination approach to overcome resistance to egfr tyrosine kinase inhibitors in lung cancer . cancer lett 405 : 100 - 110 , 2017 yang z , tam ky : combination strategies using egfr - tki in nsclc therapy : learning from the gap between pre - clinical results and clinical outcomes . 
van der steen n , leonetti a , keller k , et al : decrease in phospho - pras40 plays a role in the synergy between erlotinib and crizotinib in an egfr and cmet wild - type squamous non - small cell lung cancer cell line . 
de moor author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license corresponding author : andrew n . 
freedman , phd , epidemiology and genomics research program , division of ( continued ) purpose there are no nationally representative data on oncologists use of next - generation sequencing ( ngs ) testing in practice . 
the purpose of this study was to investigate how oncologists in the united states use ngs tests to evaluate patients with cancer and to inform treatment recommendations . methods the study used data from the national survey of precision medicine in cancer treatment , which was mailed to a nationally representative sample of oncologists in 2017 ( n = 1 , 281 ; cooperation rate = 38% )  . 
of these oncologists , 34.0% used them often to guide treatment decisions for patients with advanced refractory disease , 29.1% to determine eligibility for clinical trials , and 17.5% to decide on off - label use of food and drug administrationapproved drugs . 
oncologists younger than 50 years of age , holding a faculty appointment , having genomics training , seeing more than 50 unique patients per month , and having access to a molecular tumor board were more likely to use ngs tests . conclusion in 2017 , most oncologists in the united states were using ngs tests to guide treatment decisions for their patients . 
multimarker panels also include dna and rna analysis through next - generation sequencing ( ngs ) technologies , including custom panels that profile multiple actionable driver genes and tumor characteristics that may guide the selection of targeted therapies . despite advances in precision oncology , comparatively little empirical research is available that assesses the expectations and experiences of oncologists in the united states who may use these genomic tools to care for patients with cancer . 
to date , most studies have evaluated physicians experiences with specific genomic tests for individual gene mutations.3 - 5 studies that have attempted to assess providers experiences with custom ngs tumor panels6 - 9 have focused on intended rather than actual use . 
furthermore , previous studies of physicians use of ngs tests were on the basis of small samples and were conducted in tertiary referral centers ; as a result , their findings may not represent how oncology is practiced in the united states . 
currently , there are no nationally representative data describing oncologists awareness , knowledge , and use of ngs testing to inform patient care , especially in community practice settings . with the increasing application of precision oncology , understanding how oncologists use genomic tests in their practice and the factors that affect their use is essential to ensure that patients who can benefit receive appropriate testing and follow - up . 
the purpose of this study was to investigate how oncologists in the united states use ngs tests to evaluate patients with cancer and inform treatment recommendations . methods data source this study used data from the national survey of precision medicine in cancer treatment , a nationally representative survey of hematologists , hematologists / oncologists , and oncologists sponsored by the national cancer institute ( nci ) , the national human genomic research institute , and the american cancer society . 
 of the remaining 3 , 378 oncologists with verified contact information , 1 , 281 completed the survey ( cooperation rate = 38%10 )  . a survey packet containing a personalized invitation letter from the nci , an endorsement letter from asco , a pen with the studys name printed on it , a self - administered paper questionnaire , and a business reply envelope was mailed to eligible oncologists . 
participants received a $50 honorarium for completing the survey . the questionnaire ( data supplement ) took 20 minutes to complete on average , and data were collected from february through may of 2017 . 
information was ascertained about oncologists demographics , training , academic affiliation , specialty , and patient volume , and their practice characteristics , including practice setting , structure , and resources to support genomic testing . 
 information about oncologists use of commercially available multimarker tumor panels and noncommercial tumor panels performed at academic medical centers was collected , as were data on the clinical scenarios in which ngs test were used . 
because of differences in how survey questions were worded ( eg , some explicitly stated the exclusion of oncotype dx ) , sensitivity analyses were conducted to examine whether oncologists who reported using other gene expression tests , including the breast cancer index , mammaprint , prosigna , and / or myplan lung cancer , differed in their use of ngs tests from those who did not use these gene expression tests . 
the survey weights were applied in all analyses of the data and provide statistical adjustment so that respondents are representative of the population of practicing oncologists in the united states . each oncologist was classified as a user of ngs tests if he or she reported using at least one specific multimarker panel with ngs technologies profiling multiple actionable driver genes for guiding treatment decisions in the past 12 months . 
multivariable models were estimated to examine the independent association between each physician demographic and practice characteristic and the likelihood of ngs testing , when adjusting for the other characteristics in the model . 
all analyses were conducted using sudaan release 11.0.1 ( rti international , research triangle park , nc )  . results characteristics of survey respondents characteristics of the 1 , 281 oncologists who completed the survey are listed in table 1 . 
 more than one half of respondents ( 56.9% ) spent at least 90% of their time in patient care and almost one half ( 49.3% ) spent less than 10% of their time teaching ( data not shown )  . prevalence of ngs test use and predictors of test use to guide treatment decisions overall , 75.6% of oncologists reported using ngs tests in the past 12 months to guide treatment decisions ; use differed according to the physicians demographic and practice characteristics ( table 2 )  . 
oncologists who treated only patients with hematologic malignancies were less likely to use ngs tests than were oncologists who treated both solid and hematologic malignancies and those who only treated patients with solid tumors . 
oncologists who held a faculty appointment , had some training in genomics , or were part of a practice that had a molecular tumor board were more likely to use ngs tests than were those who did not have these characteristics . 
in addition , those who treated fewer than 50 patients with cancer per month were more likely to use ngs tests than were oncologists who treated more than 50 patients with cancer per month . 
the likelihood of ngs use was not statistically significantly associated with other provider and practice characteristics assessed . in this survey , oncologists in the united states were asked how often they used 11 commercially available ngs tests or a noncommercial ngs test during the past 12 months ( fig 1 )  . 
moreover , among oncologists who ordered any of these ngs tests ( n = 959 ) , 28.2% ordered one test , 31.7% ordered two tests , 23.3% ordered three tests , and 16.7% ordered four or more tests in the past 12 months . ngs test use practice patterns oncologists use of ngs test results varied by clinical presentation ( fig 2 )  . 
characteristics of oncologist respondents in the united states to the 2017 national survey of precision medicine in cancer treatment ( continued ) total ( n = 1 , 281 ) unweighted percentage ( % ) * weighted percentage ( % ) * characteristic no . 
we found that oncologists who used the breast cancer index , mammaprint , prosigna , and / or myplan lung cancer did not differ in the way they answered these questions in nine out of 10 comparisons . 
when analyses were restricted to oncologists who treated a high volume of patients with breast cancer , there were no differences in test use between oncologists who used the breast cancer index , mammaprint , and prosigna and those who did not ( data not shown )  . respondents were explicitly directed to exclude oncotype dx when answering questions about ngs testing for different clinical purposes . 
use of ngs testing during the past 12 months among oncologists in the united states , by physician demographics and practice characteristics ( continued ) total ( n = 1 , 281 ) ngs user ( unadjusted % ) ngs user ( adjusted % ) 95% ci adjusted or ( 95% ci ) characteristic sees patients at academic center or medical school no . 
twenty - five percent ( n = 319 ) indicated that they referred their patients to another location or provider for ngs testing ; among these oncologists , 84.4% ( n = 257 ) referred to an academic medical center , 82.1% ( n = 240 ) to a clinical trial , and 18.2% ( n = 51 ) to an oncologist outside of their practice ( data not shown )  . discussion in this nationally representative study of 1 , 281 oncologists , we examined how ngs tests are currently used in clinical practice and whether use is influenced by physician and practice characteristics . 
 initial diagnosis rare cancers advanced refractory disease unknown origin never rarely sometimes often reported using ngs test results to guide patient care , and the use of ngs tests differed by oncologists demographic and practice characteristics . 
 for example , younger oncologists were more likely to be ngs test users , suggesting that they may have had more recent training in genomic testing or that they are more receptive to the incorporation of ngs testing in their practice . 
 having a faculty appointment and access to a molecular tumor board were also associated with ngs test use , perhaps reflecting greater access to in - house ngs tests in academic settings or more involvement in clinical research . 
 not surprisingly , oncologists who treated only patients with hematologic malignancies were less likely to use ngs tests than were oncologists who treated both solid and hematologic malignancies or those who treated only patients with solid tumors , suggesting that ngs tests may be ordered reflexively by pathologists rather than by oncologists . 
use of next generation sequencing tests by clinical purpose during the past 12 months among oncologists in the united states . molecular testing for patients with hematologic malignancies . oncologists reported using ngs most often for patients with advanced refractory disease , but also used these tests often for patients diagnosed with a rare cancer or cancers of unknown origin and / or for patients with an initial diagnosis of cancer . 
these results may reflect oncologists use of ngs testing to inform treatment strategies when established therapies have failed or when there is uncertainty about the usefulness of existing treatment guidelines for less common clinical situations . 
with the recent approval of multiple therapeutic agents targeting specific driver mutations , oncologists may send a patients tumors for sequencing with the hope of identifying treatments that are potentially efficacious for their patients particular molecular tumor subtype . 
in our survey , more than one third of oncologists reported using ngs test results often to guide the use of an fda approved therapy . advances in precision oncology pose challenges for oncologists . 
at the time of the survey in may 2017 , nonsmall - cell lung cancer was the only cancer type for which there was a consensus recommendation for ngs use.13 furthermore , no professional group other than the national comprehensive cancer network has yet issued evidence - based guidelines recommending the use of ngs testing . 
 however , as the number of single - gene or focused - indication ( eg , microsatellite instability ) tests that are components of the standardized evaluation of common malignancies has grown , oncologists are increasingly faced with decisions about whether to order several targeted tests or a single ngs panel . there has also been an effort by pharmaceutical companies to develop tissue - agnostic cancer drugs that target a specific genetic marker independent of tumor type.14 given the prospect of tissue - agnostic labeling , the use of ngs will only grow , and in the absence of clinical guidelines informing ngs use , it is likely that many providers will experience uncertainty about how to clearly integrate this information into clinical care decisions . 
 treatment recommendations , suggesting that oncologists are already confronted with a large volume of genomic information that they must interpret . that ngs test results are frequently ambiguous presents another challenge for oncologists . 
in addition , 25% indicated that they referred patients to other providers for ngs testing , possibly suggesting a lack of expertise or resources for ordering and interpreting ngs tests . 
several academic and commercial groups have responded to this need , developing online decision support resources for genomic medicine , such as personalized cancer therapy , my cancer genome , and oncokb , with the goal of providing an accessible platform to oncologists.15 however , more work is needed to ensure that patients who can benefit from these new technologies receive appropriate testing and follow - up . a third challenge for oncologists is the lack of clinical usefulness data for many of the available ngs tests . 
two major , ongoing clinical trials , ( national cancer institute nci - match molecular analysis for therapy choice ) , 16 and pediatric match ( national cancer institute childrens oncology group pediatric match trial ) , will generate evidence to establish clinical usefulness to fill some of these gaps . 
furthermore , ascos targeted agent and profiling utilization registry ( tapur ) study17 and cureone ( formerly called med - c ) are building registries of ngs testing data to enhance informed treatment recommendations difficulty in interpreting results never / rarely sometimes often understanding of how testing is being used and its impact on patient outcomes.18 insurers are also recognizing the cost efficiencies of ngs panel testing as opposed to multiple single - gene testing for specific cancer - site indications but are grappling with a lack of clinical usefulness data for testing cancers broadly . 
 effective march 16 , 2018 , the centers for medicare & medicaid services has allowed non fda - approved assays run in clinical laboratory improvement amendmentscertified laboratories to be reimbursed , dependent on decisions made by local medicare administrative contractors.19 it is unclear whether and under what circumstances commercial private payers will decide to reimburse for ngs testing broadly for cancer . 
our findings offer an important baseline that could be used to evaluate the impact of these coverage decisions on ngs test use because our data were collected before implementation of these key changes in coverage . our study has several limitations . 
first , the cooperation rate was lower than that of previous surveys of physicians on the topic of genomic and genetic test use , 7 , 20 and responders may have differed from nonresponders in terms of their genomic testing practices and other characteristics such as academic affiliation . 
however , respondents are representative of the population of practicing oncologists in the united states in terms of age , sex , and geographic location on the basis of statistical adjustment for nonresponse using data available on the survey 's sample frame . another limitation is that we were unable to assess how oncologists use the tests in specific clinical situations and for which cancer types they are ordering these tests . 
however , these limitations are offset by several strengths of the study , including the nationally representative sample of practicing oncologists in a wide variety of practice settings and the large sample size , which allowed us to analyze multiple factors associated with ngs use and to examine a variety of practice patterns . the majority of oncologists in the united states use ngs tests to guide patient care , even in the absence of evidence - based practice guidelines . 
schilsky research funding : astrazeneca ( inst ) , bayer ag ( inst ) , bristol - myers squibb ( inst ) , genentech / roche ( inst ) , eli lilly ( inst ) , merck ( inst ) , pfizer ( inst ) deborah schrag consulting or advisory role : journal of the american medical association research funding : pfizer other relationship : journal of the american medical association naoko i . 
simonds stock and other ownership interests : cvs health ( i ) , walgreens boots alliance , anthem foundation , anthem foundation ( i ) , celgene ( i ) , cvs health , johnson & johnson , johnson & johnson ( i ) , walgreens boots alliance ( i ) , labcorp , labcorp ( i ) , valeant pharmaceuticals international , valeant pharmaceuticals international ( i ) , endo pharmaceuticals ( i ) , aetna ( i ) helmneh m . 
miller fa , hayeems rz , bytautas jp , et al : testing personalized medicine : patient and physician expectations of next - generation genomic sequencing in late - stage cancer care . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental findings : results from the canseq study . 
johnson lm , valdez jm , quinn ea , et al : integrating next - generation sequencing into pediatric oncology practice : an assessment of physician confidence and understanding of clinical genomics . 
 appendix physician characteristics included age , sex , race or ethnicity , faculty appointment , training in genomic testing ( eg , instruction throughout residency and / or fellowship , professional lectures or seminars , symposiums , conferences , or continuing medical education )  . 
practice characteristics , such as region , urbanicity , type of practice ( solo , single specialty group , multispecialty group , other ) , academic affiliation , and number of unique patients with cancer seen per month were also collected . 
in addition , questions were asked about whether the oncologists practice setting has a genomic or molecular tumor board , policies for genomic testing use , and / or an electronic medical record that provides alerts when a genomic test is recommended . 
an oncologists specialty was defined using information on type ( s ) of patients with cancer seen : only patients with solid tumors , only those with hematologic malignancies , or both . 
age and demographic characteristics other than race or ethnicity were obtained from the american medical association masterfile . an oncologists was classified as a user of next - generation sequencing ( ngs ) tests if he or she reported use , in the past 12 months , of specific multimarker panels with ngs technologies profiling multiple actionable driver genes used to guide treatment decisions . 
the following tests were included in this definition : cancerselect or cancer complete , caris molecular intelligence or target now , cgi complete , foundationone , foundationoneheme , foundationact , gps cancer , guardant360 , omniseq comprehensive , onkosight tumor panels , solid tumor mutation panel ( arup laboratories ) , and noncommercial tumor panels . 
multimarker tests that use gene - expression profiling ( eg , oncotype dx for breast cancer ) , primarily used to predict prognosis and / or the likelihood of recurrence , were not classified as ngs tests . 
neil hayes , md , lineberger comprehensive cancer center , university of north carolina at chapel hill , cb #7295 , 125 mason farm road , chapel hill , nc 27599 ; e - mail : hayes@ med.unc.edu. purpose a 73 - year - old woman with metastatic colon cancer experienced a complete response to chemotherapy with dose - intensified irinotecan that has been durable for 5 years . 
we sequenced her tumor and germ line dna and looked for similar patterns in publicly available genomic data from patients with colorectal cancer . patients and methods tumor dna was obtained from a biopsy before therapy , and germ line dna was obtained from blood . 
the somatic mutation and clinical annotation data files from the colon ( n = 461 ) and rectal ( n = 171 ) adenocarcinoma data sets were downloaded from the cancer genome atlas data portal and analyzed for patterns of mutations and clinical outcomes in patients with poleand / or pold1mutated tumors . results the pattern of alterations included apc biallelic inactivation and microsatellite instability high ( msi - h ) phenotype , with somatic inactivation of mlh1 and hypermutation ( estimated mutation rate > 200 per megabase )  . 
colonoscopy showed a cecal mass , and biopsy showed invasive adenocarcinoma . she had blood transfusions , with an appropriate increase in her hemoglobher medical history was significant for back surgery , depression , diverticulitis , hyperlipidemia , hypothyroidism , and osteoporosis . 
the objective of this study was to define the maximum - tolerated dose of irinotecan in folfiri plus bevacizumab as firstline therapy in metastatic colorectal cancer , with dosing of irinotecan based on ugt1a1 genotype.1 her ugt1a1 genotype was * 1 / * 28 , and she was assigned to receive irinotecan at a dose of 310 mg / m2 intravenously ( iv ) , 72% higher than the standard dose of 180 mg / m2 . 
she received standard doses of the other drugs : fu 400 mg / m2 iv bolus , then 2 , 400 mg / m2 iv over 46 hours ; leucovorin 200 mg / m2 iv ; and bevacizumab 5 mg / kg iv . 
dna from tumor and normal samples were processed through the usual lccc1108 production pipeline of targeted capture sequencing as described previously , with a modification for small - volume input of less than 1 mg of input tumor dna.3 briefly , tumor and normal samples were sequenced using commercial protocols ( agilent sureselect custom targeted panel of approximately 250 genes ; santa clara , ca ) and the illumina hiseq platform ( san diego , ca ) in either singleor paired - end format of 75 and 100 bases per end . average depth of coverage for target sequences was 665 reads in the tumor sample and 293 reads in the germline sample . 
whole - exome sequencing was performed , and the identical informatics pipeline was applied . focal validation of the pold1 mutation was performed on the whole - genomeamplified dna using sanger sequencing . 
primers were designed to flank exons 18 and 26 of pold1 and exon 6 of pole : pold1 exon 18 : 59 - gcatgattctctccccgacag - 39 ( forward ) and 59 - ctgccctgggcccatctca - 39 ( reverse ) ; pold1 exon 26 : 59 - ccgggagtctgagctgtatc - 39 ( forward ) and 59 - cagggtcgggacatggca - 39 ( reverse ) ; and pole exon 6 : 59 - ctcttgaaccaatgagcgtga - 39 ( forward ) and 59 - gtcgttctgaaccgctgatg - 39 ( reverse )  . 
polymerase chain reaction amplification and sanger sequencing were performed using a previously validated protocol within the unc hospitals molecular genetics laboratory ( chapel hill , nc )  . the somatic mutation and clinical annotation data files from the colon ( n = 461 ) and rectal ( n = 171 ) adenocarcinoma data sets were downloaded from the cancer genoma atlas ( tcga ) data portal.4 of these 632 patient cases , 430 ( colon , n = 330 ; rectum , n = 99 ; unknown , n = 1 ) contained both somatic mutation and clinical annotation data points . 
select protein - coding mutations in genes previously associated with colon cancer are listed in table 1 . review of the mutant allele fractions of apc and pik3ca was potentially informative as to the nature of the tumor genome . 
protein - coding mutations selected from 1 , 192 somatic mutations identified ; organized top to bottom by maf . abbreviations : cosmic , catalogue of somatic mutations in cancer ; maf , mean allelic frequency ; na , not applicable ; q , 210 3 log10 ( probability of sequencing error )  . * q score not defined for this deletion event . mutation in 1489 followed by genome doubling , resulting in two mutant alleles and two wild - type alleles . 
this event was followed by independent separate mutations , resulting in 25% mutant allele fractions and complete loss of functional apc . the mutation in pik3ca , as well as most of the more than 1 , 000 mutations , occurred after genome doubling , because the most common mutant allele fractions were approximately 25% . tumor evolution in this manner suggests a mechanism by which a cell with so many mutations might remain viable by offering four alleles to retain at least one functional form of the gene . despite the large number of mutations , the cancer genome remained structurally intact ( fig 3 )  . 
genomes without such copy - number changes are uncommon , with nearly every colon cancer demonstrating amplifications or deletions.7 the only evidence of genome instability in this patient case involved low - level gains of chromosomes 17 and 19 and perhaps loss of a portion of chromosome 13 . 
if the supposition of a tetraploid genome is correct , these events might best be explained by loss or gain of an additional chromosome from an average copy of four alleles . 
interestingly , it has been suggested that tumors that retain wild - type tp53 and / or are of the msi - h phenotype are more likely to have a stable genome configuration , such as we saw in our patient case.8 , 9 in our patient case , despite the large number of mutations , no evidence for tp53 mutation was detected . 
this is also consistent with the observation that the frequency of tp53 mutations is lower in msi - h tumors.10 although the msi - h phenotype with hypermutation in association with mlh1 alteration is an established entity , 10 the overall number of mutations in this patient case was particularly striking , leading us to ask whether any additional alterations might play a role . 
specifically , we queried whether previously reported mutations in pole might be present.8 because pole was not included in the original hybrid capture set , the remaining dna was submitted for wholeexome sequencing , and no pole mutation was detected . 
we then looked for associations of pole and pold1 mutations with both overall mutation rate and the pattern of hyper - indel hypermutation seen in our patient case ( fig 5a )  . 
by contrast , cancers with pold1 mutations were not associated with ultra - high mutation rates , although the median number of nonsilent mutations was much higher ( 893 mutations ) than the median for the entire data set ( 134 mutations )  . 
cancers with pole and / or pold1 mutations generally were hypermutated , with only seven patient cases ( 1.6% ) having fewer than 200 nonsilent somatic mutations . we considered the possibility that , because the set of samples being considered included those with the highest mutation rates , mutations of pold1 might simply occur by random chance . 
further arguing against chance alone , we noted that pold1 mutations were not observed in any of the patient cases of pole ultramutated tumors but rather uniquely in patients with msi - h phenotype with high numbers of indels . 
lollipop plots showing mutations in ( a ) pole and ( b ) pold1 from the cancer genome atlas ( tcga ) , as well as ( b ) the mutation in pold1 from our patient . 
this gene model includes important functional domains of the gene : dna_pol_b_exo1 , dna polymerase beta exonuclease 1 domain ; dna_pol_b , dna polymerase , family b domain ; duf1744 , domain of unknown function found on epsilon catalytic subunit of dna polymerase ; zf - , zf - c4pol ( c4 - type zinc - finger of dna polymerase delta )  . 
all domains were annotated from the pfam database . msi - h , microsatellite instability high . dna_pol_b_exo1 dna_pol_b duf1744 1200 1600 2000 2286 aa dna_pol_b_exo1 dna_pol_b zf - .. reported mutation 1000 1107 aa missense mutation nonsense mutation nonhypermutated > 2 , 000 mutations hyper indels msi - h because pold1 mutations were associated with msi - h phenotype , we considered the possibility that these mutations were a passenger event confined to the biology of msi - h cancers . 
comparison of indel rate in msi - h cancers on the basis of pold1 mutation status revealed that msi - h cancers with pold1 mutations exhibited approximately 60% more indels than msi - h cancers without pold1 mutations ( p , .03 ; fig 5b )  . 
however , polehypermutated cancers exhibited approximately 50% fewer indels than hypermutated cancers without pole mutations ( p , .001 ; fig 5c )  . discussion crs to chemotherapy have been described previously in patients with colorectal cancer . 
a recent meta - analysis of chemotherapy plus bevacizumab reported a cr rate of 2.4% based on aggregate data from seven randomized controlled trials.13 because these responses are infrequent , and many of them occurred in the era before genomic profiling of tumors , the links between tumor genomics and exceptional unclear . 
having observed a cr to folfiri and bevacizumab that has been durable for 5 years in the patient case presented here , sequencing of tumor and germline dna was undertaken to search for alterations associated with this exceptional response . 
msi - h tumors typically had hypermethylation and mlh1 silencing , whereas hypermutated tumors without msi - h typically had somatic mutations in one or more mismatchrepair genes and / or pole . 
right - sided colon cancers were recently reported to be associated with worse prognosis compared with left - sided colon cancers in a systematic review and metaanalysis , 14 but it is not clear whether the same would be true for hypermutated right - sided colon cancers . dna polymerases e ( pole ) and d ( pold1 ) are the two main enzymes involved in human dna replication . 
germline and somatic mutations in the exonuclease ( proofreading ) domains of pole and pold1 are associated with ultramutated colorectal and endometrial cancers.12 , 15 whole - genome sequencing in our patient case showed a hypermutated ( but not ultramutated ) phenotype in this right - sided tumor with many indels including a codon deletion of mlh1 , so the decision was made to pursue whole - exome sequencing to search for additional mutations in pole or pold1 . 
tumors with somatic mutations in pole ( blue ) , pold1 ( gold ) , or both pole and pold1 ( gray ) are distinguished from tumors without pole or pold1 mutations ( red )  . ( b ) indels in pold1mutant versus wild - type ( wt ) tumors with microsatellite instability high ( msi - h ) phenotype from tcga . 
number of indel was calculated for the 67 msi - h tumors from the colorectal tcga data set . msi - h tumors that also had pold1 somatic mutations exhibited more indels as compared with msi - h tumors without pold1 somatic mutations ( mean pold1 - mutant indels , n = 230 ; mean pold1 wt indels , n = 144 )  . 
 ( c ) indels among hypermutated ( n = 50 ) , nonhypermutated ( n = 356 ) , and polehypermutated ( n = 24 ) tumors from tcga ( total , n = 430 ; mean hypermutated indels , n = 176 ; mean nonhypermutated indels , n = 6 ; mean polehypermutated indels , n = 91 )  . 
of indels pold1 mutant 7 , 000 6 , 000 5 , 000 4 , 000 3 , 000 2 , 000 1 , 000 * p < .001 analysis of tcga confirmed that the observed phenotype was similar to other tumors with pold1 mutations . 
to our knowledge , this is a pattern that has not previously been reported in the literature . two previous studies have attempted to relate pole mutations to colorectal cancer outcomes . in a population - based cohort with microsatellitestable stage i to iv colorectal cancer , stenzinger et al16 reported a trend toward shorter survival for patients with pole mutations compared with their counterparts without pole mutations . along the same lines , there was a statistically significantly increased mortality for patients with stage iii to iv colorectal cancer receiving chemotherapy with pole mutations compared with their counterparts without pole mutations.16 in contrast , domingo et al17 recently reported that pole mutations were associated with a lower risk of recurrence compared with microsatellitestable stage ii to iii colorectal cancers , with correlative data suggesting that these tumors were more immunogenic . 
rizvi et al18 showed that higher nonsynonymous mutation burden was associated with markers of immunogenicity and improved outcomes with programmed death - 1 blockade in nonsmall - cell lung cancer . 
in our analyses of data from tcga , there were no statistically significant differences in survival based on overall mutation status , pole mutation status , pold1 mutation status , or combined pole and pold1 mutation status ( appendix fig a1 )  . an important limitation of this study is that it was impossible to isolate the genomic alterations most important in this patients exceptional response . 
 mutation burden and immunogenicity , 18 it is also possible that chemotherapy induced an endogenous immune response to a variety of neoantigens in this patients cancer . in conclusion , an exceptional response in a patient with metastatic colorectal cancer to folfiri plus bevacizumab led us to identify a somatic mutation in pold1 . 
grilley - olson consulting or advisory role : sanofi research funding : bayer , novartis ( inst ) , peregrine pharmaceuticals ( inst ) , nanocarrier ( inst ) , genentech ( inst ) , seattle genetics ( inst ) , medimmune ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) xiaobei zhao no relationship to disclose stergios j . 
moschos consulting or advisory role : merck sharp & dohme , amgen , paometheus , castle biosciences research funding : merck sharp & dohme , pharmacyclics , amgen , genentech / roche travel , accommodations , expenses : bristol - myers squibb , merck sharp & dohme , novartis blase n . 
neil hayes leadership : genecentric stock and other ownership interests : genecentric consulting or advisory role : genecentric patents , royalties , other intellectual property : i hold several diagnostic patents or pending patents in the area of solid tumor diagnostics federico innocenti patents , royalties , other intellectual property : royalties from the mayo foundation on the ugt1a1 testing acknowledgment we thank the patient for her enthusiasm in participating in the clinical trial and subsequent correlative studies . 
neil hayes , and federico innocenti , university of north carolina at chapel hill , chapel hill , nc ; and elena marangon , bianca posocco , and guiseppe toffoli , centro di riferimento oncologico , aviano , italy . supported by national cancer institute award no . 
therasse p , arbuck sg , eisenhauer ea , et al : new guidelines to evaluate the response to treatment in solid tumors : european organisation for research and treatment of cancer , national cancer institute of the united states , national cancer institute of canada . 
zhao x , wang a , walter v , et al : combined targeted dna sequencing in non - small cell lung cancer ( nsclc ) using uncseq and ngscopy , and rna sequencing using uncqer for the detection of genetic aberrations in nsclc . plos one 10 : e0129280 , 2015 4 . 
westra jl , boven lg , van der vlies p , et al : a substantial proportion of microsatellite - unstable colon tumors carry tp53 mutations while not showing chromosomal instability . 
mertz tm , sharma s , chabes a , et al : colon cancer - associated mutator dna polymerase d variant causes expansion of dntp pools increasing its own infidelity . 
zhang g , zhou x , lin c : efficacy of chemotherapy plus bevacizumab as first - line therapy in patients with metastatic colorectal cancer : a meta - analysis and up - date . 
petrelli f , tomasello g , borgonovo k , et al : prognostic survival associated with left - sided vs right - sided colon cancer : a systematic review and meta - analysis . 
domingo e , freeman - mills l , rayner e , et al : somatic pole proofreading domain mutation , immune response , and prognosis in colorectal cancer : a retrospective , pooled biomarker study . 
rizvi na , hellmann md , snyder a , et al : cancer immunology : mutational landscape determines sensitivity to pd - 1 blockade in non - small cell lung cancer . 
bertagnolli mm , redston m , compton cc , et al : microsatellite instability and loss of heterozygosity at chromosomal location 18q : prospective evaluation of biomarkers for stages ii and iii colon cancera study of calgb 9581 and 89803 . 
rmer mu , jensen nf , nielsen sl , et al : top1 gene copy numbers in colorectal cancer samples and cell lines and their association to in vitro drug sensitivity . 
 genomic assessment of bloodderived circulating tumor dna in patients with colorectal cancers : correlation with tissue sequencing , therapeutic response , and survival purpose genomic alterations in blood - derived circulating tumor dna ( ctdna ) from patients with colorectal cancers were correlated with clinical outcomes . patients and methods next - generation sequencing of ctdna ( 54to 73 - gene panel ) was performed in 94 patients with colorectal cancer . results most patients ( 96% ) had metastatic or recurrent disease at the time of blood draw . 
altogether , 74 patients ( 79% ) had one or more nonsynonymous alterations , 69 ( 73% ) had one or more potentially actionable alterations , and 61 ( 65% ) had an alteration actionable by a drug approved by the us food and drug administration ( on or off label )  . 
ctdna of 5% or more from blood tests as well as egfr and erbb2 ( her2 ) nonsynonymous alterations correlated with worse survival ( but only erbb2 remained significant in multivariable analysis )  . 
globally , there were 1.4 million new cases and 693 , 900 deaths in 2012 , with an increase in incidence and mortality rates in developing countries.1 , 2 at diagnosis , approximately 20% of patients have distant metastatic disease.3 for decades , systemic therapy used fluorouracil as the main active agent . 
addition of irinotecan and oxaliplatin , as well as the recently developed inhibitors that target vegf ( bevacizumab , aflibercept , and regorafenib ) and egfr ( cetuximab and panitumumab ) , have markedly improved the outcome of patients with metastatic colorectal cancer . 
however , prognosis remains poor ( median progression - free survival [ pfs ] , 10 months ; median overall survival [ os ] , 19 to 28 months ; 5 - year survival , 10%4 , 5 )  . 
 there is an unmet need to better understand the clinically relevant biology of colorectal cancer . the molecular characteristics of colorectal cancer are better understood because of advances in next - generation sequencing ( ngs ) technology.6 categorizing patients on the basis of their underlying molecular features has been proposed ( ie , consensus molecular subtypes ) , 7 and several genomic markers are now routinely used in the clinic to guide treatment . 
examples of genomically guided us food and drug administration ( fda ) approved therapies include anti - egfr agents ( cetuximab and panitumumab ) among patients with wild - type ras8 - 10 and pembrolizumab ( anti - programmed cell death protein 1 antibody ) for microsatellite instability - high or mismatch repairdeficient colorectal cancer.11 in additon , adding vemurafenib ( braf inhibitor ) to irinotecan and cetuximab demonstrated better clinical outcome among patients with brafv600mutated colorectal cancer.12 however , despite the recent progress in targeted therapy approaches , more than 50% of patients do not respond to the aforementioned regimens , and an increased understanding of the molecular underpinnings of the disease is needed . 
the study followed the guidelines of the university of california , san diego , internal review board , the declaration of helsinki for the predict study ( nct02478931 ; profile related evidence determining individualized cancer therapy ) , and any investigational therapy for which the patients gave consent . sequencing , concordance rate , matched therapy , and actionability ctdna sequencing was performed by guardant health and has been previously described ( data supplement ) .16 , 23 , 24 overall , 76 ( 81% ) of 94 patients had ngs performed on tumor tissue using the foundationone assay . 
the methods have been previously described ( data supplement ) .25 tissue ngs and plasma ctdna tests were compared by using the kappa statistic ( data supplement ) .26 we retrospectively analyzed the treatments given after ctdna testing and compared the clinical outcomes among patients who received matched and unmatched therapies ( data supplement ) .27 statistical analysis statistical analysis was performed by m.c.s. 
pfs and os were analyzed by using the kaplan - meier method28 and the logrank test ( univariable analysis ) ; a cox regression model ( multivariable analysis ) was used to compare variables . 
among the 74 patients with one or more nonsynonymous ctdna alterations , 59 ( 79.7% ) had distinct gene alteration portfolios ; 15 patients ( 20.3% ) had similar genomic alteration portfolios ( when alterations were considered at the gene level only , irrespective of the specific variant )  . 
this was the case only when patients had a small number of alterations ( three or fewer ) and included mostly the three genes with the most frequent alterations : tp53 , kras , and apc ( fig 1b )  . 
the other altered genes in our population ( fewer than five patients had the alteration ) were abl1 , akt1 , alk , araf , atm , brca1 , ccnd1 , ccnd2 , ccne1 , cdh1 , cdk6 , cdkn2a , ctnnb1 , esr1 , fgfr3 , gnaq , gnas , hras , jak3 , kit , map2k1 , mlh1 , mtor , notch1 , nras , pten , raf1 , rb1 , ret , rhoa , rit1 , ros1 , sdk6 , smo , stk11 , vhl . 
alterations of unknown significance ( variant of unknown significance ; vuss ) versus characterized mutations ( indels , amplifications , fusions , and single nucleotide variant ( snv ) point mutations ) were considered at the variant level . 
we did not observe a difference in the concordance rate when the time interval between the blood draw and tissue biopsy were taken into consideration ( a cutoff of 6 months was used because it was the median time interval )  . 
although apc alterations seemed to be detected more frequently in the tissue than in the plasma ( 22 patients were positive in both tests , 27 patients were positive in tissue only , and one patient was positive in plasma only ) , braf alterations seemed to be detected more frequently in the ctdna test ( eight patients were positive in both tests , two were positive in tissue only , and nine were positive in plasma only )  . 
in contrast , braf amplification was seen only with ctdna testing ( n = 8 )  . os analysis first , we analyzed the impact of several clinical variables on os calculated from the time of diagnosis ( table 2 )  . 
after the multivariable analysis , patients in whom an alteration was detected with ctdna of 5% or more still had statistically significant survival ( fig 2a )  . among 76 patients who had tissue ngs analysis , patients with braf alterations had significantly worse os , and patients with lung metastases had better os ( statistically significant after the multivariable analysis )  . 
 however , only erbb2 alterations remained significant in the multivariable model ( fig 2b )  . analysis of outcomes for patients with matched therapy versus patients with unmatched therapy outcomes of the patients who were treated with matched therapy after their ctdna testing ( n = 17 ) versus those who were given unmatched therapy ( n = 18 ) were evaluated ( figure 3a ; data supplement )  . 
altogether , 65% of patients in the matched therapy group attained sd for 6 months or more , pr , or cr versus 31% of patients in the unmatched therapy group ( p = .060 in univariable analysis ; p = .045 in multivariable analysis [ multivariable analysis was performed using line of therapy as a confounding variable ] )  . 
in addition , patients in the matched therapy group had a median pfs of 6.1 months compared with 2.3 months for patients in the unmatched therapy group ( p = .143 for univariable analysis ; p = .079 for multivariable analysis )  . 
 finally , patients who received matched therapy survived longer than unmatched therapy group , with a median os ( calculated from the treatment start date ) not reached ( at 11.1 months ) fig 1 . 
only patients with at least one alteration in one of these genestp53 , kras , apc , braf , pik3ca , egfr , myc , or erbb2are displayed ( n = 71 patients ; the other 23 patients had no alterations in the represented genes and their corresponding columns would have been empty or white )  . 
 ( d ) pie charts representing the potential actionability of the detected alterations in the overall population ( n = 94 ; left ) and in patients with at least one nonsynonymous alteration ( n = 74 ; right )  . 
only variables that were significant in the univariable models ( log - rank test ) were included in the multivariable analysis ( cox regression model ) , with the final model containing only significant covariables in the multivariable analyses ( forward stepwise selection model )  . 
the wald statistic tests the unique contribution of each variable ; the higher the wald statistic , the higher the association or contribution in the model . abbreviations : ctdna , circulating tumor dna ; nr , not reached . * if only alterations are included in the multivariable analysis , braf ( p = .034 ) and erbb2 ( p = .004 ) remain significantly associated with shorter survival . 
kaplan - meier curves for overall survival analysis from ( a ) the time of diagnosis and ( b ) the time of blood draw used for the ctdna testing . 
 ( b ) kaplan - meier curves comparing the progression - free survival ( pfs ) for the patients with matched treatment ( n = 17 ) v patients with unmatched treatment ( n = 18 )  . 
 ctdna alterations at baseline : ctdna alterations at progression : arid1a k1808k ( 1.5% ) mtor e162v ( 6.6% ) apc e422 * ( 2.2% ) tp53 s127f ( 1.9% ) apc i1307fs ( 15.9% ) apc e422 * ( 33.8% ) tp53 s127f ( 39% ) egfr amplification time from initiation of therapy with irinotecan plus cetuximab ( months ) imaging obtained pretreatment 4 months post - treatment 9 months post - treatment fig 4 . 
 a 49 - year - old - man with metastatic adenocarcinoma of the rectum had a history of previous treatment with ( 1 ) capecitabine plus oxaliplatin and ( 2 ) fluorouracil plus irinotecan plus bevacizumab ; ( 3 ) treatment on a clinical trial with anti - cd73 included fourthline therapy with irinotecan plus cetuximab . 
 ( b ) the patient showed initial tumor regression , but at 9 months , the tumor progressed with new lung metastases and lymphangitic spread ( red arrow )  . 
ctdna among previously observed alterations increased approximately 20 - fold ( 33.8% for apc e422 * ; 39% for tp53 s127f ) along with emerging alterations , including mtor e162v , apc i1307fs , and egfr amplification . 
 ( ) only levels of ctdna mutations were quantified using %ctdna and represented ; egfr amplification was detected at progression but not quantified . overall , 79% of patients ( 74 of 94 ) had one or more nonsynonymous ctdna alterations ( table 1 )  . 
the most frequently characterized alterations were in tp53 ( 51% of patients ) followed by kras ( 34% ) , apc ( 27% ) , braf ( 16% ) , pik3ca ( 16% ) , and egfr ( 15% ) genes ( fig 1 )  . 
hong et al29 previously reported that the ctdna ngs had 100% sensitivity for tissue - detected as well as digital droplet polymerase chain reactionbased plasma - detected brafv600e mutation among patients with colorectal cancer , which is consistent with our data . 
for instance , sensitivity of ctdna for detection of patients with tissue apc positivity was 44.9% ; sensitivity of ctdna for detection of those with tissue braf positivity was 80% ( this analysis was not restricted to brafv600e )  . 
the apparent low capacity for detecting apc alterations could have implications for plasma monitoring of this alteration . we did not observe differences in the concordance rate of driver alterations when we compared patients with a time interval between the blood draw and tissue biopsy of 6 months or less versus more than 6 months ( data supplement )  . 
 this observation differs from previous reports , which showed that the longer the time interval between the two tests , the lower the rate of concordance.20 , 30 the small number of patients in each of our subgroups may have confounded our ability to discern such differences . importantly , certain clinical and ctdna factors were associated with survival outcome . 
 when survival was evaluated from the time of blood draw to the last follow - up , the presence of apc , braf , pik3ca , egfr , myc , and erbb2 nonsynonymous alterations ( including single nucleotide variations and amplifications ) were all associated with poor overall survival ( all p < .05 by univariable analysis ) , and erbb2 alterations remained significant after the multivariable analysis ( p < .001 ) ( table 2 ; fig 2 )  . 
many of these poor prognostic alterations are potentially targetable with either fda - approved drugs ( onor off - label use ) or with investigational agents currently in clinical development . 
for instance , patients often received concomitant chemotherapy , and the putative interaction between tp53 and bevacizumab could have inflated the results.37 - 39 these considerations are important because some matched therapies have not proved to be effective in colorectal cancers.40 , 41 although the precision medicine approach of matching patients with genomically or immunotargeted treatments is potentially promising , there are challenges for implementing this strategy ( eg , tumor heterogeneity and genomic complexity among patients )  . 
in this study , we observed a median of three alterations per patient ( range , zero to 30 alterations ) , and among 74 patients with one or more alterations , there were no two patients with identical molecular profiles . 
along with this notion , we have also presented a patient with metastatic rectal adenocarcinoma whose ctdna level increased by 20 - fold when his tumor showed progression of lung metastases and lymphangitic spread while he was receiving treatment with irinotecan and cetuximab ( fig 4 )  . 
emergence of alterations similar to those in ctdna and other anomalies such as the appearance of kras alterations have been implicated in the evolution of resistance in patients with colorectal cancer who were treated with egfr inhibitors.46 there were several limitations to our study . 
third , it would be interesting to determine the impact of microsatellite stability status on the ctdna alteration profile ; this analysis could not be performed in this study because only 26 of our patients had microsatellite testing and 25 of them were microsatellite stable . 
despite these limitations , our study provided an in - depth investigation of the clinical utility of ctdna testing among patients with colorectal cancer . in conclusion , we have interrogated tumors from 94 patients with mostly advanced - stage colorectal cancer who had clinical - grade ngs performed on blood - derived ctdna . 
 although the number of patients receiving targeted therapy in our study was modest , this is the first study , to our knowledge , to demonstrate objective evidence of the clinical utility of ctdna ngs in metastatic colorectal cancer across multiple biomarkers beyond brafv600e . 
 stock and other ownership interests : merck ( i ) travel , accommodations , expenses : merck ( i ) amirali talasaz employment : guardant health leadership : guardant health shumei kato no relationship to disclose maria c . 
lanman employment : guardant health , veracyte leadership : guardant health , biolase stock and other ownership interests : guardant health , biolase research funding : guardant health victoria m . 
raymond employment : trovagene , guardant health stock and other ownership interests : trovagene , guardant health stock and other ownership interests : guardant health research funding : guardant health patents , royalties , other intellectual property : guardant health travel , accommodations , expenses : guardant health razelle kurzrock leadership : curematch stock and other ownership interests : curematch , idbydna consulting or advisory role : actuate therapeutics , loxo oncology , xbiotech , neo - med , roche speakers bureau : roche research funding : guardant health ( inst ) , sequenom ( inst ) , merck serono ( inst ) , genentech ( inst ) , pfizer ( inst ) , foundation medicine ( inst ) , incyte ( inst ) , konica minolta ( inst ) support references 2015 affiliations shumei kato , maria c . 
van der geest lg , lam - boer j , koopman m , et al : nationwide trends in incidence , treatment and survival of colorectal cancer patients with synchronous metastases . 
cassidy j , clarke s , daz - rubio e , et al : xelox vs folfox - 4 as first - line therapy for metastatic colorectal cancer : no16966 updated results . 
heinemann v , von weikersthal lf , decker t , et al : folfiri plus cetuximab versus folfiri plus bevacizumab as first - line treatment for patients with metastatic colorectal cancer ( fire - 3 ) : a randomised , open - label , phase 3 trial . 
kopetz s , mcdonough sl , morris vk , et al : randomized trial of irinotecan and cetuximab with or without vemurafenib in braf - mutant metastatic colorectal cancer ( swog 1406 )  . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
schwaederl mc , patel sp , husain h , et al : utility of genomic assessment of blood - derived circulating tumor dna ( ctdna ) in patients with advanced lung adenocarcinoma . 
thierry ar , el messaoudi s , mollevi c , et al : clinical utility of circulating dna analysis for rapid detection of actionable mutations to select metastatic colorectal patients for anti - egfr treatment . 
hong ds , morris vk , el osta b , et al : phase ib study of vemurafenib in combination with irinotecan and cetuximab in patients with metastatic colorectal cancer with brafv600e mutation . 
sartore - bianchi a , trusolino l , martino c , et al : dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - of - concept , multicentre , open - label , phase 2 trial . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
said r , hong ds , warneke cl , et al : p53 mutations in advanced cancers : clinical characteristics , outcomes , and correlation between progression - free survival and bevacizumab - containing therapy . 
schwaederl m , lazar v , validire p , et al : vegf - a expression correlates with tp53 mutations in nonsmall cell lung cancer : implications for antiangiogenesis therapy . 
hochster hs , uboha n , messersmith w , et al : phase ii study of selumetinib ( azd6244 , arry142886 ) plus irinotecan as second - line therapy in patients with k - ras mutated colorectal cancer . 
kim st , lee j , park sh , et al : prospective phase ii trial of everolimus in pik3ca amplification / mutation and / or pten loss patients with advanced solid tumors refractory to standard therapy . 
janku f , huang hj , claes b , et al : braf mutation testing in cell - free dna from the plasma of patients with advanced cancers using a rapid , automated molecular diagnostics systemol cancer ther 15 : 1397 - 1404 , 2016 44 . 
tie j , wang y , tomasetti c , et al : circulating tumor dna analysis detects minimal residual disease and predicts recurrence in patients with stage ii colon cancer . 
the analytical and clinical validation of guardant360 was conducted in conformance with evidentiary standards established by the standards for reporting of diagnostic accuracy , reporting of tumor marker studies , evaluation of genomic applications in practice and prevention , recent next - generation sequencing ( ngs ) , and standardization of clinical testing biomarker guidelines.16 the sequencing uses molecular barcoding and hybrid capture followed by ngs of the critical exons in a panel of 54 to 73 genes and reports all four major types of genomic alterations ( point mutations , insertions - deletions [ indels ] , fusions , and copy number amplifications ) 16 , 23 see the data supplement for detailed gene panels . 
the analytic sensitivity reaches detection levels of one to two single mutant fragments from a 10 - ml blood sample ( 0.1% limit of detection ) , and analytic specificity is greater than 99.9999%. 
the fractional concentration or mutation allele frequency ( maf ) for a given somatic mutation is calculated as the fraction of ctdna harboring that mutation in a background of wild - type ctdna fragments at the same nucleotide position . 
when characterized alterations are referred to , vuss were excluded in the analysis . overall , 76 ( 81% ) of 94 patients who had ctdna results also had ngs performed by agencies accredited by clinical laboratory improvement amendment and the college of american pathologists on tumor tissue using the foundationone assay ( hybrid capture–based ngs ; 182 , 236 , or 315 genes , depending on the time period )  . 
 kappa values range from 1 ( perfect agreement ) to 0 ( no agreement other than what would be expected by chance ) .26 matched therapy and actionability we retrospectively analyzed the treatments given after ctdna testing and compared the clinical outcomes among patients who received matched and unmatched therapies . 
patients were evaluable if therapy was administered for more than 10 days . actionability implies that the protein product of a genomic abnormality can be affected by a specific targeted drug.27 a potentially actionable alteration was defined as an alteration that was either the direct target ( such as an egfr inhibitor targeting an egfr mutation ) or a pathway component ( such as an mtor inhibitor for a pik3ca mutation [ because mtor is downstream of pik3ca ] ) that could be targeted by at least one us food and drug ( fda ) approved or investigational drug in a clinical trial . 
actionability was considered at the variant level ; vuss ( functional consequences and clinical significance of these gene variants are not established , as opposed to characterized alterations ) were considered nonactionable . statistical analysis medians and 95% cis or ranges were reported . 
progression - free survival and overall survival were analyzed by the kaplan - meier method , 28 and the log - rank test ( univariable analysis ) or cox regression model ( multivariable analysis ) was used to compare variables . 
 sequential her2 - targeted therapy in salivary ductal carcinoma with her2 / neu overexpression and a concomitant erbb2 mutation introduction salivary duct carcinoma ( sdc ) is a rare malignancy arising from the major and minor salivary glands.1 , 2 though curative intent surgery followed by radiation is the treatment of choice , locoregional recurrences and distant metastases are frequently reported.1 , 3 cytotoxic chemotherapeutic agents such as platinum analogs , anthracyclines , and taxanes have been effective in treating sdc but there is no established standard of care.4 overexpression of her2 / neu is frequently seen ; thus , trastuzumab can be an effective treatment option.3 however , the role of other her2 - targeting agents after trastuzumab failure is unclear . 
this involved a multiplex polymerase chain reaction using the ion ampliseq cancer hotspot primer pool and the ion ampliseq library kit ( both from thermo fisher scientific , waltham , ma )  . 
 data files were analyzed using the ion torrent variant caller software and integrated genomic viewer ( thermo fisher scientific ) using hg19 reference sequence and nextgene software ( softgenetics , state college , pa )  . 
in addition , three possible germline polymorphisms ( met n375s , tp53 p72r , and flt c.1310 3t > c ) were also detected in the tumor specimen . the patient was treated postoperatively with concurrent radiation to the parotid bed and right neck ( 6 , 600 cgy in 33 fractions over 48 days ) , with high - dose cisplatin ( 100 mg / m2 every 3 weeks for two cycles ) as radiation sensitizer . 
 he underwent a left modified radical neck dissection followed by concurrent radiation ( 6 , 000 cgy in 30 fractions over 42 days to the left neck and 6 , 600 cgy in 33 fractions over 48 days to the axilla ) with weekly carboplatin ( area under the curve , 2 ) because of marginal renal function . 
he had a possible anaphylactic reaction to pertuzumab and hence received trastuzumab monotherapy for seven additional cycles and had a partial response . the patient was disease free for 6 months and then a biopsy - proven recurrence was found on his sk lapatinib treatment was restarted and continued for 9 months ; there was a complete clinical response in his sk the patient is currently on a drug holiday , with no obvious recurrence . 
biopsy - proven skin recurrence of salivary duct carcinoma with complete resolution with lapatinib treatment . two years after the initial recurrence , the patient underwent a wedge resection of a solitary metastasis in the right lower lobe of the lung . nine months later , disease progression was detected in the right axillary and mediastinal lymph nodes . 
 however , because of the response of the sdc to her2 - targeted therapies.3 her2 overexpression is associated with higher recurrence risk , shorter survival , and aggressive clinical behavior with early regional and distant metastasis.2 taxanes and trastuzumab have been used anecdotally in metastatic sdc with her2 / neu overexpression with a good response , 7 but the role of targeted therapy remains unclear . in this case report , we have demonstrated the successful sequential use of her2 - targeted therapy in her2 - overexpressing metastatic sdc . 
after an initial response to trastuzumab docetaxel combination therapy , her2 - targeted agents , with differing mechanisms of action , were used sequentially with good response and prolonged disease control . 
the patient received , sequentially , trastuzumab ( which binds to the extracellular segment of the her2 receptor , neutralizing it and also producing antibody dependent cellular cytotoxicity ) , lapatinib ( which binds to the atp - binding pocket of the her2 protein kinase domain and inhibits tyrosine kinase activity ) , and ado - trastuzumab emtansine ( an antibody - drug conjugate in which trastuzumab inhibits the her2 receptor and the cytotoxic maytansinoid portion of the conjugate is delivered intracellularly and produces cell death )  . 
also , to the best of our knowledge , this is only the second report of ado trastuzumab emtansine use in sdc8 and the first describing sequential her2 targeting in this disease . sequential her2 - directed therapy is well established in metastatic her2 - positive breast cancer , with frontline chemotherapy along with dual her2 - targeted therapy with trastuzumab and pertuzumab followed by other her2 targeted agents.9 a higher absolute erbb2 gene copy number results in shorter time to metastasis in trastuzumab - untreated early breast cancer but longer progression - free survival upon initiation of trastuzumab - based treatment.10 though her2 - positive tumors are highly sensitive to the receptor blockade , resistance has been shown to develop through three main mechanisms : ( 1 ) incomplete blockade as a result of redundant ligands and receptors that enable alternative dimerization patterns ; ( 2 ) reactivation of pathway signaling at or downstream of the receptor layer , such as activating mutations in the pik3ca pathway ; and ( 3 ) use of pre existing or acquired alternate pathways , such as hormone - receptor pathways.11 interestingly , the patient in this case report had an erbb2 v777l mutation in a metastatic specimen before exposure to her2 - targeted therapy . 
the incidence of erbb2 mutations in sdc is uncommon , with a recent series reporting a mutation in four of 37 patients studied.12 all these mutations were in exons 17 through 19 ( namely , i767m , d769y , g776v , and v842i ) , but this series did not identify the v777l mutation . 
the coexistence of her2 amplification and her2 mutation is extremely uncommon because most of the her mutations reported in breast cancer have been seen in patients with her2 neu amplification - negative disease.13 there are limited data on the role of this mutation in breast cancer . 
v777l is present in the proximity of the kinase domain dfg motif of the erbb2 gene ( exon 20 ) and functions as an activating mutation.13 the effects of the erbb2 v777l mutation on response to her2 - targeted therapy are less clear . 
some in vitro studies suggest that this mutation did not affect the sensitivity to her2 - directed therapies in proliferation assays13 ; however , a recent report suggests that the presence of this mutation confers resistance to trastuzumab.14 because the coexistence of her2 amplification and erbb2 mutation is extremely rare , the effect of this combination on response to her2 - targeted therapy is unknown . 
 however , it is possible that the combination of these two events may have led to the excellent response seen in the patient in this report . though this is a single report , we believe that testing for the presence of an erbb2 mutation may be indicated in patients with sdc who have her2 amplification . 
sequential her2 targeting , similar to the breast cancer paradigm , may be a feasible approach in her2 - overexpressing sdcs , especially in those with a concomitant activating erbb2 mutation . 
locati ld , perrone f , cortelazzi b , et al : clinical activity of androgen deprivation therapy in patients with metastatic / relapsed androgen receptor - positive salivary gland cancers . 
van boxtel w , boon e , weijs wlj , et al : combination of docetaxel , trastuzumab and pertuzumab or treatment with trastuzumab - emtansine for metastatic salivary duct carcinoma . 
borley a , mercer t , morgan m , et al : impact of her2 copy number in ihc2 + / fish - amplified breast cancer on outcome of adjuvant trastuzumab treatment in a large uk cancer network . 
 personalized clinical decision making through implementation of a molecular tumor board : a german single - center experience rouven hoefflin anna - lena geiler ralph fritsch rainer claus julius wehrle patrick metzger meike reiser leman mehmed lisa fauth dieter henrik heiland thalia erbes friedrich stock agnes csanadi cornelius miething britta weddeling frank meiss dagmar von bubnoff christine dierks isabell ge volker brass steffen heeg henning schfer martin boeker justyna rawluk gian kayser simone hettmer hauke busch christoph peters martin werner justus duyster tilman brummer melanie boerries ( continued ) purpose dramatic advances in our understanding of the molecular pathophysiology of cancer , along with a rapidly expanding portfolio of molecular targeted drugs , have led to a paradigm shift toward personalized , biomarker - driven cancer treatment . 
here , we report the 2 - year experience of the comprehensive cancer center freiburg molecular tumor board ( mtb ) , one of the first interdisciplinary molecular tumor conferences established in europe . 
the role of the mtb is to recommend personalized therapy for patients with cancer beyond standard - of - care treatment . methods this retrospective case series includes 198 patients discussed from march 2015 through february 2017 . 
the mtb guided individual molecular diagnostics , assessed evidence of actionability of molecular alterations , and provided therapy recommendations , including approved and off - label treatments as well as available matched clinical trials . results the majority of patients had metastatic solid tumors ( 73.7% ) , mostly progressive ( 77.3% ) after a mean of 2.0 lines of standard treatment . 
 treatment recommendations were implemented in 33 of 104 patients ( 31.7% ) , of whom 19 ( 57.6% ) showed stable disease or partial response , including 14 patients ( 7.1% of the entire population ) receiving off - label treatments . conclusion personalized extended molecular - guided patient care is effective for a small but clinically meaningful proportion of patients in challenging clinical situations . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license personalized cancer medicine uses molecular biomarkers for standard - of - care treatment stratification , such as activating braf mutations for the treatment of melanoma with braf inhibitors.1 in parallel , it has become evident that therapeutic strategies with targeted drugs are no longer specific for the treatment of distinct entities but rather for particular molecular profiles across different cancers.2 - 4 thus , testing for single - drug targets can provide therapeutic information , but its predictive value may vary between entities . 
although an activating braf v600e mutation will predict response to braf inhibitors in melanoma , 1 it may not do so in colorectal cancers because of epidermal growth factor receptor ( egfr ) feedback activation with requirement of additional egfr targeting.5 , 6 moreover , non - v600 braf mutations might not be responsive to braf inhibition at all.7 thus , one - mutationone - drug approaches may be ineffective , especially in heavily pretreated patients with cancer . 
examples include the selection of ras mutant clones in colorectal cancer treated with egfr antibodies , such as cetuximab or panitumumab , 11 or the acquisition of a secondary egfr t790m kinase domain mutation mediating resistance to egfr kinase inhibitors , such as gefitinib or erlotinib in non small - cell lung cancer.12 , 13 this increasing amount of complexity requires tools to translate individual information into personalized treatment concepts . 
the initial discussion includes a clinical case presentation , review of the pathology data and the tumor - specific genetic landscape , known molecular predictive or prognostic markers , active clinical trials , and potential inand off - label molecular targeted treatments . 
 diagnostic results are presented to the mtb by the molecular pathology and / or the computational biologist teaafter discussion , treatment recommendations are given and are supported by levels of evidence ( data supplement )  . 
these are based on published molecular biomarker recommendations.14 patients and patient informed consent all patients discussed ( n = 198 ) were included in this retrospective single - center case series . 
patients with individual or family history indicative of germline disease - causing mutations were referred to the institute of human genetics for counseling and possibly germline genetic analyses . diagnostic molecular pathology appropriate tissues were subjected to molecular analyses as recommended by the mtb ( fig 1 )  . 
 a molecular diagnostic tests 36 16 immunohistochemistry per case 15 6 ddseq ( exon / hotspot ) hpv testing tngs rna - seq ( total = 867 ) ( total = 492 ) 7 - 8 antibodies ( total = 139 ) type of tngs 48 - gene panel 8 - gene panel brca1 / brca2 54 - gene myeloid panel 1 antibody 2 antibodies 3 antibodies 4 antibodies 5 antibodies 6 antibodies not annotated cosmic ( no hotspot ) hotspot ( not actionable ) actionable ( sensitizing ) actionable ( resistence ) tumor entities brain colorectal melanoma thyroid other gastrointestinal fig 1 . 
 ( a ) the panels depict the type of molecular diagnostic testing performed ( left panel ) and specify the number of immunohistochemical stains ( one to eight antibodies ) per case ( middle panel ) as well as the type of targeted next - generation sequencing ( tngs ) library sequenced ( right panel )  . 
tngs was performed either by a custom panel ( eight - gene panel ) , a 48 - gene panel ( truseq amplicon cancer panel , illumina , san diego , ca ) , a 54 - gene myeloid panel ( trusight myeloid sequencing panel , illumina ) or a custom brca1 / 2 consortium panel . 
differentially expressed genes were identified using the limma voom package from r / bioconductor.34 , 35 results from march 2015 through february 2017 , 49 mtb meetings were attended by a median of 16 physicians and scientists , ensuring continuous interdisciplinary data interpretation and discussions with diagnostic and therapeutic decision making . 
the workflow of the mtb included a case and literature review , molecular diagnostic recommendations , and follow - up discussions of the molecular diagnostic results , including treatment recommendations ( appendix fig a1 )  . 
these included 305 diagnostic and 104 treatment recommendations . patient characteristics the average patient age at the time of the initial mtb presentation was 58 years ( range , 1 to 85 years )  . 
the majority of patients ( n = 146 ; 73.7% ) suffered from metastatic disease , and 77.3% ( n = 153 ) showed disease progression while receiving the standard treatment ( table 2 )  . 
of all diagnostic recommendations , 234 ( 76.7% ) were implemented , resulting in 867 single diagnostic tests ( mean , five per patient ) , including 815 routine molecular tests and 52 extended genetic analyses ( fig 1a , left panel )  . routine molecular diagnostics included immunohistochemical ( ihc ) staining for biomarkers ( n = 492 ; fig 1a , middle panel ) , such as programmed death - ligand 1 ( pd - l1 ) and mismatch repair proteins , in situ hybridizations ( ish ) for gene copy number analyses ( n = 92 ) , and testing for microsatellite instability and / or gene hotspot variations ( n = 89 ) and tngs ( n = 139 ; fig 1a )  . 
the most frequent cosmic annotated sequence variants detected by tngs occurred in tp53 , brca1 , kdr , kit , kras , pik3ca , brca2 , and braf ( fig 1b ; data supplement )  . 
therapeutically relevant mutations in hotspot regions were identified in 41 of 139 patients ( 29.5% ) , including drug - sensitizing variants in braf , pik3ca , idh1 , egfr , and kit , as well as drug resistance variants in kras and nras . extended genetic analyses including exome and transcriptome assays were performed for 36 patients ( 18.2% ; wes and rna - seq : n = 35 ; rna - seq only : n = 1 )  . 
patient characteristics characteristic total , no . female male ( range ) tumor type soft tissue unknown primary site colorectal urogenital thyroid breast lung skin hepatobiliary upper gi tract hematologic neuroendocrine pediatric head and neck others complete remission localized disease metastatic disease 2 to 3 rare tumor others solid tumors ( n = 189 ) : stage at presentation no . 
ninety of 104 treatment recommendations ( 86.5% ) were either off - label therapies ( n = 77 ) or trial inclusions ( n = 13 )  . the implementation rate of treatment recommendations was 31.7% ( 33 of 104 )  . 
in - label recommendations were pursued in nine of 14 cases ( 64.3% ) , whereas off - label recommendations and trial inclusions were implemented in only 28.6% ( 22 of 77 ) and 15.4% ( two of 13 ) of the cases , respectively . 
intended trial inclusion in 11 patients failed because of poor performance status or patient death ( n = 5 ) , closed trial arm ( n = 4 ) , or patient will ( n = 2 )  . 
main reasons for nonimplementation of treatment recommendations included loss to follow - up ( 22.5% ) , recommendation in the future ( 19.7% ) , patient death ( 16.9% ) , patient will ( 14.1% ) , and medical reasons ( 14.1% ; data supplement )  . 
of note , evidence level of individual off - label recommendations did not affect implementation rates ( data not shown )  . clinical outcome dgi and target databases , respectively ( data supplement )  . 
 the disease impact of non - hotspot mutations is more difficult to evaluate ; however , it can lead to in 33 patients with implemented treatment recommendations , partial remissions ( pr ) and stable diseases ( sd ) were seen in 11 ( 33.3% ) and eight patients ( 24.2% ; table 1 ) , respectively . 
of 14 responders receiving off - label therapies , eight ( 57.1% ) showed a progression - free survival ( pfs ) ratio ( pfs2 / pfs1 ; pfsr ) > 1.3 , supporting the impact of the recommended therapies.36 three patients had a pfsr < 1.3 with ongoing responses , meaning that their pfsr is still increasing . 
to assess whether implementation of treatment recommendations affected overall survival from first mtb discussion , we analyzed all patients with stage iv malignancies according to three subgroups ( n = 148 ; fig 3 )  . 
the median survival was not reached for patients with implemented treatment recommendations ( n = 33 recommendations pursued ; 95% ci , 9 months to not reached ) , 8 months for patients for whom treatment recommendations were not implemented ( n = 43 recommendations not pursued ; 95% ci , 3 to 10 months ) , and 10 months for patients who did not receive a treatment recommendation ( n = 72 no recommendations ; 95% ci , 7 to 17 months )  . 
predictive biomarkers for individualized immunotherapies are emerging and changing rapidly , with strong differences between entities.44 here , we used ihc for programmed cell death protein 1 ( pd - 1 ) / pd - l1 , tumor - infiltrating lymphocytes , microsatellite instability testing , and mutational burden assessment as predictive biomarkers . 
in the near future , identifying individual cancer neoantigens might allow a more precise prediction of responses to immunotherapies.45 this highlights the importance of an interdisciplinary mtb team that analyzes and interprets biomarkers to identify patients who might benefit from off label immuno - oncology treatments . in an mtb workflow , the portfolio of molecular diagnostic tests , as well as criteria to match and prioritize targeted therapies to molecular biomarkers , affects the probability to identify patients with actionable targets . 
our approach shares similarities with memorial sloan kettering integrated mutation profiling of actionable cancer targets ( msk - impact ) , focusing on therapeutically targetable biomarkers for fast clinical decision making and referral of patients to available clinical trials.51 targeted drug combinations might offer better dcr over single - agent therapies.52 - 55 in part , this is due to crosstalk between signaling pathways as well as spatial and temporal clonal heterogeneity , especially in patients with advanced cancer who failed standard - of - care treatment.56 , 57 most current programs for precision oncology use prespecified , genetically matched , single - agent treatments ( nci - match , clinicaltrials.gov identifier : nct02465060 ; or targeted agent and profiling utilization registry [ tapur ] , clinicaltrials.gov identifier : nct02693535 )  . 
these patients did not suffer from grade 3 to 4 adverse effects , although treatment combinations may bear a higher risk of toxicity.58 earlier referral to an mtb ( eg , after failure of first - line treatment ) might prevent the institution of ineffective treatments , improve the implementation rate , and increase the likelihood of success of molecular biomarkermatched treatments . 
 because of the low sample size and the heterogeneous composition of patients in the cohorts , the validity of this survival analysis is limited . access to molecular biomarkermatched , off label agents for cancer treatment is limited . 
in a recent single - center study , only 5% of molecular biomarkermatched treatment recommendations were implemented , mainly because of limited access to clinical trials or to restricted use of drugs outside their marketed label.59 thus , it is crucial to build up platforms for patients and treating physicians to link individual molecular information of the tumor to appropriate nonapproved drugs and available clinical trials . 
in rare entities , and especially in the setting of treatment - refractory cancers , precision oncology networks should allow hypothesis - driven in vitro studies and validation in small sets of individuals . 
thus , within the concept of patient - centric , biomarker - driven trial designs , 60 an mtb might constitute a critical tool to identify informative patients for clinical trials of targeted therapies in rare molecular subgroups . in summary , this mtb experience illustrates that patient management , on the basis of individual molecular biomarker profiling and analysis , is feasible in patients beyond standard - of - care treatment . 
 hauke busch no relationship to disclose christoph peters leadership : university medical center freiburg honoraria : university medical center freiburg travel , accommodations , expenses : novartis martin werner honoraria : diakovere consulting or advisory role : roche , novartis , johnson & johnson research funding : agilent ( inst ) , novartis ( inst ) , roche ( inst ) justus duyster honoraria : novartis , genentech , pfizer consulting or advisory role : novartis , roche travel , accommodations , expenses : novartis tilman brummer no relationship to disclose melanie boerries no relationship to disclose silke lassmann honoraria : novartis , astrazeneca travel , accommodations , expenses : novartis , astrazeneca nikolas von bubnoff honoraria : astrazeneca , amgen , bristol - myers squibb consulting or advisory role : novartis research funding : novartis travel , accommodations , expenses : novartis acknowledgment we thank the team of the genomics and proteomics core facility , german cancer research center / dkfz , heidelberg , germany , for their sequencing service . affiliations all authors : university of freiburg , freiburg ; ralph fritsch , julius wehrle , cornelius miething , christoph peters , martin werner , justus duyster , tilman brummer , melanie boerries , silke lassmann , and nikolas von bubnoff , german cancer consortium , partner site freiburg , and german cancer research center , heidelberg ; rainer claus , augsburg medical center , augsburg ; and hauke busch , university of lbeck , lbeck , germany . supported by comprehensive cancer center freiburg and by deutsches konsortium fr translationale krebsforschung grant no . 
hoadley ka , yau c , wolf dm , et al : multiplatform analysis of 12 cancer types reveals molecular classification within and across tissues of origcell 158 : 929 - 944 , 2014 3 . 
hong ds , morris vk , el osta b , et al : phase ib study of vemurafenib in combination with irinotecan and cetuximab in patients with metastatic colorectal cancer with brafv600e mutation . 
goss g , tsai cm , shepherd fa , et al : osimertinib for pretreated egfr thr790met - positive advanced non - small - cell lung cancer ( aura2 ) : a multicentre , open - label , single - arm , phase 2 study . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
kovaleva v , geissler al , lutz l , et al : spatio - temporal mutation profiles of case - matched colorectal carcinomas and their metastases reveal unique de novo mutations in metachronous lung metastases by targeted next generation sequencing . 
kumar p , henikoff s , ng pc : predicting the effects of coding non - synonymous variants on protein function using the sift algorithnat protoc 4 : 1073 - 1081 , 2009 32 . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular profiling of patients tumors to find potential targets and select treatments for their refractory cancers . 
johnson db , dahlman kh , knol j , et al : enabling a genetically informed approach to cancer medicine : a retrospective evaluation of the impact of comprehensive tumor profiling using a targeted next - generation sequencing panel . 
massard c , michiels s , fert c , et al : high - throughput genomics and clinical outcome in hardto - treat advanced cancers : results of the moscato 01 trial . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
tos , tumorboard online system . online registration ( tos ) > 5 days prior to mtb treating physician analysis : adherence to recommendation entity expert review literature check trial availability molecular pathology review pathology review biomarkers treatment decision patient analysis : outcome 1 . 
 o impact of variable rna - sequencing depth on gene expression signatures and target compound robustness : case study examining brain tumor ( glioma ) disease progression alexey stupnikov paul g . 
mcart , phd , msc , bioinformatics group , health sciences ( continued ) purpose gene expression profiling can uncover biologic mechanisms underlying disease and is important in drug development . 
the impact of sequencing depth alteration on rna - seqbased downstream analyses such as gene expression connectivity mapping is not known , where this method is used to identify potential therapeutic compounds for repurposing . methods in this study , published rna - seq profiles from patients with brain tumor ( glioma ) were assembled into two disease progression gene signature contrasts for astrocytoma . 
gene signatures were subsampled to simulate sequencing alterations and analyzed in connectivity mapping to investigate target compound robustness . results data loss to gene signatures led to the loss , gain , and consistent identification of significant connections . 
 building , centre for cancer research and cell biology , queens university belfast , 97 lisburn rd , belfast , bt9 7bl , united kingdom ; twitter : @drdmcart ; e - mail : d.mcart@qub.ac.uk. measurement is rna sequencing ( rna - seq ) of cdna transcripts in a high - throughput manner . 
rna - seq has wider analytical capabilities , including single nucleotide variants , insertion - deletions , gene splice variants , post - transcriptional modifications , and gene fusion detection , but remains costly.6 , 7 experimental techniques developed to minimize sequencing costs include sample multiplexing . 
 multiplexing involves labeling each sample library with a barcode identifier , allowing multiple libraries to be pooled and sequenced simultaneously , reducing costs.7 - 10 smaller volumes of rna are analyzed for multiplexed samples ; thus , the downside to multiplexing is reduced sequencing depth for this library type . accurate assessment of transcripts depends on length , abundance , and mappability to the reference and sufficient sequencing depth , particularly for genes with low transcript abundance.11 , 12 sequencing depth alterations can affect the detection of differentially expressed genes ( degs ) and potentially the accuracy of rna - seqbased downstream analysis . 
few studies have assessed the impact of sequencing depth alterations on rna - seq downstream applications.13 more studies are required , particularly to assess applications that rely on precise gene signatures , informative in classifying cancer subtypes and improved prognostic and predictive outcomes.14 , 15 a gene signature is summarized by degs that collectively represent the most prominent features of a cancer subtype or disease progression phenotype . 
this could be particularly problematic for connectivity mapping that examines a gene expression signature contrast with the aim of predicting potentially therapeutic us food and drugapproved target compounds for repurposing.16 there is urgent need for new targeted therapies for gliomas , which are the most common form of primary brain tumor . 
gliomas can be classified from grade i to iv on the basis of histologic and molecular information.17 depending on the cell of origin , each neoplasm is classified as an astrocytoma , oligodendroglioma , or ependymoma . 
herein , reference gene signatures were compiled from publically available sequenced tumors for astrocytoma disease progression.2 subsampling was applied to simulate sequencing depth alterations of gene signatures , and the performance of connectivity mapping was assessed . 
results reveal that information loss to gene signatures significantly affects target compound robustness . methods published whole transcriptome sequencing data of brain tumor biopsy specimens from adults ( accession : gse48865 ; bao et al2 ) was downloaded from the sequence read archive.25 on average , samples had 50 million reads each . 
reads were quality controlled using trimmomatic software26 and aligned using bowtie2 , 27 allowing one mismatch against the human genome version hg38.28 aligned reads were mapped to genes from the grch38.81 annotation29 using samexplorer software.30 , 31 to benchmark a diverse range in performance of the rna - seq analysis , mapped reads were subsampled to simulate samples with a range of lower cdna library sequencing depths using a bioinformatics pipeline32 ( appendix fig a1 ; data supplement )  . 
the impact of information loss to gene signatures for degs , gene ontology ( go ) terms , and target compound detection was assessed using differential expression , go , and gene expression connectivity mapping analysis , respectively , with deseq2 , goseq , and the qub accelerated drug and transcriptomic connectivity ( quadratic ) software33 - 35 ( data supplement )  . 
the reproducibility of significant connections to the library of integrated cellular signatures identified for all cell lines and neuronal specific cell lines ( data supplement ) by quadratic was investigated16 , 36 - 38 ( data supplement )  . 
results and associated false discovery rates ( fdrs ) were visualized using the r packages venndiagram and ggplot2.39 , 40 results assessment of the l - h and h - h gene expression signatures l - h ( dataset_i ) and h - h ( dataset_ii ) gene signature contrasts comprised 47 and 33 patients , respectively ( data supplement )  . 
 when data input was reduced , the fdr for the number of degs detected increased linearly and by approximately the same amount for both data sets ( appendix fig a2 )  . 
dataset_i gene signature therefore demonstrated better resilience to data loss for deg detection compared with dataset_ii . for the full data set ( f = 1.0 ) , > 200 go terms described the functions of the degs identified for dataset_i ( appendix fig a3a )  . 
given this low number , which reduced to zero on f = 0.5 , go results for subsampled dataset_ii are not depicted . impact of information loss to gene signatures used in gene expression connectivity mapping for the full data set , a greater number of significant reverse ( rev ) and progress ( prog ) connections were identified for dataset_i compared with dataset_ii ( fig 2a )  . 
effect of decreased cdna library sequencing depth on the number of differentially expressed genes ( degs ) detected from ( a ) dataset_i , and ( b ) dataset_ii gene signatures ( data supplement )  . 
visualization of the global stratification ability of ( c ) dataset_i , low to high ( l - h ) , and ( d ) dataset_ii , high to high ( h - h ) gene signatures . 
heatmap was generated using unsupervised hierarchical clustering with the full rna - seq data ( f = 1 ) and depicts the gene expressional patterns of the top 100 differentially expressed genes identified between the gene signature contrast groups . 
the who disease grades of samples as determined by bao et al2 are overlaid . target compound identification , dataset_i was therefore more resilient to alterations in cdna sequencing depth compared with dataset_ii . the impact of data loss to gene signatures and the reproducibility of connectivity mapping is presented in figures 3 - 5 . 
for example , 3 , 135 rev connections were identified for dataset_i using f = 1.0 ; this increased to approximately 5 , 000 when subsampled to f = 0.01 , but approximately 60% of compounds were infrequently detected ( figs 3b and 3c )  . 
for dataset_i , when 50% of reads were removed , approximately 62.5% rev ( approximately 2 , 500 of 4 , 000 ) and approximately 50% prog significant connections ( approximately 1 , 500 of 3 , 000 ) were identified with every iteration ( fig 3 )  . 
for dataset_ii , when 50% of reads were removed , just approximately 13% rev ( approximately 400 of 3 , 000 ) and 9% prog significant connections ( approximately 180 of 2 , 000 ) were identified with every iteration ( fig 4 )  . 
 significant connections that potentially could progress ( prog ) or reverse ( rev ) the disease phenotype and fdrs are plotted against the data fraction included in the analysis ( f )  . 
when affected by data loss , connectivity mapping results were more robust for dataset_i compared with the dataset_ii gene signature . reducing data to the gene signature led to the loss , gain , and consistent identification of significant connections to target compounds ( fig 5 )  . 
for dataset_i , a large proportion of the significant connections across all cell lines ( 69% ; 2 , 195 of 3 , 135 ) and neuronal - specific cell lines ( 70% ; 144 of 205 ) were detected with all data fractions . 
similarly for dataset_ii , a proportion of the significant connections across all cell lines ( 7% ; 100 of 1 , 339 ) and neuronal specific cell lines ( 5% ; nine of 172 ) were detected with all data fractions . 
for example , 350 and 105 compounds were detected across all cell lines for dataset_i , f = 0.01 , that were not identified by the full data set ( fig 5a )  . 
when 50% of the reads were removed , nine and 27 target compounds identified for neuronal specific cell lines were lost , respectively , for dataset_i and ii ( figs 5c and 5d ; table 1 )  . 
thus , for dataset_ii , more target compounds identified by the full gene signature were lost , and some of these included compounds of potential clinical utility for glioma , such as suramin and dasatinib ( table 1 )  . 
a comparison of the rate of impact of data loss on go terms and significant connections detection for dataset_i can be seen by comparing figures a3 and 2a . discussion understanding molecular pathways and regulatory networks driving cancer is essential for the development of new therapies . 
gene expression profiling using rna - seq has led to the development of clinically relevant gene signatures that are informative for cancer subtypes.14 , 15 rnaseq experimental approaches such as sample multiplexing reduce cdna sequencing depth and potentially affect gene signature accuracy . 
significant connections to target compounds identified from the neuronal derived cell lines using ( c ) dataset_i and ( d ) dataset_ii across gene signatures are also compared . more patient gene expression profiles matched their who grade classifications . 
results support the subjective nature of tumor classification , which has interobserver variability.41 gene signatures provided a framework to assess connectivity mapping output for a well - performing accurate versus a poorer - performing less accurate contrast . characterization of the disease progression gene signatures revealed they differed in biologic complexity . 
thus , the l - h gene signature was more resilient to data loss for deg detection and had greater test sensitivity compared with the h - h gene signature . 
overall , the number of significant connections detected for the l - h gene signature was greater , most likely explained by the heterogeneous biologic mechanisms involved in lowto high - grade astrocytoma transition . 
with data loss , this fdr threshold was reached by the l - h and h - h gene signatures , respectively , when 70% and just 1% of reads were removed . 
thus , the l - h gene signature was more resilient to data loss for the detection of significant connections to target compounds using connectivity mapping . subsampling of gene signatures for connectivity mapping revealed that the suite of significant connections to target compounds became modified with data loss . 
compounds lost by the h - h gene signature ( who grade iii to iv ) included suramin , lopinavir , dasatinib , and vincristine , which have already been considered as glioma treatments . 
suramin , an anticancer agent , inhibits the binding of growth factors understood to play a role in glioma progression , angiogenesis , and radioresistance and has been used to treat newly diagnosed gbms.42 , 43 lopinavir , a protease inhibitor , has reached phase ii clinical trials for the treatment of high - grade glioma.44 dasatinib , a kinase inhibitor that acts on members of the src family of kinases , is well studied in glioma and has shown preclinical promise.45 vincristine , a spindle poison , is used in combination with procarbazine and lomustine to treat high - grade glioma and has also been successful in a phase iii trial for the treatment of low - grade gliomas.22 , 46 , 47 reductions in transcript abundance probably led to the loss of low - abundance genes from the full gene signature and altered the degs detected , leading to the loss of these connectivity mapping connections . 
fewer significant connections identified by the full data sets were lost by the l - h gene signature compared with the h - h gene signature , suggesting it was more resilient to data loss . 
similarly , in another subsampling rna - seq study of healthy organisms from multiple taxa , highly expressed genes regulating metabolism and pathogenesis of disease were consistently identified even when downsampling rna - seq reads to only 1 million reads , 13 thereby corroborating our findings from diseased tumors . results highlight the need for determining the optimal cdna sequencing depth for accurately identifying degs when compiling gene signatures . 
in the future , rna standard and spike - in controls may be useful to inform rna - seq best practices.48 the accuracy of a gene signature was particularly important when carrying out additional downstream analyses , such as connectivity mapping . 
given the instability of gene expression , perhaps using ontology types or ontotypes49 to characterize contrast phenotypes may be a more reliable approach compared with gene lists in connectivity mapping . 
other target compounds sensitive to data loss are being tested for their biologic efficacy against glioma stem cells using clonogenic cell survival assays and western blot analyses in ongoing studies by this research group . 
roddy no relationship to disclose manuel salto - tellez consulting or advisory role : philips healthcare , visiopharm , bristol - myers squibb , merck patents , royalties , other intellectual property : co - inventor of qupath ( open - source system for digital pathology analysis ) darragh g . 
mcart , queens university belfast ; tom flannery , estelle healy , and manuel salto - tellez , belfast health and social care trust , belfast , united kingdom ; alexey stupnikov , johns hopkins university , baltimore , md ; hayley p . 
 kurian , brain tumour research centre , university of bristol , bristol , united kingdom ; and frank emmert - streib , tampere university of technology , tampere , finland . supported by funding from the brainwaves northern ireland charity ( registered charity number : nic103464 )  . 
bao zs , chen hm , yang my , et al : rna - seq of 272 gliomas revealed a novel , recurrent ptprz1 - met fusion transcript in secondary glioblastomas . 
verhaak rg , hoadley ka , purdom e , et al : integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
wang l , si y , dedow lk , et al : a low - cost library construction protocol and data analysis pipeline for illumina - based strand - specific multiplex rna - seq . 
liu y , zhou j , white kp : rna - seq differential expression studies : more sequence or more replication ? bioinformatics 30 : 301 - 304 , 2014 13 . 
turkington rc , hill la , mcmanus d , et al : association of a dna damage response deficiency ( ddrd ) assay and prognosis in early - stage esophageal adenocarcinoma . 
lamb j , crawford ed , peck d , et al : the connectivity map : using gene - expression signatures to connect small molecules , genes , and disease . 
okamoto y , di patre pl , burkhard c , et al : population - based study on incidence , survival rates , and genetic alterations of low - grade diffuse astrocytomas and oligodendrogliomas . 
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stupp r , hegi me , mason wp , et al : effects of radiotherapy with concomitant and adjuvant temozolomide versus radiotherapy alone on survival in glioblastoma in a randomised phase iii study : 5 - year analysis of the eortc - ncic trial . 
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effect of decreased cdna library sequencing depth on the number of gene ontology ( go ) terms identified for ( a ) dataset_i and ( b ) the false discovery rate ( fdr ) for the number of go terms identified . 
 multiplex gene profiling of cellfree dna in patients with metastatic melanoma for monitoring disease purpose hotspot blood cell - free dna ( cfdna ) biomarker assays have limited utility in profiling tumor heterogeneity and burden and in capturing regional metastasis with low disease burden in patients with melanoma . 
we investigated the utility of a sensitive 54cancer gene digital next - generation sequencing approach targeting blood cfdna single nucleotide variants ( snvs ) and copy number amplification for monitoring disease in patients with melanoma with regional or distant organ metastasis ( dom )  . patients and methods a total of 142 blood samples were evaluated by digital next - generation sequencing across two patient cohorts . 
cohort 2 consisted of 12 overlapping patients who were longitudinally monitored after complete lymph node dissection to dom . results in cohort 1 , cfdna snvs were detected in 75% of patients . 
in cohort 2 , 98 longitudinal blood samples along with matched regional and distant metastases from 12 stage iii patients were analyzed before complete lymph node dissection and throughout disease progression . 
2018 by american society of clinical oncology introduction after surgical resection of regional metastatic melanoma , longitudinal molecular profiling would greatly aid in monitoring for recurrence , progression , and therapeutic efficacy.1 molecular profiling of melanoma biopsies or tumors becomes more challenging when patients experience progression to distant organ metastasis ( dom ) as a result of procedure - related morbidity risks and limited sampling efficiency in capturing tumor heterogeneity.2 blood cell - free dna ( cfdna ) biomarkers are minimally invasive and potentially allow routine monitoring of molecular changes in patients cancer over the course of therapy and follow - up.3 this would enable monitoring of treatment efficacy , 4 recurrence , and / or subclonal mutation ( s ) tracking as tumors evolve or relapse.5 unfortunately , no blood - based melanoma biomarker is available for early detection of recurrence , particularly in patients with stage iii melanoma rendered clinically disease free upon surgery , except the problematic surrogate biomarker , serum lactate dehydrogenase ( ldh ) .6 to address this need , we pioneered the investigation of selena y . 
 cfdna utility7 - 9 and explored different types of cfdna biomarkers for monitoring patients with melanoma.4 , 9 - 12 a comprehensive profile of cfdna mutations given the recent genomic classification of cutaneous melanoma ( braf , nras , nf1 , and triple wild - type ) 13 , 14 would provide real - time monitoring of postoperative residual disease to capture progression and enable earlier detection of recurrence compared with clinical or radiologic detection . 
hotspot target blood assays ( braf mutations ) may not be suitable to comprehensively profile metastatic melanomas given the high intratumor heterogeneity.15 - 17 blood cfdna profiling using a cancer panel can address this heterogeneity issue if highly sensitive for metastatic disease . 
overall , melanoma cfdna profiling could provide a clinically informative approach for monitoring disease progression , heterogeneity , and earlier detection of dom . in this study , we systemically assessed the utility of profiling melanoma blood cfdna using a sensitive digital next - generation sequencing ( ngs ) assay that includes a panel of 54 cancer genes in our clinically well - annotated patient cohorts with melanoma , with follow - up during a clinically disease - free period . 
specifically , we focused on longitudinal cfdna follow - up analysis in patients before curative surgery of american joint committee on cancer ( ajcc ) stage iii regional metastatic disease and throughout disease progression until the development of dom . 
the second cohort ( cohort 2 ) included patients overlapping with cohort 1 ( table 1 ) who were enrolled in a us food and drug administrationregistered phase iii clinical trial for ajcc stage iii melanoma ( clinicaltrials.gov identifier : nct00052130 ; appendix fig a1 ) .19 briefly , after complete lymph node dissection ( clnd ) to render patients clinically disease free , patients were randomly assigned to one of the following two treatment arms : bacillus calmette - gurin plus canvaxin melanoma vaccine ( cancervax , carlsbad , ca ) or bacillus calmette - gurin plus placebo , with all patient belonging to the treatment ar no statistically significant clinical difference between the two randomized treatment arms was reported.20 cohort 2 patients were selected on the basis of available blood samples during follow - up that were in accordance with the clinical trials protocol . 
ninety - eight blood samples were collected at baseline ( before clnd or before study ) and during follow - up with available paired formalin fixed paraffin - embedded ( ffpe ) tumors . 
specifically , the blood was collected before clnd ( ajcc stage iii disease ) and during follow - up every 2 to 4 months before dom ( ajcc stage iv disease )  . 
the follow - up time points were based on defined patient visits at 2 , 4 , and 12 months in year 1 and every 6 months in years 2 and 3 . 
standard clinical follow - up consisted of a patient visit with serum ldh blood testing , x - ray imaging every 3 months , and annual ct of the chest , abdomen , and pelvis along with brain ct or magnetic resonance imaging . 
this study was performed in accordance with reporting recommendations for tumor marker prognostic studies.21 sample collection and dna purification peripheral blood was collected , and serum was isolated , centrifuged , and filtered before cryopreservation in aliquots at 80c , as previously described7 , 11 under good laboratory practice conditions . 
the panel covers all known frequent melanoma driver mutations14 and includes full exon coverage of 18 genes , critical exons for the 36 remaining genes ( ie , having somatic mutations reported in the catalogue of somatic mutations in cancer23 ) , and three copy number variations ( cnvs )  . 
 the variant allele fraction ( vaf ) was calculated as the number of cfdna molecules with variants at a given nucleotide position divided by the total number of unique cfdna molecules at that position . 
cfdna snvs were categorized as somatic variants through referencing the catalogue of somatic mutations in cancer database23 or as variants of uncertain significance upon additional reference to the database of short genetic variation . 
snv load was calculated on the basis of the number of unique snvs per patient excluding cnvs . validation of digital ngs to validate cfdna snvs identified by digital ngs , dna from the resected matched tumor ( regional or distant metastasis ) was subjected to custom targeted sequencing using a truseq custom amplicon panel ( illumina , san diego , ca ) as performed by the john wayne cancer institute sequencing center . 
libraries were prepared with the truseq custom amplicon low input library prep kit ( illumina ) , following the manufacturers protocol , and sequenced on the illumina miseq with 150 - base pair single - end reads . 
raw sequencing reads were trimmed using trimmomatic ( version 0.33 ) , 24 mapped to the human genome ( 1000 genomes ( b37 ) build ) using bwa ( version 0.7.12 ) 25 at default settings , and processed using gatk ( version 3.4 ) 26 base quality score recalibration and indel realignment in accordance with the gatk best practices recommendations . 
the number of reads mapping to each locus of interest was counted using the mpileup function in samtools.27 concordance analysis snv concordance in paired tumor tissue and blood samples was determined as positive when the mutation was found in both tumor and cfdna or negative when cfdna snvs were not detected in the paired tumor . 
comparison of cfdna analysis versus radiologic imaging or ldh for detection of dom was assessed using fishers exact test , where an ldh cutoff value of 190 u / l was used.6 fishers exact and f tests were performed for categorical and continuous variables , respectively . 
cfdna status cutoff values were evaluated using the cutp ( ) function in statistical r package , survmisc.28 the gompertz survival regression29 - 31 was used to evaluate the disease - free survival ( dfs ) differences between cfdna snv groups . 
a single blood sample obtained from patients in cohort 1 was analyzed for known os outcome based on ( a ) snv load and ( b ) snv burden . regression was used for adjusting clinical factors in multivariable analyses . 
all statistical analyses were performed with r studio ( r studio , boston , ma )  . results cfdna snvs and association with outcomes the digital ngs assay was used to analyze 54 clinically relevant cancer genes covering all major melanoma driver genes ( appendix table a2 ) in blood cfdna of patients with ajcc stage ii , iii , or iv melanoma ( cohort 1 ; appendix table a1 ) collected before dom relapse or elective surgery . 
 the most frequently mutated genes , braf , tp53 , and nras ( appendix fig a2 ) , align with those previously reported in our studies in the melanoma tissue mutational landscape.13 , 14 to confirm that cfdna somatic snvs ( appendix table a3 ) were tumor derived , custom targeted amplicon sequencing was performed in matched tumor dna ( cohort 1 )  . 
multivariable analysis showed that higher snv load and burden were independent prognostic factors for worse os and dfs after adjusting for age , sex , and m category ( appendix tables a6 and a7 )  . 
 a pre - op < 0.1 clinically disease free disease progression curative sg ( clnd ) 2 - 4 mos 2 - 4 mos 2 - 4 mos 2 - 4 mos 2 - 6 mos cfdna snvs / cnvs detected recurrence lead time pre - op clinical recurrence 0 - 13 mos follow - up after recurrence pre - op sb12 disease free distant mets pre - op disease free distant mets pik3ca ( i663s ) met ( r1166q ) braf ( v600k ) ezh2 ( y646f ) myc ( l97f ) tp53 ( l111q ) apc ( t1689t ) egfr ( p589p ) ldh ( nd ) < 0.1 time after clnd ( mos ) time after clnd ( mos ) fig 2 . 
clnd , complete lymph node dissection ; cnv , copy number variation ; mets , metastases ; mos , months ; ldh ( nd ) , lactate dehydrogenase not done longitudinally ; pre - op , preoperative ; sg , surgery ; snv , single nucleotide variant ; vaf , variant allele fraction . cfdna profiling after clnd digital ngs was performed to longitudinally profile cfdna snvs in 98 blood samples collected from 12 patients with melanoma ( cohort 2 )  . 
the cfdna analysis of all serially collected blood samples is summarized per patient over longitudinal follow - up for somatic snvs ( appendix table a8 ) and variants of uncertain significance ( appendix table a9 )  . 
the most frequent snvs detected were in tp53 ( 75% ) and braf ( 58% ; fig 3a ) , reflecting frequently reported metastatic melanoma dna mutations.14 lack of preclnd cfdna snv detection in three patients was unlikely to be a result of low tumor burden , because all three patients had stage iiic disease with positive lymph nodes ( sb3 , n = 9 ; sb7 , n = 1 ; and sb10 , n = 1 )  . 
increasing vaf ( p = .019 ) and snv burden ( p = .039 ) after relapse was strongly associated with disease progression in this patient cohort ( cohort 2 ; fig 3b )  . earlier detection of dom by longitudinal cfdna analysis we evaluated whether longitudinal cfdna profiles can detect residual or progressive disease after clnd to provide earlier detection of dom compared with clinical or radiologic imaging . 
 given their utility in ajcc staging32 and emerging prognostic utility in immunotherapy , ldh levels were also evaluated for recurrence monitoring.33 , 34 ldh values were longitudinally assessed in eight patients ( fig 4 )  . 
 ( b ) significant correlation of increasing variant allele fraction ( vaf ; left ) and total number of cfdna variants ( right ) with tumor burden in 11 patients . 
 in patient sb11 , the presence of new somatic snvs ( brafv600e and akt1e17k ) during follow - up and upon dom suggests the value of cfdna monitoring for tumor heterogeneity after surgery . 
altogether , the longitudinal cfdna snv profiles suggest the possibility of monitoring disease through detecting the dynamic cfdna snv levels during disease - free follow - up . met and egfr cfdna amplification the recent association of cnv detection in melanoma tumors with clinical outcome and treatment response35 , 36 has yet to be clearly demonstrated in blood . 
furthermore , two of four patients with preoperative egfr / met cfdna amplification had detectable egfr / met cfdna amplification postoperatively , reflecting residual disease presence . cfdna monitoring captures tumor evolution given high tumor heterogeneity , cfdna monitoring was evaluated to determine whether dynamic or evolving tumor snv profiles can be captured , precluding the need for repetitive invasive tissue biopsies . 
 the tumor - cfdna concordance , defined as the presence of cfdna snvs in any serially collected blood sample to any matched tumors sequenced , ranged from 66% to 100% , with an average concordance of 81.5% ( appendix table a11 )  . 
 cfdna profiling in patient sb4 ( fig 5a ) captured heterogeneous tumor clones 2 to 7 months before distant metastasis biopsy , as revealed by detection of cdkn2a and braf somatic snvs in blood . 
 we focused on cfdna profiling during longitudinal follow - up at clinically relevant times , namely before curative elective surgery , during disease - free follow - up , and at relapse . 
this is critical for understanding how to use long - term longitudinal cfdna analysis to best guide management of patients with melanoma . the study explores the application of cfdna analysis in melanoma for earlier recurrence detection compared with standard radiologic imaging after surgery , and the results support previous oncologic blood cfdna studies.38 - 41 however , this study provides a novel view of cfdna snv dynamics . 
the assay containing a cancer panel that includes known melanoma driver genes minimizes the need for tumor dna sequencing to identify baseline snvs and proved advantageous in profiling dynamic cfdna snv levels , particularly for snvs not detectable at the time of surgery . 
longitudinal follow - up captured dynamic cfdna snv levels , reflecting tumor heterogeneity , and the potential increase of subclonal cfdna mutation levels upon relapse , potentially indicative for alternative treatment regimens.49 , 50 the 54cancer gene panel also permitted evaluation of cnvs and snv load and burden in melanoma blood cfdna . 
recently , the association of melanoma tumor cnvs with therapeutic outcomes has suggested their potential use for monitoring disease.36 , 37 cfdna cnv utility was evident because egfr , erbb2 , and met cfdna amplifications were detected during follow - up , suggesting that cfdna amplification has the potential to monitor for occult micrometastatic residual disease after surgery . 
this study demonstrates the feasibility of detecting cfdna amplification of metastasis driver genes in melanoma , supporting the reported associations of met / egfr amplification with tumor progression and poor outcome.51 , 52 cfdna snv load and burden were independent prognostic factors for os in stage iv patients when age , sex , and m category were not significantly different between the dichotomized groups . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . snv load and burden factors were also analyzed as continuous variables ( data not shown ) and demonstrated the same finding . 
the association of cfdna snv load or burden status with worse os supports recent findings of a high cfdna snv load ( > three snvs ) correlating with immunotherapy response.53 altogether , this highlights a cfdna snv load and burden trend that needs further validation in a larger patient cohort in a multicenter study . 
in addition , future studies are needed to determine the impact of longitudinal follow - up cfdna monitoring in patients with early - stage regional melanoma . to our knowledge , this is the first study to report blood cfdna multiplex gene analysis in patients with regional ajcc stage iii melanoma metastasis over longitudinal follow - up through dom . 
 amirali talasaz employment : guardant health leadership : guardant health stock and other ownership interests : guardant health research funding : guardant health patents , royalties , other intellectual property : guardant health travel , accommodations , expenses : guardant health dave s.b. 
hoon consulting or advisory role : guardant health acknowledgment we acknowledge dr ian hutchinson , phd , editorial services , for his support in proofreading and editing of this article , and dr yuuki iida , md , for technical assistance in preparation of the article . 
lanman and amirali talasaz , guardant health , redwood city , ca ; and shu - ching chang , medical data research center at providence saint josephs health , portland , or . supported by the dr miriam and sheldon g . 
nicholl mb , elashoff d , takeuchi h , et al : molecular upstaging based on paraffin - embedded sentinel lymph nodes : ten - year follow - up confirms prognostic utility in melanoma patients . 
wittner c , park s , rifai n , et al : circulating tumor cells and circulating tumor dna as a real time liquid biopsy approach , in rifai n ( ed ) : tietz textbook clinical chemistry and molecular diagnostics ( ed 6 )  . 
zhang j , yao yh , li bg , et al : prognostic value of pretreatment serum lactate dehydrogenase level in patients with solid tumors : a systematic review and meta - analysis . 
hoshimoto s , kuo ct , chong kk , et al : aim1 and line - 1 epigenetic aberrations in tumor and serum relate to melanoma progression and disease outcome . 
harbst k , lauss m , cirenajwis h , et al : multiregion whole - exome sequencing uncovers the genetic evolution and mutational heterogeneity of early - stage metastatic melanoma . 
hoshimoto s , shingai t , morton dl , et al : association between circulating tumor cells and prognosis in patients with stage iii melanoma with sentinel lymph node metastasis in a phase iii international multicenter trial . 
morton d , mozzillo n , thompson j , et al : an international , randomized , phase iii trial of bacillus calmette - guerin ( bcg ) plus allogeneic melanoma vaccine ( mcv ) or placebo after complete resection of melanoma metastatic to regional or distant sites . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
li h , durbin r : fast and accurate short read alignment with burrows - wheeler transfor bioinformatics 30 : 2114 - 2120 , 2014 bioinformatics 25 : 1754 - 1760 , 2009 26 . 
martens a , wistuba - hamprecht k , geukes foppen m , et al : baseline peripheral blood biomarkers associated with clinical outcome of advanced melanoma patients treated with ipilimumab . 
wilson ma , zhao f , khare s , et al : copy number changes are associated with response to treatment with carboplatin , paclitaxel , and sorafenib in melanoma . 
almodovar k , iams wt , meador cb , et al : longitudinal cell - free dna analysis in patients with small cell lung cancer reveals dynamic insights into treatment efficacy and disease relapse . 
chang ga , tadepalli js , shao y , et al : sensitivity of plasma brafmutant and nrasmutant cell - free dna assays to detect metastatic melanoma in patients with low recist scores and non - recist disease progression . 
sanmamed mf , fernndez - landzuri s , rodrguez c , et al : quantitative cell - free circulating brafv600e mutation analysis by use of droplet digital pcr in the follow - up of patients with melanoma being treated with braf inhibitors . 
tsao sc - h , weiss j , hudson c , et al : monitoring response to therapy in melanoma by quantifying circulating tumour dna with droplet digital pcr for braf and nras mutations . 
disease - free survival ( dfs ) for cellfree dna ( cfdna ) single nucleotide variant ( snv ) load and burden in patients with stage iv melanoma ( cohort 1 )  . 
the kaplan - meier curves for ( a ) two cfdna snv load groups and for ( c ) two cfdna snv burden groups with the fitted ( dashed lines ) gompertz curves . 
lennerz author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license ( continued ) purpose targeted therapy is the cornerstone of treatment of advanced egfr - mutant nonsmall - cell lung cancer ( nsclc )  . 
here , we assessed workflows designed to rapidly identify patients with actionable egfr mutations and reduce time to initiation ( tti ) of epidermal growth factor receptor ( egfr ) directed therapy . patients and methods we performed rapid testing for egfr l858r mutations and exon 19 deletions on paraffin - embedded or frozen section biopsy specimens from newly diagnosed patients with metastatic nsclc by using an egfr - specific assay ( rapid test )  . 
to determine clinical utility , we assessed concordance with ngs results , turnaround time , and tti of egfr therapy , and we evaluated reimbursement data . results between january 2015 and september 2017 , we performed 243 rapid egfr tests and identified egfr mutations in 43 patients ( 18% )  . 
escalation of the initiative into an interdisciplinary ultra - rapid next - day frozen - section workflow for highly symptomatic patients ( n = 8 ) resulted in a reduction in the median ( standard deviation ) turnaround time to 1 0.4 days and allowed several patients to initiate therapy within 1 week of biopsy . 
2018 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license : introduction nonsmall - cell lung cancer ( nsclc ) is a heterogeneous disease composed of unique molecular subsets with distinct clinical outcomes.1 , 2 multiple randomized studies have established the superiority of molecularly targeted therapies versus chemotherapy for the treatment of egfr - mutant and alk - positive nsclc.3 - 6 in other molecular subsets , single - arm studies confirm that treatment with targeted therapies can induce durable responses.7 , 8 as drugs that target these molecular drivers are approved for first - line treatment , genotyping in newly diagnosed nsclc is considered the standard of care.9 because of the need to interrogate a growing number of genes , next - generation sequencing ( ngs ) has largely replaced traditional single - gene assays.10 guidelines endorsed by oncology and pathology societies recommend that molecular testing turnaround times not exceed 10 working days.9 genotyping by ngs requires complex bioinformatics that can create treatment delays . 
we selected egfr mutant nsclc on the basis of its relatively high prevalence ( 10% to 15% ) among patients with nsclc , 12 the lack of overlap between egfr mutations and other clinically relevant molecular alterations , 13 and the fact that egfr inhibitors were readily available for hospitalized patients . 
in the first phase ( january 2015 to may 2017 ) , rapid egfr testing was performed on tissue specimens from consecutive patients diagnosed with metastatic nsclc who were never smokers / minimal smokers ( 10 pack years ) or who were hospitalized at the time of diagnosis ( data supplement )  . 
we also identified a comparator population composed of 121 patients with egfr - mutant nsclc who were diagnosed before implementation of the rapid testing ( ie , historical cohort ; data supplement )  . 
isolated nucleic acids from tumor specimens were analyzed with our ngs assay that uses anchored multiplex pcr to detect single - nucleotide variants and insertions / deletions in a target set of cancer - related genes.15 in addition , we examined fusion transcripts and met exon 14 skipping by using an rna - based ngs solid - fusion assay.15 statistical and economic analysis for contingency analyses , we used t tests , fishers exact tests , and 2 statistics . 
we defined turnaround - time from the date of accessioning to the date of reporting , and we defined tti from the date of the diagnostic biopsy to the date of ingestion of an egfr tyrosine kinase inhibitor ( tki )  . 
 for economic assessment , we reviewed line items of reimbursement data ( january 3 , 2017 , to february 8 , 2018 ) and extracted ( by payor ) the number of encounters and claim adjustment codes , and defined reimbursed as a payment greater than 0 . 
note that there is a ( variable ) delay from reporting to treatment decision and initiation of therapy because of cost coverage determination , preauthorization requirements , etc.the ultra - rapid egfr testing pathway ( pathway c ) is a multidisciplinary workflow designed to improve turnaround time using fresh tissue ( frozen sections ) to extract nucleic acids . 
among the remaining 234 patients , 23 ( 10% ) did not have ngs results because of insufficient tissue or technical failure of ngs ( data supplement )  . diagnostic utility of the rapid egfr assay improvement in turnaround time . 
first , we compared the turnaround times of the rapid and ngs assays by reviewing all specimens submitted for genotyping between july 2014 and january 2017 ( fig 2b )  . 
through ngs , we identified one additional low - level ( allelic fraction , approximately 4% ) p.l858r case , which was missed by rapid egfr testing ( fig 3 )  . 
the mutation spectrum of the tumors that underwent rapid testing is depicted in figure 3 , and the data supplement shows probabilities of therapeutically actionable variants . clinical utility of rapid egfr testing tti of tki therapy . 
p values result from t test ( age ) , fishers exact test ( sex , histology ) , or 2 test ( ethnicity , smoking )  . * includes the patient with a false - negative egfr - positive result . tki as the primary measure of clinical utility of the rapid egfr test . 
we reviewed the medical records of the 39 patients with egfr - mutant disease who underwent both rapid testing and ngs to determine whether tki therapy was initiated before ngs results . 
 validation implementation of rapid egfr testing ngs panel rapid wt rapid mut rapid egfr assay rapid egfr assay exon 19 exon 20 exon 21 del / ins t790m l858r variant fig 2 . 
scatter plots portray turnaround times of all 243 rapid egfr samples ( jan 2015 to may 2017 ; black , egfr wild type [ wt ] ; red , egfr mutation [ mut ] detected ) and all specimens that underwent ngs ( gray dots ) during this period . 
a case report of a patient who benefitted from this effort and a summary of the experience to date are described in the next section . therapeutic utility of ultra - rapid testing . 
osimertinib was selected on the basis of its activity against leptomeningeal disease.19 within days , the cough resolved , and the patient experienced marked improvement in his swallowing and regained the ability to walk . 
figure 4d illustrates the difference in turnaround time for the rapid and ultra - rapid tests and the time to initiation of tki therapy for patients tested through each workflow ( fig 4d inset )  . 
the sites of disease and presenting symptoms of these patients are detailed in the data supplement , which also summarizes our ultra - rapid workflow . rapid testing is operationally and financially sustainable . 
the heatmap portrays clinicopathologic features ( top three rows ) , rapid egfr results , and key molecular drivers along with the results of next generation sequencing ( ngs ) based fusion detection , fluorescence in - situ hybridization ( fish ) , and ngs panel results . 
key findings include ( 1 ) an isolated false - negative rapid egfr result ( arrow ) , ( 2 ) the inability of the rapid egfr test to detect egfr mutations at other residues , ( 3 ) identification of at least one underlying driver mutation in more than 50% of all tested cases by using the integrated molecular diagnostic approach , and ( 4 ) the association between clinicopathologic features and certain key drivers ( eg , never - smoking women with adenocarcinoma and egfr v > 10 pack - year smoking history and kras )  . 
 review of 214 clinical encounters with 1 , 475 line items of reimbursement data showed large variability between payors ( range , 0% to 100% ) and that , overall , 63% of encounters received reimbursement ( fig 4f )  . 
these data indicate that rapid egfr testing in our practice is operationally and financially sustainable . discussion here , we report the results of a quality improvement initiative to explore parallel testing with a rapid egfr assay and ngs in newly diagnosed nsclc . 
our findings emphasize the diagnostic , clinical , and therapeutic utility of rapid egfr testing . metastatic nsclc is a devastating and incurable disease for which the prognosis is highly dependent on identification of actionable molecular drivers.2 the established efficacy of us food and drug administrationapproved targeted therapies in specific nsclc subsets and the increasing number of investigational compounds underscore the necessity of identification of molecular alterations in a timely fashion . 
 ( a ) event curve that shows rapid egfr test reporting times and a comparison of the tyrosine kinase inhibitor ( tki ) initiation times ( relative to date of diagnosis ) for patients in the rapid and historical cohorts . 
the second block shows the 49% of patients ( n = 17 of 35 patients ) with egfr - mutant disease who started a tki before next - generation sequencing ( ngs ) results were available . 
 ( c ) response to the egfr inhibitor osimertinib in a patient with nonsmall - cell lung cancer who underwent ultra - rapid egfr testing : ( left ) pretreatment image and ( right ) response after 3 weeks ; arrow indicates primary tumor . 
 ( d ) comparison of rapid test times ( average ) and the eight patients tested with the ultra - rapid protocol ( fig 1c ) ; inset shows event curve comparison of time to initiation of tki between the rapid and ultra - rapid subsets . 
 ( e ) turnaround times for rapid ( gray ) and ultra - rapid ( blue ) workflows in a 9 - month extended standardof - care evaluation phase ; red , cases with an egfr mutation . 
several studies suggest that genotyping with multiple single - gene assays may reduce reporting time20 , 21 ; however , selective interrogation of the ever - expanding set of targets is impractical and may be limited by tissue availability.22 at the time our initiative began , consensus guidelines supported testing newly diagnosed patients with nsclc for egfr mutations and rearrangements in alk and ros1.9 these mutually exclusive genetic alterations are predominantly found in neveror light - smokers.13 , 23 testing these alterations in two stages ( ie , restriction of testing for rearrangements to patients whose disease is wild type for egfr mutations ) may lead to unnecessary delays between diagnosis and initiation of treatment for a significant proportion of patients and potentially steer symptomatic patients away from molecularly targeted treatments . 
through co - testing , we detected alk and ros1 rearrangements in 11 and six patients , respectively , and identified molecular alterations with promising investigational therapies in more than 40 additional patients ( fig 3 )  . 
for example , in a recent retrospective analysis that involved 15 community oncology centers , the median turnaround time for egfr testing and ngs was 23 days and 30 days , respectively.24 although this practice is likely more common in the community setting , where in - house testing is infrequent , one study demonstrated that 19% of patients with egfr mutations or alk rearrangements at an academic medical center in canada initiated first - line chemotherapy before testing results became available.11 the sequence of therapies may be particularly important for those patients initially treated with immunotherapy , because recent studies demonstrate that immunotherapy is seldom effective for egfr - mutant nsclc and that treatment with immunotherapy before targeted therapy increases the likelihood of the development of significant toxicities.25 - 27 given these data , we believe that rapid testing should be performed in parallel with full ngs genotyping . with a parallel - testing approach , we successfully performed rapid testing and ngs in 90% of patients in our initiative with material from a single biopsy . 
because half of the patients with tissue / dna that was insufficient for the full ngs were effectively tested for both alk and ros1 rearrangements using either fluorescence in - situ hybridization or the fusion assay , 95% of the patients in the rapid cohort met the minimum molecular testing requirement proposed by current asco guidelines . 
although pcr - based plasma genotyping is an expedient alternative to ngsbased tissue genotyping , the sensitivity of liquid biopsy for detection of egfr mutations is lower than what we report here with the rapid assay.29 , 30 despite the high sensitivity and specificity of the rapid assay , half of the patients in our study did not start tki therapy before ngs results were available ( fig 4b )  . 
 because tti was assessed retrospectively for the historical cohort , the median of 37 days between diagnosis and tki therapy might be an overestimate ; however , a similar delay was observed in another study.31 it also is conceivable that the difference in tti might be explained by process improvements over time that have shortened the interval between requests for and receipt of a drug from specialty pharmacies . 
because tki use predated ngs results in approximately 50% of patients , the reduction in time to tki initiation in the rapid group relative to the historical cohort might also reflect faster ngs reporting times . 
the scale of ngs panels currently precludes significant reduction , and the median and mean turnaround times for ngs results in the ultrarapid cohort were 9 and 10 days , respectively . 
 as a result of the short duration of follow - up of our rapid cohort and imbalances between the rapid and historical groups ( including enrollment of patients in the rapid cohort into a consolidation radiation protocol ) , we were unable to evaluate differences in progression - free survival on egfr - directed therapy . 
lennerz the potential to defer brain radiation for these patients underscore the importance of rapid identification of egfr mutations.41 , 42 the small number of patients with egfr - mutant disease in our study also limits the potential impact of our findings . 
however , many laboratories are proficient in performing targeted egfr genotyping , 43 and our extended standard of care evaluation ( fig 4e ) and reimbursement analysis ( fig 4f ) indicate operational and financial sustainability . in summary , we demonstrate that expedited egfr genotyping enables early intervention with targeted therapies and allows symptomatic patients to access effective treatments . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ibiayi dagogo - jack honoraria : foundation medicine consulting or advisory role : boehringer ingelheim administrative support : christopher g . 
farago honoraria : foundation medicine vania nose no relationship to disclose consulting or advisory role : pharmamar , takeda , abbvie , loxo , stemcentrx research funding : pharmamar ( inst ) , abbvie ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , loxo ( inst ) , ignyta ( inst ) miguel rivera consulting or advisory role : loxom asubio ( i ) speakers ' bureau : pfizer ( i ) research funding : advanced cell diagnostics , affymetrix travel , accommodations , expenses : pharmamar , abbvie , stemcentrx patents , royalties , other intellectual property : patents with affymetrix justin f . 
gainor honoraria : merck , incyte , ariad , novartis , pfizer consulting or advisory role : genentech , bristol - myers squibb , theravance , loxo , takeda , array biopharma , amgen research funding : merck ( inst ) , novartis ( inst ) , genentech , bristol - myers squibb ( inst ) , adaptimmune ( inst ) , astrazeneca ( inst ) , ariad , jounce therapeutics ( inst ) , blueprint medicines ( inst ) , moderna therapeutics ( inst ) , tesaro ( inst ) travel , accommodations , expenses : affymetrix ginger jiang employment : novartis ( i ) zofia piotrowska consulting or advisory role : boehringer ingelheim , astrazeneca , ariad , takeda , superdimension , guardant health , novartis , abbvie research funding : novartis ( inst ) , ariad ( inst ) , takeda ( inst ) , guardant health ( inst ) rebecca s . 
heist consulting or advisory role : boehringer ingelheim research funding : abbvie ( inst ) , novartis ( inst ) , roche ( inst ) , incyte ( inst ) , celgene ( inst ) , mirati therapeutics ( inst ) , peregrine pharmaceuticals ( inst ) , exelixis ( inst ) , millenium ( inst ) , debiopharm group ( inst ) , corvus pharmaceuticals ( inst ) valentina nardi stock and other ownership interests : ksq therapeutics ( i ) , navicor ( i ) consulting or advisory role : thermo fisher scientific ( i ) , cell signaling technology ( i ) , raze ( i ) , caloric tests ( i ) dora dias - santagata no relationship to disclose long p . 
le stock and other ownership interests : archer biosciences consulting or advisory role : archer biosciences patents , royalties , other intellectual property : i am a co - inventor of the anchored multiplex pcr technology which is licensed to archerdx . 
sequist honoraria : astrazeneca consulting or advisory role : astrazeneca , genentech , roche , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , merck ( inst ) , pfizer ( inst ) , guardant health ( inst ) , incyte ( inst ) martha pitman consulting or advisory role : medtronic inga t . 
shaw honoraria : pfizer , novartis , roche , genentech , foundation medicine consulting or advisory role : pfizer , novartis , genentech , roche , ariad , ignyta , blueprint medicines , daiichi sankyo , emd serono , taiho pharmaceutical , kso therapeutics , natera , loxo , takeda research funding : pfizer , novartis , roche , genentech , a . 
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leighl nb , rekhtman n , biermann wa , et al : molecular testing for selection of patients with lung cancer for epidermal growth factor receptor and anaplastic lymphoma kinase tyrosine kinase inhibitors : american society of clinical oncology endorsement of the college of american pathologists / international association for the study of lung cancer / association for molecular pathology guideline . 
gainor jf , varghese am , ou sh , et al : alk rearrangements are mutually exclusive with mutations in egfr or kras : an analysis of 1 , 683 patients with nonsmall - cell lung cancer . 
dias - santagata d , akhavanfard s , david ss , et al : rapid targeted mutational analysis of human tumours : a clinical platform to guide personalized cancer medicine . 
gainor jf , niederst mj , lennerz jk , et al : dramatic response to combination erlotinib and crizotinib in a patient with advanced , egfr - mutant lung cancer harboring de novo met amplification . 
yang jc - h , cho bc , kim d - w , et al : osimertinib for patients ( pts ) with leptomeningeal metastases ( lm ) from egfr - mutant nonsmall - cell lung cancer ( nsclc ) : updated results from the bloom study . 
barlesi f , mazieres j , merlio jp , et al : routine molecular profiling of patients with advanced non small - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
distasio m , chen y , rangachari d , et al : molecular testing turnaround time for nonsmallcell lung cancer in routine clinicalpractice confirms feasibility of cap / iaslc / amp guideline recommendations : a single - center analysis . 
drilon a , wang l , arcila me , et al : broad , hybrid capture - based next - generation sequencing identifies actionable genomic alterations in lung adenocarcinomas otherwise negative for such alterations by other genomic testing approaches . 
garassino mc , cho bc , kim jh , et al : durvalumab as third - line or later treatment for advanced nonsmall - cell lung cancer ( atlantic ) : an open - label , single - arm , phase 2 study . 
lee ck , man j , lord s , et al : clinical and molecular characteristics associated with survival among patients treated with checkpoint inhibitors for advanced nonsmall - cell lung carcinoma : a systematic review and meta - analysis . 
sholl lm , aisner dl , varella - garcia m , et al : multi - institutional oncogenic driver mutation analysis in lung adenocarcinoma : the lung cancer mutation consortium experience . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
lee ck , davies l , wu yl , et al : gefitinib or erlotinib vs chemotherapy for egfr mutation positive lung cancer : individual patient data meta - analysis of overall survival . 
yang jc , wu yl , schuler m , et al : afatinib versus cisplatin - based chemotherapy for egfr mutationpositive lung adenocarcinoma ( lux - lung 3 and lux - lung 6 ) : analysis of overall survival data from two randomised , phase 3 trials . 
vergnenegre a , massuti b , de marinis f , et al : economic analysis of first - line treatment with erlotinib in an egfr - mutated population with advanced nsclc . 
ting j , tien ho p , xiang p , et al : cost - effectiveness and value of information of erlotinib , afatinib , and cisplatin - pemetrexed for first - line treatment of advanced egfr mutationpositive nonsmall - cell lung cancer in the united states . 
lu s , ye m , ding l , et al : cost - effectiveness of gefitinib , icotinib , and pemetrexed - based chemotherapy as first - line treatments for advanced nonsmall - cell lung cancer in china . 
handorf ea , mcelligott s , vachani a , et al : cost effectiveness of personalized therapy for firstline treatment of stage iv and recurrent incurable adenocarcinoma of the lung . 
isla d , de castro j , juan o , et al : costs of adverse events associated with erlotinib or afatinib in first - line treatment of advanced egfr - positive nonsmall - cell lung cancer . 
park k , tan eh , obyrne k , et al : afatinib versus gefitinib as first - line treatment of patients with egfr mutationpositive nonsmall - cell lung cancer ( lux - lung 7 ) : a phase 2b , open - label , randomised controlled trial . 
schuler m , wu yl , hirsh v , et al : first - line afatinib versus chemotherapy in patients with non small - cell lung cancer and common epidermal growth factor receptor gene mutations and brain metastases . 
goss g , tsai cm , shepherd fa , et al : cns response to osimertinib in patients with t790mpositive advanced nsclc : pooled data from two phase ii trials . 
 o real - time genomic characterization of metastatic pancreatic neuroendocrine tumors has prognostic implications and identifies potential germline actionability purpose we assessed the usefulness of real - time molecular profiling through next - generation sequencing ( ngs ) in predicting the tumor biology of advanced pancreatic neuroendocrine tumors ( pannets ) and in characterizing genomic evolution . methods patients with metastatic pannets were recruited in the routine clinical practice setting ( between may 2014 and march 2017 ) for prospective ngs of their tumors as well as for germline analysis using the memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) sequencing platfor when possible , ngs was performed at multiple time points . results ngs was performed in 96 tumor samples from 80 patients . 
sequencing of preand post - treatment samples revealed tumor - grade progression ; clonal evolution patterns were also seen ( molecular resistance mechanisms and chemotherapy - associated mutagenesis )  . 
germline genetic analysis identified clinically actionable pathogenic or likely pathogenic variants in 14 of 88 patients ( 16% ) , including mutations in high - penetrance cancer susceptibility genes ( men1 , tsc2 , and vhl )  . conclusion a clinical ngs platform reveals pertubations of biologic pathways in metastatic pannets that may inform prognosis and direct therapies . 
2018 by american society of clinical oncology introduction pancreatic neuroendocrine tumors ( pannets ) represent 1% to 2% of all pancreatic neoplasms , but they have a rising incidence and prevalence.1 - 4 whole - exome and whole - genome sequencing , largely of resected pannets , has defined genomic events and improved our understanding of disease pathogenesis.5 , 6 these efforts have identified changes in chromatin remodeling , telomere maintenance , and mammalian target of nitya raj ronak shah zsofia stadler semanti mukherjee joanne chou brian untch janet li virginia kelly muyinat osoba leonard b . 
in addition to the well - characterized hereditary syndromes associated with pannet development ( multiple endocrine neoplasia 1 , von hippel - lindau syndrome , neurofibromatosis type 1 ) , recent data suggest the presence of germline alterations in dna damage repair genes in some patients.6 , 7 treatments for unresectable pannets include targeted and cytotoxic therapies , as well as liver directed approaches.8 - 13 no data exist to guide therapy for pannets with defined genomic alterations . 
in addition , disease heterogeneity poses a significant challenge in defining the selection and sequencing of therapy . to that end , using an institutional matched tumor - normal platform , we prospectively performed next - generation sequencing ( ngs ) of tumors in patients with metastatic well differentiated ( wd ) pannets . 
 we also hypothesized that pannets evolve over time with a more aggressive behavior that could be characterized biologically through ngs of repeat biopsies after treatment . methods study population written informed consent was obtained from patients with a diagnosis of wd pannet using a prospective , institutional review board approved protocol ( clinicaltrials.gov identifier : nct01775072 )  . 
pathologic features of the tumor samples ( differentiation and grade ) were determined according to the 2017 who classification , which recognizes the existence of a grade 3 ( g3 ) category within wd pannets ; historical values for differentiation and grade were collected through review of the electronic medical records . 
electronic medical records were also reviewed for patient data on demographics , treatments , and survival . sequencing of tumor samples ngs was performed using memorial sloan ketteringintegrated mutation profiling of actionable cancer targets ( msk - impact ) , a matched tumor - normal sequencing platform approved for clinical use by the new york state department of health , to detect base substitutions , small indels , copy number changes , and selected gene rearrangements.14 - 17 updated assay versions were released between 2014 and 2017 , and ngs of tumor tissue consisted of deep sequencing of all exons and selected introns of 275 ( preclinical pilot test ) , 341 ( version 1 ) , 410 ( version 2 ) , or 468 ( version 3 ) cancer - related genes . 
genotyping was performed using the pilot test for two of 96 samples ( 2% ) , version 2 for 16 of 96 samples ( 17% ) , version 3 for 57 of 96 samples ( 59% ) , and version 4 for 21 of 96 samples ( 22% )  . 
actionable genetic alterations were defined as changes that could guide therapy , including standard of care and investigational treatments ( annotated according to oncokb ) .18 germline sequencing germline variants from the .bam file of the normal dna sequence were called using the mutect and gatk haplotype caller as described previously ; all variants with < 1% population frequency in the exome aggregation consortium database were interpreted.19 , 20 germline analysis included 76 genes known to be associated with hereditary cancer predisposition , including all cancer predisposition genes identified in the american college of medical genetics and genomics guidelines.19 , 21 , 22 variants were interpreted on the basis of american college of medical genetics and genomics criteria . loss of heterozygosity loss of heterozygosity ( loh ) was determined through analysis of total , allele - specific , and integer dna copy number genome - wide using facets.23 statistical analysis descriptive statistics were used to characterize the study population and the somatic and germline genetic results . 
overall survival ( os ) , defined as the time from the date of first tissue acquisition ( from which ngs was completed ) until death or last known follow - up , was estimated by kaplan - meier methods . 
all p values were two sided , and p < .05 was considered to indicate statistical significance . results clinical characteristics as of march 2017 , ngs had been performed on 96 tumor samples from 80 patients ( eight patients with two samples analyzed ; four patients with three samples analyzed )  . 
in 29 patients , the primary tumor was sequenced , and in 58 patients , a metastatic tumor was sequenced ; in seven patients , both primary and metastases were sequenced ( in one instance , sequencing took place synchronously )  . 
recurrent somatic alterations occurred in key pathways and functional groups : chromatin remodeling factors ( crfs ) , histone methyltransferases ( hmts ) , and mtor pathway genes . somatic alterations in crfs ( daxx , atrx , pbrm1 , smarcb1 , arid5b , arid2 , arid1b , and arid1a ) were observed in 52 of 80 patients ( 65% )  . 
baseline patient characteristics ( continued ) wd pannets with msk - impact results systemic therapy somatostatin analogs ( octreotide long - acting release or lanreotide ) everolimus sunitinib platinum drug chemotherapy alkylating drug chemotherapy peptide receptor radionuclide therapy hepatic arterial embolization ( bland , radiotherapy , or chemotherapy ) 58 ( 73 ) 29 ( 36 ) 8 ( 10 ) 18 ( 23 ) 46 ( 58 ) 12 ( 15 ) 35 ( 44 ) note . 
 the clinical behavior of these tumors , including the single g1 tumor , was more aggressive . ten tumor samples ( collected from six patients ) harbored braf alterations : two of 10 g1 ( 20% ) , three of 10 g2 ( 30% ) , and five of 10 g3 ( 50% )  . 
 in addition to two tumors with v600e mutations , several non - v600 braf alterations were seen ( k601e , t599k , and t310i ) , and one tumor expressed both braf g596d and e451k mutations . survival with a median follow - up for survivors of 27.6 months , we observed 14 deaths ; median os was 118.9 months ( 95% ci , 99.6% - not achieved )  . 
tp53 alterations were observed in 10 of 80 patients ( 13% ) ; all were characterized as likely oncogenic . somatic loh in 50% of the genome was highly prevalent ; it was identified in 55 of 95 tested samples ( 58% )  . 
loh was observed recurrently in chromosomes 1 , 2 , 3 , 6 , 8 , 10 , 11 , 15 , 16 , 21 , and 22 ( appendix fig a1 )  . ngs results for the first sequenced sample in all patients are summarized in figure 1 . 
in the recurrently altered genes , there were no statistical differences in genetic spectrum on the basis of g1 versus g2 tumors , but a trend was noted of g2 and g3 tumors harboring tp53 , setd2 , and braf alterations . novel recurrently altered genes in this metastatic cohort , we observed a much higher frequency of setd2 alterations ( 14 of 80 patients [ 18% ] ) in comparison with previous investigations , and a novel finding of braf molecular mechanisms of resistance . 
genomic landscape of pancreatic neuroendocrine tumors , including the first sequenced sample for each patient ( n = 80 ) , as identified by the memorial sloan kettering - integrated mutation profiling of actionable cancer targets . 
 loh , loss of heterozygosity ; mb , megabyte ; mtor , mammalian target of rapamycin . post - treatment samples were available for three patients receiving the mtor inhibitor everolimus and for one patient receiving the braf v600e inhibitor vemurafenib . in all three patients receiving everolimus , mtor pathway alterations were identified at progression . 
on disease progression , a biopsy specimen revealed an oncogenic pten mutation ( q298 * ) , and the sampled areas of tumor progressed from g1 to g3 ( appendix figure a2 )  . 
this pten mutation was seen previously at a low allele frequency when the original pancreas tumor was sequenced , reflecting the possible emergence of this clone through targeted therapy . patient 2 received everolimus for 8 weeks , at which point treatment was held for infectious complications . 
a liver lesion increased in size and a biopsy was performed ; ngs identified a hotspot mutation in rheb ( y35s ) .25 subsequent sampling and ngs of this same liver lesion after 16 months of observation demonstrated the rheb alteration at a higher allele frequency . 
the msk - impact version used to sequence the pretreatment sample did not interrogate rheb , so the allele fraction of the rheb mutation is unknown in this sample ; however , it increased notably after treatment with andprogression on everolimus . patient 3 received everolimus for > 9 months before disease progression . 
at disease progression , ngs of a growing liver lesion demonstrated loss of this igf2 alteration , acquisition of a tsc2 splice site mutation ( x161_ splice ) , and an akt2 mutation ( g16d ; appendix figure a4 )  . 
surprisingly , no shared mutations were noted in sequencing of the two samples ; clinically , however , the disease was consistent with a single primary , suggesting the emergence of a previously unrecognized clone through treatment , although the possibility of a second primary cannot be excluded . patient 4 , whose tumor harbored a braf v600e mutation , enrolled in a basket clinical trial with vemurafenib and developed an nras hotspot mutation ( q61r ; appendix figure a5 ) .26 chemotherapy - associated mutagenesis . 
two patients received alkylating agents , and the third received oxaliplat a review of the tumors exposed to alkylating drugs showed that the variants shared by both samples were observed at a higher allele fraction compared with those unique to the individual samples , and the evolutionary pattern demonstrated a predominant c > t signature consistent with alkylating - agent associated mutagenesis ; in addition , consistent with previous observations , acquired alterations were observed in the mismatch repair genes for both tumors ( fig 3 ) .27 - 29 the sampled tumor in both patients increased from g1 to g3 . germline genetic testing germline testing for 76 cancer - associated genes was performed in 88 patients , 78 in the original prospective cohort and an additional 10 with surgically resected pannets . 
fourteen likely pathogenic germline alterations were identified in known cancer susceptibility genes ( 16% ) : three in established high - penetrance genes ( men1 , vhl , and tsc2 [ 3% ] ) , four in moderate - penetrance genes ( chek2 in four patients [ 5% ] ) , and seven in low - penetrance genes ( monoallelic mutyh in four patients and apc i1307k in three patients [ 8% ] )  . 
notably , we identified a germline tsc2 mutation in a 32 - year - old patient who did not exhibit the classic clinical features of tuberous sclerosis complex ( tsc ) and did not meet the criteria for tsc genetic testing ; magnetic resonance imaging of the brain identified tubers and radial bands , typical of tsc ( appendix figure a6 )  . 
among these patients , as best therapy response , two of 12 ( 17% ) had tumor regression , six of 12 ( 50% ) had stable disease , and one of 12 ( 8% ) had progressive disease ; three of 12 ( 25% ) are still receiving treatment . 
in the remaining 46 patients without somatic mtor pathway alterations , 17 of 46 ( 37% ) received everolimus ; five of 17 ( 29% ) had tumor regression , seven of 17 ( 41% ) had stable disease , four of 17 ( 24% ) had progressive disease , and there was an unknown response in one patient ( lost to follow - up )  . 
results from ngs led to the enrollment of three patients into clinical trials , but with little response noted . to our knowledge , this is the first study to evaluate the real - time clinical usefulness of ngs for patients with advanced , metastatic pannets . 
setd2 alterations have been implicated in the pathogenesis of many cancers ( breast , lung , acute lymphoblastic leukemia , renal cell carcinoma , and gliomas ) , supporting a role for setd2 as a tumor suppressor across many diseases.34 - 41 given our findings , one might consider closer monitoring and / or cytotoxic therapies in patients with setd2or table 3 . 
levels 1 and 2a include food and drug administration ( fda ) - recognized and standardof - care biomarkers predictive of response to an fda - approved drug for pancreatic neuroendocrine tumors . 
level 2b includes fda - approved biomarkers predictive of drug response in another cancer , but not fda or national comprehensive cancer network - compendium listed for pancreatic neuroendocrine tumors . 
level 3a includes alterations for which clinical evidence links the biomarker to drug response for pancreatic neuroendocrine tumors , but neither the biomarker nor the drug are standard of care in any cancer type . 
level 3b includes alterations for which clinical evidence links the biomarker to drug response for other cancers , but neither the biomarker nor the drug are standard of care in any cancer type . 
level 4 includes alterations in which preclinical evidence potentially links the biomarker to drug response , but neither the biomarker nor the drug are standard of care in any cancer type . abbreviation : msk - impact , memorial sloan kettering - integrated mutation profiling of actionable cancer targets . high penetrance high penetrance high penetrance moderate penetrance moderate penetrance moderate penetrance low penetrance low penetrance low penetrance recessive allele recessive allele braf - altered tumors and a higher burden of disease earlier in the treatment course . our study identifies pertubations of biologic pathways in metastatic pannets that were found in previous whole - exome and whole genome studies evaluating mostly localized pannets.5 , 6 we observed alterations largely along three pathways : crfs , hmts , and mtor . 
our study clarifies pannet genetics exclusively in the metastatic cohort , the group which gains immediate clinical value from realtime sequencing as we make steps toward precision medicine . in addition , we found that 16% of patients harbored a germline pathogenic or likely pathogenic alteration in high - , moderate - , or low - penetrance cancer predisposition genes . 
in looking at those patients found to have mutations in low or moderate - penetrance genes , it is notable that both chek2 and monoallaleic mutyh were noted in previous germline assessments of patients with pannets.6 notably , the patient in our series with a tsc2 germline mutation did not meet the clinical criteria for tsc genetic testing ; the identification of this mutation was incidental . 
 because mutations in men1 and tsc2 are two of the most common somatic findings in pannets , our finding of germline mutations within these two high - penetrance genes demonstrates the importance of these genes in pannet pathogenesis . 
although the contribution of the other germline alterations to pannet susceptibility has yet to be elucidated , our data suggest that there is likely a larger - than - anticipated germline contribution in this disease . 
given the lack of predictable phenotypic findings in most highand moderate - risk mutation carriers , combined with the relative rarity of this tumor subtype , consideration of genetic risk assessment for all patients with pannets is not unreasonable . 
such germline findings would have a profound impact on long - term cancer surveillance and cascade genetic testing of at - risk family members . in a small number of patients , somatic mutational signatures guided therapy . 
we identified somatic mtor alterations in a much greater proportion of patients ( 43% ) than described previously , but the presence or absence of an mtor pathway mutation was not predictive of response or resistance to treatment.8 our numbers are small , however , so additional work is needed to clarify the role of mtor pathway alterations in predicting response and / or resistance to targeted mtor pathway inhibitors . our series included only patients with wd tumors , and consistent with previous findings , rb1 alterations were essentially absent and were observed in only one post - treatment sample exposed to chemotherapy.43 , 44 wd pannets are often thought of as cancer in slower motion , and we have used our sequencing efforts to help clarify pannet evolutionary patterns over time and through therapy . 
in the 12 patients who underwent ngs of tumor tissue at multiple time points , we noted increased tumor grade in eight patients ( 67% ) , associated with marked genetic evolution after treatment . 
to our knowledge , we are the first to observe this evolutionary pattern in pannets.27 - 29 in conclusion , comprehensive molecular profiling of pannet samples using archival tissue is feasible . 
in a disease in which the natural history is thought to be indolent , we have demonstrated that the cancer transforms with grade and genetic progression over time and as therapy progresses . 
the practical usefulness of this analysis remains limited at this time ; our data suggest a higher - than - expected germline mutation rate , and consideration of genetic risk assessment for all patients with pannets is reasonable . 
in addition , given the heterogeneity of the disease , rapid , readily available , and clinically feasible ngs should be considered in clinical trials to help stratify these patients . 
specifically , our numbers are too small to clarify the genetic predictors of response or resistance to commonly used therapies in pannets , the prognostic effects of the identified genetic alterations , or the patterns of genetic evolution ( because only 12 patients underwent sequencing at multiple time points )  . 
klimstra , diane reidy - lagunes financial support : nitya raj , diane reidy - lagunes administrative support : nitya raj , joanne chou , virginia kelly , diane reidy - lagunes provision of study material or patients : nitya raj , leonard b . 
 data analysis and interpretation : nitya raj , ronak shah , zsofia stadler , semanti mukherjee , joanne chou , brian untch , janet li , muyinat osoba , leonard b . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . nitya raj research funding : novartis ( inst ) ronak shah no relationship to disclose leonard b . 
saltz consulting or advisory role : mcneil ppc ( i ) research funding : taiho pharmaceutical diana mandelker no relationship to disclose marc ladanyi honoraria : merck ( i ) consulting or advisory role : nccn / boehringer ingelheim afatinib targeted therapy advisory committee , national comprehensive cancer network / astrazeneca tagrisso request for proposal advisory committee research funding : loxo ( inst ) michael f . 
berger research funding : illumina zsofia stadler consulting or advisory role : allergan ( i ) ; genentech ( i ) , regeneron pharmaceuticals ( i ) , optos ( i ) , adverum ( i ) david s . 
klimstra stock and other ownership interests : paige.ai consulting or advisory role : wren laboratories , ipsen semanti mukherjee employment : regeneron pharmaceuticals stock and other ownership interests : regeneron pharmaceuticals research funding : regeneron pharmaceuticals diane reidy - lagunes honoraria : novartis consulting or advisory role : ipsen , pfizer , novartis research funding : novartis acknowledgment the authors thank the patients who kindly agreed to participate in this research effort . joanne chou no relationship to disclose brian untch no relationship to disclose support prior presentation affiliations nitya raj , ronak shah , zsofia stadler , semanti mukherjee , joanne chou , brian untch , janet li , virginia kelly , muyinat osoba , leonard b . 
presented , in part , as poster presentations at the 2015 gastrointestinal cancers symposium ( san francisco , ca , january 15 - 17 , 2015 ) and 2016 gastrointestinal cancers symposium ( san francisco , ca , january 21 - 23 , 2016 )  . 
dasari a , shen c , halperin d , et al : trends in the incidence , prevalence , and survival outcomes in patients with neuroendocrine tumors in the united states . 
yao jc , hassan m , phan a , et al : one hundred years after carcinoid : epidemiology of and prognostic factors for neuroendocrine tumors in 35 , 825 cases in the united states . 
yao jc , phan at , chang dz , et al : efficacy of rad001 ( everolimus ) and octreotide lar in advanced lowto intermediate - grade neuroendocrine tumors : results of a phase ii study . 
yao jc , lombard - bohas c , baudin e , et al : daily oral everolimus activity in patients with metastatic pancreatic neuroendocrine tumors after failure of cytotoxic chemotherapy : a phase ii trial . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
wagle n , berger mf , davis mj , et al : high - throughput detection of actionable genomic alterations in clinical tumor samples by targeted , massively parallel sequencing . 
cheng dt , prasad m , chekaluk y , et al : comprehensive detection of germline variants by mskimpact , a clinical diagnostic platform for solid tumor molecular oncology and concurrent cancer predisposition testing . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
kim jy , brosnan - cashman ja , an s , et al : alternative lengthening of telomeres in primary pancreatic neuroendocrine tumors is associated with aggressive clinical behavior and poor survival . 
singhi ad , liu tc , roncaioli jl , et al : alternative lengthening of telomeres and loss of daxx / atrx expression predicts metastatic disease and poor survival in patients with pancreatic neuroendocrine tumors . 
marinoni i , kurrer as , vassella e , et al : loss of daxx and atrx are associated with chromosome instability and reduced survival of patients with pancreatic neuroendocrine tumors . 
piva f , santoni m , matrana mr , et al : bap1 , pbrm1 and setd2 in clear - cell renal cell carcinoma : molecular diagnostics and possible targets for personalized therapies . 
liu l , guo r , zhang x , et al : loss of setd2 , but not h3k36me3 , correlates with aggressive clinicopathological features of clear cell renal cell carcinoma patients . 
walter dm , venancio os , buza el , et al : systematic in vivo inactivation of chromatin - regulating enzymes identifies setd2 as a potent tumor suppressor in lung adenocarcinoma . 
tang lh , basturk o , sue jj , et al : a practical approach to the classification of who grade 3 ( g3 ) well - differentiated neuroendocrine tumor ( wd - net ) and poorly differentiated neuroendocrine carcinoma ( pd - nec ) of the pancreas . 
yachida s , vakiani e , white cm , et al : small cell and large cell neuroendocrine carcinomas of the pancreas are genetically similar and distinct from well - differentiated pancreatic neuroendocrine tumors . 
tbt reimbursement within the united states in the current regulatory environment is not tied to premarket evidence of clinical utility , resulting in a vicious cycle wherein low - level evidence of utility leads to poor reimbursement , thereby impeding investment in developing new , clinically valuable tbts supported by high - level evidence . 
precise one - to - one mapping of reimbursement to cost savings or cost effectiveness is precluded by an absence of formal cost - effectiveness analyses for many emerging tbts , and for more established tbts , it has become clear that such analyses may yield wildly variable , subjective estimates . 
to address these challenges , we propose a system of tiered reimbursement that rewards development of high - quality tbts within specic use contexts , supported by strong evidence of analytic validity and clinical utility . 
we propose three use contexts of tbts , each dened by its inuence on treatment decisions relative to the current standard of careopt - out , opt - in , and the use of appropriate , alternative , effective therapies ( opt - alt )  . 
the true clinical utility of a tbt is often difcult to determine , initiating a vicious cycle in which tbts are often undervalued and poorly reimbursed because of a lack of high - level evidence of clinical utility.1 an inconsistent regulatory and reimbursement environment results in an unfavorable return on investment in the research and development ( r&d ) needed to generate the high levels of evidence ( loes ) necessary to demonstrate the clinical utility of tbts.1 indeed , despite increasing recognition of the benets of personalized medicine , medicare coverage of many emerging tbts is being signicantly reduced or denied , 2 resulting in decreased investment in tbt r&d.3 reimbursement of tbts to date has been driven primarily by a combination of commodity and labor pricing ( ie , reagent and technical costs ) , market forces , and perceived clinical value . 
this is not an effective strategy to support long - term investment in high - quality tbts . we propose that objective and transparent tiers of tbt value be created based on high loes of analytic validity ( ie , accurate and reproducible measurement of a specic analyte ) and clinical utility ( ie , improves patient outcomes ) that meet minimal specied thresholds and address unmet medical needs.4 , 5 our proposal would potentially result in redistribution of health care dollars currently spent on needless or ineffective therapies while ensuring that patients who require and are likely to benet from treatment strategies receive theit will create pathways by which tbt manufacturers could receive guaranteed minimum rates of reimbursement ( fig 1 ) and thereby increase the likelihood that tbt developers obtain a return on r&d investment . 
we propose an alternative , value - based reimbursement which clinical utility can be assessed within specic use contexts , undergo formal review , and then provide a new value - based , tiered reimbursement rate . 
note that the use of appropriate , alternative , effective therapies ( opt - alt ) context includes both the initial treatment and the monitoring paradigms . fda , us food and drug administration ; icers , cost - effectiveness ratios ; qaly , quality - adjusted life - year . dinan et al proposed valuation status quo / conventional pricing holder of tbt seeks higher , value - based reimbursement value - based application to set new reimbursement cost - saving tbts opt - out evidence to reduce treatment % treatment reduction treatment cost pricing : function of costs saved cost - effective tbts evidence of beneficial treatment treatment outcomes ( qalys ) treatment costs pricing : function of icers opt - in opt - alt approved : new value - based reimbursement set formal review by fda or other regulatory body loes of robustness in the assay itself and that its use improves patient outcomes compared with not using it , respectively.4 - 6 we propose three major contexts of use for which a tbt might have clinical utility , and therefore value , designated as optout , opt - in , and the use of appropriate , alternative , effective therapies ( opt - alt ; table 1 )  . 
each of these terms refers to the clinical decision that might be made based on the results of the tbt compared with the decision made as standard of care ( soc ) without tbt results . 
these categories can be applied to the various use contexts considered for the tbt , including assessment of cancer risk / susceptibility , screening , differential diagnosis , prognosis , prediction , and monitoring.7 similar to therapeutics , the performance and therefore value of a tbt will vary within certain subpopulations of patients , underlying the need to specify the target population when assessing value within a specic use context . 
opt - out tbts have value and the potential to be directly cost saving by reducing the use of unnecessary or ineffective yet toxic and costly therapies , either by indicating that the patient does not need additional therapy ( prognosis ) or that the therapy under consideration is unlikely to work ( prediction ; table 1 )  . perhaps the most well - known example of opt - out tbts with high analytic validity and clinical utility are genomic tests used to determine whether adjuvant chemotherapy should be given to patients with estrogen receptorpositive , human epidermal growth factor receptor 2negative , and least ve node - negative breast cancer . 
there are at commercially available tbts in this category.8 , 9 the 21 - gene recurrence score ( rs ; oncotype dx ; genomic health , redwood city , ca ) is the most well studied and provides an illuminating case study . 
before introduction of the 21 - gene rs , adjuvant chemotherapy was recommended for 50% or more of patients with estrogen receptorpositive , human epidermal growth factor 2negative , node - negative breast cancer.10 the 21 - gene rs , which has high analytic validity , 11 identies a large percentage of this group of patients for whom adjuvant chemotherapy has little or no chance of improving cancer - related outcomes , and its use is now recommended for all women in this category.8 , 12 cost - effectiveness analyses of the 21 - gene rs have varied widely and involve complex and unavoidably subjective modeling that depends on assumptions made about management strategy , impact of treatment , time horizon , inputs.13 accepted patient population , and other model estimates of the impact of the 21 - gene rs assay suggest overall absolute reductions in chemotherapy of 7% to 14% in the roughly 50 , 000 women who are newly diagnosed every year in whom testing would be recommended ( table 2 )  . 
assuming an average total adjuvant chemotherapy cost of $80 , 000 ( including modern drugs and supportive care treatments ) , 14 annual chemotherapy cost savings for women in this category would be between $280 million to $560 million per year , signicantly outpacing the roughly $175 million spent on the test for these same women ( assuming $3 , 500 per test )  . 
in this case , the value of the tbt is generated by turning a minimally effective or is indicated , and unacceptable therapy into one that therefore acceptable , because of an altered risk - benet that justies or renes treatment . 
an opt - in tbt will typically increase costs , but still has value because it may result in improved long - term clinical outcomes . an example of an opt - in tbt is provided by analysis of germline susceptibility genes , such as brca1 or brca2 , or associated genes ( table 2 )  . 
in this case , the presence of a deleterious inherited germline mutation in the brca1 or brca2 ( or related ) gene substantially increases the odds of developing and dying as a result of breast and / or ovarian cancer . 
however , the risk of developing these cancers and the odds of mortality are reduced by as much as 90% and 35% to 75% with prophylactic mastectomy and salpingooophorectomy , respectively.15 , 16 in this case , these otherwise unacceptable interventions become appropriate because of the increased chances of long - term survival as a result of the intervention in a high - risk population ( table 2 )  . 
therefore , although such tests may be relatively expensive , their value in terms of lives saved , decreased long - term medical costs , and increased economic productivity and quality of life often outweigh the immediate costs of the tests and associated downstream medical expenditures . 
this tradeoff between added costs and increased quality of life is often measured through economic metrics , such as incremental costeffectiveness ratios , which are expressed in units of cost ( dollars ) per 1 year of full quality of life , or quality - adjusted life - years ( qalys )  . 
for example , the brca test listed in table 2 , when applied to the target population , saves on average 1 qaly for every $4 , 300 spent ( $4 , 300 / qaly ) .17 opt - alt tbt the opt - alt tbt paradigm is a subcategory of opt - in . 
in this case , the value of the tbt is to help select a strategy from two or more available choices that is most likely to benet the patient , thus enhancing the precision of his or her management . 
opt - alt tbts improve outcomes via the use of appropriate , alternative , effective therapies . an example of an opt - alt tbt is illustrated by somatic mutation testing in metastatic lung adenocarcinoma to drive the use of therapies directed against genomic abnormalities ( table 2 ; opt - alt : initial rx )  . 
these abnormalities occur in various genes , including egfr , kras , alk , ros1 , erbb2 , braf , ret , and ntrk1 , which are found collectively in more than 20% of patients with metastatic nonsmall - cell lung cancer using tbts on the basis of nextthese abnormalities is generation sequencing . 
each of linked to a specic therapy that targets the genomic abnormality ( eg , erlotinib and other tyrosine kinase inhibitors ) , 18 and approximately one quarter of these patients will benet from these agents . 
in contrast , chemotherapy , which has roughly the same likelihood of benet but is associated with substantially higher toxicities , remains an soc for many of the remaining patients.19 although the clinical value in terms of quality and quantity of life is established , it is a difcult and somewhat subjective exercise to determine the true economic value of these tests , which depend heavily on the relative benets of each of the drugs in each of the many settings in which they may be used across different populations . opt - out / monitoring or opt - in / monitoring tbt in an opt - in / monitoring scenario , a patient a variation on the opt - out , opt - in , or opt - alt schema is the monitoring paradigm ( table 1 )  . 
value arises from avoiding the toxicity and cost of continuing an ineffective therapy . clinically free of apparent disease , but the tbt results indicate an impending future cancer - related event which early intervention may be more effective than waiting until the event becomes clinically evident . 
an additional variant of the opt - alt / monitoring paradigm occurs if serial tbts are used as surrogates of more expensive or inconvenient , but strongly indicated , monitoring strategies . 
in this case , the patients cancer - related outcome may not be improved by the tbt per se , but the tbt helps the patient avoid other diagnostic studies , such as radiographic imaging . 
one should note that a given tbt can fall into one or more of these use context categories , depending on the disease to which the tbt is applied and the clinical scenario . as noted , the opt / monitoring paradigm has three possibilities : opt - out / monitoring , opt - in / monitoring , or opt - alt / monitoring . 
for solid malignancies , liquid biopsies include tumor - associated proteins ( eg , carcinoembryonic antigen [ cea ] / colorectal cancer ; ca125 / ovarian cancer ; prostate - specic antigen [ psa ] / prostate cancer , and muc1 , identied by ca15 - 3 or ca27.29 / breast cancer ) , circulating tumor cells , and cell - free tumor dna . opt - out / monitoring and opt - alt / monitoring tbts might be used in many settings , and their economic value may differ in each . 
introducing earlier treatment of such patients may result in higher overall survival rates , as with patients with isolated colorectal metastases detected by an increasing cea level , 22 or may not , as in patients with ovarian and breast cancers monitored with ca125 or ca15 - 3 , respectively.23 , 24 we consider serial cea for patients with a history of colorectal cancer to have high clinical utility , and we would place this tbt for this indication in tier 1 , suggesting that reimbursement should be based on more than just commodity pricing . 
in contrast , monitoring the latter two tbts has been shown in prospective randomized clinical trials to not result in longer overall survival . we would place these markers in tier 3 , or tier x , because their clinical and economic value is not clear ( table 3 )  . 
in contrast , results of a prospective , randomized clinical trial have demonstrated that identication and treatment of hepatic oligometastases in patients with stage ii to iii colorectal cancer results in a small but denite chance of cure22 and would therefore be placed in tier 1 ( table 2 )  . 
however , the development of high - level evidence of tbts in high - risk subsets might expand their indications in the future , thus offering an incentive for biotech companies to invest in generating high - level evidence demonstrating the clinically utility of tbts . in the metastatic setting , an increasing circulating tbt either directly indicates failure of the current therapy or suggests the need for more invasive imaging to determine whether the disease is progressing . 
in this case , such tbts provide both opt - out and opt - alt information because the soc is usually to change from the apparently inactive treatment to a second or later - line treatment ( opt - alt ) or to discontinue treatment altogether ( opt - out )  . 
although few , if any , prospective randomized clinical trials exist to demonstrate the clinical utility of these markers in this use context , in general , the opt - alt paradigm is considered to be sufcient to place these tbts ( at least the circulating proteins ) in tier 2 or 3 , and they are used routinely.25 our model would suggest that reimbursement for these tbts should be commensurate with their value in managing patient care . having dened the tbt use contexts and their relative value possibilities , we propose a semiquantitative , hierarchal , tiered - based approach to help determine a reimbursement structure for tbts ( table 3 )  . 
tiers dene tbts ranging from high analytic validity and clinical utility ( tier 1 ) to less accurate analytic validity or lower evidence of clinical utility ( tiers 2 and 3 ) and tbts without conrmed clinical value ( tier x )  . 
in each case , assessment of a tbt is dependent on its specic use context as an optout , opt - in , opt - alt , or opt / monitoring tbt ( table 1 )  . 
these savings could be redistributed within the health care systeone option would be to simply use the savings , especially those generated by opt - out tbts , to reduce the cost of care . 
we maintain that this approach is unattractive , because it is likely to stie innovation for new tbts , reduce the quality of data regarding a tbts clinical utility , and further enhance the existing vicious cycle.1 rather , we argue that the value of generating high - quality tbts should instigate a redistribution of health care spending directly ( in the case of opt - out tbts ) from therapeutics to diagnostics or indirectly ( in the case of opt - in tbts ) , on the basis of the case that immediate costs should be borne by society to obtain long - term cost effectiveness . 
such redistribution of nancial resources would then stimulate greater investment into diagnostics to support r&d and reward innovation and entrepreneurship . our tiered approach provides a clear and achievable opportunity for companies to develop high - quality tbts with a guarantee for a commensurate return on investment . 
rather , tbt proposes a strategy to redistribute third - party reimbursement from unnecessary or ineffective therapies to support tbts with high clinical utility to provide a baseline assurance of reimbursement and return on investment for entities investing in tbt development . 
importantly , tbts in tiers with poor evidence ( tier 3 ) or those that are purely informative with unclear implications for management ( tier x ) cannot be expected to recoup health care resources , and we argue that such tbts should receive little , if any , third - party reimbursement . although our system does not directly reward a tbt for having slightly better performance than another for a similar indication , it does so indirectly . 
therefore , a static determination of cost effectiveness for a tbt is unrealistic . in the example of the 21 - gene rs , the cost of adjuvant chemotherapy has increased dramatically in breast cancer , in part as a result of routine hematopoietic growth factor for dose - dense treatment.14 another issue is support whether tbts should be entered into clinical practice before high loes are available , with reimbursement on the basis of a coverage - with - evidence - development approach , which has been piloted by the centers for medicare and medicaid and its afliates.27 in this case , rather than insistence on either prospective clinical trials or prospectiveretrospective4 , 5 studies , the third party payer is willing to cover the use of a tbt , with the proviso that the user or manufacturer generates evidence supporting at least clinical validity if not utility for the assay . 
this strategy represents an intriguing but special circumstance outside of our model . a key limitation of our proposed system is that there will be justiable differences in opinions regarding the relative analytic validity , meaningfulness of different clinical end points , magnitude of outcomes , and strategies to generate loes for clinical utility . 
nonetheless , this formulation is a rst conceptual and quantitative step toward what would eventually be a rened , objective , and quantitative method to assign value to emerging tbts using a practical tiered reimbursement scheme , helping to break the vicious cycle of tumor biomarker value . finally , a consideration of the proposed system would not be complete without acknowledging the critical importance of practical barriers to implementation . 
although an indepth discussion of all barriers is beyond the scope of this article , it is worth noting that efforts to implement this proposed system will require input and approval from the involved stakeholders , 1 which include the life sciences industry , private third - party payers , government and regulatory agencies , health care systems , providers and larger medical associations , and patients and patient advocacy groups . 
however , the ultimate success of this system will require large - scale adoption to provide incentives sufcient to power the proposed virtuous cycle of investment in high - quality tbt development . in conclusion , we have proposed an objective , systematic , and semiquantitative approach to guide researchers , funders , test manufacturers , clinicians , patients , and health care systems to invest health care dollars into tbt r&d . 
by providing a tiered categorical solution with clear minimum reimbursement levels , we hope to provide assurance to investors of a solid potential for return on investment via r&d into high - quality clinically useful tbts . 
by increasing entry into the market for high - quality tbts , we argue that market forces will drive real - time selection of the most clinically local useful tbt available for a given clinical context , treatment practices , and population characteristics . 
lyman consulting or advisory role : g1 therapeutics , halozyme , partners healthcare , amgen , pzer , agendia , helsinn therapeutics , celldex ( i ) , janssen ( i ) , genomic health , mylan , samsung bioepis , spectrum pharmaceuticals research funding : amgen richard l . 
schilsky research funding : astrazeneca ( inst ) , bayer ( inst ) , bristol - myers squibb ( inst ) , genentech ( inst ) , eli lilly ( inst ) , merck ( inst ) , pzer ( inst ) , boehringer ingelheim ( inst ) travel , accommodations , expenses : varian daniel f . 
hayes stock and other ownership interests : oncimmune , inbiomotion consulting or advisory role : cepheid , freenome , cellworks , cvs caremark breast cancer expert panel , agendia research funding : astrazeneca ( inst ) , puma biotechnology ( inst ) , pzer ( inst ) , eli lilly ( inst ) , merrimack ( inst ) , menarini silicon biosystems ( inst ) patents , royalties , other intellectual property : royalties from licensed technology ; diagnosis and treatment of breast cancer . 
hayes is designated as inventor / co - inventor ; title : a method for predicting progression - free and overall survival at each follow - up time point during therapy of patients with metastatic breast cancer using circulating tumor cells . 
cancer - tests / #530d572f5955 teutsch sm , bradley la , palomaki ge , et al : the evaluation of genomic applications in practice and prevention ( egapp ) initiative : methods of the egapp working group . 
harris ln , ismaila n , mcshane lm , et al : use of biomarkers to guide decisions on adjuvant systemic therapy for women with early - stage invasive breast cancer : american society of clinical oncology clinical practice guideline . 
j clin oncol 34 : 1134 - 1150 , 2016 krop i , ismaila n , andre f , et al : use of biomarkers to guide decisions on adjuvant systemic therapy for women with early - stage invasive breast cancer : american society of clinical oncology clinical practice guideline focused update . 
cronin m , sangli c , liu ml , et al : analytical validation of the oncotype dx genomic diagnostic test for recurrence prognosis and therapeutic response prediction in node - negative , estrogen receptor - positive breast cancer . 
wang sy , dang w , richman i , et al : cost - effectiveness analyses of the 21 - gene assay in breast cancer : systematic review and critical appraisal . 
balmaa j , sanz j , bonll x , et al : genetic counseling program in familial breast cancer : analysis of its effectiveness , cost and cost - effectiveness ratio . 
lindeman ni , cagle pt , beasley mb , et al : molecular testing guideline for selection of lung cancer patients for egfr and alk tyrosine kinase inhibitors : guideline from the college of american pathologists , international association for the study of lung cancer , and association for molecular pathology . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
rustin gj , van der burg me : a randomized trial in ovarian cancer ( oc ) of early treatment of relapse based on ca125 level alone versus delayed treatment based on conventional clinical indicators ( mrc ov05 / eortc 55955 trials )  . 
van poznak c , somereld mr , bast rc , et al : use of biomarkers to guide decisions on systemic therapy for women with metastatic breast cancer : american society of clinical oncology clinical practice guideline . 
reed sd , dinan ma , schulman ka , et al : cost - effectiveness of the 21 - gene recurrence score assay in the context of multifactorial decision making to guide chemotherapy for early - stage breast cancer . 
eiermann w , rezai m , k ummel s , et al : the 21 - gene recurrence score assay impacts adjuvant therapy recommendations for er - positive , node - negative and node - positive early breast cancer resulting in a risk - adapted change in chemotherapy use . 
pilon d , queener m , lefebvre p , et al : cost per median overall survival month associated with abiraterone acetate and enzalutamide for treatment of patients with metastatic castration - resistant prostate cancer . 
schremser k , rogowski wh , adler - reichel s , et al : cost - effectiveness of an individualized rst - line treatment strategy offering erlotinib based on egfr mutation testing in advanced lung adenocarcinoma patients in germany . 
 o survival outcomes by tp53 mutation status in metastatic breast cancer purpose to determine the significant genomic alterations in patients with metastatic breast cancer ( mbc ) and survival outcomes in common genotypes . patients and methods high - depth next - generation sequencing was performed for 202 genes in tumor and normal dna from 257 patients with mbc , including 165 with estrogen receptor / progesterone receptorpositive and human epidermal growth factor receptor 2 ( her2 [ hormone receptor positive ( hr + ) ] ) positive , 32 with her2 - positive , and 60 with triple - negative ( estrogen receptor / progesterone receptornegative and her2 - negative ) disease . 
kaplan - meier survival analysis was performed in the discovery set , in patients with breast cancer analyzed in the cancer genome atlas , and in a separate cohort of 98 patients with mbc who underwent clinical genomic testing . results significantly mutated genes ( smgs ) varied by histology and tumor subtype , but tp53 was an smg in all three subtypes . 
emerging data have shown that the targeting of some of these alterations , such as akt and her2 mutations , may have antitumor efficacy.1 , 2 most proof - of - principle genomically selected trials are conducted in the metastatic setting , whereas many molecular characterization efforts , such as the cancer genome atlas ( tcga ) , are performed in operable breast cancer.3 to design and interpret genotype selected trials effectively , the determination of the genomic profile of patients with metastatic breast cancer ( mbc ) , the frequency of genomic alterations and co - alterations , and the effect of common alterations on prognosis is critical . we determined the genomic profile of patients with mbc in a prospective study and report the significantly altered genes in various breast cancer subtypes . 
 an additional cohort of 98 patients with hr + mbc who underwent clinical genomic testing funda mericbernstam xiaofeng zheng maryam shariati senthil damodaran chetna wathoo lauren brusco mehmet esat demirhan coya tapia agda karina eterovic reva k . 
 were identified as a validation cohort ; patients had undergone testing with foundationone ( foundation medicine , cambridge , ma ) , ion ampliseq comprehensive cancer panel ( thermo fisher scientific , waltham , ma ) , or oncomine comprehensive assay ( thermo fisher scientific )  . 
ngs of 202 genes ( t200 platform ; data supplement ) was performed on tumor and normal dna samples as previously described.4 assays were performed while blinded to the clinical outcomes . 
 reporting was done consistent with reporting recommendations for tumor marker prognostic studies guidelines.5 molecular inversion probe ( mip ) arrays were performed as previously described.6 , 7 esr1 mutation status was tested using the qx200 droplet digital pcr system ( biorad laboratories , hercules , ca ) with primers to assess the following four esr1 mutations : y537c ( 1980a > g ) , y537n ( 1979t > a ) , y537s ( 1980a > c ) , and d538g ( 1983a > g ; data supplement )  . 
quantitative analysis was performed using quantasoft software ( bio - rad laboratories )  . bioinformatics analysis comprehensive methods for bioinformatics analysis has been previously published.4 for copy number calls , high amplification and high deletion was defined as an estimated copy number of five and 0.6 on ngs analysis and five and one on mip analysis . 
discrete independence statistic controlling for observations with varying event rates ( discover ) , a statistical test for detecting co - occurrence and mutual exclusivity in cancer genomics data , was used.8 unlike traditional approaches such as fishers exact test , discover is based on a null model that takes into account the overall tumor - specific alteration rates when deciding whether alterations co - occur more or less often than expected by chance . 
multiple testing was adjusted using false discovery rate ( fdr )  . recurrence - free survival ( rfs ) was calculated from the date of initial breast cancer diagnosis to the date of first local or distant relapse , death , or last follow - up . 
overall survival ( os ) was calculated from the date of mbc diagnosis . results somatic alterations two hundred sixty - eight samples from 257 patients were sequenced ( table 1 )  . 
distribution by tumor subtype was as follows : 165 patients ( 64.2% ) with estrogen receptor / progesterone receptorpositive ( er / pr + ) and human epidermal growth factor 2negative ( her2 ) hr + breast cancer ; 60 with triple - negative breast cancer ( tnbc ) ; and 32 with her2 + breast cancer ( 24 with er / pr + and her2 + and eight with er / pr and her2 + )  . 
forty - eight patients ( 18.7% ) had stage iv disease at presentation . a heat map of the top 50 mutated genes and 50 copy numberaltered ( cna ) genes are shown in the data supplement . 
with rfs 12 months postneoadjuvant chemotherapy postneoadjuvant endocrine therapy locoregional recurrence distant metastases soft tissue bone liver lung other patients with both primary and recurrence / metastasis ( n = 11 ) primary and recurrence primary and metastasis no . 
in her2 hr + breast cancer , a significant gain was seen of fgfr1 , gnas , smarca4 , cpamd8 , crebbp , fgfr3 , hnf1a , lrp1 , and nfkb2 and a loss of csmd1 . 
of the 36 amplifications detected by ngs , 22 were confirmed by mip arrays ( data supplement ) , including all four patients with fgfr1 amplification , all five with gnas amplification , three of four with smarca4 amplification , and all four with notch2 amplifications . 
of 11 deletions detected by ngs , nine were confirmed by mip arrays , including all three patients with nf1 and all three with pten deletions . alterations in actionable genes overall , 244 patients ( 94.9% ) had an alteration in at least one potentially actionable gene.9 of note , mutations differ in their functional consequences ; thus , not all mutations may be actionable.9 , 10 furthermore , a genomic profile may not be considered actionable because of co alterations or other patient variables . 
actionable alterations included well - recognized alterations , such as pik3ca mutations ( 24% ) and fgfr amplifications ( 10% ) , as well as less - frequent but clinically compelling alterations , such as akt1 mutations ( 3% ) and her2 mutations ( 3% )  . 
in addition , there were potentially actionable rarer alterations , such as an inactivating mutation in ptch1 , an activating mutation in idh1 , and high - level amplification of egfr . 
of note , 117 patients ( 72% ) with alterations in an actionable gene had a co - alteration in another potentially actionable gene . we previously reported that most brca1 / 2 alterations in breast cancer are germline.11 , 12 however , we observed potentially deleterious somatic alterations in dna damage repair genes brca1 / 2 , palb2 , atm , and rad51 . 
 no differences were found among these cohorts . genomic alterations in 191 primary versus 77 recurrent / metastatic tumors were compared ( data supplement ) ; no significant differences were found by fishers exact test . 
of the hr + primary tumors , 78 were chemotherapy - nave , 39 were postneoadjuvant we compared the alterations seen in this study with that in the tcga breast cohort ( data supplement )  . 
the mbc cohort was enriched for some alterations , such as tp53 mutations , compared with the tcga series . by ngs , 251 of 257 patients had esr1 sequencing ; however , only 151 patients had adequate coverage of esr1 . 
 two other patients with hr + breast cancer whose primary tumors did not show an esr1 mutation subsequently had ngs of a new distant metastatic lesion not included in this analysis , and this testing uncovered esr1 mutations . because a 4% esr1 mutation rate in mbc is lower than what we and others have reported , 13 , 14 we also used droplet digital polymerase chain reaction for four hot spot mutations ( esr1 y537s , y537c , y537n , and d538g ) in 49 patients with dna from metastatic tumor samples.13 , 14 thirty - eight patients had endocrine therapy before the biopsy of the metastasis ( 31 in the adjuvant setting , seven for recurrent disease )  . 
two of these patients also had t200 sequencing , and one was found to have the same esr1 mutation ( d538g ) , whereas the other , although the same dna was used , did not have the mutation detected , which suggests that droplet digital polymerase chain reaction may be more sensitive for detection . 
one patient had four lines of endocrine therapy in the metastatic setting , whereas the other had adjuvant tamoxifen . genomic profile and prognosis in hr + breast cancer a heat map and bar plot of the 50 most commonly altered genes in hr + breast cancer are shown in fig 2 . 
we tested for the co - occurrence between the top 50 altered genes in hr + breast cancer using the discover algoriththe p and q values for all the gene pairs are listed in the data supplement . 
with an fdr of 0.1 , we found co - alterations in fgfr3 and cripak , which are colocalized on chromosome 4 ; co - alterations in cpamd8 , smarca4 , and notch3 , which are colocalized on chromosome 19 ; and co alterations in crebbp and tsc2 , which are colocalized on chromosome 16 . 
with an fdr of 0.1 , gata3 alterations were mutually exclusive with tp53 alterations . in precision oncology trials , treatment often is given to patients with selected alterations ; thus , we assessed the effect of common genomic alterations on pfs in patients with hr + breast cancer . 
patients with missense tp53 mutations had a longer rfs than those with other types of tp53 mutations , but this difference was not significant ( p = .055 ; fig 3b )  . tp53 mutations were associated with a shorter os in patients with hr + breast cancer ( p = .003 ; fig 3c )  . 
tp53 mutation type ( missense v other ) was not associated with os or pfs on first - line endocrine therapy . when patients with pik3ca mutation / amplification , akt1 mutation / amplification , pten mutation / deletion , fgfr1 / 3 amplifications , gata3 mutations , or map3k1 / map2k4 mutation / deletion were compared with patients who lack these alterations , no significant difference was found in pfs in the first - line metastatic setting on any therapy ( data supplement ) as well as in patients treated with endocrine therapy ( data supplement )  . 
 alteration type del / mut amp / mut pik3ca tp53 gata3 notch1 fgfr1 cdh1 notch3 gnas csmd1 lrp1 cripak map3k1 mll3 fgfr3 ryr2 tsc2 crebbp lrp2 hnf1a akt1 hydin smarca4 spen hmcn1 mll2 cpamd8 znf536 csmd3 arid1a nfkb2 pten ercc5 igf1r daxx ush2a men1 bap1 pkhd1 notch2 il6r erbb2 dnmt3a top1 tgfbr2 fgfr4 pkhd1l1 spta1 tbc1d4 fig 2 . 
the samples are presented in order , with the most common alterations on the leamp , amplification ; del , deletion ; mut , mutation . discussion tp53 was an smg in all breast cancer subtypes , but mutations were more frequent in hr tumors . 
tp53 mutations were seen in 41% of patients with mbc in our sample compared with 30% in the tcga , which represents patients with earlier - stage disease ( fig 1 ) and higher rates of tp53 mutations in hr + breast cancer ( 29% v 18% )  . 
 of note , when ellis et al20 compared aromatase inhibitorsensitive versus aromatase inhibitor resistant tumors in the neoadjuvant setting ( clinicaltrials.gov identifier : nct00265759 ) , the tp53 signaling was enriched in resistant tumors ( 38% of the aromatase inhibitorresistant and 17% in the sensitive group )  . 
 however , emerging therapeutics have been targeting mutant p53.21 , 22 an urgent need exists for novel therapies for tp53 mutant tumors . in the current study , patients had a variety of genomic alterations . 
the frequency of alterations in this pathway may differ on the basis of patient population ( tumor subtype and histology and other variables ) as well as the assay and bioinformatics pipeline . 
in most breast cancer series , this potentially actionable pathway is the most frequently altered ; thus , these alterations are being actively pursued in trials with pi3k / akt / mtor inhibitors.2 , 23 , 24 cdh1 mutations , as expected , were almost exclusively found in invasive lobular carcinoma . 
mutations in map3k1 and map2k4 already have been reported in hr + breast cancer.20 ellis et al20 reported a frequency of 15.5% for map3k1 and map2k4 in er + breast cancer . 
the prognostic and predictive value of gata3 needs to be evaluated further . although our ngs platform primarily analyzes commonly mutated genes in cancer , it can provide copy number information.4 indeed , we identified common cnas , such as gain in fgfr1 and her2 . 
we recently reported that when ngs demonstrates high - level amplification , we are able to validate cnas on an orthogonal platform , such as fluorescent in situ hybridization.25 ngs - based detection of cnas is limited to high - level losses or gains ; thus , we may have underestimated the frequency of copy number changes . 
however , several of these cnas , such as notch alterations and nf1 loss , have therapeutic implications and need additional study . we had too few matched primary and recurrence samples to systematically study genomic evolution in this series . 
in another study , we reported that in 33 matched primary and recurrent tumors , 97 ( 87% ) of 112 somatic mutations were concordant.26 more recently , lefebvre et al27 reported the genomic profiling results of patients who underwent a biopsy of mbc in the context of the safir - 01 , safir - 02 , shiva ( tumor molecular profiling versus conventional therapy in patients with refractory cancer ) , or moscato ( molecular screening for cancer treatment optimization ) prospective trials . 
however , in lefebvre et al , eight genes ( esr1 , fsip2 , fras1 , osbpl3 , edc4 , palb2 , igfn1 , and agrn ) were more frequently mutated in mbc than in early breast cancer profiles in tcga , which suggests that systematic assessment of metastatic tissue in mbc may lead to identification of additional genomic alterations . the current study had some additional limitations . 
we may not have captured molecular profiles of patients who rapidly progressed while on therapy and succumbed to their disease , or alternately , those who responded well were not perceived as needing molecular characterization . 
our panel also did not include mdm2 and mdm4 , two genes that could be amplified to negatively regulate the tp53 axis in patients with wild - type tp53 . in conclusion , genomic profiling has identified multiple potentially actionable alterations . 
mills shaw provision of study materials or patients : funda mericbernstam , maryam shariati , chetna wathoo , lauren brusco , mehmet esat demirhan , filip janku , kenna r . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . funda meric - bernstam honoraria : dialecta , sumitomo group consulting or advisory role : genentech , inflection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , grail research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer ag , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pfizer , effector therapeutics xiaofeng zheng no relationship to disclose maryam shariati no relationship to disclose senthil damodaran no relationship to disclose chetna wathoo no relationship to disclose lauren brusco employment : celgene mehmet esat demirhan no relationship to disclose coya tapia research funding : armo biosciences travel , accommodations , expenses : incyte agda karina eterovic no relationship to disclose reva k . 
basho employment : davita ( i ) , castlewood treatment center ( i ) honoraria : insight strategy advisors , navigant consulting consulting or advisory role : heron therapeutics , puma biotechnology naoto t . 
ueno no relationship to disclose filip janku stock and other ownership interests : trovagene consulting or advisory role : deciphera , trovagene , novartis , sequenom , foundation medicine , guardant health , immunome research funding : novartis , biomed valley discoveries , roche , agios pharmaceutical , astellas pharma , deciphera , symphogen , plexxikon , piqur therapeutics , fujifilm other relationship : bio - rad laboratories aysegul sahin no relationship to disclose jordi rodon consulting or advisory role : novartis , eli lilly , imclone systems , servier , orion , peptomyc research funding : novartis , bayer ag russell broaddus no relationship to disclose tae - beom kim no relationship to disclose john mendelsohn leadership : merrimack stock and other ownership interests : merrimack patents , royalties , other intellectual property : royalty payments from university of california , san diego travel , accommodations , expenses : merck kenna r . 
mills shaw no relationship to disclose debu tripathy consulting or advisory role : novartis , nektar , pfizer , puma biotechnology research funding : genentech ( inst ) , roche ( inst ) , novartis ( inst ) travel , accommodations , expenses : novartis gordon b . 
 patents , royalties , other intellectual property : licensed technology hrd assay to myriad genetics acknowledgment travel , accommodations , expenses : astrazeneca , symphogen , ionis pharmaceuticals , medimmune , eli lilly , novartis , immunome , pfizer we thank kristin hargraves and the khalifa institute for personalized cancer therapy clinical research team for assistance with data curation and kurt evans for technical assistance . ken chen no relationship to disclose affiliations all authors : the university of texas md anderson cancer center , houston , tx . support supported by the sheikh khalifa al nahyan ben zayed institute for personalized cancer therapy , an astrazeneca foundation grant , national cancer institute grant no . 
connally breast cancer research endowment , cancer prevention research institute of texas precision oncology decision support core rp150535 , the bosarge foundation , and md anderson cancer center support grant no . 
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although targeted therapies , including vandetanib and cabozantinib , are used to treat mtc , resistance ( both intrinsic and acquired ) to these therapeutic approaches warrants a need to better understand the broad - spectrum anomalies that govern this phenomenon , especially in patients with aggressive disease . 
using whole - exome sequencing ( wes ) and shallow whole - genome sequencing ( swgs ) of the primary tumor , adjacent normal bone marrow tissues , and blood , we identified three germline single nucleotide polymorphisms ( snps ) within the ret proto - oncogene that remained undetected using routine hospital genetic testing procedures . 
supported by findings from both wes and swgs , we report on the occurrence of a chromothripsis - like pattern in thyroid cancer , which involved shattering of chromosome 4 leading to complete abrogation of normal chromosomal function , along with dramatic widespread copy - number aberrations across both primary tumor and bone marrow samples . a 36 - year - old man with a body mass index ( bmi ) of 45 presented with a 4 - week history of chest pain , dyspnea , and 22 kg of unintentional weight loss ( overview of the patients clinical course is presented in the data supplement )  . 
the working diagnosis was carcinoma of unknown primary . a bone marrow biopsy was performed , and immunohistochemical ( ihc ) staining revealed round and polygonal malignant cells arranged in nests and cord - like patterns with round to oval nuclei containing coarse granular chromatin patterns adjacent to areas of extensive tumor necrosis ( fig 1a1 )  . focal staining was positive for calcitonin ( fig 1a2 ) , chromogranin ( data supplement ) , thyroid transcription factor 1 ( data supplement ) , and synaptophysin ( data supplement ) , but it was negative for cd45 ( data supplement )  . 
a diagnosis of mtc was established . these results led to a thyroid ultrasound , which showed a 4 - cm hypoechoic nodule at the lower pole of the left lobe and a 1.4 - cm hypervascular echogenic focus inferomedially to it ( fig 1b )  . 
ihc of the primary tumor revealed pleomorphic polygonal and ascopubs.org / journal / po jco precision oncology sudipto das deirdre kelly bruce moran kathleen han niall mulligan ciara barrett patrick g . 
radiologic detection of primary tumor and immunohistochemical analysis of primary thyroid and bone marrow sample . ( a ) bone marrow biopsy sample stained with ( 1 ) hematoxylin and eosin staining showed infiltration of the marrow space by a proliferation of pleomorphic round to oval cells with scant eosinophilic cytoplasm and inconspicuous nucleoli . 
 ( 2 ) positive staining of the bone marrow biopsy observed for calciton ( b ) thyroid ultrasound shows a 1.4 - cm hyperechoic nodule at the lower pole of the left lobe of thyroid ( as indicated by the red arrow ) , suggestive of a primary thyroid malignancy . 
 ( d ) primary tumor sample stained with ( 1 ) hematoxylin and eosin shows that the primary tumor consisted primarily of pleomorphic polygonal and spindle cells arranged in nests separated by fibrous strand . 
serum calcitonin was 5 , 000 ng / l ( normal range , , 10 ng / l ) , and carcinoembryonic antigen was 200 mg / l ( normal range , , 5 mg / l )  . routine germline ret mutation testing in exons 10 , 11 , 13 , 14 , and 16 was negative . 
the patient died on day 31 from multiorgan failure . postmortem examination showed metastatic mtc , with complete replacement of the left lobe of the thyroid involving para - esophageal tracheal lymph nodes and the pleural surface of both lungs extending into the parenchyma . 
after receiving written informed consent from the patients family for research activities to be carried out postmortem , dna extracted from the primary tumor , adjacent normal bone marrow tissue , and blood was used to carry out wes and swgs ( data supplement )  . results chromothripsis - like pattern in genomic data . we revealed a dramatic landscape , concordant between wes and swgs ( fig 2a ) , of wideranging copy - number aberrations ( cnas ) across the primary tumor , two distinct regions of bone marrow , which showed clear tumor cell infiltration ( bm - mets1 , bm - mets2 ) , and adjacent normal tissue . 
by using the blood sample as a baseline , losses ranging from regions of several megabases to entire chromosomes were evident across all tumor samples ( fig 2a ; data supplement ) with a single gain occurring on the q arm of chromosome 1 . 
genome - wide copy - number aberrations and identification of chromothripsis - like pattern across adjacent normal tissue , blood , primary tumor , and bone marrow samples showing somatic mutations from whole - exome sequencing ( wes )  . 
 ( a ) absolute copy - number aberrations ( y - axis : 1 , loss ; 3 , gain ) across chromosomes 1 to 21 ( x - axis , denoted by blue lines , centromere denoted by dashed pink line ) compared by using data from wes and shallow wholegenome sequencing across all sample types . 
 ( b ) the copy - number aberration profile for chromosome 4 across the all samples demonstrating the chromothripsis - like pattern event generated for a 30 - kb bin using the wes data . 
ctlp is a catastrophic event involving tens to hundreds of chromosomal rearrangements up to the whole - chromosome level , which can contribute to development of a highly unstable and aggressive disease.1 - 7 the ctlp observed in this patient led to generation of approximately 30 to 40 segments with a typical oscillation of cna between two states ( loss and normal copy number ) .7 although we did carry out genomic analysis of the other metastatic lesions , including the para - esophageal , para - tracheal , and lung metastases , they were not included in the detailed genomic assessment described in this study because of unacceptable sequencing data quality . germline mutations in ret and somatic mutations in disease - associated genes . 
germline mutation analysis using wes from blood and adjacent normal tissue did not reveal any ret variants that are currently used diagnostically ( confirming the posthumous germline ret mutation profiling )  . 
however , we identified three annotated snps within ret ( rs1800861 , rs2742241 , and rs2742243 ) that were fixed with a mutant allele frequency of 1 across all samples including blood and normal tissue . we were able to validate these orthogonally across all samples by using sanger sequencing ( data supplement )  . 
the rs1800861 ( l769l , exon 13 leuctt / leuctg ) variant has previously been reported as a predisposing factor for development of aggressive mtc.8 , 9 of the other two mutations , rs2742243 ( c / t variant ) has been associated with papillary thyroid carcinoma10 and rs2742241 ( g / a variant ) has not been shown to be associated with thyroid cancer . furthermore , our somatic mutational analysis identified 109 somatic mutations , 70% of which occurred in only one of the samples ( fig 2c ; data supplement )  . 
among the nonsynonymous variants of note in disease - associated are missense mutations genes , including gse1 , cldn12 , and trim28 , which have been previously implicated as playing a role in disease processes such as metastasis , migration , and proliferation across various cancer types11 - 15 and may have had a role as potential drivers of disease progression in this patient . 
the differences in mutational patterns between the two bone marrow samples suggest marked genetic heterogeneity between tumor deposits in the same tissue . discussion the patients high bmi made palpation of a neck mass impossible , and the lack of an abnormality on routine imaging in addition to the development of dic and deteriorating respiratory status made this an extremely difficult clinical and diagnostic case . 
remarkably , it was the analysis of the bone marrow that led to the diagnosis of mtc , which further exemplified the severity of the disease in this patient showing complete infiltration of the bone marrow , potentially contributing to a total bone marrow collapse and resulting in development of dic.16 , 17 posthumously , routine clinical germline ret mutation testing did not identify any mutations within this gene . we sought to determine why this young man developed such an aggressive mtc and if it could be explained by the interplay of genomic events . our results support the hypothesis of a catastrophic event such as the evident ctlp , along with widespread copy - number alterations that may be regarded as contributing factors toward the observed phenotype.4 , 5 , 18 although ctlp has been detected in 2% to 3% of all cancers , 1 , 3 , 7 , 19 - 21 to the best of our knowledge , this is the first report to demonstrate ctlp in any form of thyroid cancer . in addition to de novo events that have an impact on cancer phenotype , known genetic alterations can often predispose patients to aggressive disease development . 
variants in the ret protooncogene are commonly associated with mtc and are used as a primary diagnostic test to identify familial and sporadic cases.22 - 25 these tests encompass well - established hot spots within ret and have largely been proven effective in detecting patients with conventional mtc . 
however , unusual patients such as this one require detailed analysis of such genes with the intent of identifying rare mutations that might either explain the atypical phenotype or allow it to be molecularly diagnosed . 
the germline ret l769l variant , previously associated with increased risk of aggressive mtc , 8 , 10 , 22 as well as the other two mutations discovered here , which have not previously been reported in mtc , could have an additive effect on increased risk of development of an aggressive phenotype . 
 ret snps were shown to have increased risk for lymph node and distant metastases at diagnosis ( odds ratio , 5.84 ) and also for developing metastases earlier.8 importantly , our results exemplify how the inclusion of more variants in clinical assays may be of use , especially in diagnostically challenging patients . although identification of mutations in individual disease - associated loci , as observed through the somatic mutation analysis , allows us to generate an appropriate hypothesis surrounding the events that could have led to the development of metastasis , the genetic heterogeneity observed across all resection samples of this patient underpin why , in the clinical setting , targeting specific mutational events therapeutically is rarely effective . 
however , it is also important to note that the study reported here describes a single patient with a rare and atypical mtc . multifactorial genomic events , including germline and somatic mutations in functionally important genes together with widespread cna ( including ctlp ) supports the need for pragmatic treatment approaches using combinations of targeted agents and possibly even immunotherapeutic approaches.26 - 28 within the context of this study and in patients who have disease of a similar nature , it is tempting to speculate that the presence of ctlp would likely lead to generation of multiple neoantigens , suggesting a potential benefit of immunotherapy.26 however , it is noteworthy that such immunotherapeutic strategies to date have not been used for patients with mtc . 
although mutational load may be inferred from routine panel - based genetic testing when only a few hot spot mutations are screened , such as in mtc , it is unlikely that candidates for immunotherapy will be identified , suggesting that a deeper examination of the genome may provide better diagnostic and therapeutic information . in conclusion , our results provide a critical insight into potential drivers of an aggressive phenotype of mtc and , in parallel , present a vital opportunity to identify effective therapeutic strategies based on the evident abnormalities in a given patient . 
kelly collection and assembly of data : sudipto das , deirdre kelly , bruce moran , kathleen han , niall mulligan , ciara barrett , peter mcmahon , hendrik f . 
relationships are self - held unless noted . deirdre kelly no relationship to disclose bruce moran no relationship to disclose kathleen han no relationship to disclose niall mulligan no relationship to disclose ciara barrett no relationship to disclose patrick g . 
van essen no relationship to disclose kate connor no relationship to disclose diether lambrechts no relationship to disclose bauke ylstra no relationship to disclose consulting or advisory role : carrick therapeutics research funding : carrick therapeutics travel , accommodations , expenses : oncomark darran p . 
gallagher employment : oncomark leadership : oncomark stock and other ownership interests : oncomark acknowledgment we thank lisa dwane , brian mooney , and camille hurley for their technical assistance on the study and the family of the patient for consenting to the study . affiliations sudipto das , deirdre kelly , bruce moran , kathleen han , niall mulligan , ciara barrett , peter mcmahon , john mccaffrey , kate connor , william m . 
oconnor , royal college of surgeons in ireland ; deirdre kelly , kathleen han , niall mulligan , ciara barrett , peter mcmahon , john mccaffrey , and catherine m . 
van essen and bauke ylstra , vrije universiteit medical center , amsterdam , the netherlands ; and diether lambrechts , vesailus research center , vlaams instituut voor biotechnologie , katholieke universiteit , leuven , belgium . supported by funding from the mater foundation , by postdoctoral fellowship crf13das from the irish cancer society ( s.d. ) , by grant no . 
cai h , kumar n , bagheri hc , et al : chromothripsis - like patterns are recurring but heterogeneously distributed features in a survey of 22 , 347 cancer genome screens . 
sromek m , czetwerty nska m , skasko e , et al : the frequency of selected polymorphic variants of the ret gene in patients with medullary thyroid carcinoma and in the general population of central poland . 
liao s , song w , liu y , et al : familial multinodular goiter syndrome with papillary thyroid carcinomas : mutational analysis of the associated genes in 5 cases from 1 chinese family . 
wei c , cheng j , zhou b , et al : tripartite motif containing 28 ( trim28 ) promotes breast cancer metastasis by stabilizing twist1 protesci rep 6 : 29822 , 2016 15 . 
yang y , cheon s , jung mk , et al : interleukin - 18 enhances breast cancer cell migration via down - regulation of claudin - 12 and induction of the p38 mapk pathway . 
forment jv , kaidi a , jackson sp : chromothripsis and cancer : causes and consequences of chromosome shattering . j gen intern med 21 : c6 - c8 , 2006 study . 
ye l , santarpia l , cote gj , et al : high resolution array - comparative genomic hybridization profiling reveals deoxyribonucleic acid copy number alterations associated with medullary thyroid carcinoma . 
 o application of circulating cell - free tumor dna proles for therapeutic monitoring and outcome prediction in genetically heterogeneous metastatic melanoma ren ata v araljai , msc1 ; kilian wistuba - hamprecht , phd2 ; teola seremet , md phd3 ; joey mark s . 
becker , md phd1 ; julia newton - bishop , md4 ; andreas stang , md mph1 ; bart neyns , md phd3 ; benjamin weide , md2 ; dirk schadendorf , md1 ; and alexander roesch , md1 purpose circulating cell - free tumor dna ( ctdna ) reects the heterogeneous spectrum of tumor - specic mutations , especially in systemic disease . 
2019 by american society of clinical oncology introduction circulating cell - free tumor dna ( ctdna ) has emerged as a potential noninvasive blood biomarker for monitoring tumor load and detecting clinically actionable driver and resistance mutations in patients with melanoma who are receiving therapy.115 most studies published on ctdna in melanoma have been , in essence , proof - of - principle reports investigating technical feasibility or focusing on ctdna courses of individual patients ( mostly brafv600e - positive patients ) based on retrospective sample and data collections . 
however , this does not account for the divergence of mutational states in blood versus tissue , because of intraand intertumor heterogeneity or the different detection sensitivities of bloodversus tissue - based assays . 
 v araljai et al melanoma monitored for the most frequently occurring mutations in braf , nras , and the promoter region of the tert geneestimated to cover 80% of patients.1 we established ctdna thresholds for disease monitoring and examined the relationship between ctdna responses to therapies , including mitogen - activated protein kinase ( mapk ) and immune checkpoint inhibition , and correlated the dynamic changes of ctdna with clinical benet . 
plasma samples were collected as part of standard care or within clinical trials . patients were treated with mapk signaling - targeted drugs ( n = 58 ) , immune checkpoint inhibitors ( n = 33 ) , or with signaling targeted therapy in combination with chemotherapy ( n = 5 ; data supplement )  . 
patients were eligible for plasma monitoring on the basis of histologically conrmed stage iii or iv melanoma and positive detection status for brafv600e , nrasq61 , tertc228t , or tertc250t mutations in a previous tumor biopsy specimen . 
patients were included in ctdna monitoring when they had available baseline and a minimum of three consecutive plasma samples during systemic therapy collected at approximately 4to 6 - week follow - up intervals . 
overview of ( a ) the training cohort ( n = 96 patients with stage iii and iv disease ) and ( b ) the validation cohort ( n = 35 patients with stage iii and iv disease )  . 
correlation of baseline circulating cell - free tumor dna ( ctdna ) levels with metastatic stage and routine serum markers in the training cohort . correlation of baseline brafv600e ctdna levels with increasing metastatic tumor load in ( a ) lymph nodes ( n1 , n = 3 ; n2 , n = 3 ; and n3 , n = 14 ) and ( b ) organs ( m1a , n = 5 ; m1b , n = 5 ; m1c , n = 41 )  . 
 v araljai et al results tomography ( ct ) , magnetic resonance imaging ( mri ) , or ultrasound imaging ( us ) was carried out at baseline and at every 6 to 12 weeks ( 6 2 weeks of plasma sampling time points )  . 
technical assay details and statistical data processing are described in the data supplement . patient validation cohort in total , 104 plasma samples from 35 patients with advanced stage iii or iv disease were prospectively collected either within pharmaceutical clinical trials , early access programs , or biobanking protocols at the department of dermatology of the t ubingen university medical center and the department of medical oncology of the universitair ziekenhuis in brussels ( fig 1b ; data supplement )  . 
informed consent procedures were followed ( approval nos . 316 / 2018bo2 and bun 143201421920 , respectively )  . patients from t ubingen were treated with pembrolizumab ( n = 17 ) or nivolumab plus ipilimumab ( n = 4 ) at the department of dermatology of the t ubingen university medical center . 
the eligibility criteria were the same as for the training cohort . patients with available baseline and a minimum of two consecutive plasma samples during systemic therapy were included in ctdna monitoring . 
radiologic tumor response evaluation of the validation cohort was performed according to immune - related response criteria ( brussels ) or response evaluation criteria in solid tumors ( recist ) 1.1 ( t ubingen )  . ctdna level correlated with melanoma tumor burden and was a risk factor for disease progression at baseline previous reports suggested a correlation between ctdna levels and tumor burden in patients with melanoma.2 - 7 for this study , candidate mutations for ctdna monitoring were selected on the basis of the most frequently occurring genomic changes in melanoma ( estimated to cover 80% of patients ; data supplement )  . 
correlation of mutant tertprom ctdna levels with metastatic progression from locoregional ( stage iiib , n = 2 ; or iiic , n = 6 ) to systemic disease ( stage iv ; n = 14 ) in patients with tertprom - mutated melanomas . 
 ( e ) correlation of baseline serum lactate dehydrogenase ( ldh ) and s100 levels with metastatic progression in brafv600e - positive patients ( gray line , upper limit of normal )  . 
 ( f - k ) correlation of serum ldh and s100 levels with brafv600e ( n = 274 and n = 216 , respectively ) , nrasq61 ( n = 97 and n = 67 , respectively ) , and mutant tertprom ( n = 152 and n = 124 , respectively ) ctdna levels in the training cohort . 
changes in the brafv600e circulating cell - free tumor dna ( ctdna ) levels correlate with therapy response ( pfs )  . and progression - free survival changes in mean brafv600e ctdna levels after therapy initiation relative to baseline ( bl ) in patients who received ( a ) immune checkpoint inhibition therapy ( n = 18 patients ) and ( b ) signaling targeted therapy ( n = 33 )  . 
 ( * ) p , .01 , ( ) p , .001 , and ( ) p , .001 from unpaired t test . the data represent mean 6 sem . kaplan - meier plots are for pfs of the same patients with melanoma assessed by routine radiologic scans . 
 ( c ) immune checkpoint inhibition ( patients with ctdna decrease [ n = 6 ] v increase [ n = 12 ] ) and ( d ) signaling targeted therapy ( patients with ctdna decrease [ n = 12 ] v increase [ n = 21 ] )  . 
 ( e , f ) scatter dot plots of brafv600e ctdna levels of responders versus nonresponders grouped according to ( e ) radiologic response 10 weeks after receiving any therapy or ( f ) radiologic pfs at 6 months of therapy ( mann - whitney u test )  . 
furthermore , the roc analysis allowed determination of ctdna thresholds that we could use subsequently to evaluate the predictive impact of ctdnas during therapy ( data supplement )  . to assess ctdna levels under targeted and immune inhibition , 540 plasma samples from 76 checkpoint patients were analyzed by ddpcr and compared with radiologic staging . 
targeted therapies seemed to decrease ctdna levels faster than immune checkpoint inhibitors ( mean decrease of 31% v 15% at week 4 ; p , .001 ; combined analysis of data from figs 3a and 3b , and figs 4a , 4b , 4c , and 4d , differences remained signicant : unpaired t test p , .001 for all time points )  . 
changes in mean nrasq61 and tertprom ctdna levels after therapy initiation relative to baseline ( bl ) in patients who received ( a , c ) immune checkpoint inhibition therapy , ( n = 10 and n = 12 , respectively ) and ( b , d ) signaling targeted therapy , ( n = 7 and n = 10 , respectively )  . 
scatter dot plots of nrasq61 and ( f ) tertprom ctdna levels of patients assessed at week 10 after receiving any therapy , grouped according to radiologic pfs at 6 months ( mann - whitney u test )  . points represent individual patients ; median with interquartile range is indicated for each plot . 
accordingly , the median was 494.5 copies / ml in patients with a pfs shorter than 6 months ( ie , signicantly higher than in patients with a pfs longer than 6 months [ mann - whitney u test p , .001 ] ; fig 3f )  . 
 ( a ) changes in mean ctdna levels after therapy initiation relative to baseline ( bl ) from patients who received immune checkpoint inhibition therapy ( n = 35 patients )  . 
 ( b ) kaplan - meier plot for progressionfree survival ( pfs ) of the same patients with melanoma who received immune checkpoint inhibition therapy who were assessed by routine radiologic scans ( patients with ctdna decrease [ n = 15 ] v increase [ n = 20 ] )  . 
regarding absolute copy numbers of ctdna across all patients treated , the median ctdna value of nonresponders was 144 copies / ml at 12 weeks of treatment , which was signicantly higher than in responders ( 12 copies / ml ; mann - whitney u test p , .001 ; fig 5c ) and above the threshold dened by roc analysis in the training cohort ( data supplement )  . 
the median was 127 copies / ml in patients with a pfs shorter than 6 months and , thus , signicantly higher than in patients with a pfs longer than 6 months ( 14 copies / ml ; mann - whitney u test p = .003 ; fig 5d )  . 
 ( c - d ) scatter dot plots of brafv600e , nrasq61 , and tertprom ctdna levels of responders versus nonresponders , grouped according to ( c ) radiologic response 12 weeks after receiving any therapy or ( d ) radiologic pfs at 6 months of therapy ( mann - whitney u test )  . 
at risk : samples tissue ngs tissue ddpcr plasma ddpcr tissue ngs tissue ddpcr plasma ddpcr tissue ngs tissue ddpcr plasma ddpcr tissue ngs tissue ddpcr plasma ddpcr tissue ngs detected not detected tissue ddpcr brafv600e plasma ddpcr brafv600e nrasq61 hotspot tert c228t tert c250t not detected nrasq61 hotspot tert c228t tert c250t not detected fig 6 . 
kaplan - meier plots for ( a ) radiologic progression - free survival ( pfs ) and ( b ) overall survival ( os ) of patients with brafv600e - positive tumors who received mapk signaling targeted therapy ( n = 21 with positive nrasq61 detection in bl plasma v n = 12 without detection )  . 
 ( c ) overview of 51 brafv600e - , nrasq61 - , and tertprom - matched tumor tissue and plasma samples of patients who had available tumor biopsy specimen at therapy bl . 
plasma was sampled at bl ( ie , before systemic therapy initiation ) and analyzed for ctdnas by droplet digital polymerase chain reaction ( ddpcr )  . to test if potential differences in the assay sensitivities of next - generation sequencing ( ngs ) versus ddpcr accounted for the observed discrepancies of the patients nrasq61 mutational states , we obtained genomic dna isolated from 51 melanoma tissue samples that previously underwent amplicon - targeted ngs and reanalyzed them on the ddpcr platforindeed , of 12 patients with brafv600e mutation whose plasma samples were positive for nrasq61 ctdna at baseline , but with negative tumor tissue according to ngs , eight were also positive in tissue samples when tested with the ddpcr assay ( fig 6c ; data supplement )  . however , in another four cases , only plasma ddpcr could detect the positive mutational nrasq61 state , whereas the tumor sample remained negative by ddpcr . 
 v araljai et al discussion to make precision oncology a reality , highly predictive , noninvasive monitoring technologies must be identied . the application of ctdna to metastatic melanoma has been reported to be a promising tool in terms of detecting the relevant tumor - derived mutant dna over time.2 - 6 , 10 - 19 here , we also considered the clinical signicance of background mutations in the ctdna of healthy individuals for statistical normalization at baseline and then later under therapy . 
this consideration is critical because mutant ctdna , derived from aging cells or from undiscovered cancer cells , also can occur throughout the lifetime of individuals without a known diagnosis of cancer.20 regarding differences between healthy plasma donors and patients with melanoma with radiologically conrmed active tumor mass , we intended to establish a molecular cutoff value with true clinical relevance using roc analysis . 
we conclude that concrete ctdna thresholds are prognostic for outcome and represent a reliable practical tool for routine diagnostics even in the context of background mutant ctdna . another goal of this study was to statistically validate a therapeutic predictive threshold on the basis of roc analyses of longitudinally assessed plasma samples from patients with melanoma with timely matching ct / mri scans . 
accordingly , patients whose ctdna levels were above a threshold of 35.85 copies / ml brafv600e , 51.5 copies / ml nrasq61 , and 32.83 copies / ml tertprom ctdna over 6 to 8 weeks despite therapy had signicantly shorter pfs as compared with patients whose ctdna levels remained below these thresholds . 
all the ctdna assays applied here were signicantly better indicators of measurable disease than were ldh or s100 levels . despite the practicability of molecular thresholds , our study indicates that the mean change in the ctdna level over consecutive time points compared with the baseline represents an additional signicant indicator of treatment effectiveness . 
our study also showed that ctdna changes relative to the previous sampling time point or even the rate of ctdna increase per week ( data supplement ) can serve as an early hint of progression in patients receiving therapy . tumor tissuebased mutational testing ( eg , by ngs with a sensitivity of approximately 1%21 ) is currently used as clinical state - of - the - art guidance for therapy selection for patients with metastatic melanoma . 
it does not account for intertumor and intrapatient heterogeneity . the issue of instead , liquid biopsies should better assess the full genetic heterogeneity of solid cancers at the systemic disease level . here , we analyzed baseline plasma samples with highly sensitive ddpcr and compared the results with existing ngs - based tissue proles . 
this may indicate that the amplicon - targeted ngs protocol , which was routinely applied to assess the mutational tumor status in our cohorts , may not be sensitive enough to detect low - frequency nras mutations within bulk tumors ( eg , when originating only from minor cell subpopulations )  . 
to test this assumption , we obtained genomic dna isolated from 51 melanoma tissue samples that previously underwent amplicon - targeted ngs and reanalyzed them on the ddpcr platforindeed , of 12 patients with brafv600e mutation whose plasma samples were positive for nrasq61 ctdna at baseline , while having a negative ngs status for nrasq61 , tumor tissue of eight also was positive when tested with the ddpcr assay . 
in contrast , enhancement of the ngs coverage from 103 to 177 and reduction of the mutant discovery threshold from 5% to 1% ( mutant allele frequency ) did not increase the nrasq61 detection rate in a control experiment with selected tissue samples ( data supplement )  . 
previous data suggest that nrasq61 ctdna emerges upon mapki therapy.3 , 16 accordingly , we observed increasing levels of nrasq61 during mapki the absolute nrasq61 copy numbers remained below the brafv600e copy level.3 , 16 therapy ; however , in summary , our study ndings support the importance of ctdna analysis as a valid clinical tool for the provision of real - time information on current treatment response and prediction of future response probability . 
in addition , the comparison of plasma - based ctdna analysis with tumor tissuebased , amplicon - targeted ngs indicated considerable differences in diagnostic sensitivity , particularly with regard to intrapatient tumor heterogeneity . 
vogel , susanne horn , dirk schadendorf , alexander roesch financial support : julia newton - bishop , dirk schadendorf administrative support : klaus griewank , dirk schadendorf , alexander roesch provision of study materials or patients : teola seremet , peter a . 
horn , bart neyns , dirk schadendorf , alexander roesch collection and assembly of data : ren ata v araljai , kilian wistubahamprecht , teola seremet , antje sucker , jan - malte placke , peter a . horn , nils von neuhoff , susanne horn , j urgen c . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . teola seremet employment : janssen ( i ) , glaxosmithkline ( i ) honoraria : novartis , janssen consulting or advisory role : novartis speakers ' bureau : novartis travel , accommodations , expenses : novartis , msd oncology , janssen , leo pharma klaus griewank patents , royalties , other intellectual property : exon 4 mutations in gnaq and gna11 , a rare gene mutation in melanoma . 
horn stock and other ownership interests : share certicates ( aktien ) of different companies patents , royalties , other intellectual property : patent applications support supported by the european union 's horizon 2020 research and innovation program under marie sklodowska - curie grant no . 
 v araljai et al lipson ej , velculescu ve , pritchard ts , et al : circulating tumor dna analysis as a real - time method for monitoring tumor burden in melanoma patients undergoing treatment with immune checkpoint blockade . 
j immunother cancer 2 : 42 , 2014 sanmamed mf , fern andez - land azuri s , rodrguez c , et al : quantitative cell - free circulating brafv600e mutation analysis by use of droplet digital pcr in the follow - up of patients with melanoma being treated with braf inhibitors . 
clin chem 61 : 297 - 304 , 2015 lee jh , long gv , boyd s , et al : circulating tumour dna predicts response to anti - pd1 antibodies in metastatic melanoma . 
ann oncol 28 : 1130 - 1136 , 2017 gangadhar tc , savitch sl , yee ss , et al : feasibility of monitoring advanced melanoma patients using cell - free dna from plasma . 
nazarian r , shi h , wang q , et al : melanomas acquire resistance to b - raf ( v600e ) inhibition by rtk or n - ras upregulation . 
nature 468 : 973 - 977 , 2010 shi h , hugo w , kong x , et al : acquired resistance and clonal evolution in melanoma during braf inhibitor therapy . 
haselmann v , gebhardt c , brechtel i , et al : liquid proling of circulating tumor dna in plasma of melanoma patients for companion diagnostics and monitoring of braf inhibitor therapy . 
santiago - walker a , gagnon r , mazumdar j , et al : correlation of braf mutation status in circulating - free dna and tumor and association with clinical outcome across four brafi and meki clinical trials . 
gonzalez - cao m , mayo - de - las - casas c , molina - vila ma , et al : braf mutation analysis in circulating free tumor dna of melanoma patients treated with braf 13 . 
chang ga , tadepalli js , shao y , et al : sensitivity of plasma brafmutant and nrasmutant cell - free dna assays to detect metastatic melanoma in patients with low recist scores and non - recist disease progression . 
schreuer m , meersseman g , van den herrewegen s , et al : quantitative assessment of braf v600 mutant circulating cell - free tumor dna as a tool for therapeutic monitoring in metastatic melanoma patients treated with braf / mek inhibitors . 
lee jh , long gv , menzies am , et al : association between circulating tumor dna and pseudoprogression in patients with metastatic melanoma treated with antiprogrammed cell death 1 antibodies . 
xi l , pham th - t , payabyab ec , et al : circulating tumor dna as an early indicator of response to t - cell transfer immunotherapy in metastatic melanoma . 
blumenthal , md1 ; and reena philip , phd1 purpose next - generation sequencing ( ngs ) oncology panels are becoming integral in hospital and academic settings to guide patient treatment and enrollment in clinical trials . 
although ngs technologies have revolutionized decision - making for cancer therapeutics , physicians may face many challenges in parsing and prioritizing ngs - based test results to determine the best course of treatment for individual patients . 
here , we discuss the presentations and discussion highlights across the four sessions of the workshop . methods the goal of the public workshop was to engage stakeholders and solicit input from experts in precision oncology to discuss the integration of complex ngs data into patient management and regulatory innovation within the precision oncology community . 
the us food and drug administration gathered representatives from academia , industry , patient advocacy , government , and professional organizations for a series of presentations followed by panel discussions . 
after the workshop , the transcript and speaker presentation slides were reviewed and summarized for manuscript preparation . results speakers and panelists provided diverse perspectives on the integration of ngs technology into patient care for oncology and on the complexities that surround data interpretation and sharing . 
2019 by american society of clinical oncology introduction the goal of precision oncology is to use the genetic informationgermline or somaticfrom a patient with cancer to help determine which drug ( s ) might be most effective in treating his or her disease . 
next - generation sequencing ( ngs ) is increasingly used in precision oncology because of its ability to identify many mutations simultaneously , thereby maximizing the amount of information obtained from a single test.1 the global endeavor to identify somatic mutations within a patients tumor genome has led to an unprecedented amount of genomic information , with varying degrees of associated clinical evidence . 
ngs can report a vast number of mutations which may lead to clinician uncertainty in the interpretation and prioritization of mutations with respect to the clinical signicance and optimal course of treatment.2 in january 2017 , the association for molecular pathology ( amp ) , asco , and the college of american pathologists ( cap ) published a joint consensus recommendation for standards and guidelines for the interpretation and reporting of sequence variants in cancer3 ; however , stakeholders have not consistently implemented these recommendations . 
 horne et al context key objective to provide an overview of a public workshop hosted by the us food and drug administration that discussed key concepts and considerations for the classication and interpretation of genetic variants in precision oncology . knowledge generated key highlights and ndings from the discussion include the conclusion that as the use of next - generation sequencing oncopanels in the clinical setting increases , it is critical to develop a framework that ensures accurate and consistent interpretation of genetic variants . 
in addition , transparency in data sourcing and reporting methodologies , as well as frequent updating of variant interpretations , are necessary to advance science and appropriately care for patients . relevance as precision medicine advances , clear communication among stakeholders in oncology will be key to creating an environment that facilitates generating and sharing data that have value to patients . treatement options , in addition to providing tumor proling data.6 , 7 with fda approval and authorization of these two ngs - based pan - tumor oncology panels ( oncopanels ) , the agency was in a unique position to foster a dialogue among key stakeholders about this innovative technology . input on january 29 , 2018 , the fda held a public workshop to engage stakeholders and solicit from experts in precision oncology and patient representatives to discuss how genetic sequencing data could be best implemented in patient management . 
to set the stage for the workshop discussion , dr philip outlined the fdas new regulatory pathway for ngs tumor - proling tests , as summarized in the fdas center for devices and radiologic health fact sheet published online on november 15 , 2017.8 as described by dr philip , the agencys three - tiered approach for reporting biomarkers in tumor - proling ngs tests includes the following : level 1 , companion diagnostic claims ; level 2 , cancer mutations with evidence of clinical signicance ; and level 3 , cancer mutations with potential clinical signicance . 
tumor - proling ngs tests may include companion diagnostic claims ( level 1 ) that are prescriptive for a specic therapy and are supported by the clinical validity of the test for each biomarker reported . 
bowles , phd , myriad genetic laboratories best practices for the use of clinical databases for variant classication and facmg interpretation in clinical oncology session 4 : future directions for data sharing , standardization , and establishing consistency in precision oncology dane dickson , md cureone us food and drug administration public workshop : variant classication dennis dean , phd seven bridges genomics creating a community view : standards , analyses , and data to advance robert grossman , phd university of chicago the important role of data commons for sharing variant classication and consistency in precision oncology interpretation data in precision oncology len lichtenfeld , md american cancer society cancer action panelist network * afliations noted in the table are based on speaker afliations at the time of the public workshop and may not reect the current afliation . validity has not been demonstrated either in professional guidelines or with the test , but is suggestive on the basis of clinical / biologic evidence . session 1 : overview of the state of science for sequence variant classication in oncology and its practical use in treating patients use of an individuals mutation prole for clinical decision making is driving the ever - expanding number of biomarkerbased clinical trials and clinical regimens in precision oncology . 
 horne et al vincent miller , md , indicated that fmi lters out germline mutations but further noted that when reporting germline mutations , laboratories need to have an operation in place , or at least have an understanding with the clinicians , so that the information can be followed up with genetic counseling . comprehensive variant annotation is necessary to inform treatment selection and match patients to clinical trials . 
the number of patients who are matched to either clinical trials or personalized treatments on the basis of their genomic data were reported by panelists to be between 10% and 37% . 
to compile and interpret the evidence , scientists and pathologists continually gather new information from guidelines , published literature , public databases , clinical trials , fdaapproved therapeutic labeling , and other sources . 
this comprehensive information is then used to sort biomarkers , either manually or in combination with bioinformatics software algorithms , on the basis of levels of evidence . panelists concluded that a key to the success of somatic genotyping will be developing statistical tools and bioinformatics infrastructure to identify clinically meaningful mutations . 
dr berger noted that as more sequencing data accumulates , integrated analyses of big data will allow for the identication of novel hotspot mutations occurring at frequencies greater than would be expected by chance . this approach would allow for these novel mutations to be directly tested in targeted clinical trials to assess drug sensitivity . 
panelists noted that the eld will continue to evolve and become more challenging with the increase in tissue - agnostic trials in which patients are enrolled on the basis of biomarker status , irrespective of the tumor type , which could , in turn , lead to an increase in tissue - agnostic drug indications . 
john deeken , md , also highlighted some of the unique challenges faced when running an in - house 50 - gene oncopanel at a community - based hospital system . these challenges included the cost of developing and supporting an oncopanel test and the lack of reimbursement for the majority of ngs testing performed . 
donna roscoe , phd , noted that the fda is striving to ensure that there are validated tests on the market that will allow for dynamic use within clinical settings to enable clinicians to optimize patient decisions in oncology and other therapeutic areas . session 2 : levels of evidence required for reporting variants and guiding patient treatment widespread implementation of ngs data in clinical settings has been accompanied by challenges in standardization , interpretation , and reporting of genetic tests . 
shashikant kulkarni , phd , provided an overview of the proposed guidelines published by a multidisciplinary working group convened by amp , asco , and cap for variant interpretation and reporting.3 the four - tiered system to categorize somatic sequence variations on the basis of their levels of evidence are as follows : tier i , variants with strong clinical signicance ; tier ii , variants with potential clinical signicance ; tier iii , variants of unknown clinical signicance ; and tier iv , variants deemed benign or likely benign.3 guidelines were developed to provide a general framework , on the basis of an evidence - based variant classication approach , for the standardized interpretation and reporting of somatic variants in cancer . 
for example , variants with strong clinical evidence include those with level a evidence ( fda - approved therapies or included in professional guidelines ) or level b evidence ( well - powered studies with consensus from experts in the eld )  . 
variants with potential clinical evidence are those with level c evidence ( fda - approved therapies for different tumor types or investigational therapies of multiple small published studies with some consensus ) or level d evidence ( preclinical trials or found in a few case reports without consensus )  . in general , it is widely accepted that tests should be optimized to ensure coverage across targets and high sensitivity for detecting low - frequency mutations ; however , as noted in the consensus manuscript , 3 the eld is split on the use of variant allele frequency ( vaf ) in reporting and clinical practice . 
one perspective , provided from a workshop attendee , was that if frequencies are too low , the detected mutations could represent subclonal events and may not necessarily be appropriate therapeutic targets . 
on the contrary , apostolia - maria tsimberidou , md , phd , noted that , as a clinical investigator , there is utility in having allele fraction present in the patient report as the data could be used to interpret clinical outcomes , particularly because patients have multiple molecular alterations . 
a consensus was not reached by workshop panelists or attendees regarding the clinical use or validity of reporting vaf in precision oncology . standardizing the annotation and reporting of somatic mutations from ngs data remains a challenge . 
john pfeifer , md , phd , pointed out that there is a gray zone between where the technical portion of the ngs test ends and the practice of medicine begins . 
although many of the speakers and panelists used the amp / asco / cap guidelines , several groups used a slightly modied tiering system . panelists generally agreed that treatment options for tier ii and below , as noted in the amp / asco / cap guidelines , should be considered only once tier i treatment options have been exhausted . 
moreover , panelists expressed the need to create a databasethat is , a knowledge basethat can assist in resolving discordances in variant interpretation and allow for the generation of community standards . session 3 : best practices for use of public / private databases for variant classication and interpretation in oncology to positively affect patient care , mutations detected using ngs technology must be appropriately interpreted and classied . 
the panel unanimously agreed that a known drawback to using publicly available databases for variant classication is that interpretation is not always consistent . heidi rehm , phd , noted that the quality of the data rests in the hands of those who deposit the information into the database and that amassing sufcient information to provide high - quality classication data requires global sharing . kenna shaw , phd , afrmed that standards and rules are needed to not only interpret but reinterpret variant classication , and she summarized the efforts being conducted at her institution to amass a personalized cancer therapy knowledge base . 
dr shaw provided an overview of aacr project genie ( genomics evidence neoplasia information exchange ) , which presently includes 17 institutions across the world that are working together to develop a regulatorygrade registry that aggregates and links cancer genomic data with clinical outcomes from tens of thousands of cancer patients . 
project genie will allow for sharing of the accumulated data with the global research community through cbioportal and the synapse platform with the noted caveat that the underlying functional evidence int the knowledge base will continue to change over time . panelists agreed that databases should be transparent about data sources , methods , and rules used for reporting mutation - associated clinical claims . 
karla bowles , phd , noted that subjective tools , such as literature reviews , population data , and structural analysis , should be used with caution , as interpretations from these data are often sources of discrepancies . 
the number of session 4 : future directions for data sharing , standardization , and establishing consistency in precision oncology many mutations identied by genomic tests for oncology are novel , rare , or otherwise lack conclusive evidence to support a clinical these mutations will only increase as additional genes are added to oncopanels and the costs of sequencing decrease . understanding the clinical utility of these mutations requires addressing barriers that prevent accurate classication . 
dane dickson , md , cited improved data sharing as a critical need and described the utility of high - quality databases that include both diagnostic results and clinical outcomes . dennis dean , phd , described the need for interoperability of complex systems and tools to enable analysis of large data sets . interoperability requires standards and languages to support reproducibility . 
dean discussed rabix , a suite of open - source development tools for creating and running computation workows , as a development environment that uses common workow language to promote the analysis of combined large data sets . 
robert grossman , phd , emphasized the need for data commonsthat is , a unied data system that promotes sharingsuch as the national cancer institute that use data models and genomic data commons , metadata services to harmonize and share cancer genomic datasets . 
grossman discussed the concept of leveraging funders , journal editors , and payers to incentivize the data sharing required to build a data commons . as a patient advocate , len lichtenfeld , md , discussed the challenges of translating the information generated by large - scale projects to communities that lack the resources and infrastructure to access the latest information necessary to improve care . 
 horne et al in conclusion , precision oncology is a rapidly evolving eld . with more oncopanels being developed , and as more genomic and patient outcome data accumulate , physicians are faced with new challenges in interpreting ngs - based test results to determine the best treatment course for each patient . 
in addition , there are multiple public and private databases available that aid in variant classication and interpretation ; however , methods used to classify variants and how these databases align remain unclear . 
to that end , the fda recently nalized a guidance document entitled , use of public human genetic variant databases to support clinical validity for genetic and genomic - based in vitro diagnostics . 
david litwack employment : prevail therapeutics travel , accommodations , expenses : prevail therapeutics no other potential conicts of interest were reported . acknowledgment the authors thank all event staff at the us food and drug administration for helping to execute a seamless public workshop that was benecial to both in - person and online attendees . 
the authors thank the workshop presenters who graciously provided their permission to publish details about their titles and summaries in the manuscript table and text . references strom sp : current practices and guidelines for clinical next - generation sequencing oncology testing . 
n engl j med 375 : 711 - 713 , 2016 li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
us food and drug administration : use of public human genetic variant databases to support clinical validity for genetic and genomic - based in vitro diagnostics : guidance for stakholders and food and drug administration staff . 
us food and drug administration : public workshop - - weighing the evidence : variant classication and interpretation in precision oncology , january 29 , 2018 , workshops and conferences ( medical devices )  . 
 biomarkers intratumoral transcriptome heterogeneity is associated with patient prognosis and sidedness in patients with colorectal cancer treated with anti - egfr therapy from the co.20 trial elisa fontana , md , phd1 , 2 ; gift nyamundanda , phd1 , 2 ; david cunningham , md3 ; dongsheng tu , phd4 ; maggie c.u. 
siu , md8 ; francesco sclafani , md3 , 9 ; katherine eason , phd1 ; chanthirika ragulan , msc1 , 2 ; maria antonietta bali , md , phd10 , 11 ; sanna hulkki - wilson , bsc1 ; jonathan m . 
waring , mbbs , phd13 ; mirella giordano , phd14 ; patrick lawrence , ms1 , 2 ; daniel nava rodrigues , md3 ; ruwaida begum , bsc3 ; jeremy d . 
price , md16 ; chiara cremolini , md17 , 18 ; naureen starling , mbbs , mrcp , md ( res ) 3 ; filippo pietrantonio , md19 , 20 ; livio trusolino , md , phd21 , 22 ; christopher j . 
ocallaghan , dvm , msc , phd4 ; and anguraj sadanandam , phd1 , 2 purpose metastatic colorectal cancers ( mcrcs ) assigned to the transit - amplifying ( ta ) crcassigner subtype are more sensitive to antiepidermal growth factor receptor ( egfr ) therapy . 
progression - free survival ( pfs ) , overall survival ( os ) , and disease control rate ( dcr ) according to ta - ness classication were assessed by univariate and multivariate analyses . results the ta - ness was measured in 772 samples from 712 patients . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction epidermal growth factor receptor ( egfr ) - targeting antibodies cetuximab and panitumumab are available treatment options for approximately 40% of patients with metastatic colorectal cancer ( mcrc ) .1 patient selection based on ras and braf wild - type status and sidedness has improved overall response rates and survival outcomes . 
nevertheless , 30% - 60% of eligible patients do not benet from these expensive drugs.2 - 4 as a shift from the traditional paradigm of negative molecular selection , we previously demonstrated that the transit - amplifying ( ta ) crcassigner ( crca ) subtype was enriched for cetuximab - responsive tumors , 5 a nding independently validated in a clinical study , 6 in a panel of crc xenografts5 and cell lines.5 , 7 however , responses were also seen in other groups , such as the poorly differentiated stem - like subtype , 5 , 7 albeit at a lower frequency . 
 intratumoral transcriptome heterogeneity and anti - egfr therapy context key objective to evaluate whether the presence of the transit - amplifying ( ta ) subtype gene signature ( dubbed as ta - ness classication ) representing the intratumoral transcriptome heterogeneity is associated with antiepidermal growth factor receptor ( egfr ) therapy outcomes . knowledge generated the ta - ness classication is an easily detectable biomarker of intratumoral transcriptome heterogeneity , which was retrospectively evaluated in 712 patient samples , including those from a clinical ( co.20 ) trial , which showed prognostic signicance in patients treated with anti - egfr therapy . 
this biomarker provides additional biologic insights for the association between ras / braf wild - type left - sided tumors ( enriched for ta - high ) and anti - egfr therapy benet . relevance with further validation , ta - ness may represent a positive selection biomarker for patients with ras / braf wild - type left - sided metastatic colorectal cancer who are most likely to benet from anti - egfr therapy . ta subtype tumors are characterized by gene signatures similar to normal ta cells of the colonic crypt , that is , those in transit between stem cells in the crypt base and differentiated cells at the top of the crypt.5 after asymmetric division , stem cells generate rapidly proliferating ta cells characterized by increased egfr expression that eventually differentiate into goblet cells and enterocytes.8 , 9 we evaluated a hypothesis that tumors with increased ta gene signature expression ( irrespective of ta or other subtypes ) may be associated with anti - egfr therapy outcomes . 
the discovery cohort included chemorefractory patients ( n = 84 ) who had received anti - egfr therapy as a single agent or in combination with chemotherapy after progression while receiving irinotecan ( during or within 3 months from the end of treatment ) as part of standard treatment at the royal marsden hospital ( rmh ; n = 59 ; united kingdom , ethics committee : 10 / h0308 / 28 ; and clinicaltrials.gov identier : nct02112357 ) or within the context of a case - control study in italian institutions ( pressing , n = 25 ; ethics committee area vasta nord ovest number 1333 / 173 )  . 
nineteen and 12 patients from the rmh cohort were treated before the implementation of kras testing ( august 2009 ) and extended ras testing ( december 2011 ) , respectively.11 , 12 all patient samples from the pressing study had extended ras / braf wildtype tumors . one of the clinical validation cohorts included 121 patients with kras exon 2 wild - type tumors who had received single - agent cetuximab within the control arm of the co.20 phase iii randomized clinical trial ( clinicaltrials.gov identier : nct00640471 ) .13 this correlative analysis was approved by the joint canadian cancer trial group and australasian gastrointestinal trial group ( cctg / agitg ) correlative sciences and tumor biology committee . two additional public gene expression datasets ( n = 397 ; not treated with anti - egfr therapy ) of primary crc samples ( gse39582 ; n = 328 ) and liver mcrc lesions ( gse73255 ; n = 69 ) were evaluated.14 , 15 only samples with known kras wild - type status were selected . nucleic acids extraction formalin - xed parafn - embedded ( ffpe ) tissues were least evaluated by a trained pathologist ; areas with at 30% of tumor content were marked on hematoxylin and eosin slides and macrodissected in unstained slides ( 7to 10 - m thickness )  . 
after deparafnization , total rna and dna were simultaneously isolated using the ambion recoverall kit ( discovery ) or qiaamp nucleic acid ffpe tissue kit ( validation ) and quantied with nanodrop 2000 spectrophotometer ( thermo fisher , waltham , ma ) according to the manufacturers instructions . 
 a fontana et al discovery cohort retrospective tissue collections validation cohort 1 prospectively enrolled in the co.20 study outcome cohort ta - ness no . median pfs ( months ) univariate analysis hazard ratio ( 95% ci ) log - rank multivariate analysis hazard ratio ( 95% ci ) cox regression rmh cohort ( n = 90 ) italian cohort ( n = 42 ) patients ( out of 374 in cetuximab arm ) ( n = 163 ) patients with quality rna ( n = 65 ) patients with quality rna ( n = 25 ) patients with quality rna ( n = 146 ) excluded because of low tumor content in the block or low rna conc . 
 after extraction ( n = 25 ) patients excluded because of qc flag after ncounter analysis ( n = 6 ) patients excluded for anti - egfr in refractory setting as re - challenge ( n = 17 ) patients excluded because of qc flag after ncounter analysis ( n = 0 ) patients for final analysis ( n = 59 ) patients for final analysis ( n = 25 ) patients for final analysis ( n = 121 ) patients excluded because of low tumor content in the block or low rna conc . 
covariates included in the validation cohort : eastern cooperative oncology group performance status , sex , age , baseline lactate dehydrogenase level , baseline alkaline phosphatase , baseline hemoglobin , number of disease sites , number of previous chemotherapy drug classes , prior vegfr target therapy , and presence of liver metastases . 
conc. , concentration ; egfr , epidermal growth factor receptor ; pdx , patient - derived xenograft ; qc , quality control ; rmh , royal marsden hospital . ve published crca - 38 centroids ( expression summary of each gene in each subtype ) 16 and gene expression , each sample was assigned either to ta - high ( increased expression of ta signature genes ) or ta - low ( reduced expression ) ta - ness classes . 
when gene expression proles were compared with the ve crca - 38 centroids , ve correlation coefcients ( one for each subtype - centroid ) were calculated for each sample . 
the coefcients were then ranked from highest to lowest ; ta - high samples were those with a correlation coefcient value for the ta centroid ranking within the rst three highest values ; ta - low samples were those with a correlation coefcient for the ta centroid , which is second to last or the lowest . 
therefore , the ta - ness classication represents a measure of transcriptome - based intratumoral heterogeneity in mcrc , based on the idea that each sample can contain more than one subtype . 
this best cut - off for ta - ness classication was established based on the highest accuracy in dening disease control , measured as area under the curve ( auc ) of a receiver operating characteristic ( roc ) curve ( appendix fig a1 )  . statistical analysis progression - free survival ( pfs ) was the primary endpoint . overall survival ( os ) , disease control rate ( dcr ) , and response rate were secondary endpoints . 
fishers exact test was used to compare categorical variables , and wilcoxon signed rank test with p , .05 was used to assess the association between ta - ness classes and percentage of tumor shrinkage ( using recist ) criteria in a subgroup of the discovery cohort . 
although the statistical analysis of discovery cohort was performed by the institute of cancer research statistician , the validation cohort was independently analyzed by cctg / agitg investigators blinded to the biomarker cut - off analysis . 
additional methods are available in the data supplement . results retrospective antiegfr - treated tumor samples from 205 patients were identied from the discovery and validation ( co.20 ) cohorts after clinical review and quality control of the tumor blocks and tumor - derived rna ( fig 1a )  . 
 intratumoral transcriptome heterogeneity and anti - egfr therapy cohort from 30 patients along with 30 patient - derived xenografts ( pdxs ; derived from the patient tumors ) that were treated with anti - egfr therapy or vehicle ( control ) were subjected to the same crca gene expression assay . 
in addition , publicly available gene expression microarray data for 80 patients with mcrc ( treated with anti - egfr therapy ) was included as an additional clinical validation cohort.17 this publicly available cohort also served to validate ta - ness classication using a different platform ( microarrays ; fig 1a )  . patient characteristics for discovery and validation co.20 cohorts are shown in the data supplement . 
with the exception of sex , there were no signicant differences in patients characteristics between the co.20 subgroup included in this analysis and the overall co.20 clinical trial cohort ( data supplement )  . using conventional subtyping , 15 of 84 samples belonged to the ta subtype in the discovery cohort . 
the association of ta - ness classication with both pfs and dcr remained signicant after adjusting for multiple variables in both the discovery and validation cohorts ( fig 1b )  . 
conversely , after adjusting for multiple variables , signicant association of ta - ness with os was only borderline ( or not signicant with p = .1 in the discovery cohort and p = .06 in the validation cohort ; data supplement ) ; postprogression treatment information was not available . in the discovery cohort , ta - high tumors ( 62% ; n = 52 ) were predominantly ras / braf wild - type ( 69% ; n = 36 ) and were found in the left side of the colon ( 79% ; n = 41 )  . 
this result was mirrored in the experimental cohort , 18 , 19 in which 30 ras / braf wild - type liver metastases were classied into ta - high ( n = 16 ) and ta - low ( n = 14 ) classes . 
the percentage of cetuximab - induced tumor volume change in the pdx - based mouse - propagated patient metastatic tumors was signicantly associated ( p , .042 ) with the ta - ness signature ( fig 3b )  . in the discovery cohort , the ta - ness classication was assessed using samples from primary tumors in 76% of patients and samples from metastatic sites in 24% of patients . 
to further conrm that the association was independent of the diagnostic sample of origin and to further validate the results , we examined the khambata - ford publicly available ( microarray ) dataset17 of mcrc samples from patients treated with cetuximab . 
to further conrm that the ta - ness can be assessed in both primary tumors and metastatic lesions , kras wild - type samples from two publicly available datasets14 , 15 were selected ; 328 primary tumors and 69 liver metastases were classied into ta - high and ta - low . 
similar distribution of the two classes was demonstrated ( fig 3c )  . beyond ras / braf mutational status , sidedness is a recognized selection factor for anti - egfr therapy benet : patients with left - sided tumors benet more than patients with right - sided tumors.4 however , the biology behind this association remains unclear . 
first , we further conrmed signicant association ( p , .001 ) between ta - ness classication and sidedness in kras wild - type primary tumors ( gse39582 ; fig 3d )  . 
then , we sought to discover whether the ta - ness classication could further rene the selection of patients in addition to ras / braf status and sidedness . within discovery and validation cohorts ( n = 205 ) , highsensitivity next - generation sequencing ras / braf mutational analysis was available for 118 patients : 71 were classied as ras / braf wild - type , of which 53 were assigned to ta - high ( 75% ) class . 
 ( a ) a waterfall plot showing a subgroup of patients within the discovery cohort ( n = 35 ) showing disease response ( treated with anti epidermal growth factor receptor [ egfr ] drug ) according to recist criteria and ta - ness classication . 
 ( b ) a waterfall plot showing change in tumor ( percent ) volume in anti - egfrtreated mouse - propagated patient tumor samples ( n = 30 ) compared with matched control treated ( baseline ; n = 30 ) mouse - propagated patient tumors . 
the bars in the graph show ta - ness classication for the matched patient metastatic liver samples ( n = 30 ) , and the bars below the graph show the same classication for matched mousepropagated patient tumors ( treated v control )  . 
this classication has the advantage of providing a qualitative assessment in all the samples , including the non - ta subtypes , overcoming the limitations posed by intratumoral heterogeneity when using the conventional molecular subtyping classication as a potential tool to assess benet from anti - egfr therapy . 
kaplan - meier survival curves of patients with transit - amplifying ( ta ) - high versus ta - low tumors treated with antiepidermal growth factor receptor ( egfr ) therapy . 
 fontana et al ( and potentially clinical benet ) in patients treated with anti - egfrbased therapy in our discovery cohort ; this was validated in a kras exon 2 wild - type trial cohort of cetuximab - onlytreated patients , 13 which has the advantage of properly assessing prognostic value in a homogeneously treated population and in the absence of confounding effect of chemotherapy . 
moreover , ta - low assignment was enriched for ras / braf - mutant tumors , providing a potential alternative method to estimate prognosis and may be a treatment benet from anti - egfr therapy when the mutational status is missing . 
this signature and its association with anti - egfr treatment outcomes were also conrmed in the publicly available samples from patients with mcrc17 and the preclinical pdx models treated with cetuximab.18 , 19 finally , the taness classication retained prognostic signicance when assessed in either archival primary tumors or metastatic samples in multiple cohorts . 
this is highly clinically relethe classication can be vant , because it means that assessed in metastatic lesions when the primary tumor sample is not available or of poor quality ; however , intrapatient concordance was not assessed ; therefore , additional validation is required . several studies have now evaluated the association between single genes or micrornas ( ereg / areg , her2 , her3 , epha2 , or mir - 31 - 3p ) and responses to anti - egfr therapy.20 in contrast , we evaluated a rened form of our previously published gene expression signature ( with multiple genes ) to identify biologically different crc subtypes with distinct cellular phenotypes.5 , 16 the subtypes summarize a complex network of pathways potentially associated with therapeutic responses , simplifying multiple levels of information derived from heterogeneous samples . hence , the deployment of subtypes and their signatures , instead of single genes , has the advantage of reducing the dimension of complexity without losing biologic information . 
although the crca and consensus molecular subtype ( cms ) classications are highly concordant , 16 , 21 cms classication was not assessed here because it is technically challenging to dichotomize samples into two groups based on the current cms classier ( with multiple centroids )  . this study has some limitations . 
the identication of such patients in the context of clinical trials is challenging ; in fact , the negative predictive value of ras / braf mutations was retrospectively demonstrated in multiple clinical trials , and to our knowledge , none of them was designed with an up - front prospective inclusion of extended ras / braf wild - type tumors . 
last , this was a proof - of - concept study and was retrospectively designed on preexisting tissue collections in the absence of a control group , limiting the assessment of a ta - ness biomarker as prognostic rather than predictive . 
shapiro , chiara cremolini , filippo pietrantonio , livio trusolino , anguraj sadanandam data analysis and interpretation : elisa fontana , gift nyamundanda , david cunningham , dongsheng tu , maggie c . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . elisa fontana consulting or advisory role : astellas pharma ( i ) , celgene ( i ) , servier ( i ) , bristol myers squibb ( i ) patents , royalties , other intellectual property : patent no : 1716712.3 pending ( i ) travel , accommodations , expenses : bristol myers squibb ( i ) , servier ( i ) gift nyamundanda patents , royalties , other intellectual property : prognostic and treatment response prediction in gastric cancer priority patent csc / bp7295892 , patient classication and prognostic method patent application number pct / ep2019 / 053845 , patent application number 2011213.2 david cunningham stock and other ownership interests : ovibio consulting or advisory role : ovibio research funding : astrazeneca ( inst ) , amgen ( inst ) , sano ( inst ) , merrimack ( inst ) , celgene ( inst ) , medimmune ( inst ) , bayer ( inst ) , 4sc ( inst ) , clovis oncology ( inst ) , eli lilly ( inst ) , janssen ( inst ) , merck ( inst ) maggie c . 
siu leadership : treadwell therapeutics ( i ) stock and other ownership interests : agios ( i ) consulting or advisory role : merck , astrazeneca / medimmune , morphosys , roche , loxo , voronoi , oncorus , symphogen , mirati therapeutics , gsk , seattle genetics , treadwell therapeutics , arvinas , navire research funding : bristol myers squibb ( inst ) , genentech ( inst ) , glaxosmithkline ( inst ) , merck ( inst ) , novartis ( inst ) , pzer ( inst ) , medimmune ( inst ) , astrazeneca ( inst ) , boehringer ingelheim ( inst ) , bayer ( inst ) , amgen ( inst ) , astellas pharma ( inst ) , shattuck labs ( inst ) , symphogen ( inst ) , avid ( inst ) , mirati therapeutics ( inst ) , intensity therapeutics ( inst ) , karyopharm therapeutics ( inst ) francesco sclafani consulting or advisory role : bayer research funding : bayer ( inst ) , astrazeneca ( inst ) , roche ( inst ) , bristol myers squibb ( inst ) travel , accommodations , expenses : bayer , eli lilly jonathan m . 
waring employment : astrazeneca leadership : pillar biosciences , xing technologies , ori healthcare stock and other ownership interests : genentech , roche ( i ) , pillar biosciences , xing technologies consulting or advisory role : pillar biosciences , xing technologies , ori healthcare travel , accommodations , expenses : pillar biosciences , xing technologies timothy j . 
 fontana et al travel , accommodations , expenses : roche , servier naureen starling honoraria : eli lilly , msd oncology , merck serono , pierre fabre , servier consulting or advisory role : servier , astra zeneca , pzer research funding : astra zeneca ( inst ) , pzer / emd serono ( inst ) , bms ( inst ) travel , accommodations , expenses : msd oncology filippo pietrantonio consulting or advisory role : amgen , merck serono , bayer , eli lilly , sano , roche , servier research funding : bristol myers squibb livio trusolino honoraria : eli lilly , astrazeneca , merck research funding : symphogen ( inst ) , merus ( inst ) , pzer ( inst ) , servier ( inst ) , menarini ( inst ) anguraj sadanandam consulting or advisory role : ploughshare innovations research funding : merck , pierre fabre , bristol myers squibb patents , royalties , other intellectual property : patent colorectal cancer classication with differential prognosis and personalized therapeutic responses ( patent number pct / ib2013 / 060416 ) , prognostic and treatment response prediction in gastric cancer priority patent csc / bp7295892 , patent patient classication and prognostic method ( gep - net ) priority patent ep18425009.0 , patent molecular predictors of therapeutic response to specic anti - cancer agents ( patent number us9506926b2 ) no other potential conicts of interest were reported . acknowledgment we thank all patients and families participating in the studies included in this article . 
tebbutt , hagen kennecke , gabriella fontanini , eugenia zanella , and andrea bertotti for their contributions in the studies included in this article . references van cutsem e , cervantes a , adam r , et al : esmo consensus guidelines for the management of patients with metastatic colorectal cancer . 
ann oncol 27 : 1386 - 1422 , 2016 de roock w , claes b , bernasconi d , et al : effects of kras , braf , nras , and pik3ca mutations on the efcacy of cetuximab plus chemotherapy in chemotherapy - refractory metastatic colorectal cancer : a retrospective consortium analysis . 
lancet oncol 11 : 753 - 762 , 2010 cremolini c , morano f , moretto r , et al : negative hyper - selection of metastatic colorectal cancer patients for anti - egfr monoclonal antibodies : the pressing case - control study . 
ann oncol 28 : 3009 - 3014 , 2017 tejpar s , stintzing s , ciardiello f , et al : prognostic and predictive relevance of primary tumor location in patients with ras wild - type metastatic colorectal cancer : retrospective analyses of the crystal and fire - 3 trials . 
jama oncol 3 : 194 - 201 , 2017 [ erratum : jama oncol 3 : 1742 , 2017 ] sadanandam a , lyssiotis ca , homicsko k , et al : a colorectal cancer classication system that associates cellular phenotype and responses to therapy . 
woolston a , khan k , spain g , et al : genomic and transcriptomic determinants of therapy resistance and immune landscape evolution during anti - egfr treatment in colorectal cancer . 
stem cells int 2017 : 7602951 , 2017 yang yp , ma h , starchenko a , et al : a chimeric egfr protein reporter mouse reveals egfr localization and trafcking in vivo . 
national institute for health and care excellence : cetuximab for the rst - line treatment of metastatic colorectal cancer : technical appraisal guidance [ ta176 ]  . 30 : 520 - 527 , 2019 12 . 
national institute for health and care excellence : panitumumab in combination with chemotherapy for the treatment of metastatic colorectal cancer ( terminated appraisal ) : technical appraisal guidance [ ta240 ]  . 
marisa l , de reyni `es a , duval a , et al : gene expression classication of colon cancer into molecular subtypes : characterization , validation , and prognostic value . 
plos med 10 : e1001453 , 2013 isella c , brundu f , bellomo se , et al : selective analysis of cancer - cell intrinsic transcriptional traits denes novel clinically relevant subtypes of colorectal cancer . 
khambata - ford s , garrett cr , meropol nj , et al : expression of epiregulin and amphiregulin and k - ras mutation status predict disease control in metastatic colorectal cancer patients treated with cetuximab . 
bertotti a , migliardi g , galimi f , et al : a molecularly annotated platform of patient - derived xenografts ( xenopatients ) identies her2 as an effective therapeutic target in cetuximab - resistant colorectal cancer . 
zanella er , galimi f , sassi f , et al : igf2 is an actionable target that identies a distinct subpopulation of colorectal cancer patients with marginal response to 20 . 
receiver operating characteristic ( roc ) curve to determine the best cut - off to dene disease control rate in the discovery cohort . 1 represents samples classied into transit - amplifying ( ta ) tumor with highest ( rank ) correlation with crcassigner ( crca ) - 38 centroids . 
 ( a ) kaplan - meier survival curve of patients with transit - amplifying ( ta ) tumor versus non - ta tumor in the discovery cohort subtyped using conventional subtyping approach . 
 molecular and clinical characterization of a claudin - low subtype of gastric cancer purpose claudin - low molecular subtypes have been identified in breast and bladder cancers and are characterized by low expression of claudins , enrichment for epithelial - to - mesenchymal transition ( emt ) , and tumor - initiating cell ( tic ) features . 
we evaluated whether the claudin - low subtype also exists in gastric cancer . materials and methods four hundred fifteen tumors from the cancer genome atlas ( tcga ) gastric cancer mrna data set were clustered on the claudin , emt , and tic gene sets to identify claudin - low tumors . 
compared with gs subtype , claudin - low subtype had significant activation in rho family of gtpases signaling , which appears to play a key role in its emt and tic properties . 
in the acrg data set , 28 of 300 samples were classified as claudinlow tumors by the 24 - gene predictor and were phenotypically similar to the initially derived claudinlow tumors . 
2017 by american society of clinical oncology introduction claudin - low tumors have been identified as a molecular subtype originally in breast cancer and more recently in bladder cancer on the basis of gene expression profiling.1 , 2 these distinct tumors are characterized by the low expression of tight - junction claudins , enrichment for epithelial - to - mesenchymal transition ( emt ) markers , and tumor - initiating cell ( tic ) features.1 , 2 clinically , claudin - low tumors , which lack luminal differentiation marker expression , are associated with poor prognosis compared with luminal tumors.1 , 3 similar to breast , bladder , and other types of cancer , gastric cancer is a heterogeneous disease and arises from multiple genetic and epigenetic aberrations . 
to better understand the biology that drives gastric cancer , molecular evaluation of gastric cancer has been performed and has led to the identification of key dysregulated pathways and the development of molecular classifications.4 gene expressionbased classifiers were reported by the asian cancer research group ( acrg ) 5 and by lei et al.6 the acrg divided gastric cancer tumors into four subtypes ( microsatellite unstable [ msi ] , emt , and tumor protein 53 active and inactive ) , and lei et al classified gastric cancer tumors into three subtypes ( proliferative , metabolic , and mesenchymal )  . on the basis of an integrative analysis of molecular profiling data , the cancer genome atlas ( tcga ) proposed the following four molecular subtypes of gastric cancer tumors : epstein - barr virus ( ebv ) positive , msi , chromosomally unstable ( cin ) , and genomically stable ( gs ) .7 this classification system first categorizes tumors by ascopubs.org / journal / po jco precision oncology tomohiro f . 
vincent author affiliations appear at the end of this article . supported by the university cancer research fund of the lineberger comprehensive cancer center at the university of north carolina at chapel hill and the university of north carolina at chapel hill oncology clinical translational research training program ( 5k12ca120780 )  . presented at the asco 2017 gastrointestinal cancers symposium , san francisco , ca , january 1921 , 2017 . corresponding author : benjamin g . 
however , gs subtype was found to have some notable features , including enrichment of lauren diffuse histologic type and alterations in the genes associated with cell adhesion and motility , such as cdh1 and rhoa mutations and cldn18 - arhgap fusions . 
missing values were imputed using the k - nearest neighbor imputation method , and gene expression values were median centered across each gene . results gene expression signatures tight - junction claudin , emt , and tic gene signatures were used in the classification of a claudin - low subtype . 
the set of claudins used was identified by herschkowitz et al.9 the bidirectional pan - cancer emt signature was derived by tan et al.10 the gastric cancerspecific tic signature was derived from the publicly available gene expression omnibus gene expression data set ( gse53276 )  . 
proliferation and immune gene signatures were derived by hippo et al11 and iglesia et al , 12 respectively . identification of a claudin - low subtype data were clustered on the claudin , emt , and tic gene sets using average linkage clustering with a centered correlation similarity metric on the cluster 3.0 platform ( stanford university , stanford , ca )  . 
sigclust2 r software ( statistical significance of clustering 2 ) was run on the node to perform a gaussian distribution analysis , which expands to the entire gene set for each increasing node . 
the data supplement contains additional details on methods . identification of a claudin - low subtype in gastric cancer from adjacent clusters of we performed unsupervised hierarchical clustering on 415 gastric cancer samples from tcga data set using gene signatures representative of biologic characteristics known to define the claudin - low subtype of breast and bladder cancers.1 , 2 this unsupervised hierarchical clustering with these gene signatures revealed a distinct cluster that had characteristics of claudin - low tumors ( fig 1a , highlighted in red )  . 
to ensure that the set of tumors within the presumed claudin - low cluster were homogeneous and distinct tumors , we performed a gaussian distribution analysis ( data supplement )  . 
this method identified a conserved node of 46 tumors ( 11.1% ) that had consensus enrichment for claudin - low features , and these tumors , therefore , were defined as claudin - low subtype . 
classification of the nonclaudin - low tumors ( n = 369 ) was as follows : ebv , 31 tumors ; msi , 79 tumors ; cin , 218 tumors ; and gs , 41 tumors . 
because the claudin - low tumors were identified originally in breast cancer , we applied the previously defined breast cancerspecific claudin - low classifier to tcga gastric cancer samples and found a significant enrichment ( p , .001 , fishers exact test ) of the breast cancerdefined claudin - low tumors within the gastric claudin - low cluster ( data supplement )  . 
this finding further supports the notion that claudin - low tumors exhibit features of previously defined claudin - low tumors . gene expression signature analysis relative to tic and stem - cell features , breast cancer claudin - low tumors express low levels of proliferation genes and are likely slowercycling tumors.1 , 3 we examined proliferation gene expression of gastric cancer by subtype using a previously reported gastric cancerspecific proliferation signature.11 expression of the proliferation - associated genes in the claudinlow subtype was lowest among all the subtypes ( figs 2a and 2b )  . 
despite the apparent similarity to gs subtype , the claudin - low subtype expressed significantly lower levels of proliferation genes than gs subtype ( p , .001 , bonferronicorrected pairwise t test )  . 
 another notable feature of the claudin - low subtype of breast and bladder cancers is high expression of immune cell genes , including t and b cells.1 , 2 to characterize the immune response in gastric claudin - low tumors , we evaluated gene signatures associated with immune cells by molecular subtype using previously defined signatures that correspond to tumor - infiltrating immune cells.12 heat maps of immune signature expression across the 415 samples in order by subtype showed generally high expression in ebv , claudin - low , and gs ( fig 3a )  . 
on the basis of the z scores of the gene signature , expression of all immune signatures other than the b - cell signature was highest in the ebv subtype ( data supplement )  . to assess the level of active immunosuppression , we examined the expression of a previously defined panel of immune checkpoint molecules ( immunosuppression signature ) 2 and found that it was also highest in the ebv subtype ( fig 3b ; data supplement )  . 
this observation is in line with the previous report by strong et al.13 wherein ebvpositive gastric carcinoma samples expressed high levels of the cytotoxic t - cell and natural killer cell inhibitor indoleamine - 2 , 3 - dioxygenase 1 , which leads to the induction of immune tolerance to tumors despite the elevated immune cell infiltration . 
similar to the previous analysis of bladder cancer , a clear correlation existed between the immune signatures and the immunosuppression signature across all gastric cancer subtypes2 ( data supplement )  . the prognostic impact of tumor - immune infiltrates , especially tumor - infiltrating lymphocytes ( tils ) , has been reported in multiple tumor types.14 , 15 for instance , the presence of cd8 + tils was associated with favorable survival outcomes.16 - 18 some studies evaluated the prognostic relevance of tils in gastric cancer , but the results were not consistent across them.19 - 21 we performed cox proportional hazards regression modeling for each immune gene signature , including immunosuppression signature , across all tumors and within each subtype . 
none of the signatures were prognostic in tcga gastric cancer samples ( data not shown )  . we explored potential mechanisms of immune response by examining predicted neoantigen burden and levels of cytokines and chemokines among subtypes . 
 ( a ) heat map of supervised clustering of gastric cancer subtypes across previously identified proliferationassociated genes ( n = 415 )  . ( b ) box plot of proliferation gene signature z scores across gastric cancer subtypes ( n = 415 )  . significance was determined by one - way analysis of variance ( anova )  . 
 ( b ) box plot of immune suppression gene signature z scores across gastric cancer subtypes ( n = 415 )  . significance was determined by one - way analysis of variance ( anova )  . 
 ( c ) and ( d ) box plots show the number of predicted neoantigens with a half - maximal inhibitory concentration , 150 nm by tumor molecular subtype . significance was determined by kruskalwallis exact test ( n = 357 )  . ( e ) box plot of cytokine and chemokine signature z scores across gastric cancer subtypes ( n = 415 )  . significance was determined by one - way anova . 
cin , chromosomally unstable ; ebv , epstein - barr virus ; gs , genomically stable ; igg , immunoglobulin g ; mac th1 , macrophageassociated t helper 1 ; msi , microsatellite unstable . difference in immune infiltration among subtypes because the predicted neoantigen burdens of ebv , claudin - low , and gs subtypes were lower than that of cin subtype and relatively similar to one another ( fig 3d )  . we next examined the relative expression of a previously defined panel of cytokines and chemokines by subtype2 and observed a strong correlation between this expression signature and multiple immune signatures , including immunosuppression signature ( data supplement )  . 
overall , claudin - low tumors appeared to have a high level of immune infiltration but lacked active immunosuppression within the tumor microenvironment . pathway analysis given that claudin - low tumors were primarily found in gs subtype , we performed ingenuity pathway analysis ( ipa ) and gene set enrichment analysis to understand the gene expression patterns that differentiate claudin - low tumors from nonclaudin - low gs tumors . 
ipa revealed that claudin - low subtype had significant activation in rho family of gtpases signaling and significant inactivation in rho guanine nucleotide dissociation inhibitor ( gdi ) signaling compared with gs subtype ( fig 4 )  . 
rhoa ( a member of the rho family of gtpases ) signaling has been reported to promote cancer stem - celllike phenotype in diffuse - type gastric cancer.22 in addition , claudinlow subtype had higher levels of actin cytoskeleton and integrin signaling relative to signaling levels in gs subtype . 
these observations are in keeping with the tic and emt phenotypes , which are defining characteristics of claudin - low tumors . mutation and copy number alteration analysis we next examined somatic mutations and copy number alterations using tcga data set to compare genomic events of claudin - low subtype with those of nonclaudin - low gs subtype ( data supplement )  . 
tcga network reported rhoa and cdh1 mutations , and cldn18 - arhgap fusions were enriched in gs subtype.7 we did not observe significant differences in the frequency of these genomic events between the two subtypes ( data supplement )  . 
nonclaudin - low tumors ( n = 272 ) were classified into the following subtypes : ebv , 17 tumors ; msi , 63 tumors ; cin , 162 tumors ; and gs , 30 tumors . 
we found that claudin - low subtype in the acrg data set was phenotypically similar to the initially derived claudin - low subtype in the discovery tcga data set as measured by expression of the claudin , emt , and tic gene signatures ( data supplement )  . 
bar graph of the most significantly activated ( gold ) or inactivated ( blue ) signaling pathways in claudin - low subtype ( n = 46 ) compared with gs subtype ( n = 41 )  . significance was determined using ipa software . 
to further compare prognosis for claudin - low subtype with gs subtype , with adjustment for potential confounders ( age and pathologic stage ) , we performed cox proportional hazards regression modeling by setting gs type as a reference group ( table 1 )  . 
in addition , we assessed a prognostic value of claudin - low subtype in patients with stage iii cancer because it was the largest subgroup with the most equal distribution of subtypes . 
similar hrs from the two independent data sets suggest that claudin - low subtype of gastric cancer has a poor prognosis as a result of its unique biologic features . tcga overall survival by subtype acrg overall survival by subtype claudin fig 5 . 
prognosis of claudin - low tumors in ( a ) the cancer genome atlas ( tcga ) and ( b ) the asian cancer research group ( acrg ) data sets . unadjusted kaplan - meier plots show overall survival of gastric cancer by molecular subtype . significance was determined by log - rank test ( n = 415 in tcga cohort ; n = 300 in the acrg cohort )  . 
thus , we especially focused on comparing molecular and clinical features of claudin - low tumors with those of nonclaudin - low gs tumors . claudin - low gastric cancer was defined by low expression levels of tight - junction claudins , high levels of emt , and enrichment for tic signatures . 
in addition , compared with gs subtype , claudin - low subtype had the lower expression of proliferation signature , significant activation in rho family of gtpases signaling , and enrichment of cell motility and adhesion - associated pathways . furthermore , the claudin - low subtype conferred significantly worse prognosis than the gs subtype , which had comparable survival to the cin and ebv subtypes . 
these observations support the claim that claudin - low subtype is distinct from gs subtype and warrants additional validation in prospective studies . we report a 24 - gene classifier that accurately classifies gastric cancer into claudin - low and non claudin - low subtypes . 
we applied this classifier to the acrg data set and identified 28 claudin - low tumors that were phenotypically similar to the initially derived claudin - low subtype in the discovery data set . 
adjusted for age and pathologic stage ( n = 415 in tcga cohort ; n = 300 in the acrg cohort )  . abbreviations : acrg , asian cancer research group ; cin , chromosomally unstable ; ebv , epsteinbarr virus ; gs , genomically stable ; msi , microsatellite unstable ; tcga , the cancer genome atlas . are also characterized by low expression of claudins and enrichment for tic signatures . 
the combined expression of emt and cancer stem - cell makers was reported to be associated with aggressive clinical features , such as vascular invasion and metastasis , and prognostic of poorer disease - free and overall survival in a study of 276 patients with gastric cancer.25 moreover , emt and / or stem - celllike biologic processes have been linked to resistance to chemotherapy and radiation.26 - 28 the mechanisms of therapeutic resistance include relative quiescence , expression of atp - binding cassette transporters , an active dna - repair capacity , and a resistance to apoptosis.29 recent work by yoon et al22 demonstrated a role of rhoa , a member of the rho family of gtpases , in gastric cancer stem - like cells ( cscs ) for the maintenance of emt phenotypes and chemotherapy resistance . 
furthermore , rhoa pathway inhibition reversed chemoresistance in diffuse gastric cscs resistant to fluorouracil and cisplatof note , our ipa revealed that , compared with gs subtype , the most significantly activated and inactivated pathway in claudin - low subtype were rho family of gtpases signaling and rhogdi signaling , respectively . 
gdis are regulators of rho gtpases and prevent activation of gtpases by acting as molecular chaperones.30 all things considered , dysregulated rho gtpase signaling appears to play a key role in the biology of gastric claudinlow tumors and contributes to the poor prognosis . 
sanoff research funding : bayer ag ( inst ) , novartis ( inst ) , merck ( inst ) , precision biologics ( inst ) , immunomedics ( inst ) references 1 . 
sabatier r , finetti p , guille a , et al : claudin - low breast cancers : clinical , pathological , molecular and prognostic jci insight 1 : e85902 , 2016 characterization . 
lei z , tan ib , das k , et al : identification of molecular subtypes of gastric cancer with different responses to pi3 - kinase inhibitors and 5 - fluorouracil . 
tan tz , miow qh , miki y , et al : epithelial - mesenchymal transition spectrum quantification and its efficacy in deciphering survival and drug responses of cancer patients . 
strong mj , xu g , coco j , et al : differences in gastric carcinoma microenvironment stratify according to ebv infection intensity : implications for possible immune adjuvant therapy . 
gooden mj , de bock gh , leffers n , et al : the prognostic influence of tumour - infiltrating lymphocytes in cancer : a systematic review with meta - analysis . 
shen z , zhou s , wang y , et al : higher intratumoral infiltrated foxp3 + treg numbers and foxp3 + / cd8 + ratio are associated with adverse prognosis in resectable gastric cancer . 
yoon c , cho sj , aksoy ba , et al : chemotherapy resistance in diffuse - type gastric adenocarcinoma is mediated by rhoa activation in cancer stem - like cells . 
ryu hs , park dj , kim hh , et al : combination of epithelial - mesenchymal transition and cancer stem cell - like phenotypes has independent prognostic value in gastric cancer . 
takaishi s , okumura t , tu s , et al : identification of gastric cancer stem cells using the cell surface marker cd44 . stem cells 27 : 1006 - 1020 , 2009 27 . 
martin , md1 introduction we read with interest two recently published articles in jco precision oncology that provide valuable insight regarding stk11 , an emerging biomarker in nonsmall - cell lung cancer ( nsclc ) .1 , 2 initially , shen et al1 detailed their ndings with the statistical learning tool oncocast . 
they identied stk11 as one of several prognostic genes afliated with poor survival from 1 , 054 patients with advanced lung adenocarcinoma proled with msk - impact next - generation sequencing ( ngs )  . 
by dividing the cohort into genomic risk - stratication groups , the authors highlighted the complexity of stk11 co - mutation patterns with other high - risk genes , including keap1 , kras , tp53 , and smarca4 . 
in the article by bange et al , 2 the authors retrospectively demonstrated heterogeneity of outcomes among patients with stk11 - mutated , advanced nsclc on the basis of co - mutation status . they reported that kras co - mutated cases had worse progression - free and overall survival outcomes after rst - line chemotherapy compared with tp53 . taken together , these ndings and others3 - 5 indicate that further work is warranted to characterize stk11 as an nsclc biomarker and to identify unique therapeutic approaches for patients with high - risk stk11mutated nsclc . 
a lumpectomy was performed in april 2014 , and adjuvant treatment included 12 doses of weekly paclitaxel , 1 year of trastuzumab , a partial breast radiation , and continuation on letrozole . 
a biopsy showed lung adenocarcinoma , and positron emission tomography ( pet ) / ct showed no additional disease . she received a robotic lobectomy , and pathologic staging revealed iiia disease . 
postoperative pet / ct in august showed a mildly hypermetabolic 1 - cm focus in the right middle lobe of the lung without other disease ; magnetic resonance imaging of the brain was negative . after radiologic review , it was initially believed that this focus represented postsurgical hypermetabolism , and close follow - up was recommended . 
she received adjuvant cisplatin and pemetrexed on day 1 of 21 - day cycles ; ct scans in october , after two of four cycles , showed no new disease . 
pet / ct revealed hypermetabolic disease limited to the 4 - cm adrenal mass . the adrenal and right middle - lobe lung lesions were biopsied , and both conrmed lung adenocarcinoma . she was referred for surgical evaluation but was not a candidate . 
testing included immunohistochemistry ( ihc ) , tumor mutational burden ( tmb ) , and 592 - gene ngs including egfr , braf , met , and her2 , as well as the previously mentioned high - risk genes stk11 , keap1 , kras , and tp53 ( nextseq ; illumina [ san diego , ca ] ) .6 ros1 and alk fusions were detected using the archerdx fusion assay ( archer fusionplex solid tumor kit )  . 
proling showed no targetable mutations , programmed death - ligand 1 ( pd - l1 ) ihc expression 0% ( 22c3 ; dako [ santa clara , ca ] ) , and tmb 15 mutations / megabase . 
no keap1 or tp53 mutations were identied . intravenous nivolumab 3 mg every 2 weeks and 1 mg / kg ipilimumab every 6 weeks were initiated in june 2018 . both treatments were withheld in july when the patient developed symptomatic autoimmune hyperthyroidism that necessitated treatment with methimazole and atenolol . 
nivolumab was resumed in august with symptom resolution , when ct scans showed a small increase in size of her adrenal metastasis with reduction of the right middle - lobe lesion . 
 nivolumab / ipilimumab in stk11 - mutated nonsmall - cell lung cancer by bange et al.2 although characterized by caris life sciences as a pathogenic mutation , we recognize that explicit pathogenicity of r39fs cannot be conrmed by commercial ngs alone . 
however , it should be noted that several studies have shown that frameshift variants ( including those of exon 1 ) generally express little stk11 protein by ihc , which serves as a reliable marker for loss of stk11.15 , 16 we recognize the complexity of dening high - risk stk11 molecular subsets from commercial ngs . 
martin consulting or advisory role : seattle genetics no other potential conicts of interest were reported . references shen r , martin a , ni a , et al : harnessing clinical sequencing data for survival stratication of patients with metastatic lung adenocarcinomas . 
cancer discov 8 : 822 - 835 , 2018 arbour kc , jordan e , kim hr , et al : effects of co - occurring genomic alterations on outcomes in patients with kras - mutant non - small cell lung cancer . 
clin cancer res 24 : 334 - 340 , 2018 skoulidis f , arbour kc , hellmann md , et al : association of stk11 / lkb1 genomic alterations with lack of benet from the addition of pembrolizumab to platinum doublet chemotherapy in non - squamous non - small cell lung cancer . 
vanderwalde a , spetzler d , xiao n , et al : microsatellite instability status determined by next - generation sequencing and compared with pd - l1 and tumor mutational burden in 11 , 348 patients . 
cancer med 7 : 746 - 756 , 2018 rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
nat rev drug discov 18 : 197 - 218 , 2019 ready n , hellmann md , awad mm , et al : first - line nivolumab plus ipilimumab in advanced non - small - cell lung cancer ( checkmate 568 ) : outcomes by programmed death ligand 1 and tumor mutational burden as biomarkers . 
frank r , schefer m , merkelbach - bruse s , et al : clinical and pathological characteristics of keap1and nfe2l2 - mutated non - small cell lung carcinoma 13 . 
p ecuchet n , laurent - puig p , mansuet - lupo a , et al : different prognostic impact of stk11 mutations in non - squamous non - small - cell lung cancer . 
 o orthogonal comparison of four plasma ngs tests with tumor suggests technical factors are a major source of assay discordance daniel stetson , ms1 ; ambar ahmed , ms1 ; xing xu , phd2 ; barrett r.b. 
2019 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction increased reliance on liquid biopsy specimens for oncologic clinical decisions emphasizes the critical need for sensitive , specic multigene tests to detect genetic aberrations . 
plasma - based genotyping tests are approved for clinical use by the us food and drug administration but are limited to recurrent hot spot mutations or specic genes such as egfr and kras.1 next - generation sequencing ( ngs ) gene panel assays , in contrast , analyze thousands to millions of contiguous base pairstens to hundreds of genes for somatic alterations at low variant allele frequency ( vaf )  . 
the food and drug administration has approved the oncomine ( thermo fisher scientic , waltham , ma ) , 2 memorial sloan ketteringintegrated mutation proling of actionable cancer targets , 3 and foundationone ( foundation medicine [ fmi ] , cambridge , ma ) 4 gene panels . 
the need for noninvasive testing of a patients current mutational status , 5 coupled with the increased throughput6 and sensitivity7 of ngs , has led to the commercialization of circulating tumor dna ( ctdna ) ngs services . studies have examined the correlation between tumor and plasma mutational proling . 
in the context of egfr testing , thress et al8 used orthogonal genotyping methods to show that acquired resistance variants detected in plasma , but not in tumor , were reproduced by different plasma genotyping plattumor heterogeneity alone forms , suggesting that may explain tissue - plasma discordance for these hotspot assays . 
for broader gene - panel mutation detection in plasma by ngs , kuderer et al9 compared actionable variants found with plasma testing versus tumor testing and found only 22% variant concordance ( 10 of 45 variants )  . 
 stetson et al to address questions regarding sources of ctdna assay discordance , baseline plasma samples from 24 patients were sent to four ctdna sequencing vendors , and reported variants were compared with independently tested , timematched , tumor - normal tissue pairs . 
we supplied challenging samples with limited ctdna from early - stage cancers , which tested the limits of sensitivity and positive predictive value ( ppv ) but may have resulted in higher than expected failure and discrepancy rates . 
the aim of this study was to improve performance of ctdna ngs assays and inform physicians of clinical use . their potential limitations methods samples twenty - four matched , tumor - normal pairs with matched plasma from lung , breast , ovary , and prostate cancers ( table 1 ) were obtained from three commercial biobanking companies . 
plasma was collected 1 to 4 hours before patient surgery or drug treatment via double - spun edta tubes . tumor ngs assays matched tumor - normal tissue samples were sent to fmi as formalin - xed parafn - embedded blocks or genomic dna puried from frozen tissues ( 400 ng )  . 
variant calls and raw data for the matched tumor - normal pairs were returned to astrazeneca and , after matched normal single - nucleotide polymorphisms ( snps ) from tumor calls were subtracted , were used as a presumed somatic truth set for comparison with plasma results . plasma ngs assays plasma samples for each patient ( 8 ml ) were thawed , mixed , pooled , and dispensed into four 2 - ml aliquots . 
general results were discussed with each vendor to better understand laboratory methodologies and reporting criteria . sample identity verication to conrm that all returned sample data traced back to the correct patient , sample identity was veried by germline snp clustering analysis from tumor , normal , and plasma samples . 
a comprehensive set of snps was dened by intersecting all vendor bed les , then the corresponding snps were used to generate phylogenetic clusters between tissue and plasma for each vendor . 
these analyses , using the open source clearup algorithm13 ( astrazeneca - ngs / clearup ) , conrmed that the plasma samples were properly handled and matched by all vendors , except for eight samples incorrectly identied by vendor a . 
the identity matching and the pattern of the four discordant samples ( ie , samples were transposed ) suggest that vendor a mislabeled the samples , possibly during the preanalytical laboratory process , because the mismatch was found in both the gender quality - control check and subsequent sequencing . two blocks of the rst comparative tumor and plasma variant analyses the four variant reports were used for all orthogonal comparisons among assays without additional modications . 
non - shedders were patients with no evidence of tumor - plasma or plasma - plasma concordant variants . was not reported by vendor c despite its presence in that vendors raw data , possibly because of a bioinformatic ltering of suspected germline variants . 
tp53 v143m ( fig 2c ) was missed owing to elevated background noise in the vendor a assay , but it was clearly present and reported by vendor c . results variant - level concordance all reported plasma variants were plotted according to mutant vaf ( fig 1 ) and vendor ( data supplement )  . 
higher - frequency plasma variants ( approximately 50% vaf ) were veried as germline by comparison with the tumor - normal sequencing data . germline snps were reported as variants by all except vendor c , but these snps were excluded from any concordance calculations . 
overall , vendor c had the highest sensitivity ( 89% ) and vendor b had the highest ppv ( 80% )  . vendor d had a ppv of 36% owing to the high level of fps ( table 2 )  . 
above a vaf of 1% , vendors a , b , and c had a ppv of 100% ; below 1% vaf , vendor a had the lowest values for sensitivity ( 10% ) and ppv ( 17% )  . analysis of fps fps were identied by examining the raw alignment data from the replicate plasmas relative to tumor and normal samples and resulted from nonspecic variant calling and sequencing noise at nonreference bases . 
examples of nonspecic variant calls include fp brca2 l1103f ( fig 3a ) and erbb2 splice acceptor ( fig 3b ) calls not present in vendor cs data . fp signatures the 40 fp calls identied in this study ( table 2 ) were enriched for vendor - specic mutational biases ( data supplement )  . 
most fp calls were novel variants not found in somatic variant databases ( data supplement ) ; 100% of fp variants reported by vendor a , 100% by vendor c , and 95% by vendor d were novel . analysis of fns patient - level concordance to understand the nature of fn variant calls , raw aligned data were examined for tumor , normal , and plasma samples . 
the pik3ca h1047r variant was called by vendor c but missed by vendor b ( fig 2a ) ; it was present in vendor bs raw data but not reported . 
the variant demonstrated high signal - to - noise ratio and similar numbers of reads ( ve for vendor c and four for vendor b ) but was apparently below vendor bs bioinformatic calling threshold . 
concordant true - positive variants ( light blue ) and discordant variants , both false positive ( red ) and false negative ( teal ) , are plotted by the log of the allele fraction ( af )  . 
af is approximated for false - negative calls by averaging the corresponding true - positive calls for that variant . 4 2019 by american society of clinical oncology the patient level we examined variant concordance at ( fig 4 )  . 
five of the 24 patients were tissue - plasma concordant , three were plasma - plasma concordant , two were partially concordant , and 14 had non - shedding tumors ( fig 4 ; table 1 )  . 
the lack of detectable concordant variants in non - shedding plasma samples was consistent with derivation from early - stage cancers ( stage i , n = 8 ; stage ii , n = 13 ; stage iii , n = 2 ; and stage iv , n = 1 ; table 1 )  . detailed analysis of two patients samples the replicate design of this study offered the opportunity to gain more insight into the variant discordance factors by comparing the results generated by four vendors . 
vendor c found all three variants ; vendor b found both the pik3ca and tp53 variants , and the tert variant was not covered by this vendors panel ; vendors a and d missed the pik3ca and tert variants because of elevated background noise ; and vendor d found the tp53 v173l variant also reported by vendor a but assigned it to the wrong patient . 
some ctdna assays claim sensitivity to 0.1% vaf ; however , it is apparent that increasing proportions of fp and fn were apparent in our study and other studies9 , 16 at vaf of less than 1% . 
inspection of the raw sequencing data revealed elevated background noise to be an issue for vendors a and d , whereas vendors b and c had little to no background noise . 
vendors were individually informed about discordant results and , in several cases , they adjusted their variant pipelines , which modestly improved reports ( data not shown )  . cluster analyses of germline snps conrmed that returned ngs datasets corresponded with the correct patients of origin except for eight discrepant samples processed by vendor a . 
the corrected results increased vendor as ppv from 55% to 73% and sensitivity from 38% to 44% ; however , we presented only the returned reports because no other laboratory mixed up samples . 
mixing up patient results during the testing process is a serious issue to be addressed by improved quality control and other best practices . of the 24 patients , 14 ( 58% ) were classied as having nonshedding tumors , because they lacked detected concordant variants matching tumor or a replicate plasma . 
this proportion is higher than the published 20% to 30% rate of non - shedding samples , 16 , 17 likely because 88% ( 21 of 24 ) of patients in our study had stage i and ii tumors ( table 1 )  . stage i and ii tumors generally shed less dna into the bloodstream than more advanced and metastatic tumors16 , 18 ; however , there is variability in sample vafs ( fig 1 )  . 
furthermore , 50% ( 22 of 44 ) of all tp somatic variants had a vaf of less than 1% , underscoring the importance of analytically validated assays with sensitivity below 1% vaf . the set of plasma samples analyzed allowed ctdna ngs methods to be evaluated under challenging conditions such as limited ctdna levels ( sensitivity ) and non - shedding tumors ( ppv ) ; however , the approach may have resulted in a higher - than - expected discrepancy rate . 
according to our results and those of others , 16 application of ctdna assays to early detection analyses may be confounded by fn and fp rates . most discordance was due to assay technical variation , but biologic factors such as clonal hematopoiesis of determinate potential ( chip ) 19 and tumor heterogeneity were responsible for some discordance . 
all vendors were concordant for the tp53 and cdkn2a variants ( fig 4 ) , but vendor c had an fn call ( fig 2b ) for brca2 and vendor a had an fn call for pdgfra . 
this likely represents tumor heterogeneity , because the esr1 variant was not detected in the tumor and , if so , would have been present at approximately 0.3% vaf , well below the detection limit of the tissue assay . discussion many studies have compared ctdna results and tumor analysis , nding substantial discordance that affects which assay to use for patient management . 
by our novel replicate plasma design , we compared sequencing data from four commercial plasma tests with one another and with tumor ndings and determined that technical factors are a major source of variation . 
furthermore , we propose insights for identifying fp variants . to our knowledge , this is the rst study to use replicate tumor - matched plasmas and multiple orthogonal assays to examine the factors affecting tumor - plasma concordance . it is important to note that this design enabled the identication of variants missed when comparing one plasma assay with a tumor9 or another plasma15 assay . 
the replicate plasmas were essential for identifying fn calls and increased the condence of tp calls , particularly for variants found in plasma but not tumor . sensitivity and ppv varied among vendors and was lower for all below 1% vaf . 
although our study demonstrated that the majority of tumor - plasma discordance is a result of technical factors , with continuous improvement over time , ngs should approach the state of genotyping technology in which the majority of discordance is attributable to biologic factors such as tumor heterogeneity and chip.19 all vendor assays performed well above 10% vaf ( none or one discordant results per vendor ) , but below 1% vaf , most variant calls were discordant . 
we determined that lowvaf calls ( fig 1 ) , mutational biases ( data supplement ) , and novel somatic variants ( data supplement ) were the main characteristics of discordant calls . 
in our study , half of tps , and most fn and fp calls , were found below 1% vaf , demonstrating the need for improved assay performance below this threshold . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . daniel stetson employment : astrazeneca stock and other ownership interests : astrazeneca ambar ahmed employment : astrazeneca stock and other ownership interests : astrazeneca xing xu employment : solvebio stock and other ownership interests : solvebio stock options ( inst ) ; gilead sciences , merck ( i ) , celgene ( i ) , bausch health ( i ) barrett r.b. 
dougherty employment : astrazeneca stock and other ownership interests : astrazeneca ( inst ) no other potential conicts of interest were reported . acknowledgment we thank david gross , david caplan , and jeff hull from solvebio for informatics assistance and technical discussions , as well as hilary north scheler from axon communications for providing medical writing assistance funded by astrazeneca . references id = p160045 2017 2016 roche molecular systems : cobas egfr mutation test v2 ( 2015 )  . 
nat rev cancer 17 : 223 - 238 , leary rj , kinde i , diehl f , et al : development of personalized tumor biomarkers using massively parallel sequencing . 
nat med 20 : 548 - 554 , 2014 thress ks , brant r , carr th , et al : egfr mutation detection in ctdna from nsclc patient plasma : a cross - platform comparison of leading technologies to support the clinical development of azd9291 . 
lung cancer 90 : 509 - 515 , 2015 kuderer nm , burton ka , blau s , et al : comparison of 2 commercially available next - generation sequencing platforms in oncology . 
jama oncol 3 : 996 - 998 , 2017 jovelet c , ileana e , le deley mc , et al : circulating cell - free tumor dna analysis of 50 genes by next - generation sequencing in the prospective moscato trial . clin cancer res 22 : 2960 - 2968 , 2016 11 . 
 exceptional response to cabozantinib in a patient with multiply relapsed wilms tumor introduction wilms tumors ( wts ) account for a majority of pediatric renal tumors and have a high cure rate with surgery , radiation , and chemotherapy.1 high - risk features in wts include anaplastic histology , blastemal predominance , bilateral presentation , and loss of heterozygosity of 1p and 16q , and patients who have these features typically have worse outcomes and are treated with more aggressive therapies . 
despite the risk - stratified approach to therapy , outcomes remain poor for the subgroup of patients with wts who relapse.2 better understanding of the biology of wt could help identify risk factors associated with disease relapse . 
 in november 2005 , 3.5 years after completion of therapy , the patient experienced a widespread relapse that was detected on routine surveillance and was treated with cyclophosphamide , etoposide , carboplatin , vincristine , and radiation . two years after therapy for the relapse , a second recurrence was detected on imaging ; he underwent surgical resection and received treatment consisting of ifosfamide / etoposide , cyclophosphamide / topotecan , and autologous stem cell transplantation . 
the patients stem cell transplantation was complicated by severe bk viral hemorrhagic cystitis infection , which necessitated a prolonged stay in the intensive care unit . in october 2010 , 2 years after transplantation , the patient began experiencing back pain and was found to have a third relapse , which was treated with vincristine , adriamycin , and irinotecan . 
approximately 1 year after this therapy was completed , a fourth relapse was treated with eight cycles of sorafenib , which led to stable disease , after which disease progression was detected and the patient began radiation therapy . 
in july 2013 , the patient was then treated with cabozantinib , and he experienced a partial response lasting close to 2 years ( fig 1 )  . after his eventual progression on cabozantinib , the patient advanced through several other therapies , including additional radiation , lorvotuzumab mertansine , axitinib , ramucirumab , and pazopanib . 
mody author affiliations and support information ( if applicable ) appear at the end of this article . none of the sponsors played a role in the design of the study ; collection , management , analysis , and interpretation of the data ; preparation , review , or approval of the manuscript ; or decision to submit the manuscript for publication . 
 the patient experienced a 33% reduction in combined target lesion tumor size by response evaluation criteria in solid tumors ( recist )  . mycn mutations are monoallelic events with no evidence of loss of heterozygosity in the tumor . 
 in addition , transcriptome sequencing ( rna sequencing ) uncovered various overexpressed tyrosine kinases ( ret , met , and tek / tie2 ) when compared with the rest of our institutions compendium of patients with wt ( table 1 )  . 
a review of the family history showed that the mother was positive for melanoma ( age of onset , 37 years ) , and the paternal grandfather had basal cell cancer ( age of onset , 64 years )  . discussion prognosis for relapsed wt continues to be poor in spite of high - dose intensive therapy . 
genetic aberrations discovered through ics can help identify new prognostic markers , can help researchers better understand tumor biology , and can sometimes lead to targeted therapies.3 somatic mutations in max ( p.r60q ) and mycn ( p.p44l ) were identified in our multiply relapsed patient with unquestionably refractory disease . 
the myc proto - oncogene has been implicated in the pathogenesis of many human tumors and was found to be overexpressed and / or activated in more than half of human cancers.7 , 8 myc coordinates changes in the tumor microenvironment , including the activation of angiogenesis.9 in patients with wt , mycn is associated with the high - risk histology features of anaplasia and blastemal predominance as well as poorer relapse - free survival and overall survival . 
this suggests the potential for a poor prognostic implication of combined max and mycn mutations in this case , but further functional studies are required to validate this interaction . cabozantinib is an oral small molecule inhibitor of numerous tyrosine kinase receptors with activity toward vegfr2 ( kdr ) and met ( hepatocyte growth factor receptor )  . 
it also targets important mediators of tumor cell survival , metastasis , and tumor angiogenesis , including ret ( rearranged during transfection ) , kit ( mast / stem cell growth factor receptor ) , axl ( anexelekto ) , tie2 ( angiopoietin receptor ) , and flt3 ( fms - like tyrosine kinase ) .4 , 14 cabozantinib has been approved by the us food and drug administration to treat advanced renal cell carcinoma ( arcc ) and has shown efficacy against medullary thyroid cancer.15 sorafenib targets many of the same kinases as cabozantinib and also targets craf , braf , vegfr3 ( flt4 ) , and pdgfr - .16 because of the patients exceptional response to cabozantinib , prolonged stable disease while receiving sorafenib , and seemingly no genetic mutations or amplifications that could be targeted , we looked at the expression of various kinases that are inhibited by both agents using rna sequencing ( table 1 )  . 
it is known that ret plays a role in the development of the kidney , and expression of high levels of ret in wt has been reported ; therefore , this overexpression may play a role in the development of the disease.17 in addition , the patients tumor was likely highly vascularized as a result of his somatic mycn mutation.9 we hypothesize that inhibition of the vegf signaling pathway enacted by both sorafenib and cabozantinib helps devascularize the tumor , leading to sustained response . 
 previous research in arcc substantiates our experience , which shows cabozantinib to be superior to other multi - tkis such as sorafenib and axitinib , leading to longer progression - free survival.18 further evidence in arcc suggests that increased expression of met and axl are associated with a poor prognosis and that their inhibition may help overcome resistance to vegf pathway inhibition.19 , 20 the rare hoxb13 germ line variant uncovered in this patient has been inconsistently reported to increase cancer risk . 
 with tumor angiogenesis and disease progression.21 there are no reported cases of this germ line mutation in wt , but it seems to be associated with an increased risk of prostate cancer , particularly in whites.22 , 23 thus , this finding led to genetic counseling for the patient and his family . to our knowledge , this is the first report of a patient with wt who had aberrations in both max and mycn genes ; in fact , if the myc / max interaction plays a significant prognostic role in wt , agents are being developed that could potentially target this interaction.24 generally , overexpression is not considered a targetable finding in precision oncology , but if there are no other tangible aberrations , targeting overexpression may be reasonable . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . rama jasty - rao no relationship to disclose yi - mi wu no relationship to disclose trisha paul no relationship to disclose dan robinson no relationship to disclose rajen j . 
grundy p , breslow n , green dm , et al : prognostic factors for children with recurrent wilms tumor : results from the second and third national wilms tumor study . 
yakes fm , chen j , tan j , et al : cabozantinib ( xl184 ) , a novel met and vegfr2 inhibitor , simultaneously suppresses metastasis , angiogenesis , and tumor growth . 
wilhelm sm , carter c , tang l , et al : bay 43 - 9006 exhibits broad spectrum oral antitumor activity and targets the raf / mek / erk pathway and receptor tyrosine kinases involved in tumor progression and angiogenesis . 
wegert j , ishaque n , vardapour r , et al : mutations in the six1 / 2 pathway and the drosha / dgcr8 mirna microprocessor complex underlie high - risk blastemal type wilms tumors . 
dela cruz fs , diolaiti d , turk at , et al : a case study of an integrative genomic and experimental therapeutic approach for rare tumors : identification of vulnerabilities in a pediatric poorly differentiated carcinoma . 
kim a , widemann bc , krailo m , et al : phase 2 trial of sorafenib in children and young adults with refractory solid tumors : a report from the childrens oncology group . 
amzal b , fu s , meng j , et al : cabozantinib versus everolimus , nivolumab , axitinib , sorafenib and best supportive care : a network meta - analysis of progression - free survival and overall survival in second line treatment of advanced renal cell carcinoma . 
choueiri tk , escudier b , powles t , et al : cabozantinib versus everolimus in advanced renal cell carcinoma ( meteor ) : final results from a randomised , open - label , phase 3 trial . 
zhu jy , sun qk , wang w , et al : high - level expression of hoxb13 is closely associated with tumor angiogenesis and poor prognosis of hepatocellular carcinoma . 
cai q , wang x , li x , et al : germline hoxb13 p.gly84glu mutation and cancer susceptibility : a pooled analysis of 25 epidemiological studies with 145 , 257 participants . 
 circulating tumor dna analysis in colorectal cancer : from dream to reality carlotta antoniotti , md1 , 2 ; filippo pietrantonio , md3 , 4 ; salvatore corallo , md3 ; filippo de braud , md3 , 4 ; alfredo falcone , md1 , 2 ; and chiara cremolini , md , phd1 , 2 liquid biopsy is a minimally invasive approach to obtain circulating materials that originate from tumor cells through the sampling of body uids , mainly peripheral blood . 
because of its abilities to detect tumor - derived nucleic acids and proteins and to characterize tumor - specic genomic abnormalities , liquid biopsy has emerged as an approach to orient care of patients with colorectal cancer ( crc )  . 
second , the reliability of studies that evaluate the concordance of ras testing between tissue and plasma samples is impaired by the adoption of assays with heterogeneous analytical sensitivity and coverage of genomic regions . 
there are now several commercially available methods for ctdna assessment and technology platforms based on digital polymerase chain reaction or next - generation sequencing approacheseach one with specic sensitivity , specicity , throughput , gene coverage , costs , and potential clinical applications.12 among them , three test kits are ce - marked in vitro diagnostic devices for detection of ras and braf mutations on ctdna in crc.13 - 16 third , some clinicopathologic variables are likely to affect the amount of tumor - released ctdna.5 , 6 , 8 , 10 , 11 whereas liver involvement and tumor burden are positively associated with the ras mutant allele fraction ( the proportion of mutant dna fragments at a given locus ) , peritoneal , nodal , and lung metastases and mucinous histology are linked to low ras inuence ctdna ctdna detection . 
 antoniotti et al ras wild - type cases , as assessed on ctdna , negligible . is not the parallel assessment of the mutant allele fractions of other key genomic tumor alterations may help solve challenging cases that have undetectable ras mutations and ctdna levels at or lower than the analytic sensitivity of adopted assays . 
to overcome these issues , preanalytic procedures should be standardized , a threshold of detectable mutation rate that confers intrinsic resistance to egfr inhibition should be set and prospectively validated , investigation to understand when plasma and additional and tissue tests are interchangeable and to improve assay sensitivities is warranted . meanwhile , the ras status assessment to address the use of anti - egfr agents must be performed as the gold standard on tumor specimens.3 , 4 , 17 , 18 only when tissuebased testing is technically or logistically unfeasible could it be replaced by ctdna analysis.4 ctdna to estimate prognosis and detect minimal residual disease retrospective studies have focused on the prognostic impact of the quantitative analysis of ctdna . 
in the metastatic setting , a correlation between ctdna concentration and survival has been described , but the independent weight of ctdna quantication when the relative impact of other well - known prognostic factors is taken into account has not been claried ( appendix table a2 )  . the role of the quantitative assessment of ctdna in monitoring response during treatment must be dened in the light of its potential added value when compared with easily available and well - established markers , including carcinoembryonic antigen or early radiologic disease reassessment . 
recently , ctdna has been proposed to detect , measure , and monitor residual disease after radical interventions . a series of proof - of - concept studies reported that liquid biopsy could disclose the persistence of minimal residual disease ( mrd ) through the detection of ctdna in patients with crc who underwent potentially curative surgery ( resection of primary tumor in early - stage crc or radical resection of metastases ) even in the absence of clinical or radiologic signs of residual disease ( appendix table a2 )  . by identifying incomplete eradication of disease after a curative treatment , detectable ctdna predicts an increased risk of relapse regardless of the exposure to an adjuvant treatment . 
the development of such a sensitive tool might improve the risk estimation of disease relapse after a curative intervention to properly stratify clinical trials in early - stage crc and to accordingly drive the therapeutic management . theoretically , two applications of the detection of mrd in this setting may be foreseen : to offer chemotherapy to all postoperative ctdna - positive patients , including those with no histopathologic risk factors to reduce their risk of progressionindeed , ctdna positivity invariably means residual diseaseand to avoid useless adjuvant therapies in postoperative ctdna - negative patients . 
in early - stage crc , ctdna is detected at a lower rate than in the advanced disease.1 therefore , highly sensitive techniques are needed to achieve appropriate accuracy to detect mrd . most available data have been achieved through a twothe identication of specic somatic step procedure : abnormalities in tissue samples , followed by the search for the same alteration in ctdna . 
only trials that aim to optimize the treatment of all postoperative ctdna - positive patients , independent of traditional histopathologic factors , are ethically acceptable . ctdna to track tumor response and resistance to therapy whereas tissue biopsies catch single snapshots of the tumor in a specic spatiotemporal fragment , liquid biopsy may more comprehensively depict the intrinsic and dynamic intratumoral heterogeneity . 
the heterogeneity and dynamism of the tumor clonal evolution under the pressure of targeted treatments are conrmed by the emergence of multiple alterations in the mitogenactivated protein kinase pathway effectors , including ras and mek mutations and kras , brafv600e , and met amplication , during the treatment with braf / egfr , braf / mek and braf / egfr / mek inhibitors in patients with brafv600e - mutant mcrc.23 - 27 two novel ntrk1 mutations have been detected as a potential mechanism of acquired resistance to entrectinib , a tyrosine kinase receptor inhibitor , in a patient with lmna - ntrk1rearranged mcrc.34 nevertheless , some steps should be covered to translate liquid biopsy from the investigational setting into clinical practice . available data indicate that the frequency of molecular alterations in ctdna at the time of disease progression is inconsistent among different series , even when the same methods for plasma ctdna analysis is applied ( table 1 )  . this inconsistency impairs the reliability of adopted techniques and the reproducibility of the ndings . 
setting and validation of a quantitative threshold to dene the clinical relevance of each detectable molecular alteration as clearly associated with a lack of benet from ongoing therapies may be relevant to biologically guide therapeutic decisions . currently , no prospective data are available about usefulness of discontinuing ongoing therapy and initiation of a tailored treatment when signals of acquired resistance emerge in ctdna before clinical or imaging - based disease progression is noted . the co - occurrence of multiple and / or subclonal molecular alterations at the time of acquired resistance highlights an increase in tumor heterogeneity , which complicates the denition of clinical value of each identied alteration as therapeutic target for subsequent tailored strategies . 
in other words , how to therapeutically target the heterogeneous mechanisms of resistance and the subclonal patterns of tumor cell populations that emerge upon drug selection is today still challenging . 
in this proof - ofconcept study , patients who are candidates for anti - egfr rechallenge are eligible only if a notable decrease in ras fractional mutational abundance occurs from the time of disease progression after a rst - line anti - egfrcontaining therapy to the time of rechallenge . liquid biopsy has emerged as a minimally invasive tool to genotype tumors , to assess patient prognosis and detect mrd , to monitor treatment efcacy , and to track the dynamism of clonal evolution over time and therapies . 
sci transl med 6 : 224ra24 , 2014 denis ja , guillerm e , coulet f , et al : the role of beaming and digital pcr for multiplexed analysis in molecular oncology in the era of next - generation sequencing . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
j clin oncol 36 : 1631 - 1641 , 2018 baraniskin a , van laethem jl , wyrwicz l , et al : clinical relevance of molecular diagnostics in gastrointestinal ( gi ) cancer : european society of digestive oncology ( esdo ) expert discussion and recommendations from the 17th european society for medical oncology ( esmo ) / world congress on gastrointestinal cancer , barcelona . 
ann oncol 29 : 1211 - 1219 , 2018 siravegna g , mussolin b , buscarino m , et al : clonal evolution and resistance to egfr blockade in the blood of colorectal cancer patients . 
nat med 21 : 795 - 801 , 2015 schmiegel w , scott rj , dooley s , et al : blood - based detection of ras mutations to guide anti - egfr therapy in colorectal cancer patients : concordance of results from circulating tumor dna and tissue - based ras testing . 
mol oncol 11 : 208 - 219 , 2017 jones fs , edelstein d , wichner k , et al : performance of standardized beaming platform for detecting ras mutations in the blood of metastatic colorectal cancer ( mcrc ) patients . 
grasselli j , elez e , carat `u g , et al : concordance of bloodand tumor - based detection of ras mutations to guide anti - egfr therapy in metastatic colorectal cancer . 
normanno n , esposito abate r , lambiase m , et al : ras testing of liquid biopsy correlates with the outcome of metastatic colorectal cancer patients treated with rst - line folfiri plus cetuximab in the capri - goim trial . 
sepulveda ar , hamilton sr , allegra cj , et al : molecular biomarkers for the evaluation of colorectal cancer : guideline from the american society for clinical pathology , college of american pathologists , association for molecular pathology , and the american society of clinical oncology . 
khan kh , cunningham d , werner b , et al : longitudinal liquid biopsy and mathematical modeling of clonal evolution forecast time to treatment failure in the prospect - c phase ii colorectal cancer clinical trial . 
pietrantonio f , oddo d , gloghini a , et al : met - driven resistance to dual egfr and braf blockade may be overcome by switching from egfr to met inhibition in braf - mutated colorectal cancer . 
misale s , di nicolantonio f , sartore - bianchi a , et al : resistance to anti - egfr therapy in colorectal cancer : from heterogeneity to convergent evolution . 
montagut c , dalmases a , bellosillo b , et al : identication of a mutation in the extracellular domain of the epidermal growth factor receptor conferring cetuximab resistance in colorectal cancer . 
misale s , arena s , lamba s , et al : blockade of egfr and mek intercepatients heterogeneous mechanisms of acquired resistance to anti - egfr therapies in 37 . 
newhall k , price t , peeters m , et al : frequency of s492r mutations in the epidermal growth factor receptor : analysis of plasma dna from metastatic colorectal cancer patients treated with panitumumab or cetuximab monotherapy . 
raghav k , morris v , tang c , et al : met amplication in metastatic colorectal cancer : an acquired response to egfr inhibition , not a de novo phenomenon . oncotarget 7 : 54627 - 54631 , 2016 41 . 
siena s , sartore - bianchi a , garcia - carbonero r , et al : dynamic molecular analysis and clinical correlates of tumor evolution within a phase ii trial of panitumumab - based therapy in metastatic colorectal cancer . 
takegawa n , yonesaka k , sakai k , et al : her2 genomic amplication in circulating tumor dna from patients with cetuximab - resistant colorectal cancer . oncotarget 7 : 3453 - 3460 , 2016 45 . 
tsuji y , shitara k , yamanaka t , et al : reverce : randomized phase ii study of regorafenib followed by cetuximab versus the reverse sequence for metastatic colorectal cancer patients previously treated with uoropyrimidine , oxaliplatin , and irinotecanbiomarker analysis . 
montagut c , argil es g , ciardiello f , et al : efcacy of sym004 in patients with metastatic colorectal cancer with acquired resistance to anti - egfr therapy and molecularly selected by circulating tumor dna analyses : a phase 2 randomized clinical trial . 
santini d , vincenzi b , addeo r , et al : cetuximab rechallenge in metastatic colorectal cancer patients : how to come away from acquired resistance ? ann oncol 23 : 4602 - 4616 , 2017 23 : 2313 - 2318 , 2012 49 . 
parseghian cm , loree jm , morris vk , et al : anti - egfr resistant clones decay exponentially after progression : implications for anti - egfr re - challenge . 
cremolini c , rossini d , dellaquila e , et al : rechallenge for patients with ras and braf wild - type metastatic colorectal cancer with acquired resistance to rstline cetuximab and irinotecan : a phase 2 single - arm clinical trial . 
bauer , md4 ; young kwang chae , md , mph , mba5 ; gary sherrill , md6 ; paul fanta , md , ms7 ; axel grothey , md8 ; andrew hendifar , md , mph9 ; david henry , md10 ; daruka mahadevan , md , phd11 ; mohammad amin nezami , md12 ; benjamin tan , md13 ; zev a . 
wainberg , md14 ; richard lanman , md2 ; scott kopetz , md , phd1 ; and van morris , md1 purpose gene fusions are established oncogenic drivers and emerging therapeutic targets in advanced colorectal cancer . 
this study aimed to detail the frequencies and clinicopathological features of gene fusions in colorectal cancer using a circulating tumor dna assay . methods circulating tumor dna samples in patients with advanced colorectal cancer were analyzed at 4 , 581 unique time points using a validated plasma - based multigene assay that includes assessment of fusions in fgfr2 , fgfr3 , ret , alk , ntrk1 , and ros1 . 
relative frequencies of genomic alterations were compared between fusion - present and fusion - absent cases using an unpaired t test . results forty - four unique fusions were identied in 40 ( 1.1% ) of the 3 , 808 patients with circulating tumor dna detected : ret ( n = 6 ; 36% of all fusions detected ) , fgfr3 ( n = 2 ; 27% ) , alk ( n = 10 , 23% ) , ntrk1 ( n = 3 ; 7% ) , ros1 ( n = 2 ; 5% ) , and fgfr2 ( n = 1 ; 2% )  . 
mutations associated with a previously reported antiepidermal growth factor receptor ( anti - egfr ) therapy resistance signature ( subclonal ras and egfr mutations ) were found with fusions in fgfr3 ( 10 of 12 patients ) , ret ( nine of 16 patients ) , and alk ( seven of 10 patients )  . 
for the 27 patients with available clinical histories , 21 ( 78% ) had egfr monoclonal antibody treatment before fusion detection . conclusion diverse and potentially actionable fusions can be detected using a circulating tumor dna assay in patients with advanced colorectal cancer . 
the 68 - gene panel included alk , ret , ros1 , and ntrk1 fusions , and the 70and 73 - gene panels also tested for fgfr2 and fgfr3 fusions ( appendix table a1 )  . 
germline variants were ltered out as previously described.27 the reportable range for single nucleotide variants ( snvs ) , indels , fusions , and amplications is greater than 0.04% per two molecules , greater than 0.02% per one molecule , greater than 0.04% per two molecules , and greater than 2.12 copies , respectively , with a greater than 99.9999% per - position analytic specicity.26 clinical information was obtained from test request forms and conrmed by pathology and medical reports and from treating clinicians when available . this research was approved by the quorum institutional review board for the generation of de - identied data sets for research . 
relative exact frequencies of genomic alterations ( point mutations , indels , and splice variants ) were compared between fusionpresent and fusion - absent cases using an unpaired t test . results occurrence of fusions in a ctdna assay the median age at time of ctdna testing was 59 years ( interquartile range , 50 - 69 years )  . 
 ( * ) indicates fusions with statistically signicant differences in prevalence between tissue and ctdna . partner , the most commonly detected fusions were the fgfr3 - tacc3 ( n = 12 ) and ncoa4 - ret ( n = 9 ) fusions ( appendix table a2 )  . 
of samples tested 3 , 808 3 , 808 3 , 808 3 , 808 abbreviation : ctdna , circulating tumor dna . of ret or ntrk fusions between ctdna and tissue assays ( fig 1c ; table 1 ) .28 genomic proling of fusion - positive patients clinicopathology history was available for a subset of patients ( table 2 ; appendix table a3 )  . 
at least some of the molecular data from tissue testing collected at the time of initial diagnosis was available for 24 of 40 ctdna fusion - positive patients , eight of whom had comprehensive ngs in which the presence of fusions was assessed . 
from the available clinical and tissue data , nine of 27 ( 33% ) were right - sided , tumors were predominantly kras wild type ( n = 23 of 24 ; 96% ) , with no concurrent nras or brafv600e mutations , and three of 22 ( 14% ) were msi - h ( table 2 ; table a3 )  . 
 9 kras overall codon 12 codon 13 codon 61 limited nos unknown nras overall codon 12 codon 13 codon 61 limited nos unknown braf v600e overall fusion overall overall loss of mlh1 / pms2 loss of pms2 clifton et al table 2 . 
cumulatively , the data suggest that a sizable proportion of the ctdna fusion - positive population may have had ras / raf mutations and / or the fusion present at levels below the limit of detection in tissue or in a subclone of the tumor tissue that was not sampled for testing . the frequency of amplications , indels , and snvs in clinically relevant cancer genes detectable using the bloodbased ngs assay were compared between fusion - positive and fusion - negative samples ( fig 2a )  . 
 actionable fusions in crc using a ctdna assay fusion not detected fusion present egfr cdk6 cdk4 fgfr1 brca1 arid1a brca2 braf pik3ca smad4 tp53 odds ratio ( 95% ci ) fig 2 . 
 ( b ) egfr , ras , and braf amplications , indels , and mutations occurring in fusion patients in circulating tumor dna ( ctdna ) and matched tissue samples . 
blank cells indicate no mutation detected ( for circulating free dna [ cfdna ] results ) or not available ( for tissue results and prior antiepidermal growth factor receptor [ egfr ] monoclonal antibody [ mab ] )  . 
mutations associated with this anti - egfr therapy resistance signature were found with fusions in fgfr3 ( 10 of 12 patients ) , ret ( nine of 16 patients ) , and alk ( seven of 10 patients ) , including two of the patients with multiple fusions ( fig 2b )  . 
furthermore , the low rvafs of cooccurring ras , egfr , and brafv600e mutations were consistent with subclonal genomic events occurring later in tumorigenesis ( appendix fig a2 )  . 
among the six patients with an anti - egfr resistance signature who had comprehensive genomic proling results available from tissue , four were wild type at the time of initial diagnosis of crc for the corresponding fusion and / or ras / raf alterations that were later detected in ctdna , consistent with these genomic events being acquired later in tumorigenesis . discussion to our knowledge , this is the largest case series describing fusion - positive cases in crc ( whether in tissue or plasma ) and demonstrates that fusions in patients with crc can be identied using a ctdna assay . 
here , fusions were detected at a prevalence of approximately 1% in patients with advanced crc , similar to fusion prevalence using orthogonal tissue - based assays in separate series of patients with crc.8 , 9 all fusions identied are potentially actionable with available targeted drugs . 
thus , this ctdna approach has the potential to allow clinicians to consider additional studies with novel therapeutic combinations for patients with metastatic crc in future trial settings . our data provide new evidence that fusions , particularly involving fgfr3 or ret , may contribute to anti - egfr therapy resistance in crc . 
on the basis of previously validated genomic signatures in this setting , we hypothesize that fusions may arise as a novel , unreported mechanism with antiegfr therapy resistance , given the clinicopathologic data and frequent co - occurrence with subclonal ras and egfr mutations in ctdna . 
the prole of concomitant egfr mutations and subclonal ras mutations mirrors prior studies that have shown associations between these mutations and post - egfr resistance.29 interestingly , prior series performed in tissue have associated fusions with ras wild - type crc tumors.9 - 12 in our series , 23 of 24 ( 96% ) of the ctdna fusionpositive patients with tissue testing available for ras mutational status were ras wild type , whereas 25 of 44 ( 57% ) of fusion - positive ctdna samples in our series had one or more ras mutations . 
we reconcile these ndings on the basis of the greater sensitivity to detect low allele frequency often not detectable with tissue - based assays . furthermore , tissue specimens are often obtained at surgical resections , before a multiple number of sequential lines of systemic therapy , and therefore before exposure to selective pressures that mediate acquisition of resistance mechanisms . 
the majority of blood samples obtained in this cohort of patients with crc came from treatment - refractory individuals seeking clinical trial options who frequently had been exposed to anti - egfr therapies . 
thus , the occurrence of subclonal resistance alterations in ctdna accounted for differences in the tumor genomic proles of advanced , typically heavily pretreated cancers , relative to the lessmutated genomic proles of the tumor taken before therapy initiation . 
 actionable fusions in crc using a ctdna assay eml4 - alk fusion strn - alk fusion fgfr2 - tacc2 fusion fgfr3 - tacc3 fusion ccdc6 - ret fusion ncoa4 - ret fusion trim24 - ret fusion plekha6 - ntrk1 fusion tpm3 - ntrk1 fusion erc1 - ros1 fusion slc34a2 - ros1 fusion anti - egfr signature - positive c other ras - positive c 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30 31 32 33 34 35 36 37 38 39 40 41 42 43 44 patient fig 3 . 
such alterations have been previously reported as acquired mechanisms of resistance to anti - egfr therapies in crc.20 , 33 collectively these and our data point to a diverse , heterogeneous landscape of potential resistance mechanisms adapted by ras wild - type crc tumors to overcome egfr blockade . fusions represent a potentially actionable therapeutic target in the anti - egfr resistance setting . 
therefore , although targeting subclonal fusions alone may be only partially successful , multipathway suppression may be a promising avenue of additional investigation , possibly in combination with antiegfr therapies . 
such strategies would need to be highly individualized , given the diversity of resistance mechanisms , and could be informed by comprehensive ctdna testing , especially because serial tissue biopsies are less feasible in patients with advanced cancer . in several previous data sets using tissue - based assays , fusions in patients with crc were associated with msi - h cancers.9 - 12 although rates of msi - h and right - sided tumors in our data set were similar to average rates reported in advanced crcs , a proportion of the fusion - positive patients in this series are suspected to have acquired the fusion after selective pressure from anti - egfr therapy , and therefore the fusion may have been present in the primary tumor at levels too low to be associated with msi - h status . 
 clifton et al this series where the fusion was tested for and detected in tissue , the tumors were found to be msi - h . one of the limitations of this data analysis is that complete clinicopathologic features were not available for all patients , given the retrospective nature of the study , and therefore we were unable to obtain clinical histories from all patients with fusions . 
however , using a previously validated method , 29 the majority of fusion - positive patients had at least one variable , which was highly predictive of prior anti - egfr exposure . 
in addition , among the patients with known treatment history and this signature , the majority were indeed conrmed to have prior anti - egfr therapy , thus internally validating the efcacy of this genomics - rst strategy to identify likely resistance cases . we also did not have matched preand post - treatment tissue and plasma for orthogonal and serial proling to conrm which fusions and other co - occurring mutations were acquired / selected for after anti - egfr therapy versus those present as truncal / clonal events . 
however , genomic events that are acquired during cancer progression tend to have lower relative vaf in ctdna than do early truncal mutations , such as those in tumor suppressor genes or clonal ras mutations.13 in our series , fusions occurring at low rvaf tended to be found in samples containing other genomic mechanisms of anti - egfr therapy resistance , which is consistent with our hypothesis that some fusions in crc occur at subclonal levels that are undetectable in pretreatment tissue but are selected for and become detectable in ctdna after anti - egfr therapy resistance . 
another limitation is that the vaf may be affected by biologic factors , such as the degree of tumor shedding , as well as technical factors , including that fusions are more difcult to detect by ngs and in ctdna samples than snvs . 
taken together , the fusion prevalences and vafs observed in this study may be lower than actual because of these technical reasons . in conclusion , actionable fusions were able to be detected at low frequencies but at similar frequencies to the historical tissue - based ngs approach in a large series of patients with crc using a ctdna assay . 
the distribution of coexisting subclonal mutations in egfr , kras , and nras in fusionpresent crc cases matches genomic proles of crc tumors after progression on prior anti - egfr therapy in tumors initially identied as ras wild type using a less - sensitive tissuebased assay . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . katherine clifton employment : wellcare ( i ) stock and other ownership interests : wellcare ( i ) thereasa a . 
raymond employment : trovagene , guardant health stock and other ownership interests : trovagene , guardant health arvind dasari consulting or advisory role : ipsen , abbvie / stemcentrx , novartis , voluntis , lexicon research funding : novartis , effector therapeutics , eisai , hutchison medipharma , merck , guardant health jonathan m . 
j cell mol med 16 : 237 - 248 , 2012 schram am , chang mt , jonsson p , et al : fusions in solid tumours : diagnostic strategies , targeted therapy , and acquired resistance . 
nat rev clin oncol 14 : 735 - 748 , 2017 drilon a , laetsch tw , kummar s , et al : efcacy of larotrectinib in trk fusion - positive cancers in adults and children . 
n engl j med 378 : 731 - 739 , 2018 yakirevich e , resnick mb , mangray s , et al : oncogenic alk fusion in rare and aggressive subtype of colorectal adenocarcinoma as a potential therapeutic target . 
clin cancer res 22 : 3831 - 3840 , 2016 amatu a , somaschini a , cerea g , et al : novel cad - alk gene rearrangement is drugable by entrectinib in colorectal cancer . 
br j cancer 113 : 1730 - 1734 , 2015 subbiah v , gainor jf , rahal r , et al : precision targeted therapy with blu - 667 for ret - driven cancers . 
cancer discov 8 : 836 - 849 , 2018 subbiah v , velcheti v , tuch bb , et al : selective ret kinase inhibition for patients with ret - altered cancers . 
nat commun 5 : 4846 , 2014 cocco e , benhamida j , middha s , et al : colorectal carcinomas containing hypermethylated mlh1 promoter and wild type braf / kras are enriched for targetable kinase fusions . 
zill oa , banks kc , fairclough sr , et al : the landscape of actionable genomic alterations in cell - free circulating tumor dna from 21 , 807 advanced cancer type braf and kras . 
daly c , castanaro c , zhang w , et al : fgfr3 - tacc3 fusion proteins act as naturally occurring drivers of tumor resistance by functionally substituting for egfr / erk signaling . 
mccoach ce , blakely cm , banks kc , et al : clinical utility of cell - free dna for the detection of alk fusions and genomic mechanisms of alk inhibitor resistance in non - small cell lung cancer . 
piotrowska z , isozaki h , lennerz jk , et al : landscape of acquired resistance to osimertinib in egfr - mutant nsclc and clinical validation of combined egfr and ret inhibition with osimertinib and blu - 667 for acquired ret fusion . 
liang w , he q , chen y , et al : metastatic eml4 - alk fusion detected by circulating dna genotyping in an egfr - mutated nsclc patient and successful management by adding alk inhibitors : a case report . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free 26 . 
odegaard ji , vincent jj , mortimer s , et al : validation of a plasma - based comprehensive cancer genotyping assay utilizing orthogonal tissueand plasma - based circulating tumor dna . 
rankin a , klempner sj , erlich r , et al : broad detection of alterations predicted to confer lack of benet from egfr antibodies or sensitivity to targeted therapy in advanced colorectal cancer . 
parseghian cm , loree jm , morris vk , et al : anti - egfr - resistant clones decay exponentially after progression : implications for anti - egfr re - challenge . 
chae yk , ranganath k , hammerman ps , et al : inhibition of the broblast growth factor receptor ( fgfr ) pathway : the current landscape and barriers to clinical oncol 30 : 243 - 249 , 2019 application . 
 actionable fusions in crc using a ctdna assay appendix fusionpositive patients ( n = 40 ) known treatment history ( n = 27 ) no known treatment history ( n = 13 ) prior anti - egfr exposure ( n = 21 ) no prior anti - egfr exposure ( n = 6 ) antiegfr therapy resistance signature ( n = 24 ) no antiegfr therapy resistance signature ( n = 16 ) known treatment history ( n = 19 ) no known treatment history ( n = 5 ) prior anti - egfr exposure ( n = 16 ) no prior anti - egfr exposure ( n = 3 ) fig a1 . 
ramkissoon , md , phd5 , 6 ; and malak abedalthaga , md7 this case study demonstrates that rst - line treatment of a neurotrophic receptor tyrosine kinase ( ntrk ) fusionpositive infantile glioblastoma with larotrectinib , an ntrk inhibitor ( ntrki ) , was a safe and effective way to achieve tumor regression in our patient . 
an 18 - month - old saudi arabian female presented with a history of right - sided weakness and partial seizures . brain magnetic resonance imaging ( mri ) revealed a large left frontal complex contrast - enhancing mass . craniotomy for gross total resection ( gtr ) was performed , and histologic pathologic analysis revealed a diagnosis of glioblastoma . 
follow - up mri was performed 8 weeks after larotrectinib treatment and showed signicant tumor regression , indicating a positive response to treatment with no reported adverse effects . this patient case highlights the importance of genomic proling for pediatric brain tumors to identify targetable alterations . 
mri showed a large , heterogeneous , complex left frontotemporal mass with internal cystic and necrotic changes with mass effect and a rightward midline shift with enhancing focus at the left posterior thalamic region ( 8 7 9 cm ; fig 1a )  . whole - spine imaging was unremarkable , and the patient underwent craniotomy for gtr . 
the patient recovered well from surgery with no neurologic decits . postoperative mri conrmed gtr but did note a small focus of nodular enhancement in the left insular cortex suggestive of residual tumor ( fig 1b )  . intermixed small neuropathologic analysis of resected tissues revealed features consistent with a high - grade glioma best classied as glioblastoma ( who grade iv )  . 
the neoplastic cells were diffusely immunopositive for vimentin ; were focally positive for s100 and synaptophysin ; showed retained nuclear staining for ini1 ; and were immunonegative for sma , ema , cd99 , cd31 , cd34 , and neun ( figs 2c to 2f )  . 
genomic proling of tumor tissue revealed the presence of an etv6 - ntrk3 fusion , which creates a novel chimeric oncoprotein that results in continuous activation of the ntrk3 kinase . 
the fusion encompassed exons 1 to 5 of etv6 and exons 14 to 20 of ntrk3 , which retains the kinase domain of ntrk3 ( fig 2g )  . as a result of the poor survival rates associated with the patients family declined chemoglioblastoma , therapy or radiation therapy despite extensive counseling on standard - of - care treatment . 
 ( b ) after total surgical resection , postgadolinium axial t1 - weighted mri demonstrated total resection of the left frontal mass . ( c ) at recurrence , postgadolinium axial t1 - weighted mri demonstrated newly appearing mass within the operative bed ( arrow ) showing intermediate diffusion signal with corresponding contrast enhancement indicating recurrent tumor . 
the patient has received continuous larotrectinib therapy since october 2019 and was scheduled for her 6 - month followup mri studies in april 2020 ; however , as a result of the global covid - 19 pandemic , the patients family has deferred further nonemergent hospital visits ( including followup mris ) until the self - isolation restrictions have been lifted . 
therefore , the patient was advanced to a digital clinic visit , where she was noted to be clinically stable and neurologically intact without any evidence of adverse events or toxicities to date . 
we obtained consent from the patients guardian to publish the patients presentation and related images . methods genomic proling next - generation sequencing was performed as previously described8 using the oncomine comprehensive assay v3 system ( thermo fisher scientic , waltham , ma )  . 
assays were performed using the ion s5 system and ion 540 chip ( thermo fisher )  . discussion primary brain tumors are a leading cause of cancer - related morbidity and mortality in children.9 high - grade gliomas ( hggs ) account for approximately 10% of pediatric brain tumors and are the second most common malignant cns tumor after medulloblastoma . 
the most frequent tumors are anaplastic astrocytoma ( who grade iii ) and glioblastoma ( who grade iv ) .10 glioblastoma occurs in both children and adults and is associated with a poor prognosis . 
 ( a ) sheet of highly cellular monomorphic round primitive cells with relative demarcation from adjacent brain tissue ( hematoxylin and eosin [ he ] ; original magnication , 20 )  . 
 ( b ) heterogeneous morphologic features of the neoplasm composed of focal areas of spindle cells arranged in small fascicles and primitive round cells in myxoid background with alternating hyperand hypocellularity ( he ; original magnication , 200 )  . ( c ) higher magnication of the primitive cells in the myxoid background ( he ; original magnication , 200 )  . 
 ( g ) schematic of etv6 - ntrk3 fusion detected in patients tumor . etv6 - ntrk3 5 14 for different n - terminal chemotherapy consisting of vincristine , carboplatin , and temozolomide.12 however , progression - free survival rates remain poor for these patients , highlighting the need for new therapeutic options , including small molecules and / or immunotherapy alone or in combination with chemotherapy regimens.13 although the etiology and genomic drivers of glioblastoma are diverse , 14 - 16 a common nding in pediatric hgg , especially infantile hggs , is the presence of fusions involving ntrk , alk , and ros1 , among others . 
trk fusion proteins are oncogenic drivers that have been reported in a wide range of adult and pediatric tumors that occur at high frequencies ( 90% ) in rare cancer types.17 , 18 gene fusions involving the kinase domain of each of the 3 neurotrophin receptors ( ntrk1 , ntrk2 , and ntrk3 ) fusion partners , were identied in 4% of diffuse intrinsic pontine gliomas and 10% of nonbrain stem ( nbs ) hggs . 
notably , in one study , 4 ( 40% ) of 10 nbs - hggs in children younger than 3 years old harbored an ntrk fusion gene . the high frequency of ntrk fusions in nbs - hggs from children age 3 years and the paucity of additional mutations in these tumors strongly suggest that the fusion genes are potent oncogenic drivers in early postnatal brain tumor development.19 ntrk fusions have been identied at low frequencies in lowgrade pediatric astrocytomas and adult glioblastomas.20 , 21 trk ligands ( commonly nerve growth factor for trka , brainderived growth factor or neurotrophin 4 for trkb , and neurotrophin 3 for trkc ) bind with high afnity to the extracellular domain of the trk receptor.22 , 23 this leads to receptor activation and the induction of signal transduction pathways involved in proliferation , differentiation , and survival ( eg , mapk , pi3k , and pkc pathways ) in both normal and neoplastic cells . the activity of the rst - generation trk - selective inhibitor larotrectinib in pediatric patients with tumors harboring ntrk fusions has been explored in clinical trials , including a phase i / ii trial in pediatric patients ( scout ; clinicaltrials.gov identier : nct02637687 ) and a phase ii trial involving adults and adolescents ( navigate ; clinicaltrials.gov identier : nct02576431 )  . 
larotrectinib is a potent and selective inhibitor of all 3 trks , producing potent and well - tolerated responses in adult and pediatric patients with ntrk - rearranged tumors , with sustained tumor regression in  . 
90% of infants , children , and adolescents with trk fusions at doses of 100 mg / m2 twice a day ( maximum , 100 mg per dose ) .1 - 7 the most common adverse events include mild elevations of liver enzyme levels , cytopenias , and vomiting . 
the high solubility of larotrectinib permit its use in liquid formulations in young patients unable to swallow capsules.5 , 24 increasingly , case reports in the literature demonstrate tolerance and clinical response to ntrki in pediatric patients with hgg , even after chemotherapy and radiation treatment.25 these patient cases highlight the need for clinical trials that assess the sustained durability of response to ntrki and whether these targeted therapies should be used as monotherapy agents or in combination with chemotherapy regimens . our patient case demonstrates that trk inhibitors can be integrated as a rst - line therapy for pediatric hggs harboring trk fusions . 
we also highlight the need for the integration of genomic proling in the routine histopathologic analyses of pediatric patients with malignant primary intracranial tumors to detect any genetic mutations that can be targeted with available therapies . 
bakhsh collection and assembly of data : musa alharbi , nahla ali mobark , malak abedalthaga data analysis and interpretation : musa alharbi , nahla ali mobark , fatmah a . 
ramkissoon employment : foundation medicine stock and other ownership interests : foundation medicine no other potential conicts of interest were reported . references bielack ss , cox mc , nathrath m , et al : rapid , complete and sustained tumour response to the trk inhibitor larotrectinib in an infant with recurrent , chemotherapy - refractory infantile brosarcoma carrying the characteristic etv6 - ntrk3 gene fusion . 
lancet oncol 19 : e187 , 2018 drilon a , laetsch tw , kummar s , et al : efcacy of larotrectinib in trk fusion - positive cancers in adults and children . 
n engl j med 378 : 731 - 739 , 2018 dubois sg , laetsch tw , federman n , et al : the use of neoadjuvant larotrectinib in the management of children with locally advanced trk fusion sarcomas . cancer 124 : 4241 - 4247 , 2018 laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
lancet oncol 19 : 705 - 714 , 2018 landman y , ilouze m , wein s , et al : rapid response to larotrectinib ( loxo - 101 ) in an adult chemotherapy - naive patient with advanced triple - negative secretory breast cancer expressing etv6 - ntrk3 fusion . 
espinoza jc , haley k , patel n , et al : outcome of young children with high - grade glioma treated with irradiation - avoiding intensive chemotherapy regimens : final report of the head start ii and iii trials . 
alharbi m , ali mobark n , almubarak l , et al : durable response to nivolumab in a pediatric patient with refractory glioblastoma and constitutional biallelic mismatch repair deciency . 
nat genet 46 : 444 - 450 , 2014 jones dt , hutter b , j ager n , et al : recurrent somatic alterations of fgfr1 and ntrk2 in pilocytic astrocytoma . 
ziegler ds , wong m , mayoh c , et al : brief report : potent clinical and radiological response to larotrectinib in trk fusion - driven high - grade glioma . 
lee , md1 ; daoqui you , phd1 ; rekha soni1 ; rachna shah1 ; marsha reyngold , md , phd1 ; nora katabi , md1 ; vanessa wu1 ; sean m . 
negative controls included samples from seven patients with hpv - negative head and neck cancers and 20 individuals without cancer . results of 97 patients with nonmetastatic , locoregionally conned oropharyngeal squamous cell carcinoma , 90 patients had detectable hpv16 ctdna and three patients had hpv33 ctdna , indicating an overall sensitivity of 95.6%. 
hpv16 ctdna was detected in 19 of 19 patients with low - volume disease , dened as patients with a single , asymptomatic positive lymph node ( n1 ) or an isolated t1 - 2 asymptomatic primary tumor . 
hpv16 ctdna levels directly corresponded to tumor responses to chemoradiation and surgery . conclusion with an updated understanding of hpv subtypes and sequence variation , hpv ctdna by ddpcr is highly sensitive and specic , identifying hpv16 and hpv33 subtypes in a similar distribution as reported in major genomic proling studies . 
2019 by american society of clinical oncology introduction detection of tumor - derived plasma epstein - barr virus dna has been successfully used in a primary screening study for nasopharyngeal cancer ( npc ) , 1 which demonstrated that npcs could be detected in asymptomatic patients with an earlier disease stage distribution than in the unscreened population . 
viral circulating tumor dna ( ctdna ) as a substrate affords unique technical advantages over single nucleotide variant detection in liquid biopsy assays because of the size of the viral genome and differentness from the human genome and because of the multiple copies of viral genome per tumor genome . 
these features elevate the sensitivity of detection of viral tumor dna , although it is unknown whether viral - associated malignancies other than npc could be similarly detected by liquid biopsy . cancers etiologically driven by human papillomaviruses ( hpvs ) include squamous cell carcinomas of the oropharynx , cervix , vulva , vagina , anal canal , and penis . 
pelvic exams and papanicolaou smears are widely adopted screening tools for early detection of early hpv - associated lesions in the cervix ; however , effective screening approaches for other disease sites are lacking . 
 damerla et al context the human papillomavirus ( hpv ) is a causative agent in cancers of the oropharynx , cervix , vulva , vagina , anal canal , and penis . 
here , we used droplet digital polymerase chain reaction technology to detect the most common hpv strains in hpv - associated oropharyngeal cancer , hpv types 16 and 33 , and achieved near - universal detection of hpv in circulating tumor dna derived from the plasma samples of these patients . 
droplet digital polymerase chain reaction of hpv types 16 and 33 was sensitive enough to detect patients with low disease burden , such as an isolated neck node or t1 - 2 primary tumors . 
these data suggest that this technology could be well suited for screening and disease monitoring . in the study , we sought to determine the clinical utility of hpv ctdna by measuring the sensitivity and specicity of the most sensitive ctdna technology available , droplet digital pcr ( ddpcr ) , 9 in patients with macroscopic gross disease and in various clinical settings after initial presentation . 
to determine the utility of ddpcr in a screening setting , we examine 19 patients in low - volume disease states that are analogous to desired subclinical , screen - detected settings . 
these include patients in whom a surgeon has already removed the primary tumor in the oropharynx with transoral robotic surgery , leaving only a single , asymptomatic lymph node in the neck ( n1 disease )  . 
the clinical characteristics of patients in the series are similar to those of previously published cohorts from our institution , 10 - 12 with stage iva , t2 , and n2b disease as the most common american joint committee on cancer seventh edition cancer stage , t stage , and n stage , respectively ( table 1 )  . study patients plasma specimens from 97 hpv - positive patients with opscc with locoregionally conned disease and eight hpv - positive patients with anal squamous cell carcinoma were accrued ( table 1 )  . 
hpv positivity was dened as p16 overexpression by immunohistochemistry with greater than 70% diffuse nuclear or cytoplasmic staining ( n = 95 ) or a clinically reported positive dnaor rna - based in situ hybridization test for hpv ( n = 53 ) .13 samples from seven patients with hpv - negative head and neck cancers , eight patients with hpv - positive opsccs who had already undergone denitive surgery , and 20 patients without cancer were included as negative controls . 
gross tumor volume was determined from the used radiation plans for which the treating radiation oncologist contoured gross disease and the plan was technically accessible ( n = 84 )  . sample collection and preparation ten milliliters of whole blood were collected from each patient into cell - free dna ( cfdna ) bct tubes ( streck , la vista , ne ) or bd vacutainer k2 edta tubes ( bd biosciences , san jose , ca )  . 
plasma was separated rst though centrifugation at 800 g for 10 minutes , followed by an additional centrifugation at 16 , 500 g for 10 minutes . when samples were collected in bd vacutainer k2 edta tubes , plasma was separated within 1 hour of blood collection and stored at 80c in eppendorf lobind tubes ( eppendorf , hamburg , germany )  . 
at a later date , samples were thawed and cfdna was extracted from 4 to 5 ml of plasma using qiagen circulating nucleic acid kits ( qiagen , germantown , md ) into a 50 - l nal elution volume . 
pretreatment plasma samples were collected a median of 2.4 weeks before the start of chemoradiation . ctdna analysis primers and probes for ddpcr assays and quantitative pcr assay are listed in appendix table a1 . 
of patients * opscc ( n = 97 ) initial presentation anal scc ( n = 8 ) 41 - 82 51 - 71 characteristic age , years median range male female race white asian african american other unknown smoking history never , 10 pack - years  . 
plates were read and analyzed using quantasoft software ( bio - rad ) to assess the number of droplets positive for the target gene , reference gene , both , or neither . 
the assay threshold sensitivity was set at two mutant droplets . pathologic data in a subset of patients , targeted next - generation sequencing ( ngs ) data of pathologic samples were available , obtained through the us food and drug administration approved msk - impact ( memorial sloan kettering cancer center , new york , ny ) sequencing platform.14 to evaluate hpv16 copy number in 10 patients , we extracted genomic dna from formalin - xed parafn - embeddedpreserved pathologic samples . 
one corresponding hematoxylin and eosinstained slide was reviewed by a pathologist ( n.k. ) and used as a template to scrape , collect , and extract genomic dna from regions of other unstained slides with greater than 75% tumor cellularity . 
genomic dna was then used for hpv16 ddpcr , and the hpv16 copy number was considered as the ratio of hpv16 - positive droplets to droplets containing the reference gene eif2c1 . statistical analysis sensitivity was dened as the number of pretreatment cfdna samples that were positive for hpv ctdna divided by the total number of patients ( n = 97 )  . 
specicity was dened as the number of negative control samples that had zero hpv - positive droplets divided by the total number of negative controls ( n = 27 )  . 
to evaluate for any correlation between gross tumor volume or copy number with the initial ctdna levels , spearman correlation coefcients were calculated using prism software by graphpad ( san diego , ca )  . 
 hpv ctdna detection results assay design we rst sought to develop the best possible primer - probe set for ddpcr using the following three criteria : location within the e6 or e7 oncogenes because these sequences are the most highly amplied sequences in tumor genomes15 ; smaller amplicon size , to increase probability of amplication in view of the highly fragmented nature of cfdna ; and primers or probes that perfectly match both european and non - european hpv16 isolates , maximizing universality of the test ( appendix fig a1 )  . 
briey , we used the papillomavirus episteme resource ( pave.niaid.nih. gov ) 16 and identied the 10 sequences representative of hpv16 sublineages ( a1 to a4 , b1 and b2 , c1 , and d1 to d3 ) , spanning european , asian , and african isolates of hpv16 ( appendix fig a1 and appendix table a2 )  . 
we chose primers and probes within e6 and e7 that match these 10 most common sequences exactly and then subsequently compared these sequences with an additional 455 hpv16 isolates found in genbank . 
a primerprobe set in e6 with a length of 97 base pairs met all criteria and demonstrated high pcr efciency and sensitivity down to a single molecule of template hpv16 dna in a ddpcr assay ( appendix fig a2 )  . 
we also tested 20 samples from normal individuals without cancer and seven samples from patients with hpv - negative head and neck cancers , and no droplets were detected in these 27 samples , demonstrating 100% specicity . 
in two of those four patients , the tumor pathology was hpv16 negative , and in both patients , no hpv16 ctdna was detected ( fig 1a , teal )  . in the two other patients , the tumor pathology was hpv16 positive , and in both of these patients , hpv16 ctdna was readily detected in plasma ( fig 1a , red ) , demonstrating 100% concordance ( four of four patients ) between plasma and the tumor specimen in hpv subtyping . 
as an additional control , we collected plasma from eight patients who had already undergone denitive surgery , and hpv was detected in none of these patients , although in two available matched samples , hpv16 ctdna was readily detected before surgery ( fig 1a , dark orange )  . the mean hpv16 ctdna level was 1 , 218 copies / ml ( range , 0 to 13 , 163 copies / ml ) , with no clear cut points for classications into groups . 
we also tested eight plasma samples from patients with anal cancers and detected hpv16 ctdna with a mean of 2 , 151 copies / ml in seven samples , demonstrating that the ddpcr assay can be used in other hpv - positive malignancies ( fig 1a )  . 
we then developed a ddpcr assay for hpv33 , which is the next most common hpv type associated with opscc.17 we observed no hpv33 - positive droplets in 20 samples from normal individuals without cancer . 
after these results , additional pathologic specimens in two of the four hpv16 and hpv33 ctdnanegative patients were genotyped by rna in situ hybridization and found to be negative for hpv16 , suggesting other high - risk hpv subtypes . 
the four negative patients ranged in regard to tumor size and stage and had no distinguishing clinical characteristics ( fig 2b )  . hpv ctdna detection in patients with low disease burden the purpose of liquid biopsy in a screening setting would be to identify subclinical tumors at early disease stages . 
we determined hpv ctdna levels in 19 patients with lowvolume tumor burden , and hpv16 ctdna was readily detectable in all 19 patients by ddpcr ( fig 2a )  . 
in 16 patients with hpv - positive opscc , the primary tumor site in the base of tongue and tonsil had been removed with denitive transoral robotic surgery , and thus , there was no remaining gross disease in the oropharynx at the time of plasma collection . 
in two additional patients , a neck dissection with negative margins had been performed to remove all gross disease , leaving only t1 - 2 primary tumors in the oropharynx . 
in these two patients , low - volume t1 base of tongue and t2 tonsillar primary tumors were imperceptible to the patient , and all gross disease in the neck had been removed before plasma collection . 
because the number of hpv genomic copies per tumor genome can be widely variable , 17 we determined the hpv copy number directly in 10 tumor pathologic samples , which ranged from 0.8 to 57 copies per tumor genome ( fig 2c )  . 
 damerla et al sensitivity : 90 / 97 = 92.8% specificity : 27 / 27 = 100% 10 , 000 1 , 000 undetectable normal individuals ( n = 20 ) hpv - negative hnscc ( n = 7 ) hpv - positive opscc ( n = 97 ) hpv - positive opscc after definitive surgery ( n = 8 ) anal cancers ( n = 8 ) pathology : hpv16 positive pathology : hpv16 negative undetermined hpv subtype matched samples , before and after surgery sensitivity : 93 / 97 = 95.9% 10 , 000 1 , 000 undetectable undetectable normal individuals ( n = 20 ) hpv - positive opsccs ( n = 7 ) pathology : hpv16 negative undetermined hpv subtype , hpv16 ctdna negative hpv - positive opsccs ( n = 97 ) hpv16 ctdna positive hpv33 ctdna positive undetectable hpv16 / 33 ctdna fig 1 . 
 ( a ) hpv16 circulating tumor dna ( ctdna ) detected by the hpv16 ddpcr assay in samples obtained from normal individuals ( n = 20 ) and patients with hpv - negative head and neck squamous cell carcinomas ( hnsccs ; n = 7 ) , hpv - associated oropharyngeal squamous cell carcinomas ( opsccs ; n = 97 ) , and anal squamous cell carcinomas ( n = 8 )  . 
 ( c ) correlation between pretreatment levels of hpv measured by hpv16 droplet digital polymerase chain reaction ( ddpcr ) and hpv copy number per tumor genome . ( d ) correlation between pretreatment levels of hpv measured by hpv16 ddpcr and product of hpv copy number and gross tumor volume . 
figure 3a shows the raw data of one patient during the course of radiotherapy , and the number of droplets positive for hpv16 ( blue ) decreases rapidly , whereas the number of droplets positive for a reference gene ( eif2c1 ) remains unchanged . 
 ( a ) amplitude plots of the ddpcr raw data are shown for crt per week of one patient with oropharyngeal squamous cell carcinoma , starting from pretreatment sample on the left , samples collected per week through 8 weeks of crt , and post - treatment sample on the right . 
 ( b ) graph representing median hpv copies per milliliter at each treatment time point from b along with interquartile range ( dark blue dashed lines ) and minimum and maximum values ( light blue dashed lines ) in patients with complete sets of plasma samples ( 28 patients ) every week . 
 ( c ) median hpv copies per milliliter measures in patient samples after every week of crt are represented as a fraction of the same - patient pretreatment sample ( 28 patients )  . 
ctdna , circulating tumor dna . with multiple samples , hpv16 ctdna was generally cleared by week 7 after the start of chemoradiation , with the exception of three patients in whom hpv16 ctdna levels remained detectable at 10 weeks ( appendix fig a3 )  . 
in this study , we demonstrated that hpv ctdna can be detected in nearly all patients with hpv - positive opscc , a marked improvement over previously reported low - cost pcr - based technologies and likely a result of the following four primary improvements : use of the ddpcr technique , which we found to be superior to quantitative pcr ; design of hpv16 primers and probes that match all hpv16 variants ; use of a combination of hpv16 and hpv33 tests ; and plasma collection and storage procedures optimized for cfdna . 
we demonstrated that the assay was portable to other hpv - associated malignancies because we also detected hpv ctdna in seven of eight anal squamous cell carcinomas . because plasma epstein - barr virus dna can be used to detect subclinical npcs in early stages , we examined whether hpv ctdna can be used to detect tumors with low disease burden . in 19 patients , plasma was collected after the symptomatic site of disease had already been resected , and yet hpv16 ctdna remained detectable . 
early detection by liquid biopsy of patients with t1n0 or t1n1 hpv - positive opsccs would be benecial to patients because these patients may be candidates for curative transoral robotic resections alone , obviating the need for postoperative radiation . 
likewise , patients with early t1n0 anal squamous cell carcinoma are candidates for curative local excisions without any radiotherapy . in addition , the specicity of the test , which is of paramount importance in any screening application , was 100% in 27 negative control samples . 
the plasma hpv16 ctdna signal completely responded to tumor - directed therapies and paralleled plasma levels of driver mutations , indicating that hpv ctdna is highly tumor specic . previous research has shown various degrees of sensitivities for hpv detection for patients with head and neck cancer3 - 6 , 8 and anogenital cancer23 - 25 using pcr - based methods . 
a disadvantage of ddpcr would be the requirement to use limited material for independent hpv16 and hpv33 tests . these two hpv subtypes constitute more than 95% of all oropharyngeal26 , 27 and anal hpv - associated squamous cell carcinomas.28 if a single test were to be used to detect cervical cancer as well , an hpv18 ddpcr test would need to be added . 
although our ctdna results match the distribution of hpv16 and hpv33 frequencies in hpv - associated opscc , we were not able to specically hpv genotype all pathologic specimens that were diagnosed as hpv positive by p16 positivity and / or dna or rna in situ hybridization by standard clinical denitions.13 in addition , it should be noted that although hpv ctdna was detected in all 19 patients with low tumor burden , these patients may not be representative of patients with early subclinical disease because micrometastatic lesions in these patients with locoregional disease could articially boost sensitivity of the assay . 
lee stock and other ownership interests : astrazeneca ( i ) consulting or advisory role : merck , pzer , merck serono , sano research funding : astrazeneca sean m . 
mcbride consulting or advisory role : bristol - myers squibb , janssen nadeem riaz honoraria : peerview speakers ' bureau : illumina research funding : bristol - myers squibb , pzer travel , accommodations , expenses : varian medical systems n . 
damerla are inventors on a provisional patent application led by their institution , memorial sloan kettering cancer center ( inst ) no other potential conicts of interest were reported . acknowledgment we thank erik anderson , luis diaz , jonathan leeman , jeremy setton , and dana tsui for helpful discussions . references chan kca , woo jks , king a , et al : analysis of plasma epstein - barr virus dna to screen for nasopharyngeal cancer . 
n engl j med 377 : 513 - 522 , 2017 chaturvedi ak , engels ea , pfeiffer rm , et al : human papillomavirus and rising oropharyngeal cancer incidence in the united states . 
j clin oncol 29 : 4294 - 4301 , 2011 ahn sm , chan jy , zhang z , et al : saliva and plasma quantitative polymerase chain reaction - based detection and surveillance of human papillomavirus - related head and neck cancer . 
jama otolaryngol head neck surg 140 : 846 - 854 , 2014 cao h , banh a , kwok s , et al : quantitation of human papillomavirus dna in plasma of oropharyngeal carcinoma patients . 
mazurek am , rutkowski t , fiszer - kierzkowska a , et al : assessment of the total cfdna and hpv16 / 18 detection in plasma samples of head and neck squamous 6 . 
wang y , springer s , mulvey cl , et al : detection of somatic mutations and hpv in the saliva and plasma of patients with head and neck squamous cell cell carcinoma patients . 
sci transl med 7 : 293ra104 , 2015 gupta gp , kumar s , marron d , et al : circulating tumor hpv16 dna as a biomarker of tumor genomics and disease control in hpv - associated oropharyngeal squamous cell carcinoma . 
int j radiat oncol biol phys 100 : 1310 - 1311 , 2018 dahlstrom kr , li g , hussey cs , et al : circulating human papillomavirus dna as a marker for disease extent and recurrence among patients with oropharyngeal cancer . 
leeman je , li jg , pei x , et al : patterns of treatment failure and postrecurrence outcomes among patients with locally advanced head and neck squamous cell carcinoma after chemoradiotherapy using modern radiation techniques . 
zumsteg zs , lok bh , ho as , et al : the toxicity and efcacy of concomitant chemoradiotherapy in patients aged 70 years and older with oropharyngeal carcinoma in the intensity - modulated radiotherapy era . 
setton j , caria n , romanyshyn j , et al : intensity - modulated radiotherapy in the treatment of oropharyngeal cancer : an update of the memorial sloan - kettering cancer center experience . 
deshmukh aa , tanner rj , luetke mc , et al : prevalence and risk of penile human papillomavirus infection : evidence from the national health and nutrition examination survey 2013 - 2014 . 
faust h , eldenhed alwan e , roslin a , et al : prevalence of human papillomavirus types , viral load and physical status of hpv16 in head and neck squamous cell carcinoma from the south swedish health care region . 
serup - hansen e , linnemann d , skovrider - ruminski w , et al : human papillomavirus genotyping and p16 expression as prognostic factors for patients with american joint committee on cancer stages i to iii carcinoma of the anal canal . 
reference name source k02718 pph16 af536179 af536179 european ( e ) european ( e ) hq644236 hq644236 european ( e ) af534061 af534061 asian ; e ( as ) af536180 af536180 african - 1 ; afr1a hq644298 hq644298 african - 1 ; afr1b af472509 af472509 african - 2 ; afr2a hq644257 hq644257 north american ( na ) 1 ay686579 ay686579 asian_american ( aa ) 2 af402678 af402678 asian_american ( aa ) 1 aligned with clustalw algorithm ( muscle 3.8 ) limited selection to early genes e6 and e7 of hpv16 genome ( amplified regions during hpv integration ) chose amplicons in e6 and e7 < 100 bp in size cross - referenced with 445 hpv16 variants from ncbi genbank alignment blast against human genome and other hpv strains selected best amplicon by ddpcr performance forward primer probe reverse primer standard curves and testing patient plasma samples fig a1 . 
 ( a - c and f ) standard curves of roche cobas hpv test , hpv16 ddpcr , hpv33 ddpcr , and hpv16 quantitative pcr ( qpcr ) using a serial dilution of hpv16 plasmid template on a plasmid . 
approximately 200 base pairs ( bp ) , likely too large for fragmented ctdna , which has a median size of 176 bp.9 ( e and h ) comparison of hpv16 ddpcr and hpv16 qpcr in the same 12 samples . 
at high levels of hpv16 , the hpv ctdna signal can begin to saturate , as observed in three samples because only 20 , 000 droplets are read on the bio - rad qx200 platforthe higher sensitivity of the ddpcr assay despite a larger amplicon size may be secondary to the partitioning of dna into droplets and reduced inhibitory factors compared with qpcr29 ct , cycle threshold . definitive crt samples 15 , 000 10 , 000 7 , 000 6 , 000 5 , 000 4 , 000 3 , 000 2 , 000 1 , 000 pre - crt sample time ( weeks of crt ) post - crt samples fig a3 . 
noonan , mbbchbao , msc1 - 3 ; sagar sardesai , md1 - 3 ; jeffrey vandeusen , md , phd1 - 3 ; robert wesolowski , md1 - 3 ; nicole williams , md1 - 3 ; clara n . 
we evaluated three prespecied questions to assess patients perceptions of genomic testing . results in all , 100 patients underwent genomic testing , with a median of ve mutations ( range , 0 to 13 mutations ) detected per patient . 
genomic testing revealed one or more potential therapies in 98% of patients ( 98 of 100 ) , and 60% of patients ( 60 of 100 ) had one or more recommended treatments with level i / ii evidence for actionability . 
we did not detect a statistically signicant difference in time - to - treatment failure ( log - rank p = .87 ) or overall survival ( p = .71 ) among patients who had treatment change supported by genomic testing versus those who had no treatment change . 
this study provides a prospective analysis of physician decision making and outcomes of patients receiving tumor sequencing as part of mbc clinical care . knowledge generated genomic testing revealed that most patients ( 60% ) had at least one recommended treatment with level i / ii evidence for actionability ; however , only a subset of patients were given a recommendation for a change in treatment , and even fewer actually changed therapy on the basis of genomic testing results . 
patients whose therapy did not change on the basis of genomic testing had a decrease in condence of treatment success . relevance even though standard of care is improving , relatively few patients with mbc changed therapy on the basis of genomic testing in this prospective study . 
this suggests a need to better understand barriers to implementation of mutation - directed therapy as well as a need for improved understanding of patient perception of somatic genomic testing . ( ia ) , pik3ca hotspot - activating missense mutations ( ia ) , microsatellite instability ( ic ) , ntrk fusions ( ic ) , esr1 hotspot - activating missense mutations ( iia ) , pten loss ( iia ) , akt1 mutations ( iib ) , and erbb2 hotspot - activating missense mutations ( iib ) .16 although genomic testing is promising for improving treatment efcacy , it is unclear how frequently it changes treatment.17 - 19 complex interactions between choice of genomic testing and patient perception of care make it imperative to understand the impact of genetic sequencing in clinical oncology.17 , 20 , 21 to date , we have little understanding of how patients perceive the value or accuracy of genomic testing , and whether changes in treatment recommendation based on genomic testing affect patients perceptions of care . 
there are discrepancies between cancer patient and physician expectations of therapy efcacy ; patients demonstrate greater optimism about therapy efcacy.22 - 25 expectations of patients with mbc and their motivations for undergoing somatic genetic testing have not yet been explored . clinical tumor genomic analyses typically rely on targeted next - generation sequencing ( ngs ) of a panel of specic , typically actionable cancer - related genes to analyze somatic gene alterations from biopsy specimens . 
most commercial targeted panel sequencing approaches , including foundationone cdx ( foundation medicine , cambridge , ma ) in this study , provide treatment suggestions that are based on literature.26 we genomic alterations and available clinical hypothesized that prospective implementation of foundationone cdx testing into clinical care for patients with mbc will identify patient - specic approaches that offer improved patient outcomes and perceptions of care . 
in this study , patients with mbc received foundationone cdx testing when a new treatment was initiated and genomic testing results released to the provider at the next progression event . 
the study was approved by the ohio state university institutional review board and informed consent was obtained from all patients . testing was performed by using foundationone cdx , formalin - xed parafnwhich used ngs on patients embedded tumor tissue . 
the foundationone cdx results were then released to the provider . survey measures physicians received a ve - item questionnaire after the foundationone cdx report was released to assess whether their treatment recommendation should be changed on the basis of those results . 
the questionnaire asked how the physician used the foundationone cdx test ( multiple choice ) and what else they would like to see in the report ( multiple choice plus an open - ended other option )  . 
attitudes toward foundationone cdx testing were assessed with three items : ( 1 ) by having the test , i will feel more condent of my treatments success , ( 2 ) i will trust the test results , and ( 3 ) i think the test results will be accurate . 
patient motivation and expectations for study participation were assessed with 15 questions using a ve - point likert scale that ranged from strongly disagree to strongly agree ( data supplement )  . because of small numbers in each group , these questions were assessed as a three - level outcome ( agree v neutral v disagree ) and as a binary outcome ( agree v neutral and disagree )  . statistical and survival analyses mcnemars test of agreement ( 2 level or 3 level ) was used to compare preand post - test survey responses and preversus post - test survey agreement by foundationone cdxsupported treatment change results from the physician questionnaire . 
the offstudy date was dened as the date of the patients second progression ( rst while on study ) , second treatment change ( rst while on study ) , death , or loss to follow - up . 
patients still alive on december 18 , 2018 , were censored as of this date . all statistical analyses were performed using sas version 9.4 ( sas institute , cary , nc ) and r version 3.4.1 , and survival curves were created using the packhv package.27 results study population a total of 142 patients with mbc provided consent and were assessed for eligibility ( fig 1 )  . 
patients were excluded from analysis if there was no available tissue , insufcient tissue , or poor dna quality ( n = 21 ) , died before the foundationone cdx report was released ( n = 13 ) , did not receive foundationone cdx testing within 10 weeks of starting their current line of therapy ( n = 4 ) , were lost to follow - up ( n = 2 ) , withdrew consent ( n = 1 ) , or had a biopsy that revealed no metastatic disease ( n = 1 )  . 
of these samples , 71% ( 71 of 100 ) were metastatic biopsies and 29% ( 29 of 100 ) were primary tumors ( breast or axillary lymph node )  . 
the study population was predominantly age 55 years or older , white , and collegeeducated with a high income ( table 1 )  . foundationone cdx genomic testing results among the 100 patients with successful foundationone cdx ngs testing , the number of mutations identied per patient ranged from 0 to 13 with a median of ve mutations ( data supplement )  . 
as anticipated , the most common mutations were missense or frameshift mutations in tp53 ( n = 49 ) and pik3ca ( n = 40 ) or amplication of myc ( n = 20 ; fig 2a )  . 
among er - positive / her2 - negative patients , 10 ( 16.7% ) of 63 harbored an esr1 mutation . in terms of therapy recommendations , 98 ( 98.0% ) of 100 patients had at least one potential therapy identied on foundationone cdx testing , with a median of nine potential treatments ( range , 0 to 35 potential treatment ; fig 2b )  . 
the most commonly recommended therapy based on a genomic alteration was an mtor inhibitor ( everolimus or temsirolimus ) for pik3ca mutations ( data supplement )  . among all patients , 60 ( 60% ) of 100 had at least one recommended treatment with level i / ii evidence ( not including erbb2 amplications ) , 16 with a median of one potential treatment with level i / ii evidence ( range , 0 to 2 potential treatments ; fig 2b )  . potential germline alterations in somatic tumor testing a known challenge in somatic tumor sequencing is potential identication of germline alterations.28 - 32 among the 100 total patients , 14 had alterations identied in brca1 ( n = 4 ) , brca2 ( n = 8 ) , or palb2 ( n = 2 )  . 
of these six patients with no prior knowledge of germline mutations , two had germline alterations conrmed ( one brca1 and one brca2 ) and one underwent germline testing in which no alterations were identied ( presumed somatic brca2 mutation )  . 
the six patients whose foundationone cdx reports were not therapy without proreleased remained on their initial gression as of september 1 , 2018 ; ve of these patients had er - positive / her2 - negative and one had er - positive / her2 - positive breast cancer . 
across the study population , 10 ( 10.0% ) of 100 total patients or 10 ( 11.5% ) of 87 patients with physician questionnaire data experienced a treatment change supported by foundationone cdx data . 
physicians described not changing treatment because the patient could not be enrolled on a clinical trial ( ie , the recommended trial closed , the patient did not want to enroll , or the patient was ineligible ; n = 10 ) , patient hospitalization ( n = 3 ) , insurance denied treatment charges ( n = 2 ) , patient transferred care to other provider ( n = 1 ) , or patient pursued a nonrecommended trial ( n = 1 ; data supplement )  . genomic alterations and survival among 76 patients evaluable for ttf analysis , there was no signicant difference in ttf ( log - rank p = .87 ) by foundationone cdx - supported treatment change status ( fig 3a )  . 
despite a high frequency of mutation , there was no signicant difference in os by pik3ca mutation status among er - positive / her2 - negative patients ( p = .18 ) or tnbc patients ( p = .66 ) , or when evaluating alterations that could activate the pi3k pathway ( pik3ca mutation , pten loss , or akt1 mutation ) among er - positive / her2 - negative patients ( p = .60 ) or tnbc ( p = .81 ) patients ( data supplement )  . 
in the msk - impact study ( clinicaltrials.gov identier : nct01775072 ) , hrpositive / her2 - negative patients with detected tumor mutations in esr1 , map kinase pathway , or myc or other transcription factors genes had a worse response to aromatase inhibitor these alterations.15 we evaluated the association of these alterations with os and found no signicant difference among the four groups ( fig 3d )  . therapy than patients without patients perceptions of genetic testing a total of 58 ( 58.0% ) of the 100 evaluable patients completed at least a portion of the survey at enrollment ( pretest ) , and 40 ( 40.0% ) completed at least a portion of the survey at study conclusion ( post - test )  . 
in the pretest survey , most patients strongly agreed or somewhat agreed that by having the genetic testing they would feel more condent in their treatments success ( 36 [ 65.5% ] of 55 ) , whereas at study completion , a minority of patients ( 12 [ 30.8% ] of 39 ) felt more condent in their treatments success by having the genetic testing . 
there was no signicant difference in patients trust of test results or thinking the results were accurate ( mcnemars p = .06 for both questions )  . foundationone cdx - supported treatment change status ( fig 3b )  . 
by subtype , there were signicant differences in os ( log - rank p = .01 ) ; patients who had tnbc had worse os than er - positive / her2 - negative patients , as anticipated ( data supplement )  . among genomic alterations , we evaluated several mutations known to be prognostic ( esr1 mutations ) or potentially predictive of outcomes ( pik3ca )  . 
in msk - impact ( a targeted tumor - sequencing assay developed at memorial sloan kettering cancer center [ msk ] termed integrated mutation proling of actionable cancer targets [ impact ] ) , there was evidence that patient response to aromatase inhibitor therapy was signicantly worse for patients whose tumors harbored one of several alterations.15 among we then assessed whether pretest and post - test survey results were associated with treatment change on the basis of foundationone cdx results in patients who completed both the pretest and post - test survey questions of interest . for treatment condence , we found that patients who did not have a treatment change supported by foundationone cdx data were signicantly more likely to change their response from agree to neutral or disagree ( mcnemars test of agreement p = .001 ; fig 4 )  . 
of potential therapies with level i / ii evidence 50 40 30 20 10 0 % mutant tp53 pik3ca cdh1 znf703 esr1 ccnd1 fgfr1 fgf4 fgf19 gata3 fgf3 map2k4 znf217 pten mcl1 brca2 erbb2 map3k1 arid1a smad4 myst mdm2 mutations or potential therapies for each patient fig 2 . 
comut plot created by using the genvisr package.47 ( b ) for each patient ( n = 100 ) , the graph shows number of detectable mutations , number of potential therapies identied , and number of potential therapies with level i / ii evidence for actionability in breast cancer based on condorelli , et al.16 ( * ) indicates patients whose treatment was changed based on genomic testing results . treatment ( data supplement )  . 
 ( a ) kaplan - meier plot of time to treatment failure stratied by patients with treatment change based on genomic testing ( red line ) v no treatment change . 
time to treatment failure dened as time from release of foundationone cdx results to the off - study date , dened as date of second progression or treatment change ( rst during the study period ) , death , or loss to follow - up . 
 ( c ) kaplan - meier plot of overall survival for patients with estrogen receptor ( er ) positive / human epidermal growth factor receptor 2 ( her2 ) negative metastatic breast cancer , stratied by presence or absence of mutation in esr1 . 
we prospectively evaluated the impact of ngs on mbc treatment decisions and potential associations with patient outcomes and their perceptions of genomic testing . in this study , more than 60% of patients had a genomic alteration associated with level i or ii evidence for actionability ( not including her2 amplication ) based on a recent consensus panel16an impressive number that emphasizes the potential for widespread use of ngs . 
a total of 37 patients answered the question both before ( pre - genomic test survey ) and after ( post - genomic test survey ) genomic test results were shared with physicians . 
this is consistent with a previous study that identied barriers such as trial ineligibility , distance to trial , and physical / emotional exhaustion.18 treatment change was not signicantly associated with ttf or os ; however , the small number of patients experiencing treatment change limits the conclusions that can be drawn from these analyses . this is the rst study to our knowledge to prospectively evaluate the inuence of somatic ngs on patient perception of care and it provides important initial data , but the lower patient survey response rate limits denitive conclusions . 
when comparing study surveys at admission to surveys at conclusion , patients seemed less condent in their treatment , particularly those whose treatment was not changed by foundationone cdx results . 
this is consistent with other studies that suggest genetic testing may increase negative emotions in patients with metastatic cancer , 18 although most studies evaluated effects from germline testing.36 - 40 our data preliminarily suggests that there may be ramications of somatic genomic testing for patients despite its known utility in selecting therapy for mbc . because negative emotions are associated with decreased quality of life and potentially with survival , 41 - 44 the possible negative implications of broadly integrating ngs into clinical practice should be considered . furthermore , pretest survey data suggest that patients have misconceptions about what somatic mutation testing can inforwe found that patients had overly optimistic expectations for somatic tumor ngs : almost half believed the test would tell them which medication to take whereas only 11.5% of the total patients switched therapy on the basis of foundationone cdx reports . 
this is similar to previous studies that demonstrate that patients have greater optimism regarding treatment efcacy than physicians do , 24 possibly because physicians provide patients with more optimistic information than their true assessment.45 in addition , most patients incorrectly believed the test would predict future genetic mutations , assess childrens disease risk , or estimate treatment success , despite the informed consent stating that participants would rarely benet personally or therapeutically from this study . 
therefore , this supports further exploration of the readability of consent forms , an area currently under investigation.46 we hypothesize that patients limited knowledge of genetics may explain their decreased condence after genomic testing , 17 - 19 and we also hypothesize that improved decision support for genomic testing for patients will improve condence in their treatment , particularly in the context of increases in available targeted treatments for mbc . there are known limitations to our study that prevent us from making denitive conclusions . 
furthermore , unlike the methodologies in the existing literature , we used a unique prospective and longitudinal methodology to evaluate patient perceptions . future studies may benet by including patient interviews to assess the experience of somatic ngs . 
furthermore , the potential treatments identied by foundationone cdx test results reect drugs approved for any indication , not necessarily for mbc , and therapies available at the time of the test . 
for example , both everolimus and temsirolimus were reported as potential therapies for patients with alterations in nf1 , pten , ak1 , pik3r1 , rptor , akt3 , fbxw7 , kit , pdgfra , stk11 , and vhl ; however , only everolimus is approved by the us food and drug administration for mbc . 
in addition , since this study was completed , multiple new therapies approved by the us food and drug administration have not been considered , suggesting that clinical implications of ngs should be assessed regularly . in conclusion , our ndings suggest that ngs by tools such as foundationone cdx may provide valuable insight for physicians and patients when determining the best treatment option for patients with mbc upon disease progression . 
there are clear clinical challenges involved with integrating ngs into the framework of mbc care , including barriers to preferred treatment options and complex interactions between genomic testing and patient perceptions , which warrant further study . affiliations 1the ohio state university college of medicine , columbus , oh 2the ohio state university comprehensive cancer center , columbus , oh 3stefanie spielman comprehensive breast center , columbus , oh 4the ohio state university , columbus , oh 5foundation medicine , cambridge , ma 6the ohio state university college of public health , columbus , oh 7mt . 
chen consulting or advisory role : novartis , immune design , syapse speakers bureau : novartis , foundation medicine research funding : eisai patents , royalties , other intellectual property : matchtx , a genomics software package that helps researchers , oncologists , and clinical trial managers identify the full set of biomarkers that collectively predict the outcome of patients with cancer to treatment siraj mahamed ali employment : foundation medicine leadership : incysus stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences consulting or advisory role : revolution medicines , azitra ( i ) , princeps tx ( i ) patents , royalties , other intellectual property : patents via foundation medicine and via seres health on microbiome in non - neoplastic disease ( i ) anne m . 
noonan consulting or advisory role : helsinn healthcare , qed therapeutics sagar sardesai consulting or advisory role : novartis speakers bureau : immunomedics travel , accommodations , expenses : novartis jeffrey vandeusen stock and other ownership interests : immunomedics robert wesolowski consulting or advisory role : pzer ( inst ) , puma biotechnology research funding : acerta pharma , astrazeneca travel , accommodations , expenses : pzer , puma biotechnologybhuvaneswari ramaswamy consulting or advisory role : pzer maryam b . 
lustberg consulting or advisory role : tempus , pledpharma other relationship : hologic / cynosure no other potential conicts of interest were reported . references oshaughnessy j : extending survival with chemotherapy in metastatic breast cancer . 
condorelli r , mosele f , verret b , et al : genomic alterations in breast cancer : level of evidence for actionability according to esmo scale for clinical actionability 17 . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental ndings : results from the canseq study . of molecular targets ( escat )  . 
gollust se , gray sw , carere da , et al : consumer perspectives on access to direct - to - consumer genetic testing : role of demographic factors and the testing 21 . 
meropol nj , weinfurt kp , burnett cb , et al : perceptions of patients and physicians regarding phase i cancer clinical trials : implications for physician - patient communication . 
lux mp , bayer cm , loehberg cr , et al : shared decision - making in metastatic breast cancer : discrepancy between the expected prolongation of life and treatment efcacy between patients and physicians , and inuencing factors . 
parsons dw , roy a , plon se , et al : clinical tumor sequencing : an incidental casualty of the american college of medical genetics and genomics recommendations for reporting of incidental ndings . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
tanioka m , fan c , parker js , et al : integrated analysis of rna and dna from the phase iii trial calgb 40601 identies predictors of response to trastuzumabbased neoadjuvant chemotherapy in her2 - positive breast cancer . 
bakos ad , hutson sp , loud jt , et al : brca mutation - negative women from hereditary breast and ovarian cancer families : a qualitative study of the brca37 . 
hay jl , meischke hw , bowen dj , et al : anticipating dissemination of cancer genomics in public health : a theoretical approach to psychosocial and behavioral negative experience . 
collins vr , meiser b , ukoumunne oc , et al : the impact of predictive genetic testing for hereditary nonpolyposis colorectal cancer : three years after testing . genet med 9 : 290 - 297 , 2007 40 . 
hendriks ks , hendriks mm , birnie e , et al : familial disease with a risk of sudden death : a longitudinal study of the psychological consequences of predictive testing for long qt syndrome . 
chida y , hamer m , wardle j , et al : do stress - related psychosocial factors contribute to cancer incidence and survival ? nat clin pract oncol 5 : 466 - 475 , 2008 42 . 
giese - davis j , collie k , rancourt km , et al : decrease in depression symptoms is associated with longer survival in patients with metastatic breast cancer : a secondary analysis . 
perni s , rooney mk , horowitz dp , et al : assessment of use , specicity , and readability of written clinical informed consent forms for patients with cancer undergoing radiotherapy . 
 leiomyosarcoma ( lms ) arises from smooth muscle , most often in the uterus or retroperitoneu localized disease is treated surgically ; unfortunately , relapse occurs in 40% to 70% of patients.1 , 2 advanced lms is treated with chemotherapy . 
the most active regimens , doxorubicin and olaratumab or gemcitabine and docetaxel , are associated with response rates of 15% to 35% and progression - free survival of 4 to 7 months.3 - 6 the cytotoxic agent trabectedin and the tyrosine kinase inhibitor pazopanib are used after chemotherapy.7 , 8 clinical trials with immune checkpoint blockade have been disappointing , possibly owing to a tumor microenvironment populated by immunosuppressive macrophages.9 , 10 the alkylating agent dacarbazine ( dtic ) , one of the oldest chemotherapeutics used in sarcoma , is often used as a therapy of last resort , but it has durable activity in some patients with lms . 
we also discuss the implications of this alteration for the dna damage response to alkylating agents and review emerging data , which suggest that lms harbors characteristic defects in the homologous recombination ( hr ) dna damage response pathway . a 51 - year - old woman presented to her family physician in december 2008 with abdominal distension . 
by november 2012 , she had further disease recurrence manifested by a 16 - cm abdominal mass , which was also resected . in march 2013 , she experienced multifocal recurrence with at least 12 mesenteric masses . 
a 51 - year - old woman developed multifocal recurrent uterine leiomyosarcoma manifested by numerous intra - abdominal masses as demonstrated by representative computed tomography images obtained in march 2013 ( left )  . 
study - related computed tomography scans every 3 months demonstrated incremental regression , and by february 2014 , she had no radiographic evidence of malignancy ( fig 1 ) and has continued to receive dtic . 
 genomic sequencing of the november 2012 tumor revealed homozygous deletion of brca2 , several variants of unknown significance , copy number gain of cyclin e1 , epidermal growth factor receptor , fibroblast growth factor receptor , platelet - derived growth factor receptor alpha , and copy number loss of phosphate and tensin homolog ( pten )  . 
 o6 - meg is efficiently repaired by the mgmt enzyme , which removes the methyl adduct from o6 - guanine , restoring the normal guanine base.11 o6 alkylating agents are most effective in cancers with low mgmt expression , such as melanoma and glioblastoma , in which o6 - meg cannot be efficiently repaired . 
approximately 40% of glioblastoma patients harbor mgmt promoter methylation , and these patients derive greatest benefit from tmz.12 - 14 the normal cellular response to o6 - meg highlights several distinct but interrelated signaling pathways that make up the dna damage response . 
different types of damage , whether inflicted by environmental insults or chemotherapy , provoke specific repair mechanisms.15 the initial response to o6 - meg requires mgmt ( fig 2 )  . 
the mismatch repair pathway normally attempts to repair this mismatch but is unable to effectively do so , and multiple futile repair attempts ultimately induce a double - stranded dna break ( dsb )  . 
 the homologous recombination ( hr ) pathway is the preferred response to dsbs because hr uses a template strand to return dna to the original sequence , whereas other pathways are less conservative and lead to accumulation of mutations , genomic instability , and cell death . 
tumors with loss of brca2 are defective in hr and highly sensitive to dsb - inducing agents such as platinum chemotherapy and poly ( adp - ribose ) polymerase ( parp ) inhibitors.18 the anticancer efficacy of o6 alkylating agents such as dtic and tmz was traditionally felt to depend on the status of the mgmt and mismatch repair pathway ; cells with deficient mgmt and intact mismatch repair should accumulate dsbs and demonstrate sensitivity to these drugs . 
however , a critical role for hr has been highlighted in recent preclinical studies primarily in glioblastoma models , in which tmz is the standard of care.19 here , disruption of the hr pathway profoundly potentiated the antitumor activity of tmz.20 - 22 furthermore , resistance to tmz and dtic was not mediated by re - expression of mgmt or acquired mismatch repair deficiency but by adaptive tumor cell augmentation of hr repair.16 , 23 , 24 recently , a model capturing the combined status of multiple repair pathways was found to be much more effective in predicting cytotoxicity from o6 alkylating agents than assessing mgmt alone , and hr pathway status was of major import.25 because the hr pathway ultimately determines whether tmzand dtic - induced dsbs are repaired , defective hr , such as that induced by brca2 loss , may sensitize patients to treatment with these drugs and warrants further evaluation as a predictive biomarker . 
the failure to observe mgmt promoter methylation in this case ( confirmed on repeat testing ) is curious because intact mgmt might be expected to repair the upstream o6 - meg lesion before downstream dsbs are created . 
our findings suggest that dysfunctional hr alone may be sufficient to sensitize tumors to alkylating agents in certain contexts . emerging - omics studies suggest that lms frequently harbors defects in hr , of which our patients brca2 loss is emblematic . 
in a whole exome and transcriptomic sequencing study of 49 lms tumors , mutations in tp53 ( 49% ) , retinoblastoma ( 27% ) , and atrx ( 24% ) were most common but are not actionable.27 moreover , the tumor mutational burden was low , suggesting that immune checkpoint inhibitors are of limited benefit . 
interestingly , deleterious alterations in hr pathway genes were observed in most lms tumors and included pten ( 57% ) , brca2 ( 53% ) , fanca ( 27% ) , atm ( 22% ) , chek1 ( 22% ) , xrcc3 ( 18% ) , chek2 ( 12% ) , brca1 ( 10% ) , and rad51 ( 10% )  . 
an alexandrovcatalogue of somatic mutations in cancer ( cosmic ) signature for defective hr contributed to the mutational signature in 98% of lms tumors.27 a separate analysis of 80 patients with lms that used the cancer genome atlas revealed different gene expression signatures between soft tissue and uterine lms , with the latter harboring a higher dna damage response score.28 unfortunately , the frequency of germ line alterations in hr genes among patients with lms remains uncerta in a comprehensive molecular study of 500 patients with various solid tumors , pathogenic germ line mutations were found in 12% , and 75% of these were in dna repair genes , highlighting the importance of the germ line analysis , which is often not performed in clinical next - generation sequencing assays.29 a defective hr phenotype is of therapeutic relevance . 
several approaches to targeting cancer related vulnerabilities in hr - deficient tumors are being explored.15 several of these approaches incorporate parp inhibitors , a novel class of dna - damaging anticancer therapeutics . 
schwartz collection and assembly of data : all authors data analysis and interpretation : all authors manuscript writing : all authors final approval of manuscript : all authors julia e . 
schwartz honoraria : daiichi sankyo , darwinhealth , biomotiv , human longevity , bionaut labs , champions oncology , karyopharm therapeutics , puretech health , ellipses pharma , array biopharma , ptc therapeutics , bayer healthcare pharmaceuticals consulting or advisory role : daiichi sankyo , puretech health , biomotiv , human longevity , darwinhealth , karyopharm therapeutics , champions oncology , bionaut labs , array biopharma , ellipses pharma , ptc therapeutics , bayer healthcare pharmaceuticals matthew a . 
coindre jm , terrier p , guillou l , et al : predictive value of grade for metastasis development in the main histologic types of adult soft tissue sarcomas : a study of 1240 patients from the french federation of cancer centers sarcoma group . 
hensley ml , blessing ja , mannel r , et al : fixed - dose rate gemcitabine plus docetaxel as firstline therapy for metastatic uterine leiomyosarcoma : a gynecologic oncology group phase ii trial . 
sutton g , blessing j , hanjani p , et al : phase ii evaluation of liposomal doxorubicin ( doxil ) in recurrent or advanced leiomyosarcoma of the uterus : a gynecologic oncology group study . 
seddon b , scurr m , jones rl , et al : a phase ii trial to assess the activity of gemcitabine and docetaxel as first line chemotherapy treatment in patients with unresectable leiomyosarcoma . 
tap wd , jones rl , van tine ba , et al : olaratumab and doxorubicin versus doxorubicin alone for treatment of soft - tissue sarcoma : an open - label phase 1b and randomised phase 2 trial . 
van der graaf wt , blay jy , chawla sp , et al : pazopanib for metastatic soft - tissue sarcoma ( palette ) : a randomised , double - blind , placebo - controlled phase 3 trial . 
demetri gd , von mehren m , jones rl , et al : efficacy and safety of trabectedin or dacarbazine for metastatic liposarcoma or leiomyosarcoma after failure of conventional chemotherapy : results of a phase iii randomized multicenter clinical trial . 
burgess ma , bolejack v , van tine ba , et al . : multicenter phase ii study of pembrolizumab ( p ) in advanced soft tissue ( sts ) and bone sarcomas ( bs ) : final results of sarc028 and biomarker analyses . 
kostine m , briaire - de bruijn ih , cleven ahg , et al : increased infiltration of m2 - macrophages , t - cells and pd - l1 expression in high grade leiomyosarcomas supports immunotherapeutic strategies . 
hegi me , liu l , herman jg , et al : correlation of o6 - methylguanine methyltransferase ( mgmt ) promoter methylation with clinical outcomes in glioblastoma and clinical strategies to modulate mgmt activity . 
paz mf , yaya - tur r , rojas - marcos i , et al : cpg island hypermethylation of the dna repair enzyme methyltransferase predicts response to temozolomide in primary gliomas . 
short sc , giampieri s , worku m , et al : rad51 inhibition is an effective means of targeting dna repair in glioma models and cd133 + tumor - derived cells . 
roos wp , nikolova t , quiros s , et al : brca2 / xrcc2 dependent hr , but not nhej , is required for protection against o ( 6 ) - methylguanine triggered apoptosis , dsbs and chromosomal aberrations by a process leading to sces . 
zhang n , wu x , yang l , et al : foxm1 inhibition sensitizes resistant glioblastoma cells to temozolomide by downregulating the expression of dna - repair gene rad51 . 
most patients present with either metastatic pdac ( 50% - 60% ) or locally advanced tumors ( 30% - 40% ) , for which the median survival is 5 - 9 months after diagnosis.1 , 2 outcomes are still suboptimal for the small subset ( 10%20% ) of patients who present with resectable tumors conned to the pancreas ; , 50% of these patients survive 5 years after surgery despite modern adjuvant chemotherapy.3 moreover , at autopsy , the disease is metastatic for 88% of recurrences , and  . 
80% have more than 10 distinct metastatic lesions4 that are genetically related to the primary tumor5 and other metastases.6 these observations indicate that majority of patients with pdac harbor nonradiographically evident , micrometastatic disease after resection and that remnant tumor cells evadeor acquire resistance toadjuvant chemotherapy . 
although tropism to specic organs during metastatic spread is still poorly understood , patients with recurrence in the liver or peritoneum7 survive signicantly shorter than patients with recurrent lung metastases.8 - 10 pdac tumors are commonly classied into two major subtypes : one that shares some features with adenosquamous tumors ( squamoid and / or basal ) and the other that retains a differentiated , glandular and / or ductal morphology ( ductal and / or classical )  . 
squamoid pdac tumors are more glycolytic , 11 , 12 more hypoxic , 13 more inammatory likely broblasts , 16 and yield a poorer prognosis than ductal tumors.17 - 21 classical subtype tumors are associated with more tumor - inltrating leukocytes , denser collagen , and better outcomes , 15 , 22 although signicant subtype heterogeneity within tumors13 complicates the relationship between subtype and outcome . to metastasize , 14 , 15 recruit more cytolytic t cells inltrate pdac tumors than most other tumors , 23 but they are ultimately insufcient to control the cancer . 
density of tumor - inltrating t cells is highly variable among pdac tumors , 24 and abundant cd8 + t cells ( along with a high number of neoantigens ) can support exceptionally long - term survival.25 however , t cellmediated tumor immunity may be restricted by several mechanisms : tumor immunosuppressive cell downregulation of hla , leukocytes , t cell proximity to tumor cells , and t cell exhaustion.26 - 30 effective t cellmediated tumor immunity is enhanced by a high diversity of functional t cell clones , tumor - specic recruitment of effector t cells , and abundant neoantigens.23 , 25 , 31 quantifying the phenotypes , functions , and locations of leukocytes is critical to identify specic tumor immunity required for exceptional positive outcomes . rare , exceptional control of pdac progression may be mediated by equally rare , idiosyncratic patient genetics , tumor - specic somatic alterations and gene expression , and / or stochastically generated tumor immunity . 
in this report , we present the cases of pt1 , who survived more than 46 months with occult , chemotherapy - resistant metastatic pdac , and her niece ( pt2 ) who succumbed to progressing metastatic disease despite aggressive treatment . 
however , during adjuvant chemotherapy , the lung lesion increased to 23 mm 18 mm , and a ct and / or pet was suspicious for malignancy with a standardized uptake value ( suv ) of 4.5. 
ca19 - 9 test results are not shown becausefor both patientsthey were reproducibly approximately 90% lower than the 37 u / ml threshold for normal , even when the primary tumor was present . 
pt1 chose to receive no further treatment and was radiographically disease - free for over 2 years ( fig 1 ) until an isolated , recurrent lung metastasis was identied by ct and fdg - pet ( suv of 9 ) and then treated by 50 gy in ve fractions using stereotactic body radiotherapy . 
pt2 died 19 months after metastatic disease recurrence . treatment a shared germline prss1 mutation and somatic alterations common to pdac we identied germline prss1 p.a16v in both patients and somatic alterations in the two most common pdac driver geneskras and tp53in both tumors from each patient ( table 1 )  . 
each scale bar is 0.5 m ( c ) pdac subtyping of each patients primary and metastatic tumors . left panel : spearman correlation coefcients for tumors from pt1 and pt2 compared with the published rank order of pdassigner genes for classical ( y - axis ) and quasimesenchymal ( x - axis ) tumors . 
both tumors from pt1 aligned well with the classical subtype , whereas the tumors from pt2 were more quasimesenchymal and / or basal with the metastasis scoring more basal than the primary tumor . leukocyte types associated with immunity in tumors from patient 1 we used a multiplex immunohistochemistry ( mihc ) workow34 to quantify the densities of tumor cells , broblasts , and 10 leukocyte subsets ( appendix table a1 )  . 
we selected regions of interest ( rois ) within each section that contained both krt + epithelial or tumor cells and cd45 + immune cells ( appendix fig a1 ) , followed by quantitative assessment of each roi . 
a detailed analysis of leukocyte subsets revealed that cd8 + t cells and cd4 + t cells were signicantly denser in the metastasis from pt1 compared with the primary tumor from pt2 ( fig 3b )  . 
 ( a ) mean cell density per roi for mutually exclusive populations of ki67 + tumor or epithelial cells , ki67neg tumor or epithelial cells , broblasts , and leukocytes . 
among subsets of cd4 + t cells , we found more pro - inammatory th1 t cells in the metastasis from pt1 than either primary tumor ( fig 3c )  . 
within cd4 + t cells , we found a greater density of both cytolytic granzyme b + ( grzb ) cells and proliferative ki67 + cells in the metastasis from pt1 than the primary tumor from pt2 and a higher density of proliferative ki67 + cells in pt1s primary tumor compared with pt2s primary tumor ( fig 3d )  . consistent with the abundant th1 - like macrophages in pt1s primary tumor , we found that the ratio of th1 - like to th2 - like macrophages was signicantly greater in pt1s primary tumor relative to the other 2 tumors ( fig 3e )  . 
a high granulocyte / neutrophil to lymphocyte ratio is associated with poor outcomes.35 , 36 consistent with this , the primary tumor from pt2 had a signicantly higher granulocyte to cd8 + t cell ratio than either tumor from pt1 ( fig 3e )  . 
in addition , across rois , there was no correlation between the densities of cd8 + t cells and granulocytes in the tumors from pt1 , but there was a signicant positive correlation in pt2s primary tumor ( p , .03 , fig 4a )  . 
furthermore , the abundant granulocytes in pt2s tumor were proximal to tumor cells and appeared within lumens ( fig 4b ) where they may contribute to pathogenesis by occluding ducts.37 we also observed tertiary lymph structures ( tlss ) at the border of both primary tumors , but these were more prevalent in the primary tumor from pt1 ( appendix fig a1 )  . 
tlss from pt1 also contained signicantly more b cells , cd4 + t cells , and cd8 + t cells ( appendix fig a2 ) as previously reported for patients with relatively positive outcomes.24 , 38 tissue acquisition and patient consent human tissues were obtained with informed consent in accordance with the declaration of helsinki and were acquired through the oregon pancreas tissue registry under oregon health & science university irb protocol #3609 . discussion we investigated multiple modalities and tumor characteristics of pdac between two related patients . 
we found several similarities between both patients cancers , cluding genes commonly altered in aggressive pdac ( kras , tp53 , and smad439 , 40 ) and a shared prss1 a16v germline mutation that may predispose to pancreatitis41 - 44 but is variably penetrant , 45 raising the possibility that this specic alteration leads to subclinical pancreatitis that accelerates tumorigenesis , consistent with pt2s early onset of disease.41 , 46 the disease course for pt1 was exceptional in the context of occult , chemotherapy - resistant metastatic disease for nearly 4 years . 
an fanca mutation in the metastasis from pt1 might have sensitized that tumor to adjuvant gemcitabine and xeloda and later to sbrt ; however , pt1s lung metastasis progressed during adjuvant chemotherapy , and no adjuvant treatment was given after surgical resection of the lung metastasis , suggesting that the indolent disease might have also been controlled by other factors . 
both tumors from pt2 contained an alteration in cdkn2a , and the metastasis from pt2 had a copy number loss of pten ; alterations in these genes are associated with poor outcomes and drug resistance.47 - 49 pt1s classical subtype tumors and metastases limited to the lungs are both favorable prognostic factors . 
specically , more prevalent tlss at the periphery of the primary tumor ( appendix fig a1 ) and denser cd8 + t cells ( fig 3b ) that did not correlate with the density of granulocytes24 , 50 ( fig 4a ) , opening the possibility that tumor cells and / or cd4 + t cells in pt1s tumors recruit fundamentally different leukocyte cell types from pt2s tumors.51 additionally , granulocytes typically promote immunosuppression in late - stage tumors , 52 consistent with the relatively low number of t cells in pt2s tumor . classical subtype pdac with lung metastases and unconventional tumor immunity may lead to exceptional outcomes . 
sears , phd , brenden - colson center for pancreatic care , oregon health and science university , 2730 s moody ave , portland , or 97201 ; e - mail : searsr@ohsu.edu. support supported by the brenden - colson foundation and nci grant u01 ca224012 to r.c. 
coussens employment : oregon health &amp ; science university ( ohsu ) honoraria : prospect creek foundation , lustgarten foundation for pancreatic cancer research , syndax pharmaceuticals , inc : external advisory board , carisma therapeutics inc : scientic advisory board , verseau therapeutics , inc , scientic advisory board , zymeworks , inc , scientic advisory board , cytomx therapeutics , inc , kineta inc , ( p30 ) koch institute for integrated cancer research , massachusetts inst . 
of tech , ( p30 ) salk institute cancer center , bloomberg - kimmel institute for cancer immunotherapy , sidney kimmel comprehensive cancer center at johns hopkins , dana farber cancer center breast spore , ( p30 ) dana farber / harvard cancer center , ( p30 ) university of california , san diego moores cancer center , starr cancer consortium , lustgarten foundation for pancreatic cancer research , therapeutics working group , nih / nci - frederick national laboratory advisory committee ( fnlac ) , susan g komen foundation , komen scholar consulting or advisory role : cell signaling technologies , pharmacyclics , cytomx therapeutics , syndax , carisma therapeutics , verseau therapeutics , zymeworks , kineta , inc , abbvie , shasqi inc research funding : syndax pharmaceuticals inc , pharmacyclics , cell signaling technologies , innate pharma , deciphera travel , accommodations , expenses : cell signaling technologies , astrazeneca , pharmacyclics , verseau , carisma therapeutics , cytomx therapeutics , zymeworks other relationship : prospect creek foundation , lustgarten foundation for pancreatic cancer research , ( p30 ) koch institute for integrated cancer research , massachusetts inst . 
n engl j med 379 : 2395 - 2406 , 2018 iacobuzio - donahue ca , fu b , yachida s , et al : dpc4 gene status of the primary carcinoma correlates with patterns of failure in patients with pancreatic cancer . j clin oncol 27 : 1806 - 1813 , 2009 yachida s , jones s , bozic i , et al : distant metastasis occurs late during the genetic evolution of pancreatic cancer . 
makohon - moore ap , zhang m , reiter jg , et al : limited heterogeneity of known driver gene mutations among the metastases of individual patients with pancreatic cancer . 
nat genet 49 : 358 - 366 , 2017 katz mhg , wang h , fleming jb , et al : long - term survival after multidisciplinary management of resected pancreatic adenocarcinoma . 
ann surg oncol 16 : 836 - 847 , 2009 downs - canner s , zenati m , boone ba , et al : the indolent nature of pulmonary metastases from ductal adenocarcinoma of the pancreas . 
j surg oncol 112 : 80 - 85 , 2015 deeb a , haque su , olowokure o : pulmonary metastases in pancreatic cancer , is there a survival inuence ? j gastrointest oncol 6 : e48 - e51 , 2015 10 . 
rashid nu , peng xl , jin c , et al : purity independent subtyping of tumors ( purist ) , a clinically robust , single - sample classier for tumor subtyping in pancreatic 34 . 
zhou y , wei q , fan j , et al : prognostic role of the neutrophil - to - lymphocyte ratio in pancreatic cancer : a meta - analysis containing 8252 patients . 
giakoustidis a , neofytou k , costa neves m , et al : identifying the role of neutrophil - to - lymphocyte ratio and platelets - to - lymphocyte ratio as prognostic markers in patients undergoing resection of pancreatic ductal adenocarcinoma . 
herman jm , jabbour sk , lin sh , et al : smad4 loss correlates with higher rates of local and distant failure in pancreatic adenocarcinoma patients receiving adjuvant chemoradiation . 
schubert s , traub f , brakensiek k , et al : cftr , spink1 , prss1 , and ctrc mutations are not associated with pancreatic cancer in german patients . 
mcwilliams rr , maisonneuve p , bamlet wr , et al : risk factors for early - onset and very - early - onset pancreatic adenocarcinoma : a pancreatic cancer casecontrol consortium ( panc4 ) analysis . 
kim m , shah a , zhang j , et al : gemcitabine resistance in cultured pancreatic tumor cells is associated with down regulation of pten and a mesenchymal phenotype . 
ferrer m , de winter jp , mastenbroek dc , et al : chemosensitizing tumor cells by targeting the fanconi anemia pathway with an adenovirus overexpressing dominant - negative fanca . 
ye k , schulz mh , long q , et al : pindel : a pattern growth approach to detect break points of large deletions and medium sized insertions from paired - end short reads . 
exome sequencing libraries were prepared with a kapa hyper prep kit , enriched using the agilent sureselectxt clinical research exome , and paired - end sequenced with an illumina hiseq 2500 to a high depth of 300  . 
rna sequencing was performed as previously reported.62 briey , rna was extracted using an rneasy kit ( qiagen ) and evaluated by the ohsu massively parallel sequencing shared resource ( mpssr ) core facility for library construction with the truseq rna access library prep kit ( illumina )  . 
30% as measured using an agilent 2100 bioanalyzer . rna was sequenced on an illumina hiseq 2500 / 4000 to generate 100 bp paired - end reads for a minimum depth of 40 million reads per sample . 
we followed the published protocol for purist subtyping33 and used the same data set as for pdassigner subtyping . tissue processing and immunostaining tumor tissue samples were xed in 10% neutral buffered formalin for 24 hours and embedded in parafn ( ffpe )  . 
ffpe sections were stained with hematoxylin and eosin , and krt5 was detected with a rabbit monoclonal antibody ( ep1601y , abcam ) and polyclonal goat anti - rabbit antibodies ( invitrogen )  . 
exposure times and signal thresholds were normalized across all images . multiplex immunohistochemistry , image acquisition , and processing multiplex ihc was performed on 5 m ffpe sections using an adapted protocol based on methodology we previously described.34 briey , slides were deparafnized and stained with hematoxylin ( s3301 , dako , santa clara , ca ) , followed by whole slide scanning at 20 magnication on an aperio at2 ( leica biosystems , wetzlar , germany )  . 
slides were digitally scanned following each chromogen development . scanned images were registered in matlab version r2018b using the surf algorithm in the computer vision toolbox ( the mathworks , inc , natick , ma )  . 
image processing and cell quantication were performed using fiji ( fiji is just imagej ) cellproler version 3.5.164 and fcs express 6 image cytometry ruo ( de novo software , glendale , ca )  . aec signal was extracted for quantication and visualization in fiji using a custom macro for color deconvolution . 
 ( a ) krt ( magenta ) and cd45 ( teal ) expression and selected rois ( yellow rectangles ) used for mihc analyses of tumors ( scale bars represent 5 mm )  . 
 o estimated cost of anticancer therapy directed by comprehensive genomic profiling in a single - center study purpose comprehensive genomic profiling ( cgp ) detects several classes of genomic alterations across numerous genes simultaneously and can match more patients with genomically targeted therapies than conventional molecular profiling . 
the current study estimated the costs of anticancer drugs and overall survival ( os ) for patients who were treated with matched and unmatched therapy . methods costs were estimated for patients with complete data ( 188 of 500 patients ) from a prospective , nonrandomized study of patients with diverse refractory cancers who underwent cgp and were treated with matched or unmatched therapy . 
incremental increases in ttf ( + 1.9 months v + 1.2 months ) and observed os ( + 2.5 months v + 2.1 months ) between matched and unmatched therapies were larger for those who underwent cgp in earlierversus later - line therapy . 
incremental increases in drug costs between matched and unmatched therapies were lower for earliercompared with later - line therapy ( + $27 , 000 v + $43 , 000 , respectively )  . conclusion matched therapy was associated with longer ttf , increased os , and manageable incremental cost increases compared with unmatched therapy . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction patients with metastatic cancer who have experienced failure with standard therapy often have few therapeutic options remaining ; however , in recent years , the development of personalized medicine has shifted the oncology treatment landscape . 
this includes the use of next - generation sequencing ( ngs ) platforms that vastly improve dna sequencing efficiency by allowing millions of reactions to occur in parallel.1 - 4 many cancers have been shown to contain genomic alterations that can be targeted by specific therapies . 
most recently , these targeted therapies have become a major area of focus in anticancer drug development.5 - 15 in 2017 , for example , the us food and drug administration ( fda ) added five new targeted drugs and biologics to its list of more than 200 approved anticancer agents.16 , 17 furthermore , recent national comprehensive cancer network clinical practice guidelines in oncology for melanoma and nonsmall - cell lung cancer recommend broad molecular profiling to identify genomic alterations for matched anita chawla filip janku jennifer j . 
 therapy or to appropriately counsel patients with metastatic disease regarding the availability of clinical trials.18 , 19 in addition , the recently developed precision medicine initiative includes the national cancer institute molecular analysis for therapy choice clinical trial , which seeks to determine the effectiveness of genomically targeted therapies.20 furthermore , several prospective pantumor studies using comprehensive genomic profiling ( cgp ) have demonstrated improvements in clinical outcomes for patients who were treated with genomically matched therapy compared with those who received unmatched therapy.7 , 12 , 13 , 21 recent evidence has also suggested that genomic testing at the time of diagnosis of metastatic disease , rather than after one or more lines of systemic therapy , may improve the chances for patients to receive clinically beneficial matched treatment before they undergo a rapid functional decline as they experience disease progression.22 the fda issued its first approval of an ngsbased diagnostic test in december 2016 , the foundationfocus cdxbrca test ( foundation medicine , cambridge , ma ) , which matches patients with advanced ovarian cancer who have either germline ( inherited ) and / or somatic ( acquired ) brca1 / 2 mutation types to treatment with the poly ( adp - ribose ) polymerase inhibitor , rucaparib.23 in addition to testing for individual genomic alterations , use of cgp allows for the detection of four major classes of dna alterations , including base substitutions , copy number alterations , insertions and deletions , and rearrangements . 
collectively , the breadth and accuracy of cgp allow several potential targets for matched therapies to be identified in parallel regardless of anatomic site and without repeated site - specific tests.3 , 4 , 24 therefore , cgp matches more patients with targeted therapies and may mitigate some of the key limitations of conventional molecular testing , including a lack of sufficient tissue because of the need for sequential testing , delays in receiving matched therapy , and an inability to detect actionable alterations.25 - 30 in 2017 , foundationone cdx ( foundation medicine ) , an ngs - based test that detects alterations in 324 genes , select rearrangements , and genomic signatures , such as microsatellite instability ( msi ) and tumor mutational burden ( tmb ) , became the first fda approved broad companion diagnostic for solid tumors . 
although this diagnostic test is newly approved , there is a robust evidence base for the foundationone laboratory - developed test , and the evidence that supports the latter test can be considered transferrable to the fda - approved foundationone cdx . although the clinical utility of genomically matched therapy has been established , questions remain about the value of cgp and the associated costs of targeted therapy . 
the objective of the current study was to estimate anticancer drug costs , time to treatment failure ( ttf ) , and overall survival ( os ) among patients with refractory cancers who had undergone cgp and were either matched or unmatched to targeted therapies . 
 methods patient population our study is a post - hoc retrospective analysis of patients with diverse refractory tumors who were enrolled in a prospective , nonrandomized , phase i oncology center study . 
detailed inclusion criteria have been described elsewhere.10 this study ( clinicaltrials.gov identifier : nct02437617 ) was approved by the md anderson cancer center internal review board , and all patients gave informed consent . 
information collected by study investigators included age , sex , eastern cooperative oncology group performance status , tumor type , number of metastatic sites , and number of prior therapies . 
a drug was considered matched if the half - maximal inhibitory concentration impacted the target at low nanomolar rangefor small - molecule inhibitorsor if the target was the primary one recognized by an antibody . 
additional details on matching definitions are available in the primary clinical study manuscript.10 outcomes we assessed clinical outcomes ttf and os during the observation period as described previously.10 for this retrospective economic analysis , ttf and os were calculated as observed casesthat is , not statistically adjusted . 
mean monthly drug costsadjusted to 2016 usd were imputed for the first regimen used after cgp on the basis of unit costs of the individual drugs or representative agents of the drug classes and their label - based dosing schedules . 
investigational drugs assumed no cost ; administration costs were assumed to be $136.41 on the basis of healthcare common procedure coding system code 96413 for 1 - hour infusion using centers for medicare & medicaid services physician fee schedule . 
total drug and administration costs were calculated as the product of mean monthly drug and administration costs and ttf . statistical analysis the goal of this economic study was to calculate drug - related costs and their association with observed periods of treatment and survival to better understand cost drivers . 
differences between these groups were assessed using t tests . to assess the drivers of drug cost differences between matched and unmatched therapies , the difference was partitioned into two components : the contribution of differences in treatment duration , calculated as the difference in mean durations for matched versus unmatched therapy multiplied by the monthly cost of unmatched therapy , and the contribution of differences in monthly treatment costs , calculated as the difference in monthly drug and administration costs for matched versus unmatched therapy multiplied by the mean duration of matched therapy . 
analyses were conducted for the overall patient and population and also stratified by line of therapy of the first regimen after cgpthat is , earlier - line ( one to three ) versus later - line ( four or later ) therapy . results patient population a total of 500 patients were enrolled . 
 adapted from wheler et al10 with permission from the american association for cancer research . patients who consented to molecular profiling ( n = 500 ) did not undergo molecular profiling insufficient / no tissue died / entered hospice before tissue could be obtained failed report / sequencing commercial ngs performed and therefore excluded not willing to be treated withdrew from study ( n = 161 ) ( n = 111 ) ( n = 37 ) ( n = 6 ) ( n = 4 ) ( n = 2 ) ( n = 1 ) patients who underwent molecular profiling ( n = 339 ) patients with one are more molecular alteration ( n = 322 ) patients with no molecular alteration ( n = 17 ) patients excluded from analysis never received new evaluable treatment after consent hospice / died before treatment could be initiated still on prior therapy lost to follow - up refused watchful waiting only prior immunotherapy action of drug unclear stem - cell transplantation ( n = 134 ) ( n = 124 ) ( n = 79 ) ( n = 32 ) ( n = 8 ) ( n = 4 ) ( n = 1 ) ( n = 6 ) ( n = 3 ) ( n = 1 ) patients included in analysis ( n = 188 ) matched therapy ( n = 122 ) unmatched therapy ( n = 66 ) mostly for reasons of insufficient / no tissue , death , or referral to hospice before tissue could be obtained . 
of the 339 patients who underwent molecular profiling , 322 had at least one genomic alteration detected317 had one or more potentially actionable alterationand 188 received subsequent treatment with either matched ( n = 122 ; 65% ) or unmatched ( n = 66 ; 35% ) therapy10 ( fig 1 )  . 
of the 134 patients with at least one alteration who were not included in the analysis , 124 never received a new evaluable treatment after providing consent , six were excluded as they had received prior immunotherapy , three received a drug with an unclear action , and one underwent stem - cell transplantation.10 median age of treated patients was 59 years ( range , 19 to 82 years ) , with 55% of patients age 60 years and 45% of patients older than age 60 years in both the matched and unmatched therapy groups . 
increased drug treatment costs for matched therapy were largely attributable to a longer duration of therapy ( 66.3% of costs ) , which was associated with longer ttf , rather than higher monthly drug costs ( 33.7% of costs ; fig 2 )  . 
a total of 16 patientsnine who received matched therapy and seven who were unmatchedreceived an investigational agent that was assumed to have no cost ; however , three of these patients received the agent in combination with either one or two costed drugs . earlierversus later - line therapy . 
in addition , the incremental increases in drug costs between matched and unmatched therapies were lower for earlier - compared with later - line therapy ( approximately $27 , 000 v $43 , 000 ; table 2 )  . 
this was a result , in part , of the use of more costly regimens for later - line therapy , including more frequent use of combination therapies ( 77.8% in later line therapy v 58.5% in earlier - line therapy )  . most of the incremental increases in drug treatment costs between matched and unmatched therapies were attributable to a longer time on treatment and survival in both earlierand later line therapies ( 87% and 58% of costs , respectively ; fig 2 )  . 
in addition , the contributions of monthly drug costs to overall anticancer drug costs were much lower in earlierversus later line therapies ( 13% v 42% , respectively )  . discussion to our knowledge , this is the first study to report anticancer drug costs for matched and unmatched therapies in patients with refractory cancer who have undergone cgp . 
patients who were treated with matched therapy generally had a longer time on treatment , greater observed os , and higher anticancer drug costs compared with those on unmatched therapy . 
it is also notable that patients in the matched group experienced these improved outcomes despite having an approximately 6 - month lower median ttf on their prior therapy compared with the unmatched group , which suggests that their disease had been comparatively less responsive to the last line of treatment these patients had received . 
the benefits of matched therapy may therefore outweigh the increased costs . in addition , our analysis found more promising outcomes for matched therapies when administered to a patient population undergoing cgp in earlier lines of therapy . 
similar to the analysis conducted on the full sample , most of the incremental increases in drug treatment costs were attributable to longer ttf and survival in both earlierand later - line therapies . 
because incremental costs were numerically lower per patient in the earlierversus later - line group , despite their increased os and ttf , these findings suggest that earlier use of cgp could enable matching to effective treatment options that have lower costs than those used in later lines . higher anticancer drug costs for matched therapy have been reported elsewhere.32 in this study , however , the observed high costs may have been a result of patients undergoing cgp in lateras opposed to earlier - line therapies , as more than 93% of the patient population had previously received chemotherapy or a targeted therapy . 
 furthermore , the study authors did not detail the individual factors that underpinned anticancer costs , such as a longer time on treatment , which represented 66.3% of the cost increase in our study , rather than higher monthly drug costs . limitations although this retrospective study estimates the anticancer drug costs associated with matched and unmatched therapies , its contribution must be balanced with the limitations of the data . 
it is also important to note that care at a phase i clinic at a premier care center may not represent the level of drug treatment accessible to patients in community practice , especially those who receive later lines of therapy . 
of note , tmb , which can be assessed using foundationone and foundationone cdx , has recently been shown to be predictive of outcomes among patients who are administered checkpoint inhibitors.35 indeed , both tmb and msi were not well - established as markers for targeted therapy during the time period of the phase i study , 10 whereas pembrolizumab is now approved for patients with unresectable or metastatic solid tumors with msi high or mismatch repair deficiency . 
 ( c ) patients with four or more lines of prior therapy . 80 , 000 60 , 000 40 , 000 20 , 000 80 , 000 60 , 000 40 , 000 20 , 000 80 , 000 60 , 000 40 , 000 20 , 000 30 , 664 12 , 825 25 , 240 68 , 729 unmatched therapy monthly drug costs ( matched therapy ) longer duration of therapy matched therapy 34 , 527 3 , 568 23 , 745 61 , 840 unmatched therapy monthly drug costs ( matched therapy ) longer duration of therapy matched therapy 17 , 954 29 , 323 24 , 939 72 , 216 unmatched therapy monthly drug costs ( matched therapy ) longer duration of therapy matched therapy increased clinical utility as more patients have the opportunity to become matched to targeted therapy . in addition , this analysis included phase i drugs that may not have engaged the target or had poor pharmacokinetics , and patients who received all dose levels were also included , which may reduce the positive effect of treatment.10 furthermore , drug acquisition and administration costs were estimated on the basis of list prices and durations of therapy , and costs for medical services were not included . 
our analysis was also limited by the relatively high number of patients who could not be administered therapy during the study as a result of the unpredictable and rapid disease course of refractory cancers . 
among included patients , it was not possible to separate out the possible impacts of line of therapy and performance status on the differential os and ttf findings.10 finally , patients were assumed to take the dose of each drug according to the prescribing information , which would not account for potential dose reduction in combination therapies . in conclusion , cgp is useful for selecting patients with refractory tumors to receive matched therapy . 
miller , rachel anhorn , zhou zhou , james signorovitch manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors vincent a . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : foundation medicine travel , accommodations , expenses : foundation medicine rachel anhorn employment : foundation medicine , pfizer stock and other ownership interests : foundation medicine zhou zhou employment : analysis group james signorovitch employment : analysis group acknowledgment the analysis presented in this article was conducted by analysis group , which received consulting fees from foundation medicine . 
we thank tim peoples , marcia reinhart , cody patton , and erica birk of analysis group for medical writing and editorial assistance . anita chawla employment : analysis group leadership : cytrx corporation stock and other ownership interests : cytrx corporation filip janku stock and other ownership interests : trovagene consulting or advisory role : deciphera , trovagene , novartis , sequenom , foundation medicine , guardant health , immunome research funding : novartis , biomed valley discoveries , roche , agios , astellas pharma , deciphera , symphony evolution , plexxikon , piqur , fujifilm other relationship : bio - rad support funded by foundation medicine . prior presentation references presented at the 2017 asco annual meeting , chicago , il , june 2 - 6 , 2017 . affiliations anita chawla , zhou zhou , and james signorovitch , analysis group , boston ; vincent a . 
singh rr , patel kp , routbort mj , et al : clinical validation of a next - generation sequencing screen for mutational hotspots in 46 cancer - related genes . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular profiling of patients tumors to find potential targets and select treatments for their refractory cancers . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
johnson db , dahlman kh , knol j , et al : enabling a genetically informed approach to cancer medicine : a retrospective evaluation of the impact of comprehensive tumor profiling using a targeted next - generation sequencing panel . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
levy bp , chioda md , herndon d , et al : molecular testing for treatment of metastatic non small - cell lung cancer : how to implement evidence - based recommendations . 
ali sm , hensing t , schrock ab , et al : comprehensive genomic profiling identifies a subset of crizotinib - responsive alk - rearranged non - small cell lung cancer not detected by fluorescence in situ hybridization . 
drilon a , wang l , arcila me , et al : broad , hybrid capture - based next - generation sequencing identifies actionable genomic alterations in lung adenocarcinomas otherwise negative for such alterations by other genomic testing approaches . 
rankin a , klempner sj , erlich r , et al : broad detection of alterations predicted to confer lack of benefit from egfr antibodies or sensitivity to targeted therapy in advanced colorectal cancer . 
schrock ab , frampton gm , herndon d , et al : comprehensive genomic profiling identifies frequent drug - sensitive egfr exon 19 deletions in nsclc not identified by prior molecular testing . 
pags a , foulon s , zou z , et al : the cost of molecular - guided therapy in oncology : a prospective cost study alongside the moscato trial . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
handorf ea , mcelligott s , vachani a , et al : cost effectiveness of personalized therapy for firstline treatment of stage iv and recurrent incurable adenocarcinoma of the lung . 
 appendix tumor type adenoid cystic breast colorectal cup esophageal gi , anus gi , stomach gi , other gyn , other hepatocellular head and neck lung melanoma neuroendocrine ovarian prostate renal sarcoma thymic thyroid uterine other table a1 . 
 biallelic deletion of palb2 occurs across multiple tumor types and suggests responsiveness to poly ( adp - ribose ) polymerase inhibition background with brca1 / 2 , palb2 ( a partner and localizer of brca2 ) plays a critical role in the dna - damage response pathway . 
palb2 is required for homologous recombination repair , and formation of the brca1 - palb2 - brca2 complex is essential for recruitment of rad51 to sites of dna damage.1 - 3 palb2 stabilizes brca2 and promotes its localization within the nucleus . 
dna repair pathways are disrupted in palb2 - deficient cells , thereby accounting for the tumor suppressor gene properties of palb2.1 , 2 monoallelic loss - of - function mutations in palb2 increase the risk of breast and pancreatic cancers . deleterious mutations in palb2 have been reported in 1% to 2% of familial breast and in 2% to 5% of familial pancreatic cancer syndromes.4 - 8 mutations in palb2 are associated with increased risk of male breast cancer , 9 prostate cancer , 10 gastric cancer , 11 and ovarian cancer.12 biallelic mutations in palb2 are less common and are linked to fanconi anemia.13 although heterozygous mutations in palb2 have been well characterized , homozygous deletions of palb2 have not been previously described . to our knowledge , we present the first published series of palb2 biallelic gene deletions across multiple tumor types . 
in absence of a standard of care , tumor tissue was submitted for comprehensive genomic profiling ( cgp ) .14 two genomic alterations were identified , including a biallelic palb2 gene deletion involving exons 8 to 10 as well as apc p.h785fs * 1 ( table 1 ; fig 3 )  . after providing informed consent , the patient was treated off label with olaparib ( lynparza ; astrazeneca , london , united kingdom )  . 
he was treated in accordance with the declaration of helsinki . restaging ct after 3 months revealed resolution of the primary pancreatic mass and significant reduction in size and number of hepatic metastases ( figs 2b and 2e )  . 
1 year after treatment initiation . palb2 genomic loss across tumor types to identify additional patients who may benefit from parp inhibition , we examined a large genomic sequencing database containing  . 
liver metastases at presentation were refractory to chemoembolization ( d ) but demonstrated durable response to olaparib ( e and f )  . gene deletions involving exons 1 to 13 ( fig 3 )  . 
the remaining 12 tumor samples harbored partial exonic deletions ( fig 3 ; table 1 )  . the majority of samples ( 77% ) involved the c - terminal wd40 domain of palb2 , which mediates interaction between palb2 and brca2 . there were insufficient numbers to assess cooccurrence or mutual exclusivity ; the most common associated gene defects involved tp53 ( 33% , six of 18 ) , cdkn2a ( 28% , five of 18 ) , and cdkn2b ( 22% , four of 18 )  . 
interestingly , the median tumor mutational burden ( tmb ) was low , at 3.47 mutations per dna megabase , among patients in our series ( table 1 )  . 
all homozygous deletions would be predicted to result in loss of function of palb2 . these mutations were previously detected in the cancer genome atlas but have not been specifically reported in the literature . discussion herein , to our knowledge , we report the first series to examine large genomic deletions in palb2 and provide indirect clinical evidence for responsiveness to parp - inhibitor therapy . 
 ( c ) the location of biallelic deletions observed across 18 samples identified by comprehensive genomic profiling are shown . 1 2 3 10 11 binding chan binding mrg15 wd40 methods such as multiplex ligation - dependent probe amplification , quantitative polymerase chain reaction , or comparative genomic hybridization.24 cgp has been demonstrated to be an effective means of identifying large genomic rearrangements.12 the functional domains of palb2 have been well characterized , with loss - of - function mutations linked to multiple cancer types.7 , 12 , 23 the recruitment of brca2 to sites of dna damage is dependent on the presence of a normally functioning palb2 . 
the c - terminal wd40 domain of palb2 , encoded by exons 7 to 13 , mediates the protein protein interactions among palb2 , brca2 , and rad51c ( fig 3 ) .25 truncation or frameshift mutations of the wd40 domain of palb2 disrupts this interaction and is associated with increased genomic instability.2 , 10 , 17 large - scale deletions of these exons is predicted to manifest similarly as a loss of function . although rare , biallelic palb2 deletions involving regions encoding important functional domains may have important clinical implications . orthogonal preclinical support for this observation includes palb2 - deficient tumor cells exhibiting diminished activity of homologous recombination and impaired dna damagerepair pathways.26 loss of functional palb2 is associated with sensitivity to dna - damaging agents1 , 27 and parp inhibitors.3 , 28 functional short interfering rna mediated palb2 knockdown is known to sensitize cell lines to parp inhibitors.3 , 26 the efficacy of olaparib in homologous recombinationdeficient cells is postulated to result from synthetic lethality , in which parp inhibition induces single - strand dna breaks . 
cells deficient in homologous recombination are more susceptible to induced dna damage , thereby leading to selective cell death of tumor cells.29 clinical data supporting the role of palb2 as a predictive biomarker are limited . 
durable benefit from olaparib in a patient with metastatic prostate cancer and heterozygous palb2 gene deletion30 and a case of palb2 - mutant pancreatic cancer treated with mitomycin c have been reported.31 because it is not yet known , further study is warranted to determine how closely the palb2 alterations described thus far share traits with cancers defined by brcaness . 
similarly , palb2 alterations are not part of current homologous recombination deficiency assays . pseudopapillary neoplasm of the pancreas is a rare epithelial tumor comprising 1% to 2% of exocrine pancreatic neoplasms.32 these tumors generally present as large encapsulated masses , although metastatic disease has been reported . 
 tumor - specific and actionable drug targets for uncommon neoplasms . would be needed to address the functional relevance of lower tmb in our data set . the median tmb in our series was low , at 3.47 mutations per dna megabase , which is an unanticipated finding . 
an analysis of ovarian cancer cases from the cancer genome atlas revealed a slightly higher tmb among brca1 / 2 - mutant tumors compared with wild - type tumors , although a subset of brca - mutant , low - tmb patients was observed.36 increased tmb is hypothesized to result from an increased propensity for error in cells deficient in homologous recombination . the genomic characteristics of homologous recombination deficiency are a broader loss of heterozygosity and aneuploidy , whereas tmb is broadly derived from counting short insertions and deletions ( indels )  . 
unfortunately , other patients in our series did not receive parp - inhibitor therapy , and clinical responses tmb is a putative predictive biomarker for immune checkpoint inhibitor responsiveness , and preclinical work suggests synergy between immunotherapy and veliparib in brca - deficient models.37 , 38 although more prospective study is needed , deleterious biallelic palb2 loss may identify a subset of patients for whom parp - inhibitor monotherapy and / or combinatorial strategies with radiation ( eg , nct01908478 ) , immunotherapies ( eg , nct02571725 ) , and / or synthetic lethal dnadamaging agents ( eg , nct02308072 ) is warranted . our series provides support for incorporating cgp in the therapeutic algorithm for patients for whom standard - of - care therapies are lacking . 
ali employment : foundation medicine stock and other ownership interests : exelixis , foundation medicine , epizyme patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on the microbiome in non - neoplastic disease ( i ) samuel j . 
klempner honoraria : foundation medicine consulting or advisory role : eli lilly , boston biomedical , celgene speakers bureau : foundation medicine travel , accommodations , expenses : eli lilly 1 . 
buisson r , dion - c ote a - m , coulombe y , et al : cooperation of breast cancer proteins palb2 and piccolo brca2 in stimulating homologous recombination . 
couch fj , hart sn , sharma p , et al : inherited mutations in 17 breast cancer susceptibility genes among a large triplenegative breast cancer cohort unselected for family history of breast cancer . 
ding yc , steele l , kuan cj , et al : mutations in brca2 and palb2 in male breast cancer cases from the united states . breast cancer res treat 126 : 771 - 778 , 2011 10 . 
lu c , xie m , wendl mc , et al : patterns and functional implications of rare germline variants across 12 cancer types . nat commun 6 : 10086 , 2015 12 . 
walsh t , casadei s , lee mk , et al : mutations in 12 genes for inherited ovarian , fallopian tube , and peritoneal carcinoma identified by massively parallel sequencing . 
pylkas k , erkko h , nikkila j , et al : analysis of large deletions in brca1 , brca2 and palb2 genes in finnish breast and ovarian cancer families . 
janatova m , kleibl z , stribrna j , et al : the palb2 gene is a strong candidate for clinical testing in brca1and brca2 - negative hereditary breast cancer . 
blanco a , de la hoya m , balma~na j , et al : detection of a large rearrangement in palb2 in spanish breast cancer families with male breast cancer . 
tischkowitz md , sabbaghian n , hamel n , et al : analysis of the gene coding for the brca2 - interacting protein palb2 in familial and sporadic pancreatic cancer . 
foulkes wd , ghadirian p , akbari mr , et al : identification of a novel truncating palb2 mutation and analysis of its contribution to early - onset breast cancer in french - canadian women . 
shen y , rehman fl , feng y , et al : bmn 673 , a novel and highly potent parp1 / 2 inhibitor for the treatment of human cancers with dna repair deficiency . 
villarroel mc , rajeshkumar nv , garrido - laguna i , et al : personalizing cancer treatment in the age of global genomic analyses : palb2 gene mutations and the response to dna damaging agents in pancreatic cancer . 
ji s , xu j , zhang b , et al : management of a malignant case of solid pseudopapillary tumor of pancreas : a case report and literature review . 
huang j , wang l , cong z , et al : the parp1 inhibitor bmn 673 exhibits immunoregulatory effects in a brca1 ( - / - ) murine model of ovarian cancer . 
2 , 3 we used our recently reported in silico tool ( dpyd - varifier ) 7 to predict that p.t132a would be deleterious to function , which was subsequently validated using ex vivo and in vitro approaches . 
these methodologies permitted us to determine an activity score for the patient that was used to calculate a safe adjusted dose of fu for adjuvant therapy . this study was approved by the mayo clinic institutional review board . 
dpyd - varifier was used to predict the function of p.t132a.7 the effect of p.t132a on dpd activity was measured in vitro as previously described.5 - 7 total rna was isolated from the patients blood sample using the paxgene blood rna kit ( preanalytix , hombrechtikon , switzerland ) , and cdna was reverse transcribed using oligo ( dt ) 15 primers ( thermo fisher scientific , waltham , ma )  . 
the full - length dpyd open reading frame was amplified ( primers : 5 - gtttgtcactggcagactcg - 3 , 5 - ttcacagcaactgtttcacaaa - 3 ) using q5 high fidelity dna polymerase ( new england biolabs , ipswich , ma )  . 
the polymerase chain reaction ( pcr ) product was cloned into the pjet1.2 vector , and 20 cloned constructs were sequenced at the mayo clinic gene analysis shared resource to determine the cis or trans conformation of the variants . 
peripheral blood mononuclear cells ( pbmcs ) were isolated and assessed ex vivo for dpd activity as previously described.9 , 10 additional pcr and quantitative pcr reactions were performed with primers specific to canonically ( e13 / 14 : 5 - ctcttgataaggacattgtgacaaa - 3 , 5 - tttgcagctcttgcgatgc - 3 ) and alternatively spliced dpyd ( e13 / 15 : 5 - ctcttgataagattgtgattgctagc - 3 , 5 - tttgcagctcttgcgatgc - 3 )  . 
 patient presentation ( bowel function alteration and red blood cell per rectum ) colonoscopy pathology staging ct scan 1st cycle began toxicity symptoms dose reduction 2nd cycle radiotherapy only radiotherapy completed 1st cycle began ( reduced mfolfox6 ) 46 - hour infusion 2nd cycle 4th cycle ( dose increased ) 5th cycle ( initial dose ) 8th cycle 10th cycle in silico prediction , ex vivo , and in vitro dpd assay , clonal rna sequencing dpyd sequencing ( mayo medical lab ) blood sample collection surgical resection diagnostic tests neoadjuvant cape + radio variants testing adjuvant mfolfox6 30 34 543 635 no . 
a 32 - year - old male with a history of gastroesophageal reflux and hyperlipidemia presented with altered bowel function and bright red blood per rectu colonoscopy revealed a polyp in the cecum and a mass approximately 10 cm within the rectosigmoid colon . 
a staging computed tomography scan of the chest , abdomen , and pelvis showed no evidence of distal metastases , which suggested stage iii disease . the patient was treated shortly after diagnosis with neoadjuvant therapy that consisted of capecitabine ( 825 mg m2 for 5 days each week ) and radiotherapy ( 50.4 gy in 28 fractions )  . 
 during hospitalization , absolute neutrophil count decreased to 700 cells / l ( normal reference range , 1 , 500 to 8 , 000 cells / l ) , which prompted discontinuation of therapy late in the second week of treatment . 
one and a half months after surgery , the patient was scheduled to begin modified infusional fu , leucovorin , and oxaliplatin ( mfolfox6 ) adjuvant therapy . because of the severe toxicity during the initial neoadjuvant therapy , genetic testing was ordered . 
dpd activity in the patients pbmcs was reduced by 64% ( 92.4 pmol fu min1 mg1 ) compared with previously reported reference values obtained from individuals who do not carry a deleterious dpyd variant10 ( 254.0 pmol fu min1 mg1 ; fig 2a )  . 
to determine whether allelic imbalance of dpyd was occurring , allele - specific pcr primers e13 / 14 and e13 / 15 were used to amplify canonical and alternatively spliced dpyd ( fig 2b , top )  . 
 ( a ) dihydropyrimidine dehydrogenase ( dpd ) enzyme activity was measured in peripheral blood mononuclear cells isolated from the patient and was compared with reference values previously published by our laboratory for peripheral blood mononuclear cells from individuals who do not carry known deleterious variants in dpyd ( noncarriers ) and those heterozygous for * 2a ( * 2a / wild type [ wt ] ) .10 ( b ) polymerase chain reaction primers were designed as indicated ( arrows ) to amplify across the exon 13 / 14 and 13 / 15 junctions to detect the presence of alternative splicing in the patient and a heterozygous carrier of * 2a . 
this level of reduction is similar to that observed for the well - studied p.d949v variant5 , 7 ; thus , the dpd activity score would be expected to be similar . 
finally , the decision was made to administer two additional cycles of therapy that did not contain oxaliplatin because of accumulating grade 1 neuropathy ( fig 1 , gold box )  . 
the patient has completed the 10th cycle of adjuvant therapy and has responded well to the treatment with no severe toxicity and no physical evidence of cancer progression . discussion this report outlines the effective management of toxicity in a patient with rectal cancer treated with an fu - based regimen using a precision oncology approach . 
to date , genetic testing of dpyd variants is not mandated in the united states , and complete dpd deficiency is only listed as a contraindication to fu treatment.11 many studies have increasingly performed functional characterizations of dpyd variants , 3 , 5 - 7 , 9 , 10 , 12 , 13 and the clinical pharmacogenetics implementation consortium has published activity - based fu dosing guidelines for many of the reported dpyd variants.8 however , a paucity of information exists with respect to fu dose adjustments in compound heterozygous variant carriers . in this case report , dpyd genotype and variant function data were used to provide guidance for adjuvant fu dosing in a patient who carries a complex dpyd genotype that includes a novel variant of unknown significance . 
the 38% reduction in in vitro dpd function attributed to p.t132a also is consistent with the approximately 36% activity measured in the patients pbmcs because the p.t132a variant in the patients genome is present in a compound complex heterozygous state ( trans ) with dpyd * 2a . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . shikshya shrestha no relationship to disclose colbren ( scout ) trogstad - isaacson no relationship to disclose timothy j . 
lee am , shi q , pavey e , et al : dpyd variants as predictors of 5 - fluorouracil toxicity in adjuvant colon cancer treatment ( ncctg n0147 )  . 
meulendijks d , henricks lm , sonke gs , et al : clinical relevance of dpyd variants c.1679t > g , c.1236g > a / hapb3 , and c.1601g > a as predictors of severe fluoropyrimidine - associated toxicity : a systematic review and meta - analysis of individual patient data . 
offer sm , wegner nj , fossum c , et al : phenotypic profiling of dpyd variations relevant to 5 - fluorouracil sensitivity using real - time cellular analysis and in vitro measurement of enzyme activity . 
lee am , shi q , alberts sr , et al : association between dpyd c.1129 - 5923 c > g / hapb3 and severe toxicity to 5 - fluorouracil - based chemotherapy in stage iii colon cancer patients : ncctg n0147 ( alliance )  . 
 genomic and proteomic alterations in desmoplastic small round bluecell tumors purpose desmoplastic small round blue - cell tumors ( dsrcts ) are sarcomas that contain the t ( 11 ; 22 ) ( p13 ; q12 ) translocation ews - wt1 fusion protebecause this is a rare tumor type , prospective clinical trials in dsrct are challenging . 
patients are treated in a manner similar to those with ewing sarcoma ; however , differences in prognosis and clinical presentation suggest fundamental differences in biology and potentially different therapeutic implications . 
 methods thirty - five dsrct tumors were assessed using next - generation sequencing , protein expression ( immunohistochemistry ) , and gene amplification ( chromogenic in situ hybridization or fluorescence in situ hybridization )  . 
independent analysis by rna sequencing confirmed higher ar expression from an independent data set of ews - wt1 fusionpositive dsrcts compared with ewing sarcoma and a pan - cancer analysis . 
dsrcts had somatic mutations that were identified in tp53 and foxo3 , averaged five mutations per megabase , and no programmed death - ligand 1 expression was detected in any dsrct samples . 
2018 by american society of clinical oncology ajaz bulbul john paul shen joanne xiu pablo tamayo hatim husain author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : hatim husain , md , university of california san diego , 3855 health sciences #3011 , la jolla , ca 92093 ; e - mail : hhusain@ucsd.edu. introduction desmoplastic small round blue - cell tumors ( dsrcts ) originate from a cell with multilineage potential and are defined by a molecular hallmark with ews - wt1 reciprocal translocation.1 dsrcts are rare , highly aggressive mesenchymal tumors , with only 200 to 450 affected patients with the disease described to date.1 , 2 ewing sarcoma and dsrcts are treated in a similar manner in the clinic ; however , dsrcts have been represented in limited numbers in sarcoma studies . 
the clinical presentations of these diseases are different , with important comparisons being the site of disease presentation and poor prognosis in dsrct groups . despite aggressive therapy , median survival ranges from 17 to 25 months , 2 , 3 and the 5 - year survival rate remains around 15%3 with higher survival reported among those who underwent removal of at least 90% of the tumor with an absence of extraperitoneal metastasis.4 almost all of these tumors contain the t ( 11 ; 22 ) ( p13 ; q12 ) translocation that fuses ews with wt1 leading to production of a chimeric protein with transcriptional regulatory activity . 
 and pelvic cavity of young adult men in 88% to 97% of cases , 2 , 5 whereas ewing sarcoma commonly occurs in the axial skeleton.7 despite similar histologic morphology , differences in disease presentation and prognosis likely reflect the impact of different biologic factors , including differences in the transcriptional effects of the ews - wt1 fusion relative to the ews - fli1 fusion observed in ewing sarcoma . although there is no standard clinical management strategy for dsrct , treatment usually includes neoadjuvant high - dose cyclophosphamide , doxorubicin , and vincristine , alternating with ifosfamide and etoposide chemotherapy combined with aggressively attempted r0 resection.4 , 8 , 9 recent accelerated us food and drug administration ( fda ) approval in october 2016 of the compound olaratumab , a platelet - derived growth factor receptor a inhibitor , was based on a highly significant improvement in overall survival of 26.5 months in soft tissue sarcomas of histologic subtypes for which an anthracycline containing regimen may be appropriate . 
however , only one patient in the phase ii olaratumab study had round blue - cell sarcoma , and that patient was negative for the ews translocation.10 patients with dsrcts are poorly represented in clinical trials as a result of the rare nature of the disease . 
a list of ongoing clinical trials in this disease is provided in the data supplement . the aim of the current study was to understand the molecular characteristics of dsrcts by analyzing 35 patients with molecularly and immunohistochemically profiled tumors and to compare these with ewing sarcoma to explore therapeutic options and potential oncogenic vulnerabilities for this extremely rare and aggressive cancer type . 
dna from formalin fixed , paraffin - embedded samples was sequenced using the nextseq ( 592 genes selected on the basis of the cosmic database ; agilent sure select xt ; illumina , san diego , ca ) and miseq ( 47 genes ; truseq ) , to evaluate mutation and gene amplification . 
the full list of markers surveyed is available.11 twenty - four tumors were sequenced with the 45 - gene panel , and 11 tumors were sequenced with the 592 - gene panel . 
additional data for ar and epidermal growth factor receptor ( egfr ) ihc in other tumors , including prostate cancer , lung cancer , breast cancer , kidney cancer , endometrial cancer , and glioblastoma , were obtained from a larger cohort of 127 , 000 pan - cancer tumor samples analyzed . we used 2 tests for comparison , and statistical significance was determined as p < .05. 
 ( a ) enrichment scores ( single - sample gene set enrichment analysis ) of selected transcriptional signatures across alveolar rhabdomyosarcoma , desmoplastic small round blue cell tumors , ewing sarcoma , and synovial sarcoma . 
desmoplastic small round blue - cell tumor ( dsrct ) sarcomas are clearly overenriched in androgen receptor ( ar ) , epidermal growth factor receptor ( egfr ) , and ews - wt1 ( kts positive / negative ) signatures compared with those of other sarcomas . 
arms , alveolar rhabdomyosarcoma ; es , ewing sarcoma ; ss , synovial sarcoma . the degree to which the genes in a particular gene set are coordinately upregulated or downregulated within each sample . 
in this manner , ssgsea projects a single sample gene expression profile from the space of single genes onto the space of gene sets . the signature for ar is the hallmark_ androgen_response gene set from the molecular signatures database hallmark subcollection.13 the egfr signature corresponds to the egfr_up.v1_up / dn gene sets from the molecular signatures database subcollection c6.14 the ews - wt1 ( kts positive / negative ) signatures were generated from the geo data set gse53301.15 the ews - fli1 signature was made from the 20 genes listed in figure 1 from mendiola et al.16 transcriptional data sets the multiple sarcoma data set shown in figure 1a is a subset of the data set from filion et al.17 sarcoma samples in figure 1b are the dsrct subset from filion et al.17 prostate samples , shown in figure 1b , consisted of 22 primary prostate cancer samples from the geo data set gse32269.18 endometrial samples are 30 samples from the endometrial cancer data set from raeder et al.19 glioblastoma multiforme samples consisted of a subset of 30 samples from the glioblastoma multiforme data set from verhaak et al.20 results demographic data from the 35 patients whose tumors underwent clinical molecular testing are provided in the data supplement . 
 ( a ) thirty - five desmoplastic small round blue - cell tumors ( dsrcts ) went through molecular profiling using a commercial , multiplatform profiling service ( caris life sciences )  . 
specific tests performed included sequencing ( next - generation sequencing [ seq ] ) , protein expression ( immunohistochemistry [ ihc ] ) , and gene amplification ( chromogenic in situ hybridization or fluorescence in situ hybridization [ ish ] )  . 
 patients with ewing sarcoma had lung and bone involvement , which is consistent with the known distribution pattern of these tumors.21 in the 35 dsrcts , increased expression of top2a was observed in 63% of cases , topo1 in 63% , pten in 62% , ar in 59% , and egfr in 42% of tumors . 
increased expression of tubb3 was observed in 56% of tumors , mgmt in 55% , ts in 52% , rrm1 in 43% , and ercc1 in 24% ( fig 2a )  . 
comparing dsrcts with ewing sarcoma tumors , we found that both ar ( 59% v 3% ; p = 1.7e10 ) and tubb3 ( 56% v 29% ; p = .03 ) were expressed in significantly more dsrcts ( fig 2b )  . 
a full list of all of the patients with ihc staining is provided in the data supplement , which includes a description of staining thresholds . given that both the ar and egfr pathways can be effectively targeted with fda - approved drugs , we sought to further evaluate the activity of these pathways in dsrcts . 
we obtained gene expression profiles for 28 dsrcts as well as profiles for ewing sarcoma , alveolar rhabdomyosarcomas , and synovial sarcoma for comparison with other primitive sarcomas.17 performing ssgsea , we found that the majority of dsrcts was enriched for the ar signature , which indicated that these tumors coordinately upregulated genes that are known to be highly expressed when the ar pathway is activated ( fig 1a )  . 
as expected , ewing sarcoma tumors were enriched for the ews - fli1 signature , and dsrcts were enriched for the ews - wt1 signature , which is consistent with the translocation event pathognomonic for each tumor . to evaluate the significance of ar pathway activation in dsrcts , we made comparisons with tumors that are known to be driven by the ar pathway . 
compared with 59% ar expression in dsrct , ihc results indicated that ar expression was most frequent in prostate cancer ( 94% [ n = 1 , 340 tumors ] ) ; however , dsrct was greater than any other tumor type , including breast cancer ( 50% [ n = 1 , 962 tumors ] ) , kidney cancer ( 30% [ n = 40 tumors ] ) , and the pan - cancer analysis , which demonstrated < 30% expression ( n = 127 , 000 )  . 
a pan - cancer analysis of egfr expression demonstrated a percentage of expression ( 53% [ n > 20 , 000 ] ) that was similar to the 42% observed in dsrct . 
furthermore , tubb3 expression ( 51% [ n = 66 , 000 ] ) and top2a ( 69% [ n = 77 , 000 ] ) was similar to that observed in dsrct . pd - l1 expression ( sp142 ) was not detected in tumors tested ( zero of four ) , whereas programmed death 1 ( pd - 1 ) staining on tumor infiltrating lymphocytes ( tils ) was found in 25% of tumors tested ( two of eight )  . 
pd - l1 expression on tumor cells in ewing sarcoma was absent ( zero of 10 ) , and pd - 1 expression on tils was observed in 32% ( six of 19 ) of ewing sarcoma tumors ( fig 2 )  . 
tumor mutational load was calculated in 11 ewing sarcoma tumors , and mean tumor mutational load was five mutations per megabase ( range , three to eight mutations )  . next - generation sequencing revealed a synonymous tp53 g245g mutation and a foxo3 mutation ( l382fs ) in dscrt , whereas six tp53 mutations ( 13% ) , two apc mutations ( l1129s and i1307k ) , one brca1 ( c.301 + 1g > a ) , and one ctnnb1 ( t41a ) mutation were identified in ewing sarcoma . 
there was no copy number amplification identified in dsrct samples for cmet , her2 ( human epidermal growth factor receptor 2 ) , and egfr with in situ hybridization ( data supplement )  . discussion our understanding of the biology of dsrcts and their distinction from other sarcomas is evolving . 
 apart from the canonical ews - wt1 fusion , some major differences between dsrct and ewing sarcoma reflect those between ar and egfr expression . significantly higher ar expression in dsrcts compared with ewing sarcoma tumors suggest the possibility of a mechanistic link between ews - wt1 activation and androgen receptor expression . 
various ews - wt1 proteins regulate the promoter activity of egr - 1 , a zinc finger transcription factor that contributes to ar pathway activation.25 , 26 egr - 1 knockdown by small interfering rna inhibited activity of the ar signaling pathway.27 evidence for ar activation in dsrcts was observed by ihc as well as the coordinate regulation of the ar - responsive transcriptome . 
the degree of ar enrichment in dsrcts was higher than that of many other tumors , and additional work is needed to understand the clinical sensitivity of these tumors to ar inhibition . fda - approved novel ar inhibitors , including enzalutamide , and cyp17a1 inhibitors , including abiraterone , will need to be explored and provide a potential opportunity for continued drug expansion in this space . 
the three patients who had benefit from complete androgen blockade ( cab ) had normal testosterone levels before cab , whereas the three who did not experience a response had baseline castrate levels of testosterone.28 in vitro studies that evaluated the functional status of ar using western blot analysis and the stimulation of growth by dihydrotestosterone in mtt calorimetric assays in 27 patient tumors suggested that ar in dsrcts is functional , and inhibition of basal and testosterone - stimulated growth by flutamide could be achieved.28 a phase ib study in prostate cancer has combined treatment with enzalutamide and docetaxel chemotherapy and has resulted in a 50% decline from baseline in prostate - specific antigen in 19 of 20 patients , and a phase ii study is ongoing in prostate cancer ( clinicaltrials.gov identifier : nct02685267 ) .29 given the poor outcomes found with conventional therapy , the role of combinatorial therapy with ar inhibitors alone or in combination with chemotherapy in dsrtc deserves additional clinical investigation . tumor mutational load may affect response rates to immunotherapy in melanoma and nonsmallcell lung cancers.30 unfortunately , single - agent antipd - 1 antibodies , to date , have had limited efficacy across sarcomas , and an ongoing phase ii study ( sarc028 ) is evaluating the role of pembrolizumab across various sarcoma histologies ( clinicaltrials.gov identifier : nct02301039 ) .31 none of the patients in our cohort had identifiable tumoral pd - l1 expression by sp142 antibody testing , and the significance of pd - 1 positive tils is unclear at this time . in conclusion , there are distinguishing molecular characteristics between dsrcts and ewing sarcoma . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ajaz bulbul consulting or advisory role : pfizer , astrazeneca travel , accommodations , expenses : pfizer , astrazeneca joanne xiu employment : caris life sciences pablo tamayo no relationship to disclose hatim husain consulting or advisory role : astrazeneca , abbvie , foundation medicine speakers ' bureau : astrazeneca , merck , bristol - myers squibb research funding : pfizer ( inst ) travel , accommodations , expenses : astrazeneca , merck , bristol - myers squibb , foundation medicine , abbvie affiliations ajaz bulbul , john paul shen , pablo tamayo , and hatim husain , university of california san diego , la jolla , ca ; and joanne xiu , caris life sciences , phoenix , az . funded by university of california san diego moores cancer center institutional funds and national institutes of health grants no . 
honor c , amroun k , vilcot l , et al : abdominal desmoplastic small round cell tumor : multimodal treatment combining chemotherapy , surgery , and radiotherapy is the best option . 
tap wd , jones rl , van tine ba , et al : olaratumab and doxorubicin versus doxorubicin alone for treatment of soft - tissue sarcoma : an open - label phase 1b and randomised phase 2 trial . 
creighton cj , hilger am , murthy s , et al : activation of mitogen - activated protein kinase in estrogen receptor alpha - positive breast cancer cells in vitro induces an in vivo molecular phenotype of estrogen receptor alpha - negative human breast tumors . 
mendiola m , carrillo j , garca e , et al : the orphan nuclear receptor dax1 is up - regulated by the ews / fli1 oncoprotein and is highly expressed in ewing tumors . 
raeder mb , birkeland e , trovik j , et al : integrated genomic analysis of the 8q24 amplification in endometrial cancers identifies atad2 as essential to myc - dependent cancers . 
verhaak rg , hoadley ka , purdom e , et al : integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
gerald wl , rosai j , ladanyi m : characterization of the genomic breakpoint and chimeric transcripts in the ews - wt1 gene fusion of desmoplastic small round cell tumor . 
sukhatme vp , cao xm , chang lc , et al : a zinc finger - encoding gene coregulated with c - fos during growth and differentiation , and after cellular depolarization . 
fine rl , shah ss , moulton ta , et al : androgen and c - kit receptors in desmoplastic small round cell tumors resistant to chemotherapy : novel targets for therapy . 
morris mj , rathkopf de , novotny w , et al : phase ib study of enzalutamide in combination with docetaxel in men with metastatic castration - resistant prostate cancer . 
burgess ma , crowley j , reinke dk , et al : sarc 028 : a phase ii study of the anti - pd1 antibody pembrolizumab ( p ) in patients ( pts ) with advanced sarcomas . 
 c case of metastatic extramammary paget disease of the vulva treated successfully with trastuzumab emtansine introduction extramammary paget disease ( empd ) is a rare adenocarcinoma in situ that originates in skin that contains apocrine glands . 
empd is associated with invasive cancer in 4% to 20% of patients.1 in a series of 1 , 439 patients with invasive empd , 80.4% had localized disease , 17.1% had locoregional spread , and only 2.5% presented with distant disease.2 treatment is primarily surgical , but empd frequently is multicentric , and relapses are common regardless of treatment modality . 
since 2002 , she underwent six excisional procedures , three laser ablations , several courses of topical imiquimod treatment , external beam vulvar radiation to a dose of 56 gy to the perineum and the left - side inguinal nodes , and interstitial brachytherapy to 30 gy . 
her treatment was complicated by urethral swelling and eventually obstruction , requiring placement of a temporary suprapubic catheter and urethral reconstruction in late 2014 . in early 2016 , the patient noted worsening urinary retention , and a computed tomography ( ct ) urogram demonstrated two centrally hypodense liver lesions that measured up to 2.2 cm , multiple enlarged retroperitoneal lymph nodes , and a circumferential soft tissue mass that infiltrated the cervix and upper vagina . 
on examination under anesthesia , a paget lesion obliterated the perineum , including the urethra , vulva , and perianal area , and vaginoscopy was required to visualize the cervix . 
vulvar biopsy specimens confirmed invasive , poorly differentiated adenocarcinoma that had arisen from empd , with extensive lymphovascular space invasion and 3 + her2 immunostaining in > 10% of cells ( fig 1 )  . 
on the basis of high concordance between dna sequencingbased methods and fluorescent in situ hybridization ( fish ) in detecting erbb2 amplification , 5 fish was foregone . the patient underwent six cycles of carboplatin area under the curve of 5 mg ml / min and paclitaxel 175 mg / m2 chemotherapy every 21 days , gillian l . 
 ( a ) nests of extramammary paget disease in the epithelium ( black arrows ) with underlying invasive adenocarcinoma in the dermis ( red arrow ; hematoxylin - eosin stain magnification , 10 )  . 
 ( b ) strong , circumferential membranous staining of human epidermal growth factor receptor 2 ( her2 ) in extramammary paget disease and invasive tumor ( her2 immunohistochemical stain magnification , 10 )  . 
 ( c ) invasive adenocarcinoma ( hematoxylin and eosin stain magnification , 10 ) with ( d ) 3 + membranous staining of her2 ( her2 immunohistochemical stain magnification , 10 )  . with trastuzumab added from cycles 2 to 6 . 
repeat pet / ct scanning after 3 months of maintenance therapy revealed an intensely fdg - avid recurrent cervical and vaginal tumor and mildly enlarged and fdg - avid left - side external iliac nodes . 
treatment was well tolerated , with toxicity limited to grade 1 fatigue and grade 1 bleeding , including intermittent vaginal bleeding , hematuria , epistaxis , and gum bleeding , which started after cycle 2 . 
follow - up pet / ct scans were notable for markedly decreased size and metabolic activity of the primary pelvic lesion after cycle 3 and for complete resolution of disease on imaging after cycle 6 ( fig 2 )  . 
positron emission tomography / computed tomography ( a ) axial fusion , ( b ) sagittal fusion , and ( c ) maximum intensity projection images before ( top ) and after treatment ( bottom )  . 
 a hypermetabolic cervical mass ( arrow ) was seen with associated hydrometra , which had complete treatment response to chemotherapy . and hormonal suppression with letrozole.6 , 7 although insufficient data exist on the application of the current breast cancer asco - cap her2 testing guidelines8 to other cancer types , the amplification of her2 has been described in many cases of invasive empd ( table 1 )  . 
 multiple large , multicenter trials have firmly established the benefit of trastuzumab in the treatment of metastatic her2 - positive breast cancer , 9 which has led to consideration of trastuzumab in the treatment of invasive metastatic her2 - amplified empd . retrospective data have suggested that her2 overexpression is higher in patients with invasive empd than with noninvasive empd.19 furthermore , a significant correlation has been demonstrated among the presence of invasion , lymph node metastasis , and her2 overexpression.24 several case reports have demonstrated partial or complete response of widely metastatic empd on trastuzumab with or without paclitaxel ( table 2 )  . the mechanisms that underlie trastuzumabs clinical activity have not been completely table 1 . 
although tdm1 has been shown to be efficacious in patients with breast cancer with her2 - overexpressed malignancy unresponsive to trastuzumab , disease response has not been consistently demonstrated with other tumor types . 
 in her2 - positive unresectable gastric or gastroesophageal junction cancers with prior her2 - targeted therapy.36 the current patients favorable response indicates that in her2 positive invasive empd , tdm1 may be considered a viable treatment option . 
in addition , in hormone receptor and her2 - positive breast cancer , dual targeting of both signaling pathways may improve outcomes significantly.37 in breast cancer , bidirectional cross talk between the estrogen receptor and her2 pathways likely contributes to anti - her2 therapy resistance . 
 preclinical models with breast cancer cell lines have demonstrated a benefit to simultaneous hormone and her2 therapy over her2 - targeted therapy alone , but no phase ii or iii trials have compared the two.38 the tandem trial demonstrated a 2.4 - month survival benefit in postmenopausal patients with metastatic breast cancer who received anastrazole and trastuzumab versus hormonal therapy with anastrazole alone.39 hormone receptor immunohistochemistry was not examined in the current patient , but dual inhibition may be a theoretically superior strategy for treating hormone receptor and her2 - positive invasive empd . one limitation to this study is that the asco - cap her2 testing guidelines have not been routinely adopted or validated for tissues other than breast carcinoma ; thus , the her2 immunohistochemistry results may not be consistent or reliable in this tumor type . 
molecular subtyping has been used increasingly to find appropriate targeted therapies and may be more reliable than immunohistochemistry.23 vornicova et al7 reported a partial response that lasted 12 months in a male with adenocarcinoma with paget disease and negative her2 testing by both immunohistochemistry and fish , but received anti - her2 therapy on the basis of tumor somatic mutation testing alone ( table 2 )  . in light of the poor prognosis with metastatic epmd , paucity of treatment options , high incidence of her2 amplifications in empd , and favorable adverse effect profile of tdm1 , we suggest her2 testing and consideration of tdm1 treatment in patients with her2 overexpressed invasive empd who experience treatment failure with trastuzumab . 
ohara k , fujisawa y , yoshino k , et al : a proposal for a tnm staging system for extramammary paget disease : retrospective analysis of 301 patients with invasive primary tumors . 
vornicova o , hershkovitz d , yablonski - peretz t , et al : treatment of metastatic extramammary pagets disease associated with adnexal adenocarcinoma , with anti - her2 drugs based on genomic alteration erbb2 s310f . 
tchrakian n , flanagan l , harford j , et al : new asco / cap guideline recommendations for her2 testing increase the proportion of reflex in situ hybridization tests and of her2 positive breast cancers . 
ogawa t , nagashima y , wada h , et al : extramammary pagets disease : analysis of growth signal pathway from the human epidermal growth factor receptor 2 prote hum pathol 36 : 12731280 , 2005 16 . 
plaza ja , torres - cabala c , ivan d , et al : her - 2 / neu expression in extramammary paget disease : a clinicopathologic and immunohistochemistry study of 47 cases with and without underlying malignancy . 
villada g , farooq u , yu w , et al : extramammary paget disease of the vulva with underlying mammary - like lobular carcinoma : a case report and review of the literature . 
tanaka r , sasajima y , tsuda h , et al : concordance of the her2 protein and gene status between primary and corresponding lymph node metastatic sites of extramammary paget disease . 
tessier - cloutier b , asleh - aburaya k , shah v , et al : molecular subtyping of mammary - like adenocarcinoma of the vulva shows molecular similarity to breast carcinomas . 
barth p , dulaimi al - saleem e , edwards kw , et al : metastatic extramammary pagets disease of scrotum responds completely to single agent trastuzumab in a hemodialysis patient : case report , molecular profiling and brief review of the literature . 
arnould l , gelly m , penault - llorca f , et al : trastuzumab - based treatment of her2 - positive breast cancer : an antibody - dependent cellular cytotoxicity mechanism ? br j cancer 94 : 259 - 267 , 2006 31 . 
lewis phillips gd , li g , dugger dl , et al : targeting her2 - positive breast cancer with trastuzumab - dm1 , an antibody - cytotoxic drug conjugate . 
krop ie , kim sb , martin ag , et al : trastuzumab emtansine versus treatment of physicians choice in patients with previously treated her2 - positive metastatic breast cancer ( th3resa ) : final overall survival results from a randomised open - label phase 3 trial . 
thuss - patience pc , shah ma , ohtsu a , et al : trastuzumab emtansine versus taxane use for previously treated her2 - positive locally advanced or metastatic gastric or gastro - oesophageal junction adenocarcinoma ( gatsby ) : an international randomised , open - label , adaptive , phase 2 / 3 study . 
lousberg l , collignon j , jerusalem g : resistance to therapy in estrogen receptor positive and human epidermal growth factor 2 positive breast cancers : progress with latest therapeutic strategies . 
kaufman b , mackey jr , clemens mr , et al : trastuzumab plus anastrozole versus anastrozole alone for the treatment of postmenopausal women with human epidermal growth factor receptor 2 - positive , hormone receptor - positive metastatic breast cancer : results from the randomized phase iii tandem study . 
 braf mutations occur infrequently in ovarian cancer but suggest responsiveness to braf and mek inhibition introduction ovarian cancer ( oc ) is the leading cause of death from gynecologic malignancies in the developed world.1 although substantial efforts have been devoted to identifying potentially actionable oncogenic driver mutations in oc , only a few genes are frequently mutated , particularly in high - grade serous oc ( hgsoc ) , the most common histologic subtype . 
the cancer genome atlas reported p53 mutations in almost all primary hgsoc tumors ( 96% ) but a low prevalence of recurrent somatic mutations in additional genes including brca1 ( 12% ) , brca2 ( 11% ) , nf1 ( 4% ) , and cdk12 ( 3% )  . 
2 in the cosmic database , additional infrequent mutations such as kras ( 6% ) , pik3ca ( 2% ) , and braf ( 2% ) have been identified in hgsoc.3 we believe that some of these mutations , although rare , are important drivers in hgsoc . 
for example , mutations in braf lead to constitutive activation of downstream mek1 and mek2 and may regulate proliferation and survival in ovarian tumor cells as in many other cancers.4 the most commonly observed braf mutation , v600e , accounts for 90% of the braf mutations found in all patients with cancer.3 treatment with braf inhibitors such as vemurafenib or dabrafenib in patients with advanced brafv600 - mutated melanoma has shown objective tumor responses in approximately half of the patients.5 recent clinical studies have suggested that concurrent inhibition of the braf and mek kinases of the mitogen - activated protein kinase ( mapk ) pathway with trametinib or cobimetinib can decrease mapk - driven acquired resistance , resulting in greater efficacy and a decrease in the cutaneous toxicities observed from paradoxical mapk pathway activation with braf inhibitor monotherapy.6 here , we report a patient with recurrent hgsoc who had experienced treatment failure with an extensive number of prior treatment regimens and whose tumor was found to harbor a brafv600e mutation . 
of note , this patient responded extremely well to treatment with a braf inhibitor ( vemurafenib ) and subsequently to a braf inhibitor in combination with a mek inhibitor ( dabrafenib and trametinib )  . 
 to further underscore this treatment rationale , we studied the growth - inhibitory effects of the braf inhibitor vemurafenib and the mek inhibitor trametinib across a panel of 32 oc cell lines that were each characterized for mutational status of braf , kras , and nf1 ( fig 1 )  . 
 cell lines , assays , and sequencing methods have been described earlier.7 in brief , cells were plated into 24 - well tissue culture plates and grown with or without increasing concentrations of inhibitors . 
she developed recurrent disease to the left paracolic gutter region , which was not amenable to surgery but treated with carboplatin plus paclitaxel and , after further progression , by liposomal doxorubic subsequent treatments included topotecan , pemetrexed , gemcitabine plus carboplatin , maira p . 
preclinical activity of ( a ) vemurafenib and ( b ) trametinib across a large panel of 32 ovarian cancer ( oc ) cell lines characterized for braf , kras , and nf1 mutations . 
growth inhibition was calculated as a function of the number of generations inhibited in the presence of vemurafenib or trametinib versus the number of generations over the same time course in the absence of the drug as reported previously.7 in brief , the log of the fractional growth inhibition was plotted against the log of the drug concentration , and the half - maximal inhibitory concentration ( ic50 ) values were interpolated from the resulting linear regression curve fit . 
in the absence of a therapeutic standard of care , tumor tissue was submitted to foundation medicine for comprehensive genomic profiling revealing an activating brafv600e mutation as well as asxl1 ( k580fs * 2 ) and runx1t1 ( r520h ) mutations . 
cp , carboplatin and paclitaxel ; gp , carboplatin and gemcitabine ; pld , liposomal doxorubicin . 10 , 000 1 , 000 cg / cp topotecan pembrolizumab / epacadostat vemurafenib pemetrexed nanoparticle albumin - bound paclitaxel dabrafenib / trametinib 2004 2005 2006 2007 2008 2009 2010 2011 2012 2013 2014 2015 2016 2017 2018 up to a 3 - log - fold difference in the half - maximal inhibitory concentration values , but were most pronounced in cell lines that harbored braf , kras , or nf1 mutations ( fig 1b )  . 
after providing informed consent , the patient was treated in accordance with the declaration of helsinki with the braf inhibitor vemurafenib at the us food and drug administrationapproved dose of 960 mg twice a day . 
despite the dose reduction , she had to stop treatment after 13 days as a result of a profound diffuse maculopapular skin rash , which significantly improved with systemic corticosteroid medication . 
despite the brevity of treatment , the patients ca - 125 levels decreased from 4 , 495 to 2 , 119 u / ml within 21 days of initiating therapy , and a ct scan of the abdomen and pelvis revealed a partial response ( pr ) 29 days after commencing vemurafenib therapy.3 while the patient remained off therapy awaiting insurance approval for dabrafenib plus trametinib , the ca - 125 level increased again from 1 , 394 to 2 , 345 u / ml with increasing symptoms of abdominal bloating and distension as well as moderate pelvic pact scans of the abdomen and pelvis done before starting new treatment showed renewed progression ( fig 3 )  . 
after starting combination therapy with dabrafenib ( 150 mg twice a day ) and trametinib ( 2 mg daily ) , the ca - 125 levels decreased from 2 , 345 to 12 u / ml ( normal range , < 35 u / ml ) within a 10 - week period . 
in the following weeks , the patient developed mild lower extremity edema and moderate hypertension , requiring a decrease in the doses of dabrafenib from 150 mg to 75 mg twice a day and of trametinib from 2 mg to 1 mg daily . 
after 10 months of combination therapy , the ca - 125 levels remained in the normal range , and updated ct scans demonstrated an ongoing pr with continued reduction in size of her retroperitoneal lymphadenopathy ( fig 2 )  . 
to identify additional patients who might benefit from braf / mek inhibition , we analyzed a subset of 2 , 983 ovarian tumors from the foundation medicine database of more than 125 , 000 clinical cases that had undergone hybrid capturebased next - generation sequencing . 
brafv600 mutations were found in 46 ( 1.5% ) of 2 , 983 serous ocs , in three ( 4.2% ) of 71 ovarian mucinous cancers , in one ( 3.6% ) of 28 ocs with neuroendocrine differentiation , in four ( 5% ) of 80 low - grade serous ocs , and in two ( 13.3% ) of 15 serous borderline tumors ( table 1 )  . discussion we present a patient diagnosed with recurrent hgsoc who had received an extensive number of prior chemotherapy regimens and whose tumor was found to harbor a brafv600e mutation . 
treatment with the braf inhibitor vemurafenib and subsequently the braf inhibitor dabrafenib and mek inhibitor trametinib led to a persistent radiographic pr with normalization of ca - 125 and marked symptomatic improvement . 
the rapid development and widespread availability of ngs provides the opportunity to select an appropriate targeted therapy.9 however , matching patients with the optimum therapy is often challenging , particularly as driver events are generally infrequent and comprehensive clinical response data are rarely available for the specific cancer type , especially with noncanonical variants . 
for example , a left periaortic lymph node is ( a ) initially seen measuring 11 14 mm at baseline and ( b ) subsequently decreased to 7 8 mm after brief treatment with vemurafenib . 
 ( c ) after holding vemurafenib , ct scans of the abdomen and pelvis showed renewed progression of the lymphadenopathy with the left periaortic node measuring 10 11 m ( d ) dabrafenib and trametinib treatment again led to a significant decrease in size of the abdominal and retroperitoneal lesions with a decrease in size of the left periaortic node to 4 6 m ( e ) after further combination therapy , the ca - 125 level remains in the normal range and updated ct scans demonstrate an ongoing partial response with continued reduction in size of the patients left periaortic lymph node now measuring 2 3 m ( f ) ca - 125 tumor marker levels are shown during treatment while on chemotherapy , followed by the braf inhibitor vemurafenib given as a single agent , followed by combination treatment with the braf inhibitor dabrafenib and the mek inhibitor trametinib . cancer type , basket trials have been initiated that categorize patients cancers on the basis of the sequencing of the tumor , rather than the organ of origin.10 nevertheless , individual case reports , such as the present description , may provide important additional evidence to support further table 1 . 
frequency of brafv600e mutations in 2 , 983 ovarian tumors brafv600positive tumors tumor type serous ovarian cancer ovarian mucinous cancer ovarian cancer with neuroendocrine differentiation low - grade serous ovarian cancer serous borderline tumors ( low malignant potential ) total no . 
similarly , mek inhibition with trametinib led to growth inhibition in es - 2 cells ; however , oc cell lines with kras , nf1 , and other braf mutations also seemed to be sensitive to mek inhibition , suggesting potentially a broader role of mek inhibitors in oc . 
 although it is clear that ngs - based technologies are already having an impact on patient care , for broad , widespread use to occur , several factors will need to be addressed in the coming years . 
in addition to expanding basket - type trials , we need further development of data - sharing consortia that are focused on generating an evidence base for precision cancer medicine by integrating robustly validated , broad - based genomic profiling data with clinical outcome data . 
konecny manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors stock and other ownership interests : personal genome diagnostics , ignyta consulting or advisory role : quintiles , janssen diagnostics , ignyta , personal genome diagnostics patents , royalties , other intellectual property : receive royalties for discoveries our group has made at johns hopkins that have been licensed by qiagen ; receive royalties for discoveries our group has made at johns hopkins that have been licensed by myriad ; receive royalties for discoveries our group has made at johns hopkins that have been licensed by personal genome diagnostics ; receive royalties for discoveries our group has made at johns hopkins that have been licensed by genzyme ; receive royalties for discoveries our group has made at johns hopkins that have been licensed by roche jennifer l . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author = center . dylan conklin no relationship to disclose dorothy hallberg no relationship to disclose dennis j . 
konecny stock and other ownership interests : foundation medicine speakers ' bureau : clovis oncology , astrazeneca , tesaro research funding : merck travel , accommodations , expenses : novartis affiliations maira p . 
kujak , rolling oaks radiology , thousand oaks , ca ; victor velculescu and dorothy hallberg , sidney kimmel comprehensive cancer center , johns hopkins university school of medicine , baltimore , md ; and julia elvin , foundation medicine , cambridge , ma . supported by the miriam and sheldon g . 
ihnen m , zu eulenburg c , kolarova t , et al : therapeutic potential of the poly ( adp - ribose ) polymerase inhibitor rucaparib for the treatment of sporadic human ovarian cancer . 
ross js , ali sm , wang k , et al : comprehensive genomic profiling of epithelial ovarian cancer by next generation sequencing - based diagnostic assay reveals new routes to targeted therapies . 
the precise impact of these panels on clinical decision making is not well understood . methods here , we report our institutional experience with a targeted 40 - gene panel ( myeloseq ) that is used to generate a report for both genetic variants and variant allele frequencies for the treating physician ( the limit of mutation detection is approximately one aml cell in 50 )  . results in total , 346 sequencing reports were generated for 325 patients with suspected hematologic malignancies over an 8 - month period ( august 2018 to april 2019 )  . 
to determine the inuence of genomic data on clinical care for patients with acute myeloid leukemia ( aml ) , we analyzed 122 consecutive reports from 109 patients diagnosed with aml and surveyed the treating physicians with a standardized questionnaire . 
inuences were often nuanced and extended beyond identifying actionable genetic variants with us food and drug administrationapproved drugs . conclusion this study provides insights into how physicians are currently using multigene panels capable of detecting relatively rare aml cells . 
the most inuential way to integrate these tools into clinical practice will be to perform prospective clinical trials that assess patient outcomes in response to genomically driven interventions . jco precis oncol 5 : 191 - 203 . 
some quires variant single - gene tests and two multitarget panels are currently us food and drug administration ( fda ) approved and have associated companion diagnostics that designate a specic cancer subtype and indication.2 however , the vast majority of variant identication and annotation is performed by laboratory developed tests ( ldts ) , 3 for which results are provided as a clinical report . 
these reports typically require a certain level of genomic literacy to understand and implement.4 , 5 lack of report standardization , inadequate genomic training , 6 , 7 limited infrastructure to support oncologists , 1 , 8 and limited resourcesfor example , low reimbursement rates and lack of access to clinical trialsare thought to hinder the impact of sequencing data on clinical care.9 , 10 the result is a discrepancy between the identication of clinically actionable variants11 and implementation of change in treatment decisions.1 , 12 acute myeloid leukemia ( aml ) sequencing data are particularly complex because of the genetic and clonal heterogeneity of aml cases . 
 barnell et al context key objective whereas physicians have increased the use of targeted sequencing panels to inform treatment decisions for patients with hematologic malignancies , the impact and utility of sequencing data on clinical decision making is not well understood . 
through standardized surveys , this study captured the nuanced impact of sequencing data on clinical decision making for patients with acute myeloid leukemia . knowledge generated physicians self - reported that 50 of 114 sequencing reports ( 44% ) inuenced clinical care decisions with 56 total inuences reported , 38 of which were related to therapeutic options , 10 related to risk stratication in rst clinical remission , and eight involving measuring persistent molecular disease . 
in 11% of all patients , the panel was ordered at multiple timepoints during the disease course for persistent molecular disease monitoring . relevance this study demonstrates that physicians are integrating sequencing data obtained at various points in the acute myeloid leukemia disease course into clinical decision making , mostly to determine therapy choices , stratify relapse risk , and measure persistent disease . signicance may depend on cooperating covariants in multiple other genes.14 for example , european leukemianet / national comprehensive cancer network guidelines specically mention six genes / mutations in their risk stratication guidelines , all of which must be evaluated in parallel for risk stratication.15 , 16 in addition , whereas pathogenic variants within three genesflt3 , idh2 , and idh1have been used as predictive markers for fda - approved targeted therapeutics , 17 - 19 ongoing clinical trials have demonstrated predictive utility for other pathogenic variants that do not yet have approved companion diagnostics.20 next - generation sequencing ( ngs ) data can provide information beyond therapeutic sensitivity / resistance that is not currently captured by fda - approved diagnostics . specically , quantication of the variant allele frequency ( vaf ) of tumor - associated variants has been used to detect persistent molecular disease ( pmd ) after therapies are administered , and predict both relapse risk21 and survival outcomes.22 - 24 although multipanel ldt diagnostics are being used on patients with aml to supplement treatment decisions , the utility of these reports is not well described . this study sought to better understand the extent to which genomic reports inuence clinical decision making for patients with aml . 
this paper describes physician experience with a targeted gene panel ( myeloseq ) that terrogates 40 recurrently mutated genes or gene hotspots and returns gene variant and vaf data to the treating physician . 
we determined usage patterns over an 8 - month period and surveyed treating physicians regarding how they used the panel results in clinical care . methods study design and patient eligibility this study was conducted at washington university school of medicine ( human research protection ofce #201801112 )  . 
the panel was a targeted sequencing assay that evaluated 40 genes and gene hotspots that are recurrently mutated in myeloid malignancies ( data supplement ) .25 for each patient who was found to have a denitive diagnosis of aml , a survey was sent to the treating physician . 
patients with acute promyelocytic leukemia ( m3 aml subtype ) were excluded.26 the treating physician was asked to complete a ninequestion survey to determine how the physician used the panel to inform treatment decisions ( data supplement )  . panel design and processing the panel uses an amplicon capture - based enrichment with unique molecular identiers for ultra - high variant sensitivity that targets an approximately 98 - kb space ( haloplex target enrichment system ; agilent technologies , santa clara , ca )  . 
this included evaluating bone marrow morphology , standard panels of ow cytometric markers , and a panel of routine cytogenetic and molecular marker studies , including uorescence in situ hybridization probes . target enrichment , variant calling strategies , and variant annotation methods are described in the data supplement . the median number of failed genes across all reports was two ( range , 0 to 24 genes )  . 
wt1 ( n = 211 cases ) , cux1 ( n = 197 cases ) , and cebpa ( n = 111 cases ) were genes that most frequently failed coverage requirements . 
if physicians did not respond to the initial contact , reminders were provided to increase the response rate . ethics , consent , permissions , and consent to publish this study was conducted at washington university school of medicine and was approved by the washington university human research protection ofce ( #201801112 )  . 
summary of patient , report , and physician characteristics characteristic ( n = 109 ) value median time from accessioning to report sign out , daysa 12 ( 4 - 36 ) patient ( n = 109 ) median age , years male female report ( n = 122 ) physician ( n = 14 ) mean time in practice , yearsb academic rank professor associate professor assistant professor degree type md / phd md / mba male female there were 124 reports from patients with aml . 
the reports from patients with aml , after removing patients with apl subtype ( n = 122 samples ) , were derived from 109 unique patients who were under the care of 14 physicians ( table 1 )  . 
only 13 samples had no observed variants , eight of which were acquired from patients who were determined to be in clinical remission using bone marrow biopsy . reports were ordered at various points in the disease course . 
the next most common timepoint was during disease assessment ( n = 28 of 122 ; [ 22.9% ] ) , followed by potential relapse ( n = 19 of 122 [ 15.6% ] ; fig 3a )  . 
for reports ordered during disease response assessments , seven were ordered post - induction , six were ordered after allogeneic hematopoietic cell transplant ( allohct ) , ve were ordered during ongoing treatment with a hypomethylating agent , two were ordered after consolidation with high - dose ara - c , and seven were ordered during or after salvage therapy ( fig 3b )  . 
on the basis of these data , the sequencing report was a factor in determining therapy decisions in 50 ( 43.8% ) of 114 cases ( fig 4a )  . 
the patient accepted the treatment plan 93% of the time ( n = 38 of 41 cases )  . predictive inuences in 35 of 50 reports , physicians indicated that they recommended at least one therapy on the basis of the variants identied by the sequencing panel ( fig 4b )  . 
on the basis of results35 reports with 38 corresequencing panel sponding inuencesphysicians reported recommending a hypomethylating agent in 14 patients for a tp5320 or tet228 , 29 variant , kinase inhibitors ( midostaurin or gilteritinib ) in 12 patients with a flt3 variant30 and one patient with a kit variant , 31 and idh1 / idh2 inhibitors were recommended for eight patients.32 there were three patients for whom a clinical trial was recommended on the basis of observed variants or persistent disease . 65 ( 23 - 90 ) 58 ( 53.2 ) 51 ( 46.8 ) 22 ( 8 - 44 ) 5 ( 36 ) 4 ( 29 ) 5 ( 36 ) 8 ( 57 ) 5 ( 36 ) 1 ( 7 ) 11 ( 79 ) 3 ( 21 ) note . 
of cases ( n = 122 ) flt3 internal tandem duplication splice acceptor variant frameshift variant missense variant flt3 tyrosine kinase domain splice donor variant inframe insertion negative no flt3 variant flt3 status stop gained variant type inframe deletion percentage of cases fig 2 . 
in 16 of 29 eligible cases ( two patients refused treatment ) , physicians reported the following inuences : 12 used the ngs panel to prescribe an flt3 inhibitor and four inuences were independent of flt3 status . 
in three of these four cases , patients had an flt3 inhibitor prescribed based on a previously known result from a different genetic test . there were 13 cases in which the patient had an flt3 variant , but the physician reported no inuence . 
of these 13 cases , three patients died before treatment initiation and eight had an flt3 inhibitor prescribed based on a previously known result from a different genetic test ( data supplement )  . risk stratication for transplant in first clinical remission physicians identied 10 reports that inuenced patient risk assessment and allohct recommendation ( fig 4b )  . specically , allohct was not recommended in rst complete remission in six patients , based on the presence of bialleleic cebpa variants ( n = 2 ) , kit variant status ( n = 1 ) , lack of high - risk variants ( n = 1 ) , or differential clearance of co - occurring variants after induction therapy ( n = 1 )  . 
for the latter patient , three variants were detected at diagnosis ( dnmt3a [ vaf = 42% ] , npm1 [ vaf = 38% ] , and rad21 [ vaf = 43% ] )  . 
these recommendations were based on tp53 variant status ( n = 2 ) , dnmt3a variant status ( n = 1 ) , and co - occurrence of multiple variants ( dnmt3a , npm1 , and flt3 internal tandem duplication ; n = 1 ) .14 assessment for pmd there were eight cases in which the sequencing panel was used to assess for pmd ( fig 4b )  . 
in ve cases , the physician indicated that the reports conrmed relapse / progression of aml , including one case of bone marrow negative , extramedullary relapse in the esophagus ( fig 5d )  . there were three patients who were being assessed for pmd while in an apparent clinical remission . 
two of the three patients did not show persistent aml via pmd assessment . the third patient showed three residual variants at low vaf ( cebpa [ vaf = 4% ] , smc1a [ vaf = 4% ] , and wt1 [ vaf = 3% ] ) , suggesting persistent disease . patients with no change in treatment regimens in response to sequencing panels there were 64 cases for which the physician noted no change in therapeutic plan on the basis of the report . 
the total number of eligible surveys completed by each physician and the total number of cases where the physician changed his or her plan is shown in figure 4c . the sequencing panel reports the vaf and thus can detect possible inherited variants . 
one patient was found to have a gata2 variant observed at a vaf of 52% , indicative of a possible germline variant , which prompted an action by the treating physician . 
a subsequent skin biopsy determined that the patient did not have a germline predisposition for disease . multiple sequencing panels for longitudinal disease monitoring and response therapy , there were 12 patients for whom the treating physician ordered multiple reporters during the disease course21 ( fig 5 and data supplement )  . 
after induction , despite some variants demonthe idh2 vaf of strating response to initial 39% ( 46% at diagnosis ) resulted in initiation of enasidenib . figure 5b shows a patient for whom the physician obtained three sequencing panels for longitudinal pmd monitoring . the rst report was ordered at relapse post - transplant and showed ve variants . 
a month later , the third report showed the re - emergence of three variants despite no excess blasts on the bone marrow biopsy , which resulted in a second allohct . 
figure 5c shows how a physician used sequential reports to observe the patients molecular response to a donor lymphocyte infusion and gilteritinib . figure 5d shows how the reports diagnosed extramedullary relapse in a patient with negative bone marrow biopsy ndings . 
the extramedullary disease showed the presence of some original variants ( nf1 and ezh2 ) , loss of other variants ( dnmt3a ) , and three novel variants ( cux1 , ptpn11 , and wt1 ) , some of which had clinical implications.34 , 35 additional cases with multiple reports are provided in the data supplement . reimbursement and clinical care access one of the biggest challenges for the widespread clinical implementation of ngs - based diagnostics has been inconsistent reimbursement from payers . 
coverage and reimbursement for myeloseq was divided into inpatient testing ( 26% ) and outpatient testing ( 74% ) , and 90% of outpatient testing was reimbursed across all payers . 
of these 124 cases , four were excluded ( acute promyelocytic leukemia [ apl ] subtype [ n = 2 ] ; no survey returned [ n = 2 ] )  . 
in 64 cases , physicians reported that the results did not inform decision making . ( c ) there were 14 physicians who contributed at least one survey to this study . was no specic pattern in terms of the diagnosis of rejected claims ( data supplement )  . discussion this study reports our institutions experience using a targeted capture sequencing panel to inform clinical care in patients with aml . 
 a addition of targeted therapy after lack of response to induction therapy persistent molecular disease monitoring barnell et al cebpa k302e smc1a r96h wt1 a38gfs * 69 wt1 r370pfs * 15 ezh2 k400del nf1 t2507i dnmt3a w297s dnmt3a f755 * smc1a / cepba ( 4% ) wt1 ( 3% ) wt1 ( 0% ) ( itd ) cux1 g1328s ptpn11 a72v wt1 r370pfs * 15 ezh2 k400del nf1 t2507i flt3 status enasidenib treatment ( itd ) gilteritinib new diagnosis of aml ( d0 diagnosis ) 22% blasts ( bmbx ) post 7 + 3 induction ( d49 post - diagnosis ) 3% blasts ( bmbx ) relapse ( d360 sct ) 44% blasts ( bmbx ) remission ( d426 sct ) < 1% blasts ( bmbx ) disease assessment ( d475 sct ) 0% blasts ( bmbx ) persistent molecular disease monitoring post - dli molecular diagnosis of extramedullary relapse bone marrow esophagus asxl1 g646wfs * 12 idh2 r140q runx1 l112cfs * 10 srsf2 p95h stag2 r146 * flt3 status treatment bcor t1129pfs * 30 bcorl1 q459 * dnmt3a r882h tet2 s1448n u2af1 s34f flt3 status flt3 status treatment treatment ( itd ) ( itd ) gilteritinib flt3 status treatment relapsed aml ( 1 month post - dli ) 21% blasts ( bmbx ) relapsed aml ( 3 months post - dli ) 6% blasts ( bmbx ) bone marrow ( ~ 10 yr sct ) 1% blasts ( bmbx ) esophageal tissue ( ~10 yr sct ) 1% blasts ( bmbx ) fig 5 . 
 ( b ) physician reported that the observation of persistent molecular disease at 475 days ( d ) poststem - cell transplantation ( sct ) indicated the need for a second allogeneic stem - cell transplantation despite clinical remission ( 0% blasts on bone marrow biopsy [ bmbx ] )  . 
 ( d ) extramedullary relapse was conrmed by comparing sequencing results of the original tumor and the periesophageal lesion . diagnosis , during disease assessment , and / or at multiple timepoints during the disease course . this study suggests that physicians are increasingly relying on the evaluation of multiple co - occurring variants in parallel ; therefore , simultaneous analysis of these genes is necessary . 
furthermore , pmd monitoring after cytotoxic induction therapy and transplantation21 , 36 has prognostic value ; therefore , the vafs reported on the gene panel studied here were being used to supplement existing standard - of - care mechanisms for residual disease assessment . 
although it is clear that physicians are using this test to measure and assess pmd , this test was not designed for measurable residual disease testing , and the limit of detection is not within the european leukemianet guidelines for measurable residual disease assessment.15 , 37 the prognostic information provided by the detection of persistent variants , the optimal depth of clearance , and the required limit of detection are all areas of active investigation requiring additional study in prospective clinical trials . there were several limitations associated with this study . reports were evaluated over an 8 - month period at a single academic institution among physicians with experience interpreting genomic results . 
 targeted panel inuences decision making for patients with aml were returned contemporaneously and tests were ordered at different timepoints during the disease course ( fig 3 )  . whereas the proportion of cases with inuences was not signicantly different among timepoints ( data supplement ) , inuence types might be different between timepoints and should be evaluated further to understand the impact of disease timepoint on treatment decisions . 
finally , each physician had a varied number of patients ( range , one to 18 patients ) with a large range in the number of cases reported to be inuential ( 0% to 90% )  . 
larger longitudinal , multi - institutional studies are needed to better understand interphysician variability in incorporating genomic data into clinical decision making . this study evaluated reports from the rst 8 months after launch of the diagnostic . 
the physicians were also experienced in interpreting genomic data , having participated in large genomic trials , 20 , 21 , 38 - 41 with many of them being clinical investigators themselves . 
given that the inuence of genomic data varies on the basis of physicians experience with genomic data , 6 , 7 the results presented here might not extrapolate to institutions that are unfamiliar with ordering and interpreting sequencing - based diagnostics . the sequencing panel has several additional limitations . the use of a tumor - only panelthat is , lack of a germline or reference sequenceprevented variants from normal being denitively called somatic . 
in future studies , it will be important to ascertain from physicians if any aspect of the test or the molecular report is unclear , biased , or difcult to interpret . there are several outstanding questions in the eld that could be addressed using a test similar to the one described in this paper . 
the prognostic value of residual dnmt3a , tet2 , and asxl1 mutations after treatment is incompletely understood , 21 , 36 , 42 and the difference between a residual leukemic clone versus rising clonal hematopoiesis43 needs additional study . 
our group is currently conducting a prospective clinical ( clinicaltrials.gov identier : nct02178241 ) to address some of these outstanding questions . trial in summary , the results from this study suggest that variants and associated vafs are being integrated into clinical care to inuence therapy choices , stratify relapse risk , and measure persistent disease . 
barnell employment : geneoscopy stock and other ownership interests : geneoscopy patents , royalties , other intellectual property : inventor of intellectual property in start - up company ( geneoscopy ) travel , accommodations , expenses : geneoscopy kenneth f . 
newcomer employment : geneoscopy ( i ) stock and other ownership interests : geneoscopy ( i ) patents , royalties , other intellectual property : inventor of intellectual property owned by geneoscopy ( i ) zachary l . 
oh consulting or advisory role : incyte , novartis , blueprint medicines , celgene , kartos , cti biopharma corp , pharmaessentia , disc medicine , constellation pharmaceuticals research funding : incyte ( inst ) , gilead sciences ( inst ) , cti biopharma corp ( inst ) , kartos ( inst ) , celgene ( inst ) , sierra oncology ( inst ) , blueprint medicines ( inst ) , constellation pharmaceuticals ( inst ) john s . 
stockerl - goldstein stock and other ownership interests : abbott laboratories , abbvie consulting or advisory role : celgene research funding : glaxosmithkline , takeda , biolinerx , janssen other relationship : cellerant ravi vij consulting or advisory role : bristol myers squibb , celgene , janssen , sano , karyopharm therapeutics , takeda , genentech , abbvie , oncopeptides research funding : takeda , celgene , bristol myers squibb travel , accommodations , expenses : celgene , bristol myers squibb , sano , janssen , davaoncology , karyopharm therapeutics , amgen , takeda , abbvie amanda f . 
abboud stock and other ownership interests : abbvie ( i ) , abbott laboratories ( i ) , gilead sciences ( i ) , bristol myers squibb ( i ) , johnson & johnson ( i ) honoraria : cardinal health , dova pharmaceuticals , nkartatherapeutics , archer biosciences research funding : actinium pharmaceuticals , selvita ( inst ) , allovir ( inst ) , forty - seven ( inst ) armin ghobadi honoraria : kite pharma consulting or advisory role : kite pharma , celgene , amgen , wugen speakers bureau : kite pharma , amgen geoffrey l . 
schroeder consulting or advisory role : astellas pharma , dova pharmaceuticals , flatiron health , glaxosmithkline , incyte , partners therapeutics , partners therapeutics , pzer speakers bureau : abbvie , merck , takeda john f . 
dipersio stock and other ownership interests : magenta therapeutics , wugen honoraria : incyte consulting or advisory role : cellworks , rivervest , magenta therapeutics , incyte research funding : amphivena therapeutics ( inst ) , macrogenics ( inst ) , incyte ( inst ) , wugen ( inst ) , biolinerx ( inst ) , maxcyte ( inst ) , bigelow aerospace ( inst ) patents , royalties , other intellectual property : patents : cd7 and cd2 knockout for cart to cd7 and cdl ; duvelisib for treatment of cytokine release syndrome ; nt - 17 to enhance cart survival ; novel wu mobilizing compounds ( inst ) ; selection of impdh mutant stem cells ; ifn , upregulate mhcii for relapsed aml ; dextran - based molecules to detect car - t cells ; combining integrin inhibitor with chemokine binders , 016131 ; jak and calcineurin inhibition , solid organ transplant ; vla4 , gro - b ; triple combinationcxcr2 , vla - 4 , gro - b ; targeting ifnr / cscr3 in gvhd ; wu / slu compounds vla4 and cxcr2 ( inst ) travel , accommodations , expenses : incyte , macrogenics , magenta therapeutics mary c . 
duncavage stock and other ownership interests : p&v licensing consulting or advisory role : cofactor genomics , bristol myers squibb , eli lilly open payments link : 317379 timothy j . 
additional thanks are also given to the siteman cancer center and the barnesjewish hospital foundation . 11 : 11 , 2016 368 : 2059 - 2074 , 2013 129 : 424 - 447 , 2017 netw 15 : 926 - 957 , 2017 2017 314 : 811 - 822 , 2015 references ray t : survey of precision oncology programs nds agreement on testing , divergence in care delivery . 
precision oncology news , july 19 , 2019 : precisiononcologynews.com / cancer / survey - precision - oncology - programs - nds - agreement - testing - divergence - care - delivery stone rm , mandrekar sj , sanford bl , et al : midostaurin plus chemotherapy for acute myeloid leukemia with a flt3 mutation . 
n engl j med 377 : 454 - 464 , 2017 kim as , bartley an , bridge ja , et al : comparison of laboratory - developed tests and fda - approved assays for braf , egfr , and kras testing . 
jama oncol 4 : 838 - 841 , 2018 li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
bmc med inform decis mak 18 : 107 , 2018 chow - white p , ha d , laskin j : knowledge , attitudes , and values among physicians working with clinical genomics : a survey of medical oncologists . 
j genet couns 27 : 187 - 196 , 2018 gornick mc , ryan ka , scherer am , et al : interpretations of the term actionable when discussing genetic test results : what you mean is not what i heard . j genet couns 28 : 334 - 342 , 2019 statz cm , patterson se , mockus sm : barriers preventing the adoption of comprehensive cancer genomic proling in the clinic . 
au ch , wa a , ho dn , et al : clinical evaluation of panel testing by next - generation sequencing ( ngs ) for gene mutations in myeloid neoplasms . 
marcucci g , mr ozek k , ruppert as , et al : abnormal cytogenetics at date of morphologic complete remission predicts short overall and disease - free survival , and higher relapse rate in adult acute myeloid leukemia : results from cancer and leukemia group b study 8461 . 
chen y , cortes j , estrov z , et al : persistence of cytogenetic abnormalities at complete remission after induction in patients with acute myeloid leukemia : prognostic signicance and the potential role of allogeneic stem - cell transplantation . 
j clin oncol 29 : 2507 - 2513 , 2011 ivey a , hills rk , simpson ma , et al : assessment of minimal residual disease in standard - risk aml . 
loken mr , alonzo ta , pardo l , et al : residual disease detected by multidimensional ow cytometry signies high relapse risk in patients with de novo acute myeloid leukemia : a report from childrens oncology group . 
hou h - a , chou wc , lin li , et al : characterization of acute myeloid leukemia with ptpn11 mutation : the mutation is closely associated with npm1 mutation but 35 . 
gaidzik vi , schlenk rf , moschny s , et al : prognostic impact of wt1 mutations in cytogenetically normal acute myeloid leukemia : a study of the germaninversely related to flt3 / itd . 
blood 113 : 4505 - 4511 , 2009 jongen - lavrencic m , grob t , hanekamp d , et al : molecular minimal residual disease in acute myeloid leukemia . 
schuurhuis gj , heuser m , freeman s , et al : minimal / measurable residual disease in aml : a consensus document from the european leukemianet mrd working party . 
clinical diincluding disease status , was dened by board - certied agnosis , hematopathologists . the panel uses an amplicon capture - based enrichment with unique molecular identiers for ultra - high variant sensitivity that targets an approximately 98 - kg base pair space ( haloplex target enrichment system ; agilent technologies , santa clara , ca )  . 
the panel is generally ordered for one of the following conditions : aml , mds , cytopenia , clonal cytopenia of undetermined signicance , clonal hematopoiesis of indeterminate signicance , myeloproliferative neoplasm , or other myeloid disorders . 
this included evaluating bone marrow morphology , standard panels of ow cytometric markers , and a panel of routine cytogenetic and molecular marker studies , including uorescence in situ hybridization probes . target enrichment for the panel used a commercially available , targeted , next - generation sequencing approach ( haloplexhs ; agilent technologies )  . 
preparation consisted of enzymatic fragmentation ; strand - specic ligation of sequencing primers , sample indexes , 10 - bp degenerate molecular barcodes , and biotin tagging of single dna molecules ; rapid liquid - phase enrichment of target loci using paramagnetic streptavidin - coated beads ; and on - bead polymerase chain reaction amplication . 
sequencing was performed using the illumina miniseq sequencing platform ( target depth = 50 coverage )  . variant calling for the panel was performed using a computational pipeline that employs custom - built tools created at washington university . 
overall reads were required to exceed 1 , 000 , 000 total reads with more than 98% aligned . during this process , unique molecular identier sequences are added to the binary alignment map le . 
once aligned , a custom java - based tool collapsed reads into read families using customized gatk software ( mckenna a , et al : genome res 20 : 1297 - 1303 , 2010 )  . 
collapsed binary alignment maps were used with standard variant calling tools , including varscan2 ( koboldt dc , et al : genome res 22 : 568 - 576 , 2012 ) , platypus ( rimmer a , et al : nat genet 46 : 912 - 918 , 2014 ) , and pindel ( ye k , et al : bioinformatics 25 : 2865 - 2871 , 2009 )  . 
these programs detected single - nucleotide substitutions , insertions or deletions ( indels ) up to 10 bp , and flt3 internal tandem duplication insertions between 21 and 108 bp . 
initial variant annotation was performed using the variant effect predictor tool ( mclaren w , et al : genome biol 17 ( 1 ) : 122 , 2016 )  . 
annotation was format le with variants augmented using a custom variant call identied in the aml the cancer genome atlas data set as well as variants observed in three published sequencing reports that evaluated patients with mds ( haferlach t , et al : leukemia 28 : 241 - 247 , 2014 ; papaemmanuil e , et al : blood 122 : 3616 - 3627 , quiz 3699 , 2013 ; walter mj , et al : leukemia 27 : 1275 - 1282 , 2013 )  . 
variant identication was subject to the following thresholds and cutoffs for reporting purposes : variants must be nonsynonymous , variants must have 2% minimum variant allele frequency and ve variant reads with support on each strand ( flt3 internal tandem duplication alleles require one read on each strand ) , amplicons must have at least ve reads assigned to it during consensus binary alignment map formation , and potential somatic variants must have 0.1% maximum population allele frequency ( max_af across all populations ; 1000 genomes [ v.phase3 ; 1000 genomes project consortium , et al : nature 526 : 6874 , 2015 ] and gnomad database [ v.170228 ; karczewski kj , et al : nature 581 : 434 - 443 , 2020 ] ) or presence in a custom mds / aml variant database . tier 1 ( variants with strong clinical signicance ) and tier 2 variants ( variants with potential clinical signicance ) , four ltered variants ( ie , variant allele frequency , 2% ) , and variants of unknown signicance were manually reviewed for potential clinical relevance . 
 sunitinib in the treatment of thymoma and associated autoimmune neutropenia introduction autoimmune disorders such as myasthenia gravis or pure red cell aplasia ( prca ) are frequent in patients with thymoma . 
thymoma - associated neutropenias , however , are rare ; to the best of our knowledge , only 17 patients have been described.1 - 16 for these patients , the diagnosis of neutropenia occurred simultaneously with that of thymoma or , less often , during the disease course , 2 , 4 - 8 , 10 - 16 and was frequently associated with myasthenia gravis , hypogammaglobulinemia , or anemia.2 - 12 , 14 - 16 granulopoiesis has been described as being completely or almost completely absent or as being arrested at the promyelocyte stage.2 - 7 , 9 , 10 , 12 - 16 bone marrow ( bm ) lymphocytosis is frequent and predominantly the result of t - cell infiltration.2 , 6 , 7 , 10 , 13 in one patient , a monoclonal rearrangement of the t - cell receptor ( tcr ) beta chain was found.8 thymoma - associated neutropenia is likely of autoimmune etiology ( ie , autoimmune neutropenia [ ain ] )  . 
antinuclear antibodies were present4 , 10 - 12 , 14 or not6 , 12 , 15 ; antineutrophil cytoplasmic antibodies were positive in one article , 11 with a decrease in titer upon neutrophil recovery . 
antigranulocyte antibodies were not detected5 , 9 , 12 or present10 ; in the latter case , the antibodies did not react with common human neutrophil antigens.10 studies consistently showed decreased granulocyte - macrophage colony formation in the bm of patients or controls in the presence of patients serum , 5 - 7 , 9 , 10 , 12 whereas formation was not affected by control sera or patients lymphocytes or thymoma cells.5 , 7 , 10 the inhibitory activity of the patients serum was present in the immunoglobulin g fraction.5 , 9 , 10 the treatment of thymoma - associated ain resembles that of prca17 and comprises the use of immunosuppressants ( eg , corticosteroids , 5 , 7 - 13 cyclosporine , 13 - 15 azathioprine , 9 cyclophosphamide , 5 , 10 , 12 mycophenolate , 14 or alemtuzumab14 ) , intravenous immunoglobulins , granulocyte colony - stimulating factor , plasmapheresis , and / or thymectomy.5 , 7 , 9 - 15 neutrophil response varied widely among the patients described . the tyrosine kinase inhibitor sunitinib has recently been shown to be effective against thymic carcinoma and , less frequently , type b thymoma in a phase ii trial and in retrospective analyses.18 , 19 sunitinib inhibits the receptors for the plateletderived growth factor receptor , vascular endothelial growth factor receptor ( vegfr ) , and stem cell factor ( kit ) , as well as other kinases . 
the patient provided written informed consent for the research use of the clinical data and biomaterial in accordance with the declaration of helsinki , as approved by the local ethics committee ( university of freiburg )  . the patient , a 33 - year - old man , was diagnosed with thymoma b2 in masaoka stage iva ( table 1 )  . he received three courses of cisplatin , doxorubicin , and cyclophosphamide ( pac ) chemotherapy followed by total thymectomy and resection of adjacent structures , leaving only microscopic tumor residues . 
shortly thereafter , computed tomography scans revealed new lesions in the right cardiophrenic angle and mediastinuthe patient then agreed to receive radiotherapy . radiotherapy was interrupted after 20 gy because of neutropenia and anemia . 
the neutrophils spontaneously rapidly recovered , but the anemia persisted until corticosteroid therapy was started . after recovery of the blood counts and stopping corticosteroids , and in the light of new lesions , radiotherapy was reinitiated but again stopped heiko becker konrad auman rainer claus nikolas von bubnoff ulrich j . 
diagnosed with thymoma b2 in masaoka stage iva . biopsy negative for variants ( non - synonymous and allele frequency > 10% ) in braf exon 15 ; egfr exons 18 , 19 , 20 , 21 ; kras exons 2 , 3 , 4 ; kit exons 9 , 11 , 13 , 17 ; nras exons 2 , 3 ; pdgfra exon 18 ; pi3kca exons 9 , 20 . 
bold font indicates days being on sunitinib treatment ( v being off treatment )  . abbreviations : gat , granulocyte agglutination test ; gift , granulocyte immunofluorescence test ; nd , not determined . * the interval between the end of cycle 2 and the start of cycle 3 was prolonged by 4 weeks because of patients personal reasons ; during this interval , granulocyte colony - stimulating factor was prophylactically applied once per week . computed tomography scan : progressive disease ; discontinuation of sunitinib treatment after 20 gy because of neutropenia , this time not coinciding with anemia . during the following treatment break , the blood counts completely recovered , but the thymoma lesions slowly progressed , which was associated with increased pain and deterioration of the patients general condition . 
at the same time , the patient developed a severe neutropenia ; the lowest wbc count at presentation was 1.290 3 109 / l with bands accounting for 8% , segmented cells 12% , basophils 2% , monocytes 15% , and lymphocytes 62% . 
immunoglobulin g was decreased ( 420 mg / dl ) ; c - reactive protein and c3d levels were increased , and procalcitonin was repeatedly normal . the patient had not received any thymoma - specific systemic therapy or radiotherapy for approximately fig 1 . 
the patient had taken valproic acid for epilepsy since adolescence . bm examination showed hypoplasia and a marked left shift of the granulopoiesis with almost complete absence of mature granulocytes ( fig 1 ) , which was associated with hyperplasia of the erythropoiesis and megakaryopoiesis , and an interstitial t - cell infiltration ( cd1a , predominantly terminal deoxynucleotidyl transferasenegative )  . in the blood , the cd4 : cd8 and tcr alpha / beta : gamma / delta cell ratios were slightly decreased ( table 2 )  . 
although a low cd4 : cd8 ratio as a result of the relative increase of cd8 + cells has been inconsistently described in patients with thymoma , 24 , 25 our patient had normal cd8 + cell counts . 
no clonal tcr gamma rearrangement was detected . in the search for granulocyte autoantibodies , we performed granulocyte agglutination ( gat ) and granulocyte immunofluorescence tests ( gifts ; table 1 )  . 
in enzyme immunoassays , no reactions were observed against hla class i antigens or human neutrophil antigens cd16b , cd11a , cd11b / cd18 , and cd177 . the neutropenia repeatedly displayed prompt but short - lasting responses to granulocyte colony - stimulating factor application . 
this decision was based on the efficacy of sunitinib against thymoma , 18 , 19 our reluctance to apply chemotherapy during neutropenia , and consideration of the immunomodulatory effect of sunitinib.21 - 23 we decided to use sunitinib at a dose of 25 mg / day because adverse effects were common at higher doses in patients with thymoma18 and in 6 - week cycles ( 4 weeks of treatment followed by 2 weeks without treatment )  . sunitinib treatment was associated with a rapid increase in neutrophil counts and decrease in inflammation parameters and granulocyte antibodies ( table 1 )  . 
moreover , the computed tomography scan showed stable disease . because adverse effects had been minimal during cycle 1 , we increased the dose to 37.5 mg / day in cycle 2 , which resulted in mucositis , sinus arrhythmia , and decreased left ventricular contractility , all of which improved during treatment break . 
from cycle 3 on , we kept the sunitinib dose at 25 mg / day and used an alternative application schedule ( ie , 3 - week cycles consisting of 2 weeks of treatment and 1 week without treatment , in accordance with a current trial [ nct01621568 ; sunitinib for advanced thymus cancer following earlier treatment ] )  . 
subsequent treatments included paclitaxel and gemcitabine . at the last follow - up , approximately 4 months after sunitinib was stopped , the patient remained without neutropenia and no granulocyte antibodies were detected . the rationale for the initial trials of sunitinib in patients with thymoma was the expression and mutation profile of distinct signaling molecules . in retrospective analyses of the thymoma biopsy from the diagnosis , immunohistochemistry showed weak expression of vegfr1 and vegfr2 and no expression of kit . 
in miseq ( illumina , san diego , ca ) - based sequencing of thymoma cells microdissected on the basis of their morphology , no variants were identified in the genes analyzed ( table 1 )  . sunitinib alters the ctla4 expression on cd8 + t cells and pd1 expression on regulatory t cells in patients with thymoma , and low ctla4 and decrease of pd1 are associated with shorter survival among patients with thymoma who are treated with sunitinib.18 although we have no data on pd1 or ctla4 , immunohistochemistry showed moderate to high pd - l1 expression on the thymoma cells . discussion the patient was diagnosed with thymoma b2 in masaoka stage iva ; he developed prca under radiotherapy , which resolved with corticosteroid treatment , and ain under progression of the thymoma , which resolved with sunitinib treatment . although we cannot exclude with certainty another cause for the ain besides the thymoma , the causative relationship is supported by the simultaneous occurrence of the ain and the progression of the thymoma and by the previous reports describing the development of ain in patients with thymoma.1 - 16 considering that the etiology of thymomaassociated ain is a matter of debate , we here demonstrate a clear association between neutrophil counts and the detection of autoantibodies against granulocytes that were present at diagnosis and disappeared under treatment . one may speculate that the neutropenic episodes under radiotherapy that were once associated with prca may have been temporary occurrences of the ain . 
however , bm findings ( ie , hypoplastic erythropoiesis , maturing granulopoiesis ) and the rapid and stable wbc recovery without immunosuppressive therapy suggest that these neutropenic episodes were indeed related to radiotoxicity . to the best of our knowledge , this is the first description of a thymoma - associated autoimmune disorder that resolved under sunitinib . 
in the study by thomas et al , 18 two patients developed prca or hypogammaglobulinemia while receiving sunitinib ; three patients had autoimmune disorders before receiving sunitinib and not during treatment , but it was not specified whether these disorders were present when sunitinib therapy was started ( as opposed to earlier ) and then improved under therapy . because our report is based on clinical observations , we cannot exclude that the neutropenia only coincidentally improved during sunitinib treatment . 
sachs no relationship to disclose konrad aumann research funding : novartis ( inst ) travel , accommodations , expenses : novartis rainer claus honoraria : janssen oncology , roche , novartis consulting or advisory role : roche , janssen oncology speakers bureau : janssen oncology travel , accommodations , expenses : janssen oncology , abbvie , roche nikolas von bubnoff honoraria : novartis , bristol - myers squibb consulting or advisory role : novartis research funding : novartis travel , accommodations , expenses : novartis cornelius f . 
waller consulting or advisory role : mylan , teva , boehringer ingelheim , bristol - myers squibb , astrazeneca , msd , roche travel , accommodations , expenses : bristol - myers squibb acknowledgment we thank ingrid bartsch for flow cytometry analyses and the molecular tumor board ( medical center , university of freiburg , germany ) for the thorough and elaborate discussion of the case . 
schweiz med wochenschr 97 : 1606 - 1611 , 1967 jacobson bm , castleman b : case 1 - 1971anemia , granulocytopenia and terminal sepsis in a 70 - year - old woman . n engl j med 284 : 39 - 47 , 1971 4 . 
nagashima s , yamato h , saito k , et al : cd8 + agranular lymphocyte proliferative disorder with t - cell receptor betachain gene rearrangement associated with thymoma and neutropenia [ in japanese ]  . 
mathieson pw , oneill jh , durrant st , et al : antibody - mediated pure neutrophil aplasia , recurrent myasthenia gravis and previous thymoma : case report and literature review . 
kobayashi m , hasegawa t , iwabuchi s , et al : the effect of thymectomy on myasthenia gravis , thrombocytopenia , and granulocytopenia associated with thymoma : report of a case . 
hirokawa m , sawada k , fujishima n , et al : long - term response and outcome following immunosuppressive therapy in thymoma - associated pure red cell aplasia : a nationwide cohort study in japan by the prca collaborative study group . 
thomas a , rajan a , berman a , et al : sunitinib in patients with chemotherapy - refractory thymoma and thymic carcinoma : an open - label phase 2 trial . 
finke jh , rini b , ireland j , et al : sunitinib reverses type - 1 immune suppression and decreases t - regulatory cells in renal cell carcinoma patients . 
ozao - choy j , ma g , kao j , et al : the novel role of tyrosine kinase inhibitor in the reversal of immune suppression and modulation of tumor microenvironment for immune - based cancer therapies . 
gu y , zhao w , meng f , et al : sunitinib impairs the proliferation and function of human peripheral t cell and prevents t - cell - mediated immune response in mice . 
hoffacker v , schultz a , tiesinga jj , et al : thymomas alter the t - cell subset composition in the blood : a potential mechanism for thymoma - associated autoimmune disease . 
rod rassekh , md , mhsc5 ; rebecca deyell , md5 ; jennifer rauw , md1 ; meg knowling , md2 ; kong khoo , md6 ; ursula lee , md6 ; krista noonan , md6 ; jason hart , md1 ; r . 
taylor2 ; simon chan , msc2 ; karen mungall2 ; eric chuah2 ; yongjun zhao , dvm2 ; andrew mungall , phd2 ; richard moore , phd2 ; howard lim , phd2 ; daniel j . 
jones , phd2 ; marco marra , phd2 ; and janessa laskin , md2 purpose this study investigated therapeutic potential of integrated genome and transcriptome proling of metastatic sarcoma , a rare but extremely heterogeneous group of aggressive mesenchymal malignancies with few systemic therapeutic options . methods forty - three adult patients with advanced or metastatic non - gi stromal tumor sarcomas of various histology subtypes who were enrolled in the personalized oncogenomics program at bc cancer were included in this study . 
fresh tumor tissues along with blood samples underwent whole - genome and transcriptome sequencing . results the most frequent genomic alterations in this cohort are large - scale structural variation and somatic copy number variation . 
outlier rna expression as well as somatic copy number variations , structural variations , and small mutations together suggest the presence of one or more potential therapeutic targets in the majority of patients in our cohort . 
point mutations or deletions in known targetable cancer genes are rare ; for example , tuberous sclerosis complex 2 provides a rationale for targeting the mammalian target of rapamycin pathway , resulting in a few patients with exceptional clinical benet from everolimus . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction adult sarcoma is one of the most difcult cancer types to study in the clinical trial setting , owing to its rarity along with complexity and heterogeneity in histology , tissue origin , and molecular subtypes . 
although improved survival is seen over time in metastatic sarcoma , the prognosis continues to be poor , with a median overall survival of approximately 18 months.1 the genomic prole of adult sarcomas was recently unveiled by a comprehensive genomic study published by the cancer genome atlas ( tcga ) consortium.2 unlike other cancer types , adult sarcomas are characterized by a predominance of copy number variations ( cnvs ) , with relatively few single - nucleotide variants ( snvs ) .2 however , these data were limited to localized primary disease in only six major sarcoma subtypes and did not explore any direct correlation with potential targeted therapies . targeted oncological therapeutics based on genomic proling ( ie , personalized cancer medicine ) , despite many controversies , seem to improve clinical outcome of patients with multiple cancer types . 
 feng et al context key objective using whole - genome and transcriptome sequencing technology , we attempt a systemic analysis of comprehensive proling on a cohort of 43 patients with metastatic non - gi stromal tumor sarcomas to identify therapeutic implication . knowledge generated our data showed large - scale structural variant aberration is the primary mechanism of mutagenesis in metastatic sarcoma . 
in addition , we reported cases of clinical outcomes of personalized oncogenomicsdirected therapy and demonstrated the clinical utility of genomic proling in metastatic sarcomas . furthermore , we reported several novel mutational signatures in metastatic sarcomas , one of which is homologous recombination deciency signature that may associate with superior sensitivity to double - strand dnadamaging agents in several sarcoma subtypes . relevance our results support the use of genomic data in precision medicine and clinical trial design to improve care for patients with metastatic sarcoma . 19 distinct types of advanced metastatic sarcoma as part of the personalized oncogenomics ( pog ) project ( clinicaltrials.gov identier : nct02155621 ) at bc cancer in canada . 
these represent cases refractory to standard therapies that were genomically analyzed with the aim to identify molecular aberrations amenable to a clinically approved targeted therapy or a theoretical targeted therapy under investigation in clinical trials . 
clinical benet of pogdirected therapy was determined by radiographic response on the basis of response evaluation criteria in solid tumors ( recist ; version 1.1 ) and / or progression - free survival of 6 months or more . methods patient samples as previously described , 5 , 6 candidate patients enrolled in pog underwent metastatic tumor biopsies and peripheral blood collection for comparison with detected somatic alterations . 
genome libraries from tumors and blood samples ( normal control ) as well as transcriptome libraries from tumors were constructed using protocols previously described.7 , 8 all patients provided written informed consent for tumor biopsies , blood sample collection , genomic proling , data analysis , and publication of results as part of pog of british columbia approved by the university of british columbia research ethics committee ( reb# h12 - 00137 ) and registered ( clinicaltrials.gov identier : nct02155621 )  . 
raw sequence data and downstream analytics were maintained within a secure computing environment . whole - genome and transcriptome sequencing and bioinformatics paired - end reads from all libraries were generated on illumina hiseq2000 or hiseq2500 sequencer ( illumina , san diego , ca )  . 
determination of somatic snvs , structural variants ( svs ) , cnvs , and gene expression was performed as previously described.5 , 6 transcript outlier expression was determined either by a greater than or a less than two - fold change against tumor illumina bodymap ( arrayexpress id : e - mtab - 513 ) or percentile less than 10% or greater than 90% ( tumor v compendium of tcga ; nih.gov / tcga / )  . 
for gene expression clustering , data were t using the deseq2 package , and hierarchical clustering of log - transformed reads per kilobase of transcript per million mapped reads was performed for genes signicant at an adjusted p value threshold of .01 ( euclidean distance , complete linkage clustering )  . 
the common histologies in this cohort were leiomyosarcoma ( lms ; nongynecologic : n = 7 [ 16% ] and gynecologic : n = 3 [ 7% ] ) , osteosarcoma ( osa ; n = 5 [ 12% ] ) , undifferentiated pleomorphic sarcoma ( ups ; n = 5 [ 12% ] ) , dedifferentiated liposarcoma ( ddlps ; n = 4 [ 9% ] ) , and ewing sarcoma ( n = 3 [ 7% ] ; table 1 )  . 
there were 29 male patients ( 67% ) and 14 female patients ( 33% ) , with a median age at time of metastatic diagnosis of 55 years ( range , 18 to 79 years )  . 
in this cohort , 28 of 43 patients ( 65% ) had received one standard systemic treatment of advanced metastatic disease at the time of sequencing biopsy , and 15 of 43 patients ( 35% ) had received multiple lines ( range , 2 to 7 )  . 
details of standard systemic treatments received in this cohort are described in appendix table a1 . at the time of data analysis , 26 of 43 patients ( 60% ) were deceased , and 17 of 43 ( 40% ) were still alive . potentially targetable alterations in a heterogeneous sarcoma cohort we sought to systematically characterize the genomic landscapes of adult metastatic sarcomas in this heterogeneous cohort and explore how these landscapes relate to therapeutic approaches . 
however , this level of information can potentially be used to inform treatment options for therapies currently available . overall clinical outcome of pog - directed therapy of 42 patients with potentially targetable alterations , 18 ( 43% ) patients attempted pog - directed therapies either in the clinical trial setting or through a compassionate access these , eight of 18 patients ( 44% ) program ( cap )  . 
of derived clinical benet from pog - directed therapy ( table 2 ) and are described in case series of patients who derived clinical benet from pog - directed therapy . response could not be assessed in four cases ( 22% ) owing to short duration ( 2 weeks ) on pog - directed toxicities and / or deterioration of therapies because of performance status ( appendix table a2 )  . 
there were six patients ( 33% ) considered nonresponders to pogdirected therapies , including tyrosine kinase inhibitors , histone deacetylase inhibitors , and immunotherapies ( appendix table a2 )  . 
this result is comparable to a recent study using genomic proling in the clinical setting.15 case series of patients who derived clinical benet from pog - directed therapy infrequent tsc2 mutation / deletion has cases 1 and 2 : therapeutic implications for mammalian target of rapamycin inhibitors . 
case 1 is a 62 - year - old male who presented with recurrent metastatic renal epithelioid angiomyolipoma with lung , liver , peritoneum , and bone metastases ( table 2 )  . 
pog identied a tsc2 pathologic truncating mutation , a relatively well - known event.18 everolimus was given through cap , yielding prolonged partial response ( pr ; appendix fig a3 ) as predicted and continued to show response at 15 months of therapy at the time of analysis . case 2 is a 57 - year - old female who presented with a large right upper lobe mass with mediastinal / hilar lymphadenopathy and pleural effusion and was diagnosed with undifferentiated round cell sarcoma . 
however , the above two cases suggest that the landscape of small mutations and deletions , although rare , has therapeutic relevance in some sarcoma subtypes . our systematic analysis of somatic events based on wholegenome sequencing reveals that the most frequent recurrent alterations in this cohort of adult metastatic sarcomas occur through large - scale structural changes in the genome ( fig 2a ) , rather than through point mutations or small deletions that are frequent in many other cancer types , 20 with a few exceptions of known tumor suppressor genes including tp53 ( approximately 30% ; 13 of 43 ) , atrx ( approximately 12% ; ve of 43 ) , and rb1 ( approximately 7% ; three of 43 ; fig 2b )  . 
 personalized oncogenomics of adult metastatic sarcoma case 3 : targeting common oncogenic amplications such as mouse double minute 2 homolog and cyclin - dependent kinase 4 may have therapeutic implications . 
she subsequently had a pr to a combination of mdm2 and cdk4 inhibitors in a phase ib / ii clinical trial ( clinicaltrials.gov identier : nct02343172 ) and continued to receive therapy for approximately 1 year before death as a result of disease progression . 
although the synergistic effect of mdm2 and cdk4 inhibitors remains controversial22 , 23 pending ongoing clinical trials , the case of this exceptional responder provides rationale for investigating and targeting these genomic abnormalities in this tumor and possibly other sarcoma types . recurrent amplications have been described as a common feature in genomically complex sarcoma subtypes.2 , 24 the canonical 12q13 - 15 amplications targeting mdm2 / cdk4 were observed in ddlps , with an additional case of highgrade osa also harboring this event , suggestive of a dedifferentiated osa arising from a low - grade osa with mdm2 amplication.25 amplication of the oncogene myc on 8q24 was also observed in three of 43 sarcomas . 
the most common region of amplication across this adult sarcoma cohort is 17p11 - 12 altered in 42% ( 18 of 43 ) of cases ( figs 3a and 3b )  . 
strikingly , when we examined the frequency of our recurrent amplication events across tcga cancer types , the amplication on 17p11 - 12 was found to be highly sarcoma specic , which is rarely observed in other tumor types ( fig 3c )  . 
furthermore , the 17p11 - 12 amplicon has been previously described only in osa26 , 27 and lms.28 in our study , this amplicon is observed in a variety of sarcoma subtypes , including ddlps , pleomorphic liposarcoma , osa , lms , chordoma , ups , and undifferentiated endometrial sarcoma ( ues ) , suggesting it harbors an oncogene that is important for sarcoma tumorigenesis . myocd , pmp22 , and cops3 are believed to be potential oncogenic targets within this amplicon in lms and osa.26 - 28 we examined transcriptome expression data for potential oncogenic targets in this region ( fig 3d )  . 
myocd and pmp22 are both within the region most frequently amplied in this cohort , with myocd showing particularly higher expression in amplied samples and pmp22 showing higher expression overall and compared with many other in addition , adora2b was noted as having tumors . amplicon - associated expression ; this gene has not previously been examined as a potential target for this amplicon , but it has been reported to have growth - promoting properties in oral and breast cancers.29 , 30 this analysis suggests that additional functional analysis of genes within this amplicon is required to clearly dene the oncogenic target ( s )  . there are few therapies available that to date , target common amplications in metastatic sarcomas . 
the future development of therapies targeting recurrent amplications such as 17p11 - 12 may be warranted , potentially improving therapeutic options in this disease . case 4 , 5 , and 6 : mutation signatures and homologous recombination deciency may delineate sarcoma subtypes and indicate sensitivity to certain dna - damaging agents . mutation signatures are characteristic patterns of mutation , which may result from specic cellular or environmental pressures and may have implications for therapy.12 the most comprehensive validated set of mutation signatures described to date is reported in cosmic ( sanger.ac.uk / cosmic / signatures )  . 
on the basis of singlenucleotide alterations , we performed mutation signature detection in our sarcoma cohort and identied eight signatures through this de novo process , denoted v1 to v8 ( appendix fig a6 )  . 
comparison of discovered sarcoma signatures to the 30 previously described mutation signatures reported in cosmic31 revealed that sarcoma signatures v1 , v3 , v4 , v5 , v6 , and v8 matched signatures 30 , 5 , 2 , 1 , 8 , and 9 , respectively ( fig 4 )  . 
for example , ddlps possessed similar rearrangement proles , with elevated signature r1 and high mutation burden . signatures v6 and v7 matched signatures 3 and 8 , both of which are associated with hrd signature , 31 also known as brcaness , which has been well described in breast , fig 2 . 
genomic structural complexity is calculated as the average of the proportion of copy segments that are nondiploid and the proportion of the genome represented in nondiploid copy segments , similar to that per the cancer genome atlas research network.2 ( b ) oncoprint of recurrent somatic dna alterations in cancer - related genes observed in sarcomas , grouped by sarcoma subtype . 
types of gene alterations include amplication ( red ) , homozygous deletion ( blue ) , gene fusion ( purple ) , truncating mutation ( black ) , or missense mutation ( green )  . 
 personalized oncogenomics of adult metastatic sarcoma ovarian , and other relatively common cancer types32 including osa.33 we further computed hrd indices and found that in addition to osa , high hrd scores were also seen in lms , ues , and a few other sarcoma subtypes ( fig 4 )  . 
the brcaness phenotype in lms that we observed is consistent with a recent report.34 interestingly , we did not observe deleterious genomic or transcriptomic aberrations of genes such as brca1 and brca2 , which have been described as accounting for the majority of hrd signatures in other tumor types . 
we do observe losses , svs , or downregulated expression of various components implicated in the homologous recombination repair pathway , such as pten , atm , and rad51 ( data not shown ) , suggesting potential alternative contributions to the hrd signature . 
a clear - cut relationship between genetic aberrations and hrd signature is also not observed in other studies.12 , 31 case 4 is a 44 - year - old woman who presented with metastatic ues with lung metastasis . 
the response to ifosfamide was not long - lasting , like all other chemotherapies , and both patients eventually experienced progression , did not respond to any additional treatment , and died as a result of disease progression . 
the hrd signature or brcaness phenotype is associated with therapeutic response to dna - damaging agents , including platinum - based chemotherapies.12 although platinums are not generally used in metastatic soft tissue sarcomas , the dna damaging chemotherapeutic agent ifosfamide has similar , though less - pronounced , dna crosslinking effects . although ifosfamide is an active drug in various sarcoma subtypes , with an overall response rate between 10% and 40% depending on dosing schedule , single - agent response is generally considered low ( , 10% ) , especially in the third - line setting or beyond for sarcomas aside from synovial sarcoma.35 we speculate that the response may relate to partial dna cross - linking property of ifosfamide alkylating agent , which may have therapeutic advantage in hrd tumors . case 6 is 53 - year - old man who presented with recurrent metastatic splenic vein lms with liver and lung metastasis . his disease progressed through docetaxel plus gemcitabine treatment . 
because of a similar hrd signature identied through pog study , he was enrolled in a phase i clinical trial ( clinicaltrials.gov identier : nct02873975 ) investigating an experimental drug ( prexasertib ) targeting hrd tumors . 
these cases support the clinical utility of genomic analysis of hrd and mutation signatures across sarcoma subtypes . case 7 and 8 : potentially targetable aberrations identied solely through transcriptome / expression analysis . 
case 7 is a 77 - year - old male presenting with recurrent multiple intraabdominal ups , which progressed through two cycles of doxorubichis tumors exhibited high rna expression of various tyrosine kinase receptors , such as plateletderived growth factor receptors ; therefore , sunitinib was attempted through cap . 
he then received pog - directed therapy in the form of sunitinib on the basis of his tumor exhibiting high rna expression of fms - like tyrosine kinase 3 and colony - stimulating factor 1 receptor . 
expression in amplicon refers to log ( reads per kilobase of transcript per million mapped reads ) ; increase in amplied samples is measured as expression in amplied samples divided by expression in nonamplied samples in this cohort ; expression percentile is determined relative to all tcga tumors ( see methods )  . 
 ( a ) structural variant ( sv ) mutation signatures ( r1 to r4 ) and single - nucleotide variant ( snv ) mutation signatures ( v1 to v8 ) were deciphered de novo from metastatic sarcomas . 
three dedifferentiated liposarcomas demonstrated high sv and snv burden , with similar r1 rearrangement signature and signatures v4 , v5 , and v6 . signature v4 matched catalogue of somatic mutations in cancer ( cosmic ) signature 2 and is known to be associated with apobec deamination . 
 ( b ) three sarcoma cases ( labeled in red ) with elevated homologous recombination deciency ( hrd ) score and / or the hrd - associated signature 3 demonstrated response to double - strand dnadamaging chemotherapy . 
 ( c ) mutation signatures deciphered de novo from sarcomas were compared against 30 canonical signatures from the cosmic using the cosine similarity metric . signatures that map most closely to a cosmic signature are highlighted . 
 personalized oncogenomics of adult metastatic sarcoma selection who had these two histology subtypes.36 , 37 taken together , these results support the notion that drug efcacy may be dictated by biology measurable through gene expression biomarkers in addition to histology subtype . furthermore , these data support additional research on these putative biomarkers in the context of a complex signaling network , which may help advance the drug development of various tyrosine kinase inhibitors in future sarcoma clinical trials . immune landscape of sarcoma subtypes despite being regarded as a poorly immunogenic tumor because of relatively low mutation burden compared with other cancer types , 2 checkpoint inhibitor immunotherapies have produced promising durable response in a few sarcoma histology subtypes such as ups and alveolar soft part sarcoma thus far.38 , 39 pd - l1 expression has been correlated with efcacy of immunotherapy in some , but not all , cancer types40 and reported as a prognostic marker in soft tissue and bone sarcoma , 41 , 42 but it has not yet been shown to correlate with immunotherapy sensitivity in sarcoma.43 the tumor immune microenvironment plays a key role in determining immunotherapy sensitivity , and emerging data demonstrated a positive correlation between clinical response and preexisting tumor immune microenvironment.44 we examined immune inltration on the basis of gene expression proles ( see methods ) and observed that a subset of tumors show high iiss ( fig 5 ; appendix fig a9 )  . 
we did not observe any correlation between high level of pd - l1 expression and immunotherapy response in a small number of cases ( n = 4 ) within our cohort . interestingly , of the four patients in our cohort treated with immunotherapies , the only patient ( case 8 , lms ) who exhibited some response to immunotherapy also demonstrated an unusually high iis ( fig 5 ; table 2 )  . 
two other cases with high iis , both ups , were not treated with immunotherapy , and two other sarcomas that were treated with immunotherapy , an lms and an osa , had low iis and did not respond . 
overall , our experience suggests that although iis alone may not be sufcient as a predictive biomarker for immunotherapy in investigation , all sarcoma types , particularly in lms . it warrants additional cases 9 and 10 : detection of fusion genes assists in sarcoma diagnosis and therapeutic intervention . 
t - cell inltration score is the sum of all t - cell subtypes excluding regulatory t cells , which are negative modulators . immune inltration score is the sum of scores for all 22 immune cell types proled . 
arms , alveolar rhabdomyosarcoma ; asps , alveolar soft part sarcoma ; ccs , clear cell sarcoma ; chsa , chondrosarcoma ; ddlps , dedifferentiated liposarcoma ; eaml , epithelioid angiomyolipoma ; ews , ewing sarcoma ; mlps , myxoid liposarcoma ; mpnst , malignant peripheral nerve sheath tumor ; msft , malignant solitary brous tumor ; osa , osteosarcoma ; other , groups urs , plps , mlps , ccs , mpnst , eaml , arms , ss , chsa , asps , and sef ; plps , pleomorphic liposarcoma ; sef , sclerosing epithelioid brosarcoma ; ss , synovial sarcoma ; stlms , nongynecologic leiomyosarcoma ; ues , undifferentiated endometrial sarcoma ; ulms , gynecologic leiomyosarcoma ; ups , undifferentiated pleomorphic sarcoma ; urs , undifferentiated round cell sarcoma . sarcoma and change to standard alternating multi - agent chemotherapies with substantial pr . 
her systemic disease also responded to second - line and third - line standard chemotherapies for ewing sarcoma , but she eventually developed brain metastasis and died as a result of disease progression . case 10 is a 68 - year - old man presenting with recurrent metastatic osa ( initial pathologic diagnosis ) of the right femur with lung metastasis . 
 feng et al rapid deterioration shortly after this diagnosis was made from genomic analysis and died as a result of disease progression . within our cohort , in all cases where a fusion would be expected based on pathologic features , we observed a fusion consistent with the sarcoma type ( appendix table a3 )  . the exceptional above two cases , where we identied fusions that had not initially been expected based on pathology , support the utility of genomic proling in rening sarcoma diagnosis and therapeutic intervention , echoing the results of a large retrospective study.17 conclusion our data lend additional support to the current literature data showing that sv and cnv are the primary mechanisms of mutagenesis in sarcomas , as opposed to single - nucleotide alteration . 
we provide anecdotal evidence showing the potential of genomic alterations , such as loss of tsc2 and amplication of mdm2 / cdk4 , to predict exceptional response to targeted treatments . 
overall , we were able to identify potentially actionable genomic alterations in the majority of cases , largely on the basis of outlier rna expression and cnv and sv aberrations . 
renouf , karen gelmon , stephen yip , marco marra , janessa laskin data analysis and interpretation : xiaolan feng , erin pleasance , eric y . zhao , tony ng , jasleen k . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . xiaolan feng honoraria : astrazeneca , nanostring / innomar strategies consulting or advisory role : astrazeneca , ipsen , genomic health , nanostring / innomar strategies , roche tony ng honoraria : nanostring technologies travel , accommodations , expenses : nanostring technologies sara k . 
 personalized oncogenomics of adult metastatic sarcoma krista noonan consulting or advisory role : merck , sano canada , bristol - myers squibb , janssen , pzer , astrazeneca speakers bureau : merck stephen yip consulting or advisory role : bayer , pzer , roche research funding : pzer , bayer , roche , foundation medicine travel , accommodations , expenses : bayer , roche , pzer jason hart honoraria : novartis martin jones employment : qiagen , thermo fisher scientic ( i ) howard lim honoraria : eli lilly / imclone systems , ipsen , merck , roche canada , eisai , taiho pharmaceutical , bristol - myers squibb canada travel , accommodations , expenses : eisai , taiho daniel j . 
renouf honoraria : celgene , servier , taiho pharmaceutical , ipsen , shire research funding : bayer ( inst ) , astrazeneca ( inst ) karen gelmon honoraria : astrazeneca , merck sharp & dohme consulting or advisory role : pzer , novartis , astrazeneca , merck , eli lilly , bristol - myers squibb , nanostring technologies , genomic health , janssen oncology , roche , mylan research funding : pzer ( inst ) , bristol - myers squibb ( inst ) , astrazeneca ( inst ) , roche ( inst ) expert testimony : genentech marco marra travel , accommodations , expenses : roche canada janessa laskin honoraria : boehringer ingelheim , roche canada , astrazeneca , pzer research funding : astrazeneca ( inst ) , roche canada ( inst ) no other potential conicts of interest were reported . acknowledgment we thank katherine mui , jessica nelson , and lindsay zibrik from the personalized oncogenomics ( pog ) program for coordinating our study . this work would not be possible without the participation of our patients and families , the entire pog team , and the generous support of the bc cancer foundation and genome british columbia ( project b20pog )  . 
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the number of potentially targetable alterations was determined by comparing observed somatic mutations and gene expression alterations to a database of events that have clinical or preclinical evidence of potential therapeutic targeting , on the basis of therapeutics currently available or in development . mutation copy number expression only samples with potentially targetable alterations ( % ) fig a2 . 
samples with potentially targetable alterations were determined by comparing observed somatic mutations and gene expression alterations to a database of events that have clinical or preclinical evidence of potential for therapeutic targeting , on the basis of therapeutics currently available or in development . 
 feng et al baseline before standard chemotherapy ( april 2016 ) progression after standard chemotherapy ( august 2016 ) response to pog - directed therapy ( july 2017 ) fig a3 . 
 personalized oncogenomics of adult metastatic sarcoma baseline before standard chemotherapy ( january 2015 ) progression after standard chemotherapy ( may 2015 ) response to pog - directed therapy ( december 2015 ) fig a4 . 
annotation tracks show exposure values calculated from mutation analysis ( structural variant [ sv ] , single - nucleotide variant [ snv ] burden ) , clinical covariates , and histologic properties of the sarcoma cohort . 
 feng et al baseline before standard chemotherapy ( august 2015 ) progression after standard chemotherapy ( july 2016 ) response to pog - directed therapy ( october 2016 ) fig a7 . 
 personalized oncogenomics of adult metastatic sarcoma baseline ( feb 2015 ) progression after standard chemotherapy ( april 2015 ) response to pog - directed therapy ( october 2015 ) fig a8 . 
other than undifferentiated pleomorphic sarcoma ( ups ) , some leiomyosarcoma ( lms ) and dedifferentiated liposarcoma ( ddlps ) and one case of synovial sarcoma ( ss ) seem to have relatively high iis compared with others . 
 impact of genetic ancestry on outcomes in ecog - acrin - 5103 purpose racial disparity in breast cancer outcomes exists between african american and white women in the united states . 
we have evaluated the impact of genetically determined ancestry on disparity in efficacy and therapy - induced toxicity for patients with breast cancer in the context of a randomized , phase iii adjuvant trial . methods this study compared outcomes between 386 patients of african ancestry ( aa ) and 2 , 473 patients of european ancestry ( ea ) in a randomized , phase iii breast cancer trial , ecogacrin - 5103 . 
the primary efficacy end point , invasive diseasefree survival ( dfs ) , and clinically significant toxicities were compared , including anthracycline - induced congestive heart failure , taxane - induced peripheral neuropathy ( tipn ) , and bevacizumab - induced hypertension . results overall , aas had significantly inferior dfs ( p = .002 ; hazard ratio , 1.5 ) compared with eas . 
2017 by american society of clinical oncology introduction african american patients with breast cancer have inferior efficacy outcomes compared with other races.1 , 2 the reason for this imbalance is multifactorial and includes higher stage , higher grade , more triple - negative breast cancer ( tnbc ) , and poorer responsiveness to chemotherapy.3 , 4 these clinical imbalances have previously been attributed to both socioeconomic factors and a different underlying biology of the tumor.2 , 5 patients of african ancestry ( aa ) also experience more adverse drug reactions , including an increase in clinically important toxicities for chemotherapeutic agents . 
although less well characterized , these toxicity disparities are also likely multifactorial and include inherited genetic variation and comorbidities , among other factors.6 - 10 much of the prior work has been based on selfreported race . 
 node - negative breast cancer to intravenous doxorubicin and cyclophosphamide ( ac ) every 2 or 3 weeks ( at discretion of treating physician ) for four cycles followed by 12 weeks of paclitaxel ( 80 mg / m2 once per week ) alone ( arm a ) or to the same chemotherapy with either concurrent bevacizumab ( arm b ) or concurrent plus sequential bevacizumab ( arm c ) ; figure 1a . 
patients with estrogen receptor ( er ) positive disease were ln positive , had a tumor > 5 cm or a tumor measuring 1 to 5 cm , with a recurrence score > 11 . genome - wide association study germline dna from whole blood and companion clinical outcome data were available in 3 , 126 patients . 
if arm c significantly improved dfs relative to arm a , then in the second step , a comparison of arm b with arm a was performed.14 in this correlative study , dfs and overall survival ( os ) were evaluated using kaplan - meier methodology . 
the differences in outcomes between aas and eas were compared with the application of cox proportionalhazards models using either univariate or multivariate analysis , which were corrected with significant covariates . 
to identify the best regression model , a forward and a backward stepwise selection procedure were performed separately to evaluate variable associations , and the akaike information criterion was used to determine the inclusion of potential confounders such as race , menopausal status , age , weight , height , side of cancer involvement , er status , histologic grade , nuclear grade , ln status , type of surgery , types of ac schedule , and dose reductions in ac or paclitaxel . both procedures returned the same model with six predictors , which are listed in the data supplement . dfs was the primary end point of the parent trial ; it was defined as invasive dfs and calculated from the date of random assignment to the date of first treatment failure ( invasive ipsilateral , local / regional invasive , distant recurrence , invasive contralateral breast cancer , invasive nonbreast second primary , or death from any cause [ whichever occurred first ] )  . cases with incomplete follow - up , without a documented invasive dfs event ( including those who developed squamous or basal cell skin cancers or in situ carcinomas of any site as their only event ) were censored at the date of last disease evaluation . 
we previously published biomarker data on each of these toxicities.15 , 17 , 18 in the present study , we sought to compare the frequency of all toxicities between aas and eas and to assess the impact of race on dose modifications . 
statistical analysis was performed using r ( version 3.3.0 ) and the x2 test . odds ratio ( or ) was used to evaluate the significance and magnitude of the differences in the toxicity frequency between aas and eas . chf cases for this study included individuals who had centrally reviewed , cardiologist - adjudicated chf . 
to be selected for inclusion in ecogacrin - 5103 , patients must have had no history of clinically significant cardiovascular disease . cardiovascular health was monitored at the start and during the trial by multigated angiograms or echocardiograms . 
cardiac events included chf , decrease in left ventricle ejection fraction , acute coronary syndrome , supraventricular tachycardia , and myocardial dysfunction diagnosed by a cardiologist . tipn cases for this study were defined as those experiencing either grades 2 to 4 or grades 3 to 4 tipn as assessed by ctcae . 
to serve as a tipn case , the patient must have received at least one dose of paclitaxel , and the neuropathy event must have occurred during treatment or within 3 months of the last dose of therapy . hypertension cases for this study were defined as those experiencing a systolic blood pressure ( sbp )  . 
blood pressure values were collected as part of standard clinical assessment before administration of therapy throughout the conduct of the trial . results genotyped group from ecog - acrin5103 and genetic ancestry a total of 3 , 394 germline dna samples from patients were collected as part of the planned correlative protocol within ecog - acrin5103 ( fig 1b )  . 
the outcomes of the entire genotyped cohort ( all ancestries combined ) used in this correlative study were almost identical to the parent trial4 ( data supplement )  . demographic data and disease comparisons table 1 summarizes the important demographic comparisons between aas and eas . 
we assessed for the differences in the parent trial stratification factors as well as other known outcome predictors , including age , hormone receptor status ( er positive v tnbc ) , ln status , height , weight , type of surgery , and tumor grade . 
there were no significant differences overall in ln status . genetic ancestry as a predictor of efficacy in ecog - acrin - 5103 dfs was the primary efficacy end point of the parent trial . 
an imbalance in associated comorbidities or environmental factors cannot be excluded as a contributing cause , and unfortunately , those data were not collected in ecog - acrin - 5103 . 
dose reductions in paclitaxel also negatively affected dfs for all ancestries ( p = .02 ; data supplement ) ; however , having a dose modification in paclitaxel did not affect dfs for eas , but it did significantly cause an inferior dfs for aas ( fig 4 )  . the difference may have been explained by more severe dose reductions in aas . 
the outcomes for the subgroup genotyped , however , were similar to the parent population , thus minimizing the concern for subgroup bias . we also compared the results of the genetic ancestry with self - reported race , and there was no significant difference in the conclusion . 
work in other disease phenotypes , however , has demonstrated that use of self - reported race as a surrogate for genetic ancestry was not perfect.25 - 27 prior work has demonstrated that  . 
9% of patients cannot supply , or choose not to supply , ancestry information.28 thus , the real impact of accurately self - reported race is probably larger than the 9% that was observed , as the result of misclassification alone . 
although genotype may provide more insight toward underlying biologic diversity , selfreported race still likely represents a reasonable surrogate for genotypic variation in the routine clinical setting for consideration of metabolism and drug toxicity . we previously evaluated genetic markers to predict some of the most clinically important toxicities in ecog - acrin - 5103 : bevacizumabinduced hypertension ( using various definitions ) , tipn , and cardiologist - adjudicated anthracyclineinduced chf.15 , 17 , 18 in this study we compared the likelihood of each of these clinically relevant toxicities between aas and eas . 
these data support prior work from a single - institution retrospective analysis as well as data in pediatric populations that revealed higher likelihood of anthracycline - induced chf in aas . 
similarly , a prior single - institution retrospective analysis demonstrated higher risk of tipn for aas.8 - 10 because aas experience greater toxicity , it is highly unlikely that the imbalance in efficacy is a result of exposure as the result of pharmacokinetic considerations , as the end organs are clearly being affected . 
as expected , all ancestries that had dose reductions in the ac portion of the chemotherapy had inferior dfs ; this difference , however , was present for both eas and aas . 
the significant difference in dfs as the result of paclitaxel dose modifications for aas may have been because of the markedly more severe dose reductions ; this was evidencedby alower meannormalizeddosein thosewho had dose reductions ( p = .03 ) , in large part because table 2 . 
this study did not evaluate socioeconomic factors , which are known to be important variables in outcomes.5 however , in the context of a randomized phase iii trial , many of these inequities are minimized . in conclusion , this study highlights the need to better understand the biologic differences in normal breast biology , tumor biology , and the inherited genetic differences between women of aa and ea . 
it also highlights the need to better personalize counseling when discussing the risk - to - benefit ratio for aas , for whom the disease - specific outcomes are inferior and drug - specific toxicities are higher . 
ecog - 1199 previously demonstrated that the dosing of docetaxel every 3 weeks was as effective but had fewer dose reductions for aas in a similar clinical setting.20 future trials should investigate whether another taxane with less risk of tipn , such as docetaxel , might be more effective for aas in the adjuvant breast cancer setting . 
sparano stock and other ownership interests : metastat consulting or advisory role : genentech , novartis , astrazeneca , celgene , eli lilly , celldex , pfizer , prescient therapeutics , juno therapeutics , merrimack research funding : prescient therapeutics ( inst ) , deciphera ( inst ) , genentech ( inst ) , merck ( inst ) , novartis ( inst ) , merrimack ( inst ) george w . 
sledge jr leadership : syndax stock and other ownership interests : syndax honoraria : symphogen consulting or advisory role : symphogen , coherus biosciences , radius health , peregrine pharmaceuticals , taiho pharmaceutical research funding : genentech ( inst ) travel , accommodations , expenses : nektar , radius health , taiho pharmaceutical kathy d . 
miller consulting or advisory role : nektar , tesaro , merck research funding : genentech ( inst ) , merrimack ( inst ) , entremed ( inst ) , taiho pharmaceutical ( inst ) , macrogenics ( inst ) , medivation ( inst ) , novartis ( inst ) , seattle genetics ( inst ) affiliations support bryan p . 
schneider , fei shen , guanglong jiang , milan radovich , lang li , laura gardner , dongbing lai , tatiana foroud , and kathy d . miller , indiana university school of medicine , indianapolis , in ; anne oneill , dana farber cancer instituteecog - acrin biostatistics center , boston , ma ; joseph a . 
keenan t , moy b , mroz ea , et al : comparison of the genomic landscape between primary breast cancer in african american versus white women and the association of racial differences with tumor recurrence . 
desantis c , jemal a , ward e : disparities in breast cancer prognostic factors by race , insurance status , and education . jama 295 : 2492 - 2502 , 2006 cancer causes control 21 : 1445 - 1450 , 2010 americans . 
kidd rs , curry tb , gallagher s , et al : identification of a null allele of cyp2c9 in an african - american exhibiting toxicity to phenytopharmacogenetics 11 : 803 - 808 , 2001 8 . 
bhatnagar b , gilmore s , goloubeva o , et al : chemotherapy dose reduction due to chemotherapy induced peripheral neuropathy in breast cancer patients receiving chemotherapy in the neoadjuvant or adjuvant settings : a single - center experience . 
cobb rj , thomas cs , laster pirtle wn , et al : self - identified race , socially assigned skin tone , and adult physiological dysregulation : assessing multiple dimensions of race in health disparities research . 
miller k , oneill am , dang ct , et al : bevacizumab ( bv ) in the adjuvant treatment of her2 - negative breast cancer : final results from eastern cooperative oncology group e5103 . 
schneider bp , li l , radovich m , et al : genome - wide association studies for taxane - induced peripheral neuropathy in ecog - 5103 and ecog - 1199 . 
killelea bk , yang vq , wang sy , et al : racial differences in the use and outcome of neoadjuvant chemotherapy for breast cancer : results from the national cancer data base . 
halder i , shriver m , thomas m , et al : a panel of ancestry informative markers for estimating individual biogeographical ancestry and admixture from four continents : utility and applications . 
louwers yv , lao o , fauser bc , et al : the impact of self - reported ethnicity versus genetic ancestry on phenotypic characteristics of polycystic ovary syndrome ( pcos )  . 
mandrekar , phd1 with the launch of the national cancer institutes precision medicine initiative in 2015 , there has been a shift to trial designs that tailor health care solutions to individual patients by using a screening platform and by moving away from the one - trial / one - biomarker - at - a - time approach . 
2019 by american society of clinical oncology introduction precision medicine takes into account the variability of an individual patients genes , environment , and lifestyle when deciding the best approach for disease prevention and treatment.1 since the rst publication of the human genome in february 2001 , 2 scientists have made great progress in understanding inherited differences in genes , making precision medicine a tangible reality . 
even though precision medicine is a relatively new term , tailoring intervention on the basis of a patients specic features is not a new idea . many currently available us food and drug administration ( fda ) approved therapies are based on specic patient subgroups . 
for example , rituximab , the rst monoclonal antibody treatment for cancer , was approved by the fda in 1997 for patients with relapsed or refractory cd20 + , b - cell , low - grade , or follicular non - hodgkin lymphoma . 
the addition of cetuximab to rst - line chemotherapy in patients with kras wild - type metastatic colorectal cancer has been shown to signicantly improve treatment outcomes compared with chemotherapy alone in two randomized clinical trials , crystal ( clinicaltrials.gov identier : nct00154102 ; cetuximab combined with irinotecan in first - line therapy for metastatic colorectal cancer ) 3 and opus ( clinicaltrials.gov identier : nct00125034 ; oxaliplatin and cetuximab in first - line treatment of metastatic colorectal cancer [ mcrc ] ) .4 erlotinib and crizotinib are fda - approved therapies for patients with advanced lung cancer who test positive for an epidermal growth factor receptor ( egfr ) mutation and the alk rearrangement , respectively . 
it was later found that patients with higher programmed death - ligand 1 expression treated with pembrolizumab had longer progression - free survival ( pfs ) and overall survival ( os ) .5 most recently , on may 23 , 2017 , the fda granted accelerated approval to pembrolizumab as the treatment for adult and pediatric patients with unresectable or metastatic microsatellite instability - high or mismatch repair decient solid tumors , 6 which is the rst time that the fda has approved a cancer treatment for an indication on the basis of a common biomarker rather than the primary site or origin ( ie , tissue agnostic ) .7 there are continuing efforts in drug development to move away from the one - size - ts - all approach and toward precision medicine . in this article , we aim to introduce novel trial designs by using case studies as examples . 
 ou et al context key objective to discuss types of clinical trial designs for accelerating development of new drugs in the era of precision medicine . knowledge generated clinical trial designs ( such as umbrella , basket , and subgroup ) that evaluate multiple hypotheses are efcient precision medicine initiatives . 
other designs include enrichment designs for validating the efcacy of an agent in biomarker - driven subgroups and window of opportunity designs to help understand the antitumor activity of an agent in a treatment - naive patient population . relevance the clinical trial designs discussed in this article are practical and relevant for precision medicine trials . 
several case studies are provided to demonstrate the utility of these clinical trial designs . the results of tumor gene sequencing or other testing techniques , such as polymerase chain reaction , ow cytometry , uorescence in situ hybridization ( fish ) , chromogenic in situ hybridization , and immunohistochemistry . 
specic to genotype - driven trials , patients will be matched to trials that are developed on the basis of prior understanding of certain molecular aberrations that may determine sensitivity to certain therapies . 
if a patient is eligible for more than one genotype - driven trial , the trial will be selected by the treating physician on the basis of the totality of information , such as the patients preferences and status , expected benets , and molecular characteristics . 
enrichment designs test selective therapeutic options for matching patients that can result in better patient outcomes.9 the genotype - driven trial mentioned in the case study is one type of enrichment design ; other types of enrichment , such as that based on the epigenome , is also appropriate . 
enrichment trial design is best suited when the rationale for the trial strongly suggests that the agent would be effective in a specic biomarkerdened patients with a specific tumor type with biomarker status unknown may be part of the trial protocol biomarker profiling with targeted biomarker trial enrollment with targeted therapy without targeted biomarker standard of care fig 1 . 
it is particularly advantageous if the biomarker used to dene the patient population is considered soc ; if so , the trial design does not need to take into account the molecular testing because the information would be available for all patients . 
highly specic screening tests are required to identify the low - prevalence molecular prole and to avoid assigning patients who tested false positive to treatment options that may not be efcacious . 
finally , certain molecular proles may have low prevalence and may result in a large proportion of screened patients receiving the soc , which can be inefcient ( eg , if the prevalence of the molecular prole of interest is only 5% , 500 patients will need to be proled to identify 25 patients who are potentially eligible )  . umbrella design umbrella trials include patients with a single tumor type or disease and for which several biomarkers have been identied and used to dene disease subtypes.10 patients are screened for a panel of biochemical , genetic , and / or immunologic markers associated with their disease and , on the basis of the markers detected , assigned to a biomarkerdriven treatment strategy or targeted therapy that is most likely to result in favorable outcomes . 
thus , an umbrella trial consists of multiple substudies , each with independent subgroups of patients receiving different therapies and with the option of assuming different statistical parameters for independent designs . 
the substudies , however , exist under an overarching master protocol that uses a common infrastructure for screening and treatment assignment to reduce the cost and time associated with enrollment to unrelated and often sequential biomarker - informed studies . 
lung - map ( clinicaltrials.gov identier : nct03851445 ; a master screening protocol previously - treated non - small cell lung cancer ) is an example of a phase ii / iii umbrella study in solid tumors.11 lung - map opened to accrual in 2014 for patients with advanced squamous cell carcinoma ( scc ) of the lung . similar to aml , scc of the lung is a biologically complex disease . 
roughly 60% of patients with lung scc harbor genetic abnormalities that might be targeted with therapy.14 lung - map provided a common infrastructure to test patient samples for multiple biomarkers , which informed therapy assignment within 10 to 14 days . 
patients were assigned to a substudy according to a predened algorithm that used specic genetic abnormalities detected via ngs in patients with a specific tumor type biomarker profiling targeted biomarker 1 targeted biomarker 2 targeted biomarker 3 targeted biomarker n no actionable biomarker regimen a regimen b regimen c regimen n standard of care or non - targeted regimen fig 2 . 
a substudy of new therapy versus soc remained open for patients without an actionable biomarker . lung - map was designed to test new therapies against soc for a particular subgroup using multiple , randomized phase ii trials with pfs as the primary end point . 
within a substudy , if a new therapy met criteria that suggested large the substudy was expanded to improvements in pfs , a phase iii study with pfs and os as co - primary end points . patients who were part of the phase ii interim analysis were included in the phase iii assessment . 
with a well - established screening platform in place , an umbrella trial design can be quite efcient in directing patients into different treatment regimens and accelerating the drug development process . 
the concept of umbrella trials can be applied in any disease setting , but it is most appropriate when there is a strong scientic rationale informing which therapies might work best in biomarker - dened subgroups . 
although not used in beat aml or lung - map , adaptive randomization can be applied within a substudy that has multiple arms to assign patients to a therapy that shows the most favorable outcome , given the data already collected.1 , 15 , 16 bayesian posterior probabilities that compare efcacy of experimental therapy with soc can be used in decision making . umbrella trials are exible and have the ability to open or close new substudies with different targeted therapies or statistical designs if appropriate . basket design basket trials are an efcient way of screening experimental therapeutics across patients with a variety of tumor types and / or histology under one master trial . 
basket trials involve several biomarker proles whereby patients are assigned to treatments based on the molecular alterations their tumors contain , regardless of the histologic type of the tumor.17 , 18 the basic premise for this trial design is that the average response to one or more experimental treatments is expected to vary across these different biomarker proles . like umbrella trials , there may be a common genetic screening platform , especially if the cohorts dened by the study are histology - independent and dened only by the presence of a single molecular aberration . 
figure 3 provides a generic representation of a basket trial design schema . basket trial designs may be appropriate when there is reason to believe that one or more experimental treatments may be effective across a range of primary tumor sites or histologies , and in particular , when patients with specic biomarker proles are expected to respond well to a particular treatment , regardless of their specic disease or histology . 
one such design is the bayesian basket design.20 in this design , a bayesian approach is used to model the response probabilities for the various histologic strata , and two hypotheses are considered : ( 1 ) the response probabilities for a particular targeted agent are equal across the corresponding histologic strata , and ( 2 ) the activity of the drug is independent across these strata . 
a hierarchical bayesian design has recently been proposed for randomized phase ii trials with multiple groups ( or baskets ) , allowing for information sharing across baskets while at the same time having the ability to help with decision making for each individual trial or basket.21 within the hierarchical bayesian design framework , the estimate of the treatment effect for each phase ii trial basket within this master protocol shrunk toward the overall mean treatment effect , which alleviates concerns regarding randomness across the trials or baskets.21 , 22 this approach is most powerful when the treatment effects are heterogeneous across the different baskets and inates the type i error in the inferior treatment effect groups or baskets in the case of heterogeneous treatment effects across baskets . 
it has been noted that the results of a basket trial can be heavily tilted toward positive conclusions , 23 even with specication of weak priors in a bayesian setting . 
the goal of this study , as noted in the publication , was to identify molecular biomarkers and determine their frequency and clinical relevance in patients with advanced nonsmall - cell lung cancer , and thymic malignancies and to evaluate the efcacy of multiple targeted therapies in specic molecular subsets of patients.27 ( p1001 ) a limitation of this trial was the lack of the lung cancer , small - cell adaptive trial feature , because seamless addition of new treatment arms for molecular targets or replacing treatments for a particular molecular subtype was not possible . another issue was the timeliness of the availability of some of the core molecular proling results , which had an impact on enrollment to the trial.27 acs e and tapur case studies . 
the french national cancer institutes acs e initiative ( secured access to innovative therapies ) 28 and ascos tapur trial ( clinicaltrials.gov identier : nct02693535 ; testing the use of food and drug administration [ fda ] approved drugs that target a specic abnormality in a tumor gene in people with advanced stage cancer ) 29 are examples of large - scale trials with basket - type design that evaluate the safety and efcacy prole of approved agents in other indications ( ie , tumor types )  . 
the goals of these trials are to provide patients with advanced diseases ( without promising treatment options ) off - label access to approved agents and to evaluate the safety and efcacy of these agents outside their approved indications . 
the acs e - crizotinib trial ( clinicaltrials.gov identier : nct02034981 ; phase 2 study assessing efcacy and safety of crizotinib in patients harboring an alteration on alk , met or ros1 ) is the rst trial coordinated by the acs e prograit includes patients with various solid and hematologic malignancies . 
basket designs test a single agent in different histologic subtypes , which can be efcient if the goal is to screen for antitumor activity of the agent in different disease settings . 
for example , only two ( nsclc with egfr mutations and nsclc with kras or braf mutations ) of the 15 substudies in the custom trial completed accruing ; accrual was unsuccessful for the other 13 rare histologic subtypes . 
 ou et al experimental therapy in the subgroup of patients positive for the biomarker as well as in either the subgroup of patients negative for the biomarker or in all patients . 
with co - primary objectives , the signicance level ( ) is allocated or split between the two objectives to maintain an acceptable overall type i family - wise error rate using a conservative bonferroni correction or a less conservative correction that considers the correlation between the two tests.31 in the case with co - primary objectives dened for the biomarker - positive subgroup and all patients , the design can be subgroup focused or all - population focused.32 a subgroup - focused design is most appropriate when there is evidence that the experimental therapy will be most effective in patients with the biomarker of interest , but it could also have a broad impact in the general disease population . 
a design with an all - population focus is most appropriate when there is less evidence that the experimental therapy will be most effective in patients with the biomarker of interest but could be effective in the general disease population . 
with an accrual goal of 618 patients egfr - positive by fish , there was 92% power to detect a hazard ratio of 0.75 for pfs in the cetuximab arm relative to the control arm with a type i error rate ( ) of 2% . 
with an accrual goal of 1 , 546 total patients , there was 86% power to detect a hazard ratio of 0.83 for os in the cetuximab arm relative to the control arm with a one - sided of 1.5%. 
because of slow accrual and a lower - than - expected percentage of patients who were egfr positive , the study was amended to 400 egfrpositive patients to detect planned differences in pfs with 80% power . 
 case studies for innovative trial designs multiple hypotheses in a subgroup design allows formal testing of efcacy for a biomarker - dened subgroup of patients and the overall patient population . 
by testing multiple hypotheses , the power for testing a specied effect in the overall population is reduced.32 furthermore , in a subgroup - focused design , as the prevalence of a biomarker decreases , the total sample size increases.32 costs also increase because tissue procurement and biomarker testing is required for all patients to reach the target number of subgroup patients.33 these additional resources can be offset by testing for larger treatment effects in the biomarker - dened subgroup.32 window of opportunity design the primary goal of window of opportunity ( woo ) design , is to unalso known as window or phase 0 design , derstand the antitumor activity of an agent in a disease state that is not disrupted by previous or simultaneous treatments . 
these trials occur between patient diagnosis and initiation of standard treatment and typically have a clinical end point such as tumor response or pfs at a predened early time point , often assessed by radiographic imaging ( figure 5 )  . 
woo designs are distinct from neoadjuvant trial settings , in which an investigational agent is commonly given preoperatively along with cytotoxic chemotherapy or hormonal therapy for a longer period of time than in a woo trial . 
woo trials have recently gained attention , specically in the context of evaluating molecular agents or in early advanced or metastatic disease in which the tumor may not be resistant to selective inhibition of a novel cancer target.38 evaluating molecular end points can be hindered by difculties in procuring tumor tissue before and after drug administration and by heterogeneity in previous exposure to cancer therapies . 
woo trials help to overcome these difculties by enrolling treatment - nave patients , including a translational research component , and occurring in a short time frame before the initiation of the standard treatment of the disease . 
the ultimate hope of woo trials is that they can expedite the drug development process by improving understanding of an agents biologic effect early in its development , validating markers that may predict subsets of patients who will benet , and targeting select short courses of experimental treatment diagnosis of disease standard of care ( eg , surgery ) standard treatment option fig 5 . 
it is a design best suited for trials in which the treatment cycles are short , and a short - term outcome ( eg , biomarker change ) is the end point of interest . 
in addition , although it is not yet documented , there is the theoretical possibility that the investigational agent may in fact induce resistance to subsequent therapies . logistically , woo trials require careful coordination among members of a multidisciplinary study team because diagnosis , workup , and study treatment must all be arranged in a short time frame . 
furthermore , tumor heterogeneity can be an issue , and thus it is essential to have the infrastructure capable of performing a centralized and high - quality review of all biomarkers.40 woo trials were initially used to inform a go / no - go decision in development of anticancer agents , to expose a small number of patients to a limited duration and dose of a drug and subsequently proceed to phase i / ii trials on the basis of the results.41 ( p2574 ) woo trials may not be advantageous in settings in which an agent has already been well - studied in other disease setfor which the toxicity prole is already welltings , understood , or even for which little safety data are available regarding the risk of delaying surgery.40 despite these concerns and considerations , woo trials have proved benecial in some settings . 
 ou et al active in untreated patients.42 , 43 woo trials should therefore be considered as a promising alternative trial design . discussion with the ability to simultaneously evaluate the effects of therapies on multiple biomarkers and diseases , umbrella and basket trial designs can help accelerate the discovery of targeted therapy . 
because each substudy of the umbrella and basket trials is essentially an enrichment trial design , we would expect a larger effect size , given the available prior knowledge of certain genotype proles and their sensitivity to therapy . 
woo trials allow investigators to understand the antitumor activity of an agent in the de novo disease setting . trial designs in the precision medicine era require a platform to carry out the biomarker proling . 
given the advances in liquid biopsies , cell - free dna from plasma may provide a minimally invasive alternative to standard tumor biopsies.44 even though we have more options for proling patients , the proling is not without challenge . 
at the same time , a screening cut point will need to be established and validated to ensure the cut point value ( ie , the high and low levels of the biomarker value to predict the response to treatment ) is appropriate.45 in an early work , mandrekar et al46 outlined the criteria for choice of phase ii designs for initial validation of a predictive marker in a review article that considered assay performance , turnaround time , preliminary evidence , and marker prevalence . with the advances in targeted therapy , we now have many therapeutic options for specic targeted biomarkers ; however , mutations that have high prevalence in a certain disease may not be common in another ( for example , human epidermal growth factor receptor 2 overexpression has been reported in approximately 15%47 of patients with breast cancer but only approximately 2% of patients with colorectal cancer ) .48 designing a trial with a biomarker target with extremely low prevalence is a challenge because it is difcult to obtain a sufcient number of patients to properly power the study . 
a statistical trial design that uses small sample sizes is needed to tackle this issue , as well as potentially international partnerships . in this article , we have focused our discussion on trial designs that are better suited for phase ii and iii studies . 
seamless phase i / ii designs , which blur the distinction between dose selection and efcacy evaluation , are one such design . hobbs et al49 provided an overview of the use of seamless designs in rst - in - human studies based on abstracts submitted to asco annual meetings from 2010 to 2017 and provided guidance on the design and conduct of such trials . 
to validate biomarker associations identied from such studies , sufcient statistical rigor is still required , such as clear denition of the primary end point , a prespecied interim and nal analysis plan , and well - dened safety monitoring rules . with immunotherapy gaining traction in oncology , it uncertain whether the current designs can adequately address the needs for these agents . 
if the primary objective is to show efcacy in a biomarker - dened , tumor - specic patient population , then both enrichment design and umbrella design ( ie , as one of the substudies ) are applicable . 
as mentioned in the introduction , pembrolizumab received the rst tissue - agnostic fda approval , and there may be several factors that could have contributed to successfully ling for approval of pembrolizumab.50 first , the tissue collection in the initial randomized pembrolizumab trials allowed investigators to retrospectively test the tissue - agnostic hypothesis . 
second , immunotherapies are designed with a strong foundation of preclinical data . third , multiple prospective clinical trials have veried the hypotheses generated by the retrospective data that contributed to its approval . 
in the case of pembrolizumab , approval was based on the data from ve different trials in which patients were retrospectively identied from two studies and prospectively enrolled in three studies.7 because this design is the rst of its kind , it is unclear which design discussed in this article will be best suited for future agents targeting tissue - agnostic indications . 
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schmitz s , caballero c , locati ld : perspectives on window of opportunity trials in head and neck cancer : lessons from the eortc 90111 - 24111 - noci - hncg and neck ( scchn )  . 
clark pi , slevin ml , joel sp , et al : a randomized trial of two etoposide schedules in small - cell lung cancer : the inuence of pharmacokinetics on efcacy and 44 . 
 successful targeting of an atg7 - raf1 gene fusion in anaplastic pleomorphic xanthoastrocytoma with leptomeningeal dissemination mehdi touat , md1 ; nadia younan , md1 ; philipp euskirchen , md1 , 2 , 3 , 4 , 5 ; maxime fontanilles , md1 ; karima mokhtari , md1 ; caroline dehais , md1 ; patrick tilleul , pharmd6 ; amithys rahimian - aghda , msc1 ; adam resnick , phd7 ; anne - paule gimenez - roqueplo , md , phd8 , 9 , 10 ; h el `ene blons , pharmd , phd8 , 9 , 11 ; kh e hoang - xuan , md , phd1 ; jean - yves delattre , md , phd1 ; ahmed idbaih , md , phd1 ; pierre laurent - puig , md , phd8 , 9 , 11 ; and marc sanson , md , phd1 introduction pleomorphic xanthoastrocytoma ( pxa ) is an uncommon primary brain tumor occurring primarily in children and young adults.1 although pxa is typically considered a relatively indolent entity , some tumors are accompanied by anaplastic features associated with high rates of recurrence after local treatment and unfavorable outcome.2 accordingly , anaplastic pxa ( who grade 3 ) has been added to the 2016 who classication of cns tumors as a distinct entity.1 there is no standard management for patients with anaplastic pxa that recurs after surgery ; neither chemotherapy nor radiotherapy have demonstrated clinical benet in this disease.2 , 3 the identication of activating in recent years , brafv600e mutations in 50% of patients with pxa has rened our understanding of these disorders as malignancies driven by aberrant activation of the mitogenactivated protein kinase ( mapk ) signaling pathway.1 , 3 - 5 this was further supported by the observation of both preclinical and clinical activity of vemurafenib , a selective brafv600e inhibitor , in brafv600e - mutant gliomas.6 , 7 however , patients with braf wild - type pxa are not candidates for treatment with selective brafv600e inhibitors , and little is known about the spectrum of molecular alterations occurring in this population . 
recent studies showed that a subset of braf wild - type pxa might harbor rare braf or raf1 fusions , 8 , 9 which have been associated with exquisite sensitivity to mapk signaling inhibition in preclinical models.10 it remains unknown whether patients who have glioma with braf or raf1 gene fusions might respond to therapies targeting mapk signaling . 
histopathologic analysis showed a tumor composed of pleomorphic glial cells with the presence of mitoses , necrosis , and microvascular proliferation , consistent with who grade 3 anaplastic pxa ( fig 2 )  . 
although rhabdoid morphology was observed in some sectors , both epithelial membrane antigen and p53 immunostainings were negative , and we did not observe loss of ini1 , features that were previously associated with rhabdoid glioblastomas and cns atypical teratoid / rhabdoid tumors , respectively . 
furthermore , targeted sequencing of the tumor did not nd mutations in braf ( exons 11 and 15 ) , idh1 , idh2 , h3f3a , hist1h3b , or smarcb1 . 
array comparative genomic hybridization revealed a 9p deletion involving cdkn2a and cdkn2b , which have been previously associated with poor outcome in brafv600e - mutant gliomas.3 , 11 , 12 given the unfavorable prognosis , she was rst treated with adjuvant chemoradiotherapy ( 60 gy in 30 fractions over 6 weeks along with once - per - day temozolomide 75 mg / m2 ) followed by temozolomide ( 200 mg / m2 ) for 6 cycles until november 2015 ( fig 1a )  . in february 2016 , routine surveillance mri scans showed increased contrast enhancement in the right occipital lobe . 
 touat et al context key objective to report the successful treatment of a patient with refractory braf - wild - type anaplastic pxas harboring an in - frame atg7raf1 fusion with the mek inhibitor cobimetinib . knowledge generated we report for the rst time , to our knowledge , that raf1 gene fusions are actionable molecular events in high - grade gliomas . this report highlights the oncogenic role of mapk - activating alterations including raf1 rearrangements and brafv600e mutations in a subset of pediatric and adult gliomas . relevance cobimetinib can achieve therapeutic exposure within the cns , including the cerebrospinal uid in patients with raf1translocated high - grade gliomas . showed leptomeningeal enhancement in the posterior cerebral fossa ( fig 1b )  . 
neoplastic meningitis was conrmed by lumbar puncture showing 42 white blood cells per l ( 84% lymphocytes ) , hyperproteinorachia ( 0.55 g / l ) , and the presence of tumor cells in the cerebrospinal uid ( csf ; fig 1b )  . 
intravenous thiotepa ( 45 mg / m2 ) was begun , the treatment was discontinued after one infusion because of grade 4 thrombopenia and febrile neutropenia with infectious pneumonia , which required intravenous antibiotics . the patient was enrolled in the precision medicine program exorare for tumor molecular characterization using rna sequencing and matched tumor or normal whole - exome sequencing . 
reverse transcriptase - polymerase chain reaction and sanger sequencing conrmed the expression of an in - frame atg7raf1 fusion transcript in the recurrent tumor ( second surgery , 2016 ; fig 3b )  . 
interestingly , no additional molecular alteration was found by whole - exome among 475 genes previously associated with cancer , which suggested that the atg7 - raf1 fusion was the main oncogenic driver . moreover , previous reports showed that fusions involving exon 8 of raf1 are recurrent events in cancer including pxa8 , 9 , 13 and can result in constitutive activation of the tyrosine kinase domain and downstream mapk signaling through the loss of the n - terminal autoinhibitory domain of raf1.14 treatment with sorafenib ( 200 mg twice per day ) was then started in october 2016 through off - label use after informed consent . 
unfortunately , her clinical condition rapidly deteriorated with partial seizures , confusion , cerebellar ataxia , diplopia , hypoacousia , headaches , and diffuse pain in the lower limbs , for which treatment with intravenous morphine , steroids , and midazolam was begun . on the basis of preclinical data suggesting that mek inhibition in astrocytomas harboring raf1 fusions has superior efcacy , 10 sorafenib was discontinued and treatment with off - label cobimetinib ( 60 mg per day , 3 weeks on and 1 week off ) was started in november 2016 , after family members provided informed consent ( fig 1a )  . 
the patient dramatically improved after a few days of treatment , with complete regression of the confusion and headaches and partial regression of the cerebellar ataxia and pain in the lower limbs . 
subsequent lumbar puncture showed complete cytologic response in the csf ( fig 1b ) with regression of both pleocytosis ( 1 white blood cell per l ) and hyperproteinorachia ( 0.15 g / l ; fig 1b )  . 
 ( b ) top : serial contrast - enhanced t1 - weighted images of brain magnetic resonance imaging ( mri ) and cerebrospinal uid ( csf ; may - gr unwald - giemsa stain ) cytology at ( left ) initial presentation , ( middle ) pretreatment , and ( right ) during treatment with cobimetinib showing the right occipital lesion , the leptomeningeal enhancement on the brain mri ( white arrows ) , and the presence of neoplastic cells in the csf ( black arrowheads ) before treatment with cobimetinib was started . 
the observation of clinical activity with both braf and mek inhibitors suggest that brafand raf1 - driven gliomas , even in patients who have been heavily pretreated , display a high level of mapk pathway dependency and possibly less molecular heterogeneity than the majority of gliomas driven by other alterations such as egfr variants.20 - 22 despite previous reports indicating activity of sorafenib in treating patients with cancer who harbor mutations of braf or araf ( both paralogs of raf1 ) , 23 , 24 our patient did not respond to treatment with sorafenib . 
 ( a ) hematoxylin - eosin and ( b ) reticulin colorations showing a pleomorphic tumor proliferation , with the presence of xanthomatous cells with nuclear atypia , reticulin bers , microvascular proliferation , and necrosis . 
 ( c - f ) immunohistochemical stains showing tumor cell immunoreactivity for ( c ) glial brillary acidic protein , ( d ) cd34 , and ( e ) oligodendrocyte transcription factor 2 . 
 ( f ) high mitotic activity was noted on mib - 1 staining . alterations is currently ongoing ( nct02639546 ; safety and pharmacokinetics of cobimetinib in pediatric and young adult participants with previously treated solid tumors [ imatrixcobi ] ) , although adult patients are not yet eligible for this study . 
furthermore , novel mek inhibitors optimized for achieving higher brain exposure might have a role in these diseases.28 in conclusion , our report provides evidence for the oncoincluding raf1 reargenic role of mapk alterations , in pediatric and adult brain tumors and rangements , suggests that raf1 fusions may represent potential therapeutic targets in a subset of patients with braf wild - type high - grade gliomas . 
a recent report of a patient with melanoma with an ano10raf1 fusion reported long - lasting clinical improvement after treatment with the mek inhibitor trametinib , 29 suggesting that patients with raf1 fusiondriven tumors might respond to mek inhibition regardless of histology . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . mehdi touat consulting or advisory role : agios pharmaceutical , taiho oncology travel , accommodations , expenses : merck sharp & dohme maxime fontanilles travel , accommodations , expenses : roche patrick tilleul honoraria : takeda , astellas pharma , roche , biogen , evidera , baxter , gr unenthal group , chiesi , bristol - myers squibb , msd , sandoz - novartis , pzer , astrazeneca h el `ene blons honoraria : astrazeneca , bristol - myers squibb , msd oncology kh e hoang - xhuan travel , accommodations , expenses : abbvie ahmed idbaih travel , accommodations , expenses : carthera pierre laurent - puig honoraria : amgen , astrazeneca , boehringer ingelheim , merck serono , merck , roche , sano consulting or advisory role : merck , bristol - myers squibb , boehringer ingelheim patents , royalties , other intellectual property : inventor of mir31 - 3p ( license to integragen ) travel , accommodations , expenses : roche , merck marc sanson consulting or advisory role : abbvie , genenta travel , accommodations , expenses : abbvie no other potential conicts of interest were reported . acknowledgment the authors thank ines detrait and delphine le corre for tissue preparation and acid nucleic extractions , and dr yvan bieche and integragen for the genomic analyses performed in this patient . references louis dn , ohgaki h , wiestler od , et al : world health organization histological classication of tumours of the central nervous system , 4th edition revised . lyon , france , international agency for research on cancer , 2016 ida cm , rodriguez fj , burger pc , et al : pleomorphic xanthoastrocytoma : natural history and long - term follow - up . 
brain pathol 25 : 575 - 586 , 2015 lassaletta a , zapotocky m , mistry m , et al : therapeutic and prognostic implications of braf v600e in pediatric low - grade gliomas . 
j clin oncol 35 : 2934 - 2941 , 2017 dias - santagata d , lam q , vernovsky k , et al : braf v600e mutations are common in pleomorphic xanthoastrocytoma : diagnostic and therapeutic implications . plos one 6 : e17948 , 2011 schindler g , capper d , meyer j , et al : analysis of braf v600e mutation in 1 , 320 nervous system tumors reveals high mutation frequencies in pleomorphic xanthoastrocytoma , ganglioglioma and extra - cerebellar pilocytic astrocytoma . 
clin cancer res 17 : 7595 - 7604 , 2011 kaley t , touat m , subbiah v , et al : braf inhibition in brafv600 - mutant gliomas : results from the ve - basket study . 
brain pathol 29 : 85 - 96 , 2018 jain p , fierst tm , han hj , et al : craf gene fusions in pediatric low - grade gliomas dene a distinct drug response based on dimerization proles . 
huillard e , hashizume r , phillips jj , et al : cooperative interactions of brafv600e kinase and cdkn2a locus deciency in pediatric malignant astrocytoma as a basis for rational therapy . 
 cobimetinib in anaplastic pleomorphic xanthoastrocytoma with raf1 fusion jones dt , hutter b , j ager n , et al : recurrent somatic alterations of fgfr1 and ntrk2 in pilocytic astrocytoma . 
nat genet 45 : 927 - 932 , 2013 johnson a , severson e , gay l , et al : comprehensive genomic proling of 282 pediatric lowand high - grade gliomas reveals genomic drivers , tumor mutational burden , and hypermutation signatures . 
reinhardt a , stichel d , schrimpf d , et al : anaplastic astrocytoma with piloid features , a novel molecular class of idh wildtype glioma with recurrent mapk pathway , cdkn2a / b and atrx alterations . 
szerlip nj , pedraza a , chakravarty d , et al : intratumoral heterogeneity of receptor tyrosine kinases egfr and pdgfra amplication in glioblastoma denes subpopulations with distinct growth factor response . 
cancer discov 4 : 956 - 971 , 2014 imielinski m , greulich h , kaplan b , et al : oncogenic and sorafenib - sensitive araf mutations in lung adenocarcinoma . 
casadei gardini a , chiadini e , faloppi l , et al : efcacy of sorafenib in braf - mutated non - small - cell lung cancer ( nsclc ) and no response in synchronous braf wild type - hepatocellular carcinoma : a case report . 
choo ef , ly j , chan j , et al : role of p - glycoprotein on the brain penetration and brain pharmacodynamic activity of the mek inhibitor cobimetinib . 
gampa g , kim m , cook - rostie n , et al : brain distribution of a novel mek inhibitor e6201 : implications in the treatment of melanoma brain metastases . 
malignant cells have a high proliferative fraction and typically express b - cell lymphoma 2 ( bcl2 ) , interferon regulatory factor 4 ( irf4 ) , and b - cell lymphoma 6 ( bcl6 ) on immunohistochemistry . gene expression proling is associated with constitutive nuclear factor ( nf ) - b pathway activation and up - regulation of apoptosis - inhibiting genes , similar to ndings in abc dlbcl . 
mutations of myd88 , resulting in constitutive nf - b activation , are reported in pbdlbcl - lt in up to 69% of cases6 , 7 and are associated with a worse clinical outcome.7 apoptosis gene expression proling in pcdlbcl - lt has shown not only high expression levels of antiapoptotic genes but also concomitant downstream inhibition of the intrinsic apoptosis pathway , as reported in chemotherapy - refractory nodal abc dlbcl.8 , 9 treatment of relapsed / refractory pcdlbcl - lt remains a signicant challenge , with many patients succumbing to uncontrolled disease.3 current therapeutic options , including access to clinical trials , are limited because of both the rarity of disease and the often frail , comorbid patient population . 
small case series of patients with myd88 - mutated pcdlbcl - lt have demonstrated responses to inhibition of b cell receptor ( bcr ) signaling via bruton 's tyrosine kinase ( btk ) inhibition , although responses are of short duration ( 4 to 40 weeks ) and associated with rapid emergence of resistance - conferring mutations.10 , 11 the efcacy of the specic bcl2 inhibitor venetoclax in pcdlbcl - lt remains unexplored . 
this study was approved by the university hospitals of leicester nhs trust ( uk ; 06 / q2501 / 122 )  . research and development written informed consent was obtained for publication purposes . expression of cd20 , cd79a , paired box 5 ( pax5 ) , bcl2 , bcl6 , irf4 , and cd10 , with a ki67 fraction of 90% ( figs 1a - 1d )  . 
 ( a ) hematoxylin and eosin staining , ( b ) interferon regulatory factor 4 ( irf4 ) , ( c ) b - cell lymphoma 2 ( bcl2 ) , and ( d ) ki67 expression . 
in 2010 , he relapsed again with left leg cutaneous involvement only , adjacent to the previously treated sites , and received additional treatment with four cycles of r - chop and radiotherapy ( 40 gy in 15 fractions ) , again attaining clinical response . 
two additional relapses in the left leg with progressively shorter disease - free intervals were treated with radiotherapy alone in 2011 and 2012 ( 4 gy , single fraction )  . 
subsequently , in 2016 , an additional relapse , treated with rituximab , gemcitabine , cyclophosphamide , vincristine , and prednisolone , was refractory to chemotherapy . because of high expression of bcl2 and the development of chemorefractory disease , in january 2017 we obtained venetoclax through the uk abbvie compassionate access scheme . 
repeat staging by ct and 18f - labeled uorodeoxyglucosepositron emission tomography / ct scans conrmed that disease remained localized to the left lower leg , as shown in figure 1e . 
the dose of venetoclax was escalated to 1 , 200 mg because of published data in dlbcl and follicular lymphoma conrming safety and tolerability of this dose.12 however , 1 , 200 mg was not tolerated because of persistent grade 2 diarrhea and grade 2 fatigue , and thus 800 mg was adopted as a maintenance dose . 
biopsy after 2 weeks of treatment showed a complete histologic and immunohistochemical response , although ighv polymerase chain reaction showed persistence of clonal b cells ( data not shown )  . 
treatment with venetoclax was stopped 1 month after demonstration of metabolic remission . however , within 4 weeks of stopping venetoclax , disease recurred , once again conned to the left lower leg , but at different anatomic sites . 
an additional biopsy was performed , which conrmed relapsed disease and showed persistent high - level bcl2 expression ( data not shown )  . venetoclax was recommenced at a dose of 400 / 800 mg on alternate days , with only mild gastrointestinal ( gi ) toxicity ( grade 1 common terminology criteria for adverse events )  . eighteen months later , with continued daily venetoclax , his disease remains in complete remission . whole - exome dna sequencing was performed only on the last relapse sample because of a lack of suitable material from prior biopsies . 
call thresholds were a minimum of 10 variant reads , depth 25 reads , variant allele frequency 10% , scale - invariant feature transform score less than 0.35 , polyphen greater than 0.7. 
potential genetic drivers of this malignancy included previously described arid1a and notch2 mutations ( table 1 ) , as well as biallelic deletion of rb1 and cdkn2a and monoallelic loss of tp53 ( fig 2 )  . 
 ( a , b ) somatic copy number analysis of the tumor biopsy was carried out using varscan and sequenza programs against patient germline dna . frequency of copy number ( log2 ratio ) obtained by pairwise comparison of read depths along the sequenced exome . 
dyer honoraria : roche pharma ag , abbvie , sandoz speakers ' bureau : roche research funding : roche ( inst ) , gilead sciences ( inst ) , astex pharmaceuticals ( inst ) , bioinvent ( inst ) travel , accommodations , expenses : abbvie no other potential conicts of interest were reported . references sokol l , naghashpour m , glass lf : primary cutaneous b - cell lymphomas : recent advances in diagnosis and management . 
blood 105 : 3768 - 3785 , 2005 grange f , beylot - barry m , courville p , et al : primary cutaneous diffuse large b - cell lymphoma , leg type : clinicopathologic features and prognostic analysis in 60 cases . 
arch dermatol 143 : 1144 - 1150 , 2007 vermeer mh , geelen fa , van haselen cw , et al : primary cutaneous large b - cell lymphomas of the legs . 
arch dermatol 132 : 1304 - 1308 , 1996 senff nj , noordijk em , kim yh , et al : european organization for research and treatment of cancer and international society for cutaneous lymphoma consensus recommendations for the management of cutaneous b - cell lymphomas . 
 successful treatment with single - agent venetoclax pham - ledard a , cappellen d , martinez f , et al : myd88 somatic mutation is a genetic feature of primary cutaneous diffuse large b - cell lymphoma , leg type . j invest dermatol 132 : 2118 - 2120 , 2012 pham - ledard a , beylot - barry m , barbe c , et al : high frequency and clinical prognostic value of myd88 l265p mutation in primary cutaneous diffuse large b - cell lymphoma , leg - type . 
jama dermatol 150 : 1173 - 1179 , 2014 cillessen sa , hess cj , hooijberg e , et al : inhibition of the intrinsic apoptosis pathway downstream of caspase - 9 activation causes chemotherapy resistance in diffuse large b - cell lymphoma . 
clin cancer res 13 : 7012 - 7021 , 2007 van galen jc , hoefnagel jj , vermeer mh , et al : proling of apoptosis genes identies distinct types of primary cutaneous large b cell lymphoma . 
fox lc , yannakou ck , ryland g , et al : molecular mechanisms of disease progression in primary cutaneous diffuse large b - cell lymphoma , leg type during 11 . 
davids ms , roberts aw , seymour jf , et al : phase i rst - in - human study of venetoclax in patients with relapsed or refractory non - hodgkin lymphoma . 
li l , pongtornpipat p , tiutan t , et al : synergistic induction of apoptosis in high - risk dlbcl by bcl2 inhibition with abt - 199 combined with pharmacologic loss 14 . 
paulli m , lucioni m , maf a , et al : primary cutaneous diffuse large b - cell lymphoma ( pcdlbcl ) , leg - type and other : an update on morphology and treatment . 
little is known about the experiences of individuals tested for cdh1 variants in the multigene panel testing era . methods participants recruited from the prospective registry of multiplex testing completed a cross - sectional self - report survey regarding cdh1 genetic testing experiences , medical management , and psychosocial adaptation . results discordance existed in interpretations of cdh1 results ; 13.3% of cases had disagreements in variant classications among commercial laboratories , and 21.4% had disagreements between participant self - report and clinvar classication . 
2019 by american society of clinical oncology introduction hereditary diffuse gastric cancer syndrome ( hdgc ) , attributed to germline cdh1 pathogenic variants ( pv ) , is associated with increased risk for diffuse gastric cancer ( dgc ) and invasive lobular breast cancer ( lbc )  . 
germline cdh1 pv are present in approximately 40% of hdgc families , 1 and 1% to 3% individuals with gastric cancer have a cdh1 pv.2 reported cumulative lifetime dgc risk ranges from 50% to 80%.1 , 3 - 5 prophylactic gastrectomy is a standard management recommendation for individuals with cdh1 pv , given the inability of endoscopic surveillance to reliably identify dgc.5 because of cumulative lifetime lbc risk estimates ranging from 39% to 52% , recommendations for those with cdh1 pv include breast cancer screening via annual mammography , with consideration of breast magnetic resonance imaging beginning at age 30 years ; risk - reducing mastectomy decisions may occur dependent on family history.3 , 6 before the advent of multigene panel testing ( mgpt ) for hereditary cancer susceptibility , candidates for cdh1 genetic testing were evaluated on criteria dened by the international gastric cancer linkage including a conrmed case of dgc consortium , younger than age 40 years , at least two cases of dgc at any age , or the presence of both dgc and lbc younger than age 50 years.5 , 7 thus , individuals undergoing cdh1 gene analysis had a signicant perfamily history of hdgc - associated sonal and / or cancers . 
 hamilton et al context key objective germline cdh1 variants that are associated with hereditary diffuse gastric cancer syndrome ( hdgc ) are rare , but growth in multigene panel testing is leading to patients with limited personal exposure to hdgc being confronted with such results . 
we addressed the question of what are the genetic testing experiences , medical management , and psychosocial adaptation of patients with cdh1 variants identied through multigene panel testing ? knowledge generated discordant interpretations of cdh1 results were observed across testing laboratories , as well as among participants reporting of their results . 
participants with pathogenic cdh1 variants were more likely than those with variants of uncertain signicance to receive recommendations for prophylactic gastrectomy , yet both groups perceived similar , moderate levels of risk for gastric cancer . relevance findings highlight the unique informational and psychosocial needs of patients living with cdh1 variants , suggesting that they may benet from support tailored to the challenges associated with their particular risk status . genetic testing services are increasingly offered outside the cancer genetics specialty , such as via primary care providers , surgeons , and direct - to - consumer companies.10 - 12 given the variability by which preand post - test genetic counseling and testing for cdh1 are currently provided , we sought to characterize the genetic testing experiences , medical management , and psychosocial adaptation of individuals living with cdh1 variants . methods participants participants were recruited from the prospective registry of multiplex testing ( prompt ) , an online genetic registry founded by investigators at memorial sloan kettering , the university of pennsylvania , dana - farber cancer institute , and mayo clinic for individuals age 18 years or older tested for cancer susceptibility genes as part of any commercial mgpt . 
on self - selected enrollment in prompt , individuals consent to participate in the registry ; complete a baseline questionnaire of personal / family history , genetic testing results , and demographic information ; and share their testing report with prompt staff . 
a centralized institutional review board ( chesapeake irb ) approved this research . procedure study data were collected using redcap software13 through an online cross - sectional survey e - mailed to prompt participants with a self - reported cdh1 variant . invitations including a link to the survey ( with two reminders for nonresponders ) were e - mailed to 135 eligible individuals from september to december , 2017 . 
participants reported their understanding of their cdh1 result ( response options : positive genetic test result , likely positive genetic test result , variant of uncertain signicance , negative genetic test result , my test results are not clear to me ) and the year when they learned their result . 
we assessed personal ( yes , no ) and family history ( yes , no , uncertain ) of breast and gastric cancer , and details ( eg , surgery date ) regarding personal cancer treatment . 
recommendation by a health care provider for risk - reducing mastectomy , meeting with a gastroenterologist , and prophylactic gastrectomy , as well as adoption of breast magnetic resonance imaging , risk - reducing mastectomy , meeting with a gastroenterologist , upper endoscopy , and prophylactic gastrectomy , were assessed ( yes , no , unsure )  . 
genetic knowledge was assessed with 21 items regarding basic genetic concepts and aspects of mgpt selected or modied from the university of north carolina genomic knowledge scale.15 cdh1 knowledge was assessed with six investigator - designed items regarding cancer risks and inheritance of cdh1 variants . item response options were true , false , and don ' t know . 
items adapted from the national cancer institute health information national trends survey assessed absolute perceived cancer risks ( how likely are you to get [ breast / gastric ] cancer in your lifetime ? ; 1 = very unlikely to 5 = very likely ) and affective perceived cancer risks ( i feel like i could easily get [ breast / gastric ] cancer in my lifetime ; 1 = i feel very strongly that this will not happen to 5 = i feel very strongly that this will happen ) .16 decision - making experiences . 
ten items selected or modied from quality of a published measure21 assessed positive ( example : my cdh1 test result allows me to take control of my health ; = 0.75 ) and negative ( example : because of my cdh1 test result , i feel awed and stigmatized ; = 0.79 ) effects of cdh1 genetic testing on quality of life . 
three investigator - designed items assessed whether patients shared their cdh1 results with family , why this information was not shared with family , and family interest in genetic testing . statistical analysis seventy - one individuals responded to the survey ( 53% response rate ; appendix figure a1 ) ; however , three respondents did not have a cdh1 result and were excluded from all analyses . 
conicting interpretation was dened as either disagreement among one or more commercial laboratories in variant classications ( evaluable participants : n = 60 ) , or disagreement between participant self - report and clinvar classication ( evaluable participants : n = 56 )  . 
 medical and psychosocial experiences after cdh1 variant detection second , to determine how individuals understanding of their cdh1 results were associated with their medical and psychosocial experiences , we evaluated the survey data of the 60 respondents who self - reported either a pv ( ie , positive genetic test result or likely positive genetic test result ) or variant of uncertain signicance ( vus )  . 
data were examined for missing values ; patients missing responses to more than 20% of variables were excluded ( n = 3 ) , and average values on the basis of existing items were computed for scales missing less than or equal to 20% of items . 
of concern , three of these cases ( 25% of cases with participant / clinvar disagreement ; 5.4% of evaluable sample ) involved participant self - report of pv ( ie , positive genetic test result or likely positive genetic test result ) but clinvar and test report classication of vus . 
dashes indicate that a p value was not computed because of inadequate cell size . ||individuals with a complete stomach at the time of survey completion only . abbreviations : pv , pathogenic variant ; vus , variant of uncertain signicance . * responses of uncertain or unsure were combined with responses of no for analyses . females with at least one healthy breast at the time of learning their cdh1 results only . females with at least one healthy breast at the time of survey completion only . individuals with a complete stomach at the time of learning their cdh1 results only . least one healthy breast at the time of learning their cdh1 results , a minority ( 25.0% ) reported that a health recommended risk - reducing care provider had ever mastectomy ; no differences in recommendation receipt were observed based on cdh1 result . 
experiences with genetic testing among participants with cdh1 variants experience pv ( n = 16 ) vus ( n = 41 ) total ( n = 57 ) ever offered cancer genetic counseling yes , pros and cons discussed but i didn ' t 0 ( 0 ) unsure ever received cancer genetic counseling was given options to have different numbers of genes tested for hereditary cancer don ' t know was sufciently informed about pros and cons of having different numbers of genes tested for hereditary cancer yes , given sufcient information yes , pros and cons discussed but more information would have been helpful understand no , pros and cons not discussed not sure i felt sufciently informed would have preferred more time to decide about how many genes to have tested don ' t know was informed about possibility of identifying vus when deciding whether to undergo testing yes , i was informed and i understood yes , i was informed but it was not clear what that meant informed after i received results no , i was never informed not sure i was informed would have preferred more time to discuss options with family , friends , or health care providers before having genetic testing don ' t know no . 
approximately 39% of the sample recalled being given options to have different numbers of genes tested for hereditary cancer ; of these they received sufcient participants , most ( 68.2% ) felt information about the pros and cons of having different numbers of genes tested . 
specically , those with pv and vus both reported mean scores for the measures of perceived gastric cancer risks consistent with scale midpoints ( ie , absolute perceived gastric cancer risk : neither unlikely nor likely ; affective perceived gastric cancer risk : i feel i am just as likely to get cancer as i am to not get cancer )  . 
regarding emotional outcomes , participants with pv reported greater distress ( p .001 ) and were more likely to be worried about future discrimination on the basis of their cdh1 result ( p = .05 ) than those with vus . participants reported low decisional regret ( mean , 13.13 , 0 to 100 scale ) regarding cdh1 testing , irrespective of their result . 
consistent with a separate analysis of laboratory interpretations of variants identied by hereditary cancer mgpt , 27 discrepancies were not 13.3% of cases , laboratories differed in their interpretation of cdh1 variant pathogenicity . 
dashes indicate that a p value was not computed because of inadequate cell size . abbreviations : pv , pathogenic variant ; vus , variant of uncertain signicance . * missing response ( n = 1 )  . asked only among those who had not shared cdh1 results with all family ( n = 19 ) and participants could select more than one response . free - text responses included i ' m adopted , so my results don ' t apply to them , and most family members would not nd meaningful . asked only among those who shared with ( some ) family , and responses of yes . 
future research should examine how and why such misunderstandings arise and their implications for patients and families . time , differential provider the survey data indicated that , consistent with clinical guidelines , 5 only participants with a pv reported ever receiving a recommendation to undergo prophylactic gastrectomy . 
however , fewer than half of these individuals recalled receiving this recommendation , and receipt of this recommendation was not associated with clinical factors relevant to the timing of this surgical intervention , such as family gastric cancer history or patient age . 
it is unclear why certain individuals with cdh1 pv have been advised to pursue prophylactic gastrectomy and others have not . although there is speculation that the lifetime risk of gastric cancer may be lower in individuals with cdh1 pv and no family history of gastric cancer ( compared with those with a family history ) , at the current time a discussion of gastrectomy remains standard of care.26 , 28 their despite growing access to genetic testing through nongenetics health care providers , most participants were offered and received genetic counseling . 
 medical and psychosocial experiences after cdh1 variant detection patients understand the risks and benets and feel prepared to make an informed decision about mgpt . results also demonstrate that individuals with cdh1 pv and vus each have unique informational and emotional needs . 
those with vus were also less satised with their health care providers knowledge about the result ; however , it is not possible to discern whether this reects a lack of provider familiarity or existing limitations in scientic knowledge about risks and appropriate management of these variants . 
furthermore , although those with pv accurately perceived themselves to be at greater risk for breast cancer than did those with vus , these individuals had similar perceived risks for gastric cancer , which on average reected scale midpoints . 
risk perceptions are important for promoting cancer prevention behaviors , 30 , 31 including management of hdgc8 ; research is needed to understand why some with cdh1 pv seem to hold inaccurate risk perceptions . 
participants with pv did experience greater distress ; however , levels of distress were modest in this sample , consistent with a recent analysis of patient experiences with mgpt for hereditary breast and ovarian cancer.14 this study has several limitations . 
consequently , these ndings may not be generalizable to the individuals with cdh1 variants . broader population of furthermore , analyses used self - reported data regarding individuals medical and genetic testing experiences . 
nonetheless , this research extends beyond past work , which has largely focused on cdh1 mutation carriers prophylactic surgical decision making and adjustment , 8 , 32 - 34 to provide novel insight into the experiences of individuals with cdh1 variants in the era of mgpt . in conclusion , although many with cdh1 pv or vus are satised with their decision to pursue genetic testing , these individuals have unique informational and psychosocial needs . 
low levels of reported recommendations for prophylactic gastrectomy and perceived gastric cancer risks among those with cdh1 pv are particularly worrisome , suggesting a need for strategies ( eg , innovative applications of risk communication principles , 35 - 37 enhanced provider genetics education38 ) to more effectively engage and educate patients and providers about relevant medical management and cancer risks . 
long employment : depuy synthes companies ( i ) stock and other ownership interests : depuy synthes companies ( i ) travel , accommodations , expenses : depuy synthes companies ( i ) fergus j . 
couch consulting or advisory role : astrazeneca research funding : grail travel , accommodations , expenses : grail , qiagen , ambry genetics research funding : novartis ( i ) , ambry genetics , susan g . 
komen for the cure ( i ) , aacr , diana helis henry medical foundation ( i ) , james p . wilmot foundation ( i ) , adrienne helis malvin medical research foundation ( i ) , global biological standards institute ( i ) , breast cancer research foundation mark e . 
robson honoraria : astrazeneca , pzer consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , pzer ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca susan m . 
jama oncol 1 : 23 - 32 , 2015 corso g , marrelli d , pascale v , et al : frequency of cdh1 germline mutations in gastric carcinoma coming from highand low - risk areas : metanalysis and systematic review of the literature . 
bmc cancer 12 : 8 , 2012 pharoah pd , guilford p , caldas c : incidence of gastric cancer and breast cancer in cdh1 ( e - cadherin ) mutation carriers from hereditary diffuse gastric cancer families . 
gastroenterology 121 : 1348 - 1353 , 2001 kaurah p , macmillan a , boyd n , et al : founder and recurrent cdh1 mutations in families with hereditary diffuse gastric cancer . 
jama 297 : 2360 - 2372 , 2007 van der post rs , vogelaar ip , carneiro f , et al : hereditary diffuse gastric cancer : updated clinical guidelines with an emphasis on germline cdh1 mutation carriers . 
national comprehensive cancer network : nccn clinical practice guidelines in oncology ( nccn guidelines ) : genetic / familial high - risk assessment : breast and ovarian , version 1.2019. 
hallowell n , badger s , richardson s , et al : an investigation of the factors effecting high - risk individuals decision - making about prophylactic total gastrectomy and surveillance for hereditary diffuse gastric cancer ( hdgc )  . 
fam cancer 15 : 665 - 676 , 2016 garland sn , lounsberry j , pelletier g , et al : how do you live without a stomach ? : a multiple case study examination of total gastrectomy for palliation or prophylaxis . 
hamilton jg , abdiwahab e , edwards hm , et al : primary care providers cancer genetic testing - related knowledge , attitudes , and communication behaviors : a systematic review and research agenda . 
harris pa , taylor r , thielke r , et al : research electronic data capture ( redcap ) - - a metadata - driven methodology and workow process for providing translational research informatics support . 
cella d , hughes c , peterman a , et al : a brief assessment of concerns associated with genetic testing for cancer : the multidimensional impact of cancer risk assessment ( micra ) questionnaire . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
balmaa j , digiovanni l , gaddam p , et al : conicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . oncol genomic med 4 : 232 - 236 , 2016 j clin oncol 33 : 3660 - 3667 , 2015 30 . 
katapodi mc , lee ka , facione nc , et al : predictors of perceived breast cancer risk and the relation between perceived risk and breast cancer screening : a meta - analytic review . 
hallowell n , lawton j , badger s , et al : the psychosocial impact of undergoing prophylactic total gastrectomy ( ptg ) to manage the risk of hereditary diffuse gastric cancer ( hdgc )  . 
worster e , liu x , richardson s , et al : the impact of prophylactic total gastrectomy on health - related quality of life : a prospective cohort study . 
odoherty k , suthers gk : risky communication : pitfalls in counseling about risk , and how to avoid thej genet couns 16 : 409 - 417 , 2007 36 . 
wolfe cr , reyna vf , widmer cl , et al : efcacy of a web - based intelligent tutoring system for communicating genetic risk of breast cancer : a fuzzy - trace theory approach . 
 appendix hamilton et al sent survey invitation ( n = 135 ) survey respondents ( n = 71 ) excluded : test report indicated no cdh1 result ( n = 3 ) survey respondents with self - reported understanding of their cdh1 result ( n = 68 ) excluded : respondent did not provide site - specific variant or test report respondent did provide sitespecific variant but it could not be found within the cdh1 gene in clinvar ( n = 5 ) ( n = 3 ) excluded : respondent self - reported understanding of their cdh1 result as my test results are not clear to me respondent self - reported understanding of their cdh1 result as negative genetic test result respondent missing responses to greater than 20% of study variables ( n = 4 ) * ( n = 3 ) ( n = 3 ) evaluable sample for analysis of disagreement among commercial laboratories in variant classifications ( n = 60 ) evaluable sample for analysis of how pv or vus cdh1 results are associated with medical and psychosocial experiences ( n = 57 ) excluded : respondent self - reported understanding of their cdh1 result as my test results are not clear to me ( n = 4 ) * evaluable sample for analysis of disagreement between participant self - report and clinvar classification ( n = 56 ) fig a1 . 
study diagra ( * ) indicates that these excluded cases are the same ; these cases are repeated in the gure to more clearly explain the derivation of the samples used in the study analyses . 
yeager , md1 ; jill fitch , md1 ; joseph stanek , ms1 ; deipanjan nandi , md1 ; and susan vear , md1 introduction ( fu ) nasopharyngeal carcinoma ( npc ) is a rare pediatric malignancy . 
npc in pediatric patients has an incidence of 0.5 to 2 per 100 , 000 persons per year , with only 1% occurring in patients younger than 19 years.1 most cases are treated with chemotherapy such as anthracyclines or pyrimidine uorouracil conjunction with radiation . 
cardiotoxicity , both primary and secondary to severe coronary vasospasm , is an infrequent but well - reported adverse effect of fu.2 life - threatening cardiotoxicity secondary to fu is reported at a frequency of less than 1% across all age groups.3 continuous infusion and concomitant use of cisplatin increases fu cardiotoxicity risk.2 , 4 , 5 pharmacogenomic studies have associated dihydropyrimidine dehydrogenase ( dpyd ) deciency with an increased risk of fu cardiotoxicity.6 - 8 dpyd is the initial and rate - limiting enzyme in the catabolism of fu . 
variants in thymidylate synthase ( tyms ) have been associated with up to a 2.5 - fold risk of toxicity in some studies , whereas others have shown no association with toxicity.9 - 11 to date , to our knowledge , there has been one reported case of a patient with severe cardiomyopathy who had variants in both dpyd and tyms.12 uridine triacetate ( ut ) is a safe and effective antidote when administered quickly after fu overdose , 13 but there are few reports of its use in children . 
on day 3 of her rst 96 - hour fu infusion , the patient developed sudden onset of acute tachycardia , and chest pain , shortness of breath , hemodynamic instability . 
her troponin level was initially mildly elevated at 0.764 ng / ml and ecg demonstrated changes consistent with coronary ischemia , including new q waves , st segment elevation , and t - wave inversions . 
fu infusion was stopped after the administration of a total of 4 , 800 mg ( 1 , 000 mg / m2 / d dosing ) following the administration of 75 mg / m2 cisplatin on day 1 of her therapy . symptoms resolved within a 10 - hour period , and troponin levels decreased to 0.566 ng / ml with improved perfusion and acidosis . 
st segment changes and t - wave inversions initially noted on the patients ecg improved on repeated ecg ( appendix fig a1 )  . given this improvement and stable clinical status , the patients treatment was transitioned to milrinone and she was weaned off dobutamine . 
epinephrine was required to maintain normotension and her chest pain and respiratory distress persisted . given the known association of fu with direct cardiotoxicity and coronary vasospasm with resultant angina and dysfunction , a nitroglycerin drip was initiated . 
ut was started 48 hours after her last dose of fu and within 24 hours after the repeated echocardiograut was dosed at 6.2 g / m2 by mouth every 6 hours for a total of 20 doses . 
because ut is only available in enteral form , it was not started earlier because of worsening respiratory distress and the need for noninvasive positive pressure ventilation , as well as initial concerns for poor gi perfusion . 
symptoms improved and she was weaned off milrinone and nitroglycerine . her troponin levels continued to increase while receiving ut , despite her improved symptoms and echocardiogram ndings ( fig 1 ) ; they eventually normalized weeks later . 
 belsky et al context key objective knowledge generated relevance to consider the effects of variants in dpyd and tyms in association with pyrimidine uorouracil ( fu ) cardiotoxicity in a pediatric patient . 
this case involving these variants adds to the literature evidence of successful uridine triacetate administration in a pediatric patient . the unique genotype of dpyd and tyms in a pediatric cancer patient with cardiotoxicity secondary to fu is presented . 
this case demonstrates the successful use of uridine triacetate in a pediatric patient with heart failure associated with fu treatment . these ndings can be applied to patients with cardiac failure who are receiving fu . 
pharmacogenomics is a rapidly changing eld and as medicine becomes more personalized , clinicians should be aware of variants associated with possible cardiac toxicity before administering fu . symptoms and cardiac dysfunction , the patient was weaned from nitroglycerin and milrinone and maintained on carvedilol . she was discharged home 10 days after her initial clinical decompensation . because of the unique nature of her cardiotoxicity , after consulting with our institutes clinical pharmacology and pharmacogenomics advisory committee , a fu pharmacogenomics panel was sent to arup laboratories ( salt lake city , ut ) after the patient underwent chemotherapy and recovery of wbcs to normal range . 
pharmacogenomic testing revealed two polymorphisms in tyms : heterozygous deletion in the 3 ( cid : 1 ) region ( rs16430 ) , associated with intermediate expression , and a g  . 
the patient was ut start ut stop 1 , 200 mg of fu administered ejection fraction , % 132 96 60 24 12 time since initial ut ( hours ) 84 120 fig 1 . 
ut was approved by the us food and drug administration in december 2015 as a safe and highly effective antidote when administered within 96 hours after fu or capecitabine overdose.13 in one clinical trial , 96% of 135 patients with fu toxicity recovered after treatment , compared with 10% in a historical control group.14 from a pharmacogenomics perspective , variants of tyms have been associated with up to a 2.5 - fold risk of toxicity with fu in some studies but were not associated with increased toxicity in others . 
adult case reports have suggested the importance of pharmacogenomic testing for tyms and dpyd mutations to help toxicity in identied personalize therapy and prevent patients.13 to date , there have been published data on dosing guidelines for fu based on dpyd genotype ; however , no dose adjustment guidelines exist for tyms variants . with these data , we opted to change therapy from fu to gemcitabine and the patient had successful remission of her npc . 
also , given the quick resolution of symptoms with primary vasodilator and scavenger use as well as rapid resolution of cardiac function , an acute cardiomyopathy is thought to be less likely . although the patient experienced relief of symptoms coinciding with the administration of ut , the denitive cause of her decompensation cannot be determined . 
although additional studies would be helpful to better identify risk factors for cardiotoxicity in this patient population and determine the need for pharmacogenomic testing in pediatric patients who receive fu , it is unlikely that such studies would be feasible because of the rarity of presentation . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / author - center . no potential conicts of interest were reported . references fandi a , cvitkovic e : biology and treatment of nasopharyngeal cancer . 
j clin pharmacol 33 : 1060 - 1070 , 1993 polk a , vaage - nilsen m , vistisen k , et al : cardiotoxicity in cancer patients treated with 5 - uorouracil or capecitabine : a systematic review of incidence , manifestations and predisposing factors . 
cancer treat rev 39 : 974 - 984 , 2013 l evy e , piedbois p , buyse m , et al : toxicity of uorouracil in patients with advanced colorectal cancer : effect of administration schedule and prognostic factors . j clin oncol 16 : 3537 - 3541 , 1998 van kuilenburg ab , meinsma r , zoetekouw l , et al : high prevalence of the ivs14 + 1g.a mutation in the dihydropyrimidine dehydrogenase gene of patients with severe 5 - uorouracil - associated toxicity . 
pharmacogenetics 12 : 555 - 558 , 2002 saif mw : dihydropyrimidine dehydrogenase gene ( dpyd ) polymorphism among caucasian and non - caucasian patients with 5 - fuand capecitabine - related toxicity using full sequencing of dpyd . 
cancer genomics proteomics 10 : 89 - 92 , 2013 campbell jm , bateman e , peters md , et al : fluoropyrimidine and platinum toxicity pharmacogenetics : an umbrella review of systematic reviews and metaanalyses . 
pharmacogenomics 17 : 435 - 451 , 2016 shahrokni a , rajebi mr , saif mw : toxicity and efcacy of 5 - uorouracil and capecitabine in a patient with tyms gene polymorphism : a challenge or a dilemma ? clin colorectal cancer 8 : 231 - 234 , 2009 10 . 
saif mw , smith m , maloney a : the rst case of severe takotsubo cardiomyopathy associated with 5 - uorouracil in a patient with abnormalities of both dihydropyrimidine dehydrogenase ( dpyd ) and thymidylate synthase ( tyms ) genes . 
ma ww , saif mw , el - rayes bf , et al : emergency use of uridine triacetate for the prevention and treatment of life - threatening 5 - uorouracil and capecitabine 14 . 
santos c , morgan bw , geller rj : the successful treatment of 5 - uorouracil ( 5 - fu ) overdose in a patient with malignancy and hiv / aids with uridine triacetate . pharmacogenomics j 8 : 278 - 288 , 2008 100 : 1549 - 1557 , 2009 toxicity . 
initial ekg with t wave inversions in inferior leads ( ii , iii , avf ) , q waves in v1 , v2 , and st segment elevation in v3 , v4 . these appear to be stable and / or improving in follow - up ekg no.1 , although st segment elevation is noted again v2 and v3 in follow - up ekg no.2. 
the latest innovations in clinical trials have followed with master protocols , which are dened by inclusive eligibility criteria and devised to interrogate multiple therapies for a given tumor histology and / or multiple histologies for a given therapy under one protocol . 
conventionally conducted within the phase ii setting , basket designs have become popular as drug developers seek to effectively evaluate and identify preliminary efcacy signals among clinical indications identied as promising in preclinical study . 
the latest innovations in clinical trials have followed with master protocols , which are dened by inclusive eligibility criteria and devised to interrogate multiple therapies for a given tumor histology and / or multiple histologies for a given therapy under one protocol.1 , 2 the use of master protocols for oncology has become more common with the desire to improve the efciency of clinical research and accelerate overall drug development . 
the lung - map study , for example , used a master protocol for a phase ii / iii comparative trial designed to evaluate biomarkermatched therapies in patients with previously treated advanced squamous nonsmall - cell lung cancer.3 shortly after initiation , the us food and drug administration approved a new immunotherapy for the same population . 
the designs exibility facilitated subsequent modication of the standard of care , which preserved the relevance of the study.1 a second example includes the create study master protocol , which evaluated the efcacy of crizotinib in patients with alk or met mutations among six different tumor histologies , where each histology constituted a subtrial of alk / met - positive or alk / met - negative tumors.2 emerging cancer therapies may target relatively rare molecular subtypes , which poses practical challenges to completing a clinical trial devised to enroll a single clinical indication . 
second , biomarkerguided treatment selection supersedes traditional clinical indicators for the studied populations such that the presence of a molecular marker predicts response to a targeted therapy irrespective of tumor histology.2 , 4 , 5 thus , basket trials are designed to enroll multiple clinical subpopulations in whom it is assumed that the therapy in question offers benecial efcacy in the presence of the targeted molecular prole . 
most often conducted within the phase ii setting , basket designs have become popular as drug developers seek to effectively evaluate and identify preliminary efcacy signals among clinical indications identied as promising in preclinical study.6 - 8 in certain circumstances , however , evidence acquired from a basket trial has served as the basis for regulatory approval.9 , 10 the framework also poses new challenges to statistical analysis . 
 kaizer et al context key objective describe recent developments in the design of basket trials for oncology studies and elucidate several issues that pertain to their statistical analysis and design . knowledge generated basket trials have evolved from their initial use in exploratory contexts to conrmatory , randomized , and platform trials . 
the context of each trial requires consideration of statistical properties for trial design ( strength and type of type i error control and implications for power ) and methods for analysis ( to pool clinical indications with a common target or accommodate the potential for heterogeneous activity among tumor histologies )  . relevance advances in genomics , disease pathways , and drug discovery have progressed into clinical cancer research . 
innovations in trial design with basket trials facilitate interrogations of multiple therapies for a given tumor histology and / or multiple histologies for a given therapy - target combination that bridges aspects of translational and clinical research paradigms . 
molecularly targeted treatment strategies may not offer acceptable efcacy to all putatively promising clinical indications . proliferation rates of tumor cells are known to vary within and between tumor types.11 moreover , contemporary sequencing methodologies have revealed extensive genetic variation among different types of cancer . 
as drug developers pursue drug approvals with broad labels ( eg , pembrolizumab for which indication was expanded in 2017 to include any unresectable or metastatic solid tumors with microsatellite instability , 12 larotrectinib in 2018 for adults and children who harbor ntrk gene fusion without a known acquired resistance mutation13 ) , trials will evaluate multiple disease indications for agnostic effects . 
for these trials , subpopulation analysis becomes central to the study design and should be considered in the evaluation of trial operating characteristics . trials , discusses this article reviews designs of basket several issues that arise with their implementation , and examines the statistical criteria considered in the development of such trials . 
this section discusses examples of exploratory trials designed as basket trials and introduces recent extensions that convey the evolving landscape of basket trial design in oncology . exploratory designs most basket trials have been conducted within exploratory settings to evaluate agent - specic estimates of tumor response . 
cunanan et al5 described three studies implemented in oncology settings that extend the basic formulation of a basket trial to multiple targets and / or agent combinations . the nci - match trial used a master protocol to enroll participants into drugand mutation - specic baskets while also incorporating genetic screening . 
a basket trial approach was selected to accommodate the rare disease setting , which is limited by traditional large prospective trials.14 the custom trial was a phase ii study with a two - stage design that aimed to identify molecular biomarkers and determine their clinical relevance in patients expected to benet from multiple targeted therapies.15 these trials facilitated the study of less common types of malignancies . 
in addition , these studies were devised to identify potential baskets in which the respective therapies demonstrated promising efcacy and , thus , were exploratory . extensions to randomized , conrmatory designs the methodology for basket trials has been extended to accommodate a wide variety of potential motivations beyond exploratory studies . 
one such extension includes randomized design such that participants are randomly assigned to either a standard - of - care arm without regard to specic genetic mutations or to an arm where a specic mutation is hypothesized to be susceptible to targeted treatment.16 , 17 these designs test the hypothesis that biomarker - guided selection demonstrates benecial treatment efcacy . 
 basket designs : statistical considerations for oncology trials fusion of basket and platform trials may accommodate exploratory and conrmatory study.18 one example of this approach is the signature program , which included a series of eight agent - specic , open - label , phase ii basket trials under a single overarching master protocol.21 the signature program was tissue agnostic and driven by molecular indications with the intention to demonstrate the feasibility of rapid signal nding across multiple tumors . 
molecularly targeted treatment strategies , however , may not offer acceptable efcacy to all putatively promising clinical trials pose challenges to the traditional paradigm for trial design and analysis , which assumes that individual patients who enroll in the same clinical study represent exchangeable units that can be averaged . 
imatinib , for example , was shown to be efcacious in treating malignancies , such as philadelphia chromosomepositive chronic myelogenous leukemia , through the dysregulation of imatinib - sensitive protein tyrosine kinases.23 to determine whether other malignancies with similar kinases respond to treatment , a single - arm , open - label , phase ii study was conducted with inclusive enrollment across 40 different pathologic diagnoses.24 neither the number of indications was constrained nor the design devised to examine subpopulation - specic effects . 
the study represents an example of the challenges posed by indication heterogeneity with conventional study design ( eg , see lacombe et al25 ) , the prediction of which may not be feasible in advance of a studys implementation . the opposite end of the spectrum is dened by studies that evaluate the effectiveness of a treatment strategy for a given subpopulation independent of the evidence acquired from patients in differing patient subsets . 
subpopulation - specic inference also fails to delineate which patient subtypes should be considered nonexchangeable on the basis of the observed data . for example , upon establishing that melanomas that exhibit braf v600 mutations respond to vemurafenib , 26 a basket trial was designed to evaluate the effectiveness of vemurafenib in patients without melanoma , with baskets dened by primary tumor origthe study was devised to interrogate the effectiveness of vemurafenib independently among patients who harbor braf v600 mutations within several prespecied tumor organ sites.5 , 9 despite having designed the study with success criteria that were invariant by tumor indication , the studys analysis plan evaluated evidentiary measures of effectiveness independently for each basket . 
with some baskets having observed low accrual and others yielding one or no response , overall conclusions are difcult to ascertain.27 the polarities of independence and pooling require strong a priori assumptions , which yield poor statistical designs when violated . 
these include multistage designs that merge subtypes at interim analyses28 or bayesian adaptive designs with hierarchical modeling strategies.29 hobbs and landin30 adapted the multisource exchangeability model ( mem ) , 31 which facilitates bayesian inference with respect to all possible pairwise exchangeability relationships among the studied subpopulations . 
the design enables the identication of disjointed subpopulations that comprise meta - subtypes or singleton subtypes on the basis of accumulating evidence during the course of study . design criteria and operating characteristics a basket designs operating characteristics should be determined by the trials intention and phase of development . control of falsely concluding that an inferior experimental therapy offers benet to any clinical indication should be emphasized for conrmatory trials that enroll multiple indications . 
statistical designs of clinical studies are conventionally devised in consideration of distributions of test statistics that measure the extent of evidence acquired against a prespecied null hypothesis upon repeated sampling of the trial data for a given decision rule . 
for hypotheses of superiority , null hypotheses dene value ( s ) of statistical parameters for which the underlying true state of nature is characterized by the absence of treatment effectiveness . 
for one - sample the null often is represented by a xed , prestudies , specied value that represents an expected response rate considered inadequately low to justify additional investigation . 
the decision rule determines the extent to which the trials conclusions could be explained as a result of chance . in this context , a type i error occurs when the null hypothesis is true but the trial yields data for which the decision rule rejects the null hypothesis in favor of a positive nding . 
for basket trials designed to examine multiple indications , the possibility of committing a type i error may occur for tests of each subpopulation , yielding two types of false conclusions : marginal type i error rates estimate the type i error rate for each indication separately , whereas family - wise type i error rates consider the entire trial violation if a single indication falsely rejects the null hyrepresents stronger pothesis . 
when selecting a statistical design devised to enroll and evaluate multiple indications , trialists must synthesize the trials operating characteristics with respect to a diverse array of possible trial outcomes , which we denote hereafter as scenarios . 
the strongest control is therefore conferred by the scenario with only one null indication . decisions that pertain to statistical approaches for analysis of multiple subpopulations , expected enrollment distribution , type i error method , and the strength of type i error control have implications for a designs statistical power . 
in the absence of heterogeneity among indications , the pooling of data acquired from all indications has the potential to increase statistical power ( identify smaller effect sizes )  . 
in addition , increasing imbalance among subpopulation sample sizes may reduce power and / or inate bias under strategies that enable data pooling . hierarchical models devised to share information across indications in relation to estimates of statistical exchangeability have been proposed by various authors18 , 35 - 38 with the intention of increasing statistical power while controlling bias . 
hierarchical models were calibrated for strong control of type i error such that marginal type i error was controlled under scenarios for which only one ( of ve or 10 ) subpopulation was truly ineffective . 
it should be noted , however , that under scenarios with multiple null subpopulations , the designs that resulted from hierarchical models demonstrated both commensurate power and reduced type i error when compared with subpopulation - specic analyses . 
in some cases , drastic reductions in type i error were observed for hierarchical models , such as the global null scenario , where strong borrowing reduced the type i error rate from a target of 10% to approximately 1% when considering 10 indications.39 moreover , the authors failed to adjust frequentist tests for multiple comparisons , which would have attenuated their power . 
in the presence of limited or imbalanced enrollment , however , one may wish to combine subpopulations or use statistical methods to facilitate information sharing among patient subpopulations.5 , 30 guidelines for evaluating the operating characteristics of subpopulation analyses are needed for both conrmatory and nonconrmatory settings.33 , 34 to provide an illustration of the existing strategies and their trade - offs , a simulation study was completed for a xedsample basket trial with ve indications each enrolling 25 patients . 
type i error , however , inates quickly to unacceptable levels in the presence of basket heterogeneity . the independent analysis approach , which adjusts for multiplicity , maintains family - wise error rates , 5% , but it is at the expense of power ( only 0.66 probability of identifying any active basket as efcacious )  . 
finally , the analysis of each basket independently and failure to adjust for multiple comparisons yielded high power ( 0.91 ) with large familywise error rates for all scenarios except the one with four active baskets ( ie , one null basket )  . the method for calibrating basket results for the bayesian model are provided for three posterior probability decision thresholds to illustrate the exibility of trials of various types . 
calibration 1 maintains a marginal type i error at 10% with no active baskets as well as increased probability for identifying effective baskets relative to independent approaches with two or more active baskets . family - wise error and marginal type i error rates are inated with fewer active baskets , however . 
reported is the basket - specic probability of being declared efcacious for null ( nonbold ) and active ( bold ) baskets for multisource exchangeability models ( mems ) with different pp threshold calibrations . 
this stands in contrast multiplicity ( low power of 0.66 ) or do not adjust for multiplicity ( higher power at the expense of higher family - wise error rates of 40% )  . 
the three calibrations presented were selected to demonstrate acceptable designs for different types of basket trials , with calibrations 1 and 2 formulated for exploratory settings and calibration 3 appropriate for conrmatory trials . discussion subpopulation heterogeneity is intrinsic to evaluations of cancer therapies that emerge within the evolving oncology landscape . 
basket trials provide a natural framework for studying molecularly targeted treatment strategies in several potentially promising clinical subpopulations while acknowledging the possibility of heterogeneous results . initiated in exploratory settings , basket designs have evolved to include randomization , enrichment of the enrolled population , and incorporation to platform trials and even acquire conrmatory evidence . 
further innovations and renements may make it possible to use the framework across the full spectrum of clinical translation with seamless design.19 as our simulation study demonstrates , basket trials should require analysis strategies and designs that acknowledge the potential for subpopulation effects . 
several aspects of basket trials , including the recommendations for weak versus strong control of type i error and adjustment for multiplicity , require additional consideration and guidance from academic and regulatory leaders to promote best practices for each stage of the research process.33 as basket trials evolve from simple exploratory trialists trials to increasingly complex master protocols , should avoid simple replication of designs from prior study and instead adapt the trial to its context with appropriate assumptions for the phase of inquiry . our simulation study demonstrates that nave pooling of all subpopulations results in unacceptable type i error , whereas independent examination of each basket without correction for multiplicity may result in inated type i error or , conversely , decreased power to detect efcacious baskets when correcting for multiplicity . 
the mem was evaluated with three different posterior probability threshold calibrations , each demonstrating appropriate operating characteristics for basket trials devised for exploratory and conrmatory settings . further improving their accessibility is the availability of the basket package in r to implement the symmetric mem approach.41 these results stand in contrast to challenges and limitations to information sharing previously reported.34 , 39 one should note a few limitations , however , that remain unresolved by the basket trial framework . 
patients described by a common subpopulation may exhibit sources of heterogeneity on the basis of other important considerations , such as immune prole , prior treatment histology , informatics that redemographics , or additional clinical quire patient - level data analysis . 
for a single tumor histology , this can yield insufcient efcacy not because the drug is necessarily ineffective for the indication but because the subtype in the trial happened to enroll a disproportionate number of patients with refractory disease.27 in settings where indication heterogeneity is not only known but also well understood , an effective means for addressing this type of heterogeneity is to construct baskets derived from information contained in clinical and auxiliary data sources . 
given sufcient enrollment , an indication can be partitioned into prognostic subpopulations and thereby provide new avenues for delineating drug versus prognostic effects at the subpopulation level without randomization . basket trials , like many master protocols , require tissue analysis and molecular proling before registration , which often limits their scope to a small number of leading academic institutions . 
molecular match rates for trials of targeted therapies have been reported to be as low as 4%.42 a single - institution study of the msk - impact assay evaluated 1 , 932 patients and a span of 49 cancer types in the real - world setting and in a matched found that 13% of patients were enroll study.43 by facilitating a centralized platform for acquiring and processing genomic data in conjunction with their functional and therapeutic implications , basket trials may overcome such deciencies . 
this has prompted interrogations of electronic health recordderived measures of real - world progression as alternatives to the response evaluation criteria in solid tumors ( recist ) .44 with the emergence of data science and machine learning , pathologic and radiologic data may offer new avenues for rapid , noninvasive patient proling . 
innovations in radiomics , for example , have effectively yielded prognostic signatures from informatics acquired from scanning technologies used routinely in clinical settings.45 - 48 to address the potential for heterogeneity within a clinical indication , innovations that facilitate use of noninvasive biomedical informatics and algorithms should be pursued with the aim of developing prognostic models in concert with the trials design . 
koopmeiners patents , royalties , other intellectual property : listed as an inventor for us patent 9 , 858 , 665 , which describes a computer - aided design system for predicting prostate cancer using magnetic resonance imaging satrajit roychoudhury employment : pzer leadership : pzer stock and other ownership interests : pzer , novartis david s . 
hong stock and other ownership interests : molecularmatch , oncorena , presagia honoraria : adaptimmune , baxter , merrimack , bayer ag consulting or advisory role : baxter , bayer ag , guidepoint global , janssen pharmaceuticals , genentech , eisai , glg , alpha insights , axiom biotechnologies , adaptimmune , grouph , merrimack , medscape , numab , pzer , seattle genetics , takeda pharmaceuticals , trieza therapeutics research funding : novartis , genentech , eisai , astrazeneca , pzer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer ag , bristol - myers squibb , genmab , ignyta , innity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo oncology , medimmune , molecular templates , takeda pharmaceuticals , seattle genetics , amgen , fate therapeutics , mologen , nci - ctep travel , accommodations , expenses : loxo oncology , mirna therapeutics , genmab brian p . 
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ann oncol 28 : 34 - 43 , 2017 steuer ce , papadimitrakopoulou v , herbst rs , et al : innovative clinical trials : the lung - map study . 
clin pharmacol ther 97 : 488 - 491 , 2015 redig aj , j anne pa : basket trials and the evolution of clinical trial design in an era of genomic medicine . 
j clin oncol 33 : 975 - 977 , 2015 cunanan km , gonen m , shen r , et al : basket trials in oncology : a trade - off between complexity and efciency . 
nakamura y , komatsu y , kato k , et al : btmb - high basket trial : a multicenter phase ii trial of nivolumab monotherapy in patients with advanced gastrointestinal cancers with high blood tumor mutational burden ( btmb )  . 
j clin oncol 37 , 2019 ( suppl ; abstr tps179 ) diamond el , subbiah v , lockhart ac , et al : vemurafenib for braf v600 - mutant erdheim - chester disease and langerhans cell histiocytosis : analysis of data from the histology - independent , phase 2 , open - label ve - basket study . 
sch offski p , wozniak a , escudier b , et al : crizotinib achieves long - lasting disease control in advanced papillary renal - cell carcinoma type 1 patients with met mutations or amplication . 
lopez - chavez a , thomas a , rajan a , et al : molecular proling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
chen c , li x , yuan s , et al : statistical design and considerations of a phase 3 basket trial for simultaneous investigation of multiple tumor types in one study . 
heinrich mc , joensuu h , demetri gd , et al : phase ii , open - label study evaluating the activity of imatinib in treating life - threatening malignancies known to be associated with imatinib - sensitive tyrosine kinases . 
freidlin b , korn el : borrowing information across subgroups in phase ii trials : is it useful ? clin cancer res 19 : 1326 - 1334 , 2013 40 . 
grifth sd , tucker m , bowser b , et al : generating real - world tumor burden endpoints from electronic health record data : comparison of recist , radiologyanchored , and clinician - anchored approaches for abstracting real - world progression in non - small cell lung cancer . 
yu w , tang c , hobbs bp , et al : development and validation of a predictive radiomics model for clinical outcomes in stage i non - small cell lung cancer . 
lacking multivariable specication of relationships among subpopulations , conventional analysis strategies represent the extremes of either pooling all indications or analyzing each indication independently of the evidence acquired for other indications . 
more specically , pooling in this context refers to an analysis strategy devised to evaluate evidence of effectiveness for all indications through statistical inference of a single response rate that is estimated using data from all indications . 
by relying on only one test , marginal and family - wise type i error rates are identical for the pooled approach . at the other extreme , independent analyses infer a total of ve response rates estimated from the data observed within specic indications . 
our simulation study considers the constrained empirical bayes ( ceb ) priors for symmetric mems described by hobbs and landin.30 briey , unconstrained empirical bayes approach to prior specication identies and conditions the analysis with respect to the mem that maximizes the marginal data likelihood . 
while acknowledging the uncertainty about identifying the true mem from the marginal likelihood , the ceb prior constrains shrinkage using an upper bound ( ub ) on the prior probability of inclusion for each source . 
for the basket trial with ve indications , there are six possible scenarios that range from all indications being null ( scenario 1 ) to all indications being alternative ( scenario 6 ) and four intermediate combinations ( scenarios 2 to 5 )  . 
for the bayesian mem approach with ub = 0.10 , posterior probability thresholds were identied that maintained the basket - specic ( marginal ) type i error rate under the global null scenario , the type i error rate for the scenario with one null basket , and the family - wise type i error rate for the global null scenario . 
 o ros1 gene fusion in advanced lung cancer in women : a systematic analysis , review of the literature , and diagnostic algorithm purpose crizotinib , a mesenchymal - epithelial transition / anaplastic lymphoma kinase / c - ros oncogene 1 ( ros1 ) inhibitor , has recently been approved by the us food and drug administration for the treatment of patients with advanced ros1 - positive nonsmall - cell lung cancer ( nsclc )  . 
limited data are available on the prevalence and distribution of ros1 fusions in patients with advanced - stage nsclc . material and methods a series of 727 lung adenocarcinomas from patients with stage iv disease , negative for epidermal growth factor receptor and anaplastic lymphoma kinase alterations , were tested for ros1 fusions by fluorescent in situ hybridization analysis , with confirmation by immunohistochemistry . 
2017 by american society of clinical oncology introduction the identification of oncogene - driven subtypes of nonsmall - cell lung cancer ( nsclc ) has opened the way to clinical application of new classes of anticancer agents directed against specific biologic targets.1 two main molecular aberrations of nsclc were first identified that now have targeted therapies approved for their treatment : mutations in the epidermal growth factor receptor ( egfr ) gene and rearrangements in the anaplastic lymphoma kinase ( alk ) gene.2 , 3 in august 2011 , the us food and drug administration approved crizotinib ( xalkori , pfizer , new york , ny ) to treat locally advanced or metastatic nsclcs that express the abnormal alk fusion protein.4 more recently , another trans - membrane tyrosine kinase receptor gene , the c - ros oncogene 1 po.ascopubs.org jco precision oncology antonio marchetti massimo barberis alessia di lorito maria vittoria pace chiara di lisio lara felicioni elena guerini - rocco andrea vingiani tommaso dantuono marcella liberatore giampaolo filice graziano de luca filippo de marinis antonio passaro luigi guetti luciana irtelli lucio crin `o felice mucilli fiamma buttitta author affiliations appear at the end of this article . corresponding author : fiamma buttitta , md , phd , oncological and cardiovascular molecular medicine unit , cesimet , g . 
 ( ros1 ) , encoding a protein with high homology with alk in its protein kinase domain , has been shown to be altered in a subset of patients with nsclc.5 the genetic alteration occurs in particular gene fusions that render ros1 a constitutively active tyrosine kinase protethe homology between the binding sites of alk1 and ros1 warranted exploration of crizotinib in patients carrying ros1 fusions . 
in a series of clinical studies , patients with advanced nsclc harboring ros1 rearrangements showed great benefit from crizotinib treatment , 6 with an objective response rate of 60%.7 on the basis of the data obtained in these clinical trials , in march 2016 , the food and drug administration expanded the use of crizotinib to include patients with metastatic nsclcs whose tumors have ros1 gene alteration.8genetic changes in ros1 are rare events , affecting approximately 0.5% to 2% of unselected patients with nsclc.5 these prevalence data have been obtained in previous studies that have mainly been conducted retrospectively on resected samples.9 - 13 only a limited number of studies have prospectively investigated ros1 fusions in patients with advanced - stage tumors for treatment selection.14 , 15 ros1 alterations may be detected with a variety of techniques but , currently , most laboratories rely on fluorescence in situ hybridization ( fish ) assays using a dualcolor break - apart probe design . 
given the rarity of ros1 rearrangements in nsclc , screening of tumors by immunohistochemistry ( ihc ) may allow unnecessary fish analyses in patients with ros1 - negative disease to be avoided and thus substantially reduce the cost of testing . although ihc is widely considered a sensitive detection method , it has been shown that in some cases , it can fail in the detection of ros1positive disease . 
given that an efficient assessment of ros1 status in patients with nsclc is important for directing patient care , a combination of different technologies has been suggested to avoid leaving behind patients for treatment . 
however , a multiple technical approach could further increase the costs of diagnosis if indiscriminately applied.16 , 17 the possibility of clinically selecting subclasses of patients with lung cancer with a high probability of harboring ros1 fusions could allow for an accurate evaluation of these patients with multiple diagnostic assays after a screening test . in this study , a large series of advanced - stage lung adenocarcinomas from patients with inoperable disease , selected by clinicians for centralized ros1 testing , were prospectively investigated by fish analysis . 
the study was conducted in accordance with the precepts of the helsinki declaration . ros1 fish and ihc analysis ros1 fish analysis was performed on unstained 4to 5 - micron , formalin - fixed , paraffinembedded tumor tissue sections using the zytolight spec ros1 dual color break apart probe ( zytovysion , bremerhaven , germany ) or the poseidon repeat free ros1 break probe ( kreatech diagnostics , netherlands ) after pretreatment and denaturation steps , according to the manufacturers protocols . 
the orange fluorochrome directlabeled probe hybridizes distal to and the green fluorochrome direct - labeled probe hybridizes proximal to the ros1 break point region at 6q22.1. fish analysis was performed with a slide scanning system under a 603 oil immersion objective with a fluorescence microscope ( olympus bx61 ; olympus corporation , tokyo , japan ) , equipped with appropriate filters , a charge - coupled device camera , and the fish imaging and capturing software solotouch ( bioview duet ; bioview , rehovat , israel )  . 
more than 50 cancer cells per patient were scored , and signals were evaluated with the imaging systetumor samples were considered ros1 fish positive if more than 15% of the tumor cells showed split red and green signals ( signals separated by one or more signal diameters ) and / or single green 39 signal ( deleted green signal ) , in addition to fused and / or broken - apart signals . 
to be included , each study had to meet all of the following criteria : ( 1 ) be performed on series of lung adenocarcinomas investigated for ros1 fusions ; ( 2 ) provided data about the status of the tumor at diagnosis ( early - stage / resectable v latestage / unresectable ) to distinguish between studies performed on patients who underwent surgical resection and studies performed on patients with advanced disease to be selected for pharmacologic treatment ; and ( 3 ) provided the total number of patients and number of patients harboring the ros1 fusion gene in two categorical groups ( positive / negative ) stratified by clinical variables , that is , sex , smoking status , and age at diagnosis . the variables measured in the study were investigated for association using fishers exact test or x2 test , as appropriate . 
the associations of ros1 fusion , as the dependent variable , with sex , age at diagnosis , and smoking history ( smoker or former smoker v nonsmoker ) were also investigated by logistic regression analysis to account for the effect of the different variables . 
in females , ros1 was found to be rearranged in 27 of 266 patients ( 10.2% ) , whereas the prevalence of ros1 fusion in the 461 males was 0.4% ( p = 1.2e - 10 , fishers exact test )  . 
of the 583 smokers , 11 ( 1.9% ) were ros1 positive , whereas 18 of the 144 nonsmokers ( 12.5% ) showed an ros1 rearrangement ( p = 4.05e - 7 , fishers exact test ; table 1 )  . 
the association of ros1 fusion with sex , age , and smoking history was also evaluated by logistic regression analysis to take into consideration the reciprocal effects of the covariables investigated . 
the highest probability of detecting a fusion involving the ros1 gene was in nonsmoking females ( 17% ) , followed by smoking females ( 6.4% ) and nonsmoking males ( 4% )  . 
in the present cohort of patients , 109 ( 15% ) were younger than 50 years of age . nineteen of these 109 patients ( 17% ) showed ros1 fusion , indicating a high prevalence of this genetic alteration in young patients with advanced lung cancer . 
in young female patients , 11 nonsmokers ( 39% ) and seven smokers ( 18% ) were found to be positive for ros1 fusions . our results were compared with those obtained in selected previous studies on ros1 fusions in patients with lung adenocarcinoma . 
on the basis of the inclusion criteria described in the materials and methods section , 13 studies were selected , including 11 studies on resected patients and two on patients with advanced - stage disease . 
 table 3 correlation of clinicopathologic variables with ros1 fusions in patients with resected and advanced - stage lung adenocarcinomas : data from the literature and this study first author no . 
of patients status total ros1 fusion ( n ) status total ( n ) ros1 fusion ( n ) smoking habits mean age ros + ( years ) resected cao18 cha19 chen20 kim21 kim22 lee23 li24 pan26 sholl27 shan16 mescam - mancini25 advanced stage go14 marchetti ( current study ) wu15 total no . 
 sex male female > 50 50 > 50 50 + + + + fig 2 diagram illustrating the risk of carrying an ros1 fusion in patients with late - stage lung adenocarcinomas . 
 , rare ; + , lowprevalence ; + + , medium prevalence ; + + + , high prevalence ; + + + + , very high prevalence . investigated in a conventional clinical workflow for the selection of patients for targeted therapy . 
seven hundred twenty - seven patients , found to be negative for egfr and alk alterations , were evaluated for ros1 gene fusions by fish analysis , with confirmation by ihc . ros1 rearrangements were detected in 29 patients ( 4% )  . 
univariable statistical analysis showed a higher prevalence of ros1 fusions in females ( all but two of 29 patients with positive results were women ) , younger patients , and nonsmokers . 
limited numbers of patients with ros1 - positive disease have been reported in previous studies , and a multivariable analysis taking into account the reciprocal relationship of these three main clinical parameters ( sex , age , and smoking habits ) has never been conducted.9 , 28 - 30 a multivariable logistic regression analysis in our series of patients with advanced lung adenocarcinoma clearly indicated a strong and independent association of ros1 fusions with female sex and younger age . 
the impact of sex , smoking history , and age on the probability of finding an ros1 - positive patient can be easily assessed on the diagrathe highest probability of detecting ros1 gene fusion in patients with lung adenocarcinoma is in nonsmoking females younger than 50 years of age ( high prevalence , near 40% )  . 
nonsmoking females older than 50 years of age showed a medium prevalence of ros1 fusions , together with nonsmoking males younger than 50 years of age . however , for the latter , the number of patients investigated was too low to draw conclusions , and additional data will be necessary to confirm this trend . 
the real - world possibility that ihc and fish , as with other nonin situ techniques ( reverse transcriptase polymerase chain reaction , next - generation sequencing ) , may fail to detect ros1 fusions strengthens the case for confirmation of results by a second if indiscriminately methodology . 
however , applied , a dual technical approach will increase costs and working time.16 , 17 the selection of patients at medium / high / very high risk in the diagram in figure 2 would substantially decrease the number of double assays required for accurate testing . 
the algorithm presented in figure 3 is proposed for an accurate selection of patients to be treated with ros1 inhibitors . for instance , according to this algorithm , a nonsmoking woman who tested negative at the first screening with ihc or fish should be retested with a second technology . our data on patients with advanced lung cancer were compared with data from the literature . because the current study was performed on patients affected by lung adenocarcinomas , only studies performed on patients with lung adenocarcinoma were considered . 
data from 11 independent studies performed on a total of 3 , 190 patients who had undergone resection were compared with those obtained from three studies , including the present one , that analyzed 918 patients with advanced - stage disease ( table 3 )  . 
instead , it clearly emerged that the incidence of ros1 fusions in females and in nonsmokers was markedly higher in patients with advanced disease than in patients with operable disease ; moreover , the mean age at diagnosis was significantly lower in patients with late - state disease . 
 nsclc ( adenocarcinoma or nonsmoker with squamous histology ) ros1 screening by ihc or fish or nonin situ techniques positive negative reconfirmation by a second method others nonsmoking female , patient younger than 50 years old reconfirmation by a second method fig 3 comprehensive algorithm for an accurate selection of patients to be treated with ros1 inhibitors . 
a comparison with data from the literature indicates a different distribution of these three main clinical parameters in patients with ros1 - positive disease at operable and nonoperable disease stages . 
in particular , it is remarkable that among patients with advanced - stage lung adenocarcinoma , there is a large predominance of women in general and women under 50 years old in particular . 
 elena guerini - rocco consulting or advisory role : thermo fisher scientific ( life technologies ) travel , accommodations , expenses : thermo fisher scientific ( life technologies ) andrea vingiani no relationship to disclose tommaso dantuono no relationship to disclose marcella liberatore no relationship to disclose giampaolo filice no relationship to disclose graziano de luca no relationship to disclose filippo de marinis no relationship to disclose antonio passaro no relationship to disclose luigi guetti no relationship to disclose luciana irtelli no relationship to disclose felice mucilli no relationship to disclose fiamma buttitta no relationship to disclose lucio crin `o honoraria : bristol - meyers squibb , astrazeneca , pfizer affiliations antonio marchetti , alessia di lorito , maria vittoria pace , chiara di lisio , lara felicioni , tommaso dantuono , marcella liberatore , giampaolo filice , graziano de luca , luigi guetti , luciana irtelli , felice mucilli , and fiamma buttitta , university of chieti - pescara , chieti ; massimo barberis , elena guerini - rocco , andrea vingiani , filippo de marinis , and antonio passaro , european institute of oncology , milan ; and lucio crin `o , istituto oncologico romagnolo irccs meldola forli , meldola , italy . references 2012 ( suppl 1 ) 1 . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as first - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
warth a , muley t , dienemann h , et al : ros1 expression and translocations in non - small - cell lung cancer : clinicopathological analysis of 1478 cases . 
cheng h , ye l , xue l : detection of ros1 gene rearrangement by fish and analysis of its clinical features in nonsmall cell lung cancer patients [ in chinese ]  . 
go h , kim dw , kim d , et al : clinicopathologic analysis of ros1 - rearranged non - small - cell lung cancer and proposal of a diagnostic algorithj thorac oncol 8 : 1445 - 1450 , 2013 15 . 
wu s , wang j , zhou l , et al : clinicopathological characteristics and outcomes of ros1 - rearranged patients with lung adenocarcinoma without egfr , kras mutations and alk rearrangements . 
shan l , lian f , guo l , et al : detection of ros1 gene rearrangement in lung adenocarcinoma : comparison of ihc , fish and real - time rt - pcr . 
wu j , lin y , he x , et al : comparison of detection methods and follow - up study on the tyrosine kinase inhibitors therapy in non - small cell lung cancer patients with ros1 fusion rearrangement . 
cao b , wei p , liu z , et al : detection of lung adenocarcinoma with ros1 rearrangement by ihc , fish , and rt - pcr and analysis of its clinicopathologic features . 
chen yf , hsieh ms , wu sg , et al : clinical and the prognostic characteristics of lung adenocarcinoma patients with ros1 fusion in comparison with other driver mutations in east asian populations . 
li c , fang r , sun y , et al : spectrum of oncogenic driver mutations in lung adenocarcinomas from east asian never mod pathol 28 : 468 - 479 , 2015 smokers . 
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pan y , zhang y , li y , et al : alk , ros1 and ret fusions in 1139 lung adenocarcinomas : a comprehensive study of common and fusion pattern - specific clinicopathologic , histologic and cytologic features . 
jurmeister p , lenze d , berg e , et al : parallel screening for alk , met and ros1 alterations in non - small cell lung cancer with implications for daily routine testing . 
lung cancer 87 : 122 - 129 , 2015 jin y , sun pl , kim h , et al : ros1 gene rearrangement and copy number gain in non - small cell lung cancer . 
 predicting expected absolute chemotherapy treatment benet in women with early - stage breast cancer using endopredict , an integrated 12 - gene clinicomolecular assay hatem soliman , md1 ; darl d . 
flake ii , phd2 ; anthony magliocco , md1 ; mark robson , md3 ; lee schwartzberg , md4 ; priyanka sharma , md5 ; krystal brown , phd2 ; saskia wehnelt2 ; ralf kronenwett , md , phd6 ; alexander gutin , phd2 ; johnathan lancaster , md , phd2 ; jack cuzick , phd7 ; and william gradishar , md8 purpose previous studies have shown endopredict ( epclin ) , a test that integrates 12 - gene expression data with nodal status and tumor size , to be predictive for risk of distant recurrence in women with estrogen receptorpositive , human epidermal growth factor receptor 2negative early - stage breast cancer . 
here , we modeled expected absolute chemotherapy benet on the basis of epclin test results . methods the effect of chemotherapy was modeled using previously validated 10 - year risk of distant recurrence as a function of epclin score for patients treated without chemotherapy . 
the early breast cancer trialists collaborative group performed a meta - analysis of more than 100 clinical trials in more than 100 , 000 women to evaluate the benet of adjuvant chemotherapy.6 although the in individual benet trials varied considerably , 3 this meta - analysis demonstrated an average 30% relative reduction in distant recurrence among women who received chemotherapy compared with those who did not.6 for many patients with er - positive disease , the risk of distant recurrence is sufciently low that et alone is adequate . 
in these patients , the adverse effects associated with chemotherapy may outweigh any benet provided by a reduced risk of disease recurrence . historically , identication of these low - risk patients has relied on clinicopathologic parameters , such as nodal status , tumor size , and tumor grade . 
 soliman et al context key objective can an integrated , 12 - gene , clinicomolecular assay predict absolute benet from chemotherapy for women with estrogen receptor ( er ) positive , human epidermal growth factor receptor 2 ( her2 ) negative breast cancer ? knowledge generated in this model , patients with low 12 - gene scores showed no difference in recurrence - free survival with or without chemotherapy , whereas those with high 12 - gene scores showed a marked increase in recurrence - free survival with the addition of chemotherapy . 
overall , this study suggests that the 12 - gene clinicomolecular score is able to predict absolute benet of chemotherapy for women with er - positive , her2 - negative breast cancer . relevance accurate risk assessment is critical for determining appropriate treatment of women with breast cancer . 
breast cancer prognostic assays like the 12 - gene clinicomolecular score have been shown to provide more information about risk than standard clinical information alone in predicting recurrence - free survival in the absence of treatment . 
these new data support the ability of the 12 - gene clinicomolecular score to also predict absolute benet from chemotherapy to help to guide chemotherapy decisions for women with er - positive , her2 - negative breast cancer . are inadequate to guide adjuvant chemotherapy decisions reliably.7 thus , when risk is dened using clinicopathologic features alone , a subset of truly low - risk patients receives unnecessary chemotherapy , whereas others at high risk forgo chemotherapy and experience avoidable disease recurrence . to address this clinical dilemma , multigene expression prognostic assays have been developed for patients with er - positive , human epidermal growth factor receptor 2 ( her2 ) negative early - stage breast cancer . 
several such assays are clinically available , with variable performance according to nodal status , and early ( 0 to 5 years ) versus late ( 5 or more years ) recurrence.8 - 11 these assays better quantify residual risk of recurrence after surgery and et than clinicopathologic features alone , which enables physicians to tailor the use of adjuvant therapies ( et alone v et + c ) more accurately . 
to this end , evidence - based practice guidelines now indicate that prognostic assays are appropriate tools to help guide decision making.12 - 14 one such test is endopredict ( myriad genetics , salt lake city , ut ) , which integrates a 12 - gene molecular score with nodal status and tumor size into a combined clinicomolecular score ( epclin )  . 
previous studies have validated that epclin accurately predicts the risk of distant metastases in patients with er - positive , her2 - negative breast cancers.11 , 15 - 18 although this information can reliably identify patients at sufciently low risk so that chemotherapy may be avoided safely , the ability of epclin to predict benet from the addition of chemotherapy has yet to be fully dened . 
ideal approaches to evaluate this are limited because archival samples from previous randomized trials of et 6 c in appropriate patients largely have been exhausted.3 , 5 a prospective trial of epclin that includes an arm randomized to receive no chemotherapy would now be unethical , given the established benet of chemotherapy for patients with high - risk disease . 
alternative study designs , therefore , are required to explore the scope of epclins ability to predict adjuvant chemotherapy benet for patients with er - positive , her2 - negative earlystage breast cancer . so far , classic factors that inuence breast cancer prognosis have not shown an interaction between the relative effect of adjuvant chemotherapy on absolute risk of recurrence.19 furthermore , the absolute benet of chemotherapy depends on the patients baseline risk of developing recurrent disease.19 as such , as we evaluate a biomarker , it is helpful to understand the principal drivers of its chemopredictive ability . 
one possibility is that chemopredictive ability is driven by high prognostic accuracy , that is , the ability of the biomarker to differentiate those patients at highest versus lowest absolute risk of recurrence and , thus , those latter patients for whom chemotherapy cannot yield any clinically meaningful benet . 
alternatively , it is possible that a biomarkers chemopredictive ability is driven by differences in relative chemotherapy benet between higher versus lower biomarker - dened patient groups ( ie , interaction between the biomarker score and relative chemotherapy benet )  . in the current study , we describe a modeling study that uses epclin score , absolute risk of recurrence , and reduction of this risk associated with the addition of chemotherapy to estimate the differences in absolute risk for distant recurrence across epclin scores . 
we demonstrate that for a molecular marker such as epclin , patients with the highest baseline absolute risk for recurrence experience the greatest absolute benet from chemotherapy . furthermore , we establish that the key factor in any biomarkers chemopredictive capacity is the ability to predict accurately the baseline absolute risk of recurrence . 
through this modeling , we estimate the differences in absolute risk of distant recurrence across epclin scores and examine the impact of different amounts of statistical interaction between epclin and chemotherapy on these estimates . methods gene expression assay the 12 - gene mrna expression assay has been previously described in detail.20 - 22 in brief , the expression of three proliferation - related target genes ( birc5 , dhcr7 , ube2c ) , ve hormone receptorrelated target genes ( azgp1 , il6st , mgp , rbbp8 , stc2 ) , and three normalization genes ( calm2 , oaz1 , rpl37a ) were measured by reversetranscription quantitative polymerase chain reaction . 
a 12gene molecular score was calculated as the linear combination of the normalized target gene expression.11 , 22 the clinicomolecular score epclin was calculated by combining the 12 - gene molecular score with tumor size and the number of positive lymph nodes and was reported as a numerical score from 1 to 6.11 , 22 tumors with an epclin score of less than 3.3 are considered low risk for distant recurrence and tumors with scores of 3.3 or greater are considered high risk for distant recurrence.11 , 17 , 18 statistical methods the ability of epclin to provide an estimate of expected chemotherapy benet was modeled , as shown in figure 1 . the primary component was the prognostic value of epclin to predict the rate of distant recurrence in the rst 10 years of follow - up . 
 soliman et al 10 - year distant recurrence in patients treated with et + c ( treated ) was estimated by introducing a relative chemotherapy benet for a particular epclin score , hrtreatment , to the untreated risk according to a proportional hazards model ( fig 1b ) , as in equation 1 : rtreated ( cid : 1 ) 1 1 runtreated ( cid : 1 ) ( cid : 3 ) hrtreatment mathematically , the dependence of the relative chemotherapy benet on the risk of distant recurrence was modeled using a main effect for chemotherapy and an interaction between treatment status and the prognostic signature.23 interactions were modeled as a linear dependence of the logarithm of hr for treatment on epclin score according to equation 2 : ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 1 ) hrtreatment ( cid : 1 ) ( cid : 1 ) ln hroverall ( cid : 1 ) epclin epclinavg in this equation , represents the interaction strength and denes how strongly the relative chemotherapy benet for a patient depends on epclin score , epclinavg is the mean epclin score in the population , and hroverall is the hazard ratio for the chemotherapy benet in the population . 
with the maximum value of determined for an interaction giving no chemotherapy benet at epclinmin , weaker interactions were modeled using a percentage of the maximum value of ( fig 1b )  . finally , the absolute benet ab from chemotherapy for treated patients was determined according to equation 3 ( fig 1c ) : december 8 , 2017 , who received valid test results . formalin - xed parafn - embedded breast resections of treatment - nave er - positive , her2 - negative breast tissue were tested . 
these scores also were used to calculate epclinavg . results we examined the impact of different magnitudes of treatment effect and interaction strengths on the estimated 10 - year risk of distant recurrence ( table 1 )  . 
maximal interaction strength ( max = 0.159 ) was rst determined by assuming that a patients relative chemotherapy benet is 0 at the lowest possible epclin score and maintaining the hroverall of treatment at 0.7. 
the corresponding hrtreatment as a function of epclin score is shown in figure 2 . hrtreatment is 1 for a patient with an epclin score of 1 and 0.45 for a patient with the maximum observed epclin score of 6 . 
the risk of distant recurrence in the treated arm also was evaluated in a conservative scenario that assumed no interaction between chemotherapy benet and epclin score ( ie , 0% interaction strength , constant hrtreatment )  . 
in this scenario , the relative chemotherapy benet was equal to the overall chemotherapy benet ( = 0 ; hrtreatment = 0.7 ; fig 2 )  . after max was determined , risk of distant recurrence was calculated for scenarios with a variety of interaction strengths between epclin and chemotherapy . 
figure 3a shows the relationship between epclin score and predicted risk of distant recurrence by 10 years for untreated and treated patients under interaction strength ( 0% , 50% , and 100% )  . 
absolute chemotherapy benet for patients with low and high epclin scores assuming different overall relative chemotherapy benet ( 20% , 30% , or 40% ) for different relative interaction strengths ( 0% , 50% , or 100% ) absolute chemotherapy benet ( % ) 20% relative chemotherapy benet low epclin high epclin 0% relative interaction ( no interaction ) 50% relative interaction ab ( cid : 1 ) runtreated rtreated 100% relative interaction ( maximal ) 30% relative chemotherapy benet low epclin high epclin absolute chemotherapy benet for the low - risk category was calculated as a mean absolute chemotherapy benet for all low - risk patients , and the same went for the high - risk category . 
 predicting chemotherapy benet in early - stage breast cancer ln ( hrtreatment ) = ln ( hroverall ) ( epclin epclinavg ) 0% interaction strength ( = 0 ) 100% interaction strength ( = 0.159 ) epclin score fig 2 . 
patient benet from chemotherapy ( hrtreatment ) according to epclin score at no interaction ( 0% ) and maximal interaction ( 100% )  . recurrence is low for low epclin scores , which results in small absolute chemotherapy benet . 
for example , the expected absolute benet of chemotherapy treatment for a patient with low epclin scores ranged from 0.3% ( epclin = 1 ) to 2.9% ( epclin = 3.3 ) for 0% interaction strength and from 0% to 3.0% for 100% interaction strength . 
similar results were obtained when overall relative chemotherapy benet was modeled to be lower ( 20% ; fig 3b ) or higher ( 40% ; table 1 ; fig 3c )  . the various risk estimates across all scenarios of interaction strength were applied to a clinical cohort of patients with er - positive , her2 - negative breast resections and representative epclin scores ( n = 2 , 185 )  . 
the full epclin distribution is shown in figure 4 . overall , 1 , 275 samples ( 58% ) were low risk , and 910 ( 42% ) were high risk . 
risk of distant recurrence as a function of epclin score for different interaction strengths under different assumptions about overall relative chemotherapy benet : ( a ) 30% , ( b ) 20% , and ( c ) 40% . 
epclin scores in pretreatment estrogen receptorpositive , human epidermal growth factor receptor 2negative breast resection tissue ( n = 2 , 185 )  . the absolute chemotherapy benet in lowand high - risk patients was calculated as a function of interaction strength ( fig 5 )  . 
indeed , even with the strongest interaction , the absolute chemotherapy benet for a 30% relative benet in high - risk patients is 7.3% , which is not dramatically different from the 5.3% benet modeled in the patients with high ( 3.3 ) epclin score patients with low ( < 3.3 ) epclin score 40% overall benefit 30% overall benefit 20% overall benefit case of no interaction ( table 1 )  . 
similarly , in low - risk patients , the absolute benet is 1.5% when we assume the strongest interaction , which is close to a 1.8% benet in the case of no interaction . discussion previous studies have demonstrated that epclin accurately identies patients at low risk for distant recurrence 10 years after surgery , with improved prognostic performance compared with clinical features alone or other molecular tests.11 , 15 - 18 for these low - risk patients , it is clear that the addition of adjuvant chemotherapy likely will not yield any clinically meaningful risk reduction . 
here , we evaluated the capacity of epclin to identify patients with er - positive , her2 - negative earlystage breast cancer who may benet most from adding adjuvant chemotherapy to et . 
thus , we evaluated the impact by modeling across a range of potential chemotherapy effects sizes and interaction strengths with epclin . to minimize potential error associated with individual trial values , the absolute benet of chemotherapy in women with various epclin scores was modeled using wellestablished estimates of the average relative benet of adjuvant chemotherapy . 
this risk is particularly noteworthy in interventions in early - stage breast studies of adjuvant cancer because event rates may be low and distant recurrence may manifest many years or even decades after the initial diagnosis and treatment . 
as a result , the absolute predicted chemotherapy benet in low - risk patients was small and largely unaffected by average chemotherapy effect or interaction strength , whereas the toxicity of therapy remains the same . 
this association is irrespective of interaction strength between epclin and predicted chemotherapy benet , and the impact of any interaction on absolute benet is much smaller than the ability to accurately estimate absolute risk . as is typical of modeling studies , this study is not without limitations . 
of note , the approximately 30% reduction in distant recurrence was selected on the basis of its association with chemotherapy regimens that are more consistent with modern patterns of care in contrast to more historic regimens . other aspects of the statistical model are also limitations of the study . 
it is assumed that the relative benet of chemotherapy linearly depends on epclin score ( eq 2 ) , which is the simplest mathematical implementation of dependence . linear dependence also was used to demonstrate interaction between chemotherapy and a prognostic score.8 in statistical analysis , the most common implementation of interaction between variables has the same functional forin addition , only positive interaction between chemotherapy benet and epclin score was included in this analysis because it is expected that high expression of the proliferation - related genes in epclin is associated with higher rather than lower relative chemotherapy benet . 
conversely , high expression of the hormone receptorrelated genes is expected to be associated with smaller relative chemotherapy benet because er - negative tumors have a much stronger response to chemotherapy than er - positive tumors . 
this again corresponds to a positive interaction because the hormone receptorrelated genes contribute negatively to the epclin score . in summary , this modeling analysis demonstrates that epclin is able to predict which patients will gain maximum absolute benet from chemotherapy . 
in addition , these data indicate that the predicted absolute impact of chemotherapy on distant recurrence depends much more on the prognostic ability of the biomarker to predict an individual womans risk of recurrence accurately . 
endopredict has been shown in multiple studies to predict risk of distant recurrence accurately in women with er - positive , her2 - negative early - stage breast cancer who receive 5 years of et , with an accuracy similar to the other best breast prognostic tests and substantially better than the 21 - gene recurrence score ( oncotype dx ; genomic health , redwood city , ca ) .18 , 24 this modeling indicates identied a substantial proportion of that endopredict women whose risk of breast cancer recurrence was so low that the addition of adjuvant chemotherapy would not produce a clinically meaningful benet on recurrence risk . conversely , patients with high epclin scores were predicted to experience the greatest benet from chemotherapy regardless of the simulated interaction strength between epclin and predicted chemotherapy benet . 
flake , anthony magliocco , mark robson , lee schwartzberg , priyanka sharma , ralf kronenwett , alexander gutin , johnathan lancaster , jack cuzick , william gradishar collection and assembly of data : darl d . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . hatem soliman consulting or advisory role : celgene , astrazeneca , eli lilly , novartis , pzer , puma biotechnology research funding : amgen ( inst ) travel , accommodations , expenses : astrazeneca , eli lilly darl d . 
flake employment : myriad genetics stock and other ownership interests : myriad genetics patents , royalties , other intellectual property : multiple patents related to the development of tests at myriad genetics anthony magliocco stock and other ownership interests : protean biodiagnostics , the genomic cancer institute , proscia honoraria : bristol - myers squibb , merck , illumina , leica consulting or advisory role : bristol - myers squibb , merck , proscia , roche , illumina speakers bureau : bristol - myers squibb research funding : biotheranostics , roche , genentech patents , royalties , other intellectual property : various patents pending as co - inventor through moftt cancer center travel , accommodations , expenses : menarini silicon biosystems , illumina , bristol - myers squibb , merck , ventana medical systems mark robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca , merck , pzer , daiichi sankyo research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca , pzer lee schwartzberg stock and other ownership interests : vector oncology honoraria : pzer , amgen , nanostring technologies , novartis , napo , taiho pharmaceutical , genentech , e.r. 
squibb and sons , helsinn therapeutics , genomic health , myriad genetics , astrazeneca consulting or advisory role : bristol - myers squibb , pzer , helsinn therapeutics , caris life sciences , spectrum pharmaceuticals , tesaro , genomic health , astrazeneca , e.r. 
squibb and sons , amgen , f . hoffmann - la roche , genentech , eli lilly , novartis , merck , biocept , abbvie , biotheranostics , athenex , coherus biosciences speakers bureau : coherus biosciences , puma biotechnology research funding : amgen ( inst ) , glaxosmithkline ( inst ) , spectrum pharmaceuticals ( inst ) , medivation ( inst ) , bayer ag ( inst ) , genentech ( inst ) , pzer ( inst ) , tesaro ( inst ) , sano ( inst ) , e.r. 
n engl j med 319 : 1681 - 1692 , 1988 early breast cancer trialists collaborative group : tamoxifen for early breast cancer : an overview of the randomised trials . 
lancet 351 : 1451 - 1467 , 1998 early breast cancer trialists collaborative group ( ebctcg ) : effects of chemotherapy and hormonal therapy for early breast cancer on recurrence and 15 - year survival : an overview of the randomised trials . 
lancet 365 : 1687 - 1717 , 2005 peto r , davies c , godwin j , et al : comparisons between different polychemotherapy regimens for early breast cancer : meta - analyses of long - term outcome among 100 , 000 women in 123 randomised trials . 
curr treat options oncol 16 : 23 , 2015 paik s , tang g , shak s , et al : gene expression and benet of chemotherapy in women with node - negative , estrogen receptor - positive breast cancer . 
j clin oncol 24 : 3726 - 3734 , 2006 van de vijver mj , he yd , vant veer lj , et al : a gene - expression signature as a predictor of survival in breast cancer . 
gnant m , filipits m , greil r , et al : predicting distant recurrence in receptor - positive breast cancer patients with limited clinicopathological risk : using the pam50 risk of recurrence score in 1478 postmenopausal patients of the abcsg - 8 trial treated with adjuvant endocrine therapy alone . 
filipits m , rudas m , jakesz r , et al : a new molecular predictor of distant recurrence in er - positive , her2 - negative breast cancer adds independent information to conventional clinical risk factors . 
coates as , winer ep , goldhirsch a , et al : tailoring therapies - - improving the management of early breast cancer : st gallen international expert consensus on the primary therapy of early breast cancer 2015 . 
harris ln , ismaila n , mcshane lm , et al : use of biomarkers to guide decisions on adjuvant systemic therapy for women with early - stage invasive breast cancer : american society of clinical oncology clinical practice guideline . 
dubsky p , filipits m , jakesz r , et al : endopredict improves the prognostic classication derived from common clinical guidelines in er - positive , her2 - negative 17 . 
martin m , brase jc , calvo l , et al : clinical validation of the endopredict test in node - positive , chemotherapy - treated er + / her2breast cancer patients : results early breast cancer . 
buus r , sestak i , kronenwett r , et al : comparison of endopredict and epclin with oncotype dx recurrence score for prediction of risk of distant recurrence after endocrine therapy . 
warf mb , rajamani s , krappmann k , et al : analytical validation of a 12 - gene molecular test for the prediction of distant recurrence in breast cancer . 
sestak i , buus r , cuzick j , et al : comparison of the performance of 6 prognostic signatures for estrogen receptor - positive breast cancer : a secondary analysis of a randomized clinical trial . 
lumbar spine magnetic resonance imaging ( mri ) demonstrated multiple bone lesions , and computed tomography scans revealed a 4 - cm right - sided hilar lung mass , regional thoracic lymphadenopathy , multiple hepatic metastases , a left - sided adrenal metastasis , and several osseous lesions ( fig 1a )  . 
biopsies of the subcarinal lymph node and the left - side adrenal lesion were performed , which confirmed adenocarcinoma of lung origin ( figs 2a and 2b )  . the patient was treated with radiation therapy to the painful vertebral metastasis and stereotactic radiosurgery to two brain lesions . 
200 genes ( foundationone ; foundation medicine , cambridge , ma ) revealed an egfr exon 19 deletion ( del19 ) mutation , a tp53 v173l mutation , an egfr amplification , and an rb1 loss of exons 18 and 19 . oral erlotinib 150 mg daily was initiated in may 2015 , and uniform disease response was evident on restaging scans in july 2015 ( fig 1b )  . 
however , in october 2015 , repeat imaging showed significant growth in a single liver lesion and a new 2.6 - cm lesion in the spleen , with continued response elsewhere , including the brain ( fig 1c )  . repeat biopsy of the enlarging liver lesion in november 2015 revealed nests of highly atypical cells with finely dispersed chromatin , inconspicuous nucleoli , and abundant mitoses ( figs 2c to 2e )  . immunohistochemical stains were positive for synaptophysin and chromogranin and negative for thyroid transcription factor 1 and napsin a . 
the overall features were consistent with small - cell lung cancer ( sclc ) transformation.4 ngs that consisted of targeted hotspot evaluation in 39 genes ( snapshot ngs ; massachusetts general hospital , boston , ma ) confirmed the presence of the original egfr del19 and tp53 mutations and showed additional mutations in pik3ca ( g545l ) , pik3ca ( g726l ) , erbb3 ( g337a ) , and fbxw7 ( l8p )  . 
a patientderived xenograft generated from this biopsy specimen lacked rb protein expression but retained minimal egfr expression and demonstrated activation of the mitogen - activated protein kinase and akt pathways ( fig 3c ) , likely as a result of the presence of an activating pik3ca mutation . the patient was treated with carboplatin and etoposide chemotherapy and ongoing erlotinib . 
scans after four cycles of chemotherapy showed a mixed response with slight regression in the previously biopsied ( sclc - transformed ) liver metastasis , stable brain metastases , and multiple new distinct sites of hepatic progression ( fig 1d )  . 
 ( a to e ) selected radiographic images of the liver illustrate involvement with cancer . treatments and key biopsy ( bx ) results ( tissue or liquid ) are indicated underneath each image in chronologic order . 
of note , the guardant360 assay can detect rb1 inactivating mutations but not allelic losses . we interpreted the emergence of an egfr t790m positive clone as the most likely resistance mechanism within the growing liver nodules . 
the patient discontinued chemotherapy , and the t790m - specific tki osimertinib7 was administered in march 2016 . restaging in june 2016 ( performed with mri because of renal dysfunction ) revealed that the hepatic lesions that had most recently progressed on chemotherapy ( presumed t790m positive ) had stabilized , but the liver lesion biopsied in 2015 ( sclc histology at that time ) had again enlarged with no other sites of systemic or intracranial progression ( fig 1e )  . 
a repeat plasma guardant360 test in june 2016 confirmed that egfr t790m was now undetectable , but increases were found in the mafs of pik3ca e726k ( 50.9% ) , pik3ca e545k ( 54.3% ) , tp53 v173l ( 54.8% ) , and egfr del19 ( 45.5% ; fig 4 )  . 
 ( a ) hematoxylin and eosin ( h&e ) stain and ( b ) thyroid transcription factor 1 ( ttf - 1 ) immunostain of fine - needle aspiration of a subcarinal lymph node at diagnosis show adenocarcinoma with diffuse ttf - 1 expression consistent with a lung primary . 
 ( c ) h&e stain and ( d ) synaptophysin ( syn ) and ( e ) ttf - 1 immunostains of a liver core biopsy at the time of acquired resistance to erlotinib demonstrate small - cell lung cancer with solid nests of highly atypical epithelial cells with finely dispersed chromatin , inconspicuous nucleoli , and brisk mitotic activity . 
 ( a ) summary of all evaluable probes across all chromosomes ( red , genomic gains ; blue , genomic losses ) shows diffuse losses across chromosome 13 , including the rb1 gene locus . 
 ( b ) a magnified view of four specific genes on chromosome 13 shows that all examined loci of rb1 are lost , with only blue signals and complete absence of red signals . 
 ( c ) tissue obtained from the november 2015 liver biopsy ( which shows sclc ) wasusedtogenerateapatient - derivedxenograft ( pdx ) inannsgmouseandsubsequentlypassagedthroughadditionalnsgmice.thepdxtumordemonstrated sclc histologic features consistent with the patient biopsy sample ( not shown )  . 
a western blot demonstrates relative protein levels of egfr , p - akt ( s473 ) , p - erk , rb , p16 , and actin ( loading control ) among pdx tumors ( mgh1529 ; two tumors shown ) with control lung adenocarcinoma ( adenoca ) and sclc samples for comparison . genetic characteristics of the various cell lines ( rb1 , p16 , and egfr exon 19 deletion [ del19 ] mutations [ mut ] ) are shown above the western blot . 
however , one resistant clone with sclc morphology emerged clinically in october 2015 , and genotyping confirmed an additional private pik3ca e545l mutation , which often is seen in sclc - transformed egfr mutant clones.4 during chemotherapy , we believe that the sclc clone diminished , whereas another clone that harbored an acquired egfr t790m mutation and perhaps two other distinct pik3ca mutations ( e545k and e726k ) emerged as observed in plasma ctdna in march 2016 . although a tissue biopsy specimen could not be obtained at that time , on the basis of our prior observation that sclc and adenocarcinoma populations can oscillate in response to specific treatment4 and that t790m is rarely seen in sclc - transformed tissue biopsy specimens , we hypothesize that the t790m - positive clone detected in plasma maintained an adenocarcinoma phenotype . 
the t790m clone was no longer detectable by june 2016 after treatment with osimertinib , but one or more other clones became dominant with increasing mafs , and subsequently , the disease became refractory to therapy ( fig 4 )  . 
this elevation in ctdna and subsequent clinical decline mirror data that demonstrated the correlation of increased mafs and decreased overall survival.9 - 11 in addition , the patient had a tumor with baseline rb1 mutation that was expected to lead to loss of function and is believed to play an essential role in the histologic transformation to sclc among egfr mutant cancers . 
we previously demonstrated that rb1 is universally lost in sclc - transformed cancers , although not sufficiently for transformation.12 recent work has demonstrated that baseline rb1 loss among egfr mutant tumors is a strong predictor for subsequent sclc transformation.13 as the clinical use of ngs panels increases and baseline inactivating rb1 mutations are more frequently detected , more data to understand the implications will be required , including a better understanding of the critical steps that lead to the lineage shift , so that we can develop more - effective treatment strategies.14 finally , this case report illustrates the potential utility of longitudinal molecular profiling during targeted therapy . 
at present , two mutationspecific food and drug administrationapproved plasma tests may be used to select egfr tkis.15 , 16 clinical practice is rapidly evolving , but on the basis of current evidence , it is reasonable to offer plasma genotyping upon progression with frontline egfr tkis to evaluate for t790m . 
 testing is negative for t790m , reflexive tissue biopsy should be performed because approximately 30% of ctdna test results will be false negative.17 the exact role of liquid biopsies for serial monitoring requires more rigorous evaluation , but a key appeal is that tumor biopsy findings may underestimate the full spectrum of resistant clones present at the time of progression.6 , 18 , 19 in practice , we commonly see the type of mixed radiographic response as observed in this patient with regression of some sites but continued growth in others . 
heterogeneity among distinct cancer subclones may explain such disparate responses , and longitudinal plasma testing might be a valuable adjunct to tissue biopsies to understand the dynamic evolution of various clones . for example , although tissue biopsy may offer critical information about the histology and molecular alterations of a specific progressing lesion , it may lack information about other sites of disease . 
conversely , ctdna genotyping could paint a more - complete picture of the competing resistance clones within a patient , although precise determination of which molecular alterations coexist within one clone or in one anatomic site are not currently possible . 
indeed , other studies have demonstrated that multiple resistance mechanisms can be detected within plasma , 18 and we and others have observed that longitudinal ctdna analyses can track the rise and fall of distinct subclones.6 , 20 in summary , this case report illustrates that the relative magnitude of resistant subclones can fluctuate in response to therapy , that liquid biopsies hold great potential to detect and monitor distinct genetic subpopulations within a patient , and that the presence of a baseline rb1 mutation in an egfr mutant cancer and subsequent sclc transformation raises important questions about monitoring such patients . 
for those with egfr mutant lung cancers , both tissue and liquid biopsy specimens can yield critical information to elucidate dominant clones that drive cancer growth at various time points . 
mooradian no relationship to disclose zofia piotrowska consulting or advisory role : boehringer ingelheim , astrazeneca , ariad pharmaceuticals , takeda pharmaceuticals , superdimension research funding : guardant health ( inst ) benjamin j . 
drapkin no relationship to disclose dora dias - santagata no relationship to disclose nicolas marcoux honoraria : bristol - myers squibb konstantinos arnaoutakis honoraria : foundation medicine , precision advisors , ariad pharmaceuticals consulting or advisory role : foundation medicine , precision advisors , ariad pharmaceuticals rebecca j . 
nagy employment : guardant health stock and other ownership interests : guardant health richard lanman employment : guardant health , veracyte leadership : guardant health stock and other ownership interests : guardant health , veracyte research funding : guardant health anthony j . 
farago honoraria : foundation medicine consulting or advisory role : pharmamar , merrimack , takeda pharmaceuticals , abbvie , intervention insights research funding : pharmamar ( inst ) , abbvie ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , loxo ( inst ) , ignyta ( inst ) travel , accommodations , expenses : pharmamar , abbvie , stemcentrx mari mino - kenudson consulting or advisory role : merrimack , h3 biomedicine , acd pharmaceuticals , roche , genentech aaron n . 
sequist honoraria : astrazeneca consulting or advisory role : astrazeneca , genentech , roche , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , pfizer ( inst ) affiliations meghan j . 
sequist lv , yang jc , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as first - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
yu ha , arcila me , rekhtman n , et al : analysis of tumor specimens at the time of acquired resistance to egfr - tki therapy in 155 patients with egfr - mutant lung cancers . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a third - generation egfr inhibitor . 
cancer discov 5 : 713 - 722 , 2015 janne pa , yang jc , kim dw , et al : azd9291 in egfr inhibitor - resistant non - small - cell lung cancer . 
schwaederle mc , patel sp , husain h , et al : utility of genomic assessment of blood - derived circulating tumor dna ( ctdna ) in patients with advanced lung adenocarcinoma . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
suda k , murakami i , sakai k , et al : small cell lung cancer transformation and t790m mutation : complimentary roles in acquired resistance to kinase inhibitors in lung cancer . 
the new era of precision medicine complicates communication even further as a result of our increasing reliance on genomic data and the varying psychological responses to genomic - based treatments and their expected outcomes . 
however , many of the communication issues are actually similar to perennial long - standing communication issues in oncology , which center on providing hope when breaking bad news and ensuring that adequate informed consent to treatments is obtained . 
we highlight these new communication issues that focus on clinical and ethical questions ( ie , informed consent , shared decision making , patient autonomy , and uncertainty in oncologic treatments ) and provide guidance on working with each scenario . 
in this article , we address common reactions of patients to genomic information and provide thoughtful communication suggestions using a shared decision making framework to help patients cope with the inherent distress - provoking uncertainties in oncology practice . introduction the practice of oncology depends on adequate communication between patients and clinicians . although the science of cancer medicine is advancing exponentially , information technology advances are seriously impeding the critical component of face - to - face communication . 
the key communication issues in oncology are always twofold : the delivery of emotionally charged bad news while sustaining hope in the presence of a lifethreatening prognosis and ensuring that patients understand the information that is provided.1 the advent of precision medicine now complicates the discussion of these issues in oncology in significant ways.2 , 3 although there is a growing emphasis on providing humanistic care in oncology ( eg , palliative care initiatives ) , the increasingly complicated science and public hype , coupled with limited time to talk with patients in busy oncology clinics , significantly threaten this goal . 
science and technology have yet again raced ahead of the human element , which depends on communication to foster those critical elements of mutual respect and trust . the application of genomic medicine is now accessible for the majority of oncology patients because the cost of genomic sequencing has decreased 1 millionfold from a decade ago.4 - 6 the development of molecular diagnostic , prognostic , and predictive biomarkers continues to change the landscape of clinical oncology.7 furthermore , technologic advances facilitate the use of largescale databases that store genomic data , such as ascos cancerlinq and ibm watson.8 - 11 also , research trial design in precision oncology is evolving from the randomized controlled trial to designs that harness these large data - collection initiatives and evaluate responses to drugs across multiple cancer subtypes ( ie , basket trial design ) .12 , 13 at the same time that genomic science and technology have created new research and clinical treatment paradigms , social media and drug direct - to - consumer marketing in the united states has brought information to the public with remarkable speed and fervor.14 , 15 although there are advantages to patients being informed consumers , handling this complex information without any interpretation of its meaning is not helpful.16 this breadth and rapidity of information adds an additional strain to the already complicated communication that occurs between clinicians and their patients.17 direct - to - consumer marketing is new and often amplifies drug benefits beyond reality . 
mcfarland , memorial sloan kettering cancer center , west harrison ; and elizabeth blackler , smita banerjee , and jimmie holland , memorial sloan kettering cancer center , new york , corresponding author : daniel c . 
 understand the implications for the overall cancer experience , eg , their satisfaction or dissatisfaction with their oncology care , or how this information influences patients treatment choices.15 its implications may be greatest when considering the delicate end - of - life conversations that are critical to quality oncology care.18 therefore , it is critical that we understand patients experiences in this new technologic age of genomic medicine . 
the shared decision making ( sdm ) model of communication promotes patient activation and engagement in health care and is an optimal model to guide communication tasks in the precision medicine era.19 , 20 the sdm model describes how clinician and patient jointly participate in making a health decision , having discussed the options and their benefits and harms , as well as having considered the patients values , preferences , and circumstances . 
it respects patient autonomy and leads to improved patient satisfaction when patients are faced with clinical options for which there is not a clearly correct choice , as is frequently encountered in the context of precision oncology.21 - 24 in this article , we highlight the psychological , social , and ethical issues that are part of our new treatments , and we provide communication suggestions on the basis of sdm . 
patients emotional reactions should be considered before , during , and after sdm to ensure effective communication . i won the lottery : the lucky biology club member jane was a 58 - year - old teacher who was diagnosed with stage iv adenocarcinoma of the lung that harbored an epidermal growth factor receptor mutation . her cancer responded well to erlotinib . 
after 15 months , her cancer began to grow as it became increasingly resistant to erlotinib , and chemotherapy was required to treat it . jane became extremely angry and frustrated that her cancer had progressed and found it hard to appreciate the benefit that the drug provided in light of its failure . she remained in shock and disbelief and had a difficult time accepting the need to adjust her treatment to the new situation . the lucky biology club members have driver actionable mutations such as epidermal growth factor receptor , anaplastic lymphoma kinase , ros1 , and brafv600e . 
subsequently , discussions about health care proxies , financial planning , and wills are often delayed . in terms of discussion , it is important to acknowledge the implications of disease biology and to corroborate and correct the information that they have from other sources . 
using sdm principles , the clinician could initiate a discussion of options by saying , there are some specific treatment options for you , on the basis of your cancers genomic make - up . 
however , the clinician must also discuss the framework for treatment and prognosis : although the cancer is still not curable , the mutation indicates that we have some additional treatment options . 
the clinician may say , given this news , it seems like a good time to talk about what to do next or we are in a different place now . 
is it okay if we talk more about the other options and next steps ? addressing the underlying emotions and acknowledging fear are important tools that should be dealt with before focusing on sdm . 
sdm can help provide clinical decision transparency and ameliorate disappointments with limited treatment effectiveness . i failed the test : the unlucky biology club member sarah was a 73 - year - old patient with newly diagnosed nonsmall - cell lung cancer who had no actionable mutation . 
at her first visit , she was clutching an article from the new york times and yelling , i want the serial killer ! she had come to memorial sloan kettering cancer center in hopes of enrolling in a clinical trial with first - line immunotherapy . when she did not meet trial entry criteria because of her pd - l1 status , she became enraged at being denied the opportunity that she had heard and read about . 
the article she held on to described how immunotherapy unleashes a so - called serial killer that ravages all cancer cells in the body , which is understandably what she wanted.29 sarah had delayed seeking cancer treatment in hopes of having the right mutation to enroll in a clinical trial . 
the unlucky biology club members feel that their tumor biology has conspired against them ; they are angered by the treatment options that are available for others but not for thethey feel that it is not fair that other patients with the same cancer are treated with more desirable targeted therapies . 
this may resonate with failures in their life before having cancer . it is crucial to validate their emotions of anger , fear , frustration , and worry by saying , i cant imagine what it has been like for you to hear this news ; i can see this is very upsetting . 
is it okay if we talk a bit more about what this means ? in this scenario , it is important to educate and reorient the patient who has been stuck on one idea as a result of their limited information . 
as part of sdm , the clinician should provide information on benefit and risk , such as , this information helps us plan the very best treatment for you . clinicians should be careful about comparing patients and especially about providing unsolicited information . this is an opportunity to re - establish / realign with the patients goals . 
given what you know about your illness , whats most important to you ? or , as you think about the future , are there situations or things that you want to make sure you accomplish or avoid ? explain that treatment options can be re - evaluated and tailored to the patients wishes . 
it also sends a positive message that although one opportunity for treatment did not work out , the team provides realistic hope and direction , despite a disappointment . a new drug has just come out : a novel treatment michael was a 47 - year - old patient with sinonasal undifferentiated carcinoma , a rare form of head and neck cancer . 
although the drug had never been tested with his specific head and neck cancer , sinonasal undifferentiated carcinoma , his clinicians believed that he had to be informed about the new treatment because he was young and otherwise healthy and , if it worked , would possibly provide a durable response . 
he did not want to complicate or disrupt the decision to accept hospice care , yet he felt ethically bound to offer a treatment for which michael had become eligible . this case highlights an ethical dilemma associated with the interface of advancing science and clinical care . 
it illustrates how the emergence of rapidly changing oncology treatments begets new levels of uncertainty in the cancer experience ( eg , no specific data for a cancer subtype , even though pembrolizumab had been approved for head and neck cancers )  . 
clinicians are taught to provide answers , which can be frustrating when new data become available and raise new questions and more uncertainty ( eg , does the drug work in this cancer subtype ? )  . 
medical training teaches clinicians how to handle uncertainty , but it does not teach them how to share its presence in a constructive way for patients.30 a full discussion was undertaken with the patient about the absence of data , the ethical reason for informing him of the new agent , and the inherent complications of considering another new treatment . 
he decided to stay with his decision to begin hospice care . it is important to discuss patients emotions about clinical uncertainty and the various treatment options , framed in the context of their current clinical situation : i realize this is all very complicated ; let me try to explain these options in the setting of your illness . 
also , it is important to frequently determine their level of understanding ( facilitates deliberation ) : can you tell me , in your words , what you understand ? also , it is helpful to review the patients clinical information together as a background to discussing the uncertainty . in situations of greatest clinical uncertainty , it is important to assure the patient that you are available for further discussion of their concerns and questions . 
a partnering statement , conveying the sense of were in this together and i will continue to work with you , is helpful to demonstrate a personal commitment to providing the best care possible despite the clinical uncertainty . 
patients who feel that they are in a partnership with their clinicians are better able to trust them and tolerate clinical uncertainty.31 i know i can beat it : the denier don was a 68 - year - old patient with progressive metastatic colon cancer who had received all conventional lines of cancer treatment . 
don said that he was the exception , frequently finding ways to explain how the negative clinical facts did not apply to hihe made many references to newly available targeted therapies that he believed could be used to treat his cancer . hope is a critical component of coping , especially in a time of great need . 
these offers are often made in the face of overwhelming disease biology . for most advanced cancers , precision oncology finds driver mutations in only a minority of cases , and the goal of most early trial design is still safety and not necessarily efficacy . 
these are difficult concepts to explain to patients who will probably only hear that there is hope . typically , educating the denier will require revisiting the topic several times to try to arrive at a shared understanding of the actual situation : you may be eligible for a trial if your cancer has a certain mutation ; however , taking the drug in this basket trial may not extend your life . 
when the patients condition worsens , the education may have to become more pointed : scans dont always reflect what is going on in terms of tumor growth and a change in functional status is an indication that the cancer is progressing . 
i hear you saying that what is most important to you is and i understand that you want to make sure to avoid the following this demonstrates that they have been heard , ensures that the goal of hope is not being taken away , and helps the patient to evaluate options . 
it is also important to keep in mind that the denier fluctuates in their level of denial and may partially accept the reality of the situation . patients often maintain two levels of awareness and acknowledgment of the situation . 
one is cognitive : i know how ill i athe other is emotional : i simply cant believe i could die . both exist simultaneously in many patients , which accounts for these day - to - day attitudinal changes . an ongoing positive clinician - patient relationship allows these feelings to emerge , and a more realistic discussion can occur about end - of - life planning , for example . 
often , a patients underlying fear will ameliorate in the context of working closely together . i have done my research : the overly or misinformed patient barbara was a 49 - year - old well - educated professional with nonsmall - cell lung cancer metastatic to brain and bone . 
barbara had strong opinions about the new treatment choices for lung cancer and was unwilling to consider therapies that were more appropriate for her type of disease . this case illustrates the complexity of precision oncology and the level of sophisticated genomic knowledge that is required to have a fully informed conversation with a patient . 
she explained the difference between inherited dna mutations , for which olaparib could be used in the presence of an inherited brca2 mutation in ovarian cancer , and the more common somatic mutations present in noninherited cancers such as her brca2 - mutated nonsmall - cell lung cancer . 
in this situation , correcting misinformation and misunderstanding is essential : there are many exciting cancer treatments , but whats important is that we find the right one for you . some patients want all available information and want to actively participate in their treatment decision . 
also , uncovering each patients major concerns is critical : what information would be most helpful for me to know about you ? then , it is important to acknowledge the patients concerns : this must be very upsetting for you . 
this acknowledges the importance of alliance.32 a request for a specific cancer treatment may be driven by an attempt to reach a goal , which may be modifiable in certain cases . 
it is crucial to demonstrate that you clearly understand their request : i hear you saying that whats most important is to continue treating your cancer to ensure you can reach your goal . case continued : a rebiopsy after progression revealed a her2 mutation that made her eligible for a basket trial . the oncologist invited another discussion of her tumor dna mutations and informed her that a newly found her2 mutation would qualify her for a basket trial . 
the previous genomics discussion on inherited and somatic mutations helped her understand that she would be treated with a group of patients with different cancers , who would all have the same somatic tumor dna mutation , to assess safety and perhaps efficacy in accordance with the trial objectives . she understood alternative treatment options and was offered a decision delay to facilitate deliberation and decision making . 
so far , the literature remains limited.7 , 33 , 34 patients acknowledge the promise of precision medicine but also consistently raise concerns about the discovery of incidental findings , information overload , complications from additional biopsies with delay in definitive cancer treatment , and the lack of a clear benefit.35 the risk of ineffective communication is that patients misunderstand the nature and seriousness of their diseases , which may lead to more aggressive and futile cancer treatments at the end of life or to increased fear and anxiety , while increasing stress and burnout in members of the medical team.36 on the other hand , effective communication enhances shared decision making , decreases patient distress , and increases patient satisfaction and trust in the medical team.25 shared decision making is the communication style that is preferred by most patients.37 patients make choices that are guided by the clinicians information and recommendations . 
patients may also have preferences on a spectrum of communication styles that can range from paternalistic ( ie , the patient is a passive recipient of their care ) to the clinician who is a nondirective information provider or educator ( ie , the patient is given choices and decides on management according to his / her preferences ) .30 it can be helpful to simply ask how the patient and family would like to make decisions , and the clinician can discuss this spectrum to gain clarification . 
discussing therapeutic uncertainty is often a difficult task for clinicians and leads to clinician behaviors of not disclosing all of the information , not talking about it , or oversimplifying the information.30 understandably , this can leave patients with a distorted account of their clinical situation . 
they may make sense of the situation by prescribing to alternative introducing so - called explanations or hopes , extramedical values , or seeking other remedies ( eg , alternative treatments ) when presented with clinical uncertainty.30 the idea of effective disclosure has been proposed as a potential goal in discussing uncertainty with patients . 
this idea supposes that patients can tolerate a certain amount of uncertainty and that extra vigilance is required by the clinician to ensure that they are given the tools and information they need to engage in decision making.30 effectively , extra care is taken in those situations of greater uncertainty to provide information and to ensure that the patient understands . 
this protects autonomy and increases patient trust in the long run . also , addressing underlying emotions , hopes , and fears is an effective way to ensure good communication and informed consent . 
a conversation analysis found that patients who are more assertive draw more empathy from their oncologists , whereas passive patients elicited much less emotional reciprocation from the oncologists.39 clinicians may use open - ended questions , such as , id like to switch gears and check in to see how you are feeling about all of this technical information ? or more closed - ended questions , such as , many patients may feel overwhelmed by all of the scientific information weve discussed ; im wondering if that is true for you ? in addition , checking understanding and emotional reactions enhances the clinician - patient relationship and is key in the setting of uncertainty . directly focusing on the therapeutic aspects of the relationshipby assessing communication preference , checking understanding , and searching for underlying emotional issuesdevelops rapport and may bolster patients resilience in the face of clinical uncertainty . 
the clinician may say something such as : im wondering if there is anything that might be difficult for you to discuss with me ? is there anything that i might be able to do to make this better for you ? or i have a sense that you are someone who likes x , y , and z ; please help me understand if i am correct . 
realigning goals may be accomplished by saying something such as : it is my goal to provide you with the best information for us to make a decision that works for you ; please let me know if that is also your goal or if youd like to focus on additional issues . this human connection dimension of medical care is needed to withstand the uncertainty . 
clinicians frequently underestimate the therapeutic power of their relationships with patients.40 a strong therapeutic bond is fundamental , not simply useful.41 patients have varying abilities to trust , hope , and have faith in their clinicians . 
the relationship is strengthened by focusing on agreed - upon common goals and tasks.32 it is always appropriate to discuss the nuts and bolts of the therapeutic relationship , especially when the clinician perceives that it may not be firmly established or upon entering areas of clinical uncertainty that are inherent in the precision medicine era . summary precision medicine presents a new era of communication in oncology . 
this article has presented some of the common patient reactions to precision medicine and basic communication issues in oncology . communication can be used to enhance rapport , trust , and support . 
zachariae r , pedersen cg , jensen ab , et al : association of perceived physician communication style with patient satisfaction , distress , cancer - related self - efficacy , and perceived control over the disease . 
blanchette ps , spreafico a , miller fa , et al : genomic testing in cancer : patient knowledge , attitudes , and expectations . cancer 120 : 3066 - 3073 , 2014 35 . 
politi mc , studts jl , hayslip jw : shared decision making in oncology practice : what do oncologists need to know ? oncologist 17 : 91 - 100 , 2012 38 . 
kenny da , veldhuijzen w , weijden tv , et al : interpersonal perception in the context of doctor - patient relationships : a dyadic analysis of doctor - patient communication . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction as our knowledge of hereditary cancer risk has testing of cancer preevolved , multigene panel disposition genes has become an important component of patient care . 
the national comprehensive cancer network provides gene - specic recommendations for changes in medical management on the basis of the identication of pathogenic variants.1 to this end , accurate and denitive variant classication is a critical component of clinical genetic testing . 
the american college of medical genetics and genomics ( acmg ) and the association for molecular pathology ( amp ) provide guidelines for clinical variant classication2 ; however , there is often insufcient evidence to support a denitive classication of pathogenic or benign when a variant is rst detected . 
as a result , testing laboratories may vary in their clinical terpretation of acmg / amp guidelines for hereditary cancer genetic testing and , ultimately , in their variant classications.3 - 6 with the increased use of multigene panels , number of variants of uncertain signicance ( vuss ) detected has also increased.7 , 8 in addition to a larger number of genes , many cancer predisposition genes have been more recently incorporated into clinical testing , and there is less evidence available to support variant classication . 
 evolution of cancer gene variant reclassication context key objective with the increasing use of hereditary cancer genetic testing and introduction of multigene panels , robust and accurate methods for variant re / classication of cancer predisposition genes are of utmost importance . 
laboratory - developed methods were the most common lines of evidence used in variant reclassication , with pheno analysis ( a clinical history weighting algorithm ) being used in approximately 40% of cases . relevance many tools traditionally used for variant re / classication are not informative for rare variants ; however , rare variants collectively affect millions of patients . 
this was followed by testing for lynch syndrome ( mlh1 , msh2 , msh6 , and pms2 ) and melanoma - pancreatic cancer syndrome ( cdkn2a ) in 2002 and for familial adenomatous polyposis ( fap ) / attenuated fap / mutyh - associated polyposis ( apc and mutyh ) in 2003 . 
in 2013 , a hereditary cancer multigene panel was introduced , which was analytically validated and described in detail previously.9 the panel included 25 genes : apc , atm , bard1 , bmpr1a , brca1 , brca2 , brip1 , cdh1 , cdk4 , cdkn2a ( p16ink4a and p14arf ) , chek2 , epcam , mlh1 , msh2 , msh6 , mutyh , nbn , palb2 , pms2 , pten , rad51c , rad51d , smad4 , stk11 , and tp53 . 
individuals who had single - site or founder mutation testing were reclassication program the reclassication program used by this testing laboratory included a multidisciplinary committee of laboratory directors , genetic counselors , phd - level scientists , and supporting variant specialists . 
variant classication and reclassication followed a stringent , welldocumented protocol as previously described.13 on the basis of acmg / amp guidelines , variants were classied into ve categories of increasing clinical severity : benign ( b ) , likely benign ( lb ) , vus , likely pathogenic ( lp ) , and pathogenic ( p ) .2 , 14 , 15 automated processes proactively monitored and gathered all available evidence to expedite reclassication . 
multiple classication tools could have been used to evaluate the pathogenicity of a variant at the time of original classication and / or if a variant was reclassied , an reclassication ( fig 1 )  . amended report was sent to health care providers for all patients who were carriers of the variant . 
 esterling et al pheno ( n = 56 , 596 ) clinical history weighting algorithm to assess phenotype severity for variant carriers v carriers of pathogenic and benign variants pt / ha ( n = 36 , 314 ) phase testing or haplotype analysis for genes associated with embryonic lethality or severe clinical phenotypes because of homozygosity or compound heterozygosity homozygosity confirmed continuous evidence evaluation threshold reached population frequency ( n = 17 , 664 ) threshold reached allele frequency from exac and gnomad functional or clinical evidence literature ( n = 4 , 509 ) expert review of automated search results and curated repository structure disrupted structural analysis ( n = 850 ) using validated protein structures mco ( n = 12 , 753 ) likelihood of co - occuring pathogenic variants in the same gene or in genes associated with the same hereditary cancer syndrome threshold reached cosegregation in multiple families segregation analysis ( n = 8 , 255 ) published pedigrees and provider communications rna analysis ( n = 610 ) in - house comprehensive rna analysis to directly assess rna splicing effects splicing disrupted splicing analysis ( n = 3 , 148 ) functional data and expert review other ( n = 4 , 598 ) knowledge of similar variants , species conservation in conjunction with structural analysis , additional statistical analysis , and classification / reclassification protocol refinements evidence queuing for review based on variant type and new evidence multiple expert reviews evidence insufficient wait for additional evidence committee discussion variant reclassified amended reports fig 1 . 
phase testing / homozygosity analysis ( pt / ha ) was only applied to genes associated with autosomal dominant cancer risks that may also be associated with embryonic lethality or severe clinical phenotypes in individuals carrying pathogenic variants in the affected gene on different parental chromosomes as a result of either homozygosity or compound heterozygosity . 
common single nucleotide polymorphisms ( snps ) observed in the patient population were used to develop gene - specic haplotypes , which were automatically assigned to determine the variants phase ( ie , in cis or in trans ) , whenever possible . 
mutation co - occurrence ( mco ) analysis was based on an assumption of a low likelihood that an individual will carry two autosomal dominant pathogenic variants that cause an increased risk for the same or a similar cancers.18 mco analysis measured the statistical signicance of a variant co - occurring multiple times with one or more pathogenic variants in the same patient ( in the same gene or in a different gene for the same syndrome )  . 
99.5%. rna splicing analysis and protein structural analysis . assessment of in silico rna splicing predictions was used to initially evaluate the potential effects of a variant on rna splicing.19 published reports of biochemical splicing analysis , which used high - quality data and appropriate controls , were considered for variant classication . 
in some cases where evidence was unavailable or of insufcient quality or detail to be conclusive , quantitative rna splicing analyses were performed in house , using informative snps , to assess potential rna splicing effects resulting from the variant of interest.20 expert protein structural analysis was also used to assess the impact of variants predicted to affect protein structure at the amino acid level . 
cascade testing is the systematic identification of relatives who are at risk for having the same mutation ( at - risk relatives ) and facilitating genetic testing for the usually , these individuals are unaffected , but they may benefit from early identification and risk management interventions . 
 currently , australian best practice guidelines recommend that genetic testing for unaffected individuals be facilitated by an appropriately trained health professional such as a genetic counselor or clinical geneticist.15 the purpose of this case report is to exemplify a collaboration between the departments of oncology and genetics to extend testing for a dpyd mutation to family members after the index case was identified . patient the index patient was diagnosed with metastatic breast cancer at age 59 years . 
 she developed locoregional recurrences in 2011 , bony metastases in 2013 , and further progression with liver , lung , bone , and soft tissue metastases in 2016 after multiple lines of endocrine therapy . 
with normal baseline renal function , she was prescribed capecitabine at 1 , 000 mg / m2 twice per day on days 1 to 14 in a 21 - day cycle . 
four weeks later , she began palliative paclitaxel to treat symptomatic cancer progression . the patients oncology team referred her to the department of genomic medicine at the royal melbourne hospital . 
the patients personal and family history of cancer had been assessed ; it was considered that there was no increased familial risk of breast ( or other ) cancers . the patients first - degree relatives were subsequently offered genetic counseling and testing for this pharmacogenomic mutation . 
communication of genetic results in families is known to be problematic for various reasons , including miscommunication or misunderstanding of genetic information and passive or active nondisclosure.20 - 22 in this case , family members were already in contact with the genetics service around the time of the index testing and were requesting testing themselves . 
a hypothetical pedigree showing the effect of systematic cascade testing for an autosomal dominant condition . to our knowledge , this is the only published case report of cascade genetic testing in the setting of dpyd pharmacogenomics . 
falvella and colleagues23 reported a case of dpyd genotyping before starting chemotherapy in a 38 - year - old man with colorectal cancer in the context of his mother having a known dpyd variant . 
our case differs in that we extended the dpyd genotyping systematically by offering it to all unaffected at - risk family members . fluoropyrimidines are commonly used drugs , and the cancers treated with these drugs are common in the general population . 
even though this family is not at an increased heritable risk of cancers , it is quite possible that members of the family may need this treatment regimen in the future . 
relationships are self - held unless noted . hereditary breast and ovarian cancer syndrome , cascade pharmacogenomics testing would be predicted to have greater utility because of the higher probability of relatives being affected by these cancers . in conclusion , this case provides an example of cascade testing of family members after an individual with dpd deficiency was identified . 
winship , university of melbourne , parkville , australia acknowledgment we acknowledge michael michael , md , consultant medical oncologist at peter maccallum cancer centre , for his input into an earlier version of this manuscript . support supported by a victorian state - funded clinical service . 
iacovelli r , pietrantonio f , palazzo a , et al : incidence and relative risk of grade 3 and 4 diarrhoea in patients treated with capecitabine or 5 - fluorouracil : a meta - analysis of published trials . 
meulendijks d , van hasselt jgc , huitema adr , et al : renal function , body surface area , and age are associated with risk of early - onset fluoropyrimidine - associated toxicity in patients treated with capecitabine - based anticancer regimens in daily clinical care . 
ison g , beaver ja , mcguinn wd jr , et al : fda approval : uridine triacetate for the treatment of patients following fluorouracil or capecitabine overdose or exhibiting early - onset severe toxicities following administration of these drugs . 
ma ww , saif mw , el - rayes bf , et al : emergency use of uridine triacetate for the prevention and treatment of life - threatening 5 - fluorouracil and capecitabine toxicity . 
henricks lm , opdam fl , beijnen jh , et al : dpyd genotype - guided dose individualization to improve patient safety of fluoropyrimidine therapy : call for a drug label update . 
lunenburg catc , henricks lm , guchelaar hj , et al : prospective dpyd genotyping to reduce the risk of fluoropyrimidine - induced severe toxicity : ready for prime time . 
liu d , li j , gao j , et al : examination of multiple ugt1a and dpyd polymorphisms has limited ability to predict the toxicity and efficacy of metastatic colorectal cancer treated with irinotecan - based chemotherapy : a retrospective analysis . 
claes e , evers - kiebooms g , boogaerts a , et al : communication with close and distant relatives in the context of genetic testing for hereditary breast and ovarian cancer in cancer patients . 
mcclaren bj , aitken m , massie j , et al : cascade carrier testing after a child is diagnosed with cystic fibrosis through newborn screening : investigating why most relatives do not have testing . 
their study is large and includes nearly 27 , 000 patients who underwent multigene panel testing ( including cdh1 ) over a 2 - year period at ambry genetics , an established commercial diagnostic laboratory , and  . 
these cases are divided into patients with igclcpartial phenotype , who exhibit some hint of hdgc in their family , such as individuals with gastric cancer , lobular breast cancer at older ages , or even lobular carcinoma in situ ; and patients who are igclcnegative , who have no evidence of gastric cancer or lobular breast cancer in their family . using this nomenclature , one - quarter of both the laboratoryand clinic - based cdh1 carriers were igclc - negative ( although the results from the laboratory - based group must be considered preliminary , because the patients family histories were obtained from the ordering form rather than through genetic counselorderived pedigrees )  . 
thus , we cannot speculate on their potential risk for early gastric cancer , despite their lack of a suggestive family history . however , three of the 10 patients with igclc partial phenotype underwent prophylactic gastrectomy procedures , and all had early gastric cancer ( one patient as young as 39 years )  . 
although this article does not fully answer what to do for the patient who was the subject of our friday afternoon genetics clinic , it does provide important insights into how to approach these difficult decisions and what additional information we need to do so with greater confidence . certainly , those cdh1 mutation carriers with any personal or family history of gastric or lobular breast cancer , even if they do not meet igclc criteria for hdgc , should at least consider a prophylactic gastrectomy . 
however , for those individuals who are truly igclcnegative after a comprehensive family history is taken by a skilled genetic counselor , it is difficult to recommend such an invasive procedure . 
both groups should definitely have regular endoscopic screening with blind biopsies , and proceed to gastrectomy if any malignant cells are identified.4 finally , all of these recommendations go out the window if and when a case of a true igclcnegative cdh1 carrier develops gastric cancer or has a prophylactic gastrectomy that identifies early gastric cancer . 
van der post rs , vogelaar ip , carneiro f , et al : hereditary diffuse gastric cancer : updated clinical guidelines with an emphasis on germline cdh1 mutation carriers . 
raymond , ms3 ; eduardo vilar , md , phd1 ; michael overman , md1 ; bryan kee , md1 ; cathy eng , md1 ; kanwal raghav , md1 ; and scott kopetz , md , phd1 purpose atypical , non - v600 braf ( abraf ) mutations represent a rare molecular subtype of metastatic colorectal cancer ( mcrc )  . 
preclinical data are used to categorize abraf mutations into class ii ( intermediate to high levels of kinase activity , ras independent ) and iii ( low kinase activity level , ras dependent )  . 
among patients with abraf ras wild - type mcrc who received anti - egfr antibodies ( monotherapy , n = 1 ; combination therapy , n = 10 ) , no responses to anti - egfr therapy were reported , and six patients ( four with class iii abraf mutations , one with class ii , and one unclassied ) achieved stable disease as best response . 
in the ctdna cohort , there was an increased prevalence of abraf mutations and subclonal abraf mutations ( p , .001 for both ) among predicted anti - egfr exposed compared with nonexposed patients . conclusion efcacy of anti - egfr therapy is limited in class ii and iii abraf mcrc . 
2019 by american society of clinical oncology introduction brafv600e missense mutations are present in 6% to 10% of patients with metastatic colorectal cancer ( mcrc ) .1 , 2 within the braf kinase domain , substitution of a valine to glutamic acid at position 600 manifests as constitutive activation and oncogenic signaling along the mitogenactivated protein kinase ( mapk ) pathway.1 brafv600e mcrc represents an aggressive molecular subtype of colorectal cancer inherently refractory to standard chemotherapy ; thus , tremendous research focus has been directed toward novel therapeutic development.2 because of increased use of next - generation sequencing ( ngs ) in the management of mcrc , various mutational hotspots of clinical signicance have emerged within interest , such as expanded ras testing . genes of however , with such broad testing including circulating tumor dna ( ctdna ) , alterations of evolving signicance without clear predictive , prognostic , or therapeutic implications have also been identied . 
atypical , non - v600 braf ( abraf ) mutations that occur outside of codon 600 are one example of an emerging molecular subtype in colorectal cancer . abraf mutations were retrospectively studied at two large centers comprehensively describing the clinical , pathologic , and survival implications of these mutations in patients with mcrc.3 a total of 9 , 643 patients with mcrc underwent ngs testing and 208 patients with abraf mutations were identied , representing 2.2% of all patients tested . 
 johnson et al context key objective to determine if atypical , non - v600 braf ( abraf ) mutations , stratied by class , affect outcomes with anti - egfr therapy and , secondarily , if acquisition of abraf mutations imparts resistance to egfr inhibition . knowledge generated clinical outcomes on the basis of functional class and their effect on anti - egfr efcacy for abraf metastatic colorectal cancer ( mcrc ) have not been dened . 
in patients with abraf wild - type ras mcrc who received anti - egfr antibodies , there were no responses among class ii or iii abraf mcrc , with stable disease as best response in our internal cohort . evaluation of a large external cohort of patients with circulating tumor dna interrogated by an anti - egfr exposure score revealed increased prevalence of abraf and subclonal abraf mutations among predicted anti - egfr exposed compared with nonexposed patients , suggesting an acquired mechanism of resistance to egfr inhibition . relevance anti - egfr therapy is limited in abraf mcrc , with class ii abraf mutations emerging as a negative predictive biomarker . detection of abraf mutations in ctdna may represent a novel mechanism of resistance warranting additional investigation . can be used sequentially throughout the course of the disease . although brafv600e mcrc is known to be predictive of poor response to anti - egfr therapy , the clinical utility of egfr inhibition in abraf mcrc remains unclear.4 , 5 of note , previous retrospective work investigating a cohort of 150 patients with refractory mcrc identied seven patients with abraf mutations and reported poor progression - free survival when they were exposed to anti - egfr therapy in comparison with a cohort with ras / raf wild - type ( ras / rafwt ) mcrc.6 preclinical work has highlighted unique biology among traditional brafv600e mutations ( class i ) and abraf mutations ( classes ii and iii ) .7 , 8 brafv600e mutations , designated as class i , result in feedback inhibition of gtp - bound ras , are ras independent , and signal as active monomers . 
in contrast , class ii abraf mutations have intermediate to high levels of kinase activity , are ras independent , signal as constitutive dimers , and are resistant to vemurafenib , whereas class iii abraf mutations have low or absent kinase activity and are primarily ras dependent and sensitive to erk - dependent feedback of ras.7 , 8 these tumors bind more tightly to ras - gtp than do wild - type braf tumors , and binding to wild - type craf is enhanced , resulting in increased erk signaling.8 these stark differences in underlying tumor biology may explain the varying response to therapy , specically the potential limitations to anti - egfr inhibition in abraf mcrc . 
cohort 1 included patients with stage iv colorectal cancer who were seen at mdacc between march 1 , 2012 , and june 27 , 2017 , and underwent targeted exome sequencing . 
all clinical and outcomes data were derived from this cohort . cohort 2 included patients with mcrc who underwent a targeted ngs ctdna assay ( guardant360 ; guardant health , redwood city , ca ) as part of their care between june 1 , 2014 , and december 26 , 2017 , at multiple institutions . 
 abraf mutations as a mechanism of resistance to egfr inhibition frequencies for both cohorts of abraf mutations : predicted anti - egfr exposed and nonexposed . statistical analysis clinicopathologic features were compared by 2 test or fishers exact test for categorical variables and assessment of odds ratios for associations as appropriate , as well as by t test to compare continuous variables . 
matched analysis adjusted by age and sidedness was undertaken to compare os among all molecular classes . 2 or fishers exact tests , as well as t test , were used to evaluate the adequacy of the matching . 
statistical analyses were performed using graphpad prism , version 6.07 ( graphpad software , la jolla , ca ) , and spss , version 23.0 ( ibm , armonk , ny )  . 
among 36 patients with abraf mcrc , 19 ( 53% ) had left - sided primary tumors and 24 ( 67% ) had microsatellite stable ( mss ) disease and were a median age of 56 years ( table 1 )  . 
of note , in contrast to brafv600e mcrc , which is mutually exclusive with ras mutations , 12 patients with abraf mcrc had ras mutations ( class iii , n = 7 of 21 [ 33% ] ; class ii , n = 5 of 10 [ 50% ] )  . 
among these , one patient with class ii abraf mcrc also had microsatellite instabilityhigh ( msi - h ) disease . for a more accurate comparison of survival outcomes among respective molecular classes , we performed a matched analysis by age and sidedness among the 36 patients with abraf mcrc compared with 36 patients with brafv600e mcrc and 36 with ras / rafwt disease ( fig 3 ; appendix table a1 )  . 
 ( % ) unless otherwise indicated . abbreviations : , not applicable ; abraf , atypical , non - v600 braf ; msi - h , microsatellite instabilityhigh ; mss , microsatellite stable ; wt , wild exposed to anti - egfr therapy in their treatment course . among patients with abraf raswt mcrc , 11 ( 50% ) received anti - egfr monoclonal antibodies ( mabs ; monotherapy , n = 1 , combination therapy , n = 10 ; class iii , n = 7 of 14 [ 50% ] , class ii , n = 3 of 5 [ 60% ] , unclassied , n = 1 )  . there were no responses reported , and six patients ( class iii , n = 4 ; class ii , n = 1 ; unclassied , n = 1 ) achieved stable abraf ( n = 36 ) brafv600e ( n = 221 ) wild - type braf ( n = 438 ) time ( months ) fig 2 . 
in line with previous reports , patients with class i or brafv600e mcrc had worse survival outcomes when exposed to egfr inhibition ( fig 4 )  . abraf mutations as a potential mechanism of resistance to anti - egfr therapy to understand our institutional ndings of limited efcacy of anti - egfr therapy in abraf mcrc , we analyzed an external ctdna cohort of 5 , 257 samples ( cohort 2 ) from 4 , 465 patients with mcrc . 
 abraf mutations as a mechanism of resistance to egfr inhibition abraf ( n = 36 ) brafv600e ( n = 36 ) wild - type braf ( n = 36 ) time ( months ) fig 3 . 
abraf , atypical , nonv600 braf . cohort , after excluding ras and brafv600e mutations , we applied a previously validated anti - egfr exposure score to divide patients into predicted prior exposure to anti - egfr ( n = 644 ) versus predicted nonexposed ( n = 2 , 880 ) .10 this revealed that the prevalence of abraf mutations increased from 3.99% among patients predicted to have no prior antiegfr exposure to 8.38% among those with predicted antiegfr exposure ( p , .001 ; fig 5a )  . as a sensitivity analysis , we evaluated the prevalence of abraf mutations among patients with egfr ectodomain mutations , compared with those without , because egfr ectodomain mutations are unequivocally present only after exposure to egfr inhibition . 
class ii activating g469a mutations ( p , .001 ) and class iii d594n ( p , .001 ) were the most common alterations among patients with predicted antiegfr exposure ( fig 5c )  . 
agents such as vemurafenib are not active , because the drug is designed to target the shape of the v600e - mutated protein and is more than 10 - fold less active against nonmutated forms . 
 ( a ) ctdna prevalence of abraf ( 3.99% ) among non - exposed patients ( n = 2 , 880 ) v ctdna prevalence of abraf ( 8.38% ) among predicted anti - egfr exposed ( n = 644 )  . 
schematic gure of the conserved region3 ( cr3 ) of the braf protein , also known as the braf kinase domain ( amino acids 457 to 717 ) , and the location of the class ii and iii hotspot mutations . 
the kinase domain contains the p - loop ( amino acids 464 - 471 ) , the c helix ( amino acids 492 - 504 ) , the dimerization interface ( dif , amino acids 504 - 511 ) , the catalytic loop ( cl , amino acids 574 - 581 ) , the dfg motif ( amino acids 594 - 596 ) , and the activation segment ( as , amino acids 594 - 623 )  . 
class ii , activating g469a mutations ( p , .001 ) and class iii , d594n ( p , .001 ) were the most common , respectively , among predicted anti - egfr exposed patients . 
although previous reports have suggested class iii abraf mcrc may achieve responses with antiegfr therapy owing to ras dependency , our cohort , albeit small , only revealed stable disease as best response.6 , 8 , 12 - 15 , 19 these results support the ndings of the breac study , which revealed no responses in six patients with abraf mcrc ( n = 2 each with class ii , class iii , and unclassied ) .6 of note , the nding of concomitant ras mutations with abraf mcrc in tissue , conrmed in our external ctdna cohort , clearly precludes the use of egfr inhibition for all patients , highlighting the need for novel combination strategies that consider this distinct signaling biology.20 , 21 in our internal and external cohorts , we did not nd a difference between patients with class ii and class iii abraf mcrc in regard to the presence of concurrent ras mutations . 
 abraf mutations as a mechanism of resistance to egfr inhibition in our mdacc internal cohort , four patients had unclassied disease ( y656d , a415v , k752r , f109i ) and had poor survival outcomes . 
in the external ctdna cohort , we found numerous unclassied abraf mutations that are yet to be functionally described ; most were commonly comutated with ras , pik3ca , and egfr . development of acquired ras and subclonal egfr ectodomain mutations are known mechanisms of resistance to anti - egfr therapy in raswt mcrc.22 - 26 considering the limitation of egfr inhibition noted in our internal cohort , the emergence of abraf potentially reects whether a novel mechanism of acquired resistance to egfr inhibition was investigated . 
analysis of our ctdna cohort showed statistically signicant increases in the prevalence of abraf mutations , subclonal abraf mutations , and multiple abraf mutations in individual ctdna samples among patients predicted to be exposed to egfr inhibition versus those predicted to be nonexposed . 
it is important to note that the rate of abraf mutation in our ctdna cohort was higher than in our internal cohort , as well as higher than what has been published in tissue - based testing.3 these ndings highlight the potential of abraf mutations as a novel acquired resistance mechanism to egfr inhibition and warrant additional prospective investigation . of note , in patients with egfr - mutant nonsmall - cell lung cancer , abraf mutations have been reported as a mechanism of acquired resistance to egfr tyrosine kinase inhibition.27 our results underscore the need for innovative combinatorial targeted approaches for abraf mutations exploiting class biology . 
data suggest that downstream signaling with novel inhibitors of mek or erk may be useful , because the pathway is still active.20 furthermore , because both class ii and class iii mutations signal through braf and / or craf target didimers , next - generation raf inhibitors that merization is of interest in combination with these agents as a rationale next step for therapeutic intervention.21 of note , regimen using safety lead - in data for a novel triplet encorafenib , binimetinib , and cetuximab for refractory brafv600e mcrc have been published showing impressive response rates and signicant in survival outcomes.28 subsequent studies will need to investigate whether this novel triplet combination strategy can also enhance optimal mapk inhibition and provide durable benet in patients with abraf mcrc . improvement there are limitations to this study . 
second , considering the rarity of abraf mcrc , we were only able to identify 36 patients in our internal cohort , of whom 30% received egfr inhibition therapy . third , detailed clinical annotation is not available for the external ctdna cohort , and we were unable to conrm that these patients had received prior anti - egfr therapy . therefore , we applied a previously validated and published anti - egfr exposure score to identify patients predicted to have anti - egfr exposure versus patients predicted to be nonexposed to conduct our ctdna analysis . our results suggest selection criteria for the use of antiegfr therapy in abraf - mutated mcrc should be based not only on raswt status but also the functional class of the atypical variant . 
in our cohort , although limited by sample size , ndings continue to generate more hypotheses in that class ii abraf mutations may represent a negative predictive biomarker of egfr inhibition , and exposure to anti - egfr mabs may adversely affect survival outcomes , whereas efcacy of egfr inhibition was limited in patients with class iii abraf mcrc . 
increased subclonal abraf mutations and prevalence of class ii and class iii variants in ctdna among patients with predicted anti - egfr exposure suggest a novel mechanism of resistance warranting additional prospective investigation . also , our data support the clinical utility of comprehensive genomic proling ( both tissue and ctdna ) in the management of advanced mcrc , because standard hotspot polymerase chain reaction testing would not capture emerging clinically signicant alterations . 
loree , kanwal raghav , scott kopetz provision of study material or patients : all authors collection and assembly of data : all authors data analysis and interpretation : benny johnson , alexandre a . 
morris v , overman mj , jiang zq , et al : progression - free survival remains poor over sequential lines of systemic therapy in patients with braf - mutated colorectal cancer . 
clin colorectal cancer 13 : 164 - 171 , 2014 jones jc , renfro la , al - shamsi ho , et al : non - v600 braf mutations dene a clinically distinct molecular subtype of metastatic colorectal cancer . 
j clin oncol 35 : 2624 - 2630 , 2017 douillard jy , oliner ks , siena s , et al : panitumumab - folfox4 treatment and ras mutations in colorectal cancer . 
n engl j med 369 : 1023 - 1034 , 2013 pietrantonio f , petrelli f , coinu a , et al : predictive role of braf mutations in patients with advanced colorectal cancer receiving cetuximab and panitumumab : a meta - analysis . 
eur j cancer 51 : 587 - 594 , 2015 shinozaki e , yoshino t , yamazaki k , et al : clinical signicance of braf non - v600e mutations on the therapeutic effects of anti - egfr monoclonal antibody treatment in patients with pretreated metastatic colorectal cancer : the biomarker research for anti - egfr monoclonal antibodies by comprehensive cancer genomics ( breac ) study . 
br j cancer 117 : 1450 - 1458 , 2017 yao z , torres nm , tao a , et al : braf mutants evade erk - dependent feedback by different mechanisms that determine their sensitivity to pharmacologic inhibition . 
cancer cell 28 : 370 - 383 , 2015 yao z , yaeger r , rodrik - outmezguine vs , et al : tumours with class 3 braf mutants are sensitive to the inhibition of activated ras . 
nature 548 : 234 - 238 , 2017 strickler jh , loree jm , ahronian lg , et al : genomic landscape of cell - free dna in patients with colorectal cancer . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
parseghian cm , loree jm , morris vk , et al : anti - egfr resistant clones decay exponentially after progression : implications for anti - egfr re - challenge . 
cremolini c , di bartolomeo m , amatu a , et al : braf codons 594 and 596 mutations identify a new molecular subtype of metastatic colorectal cancer at favorable prognosis . 
sullivan rj , infante jr , janku f , et al : first - in - class erk1 / 2 inhibitor ulixertinib ( bvd - 523 ) in patients with mapk mutant advanced solid tumors : results of a phase i dose - escalation and expansion study . 
rankin a , klempner sj , erlich r , et al : broad detection of alterations predicted to confer lack of benet from egfr antibodies or sensitivity to targeted therapy in 19 . 
schirripa m , biason p , cortiula f , et al : clinico - pathological and molecular characterization of braf mutant metastatic colorectal cancer ( mcrc ) : are all advanced colorectal cancer . 
yu ha , suzawa k , jordan e , et al : concurrent alterations in egfr - mutant lung cancers associated with resistance to egfr kinase inhibitors and characterization of mtor as a mediator of resistance . 
distribution of abraf ( atypical , non - v600 braf ) mutations in cohort 1 ( n = 36 )  . abraf mutation class appendix johnson et al table a1 . 
 distinct dicer1 hotspot mutations identify bilateral tumors as separate events introduction dicer1 syndrome1 predisposes to a variety of cancers , including pleuropulmonary blastoma ( ppb ) , 2 ovarian sertoli - leydig cell tumor ( slct ) , 3 embryonal rhabdomyosarcoma , 4 and kidney tumors.5 - 8 in dicer1 syndrome , most patients bear a germline null mutation in dicer1 , and the tumors uniformly bear a second - hit missense substitution at one of five hotspot positions ( 1705e , 1709d , 1809g , 1810d , and 1813e )  . a wide range of clinical phenotypes can be seen in dicer1 syndrome5 , 9 ; some patients are asymptomatic , whereas others develop multiple tumors . 
in the classic cases , patients with a germline null mutation develop different somatic hotspot mutations in each tumor.7 , 10 - 16 however , in some patients , multiple tumors arise from germline mosaicism of the hotspot mutation , with subsequent somatic loss of the wild - type allele.17 - 19 here we report a patient with dicer1 syndrome who developed four tumor types at six anatomic sites over the course of 12 years . 
because we found no other mutations to explain her particularly severe clinical course , we speculate that her subsequent tumors were a product of the intense chemotherapy and radiation regimens she received . methods informed consent was obtained from the patient and her guardian before collection of tumor specimens . 
when needed , pcr products were subcloned into pcr2.1topo ( thermo - fisher scientific , waltham , ma ) before sequencing . for tp53 sequencing , coding regions were amplified using the accel - amplicon comprehensive tp53 panel ( swift biosciences , ann arbor , mi )  . 
reads were trimmed using trimmomatic21 in the galaxy project and were aligned to human genome grch38 using bwa - mem22 ; 88% mapped to the tp53 locus , producing a mean depth of 13 , 367x in targeted regions . 
variants were called using the freebayes algorithm v0.9.20 using frequency - based pooled calling instead of simple diploid calling , which allowed the algorithm to detect subclonal mutations.23 results clinical presentation the patient ( cmcw11 ) presented originally at 5 years of age with a left kidney mass . 
she was treated with 10 months of combination chemotherapy ( vincristine , doxorubicin , cyclophosphamide , irinotecan , and etoposide ) targeted at both anaplastic wilms tumor and sarcoma , together with 2 , 100 cgy whole - abdomen irradiation given in 14 fractions over 19 days . when the patient was 10 years old , a new mass arose in her remaining kidney , with a histology similar to her prior tumor , and she was diagnosed with relapsed wilms tumor ( fig 1b )  . 
 on completion , she underwent right radical nephrectomy and started hemodialysis . this patients kidney tumors were diagnosed initially as wilms tumor , but in retrospect their unique histologic features are more consistent with anaplastic sarcoma of the kidney . 
this entity was first described in 2007 , after our patients kidney tumor first arose.24 biallelic dicer1 mutations have been seen in both wilms tumor and anaplastic sarcoma of the kidney , which may represent neoplastic degeneration from cystic nephroma.6 - 8 at 12 years of age , the patient developed multiple nodules throughout her thyroid . 
thyroidectomy revealed follicular adenomas ( fig 1c )  . at 13 years of age , a mass arising from her bladder was diagnosed as embryonal rhabdomyosarcoma with focal cartilaginous differentiation ( fig 1d )  . 
sanger sequencing chromatograms demonstrating the patients ( a ) dicer1 germline frameshift mutation and ( b ) rnase iiib hotspot mutations in her ovarian sertoli - leydig cell tumors ( slcts ) ; ( c ) left ( l ) kidney tumor ; and ( d ) right ( r ) kidney tumor . 
since that time , she has been observed for > 2 years , with no further disease . dicer1 mutations we performed whole - exome sequencing on the patients first kidney tumor and germline dna as table 1 . 
her tumor bore an additional somatic hotspot mutation ( c.5425g > a ; p.g1809r ; fig 2 and table 1 )  . we then sequenced the rnase iii domains of dicer1 in archival specimens from her other tumors . 
to sequence strands separately , we subcloned the pcr amplicon spanning this mutation and found that both single - nucleotide variants occurred on the same strand , making the tumor heterozygous for a single somatic hotspot mutation ( appendix fig a1 )  . 
contrary to our clinical suspicion at the time , her contralateral kidney tumor was , in fact , a second primary . we also sequenced dicer1 from her thyroid follicular adenoma and bladder rhabdomyosarcoma . 
bladder rhabdomyosarcomas have been associated previously with dicer1 syndrome , although specific discussion of their histologic features was not reported.4 her two ovarian tumors were detected at the same time , and it was unclear whether they represented distinct primary tumors or metastatic spread . 
her initial renal tumor bore a p.v274l variant , as we described previously.20 however , her remaining tumors had no additional somatic tp53 variants and did not undergo loss of heterozygosity at tp53 . discussion clinically , the discovery of a second tumor with similar histology can raise the question of whether it is a recurrence or a new primary tumor . 
had we known that her second kidney tumor was , in fact , metachronous , she might have avoided the increased toxicity of chemotherapy regimens designed for relapsed or refractory tumors . 
in fact , the cartilaginous elements of her bladder tumor led us to question whether it could instead represent a distant recurrence of her renal sarcoma , although its distinct dicer1 mutation proved its independence . thus , this case highlights a powerful but often overlooked application of clinical tumor sequencing : better understanding of the biology behind tumor formation . 
as sequencing costs fall , clinicians should be cognizant that tumor sequencing can help distinguish between new primary tumors and recurrences . in this case , sequencing at initial diagnosis would have also had the added benefit of alerting clinicians to her potential dicer1 status . 
in the case of dicer1 syndrome , because second hit mutations occur at such stereotyped positions , sequencing separate tumors could even occur by simple sanger sequencing rather than by next - generation sequencing . 
in patients with dicer1 syndrome , dedicated tests may be developed for identifying these stereotyped mutations , perhaps including circulating tumor dna assays as a noninvasive screening method . this is one of the most severe cases in the literature of multiple distinct somatic dicer1 mutations arising in a patient . 
shukla no relationship to disclose jason wang no relationship to disclose veena rajaram no relationship to disclose gordan vujanic no relationship to disclose tamra slone no relationship to disclose dinesh rakheja no relationship to disclose james f . 
slade i , bacchelli c , davies h , et al : dicer1 syndrome : clarifying the diagnosis , clinical features and management implications of a pleiotropic tumour predisposition syndrome . 
schultz ka , pacheco mc , yang j , et al : ovarian sex cord - stromal tumors , pleuropulmonary blastoma and dicer1 mutations : a report from the international pleuropulmonary blastoma registry . 
schultz ka , harris a , messinger y , et al : ovarian tumors related to intronic mutations in dicer1 : a report from the international ovarian and testicular stromal tumor registry . 
durieux e , descotes f , mauduit c , et al : the co - occurrence of an ovarian sertoli - leydig cell tumor with a thyroid carcinoma is highly suggestive of a dicer1 syndrome . 
klein s , lee h , ghahremani s , et al : expanding the phenotype of mutations in dicer1 : mosaic missense mutations in the rnase iiib domain of dicer1 cause glow syndrome . 
brenneman m , field a , yang j , et al : temporal order of rnase iiib and loss - of - function mutations during development determines phenotype in dicer1 syndrome : a unique variant of the two - hit tumor suppression model . 
vujani gm , kelsey a , perlman ej , et al : anaplastic sarcoma of the kidney : a clinicopathologic study of 20 cases of a new entity with polyphenotypic features . 
pugh tj , yu w , yang j , et al : exome sequencing of pleuropulmonary blastoma reveals frequent biallelic loss of tp53 and two hits in dicer1 resulting in retention of 5p - derived mirna hairpin loop sequences . 
 evolving landscape of molecular prescreening strategies for oncology early clinical trials rodrigo dienstmann , md1 ; elena garralda , md , msc2 ; susana aguilar , phd1 ; gemma sala , msc2 ; cristina viaplana , msc1 ; fiorella ruiz - pace , msc1 ; jenifer gonz alez - zorelle , bsc1 , 3 ; deborah grazia logiacco , phd3 ; zighereda ogbah , bsc3 ; laia ramos masdeu , phd3 ; francesco mancuso , bsc3 ; roberta fasani , md4 ; jose jimenez , bsc4 ; paola martinez , bsc4 ; ana oaknin , md , phd2 ; cristina saura , md , phd2 ; mafalda oliveira , md , phd2 ; judith balmaa , md , phd2 ; joan carles , md , phd2 ; teresa macarulla , md , phd2 ; elena elez , md , phd2 ; maria alsina , md , phd2 ; irene braa , md , phd2 ; enriqueta felip , md , phd2 ; josep tabernero , md , phd2 ; jordi rodon , md , phd2 , 5 ; paolo nuciforo , md , phd4 ; and ana vivancos , phd3 most academic precision oncology programs have been designed to facilitate enrollment of patients in early clinical trials with matched targeted agents . 
we started with a tumor - agnostic hotspot mutation panel plus in situ hybridization and immunohistochemistry of selected markers and subsequently transitioned to tumor - specic amplicon - based next - generation sequencing ( ngs ) tests together with custom copy number , fusion , and outlier gene expression panels . 
in parallel , biomarker - matched trials evolved from a scenario of few targets and large populations ( such as pi3k inhibitors in pik3ca mutants ) to a complex situation with many targets and small populations ( such as multiple targetable fusion events )  . 
the substantial increase of immunotherapy trials had a major impact in target prioritization and guided clinical implementation of new markers , such as tumor mutational burden , with larger exonbased ngs assays and gene expression signatures to capture microenvironment inltration patterns . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction during the last decade , when targeted agents entered the phase i clinical trial arena and next - generation sequencing ( ngs ) became a standard molecular prescreening test to identify actionable alterations , oncologists experienced a major shift toward biomarkerdriven drug development.1 there was a lot of enthusiasm with this approach , which culminated with the approval of many targeted drugs in molecularly selected patients on the basis of nonrandomized data . 
more recently , another important milestone was reached with the approval of tissue - agnostic therapies in biomarker - selected population , rst the immune checkpoint inhibitor pembrolizumab in microsatellite instable ( msi ) tumors and then trk inhibitors larotrectinib and entrectinib in cancers harboring ntrk fusions . 
given these exciting advances , many reference institutions initiated precision oncology programs with longitudinal patient cohorts undergoing tumor molecular proling nested to early clinical trials with matched targeted agents.2 in parallel , as advances in immuno - oncology are changing the standard of care of many cancer types , the phase i oncology community experienced another paradigm shift in drug development , with an unprecedented number of new investigational agents entering clinical testing.3 not only different antipd - 1 / l1 inhibitors but also multiple combination regimens are being investigated in early clinical trials . 
more recently , genomic biomarkers are inclusion criteria to select patients for immune checkpoint inhibitor therapy , such as tumor mutation burden ( tmb ) and mutations in dna damage repair ( ddr ) pathway genes . in this evolving scenario , early clinical trial units had to constantly adapt to new biomarker - drug codevelopment trends . 
because the molecular prescreening program was established at our institution , we customized the techniques and procedures to accurately identify molecular alterations in tumors from patients eligible for early clinical trials . 
the team meets periodically to discuss existing molecular tests and new biomarkers of interest to be added to our prescreening progracancer biologists and genomicists participate in weekly molecular tumor board meetings with medical oncologists to provide guidance on the interpretation of ngs results and discuss new markers for clinical testing in patients eligible for early clinical trials . as detailed in figure 1a , we started with a targeted single base extension mutation assay covering hotspot events in 20 oncogenes and tumor suppressor genes ( sequenom ) plus uorescent in situ hybridization ( fish ) or immunohistochemistry ( ihc ) analysis of selected genes and proteins . 
in 2013 we implemented an ncounter rna platform ( nanostring ) fusions and gene expression ( gex ) analysis of 26 genesfusion and gex ncounter . in 2014 we substituted the hotspot mutation panel with a custom amplicon - based ngs assay covering 59 genes ( miseq ) , and 1 year later we replaced the fish analysis with a targeted copy number ncounter dna panel of 44 genescna ncounter . 
during 2015 we also added brca1 / brca2 genes to the ngs panel , introduced pdl1 ihc and msi testing by ihc ( with polymerase chain reactionbased test in equivocal cases )  . 
in 2018 we developed an exonbased ngs assay ( hiseq ) with 420 genes , encompassing ddr plus epigenetic pathway genes and ne - tuned for tmb quantication and other genomic signatures , such as msi . 
so far , this assay is limited to selected cases of particular interest , as per discussions in weekly molecular tumor boards , but will eventually replace the amplicon ngs and nanocopy dna panels in the coming year . 
to identify patients eligible for antibody - drug conjugates , different ihc assays were developed in collaboration with pharmaceutical companies , which allowed local testing instead of sample shipment for central proling . 
most pharmaceutical companies also accept our in - housedeveloped genomic testing as screening for biomarker - guided trials , but we noticed that a growing number of early clinical trials mandate central ngs companion diagnostic tests , specically in lung , bladder , and biliary tract cancers . all assays were optimized for archived formalin - xed parafn - embedded tumor tissues . 
importantly , ngs assays had frequent modications in gene coverage to capture emerging biomarkers being investigated in clinical trials at our institution , such as the recent additions of notch family genes to the mutation panel , ntrk breakpoints to the fusion assay , and cd274 ( pd - l1 ) to the cna ncounter test . 
in 2018 , the amplicon - based ngs panel was tailored as multiple tumortypespecic panels , with coverage limited to genes that have been previously found to be mutated in each malignancy . 
finally , circulating tumor dna ( ctdna ) mutation detection panels are under development but still limited to patient cohorts with predened tumor types participating in validation studies . each oncologist has the responsibility to dene a patients eligibility for molecular prescreening on the basis of clinical features , tumor type , and disease setting . 
cna ncounter , copy number alteration nanostring panel ; fish , uorescent in situ hybridization ; fusion and gex ncounter , fusion and gene expression nanostring panel ; ihc , immunohistochemistry ; msi , microsatellite instability ; ngs , next - generation sequencing . yield ( combined prevalence of targetable molecular alterations ) exceeds 3% . 
depending on the tumor type , molecular tests are performed up front ( such as in lung cancer when sufcient tissue is available for ngs ) , while patients receive standard - of - care chemotherapies ( such as biliary tract cancer and hormone receptorpositive breast cancer ) , or after progression to approved regimens ( such as cervical cancer )  . 
we educate clinicians not to indicate ngs as a rescue diagnostic test to identify targets for experimental therapies when patients have fast clinical deterioration , but also to avoid the all - comers up - front strategy , given the potential reduced cost effectiveness of this approach for all advanced tumor types . 
 dienstmann et al after the patient signs informed consent for broad tumor molecular proling , requests are submitted to the molecular oncology unit for sample retrieval , qualication , and preparation , and to perform ihc / fish tests . 
turnaround time is , 1 week for ihc or fish tests and approximately 2 weeks for the amplicon - based ngs panel ; ncounter results are reported within 2 - 3 weeks and exon - based ngs panel in 3 - 4 weeks . 
depending on the assays coverage , it serves as a substitute for the internal program . our molecular prescreening program is free of charge to patients and nanced with both internal resources acquired through competitive grants or donations ( institutional patronage ) and external funds from agreements with pharmaceutical companies running early clinical trials with mandatory biomarker matches . 
in the latter case , which represents 15% of total budget , the conancing models can be a molecular prescreening fee for each patient recruited in the trial or a pay - per - test fee while the trial is recruiting patients ( with monthly reports detailing number of tests performed and positive results )  . as shown in figure 1b , close to 2 , 500 molecular tests were performed in 2018 , a 10 - fold increase as compared with 2010 . 
in 2010 , most early therapeutic trials tested pi3k pathway inhibitors ( n = 11 ) , whereas in 2018 , immunotherapy trials represented the great majority ( n = 75 ) , followed by antibody - drug conjugates ( n = 9 ) , epigenetics ( n = 9 ) , fgfr inhibitors ( n = 9 ) , pi3k pathway inhibitors ( n = 8 ) , mek / erk inhibitors ( n = 8 ) , and egfr / erbb2 inhibitors ( n = 7 )  . 
regarding phase i trials with targeted drugs ( fig 2a ) , we observed a gradual increase in the number of targets of interest for clinical development from 2010 to 2016 , including alk / ros1 , fgfr1 - 3 , braf , met , notch1 - 2 , ddr pathways alterations , and others ( hdm2 , kit , pdgfr , idh1 - 2 , ret , ntrk1 - 3 , cyclin , and wnt pathways )  . 
this was accompanied by a major increase in the number of immunooncology trials , which escalated since 2015 ( fig 2b )  . the criteria for patient enrollment in a given trial go beyond genomic markers . 
in cases of borderline evidence of clinical actionability of molecular targets ( enrichment criteria ) or no oncogene alteration , alternative therapies are considered , type and taking into consideration tumor availability of slots in trials with immunotherapies and other drugs . 
more recently , immune - related markers are used as positive selection criteria for clinical trials with novel immune - oncology drugs and combinations . out of 161 early clinical trials actively recruiting patients in 2018 , 57 investigated targeted agents ( fig 2a ) , 24 of them ( 42% ) were combination regimens , and 48 ( 84% ) had mandatory or enrichment molecular inclusion criteria , the most common being fgfr , mapk , pi3k , egfr / erbb2 , and ddr pathway alterations . 
regarding immunotherapy trials , 57 out of 75 ( 76% ) were combination regimens and 32 ( 43% ) had mandatory or enrichment molecular criteria for recruitment , with pd - l1 expression and msi status being the most common biomarkers ( figs 2b and 2d )  . 
we also gradually increased the number of clinical trials testing antibody - drug conjugates , most of them with mandatory ihc analysis for patient selection , and epigenetic targets , rarely recruiting patients on the basis of genomic proling ( as brd4 - nut fusions for bet inhibitors )  . inclusions in clinical trials with targeted agents uctuated from 2010 to 2018 ( fig 2c )  . 
the multiplicity of drug targets under investigation coupled with a growing number of molecular tests being performed during this period allowed recruitment of more patients in phase i including trials assessing novel biomarkers , fgfr1 - 3 , notch1 - 2 alterations , and brca1 - 2 mutations , among others . 
we observed a major decrease in recruitment rates in phase i trials with targeted agents in 2017 , in part related to lower interest in some targets , such as pi3k pathway inhibitors , but also a 3 - fold increase in the number of patients referred to phase ii or iii trials with molecular matches , from 84 in 2016 to 224 in 2018 . 
chemo , chemotherapy ; immuno , immunotherapy ; msi , microsatellite instability . 306 patients recruited in immunotherapy trials during 2018 , 92 ( 30% ) were based on biomarkers . to investigate the clinical utility of our program , we assessed how the results of proling ( both in - house and external ) affected the immediate treatment decision of each patient . 
the most common tumor types undergoing molecular proling in the last 3 years are shown in figure 3a . in 2018 , we noticed an increase in lung , breast , and pancreatobiliary cancers being tested in line with major advances in precision cancer therapy across these tumor types . 
it is important to emphasize that these represent patients not eligible for standard - of - care genomically guided therapy , such as braf inhibitors in brafv600emutated melanomas , or her2 - targeted therapy in erbb2amplied breast cancer . 
 a 2016 ( n = 1 , 281 ) 18 19 26 dienstmann et al 2017 ( n = 1 , 218 ) 15 22 18 1 , 104 2018 ( n = 1 , 416 ) 18 12 18 colorectal lung breast pancreatobiliary gynecologic gastric head and neck other brain urinary sarcoma skin endocrine inner ring no trial immunotherapy nonimmunotherapy matched phase 1 - 3 trial outer ring biomarker mandatory biomarker enrichment fig 3 . 
 ( b ) recruitment in biomarker - guided ( mandatory or enrichment ) and other alternative trials ( immunotherapy or nonimmunotherapy )  . guided targeted agents , antibody - drug conjugates , and immunotherapies . discussion the vall dhebron institute of oncology ( vhio ) molecular prescreening program is constantly adapting to the needs of our early clinical trial portfolio . 
we observed a dramatic change in the landscape of phase i clinical trials , now focused on targeted agents for rare molecular alterations , immunotherapy combinations , antibody - drug conjugates , and epigenetic agents . 
in parallel , different ngs assays were developed for accurate detection of rare actionable mutations , copy number alterations , fusion events , and novel ihc tests were introduced . from the beginning , we followed a personalized prescreening approach , whereby oncologists are empowered to decide which patients are eligible for testing based on clinicopathological features and which molecular tests are indicated in each disease setting . 
by avoiding the one - testfor - all strategy , we were able to optimize the use of our prescreening program and educate the clinicians on molecular epidemiology of each tumor type as well as emerging diagnostic tests . 
the decision to transition from smaller tumor - specic panels to a larger exon - based ngs that covers both mutation and copy number tests is related to the need to accommodate emerging biomarkers in the ddr and epigenetic pathways as well as tmb quantication . 
overall , 1 out of 10 patients proled are ultimately enrolled in matched targeted trials , which is in line with other academic molecular prescreening programs with nested clinical studies.4 regarding germline sequencing , we follow guideline - directed testing and have regular meetings with genetic counselors to discuss secondary incidental ndings in tumor sequencing.5 in the last decade , biomarker - matched trials evolved from a scenario of few targets and large populations to a complex situation with many targets and small populations . 
even with a growing number of targets being investigated in phase i trials , and the multiplicity of trials per target , we observed a relative reduction in the number of patients enrolled in molecularly guided trials in the last years . 
this is the result of shifting interests in drug development and a clear focus on a limited number of promising biomarkers , such as rare fusion events in fgfr1 - 3 , ret , and ntrk1 - 3 genes . 
in this scenario , liquid biopsies for target identication are becoming quite useful , which has guiding our current development of a ctdna ampliconbased ngs test and prompted collaborations with commercial partners for molecular prescreening . the substantial increase in immunotherapy trials had a major impact on trial prioritization . 
inclusion criteria of immuno - oncology phase i trials are frequently limited to tumor type and treatment line , with few trials having a mandatory molecular match , which facilitates patient recruitment . 
we noticed an increase in biomarker - guided immunotherapy trial recruitment in 2018 , which is guiding implementation of a multimodality biomarker strategy that moves beyond tmb quantication , such as immune cytotoxic / suppressive microenvironment signatures measured through the gex ncounter panel , 6 as well as multiplex ihc panels.7 to conclude , we believe that to accelerate progress in precision oncology , clinical trials with adaptive designs to enroll patients on the basis of multiomics enrichment criteria are needed . 
the previous era of molecularly guided targeted agents is restrictive , and larger portfolios of drugs that include immunotherapeutic and antibody - drug conjugates with recruitment guided by molecular tests must be pursued . 
in our view , the future of cancer drug development will encompass sequential genomic proling to guide matched targeted therapies , complex multimodality biomarkers for immune - oncology agents , individualized immunotherapeutics , novel combination regimens with epigenetic drugs , and antibody - drug conjugates . 
as precision oncology becomes a more paved road , clinicians in the community oncology setting must be cognizant of its full potential and reference institutions must establish patient referral networks to increase the access to innovative experimental therapies . 
 dienstmann et al speakers bureau : msd , roche , thermo fisher scientic research funding : novartis , roche ( inst ) , thermo fisher scientic ( inst ) travel , accommodations , expenses : bristol - myers squibb , menarini , glycotope , merck sharp & dohme ana oaknin consulting or advisory role : roche , astrazeneca , pharmamar , clovis oncology , tesaro , immunogen , genmab research funding : abbvie deutschland ( inst ) , ability pharmaceuticals ( inst ) , advaxis ( inst ) , aeterna zentaris ( inst ) , amgen ( inst ) , aprea therapeutics ( inst ) , clovis oncology ( inst ) , eisai ( inst ) , f . 
mandelker d , donoghue m , talukdar s , et al : germline - focussed analysis of tumour - only sequencing : recommendations from the esmo precision medicine working group . 
lu s , stein je , rimm dl , et al : comparison of biomarker modalities for predicting response to pd - 1 / pd - l1 checkpoint blockade : a systematic review and meta - analysis . 
calvo f , apolone g , baumann m , et al : cancer core europe : a european cancer research alliance realizing a research infrastructure with critical mass and programmatic approach to cure cancer in the 21st century . 
thirty - one patients ( 38% ) and 17 patients ( 46% ) underwent germline testing from the automatic pipeline and other referrals , respectively , and of these patients , 23 ( 72% ) and four ( 24% ) had conrmed germline pathogenic variants ( gpvs ) , respectively . 
the majority of conrmed gpvs were in automatic referral genes , with brca2 being most common ( conrmed gpvs in 11 [ 85% ] of 13 patients tested ) , followed by palb2 ( ve [ 67% ] of six patients ) , brca1 ( two [ 40% ] of ve patients ) , msh6 ( two of three patients ) , and mlh1 ( two of two patients )  . 
germline testing was not performed in 50 ( 62% ) of 81 patients identied by automatic referral as a result of poor patient health or death ( 30% ) , lack of follow - up ( 30% ) , and patient refusal ( 30% )  . conclusion of patients undergoing tgp , 5% had somatic ndings triggering referral , and implementation of an automatic referral pipeline based solely on gene versus other clinical or molecular features resulted in a 74% germline conrmation . 
use of such testing has rapidly increased , with further growth anticipated.1 mutations identied on tumor sequencing may be acquired somatically , caused by postzygotic mosaicism , or identication of inherited through the germline . germline mutations potentially inuences treatment of the current cancer , may provide prognostic information about the potential development of future cancers , and has important implications for family members in terms of risk and prevention of disease.2 however , guidelines on both how to determine which somatic ndings may be potentially germline and the optimal clinical practice for referral and germline testing of patients undergoing tumor sequencing are not widely available , and there is no established standard of care.3 genomic testing of tumor tissue can be performed in tandem with germline testing ( via blood or sequence matched normal tissue ) 4 - 6 ; such tumor - germline paired sequencing allows determination of mutation etiology ( inherited v acquired )  . 
 clark et al context key objective as the use of somatic tumor genomic testing rapidly increases , a pipeline for referral of potential germline genetic ndings is critically needed . knowledge generated more than 70% of known cancer predisposition gene mutations identied in patients tumor genomic testing were conrmed to be germline . 
however , less than half of eligible patients underwent germline genetic testing as a result of poor patient health or death , lack of follow - up , and / or patient refusal . relevance our ndings indicate that patients with pathogenic mutations in well - characterized cancer predisposition genes should be referred for consideration of germline genetic testing , although signicant implementation challenges remain . be associated with hereditary cancer syndromes for both the patients and their family members . 
however , potential germline variants on tgp may be under - recognized.8 national comprehensive cancer network ( nccn ) guidelines are evolving ; they currently state that pathogenic variants in cancer susceptibility genes identied on tumor proling of any tumor type should undergo germline conrmation.9 however , the logistics of identifying potentially actionable germline mutations , such as those in brca1 and brca2 , from tgp can be complex , in large part as a result of the coordination of germline genetic testing for ill patients who may be unaware that their tumor testing could reveal inherited mutations . 
somatic pathogenic mutations as dened in cbioportal were downloaded from the provisional data sets of multiple tumor types in july 2015 ( data supplement ) and updated in july 2018 ( table 1 )  . 
original germline mutation rates were averaged from two large studies of patients with metastatic cancer5 , 6 and updated with tcga data , 11 and mutations were dened as reported in the original studies.5 , 6 , 11 the ratio of the germline mutation rate to total mutation rate was determined ( table 1 ; appendix fig a1 )  . 
genes were also annotated with the number of tumor types with somatic mutation rates greater than 10% ( data supplement )  . delineation of criteria for automatic referral for germline testing criteria for automatic referral for germline testing after tgp from june 2016 through june 2018 , the center for personalized diagnostics ( cpd ; college of american pathologists and clinical laboratory improvement amendments approved ) at penn medicine evaluated 2 , 308 unique tgp tests with either a 153 - gene panel ( n = 2 , 087 ) or a 47 - gene panel ( n = 221 ) , depending on the version of the panel available ( data supplement )  . 
a multidisciplinary team , including genetic counselors , medical oncologists , medical geneticists , and molecular pathologists , was established to determine which somatic results warranted automatic referral for germline genetic testing . 
 clark et al was not included in our analysis because of controversy over screening guidelines and its relatively high prevalence.12 implementation of germline testing referral pipeline solid tumor sequencing reports were signed out per clinical practice standards , and variants in the automatic referral pipeline were identied manually by the reviewing cpd attendings . 
language for clinical reports was created stating that additional testing would be necessary to determine whether the identied pathogenic variant on somatic testing was a germline pathogenic variant ( gpv )  . 
an e - mail was sent from the cpd to the ordering oncologist and a designated genetic counselor ( gc ) when a variant meeting automatic referral criteria was identied . 
initial disclosure of the somatic test results , including the possibility of a germline nding , was the responsibility of the ordering provider.13 after patients were made aware of somatic ndings by their oncologist , patients were contacted by the gc for coordination of care . 
molecular pathologists and oncologists also were encouraged to refer patients outside the automatic pipeline on the basis of genotype - phenotype correlation . data collection , chart review , and statistical analysis a university of pennsylvania institutional review board approved retrospective chart review was conducted , with data collected for all referrals within the automatic pipeline and other referrals based on tgp by the academic laboratory between june 2016 and june 2018 ( 81 referrals by automatic pipeline and 37 referrals outside the pipeline )  . data were collected on patient demographics , tumor type tested ( data supplement ) , and somatic and germline testing results . 
continuous variables were compared using the t test , and contingency tables were analyzed using fishers exact test . results referral characteristics from june 2016 to june 2018 , 2 , 308 patients underwent tgp at penn medicines cpd . 
of those patients , 118 ( 5.1% ) were referred for clinical germline genetic testing based on tgp performed at the cpd . referral of 81 patients was triggered by the automatic algorithm , and 37 patients were referred from either the molecular pathologist ( n = 21 ) or the patients physician ( n = 16 ; fig 2a )  . 
the majority of patients were white ( 88% ) and female ( 52% ) , and the mean age at tgp was tumor types 58 years ( table 2 )  . 
thirteen patients were referred for variants with a high likelihood in chek2 of being germline ( founder mutations ) ( n = 11 ) and one each for variants in atm and egfr ( fig 2a ; data supplement )  . 
direct referrals for germline genetic testing by the molecular pathologist and primary oncologists after a variant was found on tgp were largely based on genotype - phenotype concerns ( eg , tp53 mutations in patients with cancer age 45 years or younger or patients with brain tumors or sarcomas ; cdkn2a / cdk4 mutations in patients with melanoma )  . 
referrals of 21 patients by the molecular pathologist were initiated by e - mail to the gc and primary oncologist and included ndings in nine genes , most commonly tp53 ( fig 2a ; data supplement )  . treating physicians referred 16 patients with variants in 12 different genes ( fig 2a , data supplement )  . results of germline conrmation of 118 patients with referrals , 48 ( 41% ) underwent clinical genetic counseling and genetic testing ( fig 2a )  . 
genetic testing rates were similar for referrals from the automatic referral pipeline and those sent by the molecular pathologist ( 38% and 33% , respectively ) , whereas 63% of patients referred by their treating physician underwent genetic testing ( fig 2a )  . 
a majority of patients ( 27 [ 57% ] of 48 patients ) had variants that were conrmed gpvs , with 74% of automatic referrals being conrmed gpvs and 29% and 20% of molecular pathologist and treating physician referrals being conrmed gpvs ( fig 2a )  . 
the majority of patients ( 60% ) had multiplex panel testing ; however , 19% underwent a small custom panel , 17% were only tested for the variant by single - site testing , and 4% had ashkenazi jewish founder testing ( data supplement )  . the 81 patients referred by the automatic referral pipeline , the majority ( n = 59 ) were referred for variants in high - risk genes ( 73% ; fig 2b )  . 
genetic testing rates were highest for high - risk genes ( 28 referrals [ 47% ] underwent genetic testing compared with three referrals [ 14% ] in the other groups )  . 
mutations in the automatic referral pipeline were agged by the tumor testing laboratory , and an e - mail was sent from molecular pathologist to the ordering physician ( md ) and genetic counselor ( gc )  . 
results not included in the automatic referral pipeline but of concern to the molecular pathologist or ordering oncologist to be possibly germline were also e - mailed to the gc . 
the gc called the patient only after the somatic results were discussed with the patient by the ordering md , the patient agreed to be contacted , and the oncologist contacted the gc . 
an inperson cancer risk evaluation appointment was scheduled , and the appropriate germline testing modality was determined by gc at time of visit ( panel or single - site testing )  . 
results were provided by telephone by the gc , and patients with positive testing results along with their relatives were offered in - person follow - up visits for medical management . 
one hundred eighteen patients were referred for germline testing83 by the automatic pipeline , 20 by the testing laboratory at the discretion of the molecular pathologist , and 15 directly from the ordering physician . 
 ( b ) of the 83 patients referred by the automatic pipeline , 61 had mutations in high - risk genes ( brca1 , brca2 , palb2 , mlh1 , msh2 , and msh6 ) , nine had mutations in moderate - risk genes ( brip1 , rad51c , and rad51d ) , and 13 had mutations with high prior probability of being germline ( likely germline )  . 
 ( c ) in the 51 patients referred by the automatic pipeline but who did not undergo testing , patients were not seen as a result of death before scheduling an appointment , refusal of the consult by the patient , absence of referral placed by ordering physician , or other reason . or both ( fig 2c )  . 
 characteristic age , years mean range male race tumor type white black other lung brain breast other melanoma 526 ( 23 ) 676 ( 29 ) 519 ( 22 ) 125 ( 5 ) 59 ( 3 ) 25 ( 1 ) 122 ( 5 ) germline results in tumor - only genomic testing table 2 . 
 ( a ) in patients who presented for conrmatory germline testing , the age at diagnosis for patients with a conrmed germline pathogenic variant ( gpv ) versus somatic pathogenic variants ( spvs ) not conrmed to be in the germline . 
 ( c ) percentage of patients with a conrmed gpv versus an spv for whom the gene is known to be associated with the tumor where the variant was found . 
of 2 , 308 patients who underwent tgp at penn medicines cpd , 149 ( 6.6% ) had variants in the automatic referral genes , and 118 ( 5% ) were referred for clinical germline genetic testing . 
a majority of the variants tested were conrmed gpvs ( 27 [ 54% ] of 50 variants ) , with the highest germline conrmation rate in high - risk genes ( 21 [ 72% ] of 29 genes )  . 
thus , we have demonstrated that an automatic referral algorithm results in a high yield of conrmed germline mutations . in total , 27 ( 1.1% ) of 2 , 308 patients undergoing tgp had a conrmed gpv . 
germline ndings have been found by retrospective analysis in 4% to 12% of prior clinical tumor sequencing cohorts5 , 6 , 14 and in 8% of the tcga cohort , 11 with 2.8% of the tcga cohort having germline mutations in the genes selected for automatic referral in this study . 
if all 149 patients with mutations in automatic referral genes in our cohort had undergone germline testing , we would have expected 107 to have a germline mutation ( based on our 72% germline conrmation rate )  . 
a limitation of this study is that sequencing was not performed on all patients with metastatic disease at the university of pennsylvania ; in addition , germline sequencing was not performed in all dividuals with somatic sequencing . 
thus , we do not know the exact prevalence of germline mutations in our population . genes were chosen for automatic referral based on several factors , but the major determinant was the ratio of germline mutation rate to total ( germline plus somatic ) mutation rate calculated from public databases . 
thus , referring all individuals with mutations identied in such genes ( eg , tp53 and pten ) identied by tgp in the absence of other factors rarely results in a positive germline nding . 
however , other genes have higher mutation rates in the germline compared with somatic only ( eg , brca1 / 2 ) , and known founder mutations would likely always be germline . 
for example , in our study , all three ashkenazi jewish founder mutations in brca1 / 2 that were found on tgp were conrmed gpvs . the automatic referral algorithm did not rely on clinical characteristics or variant af or exclude patients with likely hypermutated tumors . 
the nding that germline af can be lower than the expected range of 50% or greater is consistent with prior data.15 multiple patients had germline mutations identied despite somatic testing done on tumors not generally considered part of the hereditary syndrome . 
the high germline conrmation rate for the automatic referral genes validates our approach of prioritizing the ratio of germline to total mutations of a gene , with lesser emphasis placed on af or tumor type . 
we have updated both germline and somatic mutation rates with current11 data ( table 1 ) , demonstrating that most of these genes have a ratio of germline mutation rate to total mutation rate of greater than 0.25. 
the only genes not included on our original list that t these criteria are atm and chek2 . we are adding all mutations in these genes to our referral list ( rather than restricting to certain mutations with high prior probability of being germline )  . other approaches for gene selection exist ; however , we wished to prioritize the highest impact genes related to prognosis or therapy , clinical trial enrollment ( eg , brca1 / 2 mutations and poly [ adp - ribose ] polymerase inhibitors ) , or effect on family members.16 - 19 in addition , we wished to assess the success of this approach and potential burdens before widening the scope . 
curation of the list of genes in which mutations prompt referral for germline genetic testing will be an ongoing process and will need to reect updates in guidelines from the american college of medical genetics and nccn . 
the automated referral algorithm had a high specicity , as 72% of ndings were conrmed gpvs . in patients for whom somatic sequencing triggered a referral by their oncologist without meeting criteria on the algorithm , only two patients ( 20% ) had conrmed gpvs ( atm and chek2 )  . 
as mentioned earlier , both genes are being added to our automated referral algorithm . criteria for germline genetic testing are rapidly evolving , and routine germline multiplex panel testing may soon become standard for all patients with metastatic disease . 
in our study , of 28 patients who underwent multiplex panels , either testing was negative ( n = 13 ) or only the somatic variant was found ( n = 15 ) , indicating that there may be limited incremental benet to expanded germline testing in patients with metastatic cancer who have undergone tumor testing . 
however , individuals with a high likelihood of having a germline mutation in a cancer susceptibility gene should be considered for germline testing even in the setting of a negative tgp . 
for example , in individuals with a strong family history of breast and ovarian cancer , approximately 10% of brca1 mutations are large genomic rearrangement , which may be more difcult to detect with current tgp assays . the majority of patients ( 61% ) with a somatic nding identied by the automatic referral pipeline were not seen by clinical cancer genetics services . 
published data suggest that patients express great interest in wishing to learn their germline status20 ; therefore , it is likely that patient and provider education and improved infrastructure for referrals are needed . 
 germline results in tumor - only genomic testing cancer therapy and symptom management , simplifying the process by which patients become aware of the possibility of germline ndings arising from tgp and have access to germline conrmation is critical . 
the ongoing communication and education in tumor proling ( comet ) trial ( clinicaltrials.gov identier : nct02823652 ) , a companion study to the national cancer institute molecular analysis for therapy choice ( nci - match ) trial , will provide additional information regarding best practices . genetic counseling challenges in this population of patients with advanced cancer included the substantial burden of patient illness ( including both symptom and appointment burdens , although considerable efforts were made to coordinate appointments with other visits )  . 
there was an appreciable time commitment by the gc that was not billable ( eg , discussions by phone ) , and a number of patients tested did not have insurance coverage because their tumor type did not meet published criteria for germline testing . 
nccn criteria for further genetic risk evaluation ( version 2.2019 ) now include individuals at any age with a known pathogenic variant or likely pathogenic variant in a cancer susceptibility gene found on tumor testing ; however , during the dates of our study , existing criteria included brca1 / 2 only.9 we performed a single - institution study and only evaluated ndings from penn medicines cpd ; thus , generalizability of this approach is not yet known . 
in addition , full somatic sequencing for all of the automatic referral genes was not performed on every patient as a result of availability of specic somatic sequencing panels at different points in time . 
we did not implement approaches such as telegenetics , which may further reduce patient burden ( although germline samples must still be obtained )  . we have demonstrated that an automated referral process for patients with mutations detected in tgp can lead to the identication of germline mutations in cancer susceptibility genes with implications for both patients and their family members . 
 clark et al jacquelyn powers employment : carevive systems honoraria : cureconnect consulting or advisory role : carevive systems travel , accommodations , expenses : hospital of the university of pennsylvania jessica m . 
long employment : depuy companies ( i ) stock and other ownership interests : depuy companies ( i ) travel , accommodations , expenses : depuy companies ( i ) payal shah stock and other ownership interests : johnson & johnson ( i ) , novartis ( i ) , novo nordisk ( i ) , pzer ( i ) , merck ( i ) , amgen , johnson & johnson , novo nordisk consulting or advisory role : tmunity therapeutics jennifer j.d. 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) no other potential conicts of interest were reported . references raymond vm , gray sw , roychowdhury s , et al : germline ndings in tumor - only sequencing : points to consider for clinicians and laboratories . 
j pathol 244 : 610 - 615 , 2018 arango np , brusco l , mills shaw kr , et al : a feasibility study of returning clinically actionable somatic genomic alterations identied in a research laboratory . oncotarget 8 : 41806 - 41814 , 2017 4 . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
ann oncol 27 : 795 - 800 , 2016 schrader ka , cheng dt , joseph v , et al : germline variants in targeted tumor sequencing using matched normal dna . 
jama oncol 2 : 104 - 111 , 2016 robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . j clin oncol 33 : 3660 - 3667 , 2015 catenacci dv , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 9 . 
yurgelun mb , chittenden ab , morales - oyarvide v , et al : germline cancer susceptibility gene variants , somatic second hits , and survival outcomes in patients with resected pancreatic cancer . 
bolton kl , chenevix - trench g , goh c , et al : association between brca1 and brca2 mutations and survival in women with invasive epithelial ovarian cancer . 2014 res 22 : 4087 - 4094 , 2016 jama 307 : 382 - 390 , 2012 33 : 244 - 250 , 2015 18 . 
hamilton jg , shuk e , garzon mg , et al : decision - making preferences about secondary germline ndings that arise from tumor genomic proling among patients with advanced cancers . 
 germline results in tumor - only genomic testing appendix brca1 brca2 palb2 mlh1 msh2 msh6 brip1 rad51c rad51d chek2 tp53 bap1 cdh1 cdkn2a men1 pten smad4 smarca4 stk11 tsc1 tsc2 original updated ratio of germline mutation rate to overall mutation rate fig a1 . 
 metabolic derangements in succinate dehydrogenase bmutated renal - cell carcinomas : more than meets the eye ? see accompanying article doi : succinate dehydrogenase - deficient renal cell carcinomas ( sdh - rccs ) are rare but highly aggressive malignancies associated with mutations in the four subunits ( sdha , sdhb , sdhc , or sdhd ) of the succinate dehydrogenase ( sdh ) enzyme complex . 
in practically all sdh - rcc cases , patients have monoallelic germ - line inactivating mutations in one of the four sdh genes , followed by somatic loss of the second gene allele in the tumor cells . 
sdhc deficiency is the second most common cause of sdh - rcc , whereas sdha and sdhd loss is rarely associated with rccs.1 - 4 because of the rarity of sdh - rccs , there is little guidance on how to best diagnose , monitor , and treat patients with this disease . lee et al5 retrospectively clinically and genomically profiled three patients with sdh - rcc resulting from biallelic sdhb inactivation . 
they showed that the sdhb gene acts as a tumor suppressor on the basis of the identification of germ - lineinactivating sdhb mutations in all three cases , followed by second - hit somatic loss of the short arm of chromosome 1 ( 1p ) where sdhb is located . 
although arm - level chromosomal deletions are certainly not uncommon among solid tumors , they tend to occur more frequently in regions of low gene density that are less likely to contain genes whose deletion will be poorly tolerated by cells.6 chromosome 1p harbors a large number of genes and has accordingly been found to be one of the least frequently deleted chromosome arms across several solid tumor types.6 however , in addition to sdhrccs , somatic loss of heterozygosity is also the preferred mode of second - hit inactivation in other sdhb - associated tumors such as paragangliomas and pheochromocytomas.7 it is therefore possible that loss of the genes in chromosome 1p produces a net positive effect for cell survival when there is biallelic inactivation of sdhb . 
mutyh encodes the enzyme myh glycosylase , which is involved in dna repair and is associated with polyposis when both mutyh alleles are inactivated.8 such molecular pathways may be exploited therapeutically . for example , loss of the chromosome 1p gene urod , encoding for uroporphyrinogen decarboxylase , can increase production of reactive oxygen species and thus sensitize cells to radiation or cisplatin - based therapy.9 , 10 it is worth noting that all three patients were young ( age 19 to 37 years ) and were initially incorrectly diagnosed despite being evaluated by experienced clinicians and pathologists at a large academic referral center.5 indeed , two of three primary tumors in the study lacked the histologic findings commonly associated with sdhbdeficient sdh - rccs . 
of note , all cases of sdh - rcc are associated with immunohistochemical ( ihc ) loss of sdhb expression , regardless of which sdh subunit inactivation led to the development of tumor.1 , 2 , 5 therefore , it may be prudent to first po.ascopubs.org jco precision oncology pavlos msaouel gabriel g . 
in theory , serum concentrations of lactic acid in such patients should reflect tumor burden independently of the associated cancer type ( sdh - rcc , pheochromocytoma , paraganglioma , or gi stromal tumors )  . this should also be true in patients with hereditary leiomyomatosis and rcc ( hlrcc ) , which is associated with loss of fumarate hydratase ( fh ) , another key krebs cycle enzyme.14 it will be interesting to further explore the value of longitudinal monitoring of lactic acid to determine disease burden in patients with these malignancies or as a screening test for individuals with known germ - line sdh or fh mutations . 
notably , the metabolic shift to aerobic glycolysis also leads to more intense fluorodeoxyglucose ( fdg ) uptake in positron emission tomography ( pet ) imaging of sdh - rcc and hlrcc compared with what is usually seen in other rccs.3 , 5 , 15 how can we best use precision oncology to treat sdh - rcc ? as already mentioned , there may be pathways associated with sdhb or chromosome 1p loss that may be amenable to targeted therapeutic strategies . 
because of the retrospective nature of the study by lee et al , 5 no rna had been banked to allow transcriptome profiling , which would have elucidated the impact of sdhb and chromosome 1p loss on gene expression . tumors such as those in sdh - rcc and hlrcc are highly dependent on glucose influx to maintain aerobic glycolysis . 
bevacizumab inhibits angiogenesis and thus blocks the delivery of glucose to the tumor microenvironment.16 in addition , the epidermal growth factor receptor inhibitor erlotinib can interfere with active glucose transport into tumor cells by downregulating glucose transporter 3.17 accordingly , the combination of bevacizumab with erlotinib has been shown to produce high clinical activity in patients with hlrcc.18 sdh - rcc may similarly benefit from this combination therapy , which has not yet been tested in this tumor type . 
in addition to their addiction to glucose , the loss of sdh activity makes sdh - rcc tumor cells more reliant on glutamine for their metabolism , as shown by the increased glutamine uptake on 18fglutamine pet imaging.5 glutamine supplies biosynthetic intermediates that are crucial for amino acid and lipid synthesis in sdh - deficient tumors . 
inhibition of the glutaminase enzyme , which generates glutamate from glutamine , may impair this metabolic pathway resulting in the death of glutamine - dependent tumor cells.19 nevertheless , the patient treated with glutaminase inhibitor cb - 839 in the lee et al5 study ultimately succumbed to his disease . 
it is possible that the tumor cells overcame the glutaminase inhibition by generating intermediates for macromolecule biosynthesis via alternative pathways.20 therefore , glutaminase inhibition may be more beneficial when used as part of a combination treatment regimen to fully block the production of key metabolic intermediates in sdh - rcc . putting it all together , the study by lee et al , 5 in conjunction with earlier reports on sdh - rcc , 1 , 2 shows that clinicians should be acutely aware of the possibility of sdh - rcc when seeing young patients who harbor aggressive kidney tumors with unusual histology and / or high fdg avidity . the evaluation should begin with a thorough personal and family history that looks for occurrences of paragangliomas , pheochromocytomas , gi stromal tumors , or unexplained earlyor lateonset neurodegenerative disease and / or encephalopathy.21 one should keep in mind that a negative family history in patients with sdh - rcc may be the result of de novo germ - line mutation or incomplete penetrance as in patient 1 in the article by lee et al.5 if there is a positive history of sdhrcc or if the suggestion of that disease remains high despite the lack of associated disorders in the patients family , then ihc for sdhb should be attempted . 
malouf honoraria : novartis , roche , glaxosmithkline , janssen oncology consulting or advisory role : novartis , pfizer , bristol - myers squibb research funding : pfizer , novartis travel , accommodations , expenses : amgen , pfizer , janssen , novartis nizar m . 
tannir honoraria : pfizer , novartis , bristol - myers squibb , exelixis , nektar therapeutics , argos therapeutics , calithera biosciences consulting or advisory role : novartis , exelixis , bristolmyers squibb , nektar therapeutics , pfizer , argos therapeutics , calithera biosciences research funding : bristol - myers squibb , novartis , exelixis , epizyme , mirati therapeutics travel , accommodations , expenses : pfizer , novartis , exelixis , nektar therapeutics , bristol - myers squibb , argos therapeutics , calithera biosciences acknowledgment supported by the grant no . 
gill aj , hes o , papathomas t , et al : succinate dehydrogenase ( sdh ) - deficient renal carcinoma : a morphologically distinct entitya clinicopathologic series of 36 tumors from 27 patients . 
ozluk y , taheri d , matoso a , et al : renal carcinoma associated with a novel succinate dehydrogenase a mutation : a case report and review of literature of a rare subtype of renal carcinoma . hum pathol 46 : 1951 - 1955 , 2015 5 . 
lee ch , gundem g , lee w , et al : persistent severe hyperlactatemia and metabolic derangement in lethal succinate dehydrogenase bmutated metastatic kidney cancer : clinical challenges and examples of extreme warburg effect . 
n engl j med 348 : 791 - 799 , 2003 ito e , yue s , moriyama eh , et al : uroporphyrinogen decarboxylase is a radiosensitizing target for head and neck cancer . 
sudarshan s , sourbier c , kong hs , et al : fumarate hydratase deficiency in renal cancer induces glycolytic addiction and hypoxia - inducible transcription factor 1alpha stabilization by glucosedependent generation of reactive oxygen species . 
makinoshima h , takita m , matsumoto s , et al : epidermal growth factor receptor ( egfr ) signaling regulates global metabolic pathways in egfr - mutated lung adenocarcinoma . 
srinivasan r , su d , stamatakis l , et al : mechanism based targeted therapy for hereditary leiomyomatosis and renal cell cancer ( hlrcc ) and sporadic papillary renal cell carcinoma : interim results from a phase 2 study of bevacizumab and erlotinib . 
lussey - lepoutre c , hollinshead ke , ludwig c , et al : loss of succinate dehydrogenase activity results in dependency on pyruvate carboxylation for cellular anabolisnat commun 6 : 8784 , 2015 21 . 
sartori et al we thank sartori et al1 for their interest in the recently published review , which characterizes the her2 aberrations observed in nonsmall - cell lung cancer ( nsclc ) and summarizes the efcacy of her2targeted therapies in patients with nsclc.2 nsclc with her2 alterations is a highly heterogeneous disease . 
her2 overexpression , her2 amplication , and her2 mutation could exist alone or synchronously . sartori et al1 highlighted the contribution of immunologic features to the response to her2 - targeted therapy . 
as per the authors exploration , a strong antibody - dependent cell - mediated cytotoxicity triggered by the valine / valine ( v / v ) variant of fcriiia rather than sole target inhibition is the possible reason . the back - line application of singleunfortunately , agent immunotherapy to case 1 eventually led to hyperprogression disease ( hpd )  . 
indeed , the denition of hpd remains controversial to date , let alone the solid association between driver gene mutation and hpd.5 recently , our group also reported a patient with erbb1 exon 20 insertion mutation who suffered from hpd after nivolumab monotherapy.6 we speculated that one of the reasonable causes might be myc amplication , whose upregulation could result in cd47 activation and programmed death ligand 1 overexpression , consequently contributing to tumor growth . to the efcacy of with respect immunotherapy in her2 - mutant nsclc , 4 retrospective studies reported the outcomes.7 - 10 a total of 92 patients were treated with single - agent pd - 1 or pd - l1 inhibitor , most of them having experienced disease progression on standard chemotherapy . 
here , we call for in - depth studies of hpd mechanisms , especially the development of screening methods to identify specic subgroups in whom immune treatment would be harmful . up to now , her2 mutation , especially exon 20 insertion , is a potential therapeutic target with accumulated evidence . 
recent preclinical research reported that poziotinib potentiated the antitumor effect of trastuzumab emtansine ( t - dm1 ) by upregulating her2 expression.11 this mechanism ts the logic and the observed encouraging clinical benet from t - dm1 after disease progression on poziotinib in case 2 . 
in addition , a preclinical study conducted by li et al12 found that cotreatment of t - dm1 with irreversible pan - her inhibitors neratinib or lapatinib enhanced her2 receptor ubiquitination and consequently improved t - dm1 internalization and efcacy . 
whether the optimal combination mode is sequential or synchronous warrants further validation . trastuzumab deruxtecan ( t - dxd ) , another antibody - drug conjugate ( adc ) , harbors a different cytotoxic payload , showed better and more durable responses in her2mutant nsclc , and may be still effective after resistance to t - dm1.12 in extension , on top of her2 mutation , her2 amplication may also confer sensitivity to t - dm1 . 
according to recently released clinical trial data , t - dm1 exhibited identical orr in patients with nsclc with her2 amplication , her2 mutation , or concurrent her2 mutation and amplication ( 55% v 50% v 50% ) .12 collectively , her2 alterations in nsclc are rather heterogeneous . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . no potential conicts of interest were reported . references zhao j , xia y : targeting her2 alterations in non - small - cell lung cancer : a comprehensive review . 
precision oncol 4 : 411 - 425 , 2020 krug lm , miller va , patel j , et al : randomized phase ii study of weekly docetaxel plus trastuzumab versus weekly paclitaxel plus trastuzumab in patients with previously untreated advanced nonsmall cell lung carcinoma . cancer 104 : 2149 - 2155 , 2005 xu x , de angelis c , burke ka , et al : her2 reactivation through acquisition of the her2 l755s mutation as a mechanism of acquired resistance to her2 - targeted therapy in her2 + breast cancer . 
clin cancer res 23 : 5123 - 5134 , 2017 jin r , zhao j , xia l , et al : application of immune checkpoint inhibitors in egfr - mutant non - small - cell lung cancer : from bed to bench . 
huang x , xia l , lan f , et al : treatment of nivolumab results in hyperprogressive disease in a patient harboring egfr exon 20 insertion and myc amplication . 
mazieres j , drilon a , lusque a , et al : immune checkpoint inhibitors for patients with advanced lung cancer and oncogenic driver alterations : results from the immunotarget registry . 
ann oncol 30 : 1321 - 1328 , 2019 lai w - cv , feldman dl , buonocore dj , et al : pd - l1 expression , tumor mutation burden and response to immune checkpoint blockade in patients with her2 - mutant lung cancers . 
j clin oncol 36 , 2018 ( suppl 15 ; abstr 9060 ) dudnik e , bshara e , grubstein a , et al : rare targetable drivers ( rtds ) in non - small cell lung cancer ( nsclc ) : outcomes with immune check - point inhibitors ( icpi )  . 
guisier f , dubos - arvis c , vias f , et al : efcacy and safety of anti - pd - 1 immunotherapy in patients with advanced nsclc with braf , her2 , or met mutations or ret translocation : gfpc 01 - 2018 . 
robichaux jp , elamin yy , vijayan rsk , et al : pan - cancer landscape and analysis of erbb2 mutations identies poziotinib as a clinically active inhibitor and enhancer of t - dm1 activity . 
cancer discov 10 : 674 - 687 , 2020 sartori g , belluomini l , trovato r , et al : her2 aberrations in nsclc : so close yet so far . 
 de novo esr1 hotspot mutation in a patient with endometrial cancer treated with an aromatase inhibitor adeline morel , md1 ; julien masliah - planchon , phd1 ; guillaume bataillon , md2 ; v eronique becette , md2 ; claire morel , msc3 ; samantha antonio1 ; elodie girard , md4 ; ivan bi `eche , phd1 , 5 ; christophe le tourneau , md , phd3 , 4 , 6 ; and maud kamal , phd3 introduction endometrial carcinoma is the fourth most frequent cancer in women . 
endometrial carcinoma is classied into two subtypes : type 1 endometrial carcinoma characterized by estrogen receptor ( er ) expression and obesity , and type 2 endometrial carcinoma in nonobese , older women . 
type 1 endometrial carcinoma is associated with a favorable prognosis , whereas type 2 has a poorer prognosis.1 a prognostic genomic classication of endometrial cancers into four groups has been established using exome sequencing ; however , this classication is not used in the clinic.2 standard - of - care treatment of endometrial carcinoma consists of primary hysterectomy , bilateral salpingooophorectomy , and pelvic lymph node dissection followed by adjuvant therapy based on the histologic assessment of the specimen.3 chemotherapy is proposed in the recurrent and / or metastatic setting , whereas hormone therapy represents a treatment option for patients with er expression.4 in breast cancer , esr1 mutations were clearly identied as a mechanism of resistance to aromatase inhibitors.5 - 8 esr1 mutations were reported in 2% of endometrial cancers , 9 yet their potential occurrence following hormonal therapy is unknown . 
the diagnosis of grade 1 endometrioid carcinoma was conrmed , with less than 50% invasion of the myometrial wall thickness , 4 cm in greatest dimension , lymphovascular invasion , bilateral ovarian metastases , and no pelvic lymph node metastases ( pt3an0 f ed eration internationale de gyn ecologie et dobst etrique iiia )  . 
using immunohistochemistry , tumor cells were shown to express er , progesterone receptor , and a wild - type staining of p53 . in addition , tumor cells expressed ck7 and pax8 and did not express ck20 , ttf1 , cdx2 , and wt1 , conrming the endometrial origin of the tumor . ( ie , letrozole )  . 
after nine cycles of chemotherapy , the patient received maintenance therapy with an aromatase inhibitor receiving letrozole for 6 months , the patient experienced disease progression and was subsequently treated with doxorubicin and cyclophosphamide and then carboplatin alone . 
the patient was then biopsied in the framework of the shiva02 trial ( evaluation of the efcacy of targeted therapy based on tumor molecular proling in patients with advanced cancer using each patient as its own control ; clinicaltrials.gov identier : nct03084757 ) , which aimed to identify druggable molecular alterations , and received a fourth line of chemotherapy with gemcitabine ( fig 1 )  . molecular proling was performed on a frozen biopsy of a metastatic lymph node in the shiva02 trial using a dedicated targeted sequencing panel covering 80 genes . 
in patients with breast cancer , esr1 hotspot mutations in the ligand - binding domain were observed exclusively after hormone therapy5 - 8 and have been shown to be associated with poor prognosis.11 after exposure to aromatase inhibitors , the prevalence of esr1 mutations was signicantly higher in patients exposed during the metastatic phase than during the adjuvant phase ( 36% v 6% ) .11 in a recent study , advanced breast cancer tumors harboring esr1 mutations , or alterations in genes involved in the mitogenactivated protein kinase pathway and in the er transcriptional machinery , were shown to barely benet from aromatase inhibitors.5 esr1 amplications were detected in 12% of endometrial carcinomas , 12 whereas esr1 hotspot mutations were less frequent ( 2% ) .9 esr1 amplications were shown to be associated with a poor prognosis and seemed to be an early event in endometrial carcinoma development.12 selective er degraders , such as fulvestrant , were shown to be effective in patients with hormone receptorpositive breast cancer . 
esr1 mutations were not reported to be associated with clinical resistance to fulvestrant.13 to our knowledge , our case report is the rst to report a potential de novo esr1 mutation in a patient with erpositive endometrial carcinoma treated with an aromatase inhibitor . 
curr opin obstet gynecol 29 : 47 - 58 , 2017 kokka f , brockbank e , oram d , et al : hormonal therapy in advanced or recurrent endometrial cancer . 
cochrane database syst rev ( 12 ) : cd007926 , 2010 razavi p , chang mt , xu g , et al : the genomic landscape of endocrine - resistant advanced breast cancers . 
cancer cell 34 : 427 - 438.e6 , 2018 robinson dr , wu y - m , vats p , et al : activating esr1 mutations in hormone - resistant metastatic breast cancer . 
nat genet 45 : 1446 - 1451 , 2013 toy w , shen y , won h , et al : esr1 ligand - binding domain mutations in hormone - resistant breast cancer . 
nat genet 45 : 1439 - 1445 , 2013 bartels s , christgen m , luft a , et al : estrogen receptor ( esr1 ) mutation in bone metastases from breast cancer . 
mod pathol 31 : 56 - 61 , 2018 backes fj , walker cj , goodfellow pj , et al : estrogen receptor - alpha as a predictive biomarker in endometrioid endometrial cancer . 
schiavon g , hrebien s , garcia - murillas i , et al : analysis of esr1 mutation in circulating tumor dna demonstrates evolution during therapy for metastatic breast 12 . 
spoerke jm , gendreau s , walter k , et al : heterogeneity and clinical signicance of esr1 mutations in er - positive metastatic breast cancer patients receiving mol endocrinol 10 : 1388 - 1398 , 1996 cancer . 
tumor biopsies taken prior to neoadjuvant treatment were analyzed by reverse - phase protein arrays ( rppa ) for expression levels of 210 bc - relevant ( phospho - ) proteins . 
similarly , the mrna virp score was validated ( p , .001 ) in an independent phase ii clinical trial ( promix )  . conclusion our virp score , integrating the expression of nine proteins and validated on mrna data both internally and in an independent clinical trial , may be used to increase the likelihood of benet from treatment with bevacizumab combined with chemotherapy in patients with her2 - negative bc . jco precis oncol 5 : 286 - 306 . 
2021 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction treatment of solid tumors using antiangiogenic therapy has been explored for several decades.1 , 2 discovery of vascular endothelial growth factor a ( vegf - a ) as a major culprit in tumor angiogenesis led to the development of bevacizumab , a recombinant humanized monoclonal antibody targeting vegf - a.3 addition of bevacizumab to various chemotherapy regimens has proven highly benecial in patients with several types of advanced solid tumors resulting in a signicant improvement in overall survival ( os ) and / or progression - free survival ( pfs )  . despite good response to bevacizumab therapy in many individual patients with breast cancer ( bc ) , randomly selected treatment populations do not demonstrate improved os.4 , 5 thus , the clinical use of bevacizumab in bc is limited and currently only approved in europe . 
regardless of this , activity is observed in subsets of patients pointing to the urgent need for novel biomarkers to select subpopulations in which adequate clinical benet can be achieved.6 , 7 one of the most obvious and biological plausible biomarkers was the plasma vegf - a level , and although promising in some studies , evidence from the latter meridian trial did not support its use for identifying patients with benet from added bevacizumab.8 other biomarkers at various molecular levels have been investigated such as soluble carbonic anhydrase ix , 9 brca1 / 2 mutations , 10 and dna methylation signatures.11 however , tissue protein expression and protein signatures have not previously been explored , although data at the proteomic level in general have proven highly valuable in drug response prediction models.12 in this study , we sought to establish protein expression features predicting the response to treatment with bevacizumab in combination with chemotherapy . 
 protein signature predicts response to chemotherapy plus bevacizumab context key objective the use of antivascular endothelial growth factor ( vegf ) targeted therapies in combination with chemotherapy in breast cancer ( bc ) is limited because of the lack of a predictive biomarker . 
in this study , protein expression in pretreatment tumor biopsies was used to develop a predictor for patients with large bcs . knowledge generated a nine - protein response predictor was established by lasso regression trained by a continuous response evaluation . 
the protein signature was validated using corresponding mrna expression in the same patient cohort as well as in an independent patient cohort . relevance our study supports using this protein signature as a predictive marker for vegf inhibition in combination with chemotherapy , and represents a novel opportunity for rational use of this therapy in patients with bc . samples collected from patients with bc prior to neotreatment ( nat ) with chemotherapy ( ctx ) or adjuvant chemotherapy in combination with bevacizumab ( bev plus ctx ) , and analyzed expression against treatment effect on tumor size and clinical outcomes . 
patients with human epidermal growth factor receptor 2 ( her2 ) negative , previously untreated , breast carcinomas with size 2.5 cm were included , and 67 and 71 patients randomly assigned to treatment with ctx or bev plus ctx , respectively . 
one hundred nine samples collected prior to treatment were available for protein analysis on rppa in the ctx treatment arm ( n = 55 ) and in the bev plus ctx treatment arm ( n = 54 ) ( appendix fig a1 )  . 
clinicopathologic characteristics of patients , including adverse events , have previously been described.13 in brief , the primary end point of the clinical study , pcr , was dened as pathologic stage ypt0 and ypn0 after end of therapy . 
in the subset of patients with available protein proles ( n = 109 ) , pcr rates were overall higher in the bev plus ctx ( 26 % ) compared with the ctx ( 13 % ) treatment arm , although not signicantly ( p = .094 ) ( appendix fig a2 )  . 
relative tumor size in percent after 24 weeks of nat was calculated as tumor size at the time of surgery ( longest diameter on histopathologic specimen ) relative to tumor size at week 0 ( mri if available or ultrasound or mammography )  . 
tumor cell content in samples was assessed by use of ascat15 as previously reported.16 the study was approved by the institutional protocol review board , the regional ethics committee , the norwegian medicines agency , performed in accordance with the declaration of helsinki , and informed consent was obtained . 
we further used an external cohort with similar treatment characteristics ( promix trial , clinicaltrials.gov identier : nct00957125 ) , with mrna expression data available , 17 for validation of the virp score . reverse phase protein arrays ( rppa ) proling of 210 cancer - relevant proteins of which 54 were in a phosphorylated state ( appendix table a1 ) were performed by the rppa18 core facility at md anderson cancer center ( houston , tx )  . 
tumor protein lysates were serially diluted two - fold for 5 dilutions ( from undiluted to 1 : 16 dilution ) , probed with antibodies , and visualized by dab colorimetric reaction . 
for development of the virp score , the continuous response parameter relative tumor size was used as outcome , whereas the other clinically used response parameters pcr and rcb were used for evaluation of predictive performance . 
relative importance of each model variable was assessed using the r - package relaimpo23 with metrics lmg . virp scores based on mrna data in the neoava and promix study were computed using the intercept and beta - coefcients determined from the protein data in the neoava study . 
the corresponding surrogate mrna scores were determined using quantile - normalized and probeaveraged mrna expressions from the genes corresponding to the proteins in the original protein signature , including the phosphoproteins . results protein prole of tumors before treatment using unsupervised hierarchical clustering on the expression of the 210 proteins in all 109 tumors collected prior to treatment , they cluster into groups signicantly related to tumor shrinkage and to pam50 subtypes , with most estrogen receptor ( er ) - negative patients ( 17 of 21 ) localizing in a separate subcluster ( appendix fig a4 )  . univariate spearman correlation analysis of protein expressions related to relative tumor size visualized by the nonvariable - dependent rst principal component demonstrated a positive yet limited relationship between the two treatment arms , with expression of almost half of proteins ( n = 103 ) being inversely correlated with response . 
the number of proteins signicantly ( p , .05 unadjusted ) related to response was higher in the ctx treatment arm ( n = 54 ) than in the bev plus ctx arm ( n = 38 ) , with only ten in common and of which two had rho - values with opposite signs ( appendix fig a5 and appendix table a2 )  . development of a protein signature score predicting response to treatment with bev plus ctx addition of bevacizumab to standard treatment with chemotherapy demonstrated benet compared with chemotherapy alone , although not signicant ( appendix fig a2 )  . to develop a signature predicting response to treatment with bev plus ctx , protein expression in biopsies taken prior to treatment were used from patients with available relative tumor size after nat ( n = 54 )  . 
low - variance proteins are likely to have low predictive value , thus a certain level of variance in expression should be present in order for clinical markers to be applicable . 
we thus reduced the original panel of 210 proteins by plotting the variance in expression and demonstrated a mixed distribution ( appendix fig a3 ) where only members belonging mainly to the proteins with higher variance ( n = 114 ; appendix table a3 ) were considered for use in the adaptive lasso regression model . 
a second iterative round of lasso on this subset of ten proteins gave the nal intercept and beta coefcients , of which one was shrunk to zero giving a nal signature of nine proteins with corresponding beta coefcients . 
 protein signature predicts response to chemotherapy plus bevacizumab the virp score for each patient was calculated as the sum of the intercept and beta coefcient weighted expression of the nine proteins . 
in univariate analysis , only the virp score , both as a continuous value and dichotomized ( low v high ) , was signicantly associated with pcr ( table 2 )  . 
no signicant association was found for tumor stage , pam50 subtypes , age , pgr , tp53 mutation , and nodal or er status . we next sought to establish and evaluate the corresponding mrna expression score as a surrogate to the virp protein score . 
by taking the corresponding genes from the virp ( including the parent protein for the phosphoprotein antibodies ) and using the predened lasso intercept and beta coefcients , the mrna score for the neoava patients ( mrna virp scores ) was calculated . 
this demonstrated a signicant increase , approximately doubling , in the percentage of both pcr responders ( p = .009 ) and low rcb ( p = .022 ) in the virp score selected patient population . 
use of the virp score for selecting patients to bev plus ctx demonstrated a clear benet with an increased response both by pcr ( p , .001 ) and rcb ( p , .001 ) compared with standard ctx treatment ( fig 3 )  . discussion we have dened a protein signature score named virp for use in large her2 - negative primary bcs that identies good responders to nat with chemotherapy plus bevacizumab . 
use of the virp score for selection to bev plus ctx therapy signicantly enriches for patients responding 290 2021 by american society of clinical oncology to treatment ( pcr or rcb - low )  . 
importantly , the robustness of the virp score was conrmed through validation in an independent clinical cohort ( promix )  . the lasso regression method was used to select proteins for the virp score . 
however , in silico evaluation the virp proteins under stimulus of bevacizumab treatment links them to response on relevant biological processes ( appendix fig a7 )  . ranking the relative importance of each protein in the virp signature is interesting with respect to , for example , the potential to use each or selected proteins as biomarkers separately . 
it appears that the syk protein is of high importance ( appendix fig a8 ) , which also coincides with being the only protein in the signature differently expressed ( p = .002 ) in pcr versus non - pcr patients . 
the syk protein is enriched in immune cells , but also expressed in breast epithelium and endothelial cells where it plays a role in angiogenesis.26 when passing from protein to mrna expression , functional dimension of activating or deactivating phosphorylations is lost . 
this potentially inuences the performance of the mrna virp score when used as surrogate for the original protein score , and could partly explain the observed drop in auc for the roc analysis between the protein and mrna data sets in the neoava trial ( fig 2a and appendix fig a6a )  . 
spearman correlation between expression of all 210 assessed proteins and mrnas showed that of the nine proteins in the signature , the four with the lowest correlation were phosphorylated or extracellularly localized proteins . 
however , the signature members had a signicantly ( p = .039 ) higher correlation compared with all proteins in the original data set ( appendix fig a9 )  . 
although the neoava protein data set is too small to draw conclusions , a previous observation of nearly 10 , 000 proteins in bc showed that established prognostic mrna - centered signatures ( ie , pam50 - ror , oncotype dx , and mammaprint ) in general had higher protein - mrna correlation than average for the human genome.27 we propose that because of the closer relation proteins have to phenotype , biomarker signatures being developed to identify features with clinical , and thus phenotypical impact , will represent genes with high expressional and translational penetrance . in the neoava clinical trial , patient subgroups were divided based on er expression ( using 1% positivity as cutoff ) , and better response ( as assessed by pcr and rcb ) was in general observed for the er - negative group , whereas only the er - positive group had signicant benet of added in univariate analysis , er bevacizumab . 
this is also consistent with the discrepancy seen in large studies regarding the benet of added bevacizumab in the er - positive or er - negative subpopulations of patients.28 - 30 the relative higher number of proteins signicantly correlated with tumor size after treatment in the ctx arm ( n = 54 ) suggested that a similar protein signature predicting response to chemotherapy alone might be developed . however , use of adaptive lasso regression only returned a signature of two proteins with low predictive performance , and not represented in the bev plus ctx virp signature . use of the virp score developed for bev plus ctx treatment applied on the ctx patients did demonstrate a signicantly lower score in the limited number of patients with pcr ( n = 7 ) , but not when assessed for the low - rcb patients ( n = 14 )  . 
this does not exclude the possibility that the proteins in the virp signature also reect sensitivity to the baseline chemotherapy when combined with bevacizumab . bulk tumor samples may have variable tumor cell content , which might inuence the readout of mrna or proteinbased molecular signatures.31 inuence of tumor cell content ( median of 42% ) on the virp signature , or on its individual proteins , did not demonstrate any signicant associations in the bev plus ctx - treated patients ( appendix fig a11 )  . 
furthermore , the virp score should be related to the mechanism of action of the anti - vegf therapy , which involves normal tissue constituents and in particular endothelial cells and vessels.32 thus , a composite tissue is likely required for the score to function . 
 ( a ) fraction of patients obtaining pcr when treated with standard ctx in all neoava patients ( n = 55 ) or bev plus ctx in all neoava patients ( n = 54 ) and selected based on virp score ( n = 22 )  . 
 ( b ) fraction of patients obtaining low rcb ( 0 and i ) when treated with standard ctx in all neoava patients ( n = 55 ) or bev plus ctx in all neoava patients ( n = 54 ) and selected based on virp score ( n = 22 )  . 
pcr , pathologic complete response ; rcb , residual cancer burden ; virp , vegf inhibition response predictor . 100% 100% random population ctx treatment ( low = 14 high = 41 ) random population bev plus ctx treatment ( low = 20 high = 34 ) virp selected population bev plus ctx treatment ( low = 15 high = 7 ) from treatment with bevacizumab in combination with chemotherapy.34 the virp score is predicting responses , but further studies are warranted to assess for impact on survival . although the discovered virp signature was established for patients treated with bev plus ctx in a neoadjuvant setting , it recapitulates biology related to treatment response and could have the potential to also predict response to bev plus ctx therapy in the metastatic setting . 
additionally , studies are initiated to investigate whether the virp signature recapitulates common response biology shared by other solid cancer types for which bevacizumab in combination with chemotherapy is commonly used.35 affiliations 1department of tumor biology , institute for cancer research , division of cancer medicine , oslo university hospital , the norwegian radium hospital , oslo , norway 2department of genetics , institute for cancer research , division of cancer medicine , oslo university hospital , the norwegian radium hospital , oslo , norway 3department of informaticsbiomedical informatics , university of oslo , oslo , norway 4k.g. 
mills , olav engebraaten provision of study materials or patients : ingrid hedenfalk , elin borgen , niklas loman , thomas hatschek , anne - lise brresen - dale , bjrn naume , gordon b . 
mills , olav engebraaten manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors thomas hatschek consulting or advisory role : roche , pzer , pierre fabre research funding : roche , pzer travel , accommodations , expenses : roche anne - lise brresen - dale employment : arctic pharma as , pubgene stock and other ownership interests : arctic pharma as gordon b . 
mills stock and other ownership interests : catena , signalchem , tarveda therapeutics , immunomet honoraria : nuevolution : astrazeneca , tarveda therapeutics , tesaro , symphogen , pdx pharmacy , immunomet , lilly consulting or advisory role : astrazeneca , signalchem , tarveda therapeutics , symphogen , takeda / millennium , pdx pharmacy , immunomet , lilly , turbine , ion pharma , zentalis research funding : adelson medical research foundation , astrazeneca , nanostring technologies , breast cancer research foundation , karus therapeutics , pzer , prospect creek foundation , tarveda therapeutics , ions pharmaceuticals , immunomet patents , royalties , other intellectual property : hrd assay to myriad genetics , dsp technology patent with nanostring travel , accommodations , expenses : astrazeneca , pzer , symphogen , chrysalis biomedical advisors , immunomet , michigan primary care consortium gunhild m . 
mlandsmo patents , royalties , other intellectual property : patent application submitted for a nine - protein / gene panel predicting response to anti vegf therapies in combination with chemotherapy olav engebraaten patents , royalties , other intellectual property : patent application pending for a biomarker for antibody drug conjugates , patent application submitted for a nine - protein / gene panel predicting response to anti vegf therapies in combination with chemotherapy no other potential conicts of interest were reported . references folkman j : anti - angiogenesis : new concept for therapy of solid tumors . 
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maru d , venook ap , ellis lm : predictive biomarkers for bevacizumab : are we there yet ? clin cancer res 19 : 2824 - 2827 , 2013 gampenrieder sp , westphal t , greil r : antiangiogenic therapy in breast cancer . 
miles d , cameron d , bondarenko i , et al : bevacizumab plus paclitaxel versus placebo plus paclitaxel as rst - line therapy for her2 - negative metastatic breast cancer ( meridian ) : a double - blind placebo - controlled randomised phase iii trial with prospective biomarker evaluation . 
eur j cancer 70 : 146 - 155 , 2017 janning m , m uller v , vettorazzi e , et al : evaluation of soluble carbonic anhydrase ix as predictive marker for efcacy of bevacizumab : a biomarker analysis from the geparquinto phase iii neoadjuvant breast cancer trial . 
fasching pa , loibl s , hu c , et al : brca1 / 2 mutations and bevacizumab in the neoadjuvant treatment of breast cancer : response and prognosis results in patients with triple - negative breast cancer from the geparquinto study . 
ali m , khan sa , wennerberg k , et al : global proteomics proling improves drug sensitivity prediction : results from a multi - omics , pan - cancer modeling 13 . 
silwal - pandit l , nord s , von der lippe gythfeldt h , et al : the longitudinal transcriptional response to neoadjuvant chemotherapy with and without bevacizumab 8 : 2278 - 2288 , 2018 approach . 
h oglander ek , nord s , wedge dc , et al : time series analysis of neoadjuvant chemotherapy and bevacizumab - treated breast carcinomas reveals a systemic shift in genomic aberrations . 
lu y , ling s , hegde am , et al : using reverse - phase protein arrays as pharmacodynamic assays for functional proteomics , biomarker discovery , and drug development in cancer . 
robin x , turck n , hainard a , et al : proc : an open - source package for r and s + to analyze and compare roc curves . 
loibl s , denkert c : how much information do we really need after neoadjuvant therapy for breast cancer ? j clin oncol 35 : 1029 - 1030 , 2017 25 . 
kazerounian s , duquette m , reyes ma , et al : priming of the vascular endothelial growth factor signaling pathway by thrombospondin - 1 , cd36 , and spleen subtype . 
nat commun 10 : 1600 , 2019 von minckwitz g , eidtmann h , rezai m , et al : neoadjuvant chemotherapy and bevacizumab for her2 - negative breast cancer . 
earl hm , hiller l , dunn ja , et al : efcacy of neoadjuvant bevacizumab added to docetaxel followed by uorouracil , epirubicin , and cyclophosphamide , for women with her2 - negative early breast cancer ( artemis ) : an open - label , randomised , phase 3 trial . 
garcia j , hurwitz hi , sandler ab , et al : bevacizumab ( avastin ( r ) ) in cancer treatment : a review of 15 years of clinical experience and future outlook . 
robert nj , di eras v , glaspy j , et al : ribbon - 1 : randomized , double - blind , placebo - controlled , phase iii trial of chemotherapy with or without bevacizumab for rst - line treatment of human epidermal growth factor receptor 2 - negative , locally recurrent or metastatic breast cancer . 
delaloge s , p erol d , courtinard c , et al : paclitaxel plus bevacizumab or paclitaxel as rst - line treatment for her2 - negative metastatic breast cancer in a multicenter national observational study . 
 protein signature predicts response to chemotherapy plus bevacizumab appendix patients assigned to treatment with chemotherapy with or without bevacizumab ( n = 138 ) patients randomly assigned to chemotherapy ( ctx ) ( n = 67 ) patients randomly assigned to chemotherapy and bevacizumab ( bev plus ctx ) ( n = 71 ) ineligible ( n = 1 ) ineligible ( n = 2 ) discontinued treatment ( n = 2 ) patients included in primary endpoint analysis ( n = 66 ) patients included in primary endpoint analysis ( n = 66 ) start of treatment ( n = 55 ) start of treatment ( n = 54 ) fig a1 . 
mixed distribution of protein expression variances ( solid green and blue lines ) ; only proteins with variance above intersection ( red line ) were selected for input in lasso regression to determine the virp ( appendix table a3 )  . 
 protein signature predicts response to chemotherapy plus bevacizumab relative tumor size ( p = .003 ) bevacizumab ( p = .815 ) pam50 ( p < .001 ) bevacizumab relative tumor size pam50 basal her2 luma lumb normal 150% fig a4 . 
rho - values derived from the spearman correlation of protein expression to relative tumor size for patients receiving the bev plus ctx combination ( x - axis ) and ctx treatment only ( y - axis ) with rst principal component of relation between the treatment arms ( stitched red line )  . 
in silico simulation with ingenuity pathway analysis ( version 47547484 , qiagen ) was used to predict biologic effects ( lower row ) affected by the virp member proteins ( second bottom row ) when inuenced by bevacizumab treatment ( top row ) through a set of intermediate proteins ( second top row )  . 
 ( c ) virp scores in rcb low ( 0 and i ) and high ( ii and iii ) patients . ( d ) fraction of patients obtaining pcr when treated with standard ctx in all neoava patients ( n = 55 ) or selected based on virp score ( n = 17 )  . 
 ( e ) fraction of patients obtaining low rcb ( 0 and i ) when treated with standard ctx in all neoava patients ( n = 55 ) or selected based on virp score ( n = 17 )  . 
 o validating comprehensive nextgeneration sequencing results for precision oncology : the nct / dktk molecularly aided stratification for tumor eradication research experience amelie lier roland penzel christoph heining peter horak martina frhlich sebastian uhrig jan budczies martina kirchner anna - lena volckmar barbara hutter simon kreutzfeldt volker endris daniela richter stephan wolf katrin pftze olaf neumann ivo buchhalter cristiano m . 
rieke ( continued ) purpose rapidly evolving genomics technologies , in particular comprehensive next generation sequencing ( ngs ) , have led to exponential growth in the understanding of cancer biology , shifting oncology toward personalized treatment strategies . 
2018 by american society of clinical oncology precision oncology and next - generation sequencing precision oncology is based on a profound understanding of tumor biology through comprehensive molecular profiling that can be leveraged to predict response to specific cancer therapies . 
contributed equally to this work . corresponding author : albrecht stenzinger , md , institute of pathology , heidelberg university hospital , im neuenheimer feld 224 , 69120 heidelberg , germany ; e - mail : albrecht . 
 range from the focused sequencing of hotspot regions to whole - exome sequencing ( wes ) / whole - genome sequencing ( wgs ) as well as total rna sequencing ( rna - seq )  . 
whereas the targeted panel sequencing of selected cancer related genes and genomic regions has been widely adopted in routine molecular diagnostics at many institutions worldwide , 1 , 4 - 7 comprehensive molecular profiling in a clinical setting is currently only performed at dedicated centers ; however , as sequencing costs continue to drop and new actionable targets continuously emerge , comprehensive ngs will be increasingly used with clinical intention . 
 request form 4 - 6 work days sample acquisition ( tissue sectioning , h&e staining , biobanking ) histopathologic diagnosis ( tumor cell content ) request form 8 - 14 work days target validation ( sanger sequencing , fish , ihc ) wes / wgs / rna - seq ( target identification ) 15 work days tumor board ( target identification , clinical interpretation , treatment recommendations ) personalized cancer treatment fig 1 . 
 fish , fluorescence in situ hybridization ; h&e , hematoxylin and eosin ; ihc , immunohistochemistry ; rna - seq , rna sequencing ; wes , whole - exome sequencing ; wgs , whole - genome sequencing . study at the following german cancer centers : nct heidelberg , nct dresden , university hospital heidelberg , university hospital dresden , university hospital munich , charit comprehensive cancer center , charit university hospital berlin , comprehensive cancer center tbingen , university hospital tbingen , university hospital freiburg , university cancer center frankfurt , university cancer center mainz , west german cancer center , and university hospital essen . samples were pseudonymized , and tumor histology , including tumor cellularity , was reviewed and assessed for all cases according to current who criteria by the iph before additional processing . 
of the 220 patients , 77.5% were younger than age 51 years ( fig 2b ) , 49% were registered for the master program within the first 2 years after diagnosis ( fig 2c ) , and the male - to - female ratio was close to 1 ( fig 2d )  . 
patients with bone and soft tissue sarcomas represented the largest subgroup ( 24.9% ) of the 220 patients and together with patients with cancer of unknown primary ( 6.6% ) , skin cancer ( 8% ) , neuroendocrine tumors ( 8% ) , and breast cancer ( 6.6% ) accounted for 54.1% of the validation cohort ( fig 2e )  . 
as shown in figure 2f , the number of validation requests increased over time as a result of the extension of the master program to nine additional referring centers within the german cancer research center in march 2016 . validation statistics a total of 349 genetic alterations , which corresponded to an average of 1.6 alterations per patient , were subjected to molecular pathology validation with a mean turnaround of 10 working days ( range , 1 to 24 days ) to avoid delays in reporting and genomics - guided clinical management . 
validation was performed after review of wes and rna - seq data and in parallel to additional clinical work - up of the cases , which takes place before discussion in the mtb . 
af , allele frequency ; amp , amplification ; cup , cancer of unknown primary ; del , deletion ; fus , gene fusion ; ins , insertion ; oex , overexpression . was requested is shown in the data supplement . 
 for validation requests and validation reports , a quality - controlled standard operating procedure and specific forms were established to ensure a standardized flow of information that provides clear and unambiguous results . 
the request form has a mandatory requirement for the following data : request date , patient identifier , tumor type as defined by histopathologic analysis , full name and affiliation of the requesting physician , and a precise description of the target of interest identified by comprehensive ngs , including official gene name , refseq ( national center for biotechnology information ) , human genome version used for alignment ( eg , hg19 [ grch37 ] ) , chromosome , position of the alteration , type of alteration , allele frequency , and annotations on the cdna and protein level . 
to validate fusion genes , the fusion sequence as well as the 5 and 3 fusion partnerschromosome , position , and exonneed to be stated . nonsynonymous snvs were the most frequently requested alterations ( n = 241 ; 69.1% ) , followed by gene fusions ( n = 44 ; 12.6% ) , small indels ( n = 41 [ 31 deletions and 10 insertions ] ; 11.8% ) , gene amplifications ( n = 10 ; 2.9% ) , and overexpression ( n = 13 ; 3.7% ) of the corresponding protein products ( fig 3b )  . 
a more detailed analysis of the nine snvs that were detected by wes that were not confirmed by sanger sequencing revealed that seven ( 77.8% ) showed allele frequencies of less than 10% ( as low as 5% ) , whereas two ( 22.2% ) showed allele frequencies ( 22% and 27% ) above the lod of sanger sequencing , which indicated other causes underlying the discrepant results . 
 among the patients with discordant validation results , bone and soft tissue sarcoma ( 23.3% ) , cancer of unknown primary ( 16.7% ) , pancreatic adenocarcinoma ( 16.7% ) , and neuroendocrine fig 4 . 
as validation efforts were focused on specific mutations of individual genes and did not involve complex biomarkers , such as high tumor mutational burden ( tmb ) , which represents the most common genetic rationale for assigning patients to immunotherapy , validation requests in the ie basket were infrequent ( 0.9% ; fig 4a ) and mainly related to alterations of cd274 ( also called pd - l1 )  . 
 discussion here , we describe the systematic validation of clinically actionable genetic lesions that were detected by combined wes and rna - seq within a multi - institutional precision oncology progra to our knowledge , this study reports on the largest clinically affiliated program worldwide that systematically validates actionable genetic lesions in tumors that are detected by comprehensive ngs . 
whereas some studies on the value of sanger sequencingbased validation of germline - derived ngs data sets and ngs assays that are in use for hereditary cancer testing challenged the need for independent validation approaches , 19 , 23 , 24 our results not only underscore the need for validation of ngs assays for the interrogation of tumor tissue in a clinical setting , but also highlight the value of orthogonal methods for guiding the development of bioinformatics pipelines , 19 , 25 - 27 which are a critical cornerstone and determinant of any ngs result . 
in contrast , the ie basket , with its major biomarkers tmb and pd - l1 amplification / expression , is underrepresented , because validations were confined to single genetic aberrationsfor example , pd - l1 amplification / overexpression and did not include tmb . when comprehensive ngs entered the clinical arena more than 5 years ago , 28 - 31 our understanding of the pros and cons of ngs technology was still evolving . 
it was noted that , compared with sanger sequencing , ngs platforms can have a generally lower quality per base , which results in decreased specificity and sensitivity.17 - 19 it became evident that many parameters , including tumor cellularity , coverage , read depth , and lod thresholds for variant calling , influence clinical - grade ngs results . 
in our study , validation is defined as testing of genetic aberrations identified by wes and rna - seq by orthogonal methods in a running molecular profiling progra sequencing in master is carried out at the german cancer research center , and results are validated by the center for molecular pathology6 , 32 at the iph . 
whereas comprehensive sequencing is performed on a research - grade level , validation of putative targets is performed in a laboratory for molecular diagnostics that is regularly audited by the german accreditation agency33 and that leads and participates in nationwide round robin trials5 of the quality assurance initiative pathology.34 this dual and complementary approach ensures clinical - grade diagnostics . more than 90% of clinically actionable genomic alterations identified by combined wes and rna - seq were successfully validated with an imas of 0.93 , which demonstrates the high concordance that can be reached within a multi institutional comprehensive ngs program and indicates the importance of an implemented validation step within the workflow . the combination of wes and rna - seq can also yield information on gene fusions and associated transcript levels ; however , this approach must be coupled with data analysis tools that provide sufficient sensitivity and specificity to minimize the risk of false - negative or false - positive results.35 , 36 in the context of the current study , the implementation of a new computational strategy for gene fusion detection in 2016 ( com / suhrig / arriba ) substantially improved sensitivity and specificity , and the concordance rate for gene fusion detection increased to greater than 95% with an imas of 0.96 , which equaled the high imas of snv calling results . systematic re - evaluation of histopathologic diagnosis and tumor cellularity revealed that 25% of patients had insufficient tissue quantity and / or quality . 
first , whereas mathematical modeling predicts that most cancers harbor five to eight driver mutations in their genome , 38 the clinical utility of genetic lesions is governed by the number and type of drugs that are currently available . 
as a consequence , on average , 1.6 alterations per patient are currently subjected to validation in the master program , representing the druggable subset of putative biologically relevant genetic lesions per tumor . 
second , although our approach allows for the analysis of concordance levels between gold standard methods and ngs , the data set is not suited to calculate sensitivity and specificity . 
although an experienced observer may still recognize the variant of interest in an optimal settingthat is , low background noise because of high dna quality or low nontumor contaminationone evidently operates at sensitivity limits . 
conversely , comprehensive sequencing approaches , such as wes , also have inherent limitations when it comes to the coverage of genes and read depth per locus , which can become particularly challenging in the context of genetic heterogeneity and tumor evolution . 
 our approach not only aids clinical decision making on the basis of molecular tumor profiles and helps to optimize bioinformatics pipelines and sequencing protocols , but will also serve as a solid reference in the field . 
whereas overall concordance rates between wes and rna - seq and orthogonal methods are high , low abundant variants remain challenging and should be verified by independent methods , ideally by targeted ngs . 
finally , influenced by our study results , we have now implemented combined wgs and rna - seq to further enhance the detection of gene fusions and to analyze intronic regions for putative cancer drivers . 
our validation approach enables the continuous monitoring of results and associated test parameters for maintenance and for the identification of weak spots of a given assay which may require improvement . 
thus , this program does not replace but complements validation measures that were taken before the use of the assay in a clinical setting . next to ngs of dna and rna , it is foreseeable that additional omics approaches will enter the clinic to capture the entire spectrum of epigenetic , proteomic , and metabolic adaptations that cancers use to facilitate growth and metastatic spread . 
 data analysis and interpretation : amelie lier , christoph heining , martina frhlich , sebastian uhrig , jan budczies , barbara hutter , volker endris , olaf neumann , ivo buchhalter , cristiano m . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . amelie lier no relationship to disclose roland penzel no relationship to disclose christoph heining no relationship to disclose peter horak honoraria : astellas pharma martina frhlich no relationship to disclose sebastian uhrig no relationship to disclose travel , accommodations , expenses : astellas pharma jan budczies patents , royalties , other intellectual property : patent application ep1806413a1 ( inst ) , patent application wo2010076322a1 ( inst ) martina kirchner no relationship to disclose anna - lena volckmar consulting or advisory role : astrazeneca barbara hutter no relationship to disclose simon kreutzfeldt consulting or advisory role : novartis , boehringer ingelheim travel , accommodations , expenses : pfizer , boehringer ingelheim , pharmamar , novartis volker endris honoraria : astrazeneca , thermo fisher scientific consulting or advisory role : novartis , pfizer daniela richter no relationship to disclose stephan wolf no relationship to disclose katrin pftze no relationship to disclose olaf neumann no relationship to disclose ivo buchhalter no relationship to disclose cristiano m . 
morais de oliveira no relationship to disclose stephan singer no relationship to disclose jonas leichsenring honoraria : astrazeneca expert testimony : astrazeneca esther herpel no relationship to disclose frederick klauschen no relationship to disclose philipp j . 
jost honoraria : novartis , bristol - myers squibb consulting or advisory role : novartis research funding : boehringer ingelheim ( inst ) , abbvie ( inst ) klaus h . 
the authors thank the german cancer research center ( dkfz ) heidelberg center for personalized oncology ( hipo ) and nct precision oncology program ( pop ) sample processing laboratory , the dkfz genomics and proteomics core facility , and the dkfz - hipo data management group for technical support and expertise . 
the authors also thank roland eils for providing the bioinformatics infrastructure within dkfz - hipo . affiliations amelie lier , roland penzel , peter horak , jan budczies , martina kirchner , anna - lena volckmar , simon kreutzfeldt , volker endris , olaf neumann , ivo buchhalter , cristiano m . 
morais de oliveira , christof von kalle , peter schirmacher , stefan frhling , and albrecht stenzinger , german cancer consortium , heidelberg ; christoph heining , daniela richter , and hanno glimm , national center for tumor diseases dresden ; christoph heining , evelin schrck , gunnar folprecht , and hanno glimm , technische universitt dresden ; christoph heining , daniela richter , evelin schrck , gunnar folprecht , and hanno glimm , german cancer consortium ; gunnar folprecht , university hospital , dresden ; frederick klauschen , charit university hospital ; frederick klauschen and mario lamping , german cancer consortium ; damian t . 
h021 from german cancer research centerheidelberg center for personalized oncology and national center for tumor diseases precision oncology program . support references 30 : 293 - 303 , 307 , 2016 1 . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
endris v , stenzinger a , pfarr n , et al : ngs - based brca1 / 2 mutation testing of high - grade serous ovarian cancer tissue : results and conclusions of the first international round robin trial . 
czink e , heining c , weber tf , et al : durable remission under dual her2 blockade with trastuzumab and pertuzumab in a patient with metastatic gallbladder cancer [ in german ]  . 
grschel s , bommer m , hutter b , et al : integration of genomics and histology revises diagnosis and enables effective therapy of refractory cancer of unknown primary with pdl1 amplification . 
kordes m , rring m , heining c , et al : cooperation of braf ( f595l ) and mutant hras in histiocytic sarcoma provides new insights into oncogenic braf signaling . 
barbano r , pasculli b , coco m , et al : competitive allele - specific taqman pcr ( cast - pcr ) is a sensitive , specific and fast method for braf v600 mutation detection in melanoma patients . 
rennert h , eng k , zhang t , et al : development and validation of a whole - exome sequencing test for simultaneous detection of point mutations , indels and copy - number alterations for precision cancer care . 
roy s , coldren c , karunamurthy a , et al : standards and guidelines for validating next - generation sequencing bioinformatics pipelines : a joint recommendation of the association for molecular pathology and the college of american pathologists . 
jennings lj , arcila me , corless c , et al : guidelines for validation of next - generation sequencingbased oncology panels : a joint consensus recommendation of the association for molecular pathology and college of american pathologists . 
wagle n , berger mf , davis mj , et al : high - throughput detection of actionable genomic alterations in clinical tumor samples by targeted , massively parallel sequencing . 
christopoulos p , endris v , bozorgmehr f , et al : eml4 - alk fusion variant v3 is a high - risk feature conferring accelerated metastatic spread , early treatment failure and worse overall survival in alk + non - small cell lung cancer . 
carrara m , beccuti m , cavallo f , et al : state of art fusion - finder algorithms are suitable to detect transcription - induced chimeras in normal tissues ? bmc bioinformatics 14 : s2 , 2013 ( suppl 7 ) 36 . 
leichsenring j , volckmar al , kirchner m , et al : targeted deep sequencing of effusion cytology samples is feasible , informs spatiotemporal tumor evolution , and has clinical and diagnostic utility . 
dignam , phd2 in this precision oncology era , where molecular proling at the individual patient level becomes increasingly accessible and affordable , more and more clinical trials are now driven by biomarkers , with an overarching objective to optimize and personalize disease management . 
as compared with the conventional clinical development paradigms , where the key is to evaluate treatment effects in histology - dened populations , the choices of biomarker - driven clinical trial designs and analysis plans require additional considerations that are heavily dependent on the nature of biomarkers ( eg , prognostic or predictive , integral or integrated ) and the credential of biomarkers performance and clinical utility . 
here we provide a concise overview of design options for both the setting of singlebiomarker / single - disease and the setting of multiple - biomarker / multiple - disease types . 
we focus on explaining the trial design and practical considerations and rationale of when to use which designs , as well as how to incorporate various adaptive design components to provide additional exibility , enhance logistical efciency , and optimize resource allocation . 
2019 by american society of clinical oncology introduction in the past 10 to 15 years , cancer clinical trials have experienced some important paradigm changes to embrace the era of precision oncology as dened by various biomarkers . 
the central hypothesis driving this movement is that by integrating the right biomarker information we can properly select , or at least enrich , trial cohorts for patients who are most likely to benet from a particular therapy . 
multiple factors collectively contribute to this movementour knowledge about oncogenic pathways has been greatly advanced ; highthroughput screening and other drug discovery developments have made a lot more candidate agents available for evaluation ; and the rapid development of various omics - based technologies , especially the increasing availability of next - generation genomic sequencing , makes it more feasible and affordable to incorporate biomarker information into clinical trials . 
all of these call for novel biomarker - driven trial designs to expedite the clinical development of multiple treatment agents and newly dened patient populations . in this review , we use biomarker to generically describe any characterizations of biologic molecules or diagnostic tests carried out on dna , rna , proteins , and metabolites from blood , body uids , or tissues for diagnosis purposes including disease conrmation , staging , subtyping , and so on . 
under this working denition , the presence of some actionable mutation , such as a mutation in epidermal growth factor receptor ( egfr ) measured at the protein level , is viewed as a single biomarker ; a dna - based multiplex genotyping that simultaneously determines multiple actionable mutations such as egfr , kras , or eml4 - alk is viewed as multiple biomarkers . treatment benet compared with the traditional paradigm , there are even greater consequences of asking the right questions ( or wrong questions ) in these biomarker - driven clinical trials . 
for example , although often there is good biologic rationale to consider biomarker - negative ( m - negative ) patients unlikely or less likely to benet from the new ( targeted ) therapy , the clinical evidence of whether is conned only in the potential biomarker - positive ( m - positive ) patients may or may not be strong . 
moreover , the development of a validated companion biomarker , including establishing a widely accepted partition or cutoff value to determine whether the biomarker is positive or negative , is sometimes lagging behind the development of novel therapeutic agents . 
 hu and dignam context key objective in the past few decades , clinical trials have experienced a major paradigm shift , aiming to incorporate ever - growing tumor biomarker information and evaluate biomarker - dened patient cohorts , while accelerating the clinical development process simultaneously . 
what are the key considerations when designing and conducting biomarker - driven clinical trials ? knowledge generated we present an overview of the rationale , trial types , key design elements and features , and practical considerations for commonly used biomarker - driven clinical trials . 
examples of trials conducted and the lessons learned are also presented . relevance when properly designed and implemented with adequate resources , biomarker - driven clinical trials may efciently and effectively generate evidence on biomarker - based personalized disease management . 
clinicians and clinical trialists should think thoroughly and critically if and how to design and conduct these trials . properly tailor the trial designs and prioritize research questions on the basis of the development stage of the biomarker and the credentials of its clinical utility . the demand for trial development and conduct has become more daunting than ever , as high - throughput molecular proling becomes more accessible . 
rather than mounting separate trials , an important paradigm shift to expedite clinical development is to establish the so - called master protocol or platform triala program of trial development and conduct implemented with an up - front molecular screen and enrollment infrastructure into subtrials across multiple biomarkers and / or multiple disease typesto enhance logistic and regulatory efciency . some important and useful concepts in development of biomarkers for clinical utility are rst briey introduced here and expanded on in the next sections . 
throughout this review , we assume biomarkers of interest already have good analytical validity ( eg , they can be accurately , reliably , and reproducibly measured ) .1 , 2 a biomarker is called prognostic if it is associated with disease prognosis regardless of treatment type and is called predictive when it exerts prognostic inuence differentially according to different treatments . 
it is desirable to have a biomarker ( either prognostic or predictive ) with good clinical utility ( ie , the biomarker can reliably prompt clinical actions that benet patients )  . 
according to dancey et al , 3 biomarkers are integral when they are inherent in the study design from the onset and must be performed in real time to establish eligibility , identify the correct stratum for stratied enrollment , or assign treatment . 
in other words , to make a biomarker usable for clinical trial setting , an integral biomarker should be fully developed and validated ( eg , the cutoff that dichotomizes the continuous marker measurement is xed ) , with a rapid assay turnaround time . 
fast assay turnaround time is desirable but not required for integrated biomarkers . to design more efcient trials and overcome the aforementioned challenges , the idea of adaptive designs has been promoted , and aspects of this approach play an important role in virtually all existing biomarker - driven trials . although modern oncology trial design has promoted adaptive designs as a new aspect of clinical trials , we note that adaptive elements have played a long - standing role in oncology clinical trials , dating back to early multistage design concepts4 , 5 and continuing in the rich development of group sequential monitoring methods that permit early efcacy or futility stopping.6 also , both traditional and newer phase i oncology trial designs are by their nature adaptive to accumulating data . 
we will discuss the rationale and features of established as well as newer adaptive design elements as they arise in respective biomarker - driven trial designs . finally , a new nomenclature that generally describes trial constructs has been introduced , attempting to describe heuristically the structure , particularly when multiple biomarkers and / or treatment agents are considered . 
the term basket trial refers to a trial with an agent tested among multiple disease types sharing a common molecular feature or target identied by biomarker ( s )  . 
in contrast , an umbrella trial describes the case where , for a common disease entity , multiple agents may be investigated in conjunction with specic molecular targets and biomarkers . 
we note that all of these terms lack precision , and thus the specic study features will provide more detail as to the structure . this article aims to provide a concise and up - to - date overview on the current status of biomarker - driven clinical trials , with a focus on the underlying design considerations , rationale , and lessons learned . 
we organize these discussions in terms of the biomarkers role ( integral v integrated ) , number of biomarkers involved ( one v multiple ) , and trial objective ( conrmatory v discovery )  . 
interim monitoring , including but not limited to group sequential methods , provides the statistical framework to allow repeated assessments of treatment efcacy and early stopping as soon as the accumulated data already provide adequate evidence to conclude that the experimental regimen is highly likely ( efcacy monitoring ) or unlikely ( futility monitoring ) benecial . 
for example , phase ii trials traditionally have implemented a single - arm , noncomparative design , with a planned interim futility analysis , such as simons two - stage design , 7 to minimize patient exposure to ineffective regimens . 
in the late - phase setting , integrated randomized phase ii / iii design8 is a useful adaptive design that combines both screening ( phase ii component ) and conrmatory ( phase iii component ) in a single trial . 
as the data based on the the overall phase ii component are used to provisionally test the study hypothesis of the phase iii component , integrated phase ii / iii designs can effectively be viewed as phase iii studies with rather aggressive ( ie , likely to stop ) interim futility analyses . if more than one experimental regimen is of interest in the phase ii component , a plan of selecting treatment arms can also be incorporated when making the go / no - go decision from phase ii to phase iii . more formally speaking , adaptive designs are those that allow prospectively planned modications in both the statistical and scientic aspects of study designs , on the basis of accumulating data while the trials are still progress.9 adaptations to the statistical aspects of study designs arise when the primary estimand ( eg , the target of estimation ) addressing the scientic question of interest10 remains unchanged ; examples include group sequential designs , 6 sample size adaptation , 11 and , more recently ( although the concept dates back several decades ) , outcome / response - adaptive randomization.12 - 14 adaptations to the scientic aspects of study designs occur when the primary estimand does change ( eg , enriching patient population , or selecting new treatment arms or end points while the trial is still ongoing )  . 
among these adaptive design features , group sequential theorybased interim analysis and treatment assignment modication ( such as add or drop arms ) have been used most frequently , whereas other adaptive design features have not been widely adopted in practice . 
if the new agent is expected to have little effect on tumor shrinkage , or must be combined with an active agent , randomized phase ii screening designs17 with end points such as progression - free survival may be considered and provide valuable information on whether a conrmatory , randomized phase iii enrichment design should be performed . 
of note , although enrichment designs should be efcient ( a small sample size ) because we anticipate a large effect size , if the prevalence of mpositive patients is low , many patients must be screened to obtain the necessary sample size ; if the prevalence is too low , the trial may simply be infeasible . when there is strong evidence suggesting the biomarker is predictive with respect to the experimental regimen ( ie , m - positive patients benet ) , but it remains unclear whether the new treatment may also have a clinically meaningful ( but likely smaller ) benet for m - negative patients , the socalled biomarker - stratied design , which randomly assigns all patients with a valid marker result ( m - positive and m - negative ) as a stratication factor , can be considered ( fig 1b )  . 
one can also view this as an umbrella trial ( dened in a later section ) that contains two separate rcts for m - positive and m - negative subgroups . 
the key design consideration for conrmatory trials is if and how to prioritize the multiple hypotheses within the m - positive subgroup , the m - negative subgroup , or the overall population and properly power for each separately as applicable . 
 a biomarker - driven oncology clinical trial designs biomarker assay biomarker assay m - negative m - positive m - negative m - positive off study randomize randomize randomize standard rx new rx standard rx new rx standard rx new rx biomarker assay randomize biomarker assay nonmarkerbased strategy marker - based strategy marker subgroup 1 marker subgroup 2 marker subgroup 3 new rx randomize standard rx randomize new rx v standard rx standard rx m - negative , standard rx m - positive , new rx standard rx new rx fig 1 . 
m - negative , biomarker - negative ; m - positive , biomarker - positive ; rx , treatment . strategy can be considered by rst testing the m - positive subgroup at signicance level and then testing the m - negative subgroup at the same level if and only if the rst test is statistically signicant.20 an alternative approach to reect such prioritization is to split the overall unequally with a bonferroni correction ( eg , 1 = 0.04 and 2 = 0.01 for m - positive and m - negative , respectively )  . ( cid : 129 ) if the effect in the overall population is of secondary interest , the aforementioned sequential procedure needs to be modied , because the treatment effect of the overall population can still seem to be clinically meaningful even when the new treatment only works in the in the m - negative m - positive subpopulation but not subpopulation at all . 
to mitigate the potentially misleading conclusion that treatment works in all comers ( m - positive and m - negative ) , the marker sequential test design21 was proposed , which rst tests the m - positive subgroup at a reduced signicance level 1 ( , ) : if the test yields a statistically signicant result , the m - negative subgroup will be tested at level , whereas the overall population will be tested at 1 if the test among the m - negative subgroup is not signicant . ( cid : 129 ) if there is no convincing evidence suggesting a particular biomarker is predictive , a fallback strategy can be used , which rst tests the overall population at 1 ( , ) : if the result is signicant , one can claim that the treatment is effective in all patients ; if it is not signicant , then the m - positive population must meet 1 for signicance.22 although biomarker - stratied designs are typically used in the context of a conrmatory phase iii setting , randomized phase ii screening designs may still be considered if the overarching goal is to efciently inform whether to conduct a randomized phase iii enrichment design . 
when the primary interest is to evaluate whether the biomarker - based treatment assignment strategy is more effective than nonbiomarker - based treatment assignment strategy , one may consider a biomarker - strategy design , which randomly assigns all patients ( m - positive and m - negative ) to receive treatments either on the basis of or independent of biomarker status ( fig 1c )  . 
this design may also be used to evaluate whether the biomarker is predictive with some efciency loss , 16 , 23 because there can be a signicant portion of patients with the same biomarker status receiving the same treatments in both arms , reducing the treatment effect size that can realistically be specied . biomarker - directed design may be considered when it is desirable to have an integral biomarker evaluation for all patients , and there is compelling existing evidence suggesting a particular biomarker - dened subgroup should receive a certain regimen with satisfactory efcacy and safety proles ( fig 1d )  . 
in this case , like enrichment designs , a biomarker - directed design only randomizes the biomarker - dened subgroup where the biomarkers clinical utility in directing treatment decisions remains unclear ; meanwhile the other biomarker - dened subgroups are treated deterministically . 
for in tailorx ( program for the assessment of example , clinical cancer tests [ pacct - 1 ] : trial assigning individualized options for treatment ) , 24 patients with breast cancer treated with tamoxifen were classied as low , intermediate , and high risk on the basis of a 21 - gene recurrence score ( oncotype dx , genomic health , redwood city , ca )  . 
patients with intermediate risk were randomly assigned to receive hormonal therapy with or without chemotherapy , whereas lowrisk patients and high - risk patients always received only hormonal therapy with chemotherapy , respectively . in these conrmatory integral biomarker - driven trials , interim monitoring , especially futility monitoring , plays an even more critical role to help prioritize the limited resources by dropping subgroups with unpromising or unresponsive treatment benet and / or dropping ineffective experimental regimens if more than one is being investigated . 
for a biomarker classier that is based on a multiplex assay of genomic , proteomic , and transcriptomic data , the adaptive signature design29 was proposed to evaluate whether the experimental regimen is effective in the overall population or a subset of patients only while developing the biomarker classier simultaneously . 
if the treatment comparison for all patients is not signicant in the overall population at 1 ( , ) , we will either split all patients into training and testing subsets or use k - fold cross - validation30 to develop the biomarker and then evaluate efcacy in identied subgroups . 
of note , the cross - validated approach has also been shown to substantially improve the power of identifying the m - positive subgroup that benets from the new treatment . 
by transforming the multiple candidate genes to a binary classier , the approach does not suffer too much with respect to type i error control as the dimension of genes increases . 
when a biomarker or gene signature can be quantied on a continuous or ordinal scale , we can consider the biomarker - adaptive threshold design31 using a similar strategy to identify and validate an optimal cutoff point that separates m - positive and m - negative subgroups . the use of bootstrap resampling for estimation and inference of the threshold , although accounting for the multiplicity issue due to combining the tests for subgroup m - positive and overall population , has been shown to preserve the power to detect a global treatment effect while developing the biomarker . 
comparing with the conventional approaches , these methods have been shown to substantially improve the likelihood of detecting the mpositive subgroup when differential treatment effect does exist , especially when the prevalence of m - positive is low . 
for example , after the approval of vemurafenib for brafv600 mutation - positive metastatic melanoma , a nonrandomized phase ii basket trial of vemurafenib for multiple nonmelanoma cancers with brafv600 mutation was conducted , 33 with objective response as the primary end point . from a trial conduct perspective , basket trials can be more efcient than multiple histology - specic enrichment trials to carry out conducted separately and are convenient because the biomarker can ( although not necessarily ) be assessed locally at participating sites as part of the eligibility criteria screen . 
furthermore , this trial design can be quite appealing to patients because it conveniently provides access to the experimental therapy across multiple disease types , including in settings where our understanding of biomarker - treatment relationship is relatively limited . 
 molecular target a molecular target b molecular target y molecular target z targeted therapy a standard therapy targeted therapy b standard therapy targeted therapy y standard therapy targeted therapy z standard therapy biomarker - driven oncology clinical trial designs targeted therapy x tumor type a tumor type b tumor type y tumor type z biomarker assays phase iii continue to follow for definitive end point accrue additional n2 patients for definitive end point primary analysis treatment effect sufficiently large initiate phase ii trial phase ii accrue n1 patients assess stop insufficient ie activity promising ie activity run - in : randomization ( p1 = p2 ) randomization arm 1 ( p1 ) v arm 2 ( p2 ) assess interim estimate of treatment effect stop and conclude new rx better treatment effect not sufficiently large arm 1 better arm 2 better increase p1 decrease p2 increase p2 decrease p1 fig 2 . 
 hu and dignam from a scientic perspective , the underlying rationale of conducting a basket trial is that the biomarkers presence may independently predict responses attributed to the corresponding targeted therapy , regardless of histology or disease type.34 if this truly holds , it would be reasonable to redene cancer in a histology - agnostic fashion , suggesting an exciting new approach to therapy development . 
for example , in may 2017 , the us food and drug administration approved pembrolizumab for any patients with microsatellite instabilityhigh / decient dna mismatch repair regardless of histology.35 this approval was the rstever histology - agnostic indication and was partly based on a small , proof - of - concept basket trial.36 because basket trials may be viewed as a collection of enrichment trials , they also inherit all of the advantages and disadvantages , with the same practical considerations as elaborated earlier . 
one unique challenge facing basket trials is the balance between feasibility and the exchangeability ( eg , histology agnostic ) hypothesis , given the potential heterogeneity across different disease types . 
that is , if and when can we assume the molecular proling is sufcient to replace histology and pool patients together with the same biomarker ? for many biomarkers , prevalence is so low that it may be infeasible to accrue enough patients and analyze by each disease type . 
meanwhile , pooling all patients with the same biomarker can be questionable if not at all unrealistic , because the approach implies we can completely ignore the prognosis heterogeneity across different histology and assume disease subtype is not prognostic at all . 
in the case of vemurafenib for patients with brafv600 mutations , response to treatment was high when the primary site was melanoma but low when the primary site was colorectal cancer.33 a practical compromise is to combine some disease types for which prevalence is signicantly lower than others . 
in le et al , 36 patients with microsatellite instability high / decient dna mismatch repair were accrued and analyzed by colorectal and noncolorectal cohorts separately , because the prevalence in colorectal cancer is notably higher than other disease types . several novel adaptive designs have been developed to avoid separate analyses and properly share response information across disease types . 
one approach is based on preplanned interim analyses to determine the next steps.37 for example , if there is adequate evidence suggesting some histology - specic cohorts have similar and promising activities , these cohorts will be aggregated to allow more efcient statistical inference with fewer patients ; otherwise , histology - specic cohorts with exceptionally favorable response will remain separate , and cohorts with low responses will be terminated . 
the other approach is based on statistical modeling and bayesian inference , 38 , 39 which explicitly allows information sharing across different histology - specic cohorts and permits early stopping for some cohorts naturally on the basis of posterior probability of histology - specic response rates . 
nonetheless , it was argued that , for sample sizes typically used in phase ii trials and a reasonable number of cohorts / histology types under investigation , these designs that are meant to share information may not be as useful as one would hope , unless there is a strong rationale and evidence indicating uniform responses across cohorts.40 another important consideration when designing discovery basket trials is whether randomization should be used or not . 
the nonrandomized basket trial may be clearly preferred because of its feasibility and close connection to the conventional single - arm phase ii design traditionally used in early - stage development . 
however , nonrandomized basket design practically mandates objective response to be the only choice of the primary end point , because it is generally considered the only interpretable efcacy end point without a comparator . 
even with this end point , concerns may still arise regarding the relevance of historical control in at least some histology cohorts , because the biomarker likely denes a new disease subtype for which there is little or no historical information on prognosis.41 furthermore , if the experimental regimen is to be administered in combination with other active regimens , how to isolate the impacts of background treatments and properly the experimental regimens role can be chalinterpret lenging . 
in this case , because a centralized molecular screening platform is typically used , one may also view them as umbrella trials . from a pure statistical perspective , one could argue that basket trials may have multiplicity issues , because we simultaneously evaluate multiple histology - specic cohorts . pragmatically speaking , this may not be that problematic , because we are more tolerant of a higher type i error for discovery purposes ; the same issue also exists if we conduct separate trials for each cohort , and more practical concerns such as accrual feasibility often outweigh the type i error control . 
a randomized phase ii / iii trial example is alchemist ( adjuvant lung cancer enrichment marker identication and sequencing trial ) for resectable nonsmall - cell lung cancer ( nsclc ) , 42 , 43 which consists of three treatment subtrials , alchemistegfr for patients with egfr mutation ( clinicaltrials.gov identier : nct02193282 ) , alchemist - alk for patients with alk rearrangements ( clinicaltrials.gov identier : nct02201992 ) , and anvil ( clinicaltrials.gov identier : nct02595944 ) for unmatched patients ( eg , squamous histology , or nonsquamous histology and neither egfr mutation nor alk rearrangements )  . an observation cohort is also available for unmatched patients who refuse to participate in anvil . 
another prominent example is lung - map ( clinicaltrials.gov identier : nct02154490 ) , 44 which was initially for squamous lung cancer but recently was amended for all types of advanced nsclc . 
using sequential development features such as phase ii / iii designs and interim analyses that permit adaptation to ndings , these trials adaptively provide the necessary exibility for the umbrella trial objectives as a whole ( fig 2c )  . when there are multiple candidate regimens that are of interest equally for some or all biomarker cohorts , umbrella trials also can be designed solely for discovery objectives . 
for example , in the battle - 1 ( clinicaltrials.gov identier : nct00411632 , nct00409968 , nct00410059 , nct00410189 , nct00411632 , nct00411671 ) trial , patients with chemotherapy - refractory nsclc were assayed for four candidate biomarkers to be allocated to a total of ve marker strata ( including one nonmatched ) and then randomly assigned to one of four drug regimens.15 in nrglu003 ( clinicaltrials.gov identier : nct03737994 ) , an umbrella trial of previously treated patients with alk - positive lung cancer , a total of 10 marker cohorts ( including an unmatched cohort ) and up to seven new - generation alk inhibitors are to be evaluated . 
however , as the total number of possible drug - marker strata increases , the likelihood to accrue enough patients to have a reasonably accurate estimate of efcacy for each drug - biomarker stratum decreases . 
by exploiting the fact that biomarker allocation is not informative for treatment assignments , battle - 1 considered a learn - as - go approach by explicitly using a bayesian hierarchical probit model for information sharing , 45 along with outcome - adaptive randomization , 12 , 46 which allocates more patients to drug - marker strata that are more likely to have exceptional activities , to potentially provide individuals with more efcacious treatments and improve estimation precision ( fig 2d )  . 
in nrg - lu003 , for each biomarker the investigators are able to determine and prioritize the experimental regimens of interest on the basis of preclinical data , which substantially reduces the total number of drug - biomarker strata to be evaluated . 
freidlin and korn40 suggested that under typical phase ii trial design settings , both approaches may require similar resources . one implication of conducting umbrella trials is that an explicit rule governing how to match biomarkers and candidate regimens needs to be specied prospectively . 
therefore , umbrella trials also provide a unique opportunity to evaluate whether a rule - based policy that matches biomarkers and drugs is effective at all and , if so , to what extent across all genomic characterizations . 
to make such evaluation interpretable , the rule - based assignment policy should be as stable as possible during the trial conduct and ideally cover a wide range of biomarker - drug combinations.47 another unique consideration with umbrella trials is that a patient could be eligible for multiple biomarker cohort allocation because the tumor contains multiple biomarkers . 
with the emergent use of molecular proling , basket trials and umbrella trials , as well as extensions discussed here , can be collectively called master protocols or platform trials . 
more importantly , such a protocol provides substantial exibility in terms of discontinuing unpromising investigations , carrying forward favorable early results to denitive testing in a phase ii / iii framework , and introducing new subtrials as targets and agents are identied in a perpetual manner , using the aforementioned adaptive design methods for single - biomarker settings.48 in addition , the infrastructure advantages of conducting master protocols , such as centralized and streamlined trial conduct ( enrollment , informed consent ) , data collection , governance ( institutional review board , data and safety monitoring committee ) , and quality assurance ( clinical monitoring , imaging reading ) , are subtrials stantial as compared with conducting individual separately . 
when it was activated in 2015 , it started with 10 parallel biomarker - based cohorts to evaluate eight different in may 2016 , a preplanned feasibility interim analysis revealed that only 9% of patients had actionable mutations that could be matched with any of the multiple targeted therapies under investigation . 
the lower - than - expected matching success rate led to a major amendment to improve the overall matching rate by adding additional marker - specic cohorts.49 in june 2017 , when the original screening target was met ( n = 6 , 000 ) , it was found that the common molecular subtypes were rarer than expected.50 the study therefore underwent another major amendment by collapsing multiple subtype cohorts and relaxing the screening process . 
to date , the study remains open to accrual , with a total of 19 cohorts to evaluate 13 drugs.51 four lung - map was originally designed in 2014 for advanced squamous nsclc , consisting of targeted therapy subgroups and one nonmatched subgroup , each using a phase ii / iii seamless design , with progression - free survival and overall survival as primary end points , respectively.52 since 2015 , the treatment landscape of advanced nsclc has changed tremendously because of a series of approvals in immunotherapies especially for squamous and nonsquamous nsclc by the us food and drug administration , which fundamentally changed the standard of care and the study control arms . 
after multiple minor amendments for adding and closing biomarker - specic subtrials , in 2018 the study was completely revamped by expanding eligibility to all histology of advanced nsclc , using a new screening protocol and introducing new biomarker - dened subtrials.53 in summary , although conceptually offering efciency and exibility , master protocols are more prone to various factors that are unknown ( eg , low biomarker prevalence ) or cannot be foreseen ( eg , changing treatment landscape ) at the trial inilogistical tiation . 
these trials also come with substantial complications , especially when several sponsors are involved who may have conicting proprietary interests and regulatory concerns . discussion biomarker - driven clinical trials allow us to investigate patient heterogeneity on the basis of molecular proling , which consequently introduces new opportunities and challenges . 
comparing with the conventional paradigm , these trials require even more thorough planning and comprehensive evaluation on the overarching objectives ( discovery or conrmatory ) , the credential of biomarkers clinical utility , choice of adaptive design and analysis plans , knowledge of cancer biology , existing data from preclinical and early clinical trials , prevalence of each subtype population , logistic readiness to conduct immortal clinical trials , and so on . 
the success of any biomarker - driven trials therefore certainly relies on an even closer collaboration involved in advancing cancer care , including among all clinical investigators , statisticians , sponsors , regulators , drug and assay developers , and patient advocates . our discussions have been limited to phase ii and iii trial designs for discovery and conrmatory purposes . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . chen hu consulting or advisory role : merck sharp & dohme james j . 
j clin oncol 30 : 4223 - 4232 , 2012 pennello ga : analytical and clinical evaluation of biomarkers assays : when are biomarkers ready for prime time ? clin trials 10 : 666 - 676 , 2013 dancey je , dobbin kk , groshen s , et al : guidelines for the development and incorporation of biomarker studies in early clinical trials of novel agents . 
biometrics 38 : 143 - 151 , 1982 gehan ea : the determination of the number of patients required in a preliminary and a follow - up trial of a new chemotherapeutic agent . 
j chronic dis 13 : 346 - 353 , 1961 jennison c , turnbull bw : group sequential methods with applications to clinical applications - to - clinical - trials / jennison - turnbull / p / book / 9780849303166 simon r : optimal two - stage designs for phase ii clinical trials . 
clin cancer res 16 : 691 - 698 , 2010 jiang w , freidlin b , simon r : biomarker - adaptive threshold design : a procedure for evaluating treatment with possible biomarker - dened subset effect . 
freidlin b , korn el : borrowing information across subgroups in phase ii trials : is it useful ? clin cancer res 19 : 1326 - 1334 , 2013 41 . 
le - rademacher j , dahlberg s , lee jj , et al : biomarker clinical trials in lung cancer : design , logistics , challenges , and practical considerations . 
lih cj , sims dj , harrington rd , et al : analytical validation and application of a targeted next - generation sequencing mutation - detection assay for use in treatment assignment in the nci - mpact trial . 
peeters m , jay price tj , cervantes a : randomized phase iii study of panitumumab with uorouracil , leucovorin , and irinotecan ( folfiri ) compared with folfiri alone as second - line treatment in patients with metastatic colorectal cancer . 
herbst rs , redman mw , kim es , et al : cetuximab plus carboplatin and paclitaxel with or without bevacizumab versus carboplatin and paclitaxel with or without bevacizumab in advanced nsclc ( swog s0819 ) : a randomised , phase 3 study . 
spigel dr , ervin tj , ramlau ra , et al : randomized phase ii trial of onartuzumab in combination with erlotinib in patients with advanced non - small - cell lung cancer . 
bradley jd , paulus r , komaki r , et al : standard - dose versus high - dose conformal radiotherapy with concurrent and consolidation carboplatin plus paclitaxel with or without cetuximab for patients with stage iiia or iiib non - small - cell lung cancer ( rtog 0617 ) : a randomised , two - by - two factorial phase 3 study . 
vansteenkiste jf , cho bc , vanakesa t , et al : efcacy of the mage - a3 cancer immunotherapeutic as adjuvant therapy in patients with resected mage - a3positive non - small - cell lung cancer ( magrit ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
cobo m , isla d , massuti b , et al : customizing cisplatin based on quantitative excision repair cross - complementing 1 mrna expression : a phase iii trial in nonsmall - cell lung cancer . 
 c dramatic response to sequential braf inhibition in braf v600emutant metastatic lung adenocarcinoma introduction lung [ aq1 ] [ aq2 ] cancer is the leading cause of cancer related death.1 targeted therapy directed toward molecular pathways that drive nonsmall - cell lung cancer ( nsclc ) has dramatically improved treatment options . 
some of the oncogenic drivers identified in lung adenocarcinoma involve the ras - raf - mitogen - activated protein kinase ( mapk ) kinase ( mek ) - extracellular regulated kinase ( erk ) pathway ( mapk - erk pathway ) .2 braf is a key protein in mapk - erk signaling . 
 mutations in braf [ aq3 ] are present in 1% to 3% of nsclc and lead to constitutive activation of the mapk - erk pathway , promoting cancer cell proliferation and survival . 
several other mutations of braf have been identified and are grouped as non - v600e mutations.3 patients with nsclc harboring braf v600e mutations are sensitive to braf inhibitors ( brafis ) alone or in combination with mek inhibitors ( mekis ) .4 - 6 after initial response , patients typically experience relapse as a result of various resistance mechanisms . 
imaging revealed a left - side hilar lung mass , enlarged mediastinal lymph nodes , vertebral body sclerotic lesions , small bilateral pleural effusions , and a pericardial effusion consistent with metastatic disease . 
the repeat biopsy specimen was sent for massively parallel dna sequencing using the illumina hiseq2000 platform ( foundation medicine , cambridge , ma ) to characterize base substitutions , short insertions and deletions , copy number alterations , and selected fusions across 287 cancer - related genes . 
several tumor mutations , including braf v600e , mapk1 ( r306h ) , smad4 ( r361c ) , and setd2 ( splice site 65_71 + 13del20 ) , were identified . 
 a through lymphangitic spread ( fig 2 ) that required oxygen supplementation at 5 l / min and showed malignant involvement of the right - side iliopsoas muscle , which caused significant pa after palliative radiation to the right - side pelvic mass for pain control , he began a combination of dabrafenib 150 mg twice daily and trametinib 2 mg daily . 
at the same time , the patient became oxygen independent , and functional status improved , which allowed him to fulfill his desire to travel to his home country to visit family . more than 5 months later , after dose reduction for grade 3 fatigue , his lung mass again increased in size . 
by that point , he had survived 3.5 years since diagnosis of nsclc with a response duration of 12 months on braf targeted therapy . discussion in this era of personalized medicine , targeted therapies against braf v600e and mek have changed the standard of care in the treatment of braf - mutated metastatic melanoma . 
two brafis , dabrafenib and vemurafenib , with or without mekis , trametinib and cobimetinib , are approved for braf v600emutant metastatic melanoma.7 , 8 such targeted medications also have clinical activity in braf v600emutant nsclc.4 - 6 , 9 , 10 in a retrospective analysis of the european euraf cohort , 35 patients with braf - mutant nsclc treated with brafis were identified . 
after first - line therapy with brafis , overall survival ( os ) was 25.3 months in patients with braf v600emutant nsclc ( n = 29 ) and 11.8 months in patients with nonv600e braf mutations ( n = 6 ) .9 response to chest before and after initiation of vemurafenib , at 2 weeks , and at 3 months demonstrated a significant decrease in the size of the rightside upper - lobe mass [ aq4 ] and improvement of the air space disease , with an overall decrease in tumor volume of greater than 90% ( fig 1 )  . 
the dosage of vemurafenib was reduced twice for grade 3 fatigue , recurrent grade 2 skin rash , and transaminitis . after maintaining response for 7 months on vemurafenib , the patients tumor burden escalated fig 1 . 
computed tomography scans of chest demonstrating response to combination dabrafenib and trametinib treatment brafis also was documented in a phase ii basket trial of vemurafenib in braf v600mutant positive nonmelanoma cancers with an overall response rate ( orr ) of 42% in 20 patients with nsclc.10 in a prospective multicenter phase ii clinical trial , planchard et al5 evaluated the safety and efficacy of dabrafenib trametinib in nsclc . 
previously treated patients ( n = 78 ) and treatment - nave patients ( n = 6 ) responded to dabrafenib alone with a median progression - free survival ( pfs ) of 5.5 months , a median os of 12.7 months , and an orr of 33% . 
testing for braf is recommended as part of the initial molecular analysis in patients with lung cancer of adenocarcinoma histology and is considered in some patients with squamous subtype.11 all patients with braf v600emutant nsclc eventually progress after brafis with or without mekis . 
resistance mechanisms are not as well characterized in nsclc compared with braf v600emutant melanoma.12 secondary resistance mechanisms in melanoma include ras mutations , braf splice variants , braf v600 amplifications , mek1 / 2 mutations , and non - mapk pathway alterations.13 in nsclc , lin et al14 described two classes of resistance patterns to vemurafenib using a preclinical model of hcc364 braf v600emutant lung cancer cells . 
in contrast , expression of c - junmediated egfr ligands that promote continued egfr signaling represents another class.14 plx9394 , a novel brafi , evades resistance caused by alternatively spliced truncated braf v600e , but subsequent resistance occurs through egfr - mediated ras - mammalian target of rapamycin signaling.15 in the clinical setting , kras , tp53 , and cdkn2a mutations were acquired in one patient after progression on dabrafenib.16 currently , there is no standard therapy for patients with braf v600emutant nsclc after progression on brafis . 
in a phase i / ii study , the combination of brafi and meki was evaluated in patients with braf v600mutant metastatic melanoma who had disease progression on a single - agent brafi . 
one of these patients had a partial response to dabrafenib monotherapy after prior treatment with vemurafenib.9 another case report showed a similar response ; a patient who progressed on vemurafenib achieved a 3 - month clinical benefit with single - agent dabrafenib.18 our patient attained clinical response for an additional 5 months with an alternative brafi , dabrafenib , combined with the meki trametinib after progression on vemurafenib . 
two prior case studies described the benefit of combination treatment after progression on initial brafi monotherapy.19 , 20 similar to our patient , schmid et al19 reported on a patient who responded to combination dabrafenib and trametinib for 6 months after progression on vemurafenib . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . sushma jonna no relationship to disclose affiliations all authors : georgetown university , washington , dc . clinical trials or have already progressed on other lines of therapy . 
chen d , zhang lq , huang jf , et al : braf mutations in patients with non - small cell lung cancer : a systematic review and meta - analysis . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) - mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
planchard d , kim tm , mazieres j , et al : dabrafenib in patients with braf ( v600e ) - positive advanced non - small - cell lung cancer : a single - arm , multicentre , open - label , phase 2 trial . 
planchard d , smit ef , groen hjm , et al : dabrafenib plus trametinib in patients with previously untreated brafv600e - mutant metastatic non - small - cell lung cancer : an open - label , phase 2 trial . 
lindeman ni , cagle pt , aisner dl , et al : updated molecular testing guideline for the selection of lung cancer patients for treatment with targeted tyrosine kinase inhibitors : guideline from the college of american pathologists , the international association for the study of lung cancer , and the association for molecular pathology . 
johnson db , menzies am , zimmer l , et al : acquired braf inhibitor resistance : a multicenter meta - analysis of the spectrum and frequencies , clinical behaviour , and phenotypic associations of resistance mechanisms . 
okimoto ra , lin l , olivas v , et al : preclinical efficacy of a raf inhibitor that evades paradoxical mapk pathway activation in protein kinase braf - mutant lung cancer . 
rudin cm , hong k , streit m : molecular characterization of acquired resistance to the braf inhibitor dabrafenib in a patient with braf - mutant non - small - cell lung cancer . 
johnson db , flaherty kt , weber js , et al : combined braf ( dabrafenib ) and mek inhibition ( trametinib ) in patients with brafv600 - mutant melanoma experiencing progression with single - agent braf inhibitor . 
schmid s , siano m , joerger m , et al : response to dabrafenib after progression on vemurafenib in a patient with advanced braf v600e - mutant bronchial adenocarcinoma . 
 approximately 40% of families fulfilling the clinical criteria for hdgc have germline cdh1 mutations.5 a subset of the remaining families of hdgc , and ones fulfilling the criteria of other familial gc , harbor pathogenic germline mutation in other genes that are associated with hereditary cancer predisposition syndromes.4 hereditary breast and ovarian cancer is one of the best - described inherited cancer predisposition syndromes , caused by pathogenic germline brca1 or brca2 ( brca1 / 2 ) mutations.6 - 9 the increased risks of cancers other than breast and ovarian cancers were observed in the carriers.10 the association between germline brca1 / 2 mutation and increased risk of gc were demonstrated in previous studies for families with hereditary breast and ovarian cancer.11 - 14 regarding fgc , a recent large - scale study demonstrated that germline brca2 mutations were identified in patients who had a family history that fulfilled the criteria of hdgc but were lacking cdh1 mutations.15 therefore , it is possible that germline brca1 / 2 mutations may cause familial predisposition to gc . recent advances of comprehensive genomic analysis enable us to identify the genomic alterations in gc.16 brca1 / 2 mutations were shown in the subset of gc tumor tissues ; however , the association between germline brca1 / 2 mutations and familial predisposition to gc were not fully understood . 
previously , we performed genomic sequencing of 207 japanese gcs using a 435 - gene panel and identified brca1 / 2 mutations in tumor.17 in this study , we conducted brca1 / 2 genetic testing in seven japanese patients with gc whose tumor had brca1 / 2 mutations . 
we identified pathogenic germline brca1 / 2 mutations in three patients who have a familial component of gc . methods among 28 patients whose tumor had brca1 / 2 mutations in our previous study , seven patients who could provide written informed consent were enrolled . 
we assessed the family history using the criteria for referral for genetic risk assessment and fgc defined by international gastric cancer linkage consortium after the enrollment ( table 1 ) .4 clinicopathological data are listed in table 2 . 
this study was approved by the institutional review boards at niigata university and niigata cancer center hospital . results family history of cases 1 to 4 met the criteria for referral to genetic risk assessment , and that of cases 1 , 3 , and 4 met the criteria for fgc ( table 2 )  . 
cases 5 to 7 also had germline brca1 or brca2 mutations ; however , pathogenicity was determined to be uncertacase 4 had no germline mutations in brca1 / 2 ( table 3 )  . 
he had a strong family history of cancers , with three gc and one breast cancer in firstor second - degree relatives ( fig 2a ) , which met the criteria for fgc ( table 1 )  . 
although adjuvant chemotherapy with s - 1 , an oral fluoropyrimidine preparation combining tegafur , gimeracil , and oteracil potassium , was performed , she suffered para - aortic lymph node recurrence 6 months after gastrectomy . 
she had a strong family history of cancers , with two gcs and one case each of breast , lung , and cervical cancers in firstor second - degree relatives , which did not fulfill the criteria for fgc ( fig 2b )  . 
genetic testing detected double pathogenic nonsense germline mutations in brca1 c.188t > a ( p.l63x ) and in brca2 c.6922a > t ( p.k2308x ) , which were identical to the variants detected in tumor ( table 3 )  . case 3 a 56 - year - old man underwent curative gastrectomy with d2 lymphadenectomy for gc . 
genetic testing detected a pathogenic nonsense germline mutation in brca2 c.9310a > t ( p.k3104x ) , which was identical to the variant detected in tumor ( table 3 )  . discussion previous studies have shown that germline brca1 / 2 mutations increase the risk of gc.11 - 14 however , there is a paucity of data regarding the relationship between germline brca1 / 2 mutations and familial predisposition to gc in japan . 
among these , one patient ( case 2 ) had double pathogenic germline mutations in brca1 and brca2 , which were considered to be rare , as shown by a previous study for ashkenazi jewish double - founder mutations.18 to the best of our knowledge , this is the first report of japanese patients with fgc harboring brca1 / 2 mutations . multiple genetic and environmental factors influence the etiology of gc . 
the well - known environmental factors are high salt intake and hp infection , which cause chronic gastritis.19 the development of gc stands out in the family history of our three cases , rather than breast and ovarian cancers ( fig 2 )  . 
hp infection was detected in cases 1 and 3 and intestinal - type gc , which is most associated with chronic gastritis , was observed in cases 1 and 2 ( fig 1 )  . 
these findings suggested that chronic gastritis , which is associated with hp infection and / or environmental factors , may cause the loss of brca1 / 2 function by the second - hit mutations in patients with the germline mutations . 
this synergistic exacerbatory effect confers the familial predisposition to gc in japan , where a high incidence is observed . brca1 / 2 mutation carriers might have a risk of multiple gcs . 
brca1 / 2 mutations are considered risk factors for ipsilateral breast cancer recurrence.20 regarding hdgc caused by cdh1 germline mutation , multiple foci of signet ring cell carcinoma were detected in the stomach of individual patients.21 , 22 prophylactic total gastrectomy is recommended for cdh1 mutation carriers because of the high cumulative incidence and the difficulty of early detection of hdgc by endoscopy.23 in this report , the intestinal type of gc , which is relatively easy to detect at an early stage by endoscopy , predominantly developed in the affected patients . 
brca1 / 2 - mutated ovarian and breast cancers have high sensitivity to platinum chemotherapy and poly ( adenosine diphosphate ribose ) polymerase ( parp ) inhibitors because of defective dna double - strand break repair.24 - 26 the us food and drug administration has approved the parp inhibitor olaparib for brca1 / 2 - mutated advanced ovarian cancer . 
in this report , case 2 , with both brca1 and brca2 germline mutations , showed high response of platinum - based chemotherapy for lymph node recurrence and long - term survival after the recurrence , in a manner similar to brca1 / 2 - mutated ovarian and breast cancers . 
additional clinical studies are required to clarify whether the brca1 / 2 mutations contribute to the good response to platinum - based chemotherapy and parp inhibitors in gc . in conclusion , brca1 / 2 mutations may predispose to familial gc . 
 shujiro okuda no relationship to disclose stephen lyle employment : kew stock and other ownership interests : kew consulting or advisory role : pfizer kazuaki takabe no relationship to disclose acknowledgment we thank our colleagues masaki aizawa and atsushi matsuki from niigata cancer center hospital for collection of the clinicopathological data . affiliations hiroshi ichikawa , toshifumi wakai , masayuki nagahashi , yoshifumi shimada , takaaki hanyu , yosuke kano , yosoke tajima , yusuke muneoka , takashi ishikawa , kazuyasu takizawa , jun sakata , takashi kobayashi , hitoshi kemeyama , and shujiro okuda , niigata university graduate school of medical and dental sciences ; hiroshi yabusaki , satoru nakagawa , nobuaki sato , takashi kawasaki , keiichi homma , niigata cancer center hospital , niigata city , niigata , japan ; stephen lyle , university of massachusetts medical school , worcester , ma ; and kazuaki takabe , roswell park cancer institute , and university at buffalo , the state university of new york , buffalo , ny . supported by funding from niigata prefecture , japan society for the promotion of science ( jsps ) grants - in - aid for scientific research ( kakenhi ) grant no . 
zanghieri g , di gregorio c , sacchetti c , et al : familial occurrence of gastric cancer in the 2 - year experience of a population - based registry . 
van der post rs , vogelaar ip , carneiro f , et al : hereditary diffuse gastric cancer : updated clinical guidelines with an emphasis on germline cdh1 mutation carriers . 
alsop k , fereday s , meldrum c , et al : brca mutation frequency and patterns of treatment response in brca mutation - positive women with ovarian cancer : a report from the australian ovarian cancer study group . 
 in a multivariable regression analysis adjusted for age , smoking , eastern cooperative oncology group performance status , and the presence of tp53 mt ( p = .063 ) and other coexisting mts ( p = .064 ) did not achieve statistical significance . 
2018 by american society of clinical oncology introduction epidermal growth factor receptor ( egfr ) and tumor suppressor tp53 genes are commonly mutated in patients with nonsmall - cell lung cancer ( nsclc ) with independent prognostic implications . 
a second site mutation in exon 20 of egfrt790maccounts for a significant proportion of acquired resistance to firstand second - generation tkis.5 - 7 resistance mechanisms also include other mutations in egfr ( c797s ) , met amplification , and mutations in other downstream oncogenic pathways.6 , 8 tp53 is a tumor suppressor gene that is located on the short arm of chromosome 17 at band charu aggarwal christiana w . 
inactivation of retinoblastoma and p53 has been demonstrated to be an early clinical biomarker for transformation to small - cell lung cancer.22 the primary objective of this study was to determine the prognostic impact of tp53 mutation on survival in patients with egfr - mt nsclc . 
smoking status was defined as never smokers ( fewer than 100 cigarettes lifetime ) , former smoker ( more than 100 cigarettes lifetime ) , and current smoker ( active smoker within 1 year of diagnosis )  . 
we searched the national death index and online obituaries to determine survival status for patients who were lost to follow - up . egfr and tp53 mutation analysis tissue testing solid tumor dna sequencing was performed using amplicon - based next - generation sequencing ( ngs ) to determine the mutation status of exons 18 through 21 of egfr and exons 4 through 10 of tp53 in a college of american pathologists / clinical laboratory improvement amendmentscertified laboratory at our institution , as previously described.24 patient samples were sequenced using one of three different panels that covered the regions of interest and other commonly mutated oncogenes . 
an illumina truseq amplicon cancer panel ( illumina , san diego , ca ) was used to sequence targeted hotspots or larger exonic regions for 47 genes ( appendix table a1 )  . 
samples with poor - quality tissue and / or insufficient dna for the truseq amplicon cancer panel assay input requirements were sequenced on a custom 20 - gene targeted hotspot panel , the penn precision panel ( appendix table a2 ) , and more recently , with an expanded 153 wholegene panel ( appendix table a3 ; haloplex ; agilent technologies , santa clara , ca )  . 
results were analyzed using a clinically validated bioinformatics pipeline using hg19 genome build as the reference genome.25 the limit of detection for mutations in tp53 and egfr is at 4% allele frequency , typically corresponding to at least 8% tumor in the submitted tissue specimen . 
 the expanded 153 - gene panel has full coverage of tp53 , whereas the 47 - gene panel and penn precision panels detect point mutations and small insertions and deletions in select regions with partial coverage of tp53 ( appendix tables a1 to a3 )  . plasma - based cell - free circulating tumor dna testing blood was collected in two 10 - ml streck tubes ( streck , la vista , ne ) and shipped overnight at ambient temperature to guardant health ( redwood city , ca ) , a clinical laboratory improvement amendmentscertified , college of american pathologistsaccredited laboratory facility . 
samples were sequenced on the 68 - gene panel for 12 patients , on the 70 - gene panel for 46 patients , and on the 73 - gene panel for the remaining seven patients.27 the plasma - based gene panel has full coverage of tp53 ( appendix table a4 )  . a coexisting oncogenic mutation was defined as a nonsynonymous variant detected in genes from solid tissue or plasma sequencing that occurred in addition to the identified egfr / tp53 mutations at the time of assessment . 
 only genes that were covered on both the tissue and plasma platforms were included in the analysis . statistical analysis descriptive statistics summarized patient characteristics and included frequencies and percentages for categorical variables , and mean , standard deviation , and standard error of the mean for continuous variables . 
overall , patient demographics and tumor characteristics were similar between tp53 wild - type ( wt ) and egfr / tp53 double - mt groups ( table 1 )  . 
 other oncogenic coexisting mts were present in 36% of patients with tp53 wt and 45.7% of those with egfr / tp53 double mt ( p = .362 ; fig 2c )  . 
a total of 86 oncogenic coexisting mts were observed in these 55 patients , 18.2% of which was in phosphatidylinositol - 4 , 5 - bisphosphate 3 - kinase catalytic subunit ( pik3ca ; fig 2d and appendix table a8 )  . 
consort diagra ( * ) patients had concurrent tissue and plasma ngs ( next - generation sequencing ) performed ( n = 42 ) ; tissue ngs results were used for analyses . 
 ( c ) prevalence of coexisting mts in the entire cohort , and in patients with tp53 mt , 55 patients were found to have coexisting mts , 37 of whom also harbored a tp53 mt . 
in one patient ( age 67 years , smoker ) , t790m mt emergent mt was evident , and in the other patient ( age 45 years , never smoker ) , a new rb1 mutation appeared . 
findings in individual patients at the time of sclc transformation included the disappearance of the emergent t790m , persistence of the rb1 mutation , and maintenance of a pik3ca mutation ( table 3 )  . 
similar to other series , we observed a significant improvement in os in patients who had a t790m mutation , likely related to the availability and effectiveness of third - generation egfr tkis , such as osimertinib . 
 ( a ) kaplan - meier curve representing os of patients with stage iv disease at diagnosis and tumors with tp53 mutation ( mt ; n = 81 ) and tp53 wild - type ( wt ) cohorts ( n = 50 )  . 
 ( b ) kaplan - meier curve representing os of patients with stage iv disease at diagnosis and tumors with coexisting mt ( n = 55 ) and without coexisting mt ( n = 76 )  . 
 ( c ) kaplan - meier curve representing os of patients with stage iv disease at diagnosis and tumors with tp53 exon 8 mt ( n = 18 ) and tp53 mt other than exon 8 ( n = 63 )  . 
a larger study with 136 patients corroborated the finding that tp53 mutationsanalyzed for 123 patientswere associated with a lower response rate and poor prognosis with the use of tkis in egfr - mt nsclc.36 survival was not statistically significant in this study for the overall population , but there was a significant survival difference for a specific subset of patientsthose with exon 8 mutations36 ( n = 12 )  . 
we report on five patients whose tumors transformed to sclc , with paired biopsies showing an increase in tp53 mt allelic fraction , which is suggestive of an increase in genomic heterogeneity at the time of transformation and potentially complete inactivation of p53 . 
to our knowledge , this is the first report of serial analysis of multiple patients where tp53 mutation was detected with routine clinically indicated ngs at the time of transformation to sclc . 
although these mutations were heterogonous and distinct , our findings offer supportive evidence of the role of p53 inactivation in the clonal evolution of egfr - mt nsclc.45 the current study has a number of important limitations . 
carpenter mutations within the introns , the loss of chromosome 17p or the deletion of the tp53 locus would not be detectable by ngs assays that were used for this analysis . 
this analysis also does not account for tumor heterogeneity with low - level mutations in subpopulations that were not detected , either because of mutation below the level of detection in the submitted specimen or regional heterogeneity within a tumor mass or between metastatic sites . 
furthermore , although our study cohort of double mutants81 patients with egfr / tp53 double - mt nsclcis one of the largest series reported to date , it is still relatively small . 
we controlled for confounding factors by using multivariable regression analyses . in conclusion , tp53 mt and other oncogenic coexisting mutations were associated with worse os in patients with egfr - mt nsclc . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . charu aggarwal consulting or advisory role : genentech , bristol - myers squibb , eli lilly , celgene research funding : genentech ( inst ) , incyte ( inst ) , macrogenics ( inst ) , merck sharp & dohme ( inst ) christiana w . 
thompson consulting or advisory role : oncocyte saman ahmed no relationship to disclose seth jeffries no relationship to disclose stephen bagley research funding : incyte , novocure peter gabriel research funding : varian medical systems tracey l . 
evans honoraria : genentech , genentech ( i ) consulting or advisory role : genentech , genentech ( i ) speakers ' bureau : genentech , genentech ( i ) travel , accommodations , expenses : genentech , genentech ( i ) joshua m . 
bauml consulting or advisory role : bristol - myers squibb , merck , astrazeneca , genentech , celgene , boehringer ingelheim , guardant health research funding : merck ( inst ) , carevive systems ( inst ) , novartis ( inst ) , incyte ( inst ) , bayer ( inst ) , janssen pharmaceuticals ( inst ) christine ciunci no relationship to disclose evan alley no relationship to disclose jennifer j.d. 
cohen honoraria : bristol - myers squibb consulting or advisory role : heat biologics , takeda , cerulean pharma , kolltan pharmaceuticals , zymeworks , pfizer research funding : heat biologics ( inst ) , macrogenics ( inst ) , merck ( inst ) , takeda ( inst ) , cleave biosciences ( inst ) , celldex ( inst ) travel , accommodations , expenses : heat biologics , takeda , kolltan pharmaceuticals , cerulean pharma , zymeworks , bristol - myers squibb , pfizer erica l . 
langer honoraria : bristol - myers squibb , genentech , eli lilly , imclone consulting or advisory role : genentech , eli lilly , imclone , merck , abbott biotherapeutics , bayer , onyx pharmaceuticals , clarient , clovis oncology , celgene , cancer support community , bristol - myers squibb , ariad pharmaceuticals , takeda , astrazeneca research funding : merck ( inst ) , advantagene ( inst ) , clovis oncology ( inst ) , celgene ( inst ) , inovio pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , genentech ( inst ) , stem centrx ( inst ) other relationship : eli lilly , amgen , peregrine pharmaceuticals , synta affiliations charu aggarwal , christiana w . 
pao w , miller v , zakowski m , et al : egf receptor gene mutations are common in lung cancers from never smokers and are associated with sensitivity of tumors to gefitinib and erlotinib . 
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molina - vila ma , bertran - alamillo j , gasc a , et al : nondisruptive p53 mutations are associated with shorter survival in patients with advanced nonsmall - cell lung cancer . 
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lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
cortot ab , younes m , martel - planche g , et al : mutation of tp53 and alteration of p14 ( arf ) expression in egfrand kras - mutated lung adenocarcinomas . 
ozenne p , dayde d , brambilla e , et al : p14 ( arf ) inhibits the growth of lung adenocarcinoma cells harbouring an egfr l858r mutation by activating a stat3 - dependent pro - apoptotic signalling pathway . 
lueers ac , halbfass v , prenzel r , et al : incidence of egfr , kras , braf , alk and p53 alterations in a cohort of 218 consecutively tested patients from a certified lung cancer center : correlation with clinical characteristics and treatment outcome . 
yu ha , jordan e , ni a , et al : concurrent genetic alterations identified by next - generation sequencing in untreated , metastatic egfr - mutant lung cancers . 
lim sm , kim hr , cho ek , et al : targeted sequencing identifies genetic alterations that confer primary resistance to egfr tyrosine kinase inhibitor ( korean lung cancer consortium )  . 
bria e , pilotto s , amato e , et al : molecular heterogeneity assessment by next - generation sequencing and response to gefitinib of egfr mutant advanced lung adenocarcinoma . 
aisner dl , sholl lm , berry ld , et al : the impact of smoking and tp53 mutations in lung adenocarcinoma patients with targetable mutations : the lung cancer mutation consortium ( lcmc2 )  . 
hata a , katakami n , yoshioka h , et al : spatiotemporal t790m heterogeneity in individual patients with egfr - mutant nonsmall - cell lung cancer after acquired resistance to egfr - tki . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a thirdgeneration egfr inhibitor . 
mooradian mj , piotrowska z , drapkin bj , et al : clonal evolution and the role of serial liquid biopsies in a case of small - cell lung cancertransformed egfr mutant nonsmall - cell lung cancer . 
an endobronchial biopsy showed an adenocarcinoma consistent with a lung primary ( thyroid transcription factor 1 positive , napsin a positive , and cytokeratin 7 positive by immunohistochemistry ; figs 1a and 1b )  . targeted exon sequencing of 468 genes with memorial sloan kettering integrated mutation proling of actionable cancer targets ( msk - impact ) was negative for known mitogenic drivers , including kras , egfr , braf , met , and erbb2 mutations and alk , ros1 , and ret rearrangements . 
photomicrographs of ( a ) cytology from the patients lung adenocarcinoma and ( b ) positive immunohistochemistry results remarkable for cytoplasmic and membranous staining using a pan - trk antibody are shown . 
this identied a novel activating trk fusion ( in - frame fusion between eps15 exon 21 and ntrk1 exon 10 ; figs 1c and 1d )  . the patient consented to receive larotrectinib in a basket study for trk fusion - positive cancers ( navigate ; clinicaltrials.gov identier : nct02576431 )  . 
a brisk partial response to therapy was achieved at 4 weeks , which was subsequently conrmed at 8 weeks ( 34% by response evaluation criteria in solid tumors [ recist ] version 1.1 ; fig 2 ) , with regression of all areas of disease . 
this included near total resolution of all brain metastases at 8 weeks ( 95% reduction in aggregate tumor volume ) and subsequently , a complete intracranial response by 16 weeks ( fig 3 )  . 
pathology showed a stage iiic ( t1cn3m0 ) multifocal invasive ductal carcinoma ; the largest lesion measured 1.8 cimmunohistochemistry was positive for estrogen and progesterone receptors and negative for human epidermal growth factor receptor 2 . 
she was treated initially with adjuvant dose - dense doxorubicin , cyclophosphamide , plus paclitaxel and radiotherapy , after which she received anastrozole followed by bilateral salpingo - oophorectomy . the patient developed recurrent , metastatic disease approximately 17 months after completing adjuvant radiolymph node biopsy conrmed therapy . 
sequencing of an abdominal lymph node and a subsequently biopsied liver metastasis using msk - impact revealed the previously reported fusion between lmna exons 1 and 20 and ntrk1 exons 11 and 17 , which was veried using targeted multiplex rna sequencing . the patient consented to receive larotrectinib in the same basket study for trk fusion - positive cancers ( navigate )  . at enrollment , her disease was widely metastatic to liver , adrenal gland , lymph nodes , and bone . 
a brisk and conrmed partial response by recist version 1.1 ( 32% , 47% , and 56% at 4 , 8 , and 16 weeks , respectively ) was achieved . 
of note , her cns metastases likewise regressed at the rst follow - up assessment at 4 weeks , with a complete response in the cns at 8 weeks ( fig 4 )  . 
axial contrastenhanced t1 - weighted images at ( a ) baseline ( brain metastases highlighted by circles ) , ( b ) 8 weeks , and ( c ) 16 weeks after treatment with larotrectinib was initiated demonstrate decreased and then resolved metastases in the right - side insula and left - side occipital lobe . 
three - dimensional models at ( d ) baseline and ( e ) post - treatment at 8 weeks and ( f ) post - treatment at 16 weeks conrmed decreased burden of metastatic intracranial disease ( segmented in green voxels and quantied at bottom )  . 
response to larotrectinib in a patient with a trk fusion - positive metastatic breast cancer . baseline axial computed tomography imaging of the brain was performed with the addition of iodinated contrast that showed ( a ) metastatic brain disease ( circles ) and after 8 weeks of treatment with larotrectinib , ( b ) complete response . 
 rosen et al discussion to our knowledge , this report is the rst to showcase the intracranial efcacy of larotrectinib in metastatic trk fusion - positive cancers of any histology . 
these cases demonstrate that larotrectinib can achieve clinically relevant cns exposure , which highlights its role in the management of trk fusion - positive cancers with intracranial disease . beyond nsclcs and breast cancers , other trk fusionpositive tumors have a proclivity for brain metastases.1 the intracranial activity featured here is consistent with prior work that did not identify cns metastasis as a site of progression on larotrectinib across multiple tumor types4 and with a report that showed a response to larotrectinib in a trk fusion - positive glioma.5 additional clinical experience in patients with trk fusion - positive cancers with cns involvement ultimately will delineate the overall activity and durability of larotrectinib within the cns . although this article represents what is to our knowledge the rst report of intracranial responses to a sein patients with trk fusionlective trk inhibitor positive cancers and brain metastases , intracranial disease control also has been reported with multikinase trk inhibitors . 
entrectinib , a multikinase trk , ros1 , and alk inhibitor , displayed activity in a patient with a trk fusion - positive lung cancer and brain metastases6 and in ros1 fusion - positive lung cancers with intracranial disease.7 repotrectinib , a multikinase trk , ros1 , and alk inhibitor , achieved intracranial disease regression in untreated brain metastases in a patient with a ros1 fusion - positive nsclc.8 finally , this report represents the rst description of the novel eps15 - ntrk1 fusion . 
young stock and other ownership interests : agios , alexion pharmaceuticals , biogen , celgene , gilead sciences , karyopharm therapeutics , spark therapeutics , regeneron pharmaceuticals , stemline therapeutics , vertex consulting or advisory role : agios , puma biotechnology , nordicneurolab , icon clinical research research funding : agios ( inst ) jaclyn f . 
shu research funding : celgene ( inst ) , genentech ( inst ) , roche ( inst ) , janssen pharmaceuticals ( inst ) , medimmune ( inst ) travel , accommodations , expenses : genentech , roche nora c . 
 cns efcacy of larotrectinib in trk fusion - positive solid tumors travel , accommodations , expenses : novartis ( i ) , biotheranostics ( i ) , pzer ( i ) , amgen ( i ) , genentech ( i ) , roche ( i ) , astrazeneca ( i ) , macrogenics ( i ) , peregrine pharmaceuticals ( i ) , pierian bioscience ( i ) david m . 
ziegler ds , wong m , mayoh c , et al : brief report : potent clinical and radiological response to larotrectinib in trk fusion - driven high - grade glioma . 
drilon a , siena s , ou s - hi , et al : safety and antitumor activity of the multi - targeted pan - trk , ros1 , and alk inhibitor entrectinib ( rxdx - 101 ) : combined results from two phase 1 trials ( alka - 372 - 001 and startrk - 1 )  . 
doebele r , ahn m , siena s , et al : oa02.01 : efcacy and safety of entrectinib in locally advanced or metastatic ros1 fusion - positive non - small cell lung cancer 8 . 
drilon a , ou si , cho bc , et al : repotrectinib ( tpx - 0005 ) is a next - generation ros1 / trk / alk inhibitor that potently inhibits ros1 / trk / alk solvent - front 9 . 
pathologic examination showed a 2.9 - cm collecting duct carcinoma ( cdc ) with metastases in eight of 15 resected hilar , suprahilar , and periaortic lymph nodes . after surgery , the patient was initiated on therapy with cisplatin and gemcitabine on a dosing schedule of once every 3 weeks . 
cytologic examination of pleural fluid retrieved during thoracentesis confirmed malignant pleural effusions . given the absence of any standard second - line treatment of cdc , comprehensive genomic profiling ( cgp ) was performed using a commercially available assay in a clinical laboratory improvement amendmentscertified , college of american pathologistsaccredited laboratory ( foundation medicine ; cambridge , ma )  . 
formalin - fixed paraffin - embedded tumor derived from the original nephrectomy specimen was analyzed by hybridization capture of all coding exons from 315 cancerrelated genes and select introns of 28 genes commonly rearranged in cancer . 
sequencing and bioinformatics methods for characterization of genomic alterations ( ga ) have previously been described in detail.1 the sole ga observed in this case was homozygous deletion of cdkn2a / b . 
multiple variants of unknown significance were identiincluding bard1 ( p358_s364del ) , brip1 fied , ( r264w ) , crlf2 ( e213k ) , dicer1 ( v594i ) , fgf6 ( n113k ) , igf1r ( p190s ) , mll2 ( r1292c ) , notch1 ( v1232m ) , pdgfrb ( s408c ) , ros1 ( e401k ) , socs1 ( a44_v45insvp ) , and tet2 ( e1405q )  . 
cdkn2a alteration has been suggested to be a potential predictive biomarker for cdk4 / 6 inhibitors.2 , 3 in light of loss of cdkn2a / b , the patient was offered therapy with the cdk4 / 6 inhibitor palbociclib . 
chung , foundation medicine , cambridge ; and toni k . choueiri , dana - farber cancer institute / brigham and womens cancer center , boston , ma corresponding author : sumanta k . 
the genomic landscape of cdc was defined in a previous report from our group.11 potential biomarkers for response to cdk4 / 6 inhibitors such as palbociclib include alterations in genes involved in the regulation of cdk4 / 6cyclin d kinase complexes , 2 , 3 such as cdk4 amplification , and palbociclib has demonstrated encouraging activity in phase 2 studies of patients with liposarcoma who harbor this driver.12 , 13 although preclinical studies of cell lines from multiple cancer types , including rcc , have reported that cdkn2a / p16ink4a loss of function is associated with sensitivity to cdk4 / 6 inhibitors , 14 - 18 there is limited clinical evidence supporting cdkn2a as a predictive biomarker , with one case study reporting that a patient with uterine leiomyosarcoma harboring cdkn2a homozygous deletion and a concurrent nf2 mutation experienced 4 months of stable disease on palbociclib treatment . in contrast , for patients with advanced breast cancer , for which palbociclib is approved with either letrozole or fulvestrant , cdkn2a loss ( assessed by fluorescent in situ hybridization ) was not associated with further benefit from palbociclib in combination with letrozole , in the palbociclib ongoing trials in the management of breast cancer ( paloma ) - 1 trial for patients with er + / her22 breast cancer.19 similarly , in a basket trial of the cdk4 / 6 inhibitor ribociclib , no responses were observed among the 73 patients with cancer whose tumor harbored a cdkn2a ga , as assessed by cgp.20 in this context and that of limited single - agent efficacy of cdk4 / 6 inhibitors in unselected populations , 19 , 20 the partial response to palbociclib experienced here by a patient with metastatic refractory cdc harboring cdkn2a / b homozygous deletion is unusual . 
in a series of 17 patients with cdc assessed by cgp , the most frequently identified gas were in nf2 ( 29% ) , setd2 ( 24% ) , smarcb1 ( 18% ) , and cdkn2a / b ( 12% , including homozygous deletion and mutation )  . 
characteristics for cases with cdkn2a or cdkn2a / b homozygous deletion characteristic total cases , no . total cases with cdkn2a or cdkn2a / b homozygous deletion , no . cases with cdkn2a or cdkn2a / b homozygous deletion and no co - occurring alteration , no . characteristics of patients with cdkn2a or cdkn2a / b homozygous deletion and no co - occurring alteration female male age , years , median ( range ) median tumor mutational burden , no . 
cdkn2a ( or cdkn2a / b ) homozygous deletion was identified as the sole driver alteration in 1.2% ( 16 of 1 , 322 ) rcc cases and also in other disease types , including 15.2% of salivary gland acinic cell tumors , 14.3% of bone giant - cell tumors , and 11.3% of bone chordomas ( table 1 )  . 
it is conceivable , however , that some of these cases with cdkn2a homozygous deletion as the sole known ga may harbor concurrent driver alterations that have not yet been discovered . 
a larger subset of cases ( 16% ) had homozygous deletion of this locus as well as other gas in other genes ( table 1 ) , and additional cases had loss of heterozygosity of cdkn2a with the remaining allele mutated . 
more investigation is also required to understand how responses to cdk4 / 6 inhibitors for patients with cdkn2a alteration may be modulated by the presence or absence of different driver gene alterations . for patients with cdc , additional genomic profiling studies are needed , given the response to palbociclib observed in this study , which suggests that cdk4 / 6 inhibitors should be further explored for patients with cdkn2a - altered cdc . 
more broadly , this study identifies cdkn2a homozygous deletion as the sole known ga in a small subset ( 0.25% ) of advanced cancer cases and at higher frequency in specific tumor types ( table 1 )  . 
 patents , royalties , other intellectual property : patents via foundation medicine , seres health on microbiome research in non - neoplastic disease ( inst ) genentech , eisai , foundation medicine , cerulean pharma , astrazeneca , peloton therapeutics , exelixis , prometheus , alligent jeffrey ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine honoraria : pfizer , emd merck serono research funding : foundation medicine toni k . 
choueiri honoraria : national comprehensive cancer network , uptodate consulting or advisory role : pfizer , bayer , novartis , glaxosmithkline , merck , bristol - myers squibb , roche / research funding : pfizer ( inst ) , novartis ( inst ) , merck ( inst ) , exelixis ( inst ) , tracon pharma ( inst ) , glaxosmithkline ( inst ) , bristol - myers squibb ( inst ) , astrazeneca ( inst ) , peloton therapeutics ( inst ) , roche / genentech ( inst ) , celldex ( inst ) , agensys ( inst ) travel , accommodations , expenses : advisory boards / consultancy jon h . 
curr oncol 20 : e223 - e232 , 2013 von der maase h , hansen sw , roberts jt , et al : gemcitabine and cisplatin versus methotrexate , vinblastine , doxorubicin , and cisplatin in advanced or metastatic bladder cancer : results of a large , randomized , multinational , multicenter , phase iii study . 
miyake h , haraguchi t , takenaka a , et al : metastatic collecting duct carcinoma of the kidney responded to sunitinib . int j clin oncol 16 : 153 - 155 , 2011 10 . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
dickson ma , tap wd , keohan ml , et al : phase ii trial of the cdk4 inhibitor pd0332991 in patients with advanced cdk4 - amplified well - differentiated or dedifferentiated liposarcoma . 
logan je , mostofizadeh n , desai aj , et al : pd - 0332991 , a potent and selective inhibitor of cyclin - dependent kinase 4 / 6 , demonstrates inhibition of proliferation in renal cell carcinoma at nanomolar concentrations and molecular markers predict for sensitivity . 
young rj , waldeck k , martin c , et al : loss of cdkn2a expression is a frequent event in primary invasive melanoma and correlates with sensitivity to the cdk4 / 6 inhibitor pd0332991 in melanoma cell lines . 
finn rs , crown jp , lang i , et al : the cyclin - dependent kinase 4 / 6 inhibitor palbociclib in combination with letrozole versus letrozole alone as first - line treatment of oestrogen receptor - positive , her2 - negative , advanced breast cancer ( paloma - 1 / trio - 18 ) : a randomised phase 2 study . 
peguero ja , oneil bh , sohal d , et al : genomic mutation profiling ( gmp ) and clinical outcome in patients ( pts ) treated with ribociclib ( cdk4 / 6 inhibitor ) in the signature prograj clin oncol 34 , 2016 ( suppl ; abstr 2528 ) 21 . 
wang j , papanicolau - sengos a , chintala s , et al : collecting duct carcinoma of the kidney is associated with cdkn2a deletion and slc family gene up - regulation . 
the utility of ultra - deep genomic testing to predict and the impact of conditioning intensity to prevent mds relapse are unknown . methods targeted error - corrected dna sequencing was performed on preconditioning blood samples from patients with mds ( n = 48 ) from the blood and marrow transplant clinical trials network 0901 phase iii randomized clinical trial , which compared outcomes by allogeneic hematopoietic cell transplantation conditioning intensity in adult patients with , 5% marrow myeloblasts and no leukemic myeloblasts in blood on morphological analysis at the time of pretransplant assessment . 
clinical end points ( 53 - month median follow - up ) included transplant - related mortality ( trm ) , relapse , relapse - free survival ( rfs ) , and overall survival ( os )  . 
of the 48 patients examined , 14 experienced trm , 23 are relapse - free , and 11 relapsed , of which 7 died . results using a previously described set of 10 gene regions , 42% of patients ( n = 20 ) had mutations detectable before random assignment to reduced intensity conditioning ( ric ) or myeloablative conditioning ( mac )  . 
testing additional genes , including those associated with mds , did not improve prognostication . conclusion this study provides evidence that targeted dna sequencing in patients with mds before transplant can identify those with highest post - transplant relapse rates . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction myelodysplastic syndrome ( mds ) , one of the most common hematologic disorders , is a collection of clinically and genetically heterogeneous diseases . 
 dillon et al context key objective allogeneic hematopoetic cell transplantation ( allohct ) is the only curative therapy for myelodysplastic syndrome ( mds ) but is associated with suboptimal rates of transplant - related mortality ( trm )  . 
using samples from a randomized phase iii clinical trial comparing allohct conditioning intensity in patients with mds , this study examined the prognostic signicance of pretransplant genetic markers on post - transplant outcomes . knowledge generated the presence of mutations within a previously identied set of 10 gene regions before allohct was associated with increased rates of relapse and decreased relapse - free survival in patients with mds who received reduced intensity versus myeloablative conditioning . 
library preparation and pairedend 150 - bp sequencing were performed using unique dualsample indices on an hiseq 2500 ( rapid run mode ; illumina , san diego , ca ) as previously described.10 an average of 43 million paired - end reads were acquired per sample ( data supplement )  . 
details are provided in the data supplement . bioinformatics consensus sequences based on umi read families were mapped to human genome version hg19 ( build grch37 )  . de novo variant calls were made using a minimum allele frequency of 0.001 and were ltered using information regarding umi read families , background error rate models , unique start sites , strand - specic priming , and homopolymer runs . 
alternative approaches were used for insertional mutations in npm1 and flt3 internal tandem duplication . details are provided in the data supplement . statistical analysis kaplan - meier estimation and log - rank test were used for analysis of os and relapse - free survival ( rfs ) and grays test for competing risks of trm and relapse . 
details are provided in the data supplement . results patient cohort a total of 54 patients with mds participated in the bmtctn 0901 clinical trial , of which 48 had blood collected after study enrollment before random assignment to mac ( n = 25 ) or ric ( n = 23 ) conditioning regimens , which was used for genomic analysis in this study . 
this subset of patients was well - matched for baseline characteristics ( table 1 ) , and clinical outcomes were aligned with those previously reported ( data supplement )  . 
ngsg10 mutational status served as a strong predictor of relapse in this cohort of patients with mds , predicting 73% of relapses at 24 months ( 100% for those receiving mac ) , with a specicity of 78% ( 100% for those receiving ric ) ( data supplement )  . to ngsg10 mutational status , no signicant in contrast difference in rates of relapse or os was observed when stratifying patients by disease classication , disease risk group , or cytogenetic prognostic group ( data supplement )  . rates of relapse trended higher in patients with poor cytogenetics or categorized as high risk . 
inclusion of patients with poor cytogenetics before transplant with ngsg10 mutational status improved prediction of relapse at 24 months from 73% to 91% ( data supplement ) and was associated with signicantly higher rates of relapse compared with ngsg10 - negative patients ( data supplement )  . presence of mutations pretransplant predicts relapse by conditioning intensity the impact of conditioning intensity and ngsg10 next , mutational status was examined ( data supplement )  . 
inclusion of patients with poor cytogenetics before transplant with ngsg10 mutational status improved prediction of relapse at 24 months in the ric group to 89% , with a specicity of 89% , and is associated with signicantly increased rates of relapse and decreased rfs compared with patients receiving mac ( data supplement )  . screening for additional genes does not improve test performance the mutational spectrum of mds is complex , with many additional genes recurrently mutated beyond the 10 amlassociated genes described above.7 , 11 , 12 therefore , we expanded our testing to also cover regions in an additional 19 genes including those commonly found in mds at diagnosis ( asxl1 , bcor , cbl , cux1 , dnmt3a , etv6 , ezh2 , gata2 , kras , phf6 , ppm1d , ptpn11 , setbp1 , srsf2 , stag2 , tet2 , u2af1 , wt1 , and zrsr2 )  . 
 ( c ) 10 - gene ngspositive patients had signicantly decreased rfs ( 3 - year rfs , 34% v 71% , p = .006 ) and os ( 3year os , 55% v 79% , p = .045 ) compared with ngs - negative patients . 
the inclusion of dta ( dnmt3a , tet2 , and asxl1 ) genes , known to be associated with age - related clonal hematopoiesis , 13 , 14 resulted in reclassication of 21% ( n = 6 ) of ngsg10negative patients to positive . 
similar to what we observed in patients with aml , 10 samples testing positive for only dta mutations showed no difference in relapse rates or os compared with those testing negative . 
no relapses were observed in patients testing positive only for these 16 genes regardless of conditioning intensity , and only one death was observed ( trm in the mac group )  . 
limiting analysis to those testing positive for an ngsg10 mutation at or above 2.5% vaf reduced the sensitivity at 24 months from 73% to 45% ( data supplement )  . 
overall p values ( in bold ) : grays test for transplant - related mortality and relapse ; log - rank test for rfs and os . abbreviations : ngsg10 , next - generation sequencing 10 - gene ; pos , positive ; neg , negative ; mac , myeloablative conditioning ; ric , reduced intensity conditioning ; rfs , relapse - free survival ; freq , frequency ; os , overall survival ; ci , condence interval . on patient outcomes and found no signicant difference in os based on the mutation number ( data supplement ) or number of mutated genes ( data supplement )  . patients with mds with excess blasts although the requirement for inclusion in the bmt - ctn 0901 study was , 5% marrow myeloblasts and no leukemic myeloblasts in blood on morphological analysis at the time of pretransplant assessment , a total of 22 of the 54 patients with mds ( 41% ) treated on the bmt - ctn 0901 trial had an initial diagnosis of refractory anemia with excess blasts ( raeb ) i or ii ( ie , between 5% and 19% blasts )  . 
seven of these samples tested positive for ngs10g , for which survival was 0% for ric ( n = 2 , relapse ) and 60% for mac - treated patients ( with one death from each relapse and transplantrelated mortality )  . 
ngs10g - positive patients accounted for four of six relapses observed in the raeb cohort , and the other two patients had high - risk cytogenetics with a monosomal karyotype that would not be detectable using this ngs assay . discussion here , we present the impact of genetic mutations detected before random assignment to ric or mac , identied without knowledge of the mutations originally present at diagnosis , on transplant outcomes in patients with mds . 
detection of mutations using a dna - sequencing panel covering regions of 10 genes , previously shown to have utility at the same timepoint in patients with aml , 10 was associated with increased rates of relapse and decreased rfs and os . 
 ( a ) differences in rates of relapse were identied between subgroups dened by conditioning intensity ( ric or mac ) and mutational status ( p , .001 ) , with the highest rate occurring in 10 - gene ngspositive ( ngsg10 - positive ) patients with mds receiving ric . 
the prognostic signicance of the remaining mutations on relapse was dependent on conditioning intensity , with higher rates of relapse and lower rfs observed in patients randomly assigned to receive ric compared with mac . this study provides evidence that the benet of mac versus ric in reducing relapse is found in patients with mds with detectable mutations using a 10 - gene region dnasequencing panel before allohct . 
patients are displayed in columns and grouped by conditioning intensity ( ric or mac ] ) and clinical outcome ( relapse , no relapse , or transplant - related mortality [ trm ] )  . 
genes are displayed in rows and sorted by diagnostic panel groupings , including 10 - gene ( prognostic in aml ) , dta ( associated with age - related clonal hematopoiesis ) , and 16 - gene ( commonly mutated in mds )  . 
although the size of this cohort limits extrapolation , it is possible that the prognostic implications of tp53 mutation detection in patients with mds before allohct and the impact of conditioning intensity differ from those reported previously when those variants are found at a level below the limit of detection of routinely used ngs assays . 
in addition to vaf , other factors such as persistence since initial diagnosis , development during therapy , mutation type , functional classication , and zygosity are likely to be important for determining the relapse risk associated with detecting a tp53 mutation.15 - 22 although mutation detection by targeted dna sequencing before allohct was strongly associated with increased relapse and decreased rfs and these outcomes could be improved with mac , unlike in patients10 with aml , we did not detect an os advantage for conditioning intensication in those testing positive . 
this might have been due to limited sample size , predominately nonrelapse causes of death in this mds cohort ( 67% of deaths , compared with 39% in the previously reported aml cohort ) , or other factors . mds is a genetically heterogenous disease.1 , 11 , 12 , 23 as was observed previously , 8 we found that inclusion of a large number of genes resulted in the majority of patients having mutations present before transplant . 
furthermore , mutations in genes associated with clonal hematopoiesis ( dta ) or 16 other mds - associated genes outside of 10 - gene improve test performance . mutational status did not reanalysis of pretransplant mutational status using only the 10 genes reported here , from another study of patients with mds with , 5% myeloblasts before allohct , 8 conrms our nding of signicantly increased relapse rates in patients testing positive and receiving ric versus mac . 
the modest there are several sample size here offers only a partial sampling of the heterogenous genetics associated with mds , whereas differences in pretransplantation disease burden , biology , and prior treatment history further limit exact comparisons . the signicance of mutation detection before allohct might be inuenced by history of prior treatment , and previous work using the same testing in patients with aml included only those treated to cytomorphological remission before transplant . 
 mds relapse after allohct allohct.9 two randomized studies of conditioning intensity in mds have failed to show a difference in survival between mac and ric , 4 , 6 , 25 although we show here a trend toward improved survival with increased conditioning intensity for those with detectable mutations particularly in the raeb group ( ie , biology and treatment history most analogous to aml )  . 
prior work had shown a benet for increased conditioning intensity in patients with mds with ras pathway mutations ( nras , kras , ptpn11 , cbl , nf1 , rit1 , flt3 , and kit ) undergoing allohct.9 as relapse is not primary cause of death in patients with mds undergoing allohct , the choice of conditioning intensity is currently dependent on the estimated ability of a patient to tolerate transplant - related toxicity.26 allohct remains the only curative therapy for mds ; however , given the median age at diagnosis , many patients will not be eligible for myeloablative approaches.27 , 28 as it is now possible to determine the genomic basis of disease before and after transplantation , personalized approaches for allohct of patients with mds are now conceivable with targeted strategies for those with detectable tp53 , ras pathway ( including flt3 ) , immune augmentation , or other therapies potentially able to supplement the impact of chosen conditioning intensity to minimize relapse risk.29 - 31 idh and jak2 mutations , in conclusion , we show that in adult patients with mds with , 5% marrow myeloblasts and no leukemic myeloblasts in blood before allohct , ultra - deep dna sequencing for mutations in 10 gene regions previously shown to be high risk in patients with aml could identify a subset of 42% of patients who experienced the majority of post - transplant relapses . 
the cibmtr registry is supported primarily by the u24 - ca76518 from nhlbi , nci , and the national institute of allergy and infectious diseases and from hhsh234200637015c ( hrsa / dhhs ) to the center for international blood and marrow transplant research . 
blood 122 : 2943 - 2964 , 2013 luger sm , ringden o , zhang mj , et al : similar outcomes using myeloablative vs reduced - intensity allogeneic transplant preparative regimens for aml or mds . bone marrow transpl 47 : 203 - 211 , 2012 shimoni a , hardan i , shem - tov n , et al : allogeneic hematopoietic stem - cell transplantation in aml and mds using myeloablative versus reduced - intensity conditioning : the role of dose intensity . 
leukemia 20 : 322 - 328 , 2006 kroger n , iacobelli s , franke gn , et al : dose - reduced versus standard conditioning followed by allogeneic stem - cell transplantation for patients with myelodysplastic syndrome : a prospective randomized phase iii study of the ebmt ( ricmac trial )  . 
j clin oncol 35 : 2157 - 2164 , 2017 pulsipher ma : reduced intensity for myelodysplastic syndrome : worth the gamble ? j clin oncol 35 : 2106 - 2108 , 2017 scott bl , pasquini mc , logan br , et al : myeloablative versus reduced - intensity hematopoietic cell transplantation for acute myeloid leukemia and myelodysplastic syndromes . 
j clin oncol 35 : 1154 - 1161 , 2017 bejar r , stevenson ke , caughey b , et al : somatic mutations predict poor outcome in patients with myelodysplastic syndrome after hematopoietic stem - cell transplantation . 
n engl j med 379 : 1028 - 1041 , 2018 lindsley rc , saber w , mar bg , et al : prognostic mutations in myelodysplastic syndrome after stem - cell transplantation . 
n engl j med 371 : 2477 - 2487 , jaiswal s , fontanillas p , flannick j , et al : age - related clonal hematopoiesis associated with adverse outcomes . 
montalban - bravo g , kanagal - shamanna r , benton cb , et al : genomic context and tp53 allele frequency dene clinical outcomes in tp53 - mutated 16 . 
coombs cc , zehir a , devlin sm , et al : therapy - related clonal hematopoiesis in patients with non - hematologic cancers is common and associated with adverse 18 . 
al - kali a , zblewski d , foran jm , et al : outcome of myelodysplastic syndromes over time in the united states : a national cancer data base study from 20042013 . 
sorror ml , sandmaier bm , storer be , et al : long - term outcomes among older patients following nonmyeloablative conditioning and allogeneic hematopoietic cell transplantation for advanced hematologic malignancies . 
maslah n , salomao n , drevon l , et al : synergistic effects of prima - 1met ( apr - 246 ) and azacitidine in tp53 - mutated myelodysplastic syndromes and acute myeloid leukemia . 
 entrectinib in trk and ros1 fusion - positive metastatic pancreatic cancer introduction the treatment of patients with metastatic pancreatic cancer ( paca ) has improved in recent years with the development of chemotherapy combinations ; however , the undeniable improvements in survival have been modest , and response rates remain low at approximately 25% to 35%.1 , 2 it is hoped that by identifying subgroups of patients with paca who harbor distinct actionable molecular alterations , major gains can be realized by using targeted therapies . 
for example , patients with paca who have homologous recombination deficiencypositive tumors may derive benefit with poly ( adp ribose ) polymerase inhibitorbased therapy , 3 - 5 and patients with mismatch repairdeficient / microsatellite instabilityhigh disease have demonstrated response to pembrolizumab.6 , 7 entrectinib ( rxdx - 101 ) is an investigational , cns - active , potent , selective inhibitor of the tyrosine kinases trka , trkb , trkc , ros1 , and alk encoded by ntrk1 , ntrk2 , ntrk3 , ros1 , and alk , respectively . 
8 gene fusions ( rearrangements ) of these target kinases have the potential to be oncogenic drivers , and they are present in small percentages across a variety of tumor types.9 in addition , they are mutually exclusive with other drivers.10 two phase i clinical studies ( alka - 372 - 001 [ first - in - human phase 1 study of entrectinib , an oral pan - trk , ros1 , and alk inhibitor , in patients with advanced solid tumors with relevant molecular alterations ] and startrk - 1 [ study of oral rxdx101 in adult patients with locally advanced or metastatic cancer targeting ntrk1 , ntrk2 , ntrk3 , ros1 , or alk molecular alterations ] ) that evaluated entrectinib in patients with extracranial solid tumors who harbored ntrk , ros1 , or alk gene fusions and who were tyrosine kinase inhibitor nave reported a response rate of 79% ( 19 of 24 ) .11 we present three patients with paca who harbor highly actionable gene fusions ( ntrk1 and ros1 ) who were treated in an ongoing phase ii trial of entrectinib ( nct02568267 ; basket study of entrectinib [ rxdx - 101 ] for the treatment of patients with solid tumors harboring ntrk 1 / 2 / 3 [ trk a / b / c ] , ros1 , or alk gene rearrangements [ fusions ] [ startrk - 2 ] )  . 
treatment duration with entrectinib ( 600 mg once per day ) ranged from approximately 7 months to more than 1 year , and one patient is still receiving treatment . patient 1 : tpr - ntrk1 fusion patient 1 is a 51 - year - old man who was diagnosed with stage iv paca in april 2015 , with lung , liver , and adrenal gland metastases . 
the first positron emission tomography / computed tomography ( pet / ct ) scan after the end of the first cycle ( october 18 , 2016 ) showed stable disease michael j . 
 ( b ) the tumors for patients 1 and 2 harbored a tpr - ntrk1 fusion , and ( c ) the tumor for patient 3 harbored an slc4a4 - ros1 fusion . 
 chr , chromosome ; tm , transmembrane domain . slc4a4 ros1 slc4a4 - ros1 fusion ( 9% by response evaluation criteria in solid tumors [ recist ] v1.1 ) along with a decrease in pet standardized uptake value , mainly in the liver ( figs 2a and 2b )  . 
the bone lesions and primary tumor remained stable , and his carbohydrate antigen 19 - 9 ( ca19 - 9 ) fell to 30 ku / l ( fig 2c )  . 
he gained 20 kg over approximately 3.5 months , which is a possible on - target effect of appetite enhancement as a result of trkb inhibition13 and not a manifestation of peripheral edema . 
in the last 2 months , he also developed hypogonadis he was still receiving entrectinib at the time of this report . patient 2 : tpr - ntrk1 fusion patient 2 is a 47 - year - old man who was diagnosed with borderline resectable paca in april 2016 . 
ngs with foundationone revealed a tpr - ntrk1 fusion ( fig 1 ) , cdkn2a / b loss , and kras wild type.14 on december 8 , 2016 , he started treatment with entrectinib ; at that time , he was rapidly losing weight . 
restaging ct scans on february 27 , 2017 , showed a partial response ( 32% by recist v1.1 ) , which was subsequently confirmed on april 24 , 2017 ( 38% ; fig 3a ) ; his ca19 - 9 fell to 9 ku / l by april 2017 ( fig 3b )  . 
treatment continued for approximately 8 months , at which time the ct scan showed continued response in the pancreas and liver and a slight increase in the size of a nontarget lesion in a portal lymph node . 
 ( b ) positron emission tomography / computed tomography scans at the start of entrectinib treatment ( baseline ) , after cycle 1 , and after cycle 2 demonstrating significant reduction of metabolic activity in liver metastases . 
 ( a ) axial images at the start of entrectinib therapy ( baseline ) , after cycle 5 , and after cycle 7 demonstrating a partial response to entrectinib with decreases in the size of the primary tumor in the pancreas and in liver metastases . 
 ( b ) carbohydrate antigen 19 - 9 ( ca19 - 9 ) biomarker levels during entrectinib treatment ; his ca19 - 9 level was 154 ku / l before starting entrectinib . patient 2 ca19 - 9 during entrectinib treatment ( start 8 december 2016 ) dec - 16 jan - 17 feb - 17 mar - 17 apr - 17 may - 17 jun - 17 jul - 17 aug - 17 the last ct scan in august 2017 showed progression in the portal lymph nodes and liver , and the patient discontinued the study . patient 3 : slc4a4 - ros1 fusion patient 3 is a 54 - year - old man who was diagnosed with metastatic paca in march 2016 . 
 previous treatments included a clinical trial of gemcitabine plus nab - paclitaxel with or without a notch inhibitor , folfirinox , and liver directed transarterial chemoembolization ( with gemcitabine , cisplatin , and mitomycin )  . 
testing with msk - impact , 15 a tumor - profiling multiplex panel , revealed that the tumor had several alterations , including a mutation in cdkn2a , somatic mutations in atm and brca2 , deletion of pik3ca , and amplification of erbb2 ( without her2 overexpression ) , but it was kras wild type . 
within 2 weeks of treatment , the patient experienced myalgias and fatigue , which abated with short - dose interruptions , and the patient resumed the highly active lifestyle he had at baseline , with a normal performance status and no loss of appetite or weight . 
he had a minor response ( a reduction of 12.5% ; stable disease per recist v1.1 ) and was considering definitive resection of the primary pancreatic mass , as well as metastasectomy of the liver disease . 
 discussion although paca remains a devastating disease , we are beginning to identify subgroups of patients whose disease harbors highly actionable molecular alterations , and therapies targeting these molecular alterations have the potential to significantly improve outcomes over standard therapy.1 , 2 , 16 here , we presented three patients with paca who harbored gene fusions and who were responsive to single - agent treatment with the investigational agent entrectinib . 
acquired resistance as a result of the development of secondary mutations that disrupt drug binding has been noted for many tyrosine kinase inhibitors.17 it is not known whether resistance mutations developed in these patients . 
 this effect , although it has been documented as an adverse effect of treatment , may be clinically meaningful considering the high incidence of cachexia in patients with paca.18 this is one of the first reports demonstrating such a substantial response in this specific subset of patients with this difficult - to - treat cancer . interestingly , the two patients with ntrk fusion positive tumors harbored tpr - ntrk1 gene fusions . 
this occurrence may be coincidental , because ntrk fusions can involve ntrk1 , ntrk2 , or ntrk3 and , to date , have been shown to combine with more than 25 fusion partners.17 furthermore , a different gene fusion partner for ntrk , etv6 - ntrk3 , was identified in an elderly patient with paca.19 these results strengthen the case for molecular profiling of patients with advanced paca . 
across more than 1 , 000 patients and samples tested , approximately 25% of patients have molecular alterations for which specific therapies are available.22 in a recent survey of 640 patients with paca who underwent molecular profiling , gene fusions were identified in 1% of the patients , most of which were targetable by entrectinib ( ntrk , ros1 , or alk fusions ) ( pishvaian et al , manuscript submitted for publication ) , which is similar to the percentage of patients with mismatch repairdeficient / microsatellite instability high tumors for which pembrolizumab was approved . 
furthermore , although kras mutations are present in > 90% of patients with pancreatic ductal adenocarcinoma ( pdac ) , 23 none of the gene fusionpositive tumors described here or in a previous report of alk fusion positive pdac24 harbored kras mutations . 
 notwithstanding small numbers , these combined observations suggest that fusions of ntrk , ros1 , or alk may be more likely in younger patients ( those younger than age 55 years ) with kras wild type pdac.24 in support of these observations , a recent analysis of 3 , 426 patients with pdac reported that approximately 12% were kras wild type . 
of these , kinase gene fusions were identified in 8% of pdacs that were kras wild type , 25 including five patients with alk fusions and three with ntrk fusions . 
pishvaian consulting or advisory role : ignyta , perthera ignacio garrido - laguna consulting or advisory role : ignyta stephen liu consulting or advisory role : ariad / takeda , genentech / roche , ignyta , pfizer edna chow - maneval employment : ignyta christian rolfo no relationship to disclose acknowledgments we thank the patients who gave consent to present their cases for the benefit of the scientific , medical , and patient communities worldwide ; laurens carp , md , department of nuclear medicine , and bart op de beeck , md , radiology department , antwerp university hospital , for help with imaging ; and meredith rogers , ms , cmpp , and nick cianciola , phd , of the lockwood group for providing editorial support funded by ignyta . 
liu , lombardi comprehensive cancer center , georgetown university , washington , dc ; ignacio garrido - laguna , huntsman cancer institute , university of utah , salt lake city , ut ; pratik s . 
lowery ma , kelsen dp , stadler zk , et al : an emerging entity : pancreatic adenocarcinoma associated with a known brca mutationclinical descriptors , treatment implications , and future directions . 
pishvaian mj , wang h , zhuang t , et al : a phase i / ii study of abt - 888 in combination with 5 - fluorouracil ( 5 - fu ) and oxaliplatin ( ox ) in patients with metastatic pancreatic cancer ( mpc )  . 
diaz la , marabelle a , delord jp , et al : pembrolizumab therapy for microsatellite instability high ( msi - h ) colorectal cancer ( crc ) and non - crc . 
de braud fg , pilla l , niger m , et al : phase 1 open label , dose escalation study of rxdx101 , an oral pan - trk , ros1 , and alk inhibitor , in patients with advanced solid tumors with relevant molecular alterations . 
drilon a , nagasubramanian r , blake jf , et al : a next - generation trk kinase inhibitor overcomes acquired resistance to prior trk kinase inhibition in patients with trk fusion - positive solid tumors . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multitargeted pan - trk , ros1 , and alk inhibitor entrectinib : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . 
murphy da , ely ha , shoemaker r , et al : detecting gene rearrangements in patient populations through a 2 - step diagnostic test comprised of rapid ihc enrichment followed by sensitive nextgeneration sequencing . 
perreault m , feng g , will s , et al : activation of trkb with tam - 163 results in opposite effects on body weight in rodents and non - human primates . 
 real - time genomic characterization of metastatic pancreatic neuroendocrine tumors has prognostic implications and identifies potential germline actionability purpose we assessed the usefulness of real - time molecular profiling through next - generation sequencing ( ngs ) in predicting the tumor biology of advanced pancreatic neuroendocrine tumors ( pannets ) and in characterizing genomic evolution . methods patients with metastatic pannets were recruited in the routine clinical practice setting ( between may 2014 and march 2017 ) for prospective ngs of their tumors as well as for germline analysis using the memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) sequencing platfor when possible , ngs was performed at multiple time points . results ngs was performed in 96 tumor samples from 80 patients . 
sequencing of preand post - treatment samples revealed tumor - grade progression ; clonal evolution patterns were also seen ( molecular resistance mechanisms and chemotherapy - associated mutagenesis )  . 
germline genetic analysis identified clinically actionable pathogenic or likely pathogenic variants in 14 of 88 patients ( 16% ) , including mutations in high - penetrance cancer susceptibility genes ( men1 , tsc2 , and vhl )  . conclusion a clinical ngs platform reveals pertubations of biologic pathways in metastatic pannets that may inform prognosis and direct therapies . 
2018 by american society of clinical oncology introduction pancreatic neuroendocrine tumors ( pannets ) represent 1% to 2% of all pancreatic neoplasms , but they have a rising incidence and prevalence.1 - 4 whole - exome and whole - genome sequencing , largely of resected pannets , has defined genomic events and improved our understanding of disease pathogenesis.5 , 6 these efforts have identified changes in chromatin remodeling , telomere maintenance , and mammalian target of nitya raj ronak shah zsofia stadler semanti mukherjee joanne chou brian untch janet li virginia kelly muyinat osoba leonard b . 
in addition to the well - characterized hereditary syndromes associated with pannet development ( multiple endocrine neoplasia 1 , von hippel - lindau syndrome , neurofibromatosis type 1 ) , recent data suggest the presence of germline alterations in dna damage repair genes in some patients.6 , 7 treatments for unresectable pannets include targeted and cytotoxic therapies , as well as liver directed approaches.8 - 13 no data exist to guide therapy for pannets with defined genomic alterations . 
in addition , disease heterogeneity poses a significant challenge in defining the selection and sequencing of therapy . to that end , using an institutional matched tumor - normal platform , we prospectively performed next - generation sequencing ( ngs ) of tumors in patients with metastatic well differentiated ( wd ) pannets . 
 we also hypothesized that pannets evolve over time with a more aggressive behavior that could be characterized biologically through ngs of repeat biopsies after treatment . methods study population written informed consent was obtained from patients with a diagnosis of wd pannet using a prospective , institutional review board approved protocol ( clinicaltrials.gov identifier : nct01775072 )  . 
pathologic features of the tumor samples ( differentiation and grade ) were determined according to the 2017 who classification , which recognizes the existence of a grade 3 ( g3 ) category within wd pannets ; historical values for differentiation and grade were collected through review of the electronic medical records . 
electronic medical records were also reviewed for patient data on demographics , treatments , and survival . sequencing of tumor samples ngs was performed using memorial sloan ketteringintegrated mutation profiling of actionable cancer targets ( msk - impact ) , a matched tumor - normal sequencing platform approved for clinical use by the new york state department of health , to detect base substitutions , small indels , copy number changes , and selected gene rearrangements.14 - 17 updated assay versions were released between 2014 and 2017 , and ngs of tumor tissue consisted of deep sequencing of all exons and selected introns of 275 ( preclinical pilot test ) , 341 ( version 1 ) , 410 ( version 2 ) , or 468 ( version 3 ) cancer - related genes . 
genotyping was performed using the pilot test for two of 96 samples ( 2% ) , version 2 for 16 of 96 samples ( 17% ) , version 3 for 57 of 96 samples ( 59% ) , and version 4 for 21 of 96 samples ( 22% )  . 
actionable genetic alterations were defined as changes that could guide therapy , including standard of care and investigational treatments ( annotated according to oncokb ) .18 germline sequencing germline variants from the .bam file of the normal dna sequence were called using the mutect and gatk haplotype caller as described previously ; all variants with < 1% population frequency in the exome aggregation consortium database were interpreted.19 , 20 germline analysis included 76 genes known to be associated with hereditary cancer predisposition , including all cancer predisposition genes identified in the american college of medical genetics and genomics guidelines.19 , 21 , 22 variants were interpreted on the basis of american college of medical genetics and genomics criteria . loss of heterozygosity loss of heterozygosity ( loh ) was determined through analysis of total , allele - specific , and integer dna copy number genome - wide using facets.23 statistical analysis descriptive statistics were used to characterize the study population and the somatic and germline genetic results . 
overall survival ( os ) , defined as the time from the date of first tissue acquisition ( from which ngs was completed ) until death or last known follow - up , was estimated by kaplan - meier methods . 
all p values were two sided , and p < .05 was considered to indicate statistical significance . results clinical characteristics as of march 2017 , ngs had been performed on 96 tumor samples from 80 patients ( eight patients with two samples analyzed ; four patients with three samples analyzed )  . 
in 29 patients , the primary tumor was sequenced , and in 58 patients , a metastatic tumor was sequenced ; in seven patients , both primary and metastases were sequenced ( in one instance , sequencing took place synchronously )  . 
recurrent somatic alterations occurred in key pathways and functional groups : chromatin remodeling factors ( crfs ) , histone methyltransferases ( hmts ) , and mtor pathway genes . somatic alterations in crfs ( daxx , atrx , pbrm1 , smarcb1 , arid5b , arid2 , arid1b , and arid1a ) were observed in 52 of 80 patients ( 65% )  . 
baseline patient characteristics ( continued ) wd pannets with msk - impact results systemic therapy somatostatin analogs ( octreotide long - acting release or lanreotide ) everolimus sunitinib platinum drug chemotherapy alkylating drug chemotherapy peptide receptor radionuclide therapy hepatic arterial embolization ( bland , radiotherapy , or chemotherapy ) 58 ( 73 ) 29 ( 36 ) 8 ( 10 ) 18 ( 23 ) 46 ( 58 ) 12 ( 15 ) 35 ( 44 ) note . 
 the clinical behavior of these tumors , including the single g1 tumor , was more aggressive . ten tumor samples ( collected from six patients ) harbored braf alterations : two of 10 g1 ( 20% ) , three of 10 g2 ( 30% ) , and five of 10 g3 ( 50% )  . 
 in addition to two tumors with v600e mutations , several non - v600 braf alterations were seen ( k601e , t599k , and t310i ) , and one tumor expressed both braf g596d and e451k mutations . survival with a median follow - up for survivors of 27.6 months , we observed 14 deaths ; median os was 118.9 months ( 95% ci , 99.6% - not achieved )  . 
tp53 alterations were observed in 10 of 80 patients ( 13% ) ; all were characterized as likely oncogenic . somatic loh in 50% of the genome was highly prevalent ; it was identified in 55 of 95 tested samples ( 58% )  . 
loh was observed recurrently in chromosomes 1 , 2 , 3 , 6 , 8 , 10 , 11 , 15 , 16 , 21 , and 22 ( appendix fig a1 )  . ngs results for the first sequenced sample in all patients are summarized in figure 1 . 
in the recurrently altered genes , there were no statistical differences in genetic spectrum on the basis of g1 versus g2 tumors , but a trend was noted of g2 and g3 tumors harboring tp53 , setd2 , and braf alterations . novel recurrently altered genes in this metastatic cohort , we observed a much higher frequency of setd2 alterations ( 14 of 80 patients [ 18% ] ) in comparison with previous investigations , and a novel finding of braf molecular mechanisms of resistance . 
genomic landscape of pancreatic neuroendocrine tumors , including the first sequenced sample for each patient ( n = 80 ) , as identified by the memorial sloan kettering - integrated mutation profiling of actionable cancer targets . 
 loh , loss of heterozygosity ; mb , megabyte ; mtor , mammalian target of rapamycin . post - treatment samples were available for three patients receiving the mtor inhibitor everolimus and for one patient receiving the braf v600e inhibitor vemurafenib . in all three patients receiving everolimus , mtor pathway alterations were identified at progression . 
on disease progression , a biopsy specimen revealed an oncogenic pten mutation ( q298 * ) , and the sampled areas of tumor progressed from g1 to g3 ( appendix figure a2 )  . 
this pten mutation was seen previously at a low allele frequency when the original pancreas tumor was sequenced , reflecting the possible emergence of this clone through targeted therapy . patient 2 received everolimus for 8 weeks , at which point treatment was held for infectious complications . 
a liver lesion increased in size and a biopsy was performed ; ngs identified a hotspot mutation in rheb ( y35s ) .25 subsequent sampling and ngs of this same liver lesion after 16 months of observation demonstrated the rheb alteration at a higher allele frequency . 
the msk - impact version used to sequence the pretreatment sample did not interrogate rheb , so the allele fraction of the rheb mutation is unknown in this sample ; however , it increased notably after treatment with andprogression on everolimus . patient 3 received everolimus for > 9 months before disease progression . 
at disease progression , ngs of a growing liver lesion demonstrated loss of this igf2 alteration , acquisition of a tsc2 splice site mutation ( x161_ splice ) , and an akt2 mutation ( g16d ; appendix figure a4 )  . 
surprisingly , no shared mutations were noted in sequencing of the two samples ; clinically , however , the disease was consistent with a single primary , suggesting the emergence of a previously unrecognized clone through treatment , although the possibility of a second primary cannot be excluded . patient 4 , whose tumor harbored a braf v600e mutation , enrolled in a basket clinical trial with vemurafenib and developed an nras hotspot mutation ( q61r ; appendix figure a5 ) .26 chemotherapy - associated mutagenesis . 
two patients received alkylating agents , and the third received oxaliplat a review of the tumors exposed to alkylating drugs showed that the variants shared by both samples were observed at a higher allele fraction compared with those unique to the individual samples , and the evolutionary pattern demonstrated a predominant c > t signature consistent with alkylating - agent associated mutagenesis ; in addition , consistent with previous observations , acquired alterations were observed in the mismatch repair genes for both tumors ( fig 3 ) .27 - 29 the sampled tumor in both patients increased from g1 to g3 . germline genetic testing germline testing for 76 cancer - associated genes was performed in 88 patients , 78 in the original prospective cohort and an additional 10 with surgically resected pannets . 
fourteen likely pathogenic germline alterations were identified in known cancer susceptibility genes ( 16% ) : three in established high - penetrance genes ( men1 , vhl , and tsc2 [ 3% ] ) , four in moderate - penetrance genes ( chek2 in four patients [ 5% ] ) , and seven in low - penetrance genes ( monoallelic mutyh in four patients and apc i1307k in three patients [ 8% ] )  . 
notably , we identified a germline tsc2 mutation in a 32 - year - old patient who did not exhibit the classic clinical features of tuberous sclerosis complex ( tsc ) and did not meet the criteria for tsc genetic testing ; magnetic resonance imaging of the brain identified tubers and radial bands , typical of tsc ( appendix figure a6 )  . 
among these patients , as best therapy response , two of 12 ( 17% ) had tumor regression , six of 12 ( 50% ) had stable disease , and one of 12 ( 8% ) had progressive disease ; three of 12 ( 25% ) are still receiving treatment . 
in the remaining 46 patients without somatic mtor pathway alterations , 17 of 46 ( 37% ) received everolimus ; five of 17 ( 29% ) had tumor regression , seven of 17 ( 41% ) had stable disease , four of 17 ( 24% ) had progressive disease , and there was an unknown response in one patient ( lost to follow - up )  . 
results from ngs led to the enrollment of three patients into clinical trials , but with little response noted . to our knowledge , this is the first study to evaluate the real - time clinical usefulness of ngs for patients with advanced , metastatic pannets . 
setd2 alterations have been implicated in the pathogenesis of many cancers ( breast , lung , acute lymphoblastic leukemia , renal cell carcinoma , and gliomas ) , supporting a role for setd2 as a tumor suppressor across many diseases.34 - 41 given our findings , one might consider closer monitoring and / or cytotoxic therapies in patients with setd2or table 3 . 
levels 1 and 2a include food and drug administration ( fda ) - recognized and standardof - care biomarkers predictive of response to an fda - approved drug for pancreatic neuroendocrine tumors . 
level 2b includes fda - approved biomarkers predictive of drug response in another cancer , but not fda or national comprehensive cancer network - compendium listed for pancreatic neuroendocrine tumors . 
level 3a includes alterations for which clinical evidence links the biomarker to drug response for pancreatic neuroendocrine tumors , but neither the biomarker nor the drug are standard of care in any cancer type . 
level 3b includes alterations for which clinical evidence links the biomarker to drug response for other cancers , but neither the biomarker nor the drug are standard of care in any cancer type . 
level 4 includes alterations in which preclinical evidence potentially links the biomarker to drug response , but neither the biomarker nor the drug are standard of care in any cancer type . abbreviation : msk - impact , memorial sloan kettering - integrated mutation profiling of actionable cancer targets . high penetrance high penetrance high penetrance moderate penetrance moderate penetrance moderate penetrance low penetrance low penetrance low penetrance recessive allele recessive allele braf - altered tumors and a higher burden of disease earlier in the treatment course . our study identifies pertubations of biologic pathways in metastatic pannets that were found in previous whole - exome and whole genome studies evaluating mostly localized pannets.5 , 6 we observed alterations largely along three pathways : crfs , hmts , and mtor . 
our study clarifies pannet genetics exclusively in the metastatic cohort , the group which gains immediate clinical value from realtime sequencing as we make steps toward precision medicine . in addition , we found that 16% of patients harbored a germline pathogenic or likely pathogenic alteration in high - , moderate - , or low - penetrance cancer predisposition genes . 
in looking at those patients found to have mutations in low or moderate - penetrance genes , it is notable that both chek2 and monoallaleic mutyh were noted in previous germline assessments of patients with pannets.6 notably , the patient in our series with a tsc2 germline mutation did not meet the clinical criteria for tsc genetic testing ; the identification of this mutation was incidental . 
 because mutations in men1 and tsc2 are two of the most common somatic findings in pannets , our finding of germline mutations within these two high - penetrance genes demonstrates the importance of these genes in pannet pathogenesis . 
although the contribution of the other germline alterations to pannet susceptibility has yet to be elucidated , our data suggest that there is likely a larger - than - anticipated germline contribution in this disease . 
given the lack of predictable phenotypic findings in most highand moderate - risk mutation carriers , combined with the relative rarity of this tumor subtype , consideration of genetic risk assessment for all patients with pannets is not unreasonable . 
such germline findings would have a profound impact on long - term cancer surveillance and cascade genetic testing of at - risk family members . in a small number of patients , somatic mutational signatures guided therapy . 
we identified somatic mtor alterations in a much greater proportion of patients ( 43% ) than described previously , but the presence or absence of an mtor pathway mutation was not predictive of response or resistance to treatment.8 our numbers are small , however , so additional work is needed to clarify the role of mtor pathway alterations in predicting response and / or resistance to targeted mtor pathway inhibitors . our series included only patients with wd tumors , and consistent with previous findings , rb1 alterations were essentially absent and were observed in only one post - treatment sample exposed to chemotherapy.43 , 44 wd pannets are often thought of as cancer in slower motion , and we have used our sequencing efforts to help clarify pannet evolutionary patterns over time and through therapy . 
in the 12 patients who underwent ngs of tumor tissue at multiple time points , we noted increased tumor grade in eight patients ( 67% ) , associated with marked genetic evolution after treatment . 
to our knowledge , we are the first to observe this evolutionary pattern in pannets.27 - 29 in conclusion , comprehensive molecular profiling of pannet samples using archival tissue is feasible . 
in a disease in which the natural history is thought to be indolent , we have demonstrated that the cancer transforms with grade and genetic progression over time and as therapy progresses . 
the practical usefulness of this analysis remains limited at this time ; our data suggest a higher - than - expected germline mutation rate , and consideration of genetic risk assessment for all patients with pannets is reasonable . 
in addition , given the heterogeneity of the disease , rapid , readily available , and clinically feasible ngs should be considered in clinical trials to help stratify these patients . 
specifically , our numbers are too small to clarify the genetic predictors of response or resistance to commonly used therapies in pannets , the prognostic effects of the identified genetic alterations , or the patterns of genetic evolution ( because only 12 patients underwent sequencing at multiple time points )  . 
klimstra , diane reidy - lagunes financial support : nitya raj , diane reidy - lagunes administrative support : nitya raj , joanne chou , virginia kelly , diane reidy - lagunes provision of study material or patients : nitya raj , leonard b . 
 data analysis and interpretation : nitya raj , ronak shah , zsofia stadler , semanti mukherjee , joanne chou , brian untch , janet li , muyinat osoba , leonard b . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . nitya raj research funding : novartis ( inst ) ronak shah no relationship to disclose leonard b . 
saltz consulting or advisory role : mcneil ppc ( i ) research funding : taiho pharmaceutical diana mandelker no relationship to disclose marc ladanyi honoraria : merck ( i ) consulting or advisory role : nccn / boehringer ingelheim afatinib targeted therapy advisory committee , national comprehensive cancer network / astrazeneca tagrisso request for proposal advisory committee research funding : loxo ( inst ) michael f . 
berger research funding : illumina zsofia stadler consulting or advisory role : allergan ( i ) ; genentech ( i ) , regeneron pharmaceuticals ( i ) , optos ( i ) , adverum ( i ) david s . 
klimstra stock and other ownership interests : paige.ai consulting or advisory role : wren laboratories , ipsen semanti mukherjee employment : regeneron pharmaceuticals stock and other ownership interests : regeneron pharmaceuticals research funding : regeneron pharmaceuticals diane reidy - lagunes honoraria : novartis consulting or advisory role : ipsen , pfizer , novartis research funding : novartis acknowledgment the authors thank the patients who kindly agreed to participate in this research effort . joanne chou no relationship to disclose brian untch no relationship to disclose support prior presentation affiliations nitya raj , ronak shah , zsofia stadler , semanti mukherjee , joanne chou , brian untch , janet li , virginia kelly , muyinat osoba , leonard b . 
presented , in part , as poster presentations at the 2015 gastrointestinal cancers symposium ( san francisco , ca , january 15 - 17 , 2015 ) and 2016 gastrointestinal cancers symposium ( san francisco , ca , january 21 - 23 , 2016 )  . 
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walter dm , venancio os , buza el , et al : systematic in vivo inactivation of chromatin - regulating enzymes identifies setd2 as a potent tumor suppressor in lung adenocarcinoma . 
tang lh , basturk o , sue jj , et al : a practical approach to the classification of who grade 3 ( g3 ) well - differentiated neuroendocrine tumor ( wd - net ) and poorly differentiated neuroendocrine carcinoma ( pd - nec ) of the pancreas . 
yachida s , vakiani e , white cm , et al : small cell and large cell neuroendocrine carcinomas of the pancreas are genetically similar and distinct from well - differentiated pancreatic neuroendocrine tumors . 
pathology demonstrated metastatic colloid / mucinous adenocarcinoma ( stage pt4a , pn2b , pm1c )  . immunohistologic testing for dna mismatch repair ( mmr ) proteins on tissue biopsy specimen showed preservation of muts protein homolog 2 ( msh2 ) and muts homolog 6 ( msh6 ) , but loss of mutl homolog 1 ( mlh1 ) and mismatch repair endonuclease pms2 ( pms2 ) , consistent with mmr deciency . 
initially , the patient was treated with four doses of uorouracil , leucovorin , oxaliplatin , and irinotecan ( folfoxiri ) until computed tomography scanning revealed an increase in peritoneal masses and liver metastases . 
he then was treated with pembrolizumab on the basis of mmr deciency ; however , this was discontinued after three doses when scans revealed progressive disease , and a doubling of carcinoembryonic antigen since initiation was noted ( 401 ng / ml to 848 ng / ml )  . 
all patient information was curated under an institutional review board protocol ( mcc 19161 ) , which was formally reviewed and granted approval by moftt cancer center ( mcc )  . 
this institutional review board protocol includes a waiver of consent , because no identifying information is reported in the case . a foundationone cdx test ( foundation medicine , cambridge , ma ) was ordered on the diagnosed omental tissue with subsequent review by the personalized medicine clinical service ( pmcs ) at mcc for guidance regarding future therapeutic options ( table 1 )  . 
the molecular tumor board ( mtb ) discussion focused on approaches for targeted therapeutic considerations in a patient with high tumor mutation burden ( tmb ) after disease progression on an immune checkpoint inhibitor . the patient had 93 reported alterations ; the foundationone cdx report provided interpretive content for 26 of them for correlated therapies with clinical benet , clinical trials , or therapies with a lack of response . 
in a patient with high tmb status and microsatellite instability ( msi ) , the likelihood of an individual alteration primarily driving the cancer is difcult to ascertathe pmcs categorized alterations into common repair / signaling pathways , associating the alterations with possible therapies and ranking therapeutic options on the available evidence ( table 1 )  . 
figure 1 and appendix table a1 illustrate the workow taken by the pmcs to identify and prioritize treatment options . of the 26 alterations for which foundationone cdx provided interpretive content , impaired homologous repair ( hr ) was a commonly altered pathway . 
highlight alterations with targeted therapies tmb : high ( 105 muts / mb ) microsatellite status : unstable kras a59t atm r2227c brca2 n319fs * 8 nf1 i679fs * 21 ptch1 r1308fs * 64 akt1 e17k msh6 f1088fs * 2 men1 r612h mtor a469t apc h298fs * 28 apc r1114 * apc v2194fs * 5 arid1a g889fs * 2 asxl1 g646fs * 12 bcorl1 p1681fs * 20 ctcf t204fs * 18 keap1 f478fs * 2 mll2 p2354fs * 30 notch3 a1701v notch3 g2035fs * 60 notch3 p1317fs * 103 pbrm1 w992fs * 23 ptpn11 s502p qki k134fs * 14 setd2 f1650v sox9 v306fs * 77 pold1 r17q flt1 s733del 66 vus 2 . 
categorize by mechanism tmb - high msh6 arid1a brca2 akt1 kras * nf1 * mmr deficiency mmr deficiency mmr deficiency hr deficiency hr deficiency hr deficiency akt activation ras activation ras activation 3 . 
correlate mechanisms to therapies parp or atr inhibitor second line of immunotherapy ( combination therapy or novel agent on trial ) pi3k - akt - mtor inhibitor arid1a brca2 tmb - high msh6 arid1a brca2 akt1 4 . 
 ( 3 ) correlating grouped repair / signaling mechanisms from step 2 with possible targeted therapy options assists collecting and correlating supporting evidence to be considered by a molecular tumor board ( mtb )  . 
 ( 4 ) the mtb reviewed the evidence and prioritized therapy options according to the patients current disease state , current failed line of therapy , patient preference , strength of evidence associated with an alteration and therapy option , and available clinical trials . 
nct03188965 ( first - in - human study of atr inhibitor bay1895344 in patients with advanced solid tumors and lymphomas ) was recruiting patients with atm alterations and was further supported by clinical , in vivo , and in vitro data . 
 ( * ) the kras a59t and nf1 i679fs * 21 alterations produced conicting likelihoods of response to epidermal growth factor receptor ( egfr ) inhibitors and were based on minimal case report data . 
 nelson et al ( parp ) inhibitors or immunotherapy.2 , 3 parp inhibition in the context of brca alterations has demonstrated clinical benet in breast , ovarian , and prostate cancer and has produced discussion of expansion to other ddr deciencyrelated alterations.4 atm encodes a protein kinase that plays a key role in dna repair , cell cycle checkpoints , and apoptosis in response to dna damage.5 the atm r2227c alteration is clinically relevant , because it produces a missense alteration in the frap - atm - trrap ( fat ) domain , has been categorized as deleterious in breast cancer and adenoid cystic carcinoma , and is classied as pathogenic by clinvar ( clinvar / )  . 
in a phase ii trial of patients with ddr - defective metastatic castrate - resistant prostate cancer receiving olaparib , patients with germline or somatic alterations in genes involved in ddr showed signicantly increased activity , with responses occurring in 14 out of 16 patients ( 88% ) .6 , 7 the at - rich interactive domain - containing protein 1a ( arid1a ) g889fs * 2 alteration is likely inactivating ( catalogue of somatic mutations in cancer mutation id : cosm6911235 )  . arid1a is a subunit of the chromatin remodeling complex swi / snf that is involved in facilitating access of proteins to dna , and inactivating alterations are common across various cancer types.8 pathways involved in ddr have been shown to interact with arid1a , including msh2 . 
during dna replication , it has been demonstrated that arid1a recruits msh2 to chromatin and promotes mmr.8 thus , inactivation of arid1a has been shown to impair mmr . arid1a deciency has demonstrated sensitization to parp inhibitors in vitro and in vivo.9 atr , another important genetic component of ddr , has been the target of novel investigational drugs that inhibit atr and arid1a signaling in vitro and in vivo.5 , 10 collectively , arid1a , atm , and brca2 produce a common theme of ddr / hr deciency , which leads to atr or parp inhibition alone or in combination with platinum or another dna - damaging chemotherapy agent in an off - label or ( more preferred ) clinical trial setting were recommended as viable options . akt1 e17k has been reported as a missense alteration that occurs in the pleckstrin homology domain of rac - alpha serine / threonine - protein kinase ( akt1 ) and activates akt signaling leading to inhibition of cell apoptosis and promotion of cellular proliferation.11 this alteration is therefore considered oncogenic and is well described in the literature . 
in a phase i , dose - escalation trial of the pan - akt inhibitor azd5363 , 58 patients with solid tumor found to have somatic akt1 e17k alterations were enrolled . 
the median progression - free survival was 5.5 months for patients with estrogen - positive breast cancer , 6.6 months for patients with gynecologic disease , and 4.2 months for patients with other solid tumors , including two patients with colorectal cancer ( crc ) .12 however , in a patient with a high tmb and msi , the value of this akt1 e17k mutation as a clinically relevant driver is unclear . 
in case the clinical team decided to target akt , clinical trials , including nct02465060 ( nci - match - arm z1k ) , nct03310541 , or nct02761694 , could be considered . finally , the kras a59t alteration is less common than other known activating kras alterations but has been reported as resulting in increased activation of the map kinase and pi3k pathways in vivo.13 interestingly , this alteration may demonstrate an exception to the observation that patients with kras - mutated metastatic crc do not receptor respond to epidermal growth factor ( egfr ) targeted monoclonal antibodies cetuximab or panitumumab . 
there is one case report of a patient with metastatic crc and the kras a59t alteration who was treated with panitumumab plus uorouracil , leucovorin , and irinotecan and experienced a partial radiographic response ( 36% decrease per response evaluation criteria in solid tumors 1.1 ) , stable carcinoembryonic antigen biomarker , and decreased size of metastases for an 8 - month duration.14 the patient showed no other alterations in exons 2 and 3 of kras , nras , and hras genes ; exon 15 of braf ; and exons 2 , 5 , 9 , 10 , 20 , and 21 of pik3ca . this seems to be the rst observed documentation of the a59t allele not producing resistance to egfr - targeting monoclonal antibodies and may provide a potential future consideration for our patient.14 however , there is limited evidence that the nf1 frame shift may predict poorer response to cetuximab or panitumumab therapy on the basis of a small case series of four chinese patients with metastatic crc who were kras g12 and g13 wt but found to have inactivating nf1 alterations . 
the alterations involved in hr deciency ( brca2 , atm , and arid1a inactivation ) provided the most robust combined evidence of predicted response to future therapy options . the akt1 e17k alteration is known to be activating , but its importance in a highly mutated , unstable tumor was less well dened . 
 therapy option prioritization in crc with high mutation burden follow - up of the patients case , unfortunately , showed that after three treatments of pembrolizumab , there was no sign of response , which led the clinical team to refer back to the above options to consider treatment beyond immunotherapy . 
the clinical team discussed the predominant grouping of alterations ( arid1a , atm , and brca2 ) with the common theme of ddr / hr deciency and ultimately decided to enroll the patient in a clinical trial ( clinicaltrials.gov identier : nct03188965 ) investigating the atr inhibitor bay1895344 in patients with solid tumor with atm loss . the lesson learned with this patient was one of categorizing a large list of alterations and prioritizing each according to therapeutic targets on the basis of dominant signaling / repair pathways and strength of available evidence . 
in doing so , the pmcs was able to provide the treating physician with a succinct , prioritized grouping of alterations validating the initial line of therapy and considerations for future therapeutic options , which led to the patient being enrolled in a clinical trial with the greatest anticipated therapeutic benet . 
walko , pharmd , 12902 magnolia dr , tampa , fl 33612 ; twitter : @mofttnews ; e - mail : christine.walko@moftt.org. support supported in part by national cancer institute comprehensive cancer center support grant no . 
mcleod leadership : cancer genetics stock and other ownership interests : cancer genetics , interpares biomedicine honoraria : genentech , illumina consulting or advisory role : gentris , cancer genetics , saladax biomedical , national institutes of health / national cancer institute , admera health , evicore healthcare , pharmazam speakers bureau : genentech christine m . 
walko employment : mission healthcare stock and other ownership interests : alexion pharmaceuticals ( i ) consulting or advisory role : foundation medicine , jackson laboratory for genomic medicine , intermountain precision genomics other relationship : mission hospital no other potential conicts of interest were reported . references cerniglia m , xiu j , grothey a , et al : association of dna damage response and repair genes ( ddr ) mutations and microsatellite instability ( msi ) , pd - l1 expression , tumor mutational burden ( tmb ) in gastroesophageal cancers . 
j clin oncol 37 , 2019 ( suppl 4 ; abstr 60 ) overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - decient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
lancet oncol 18 : 1182 - 1191 , 2017 ghiringhelli f , richard c , chevrier s , et al : efciency of olaparib in colorectal cancer patients with an alteration of the homologous repair proteworld j gastroenterol 22 : 10680 - 10686 , 2016 pili e pg , gay cm , byers la , et al : parp inhibitors : extending benet beyond brca - mutant cancers . 
clin cancer res 25 : 3759 - 3771 , 2019 shiloh y , ziv y : the atm protein kinase : regulating the cellular response to genotoxic stress , and more . 
n engl j med 373 : 1697 - 1708 , 2015 shen j , ju z , zhao w , et al : arid1a deciency promotes mutability and potentiates therapeutic antitumor immunity unleashed by immune checkpoint blockade . 
nat med 24 : 556 - 562 , 2018 shen j , peng y , wei l , et al : arid1a deciency impairs the dna damage checkpoint and sensitizes cells to parp inhibitors . 
banerji u , dean ej , p erez - fidalgo ja , et al : a phase i open - label study to identify a dosing regimen of the pan - akt inhibitor azd5363 for evaluation in solid tumors and in pik3ca - mutated breast and gynecologic cancers . 
mei z , shao yw , lin p , et al : smad4 and nf1 mutations as potential biomarkers for poor prognosis to cetuximab - based therapy in chinese metastatic colorectal cancer patients . 
ninety - three alterations were reported on the foundationone cdx report ( including variants of known and unknown signicance )  . twenty - six of the alterations had interpretive content for correlated therapies with clinical benet , clinical trials , or therapies with a lack of response . 
twenty - seven alterations had potentially relevant information ( maf , listed in exac , protein domain location , in oncokb and others ) as reported in the initial screening of ndings . 
 c not so typical : development of atypical chronic myeloid leukemia in a patient with chronic myeloid leukemia introduction chronic myeloid leukemia ( cml ) is a myeloproliferative neoplasm characterized by the uncontrolled production and proliferation of mature well - differentiated granulocytes . 
the hallmark of cml is the translocation of the abelson murine leukemia ( abl1 ) gene on chromosome 9 and the breakpoint cluster region ( bcr ) gene on chromosome 22 ( bcr - abl ) , which results in the abnormal chromosome 22 , the philadelphia ( ph ) chromosome . 
since the approval of imatinib in 2001 , 1 cml has been treated with tyrosine kinase inhibitors ( tkis ) , which has improved the survival of patients with cml to close to that of the normal population.2 although cml itself has been associated with an increased risk of secondary primary malignancies ( spms ) suggestive of an inherent stemcell defect , treatment has been implicated in this phenomenon as well.3 the data on the risk for spms among patients treated with tkis have been conflicting.3 - 6 this discrepancy may be due to the limiting retrospective nature of these studies , heterogeneity across patients , and possible lack of a significant effect . 
however , it is interesting to note that most of the reported spms were solid malignancies , with few cases of chronic monomyelocytic leukemia , lymphoid neoplasms , and plasma cell neoplasms . 
she achieved major molecular response at 30 months and complete molecular response ( > 4 log reduction ) at 40 months , and she had remained in hematologic , cytogenetic , and molecular remission since 2007 with no additional karyotypic abnormalities . in october of 2016 , the patient presented with progressive fatigue . 
she was diagnosed with acml on the basis of the who criteria of prominent dysplastic granulopoiesis , > 10% immature myeloid cells in peripheral blood , and no increase in absolute monocytes . 
bm was sent for next - generation sequencing ( performed at genoptix , carlsbad , ca ) to interrogate 40 genes that are known to be recurrently mutated in myeloid malignancies . 
mutational analysis showed alterations in setbp1d868n ( 49% variant allele frequency ) , nrasg12d ( 19% ) , cblc396y ( 17% ) , runx1g12d ( 47% ) , and gata2r396q ( 47% )  . 
no plans for allogenic hematopoietic cell transplantation were made because of her age and frailty . discussion to our knowledge , this is the first case report of acml occurring in a patient with cml who is in complete remission receiving long - term imatinib therapy . 
secondary hematologic neoplasms reported in the previous studies occurred primarily in older patients , suggesting that a possible antecedent clonal hematopoiesis of indeterminate potential ( chip ) progressed while cml was well controlled on tkis.2 , 10 , 11 recent genomic studies have demonstrated the clonal diversity in the evolution of cml and showed that the mutational persistence does not alter the response to tkis . 
these mutations are predominantly in epigenetic machinery ( tet2 , asxl1 , and dnmt3a ) that are commonly attributed to the development of chip.12 a recent report by kim et al10 detected a spectrum of mutations in patients with cml after tki therapy . 
another theory is that the bcr - abl translocation is an acquired event on top of preexisting chip mutations , thereby converting ph - negative clones into ph - positive clones that lead to cml . 
these ph - positive clones are eliminated by tkis , and the ph - negative clones gain additional mutations such as setbp1 to progress to acml.12 on the basis of large population - based studies , chip is seen at an incidence of 10% to 20% in persons age 70 to 80 years.13 unfortunately , our patient did not have prior sequencing performed that could have identified common chip mutations . focused gene sequencing in this case identified gene mutations that support the diagnosis of acml . 
somatic mutations of genes associated with proliferation signaling are frequently mutated in myeloproliferative neoplasms ; setbp1 is involved in dna replication , cbl encodes e3 ubiquitin - protein ligase , nras is involved in growth factor signaling , and runx1 encodes core binding factor and is involved in normal hematopoiesis.14 acml specifically is associated with frequent setbp1 and nras mutations.15 , 16 furthermore , it is distinguished from chronic neutrophilic leukemia by the absent to rare finding of jak2 and csf3r mutations.17 , 18 morgana is another important factor in the pathogenesis of acml . 
interestingly , low levels of morgana were also found in 16% of patients with typical cml and correlated with a poor response to imatinib.20 testing for this specific gene is not widely available and could not be performed for this patient . although there have been reports of rare pedigrees with genetic predisposition to cml , 21 , 22 the literature does not support any familial aggregation in the general population.23 likewise , family history in our patient was noncontributory , and dna germline sequencing was not deemed necessary or cost effective . 
the median survival of patients with acml is 25 months , with progression to acute myeloid leukemia in 40% of patients at a median duration of 18 months.28 leukocytosis , female sex , and older age have been shown to be adverse prognostic factors for overall survival in multiple studies.16 , 25 , 28 in summary , we present here a patient with cml in the chronic phase who responded to tki therapy for nearly 13 years before developing bcr - ablnegative disease that best fits the diagnosis of acml . 
nras and cbl have also been shown to be drivers of malignant transformation and probably occurred as later events.24 setbp1 mutations are associated with leukocytosis , anemia , and thrombocytopenia at presentation and are often associated with cbl in acml . 
presence of setbp1 mutations in patients with acml is associated with worse overall survival in one study15 but not another.25 other mutations ( ie , tet2 , asxl1 ) have been described in acml and can also be seen in healthy individuals26 , 27 but were not detected in our patient . 
more importantly , next - generation sequencing was not routinely done at the time of the patients initial diagnosis , nor is it currently the standard of care at diagnosis . 
druker bj , tamura s , buchdunger e , et al : effects of a selective inhibitor of the abl tyrosine kinase on the growth of bcr - abl positive cells . 
voglova j , muzik j , faber e , et al : incidence of second malignancies during treatment of chronic myeloid leukemia with tyrosine kinase inhibitors in the czech republic and slovakia . 
verma d , kantarjian h , strom ss , et al : malignancies occurring during therapy with tyrosine kinase inhibitors ( tkis ) for chronic myeloid leukemia ( cml ) and other hematologic malignancies . 
au wy , ma sk , kwong yl : the occurrence of philadelphia chromosome ( ph ) negative leukemia after hematopoietic stem cell transplantation for ph positive chronic myeloid leukemia : implications for disease monitoring and treatment . 
miranda mb , lauseker m , kraus mp , et al : secondary malignancies in chronic myeloid leukemia patients after imatinib - based treatment : long - term observation in cml study iv . 
schmidt m , rinke j , schfer v , et al : molecular - defined clonal evolution in patients with chronic myeloid leukemia independent of the bcr - abl status . 
meggendorfer m , bacher u , alpermann t , et al : setbp1 mutations occur in 9% of mds / mpn and in 4% of mpn cases and are strongly associated with atypical cml , monosomy 7 , isochromosome i ( 17 ) ( q10 ) , asxl1 and cbl mutations . 
patnaik mm , barraco d , lasho tl , et al : targeted next generation sequencing and identification of risk factors in world health organization defined atypical chronic myeloid leukemia . 
 palbociclib for the treatment of metastatic nasopharyngeal carcinoma with cdk4 amplication : a case report xiao - dong jiao , md1 ; ke liu , md1 ; bao - dong qin , md , phd1 ; ying wu , md1 ; ming - qin lin , md1 ; jun liu , md1 ; xi he , md1 ; junjun liu , md2 ; han han - zhang , phd2 ; jianxing xiang , phd2 ; hao liu , ms2 ; and yuan - sheng zang , md , phd1 introduction nasopharyngeal carcinoma ( npc ) , which causes approximately 65 , 000 deaths annually , is an epithelial malignancy with unique geographic distribution . 
although rare in western countries , its incidence exceeds 20 cases per 100 , 000 people in the endemic area , including in southern china , southeast asia , and the middle east / north africa.1 , 2 factors that contribute to the pathogenesis of npc include but are not limited to epstein - barr virus infection , host genetics , and environmental factors . 
although optimal local control has been achieved and the overall prognosis has significantly improved in recent years as a result of the development of intensity - modulated radiotherapy and the adoption of concurrent chemotherapy , 3 , 4 distant metastasis remains a major challenge in the management of npc . 
during radiotherapy , rapid onset of a bilateral sensorineural hearing loss occurred but did not progress beyond moderate impairment . complete remission was achieved after the completion of radiotherapy ; however , 6 months later , follow - up positron emission tomography / computed tomography scan revealed multiple hypermetabolic nodules of the bilateral lung , indicating recurrence . 
he was subsequently treated with nimotuzumab and unfortunately experienced disease progression with an enlarged mass with a total diameter of 59.1 mm after 6 weeks ( fig 2a )  . 
this revealed cdk4 amplication ( copy number , 6.62 ) , among other mutations with no targeted therapy available , including copy number variations in kdm5a , etv6 , nfe2l2 , mdm2 , daxx , pnrc1 , tiparp , and tnfaip3 , as well as single - nucleotide variations in nfkbia , pik3cg , bap1 , and rad5 . 
the patient subsequently began palbociclib 125 mg / d on june 12 , 2017 , for 14 consecutive days followed by 7 days off therapy , comprising a complete cycle of 21 days . 
he experienced grade 3 neutropenia , thrombocytopenia , and myelosuppression , which resulted in interruptions of the treatment two times , a total of 14 days during the rst four cycles . 
 jiao et al capture - based targeted sequencing was performed on biopsy of lung tumor tissue and revealed mutations in cdkn2a / 2b , ccnd1 , cyld , bap1 , arid5b , pik3cg , notch1 , and mdm4 . 
the patient was subsequently switched to ribociclib . discussion in this case study , we have presented clinical evidence of palbociclib in an elderly patient with metastatic npc , highlighting the potential of cdk4 inhibitors for the treatment of metastatic npc , a devastating condition with median overall survival that ranges from 5 months to 11 months.20 , 21 currently , combined chemoradiotherapy is the predominant treatment strategy for patients with metastatic disease , but benets are surprisingly modest.21 - 24 as a result of the lack of comprehensive understanding of the molecular pathogenesis associated with npc , targeted therapy is relatively underdeveloped . 
to our knowledge , there is only one other study reporting the efcacy of palbociclib as a salvage treatment in a patient with metastatic ccnd1 - amplied npc who achieved stable disease as a best response with a pfs of 4 months.19 numerous lines of evidence from both in vitro and in vivo perspectives , as well as from the clinical setting , have demonstrated the potential of cdk4 inhibitors for treating npc . 
at the protein level , rb , cyclin d1 , and its regulator cdk4 are overexpressed in 90.6% , 92% , and 71% of respectively.26 numerous studies have npc tissues , demonstrated that npc cell lines and patient - derived xenografts that harbor mutations in the cdk4 pathway are sensitive to cdk4 / 6 inhibitors.19 , 27 in addition , some studies have shown the prognostic value of cdk4 overexpression.28 it has been reported that the serum level of cdk4 is signicantly elevated in patients with lung cancer and head and neck squamous cell carcinoma and is associated with a more aggressive clinical behavior and shorter survival , which suggests its potential as a biomarker in clinical practice.28 in addition , other studies have shown that cdk4 overexpression is an independent prognostic indicator of distal metastasis and local recurrence.14 available data support the idea that amplication is primarily responsible for cdk4 overexpression . in conclusion , we have reported on an elderly patient with cdk4 - amplied npc who was treated with palbociclib and achieved pr with a pfs of 15 months . 
what is the most clinically relevant biomarker for palbociclib ? what is the most appropriate way to select patients for this treatment ? the patient provided written informed consent and gave permission for the use of biopsies and the publication of case details . 
the patient achieved partial remission ( pr ) with considerable shrinkage of lung lesions , which measured 40.5 mm after 6 months of treatment . disease remained as pr until august 2018 when a ct scan revealed enlarged lesions of bilateral lung measuring 64.4 mm , accompanied by the development of malignant pleural effusion with a progression - free survival ( pfs ) of 15 months ( figs 2b and 2c and 3 )  . 
 ( a ) before the initiation of palbociclib , enlarged masses with a total diameter of 59.1 m ( b ) at partial response , a signicant lesions was observed , measuring 40.5 mm after shrinkage of 6 months of palbociclib treatment . 
lancet 387 : 1012 - 1024 , 2016 paul p , deka h , malakar ak , et al : nasopharyngeal carcinoma : understanding its molecular biology at a ne scale . 
 jiao et al pan c - c , lu j , yu j - r , et al : challenges in the modication of the m1 stage of the tnm staging system for nasopharyngeal carcinoma : a study of 1027 cases and review of the literature . 
exp ther med 4 : 334 - 338 , 2012 leung tw , tung sy , sze wk , et al : treatment results of 1070 patients with nasopharyngeal carcinoma : an analysis of survival and failure patterns . 
head neck 27 : 555 - 565 , 2005 lee aw , sze wm , au js , et al : treatment results for nasopharyngeal carcinoma in the modern era : the hong kong experience . 
int j radiat oncol biol phys 61 : 1107 - 1116 , 2005 baujat b , audry h , bourhis j , et al : chemotherapy in locally advanced nasopharyngeal carcinoma : an individual patient data meta - analysis of eight randomized trials and 1753 patients . 
int j radiat oncol biol phys 64 : 47 - 56 , 2006 sherr cj , beach d , shapiro gi : targeting cdk4 and cdk6 : from discovery to therapy . 
cancer res 65 : 854 , 2005 ( suppl ) jiang q , mai c , yang h , et al : nuclear expression of cdk4 correlates with disease progression and poor prognosis in human nasopharyngeal carcinoma . histopathology 64 : 722 - 730 , 2014 14 . 
chen t - j , lee s - w , lin l - c , et al : cyclin - dependent kinase 4 overexpression is mostly independent of gene amplication and constitutes an independent prognosticator for nasopharyngeal carcinoma . 
rugo hs , di eras v , gelmon ka , et al : impact of palbociclib plus letrozole on patient - reported health - related quality of life : results from the paloma - 2 trial . 
hsu c - l , lui k - w , chi l - m , et al : integrated genomic analyses in pdx model reveal a cyclin - dependent kinase inhibitor palbociclib as a novel candidate drug for nasopharyngeal carcinoma . 
zhang l , huang y , hong s , et al : gemcitabine plus cisplatin versus uorouracil plus cisplatin in recurrent or metastatic nasopharyngeal carcinoma : a multicentre , randomised , open - label , phase 3 trial . 
lancet 388 : 1883 - 1892 , 2016 jin y , shi yx , cai xy , et al : comparison of ve cisplatin - based regimens frequently used as the rst - line protocols in metastatic nasopharyngeal carcinoma . j cancer res clin oncol 138 : 1717 - 1725 , 2012 [ erratum : j cancer res clin oncol 141 : 767 , 2015 ] 23 . 
chen l , hu c - s , chen x - z , et al : concurrent chemoradiotherapy plus adjuvant chemotherapy versus concurrent chemoradiotherapy alone in patients with locoregionally advanced nasopharyngeal carcinoma : a phase 3 multicentre randomised controlled trial . 
tan t , lim w - t , fong k - w , et al : concurrent chemo - radiation with or without induction gemcitabine , carboplatin , and paclitaxel : a randomized , phase 2 / 3 trial in locally advanced nasopharyngeal carcinoma . 
hwang c - f , cho c - l , huang c - c , et al : loss of cyclin d1 and p16 expression correlates with local recurrence in nasopharyngeal carcinoma following radiotherapy . 
zhang w , zeng z , zhou y , et al : identication of aberrant cell cycle regulation in epstein - barr virus - associated nasopharyngeal carcinoma by cdna microarray and gene set enrichment analysis . 
wong c - h , ma bby , hui cwc , et al : preclinical evaluation of ribociclib and its synergistic effect in combination with alpelisib in non - keratinizing nasopharyngeal carcinoma . 
bliss , msc1 ; ian smith , md2 ; and mitch dowsett , phd1 , 2 on behalf of the poetic trial management group and trialists purpose although aromatase inhibitor ( ai ) treatment is effective in estrogen receptorpositive postmenopausal breast cancer , resistance is common and incompletely explained . 
scnas to specic genes may drive intrinsic resistance , or high genomic instability may drive tumor heterogeneity , which allows differential response across tumors and surviving cells to evolve resistance to treatment rapidly . 
fifty - six samples from the ai group included 28 poor responders ( prrs , less than 60% reduction in protein encoded by the mki67 gene [ ki - 67 ] ) and 28 good responders ( gdrs , greater than 75% reduction in ki - 67 )  . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction estrogen deprivation is the major treatment strategy for hormone - dependent breast cancer ( bc ) and typically involves agents that inhibit aromatase , the enzyme that catalyzes the conversion of androgens to estrogens . despite near - complete suppression of circulating estrogen levels by aromatase inhibitor ( ai ) treatment , acquired and de novo resistance to ai is common.1 few pretreatment biomarkers exist for ai resistance , and mechanisms of resistance are incompletely understood.2 mutations and somatic copy number alterations ( scnas ) can play important roles in activating oncogenes or inactivating tumor suppressors , and bc is characterized by multiple recurrent scnas and few recurrent mutations.3 we have previously shown that tp53 mutations ( tp53mut ) occur at a higher rate in tumors with poor response to ai treatment , which suggests that these patients received less benet from ai4 but that scnas to specic genes also may play an important role in ai resistance.5 nonspecic genomic alterations , like high genomic instability , are known to be associated with poor prognosis and probably at least partly the result of tumor heterogeneity , which allows some cells to survive and evolve resistance to treatment.6 there is evidence in other solid tumors of an association between high genomic instability and intrinsic resistance to chemotherapy.7 however , few studies of genomic instability and response to endocrine treatment exist . 
 schuster et al context key objective our study was focused on understanding the link between somatic copy number alterations ( scnas ) and intrinsic resistance to aromatase inhibitor ( ai ) therapy , and we observed that tumors with high levels scnas had intrinsic resistance to therapy . knowledge generated a well - established link exists between high genomic instability and tp53 mutations and resistance to cancer treatment ; however , we are the rst to our knowledge to show that primary estrogen receptor ( er ) positive tumors with high genomic instability have an intrinsic resistance to treatment that can be measured after a short , 2 - week ai treatment . 
high genomic instability tumors do not require time to evolve resistance to estrogen deprivation therapy because they already have de novo resistance to treatment . relevance estrogen deprivation therapy with ai treatment is highly effective in er - positive breast cancer , but more than 20% of postmenopausal women with early - stage breast cancer suffer a relapse . 
the perioperative endocrine therapyindividualizing care ( poetic ) phase iii trial with 2 weeks of perioperative ai therapy offers the opportunity to identify mechanisms and biomarkers of intrinsic ai resistance , and in the poetic trial , up to 20% of tumors showed resistance to ai treatment after just 2 weeks of treatment . 
validation of these results in a larger study would provide a framework for better stratifying patients into high risk of ai resistance who are likely to benet from added or alternative treatment . therefore , was to determine whether genome - wide measures of scnas ( ie , genomic instability ) and / or focal scnas are associated with intrinsic resistance to ai treatment . response to ai treatment can be measured by change in the proliferation marker protein encoded by the mki67 gene ( ki - 67 ) after 2 to 4 weeks of presurgical therapy , and ai resistance in primary tumors can be characterized and dened by limited or no ki - 67 response to ai treatment.8 - 10 this change in ki - 67 has been found to predict benet from endocrine therapy better than clinical response.10 we therefore extended our earlier study on the relationship between mutations and resistance to ais in the presurgical perioperative endocrine therapyindividualizing care ( poetic ) trial . 
poor responders ( prrs ; n = 28 ) were dened as having a ki - 67 decrease of less than 60% between baseline and surgery and good responders ( gdrs ; n = 28 ) as having a greater than 75% ki - 67 decrease . 
patients with intermediate ki - 67 decrease between 60% and 75% were not considered . exome sequencing was available for 72 tumors from a previous study.4 samples from 17 patients who received no ai also were analyzed to ensure that changes in scnas ascribed to ai treatment were not artifactual . 
aliquots were taken from 10 tumor dna samples and assessed as technical replicates ( data supplement )  . dna extractions eight - micrometer sections were taken from rnalaterstored core - cuts embedded in optimal cutting temperature compound ( cryo - m - bed , bright instruments , luton , united kingdom ) and stained with nuclear fast red ( 0.1% weight - to - volume ratio )  . 
 genomic instability and resistance to ai treatment blood using the ez1 system ( life technologies , carlsbad , ca )  . snp array analysis human omniexpressexome v.3 beadchip ( illumina , san diego , ca ) was used to generate genotype and intensity data for blood and tumor samples , and allele - specic copy number analysis of tumors ( ascat ) 13 was used for the estimate of ploidy , fraction of tumor cells , and cnas in the tumor samples . 
either the segmentation penalty in ascat was increased ( 22 samples ) or the estimate of ploidy and purity from oncosnp was used in ascat ( four samples ) to generate scna calls that best described the data . 
data have been deposited in the european genome - phenome archive ( egas00001001940 )  . measures of genomic instability chromosomal gains and losses were determined relative to estimates of tumor ploidy by ascat ( sum of major and minor allele calls minus tumor ploidy rounded to the nearest integer )  . 
the median percentage of the genome with scnas was 46% for tumors , with a single representative tumor sample chosen from matched baseline , surgery , or technical replicate samples to calculate the median percentage of scnas . 
the median percentage of the genome with gains relative to tumor ploidy , losses relative to tumor ploidy , and loh was 15% , 16% , and 15% , respectively ( fig 1b )  . highly recurrent scnas ( gains at 1q , 16p , 20q , and 8q and losses / loh at 11q 16q , 17p , and 8p ) occurred in more than 50% of all representative samples . 
the majority of sites with losses overlapped with loh ( data supplement ) , as expected.17 , 18 intratumoral heterogeneity of scnas overlap of scnas between paired core - cuts . 
of note , these samples had the highest genomic instability , with more than 90% of the genome with scnas ( p088 samples )  . overall scna calls in baseline and surgery ai pairs were similar ( data supplement ) , with the median overlap for scnas at 87% and 88% for 33 baseline / surgery ai pairs and 11 no - ai pairs . 
there was no signicant difference between the frequency of discordant snca calls between baseline and surgery ai pairs after correction for multiple testing , and only 4% of 47 , 807 nonoverlapping regions had greater than 10% more events in baseline or surgery samples ( more than four additional scna events in the baseline or surgery samples in the 33 pairs )  . 
for pairs of baseline and surgery samples , the median percentage the genome with discordant scna calls was 5% ( fig 1c ) , and discordance between samples was associated with the percentage of the genome with scnas . there was only one paired set of core - cuts in which discordant scnas were greater than the scnas shared between the pair of samples , which suggests two independently evolved tumors . discordance in prr and gdr paired samples . 
there was a trend for prrs to have more discordant scnas between paired samples than gdrs ( prr average , 10% ; gdr average , 6% ) , but this difference was not signicant . 
however , the variance in the percentage of the genome with discordant scnas was signicantly greater in prrs than in gdrs ( p , .001 , f test ; fig 1d )  . 
 e gdrs ki - 67 > 75% prrs ki - 67 < 60% controls no ai all scnas ( genomic instability ) gains losses schuster et al gdrs prrs controls baseline - surgery tumor pairs gdrs prrs controls fig 1 . 
 ( a ) arrow plot showing the change in the protein encoded by the mki67 gene ( ki - 67 ) between baseline and surgery for good responder ( gdr ) , poor responder ( prr ) , and untreated control samples ( controls as determined by immunohistochemistry scores )  . 
 ( b ) box plot showing percentage of the genome with somatic copy number alterations ( scnas ) , gains relative tumor ploidy , losses relative to tumor ploidy , loss of heterozygosity ( loh ) , and homozygous deletion ( hd ) for 127 tumor samples . 
 ( c ) bar plot and ( d ) box plot showing the average percentage of genome discordance between pairs of core - cuts ( baseline and surgery ) for all scnas . 
there was an enrichment of poor prognosis intrinsic subtypes ( prr nonluminal / luminal b ) in prr samples ( 64% ) compared with gdr samples ( 20% ) ; however , more than 30% of measured prr samples were luminal a subtypes , which suggests that fully capture intrinsic subtyping did not the higher risk of recurrence in these samples ( data supplement )  . comparison between prrs and gdrs in percentage of genome altered . 
given the overall concordance between baseline and surgery core - cuts in scnas and the results of previous observations of minimal impact of ai treatment on mutation counts , 4 we merged all the scna events from multiple samples from the same tumor to represent the scna events in that tumor ( baseline and surgery , 35 events ; baseline , surgery , and technical replicates , nine events ; baseline technical replicates , one event )  . 
 ( a ) box plot showing the difference in genomic instability ( the percentage of genome with somatic copy number alterations [ scnas ] ) between good responder ( gdr ) and poor responder ( prr ) tumors . 
 ( b ) comparisons of protein encoded by the mki67 gene ( ki - 67 ) baseline immunohistochemistry scores with genomic instability ( the percentage of the genome with scnas ) for gdr , prr , and untreated control samples ( controls , blue )  . 
 ( c ) comparisons of ki - 67 surgery immunohistochemistry scores after aromatase inhibitor treatment with genomic instability ( the percentage of the genome with scnas ) for prrs and gdrs . 
the percentage of a chromosomal arm with gains , losses , and loh was calculated , and prrs showed a signicantly higher percentage of gains in 6p ; losses in 5q ; and loh in 10q , 17p , and 19p ( fdr , 0.1 , one - sided mann - whitney u test ; figs 3a to 3c )  . 
the largest difference in percent values ( mean and median ) for arms between gdrs and prrs was observed in loh at 17p ( figs 3d to 3g ) followed by loh in 8p and gains in 8q . 
these regions had approximately 40% more events in prrs ( 10 to 13 more scna events in the 28 prr samples v gdr samples , respectively ) but were not signicant after multiple correction . tp53 alterations occurrence of tp53mut and loh in cohort . 
our previous work from exome sequencing showed prrs and tp53mut associated with a higher mutational mutational load was correlated with ki - 67 levels at surgery after 2 weeks of ai treatment.4 we did not observe a signicant correlation between the percentage of the genome load and that load , but we did observe with scnas and mutational greater genomic instability in tumors with tp53mut ( fig 4e )  . as expected for a tumor suppressor , loh at the tp53 locus in 17p was associated with tp53mut across all tumors ( which drove loss of the functioning copy of the tumor suppressor gene ; p = .004 , fishers exact test )  . 
of the 17 patients with tp53 mutations in baseline or surgery samples , 15 had loh at the tp53 locus ( nine prr , ve gdr , and three control samples )  . 
there was a signicant enrichment of tp53 genomic alterations in prrs ( p = .03 , fishers exact test ) and a signicant difference in the distribution of tp53 genetic alterations between prrs and gdrs ( p = .02 , 2 test ; fig 4a )  . ai resistance and tp53 status . 
 ( a ) percentage of samples with gains relative to tumor ploidy for poor responders ( prrs ; dark red ) and good responders ( gdrs ; light red ) , ( b ) with losses for gdrs ( light blue ) and prrs ( dark blue ) , and ( c ) with loss of heterozygosity ( loh ) for gdrs ( light green ) and prrs ( dark green ) at 47 , 807 segments generated from the somatic copy number alteration ( scna ) analysis of perioperative endocrine therapyindividualizing care ( poetic ) tumor samples . 
 ( d ) percentage of samples with loh ( gdrs , light green ; prrs , dark green ) for chromosome 17 ( chr17 ) , including ( e ) a table for loh events at tp53 and ( f ) the difference in the percentage of samples with loh between prrs and gdrs . 
bar plot showing the percentage of good responder ( gdr ) and poor responder ( prr ) samples with tp53 wild type ( tp53wt ) and no loss of heterozygosity ( loh ) at the tp53 locus , tp53wt and loh at the tp53 locus , tp53 mutation ( tp53mut ) and no loh at the tp53 locus , and tp53mut and loh at the tp53 locus . 
box plots showing ( b ) the percent change in the protein encoded by the mki67 gene ( ki - 67 ) , ( c ) the ki - 67 baseline immunohistochemistry scores , ( d ) the ki - 67 surgery immunohistochemistry score , and ( e ) genomic instability ( the percentage of the genome with somatic copy number alterations [ scnas ] ) for prrs with tp53wt and no loh at the tp53 locus , tp53wt and loh at the tp53 locus , and tp53mut and loh at the tp53 locus . 
the results with her2 - negative samples were similar to those with all samples , with the most signicant differences between prrs and gdrs being loss at 5q and loh at 17p for her2 - negative samples . 
there was also a signicant enrichment of tp53 genomic alterations in prrs ( p = .02 , fishers exact test ) and a signicant difference in the distribution of tp53 genetic alterations between prrs and gdrs in her2 - negative samples ( p = .03 , 2 test )  . discussion our primary goal was to identify global and focal scnas that were associated with the antiproliferative response of erpositive bc to short - term estrogen deprivation using ais . our selection of samples from more than 3 , 000 patients in the ai group from the poetic trial aimed to exploit this large study to understand good / poor response to ai treatment in a general er - positive bc population but not to represent the trial population per se . 
the sampling of tumors before and after 2 weeks of ai treatment allowed the impact of tissue heterogeneity to be assessed , and prior exome sequencing gave the opportunity to integrate the scna and mutation data to better understand intrinsic resistance . 
 schuster et al not change signicantly in the nearly 3 , 000 poetic aitreated patients within the 2 - week treatment window ( data not shown ) , which indicates little opportunity for selection of resistant cells in that time . 
reduced heterogeneity might be observed from longer treatment.20 these data , therefore , indicate that a small biopsy sample before or after short - term ai treatment is likely to be representative of the whole tumor for most bcs ; however , for tumors with high genomic instability and greater heterogeneity , multiple biopsy samples may be necessary to capture all genomic alterations . there is a large body of evidence to associate genomic instability with poor outcomes in solid tumors , 6 and incorporation of genomic instability scores can greatly improve molecular prognostic models for bc.21 , 22 it is not known whether high genomic instability and greater tumor heterogeneity allow the few surviving tumors to evolve resistance to ai treatment or whether there is intrinsic resistance to ai in these tumors . 
loh and mutations in tp53 have been shown to result in worse outcomes , 23 and we have now shown that it is also associated with poor antiproliferation response to ai and intrinsic resistance to treatment . 
even in tumors with high er expression and good prognosis , tp53 genomic alterations can result in worse outcomes . work by other groups has associated mutations in dna repair pathways25 or mismatch repair pathways19 and coamplication of fgfr1 and ccnd15 with resistance to ai treatment , but we have not observed enrichment of these genomic alterations in our prrs . 
this may be the result of small samples sizes in each study and additional differences in how ai resistance is classied : we classied response / resistance on the basis of changes of ki - 67 between baseline and ai - treated tumors because this dynamic assessment relates to benet from treatment . 
others have used the level of residual ki - 67 in ai - treated tumors as the end point to dene resistance , which reects residual risk of recurrence while on ais . 
of note , a patient with a large reduction in proliferation after treatment has clearly beneted from and responded to ai treatment , regardless of her residual risk on the basis of ki - 67 measurements at surgery.26 we conclude that the poor prognosis of er - positive postmenopausal tumors associated with high genomic instability , tp53 loh , and tp53mut is due at least in part to intrinsic resistance of these tumors to ai therapy . 
short , 2 - week ai treatment can reveal poor antiproliferative response in these primary tumors , which indicates that they continue to proliferate in an estrogen - deprived environment and do not require additional evolution to enable the tumor to resist treatment . 
j clin oncol 27 : 1382 - 1387 , 2009 l opez - knowles e , wilkerson pm , ribas r , et al : integrative analyses identify modulators of response to neoadjuvant aromatase inhibitors in patients with early breast cancer . 
nat genet 45 : 1127 - 1133 , 2013 gellert p , segal cv , gao q , et al : impact of mutational proles on response of primary oestrogen receptor - positive breast cancers to oestrogen deprivation . 
nat commun 7 : 13294 , 2016 giltnane jm , hutchinson ke , stricker tp , et al : genomic proling of er + breast cancers after short - term estrogen suppression reveals alterations associated with endocrine resistance . 
j natl cancer inst 99 : 167 - 170 , 2007 ellis mj , suman vj , hoog j , et al : ki67 proliferation index as a tool for chemotherapy decisions during and after neoadjuvant aromatase inhibitor treatment of breast cancer : results from the american college of surgeons oncology group z1031 trial ( alliance )  . 
dowsett m , smith ie , ebbs sr , et al : short - term changes in ki - 67 during neoadjuvant treatment of primary breast cancer with anastrozole or tamoxifen alone or combined correlate with recurrence - free survival . 
l opez - knowles e , gao q , cheang mc , et al : heterogeneity in global gene expression proles between biopsy specimens taken peri - surgically from primary er - positive breast carcinomas . 
haricharan s , punturi n , singh p , et al : loss of mutl disrupts chk2 - dependent cell - cycle control through cdk4 / 6 to promote intrinsic endocrine therapy resistance in primary breast cancer . 
quenel - tueux n , debled m , rudewicz j , et al : clinical and genomic analysis of a randomised phase ii study evaluating anastrozole and fulvestrant in postmenopausal patients treated for large operable or locally advanced hormone - receptor - positive breast cancer . 
haricharan s , bainbridge mn , scheet p , et al : somatic mutation load of estrogen receptor - positive breast tumors predicts overall survival : an analysis of genome sequence data . 
 de novo esr1 hotspot mutation in a patient with endometrial cancer treated with an aromatase inhibitor adeline morel , md1 ; julien masliah - planchon , phd1 ; guillaume bataillon , md2 ; v eronique becette , md2 ; claire morel , msc3 ; samantha antonio1 ; elodie girard , md4 ; ivan bi `eche , phd1 , 5 ; christophe le tourneau , md , phd3 , 4 , 6 ; and maud kamal , phd3 introduction endometrial carcinoma is the fourth most frequent cancer in women . 
endometrial carcinoma is classied into two subtypes : type 1 endometrial carcinoma characterized by estrogen receptor ( er ) expression and obesity , and type 2 endometrial carcinoma in nonobese , older women . 
type 1 endometrial carcinoma is associated with a favorable prognosis , whereas type 2 has a poorer prognosis.1 a prognostic genomic classication of endometrial cancers into four groups has been established using exome sequencing ; however , this classication is not used in the clinic.2 standard - of - care treatment of endometrial carcinoma consists of primary hysterectomy , bilateral salpingooophorectomy , and pelvic lymph node dissection followed by adjuvant therapy based on the histologic assessment of the specimen.3 chemotherapy is proposed in the recurrent and / or metastatic setting , whereas hormone therapy represents a treatment option for patients with er expression.4 in breast cancer , esr1 mutations were clearly identied as a mechanism of resistance to aromatase inhibitors.5 - 8 esr1 mutations were reported in 2% of endometrial cancers , 9 yet their potential occurrence following hormonal therapy is unknown . 
the diagnosis of grade 1 endometrioid carcinoma was conrmed , with less than 50% invasion of the myometrial wall thickness , 4 cm in greatest dimension , lymphovascular invasion , bilateral ovarian metastases , and no pelvic lymph node metastases ( pt3an0 f ed eration internationale de gyn ecologie et dobst etrique iiia )  . 
using immunohistochemistry , tumor cells were shown to express er , progesterone receptor , and a wild - type staining of p53 . in addition , tumor cells expressed ck7 and pax8 and did not express ck20 , ttf1 , cdx2 , and wt1 , conrming the endometrial origin of the tumor . ( ie , letrozole )  . 
after nine cycles of chemotherapy , the patient received maintenance therapy with an aromatase inhibitor receiving letrozole for 6 months , the patient experienced disease progression and was subsequently treated with doxorubicin and cyclophosphamide and then carboplatin alone . 
the patient was then biopsied in the framework of the shiva02 trial ( evaluation of the efcacy of targeted therapy based on tumor molecular proling in patients with advanced cancer using each patient as its own control ; clinicaltrials.gov identier : nct03084757 ) , which aimed to identify druggable molecular alterations , and received a fourth line of chemotherapy with gemcitabine ( fig 1 )  . molecular proling was performed on a frozen biopsy of a metastatic lymph node in the shiva02 trial using a dedicated targeted sequencing panel covering 80 genes . 
in patients with breast cancer , esr1 hotspot mutations in the ligand - binding domain were observed exclusively after hormone therapy5 - 8 and have been shown to be associated with poor prognosis.11 after exposure to aromatase inhibitors , the prevalence of esr1 mutations was signicantly higher in patients exposed during the metastatic phase than during the adjuvant phase ( 36% v 6% ) .11 in a recent study , advanced breast cancer tumors harboring esr1 mutations , or alterations in genes involved in the mitogenactivated protein kinase pathway and in the er transcriptional machinery , were shown to barely benet from aromatase inhibitors.5 esr1 amplications were detected in 12% of endometrial carcinomas , 12 whereas esr1 hotspot mutations were less frequent ( 2% ) .9 esr1 amplications were shown to be associated with a poor prognosis and seemed to be an early event in endometrial carcinoma development.12 selective er degraders , such as fulvestrant , were shown to be effective in patients with hormone receptorpositive breast cancer . 
esr1 mutations were not reported to be associated with clinical resistance to fulvestrant.13 to our knowledge , our case report is the rst to report a potential de novo esr1 mutation in a patient with erpositive endometrial carcinoma treated with an aromatase inhibitor . 
curr opin obstet gynecol 29 : 47 - 58 , 2017 kokka f , brockbank e , oram d , et al : hormonal therapy in advanced or recurrent endometrial cancer . 
cochrane database syst rev ( 12 ) : cd007926 , 2010 razavi p , chang mt , xu g , et al : the genomic landscape of endocrine - resistant advanced breast cancers . 
cancer cell 34 : 427 - 438.e6 , 2018 robinson dr , wu y - m , vats p , et al : activating esr1 mutations in hormone - resistant metastatic breast cancer . 
nat genet 45 : 1446 - 1451 , 2013 toy w , shen y , won h , et al : esr1 ligand - binding domain mutations in hormone - resistant breast cancer . 
nat genet 45 : 1439 - 1445 , 2013 bartels s , christgen m , luft a , et al : estrogen receptor ( esr1 ) mutation in bone metastases from breast cancer . 
mod pathol 31 : 56 - 61 , 2018 backes fj , walker cj , goodfellow pj , et al : estrogen receptor - alpha as a predictive biomarker in endometrioid endometrial cancer . 
schiavon g , hrebien s , garcia - murillas i , et al : analysis of esr1 mutation in circulating tumor dna demonstrates evolution during therapy for metastatic breast 12 . 
spoerke jm , gendreau s , walter k , et al : heterogeneity and clinical signicance of esr1 mutations in er - positive metastatic breast cancer patients receiving mol endocrinol 10 : 1388 - 1398 , 1996 cancer . 
a study of patients with myeloid malignancy compared the response rate of trametinib among patients with ras wild - type ( n = 30 ) and ras - mutated mds or aml ( n = 50 )  . 
five patients with ras - mutated mds or aml achieved a complete response ( cr ) or cr with incomplete platelet recovery compared with no patients with ras wild - type mds or aml.5 herein , we describe a patient with relapsed mds after undergoing allogeneic stem - cell transplant ( allo - sct ) who had next - generation sequencing ( ngs ) identifying map2k2 p298l , for which the patient received trametinib plus decitabine and achieved a durable cr . 
the map2k2 p298l mutation has been identified previously in a patient with lung cancer , but the functional significance at the protein level has not yet been elucidated.6 the patient is a 52 - year - old asian woman with a 12 - year history of jak2 - negative essential thrombocythemia ( et ) treated with anagrelide ( 10 years ) and hydroxyurea ( 2 years )  . 
time points indicate number of months after transplantation each next - generation sequencing panel was obtained . dnmt3a tet2 calr map2k runx1 mutations , notably runx1 s141 * ( mutation allele frequency [ maf ] , 12% ) , zmym3 g49wfs * 13 ( maf , 27% ) , calr k368rfs * 51 ( maf , 39% ) , and map2k2 p298l ( maf , 30% )  . 
after a 1 - month treatment interruption , the mucositis resolved and treatment resumed with decitabine 20 mg / m2 intravenously on days 1 through 3 of a 28 - day cycle and trametinib 2 mg daily for 21 days of a 28 - day cycle . 
after resolution , treatment with decitabine 20 mg / m2 intravenously on days 1 through 5 of a 28 - day cycle and trametinib 0.5 mg daily for 7 days of a 14 - day cycle continued without additional issues . 
instead , a benign pdgfrb t88i ( maf , 47% ) alteration and tet2 h1380y ( maf , 5% ) and dnmt3a r882s ( maf , 15% ) mutations were identified ( fig 1 ; data supplement )  . subsequently , a donor pb sample was analyzed by a clinical laboratory improvement amendments - certified moffitt 54 - genetargeted myeloid ngs panel8 with an average coverage of 11 , 987 reads . 
a benign asxl1 g652s variant was detected in the patient and the related donor ( maf , 49% ) , likely reflecting a heterozygous germline variant detected in both persons as a result of shared inheritance . 
 this acquired mutation in the patient suggests donor - derived acquisition of a chip mutation . at the time of this report , the patient was without gvhd symptoms , received a donor lymphocyte infusion ( dli ) 16 months after trametinib initiation , and remains in cr 18.5 months after trametinib initiation ( 29.5 months after allo - sct )  . 
 the primary oncologist felt that a dli may achieve the best long - term outcomes because there are no long - term efficacy data of trametinib plus a hypomethylating agent ( hma ) in relapsed mds after allo - sct . 
the patient continues to receive treatment with trametinib and decitabine without evidence of dysplasia or relapse . discussion protein function in the presence of map2k2 p298l has not been previously characterized to our knowledge . 
this map2k2 alteration is located in a proline - rich segment of the protein kinase domain , is near a map2k2 phosphorylation site , and has been observed previously in cancer.6 additionally , per the catalog of somatic mutations in cancer , the map2k2 p298l alteration had been identified as somatic and pathogenic per their prediction tool.11 despite not knowing the functional significance of the alteration , a clinical response was observed after the administration of trametinib and decitabine . 
 the 2 - year os was 12.4% and in those achieving a cr after azacitidine administration , the 2 - year os was 48.4%.12 therefore , it is difficult to determine to what degree , if any , the clinical benefit observed could be attributed to trametinib , because hmas with or without dli have demonstrated clinical efficacy in patients with relapsed mds after sct transplant . adverse effects and their management with trametinib plus decitabine has not been previously discussed to our knowledge . 
based on phase ii data , trametinib was not believed to result in the infectious complications experienced in our case.4 trametinib and decitabine were held to evaluate the etiology of the adverse effects of dermatitis and mucositis , for which a biopsy specimen demonstrated gvhd . 
kevin hicks no relationship to disclose lia perez no relationship to disclose eric padron honoraria : incyte , cell therapeutics , cell therapeutics ( inst ) research funding : incyte ( inst ) rami s . 
kim kb , kefford r , pavlick ac , et al : phase ii study of the mek1 / mek2 inhibitor trametinib in patients with metastatic braf - mutant cutaneous melanoma previously treated with or without a braf inhibitor . 
borthakur g , popplewell l , boyiadzis m , et al : activity of the oral mitogen - activated protein kinase kinase inhibitor trametinib in ras - mutant relapsed or refractory myeloid malignancies . 
kahle , phd1 ; ann marie bailey , phd1 ; chetna wathoo , md1 ; kavitha balaji , phd1 ; mehmet esat demirhan , md1 , dong yang , phd1 ; milind javle , md1 ; ahmed kaseb , md1 ; cathy eng , md1 ; vivek subbiah , md1 ; filip janku , md , phd1 ; victoria m . 
mills shaw , phd1 , and funda meric - bernstam , md1 purpose cell - free dna ( cfdna ) next - generation sequencing is a noninvasive approach for genomic testing . 
of these patients , 438 ( 76.2% ) had at least one alteration detected , and 205 ( 35.7% ) had one or more alterations of high potential for clinical action . 
trials were identied in 80% of patients ( 286 of 357 ) with any alteration and in 92% of patients ( 188 of 205 ) with one or more alterations of high potential for clinical action of whom 57.6% ( 118 of 205 ) had 6 or more months of follow - up available . 
of these patients , 10% ( 12 of 118 ) had received genomically matched therapy through enrollment in clinical trials ( n = 8 ) , off - label drug use ( n = 3 ) , or standard of care ( n = 1 )  . 
2019 by american society of clinical oncology introduction molecular proling of tumors through circulating cellfree dna ( cfdna ) has gained signicant traction in recent years because of its noninvasiveness , sensitivity , and quick turnaround time.1 - 4 for patients with advanced cancers , specically those who have either exhausted their solid tumor block or have quickly progressed on compelling intervening therapy , repeat invasive tissue biopsy is necessary to identify driver mutations and / or resistance mechanisms that arise in tumor evolution / response to treatment or natural progression.3 , 5 in addition , a single sample can serve as a global representation of the mutational landscape across multiple metastatic lesions.6 - 8 together , these attributes make cfdna testing especially attractive for patients with advanced cancer where a quick clinical decision is necessary to identify genomically relevant clinical trials . functional annotation , assignment of potential clinical actionability , and clinical trial matching to guide clinical decision making on the basis of cfdna testing . 
in this prospective study of 575 patients with advanced cancers , we provided such postprocessing to evaluate the clinical utility of cfdna testing in identifying clinically actionable genomic alterations . this entailed the delivery of personalized annotation reports , including functional interpretation of variants and retrieval of genomically relevant clinical trials . however , physicians were allowed to order testing and initiate treatments without waiting for results , as appropriate . 
 s anchez et al context key objective what is the frequency of actionable alterations in patients with advanced / metastatic cancer who undergo cell - free dna ( cfdna ) testing ? knowledge generated in this study , of 575 patients who had cfdna testing , 76.2% had at least one alteration detected and 35.7% had one or more alterations of high potential for clinical action . 
criteria for enrollment were active metastatic / local inoperable advanced cancer , consideration of clinical trial enrollment within the next two lines of therapy , and exhausted tissue block or archival tissue older than 1 year or available tissue block but progression on compelling intervening therapy . 
human investigations were performed after approval by the md anderson institutional review board and in accordance with an assurance led with and approved by the us department of health and human services . comprehensive genomic testing in plasma cfdna was extracted from whole blood collected in 10 - ml streck tubes . 
only variants that occurred within an actionable gene were annotated.17 , 18 a gene is considered actionable if it has an established biologic role in cancer and there is a clinically available drug to which the gene confers sensitivity or resistance , where actionability can be applicable to all or select alteration or tumor types . 
of note , other genes are included in the guardant360 panel , such as tumor suppressor genes , which may not be targetable , but clonal driver mutations in the highest allele these genes are usually variants at fractions , which makes them ideal candidates to index the degree of tumor dna shedding into the bloodstream and to determine the relative subclonality of other variants in the same sample . dening a variants potential for clinical action variants reported in an actionable gene were annotated as follows : ( cid : 129 ) functional signicance ( fs ) : activating , activating inferred , inactivating , inactivating inferred , inactivating and neomorphic , unknown , or likely benign ( cid : 129 ) actionable variant call ( avc ; from highest level of evidence [ loe ] to lowest ) : yes : literature - based ( peerreviewed scientic literature ) ; yes : functional genomics ( institute for personalized cancer therapy internal functional genomics platform ) ; yes : inferred ( intermediate loe includes inferences dictated by the type of alteration and is mostly applicable to frameshift / truncation alterations where loss of region is inferred to be activating / inactivating ) ; potentially ( lower loe where there are indirect and / or limited data to support the function of a specic alteration ) ; unknown ; or no ( fs call is likely benign or inactivating alteration in an oncogene ) ( cid : 129 ) actionable for call : the combination of an fs call and avc : therapeutic intervention , resistance to drugs , or enrollment in select clinical trials . finally , gene actionability can be applicable to all , or specic , tumor types . 
although specic food and drug administration approved indications and / or national comprehensive cancer network guidelines are not included within this parameter , the upstream annotation process depends on gene - level actionability . 
the workow for categorizing a variants potential for clinical action is illustrated in the data supplement . clinical trials identied on the basis of patient genomic prole trial retrieval was restricted to variants that were deemed actionable and to trials available at the md anderson cancer center at the time of patient annotation . patient follow - up patients were followed for at least 6 months after the initial annotation to collect treatment decisions , performance status ( ps ) , and trial screening / enrollment ( and reasons for eligibility / ineligibility )  . results patient characteristics we enrolled 575 patients into the study . 
consistent with this , single nucleotide variants were the most commonly reported alteration type , followed by amplications , indels , and fusions . the results reected the genomic landscape reported across tumor types through solid tumor testing19 , 20 and is shown in figure 2a . 
amplication levels detected ranged from positive , strongly positive , to very strongly positive , as previously dened.9 - 14 genes most frequently reported with very strong positive amplication levels were ccne1 , fgfr1 , met , erbb2 , and ar . 
 s anchez et al patients ( n = 575 ) no alterations reported ( n = 137 ) any alteration reported ( n = 438 ) only alterations in nonactionable genes ( n = 81 ) one or more alterations within actionable genes ( n = 357 ) fig 1 . 
a total of 575 patients was enrolled , of whom 76.2% ( n = 438 ) had at least one alteration reported . of these 438 , 81.5% ( n = 357 ) had at least one alteration reported within an actionable gene , of whom in turn , 54.7% ( n = 205 ) had at least one high potential for clinical action alteration . 
again , these results highlight the importance of assessing each alterations biologic fs individually and in the disease context ( fig 2c )  . the actual variant actionability , or potential for clinical action , was used to stratify patients by disease type into three categories : hpca , low potential for clinical action , and not recommended for clinical action . 
among diseases with 10 or more patients enrolled , the proportion of patients who had at least one hpca alteration was as follows : breast , 67.6% ; colorectal , 60% ; lung , 56.5% ; gall bladder , 56.3% ; ovarian , 50% ; head and neck , 43.5% ; cholangiocarcinoma , 43.3% ; prostate , 40% ; hepatocellular , 25.4% ; pancreatic , 19.5% ; neuroendocrine , 15.4% ; sarcoma , 14.9% ; and appendiceal , 10.6% ( fig 4a )  . overall , these ndings demonstrate that cfdna testing is informative across all tumor types included in this study . specically , among tumor types with greater representation ( 10 patients enrolled ) , 50% or more patients had at least one hpca alteration . 
 a genomic alterations in cell - free dna amplification fusion frameshift / truncation indel very strong positive ( + + + ) strong positive ( + + ) positive ( + ) fig 2 . 
 ( b ) identication of clinical trials across all disease types in the context of variants potential for clinical action . alterations ( 143 patients ) , the concordance rate was 44% ( 56 of 127 alterations )  . 
these alterations potentially represent genomic evolution and mechanisms of acquired resistance and included detection of a pik3ca mutation after treatment with a braf inhibitor and braf and met mutations after treatment with akt / mtor inhibitors . on the other hand , among 391 patients with no previous solid tumor testing attempted , 529 alterations in actionable genes were reported on cfdna testing . 
in addition , of 14 patients who had previous solid tumor testing attempted but the tumor genomic assays failed ( eg , because of an insufcient amount of dna obtained from the sample ) , cfdna testing reported 17 alterations in actionable genes , with 10 patients having any alteration detected , seven having at least one alteration in an actionable gene , and two having at least one specic alteration that was actionable at the time of annotation . identication of clinical trials for variants identied through cfdna the utility of cfdna testing depends on the ability to match patients to relevant targeted therapy delivered through clinical trials , standard of care , or off - label use . 
in addition to variant annotation , for patients with hpca variants and / or select low potential for clinical action variants ( ie , fs , unknown ; avc , potentially ; actionable for call , therapeutic intervention ) , the decision support team identied genotype - matched trials for the patients tumor type , which accounted for additional biomarker inclusion / exclusion criteria , where applicable . 
among patients who had at least one hpca alteration , identication of trials was even higher , with potential trials identied for 188 ( 92% ) of 205 patients ( fig 3b )  . clinical course of action after cfdna testing of the 205 patients with at least one hpca variant , 118 had reached the 6 - month follow - up period at the time of data freeze ( march 6 , 2018 )  . 
at this time , 11% of patients ( 13 of 118 ) had been treated with genotype - matched targeted therapy on the basis of cfdna testing , where a match included enrollment into a clinical trial ( n = 9 ) , off - label drug use ( n = 3 ) , or standard of care ( n = 1 )  . 
on the basis of at least 6 months of follow - up , a major contributor to not acting on a genomic alteration was the ps of patients at the time of trial consideration . 
reports from the university of california , los angeles , also found that biopsy samples required for trial eligibility led to delays and decline in ps , which resulted in reduced enrollment by approximately one half.22 similarly , a review of 55 nonsmall - cell lung cancer trials at princess margaret hospital reported a significant reduction in enrollment because of declining ps or insufcient tissue biopsy sample material when required.23 in addition , we evaluated a novel and important factorinitiation of alternative therapy when ordering cfdna testingthat may have reduced the number of trial - eligible patients because of a decline of ps during next - line therapy . 
of note , cfdna testing has a short enough turnaround time to facilitate selection of next - line therapy ( a median of 7 calendar days now is achieved at the high - volume laboratory used herein ) .3 , 24 thus , its use at the point of care may increase its clinical utility before a decline in ps . 
testing earlier , when ps is better , also is likely to optimize patient outcomes from investigational therapies . reports on cfdna testing there have been several utility.3 , 25 - 27 laufer - geva et al28 reported that treatment decisions were changed in 23% to 32% of patients with nonsmall - cell lung cancer dependent on the clinical scenario . 
of note , we accrued very few patients with lung cancer and accrued predominantly tumor types without standard - of - care , genomically informed treatment options . this may have affected overall actionability rates as well as the number of patients who received genomically matched therapy . previous studies have reported higher concordance rates for cfdna results and tumor testing.24 , 29 leighl et al30 reported that in untreated nonsquamous cell carcinoma , food and drug administrationapproved target ( egfr , alk , ros1 , braf ) concordance was greater than 98.2% , with a 100% positive predictive value for cfdna versus tissue ( 34 of 34 patients with egfr - , alk - , or brafpositive mutations )  . 
our study was not designed to compare cfdna and tissue testing ; thus , it had inherent limitations to investigate this issue , including intervening time between sample collections , intervening treatments and resulting tumor evolution , tumor heterogeneity of solid tumor testing versus global representation of primary and metastatic sites from cfdna , and tumor type dependence on the extent of cfdna shedding . 
however , cfdna testing reported potentially clinically relevant alterations that otherwise may have been missed because solid tumor testing was not attempted or not technically feasible because of lack of tissue or did not have sufcient coverage . our study has other limitations . 
although there may have been greater use of cfdna results for treatment selection if patients were prospectively tested and treatment initiated after results , we believe that our study design gives insight into clinical practice patterns . second , we enrolled patients with a variety of tumor types . this design allowed us to determine that the detection of cfdna and the detection of actionable alterations vary by tumor type . 
third , actionability was assessed at the time of testing by a designated decision support team , but trial matching was performed automatically on the basis of gene - drug associations . where there were trial matches , additional clinical exclusion criteria possibly made patients ineligible for selected trials . 
cfdna also can identify actionable resistance mutations , and including those would have potentially enhanced clinical utility.3 in summary , we demonstrated that cfdna testing detects actionable alterations in patients with advanced cancers across a variety of tumor types . 
lanman employment : guardant health , veracyte leadership : guardant health , biolase stock and other ownership interests : guardant health , biolase , forward medical consulting or advisory role : forward medical research funding : guardant health kenna r . 
 s anchez et al references lebofsky r , decraene c , bernard v , et al : circulating tumor dna as a non - invasive substitute to metastasis biopsy for tumor genotyping and personalized medicine in a prospective trial across all tumor types . 
normanno n , cervantes a , ciardiello f , et al : the liquid biopsy in the management of colorectal cancer patients : current applications and future scenarios . cancer treat rev 70 : 1 - 8 , 2018 zill oa , banks kc , fairclough sr , et al : the landscape of actionable genomic alterations in cell - free circulating tumor dna from 21 , 807 advanced cancer patients . 
clin cancer res 24 : 3528 - 3538 , 2018 polivka j jr , pesta m , janku f : testing for oncogenic molecular aberrations in cell - free dna - based liquid biopsies in the clinic : are we there yet ? expert rev mol diagn 15 : 1631 - 1644 , 2015 diaz la jr , bardelli a : liquid biopsies : genotyping circulating tumor dna . 
biochim biophys acta 1775 : 181 - 232 , 2007 suraj s , dhar c , srivastava s : circulating nucleic acids : an analysis of their occurrence in malignancies . 
biomed rep 6 : 8 - 14 , 2017 janku f , zhang s , waters j , et al : development and validation of an ultradeep next - generation sequencing assay for testing of plasma cell - free dna from patients with advanced cancer . 
clin cancer res 23 : 5648 - 5656 , 2017 zill oa , greene c , sebisanovic d , et al : cell - free dna next - generation sequencing in pancreatobiliary carcinomas . 
kim st , lee ws , lanman rb , et al : prospective blinded study of somatic mutation detection in cell - free dna utilizing a targeted 54 - gene next generation sequencing panel in metastatic solid tumor patients . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
spiegel ml , goldman jw , wolf br , et al : non - small cell lung cancer clinical trials requiring biopsies with biomarker - specic results for enrollment provide unique challenges . 
schwaederle mc , patel sp , husain h , et al : utility of genomic assessment of blood - derived circulating tumor dna ( ctdna ) in patients with advanced lung methodologies . 
clin cancer res 23 : 5101 - 5111 , 2017 janku f , angenendt p , tsimberidou am , et al : actionable mutations in plasma cell - free dna in patients with advanced cancers referred for experimental targeted therapies . 
laufer - geva s , rozenblum ab , twito t , et al : the clinical impact of comprehensive genomic testing of circulating cell - free dna in advanced lung cancer . j thorac oncol 13 : 1705 - 1716 , 2018 29 . 
kato s , schwaederle mc , fanta pt , et al : genomic assessment of blood - derived circulating tumor dna in patients with colorectal cancers : correlation with tissue sequencing , therapeutic response , and survival . 
leighl nb , page rd , raymond vm , et al : clinical utility of comprehensive cell - free dna analysis to identify genomic biomarkers in patients with newly diagnosed metastatic non - small cell lung cancer . 
 outcomes by egfr , kras , and alk genotype after combined modality therapy for locally advanced nonsmall - cell lung cancer purpose in 699 patients with locally advanced nonsmall - cell lung cancer ( nsclc ) treated with radiation therapy as part of combined modality therapy , we compared outcomes among genotyped and ungenotyped patients and by tumor genotype status ( egfr , kras , and alk )  . patients and methods genotyping was performed in 250 patients : egfr + ( 19% ) , kras + ( 32% ) , alk + ( 9% ) , and wild type ( wt / / ; 40% )  . 
there was higher freedom from locoregional recurrence ( lrr ) for egfr + tumors and lower freedom from lrr in alk + tumors , compared with kras + and wt / / tumors ( 3 - year : 77% v 38% v 49% v 46% )  . 
 analysis of post - recurrence survival demonstrated that egfr + / alk + patients treated with appropriate tyrosine kinase inhibitors had higher os compared with other groups . conclusion in this series of locally advanced nsclc treated with combined modality therapy , egfr + and alk + were associated with higher os , whereas lrr was lower in egfr + patients , and the risk of distant metastases was high in all subgroups . 
2018 by american society of clinical oncology introduction advances in cancer genomics in the past decade have identified genetically distinct subgroups of lung adenocarcinoma defined by activating genomic alterations in oncogenes such as kras , egfr , and alk.1 - 5 the unique biology of each subgroup has led to the development of genotype - directed therapy in stage iv disease , with level 1 evidence that targeted therapies for egfr - mutant , 6 - 8 and alk - rearranged stage iv nonsmall - cell lung cancer ( nsclc ) 9 improve outcomes when compared with chemotherapy . 
although the 10 - year anniversary of the discovery of egfr mutations in 2014 marked a new era of targeted therapy and precision medicine for genotypic subgroups of stage iv lung adenocarcinoma , the clinical potential of integration of targeted therapies with conventional modalities of curative therapy ( eg , surgery , radiation , and / or chemotherapy ) for earlier - stage disease has not been fully realized . first , the impact of tumor genotype on the natural history and responsiveness to conventional treatment of earlier stages of disease remains understudied and controversial . 
second , although radiation therapy ( rt ) plays a critical role in combined modality therapy ( cmt ) for locally advanced nsclc ( la - nsclc ) , radiation responsiveness and clinical outcomes after thoracic rt for the genotypic subgroups of nsclc are not well elucidated . 
direct sanger sequencing and / or polymerase chain reaction with capillary gel electrophoresis using primers specific for codons 18 to 21 for egfr and codons 12 , 13 , and 61 of the kras gene27 was performed ( data supplement )  . 
alk testing was performed using immunohistochemistry ( n = 13 ) , fluorescent in situ hybridization ( n = 129 ) , or both ( n = 7 )  . because the indications and scope of genotyping changed during the follow - up period ( eg , the development of alk assays in the later period ) , some patients did not have complete genotyping data for all three oncogenes . 
tumors that had genotyping data for all three oncogenes were classified as egfr + , alk + , kras + , or triple wild type ( wt / / ) and were included in a fourway analysis . 
tumors with partial genotyping results were classified as unknown for four - way analyses but were analyzed in comparisons of wt versus mutant for individual oncogenes . covariates patient age , sex , ethnicity , eastern cooperative oncology group performance status , smoking history ( 1 [ never smokers ] : < 100 cigarettes in lifetime ; 2 [ former smokers ] : quit smoking > 1 year before diagnosis ; 3 [ current smokers ] : smoking at time of diagnosis or quit < 1 year before ) , and tumor characteristics ( size , histology , 7th edition american joint committee on cancer stage , and number of nodal stations involved per the international association for the study of lung cancer atlas ) 28 were analyzed . 
 treatment and follow - up the cmt for each patient was selected with a multidisciplinary approach , typically trimodality therapy for stage iiia and concurrent chemoradiation for medically inoperable ii to iiia or n3 disease . 
all patients were treated with rt per institutional norms , with three - dimensional or four - dimensional computed tomography ( ct ) simulation and either 3dcrt or imrt planning . 
the rt target included primary and nodal disease as defined by positron emission tomography ( pet ) - ct , microscopic margin ( 0 to 7 mm ) , and setup margin ( 5 to 10 mm , depending on localization technology at the time ) , and elective nodal irradiation was not performed . patients were observed with chest ct every 3 to 4 months after treatment ( years 1 and 2 ) , then every 6 months ( years 3 to 5 ) , and annually thereafter . outcomes overall survival ( os ) and patterns of failure , including lrr , distant metastases ( dm ) , any recurrence , and progression - free survival ( pfs ; survival with absence of recurrence ) , were calculated from the date of initiation of treatment to the time of first failure . 
out - offield lrr was defined as occurring outside of the planning target volume . statistical analyses all survival and recurrence outcomes were analyzed using the kaplan - meier method and log - rank test . 
because risk of failures may be altered by salvage systemic treatment during the follow - up period , a cox proportional hazards regression model with systemic treatment as a time - dependent covariate was used to analyze patterns of failures . 
to analyze the impact on os of salvage targeted therapies at the time of recurrence , a postrecurrence landmark analysis of os was performed with cutoffs of 3 , 6 , and 9 months after recurrence . 
all the analyses were performed using sas version 9.3 ( carey , nc )  . results tumor genotyping data and genotyped cohort characteristics genotyping was performed as part of routine clinical care in 250 patients , either before rt ( 50% ) or after rt ( 50% )  . 
the majority of patients received definitive chemoradiation , but 35% of patients also underwent surgery as part of cmt . outcomes and patterns of recurrence : all patients with a median follow - up of 57.4 months among all patients ( n = 699 ) , the median os was 26.9 months ( 3 - year estimate : 41% ) and the median pfs was 11.9 months ( 3 - year estimate : 25% )  . 
patient , tumor , and treatment characteristics by genotypic subgroup * ( continued ) characteristic alk + egfr + kras + total 50.4 - 66 45 - 66.6 45 - 66 6 - 68 6 - 68 rt dose per fraction no . 
 ( % ) unless indicated otherwise . abbreviations : 3dcrt , three dimensionalconformal radiation therapy ; adenoca , adenocarcinoma ; fev1 , forced expiratory volume in 1 second ; imrt , intensity modulated radiation therapy ; nsclc , nonsmall - cell lung cancer ; pretx , pre - treatment ; rt , radiation therapy ; scc , squamous cell carcinoma ; suv , standard uptake value ; wt , wild type for egfr , alk , and kras . * among patients with full genotyping available . the 3 - year estimates of freedom from lrr , dm , and any recurrence were 53% , 41% , and 32% , respectively ( data supplement )  . outcomes and patterns of recurrence : egfr + versus alk + versus kras + versus wt / / the median follow - up among genotyped patients was 48.2 months ; outcomes by genotype are listed in table 2 . 
the median os was 55.8 months for egfr + and was not reached for alk + patients , versus 28.0 months for kras + and 33.2 months for wt / / patients ( p = .02 ; fig 1a )  . 
 there was no significant difference in dm and any recurrence ( table 2 )  . univariable and multivariable analysis univariable analysis showed that younger age , female sex , nodal stations involved , surgery , rt dose , and alk + were associated with increased os , and genotypic subgroup ( egfr + v alk + v kras + v wt / / ) was also associated ( data supplement )  . 
pfs and any recurrence were not associated with tumor genotype ( data supplement )  . analysis of post - recurrence outcomes we analyzed post - recurrence os among genotyped patients to assess the impact of salvage tki on the increased os observed in alk + / egfr +  . 
of those who recurred , 88% of egfr + patients ( 21 of 24 ) and 75% of alk + patients ( nine of 12 ) received tki after recurrence ( three egfr + and two alk + patients died as a result of disease progression before tki , and one alk + patient had a complete response to salvage chemotherapy )  . 
among patients with pre - recurrence genotyping , there was a significant difference in post - recurrence os when comparing egfr + / alk + patients who received appropriate tki with those who did not receive tki and with other genotypic subgroups ( table 5 ; data supplement ) , with similar findings on landmark analyses . those without tumor genotyping ( n = 449 )  . 
the median follow - up was 48.2 months in genotyped patients versus 67.4 months in ungenotyped patients , reflecting more recent adoption of clinical genotyping ( data supplement )  . 
first , in univariable analysis , we demonstrate increased os in patients with alk + and egfr + tumors compared with patients with kras + and wt / / tumors . 
our findings of lower lrr in egfr + tumors may suggest increased radiation sensitivity , supporting the findings of previous in vitro studies.30 , 31 however , the existing literature has been mixed ; some series of chemoradiation for la - nsclc20 , 21 and cns metastases treated with whole - brain rt32 have shown increased rt sensitivity in egfr + tumors , whereas other series have not demonstrated a difference in radiation response.22 , 23 moreover , the numbers of patients in these subgroups were small , and these hypothesis generating results must be interpreted with caution and validated in larger data sets . another key finding of this study is that the incidence of dm was high among all patients , including egfr + and alk + ( 3 - year estimates : 58% and 51% , respectively ) , despite treatment with platinum - based doublet chemotherapy in most patients . 
in addition , using a landmark analysis , we demonstrated that post - recurrence os was higher in patients receiving appropriate genotype - directed tki , reaffirming the efficacy of these therapies and the importance of clinical genotyping.29 these two findings together underscore the importance of continuing to test the optimal integration of tki with curative cmt to reduce dm and improve cure rates . 
in comparison , post hoc analyses of the radiant ( clinicaltrials.gov identifier : nct00373425 ) and br.19 trials of adjuvant tki after cmt in unselected patients have not shown pfs or os benefit in egfr + patients ; however , these trials are limited by inadequate power and possible biases.25 , 26 the effects of indication bias ( eg , genotyping at the time recurrence ) , appropriate wt control groups , and the impact of salvage tki in prolonging os are illustrated in our studys unique analysis of outcomes by genotyped versus ungenotyped status . 
 survival , given the uncertainties in therapeutic interactions and cross - resistance . the strengths of this study include ( 1 ) an analysis of outcomes in one of the largest cohorts of la - nsclc with genotype data available on the three most common genotypic subgroups reported to date , ( 2 ) multiple control groups including wt / / and ungenotyped patients to ascertain the effects of testing bias , ( 3 ) contemporary cmt with modern rt techniques representative of current standards of care , and ( 4 ) sufficiently long follow - up ( median follow - up in genotyped patients : 48 months ) to provide a full natural history of the genotypic subgroups after cmt . 
furthermore , this study was conducted in an era when clinical genotyping involved only a limited gene panel ( kras / egfr / alk ) , and thus , commutations in genes such as those critical in the biology of kras + tumors such as lkb1 / p53 could not be analyzed.35 the heterogeneity of kras + nsclc may account in part for our findings of no difference in outcomes by kras status , as opposed to the findings of a previous chemoradiation series showing worse outcomes with kras + .36 similarly , less common genotypic subgroups of nsclc with targetable mutations ( eg , ros1 rearrangements ) could not be analyzed in this cohort . 
larger studies analyzing tumor responsiveness to rt across a more comprehensive set of targetable genes are needed . the findings from this study will have implications for designing future prospective trials incorporating conventional cmt with targeted therapies for genotypic subgroups of la - nsclc . 
using the higher observed median pfs ( egfr + , 15.3 months and alk + , 13.7 months ) from our study for the control group , the revised sample size estimate would be 412 egfr + and 132 alk + patients ( data supplement )  . 
although the pfs point estimates from our study may not be entirely generalizable because of the sample size and the potential biases as outlined , this exercise illustrates the importance of obtaining accurate estimates of pfs for genotypic subgroups for trial design . these challenges underscore the need for cooperation among multiple centers to comprehensively genotype patients with la - nsclc who are undergoing conventional cmt to further understand the natural history and biology of genotypic subtypes of nsclc , and for the development of novel trial designs to integrate targeted therapies with conventional cmt . 
novel trial designs implemented in the metastatic setting , including basket trials such as nci - match ( clinicaltrials.gov identifier : nct02465060 ) , nci - mpact ( clinicaltrials.gov identifier : nct01827384 ) , and custom ( clinicaltrials.gov identifier : nct01306045 ) , 37 have some appeal but may be complicated by uncertainties regarding interactions between targeted therapies and existing curative modalities . 
thus , obtaining a more detailed understanding of clinical outcomes of rare genotypic subgroups treated with conventional therapy off - trial will be critical to inform the optimal combination therapy , in conjunction with preclinical testing of different combinations of targeted and conventional therapies in genetically engineered mouse models in co - clinical trials as described previously.38 , 39 in this series comparing outcomes in patients with egfr + , alk + , and kras + la - nsclc who were treated with rt as part of curative cmt , we observed differences in os ( increased in alk + ) and lrr ( decreased in egfr + )  . 
the risk of dm and progression were high in all subgroups , and post - recurrence os was higher among egfr + / alk + patients receiving appropriate targeted therapies , underscoring the need for additional integration of genotype - directed therapies with curative cmt and routine genotyping for la - nsclc . 
aerts leadership : sphera stock and other ownership interests : sphera consulting or advisory role : sphera , genospace research funding : varian medical systems travel , accommodations , expenses : genospace elizabeth h . 
swanson honoraria : ethicon , covidien / medtronic consulting or advisory role : armada health care research funding : ethicon ( inst ) yu - hui chen employment : constellation pharmaceuticals ( i ) paul catalano consulting or advisory role : eli lilly bruce e . 
johnson stock and other ownership interests : kew honoraria : chugai pharma consulting or advisory role : novartis , kew , merck , eli lilly , chugai pharmaceutical , boehringer ingelheim , amgen , astrazeneca research funding : novartis ( inst ) , glaxosmithkline ( inst ) , genentech / roche ( inst ) , genentech / roche ( inst ) , toshiba ( inst ) patents , royalties , other intellectual property : danafarber cancer institute pasi a . 
jnne stock and other ownership interests : gatekeeper pharmaceuticals consulting or advisory role : pfizer , boehringer ingelheim , astrazeneca , merrimack , ariad pharmaceuticals , chugai pharmaceutical , roche / genentech , loxo , mirati therapeutics , araxes pharmaceuticals , ignyta , eli lilly research funding : astrazeneca , astellas pharma , daiichi sankyo , eli lilly , boehringer ingelheim , puma biotechnology patents , royalties , other intellectual property : i am a co - inventor on a dana - farber cancer instituteowned patent on egfr mutations licensed to laboratory corp . 
 supported in part by a radiological society of north america ( rsna ) seed grant , department of radiation oncology joint center for radiation therapy ( jcrt ) , and clinical - translational and kaye grants . presented at the american society of radiation oncology annual conference , september 25 - 28 , 2016 , boston , ma . support prior presentation references 1 . 
pao w , miller v , zakowski m , et al : egf receptor gene mutations are common in lung cancers from never smokers and are associated with sensitivity of tumors to gefitinib and erlotinib . 
lynch tj , bell dw , sordella r , et al : activating mutations in the epidermal growth factor receptor underlying responsiveness of non - small - cell lung cancer to gefitinib . 
mitsudomi t , morita s , yatabe y , et al : gefitinib versus cisplatin plus docetaxel in patients with non - small - cell lung cancer harbouring mutations of the epidermal growth factor receptor ( wjtog3405 ) : an open label , randomised phase 3 trial . 
loriot y , mordant p , deutsch e , et al : are ras mutations predictive markers of resistance to standard chemotherapy ? nat rev clin oncol 6 : 528 - 534 , 2009 11 . 
cuffe s , bourredjem a , graziano s , et al : a pooled exploratory analysis of the effect of tumor size and kras mutations on survival benefit from adjuvant platinum - based chemotherapy in nodenegative non - small cell lung cancer . 
chaft je , rusch v , ginsberg ms , et al : phase ii trial of neoadjuvant bevacizumab plus chemotherapy and adjuvant bevacizumab in patients with resectable nonsquamous non - smallcell lung cancers . 
shepherd fa , domerg c , hainaut p , et al : pooled analysis of the prognostic and predictive effects of kras mutation status and kras mutation subtype in early - stage resected non - smallcell lung cancer in four trials of adjuvant chemotherapy . 
schiller jh , adak s , feins rh , et al : lack of prognostic significance of p53 and k - ras mutations in primary resected non - small - cell lung cancer on e4592 : a laboratory ancillary study on an eastern cooperative oncology group prospective randomized trial of postoperative adjuvant therapy . 
tsao ms , sakurada a , ding k , et al : prognostic and predictive value of epidermal growth factor receptor tyrosine kinase domain mutation status and gene copy number for adjuvant chemotherapy in non - small cell lung cancer . 
sun hb , ou w , li y , et al : epidermal growth factor receptor mutation status and adjuvant chemotherapy in resected advanced non - small - cell lung cancer . 
yagishita s , horinouchi h , katsui taniyama t , et al : epidermal growth factor receptor mutation is associated with longer local control after definitive chemoradiotherapy in patients with stage iii nonsquamous non - small - cell lung cancer . 
ahn hk , choi yl , han jh , et al : epidermal growth factor receptor mutation and treatment outcome of mediastinoscopic n2 positive non - small cell lung cancer patients treated with neoadjuvant chemoradiotherapy followed by surgery . 
akamatsu h , kaira k , murakami h , et al : the impact of clinical outcomes according to egfr mutation status in patients with locally advanced lung adenocarcinoma who received concurrent chemoradiotherapy . 
mak rh , doran e , muzikansky a , et al : kras mutation is associated with decreased overall survival after thoracic radiation therapy in patients with locally advanced non - small cell lung cancer . 
kelly k , altorki nk , eberhardt we , et al : adjuvant erlotinib versus placebo in patients with stage ib - iiia non - small - cell lung cancer ( radiant ) : a randomized , double - blind , phase iii trial . 
eberhard da , johnson be , amler lc , et al : mutations in the epidermal growth factor receptor and in kras are predictive and prognostic indicators in patients with non - small - cell lung cancer treated with chemotherapy alone and in combination with erlotinib . 
rusch vw , asamura h , watanabe h , et al : the iaslc lung cancer staging project : a proposal for a new international lymph node map in the forthcoming seventh edition of the tnm classification for lung cancer . 
das ak , chen bp , story md , et al : somatic mutations in the tyrosine kinase domain of epidermal growth factor receptor ( egfr ) abrogate egfr - mediated radioprotection in non - small cell lung carcinoma . 
das ak , sato m , story md , et al : non - small - cell lung cancers with kinase domain mutations in the epidermal growth factor receptor are sensitive to ionizing radiation . 
gow ch , chien cr , chang yl , et al : radiotherapy in lung adenocarcinoma with brain metastases : effects of activating epidermal growth factor receptor mutations on clinical response . 
neal jw , pennell na , govindan r , et al : the select study : a multicenter phase ii trial of adjuvant erlotinib in resected epidermal growth factor receptor ( egfr ) mutation - positive nonsmall cell lung cancer ( nsclc )  . 
li n , ou w , ye x , et al : pemetrexed - carboplatin adjuvant chemotherapy with or without gefitinib in resected stage iiia - n2 non - small cell lung cancer harbouring egfr mutations : a randomized , phase ii study . 
yagishita s , horinouchi h , sunami ks , et al : impact of kras mutation on response and outcome of patients with stageiii non - squamous non - small cell lung cancer . 
lopez - chavez a , thomas a , rajan a , et al : molecular profiling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
chen z , akbay e , mikse o , et al : co - clinical trials demonstrate superiority of crizotinib to chemotherapy in alk - rearranged non - small cell lung cancer and predict strategies to overcome resistance . 
 programmed death - ligand 1 expression in a large cohort of pediatric patients with solid tumor and association with clinicopathologic features in neuroblastoma purpose programmed death - ligand 1 ( pd - l1 ) expression represents a potential predictive biomarker of immune checkpoint blockade response . 
however , literature about the prevalence of pd - l1 expression in the pediatric cancer setting is discordant . methods pd - l1 expression was analyzed using immunohistochemistry in 500 pediatric tumors ( including neuroblastoma , sarcomas , and brain cancers )  . 
positive cases were further characterized , with cases with weak intensity pd - l1 staining reported as having low pd - l1 expression and cases with a moderate or strong intensity of staining considered to have high pd - l1 expression . results pd - l1positive staining was identified in 13% of cases , whereas high pd - l1 expression was found in 3% of cases . 
2017 by american society of clinical oncology introduction in recent years , the ability of tumor cells to exert an immunosuppressive action in their local microenvironment has been well described.1 escaping the host immune system occurs via multiple strategies , including loss of tumor antigens or reduced expression of major histocompatibility complex molecules , as well as via recruitment of immunosuppressive inflammatory cells or inadequate costimulation of t cells.2 as a consequence , the ability to evade host immunity has been recognized as one of the hallmarks of cancer.3 the expression of immune inhibitory ligands such as programmed death - ligand 1 ( pd - l1 ) is another strategy used by cancer cells to inhibit the immunologic response.4 pd - l1 is a trans - membrane surface glycoprotein overexpressed in many solid tumors , including carcinomas5 - 8 and melanoma.9 moreover , pd - l1 is one of the two known ligands for programmed death ( pd ) - 1 , a receptor expressed by immune system cells ( including activated t cells , regulatory t cells , b cells , natural killer cells , activated monocytes , and dendritic cells ) that negatively regulates their proliferation federica saletta ricardo e . 
antibody - mediated blockade of pd - l1 induced objective response rates in 6% to 17% and prolonged disease stabilization in 12% to 41% of patients with advanced cancers , including nonsmall - cell lung cancer , melanoma , and renal cell cancer.16 similarly , cumulative response rates for pd - 1 mab immunotherapy were achieved in 18% of patients with nonsmall - cell lung cancer , 28% of patients with melanoma , and 27% of patients with renal - cell cancer.13 despite these promising results achieved in adult cancers , the prevalence of pd - l1 expression in the pediatric setting and the potential use of mabs directed against pd - 1 have only started to be explored . 
the 53 analyzed cases included 18 neuroblastomas , eight extracranial germ - cell tumors , seven germinomas , seven hepatoblastomas , four medulloblatomas , four renal tumors , three rhabdomyosarcomas , and two atypical teratoid / rhabdoid tumors . 
in contrast , chowdhury et al20 observed 66 of 115 pd - l1positive samples ( 57% , ranging from 47% to 86% , depending on tumor type ) in a multitumor study including neuroblastoma , rhabdomyosarcoma , ewing sarcoma , and osteosarcoma . 
alveolar rhabdomyosarcoma showed the highest prevalence of pd - l1positive cases ( 12 of 14 [ 86% ] ) and patients with high - risk neuroblastoma were commonly pd - l1 positive ( 31 of 43 [ 72% ] )  . no previous study has reported associations between pd - l1 staining and the features of pediatric patients with cancer . 
here we present the clinicopathologic features of and survival analysis associated with pd - l1 expression in patients with neuroblastoma , with particular focus on the potential relationship between pd - l1 expression and the risk of cancer relapse . 
we identified a subcohort of patients with pd - l1positive staining and poor outcome , suggesting that pd - l1 may be a negative prognostic factor associated with an elevated risk of cancer recurrence . methods patient cohort the retrospective pediatric cohort consisted of 500 patients who underwent diagnostic biopsy or surgical resection at the childrens hospital at westmead , new south wales , australia . 
formalin - fixed paraffin - embedded hematoxylin and eosinstained tumor samples were reviewed by a histopathologist , and approved samples were used to construct tissue microarrays ( tmas ) using a manual tissue arrayer ( beecher mta1 , diagnostic technology , belrose , new south wales , australia ) and a 1 - mm unitma premade recipient block ( ub06 - 1 , diagnostic technology , belrose , new south wales , australia )  . 
 immunohistochemistry each tma was sectioned at 4 mm , and immunohistochemistry was performed using a bondrx automatic stainer ( leica biosystems , macquarie park , new south wales , australia )  . 
slide deparaffinization was performed with bond dewax solution , followed by alcohol dehydration . epitope retrieval was performed using hier2 buffer ( bond , ar9540 ) , and slides were incubated for 60 minutes at room temperature using a rabbit monoclonal antipd - l1 primary antibody ( e1l3n , no.13684 , cell signaling technology , genesearch , arundel , queensland , australia ) at 1 : 500 dilution in primary antibody diluent ( bond , ar9352 )  . 
staining was visualized using a polymer refine detection kit ( bond , ds9800 ) , and nuclei were counterstained with hematoxylin . tumors with > 1% of cells showing pd - l1 membrane staining ( or a combination of membrane and cytoplasmic staining ) of any intensity were considered pd - l1 positive . 
pd - l1 intensity was scored as weak , moderate , or strong by a histopathologist ( r.e.v. ) with specific expertise in pd - l1 staining assessment in patients with melanoma . 
similarly , fibrillary and stromal pd - l1 staining was also observed occasionally but was not scored positively because the significance of nonmembranous pd - l1 staining remains unclear . statistical analyses statistical analyses were undertaken using spss version 20.0 ( spss , chicago , il )  . 
bivariate relationships between pd - l1positive cases and patient features were analyzed with cross - tabulation , and significance was tested with fishers exact test . overall survival and relapse or progression - free survival were assessed using the kaplan - meier method , and significance was established using a log - rank ( mantel - cox ) test . 
statistical significance was set at p , .05 for two - sided tests . results prevalence of pd - l1positive pediatric patients with cancer as summarized in table 1 , in the overall cohort , 65 ( 13.0% ) of 500 cases were found to be pd - l1 positive . 
of these , 50 ( 76.9% ) of 65 showed weak pd - l1 intensity , whereas 15 ( 23.1% ) of 65 showed moderate to strong pd - l1 intensity . 
as such , in the overall cohort , only 15 ( 3.0% ) of 500 cases had moderate or strong pd - l1 positivity . neuroblastoma cases showed pd - l1 expression more commonly ( 48 of 254 [ 18.9% ] ) than did sarcomas or brain tumors . 
of the 48 positive cases , 40 ( 83.3% ) of 48 were weakly positive for pd - l1 , whereas eight ( 16.7% ) of 48 were moderately to strongly pd - l1 positive . 
overall , the distribution of weakly versus moderately or strongly positive pd - l1 staining in the neuroblastoma cohort was 15.7% ( 40 of 254 ) and 3.1% ( eight of 254 ) , respectively . 
in the brain tumor cohort , six ( 4.4% ) of 136 cases stained positively for pd - l1 , of which three ( 50.0% ) of six showed moderate to strong pd - l1 positivity . 
of the 96 sarcoma samples , seven ( 7.3% ) of 96 stained positively for pd - l1 , with only one of 96 cases ( an undifferentiated sarcoma ) being moderately positive . 
of the lymphoma cases , three ( 50% ) of six were pd - l1 positive ; two of these ( two of three [ 66.7% ] ) were moderately or strongly positive . 
one nasopharyngeal carcinoma showed moderate to strong pd - l1 staining . pd - l1 immunohistochemistry staining pattern observed although in this study only membranous pd - l1 staining was considered positive , together with the occasional combination of both membranous and cytoplasmic positive staining ( n = 5 ) , a range of other staining patterns was observed . 
an example of each pattern is presented in figure 1 ; they included membranous staining in the placenta as a positive control ( fig 1a ) , membranous tumor staining of weak , moderate , and strong intensity ( figs 1b , 1c , and 1d , respectively ) , as well as the combination of both membranous and cytoplasmic tumor pd - l1positive staining ( fig 1e )  . 
pd - l1 positive cytoplasmic ( fig 1f ) , fibrillary ( fig 1g ) , and schwannian stromal staining ( fig 1h ) were also observed , together with pd - l1positive macrophage ( fig 1i ) , but they were scored as negative . cytoplasmic pd - l1 staining was detected in 30 ( 11.8% ) of 254 neuroblastoma cases , ranging from weak ( n = 24 [ 80.0% ] ) to moderate or strong ( n = 6 [ 20.0% ] ) ; however , these cases were not considered pd - l1 positive . 
exclusive macrophage pd - l1 staining ( without pd - l1 positivity in tumor cells ) was detected in one ( 5.6% ) of 18 rhabdomyosarcomas , one ( 3.3% ) of 30 osteosarcomas , one ( 0.4% ) of 254 neuroblastomas , and one ( 2.6% ) of 38 lowgrade gliomas . 
the presence of macrophages was verified via hematoxylin and eosin staining observation . association with clinicopathologic features in pd - l1positive neuroblastoma cases information concerning a number of clinicopathologic features of the broader pediatric cohort was collated and tested ( using a two - sided fishers exact test ) for nonrandom associations with pd - l1 staining . 
interestingly , no differences in pd - l1 staining were found between biopsy specimens obtained before and after radiotherapy ( p = .702 ) , but a significant association between pd - l1 positivity and biopsy specimens obtained before chemotherapy was observed ( p = .044 ) , contrary to the suggestion of uehara et al.18 other clinicopathologic features that define patient prognosis in the neuroblastoma population at diagnosis include the mitosis - karyorrhexis index , shimada classification , mycn status , and overall patient risk ( table 2 )  . 
next , we sought to analyze whether pd - l1positive neuroblastoma cases were associated with cancer recurrence or progression ; however , no significant ( p = .939 ) association was observed ( fig 2b )  . 
although we did not find an association ( p = .508 ) between moderate to strong pd - l1 staining and overall survival ( fig 2c ) , the association with poorer relapse - free survival in this subcohort was significant ( p = .002 , fig 2d )  . 
programmed death - ligand 1 ( pd - l1 ) immunohistochemistry staining patterns . representative images of pd - l1 staining ( in brown ) and counterstained nuclei ( in blue )  . 
black arrows highlight examples of ( a ) pd - l1 staining in placenta used as positive control tissue ; pd - l1 membranous staining of ( b ) weak , ( c ) moderate , and ( d ) strong intensity in lymphoma ; and ( e ) pd - l1positive staining in both membrane and cytoplasm in neuroblastoma . 
 ( f ) exclusive cytoplasmic pdl1 staining and ( g ) pdl1positive schwannian stroma in neuroblastoma were considered negative . ( h ) pd - l1positive fibrillary staining in medulloblastoma and ( i ) pd - l1positive macrophages in osteosarcoma were also scored as negative . 
there were no differences in overall survival ( p = .298 ) or relapse - free survival ( p = .507 ) according to pd - l1 positivity of any intensity ( figs 3a and 3b )  . 
when restricting the analysis to the lowand intermediate - risk neuroblastoma cohort with moderate to strong pd - l1 staining , we found no association ( p = .524 ) with overall survival ( fig 3c ) but significantly ( p , .001 ) poorer relapse - free survival ( fig 3d )  . discussion since discovering that pd - 1 / pd - l1 binding promotes cancer tolerance by blocking the t - cell antigen receptor - induced stop signal , 22 substantial research effort has been aimed at targeting this interaction . 
a list of the pd - l1 antibodies and the staining and scoring methods used by other research groups is summarized in table 3 , which highlights the need for standardized immunohistochemistry methodology and a standardized scoring system for pd - l1positive cases . 
 ( a ) and ( b ) show overall survival and relapsefree survival ( in months ) in association with pd - l1 positivity ( of any intensity ) , respectively . 
 ( c ) and ( d ) show overall survival and relapse - free survival ( in months ) in association with moderate or strong pd - l1 staining intensity , respectively . 
for example , in a glioblastoma study , there was no association between fibrillary pd - l1 detection and overall survival in patients with glioblastoma.31 in our cohort , pd - l1 fibrillary staining was observed in only one of 38 medulloblastoma biopsy specimens , whereas pd - l1 schwannian stromal staining was detected in twelve of 254 patients with neuroblastoma . 
associations between programmed death - ligand 1 ( pd - l1 ) status and survival of patients with neuroblastoma ( nb ) with low and intermediate risk . kaplan - meier plots compare patient survival ( in months ) in the lowand intermediate - risk nb cohort . 
 ( a ) and ( b ) show overall survival and relapsefree survival ( in months ) in association with pd - l1 positivity ( of any intensity ) , respectively . 
 ( c ) and ( d ) show overall survival and relapse - free survival ( in months ) in association with moderate or strong pd - l1 staining intensity , respectively . 
previous reports have shown a discordant association between myc oncogene status and pd - l1 expression . in fact , casey et al36 stated that myc regulates the antitumor immune response through cd47 and pd - l1 in melanoma and nonsmall - cell lung cancer cell lines , whereas dondero et al37 showed that pd - l1 expression in neuroblastoma was interferon - gamma dependent and mycn independent . 
because strong pdl1 staining has been shown to correlate with an elevated mutation burden , 26 we can speculate that these cases may share an underlying dna repair deficit that results in an increased presence of neoantigens and particularly high pd - l1 expression . 
more studies are necessary to verify this hypothesis and to correlate mutation burden in children with stronger pd - l1 staining and a higher likelihood of cancer relapse despite favorable clinical features . pd - l1 may represent a novel predictive marker of cancer recurrence that could be used to identify the proportion of children who may benefit from pd - 1 / pd - l1 mab therapy . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . geoffrey mccowage research funding : novartis ( inst ) , merck ( inst ) acknowledgment we thank the patients and families who agreed to donate samples to the childrens hospital at westmead tumour bank . 
we also thank michael krivanek , md , of childrens hospital at westmead for his help with the histologic review of patient samples before tissue coring for tma construction , and jason madore of royal prince alfred hospital for his help in optimizing the immunohistochemistry protocol and staining interpretation . federica saletta no relationship to disclose ricardo e . 
blank c , gajewski tf , mackensen a : interaction of pd - l1 on tumor cells with pd - 1 on tumor - specific t cells as a mechanism of immune evasion : implications for tumor immunotherapy . 
karim r , jordanova es , piersma sj , et al : tumor - expressed b7 - h1 and b7 - dc in relation to pd - 1 + t - cell infiltration and survival of patients with cervical carcinoma . 
thompson rh , kuntz sm , leibovich bc , et al : tumor b7 - h1 is associated with poor prognosis in renal cell carcinoma patients with long - term follow - up . 
madore j , vilain re , menzies am , et al : pd - l1 expression in melanoma shows marked heterogeneity within and between patients : implications for anti - pd - 1 / pd - l1 clinical trials . 
freeman gj , long aj , iwai y , et al : engagement of the pd - 1 immunoinhibitory receptor by a novel b7 family member leads to negative regulation of lymphocyte activation . 
topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of anti - pd - 1 antibody in cancer . n engl j med 366 : 2443 - 2454 , 2012 14 . 
chowdhury f , dunn s , mitchell s , et al : pd - l1 and cd8 + pd1 + lymphocytes exist as targets in the pediatric tumor microenvironment for immunomodulatory therapy . 
fife bt , pauken ke , eagar tn , et al : interactions between pd - 1 and pd - l1 promote tolerance by blocking the tcr - induced stop signal . 
saletta f , wadham c , ziegler ds , et al : molecular profiling of childhood cancer : biomarkers and novel therapies . 703 - 718 , 2013 bba clin 1 : 59 - 77 , 2014 26 . 
madore j , strbenac d , vilain r , et al : pd - l1 negative status is associated with lower mutation burden , differential expression of immune - related genes , and worse survival in stage iii melanoma . 
mu cy , huang ja , chen y , et al : high expression of pd - l1 in lung cancer may contribute to poor prognosis and tumor cells immune escape through suppressing tumor infiltrating dendritic cells maturation . 
yang cy , lin mw , chang yl , et al : programmed cell death - ligand 1 expression in surgically resected stage i pulmonary adenocarcinoma and its correlation with driver mutations and clinical outcomes . 
preusser m , berghoff as , wick w , et al : clinical neuropathology mini - review 6 - 2015 : pd - l1 : emerging biomarker in glioblastoma ? clin neuropathol 34 : 313 - 321 , 2015 32 . 
taube jm , klein a , brahmer jr , et al : association of pd - 1 , pd - 1 ligands , and other features of the tumor immune microenvironment with response to anti - pd - 1 therapy . 
 c prolonged partial response to bevacizumab and valproic acid in a patient with glioblastoma introduction glioblastoma is the most common and malignant type of primary cns tumor.1 , 2 the estimated median overall survival ( os ) duration ranges from 14 months to 16 months , whereas the 5 - year os rate is estimated to be 5%.1 , 3 - 5 chemoradiation followed by adjuvant temozolomide remains the standard frontline therapy.3 bevacizumab has been used as a single agent or in combination with other agents at the time of diagnosis or at disease progression.6 - 11 in patients with newly diagnosed glioblastoma , the addition of bevacizumab to standard treatment regimens did not improve os , which has resulted in limited use.11 in recurrent glioblastoma , bevacizumab monotherapy was associated with higher rates of response ( 28% ) and 6 - month progression - free survival ( pfs ; 29% to 43% ) compared with historical data with radiotherapy and other regimens ( 4% to 9% and 9% to 21% , respectively ) .11 in recent years , immunotherapy has demonstrated promising results in selected patients , although long - term os data are unavailable.12 - 16 valproic acid is a histone deacetylase inhibitor ( hdi ) that has antitumor activity associated with antiangiogenic effects.17 in in vitro and in vivo animal models , hdis upregulated p53 and von hippel - lindau and downregulated hif - 1 and vascular endothelial growth factor ( vegf ) , which inhibits angiogenesis.17 hdis also inhibit vegf - stimulated endothelial cells and angiogenesis , and their antitumor activity increases in combination with a vegf receptor tyrosine kinase inhibitor.18 we have previously reported on the safety of bevacizumab and valproic acid in patients with advanced cancer.19 here , we present a patient with progressive glioblastoma in whom prolonged partial response ( pr ) was achieved with bevacizumab and valproic acid . 
magnetic resonance imaging ( mri ) of the brain revealed a 5.1 - cm mass in the left parietal lobe , peripheral enhancement with edema , and mass effect on the left lateral ventricle . 
in july 2011 , the patient underwent a partial tumor resection followed by intensity - modulated radiation therapy ( total dose , 59.4 gy in 33 fractions ; completed september 2011 ) with concurrent administration of temozolamide . 
mri of the brain in september 2011 demonstrated disease progression and temozolamide was discontinued . in november 2011 , the patient referred himself to our phase i program and was enrolled in a clinical trial of a poly ( adp - ribose ) polymerase inhibitor and temozolamide . 
after three cycles , treatment with the phosphatidylinositol - 3 kinase inhibitor was discontinued because of disease progression . in june 2012 , the patient returned to our clinic and was enrolled in a clinical trial of bevacizumab , temsirolimus , and valproic acid ( clinicaltrials . gov identifier : nct01552434 )  . 
bevacizumab 5 mg / kg was administered iv on days 1 and 15 , valproic acid 5 mg / kg orally once per day , and temsirolimus 20 mg iv once per week . 
he required interruption of bevacizumab after cycle 33 because he underwent transurethral prostate resection as a result of an abscess that was not responding to drainage or iv antibiotics and after cycles 44 and 55 because of transient grade 2 proteinuria . 
in june 2018 , molecular profiling was retrospectively performed on the patients tumor tissue obtained in july 2011 using a 595 - gene panel ( table 1 )  . discussion despite various treatment options , the prognosis of patients with advanced glioblastoma is poor.22 the efficacy of standard treatments is suboptimal and patients are encouraged to participate in clinical trials . 
his tumor had multiple alterations , including cyclin - dependent kinase 4 ( cdk4 ) amplification and fgfr3tacc3 chromosomal fusion . glioblastomas harbor several molecular alterations implicated in the activation of oncogenic pathways.23 - 25 amplification of cdk4located at chromosome 12is common in glioblastoma , 26 , 27 and its incidence was 13% in a comprehensive analysis.25 our patient was treated with valproic acid , which suppresses cdk4 , among other proteins , and induces growth inhibition , apoptosis , and senescence in medulloblastoma cell lines.28 valproic acid was demonstrated to inhibit the proliferation of mcf - 7 breast cancer cells via apoptosis and g1 phase arrest , possibly by downregulating cyclin d1 , 29 which , in turn , decreased cdk4 protein levels.30 other investigators demonstrated that valproic acid significantly reduced mrna expression of cyclin d1 and cdk4 in leukemic cells used in a murine xenograft tumor model , which leads to g0 / g1 arrest.31 cdk4 amplification was found in tumors with fgfr3tacc3 fusions and it was more frequent in isocitrate dehydrogenase wild - type gliomas that harbored fgfr3 - tacc3 fusions than in those without the fusion.32 the fgfr3 gene fuses with multiple partners , including the tacc3 gene , which encodes a protein that participates in the stabilization of the mitotic spindle . 
magnetic resonance images of the brain [ t1 - weighted imaging post gadolinium contrast ; axial plane ( a and b ) , coronal ( c ) ] at ( 1 ) baseline and ( 2 ) after first restaging after two cycles of treatment with bevacizumab and valproic acid . 
formalin - fixed , paraffin - embedded samples were sequenced to detect somatic single - nucleotide variants , insertion - deletions , copy number variants , gene rearrangements , and microsatellite instability . 
we also performed a tempus rna whole - transcriptome panel and used this for expanded detection of gene rearrangements , immune infiltration , and gene expression for immune and targeted therapy related genes . abbreviation : cdk4 , cyclin - dependent kinase 4 . regulates cell growth , differentiation , and tumor neoangiogenesis.38 - 40 our patient was also treated with bevacizumab , an anti - vegf agent . 
ostrom qt , gittleman h , liao p , et al : cbtrus statistical report : primary brain and other central nervous system tumors diagnosed in the united states in 2010 - 2014 . 
stupp r , hegi me , mason wp , et al : effects of radiotherapy with concomitant and adjuvant temozolomide versus radiotherapy alone on survival in glioblastoma in a randomised phase iii study : 5 - year analysis of the eortc - ncic trial . 
kreisl tn , kim l , moore k , et al : phase ii trial of single - agent bevacizumab followed by bevacizumab plus irinotecan at tumor progression in recurrent glioblastoma . 
taal w , oosterkamp hm , walenkamp am , et al : single - agent bevacizumab or lomustine versus a combination of bevacizumab plus lomustine in patients with recurrent glioblastoma ( belob trial ) : a randomised controlled phase 2 trial . 
omuro a , vlahovic g , lim m , et al : nivolumab with or without ipilimumab in patients with recurrent glioblastoma : results from exploratory phase i cohorts of checkmate 143 . 
van den bent m , french p , eoli m , et al : updated results of the intellance 2 / eortc trial 1410 randomized phase ii study on depatux - m alone , depatux - m in combination with temozolomide ( tmz ) and either tmz or lomustine ( lom ) in recurrent egfr amplified glioblastoma ( nct02343406 )  . 
qian dz , wang x , kachhap sk , et al : the histone deacetylase inhibitor nvp - laq824 inhibits angiogenesis and has a greater antitumor effect in combination with the vascular endothelial growth factor receptor tyrosine kinase inhibitor ptk787 / zk222584 . 
wheler jj , janku f , falchook gs , et al : phase i study of anti - vegf monoclonal antibody bevacizumab and histone deacetylase inhibitor valproic acid in patients with advanced cancers . 
verhaak rg , hoadley ka , purdom e , et al : integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
reifenberger g , reifenberger j , ichimura k , et al : amplification of multiple genes from chromosomal region 12q13 - 14 in human malignant gliomas : preliminary mapping of the amplicons shows preferential involvement of cdk4 , sas , and mdm2 . 
li xn , shu q , su jm , et al : valproic acid induces growth arrest , apoptosis , and senescence in medulloblastomas by increasing histone hyperacetylation and regulating expression of p21cip1 , cdk4 , and cmyc . 
ma xj , wang ys , gu wp , et al : the role and possible molecular mechanism of valproic acid in the growth of mcf - 7 breast cancer cells . 
yu b , lane me , pestell rg , et al : downregulation of cyclin d1 alters cdk 4and cdk 2 - specific phosphorylation of retinoblastoma protemol cell biol res commun 3 : 352 - 359 , 2000 31 . 
bao zs , chen hm , yang my , et al : rna - seq of 272 gliomas revealed a novel , recurrent ptprz1 - met fusion transcript in secondary glioblastomas . 
fons p , gueguen - dorbes g , herault jp , et al : tumor vasculature is regulated by fgf / fgfr signaling - mediated angiogenesis and bone marrow - derived cell recruitment : this mechanism is inhibited by ssr128129e , the first allosteric antagonist of fgfrs . 
giavazzi r , sennino b , coltrini d , et al : distinct role of fibroblast growth factor - 2 and vascular endothelial growth factor on tumor growth and angiogenesis . 
 homologous recombination deficiency in breast cancer : a clinical review brca1 and brca2 germline mutationassociated breast cancers are known to be deficient in the process of homologous recombination and often respond favorably to drugs targeting this important dna repair pathway . 
there is emerging evidence that a significant proportion of patients with brca1 / brca2 wild - type breast cancer are also deficient in homologous recombination , and it is hypothesized that these patients may derive similar benefit from drugs targeting this pathway . 
this review outlines the various approaches that researchers have taken to predict homologous recombination deficiency as part of correlative biomarker work in various studies and clinical trials in breast cancer . 
recent evidence demonstrates that parp is important for resolving stalled replication forks , and its inhibition during base excision repair requires brca - dependent hr to resolve.3 , 4 targeting dna damage response pathways has emerged as an attractive strategy to destabilize tumor genomic integrity and trigger genomic catastrophe and cell death in a tumor - specific fashion . the role of brca1 / brca2 in double - strand dna repair via hr has been well documented , 5 and there is mounting evidence that breast cancers arising in brca1 / brca2 germline mutation carriers respond favorably to therapies that target dna repair pathways , such as platinum salts and parp inhibitors ( parpis ) .6 - 8 hereditary brca1 / brca2 mutations account for up to 7% of all unselected breast cancers , 9 increasing to 11% to 15% of unselected individuals with triple - negative breast cancer ( tnbc : estrogen receptor [ er ] , progesterone receptor [ pr ] , human epidermal growth factor receptor 2 [ her2 ] negative ) and as high as 50% with a strong family history.10 - 12 brca1 mutations are most commonly associated with the tnbc clinical subtype , whereas brca2 mutations are more frequently associated with erpositive tumors . 
some sporadic ( ie , brca1 / brca2 wild - type [ wt ] ) breast cancers also harbor defects involving the hr pathway and respond similarly to platinum salts . 
 ( a ) somatic mutations , including substitutions and small insertions / deletions in key hr - related genes , such as brca1 and brca2 , can be associated with hrd . 
these include telomeric allelic imbalance ( tai ; large allelic imbalances extending into a telomere ) , large - scale transition ( lst ; number of transitions between large regions of differing allelic states ) , and loss of heterozygosity ( loh ; large regions displaying somatic loss of one haplotype , which can be copy variable as in deletion loh or copy neutral )  . current research has focused on the development of a companion diagnostic to identify sporadic brca - like tumors that would allow clinicians to identify those patients who may benefit from drugs targeting dna repair pathways and to spare those who are unlikely to benefit . 
driver germline ( inherited ) or somatic ( acquired ) mutations may take the form of sequence or structural variants that generally result in loss of function or aberrant functioning of brca1 / brca2 or other genes encoding members of the hr pathway . 
the genes and their protein products involved in hr are numerous , and their interactions are complex . germline mutations in hr - associated genes in addition to germline brca1 / brca2 mutations , clinical genetic testing panels now include a number of proposed breast cancer predisposition genes , although not all of these genes have definitively been shown to increase breast cancer risk . 
other hereditary predisposition genes involved in hr that are proven to be moderate to high risk include palb2 , atm , and chek2 . more recently , bard1 and rad51d have been shown to increase breast cancer risk , whereas some genes ( nbn , mre11a , rad50 , rad51c , brip1 ) are unlikely or confirmed not to increase breast cancer risk.15 interestingly , some of these hr genes do increase the risk of ovarian cancer , suggesting that the underlying biology of breast and ovarian cancer is different despite the importance of the role of hrd in both of these malignancies . although considered brca - like , it is not clear if breast cancers arising from these germline mutations are as sensitive to dna - damaging therapies as brca1 / brca2 - mutated breast cancers in large part as a consequence of the rarity and relative recent discovery of these mutations.16 incidence and accurate risk estimates are emerging for non - brca germline mutations , but the prognosis and response to anticancer therapy remain unknown.15 , 17 somatic mutations in hr genes somatic mutations may also arise in genes involved in hr . 
as in ovarian cancer , where somatic mutations in brca1 / brca2 occur in up to 7% of patients , 19 somatic brca1 / brca2 mutations constitute up to 3% of unselected patients with breast cancer20 and likely contribute to the brca - like phenotype , where dna - damaging therapy may also be effective . 
the extent to which these hr genes drive tumorigenesis continues to be explored , but it is likely that they too contribute to the brca - like phenotype . looking beyond germline brca1 / brca2 mutations has implications in terms of choosing patients who stand to benefit from dna - damaging therapies , most notably parpis . 
how this can be achieved is not certafor example , in ovarian cancer , the parpi niraparib resulted in a significant increase in progression - free survival irrespective of brca1 / brca2 mutation status or hrd status ( by myriads mychoice hrd , salt lake city , ut ) for patients with recurrent and highly platinum - sensitive disease.22 unlike in ovarian cancer , parpis in nonbrca1 / brca2mutated breast cancer have shown little activity to date , likely highlighting a different underlying biology , although patient selection may also be a factor . 
early - phase clinical trials of parpis in metastatic tnbc and brca - wt her2 - negative breast cancer are underway , with correlative hrd assessment ( clinicaltrials.gov identifiers : nct02401347 and nct00707707 )  . gene panels of hrd as researchers began to understand the complex nature of hrd , with contributions beyond brca1 / brca2 function , the focus shifted to characterization of brca1 - associated gene expression patterns to identify sets of differently expressed genes . 
seventy - seven of the 115 her2 - negative cohort were predicted to have dna repair deficiency by one of these signatures or by the presence of brca1 / brca2 germline mutations ( 56 of 59 tnbc and 21 of 56 er positive )  . 
thus , the genes involved in hr are not yet well defined , and equal weighting may overestimate hrd , as seen in a study of ovarian cancer.25 similarly , predictive model systems based on an empirical set of genes differentially expressed in brca1 / brca2mutated breast cancers are unlikely to clearly define hrd . 
these caveats represent major limitations to the hr panels currently being developed . epigenetic changes brca1 promoter methylation ( pm ) , which is unique to brca1 and mutually exclusive of germline brca1 mutations , 26 has also been implicated in hrd ( fig 1b )  . 
the importance of brca1 pm alone in this study is difficult to interpret , and results may be explained by deficiencies in brca1 as a result of germline mutations or by mrna expression . 
currently , the role of brca1 pm in hrd remains controversial . copy number aberrations copy number aberration / alteration ( cna ) refers to acquired changes in copy number of genes in tissue , such as tumor , whereas copy number variant ( cnv ) refers to changes in copy number of genes in the germline , affecting all cells in an individual . 
cnvs may also be reported in cancer , although they are usually qualified with the term acquired as compared with constitutional , so as to differentiate between the somatic and germline settings . 
in contrast to entire chromosome number gains or losses ( ie , aneuploidy ) , cna / cnvs are on a much smaller , generally submicroscopic , scale , with the size of dna copy - number alterations ( gain or loss ) being  . 
although the extent to which cnas contribute to tumorigenesis is not entirely known , some of the well - established driver events in cancer are cnas ( eg , myc , her2 , cyclin d1 )  . 
furthermore , an increased burden of cnas is associated with higher genomic instability and subsequent malignant transformation.31 using dna microarray technologies , such as array comparative genomic hybridization ( acgh ) , entire genome imbalances can be identified . 
this technique compares test dna and control dna , allowing the relative fluorescent intensity to be quantified , providing information on relative copy number sequences in the test genome versus the control genome.32 clinically , acgh was first reported using a classifier of brca1 - like tumors on the basis of cna in brca1 - mutated breast cancers.33 this study included 230 patients with stage iii her2negative breast cancer randomly assigned to adjuvant high - dose platinum - based or anthracyclinebased chemotherapy . 
all were statistically significant , and test for interaction was positive . studies of nonplatinum - containing regimens have not shown a benefit in patients with brca1 - like signatures identified by this method . a study in patients with tnbc treated with adjuvant ac ; fec ; docetaxel , doxorubicin , cyclophosphamide ; or cyclophosphamide , methotrexate , fluorouracil chemotherapy found that 65% had brca1 - like disease but with no statistically significant difference in 5 - year rfs in any of the treatment arms.35 similarly , a neoadjuvant study of dose - dense ac or capecitabine / docetaxel in 163 her2 - negative breast cancers showed tumors identified as brca1 - like by this method were not predictive of chemotherapy response even though present in 57% of patients with tnbc.36 these studies suggest that brca1 - like tumors , as defined by acgh , are most commonly associated with tnbc , and platinum - containing regimens are beneficial in those with a brca1 - like signature , whereas nonplatinum - containing regimens fail to improve responses over those without a brca1 - like signature . 
however , the above studies used unusual regimens of high - dose platinum and intensified alkylating agents that are not standard of care , and the response seen in the brca1like group may be due to intensified alkylator therapy . 
the acgh classifier also failed to identify some patients with brca1 / brca2 germline mutations , making it a promising but incomplete test of hrd . structural rearrangements inversions , translocations , and recombination change the location or orientation of a dna sequence.14 translocations result in the exchange of dna between nonhomologous regions of dna . 
recombination results in exchange of dna between homologous regions of dna , and this structural rearrangement may lead to loss of heterozygosity ( loh ) , a gross chromosomal event that results in the loss of entire genes ( eg , brca1 , brca2 )  . two types of acquired loh are important to note : deletion loh , where there is a copy number loss ; and copy numberneutral loh , where the absolute copy number remains the same ( fig 1d )  . 
both deletion and copy number neutral loh , as with cnas , lead to allelic imbalance that can be inferred by studying singlenucleotide common variation across the genome ( single - nucleotide polymorphism [ snp ] analysis ) ; this may be in the form of other types of dna microarrays that may be fully or partially based on snp probes across the genome . three tests of structural rearrangements have come to the forefront : telomeric allelic imbalance ( tai ) , large - scale transition ( lst ) , and loh . tai was developed using a snp genotype array platform37 to detect the number of chromosomal regions with allelic imbalance extending to the subtelomere , a common genomic abnormality that leads to an unequal contribution of maternal and paternal dna sequence but does not necessarily change overall dna copy number . 
breakpoints of tai regions were nonrandom and enriched for cnvs , which results in an imbalance and then leads to hrd , which may result in platinum sensitivity in the way that brca1associated cancer responds . 
allelic imbalance was the best predictor of cisplatin sensitivity after identifying associations between a variety of subchromosomal abnormalities and cisplatin sensitivity , and tai predicted higher rates of pcr in 79 patients enrolled in the neoadjuvant cisplatin - 1 ( monotherapy ) and cisplatin - 2 ( cisplatin plus bevacizumab ) tnbc trials . lst measures chromosomal breaks between adjacent chromosomal regions of at least 10 mb . 
lst was developed using snp array analysis on 65 patients with basal - like ( an intrinsic breast cancer subtype that overlaps with approximately 80% of tnbc ) breast cancer to define brca1 - associated genomic instability.38 lst was predictive of brca1 status and identified 85% of proven brca1 - inactivated cases . 
15 mb and less than a whole chromosome and was recognized as a discriminatory assay in two independent data sets of ovarian tumors.39 loh was more frequently identified in tumors with defective brca1 / brca2 and detected hrd regardless of etiology . 
the combination of all three scores has been shown to correlate with brca1 / brca2 deficiency in all breast cancer subtypes and captures more brca1 / brca2 deficiency information than the individual scores.27 in the geparsixto study42 of neoadjuvant paclitaxel / liposomal doxorubicin with or without carboplatin , the unweighted sums of loh , tai , and lst , in addition to brca1 / brca2 mutation in the primary tumor ( n = 193 ) , found hrd in 70.5% of tnbc tumors ; 60.3% without a brca mutation in the primary tumor were hrd high . 
in the phase iii treating to new targets ( tnt ) study , patients with metastatic tnbc were treated with carboplatin or docetaxel.8 the dichotomized score did not select those patients who would be sensitive to carboplatin versus docetaxel . 
the response rate was 38.2% in patients with hrd - high disease treated with carboplatin versus 42.6% in patients with hrd - high disease treated with docetaxel ; response rate was 29.2% in patients with hrdlow disease treated with carboplatin , versus 34.7% in patients with hrd - low disease treated with docetaxel . 
there is a paucity of published data on the ability of this assay to discriminate between hr - defective tumors and hr - intact tumors on the basis of tissue from a metastatic lesion . 
herein lies a possible explanation for the discrepancy of findings from the tnt trial , in that the assay may be measuring a scar of what has been but does not necessarily reflect what is occurring in the cell at present . 
to determine hr function , viable cells first need to be subjected to dna - damaging insults ( eg , radiation ) followed by assessment of hr . formation of rad51 foci is a functional , or live , assessment of a cells ability to perform hr . 
one study showed that low rad51 scores were more common in tnbc and associated with high grade and high ki - 67 and strongly predicted pcr.46 in this study of sporadic breast cancers receiving anthracycline - based chemotherapy , 68 patients underwent biopsies 24 hours post chemotherapy with rad51 focus formation assessed by immunofluorescence . 
in another study , 54 her2negative fresh primary breast tumors underwent ex vivo irradiation followed by analysis of the formation of ionizing radiationinduced foci of rad51 , and those with impaired foci formation underwent further genetic and epigenetic analysis.47 again , this hr defect was significantly associated with tnbc , but only five of 45 tumors with sufficient numbers of proliferating tumor cells were rad51 - formation deficient . 
more recently , functional assessment of rad51 foci formation in response to ex vivo irradiation coupled with whole - exome sequencing to determine structural genomic alterations ( ie , genomic scar ) showed that the combination of deficient rad51 foci formation and elevated lst or dna repair mutational panel may identify genetic alterations of an hr gene as a result of somatic or germline mutation.48 none of these studies reported outcomes , and they are limited by small numbers , but functional assessment of hr is promising and further studies are warranted . discussion the ability to consistently measure clinically meaningful deficiencies in hr has proven a difficult task . 
developing a reliable biomarker will be key to identifying patients with hrd tumors who may benefit from hrd - targeted therapies . studies attempting to use gene panels known to be involved in hr make sense mechanistically , but it is clear that not all genes are equal in the process , and basing a score on a composite of these genes may overestimate hrd . 
similarly , identifying brca1 pm has not consistently been shown to be useful in defining hrd tumors , as highlighted in the study where patients with either germline brca1 / brca2 mutations , low brca1 mrna expression , or brca1 pm were analyzed together . although platinum - based neoadjuvant chemotherapy resulted in improved os for the entire cohort , the impact brca1 pm had on clinical outcomes remains unclear . the acgh classifier was able to show that patients with brca - like tumors had significantly better rfs and os when treated with high - dose platinum - based chemotherapy versus conventional anthracycline - based chemotherapy . 
however , in the subset of patients with tnbc , the acgh classifier failed to identify nearly 40% of patients with a germline brca1 / brca2 mutation , and the experimental high - dose alkylator chemotherapy regimens used in this study are not standard and confound the findings of this study . more recent tests of hrd that are based on snp analysis have been combined in various ways , such as the myriad genetics mychoice hrd assay ( hrd - tai , hrd - loh , hrd - lst )  . 
this assay is the most developed for clinical use , with promising results in platinum - based neoadjuvant clinical trials of breast cancer with the primary end point of pcr . 
even when patients with known germline brca1 / brca2 were removed from analysis , those with high scores had better rates of pcr . in the metastatic setting , the mychoice hrd assay failed to select those patients who may benefit from platinum - based therapy in the tnt study . 
this discrepancy supports emerging evidence that early - stage breast cancer and advanced disease are different entities whereby treatment - resistant clones emerge in advanced disease , resulting in different tumor characteristics that may involve reversions from an hrdeficient state to an hr - efficient state . 
thus , the approach to identify biomarkers will need to take temporal tumor evolution into consideration . hrd assays that have been developed to date and that focus on the genotype are similar in that they measure a scar , a record of what the genome has been . 
it is known that brca1 / brca2 - deficient cells can over time regain their ability to perform hr , and current biomarkers of hrd are limited copy gains copy losses loss of heterozygosity structural variants genome transcriptome fig 2 . 
in addition to cataloging somatic point mutations and small insertions / deletions , the use of wholegenome sequencing enables characterization of large - scale copy - number variation , loss of heterozygosity , and structural variation . 
patient - derived xenografts represent reasonable models of the human breast tumor49 that could be used to explore real - time functional hr versus measures of hr by other methods described in this review and provide further insight into understanding hrd . ultimately , whole - genome sequencing can provide direct or supportive evidence of almost all the information that each of the above assays is intending to measure ( fig 2 )  . 
this approach , combined with brca mutation status , accurately detected all classes of genomic alterations in the assessment of rucaparib in ovarian cancer : phase 2 clinical trial ( ariel2 ) trial of ovarian cancer , 50 and wholegenome sequencing of breast cancers has identified three signatures that seem to be associated with hrd.18 however , until the cost of whole - genome sequencing decreases , scientists and clinicians are left to find less - expensive alternatives . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . meta - summary there is evidence that hrd assays have predictive value for response to platinum and possibly parpis in combination with standard therapy . 
head - to - head comparisons of the different hrd assays have not been performed , and it is not clear which assays or combination of assays is the best predictor of hrd . 
the asco ( 2014 and 2015 ) and san antonio breast cancer symposium ( 2014 to 2016 ) databases were searched at the title and abstract levels using the search terms breast cancer , brca1 , brca2 , and homologous recombination deficiency . 
nucleic acids res 40 : nature 535 : 382 - 387 , 2016 5795 - 5818 , 2012 von minckwitz g , schneeweiss a , loibl s , et al : neoadjuvant carboplatin in patients with triple - negative and her2positive early breast cancer ( geparsixto ; gbg 66 ) : a randomised phase 2 trial . 
sikov wm , berry da , perou cm , et al : impact of the addition of carboplatin and / or bevacizumab to neoadjuvant once - per - week paclitaxel followed by dose - dense doxorubicin and cyclophosphamide on pathologic complete response rates in stage ii to iii triple - negative breast cancer : calgb 40603 ( alliance )  . 
tutt a , ellis p , kilburn l , et al : the tnt trial : a randomized phase iii trial of carboplatin ( c ) compared with docetaxel ( d ) for patients with metastatic or recurrent locally advanced triple negative or brca1 / 2 breast cancer ( cruk / 07 / 012 )  . 
antoniou a , pharoah pd , narod s , et al : average risks of breast and ovarian cancer associated with brca1 or brca2 mutations detected in case series unselected for family history : a combined analysis of 22 studies . 
couch fj , hart sn , sharma p , et al : inherited mutations in 17 breast cancer susceptibility genes among a large triplenegative breast cancer cohort unselected for family history of breast cancer . 
sharma p , klemp jr , kimler bf , et al : germline brca mutation evaluation in a prospective triple - negative breast cancer registry : implications for hereditary breast and / or ovarian cancer syndrome testing . 
akashi - tanaka s , watanabe c , takamaru t , et al : brcaness predicts resistance to taxane - containing regimens in triple negative breast cancer during neoadjuvant chemotherapy . 
couch fj , hu c , lilyquist j , et al : breast cancer risks associated with mutations in cancer predisposition genes identified by clinical genetic testing of 60 , 000 breast cancer patients . 
nik - zainal s , davies h , staaf j , et al : landscape of somatic mutations in 560 breast cancer whole - genome sequences . nature 534 : 47 - 54 , 2016 19 . 
hennessy btj , timms km , carey ms , et al : somatic mutations in brca1 and brca2 could expand the number of patients that benefit from poly ( adp ribose ) polymerase inhibitors in ovarian cancer . 
winter c , nilsson mp , olsson e , et al : targeted sequencing of brca1 and brca2 across a large unselected breast cancer cohort suggests that one - third of mutations are somatic . 
van t veer l , esserman l , sanil a , et al : dna repair deficiency biomarkers identify hr + / her2breast cancer patients who may benefit from veliparib / carboplatin : results from the i - spy 2 trial . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deficiency among breast cancer subtypes . 
sharma p , stecklein s , kimler bf , et al : brca1 insufficiency is predictive of superior survival in patients with triple negative breast cancer treated with platinum based chemotherapy . 
bergamaschi a , kim yh , wang p , et al : distinct patterns of dna copy number alteration are associated with different clinicopathological features and gene - expression subtypes of breast cancer . 
vollebergh ma , lips eh , nederlof pm , et al : an acgh classifier derived from brca1 - mutated breast cancer and benefit of high - dose platinum - based chemotherapy in her2 - negative breast cancer patients . 
schouten pc , marme f , aulmann s , et al : breast cancers with a brca1 - like dna copy number profile recur less often than expected after high - dose alkylating chemotherapy . 
popova t , manie e , rieunier g , et al : ploidy and large - scale genomic instability consistently identify basal - like breast carcinomas with brca1 / 2 inactivation . 
telli ml , jensen kc , vinayak s , et al : phase ii study of gemcitabine , carboplatin , and iniparib as neoadjuvant therapy for triple - negative and brca1 / 2 mutation - associated breast cancer with assessment of a tumor - based measure of genomic instability : precog 0105 . 
isakoff sj , mayer el , he l , et al : tbcrc009 : a multicenter phase ii clinical trial of platinum monotherapy with biomarker assessment in metastatic triple - negative breast cancer . 
von minckwitz g , timms k , untch m , et al : prediction of pathological complete response ( pcr ) by homologous recombination deficiency ( hrd ) after carboplatin - containing neoadjuvant chemotherapy in patients with tnbc : results from geparsixto . 
telli ml , mcmillan a , ford jm , et al : homologous recombination deficiency ( hrd ) as a predictive biomarker of response to neoadjuvant platinum - based therapy in patients with triple negative breast cancer ( tnbc ) : a pooled analysis . 
connolly r , elkin e , timms k et al : homologous recombination deficiency ( hrd ) as a predictive biomarker of response to preoperative systemic therapy ( pst ) in tbcrc008 comprising a platinum in her2 - negative primary operable breast cancer . 
powell sn , riaz n , mutter rw , et al : a functional assay for homologous recombination ( hr ) dna repair and whole exome sequencing reveal that hr - defective sporadic breast cancers are enriched for genetic alterations in dna repair genes . 
zhang x , claerhout s , prat a , et al : a renewable tissue resource of phenotypically stable , biologically and ethnically diverse , patient - derived human breast cancer xenograft models . 
mcneish ia , oza am , coleman rl , et al : results of ariel2 : a phase 2 trial to prospectively identify ovarian cancer patients likely to respond to rucaparib using tumor genetic analysis . 
 systemic immunotherapy effective for refractory extramedullary acute myeloid leukemia mansour alfayez , md1 ; doina ivan , md1 ; naveen pemmaraju , md1 ; naval daver , md1 ; and courtney d . 
not letting the exception pass by unnoticed , dr coley harnessed this observation and injected a number of his patients with bacterial toxins ( coleys toxin )  . this toxin represented a powerful superantigen , leading to dramatic immune system upregulation , including massive polyclonal t - cell activation and cytokine release leading to tumor regression in a notable minority of cases . 
although the mechanism was not understood at that time , this observation captures an important concept : cancer is dependent on immune escape.2 immunity for the treatment of hematologic malignancies , including acute myelogenous leukemia ( aml ) , has been leveraged for decades in the form of allogeneic stem - cell transplantation.3 - 5 aside from allogeneic stemtransplantation , other immune - based strategies cell have been evaluated in aml , including bacillus calmettegu erin vaccination , interleukin - 2 , and interferon alfa , all of which have shown inferior results compared with standard chemotherapy.2 , 6 - 10 however , those strategies were not specic and were not directed against specic immune escape pathways used by malignant cells . 
more recently , with the discovery of immune checkpoint inhibitors ( icpi ) and the successful redirection of the immune system for the treatment of various solid tumors , using the same concept in hematologic malignancy is alluring . we herein report on a 68 - year - old man with refractory extramedullary aml who successfully achieved remission using icpi . 
the patient was originally diagnosed at age 65 years with stage iiia melanoma in the left upper posterior arm ( appendix fig a1 ) , which was treated with surgical excision and lymph node resection , followed by radiation therapy in 2014 . 
the patient went into remission without evidence of recurrence on follow - up imaging ( fig 1 )  . one year later ( october 2015 ) , the patient was referred to the leukemia department with pancytopenia . 
bone marrow aspirate and biopsy revealed myelodysplastic syndrome , 2% blasts , with complex cytogenetics and mutation in nucleophosmin 1 ( npm1 ) and dna methyltransferase 3 alpha ( dnmt3a )  . 
he received a total of 19 cycles , with including full hematologic recomplete remission , covery , resolution of dysplastic morphology on subsequent bone marrow examinations , and cytogenetic remission . 
eighteen months after his original myelodysplastic syndrome diagnosis , the patient was noted to have a dark - colored skin lesion on the left upper arm that was suggestive of melanoma recurrence ( fig 2 )  . positron emission tomography / computed tomography scan showed a single uorodeoxyglucose - avid lesion in the skin and subcutaneous region of the left upper arm ( fig 2 )  . 
the patient then received two cycles of intensive cytarabine - based chemotherapy with cladribine 5 mg / m2 , idarubicin 10 mg / m2 , and cytarabine 1 g / m2 days 1 to 3 every 28 days , with follow - up positron emission tomography scan after two cycles showing progressive disease ( fig 3 )  . 
surveillance bone marrow examination showed myelodysplasia with 2% blasts , diploid cytogenetics , and dnmt3a mutation identied , and npm1 mutation no longer detected at variant allele frequency level of sensitivity of approximately 1% . 
given the progressive yet self - contained extramedullary disease to sites within the left upper arm , the patient was then treated with nine fractions of radiotherapy ( 10 gy ) , without evidence of response to radiation therapy . 
the treatment regimen consisted of azacitidine 75 mg / m2 ( days 1 to 7 ) and nivolumab 3 mg / kg ( day 1 and day 14 ) every 28 days , in addition to ipilimumab 1 mg / kg every 42 days . 
 alfayez et al lymph node resection followed by radiation october 15 , 2014 intensive cytarabine - based chemotherapy ( clia ) 2 cycles june 21 , 2017 radiotherapy september 7 , 2017 guadecitabine ( sgi - 110 ) 19 cycles october 26 , 2015 progressive disease september 15 , 2017 remission november 8 , 2017 stage iiia melanoma october 1 , 2014 progressive disease august 17 , 2017 azacitidine plus nivolumab plus ipilimumab september 18 , 2017 leukemia cutis may 26 , 2017 myelodysplastic syndrome october 1 , 2015 fig 1 . 
the patient continued receiving treatment for another cycle , and a skin biopsy after cycle 2 was negative for cd33 myeloid sarcoma , instead demonstrating lymphocyte ( cd3 + ) inltration , with predominant t - cell predominance of cd8 over cd4 + lymphocytes ( including cd4 + histiocytes ; fig 4 )  . 
the patient has continued receiving this combination therapy and so far received six cycles , with continued clinical and radiologic clearance of his skin lesion ( fig 4 ) and ongoing bone marrow response . inhibitors are antibodies directed immune checkpoint against t - cell inhibitory signals to modulate the interaction between cytotoxic t cells and tumor cells . 
activating programmed cell death protein 1 ( pd - 1 ) prevents cd28 / b7 signaling that is crucial for cd8 t - cell activation.11 pd - 1 interactions and programmed death - ligand 1 ( pd - l1 ) inhibited antitumor immune responses in a murine aml model.12 treatment with antipd - 1 antibody improved survival in those models , indicating the importance of the pd - 1 / pd - l1 pathway in immune evasion by aml blasts as well as providing a rationale for clinical trials targeting this pathway in aml ( eg , with nivolumab ) .12 seventeen - color multiparameter ow cytometry was reported on 38 patients with relapsed aml , 36 patients with untreated aml , and eight healthy controls . 
all t - cell subpopulations ( cd3 + , cd4 + , and cd8 + t cells ) had signicantly higher pd1 expression in relapsed aml ( p , .006 ) and untreated aml ( p , .05 ) compared with healthy controls.13 this suggests that pd1 overexpression is an escape route used by leukemia . 
this nding was also supported in other reports.14 - 16 in a report , t - cell receptor ( tcr ) clonotypes that were minimal or undetectable became enriched after nivolumab administration , and one patient had marked reduction in tcr diversity indexes and clearance of measurable residual disease with tcr clone directed against wilms tumor 1 ( wt1 ) .17 in an ongoing phase ib / ii study of nivolumab in combination with azacitidine in relapsed aml ( clinicaltrials.gov identier : nct02397720 ) , 70 evaluable patients were reported with 63% overall response rate , which compared favorably to historical response rate of 15% to 20% treated at the same institute . 
expression of cd86 was reported on aml blasts in more than half of 100 samples tested , and , in some cases , the level of expression was so high that it was equivalent to that of mature monocytes and activated b lymphocytes , 20 which gives a rationale for targeting this pathway ( eg , with ipilimumab )  . 
in a phase i / ib multicenter trial of ipilimumab in patients with relapsed hematologic cancers after allogeneic stem cell transplantation , 12 patients with relapsed aml and another four with extramedullary relapsed disease were included . 
 ( c ) skin lesion at the time of presentation . immunohistochemical studies demonstrating neoplastic cells positivity for ( d ) cd33 , ( e ) myeloperoxidase ( mpo ) , and ( f ) cd43 . locus16 and dose - dependent upregulation of pd - l1 , pd - l2 , pd - 1 , and cytotoxic t - lymphocyte associated protein 4 ( twofold or greater ) .16 there was trend toward increased expression of those checkpoints in hma - resistant patients compared with sensitive patients , suggesting upregulation of inhibitory immune signals as a mechanism of resistance to hmas . 
 ( c ) positron emission tomography / computed tomography post cycle 2 of cladribine , idarubicin , and cytarabine shows previously identied cutaneous nodule within the left posterior arm has increased in number and uorodeoxyglucose activity . 
 ( a - d ) skin immunohistochemical studies post cycle 2 of azacitidine with dual checkpoint inhibition showing negative cd 33 , t - cell lymphocyte ( cd3positive ) inltration , and predominance of cd8 over cd4 + lymphocytes . 
 ( g ) positron emission tomography / computed tomography post cycle 6 of azacitidine with dual checkpoint inhibition demonstrates complete metabolic response to therapy in terms of previously identied multiple cutaneous and subcutaneous nodules in the left arm . the hypothesis that concomitant administration of immune checkpoint inhibitors in combination with hmas may overcome resistance via immune evasion.16 aml with mutant npm1 is considered to be of favorable risk , and , interestingly , one suggested explanation relates to immune responses developed against epitopes derived from the mutated region of npm1 . 
higher pd - l1 expression in npm1 mutated patients , particularly in leukemic stem / progenitor cells , has been noted , potentially making this particular subgroup of aml more likely to benet from icpi treatment.23 - 25 in this particular case , myeloid sarcoma arising from a previous melanoma site , in a patient with complete remission from previously diagnosed myelodysplastic syndrome , highlights important questions , as does the excellent response to icpi . 
we wondered if the local microenvironment has immune - based hosting and homing characteristics ( ie , poor immune surveillance ) , which leads to weak containment of neoplastic cell expansion . 
also , it is interesting to note that , leukemia cutis started as single lesion , then had what we think was an intransit metastasis with multiple sentinel lesions ( fig 3 )  . 
although no clear data exist to date , this case and previous cases of myeloid sarcoma and leukemia cutis suggest icpi therapy may be an effective treatment modality for patients with isolated extramedullary aml . in conclusion , we report on the successful treatment of primary refractory myeloid sarcoma with hypomethylating agent therapy in combination with pdl1 and cytotoxic t - lymphocyte associated protein 4 inhibition . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . research funding : novartis , stemline therapeutics , incyte , samus therapeutics , abbvie , cellectis , affymetrix / thermo fisher scientic , daiichi sankyo , plexxikon travel , accommodations , expenses : stemline therapeutics , celgene , mustang bio naval daver consulting or advisory role : celgene , agios pharmaceuticals , jazz pharmaceuticals , pzer , abbvie , astellas pharma , daiichi sankyo , novartis , bristol - myers squibb research funding : bristol - myers squibb , pzer , immunogen , genentech , nohla therapeutics , abbvie , astellas pharma , servier , daiichi sankyo naveen pemmaraju honoraria : incyte , novartis , lfb biotechnologies , stemline therapeutics , celgene consulting or advisory role : incyte , novartis , lfb biotechnologies , stemline therapeutics , celgene courtney d . 
hall ss : a commotion in the blood : life , death , and the immune systenew york , ny , henry holt , 1997 alfayez m , borthakur g : checkpoint inhibitors and acute myelogenous leukemia : promises and challenges . 
expert rev hematol 11 : 373 - 389 , 2018 schmid c , labopin m , nagler a , et al : donor lymphocyte infusion in the treatment of rst hematological relapse after allogeneic stem - cell transplantation in adults with acute myeloid leukemia : a retrospective risk factors analysis and comparison with other strategies by the ebmt acute leukemia working party . j clin oncol 25 : 4938 - 4945 , 2007 4 . 
blood 75 : 555 - 562 , 1990 sullivan km , weiden pl , storb r , et al : inuence of acute and chronic graft - versus - host disease on relapse and survival after bone marrow transplantation from hla - identical siblings as treatment of acute and chronic leukemia . 
blood 73 : 1720 - 1728 , 1989 powles rl , russell j , lister ta , et al : immunotherapy for acute myelogenous leukaemia : a controlled clinical study 2 1 / 2 years after entry of the last patient . 
int j oncol 2 : 469 - 472 , 1993 goldstone ah , burnett ak , wheatley k , et al : attempts to improve treatment outcomes in acute myeloid leukemia ( aml ) in older patients : the results of the united kingdom medical research council aml11 trial . 
meloni g , vignetti m , andrizzi c , et al : interleukin - 2 for the treatment of advanced acute myelogenous leukemia patients with limited disease : updated experience with 20 cases . 
daver n , basu s , garcia - manero g , et al : dening the immune checkpoint landscape in patients ( pts ) with acute myeloid leukemia ( aml )  . 
andorsky dj , yamada re , said j , et al : programmed death ligand 1 is expressed by non - hodgkin lymphomas and inhibits the activity of tumor - associated t cells . 
yang h , bueso - ramos c , dinardo c , et al : expression of pd - l1 , pd - l2 , pd - 1 and ctla4 in myelodysplastic syndromes is enhanced by treatment with hypomethylating agents . 
liu h , park j - h , fulton n , et al : tcr clonal evolution in aml patients in morphologic remission treated with anti - pd1 antibody , nivolumab . 
daver n , basu s , garcia - manero g , et al : phase ib / ii study of nivolumab in combination with azacytidine ( aza ) in patients ( pts ) with relapsed acute myeloid leukemia ( aml )  . 
greiner j , ono y , hofmann s , et al : mutated regions of nucleophosmin 1 elicit both cd4 ( + ) and cd8 ( + ) t - cell responses in patients with acute myeloid leukemia . 
greiner j , schneider v , schmitt m , et al : immune responses against the mutated region of cytoplasmatic npm1 might contribute to the favorable clinical outcome of aml patients with npm1 mutations ( npm1mut )  . 
greiner j , hofmann s , schmitt m , et al : acute myeloid leukemia with mutated nucleophosmin 1 : an immunogenic acute myeloid leukemia subtype and potential candidate for immune checkpoint inhibition . 
 poly ( adp - ribose ) polymerase inhibitors for de novo brca2 - null small - cell prostate cancer introduction neuroendocrine prostate cancer ( nepc ) represents 0.5% to 2% of all primary prostate cancers ( pcas ) , 1 and primary pure nepc is even more rare . 
pure small - cell prostate carcinoma ( scpc ) , a subtype of nepc , can occur in two different settings : exceptionally , it can develop de novo ; more frequently , small cells are detected during the evolution to castration - resistant prostate cancer ( crpc ) 2 as a consequence of androgen suppressive therapy . scpc is a proliferation of small and round cells with a high mitotic index and immunohistochemistry staining for synaptophysin , chromogranin a ( cha ) , or neuron - specific enolase , 3 whereas prostate - specific antigen ( psa ) and androgen receptor ( ar ) expression often are associated with a tmprss2 - erg fusion detected in 50% of scpcs.2 , 4 in all cases , the neuroendocrine presentation is associated with poor prognosis and frequent visceral , bone , or brain metastases , which contrasts with a low or normal psa . 
whole - body [ 18f ] fluorodeoxyglucose ( fdg ) positron emission tomography ( pet ) / ct scan showed a large left lobe prostatic infiltration and detected bulky retroperitoneal iliac nodes and l2 to l3 abnormal fdg uptake ( fig 1a )  . 
the patient was treated with luteinizing hormone releasing hormone ( lhrh ) agonist because of the rapid rise in psa and focal ar staining on biopsy specimens . initial treatment : cisplatin and etoposide regimen the patient received six courses of cisplatin 33 mg / m2 / d and etoposide 100 mg / m2 / d for 3 days and every 3 weeks and lhrh agonists . 
after three cycles , the symptoms disappeared , and pet / ct scan showed a major metabolic and biologic response ( psa , 0.18 ng / ml ) confirmed after six courses ( figs 1a and 1b )  . 
important adverse effects occurred , and lhrh agonist was maintained alone . second - line treatment : topotecan regimen nine months after the end of platinum therapy , progression was detected on the right - side adrenal gland with abnormal fdg uptake . 
 prostate - specific antigen ( psa ) and neuron - specific enolase ( nse ) concentrations are plotted on the left y - axis and chromogranin a on the right y - axis with the upper limit of normal represented with dotted lines of the corresponding colors . 
 to identify clinically actionable gene mutations and putative druggable pathways , gene copy number aberrations and somatic mutation status were identified by using whole - genome array comparative genomic hybridization and targeted next - generation sequencing , respectively , of 559 genes as previously described5 , 6 ( gene panel provided in the data supplement )  . 
the array comparative genomic hybridization analysis showed a genomic instability associated with a brcalike profile associated with a homologous repair deficiency ( hrd ) score of 197 ( fig 2a ) , which was calculated on the basis of the number of lost regions with intermediate size ( > 15 mb ) known to be more frequently observed in brca defective tumors . 
 from left to right , the chromosome 13 ideogram with its genomic profile exhibits several copy number aberrations ; the zoom - in on the 13q12.2 to q13 heterozygous lost region 13 : 24 , 648 , 264 to 41 , 238 , 009 ( 16.5 mb ) includes brca2 . copy number aberrations showed ar amplification ( > 11 copies ) and regional heterozygous losses , including brca2 ( fig 2b ) and tp53 genes ( data not shown )  . 
gene transition profiles with breakages in both tmprss2 and erg loci suggested an unbalanced translocation and the presence of a tmprss2 - erg fusion ( data not shown )  . 
the germinal brca2 mutation could have come from the patients fathers side , where a breast cancer aggregation had been observed in the patients sister and two of his fathers aunts ( fig a1 )  . 
pathology analysis found the same nepc and pca - related stainings ( fig 3 )  . third - line treatment : parpi three months later , pet / ct scan revealed a new radiologic progression ( vertebrae and retroperitoneum nodes ) with biologic progression ( figs 1b and c )  . 
after 2 months , pet / ct scan showed a complete response , which was maintained after 12 months treatment ( fig 1c )  . in november 2017 , 4 years after initial diagnosis , the patient was free from tumor symptoms , and serum markers were normal . 
optic microscope photographs show positive staining for synaptophysin ( syn ; magnification , 10 ) , androgen receptor ( ar ; magnification , 10 ) , prostate - specific antigen ( psa ; magnification , 20 ) , prostate - specific acid phosphatase ( psap ; magnification , 20 ) , and ets - related gene ( erg , magnification , 20 ) alpha - methylacyl - coa racemase enzyme ( p504s )  . 
 these stainings are typical of both prostate adenocarcinoma and small neuroendocrine cells . psap p504s but because of the rarity and inconsistent definition of the neuroendocrine disease among studies , no gold standard has been established . 
 guidelines recommend the use of aggressive chemotherapy , such as platinum salts and etoposide , for pure de novo scpc , but for advanced pure or mixed scpc that occurs during adenocarcinoma treatment , docetaxel - based regimen with or without anti - androgen usually is used if the patient is fit enough.2 , 9 at diagnosis , the current patient had elevated serum psa and partial immunostaining for tumor psa and ar ; hence , he benefited from lhrh agonist treatment , which suggests that the tumor was at least partly androgen driven . 
in brca - mutated tumors , inhibition of parp increases the genomic instability and leads to cell lethality when unrepaired single - strand breaks evolve to double - strand breaks.15 , 16 a phase ii study reported a good tolerance in 49 patients treated with olaparib alone for progressive nonselected metastatic crpc , and treatment was associated with tumor response on ct scan , psa level reduction , and decreased number of circulating tumor cells in 16 patients ( 33% )  . 
response to treatment was strongly correlated with mutation or deletion in homologous recombination genes.17 in 2016 , olaparib was given a breakthrough therapy designation by the food and drug administration for crpc , 18 and a more systematic screening for dna repair gene mutations for patients with crpc has been proposed.19 , 20 two phase iii studies currently are investigating olaparib ( profound ; clinicaltrials identifier : nct02987543 ) and rucaparib ( triton3 ; clinicaltrials.gov identifier : nct02975934 ) versus a second line of new hormonal therapy ( nht ; enzalutamide or abiraterone ) in advanced crpc with altered dna repair pathway , and one phase iii study is investigating talazoparib plus nht versus placebo plus nht ( talapro - 2 ; clinicaltrials . gov identifier : nct03395197 ) as first - line treatment of crpc , all with a primary end point of improving radiologic progression - free survival . the current study confirms the sensitivity of scpc to platinum drugs as well as parpis in the case of defect in the homologous recombination dna repair system and highlights interest in sequencing tumor samples when dealing with rare disease and limited guidelines . 
 sverine garnier no relationship to disclose nadine carbuccia no relationship to disclose arnaud guille no relationship to disclose nathalie charrier no relationship to disclose jihane pakradouni no relationship to disclose anthony gonalvs research funding : msd ( inst ) , bristol - myers squibb ( inst ) , novartis ( inst ) , cascadian therapeutics ( inst ) , nektar ( inst ) , boehringer ingelheim ( inst ) , eli lilly ( inst ) , abbvie ( inst ) travel , accommodations , expenses : pfizer , novartis , roche , genentech , celgene isabelle brenot - rossi honoraria : 3a pharma , ipsen , astellas pharma consulting or advisory role : janssen pharmaceuticals , astellas pharma , sanofi , 3a pharma travel , accommodations , expenses : 3a pharma franois eisinger honoraria : roche , msd consulting or advisory role : roche research funding : roche , roche ( inst ) travel , accommodations , expenses : roche , sanofi , celgene jochen walz no relationship to disclose graldine pignot honoraria : janssen - cilag , roche , ipsen , astellas pharma consulting or advisory role : janssen - cilag , roche , novartis ( inst ) , msd ( inst ) travel , accommodations , expenses : pfizer , janssen - cilag , ipsen , roche , ferring pharmaceuticals , intuitive surgical franois bertucci no relationship to disclose daniel birnbaum research funding : amgen gwenalle gravis travel , accommodations , expenses : sanofi , janssen pharmaceuticals , bristol - myers squibb , astellas pharma , pfizer , roche affiliations all authors : institut paoli - calmettes , marseille , france . support supported by national cancer institute integrated cancer research site - linstitut national de la sant et de la recherche mdicale grant no . 
wang l , williamson sr , zhang s , et al : increased androgen receptor gene copy number is associated with tmprss2 - erg rearrangement in prostatic small cell carcinoma . 
gonalves a , bertucci f , guille a , et al : targeted ngs , array - cgh , and patient - derived tumor xenografts for precision medicine in advanced breast cancer : a single - center prospective study . 
corn pg , tapia eln , xiao l , et al : confirmatory analysis to determine associations between platinum - sensitivity , molecular signature of combined tumor suppressor defects and aggressive variant prostate carcinomas ( avpc )  . 
flchon a , pouessel d , ferlay c , et al : phase ii study of carboplatin and etoposide in patients with anaplastic progressive metastatic castration - resistant prostate cancer ( mcrpc ) with or without neuroendocrine differentiation : results of the french genito - urinary tumor group ( getug ) p01 trial . 
pomerantz mm , spisk s , jia l , et al : the association between germline brca2 variants and sensitivity to platinum - based chemotherapy among men with metastatic prostate cancer . 
horita n , yamamoto m , sato t , et al : topotecan for relapsed small - cell lung cancer : systematic review and meta - analysis of 1347 patients . 
family analysis shows a breast cancer aggregation on the fathers side and a breast cancer before 50 years of age in the patients sister , which might be related to brca autosomal dominant transmission . 
carl barrett , phd1 ; and jeeyun lee , md3 purpose some gastric cancers harbor met gene amplications that can be targeted by selective met inhibitors to achieve tumor responses , but resistance eventually develops . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction gastric cancer is the fth most common cancer worldwide and the third leading cause of cancerrelated death.1 gastric cancer is a heterogenous disease , the drivers of which remain unclear , making it difcult to treat these patients . 
pembrolizumab was approved for treating gi malignancies with mismatch repair deciencies and for third - line programmed death ligand 1positive gastric cancer based on its recently observed promising antitumor activity.2 , 3 however , it remains urgent to identify a subset of patients with gastric cancer who may benet from molecularly targeted agents . 
one such potential target is met amplication , which is observed in approximately 5% of patients with gastric cancer.3 - 9 savolitinib ( azd6094 , hmpl - 504 , volitinib ) is a potent small - molecule met kinase inhibitor that inhibits met inhibitory concentration kinase at a half - maximal ( ic50 ) of 4 nm and met phosphorylation in tumor cells . savolitinib was found to inhibit cell growth in vitro against tumors with met gene amplication in the absence of hepatocyte growth factor stimulation , with ic50 generally , 10 nm . 
 met inhibitor in met - amplied gastric cancer context key objective we evaluated the mechanisms of acquired resistance to savolitinib in 3 patients with met - amplied gastric cancer who showed a clinical response and then cancer progression using tumor and circulating tumor dna ( ctdna ) sequencing . knowledge generated ctdna is a powerful tool for identifying potential genomic aberrations that emerge during therapy to confer resistance to targeted therapies . 
using a next - generation sequencing 100 - gene panel , we identied the target mechanisms of resistance met d1228v / n / h and y1230c mutations or high copy number met gene amplications that emerge when resistance to savolitinib develops in patients with met - amplied gastric cancer . relevance we demonstrated the utility of ctdna in gastric cancer and conrmed this approach using baseline tumor tissue or rebiopsy . we identied various met mutations previously unidentied in gastric cancer upon progression to savolitinib , as well as met amplications as drivers of savolitinib resistance during monotherapy treatment of patients with met - amplied gastric cancer . circulating tumor dna ( ctdna ) from baseline until progression every 2 cycles to evaluate the tumor biology during treatment with targeted agents . 
the human investigations were performed after approval by a local human investigations committee ( institutional review board ) and in accordance with an assurance led with and approved by the health authority in korea . 
this prospective open - label trial was designed as a single - arm phase ii study at an academic cancer center ( clinicaltrials.gov identier : nct02449551 )  . treatment was administered as follows : savolitinib 800 mg once a day until disease progression or unacceptable toxicity . 
tumor tissue and plasma ctdna samples from 3 patients enrolled in the viktory trial were obtained before treatment , during therapy , and at the time of progression . next - generation sequencing a targeted next - generation sequencing 100 - gene panel was used to analyze matched tumor dna at baseline and progression and longitudinal ctdna to determine the mechanisms of acquired resistance to savolitinib ( az translational genomics labs , boston , ma )  . 
genes included in this panel are provided in appendix figure a1a . sequencing libraries were prepared using the kapa biosystems hyperprep kit ( wilmington , ma ) and roche nimblegen hybridization capture reagents ( basel , switzerland )  . 
raw sequencing data were processed using the bcbio framework.12 the quality of sequencing data was assessed using the multiqc report.13 fastq les were aligned to the reference genome hg38 using bwa mem aligner , 14 yielding a median depth of coverage of 2 , 000 ( range , 1 , 300 - 6 , 600 ) in plasma samples and 1 , 200 ( range , 1 , 100 - 1 , 400 ) in tissue samples . 
variants were called using vardict15 and classied into the following 3 tiers from high to low based on the likelihood of the variant contributing to cancer - relevant processes : known , likely , and unknown.15 copy number analysis of sequencing data were performed using the copy number caller seq2c.16 all plasma samples were analyzed together as a plasma cohort , whereas tissue samples were processed together as a tissue cohort . 
mapping and sequencing statistics for formalin - xed parafn - embedded tumor tissue ( fig a1b ) and ctdna from frozen plasma ( fig a1c ) indicated that  . 90% and 96% of the 100 genes were sequenced with 500 coverage in tumor and ctdna , respectively , providing a quality data set for analysis . et immunohistochemistry and met fluorescent in situ hybridization met immunohistochemistry ( ihc ) was performed using the rabbit monoclonal primary antibody , confirm antitotal met ( sp44 ; ventana medical systems , tucson , az ) according to the manufacturers protocol . 
 frigault et al performed using dual - color dna - specic met / cep7 probes ( abnova , walnut , ca ) , as described previously.5 , 8 results we analyzed the rst 3 patients enrolled in the savolitinib trial , which enrolls patients with gastric cancer with met amplication in the salvage setting . 
patients were screened for the presence of met amplication by tumor sequencing as part of the viktory trial and are conrmed wild type for met.11 the viktory trial screened 715 patients with genomic sequencing , and the incidence of met amplication was 3.5% ( 25 of 715 patients )  . 
in this study , we tested the feasibility of using a 100 - gene panel in patients with met - amplied gastric cancer serially from baseline until disease progression using both matched biopsies and ctdna . 
the patient had microsatellite - stable and her2 - negative gastric cancer ( fig 1a ) and experienced rapid progression after 5 cycles of capecitabine plus oxaliplatin ( initially stable disease ) to extensive dissemination in the lymph nodes ( fig 1b )  . 
the patient responded dramatically to 2 cycles of savolitinib ( fig 1b , middle panel ) , which was concordant with the decrease in the allele frequency of tp53 p190l ( 7% ) , met 1.4 copy number , and myc 3.4 copy number in the ctdna . 
notably , although the patient maintained a radiologic and clinical partial response ( pr ) to savolitinib , low frequencies of met d1228h ( 5% ) , met d1228n ( 5% ) , met d1228v ( 35% ) , and met y1230c ( 3% ) were newly detected . 
met d1228n is a resistant mutation to crizotinib in lung cancer.17 in addition , met d1228v has been shown to induce resistance to type 1 met tyrosine kinase inhibitors in lung cancer.18 finally , met y1230c is associated with resistance to crizotinib in nonsmall - cell lung cancer.19 the high concordance for the copy number level between ctdna 100 - gene sequencing and tumor rebiopsy specimen sequencing supports the usefulness of copy number evaluation from longitudinal plasma ctdna ( appendix fig a2 )  . 
at disease progression , the patient had mostly experienced progression to bone and bone marrow metastases rather than previous lymph nodes , suggesting the emergence of an aggressive clone that spread to the bone and bone marrow at progression . 
our data suggest that , rather than met amplications , met mutations drove the rapid progression observed in this patient ( fig 1c )  . the second patient was a 74 - year - old woman who was diagnosed with gastric cancer with extensive liver metastases at presentation and enrolled in the viktory trial at diagnosis . 
after 4 cycles of savolitinib , with her pr conrmed radiologically , the met copy number was 2.7 and showed a slight increase from diploid , and a tp53 g245d ( 2% ) variant began to emerge as detected in the ctdna . 
after 6 months ( 7 cycles of savolitinib ) , the patient developed radiologic progression . interestingly , in contrast to the newly emerging mutations conferring resistance to savolitinib in patient 1 ( fig 1 ) , the second patient developed a high level of met amplication of 13 copies and cdk6 copy number of 3.9 at progression ( fig 2a )  . 
although both genes are proximal to one another on chromosome 7 , they are not part of the same amplicon because the trap and pik3cg gene loci are between met and cdk6 , and they remained at a normal copy number in both the ctdna and tumor samples at progression ( fig 2b , top panel )  . 
high concordance was observed between the ctdna and tumor tissue dna ( liver metastasis ) with a reincrease in met amplication and cdk6 amplication that was not detected at pr . 
in addition , the ctdna sample at progression indicated that the tp53 g245d substitution containing the clone had expanded , as suggested by an increase from a 2% allele fraction ( at the third follow - up ) to a 22% allele fraction ( at progression )  . 
this was conrmed in the progression rebiopsy , where the same tp53 g245d substitution that was not detected in normal dna had subsequently increased to an 82% allele fraction ( fig 2b , bottom panel )  . the third patient was a 31 - year - old woman who underwent total gastrectomy for gastric cancer in 2013 . 
pathology , clinical assessment , and circulating tumor dna ( ctdna ) monitoring for patient 1 ( b5 - 002 ) identies met d1228 and y1230 mutations as mechanism of resistance to savolitinib . 
 ( a ) hematoxylin and eosin ( he ) , met immunohistochemistry ( ihc ) , and met uorescence in situ hybridization ( fish ; left to right ) from baseline tumor tissue . 
 ( b ) tumor assessment by radiologic assessment at baseline before savolitinib treatment , after 2 cycles at time of partial response ( pr ) , and after 4 cycles at time of progressive disease ( pd )  . 
clinical assessment and circulating tumor dna ( ctdna ) monitoring for patient 2 ( b5 - 001 ) identify on - target high - level met amplication ( amp ) as mechanism of resistance to savolitinib . 
 ( a ) radiologic assessment of tumor at baseline before savolitinib treatment ( follow - up [ fu ] 1 ) ; after 2 cycles ( fu2 ) and 4 cycles ( fu3 ) , both at time of partial response ( pr ) ; and after 7 cycles at time of progressive disease ( pd )  . 
 ( b ) copy number prole of ctdna plasma ( top ) and tumor tissue or normal dna at progression ( bottom ) , where each sample is represented by a different color at baseline ( fu1 ) , after 2 cycles ( fu2 ) and 4 cycles ( fu3 ) , and after 7 cycles at time of progression . patient was administered postoperative chemoradiation therapy with a ts - 1 plus oxaliplatin regimen and developed recurrent metastases to both ovaries 18 months later . 
 ( a ) hematoxylin and eosin ( he ) , met immunohistochemistry ( ihc ) , and met uorescence in situ hybridization ( fish ; left to right ) from baseline tumor tissue . 
 ( b ) tumor assessment by radiologic assessment at baseline before savolitinib treatment , after 2 cycles at time of partial response ( pr ) , and after 8 cycles at time of progressive disease ( pd )  . 
 frigault et al discussion the aim of this exploratory study was to determine whether relapses on savolitinib in patients with gastric cancer after an initial pr resulted from the development of on - target or bypass mechanisms of resistance . 
furthermore , we established the utility of ctdna from plasma as a matrix for monitoring changes in dna alterations during the course of treatment of gastric cancer and demonstrated the concordance of genomic alterations in ctdna to tumor biopsy both before treatment with a targeted therapy and at the time of progression . 
the efcacy of the trial will be reported once the trial completes recruitment ; here , we focused on the utility of ctdna sequencing to identify potential resistance mechanisms in gastric cancer after met inhibition . 
we identied the following two potential mechanisms of acquired resistance at progression following a dramatic response to savolitinib in met - amplied gastric cancer : newly developed met mutations previously only described in lung cancer and an increase in the met copy number at resistance , which decreased during the clinical response but increased again at disease progression . in the rst patient , newly emerging met d1228h ( 31% ) , met d1228n ( 12% ) , met d1228v ( 1% ) , and met y1230c ( 1% ) mutations were detected with the sudden onset of disease progression to multiple bones and the bone marrow . 
this patient died of rapid progression immediately after developing resistance to savolitinib therapy . mutations in met , including at positions d1228 and y1230 , are among the reported mechanisms of acquired resistance in preclinical models21 , 22 and have been reported to confer clinical resistance to met inhibition in lung cancer.17 , 19 the cocrystal structure of the met kinase domain and met kinase inhibitor revealed an important binding interaction of the met inhibitor and y1230 and explains the abrogation of compound binding with the emergence of mutations at this residue . 
in addition , d1228 is engaged in interactions with other residues to maintain the activation loop in a conformation that enables the critical interaction between y1230 and the met inhibitor.21 these results demonstrate that the on - target resistance mutations emerge in met - amplied gastric cancer treated with a selective met kinase inhibitor . 
therefore , upregulation of met ( in a savolitinib - responsive tumor ) similar to her2 ( in a lapatinib - responsive tumor ) may confer resistance via epithelial to mesenchymal transition and by promoting a metastatic phenotype.26 , 27 an on - target met copy number gain as a mechanism of resistance has been reported in lung cancer , where one met exon 14skipping patient became a responder to a met inhibitor in the clinic ; however , at the time of progression , the exon 14 met allele was amplied , but not the wild - type allele of met , 28 suggesting that highlevel amplication of the met gene is a mechanism of resistance to met inhibitors across indications . in 2 of 3 patients studied , ctdna was detectable in the circulation , harboring somatic alterations in the met pathway that changed over time and were conrmed by rebiopsy at recurrence . 
our data agree with this hypothesis ; in the rst patient , tp53 p190l changed from a fraction of 44% at baseline to 7% during pr and then back to 13% at disease progression , which was further conrmed in tumor tissue with a 17% allele fraction harboring the same mutation in tp53 . 
 met inhibitor in met - amplied gastric cancer contained no detectable ctdna tp53 until after 4 cycles , at which point a g245d amino acid substitution was detectable at a 2% allele fraction and increased to 22% at progression . 
the same alteration was identied by rebiopsy at an 82% allele fraction . in 1 of 3 patients studied , no mutations in any of the 100 genes on the high - coverage deep - sequencing gene panel were detected , and therefore , this patients tumors may not be shedding ctdna into circulation . 
this patient demonstrates the limitations of the use of ctdna to the 57% - 87% of patients with gastric cancer who are shedding ctdna from their tumor into circulation.30 , 31 this patient highlights that tumor collection at the time of progression will still be important for identifying resistance mechanisms to targeted treatments in nonshedders and to understand tumor heterogeneity . in summary , ctdna is a powerful tool for identifying potential genomic aberrations that emerge during therapy to confer resistance to targeted therapies . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . aleksandra markovets employment : astrazeneca stock and other ownership interests : astrazeneca barrett nuttall employment : astrazeneca , cvs health ( i ) stock and other ownership interests : astrazeneca , cvs health ( i ) travel , accommodations , expenses : astrazeneca , cvs health ( i ) se hoon park honoraria : merck sharp & dohme , sano - aventis consulting or advisory role : eli lilly , janssen oncology research funding : kura oncology , ono pharmaceutical esha a . 
gangolli employment : clovis oncology stock and other ownership interests : astrazeneca , clovis oncology , novartis , merck , bristol - myers squibb , jounce therapeutics , unum therapeutics , incyte , alcon , guardant health , titan medical travel , accommodations , expenses : clovis oncology peter g.s. 
nat rev dis primers 3 : 17036 , 2017 fuchs c , doi t , jang r , et al : keynote - 059 cohort 1 : efcacy and safety of pembrolizumab ( pembro ) monotherapy in patients with previously treated advanced gastric cancer . 
n engl j med 372 : 2509 - 2520 , 2015 lee j , ou sh , lee jm , et al : gastrointestinal malignancies harbor actionable met exon 14 deletions . 
mod pathol 26 : 1632 - 1641 , 2013 lee j , kim km , kang wk , et al : innovative personalized medicine in gastric cancer : time to move forward . 
nature 513 : 202 - 209 , 2014 lee j , seo jw , jun hj , et al : impact of met amplication on gastric cancer : possible roles as a novel prognostic marker and a potential therapeutic target . 
oncol rep 25 : 1517 - 1524 , 2011 ahn s , brant r , sharpe a , et al : correlation between mek signature and ras gene alteration in advanced gastric cancer . 
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kim st , banks kc , pectasides e , et al : impact of genomic alterations on lapatinib treatment outcome and cell - free genomic landscape during her2 therapy in her2 + gastric cancer patients . 
tiedt r , degenkolbe e , furet p , et al : a drug resistance screen using a selective met inhibitor reveals a spectrum of mutations that partially overlap with activating mutations found in cancer patients . 
kim dc , park kr , jeong yj , et al : resistance to the c - met inhibitor krc - 108 induces the epithelial transition of gastric cancer cells . 
oliveras - ferraros c , corominas - faja b , cuf s , et al : epithelial - to - mesenchymal transition ( emt ) confers primary resistance to trastuzumab ( herceptin )  . 
shi j , li f , yao x , et al : the her4 - yap1 axis promotes trastuzumab resistance in her2 - positive gastric cancer by inducing epithelial and mesenchymal transition . 
awad mm , bahcall m , sholl lm , et al : mechanisms of acquired resistance to met tyrosine kinase inhibitors ( tkis ) in met exon 14 ( metex14 ) mutant non - small cell lung cancer ( nsclc )  . 
 ( b ) sequencing and mapping statistics of tissue samples and ( c ) plasma circulating tumor dna ( ctdna ) describing number of sequenced reads , percentage of aligned reads , percentage of duplicated reads , percentage of reads mapped on targets ( + 200 base pairs ) , percentage of usable reads , average depth of coverage , gc content ( percentage of nitrogenous bases that are either guanine or cytosine ) , average insert size , and percentage of targeted bases with given coverage . 
sartori et al we thank sartori et al1 for their interest in the recently published review , which characterizes the her2 aberrations observed in nonsmall - cell lung cancer ( nsclc ) and summarizes the efcacy of her2targeted therapies in patients with nsclc.2 nsclc with her2 alterations is a highly heterogeneous disease . 
her2 overexpression , her2 amplication , and her2 mutation could exist alone or synchronously . sartori et al1 highlighted the contribution of immunologic features to the response to her2 - targeted therapy . 
as per the authors exploration , a strong antibody - dependent cell - mediated cytotoxicity triggered by the valine / valine ( v / v ) variant of fcriiia rather than sole target inhibition is the possible reason . the back - line application of singleunfortunately , agent immunotherapy to case 1 eventually led to hyperprogression disease ( hpd )  . 
indeed , the denition of hpd remains controversial to date , let alone the solid association between driver gene mutation and hpd.5 recently , our group also reported a patient with erbb1 exon 20 insertion mutation who suffered from hpd after nivolumab monotherapy.6 we speculated that one of the reasonable causes might be myc amplication , whose upregulation could result in cd47 activation and programmed death ligand 1 overexpression , consequently contributing to tumor growth . to the efcacy of with respect immunotherapy in her2 - mutant nsclc , 4 retrospective studies reported the outcomes.7 - 10 a total of 92 patients were treated with single - agent pd - 1 or pd - l1 inhibitor , most of them having experienced disease progression on standard chemotherapy . 
here , we call for in - depth studies of hpd mechanisms , especially the development of screening methods to identify specic subgroups in whom immune treatment would be harmful . up to now , her2 mutation , especially exon 20 insertion , is a potential therapeutic target with accumulated evidence . 
recent preclinical research reported that poziotinib potentiated the antitumor effect of trastuzumab emtansine ( t - dm1 ) by upregulating her2 expression.11 this mechanism ts the logic and the observed encouraging clinical benet from t - dm1 after disease progression on poziotinib in case 2 . 
in addition , a preclinical study conducted by li et al12 found that cotreatment of t - dm1 with irreversible pan - her inhibitors neratinib or lapatinib enhanced her2 receptor ubiquitination and consequently improved t - dm1 internalization and efcacy . 
whether the optimal combination mode is sequential or synchronous warrants further validation . trastuzumab deruxtecan ( t - dxd ) , another antibody - drug conjugate ( adc ) , harbors a different cytotoxic payload , showed better and more durable responses in her2mutant nsclc , and may be still effective after resistance to t - dm1.12 in extension , on top of her2 mutation , her2 amplication may also confer sensitivity to t - dm1 . 
according to recently released clinical trial data , t - dm1 exhibited identical orr in patients with nsclc with her2 amplication , her2 mutation , or concurrent her2 mutation and amplication ( 55% v 50% v 50% ) .12 collectively , her2 alterations in nsclc are rather heterogeneous . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . no potential conicts of interest were reported . references zhao j , xia y : targeting her2 alterations in non - small - cell lung cancer : a comprehensive review . 
precision oncol 4 : 411 - 425 , 2020 krug lm , miller va , patel j , et al : randomized phase ii study of weekly docetaxel plus trastuzumab versus weekly paclitaxel plus trastuzumab in patients with previously untreated advanced nonsmall cell lung carcinoma . cancer 104 : 2149 - 2155 , 2005 xu x , de angelis c , burke ka , et al : her2 reactivation through acquisition of the her2 l755s mutation as a mechanism of acquired resistance to her2 - targeted therapy in her2 + breast cancer . 
clin cancer res 23 : 5123 - 5134 , 2017 jin r , zhao j , xia l , et al : application of immune checkpoint inhibitors in egfr - mutant non - small - cell lung cancer : from bed to bench . 
huang x , xia l , lan f , et al : treatment of nivolumab results in hyperprogressive disease in a patient harboring egfr exon 20 insertion and myc amplication . 
mazieres j , drilon a , lusque a , et al : immune checkpoint inhibitors for patients with advanced lung cancer and oncogenic driver alterations : results from the immunotarget registry . 
ann oncol 30 : 1321 - 1328 , 2019 lai w - cv , feldman dl , buonocore dj , et al : pd - l1 expression , tumor mutation burden and response to immune checkpoint blockade in patients with her2 - mutant lung cancers . 
j clin oncol 36 , 2018 ( suppl 15 ; abstr 9060 ) dudnik e , bshara e , grubstein a , et al : rare targetable drivers ( rtds ) in non - small cell lung cancer ( nsclc ) : outcomes with immune check - point inhibitors ( icpi )  . 
guisier f , dubos - arvis c , vias f , et al : efcacy and safety of anti - pd - 1 immunotherapy in patients with advanced nsclc with braf , her2 , or met mutations or ret translocation : gfpc 01 - 2018 . 
robichaux jp , elamin yy , vijayan rsk , et al : pan - cancer landscape and analysis of erbb2 mutations identies poziotinib as a clinically active inhibitor and enhancer of t - dm1 activity . 
cancer discov 10 : 674 - 687 , 2020 sartori g , belluomini l , trovato r , et al : her2 aberrations in nsclc : so close yet so far . 
 contributed equally to this work . ( continued ) purpose alk ( anaplastic lymphoma kinase ) rearrangements predict for sensitivity to alk tyrosine kinase inhibitors ( tkis ) ; however , responses to alk tkis are generally short lived . 
although multiple studies support the clinical benefits of repeat tissue sampling , the clinical utility of longitudinal circulating tumor dna analysis has not been established in alk - positive lung cancer . patients and methods we used a 566 - gene hybrid - capture next - generation sequencing assay to perform a longitudinal analysis of plasma specimens from 22 alk - positive patients with acquired resistance to alk tkis to track the evolution of resistance during treatment . 
to determine tissueplasma concordance , we compared plasma findings with the results of repeat biopsies . results at disease progression , we detected an alk fusion in plasma from 19 ( 86% ) of 22 patients and identified alk resistance mutations in plasma specimens from 11 patients ( 50% )  . 
alk g1202rthe most frequent plasma mutation detected after progression on a second - generation tkiwas consistently suppressed during treatment with lorlatinib . conclusion plasma genotyping by next - generation sequencing is an effective method for detecting alk fusions and alk mutations in patients who experience disease progression on alk tkis . 
2018 by american society of clinical oncology introduction oncogenic rearrangements that result in the constitutive activation of anaplastic lymphoma kinase ( alk ) define a molecular subtype of nonsmalllung cancer ( nsclc ) that is characterized by sensitivity to alk tyrosine kinase inhibitors ( tkis ) .1 , 2 since the identification of alk rearrangements in nsclc in 2007 , four tkis have become standard therapies for patients with advanced disease.3 - 6 although these tkis have significantly improved clinical outcomes , most patients experience relapse within 1 to 2 years.1 despite a shared molecular driver , the magnitude of benefit from tki treatment varies widely between patients . 
repeat biopsies upon disease progression have been instrumental in elucidating the molecular mechanisms that drive resistance to alk inhibitors , including the distinct spectrum of alk mutations associated with resistance to each tki7 ; however , repeat biopsies may be challenging to obtain and single - site sampling may not capture the spatial heterogeneity of resistance mechanisms . analysis of circulating tumor dna ( ctdna ) is an emerging approach for tumor genotyping . 
shaw , md , phd , department of medicine , massachusetts general hospital , 32 fruit st , boston , ma 02114 ; e - mail : ashaw1@ partners.org. as plasma sampling is minimally invasive and ctdna may be derived from all metastatic sites , longitudinal monitoring of genetic alterations in ctdna may overcome many of the limitations of tissue sampling . 
 libraries were constructed with illumina truseq nano dna library prep kit ( illumina , san diego , ca ) , enriched for a 566 - gene pancancer gene panel ( data supplement ) by using agilent sureselect xt custom baits ( agilent technologies , santa clara , ca ) , and sequenced on an illumina hisequation 2500 sequencer to a median of 105 million reads , which yielded a median coverage of 1 , 195.18 sequence data were aligned to the hg19 reference genome . 
those with at least four alternate reads were retained on the basis of a calculated background mutation rate and false - positive rate of 1e - 4 and 1e - 6 , respectively . 
ctdna insufficient for analysis indicates those samples that were technically successful , but had insufficient tumor dna present in the plasma to reliably estimate underlying tumor genotype . longitudinal ctdna analysis ( n = 79 ) disease progression on study ( n = 29 ) ctdna analysis successful ( n = 22 ) ctdna insufficient for analysis ( n = 7 ) 23 repeat biopsies attempted for 20 patients * repeat biopsy not attempted ( n = 2 ) tissue insufficient ( n = 7 ) tissue sufficient ( n = 16 ) inaccessible site ( n = 1 ) patient preference ( n = 1 ) * three patients underwent tissue sampling twice during plasma surveillance patients with cns - only progression patients with isolated intrathoracic disease progression patients with isolated progression of a liver lesion ( n = 1 ) ( n = 5 ) ( n = 1 ) three of six attempted repeat biopsies sufficient for analysis results patient characteristics that were administered is depicted in the data supplement and figure 2 . plasma was longitudinally collected from 79 patients with metastatic , alk - positive nsclc ( fig 1 )  . 
as this study was primarily focused on investigating the role of ctdna analysis at disease progression , this report is limited to patients who had progressive disease and analyzable plasma specimens . 
of the seven patients who did not have detectable ctdna , one patient experienced cns - only progression , five patients had intrathoracic progression , and one patient had liver oligoprogression ( fig 1 )  . 
baseline characteristics of the 22 patients and their treatment histories are summarized in table 1 , figure 2 , and the data supplement . plasma genotyping was performed on 88 plasma samples from 22 patients . 
the temporal relationship between plasma collection and the treatments concordance between tissue and plasma genotypes we first evaluated concordance between tissue and plasma genotyping for alk fusions , alk mutations , and non - alk alterations . 
 ( % ) of alk tkis before initial plasma collection * abbreviation : alk , anaplastic lymphoma kinase ; tki , tyrosine kinase inhibitor . * the total number of alk tkis on which a patient had experienced progression before the collection of the initial plasma specimen . 
in instances where plasma was collected during sequential treatment with distinct alk inhibitors , the line of therapy at initial plasma collection is represented . ( 94% ; appendix fig a1 )  . 
among the 12 patients for whom the fusion partner was known and an alk fusion was detected in the plasma , there was 100% agreement between tissue and plasma fusion calls ( fig 3a )  . 
point mutations in the alk kinase domain were identified in plasma specimens from 11 patients ( 50% ) , five of whom had paired biopsies at the time of mutation detection ( fig 3b )  . 
three patients had multiple alk mutations . all tissue - detected alk mutations were also identified in corresponding plasma samples , and all plasma - detected alk mutations were also present in paired biopsies . 
 among 17 patients who had plasma collected during progression on a second - generation alk inhibitorthat is , ceritinib , alectinib , or brigatinibplasma alk mutations were identified in eight patients ( 47% ; data supplement ) , including i1171n ( n = 1 ) , g1202r ( n = 5 ) , i1171n / g1202r ( n = 1 ) , and e1210k ( n = 1 )  . 
 the observed frequency of plasma alk mutations is consistent with our previous analysis of resistance biopsies from patients who developed resistance to second - generation inhibitors , which included five patients from the current plasma cohort.7 non - alk alterations . 
as we did not detect any differences in tissue alterations that were identified in serial specimens from the three patients who underwent multiple biopsies , we restricted the concordance assessment to one biopsy per individual . 
although we were not able to obtain tissue after the patient had developed progression on lorlatinib , amplification was not present when a prelorlatinib liver biopsy was assessed using the same 566gene panel . 
despite high - level met amplification ( > 25 copies ) in tissue , we did not detect met amplification in the corresponding plasma specimen ; however , as the maximum allelic frequency ( af ) of detected alterations in the plasma of mgh939 was approximately 2% , the degree of amplification was below the limit of detection of the assay . evolution of resistance during molecular surveillance alk fusion kinetics and correlation with disease status . 
preclinical models and case reports suggest that the presence of a specific alk mutation in a tki - resistant tissue specimen may predict response to subsequent alk tkis1 , 7 , 23 ; therefore , we analyzed plasma specimens from patients with alk mutations who received treatment with additional alk tkis to evaluate the potential of using plasma findings to inform sequential therapies . 
during the follow - up period , seven of these patients ( 88% ) went on to receive treatment with a tki that targeted the alk mutation ( data supplement )  . 
 detected in plasma only detected in plasma and tissue mutation no paired biopsy paired biopsy available detected in plasma only detected in plasma and tissue eml4 - alk variant 1 variant 2 variant 3 variant 5 i1171n f1174c f1174l g1202r d1203n e1210k fig 3 . 
parentheses denote patients for whom the alk mutation was considered the dominant resistance mechanisfor patients without paired biopsies , alk mutations that were detected at the time of progression on an alk tyrosine kinase inhibitor are listed . 
because the mutations were separated by too many bases , the allelic relationship ( cis v trans ) could not be determined for mgh990s alk mutation . in alk i1171n af from 4.5% to undetectable after 6 weeks ( fig 4a )  . 
one patient ( mgh989 ) underwent microwave ablation to treat a liver lesion with a biopsy - proven g1202r mutation and continued treatment with alectinib for an additional 6 months . 
 mgh990 had a radiographic response to treatment , but we could not evaluate the molecular response as we were only able to collect a single plasma specimen . although the g1202r mutation was suppressed in plasma during the treatment with lorlatinib , two of the four patients with plasma - detected g1202r developed progressive disease soon after initiating lorlatinib ( appendix fig a3 )  . 
we were not able to obtain a biopsy , but plasma analysis demonstrated an increase in copy number of gnas and bcl2l1 and a marked increase in the af of mutations that involved other genes during treatment ( fig 5 )  . 
in both cases , eml4 - alk fusion af increased at progression despite the suppression of alk mutations , which supports the notion that resistance was independent of genetic alk alterations . discussion despite a shared molecular driver , the clinical course is variable for patients with alk - positive nsclc treated with alk tkis . 
our findings highlight the potential clinical utility of hybrid - capture ngs for improving our understanding of the molecular drivers of resistance . in our cohort of patients , 76% of plasma samples contained sufficient tumor - derived dna for molecular analysis compared with 65% of biopsy specimens , which confirms that both are reliable approaches . 
 furthermore , our observation that the presence of specific plasma alk mutations correlated with the response and resistance to distinct alk tkis lends support to the emerging practice of using alk mutations to inform the selection of alk tkis . although tissue sampling is the gold standard for molecular analysis , sampling a single site of disease may overestimate the contribution of a particular alteration to the resistant phenotype . 
for example , we detected an alk g1202r mutation at 50% af in a progressing liver lesion , which suggested that it was a major contributor to alectinib resistance in the case of mgh919 . 
in contrast , the plasma g1202r af of 1% was less than the af of other plasma - detected molecular alterations , including multiple non - alk alterations ( fig 5 )  . 
moreover , this case reinforces the notion that the analysis of liquid biopsies may be more informative than tissue - based genotyping in certain situations . to date , the study of resistance to alk therapeutics has primarily focused on alk mutations . 
figure illustrates the change in the allelic fraction of eml4alk and alk mutations during sequential treatment with next - generation alk inhibitors for ( a ) mgh987 and ( b ) mgh087 . 
 ( a ) allelic fraction of alk ( anaplastic lymphoma kinase ) fusion ( blue ) , alk mutations ( red and gold ) , and non - alk alterations ( gray ) during treatment with sequential alk inhibitors . 
despite these shortcomings , our data suggest that the quantitative assessment of structural variants may be clinically useful and complementary to radiographic assessment in some patients . overall , our data confirm that plasma genotyping by using hybrid - capture ngs technology can reliably detect alk fusions and alk resistance mutations in patients with alk - positive nsclc ; however , there are several limitations of this study , including the small size of our cohort , inconsistent sampling intervals that led to variation in the duration of follow - up after and before disease progression , and the inability to obtain pretreatment plasma and paired biopsies for all patients . 
furthermore , as a result of the small contribution of tumor dna to total cellfree dna in most patients , we cannot definitively exclude the presence of undetected amplification events at resistance . 
as identifying alk resistance mutations is emerging as an important consideration for the management of alk - positive nsclc , we anticipate that genotyping plasma to characterize resistance to alk tkis will also become a routine part of patient care . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ibiayi dagogo - jack consulting or advisory role : boehringer ingelheim honoraria : foundation medicine a . 
campbell employment : novartis , pfizer ( i ) manuscript writing : all authors stock and other ownership interests : novartis final approval of manuscript : all authors accountable for all aspects of the work : all authors jessica j . 
schultz no relationship to disclose jennifer ackil no relationship to disclose sara stevens no relationship to disclose leila dardaei no relationship to disclose satoshi yoda no relationship to disclose harper hubbeling no relationship to disclose subba r . 
sequist honoraria : astrazeneca consulting or advisory role : astrazeneca , genentech , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack pharmaceuticals ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , merck ( inst ) , pfizer ( inst ) inga t . 
lennes honoraria : blue cross and blue shield of massachusetts consulting or advisory role : kyruus anthony john iafrate stock and other ownership interests : archer biosciences consulting or advisory role : debiopharm group , constellation pharmaceuticals , chugai pharma , roche research funding : blueprint medicines patents , royalties , other intellectual property : archerdx exclusive license to amp technology rebecca s . 
heist consulting or advisory role : boehringer ingelheim research funding : glaxosmithkline , sanofi , abbvie , novartis , roche , incyte , celgene , mirati therapeutics , peregrine pharmaceuticals , exelixis , millennium pharmaceuticals , debiopharm group christopher g . 
azzoli consulting or advisory role : merck , ariad pharmaceuticals , takeda research funding : pharmamar ( inst ) , abbvie ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , loxo ( inst ) , ignyta ( inst ) travel , accommodations , expenses : pharmamar , abbvie , stemcentrx jeffrey a . 
engelman employment : novartis stock and other ownership interests : loxo , agios , kura , gatekeeper pharmaceuticals , novartis consulting or advisory role : novartis , agios , loxo , clovis oncology , ventana medical systems , g1 therapeutics , sanofi , chugai pharma , warp drive bio , asana biosciences , emd serono , synta , allostery , genentech , aveo , biodesix , merck , cell signaling technology , endo pharmaceuticals , astrazeneca , glaxosmithkline , amgen , bristol - myers squibb , cancer progress research funding : novartis , jounce therapeutics , sanofi , araxes , astrazeneca , amgen ( inst ) patents , royalties , other intellectual property : coinventor on a patent application that has been licensed to ventana medical system / roche other relationship : third rock ventures jochen k . 
leary employment : novartis stock and other ownership interests : novartis patents , royalties , other intellectual property : patents , pending patents , and a royalty - sharing agreement with johns hopkins university alice t . 
shaw honoraria : pfizer , novartis , genentech , foundation medicine consulting or advisory role : pfizer , novartis , genentech , roche , ariad pharmaceuticals , ignyta , blueprint medicines , daiichi sankyo , emd serono , taiho pharmaceutical , ksq therapeutics research funding : pfizer , novartis , genentech justin f . 
gainor honoraria : merck , incyte , ariad pharmaceuticals consulting or advisory role : novartis , boehringer ingelheim , clovis oncology , genentech , bristol - myers squibb , theravance , loxo research funding : merck , novartis , genentech , bristolmyers squibb , adaptimmune , astrazeneca , ariad pharmaceuticals travel , accommodations , expenses : affymetrix anna f . 
farago honoraria : foundation medicine consulting or advisory role : pharmamar , merrimack pharmaceuticals , takeda , abbvie , intervention insights acknowledgment we also thank jeremy decker for assistance with plasma preparation and circulating tumor dna processing . 
shaw at , yeap by , mino - kenudson m , et al : clinical features and outcome of patients with nonsmall - cell lung cancer who harbor eml4 - alk . 
kim dw , mehra r , tan ds , et al : activity and safety of ceritinib in patients with alk - rearranged nonsmall - cell lung cancer ( ascend - 1 ) : updated results from the multicentre , open - label , phase 1 trial . 
shaw at , gandhi l , gadgeel s , et al : alectinib in alk - positive , crizotinib - resistant , nonsmallcell lung cancer : a single - group , multicentre , phase 2 trial . 
kim dw , tiseo m , ahn mj , et al : brigatinib in patients with crizotinib - refractory anaplastic lymphoma kinase - positive nonsmall - cell lung cancer : a randomized , multicenter phase ii trial . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
paweletz cp , sacher ag , raymond ck , et al : bias - corrected targeted next - generation sequencing for rapid , multiplexed detection of actionable alterations in cell - free dna from advanced lung cancer patients . 
schwaederl mc , patel sp , husain h , et al : utility of genomic assessment of blood - derived circulating tumor dna ( ctdna ) in patients with advanced lung adenocarcinoma . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
curigliano g , gmez pardo p , meric - bernstam f , et al : ribociclib plus letrozole in early breast cancer : a presurgical , window - of - opportunity study . 
ye k , schulz mh , long q , et al : pindel : a pattern growth approach to detect break points of large deletions and medium sized insertions from paired - end short reads . 
solomon b , bauer tm , felip e , et al : safety and efficacy of lorlatinib ( pf - 06463922 ) from the dose - escalation component of a study in patients with advanced alk + or ros1 + non - small cell lung cancer ( nsclc )  . 
 in two of the three patients for whom plasma analysis failed to detect a fusion , an eml4 - alk fusion ( variants 3 and 5 ) was identified in matching tissue . 
kornaga , msc1 , 2 ; cheryl crozier , msc1 ; gun ho jang , phd1 ; lauren bathurst , msc1 , 3 ; irina kalatskaya , phd1 , 4 ; quang m . 
pathways were identied as aberrant if there were copy number aberrations and / or mutations in any of the predetermined pathway genes : ccnd1 / ccnd2 / ccnd3 / cdk4 / cdk6 , fgfr1 / fgfr2 / fgfr2 / fgfr4 , and akt1 / akt2 / pik3ca / pten . results the 390 of 420 samples that passed quality control were analyzed for distant metastasisfree survival between groups . 
these bcas represent the majority of new bca diagnoses ( 70% to 80% ) , and a recent meta - analysis of 62 , 923 women with estrogen receptor ( er ) positive bca , who were disease free after 5 years of endocrine therapy , reported that approximately one in three women will experience a relapse during the next 20 years.1 - 3 although the development of diagnostic tests have helped to inform patients with regard to residual relapse risk , 4 , 5 as well as the identication of those who do not benet from chemotherapy , 6 none have yet to provide insight for those high - risk patients who may benet from the precision medicine approaches offered in the metastatic setting . 
to fully maximize the benet of targeted therapies seen in unselected patients in the advance / metastatic setting , upfront stratication of patients at risk for recurrence to these targeted agents in the early setting would reduce unnecessary treatment and associated toxicities and form a rational basis for treatment selection . 
this retrospective study of 390 early breast cancers from a phase iii clinical trial demonstrates that genomic changes within key genes in the cyclin d / cyclin - dependent kinase , phosphatidylinositol 3 - kinase / protein kinase b , and broblast growth factor receptor pathways could identify patients who might benet most from treatment that targets those deregulated pathways . knowledge generated in this focused approach , aberrations among genes in these pathways were shown to affect risk of distant relapse . relevance the use of this stratication approach , which benets from the interrogation of a limited number of genes , could be implemented effectively by using existing genomic technologies in the clinical laboratory to aid clinicians in identifying patients for whom specic targeted treatments are needed in combination with standard endocrine therapy . and the cancer genome atlas , 13 , 14 translation of these ndings into novel approaches to the management of cancer is slow . in response , we generated data focused on specic signaling pathways derived from the international cancer genome consortium and the cancer genome atlas13 , 14 together with whole - genome copy number analyses . 
the analysis was performed on the basis of an a priori hypothesis related to molecular pathways for which there are existing targeted therapies currently under evaluation in late - stage clinical trials . 
in a case - control study , 420 patients from the tamoxifen versus exemestane adjuvant multinational ( team ) trial pathology cohort ( clinicaltrials . identiers : nct00279448 , nct00032136 , and nct00036270 ) 15 were selected to determine the prognostic ability of copy number events and specic mutational changes that represent the cyclin d / cyclin - dependent kinase ( ccnd / cdk ) , broblast growth factor receptor / broblast growth factor ( fgfr / fgf ) , and phosphatidylinositol 3 - kinase / protein kinase b ( pi3k / akt ) pathways to predict risk of recurrence after anti - endocrine therapy in the early setting . 
distant metastasisfree survival ( dmfs ) was dened as time from random assignment to distant relapse or death as a result of bca.15 this study complies with the declaration of helsinki , institutional ethics committees , and the international conference on harmonization and good clinical practice guidelines . 
patients provided informed consent , and this study was approved by the university of toronto research ethics board ( protocol number 35339 )  . targeted sequencing and copy number analysis forty nanograms of dna extracted from formalin - xed parafn - embedded tissues were processed for targeted sequencing ( appendix )  . 
only variants that were on target and passed ltering criteria were included in the downstream analysis as described by kalatskaya et al.19 for copy number aberration ( cna ) analyses , 200 ng of dna were processed using oncoscan ffpe express 2.0 snp arrays ( affymetrix , santa clara , ca )  . 
 prognostic signatures in early breast cancers highly variable log - r ratio ( lrr ) , unevenly distributed b - allele frequencies , and waviness in lrr were measured using penncnv.20 estimation of tumor ploidy and aberrant tumor fraction was performed , and copy number segments were used by combining segments generated by two algorithms : allele - specic copy number analysis of tumors version 2.121 and circular binary segmentation22 implemented in the dnacopy package of r . 
an algorithm described by boutros et al23 was used to recalibrate tumor ploidy , aberrant tumor fraction , and copy numbers on the basis of lrr and b - allele frequency data , and adjacent segments having the same copy numbers were merged . segment boundaries were adjusted to obtain smaller argument function values . 
analyses were performed using r version 3.1.0. statistical analysis of the 420 patients , 390 passed ltering criteria and were included in subsequent analyses using stata 12.1 software ( statacorp , college station , tx )  . 
genes that represented pathways of interest were identied as aberrant according to the following criteria : ccnd / cdk pathway ( gains / amplications in any of ccnd1 / ccnd2 / ccnd3 / cdk4 / cdk6 ) , fgfr pathway ( gains / amplications in any of fgfr1 / fgfr2 / fgfr3 / fgfr4 ) , and pi3k / atk pathway ( aberrations in any of the following : gain / amplication of akt1 or possession of a mutation in akt1 , gain / amplication of akt2 , gain / amplication of pik3ca , and pten mutation and accompanying pten loss akt1 / akt2 / pik3ca / pten )  . a second model for the pi3k / akt was analyzed where pik3ca mutation data were included alongside pik3ca cnas and alterations in the genes of the dened pathways . kaplan - meier method and log - rank analyses were used to assess differences in dmfs . 
hrs were calculated using cox proportional hazards regression models , and models were adjusted for age ( continuous variable ) , tumor size ( dichotomized at 2 cm ) , tumor grade ( 1 / 2 v 3 ) , lymph node status , and her2 status ( negative v positive )  . 
all p values reported were two - sided , and p , .05 was considered statistically signicant . results changes in copy number of genes associated with signaling pathways are independently linked to high risk or relapse after anti - endocrine therapy our a priori hypothesis identied candidate pathways and specic genomic changes linked to endocrine treatment failure and outcome , namely ccnd / cdk signaling , the pi3k / akt axis , and fgfr / fgf pathway . 
no statistically signicant differences in age , tumor size , grade , lymph node status , or her2 status between patients with a dmfs event and those without were noted ( table 1 )  . 
of the 272 patients , 172 had aberrations in the specied ccnd / cdk genes ( 147 with aberrations in the fgfr genes and 138 with aberrations in pi3k / akt genes )  . 
of the 390 patients , 54 ( 13.8% ) , 34 ( 8.7% ) , and 43 ( 11% ) possessed aberrations in only one pathway ( ccnd / cdk , pi3k / akt , and fgfr , respectively )  . slightly fewer patients possessed aberrations in two pathways : 37 ( 9.5% ) with aberrant ccnd / cdkand pi3k / aktrelated genes , 37 ( 9.5% ) with aberrant ccnd / cdkand fgfr - related genes , and 23 ( 5.9% ) with aberrant pi3k / aktand fgfr - related genes . 
correlation to grade according to the number of pathways showed that patients with lower - grade tumors ( grade 1 / 2 ) had fewer altered pathways than those with grade 3 tumors ( appendix table a2 )  . 
although widely viewed as a good - prognosis subtype , hormone receptorpositive bcas account more than 84% of newly diagnosed early bca and therefore comprise the majority of bca deaths . 
despite recent advances in adjuvant therapy , outcomes for high - risk hormone receptorpositive bca are suboptimal , with an estimated relapse rate of 25% at 5 years.1 , 2 , 28 patients who are disease free at 5 years after diagnosis can still experelapse 5 to 20 years rience a high risk of distant postdiagnosis , 1 , 28 which directly challenges the dogma that such cancers are low risk and responsive to treatment . we tested the hypothesis that aberrations in key signaling pathways , where targeted therapies exist for bca ( in the advanced or metastatic setting ) , are prognostic in the early bca setting . 
aberrations in key genes of the ccnd / cdk pathway were more frequently detected than those in the pi3k / akt or fgfr axes ; however , the majority of patients ( 52% ) had aberrations in more than one pathway , which offers a rationale for incomplete responses to monotargeted therapy . 
kaplan - meier survival curves for aberrant pathways ( a ) cyclin d / cyclin - dependent kinase ( ccnd / cdk ) , ( b ) broblast growth factor receptor ( fgfr ) , ( c ) phosphatidylinositol 3 - kinase / protein kinase b ( pi3k / akt ) in the absence of pik3ca mutation , and ( d ) pi3k / akt pathway with pik3ca mutations . 
patients who possessed ccnd / cdk alterations exhibited signicantly poorer outcomes ( fig 1a ) than patients with fgfr and pi3k / akt aberrations ( figs 1b and 1c , respectively )  . 
in combination , patients with ccnd / cdk and fgfr aberrations were also at higher risk for relapse ( figs 2 and 3 ) possibly because of the proximity of ccnd1 and ligands fgf2 and fgf3 on chromosome 11q and their frequent co - amplication.29 indeed , the outcome for patients with ccnd / cdk and fgfr aberrations was similar to patients with ccnd / cdk aberrations only ( fig 3b )  . 
when pik3ca mutations were included in the stratication , there was no difference in survival between the two groups , consistent with the nding that pik3ca mutations in early bca and in the context of endocrine therapy seems to have no impact on outcome.30 , 31 increasing numbers of aberrant pathways also were associated with higher grade ( appendix tables a1 and a2 ) , consistent with the role of grade as an important prognostic factor32 and its association with gene expression changes that drive proliferation.33 - 35 intrinsic , endocrine resistance , acquired or remains a therapeutic challenge . 
for example , we have shown that up to one in ve early bcas exhibit amplications of cdk2 / 4 / 6 and ccnds39 , 40 and that ccnd1 amplication , but not overexpression , is associated with increased risk of distant relapse in endocrine - treated early bca.40 similarly , the trial study design did not stratify patients upfront by biomarker . 
consistent with published work , our data support evidence for a key role of cnas in this gene pathway.52 , 53 toxicities associated with mtor inhibitors like everolimus remain a concern . 
kaplan - meier curves of distant metastasisfree survival ( dmfs ) according to ( a ) risk order ( no aberrant pathway , any cyclin d / cyclin - dependent kinase [ ccnd / cdk ] , phosphatidylinositol 3 - kinase / protein kinase b [ pi3k / akt ] and broblast growth factor receptor [ fgfr ] , and fgfr only )  . 
 ( b ) frequency of aberration ( no aberrant pathway ; any pi3k / akt , fgfr and ccnd / cdk ; and ccnd / cdk only )  . class of drug would greatly affect patient management . phase iii trials are now under way to evaluate pi3k / akt inhibitors , including pi3kselective inhibitors in combination with fulvestrant in the advanced / metastatic bca setting ( clinicaltrials.gov identiers : nct02437318 and nct02340221 )  . 
phase ii neoadjuvant trials also are being conducted in the early bca setting ( clinicaltrials.gov identiers : nct01923168 and nct02273973 ) , which requires tumor pik3ca mutation status before determination of treatment randomization . 
however , we and others have shown that in early hormone receptorpositive bca , pik3ca mutations represent one of the most frequent mutations ( 35% ) 31 , 54 , 55 but show limited evidence that these mutations are linked to endocrine resistance in the early setting . the fgfr family of genes are recognized to be amplied in 10% to 15% of bcas.56 , 57 although fgfr1 is most frequently amplied , there is evidence for lower frequency amplication of fgfr2 , fgfr3 , and fgfr458 - 60 in early bca . 
evidence has emerged that links fgfrs to endocrine resistance.58 , 60 - 62 in preclinical studies , fgfr1 amplication enhanced pi3k and mitogen - activated protein kinase pathway signaling , which leads to endocrine resistance and could be reversed using rna interference against fgfr1.57 between 30% and 40% of cancers with ccnd1 amplication exhibit fgfr1 co - amplication despite the fact that these genes are mapped within different amplication loci on chromosomes 11 and 8.63 a challenge in targeting both ccnd1 and fgf pathwayamplied tumors is the proximity of the ligands fgf3 and fgf4 to ccnd1 on chromosome 11q13 . 
the role of fgfr signaling in a number of cancer settings suggests that it is a potential driver of cancer progression.58 , 64 , 65 several fgfr - targeted inhibitors are under investigation in phase ii clinical trials , including fgfr1 to 4 selective inhibitors bgj398 identiers : nct01004224 and ( clinicaltrials.gov nct02160041 ) and azd4547 ( clinicaltrials.gov identiers : nct01791985 , nct01795768 , and nct01202591 )  . 
to date , all trials that involve fgfr - targeted inhibitors are for patients with advanced or metastatic disease , with almost all trials requiring molecular prescreening for only fgfr1 or 11q amplication before study entry . issues of early hormone receptorpositive bca critical management must be addressed , 66 - 70 including molecular heterogeneity7 , 8 , 71 and emergent drug resistance.72 , 73 clinically , patients with such features would benet from early treatment with combinatorial therapies . 
in a drug screen of 42 agents , ribociclib was identied as a strong sensitizer to pi3k inhibition in three er - positive bca cell lines with acquired resistance to pi3k inhibitors.74 targeted doublet combinations of cdk4 / 6 or pi3k / mtor inhibitors with endocrine therapy have improved progression - free survival compared with endocrine therapy alone , 37 , 75 , 76 whereas another study showed that palbociclib plus pictilisib and fulvestrant was more effective than doublet combinations.77 we show that early hormone receptorpositive bcas could be stratied using genomic markers representative of pathways linked to targeted therapeutics that predict risk of recurrence after endocrine treatment . 
bartlett provision of study material or patients : daniel rea collection and assembly of data : jane bayani , cheryl crozier , paul c . boutros , melanie spears , john d . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . jane bayani patents , royalties , other intellectual property : 95 gene signature of residual risk in endocrine - treated early breast cancer ( provisional us patent 62 / 263 , 805 ) daniel rea honoraria : roche , novartis , pzer , eli lilly consulting or advisory role : genomic health research funding : celgene ( inst ) , roche ( inst ) , biotheranostics ( inst ) travel , accommodations , expenses : pzer , daiichi sankyo john m.s. 
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heiskanen m , kononen j , b arlund m , et al : cgh , cdna and tissue microarray analyses implicate fgfr2 amplication in a small subset of breast tumors . 
taylor - harding b , aspuria pj , agadjanian h , et al : cyclin e1 and rtk / ras signaling drive cdk inhibitor resistance via activation of e2f and ets . 
sledge gw jr , toi m , neven p , et al : monarch 2 : abemaciclib in combination with fulvestrant in women with hr + / her2advanced breast cancer who had progressed while receiving endocrine therapy . 
 prognostic signatures in early breast cancers appendix targeted sequencing submission of 101 selected genes resulted in 6 , 318 amplicons , with a median size of 109 base pairs ( bp ; range , 64 to 142 bp ) that covered 612.79 kbp ( unpublished data )  . 
using ampliseq polymerase chain reaction primer panels ( thermo fisher scientic , waltham , ma ) for the gene set developed above , we adapted our current protocol for illumina ( san diego , ca ) sequencing . 
after amplication of dna regions in four separate pools of the total 6 , 318 amplicons ( pool 1 , 1 , 587 amplicons ; pool 2 , 1 , 580 amplicons ; pool 3 , 1 , 578 amplicons ; pool 4 , 1 , 573 amplicons ; 10 ng / pool , 40 ng total dna ) , library polymerase chain reaction products were combined ( per sample ) , barcoded , and pooled in sets of 96 samples . 
t raw reads ( 101 - bp paired - end ) were aligned against the university of california , santa cruz , human reference sequence hg19 ( including random and unknown sequences ) using novoalign version 2.07.14 ( novocraft technologies , selangor , malaysia )  . 
aligned reads were ltered with samtools version 0.1.1816 to remove unmapped reads , nonprimary aligned reads , and reads aligned with mapping quality less than 30 ( ie , nonunique alignments )  . 
because the tamoxifen versus exemestane adjuvant multinational trial ( clinicaltrial . gov identiers : nct00279448 and nct00032136 , and nct00036270 ) cohort did not have matching normal tissue , the conventional mutation calling pipelines were not applicable . 
 c vemurafenib in patients with relapsed refractory multiple myeloma harboring brafv600 mutations : a cohort of the histology - independent ve - basket study noopur raje ian chau david m . 
yee martin kaiser heather landau jean - marie michot antoine hollebecque luisa veronese martina makrutzki bethany pitcher igor puzanov jose baselga author affiliations and support information ( if applicable ) appear at the end of this article . clinical trial information : nct01524978 . corresponding author : noopur raje , md , professional office building 216 , harvard medical school , 55 fruit st , boston , ma 02114 ; e - mail : nraje@mgh.harvard.edu. introduction multiple myeloma ( mm ) is a genetically heterogeneous , complex disease that arises as a result of a variety of mutations in pathways deregulating the intrinsic biology of the plasma cell.1 although immunomodulatory drugs and proteasome inhibitors have improved outcomes in patients with mm , 2 , 3 patients with relapsed or refractory disease have a poor prognosis.4 despite the identification of many of the genetic events involved in the development of mm , no treatments specifically targeting genetic mutations have been developed to date . 
additional study design details are described in the data supplement . patients patients in the mm cohort had to have previously treated , measurable , relapsed or refractory mm with confirmed brafv600 mutation . 
the presence of brafv600 mutations was confirmed retrospectively in a central laboratory using the roche companion diagnostic cobas 4800 braf v600 test or other standard methodology . assessments the following assessments for mm were performed 8 weeks after the start of therapy and every 4 weeks thereafter : serum protein electrophoresis with quantitation of monoclonal protein level ; urine protein electrophoresis using 24 - hour urine protein electrophoresis ; and serum levels of free light chains , lactate dehydrogenase , and - 2 microglobulbone marrow analysis was performed only to confirm complete response ( cr ) after two consecutive immunofixation analyses were negative . efficacy was evaluated using international myeloma working group uniform response criteria.17 , 18 evaluations were performed at baseline , 8 weeks after the start of vemurafenib administration , every 4 weeks thereafter during treatment , and at the end of treatment . 
responses were classed as cr , stringent cr , very good partial response ( vgpr ) , partial response ( pr ) , stable disease ( sd ) , progressive disease , and clinical relapse . 
responders were defined as those patients with pr or better ( ie , cr , stringent cr , pr , or vgpr )  . statistical analysis the primary efficacy end point of ve - basket was the response rate at week 8 . 
for the purposes of this analysis , two response assessments were required with no specified time between these assessments , although the protocol required that these two assessments be 4 weeks apart . an adaptive simon two - stage design was used to minimize the number of patients treated if vemurafenib was deemed ineffective for a specific tumor type . 
assuming response rates as specified in the hypothesis testing , a power of 80% for a high desirable response and 70% for a low desirable response , and a two - sided of 0.1 , the number of patients required in each cohort was seven for stage 1 , and 13 or 19 for stage 2 , depending on the results in stage 1 . 
however , if a clear clinical benefit was observed for patients in a cohort ( eg , the majority of patients recorded sd at week 8 and no cr or pr was recorded ) , then enrollment in stage 2 might be allowed for the cohort after discussion with the sponsor and study steering committee . 
the data presented here are the results of the final analysis . seven patients entered stage 1 of the mm cohort of the ve - basket study , followed by enrollment of an additional two patients because clear clinical benefit was observed , even though the prespecified minimal response rate was not achieved . 
the patient received palliative radiotherapy and eight cycles of lenalidomide , bortezomib , and dexamethasone before undergoing high - dose melphalan therapy with autologous stem - cell transplantation in november 2008 . 
baseline characteristics of patients with brafv600 mutationpositive multiple myeloma treated with vemurafenib patients with multiple myeloma ( n = 9 ) characteristic male female age , years , median ( range ) ecog performance status brafv600 mutation type * monoclonal protein v600e v600k iga kappa iga lambda igg kappa igg lambda risk stratification high standard lines of prior systemic therapies prior systemic therapies * immunomodulators ( lenalidomide , thalidomide , pomalidomide ) corticosteroids ( dexamethasone ) alkylating agents ( cyclophosphamide , melphalan , bendamustine ) proteasome inhibitors ( bortezomib , carfilzomib ) cytotoxic agents ( doxorubicin , idarubicin ) platinum agent ( cisplatin ) topoisomerase inhibitors ( etoposide ) novel antineoplastic agents ( acy - 1215 , cc - 223 ) note . 
 ( % ) unless indicated otherwise . abbreviations : ecog , eastern cooperative oncology group performance status ; ig , immunoglobulin . * on the basis of a manual review of the data . 
 testing was by snapshot ( n = 2 ) , capillary electrophoresis single - strand conformation analysis ( n = 2 ) , direct ( sanger ) sequencing ( n = 1 ) , sequenom ( n = 1 ) , single - strand conformation analysis ( n = 1 ) , 3730 dna analyzer ( n = 1 ) , and immunohistochemistry ( n = 1 )  . 
at the time of closure of the ve - basket study , the patient was still receiving treatment in the extension study . the second patient was diagnosed with smoldering mm in may 2006 and progressed to stage ii active mm in december 2009 , at which time he was treated with lenalidomide , bortezomib , and dexamethasone . 
 ( b ) change from baseline in serum m protein according to best overall response in individual patients with brafv600 mutation positive multiple myeloma treated with vemurafenib ( n = 9 )  . 
one patient with a substantial reduction in serum m protein level had an unconfirmed pr but was considered to have sd because the patient had pd at the subsequent assessment . 
 subsequent relapses were treated with cyclophosphamide , lenalidomide , and dexamethasone ( april 2013 ) ; carfilzomib , thalidomide , and dexamethasone ( august 2013 ) ; pomalidomide , bortezomib , and dexamethasone ( march 2014 ) ; and carfilzomib , pomalidomide , and dexamethasone ( august 2014 )  . 
snapshot testing of bone marrow aspirate identified an additional nras mutation at the time of relapse that had not been seen at study entry and was reported after study closure ; the original brafv600g mutation was also present at this time . one other patient , who had been treated previously with bortezomib and dexamethasone in the first line , the mammalian target of rapamycin inhibitor cc - 223 on relapse , and lenalidomide in the third line , had a vgpr after treatment with vemurafenib . 
one patient achieved an 83% reduction in serum monoclonal protein level and had a pr at one assessment but progressive disease at the next assessment , for a best overall response of sd . 
time to event details and change from baseline in serum monoclonal protein for individual patients are shown in figure 1 . at the time of study closure , disease progression was observed in six patients . 
median investigator assessed pfs was 4.63 months ( 95% ci , 2.89 months to not estimable ) ; the 6 - month pfs rate was 40% ( 95% ci , 6% to 74% ) , and the median time to progression was 4.63 months ( 95% ci , 2.89 months to not estimable )  . 
kaplan - meier plots of pfs and os are shown in the data supplement . safety the median vemurafenib dose intensity was 79% ( range , 51% to 100% )  . 
adverse events occurring in 20% of patients with brafv600 mutationpositive multiple myeloma treated with vemurafenib ( n = 9 ) any grade grade 3 or 4 event alopecia melanocytic nevus anemia hypokalemia keratosis pilaris skin papilloma sunburn acne back pain constipation diarrhea dysphonia fatigue * hyperkeratosis keratosis follicular leukoplakia oral rash papular seborrheic keratosis skin lesion xerosis upper respiratory tract infection blood alkaline phosphatase increase increased alanine aminotransferase note . 
one patient had grade 2 hypercalcemia , which was judged unrelated to vemurafenib treatment and resolved without treatment interruption , and a grade 3 chest infection , also unrelated to treatment , during which treatment was interrupted temporarily . 
the second patient had grade 4 diabetes that was judged unrelated to the study drug but resulted in dose reduction and grade 3 cellulitis that was also unrelated to treatment but required treatment interruption . 
 the final patient had treatment - related grade 4 sepsis that resolved with dose reduction and treatment - related grade 3 skin lesion and grade 2 upper respiratory infection that were not considered serious but resulted in permanent discontinuation of treatment . 
seven patients had at least one adverse event leading to dose reduction or interruption ( infections [ n = 4 ] , skin disorders [ n = 2 ] , anemia [ n = 1 ] , blood alkaline phosphatase increased [ n = 1 ] , keratosis follicular [ n = 1 ] , diabetes mellitus [ n = 1 ] , and acute kidney injury [ n = 1 ] ) ; one patient had a dose interruption for cataract surgery . qt prolongation , squamous cell carcinoma of the skin , and keratoacanthoma were not observed . 
however , identification of the brafv600 mutation as a driver mutation in mm may lead to patients with this mutation benefitting from targeted treatment with brafv600 inhibitors.1 , 7 , 20 in this study , we have shown that vemurafenib has promising efficacy in patients with brafv600 mutationpositive mm : two patients of nine had encouraging and long - lasting responses to treatment that were ongoing at the time of study closure , and an additional patient had a shorter response . 
these patients had been treated previously with bortezomib and lenalidomide , among other agents , suggesting that resistance mechanisms in those patients did not prevent response to vemurafenib . in this study , not all patients with the brafv600 mutation responded to therapy , providing us with the opportunity to study mechanisms of resistance in this patient population in the future . 
clonal evolution of mm cells and changes in the bone marrow environment have been implicated in resistance , 21 and alterations in the erk pathway are present in almost one half of patients with mm . 
interestingly , the patient in our study who relapsed after achieving a pr had acquired an nras mutation , suggesting an escape mechanism and possible resistance via this molecular pathway . 
 hyman , jean - yves blay , josep tabernero , jrgen wolf , igor puzanov , jose baselga provision of study material or patients : all authors collection and assembly of data : all authors data analysis and interpretation : noopur raje , martina makrutzki , bethany pitcher manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors mechanisms , including driver mutations within subclonal populations , may also account for differential responses . 
understanding resistance mechanisms could lead to the development of new therapies acting on the ras / raf pathway , either alone or in combination , or to the use of mek or pan - raf inhibitors . 
this subject is being addressed in an ongoing clinical trial using a braf inhibitor and a mek inhibitor ( dabrafenib and trametinib , respectively ; clinicaltrials.gov identifier : nct03091257 )  . the safety profile of vemurafenib in this patient cohort was broadly similar to that reported previously , 8 , 9 and no new safety signals were identified . 
cutaneous squamous cell carcinoma , which has been reported in vemurafenib treated patients in earlier studies , 8 , 9 was not observed in our patients . in conclusion , vemurafenib may be an appropriate and effective choice for patients with mm in whom a brafv600 mutation has been identified . 
because the ve - basket study included few patients with mm , additional studies are required to establish the role of vemurafenib , whether as monotherapy or in combination with other agents , for earlyor later - stage disease in the treatment of this poor - prognosis population . 
 ian chau honoraria : eli lilly , gilead sciences consulting or advisory role : eli lilly , bristol - myers squibb , msd , merck serono research funding : janssen - cilag ( inst ) , sanofi ( inst ) , merck serono ( inst ) , eli lilly ( inst ) travel , accommodations , expenses : msd , merck serono , sanofi , eli lilly , bristol - myers squibb martin kaiser honoraria : takeda pharmaceuticals , celgene , amgen , janssen oncology consulting or advisory role : janssen oncology , celgene , bristol - myers squibb , takeda pharmaceuticals , amgen , chugai pharmaceutical research funding : celgene travel , accommodations , expenses : takeda pharmaceuticals david m . 
yee consulting or advisory role : takeda pharmaceuticals , dexcel pharma , adaptive biotechnologies , celgene , janssen pharmaceuticals research funding : bristol - myers squibb ( inst ) , celgene ( inst ) bethany pitcher employment : f . 
hoffmann - la roche igor puzanov consulting or advisory role : amgen , roche / genentech , bristol - myers squibb travel , accommodations , expenses : amgen , merck jose baselga leadership : infinity pharmaceuticals , varian medical systems , grail , bristol - myers squibb stock or other ownership : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , varian medical systems , tango , foghorn , aura biomedical , apogen , northern biologics , bristol - myers squibb honoraria : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , northern biologics consulting or advisory role : eli lilly , novartis , grail patents , royalties , other intellectual property : combination therapy using pdk1 and pi3k inhibitors . 
hyman , heather landau , and jose baselga , memorial sloan kettering cancer center , new york ; igor puzanov , roswell park cancer institute , buffalo , ny ; vincent ribrag , jean - marie michot , and antoine hollebecque , institut gustave roussy , villejuif ; jean - yves blay , centre leonberard , lyon , france ; josep tabernero and elena elez , vall dhebron university hospital and institute of oncology , universitat autnoma de barcelona , barcelona , spain ; jrgen wolf , university hospital kln , kln , germany ; luisa veronese and martina makrutzki , f . 
hoffmann - la roche funded third - party writing and editorial support , which was provided by miller medical communications . presented in part at the 57th annual meeting of the american society of hematology , orlando , fl , december 5 - 8 , 2015 . support prior presentation references 1 . 
dimopoulos ma , swern as , li js , et al : efficacy and safety of long - term treatment with lenalidomide and dexamethasone in patients with relapsed / refractory multiple myeloma . 
kumar sk , lee jh , lahuerta jj , et al : risk of progression and survival in multiple myeloma relapsing after therapy with imids and bortezomib : a multicenter international myeloma working group study . 
walker ba , boyle em , wardell cp , et al : mutational spectrum , copy number changes , and outcome : results of a sequencing study of patients with newly diagnosed myeloma . 
mcarthur ga , chapman pb , robert c , et al : safety and efficacy of vemurafenib in braf ( v600e ) and braf ( v600k ) mutation - positive melanoma ( brim - 3 ) : extended follow - up of a phase 3 , randomised , open - label study . 
larkin j , del vecchio m , ascierto pa , et al : vemurafenib in patients with braf ( v600 ) mutated metastatic melanoma : an open - label , multicentre , safety study . 
subbiah v , gervais r , riely gj , et al : efficacy of vemurafenib in patients ( pts ) with nonsmall cell lung cancer ( nsclc ) with brafv600 mutation . 
hyman dm , kaley tj , hollebecque a , et al : vemurafenib in patients with brafv600 mutant glioma : a cohort of the histology - independent ve - basket study . 
diamond el , subbiah v , lockhart ac , et al : vemurafenib for brafv600 - mutant erdheimchester disease and langerhans cell histiocytosis : analysis of data from the histology - independent phase 2 open - label ve - basket study . 
rajkumar sv , harousseau jl , durie b , et al : consensus recommendations for the uniform reporting of clinical trials : report of the international myeloma workshop consensus panel 1 . 
 harnessing clinical sequencing data for survival stratication of patients with metastatic lung adenocarcinomas ronglai shen , phd1 ; axel martin , ms1 ; ai ni , phd1 ; matthew hellmann , md1 ; kathryn c . 
we sought to extend the use of broad - panel sequencing results to survival stratication and clinical outcome prediction . methods by using sequencing results from a cohort of 1 , 054 patients with advanced lung adenocarcinomas , we developed oncocast , a machine learning tool for survival risk stratication and biomarker identication . results with oncocast , we stratied this patient cohort into four risk groups on the basis of tumor genomic prole . 
2019 by american society of clinical oncology introduction with the growth of precision medicine programs driven by genomic testing as well as recent us food and drug administration clearance of next - generation sequencing ( ngs ) platforms for clinical use , there has been rapid growth in the availability of broad - panel sequencing data for patients with cancer . 
zehir et al1 delineated the molecular landscape of 10 , 000 metastatic cancers in a pretreated real - world cohort sequenced by the memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) platform , a hybridization capture - based ngs panel that can detect mutations and copy number alterations in 341 or more cancer - associated genes.2 this study showed that 37% of patients harbored at least one therapeutically actionable alteration , and 11% were matched to genome - directed clinical trials . in patients with lung adenocarcinoma , tumor genotyping is now an essential step in routine clinical decision making . 
to determine treatment , patients with lung adenocarcinomas are currently categorized on the basis of the presence of mutated driver oncogenes ( eg , egfr , alk , ros1 , and braf )  . 
a multiinstitutional study characterized genetic aberrations across 10 genes in 733 tumor samples and identied an oncogenic driver in 64% of the patients.3 by using broad - panel sequencing , jordan et al4 reported on a single - institution experience of 860 patients with metastatic lung adenocarcinoma . 
more than 37% of patients received a matched therapy , and the use of matched therapy was strongly inuenced by the level of pre - existent clinical evidence that the mutation identied predicts the drug response . although the focus of tumor genotyping has been on ascertaining mutations that identify therapeutic targets , there is considerable unexplained variability in clinical outcomes , even within specic molecular subsets of patients with metastatic cancer . 
 shen et al death - ligand 1 ( pd - 1 / pd - l1 ) inhibitors.5 however , additional markers are needed to predict durable benet and long - term survival among these patients . 
some studies have explored the effects of single co - occurring alterations on outcome in patients with egfr - mutant and kras - mutant lung adenocarcinoma , and they observed that the presence or absence of pairs of co - occurring events could be used to identify those patients with a poor prognosis most in need of novel therapeutic approaches.3 , 6 - 8 however , a systematic approach is needed to additionally improve our understanding of survival and treatment outcome of patients . thus , we developed oncocast , a computational tool for survival stratication , and applied it to a large clinical series of patients with metastatic lung adenocarcinomas to improve the understanding of heterogeneity in clinical outcome for these patients and the mutation and comutational patterns that underlie such heterogeneity . 
such real - world evidence can supplement information from randomized clinical trials in that the results are more generalizable to patients treated outside randomized clinical trials , and the larger sample sizes of real - world data sets allow subset analysis that clinical trials are not powered for . 
the open - source computational pipeline that we have developed can facilitate the application of statistical and machine learning approaches for clinico - genomics analysis of precision medicine data sets . methods the oncocast method is described in the data supplement . 
electronic medical records were used to identify patient clinical factors as well as survival outcomes as previously described.4 overall survival ( os ) was dened as the time from date of diagnosis of advanced disease ( stage iv or recurrent cancer ) until date of death or last follow - up . 
however , a fraction ( 21% ) of the tumors were sampled and sequenced more than 6 months from the date of metastatic disease , with 16% sequenced at more than 1 year and 8% sequenced at more than 2 years , which represents older samples used for sequencing analysis . 
those patients with older samples which had been taken at initial diagnosis of from their initial advanced lung cancer were immortal sampling time to the time of referral for msk - impact sequencing . 
this interval can be long for a small fraction of patients ( 8% with a delayed interval of more than 2 years , as mentioned earlier ) , which introduces survival bias . 
details of lefttruncation analysis are described in the data supplement . the most frequently mutated genes were tp53 ( 55.1% ) , kras ( 30% ) , egfr ( 29.4% ) , stk11 ( 17.7% ) , and keap1 ( 17.7% ; data supplement )  . 
among the frequently comutated gene pairs , stk11 and keap1 were comutated in 10% of the tumors , and kras and stk11 were comutated in 9% of the tumors ( data supplement )  . prognostic relevance and clonality of cancer genes to dene the prognostic signicance of msk - impact panel genes that were sequenced , we developed oncocast , a machine learning tool for survival risk stratication and biomarker identication by implementing a lassopenalized proportional hazards regression for deriving prediction rules for os and feature selection ( data supplement )  . 
oncocast uses an ensemble learning strategy by repeatedly splitting the cohort into training and test sets that generate an ensemble of classiers with varying selection of genes and gene combinations ( data supplement )  . the median number of prognostic genes selected was 19 ( range , 4 - 67 genes ) , with a total of 169 cancer genes selected at least once by the ensemble learner . 
the relative prognostic importance of each gene was measured by how often it was selected ( fraction of the models containing the gene ) and its average regression coefcients , which determined the corresponding weights for individual genes in the scoring rule . 
circle size is proportional to mutation frequency . targeted and immunotherapies than subclonal events.9 - 11 we thus used the high depth of coverage afforded by our sequencing data ( mean coverage , 758 ) to determine the clonality of the gene alterations found to be associated with prognosis in the analysis we outlined earlier . 
 shen et al oncocast : an integrated prognostic scoring system based on ngs tumor proling in addition , improvement . oncocast aggregates prognostic effects across the sequenced cancer genes to derive a genomic risk score for each patient ( scaled from 0 to 10 ) , with a higher score indicating a greater likelihood of shorter survival . 
there was a difference of more than 6 units in average risk score between the highand low - risk groups . the oncocast classication substantially outperformed all of the individual genes as a predictor of os ( fig 3b )  . 
oncocast risk score remained a highly signicant predictor after adjusting for clinical variables and treatment types as potential confounding factors in a multivariable cox regression model ( data supplement )  . to conrm the validity of the oncocast survival stratication , we applied it to a separate data set of patients with mostly early - stage nonsmall - cell lung cancer obtained from the cancer genome atlas lung adenocarcinoma analysis . 
stk11 is a tumor suppressor gene that encodes for the serine / threonine kinase lkb1 that functions as a negative regulator of mammalian target of rapamycin ( mtor ) signaling . 
to examine the status of the other allele in such cases , we performed allele - specic cna using the fraction and allele - specic copy number estimates from tumor sequencing ( facets ) algorithm.15 strikingly , more than 90% of stk11 mutant tumors had evidence of biallelic inactivation through loss of heterogeneity ( loh ) of chromosome 19p ( data supplement )  . 
the majority of keap1 mutations were missense , and the mutant copy was frequently duplicated ( present as copy - neutral loh and uniparental gains ) as reected in the average total copy number . we also explored whether other tumor characteristics such as tumor mutational signature or intratumor heterogeneity were prognostic and associated with oncocast risk score . previously dened smoking - associated and apolipoprotein b mrna editing enzyme , catalytic polypeptide - like ( apobec ) signatures were the most prevalent mutational signatures in this cohort . 
however , mutation burden did not provide additional prognostic value beyond oncocast risk score in a multivariable cox model ( data supplement )  . clonal diversity was calculated for each tumor by summarizing the cancer cell fraction for all somatic mutations using the shannon index . 
 ( a ) kaplan - meier plot of survival curves for the four risk subgroups ( low , intermediate - low [ int - low ] , intermediate - high [ int - high ] , and high )  . 
the average risk score ( avg rs ) , median overall survival ( os ) , and 1 - year and 3 - year survival probabilities are reported for each group . 
 ( b ) forest plot of hazard ratios ( hrs ) for age , sex , smoking status , and individual driver gene alterations compared with the oncocast integrated scoring approach . genotypes associated with risk groups to better understand the association between targetable cancer driver mutations and oncocast risk score , we explored the distribution of genotypes within four major risk categories ( fig 5 )  . 
the dening characteristic for the patients in the low - risk group without egfr , alk , ret , and ros1 alterations was an absence of any of the poor prognostic gene alterations . 
this suggests that stk11 and keap1 comutation denes a cohort of patients with resected lung adenocarcinoma at higher risk of disease progression and cancerspecic mortality . survival stratication in specic treatment subsets we then sought to demonstrate the ability of the oncocast technique to explore tumor genomic predictor outcomes in last to death or the subset of patients with mutated driver oncogenes treated with kinase inhibitors . 
the model , oncocast - tr ( targeted therapies model ) , was derived using the genomic proles and survival outcomes from the start of therapy for the 387 patients who received targeted therapies ( egfr , alk , ros )  . 
tp53 is strongly associated with worse survival outcome ( fig 6c ) , with 96% of patients in the tr2 group harboring concurrent tp53 mutations and 0% concurrent tp53 mutations in the tr1 group . 
arid1a also showed association with poor survival with 11 ( 78% ) of 14 arid1a mutations in tr2 . interactive tool for visualizing and exploring mutation pattern and survival to facilitate clinical translation and research use of the data , we created an interactive web application ( data that allows for visualization of mutation supplement ) ros1 fusion , 6% ret fusion , low - intermediate tp53 , egfr , smarca4 , 2% tp53 , ret fusion , 1% tp53 , alk fusion , 1% tp53 , ros1 fusion , 2% tp53 , smarca4 , 3% egfr , 40% tp53 , kras , tp53 , egfr , tp53 , egfr , alk fusion , other , 30% kras , 17% tp53 , 24% high - intermediate keap1 , 2% stk11 , 5% tp53 , kras , stk11 , 6% tp53 , kras , keap1 , 6% tp53 , keap1 , kras , keap1 , kras , stk11 , stk11 , keap1 , smarca4 , 7% tp53 , kras , stk11 , keap1 , 8% stk11 , keap1 , 8% high tp53 , stk11 , keap1 , smarca4 , 6% kras , stk11 , keap1 , 28% tp53 , stk11 , keap1 , 25% tp53 , stk11 , 10% kras , stk11 , keap1 , smarca4 , 16% fig 5 . 
 ( c ) gene importance plot for the oncocast - tr model . patterns and individualized prediction of os to be generated on the basis of a user - dened mutational prole and clinical characteristics . 
along with a patients clinical prole , the application outputs the predicted survival probabilities and 95% cis . although the tool was built using the largest metastatic lung adenocarcinoma cohort to date , it was designed to be dynamically updated as new data are incorporated into the model . discussion tumors from patients with lung adenocarcinoma have a high frequency of actionable oncogenic drivers.16 , 17 the introduction of targeted therapy has transformed the clinical care of patients with lung adenocarcinoma by incorporating tumor genotyping into therapeutic decision making . 
by using an ensemble learning approach , we demonstrated the prognostic utility of data from a large panel ngs assay interrogating 341 cancer - associated genes in 1 , 054 patients with metastatic lung adenocarcinoma treated with currently available therapies . 
we show that it is a practical approach to molecular stratication in metastatic lung adenocarcinoma and provides the ability to identify biomarkers that predict survival outcome . overlaying the oncocast risk score with the tumor genomic landscape revealed novel biologic and clinical insights . 
the major prognostic genes associated with poor survival included stk11 , keap1 , tp53 , kras , and smarca4 . remarkably , comutations of both stk11 and keap1 dened an exceptionally high - risk prole with a short median os of 7.3 months and an increase of more than 6 units in risk score compared with a low - risk group , corresponding to an hr of 4.6. 
some of the favorable prognostic genes may reect the availability of effective targeted therapies in the case of egfr , alk , and ros1 . however , in patients with these targetable oncogenes , there is heterogeneity in the additional mutations their tumors harbor . 
for example , our model revealed that mutations in tp53 and arid1a dene a high - risk subgroup with shorter survival in the tyrosine kinase inhibitortreated patient cohort . is novel in that conversely , some of the unfavorable prognostic genes may reect negative associations with treatment responses ( eg , the recent observation that stk11 inactivation is associated with poor responses to immunotherapy18 )  . 
mutations in keap1 are associated with chemotherapy resistance and poor survival . some studies have suggested that targeting nrf2 may enhance chemotherapy sensitization.19 , 20 mtor is a kinase downstream of lkb1 ( stk11 ) , and mtor inhibitors have been proposed as a potential therapeutic approach in stk11 - mutant tumors.21 smarca4 was also identied as a major driver of a poor prognosis factor in metastatic lung adenocarcinoma in our study . 
 shen et al complexes that regulate genomic instability and dna repair . smarca4 was mutated in 9.4% of lung adenocarcinomas in the msk - impact cohort , with 42% of the mutations being truncating and residing in regions of loh . 
with increasing sample sizes , we will be poised to identify outcome associations with rare alterations , and we will be better able to explain the heterogeneity in clinical outcomes for patients with advanced lung adenocarcinoma . in addition , the oncocast risk score described here provides a valuable tool for more accurately determining the prognosis of patients enrolled in clinical trials or included in real - world data sets . 
although conventional clinical factors such as age , sex , and performance status have long been used , our data indicate that we can signicantly improve the description of patient populations by incorporating the genomic risk scores in our understanding to allow better comparisons of groups of patients enrolled in clinical trials or included in real - world data sets . with the growth of precision medicine programs driven by genomic testing as well as recent us food and drug administration clearance of ngs platforms for clinical use , there will be a rapid growth in the availability of broad sequencing data for patients with a variety of cancers and growing integration with clinical data through institutional databases and electronic health records . 
riely manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors matthew hellmann stock and other ownership interests : shattuck labs honoraria : astrazeneca , bristol - myers squibb consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca / medimmune , novartis , janssen , nektar therapeutics , syndax pharmaceuticals , mirati therapeutics , shattuck labs research funding : bristol - myers squibb ( inst ) patents , royalties , other intellectual property : a patent has been led by memorial sloan kettering ( pct / us2015 / 062208 ) for the use of tumor mutation burden for prediction of immunotherapy efcacy , which is licensed to personal genome diagnostics ( inst ) travel , accommodations , expenses : astrazeneca , bristol - myers squibb kathryn c . 
rudin consulting or advisory role : bristol - myers squibb , abbvie , seattle genetics , harpoon therapeutics , genentech , astrazeneca , ascentage pharma , bicycle therapeutics , celgene , daiichi sankyo , ipsen , loxo oncology , pharmamar , elucida oncology research funding : abbvie / stemcentrx ( inst ) , viralytics ( inst ) , merck ( inst ) , daiichi sankyo ( inst ) michael f . 
solit stock and other ownership interests : loxo oncology consulting or advisory role : pzer , loxo oncology , illumina , intezyne technologies , vivideon therapeutics travel , accommodations , expenses : merck maria arcila consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe technologies , raindance technologies marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso request for proposal advisory committee , takeda pharmaceuticals , bristol - myers squibb , bayer ag , merck ( i ) research funding : loxo oncology ( inst ) , helsinn therapeutics gregory j . 
riely research funding : novartis ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pzer ( inst ) , innity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : merck sharp & dohme no other potential conicts of interest were reported . references zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
nat med 23 : 703 - 713 , 2017 cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
j mol diagn 17 : 251 - 264 , 2015 kris mg , johnson be , berry ld , et al : using multiplexed assays of oncogenic drivers in lung cancers to select targeted drugs . 
jama 311 : 1998 - 2006 , 2014 jordan ej , kim hr , arcila me , et al : prospective comprehensive molecular characterization of lung adenocarcinomas for efcient patient matching to approved and emerging therapies . 
hellmann md , nathanson t , rizvi h , et al : genomic features of response to combination immunotherapy in patients with advanced non - small - cell lung cancer . cancer cell 33 : 843 - 852.e4 , 2018 arbour kc , jordan e , kim hr , et al : effects of co - occurring genomic alterations on outcomes in patients with kras - mutant non - small cell lung cancer . 
clin cancer res 24 : 334 - 340 , 2018 yu ha , suzawa k , jordan e , et al : concurrent alterations in egfr - mutant lung cancers associated with resistance to egfr kinase inhibitors and characterization of mtor as a mediator of resistance . 
clin cancer res 24 : 3108 - 3118 , 2018 yu ha , sima cs , shen r , et al : prognostic impact of kras mutation subtypes in 677 patients with metastatic lung adenocarcinomas . 
j thorac oncol 10 : 431 - 437 , 2015 de bruin ec , mcgranahan n , mitter r , et al : spatial and temporal diversity in genomic instability processes denes lung cancer evolution . 
rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
azzoli cg , temin s , giaccone g : 2011 focused update of 2009 american society of clinical oncology clinical practice guideline update on chemotherapy for stage iv non - small - cell lung cancer . 
directors challenge consortium for the molecular classication of lung adenocarcinoma , shedden k , taylor jm , et al : gene expression - based survival prediction in lung adenocarcinoma : a multi - site , blinded validation study . 
ren d , villeneuve nf , jiang t , et al : brusatol enhances the efcacy of chemotherapy by inhibiting the nrf2 - mediated defense mechanisproc natl acad sci u 21 . 
tagal v , wei s , zhang w , et al : smarca4 - inactivating mutations increase sensitivity to aurora kinase a inhibitor vx - 680 in non - small cell lung cancers . 
 o intrahepatic cholangiocarcinoma : genomic heterogeneity between eastern and western patients jingyu cao , md1 ; jing hu , phd2 ; siqin liu , phd3 ; funda meric - bernstam , md4 ; reham abdel - wahab , md5 ; junjie xu , md6 ; qiang li , md7 ; maolin yan , md8 ; yujie feng , phd1 ; jianzhen lin , md9 ; songhui zhao , msc3 ; jian wang , ms3 ; lawrence n . 
borad , md10 ; kai wang , md , phd3 ; milind javle , md4 ; and haitao zhao , md9 purpose intrahepatic cholangiocarcinoma ( ihcca ) , a global health problem , is increasing in incidence and has differing etiologies worldwide . 
ngs data from asia , where ihcca is most prevalent , are limited . methods comprehensive genomic proling of formalin - xed parafn - embedded tumor tissue from 164 asian and 283 western patients with ihcca was performed using ngs . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction cholangiocarcinoma ( cca ) , a global health problem , constitutes about 10% - 20% of all primary liver cancers worldwide . 
in western countries , including the united states , metabolic syndrome , inammatory bowel disease , primary sclerosing cholangitis , hepatitis c , and alcohol abuse are the main cca risk factors , and the age - standardized incidence rate is 1.6 per 100 , 000.1 the incidence in southeast asia is extremely high , up to 71.3 per 100 , 000 in certain parts of asia , and is associated with liver uke and hepatitis b virus ( hbv ) infection.2 notably , there is an increasing incidence of intrahepatic cholangiocarcinoma ( ihcca ) worldwide , and its etiology is unclear.3 surgical resection is the only potentially curative treatment , but the majority of patients present with an advanced disease stage and have a limited therapeutic options . 
ihcca , in particular , is enriched with a relatively high number of actionable mutations , and early reports indicate several promising leads with targeted therapies for broblast growth factor receptor 2 fusion ( fgfr ) , isocitrate dehydrogenase - 1 ( idh1 ) , braf v600e mutations , and her2 / neu amplication.2 nevertheless , ngs data from asia , where cca is most prevalent , are limited . 
patients with high tmb had alterations in direct dna repair genes and caretaker genes , especially in the asian population . relevance these results may reect differences in disease etiology and are relevant for targeted therapy and immunotherapy trials for patients with intrahepatic cholangiocarcinoma . methods comprehensive genomic proling of formalin - xed parafn - embedded ( ffpe ) tumor tissue blocks from the primary tumor or metastatic lesions obtained from patients with ihcca was performed in 283 patients from a single center in the united states and in 164 patients from china . in the united states , all genomic proling analysis was performed using a clinical laboratory improvement amendments ( clia ) - validated platform ( foundation medicine , cambridge , ma )  . 
in china , genomic proling was performed by using another clia - validated targeted sequencing platform ( origimed , shanghai , china ) .5 a bridging study comparing the 2 platforms indicated high concordance ( 96.3% ; 26 / 27 ) for the same study samples ( results indicated in appendix table a1 )  . 
all ffpe tissue blocks were sectioned and stained with hematoxylin and eosin and reviewed by an expert pathologist to conrm the diagnosis and presence of least 20% of the dna derived from tumor cells . 
this research was approved by the institutional review boards at md anderson cancer center and peking union medical college . hybrid selection and sequencing a custom hybridization capture panel including over 23 , 660 individually synthesized 5 ( cid : 3 ) - biotinylated dna 120 bp oligonucleotides was used to target the exons of cancer - related genes , as well as selected introns of genes frequently rearranged in cancer . 
hybridization capture followed the protocol of hybridization capture of dna libraries using xgen lockdown probes and reagents ( version 3 ; integrated dna technologies , san diego , ca )  . postcapture libraries were mixed together , denatured , diluted , and then sequenced . 
for the purpose of estimation of sequencing error rate , a phix spike - in was added as an external control to measure the percentage of reads with 0 - 4 mismatches , following the method described by manley et al.6 bioinformatics pipeline all types of genetic alterations , including single - nucleotide variant ( snv ) , short and long indels , copy number alterations ( cnas ) , and gene rearrangement , were called using a suite of bioinformatics pipelines.5 analysis of snvs and indels began with the alignment of raw reads to the human genome reference sequence ( hg19 ) with the burrows - wheeler aligner ( v0.62 ; bwa , cambridge , ma ) , followed by polymerase chain reaction ( pcr ) duplicates removal using markduplicates algorithm from picard ( version 1.47 ; cambridge , ma )  . 
local realignment and base quality recalibration for snvs were performed using gatk ( v3.1 - 1 ; cambridge , ma ) and subsequently called by mutect ( v1.7 ; cambridge , ma )  . 
the cnas included : ( 1 ) amplication , dened as an increase in the number of gene segment copies by 8 , and ( 2 ) homozygous deletion , dened as decrease of complete loss of gene segment copies in samples with  . 
2 , 000 or zero bp were collected and used as discordant reads , that is , paired - end reads that could not be closely mapped to a genome reference , with each read of paired reads aligned to the same chromosomes or different chromosomes . 
the breakpoints were double conrmed by blat , and the resulting chimeric gene candidates were annotated . oncogenic genetic mutations statistical analysis was only based on oncogenic genetic variants and the variants of unknown signicance ; lowfrequency ( variant allele frequency , .01 ) variants were excluded . 
data are % unless otherwise specied . abbreviations : fhx , family history ; hav , hepatitis a virus ; hbv , hepatitis b virus ; hcv , hepatitis c virus ; hx , history ; sd , standard deviation . studies exist on the mutations situated on the same genome loci and structural disrupting mutations on tumor suppressor genes , such as truncations , splicing sites , and frameshifts ; ( 3 ) conrmed somatic : somatic mutations recorded on the public genomic database , such as cosmic , and detected at least once in any tumor types . tumor mutation burden and known germline alterations in dbsnp were not counted . 
we classied our patients according to the tmb scores into : ( 1 ) tmb low ( tmb - l ) if the number of mutations per megabase ( mut / mb ) was , 6 , ( 2 ) tmb inthe number of mutations per termediate ( tmb - i ) megabase was between 6 and 9 , and ( 3 ) tmb high ( tmb - h ) if the number of mutations per megabase was 10 . 
the tmb cutoff was dened per prior lung cancer trials.7 , 8 tumor mutation burden ( tmb ) was estimated for 157 us patients and 164 chinese patients with ihcca by counting its somatic mutations , including coding snvs and indels per megabase of the sequence examined . 
 cao et al msi score , we classied the samples as msi high ( msi - h ) , dened as instability in 2 microsatellite loci ; msi low , dened as instability in only 1 loci ; and microsatellite stable , dened as absence of any evidence of microsatellite loci instability . 
furthermore , the chinese patients had a signicantly higher rate of well - differentiated adenocarcinoma compared with their us counterparts ( p = .002 ; table 1 )  . western versus asian ngs comprehensive genomic proling comprehensive genomic proling identied 1 , 007 genetic aberrations ( gas ) in chinese patients compared with 971 gas in us patients ( appendix table a2 )  . 
each patient harbored at least 1 ga , with an average of 6.1 ( range , 1 to approximately 20 ) and 3.4 ( range , 1 to approximately 16 ) gas per tumor in chinese and us patients , respectively . 
as indicated in figure 1 , the most commonly reported gas in chinese patients were tumor protein 53 ( tp53 ; 41.5% ) , kirsten rat sarcoma viral oncogene homolog ( kras ; 28.7% ) , at - rich interactive domain - containing protein 1a ( arid1a ; 18.3% ) , chinese patients ( n = 164 ) us patients ( n = 283 ) dna repair genes china substitution / indel gene amplification gene homozygous deletion fusion / rearrangement truncation fig 1 . 
 ( b ) the afliated chart indicates the alterations among direct and caretaker dna repair genes . mutations are colored according to mutation types of substitution / indel , gene amplication , gene homozygous deletion , truncation , and fusion / rearrangement . 
in our cohorts , we dened dna repair genes to include the 20 most frequent previously reported dna repair gene gas , including direct dna repair genes ( atm , atr , brca1 , brca2 , fanca , fancd2 , mlh1 , msh2 , msh6 , palb2 , pold1 , pole , prkdc , rad50 , and slx4 ) and caretaker genes ( bap1 , cdk12 , kmt2c / mll3 , tp53 , and blm ) .9 remarkably , chinese patients harbored more dna repair gas compared with us patients with ihcca , with predominant gas in tp53 , brca1 / 2 , kmt2c , and rad50 . 
furthermore , there was no signicant difference in the median values of tmb - h , tmb - i , and tmb - l groups among the chinese ( 14 , 8 , and 2 mut / mb , respectively ) and us patients with ihcca ( 19 , 7 , and 3 mut / mb , respectively )  . 
moreover , we identied that the rate of msi - h in chinese and us patients was 1.8% ( n = 3 ) and 0.6% ( n = 1 ) , respectively , and all msi - h patients were associated with high tmb values ( fig 2 )  . we explored the association between dna repair gene gas and tmb , and identied a signicantly higher rate of tmb - i and tmb - h in patients who had combined direct and caretaker dna repair gas compared with patients without dna repair gas among the chinese ( p , .001 ) and us ( p = .05 ) patients with ihcca . 
the advent of ngs offers promising breakthroughs with targeted therapy and immunologic interventions . however , it is important to identify genomic heterogeneity between populations because this will have a signicant impact on precision medicine approaches for this cancer . in our study , we performed comprehensive molecular proling of 164 chinese and 283 us patients with ihcca to explore genomic heterogeneity between populations . 
mutation types are presented in the color key at the bottomss , microsatellite stable ; mut / mb , mutations per megabase . noted important differences between asian and western patients with ihcca . 
through the results , chinese patients had signicantly higher frequency of tp53 as well as kmt2c , brca1 / 2 , ddr , tert , tgfbr2 , rbm10 , nf1 , spta1 , and rb1 gas . 
 ( b ) the correlation between tmb status and dna repair genetic aberrations ( gas ) by presenting the rates of tmb levels in different existence patterns of direct dna repair gas and caretaker gas . genetic diversity could be attributed to variations in the in western underlying disease risk factors ( table 2 )  . countries , cca is associated with metabolic syndrome , inammatory bowel disease , primary sclerosing cholangitis , and hepatolithiasis , whereas liver uke and hbv are important risk factors in asian countries . 
in this study , high tmb was associated with longer progression - free survival.13 also , pembrolizumab has been approved by the food and drug administration for the dna mismatch repair decient ( mmr - d ) cancers based on a phase ii clinical trial that showed a 40% objective response rate and 78% progression - free survival rate in patients with colorectal cancer with mmr - d compared with 0% and 11% , respectively , for mmr - procient patients.14 similar results have been achieved in noncolorectal cancers that included 4 patients ( 44% ) with biliary tract cancer . 
the role of combined poly ( adp - ribose ) polymerase inhibitors and pd - 1 inhibitors in advanced solid tumor is currently under investigation and may be applicable to this subgroup . our study has important limitations . 
in these panels : ( 1 ) the content genes had some dissimilarities ; to address this issue , we ltered out differential genes and only included the 320 overlapped genes into the analysis , thereby ensuring the comparability ; ( 2 ) sequencing platforms were illumina hiseq2500 ( illumina , san diego , ca ) for foundationone and novaseq ( illumina ) for origimed450 , with effective depths of 500 and 700 , both reecting the accuracy of sequencing results17 ; ( 3 ) the tmb algorithm of origimed450 was based on the published algorithm of foundationone , and the genomic alterations were selected similarly18 ; ( 4 ) the origimed450 platform uses blood samples from individual patients as their own control for eliminating the impact of germline polymorphisms , whereas foundationone uses the somatic - germline - zygosity algorithm and databases of dbsnp and exac for the same , and nally ; and ( 5 ) we conducted a bridging study comparing the 2 platforms and showed a high degree of concordance . 
furthermore , we have examined the clinical characteristics of the chinese and us patients and demonstrated that demographic differences between these populations were minor , with most patients having an advanced disease stage . 
there was a higher proportion of hepatitis b exposure in the asian cohort , and the pathophysiologic relationship between the viral infection and somatic mutations in cancer is unknown at this time . future studies to investigate the genomic proling in different populations , taking into consideration the disease risk factors , are warranted . 
data regarding pd - 1 and pd - l1 expression were not available ; therefore , we could not identify variations in immune biomarker expression between the 2 cohorts in this study . 
borad , kai wang , milind javle , haitao zhao administrative support : jingyu cao , jing hu , maolin yan provision of study materials or patients : qiang li , jianzhen lin , lawrence n . 
kwong , haitao zhao collection and assembly of data : jingyu cao , jing hu , siqin liu , reham abdel - wahab , qiang li , maolin yan , yujie feng , jianzhen lin , lawrence n . 
kwong , jinwei hu , fernando carapeto , milind javle , haitao zhao data analysis and interpretation : siqin liu , funda meric - bernstam , reham abdel - wahab , qiang li , songhui zhao , jian wang , lawrence n . 
 ihcca : genomic heterogeneity between eastern and western patients funda meric - bernstam employment : md anderson cancer center honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group , mersana , seattle genetics , silverback therapeutics , immunomedics , ibm watson health , f . 
hoffman - laroche , ibm watson health , pact pharma , effector therapeutics speakers bureau : chugai biopharmaceuticals research funding : novartis ( inst ) , astrazeneca ( inst ) , taiho pharmaceutical ( inst ) , genentech ( inst ) , calithera biosciences , debiopharm group ( inst ) , bayer ( inst ) , aileron therapeutics ( inst ) , puma biotechnology ( inst ) , cytomx therapeutics ( inst ) , jounce therapeutics ( inst ) , zymeworks ( inst ) , curis ( inst ) , pzer ( inst ) , effector therapeutics ( inst ) , abbvie ( inst ) , boehringer ingelheim ( i ) , guardant health ( inst ) , daiichi sankyo ( inst ) , glaxosmithkline ( inst ) , seattle genetics ( inst ) travel , accommodations , expenses : taiho pharmaceutical , seattle genetics , beth israel deaconess medical center songhui zhao employment : origimed lawrence n . 
borad stock and other ownership interests : gilead sciences , aveo , intercept pharmaceuticals , spectrum pharmaceuticals consulting or advisory role : g1 therapeutics , fujilm ( inst ) , agios ( inst ) , insys therapeutics ( inst ) , novartis ( inst ) , arqule ( inst ) , celgene ( inst ) , inspyr therapeutics , halozyme ( inst ) , pieris pharmaceuticals ( inst ) , taiho pharmaceutical ( inst ) , immunovative therapies , exelixis , lynx group , genentech , western oncolytics , klus pharma , denovo , merck , imvax research funding : boston biomedical ( inst ) , mirna therapeutics ( inst ) , senhwa biosciences ( inst ) , medimmune ( inst ) , biolinerx ( inst ) , agios ( inst ) , halozyme ( inst ) , celgene ( inst ) , threshold pharmaceuticals ( inst ) , toray industries ( inst ) , dicerna ( inst ) , sillajen ( inst ) , eisai ( inst ) , taiho pharmaceutical ( inst ) , emd serono ( inst ) , isis pharmaceuticals ( inst ) , incyte ( inst ) , sun biopharma ( inst ) , ariad ( inst ) , imclone systems ( inst ) , qed therapeutics ( inst ) , incyte ( inst ) , puma biotechnology ( inst ) , adaptimmune ( inst ) , merck serono ( inst ) , redhill biopharma ( inst ) , basilea ( inst ) travel , accommodations , expenses : arqule , celgene , astrazeneca kai wang employment : origimed leadership : origimed milind javle consulting or advisory role : qed , oncosil , incyte , mundi other relationship : rafael pharmaceuticals , incyte , pieris pharmaceuticals , merck , merck serono , novartis , seattle genetics , beigene , qed therapeutics , bayer no other potential conicts of interest were reported . references chun ys , javle m : systemic and adjuvant therapies for intrahepatic cholangiocarcinoma . 
curr treat options oncol 17 : 58 , 2016 saha sk , zhu ax , fuchs cs , et al : forty - year trends in cholangiocarcinoma incidence in the u.s. : intrahepatic disease on the rise . 
nat genet 44 : 690 - 693 , 2012 cao j , chen l , li h , et al : an accurate and comprehensive clinical sequencing assay for cancer targeted and immunotherapies . 
n engl j med 378 : 2093 - 2104 , 2018 rizvi na , mazi `eres j , planchard d , et al : activity and safety of nivolumab , an anti - pd - 1 immune checkpoint inhibitor , for patients with advanced , refractory squamous non - small - cell lung cancer ( checkmate 063 ) : a phase 2 , single - arm trial . 
lancet oncol 16 : 257 - 265 , 2015 chae yk , anker jf , bais p , et al : mutations in dna repair genes are associated with increased neo - antigen load and activated t cell inltration in lung adenocarcinoma . 
oncotarget 9 : 7949 - 7960 , 2017 jusakul a , cutcutache i , yong ch , et al : whole - genome and epigenomic landscapes of etiologically distinct subtypes of cholangiocarcinoma . 
chan - on w , nairism agi ml , ong ck , et al : exome sequencing identies distinct mutational patterns in liver uke - related and non - infection - related bile duct cancers . 
clarke b , tinker av , lee ch , et al : intraepithelial t cells and prognosis in ovarian carcinoma : novel associations with stage , tumor type , and brca1 loss . 
ali sm , yao m , yao j , et al : comprehensive genomic proling of different subtypes of nasopharyngeal carcinoma reveals similarities and differences to guide pathol 22 : 393 - 402 , 2009 gynecol oncol 141 : 293 - 302 , 2016 targeted therapy . 
the respected blocks were sectioned at 5 mm ; the tumor content size and were conrmed by a trained pathologist , and a minimum of 5 unstained slides were submitted for conrmation using the origimed platforinstitutional review board approval was obtained for this study . 
the discussion mainly focuses on inference for a beneting subpopulation , that is , a characterization of a group of patients who benet from the treatment under consideration more than the overall population . 
when the selection of the interesting subpopulation is carried out as the trial proceeds , the design becomes an adaptive clinical trial design , using subgroup analysis to inform the randomization and assignment of treatments to patients . 
that is , subgroup analysis is concerned with the question of whether a conclusion for the entire eligible patient population in a clinical trial remains valid for subpopulations of interest . 
to be specic , consider a two - arm randomized trial that is carried out to learn about the effectiveness of an experimental therapy versus a control , and assume that no signicant treatment effect can be established in the overall population . 
the question is closely related to personalized optimal treatment selection as it is needed , for example , in precision oncology . the investigation of hypotheses related to the notion that certain subgroups may benet from certain therapies more than others necessitates a disciplined way to identify such subgroups and to quantify the benet to these groups . 
dangers that investigators face in setting up subgroup analyses include studies being underpowered to detect signicant effects in subgroups , the issue of multiple testing , and the possibility for data dredging . we focus on a bayesian perspective because it naturally addresses multiplicities through the use of priors and because of its alignment with decision theoretic approaches , 1 which provide an elegant way to address competing aims in subgroup analysis . 
first , we discuss in general terms some of the questions that arise in subgroup analysis and then present some approaches that have been developed in the bayesian literature and compare them in a small simulation . 
 nugent et al context key objective review and comparison of subgroup analysis approaches and discussion of subgroup enrichment designs for clinical trials . knowledge generated we demonstrate how subgroup analysis can be carried out by different bayesian approaches and discuss how these different approaches identify potentially different subpopulations on the basis of the interests and objectives in practice . relevance subgroup analysis and subgroup enrichment designs are a focus point of precision oncology . 
this may help guide future implementation of these novel statistical methods in real - world trials . parsimony can be induced by restricting the model space . for example , the model space might only include models dened by one or two binary covariates , thereby only allowing subgroups dened by at most two covariates . alternatively , parsimony can be induced through the use an explicit utility function . 
for patient i , let yi denote an outcome that is assumed to be some measure of efcacy , let ti denote a treatment indicator , and let x i ( cid : 1 ) ( xi1 , , xij ) denote a set of covariates . 
the covariates could potentially dene subgroups . regression the earliest discussions of bayesian subgroup one of analysis is by dixon and simon , 3 who approach subgroup analysis as inference on regression coefcients , specically the coefcient for the interaction between a treatment indicator ( ti ) and a covariate ( xij )  . 
although this shrinks the covariates for variables with no effect toward zero , it does not introduce sparsity . sparsity could be enforced by putting alternate priors on these coefcients , such as spike and slab4 - 7 or nonlocal priors.8 model selection here , subgroups are dened by competing models , where the covariates included in the winning model dene the subgroup . 
the general setup starts with a list of possible models and then compares models in a principled manner . in general , bayesian model selection induces sparsity through prior distributions that are specied for each model . one can argue that the use of prior probability models implicitly introduces a complexity penalty by spreading out probability mass for additional parameters.9 , 10 by including the model choice in the prior specication , the approach naturally considers the entire model space at once , making all models directly comparable . we consider two methods that use model selection to perform subgroup analysis.11 , 12 in the method of berger et al , 11 the model space is restricted to models that can be written as a tree dened by one or two covariates . 
in this gure , the enhanced treatment effects for the winning subgroups are circled in red , and the subgroups are underlined . construction , this only allows for subgroups dened by up to two covariates , enforcing a minimum level of sparsity . rather than trees , sivaganesan et al12 use clustering to dene a model space . 
because only models within a family are directly comparable , the approach introduces a reasonable , but ad hoc , rule on the basis of thresholds for selecting models to report as formal subgroups . 
the thresholds can be tuned to control desired frequentist properties of the procedure , such as the rate of falsely choosing a model with a common overall treatment effect over a subgroup model . 
because the algorithm may select multiple subgroups corresponding to different families , it can potentially be difcult to interpret the results , especially because models in different families are not directly comparable . 
in particular , if there is a signicant amount of correlation between covariates , the algorithm is not designed to pick a clear winner . potential outcomes although many approaches to subgroup analysis implicitly include a notion of potential outcomes , some explicitly use potential outcomes as the input to the search for subgroups . 
the authors rst use a random forest to estimate the potential outcomes ( y ( 0 ) ) for each patient and then input this into another tree - based regression model to identify an estimate b ( cid : 1 ) { x : ( x )  . 
here ( x ) is the unknown true difference in expected potential outcomes . subgroups are identied as the paths that lead to leaves of the tree that have an estimated treatment effect above zero or above a specied threshold . , y ( 1 ) decision problems some approaches focus on the nature of a subgroup report as a decision problem and introduce a utility function , u ( a , , y ) , to characterize the preference for a decision a , in this case the beneting subgroup , under data y and a hypothetical truth , represented by the parameters , in an assumed sampling model . 
the utility usually includes a preference for parsimony but can also account for other aims , such as a preference for patient populations that are not well served by currently available treatments . 
although we introduce here a decision theoretic choice of a subgroup report as an alternative to other methods , it could also be argued that it can be included as an additional step in any of the earlier considered approaches . the approach taken by morita and m uller14 denes a utility function that favors a subgroup with a large difference in treatment effect relative to the overall population , a large subgroup that includes many potential patients , and a subgroup that can be parsimoniously described by only a few covariates . 
besides type i and type ii errors related to selecting an overall null or an overall alternative hypothesis , meaning the absence of any treatment effect or the presence of a common treatment effect , respectively , several other frequentist summaries are of interest . 
for example , under a scenario with a true subgroup , morita and m uller14 report a false subgroup rate as the probability of reporting a subgroup effect that is different from the true subgroup effect and a true subgroup rate as the probability of correctly reporting the true subgroup . subgroup as a random quantity the nature of the true subgroup ( b ) as a function of the unknown parameters ( ie , as a random variable ) is the focus in the article by schnell et al.15 although b itself is unknown , bounds on b can be calculated . 
 nugent et al outside of e ( ie , in e c ) have a low probability of benetting . in this way , they dene a credible region , bounded by s and e , that contains the true benetting subgroup ( b ) with a prespecied probability . 
the discussion in schnell et al16 includes a straightforward algorithm to determine ( s , e )  . a strength , and perhaps at the same time a limitation , is that s and e could be complicated subsets of the covariate space that are not necessarily easy to communicate , and the joint report of ( s , e ) could be difcult to interpret . 
we refer to the approaches by the following acronyms : ds for dixon and simon3 ; vt13 ; bw for berger and wang11 ; pu for polya urn12 ; bapofi for bayesian population nding14 ; cs - i for credible subgroups ( inclusive subset ) 15 ; and cs - e for credible subgroups ( exclusive subset ) .15 setup of the simulation study consider a patient population where three biomarkers of interest have been recorded for each patient . 
we consider two scenarios , one that has a predictive effect for biomarker 3 and another that has a predictive effect for biomarker 3 as well as a prognostic effect for biomarker 1 . 
under the simulation truth , patients with the following baseline covariates [ x ( cid : 1 ) ( x1 , x2 , x3 ) ] should be agged : { ( 0 , 0 , 1 ) , ( 1 , 0 , 1 ) , ( 0 , 1 , 1 ) , ( 1 , 1 , 1 ) }  . in addition to identifying subsets of beneting patients , some methods allow a report of no treatment effect ( h0 ) , meaning the treatment is not effective for anyone in the population , or an overall treatment effect ( h1 ) , meaning that the treatment is equally effective for everyone in the population regardless of the presence or absence of a biomarker . 
because h1 was never chosen in this simulation , it is excluded from tables 2 and 3 ( data supplement )  . interpretation the results in tables 2 and 3 show that bapofi and cs - i performed the best in both scenarios . 
bapofi , in particular , correctly identied the beneting subgroup , and only the beneting subgroup , 100% of the time for both scenarios . all methods correctly identied the beneting subgroup the vast majority of the time in both scenarios . 
this table shows the probability ( under repeat simulation ) of x2 b for scenario 1 , that is , a future patient with the indicated baseline covariates x being included in the reported subgroup . 
for berger and wang11 ( bw ) , the rst number refers to all patients who would be recommended for treatment , and the number in parentheses refers to the patients who would be designated as beneting most . 
the table shows the probability ( under repeat simulation ) of x2 b for scenario 2 , that is , a future patient with the indicated baseline covariates x being included in the reported subgroup . 
for berger and wang11 ( bw ) , the rst number refers to all patients who would be recommended for treatment , and the number in parentheses refers to the patients who would be designated as beneting most . 
the column e ( n ) shows the expected number of patients with the respective covariates according to the simulation truth . abbreviations : bapofi , bayesian population nding ; cs - e , credible subgroups ( exclusive subset ) ; cs - i , credible subgroups ( inclusive subset ) ; ds , dixon and simon3 ; pu , polya urn . * covariate combinations that correspond to an enhanced treatment effect under the simulation truth . some of the methods were more prone to identifying a larger subset . 
this is probably because it allows all possible combinations and does not include any penalty for identifying small or awkwardly described groups or for lack of parsimony . as noted , some of the methods explicitly only allow for subgroups dened by one covariate ( bw ) , combinations of subgroups dened by one covariate ( pu ) , or two covariates ( bapofi )  . 
when evaluating their performance , keep in mind that the simulation truth for both scenarios happens to fall within the restricted scope of these methods , with the exception of bw for scenario 2 ; the version of bw implemented in this simulation does not take into account prognostic effects , although it could be set up to do so . because of the nature of the models that are considered in bw , the model that usually wins is the model that nds an enhanced treatment effect for both patients with x13 ( cid : 1 ) 1 and for patients with x13 ( cid : 1 ) 0 . 
bapofi avoided this problem by explicitly including a penalty for complexity . all of these methods can easily be extended to include more covariates and can be modied to include interaction structures . 
however , because each method is geared toward a slightly different aim , it becomes difcult to directly compare them when the data become more complicated . as a result , it becomes more important to specify the aim of the analysis . 
it is useful to distinguish different types of subgroup - based designs , as shown in figure 2 . traditional two - step process the standard subgroup - driven clinical development consists of at least two clinical trialsan exploratory trial for subgroup nding and a conrmatory trial for efcacy conrmation in the identied subgroup . 
the rst is a one - stage subgroup enrichment design , 25 in which one would prospectively specify the subgroups that the new therapy is expected to benet . such subgroup enrichment designs recruit patients from prespecied subpopulations and do not modify the inclusion criteria during the trial . 
however , a sponsor may be primarily interested in a large at - risk population and may consider a biomarker - stratied design that recruits patients from a larger subpopulation , or even the whole patient population ( denoted as f ) , and then includes patient strata ( denoted as s )  . 
the objective of the biomarker - stratied designs is to demonstrate the efcacy of the treatment in f and , if the rst objective fails , to demonstrate the efcacy of in s . 
because there are multiple tests , the treatment a multiple testing procedure can be used to control the the null hypotheses of nofamily - wise error treatment effect in s and in f .26 - 28 rate for conrmatory adaptive subgroup enrichment designs to improve the probability of success in drug development and to speed up the process , several authors have proposed conrmatory adaptive subgroup enrichment designs for phase ii and iii trials.18 - 20 , 29 - 31 in such designs , the trial is divided into several stages with possible subpopulation enrichment after each interim analysis , such as restricting future enrollment to only those subgroups that seemed to be benetting from the experimental therapy . 
on the basis of the results of each interim analysis , the trial may continue as initially planned , be stopped early , or continue with adaptive modications ( eg , revision of recruitment clusion criteria or sample size reestimation )  . 
in the absence inference is conducted to test of enrichment , statistical whether there is a signicant treatment effect in the whole population or in any of the predetermined subgroups . 
the family - wise error rate is controlled by closed testing principles in the strong sense . bayesian tools can be used in the go / no - go decision for the original population or specic subgroups . 
for example , brannath et al19 developed a decision tool on the basis of predictive probabilities for rejecting certain null hypotheses to determine which of two populations , the full population or subpopulation , should be further investigated in the second stage . 
this approach has been applied to an oncology phase ii / iii trial.32 seamless exploratory and conrmatory trials one may also consider combining the exploratory trial and the conrmatory trial seamlessly . 
the subgroups and decision rule be prespecied . in simon and simon , 21 a class of adaptive subgroup enrichment designs is proposed that adaptively update the eligibility criteria without prespecied subgroups . 
this test preserves the type i error regardless of the method used for making enrichment decisions and regardless of , possibly data dependent , time trends in the characteristics of the patients . subgroup estimation will be reported at the nal analysis for regulatory labeling . 
simon and simon22 extended their previous designs21 by incorporating bayesian decision tools into the interim decision making for enrichment and bayesian inference for the treatment effect in the estimated subgroup . 
although the hypothesis testing is statistically sound in both approaches by simon and simon , 21 , 22 the the overall null hypothesis is rejected , treatment effect in the estimated subgroup may be subject to a resubstitution bias . 
to correct for the resubstitution bias in estimating treatment efcacy for the selected subgroup , zhang et al33 propose cross - validation and bootstrap methods . exploratory adaptive enrichment designs some recent literature has developed exploratory adaptive enrichment designs23 , 24 with response - adaptive randomization . 
xu et al23 proposed a bayesian subgroupbased adaptive design ( suba ) using a random partition model for continuous biomarkers ( x ) and binary outcome ( y )  . 
for an example of suba applied to a real - world trial , see the article by simon et al.34 this is an ongoing trial at northshore biomarker 2 biomarker 1 biomarker 1 round 1 biomarker 2 d 2 biomarker 2 round 3 biomarker 2 ss11 sl11 ll12 ls12 ll12 lss121 lsl121 biomarker 1 biomarker 1 fig 3 . 
 nugent et al university health system , which adopts suba for adaptive allocation of patients to the best treatment arm on the basis of posterior predictive probabilities . another adaptive enrichment design for a basket trial of targeted therapies across multiple cancers is discussed in the article by xu et al.35 the design is based on an approach similar to that of morita and m uller , 14 with subgroups dened by binary covariates that include biomarkers and tumor types . discussion we have reviewed several approaches to bayesian subgroup analysis . 
alternatively , an investigator might be mainly interested in an informed individualized treatment choice , in which case an approach that allows for more complex subgroups , such as the potential outcomes approach , might be preferred . 
focusing on the nature of the subgroup as a random quantity enables investigators to explicitly describe the uncertainty of the subgroup report and to make an informed choice to be more or less conservative . a common context for subgroup analysis is the planning of future trials or the closely related problem of adaptation in a current trial . 
an interesting aspect of this application is that one can use bayesian inference to nd an interesting subpopulation but can then proceed with a purely frequentist design for the trial . planning for future trials is not the only application . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . wentian guo employment : laiya consulting stock and other ownership interests : laiya consulting travel , accommodations , expenses : laiya consulting peter m uller consulting or advisory role : novartis yuan ji stock and other ownership interests : laiya consulting , laiya consulting ( i ) consulting or advisory role : astellas pharma no other potential conicts of interest were reported . references robert c : the bayesian choice . 
new york , ny , springer - verlag , 2007 jones he , ohlssen di , neuenschwander b , et al : bayesian models for subgroup analysis in clinical trials . 
biom j 43 : 581 - 589 , 2001 jenkins m , stone a , jennison c : an adaptive seamless phase ii / iii design for oncology trials with subpopulation selection using correlated survival endpoints . pharm stat 10 : 347 - 356 , 2011 30 . 
martn m , chan a , dirix l , et al : a randomized adaptive phase ii / iii study of buparlisib , a pan - class i pi3k inhibitor , combined with paclitaxel for the treatment of her2 - advanced breast cancer ( belle - 4 )  . 
simon kc , tideman s , hillman l , et al : design and implementation of pragmatic clinical trials using the electronic medical record and an adaptive design . jamia open 1 : 99 - 106 , 2018 35 . 
 wide and cystic brain metastases reveal ret - rearranged nonsmall - cell lung cancers francesco facchinetti , md , msc1 , 2 ; francesca bozzetti , md1 ; letizia gnetti , md1 ; roberta minari , phd1 ; pellegrino crafa , md1 ; sara elena rebuzzi , md1 ; roberto ferrara , md3 ; elisa gruppioni , phd4 ; elisa capizzi , phd4 ; ermanno giombelli , md1 ; girolamo crisi , md1 ; annalisa altimari , phd4 ; and marcello tiseo , md , phd1 , 5 introduction the detection of specic molecular activations ( eg , egfr , alk , ros1 , braf , met , ret ) is the basis of effective targeted treatments in nonsmall - cell lung cancer ( nsclc ) .1 in this eld , novel selective inhibitors extend survival outcomes , coupling global prolonged disease control and meaningful activity against metastases developing in the cns.2 lung tumors harboring egfr mutations or alk , ros1 , or ret rearrangements have a tendency toward more frequent cns spreading compared with wild - type ( wt ) nsclc.3 - 5 peculiar neuroradiologic characteristics have been reported for brain metastases from alkpositive nsclc , in terms of cystic aspects acquired after crizotinib treatment.6 - 8 such features can even be misleading , because intracranial cystic lesions from alk - rearranged tumors may be attributed to infectious diseases.9 here we report the histories of two patients presenting with wide cystic brain lesions that were neurosurgically removed and discovered to be metastases from ret - rearranged nsclc . 
brain computed tomography ( ct ) scan and magnetic resonance imaging ( mri ) were performed , documenting a unique bulky cystic - like lesion in the frontal region of the left hemisphere , the morphologic and functional characteristics of which were pathognomonic for an anaplastic astrocytoma ( fig 1 )  . 
a chest x - ray revealed a parahilar lesion of the left lung . diagnosis and staging neurosurgery was then performed with the radical removal of the wide cerebral lesion , the intraoperative macroscopic aspects of which were still in keeping with an anaplastic astrocytoma . 
the postoperative course was uneventful , with a rapid neurologic improvement . the histologic examination revealed a large ( 40 25 20 mm ) lesion , conrming the cystic structure that was evident at sampling ( fig 2a )  . 
ct and pet scans revealed a mass in the left pulmonary hilum and ipsilateral and contralateral lymph nodes ( ct4n3m1b according to tnm staging classication [ eighth edition ] ; fig 3 )  . 
considering the radiologic , pathologic , and molecular elements , which were clearly in line with a diagnosis of advanced nsclc , biopsies of the lung and nodal lesions were not performed . molecular analyses neither the molecular analyses nor ihc performed on the brain metastasis detected egfr , braf , or kras mutations or alk or ros1 rearrangements ; programmed death - 1 ligand ( clone sp263 ) was expressed by 10% of tumor cells . 
next - generation sequencing with a 52 - gene panel ( ion torrent oncomine focus assay kit ; thermo fisher scientic , waltham , ma ; gene list provided in data supplement ) was performed , and a kif5b - ret fusion was found ( figs 4a and 4b )  . 
ret rearrangement was conrmed by uorescence in situ hybridization analysis in 52% of tumor cells ( fig 4c )  . treatment received rst - line chemotherapy with the patient cisplatin and pemetrexed . 
postoperative stereotactic brain radiotherapy ( sbrt ) to the resection cavity was not performed , because available evidence supporting sbrt for better local control has not yet indicated a survival benet.10 , 11 brain mri after 4 months revealed normal surgical outcomes , with no residual disease . 
ct scan after four courses of cisplatin plus pemetrexed showed partial disease response , so the patient was switched to pemetrexed maintenance , four cycles of which led to further reduction of lymph node size , with continuing absence of brain disease on mri . 
no evidence is available concerning ret - rearranged nsclc , an entity of emerging interest given the current development of selective ret inhibitors , also active against cns disease . knowledge generated here we report the similar clinical histories of two patients with ret - positive nsclc , whose diagnoses were obtained on pathologic and molecular analyses performed on wide , cystic , and symptomatic brain metastases with a peculiar neuroradiologic presentation . relevance a characteristic behavior of cns lesions from ret - rearranged nsclc was recognized . 
the current or upcoming availability of selective , cns - active ret inhibitors strongly reinforces the importance of wide molecular screening of cns lung metastases , even more so in the presence of the reported neuroradiologic and pathologic features of brain lesions . the abrupt onset of dizziness , worsening headache , difculty with handgrip , and right homonymous hemianopsia . the observation of a large and cystic - like brain lesion in the left parietal - occipital region was followed by a contrastenhanced mri ( fig 5 )  . 
the brain imaging was suggestive for metastases from an extracerebral tumor . diagnosis and staging the whole - body ct scan documented a mass in the upper left lung lobe , with ipsilateral and contralateral nodal volvement in the hilar - mediastinal and retro - clavicular regions ( fig 6 ) , with clinical staging determined as ct2an3m1c . given the persisting neurologic symptoms , the patient underwent neurosurgery . the pathologic examination conrmed the radiologic hypothesis of a cavitated cystic ( fig 2f ) brain metastasis ( 40 30 20 mm ) from a lung tumor ( figs 2g to 2i )  . 
 ( a ) t1 weighted imaging ( wi ) and ( b ) t2 wi sequences show a well - delineated ( a ) hypointense and hyperintense mass in left frontal lobe cortex involving the subcortical area and deep white matter , ( c ) without dense dystrophic calcication or hemosiderin staining on t2 * gre . 
 ( d ) ttf - 1 ( 40 ) and ( e ) napsin a ( 40 ) immunohistochemistry showed diffuse ( d ) nuclear and ( e ) cytoplasmic positivity . 
 ( a ) a left parahilar lesion conditioning atelectasis was detected , together with ( b ) ipsilateral and ( c ) contralateral pathologic lymph nodes . elements supporting the diagnosis of nsclc , biopsies of the primary tumor and lymph nodes were not proposed . molecular analyses status of egfr , alk , ros1 , kras , braf , and met was found to wt , and ihc showed programmed death - 1 ligand ( clone sp263 ) negative status . 
again , targeted ngs was performed on the brain metastasis ( ion torrent oncomine focus assay kit ; thermo fisher scientic ; data supplement ) , and kif5b - ret fusion was revealed , conrmed by uorescence in situ hybridization analysis in 40% of tumor cells ( figs 4a to 4b and 4d )  . treatment because of the lack of trials with ret inhibitors in the rstline setting and the substantial benet potentially driven by pemetrexed , 12 pemetrexed was combined with cisplatin and administered as a rst - line treatment , once postsurgical recovery was complete . 
again , sbrt to the resection cavity was discussed but not performed , for the same reasons reported in the rst patient case15 , 16 and because of the presence of multiple brain metastases . 
 ( b ) next - generation sequencing analysis report showing the ret fusion with kif5b gene ( ion reporter software and irgv visualization [ thermo fisher scientic , waltham , ma ] ) detected in brain samples from patient cases 1 and 2 . 
t1 weighted imaging ( wi ) and t2 wi sequences show a well - delineated ( a ) hypointense and ( b ) hyperintense mass in left occipital lobe cortex , with a linear internal septum , involving the subcortical area and deep white matter , ( c ) without dense dystrophic calcication or hemosiderin staining on t2 * gre . 
 ( d ) axial t1 postcontrast imaging shows a large bilobed cystic - like supratentorial mass with ring enhancement , sharply delineated borders , and well - dened internal septu ( e ) the content is liquid , with no intralesional levels and with high diffusivity ( apparent diffusion coefcient , 0.00269 mm2 per second v csf , 0.00290 mm2 per second )  . 
similar radiologic appearance is shown by the following : ( g ) t1 wi before gadolinium administration , ( h ) t1 wi after gadolinium administration , and ( i ) t2 wi . imaging documented , in addition to the regular outcomes of the surgical intervention , signs of response in the two residual lesions ( data not shown )  . 
nevertheless , this was not conrmed in another series of ros1 - rearranged lung cancer with baseline brain involvement ; in that series , the ros1 partner gene was known in 17 patients for whom mri results were available.14 in ret - driven lung cancer , the most frequent fusion partner gene is kif5b , as observed in the two patient cases reported here . 
although no associations between ret partner genes and brain metastasis incidence have been anticipated , drilon et al5 reported that intracranial disease response to multitarget kinase inhibitors seemed to occur specically in nonkif5b - ret patient cases ( n = 2 of 5 ) , with no responses in the kif5bret patient cases ( n = 0 of 9 ) .5 at least ve cns responses to the selective ret inhibitor loxo - 292 were observed in ret - rearranged lung tumors ( n = 4 of 4 in the phase i study ) 15 , 16 harboring either kif5b ( n = 2 ) or non - kif5b ( clip - 1 ; n = 1 ) ret partner genes.15 - 17 because of the descriptive nature of our patient cases , no conclusion can be drawn with regard to a novel specic pattern of ret - rearranged lung tumors , potentially associated with large and cystic - like brain metastases at diagnosis . nevertheless , besides providing atypical and intriguing radiologic ndings , the surprising similarity between these two reports , together with the rarity of ret rearrangements in nsclc , suggests a characteristic behavior of cns lesions from this molecular subclass of tumors . 
these observations reinforce the importance of screening for nsclc molecular activations in addition to the canonical and frequent ones , with particular reference to ret fusions in the presence of atypical features of brain metastases . 
 ( a - c ) the lesion was not dissociable and was not completely distinguishable from an obstructive inammatory / atelectasic consolidation involving the entire lingula and part of the upper left lobe . 
 ( c , d ) bilateral hilar , mediastinal , and retro - clavicular lymph nodes were reported ( white arrows )  . involvement , with special regard to novel , specic agents , such as loxo - 292 and blu - 667.5 , 15 - 18 we hope that our two patients will not require further systemic treatment , meaning that their disease is controlled with the current chemotherapy and potential administration of radiotherapy . 
 large and cystic brain metastases from ret - rearranged nsclcs references reck m , rabe kf : precision diagnosis and treatment for advanced non - small - cell lung cancer . 
n engl j med 377 : 849 - 861 , 2017 remon j , besse b : brain metastases in oncogene - addicted non - small cell lung cancer patients : incidence and treatment . 
front oncol 8 : 88 , 2018 tan l , wu y , ma x , et al : a comprehensive meta - analysis of association between egfr mutation status and brain metastases in nsclc . 
pathol oncol res 25 : 791 - 799 , 2019 gainor jf , tseng d , yoda s , et al : patterns of metastatic spread and mechanisms of resistance to crizotinib in ros1 - positive nonsmall - cell lung cancer . 
j clin oncol 32 : e122 - e124 , 2014 saraceni c , li pm , gainor jf , et al : cystic brain metastases in nsclc harboring the eml4 - alk translocation after treatment with crizotinib . 
narayanan v , honce mj , mehrotra s , et al : cystic brain metastases occurring in anaplastic lymphoma kinase gene rearranged non - small - cell lung cancer patients receiving crizotinib . 
clin lung cancer 17 : 85 - 90 , 2016 kim sh , hyun jw , kim hj , et al : de novo cystic brain lesions mimicking neurocysticercosis in alk - positive lung cancer . 
mahajan a , ahmed s , mcaleer mf , et al : post - operative stereotactic radiosurgery versus observation for completely resected brain metastases : a single - centre , randomised , controlled , phase 3 trial . 
patil t , smith de , bunn pa , et al : the incidence of brain metastases in stage iv ros1 - rearranged non - small cell lung cancer and rate of central nervous system progression on crizotinib . 
drilon a , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
oxnard g , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer . 326 , 2013 27 : 1286 - 1291 , 2016 j thorac oncol 13 : 987 - 995 , 2018 oncol 36 , 2018 ( suppl ; abstr 102 ) j thorac oncol 13 : s349 - s350 , 2018 17 . 
a computed tomography ( ct ) scan of the abdomen revealed a 7.5 - cm head of pancreas mass encasing the celiac and superior mesenteric arteries and the portal vasculature , with dilation of the pancreatic and common bile ducts ( fig 1a )  . 
completion staging with a ct scan of the chest was negative . the patient , with locally advanced unresectable pancreatic ductal adenocarcinoma ( pdac ) , was administered a chemotherapy regimen of fluorouracil , folinic acid , irinotecan , and oxaliplatin on april 8 , 2016.1 after 4 cycles of treatment , restaging ct showed progression of the primary tumor ( fig 1b ) with an increase in cancer antigen 19 - 9 from 202 to 410 ( fig 3 ) and clinical deterioration requiring duodenal stent and gastrostomy tube placement . 
given his young age , his otherwise good health and lack of expected risk factors , and his family history , comprehensive multiomic molecular analysis was performed by perthera , a precision oncology company in mclean , va , that facilitates molecular testing and provides patients with a list of therapy options that match their molecular profile , the specific characteristics of their tumor , and their treatment history . 
all molecular testing , which includes multiomic analysis , is performed at college of american pathologist ( cap ) and clinical laboratory improvement amendment ( clia ) accredited and licensed laboratories and is commercially available ( foundation medicine , cambridge , ma , for nextgeneration sequencing ( ngs ) analysis and caris life sciences ( irving , tx ) for multiplexed proteomic immunohistochemistry [ ihc ] and fluorescent in situ hybridization [ fish ] analysis )  . before providing its services to this patient , perthera obtained informed consent under an institutional review boardapproved registry protocol . as part of the perthera analysis , a clia - certified / cap - accredited commercial ngs - based test ( foundationone ; foundation medicine ) revealed the anaplastic lymphoma kinase ( alk ) rearrangement , recurrent striatin ( strn ) - alk . 
in addition , a clia - certified and capaccredited commercial ihc test ( caris molecular intelligence ; caris life sciences ) revealed overexpression of the alk protein ( fig 2d ) , which confirmed genomic alteration at the protein level . fish testing was not performed . as a result of this finding , treatment options included standard second - line chemotherapies with or without radiation , as well as the possibility of adding crizotinib . 
after conferring with multiple colleagues , it was decided to treat the patient with intensity - modulated radiotherapy ( 60 gy in 2 - gy fractions , from june 23 , 2016 , to august 5 , 2016 ) , concurrent gemcitabine ( 600 mg / m2 / wk ) for 6 weeks , and crizotinib ( 250 mg twice a day ) for the duration of radiotherapy . 
joseph bender emanuel petricoin jonathan brody nicholas nissen richard tuli , simon lo , jaimie koo , and nicholas nissen , cedars - sinai medical center , los angeles , ca ; and michael pishvaian , r . 
computed tomography of the abdomen ( a ) with venous phase contrast pretreatment ; ( b ) after first - line therapy with fluorouracil , folinic acid , irinotecan , and oxaliplatin ; ( c ) 6 weeks after gemcitabine , radiotherapy , and crizotinib ; and ( d ) after 3 months of additional crizotinib . 
restaging ct on september 26 , 2016 , showed significant partial response of tumor ( fig 1c ) with a commensurate decline in cancer antigen 19 - 9 to 25 ( fig 3 )  . 
cancer antigen ( ca ) 19 - 9 values ( a ) after first - line therapy with fluorouracil , folinic acid , irinotecan , and oxaliplatin ; ( b ) after gemcitabine , radiotherapy , and crizotinib ; and ( c ) after approximately 5 months of additional crizotinib . status , suggesting a persistent response to crizotinib combination and single - agent therapies . 
one such targetable oncogenic driver is the alk rearrangement identified in 3% to 5% of nsclcs.4 initially identified by soda et al , 5 a small inversion within chromosome 2p resulted in the formation of a fusion gene comprising portions of the echinoderm microtubule - associated protein - like 4 gene and the alk gene in nsclc . 
archival analysis of 140 pdacs for alk1 expression using ihc and fish was negative in all cases , suggesting that alk is an unlikely therapeutic target in pdac.6 using panel - based multiplexed genomic and proteomic profiling , we were able to identify this actionable mutation previously undetected using standard ihc / fish ( fig 2d )  . 
if the strn gene is a preferred fusion partner of alk in pdac , this may provide an explanation for the negative fish results in the study by graham et al.6 therefore , any pdac case without an identifiable kras driver mutation should be considered for multiplexed sequencingbased testing to identify potential additional drivers , including alk rearrangements . functional alk rearrangements have been found largely to be mutually exclusive of oncogenic driver mutations such as egfr and kras mutations in nsclc.4 although kras mutations serve as oncogenic drivers in 90% of pdacs , our patients tumor did not harbor this mutation . 
in addition , clinical and pathologic variables unique to alkrearranged nsclc include young age , prominent mucinous cells ( adenocarcinoma subtype ) , and never - smokers.8 the young age of our patient in the absence of any risk factors is perhaps suggestive of alk - mediated tumorigenesis , especially given that the median age of patients with pdac is 71 years . patients with alk - rearranged nsclcs are extremely responsive to the tyrosine kinase inhibitors crizotinib and ceritinib.4 the recent phase 3 profile 1014 study ( a clinical trial testing the efficacy of crizotinib versus standard chemotherapy pemetrexed plus cisplatin or carboplatin with alk positive non squamous cancer of the lung ) established crizotinib as standard first - line therapy for patients with metastatic nonsquamous nsclc , with an objective response rate of 74% and progressionfree survival of 11 months , both of which were significantly higher than in standard platinumbased doublet chemotherapy.9 despite a relatively durable response to tyrosine kinase inhibitors , patients ultimately develop resistance to therapy . 
in addition to kras - activating mutations , inactivation of tumor suppressors tp53 , cdkn2a , and smad4 occur at 50% frequency , followed by aberration of genes related to dna damage repair , chromatin remodeling , and others at a much lower frequency.10 using whole - genome sequencing and copy number variation , a recent study identified an average of 119 variations in chromosomal structure per pancreatic cancer , further highlighting this diversity.11 indeed , this diverse intertumoral heterogeneity warrants genomic profiling to increase the likelihood of identifying druggable targets , as noted in the described case . 
although kras is a difficult driver mutation to target therapeutically , many other drivers , such as the alk fusion detected here , have been demonstrated to sensitize tumors to therapies . 
taken together with our previous observation that kras wild - type tumors are enriched for braf mutations and erbb2 amplifications , this suggests that kras wildtype pdac cases have a high potential for sensitivity to molecularly targeted therapies . our patient harbored fusion of strn - alk , which has been characterized previously in multiple other malignancies , including colon , breast , renal , and lung cancers , among others.12 - 14 an alk fusion has been observed in one case of pdac , but with a different fusion partner ( dctn1 ) .15 notably , the case with the dctn1alk fusion also lacked a kras mutation . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . richard tuli no relationship to disclose simon lo no relationship to disclose jamie koo no relationship to disclose michael pishvaian stock and other ownership interests : perthera honoraria : caris life sciences , celgene , sirtex medical consulting or advisory role : caris life sciences , perthera , celgene , sirtex medical research funding : genentech ( inst ) , celldex ( inst ) , merck ( inst ) , daiichi sankyo ( inst ) , glaxosmithkline ( inst ) , medimmune ( inst ) , pfizer ( inst ) , gilead sciences ( inst ) , regeneron pharmaceuticals ( inst ) , novartis ( inst ) travel , accommodations , expenses : caris life sciences , sirtex medical , perthera r . 
 emanuel petricoin leadership : perthera , ceres nanosciences stock and other ownership interests : perthera , ceres nanosciences , d3d consulting or advisory role : perthera , ceres nanosciences , zymeworks research funding : ceres nanosciences ( inst ) , glaxosmithkline ( inst ) patents , royalties , other intellectual property : national institutes of health patents licensing fee distribution or royalty , university - assigned patent licensing fee or royalty travel , accommodations , expenses : perthera , ceres nanosciences jonathan brody employment : perthera stock and other ownership interests : perthera consulting or advisory role : perthera research funding : american association for cancer research , national institutes of health expert testimony : king and spalding llp travel , accommodations , expenses : perthera nicholas nissen no relationship to disclose references med 364 : 1817 - 1825 , 2011 1 . 
vogelzang nj , benowitz si , adams s , et al : clinical cancer advances 2011 : annual report on progress against cancer from the american society of clinical oncology . 
von hoff dd , ervin t , arena fp , et al : increased survival in pancreatic cancer with nab - paclitaxel plus gemcitabine . n engl j med 369 : 1691 - 1703 , 2013 4 . 
gainor jf , varghese am , ou sh , et al : alk rearrangements are mutually exclusive with mutations in egfr or kras : an analysis of 1 , 683 patients with non - small cell lung cancer . 
kelly lm , barila g , liu p , et al : identification of the transforming strn - alk fusion as a potential therapeutic target in the aggressive forms of thyroid cancer . 
 first case report of a dramatic radiographic response to a checkpoint inhibitor in a patient with proficient mismatch repair gene expressing metastatic colorectal cancer metastatic colorectal cancer ( mcrc ) remains the second most common cause of cancer death in the united states , and therapeutic options are limited . 
recently , the checkpoint inhibitor pembrolizumab was given the food and drug administration breakthrough therapy designation for the treatment of patients with mcrc whose tumors demonstrate deficient mismatch repair gene ( dmmr ) expression ( as evidenced by microsatellite instabilityhigh [ msi - h ] )  . 
the designation was based on a phase ii study showing that in patients with dmmr , an objective response rate of 40% was seen , whereas in patients with proficient mismatch repair gene mcrcs , the response rate was 0% . 
because this patients tumor harbored amplification of both the pd - l1 and pd - l2 genes , the observed response was consistent with the presumed mechanism of action of checkpoint inhibitors . 
pathology showed stage iiib ( t4bn1mx ) colonic adenocarcinoma , and a computed tomography ( ct ) scan of the chest , abdomen , and pelvis in december 2014 showed no evidence of metastatic disease . 
 ( pd - l1 ) and the pdcd1lg2 ( pd - l2 ) gene , normal sequence of mlh1 , msh2 , msh6 , and pms2 , and no microsatellite instability ( msi )  . 
the msi test performed by foundation medicine has been validated against currently accepted methods of testing msi , including immunochemical ( ihc ) and polymerase chain reaction , with a concordance of 97% in 60 colorectal and endometrial cancers . 
immunohistochemical assay demonstrated retained nuclear expression of mlh1 , msh2 , msh6 , and pms2 ( department of pathology , baptist hospital and wake forest medical school , winston - salem , nc )  . on january 27 , 2016 , the patient began receiving intravenous nivolumab ( 3mg / kg ) every 2 weeks , and after six doses , a repeat ct chest , abdomen , and pelvis scan on april 13 , 2016 , showed not only improvement in the previously radiated area , but also , as the radiologist noted , other multiple previously described lymph nodes as well as multiple subcutaneous soft tissue nodules and a few small pulmonary nodules had either resolved or considerably decreased in size compared with the most recent examination . 
she continued receiving the nivolumab , and a further response was documented in july 2016 when a ct scan showed only one , further diminished , left posterior subcutaneous nodule remaining , and again no new lesions . discussion the programmed death pathway represses a cytotoxic immune response to tumors . 
checkpoint inhibitors are thought to activate that cytotoxic pathway by inhibiting the programmed death pathway ligands ( pd - l1 and pd - l2 ) .4 , 5 in non small - cell lung cancer , the expression of these ligands predicts responsiveness . 
as a result , the food and drug administration ( fda ) has approved different ihc assays for pd - l1 expression to be used in deciding whether to treat patients using the checkpoint inhibitors approved for lung cancer treatment.6 in mcrc , pd - l1 or pd - l2 expression or gene amplification have not been studied as a marker of responsiveness to the checkpoint inhibitors , although pd - l1 and pd - l2 overexpression has been assessed in deficient mismatch repair gene ( dmmr ) expression and proficient mismatch repair gene ( pmmr ) colon cancers and are associated with prognosis in these cancers.7 yet the basis for the recent fda breakthrough designation of the checkpoint inhibitor pembrolizumab was the result of a study in which the investigators hypothesized that dmmr mcrc would respond to checkpoint inhibitors because these tumors are known to overexpress pd - l1 and pd - l2 far more commonly . 
in fact , in this study , pdl - 1 expression occurred only in dmmr tumors , not in pmmr tumors . le et al8 used msi - h as a surrogate for dmmr ; if msi - h is identified , the same colorectal tumor nearly always demonstrates dmmr , 9 still , it is known that pmmr crcs ( colorectal cancers ) may overexpress pd - l1 or pd - l2 , and that certain clinical features ( eg , tumors with vascular invasion ) might predict this pattern.5 , 10 expression may correlate more closely with the mutation frequency in the tumors , which is characteristically far higher in dmmr crc cases compared with pmmr crc cases.1 pd - l1 or pd - l2 amplification ( as in this case ) would not necessarily result in overexpression . 
however , given the mechanism of action of the checkpoint inhibitors and the dramatic response , and given that this patient had had progressive mcrc despite prior standard therapy , it seems reasonable to conclude that inhibition of pd - l1 and pd - l2 occurred and that that explains the robust response . there are important examples in which gene amplification without wild - type gene product overexpression nonetheless predicts benefit of drugs targeting the gene product . 
 similarly , defining a best test for identifying which patients are likely to benefit from checkpoint inhibitor therapy has been challenging . despite the fact that the results of assays for pdl - 1 and pdl - 2 expression , dmmr ( or msih ) , and mutational burden might not correlate with each other in an individual tumor , all have been shown to predict benefit from checkpoint inhibitor therapy for various malignancies.4 , 6 , 12 given the efficacy of the checkpoint inhibitor seen in our patient , one might predict her tumor to be msi - h ( despite the pmmr ) and / or to demonstrate a high mutational burden . 
regardless of that result , however , reports of tumors with pd - l1 or pd - l2 gene amplification and responsiveness to checkpoint inhibitors would be needed to confirm that gene amplification is another predictor of benefit from the targeting agent , as has been shown to be true for breast cancer , in which her2 ihc is negative but the her2 gene amplification independently predicts benefit . because this is a single case report , it should not be used as confirmation that pdl - 1 and pdl - 2 gene amplification is a confirmed predictor of responsiveness to checkpoint inhibitor therapy in crc . if additional responses of crcs in patients whose tumors show pmmr and pdl - 1 and pdl - 2 gene amplification are reported , consideration should be given to including patients with such tumors in trials aimed at identifying whether this molecular profile might serve as a predictive marker of likely responsiveness to checkpoint inhibitor therapy . in conclusion , the current fda breakthrough designation of checkpoint inhibitor therapy pertains only to mcrcs in patients whose tumors demonstrate dmmr ( as evidenced by msi - h )  . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . steven sorscher consulting or advisory role : merrimack speakers bureau : celgene jamie resnick no relationship to disclose first case report of a dramatic radiographic response to a checkpoint inhibitor in a patient with proficient mismatch repair gene expressing metastatic colorectal cancer the following represents disclosure information provided by authors of this manuscript . 
i = michael goodman stock and other ownership interests : exelixis consulting or advisory role : sanofi , alexion pharmaceuticals research funding : wake forest , veterans administration travel , accommodations , expenses : sanofi , alexion pharmaceuticals , jannsen pharmaceuticals references 1 . 
hall , mj , gowan k , sanford sm , et al : evaluation of microsatellite instability ( msi ) status in gastrointestinal ( gi ) tumor samples tested with comprehensive genomic profiling ( cgp )  . 
cicek ms , lindor nm , gallinger s : quality assessment and correlation of microsatellite instability and immunohistochemical markers among population - and clinic - based colorectal tumors results from the colon cancer family registry . 
droeser ra , hirt c , viehl ct , et al : clinical impact of programmed cell death ligand 1 expression in colorectal cancer . eur j cancer 49 : 2233 - 2242 , 2013 11 . 
gradishar wj , anderson bo , balassanian r , et al : breast cancer guideline in the national comprehensive cancer network guideline , harborside press , huntington , ny , version 2 . 
 targeted error - suppressed detection of circulating paternal dna to establish a diagnosis of gestational trophoblastic neoplasm introduction gestational trophoblastic neoplasms ( gtns ) are a family of pregnancy - related gynecologic malignancies that are derived from invasive placental trophoblast tissue and characterized by their secretion of human choriogonadotropin ( hcg )  . 
these neoplasms cover a wide spectrum of clinical and histologic presentations , from molar pregnancies to metastatic choriocarcinoma.1 whereas presentations vary , gtn is a highly curable disease , even for patients with poor - risk features . 
achieving favorable outcomes largely depends on accurate and timely diagnosis as well as close follow - up of the response to treatment.2 the case presented here illustrates the potential diagnostic challenges that are encountered when outcomes differ from initial expectations . 
clinical diagnosis of gtn was made as an international federation of gynecology and obstetrics stage iii and a risk score of 11term pregnancy , 4 - cm lesion , hcg  . 
as a result of her large burden of lung metastases , the patient received a short course of induction cisplatin and etoposide for 3 days.6 - 9 this led to a drop in hcg and the resolution of hemoptysis and vaginal hemorrhage . 
she then received first - line multiagent chemotherapy with etoposide , methotrexate , actinomycin d , cyclophosphamide , and vincristine ( ema / co ) for nine cycles , with a plateau in hcg that was suggestive of treatment resistance . 
switching to a paclitaxel , cisplatin , and etoposide ( tp / te ) salvage regimen resulted in the normalization of hcg . post - treatment monitoring detected an increase in hcg 4 weeks after the last dose of chemotherapy . induction chemotherapytwo cycles of tp / te followed by two cycles of high - dose chemotherapy with autologous stem - cell rescue were delivered , with the normalization of hcg . 
the patients hcg continued to rise , there was a recurrence of productive cough with blood - tinged sputum , and imaging confirmed the progression of multiple bilateral lung nodules , with no extrapulmonary disease . in the setting of progression after four lines of treatment , the possibility of an alternate diagnosis was entertained . 
the lack of a pathologic correlate opened the possibility of a non - gtn hcg - secreting malignancy , such as an occult gastric or bladder jean - michel lavoie miguel alcaide rosemary a . 
chemotherapy regimen used in the patient case reported regimen schedule dose ( per day ) ema / co ( 14 - day protocol ) etoposide actinomycin d methotrexate folinic acid rescue days 1 and 2 days 1 and 2 day 1 start 24 hours after methotrexate 100 mg / m2 0.5 mg iv bolus 300 mg / m2 15 mg iv every 12 hours vincristine cyclophosphamide day 8 day 8 tp / te ( 28 - day protocol ) paclitaxel days 1 and 15 carboplatin ( replaces day 1 cisplatin ) etoposide hdc / sct carboplatin etoposide autologous hematopoietic stem cells escalated ep ( 14 - day protocol ) etoposide cisplatin day 15 days 1 - 3 day 1 day 7 day 1 day 1 1 mg / m2 600 mg / m2 135 mg / m2 auc 5 150 mg / m2 550 mg / m2 2 , 250 mg / m2 500 mg / m2 60 mg / m2 note . 
escalated etoposide and cisplatin ( ep ) was administered with growth factor support for profilaxis of neutropenia . abbreviations : auc , area under the curve ; ema / co , etoposide , methotrexate , actinomycin d , cyclophosphamide , and vincristine ; hdc / sct , high - dose chemotherapy with autologous stem cell transplantation ; iv , intravenous . targeted hybridization capture and next - generation sequencing we pooled 250 ng of libraries from each partner and enriched them by using a panel of xgen lockdown probes ( integrated dna technologies , coralville , ia ) that targeted the exons of 83 genes according to the hybridization capture protocol provided by the manufacturer . 
the main purpose of this experiment was to select a few genetic polymorphisms to be used as biomarkers for the detection of paternal dna in the patients bloodstreain particular , we were interested in rare , paternally exclusive single - nucleotide polymorphisms ( snps ) or snps that were homozygous for the common allele in the patient , but heterozygous in her partner . 
we selected a panel of five snps ( table 2 ) and performed two successive rounds of hybridization capture using a personalized panel of xgen lockdown probes that targeted each one of the selected snps . enriched , dual - indexed libraries were sequenced in a miseq automated sequencer ( illumina , san diego , ca ) using pe 150 reads and analyzed according to previously reported methods.4 results we detected paternal cell - free dna in four of five markers investigated , all of them located on different chromosomes , at allele frequencies , 1% . all positive loci exhibited duplex sequencing support4 ( fig 3 )  . 
table 2 summarizes the snps that we used to track paternal - derived cell - free dna in the patients bloodstream , minor allele frequency ( according to the exac browser ) , 13 and the genotypes of the patient and her partner at each of the five genomic positions were investigated . given the presence of circulating paternal dna , diagnosis of gtn was confirmed . 
pretreatment hcg was 1 , 300 iu / l ; it briefly became undetectable , then stabilized under 10 iu / l . the patient remained stable on treatment of at least 18 weeks . discussion to our knowledge , this is the first patient in whom paternal dna could be detected at low ( , 1 , 000 iu / l ) hcg levels with high confidence . 
the number of molecules with duplex support and the total number of consensus sequences derived from individual dna strands that support each variant ( in parentheses ) is also indicated . 
mapping consensus sequences from individual dna strands against the reference reveals the presence of paternal - derived cell - free dna in the patients bloodstreatwo molecules with duplex support can be noticed . nucleotide disagreements with respect to the reference ( t ) are colored in green . 
the structure of a circulating tumor dna molecule with duplex support4 is also shown . 100100 210 214 12 - semidegenerate barcode 12 - semidegenerate barcode paternal - derived variant with duplex support strand - specific tags diagnosis of gtn . 
they used 15 primers for the detection of short tandem repeats on 13 different chromosomes , and sequenced cell - free dna in patients serum , maternal genome , paternal genome , and tumor tissue ( when available )  . 
all 14 confirmed cases had hcg levels of > 16 , 326 iu / l , whereas the 11 cases without detectable ctdna had hcg levels of < 14 , 884 iu / l . 
the use of semidegenerate barcoded adapters and biotinylated baits is an attractive option as it is potentially much more sensitive and , therefore , applicable in situations in which genotyping would be unlikely to yield a result . 
similar ultrasensitive methods for rare allele detection that rely on duplex sequencing have been used by kennedy et al14 and newman et al.15 in our case , targeted error - suppressed detection of circulating paternal dna obviated the need for a potentially high - risk biopsy of pulmonary disease , it was sensitive despite low hcg levels , and it was feasible within a clinically relevant timeframe of a few weeks . the advent of multiagent chemotherapy has led to gtn becoming a highly curable malignancy . proper diagnosis is paramount for directing treatment . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . jean - michel lavoie no relationship to disclose miguel alcaide no relationship to disclose rosemary a . 
seckl consulting or advisory role : bristol - myers squibb expert testimony : actavis travel , accommodations , expenses : bristol - myers squibb ryan morin consulting or advisory role : epizyme anna v . 
tinker consulting or advisory role : astrazeneca research funding : astrazeneca , medimmune other relationship : astrazeneca acknowledgment we thank our patient for kindly agreeing to have her case reported . jean - michel lavoie and anna v . 
openshaw mr , harvey ra , sebire nj , et al : circulating cell - free dna in the diagnosis of trophoblastic tumors . ebiomedicine 4 : 146 - 152 , 2015 4 . 
gillessen s , powles t , lim l , et al : low - dose induction chemotherapy with baby - bop in patients with metastatic germ - cell tumours does not compromise outcome : a single - centre experience . 
alifrangis c , agarwal r , short d , et al : ema / co for high - risk gestational trophoblastic neoplasia : good outcomes with induction low - dose etoposide - cisplatin and genetic analysis . 
bolze pa , patrier s , massardier j , et al : pd - l1 expression in premalignant and malignant trophoblasts from gestational trophoblastic diseases is ubiquitous and independent of clinical outcomes . 
 complete response to pd - 1 inhibition in an adolescent with relapsed clear cell adenocarcinoma of the cervix predicted by neoepitope burden and apobec signature anya levinson , md1 ; alex g . 
alejandro sweet - cordero , md1 , 2 ; and elliot stieglitz , md1 , 2 introduction utilization of checkpoint inhibition therapy in the management of malignant diseases is increasing . however , response to these therapies is highly variable , and robust predictive markers remain elusive . identication of predictive biomarkers is crucial considering the toxicities and high nancial cost associated with this approach . 
here , we report an adolescent with relapsed clear cell adenocarcinoma of the cervix ( ccac ) who experienced a complete response to checkpoint blockade despite not exhibiting positive pd - l1 immunohistochemical ( ihc ) staining , microsatellite instability ( msi ) , or a high tumor mutational burden ( tmb )  . 
biopsy of an exophytic mass protruding into the vagina conrmed a human papillomavirus / p16 - negative ccac ( fig 1 )  . family history was notable for paternal clear cell renal carcinoma . 
sixteen months after entering remission , surveillance positron emission tomography ( pet ) computed tomography ( ct ) revealed new hypermetabolic disease , including a new right upper lobe ( rul ) pulmonary nodule , enlarged prevascular right internal mammary , and right paratracheal nodes ( fig 2a ) and a left supraclavicular node . 
biopsy of the supraclavicular node conrmed recurrence of ccac ( fig 3 )  . her relapsed tumor exhibited 0% staining for pd - l1 by ihc , microsatellite stability ( 1 , 149 of 1 , 157 tested microsatellite regions were stable ) , and a low tmb ( 1.9 single nucleotide variants per megabase on wgs , less than the pediatric threshold of 2 ; appendix )  . 
genomic assays performed included targeted dna sequencing , wgs , and rna - seq ( appendix table a1 )  . a targeted institutional dna - seq panel assaying 479 cancer - relevant genes4 showed that both diagnostic and relapsed tumors had a broad approximately 11 - fold amplication on chromosome 20 containing aurora kinase a as a putative driver.5 the diagnostic sample also displayed a chromosome 1p deletion containing arid1a , a gene frequently mutated in cervical cancer , 6 which was absent at relapse . no pathogenic point mutations , insertions / deletions ( indels ) , or germline alterations were detected on this panel at diagnosis or relapse . 
pathologic conrmation of clear cell carcinoma of the cervix . ( a ) primary clear cell carcinoma of the cervix , showing hyperchromatic tumor cell nests in the stroma at left and normal endocervical glandular epithelium at the right ( 40 )  . 
 ( c ) an immunohistochemical stain for hepatocyte nuclear factor 1 - , which is a marker of clear cell carcinoma , shows strong positive nuclear staining in the tumor cells , a positive test result ( 200 )  . the rul pulmonary nodule and the prevascular lymph lymph nodes denode ( fig 2b )  . 
the median age was 53 years , and only three patients were , 30 years of age , 13 making the patient presented here one of the youngest patients ever reported with idiopathic ccac . 
 ( a ) patient developed a new hypermetabolic pulmonary nodule in the right upper lobe ( blue arrow ) , along with prominent hypermetabolic prevascular nodes ( red arrow )  . 
 ( b ) after initial nivolumab therapy , patients right upper lobe nodule decreased in size ( blue arrow ) , and the prevascular node had nearly resolved ( red arrow )  . 
 ( c ) approximately 16 months after initial recurrent disease , the pulmonary nodule has nearly completely resolved ( blue arrow ) , and no new pathologic nodes have developed . known biomarkers for response to checkpoint inhibition are ihc staining for pd - l1 , presence of msi , and high tmb . this patient , who achieved a complete and durable remission from checkpoint inhibition without any of these markers , highlights the need for additional biomarkers . 
we sought to analyze the genomics of her tumors to explain her dramatic response . somatic variations that give rise to amino acid substitutions in tumors yield neoepitopes , or mutated , tumor - specic peptides on the surface of cancer cells that can serve as neoantigens for the adaptive immune system , even if they are not oncogenic . 
determinants of neoantigen tness are the likelihood of their presentation by the major histocompatibility complex and of subsequent t - cell recognition.16 the number of neoepitopes per tumor can be more functionally relevant than the tmb . 
biopsy of supraclavicular node conrms metastatic disease . ( a ) metastatic clear cell carcinoma in a supraclavicular lymph node . the tumor cells line glands or grow in nests and are surrounded by lymphocytes , seen at the lower left ( 200 )  . ( b ) metastatic clear cell carcinoma in a supraclavicular lymph node . 
an immunohistochemical stain for pd - l1 shows minimal staining in the tumor cells and staining of scattered lymphoid cells around the tumor ( 200 )  . patients relapsed tumor , higher than that of available ( although biologically distinct ) comparison cohorts , supporting the idea that high neoepitope burden may predict favorable response to immunotherapy . 
of these , signatures 1 ( aging ) and 3 ( homologous recombination deciency ; appendix fig a4 ) are commonly found in cancer.18 , 19 signatures 2 and 13 represent activity of the aid / apobec family of enzymes.18 , 19 is associated with expression of apobec , a family of zinc - coordinating enzymes that convert cytosines to uracils , has been implicated in mutagenesis of nonsmall - cell lung cancer . 
systematic cancer genomic and transcriptomic association studies have shown that overexpression of one of the family members , apobec3b , immune genes and known immunotherapy response biomarkers such as pd - l1.20 a positive correlation was recently documented between strength of the apobec signature and the neoepitope burden in many cancers , including cervical.21 the authors also found that this mutational signature corresponded to increased abundance of tumorinltrating lymphocytes in some cancers , 21 although these were absent in this case . 
clinically , the apobec mutational signature is enriched in patients with durable clinical benet after immunotherapy , and an apobec signature may be better than tmb in predicting immunotherapy response.22 , 23 finally , there was a small contribution from signature 8 of uncertain etiology ( it is perhaps related to nucleotide excision repair deciency ) .24 the present patient is of interest for several reasons . 
box - and - whisker plots display the interquartile range ( box ) and outlier thresholds ( whiskers ) for the therapeutically applicable research to generate effective treatments neuroblastoma and the cancer genome atlas prostate adenocarcinoma data sets . 
although there may be other factors that contributed to the patients dramatic response , this case supports emerging evidence that a high neoepitope burden and an apobec mutational signature response to are potentially actionable biomarkers of checkpoint blockade . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . jessica van zife employment : adaptive biotechnologies ( i ) stock and other ownership interests : adaptive biotechnologies ( i ) patents , royalties , other intellectual property : adaptive biotechnologies ( i ) benjamin laguna leadership : sira medical stock and other ownership interests : sira medical stanley g . 
leung stock and other ownership interests : illumina , pzer , thermo fisher jacob pfeil employment : abbvie no other potential conicts of interest were reported . acknowledgment we thank the patient and her family for their willingness to share their experience using an unconventional treatment approach . 
naumann rw , hollebecque a , meyer t , et al : safety and efcacy of nivolumab monotherapy in recurrent or metastatic cervical , vaginal , or vulvar carcinoma : results from the phase i / ii checkmate 358 trial . 
european society for medical oncology meeting , barcelona , spain , september 27 - october 1 , 2019 ( abstr lba62 ) kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identies pathogenic germline mutations , and directs targeted therapy . 
curr oncol rep 15 : 566 - 572 , 2013 cho h , kim js , chung h , et al : loss of arid1a / baf250a expression is linked to tumor progression and adverse prognosis in cervical cancer . 
n engl j med 377 : 1345 - 1356 , 2017 rao aa , madejska aa , pfeil j , et al : protect : prediction of t - cell epitopes for cancer therapy . 
reich o , tamussino k , lahousen m , et al : clear cell carcinoma of the uterine cervix : pathology and prognosis in surgically treated stage ib - iib disease in women not exposed in utero to diethylstilbestrol . 
thomas mb , wright jd , leiser al , et al : clear cell carcinoma of the cervix : a multi - institutional review in the post - des era . 
boyd j , takahashi h , waggoner se , et al : molecular genetic analysis of clear cell adenocarcinomas of the vagina and cervix associated and unassociated with diethylstilbestrol exposure in utero . 
turajlic s , litcheld k , xu h , et al : insertion - and - deletion - derived tumour - specic neoantigens and the immunogenic phenotype : a pan - cancer analysis . 28 : 15 - 17 , 2019 lancet oncol 18 : 1009 - 1021 , 2017 18 . 
wang s , jia m , he z , et al : apobec3b and apobec mutational signature as potential predictive markers for immunotherapy response in non - small cell lung cancer . 
chen z , wen w , bao j , et al : integrative genomic analyses of apobec - mutational signature , expression and germline deletion of apobec3 genes , and immunogenicity in multiple cancer types . 
chen pl , roh w , reuben a , et al : analysis of immune signatures in longitudinal tumor samples yields insight into biomarkers of response and mechanisms of resistance to immune checkpoint blockade . 
boichard a , tsigelny if , kurzrock r : high expression of pd - 1 ligands is associated with kataegis mutational signature and apobec3 alterations . oncoimmunology 6 : e1284719 , 2017 jager m , blokzijl f , kuijk e , et al : deciency of nucleotide excision repair is associated with mutational signature observed in cancer . 
the lymph node from the patient was snap frozen and ffpe into optimal cutting temperature ( oct ) mediuall tissues were sectioned to a depth of 5 m and stained with hematoxylin and eossamples were evaluated for tumor content by a certied pathologist . 
rna integrity was quantied with the high sensitivity rna kit dnf - 472 ( advanced analytical technologies , orangeburg , ny ) on the fragment analyzer ( advanced analytical technologies )  . 
immunohistochemical pd - l1 staining was performed on tumor cells with the us food and drug administrationapproved pd - l1 28 - 8 pharmdx antibody for opdivo ( neogenomics laboratories , fort myers , fl )  . whole blood was collected during lymph node metastasectomy in a 4ml edta vacutainer . 
germline dna was extracted using the dneasy blood and tissue kit 69504 ( qiagen )  . dna was quantied using the nanodrop 2000 ( thermo fisher , waltham , ma ) and qubit high sensitivity dsdna assay q32851 ( thermo fisher ) and integrity quantied using the high sensitivity gdna kit dnf488 ( advanced analytical technologies ) on the fragment analyzer ( advanced analytical technologies )  . 
libraries from ffpe samples were made using the truseq rna access kit ( rs - 301 - 2001 ; illumina , san diego , ca ) with an input of 100 ng in accordance with manufacturers instructions . libraries from ffpe samples were made using the truseq stranded mrna kit ( rs - 122 - 2101 ; illumina ) with an input of 400 ng in accordance with manufacturers instructions . 
outliers ( ie , underor overexpression ) were identied using tukey outlier denition . targeted dna sequencing an institutional dna sequencing panel assaying 479 cancer - related genes was used.4 as per kline et al , 4 genomic dna was extracted from peripheral blood and tumor tissue microdissected from ffpe blocks . 
capture - based next - generation sequencing ( ngs ) was performed at the university of california , san francisco ( ucsf ) clinical cancer genomics laboratory , using an assay targeting the coding regions of these genes , tert promoter , select introns from 40 genes ( for detection of gene fusions and other structural variants ) , and intergenic regions at regular intervals along each chromosome ( for chromosomal copy number assessment ) , altogether with a total sequencing footprint of 2.8 mb ( ucsf500 cancer gene panel , appendix fig a2 )  . 
a list of genes included can be found at the following url ( although some genes may have been added or deleted since this patients analysis in 2017 ) : gene - panel - test - ucsf500 - uc500 . whole - genome sequencing libraries were generated using the truseq nano kit fc - 121 - 4001 ( illumina ) with a 350 - bp insert , per manufacturers instructions . 
libraries were made using 200 - ng input gdna , and then quantied on the tapestation 4200 ( agilent , santa clara , ca ) and sequenced on the hiseq x ten ( illumina ) using 2 150 bp paired - end reads . 
nonsynonymous variants were annotated using variant effect predictor ( mclaren w , et al : genome biol 17 : 122 , 2016 )  . predicted tumor neoepitope analysis we used the prediction of t - cell epitopes for cancer therapy ( protect ) pipeline v 2.6.18 to investigate the patients neoepitope burden . 
we compared the patients tumor mutation and neoepitope burden to publicly available protect data for the therapeutically applicable research to generate effective treatments neuroblastoma ( pmid : 23334666 ) and the cancer genome atlas prostate adenocarcinoma data sets ( pmid : 26544944 ) and assessed for signicance using tukeys outlier denition . apobec signature analysis single base substitution mutational signatures were extracted from the samples wgs data using deconstructsigs ( rosenthal r , et al : genome biol 17 : 31 , 2016 ) , with default parameters . 
the patients sample is notable for a signature 3 ( homologous recombination deciency [ hrd ] ) signature . violin plot of the fraction of mutations in each sample from ma et al11 attributed to signature 3 . 
reis - filho , md , phd1 ; diana mandelker , md , phd1 ; and britta weigelt , phd1 purpose endometrial cancer ( ec ) is not considered a component of the hereditary breast and ovarian cancer syndrome but can arise in patients with germline brca1 / 2 ( gbrca1 / 2 ) mutations . 
we sought to determine if ecs in gbrca1 / 2 mutation carriers harbor biallelic alterations and / or features of hrd . methods of 769 patients with ec who underwent germline panel testing , 10 pathogenic gbrca1 / 2 mutation carriers were identied , and their tumorand normal - derived dna was subjected to massively parallel sequencing targeting at least 410 cancer - related genes . 
somatic mutations , copy number alterations , loss of heterozygosity , microsatellite instability ( msi ) , and genomic hrd features were assessed . results of the 13 patients included who had ec , eight harbored pathogenic gbrca1 mutations and ve harbored gbrca2 mutations . 
 smith et al context key objective to determine if endometrial cancers ( ecs ) that arise in patients with pathogenic brca1 or brca2 germline mutations are sporadic cancers or display genomic features of homologous recombination dna repair deciency ( hrd ) , which may guide treatment strategies . knowledge generated ecs in patients with brca1 germline mutations showed biallelic brca1 alterations coupled with genomic features of hrd . 
in contrast , only a subset of ecs in brca2 germline mutation carriers harbored biallelic brca2 alterations ; the remaining cases were likely sporadic cancers . relevance knowledge about the brca1 / 2 allele status and / or hrd features of ecs in patients with germline brca1 / 2 alterations may guide therapeutic decision making , given that tumors with biallelic alterations in brca1 / 2 have been associated with increased response to hr - targeted therapies such as platinum salts and parp inhibitors . brca1 / 2 alterations and show features of hr deciency , including the catalog of somatic mutations in cancer mutational signature 3 , signature multivariate analysis ( sigma ) hr deciency signature sig3 , or large - scale chromosomal breaks in the form of large - scale state transitions ( lsts )  . 
in addition , we assessed the clinicopathologic data of ecs in gbrca1 / 2 mutation carriers and explored the repertoire of somatic mutations present in these tumors . methods case selection all patients with ec and gbrca1 / 2 mutations who consented to germline analysis under an institutional review boardapproved protocol at memorial sloan kettering cancer center and whose tumors were subjected to targeted massively parallel sequencing via memorial sloan ketteringintegrated mutation proling of actionable cancer targets ( msk - impact ) 10 , 11 from july 2015 to may 2019 were identied ( n = 769 sequenced ; n = 10 with pathogenic gbrca1 / 2 mutation )  . 
all gbrca1 / 2 variants were reviewed by a board - certied molecular pathologist ( d.m. ) and classied according to the american college of medical genetics and genomics criteria12 as pathogenic . clinicopathologic data , including age at diagnosis , cancer stage , and past cancer history , were obtained from medical records . 
mlh1 promoter methylation was assessed in the clinical setting on dna obtained from formalin - xed parafn - embedded tumor samples , as previously described.28 statistical analyses fishers exact and mann - whitney u tests were used for comparison of categorical and continuous variables , respectively . 
two - tailed p , 0.05 was considered statistically signicant . results clinicopathologic features of ecs arising in gbrca1 / 2 carriers ten ecs from patients with pathogenic gbrca1 / 2 mutations subjected to msk - impact sequencing ( n = 769 ecs ; 1.3% ) and three subjected to wes by tcga ( n = 232 ecs ; 1.3% ) 13 were included in this study . 
of these 13 gbrca1 / 2associated ecs , eight and ve patients with ec harbored gbrca1 and germline brca2 ( gbrca2 ) mutations , respectively ( table 1 )  . 
the majority of gbrca1 / 2 - associated ecs ( n = 6 of 8 ; 75% ) displayed an endometrioid histology ( n = 2 and 4 international federation of gynecology and obstetrics [ figo ] grades ii and iii , respectively ) but lacked a solid / pseudoendometrioid / transitional cell - like pattern of morphology , which has been associated with gbrca1 / 2 mutations in high - grade serous ovarian cancers.29 , 30 in contrast , ecs from patients with pathogenic gbrca2 mutations were more heterogeneous at the phenotypic level , and included endometrioid ( n = 1 ; figo grade ii ) , carcinosarcoma ( n = 2 ) , high - grade ec not otherwise specied ( nos ; n = 1 ) and serous ( n = 1 ) cancers ( tables 1 and 2 )  . 
of note , none of the gbrca1 / 2 - associated ecs included in this study were of serous histology . gbrca1 / 2 - associated ecs presented at different clinical figo stages ( 2009 staging system31 )  . 
taken together , our data suggest the clinicopathologic features associated with ecs occurring in patients with pathogenic gbrca1 or gbrca2 mutations may be heterogeneous . biallelic brca1 / 2 alterations allele - specic copy number analysis revealed that 77% ( n = 10 of 13 ) of the ecs in patients with pathogenic gbrca1 / 2 mutations displayed biallelic inactivation of brca1 / 2 uniformly through loh of the wild - type allele ( table 2 ; fig 1 )  . 
not all ecs occurring in pathogenic gbrca1 / 2 mutation carriers harbored biallelic brca1 / 2 alterations , which have previously been associated with hr deciency.8 although all ecs in pathogenic gbrca1 mutation carriers ( 100% ) harbored biallelic brca1 inactivation , only two of the ve ecs ( 40% ) from patients with pathogenic gbrca2 mutations displayed biallelic brca2 inactivation ( table 2 ; fig 1 )  . biallelic brca1 / 2 inactivation was found across all histologic subtypes and clinical stages of ec . 
ecs in brca2 mutation carriers lacking loh of the wild - type allele are likely sporadic tumors ; all three were stage iii at diagnosis and were endometrioid grade ii , serous , or high - grade ecs ( table 2 ; fig 1 )  . 
 ( % ) unless otherwise indicated . abbreviations : msk - impact , memorial sloan ketteringintegrated mutation proling of actionable cancer targets ; nos , not otherwise specied ; tcga , the cancer genome atlas ; wes , whole - exome sequencing . * fishers exact and mann - whitney u tests were used for comparison of categorical and continuous variables , respectively . staging information was performed according to the international federation of gynecology and obstetrics system.31 past cancer histories and information regarding radiation exposure were available for the 10 msk - impact cases and reect cancers diagnosed and treated prior to the diagnosis of ec . 13 gbrca1 / 2 - associated ecs was six ( range , 2 to 38 ) , with a median of ve ( range , 2 to 32 ) nonsynonymous mutations ( data supplement )  . 
we observed that all ecs analyzed , irrespective of the presence of monoor biallelic brca1 / 2 alterations , harbored somatic tp53 mutations , of which 12 ( 92% ) were hotspot mutations ( fig 1 ; data supplement )  . 
alterations affecting the pi3k pathway were 4 2019 by american society of clinical oncology common , with pik3ca mutations present in ve ecs ( 38% ) , pik3r1 mutations in two ecs ( 15% ) , and pten mutations / homozygous deletions in three ecs ( 23% ; figs 1 and 2 )  . 
other recurrently altered genes included fat1 , ptch1 , kras , and map3k1 ( each n = 2 ; fig 1 , data supplement )  . we noted that bec - 1 , a likely sporadic ec from a gbrca2 mutation carrier with a monoallelic brca2 alteration , had a high mutational burden with 32 nonsynonymous somatic mutations . 
the ecs with very low levels of gene cnas ( ie , bec - 1 , bec - 6 , and bec - 12 ) had monoallelic brca2 alterations and were likely sporadic , with one ( bec - 1 ) being msi high , as mentioned . 
in addition , we found an nf1 homozygous deletion in the biallelic brca1 grade ii endometrioid tcga - 2 and a smarca4 homozygous deletion in the biallelic brca2 carcinosarcoma bec - 2 . 
of note , smarca4 ( brg1 ) loss is commonly found in unthe endometrium , 32 , 33 and differentiated carcinoma of bec - 2 was a carcinosarcoma with heterologous elements , which , in addition to the carcinoma and sarcomatous components , also displayed an undifferentiated component . 
finally , amplication of bcl6 , tp63 , and eed was found in the biallelic brca1 grade iii endometrioid tcga - 1 ec ( fig 2 )  . taken together , we found that ecs in patients with a gbrca1 / 2 mutation are heterogeneous at the mutational and gene copy number levels . 
we observed that ecs with biallelic brca1 / 2 alterations ( n = 10 ) had high lst scores , whereas ecs with monoallelic brca1 / 2 alterations did not ( table 2 ; fig 3a )  . 
nonsynonymous somatic mutations identied in 410 cancer - related cancer genes in ecs from germline brca1 ( n = 8 ) and germline brca2 ( n = 5 ) mutation carriers ( left ) are shown . the mutation types are color coded according to the legend . 
information on the germline mutation status , somatic loss of heterozygosity of brca1 / 2 , histologic type , microsatellite instability ( msi ) status , and sequencing type is provided in the phenobar below the sample names . 
tcga , the cancer genome atlas . with hr deciency ( fig 3b ) .14 given the limited number of snvs and indels in the ecs subjected to msk - impact sequencing , other genomic hr - deciency features such as indel length , microhomology , or mutational signatures using decomposition algorithms could not be used . therefore , we used sigma , a recently described , likelihoodbased measure signature analysis combined with machinelearning techniques , which can be used to detect the mutational signature sig3 associated with hr deciency from targeted gene panels including msk - impact ( sensitivity range , 48% to 62% for uterine cancers ) .25 consistent with the lst analysis , all six biallelic , brca1 / 2associated ecs subjected to msk - impact and with at least ve snvs displayed either a dominant hr deciency - related sig3 ( n = 2 ) or a dominant clock signature with secondary hr - deciency signatures sig3 ( n = 3 ) or sig834 ( n = 1 ) , to the two sporadic ecs with monoallelic in contrast brca2 alterations , which displayed msi ( sigma ) / signature 6 ( deconstructsigs ) and apobec signatures ( table 2 ; fig 3c )  . 
previous reports of ecs in this population have acknowledged that the prevalence of ec in gbrca1 / 2 mutation carriers is low.5 here , through an in - depth analysis of ecs from patients with pathogenic gbrca1 / 2 mutations , we demonstrate that the majority of these cases ( 77% ) harbored biallelic brca1 / 2 alterations and displayed genomic features of hrd , providing evidence to suggest an etiological link between the pathogenic gbrca1 / 2 mutations and the development of these ecs . 
in fact , this phenomenon was uniformly observed in patients with pathogenic gbrca1 mutations ; conversely , only two of the ve patients with pathogenic gbrca2 mutations had somatic inactivation of the brca2 wild - type allele and genomics features of hr deciency . 
in ovarian cancer , patients with hr - decient tumors have improved overall survival with platinum - based therapy and have better responses to hr deciencydirected treatments such as parp inhibitors than their wild - type counterparts.35 , 36 knowledge of the allele status of brca1 / 2 alterations and / or hr - deciency features could be benecial in therapeutic decision making for patients with gbrca1 / 2 mutations and ec . 
our analysis has demonstrated that not all ecs arising in the context of pathogenic gbrca2 mutations harbor loh of the wild - type allele and genomics features of hr deciency . 
in addition , it revealed that one of these cases was msi high , likely representing a sporadic ( ie , non - brca1 / 2 ) ec arising in a gbrca2 mutation carrier . 
in this context , this patient would potentially benet from immune checkpoint inhibitors , which have been approved for the management of recurrent msi - high / dna mmrdecient cancers.37 in fact , a recent case report highlighted a complete remission after pd - 1 blockade in a patient with mmr - decient ec and a pathogenic monoallelic gbrca1 mutation.38 the majority ( 75% ) of biallelic gbrca1 / 2 - associated ecs were of intermediate / high - grade endometrioid as opposed to serous histology in previous reports.5 , 6 all six biallelic gbrca1 / 2 - associated endometrioid ecs harbored tp53 mutations , had high lst scores , and relatively high levels of cnas ( table 2 ; fig 2 ) , and would likely be of copy - number high ( serous - like ) molecular subtype , as described by tcga.13 it should be noted , however , that of these six endometrioid ecs with biallelic brca1 alterations , four harbored somatic mutations characteristic of endometrioid ecs , including pik3ca mutations , pik3r1 mutations , and pten mutations / homozygous deletions . 
conversely , two of these ecs lacked alterations affecting genes recurrently altered in endometrioid ecs ( fig 1 ) , suggesting that at the these latter two cases resembled serous genetic level , rather than endometrioid carcinomas , and that there is heterogeneity in gbrca1 / 2 - associated ecs . 
carcinosarcomas of the uterus are rare , representing less than 5% of all uterine tumors.39 we noted a high frequency ( 30% ) of carcinosarcomas in the 10 gbrca1 / 2 - associated ecs subjected to msk - impact sequencing , whereas overall , only 10% of the 769 ecs subjected to germline mskimpact sequencing were carcinosarcomas ( remaining cases : 55% endometrioid , 15% serous , 10% endometrial cancer nos , 4% mixed endometrial , 3% clear cell , 1% deor undifferentiated , and 1% other )  . 
interestingly , recurrent somatic brca1 / 2 mutations and brca2 deletions also have been reported in uterine carcinosarcomas.40 - 42 these ndings suggest that ecs arising in gbrca1 / 2 mutation carriers are heterogeneous at the histologic level and are potentially enriched for endometrioid tumors and carcinosarcomas . the data presented here do provide insight into the genomics of ecs in patients with pathogenic gbrca1 / 2 mutations , which may play a role in the tumorigenesis and / or progression of ec in some patients . 
this study has several limitations , however , primarily driven by the small sample size , and it does not resolve the controversy of ec as a feature of hboc syndrome . 
the low incidence of these cases ( 1.3% ; n = 10 of 769 ecs subjected to germline mskimpact testing ) not only limits the sample size of this study but also , on its own , presents a challenge in dening ec as part of the hboc syndrome spectrum of malignancies . 
 brca1 / 2 endometrial cancer lsts mutational signatures ( decontructsigs ) signature 1 ( aging ) signature 3 ( hr defect ) signature 15 ( mmr defect ) signature 19 signature 20 ( mmr defect ) signature 24 signature 25 unknown tcga - 1 tcga - 2 tcga - 3 mlh1 biallelic brca1 / 2 ( n = 10 ) monoallelic brca2 ( n = 3 ) pms2 msh2 msh6 signature 1 aging signature 6 mmr defect signature 21 mmr defect unknown mutational signatures bec - 1 fig 3 . 
 ( a ) large - scale state transition ( lst ) scores in germline ( gbrca1 / 2 ) - associated endometrial cancers with biallelic ( n = 10 ) and monoallelic ( n = 3 ) brca1 / 2 alterations . 
 ( b ) mutational signatures dened by deconstructsigs24 in three gbrca1 / 2 - associated endometrial cancers from the cancer genome atlas ( tcga ) subjected to whole - exome sequencing.13 , 14 mutational signatures are color coded according to the legend on the right . 
 ( c ) immunohistochemical analysis of the ( left ) dna mismatch repair ( mmr ) proteins mlh1 , pms2 , msh2 , and msh6 and ( right ) mutational signatures of case bec - 1 , a monoallelic / sporadic gbrca1 / 2 - associated endometrial cancer . 
bec - 1 shows loss of mlh1 and pms2 expression , mlh1 promoter hypermethylation ( not shown ) , and dominant mutational signatures 6 and 21 associated with defective dna mmr . mutations in patients with ec nor the impact of these mutations on the outcome of patients with ec could be fully dened . 
although we have assessed the genomics features of hr deciency , including lsts and sigma hr deciency signature sig3 in all cases , hr deciency is more accurately assessed with whole - genome sequencing.43 hence , additional studies testing ecs developing in the context of pathogenic gbrca1 / 2 mutations but lacking loss of the wildtype allele by whole - genome sequencing are warranted . despite these limitations , here we demonstrate the importance of germline and somatic genetic characterization of ecs . 
in fact , ecs developing in the context of pathogenic gbrca1 / 2 mutations may harbor genomics features of hr deciency and be causally linked to the loss of function of these tumor suppressor genes . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . nadeem riaz honoraria : peerview speakers bureau : illumina research funding : bristol - myers squibb , pzer travel , accommodations , expenses : varian medical systems mark e . 
robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca , pzer other relationship : research to practice , clinical care options , physician education resource robert a . 
assignee : 2015 the regents of the university of california 8 / 18 / 2015 ( inst ) ; application : compositions and methods for the diagnosis and treatment of ovarian cancers that are associated with reduced smarca4 gene expression or protein function ( inst ) ; royalties from published books : cambridge university press and springer publishing jorge s . 
reis - filho consulting or advisory role : roche , invicro , ventana medical systems , volition rx , paige.ai , goldman sachs , novartis britta weigelt consulting or advisory role : roche ( i ) , invicro ( i ) , ventana medical systems ( i ) , volition rx ( i ) , paige.ai ( i ) , goldman sachs ( i ) , novartis ( i ) no other potential conicts of interest were reported . acknowlegement we thank the members of the molecular diagnostics service in the department of pathology , memorial sloan kettering cancer center . references gudmundsdottir k , ashworth a : the roles of brca1 and brca2 and associated proteins in the maintenance of genomic stability . 
oncogene 25 : 5864 - 5874 , 2006 king mc , marks jh , mandell jb : breast and ovarian cancer risks due to inherited mutations in brca1 and brca2 . 
nat rev clin oncol 13 : 41 - 54 , 2016 segev y , iqbal j , lubinski j , et al : the incidence of endometrial cancer in women with brca1 and brca2 mutations : an international prospective cohort study . gynecol oncol 130 : 127 - 131 , 2013 shu ca , pike mc , jotwani ar , et al : uterine cancer after risk - reducing salpingo - oophorectomy without hysterectomy in women with brca mutations . 
jama oncol 2 : 1434 - 1440 , 2016 pennington kp , walsh t , lee m , et al : brca1 , tp53 , and chek2 germline mutations in uterine serous carcinoma . 
cell 173 : 355 - 370.e14 , 2018 riaz n , blecua p , lim rs , et al : pan - cancer analysis of bi - allelic alterations in homologous recombination dna repair genes . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
ashley cw , da cruz paula a , kumar r , et al : analysis of mutational signatures in primary and metastatic endometrial cancer reveals distinct patterns of dna repair defects and shifts during tumor progression . 
geyer fc , li a , papanastasiou ad , et al : recurrent hotspot mutations in hras q61 and pi3k - akt pathway genes as drivers of breast adenomyoepitheliomas . nat commun 9 : 1816 , 2018 e131 , 2016 17 . 
karnezis an , hoang ln , coatham m , et al : loss of switch / sucrose non - fermenting complex protein expression is associated with dedifferentiation in endometrial carcinomas . 
ramalingam p , croce s , mccluggage wg : loss of expression of smarca4 ( brg1 ) , smarca2 ( brm ) and smarcb1 ( ini1 ) in undifferentiated carcinoma of the endometrium is not uncommon and is not always associated with rhabdoid morphology . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
dizon ds , dias - santagata d , bregar a , et al : complete remission following pembrolizumab in a woman with mismatch repair - decient endometrial cancer and a germline brca1 mutation . 
gynecol oncol 137 : 581 - 588 , 2015 jones s , stransky n , mccord cl , et al : genomic analyses of gynaecologic carcinosarcomas reveal frequent mutations in chromatin remodelling genes . 
zhao s , bellone s , lopez s , et al : mutational landscape of uterine and ovarian carcinosarcomas implicates histone genes in epithelial - mesenchymal transition . proc natl acad sci usa 113 : 12238 - 12243 , 2016 jones nl , xiu j , chatterjee - paer s , et al : distinct molecular landscapes between endometrioid and nonendometrioid uterine carcinomas . 
 next - generation sequencing of advanced gi tumors reveals individual treatment options michael bitzer , md1 , 2 , 5 ; leonie ostermann1 ; marius horger , md3 ; saskia biskup , md , phd4 ; martin schulze , dsc4 ; kristina ruhm , msc5 ; franz hilke , msc6 ; oznur oner , msc5 ; konstantin nikolaou , md , mba2 , 3 ; christopher schroeder , md6 ; olaf riess , md6 ; falko fend , md7 , 8 ; daniel zips , md8 , 9 ; martina hinterleitner , md10 ; lars zender , md2 , 8 , 10 ; ghazaleh tabatabai , md , phd2 , 8 , 11 ; janina beha , phd5 ; and nisar p . 
malek , md1 , 2 , 5 , 8 purpose precision oncology connects highly complex diagnostic procedures with patient histories to identify individualized treatment options in interdisciplinary molecular tumor boards ( mtbs )  . 
follow - up data and a response assessment that was based on radiologic imaging were recorded . results ninety - six patients were presented to the mtb of tuebingen university hospital . 
patients with pr or sd in the course of mtb - recommended treatments seemed to benet with respect to pfs and os . jco precis oncol 4 : 258 - 271 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction the challenge of precision oncology is to connect highly complex diagnostic procedures with individual patient histories to identify optimal treatments . 
detailed data on mtbguided treatment suggestions , and specically the outcomes of patients , have only been reported for nonselected patient groups , including for a variety of different tumors.1 - 4 however , each tumor entity , including gi cancers , harbors unique features that will have to be considered to identify the patients who will benet the most from such an approach.4 recent reports highlight the experiences of mtbs in everyday practice . 
a series from the md anderson cancer center that examined hot - spot regions in 11 to 50 genes for 2 , 000 cancer tissues found actionable mutations for 39% of patients.2 only 11% of these selected patients could be enrolled in genotype - matched clinical trials.2 a report from the mayo clinic identied actionable mutations in 65% of 141 patients , but only 29 ( 21% ) were subsequently treated in clinical trials or with targeted food and drug administration ( fda ) approved drugs , with an objective response or stable disease ( sd ) for 4 months in 10 patients.3 freiburg university reported 104 patients with recommendations that were based on diagnostic tests that ranged from an 8 - gene panel to whole - exome sequencing ( wes ) .1 thirty - three patients received a recommended treatment ; 11 had an objective response , and 8 additional patients reached sd at 10 weeks . 
 molecular tumor board for advanced gi cancers context key objectives academic molecular tumor boards ( mtbs ) bridge the gap between a growing complexity in diagnostic procedures and clinicians at the bedside . 
this retrospective study investigated the course of patients with advanced gastrointestinal ( gi ) cancers that have been considered for personalized treatment options , including the outcome receiving mtb - guided treatment . knowledge generated next - generation sequencing ( ngs ) revealed a relevant number of germline variants , suggesting genetic counseling . 
responding patients with prolonged disease stabilization seemed to derive a meaningful survival benet from cancer genome sequencing and matched treatments . relevance patients with gi cancers can benet from currently available ngs sequencing procedures . 
in perspective , a continued improvement of mtb recommendations and the inclusion of additional complex diagnostic procedures might substantively enhance treatment opportunities in everyday clinical practice for these patients in the near future . the sequencing of matched tumor and normal tissue is an important procedure for the precise identication of potentially actionable genes.5 , 6 this inevitably leads to the detection of germline alterations . 
a recent investigation in 10 , 389 patients across 33 cancer types detected pathogenic or likely pathogenic germline variants in 8% of all patients with cancer and in 8.8% of patients with gi tumors.7 the frequency of germline mutations varied greatly across cancer types in general but also across different gi cancers , ranging from 2.2% for cholangiocarcinoma to 14.1% for pancreatic cancer ( pc ) .7 to our knowledge , our experience with gi tumors in an academic mtb is to date the largest reported series of this group with detailed information of comprehensive sequencing data , subsequent board recommendations , and documented outcome . 
the mtb consists of an interdisciplinary team coordinated by the tuebingen center for personalized medicine and includes experts in clinical and translational oncology , pathology , bioinformatics , molecular biology , radiology , and human genetics . 
an electronic web - based platform ( mtb platform ) was established to introduce patients to the mtb team with all necessary information to prepare and follow up the weekly face - to - face meetings and subsequently document treatment outcomes ( data supplement )  . 
best response assessment was based on radiologic imaging in line with recist 1.1 , for checkpoint inhibitor therapy , irecist , or for hepatocellular carcinomas ( hcc ) , mrecist criteria.8 - 10 genetic tumor / normal characterization tumor and normal tissues were genetically characterized either by ngs panel sequencing of full coding sequences or by wes ( more information in data supplement )  . 
off - label use refers to the administration of an fda / european medicines agency - approved drug outside its approved indication . for recommended off - label therapies , an application for reimbursement was submitted to the patients health individual treatment describes insurance . 
patients treated within a heilversuch have been registered at the local authority , in this case the regierungspr asidium tuebingen . statistical analysis progression - free survival ( pfs ) and overall survival ( os ) were analyzed with the kaplan - meier method dependent on the treatment response ( sd and pr v progressive disease [ pd ] ) compared by log - rank testing . 
btc , biliary tract cancer ; crc , colorectal cancer ; gc , gastric cancer ; hcc , hepatocellular carcinoma ; net , neuroendocrine tumor ; pc , pancreatic cancer ; ugc , upper gi tract cancer . results diagnostic procedure and clinical work - up ninety - six patients received ngs of advanced gi tumors and were presented to the mtb . 
this cohort included 32 colorectal cancer ( crc ) , 22 pc , 19 biliary tract cancer ( btc ) , 11 hcc , 9 upper gi tract cancer ( ugc ) , and 3 neuroendocrine tumors ( net ; fig 1a )  . 
the mean number of systemic anticancer pretreatments was 2.8 ( fig 1b )  . ninety - one patients received a gene panel analysis that examined between 337 and 710 genes , and 5 patients had wes ( fig 1c )  . 
genes represented in the different panels are summarized in the data supplement , together with the total size and the average and median coverage of the 649 and 710 gene panels . germline variants in gi cancers germline ndings were ranked according to a 5 - tiered classication.11 , 12 sixteen patients ( 17% ) had germline variants classied as pathogenic or likely pathogenic ( figs 1d - 1f ) , and in 1 patient with gastric cancer , 2 likely pathogenic variants were detected ( palb2 and fancm )  . five patients ( 5% ) had pathogenic or likely pathogenic germline variants in one of the brca2 , msh6 , or sdhb genes . 
these alterations belong to a list of secondary ndings that should be reported because of the possibility for interventions to signicantly reduce morbidity and mortality.13 in addition , 3 patients showed germline variants in pharmacologically relevant genes , 2 in dpyd and 1 in g6pd ( data supplement ) without showing unusual adverse reactions during chemotherapy . 
this variant has been reported with classications ranging from variant of unknown signicance to pathogenic.14 a germline alteration was directly responsible for mtb recommendations for 5 patients ( 5% ) : brca2 for poly ( adpribose ) - polymerase ( parp ) inhibition ( 3 pc ) , chek2 combined with 2 somatic atm truncations for atr - inhibition and carboplatin ( 1 crc ) , and msh6 and therefore a resulting high tumor mutational burden ( tmb ) for pembrolizumab ( 1 crc )  . 
 molecular tumor board for advanced gi cancers frequency of germline mutations ( n = 96 ) presentation of ngs for gi tumors ( n = 96 ) molecular target identification ( n = 96 ) patients with clinically relevant ( n = 19 [ 20% ] ) germline mutations patients with pathogenic or likely pathogenic ( n = 16 ) variants patients with pharmacogenomic relevant variants ( n = 3 ) patients with at least 1 molecular target ( n = 47 [ 49% ] ) patients without mtb recommendation ( n = 6 ) no progression under last line treatment ( n = 4 ) complete tumor resection ( n = 2 ) patients not treated with recommendation ( n = 16 ) patients with poor performance status ( n = 15 ) patients not evaluable ( n = 5 ) without imaging for response monitoring ( n = 3 ) died within 21 days after treatment start ( n = 2 ) patient not evaluable ( n = 1 ) alternative therapy before response monitoring patients with mtb treatment recommendation ( n = 41 [ 43% ] ) patients received the suggested treatment ( n = 25 [ 26% ] ) patients with colorectal cancer ( n = 11 ) patients with pancreatic cancer ( n = 7 ) patients with biliary tract cancer ( n = 4 ) patients with upper gi tract cancer ( n = 2 ) patient with hepatocellular carcinoma ( n = 1 ) patients evaluable for best response and os ( n = 20 [ 21% ] ) patients pr ( n = 3 [ 15% of 20 patients ] ) patients sd ( n = 6 [ 30% of 20 patients ] ) patients pd ( n = 11 [ 55% of 20 patients ] ) fig 2 . 
 ( b ) frequency of potential target identication by the molecular tumor board ( mtb ) , patients with target identication but no treatment , and patients with mtb - recommended treatment initiation . 
btc , biliary tract cancer ; crc , colorectal cancer ; hcc , hepatocellular carcinoma ; net , neuroendocrine tumor ; pc , pancreatic cancer ; ugc , upper gi tract cancer ; w / o , without . pharyngeal , or bladder cancer ; and the patient with a chek2 mutation had a rst - degree relative with ovarian cancer . 
eight of these 10 patients were also tested for msi , but only 2 patients were found to have a msi - high tumor . tmb is currently regarded as relevant in predicting therapeutic success with checkpoint inhibitors beyond tumors with mismatch repair deciency.15 - 18 this has been shown for patients with crc and ugc , 18 but is less clear for hepatobiliary cancer and pc . 
for tumors known to have a low tmb in general , those with values molecular target identication by the mtb at least 1 potential molecular target was identied in 47 of 96 patients ( 49% ; figs 2b and 3b )  . 
the frequency of target identication varied among tumor types ( fig 3c , table 2 ) , with 74% for btc , 56% for upper gi cancers , 50% for pc , 44% for crc , and 27% for hcc . 
the most frequently altered genes with single - nucleotide variants or copy number variants were cdkn2a / b , brca2 , idh1 , erbb2 , myc , fgf3 , fgf4 , flt3 , fgfr4 , cdk6 , braf , and atm ( table 2 ; data supplement )  . 
target identication per tumor type ( continued ) diagnosis patients tested ( no . ) molecular target frequency erbb2 braf brd4 cdkn2a / b chek2 fgf3 / 4 / 19a flt1 / 3 mlh1 msh6 fgfr2 - bicc1 idh1 braf brca1 brca2 cdkn2a fgfr1 fgfr2b fgfr4 fgfr2 - prkcq fgfr2 - ahcyl2 cdkn2a / b brca2 cdk6 erbb3 nrg3 nrg1 - cdh6 tmem66 - nrg1 cdkn2a / b cdk6 fgf3 / 4 idh1 idh1 abbreviations : btc , biliary tract cancer ; crc , colorectal cancer ; hcc , hepatocellular carcinoma ; pc , pancreatic cancer ; tmb , tumor mutational burden . afgf3 / fgf4 / fgf19 cluster amplication . bcoincident fgfr2 mutation in tumor with fgfr2_ahcyl2 fusion gene . cdkn2a / b alterations , 6 were detected in pc , 2 in ugc , 1 in btc , and 1 in crc . 
three out of 4 brca2 alterations were detected in pc , and 1 in btc ( table 2 )  . outcome and clinical course of patients the course of all patients presented to the mtb is shown in fig 2b . 
mtb recommendations for matched treatments were given for 41 patients ( 43% )  . twenty - ve patients with a mean of 3.4 previous anticancer treatments received the suggested medication ( 61% of patients with mtb recommendation ; 26% of the whole cohort )  . 
the alterations in included cdkn2a / b this subgroup without treatment deletions , braf mutations , brca deletions , flt1 / 3 amplication , fgfr2 fusion , idh mutation , and high tmb ( data supplement )  . treatment was initiated in 11 patients with crc ( 34% of patients with crc ) , 7 patients with pc ( 32% of patients with pc ) , 4 patients with btc ( 21% of patients with btc ) , 2 patients with ugc ( 22% of patients with ugc ) , and 1 patient with hcc ( 9% of patients with hcc )  . 
the applied drugs were either used in - label , used off - label , obtained via a clinical study , or supplied for a matched experimental treatment ( table 1 , drug availability column )  . 
 molecular tumor board for advanced gi cancers patients who reached either sd or pr were treated with pd1 blocking antibodies ( high tmb ) , atr inhibitor with carboplatin ( simultaneous mutations in atm , chek2 , and tp53bp1 ) , trastuzumab with lapatinib ( erbb2 amplication ) , pertuzumab with erlotinib ( nrg1 fusion , high - expression erbb3 and nrg3 ) , idh1 inhibitor bay 1436032 ( idh1 mutation ) , or lenvatinib ( fgfr2 fusion gene ; table 1 )  . 
1 year after treatment initiation reached either sd or pr ( data supplement )  . therefore , as a surrogate end point to estimate whether patients might benet from the mtb - recommended treatment , the achievement of sd for at least 3 months or even pr as best response was compared with pd in a kaplan - meier estimation for pfs and os . 
in several studies , the inclusion of germline ndings enabled a more comprehensive characterization of tumor biology , potential resistances , or even treatment opportunities.22 , 23 in this study , germline variants classied as pathogenic , likely pathogenic , or pharmacogenomic could be identied in 19 patients ( 20% )  . 
these numbers are higher than in a recent investigation that reported pathogenic or likely pathogenic germline predisposition variants in 8.8% of gi tumors , 7 and could be mainly a result of the smaller sample size in our study . 
for example , for brca mutations , the tumor lineage indeed seems to determine the therapeutic benet of parp inhibition.24 conversely , emerging data suggest that patients with germline mutations that are not typically associated with a diagnosed cancer might nevertheless benet from drugs that target this alteration.25 germline variant reporting and the inclusion of experts in clinical genetics , should therefore be a prerequisite for mtbs.22 , 23 , 26 in predicting therapeutic tmb is regarded as relevant outcome with checkpoint inhibitors.15 - 18 the minimum size of tumor panels to reliably calculate tmb was suggested to include at least 300 genes , or more precisely , 1.5 mb of the target region , 21 , 27 , 28 which is met in our approach . 
one patient with crc and high tmb ( 118 var / mb ) who showed progression under pd - 1 inhibition even responded after the addition of ctla4 inhibition on progression . 
in the 4 patients who did not show any response to checkpoint inhibition , the molecular analysis did not reveal one of the currently discussed mechanisms of resistance.29 of note , only a minority of patients with high tmb also had msi - high tumors . 
this observation is in line with an investigation in a broad range of different tumor types , showing that only 16% with high tmb were classied as msi high.21 another study in 6 , 004 patients with crc identied 465 patients with high tmb ; however , only 65% of these could be classied as msi high.30 these observations suggest that a reliable method for tmb estimation should be used if patients with gi tumors are evaluated for personalized treatment options . of 96 patients with advanced gi tumors , mtb treatment recommendations were given for 41 ( 43% ) , which means an additional therapy option beyond established treatment lines for 4 out of 10 patients . 
14 months in our cohort , compared with patients with pd as best response ( fig 4d ) , is remarkable ; however , it has to be interpreted with caution and should be conrmed in larger patient populations with gi or other cancers . 
if this observation could be conrmed , 1 goal in the constant improvement of mtb recommendations should be to gradually increase the percentage of patients who reach disease control of at least 3 months in advanced cancers . early cohorts with molecular - matched therapies have been reported for crc31 and btc.32 in the rst study , 68 out of 254 patients with advanced crc received selected matched therapies to kras / braf / pik3ca mutations , pten , or phosphorylated met expression . 
a subgroup with btc from the moscato - 01 trial reported molecular targets in 23 of 34 patients , with 18 receiving matched therapies ( 53% ) .32 the overall response rate and pfs of 6 months in that study were 33% and 37% , respectively . 
several techniques , such as transcriptome34 , 35 and epigenome36 analysis or wholegenome37 and single - cell sequencing , are expected to improve tumor characterization up front.38 such a constant evolution will require more specialists in these methods to join academic mtbs , which means a new era of terdisciplinary patient care to bridge the gap between a growing complexity in diagnostic procedures and clinicians at the bedside . 
 ( a ) progression - free survival ( pfs ) , dened as the time from start of an mtb - recommended treatment to radiographic progression or death , and ( b ) overall survival ( os ) , dened as the time from start of an mtbrecommended treatment to death as a result of any cause , in days . 
recent examples in crc are pd - l1 and ctla - 4 inhibition in msi - high cancers41 or the combination of a braf inhibitor , mek inhibitor , and antiepidermal growth factor receptor antibody in braf v600e mutated cancers.42 third , a reduction in dropout rates might be achieved with more focused and earlier patient selection for ngs - based diagnostic procedures and a shortening of time intervals to get access to suggested drugs . 
fourth , each patient who is treated according to an mtb recommendation outside clinical trials should be regarded as an n - of - 1 trial.43 this implies a thorough documentation of adverse events and a reliable response assessment along a predened routine . in conclusion , gi tumors are an important group in the eld of personalized medicine . 
malek provision of study material or patients : michael bitzer , falko fend collection and assembly of data : michael bitzer , leonie ostermann , marius horger , saskia biskup , kristina ruhm , oznur oner , christopher schroeder , olaf riess , falko fend , daniel zips , martina hinterleitner , lars zender , janina beha data analysis and interpretation : michael bitzer , leonie ostermann , marius horger , saskia biskup , martin schulze , franz hilke , konstantin nikolaou , christopher schroeder , olaf riess , daniel zips , martina hinterleitner , lars zender , janina beha , nisar p . 
 bitzer et al falko fend consulting or advisory role : roche , eusa pharma daniel zips research funding : elekta ( inst ) , siemens ( inst ) , sennewald ( inst ) travel , accommodations , expenses : elekta ( inst ) martina hinterleitner travel , accommodations , expenses : novartis / ipsen lars zender leadership : heparegenix gmbh consulting or advisory role : boehringer ingelheim research funding : heparegenix gmbh patents , royalties , other intellectual property : patent on mkk4 inhibition for the treatment of acute and chronic liver diseases travel , accommodations , expenses : ipsen ghazaleh tabatabai honoraria : abbvie , bayer , medac , novocure ( inst ) consulting or advisory role : abbvie , bayer travel , accommodations , expenses : novocure ( inst ) nisar p . 
hoefin r , geiler a - l , fritsch r , et al : personalized clinical decision making through implementation of a molecular tumor board : a german single - center experience . 
j clin oncol 33 : 2753 - 2762 , 2015 bryce ah , egan jb , borad mj , et al : experience with precision genomics and tumor board , indicates frequent target identication , but barriers to delivery . oncotarget 8 : 27145 - 27154 , 2017 zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
nat med 23 : 703 - 713 , 2017 [ erratum : nat med , 2017 ] jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
sci transl med 7 : 283ra53 , 2015 cheng dt , prasad m , chekaluk y , et al : comprehensive detection of germline variants by msk - impact , a clinical diagnostic platform for solid tumor molecular oncology and concurrent cancer predisposition testing . 
eur j cancer 45 : 228 - 247 , 2009 seymour l , bogaerts j , perrone a , et al : irecist : guidelines for response criteria for use in trials testing immunotherapeutics . 
plon se , eccles dm , easton d , et al : sequence variant classication and reporting : recommendations for improving the interpretation of cancer susceptibility j hepatol 66 : 1166 - 1172 , 2017 genetic test results . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
n engl j med 377 : 2500 - 2501 , 2017 jenkins rw , thummalapalli r , carter j , et al : molecular and genomic determinants of response to immune checkpoint inhibition in cancer . 
fabrizio da , george tj jr , dunne rf , et al : beyond microsatellite testing : assessment of tumor mutational burden identies subsets of colorectal cancer who may respond to immune checkpoint inhibition . 
verlingue l , malka d , allorant a , et al : precision medicine for patients with advanced biliary tract cancers : an effective strategy within the prospective moscato - 01 trial . 
overman mj , lonardi s , wong kym , et al : durable clinical benet with nivolumab plus ipilimumab in dna mismatch repair - decient / microsatellite instabilityhigh metastatic colorectal cancer . 
 duality of purpose : participant and parent understanding of the purpose of genomic tumor profiling research among children and young adults with solid tumors purpose increasing use of genomic tumor profiling may blur the line between research and clinical care . 
we aimed to describe perspectives of research participants about the purpose of genomic tumor profiling research in pediatric oncology . methods we surveyed 45 participants ( response rate , 85% ) in a pilot study of genomic profiling in pediatric solid tumors at four academic cancer centers after the return of sequencing results . 
we defined understanding according to a one - item ( basic ) definition ( recognition that the primary purpose was not to improve the patients treatment ) and a four - item ( comprehensive ) definition ( primary purpose was not to improve patients treatment ; primary purpose was to improve treatment of future patients ; there may not be direct medical benefit ; most likely result of participation was not increased likelihood of cure )  . results sixty - eight percent of respondents ( 30 of 44 respondents ) demonstrated basic understanding of the study purpose ; 55% ( 24 of 44 respondents ) demonstrated comprehensive understanding . 
ninety - three percent of respondents who believed the primary purpose was to improve the patients care simultaneously stated that the research also aimed to benefit future patients . conclusion most participants in pediatric tumor profiling research understand that the primary goal of this research is to improve care for future patients , but many express dual goals when they participate in sequencing research . 
2019 by american society of clinical oncology introduction parents of children with cancer1 , 2 and adults with cancer3 - 5 often fail to understand the purpose of clinical trials in which they participate . 
understanding the distinction between the goals of research and clinical care is of particular importance in early - phase oncology trials , in which response rates approximate 10%.6 , 7 up to 60% of research participants demonstrate evidence of therapeutic misconception , 3 , 4 , 8 , 9 the belief that the primary purpose of research is therapeutic in nature rather than acquisition of generalizable knowledge.10 , 11 the precision medicine era invites new exploration of these findings . 
 among adults16 , 17 and children.17 - 20 although advances in targeted therapeutics generate great excitement , they may also blur the line between research and clinical care.21 , 22 young adult patients and parents of children with cancer have high hopes / expectations for tumor sequencing , 23 , 24 though only a minority experience clinical benefit.25 - 29 this mirrors findings among adult patients with cancer30 - 33 and highlights the need for a deeper understanding of the tumor profiling consent process . 
furthermore , many participants simultaneously identified dual purposes for genomic tumor profiling research in pediatric oncology . relevance consenting clinicians should query and explore participant goals during presequencing counseling to identify both ( 1 ) those who do not recognize that the primary purpose of research sequencing is to generate knowledge to help future patients and ( 2 ) those who report dual purposes for this research . 
additional work is necessary to better understand the perspectives and motivations of those who express this duality and to develop and test interventions to improve equitable understanding of the purpose of genomic tumor profiling research in pediatric oncology . methods we surveyed consenting participants in the icat ( individualized cancer therapy ) pilot study of genomic profiling in children with relapsed , recurrent , and high - risk solid tumors ( clinicaltrials.gov identifier : nct01853345 ) .25 participants were approached at dana - farber / boston childrens cancer and blood disorders center ( boston , ma ) , university of california at san francisco ( san francisco , ca ) , columbia university medical center ( new york , ny ) , and childrens national medical center ( washington , dc )  . 
the study was approved by the institutional review board of all participating institutions . individualized cancer therapy study icat study procedures have been reported previously.25 all patients receiving care at participating institutions were eligible for enrollment if they were age 30 years or younger at enrollment and had a recurrent , refractory , or high - risk ( expected likelihood of cure < 25% ) extracranial solid tumor with sufficient tumor for submission . 
the study consent document described the purpose of the study as follows : to determine how often the panel of experts can [ use tumor sequencing results to ] make an individual treatment recommendation and to use this information to help future patients with cancer . 
 consent discussions were not standardized , nor were data collected on the content of these discussions . enrolled participants underwent tumor profiling via targeted next - generation sequencing and copy number assessment or a sequenom assay . 
survey items for assessment of participant understanding of the purpose of genomic profiling research in pediatric oncology question stem answer choice agree unsure * disagree * the main reason this study was done was to improve the treatment of myself / my child . the main reason this study was done was to improve the treatment of future patients with cancer . there may not have been direct medical benefit to me / my child from participation . what of the following did you think was most likely to happen because of your participation in this research study ? agree * unsure * disagree agree * unsure * disagree i / my child would have a better chance of being cured . doing this testing would give me peace of mind . * doctors would be better able to find cures for future patients . * doctors would be able to learn more about my / my childs cancer . * i / my child would have a greater number of treatment options . * nothing was likely to happen as a result of this research . * i would learn about my / my childs genes . * i would learn about my familys genes . * other * alterations for which a matched targeted therapy was available via clinical trial or us food and drug administrationapproved medication ; the recommendation described actionable alteration ( s ) found and strength of evidence for each treatment recommendation . study population icat participants were offered a self - administered written survey after return of study results to the patients oncologist . 
surveys were offered in english to the consenting individual : the patient if he / she was age 18 years or older at enrollment , or the patients parent / guardian if the patient was younger than age 18 years at enrollment . 
 surveys were not offered if the patient died between the time of enrollment and approach by the study team ( n = 41 ) ; the patient / parent did not understand english sufficiently to complete the survey ( n = 3 ) ; the patient / parent declined additional contact from study investigators after enrollment ( n = 0 ) ; and / or the oncologist did not permit approach by the study team ( n = 4 )  . survey methods survey procedures have been reported previously.24 surveys consisted of 103 items and included scales that addressed participant understanding of the purpose of clinical research , 34 genetic knowledge , 35 and the short form - 36 general health perceptions question . 
secondary outcomes were participant - level predictors of understanding ( demographic characteristics , genetic knowledge , experience with genetics , clinical status , receipt of icat recommendation / targeted therapy )  . 
participants were enrolled between september 2012 and november 2013 ; surveys were administered between september 2014 and july 2015 . participant understanding of the purpose of research sequencing we assessed participant understanding with four independent items ( table 1 )  . 
three items were adapted from the quality of informed consent measurea validated measure to assess understanding of the purpose of oncology clinical trials , 34 by adult patients with cancer and further validated in parents of children with cancer1 ; answer choices were agree , unsure , and disagree.34 the fourth item offered respondents multiple choices about their perceived most likely result of study participation . participants were asked how well they understood conversation ( s ) they had with the doctor about the icat study and the testing involved in it , and responses were collected on a 5 - point likert scale ( responses of extremely well , well , moderately , poorly , extremely poorly )  . 
 to measure patient knowledge about genetics / genomics.24 , 36 , 37 respondents were asked if they had regular exposure to genetics and / or genetic information through their job and if they had ever attended any classes / lectures on genes / genetics . statistical methods understanding of the purpose of the study was defined in two ways . 
 comprehensive understanding was defined as an understanding of all four of the following : ( 1 ) the primary purpose was not to improve their / their childs treatment ; ( 2 ) the primary purpose was to improve treatment of future patients with cancer ; ( 3 ) there may not have been direct medical benefit to them / their child ; and ( 4 ) the most likely result of participation was not an increased likelihood of cure for themselves / their child . 
for example , if a participant identified that the primary purpose of the study was not to improve her childs treatment , he or she demonstrated basic understanding of the studys purpose . 
to be as inclusive as possible , and because of the complexity and uncertainty inherent in tumor profiling research , responses of unsure to any of the first three items were coded as consistent with understanding . 
for the fourth item , only responses that the most likely result of participation in the study was cure were coded as inconsistent with understanding ; all other responses , including answers of other , were coded as understanding . 
missing responses to any of the four understanding items were excluded from analysis of comprehensive understanding ; only those that were missing the first item were excluded from analysis of basic understanding . self - report of degree of understanding of the consent conversation ( s ) was dichotomized as well or extremely well ( coded as good self reported understanding ) versus all others . 
those who answered extremely true or very true to the item about how helpful participation was to them / their child were coded as feeling the study to have been helpful , and those who answered with the other answer choices were coded as feeling it was not . experience with genetics was defined as an affirmative response to questions of regular exposure to genetics or experience with genetics / genetic information and / or enrollment in any classes / lectures on genes or genetics . 
high genetic knowledge was defined as correct answers of all four items from the gki.35 those who answered fewer than four gki items correctly were coded as having low genetic knowledge . respondent demographics and clinical characteristics and understanding of results and the purpose of testing were evaluated using descriptive statistics . 
item nonresponse was less than 10% , and participants with nonresponse to an item were excluded from analyses of that ite all analyses were performed using stata , version 13.1 ( statacorp , college station , tx )  . results respondent characteristics of 101 participants who underwent profiling on the icat study , 53 were eligible for survey administration . 
characteristics of survey respondents are listed in table 2 for the overall cohort and are subdivided into patient ( n = 11 ; 24% ) and parent / guardian ( n = 34 ; 76% ) respondents . 
participant and patient demographics , overall and separately , according to whether the survey was completed by the patients parent / guardian or by the patient himself or herself overall ( n = 45 ) patient respondents ( n = 11 ) no . 
participant and patient demographics , overall and separately , according to whether the survey was completed by the patients parent / guardian or by the patient himself or herself ( continued ) overall ( n = 45 ) patient respondents ( n = 11 ) no . 
sixty - eight percent of respondents ( 30 of 44 respondents ) recognized that the primary reason the study was performed was not to improve the treatment of them / their child , which met our definition of basic understanding of the purpose of the study . 
no significant differences were seen according to respondent age , sex , or race / ethnicity ; according to self - reported health status or likelihood of cure , receipt of an icat treatment recommendation or matched targeted therapy ; or according to participant - identified understanding of what they were told about the study . 
 results were similar when responses of unsure were excluded from analysis ( appendix fig a1 )  . similar results were seen with understanding defined by the composite four - item scale . 
comprehensive understanding of the purpose of genomic profiling research was seen with statistically greater frequency among those with at least a college education ( 73% v 28% ; p = .01 ) and with higher genetic knowledge ( 71% v 23% ; p = .01 ) and among white / non - hispanic respondents ( 68% v 37% ; p = .07 ) , though the comparison by race / ethnicity was not statistically significant . 
similarly , no statistical difference in understanding was seen according to receipt of an icat treatment recommendation or matched targeted therapy or according to whether the respondent reported a good understanding of what they were told about the study / testing . 
among those who mistakenly identified the primary purpose as improvement of their / their childs treatment , 93% ( 13 of 14 respondents ) simultaneously recognized that it aimed to benefit future patients . 
twenty - eight percent ( 12 of 43 respondents ) of those who identified that the primary purpose was to benefit future patients also reported that the primary purpose was to improve their / their childs treatment . discussion in this multi - institutional study that examined the role of molecular profiling of pediatric solid tumors , nearly all participants recognized that the primary purpose was to benefit future patients . 
 however , approximately one third of respondents believed that the primary purpose of the trial was to improve their / their childs treatment , and nearly one fifth expected participation to impart a greater chance of cure . although these responses raise concerns about the quality of informed consent for tumor fig 1 . 
relationship between participant demographics and understanding of purpose of research tumor profiling ( continued ) helpfulness of participating in the study not helpful to myself / my child helpful note . 
 ( % ) 17 ( 71 ) 7 ( 35 ) sequencing , they must be considered in context of a complex technology with an evolving role in clinical care . 
this duality is echoed by the american society of clinical oncology , which states that early - phase clinical trials in oncology simultaneously generate new knowledge and provide participants the opportunity for psychological and clinical benefit.22 , 38 oncologists often balance dual goals for patients by recommending enrollment in a phase i trial while hoping for patient benefit or by simultaneously providing palliative and cancer - directed ( ie , blended ) care.39 in the era of precision cancer medicine , it is reasonable that patients / families might perceive such dualities as well . this duality has important clinical implications . 
however , an initial approach could be to discuss the primary goal of the study as gaining new knowledge to help future patients , followed by an acknowledgment , tempered with realistic expectations , that many patients / parentsand many clinicianshold hope that the child will also benefit from participation . 
in the case of next - generation sequencing , for example , it is important to note that the number of patients who experience direct benefit via receipt of a targeted therapy is quite low , likely in the range of 3% to 19%.25 - 29 our results also underscore the importance of hope among patients and parents of children with cancer in clinical and research settings.40 - 42 hopeful thinking may partially explain why participants who felt the study had helped them / their child and those who were receiving cancer directed therapy at the time of survey completion less frequently demonstrated understanding of the purpose of research tumor sequencing . in this cohort , understanding was observed more frequently in those with at least a college education and those with good genetic knowledge . 
 this finding , also reported elsewhere , 23 is not surprising , given the complexity of these concepts and the expected link between understanding and health literacy / numeracy.43 understanding also varied according to race / ethnicity , consistent with similar work in the pediatric oncology phase i literature , 2 although the difference did not reach statistical significance in this pilot study . 
these disparities underscore the importance of attention to the needs of vulnerable populations when they are counseled about genomic results ; however , the optimal mechanism for such counseling remains unclear.44 prior work in pediatric oncology has identified that refinement of the consent process may improve understanding , 45 but optimal strategies to adequately convey the complexities of tumor sequencing and support fully informed consent for participation in sequencing research are not yet known . 
a follow - up study is in development to examine the benefit of such an intervention for those who demonstrate less than comprehensive understanding , as defined in this cohort . 
patients / parents may have better understood the purpose of profiling closer to the time of consent , but understanding did not vary statistically with time to survey completion in this cohort . 
many study participants died before surveys could be administered ; however , demographic and clinical characteristics of respondents mirrored those of the overall cohort.25 finally , participants were enrolled at four large academic centers , so results may not be generalizable to those from smaller and / or community centers . 
this could , for example , explain the unexpectedly high genetic knowledge and experience seen in this cohort . although some participants misidentified the primary goal of tumor profiling research as therapeutic in nature , participant views are nuanced . 
dubois honoraria : loxo consulting or advisory role : loxo research funding : millennium ( inst ) , merck ( inst ) , novartis ( inst ) , roche ( inst ) , genentech ( inst ) , lilly ( inst ) , curis ( inst ) , loxo ( inst ) travel , accommodations , expenses : loxo , roche , genentech julia glade - bender research funding : bristol - myers squibb ( inst ) , pfizer ( inst ) , novartis ( inst ) , ignyta ( inst ) , amgen ( inst ) , celgene ( inst ) , eisai ( inst ) , lilly ( inst ) , merck ( inst ) travel , accommodations , expenses : novartis , amgen , merck aerang kim no relationship to disclose brian d . 
weinfurt kp , seils dm , lin l , et al : research participants high expectations of benefit in earlyphase oncology trials : are we asking the right question ? j clin oncol 30 : 4396 - 4400 , 2012 6 . 
italiano a , massard c , bahleda r , et al : treatment outcome and survival in participants of phase i oncology trials carried out from 2003 to 2006 at institut gustave roussy . 
druker bj , sawyers cl , kantarjian h , et al : activity of a specific inhibitor of the bcr - abl tyrosine kinase in the blast crisis of chronic myeloid leukemia and acute lymphoblastic leukemia with the philadelphia chromosome . 
kantarjian hm , shah np , cortes je , et al : dasatinib or imatinib in newly diagnosed chronicphase chronic myeloid leukemia : 2 - year follow - up from a randomized phase 3 trial ( dasision )  . 
wagle n , grabiner bc , van allen em , et al : activating mtor mutations in a patient with an extraordinary response on a phase i trial of everolimus and pazopanib . 
kushner bh , cheung nv , modak s , et al : a phase i / ib trial targeting the pi3k / akt pathway using perifosine : long - term progression - free survival of patients with resistant neuroblastoma . 
laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
weber js , levit la , adamson pc , et al : reaffirming and clarifying the american society of clinical oncologys policy statement on the critical role of phase i trials in cancer research and treatment . 
oberg ja , ruiz j , ali - shaw t , et al : whole - genome and whole - exome sequencing in pediatric oncology : an assessment of parent and young adult patient knowledge , attitudes , and expectations . 
marron jm , dubois sg , glade bender j , et al : patient / parent perspectives on genomic tumor profiling of pediatric solid tumors : the individualized cancer therapy ( icat ) experience . 
harris mh , dubois sg , glade bender jl , et al : multicenter feasibility study of tumor molecular profiling to inform therapeutic decisions in advanced pediatric solid tumors : the individualized cancer therapy ( icat ) study . 
chang w , brohl as , patidar r , et al : multidimensional clinomics for precision therapy of children and adolescent young adults with relapsed and refractory cancer : a report from the center for cancer research . 
harttrampf ac , lacroix l , deloger m , et al : molecular screening for cancer treatment optimization ( moscato - 01 ) in pediatric patients : a single - institutional prospective molecular stratification trial . 
miller fa , hayeems rz , bytautas jp , et al : testing personalized medicine : patient and physician expectations of next - generation genomic sequencing in late - stage cancer care . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental findings : results from the canseq study . 
carere da , couper mp , crawford sd , et al : design , methods , and participant characteristics of the impact of personal genomics ( pgen ) study , a prospective cohort study of direct - to - consumer personal genomic testing customers . 
weber js , levit la , adamson pc , et al : american society of clinical oncology policy statement update : the critical role of phase i trials in cancer research and treatment . 
ferrell br , temel js , temin s , et al : integration of palliative care into standard oncology care : american society of clinical oncology clinical practice guideline update . 
sensitivity analyses for the relationship between participant demographics and understanding of the purpose of research tumor profiling basic understanding ( n = 33 ) comprehensive understanding ( n = 26 ) variable survey respondent characteristic no . 
 ( % ) respondent attitudes about icat study understanding of icat information poor self - reported understanding good self - reported understanding helpfulness of participating in icat study not helpful to myself / my child helpful basic understanding ( n = 33 ) comprehensive understanding ( n = 26 ) 10 ( 77 ) 9 ( 45 ) 11 ( 69 ) 8 ( 47 ) 8 ( 80 ) 8 ( 50 ) 10 ( 77 ) 6 ( 46 ) note . 
 erbb3 - activating mutations in small bowel adenocarcinomas purpose functional studies have demonstrated that some mutations of erbb3 , which encodes for human epidermal growth factor receptor ( her ) 3 , are oncogenic via activation of the erbb family signaling pathway . 
this study was designed to report the rate of activating erbb3 mutations in small bowel adenocarcinoma ( sba ) , a rare tumor type in which we previously reported a high rate ( 12% ) of erbb2 - activating mutations . materials and methods dna from 74 sbas , previously characterized for erbb2 mutations and mismatch repair status , was submitted for sequencing of erbb3 exons 3 , 6 , 7 , 8 , and 23 . 
mutant allelic frequencies suggested that both mutations were shared by the same clone rather than being harbored by mutually exclusive tumor subclones . conclusion sbas display a high rate of erbb3 - activating mutations , which have been shown to be targetable by anti - her2 therapies . 
2018 by american society of clinical oncology human epidermal growth factor receptor ( her ) 3 is a tyrosine kinase transmembrane receptor and a member of the her receptor family , which consists of four members : epidermal growth factor receptor ( egfr ) , her2 , her3 , and her4 , which are encoded by the egfr , erbb2 , erbb3 , and erbb4 genes , respectively . 
 unlike other members of this family , her3 has an impaired intracellular kinase domain1 and must heterodimerize with egfr , her2 , or her4 to initiate an intracellular signal , which activates downstream survival signaling such as the phosphoinositide 3 - kinase ( pik3ca ) pathway.2 in 2013 , a first report established that erbb3 displays recurrent hotspot mutations in several cancers , especially in colorectal , gastric , 3 and lobular breast cancer4 ; the most frequent amino acid change ( p.v104m / l ) is related to a single nucleotide variation hotspot located in exon 3 . 
sba is usually treated the same way as colorectal cancer , but few studies have been devoted to this cancer type.8 a first report from our team addressing the specific genomic landscape of sba was published by laforest et al , 9 in which 83 sba samples were subjected to targeted panel sequencing ( 46 genes , ion ampliseq cancer hotspot panel v2 )  . 
this study , which was performed before the discovery of erbb3 activating mutations , reported eight genes that were mutated in more than 5% of sba cases : kras , tp53 , apc , smad4 , pik3ca , erbb2 , braf , and fbxw7 . 
errb2 alterations were highly prevalent : 10 tumors ( 12% ) presented either erbb2 - activating point mutations ( n = 7 ) or erbb2 amplifications ( n = 3 )  . 
2 ethics committee under id - rcb number 2008a01058 - 47 . sample preparation tumor samples were collected as described elsewhere.9 briefly , using a 1.0 - mm punch , paraffin - embedded tissues from all cases were sampled from representative areas containing more than 50% of tumor cells . 
sequencing products were purified with sephadex gel ( ge healthcare , vlizy villacoublay , france ) before running them on a 3500 genetic analyzer ( applied biosystems , foster city , ca )  . 
sequencing data were visualized using finch tv ( geospiza , seattle , wa ) with a detection sensitivity of 10% mutated cells . next - generation sequencing ( ngs ) targeted ngs ( a panel of 39 genes ) was performed on samples with co - occurrence of erbb2 and erbb3 . 
of patients ( % ) 74 ( 100 ) median age in years , range 62 years , 32 - 98 male female tumor stage ( tnm classification ) primary tumor site duodenum jejunum ileum dmmr status msi - h histologic grading 40 ( 54 ) 34 ( 46 ) 1 ( 1 ) 25 ( 34 ) 27 ( 37 ) 19 ( 25 ) 2 ( 3 ) 36 ( 49 ) 26 ( 35 ) 12 ( 16 ) 17 ( 23 ) 57 ( 77 ) 20 ( 27 ) 23 ( 31 ) 30 ( 41 ) 1 ( 1 ) abbreviations : dmmr , mismatch repairdeficient ; msi , microsatellite instability ; mss , microsatellite stable ; na , not available raw reads were aligned on the reference human genome hg19 using the tmap aligner v0.3.7 ( life technologies )  . 
only studies with more than 100 patients and an erbb2 / erbb3 mutation rate higher than 5% ( including putative driver or passenger mutations and at least one erbb3 driver mutation ) were taken into account , with the exception of the mutation rate in the genie cohort . 
after combining erbb3 data with the previous genotyping data , a significant correlation was observed with erbb2 mutation three of the four erbb3 - mutated sba samples also displayed an erbb2 - activating mutation . 
 because the activation of two oncogenes in the same pathway is unusual , this finding was validated by subjecting two samples with sufficient dna to another ngs assay targeting both erbb2 and erbb3 to investigate whether these mutations were restricted to tumor subclones . 
in addition to confirming that erbb2 and erbb3 mutations co - occurred in the same tumor , mafs suggested a clonal distribution , ie , that both mutations were indeed harbored by the same tumor cells . erbb3 mutations , mismatch repair ( mmr ) status , and erbb2 mutations in other tumor types we investigated whether the correlation among erbb3 - activating mutations , erbb2 mutations , and msi - h status was also observed in other tumor types by performing in silico analysis of publicly available data . 
 ( * ) p < .01 between msi - h and microsatellite stable ( mss ) cancers . in 1% to 3% of the following cancer types : lobular breast , gastric , colorectal , endometrial , and cervix adenocarcinoma , together with cholangiocarcinoma and bladder cancer.3 , 4 , 11 - 18 this spectrum of erbb3 - mutated cancers overlaps with that of erbb2 - mutated and erbb2 amplified cancers , supporting the biologic concept of her2 - driven cancer because erbb3 activating mutations act via her2 signaling . 
 because sba is the most common form of erbb2 - mutated cancer ( as initially reported by laforest et al9 ) , we hypothesized that erbb3 sequencing would detect a high rate of erbb3 mutations . 
in more detail , three of the four mutated sba samples harbored the most frequent hotspot mutation of erbb3 ( v104m ) , whereas one sample harbored the e928g mutation , which has been mainly described in lobular breast adenocarcinoma18 and found in only one case in the two largest series of colorectal cancer sequencing.17 , 19 a striking finding of this study was the significant co - occurrence of erbb2 and erbb3 mutations across tumor samples . 
oncogenic mutations that activate the same signaling pathway are usually distributed according to a mutually exclusive mode in a given cancer type , eg , kras , nras , and braf mutations in colorectal cancers.17 in breast cancer , the study of heterogeneous erbb2 - amplified tumors ( a rare phenotype ) has shown that erbb2 - amplified subclones coexisted with her2 - mutated subclones.20 however , the ngs targeted analysis performed in the current study on two of the three cases with both erbb3 and erbb2 mutations did not demonstrate any significant differences between their allelic frequencies . 
the three sba samples with both erbb2 and erbb3 mutations exhibited microsatellite instability and likely had a high mutational load , 21 suggesting a possible causality that has yet to be investigated . more recently , a study performed genomic profiling of 317 sba cases , using colorectal and gastric cancers as controls.22 the reported overall erbb3 mutation rate was 6.3% , similar to that observed in our study , and was significantly higher than that observed in colorectal ( p = .001 ) and gastric ( p = .02 ) cancers in their cohort . 
this previous report provided no data regarding erbb3 and erbb2 mutation co - occurrence or the association between erbb3 mutation and msi - h . in 2017 , the food and drug administration granted accelerated approval to an immune checkpoint inhibitor ( pembrolizumab , an anti pd - 1 antibody ) for the treatment of patients with unresectable or metastatic msi - h solid tumors , regardless of the histology , on the basis of the impressive results observed in these tumors.23 for patients with concomitant msi - h tumors and erbb2 / 3 mutations , anti - her2 and antipd - 1 drugs can therefore both be considered as treatment options . 
in view of the clearly demonstrated benefit of antipd - 1 drugs in this setting , 23 , 24 which can achieve long - lasting complete responses , although anti - her2 / 3 drugs are not currently approved in this setting , anti pd - 1 drugs should probably be preferred . 
studies testing the toxicity and efficacy of immune checkpoint inhibitors and anti - her2 / 3 targeted therapies could be particularly relevant for msi - h erbb2 / 3 - mutated cancers . finally , we acknowledge that our study has several limitations . 
these include the limited sample size resulted in large cis for estimation of mutation rates , the lack of fresh frozen material prevented the performance of more comprehensive whole - exome sequencing , and , in cases with dual erbb2 / erbb3 mutations , the absence of single cell sequencing did not allow the demonstration of epistatic interactions between erbb2 and erbb3 mutations . 
hyman dm , piha - paul sa , rodon j , et al : abstract ct001 : neratinib in her2 or her3 mutant solid tumors : summit , a global , multi - histology , open - label , phase 2 basket study . 
pereira b , chin s - f , rueda om , et al : the somatic mutation profiles of 2 , 433 breast cancers refines their genomic and transcriptomic landscapes . 
ng cky , martelotto lg , gauthier a , et al : intra - tumor genetic heterogeneity and alternative driver genetic alterations in breast cancers with heterogeneous her2 gene amplification . 
 graft - versus - leukemia effect of allogeneic stem - cell transplantation and minimal residual disease in patients with acute myeloid leukemia in first complete remission purpose the detection of minimal residual disease ( mrd ) in patients with acute myeloid leukemia ( aml ) may improve future risk - adapted treatment strategies . 
we assessed whether mrd - positive and mrd - negative patients with aml benefit differently from the graft - versusleukemia effect of allogeneic hematopoietic stem - cell transplantation ( allohsct )  . methods a total of 1 , 511 patients were treated in subsequent dutch - belgian hemato - oncology cooperative group and the swiss group for clinical cancer research aml trials , of whom 547 obtained a first complete remission , received postremission treatment ( prt ) , and had available flow cytometric mrd before prt . 
prt consisted of allohsct ( n = 282 ) , conventional prt by a third cycle of chemotherapy ( n = 160 ) , or autologous hematopoietic stem - cell transplantation ( n = 105 )  . results mrd was positive in 129 patients ( 24% ) after induction chemotherapy before proceeding to prt . 
2017 by american society of clinical oncology introduction acute myeloid leukemia ( aml ) is a heterogeneous malignancy characterized by a variety of underlying cytogenetic and molecular aberrations , which are associated with distinct prognostic features.1 although current treatment approaches induce high percentages of hematologic remission , relapse rates are high and vary according to the underlying risk profile.2 recently , the european leukemianet ( eln ) developed an updated classification on the basis of cytogenetic and molecular aberrancies distinguishing patients with a favorable , intermediate , jurjen versluis burak kalin wendelien zeijlemaker jakob passweg carlos graux markus g . 
therefore , we evaluated whether and to what extent allohsct quantitatively reduces relapse compared with conventional prt in upfront - treated patients with mrd - positive or mrd - negative aml in first cr ( cr1 )  . assessed for eligibility hovon - sakk aml42a hovon - sakk aml92 hovon - sakk aml102 ( n = 1 , 511 ) ( n = 511 ) ( n = 142 ) ( n = 858 ) excluded obtained no cr received no prt no available mrd ( n = 964 ) ( n = 255 ) ( n = 234 ) ( n = 475 ) patients eligible for analysis ( n = 547 ) mrd negative ct auto allo ( n = 418 ) ( n = 118 ) ( n = 89 ) ( n = 211 ) mrd positive ct auto allo ( n = 129 ) ( n = 42 ) ( n = 16 ) ( n = 71 ) methods patients patients participated in three prospective , consecutive dutch - belgian hemato - oncology cooperative group and the swiss group for clinical cancer research ( hovon - sakk ) collaborative group trials ( aml42 , aml92 , and aml102 ; the netherlands trial register numbers ntr230 , ntr1446 , and nrt2187 , respectively ) , for whom assessment of mrd after induction therapy and before prt by allohsct , chemotherapy , or autologous hsct ( autohsct ) was performed.25 , 26 the results of the aml92 trial have not yet been published , but trial information is available in the netherlands trial register ( ntr1446 )  . 
patients were excluded if cr1 did not occur after two induction cycles of chemotherapy ( n = 255 ; 17% ) or the patient did not receive prt after obtaining cr1 ( n = 234 ; 15% )  . 
in addition , a total of 475 patients ( 31% ) received prt in cr1 ; however , their mrd status was not available within a time window of 4 months before prt . 
patients were classified by aml prognostic risk on the basis of the cytogenetic and molecular profile of the underlying aml , according to the eln2017 risk classification.3 molecular analysis was available for the majority of patients , specifically for npm1 ( 93% ) ; fms - like tyrosine kinase 3 internal tandem duplication ( flt3 - itd ; 91% ) , including the flt3 - itd mutant to wild - type ratio ( 86% ) ; evi1 ( 79% ) ; asxl1 ( 83% ) ; runx1 ( 47% ) ; and tp53 ( 47% )  . 
patient characteristics mrd negative ( n = 418 ) mrd positive ( n = 129 ) wbc count at diagnosis , 109 / l cytogenetics of aml cytogenetic abnormalities monosomal karyotype characteristic male female age , years median range < 100  . 
prt included a third cycle of chemotherapy with mitoxantrone and etoposide , high - dose chemotherapy with busulfan and cyclophosphamide followed by autohsct , or allohsct after either myeloablative conditioning or reduced intensity conditioning ( ric )  . 
the myeloablative conditioning regimen contained high - dose cyclophosphamide with at least 8 gy total body irradiation ( tbi ) in 83 patients ( 76% ) ; the remainder of the patients received busulfan with cyclophosphamide . 
although ric regimens varied , the majority contained low - dose ( 2 or 4 gy ) tbi preceded by fludarabine ( n = 126 ; 77% ) , whereas 23% of the patients received fludarabine with busulfan . 
these different prt modalities were applied according to a riskadapted strategy : patients with aml classified as favorable risk , according to cytogenetic and molecular analysis , were planned for a third cycle of chemotherapy ; intermediate - risk patients were preferentially treated with allohsct using an hla - matched sibling donor or a fully hlamatched unrelated donor , if available ; patients with adverse - risk aml proceeded to allohsct using a sibling donor , an unrelated donor , or cord blood grafts ; and patients alternatively received autohsct or a third cycle of chemotherapy if no suitable donor was available.25 - 28 mrd detection and sample selection mrd flow cytometric analysis was performed in a two - step procedure , as previously described.18 in summary , the immunophenotype was determined on blasts defined by cd45 expression with a low sideward scatter . 
mrd percentage was defined as the percentage of laip cells within the wbc compartment multiplied by the correction factor ( 100% divided by the percentage of laippositive blasts at diagnosis )  . 
patient characteristics ( continued ) characteristic year of prt median range mrd negative ( n = 418 ) mrd positive ( n = 129 ) p = .11 2011 2006 - 2014 2010 2006 - 2014 abbreviations : aml , acute myeloid leukemia ; cn - x - y , cytogenetically normal or only loss of x or y chromosome ; cr , complete remission ; eln2017 , european leukemianet 2017 ; hsct , hematopoietic stem - cell transplantation ; iqr , interquartile range ; flt3 - itd , fms - like tyrosine kinase 3 internal tandem duplication ; mrd , minimal residual disease ; npm1 , nucleophosmin - 1 ; prt , postremission treatment . * the cutoff of the flt3 - itd ratio is defined as 0.50. number of induction courses ( ie , i or ii ) was performed to allow the baseline hazard to differ between these two patient groups . 
all analyses were performed with stata software ( release 13.1 ; stata corporation , college station , tx )  . results patient characteristics a total of 547 patients with aml in cr1 and available mrd status proceeded to prt with either allohsct ( n = 282 ) , chemotherapy ( n = 160 ) , or autohsct ( n = 105 )  . 
patients with mutated npm1 were more frequently mrd negative , whereas mrd - positive patients more frequently tended to obtain a late cr1 ( ie , after induction cycle 2 )  . 
the eln2017 risk classification was similarly distributed among the mrd - negative and mrd - positive patients . interestingly , the time interval from cr1 to prt for patients with mrd - positive aml was shorter compared with their negative counterparts , which was mainly apparent in favorablerisk patients with aml . 
no other differences with regard to donor source , conditioning , cytomegalovirus serostatus , and european group for blood and marrow transplantation ( ebmt ) risk score were apparent between mrd - negative and mrdpositive patients . 
patients with a high risk of nrm according to the ebmt risk score32 ( > 3 points ) represented 45% of the patients who underwent transplantation . treatment outcome os and rfs were significantly better in patients without mrd before prt compared with mrdpositive patients ( 65% 6 2% v 50% 6 5% at 4 years ; p = .002 ; and 58% 6 3% v 38% 6 4% ; p , .001 , respectively ; figs 2a and 2b )  . 
the sample with the shortest time interval between prt and the date of collection was selected for analysis . end points the primary end point of the study was the cumulative incidence of relapse . 
the cumulative risks of relapse and nrm over time were calculated as competing risks with actuarial methods , where patients alive in continuing cr1 were censored at the date of last contact . statistical methods a time - dependent analysis of prt was performed as described previously28 , 29 by applying multivariable cox regression with allohsct as the timedependent covariable . 
in both the multivariable analysis and the estimation of the survival curves , these patients were counted as at risk in the chemotherapy group from the start of prt until allohsct and after that as at risk in the allohsct group . 
more detailed outcome estimates according to mrd status , type of prt , and risk of nrm on the basis of the ebmt risk score are presented in the data supplement . the cumulative incidence of relapse was significantly lower in patients without mrd receiving allohsct compared with chemotherapy or autohsct ( 26% 6 3% v 38% 6 3% at 4 years ; p = .027 , respectively ; fig 3a )  . 
the cumulative incidence of relapse in mrd - positive patients is estimated to be 45% 6 6% compared with 66% 6 6% at 4 years ( p = .058 ) for recipients of allohsct compared with recipients of chemotherapy or autohsct , respectively ( fig 3b )  . 
rfs after allohsct proved similar compared with prt with chemotherapy or autohsct in patients without mrd before prt ( 58% 6 4% v 58% 6 4% at 4 years ; p = .99 , respectively ; fig 3c )  . 
rfs after allohsct in mrd - positive patients before prt was 44% 6 6% compared with 31% 6 6% at 4 years ( p = .20 ) after chemotherapy or autohsct , respectively ( fig 3d )  . 
only 46 of relapsing patients ( 22% ) proceeded to allohsct after obtaining a second cr . multivariable analysis the following variables significantly predicted for relapse in the univariable analysis : mrd status , type of prt , age , wbc category , flt3 - itd category , year of prt , time from diagnosis to cr , time from cr to prt , cytogenetics , number of cycles to cr , eln2017 risk classification , npm1 mutation , evi1 overexpression , and cebpa double mutation . 
after forward selection , the multivariable analysis was performed , stratified by the total number of induction courses with adjustment for mrd status , type of prt , age , wbc category at diagnosis , flt3 - itd , eln2017 risk classification , number of cycles to cr , and year of prt ( table 3 )  . 
different variables in the multivariable model were significantly associated with relapse , with the eln2017 risk classification , flt3 - itd mutant to wild - type ratio , number of cycles to reach cr , and type of prt being the most important variables . discussion the development of treatment approaches in patients with aml is increasingly personalized by using genetic and molecular leukemia characteristics at diagnosis and individual treatment response.3 - 6 response and especially mrd , detected by either multiparametric flow cytometry or quantitative polymerase chain reaction , has become an important parameter in a more precise treatment approach for patients with aml.10 - 24 currently , it is unknown whether and how the presence or absence of mrd should guide the application of allohsct as prt . 
recently , the quantitative detection of mutated npm1 has been shown to have high predictive value , and recommendations to tailor the application of allohsct by mrd were made.10 - 12 balsat et al10 suggested refraining from allohsct in npm1 mrdnegative patients and to selectively proceed to allohsct as prt in cr1 in mrd - positive patients or adverse - risk patients on the basis of karyotype or the presence of flt3 - itd . 
kaplan - meier estimates of the cumulative incidence ( ci ) of relapse in ( a ) minimal residual disease ( mrd ) negative patients ; ( b ) ci of relapse in mrdpositive patients ; ( c ) relapse - free survival ( rfs ) in mrd - negative patients ; and ( d ) rfs in mrdpositive patients by type of prt in patients with acute myeloid leukemia in first complete remission from start of prt . 
nevertheless , the advantages of personalized treatment are obvious and continuously being refined by updated and better methods of risk assessment . also , new technologies to better define mrd , such as quantification of leukemic stem - cell content , standardized protocols and antibody panels , and novel software possibilities , are emerging.45 - 47 a personalized approach including mrd identifies patients with a high risk of relapse who qualify for allohsct , but who might benefit from attempts to induce mrd negativity before transplantation . 
previously , a number of investigators reported that patients in cr1 with persistence of mrd before allohsct have worse survival compared with recipients of allohsct with an mrd - negative cr1.17 , 19 - 24 although allohsct is clearly indicated in mrd - positive patients , it is important to study the value of approaches intended to induce mrd negativity before allohsct . 
it has been suggested that continued chemotherapy with one or two consolidation cycles may not be the preferred strategy to obtain an mrd - negative cr before allohsct , 48 but several new drugs are currently being developed and evaluated for aml.49 possible other strategies may include efforts to improve allogeneic immunotherapy by early tapering of immunosuppression and / or preemptive donor lymphocyte infusions , which also could be guided by mrd . 
of events / patients allo ct / auto hr & 95% ci ( ct / auto : allo ) reduction ( sd ) mrd status ( cut - off 0.1 ) negative positive 93 / 207 40 / 58 90 / 211 40 / 71 total 133 / 265 ( 50% ) 130 / 282 ( 46% ) allo better ct / auto better 45% ( 8 ) reduction 2p < .001 collectively , our study shows that the gvl effect was strikingly similar in mrd - positive and mrdnegative patients . 
additional prospective studies are needed to evaluate whether the conversion of mrd positivity into an mrd - negative remission before allohsct further optimizes outcome , and how the gvl effect after allohsct can be optimized . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . jurjen versluis no relationship to disclose burak kalin no relationship to disclose wendelien zeijlemaker patents , royalties , other intellectual property : i have a patent for a laboratory test to identify specific leukemia cells that can be used in patients with acute myeloid leukemia . 
manz consulting or advisory role : amgen , novartis , roche , pfizer marie - christiane vekemans consulting or advisory role : amgen ( inst ) , celgene ( inst ) , bristol - myers squibb ( inst ) , janssen ( inst ) , takeda ( inst ) travel , accommodations , expenses : amgen , bristol - myers squibb , teva , janssen bart j . 
bargetzi no relationship to disclose juergen kuball employment : gadeta stock and other ownership interests : gadeta consulting or advisory role : gadeta , novartis ( inst ) speakers bureau : gadeta research funding : gadeta , miltenyi biotec , novartis patents , royalties , other intellectual property : multiple patents on gamma - delta t cell receptor sequences isolation strategies and targets in combination with gamma - delta t cell receptor sequences travel , accommodations , expenses : gadeta , novartis , miltenyi biotec harry c . 
van der velden consulting or advisory role : celgene ( inst ) research funding : bd biosciences ( inst ) patents , royalties , other intellectual property : patent for euroflow mrd antibody tubes . 
janssen honoraria : bristol - myers squibb netherlands , pfizer europe consulting or advisory role : pfizer europe , novartis research funding : novartis travel , accommodations , expenses : novartis thomas pabst no relationship to disclose bob lowenberg consulting or advisory role : astex pharmaceuticals , clear creek bio , agio pharmaceuticals , celgene mojca jongen - lavrencic no relationship to disclose gerrit jan schuurhuis research funding : becton dickinson ( inst ) gert ossenkoppele honoraria : roche consulting or advisory role : celgene , sunesis pharmaceuticals , janssen , novartis , cti , amgen , pfizer , roche research funding : amgen ( inst ) , janssen ( inst ) , celgene ( inst ) travel , accommodations , expenses : roche jan j . 
cornelissen no relationship to disclose acknowledgment following dutch - belgian hemato - oncology cooperative group and the swiss group for clinical cancer research ( hovon - sakk ) publication rules , coauthorship was offered to centers contributing the highest number of patients . nevertheless , the authors highly appreciate the contribution of many physicians and data managers throughout hovonsakk , who made this analysis possible . affiliations jurjen versluis , burak kalin , bob lowenberg , mojca jongen - lavrencic , and jan j . 
van der velden , erasmus university medical center , rotterdam ; wendelien zeijlemaker , jeroen j.w.m. janssen , gerrit jan schuurhuis , and gert ossenkoppele , vu university medical center ; bart j . 
wijermans , haga hospital , the hague ; mels hoogendoorn , medical center leeuwarden , leeuwarden ; juergen kuball , university medical center utrecht , utrecht ; harry c . schouten , maastricht university medical center , maastricht , the netherlands ; jakob passweg , university hospital basel , basel ; markus g . 
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 c crizotinib failure in a tpm4alkrearranged inflammatory myofibroblastic tumor with an emerging alk kinase domain mutation inflammatory myofibroblastic tumors ( imts ) are a group of rare tumors usually presenting in children and young adults , most commonly in the abdomen , lung , and retroperitoneusurgical excision is the treatment of choice , but the tumors tend to recur locally . 
they show distinct pathologic and molecular features , and approximately one half of them express anaplastic lymphoma kinase ( alk ) protein1 , 2 as a result of alk gene fusions with a variety of partners.3 , 4 inhibition of alk is a valid therapeutic approach for alk - driven malignancies . 
there are currently three tyrosine kinase inhibitors ( tkis ) , crizotinib , ceritinib , and alectinib , approved for alk - positive nonsmall - cell lung cancer and several others tested in clinical trials.5 alk - tkis have shown encouraging results in several published cases of imt with alk rearrangements , 6 - 15 and the national comprehensive cancer network recommends crizotinib and ceritinib in imts with an alk translocation . herein , we present the case of a patient with an alk - positive imt of high - grade malignancy . after two debulking surgeries and hyperthermic intraperitoneal chemotherapy ( hipec ) treatment , the tumor relapsed , and the patient was treated with crizotinib . 
regarding family history , the patients paternal grandfather died at 75 years of pancreatic cancer , and both grandmothers died of colon cancer during their eighth decade . the patient had one debulking surgery at baseline , which was followed by hipec ( fig 1a )  . 
in both cases , histology and immunohistochemistry ( ihc ) were consistent with grade 3 imt expressing alk protein . one month after the second surgery , the ct scan showed a new mass between small intestinal loops . at this point , the patient was admitted to our department . a combined 18f - fluorodeoxyglucose positron emission tomography and ct ( pet / ct ) scan in april 2015 confirmed the presence of a hypermetabolic mass on the left lateral abdominal region ( fig 1b )  . 
fluorescent in situ hybridization ( fish ) was performed retrospectively for the two excised tumors , alk gene rearrangement was demonstrated in both instances , and the patient was started on oral crizotinib 250 mg twice daily ( fig 1a )  . 
green type : additional investigations , including tumor genotyping and phenotyping , germline genotyping , and cell - free dna testing for biologic samples that were obtained at the indicated time points . 
the primary retroperitoneal mass was surgically removed along with two peritoneal implants ; in addition , 27 lymph nodes , the sigmoid colon , and the meckel diverticulum were free of disease . 
on the basis of confirmatory alk immunohistochemistry ( ihc ) and fluorescent in situ hybridization ( fish ) for alk protein expression and gene rearrangement , respectively , the patient received crizotinib and experienced partial response ( 4 )  . 
the tumor grew despite crizotinib , and the patient had a third operation ; except for the mass , 36 cm of adjacent small intestine and 12 lymph nodes free of malignancy were also removed . 
the patient received adjuvant ceritinib , had a negative positron emission tomography ( pet ) / ct scan 14 months later , and remains disease - free ( 6 )  . 
left : strong 18ffluorodeoxyglucose uptake by the relapsed tumor before crizotinib ; middle : subtle uptake after 2.5 months of crizotinib ; right , horizontal and vertical : no uptake after 14 months of ceritinib . 
as of this writing , the patient is in the 21st month of ceritinib without clinical signs of progression or drug - related toxicity . to characterize the alk fusion partner ( figs 2a and 2b ) and to investigate the cause of resistance to crizotinib , the baseline and the postcrizotinib tumors ( fig 1a ) were submitted for genotyping to neo new oncology , cologne , germany . 
dna isolated from paraffin - embedded sections was sheared and subjected to hybrid capturebased next - generation sequencing ( illumina , san diego , ca ) with the neoplus assay ; genomic alterations ( point mutations , small insertions and deletions , copy number changes , and translocations ) were analyzed using neo new oncologys proprietary computational biology analysis pipeline . 
the three vertical microphotograph panels correspond to the three tumors excised from the patient , as indicated . gray stars : tumors submitted for next - generation sequencing genotyping ; tumor cell content at baseline and postcrizotinib was 60% and 80% , respectively . ( a ) hematoxylin and eosin sections showing the initial high - grade sarcoma at baseline , many apoptotic bodies and myxoid stroma after hyperthermic intraperitoneal chemotherapy ( hipec ; inset ) , and morphology similar to baseline and postcrizotinib . 
note the separate green and red dots ( arrows ) , and the multiple copies of the alk locus in occasional nuclei ( arrowheads ; up to five copies per nucleus )  . 
 ( c ) targeted next - generation sequencing revealed the breakpoint ( vertical line ) in intron 8 of tpm4 and intron 19 of alk , and the fusion of the two genes at dna level . 
 ( d ) the graphic representation shows the resulting tpm4 - alk protein ( not to scale ) that was strongly expressed as detected with immunohistochemistry ( clone d5f3 [ ventana , basel , switzerland ] , 1 : 250 ) in all three tumors of the patient . 
the integrative genomics viewer screenshots at the bottom show that the postcrizotinib tumor carried a c.3383g.c substitution at chromosomal position 2 : 29445450 ( grch 37 ) , whereas the same position in the baseline tumor was free of changes ; the reads were of high quality and the position was covered at high depth in both tumors , with assay sensitivity  . 
the substitution localized in exon 21 of the alk gene resulting in the p.g1128a activating mutation ( cosm98475 ) in the kinase domain of the protein ( red star )  . 
in the absence of copy number alterations and at 80% tumor cell content , the observed 13% variant allele frequency for alk c.3383g.c suggested that the new mutation was present in approximately 33% of the neoplastic cells in the crizotinib - resistant tumor . 
 an extremely rare single - nucleotide polymorphism ( snp ; rs750032802 at national center for biotechnology information ; exac minor allele frequency 1 / 106 to 1 / 107 ) of unknown functional significance . 
on the basis of this finding , and also to observe treatment effects on tumor inflammatory infiltrates , we applied ihc for bcl6 , cd138 , cd3 , cd8 , and pd - l1 protein expression on all three tumors ( fig 3 )  . 
in comparison with the baseline tumor , t - cell and cytotoxic t - cell rate declined on hipec and further on crizotinib , whereas pd - l1 was expressed in the postcrizotinib tumor only . on the basis of the patients family history , germline genotyping was performed with the illumina trusight cancer sequencing panel at the molecular diagnostics laboratory , national center for scientific research demokritos . 
this variant lies within the kinase domain but outside the atp - binding pocket , which is targeted by epidermal growth factor receptor tkis ; thus , at present , it appears clinically irrelevant . 
for this sample , the sensitivity of the test was not reached because of low cell - free dna quantity , which was indication of disease considered an additional absence ( no tumor dna shedding )  . discussion apparently , tpm4 - alk is the driving genomic alteration of the present imt , because it was persistent in every tumor this patient developed . although less frequent than tpm3 - alk , tpm4alk fusions are described in imt.3 , 4 the second recurrence in our patient was crizotinib resistant . the most likely resistance mechanism seemed to be the emergence of the alk kinase domain p.g1128a mutation , which is described herein as a novel crizotinib - resistance mutation in imt . 
notably , aside from alk p.g1128a , which was present in approximately 33% of the neoplastic cells , additional resistance mechanism ( s ) may have operated in the present imt . in experimental models , immune escape has been proposed as a mechanism of crizotinib resistance in alk - rearranged lung cancer ( eg , through stat3 activation ) .18 in clinical research , eml4alkrearranged lung adenocarcinomas are reported to express pd - l1 , 19 , 20 which may decrease after crizotinib19 ; these results are , however , not directly comparable to our case , which differs in tumor type and alk translocation . 
here , in three sequential tpm4 - alkrearranged imts from the same patient , we observed a drop in t cell infiltrates and induction of pd - l1 after crizotinib , indicating a different state of immune escape21 in the resistant tumor compared with baseline , which may have contributed to crizotinib resistance as well , together with the emerging alk kinase domain mutation . 
immunohistochemistry pictures are shown for ( a ) bcl6 ( germinal center differentiation factor ; clone pg - b6p [ thermo fisher scientific , paisley , united kingdom ] , 1 : 150 ) ; ( b ) cd138 ( plasma cell marker ; clone mi15 [ thermo fisher scientific ] , 1 : 50 ) ; ( c ) cd3 ( t cells ; clone ps1 [ novocastra , newcastle - upon - tyne , united kingdom ] , 1 : 50 ) ; ( d ) cd8 ( cytotoxic t cells ; clone c8 / 1444b [ dako , glostrup , denmark ] ) ; ( e ) pd - l1 ( immune checkpoint ligand ; clone cal10 [ biocare medical , pacheco , ca ] , ready to use )  . 
as shown in ( a ) , bcl6 protein expression was focally positive in the neoplastic nuclei at baseline ( inset ; overall 15% positive nuclei ) but absent after treatments , indicating that bcl6 p.p139l is not related to the expression of the corresponding prote ( b ) with cd138 , plasma cells were present and positive in all three tumors ; interestingly , 50% of the neoplastic cells at baseline were strongly positive with a diffuse cytoplasmic staining ( inset ) , 25% of the neoplastic cells exhibited intermediate positivity posthyperthermic intraperitoneal chemotherapy ( hipec ) , and a rough granular cytoplasmic pattern was observed in 70% of the neoplastic cells postcrizotinib ( inset )  . 
 ( c , d ) tumor - infiltrating cd3and cd8 - positive t cells constituted 30% and 25% of the tumor tissue population at baseline , respectively ; the rate of both phenotypes decreased to 15% post - hipec and to 2% and 1% postcrizotinib , respectively ( turquoise arrows )  . 
 ( e ) pd - l1 expression followed the opposite pattern as compared with cd3 ; it was completely absent at baseline and post - hipec , but it was present , albeit focally , in neoplastic cells postcrizotinib ( cytoplasmic and membranous staining , inset ) , with an overall positivity of 10% . 
bcl6 and cd138 protein expression by the neoplastic cells are novel reports in imt ; their role , if any , in the biology of these tumors needs to be elucidated . in conclusion , we have presented the disease course of a patient with tpm4 - alkrearranged imt . 
the tumor was locally aggressive and developed resistance to crizotinib through the emergence of an alk kinase domain mutation described for the first time in imts and potentially also through the induction of immune escape . 
cessna mh , zhou h , sanger wg , et al : expression of alk1 and p80 in inflammatory myofibroblastic tumor and its mesenchymal mimics : a study of 135 cases . 
butrynski je , dadamo dr , hornick jl , et al : crizotinib in alk - rearranged inflammatory myofibroblastic tumor . 104 - 108 , 2015 n engl j med 363 : 1727 - 1733 , 2010 7 . 
sasaki t , okuda k , zheng w , et al : the neuroblastoma - associated f1174l alk mutation causes resistance to an alk kinase inhibitor in alk - translocated cancers . 
mosse yp , lim ms , voss sd , et al : safety and activity of crizotinib for paediatric patients with refractory solid tumours or anaplastic large - cell lymphoma : a childrens oncology group phase 1 consortium study . 
lancet oncol 14 : 472 - 480 , 2013 jacob sv , reith jd , kojima ay , et al : an unusual case of systemic inflammatory myofibroblastic tumor with successful treatment with alk - inhibitor . 
kimbara s , takeda k , fukushima h , et al : a case report of epithelioid inflammatory myofibroblastic sarcoma with ranbp2 - alk fusion gene treated with the alk inhibitor , crizotinib . 
subbiah v , mcmahon c , patel s , et al : stump unstumped : anti - tumor response to anaplastic lymphoma kinase ( alk ) inhibitor based targeted therapy in uterine inflammatory myofibroblastic tumor with myxoid features harboring dctn1 - alk fusion . 
ono a , murakami h , serizawa m , et al : drastic initial response and subsequent response to two alk inhibitors in a patient with a highly aggressive alk - rearranged inflammatory myofibroblastic tumor arising in the pleural cavity . lung cancer 99 : 151 - 154 , 2016 14 . 
nishio m , murakami h , horiike a , et al : phase i study of ceritinib ( ldk378 ) in japanese patients with advanced , anaplastic lymphoma kinase - rearranged nonsmall - cell lung cancer or other tumors . 
mansfield as , murphy sj , harris fr , et al : chromoplectic tpm3 - alk rearrangement in a patient with inflammatory myofibroblastic tumor who responded to ceritinib after progression on crizotinib . 
cuy`as e , perez - sanchez a , micol v , et al : stat3 - targeted treatment with silibinin overcomes the acquired resistance to crizotinib in alk - rearranged lung cancer . 
gainor jf , shaw at , sequist lv , et al : egfr mutations and alk rearrangements are associated with low response rates to pd - 1 pathway blockade in nonsmall cell lung cancer : a retrospective analysis . 
koh j , jang jy , keam b , et al : eml4 - alk enhances programmed cell death - ligand 1 expression in pulmonary adenocarcinoma via hypoxia - inducible factor ( hif ) - 1a and stat3 . 
laboratory tests , magnetic resonance imaging ( mri ) , and positron emission tomographycomputed tomography did not indicate involvement of organs other than the skbecause of the limited cutaneous lesions classified as single system lch , topical corticosteroids were used as first - line treatment for 10 weeks , with no improvement . 
treatment with desmopressin ( initial dosage , 0.4 mg daily divided into three doses ) was started , and polyuria and polydipsia improved . function of the anterior pituitary was not affected . targeted next - generation sequencing of the skin biopsy indicated an activating mutation in mek1 ( p.e102_i103delei ; fig 3 )  . 
for this mutation , ex vivo sensitivity to an mek inhibitor ( meki ) has been reported.1a because the skin and the pituitary gland were affected , the disease was now classified as multisystem lch . 
finally , an off - label treatment with trametinib was offered to the patient after interdisciplinary discussion . after detailed explanation and obtaining informed consent , trametinib ( 2 mg once daily ) was started . an mri performed 4 weeks later showed a significant shrinkage of the pituitary enlargement ( fig 3 ) , and skin manifestations resolved both clinically and histologically ( fig 1 )  . 
positron emission tomographycomputed tomography and mri performed in week 12 of treatment showed a slight increase of the pituitary gland in size ; however , the patient had not been receiving trametinib in the previous 3 weeks . 
importantly , the daily dose of desmopressin could be reduced to 0.1 mg / d on trametinib treatment , and anterior pituitary function remained normal . because of the excellent overall response , a drug holiday was recommended , and trametinib treatment was stopped in week 38 . 
hematoxylin and eosin ( h&e ) staining and immunohistochemistry of langerin of a biopsy taken from cutaneous lesions before therapy ( left panels ) and after 4 weeks of therapy ( right panels )  . 
initially , a band - like infiltrate by histiocytes with reniform nuclei and eosinophilic cytoplasm ( upper left , h&e ) reactive with an antilangerin antibody ( brown , lower left ) was observed in the upper dermis and also perifollicular in the lower dermis . 
roughly , clinical subtypes are divided into single system and multisystem ( ms ) forms.3 limited disease usually causes low morbidity , but ms - lch or leukemic forms are a severe threat for patients . organ involvement can cause significant morbidity in patients with lch . 
standard therapies for ms - lch in adults are cytotoxic regimens.4 , 5 radiotherapy is used to treat pituitary lch ; however , this contributes to gradual and often complete loss of anterior pituitary function.6 , 7 the mitogen - activated protein kinase ( mapk ) pathway is critical for cell survival and proliferation . it can be activated by various receptor tyrosine kinases but also by oncogenic mutations in braf or nras found in melanoma and other human malignancies . 
recently , recurrent oncogenic mutations affecting the mapk pathway have been described in lch.1a , 8 these mutations affect braf in approximately 50% and mitogenactivated protein kinase 1 ( map2k1 / mek1 ) in approximately 25% of patients . 
mutations in these genes seem to be mutually exclusive.8 in a multibasket trial for malignancies harboring brafv600 mutations , targeted therapy with the selective braf inhibitor ( brafi ) vemurafenib showed clinical activity in lch.9 besides selective brafi , other small molecules , such as meki , have been evaluated in cancers with oncogenic mapk activation.9 , 10 it has been proposed that activating mek1 mutations is a difficult target in the treatment of lch.3 however , no clinical data on mek inhibition in patients with lch have been reported so far . ( poly ) chemotherapy and radiation are considered standard of care for treatment of ms - lch.3 - 7 high rates of toxicity are observed in adults , and recovery of endocrine function of the pituitary gland is rarely observed with these therapies . 
in week 4 of therapy with trametinib , a significant shrinkage and only a residual contrast enhancement were found . after short - term treatment break , the posterior pituitary gland appeared slightly enlarged again in week 12 . 
in week 28 , size was normalized . representative sagittal images from t1 contrastenhanced magnetic resonance imaging sequences shown ; arrows indicate affected part of the hypophysis . pretreatment after 4 weeks after 12 weeks after 28 weeks harboring a somatic mutation in mek1 . 
radiotherapy and chemotherapy might eventually still have to be considered in these patients . it remains unclear if meki can induce durable responses in lch and non - lch with lasting functional recovery of organs involved . 
 ( b ) the wildtype braf sequencing result is shown with a dotted line and arrow highlighting the c.t1799 location where a braf v600e mutation would be detected if it had been present . 
moeller , dagmar f uhrer , lisa zimmer , antje sucker , dirk schadendorf , elisabeth livingstone , bastian schilling data analysis and interpretation : matina papapanagiotou , klaus g . 
t1799 uwe hillen honoraria : novartis consulting or advisory role : novartis , roche , therakos research funding : novartis ( inst ) travel , accommodations , expenses : novartis tobias t . 
moeller honoraria : pfizer , henning dagmar f uhrer honoraria : ipsen , sanofi , bayer healthcare pharmaceuticals , eisai , genzyme , sobi , pfizer consulting or advisory role : novartis ( inst ) , ipsen , sanofi , bayer , eisai , genzyme , sobi , pfizer research funding : novartis ( inst ) , pfizer ( inst ) , ipsen ( inst ) , novartis , pfizer travel , accommodations , expenses : ipsen , sanofi , bayer , eisai , genzyme , sobi , pfizer lisa zimmer honoraria : novartis , merck sharp & dohme , bristol - myers squibb , roche , merck , glaxosmithkline consulting or advisory role : novartis , bristol - myers squibb , merck sharp & dohme , roche travel , accommodations , expenses : novartis , bristolmyers squibb , amgen , merck sharp & dohme alexander roesch research funding : novartis travel , accommodations , expenses : roche , bristol - myers squibb , merck sharp & dohme , amgen , novartis klaus g . 
 dirk schadendorf honoraria : amgen , array , astra zeneca , bristol - myers squibb , immunocore , merck sharp & dohme , merck , novartis , pfizer , philogen , pierre fabre , regeneron , roche consulting or advisory role : amgen , array biopharma , astrazeneca , bristol - myers squibb , immunocore , merck sharp & dohme , merck , novartis , pfizer , philogen , pierre fabre , regeneron , roche speakers bureau : amgen , bristol - myers squibb , merck sharp & dohme , novartis , pierre fabre , roche research funding : amgen ( inst ) , array ( inst ) , bristol - myers squibb ( inst ) , immunocore , merck sharp & dohme ( inst ) , novartis ( inst ) , philogen ( inst ) , regeneron ( inst ) , roche ( inst ) , bristol - myers squibb , novartis travel , accommodations , expenses : amgen , array , astra zeneca , bristol - myers squibb , immunocore , merck sharp & dohme , merck , novartis , pfizer , philogen , pierre fabre , regeneron , roche elisabeth livingstone no relationship to disclose bastian schilling honoraria : novartis , roche , bristol - myers squibb , merck sharp & dohme consulting or advisory role : roche , bristol - myers squibb speakers bureau : roche , bristol - myers squibb , merck sharp & dohme research funding : bristol - myers squibb ( inst ) , merck sharp & dohme travel , accommodations , expenses : novartis , roche , bristol - myers squibb , amgen matina papapanagiotou , klaus g . 
m oller i , murali r , m uller h , et al : activating cysteinyl leukotriene receptor 2 ( cysltr2 ) mutations in blue nevi . mod pathol 30 : 350 - 356 , 2017 2 . 
girschikofsky m , arico m , castillo d , et al : management of adult patients with langerhans cell histiocytosis : recommendations from an expert panel on behalf of euro - histio - net . 
duan mh , han x , li j , et al : comparison of vindesine and prednisone and cyclophosphamide , etoposide , vindesine , and prednisone as first - line treatment for adult langerhans cell histiocytosis : a single - center retrospective study . 
endocrine 48 : 949 - 956 , 2015 imashuku s , kudo n , kaneda s , et al : treatment of patients with hypothalamic - pituitary lesions as adult - onset langerhans cell histiocytosis . 
hyman dm , puzanov i , subbiah v , et al : vemurafenib in multiple nonmelanoma cancers with braf v600 mutations . 1919 - 1923 , 2010 n engl j med 373 : 726 - 736 , 2015 10 . 
cascade testing is the systematic identification of relatives who are at risk for having the same mutation ( at - risk relatives ) and facilitating genetic testing for the usually , these individuals are unaffected , but they may benefit from early identification and risk management interventions . 
 currently , australian best practice guidelines recommend that genetic testing for unaffected individuals be facilitated by an appropriately trained health professional such as a genetic counselor or clinical geneticist.15 the purpose of this case report is to exemplify a collaboration between the departments of oncology and genetics to extend testing for a dpyd mutation to family members after the index case was identified . patient the index patient was diagnosed with metastatic breast cancer at age 59 years . 
 she developed locoregional recurrences in 2011 , bony metastases in 2013 , and further progression with liver , lung , bone , and soft tissue metastases in 2016 after multiple lines of endocrine therapy . 
with normal baseline renal function , she was prescribed capecitabine at 1 , 000 mg / m2 twice per day on days 1 to 14 in a 21 - day cycle . 
four weeks later , she began palliative paclitaxel to treat symptomatic cancer progression . the patients oncology team referred her to the department of genomic medicine at the royal melbourne hospital . 
the patients personal and family history of cancer had been assessed ; it was considered that there was no increased familial risk of breast ( or other ) cancers . the patients first - degree relatives were subsequently offered genetic counseling and testing for this pharmacogenomic mutation . 
communication of genetic results in families is known to be problematic for various reasons , including miscommunication or misunderstanding of genetic information and passive or active nondisclosure.20 - 22 in this case , family members were already in contact with the genetics service around the time of the index testing and were requesting testing themselves . 
a hypothetical pedigree showing the effect of systematic cascade testing for an autosomal dominant condition . to our knowledge , this is the only published case report of cascade genetic testing in the setting of dpyd pharmacogenomics . 
falvella and colleagues23 reported a case of dpyd genotyping before starting chemotherapy in a 38 - year - old man with colorectal cancer in the context of his mother having a known dpyd variant . 
our case differs in that we extended the dpyd genotyping systematically by offering it to all unaffected at - risk family members . fluoropyrimidines are commonly used drugs , and the cancers treated with these drugs are common in the general population . 
even though this family is not at an increased heritable risk of cancers , it is quite possible that members of the family may need this treatment regimen in the future . 
relationships are self - held unless noted . hereditary breast and ovarian cancer syndrome , cascade pharmacogenomics testing would be predicted to have greater utility because of the higher probability of relatives being affected by these cancers . in conclusion , this case provides an example of cascade testing of family members after an individual with dpd deficiency was identified . 
winship , university of melbourne , parkville , australia acknowledgment we acknowledge michael michael , md , consultant medical oncologist at peter maccallum cancer centre , for his input into an earlier version of this manuscript . support supported by a victorian state - funded clinical service . 
iacovelli r , pietrantonio f , palazzo a , et al : incidence and relative risk of grade 3 and 4 diarrhoea in patients treated with capecitabine or 5 - fluorouracil : a meta - analysis of published trials . 
meulendijks d , van hasselt jgc , huitema adr , et al : renal function , body surface area , and age are associated with risk of early - onset fluoropyrimidine - associated toxicity in patients treated with capecitabine - based anticancer regimens in daily clinical care . 
ison g , beaver ja , mcguinn wd jr , et al : fda approval : uridine triacetate for the treatment of patients following fluorouracil or capecitabine overdose or exhibiting early - onset severe toxicities following administration of these drugs . 
ma ww , saif mw , el - rayes bf , et al : emergency use of uridine triacetate for the prevention and treatment of life - threatening 5 - fluorouracil and capecitabine toxicity . 
henricks lm , opdam fl , beijnen jh , et al : dpyd genotype - guided dose individualization to improve patient safety of fluoropyrimidine therapy : call for a drug label update . 
lunenburg catc , henricks lm , guchelaar hj , et al : prospective dpyd genotyping to reduce the risk of fluoropyrimidine - induced severe toxicity : ready for prime time . 
liu d , li j , gao j , et al : examination of multiple ugt1a and dpyd polymorphisms has limited ability to predict the toxicity and efficacy of metastatic colorectal cancer treated with irinotecan - based chemotherapy : a retrospective analysis . 
claes e , evers - kiebooms g , boogaerts a , et al : communication with close and distant relatives in the context of genetic testing for hereditary breast and ovarian cancer in cancer patients . 
mcclaren bj , aitken m , massie j , et al : cascade carrier testing after a child is diagnosed with cystic fibrosis through newborn screening : investigating why most relatives do not have testing . 
in patients with stage iii or iv melanoma , early changes in ctdna within 1 month after initiation of treatment correctly predicted recist response categories in 19 of 20 patients . 
 braune et al context key objective we evaluated ctdna in stage iii and iv melanoma to detect active disease and to predict response to treatment . knowledge generated ctdna had superior sensitivity to ldh and s100 in detecting active disease in stage iv melanoma . 
written informed consent was obtained from all patients . isolation and quantitation of ctdna from plasma blood samples were collected in edta tubes ( sarstedt , n umbrecht , germany ) and centrifuged twice within the 2 hours after collection . 
the supernatant was stored at 80c . cell - free ctdna was extracted from 2 ml using the qiasymphony circulating dna kit ( qiagen , hilden , germany ) according to the manufacturers instructions and was eluted in 60 l of elution buffer . 
the limit of blank , limit of detection , and lowest detectable copy ratio were determined for each assay ( data supplement )  . imaging analysis imaging and quantitative analyses were performed by a single radiologist blinded to results of the ctdna analyses . 
workows for ct and magnetic resonance imaging are capable of automated segmentation and volume measurements . pet imaging and quantication 18f - uorodeoxyglucose scans were performed with a 64 - slice gemini tf positron emission tomography ( pet ) / ct scanner or a 16 - slice gemini tf big bore pet / ct scanner ( philips healthcare for both ) .17 a contrast - enhanced diagnostic ct ( 120 kvp , 100 , 400 mas , dose modulation applied ) or a low - dose ct ( 120 kvp , 25 mas ) scan was performed for attenuation correction and spatial allocation . 
for each pet study , a quantitative analysis was performed using rover v2.1.12 ( abx , radeberg , germany ) .18 , 19 a threshold of 40% of maximum standardized uptake value was chosen for the determination of the metabolic tumor volume ( mtv ) .20 statistical analysis data analysis was performed separately by stage for all eligible patients . 
correlations were calculated by using a log scale , and ldh and s100 measurements below the standard value were set to the standard value . within - patient correlation was accounted for in the correlation analysis and in the estimation of the progression - free survival ( pfs ) hazard ratio ( hr ) in stage iv patients . 
patient characteristics ( continued ) characteristic 66 ( 28 - 92 ) tissue mutation status braf exon 15 v600e v600k v600r k601n d594g l597s w604c nras q61 q61k q61r total patients female male age , years median ( range ) 60  . 
60 stage stage iii newly diagnosed previous treatment treatment after inclusion surgery surgery radiation systemic treatment relapsed previous treatment of relapse treatment of relapse after inclusion surgery radiation systemic treatment no . 
of previous lines of therapy stage iv mean ( range ) treatment at inclusion braf / mek inhibitor immunotherapy treatment after inclusion immunotherapy braf / mek inhibitor radiotherapy surgery interferon vaccination ( continued in next column ) 1.7 ( 0 - 7 ) * systemic treatment after progression to stage iv . three patients received systemic treatment for unresectable stage iii melanoma , and three patients received systemic treatment after progression to stage iv melanoma . total number of tissue mutations is 64 . 
patient 62 was tissue positive for nras q61r and braf w604c , patient 55 had resection of two different melanomas before inclusion in the study ( one was positive for braf v600e , and the other was positive for nras q61k )  . 
the mean number of samples was 6.8 ( range , 1 to 15 samples ) per patient with stage iii disease , and the mean was 5.8 ( range , 1 to 27 samples ) for stage iv patients . in patients with stage iii disease , 10 ( 83.3% ) of 12 were positive for ctdna at least once ; for patients with stage iv disease , 44 ( 88% ) of 50 patients were positive for ctdna at least once ( table 2 )  . 
s100 and ldh are indicated as being increased when level is above the normal range of , 0.105 mg / l for s100 and 135 to 225 u / l for ldh . 
we identied 10 stage iii and 30 stage iv patients with 56 samples obtained up to 30 days before surgery , initiation of systemic treatment , or change in systemic treatment . 
even when they were combined , ldh and s100 detected measurable disease in only 34 ( 60.7% ) of 56 samples before initiation of treatment ( table 3 ; fig 1c )  . 
thus , ctdna detected a higher proportion of patients with active disease . amount of mutated ctdna correlates with ldh and s100 to compare ctdna with the established biomarkers ldh and s100 , we studied measurement pairs obtained at the same time points . 
ctdna strongly correlated with s100 ( r = 0.64 based on 278 measurement pairs from 62 patients ) and ldh ( r = 0.50 based on 288 measurement pairs from 61 patients )  . ctdna reects tumor volume and metabolic activity we next asked whether mutant ctdna levels correlate with tumor burden . 
analysis was performed according to change in the sum of the diameters of target tumor lesions from baseline to rst ( fig 2a ) and subsequent ( fig 2b ) follow - up imaging scans according to recist 1.1. 
 ( a ) percentage of positive ( ctdna ) or increased ( lactate dehydrogenase [ ldh ] , s100 ) samples from 274 time points with matched ctdna , ldh , and s100 samples for stage iii and stage iv patients , respectively . 
red lines indicate the mean value for ctdna , ldh , or s100 . dotted lines indicate the thresholds of ldh ( 225 u / l ) and s100 ( 0.105 ug / l ) above which values are stated as being increased . 
 ( c ) sensitivity of ctdna , ldh , and s100 to detect disease within 30 days before surgery , initiation of treatment , or change in treatment ( see table 3 for details )  . 
of note , one patient who displayed a new lesion despite favorable ctdna course had an additional braf w604c mutation detectable at baseline that converted from negative at day 43 to positive at day 91 . 
conversely , all nine patients with partial response according to recist had a positive - to - negative conversion , had a decrease in ctdna , or remained ctdna negative . thus , early ctdna dynamics correctly predicted progressive disease or partial response according to recist in 21 of 24 patients . 
the remaining patient had a ctdna - positive sample available 1 day after imaging ( patient 60 ; fig 2c )  . ctdna predicts outcome we analyzed stage iii patients with a ctdna measurement within 30 days after surgery or at initiation of systemic therapy . 
four patients did not meet these criteria because they had no samples within 30 days after surgery ( n = 3 ) or at the initiation of systemic treatment ( n = 1 )  . 
thus , the higher levels of ctdna that appeared early after initiation of treatment or change in treatment indicated inferior pfs . dynamic ctdna proles of individual patients results of biomarker assessment in individual patients demonstrate that ctdna analysis over time is informative with respect to tumor dynamics as shown in the data supplement . 
ctdna demonstrated a superior dynamic signal range compared with ldh and s100 , and ctdna detected progression whereas ldh ( data supplement ) or ldh and s100 ( fig 1c , g ) failed to detect progression . 
of note , the combination of all three biomarkers provides an 8.9% increase in sensitivity to ctdna alone . thus , ctdna might be used together with ldh and s100 in a combined biomarker score . 
we observed a signicant association of ctdna at baseline with ldh , s100 , tumor size , and mtv ( r2 = 0.87 ) , the latter displaying the strongest correlation . 
this is in agreement with two other studies demonstrating a strong correlation between the number of ctdna copies and mtv in melanoma ( r = 0.63 , 23 and r2 = 0.6949 , 24 respectively )  . 
 ( d ) correlation between ctdna and ( continued on following page ) recist 1.1 , ( e ) tumor volume at baseline assessed by radiologic analysis , and ( f ) tumor metabolic activity , assessed by positron emission tomography / computed tomography ( pet / ct ) scan and expressed as the mean total lesion glycolysis ( tlg ) in [ g / ml x ccm ]  . 
the tlg in the equation [ g / ml x ccm ] was calculated by multiplying the lesion volume with the mean standardized uptake value in the volume of interest . 
eleven patients with stage iii and 22 with stage iv disease with a baseline ctdna sample , radiographic imaging before intervention , and a ctdna sample taken within 30 days after initiation of treatment or change in treatment were analyzed . 
 ( a ) waterfall plot showing the change in sum of diameter ( sod ) of target tumor lesions from baseline to rst follow - up imaging according to recist 1.1 in relation to early changes in ctdna . 
t0 denotes baseline ctdna sample , and t1denotes rst sample after baseline at day 8 to 28 after initiation of or change in treatment with ctdna detectable ( + ) or not detectable ( )  . 
dotted lines represent 20% increase in sod , which indicated progressive disease ( pd ) , or 30% decrease , which indicated partial response ( pr ) according to recist 1.1. 
 ( b ) spider plot showing changes in sod from baseline to rst and subsequent follow - up imaging according to early ctdna dynamic changes from baseline to rst sample after baseline taken within 28 days after institution of or change in treatment . 
cr , complete response ; sd , stable disease . importantly , early changes in ctdna levels were superior to ldh and s100 for early assessment of treatment response . of all the patients who achieved partial response , 76.9% had favorable ctdna dynamics as early as 8 to 28 days after initiation of or change in treatment . 
in line with these observations , detectable ctdna as early as within 30 days after initiation of or change to therapy predicted inferior pfs for patients with stage iii or iv disease . 
in stage iv disease , ctdna with more than 10 copies per ml within 30 days after initiation of or change in treatment indicated a population with a particularly short pfs of only 4 months . 
we included patients who were alive and free of progression 1 month after surgery or at the start of systemic therapy and who had a ctdna measurement within 1 month . 
pfs was dened as the time from initiation of treatment to rst reported progression or to the most recent visit . progression events included progression as dened by recist 1.1 , clinical progression , or melanoma - specic death . 
 ( a ) pfs in eight patients with stage iii disease alive and free of progression after 1 month with a ctdna measurement within 1 month after surgery or start of systemic treatment . 
 ( b - c ) pfs in 36 patients with stage iv disease with 46 pfs sections , alive and free of progression at 1 month by the rst ctdna value taken within 30 patients with days ( median , day 22 ; range , days 1 to 30 ) after start of or change in systemic treatment with a ctdna measurement within 1 month , by ( b ) positive v negative , and ( c ) negative or 10 or fewer copies per ml v more than 10 copies per ml . 
our data suggest that ctdna dynamics allow prediction of response and pfs within in the rst month after implementing braf / mek inhibitors or immunotherapy . in contrast to previous reports , 27 - 30 ctdna at baseline was not a prognostic marker for pfs in patients with stage iv disease in our cohort , whereas the level of ctdna at rst measurement after baseline was clearly predictive for pfs , most likely as an expression of response to treatment . notably in the aforementioned studies , most patients were treated with braf / mek inhibitors whereas the majority of our patients received immunotherapy . 
in two other studies of patients with or without melanoma who were receiving pd - 1 antibodies , there was no association between baseline ctdna and pfs.25 , 31 however , subgroup analyses did not reveal signicant differences because this study was not designed to examine the signicance of baseline ctdna in patients treated with braf / mek inhibitors versus immunotherapy . 
 braune et al nras mutations.27 , 32 this is a possible explanation for the increasing copies of nras - mutated ctdna detected in patient 53 after changing the treatment to dabrafenib and trametinib , which suggests selection of a subclonal mutation that mediates resistance to treatment with braf / mek inhibitors . 
nevertheless , previous studies have demonstrated tumor interand intraheterogeneity involving additional genetic events that lead to mapk or pi3k / pten / akt reactivation when disease progresses during treatment with braf inhibitors.33 , 34 few studies address the use of ctdna as a biomarker in stage iii melanoma . 
but in one recent study , ctdna positivity within 12 weeks after surgery indicated adverse disease - free survival and os.35 in our cohort , ctdna positivity after resection of the primary tumor and within 1 month after denitive locoregional treatment or start of systemic therapy predicted a poor pfs . 
with adjuvant therapies showing benet for high - risk stage iii melanoma , 9 , 10 ctdna positivity might help to stratify patients for adjuvant treatment . one limitation of this study is the small sample size . 
validation in a larger prospective trial is required , especially for detection of minimal residual disease in stage iii and to examine whether changes of ctdna early after the start of treatment constitute an independent marker for pfs and os for braf / mek inhibitor treatment versus immunotherapy . 
although mutationspecic assays might be most suitable for monitoring response and minimal residual disease , a broader sequencing approach using next - generation sequencing might be used in previously treated patients to track subclonal mutations to understand treatment resistance and to guide further therapy.34 in addition , including tert promoter mutations present in 70% of melanomas36 could increase coverage when added to brafand nrasspecic ctdna assays.37 in conclusion , our results demonstrate that ctdna is superior to ldh and s100 for detecting active disease and suggest that changes in ctdna early after initiation of treatment predict response to treatment and pfs . 
 ctdna as a biomarker in malignant melanoma dagmar von bubnoff honoraria : roche , iomedico travel , accommodations , expenses : bristol - myers squibb frank meiss honoraria : bristol - myers squibb , novartis , pierre fabre consulting or advisory role : bristol - myers squibb , novartis , pierre fabre , roche pharma ag speakers bureau : bristol - myers squibb travel , accommodations , expenses : novartis , bristol - myers squibb , pierre fabre nikolas von bubnoff honoraria : astrazeneca , amgen , bristol - myers squibb , novartis consulting or advisory role : novartis ( inst ) research funding : novartis ( inst ) no other potential conicts of interest were reported . acknowledgments the authors thank renata koch and aurelia winter for sample collection , patient management , and administrative support . references cancer genome atlas network : genomic classication of cutaneous melanoma . 
cell 161 : 1681 - 1696 , 2015 dummer r , ascierto pa , gogas hj , et al : overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 19 : 1315 - 1327 , 2018 long gv , flaherty kt , stroyakovskiy d , et al : dabrafenib plus trametinib versus dabrafenib monotherapy in patients with metastatic braf v600e / k - mutant melanoma : long - term survival and safety analysis of a phase 3 study . 
weber js , gibney g , sullivan rj , et al : sequential administration of nivolumab and ipilimumab with a planned switch in patients with advanced melanoma ( checkmate 064 ) : an open - label , randomised , phase 2 trial . 
lancet oncol 17 : 943 - 955 , 2016 topalian sl , sznol m , mcdermott df , et al : survival , durable tumor remission , and long - term safety in patients with advanced melanoma receiving nivolumab . j clin oncol 32 : 1020 - 1030 , 2014 schadendorf d , hodi fs , robert c , et al : pooled analysis of long - term survival data from phase ii and phase iii trials of ipilimumab in unresectable or metastatic melanoma . 
j clin oncol 33 : 1889 - 1894 , 2015 barbour ap , tang yh , armour n , et al : braf mutation status is an independent prognostic factor for resected stage iiib and iiic melanoma : implications for melanoma staging and adjuvant therapy . 
hofheinz f , p otzsch c , oehme l , et al : automatic volume delineation in oncological pet : evaluation of a dedicated software tool and comparison with manual delineation in clinical data sets . 
krohn t , kaiser hj , gagel b , et al : 3d volume and suv analysis of oncological pet studies : a voxel - based image processing tool with nsclc as example [ in german ]  . 
welsh jl , bodeker k , fallon e , et al : comparison of response evaluation criteria in solid tumors with volumetric measurements for estimation of tumor burden in pancreatic adenocarcinoma and hepatocellular carcinoma . 
gonzalez - cao m , mayo de las casas c , jordana ariza n , et al : early evolution of brafv600 status in the blood of melanoma patients correlates with clinical outcome and identies patients refractory to therapy . 
gonzalez - cao m , mayo - de - las - casas c , molina - vila ma , et al : braf mutation analysis in circulating free tumor dna of melanoma patients treated with braf oncotarget 6 : 42008 - 42018 , 2015 inhibitors . 
santiago - walker a , gagnon r , mazumdar j , et al : correlation of braf mutation status in circulating - free dna and tumor and association with clinical outcome across four brafi and meki clinical trials . 
ascierto pa , minor d , ribas a , et al : phase ii trial ( break - 2 ) of the braf inhibitor dabrafenib ( gsk2118436 ) in patients with metastatic melanoma . 
cabel l , riva f , servois v , et al : circulating tumor dna changes for early monitoring of anti - pd1 immunotherapy : a proof - of - concept study . 
long gv , fung c , menzies am , et al : increased mapk reactivation in early resistance to dabrafenib / trametinib combination therapy of braf - mutant metastatic 28 : 1996 - 2001 , 2017 melanoma . 
mcevoy ac , calapre l , pereira mr , et al : sensitive droplet digital pcr method for detection of tert promoter mutations in cell free dna from patients with metastatic melanoma . 
lum , md1 ; shirley zhu , md , mph1 ; sujay vennam1 ; erna forg o , md1 ; sushama varma , ms1 ; kristen ganjoo , md1 ; trevor hastie , phd3 ; rafck bowen , phd1 ; maria debiec - rychter , md , phd2 ; and matt van de rijn , md , phd1 purpose the preoperative distinction between uterine leiomyoma ( lm ) and leiomyosarcoma ( lms ) is difcult , which may result in dissemination of an unexpected malignancy during surgery for a presumed benign lesion . an assay based on circulating tumor dna ( ctdna ) could help in the preoperative distinction between lm and lms . 
we also proled 36 lm tumor specimens by exome sequencing to develop a panel for targeted detection of point mutations in ctdna of patients with lm . results we identied tumor - derived cnas in the plasma dna of 50% ( six of 12 ) of patients with lm . 
we identied only two recurrently mutated genes in lm tumors ( med12 and acly )  . conclusion our results show that lms do shed dna into the circulation , which provides an opportunity for the development of ctdna - based testing to distinguish lm from lms . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction uterine leiomyomas ( lms ) are common benign smooth muscle tumors that may present with symptoms similar to those associated with uterine leiomyosarcoma ( lms ) , a rare malignant tumor with a poor prognosis.1 with the exception of endometrial lesions , most uterine masses are not biopsied before surgery , and the preoperative distinction between benign and malignant uterine smooth muscle tumors relies primarily on clinical evaluation and imaging . 
as a result , patients may undergo surgery without a denitive distinction between the two entities . it is estimated that one in nine women in the united states will undergo a hysterectomy for benign gynein their lifetime.2 cologic indications , such as lm , power morcellation used to be performed in many in 2014 the us food and drug such cases , until administration discouraged the use of power morcellation for the removal of the uterus or uterine masses , after reporting that this procedure may lead to inadvertent retroperitoneal spread of an unsuspected malignancy in one in 305 patients.3 however , intraabdominal manual morcellation is still performed in patients with large masses diagnosed as lm , and although this is less aggressive than power morcellation , it still carries a risk for dissemination of an unexpected lms . 
risk factors that may favor the diagnosis of lms over lm include postmenopausal status , tamoxifen use , history of retinoblastoma , pelvic irradiation , hereditary leiomyomatosis , and renal cell cancer syndrome , 4 but these factors do not always correlate with a diagnosis of lms . also , the new emerging magnetic resonance imaging techniques present unsatisfactory positive predictive values for the distinction between lm and lms.4 therefore , there is a high need for improved methods for preoperative discrimination between benign lm and malignant tumors . 
in an attempt to improve the distinction between lm and lms , nagai et al5 developed a revised preoperative sarcoma score ( rpress ) based on patients age , serum lactate dehydrogenase ( ldh ) levels , and endometrial cytology ndings . 
 przybyl et al context key objective we sought to explore the feasibility of distinguishing between uterine leiomyoma and leiomyosarcoma based on the analysis of tumor - specic aberrations in circulating tumor dna ( ctdna )  . 
for this purpose , in the current study we aimed to determine whether uterine leiomyomas shed dna into the circulation . knowledge generated we demonstrate that it is feasible to detect ctdna derived from leiomyomas . 
in the limited number of cases analyzed to date , we show that these benign tumors do not carry alterations in tumor suppressor genes that can be detected in the ctdna of most patients with leiomyosarcoma . relevance our ndings are a rst and necessary step toward developing a blood test that , together with clinical and imaging information , ultimately could help clinicians to better evaluate the risk of leiomyosarcoma in a patient presenting with a uterine mass . was developed in a group of 63 patients with lm and lms but has not yet been validated in an independent study . we recently demonstrated that tumor - associated genetic aberrations can be detected in the circulating tumor dna ( ctdna ) of patients with lms.6 in that study , we used two technologies to detect different classes of genomic aberrations in plasma dna : cancer personalized proling by deep sequencing ( capp - seq ) for the analysis of point mutations , 7 , 8 and a genome - wide interrogation of copy number alterations ( cnas ) by shallow whole - genome sequencing.9 , 10 using these two approaches , we were able to detect ctdna in six of seven patients with lms with  . 
the study was approved by the stanford university institutional review board ( irb - 31067 )  . proling plasma cell - free dna cell - free dna was extracted from plasma using qiaamp circulating nucleic acid kit ( qiagen )  . 
sequencing libraries were prepared with the truseq chip preparation kit ( illumina , foster city , ca ) and sequenced using hiseq 2500 instrument ( illumina ) ( data supplement )  . plasma ldh measurement plasma ldh levels were measured on a roche cobas 8000 ( roche , indianapolis , in ) automated platform ( data supplement )  . proling tumor specimens genomic dna extracted from 12 archival lm tumor specimens and germline dna extracted from patient - matched blood leukocytes were used for genome - wide copy number proling with the oncoscan ffpe assay ( thermo fisher scientic / affymetrix , santa clara , ca )  . thirty - six archival lm tumor specimens and normal patientmatched counterpart tissues or peripheral blood leukocytes were used for whole - exome sequencing using the seqcap ez human exome v3.0 library ( roche ) on hiseq 4000 instrument ( illumina ) ( data supplement )  . results tumor - derived copy number aberrations can be detected in plasma dna of patients with lm to explore the possibility of developing a blood - based test for the distinction between lm and lms , we rst determined whether lm can shed dna in the blood . 
we calculated genome - wide segmented z - scores in plasma cell - free dna , and we intersected each genomic region of cnas identied in the eight lm tumor specimens with the segments identied in plasma dna of the matching patients . 
of the 33 cnas detected in the eight tumor specimens , 30 cnas had the same type of copy number alteration in tumor and plasma dna ( ie , matching dna copy number gain or loss ; data supplement )  . 
1.5 in cell - free dna , we found 11 tumor - derived cnas in the plasma dna of six patients with lm ( correlation between log2 ratio in the tumor and z - score in the plasma determined by linear regression was r2 = 0.74 ; p value = .0007 ; table 3 ; appendix fig a1 )  . 
selected large dna cnas identied in lm tumor specimens were not detected in plasma specimens , which is most likely the result of the limit of detection of our method and / or the effect of stochastic sampling of blood specimens . 
we have previously demonstrated that it is possible to detect tumorderived cnas in cell - free dna among patients with lms using the same technology as applied to the patients with lm in the current study.6 we sought to verify whether the aberrations found in ctdna of patients with lm in the present report are specic to these benign tumors or whether the same aberrations could be found also in lms tumor specimens . 
for this purpose , we reanalyzed the previously generated genomic proles of 22 tumors from seven patients with lms using exactly the same criteria as were used for the lm tumor specimens . 
our results show that 10 of 11 genomic aberrations found in the ctdna of patients with lm were also present in the tumor dna of patients with lms analyzed in our previous study , 6 with a median of four aberrations per lms tumor sample ( range , 1 - 8 )  . 
these results demonstrate that the majority of cnas found in lm tumors are not specic for this entity ; therefore , proling these cnas in plasma dna may not be useful to distinguish between lm and lms . 
on the other hand , cnas found in lm specimens did not affect any of the frequently deleted tumor suppressor genes in lms ( eg , tp53 , rb1 , atrx , pten , atm , or cdkn2a )  . 
therefore , the detection of cnas in these tumor suppressor genes in ctdna may favor a diagnosis of lms . patient age and levels of ldh do not allow for distinction between lm and lms previous studies have proposed that ldh level measurements and patient age may be helpful in the distinction between lm and lms.5 , 11 we evaluated the ldh levels in plasma specimens of nine of 12 patients with lm proled for the presence of ctdna and eight untreated patients with uterine lms . 
in the rpress algorithm , the cutoff of serum ldh levels indicative of lms was set at 279 u / l.5 in our group of patients , the sensitivity and specicity values of this test were found to be only 50% and 89% , respectively . 
the mean age of the patients with lm and lms was 48 and 54 years , respectively ( t test two - tailed p value = .19 ; fig 2b )  . 
this performance was poorer than the ndings reported in the rpress study , where the sensitivity , specicity , positive predictive value , and negative predictive value were 93% , 65% , 45% , and 97% , respectively.5 low mutation burden in lm previous genomic studies of lm have identied med12 as the most frequently mutated gene in these lesions , but these studies did not report on other recurrent somatic mutations in these tumors.12 - 14 however , med12 mutations have been reported also in a subset of lms tumors , and therefore these mutations cannot be used for a molecular distinction between lm and lms.15 to investigate whether lm tumors might have recurrently mutated genes other than med12 , we performed whole - exome sequencing on 36 pairs of matched tumor and normal dna specimens from patients with lm . 
mutations in exon 2 of med12 were identied in 39% ( 14 of 36 ) of lm tumor specimens , and the acly gene was mutated in 6% ( two of 36 ) of lm tumor specimens ( data supplement )  . 
mutations in these two genes were present in 15 of 36 patients , with a median of one mutation per tumor ( range , 0 - 2 across all 36 tumors )  . 
all med12 mutations identied in our study were previously reported in the cosmic database ( cosmic v84 ; accessed on november 12 , 2018 ) .16 our results show that recurrent mutations other than in the med12 gene rarely occur in lm . 
importantly , we did not detect in any lm case any of the mutations in tumor suppressor genes that are frequently mutated in lms , such as tp53 , rb1 , pten , atrx , atm , and arid1a.6 this indicates that mutations in these driver genes may be highly specic to malignant tumors such as lms . 
because lms do not carry mutations in these tumor suppressor genes , we propose that detection of these mutations in plasma dna of patients with uncertain diagnosis , using the capp - seq lms - specic panel developed in our previous study , may favor the diagnosis of lms . discussion the clinical utility of ctdna proling has been widely demonstrated in malignant tumors that harbor highly recurrent mutations.7 , 8 , 17 , 18 currently , the two most frequently used sequencing - based approaches for ctdna monitoring include deep targeted sequencing for ultrasensitive quantitative analysis of point mutations , such as capp - seq , and shallow whole - genome sequencing for the detection of cnas . 
histologic appearance of representative leiomyoma ( lm ) cases with ( a ) no detectable dna copy number alterations , ( b ) 20 dna copy number alterations , and ( c ) six dna copy number alterations . 
however , it is not practical to design an lm - specic capture panel for detection of point mutations by deep targeted sequencing of ctdna , because we identied only two recurrently mutated genes in a low percentage of 36 lm tumors . we assume that an approximately two - fold increase of coverage may result in improving the reliability of the calls , by reducing the number of false - positive calls and increasing the number of true - positive calls.22 moreover , most of the patients included in our study had multifocal disease , and we expect that proling all nodules from these patients would reveal a wider spectrum of cnas and thus allow for the detection of overlapping aberrations between plasma and tumor dna in a higher percentage of patients with lm . although ctdna released from malignant tumors has been well characterized in multiple types of cancer , ctdna derived from benign lesions has not been extensively studied . an incidental nding of lm - derived dna in the circulatory system has been reported in pregnant women undergoing noninvasive prenatal testing ( nipt )  . 
dharajiya et al19 reported unexpectedly abnormal nipt proles in 55 of 450 , 000 pregnant women tested for fetal aneuploidy ; 20 of these 55 women were known to have had lm at the time of nipt . 
but the genomic prole of a matching tumor was examined only in a single patient from this group to conrm levels of cell - free dna were indeed that the abnormal derived from this lm.19 although these incidental ndings indicated that lm can shed dna into the circulatory system , the overall sensitivity of shallow whole - genome sequencing for the detection of lm - derived ctdna has not been investigated . 
in the current study , by prospective analysis of plasma and tumor samples of 12 patients with lm , we found ctdna in 50% of these patients , which is a comparable detection rate to the current sensitivity of ctdna detection in many stage i cancers.20 , 21 importantly , the nipt assays used for detecting fetal abnormalities usually focus solely on screening for monosomy or trisomy of chromosomes 13 , 18 , and / or 21 . 
in the current study , instead of focusing only on selected chromosomes , we performed a genome - wide analysis in which we aimed to detect not only chromosome - wide aberrations but also small focal aberrations . 
we performed shallow whole - genome sequencing at approximately 0.1 genomewide coverage ; however , we expect that deeper sequencing would allow for the detection of ctdna in a higher percentage of patients with lm . 
on the basis of previously published studies , it must be noted that the development of a reliable assay for the distinction between lm and lms is challenged by the great difference in prevalence of these two entities . 
 circulating tumor dna in leiomyoma predictive value for any positive result indicating lms would be only 2% , while the negative predictive value of a negative result would be 99.99%. 
on the basis of the genomic proles of lm and lms , we propose that it may be more practical to apply an assay that would rule out the diagnosis of lm . 
this could be possible by applying capp - seq for detection of mutations in tumor suppressor genes that are frequently mutated in lms but have never been reported in lm . 
regardless , given the statistical considerations on the prevalence of lm and lms , validation of such assay in the clinical setting may be challenging and would require a very large prospective study . in summary , we demonstrate in the current study that a substantial portion of lms do shed dna into the circulatory systethese ndings provide an opportunity to develop a noninvasive test for distinction between lm and lms on the basis of ctdna in plasma . 
lyon , iarc , 2014 , in kurman rj , carcangiu ml , herrington cs , et al ( eds ) : who classication of tumours of female reproductive organs . 
nagai t , takai y , akahori t , et al : highly improved accuracy of the revised preoperative sarcoma score ( rpress ) in the decision of performing surgery for patients presenting with a uterine mass . 
nat biotechnol 34 : 547 - 555 , 2016 1 : 814 - 819 , 2015 334 : 252 - 255 , 2011 bayindir b , dehaspe l , brison n , et al : noninvasive prenatal testing using a novel analysis pipeline to screen for all autosomal fetal aneuploidies improves pregnancy management . 
goto a , takeuchi s , sugimura k , et al : usefulness of gd - dtpa contrast - enhanced dynamic mri and serum determination of ldh and its isozymes in the differential diagnosis of leiomyosarcoma from degenerated leiomyoma of the uterus . 
m akinen n , mehine m , tolvanen j , et al : med12 , the mediator complex subunit 12 gene , is mutated at high frequency in uterine leiomyomas . 
wan r , wang z , lee jj , et al : comprehensive analysis of the discordance of egfr mutation status between tumor tissues and matched circulating tumor dna in advanced non - small cell lung cancer . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
sci transl med van beek dm : detection of copy number variation using shallow whole genome sequencing data to replace array - comparative genomic hybridization analysis [ masters thesis ]  . 
heitzer e , ulz p , belic j , et al : tumor - associated copy number changes in the circulation of patients with prostate cancer identied through whole - genome 27 . 
karczewski kj , francioli lc , tiao g , et al : variation across 141 , 456 human exomes and genomes reveals the spectrum of loss - of - function intolerance across 37 . 
correlation between log2 ratio in tumor dna and z - score in cell - free dna for 11 tumor - derived copy number alterations detected in plasma of leiomyoma patients . 
in their letter , karam et al express concerns about the claims made regarding the inability of rna sequencing ( rna - seq ) to perform allele - specic quantication . however , we believe our statement that rna - seq does not allow the allele - specic quantication of normal full - length transcript is correct . the percent splicing index measures the frequency at which a given splice event occurs compared with others affecting the same site.3 as karam et al1 note , this allows one to quantify reads from aberrant transcripts relative to reference transcripts but it does not provide an allele - specic quantication of splicing . 
however , in the case of intronic variants , rnaseq cannot determine whether any of the full - length transcript is also produced by the variant allele because the variant is not part of the messenger rna sequence . 
in the absence of an additional informative variant in the exon , rna - seq cannot distinguish between a full splice defect ( no full - length transcript is made by the variant allele ) and a partial or leaky splice defect ( some full - length transcript is produced by the variant allele )  . 
as gelli et al4 noted , partial splice defects may not be pathogenic if the variant allele produces enough full - length transcript to support normal protein function . in their letter , karam et al1 highlighted a recent publication by landrith et al3 and indicated that rnaseq was used to identify partial skipping of exon 5 in the brca2 c.426 - 12_426 - 8del variant carrier and control patients . 
of note , the landrith et al denition of partial exon skipping is some portion of the exon is skipped ( ie , alternative acceptor / donor ) , 3 not as a partial splice defect . 
however , other published data do show that brca2 c.426 - 12_426 - 8del causes a partial splice defect.8 our laboratory now classies this variant as benign based on additional phenotypic and mutation co - occurrence data , 2 which suggests that the amount of normal transcript produced by the variant allele does support normal protein function . with increased use of tools such as rna - seq to aid in variant classication , physician understanding of how these tools should be used is critical to appropriate patient care . 
we would like to emphasize that we are not arguing against the use of functional rna studies in producing data to support variant classication . rather , we are promoting the need for improved guidelines for interpretation and use of such data in variant classication . 
sharing of reclassication advancements and variant classication information through publications such as the article by nix et al2 allows for dissemination of high - quality data that has passed peer review . 
nix p , mundt e , manley s , et al : functional rna studies are a useful tool in variant classication but must be used with caution : a case study of one brca2 variant . 
gelli e , colombo m , pinto am , et al : usefulness and limitations of comprehensive characterization of mrna splicing proles in the denition of the clinical relevance of brca1 / 2 variants of uncertain signicance . 
 consistency of brca1 and brca2 variant classifications among clinical diagnostic laboratories purpose genetic tests of cancer predisposition genes , brca1 and brca2 , inform significant clinical decisions for both physicians and patients . 
the clinvar database makes deidentified clinical variant classifications from multiple laboratories publicly available for comparison and review , per recommendations by the american medical association , the american college of medical genetics , the national society for genetic counselors , and other organizations . methods classifications of more than 2 , 000 brca1 / 2 variants in clinvar that represent approximately 22 , 000 patients were dichotomized as clinically actionable or not actionable and compared among as many as seven laboratories . 
clinvar facilitated resolution of many of the discordant variants , and concordance increased to 99.0% per variant and 99.8% per patient when reclassified , but not yet resubmitted , variants and submission errors were addressed . 
most of the remaining discordances seemed to involve either legitimate differences in expert judgment regarding particular scientific evidence or were classifications that predated the availability of important scientific evidence . conclusion significant classification disagreements among professional clinical laboratories represented in clinvar are infrequent yet important . 
2017 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction hereditary breast and ovarian cancer is a cancer predisposition syndrome that results from inherited is , germlineloss - of - function mutations in that brca1 or brca2 genes , collectively , brca1 / 2.such pathogenic , or disease - causing , genetic variants result in a 40% to 80% lifetime risk of developing breast cancer , an 11% to 40% risk of ovarian cancer , and striking increases in the risk of male breast , pancreatic , and prostate cancers.1 , 2 up to 10% of breast cancers are caused by these genes.3 , 4 approximately one in 250 individuals of european descent are born with a pathogenic variant in brca1 / 2 , and prevalence is much higher in certain populationsfor example , ashkenazi jews.5 , 6 decades of clinical testing and research have uncovered tens of thousands of brca1 / 2 genetic variants across the human population.7 the great majority of these variants are benign and confer no increased cancer risk , whereas others are pathogenic . 
to help standardize variant interpretation , the american college of medical genetics ( acmg ) and the association for molecular pathology ( amp ) jointly issued revised guidelines8 for variant classification . 
whereas vus , likely benign , and benign variants in brca1 / 2 are not medically actionable , pathogenic and likely pathogenic variants are actionable , which warrants consideration of additional screening , prevention , or treatment options.6 , 11 , 12 thus , rigorous and consistent variant interpretation is critical to patient care . variant classifications can also potentially conflict if one laboratory has access to proprietary data that are unavailable to others . 
in the 1990s , myriad genetics patented the brca1 / 2 genes and prohibited testing by other laboratories.13 , 14 myriad genetics continued as the sole provider for nearly 20 years until the patents were overturned . 
the company used its monopoly to accumulate a substantial database of variants that it ceased releasing publicly in 2006 and from which it claims a competitive advantage.15 - 17 this practice is contrary to the recommendations of the american medical association ( ama ) , the acmg , the national society for genetic counselors , and other organizations.18 - 20 recognizing that shared knowledge about genetic variants is critical to high - quality medical care , the national institutes of health established clinvar , a public database of clinically observed genetic variants , their pathogenicity classifications from various laboratories , and a summary of the scientific evidence used in those classifications.21 - 25 whereas many commercial and academic laboratories collaboratively submit data to clinvar , others , including myriad , do not . 
nevertheless , a substantial myriad genetics data set has been submitted by ordering clinicians and patients through the sharing clinical reports project ( scrp ) .13 , 26 in this study , we used publicly available data from clinvar to assess agreement among clinical laboratories for classifications of brca1 / 2 variants . experiencedclinical laboratories , and older data sets . 
the complete data set that was used in our analysis is also provided as a data supplement . to compare potential clinical impact , we dichotomized classifications into positive ( pathogenic , likely pathogenic ) or not positive ( benign , likely benign , vus )  . 
although many laboratories exclude benign and likely benign variants from clinical reports , these variants are often submitted to clinvar and many are available for comparison.27 scrp , which is derived directly from clinical reportsand thus benign and likely benign variants are under - represented from this submitter ( table 1 and data supplement ) is an exception . general population allele frequencies for these variants were determined by using the exac database , 28 the 1000 genomes project phase iii database , 29 and the exome variant server.30 common variants were defined as those with allele frequencies greater than 1% in any of these databases . 
these patients variants were also part of the clinvar data set described above . cis were computed by using the wilson method.31 evaluation of the scientific evidence that underlies discordant classifications was performed according to the most recent acmg / amp recommendations.8 our methods for estimating the number of patients who were expected to have discordant variants are detailed in the data supplement . methods classifications of brca1 / 2 variants were extracted from the clinvar may 2016 release . 
variants in clinvar are classified as pathogenic , likely pathogenic , vus , likely benign , or benign , which is consistent with acmg / amp terminology.8 laboratory - specific classification categoriesfor example , deleterious instead of pathogenic or polymorphism instead of benignare mapped to thestandardized nomenclature . 
we thus excluded data from research laboratories , consortia , smallerpossibly less results there were 5 , 124 brca1 / 2 variants submitted to clinvar by seven groups that met our inclusion criteria ( table 1 )  . 
nearly 90% of these variants ( 1 , 769 of 2 , 006 ) were rare , having allele frequencies less than 0.05% in all of the general population databases we examined and less than 0.1% in our clinical database ( fig 1 )  . 
classified variants comparable variants full name in clinvar most recent classification evidence provided note clinvar submitter ambry scrp / myriad genetics invitae genedx counsyl cheo emory total 2 , 792 2 , 327 1 , 998 1 , 216 5 , 124 1 , 613 1 , 351 1 , 367 2 , 006 ambry genetics february 2015 sharing clinical reports december 2015 project invitae genedx counsyl march 2016 october 2015 february 2015 benign and likely benign variants are under - reported no vus submitted molecular genetics dates not provided diagnostic laboratory , childrens hospital of eastern ontario emory genetics laboratory june 2015 note . 
ambry and counsyl had not submitted brca1 / 2 updates for more than 1 year , although all data sets shown here met our study inclusion criteria ( data supplement )  . abbreviation : scrp , sharing clinical reports project ; vus , variants of uncertain significance . variants were a representative subset of 5 , 124 clinvar variants in overall properties , with an expected bias away from rare variants , albeit small in magnitude ( table 2 )  . 
clinvar data were also representative of those observed in clinical practice , with some submitter - specific exceptions ( table 1 and data supplement )  . we compared variant classifications in terms of whether they would or would not potentially affect clinical management ( see methods )  . 
on the basis of the prevalence distribution of variants in clinical testing , we calculated the expected concordance on a per - patient basis to be 99.7% ( fig 3 ; data supplement )  . 
this concordance rate is similar to that reported ( 99.8% ) in a prior study of approximately 1 , 000 prospectively accrued patients that compared acmg / amp - based classifications with those from myriad genetics.32 , 33 a feature of clinvar is that it records the date on which each classification was made , thereby allowing us to consider whether the high concordance we observed could be a result of laboratories being overly influenced by each others prior classifications . 
such influence would be most concerning in the case of myriad genetics classifications submitted by scrp , for which underlying evidence is unavailable for other laboratory directors to evaluate.14 we saw no evidence of such bias , as 99.4% ( 503 of 506 ) of classifications that predated a myriad genetics / scrp entry were concordant with it compared with 99.1% ( 2 , 385 of 2 , 406 ) that postdated it ( data supplement )  . 
these rates are not significantly different . although classifications from the enigma consortium ( evidence - based network from the interpretation of germline mutant alleles ) 34 were not considered in our comparison , they can provide evidence that clinical laboratories use in their classifications . 
although clearly important , rare missense variants are infrequently observed in patients6.3% prevalence in our clinical data set . rare protein truncating and silent variants were also numerous ( 439 of 2 , 006 and 173 of 2 , 006 , respectively ; 30.5% of the data set together ) and were concordantly classified with one exception . other discordant variants were in canonical rna splice sites ( five of 30 ) or an intron ( two of 30 ) or were in - frame deletions ( two of 30 )  . 
finally , two truncating mutations in the last coding exon of brca2 had discordant classifications . to gain insight into the basis for the small number of discordant classifications , we examined all publicly available evidence for and against pathogenicity for each of the 30 discordant variants . 
we also contacted submitting laboratories regarding specific discordant classifications , particularly those for variants with three or more submitters . we found two common explanations for discordant classifications ( data supplement ) : in seven variants , there was a historical difference , meaning that one or more classifications in clinvar was out of date , and although the variant had been reclassified , thus becoming concordant , updates had not yet been submitted to clinvar . 
this mutation causes upregulation of an endogenous alternate rna isoform missing exons 9 and 10 but that seems to provide brca1 functionality.36 this result suggests that laboratory directors should carefully evaluate other mutations in exons 9 and 10 and highlights the complexities of variant classification that laboratory directors must consider in some cases . overall , however , our analysis suggests that a high level of concordance should , perhaps , have been expected . 
nevertheless , the reports significance for clinical management decisions remain similar . furthermore , we explored the likely cause of the few observed discordances and found that approximately one half resulted from out - of - date classifications or submission errors , whereas the remainder were likely expert judgment differences regarding the strength or quality of particular scientific evidence . 
we were pleased that all but one laboratory responded collaboratively to requests for detailed information about their classificationsdespite those requests coming directly from a commercial competitor ( invitae )  . 
this process of identifying and reconciling differences was made possible by shared data in a central and unrestricted public database ( clinvar )  . our findings might at first seem to be at odds with other studies that compared variant classifications . a study by vail et al42 compared the interpretation of approximately 2 , 000 brca1 / 2 variants among a number of public databases and found greater discordance than we report . 
of importance , it incorporated data from research laboratories , older data , and data from curated literature databases that were not classified using modern clinical criteria.8 , 43 , 44 furthermore , it counted differences that would not significantly change management , for example , vus versus likely benign . 
discordances that maxwell et al found were in other cancer genesonly recently incorporated into testsfor which less information is generally available and thus discordance may indeed be higher than it is for brca1 / 2 . separately , balma~na et al46 , 47 examined variants in cancer genes other than brca1 / 2 in the prompt registry.48 the authors found 19 unique variants , which represent 57 of 603 comparable test findings ( 9.5% ) , that had two or more significantly 5 , 000 10 , 000 15 , 000 20 , 000 25 , 000 30 , 000 35 , 000 no . 
other variant typesnotably rare missense and splice - site changesrequire additional experimental or genetic data to classify , but relatively few patients ( , 7% ) carry any such variants , and they are often ( 97.6% ) concordant across laboratories ( table 2 )  . 
when not considered vus , these variants are usually classified as benign , or likely benign , and not pathogenic ( data supplement )  . indeed , a comparison of clinvar releases over the past 2 years shows that most ( 94.5% ) missense vus , when reclassified , are downgraded to benign or likely benign and thus remain not clinically actionable , which is consistent with prior studies.37 discussion in this study , we analyzed publicly available data from the clinvar database and found remarkably few clinically significant discordances in the classifications of more than 2 , 000 variants in two wellcharacterized cancer risk genes , brca1 and brca2 . 
the observation that all discordant variants were rare , although most rare variants remained concordant , suggests that roughly one of 500 patients would be expected to receive results that would significantly change clinical management from the various laboratories in this study . 
percentages indicate the fraction of all variants in this study ( column 2 ) , comparable variants ( those with two or more submitters ; column 3 ) , and concordance for each variant class ( columns 4 and 5 )  . 
clinical prevalence ( column 6 ) indicates the fraction of patients in our clinical database who carry one or more such variants , regardless of pathogenicity ( many are indeed classified benign )  . 
the authors concluded that conflicting interpretation is frequent and may have implications for medical management.48 ( p 46 ) we examined current ( september 30 , 2016 ) clinvar entries for all 19 of these variants and found that six had discordant interpretations only from a nonclinical source ( most commonly , omim49 ) , whereas all clinical laboratories , in fact , agreed with each other.47 one variant was no longer discordant after a 1 - year - old , but more recently submitted , reclassification . 
two low - risk variants had discordance that was attributable to the fact that nomenclature and classification criteria for such variants are not standardized under current acmg guidelines , yet most laboratories still agreed . 
we count 10 variants from balma~na et al , representing 2.2% of findings ( 13 of 603 ) , having a clinically substantial discordance between clinical testing laboratories , 4.3 - fold fewer than the 57 of 603 they report . some of this remaining discordance in non - brca1 / 2 genes seems to be attributable to factors we describe above for brca1 / 2 , for example , older data , although , unfortunately , balma~na et al46 did not contact submitting laboratories to understand the basis of discordance as we did . in another study , the national institutes of health funded clinical sequencing exploratory research consortium performed an experiment in which 99 variants in various genesbiased toward relatively challenging caseswere classified by up to nine laboratories.50 although many classification differences were observed , only a fraction would change management , and only five variants in brca1 / 2 were included . 
of importance , the authors found that sharing classifications among laboratories , thus identifying discordances , enabled discussions that resolved many of the differences and contributed to an overall higher quality than any one laboratory could achieve alone . our study and those mentioned above highlight important best practices in the use of public databases . 
the only classification discordances we observed were in rare variants , which few patients carry , and most rare variants were completely concordant when observed by multiple laboratories ( data supplement )  . sources are valuable and important to centralize and share , database users must apply good judgment and quality control . 
they must pay attention to dates , as variant classifications can become outdated , for example , when new scientific evidence is published . moreover , users must consider whether a classification originates from a clinical laboratory that rigorously follows guidelines - based classification procedures or from a submitter who may have applied a different standard . 
at present , only two of the laboratories included in this study genedx and invitae provide the evidence that supports the classification of specific variants in their clinvar submissions , a situation that we hope will change . 
other laboratories include evidence only in patient reports , but these are not broadly available for both logistical and patient privacy reasons . although our analysis shows that clinically significant disagreements in brca1 / 2 variant classification are infrequent , they are , of course , important to patients and clinicians . 
we believe it is essential for the genetics community to resolve these differences collaboratively , as is standard practice in other areas of oncology , to deliver the best possible patient care.21 - 23 , 38 - 41 , 50 our study supports others in demonstrating that collaborative interaction among laboratories improves the quality of clinical testing.39 - 41 , 50 unlike proprietary databases , clinvar is freely open to all and makes such collaboration possible on a global scale . 
although laboratories with proprietary databases have made claims of superior accuracy , such claims are not subject to detailed and ongoing independent review.14 , 17 indeed , our observation of high concordance across laboratories calls into question some of those claims . 
we note that semipublic databases with restrictive licensing terms , such as brca share , 51 - 53 can present many of the same challenges that are encountered with proprietary databasesfor example , license restrictions prevented the consideration of such data in this study . 
we also note that patient registries , including prompt , although highly valuable for other reasons , do not address the needs that clinvar does.14 , 21 for these reasons , the open sharing of deidentified variant classifications is recommended by the ama , acmg , national society for genetic counselors , and other professional societies . 
in collaboration with international groups , the national institutes of health has recently funded initiatives , including clingen21 , 22 and the brca exchange , 7 that leverage clinvar , the literature , and other resources , to share , compare , and reconcile variant classifications , thus continually improving this important aspect of precision oncology . 
however , at least one major laboratory , myriad genetics , has revised its terms of service to prohibit ordering clinicians from sharing deidentified variant classifications , 54 which is how scrp data used in this study were obtained . 
myriad genetics has also historically resisted requests from patients for their unreported benign variants , prompting legal action by the american civil liberties union.55 such restrictions will make ongoing comparative analyses impossible . 
lincoln employment : invitae stock and other ownership interests : invitae travel , accommodations , expenses : invitae shan yang employment : invitae stock and other ownership interests : invitae melissa s . 
cline no relationship to disclose yuya kobayashi employment : invitae stock and other ownership interests : invitae can zhang no relationship to disclose scott topper employment : invitae stock and other ownership interests : invitae david haussler no relationship to disclose benedict paten stock and other ownership interests : bioturing robert l . 
nussbaum employment : invitae leadership : invitae , personalis , complete genomics honoraria : baxter ( i ) , genzyme , personalis , complete genomics consulting or advisory role : baxter ( i ) , invitae , personals , complete genomics research funding : baxter ( i ) patents , royalties , other intellectual property : national institutes of health , university of california ( inst ) , national institutes of health , university of california expert testimony : ariosa travel , accommodations , expenses : baxter ( i ) , genzyme acknowledgments we are deeply grateful to the laboratories and other groups who are working to advance medical care by submitting data to the clinvar database . 
we particularly thank the staff at scrp , ambry genetics , genedx , counsyl , the cheo molecular genetics laboratory , and the emory genetics laboratory for their hard work on data submissions . 
we thank george riley ( national institutes of health / national center for biotechnology information ) and salina chan ( university of california , san francisco ) for providing updated scrp data . 
we thank olga jarinova and hussein daoud ( cheo molecular genetics laboratory ) , jill dolinsky and tina pesaran ( ambry genetics ) , peter kang ( counsyl ) , and kathryn garber ( emory genetics laboratory ) for clarifying aspects of their data in clinvar . 
whittemore as , gong g , john em , et al : prevalence of brca1 mutation carriers among us non - hispanic whites . cancer epidemiol biomarkers prev 13 : 2078 - 2083 , 2004 6 . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
lindor nm , goldgar de , tavtigian sv , et al : brca1 / 2 sequence variants of uncertain significance : a primer for providers to assist in discussions and in medical management . 
angrist m , cook - deegan r : distributing the future : the weak justifications for keeping human genomic databases secret and the challenges and opportunities in reverse engineering theappl transl genomics 3 : 124 - 127 , 2014 15 . 
pruss d , morris b , hughes e , et al : development and validation of a new algorithm for the reclassification of genetic variants identified in the brca1 and brca2 genes . 
cook - deegan r , conley jm , evans jp , et al : the next controversy in genetic testing : clinical data as trade secrets ? eur j hum genet 21 : 585 - 588 , 2013 18 . 
acmg board of directors : laboratory and clinical genomic data sharing is crucial to improving genetic health care : a position statement of the american college of medical genetics and genomics . 
nucleic acids res 44 ( d1 ) : d862 - d868 , 2016 sharing / sharing - clinical - reports - project - scrp / symp biocomput 22 : 166 - 176 , 2016 285 - 291 , 2016 variation . 
lincoln se , kobayashi y , anderson mj , et al : a systematic comparison of traditional and multigene panel testing for hereditary breast and ovarian cancer genes in more than 1000 patients . 
spurdle ab , healey s , devereau a , et al : enigmaevidence - based network for the interpretation of germline mutant alleles : an international initiative to evaluate risk and clinical significance associated with sequence variation in brca1 and brca2 genes . 
rosenthal et , bowles kr , pruss d , et al : exceptions to the rule : case studies in the prediction of pathogenicity for genetic variants in hereditary cancer genes . 
wong - brown m , mcphillips m , gleeson m , et al : when is a mutation not a mutation : the case of the c.5942a.c splice variant in a woman harbouring another brca1 mutation in trans . 
murray ml , cerrato f , bennett rl , et al : follow - up of carriers of brca1 and brca2 variants of unknown significance : variant reclassification and surgical decisions . 
vail pj , morris b , van kan a , et al : comparison of locus - specific databases for brca1 and brca2 variants reveals disparity in variant classification within and among databases . 
maxwell kn , hart sn , vijai j , et al : evaluation of acmg - guideline - based variant classification of cancer susceptibility and non - cancer - associated genes in families affected by breast cancer . 
balma~na j , digiovanni l , gaddam p , et al : conflicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
nussbaum rl , yang s , lincoln se : clinical genetics testing laboratories have a remarkably low rate of clinically significant discordance when interpreting variants in hereditary cancer syndrome genes . 
amberger js , bocchini ca , schiettecatte f , et al : omim.org : online mendelian inheritance in man ( omim ) , an online catalog of human genes and genetic disorders . 
amendola lm , jarvik gp , leo mc , et al : performance of acmg - amp variant - interpretation guidelines among nine laboratories in the clinical sequencing exploratory research consortiuam j hum genet 98 : 1067 - 1076 , 2016 51 . 
caputo s , benboudjema l , sinilnikova o , et al : description and analysis of genetic variants in french hereditary breast and ovarian cancer families recorded in the umd - brca1 / brca2 databases . 
 genetic alterations detected in cell - free dna are associated with enzalutamide and abiraterone resistance in castration - resistant prostate cancer samantha torquato , phd1 ; aparna pallavajjala , ms1 ; alexa goldstein , ms1 ; patricia valda toro , ms1 ; john l . 
hurley , phd1 purpose androgen receptor ( ar ) gene alterations , including ligand - binding domain mutations and copy number ( cn ) gain , have yet to be fully established as predictive markers of resistance to enzalutamide and abiraterone in men with metastatic castration - resistant prostate cancer ( mcrpc )  . 
the goal of this study was to validate ar gene alterations detected in cell - free dna ( cfdna ) as markers of enzalutamide and abiraterone resistance in patients with mcrpc . methods patients with mcrpc ( n = 62 ) were prospectively enrolled between 2014 and 2018 . 
blood was collected before therapiesenzalutamide ( n = 25 ) , abiraterone ( n = 35 ) , or enzalutamide and abiraterone ( n = 2 ) and at disease progression . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction next - generation therapies that target the androgen androgen receptor ( ar ) axis , such as abiraterone and enzalutamide , have improved survival outcomes for men with metastatic castration - resistant prostate cancer ( mcrpc ) , 1 - 4 but both primary and acquired resistance to these drugs continue to be a substantial clinical challenge . 
resistance mechanisms are not fully understood ; however , some forms of resistance likely involve alterations to ar , including amplication and ligand - binding domain ( lbd ) missense mutations . 
although rare in primary prostate cancers , 5 - 7 ar gene alterations are highly prevalent in mcrpc.8 - 13 metastatic tissue biopsies as a sole means to detect and observe changes in ar status is impractical , and thus cell - free dna ( cfdna ) is gaining traction as a minimally invasive and easily obtainable tumor biopsy surrogate . 
previous studies using cfdna from the blood to evaluate the association of ar gene aberrations with resistance to abiraterone and enzalutamide are inclusive.14 - 17 ar copy number ( cn ) gain18 , 19 and / or amplication20 or detection of two or more ar mutations20 have been associated with worse outcomes to such therapies as abiraterone and enzalutamide . 
the ar splice variant ar - v7 is associated with resistance to enzalutamide and abiraterone21 - 23 and is also associated with increased ar cn.24 in addition to ar , alterations in other genes , including tumor protein p53 ( tp53 ) , phosphatase and tensin homolog ( pten ) , and breast cancer gene 2 ( brca2 ) , are enriched in lethal prostate cancer.8 - 11 studies support the idea that lineage plasticity from an ardependent to an ar - independent state through loss of tp53 and retinoblastoma - associated protein 1 ( rb1 ) mediates resistance to ar - targeted therapies.25 - 28 consistent with this , tp53 defects have been shown to be associated with worse outcomes with abiraterone and enzalutamide therapies.17 the role of brca2 and other homology - directed repair ( hdr ) genes in mediating resistance to enzalutamide and abiraterone has not been denitively determined . 
the secondary goal was to determine if alterations in other genes that are enriched in lethal prostate cancer , including tp53 , pten , and brca2 , were associated with response to enzalutamide and abiraterone . in this study , high circulating tumor dna ( ctdna ) burden was signicantly associated with prostate - specic antigen ( psa ) ( pfs ) , and overall survival ( os )  . 
study limitations , including sample size and patient heterogeneity , necessitate larger and prospective validation of the association of plasma ar status with outcomes . response , progression - free survival methods patient information , study end points , sample collection , deep next - generation sequencing ( ngs ) , sequence alignment and analysis of variants , cn variation , estimation of ctdna fraction , and statistical analyses are found in the data supplement . results patient cohort patient characteristics are listed in table 1 . 
clinvarannotated pathogenic or likely pathogenic missense mutations , truncating mutations , and / or cn alterations were detected in cfdna from 89% of patients before therapy initiation and in 92% of patients at disease progression ( figs 1a - 1d and data supplement )  . ctdna total cfdna concentration before therapy was associated with psa ( p = .002 ; data supplement )  . 
nearly all patients ( 61 of 62 ) had detectable cn variation ( s ) and / or mutation ( s ) with an allelic frequency above the 1% cutoff before therapy ( figs 1b and 1c )  . 
multivariable analyses controlled for ctdna high . abbreviations : ar , androgen receptor ; atm , ataxia - telangiectasia mutated gene ; brca1 / 2 , breast cancer gene 1 / 2 ; cn , copy number ; ctdna , circulating tumor dna ; lbd , ligand - binding domain ; or , odds ratio ; pi3k , phosphoinositide 3 - kinase ; psa , prostate - specic antigen ; rb1 , retinoblastoma - associated protein 1 ; tp53 , tumor protein 53 ; wnt , wingless - type mmtv integration site . h875y mutation had psa responses on abiraterone ( fig 2c )  . 
 ( b ) total number of protein - altering genetic changes in 46 genes detected by next - generation sequencing ( ngs ) of cfdna from 62 patients before abiraterone ( abi ) and enzalutamide ( enza ) therapy . 
 ( c ) genetic alterationscopy number ( cn ) status , clinvar pathogenic / likely pathogenic missense and germline mutations , and truncating mutationsin 46 genes detected by ngs of cfdna from 62 patients before abiraterone and enzalutamide therapy in order of best psa response . 
 ( d ) total number of genetic alterationscn , clinvar pathogenic / likely pathogenic missense and germline mutations , and truncating mutationsin 46 genes detected by ngs of cfdna from 62 patients before abiraterone and enzalutamide therapy . 
ar , androgen receptor ; ctdna , circulating tumor dna . defectspathogenic mutations and / or cn losswere not associated with psa response ( p = .602 ) or pfs ( p = .314 ; tables 2 and 3 )  . 
progression - free survival ( pfs ) : pathogenic androgen receptor ( ar ) ligand - binding domain ( lbd ) mutations are associated with a shorter time to progression . 
 ( a ) kaplan - meier method and log - rank test were used to determine median time to progression for patients who had high versus low circulating tumor dna ( ctdna ) before therapy . 
 ( b ) waterfall plot of best prostate - specic antigen ( psa ) response for all patients ( n = 62 ) after therapy as determined by best percentage fold change in psa . 
wingless - type mmtv integration site pathway defects involving genetic alterations in adenomatous polyposis colicn loss and / or truncating mutationsand - catenincn gain and pathogenic missense mutationswere detected in nearly 15% of patients before to therapy ( figs 1c and 1d )  . 
analysis of brca2 , and atm did not increase prognostic signicance . discussion liquid biopsies using cfdna as a tumor analyte are rapidly being developed for cancer diagnostics of solid tumors.35 - 37 when obtained concurrently , plasma - derived cfdna is highly concordant with tissue biopsies for tumor - specic genetic alterations.38 , 39 as a result of their advantages over traditional tissue biopsies , including the ease of accessibility for sequential monitoring of cancer dynamics and recapitulation of tumor heterogeneity , clinical development of cfdna has the potential to advance prostate cancer precision medicine.40 mechanisms of resistance to abiraterone and enzalutamide likely involve alterations to androgenar axis signaling . 
deregulation of these pathways likely mediates resistance to androgenar axis therapies . concurrent tp53 and rb1 defects are highly enriched in ar - independent neuroendocrine mcrpc compared with adenocarcinoma mcrpc.42 combined tp53 and rb1 loss has been shown to promote lineage switching from an ardependent to an ar - independent state41 , 43 , 44 and consequent resistance to ar - targeted therapies . 
similar to tp53 , genetic alterations in pten are enriched in mcrpc compared with metastatic castration - sensitive prostate cancer and localized prostate cancer.11 studies suggest that pten loss may mediate castration resistance by downregulating ar , 25 - 28 thereby supporting a rationale for combined inhibition of pi3k and arin pten - decient mcrpcs.45 , 46 association of pathogenic mutations in hdr genes with response to abiraterone and enzalutamide therapy is conicting . 
a clinical trial in patients with mcrpc suggested that genetic alterations in hdr genes that were detected in metastatic biopsy tissue may be associated with longer pfs when on abiraterone therapy.29 concordant ndings were observed in a second study that supported the idea that patients with mcrpc harboring a germline brca1 / 2 or atm mutation may also have improved outcomes to abiraterone and enzalutamide.30 in contrast , another study showed that truncating mutations in brca2 and atm detected in cfdna were associated with a shorter time to progression on abiraterone and enzalutamide therapies in treatment - nave patients with mcrpc.17 in our study , collective somatic and germline genetic alterations were also not associated with worse outcomes to enzalutamide and abiraterone . 
association differences may reect variables , such as sample size , prior treatment status , disease burden , disease heterogeneity , somatic versus germline , and single versus dual loss . 
certainly , additional prospective investigation is needed to determine the clinical signicance of hdr mutations as predictive markers to abiraterone and enzalutamide therapies . in the current study , many patients had detectable alterations that could serve as potential therapeutic targets . previous studies have shown that patients with mcrpc with either germline or somatic mutations in hdr genes achieved signicant responses to olaparib47 and to abiraterone plus veliparib.29 more than one quarter of patients in our study had a deleterious germline or somatic brca1 , brca2 , or atm mutation detected before therapy or at disease progression , which suggests that these patients may benet from therapies that target poly ( adp - ribose ) polymerase or platinum - based chemotherapy.29 , 47 , 48 in addition , immunotherapy trials have been largely unsuccessful in men with mcrpc49 ; however , rare responders have been reported.50 a seminal clinical trial demonstrated that microsatellite instable cancers caused by mismatch repair ( mmr ) gene deciency were sensitive to programmed death - 1 blockade , perhaps because of the formation of neoantigens resulting from increased mutational burden.51 inactivation of mmr genes and elevated mutational burden have been detected in some men with aggressive prostate cancers.33 , 52 , 53 one patient in our study had a detectable noncanonical mmr gene mutation in his cfdna and a correspondingly high fig 3 . 
 ( a ) kaplan - meier method and log - rank test were used to determine median os for patients who had high versus low circulating tumor dna ( ctdna ) before therapy . 
 ( b ) kaplan - meier method and log - rank test were used to determine median os for patients who had androgen receptor ( ar ) copy number ( cn ) gain before therapy . 
 ( c ) gene schematic illustrating deleterious tp53 mutations detected by deep next - generation sequencing ( ngs ) of cellfree dna ( cfdna ) before abiraterone and enzalutamide therapies and at disease progression while on therapy . 
 ( d ) kaplan - meier method and log - rank test were used to determine median os for patients who had tp53 defectscn loss and or clinvar pathogenic / likely pathogenic mutationsbefore therapy . 
 ( e ) kaplan - meier method and log - rank test were used to determine median os for patients who had both tp53 and retinoblastomaassociated protein 1 ( rb1 ) defects compared with patients who had tp53 defects but were rb1 intactcn loss and or clinvar pathogenic / likely pathogenic mutationsbefore therapy . 
 ( f ) kaplan - meier method and log - rank test were used to determine median os for patients who had pi3k pathway defectscn loss and / or truncating mutations in phosphatase and tensin homolog and / or cn gain of pik3cabefore therapy . association of pi3k defects with os controlled for ctdna burden using multivariable proportional hazards regression modeling . 
 ( g ) kaplan - meier method and log - rank test were used to determine median os for patients who had wingless - type mmtv integration site ( wnt ) pathway defectscn loss and / or truncating mutations in adenomatous polyposis coli and / or cn gain and / or pathogenic missense mutations in - cateninbefore therapy . 
consistent with other reports , patients with prior exposure to abiraterone and enzalutamide experienced worse outcomes.54 - 59 statistical signicance was not reached , likely because of the small overall sample size and the few patients with prior therapy . 
ngs protocols were adjusted on the basis of total input , but for patients with low input the lack of genetic alteration detection was considered indeterminate as opposed to negative . 
in addition , mutations in such genes as including ar - v7 , because of tp53 and atm detected in cfdna at low allelic frequencies may be false positives as a result of clonal hematopoiesis.60 corresponding tissue was not available for all samples to conrm tp53 status , and future studies will examine both prostate tumor tissue and blood leukocytes for genetic alterations . 
a nal limitation was our inability to evaluate ar the resplice variants , quirement of circulating tumor cells or whole - blood rna . the presence of ar - v7 is certainly another established mechanism of primary and acquired resistance to nextgeneration hormonal therapies.21 - 23 future studies should aim to simultaneously analyze the full complement of ar aberrations , including gene mutations , amplications , genomic structural rearrangements , and mrna splice variants , from a single liquid biopsy . in summary , our ndings indicate ctdna burden was highly associated with worse outcomes to enzalutamide and abiraterone . 
eisenberger leadership : veru stock and other ownership interests : veru honoraria : sano , pzer consulting or advisory role : astellas pharma , ipsen , bayer , sano , pzer research funding : sano , tokai pharmaceuticals , genentech travel , accommodations , expenses : bayer , astellas pharma , sano , pzer , veru emmanuel s . 
antonarakis honoraria : sano , dendreon , medivation , janssen biotech , essa pharma , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , medivation , janssen biotech , essa pharma , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : coinventor of a biomarker technology licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation bruce j . 
park leadership : loxo pharmaceuticals stock and other ownership interests : loxo pharmaceuticals consulting or advisory role : horizon discovery , foundation medicine , loxo pharmaceuticals , casdin capital , h3 biomedicine , jackson laboratory for genomic medicine , eli lilly speakers ' bureau : astrazeneca research funding : foundation medicine , abbvie , pzer patents , royalties , other intellectual property : royalties paid through inventions at johns hopkins university by horizon discovery travel , accommodations , expenses : eli lilly , loxo pharmaceuticals paula j . 
hurley stock and other ownership interests : loxo pharmaceuticals ( i ) honoraria : foundation medicine ( i ) , roche ( i ) , h3 biomedicine ( i ) , casdin capital ( i ) , loxo pharmaceuticals ( i ) , eli lilly ( i ) consulting or advisory role : loxo pharmaceuticals ( i ) , foundation medicine ( i ) , roche ( i ) , h3 biomedicine ( i ) , casdin capital ( i ) , lilly ( i ) patents , royalties , other intellectual property : cell lines at horizon ( i ) no other potential conicts of interest were reported . acknowledgment we thank the patients who consented to participate in this study . 
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 o identifying a clinically applicable mutational burden threshold as a potential biomarker of response to immune checkpoint therapy in solid tumors purpose an association between mutational burden and response to immune checkpoint therapy has been documented in several cancer types . 
the potential for such a mutational burden threshold to predict response to immune checkpoint therapy was evaluated in several clinical datasets , where mutational burden was measured either by whole - exome sequencing or by using commercially available sequencing panels . anshuman panda anil betigeri kalyanasundaram subramanian jeffrey s . 
johnson gyan bhanot shridar ganesan author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : shridar ganesan , md , phd , 195 little albany st , new brunswick , nj 08903 ; e - mail : ganesash@ cinj.rutgers.edu. methods whole - exome sequencing and rna sequencing data of 33 solid cancer types from the cancer genome atlas were analyzed to determine whether a robust immune checkpoint activating mutation ( icam ) burden threshold associated with evidence of immune checkpoint activation exists in these cancers that may serve as a biomarker of response to immune checkpoint blockade therapy . results we found that a robust icam threshold , associated with signatures of immune checkpoint activation , exists in eight of 33 solid cancers : melanoma , lung adenocarcinoma , colon adenocarcinoma , endometrial cancer , stomach adenocarcinoma , cervical cancer , estrogen receptorpositive / human epidermal growth factor receptor 2negative breast cancer , and bladder - urothelial cancer . 
in published datasets of melanoma , lung adenocarcinoma , and colon cancer , patients with icam - positive tumors had significantly better response to immune checkpoint therapy compared with those with icamnegative tumors . 
receiver operating characteristic analysis using the cancer genome atlas predictions as the gold standard showed that icam - positive tumors are accurately identifiable using clinical sequencing assays , such as foundationone ( foundation medicine , cambridge , ma ) or strandadvantage ( strand life sciences , bangalore , india )  . 
icam - positive and icamnegative tumors have distinct mutation patterns and different immune microenvironments . conclusion in eight solid cancers , a mutational burden threshold exists that may predict response to immune checkpoint blockade . 
2017 by american society of clinical oncology introduction antiprogrammed death - 1 ( pd - 1 ) and anti cytotoxic t - lymphocyte antigen - 4 ( ctla - 4 ) therapy results in prolonged response in some solid cancers.1 - 5 response to ctla - 4 blockade in melanoma1 , 2 and pd - 1 blockade in lung , 3 colorectal , 4 and urothelial5 cancers is associated with increased mutational burden . 
although this association between mutational burden and response to immune checkpoint therapy is documented in some cancers , 1 - 5 it is unclear whether this relationship exists in other cancers . 
using rna sequencing ( rna - seq ) and whole - exome sequencing data for all solid cancers in the cancer genome atlas ( tcga ) , we asked the following three questions : ( 1 ) is there a mutational burden threshold above which there is a signature of immune activation and immune checkpoint pathway upregulation in some cancers ? ( 2 ) can this threshold be identified using clinical sequencing assays that interrogate a subset of the exome ? ( 3 ) does this threshold identify responders to immune checkpoint therapy ? we found that a robust immune checkpoint activating mutation ( icam ) threshold satisfying the first two conditions exists in eight classes of solid tumors . 
in published datasets where condition ( 3 ) is testable , patients with icam - positive cancers have significantly better clinical response to immune checkpoint therapy than patients with icamnegative cancers . 
analysis of a cohort of patients with melanoma , sequenced using the foundationone assay ( foundation medicine , cambridge , ma ) , 6 demonstrated that patients with icam - positive melanomas had significantly better response to pd - 1 blockade than patients with icam - negative melanomas . 
finally , for these cancer types , distinct patterns of mutations are present in icam - positive versus icam - negative tumors , suggesting potentially distinct underlying disease mechanisms . methods data collection and processing mutation data were obtained from tcga ( maf + files )  . 
all mutation annotation format files current as of january 31 , 2016 ( public and protected ) were downloaded , mapped from hg18 to hg19 using liftover if necessary ( ucsc.edu / cgi - bin / hgliftover ) , re - annotated using oncotator , 7 merged , and de - duplicated . 
for each tumor , rnaseqv2 - scaled estimates from the broad institute broad genome data analysis center ( org ) and tcga data portal were divided by the median value per sample and used to quantify immune infiltration and leukocyte composition by estimate8 and cibersort , 9 respectively . only unambiguous ( p , .05 ) cibersort outputs were used . 
erbb2 focal copy number data and esr1 mrna expression data from the broad genome data analysis center were used to classify breast cancer samples into clinical subtypes ( estrogen receptor [ er ] positive / human epidermal growth factor receptor 2 [ her2 ] negative , er negative / her2 negative , or her2 positive ) , and these subtypes were analyzed separately . 
in addition to cibersort9 p values , two - sided ( p , .05 ) fishers test and log - rank test were used to compare response and survival rates , respectively . 
all bracketed ranges throughout this article correspond to 95% confidence intervals . determination of icam threshold in tcga if nonsynonymous mutational burden is associated with immune checkpoint activation , there should be a mutational burden threshold above which tumors have the following : ( 1 ) cd8 - positive t - cell response ( data supplement ) and ( 2 ) overexpression of immune checkpoint pathways ( data supplement )  . 
for each xi , we tested whether tumors with mutational burden > xi had significantly higher cd8 - positive t - cell activation and pd - 1 / ctla - 4 pathway upregulation compared with tumors with mutational burden , xi ( data supplement )  . 
in eight cancer types , criteria ( 1 ) and ( 2 ) were simultaneously satisfied for several x - values , confirming an association between mutational burden and immune checkpoint activation in those cancer types . 
the presence of tumor - infiltrating lymphocytes was assessed in > 10 fields at the highest magnification , and tumors were graded for lymphocytic density and distribution , on all slides for each case . 
the score per slide was the cumulative grade of density and distribution , with the highest score for each case taken as the final score . melanoma samples used for prospective validation of icam threshold mutation , treatment , and outcome data in a cohort of 196 de - identified samples were obtained under institutional review boardapproved protocols to test the icam threshold for the foundationone assay.6 one hundred eleven samples from the rutgers cancer institute of new jersey and 85 from either the vanderbilt - ingram cancer center or massachusetts general hospital had data from either the 315or 236 - gene foundationone panels . 
one hundred thirteen samples from patients treated with single - agent pd - 1 therapy ( 28 from rutgers cancer institute of new jersey , 85 from vanderbilt - ingram cancer center and massachusetts general hospital ) were stratified by icam status using the mutational burden threshold of either 14 or nine mutations for the foundationone 315and 236 - gene panels , respectively ( data supplement )  . results identification of icam threshold using tcga whole - exome sequencing and rnaseq data for 33 solid cancers , we looked for an icam mutational burden threshold , such that icam - positive tumors ( ie , tumors with mutational burden above the threshold ) had evidence of the following : ( 1 ) immune activation : high cd8a mrna levels , evidence of immune infiltration ( measured by estimate8 ) , and high cd8 - positive t - cell fraction in leukocytes ( measured by cibersort9 ) ; and ( 2 ) upregulation of immune checkpoint pathway gene expression ( ie , pd - 1 , ctla - 4 , and their ligands ; data supplement )  . 
although these tumor features have been previously shown to associate with response to immune checkpoint therapy , 4 , 5 , 12 in this study we used rna - seq data to indirectly measure these criteria . mutational burden has been identified to predict response to immune checkpoint blockade in melanoma , 1 , 2 lung adenocarcinoma , 3 colon adenocarcinoma , 4 and bladder - urothelial cancer.5 we found that , in addition , a robust icam threshold also exists in endometrial cancer , stomach adenocarcinoma , cervical cancer , and erpositive / her2 - negative breast cancers ( data supplement )  . 
a robust mutational burden threshold could not be identified for triple - negative breast cancer and renal cell cancercancer types where immune checkpoint therapy has some clinical activity.13 , 14 as an independent test , a blinded pathologic analysis of high - resolution , whole - slide images of hematoxylin and eosinstained sections from tcga of 15 icam - positive and 15 icam - negative tumors for each cancer type showed that icam - positive tumors had significantly higher lymphocyte infiltration than icam - negative tumors in all eight cancer types ( fig 1c )  . 
for different definitions of mutational burden or different sequencing depths , the thresholds need to be recomputed . icam status predicts response to pd - 1 and ctla - 4 blockade in published data to test the utility of icam , the icam thresholds were evaluated in published datasets for patients treated with ctla - 4 blockade in skin melanoma1 , 2 and pd - 1 blockade in lung adenocarcinoma3 and colon adenocarcinoma4 ( fig 2 ) , with samples stratified into icam - positive and icam - negative classes , as described in the data supplement . 
a robust immune checkpointactivating mutation ( icam ) threshold associated with evidence of immune checkpoint activation can be identified in eight cancer types in the cancer genome atlas ( tcga )  . 
 ( a ) distributions of nonsynonymous mutational burden in eight cancer types ( in log10 scale ) separate the samples into icam - positive ( blue ) and icam - negative ( gold ) subsets . 
 ( b ) immune checkpoint activation criterion ( data supplement ) significantly higher in icam - positive compared with icam - negative is shown in gold for the eight cancer types . 
 ( c ) results from blinded pathologic quantification of lymphocyte infiltration in high - resolution histologic images from tcga of 15 icam - positive and 15 icam - negative tumors in each of the eight cancer types . 
 ( a ) comparison of response in patients with skin melanoma to cytotoxic t - lymphocyte antigen - 4 ( ctla - 4 ) targeted therapy by icam status in two independent datasets.1 , 2 ( b ) comparison of response in patients with lung adenocarcinoma3 and colorectal cancer4 to programmed death - 1 targeted therapy by icam status . 
cb , clinical benefit ; cr , complete response ; dcb , durable clinical benefit ; pd , progressive disease ; pr , partial response . validation of icam threshold in predicting response to immune checkpoint blockade in melanoma using the foundationone assay one hundred ninety - six skin melanoma samples were sequenced using the foundationone assay6 ( data supplement ) and the number of nonsynonymous mutations was calculated per tumor by summing known or likely mutations and variants of unknown significance . 
the icam threshold projected from tcga was estimated as nine or 14 nonsynonymous mutations for foundationone assays that interrogated 236 or 315 genes , respectively ( data supplement )  . 
immune checkpointactivating mutation ( icam ) positive tumors can be identified with high accuracy using routine clinical assays . receiver operating characteristic curves for icam status determination of the cancer genome atlas ( tcga ) samples using only the exons used in foundationone6 ( blue ) and strandadvantage15 ( gold ) assays . 
blca , bladder cancer ; cesc , cervical cancer ; coad , colon adenocarcinoma ; luad , lung adenocarcinoma ; skcm , skin cutaneous melanoma ; stad , stomach adenocarcinoma ; ucec , endometrial cancer . false positive rate ( 1 specificity ) tumors ( but not icam - negative tumors ) had mutations in rnf43 , arid1a , braf , bmpr2 , acvr2a , and rpl22 . 
egfr mutations in lung cancer and apc and tp53 mutations in colon cancer were associated with lower incidences of icampositive tumors , whereas mutations in arid1a in lung cancer and mutations in rnf43 , arid1a , braf , bmpr2 , and acvr2a in colon cancer were associated with higher incidences of icampositive tumors ( data supplement )  . 
tumor suppressor genes rnf43 , 19 acvr2a , 20 and rpl2221 were significantly mutated in icam - positive colon adenocarcinoma ( fig 5 ) , endometrial cancer , and stomach adenocarcinoma ( data supplement ) , but rarely in icam - negative tumors . 
in the other four cancer types , several genes were significantly mutated in icam - positive but not icam - negative tumors and vice versa ( data supplement )  . 
these findings suggest that icam - positive tumors may have distinct underlying driver mutations compared with icam - negative tumors . mutational etiology of icam - positive tumors for each tumor , we estimated the fractional contribution of 30 mutation signatures ( data supplement ) from the catalogue of somatic mutations in cancer22 , 23 ( uk / cosmic / signatures )  . 
compared with icamnegative tumors , icam - positive tumors had a higher contribution from an ultraviolet signature in melanoma and a smoking signature in lung adenocarcinoma ( fig 6a ) , consistent with known pathogenesis of melanoma24 and lung25 cancers . smoking history was also strongly associated with icam status in lung adenocarcinoma ( data supplement )  . in colon adenocarcinoma , endometrial cancer , and stomach adenocarcinoma , icam - positive tumors were enriched in either mismatch repair or pole proofreading defects ( fig 6a )  . 
prospective validation of immune checkpointactivating mutation ( icam ) threshold for melanoma using foundationone6 assay results predicts outcome of immune checkpoint blockade in an independent cohort of patients with melanoma . shown are comparisons of response rates , progression - free survival ( pfs ) , and overall survival in 113 patients with metastatic melanoma treated with single - agent programmed death - 1 ( pd - 1 ) targeted therapy , stratified by icam status using the foundationone assay.6 cr , objective complete response ; pd , progressive disease ; pr , objective partial response ; sd , stable disease ( includes mixed response )  . time ( years ) time ( years ) apolipoprotein b mrna editing enzyme , catalytic polypeptide - like mutation signatures ( fig 6a ) , which builds on the previously reported presence of apolipoprotein b mrna editing enzyme , catalytic polypeptice - like signatures in these cancers.27 in er - positive / her2 - negative breast cancer , approximately 25% of luminal - b tumors were icam positive , whereas , 10% of luminal - a tumors were icam positive ( data supplement )  . 
in all eight cancer types , icam - negative tumors had a higher fractional contribution from deamination of 5 - methylcytosine compared with icam - positive tumors ( fig 6a )  . additional immunologic properties of icam - positive tumors in most of the eight cancer types , icam - positive tumors had significantly higher fractions of natural killer cells in leukocytes and m1 cells in macrophages , and significantly lower fractions of regulatory t cells in t cells ( fig 6b ) , by cibersort9 analysis . 
natural killer cells are involved in immune surveillance , 28 m1 macrophages suppress angiogenesis and induce apoptosis , 29 and regulatory t cells suppress immune response.30 thus icam - positive tumors may have a more favorable immune microenvironment for immune checkpoint therapy . 
these data are consistent with reports suggesting that specific features of immune microenvironments may associate with response to immune checkpoint therapy.31 , 32 sixty - one genes were significantly overexpressed in icam - positive tumors compared with icamnegative tumors in all eight cancer types ( data supplement ) , and approximately 70% of these genes were immune - system related : associated with the interferon - gamma pathway ( ifng , cxcl9 , cxcl10 , and cxcl11 ) and cytotoxic t cells ( cd8a , prf1 , gzma , and gzmb )  . expression of interferon - pathway genes is associated with recruitment of cytotoxic t cells to the tumor microenvironment.33 the immune checkpoint gene lag3 was significantly overexpressed in icam - positive tumors in all eight cancers , suggesting an additional drug target pathway . discussion in eight of 33 solid cancers in tcga , we found a mutational burden threshold ( icam ) that identified tumors with signatures of immune checkpoint activation . 
the icam threshold can be accurately identified using routine clinical sequencing assays . applied to an independent melanoma data set using the foundationone assay , 6 icam - positive status was able to identify responders to singleagent pd - 1 blockade with high accuracy . 
note that these assays do not have germline controls , so some variant calls may be rare germline polymorphisms . however , these should not affect the presence of an icam threshold . 
the thresholds found in this study could be further refined by removing likely germline variants , increasing sequencing depth , analyzing more samples , and conducting a detailed analysis of tumor purity and mutant allele frequency . 
selected significantly mutated genes ( mutsigcv , 17 false discovery rate , 0.1 ) in immune checkpoint activating mutation ( icam ) positive and icam - negative tumors . columns are samples and rows are genes ( white , gene not significantly mutated in that class ; gold , gene significantly mutated in that class but not mutated in that sample ; blue and gray , gene significantly mutated in icam - positive [ blue ] / icam - negative [ gray ] class and mutated in that sample )  . in many cancer types , a robust mutational burden threshold associated with evidence of immune checkpoint activation could not be identified . 
this includes triple - negative breast cancer and renal cell carcinoma , which are cancers with substantial response rates to single - agent immune checkpoint blockade.13 , 14 in these cancers , features other than tumor mutational load are probably responsible for immune checkpoint activation . 
similarly , other features , such as viral etiology , seen in merkel cell cancer , may be strongly immunogenic , yet do not associate with a high nonsynonymous mutational burden.35 , 36 the patterns of mutations present in icampositive tumors reflect the underlying nature of mutagenesis . 
 ( a ) comparison of the fractional contribution of mutation signatures from catalogue of somatic mutations in cancer for etiologies associated with icam - positive versus icamnegative status in the eight cancer types . 
 ( b ) other immune signatures associated with icam status ( natural killer [ nk ] fraction in leukocytes , m1 fraction in macrophages , and regulatory t cell ( t - regs ) fraction in t cells in icam - positive and icam - negative tumors )  . 
similarly , some patients with icam - negative cancers did respond to pd - 1 or ctla - 4 blockade , possibly because of immune responses triggered by mechanisms other than high mutational burden ( eg , expression of exogenous viruses , 35 , 36 expression of endogenous retroviruses40 )  . 
for more information about ascos conflict of interest policy , please refer to or ascopubs.org / po / author - center . anshuman panda no relationship to disclose anil betigeri employment : strand life sciences kalyanasundaram subramanian employment : strand life sciences , syngene international patents , royalties , other intellectual property : patent to predict drug toxicity jeffrey s . 
pavlick employment : foundation medicine stock and other ownership interests : foundation medicine siraj ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health on microbiome stuff in non - neoplastic disease ( i ) paul markowski no relationship to disclose howard l . 
kaufman employment : compass therapeutics leadership : compass therapeutics honoraria : amgen , emd serono , merck , celldex , prometheus , turnstone bio , compass therapeutics consulting or advisory role : amgen , merck , merck serono , paometheus , celldex , turnstone bio , bristol - myers squibb , compass therapeutics speakers bureau : merck research funding : amgen ( inst ) , merck ( inst ) travel , accommodations , expenses : emd serono , turnstone bio edmund lattime stock and other ownership interests : johnson & johnson ( i ) patents , royalties , other intellectual property : i am an inventor of an oncolytic virus , for which the patent is held by thomas jefferson university , where i worked from 1989 to 1998 . 
mehnert honoraria : genentech , emd serono consulting or advisory role : merck sharp & dohme , amgen research funding : merck ( inst ) , sanofi ( inst ) , novartis ( inst ) , polynoma ( inst ) , immunocore ( inst ) , amgen ( inst ) , astrazeneca ( inst ) travel , accommodations , expenses : emd serono , merck sharp & dohme other relationship : amgen , emd serono , merck ryan sullivan honoraria : genentech consulting or advisory role : novartis , biodesix , paometheus , amgen , takeda , worldcare clinical , aci clinical , merck , biolinerx research funding : amgen ( inst ) , eli lilly ( inst ) , biomed valley discoveries ( inst ) , merck ( inst ) , deciphera ( inst ) , genentech ( inst ) other relationship : boehringer ingelheim christine m . 
lovly honoraria : novartis , sequenom , qiagen , pfizer , nccn , takeda consulting or advisory role : ariad , clovis oncology , genoptix , novartis , foundation medicine research funding : astrazeneca , novartis travel , accommodations , expenses : pfizer jeffrey sosman honoraria : amgen , merck , array biopharma , bristol - myers squibb consulting or advisory role : amgen , merck , array biopharma , bristol - myers squibb douglas b . 
 shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis patents , royalties , other intellectual property : i hold two patents for digital imaging that may be licensed to ibris and inspirata . travel , accommodations , expenses : inspirata acknowledgment we thank hossein khiabanian , phd , for help with analysis of the foundation medicine mutation data for the rutgers cancer institute of new jersey samples in the prospective cohort . affiliations anshuman panda , ann silk , howard l . 
mehnert , and shridar ganesan , rutgers robert wood johnson medical school , new brunswick ; anshuman panda and gyan bhanot , rutgers university , piscataway , nj ; anil betigeri and kalyanasundaram subramanian , strand life sciences , bangalore , india ; jeffrey s . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
koo b - k , spit m , jordens i , et al : tumour suppressor rnf43 is a stem - cell e3 ligase that induces endocytosis of wnt receptors . 
deacu e , mori y , sato f , et al : activin type ii receptor restoration in acvr2 - deficient colon cancer cells induces transforming growth factor - beta response pathway genes . 
rao s , stadanlick je , cai kq , et al : loss of rpl22 promotes tumor progression through regulation of angiogenesis . cancer res 75 , 2015 ( suppl 15 ; abstr 521 ) 22 . 
yuan a , hsiao y - j , chen h - y , et al : opposite effects of m1 and m2 macrophage subtypes on lung cancer progression . sci rep 5 : 14273 , 2015 30 . 
nghiem pt , bhatia s , lipson ej , et al : pd - 1 blockade with pembrolizumab in advanced merkel - cell carcinoma . n engl j med 374 : 2542 - 2552 , 2016 36 . 
kaufman hl , russell j , hamid o , et al : avelumab in patients with chemotherapy - refractory metastatic merkel cell carcinoma : a multicentre , single - group , open - label , phase 2 trial . 
marvel d , gabrilovich di : myeloid - derived suppressor cells in the tumor microenvironment : expect the unexpected . j clin invest 125 : 3356 - 3364 , 2015 39 . 
laboratory tests , magnetic resonance imaging ( mri ) , and positron emission tomographycomputed tomography did not indicate involvement of organs other than the skbecause of the limited cutaneous lesions classified as single system lch , topical corticosteroids were used as first - line treatment for 10 weeks , with no improvement . 
treatment with desmopressin ( initial dosage , 0.4 mg daily divided into three doses ) was started , and polyuria and polydipsia improved . function of the anterior pituitary was not affected . targeted next - generation sequencing of the skin biopsy indicated an activating mutation in mek1 ( p.e102_i103delei ; fig 3 )  . 
for this mutation , ex vivo sensitivity to an mek inhibitor ( meki ) has been reported.1a because the skin and the pituitary gland were affected , the disease was now classified as multisystem lch . 
finally , an off - label treatment with trametinib was offered to the patient after interdisciplinary discussion . after detailed explanation and obtaining informed consent , trametinib ( 2 mg once daily ) was started . an mri performed 4 weeks later showed a significant shrinkage of the pituitary enlargement ( fig 3 ) , and skin manifestations resolved both clinically and histologically ( fig 1 )  . 
positron emission tomographycomputed tomography and mri performed in week 12 of treatment showed a slight increase of the pituitary gland in size ; however , the patient had not been receiving trametinib in the previous 3 weeks . 
importantly , the daily dose of desmopressin could be reduced to 0.1 mg / d on trametinib treatment , and anterior pituitary function remained normal . because of the excellent overall response , a drug holiday was recommended , and trametinib treatment was stopped in week 38 . 
hematoxylin and eosin ( h&e ) staining and immunohistochemistry of langerin of a biopsy taken from cutaneous lesions before therapy ( left panels ) and after 4 weeks of therapy ( right panels )  . 
initially , a band - like infiltrate by histiocytes with reniform nuclei and eosinophilic cytoplasm ( upper left , h&e ) reactive with an antilangerin antibody ( brown , lower left ) was observed in the upper dermis and also perifollicular in the lower dermis . 
roughly , clinical subtypes are divided into single system and multisystem ( ms ) forms.3 limited disease usually causes low morbidity , but ms - lch or leukemic forms are a severe threat for patients . organ involvement can cause significant morbidity in patients with lch . 
standard therapies for ms - lch in adults are cytotoxic regimens.4 , 5 radiotherapy is used to treat pituitary lch ; however , this contributes to gradual and often complete loss of anterior pituitary function.6 , 7 the mitogen - activated protein kinase ( mapk ) pathway is critical for cell survival and proliferation . it can be activated by various receptor tyrosine kinases but also by oncogenic mutations in braf or nras found in melanoma and other human malignancies . 
recently , recurrent oncogenic mutations affecting the mapk pathway have been described in lch.1a , 8 these mutations affect braf in approximately 50% and mitogenactivated protein kinase 1 ( map2k1 / mek1 ) in approximately 25% of patients . 
mutations in these genes seem to be mutually exclusive.8 in a multibasket trial for malignancies harboring brafv600 mutations , targeted therapy with the selective braf inhibitor ( brafi ) vemurafenib showed clinical activity in lch.9 besides selective brafi , other small molecules , such as meki , have been evaluated in cancers with oncogenic mapk activation.9 , 10 it has been proposed that activating mek1 mutations is a difficult target in the treatment of lch.3 however , no clinical data on mek inhibition in patients with lch have been reported so far . ( poly ) chemotherapy and radiation are considered standard of care for treatment of ms - lch.3 - 7 high rates of toxicity are observed in adults , and recovery of endocrine function of the pituitary gland is rarely observed with these therapies . 
in week 4 of therapy with trametinib , a significant shrinkage and only a residual contrast enhancement were found . after short - term treatment break , the posterior pituitary gland appeared slightly enlarged again in week 12 . 
in week 28 , size was normalized . representative sagittal images from t1 contrastenhanced magnetic resonance imaging sequences shown ; arrows indicate affected part of the hypophysis . pretreatment after 4 weeks after 12 weeks after 28 weeks harboring a somatic mutation in mek1 . 
radiotherapy and chemotherapy might eventually still have to be considered in these patients . it remains unclear if meki can induce durable responses in lch and non - lch with lasting functional recovery of organs involved . 
 ( b ) the wildtype braf sequencing result is shown with a dotted line and arrow highlighting the c.t1799 location where a braf v600e mutation would be detected if it had been present . 
moeller , dagmar f uhrer , lisa zimmer , antje sucker , dirk schadendorf , elisabeth livingstone , bastian schilling data analysis and interpretation : matina papapanagiotou , klaus g . 
t1799 uwe hillen honoraria : novartis consulting or advisory role : novartis , roche , therakos research funding : novartis ( inst ) travel , accommodations , expenses : novartis tobias t . 
moeller honoraria : pfizer , henning dagmar f uhrer honoraria : ipsen , sanofi , bayer healthcare pharmaceuticals , eisai , genzyme , sobi , pfizer consulting or advisory role : novartis ( inst ) , ipsen , sanofi , bayer , eisai , genzyme , sobi , pfizer research funding : novartis ( inst ) , pfizer ( inst ) , ipsen ( inst ) , novartis , pfizer travel , accommodations , expenses : ipsen , sanofi , bayer , eisai , genzyme , sobi , pfizer lisa zimmer honoraria : novartis , merck sharp & dohme , bristol - myers squibb , roche , merck , glaxosmithkline consulting or advisory role : novartis , bristol - myers squibb , merck sharp & dohme , roche travel , accommodations , expenses : novartis , bristolmyers squibb , amgen , merck sharp & dohme alexander roesch research funding : novartis travel , accommodations , expenses : roche , bristol - myers squibb , merck sharp & dohme , amgen , novartis klaus g . 
 dirk schadendorf honoraria : amgen , array , astra zeneca , bristol - myers squibb , immunocore , merck sharp & dohme , merck , novartis , pfizer , philogen , pierre fabre , regeneron , roche consulting or advisory role : amgen , array biopharma , astrazeneca , bristol - myers squibb , immunocore , merck sharp & dohme , merck , novartis , pfizer , philogen , pierre fabre , regeneron , roche speakers bureau : amgen , bristol - myers squibb , merck sharp & dohme , novartis , pierre fabre , roche research funding : amgen ( inst ) , array ( inst ) , bristol - myers squibb ( inst ) , immunocore , merck sharp & dohme ( inst ) , novartis ( inst ) , philogen ( inst ) , regeneron ( inst ) , roche ( inst ) , bristol - myers squibb , novartis travel , accommodations , expenses : amgen , array , astra zeneca , bristol - myers squibb , immunocore , merck sharp & dohme , merck , novartis , pfizer , philogen , pierre fabre , regeneron , roche elisabeth livingstone no relationship to disclose bastian schilling honoraria : novartis , roche , bristol - myers squibb , merck sharp & dohme consulting or advisory role : roche , bristol - myers squibb speakers bureau : roche , bristol - myers squibb , merck sharp & dohme research funding : bristol - myers squibb ( inst ) , merck sharp & dohme travel , accommodations , expenses : novartis , roche , bristol - myers squibb , amgen matina papapanagiotou , klaus g . 
m oller i , murali r , m uller h , et al : activating cysteinyl leukotriene receptor 2 ( cysltr2 ) mutations in blue nevi . mod pathol 30 : 350 - 356 , 2017 2 . 
girschikofsky m , arico m , castillo d , et al : management of adult patients with langerhans cell histiocytosis : recommendations from an expert panel on behalf of euro - histio - net . 
duan mh , han x , li j , et al : comparison of vindesine and prednisone and cyclophosphamide , etoposide , vindesine , and prednisone as first - line treatment for adult langerhans cell histiocytosis : a single - center retrospective study . 
endocrine 48 : 949 - 956 , 2015 imashuku s , kudo n , kaneda s , et al : treatment of patients with hypothalamic - pituitary lesions as adult - onset langerhans cell histiocytosis . 
hyman dm , puzanov i , subbiah v , et al : vemurafenib in multiple nonmelanoma cancers with braf v600 mutations . 1919 - 1923 , 2010 n engl j med 373 : 726 - 736 , 2015 10 . 
walsh , md1 , 2 ; rosalba sacca , phd1 ; temima wildman , ms1 ; kimberly amoroso , ms1 ; jennifer kennedy , ms1 ; liying zhang , md , phd1 ; ozge birsoy , phd1 ; diana mandelker , md , phd1 ; zoe steinsnyder1 ; alicia latham , md1 , 2 ; maria i . 
stadler , md1 , 2 ; and kenneth oft , md , mph1 , 2 introduction telomere length assessthe original dyskeratosis congenita , telomere syndrome , was clinically described more than 100 years ago on the basis of individuals who presented with a distinct rash , abnormal nails , and whitening of the tongue.1 from this rare syndrome , our clinical and molecular understanding of telomere syndromes has evolved and has now expanded to include aplastic anemia , myelodysplastic syndrome , and pulmonary brosis.2 - 5 the identication of patients with telomere syndromes is of signicant clinical importance because these patients are exquisitely sensitive to alkylating chemotherapeutic agents and ionizing radiation.6 - 8 precision medicine efforts that deploy tumor - normal sequencing have used various molecular assays and platforms to interrogate and annotate the cancer census genes.9 , 10 tert , a gene that encodes a key protein involved in telomere maintenance , has been analyzed predominantly to identify genomic alterations that occur in tumors.11 , 12 although constitutional telomere syndromes are recognized , they are rarely considered in the oncologists differential diagnosis unless a diagnosis of a telomere syndrome occurred before the patients cancer diagnosis.13 from january 2016 to may 2019 , unselected patients with advanced solid tumors were presented with the option to participate and consent to a memorial sloan kettering cancer center institutional review board approved protocol ( #12 - 245 ; clinicaltrials.gov identier : nct01775072 ) of tumor and germline dna sequencing . 
cancer types in our cohort included four female patients with breast cancer ( ages at diagnosis , 28 , 37 , 46 , and 58 years ) , one male patient with gall bladder adenocarcinoma ( age 33 years ) , one male patient with pancreatic ampullary adenocarcinoma ( age 45 years ) , and one male patient with two malignancies : lymphoma at age 58 years and prostate cancer at age 66 years . 
in the six patients with a solid tumor as their rst malignancy , all were younger than the median age of diagnosis in the general population for their type of cancer24 - 27 ( data supplement )  . clinical histories of three ( 42.8% ) of the seven patients were suggestive of telomere syndromes . 
individual i , diagnosed with breast cancer , endured therapy - induced radiation pneumonitis and refractory thrombocytopenia ; individual iv , diagnosed with ampulla of vater cancer , experienced premature graying and thrombocytopenia that preceded a cancer diagnosis at age 19 years ; and individual vii revealed a history of bone marrow failure in a family member with a segregating tert mutation and showed abnormal pulmonary function testing ( table 1 )  . an understanding of the genetic basis that contributes to therapeutic sensitivities is important for oncology patients who receive chemotherapy , radiation , and other biologic therapeutics . 
patients with telomere syndromes may manifest overt or subtle clinical ndings.5 moreover , for patients with both obvious and subtle telomere syndromes , exquisite treatment sensitivities have been reported.6 , 7 although only one in 1 , 571 individuals in this series of patients with advanced cancer showed a germline tert mutation , this could translate to more than 1 , 000 patients diagnosed with malignancies a year in the united states who may have increased therapeutic sensitivities . 
because telomere syndrome disorders are complex and exhibit anticipation , incomplete penetrance , multiple genes that underpin disease , recognized modiers , and both autosomal dominant and autosomal recessive patterns of inheritance , this estimate will be rened with time . however , until a clearer picture is possible , it seems reasonable for individuals with constitutional germline tert mutations to be considered for monitoring given the potential long - term sequalae from chemotherapy and radiation as well as increased organ - specic damage.7 , 8 , 31 for two individuals , telomere length testing through cytometric uorescence in situ hybridization identied telomere lengths in the 1st percentile or less ; in two additional individuals , telomere lengths were in the 10th percentile or telomere length less ; and in one additional testing failed because of low blood counts that did not recover after chemotherapy ( fig 1 )  . 
somatic mutation analysis of all ve individuals with germline tert mutations and tumor specimens available for analysis individual , integration of germline , somatic , and clinical data for patients in our cohort was also notable for somatic tp53 mutations and a younger age at cancer diagnosis compared with the general population . 
moreover , multiple tert single nucleotide polymorphisms have been shown to be associated with telomere length and breast and ovarian cancer risk.31 all this information together with telomere lengths may provide insights for stratifying patients with regard to age at presentation , outcome , and tumor evolution . lymphocytes granulocytes 99th percentile 50th percentile 90th percentile 99th percentile 50th percentile 90th percentile 1st percentile 10th percentile 1st percentile 10th percentile age ( years ) age ( years ) fig 1 . 
 e walsh et al e113rfs * 79 p308hfs * 43 l392vfs * 145 r486c v694m exon 4 deletion f1084 * telomerase rvt1 1 , 000 1 , 132 aa a86vfs * 55 y163 * m237i m273h / c truncating mutations missense mutations rvt1 i , v / vi fig 2 . 
walsh , md , memorial sloan kettering cancer center , 222 70th st , room 412 , new york , ny 10021 ; e - mail : walshm2@ makcc.org. support supported by the robert and kate niehaus center for inherited cancer genomics and members of the molecular diagnostics service in the department of pathology and the marie - jos ee and henry r . 
also receives grant support from the v foundation , corning fund , and crawford fund for pediatric genomics . all authors at memorial sloan kettering are supported by the memorial sloan kettering cancer center support grant / core grant through national cancer institute grant no . 
walsh , kimberly amoroso , liying zhang collection and assembly of data : rosalba sacca , temima wildman , kimberly amoroso , jennifer kennedy , ozge birsoy , zoe steinsnyder , alicia latham , maria i . 
carlo consulting or advisory role : pzer other relationship : prostate cancer foundation , robert wood johnson foundation karen cadoo research funding : astrazeneca ( inst ) , syndax ( inst ) travel , accommodations , expenses : astrazeneca mark robson honoraria : astrazeneca consulting or advisory role : mckesson , astrazeneca references research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca , pzer other relationship : research to practice , clinical care options , physician education resource zsoa k . 
stadler consulting or advisory role : allergan ( i ) , genentech ( i ) , roche ( i ) , regeneron pharmaceuticals ( inst ) , optos ( i ) , adverum ( i ) , biomarin ( i ) , alimera sciences ( i ) , novartis ( i ) , spark therapeutics ( i ) , fortress biotech ( i ) , regenxbio ( i ) no other potential conicts of interest were reported . zinsser f : atrophia cutis reticularis cum pigmentatione , dystrophia unguium et leukoplakia oris . 
n engl j med 361 : 2353 - 2365 , 2009 alder jk , guo n , kembou f , et al : telomere length is a determinant of emphysema susceptibility . 
am j respir crit care med 184 : 904 - 912 , 2011 alder jk , parry em , yegnasubramanian s , et al : telomere phenotypes in females with heterozygous mutations in the dyskeratosis congenita 1 ( dkc1 ) gene . hum mutat 34 : 1481 - 1485 , 2013 armanios m , blackburn eh : the telomere syndromes . 
nat rev genet 13 : 693 - 704 , 2012 [ erratum : nat rev genet 14 : 235 , 2013 ] agrusa je , bertuch aa , dinardo cd , et al : severe therapy - related toxicities after treatment for hodgkin lymphoma due to a pathogenic tert variant and shortened telomeres . 
pediatr blood cancer 66 : e27779 , 2019 de la fuente j , dokal i : dyskeratosis congenita : advances in the understanding of the telomerase defect and the role of stem cell transplantation . 
pediatr transplant 11 : 584 - 594 , 2007 dietz ac , orchard pj , baker ks , et al : disease - specic hematopoietic cell transplantation : nonmyeloablative conditioning regimen for dyskeratosis congenita . bone marrow transplant 46 : 98 - 104 , 2011 cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
rusch m , nakitandwe j , shurtleff s , et al : clinical cancer genomic proling by three - platform sequencing of whole genome , whole exome and transcriptome . nat commun 9 : 3962 , 2018 11 . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
hampel h , bennett rl , buchanan a , et al : a practice guideline from the american college of medical genetics and genomics and the national society of genetic counselors : referral indications for cancer predisposition assessment . 
weitzel jn , blazer kr , macdonald dj , et al : genetics , genomics , and cancer risk assessment : state of the art and future directions in the era of personalized medicine . 
noone am , cronin ka , altekruse sf , et al : cancer incidence and survival trends by subtype using data from the surveillance epidemiology and end results program , 1992 - 2013 . 
bojesen se , pooley ka , johnatty se , et al : multiple independent variants at the tert locus are associated with telomere length and risks of breast and ovarian cancer . 
 mutational landscape in resected periampullary adenocarcinoma : relationship with morphology and clinical outcome sebastian lundgren , md1 ; soe olsson hau , md1 ; jacob elebro , md , phd1 ; margareta heby , md , phd1 ; emelie karnevi , phd1 ; bj orn nodin , phd1 ; jakob eberhard , md , phd1 ; karolina holm , phd1 ; johan staaf , phd1 ; g oran b . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction periampullary adenocarcinoma is a collective term for tumors arising in the area surrounding the ampulla of vater , including the head of the pancreas , the duodenum , and the common bile duct . 
a morphologic classication into intestinal type ( i - type ) and pancreatobiliary type ( pb - type ) has been shown to provide better prognostic information than anatomic origin , with the former having a more favorable clinical outcome.1 - 3 although a plethora of mutations has been documented in pancreatic cancer , 4 - 7 the mutational landscape of other periampullary cancers has been less studied . 
no targeted therapies have proven to be efcient , and adjuvant chemotherapy therefore remains standard of care after resection of these tumors . hence , there is evident need for additional studies on the distribution and clinical signicance of the mutational landscape in the full range of periampullary including pancreatic cancer , adenocarcinomas , enable a better patient stratication and identify potential responders to targeted therapies . 
 lundgren et al context ( cid : 129 ) to what extent does morphology inuence the mutational landscape in periampullary adenocarcinomas , and can we nd novel prognostic and predictive biomarkers that differ by morphology , so as to better characterize this heterogeneous group of tumors in a clinical context ? ( cid : 129 ) the results presented here demonstrate that the distribution and prognostic impact of mutations in key genes indeed differ according to morphology and that emphasis on morphology rather than anatomy is of importance . 
approval for the study was obtained from the ethics committee of lund university ( reference number 445 / 07 ) , whereby the committee waived the need for consent other than the option to opt ; out . next - generation sequencing tissue cores of 1 - mm diameter were taken from tumor cellenriched formalin - xed parafn - embedded tissue . dna extraction was performed using the qiagen generead ( qiagen , hilden , germany ) kit for formalin - xed parafnembedded tissue according to the manufacturers instructions . 
forty - one ( 39.8% ) were classied as i - type and 62 ( 60.2% ) as pb - type . a panel of 70 cancer - associated genes was put together for this study and characterized using illumina truseq custom amplicon assay ( illumina , san diego , ca ) with a miseq instrument according to manufacturers instructions . 
detected mutations were screened against the cosmic and exac databases , to lter single - nucleotide polymorphisms commonly reported in different populations . immunohistochemical analysis of brahma - related gene 1 protein expression immunohistochemical analysis of brahma - related gene 1 ( brg1 ) protein expression , 4 - m tissue microarray sections were automatically pretreated in the pt - link system ( dako , glostrup , denmark ) and stained in an automated immunostainer ( autostainer plus , dako ) using the dako envision flex + detection system , peroxidase / dab , rabbit / mouse with the monoclonal anti - brg1 antibody clone g - 7 ( santa cruz biotechnology , dallas , tx ) , diluted 1 : 25 . brg1 was expressed in the tumor cell nuclei and present in the majority of tumor cells in positive cases . 
kaplanmeier analysis log - rank test was applied to illustrate any difference in 5 - year overall survival ( os ) , and cox regression proportional hazard models were used to estimate hazard ratios ( hrs ) for death within 5 years in both univariable and multivariable analysis . 
multivariable cox regression included adjustment for age ( continuous ) , t - stage ( t1 or t2 v t3 or t4 ) , n - stage ( negative v positive nodal status ) , grade ( well to moderate v poor ) , morphology ( i - type v pb - type ) in the entire cohort , adjuvant chemotherapy ( none v any ) , invasion into vascular and lymphatic structures , and perineural growth . 
the proportional hazard ( ph ) assumption was tested using cox regression with a timedependent covariate analysis , whereby the ph assumption was considered to be satised when the factor time interaction was nonsignicant . 
the ph assumption was also evaluated graphically using log - minus - log plots . in the entire cohort , three cases were excluded in the survival analyses : one patient with a pb - type tumor who was lost to follow - up because of emigration , and two patients with i - type tumors who died as a result of complications from the initial surgical treatment . 
to estimate the interaction treatment and selected bioeffect between adjuvant markers , the following interaction variable was constructed : any adjuvant treatment ( + / ) biomarker ( + / )  . 
all data generated or analyzed during this study are included in this published article ( data supplement )  . results distribution of mutations according to morphologic type there were no signicant differences in the distribution of clinicopathological characteristics between cases with known and unknown mutational status ( data supplement )  . the frequency of mutations according to morphologic type is shown in figure 1 and further outlined in the data supplement . 
the frequency of mutations according to anatomic origin is shown in the data supplement . prognostic impact of the most frequent mutations kaplan - meier analyses demonstrate a signicantly prolonged os for patients with i - type compared with patients with pb - type tumors ( data supplement )  . 
when stratifying for anatomic origin , the survival curves cluster into two groups concordant with morphology ( data supplement )  . of the nine most frequently mutated genes outlined above , only apc , erbb3 , kras , and smarca4 were shown to confer a prognostic value , depending on the context . 
apc mutation was not prognostic in i - type tumors ( data not shown ) , and erbb3 mutation was not prognostic in analyses stratied for morphology ( data not shown )  . kras mutation was the strongest predictor of survival , as visualized in figure 2 . 
when stratifying for ampullary origin , kras mutation remained a prognostic factor in i - type tumors ( p = 0.033 ; fig 2d ) but was not prognostic in pb - type tumors ( fig 2e )  . 
 intestinal type pancreatobiliary type tp53 kras rnf43 smad4 erbb3 smarca4 cdkn2a lundgren et al tp53 kras rnf43 smad4 smarca4 cdkn2a erbb3 genetic alteration no alterations truncating mutation in - frame mutation missense mutation fig 1 . 
the genetic alterations were classied as either truncating , missense , or in - frame mutations . mutation did not differ according to adjuvant chemotherapy in i - type tumors ( data not shown )  . 
in the entire cohort , high brg1 expression was an adverse prognostic factor in patients not receiving adjuvant chemotherapy but was not prognostic in patients receiving adjuvant chemotherapy ( data not shown )  . 
the mutational burden of the analyzed genes did not differ signicantly between i - type and pb - type tumors ( p = .577 ) and was not prognostic in the whole cohort or stratied for morphologic type . discussion morphology is emerging as an important prognostic factor in periampullary adenocarcinoma , 1 , 2 and to our knowledge , this is the rst study to comprehensively map common cancer - associated mutations in the full range of periampullary adenocarcinoma , with particular reference to morphology . 
these ndings are in line with a study on 112 cancers of ampullary origin , demonstrating that the mutational spectrum in i - type tumors resembles that of colorectal cancer , and the mutational spectrum in pb - type tumors resembles that of pancreatic cancer.12 in the current study , mutations in apc but not in cdkn2a were found to be prognostic . 
given that no pb - type tumors harbored apc mutations , it is plausible to assume that the link between these mutations and a favorable outcome in the entire cohort is mainly due to their association with i - type morphology . 
the same line of reasoning applies to the association between erbb3 mutations , being more prevalent in i - type tumors , and a prolonged survival in the entire cohort . 
adding to this , there was no signicant association between her3 expression and erbb3 mutational status , and the clinical utility of assessment of erbb3 mutation status for prognostication purposes needs additional validation . kras mutation was found to signify a signicantly shorter survival in patients with i - type tumors , also when adjusted for established clinical factors , whereas patients with kras wild - type i - type tumors could indeed be classied as long - term survivors . 
as of yet , epidermal growth factor receptor ( egfr ) inhibition has not shown clinical efcacy in pancreatic cancer , 15 but no study has investigated the efcacy of egfr inhibitors in periampullary adenocarcinoma in relation to morphology . although none of the patients in this study had received egfr - inhibiting treatment , the ndings indicate that some ras wild - type periampullary cancers of i - type may indeed benet from such treatment . 
 mutational spectrum and morphology in periampullary cancer kras wt kras mut p = .033 kras wt kras mut p = .018 time since diagnosis ( months ) time since diagnosis ( months ) 2 . 
kaplan - meier curves visualize differences in 5 - year overall survival for patients with kras - mutated ( mut ) and wild - type ( wt ) tumors in ( a ) the entire cohort , intestinal - type tumors , ( c ) pancreatobiliary - type tumors , ( d ) intestinal - type amtumors , and ( e ) pullary pancreatobiliary - type pullary tumors . kras wt kras mut p = .680 kras wt kras mut p = .033 time since diagnosis ( months ) time since diagnosis ( months ) no . 
 lundgren et al smarca4 wt smarca4 mut p = .050 smarca4 wt smarca4 mut p = .803 time since diagnosis ( months ) time since diagnosis ( months ) score 0 score 2 score 3 brg1 low brg1 hight p = .061 brg1 low brg1 high p = .037 time since diagnosis ( months ) time since diagnosis ( months ) no . 
relationship of smarca4 mutation status and brahma - related gene 1 ( brg1 ) protein expression with overall survival according to adjuvant chemotherapy in patients with pancreatobiliary ( pb ) - type tumors . 
 ( a , b ) kaplanmeier curves visualizing differences in 5 - year overall survival in patients with pb - type tumors according to smarca4 mutation status ( a ) without adjuvant chemotherapy , and ( b ) with adjuvant chemotherapy . ( c ) sample immunohistochemical images of brg - 1 expression . 
 ( d , e ) kaplan - meier analyses visualizing differences in 5 - year overall survival in patients with pb - type tumors according to low and high brg1 expression ( d ) without adjuvant chemotherapy , and ( e ) with adjuvant chemotherapy . 
 mutational spectrum and morphology in periampullary cancer despite the lack of a signicant interaction between smarca4 mutation and adjuvant treatment , this observation led us to further explore the expression and prognostic value of brg1 , the protein encoded by smarca4 , in tumors from the full study cohort . 
brg1 was found to be an adverse factor in patients who did not receive adjuvant chemotherapy and , in addition , there was a signicant interaction with adjuvant chemotherapy in pbtype tumors . 
one study on pancreatic cancer ( n = 68 ) failed to demonstrate an association between brg1 expression and gemcitabine response or survival , 17 but the nding of a potential predictive role for smarca4 / brg1 in the current study merits further validation in additional patient cohorts . to our knowledge , this is the rst study to map the prevalence and prognostic signicance of mutations in common cancer - associated genes in the full spectrum of periampullary adenocarcinoma . 
in particular , kras mutation status may be a suitable biomarker for prognostication in patients with i - type tumors , and smarca4 / brg1 expression may add value in the prediction of response to adjuvant chemotherapy treatment in patients with pbtype tumors . 
bmc cancer 8 : 170 , 2008 bronsert p , kohler i , werner m , et al : intestinal - type of differentiation predicts favourable overall survival : conrmatory clinicopathological analysis of 198 periampullary adenocarcinomas of pancreatic , biliary , ampullary and duodenal origbmc cancer 13 : 428 , 2013 kimura w , futakawa n , zhao b : neoplastic diseases of the papilla of vater . 
nature 531 : 47 - 52 , 2016 genet 47 : 1168 - 1178 , 2015 collisson ea , sadanandam a , olson p , et al : subtypes of pancreatic ductal adenocarcinoma and their differing responses to therapy . 
nat med 17 : 500 - 503 , 2011 elebro j , jirstr om k : use of a standardized diagnostic approach improves the prognostic information of histopathologic factors in pancreatic and periampullary adenocarcinoma . 
diagn pathol 9 : 80 , 2014 elebro j , heby m , warfvinge cf , et al : expression and prognostic signicance of human epidermal growth factor receptors 1 , 2 and 3 in periampullary adenocarcinoma . 
philip pa , benedetti j , corless cl , et al : phase iii study comparing gemcitabine plus cetuximab versus gemcitabine in patients with advanced pancreatic adenocarcinoma : southwest oncology group - directed intergroup trial s0205 . 
 total number of alterations in liquid biopsies is an independent predictor of survival in patients with advanced cancers peter vu , md1 ; yulian khagi , md1 ; paul riviere , bs1 ; aaron goodman , md2 ; and razelle kurzrock , md1 purpose studies have demonstrated an association between quantity of circulating tumor dna ( ctdna ) and poorer survival . 
our ndings suggest that the total number of alterations in plasma may be an indicator of more aggressive tumor biology and therefore poorer survival . jco precis oncol 4 : 192 - 201 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction five - year survival rates are incredibly variable among cancer types , ranging from more than 90% in prostate cancer to less than 8% in pancreas cancer , and depend heavily on clinical and pathologic stage.1 although repeat tissue biopsies during the course of treatment or at the time of progression may provide clinically important information , such biopsies are not routinely performed because they can be technically difcult , time consuming , medically invasive , and lead to complications . 
however , liquid biopsies , or cell - free dna ( cfdna ) obtained from blood plasma that contains fragments of circulating tumor dna ( ctdna ) shed from tumor cells into the bloodstream , can identify new actionable alterations and be performed repeatedly with minimal procedural risk.2 - 5 ctdna can then be analyzed using technologies such as digital polymerase chain reaction to detect specic known somatic variants ( eg , egfr t790m ) or next - generation sequencing ( ngs ) that uses massive parallel sequencing to detect up to thousands of somatic and germline alterations in a single run.6 in addition , genomic alterations found on liquid biopsies are often concordant with alterations found on tissue biopsy when obtained within close proximity to one another.7 - 9 a number of studies have demonstrated that there is an association between higher amounts of cfdna or ctdna and poorer survival , perhaps because percent ctdna ( %ctdna ) correlates with tumor burden.10 , 11 for the most part , these reports dichotomized the level of cfdna or ctdna at a cut - point ( often but not always at approximately 5% or 10% ctdna ) .10 , 12 - 18 in the case of surgical candidates , the cut - points may be lower . 
eligible patients included those who had solid tumor malignancies , never received immunotherapy treatment , and were evaluable for clinical correlations , including overall survival ( os ) from ctdna collection date . 
immunotherapytreated patients were omitted because a correlation with blood or tissue tumor mutational burden has been associated with better immunotherapy response and might therefore alter the survival curve.19 , 20 patients with amplications only in ctdna were omitted because the %ctdna for amplications could not be determined . 
in addition to os evaluation , patients data were also collected and analyzed for %ctdna ; the alteration with the highest allele fraction was calculated from all alterations , including variants of unknown signicance ( vuss ) , total number of vuss , and total number of alterations ( which included vuss )  . 
all values for the total number of ctdna alterations and the number of vuss were corrected for the length ( kilobase pairs [ kbp ] ) of dna sequenced based on the date sequencing was performed and multiplied by 100 ( appendix table a1 )  . 
all data were analyzed from the time of ctdna collection from plasma ( two 10 - ml blood tubes )  . this ctdna assay has a sensitivity and specicity of  . 
hazard ratios ( hrs ) for survival were calculated by comparing os above and below cutoffs and performed from the time of ctdna collection ; dichotomization for each variable ( ie , total number of alterations , total number of vuss , %ctdna ) was performed at the median . 
multivariate analyses were conducted using the wald 2 test from a cox proportional hazards model that included all variables with p .05 in univariate analyses ( ie , sex , age , total number of alterations , %ctdna ) , with the exception of vuss because these alterations are already encompassed within the total number of alterations variable . 
associations between %ctdna and total number of alterations were determined using spearmans rank - order correlation . bootstrapping using random sampling with replacement ( n = 1 , 000 bootstrap samples ) and multiple logistic regression analysis were performed , permitting the data of the sample study to be used as a surrogate for a larger population to validate the model . 
intermediate to high %ctdna was dichotomized at 5% because it had been found to be signicant in prior studies.10 the %ctdna for each patient was calculated using the alteration with the highest allele fraction , including variants of unknown signicance validation cohort , as was the case in our study.22 statistical analyses were carried out using prism version 7.0 ( graphpad , san diego , ca ) and r version 3.5 ( r foundation for statistical computing , vienna , austria )  . results patient characteristics this study included 418 patients who had ngs performed on plasma - derived ctdna and did not receive immunotherapy treatment . 
after correcting for the kbp length of dna sequenced for each sample , the median total number of ctdna alterations ( including vuss ) per patient was 1.46 ( range , 0 - 78.8 ) ; the median total number of vus alterations per patient was 0.66 ( range , 0 - 64.2 ) ; and the median %ctdna was 0.4% ( range , 0% - 80.3% ; table 1 )  . 
 total number of alterations in liquid biopsies is prognostic regression model showed that age , sex , and the total number of alterations were independently prognostic for survival ( table 1 )  . 
among these characteristics , only total number of alterations was signicantly associated with survival ( p , .0001 ; table 1 )  . discussion liquid biopsies have been incorporated into clinical practice as a means to obtain noninvasive molecular proling to identify specic oncogenic driver mutations or other alterations that can guide treatment selection . 
in this study , we evaluated the relationship between the total number of alterations and the %ctdna detected by liquid biopsy and survival outcomes in 418 patients with advanced cancers . 
in addition , we intentionally excluded patients who subsequently received immunotherapy treatment , because several studies have suggested that the use of immune checkpoint inhibitors may alter the survival curve in patients with increased tumor mutational burden.19 , 20 , 23 we demonstrate that both the total number of alterations and the %ctdna have prognostic value and correlate with one another , but only an intermediate to high ( 1.46 ) total number of alterations / kbp ( and not high %ctdna ) was independently associated with worse survival outcomes in multivariate analysis in patients with gi tumors ( table 2 ) , as well as in patients with a diverse group of advanced cancers ( table 1 )  . 
it is also plausible that the higher number of alterations and accompanying aggressive biology results in a higher tumor burden that yields a higher %ctdna ( rather than vice versa )  . a strength of our study is that we used sequencing technology that allows for the detection of %ctdna at a low level with high sensitivity and high specicity.21 , 24 in comparison , some prior studies have used low - depth sequencing , which is less capable of detecting ctdna . 
as a result , these studies were only able to conclude that the presence of ctdna was associated with worse outcomes compared with the absence of detectable ctdna.14 , 18 , 25 , 26 indeed , yang et al27 proposed that the presence or absence of ctdna should be added to the tnm staging classication of tumors because it has diagnostic , therapeutic , and prognostic value . 
when greater depth of ctdna sequencing was used , prior studies have reported that %ctdna is correlated with worse survival and also with increased tumor volume.10 , 11 , 14 we also demonstrated that %ctdna correlates with survival measured from the time of blood draw ( fig 1 ) , which suggests that the association between %ctdna and outcomes may be more reective of tumor burden . limitations to our ndings , given the there are several retrospective nature of the analysis . 
although our study used a relatively large sample of 418 patients , we included a diverse group of advanced cancers and , therefore , our ndings may not be applicable to certain tumor types . despite this , the variety of tumor types in our study may make our ndings more generalizable across advanced total no . 
in addition , 112 patients in this study had no detectable %ctdna , which may be due to low disease burden or due to limitations of the ctdna sequencing technique . 
it should also be noted that there was a different number of subgroups in the analysis of %ctdna and number of ctdna alterations ; hence , the conclusion that the total number of alterations and %ctdna have prognostic value and correlate with one another but that only the total number of alterations was independently associated with survival outcomes will need to be further examined and validated . 
also , we do not know whether this patient population is comparable with those who were not analyzed for ctdna because physicians chose not to perform the analysis or with patients who were lost to follow - up early and hence were inevaluable . 
finally , patients had a diverse array of prior treatments , some of which could have confounded the results ; patients treated with immunotherapy were excluded because cancers with higher mutational burden / number appear to do better on this modality . in conclusion , to our knowledge , this is the rst demonstration that the total number of alterations and %ctdna are highly correlated and have prognostic value . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . support supported in part by the joan and irwin jacobs fund and by national cancer institute grant no . 
 total number of alterations in liquid biopsies is prognostic aaron goodman consulting or advisory role : mitsubishi tanabe pharma , gerson lehrman group , jazz pharmaceuticals , speakers bureau : seattle genetics razelle kurzrock leadership : curematch stock and other ownership interests : curematch , idbydna , soluventis , actuate therapeutics , loxo , xbiotech , neo - med , roche , gaido , soluventis , pzer , merck speakers bureau : roche research funding : guardant health ( inst ) , sequenom ( inst ) , merck serono ( inst ) , genentech ( inst ) , pzer ( inst ) , foundation medicine ( inst ) , incyte ( inst ) , konica minolta ( inst ) , grifols ( inst ) , omniseq ( inst ) , debiopharm group ( inst ) , boerhinger ingelheim ( inst ) no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
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intermediate to high %ctdna was dichotomized at 5% because it had been found to be signicant in prior studies.10 the %ctdna for each patient was calculated using the alteration with the highest allele fraction , including variants of unknown signicance . time ( months ) fig a2 . 
gazzaniga et al we are grateful for your comments on our recent publication1 that highlighted that nearly 50% of the patients with ras - mutated metastatic colorectal cancer and prior chemotherapy could display wildtype ras status in the circulating tumoral dna ( ctdna ) , and benet from the late introduction of an antiepidermal growth factor receptor ( egfr ) .2 we indeed acknowledge that your team had worked in a similar direction , and appropriately cited the report that your group published in 2019.3 this article also includes results from preliminary ndings in abstract forms . 
both of our works , as well as that from moati et al , 4 conrm the principle of expected efcacy from targeting egfr in the late stage of treatment of patients with ras - mutated colorectal cancer , if their liquid biopsy does not identify any ras mutation in the ctdna.2 - 4 however , there is a broad discrepancy in the rates of patients without ras mutation detection in plasma between these studies , ranging from 9 / 16 ( 56% ) , 2 through 5 / 11 ( 45% ) 3 to 8 / 36 ( 22% ) , 4 as also discussed in your opinion paper.5 a critical issue involves the conrmation of circulating tumoral dna in the absence of ras mutation , which could be reached through the detection of a persistent somatic mutation3 or the occurrence of wif1 / npy methylation.4 however , we concur and admit that these and other methods have intrinsic limitations , such that no standard one can currently ascertain the presence of circulating tumor dna in the absence of detected ras mutation.5 moreover , although their application drastically reduced the ras mutation conversion rate down to 6.6% - 14% , 3 , 4 this did not impair the fact that the introduction of an antiegfr apparently extended median progression - free survival to nearly 6 months in previously treated patients from both studies.2 , 3 therefore , we feel that two important issues need to be jointly addressed to advance the current guidelines for anti - egfr indication for metastatic colorectal cancer . 
gazzaniga p , nicolazzo c , caponnetto s , et al : about ras mutation clearance in plasma ctdna from ras - mutant colorectal cancer patients . jco precis oncol , 2021 2 . 
bouchahda m , saffroy r , karaboue a , et al : undetectable ras - mutant clones in plasma : possible implication for anti - egfr therapy and prognosis in patients with ras - mutant metastatic colorectal cancer . 
raimondi c , nicolazzo c , belardinilli f , et al : transient disappearance of ras mutant clones in plasma : a counterintuitive clinical use of egfr inhibitors in ras mutant metastatic colorectal cancer . 
nicolazzo c , belardinilli f , caponnetto s , et al : why the therapeutic impact of ras mutation clearance in plasma ctdna deserves to be further explored in metastatic colorectal cancer . 
 eye - tracking study to enhance usability of molecular diagnostics reports in cancer precision medicine purpose we conducted usability studies on commercially available molecular diagnostic ( mdx ) test reports to identify strengths and weaknesses in content and form that drive clinical decision making . 
this work aims to evaluate effectiveness of mdx reports in facilitating cancer treatment planning . methods fourteen clinicians at an academic tertiary care medical facility , with a wide range of experience in oncology and in the use of molecular testing , participated in this study . 
three commercially available , widely used , clinical laboratory improvement amendments ( clia ) certified , college of american pathologists ( cap ) accredited test reports ( labeled laboratories a , b , and c ) were used . 
eye tracking , surveys , and thinkaloud protocols were used to collect usability data for these mdx reports focusing on ease of comprehension and actionability results clinicians found two primary areas in molecular diagnostic reports most useful for patient care : therapy options with benefit or lack of benefit to patients , including enrolling clinical trials ; and pathogenic tumor molecular anomalies detected . 
however , all reports had usability and comprehension issues in these areas and could be improved . conclusion focused usability studies can help drive our understanding of the clinical workflow for use of molecular diagnostic tests in cancer care . 
2018 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license : introduction academic and community clinics are increasingly conducting genomic testing to inform treatment decisions for patients with cancer . 
accumulating research indicates significant potential to improve outcomes by effectively using this rich source of data in treatment planning , especially for clinical trial selection , by matching a patients molecular characteristics to trial eligibility criteria . currently , results from molecular diagnostic ( mdx ) testing are usually provided to clinicians and tumor boards as a multipage pdf document with a one - page summary highlighting any clinically actionable anomalies and treatment vishakha sharma allan fong robert a . 
 standards exist for classification , although they are not always adhered to by the testing vendors at this time.4 subsequent pages contain literature evidence associating the biomarkers to treatment and clinical trial options . 
biomarkers in mdx reports must be evaluated on the basis of their strength of evidence of clinical utility and actionability.5 , 6 mdx reports often provide an evaluation of the evidence and / or links to publications , but the evidence representation is not standardized . 
the increasing availability of mdx tests has caused concern , given the complexity of information presented.7 , 8 there is a clear need to enhance usability of patient - specific , clinically actionable molecular profiling information presented in mdx reports . electronic health record usability is a concern for health care vendors , because poor usability can lead to frustration and safety risks and can keep users from achieving their goals in routine work.9 , 10 the evaluation of cancer care and research products for usability and comprehension has been emphasized recently.3 , 11 - 13 usability techniques , such as surveys , thinkaloud protocols , semistructured interviews , and eye tracking , have been widely used in health care system design.9 , 14 - 21 usability evaluation of oncology electronic medical records and clinical practice guidelines have been performed using survey questionnaires and think - aloud protocols.22 - 26 eye tracking helps elucidate how users visually search and integrate information and has been used to understand the visual search patterns of anesthesiologists and emergency medicine physicians.27 , 28 methods experimental design we invited 43 oncology fellows and attending physicians ( 21 men , 22 women ) to participate in this study from the medstar health syste fourteen volunteered to participate ( 11 women , three men )  . 
six of 14 participants were excluded from the eye - tracking analysis because of low - quality eye - tracking data ( insufficient data for at least 75% of the session ) .28 eye - tracking studies with < 10 participants are common in anesthesiology and radiology studies.29 , 30 studies on usability are generally less concerned with sex variations in the population , unless the specific display requires knowledge that only a certain sex may have . 
 each participant reviewed three mdx reports in a randomly assigned three - period crossover design , which has the advantage of improved efficiency , because each participant serves as his / her own control.32 the reports chosen represent the three most commonly used clia - certified cap - accredited testing laboratories across the georgetown - medstar health system in the washington , dcbaltimore region . 
characteristics of the study participants all participants ( n = 14 ) eye tracking only ( n = 8 ) characteristic highest degree md , msc md , phd position fellow female male attending physician current specialty blood / marrow transplant oncology / breast oncology / gi oncology / hematology oncology / lung and brain years in practice weekly mdx reports weekly patients 5 - 10 10 - 15 20 - 30 5 - 10 0 - 10 10 - 25 25 - 50 50 - 100 abbreviation : mdx , molecular diagnostic . molecular test findings : gene / protein names , alterations , positive or negative test results ; and potential therapies : drug options and clinical trials . 
aois serve as meaningful regions in eye - tracking studies to correlate the eye movements with the interpretations provided by the clinicians from think - aloud recordings and survey answers . 
images of the mdx reports with aois as well as detailed descriptions of the similarities and differences between reports are provided in the data supplement . eye - tracking data collection eye - tracking was used to capture the visual scanning patterns of participants . 
we measured four common eye - tracking measures for all participants33 : fixation count : frequency of fixations within an aoi ; fixation duration : amount of time a participant fixated at an aoi ; refixation count : frequency of return fixations for an aoi ; and fixation transition : frequency of fixation transitions between aois . think - aloud protocol and recording in addition to eye tracking , each session involved a think - aloud protocol that was audio - video recorded . 
 recruit participants conduct eye - tracking study collect data outcomes analyze data for aois clinicians laboratory a laboratory b laboratory c three mdx reports from three laboratories were shown in randomized order eye - tracking survey questionnaire think - aloud protocol aois think - aloud data transcription ranked aois driving cancer treatment planning fig 1 . 
what if anything should be added to this patient report to help you make a treatment decision for this patient ? results comparison of mdx reports information and layout commonalities and variations in information content , location , and variation in labels and descriptive language used across the mdx reports and aois from laboratory a , b , and c were identified , analyzed , and categorized . 
six of 14 participants were excluded from the eye - tracking analysis because of insufficient eye - tracking data for at least 75% of the session.28 the survey results from eight clinicians with eye - tracking data were consistent with the results for the 14 in the relative numbers that agreed or disagreed on a question . 
survey results for just the eight with eye tracking and answers for all s5 suggestions for improvements are included in the data supplement . eye - tracking data analysis table 2 presents the eye movement measures for the three reports , fixation counts , average fixation durations , and refixations from eight participants . 
both higher fixation counts and longer fixation durations are indicative of deeper perceptual processing.34 , 35 the refixation count is how many times an aoi is returned to and shows transitions between different areas . 
more refixations and transitions may indicate inefficient search.36 although it is well understood that these trends are task specific , our results work to bridge this theoretical understanding of eye movement data to the processing of mdx reports . 
 strongly agree agree disagree strongly disagree strongly agree agree disagree strongly disagree laboratory a laboratory b laboratory c laboratory a laboratory b laboratory c laboratory a laboratory b laboratory c laboratory a laboratory b laboratory c strongly agree agree disagree strongly disagree strongly agree agree disagree strongly disagree fig 2 . 
it is easy to find the therapy class ( such as us food and drug administration approved off - label , on - label , clinical trials ) in this patient report . 
it is easy for you to decide on a treatment of this patient on the basis of this report . were 29 instances when participants looked at lack of benefit after clinical trials . think - aloud protocol and video analysis the data supplement summarizes the verbal feedback received from clinicians from the thinkaloud protocol transcription and video analysis . 
think - aloud and video analysis helped gain insight into improvements needed in the mdx reports and helps confirm the survey and eye - movement data . discussion molecular diagnostic reports try to distill the results of genetic tests with therapy and clinical trial options into a single - page summary to help overburdened oncologists make appropriate treatment decisions for their patients . 
perception and comprehension of information are two processes important to understanding.37 what we perceive ( visually through our eyes as captured by the eye tracker ) and how we comprehend it ( captured by our think aloud ) are two necessary components to understanding and fundamental to the usability evaluation . 
the survey showed that all the participants agreed with s2 ( it is easy to find the therapeutic implications [ benefit , lack of benefit ] in this patient report ) , but a participant said , under the indeterminate benefit , i do not know what those mean . 
detailed descriptions of the aois are in the data supplement . abbreviations : aoi , area of interest ; mdx , molecular diagnostic . clinicians were voicing about certain content , their eyes were fixated on a different section , perhaps indicating where their comprehension was heading next . 
hence , we noticed it was important to summarize results from both techniques and call out areas where results from one technique validated those from the other method . the eye - movement analysis ( tables 2 and 3 ) shows that participants fixated most in regions that described therapy options . 
however , each laboratory had a different approach to this information ( data supplement ) , and there were clear differences in how laboratories presented and clinicians responded to the presentation . 
however , for s3 ( it is easy to find the therapy class , such as fda approved off - label , on - label , and clinical trials ) , the majority disagreed , and the larger number of eye fixations and refixations in the therapy sections suggests more cognitive difficulty in interpretation . 
 laboratory a laboratory b laboratory c potential benefit genomic alteration ranked therapy transition count transition count transition count clinical trials lack of benefit results summary therapy genomic findings potential benefit clinical trials lack of benefit genomic alteration results therapy ranked therapy summary genomic findings fig 3 . 
in the laboratory b report , there were 26 instances when participants looked at results after genomic alteration , and in the laboratory c report , there were 19 instances when participants looked at summary after ranked therapy . 
for laboratory c , the majority agreed with s2 , that therapeutic implications were easy to find , but by the same margins they disagreed with s3 , that it is easy to find the therapy class.... 
 unfortunately , participants found this system confusing , as indicated in several comments in the think - aloud transcripts and suggestions . the genomic anomaly results were of high interest as measured by fixations and refixations to the aois , think - aloud comments , and s5 suggestions . 
laboratory a , for s1 ( is it easy to find the molecular anomalies ) did the worst , with half the participants agreeing and half disagreeing with comments about the lack of detail . 
laboratory a did not have a section specific to genomic anomalies ; it only showed gene symbols in the therapy sections and not the actual variants detected , implying that there were anomalies in the gene . 
laboratory cs anomalies section had lower fixation counts , fixation duration , and refixations than laboratory b , suggesting the display was more clear and efficient . how can these results be applied to design improved mdx summary reports ? some simple suggestions include the following : diagnosis should be clearly labeled at or near top of a report . 
 reports should try to work in grayscale and not be too reliant on color , because reports are still often faxed , and approximately 4% to 8% of the population is colorblind.38 genomic anomalies should be clearly labeled with some detail ( laboratory c did best in this area )  . 
therapy sections are the most important and need to distinctly relate anomalies to therapies , with a clear delineation between fda - approved , national comprehensive cancer network guideline , and experimental treatments and appropriate clinical trials . 
a ranking system to summarize complex clinical information on the basis of standardization of clinical evidence seems to be needed ( laboratory c included a ranking , but it was not clear to the participants )  . our current understanding of the science of interpreting variants and treatment options is in flux , and any ranking system would need to be understandable , flexible , and adapt quickly as our knowledge of actionable variants evolves . 
 ( p12 ) this is most of the information that i would care about . ( p01 ) under ranked therapy , i am not really sure what it means when it says molecular profile and there is a number there . 
 ( p15 ) the biggest advantage of this is , its actually making a clear - cut recommendation for oncologists who does not know how to interpret these results ( p13 ) i dont see what mutations the patient has . 
 ( p05 ) they are not really showing the molecular anomalies , just tells you the therapies that they are recommending , ( .. ) so i can infer that braf is negative because they are saying braf has lack of benefit . 
average duration indicates average fixation duration . abbreviations : aoi , area of interest ; fda , us food and drug administration ; nccn , national comprehensive cancer network ; p , physician . are beginning to revise their reports and present additional evidence on request from clinicians who ordered these tests . the sex difference is an unfortunate limitation ; however , it is not uncommon in human factor studies . 
many studies use three to five participants , which provides saturation when looking at specific usability and cognitive aspects of a display or product , and no additional data collection or analysis is necessary after saturation has been attained.31 , 39 recruiting busy expert participants is an ongoing challenge for clinical usability studies . 
 than the other laboratory reports , this study showed numerous issues with presentation of information in laboratory as report indicating that bias , if present , was not a large issue . 
the participants expressed great interest in optimizing the information presented to them to augment their day - to - day clinical work , indicating a clear need for improvement in mdx reports to support decision making . these findings revealed that participants prefer mdx reports with clear therapeutic implications supported by biomarker implications . 
a summary on a tablet or a web site dashboard with options for additional details on trials , drugs , or implicated biomarkers might be the personalized medicine coalition conducted a nationwide survey and found that although most people had not heard about personalized medicine , those who did , or had it explained , were excited about the potential benefits.40 similar usability studies with patients will benefit laboratories that are beginning to generate patient - targeted reports to improve patient understanding of treatment options and enable informed discussions with their clinicians . 
efforts such as sync for science41 and blue button42 allow individuals to access their health data to support the goals of the precision medicine initiative and allow individuals to have control over their personal health information . 
beckman employment : onco - mind stock and other ownership interests : johnson & johnson consulting or advisory role : astrazeneca ; emd serono patents , royalties , other intellectual property : two patents for dynamic precision medicine , a novel approach to precision medicine , have been granted in japan and taiwan and transferred to onco - mind . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . vishakha sharma no relationship to disclose allan fong no relationship to disclose simina m . 
1u01hg008390 - 01 , 2015 - 2016 . presented in part at the american medical informatics association translational summits , san francisco , ca , march 27 - 30 , 2017 , and american society for clinical pharmacology & therapeutics annual meeting , washington , dc , march 21 - 24 , 2018 . support prior presentation references 1 . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
madhavan s : barriers to implementation of precision medicine for cancer treatment in the us healthcare systejournal of precision medicine may / june : 48 - 56 , 2016 8 . 
ratwani rm , fairbanks rj , hettinger az , et al : electronic health record usability : analysis of the user - centered design processes of eleven electronic health record vendors . 
clark ln , guarrera tk , mcgeorge nm , et al : usability evaluation and assessment of a novel emergency department it system developed using a cognitive systems engineering approach . proceedings of the international symposium on human factors and ergonomics in health care 3 : 76 - 80 , 2014 14 . 
fonda sj , paulsen ca , perkins j , et al : usability test of an internet - based informatics tool for diabetes care providers : the comprehensive diabetes management progradiabetes technol ther 10 : 16 - 24 , 2008 21 . 
kushniruk aw , triola mm , borycki em , et al : technology induced error and usability : the relationship between usability problems and prescription errors when using a handheld application . 
sasaki t , kato y , sato a , et al : a questionnaire survey of pharmacists regarding the clinical practice guidelines for the appropriate use of granulocyte - colony stimulating factors . 
phillips p , boone d , mallett s , et al : method for tracking eye gaze during interpretation of endoluminal 3d ct colonography : technical description and proposed metrics for analysis . 
helbren e , halligan s , phillips p , et al : towards a framework for analysis of eye - tracking studies in the three dimensional environment : a study of visual search by experienced readers of endoluminal ct colonography . 
irwin de : fixation location and fixation duration as indices of cognitive processing , in henderson jm , ferriera f ( eds ) : the interface of language , vision , and action : eye movements and the visual world . 
in this study , metex14 ( c.2899g.a ) was detected by targeted next - generation sequencing with memorial sloan kettering integrated mutation proling of actionable cancer targets ( msk - impact ) in a case of advanced lung adenocarcinoma driven by egfr l858r mutation , after 12.5 months of frontline egfrtyrosine kinase inhibitor ( tki ) treatment . 
interestingly , metex14 co - occurred with met amplication and egfr t790m at the time of progression , as revealed by digital polymerase chain reaction on cell - free dna ( but not conrmed on tumor tissue )  . 
earlier , we described a patient whose primary resection sample tested positive for both egfr l858r and metex14 ( c3028 + 1g.t ) , but not for met amplication , as assessed by next - generation sequencing.2 in the current study , although the patient did not respond to met - targeted therapy alone , a combination of crizotinib ( met - tki ) and osimertinib ( third - generation egfr - tki ) led to durable disease control.1 however , we believe that additional key points should be discussed in more detail . 
targeted sequencing did not assess unknown potential mechanisms of resistance . it would have been interesting to learn which other pathways were abnormally activated in this tumor , such as fas or components of the nf - b pathway that specically enhanced cell death induced by rstgeneration egfr - tki erlotinib and caused acquired resistance to third - generation egfr - tki rociletinib in egfr - mutant lung cancer cells.3 , 4 met amplication should be further investigated . 
two recent studies reported a response to a combination of osimertinib and crizotinib in patients with nonsmallcell lung cancer ( nsclc ) harboring egfr l858r , while a rebiopsy showed met amplication after disease progression on erlotinib.5 , 6 similarly , a dramatic response was achieved using crizotinib and erlotinib in a case of met amplication emerging in the setting of egfr l858r mutation , suggesting the potential role of erlotinib and crizotinib combination , 5 which was not tested in vitro . 
in this model , crizotinib monotherapy was unable to modulate cell growth and switch off the egfr downstream signaling . although the drugs were used at a low concentration and no analysis was performed to assess pharmacointeractions , 7 crizotinib restored sensitivity to logical osimertinib in both pc9 and h1975 metex14 models . mechanistically , it was shown that the combination inhibited activation of egfr , met , as well as downstream akt and erk.1 these ndings underline the effectiveness of different tki combinations in inhibition of multiple signaling cascades to overcome cancer cell resistance.8 in particular , met signaling plays a crucial role in driving egfr - tki resistance in oncogene - addicted nsclc , and met inhibition can be a successful strategy to recover sensitivity in cases of met aberrations . 
despite the striking clinical activity of the combination in the current study , there is often a large gap between preclinical evaluations of tki combinations and clinical outcome.9 thus , the identication of predictive biomarkers for response could be useful for proper selection of patients who would likely benet from the therapeutic combination . 
we recently identied p - her3 and p - pras40 as potential candidates to assess the synergy between erlotinib and crizotinib in vitro.10 erlotinib and crizotinib showed remarkable synergy in the ludlu squamous - cell lung cancer ( scc ) cell line , which does not harbor egfrsensitizing mutations , met amplication , or metex14 . interestingly , other investigated scc cell lines ( h1703 and skmes - 1 ) , which were also wild - type for egfr and met , reacted differently ( but still additive ) , suggesting a role for the differential expression of p - her3 and p - pras40 expression in this synergy . 
because we observed a synergistic effect of the combination treatment of erlotinib and crizotinib only in scc cells that showed concordant expression of p - her3 and p - pras40 , we assume that p - her3 and p - pras40 may be candidate biomarkers for effective egfr + met blockade in patients with scc.10 taking into account our ndings , other components of the egfr and met pathways , including p - her3 and p - pras40 , should be investigated in tissues obtained from patients receiving a combination of egfr - tki and met - tki . in conclusion , we are indebted to suzawa et al1 for their elegant study . 
 correspondence alessandro leonetti , md amsterdam umc , vu university medical center , cancer center amsterdam , amsterdam , the netherlands , and university hospital of parma , parma , italy marcello tiseo , md , phd university hospital of parma and university of parma , parma , italy christian rolfo , md , phd , mba university of maryland greenebaum comprehensive cancer center , baltimore , md nele van der steen , phd amsterdam umc , vu university medical center , cancer center amsterdam , amsterdam , the netherlands , and center for oncological research ( core ) , university of antwerp , wilrijk , belgium godefridus j . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . marcello tiseo consulting or advisory role : astrazeneca , bristol - myers squibb , msd , boehringer ingelheim , takeda research funding : astrazeneca christian rolfo consulting or advisory role : mylan speakers bureau : novartis , msd , boehringer ingelheim , guardant health travel , accommodations , expenses : astrazeneca godefridus j . 
peters consulting or advisory role : taiho pharmaceutical , clear creek bio , ellipses pharma research funding : rexahn pharmaceuticals ( inst ) travel , accommodations , expenses : rexahn pharmaceuticals , taiho pharmaceutical no other potential conicts of interest were reported . references suzawa k , ofn m , schoenfeld aj , et al : acquired met exon 14 alteration drives secondary resistance to epidermal growth factor receptor tyrosine kinase inhibitor in egfr - mutated lung cancer . 
clin lung cancer 19 : 35 - 41 , 2018 bivona tg , hieronymus h , parker j , et al : fas and nf - b signalling modulate dependence of lung cancers on mutant egfr . 
nature 471 : 523 - 526 , 2011 galvani e , sun j , leon lg , et al : nf - b drives acquired resistance to a novel mutant - selective egfr inhibitor . 
oncotarget 6 : 42717 - 42732 , 2015 giroux - leprieur e , dumenil c , chinet t : combination of crizotinib and osimertinib or erlotinib might overcome met - mediated resistance to egfr tyrosine kinase inhibitor in egfr - mutated adenocarcinoma . 
j thorac oncol 13 : e232 - e234 , 2018 zhu vw , schrock ab , ali sm , et al : differential response to a combination of full - dose osimertinib and crizotinib in a patient with egfr - mutant nonlung cancer and emergent met amplication . 
lung cancer small cell ( auckl ) 10 : 21 - 26 , 2019 bijnsdorp iv , giovannetti e , peters gj : analysis of drug interactions . methods mol biol 731 : 421 - 434 , 2011 tong cws , wu wkk , loong hhf , et al : drug combination approach to overcome resistance to egfr tyrosine kinase inhibitors in lung cancer . cancer lett 405 : 100 - 110 , 2017 yang z , tam ky : combination strategies using egfr - tki in nsclc therapy : learning from the gap between pre - clinical results and clinical outcomes . 
van der steen n , leonetti a , keller k , et al : decrease in phospho - pras40 plays a role in the synergy between erlotinib and crizotinib in an egfr and cmet wild - type squamous non - small cell lung cancer cell line . 
 next - generation sequencing reveals potentially actionable alterations in the majority of patients with lymphoid malignancies purpose next - generation sequencing ( ngs ) identifies potentially targetable alterations by us food and drug administration ( fda ) approved drugs and / or by available experimental agents that may not have otherwise been contemplated . 
many targeted drugs have been developed for diverse solid cancers ; a smaller number of genomically targeted drugs have been approved for lymphoid malignancies . materials and methods we analyzed ngs results from 60 patients with various lymphoid malignancies and found 224 alterations ( median per patient , three alterations )  . results forty - nine patients ( 82% ) had potentially actionable alterations with the use of fdaapproved drugs and / or experimental therapies ; only 11 patients ( 18% ) had no theoretically actionable alterations . 
only three patients ( 5% ) had an alteration for which an approved drug in the disease is available ( on label ) ; 45 patients ( 75% ) had an alteration for which an approved drug is available for another disease ( off label )  . 
of note , 19 ( 32% ) of 60 patients had intermediate to high tumor mutational burden , which may predict response to certain immunotherapy agents . conclusion ngs identifies alterations that may be pharmacologically tractable in most patients with lymphoid malignancies , albeit with drugs that have usually been developed in the context of solid tumors . 
goodman michael choi matthew wieduwilt carolyn mulroney caitlin costello garrett frampton vincent miller razelle kurzrock author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : aaron m . 
goodman , md , moores cancer center , university of california san diego , 3855 health science dr , la jolla , ca 92093 ; e - mail : a1goodman@ucsd.edu. introduction the lymphoid malignancies have diverse biologic and clinical behavior and typically are treated with multiagent chemotherapy . 
many therapeutic regimens for b - cell non - hodgkin lymphomas and leukemias also incorporate the anti - cd20 monoclonal antibody rituximab , which has improved patient outcomes.1 treatment of metastatic solid tumors , like lymphoid malignancies , has also relied heavily on the use of cytotoxic chemotherapy . however , over the past decade , the treatment paradigm for metastatic solid tumors has shifted away from chemotherapy toward matching oncogenic driver mutations with targeted therapy ( precision medicine ) .2 - 4 for example , in patients with braf - mutated metastatic melanoma , the braf inhibitor vemurafenib markedly increases overall survival compared with chemotherapy.5 numerous targeted therapies are now approved by the us food and drug administration ( fda ) for patients with metastatic solid tumors across a wide array of histologies ( data supplement )  . 
the first example of targeted therapeutic efficacy is the hematologic disorder chronic myelogenous leukemia , which has been transformed by the use of agents that affect bcr - abl kinase activity . despite the rapid success in development , approval , and use of small - moleculetargeted agents in patients with solid malignancies , a paucity of such therapies approved for use in lymphoid malignancies remains ( data supplement )  . 
 small - moleculetargeted therapeutics are not an available option . the rapid technological advances in nextgeneration sequencing ( ngs ) have allowed oncologists to sequence tumor exomes in a clinically meaningful period of time.6 - 8 some studies have shown that patients with solid malignancies treated with matched therapy have improved outcomes , 9 and meta - analyses in approximately 85 , 000 patients have supported this finding.10 - 12 the targeting of alterations such as braf can result in responses across a wide variety of cancers , including lymphoid malignancies ( eg , hairy cell leukemia ) .13 , 14 although not all malignancies that harbor braf mutations will respond equally well to braf inhibition , the strategy of crosscancer basket trials has been established as highly worthwhile . ngs accurately identifies substitutions , indels , copy number alterations , and gene fusions in hematologic malignancies.15 in this report , we use this technology to analyze the genomic alterations in a cohort of 60 patients with various lymphoid malignancies to estimate the frequency of theoretically actionable alterations . 
this study was performed and consents obtained in accordance with university of california san diego institutional review board guidelines . tumor samples from tissue ( table 1 ) or peripheral blood were collected from 60 patients and submitted for ngs to foundation medicine , a laboratory improvement amendments clinical certified laboratory for ngs . 
the foundationone heme panel was used , which is a hybrid capturebased ngs test.16 the methods used in this assay have been described in detail in previous reports.7 , 15 the foundationone heme assay simultaneously detects all genomic alterations , including base pair substitutions , indels , copy number alterations , and select gene rearrangements , in 405 cancer - related genes . 
for tumor mutational burden ( tmb ) , the number of somatic mutations detected on ngs are quantified , and that value was extrapolated to the whole exome by using a validated algorithm described in detail in earlier publications.17 , 18 alterations with known and likely effects on functional status are not counted . definition of actionable alteration an alteration was defined as potentially actionable if its protein product is a component of a molecularly defined pathway for which there is at least one available fda - approved drug or investigational drug that may affect the function of the protein product of the alteration or the immediate downstream effectors of the protein product or that differentially recognizes the protein in tumor versus normal cells . 
the protein products of genomic alterations were considered to be functional the genomic alterations have been previously identified as relevant to cancer in the cosmic database , 19 which catalogs recurrent somatic alterations in cancer . 
novel base substitution , indel , and rearrangement alterations that result in truncations and homozygous copy number deletions that occur in tumor suppressor genes were considered to have likely functional implications . 
novel genomic alterations that occur at the same position as known alterations as well as alterations with conflicting evidence with regard to implication for function were subject to review by an internal panel of subject matter experts to determine functional status of the relevant protein product on the basis of all available evidence , including , but not limited to , the exac , dbsnp , and clinvar databases.20 - 22 data and statistical analyses patient characteristics were obtained through electronic medical record review . 
descriptive statistics were used , including medians , ranges , and frequencies . results patient characteristics sixty patients ( 35 men [ 58% ] and 25 women [ 42% ] ) with lymphoid malignancies were identified ( table 1 )  . 
the most common malignancy in the cohort was chronic lymphocytic leukemia ( cll ; 32% ) , followed by acute lymphoblastic leukemia ( all ; 20% ) , multiple myeloma ( 18% ) , diffuse large b - cell lymphoma ( dlbcl ; 10% ) , follicular lymphoma ( 8% ) , and other lymphoid neoplasms ( 5% )  . 
however , the actual alteration in nras differed between the two patients ( nras g13d v nras q61r )  . the median number of alterations detected per patient was three ( range , zero to 14 )  . 
as demonstrated in figure 1b , seven patients ( 12% ) had no reportable alterations , 10 ( 17% ) had one alteration , and 43 ( 71% ) had two or more alterations . 
the maximum number of alterations identified was 14 , which was observed in two patients ( 3% ) , one with cll , the other with dlbcl . of note , all patients with dlbcl had five or more alterations . actionable alterations potentially actionable alterations were identified in all disease subtypes ( table 2 )  . 
all disease subtypes , except marginal zone lymphoma , had alterations targetable by fda - approved drugs . forty - nine patients ( 82% ) had potentially actionable alterations with fda - approved drugs and / or experimental therapies ( clinical trials ) , whereas 11 patients ( 18% ) had no theoretically actionable alterations . depicted in figure 2 is the number of patients with potentially fda actionable alterations per disease group . 
only three patients had an alteration for which an approved drug in the disease is available ( on label ) , whereas 45 patients ( 75% ) had an alteration for which an approved drug is available in another disease ( off label )  . 
eleven patients had no targetable alterations ; these patients included seven with no detected genomic alterations . two patients with b - cell all ( b - all ) and one with waldenstr om macroglobulinemia had alterations targetable with on - labelapproved drugs ( fig 3 )  . 
high tmb was seen in five patients ( 8% ) , intermediate in 14 ( 23% ) , and low in 40 ( 67% )  . tmb was not available for one patient ( 2% )  . intermediate to high tmb was noted across almost all histologies ( except for marginal zone lymphoma , natural killer / t - cell lymphoma , and cutaneous t - cell lymphoma )  . 
three patients with multiple myeloma had an intermediate level of tmb . discussion this study demonstrates that in the majority of patients ( 82% ) with lymphoid malignancies whose disease was interrogated by ngs , alterations were found that might be pharmacologically tractable , a percentage similar to the 77% reported by he et al15 for diverse hematologic malignancies . 
another study reported that 70% of patients with various solid tumors had an alteration that was theoretically actionable with an approved drug.24 this finding is similar for lymphoid malignancies , with 75% of the current study patients having an alteration potentially actionable by an approved drug . 
table 3 lists therapeutics with their corresponding targets that were identified in the patient cohort . one of the major obstacles to performing comprehensive genomic profiling of clinical specimens is the necessity for an adequate tumor sample . 
unlike solid malignancies where invasive biopsy is almost always required to obtain a tissue sample , comprehensive genomic profiling of lymphoid malignancies often can be performed with the use of peripheral blood and / or bone marrow . in this cohort , 54% of patients had specimens obtained from blood and / or bone marrow . tumors can acquire new mutations as they progress , which underscores the importance of obtaining new tissue when available for sequencing at the time of therapeutic decision making . 
 other not actionable , 2 mm not actionable , 2 other actionable , actionable , actionable , cll not actionable , fl not actionable , 2 actionable , 3 actionable , dlbcl actionable , fig 2 . 
in one study , 42% of patients did not have metastatic disease at the time of their biopsy.24 lymphoid malignancies are more amenable to repeat biopsy , with more than one half of the current cohort having tissue available from the blood and / or bone marrow . 
this accessibility facilitates repeat ngs to guide therapy . over the past decade , 26 orally administered targeted therapies have been fda approved for the treatment of 13 different solid malignancies ( data supplement )  . 
over the same period , only five orally administered targeted therapies have been approved for the treatment of lymphoid malignancies ( philadelphia chromosomepositive all , cll , follicular lymphoma , mantle cell lymphoma , and waldenstr om macroglobulinemia )  . the current data demonstrate that 45 patients ( 75% ) had an alteration that theoretically could have been targeted with an approved , albeit offlabel , drug , whereas only three patients ( 5% ) had an alteration for which an approved on - label drug was available . 
in a similar study in patients with solid malignancies , 20% had an alteration targeted by on - label agents , whereas 67% had an alteration targetable by off - label use.24 ( of note , the study used the same definitions for actionability as were used in this analysis . ) currently , a paucity of orally administered targeted therapy is available for onlabel use in lymphoid malignancies . 
however , as our findings suggest , the majority of cases likely will have potentially targetable alterations . the mutational landscape for numerous lymphomas has now been well characterized by several whole - exome sequencing studies.46 , 47 for example , mll2 , crebbp , and tp53 alterations in dlbcl , as described by pasqualucci et al , 46 were some of the most common recurrent mutations in the current cohort of patients with dlbcl . 
this alteration was also the most common ( 12% ) in a cohort of patients with cll sequenced by puente et al.47 furthermore , 82% of our patients had alterations that were pharmacologically tractable , similar to the 77% reported by he et al15 in diverse hematologic malignancies . 
these similar findings in other cohorts provide further support of the generalizability of our findings to other large cohorts of lymphoid malignancies . myd88 , an adapter protein used by toll - like receptors , was shown to be mutated ( myd88 l265p ) in  . 
90% of patients with waldenstr om macroglobulinemia ( lymphoplasmacytic lymphoma ) .48 this mutation not only is relatively specific for the disease but also predicts clinical presentation and survival.49 myd88 signaling is important in lymphomagenesis and signals through btk.50 in a phase ii trial , ibrutinib produced an overall response rate of 91% in a group of previously treated patients with waldenstr om macroglobulinemia , which led to its fda approval.37 furthermore , response rates to ibrutinib were significantly higher in patients with myd88 mutations versus wild - type myd88.51 in the current cohort , myd88 l265p mutation was found in the one patient with waldenstr om macroglobulinemia . 
however , myd88 alterations were also identified in one patient with dlbcl ( myd88 l265p ) , one with follicular lymphoma ( myd88 s219c ) , and one with primary cns lymphoma ( myd88 l265p )  . 
myd88 mutations have been discerned in marginal zone b - cell lymphoma , 52 cll , 53 dlbcl , 54 and primary cns lymphoma.55 preliminary data from a phase i trial of single - agent ibrutnib in four patients with cns lymphoma demonstrated responses in two of the three patients evaluated . 
in a phase i trial of 17 patients with relapsed mantle cell lymphoma treated with single - agent palbociclib , five ( 18% ) achieved progression - free survival of  . 
1 year , with one complete and two partial responses.58 the high percentage of cdkn2a / b alterations in the current study population gives further rationale for designing trials with cdk inhibitors in lymphoid malignancies . activating mutations in braf were found in three patients with cll ( two with braf g469a and one with braf v600e ) and one patient with multiple myeloma ( braf v600e )  . 
these mutations are potentially targetable by the braf inhibitors vemurafenib and dabrafenib and the mek inhibitors trametinib and cobimetinib.5 , 27 braf alterations have been identified as a driver mutation and as a biomarker for sensitivity to braf inhibition in both hairy cell leukemia and erdheim - chester disease.59 - 61 braf alterations have been found in approximately 3% of patients with cll.62 in the current study , two patients had mutations that led to an alanine substitution for a glycine at position 469 . 
ngs readily identified philadelphia chromosomelike b - all and can assist in selecting patients for clinical trials of targeted agents aimed at improving the poor outcome of these patients.15 higher neoantigen burden , which may be largely predicted by tmb , has been associated with higher objective response rates and progressionin patients treated with pd - 1 free survival blockade.67 , 68 melanoma , lung cancer , and renal cell carcinoma , all of which are highly responsive to pd - 1 blockade , have been shown to have a high degree of mutational burden from wholegenome and - exome sequencing studies.69 in the current cohort , tmb ranged from one or fewer to 140 ( data supplement )  . 
intermediate to high tmb was noted across almost all histologies ( except for marginal zone lymphoma , natural killer / t - cell lymphoma , and cutaneous t - cell lymphoma )  . 
the majority of the patients had cll , multiple myeloma , and all , whereas other nonhodgkin lymphomas were less well represented . although the majority of patients had actionable mutations theoretically targeted by fda - approved drugs , in practice , insurance approval for off - label drug use often is difficult to obtain.73 in addition , no standard definition exists for a targetable alteration , and the level of evidence needed to support this is a matter of debate . 
the number of actionable alterations discussed in this article may be overestimated , but even so , these patients should still be directed toward clinical trials that target these alterations so that the responsiveness or lack thereof can be determined . 
numerous additional clinical trials with a standardized definition of what constitutes a targetable alteration are needed to determine the extent to which patients respond when an alteration is theoretically druggable . 
currently , a number of such trials are ongoing ( clinicaltrials.gov identifiers nct02534675 , nct00851032 , and nct02465060 )  . in conclusion , we found that most patients with lymphoid malignancies have unique and complex molecular portfolios . 
goodman administrative support : caitlin costello , razelle kurzrock provision of study materials or patients : michael choi , matthew wieduwilt , carolyn mulroney , caitlin costello collection and assembly of data : aaron m . 
 novartis , merck , roche / genetech , genentech mypath , foundation medicine , pfizer , guardant health , merck serono patents , royalties , other intellectual property : four patents travel , accommodations , expenses : win , emd serono , gateway research advisory committee , icrp , win 2015 , caris centers of excellence , aacr , association of american cancer institutes , emd serono & quintiles , global biomarkers consortium , guardant health , global source ventures / novena therapeutics , ascpt , meyers consulting , fda - ocra , genentech , orbimed / global source ventures , sylvester cancer center , journal of precision medicine , curematch , lynx group , mayo clinic cancer center , kaiser permanente , pancan , cedars - sinai , medimmune / jk associates medical communications group affiliations aaron m . 
sehn lh , donaldson j , chhanabhai m , et al : introduction of combined chop plus rituximab therapy dramatically improved outcome of diffuse large b - cell lymphoma in british columbia . 
helsten t , kato s , schwaederle m , et al : cell - cycle gene alterations in 4 , 864 tumors analyzed by next - generation sequencing : implications for targeted therapeutics . 
wheler j , lee jj , kurzrock r : unique molecular landscapes in cancer : implications for individualized , curated drug clin can res 22 : 5497 - 5505 , 2016 mutation . 
nat biotechnol 31 : 1023 - 1031 , 2013 janku f , wheler jj , naing a , et al : pik3ca mutation h1047r is associated with response to pi3k / akt / mtor signaling pathway inhibitors in early - phase clinical trials . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
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he j , abdel - wahab o , nahas mk , et al : integrated genomic dna / rna profiling of hematologic malignancies in the n engl j med 373 : 726 - 736 , 2015 clinical setting . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
spigel dr , schrock ab , fabrizio d , et al : total mutation burden ( tmb ) in lung cancer ( lc ) and relationship with response to pd - 1 / pd - l1 targeted therapies . 
samadder nj , neklason dw , boucher km , et al : effect of sulindac and erlotinib vs placebo on duodenal neoplasia in familial adenomatous polyposis : a randomized clinical trial . 
robert c , karaszewska b , schachter j , et al : improved overall survival in melanoma with combined dabrafenib and n engl j med 374 : 311 - 322 , 2016 trametinib . 
emadi a , faramand r , carter - cooper b , et al : presence of isocitrate dehydrogenase mutations may predict clinical response to hypomethylating agents in patients with acute myeloid leukemia . 
furumoto y , gadina m : the arrival of jak inhibitors : advancing the treatment of immune and hematologic disopin investig drugs 21 : 637 - 655 , 2012 orders . 
infante jr , fecher la , falchook gs , et al : safety , pharmacokinetic , pharmacodynamic , and efficacy data for the oral mek inhibitor trametinib : a phase 1 dose - escalation trial . 
migden mr , guminski a , gutzmer r , et al : treatment with two different doses of sonidegib in patients with locally advanced or metastatic basal cell carcinoma ( bolt ) : a multicentre , randomised , double - blind phase 2 trial . 
said r , hong ds , warneke cl , et al : p53 mutations in advanced cancers : clinical characteristics , outcomes , and correlation between progression - free survival and bevacizumab - containing therapy . 
schwaederle m , lazar v , validire p , et al : vegf - a expression correlates with tp53 mutations in non - small cell lung cancer : implications for anti - angiogenesis therapy . 
koehler k , liebner d , chen jl : tp53 mutational status is predictive of pazopanib response in advanced sarcomas . ann oncol 27 : 539 - 543 , 2016 44 . 
von bubnoff n , schneller f , peschel c , et al : bcr - abl gene mutations in relation to clinical resistance of philadelphia - chromosome - positive leukaemia to sti571 : a prospective study . 
treon sp , cao y , xu l , et al : somatic mutations in myd88 and cxcr4 are determinants of clinical presentation and overall survival in waldenstr om macroglobulinemia . 
finn rs , crown jp , lang i , et al : the cyclin - dependent kinase 4 / 6 inhibitor palbociclib in combination with letrozole versus letrozole alone as first - line treatment of oestrogen receptor - positive , her2 - negative , advanced breast cancer ( paloma - 1 / trio - 18 ) : a randomised phase 2 study . 
nadeu f , delgado j , royo c , et al : clinical impact of clonal and subclonal tp53 , sf3b1 , birc3 , notch1 , and atm mutations in chronic lymphocytic leukemia . 
woyach ja , furman rr , liu t - m , et al : resistance mechanisms for the brutons tyrosine kinase inhibitor ibrutinib . n engl j med 370 : 2286 - 2294 , 2014 66 . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
from march to december 2015 , a local oncology practice administered 10 cycles of the recommended systemic chemotherapy with liposomal pegylated doxorubicin ( 30 to 35 mg / m2 once every 28 days ) , which resulted in complete disappearance of cutaneous lesions . 
at this time , the sarcoma lesions were markedly progressive and caused deep ulcerations that led to constant bleeding and a massively increased need for potent analgesics ( fig 1 )  . 
under this treatment , ulcerations worsened and the patient required red blood cell transfusions once per week because of the continuous bleeding from his sarcomatous lesions ( fig 1 )  . a histopathologic re - examination of the biopsy taken at recurrence revealed expression of programmed death - ligand 1 ( pd - l1 ) on sarcoma cells in 10% of the sections ( fig 2 ) by using the pd - l1 ihc 22c3 pharmdx assay ( dako agilent , waldbronn , germany ) and the monoclonal 28 - 8 antibody ( abcam , cambridge , uk ; staining on dako omnis platform , waldbronn , germany )  . 
of note , the tumor showed a high level of immune cell infiltrates with formation of lymph follicles and germinal centers as well as focal infiltration of cd8 + t cells ( fig 2 )  . 
after five cycles of pembrolizumab , a very good clinical response of all sarcoma lesions was observed , and the patient required rainer hamacher dietrich kmpfe kirsten reuter - jessen christoph pttgen lars e . 
clinical macroscopic course during pembrolizumab treatment course of preauricular and submandibular tumor on the left side and preauricular tumor on the right side before at baseline ( october and november 2016 ) , after five cycles ( march 2017 ) , and after 10 cycles ( august 2017 ) of treatment with 2 mg / kg pembrolizumab in a 3 - week cycle . no more analgesics ( fig 1 )  . 
 moreover , the patient experienced a marked with cas in the head and neck region , those occurrences represent less than 0.15% of all head and neck malignancies.2 , 3 the incidence is highest in elderly white patients with a mean age of 73 years , and there is no difference between sexes.2 , 4 aside from sporadic occurrences , long - standing lymphedema and prior radiation pd - l1 pd - l1 pd - l1 fig 2 . 
three representative photos of immunohistochemical stainings with anti - pd - l1 ( on the left ) and one photo with anti - cd8 ( on the right ) of the re - examined local recurrence of the lesion obtained between 2014 and 2016 . 
 disease followed by salvage surgery of local recurrence.6 , 7 after progression , he received a standard sequence of palliative systemic therapies , 7 - 9 and he exhibited good but transient responses . 
subsequent treatments for his highly symptomatic disease , chosen on the basis of prior reports of clinical activity , 10 - 14 were poorly tolerated or showed no efficacy . overall , patients with cas have a poor prognosis with a high local recurrence rate and 5 - year survival of only 30%.1 , 4 for cas of the scalp , the median overall survival ranges from 6 to 24 months with a 2 - year survival rate of less than 15% in patients with advanced disease.15 although lung metastases are frequent , patients quality of life is often massively compromised by local recurrence with highly mutilating , ulcerating , and disfiguring lesions . 
the interaction of pd - 1 ( a receptor on t cells ) and its ligands ( pd - l1 and pd - l2 ) on target cells is one dominant immune checkpoint pathway that represses cytotoxic immune response . 
whereas the physiologic function of pd - l1 is controlling immune homeostasis , upregulation of pd - l1 by cancer cells and cells of the microenvironment has been described as a mechanism of immune escape.16 , 17 development of monoclonal antibodies blocking either pd - 1 ( such as pembrolizumab or nivolumab ) or pd - l1 ( such as atezolizumab , durvalumab , or avelumab ) have opened novel treatment approaches that show improved overall survival in several cancers , including melanoma , non - small - cell lung cancers ( nsclcs ) , and renal cell cancer ; the list of additional susceptible cancer entities is expanding rapidly.16 , 17 soft tissue sarcomas are not yet in the immunotherapy spotlight , and there is a surprisingly low number of clinical trials , most of which studied cellular therapies that target tumor antigens or sarcoma - specific gene products from oncogenic transcripts.18 - 20 nevertheless , several fusion studies found evidence that sarcomas suppress immune response and have also discovered additional characteristics that provide a rationale for immune checkpoint blockade.18 , 20 , 21 preliminary results of the recent sarc028 phase ii trial reported early responses on pembrolizumab in undifferentiated pleomorphic sarcoma and in a low number of osteosarcoma , liposarcoma , and high - grade or dedifferentiated chondrosarcoma.22 in contrast , ipilimumab , a monoclonal antibody targeting ctla - 4 ( which has been approved for immunotherapy of melanoma ) , showed little activity in a group of 17 adolescent patients with sarcoma.23 numerous studies investigating the role of immunotherapy in soft tissue sarcoma are currently ongoing , but many exclude rare subtypes such as angiosarcoma . predictive biomarkers for icis have not yet been identified in rare tumor types . 
studies in other cancer types ( eg , ncslc ) indicate that intratumoral pd - l1 expression , lymphoid infiltration , and mutational burden are associated with improved therapeutic response.17 two recent retrospective studies reported expression of pd - l1 in 30% to 40% of patients with cas and found an inverse correlation between prognosis and expression levels of pd - l1 and infiltrating t cells.24 , 25 we observed expression of pd - l1 in our patient in 10% of the sarcoma cells in his recurrent lesion ( fig 2 )  . 
notably , a patient with cas who had similar intratumoral pd - l1 expression more than 5% has recently been reported with response to pembrolizumab.26 in addition to pd - l1 expression , we observed a high rate of tumor - infiltrating immune cells , notably with the formation of intratumoral lymph follicles and infiltration by cd8 + cells ( fig 2 )  . 
although single patients preclude making any sort of generalization , the relatively high level of pd - l1 expression could serve as one explanation for the response , especially in light of the generally low pd - l1 expression rates found in sarcomas.22 the recent sarc study used a cutoff of 1% pd - l1 expression resulting in 4% positive tumors when using this threshold in this cohort.22 this cutoff is useful in nsclc , in which pd - l1 positivity of more than 1% is associated with a higher overall response rate.17 , 27 , 28 moreover , we observed an infiltration with lymphoid cells and the presence of lymph follicles , which could be a consequence of chronic inflammation resulting from the ulceration but may also indicate that the tumor has elicited an immune response , which might be useful to explore in a larger cohort of patients . 
 interestingly , other studies indicate sensitivity to immunotherapy of other kinds of skin malignancy beyond melanoma , such as basal cell , cutaneous squamous cell , and merkel cell carcinoma , that is associated with high exposure to ultraviolet light.29 , 30 given the devastating consequences and the limitations of currently available treatments , we believe the unusual response in our report and in one other case report26 strongly warrants further studies in cas . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . rainer hamacher travel , accommodations , expenses : eli lilly , pharmamar , novartis dietrich kmpfe no relationship to disclose kirsten reuter - jessen honoraria : zytovision , ah diagnostics travel , accommodations , expenses : zytovision , ah diagnistics , astrazeneca honoraria : roche pharma ag , boehringer ingelheim speakers bureau : roche pharma ag , boehringer ingelheim christoph pttgen no relationship to disclose lars e . 
dill , md , for providing paraffin blocks of the patients tumor , and the members of the bauer and schildhaus laboratory for expert technical assistance , helpful discussions , and critical reading . 
podleska , farhad farzaliyev , and hans - ulrich steinau , university hospital essen , university duisburg - essen ; martin schuler and sebastian bauer , german cancer consortium , partner site university hospital essen , essen ; dietrich kmpfe , hematology and oncology practice , ldenscheid ; and kirsten reuter - jessen and hans - ulrich schildhaus , university hospital gttingen , gttingen , germany . support supported by sarkomtour ( s.b. ) references 39 : 258 - 263 , 2015 1 . 
albores - saavedra j , schwartz am , henson de , et al : cutaneous angiosarcoma : analysis of 434 cases from the surveillance , epidemiology , and end results program , 1973 - 2007 . 
schlemmer m , reichardt p , verweij j , et al : paclitaxel in patients with advanced angiosarcomas of soft tissue : a retrospective study of the eortc soft tissue and bone sarcoma group . 
kollr a , jones rl , stacchiotti s , et al : pazopanib in advanced vascular sarcomas : an eortc soft tissue and bone sarcoma group ( stbsg ) retrospective analysis . 
le cesne a , ray - coquard i , duffaud f , et al : trabectedin in patients with advanced soft tissue sarcoma : a retrospective national analysis of the french sarcoma group . 
kim jr , moon yj , kwon ks , et al : tumor infiltrating pd1 - positive lymphocytes and the expression of pd - l1 predict poor prognosis of soft tissue sarcomas . 
tawbi ha , burgess m , bolejack v , et al : pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
honda y , otsuka a , ono s , et al : infiltration of pd - 1 - positive cells in combination with tumor site pd - l1 expression is a positive prognostic factor in cutaneous angiosarcoma . 
gandini s , massi d , mandal m : pd - l1 expression in cancer patients receiving anti pd - 1 / pdl1 antibodies : a systematic review and meta - analysis . 
dmmr / microsatellite high ( msi - h ) breast cancers were among the responding tumors that led to the recent us food and drug administration accelerated approval of pembrolizumab for any patient with a dmmr / msi - h metastatic solid tumor.2 the authors conclude that they would like to make a case for msi testing in patients with metastatic cancer beyond typical lynch - associated cancers.1 i also propose the study of whether patients now identified with dmmr breast cancers might harbor germline mismatch repair ( mmr ) - mutated genes and , therefore , would be molecularly defined as lynch syndrome family members . the us food and drug administration accelerated approval and suggestion by kok et al represent an opportunity to clarify whether breast cancer should be considered a lynch - associated cancer . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . steven sorscher honoraria : celgene , pfizer , puma biotechnology speakers bureau : celgene , pfizer , puma biotechnology travel , accommodations , expenses : celgene , pfizer , puma biotechnology 1 . 
dinardo , md1 introduction germline predispositions to hematologic malignancies in adult patients presenting with a diagnosis of myelodysplastic syndrome ( mds ) or acute myeloid leukemia ( aml ) are commonly underestimated . 
through next - generation sequencing ( ngs ) , many genes involved in hereditary mds or aml are now evaluated , including runx1 , cebpa , gata2 , tp53 , etv6 , and ddx41.1 , 2 germline gata2 mutations are a common cause for predisposition to mds or aml.3 patients with gata2 deciency can have manifestations ranging from mild cytopenias to life - threatening infections and myeloid neoplasia . 
the incidence of gata2 deciency is still unknown ; however , gata2 mutations may account for approximately 75% of adolescent patients with monosomy 7 mds.4 approximately 20% to 30% of gata2 mutations are inherited in an autosomal dominant fashion , whereas others are sporadic or de novo mutations.5 because molecular testing for mds and aml has become more commonplace , we recognize that some clinicians may incorrectly equate a negative ngs panel as ruling out any potential inherited malignancy predisposition . 
in addition , promoter mutations ( ie , ankrd26 ) and intronic mutations ( ie gata2 ) may often be missed if the ngs panel is restricted to exonic sequences . 
specic testing for fanconi anemia and dyskeratosis congenita when clinically indicated should be performed , for example , diepoxybutane or mitomycin cinduced chromosomal breakage assay and telomere length owuorescence in situ hybridization analysis , respectively . 
publically available registries and genomic data sets such as clinvar and gnomad are increasingly useful to provide insight into clinical signicance of identied variants . here , we report on two patients with a history of immunodeciency and myeloid neoplasia . 
1 is a 24 - year - old hispanic man who presented for evaluation of pancytopenia , mainly leukopenia associated with recurrent extensive warts on bilateral hands and recurrent panniculitis . 
his blood counts were as follows : white blood cell count , 3.2 109 / l ; hemoglobin , 14.1 g / dl ; and platelet count , 186 109 / l . 
concurrent ow cytometry analysis demonstrated a small population of aberrant myeloblasts , lack of hematogones , virtual absence of monocytes , and markedly reduced natural killer ( nk ) cells . 
a peripheral blood sample was obtained for ow cytometry study that showed no monocytes , nk cell lymphopenia ( 0.4% of lymphocyte gate ; fig 1b ) , and decreased b cells ( 3.8% of lymphocyte gate )  . 
a targeted exome sequence analysis of the following genes was performed on cultured skin broblasts : ankrd26 , cebpa , ddx41 , etv6 , gata2 , runx1 , srp72 , terc , tert , and tp53 . 
her blood counts showed a white blood cell count of 2.9 109 / l , with 75% neutrophils , 21% lymphocytes , 1% monocytes , hemoglobin of 10.1 g / dl , and platelet count of 164 109 / l . 
her past medical history was unremarkable , and her family history was negative for any immunologic or hematologic diseases . because of persistent ebv viremia , she received autologous ebv - specic cytotoxic t - lymphocyte cells . 
she received intensive cytarabine - based chemotherapy , and her induction course was complicated by an infection with mycobacterium fortuituflow cytometry analysis showed that she achieved complete remission with negative minimal residual disease . 
before proceeding with allogeneic hematopoietic stem - cell transplantation ( hsct ) from her sibling , the patient was referred to our hereditary hematologic malignancy clinic.6 a skin biopsy was performed for cultured skin broblasts , and genetic testing demonstrated a heterozygous deletion that included at least exon 2 of the gata2 gene . 
top : prehsct , the bone marrow shows a near absence of monocytes on ( left ) cd45 / ssc and ( middle ) cd14 ( thick arrows ) ; ( right ) no stage i or stage ii hematogones or mature b cells ( thin arrows )  . 
this variant has been previously reported in at least 29 other patients.4 , 10 - 14 the gata2 mutation detected in patient no . 2 was a large deletion involving at least exon 2 . 
to our knowledge , this is the rst time this specic deletion has been reported , although other in - frame or full gene gata2 deletions have been described.4 , 15 gata2 deciency can have various clinical presentations.11 , 16 patient no.1 presented initially with dermatologic problems , including extragenital warts and recurrent severe panniculitis ; mild cytopenias and hypocellular mds occurred later in his disease course . 
laboratory ndings include monocytopenia , dendritic cell cytopenias , b and nk lymphocytopenia , relative increase in t cells with an inverted cd4 : cd8 ratio , lack of hematogones , and various degrees of dysplasia.13 bm cellularity may vary from hypocellular marrow with severe cytopenias to normoor hypercellular marrow . 
 abou dalle et al stem cell exhaustion.3 the median age at diagnosis of 380 younger patients was approximately 20 years ( range , 12 to 35 years ) , with a high risk of progression to aml in 75% of carriers . 
complex cytogenetics and del ( 5q ) were not usually observed.5 patients with immunodeciency and recurrent infections along with a new diagnosis of mds at a younger age should be screened for an underlying germline mutation . 
genetic testing for germline mutations should sequence the most common genes responsible for familial predisposition to mds or aml , including ankrd26 , cebpa , ddx41 , etv6 , gata2 , runx1 , srp72 , samd9 , samd9l , terc , tert , and tp53 using nonhematopoietic tissue , usually cultured skin broblasts . gata2 sequencing should involve deletion and duplication analysis and intron 5 of the gata2 gene to detect all possible pathogenic variants . 
dinardo , md , department of leukemia , the university of texas md anderson cancer center , 1515 holcombe blvd , unit 0428 , houston , tx 77030 ; e - mail : cdinardo@mdanderson.org. support supported in part by specialized programs of research excellence grant no . 
cortes consulting or advisory role : bristol - myers squibb , biolinerx , novartis , pzer , amphivena therapeutics , daiichi sankyo , bio - path holdings , astellas pharma , takeda pharmaceuticals research funding : bristol - myers squibb ( inst ) , novartis ( inst ) , pzer ( inst ) , celgene ( inst ) , arog pharmaceuticals ( inst ) , astellas pharma ( inst ) , ambit biosciences ( inst ) , celator pharmaceuticals ( inst ) , immunogen ( inst ) , sun pharmaceutical industries ( inst ) , takeda pharmaceuticals ( inst ) alessandra ferrajoli research funding : celgene , genentech , acerta pharma dimitrios p . 
kontoyiannis employment : md anderson cancer center honoraria : gilead sciences , astellas pharma , t2 biosystems , mylan consulting or advisory role : merck , astellas pharma , fast track to growth , pzer , astellas pharma sa a . 
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kazenwadel j , secker ga , liu yj , et al : loss - of - function germline gata2 mutations in patients with mds / aml or monomac syndrome and primary lymphedema reveal a key role for gata2 in the lymphatic vasculature . 
we demonstrated previously that pemetrexed - based chemotherapy can achieve an objective response rate of 45% and a median progression - free survival ( pfs ) of 19 months.3 furthermore , the activity of targeted therapy has improved dramatically with the introduction of selective ret inhibitors to the clinic . 
in early - phase testing , objective response rates with loxo - 2924 and blu - 6675 are 68% ( 26 of 38 ) and 50% ( seven of 14 ) , respectively . 
these outcomes exceed the modest activity observed previously with multikinase inhibitors such as cabozantinib6 and vandetanib.7 in contrast , the activity of immunotherapy in retrearranged lung cancers has not been well characterized . 
this represents a clear unmet need , given that all prior regulatory approvals of immune checkpoint inhibitors , either alone or in combination with chemotherapy , and in stage iii or iv disease , have technically included patients with ret - rearranged lung cancers.8 , 9 furthermore , although increasing levels of programmed death - ligand 1 ( pd - l1 ) expression and high tumor mutational burden ( tmb ) have been associated with benet from immune checkpoint blockade , 10 the immunophenotype of ret - rearranged lung cancers and the role of pd - l1 and tmb status in relation to benet with immunotherapy remain poorly described . 
we set out to characterize these factors . methods in this retrospective study , patients from memorial sloan kettering cancer center with ret - rearranged lung cancers diagnosed between 2009 and 2017 were identied under an institutional review board approved waiver . 
patients who received immunotherapy , dened as a monoclonal antibody against programmed cell death protein 1 ( pd - 1 ) or pd - l1 , were included in an analysis of treatment history . ret rearrangements were identied using targeted next - generation sequencing of dna ( memorial sloan ketteringintegrated mutation proling of actionable cancer targets [ msk - impact ] or foundation one ) or rna ( anchored multiplex polymerase chain reaction [ pcr ] ; memorial sloan kettering solid fusion panel ) in more contemporary samples , and uorescence in situ hybridization ( 10q11 and 6q22 break apart probe , reversemetasystems , altussheim , germany ) or transcriptase pcr in older samples.11 , 12 pd - l1 immunohistochemistry was evaluated using the e1l3n antibody ( cell signaling technology , danvers , ma ) , our institutional standard , which has been validated against a 22c3 kit performed in a commercial laboratory with comparable results.13 for uniformity , tmb ( reported as the number of nonsynonymous mutations per megabase ) was analyzed only for samples sequenced using msk - impact.14 , 15 the median tmb of ret - rearranged was compared with that of ret wildtype nsclcs ( mann - whitney u test )  . in patients with both baseline and serial on - treatment imaging , the best objective response to therapy ( response evaluation criteria in solid tumors [ recist ] v1.1 ) was determined by a study radiologist . 
time to treatment discontinuation ( ttd ) was dened as the time from therapy initiation to the last dose.16 pfs was dened as the time from therapy initiation to radiologic progression or death . 
ret rearrangement was identied as follows : dna - based next - generation sequencing ( 80% [ n = 59 ] ) , rnabased anchored multiplex pcr ( 1% [ n = 1 ] ) , uorescence in situ hybridization ( 15% [ n = 11 ] ) , and reverse - transcriptase pcr ( 4% [ n = 3 ] )  . 
clinicopathologic features of ret - rearranged lung cancers : summary of demographics and tumor molecular features of 74 patients with ret - rearranged lung cancers feature all patients ( n = 74 ) age , years median range sex , no . 
in 44 patients with sufcient tissue for tmb analysis , the median tmb was 1.75 mutations / mb ( range , 0 to 9.65 mutations / mb ) , signicantly lower ( p , .0001 ) than the median tmb of 5.27 mutations / mb ( range , 0 to 164.20 mutations / mb ) in 3 , 631 patients with ret wild - type nsclcs ( fig 1b )  . the clinical outcomes of immunotherapy in patients with advanced ret - rearranged lung cancers are summarized in table 2 . 
 ( a ) the programmed death - ligand 1 ( pd - l1 ) expression ( e1l3n , cell signaling ) of 26 ret - rearranged lung cancers with sufcient tissue for testing is shown . 
 ( b ) the tumor mutational burden ( tmb ) of 44 ret - rearranged lung cancers is displayed ( left ) relative to the tmb of 3 , 631 ret wild - type lung cancers ( right )  . 
for ease of representation , three outlier ret wild - type lung cancer samples with tmb greater than 75 mutations / mb that were included in the statistical analysis were excluded in this plot . nivolumab ( n = 6 ) , atezolizumab ( n = 2 ) , durvalumab ( n = 1 ) , or ipilimumab plus nivolumab ( n = 1 )  . 
dashes represent tumor samples in which tissue was insufcient for pd - l1 or tmb testing . abbreviations : cr , complete response ; pd , progressive disease ; pd - l1 , programmed death - ligand 1 ; pfs , progression - free survival ; sd , stable disease ; non - cr / non - pd , not cr and not pd in nontarget lesions ; tmb , tumor mutational burden . * treatment discontinued for toxicity . a total of 13 patients with ret - rearranged lung cancers were assessed for clinical and / or radiologic response . response to immunotherapy was not observed . 
progression of disease was observed in 62% of cases ( n = eight of 13 ; table 2 ) ; disease progression involved new or worsening brain metastases in three patients ( cases 4 , 6 , and 15 )  . 
stable disease was achieved in 23% ( three of 13 ) and non - cr / non - pd ( not complete reponse and not progressive disease in nontarget lesions ) in 15% ( two of 13 )  . 
 ret - rearranged nsclc : immunophenotype and immunotherapy response these ndings are consistent with a growing body of evidence uncovering poor outcomes with immune checkpoint inhibition in select oncogene - addicted lung in egfr - mutant and alk - rearranged lung cancers . cancers , early data on the decreased activity ( compared with unselected cancers ) of immunotherapy resulted in the exclusion of patients with these tumors in registrationenabling studies . 
furthermore , we showed previously that met exon 14altered nsclcs had low tmb and poor outcomes with immunotherapy.17 finally , an ongoing global registry ( immunotarget ) and independent series have shown similarly low response rates and short median pfs with single - agent immune checkpoint inhibition in lung cancers with oncogenic drivers.18 immunotarget had 16 patients in the ret - rearranged cohort and reported a response rate of 6% and median pfs of 2.1 months , comparable to the ndings in our study . the clinical implications of these observations relate to the sequence with which immunotherapy is used and the type of immunotherapy strategy selected . 
regarding the former , it is becoming increasingly clear that specic , targeted therapies ( selective ret inhibitors ) 2 , 4 , 19 and chemotherapy agents ( pemetrexed - containing regimens ) 3 can achieve superior outcomes compared with immunotherapy in this series . 
thus , is reasonable to consider the use of checkpoint inhibition only after select targeted therapies and platinum doublet - containing chemotherapy have been administered . note that high pd - l1 expression ( 50% or more ) was uncommon in ret - rearranged lung cancers in this study . only one case treated with immunotherapy highly expressed pd - l1 ( 50% ) and , despite this , still responded poorly to dual immune checkpoint inhibitor therapy ( case 16 )  . 
a recommendation regarding the use of pembrolizumab in treatment - nave , advanced ret - rearranged lung cancers with high pd - l1 expression cannot be made on the basis of our ndings , although its use should be approached with caution . 
in met exon 14altered lung cancers , tmb is similarly low ; although a higher proportion of tumors have high pd - l1 expression , this was not associated with increased benet with single - agent immunotherapy.17 finally , no patients in this series received the combination chemotherapy and immunotherapy that is currently approved for the treatment of egfr and alk wild - type advanced nsclc . 
prospective trials of immunotherapy combinations should incorporate comprehensive molecular proling to establish prospective data in driver - positive subpopulations of patients . in summary , most ret - rearranged lung cancers have low pd - l1 expression and low tmb , and response to immunotherapy was not observed in this series . 
although this study is limited by a small sample size , given the rarity of ret - rearranged nsclcs , these ndings remain meaningful and support evolving literature showing that outcomes with immune checkpoint inhibition are poor in select oncogene - addicted nsclcs . 
contributed equally to this work . support supported in part by the national cancer institute of the national institutes of health ( t32 ca009207 , p30 ca008748 )  . provision of study material or patients : gregory j . 
rudin consulting or advisory role : bristol - myers squibb , abbvie , seattle genetics , harpoon therapeutics , genentech / roche , astrazeneca , ascentage pharma , bicycle therapeutics , celgene , daiichi sankyo , ipsen , loxo , pharmamar , elucida oncology research funding : abbvie / stemcentrx ( inst ) , viralytics ( inst ) , merck ( inst ) , daiichi sankyo ( inst ) gregory j . 
riely research funding : novartis ( inst ) , roche / genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pzer ( inst ) , innity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) , mirati therapeutics ( inst ) , merck ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : merck sharp & dohme matthew d . 
hellmann stock and other ownership interests : shattuck labs honoraria : astrazeneca , bristol - myers squibb consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca / medimmune , novartis , janssen pharmaceuticals , nektar , syndax pharmaceuticals , mirati therapeutics , shattuck labs research funding : bristol - myers squibb ( inst ) patents , royalties , other intellectual property : a patent has been led by memorial sloan kettering ( pct / us2015 / 062208 ) for the use of tumor mutation burden for prediction of immunotherapy efcacy , and which is licensed to personal genome diagnostics ( inst ) travel , accommodations , expenses : astrazeneca , bristol - myers squibb maria arcila honoraria : invivoscribe consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe , raindance technologies mark g . 
li consulting or advisory role : roche , biosceptre international , thermo fisher scientic , mersana , guardant health , hengrui therapeutics research funding : roche / genentech ( inst ) , illumina ( inst ) , biomed valley discoveries ( inst ) , astrazeneca ( inst ) , grail ( inst ) , daiichi sankyo ( inst ) , hengrui therapeutics ( inst ) , guardant health ( inst ) marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso request for proposal advisory committee , takeda pharmaceuticals , bristol - myers squibb , bayer ag , merck ( i ) research funding : loxo ( inst ) , helsinn therapeutics alexander drilon honoraria : medscape , onclive , peervoice , physicians education resources , targeted oncology , more health , research to practice , foundation medicine , peerview consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pzer , blueprint medicines , genentech / roche , helsinn therapeutics , beigene , hengrui therapeutics , exelixis , bayer ag , tyra biosciences , verastem , takeda pharmaceuticals / ariad pharmaceuticals / millenium pharmaceuticals , bergenbio , more health patents , royalties , other intellectual property : wolters kluwer ( royalties for pocket oncology ) other relationship : merck , glaxosmithkline , teva pharmaceuticals industries , taiho pharmaceutical no other potential conicts of interest were reported . references stransky n , cerami e , schalm s , et al : the landscape of kinase fusions in cancer . 
nat commun 5 : 4846 , 2014 drilon a , hu zi , lai ggy , et al : targeting ret - driven cancers : lessons from evolving preclinical and clinical landscapes . 
nat rev clin oncol 15 : 151 - 167 , 2018 drilon a , bergagnini i , delasos l , et al : clinical outcomes with pemetrexed - based systemic therapies in ret - rearranged lung cancers . 
ann oncol 27 : 1286 - 1291 , 2016 oxnard gr , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer : an update from asco 2018 . 
toronto , canada , september 23 - 26 , 2018 subbiah v , taylor m , lin j , et al : abstract ct043 : highly potent and selective ret inhibitor , blu - 667 , achieves proof of concept in a phase i study of advanced , ret - altered solid tumors . 
drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 2 , single - arm trial . 
lancet oncol 17 : 1653 - 1660 , 2016 lee sh , lee jk , ahn mj , et al : vandetanib in pretreated patients with advanced non - small cell lung cancer - harboring ret rearrangement : a phase ii clinical trial . 
ann oncol 28 : 292 - 297 , 2017 gandhi l , rodrguez - abreu d , gadgeel s , et al : pembrolizumab plus chemotherapy in metastatic non - small - cell lung cancer . 
n engl j med 378 : 2078 - 2092 , 2018 reck m , rodrguez - abreu d , robinson ag , et al : pembrolizumab versus chemotherapy for pd - l1 - positive non - small - cell 375 : 1823 - 1833 , 2016 lung cancer . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
rizvi h , sanchez - vega f , la k , et al : molecular determinants of response to anti - programmed cell death ( pd ) - 1 and anti - programmed death - ligand 1 ( pd - l1 ) blockade in patients with non - small - cell lung cancer proled with targeted next - generation sequencing . 
ofn m , rizvi h , tenet m , et al : tumor mutation burden and efcacy of egfr - tyrosine kinase inhibitors in patients with egfr - mutant lung cancers . 
sabari jk , leonardi gc , shu ca , et al : pd - l1 expression , tumor mutational burden , and response to immunotherapy in patients with met exon 14 altered lung 18 . 
mazieres j , drilon ae , mhanna l , et al : efcacy of immune - checkpoint inhibitors ( ici ) in non - small cell lung cancer ( nsclc ) patients harboring activating molecular alterations ( immunotarget )  . 
 ofn et al immunotherapy naive ( n = 46 ) immunotherapy administered ( n = 16 ) log - rank p = .35 time since metastasis diagnosis ( years ) no . 
overall survival from the diagnosis of metastatic disease was compared between patients who received an immune checkpoint inhibitor ( n = 16 ) and those who did not ( n = 46 )  . 
 genetic testing and clinical management practices for variants in non - brca1 / 2 breast ( and breast / ovarian ) cancer susceptibility genes : an international survey by the evidence - based network for the interpretation of germline mutant alleles ( enigma ) clinical working group sarah m . 
domchek ros eeles anna efremidis ( continued ) purpose to describe a snapshot of international genetic testing practices , specifically regarding the use of multigene panels , for hereditary breast / ovarian cancers . 
we conducted a survey through the evidence - based network for the interpretation of germline mutant alleles ( enigma ) consortium , covering questions about 16 non - brca1 / 2 genes . methods data were collected via in - person and paper / electronic surveys . 
additional information was collected via country networks in the united kingdom and in italy . results responses from 61 cancer genetics practices across 20 countries showed that 16 genes were tested by > 50% of the centers , but only six ( palb2 , tp53 , pten , chek2 , atm , and brip1 ) were tested regularly . 
us centers tested the genes most often , whereas united kingdom and italian centers with no direct enigma affiliation at the time of the survey were the least likely to regularly test the most centers tested the 16 genes through multigene panels ; some centers tested tp53 , pten , and other cancer syndromeassociated genes individually . 
gene - specific guidelines for breast and ovarian cancer risk management were limited and differed among countries , especially with regard to starting age and type of imaging and risk - reducing surgery recommendations . conclusion currently , a small number of genes beyond brca1 / 2 are routinely analyzed worldwide , and management guidelines are limited and largely based on expert opinion . 
pedersen maria piane marianna puzzo mark robson maria rossing maria christina sini angela solano jana soukupova gianluca tedaldi manuel teixeira mads thomassen maria grazia tibiletti amanda toland therese trngren erica vaccari liliana varesco ana vega yvonne wallis barbara wappenschmidt jeffrey weitzel amanda b . 
currently , several multigene panels are available that include from < 10 to > 100 known or candidate cancer susceptibility genes , which are tested for diagnostic or research purposes . 
some panels are targeted at diverse cancers ( pan - cancer panels ) , whereas others target specific cancers only ( disease specific panels )  . the ability to run multigene panels at affordable prices has expanded the eligibility criteria and increased the demand for testing.1 - 5 however , the rapid pace at which candidate risk genes are moving from research based to clinical diagnostic testing has its drawbacks . 
the rate of variants of uncertain significance ( vus ) has increased proportionally to the extent of the sequenced genome.5 - 7 moreover , many genes currently included on multigene panels have imprecise cancer risk estimates , and there is no consensus on when to test for a given gene or how to manage a reported ( likely ) pathogenic variant.8 , 9 the aim of this study was to describe a snapshot of the landscape of international genetic testing practices and risk management approaches for bc and boc susceptibility genes beyond brca1 and brca2 . 
a survey was conducted among members of the evidence - based network for the interpretation of germline mutant alleles ( enigma ) , an international consortium focused on determining the clinical significance of variants in brca1 , brca2 , and other ( ascertained or suspected ) bc and boc susceptibility genes , providing expertise to global database and classification initiatives , and exploring optimal avenues of communication of such information at the provider and patient levels . 
additional information was collected via country networks in the united kingdom and in italy , from centers that were not directly involved in enigma research at the time of study initiation . in total , respondents represented cancer genetic experts from 61 centers across 20 countries . 
 to our knowledge , this is the first study to describe international testing practices and risk management guidelines for non - brca1 / 2 genes implicated in bc and boc susceptibility . methods this study was submitted for approval to the ethics committees of the two coordinating sites , the university of chicago and maastricht university . 
a survey about genetic testing practices for nonbrca1 / 2 bc and boc susceptibility genes was developed by enigma clinical working group ( cwg ) leaders during 2016 ( appendix table a1 )  . 
enigma members were invited to complete the survey if they had a clinical genetic testing or diagnostic laboratory affiliation and were involved in ordering , performing , or interpreting dna tests for inherited susceptibility to bc / boc at their center . 
an enigma member is currently defined as a researcher or research group ( consortium ) who is willing to work collaboratively toward classification of variants by contributing data from families and / or conducting statistical analysis or laboratory - based assays within a working group framework . 
there is no requirement for enigma members to state their primary role ( clinician , genetic counselor , laboratory scientist , basic researcher ) , but all members by definition have a research interest in the topic of gene / variant classification . individuals from the same center could work on the survey together or choose a designated representative to complete it , so only one survey per center was counted . 
in brief , an in - person survey of members of the cwg , consisting mainly of laboratory and clinical scientists from academic centers , was conducted during the enigma consortium meeting in limassol , cyprus , in january 2017 . 
 a total of 30 centers from 17 countries participated . a more detailed version of the survey was then distributed by e - mail ( paper / electronic survey ) to the same 30 centers that participated in the in - person survey and to additional enigma affiliated centers worldwide . 
participants were sent a copy of their answers and asked to verify them or to clarify any discrepancies . notably , in italy and in the united kingdom , the paper / electronic version of the survey was also distributed , via country networks , to centers that were not actively involved in enigma research . 
the effort comprised both the enigma - affiliated fondazione istituto di ricovero e cura a carattere scientifico istituto nazionale dei tumori ( milan ) and the santa chiara university hospital ( pisa ) , which were counted among the 38 participating enigma centers , and 14 additional centers , which were not directly affiliated with enigma at the time of the survey ( henceforth referred to as non - enigma ; fig 1 , lower right )  . 
of the 14 italian non - enigma centers , five were dedicated to diagnostic testing only , and nine were dedicated to both diagnostics and research ; moreover , half of them were university affiliated , and half were not . 
 completed the survey for her own enigma affiliated center ( one of the 38 participating enigma centers ) and also coordinated , with the assistance of y.w. , the distribution of the survey through surveymonkey via the association for clinical genetic science mailing list to cancer genetic leads from diagnostic laboratories providing genetic testing for the publicly funded national health service ( nhs )  . 
the recruitment flowchart and the global distribution of participants are illustrated in figure 1 . clinical utility to get a preliminary idea of the participants opinions about the clinical utility of the 16 genes on which the survey focused , the cwg members present at the 2017 enigma meeting in cyprus were asked to answer the following questions relating to each of them : should every patient with bc / oc who qualifies for ( brca1 / 2 ) genetic testing ( by criteria that we recognize may differ by country / center ) be tested for the gene ? and do you agree that the cancer risk associated with ( pathogenic variants in ) the gene is high enough to inform clinical management ? all participants ( n = 23 at this specific session ) stated that they would test every qualifying patient with bc ( as defined in the question ) for palb2 and every qualifying patient with oc ( as defined ) for brip1 , rad51c , and rad51d . 
results for the other nine genes were variable ( appendix fig a1a )  . with regard to clinical management , all participants agreed that palb2 , tp53 , cdh1 , pten , and stk11 along with brip1 , rad51c , and rad51d were associated with high enough ( bc or oc ) risk to alter clinical management . 
please note that 95% cis for this figure and for all the following figures are provided in appendix ( tables a2 - a10 )  . testing practices participants were also asked ( via in - person and / or paper / electronic surveys ) if and how frequently they tested each gene , the method ( single gene v gene panel ) and purpose of testing ( clinical v research ) , and the practices of reporting ( likely ) pathogenic variants and vus to patients . 
of centers that responded to the question varied by gene ( range , 29 to 38 centers ) .regularly was defined as ordered for > 50% of eligible patients ( ie , those who qualified for genetic testing , by criteria that we recognize may differ by center / country )  . 
even though each gene was tested by > 50% of the centers ( range , 52% to 100% ) , only palb2 , tp53 , pten , chek2 , atm , and brip1 were tested regularly by > 50% of centers . testing in a research setting in addition to the clinical setting was common for enigma centers ( appendix fig a2 )  . 
the genes that were most frequently tested ( ie , tested by at least > 30% of centers ) for research purposes only were : nbn , bard1 , rad50 , and mre11a . 
 single - gene testing was performed by a number of centers , varying from one to 21 , for : tp53 , pten , cdh1 , stk11 , palb2 , chek2 , nf1 , atm , men1 , and nbn ( in decreasing order of frequency ) , often based on a specific phenotype ( eg , pten hamartoma syndrome or neurofibromatosis type 1 ) , or these genes were tested as a reflex only when brca1 / 2 testing was noninformative . 
seven centers from four countries ( belgium , brazil , the netherlands , and spain ) testing chek2 only tested for the 1100delc variant . regarding the types of gene panels used , us respondents typically ordered broad cancer panels from commercial laboratories , although the specific panels varied depending on patient preferences , insurance considerations , and clinical scenarios . 
separately , the nine united kingdom nhs laboratories were asked , if you currently only report brca genes but might report broader panels in the future , what issues are major barriers / problems to overcome ? responses were chosen from a menu of nine options plus other , and the four main reasons selected ( by half or more of respondents ) were no request by the oncologists ( of note , nhs oncologists can ask directly for brca1 and brca2 testing but not for multigene panels ) , lengthy and laborious process of variant interpretation , lack of standardization of reporting , and lack of demand for testing . reporting practices and cascade testing . 
for genes analyzed through clinical testing , > 90% of enigma centers reported ( likely ) pathogenic variants to patients ( for chek2 and nbn , the percentages were slightly lower , at 88% and 71% , respectively ; fig 4 )  . 
some centers reported these variants only if the patient met criteria for the associated syndrome ( eg , hereditary diffuse gastric cancer for cdh1 , neurofibromatosis type 1 for nf1 )  . 
almost all centers ( 67% to 81% for nbn , rad50 , mre11a , and bard1 and > 90% for the other genes ) offered cascade testing to family members if a ( likely ) pathogenic variant was identified ( data not shown )  . 
notably , participants from the netherlands reported that they only tested first - degree relatives for chek2 1100delc variant when the estimated risk based on family history was lower than the risk conferred by having the variant , so testing for the variant had clinical utility because it would change surveillance recommendations.11 a high percentage ( 50% to 82% ) of enigma centers reported vus to patients ( fig 4 )  . 
 variant classification systems all respondents reported using the international agency for research on cancer five - tier classification system , 12 and many also used american college of medical genetics and genomics13 classification criteria . 
 the three methods are not mutually exclusive ; notably , the center in kuwait performs whole - genome sequencing for all cases , which is not represented in the figure . 
enigma , evidence - based network for the interpretation of germline mutant alleles . clinical management practices and guidelines most enigma centers ( 80% ) had risk management guidelines for a majority of non - brca1 / 2 genes considered reportable to patients ( fig 5 )  . 
 exceptions were bard1 , rad50 , and mre11a , for which 30% of centers had guidelines . although most enigma centers reported having some type of management guidelines for all genes except bard1 , rad50 , and mre11a , after review , only 10 of 20 countries had national guidelines for ( some of ) these genes ( table 1 )  . 
 furthermore , in some countries ( denmark and germany ) , the national guidelines were not gene specific ( ie , they were broken down by highand moderate - risk categories rather than by specific gene )  . 
ten countries had national guidelines for high - risk cancer syndromeassociated genes such as tp53 , cdh1 , and pten ( with the exception of belgium not having guidelines for cdh1 )  . 
the primary differences between countries were the starting age and type of diagnostic imaging ( mammography v magnetic resonance imaging [ mri ] v sonography ) and the policy on risk - reducing mastectomy . 
for instance , there was no consensus on the age to begin mammograms / mri for carriers of pathogenic variants in nf1 , men1 , palb2 ( age 25 v 30 years ) , or tp53 ( age 20 v 25 years )  . 
 the united kingdom guidelines differed from all others in that breast mri was not the standard imaging technique for carriers of pathogenic variants in other gene carriers ( except for tp53 )  . 
guidelines for risk - reducing mastectomy in carriers of palb2 pathogenic variants ranged among accepted ( n = 1 ) , consider depending on personal / family history ( n = 5 ) , and not enough evidence to recommend ( n = 1 )  . 
for pten and cdh1 , the guidelines that commented on preventive surgery ( four of the seven and five of the eight national guidelines , respectively ) mentioned risk - reducing mastectomy as a possible option . 
 subanalyses : enigma - us versus enigma - other centers and versus non - enigma centers discussion responses from the seven enigma centers in the united states ( enigma - us ) were compared with those of the other 31 enigma centers ( enigma - other )  . 
in addition , responses from 14 non - enigma centers in italy and nine non - enigma laboratories in the united kingdom were compared with those from 38 enigma centers across all countries . results of these comparisons are summarized in appendix figs a3 and a4 . 
a much smaller proportion of non - enigma centers from italy and the united kingdom tested each gene compared with enigma - affiliated centers ( appendix fig a3 )  . management guidelines were more likely to be available in the us - based enigma centers compared with the other enigma centers for all genes except bard1 , rad50 , mre11a , and men1 . 
of centers that responded varied by gene ( range , 12 to 36 centers responding about reporting pathogenic variants ; range , four to 20 centers responding about reporting vus )  . 
our global survey demonstrated that only a few genes are routinely analyzed beyond brca1 / 2 ; most centers clinically test them through multigene panels and report ( likely ) pathogenic variants ( and vus , to a slightly lesser extent ) to patients ; and gene - specific guidelines for bc and oc risk management are limited and differ between countries , especially in regard to starting age and type of imaging and risk - reducing surgery recommendations . with falling costs of sequencing and more genes being identified that are associated with increased bc and boc risk , multigene ( panel ) testing is becoming the northe results of our survey confirm this trend , showing that genes that are commonly offered on commercial panels were tested by > 50% of the surveyed centers . nevertheless , the value of multigene panel testing continues to be debated in the context of three main areas : limited additional yield of pathogenic variants in genes other than brca1 / 2 coupled with significantly increased interpretation workload , reliability of penetrance estimates for moderateor uncertain risk genes ( clinical validity ) , and evidence for informing management recommendations to improve patient outcomes ( clinical utility ) .9 our international survey demonstrates that the use of panel testing varies widely among countries . 
moreover , differences were observed when comparing enigma - affiliated centers with non - enigma italian and united kingdom centers ( with the latter testing nonbrca1 / 2 genes less than one third of the time )  . 
if management guidelines were available , centers were asked to specify the source of such guidelines ( local , national , or international , such as national comprehensive cancer network or national institute for health and care excellence )  . the genes included on panels was the most common concern raised by the participating centers . 
easton et al8 asserted that a genomic test should not be offered until its clinical validity is established8 ( p2 ) ; however , the utility of a gene needs to be continuously reconsidered as more data become available , and this can only be done by analyzing results from large cohorts of individuals who have been tested . 
concerns about the rates of vus were frequently expressed by the study participants , but just as variant rates have significantly decreased over the years for brca1 / 2 as a result of concerted classification efforts , the same trend will likely occur for other susceptibility genes , arguably at a faster pace as ( and provided that ) more laboratories worldwide contribute their testing data to population and peer - reviewed databases.5 , 28 , 29 despite the establishment of such databases , survey participants felt that robust , constantly updated international databases and global data sharing are still lacking . 
this is a worthy goal , but expert judgment in variant classification methods is still required , because fully automated approaches to variant classification that apply guidelines are not ready for clinical practice.6 at a basic level , some centers reported validation of the testing method as a barrier . 
therefore , it is important to recognize the technologic barriers in certain countries , although the transition to massively parallel sequencing is ultimately expected to increase throughput and optimize diagnosis without significantly elevating costs.30 there were also nonmedical barriers to implementing routine testing of many of these surveyed genes . 
insurance can be a major barrier in the united states , where , for example , medicare ( a us federal health insurance program for people who are age 65 years and for certain younger people with disabilities ) will only cover testing for individuals with a bc or oc diagnosis , and many insurers will not cover multigene panel testing if the patient has already had prior genetic testing . 
in many other countries , particularly those with national ( ie , universal ) health care , testing is approved on a gene - by - gene basis or as a package if research - derived evidence is considered robust enough to change clinical management . in terms of risk magnitudes , palb2 and tp53 are the only bc genes , in addition to brca1 / 2 , that consistently fall into the high - risk category across studies ( ie , confer levels of risk greater than four times that in the general population ) 8 ; the remainder have conflicting evidence regarding the risk category into which they fit.8 , 9 , 31 - 33 our survey confirmed that enigma centers test palb2 and tp53 relatively frequently and regard them as clinically actionable genes . 
 these two genes were tested much less consistently by non - enigma centers , evidencing the lack of consensus , even for genes that are generally regarded as high risk . 
 brip1 , rad51c , and rad51d are ever more accepted as oc but not bc risk predisposition genes ( two to five times the risk compared with the general population ) .15 , 32 notably , many respondents agreed that every patient with oc should be tested for these three genes ( in addition to brca1 / 2 )  . 
although there is currently no indication that oc treatment for a carrier of a pathogenic variant in one of these three genes would differ from that for a noncarrier , carriers may benefit from rrso at menopause . the uncertainties and inconsistencies regarding risk and testing practices are magnified when it comes to syndromic cancer genes like pten , cdh1 , stk11 , nf1 , nbn , and men1 , as well as genes conferring an uncertain risk such as bard1 , rad50 , and mre11a . 
although there is significant evidence for elevated bc risk and lobular bc risk in carriers of pathogenic variants in pten and in cdh1 , respectively , 34 - 36 it is likely that these bc risks ( and those from the other syndromic genes ) are overestimated and therefore unreliable , because they were derived from patients whose histories were consistent with these rare syndromes rather than from unselected patients.8 more robust and replicable penetrance estimates from large - cohort and population studies are certainly needed to further define risks . 
however , on the basis of both the evidence available from the literature and the results of our survey , which incorporate an international clinical perspective , the 16 genes can be grouped into five categories : high bc risk : palb2 , tp53 , pten , and cdh1 ; moderate bc risk : atm and chek2 ; bc risk of unclear magnitude ( but established risk for other cancer types ) : stk11 , nf1 , nbn , and men1 ; moderate oc risk : brip1 , rad51c , and rad51d ; and insufficient evidence for bc or oc risk : bard1 , rad50 , and mre11a . the clinical utility of multigene panel testing is assessed based on the improved outcomes of those managed by evidence - based surveillance or prevention approaches . 
a framework for management of moderate - risk bc / boc genes has been extensively reviewed by tung et al9 and includes a comparison of surveillance guidelines among the united states , united kingdom , and germany . 
there are limited national guidelines available even for genes such as palb2 , brip1 , rad51c , and rad51d , which most participants felt should always be tested because they importantly , are clinically actionable . 
this explains why the guidelines often differ in important aspects such as indication for risk - reducing surgery and type of diagnostic imaging recommendations . our study was initiated to provide a snapshot of enigma clinical practice for non - brca1 / 2 genes . 
because panel testing is currently being implemented in large regions of the world like asia , africa , and south america , similar surveys will need to be redistributed once more countries have established testing protocols . 
even at the time of the survey , testing protocols and surveillance recommendations were in flux in some countries , and broader gene panels were expected to be offered within a short time . 
 we acknowledge that our sampling of nonenigma centers was limited , and we aim to survey a more diverse collection of us , canadian , and other worldwide regional or community practices in future studies . massively parallel sequencing represents a transformational technology that we must learn to apply appropriately in health care . 
although the number of genes , other than brca1 / 2 , associated with bc / boc risk is growing , only a small subset of them have clinical utility at the moment . 
the goal of this study was to highlight the differences across countries and to determine what additional information and infrastructure are still needed to move toward more uniform testing practices and management guidelines internationally . our collected evidence suggests that the clinical usefulness of multigene panel testing for bc / boc predisposition can be improved by a better definition of the cancer risks associated with genetic variation in cancer susceptibility genes and by the availability of evidence - based management guidelines . 
to this end , it is key that clinicians share clinical and genetic data , through enigma and / or other international consortia focused on the clarification of the bc and oc risk associated with genetic variation , and that tested individuals are encouraged to participate in initiatives that collate genetic testing data and in long - term follow - up studies that evaluate intervention strategies . 
palmero , maria piane , marianna puzzo , maria christina sini , angela solano , manuel teixeira , mads thomassen , amanda toland , therese trngren , liliana varesco , jeffrey weitzel , encarna b . 
pedersen , maria piane , marianna puzzo , mark robson , maria rossing , maria christina sini , angela solano , jana soukupova , gianluca tedaldi , manuel teixeira , mads thomassen , maria grazia tibiletti , amanda toland , therese trngren , erica vaccari , liliana varesco , ana vega , barbara wappenschmidt , jeffrey weitzel , arcangela de nicolo , encarna b . 
 rien blok no relationship to disclose akira hirasawa research funding : astrazeneca maria adelaide caligo travel , accommodations , expenses : technogenetics mariarosaria calvello no relationship to disclose gabriele lorenzo capone no relationship to disclose pietro cavalli no relationship to disclose t.l. 
couch consulting or advisory role : astrazeneca research funding : grail other relationship : ambry genetics miguel de la hoya no relationship to disclose simona de toffol no relationship to disclose orland diez no relationship to disclose susan m . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) ros eeles honoraria : janssen - cilag speakers bureau : janssen - cilag anna efremidis no relationship to disclose florentia fostira no relationship to disclose david goldgar no relationship to disclose andreas hadjisavvas no relationship to disclose thomas v.o. 
hansen no relationship to disclose claude houdayer no relationship to disclose petra kleiblova no relationship to disclose sophie krieger no relationship to disclose conxi lzaro no relationship to disclose maria loizidou no relationship to disclose siranoush manoukian no relationship to disclose arjen r . 
 mark robson honoraria : astrazeneca erica vaccari consulting or advisory role : color genomics consulting or advisory role : mckesson , astrazeneca research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , pfizer ( inst ) travel , accommodations , expenses : astrazeneca liliana varesco consulting or advisory role : pfizer maria rossing no relationship to disclose maria christina sini no relationship to disclose angela solano no relationship to disclose jana soukupova no relationship to disclose gianluca tedaldi no relationship to disclose manuel teixeira no relationship to disclose mads thomassen no relationship to disclose maria grazia tibiletti no relationship to disclose amanda toland no relationship to disclose therese trngren honoraria : pfizer , astrazeneca ana vega no relationship to disclose yvonne wallis no relationship to disclose barbara wappenschmidt no relationship to disclose jeffrey weitzel no relationship to disclose amanda b . 
domchek , university of pennsylvania , philadelphia , pa ; anna efremidis , athens medical center ; florentia fostira , national centre for scientific research demokritos , athens , greece ; david goldgar , university of utah school of medicine , salt lake city , ut ; andreas hadjisavvas and maria loizidou , cyprus institute of neurology and genetics , nicosia , cyprus ; thomas v.o. 
pedersen , aalborg university hospital , aalborg , denmark ; akira hirasawa , keio university school of medicine , tokyo , japan ; claude houdayer , universit paris descartes and unicancer genetic group , paris ; sophie krieger , normandy university , cancer center f . 
palmero , barretos cancer hospital , barretos , so paulo , brazil ; mark robson , memorial sloan kettering cancer center , new york , ny ; angela solano , university of buenos aires , buenos aires , argentina ; manuel teixeira , instituto portugus de oncologia do porto francisco gentil , porto , portugal ; amanda toland , ohio state university , columbus , oh ; therese trngren , lund university , lund , sweden ; erica vaccari , dana - farber cancer institute , boston , ma ; barbara wappenschmidt , university hospital cologne and german consortium of hereditary breast and ovarian cancer , cologne , germany ; and jeffrey weitzel , city of hope , duarte , ca . support supported by grant no . 
couch fj , hart sn , sharma p , et al : inherited mutations in 17 breast cancer susceptibility genes among a large triple - negative breast cancer cohort unselected for family history of breast cancer . 
laduca h , stuenkel aj , dolinsky js , et al : utilization of multigene panels in hereditary cancer predisposition testing : analysis of more than 2 , 000 patients . 
maxwell kn , hart sn , vijai j , et al : evaluation of acmg - guideline - based variant classification of cancer susceptibility and non - cancer - associated genes in families affected by breast cancer . 
domchek sm , bradbury a , garber je , et al : multiplex genetic testing for cancer susceptibility : out on the high wire without a net ? j clin oncol 31 : 1267 - 1270 , 2013 8 . 
richards s , aziz n , bale s , et al : acmg laboratory quality assurance committee : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
janatov m , boreck m , soukupov j , et al : palb2 as another candidate gene for genetic testing in patients with hereditary breast cancer in czech republic [ in czech ]  . 
robays j , stordeur s , hulstaert f , et al : oncogenetic testing and follow - up for women with hereditary breast / ovarian cancer , li fraumeni syndrome and cowden syndrome . 
robays j , stordeur s , hulstaert f , et al : oncogenetic testing , diagnosis and follow - up in birt - hoggdub syndrome , familial atypical multiple mole melanoma syndrome and neurofibromatosis 1 and 2 . 
national institute for health and care excellence : familial breast cancer : classification , care and managing breast cancer and related risks in people with a family history of breast cancer . 
lincoln se , kobayashi y , anderson mj , et al : a systematic comparison of traditional and multigene panel testing for hereditary breast and ovarian cancer genes in more than 1000 patients . 
castra l , krieger s , rousselin a , et al : next - generation sequencing for the diagnosis of hereditary breast and ovarian cancer using genomic capture targeting multiple candidate genes . 
pharoah pd , guilford p , caldas c : incidence of gastric cancer and breast cancer in cdh1 ( e - cadherin ) mutation carriers from hereditary diffuse gastric cancer families . 
questions included in the surveys ( by mode of distribution ) ( continued ) question testing methods and setting which method is used to test for gene x ? in - person survey only which genes do you agree should be tested for every bc or oc patient eligible for genetic testing ? describe the gene panels currently used ( if any ) and if they are used in the diagnostic or research setting if you are not currently using gene panels but may in the future , what do you think is required before starting to use them ? ii variant classification classification system ii - 1 ii - 2 reporting and cascade testing of variants clinical i . 
questions included in the surveys ( by mode of distribution ) ( continued ) in - person survey only question ii - 3 variant interpretation in - person and paper surveys paper survey only surveymonkey * who takes responsibility for interpreting the clinical significance of the identified variants ? for cancer susceptibility genes : who takes responsibility for variant interpretation and reporting ? clinical scientist clinical geneticist genetic counselor oncologist ( medical / surgical ) other ( specify ) who takes responsibility for discussing the clinical significance / utility of an identified variant ? ( same choices as above ) are there clinical guidelines for managing patients who carry a pathogenic or likely pathogenic variant in a bc susceptibility gene ? iii risk management guidelines for which genes do you agree that the cancer - associated risks are high enough to alter clinical practice / management ? are management guidelines available at your center for patients with ( likely ) pathogenic variants in these genes ? yes , national guidelines yes , local guidelines or local adaptations of national guidelines no , guidelines are not currently available if clinical management guidelines are available at your center for the specified genes , please provide digital copy , reference , or web site link note . 
questions i - 4 and iii of the in - person survey were asked at a different time compared with the remainder of the survey ; therefore , answers were collected from only 23 centers . 
 these two questions were asked at a different time ( during evidence - based network for the interpretation of germline mutant alleles meeting in cyprus in january 2017 compared with survey questionnaire )  . 
the centers that tested each gene through research only were compared with the proportion of centers that tested the gene only clinically and proportion of those that tested the gene for both clinical and research purposes . 
genes tested regularly by evidence based network for the interpretation of germline mutant alleles ( enigma ) centers in the united states ( enigma - us ) versus other enigma centers ( enigma - other ) versus italian and united kingdom non - enigma centers . 
 of centers testing given gene regularly ( defined as ordered for > 50% of patients eligible for genetic testing , by criteria that we recognize may differ by center / country ) is shown above each bar . 
of centers that answered this question was four to seven , depending on the gene ; of the 31 enigma - other centers , a range of 22 to 30 centers answered this question . 
mcgowan , phd1 , 2 purpose although analyzing germline and tumor samples concurrently provides the best opportunity for differentiating between germline and somatic mutations , tumor - only sequencing is becoming increasingly common in clinical care . 
with limited professional society guidance on how to manage pathogenic mutations identied via tumor - only sequencing , this study contemplates the professional knowledge and skills necessary to have represented on an mgtb to interpret these results in context of potential germline ndings . methods qualitative interviews with mgtb members and an ethnographic case study of a breast cancer mgtb at a national cancer institute cancer center were examined . results this mgtb discussed 34 cases of women with advanced - stage breast cancer over 13 months . interviews and observations of mgtb meetings indicated that members of the mgtb contemplated whether variants were germline or somatic and potential for identication of germline cancer predisposition . 
however , the mgtb only referred 11 patients ( 61% ) for additional germline testing , and the remaining seven patients ( 39% ) were not referred , raising questions about the kind of genomic expertise needed on an mgtb to optimize results interpretation and referrals . conclusion to ensure adequate interpretation , recommendation , and communication of tumor sequencing results , an mgtb should include professionals with knowledge and experience in clinical translation of tumor sequencing , testing methodology , molecular pathology , cancer biology , genomic pathways , germline variant interpretation , evaluation of family history , and application of professional recommendations for germline testing after tumor - only sequencing . 
 fishler et al context key objective : how are tumor - only sequencing results interpreted by a multidisciplinary genomic tumor board ( mgtb ) ? which professional expertise ought to be represented when discussing these results and recommendations ? knowledge generated : commercial laboratories provision of tumor - only sequencing without germline reference samples can complicate the ability of an mgtb to interpret patients genomic sequencing results and make recommendations for targeted treatment and referrals for additional genetic testing . 
providers on an mgtb questioned whether a known or likely pathogenic tumor sequencing variant was germline or somatic , sometimes overlooked known / likely pathogenic mutations in cancer susceptibility genes other than brca1 / 2 , and recognized the necessity of varied professional expertise when interpreting tumor - only sequencing results . relevance : to ensure appropriate interpretation of tumor - only sequencing and identication of patients who ought to be referred to genetics , an mgtb should include individuals with expertise in clinical translation of tumor sequencing , testing methodology , molecular pathology , cancer biology and genomic pathways , germline variant interpretation , evaluation of personal and family history , and application of professional guidelines for germline testing . 
to mitigate provider deliberation and genomic knowledge necessary to determine if additional germline testing is necessary , genetics professional societies and clinical laboratories ought to consider whether tumor - only sequencing should be routinely paired with germline samples to facilitate standardized reporting of germline variants . the basis of tumor - only sequencing results , even when combined with their family history . a previously published study from a breast cancer mgtb revealed that decisions about which patients received genetics referrals were not standardized.10 this prior analysis did not explore the factors the mgtb used to determine which patients received genetics referrals after tumor - only sequencing . 
our study aimed to identify these factors and to explore which professionals ought to be involved on an mgtb to ensure adequate interpretation , clinical application , and referral for additional germline testing when appropriate . each interview ranged in length from 25 to 49 minutes . 
all mgtb members signed a written informed consent , which allowed for recording , transcription , and analysis of the meeting minutes and interview data . data were collected using standard qualitative research including ethnography and in - depth inmethods , interviews and mgtb meetings were audio terviews . recorded and transcribed verbatim by a medical transcriptionist . 
participants in this study included 22 members of a breast cancer mgtb at one urban national cancer institute cancer center . methods included an ethnographic case study of mgtb meetings and interviews with mgtb members . 
this group met monthly from october 2013 to november 2014 to discuss results of tumor - only sequencing ordered for patients with advanced - stage breast cancer in a clinical setting . mgtb members were invited to participate in a semistructured interview regarding their opinions about a tumor board approach to interpreting tumor sequencing results . in total , 12 members of the board were interviewed by the research team , including treating physicians ( n = 6 ) , bioinformaticians ( n = 3 ) , a pathologist ( n = 1 ) , a medical geneticist ( n = 1 ) , and an administrator ( n = 1 ) .10 all patients discussed by this mgtb were women with advanced - stage breast cancer and tumor - only sequencing performed as part of their clinical care ( n = 34 )  . 
the mgtb discussed all of the hospitals patients with breast cancer who underwent tumor sequencing during the study period . all patient samples were sent to the same commercial laboratory for sequencing and analysis . the laboratory - generated tumor sequencing report suggested on - label / off - label treatments and clinical trial options on the basis of known / likely pathogenic mutations . pathogenic and likely pathogenic results were listed separately from vus results . 
as published in the preliminary analysis , mgtb recommendations included genetics referrals for suspected germline variants , clinical trial recommendations , us food and drug administrationapproved on - label therapies , androgen receptor testing , and repeat human epidermal growth factor receptor 2 testing . 
 underlying germline variants in tumor - only sequencing leaderships commitment to adherence with evidencebased medicine and bioethical principles of benecence and nonmalecence.10 of the 34 patients tumor sequencing results that the mgtb reviewed during the study period , 18 patients met nccn criteria for additional germline testing on the basis of their personal history , including type of breast cancer , age of onset , and / or the identication of a known / likely pathogenic tumor mutation in a cancer susceptibility gene . 
the remaining seven patients ( 39% ) represent missed opportunities for additional germline testing on the basis of the patients personal history , prior germline testing , and / or tumor - only sequencing result ( table 2 )  . 
five of these patients were missed on the basis of a combination of these factors ; two were missed on the basis of personal history alone . through analysis of mgtb member interview transcripts and mgtb meetings , three themes emerged : provider confusion about whether a variant identied by tumoronly sequencing was germline or somatic , potential for tumor - sequencing identication of germline cancer predisposition , and genetics expertise necessary for inclusion on an mgtb . provider confusion about whether a mutation was germline or somatic one key question raised by mgtb members was whether the variants listed on tumor sequencing reports were germline or somatic . 
on the basis of the way mgtb members managed the referral process , it became apparent that they disagreed about their role as evaluators of tumor - only sequencing results , including determining whether follow - up with additional germline testing was necessary . 
for example , one medical oncologist mentioned that all mutations relevant treatment were listed on the rst page of the patients report and that if we dont have a lot of time , we may not ip through the rest to see what else might be listed there . in contrast , another oncologist advocated for a more active interpretation : we cant role in report take what [ commercial vendor ] recommends as gospel truth and say okay , this is what were going to go with , because they recommended itthe interpretation needs to happen from our end . just result in addition to differing perspectives about terpretation , there was confusion among the mgtb members regarding whether the reported mutations were somatic or germline . 
a discussion about a patient with a reported mutation in fancc highlights this confusion , which affected their thoughts about whether the patient should receive a genetics referral ( table 3 )  . 
of times reason was discussed during the mgtb meetings patient referrals for additional germline testing on the basis of personal history triple - negative cancer and age of diagnoses , 60 years diagnosis of bilateral breast cancer on the basis of results of tumor - only sequencing report for parp inhibitors identication of known / likely pathogenic fancc mutation identication of known / likely pathogenic chek2 mutation identication of known / likely pathogenic mlh1 mutation identication of known / likely pathogenic nf1 mutation identication of known / likely pathogenic mutation or vus in brca1 / 2 to determine eligibility on the basis of personal history and of tumor - only sequencing report re - evaluation of brca1 / 2 status for parp inhibitors because of prior negative germline results and negative tumor sequencing results for brca1 / 2 identication of known / likely pathogenic tp53 mutation on tumor sequencing and age of diagnoses note . 
missed opportunities for referral for additional germline testing ( n = 7 ) fishler et al missed opportunity on the basis of personal history on the basis of tumor - only sequencing report identication of known / likely pathogenic pten variant on the basis of personal history and tumor - only sequencing report triple - negative breast cancer , rst breast cancer diagnoses , 60 years , and no prior germline genetic testing personal diagnosis of lobular breast cancer and identication of known / likely pathogenic cdh1 variant on the basis of previous genetic test results and tumor - only sequencing report negative brca1 / 2 germline testing before availability of bart testing , no mutation in brca1 / 2 gene identied on tumor negative brca1 / 2 germline testing before availability of bart testing , pten mutation identied on tumor sequencing sequencing total no . 
the tumor - only report does not distinguish variants that are reported pathogenic from variants that are reported likely pathogenic . they are reported as one category on the front page of the report . 
seven patients out of 18 discussed at the mgtb did not receive a genetics referral for additional germline testing , although it would have been indicated by nccn criteria or a known / likely pathogenic mutation identied in a cancer susceptibility gene by tumor - only sequencing . 
at the time of the study of this mgtb , nccn criteria recommended that patients with negative brca1 / 2 sequencing before 2006 have bart testing and women with triple - negative breast cancer and their rst breast cancer diagnoses before age 60 years have brca1 / 2 germline testing . 
in addition , the american college of medical genetics and genomics recommended that pathogenic germline mutations associated with hereditary cancer syndromes be returned to patients ( such as pten and cdh1 )  . abbreviations : bart , brac analysis rearrangement test ; mgtb , multidisciplinary genomic tumor board ; nccn , national comprehensive cancer network . testing , some of the medical oncologists were reluctant , because the gene was not directly related to hereditary breast and ovarian cancer syndrome . 
mgtb interviewees indicated lack of education regarding medical genetics as a limitation of the mgtb , which is a recognized barrier to autonomous use of genetic testing by ordering physicians.2 , 12 potential for identication of germline cancer predisposition consistent with the mgtbs focus on identifying treatment options , 10 members of this mgtb were most concerned about whether a patient had a brca1 / 2 mutation to determine their eligibility for treatment with poly ( adp - ribose ) table 3 . 
vignette : confusion about somatic versus germline mutations vignette medical oncologist 7 : it says in the report that germline mutations in fancc cause fanconi anemia , a clinical heterogeneous disorder , and that appropriate clinical testing [ to detect ] the presence of a germline mutation is recommended . 
whenever we see a mutation , we have to make sure that we realize its one test and we would need it to be validated , but does it have relevance for treatment ? ( talking about prior treatment responses and discussion about parp inhibitor recommendations ) medical oncologist 7 : and she was germline brca tested and all thats negative ? medical oncologist 1 : yeah , she was brca negative . medical oncologist 2 : should we refer to genetics about this fancc thing ? medical oncologist 1 : you think we should refer ? is there a reason to think about it ? medical oncologist 7 : the only way you can test it is on those panels . 
every genetics has a panel where you can test for fanconi anemia genesi dont know how much breast cancer risk or other risks [ are associated with variants in this gene ]  . 
 underlying germline variants in tumor - only sequencing polymerase inhibitors , which gained traction as a mutationguided treatment option during the study period.13 , 14 thus , all patients with tumor - only sequencing results that included a vus or known / likely pathogenic mutation in brca1 / 2 were referred to genetics ( n = 4 )  . patients with known / likely pathogenic mutations in other cancer susceptibility genes ( such as pten ) were not routinely referred to genetics ( table 2 )  . 
at the time of this study , american college of medical genetics and genomics recommended that when analyzing a tumor and paired germline sample , such results should be conrmed and communicated to patients as secondary ndings , because of their association with a hereditary cancer syndrome . however , nccn guidelines did not include a recommendation for additional germline testing for mutations in genes on the secondary ndings list , 7 which may have contributed to inconsistent referral patterns , especially given that the mgtb was reviewing tumor - only sequencing results . two additional patients who met nccn guidelines for germline testing on the basis of their personal history were not referred for germline testing ( table 2 )  . 
at the time of the study of this mgtb , nccn recommended bart ( brac analysis rearrangement test ) testing for patients who had received negative brca1 / 2 germline test results before 2006.7 two patients with negative brca1 / 2 tumor - only sequencing results and negative brca1 / 2 germline test results before the availability of bart testing were not referred to genetics , although a genetics referral would have been indicated by nccn guidelines . 
in discussing how well individual disciplines were represented on the mgtb , a medical oncologist who co - led the mgtb recognized the value of genetics expertise in interpreting whether certain mutations were common or rare and how to manage referrals on the basis of a variants likelihood of being germline . 
explicitly , she noted that knowledge and experience with specic gene pathways enhanced the variant interpretation and productivity of the discussions about treatment options and result interpretation during the mgtb meetings . 
she also described disappointment that a medical geneticist and genetic counselors were invited , but that a medical geneticist only attended one mgtb meeting over the 13 - month study period and no genetic counselors participated . 
however , the other medical oncologist who co - led the mgtb mentioned that scheduling posed a barrier to genetic counselors attendance . mgtb members discussed the limitations of the test throughout the entire study period . 
the pathologist cautioned during her interview that not all providers who order tumor - only sequencing may understand the limitations of the test in terms of identifying germline variants : its hard to speak for other doctors , other community doctors . 
furthermore , at one meeting , the medical geneticist explained sequencing methodology , utility of bart testing for patients who have previously tested negative for brca1 / 2 , and guidelines for germline testing on the basis of a patients personal history , including age and triple - negative diagnosis . 
this information shifted the conversation from discussion of clinical trial options for a patient with triple - negative breast cancer who previously tested negative for mutations in brca1 / 2 to clarication of other germline testing options including bart testing , in accordance with nccn recommendations.7 during his interview , the medical geneticist stressed the value of genetics professionals who can address psychosocial concerns with patients during result return when a germline mutation is suspected . 
he noted that this skill was outside of his scope of practice and was one of the most difcult parts of result return . discussion for patients discussed by this mgtb , tumor sequencing was performed as part of clinical care . 
members of this mgtb , including medical oncologists , questioned whether the results of tumor sequencing were somatic or germline and queried what resources were available to them to clarify this information . 
the medical geneticist was the only mgtb member who was board certied in medical genetics . however , he was not present at the majority of mgtb meetings to provide clarication regarding whether a patient discussed on the mgtb should receive additional germline genetic testing . 
other mgtb members without medical genetics board certication may have qualied as a commission on cancer ( coc ) dened genetics professional by providing cancer risk assessment on a regular basis.15 ( p51 ) a key question that emerged through this analysis is whether these criteria are sufcient to ensure optimal implementation and interpretation of tumor sequencing by an mgtb and how best to support clinicians as they move into using new genomic technologies in their practices . nccn currently recommends genetic risk evaluation for patients with a known / likely pathogenic variant identied in a cancer susceptibility gene via tumor sequencing . 
perceived value of types genetics expertise on an mgtb perceived value by mgtb members member illustrative quote medical oncologists identication of clinical trials evaluation of treatment options medical oncologist : i can look and see if that [ three prior investigational studies ] will exclude her from [ clinical trials ] in the area , but that would sort of be my preference would be to put her on the phase i while looking for regional studies , and ill contact [ name ] and look on clinicaltrials.gov. 
and i guess were not recommending treatment off study with one of these m2r inhibitors ? basic scientists evaluation of functional studies radiation oncologist : someone who has more expertise in the basic science stuffwith better knowledge about genomic pathways understanding of mechanisms of the different mutations and how that may or may not translate into something that the drug might actually work for . medical evaluation of testing geneticists methodology variant classication genetic evaluation of family history counselors variant classication psychosocial counseling during result return medical geneticist : it is still not clear using next - generation sequencing whether a negative result is [ a true negative ] , because you have to look at the coverage across each position and the number of reads theyre reporting . 
second , rearrangements can be missed , so wed want to have her get bartshe should get the [ germline ] testingjust given her age of diagnosis and the fact that its triple - negative . medical geneticist : the most challenging patient encounters ive had is telling a mom that shes passed [ the mutation ] along to her daughter , and having the daughter understand that her mom just passed along a gene that basically assures her that shell get breast cancer in her lifebut it is very challenging , the psychosocial aspect . abbreviations : bart , brac analysis rearrangement test ; mgtb , multidisciplinary genomic tumor board . family history to determine whether people with known / likely pathogenic mutations in cancer susceptibility genes should receive additional germline testing . 
when clinical sequencing laboratories do not compare variants identied in a tumor sample with a germline sample , ordering providers are responsible for lling this gap in professional recommendations by recognizing when clinical germline testing is indicated on the basis of the combination of personal history , tumor sequencing results , and family history . currently , there are no guidelines or recommendations for which professionals or types of genomic expertise should be included by an mgtb to ensure adequate interpretation , recommendation , and communication of genomic test results . 
the coc denes certain roles within a cancer center and provides guidelines for the frequency and format of multidisciplinary tumor boards.15 however , it does not dene what disciplines should be included to constitute an mgtb , nor does it specify guidelines for tumor boards that evaluate tumor - only sequencing . 
the coc denes a genetics professional in a cancer center as someone who provides cancer risk assessment on a regular basis15 ( p51 )  . although multiple clinicians on this mgtb may have met this coc denition , many expressed confusion regarding benets and limitations of genetic testing and genetic risk assessment as well as knowledge deciencies surrounding testing methodology and result interpretation . 
this suggests that the genetics expertise pertinent for interpreting tumor - only sequencing results may be partial or unevenly distributed among those who were tapped to lend their expertise to an mgtb . on the basis of the results of this single - site case study , when considering how denitions of a genetic professional may be applied to mgtbs , providing cancer risk assessment on a regular basis is insufcient for conferring expertise for implementing tumor sequencing in clinical care . to ensure appropriate interpretation of tumor sequencing and identication of patients who ought to be referred to genetics , an mgtb should include individuals with expertise in clinical translation of tumor sequencing , testing methodology , molecular pathology , cancer biology and genomic pathways , germline variant interpretation , evaluation of personal and family history , and application of professional guidelines for germline testing . 
 underlying germline variants in tumor - only sequencing societies and organizations and clinical laboratories ought to consider whether tumor - only sequencing should be routinely paired with germline samples to facilitate standardized reporting of germline variants . given that the mgtb under study was primarily focused on treatment and clinical trial recommendations on the basis of results of tumor sequencing , it may not have been the optimal setting to discuss a patients personal history , including prior genetic testing and / or potentially pathogenic variants in cancer susceptibility genes lacking treatment implications . 
however , to ensure comprehensive referrals for additional germline sequencing after tumor - only sequencing , ordering providers ought to interpret the patients personal history in combination with their tumor - only sequencing results , as discussed by the mgtb . 
for two patients with negative brca1 / 2 tumor - only sequencing results and negative brca1 / 2 germline testing before the availability of bart testing , negative brca1 / 2 tumor - only sequencing results may have been falsely reassuring for these providers , especially considering the possibility that other cancer susceptibility genes may have been responsible for the cause of their cancer . is possible that provider deliberation about whether certain patients should be referred to genetics on the basis of these factors , not specic to the purpose of convening the mgtb the mgtb , may have occurred outside of meetings and would not have been captured by this analysis . 
in a climate where there is a paucity of genetic counselors and medical geneticists , creative strategies for engaging genetics professionals formally and informally in mgtb deliberations should be considered to optimize interpretation of tumor sequencing results . 
this study was limited by the information discussed as part of the mgtb meetings focused on patients with advanced breast cancer and interviews with mgtb members at a single national cancer institutedesignated cancer center . 
thus , possible that there were additional patients with known / likely pathogenic variants in genes associated with an inherited cancer predisposition syndrome that were not captured by this analysis , or that geneticists or genetic counselors may have been consulted about interpretation of laboratory reports outside of the mgtb context . 
fishler research funding : illumina ( inst ) lauren walters - sen employment : invitae stock and other ownership interests : invitae consulting or advisory role : ischemia care no other potential conicts of interest were reported . acknowledgment we thank roselle ponsaran , tracie baker , rebecca sisson , and the multidisciplinary genomic tumor board members for their time and contribution to this study . 
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mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
mcgowan ml , ponsaran rs , silverman p , et al : a rising tide lifts all boats : establishing a multidisciplinary genomic tumor board for breast cancer patients with advanced disease . 
catenacci dv , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 13 . 
 poly ( adp - ribose ) polymerase inhibitor activity in prostate cancers harboring mutations in dna repair genes : who benets ? shridar ganesan , md , phd1 and judy garber , md , mph2 the seminal nding that cancers harboring mutations in brca1 or brca2 are often exquisitely sensitive to poly ( adp - ribose ) polymerase ( parp ) inhibition has led to the successful development of parp inhibitors as effective targeted therapies for brca1 / 2 - mutated ovarian , breast , prostate , and pancreatic cancers.1 - 7 because many other genes are indirectly or directly involved in the brca1 / 2 - associated homologous recombination ( hr ) mediated dna repair ( hrd ) pathway , there has been a great deal of interest in rationally expanding the use of parp inhibitors to include cancers harboring mutations in these related dna repair genes.8 , 9 these include genes intimately associated with the brca1 / 2 hrd pathway , such as palb2 , bard1 , brip1 , and the rad51 paralogs , as well as genes less directly involved in hrd , such as atm and chek2 . 
is there evidence of biallelic loss of function of the gene in the tumor ? both of these criteria would presumably be required for a tumor to manifest a defect in hr - mediated repair sufciently profound to lead to sensitivity to parp inhibitors . 
the second criterion is especially important because , for many dna repair genes , the heterozygous state has at most a subtle repair phenotype that would not impart sensitivity to parp inhibitors . 
even if a lossof - function mutation in a critical dna repair gene is detected in a tumor , there must also be loss of the wildtype allele or , rarely , a dominant negative heterozygous mutation or evidence of epigenetic silencing of the wildtype allele for the tumor to have a profound dna repair defect . 
similarly , for each gene considered as a biomarker of sensitivity to parp inhibitors , data regarding the functional effect of biallelic loss on the hrd pathway and subsequent relative sensitivity to parp inhibitors need to be carefully evaluated . this leads us to the recently published randomized phase iii profound study ( clinicaltrial.gov identier : nct02987543 ) of the efcacy and safety of olaparib in men with metastatic castration - resistant prostate cancer harboring germline mutations in a set of dna repair genes who experienced disease progression on initial hormonal treatment.10 all patients had an alteration in one of 15 genes ( brca1 , brca2 , atm , brip1 , bard1 , cdk12 , chek1 , chek2 , fancl , palb2 , ppp2r2a , rad51b , rad51c , rad51d , and rad54l ) and were randomly assigned in a 2 : 1 fashion to receive either the parp inhibitor olaparib or physicians choice of second - line hormonal therapy with enzalutamide or abiraterone . 
the trial was divided into two cohorts , with cohort a ( n = 245 ) having an alteration in brca1 , brca2 , or atm , and cohort b ( n = 142 ) having alterations in any of the other 12 genes . 
the key question is whether the benet of olaparib treatment seen in both cohort a and cohorts a and b overall is driven primarily by benet in patients with brca2 mutations in both instances . 
here again , analysis of high - depth sequencing data may be able to identify which brca1mutant prostate cancers have undergone loss of heterozygosity with loss of wild - type brca1 allele and are thus truly sensitive to parp inhibitors.13 some individual gene analyses were presented as exploratory analyses as well . 
cancers with mutations in rad51b and rad54l , which are genes directly involved in hrd , had some evidence of benet , but numbers are small ( see supplementary figure s6 in de bono et al10 )  . 
the rest of the genes , including palb2 , bard1 , brip1 , fancl , chek1 , rad51c , and rad51d , conferred eligibility on fewer than ve randomly assigned patients each and cannot be assessed . these data suggest that brca2 - mutant prostate cancers denitely benet from olaparib treatment , and this is a clear advance in the treatment of this subset of prostate cancers . however , it may well be that the benet seen in the brca2mutant population is driving the overall benet seen in both cohort a and the combined group of cohorts a and b in this study . 
the reason for lack of a clear signal in atm - mutant prostate cancer needs to be further investigated , and analysis of both allelic status of the mutations and molecular evidence of patterns of genomic instability associated with hrd may help resolve these issues . 
several reports have shown that atm - mutant breast cancers may not respond to parp inhibitors , 14 , 15 suggesting that atm mutation may not confer clinical sensitivity to parp inhibitors . 
different therapeutic strategies may be required to effectively treat atm - mutant prostate cancers , and other rational treatments , such as atr inhibitors , need to be investigated.16 the lack of clear signal of benet in prostate cancers harboring brca1 mutations may be a result of the small numbers and the fact that , unlike breast , ovarian , and pancreatic cancers , many brca1 - mutant prostate tumors often do not show evidence of biallelic alteration.11 , 17 although there are hints of benet in cancers harboring mutations in other genes critical for hr , including the rad51 paralogs , the numbers in this trial are too small to make any denitive conclusion . 
for example , palb2 and rad51 paralogs clearly play a central role in hrd , and there are data demonstrating that palb2 mutation in breast and prostate cancer and rad51 paralog mutation in ovarian cancer are associated with benet from parp inhibitors.14 , 15 , 18 - 20 evaluation of the landscape of other hrd gene mutations in different cancer types and data regarding the settings in which there is strong evidence of biallelic loss may help guide development of these genes as biomarkers for parp inhibitors . in designing future trials that rationally target specic dna repair defects in cancer , simply identifying a pathogenic mutation in a broad set of genes in the tumor or in germline may not be sufcient to dene the population likely to benet . 
clear evidence that loss of function of each gene of interest confers high - level sensitivity to the drugs being evaluated needs to be presented , and the allelic status of the gene in the tumor may need to be assayed . 
in some settings , such as ovarian and breast cancer , the nding of a pathogenic brca1 or brca2 mutation , either germline or somatic , is almost always associated with evidence of biallelic mutations , but in other cancers and with other dna this may not necessarily be the case.17 repair genes , evaluation of allelic status can be approached by computational methods , but there may be settings , including epigenetic silencing and dominant negative alleles , where this approach will need to be complemented by functional assays of genomic instability . 
here , assays using wholegenome sequencing or targeted sequencing may also be informative in determining whether the presence of a dna repair gene mutation is accompanied by mutation patterns consistent with a profound defect in hrd.21 - 23 the presence of reversion mutations or mutations in compensating genes also can affect sensitivity to parp inhibitors and may need to be considered.24 , 25 in summary , a more sophisticated approach to analysis of dna repair status of cancers , which includes not only identifying the presence of a pathogenic mutation , but also demonstrating that there is loss of the wild - type allele , lack of reversion mutation , and / or genomic evidence of a profound dna repair defect , may be required to optimally identify cancers that may benet from parp inhibitors and related dna - damaging agents . 
grouping together a set of related genes for pooled analysis may , given differences in prevalence of individual mutations and effect size of benet for different genes , lead to settings where the overall benet in the pool may be driven only by a subset of genes . 
if this possibility is not considered , pooled analysis could lead to approval of therapies for gene alterations when these therapies are ineffective and prevent or delay development of more effective targeted therapies for those patients . 
gene - level analysis may make trial design more difcult , but ultimately , it may lead to more precise use of therapies that target specic dna repair defects or other loss - of - function alterations in cancer . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / authors / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis , roche , foghorn therapeutics , foundation medicine , merck sharp & dohme research funding : m2gen ( inst ) patents , royalties , other intellectual property : i hold 2 patents for digital imaging that may be licensed to ibris and inspirata other relationship : national cancer institute / national institutes of health judy garber consulting or advisory role : novartis ( i ) , gtx ( i ) , helix biopharma , konica minolta , aleta biotherapeutics ( i ) , h3 biomedicine ( i ) , kronos bio ( i ) research funding : novartis ( i ) , ambry genetics , invitae genetics , myriad genetics other relationship : susan g . 
n engl j med 361 : 123 - 134 , 2009 gonz alez - martn a , pothuri b , vergote i , et al : niraparib in patients with newly diagnosed advanced ovarian cancer . 
n engl j med 381 : 2391 - 2402 , 2019 kaufman b , shapira - frommer r , schmutzler rk , et al : olaparib monotherapy in patients with advanced cancer and a germline brca1 / 2 mutation . 
moore kn , secord aa , geller ma , et al : niraparib monotherapy for late - line treatment of ovarian cancer ( quadra ) : a multicentre , open - label , single - arm , phase 2 trial . 
lancet oncol 20 : 636 - 648 , 2019 litton jk , rugo hs , ettl j , et al : talazoparib in patients with advanced breast cancer and a germline brca mutation . 
n engl j med 379 : 753 - 763 , 2018 golan t , hammel p , reni m , et al : maintenance olaparib for germline brca - mutated metastatic pancreatic cancer . 
sokol es , pavlick d , khiabanian h , et al : pan - cancer analysis of brca1 and brca2 genomic alterations and their association with genomic instability as measured by genome - wide loss of heterozygosity . 
sakamoto s , iijima k , mochizuki d , et al : homologous recombination repair is regulated by domains at the nand c - terminus of nbs1 and is dissociated with 13 . 
khiabanian h , hirsheld km , goldnger m , et al : inference of germline mutational status and evaluation of loss of heterozygosity in high - depth , tumor - only atm functions . 
gruber jj , afghahi a , hatton a , et al : talazoparib beyond brca : a phase ii trial of talazoparib monotherapy in brca1 and brca2 wild - type patients with advanced her2 - negative breast cancer or other solid tumors with a mutation in homologous recombination ( hr ) pathway genes . 
tung nm , robson me , ventz s , et al : tbcrc 048 : a phase ii study of olaparib monotherapy in metastatic breast cancer patients with germline or somatic mutations in dna damage response ( ddr ) pathway genes ( olaparib expanded )  . 
yap ta , ocarrigan b , penney ms , et al : phase i trial of rst - in - class atr inhibitor m6620 ( vx - 970 ) as monotherapy or in combination with carboplatin in patients with advanced solid tumors . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
chandran ea , kennedy i : signicant tumor response to the poly ( adp - ribose ) polymerase inhibitor olaparib in heavily pretreated patient with ovarian carcinosarcoma harboring a germline rad51d mutation . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deciency among breast cancer subtypes . 
telli ml , timms km , reid j , et al : homologous recombination deciency ( hrd ) score predicts response to platinum - containing neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
poly ( adp - ribose ) polymerase inhibitors ( parpi ) represent one approach , as investigated in previous studies using olaparib.5 - 7 we describe a patient with an unresectable mgmt unmethylated , idh wild - type gbm . 
the patient was enrolled in an observational clinical study ( sponsored by strata through which wholeoncology , ann arbor , mi ) , exome and rna sequencing on formalin - xed parafn - embedded tumor tissue revealed loss - offunction mutations in atm and tumor protein 53 ( tp53 )  . 
the tumor was classied as tumor mutational burden ( tmb ) high , programmed death - ligand 1 ( pd - l1 ) low , and microsatellite stable ( mss ; table 1 )  . 
after completion of therapy , additional review of patients records revealed a germline msh6 loss - offunction mutation , which conrmed lynch syndrome . the genomic ndings and high likelihood of lynch syndrome , along with early - phase data suggesting safety and brain penetration , provided rationale for the treating oncologist to initiate olaparib with standard chemoradiation . 
she was also treated with alternating tumor - treating elds ( optune ; novocure , st helier , jersey ) , an externally applied , low - intensity electromagnetic eld treatment shown to improve survival by 4.9 months over maintenance temozolomide alone when used 18 hours per day.8 device compliance was limited , and treatment was discontinued after 1 month . 
outside hospital records included this nding on germline testing performed by ambry genetics ( aliso viejo , ca )  . msh6 is involved in dna mismatch repair ( appendix table a1 )  . 
most mutations are somatic , found almost exclusively after temozolomide therapy.11 in this setting , they are associated with resistance to alkylating agents , hypothesized to be the dominant mechanism of acquired temozolomide resistance after therapy , likely because of failure of temozolomideinduced dna damage to result in apoptosis in mismatch repairdecient ( dmmr ) cells.12 - 24 when msh6 mutations in treatment - nave patients with mgmt are present methylated , otherwise chemosensitive tumors , treatment response is markedly attenuated.13 beyond treatment resistance , ongoing temozolomide exposure after msh6 inactivation leads to a hypermutator phenotype and tumor progression.14 - 16 parpi restore sensitivity to temozolomide in dmmr cells.25 dmmr cells may also have increased resistance to radiotherapy.26 - 28 lynch syndrome was not identied by somatic testing . often , lynch syndrome is discovered after a tumor is found to be microsatellite instability high ( msi - h ) or dmmr on immunohistochemistry . 
msh6 - mutated brain tumors , however , are often not msi - h by standard polymerase chain reaction testing , and immunohistochemistry is not standardly performed.29 in this case , mss status was determined from next - generation sequencing ( ngs ) on the basis of length variant allele counts at multiple microsatellite loci . 
while alternate ngs methods have demonstrated sensitivity and specicity in brain tumors , this specic methodology in gbm is performance of unknown.30 , 31 while decient msh6 immunohistochemical staining would conrm a pathogenic mutation , intact staining would not rule out dmmr because some mutations result in intact expression of dysfunctional protein.32 - 35 the msh6 mutation was not reported by somatic testing because of its presence in a stretch of repeating cytosines , known as a homopolymer region . 
380 cns tumors associated with protein loss of function.45 as previously mentioned , p53 - decent cells may be particularly vulnerable to dna - damaging treatment when an atm mutation is present . 
conversely , the combination of dmmr and p53 - decient cells worsens response because of failed phosphorylation of p53 and , thus , failed cell arrest after treatment - induced dna damage.46 in general , cancers with mutant p53 have reduced sensitivity to chemotherapy and radiation ; however , there are many instances where mutant p53 has no effect or even enhances treatment effect.47 tmb high tmb was determined from ngs and included noncoding and coding , synonymous and nonsynonymous , and singlenucleotide and multinucleotide variants present at  . 
while frequently performed through immunohistochemistry , classication was based on sequencing results in this patient , using a score derived from the percent of maximum pd - l1 expression across tested tumor samples . 
this method is validated in a lung cancer cohort , but accuracy in gbm is less certapd - l1 is expressed on the surface of most glioma cells , with increased frequency in high - grade gliomas such as gbm , and variable detection is based on technique.52 - 54 of note , several studies demonstrated high pd - l1 association with worse survival gbm.55 there are no currently approved drugs that target pd - l1 in gbm , although several trials are ongoing . 
given the efcacy of programmed death 1 ( pd - 1 ) / pd - l1 blockade in dmmr tumors , immunotherapy could be considered.56 the pd - 1 inhibitor pembrolizumab is approved for all msi - h tumors , making it a treatment option for patients with lynch syndromeassociated cancers , which are typically msi - h . rationale for olaparib parp is involved in single - strand dna break and base excision repair . 
 file , morgan , and khagi expression in gbm.57 olaparib is a parpi that impairs the ddr , increasing treatment - induced chromosomal instability , cell cycle arrest , and apoptosis.58 in patients with germline brca1 / 2 mutations that impair double - strand dna break repair by homologous recombination , parpi cause synthetic lethality with signicant clinical benet.59 - 62 parpi also have efcacy in tumors with mutations in ddr including atm , and in patients with neither genes , a germline brca mutation nor other homologous recombination deciency.63 , 64 parpi have been used as monotherapy and in combination with radiation and chemotherapy to prevent the repair of treatment - induced dna breaks , thereby promoting tumor cell death . 
parpi increase sensitivity to temozolomide in cell and xenograft models of gbm.65 - 67 this effect persists in mgmt unmethylated tumors.68 parpi also restore sensitivity to temozolomide in dmmr cells.25 , 69 in addition , exposure to temozolomide before or concurrently with a parpi increases the magnitude of dna damage and led to complete regression of gbm cells in one study.70 this treatment - sensitizing effect is not present in patients with temozolomide resistance , which suggests optimal corporation in newly diagnosed gbm.71 there have been 3 phase i trials of olaparib with temozolomide and / or radiation in gbm . 
the oparatic trial conrmed tumor penetration and dosing schedule , with promising early results.5 , 7 paradigm - 2 investigated olaparib plus radiotherapy with or without temozolomide.6 , 72 these studies support the addition of olaparib to temozolomide and radiation as safe , well tolerated , and potentially radiosensitizing.5 discussion this patient had an excellent , durable response despite many factors that predict a poor prognosis . 
in addition , somatic msh6 loss - of - function mutations contribute to temozolomide resistance , glioma recurrence , and tumor progression , with similar effects expected from a deleterious germline mutation . 
while atm mutations improve treatment sensitivity , particularly with concurrent tp53 mutations , it is unlikely that this would result in a sustained , near - complete response with standard chemoradiation alone . 
it is also unlikely that tumor - treating elds improved clinical outcome given short duration of use . in addition to the general chemoand radiosensitizing properties of parpi , the ability for parpi to restore sensitivity to temozolomide in dmmr and mgmt unmethylated tumors , as well as efcacy of parpi in ddr - decient tumors , strongly suggests that olaparib was an essential component of the treatment regimen . 
the likelihood of olaparib - induced synthetic lethality is high , through impairment of single - stranded dna break repairs in a tumor already decient in base - base substitution , single - base insertion , and single - base deletion mismatch repair as well as double - stranded dna break repair . genomic sequencing allows identication of patients with targetable mutations who may benet from currently available treatments , which are increasing rapidly.73 this is particularly important for patients predicted to have poor outcomes with standard treatment and limited access to clinical trials . novel treatment approaches in the rst - line setting are needed . 
morgan honoraria : medscape , pharmacy times continuing education travel , accommodations , expenses : medscape , pharmacy times continuing education simon khagi research funding : lambda technologies no other potential conicts of interest were reported . acknowledgment we acknowledge jason merker , md , phd ; william kim , md ; shetal patel md , phd ; amber cipriani , pharmd ; and ashlynn messmore , ms , for their contributions to the university of north carolina multidisciplinary mtb . we also acknowledge carlos zamora , md , phd , for review of the radiographic images and scott tomlins , md , phd , co - founder and chief medical ofcer of strata oncology , for providing descriptions of the sequencing methodology . 
we thank the patient for allowing us to share a part of her story . references stupp r , mason wp , van den bent mj , et al : radiotherapy plus concomitant and adjuvant temozolomide for glioblastoma . 
n engl j med 352 : 987 - 996 , 2005 kreth fw , thon n , simon m , et al : gross total but not incomplete resection of glioblastoma prolongs survival in the era of radiochemotherapy . 
n engl j med 360 : 765 - 773 , 2009 chalmers aj , short s , watts c , et al : phase i clinical trials evaluating olaparib in combination with radiotherapy ( rt ) and / or temozolomide ( tmz ) in glioblastoma patients : results of oparatic and paradigm phase i and early results of paradigm - 2 . 
j clin oncol 36 , 2018 ( suppl ; abstr 2018 ) fulton b , short sc , james a , et al : paradigm - 2 : two parallel phase i studies of olaparib and radiotherapy or olaparib and radiotherapy plus temozolomide in patients with newly diagnosed glioblastoma , with treatment stratied by mgmt status . 
halford se , cruickshank g , dunn l , et al : results of the oparatic trial : a phase i dose escalation study of olaparib in combination with temozolomide ( tmz ) in patients with relapsed glioblastoma ( gbm )  . 
j clin oncol 35 , 2017 ( suppl ; abstr 2022 ) stupp r , taillibert s , kanner a , et al : effect of tumor - treating elds plus maintenance temozolomide vs maintenance temozolomide alone on survival in patients with glioblastoma : a randomized clinical trial . 
jama 318 : 2306 - 2316 , 2017 edelmann w , yang k , umar a , et al : mutation in the mismatch repair gene msh6 causes cancer susceptibility . 
cahill dp , levine kk , betensky ra , et al : loss of the mismatch repair protein msh6 in human glioblastomas is associated with tumor progression during temozolomide treatment . 
nguyen sa , stechishin od , luchman ha , et al : novel msh6 mutations in treatment - nave glioblastoma and anaplastic oligodendroglioma contribute to temozolomide resistance independently of mgmt promoter methylation . 
liu l , markowitz s , gerson sl : mismatch repair mutations override alkyltransferase in conferring resistance to temozolomide but not to 1 , 3 - bis ( 2 - chloroethyl ) 1068 , 2008 [ erratum : nature 494 : 506 , 2013 ] nitrosourea . 
pepponi r , marra g , fuggetta mp , et al : the effect of o6 - alkylguanine - dna alkyltransferase and mismatch repair activities on the sensitivity of human melanoma cells to temozolomide , 1 , 3 - bis ( 2 - chloroethyl ) 1 - nitrosourea , and cisplatj pharmacol exp ther 304 : 661 - 668 , 2003 19 . 
hochhauser d , glynne - jones r , potter v , et al : a phase ii study of temozolomide in patients with advanced aerodigestive tract and colorectal cancers and methylation of the o6 - methylguanine - dna methyltransferase promoter . 
aquilina g , ceccotti s , martinelli s , et al : n - ( 2 - chloroethyl ) - n ( cid : 2 ) - cyclohexyl - n - nitrosourea sensitivity in mismatch repair - defective human cells . 
stark am , doukas a , hugo hh , et al : the expression of mismatch repair proteins mlh1 , msh2 and msh6 correlates with the ki67 proliferation index and survival in patients with recurrent glioblastoma . 
koi m , umar a , chauhan dp , et al : human chromosome 3 corrects mismatch repair deciency and microsatellite instability and reduces n - methyl - n ( cid : 2 ) - nitro - nnitrosoguanidine tolerance in colon tumor cells with homozygous hmlh1 mutation . 
curtin nj , wang lz , yiakouvaki a , et al : novel poly ( adp - ribose ) polymerase - 1 inhibitor , ag14361 , restores sensitivity to temozolomide in mismatch repairdecient cells . 
yan t , schupp je , hwang hs , et al : loss of dna mismatch repair imparts defective cdc2 signaling and g ( 2 ) arrest responses without altering survival after ionizing radiation . 
gylling ah , nieminen tt , abdel - rahman wm , et al : differential cancer predisposition in lynch syndrome : insights from molecular analysis of brain and urinary 30 . 
trabucco se , gowen k , maund sl , et al : a novel next - generation sequencing approach to detecting microsatellite instability and pan - tumor characterization of 1000 microsatellite instability - high cases in 67 , 000 patient samples . 
dudley b , brand re , thull d , et al : germline mlh1 mutations are frequently identied in lynch syndrome patients with colorectal and endometrial carcinoma demonstrating isolated loss of pms2 immunohistochemical expression . 
am j surg pathol 39 : 1114 - 1120 , 2015 iv ady g , madar l , dzsudzs ak e , et al : analytical parameters and validation of homopolymer detection in a pyrosequencing - based next generation sequencing systebmc genomics 19 : 158 , 2018 36 . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
int j radiat oncol biol phys 50 : 511 - 523 , 2001 19 : 3189 - 3200 , 2013 18 : 1899 - 1908 , 2019 jiang h , reinhardt hc , bartkova j , et al : the combined status of atm and p53 link tumor development with therapeutic response . 
tchelebi l , ashamalla h , graves p : mutant p53 and the response to chemotherapy and radiation , in deb s , deb s ( eds ) : mutant p53 and mdm2 in cancer . subcellular biochemistry , volume 85 . 
salem m , grothey a , kim e , et al : impact of mlh1 , pms2 , msh2 , and msh6 alterations on tumor mutation burden ( tmb ) and pd - l1 expression in 1 , 057 microsatellite instability - high ( msi - h ) tumors . 
tentori l , leonetti c , scarsella m , et al : systemic administration of gpi 15427 , a novel poly ( adp - ribose ) polymerase - 1 inhibitor , increases the antitumor activity of temozolomide against intracranial melanoma , glioma , lymphoma . 
boulton s , pemberton lc , porteous jk , et al : potentiation of temozolomide - induced cytotoxicity : a comparative study of the biological effects of poly ( adpribose ) polymerase inhibitors . 
delaney ca , wang lz , kyle s , et al : potentiation of temozolomide and topotecan growth inhibition and cytotoxicity by novel poly ( adenosine diphosphoribose ) polymerase inhibitors in a panel of human tumor cell lines . 
miknyoczki sj , jones - bolin s , pritchard s , et al : chemopotentiation of temozolomide , irinotecan , and cisplatin activity by cep - 6800 , a poly ( adp - ribose ) base excision repair . 
clarke mj , mulligan ea , grogan pt , et al : effective sensitization of temozolomide by abt - 888 is lost with development of temozolomide resistance in glioblastoma xenograft lines . 
lesueur p , lequesne j , grellard jm , et al : phase i / iia study of concomitant radiotherapy with olaparib and temozolomide in unresectable or partially resectable glioblastoma : ola - tmz - rte - 01 trial protocol . 
 translating in vivo metabolomic analysis of succinate dehydrogenasedeficient tumors into clinical utility purpose mutations in the mitochondrial enzyme succinate dehydrogenase ( sdh ) subunit genes are associated with a wide spectrum of tumors , including pheochromocytomas and paragangliomas , gi stromal tumors , renal cell carcinomas , and pituitary adenomas . 
our aim was to investigate the potential clinical applications of proton - 1 magnetic resonance spectroscopy ( 1h - mrs ) in a range of suspected sdh related tumors . patients and methods fifteen patients were recruited to this study . 
sequential imaging in a patient with a metastatic abdominal paraganglioma demonstrated loss of the succinate peak after four cycles of [ 177lu ] dotatate , with a corresponding biochemical response in normetanephrine . conclusion this study has demonstrated the translation into clinical practice of in vivo metabolomic analysis using 1h - mrs in patients with sdh - deficient tumors . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the succinate dehydrogenase ( sdh ) enzyme is composed of four subunits ( a to d ) and plays a key role in the krebs cycle and oxidative phos phorylation.1 in the past two decades , germ line mutations in the genes encoding the four sdh subunits ( sdha , sdhb , sdhc , and sdhd ) , collectively known as sdhx , have emerged as an important cause of human neoplasia and a par adigm for the role of disordered cellular meta bolism in oncogenesis.27 sdhx mutations were described initially in association with head and neck paragangliomas ( pgls ; derived from para sympathetic ganglia ) and in pheochromocytomas and pgls ( ppgls ; derived from sympathetic ganglia and often secreting catecholamines ) .2 , 3 it is now recognized that approximately 40% of patients with ppgls harbor germ line muta tions in inherited ppgl genes , and sdhx mutations comprise the most common cause of ppgl predisposition.8 in addition , germ line sdhb mutations are associated with a high risk of malignancy in ppgls.9 other tumor types associated with sdhx mutations include gi stromal tumors ( gists ) and renal cell car cinomas ( rccs ) .1013 gists are mesenchymal tumors of the gi tract and in adults are usually associated with somatic activating mutations in ruth t . 
 the kit or pdgfra gene.4 , 11 however , gists without kit or pdgfra gene mutations , 4 known as wildtype gists ( wtgists ) , account for 15% of adult and 85% of pediatric gists , and recent studies suggest that up to 88% of wtgists are sdh deficient.11 a wtgist with sdh deficiency may harbor a germ line sdhx mutation ( 75% of cases ) or an sdhc gene epi mutation with hypermethylation of the pro moter region.11 only approximately one third of patients with sdhdeficient wtgists achieve disease stabilization with imatinib therapy , 12 and the risk of metastatic disease is higher with sdhdeficient gists compared with conven tional gists.11 , 12 sdhx - associated rcc may present in patients with a personal or family his tory of ppgl or may present with an rcconly phenotype.13 finally , germ line sdhx mutations have been described in rare patients with pitu itary adenomas.10 despite recent advances in the understanding of the sdhx genes , there are many areas of unmet clinical need , including a lack of robust biomarkers to predict aggressive biologic behavior and inform clinical surveil lance and management.14 succinate has been shown to be elevated by 100fold in sdhxmutated ppgls ex vivo compared with nonsdhxmutated ppgls.15 recently , in vivo detection of succinate by mag netic resonance spectroscopy ( mrs ) was reported in two patient cohorts with sdhdeficient ppgls.16 , 17 similarly , the noninvasive detec tion of 2hydroxyglutarate with proton1 mrs ( 1hmrs ) has been demonstrated within glio mas in patients with gainoffunction mutations in another citric acid cycle enzyme , isocitrate dehydrogenase 1.18 the ability to measure succi nate in vivo has a number of important potential clinical applications , including early identifica tion of sdh deficiency , which could enable tai lored patient surveillance and management . 
suitable patients were identi fied based on sdhx germ line status , suspicious clinical phenotype ( metastatic ppgl , pgl , or wtgist ) , and / or immunohistochemistry of tumor tissue showing absent sdhb immuno staining . 
all participants provided written informed consent , and the study was approved by the cambridge south research ethics committee . mrs analysis both sage ( ge healthcare , waukesha , wi ) and lcmodel ( sprovencher.com ) 19 spectros copy analysis programs were used to recon struct , analyze , and display spectra . 
 ( c ) axial fused [ 18f ] fluorodeoxyglucose ( [ 18f ] fdg ) positron emission tomography ( pet ) / computed tomography ( ct ) image demonstrating an [ 18f ] fdgavid carotid body paraganglioma after sdh deficiency was demonstrated on proton1 mr spectroscopy ( 1hmrs )  . 
three patients had multicentric primary tumors , including patient 5 , who presented with a metastatic wtgist and was subsequently diagnosed with a 1.9cm carotid body pgl ( fig 1d ) ; patient 9 , with an abdominal pgl and a small leftsided 1.5cm carotid pgl ( fig 2b ) ; and patient 8 , with a large leftsided glomus pgl and a 2cm prolactin secreting pituitary adenoma ( data supplement )  . 
 genotype a germ line mutation in an sdhx gene was iden tified in nine ( 60% ) of 15 patients : five in sdhb ( four missense variants and one truncating vari ant ) and four in sdha ( one missense and three truncating )  . 
two additional patients were found to have somatic sdhc epimutations ( table 1 )  . 1h - mrs succinate analysis the 1hmrs characteristics of the 15 patients are listed in the data supplement . 
the liver was the most common site to be assessed ( n = 6 ) , but goodquality spectra were also obtained from a pituitary tumor ( n = 1 ) and ppgls ( n = 5 )  . 
patient 4 had a met astatic wtgist with no detectable germ line sdhx mutation and preserved sdhb protein expression in the tumor tissue ; choline was con fidently fitted on lcmodel , but no succinate was seen . 
patient 6 demonstrated a goodquality spectrum from the remnant pituitary adenoma ; choline was detected on lcmodel and sage processing , but no succinate was detected , and this finding was consistent with the preserva tion of sdhb protein expression in the pitu itary tumor by immunohistochemistry ( fig 4 )  . 
patient 12 demonstrated no reliable detection of succinate or choline because of motion artifact and a low signaltonoise ratio ( snr ) , which probably resulted from inconsistent breathing , because the voxel was at the edge of the liver . 
a metastasis on the edge of the liver was imaged in patient 14 , where again incon sistent respiration probably led to displace ment of the voxel into adjacent adipose tissue . 
 ( a ) t2weighted magnetic resonance image from patient 1 and ( b ) t1weighted image from patient 3 demonstrating liver metastases from which spectra were acquired in the locations indicated by the white arrows . 
after four cycles of treatment , a repeat 1hmrs examina tion on the same pelvic nodal metastases revealed a choline peak but no succinate peak ( fig 5c )  . 
 although the magnetic resonance imaging fea tures of the metastatic lesions were unchanged pre and posttreatment , the loss of a succi nate peak was correlated with a reduction in plasma normetanephrine levels ( from 1 , 861 to 1 , 193 pmol / l ) and tumor avidity on [ 18f ] fluo rodeoxyglucose ( [ 18f ] fdg ) positron emission tomography ( pet ) / computed tomography ( ct ; standardized uptake value : pretreatment , 16.1 ; posttreatment , 9.3 ; figs 5d to 5f )  . 
the detec tion of choline on the acquired spectra both before and after treatment indicates that tumor necrosis is unlikely to account for the absent suc cinate peak posttreatment . a sequential 1hmrs study was performed for patient 5 because of evidence of progressive disease on surveillance ct , despite treatment with a multikinase inhibitor , regorafenib . 
the results for scr were almost identical in these two patients , suggesting good test reproducibility ( data supplement )  . discussion this proofofprinciple study demonstrates that detection of a succinate peak and an increased scr was specific for a variety of sdhdeficient tumor types . 
all six tumors with a positive suc cinate peak and elevated scr were associated with a germ line sdhx mutation ( n = 4 ) or an sdhc epimutation ( n = 2 )  . 
 ( c ) succinate dehydrogenase b ( sdhb ) immunohistochemistry demonstrating preserva tion of the sdhb protein performed on a section of tumor tissue debulked from the pituitary tumor . adequate 1hmrs demonstrated preservation of sdhb expression in the tumors analyzed . 
our findings are complementary to a previous study in which 1hmrs was applied in nine patients with pgls , and succinate peaks were detected in all five with sdhx mutations but not in the four patients without mutations.16 we demonstrate for the first time to our knowledge that 1hmrs can also be used to determine the sdh status of gists and pituitary adenomas and that succinate peaks can be detected in sdhdeficient tumors with epigenetic inactivation of sdhc . 
potential diagnostic applications of this new approach include : assessing the pathoge nicity of patients with germ line sdhx variants of uncertain significance and potentially sdh related tumors ; investigating possible metastatic lesions ( eg , in the liver ) in patients with germ line sdhx mutations and primary sdhdeficient tumors ; assessing patients with multiple pri mary tumors to determine if all are sdh defi cient ; identifying patients without detectable germ line sdhx mutations who might benefit from specialist genetic investigations , such as sdhc promoter methylation status ; and assess ing sdh tumor status preoperatively , particu larly for patients with possible wtgists , because standard adjuvant treatment with imatinib has proven to be less effective in patients with sdh deficient disease.12 notably , here we use the presence of a choline signal as an internal control for viable tissue to discriminate technical failures from a negative finding . 
 this trend is the opposite of what would be expected if necrosis were artificially lowering the overall succinate levels in large tumors and therefore suggests that the method is measuring real differences in succinate , which are indepen dent of tumor size . 
 ( b ) spectra acquired before treatment illustrating succi nate accumulation at 2.4 pp ( c ) spectra ac quired after four cycles of [ 177lu ] dotatate with no detectable succinate peak at 2.4 pp ( d ) plasma metanephrine and methoxytyramine levels before and after treatment with [ 177lu ] dotatate . 
as a consequence , sdhdeficient tumors demonstrate epigenetic abnormalities and activated hypoxic gene responses , and more recently , evidence has suggested that succinate may have a paracrine effect on stromal tis sue.2022 understanding the molecular mech anisms of sdhrelated tumorigenesis provides a rationale for novel therapeutic interventions such as reversing the epigenetic abnormalities or exploiting metabolic vulnerabilities , similar to the recent discovery that tumoral 2hydroxyglutarate accumulation may increase responsiveness to olapa rib , a poly ( adpribose ) polymerase inhibitor.23 the availability of sensitive noninvasive bio markers would greatly facilitate precision medicinebased clinical trials . 
1hmrs is highly specific and allows in vivo detection of individual metabolites without the use of ionizing radiation ; however , 1hmrs is significantly less sensitive than pet , which could limit the detection of low levels of succinate , and it can be challenging to differen tiate intracellular from extracellular metabolites . 
 in the future , 1hmrs may be complemented by other techniques , such as hyperpolarized car bon13 mrs , which can increase 13mrs snr by several orders of magnitude , allowing assess ment of enzyme flux in vivo.26 we show that 1hmrs could be a valuable tool for the assessment of tumor response in the con text of radionuclide and other therapies , because alterations in succinate levels were detected despite stable appearance of the tumor diam eters . 
this important application of 1hmrs could be expanded to include other tumors with specific metabolic defects , including fuma rate hydratasedeficient tumors , 27 idh1mutant tumors , 18 and the recently identified malate dehydrogenase 2deficient tumors.28 however , important limitations of in vivo metabolomic analysis using 1hmrs were also revealed by our study ; for example , spectral quality was poor in close proximity to metal dental work , in areas adjacent to air spaces such as the lung , and in bone metastases and was susceptible to motion artifact . 
in this study , the technical failure rate was 26% , which is similar to the failure rate reported in previous studies using 1hmrs.16 importantly , no patient cases were excluded from this prospective study , with the intention that this would inform the translation of this imaging modality into clinical practice . 
on the basis of the evidence from this exploratory study , we recommend that tumors be selected for 1hmrs analysis based on the following : ideally the largest tumor deposit but at least > 2 cm in size ; tumors located close to bone or lung should be avoided ; tumors with significant necrosis or hemorrhage should be avoided ; superficial tumor deposits should be selected preferentially ; and respiratorytriggered acquisition should be used for tumors in the upper abdomen , such as hepatic metastases . although the use of 1hmrs as a diagnos tic tool is likely to be limited to specialist cen ters , the number of scan averages in our study during spectral acquisition was less than half those reported in a previous study16 ( 200 v 512 ) , without demonstrating a reduction in sensi tivity . 
furthermore , this imaging modal ity could be used to investigate other metaboli cally driven tumors . in conclusion , this study is the largest to date to our knowledge to evaluate 1hmrs in patients with sdh deficiency . 
it reveals that 1hmrs has the potential to be used as a noninvasive biomarker in the precision management of sdhdeficient disease and could have a role as a biomarker of successful treatment response . 
mclean stock and other ownership interests : veryan medical patents , royalties , other intellectual property : patent for stent design for arterial bypass graft basetti madhu no relationship to disclose benjamin g . 
challis no relationship to disclose rogier ten hoopen no relationship to disclose thomas roberts no relationship to disclose consulting or advisory role : bayer healthcare pharmaceuticals , ariad pharmaceuticals speakers bureau : pfizer travel , accommodations , expenses : pierre fabre , teva pharmaceuticals europe helen l . 
bulusu honoraria : pierre fabre kieran allinson no relationship to disclose lisa happerfield no relationship to disclose soo - mi park no relationship to disclose alison marker no relationship to disclose olivier giger stock and other ownership interests : cambridge pathology eamonn r . 
xekouki p , stratakis ca : succinate dehydrogenase ( sdhx ) mutations in pituitary tumors : could this be a new role for mitochondrial complex ii and / or krebs cycle defects ? endocr relat cancer 19 : c33c40 , 2012 7 . 
boikos sa , pappo as , killian jk , et al : molecular subtypes of kit / pdgfra wildtype gastrointestinal stromal tumors : a report from the national institutes of health gastrointestinal stromal tumor clinic . 
holdsworth ch , badawi rd , manola jb , et al : ct and pet : early prognostic indicators of response to imatinib mesylate in patients with gastrointestinal stromal tumor . 
 signicant and durable clinical response to sorafenib and radiation therapy for a patient with stage iv hepatocellular carcinoma and lrrk2 mutation linlin yang , md1 ; patrick wald , md1 ; sameek roychowdhury , md , phd1 ; anne m . 
the level was elevated to alpha fetoprotein ( afp ) 57 , 400 ng / ml , and ct - guided biopsy of the large hepatic lesion revealed stage iv hcc . 
because of radiographic concern for disease progression and invasion into the transverse colon , sorafenib was discontinued and radiation therapy was in addition , started 1 week after sorafenib was discontinued . 
the two large masses were irradiated to a dose of 40 gy in 16 fractions using a conformal radiation plan ( fig 1d )  . repeat ct scans 1 month later showed a large decrease in the size of not only the two radiated extrahepatic lesions but also the unirradiated hepatic lesions , and it was decided to restart the patient on maintenance sorafenib ( 200 mg twice daily ) 6 weeks after radiation . 
on the basis of this impressive response , sorafenib doses were held , and the patient underwent laparoscopic partial left hepatectomy of segment 4b with removal of additional primary liver and extrahepatic omental masses . 
at abdominal masses showed no residual 3 weeks after surgery , sorafenib was restarted at 200 mg twice daily but was discontinued after 2 more months because of sorafenib - related pulmonary toxicity . 
after this exceptional response , we performed next - generation sequencing of whole blood lymphocytes and tumor dna from the diagnostic biopsy specimen ( table 1 ) , which revealed mutations in lrrk2 ( k1316n ) , lrp1b ( v4250a , y4256c ) , tp53 ( v157insa , a nonframeshift insertion of three base pairs : cgc ) , and notch3 ( g501s )  . 
 yang et al started sorafenib 400 mg twice a day sorefenib stopped and rt delivered started maintenance sorafenib 200 mg twice a day surgery sorafenib 200 mg twice a day sorafenib discontinued 9 10 11 12 14 47 52 time ( months ) 180000 160000 140000 120000 100000 80000 60000 40000 20000 fig 1 . 
 ( right ) disappearance of intrahepatic lesions noted in fig 1b . lrrk2 we turned our attention to lrrk2 , a gene that has been linked to the pathogenesis of parkinson disease with known roles in the antioxidant response.2 , 3 ionizing radiation generates reactive oxygen species ( ros ) , which are critical for the ability of radiation to promote tumor cell kill through dna damage . 
the degree of ros generation correlates with serum levels of advanced oxidation protein products and clinical effectiveness in sorafenib - treated patients with hcc.4 because ros are in the response to both radiation and sorafenib , critical through promotion of dna damage , we hypothesized that this mutation in lrrk2 could alter the response to both therapies . 
we observed adequate transfected wild - type ( wt ) and k1316n expression of leucine - rich repeat kinase 2 ( lrrk2 ) protein in multiple cell lines ( appendix fig a3 for rna and protein ; primer sequences intable a1 )  . 
we also tested genetic silencing of lrrk2 with small interfering rna ( sirna ) and found that lrrk2 depletion likewise sensitized hcc cells to sorafenib ( figs 2c and 2d )  . 
in addition , we found that expression of the lrrk2 k1316n mutation in both hela and hepg2 cells resulted in notable radiation sensitization in radiation clonogenic assays , whereas wt lrrk2 had no radiosensitizing effects ( figs 2e and 2f )  . because of the previously identied role of lrrk2 in ros , we assessed whether wt lrrk2 or the k1316n mutant altered levels of ros in cancer cells . 
 ( a , b ) overexpression of lrrk2 k1316n signicantly increases sorafenib sensitivity on hcc cells . ( c , d ) genetic silencing of lrrk2 with sirna sensitizes hcc cells to sorafenib treatment . 
sorafenib sensitivity on hcc cells was determined by alamarblue assay ( thermofisher , waltham , ma ) 72 hours after transfection , whereas radiation sensitivity was determined by clonogenic assay . 
similarly , we found that lrrk2 k1316n greatly increased hydrogen peroxide ( h2o2 ) levels , another known mediator of ros damage , and this increase was reversed by treatment of cells with ebselen , an h2o2 scavenger ( figs 3d , 3e , and 3f )  . 
finally , the addition of the superoxide scavenger tiron greatly attenuated the radiation sensitivity induced by lrrk2 k1316n in radiation clonogenic assays ( figs 4a and 4b )  . discussion in this case of a patient with an exceptional response to sorafenib and radiation , we identied a novel lrrk2 k1316n mutation that induced sorafenib and radiation sensitivity in various hcc cell lines , consistent with our clinical observations . 
 ( * ) signicant difference from corresponding tiron or ebselen treatment group ; ( ) signicant difference from empty vector ; ( ) signicant difference from lrrk2 wild type ( wt )  . 
hepg2 and hela cells transfected with wild - type ( wt ) lrrk2 and lrrk2 k1316n were preincubated with dmso or tiron ( 1 mm ) and then exposed to 4 gy of radiation . 
thus , we hypothesize that this lrrk2 mutation increases lrrk2 kinase activity and enhances sorafenib and radiation - induced apoptotic cell death signaling via increased p53 and p21 activity . our in vitro data suggest that this lrrk2 k1316n mutation like other canonical lrrk2 mutations increases ros , observed in parkinson disease . 
thus , another potential hypothesis to explain the radiosensitivity of disease in this patient is that increased lrrk2 kinase activity in lrrk2 mutants may render cells more susceptible to oxidative stress imparted by radiotherapy through creation of ros , such as oxygen free radicals.6 multiple publications show that lrrk2 mutations induce synergistic or additive cell killing in the presence of oxidative stress.7 , 8 taken together , the presence of increased oxidative stress imparted by an activating lrrk2 mutation could prime tumor cells to increased radiation - mediated cell death . the near - complete pathologic response and more than 4 - year disease - free interval since completion of all therapy are remarkable results from a low to moderate dose of radiation and a drug that rarely induces complete response ( 0% in the sharp trial )  . 
it is also interesting to note the dramatic radiographic responses seen in lesions that were not directly radiated , which suggests an abscopal effect from the combination of sorafenib and radiotherapy . 
certainly , we cannot overlook that the dramatic responses observed may have been due in part to the development of an antitumor immune response , which has been previously attributed to both sorafenib and radiation.9 , 10 indeed , the radiologic progression initially noted after sorafenib started may be related to pseudoprogression and development of an early immune response or apoptosis / necrosis of the tumor , despite the observation of the most dramatic clinical and radiographic response with postradiation sorafenib . in conclusion , these data support a role for a novel , previously unidentied lrrk2 mutation that promotes sorafenib and radiation sensitivity through an ros - dependent mechanism . in addition , the combination of radiation and sorafenib also may have induced an antitumor immune response . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . patrick wald employment : riverside radiation oncology sameek roychowdhury stock and other ownership interests : johnson & johnson ( i ) consulting or advisory role : incyte , abbvie , qed therapeutics research funding : takeda , ignyte anne m . 
noonan consulting or advisory role : helsinn healthcare no other potential conicts of interest were reported . references llovet jm , ricci s , mazzaferro v , et al : sorafenib in advanced hepatocellular carcinoma . 
n engl j med 359 : 378 - 390 , 2008 goldwurm s , di fonzo a , simons ej , et al : the g6055a ( g2019s ) mutation in lrrk2 is frequent in both early and late onset parkinsons disease and originates from a common ancestor . 
j med genet 42 : e65 , 2005 loefer da , klaver ac , coffey mp , et al : increased oxidative stress markers in cerebrospinal uid from healthy subjects with parkinsons diseaseassociated lrrk2 gene mutations . 
front aging neurosci 9 : 89 , 2017 coriat r , nicco c , ch ereau c , et al : sorafenib - induced hepatocellular carcinoma cell death depends on reactive oxygen species production in vitro and in vivo . mol cancer ther 11 : 2284 - 2293 , 2012 5 . 
ho dh , kim h , kim j , et al : leucine - rich repeat kinase 2 ( lrrk2 ) phosphorylates p53 and induces p21 ( waf1 / cip1 ) expression . 
gene 532 : 18 - 23 , 2013 yang d , li t , liu z , et al : lrrk2 kinase activity mediates toxic interactions between genetic mutation and oxidative stress in a drosophila model : suppression by curcumneurobiol dis 47 : 385 - 392 , 2012 8 . 
ho v , lim ts , lee j , et al : tlr3 agonist and sorafenib combinatorial therapy promotes immune activation and controls hepatocellular carcinoma progression . oncotarget 6 : 27252 - 27266 , 2015 10 . 
stable post - operative changes are seen , and there is no evidence of disease . 1 / 30 / 14 : afp decrease to 26 , 343 ng / ml but radiographic progression seen . sorafenib radiation surveillance 2 / 17 / 14 - 3 / 10 / 14 : received 40 gy in 16 fractions . 4 / 21 / 14 - 6 / 20 / 14 : sorafenib restarted at 200 mg twice daily . 
quantitative polymerase chain reaction ( qpcr ) analysis ( a ) and western blot ( b ) conrmed overexpression of wild - type ( wt ) lrrk2 and lrrk2 - k1316n ( mutant ) on four cell lines 72 hours after transfection . 
finally , we characterize the in vitro use of entrectinib against a common alk fusion gatekeeper resistance mutation . methods genomic profiling we performed broad , hybrid capturebased next - generation sequencing using the integrated mutational profiling of actionable cancer targets assay and hisequation 2500 ( illumina , san diego , ca ) .14 alk immunohistochemistry and fluorescence in situ hybridization alk immunohistochemistry was performed using the ventana alk ( d5f3 ) cdx assay ( ventana medical systems , tucson , az )  . 
response , assessed by response evaluation criteria in solid tumors ( recist ) version 1.1 , was monitored by computed tomography ( ct ) imaging performed at baseline , 4 weeks after treatment initiation , and approximately every 8 weeks thereafter.15 treatment was administered until the patient experienced disease progression or unacceptable toxicity . 
permission to publish the patients case was obtained from his health care proxy . generation of engineered ba / f3 cells expressing vcl - alk fusion proteins cdnas that encode vcl - alk and vcl - alk l1196m fusion proteins were inserted into lentiviral vector pvlpuro - ef1a - mcs ( biosettia , san diego , ca )  . 
 transduced ba / f3 cells were selected in puromycin in rpmi 1640 media that contained 10% fetal bovine serum and 10 ng / ml mouse il - 3 ( thermo fisher scientific , waltham , ma ) for 2 weeks . 
 antiproliferative activities of entrectinib and crizotinib in engineered ba / f3 cells results cells seeded at 5 , 000 cells per well in 96 - well plates ( corning , corning , ny ) were treated with serial dilutions of entrectinib ( ignyta , san diego , ca ) and crizotinib ( selleckchem , houston , tx ) added in duplicate to the wells . 
data are averaged from at least two independent experiments and with an r2 of more than 0.9. western blot analysis ten million cells were treated with drug at the indicated concentrations for 2 hours , washed with phosphate - buffered saline , and lysed in 1 radioimmunoprecipitation assay buffer ( emd millipore , billerica , ma ) with benzonase , protease inhibitor , and phosphatase inhibitor cocktails ( emd millipore )  . 
exons 1 to 16 of vcl are fused to exons 20 to 26 of alk , which include the kinase domain . tpm3 eml4 rad51ap2 eml4 22 exons 26 exons exon 1 exon 16 exon 20 - 26 identification of rccs harboring alk fusions a total of 561 samples from 517 patients with rcc were sequenced using broad , hybrid capture based next - generation sequencing ( integrated mutational profiling of actionable cancer targets assay ) .14 , 16 , 17 three ( 0.6% ) of 517 patients with renal cell cancer had tumors that harbored alk fusions . in renal cell cancer , several fusion partners with alk have been previously identified , including vcl , tpm3 , and eml412 , 18 , 19 ( fig 1a )  . 
 the three alk fusions identified in our data set are represented in figure 1b and consist of unclassified - type rcc harboring an vcl - alk fusion developing in a patient with sickle cell trait , chromophobe - type rcc harboring an rad51ap2 - alk fusion , and unclassified - type rcc with an eml4 - alk fusion ( table 1 )  . of these three patients , one was eligible for therapy with a targeted agent against alk , as described below . 
he underwent a right radical nephrectomy , revealing a stage iii ( pt3an1 ) high - grade ( nuclear grade iv ) rcc with rhabdoid and pleomorphic features and nine of 23 positive lymph nodes . 
ct scan 2 months later demonstrated no evidence of recurrence . next - generation sequencing of the primary tumor identified a vcl - alk translocation generating a fusion between exon 16 of vcl and exon 20 of alk ( fig 1c )  . 
clinicopathologic characteristics and therapeutic interventions in patients with alk fusionpositive renal cell carcinoma case age at diagnosis , years pathology fusion additional alterations systemic therapy received vcl - alk none entrectinib renal cell carcinoma , unclassified type renal cell carcinoma , chromophobe type alkrad51ap2 * tert promoter variant pazopanib malt1 h257r nivolumab + bevacizumab nivolumab + lenvatinib lenvatinib + everolimus eml4 - alk tp53 d257y everolimus + bevacizumab renal cell carcinoma , unclassified type erbb4 t194s mst1r f803s dot1l g1358v nivolumab cabozantib abbreviations : alk , anaplastic lymphoma kinase ; f , female ; m ; male . * next - generation sequencing performed on the sarcomatous component of a metastasis . tumor and the age of the patient , hemoglobin electrophoresis was performed , discovering the presence of sickle cell trait.20 entrectinib demonstrates superior in vitro target inhibition and antitumor effect compared with crizotinib twelve months after nephrectomy , surveillance imaging demonstrated confluent lymphadenopathy in the right retrocrural space and an enlarged left superior mediastinal metastatic node . 
given evidence that suggested activity of entrectinib , a multikinase inhibitor of alk , ros1 , trka , trkb , and trkc , against common alk resistance mutations and improved cns penetration compared with crizotinib , the patient enrolled in a clinical trial of entrectinib ( rxdx - 101 ; clinicaltrials.gov identifier : nct02097810 ) .21 four weeks after commencing entrectinib 600 mg per day , a ct scan demonstrated a 31.4% decrease in disease , or partial response . 
the patient maintained excellent performance status throughout treatment , tolerating entrectinib well with the exception of grade 1 peripheral lower extremity edema and grade 2 weight gahis response to entrectinib continued for 19 months , after which imaging revealed radiographic disease progression with increased mediastinal adenopathy , which led to the discontinuation of entrectinib . we interrogated the activity of entrectinib against alk fusions and its common resistance mutations with ba / f3 cell lines that were engineered to overexpress vcl - alk and vclalk l1196m fusion proteins . 
vcl - alk l1196m , a key gatekeeper mutation in the atp binding pocket , confers resistance to crizotinib.22 , 23 for ba / f3 cells that harbor the vcl - alk fusion , entrectinib was more potent than crizotinib ( ic50 = 90.8 nm for entrectinib ; ic50 = 253.0 nm for crizotinib ; fig 3a )  . 
entrectinib and crizotinib both resulted in reduced levels of phospho - alk and the inhibition of phosphorylation of downstream targets , phospholipase c , extracellular signalregulated kinase , and signal transducer and activator of transcription 3 ( fig 3b )  . 
the introduction of the alk l1196m mutation to the vcl - alk construct ( ba / f3 - vcl - alk l1196m ) conferred significantly reduced sensitivity to crizotinib , with an ic50 proliferation value of more than 1 , 000 nm ; however , ba / f3 - vcl - alk l1196m cells remained sensitive to entrectinib , with an ic50 value that was only modestly increased compared with that of ba / f3 - vcl - alk cells ( ic50 = 111.9 nm ; fig 3a )  . 
recently , response to alectinib was reported in patients with metastatic papillary rcc.24 the case detailed here of durable clinical response in a patient with rccadditionally underscores the utility of alk inhibition in alk - rearranged rcc and the potential of targeting alk fusions irrespective of histology . large - scale sequencing efforts have increased the ability to identify alk fusions . 
given their low frequency , single analyte testing for specific alterations is impractical ; however , the increasingly widespread availability of multiplexed next - generation sequencing enhances the feasibility of detecting targetable fusions . 
screening efforts can lead to the detection of other actionable mutations in rcc , such as alterations that involve met , pten , bap1 , mtor , pik3ca , and birc7.25 , 26 clinical outcomes for nonclear - cell rcc ( ncrcc ) remain poor compared with clear - cell rcc . 
despite the small proportion of patients with alk fusion positive rcc , failure to screen in this patient would have prevented the delivery of a well tolerated therapy with a durable response that lasted 19 months . 
 ( b ) treatment of wt ba / f3 vcl - alk and resistant baf3 vcl - alk l1196m cell lines with entrectinib leads to more complete inhibition of downstream targets phosphophospholipase c ( plc ) and phosphosignal transducer and activator of transcription 3 ( stat3 ) compared with crizotinib . 
erk , extracellular regulated kinase . observed in other fusions led to the opening of a multicenter , phase ii basket trial of entrectinib ( clinicaltrials.gov identifier : nct02568267 )  . ultimately , as with this patient , resistance to therapy almost inevitably develops . 
 arcila , hikmat al - ahmadie , gary li , alexander drilon roopal patel employment : ignyta provision of study materials or patients : chung - han lee stock and other ownership interests : ignyta collection and assembly of data : jessica j . 
tao no relationship to disclose ge wei stock and other ownership interests : ignyta , halozyme research funding : ignyta patents , royalties , other intellectual property : ignyta , halozyme travel , accommodations , expenses : ignyta patrick fagan employment : ignyta stock and other ownership interests : ignyta travel , accommodations , expenses : ignyta xueli hao no relationship to disclose julia a . 
arcila consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe , raindance technologies hikmat al - ahmadie consulting or advisory role : bristol - myers squibb , emd serono chung - han lee consulting or advisory role : exelixis , eisai research funding : pfizer ( inst ) , eisai ( inst ) , bristol - myers squibb ( inst ) , calithera biosciences ( inst ) travel , accommodations , expenses : eisai gary li employment : ignyta alexander drilon consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pfizer , blueprint medicines , genentech , takeda , helsinn therapeutics , beigene affiliations jessica j . 
arcila , hikmat al - ahmadie , chung - han lee , and alexander drilon , memorial sloan kettering cancer center ; alexander drilon , weill cornell medical center , new york , ny ; ge wei , roopal patel , patrick fagan , and gary li , ignyta , san diego , ca ; xueli hao , st louis pathology associates , mercy hospital , st louis , mo ; and julia a . 
cui jj , tran - dub m , shen h , et al : structure based drug design of crizotinib ( pf - 02341066 ) , a potent and selective dual inhibitor of mesenchymal - epithelial transition factor ( c - met ) kinase and anaplastic lymphoma kinase ( alk )  . 
lin e , li l , guan y , et al : exon array profiling detects eml4 - alk fusion in breast , colorectal , and nonsmall - cell lung cancers . 
sugawara e , togashi y , kuroda n , et al : identification of anaplastic lymphoma kinase fusions in renal cancer : large - scale immunohistochemical screening by the intercalated antibody - enhanced polymer method . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
hyman dm , solit db , arcila me , et al : precision medicine at memorial sloan kettering cancer center : clinical next - generation sequencing enabling next - generation targeted therapy trials . 
debelenko lv , raimondi sc , daw n , et al : renal cell carcinoma with novel vcl - alk fusion : new representative of alk - associated tumor spectrumod pathol 24 : 430 - 442 , 2011 19 . 
smith ne , deyrup at , mario - enriquez a , et al : vcl - alk renal cell carcinoma in children with sickle - cell trait : the eighth sickle - cell nephropathy ? am j surg pathol 38 : 858 - 863 , 2014 21 . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multitargeted pan - trk , ros1 , and alk inhibitor entrectinib : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . 
lee j - l , ahn j - h , lim hy , et al : multicenter phase ii study of sunitinib in patients with non clear cell renal cell carcinoma . 
tannir nm , jonasch e , albiges l , et al : everolimus versus sunitinib prospective evaluation in metastatic nonclear cell renal cell carcinoma ( espn ) : a randomized multicenter phase 2 trial . 
ardini e , menichincheri m , banfi p , et al : entrectinib , a pan - trk , ros1 , and alk inhibitor with activity in multiple molecularly defined cancer indications . 
 o detection of circulating tumor dna in patients with leiomyosarcoma with progressive disease purpose leiomyosarcoma ( lms ) is a soft - tissue sarcoma characterized by multiple copy number alterations ( cnas ) and without common recurrent single - nucleotide variants . 
 we evaluated the feasibility of detecting circulating tumor dna ( ctdna ) with next generation sequencing in a cohort of patients with lms whose tumor burden ranged from no evidence of disease to metastatic progressive disease . patients and methods we evaluated cell - free dna in plasma samples and paired genomic dna from resected tumors from patients with lms by ultra - low passage whole genome sequencing . 
sequencing reads were aligned to the human genome and cnas that were identified in cell - free dna and tumor dna by ichorcna software to determine the presence of ctdna . 
clinical data were reviewed to assess disease burden and clinicopathologic features . results we identified lms ctdna in 11 ( 69% ) of 16 patients with disease progression and total tumor burden greater than 5 csixteen patients with stable disease or low disease burden at the time of blood draw were found to have no detectable ctdna . 
ctdna levels declined after resection of progressive disease in one case and became detectable upon disease relapse in another individual patient . conclusion these results suggest that ctdna , assayed by a widely available sequencing approach , may be useful as a biomarker for a subset of patients with uterine and extrauterine lms . 
2018 by american society of clinical oncology introduction leiomyosarcoma ( lms ) is a malignant neoplasm derived from smooth muscle that represents one of the most common subtypes of soft - tissue sarcoma.1 , 2 although the majority of lms cases are sporadic , predisposing factors include li fraumeni syndrome , hereditary retinoblastoma , and radiation exposure.3 , 4 there are no oncogenic single - nucleotide variants ( snvs ) that characterize lms , although loss of tumor suppressors , including tp53 , rb1 , and pten , are commonly observed , as are multiple copy number alterations ( cnas ) .5 - 8 lms is frequently a clinically aggressive disease , and patients are at high risk for local and metastatic relapse after initial complete resection.9 , 10 efforts to improve outcomes for patients would benefit from more reliable indicators of high - risk disease and biomarkers of response to therapy . detection of circulating tumor dna ( ctdna ) has emerged as a new approach for identifying oncogenic mutations , measuring disease burden , clinical prognostication , and assessing tumor response to therapy.11 , 12 most ctdna assays matthew l . 
 have been developed to detect snvs that are highly recurrent in many types of carcinomas.13 although the lack of recurrent snvs in lms limits efforts at targeted sequencing , the numerous cnas that are characteristic of this disease represent an ideal target for detection . 
 a next - generation sequencing approach using ultra - low passage whole - genome sequencing ( ulp - wgs ) can detect cnas in cell - free dna , which indicates the tumor fraction of ctdna present in blood.14 , 15 previous studies have shown that ctdna can be detected in cell - free dna samples that are sequenced at a minimum coverage of 0.1 across the whole genome.14 sequencing for ulp - wgs uses the standard illumina next - generation sequencing platform without modifications or special adaptions ( illumina , san diego , ca )  . 
the ichorcna algorithm is used to detect megabase - scale cnas from ulp - wgs data in which ctdna comprise as little as 3% of the total cell - free dna extracted from a plasma sample.14 in the current study , we evaluated plasma from patients with uterine and extrauterine lms for the presence of ctdna using ulp - wgs . 
paired resected tumors from each patient were also sequenced when available ( 29 of 30 patients ) , which enabled the identification and comparison of cnas between primary tumors and ctdna . 
high - molecular - weight dna contamination of cell - free dna was determined by bioanalyzer ( agilent technologies , santa clara , ca ) and size selection was performed if necessary ( ampure xp beads ; beckman coulter , brea , ca )  . 
up to 40 ng of cell - free dna , 100 ng of dna from fresh frozen tissue , and 200 ng of dna from ffpe tissue were used for kapa hyper library preparation ( kapa biosystems , wilmington , ma )  . 
 after bioruptor sonication ( diagenode ) of formaldehyde - fixed fresh frozen sample , with library preparation using a thruplex dna sequencing kit ( rubicon ) and sequencing on an illumina nextseq 500 . 
this higher sequencing coverage did not alter downstream analyses or data interpretation . sequencing results were demultiplexed , aligned , and processed using picard , burrows - wheeler alignment tool , 17 and genome analysis toolkit.18 , 19 to assess for cnas in tumor and cellfree dna and determine tumor fraction or percentage of ctdna in cell - free dna , we used ichorcna software14 with manual curation of results as necessary to confirm tumor percentages . 
previous studies have demonstrated that this technique can be used to identify and quantitate ctdna that constitutes as little as 3% of the cell - free dna in a sample.14 copy number analysis copy number segments and estimates of tumor fraction and ploidy were generated by ichorcna . 
this analysis was performed separately on tumor resection samples , including the eight samples for which plasma was not available , and on plasma samples that were positive for detectable levels of ctdna . statistical analysis group comparisons between patients with lms with active or indolent disease at the time of plasma collection was performed by nonparametric mann - whitney test , and we performed pearson correlation coefficient between tumor fraction or cell - free dna and tumor burden using graphpad prism ( version 7.0 ; graphpad software , la jolla , ca )  . 
one was added to integer values before log2 transformation to generate non - negative values for data representation . results detection of lms ctdna we retrospectively identified 30 patients who were diagnosed with metastatic lms who had plasma banking performed at variable time points in their treatment history between january 2007 and november 2017 . 
median age at diagnosis was 51 years , most patients were female , the most common primary tumor location was the uterus ( n = 16 ) followed by the retroperitoneum ( n = 8 ) , and most tumors were originally of intermediate or high grade ( table 1 )  . 
twenty - nine of 30 patients had a tumor resection sample available for comparison with cell - free dna . in review of clinical data at the time of plasma banking , the cases could be divided into active disease or indolent disease groups on the basis of tumor volume and evidence of disease progression . 
the active disease group consisted of 16 patients and was defined by having a total tumor burden greater than 5 cm in greatest diameter and progressive disease at the time of blood draw on the basis of imaging or clinical determination . 
in contrast , 16 patients in the indolent disease group had stable disease at the time of blood draw and / or tumor burden less than 5 camong the active disease group , 11 ( 69% ) of 16 patients had detectible ctdna , including patients with both uterine and extrauterine primary tumors . 
none of the samples obtained from the indolent disease group had detectible ctdna ( fig 1a )  . when comparing the amount of ctdna measured as a fraction of total cell - free dna in the plasma sample to the volume of tumor burden reported by computed tomography scan , there was a significant association between higher ctdna levels and increasing tumor burden ( fig 1b )  . 
 abbreviations : a , abdomen ; b , bone ; c , chest ; ctdna , circulating tumor dna ; f , female ; hpf , high - power field ; l , liver ; m , male ; na , not available ( data not reported during pathology review ) ; p , pelvis ; st , soft tissue , including subcutaneous , muscle , and paraspinal locations . cna concordance between lms tumors and ctdna in the 11 plasma samples with detectible levels of ctdna , there was a high concordance of cnas between the tumor sample and ctdna ( figs 2a - 2d ) , with blood collection occurring less than 2 years apart from resection of the matched tumor specimen . 
the active disease group consists of patients with tumors > 5 cm in size and with progressive disease at the time of blood draw as indicated by computed tomography ( ct ) scan or clinical report . 
labels indicate the active disease subgroup ( red ) with tumor size > 5 cm and progressive disease ( n = 16 ) , or indolent disease subgroups ( gray ) with tumor size > 5 cm and stable disease ( n = 2 , diamond ) , tumor size < 5 cm and progressive disease ( n = 4 ; triangle ) , and tumor size < 5 cm and stable disease ( n = 10 ; circle )  . 
overall , recurrent cnas from tumors in this cohort are remarkably similar to those found in prior studies.5 , 8 the most significantly amplified genomic region was found on chromosome 17p , which includes the transcriptional regulator myocd ( copy gained in 20 of 37 tumors )  . 
this gene has previously been reported as significantly amplified in lms and is associated with smooth muscle differentiation.22 additional putative oncogenic and lms associated genes that were recurrently amplified include hdgf in 20 , myc in 14 , cthrc1 in 17 , tnfrsf19 in 10 , and myh2 in 16 of 37 tumors ( fig 3a )  . 
copy gains in these genes were also observed in a portion of cell - free dna samples with detectable ctdna ( myocd in four , hdgf in six , myc in eight , cthrc1 in nine , tnfrsf19 in three , and myh2 in four of 11 ctdna - positive samples ) ; however , the number of evaluable samples was too small for any copy gains of these genes to reach statistical significance ( fig 3b )  . 
from tumor samples , recurrent deletions in tumor suppressors were found , which are characteristic of lms , 5 , 8 , 23 including pten deletions in 27 , rb1 in 27 , and tp53 in 11 of 37 tumors profiled ( fig 3c )  . 
deletions that involved these genes were also detected in ctdna ( pten in eight , rb1 in six , and tp53 in two of 11 ctdna - positive samples ) , but sample size was too small for many of these deletions to reach significance ( fig 3d )  . 
 thus , ulp - wgs is capable of detecting recurrent cnas characteristic of lms , and these methods may be helpful in identifying genelevel cnas in ctdna . ctdna longitudinally correlates with disease status to determine whether ctdna levels change in agreement with longitudinal disease status , we evaluated serial plasma samples in two patients after either resection of localized lms or with disease recurrence after surgery . 
in contrast , in the patient with disease recurrence 32 months after surgical resection , cell - free dna tumor fraction increased from undetectable postoperatively to detectable at the time of disease recurrence ( fig 4b )  . 
 ( a - e ) copy number plots generated from ultra - low passage whole - genome sequencing of five representative tumor surgical ( left panels ) and plasma ( right panels ) sample pairs . 
tumor fraction is indicated for each plot . discussion in the current study , we analyzed cell - free dna from the plasma of patients with lms for evidence of ctdna . 
a significant association between tumor burden and the amount of ctdna was identified , which suggests that larger and actively growing tumors are more likely to release tumor dna into circulation . 
 ( a - d ) gistic2.0 analysis identifying recurrent focal amplified ( a and b ) and deleted ( c and d ) regions in lms tumors ( n = 37 ; left panels ) and cell - free dna samples with detectable circulating tumor dna ( n = 11 ; right panels )  . 
the green line indicates an fdr of 0.25. tumor cell - free dna amplifications tnfrsf19 myocd myh2 amplifications cthrc1 6 7 8 9 10 chromosome 12 14 16 18 20 x 12 14 16 18 20 6 7 8 9 10 chromosome deletions hdlbp deletions cdkn2aip brca2 tp53 pten tsc1 ypel3 12 14 16 18 20 x 12 14 16 18 20 x 6 7 8 9 10 chromosome 6 7 8 9 10 chromosome 10 - 1 0.25 10 - 2 10 - 1 0.25 less than 5 cm in size , regardless of evidence of disease progression , which may represent a technologic sensitivity threshold . 
we further found that ctdna levels decline with resection of disease and increase with disease recurrence in individual patients , which indicates that these methods may be useful for supporting a diagnosis of disease recurrence or response to therapy . sequencing of snvs in cell - free dna has proven clinical utility in detecting resistance mutations to targeted therapies and directing treatment strategies.24 emerging use of whole - genome sequencing to identify and quantify cnas from tumor - derived dna circulating in patients with cancer has been evaluated in a number of cancer types.14 , 25 - 27 this noninvasive approach can be useful in the genomic characterization of malignancy and provide diagnostic and prognostic information relevant for clinical care.15 , 21 , 28 in a recent study of patients with lms , a highly customized lms - specific assay ( cancer personalized profiling by deep sequencing , or cappseq ) was designed to detect selected snvs and combined with cna analysis to identify and quantify ctdna in patients with progressive disease.29 in this study , the investigators found that approximately 20% of patients ( two of nine ) had tumors that did not have somatic events that were detectable by the assay . 
in contrast , we found that tumors from 100% of cases had cnas that were detectable by ulp - wgs , which suggests that ulp - wgs may be more broadly applicable for patients with lms . 
 the interval between surgical date and cell - free dna collection is indicated . in six of seven baseline samples of patients who were eligible for study ( 86% ) and had a sensitivity of 68% among all samples tested from their cohort . 
although these numbers are small , this suggests that capp - seq may have a higher sensitivity for ctdna , which might be expected given the deep sequencing coverage used in this assay . 
for example , our recent study in osteosarcoma demonstrated that pretreatment ctdna levels detected by ulpwgs are prognostic , 28 whereas a more sensitive assay , such as capp - seq , may be advantageous in the setting of disease surveillance.29 there are several potential clinical uses of ctdna in the diagnosis and management of patients with lms . 
crompton strategies for uterine tumors that could potentially harbor lms.32 second , there is significant clinical uncertainty regarding which patients with lms derive benefit from adjuvant chemotherapy and radiation.10 , 33 , 34 should ctdna levels bear prognostic significance for tumors that are at highest risk of recurrence or identify the presence of residual disease , their measurement may help guide clinical decisions regarding adjuvant therapies . 
finally , ctdna levels may be a useful indicator of response to systemic therapy and provide an early indication for switching or intensifying treatment regimens used in this disease.3 , 35 together with technologic improvements in sensitivity and throughput , these initial reports that identify ctdna in lms may quickly evolve to transform clinical practice . 
andersen no relationship to discloses edwin thai no relationship to discloses suzanne george stock and other ownership interests : abbott laboratories , abbvie ( i ) , allergan ( i ) consulting or advisory role : blueprint medicines , deciphera , astrazeneca , blueprint medicines , bayer , eli lilly research funding : pfizer ( inst ) , novartis ( inst ) , bayer ( inst ) , ariad pharmaceuticals ( inst ) , blueprint medicines ( inst ) , deciphera ( inst ) patents , royalties , other intellectual property : uptodate expert testimony : bayer other relationship : research to practice brian d . 
crompton , broad institute of massachusetts institute of technology and harvard , cambridge , ma ; and gavin ha , fred hutchinson cancer research center , seattle , wa . supported by the american society of oncology conquer cancer foundation young investigator award ( m.l.h. ) , national institutes of health grant no . 
toro jr , travis lb , wu hj , et al : incidence patterns of soft tissue sarcomas , regardless of primary site , in the surveillance , epidemiology and end results program , 1978 - 2001 : an analysis of 26 , 758 cases . 
ducimetire f , lurkin a , ranchre - vince d , et al : incidence of sarcoma histotypes and molecular subtypes in a prospective epidemiological study with central pathology review and molecular testing . 
hensley ml , ishill n , soslow r , et al : adjuvant gemcitabine plus docetaxel for completely resected stages i - iv high grade uterine leiomyosarcoma : results of a prospective study . 
oxnard gr , paweletz cp , kuang y , et al : noninvasive detection of response and resistance in egfr - mutant lung cancer using quantitative next - generation genotyping of cell - free plasma dna . 
klega k , imamovic - tuco a , ha g , et al : detection of somatic structural variants enables quantification and characterization of circulating tumor dna in children with solid tumors . 
mermel ch , schumacher se , hill b , et al : gistic2.0 facilitates sensitive and confident localization of the targets of focal somatic copy - number alteration in human cancers . 
stover dg , parsons ha , ha g , et al : association of cell - free dna tumor fraction and somatic copy number alterations with survival in metastatic triple - negative breast cancer . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
van roy n , van der linden m , menten b , et al : shallow whole genome sequencing on circulating cell - free dna allows reliable noninvasive copy - number profiling in neuroblastoma patients . 
heitzer e , ulz p , belic j , et al : tumor - associated copy number changes in the circulation of patients with prostate cancer identified through whole - genome sequencing . 
shulman ds , klega k , imamovic - tuco a , et al : detection of circulating tumour dna is associated with inferior outcomes in ewing sarcoma and osteosarcoma : a report from the childrens oncology group . 
hensley ml , wathen jk , maki rg , et al : adjuvant therapy for high - grade , uterus - limited leiomyosarcoma : results of a phase 2 trial ( sarc 005 )  . 
reed ns , mangioni c , malmstrm h , et al : phase iii randomised study to evaluate the role of adjuvant pelvic radiotherapy in the treatment of uterine sarcomas stages i and ii : an european organisation for research and treatment of cancer gynaecological cancer group study ( protocol 55874 )  . 
bowles , md2 , 3 introduction fibroblast growth factor receptors ( fgfrs ) 1 through 4 are transmembrane tyrosine kinase receptors that play a key role in cell survival , differentiation , migration , angiogenesis , and carcinogenesis.1 uncontrolled activation of fgfr signaling has been described in almost every type of malignancy and typically is the result of amplication or activating mutation affecting the fgfr genes.2 these aberrations can one of function as cancer drivers but also may inuence prognosis and sensitivity to treatment.3 - 5 only two fgfr - specic inhibitors , erdatinib and pemigatinib , have been approved by the us food and drug administration , though a number of multikinase kinase inhibitors ( mkis ) have some degree of fgfr2 inhibiting properties . although fgfr1 and fgfr3 mutations are more frequent overall , activation of fgfr2 is common in patients with endometrial adenocarcinoma , cholangiocarcinoma , gastric adenocarcinoma , and ameloblastoma , a rare and difcult - to - treat odontogenic tumor.2 , 6 - 9 here , we present the case of a patient with ameloblastoma harboring an activating fgfr2 y375c mutation who had signicant tumor regression in response to treatment with lenvatinib . 
a specimen from a repeated biopsy was sent for nextgeneration sequencing using cancerselect 125 ( personal genome diagnostics , baltimore , md )  . analysis revealed clonal fgfr2 y375c , an activating mutation in the transmembrane domain causing constitutive receptor dimerization through the formation of intermolecular disulde bonds.12 although fgfr2 aberrations are common in ameloblastoma , this point mutation appears not to have been identied previously . 
first characterized in bearestevenson cutis gyrate syndrome , y375c is rare in cancers but has been described in adenoid cystic carcinoma and endometrial carcinoma.13 , 14 a second potential driver mutation affecting the hedgehog signaling pathway , smo l412f , was also found at a lower allele fraction . 
frequently seen in ameloblastoma as well as basal cell carcinoma , medulloblastoma , and a subset of meningiomas , this activating mutation alters the drug - binding pocket of smo , conferring resistance to smo inhibitors such as vismodegib and itraconazole.6 a third mutation , palb2 h786y , was reported but is of unclear signicance , having never been associated with human disease . 
although sensitivity to fgfr inhibition varies by type of mutation , drug - binding site , and degree of fgfr specicity , 15 , 16 cancer cell lines harboring fgfr2 y375c mutations were previously found to be responsive to nonselective pan - fgfr inhibition in vitro.17 because the fgfr - specic inhibitors were not yet commercially available , lenvatinib was selected because of its favorable half maximal inhibitory concentration for fgfr2 ( 27 nmol / l ) and efcacy in other malignancies . the patient started receiving the standard dose for radioactive - iodine refractory thyroid cancer of 24 mg daily . his dose was reduced to 20 mg daily after 1 month , then 20 mg alternating with 10 mg daily after an additional month . 
he experienced typical adverse effects of grade 2 hypertension , grade 2 hypothyroidism , grade 1 diarrhea , and grade 2 weight loss . on follow - up imaging at 6 months , he experienced a partial response with 40% shrinkage , per recist , version 1.1 ( fig 1 )  . 
as of this writing , the patient has been receiving this treatment for 13 months and has a continued partial response . discussion ameloblastoma is a locally invasive , typically benign distransformation with ease that can undergo malignant regional or distant metastasis , sometimes occurring decades after initial presentation.18 - 23 surgery is the mainstay of treatment , although conservative enucleation and curettage are associated with recurrence rates as high as 60% to 90%.24 radical surgery with wide en bloc resection improves these rates but at the cost of disgurement and high morbidity . 
overall , guidance regarding use of adjuvant treatment modalities is lacking . given the dearth of effective and tolerable treatment options , reports of targetable mutations dominating the genetic landscape of ameloblastoma were met with great interest.6 - 8 a large percentage of ameloblastomas , especially those arising from the mandible , have braf v600e mutation . 
ameloblastomas harboring braf v600e mutation are sensitive to braf inhibition in vitro at clinically relevant drug concentrations.6 multiple case reports have demonstrated durable clinical response to braf inhibition or combined braf / mek inhibition , on the basis of braf status.26 - 30 a second , and typically mutually exclusive , molecular phenotype featured mutations in fgfr2 , including c382r and v395d in the transmembrane domain and n549k in the kinase domatogether , braf and fgfr2 mutations are present in approximately 80% of ameloblastomas , with additional somatic mutations in smo , cttnb1 , pik3ca , and smarcb1 . interestingly , the patient we report on here had nearly 90% allele frequency of fgfr2 y375c , suggesting this may have been the initial truncal mutation . 
the implications of clonality for fgfr point mutations and fusions are not well understood , but truncal amplication of fgfr2 is an important predictor of drug response in gastric cancer.31 in a small trial of the selective fgfr inhibitor azd4547 in fgfr2 - amplied gastroesophageal cancer , robust , singleagent clinical response was restricted to high copy - number amplication events with associated high expression of fgfr2 mrna and fgfr2 protethe mechanism for this fig 1 . 
 case report effect was thought to be transactivation of alternate receptor tyrosine kinases resulting in a distinct oncogene addiction phenotype characterized by fgfr - dependent phosphatidylinositol - 3 - kinase and mammalian target of rapamycin signaling . although prospective trials in ameloblastoma continue to insight into be limited by low case numbers , additional treatment of this disease may be drawn from other , molecularly similar cancer types , including endometrial and gastric adenocarcinomas . 
fgfr2 mutations occur in approximately 10% of both tumor types and are mutually exclusive , with kras mutations suggesting a shared signaling mechanism.9 , 32 , 33 in vitro data from endometrial cancer conrmed fgfr2 activation results in increased mapk signaling that is abrogated by fgfr inhibition.34 , 35 these preclinical data prompted a phase ii trial of lenvatinib in advanced endometrial cancer , which reported an objective response rate of 14% and a clinical benet rate of 37% without selection for fgfr status.36 conrmatory trials of fgfr inhibition in endometrial cancer , both alone and in combination with pembrolizumab or other checkpoint blockade , are ongoing.37 subgroup analysis of biomarkerselected populations in studies like these may be a helpful surrogate for utility in rare cancers such as ameloblastoma . complicating the generalization of fgfr inhibitor trial data are the multiple mechanisms of fgfr dysregulation . 
although studies typically lump together patients with any fgfr aberration , the type of mutationfgfr overexpression including gene amplication , increased ligandbinding afnity or ligand expression , or ligand - independent receptor activationresults in differential effects on fgfr signaling . 
using mkis as an example , brivanib primarily affects cells with fgfr1 amplication , dovitinib inhibits fgfr1 - 3 kinase activity in a predominately liganddependent fashion , and ponatinib targets fgfr1 - 4 with three patterns of signaling alteration we have described.17 although the exibility of some nonselective mkis in targeting multiple fgfr aberrations may broaden their use , it comes at the cost of increased toxicity . 
in contrast , early data from selective fgfr tkis demonstrated a favorable adverse effect prole but more limited efcacy.38 , 39 characterizing drug - susceptibility phenotypes will be crucial for the continued development of these agents and other approaches to fgfr inhibition , including monoclonal antibody or peptide inhibitors and fgf ligand traps . although lenvatinib was chosen in this case to target fgfr2 , it is possible the patients response was due to inhibition of other targets , such as vascular endothelial growth factor receptors , platelet - derived growth factors , or kit . 
assessment of phosphorylated - fgfr2 by immunohistochemistry before and after therapy could clarify if his response was due to on - target or off - target effects , but he declined a repeated biopsy procedure . 
lenvatinib has been effective in thyroid , renal , and hepatocellular carcinomas without identiable mutation or overexpression of these kinases , suggesting the mechanism underlying drug sensitivity is incompletely understood.37 most clinical trials of lenvatinib have been in solid tumor types selected on the basis of response to other inhibitors of angiogenesis , but these agents have not been investigated in ameloblastoma . more studies are needed to clarify the role of fgf signaling in drug response and identify predictive biomarkers for lenvatinib . 
clin cancer res 22 : 259 - 267 , 2016 donnem t , al - shibli k , al - saad s , et al : prognostic impact of broblast growth factor 2 in non - small cell lung cancer : coexpression with vegfr - 3 and pdgf - b predicts poor survival . 
j thorac oncol 4 : 578 - 585 , 2009 turner n , pearson a , sharpe r , et al : fgfr1 amplication drives endocrine therapy resistance and is a therapeutic target in breast cancer . 
ware ke , hinz tk , kleczko e , et al : a mechanism of resistance to getinib mediated by cellular reprogramming and the acquisition of an fgf2 - fgfr1 autocrine growth loop . 
nat genet 46 : 722 - 725 , 2014 [ erratum : nat genet 47 : 97 , 2015 ] kurppa kj , cat on j , morgan pr , et al : high frequency of braf v600e mutations in ameloblastoma . 
j pathol 232 : 492 - 498 , 2014 brown na , rolland d , mchugh jb , et al : activating fgfr2 - ras - braf mutations in ameloblastoma . 
clin cancer res 20 : 5517 - 5526 , 2014 dienstmann r , rodon j , prat a , et al : genomic aberrations in the fgfr pathway : opportunities for targeted therapies in solid tumors . 
byron sa , chen h , wortmann a , et al : the n550k / h mutations in fgfr2 confer differential resistance to pd173074 , dovitinib , and ponatinib atp - competitive 17 . 
gozgit jm , wong mj , moran l , et al : ponatinib ( ap24534 ) , a multitargeted pan - fgfr inhibitor with activity in multiple fgfr - amplied or mutated cancer 18 . 
brunet m , khalifa e , italiano a : enabling precision medicine for rare head and neck tumors : the example of braf / mek targeting in patients with metastatic 27 . 
faden dl , algazi a : durable treatment of ameloblastoma with single agent brafi re : clinical and radiographic response with combined braf - targeted therapy in stage 4 ameloblastoma . 
byron sa , gartside m powell ma , et al : fgfr2 point mutations in 466 endometrioid endometrial tumors : relationship with msi , kras , pik3ca , ctnnb1 mutations and clinicopathological features . 
plos one 7 : e30801 , 2012 [ erratum : plos one 7 , 2012 doi : 10.1371 / annotation / 0bfaecca - 0f87 - 43fe - 97ccf2ae3ddeb6d5 ] 33 . 
konecny ge , kolarova t , obrien na , et al : activity of the broblast growth factor receptor inhibitors dovitinib ( tki258 ) and nvp - bgj398 in human endometrial cancer cells . 
chae yk , ranganath k , hammerman ps , et al : inhibition of the broblast growth factor receptor ( fgfr ) pathway : the current landscape and barriers to clinical application . 
differences in the relative fractions of immune cell subpopulations between immune - rich er - positive and tnbcs3 suggested disparate immunotherapy strategies in the two immune - rich subsets . concerning the study of tnbc immune microenvironment , we recently observed the existence of at least three immune - clusters ( im ) in tnbcs by computing transcriptional - based deconvolution algorithms.4 ima , considered hot or t cell - inamed , shows greater enrichment of cytotoxic t cells , inferred by deconvolutions tools or by histologic til counts , and accounts for approximately 30% of the tnbcs analyzed . 
finally , imc was described as warm tumors , because intrinsic immune activities are effectively mounted , but tumors are able to escape and suppress such responses , as indicated by the greater abundance of tregs and the lower expression of pdl - 1 and pd - 1 compared with ima . 
on the basis of our ndings , we would like to comment that besides the heterogeneity of tnbcs in terms of immune - cell inltration , the immune - rich subtype represents immune - related transcriptional heterogeneity , with signicant implications for potential immunotherapeutic strategies . consistent with the genomic characterization of immune - cell inltration obtained in our tnbc cohort , the incidence of immune - enriched ima in tcga and metabric data sets does not exceed 30% ( fig 1a ) , supporting the reproducibility of our immune clusters , especially for hot tumors . 
 ( a ) proportion of immuno - clusters ( im ) previously reported in romero et al4 with the ital - mex , molecular taxonomy of breast cancer international consortium ( metabric ) , and the cancer genome atlas ( tcga ) datasets . 
 ( b ) donut plot of the percentage of immuno - clusters among tumors classied as immune - rich or non - immune - rich from the tcga and metbric cohorts . 
by applying cluster analysis of our immune clusters to tcga and metabric data sets , we found that immune - rich tnbcs ( high til metagene described by omeara et al1 ) are composed mainly of ima ( n = 160 , 62% ) , followed by imc ( n = 54 , 21% ; fig 1b ) , with cases categorized as imb ( n = 44 , 17% ) also present . 
when considering the distribution of high til metagenes ( top 25th percentile ) applied by omeara et al1 in our cohort ( ital - mex , n = 158 ) and classied according to immune - related clusters , we conrmed that immune - rich cases ( ima ) are almost exclusively integrated by high til metagene tumors ( n = 41 , 94% )  . however , we also observed that a relevant percentage of high til cases are also distributed among imc ( n = 17 , 32% ) and less represented in the cold imb immune cluster ( n = 11 , 18% ; fig 1c )  . 
omeara t , marczyk m , qing t , et al : immunological differences between immune - rich estrogen receptor - positive and immune - rich triple - negative breast cancers . 
 identifying erbb2 activating mutations in her2 - negative breast cancer : clinical impact of institute - wide genomic testing and enrollment in matched therapy trials pedro exman , md1 ; ana c . 
our primary aim was to describe the proportion of patients with a qualifying erbb2 mutation identied by our institutional genomic panel ( oncomap or oncopanel ) who enrolled in the trial . 
associations were calculated using fishers exact test . results we identied a total of 1 , 045 patients with metastatic breast cancer without erbb2 amplication who had available genomic testing results . 
of these , 42 patients were found to have erbb2 mutation and 19 patients ( 1.8% ) were eligible for the trial on the basis of the presence of an activating mutation , 18 of which were identied by oncopanel testing . 
fifty - eight percent of potentially eligible patients were approached , and 33.3% of eligible patients enrolled in the trial guided exclusively by oncopanel testing . conclusion more than one half of eligible patients were approached for trial participation and , signicantly , one third of those were enrolled in nct01670877 . 
 exman et al context key objective although tumor genomic sequencing has become more accessible , bridging the gap between patients with targetable mutations and recruitment to specic trials remains a challenge . 
this phase ii study has been active at dfci since 2013 , with consistent slot availability during this time . patients we included 1 , 817 patients in the profile cohort with mbc who had available genomic proling results between august 1 , 2011 , and june 1 , 2017 . 
from the ccpm cohort , we included patients with metastatic her2 - negative ( per ihc and / or fish ) breast cancer in whom targeted genomic panel results were available between june 22 , 2015 , and june we collected data on those patients who consented to be in the profile cohort and who had available oncomap or oncopanel . 
clinical data abstraction was performed via medical record review and included age and stage at initial diagnosis , date of recurrence , histologic features , and date of death or last follow - up . 
clinical her2 status was dened by the 2013 asco / college of american pathologists guidelines.7 survival data were collected through a combination of medical record review and linkage to the national death index . 
all data are stored in a custom redcap database . genomic analysis genomic testing was performed in a clia - certied environment within the center for advanced molecular diagnostics at brigham and womens hospital . 
 excluded patients with her2 - positive disease ( n = 772 ) profile cohort patients with mbc with at least one dfci visit and available oncopanel results between 2011 and 2017 ( n = 1 , 817 ) patients with er - positive / her2negative mbc with oncopanel result ( n = 1 , 045 ) patients with erbb2 mutation previously detected by other genomic test modality ( n = 1 ) erbb2 activating mutations in her2 metastatic breast cancer ccpm cohort patients with mbc with at least one dfci visit and available oncopanel results between 2015 and 2017 ( n = 194 ) excluded patients with her2 - positive disease ( n = 28 ) patients with her2negative mbc with oncopanel result ( n = 166 ) patients with erbb2 mutations ( n = 42 ) patients with eligible erbb2 mutations diagnosed by profile ( n = 18 ) patients approached by trial team after oncopanel result ( n = 11 ) patients approached by trial team after ccpm result ( n = 1 ) patients with eligible erbb2 mutations diagnosed by ccpm ( n = 6 ) patients with erbb2 mutations ( n = 10 ) patients enrolled on the basis of oncopanel results ( n = 6 ) patients enrolled on the basis of ccpm result ( n = 1 ) fig 1 . 
dfci , danafarber cancer institute ; er , estrogen receptor ; her2 , human epidermal growth factor receptor 2 ; mbc , metastatic breast cancer . muther trial this multi - institutional phase ii clinical trial ( clinicaltrials.gov identier : nct 01670877 ) evaluates the efcacy of neratinib in patients with her2 - negative ( per ihc and / or fish ) , erbb2 - mutant mbc . 
the study opened to accrual at dfci on september 20 , 2013 , and it remains open as of december 18 , 2018 . trial matching in 2016 , we instituted several programs , such as the ending metastatic breast cancer for everyone ( embrace ) program for patients with mbc , 11 the matchminer platform , 12 and an interactive web - based trial - matching tool13 ( data supplement ) to assist physicians in trial selection . 
through these programs , key data from oncopanel ( derived either from the profile or ccpm protocols ) , as well as results from other research testing conducted in a clia - environment , were collated into a central database . the data supplement presents details of the embrace prograa custom report ( data supplement ) was shared with the medical oncologist by a designated research coordinator at the time of a patients visit to facilitate realtime trial matching . 
in addition , a custom query for erbb2 alterations was created within the matchminer platform and allowed for the identication of all patients with breast cancer with an erbb2 alteration at dfci . 
this list was used to reach out directly to treating physicians as an extra outreach method to capture patients who might not have a return visit to dfci scheduled . statistical analysis the primary objective of our study was to describe the proportion of patients in the prespecied profile cohort with eligible erbb2 mutations detected by genomic analysis who enrolled in the selected trial . 
secondary objectives included describing the proportion of patients approached for trial screening , the median time from genomic testing results to trial enrollment , the median time from genomic testing to death , and overall survival ( os )  . 
os was dened as the time from diagnosis of metastatic disease ( by imaging or biopsy ) to death from any cause and was estimated using the kaplan - meier method . 
between august 2011 and june 2017 , 1 , 045 patients with her2 - negative mbc consented to the profile protocol and had successful genomic testing . oncopanel was performed in most of the patients of this cohort ( 98.8% , n = 1 , 032 of 1 , 045 )  . 
forty - two patients ( 4.0% ) were found to have erbb2 mutations in their tumors , and of these , 19 ( 1.8% ) had mutations eligible for the trial ( 18 detected by oncopanel , none by oncomap , and one by commercial panel )  . 
between june 2015 and june 2017 , 166 patients with her2 - negative mbc underwent successful oncopanel testing of a fresh tumor biopsy as part of the ccpm initiative ( fig 1 )  . 
in terms of our prespecied primary end point , the proportion of patients with eligible erbb2 mutations who enrolled in the selected neratinib trial on the basis of only oncopanel results was 33.3% ( six of 18 ) , representing 0.5% of the total tested population ( six of 1 , 045 )  . 
one additional patient with a previously known erbb2 mutation detected through commercial testing enrolled in the neratinib trial ; another patient enrolled in the trial on the basis of testing of a fresh metastatic specimen collected in the ccpm protocol ( fig 1 )  . all patients who enrolled in the trial had other multiple mutations detected by oncopanel ( data supplement ) , but none received additional treatment guided by another specic mutation . 
for patients with eligible erbb2 mutations , the median os was not reached ( data supplement )  . among 1 , 045 patients with her2 - negative mbc with available genomic results between 2011 and 2017 and included in our profile cohort , we identied a total of 19 patients with erbb2 mutations that rendered them eligible for the neratinib trial . 
although the total number of enrolled patients ( n = 8 ) at dfci was low , our site was the second - highest accruing site nationally , reecting the low overall prevalence of erbb2 mutations in breast cancer . we observed that the conversion rate from genomic result to trial enrollment was numerically higher in the profile cohort compared with the ccpm cohort , although the patients in the ccpm cohort were not approached because they had stable disease on current therapy . 
patients who enrolled in the trial had received a median of four ( range , one to six ) lines of systemic treatment in the metastatic ( mets ) setting before oncopanel results were available . 
in addition , 75% ( six of eight ) of the registered patients were enrolled after the rst progression after the oncopanel result was available and 25% ( two of eight ) after the second progression . 
 erbb2 activating mutations in her2 metastatic breast cancer mutated and eligible mutated not mutated test technical lack of an adequate archival sample , insufcient archival material , or failure ( the last being uncommon )  . 
because patients were not randomly assigned to undergo testing , we cannot denitively comment on the impact of enterprise - wide testing versus an approach of more selective testing at the time of clinical need . 
the potential for referral bias , given the long median interval between initial metastatic diagnosis and oncopanel testing , and the possibility that only more t patients were able to travel to our site later in their disease course , could have diluted differences in survival by erbb2 mutation status . 
in addition , 20% of patients with eligible mutations were lost to follow - up . the rarity of the patient population meant that only 0.5% of the total tested population ultimately enrolled in the neratinib study . 
it is notable that the median time from metastatic diagnosis to oncopanel result in mutated patients was 7.0 months , and in large part , this reected patients being referred to our institution after having lived with a diagnosis of mbc for some time before their initial visit . our data illustrate the hurdles involved in identifying and enrolling patients with rare molecular alterations in clinical trials . 
we believe that our data suggest that broad - based testing , the development of systems with the ability to query genomic testing results across a clinic population , and robust strategies to approach patients will be critical to the success of studies enrolling rare subsets . 
1 , 000 women to enroll eight patients in the selected trial ; however , this testing simultaneously identied patients for multiple other trials , in a tissueand timeefcient manner . one half of the patients enrolled in the neratinib trial were also potentially eligible for other simultaneous trials on the basis of targetable mutations such as in palb2 or pik3ca ( data supplement )  . 
a direct assessment of the drug activity of neratinib ( with or without fulvestrant ) will be performed in the muther trial , and progression - free survival will be evaluated as a secondary end point.17 a strength of our study is the selection of a specic clinical trial with wide slot availability over an extended period to evaluate the conversion rate from biomarker result to trial enrollment . 
a slightly lower conversion rate was observed by wheler et al , 5 who prospectively evaluated 500 patients ( only 16% with breast cancer ) ; 22% of them received directly guided treatment after tumor molecular proling . 
meric - bernstam et al18 evaluated 2 , 000 patients with different cancer types ; 7% of patients with potentially actionable alterations were enrolled in a specic mutation - driven trial , and 4% were treated in a trial with a molecular rationale . 
the safir - 01 study enrolled 423 patients with advanced breast cancer , and 13% of them were considered eligible for a mutationguided clinical trial.3 our study has several limitations . 
although all new patients to dfci were approached for participation in the overarching protocol allowing for tumor testing , we did not prospectively collect the decline rate , nor did we collect reasons for decline . 
not all consented patients with mbc underwent tumor testing , for a variety of reasons , including affiliations 1dana - farber cancer institute , boston , ma 2washington university school of medicine , st . 
freedman research funding : puma biotechnology ( inst ) , eisai ( inst ) lorenzo trippa consulting or advisory role : galera therapeutics romualdo barroso - sousa consulting or advisory role : lilly speakers bureau : roche , bristol - myers squibb travel , accommodations , expenses : roche simona di lascio honoraria : roche / genentech ethan cerami stock and other ownership interests : blueprint medicines honoraria : merck travel , accommodations , expenses : merck margaret s . 
tolaney consulting or advisory role : novartis , pzer , merck , lilly , nektar , nanostring technologies , astrazeneca , puma biotechnology , genentech , eisai , immunomedics , sano , celldex , bristol - myers squibb , paxman , seattle genetics research funding : genentech / roche ( inst ) , merck ( inst ) , exelixis ( inst ) , pzer ( inst ) , lilly ( inst ) , novartis ( inst ) , bristol - myers squibb ( inst ) , eisai ( inst ) , astrazeneca ( inst ) , nanostring technologies ( inst ) , cyclacel ( inst ) , nektar ( inst ) , immunomedics ( inst ) travel , accommodations , expenses : astrazeneca , lilly , merck , nektar , novartis , pzer , genentech / roche , immunomedics , eisai , nanostring technologies , puma biotechnology , celldex ian e . 
krop employment : amag pharmaceuticals ( i ) leadership : amag pharmaceuticals ( i ) stock and other ownership interests : amag pharmaceuticals ( i ) honoraria : genentech / roche consulting or advisory role : genentech / roche , daiichi sankyo , context therapeutics , macrogenics , taiho pharmaceutical research funding : genentech / roche ( inst ) , seattle genetics ( inst ) , pzer ( inst ) , daiichi sankyo ( inst ) ron bose honoraria : genentech , foundation medicine consulting or advisory role : genentech research funding : puma biotechnology ( inst ) bruce e . 
johnson research funding : novartis ( inst ) , toshiba ( inst ) , novartis ( inst ) , novartis ( inst ) patents , royalties , other intellectual property : dana - farber cancer institute cynthia x . 
ma consulting or advisory role : pzer , novartis , syndax , lilly , biovica , tempus , seattle genetics , agendia , myriad genetics , lilly research funding : pzer ( inst ) , eisai ( inst ) , puma ( inst ) travel , accommodations , expenses : syndax , lilly , agendia , pzer deborah a . 
winer stock and other ownership interests : verastem honoraria : genentech / roche , tesaro , genomic health consulting or advisory role : leap therapeutics , seattle genetics , jounce therapeutics , glaxosmithkline , carrick therapeutics , lilly research funding : genentech ( inst ) , novartis ( inst ) , merck ( inst ) nikhil wagle stock and other ownership interests : foundation medicine honoraria : lilly consulting or advisory role : novartis , lilly research funding : novartis , puma biotechnology nancy u . 
 erbb2 activating mutations in her2 metastatic breast cancer acknowledgment we thank kaitlyn bifolck for her editorial support . references 5 , 2010 ] andre f , mardis e , salm m , et al : prioritizing targets for precision cancer medicine . 
gynecol oncol 148 : 585 - 590 , 2018 andr e f , bachelot t , commo f , et al : comparative genomic hybridisation array and dna sequencing to direct treatment of metastatic breast cancer : a multicentre , prospective trial ( safir01 / unicancer )  . 
lancet oncol 15 : 267 - 274 , 2014 schwaederle m , zhao m , lee jj , et al : impact of precision medicine in diverse cancers : a meta - analysis of phase ii clinical trials . 
cancer res 76 : 3690 - 3701 , 2016 sholl lm , do k , shivdasani p , et al : institutional implementation of clinical tumor proling on an unselected cancer population . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
plos one 4 : e7887 , 2009 [ erratum : plos one garcia ep , minkovsky a , jia y , et al : validation of oncopanel : a targeted next - generation sequencing assay for the detection of somatic variants in cancer . 
ramkissoon sh , bandopadhayay p , hwang j , et al : clinical targeted exome - based sequencing in combination with genome - wide copy number proling : precision medicine analysis of 203 pediatric brain tumors . 
hughes me , frank es , merrill ms , et al : embrace ( ending metastatic breast cancer for everyone ) : a comprehensive approach to improve the care of patients with metastatic breast cancer . 
lindsay j , del vecchio fitz c , zwiesler z , et al : matchminer : an open source computational platform for real - time matching of cancer patients to precision medicine clinical trials using genomic and clinical criteria . 
collins jr , md1 a 61 - year - old man was diagnosed with acute myeloid leukemia ( aml ) associated with trisomy 8 cytogenetic abnormality and flt3 itd mutation . 
post - transplantation , he showed no morphologic or ow cytometric evidence of disease and his bone marrow chimerism was more than 95% donor cells at several timepoints post - transplantation , including 24 months after the transplant . 
he received tacrolimus post - transplantation and developed mild chronic graft - versus - host disease that was limited to the skthe patient remained on tacrolimus . twenty - nine months after transplantation , he presented with abdominal pacomputed tomography scan of the abdomen and pelvis revealed a known , unchanged ventral abdominal hernia , but also showed a new lytic lesion on the inferior pubic ramus that was concerning for a new malignancy ( fig 1a )  . 
flow cytometry of the lesion demonstrated a predominance of cd117bright positive , cd34 - negative myeloid cells suspected to be mast cells that did not aberrantly express cd2 or cd25 ( fig 3 )  . 
these cells showed atypical expression of fcri ( cd64 ) , which is seen upon mast cell activation . immunohistochemical analysis demonstrated that the cells were positive for cd117 and weakly positive for mast cell tryptase and negative for cd2 , cd25 , and cd34 ( fig 4 )  . 
altogether , supportive of a diagnosis of mast cell sarcoma ( mcs )  . the tumor next - generation sequencing ( foundationone heme panel ; foundation medicine , cambridge , ma ) on the biopsy was signicant for kit y503_f504insay , idh2 r140q , and srsf2 p95h mutations , but was negative for flt3 mutations . 
the particular kit mutation detected has been reported to be responsive to imatinib.1 - 4 the idh2 mutation has not previously been identied in mast cell neoplasms.5 the patient was treated with imatinib 400 mg per day in addition to radiation to the sacrum and pubic ramus4 , 500 cgy in 25 fractions . 
he remains without evidence of aml recurrence 71 months after hematopoietic sct . the original diagnosis of aml and subsequent bone marrow evaluations were reviewed in light of the development of mcs . 
cytogenetic studies revealed 47xy , + 8 [ 13 ] / 46 , xy [ 7 ] and uorescence in situ hybridization was positive for an extra signal for runx1t1 ( 8q22 ) in 59 of 200 interphase cells . 
sanger sequencing on dna from a saliva sample demonstrated wild - type germline idh2 and srsf2 . identical idh2 and srsf2 mutations implied a clonal relationship between the mcs and aml ( fig 5 )  . 
 brown et al context and mast cell sarcoma ? can tools , such as next - generation sequencing ( ngs ) , delineate a clonal relationship in a patient with acute myeloid leukemia we identied a probable clonal relatedness between the two neoplasms , with both sharing identical idh2 and srsf2 mutations . 
this report provides anecdotal evidence of a clonal relationship between acute myeloid leukemia and mast cell sarcoma that is developmentally feasible and describes a unique scenario in which ngs was effective at directing therapy . 
clinicians should consider performing ngs in patients with two neoplasms , particularly if a progenitor cell is feasible , as well as in patients with mast cell disorders and a neoplasm . the clonal progenitor that harbored the idh2 and srsf2 mutations persisted . 
shared mutations between aml and mcs support the existence of a preleukemic clonal progenitor that developed into aml initially and later into mcs . mcs was rst described in 1986 and is one of many diseases arising from the spectrum of mastocytosis.11 - 13 it typically presents as a solitary mass that may arise anywhere in the body and has intensely avid uorodeoxyglucose uptake on petcomputed tomography scan.9 - 11 , 14 - 20 diagnosis depends on the synthesis of pathologic and immunophenotypic that are features in a patient with an aggressive , initially sarcoma - like tumor.16 , 17 although initially localized , these tumors typically metastasize fig 1 . 
 ( a ) computed tomography ( ct ) scan of the abdomen and pelvis obtained for evaluation of abdominal pain incidentally revealed a destructive lesion of the left inferior pubic ramus that measured approximately 3 cm 2 cm , worrisome for malignancy . 
survival ranges from 2 months to 8 years , with a median survival of 6 months.10 , 12 , 15 , 16 , 18 - 21 cells are usually more atypical than those observed in systemic mastocytosis , with an epithelioid appearance with abundant granular cytoplasm and bilobed or multilobed nucleoli.15 , 22 mcs can be misdiagnosed on initial pathologic review given its rarity and resemblance to other tumor types , including lymphomas . 
these cells often lose markers that are characteristic for mast cells , which further complicates the diagnosis.20 , 23 evaluation of markers that are helpful to establish the diagnosis include cd2 , cd25 , cd30 , cd33 , cd34 , cd45 , cd117 , and mast cell tryptase.12 , 18 absence of cd117 positivity should call into question the diagnosis of a mast cell disorder . 
mast cell tryptase is highly specic for mast cell lineage , but may only show variable positivity in mcs.12 , 23 other immunohistochemical markers that overlap with melanoma , lymphomas , or other histiocytic processes have been reported.12 in the absence of another concurrent myeloid neoplasm , serum tryptase elevation strongly supports the diagnosis of a mast cell disorder.12 , 23 mcs have possessed kit mutations in eight of 15 cases that have reported on kit mutation testing , including the present case.10 , 11 , 19 , 20 cells with kit mutations fig 2 . 
flow cytometry of pubic ramus lesion detected a population of medium - sized to large cells , which accounted for approximately 60% of the total events , with high orthogonal light scatter indicative of high granularity / internal complexity ( red , abnormal cells ; blue , lymphocytes )  . 
abnormal cells were cd15 negative , cd117 bright positive , cd7 equivocal , cd13 + , cd2 , cd25 , cd36 , and cd64 + ( variable intensity )  . 
by immunohistochemistry , tumor cells were positive for cd117 and mast cell tryptase ( weakly ; top ) but negative for cd2 and cd25 ( bottom )  . cd25 remain cd117 bright on immunohistochemistry and are unaffected by changes induced by these mutations.24 kit mutations do not affect the ow cytometric detection of cd117 . therapy of mcs is poorly dened but typically involves surgery and radiation to localized lesions ; chemotherapy is usually ineffective.19 , 20 we would suggest that all patients with suspected mcs have kit sequenced . 
results of next - generation sequencing on both mcs and aml mutated allele genomic alteration frequency , % detected fda - approved therapy for patients tumor kit ( y503_ f504insay ) idh2 ( r140q ) srsf2 ( p95h ) flt3 ( s451f ) idh2 ( r140q ) ptpn11 d61h - subclonal n308dsubclonal srsf2 ( p95h ) imatinib none * none none none none enasidenib ( 2017 ) common myeloid progenitor cell idh2 srsf2 idh2 srsf2 flt3 ptpn11 mast cell idh2 srsf2 note . 
enasidenib was approved by the fda in 2017 , several years after the patient had aml . abbreviations : aml , acute myeloid leukemia ; fda , us food and drug administration ; mcs , mast cell sarcoma . * although enasidenib is not fda approved for mcs , it is conceivable that the drug , which targets mutant idh2 , may have activity in this patients case . and thus remains sensitive to imatinib.28 mcs with d816v mutations may be sensitive to other tyrosine kinase inhibitors , including avapritinib , which selectively targets the d816v mutation and is well tolerated.29 , 30 of interest , the idh2 mutation in our patients case is shared between aml and mcs , which suggests that it was present in a lessdifferentiated common progenitor cell . 
collins jr employment : university of texas southwestern medical centersimmons cancer center honoraria : optumhealth research funding : agios , arog , bristol - myers squibb , celgene no other potential conicts of interest were reported . references 2011 guo t , hajdu m , agaram np , et al : mechanisms of sunitinib resistance in gastrointestinal stromal tumors harboring kitay502 - 3ins mutation : an in vitro mutagenesis screen for drug resistance . 
br j haematol 173 : 323 - 326 , 2016 cancer genome atlas research network ; ley tj , miller c , et al : genomic and epigenomic landscapes of adult de novo acute myeloid leukemia . 
cell 168 : 1041 - 1052.e18 , 2017 yamashita a , saito t , akaike k , et al : mast cell sarcoma of the sternum , clonally related to an antecedent germ cell tumor with a novel d579del kit mutation . virchows arch 470 : 583 - 588 , 2017 10 . 
georgin - lavialle s , aguilar c , guieze r , et al : mast cell sarcoma : a rare and aggressive entityreport of two cases and review of the literature . 
krauth mt , f odinger m , rebuzzi l , et al : aggressive systemic mastocytosis with sarcoma - like growth in the skeleton , leukemic progression , and partial loss of mast cell differentiation antigens . 
verstovsek s , tefferi a , cortes j , et al : phase ii study of dasatinib in philadelphia chromosome - negative acute and chronic myeloid diseases , including systemic j cancer 42 : 1093 - 1103 , 2006 mastocytosis . 
brunner am , neuberg ds , wander sa , et al : isocitrate dehydrogenase 1 and 2 mutations , 2 - hydroxyglutarate levels , and response to standard chemotherapy for patients with newly diagnosed acute myeloid leukemia . 
schuurhuis gj , heuser m , freeman s , et al : minimal / measurable residual disease in aml : a consensus document from the european leukemianet mrd working party . 
we identied , for the rst time , an epigenomic factor that can potentially complement dna mutation status in discriminating patients with lung adenocarcinoma who are less likely to benet from egfr - tki treatment , thereby leading to improved patient management in precision medicine . jco precis oncol 5 : 418 - 431 . 
inhibition of epidermal growth factor receptor ( egfr ) kinase activity by egfr - tyrosine kinase inhibitors ( tkis ) , such as erlotinib , getinib , and afatinib , was effective in patients with nsclc with egfr - activating mutations . however , despite the remarkable clinical success , the treatment efcacy was still limited to 50% - 80%.10 , 11 the sizable percentage of nonresponders ( 20% - 30% ) suggested intrinsic tki resistance and substantial heterogeneity among tumors , even among egfrmutant tumors , highlighting the need for reliable predictive biomarkers . the comprehensive molecular proling of pretreatment lung adenocarcinoma to identify inherently tkiresistant cases can aid the development of potential strategies to manage such cases . 
 dna methylation proling for egfr - tki responses context key objective a sizable portion ( 20% - 30% ) of patients with epidermal growth factor receptor ( egfr ) mutant nonsmall - cell lung cancer have no good initial clinical response to egfr - tyrosine kinase inhibitors ( tkis ) , and how to predict intrinsic drug resistance accurately is challenging . 
global dna methylation landscape of tumors from patients with lung adenocarcinoma before tki treatment was analyzed to investigate the association with egfr - tki responses . knowledge generated a total of 216 tki responseassociated methylated sites were identied , and functional analysis revealed the enrichment of homeobox genes . 
in particular , increased methylation of hoxb9 correlated with higher rate of intrinsic resistance ( ir ) to egfr - tki . relevance dna methylation provides a different dimension to complement the dna mutationbased markers for understanding the mechanism of ir . 
evaluation of the methylation level on hoxb9 may be incorporated in the management of lung adenocarcinoma to aid the prediction of egfr - tki response . egfr - tki14 suggest many dna - based biomarkers for ir prediction . 
on the other hand , tumor suppressor genes involved in the alternative mechanisms of ir may be inactivated by epigenetic mechanisms that result in phenotypic or functional changes.15 however , although studies have reported that epigenetic changes in tumor participate in the evolution of acquired drug resistance through regulating gene expression patterns , 16 epigenomic data associated with ir to tki are lacking . 
modication of methylation on dna is stable and abnormal methylation represents an early event for cancer diagnosis , making methylation aberrations equally suitable candidates for recurrence detection and prediction of patient survival.17 - 21 therefore , we undertook a genome - wide approach to investigate dna methylation patterns associated with ir to tki . dna methylation that occurs at cytosines of cpg dinucleotides , especially within cpg islands in the promoter region , can lock genes in off status , resulting in a transcriptionally silent state.22 , 23 although dna methylation is an important mechanism for maintaining normal development and cellular homeostasis , aberrant dna methylationmediated silencing of tumor suppressor genes has been reported to be associated with cell survival and progression in cancer.24 dna methylation proling of tumors , including those of glioma , acute myeloid leukemia , and colorectal and lung cancers , has aided the identication of cancer subtypes correlated with clinical outcomes.25 - 29 in this study , we aimed to identify epigenetic markers for predicting drug efcacy in patients with lung adenocarcinoma . 
we conducted genome - wide dna methylation proling of tumors from patients before their egfr - tki therapy and established a dna methylation landscape to elucidate the association of dna methylation with the egfr - tki response status of patients via a pipeline of statistical analysis , gene ontology ( go ) , and bioinformatics analysis . 
detailed accounts of sample collection and protocols for dna extraction , bisulte conversion , dna methylation analysis , pyrosequencing along with statistical analysis , bioinformatics analysis , and data availability are presented in the data supplement . results clinicopathologic features of the patients table 1 lists the clinicopathologic features of the two cohorts . 
the validation cohort consisted of 163 egfrmutant patients and the majority ( 85.28% ) were at stage iv . the tki response assessmentprogressive disease ( pd ) , stable disease ( sd ) , partial response ( pr ) , or complete response ( cr ) was determined according to the recist guidelines.30 the pd group , dened at the rst scan done at 8 weeks following the start of egfr - tki , is considered as patients with ir . 
using the top 5% coefcient of variation as the cutoff , 24 , 121 probes with the greatest variability were analyzed , and 391 probes were found correlated with egfr - tki response . 
the majority of the probes ( 203 ) had higher dna methylation in patients with a poor response than in those with a favorable response ; hypermethylation correlated with poor response . 
a global view of the dna methylation distribution contrasting the patients with pd against those with pr showed that all but 13 probes were located above the diagonal line , elucidating a clear pattern of methylation gain in patients with pd ( fig 2b - d )  . 
the tumors of patients who were more likely to be resistant to egfr - tkis tended to have higher pretreatment methylation levels . chromosomal context analysis of candidate cpg sites showed enrichment in cpg islands and gene promoter regions the cpg sites were assigned to the annotated categories according to their chromosome positions relative to the nearby transcription start sites and the closest cpg islands ( data supplement )  . 
we examined the changes in the proportion of each category during our probe selection and found an increasing trend in cpg islands and the gene promoter region tss1500 ( between 1 , 500 bp and 200 bp upstream of the transcription start site )  . 
for the 37 transcription - repressive sites , the enrichment pattern in cpg islands was retained and that in tss1500 was increased to 27.03% ( fig 2e )  . identication of transcription - repressive methylation sites we investigated the potential of the 216 methylation sites in cis - regulation of gene expression by correlating publicly accessible mrna gene expression data ( gse60644 ) with dna methylation data ( gse56044 ) in lung adenocarcinoma ( data supplement )  . 
a total of 37 sites were identied as transcription - repressive sites ( data supplement )  . functional enrichment analysis of transcript - linked methylation showed eight probes linked to tfs ( go : 0003677 ) , to evaluate the molecular function of the genes mapped by the 37 transcription - repressive sites , go enrichment analysis was conducted . 
furthermore , using animal transcription factor database ( animaltfdb ) , we found that eight of the 37 sites were annotated to ve tfs : ikzf1 , hoxb9 , sp8 , lass4 , and vax2 ( table 2 and data supplement )  . figure 2g shows the f statistic and the corresponding p value from analysis of variance for each of the eight sites , along with the location and chromosome context information . 
we found that seven of the eight tf - linked sites are located in the context of cpg islands and ve in the transcription start site ( tss ) region ( table 2 )  . 
the two vax2 methylation sites also showed a moderate ability to predict the egfr - tki response ( data supplement )  . we further performed stratication analysis by classifying patients as those with egfr - activating mutations and those increased methylation of hoxb9 without ( figs 3d - f )  . ( cg13643585 ) was observed in pd patients . 
for the egfr wild - type group , the or ( 7.59 ) was comparable , but the p value was .09 , likely because of the small sample size ( fig 3e )  . 
the data in table 3 conrmed the pattern of increased hoxb9 methylation in the egfr - tkiresistant ( pd ) group compared with the disease control group ( cr , pr , or sd )  . 
the pd group was ranked rst in each quartile , and the one - sided rank - sum test for between - group differences indicated a signicant difference ( p = .036 ) ( data supplement )  . in addition , analysis of the auroc showed that hoxb9 methylation statistically signicantly increased the predictive precision of egfr - tki resistance for the dcr ( table 3 )  . 
although signicant advances have been made in understanding acquired resistance ( ar ) , the causes of ir remain unclear.12 in addition to being classied as ar versus ir , resistance mechanisms can be classied in terms of on - target versus off - target , 31 suggesting the activation of collateral signaling . 
the patients characteristics , smoking behavior ( p1 ) , sex ( p2 ) , egfr status ( p3 ) , and egfr - tki response ( p4 ) , are shown by the bars at the top of the heatmap . 
for each cpg probe , the average beta value across patients with pd was plotted against that across patients with pr and is shown as a smooth kernel scatter plot . 
in the gradient scale , red represents the densest region , whereas purple represents the sparsest region ; pr ( red ) , sd ( yellow ) , and pd ( blue )  . 
the probe distributions in the cpg context and the gene context are shown on the left and right , respectively , for all probes in the array ( top ) , for the most variably methylated probes ( upper middle ) , for the tki responseassociated methylation sites ( lower middle ) , and for the transcription - repressive sites ( bottom )  . 
moreover , where genomic resistance has been found , epigenomic modulation has been proposed as the potential mechanism . changes in resistant phenotypes , including epithelialtransition ( emt ) and cancer stemness mesenchymal shift , have been found to be driven by epigenetic remodeling . 
tki - induced dna methylation changes have been reported in advanced egfr - mutated lung cancer.33 decitabine , the dna methyl transferase inhibitor , could reverse the sensitivity of egfr - tkiresistant nsclc cell line pc9 / gr through demethylation of rassf1a and gadd45.34 the combination of tkis with epigenetic drugs has shown in preclinical and clinical promise as a treatment studies.33 - 35 in this study , we conducted clinical oncological investigation on the potential role of dna methylation in mediating ir to egfr - tki treatment in patients with advanced lung adenocarcinoma . 
aberrant dna methylation is one of the most classical events that occurs during lung cancer development.36 many studies have shown altered methylation patterns in lung cancer , indicating roles of epigenetic biomarkers and therapeutic targets.37 - 39 earlier study by zhu et al40 focused on the methylation patterns of wnt antagonists , showing the association of methylated sfrp5 with shortened progression - free survival under egfr - tki treatment , but not with ir to tki . 
interestingly , two 428 2021 by american society of clinical oncology of those ve genes , axl1 and hoxa9 , are homeobox tfs . our pursuit of the primary egfr - tkiresistant methylation markers also identied enrichment of homeobox genes . among the 30 tki - associated methylation probes annotated to tfs , 11 accounted for nine homeobox genes ( data supplement )  . we identied and conrmed the correlation of hoxb9 dna methylation with an increased rate of ir to egfr - tkis . hoxb9 is involved in cell development and proliferation43 and is suggested to function as a tf that can induce the expression of emt genes and several angiogenic factors , such as vegf , il - 8 , and tgf , resulting in the activation of egfr and erbb2.44 - 46 egfr signaling is connected to the nf - b pathway , giving the role in ir or ar to egfr inhibitors.47 however , the molecular mechanisms by which hoxb9 contributes to carcinogenesis are debated.48 , 49 the overexpression of hoxb9 can suppress the akt / nf - b / snail pathway and inhibit the proliferation of gastric carcinoma cells.50 we analyzed the correlation between egfr signaling and nf - bdependent pathways ( gse60644 ) and found that expression of hoxb9 negatively associated with that of kiaa1199 ( cell migrationinducing hyaluronidase 1 ; data supplement )  . 
through protein - protein interaction ( ppi ) analysis , we found that hoxb9 might cross talk with both ir and ar to egfr - tki through ezh2 , sirt1 , and egr2 ( data supplement )  . 
therefore , regulation of hoxb9 is crucial in the cooperated oncogenic loops.12 our data suggested that hoxb9 hypermethylation may be a novel tumor cellular state that is useful for precise categorization of tumor heterogeneity in the study of intrinsic egfr - tki resistance via off - target effects such as redundant or compensating signaling . pattern was consistent between patients with egfr - activating mutations and patients with wild - type egfr , implying that the regulatory effect of dna methylation of hoxb9 may be independent of egfr activity . in addition , dna methylation changes can be accurately detected in tumors and liquid biopsies . 
such detection is promising for the development of biomarkers for cancer screening.51 dna methylation in distal regulatory sites , such as enhancer regions , plays important roles in gene regulation through the binding of cell typespecic tfs and interaction with promoters.52 - 54 we validated a dna methylation site in the enhancer region of hoxb9 that can help the prediction of nonresponse to egfr - tki . 
in cancer , aberrant dna methylation at enhancers couples with recruitment of coactivators or corepressors , forming networks of cancer - associated tfs and their targeted genes.55 - 57 stone et al58 dened hypermethylation enhancers that correlate with sensitivity to endocrine therapy , suggesting the impact of enhancer status on the drug treatment response . 
 dna methylation proling for egfr - tki responses the combination of genetic aberrations , gene expression , and dna methylation highlights the potential of the identied candidates in the development of biomarkers for tumor diagnosis or prognosis . 
in this study , with a focus on medical actionability , we discovered that hoxb9 methylation could be a biomarker useful for discriminating patients with tki resistance from those with tki sensitivity , especially patients whose tumors harbor egfr - activating mutations . 
although improving the sensitivity and specicity of hoxb9 methylation is recommended , our work provided a preliminary proof of concept on the usefulness of hoxb9 methylation for opening up more clinical options to manage lung adenocarcinoma . 
for example , in accordance with the current clinical standard of treating egfr - mutant patients with egfr - tki , for patients with hoxb9 hypermethylation , combination treatment such as egfr - tki plus antiangiogenic therapy59 or egfr - tki plus chemotherapy60 may be another option to overcome the resistance and improve the response rate . 
 acknowledgment the authors thank all the patients and research staff who participated in this work . su et al references siegel rl , miller kd , jemal a : cancer statistics , 2019 . 
mitsudomi t , morita s , yatabe y , et al : getinib versus cisplatin plus docetaxel in patients with non - small - cell lung cancer harbouring mutations of the epidermal growth factor receptor ( wjtog3405 ) : an open label , randomised phase 3 trial . 
lancet oncol 11 : 121 - 128 , 2010 zhou c , wu yl , chen g , et al : erlotinib versus chemotherapy as rst - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
lancet oncol 12 : 735 - 742 , 2011 rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutationpositive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
wu yl , zhou c , liam ck , et al : first - line erlotinib versus gemcitabine / cisplatin in patients with advanced egfr mutation - positive non - small - cell lung cancer : analyses from the phase iii , randomized , open - label , ensure study . 
ann oncol 26 : 1883 - 1889 , 2015 yang jch , sequist lv , geater sl , et al : clinical activity of afatinib in patients with advanced non - small - cell lung cancer harbouring uncommon egfr mutations : a combined post - hoc analysis of lux - lung 2 , lux - lung 3 , and lux - lung 6 . 
lancet oncol 16 : 830 - 838 , 2015 yang jch , wu yl , schuler m , et al : afatinib versus cisplatin - based chemotherapy for egfr mutation - positive lung adenocarcinoma ( lux - lung 3 and luxlung 6 ) : analysis of overall survival data from two randomised , phase 3 trials . 
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lee ck , davies l , wu yl , et al : getinib or erlotinib vs chemotherapy for egfr mutation - positive lung cancer : individual patient data meta - analysis of overall survival . 
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zhu j , wang y , duan j , et al : dna methylation status of wnt antagonist sfrp5 can predict the response to the egfr - tyrosine kinase inhibitor therapy in nonsmall cell lung cancer . 
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zhang l , wu q , he c , et al : hoxb9 inhibits proliferation in gastric carcinoma cells via suppression of phosphorylated - akt and nf - b - dependent snail expression . 
taberlay pc , statham al , kelly tk , et al : reconguration of nucleosome - depleted regions at distal regulatory elements accompanies dna methylation of enhancers and insulators in cancer . 
h saito , t fukuhara , n furuya , et al : erlotinib plus bevacizumab versus erlotinib alone in patients with egfr - positive advanced non - squamous non - small - cell lung cancer ( nej026 ) : interim analysis of an open - label , randomised , multicentre , phase 3 trial . 
hosomi y , morita s , sugawara s , et al : getinib alone versus getinib plus chemotherapy for non - small - cell lung cancer with mutated epidermal growth factor receptor : nej009 study . 
kornaga , msc1 , 2 ; cheryl crozier , msc1 ; gun ho jang , phd1 ; lauren bathurst , msc1 , 3 ; irina kalatskaya , phd1 , 4 ; quang m . 
pathways were identied as aberrant if there were copy number aberrations and / or mutations in any of the predetermined pathway genes : ccnd1 / ccnd2 / ccnd3 / cdk4 / cdk6 , fgfr1 / fgfr2 / fgfr2 / fgfr4 , and akt1 / akt2 / pik3ca / pten . results the 390 of 420 samples that passed quality control were analyzed for distant metastasisfree survival between groups . 
these bcas represent the majority of new bca diagnoses ( 70% to 80% ) , and a recent meta - analysis of 62 , 923 women with estrogen receptor ( er ) positive bca , who were disease free after 5 years of endocrine therapy , reported that approximately one in three women will experience a relapse during the next 20 years.1 - 3 although the development of diagnostic tests have helped to inform patients with regard to residual relapse risk , 4 , 5 as well as the identication of those who do not benet from chemotherapy , 6 none have yet to provide insight for those high - risk patients who may benet from the precision medicine approaches offered in the metastatic setting . 
to fully maximize the benet of targeted therapies seen in unselected patients in the advance / metastatic setting , upfront stratication of patients at risk for recurrence to these targeted agents in the early setting would reduce unnecessary treatment and associated toxicities and form a rational basis for treatment selection . 
this retrospective study of 390 early breast cancers from a phase iii clinical trial demonstrates that genomic changes within key genes in the cyclin d / cyclin - dependent kinase , phosphatidylinositol 3 - kinase / protein kinase b , and broblast growth factor receptor pathways could identify patients who might benet most from treatment that targets those deregulated pathways . knowledge generated in this focused approach , aberrations among genes in these pathways were shown to affect risk of distant relapse . relevance the use of this stratication approach , which benets from the interrogation of a limited number of genes , could be implemented effectively by using existing genomic technologies in the clinical laboratory to aid clinicians in identifying patients for whom specic targeted treatments are needed in combination with standard endocrine therapy . and the cancer genome atlas , 13 , 14 translation of these ndings into novel approaches to the management of cancer is slow . in response , we generated data focused on specic signaling pathways derived from the international cancer genome consortium and the cancer genome atlas13 , 14 together with whole - genome copy number analyses . 
the analysis was performed on the basis of an a priori hypothesis related to molecular pathways for which there are existing targeted therapies currently under evaluation in late - stage clinical trials . 
in a case - control study , 420 patients from the tamoxifen versus exemestane adjuvant multinational ( team ) trial pathology cohort ( clinicaltrials . identiers : nct00279448 , nct00032136 , and nct00036270 ) 15 were selected to determine the prognostic ability of copy number events and specic mutational changes that represent the cyclin d / cyclin - dependent kinase ( ccnd / cdk ) , broblast growth factor receptor / broblast growth factor ( fgfr / fgf ) , and phosphatidylinositol 3 - kinase / protein kinase b ( pi3k / akt ) pathways to predict risk of recurrence after anti - endocrine therapy in the early setting . 
distant metastasisfree survival ( dmfs ) was dened as time from random assignment to distant relapse or death as a result of bca.15 this study complies with the declaration of helsinki , institutional ethics committees , and the international conference on harmonization and good clinical practice guidelines . 
patients provided informed consent , and this study was approved by the university of toronto research ethics board ( protocol number 35339 )  . targeted sequencing and copy number analysis forty nanograms of dna extracted from formalin - xed parafn - embedded tissues were processed for targeted sequencing ( appendix )  . 
only variants that were on target and passed ltering criteria were included in the downstream analysis as described by kalatskaya et al.19 for copy number aberration ( cna ) analyses , 200 ng of dna were processed using oncoscan ffpe express 2.0 snp arrays ( affymetrix , santa clara , ca )  . 
 prognostic signatures in early breast cancers highly variable log - r ratio ( lrr ) , unevenly distributed b - allele frequencies , and waviness in lrr were measured using penncnv.20 estimation of tumor ploidy and aberrant tumor fraction was performed , and copy number segments were used by combining segments generated by two algorithms : allele - specic copy number analysis of tumors version 2.121 and circular binary segmentation22 implemented in the dnacopy package of r . 
an algorithm described by boutros et al23 was used to recalibrate tumor ploidy , aberrant tumor fraction , and copy numbers on the basis of lrr and b - allele frequency data , and adjacent segments having the same copy numbers were merged . segment boundaries were adjusted to obtain smaller argument function values . 
analyses were performed using r version 3.1.0. statistical analysis of the 420 patients , 390 passed ltering criteria and were included in subsequent analyses using stata 12.1 software ( statacorp , college station , tx )  . 
genes that represented pathways of interest were identied as aberrant according to the following criteria : ccnd / cdk pathway ( gains / amplications in any of ccnd1 / ccnd2 / ccnd3 / cdk4 / cdk6 ) , fgfr pathway ( gains / amplications in any of fgfr1 / fgfr2 / fgfr3 / fgfr4 ) , and pi3k / atk pathway ( aberrations in any of the following : gain / amplication of akt1 or possession of a mutation in akt1 , gain / amplication of akt2 , gain / amplication of pik3ca , and pten mutation and accompanying pten loss akt1 / akt2 / pik3ca / pten )  . a second model for the pi3k / akt was analyzed where pik3ca mutation data were included alongside pik3ca cnas and alterations in the genes of the dened pathways . kaplan - meier method and log - rank analyses were used to assess differences in dmfs . 
hrs were calculated using cox proportional hazards regression models , and models were adjusted for age ( continuous variable ) , tumor size ( dichotomized at 2 cm ) , tumor grade ( 1 / 2 v 3 ) , lymph node status , and her2 status ( negative v positive )  . 
all p values reported were two - sided , and p , .05 was considered statistically signicant . results changes in copy number of genes associated with signaling pathways are independently linked to high risk or relapse after anti - endocrine therapy our a priori hypothesis identied candidate pathways and specic genomic changes linked to endocrine treatment failure and outcome , namely ccnd / cdk signaling , the pi3k / akt axis , and fgfr / fgf pathway . 
no statistically signicant differences in age , tumor size , grade , lymph node status , or her2 status between patients with a dmfs event and those without were noted ( table 1 )  . 
of the 272 patients , 172 had aberrations in the specied ccnd / cdk genes ( 147 with aberrations in the fgfr genes and 138 with aberrations in pi3k / akt genes )  . 
of the 390 patients , 54 ( 13.8% ) , 34 ( 8.7% ) , and 43 ( 11% ) possessed aberrations in only one pathway ( ccnd / cdk , pi3k / akt , and fgfr , respectively )  . slightly fewer patients possessed aberrations in two pathways : 37 ( 9.5% ) with aberrant ccnd / cdkand pi3k / aktrelated genes , 37 ( 9.5% ) with aberrant ccnd / cdkand fgfr - related genes , and 23 ( 5.9% ) with aberrant pi3k / aktand fgfr - related genes . 
correlation to grade according to the number of pathways showed that patients with lower - grade tumors ( grade 1 / 2 ) had fewer altered pathways than those with grade 3 tumors ( appendix table a2 )  . 
although widely viewed as a good - prognosis subtype , hormone receptorpositive bcas account more than 84% of newly diagnosed early bca and therefore comprise the majority of bca deaths . 
despite recent advances in adjuvant therapy , outcomes for high - risk hormone receptorpositive bca are suboptimal , with an estimated relapse rate of 25% at 5 years.1 , 2 , 28 patients who are disease free at 5 years after diagnosis can still experelapse 5 to 20 years rience a high risk of distant postdiagnosis , 1 , 28 which directly challenges the dogma that such cancers are low risk and responsive to treatment . we tested the hypothesis that aberrations in key signaling pathways , where targeted therapies exist for bca ( in the advanced or metastatic setting ) , are prognostic in the early bca setting . 
aberrations in key genes of the ccnd / cdk pathway were more frequently detected than those in the pi3k / akt or fgfr axes ; however , the majority of patients ( 52% ) had aberrations in more than one pathway , which offers a rationale for incomplete responses to monotargeted therapy . 
kaplan - meier survival curves for aberrant pathways ( a ) cyclin d / cyclin - dependent kinase ( ccnd / cdk ) , ( b ) broblast growth factor receptor ( fgfr ) , ( c ) phosphatidylinositol 3 - kinase / protein kinase b ( pi3k / akt ) in the absence of pik3ca mutation , and ( d ) pi3k / akt pathway with pik3ca mutations . 
patients who possessed ccnd / cdk alterations exhibited signicantly poorer outcomes ( fig 1a ) than patients with fgfr and pi3k / akt aberrations ( figs 1b and 1c , respectively )  . 
in combination , patients with ccnd / cdk and fgfr aberrations were also at higher risk for relapse ( figs 2 and 3 ) possibly because of the proximity of ccnd1 and ligands fgf2 and fgf3 on chromosome 11q and their frequent co - amplication.29 indeed , the outcome for patients with ccnd / cdk and fgfr aberrations was similar to patients with ccnd / cdk aberrations only ( fig 3b )  . 
when pik3ca mutations were included in the stratication , there was no difference in survival between the two groups , consistent with the nding that pik3ca mutations in early bca and in the context of endocrine therapy seems to have no impact on outcome.30 , 31 increasing numbers of aberrant pathways also were associated with higher grade ( appendix tables a1 and a2 ) , consistent with the role of grade as an important prognostic factor32 and its association with gene expression changes that drive proliferation.33 - 35 intrinsic , endocrine resistance , acquired or remains a therapeutic challenge . 
for example , we have shown that up to one in ve early bcas exhibit amplications of cdk2 / 4 / 6 and ccnds39 , 40 and that ccnd1 amplication , but not overexpression , is associated with increased risk of distant relapse in endocrine - treated early bca.40 similarly , the trial study design did not stratify patients upfront by biomarker . 
consistent with published work , our data support evidence for a key role of cnas in this gene pathway.52 , 53 toxicities associated with mtor inhibitors like everolimus remain a concern . 
kaplan - meier curves of distant metastasisfree survival ( dmfs ) according to ( a ) risk order ( no aberrant pathway , any cyclin d / cyclin - dependent kinase [ ccnd / cdk ] , phosphatidylinositol 3 - kinase / protein kinase b [ pi3k / akt ] and broblast growth factor receptor [ fgfr ] , and fgfr only )  . 
 ( b ) frequency of aberration ( no aberrant pathway ; any pi3k / akt , fgfr and ccnd / cdk ; and ccnd / cdk only )  . class of drug would greatly affect patient management . phase iii trials are now under way to evaluate pi3k / akt inhibitors , including pi3kselective inhibitors in combination with fulvestrant in the advanced / metastatic bca setting ( clinicaltrials.gov identiers : nct02437318 and nct02340221 )  . 
phase ii neoadjuvant trials also are being conducted in the early bca setting ( clinicaltrials.gov identiers : nct01923168 and nct02273973 ) , which requires tumor pik3ca mutation status before determination of treatment randomization . 
however , we and others have shown that in early hormone receptorpositive bca , pik3ca mutations represent one of the most frequent mutations ( 35% ) 31 , 54 , 55 but show limited evidence that these mutations are linked to endocrine resistance in the early setting . the fgfr family of genes are recognized to be amplied in 10% to 15% of bcas.56 , 57 although fgfr1 is most frequently amplied , there is evidence for lower frequency amplication of fgfr2 , fgfr3 , and fgfr458 - 60 in early bca . 
evidence has emerged that links fgfrs to endocrine resistance.58 , 60 - 62 in preclinical studies , fgfr1 amplication enhanced pi3k and mitogen - activated protein kinase pathway signaling , which leads to endocrine resistance and could be reversed using rna interference against fgfr1.57 between 30% and 40% of cancers with ccnd1 amplication exhibit fgfr1 co - amplication despite the fact that these genes are mapped within different amplication loci on chromosomes 11 and 8.63 a challenge in targeting both ccnd1 and fgf pathwayamplied tumors is the proximity of the ligands fgf3 and fgf4 to ccnd1 on chromosome 11q13 . 
the role of fgfr signaling in a number of cancer settings suggests that it is a potential driver of cancer progression.58 , 64 , 65 several fgfr - targeted inhibitors are under investigation in phase ii clinical trials , including fgfr1 to 4 selective inhibitors bgj398 identiers : nct01004224 and ( clinicaltrials.gov nct02160041 ) and azd4547 ( clinicaltrials.gov identiers : nct01791985 , nct01795768 , and nct01202591 )  . 
to date , all trials that involve fgfr - targeted inhibitors are for patients with advanced or metastatic disease , with almost all trials requiring molecular prescreening for only fgfr1 or 11q amplication before study entry . issues of early hormone receptorpositive bca critical management must be addressed , 66 - 70 including molecular heterogeneity7 , 8 , 71 and emergent drug resistance.72 , 73 clinically , patients with such features would benet from early treatment with combinatorial therapies . 
in a drug screen of 42 agents , ribociclib was identied as a strong sensitizer to pi3k inhibition in three er - positive bca cell lines with acquired resistance to pi3k inhibitors.74 targeted doublet combinations of cdk4 / 6 or pi3k / mtor inhibitors with endocrine therapy have improved progression - free survival compared with endocrine therapy alone , 37 , 75 , 76 whereas another study showed that palbociclib plus pictilisib and fulvestrant was more effective than doublet combinations.77 we show that early hormone receptorpositive bcas could be stratied using genomic markers representative of pathways linked to targeted therapeutics that predict risk of recurrence after endocrine treatment . 
bartlett provision of study material or patients : daniel rea collection and assembly of data : jane bayani , cheryl crozier , paul c . boutros , melanie spears , john d . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . jane bayani patents , royalties , other intellectual property : 95 gene signature of residual risk in endocrine - treated early breast cancer ( provisional us patent 62 / 263 , 805 ) daniel rea honoraria : roche , novartis , pzer , eli lilly consulting or advisory role : genomic health research funding : celgene ( inst ) , roche ( inst ) , biotheranostics ( inst ) travel , accommodations , expenses : pzer , daiichi sankyo john m.s. 
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finn rs , crown jp , lang i , et al : the cyclin - dependent kinase 4 / 6 inhibitor palbociclib in combination with letrozole versus letrozole alone as rst - line treatment of oestrogen receptor - positive , her2 - negative , advanced breast cancer ( paloma - 1 / trio - 18 ) : a randomised phase 2 study . 
n engl j med 375 : 1925 - 1936 , 2016 jensen lb , bartlett jms , witton cj , et al : frequent amplications and deletions of g1 / s - phase transition genes , ccnd1 and myc in early breast cancers : a potential role in g1 / s escape . 
miller tw , hennessy bt , gonz alez - angulo am , et al : hyperactivation of phosphatidylinositol - 3 kinase promotes escape from hormone dependence in estrogen receptor - positive human breast cancer . 
baselga j , semiglazov v , van dam p , et al : phase ii randomized study of neoadjuvant everolimus plus letrozole compared with placebo plus letrozole in patients with estrogen receptor - positive breast cancer . 
loi s , michiels s , baselga j , et al : pik3ca genotype and a pik3ca mutation - related gene signature and response to everolimus and letrozole in estrogen 49 . 
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sabine vs , sims ah , macaskill ej , et al : gene expression proling of response to mtor inhibitor everolimus in pre - operatively treated post - menopausal women with oestrogen receptor - positive breast cancer . 
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beelen k , opdam m , severson tm , et al : pik3ca mutations , phosphatase and tensin homolog , human epidermal growth factor receptor 2 , and insulin - like growth factor 1 receptor and adjuvant tamoxifen resistance in postmenopausal breast cancer patients . 
cancer res 70 : 2085 - 2094 , 2010 jaakkola s , salmikangas p , nylund s , et al : amplication of fgfr4 gene in human breast and gynecological cancers . 
heiskanen m , kononen j , b arlund m , et al : cgh , cdna and tissue microarray analyses implicate fgfr2 amplication in a small subset of breast tumors . 
taylor - harding b , aspuria pj , agadjanian h , et al : cyclin e1 and rtk / ras signaling drive cdk inhibitor resistance via activation of e2f and ets . 
sledge gw jr , toi m , neven p , et al : monarch 2 : abemaciclib in combination with fulvestrant in women with hr + / her2advanced breast cancer who had progressed while receiving endocrine therapy . 
 prognostic signatures in early breast cancers appendix targeted sequencing submission of 101 selected genes resulted in 6 , 318 amplicons , with a median size of 109 base pairs ( bp ; range , 64 to 142 bp ) that covered 612.79 kbp ( unpublished data )  . 
using ampliseq polymerase chain reaction primer panels ( thermo fisher scientic , waltham , ma ) for the gene set developed above , we adapted our current protocol for illumina ( san diego , ca ) sequencing . 
after amplication of dna regions in four separate pools of the total 6 , 318 amplicons ( pool 1 , 1 , 587 amplicons ; pool 2 , 1 , 580 amplicons ; pool 3 , 1 , 578 amplicons ; pool 4 , 1 , 573 amplicons ; 10 ng / pool , 40 ng total dna ) , library polymerase chain reaction products were combined ( per sample ) , barcoded , and pooled in sets of 96 samples . 
t raw reads ( 101 - bp paired - end ) were aligned against the university of california , santa cruz , human reference sequence hg19 ( including random and unknown sequences ) using novoalign version 2.07.14 ( novocraft technologies , selangor , malaysia )  . 
aligned reads were ltered with samtools version 0.1.1816 to remove unmapped reads , nonprimary aligned reads , and reads aligned with mapping quality less than 30 ( ie , nonunique alignments )  . 
because the tamoxifen versus exemestane adjuvant multinational trial ( clinicaltrial . gov identiers : nct00279448 and nct00032136 , and nct00036270 ) cohort did not have matching normal tissue , the conventional mutation calling pipelines were not applicable . 
 radiogenomics analysis of intratumor heterogeneity in a patient with high - grade serous ovarian cancer britta weigelt , phd1 ; hebert alberto vargas , md1 ; pier selenica1 ; felipe c . 
reis - filho , md , phd1 ; and evis sala , md , phd1 , 3 introduction the overall survival of patients with high - grade serous ovarian cancer ( hgsoc ) has not improved during the past 20 years.1 studies have revealed that genomic intratumor heterogeneity correlates with poor survival2 , 3 and specic patterns of malignant cell spread in hgsoc.4 the physical distribution of malignant clones across the peritoneal cavity may be nonrandom , because some sites harbor genetically diverse clones.5 these region - specic properties may invasion and expansion , modulate malignant cell thereby shaping evolutionary selection.3 , 6 our understanding of genomic heterogeneity in hgsoc is limited to single biopsies ; little is known about individual spatial and temporal variation across various tumor sites.2 - 5 hence , developing imaging methods for guiding tissue sampling to physiologically and metabolically distinct tumor habitats is desirable . 
such approaches will be vital for new clinical trials , especially those combining immunologic and genomically targeted therapies . here we use lesion - specic three - dimensional ( 3d ) molds for phenotypic image - guided tumor sampling to ensure spatial colocation of imaging , histology , and genomic data , critical for understanding tumor biology . phenotypic imaging maps of heterogeneity ( ie , imaging habitats ) of two hgsoc sites were obtained by combining perfusion , diffusion , and metabolic maps derived from multiparametric imaging . 
four days before primary cytoreductive surgery the patient underwent same - day multiparametric magnetic resonance imaging ( mpmri ; discovery mr750 3t mri system , ge healthcare , chicago , il ) of the abdomen and pelvis and 18f - uorodeoxyglucose ( fdg ) positron emission tomography ( pet ) / computed tomography ( ct ; discovery pet / ct system , ge healthcare )  . 
details of image acquisition , analysis , and mr - pet / ct coregistration are described in the appendix and in appendix table a1 . cluster - guided specimen sampling imaging habitats were identied using k - means clustering of the standardized uptake value ( suv ) , diffusion coefcient ( d ) , perfusion fraction ( f ) , and transfer constant ( dynamic contrast - enhanced parameter ktrans ) voxels , with the number of clusters ( k ) being xed to k = 3.7 custom - made 3d molds of the lesions were printed using a 3d printer ( makerbot replicator 2 ; makerbot , brooklyn , ny ) on the basis of manual segmentation of the right ovarian tumor and metastatic implant on the axial t2 - weighted mri ( appendix )  . 
tissue samples of each imaging cluster were obtained , cut in half , and formalin - xed and parafn - embedded for histopathologic analysis or snap - frozen for genomic analysis ( fig 1a )  . histologic review and immunohistochemistry the three right ovarian mass hgsoc imaging - based habitats ( labeled blue , yellow , or green ) and the omental implant ( blue ) were reviewed by two pathologists blinded to the habitat assignment . 
 ( a ) phenotypically distinct areas of a highgrade serous ovarian cancer ( hgsoc ) were identied by k - means clustering of imaging features derived from magnetic resonance imaging ( mri ) and positron emission tomography ( pet ) / computed tomography . 
the distinct imaging habitats ( labeled blue , yellow , and green ) were sampled from the surgically removed primary hgsoc and metastatic implant using a three - dimensional ( 3d ) mold . 
half of each imaging - based tissue area was formalin - xed parafnembedded for histopathologic review and immunohistochemical analysis , and the other half was ash - frozen for whole - exome sequencing analysis . 
 ( b ) micrographs of representative hematoxylin and eosin ( h and e ) stained sections of the imaging - based hgsoc areas ( top row ) , and immunohistochemical analysis of cd31 , ki - 67 , ca - ix , and hif - 1 . 
 ( c ) imaging features associated with the distinct color areas as dened by k - means clustering of standardized uptake values ( suv ) , diffusion coefcient ( d ) , dynamic contrast - enhanced dce parameter ( ktrans ) , and water volume fraction owing through microvessels ( f ) are plotted on top , and the histopathologic features of the distinct imaging - based tumor areas are shown at the bottocolor - coding according to the legend . dw , diffusion - weighted ; fdg , 18f - uorodeoxyglucose ; til , tumor - inltrating lymphocyte . nonsynonymous somatic mutations ( 74% ) not detected in all tumor areas by wes were independently validated using a custom hybrid - capture targeted massively parallel sequencing assay . 
the clusters were labeled blue ( lowest ktrans , highest suv , highest f ) , yellow ( highest d , lowest f ) , or green ( lowest d , highest ktrans , lowest suv )  . 
the right ovarian cancer contained all three distinct imagingbased clusters , whereas the omental metastatic implant was entirely composed of one cluster ( blue ; fig 1a ) , suggestive of phenotypic imaging heterogeneity in the primary hgsoc . tissue from the distinct imaging - based clusters for immunohistochemical and genetic analyses was obtained through a custom - made 3d mold ( fig 1a )  . imaging - based clusters are underpinned by distinct growth patterns and expression of hypoxia - related markers phenotypic imaging - based clusters were associated with distinct histopathologic growth patterns . 
 ( d ) unsupervised hierarchical clustering of the somatic mutations ( left ) and of the gene copy number alterations ( right ) identied not to be shared by all four imaging - based hgsoc areas using wards algorithm and euclidean distance . left , genes affected by mutations are shown in black ; right , amplication , gain , loss , and deletion are shown in dark red , red , blue , and dark blue , respectively . 
the values on the edges of the clustering are derived from pvclust analysis to assess the stability of the clusters ; both the approximatelyunbiased and bootstrap - probability p values were 100% . 
 weigelt et al signature 1 signature 3 other signatures mutant wild type somatic mutations copy number alterations amplification no change deletion gain loss ovary green ovary yellow ovary blue omentum blue ovary green ovary yellow ovary blue omentum blue 7q11 amp 2q11 amp ovary yellow ovary green tp53 pot1 16p12 amp 6p21 amp ovary blue fig 2 . 
the expression levels and patterns of the hypoxia - marker hif - 1 and its downstream target ca - ix correlated with the distinct areas dened by multiparametric imaging ( fig 1c )  . 
consistent with the imaging ndings , which demonstrated that the ovary blue and omentum blue areas displayed the highest f , an mri marker of tissue vascularity , cd31 immunohistochemical assessment revealed a higher density of tumor neovascularization ( 4 + ) in the ovary blue and omentum blue areas than in the ovary green and ovary yellow areas ( 2 + ; fig 1c )  . 
furthermore , distinct patterns and levels of ca - ix expression were observed among these areas , with ovary yellow and green having h - scores of 80 , compared with 230 and 195 in ovary blue and omentum blue , respectively . 
for hif - 1 , a reverse pattern was found , with ovary yellow and ovary green areas displaying high levels of hif - 1 expression ( h - scores , 115 ) compared with ovary blue and omentum blue ( h - scores , 75 and 60 , respectively ; figs 1b and 1c )  . imaging - based clusters are underpinned by distinct repertoires of genetic alterations high - depth wes of microdissected tumor and normal samples revealed 50 nonsynonymous somatic mutations , including a tp53 p.p47tfs * 5 frameshift mutation , which were shared among all four imaging - based tumor areas ( fig 2 )  . 
twenty - eight nonsynonymous somatic mutations were shared exclusively between ovary blue and omentum blue , and 46 between the ovary green and ovary yellow components ( fig 2a )  . 
although all imaging habitats displayed genomics features of homologous recombination dna repair deciency ( dominant mutational signature 3 , high large - scale transition scores ; fig 2c ) , hierarchical clustering of the 146 nonsynonymous somatic mutations or the 718 gene copy number alterations not shared among all four imagingbased areas revealed that both at the mutational and gene copy number levels , ovary blue and omentum blue clustered together and were distinct from ovary yellow and ovary green ( fig 2d )  . 
several somatic mutations found to be subclonal in ovary blue , including mutations affecting auts2 , eif2ak4 , and trim41 , became clonal in omentum blue ( fig 2a ) , and a subset of genes affected by copy number losses in ovary blue became homozygously deleted in omentum blue ( eg , chromosome 18q23 ; fig 2d )  . discussion several studies have demonstrated that hgsocs display spatial and temporal genetic heterogeneity , 2 - 6 , 22 with tumors composed of genetically distinct clones and exhibiting distinct evolutionary trajectories and mechanisms of therapy resistance.4 , 23 , 24 our observations support the contention that phenotypic and genetic analysis of single biopsy or single tumor samples may not provide a sufciently accurate representation of hgsoc heterogeneity.4 this proof - of - principle study suggests that multiparametric imaging assessment may provide a noninvasive surrogate for intratumor genetic heterogeneity and may guide precise tissue sampling . 
given the evidence supporting the impact of intratumor genetic heterogeneity on tumors metastatic ability and resistance to therapeutic interventions , 25 the results of this proof - of - principle observation provide the basis for studies to dene the type of sampling required for the assessment of preand posttreatment hgsocs . 
it should be noted , however , that multiparametric imaging for tumor heterogeneity and tumor evolution assessment requires not only manual segmentation of the imaging data but also standardization of the image acquisition protocols across different imaging platforms . targeted therapy and immunotherapy are being progressively applied earlier in the treatment of patients with cancer , and certain agents are anticipated to become part of front - line therapy . 
minimally invasive methods for disease monitoring in the form of circulating cell - free plasma dna hold great promise in the assessment of genetic heterogeneity within a patient.26 - 28 our imaging habitatbased method would constitute a noninvasive and complementary approach to such endeavors , given that it may allow for the sampling of selected image habitats without having to analyze every section of every tumor , an impossible task particularly in the metastatic and recurrent settings . 
for more information about asco 's conict of interest policy , please refer to or po.ascopubs.org / site / ifc . britta weigelt consulting or advisory role : genentech ( i ) , invicro ( i ) , ventana medical systems ( i ) , volitionrx ( i ) , paige.ai ( i ) , goldman sachs ( i ) felipe c . 
 weigelt et al niamh conlon employment : abbvie ( i ) stock and other ownership interests : merck ( i ) alexandra snyder employment : adaptive biotechnologies , merck stock and other ownership interests : merck consulting or advisory role : driver group research funding : bristol - myers squibb travel , accommodations , expenses : genentech , bristol - myers squibb robert a . 
assignee : the regents of the university of california august 18 , 2015 ( inst ) ; application : compositions and methods for the diagnosis and treatment of ovarian cancers that are associated with reduced smarca4 gene expression or protein function ( inst ) ; royalties from published books : cambridge university press and springer publishing dennis s . 
chi leadership : csurgeries stock and other ownership interests : bovie medical , verthermia , intuitive surgical , transenterix consulting or advisory role : bovie medical , verthemia ginger j . 
reis - filho consulting or advisory role : genentech , invicro , ventana medical systems , volitionrx , paige.ai , goldman sachs evis sala honoraria : siemens healthineers speakers ' bureau : siemens healthineers travel , accommodations , expenses : siemens healthineers no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
ca cancer j clin 68 : 7 - 30 , 2018 schwarz rf , ng ck , cooke sl , et al : spatial and temporal heterogeneity in high - grade serous ovarian cancer : a phylogenetic analysis . 
cell 173 : 1755 - 1769.e22 , 2018 bashashati a , ha g , tone a , et al : distinct evolutionary trajectories of primary high - grade serous ovarian cancers revealed through spatial mutational proling . j pathol 231 : 21 - 34 , 2013 5 . 
nat genet 48 : 758 - 767 , 2016 jim enez - s anchez a , memon d , pourpe s , et al : heterogeneous tumor - immune microenvironments among differentially growing metastases in an ovarian cancer patient . 
magn reson med 51 : 542 - 551 , 2004 guerini - rocco e , hodi z , piscuoglio s , et al : the repertoire of somatic genetic alterations of acinic cell carcinomas of the breast : an exploratory , hypothesisgenerating study . 
j pathol 237 : 166 - 178 , 2015 al - ahmadie ha , alden d , qin lx , et al : carbonic anhydrase ix expression in clear cell renal cell carcinoma : an immunohistochemical study comparing 2 antibodies . 
salgado r , denkert c , demaria s , et al : the evaluation of tumor - inltrating lymphocytes ( tils ) in breast cancer : recommendations by an international tils 12 . 
dowsett m , nielsen to , ahern r , et al : assessment of ki67 in breast cancer : recommendations from the international ki67 in breast cancer working group . int j gynecol pathol 34 : 437 - 444 , 2015 working group 2014 . 
detre s , saclani jotti g , dowsett m : a quickscore method for immunohistochemical semiquantitation : validation for oestrogen receptor in breast carcinomas . j clin pathol 48 : 876 - 878 , 1995 110 : 1030 - 1034 , 2018 15 . 
schultheis am , ng ck , de filippo mr , et al : massively parallel sequencing - based clonality analysis of synchronous endometrioid endometrial and ovarian cancer res 72 : 5454 - 5462 , 2012 carcinomas . 
the examination was performed on a 3t magnetic resonance imaging ( mri ) whole - body scanner unit ( discovery mr750 ; ge healthcare , chicago , il ) using a dedicated multichannel torso phased - array coil as the receive coil . the standard protocol included the following sequences acquired in two - dimensional t2 - weighted fast spin - echo , t1an axial plane : weighted gradient - echo . 
single - shot incoherent motion intravoxel ( ivim ) based diffusion - weighted images were obtained using echoplanar imaging with a pair of motion - probing gradients along three orthogonal axes , using a chemical shift selective fat - saturation technique . 
dynamic contrast - enhanced ( dce ) images were acquired before and after the intravenous injection of gadopentetate dimeglumine ( magnevist ; berlex laboratories , montville , nj ; 0.1 mmol per kilogram of body weight at a rate of 2 ml / s ) using an automatic injector ( medrad , bayer , pittsburgh , pa )  . 
the patient was scanned on a dedicated positron emission tomography ( pet ) / computed tomography ( ct ) system ( discovery 690 ; ge healthcare , chicago , il )  . 
a standard - of - care acquisition protocol was applied with an intravenous injection of approximately 400 to 455 mbq 18f - uorodeoxyglucose after at least 6 hours of fasting and documentation of blood glucose less than 200 mg / dl followed by a 60 - minute uptake period . 
subsequently , a low - dose , attenuation - correction ct scan ( 120 to 140 kv , approximately 80 ma ) was acquired with the patient in the supine position , followed by acquisition of pet emission images of the whole body ( 3 minutes per bed position , ve to six bed positions )  . imaging analysis and mr - pet coregistration . 
using anatomic landmarks available on axial t2 - weighted mr images and on the axial pet and low - dose ct images , the tumor regions outlined on mri were coregistered with pet . 
this was achieved by calculating the mean location ( corresponding to the center of mass of the tumor ) on the mri image ( t2w ) and the corresponding mean location on the pet / ct image . 
rigid registration was selected to ensure that the geometry ( and the voxel count ) of the region of interest ( roi ) for each slice was maintained between mri and pet . 
the translational matrix was applied to the roi for each slice to determine the displacement of the roi . the ivim biexponential model proposed by le bihan et al ( le bihan d , et al : radiology 168 : 497 - 505 , 1988 ; le bihan d , et al : radiology 161 : 401 - 407 , 1986 ; le bihan d , et al : magn reson med 10 : 324 - 337 , 1989 ) was used to estimate the diffusion parameters for each lesion outlined , including diffusion coefcient ( d ) and the volume fraction of the water owing through the microvessels ( f )  . 
the segmented analysis procedure ( callot v , et al : magn reson med 50 : 531 - 540 , 2003 ; yao l , et al : acad radiol 7 : 27 - 32 , 2000 ) was used to estimate ivim parameters on a voxel - wise basis . 
pharmacokinetic analysis of the dce data were carried out using a one - compartment tofts model ( tofts ps : j magn reson imaging 7 : 91 - 101 , 1997 )  . 
for each outlined lesion , voxel - wise estimates of the volume transfer constant between the blood plasma and the extravascular extracellular space ( ktrans [ min1 ] ) was calculated . 
arterial input function was calculated using a biexponent model as previously described ( weinmann hj , et al : physiol chem phys med nmr 16 : 167 - 172 , 1984 ; priest an , et al : magn reson med 63 : 1044 - 1049 , 2010 )  . gaussian smoothing was applied to all raw mr images before processing with variance of half a voxel , to smooth the parameters . 
for voxels that had estimated parameters that exceeded the bounds set by the tting curve , the values were set to nan ( not - a - number )  . 
once all voxels were tted , the voxels with nan value were replaced by an average of the surrounding voxels so that each voxel had an estimated parameter for the purpose of clustering . the standardized uptake values ( suv ) of the voxels contained within each lesion on 18f - uorodeoxyglucose pet was calculated based on the standard expression given by kinahan et al ( kinahan pe , et al : transl oncol 2 : 223 - 230 , 2009 )  . three - dimensional printing methodology . 
custom made threedimensional ( 3d ) molds were printed based on manual segmentation of the ovarian primary tumor and metastatic implants on the preoperative axial t2 - weighted mr images . 
the 3d model was then compared with the mr images and manually adjusted to resolve any discrepancies using meshlab ( meshlab , visual computing labisti - cnr ) , an extensible mesh processing system , aimed at editing and rendering unstructured 3d triangular meshes . 
the nal 3d models of each lesion were imported into openscad ( openscad , the openscad developers ) , 3d cad modeling software , which was used to create an internal cavity that exactly shaped each lesion according to the mri shape and contour . 
the slits for slicing each lesion were designed into the molds at 5 - mm intervals , which corresponded to the slice thickness and locations of the axial t2w fast relaxation fast spin echo mr images . 
carlo , md1 ; nabeela khan , md1 ; ahmet zehir , phd1 ; sujata patil , phd1 ; yasser ged , mbbs1 ; almedina redzematovic , ms1 ; devyn t . 
voss , md1 purpose nonclear - cell renal cell carcinoma ( nccrcc ) encompasses approximately 20% of renal cell carcinomas and includes subtypes that vary in clinical and molecular biology . 
compared with clear cell renal cell carcinoma , nccrcc demonstrates limited sensitivity to conventional vascular endothelial growth factor and mammalian target of rapamycindirected agents , indicating a need for better therapies . 
microsatellite instability ( msi ) in the tumor was investigated . results of 116 patients included in the analysis , 57 ( 49% ) presented with de novo metastatic disease , and 59 ( 51% ) presented with localized disease that later metastasized . 
of all tumors , 15 ( 13% ) had putative driver somatic alterations amenable to targeted therapies , including alterations in met , tsc1 / 2 , and an alk translocation . 
of 115 available tumors for analysis , two ( 1.7% ) had high and six ( 5% ) had intermediate msi status . conclusion the mutation proles of metastatic nccrcc vary by subtype . 
2019 by american society of clinical oncology introduction there are 63 , 000 estimated new patients diagnosed with renal cell carcinoma ( rcc ) annually in the united states and 14 , 000 deaths per year from advanced disease.1 the most common subtype of rcc is clear cell rcc ( ccrcc ) , which makes up approximately 75% to 80% of all rccs , with dened roles for targeted systemic therapy in localized and metastatic disease.2 the remaining histologic variants are collectively termed nonclear - cell rcc ( nccrcc ) and include papillary , chromophobe , collecting duct , translocationassociated , and unclassied types.3 comparing outcomes to ccrcc , cancer - specic survival is more favorable in patients with nccrcc with localized disease but tends to be worse in the metastatic setting.4 , 5 better treatments for metastatic nccrcc are clearly needed . 
a limited number of phase ii randomized trials have specically studied nccrcc . the espn ( everolimus versus sunitinib prospective evaluation in metastatic nonclear - cell renal cell carcinoma ) and aspen ( everolimus versus sunitinib for patients with metastatic nonclear - cell renal cell carcinoma ) trials compared the antivascular endothelial growth factor ( vegf ) agent sunitinib to the mammalian target of rapamycin ( mtor ) inhibitor everolimus as rst - line treatment of patients with nccrcc.6 , 7 per primary end point analyses , everolimus was not superior to sunitinib , but the heterogeneity of the study populations and the small sizes of variant subgroups limit the applicability of these data . 
these studies have highlighted the need for novel therapeutic approaches and a better understanding of how rcc biology differs among subtypes . increased knowledge of genomics may help identify novel treatment strategies . 
 carlo et al context ( nccrcc ) ? key objective what is the frequency of clinically actionable mutations in patients with advanced nonclear - cell renal cell carcinoma knowledge generated somatic mutation proles vary by nccrcc subtype . 
sequencing the tumor and germline and tumor microsatellite instability analysis reveal clinically actionable mutations in 22% of patients with advanced disease . relevance metastatic nccrcc can have a poor prognosis , and treatment is often extrapolated from clear cell renal cell carcinoma as a result of few studies that include this rare group of cancers . 
routine sequencing of nccrcc yields alterations such as high microsatellite instability , which may affect clinical management . marked responses to several targeted therapies when selected by molecular tumor features , rather than by tumor type.8 , 9 similarly , tumor microsatellite instability ( msi ) status is predictive of response to the antiprogrammed cell death protein 1 inhibitor pembrolizumab.10 indeed , msi status and defective mismatch repair are the rst molecular features linked to a regulatory agency approval irrespective of underlying disease histology . 
this study was approved by the mskcc institutional review board . ngs analysis tumor samples from either primary or metastatic sites were reviewed by genitourinary pathologists and microdissected for maximum tumor content for dna extraction . 
tumor and blood samples were sequenced using msk - impact , an ngs assay developed at mskcc that achieves hybridization capture with target - specic probes from exons of at least 341 cancer - associated genes , as described previously.13 mean depth of sequencing for the cohort was 660 . 
the gene panel is available in appendix table a1 . msi was quantied using msisensor.14 , 15 germline variants for 76 genes associated with cancer predisposition included in msk - impact were analyzed ( appendix table a1 )  . 
variants were classied by a clinical molecular geneticist or molecular pathologist as pathogenic , likely pathogenic , of uncertain signicance , likely benign , or benign , according to american college of medical genetics criteria.16 only pathogenic or likely pathogenic variants ( associated with disease causation and henceforth referred to as pathogenic variants ) are included in this analysis . somatic mutation clinical annotation somatic alterations were annotated through oncokb ( oncokb.org ) , a curated precision oncology knowledge base that stores information about the biologic function and therapeutic implications of individual gene alterations in a tumor typespecic manner . 
gene alterations that act as predictive biomarkers of response to specic targeted therapies are assigned a specic oncokb level of evidence . 17 levels 1 and 2a are us food and drug administration ( fda ) recognized or national comprehensive cancer network ( nccn ) listed biomarkers predictive of response to an fda - approved targeted therapeutic . 
msi - high ( msi - h ) status in solid cancers is considered oncokb level 1 , based on the fda approval of pembrolizumab.10 level 2b is a standard of care biomarker in another indication ( but not in rcc )  . 
mutations with level 4 assignment are those that are considered hypothetical biomarkers for which there is compelling biologic evidence that supports their being predictive of response to a drug and hence their potential use as eligibility criteria for clinical trials . statistical analysis clinical characteristics , somatic and germline results , and msisensor score are presented using descriptive statistics . objective response rate was dened as the best response according to response evaluation criteria in solid tumors ( recist ) , version 1.1. 
overall survival , dened as the time from diagnosis of metastatic disease to death or last known follow - up , was estimated using the kaplan - meier method . statistical analyses were performed using r version 3.5. results patient characteristics a total of 116 patients with metastatic nccrcc were included in this cohort ; demographics are listed in table 1 . median age was 53 years ( range , 12 to 77 years ) , and 67% of patients were male . 
patients with unclassied and papillary rcc had similar characteristics : most patients were male ( 78% and 89% , respectively ) and were diagnosed initially with localized disease , followed by subsequent recurrence . in comparison , most patients with chromophobe and translocation - associated rcc were female ( 53% and 69% , respectively )  . 
the median overall survival time for the cohort from time of diagnosis of metastatic disease was 34 months ( 95% ci , 24 to 59 months ) , with a median follow - up of 18 months . somatic mutation frequencies and clinically actionable somatic alterations most patients ( 57% ) had sequencing of the primary renal tumor . 
in comparison , in papillary tumors , the most frequent mutations were tert promoter mutations ( n = 12 ; 50% ) , followed by alterations in met ( n = 9 ; 38% ) and nf2 ( n = 2 ; 17% )  . chromophobe tumors had a distinct prole , with a high frequency of mutations in tp53 ( n = 10 ; 63% )  . translocation - associated tumors all had tfe3 translocations conrmed by uorescence in situ hybridization or ngs but had a paucity of other somatic alterations . we classied somatic alterations as potentially actionable per denitions previously established through oncokb.17 as summarized in table 2 , tumors of 15 patients ( 13% ) harbored an actionable , putative driver somatic mutation assigned an oncokb level of evidence of 2a , 2b , 3a , or 3b ( fig 1 and appendix table a3 )  . 
ten patients had mtor pathway alterations , including in pik3ca ( level 3 ; predictive of response to phosphatidylinositol 3 - kinase inhibitors ) , tsc1 / 2 ( level 2b ; predictive of response to nccn - listed everolimus ) , and mtor ( hypothetical predictor of response to mtor inhibitors ) .18 of these , six patients received an mtor inhibitor alone or in combination with bevacizumab or lenvatinib ( table 3 ) .19 an additional patient with a pten mutation ( level 4 ) was treated with bevacizumab and everolimus . 
median duration on treatment with an mtor inhibitor for the seven patients was 16 months ( range , 1 to 42 months ) , with one patient still on treatment ; three patients experienced a partial response ( all with predicted driver mtor pathway mutations ) , one had stable disease , and three were not evaluable . three patients had amplications in met ( level 3 ; possibly predictive of response to cabozantinib ) , and ve patients had additional driver mutations ; of these , two patients received the vegf and met inhibitor cabozantinib as second - line therapy and were evaluable for response . 
one patient had an alk translocation ( level 2b ; predictive of response to alk inhibitors in lung cancer ) , was enrolled onto a clinical trial with a multitarget alk inhibitor , and , as previously reported , achieved a partial response with 19 months on therapy.20 twenty - eight patients ( 24% ) had a level 4 alteration ( hypothetical biomarker , not proven to including mutations in pten , be clinically actionable ) , smarcb1 , cdkn2a , and atm ( figs 1b and 1c )  . fourteen patients had both the primary tumor and a metastatic lesion sequenced ( and one additional patient had two metastatic sites sequenced )  . 
of these , four patients ( 27% ) had a primary or metastatic site tumor sample with an actionable somatic alteration ( three with tsc2 and one with alk translocation ; appendix table a4 )  . 
additional patients received rst - line treatment elsewhere and are not included in this section . germline mutation analysis of the 116 patients , 45 ( 39% ) underwent germline mutation testing with a panel of 76 cancer - associated genes ; some of these patients were included in a previous report.21 in total , 11 ( 24% ) of 45 patients harbored germline events in cancer - associated genes . 
the most frequently germline mutated gene was fh ( n = 6 ; 13% ) , followed by one patient each who carried mutations in met , atm , chek2 , palb2 , and apc . 
 ( b ) percentages of tumors with somatic alterations by oncokb level of evidence , of tumors with oncogenic drivers without known potentially actionable alterations , and of tumors with no known driver . 
the tcga analyzed papillary and chromophobe tumors in two separate efforts.11 , 12 in contrast with the tcga analyses , where only primary tumors were processed , the patients in our study had primary and metastatic sites sequenced , perhaps better representing the limitations seen in clinic , where primary tumor tissue is either not available or not sampled . 
similar to these authors , 26 we found a predominance of met , tert promoter , and nf2 mutations in papillary tumors ( although unlike the pal et al26 study , we did not distinguish between type 1 and type 2 papillary tumors )  . 
this is consistent with a previous study that showed that nf2 loss in unclassied rcc may be a driver of tumorigenesis and associated with worse clinical outcome.27 the comparatively high proportion of unclassied patients , many with molecular similarities to patients with papillary rcc , reects the evolving denitions of rcc variant , with rccs previously termed high - grade papillary rcc now termed unclassied . using the oncokb classication to annotate individual mutations for their therapeutic potential , we found that 15% of tumors harbored potentially actionable somatic mutations . 
unlike in other cancers such as melanoma or nonsmall - cell lung cancer , in rcc , there are no fdarecognized or nccn - listed biomarkers predictive of response to therapies ( ie , level 1 oncokb ) ; the only exception is high tumor msi , which is predictive of response to pembrolizumab in any cancer type . 
we did nd 10 patient tumors ( 9% ) with a level 2 alteration , indicating a standard care biomarker predictive of response in an fda - approved drug in rcc or another indication . 
oncoprint of the most frequently mutated genes overall and microsatellite instability ( msi ) in tumors of 116 patients with advanced nonclear - cell renal cell carcinoma ( rcc )  . 
genetic alteration type , including germline pathogenic mutations , is indicated at the bottom of the oncoprint . included an alk translocation , met amplications , and tsc1 or tsc2 alterations . 
level 3 indicates compelling clinical evidence supporting the biomarker as predictive of response ( in this or other indication )  . * high microsatellite instability is classied as oncokb level 1 . alterations in mtor and pik3ca . 
most alterations were level 4 , which are hypothetical biomarkers potentially predictive of response on the basis of preclinical data . although these are not considered clinically actionable , they may be biomarkers and may be used as eligibility criteria for early - phase clinical trials . we explored the efcacy of targeted therapies in patients with alterations considered potentially actionable who had received matched treatment . 
although the number of patients was small , 33% of patients had an objective response , and an additional 25% had stable disease , which is notable in a group of diseases for which there are few effective therapies . 
patients with met alterations ( amplications or driver missense mutations ) who received cabozantinib and patients with mtor pathway driver alterations who received everolimus seemed to benet from therapy , such as a patient with a pik3ca driver mutation who had a partial response for more than 42 months on the combination of everolimus and bevacizumab . 
actionable somatic alterations and response to targeted treatment mutation predicted function effect * therapy length on therapy ( months ) best response patient ncc049 ncc108 ncc055 ncc024 ncc031 ncc112 ncc022 ncc051 ncc014 ncc019 ncc035 ncc115 met amplication met missense mtor missense pik3ca missense pik3ca missense tsc1 missense tsc1 truncating tsc2 missense tsc2 truncating alk translocation pten truncating pten truncating driver driver driver driver driver unknown driver unknown driver driver driver driver everolimus + bevacizumab cabozantinib cabozantinib lenvatinib + everolimus everolimus + bevacizumab everolimus + bevacizumab everolimus + bevacizumab everolimus everolimus entrectinib everolimus + bevacizumab everolimus + lenvatinib not evaluable not evaluable not evaluable not evaluable not evaluable note . 
two patients in our study , one with medullary rcc and one with chromophobe rcc , had high msi scores ; neither had received immunotherapy at the time of analysis . 
of interest , 29% of chromophobe tumors were msi - h ( msisensor score of 10 or greater ) or msi - i ( msisensor score between 3 and 9 )  . 
previous analyses of prevalence of msi - h in limited subtypes of nccrcc showed a 1% or lower prevalence of msi - h ; however , in these cohorts , less than 10% of patients had metastatic disease.11 , 12 , 30 , 31 additional investigation to characterize larger cohorts of chromophobe , medullary , and other nccrcc tumors , especially in patients with metastatic disease , is warranted . 
the overall low rate of msi - h in nccrcc should not preclude the possibility of benet from checkpoint inhibitors ; despite msi - h being rare in ccrcc , these tumors are clearly responsive to checkpoint hibitors.32 , 33 in addition , retrospective series in nccrcc table 4 . 
 ( % ) tumor subtype unclassied papillary chromophobe translocation other 1 ( 2 ) 1 ( 4 ) 4 ( 24 ) 1 ( 6 ) 1 ( 8 ) have suggested benet from antiprogrammed cell death protein 1 therapy.34 notably , consistent with previous reports , there was a high proportion of patients with germline mutations , some which could direct therapy.21 of 45 patients receiving germline genetic testing through our protocol , 13% had mutations in fh , which is diagnostic of the syndrome hereditary leiomyomatosis and rcc ( hlrcc ) , which in turn is associated with nccrcc and cutaneous and uterine leiomyomas.21 , 35 identication of patients with hlrcc has become particfor treatment decisions since the 2018 ularly relevant nccn guidelines added two bevacizumab - containing combination therapies ( bevacizumab plus everolimus and bevacizumab plus erlotinib ) as potential treatment for patients with hlrcc.36 in our exploratory analysis of response to bevacizumab and everolimus , most patients had an objective response , with a median progression - free survival nearing 12 months . 
in a phase ii study of a dual met / vegf receptor 2 inhibitor in patients with papillary rcc , the presence of a germline met mutation was highly predictive of response.37 one patient in our cohort harbored a met germline mutation , but although met - directed therapy with cabozantinib was initiated , the patient was subsequently lost to follow - up . of note , there was a high percentage of black patients with nccrcc ( 21% ) in this cohort . 
 carlo et al potential tumor genomic differences.38 , 39 these observations merit additional investigation in larger cohorts . this approach could have missed other nonexonic as well as epigenetic changes although this study represents a large cohort of patients with several subtypes of nccrcc , it is important to recognize its limitations . 
finally , our analysis was limited to targeted exome sequencing , and in summary , in this detailed genomic analysis of a wide array of metastatic nccrcc tumors , matched germline and tumor analyses revealed recurrent genomic events across rcc variants and suggest that a relevant proportion of patients harbor potentially actionable alterations . 
there is a need for additional collaborative studies to characterize metastatic nccrcc further so that targeted therapies can be pursued rationally , exploiting such information . affiliation 1memorial sloan kettering cancer center , new york , ny this manuscript . 
hyman consulting or advisory role : atara biotherapeutics , chugai pharma , cytomx therapeutics , boehringer ingelheim , astrazeneca , pzer , bayer , debiopharm group , genentech research funding : astrazeneca , puma biotechnology , loxo travel , accommodations , expenses : genentech , chugai pharma marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso rfp advisory committee , takeda , bristol - myers squibb , bayer , merck ( i ) research funding : loxo ( inst ) , helsinn therapeutics mark robson honoraria : astrazeneca , pzer consulting or advisory role : mckesson , astrazeneca , merck research funding : astrazeneca ( inst ) , myriad genetics ( inst ) , invitae ( inst ) , pzer ( inst ) , abbvie ( inst ) , tesaro ( inst ) , medivation ( inst ) travel , accommodations , expenses : astrazeneca chung - han lee consulting or advisory role : exelixis , eisai research funding : pzer ( inst ) , eisai ( inst ) , bristol - myers squibb ( inst ) , calithera biosciences ( inst ) , exelixis ( inst ) travel , accommodations , expenses : eisai darren r . 
motzer consulting or advisory role : pzer , novartis , eisai , exelixis , merck , genentech , incyte research funding : pzer ( inst ) , bristol - myers squibb ( inst ) , eisai ( inst ) , novartis ( inst ) , genentech ( inst ) martin h . 
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muller m , ferlicot s , guillaud - bataille m , et al : reassessing the clinical spectrum associated with hereditary leiomyomatosis and renal cell carcinoma syndrome in french fh mutation carriers . 
choueiri tk , vaishampayan u , rosenberg je , et al : phase ii and biomarker study of the dual met / vegfr2 inhibitor foretinib in patients with papillary renal cell carcinoma . 
 gene ctcf ctla4 ctnnb1 cul3 cxcr4 cyld cysltr2 daxx dcun1d1 ddr2 dicer1 * dis3 dnajb1 dnmt1 dnmt3a dnmt3b dot1l drosha dusp4 e2f3 egfl7 egfr * eif1ax ago2 eif4a2 eif4e elf3 ep300 epas1 epcam * epha3 epha5 epha7 ephb1 erbb2 erbb3 erbb4 ercc2 ercc3 ercc4 ercc5 oncogenomics of metastatic nonclear - cell renal cell carcinoma table a1 . 
this study aimed to describe the hr pathway mutations and hrd status and determine their association with treatment response and outcome in patients with pdac . patients and methods we performed a retrospective analysis of tumor samples from patients treated at indiana university for locally advanced or metastatic pdac . 
patients were included if they received gemcitabine plus nanoparticle albumin - bound paclitaxel ( control ) or fluorouracil , oxaliplatin , leucovorin , and irinotecan ( folfirinox ) and had adequate follow - up to assess survival and response to therapy . 
tumor analysis generated a three - biomarker hrd score and mutation data for 44 genes . results ninety - one samples met inclusion criteria , and 78 samples ( formalin - fixed paraffinembedded , n = 15 ; fine - needle aspiration , n = 63 ) generated mutation data . 
hrd analysis was successful for 57 samples ( hrd score : median , 18 ; range , 5 to 61 ) ; the primary cause of failure was low tumor cellularity . 
2018 by american society of clinical oncology introduction pancreatic ductal adenocarcinoma ( pdac ) is the fourth leading cause of cancer - related mortality in the united states.1 most patients present with advanced disease where palliative chemotherapy is minimally effective with high rates of toxicity , and the lack of meaningful benefit associated with targeted therapy continues to be a challenge.2 gemcitabine plus nanoparticle albumin - bound ( nab ) paclitaxel ( g + nab - p ) and fluorouracil , oxaliplatin , leucovorin , and irinotecan ( folfirinox ) are commonly used first - line treatment regimens for advanced disease , with objective response rates of 23% to 31% and median overall survival ( os ) times of , 1 year.3 , 4 kras and tp53 mutations remain the most common molecular abnormalities in pdac , 5 in the absence of effective therapy targeting these mutations . 
genomic analysis has revealed the presence of low - frequency , potentially actionable mutations in patients with pdac6 ; 15% of patients with pdac may carry a mutation in the safi shahda kirsten m . 
therefore , a score of 42 was not chosen as a cutoff in this study ; instead , we decided to evaluate the range of scores and correlate outcome based on hrd scores greater than and less than the median , without intending to establish the median as the cutoff . data collection data were retrieved from a retrospective database ( under a separate irb - approved protocol ) of patients who were diagnosed with pdac and who were partially or completely observed at our institution . 
the data were housed in an oncore ( forte research systems , madison , wi ) database per institutional guidelines . determination of radiographic response and outcome the principal investigator reviewed all images of eligible patients and analyzed response to therapy per response evaluation criteria in solid tumors ( recist ) v1.1. 
median follow - up time for the 16 patients without progression was 9 months ( 11 months for the six patients without progression who were alive at end of study )  . 
pfs and os were calculated from the time of initiating second - line therapy . tissue samples the direct smears prepared from the pancreatic fine - needle aspirates ( fna ) were screened by a cytopathologist ( a.a.i. ) to assure adequacy for molecular testing . 
 formalin - fixed paraffin - embedded ( ffpe ) cell blocks were prepared in a subset of the fnas . the hematoxylin and eosinstained sections cut from those blocks were also examined by a cytopathologist ( a.a.i. ) , and the block was considered acceptable for molecular testing if the estimated tumor cellularity was at least 20% . 
either the entire paraffin cell block or sections cut from the block ( one 4to 5 - mm hematoxylin and eosin slide followed by five consecutive 10 - mm unstained slides ) were submitted for analysis . tissue processing and dna extraction ffpe blocks and fna smears from pretreatment samples were retrieved . 
mutations identified were only included in the analysis if they were classified as deleterious or suspected deleterious on the basis of previously described criteria.21 to calculate the hrd score for samples analyzed by custom hybridization sequencing assay , reads covering snp positions were used to generate allelic imbalance profiles as described previously.14 hrd score was defined as the unweighted sum of loh , tai , and lst scores ( hrd = loh + tai + lst )  . statistical analysis clinical characteristics were compared between treatment groups using nonparametric methods ( wilcoxon rank sum or fishers exact test )  . 
response was coded as a binary variable ( complete response [ cr ] + partial response [ pr ] v stable disease [ sd ] + progressive disease [ pd ] or cr + pr v pd , unless otherwise noted ) , and logistic regression analysis was used to test association with clinical and molecular variables . 
hrd score was dichotomized at the median of 18 ( score , or > 18 ) , and median survival times were estimated using kaplan - meier curves compared by log - rank tests . 
all p values are two - sided , with significance set at p = .05. study approval and ethical considerations this was a retrospective analysis , and at the time of analysis , most patients had died as a result of the advanced nature of their illness . 
patients received care at the discretion of their treating oncologist , with genetic counseling and testing as deemed appropriate . results study population ninety - one patients met inclusion criteria , of whom seven had inadequate tissue for analysis after a second screening process by a pathologist from myriad genetics , 14 had ffpe tissue , and 70 had fna ( fig 1 )  . patients characteristics and treatment patient characteristics are listed in table 1 . 
summary of sample screening and number of samples used in the final analysis . hrd , homologous recombination deficiency . tumor samples ( n = 91 ) final clinical data merged with molecular results ( n = 84 ) inadequate tissue for molecular analysis ( n = 7 ) mutation screen and hrd score failed ( n = 6 ) mutation screen passed ( n = 78 ) brca1 / 2 mutation ( n = 6 ) brca1 / 2 wild type ( n = 72 ) hrd score failed ( n = 1 ) hrd score passed ( n = 5 ) hrd score failed ( n = 20 ) hrd score passed ( n = 52 ) mutant with no hrd score ( n = 1 ) mutants with hrd score ( n = 5 ) wild type with no hrd score ( n = 20 ) wild type with hrd score ( n = 52 ) 5 to 61 , with a median score of 18 . 
six brca1 / 2 mutants were detected in this cohort , and hrd score analysis was successful in five of six patients , with scores ranging from 13 to 61 and a median score of 44 . 
loss of the second allele of the mutant locus via either loh or a second deleterious mutation was observed in three of the six mutant samples , with hrd scores of 43 , 52 , and 53 , respectively . 
in comparison , the median hrd score observed in brca1 / 2 mutation carriers with breast or ovarian tumors was 65 , suggesting that the distribution of hrd scores may differ between pdac and these other tumor types , consistent with our preclinical observations . description of brca mutation functionality and pathogenicity six patients harbored brca mutations , four brca1 mutations and two brca2 mutations . individual mutations and hrd scores associated with those mutations are listed in table 2 . association of hrd with response to folfirinox for the purpose of this study we explored the following two scenarios , which were disease response defined as cr + pr versus sd + pd or cr + pr versus pd ( fig 2 )  . 
the composite variables that were assessed were any pathogenic mutation regardless of the status of the second allele and any brca1 / 2 mutation regardless of the status of the second allele against response , pfs , and os . 
in a subgroup analysis of metastatic status , with or without adjusting for treatment , hrd score was not significant for any of the outcomes ; however , the sample size was not large enough to test whether hrd behaves differently in these two groups . discussion this is the first study to our knowledge to evaluate the relationship between hr gene mutations , hrd score , and response to chemotherapy in patients with pdac . 
higher hrd score was correlated with brca1 / 2 mutations but was not associated with the presence of other hr brca1 mutation brca2 mutation brca1 / 2 wild type brca1 mutation brca2 mutation brca1 / 2 wild type fig 2 . 
 ( a ) complete response ( cr ) or partial response ( pr ) versus stable disease or progressive disease ( pd ) , and ( b ) cr or pr versus pd . 
distribution of homologous recombination deficiency ( hrd ) scores across samples of locally advanced ( la ) and metastatic pancreatic ductal adenocarcinoma ( pdac )  . max , maximum ; min , minimum ; qu , quartile ; sd , standard deviation . time from start of metastatic therapy ( months ) pathway mutations . 
one possible explanation for the absence of an elevated hrd score despite the presence of an hr pathway mutation is the retained functional allele in the affected genes . although conducted retrospectively , our study demonstrates the feasibility of performing genomic analysis on fna samples available from patients with pdac . 
on the contrary , however , this study also highlights the challenge of conducting correlative studies in patients with pdac ; most patients with pancreatic malignancies are diagnosed based on endoscopic ultrasound - guided fna only.22 in addition , high nontumor content , likely as a result of abundant desmoplastic stroma , often led to low dna content and thus a high assay failure rate . interestingly , we experienced a higher failure rate associated with core needle biopsy samples as opposed to fna samples , as a result of higher levels of nontumor dna content , even after macrodissection . 
 despite the low incidence of dna repair deficiency in pdac , it continues to represent an attractive target for drug development.23 several clinical trials using single agents or drug combinations are ongoing . 
in addition , patients with pdac tend to have a higher symptom burden and experience rapid progression after first - line therapy , frequently prohibiting second - line therapy.3 , 4 therefore , the optimal timing for testing such methods to select patients for subsequent therapies will likely be early in the disease process to inform secondline therapy.24 although our study does not address the presence of heterogeneity between the primary and metastatic lesions , some literature exists regarding hrd heterogeneity in other tumor types . for example , a study of patients with triplenegative breast cancer compared hr score in three different areas from the same primary tumor.25 overall , there was no significant difference among these samples , and the authors concluded that heterogeneity for hrd metrics was small and did not influence hrd score or status from three samples in the same tumor . whether hrd is more common in metastatic sites remains unknown in pdac ; however , a higher rate of germline mutations associated with dna repair genes ( without examining hrd score ) was found in metastatic prostate cancer when compared with localized disease.26 this study has limitations . 
it is a single - institution , nonrandomized , retrospective study comparing two commonly used chemotherapy regimens and including patients who had locally advanced and metastatic disease , which may carry different biology and represent a challenge in assessing response to therapy in locally advanced pdac . 
we had a relatively high assay failure rate in both fna and ffpe , although it was higher in the ffpe samples . in conclusion , this study did not demonstrate a correlation between hrd score and radiographic response to platinum - based therapy in patients with pdac . 
although hr gene mutations or hrd score may represent targets for drug development in pdac , larger prospective studies may be needed to evaluate the utility of these markers and their correlation with response to dna - damaging agents . 
for more information about ascos conflict of interest policy , please refer to or ascopubs.org / po / author - center . safi shahda consulting or advisory role : merrimack , bayer research funding : myriad genetics kirsten m . 
timms employment : myriad genetics stock and other ownership interests : myriad genetics patents , royalties , other intellectual property : austria ( e840080 , 3012329 ) , china pr ( zl 201280070358.0 ) , denmark , european patent convention , finland , france , great britain , ireland , the netherlands , spain , sweden , and switzerland ( 2582847 , 3012329 ) , germany ( 602011031723.7 , 3012329 ) , italy ( 502016000131029 , 3012329 ) , japan ( 6117194 ) , new zealand ( 625468 ) , united states ( 9 , 574 , 229 ; 9 , 279 , 156 ; 9 , 388 , 427 ) travel , accommodations , expenses : myriad genetics ashley a . 
 milan radovich no relationship to disclose sulfikar ibrahim no relationship to disclose brian allen employment : myriad genetics , grail stock and other ownership interests : myriad genetics , grail bert h . 
oneil , indiana university school of medicine , indianapolis ; ashley a . ibrahim and sulfikar ibrahim , indiana university health ball memorial hospital , muncie , in ; and kirsten m . 
moore mj , goldstein d , hamm j , et al : erlotinib plus gemcitabine compared with gemcitabine alone in patients with advanced pancreatic cancer : a phase iii trial of the national cancer institute of canada clinical trials group . j clin oncol 25 : 1960 - 1966 , 2007 3 . 
von hoff dd , ervin t , arena fp , et al : increased survival in pancreatic cancer with nab - paclitaxel plus gemcitabine . med 364 : 1817 - 1825 , 2011 n engl j med 369 : 1691 - 1703 , 2013 jones s , zhang x , parsons dw , et al : core signaling pathways in human pancreatic cancers revealed by global genomic analyses . 
risch ha , mclaughlin jr , cole de , et al : population brca1 and brca2 mutation frequencies and cancer penetrances : a kin - cohort study in ontario , canada . 
yang d , khan s , sun y , et al : association of brca1 and brca2 mutations with survival , chemotherapy sensitivity , and gene mutator phenotype in patients with ovarian cancer . 
mccabe n , turner nc , lord cj , et al : deficiency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deficiency among breast cancer subtypes . 
telli ml , timms km , reid j , et al : homologous recombination deficiency score predicts response to platinumcontaining neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
mills gb , timms km , reid je , et al : homologous recombination deficiency score shows superior association with outcome compared with its individual score components in platinum - treated serous ovarian cancer . 
 future of evidence synthesis in precision oncology : between systematic reviews and biocuration precision medicine refers to the tailoring of interventions to patients using approaches that go beyond traditional clinical characteristics ( eg , age , sex , disease , symptoms , and medical history ) by considering biomarkers consisting of genetic characteristics or molecular profiles.1 in particular , precision oncology ( po ) 2 includes both the development of novel cancer therapies targeting specific changes that occur in some individuals but not others ( eg , inherited mutations or somatic mutations that arise in the carcinogenesis process ) and the stratification of individuals according to existing interventions ( eg , via screening programs tiered by genetic risk or chemotherapies predicted to work for certain molecular profiles ) , which is expected to show improved outcomes in the resulting subgroups . 
 herein , we discuss two approaches for synthesizing evidence for or against the use of specific po interventions , namely , systematic reviews ( srs ) and biocuration , and argue that their engagement with each other could facilitate the timely delivery of appropriate po interventions . cancer is known to be highly heterogeneous , and clinical responses differ among patients . 
 po thus includes a wide variety of applications , including both the use of targeted therapies against particular changes occurring in individual tumorssuch imatinib against the bcr - abl fusion in chronic myeloid leukemia , 3 vemurafenib4 and dabrafenib5 against specific braf mutations in melanoma , and trastuzumab against her2 - postive breast cancer6and the assignment between existing therapy classes via biomarkers that are not direct drug targets . 
this can be based either on the activation of certain pathways , as in the case of egfr inhibitors in kras - wild type colon cancer , 7 , 8 or on gene expression signatures or other molecular characteristics ( ie , oncotype dx test for breast cancer , used to predict recurrence and likely benefit of chemotherapy ) .9 , 10 these biomarkers are well - established and have been approved by the us food and drug administration for specific cancer types . the biomarkers discussed in the previous paragraph are classified as having the highest level of evidence for clinical use in society guidelines ( eg , those jointly put forward by the association for molecular pathology , asco , and the college of american pathologists ) .11 to be meaningful for clinical decision making , biomarkers should have high predictive performance ( ie , they can be used to stratify patients into treatment groups with differential outcomes )  . 
most research to date , however , has assessed whether biomarkers are prognostic ( ie , are associated with a clinical outcome for untreated or standardof - care patients ) .12 it is often the case that the supporting literature includes few if any randomized control trials.13 as a result , lower levels of evidence may be assigned , eg , to biomarkers that predict response to a treatment based on well - powered studies evaluated by expert consensus or that predict response in a different tumor type than that being studied . many conceptual frameworks have been proposed to facilitate clinical decision making by helping end users ( especially patients and clinicians ) assess the evidence for or against the use of medical tests , including biomarkers.14 , 15 with minor variations , the different frameworks involve a stepwise approach that starts with analytic validity ( laboratory reproducibility ) , proceeds to clinical validity ( predictive accuracy , including sensitivity , specificity , and positive and negative predictive values ) and clinical utility ( use of the biomarker leads directly to improvements in outcomes like survival and quality of life ) , and eventually assesses the cost effectiveness of the biomarker . 
comparison of key features of systematic reviews and biocuration feature systematic reviews biocuration overall approach top down ; starts with a key scientific question and develops evidence base around it either top down or bottom up ; starts with a number of scientific questions or allows individual articles to be curated and slotted into categories evidence assessment exhaustive literature searches and systematic multiple frameworks exist assessment of evidence presence of bias systematic assessment of the risk of bias higher chance for bias by selecting studies with delivery approach peer - reviewed article or whitepaper research approach team usually assembled at the start of the project often relies on crowdsourcing and expert review of updating significant lag closer to real time , depending on availability of authors or curators multidisciplinary teams , often exclude or reduce role of primary study authors or subject matter experts due to risk of bias scientists and clinicians , who are frequently subject matter experts , from a variety of fields , and often with an expert panel to resolve conflicting interpretations significant findings database of entries may include summary of findings and links to original studies and other resources entries curators as with all tests in clinical practice , tests related to biomarkers are delivered within given health care settings , and currently , little structured evidence exists in regard to how po can successfully be implemented for particular sets of patients , with different degrees of access to health care , across diverse health care systems . 
the first is the traditional evidence appraisal that applies the well - established concepts of evidence - based medicine ( ebm ) .17 , 18 ebm integrates a physicians clinical experience with scientific evidence that has undergone an sr , which involves extensive surveying of the literature followed by a synthesis of the primary studies.19 the second is biocuration , which refers to the distillation and integration of biologic information from scientific literature and large data sets using databaseor research field specific , controlled vocabularies or ontologies ; it is a cornerstone of bioinformatics.20 both disciplines have the same overarching goal of bringing to patients only the interventions proven to be effective by carefully balancing benefits and harms , doing so in different ways ; srs start with a particular question and systematically develop the evidence base around it , whereas biocuration may be either top - down or bottom - up and usually involves more real - time updating . 
we compare key aspects of these two approaches in table 1 and summarize important feature of specific curated databases in appendix table a1 . the goal of srs is to allow a comprehensive and global view of the available evidence base on a particular question of interest by analyzing primary studies that meet prespecified eligibility criteria via explicit , reproducible methodologies that minimize bias . 
the typical steps involved in an sr include identification of the clinical question , specification of eligibility criteria , systematic search for all studies that meet these criteria , extraction of evidence from eligible studies and assessment of their methodologic rigor , and analysis and qualitative and / or quantitative synthesis ( meta - analysis ) of the extracted data.19 an sr is typically structured around the picots elements : the population toward which the findings will be applicable , the intervention , the comparisons being performed , the clinical outcomes , the timing of the eligible studies , and the clinical setting . 
during the course of decades , a toolbox of methods has been developed in srs and ebm to evaluate key elements of published studies including systematic biases , statistical precision , applicability to a target clinical setting , and others.21 - 23 evidence for specific interventions on the basis of supporting srs is generally considered strong . 
 clinical practice guidelines on the basis of srs that support the use of a genomic test as tier one ( ready to implement in clinical practice24 ) and those that are not based on srs as tier two ( may be useful in the context of informed clinical decision making24 )  . in general , sr teams are multidisciplinary , consisting of clinicians , content experts , methodologists , statisticians , and librarians . 
because researchers may often be influenced by their own investment in the field when interpreting the evidence base , 25 ideally , parties involved in a sr should have no personal vested interests in the topic of the sr . 
although content experts are critical for the clinical interpretation of primary studies and for putting them in context with the broader evidence , their role as authors in srs has been debated.26 however , since srs have various degrees of complexity , relevant sponsors often make decisions on a case - by - case basis by thoroughly reviewing the potential conflicts of individual researchers . 
for example , the agency for healthcare and research quality evidence - based practice centers program has a set of guidelines for how different types of conflicts should be handled and alleviated.27 given that precision medicine is a relatively new and rapidly evolving field with potentially more complex statistical analyses and contextual questions compared to traditional studies , including and relying on content experts is more critical . synthesis of evidence from po studies encounters a number of specific challenges . 
consider for instance a cochrane review of first - line treatments in individuals with egfr - mutated noncurable stage iiib to iv nonsquamous nonsmall - cell lung cancer , which included 19 rcts.28 the overall conclusion was that the tyrosine kinase inhibitor therapies ( erlotinib , gefitinib , and afatinib ) led to improved progression - free survival but not to improved overall survival , whereas the monoclonal antibody cetuximab did not show any improved outcomes . 
while this study included 19 rcts total , comparing targeted therapies to chemotherapy or best supportive care , the number of rcts conducted for each therapy was between two and eight and the study designs , outcome measures , and analyses performed and reported varied . 
srs have also identified existing evidence gaps for other prevision medicine interventions , such as the lack of robust evidence for tailoring smoking cessation interventions on the basis of germline genetic variation.29 many issues with the sr of evidence for po interventions will be solved in time , as more studies accumulate , but it is important to note that the desire for new therapies may be at a historical high given the stated promise of precision medicine and po in particular . 
however , another challenge that will linger is that the definition of precision medicine will continue to make it difficult to satisfy the picots framework as , for example , more drugs are tested separately in different subsets of patients ( eg , if the same biomarker is considered for different tumor types ) or molecular tests rapidly evolve to add more biomarkers or change how they are tested ( eg , protein expression , gene expression , or dna amplification ) .13 new rct designs such as umbrella and basket trials are now being implemented to meet some of these challenges . 
although other study designs may provide additional valuable information on specific treatments , the question of clinical utility , in particular , is difficult to answer in the absence of evidence from rcts . biocuration identifies and summarizes biomedical results , including potentially those from srs , into bioinformatic databases , often by using controlled vocabularies and prespecified standards.20 a text summary of the evidence related to specific scientific questions may also be included , along with links to the original studies or other resources . 
in particular , medical curation focuses on disease associations and genetic factors and includes efforts like the omim ( online mendelian inheritance in man ) database30 as well as specialized databases for particular genes , variants , and diseases . 
clinvar , a public archive of relationships among medically important germline and somatic variants and human phenotypes , was launched in april 2013.31 biocuration generally provides more immediate updating than formal srs , but the lack of a unified systematic framework may lead to only partial or inconsistent results . 
 curators , resulting in a wealth of information but also in issues such as contradictory interpretations and many variants of uncertain significance.32 the clingen ( clinical genome resource ) initiative aims to resolve some of these problems and answer the critical questions of clinical validity , disease causality ( pathogenicity ) , and clinical actionability by standardizing data collection and sharing and implementing an approach for consensus among expert curators.32 many other cancer - specific databases now exist for synthesizing evidence for po approaches , 33 - 37 leading clingen to recently develop recommendations and guidelines for defining cancer somatic variants on the basis of their diagnostic , prognostic , and predictive roles , using evidence of their significance and clinical utility.38 in a translational field such as po , where molecular genomics and clinical practice come together , a particular challenge for biocuration is that each content area has its own detailed terminology ( eg , specific diseases and syndromes can be described using icd - 10 codes39 and snomed terms40 )  . 
however , mapping these terminologies to specific causal mutations , as well as to biomarkers and tratments , can often be a challenge . biocurators come from a wide variety of backgrounds , usually in biology , biochemistry , or medical genetics , and increasingly have interdisciplinary training that includes computer and information sciences , with subject matter experts playing an important role in the field of biocuration.20 , 41 a growing number of clinical laboratories in hospitals and community clinics are now also conducting molecular diagnostic testing to identify sequence variants and inform treatment decisions for patients , in which case the curation is often performed by molecular pathologists as well as clinicians . 
the expert panels used by resources such as clingen to resolve conflicting interpretations and curate variants of unknown significance include medical professionals , medical geneticists , clinical laboratory diagnosticians and molecular pathologists that have a long standing scope of work in the disease gene in question . an example of a curated cancer database is the recently released civic ( clinical interpretation of variants in cancer ) database , 36 which provides associations between drugs and genes or variants in specific cancer types . 
however , the authors state the presence of a bias toward positive associations with treatment outcomes ( 91% of records show support for the use of a therapy ) , which illustrates the absence of a systematic , unbiased framework for identifying the evidence base . 
given that civic considers many different types of studies and that studies of cancer drugs may have many different designs , it is true that it would be extremely challenging to have a fixed list of terms that would be applicable to all studies and easily translatable into picots terminology . in general , literature searches for srs are typically more exhaustive and thorough than for curated databases , where eligible studies tend to be identified by experts in a given field . 
 although currently this may have little direct impact on identifying relevant studies for biocuration , given the small number of clinical po publications , this will eventually become a major issue in the next years , because the field will need to deal with increasing amounts of published and unpublished evidence . 
srs also tend to have more well - defined a priori eligibility criteria that a study has to meet to be considered in the evidence synthesis ; in contrast , biocuration approaches show more variability and rely more on individual experts in the field . 
although biocuration currently lacks a standardized and widely accepted framework to assess the quality of published evidence , several efforts are under way to change this.38 , 42 - 44 beyond trying to develop standardized frameworks for biocuration , a number of other approaches for improving curated databases have been considered , including the use of specific incentives . 
the emphasis on a systematic survey of the literature which includes non - significant results that is present in srs is also not an explicit part of the biocuration philosophy . 
for example , if the ebm community engages the biocuration community , they may find ways of incorporating more elements of the picots framework into existing and future databases . there is often a tension between systematic , unbiased syntheses and assessments versus timely and accessible curated information , and the highly promising field of po is a clear example that shows the difficulties in finding a good solution that considers both of these dimensions . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . approaches , and products , instead of continuing to proceed on parallel paths . 
curated databases will continue to be an initial first stop for many researchers and clinicians , especially because srs may lag years behind current studies , and decisions often need to be made in cases where srs are lacking . 
 however , more training is needed for users to understand that , for example , a higher risk of bias exists for finding more significant associations when consulting a curated po database than when using a sr . 
obrien sg , guilhot f , larson ra , et al ; iris investigators : imatinib compared with interferon and low - dose cytarabine for newly diagnosed chronic - phase chronic myeloid leukemia . 
hauschild a , grob j - j , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
slamon dj , leyland - jones b , shak s , et al : use of chemotherapy plus a monoclonal antibody against her2 for metastatic breast cancer that overexpresses her2 . 
de roock w , piessevaux h , de schutter j , et al : kras wild - type state predicts survival and is associated to early radiological response in metastatic colorectal cancer treated with cetuximab . 
calonge n , klein rd , berg js , et al : recommendations from the egapp working group : does the use of oncotype dx tumor gene expression profiling to guide treatment decisions improve outcomes in patients with breast cancer ?  . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
panagiotou oa , ioannidis jp : primary study authors of significant studies are more likely to believe that a strong association exists in a heterogeneous meta - analysis compared with methodologists . 
greenhalgh j , dwan k , boland a , et al : first - line treatment of advanced epidermal growth factor receptor ( egfr ) mutation positive non - squamous non - small cell lung cancer . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
hunter je , irving sa , biesecker lg , et al : a standardized , evidence - based protocol to assess clinical actionability of genetic disorders associated with genomic variation . 
strande nt , riggs er , buchanan ah , et al : evaluating the clinical validity of gene - disease associations : an evidence - based framework developed by the clinical genome resource . 
uniprot is not disease focused ; omim , clinvar , and clingen are disease agnostic ; the remaining databases are specific to cancer . abbreviations : asco , american society of clinical oncology ; civic , clinical interpretation of variants in cancer ; clingen , clinical genome resource ; cosmic , catalogue of somatic mutations in cancer ; fda , us food and drug administration ; nccn , national comprehensive cancer network ; nih , national institutes of health ; omim , online mendelian inheritance in man ; po , precision oncology . 
nucleic acids res 43 : d204 - d212 , 2015 . landrum mj , lee jm , benson m , et al : clinvar : public archive of interpretations of clinically relevant variants . 
nucleic acids res 44 : d862 - d868 , 2016 forbes sa , beare d , boutselakis h , et al : cosmic : somatic cancer genetics at high - resolution . 
nucleic acids res 45 : d777 - d783 , 2017 . taylor ad , micheel cm , anderson ia , et al : the path ( way ) less traveled : a pathway - oriented approach to providing information about precision cancer medicine on my cancer genome . 
riedlinger , md , phd1 ; aleksander chojecki , md1 , 2 ; hana aviv , phd1 ; david weissmann , md1 ; sonali joshi , ms1 ; susan m . 
hirsheld , md , phd1 , 3 ; and shridar ganesan , md , phd1 introduction the 2016 revision to the who classication of myeloid neoplasms and acute leukemia added myeloid or lymphoid neoplasms with pcm1 - jak2 as provisional entities.1 the t ( 8 ; 9 ) ( p22 ; p24.1 ) translocation was rst described in a patient in 1990 , 2 and this cytogenetic abnormality was subsequently found to result a pcm1 - jak2 fusion gene in 2005.3 approximately 50 patients with lymphoid or myeloid neoplasms associated with t ( 8 ; 9 ) ( p22 ; p24.1 ) pcm1 - jak2 have been reported , and these neoplasms have had an array of presenting diagnoses.4 , 5 common features associated with this translocation are a male predominance , hepatosplenomegaly , and eosinophilia . 
one of the initial reports in the literature describing the t ( 8 ; 9 ) ( p22 ; p24 ) translocation was found in the cutaneous t - cell lymphoma of a patient who initially was reported to have lymphomatoid papulosis , followed by a diagnosis of hodgkin disease , with evidence that all three of these diseases were derived from a common t - cell clone.6 here , we report what we believe is the second patient harboring the pcm1 - jak2 fusion with a history of cutaneous t - cell lymphoma who was later diagnosed with classic hodgkin lymphoma . 
the patient had a left axillary lymph node biopsy performed in may 2010 , which was diagnosed as dermatopathic lymphadenopathy , with t - cell receptor rearrangement studies detecting a clonal t - cell population suggestive of minimal involvement by t - cell lymphoma despite unremarkable morphologic and immunophenotypic ndings . 
computed tomography scan at this time showed multiple enlarged lymph nodes in the chest , abdomen , and pelvis . skin biopsy of the right abdomen during this workup was highly suggestive for a cutaneous t - cell lymphoma , with the vast majority of cells positive for cd3 and cd4 and virtually negative for cd7 and cd8 and a clonal t - cell population detected by t - cell rearrangement studies . 
the patient received eight cycles of bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisone chemotherapy from december 2012 to july of 2013 and did not receive any radiation therapy . 
in june 2015 , the skin condition worsened and became pruritic with a cervical lymph node with increased uptake noted on positron emission tomography scan . two lymph nodes from the right axillary region were biopsied , with one lymph node showing a nodular lymphoid inltrate divided by thick collagenous bands and numerous large atypical cd30 + cells but only a few with reed - sternberg cells or mononuclear variants ( fig 1 )  . 
 ( d ) a 2015 left back skin biopsy showing a brotic , partially necrotic nodule with overlying skin with a dense subepidermoid lymphoid inltrate consistent with cutaneous t - cell lymphoma . biopsy performed at that time showing cutaneous t - cell lymphoma showed the same t - cell clone . 
after completing this therapy , the patient was felt to be stable for approximately 11 months before possible recurrence of transformation of disease with adenopathy in the inguinal region in july 2017 . the patients last scan was september 2017 , which revealed stable disease . 
tissues from the axillary node from december 2012 diagnosed as classic hodgkin lymphoma , nodular sclerosis subtype ; from the axillary lymph node from june 2015 with large atypical cells favored to be cutaneous t - cell lymphoma ; and from the skin from the axillary region in june 2015 diagnosed as cutaneous t - cell lymphoma were all sent for comprehensive genomic proling in june and july of 2015 ( foundation medicine , cambridge , ma )  . 
all three samples showed pcm1 - jak2 fusions and identical single nucleotide variants of unclear function in six genes ( prkdc a1680v , brca2 t2515i , nfe2l2 a480v , cux1 q191p , epha5 g409d , and flt1 s722del ) , which supports these being different manifestations of the same disease process . 
the pcm1 - jak2 fusion is reported to be sensitive to jak inhibitors in vitro , and there is a report of a patient with chronic eosinophilic leukemia harboring this fusion who experienced complete cytogenetic remission after treatment with ruxolitinib.7 the genomic proling results from this patient were presented at our institutional molecular tumor board , with the recommendation for treatment with a jak inhibitor on disease progression . subsequent uorescence in situ hybridization studies performed on the specimen diagnosed as classic hodgkin lymphoma and specimen with large atypical cells favored to be cutaneous t - cell lymphoma showed separation of a jak2 probe indicating a translocation had taken place ( appendix fig a1 )  . 
fish performed in april 2018 showed jak2 rearrangement . completed 16 cycles of brentuximab . august 2016 right axillary lymph node 1 favored to be large - cell transformation of t - cell lymphoma . 
genomic profiling performed in july 2015 with pcm1 - jak2 . fish performed in april 2018 showed jak2 rearrangement . stopped bexarotene and started brentuximab . right axillary lymph node 2 suggestive of involvement of cutaneous t - cell lymphoma . 
clonal t - cell receptor . genomic profiling performed in july 2015 with pcm1 - jak2 rearrangement . inguinal region adenopathy , but otherwise stable disease . subsequently lost to follow - up . 2000 2009 may 2010 may 2014 june 2015 july 2017 fig 2 . 
beacopp , bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisone ; fish , uorescence in situ hybridization ; puva , psoralen and ultraviolet a . the right axillary lymph node atypical nodular lymphoid inltrate and skin biopsy showing cutaneous t - cell lymphoma in june 2015 ( fig 3 )  . 
in total , these results argue that the same underlying disease process was present beginning in may 2010 and potentially earlier and was responsible for all of the patients subsequent lymphoproliferative disorders , including the specimen diagnosed as classic hodgkin lymphoma in december 2012 , which instead seems to have been a cd30 + t - cell lymphoma . discussion comprehensive genomic proling is now routinely performed at major academic medical centers with a major identifying clinically actionable alterations.8 goal of another benet of genomic proling is that repeat testing of specimens from a patient can indicate if they the same underlying clonal process , are a result of possibly with tumor evolution as a result of resistance to therapy , or are the result of separate primary clonal disorders.9 - 11 classic hodgkin lymphoma is dened by the presence of reed - sternberg cells . 
nodular sclerosing is the most common subtype and is characterized by the presence of rare , scattered lacunar reed - sternberg cells , which often compose less than 1% of the tumor cell mass , in a background of reactive lymphocytes , eosinophils , plasma cells , and brosis . 
reed - sternberg cells in classic hodgkin disease are generally believed to originate from b cells , but there are reports that a small fraction may arise from t cells , incidence as low as 1% to 2%.12 , 13 inwith an overall terestingly , several reports in the literature describing hodgkin lymphoma of t - cell derivation report an association with cd30 + lymphoproliferative disorders , whose atypical cells often have a similar morphology to reedsternberg cells.6 , 14 , 15 in addition to the pcm1 - jak2 fusion , two cases of classic hodgkin lymphoma that lacked the b - cell lineage marker pax5 and were positive for tia1 have been reported to harbor an sec31a - jak2 fusion . 
the sec31a - jak2 fusion caused a lethal t - cell lymphoblastic lymphoma and myeloid phenotype in a murine model.16 additional uncharacterized jak2 rearrangements have been reported in lymphomas diagnosed histologically as classic hodgkin lymphoma.17 it is possible that a small fraction of tumors histologically classied as hodgkin disease actually are cd30 + t - cell lymphomas , which may have different optimal treatment strategies and prognosis than standard hodgkin disease . 
in addition to pcm1 - jak2 , sec31a - jak2 is also reported to respond to jak inhibitors , and other jak2 rearrangements may also be targetable with these agents . 
studies of t - cell receptor gene rearrangement were performed on the ( a ) 2010 left axillary lymph node , ( b ) 2012 left axillary lymph node biopsy diagnosed as nodular sclerosing classic hodgkin lymphoma , ( c ) 2012 right abdomen skin biopsy , ( d ) 2015 right axillary lymph node favored to be nodal involvement of the patients t - cell lymphoma , and ( e ) 2015 left back skin biopsy involved by cutaneous t - cell lymphoma . 
a similar clonal product of approximately 263 base pairs ( bp ) was detected using the t - cell receptor v beta and j beta 1 / 2 primer set in all of the samples except the 2010 specimen and the 2012 classic hodgkin lymphoma , which were polyclonal ( left column )  . 
riedlinger , md , phd , rutgers cancer institute of new jersey , 195 little albany st , new brunswick , nj 08901 ; e - mail : gr338@ cinj.rutgers.edu. support supported by national institutes of health grant no . 
riedlinger honoraria : mjh healthcare holdings , gerson lehrman group consulting or advisory role : personal genome diagnostics hana aviv patents , royalties , other intellectual property : patent for markers to detect transformation of barrett esophagus into esophageal adenocarcinoma ( inst ) kim m . 
hirsheld employment : merck stock and other ownership interests : merck travel , accommodations , expenses : merck shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis , roche , foghorn therapeutics , foundation medicine patents , royalties , other intellectual property : i hold two patents for digital imaging that may be licensed to ibris and inspirata travel , accommodations , expenses : inspirata no other potential conicts of interest were reported . references arber da , orazi a , hasserjian r , et al : the 2016 revision to the world health organization classication of myeloid neoplasms and acute leukemia . 
blood 127 : 2391 - 2405 , 2016 stewart k , carstairs kc , dub e id , et al : neutrophilic myelobrosis presenting as philadelphia chromosome negative bcr non - rearranged chronic myeloid leukemia . 
cancer res 65 : 2662 - 2667 , 2005 bain bj , ahmad s : should myeloid and lymphoid neoplasms with pcm1 - jak2 and other rearrangements of jak2 be recognized as specic entities ? br j haematol 166 : 809 - 817 , 2014 tang g , sydney sir philip jk , weinberg o , et al : hematopoietic neoplasms with 9p24 / jak2 rearrangement : a multicenter study . 
mod pathol 32 : 490 - 498 , 2019 davis th , morton cc , miller - cassman r , et al : hodgkins disease , lymphomatoid papulosis , and cutaneous t - cell lymphoma derived from a common t - cell clone . 
n engl j med 326 : 1115 - 1122 , 1992 lierman e , selleslag d , smits s , et al : ruxolitinib inhibits transforming jak2 fusion proteins in vitro and induces complete cytogenetic remission in t ( 8 ; 9 ) ( p22 ; p24 ) / pcm1 - jak2 - positive chronic eosinophilic leukemia . 
oncologist vignot s , frampton gm , soria jc , et al : next - generation sequencing reveals high concordance of recurrent somatic alterations between primary tumor and metastases from patients with non - small - cell lung cancer . 
foss hd , reusch r , demel g , et al : frequent expression of the b - cell - specic activator protein in reed - sternberg cells of classical hodgkins disease provides further evidence for its b - cell origblood 94 : 3108 - 3113 , 1999 13 . 
willenbrock k , ichinohasama r , kadin me , et al : t - cell variant of classical hodgkins lymphoma with nodal and cutaneous manifestations demonstrated by single - cell polymerase chain reaction . 
 ( a ) a 2012 left axillary lymph node biopsy diagnosed as nodular sclerosing classic hodgkin lymphoma showed translocation involving the jak2 gene on chromosome 9p24.1 in 62% of 100 interphase cells . 
 ( b ) in the 2015 right axillary lymph node favored to be nodal involvement of the patients t - cell lymphoma , jak2 translocation was detected in 13% of 100 interphase cells . 
with the jak2 break - apart probe , the normal pattern appears as fusion of red and green ( yellow ) , whereas a translocation shows up as red and green separated on one or more chromosomes 9 . 
 temporal dynamics of genomic alterations in a brca1 germline mutated pancreatic cancer with low genomic instability burden but exceptional response to fluorouracil , oxaliplatin , leucovorin , and irinotecan hui - li wong eric y . 
this approach helped to reconcile the following paradoxical findings : genomic stability and low hrd mutation signature despite a germline brca1 mutation and exceptional response to fluorouracil , oxaliplatin , leucovorin , and irinotecan ( folfirinox )  . 
the primary tumor had been resected previously , followed by 6 months of adjuvant cisplatin and gemcitabine chemotherapy , before detection of liver metastases 12 months after surgery and within 6 months after discontinuing chemotherapy . 
the patient had an excellent response to treatment , with ca19 - 9 halving in 2 months and a complete positron emission tomography response within 4 months ( fig 1a )  . 
renouf , md , mph , british columbia cancer agency , 600 w 10th ave , vancouver , bc v5z 4e6 , canada ; twitter : @zhaoez , @bccancerfdn , @ubcmedicine ; e - mail : drenouf@bccancer.bc.ca. methods mutation signature and timing analysis sample processing , sequencing , and bioinformatics tissue from the primary pancreatic tumor and liver metastasis was sequenced along with matched normal blood . 
the primary samples low tumor content necessitates careful interpretation of variant calls along with orthogonal validation of key findings . patterns of somatic structural variants ( svs ) , single nucleotide variants ( snvs ) , and copy number variants ( cnvs ) were interrogated to determine the contribution of hrd to mutagenesis . 
timing started folfirinox stopped oxaliplatin ( 16 cycles ) complete response on pet week 1 week 20 time since diagnosis of metastatic pdac ( weeks ) 0 1 2 0 1 2 8 6 7 8 6 7 fig 1 . 
within 4 weeks of commencing fluorouracil , oxaliplatin , leucovorin , and irinotecan ( folfirinox ) , ca19 - 9 decreased by > 50% ; positron emission tomography ( pet ) complete response was seen at 20 weeks . 
verification of signit signatures and temporal dissection was performed using deconstructsigs with temporal partioning of mutations into early and late categories ( data supplement ) as described previously.16 data availability wgs data ( binary alignment map files ) have been submitted to the european genome - phenome archive17 under the study accession number egas00001001159 and sample accession egad00001003029 . results brca1 loss in the primary and metastasis both the primary tumor and the metastasis demonstrated low sv burden , which falls into the stable category defined by waddell et al , 18 and possessed < 50 sv events ( figs 1b to 1c )  . 
to our knowledge , this is the first biologic validation of a mutation timing inference model using multiple sequencing time points . metastasis and the 17th of 41 events ( 0 = 0.40 ) in the primary ( figs 2c and 2d )  . 
tumor content in the pancreatic primary was insufficient to estimate clonality . evolution of mutation signatures from primary to metastasis the relative contributions of 30 previously described mutation signatures12 were determined from 5 , 683 snvs in the primary and 8 , 315 in the metastasis . 
signature 3 and , to a lesser extent , signature 8 have been associated with hrd.20 , 21 mutations associated with signature 3 rose by 1 , 593 in the metastasis , and signature 8 rose by 1 , 424 , more than any other signature ( fig 3a )  . 
furthermore , of new somatic mutations ( present in the metastasis but absent in the primary tumor ) , 26% were associated with the hrd signature ( fig 3b ) , which suggests major involvement of hrd - associated mutagenesis in the evolution of this pdac . 
strong signature bleed was observed between signatures 3 and 8 ( data supplement ) , but there was little bleed between hrd and other signatures . evolution of orthogonal hrd - associated mutational signatures the presence of recently described genomic signatures associated with hrd21 was investigated in the primary and metastasis . 
rearrangement signatures 3 and 5 ( fig 4a ) and the fraction of indels with microhomology ( fig 4b ) were low but rose between the primary and the metastasis . 
 the hrd composite score , combining loh , telomeric allelic imbalance , and large - scale transition , increased from 30 in the primary to 38 in the metastasis ( fig 4c )  . mutation signature timing the cnloh event on chromosome 17 that resulted in homozygosity of brca1 was the ninth earliest of 30 events ( 0 = 0.15 ) in the analysis with signit revealed the evolution of mutation signatures between two tumor subpopulations . 
 ( a ) inferred timing of copy change events in the primary tumor and metastasis were strongly correlated , with a slope of 0.45 , intercept of 0.02 , r = 0.7 , and p < .001. 
the loss of heterozygosity event encompassing brca1 has been highlighted , and is the 17th earliest of 41 inferred events in the primary and ninth of 30 events in the metastasis . 
these early mutations accounted for 36% of mutations , whereas later mutations made up 64% . the early subpopulation was dominated by signature 1 , which accounted for 59% of early mutations , whereas signatures 3 , 8 , 9 , and 16 were active in the later subpopulation . 
 ( b ) the complete catalog of new somatic snvs ( present in metastasis but absent in primary tumor ) , with snvs categorized into 96 classes on the basis of variant type and 3 / 5 context , was matched against 30 predefined mutation signatures . 
 ( c ) temporal dissection by signit revealed two tumor subpopulations , which revealed a drop in signature 1 and a rise in signatures 3 and 8 . signatures 3 , 8 , and 9 from the primary to the metastatic sample . 
these findings provide additional evidence that hrd remains an active mutation - causing process in the metastatic tumor , despite the overall low sv burden and moderate hrd signature exposure . discussion previous studies have reported platinum sensitivity in pdacs with brca1 / 2 mutations , rampant svs , and strong mutation signature.18 we explored the genomic evolution of a brca1 germlinemutated pdac with paradoxically low hrd mutation signature and sv burden . 
on the basis of temporal analysis of mutational signatures , we postulate that hrd onset may have occurred too recently or gradually to produce a heavy burden of genomic instability . 
however , rising hrd signature exposure suggests that hrd remains a currently active process , which may explain the patients excellent and sustained response to folfirinox . this analysis has some limitations . 
the archival primary sample had low tumor content ( 25% ) , which is known to limit the accuracy of mutation calling , and thus required analytical validation of the major findings . 
snvs were called by strelka , which is designed to operate under low cellularity.22 despite the low tumor content , timing of cnvs was concordant between the primary and metastasis , and temporal dissection of the metastasis corroborated mutation signature evolution patterns . of note , the patient did not exhibit a dramatic response to adjuvant cisplatin and gemcitabine therapy in the primary setting . 
another explanation is mechanistic differences between cisplatin and oxaliplatin action , 23 which may limit cross - resistance between them as corroborated by differing activities of the two agents across cancer types . 
should the disease progress on folfirinox , we intend to perform a follow - up screening for brca1 reversion27 and associated hrd dynamics . there is growing evidence that hrd may predict response to platinum - based therapy and poly ( adp - ribose ) polymerase inhibitors . 
 ( c ) the total hrd score rose from 30 to 38 , largely driven by a rise in loss of heterozygosity ( loh ) and large - scale transitions ( lsts )  . 
morin consulting or advisory role : epizyme janessa laskin honoraria : boehringer ingelheim , roche canada , astrazeneca , pfizer research funding : astrazeneca ( inst ) , roche canada ( inst ) marco a . 
renouf honoraria : celgene , shire consulting or advisory role : celgene , shire research funding : bayer ag ( inst ) , astrazeneca ( inst ) acknowledgment we thank the patient and his family for participating in the personalized oncogenomics program of british columbia . 
is supported by a bcca - cihr - ubc / phd studentship , a university of british columbia 4 - year doctoral fellowship , and a canadian institutes of health research vanier canada graduate scholarship . references res 18 : 99 - 113 , 2008 nature 408 : 429 - 432 , 2000 1 . 
tutt a , tovey h , cheang mcu , et al : carboplatin in brca1 / 2 - mutated and triple - negative breast cancer brcaness subgroups : the tnt trial . 
laskin j , jones s , aparicio s , et al : lessons learned from the application of whole - genome analysis to the treatment of patients with advanced cancers . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deficiency among breast cancer subtypes . 
ha g , roth a , khattra j , et al : titan : inference of copy number architectures in clonal cell populations from tumor whole - genome sequence data . 
boot a , huang mn , ng awt , et al : in - depth characterization of the cisplatin mutational signature in a human cell lines and in esophageal and liver tumors . 
 sequential her2 - targeted therapy in salivary ductal carcinoma with her2 / neu overexpression and a concomitant erbb2 mutation introduction salivary duct carcinoma ( sdc ) is a rare malignancy arising from the major and minor salivary glands.1 , 2 though curative intent surgery followed by radiation is the treatment of choice , locoregional recurrences and distant metastases are frequently reported.1 , 3 cytotoxic chemotherapeutic agents such as platinum analogs , anthracyclines , and taxanes have been effective in treating sdc but there is no established standard of care.4 overexpression of her2 / neu is frequently seen ; thus , trastuzumab can be an effective treatment option.3 however , the role of other her2 - targeting agents after trastuzumab failure is unclear . 
this involved a multiplex polymerase chain reaction using the ion ampliseq cancer hotspot primer pool and the ion ampliseq library kit ( both from thermo fisher scientific , waltham , ma )  . 
 data files were analyzed using the ion torrent variant caller software and integrated genomic viewer ( thermo fisher scientific ) using hg19 reference sequence and nextgene software ( softgenetics , state college , pa )  . 
in addition , three possible germline polymorphisms ( met n375s , tp53 p72r , and flt c.1310 3t > c ) were also detected in the tumor specimen . the patient was treated postoperatively with concurrent radiation to the parotid bed and right neck ( 6 , 600 cgy in 33 fractions over 48 days ) , with high - dose cisplatin ( 100 mg / m2 every 3 weeks for two cycles ) as radiation sensitizer . 
 he underwent a left modified radical neck dissection followed by concurrent radiation ( 6 , 000 cgy in 30 fractions over 42 days to the left neck and 6 , 600 cgy in 33 fractions over 48 days to the axilla ) with weekly carboplatin ( area under the curve , 2 ) because of marginal renal function . 
he had a possible anaphylactic reaction to pertuzumab and hence received trastuzumab monotherapy for seven additional cycles and had a partial response . the patient was disease free for 6 months and then a biopsy - proven recurrence was found on his sk lapatinib treatment was restarted and continued for 9 months ; there was a complete clinical response in his sk the patient is currently on a drug holiday , with no obvious recurrence . 
biopsy - proven skin recurrence of salivary duct carcinoma with complete resolution with lapatinib treatment . two years after the initial recurrence , the patient underwent a wedge resection of a solitary metastasis in the right lower lobe of the lung . nine months later , disease progression was detected in the right axillary and mediastinal lymph nodes . 
 however , because of the response of the sdc to her2 - targeted therapies.3 her2 overexpression is associated with higher recurrence risk , shorter survival , and aggressive clinical behavior with early regional and distant metastasis.2 taxanes and trastuzumab have been used anecdotally in metastatic sdc with her2 / neu overexpression with a good response , 7 but the role of targeted therapy remains unclear . in this case report , we have demonstrated the successful sequential use of her2 - targeted therapy in her2 - overexpressing metastatic sdc . 
after an initial response to trastuzumab docetaxel combination therapy , her2 - targeted agents , with differing mechanisms of action , were used sequentially with good response and prolonged disease control . 
the patient received , sequentially , trastuzumab ( which binds to the extracellular segment of the her2 receptor , neutralizing it and also producing antibody dependent cellular cytotoxicity ) , lapatinib ( which binds to the atp - binding pocket of the her2 protein kinase domain and inhibits tyrosine kinase activity ) , and ado - trastuzumab emtansine ( an antibody - drug conjugate in which trastuzumab inhibits the her2 receptor and the cytotoxic maytansinoid portion of the conjugate is delivered intracellularly and produces cell death )  . 
also , to the best of our knowledge , this is only the second report of ado trastuzumab emtansine use in sdc8 and the first describing sequential her2 targeting in this disease . sequential her2 - directed therapy is well established in metastatic her2 - positive breast cancer , with frontline chemotherapy along with dual her2 - targeted therapy with trastuzumab and pertuzumab followed by other her2 targeted agents.9 a higher absolute erbb2 gene copy number results in shorter time to metastasis in trastuzumab - untreated early breast cancer but longer progression - free survival upon initiation of trastuzumab - based treatment.10 though her2 - positive tumors are highly sensitive to the receptor blockade , resistance has been shown to develop through three main mechanisms : ( 1 ) incomplete blockade as a result of redundant ligands and receptors that enable alternative dimerization patterns ; ( 2 ) reactivation of pathway signaling at or downstream of the receptor layer , such as activating mutations in the pik3ca pathway ; and ( 3 ) use of pre existing or acquired alternate pathways , such as hormone - receptor pathways.11 interestingly , the patient in this case report had an erbb2 v777l mutation in a metastatic specimen before exposure to her2 - targeted therapy . 
the incidence of erbb2 mutations in sdc is uncommon , with a recent series reporting a mutation in four of 37 patients studied.12 all these mutations were in exons 17 through 19 ( namely , i767m , d769y , g776v , and v842i ) , but this series did not identify the v777l mutation . 
the coexistence of her2 amplification and her2 mutation is extremely uncommon because most of the her mutations reported in breast cancer have been seen in patients with her2 neu amplification - negative disease.13 there are limited data on the role of this mutation in breast cancer . 
v777l is present in the proximity of the kinase domain dfg motif of the erbb2 gene ( exon 20 ) and functions as an activating mutation.13 the effects of the erbb2 v777l mutation on response to her2 - targeted therapy are less clear . 
some in vitro studies suggest that this mutation did not affect the sensitivity to her2 - directed therapies in proliferation assays13 ; however , a recent report suggests that the presence of this mutation confers resistance to trastuzumab.14 because the coexistence of her2 amplification and erbb2 mutation is extremely rare , the effect of this combination on response to her2 - targeted therapy is unknown . 
 however , it is possible that the combination of these two events may have led to the excellent response seen in the patient in this report . though this is a single report , we believe that testing for the presence of an erbb2 mutation may be indicated in patients with sdc who have her2 amplification . 
sequential her2 targeting , similar to the breast cancer paradigm , may be a feasible approach in her2 - overexpressing sdcs , especially in those with a concomitant activating erbb2 mutation . 
locati ld , perrone f , cortelazzi b , et al : clinical activity of androgen deprivation therapy in patients with metastatic / relapsed androgen receptor - positive salivary gland cancers . 
van boxtel w , boon e , weijs wlj , et al : combination of docetaxel , trastuzumab and pertuzumab or treatment with trastuzumab - emtansine for metastatic salivary duct carcinoma . 
borley a , mercer t , morgan m , et al : impact of her2 copy number in ihc2 + / fish - amplified breast cancer on outcome of adjuvant trastuzumab treatment in a large uk cancer network . 
 o intrahepatic cholangiocarcinoma : genomic heterogeneity between eastern and western patients jingyu cao , md1 ; jing hu , phd2 ; siqin liu , phd3 ; funda meric - bernstam , md4 ; reham abdel - wahab , md5 ; junjie xu , md6 ; qiang li , md7 ; maolin yan , md8 ; yujie feng , phd1 ; jianzhen lin , md9 ; songhui zhao , msc3 ; jian wang , ms3 ; lawrence n . 
borad , md10 ; kai wang , md , phd3 ; milind javle , md4 ; and haitao zhao , md9 purpose intrahepatic cholangiocarcinoma ( ihcca ) , a global health problem , is increasing in incidence and has differing etiologies worldwide . 
ngs data from asia , where ihcca is most prevalent , are limited . methods comprehensive genomic proling of formalin - xed parafn - embedded tumor tissue from 164 asian and 283 western patients with ihcca was performed using ngs . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction cholangiocarcinoma ( cca ) , a global health problem , constitutes about 10% - 20% of all primary liver cancers worldwide . 
in western countries , including the united states , metabolic syndrome , inammatory bowel disease , primary sclerosing cholangitis , hepatitis c , and alcohol abuse are the main cca risk factors , and the age - standardized incidence rate is 1.6 per 100 , 000.1 the incidence in southeast asia is extremely high , up to 71.3 per 100 , 000 in certain parts of asia , and is associated with liver uke and hepatitis b virus ( hbv ) infection.2 notably , there is an increasing incidence of intrahepatic cholangiocarcinoma ( ihcca ) worldwide , and its etiology is unclear.3 surgical resection is the only potentially curative treatment , but the majority of patients present with an advanced disease stage and have a limited therapeutic options . 
ihcca , in particular , is enriched with a relatively high number of actionable mutations , and early reports indicate several promising leads with targeted therapies for broblast growth factor receptor 2 fusion ( fgfr ) , isocitrate dehydrogenase - 1 ( idh1 ) , braf v600e mutations , and her2 / neu amplication.2 nevertheless , ngs data from asia , where cca is most prevalent , are limited . 
patients with high tmb had alterations in direct dna repair genes and caretaker genes , especially in the asian population . relevance these results may reect differences in disease etiology and are relevant for targeted therapy and immunotherapy trials for patients with intrahepatic cholangiocarcinoma . methods comprehensive genomic proling of formalin - xed parafn - embedded ( ffpe ) tumor tissue blocks from the primary tumor or metastatic lesions obtained from patients with ihcca was performed in 283 patients from a single center in the united states and in 164 patients from china . in the united states , all genomic proling analysis was performed using a clinical laboratory improvement amendments ( clia ) - validated platform ( foundation medicine , cambridge , ma )  . 
in china , genomic proling was performed by using another clia - validated targeted sequencing platform ( origimed , shanghai , china ) .5 a bridging study comparing the 2 platforms indicated high concordance ( 96.3% ; 26 / 27 ) for the same study samples ( results indicated in appendix table a1 )  . 
all ffpe tissue blocks were sectioned and stained with hematoxylin and eosin and reviewed by an expert pathologist to conrm the diagnosis and presence of least 20% of the dna derived from tumor cells . 
this research was approved by the institutional review boards at md anderson cancer center and peking union medical college . hybrid selection and sequencing a custom hybridization capture panel including over 23 , 660 individually synthesized 5 ( cid : 3 ) - biotinylated dna 120 bp oligonucleotides was used to target the exons of cancer - related genes , as well as selected introns of genes frequently rearranged in cancer . 
hybridization capture followed the protocol of hybridization capture of dna libraries using xgen lockdown probes and reagents ( version 3 ; integrated dna technologies , san diego , ca )  . postcapture libraries were mixed together , denatured , diluted , and then sequenced . 
for the purpose of estimation of sequencing error rate , a phix spike - in was added as an external control to measure the percentage of reads with 0 - 4 mismatches , following the method described by manley et al.6 bioinformatics pipeline all types of genetic alterations , including single - nucleotide variant ( snv ) , short and long indels , copy number alterations ( cnas ) , and gene rearrangement , were called using a suite of bioinformatics pipelines.5 analysis of snvs and indels began with the alignment of raw reads to the human genome reference sequence ( hg19 ) with the burrows - wheeler aligner ( v0.62 ; bwa , cambridge , ma ) , followed by polymerase chain reaction ( pcr ) duplicates removal using markduplicates algorithm from picard ( version 1.47 ; cambridge , ma )  . 
local realignment and base quality recalibration for snvs were performed using gatk ( v3.1 - 1 ; cambridge , ma ) and subsequently called by mutect ( v1.7 ; cambridge , ma )  . 
the cnas included : ( 1 ) amplication , dened as an increase in the number of gene segment copies by 8 , and ( 2 ) homozygous deletion , dened as decrease of complete loss of gene segment copies in samples with  . 
2 , 000 or zero bp were collected and used as discordant reads , that is , paired - end reads that could not be closely mapped to a genome reference , with each read of paired reads aligned to the same chromosomes or different chromosomes . 
the breakpoints were double conrmed by blat , and the resulting chimeric gene candidates were annotated . oncogenic genetic mutations statistical analysis was only based on oncogenic genetic variants and the variants of unknown signicance ; lowfrequency ( variant allele frequency , .01 ) variants were excluded . 
data are % unless otherwise specied . abbreviations : fhx , family history ; hav , hepatitis a virus ; hbv , hepatitis b virus ; hcv , hepatitis c virus ; hx , history ; sd , standard deviation . studies exist on the mutations situated on the same genome loci and structural disrupting mutations on tumor suppressor genes , such as truncations , splicing sites , and frameshifts ; ( 3 ) conrmed somatic : somatic mutations recorded on the public genomic database , such as cosmic , and detected at least once in any tumor types . tumor mutation burden and known germline alterations in dbsnp were not counted . 
we classied our patients according to the tmb scores into : ( 1 ) tmb low ( tmb - l ) if the number of mutations per megabase ( mut / mb ) was , 6 , ( 2 ) tmb inthe number of mutations per termediate ( tmb - i ) megabase was between 6 and 9 , and ( 3 ) tmb high ( tmb - h ) if the number of mutations per megabase was 10 . 
the tmb cutoff was dened per prior lung cancer trials.7 , 8 tumor mutation burden ( tmb ) was estimated for 157 us patients and 164 chinese patients with ihcca by counting its somatic mutations , including coding snvs and indels per megabase of the sequence examined . 
 cao et al msi score , we classied the samples as msi high ( msi - h ) , dened as instability in 2 microsatellite loci ; msi low , dened as instability in only 1 loci ; and microsatellite stable , dened as absence of any evidence of microsatellite loci instability . 
furthermore , the chinese patients had a signicantly higher rate of well - differentiated adenocarcinoma compared with their us counterparts ( p = .002 ; table 1 )  . western versus asian ngs comprehensive genomic proling comprehensive genomic proling identied 1 , 007 genetic aberrations ( gas ) in chinese patients compared with 971 gas in us patients ( appendix table a2 )  . 
each patient harbored at least 1 ga , with an average of 6.1 ( range , 1 to approximately 20 ) and 3.4 ( range , 1 to approximately 16 ) gas per tumor in chinese and us patients , respectively . 
as indicated in figure 1 , the most commonly reported gas in chinese patients were tumor protein 53 ( tp53 ; 41.5% ) , kirsten rat sarcoma viral oncogene homolog ( kras ; 28.7% ) , at - rich interactive domain - containing protein 1a ( arid1a ; 18.3% ) , chinese patients ( n = 164 ) us patients ( n = 283 ) dna repair genes china substitution / indel gene amplification gene homozygous deletion fusion / rearrangement truncation fig 1 . 
 ( b ) the afliated chart indicates the alterations among direct and caretaker dna repair genes . mutations are colored according to mutation types of substitution / indel , gene amplication , gene homozygous deletion , truncation , and fusion / rearrangement . 
in our cohorts , we dened dna repair genes to include the 20 most frequent previously reported dna repair gene gas , including direct dna repair genes ( atm , atr , brca1 , brca2 , fanca , fancd2 , mlh1 , msh2 , msh6 , palb2 , pold1 , pole , prkdc , rad50 , and slx4 ) and caretaker genes ( bap1 , cdk12 , kmt2c / mll3 , tp53 , and blm ) .9 remarkably , chinese patients harbored more dna repair gas compared with us patients with ihcca , with predominant gas in tp53 , brca1 / 2 , kmt2c , and rad50 . 
furthermore , there was no signicant difference in the median values of tmb - h , tmb - i , and tmb - l groups among the chinese ( 14 , 8 , and 2 mut / mb , respectively ) and us patients with ihcca ( 19 , 7 , and 3 mut / mb , respectively )  . 
moreover , we identied that the rate of msi - h in chinese and us patients was 1.8% ( n = 3 ) and 0.6% ( n = 1 ) , respectively , and all msi - h patients were associated with high tmb values ( fig 2 )  . we explored the association between dna repair gene gas and tmb , and identied a signicantly higher rate of tmb - i and tmb - h in patients who had combined direct and caretaker dna repair gas compared with patients without dna repair gas among the chinese ( p , .001 ) and us ( p = .05 ) patients with ihcca . 
the advent of ngs offers promising breakthroughs with targeted therapy and immunologic interventions . however , it is important to identify genomic heterogeneity between populations because this will have a signicant impact on precision medicine approaches for this cancer . in our study , we performed comprehensive molecular proling of 164 chinese and 283 us patients with ihcca to explore genomic heterogeneity between populations . 
mutation types are presented in the color key at the bottomss , microsatellite stable ; mut / mb , mutations per megabase . noted important differences between asian and western patients with ihcca . 
through the results , chinese patients had signicantly higher frequency of tp53 as well as kmt2c , brca1 / 2 , ddr , tert , tgfbr2 , rbm10 , nf1 , spta1 , and rb1 gas . 
 ( b ) the correlation between tmb status and dna repair genetic aberrations ( gas ) by presenting the rates of tmb levels in different existence patterns of direct dna repair gas and caretaker gas . genetic diversity could be attributed to variations in the in western underlying disease risk factors ( table 2 )  . countries , cca is associated with metabolic syndrome , inammatory bowel disease , primary sclerosing cholangitis , and hepatolithiasis , whereas liver uke and hbv are important risk factors in asian countries . 
in this study , high tmb was associated with longer progression - free survival.13 also , pembrolizumab has been approved by the food and drug administration for the dna mismatch repair decient ( mmr - d ) cancers based on a phase ii clinical trial that showed a 40% objective response rate and 78% progression - free survival rate in patients with colorectal cancer with mmr - d compared with 0% and 11% , respectively , for mmr - procient patients.14 similar results have been achieved in noncolorectal cancers that included 4 patients ( 44% ) with biliary tract cancer . 
the role of combined poly ( adp - ribose ) polymerase inhibitors and pd - 1 inhibitors in advanced solid tumor is currently under investigation and may be applicable to this subgroup . our study has important limitations . 
in these panels : ( 1 ) the content genes had some dissimilarities ; to address this issue , we ltered out differential genes and only included the 320 overlapped genes into the analysis , thereby ensuring the comparability ; ( 2 ) sequencing platforms were illumina hiseq2500 ( illumina , san diego , ca ) for foundationone and novaseq ( illumina ) for origimed450 , with effective depths of 500 and 700 , both reecting the accuracy of sequencing results17 ; ( 3 ) the tmb algorithm of origimed450 was based on the published algorithm of foundationone , and the genomic alterations were selected similarly18 ; ( 4 ) the origimed450 platform uses blood samples from individual patients as their own control for eliminating the impact of germline polymorphisms , whereas foundationone uses the somatic - germline - zygosity algorithm and databases of dbsnp and exac for the same , and nally ; and ( 5 ) we conducted a bridging study comparing the 2 platforms and showed a high degree of concordance . 
furthermore , we have examined the clinical characteristics of the chinese and us patients and demonstrated that demographic differences between these populations were minor , with most patients having an advanced disease stage . 
there was a higher proportion of hepatitis b exposure in the asian cohort , and the pathophysiologic relationship between the viral infection and somatic mutations in cancer is unknown at this time . future studies to investigate the genomic proling in different populations , taking into consideration the disease risk factors , are warranted . 
data regarding pd - 1 and pd - l1 expression were not available ; therefore , we could not identify variations in immune biomarker expression between the 2 cohorts in this study . 
borad , kai wang , milind javle , haitao zhao administrative support : jingyu cao , jing hu , maolin yan provision of study materials or patients : qiang li , jianzhen lin , lawrence n . 
kwong , haitao zhao collection and assembly of data : jingyu cao , jing hu , siqin liu , reham abdel - wahab , qiang li , maolin yan , yujie feng , jianzhen lin , lawrence n . 
kwong , jinwei hu , fernando carapeto , milind javle , haitao zhao data analysis and interpretation : siqin liu , funda meric - bernstam , reham abdel - wahab , qiang li , songhui zhao , jian wang , lawrence n . 
 ihcca : genomic heterogeneity between eastern and western patients funda meric - bernstam employment : md anderson cancer center honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group , mersana , seattle genetics , silverback therapeutics , immunomedics , ibm watson health , f . 
hoffman - laroche , ibm watson health , pact pharma , effector therapeutics speakers bureau : chugai biopharmaceuticals research funding : novartis ( inst ) , astrazeneca ( inst ) , taiho pharmaceutical ( inst ) , genentech ( inst ) , calithera biosciences , debiopharm group ( inst ) , bayer ( inst ) , aileron therapeutics ( inst ) , puma biotechnology ( inst ) , cytomx therapeutics ( inst ) , jounce therapeutics ( inst ) , zymeworks ( inst ) , curis ( inst ) , pzer ( inst ) , effector therapeutics ( inst ) , abbvie ( inst ) , boehringer ingelheim ( i ) , guardant health ( inst ) , daiichi sankyo ( inst ) , glaxosmithkline ( inst ) , seattle genetics ( inst ) travel , accommodations , expenses : taiho pharmaceutical , seattle genetics , beth israel deaconess medical center songhui zhao employment : origimed lawrence n . 
borad stock and other ownership interests : gilead sciences , aveo , intercept pharmaceuticals , spectrum pharmaceuticals consulting or advisory role : g1 therapeutics , fujilm ( inst ) , agios ( inst ) , insys therapeutics ( inst ) , novartis ( inst ) , arqule ( inst ) , celgene ( inst ) , inspyr therapeutics , halozyme ( inst ) , pieris pharmaceuticals ( inst ) , taiho pharmaceutical ( inst ) , immunovative therapies , exelixis , lynx group , genentech , western oncolytics , klus pharma , denovo , merck , imvax research funding : boston biomedical ( inst ) , mirna therapeutics ( inst ) , senhwa biosciences ( inst ) , medimmune ( inst ) , biolinerx ( inst ) , agios ( inst ) , halozyme ( inst ) , celgene ( inst ) , threshold pharmaceuticals ( inst ) , toray industries ( inst ) , dicerna ( inst ) , sillajen ( inst ) , eisai ( inst ) , taiho pharmaceutical ( inst ) , emd serono ( inst ) , isis pharmaceuticals ( inst ) , incyte ( inst ) , sun biopharma ( inst ) , ariad ( inst ) , imclone systems ( inst ) , qed therapeutics ( inst ) , incyte ( inst ) , puma biotechnology ( inst ) , adaptimmune ( inst ) , merck serono ( inst ) , redhill biopharma ( inst ) , basilea ( inst ) travel , accommodations , expenses : arqule , celgene , astrazeneca kai wang employment : origimed leadership : origimed milind javle consulting or advisory role : qed , oncosil , incyte , mundi other relationship : rafael pharmaceuticals , incyte , pieris pharmaceuticals , merck , merck serono , novartis , seattle genetics , beigene , qed therapeutics , bayer no other potential conicts of interest were reported . references chun ys , javle m : systemic and adjuvant therapies for intrahepatic cholangiocarcinoma . 
curr treat options oncol 17 : 58 , 2016 saha sk , zhu ax , fuchs cs , et al : forty - year trends in cholangiocarcinoma incidence in the u.s. : intrahepatic disease on the rise . 
nat genet 44 : 690 - 693 , 2012 cao j , chen l , li h , et al : an accurate and comprehensive clinical sequencing assay for cancer targeted and immunotherapies . 
n engl j med 378 : 2093 - 2104 , 2018 rizvi na , mazi `eres j , planchard d , et al : activity and safety of nivolumab , an anti - pd - 1 immune checkpoint inhibitor , for patients with advanced , refractory squamous non - small - cell lung cancer ( checkmate 063 ) : a phase 2 , single - arm trial . 
lancet oncol 16 : 257 - 265 , 2015 chae yk , anker jf , bais p , et al : mutations in dna repair genes are associated with increased neo - antigen load and activated t cell inltration in lung adenocarcinoma . 
oncotarget 9 : 7949 - 7960 , 2017 jusakul a , cutcutache i , yong ch , et al : whole - genome and epigenomic landscapes of etiologically distinct subtypes of cholangiocarcinoma . 
chan - on w , nairism agi ml , ong ck , et al : exome sequencing identies distinct mutational patterns in liver uke - related and non - infection - related bile duct cancers . 
clarke b , tinker av , lee ch , et al : intraepithelial t cells and prognosis in ovarian carcinoma : novel associations with stage , tumor type , and brca1 loss . 
ali sm , yao m , yao j , et al : comprehensive genomic proling of different subtypes of nasopharyngeal carcinoma reveals similarities and differences to guide pathol 22 : 393 - 402 , 2009 gynecol oncol 141 : 293 - 302 , 2016 targeted therapy . 
the respected blocks were sectioned at 5 mm ; the tumor content size and were conrmed by a trained pathologist , and a minimum of 5 unstained slides were submitted for conrmation using the origimed platforinstitutional review board approval was obtained for this study . 
 o tissue / site - agnostic study of ribociclib for tumors with cyclin dcdk4 / 6 pathway genomic alterations : a phase ii , open - label , single - arm basket study julio peguero , md1 ; davendra p . 
grilley - olson , md6 ; vivek subbiah , md7 ; lincoln nadauld , md , phd8 ; das purkayastha , phd9 ; erica stealey , ms9 ; alejandro d . 
kang , phd9 ; and joseph paul eder , md10 purpose as part of the novartis signature program , this study evaluated the efcacy of ribociclib ( selective cyclin - dependent kinase 4 / 6 [ cdk4 / 6 ] inhibitor ) in patients with cyclin dcdk4 / 6 pathwayaberrant tumors . methods this was a phase ii , single - arm , signal - seeking study in patients with advanced malignancies that had progressed on or after standard treatment . 
clinical benet ( dened as the proportion of patients with response or stable disease at 16 weeks ) was the primary end point . results from 61 centers in the united states , 106 patients ( median age , 62.5 years ) were enrolled across multiple malignancies . 
in patients with solid tumors , the clinical benet rate was 18.1% ( n = 19 of 105 ) and the overall response rate was 2.9% ( n = 3 of 105 ) ; three partial responses occurred in patients with adenocarcinoma ( unknown primary ) , soft tissue sarcoma , and urothelial carcinoma . 
2019 by american society of clinical oncology introduction cyclin - dependent kinases 4 and 6 ( cdk4 / 6 ) , in conjunction with their protein regulator cyclin d1 ( encoded by ccnd1 ) , phosphorylate the retinoblastoma ( rb ) protein and regulate g1 cell - cycle progression . 
the p16 ( cdkn2a ) and p15 ( cdkn2b ) tumor suppressors and negaproteins are critical tive regulators of this pathway , mediating cellular senescence.1 , 2 arf ( p19 ) plays an important role in the p53 / mouse double minute 2 homolog ( mdm2 ) - dependent checkpoint ; arf expression leads to activation and stabilization of p53 by promoting mdm2 degradation.3 , 4 pathway alteration can result including from multiple mechanisms , rb mutation or loss , increased signaling through cdk4 and cdk6 amplication , cyclin d1 overexpression , and loss of inhibitors.1 cdk pathway alterations contribute to tumor proliferation and genomic instability , and have been linked to poorer clinical outcomes in multiple cancers . 
cdk4 / 6 and cdkn2a / b abnormalities were reported in 22.8% of patients with various cancers who underwent molecular proling by targeted next - generation sequencing.2 ribociclib is a selective cdk4 / 6 inhibitor that induces dose - dependent rb dephosphorylation , reducing cell proliferation via g1 arrest . 
ribociclib is approved in combination with an aromatase inhibitor as initial endocrine - based therapy for postmenopausal women with hormone receptorpositive / human epidermal growth factor receptor 2 ( her2 ) - negative advanced or metastatic breast cancer . 
 peguero et al context key objective to determine if tumor cyclin dcyclin - dependent kinase 4 / 6 ( cdk4 / 6 ) pathway alterations are an effective signal of efcacy for treatment with ribociclib , a selective cdk4 / 6 inhibitor . knowledge generated in this phase ii , signal - seeking study , 105 patients with heavily pretreated cyclin dcdk4 / 6 pathwayaberrant solid tumors received ribociclib treatment . 
although the primary end point of the study was not met , the clinical benet rate was 18.1% , with partial responses observed in three patients with single gene amplications in the cyclin dcdk4 / 6 pathway . relevance a deeper understanding of the molecular context of tumors is required to accurately match patients to ribociclib , either as a monotherapy or in combination with agents that target interconnected signaling pathways . we present ndings from a signal - seeking study that assessed ribociclib as part of the novartis signature program ( clinicaltrials.gov identier : nct02187783 ) , comprising a series of signal - nding basket protocols in which different single - agent targeted therapies were investigated in a tissueor site - agnostic indication , mutation - specic manner.6 , 7 in this study , patients preidentied as having cdk4 / 6 pathwayaberrant tumors were matched to ribociclib monotherapy . methods study design this was a phase ii , open - label , singletreatment arm , basket study in patients with solid tumors or hematologic malignancies with cdk4 / 6 pathway alterations and whose disease had progressed on or after standard treatment . patients received ribociclib 600 mg , once daily , on a 3week - on / 1 - week - off schedule until disease progression ( by investigator assessment ) , unacceptable toxicity , death , or discontinuation from study treatment ( eg , consent withdrawal , starting a new antineoplastic therapy , investigator decision )  . 
ribociclib dose was reduced to 400 mg , and then to 200 mg if an additional dose reduction was required ; ribociclib dose could not be reescalated . the primary end point was the clinical benet rate assoinvestigator asciated with ribociclib treatment by local sessment , dened as the proportion of patients achieving a complete response ( cr ) , partial response ( pr ) , or stable disease ( sd ) at 16 weeks or later by response evaluation criteria in solid tumors 1.1. 
patients who discontinued treatment before week 16 for reasons other than progressive disease ( pd ) were considered nonevaluable ; patients who had pd before week 16 were considered to have no clinical benet . 
overall response rate ( orr ; ie , cr or pr ) by local investigator assessment was the key secondary end point . patient eligibility criteria patients at least 18 years old with solid tumors or hematologic malignancies with cdk4 / 6 mutations or amplications , cyclin - d1 / d3 gene amplications , or p16 gene mutations or loss were enrolled . 
patients had at least one prior treatment of their recurrent , metastatic , and / or locally advanced disease and had no remaining standard therapy options expected to result in durable response . 
because of overlapping disease - oriented studies , the following tumor types were excluded : breast cancer ( except triple negative ) , liposarcoma , teratoma , castrate - resistant prostate cancer , melanoma , and mantle cell lymphoma . 
all patients gave written informed consent before treatment , according to federal and local stitutional guidelines . genomic proling gene aberrations were assessed in a local clinical laboratory improvement amendmentscertied laboratory before patient consent . 
once a patient was identied , vestigators contacted novartis study enrollment consideration.8 post hoc broad molecular proling using a next - generation dna sequencing panel of more than 280 cancerassociated genes9 was performed centrally on pretreatment tumor biopsy specimens from all patients . 
 mutation - specic , tissue / site - agnostic study of ribociclib statistical analysis tumor cohorts were formed when four or more patients with a particular tumor type were enrolled . 
the number of patients enrolled per tumor type was based on a patientsparing , adaptive design , allowing early closure of nonresponding groups and / or groups with early success . clinical benet was evaluated using a bayesian adaptive statistical design that allowed dynamic borrowing of information across cohorts on the basis of their degree of similarity.8 the statistical design used a hierarchical model that allowed dynamic borrowing of information between groups . 
this design allowed analyses with small sample sizes for each cohort . at least 10 patients were required to evaluate early futility , and at least 15 to evaluate early success and make a go or no - go decision for each tumor type cohort . 
if there was an 80% or greater probability that the response rate exceeded the historical rate , the group was considered a success . orr , pr , or cr on the basis of local investigator assessment were summarized , and 95% exact cis using the clopperpearson method were also reported.8 correlation between a specic genomic ( somatic ) dna prole , based laboratory analysis , and clinical benet was on central explored . 
in addition , ribociclib safety and tolerability were reported . results patients in total , 106 patients from 61 centers in the united states were enrolled across multiple malignancies between august 25 , 2014 , and may 4 , 2015 . 
of the 105 patients with solid tumors , 19 ( 18.1% ) achieved clinical benet ( primary end point ) ; the orr ( key secondary end point ) was 2.9% ( three prs ; table 2 )  . 
the rst patient , a 59 - year - old man with poorly differentiated adenocarcinoma of unknown primary with cdk6 amplication , achieved a pr ( 100% reduction in target lesions ) after the fourth cycle of ribociclib and was continuing therapy at last data cutoff with a duration of response of + 796 days . 
the second patient , a 25year - old man with poorly differentiated , round blue cell soft tissue sarcoma not otherwise specied with cdk4 amplication , had a pr ( 100% reduction ) after two cycles of ribociclib , with a duration of response of 330 days . 
the third patient , a 53 - year - old man with urothelial carcinoma of the bladder with ccnd1 amplication , also experienced a pr ( 37.5% reduction ) after two cycles of ribociclib , with a duration of response of 254 days . 
his bladder cancer had not responded to either rst - line cisplatin plus gemcitabine combination or apatorsen ( ogx - 427 ) an experimental antisense inhibitor targeting heat shock protein 27 . 
one patient with papillary serous ovarian carcinoma with cdk6 mutation ( not conrmed by central review ) experienced a tumor burden reduction of at least 30% , without subsequent conrmation , and had sd for 239 days . 
 ( % ) unless otherwise indicated . abbreviations : ecog , eastern cooperative oncology group ; ps , performance status . * gastroesophageal junction ( n = 4 ) , head and neck nonsquamous cell carcinoma ( n = 4 ) , unknown primary site ( n = 4 ) , uterus ( n = 4 ) , esophagus ( n = 3 ) , ovarian ( n = 3 ) , skin nonmelanoma ( n = 3 ) , cholangiocarcinoma ( n = 2 ) , colorectal ( n = 2 ) , renal cell carcinoma ( n = 2 ) , liver ( n = 2 ) , neuroendocrine ( n = 2 )  . 
other histologies ( n = 10 ) only included one each . based on local molecular proling . a patient can be counted in multiple categories ; therefore , the overall count can be  . 
100. 4 2019 by american society of clinical oncology there was no association between any specic genomic ( somatic ) dna prole and clinical benet per central analysis ( fig 3 )  . 
however , 18 of 19 patients ( 94.7% ) with clinical benet had tumors with a single hit in the cyclin d - cdk4 / 6 pathway and one patient with clinical benet had multiple mutational events ; patients with a pr had tumors with cdk4 / 6 or ccnd1 amplication . 
in total , 86 patients had a single cyclin dcdk4 / 6 pathway mutation and 10 patients had multiple pathway mutations ; central mutation analysis was not available in nine patients . 
the most common aes suspected to be related to the study drug included fatigue ( 31.1% ) , neutropenia ( 30.2% ; decreased neutrophils , 15.1% ) , and nausea ( 29.2% ; table 3 )  . 
of these , fatigue and nausea were typically mild . the most common grade 3 / 4 ae suspected to be related to the study drug was neutropenia ( 18.9% ; n = 20 ; decreased neutrophils , 7.5% , n = 8 ) ; only one incident of febrile neutropenia ( grade 3 ) occurred , but it was effectively managed with supportive care and antibiotics . 
 mutation - specic , tissue / site - agnostic study of ribociclib screened ( n = 176 ) enrolled ( n = 106 ) excluded * unacceptable laboratory value unacceptable test result unacceptable medical history intercurrent medical event did not meet diagnostic / severity criteria use of excluded medications patient withdrew consent other ( n = 70 ) ( n = 22 ) ( n = 15 ) ( n = 6 ) ( n = 6 ) ( n = 7 ) ( n = 8 ) ( n = 2 ) ( n = 10 ) still receiving study drug ( n = 1 ) discontinued disease progression patient / guardian decision adverse event death protocol deviation physician decision ( n = 105 ) ( n = 80 ) ( n = 9 ) ( n = 8 ) ( n = 3 ) ( n = 3 ) ( n = 2 ) consented for survival follow - up ( n = 89 ) death lost to follow - up ( n = 58 ) ( n = 31 ) fig 1 . 
as such , more patients have been identied with potentially actionable pathway activation , raising the hope of personalized medicine through targeted drug treatment.10 , 11 the design of basket trials enables molecularly driven enrollment and treatment assignment , with simultaneous testing of a single targeted agent in tumors of different histologies that harbor genetic alterations in the targeted pathway.12 - 14 the signature program was built on this approach and included eight agentspecic , signal - seeking phase ii basket trials of various targeted therapies in a histology - agnostic , mutation - specic manner , matching patients with potentially actionable mutations to the corresponding agent . 
the aim of the signature program was to support or refute the hypothesis that driver mutations determine therapeutic response to treatment in a histology - agnostic manner . this tissueor site - agnostic approach was recently evaluated in patients with solid tumors and led to the us food and drug administration granting accelerated approval to pembrolizumab for the rst tissueor site - agnostic indication.15 indeed , the prospects for the tissueor siteagnostic approach in oncology have never looked brighter , as the successful stories of larotrectinib and entrectinib continue to unfold.16 moreover , the food and drug administration has also recently granted marketing approval to several diagnostics based on next - generation sequencing : the praxis extended ras panel ( illumina , san diego , ca ) , the oncomine dx target test ( thermo fisher scientic , waltham , ma ) , and the foundationone cdx ( foundation medicine , cambridge , ma ) .17 - 19 these tests , and others under clinical investigation , could identify which patients with pathway - aberrant tumors may benet from targeted treatment options . 
thus , the aim for the present ribociclib signal - seeking study was to match patients with cdk4 / 6 pathway - aberrant tumors with the selective cdk4 / 6 inhibitor ribociclib . the primary end point of the study was the rate of clinical benet associated with ribociclib monotherapy , based on local investigator assessment . 
prs were observed in three patients , and 16 patients had sd for 16 weeks or longer . two patients with pr had the maximum percentage reduction from baseline in target lesions ( 100% )  . 
unlike the mutations affecting rb activation , cdkn2a mutation or loss concomitantly decreases the critical function of the p53 - stabilizing effect of the arf protein on the ubiquitin ligase mdm2 , mimicking many mutations in tp53 . 
other selective cdk4 / 6 inhibitors , palbociclib and abemaciclib , have shown low - rate monotherapy activity outside of breast cancer.20 - 23 similarly , a few extraordinary long - term responses have been observed with these agents in tumors with ccnd1cdk4 / 6 amplications . 
these observations may be partly due to the molecular context of the tumor . cyclin dcdk4 / 6 pathway activity is regulated by a number of mitogenic signals , including epidermal growth factors , signaling through the her2 and estrogen receptors , and the phosphoinositide 3 - kinase ( pi3k ) akt pathway.24 studies have suggested that response to targeted therapy may be affected by the presence of tumor mutations in related signaling pathways . 
 mutation - specic , tissue / site - agnostic study of ribociclib chromosome head and neck nonsquamous - cell carinoma head and neck squamous - cell carinoma adrenals bladder breast , triple negative cervix cholangiocarcinoma chordoma colorectal esophagus gallbladder ducts gastroesophageal junction gist kidneys liver lung , nonsmall - cell nonadenocarcinoma lung , nonsmall - cell adenocarcinoma lung , nonsmall - cell squamous lymphoma mesothelioma neuroendocrine ovarian pancreas penile prostate salivary gland sarcoma skin , nonmelanoma thyroid unknown primary uterus shrinkage mutation amplication loss rearrangement short variant fig 3 . 
the most common grade 3 / 4 aes suspected to be related to ribociclib was neutropenia ( 18.9% ) and decreased neutrophils ( 7.5% ) ; only one incident of febrile neutropenia ( grade 3 ) was reported , which was effectively managed with supportive care and antibiotics . 
no deaths due to aes were suspected to be related to study drug per the investigator . one study limitation was the restriction of cohorts by tumor type rather than molecular subtype . 
a second limitation was the exclusion of the most obvious indications for single - agent cdk4 / 6 inhibition : hormone - sensitive breast cancer , liposarcoma , teratoma , castrate - resistant prostate cancer , melanoma , and mantle cell lymphoma . 
this exclusion was due to overlapping disease - oriented studies in these indications , which already were in place by the time this tissueor site - agnostic study started . in conclusion , although no tumor - type cohort graduation was observed , preliminary activity was seen in tumors with single - hit ccnd1cdk4 / 6 amplications . 
these ndings investigation and suggest that in the warrant additional absence of ccnd1cdk4 / 6 amplications or in patients with multiple mutational events , cdk4 / 6 inhibition may require combination with other agents that provide additive or synergistic effects . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . julio peguero employment : oncology consultants leadership : oncology consultants davendra p . 
sohal honoraria : foundation medicine consulting or advisory role : perthera , ability pharma research funding : novartis ( inst ) , celgene ( inst ) , oncomed ( inst ) , bayer ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) , loxo ( inst ) bert h . 
oneil employment : eli lilly consulting or advisory role : bristol - myers squibb , merck karen kelly honoraria : merck consulting or advisory role : astrazeneca , roche , eli lilly , regeneron , abbvie , janssen , emd serono , merck , pzer , astrazeneca research funding : emd serono ( inst ) , genentech ( inst ) , abbvie ( inst ) , five prime therapeutics ( inst ) , regeneron ( inst ) patents , royalties , other intellectual property : author royalties for uptodate travel , accommodations , expenses : astrazeneca , roche , merck , regeneron , eli lilly , abbvie , emd serono , merck juneko e . 
grilley - olson consulting or advisory role : bayer , chimerix research funding : nanocarrier ( inst ) , genentech ( inst ) , seattle genetics ( inst ) , medimmune ( inst ) , pzer ( inst ) vivek subbiah consulting or advisory role : medimmune research funding : novartis ( inst ) , glaxosmithkline ( inst ) , nanocarrier ( inst ) , northwest biotherapeutics ( inst ) , roche ( inst ) , berg pharma ( inst ) , bayer ( inst ) , incyte ( inst ) , fujilm ( inst ) , pharmamar ( inst ) , d3 oncology solutions ( inst ) , pzer ( inst ) , amgen ( inst ) , abbvie ( inst ) , multivir ( inst ) , blueprint medicines ( inst ) , loxo ( inst ) , vegenics ( inst ) , takeda ( inst ) , alfasigma ( inst ) , agensys ( inst ) , idera ( inst ) , boston biomedical ( inst ) , inhibrx ( inst ) , exelixis ( inst ) travel , accommodations , expenses : pharmamar , bayer lincoln nadauld stock and other ownership interests : toma biosciences , citizen corporation consulting or advisory role : roche speakers bureau : genentech patents , royalties , other intellectual property : navican travel , accommodations , expenses : roche , chugai pharma das purkayastha employment : novartis pharmaceuticals erica stealey employment : novartis stock and other ownership interests : novartis alejandro d . 
clin cancer res 21 : 2905 - 2910 , 2015 kato s , schwaederle m , daniels ga , et al : cyclin - dependent kinase pathway aberrations in diverse malignancies : clinical and molecular characteristics . 
cell cycle 14 : 1252 - 1259 , 2015 zhang y , xiong y , yarbrough wg : arf promotes mdm2 degradation and stabilizes p53 : arf - ink4a locus deletion impairs both the rb and p53 tumor suppression pathways . 
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n engl j med 375 : 1738 - 1748 , 2016 kang bp , slosberg e , snodgrass s , et al : the signature program : bringing the protocol to the patient . 
n engl j med 377 : 62 - 70 , 2017 slosberg ed , kang bp , peguero j , et al : signature program : a platform of basket trials . 
oncotarget 9 : 21383 - 21395 , 2018 frampton gm , fichtenholtz a , otto ga , et al : development and validation of a clinical cancer genomic proling test based on massively parallel dna sequencing . 
lopez - chavez a , thomas a , rajan a , et al : molecular proling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
patnaik a , rosen ls , tolaney sm , et al : efcacy and safety of abemaciclib , an inhibitor of cdk4 and cdk6 , for patients with breast cancer , non - small cell lung cancer , and other solid tumors . 
goldman jw , shi p , reck m , et al : treatment rationale and study design for the juniper study : a randomized phase iii study of abemaciclib with best supportive care versus erlotinib with best supportive care in patients with stage iv non - small - cell lung cancer with a detectable kras mutation whose disease has progressed after platinum - based chemotherapy . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
edelman mj , redman mw , albain ks , et al : a phase ii study of palbociclib ( p ) for previously treated cell cycle gene alteration positive patients ( pts ) with stage iv squamous cell lung cancer ( scc ) : lung - map sub - study swog s1400c . 
ther adv med oncol 10 : 1 - 15 , 2018 janku f , hong ds , fu s , et al : assessing pik3ca and pten in early - phase trials with pi3k / akt / mtor inhibitors . 
kim s , tiedt r , loo a , et al : the potent and selective cyclin - dependent kinases 4 and 6 inhibitor ribociclib ( lee011 ) is a versatile combination partner in preclinical cancer models . 
carbone , md , phd4 immunotherapy , the advent of including immune checkpoint inhibitors ( icis ) , has contributed to improved survival in patients with lung cancer.1 three antiprogrammed death - 1 ( pd - 1 ) / programmed death ligand 1 ( pd - l1 ) therapies , nivolumab , pembrolizumab , and atezolizumab , are approved by the us food and drug administration ( fda ) for the treatment of patients with advanced nonsmall - cell lung cancer ( nsclc ) in the rst - line setting.2 - 4 despite the improvements in survival seen with icis , there remains a subset of patients who do not benet from ici monotherapy or combination treatments.5 as a result , many research efforts have been initiated to identify biomarkers predictive of response to treatment with icis . 
predictive biomarkers that have entered clinical practice include pd - l1 expression on tumor and immune cells , and tumor mutational burden.2 - 4 , 6 , 7 however , the accuracy of predictions of patient response based on current biomarkers leaves ample room for improvement . 
successful attempts will likely rely on integrated models combining multiple features . the scientic to tackle such complex challenges , community has become increasingly interested in the possibilities offered by data sharing and crowdsourcing as a framework for mobilizing groups of people with shared interests around the world and bringing forward augmented solutions to the existing problems while encouraging collaboration . 
in this context , data sharing can be executed according to two paradigms.8 in the data - to - modeler paradigm , both training and validation data sets are provided to participants . 
the model - to - data paradigm , where participants submit containerized models to organizers , allows validation data sets to remain hidden from participants , which both protects condential data and helps ensure unbiased assessment of predictions . 
these approaches are instrumental broadening our understanding of tumor biology and the tumor microenvironment , which will ultimately drive precision medicine with immunotherapy . to enable such collaboration among scientists and physicians , dialogue on reverse engineering and assessment methods ( dream ) challenges engage experts from around the world and offer novel solutions to biological problems.9 since the rst dream challenges were initiated in 2006 , more than 60 have completed , with analysis results generated through virtual collaborative interactions.10 in oncology , crowdsourcing approaches have been used in multiple tumor types since 2012 for augmenting the work of teams generating data , developing protocols for randomized controlled trials , developing prognostic models , and assessing healthcare behaviors on a large scale.11 more specically , three key dream challenges in oncology have demonstrated the value of crowdsourcing for the development of prognosis models or the renement of diagnostic methods . 
 vincent et al following on from these successful dream challenges , experts in lung cancer have shown interest in accessing primary clinical trial data to explore alternative biomarkers to pd - l1 expression and tumor mutational burden . 
the antipd - 1 response prediction challenge will be the rst dream challenge focused on the prediction of response to immuno - oncology therapies using data from a large phase iii clinical trial , with the goal of addressing the need for additional predictive biomarkers to use with icis in patients with nsclc . 
moreover , this initiative will also enhance the understanding of tumor biology and provide further insights into the potential mechanisms underpinning treatment resistance to icis . challenge objectives the antipd - 1 response prediction challenge will focus on developing models that are predictive of benet from ici treatment , specically nivolumab monotherapy , using patient samples obtained during the conduct of a clinical trial . clinical trial data related to nivolumab , including data related to pd - l1 expression , tumor mutational burden , and tumor transcriptomics , will be used to assess the performance of predictive models submitted in a crowdsourced challenge setting . 
the testing data set will use deidentied data from checkmate 026 ( clinicaltrials.gov identier : nct02041533 ) , a phase iii trial that compared nivolumab with platinum - based chemotherapy in patients with metastatic or recurrent nsclc and pd - l1 tumor expression 5%.15 critically , the data set from checkmate 026 is large , randomized , mature , and well annotated , allowing it to support robust testing of predictive models . 
this challenge also lays the foundation for potential future challenges as the immunooncology landscape is rapidly evolving . the antipd - 1 response prediction challenge aims to assess the accuracy of models for predicting clinical outcomes after nivolumab monotherapy , including efcacy end points such as overall survival , progression - free survival , and best overall response , applying clinical and genomic data from checkmate 026 . 
the challenge will comprise three subchallenges , and their objectives are summarized in figure 1 . challenge design framework has been developed to receive and evaluate dockerized models , which are in silico packages comitself plus necessary software compoprising the model nents to run the model as developed by the participant team . the challenge is open to anyone who will be able to construct models for submission , subject to specications in the challenge rules , including experts and innovators in genomics , computational biology , and translational biomarker development . 
participants can sign up on the synapse website.16 to facilitate data ingestion , participants will have access to a small synthetic data set with the same formatting as the validation data set . 
the full synthetic data set can be downloaded on the synapse website.17 in the rst phase , participants will construct models using any data available to thethe iatlas platform , 18 a database supporting the study of interactions between cancer and the immune microenvironment , hosts harmonized genomics data and associated clinical annotations from published immuno - oncology studies . 
participants can use these as training data sets or to augment other training data already available to them.19 participants could also use professor shirley lius labs tide resources , 20 a computational framework that integrated and modeled data from 189 human cancer studies , comprising 33 , 197 samples.21 more resources to consider are listed on the antipd - 1 response prediction challenge website.16 participants dockerized models will be applied to the checkmate 026 data and evaluated during the competitive phase . 
performance metrics , such as area under the receiver operating characteristic or precision - recall curves and harrells c - index , will be used to assess the predictive performance of participants models in each arm of the checkmate 026 trial . top - performing teams will be invited to participate in the collaborative model - development phase , during which data will be analyzed and interpreted to deepen the understanding of the submitted models . 
eventually , opportunities for additional subchallenges and potential projects will be dened based on the learnings from the current challenge , and teams submitting the best - performing models will have the opportunity to co - author the planned publication in accordance with medical publication standards and best practices . the challenge will rely on a partnership between sage the organization supporting the dream bionetworks , challenge initiatives , and bristol myers squibb and will comprise three phases : competitive , collaborative , and nal . 
the anticipated outcome and impact the identied models are expected to identify potential biomarkers of response to nivolumab monotherapy and may then be applied to predict which patients are more likely to derive clinical benet from icis . 
nsclc , nonsmallcell lung cancer ; os , overall survival ; pd , progressive disease ; pd - 1 , programmed death - 1 ; pfs , progression - free survival . dream challenge challenge question 1 predict response to nivolumab , in terms of pfs , via an immune checkpointspecific model using clinical , demographic , and gene expression data challenge question 2 predict response to nivolumab , in terms of os , via an immune checkpointspecific model using clinical , demographic , and gene expression data challenge question 3 predict which patients will have a best overall response of pd checkmate 026 mature data set from a large randomized phase iii clinical trial in patients with nsclc nivolumab chemotherapy dream challenge impact ( cid : 129 ) provide biomarkers with predictive value for patients via a transparent and collaborative approach ( cid : 129 ) lay the foundation for understanding the utility of biomarkers in the setting of combination therapy patients . 
it is anticipated that some of the models may also have prognostic value for patients with nsclc . phenotype , thereby increasing their responsiveness to ici therapies . the challenge results should also provide a deeper understanding of biological mechanisms resulting in tumor resistance to treatment and assist in understanding why patients with advanced nsclc receiving nivolumab had similar efcacy outcomes to patients receiving chemotherapy in checkmate 026 . 
an improved understanding of the biological mechanisms behind resistance could pave the way to therapeutic interventions that immunologically activate tumors that do not display an immune - inltrated successful completion of this dream challenge will provide a model for future collaborations among industry , academia , and citizen scientists to discover determinants of response or resistance to immunotherapy , facilitating rapid development of clinically actionable biomarkers . 
szustakowski employment : bristol myers squibb stock and other ownership interests : bristol myers squibb research funding : bristol myers squibb patents , royalties , other intellectual property : i am an employee of bristol myers squibb , and an inventor on one or more pending patent applications , including applications for tmb as a predictive biomarker of immunotherapy travel , accommodations , expenses : bristol myers squibb parul doshi employment : bristol myers squibb stock and other ownership interests : bristol myers squibb travel , accommodations , expenses : bristol myers squibb justin guinney consulting or advisory role : astrazeneca research funding : celgene , genentech / roche , bristol myers squibb david p . 
carbone manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors references american cancer society : facts & figures 2020 reports largest one - year drop in cancer mortality . 
sambi m , bagheri l , szewczuk mr : current challenges in cancer immunotherapy : multimodal approaches to improve efcacy and patient response rates . j oncol 2019 : 4508794 , 2019 bristol myers squibb : yervoy ( ipilimumab ) [ package insert ]  . 
nat biotechnol 36 : 391 - 392 , 2018 saez - rodriguez j , costello jc , friend sh , et al : crowdsourcing biomedical research : leveraging communities as innovation engines . 
guinney j , wang t , laajala td , et al : prediction of overall survival for patients with metastatic castration - resistant prostate cancer : development of a prognostic model through a crowdsourced challenge with open clinical trial data . 
carbone dp , reck m , paz - ares l , et al : first - line nivolumab in stage iv or recurrent non - small - cell lung cancer . 
immunity 48 : 812 - 830.e814 , 2018 jiang p , gu s , pan d , et al : signatures of t cell dysfunction and exclusion predict cancer immunotherapy response . 
 whole - genome and whole - exome sequencing in pediatric oncology : an assessment of parent and young adult patient knowledge , attitudes , and expectations purpose the complexity of results generated from whole - genome sequencing ( wgs ) and whole - exome sequencing ( wes ) adds challenges to obtaining informed consent in pediatric oncology . 
little is known about knowledge of wgs and wes in this population , and no validated tools exist in pediatric oncology . methods we developed and psychometrically evaluated a novel wgs and wes knowledge questionnaire , the precision in pediatric sequencing knowledge questionnaire ( pipseqkq ) , to identify levels of understanding among parents and young adult cancer survivors ( 18 years old ) , off therapy for at least 1 year from a single - institution pediatric oncology outpatient clinic . 
of the total cohort , 77 ( 69% ) were female , 63 ( 57% ) self - identified as white , and 74 ( 67% ) self - identified as non - hispanic . 
 overall , participants felt the benefits of wgs and wes outweighed the potential risks . conclusion parents and young adult cancer survivors have some genetics knowledge , but they lack knowledge about wgs and wes . 
the pipseqkq is a reliable tool that can identify deficits in knowledge , identify perceptions of risks and benefits of wgs and wes , and help clinicians tailor their consent discussions to best fit families . 
2018 by american society of clinical oncology introduction advances in next - generation sequencing , particularly whole - genome sequencing ( wgs ) and whole - exome sequencing ( wes ) have led to a deeper understanding of the pathogenesis of cancer and offer promising avenues for clinical applications.1 , 2 in pediatric oncology , wgs and wes is being used to identify targetable mutations , clarify diagnosis , provide risk stratification , and identify pharmacogenomic modifiers.3 - 6 although these genome - scale sequencing methods yield a wide spectrum of potential results , only a few are medically actionable ; a large number are classified as variants of unknown significance ( vus )  . 
furthermore , wgs and wes of matched tumornormal tissue can identify pathogenic germline mutations not related to the indication for which testing was ordered , commonly referred to as secondary findings , and jennifer a . 
the american college of medical genetics has defined a list of secondary findings that include noncancerous germline disease - causing mutations and cancer susceptibility mutations recommended for return by clinical laboratories.7 , 8 such findings may be of clinical significance not only to the patient but also to family members not directly involved in testing.9 - 13 an understanding of these complexities is necessary for parents and patients to make informed decisions about consent to genomic sequencing.14 , 15 for most pediatric cancers , standard treatment protocols are highly effective , and wgs and wes results infrequently alter the initial treatment plan.16 however , among parents of pediatric patients with cancer , the hope that genomic sequencing will lead to a cure often exceeds the expected results of testing.17 , 18 thus , parents may be more inclined to participate in wgs and wes without fully understanding the range of results that may be returned , including vus and secondary findings.17 , 18 even within the general public , including those who are well educated , there is a relatively low understanding of genetic concepts.19 research to examine knowledge held by parents and young adult patients about the utility and limitations of genome sequencing is scarce , although there is evidence to suggest that participants with lower educational attainment or those from racial / ethnic minority groups may possess less knowledge.14 within pediatric oncology , there are almost no data related to parent and young adult patient knowledge about genetics and wgs and wes , and there are no validated tools to assess these concepts in pediatric cancer . as part of our clinical sequencing program at columbia university medical center ( cumc ) , we developed the precision in pediatric sequencing knowledge questionnaire ( pipseqkq ) to assess knowledge , attitudes , and expectations of parents and young adult patients about wgs and wes . 
the objectives of the study were to describe the development and psychometric properties of the pipseqkq and to identify preliminary levels of understanding within this population . methods participants participants were recruited from the pediatric oncology outpatient clinic at cumc between august 2015 and june 2016 . 
wgs and wes in pediatric oncology at cumc commenced in january 2014 , and 1 year off therapy was chosen as a cutpoint to minimize the likelihood that participants had undergone or had been exposed to the concepts of wgs and wes in the clinic setting . 
a total of 35 items and three knowledge domains were generated : general genetic concepts ( n = 7 items ) , genetic concepts associated with general health and cancer ( n = 12 items ) , and wgs and wes concepts ( n = 16 items )  . 
a multidisciplinary team of experts from medical genetics , psychiatry , pediatric oncology , molecular pathology , nursing , and behavioral science reviewed the items and domains for content and clarity and to ensure good content validity across the three domains.26 response categories included true , false , and not sure . 
health literacy was assessed with the newest vital sign.27 the six - question validated tool was scored as follows : 4 or greater ( adequate literacy ) , 2 to 3 ( possibly limited literacy ) , and 0 to 1 ( limited literacy )  . 
 numeracy was evaluated with an abbreviated ( five - question ) version of a validated objective numeracy scale , 28 which assessed the ability to comprehend risks and probabilities of disease . 
both measures were available in english and spanish . exploratory analyses were conducted by using two - tailed independent sample t tests to examine differences in pipseqkq scores for select dichotomized demographic variables : race / ethnicity ( white non - hispanic v others ) and educational attainment ( less than college / college v graduate / postgraduate )  . 
participants were contacted 2 weeks later by e - mail or standard post to complete the second pipseqkq ( required to be completed within 4 weeks after the first administration )  . 
participants who completed both surveys received a $15 gift card . data analysis pipseqkq responses were examined for high levels of nonresponse , which indicated an issue with an ite descriptive statistics were examined for all items . 
a floor or ceiling effect was present if more than 10% of participants achieved the results participants of the 135 eligible participants , 11 ( 8% ) declined participation and 13 ( 10% ) were not approached because of timing conflicts ( eg , rapid triage , radiology scans ) during their clinic visits . 
 ( % ) of patients ( n = 111 ) 34 ( 31 ) 77 ( 69 ) 35 ( 32 ) 76 ( 68 ) 103 ( 93 ) 8 ( 7 ) characteristic unknown health literacy limited possibly limited adequate numeracy limited adequate no . 
main health literacy and numeracy data are presented as mean ( standard deviation ) scores . * hematologic conditions consisted primarily of hematologic malignancies ( 61 of 65 )  . for race , other , 17 of 25 self - identified as dominican . pipseqkq scale and item descriptive statistics item response distributions that showed items for which knowledge and uncertainty were highest and lowest are displayed in figure 1 . 
 only a ceiling effect was detected for three items , which were retained for their importance in evaluation of general genetic knowledge and genetics knowledge related to health and cancer . 
test - retest reliability from the 75 participants who completed the pipseqkq twice was 0.82. pipseqkq scores figure 2 shows the proportion of correct and incorrect responses for the pipseqkq . 
internal and test - retest reliability knowledge domain general genetic concepts genetic concepts , general health , and cancer whole - genome / whole - exome sequencing concepts total score no . 
ggc , general genetic concepts ; gghc , general genetic concepts related to health and cancer ; sc , sequencing concepts . ggc1 ggc2 ggc3 ggc4 ggc5 ggc6 ggc7 gghc8 gghc9 gghc10 gghc11 gghc12 gghc13 gghc14 gghc15 gghc16 gghc17 gghc18 gghc19 sc20 sc21 sc22 sc23 sc24 sc25 sc26 sc27 sc28 sc29 sc30 sc31 sc32 sc33 sc34 sc35 correct incorrect not sure frequency of responses ( mean , 4.11 ; sd , 1.41 ; range , 1 to 7 of 7 )  . 
the two items with the most incorrect or not sure responses were the definition of an exome ( n = 79 ; 71% ) and that statement about blood containing a full copy of your genes ( n = 60 ; 53% )  . genetic concepts related to general health and cancer . 
the median domain score for genetic concepts related to general health and cancer was 8.0 ( mean , 8.07 ; sd , 2.37 ; range , 1 to 12 of 12 )  . 
the most frequent items answered incorrectly or not sure were wgs / wes in children with cancer performed at diagnosis will commonly guide initial treatment ( n = 97 ; 88% ) ; there are laws that prevent the use of genetic information to determine eligibility for life insurance , disability insurance , and long - term care insurance ( n = 102 ; 93% ) ; and wgs / wes will have no impact on cancer care for most children with cancer ( n = 98 ; 89% )  . 
 greater than 50% of participants were uncertain about the number of genes that can be tested with wgs and wes ( ie , a small subset v the complete set of genes ) , whether wgs and wes compares the dna of cancer cells to the dna of normal cells , whether wgs and wes can find changes in genes related to diseases other than cancer , and what vus means . 
last , although 60% understood that secondary findings also may provide information about present and future health risks of other family members , 36% were unsure of the correct answer . perceptions of risks and benefits of wgs and wes . 
furthermore , content validity was high , because item generation focused on areas of knowledge necessary to make informed decisions about wgs and wes . consistent with studies in other populations , 14 , 24 , 33 participants had a basic understanding of genetics and heredity . 
lower knowledge has been associated with racial and ethnic minority groups , 14 and we observed this for knowledge related to genetic concepts associated with health and cancer . the strengths and limitations of wgs and wes were not well understood . 
deficits in knowledge were observed for items related to the likelihood of wgs and wes to guide initial treatment or to have an effect on cancer care for most children and whether laws existed to prevent discrimination for certain types of insurance on the basis of genetic information . 
similar to tolusso et al , 39 we found that participants were uncertain about the ability of wgs and wes to examine the complete set of genes , compare tumor and normal dna , find changes in genes related to diseases other than cancer , and identify vus . although there is strong parent / patient interest in genomic sequencing , 17 , 40 - 43 its potential benefit in cancer care was overestimated . 
in a recent study of adult patients with advanced cancer , 64% who underwent genomic testing had a strong belief that testing would significantly improve their cancer care.42 similarly , results from the dana farber cancer institute44 revealed that parents and patients express significant hopes for molecular testing , particularly regarding increased number of treatment options ( 72% ) and increased hope for a cure ( 59% ) .17 in our study , 61% felt that even a small chance that their child would benefit outweighed all other risks of wgs and wes . 
thus far , relatively few pediatric patients with cancer who undergo genomic testing are matched to a targeted therapy.3 , 4 , 6 , 44 these findings reflect two salient issues in pediatric oncology . 
many of the newer molecularly targeted drugs lack efficacy data in pediatric diseases or safety data in children and , therefore , are not approved for administration in this population . 
 consequently , families should be provided with realistic information during consent discussions to manage expectations when they consider genomic testing . our previous work indicates that families strongly desire more education and improved modalities to communicate wgs and wes information before consent for genomic sequencing.18 similarly , parents have reported that the standard consent process for genome - wide sequencing was not adequate and have requested availability of more resources to aid their understanding.45 the pipseqkq is a valid tool that can help identify knowledge deficits and guide the development of patient education materials to improve understanding of wgs and wes . 
our center is testing the effectiveness of a web - based tool in english and spanish as an educational resource to improve patient education and informed consent for clinical wgs and wes . this study had a number of limitations to consider , which represent important areas for future research . 
 second , those surveyed had children who were off therapy for more than 1 year , and their prolonged exposure to treatment in a pediatric oncology center may have biased their knowledge of the concepts presented here , including their assessment of risk and benefit . 
third , we did not have sufficient sample size to validate the pipseqkq spanish version , evaluate cultural differences for non - english speaking participants , or conduct factor analyses or item - response theory analyses . 
last , a factor not addressed by the pipseqkq that is being investigated through ancillary studies relates to evaluation of the potential cost to families for clinical wgs and wes . 
insurance companies provide inconsistent coverage and variable payment for wgs and wes , and families will need to understand the financial responsibility they may incur from testing . in conclusion , as wgs and wes become more ubiquitous in pediatric oncology , medical providers will need to help families understand the benefits and limitations of testing , including the potential financial cost to the family for testing and the possible identification of secondary findings . 
this may be especially advantageous for providers who lack the expertise or time to fully engage with their patients about testing . our findings highlight that , although participants understand that there are risks and benefits of wgs and wes , many would accept any risk for the possibility of a small benefit , and their hope for a cure often exceeds the expected results from sequencing . 
the pipseqkq is a valid tool that can aid providers in precision oncology to identify levels of knowledge and tailor their informed consent discussions to best fit the patient and family . 
kung consulting or advisory role : darwin health , mi bioresearch , imago bioscience patents , royalties , other intellectual property : royalty from licensing agreements with mi bioresearch wendy k . 
glade bender research funding : bristol - myers squibb ( inst ) , pfizer ( inst ) , novartis ( inst ) , ignyta ( inst ) , amgen ( inst ) , celgene ( inst ) , eisai ( inst ) , lilly ( inst ) , merck ( inst ) travel , accommodations , expenses : novartis , amgen , merck jennifer m . 
worst bc , van tilburg cm , balasubramanian gp , et al : next - generation personalised medicine for high - risk paediatric cancer patients : the inform pilot study . 
marron jm , dubois sg , glade bender j , et al : patient / parent perspectives on genomic tumor profiling of pediatric solid tumors : the individualized cancer therapy ( icat ) experience . 
morren m , rijken m , baanders an , et al : perceived genetic knowledge , attitudes towards genetic testing , and the relationship between these among patients with a chronic disease . 
streicher sa , sanderson sc , jabs ew , et al : reasons for participating and genetic information needs among racially and ethnically diverse biobank participants : a focus group study . 
kaphingst ka , blanchard m , milam l , et al : relationships between health literacy and genomicsrelated knowledge , self - efficacy , perceived importance , and communication in a medically underserved population . 
langer mm , roche mi , brewer nt , et al : development and validation of a genomic knowledge scale to advance informed decision - making research in genomic sequencing . 
calsbeek h , morren m , bensing j , et al : knowledge and attitudes towards genetic testing : a two year follow - up study in patients with asthma , diabetes mellitus and cardiovascular disease . 
miller fa , hayeems rz , bytautas jp , et al : testing personalized medicine : patient and physician expectations of next - generation genomic sequencing in late - stage cancer care . 
mccullough lb , slashinski mj , mcguire al , et al : is whole - exome sequencing an ethically disruptive technology ? perspectives of pediatric oncologists and parents of pediatric patients with solid tumors . 
harris mh , dubois sg , glade bender jl , et al : multicenter feasibility study of tumor molecular profiling to inform therapeutic decisions in advanced pediatric solid tumors : the individualized cancer therapy ( icat ) study . 
chinnaiyan , md , phd4 , 5 case description in january 2018 , a 79 - year - old man was referred to our genitourinary medical oncology clinic for management of his prostate adenocarcinoma metastatic to multiple bones . 
his prostate cancer spread to additional bony sites , which were likewise treated with radiation , including radiation to the thoracic spine in july 2017 and the proximal humerus in august 2017 , rather than any systemic in december 2017 , he had prophylactic therapy . nipple irradiation to prevent gynecomastia in preparation for noncastrating medical therapy with singleagent bicalutamide . 
on meeting the patient for the rst time in january 2018 , we elected to continue with the plan for single - agent bicalutamide 50 mg per day , given the patients preference and the uncertain prognosis from his metastatic melanoma . 
his prostatespecic antigen ( psa ) was 30.8 ng / ml at the time of treatment initiation and responded rapidly to bicalutamide , reaching a nadir of 1.1 ng / ml in september 2018 ( fig 1a )  . his melanoma was diagnosed from a shave biopsy of the right superior lateral lower back in august 2015 as localized ulcerated malignant melanoma , unclassied , with nevoid features . 
he subsequently had a microstaging excision and a right back excision with a negative sentinel lymph node in the right groin 2017 , the patient noticed a new lump on his right lower back scar in 2017 . 
in november 2017 , excisional biopsies of his right lower back and right groin both showed metastatic melanoma , as conrmed by immunohistochemistry ( ihc ) showing positive staining for sox - 10 and mart - 1 . 
a 7 - mm lesion was also detected on his posterior scalp and was also visible on magnetic resonance imaging of his brain and metabolically active on positron emission tomography ( pet ) / computed tomography ( ct ) ; hence , it was diagnosed as stage iv melanoma . 
he began treatment of his metastatic melanoma with pembrolizumab 200 mg intravenous every 3 weeks and received four treatments before the pembrolizumab was stopped because of the development of pneumonitis . 
his pneumonitis was treated with a taper of prednisone , which was reduced to physiologic dosing by august 2018 . however , despite evidence of response in his melanoma by physical examination , there was concern for progression on pet / ct in june 2018 , with fdg update in the descending colon / small bowel wall , perisplenic region , a mildly fdg - avid left internal iliac lymph node , and a right external iliac nodal conglomerate encasing the right ureter , 4.1 cm in diameter and with an suv max of 11.7. 
 case report systemic therapy : gem - carbo docetaxel bicalutamide pembro bicalutamide leuprolide 1.1 ureter stent and pelvic mass biopsy abdominal wall excisional biopsy psa : ( ng / ml ) 30.8 event : date : 1 / 2018 6 / 2018 1 / 2019 6 / 2019 1 / 2020 6 / 2020 before gem - carbo after gem - carbo before docetaxel after docetaxel fig 1 . 
psa , prostate - specic antigen . pelvic mass was judged to be atypical for either prostate cancer or melanoma , it was biopsied by pelvic laparoscopy in november 2018 and was found on surgical pathology assessment to be consistent with a high - grade carcinoma with squamous features ( fig 2a )  . 
we performed exome sequencing using the university of michigan oncoseq panel ( mi - oncoseq ) and whole transcriptome analysis on formalin - xed parafn - embedded tissue from this biopsy . 
all patients enrolled in the mi - oncoseq study provided written informed consent approved by the university of michigan institutional review board . consent is inclusive of publishing information and / or images from participants ( or their designate )  . 
because the pelvic mass was causing pain and urinary obstruction , we elected to treat it with a platinum doublet active in urothelial carcinoma and carcinoma of unknown primary , despite not knowing the tissue of origin january 2019 , we began carboplatin area under the curve 5 mg / ml / minute on day 1 and gemcitabine 1 , 000 mg / m2 on days 1 and 8 of 21 - day cycles , and we completed six cycles before stopping because of progressive fatigue . 
 ( d ) ihc for erg of the primary prostate tumor showing strong labeling . ( e ) h&e histology of the abd wall nodule biopsy specimen used for molecular analysis . 
 ( f ) ihc for erg of the abd wall nodule showing much weaker labeling . in june 2019 , while being treated only with bicalutamide , the patient was noted on ct scan as having a 1.4 - cm nodule in the supercial anterior abdominal wall , which subsequently became easily palpable and caused skin together with smaller adjacent erythema . 
this nodule , nodules , was removed by excisional biopsy in july 2019 , where surgical pathology assessment demonstrated tumor features consistent with metastatic squamous cell carcinoma ( fig 2b )  . 
a fresh portion of this specimen was sent for analysis using the mi - oncoseq platforthis specimen showed a much higher tumor content of 54% , allowing the discovery of additional molecular alterations . precision medicine tumor board discussion results were discussed at the university of michigan precision medicine tumor board in september 2019 . somatic aberrations detected in the previous sample were detected in the new biopsy specimen , suggesting clonal relatedness , and additional alterations consistent with the increased tumor content were noted as well ( table 2 )  . 
for prostate adenocarcinoma , the addition of medical castration , likely in addition to either abiraterone and prednisone or a nonsteroidal second - generation antiandrogen , would have been a reasonable next line of therapy . 
however , the transcriptomics data of the mi - oncoseq platform showed low expression of the androgen receptor and androgen responsive genes klk2 , klk3 ( psa ) , tmprss2 , acpp , and slc45a3 ( fig 3b )  . 
therefore , we did not plan chemotherapy with a regimen such as carboplatin and etoposide , which is active against small - cell neuroendocrine carcinomas . we examined the remainder of the molecular results in an effort to nd alternative , clinically actionable molecular targets . 
however , overall , the results for mtor inhibitors in prostate cancer have been disappointing.3 some randomized data support the use of pi3k inhibitors in metastatic castration - resistant prostate cancer.4 however , this was in combination with abiraterone , which made pi3k inhibitors less attractive in this case , given the patients near total lack of androgen signaling . 
however , we decided against this option because cdk4 / 6 inhibitors have thus far shown disappointing results in prostate cancer.5 therefore , we elected to treat with docetaxel , the most common cytotoxic chemotherapy drug for castration - resistant prostate cancer . at this point , the patients lung nodules , which were previously indeterminate , had enlarged greatly ( fig 1d )  . 
we started treatment with docetaxel at 75 mg / m2 for one cycle , then decreased the dose to 60 mg / m2 because of fatigue , and completed three more cycles . 
ct completed after three cycles showed an interval decrease in the size of multiple bilateral lung nodules , and a decrease in size of his right pelvic mass , compatible with a therapeutic response ( fig 1e )  . discussion in this case , we used next - generation sequencing to determine that the patients squamous cell carcinoma was actually of prostate origin , because of the presence of a gene fusion between tmprss2 and erg . 
 case report prostate cancer subtypes has become more common since the development of abiraterone and nonsteroidal secondgeneration antiandrogens , 6 possibly as a means to escape continual selective pressure against androgen signaling , a phenomenon that had been described rarely in the past.9 some of these double - negative prostate cancer ( dnpc ) tumors seem to be driven by broblast growth factor ( fgf ) alterations , and trials of fgf inhibitors have recently begun in advanced prostate cancer.10 our patient did not have an fgf abnormality . 
in the current case , despite having squamous differentiation , this patient had only stable disease in response to platinum - based chemotherapy . after using whole exome sequencing and rna sequencing to identify this tumor as a squamous neoplasm of prostate origin , we elected to treat him with an agent approved for prostate cancer ( docetaxel ) , an agent we would not have elected to use without knowing the tissue of origwe elected not to pursue the therapies that could target molecular alterations in his tumor because of the known survival benet of docetaxel in men with advanced prostate cancer , but therapies targeting his tumors molecular alterations remain options down the road if his disease progresses . 
alumkal consulting or advisory role : merck sharp & dohme , dendreon research funding : aragon pharmaceuticals ( inst ) , astellas pharma ( inst ) , zenith epigenetics ( inst ) , gilead sciences ( inst ) travel , accommodations , expenses : astellas pharma , merck sharp & dohme other relationship : astellas pharma arul chinnaiyan stock and other ownership interests : oncopia , tempus , esanik , oncofusion therapeutics , medsyn consulting or advisory role : tempus patents , royalties , other intellectual property : co - inventor on a patent on the detection of ets gene fusions in prostate cancer issued to the university of michigan . no other potential conicts of interest were reported . acknowledgment we thank the mi - oncoseq clinical sequencing team , leslie fecher , md , jeff montgomery , md , and michael sabel , md , for collaborative clinical care and discussion ; alex hopkins for assistance with gures ; and jyoti athanikar for assistance with scientic editing and manuscript preparation . 
cell 161 : 1215 - 1228 , 2015 [ erratum : cell 162 : 454 , 2015 ] statz cm , patterson se , mockus sm : mtor inhibitors in castration - resistant prostate cancer : a systematic review . 
target oncol 12 : 47 - 59 , 2017 de bono js , de giorgi u , rodrigues dn , et al : randomized phase ii study evaluating akt blockade with ipatasertib , in combination with abiraterone , in patients with metastatic prostate cancer with and without pten loss . 
clin cancer res 25 : 928 - 936 , 2019 clinicaltrials.gov : a phase ii study of androgen deprivation therapy with or without palbociclib in rb - positive metastatic prostate cancer . 
gov / ct2 / show / nct02059213 bluemn eg , coleman im , lucas jm , et al : androgen receptor pathway - independent prostate cancer is sustained through fgf signaling . 
cancer cell 32 : 474 - 489.e6 , 2017 labrecque mp , coleman im , brown lg , et al : molecular proling straties diverse phenotypes of treatment - refractory metastatic castration - resistant prostate cancer . 
j clin invest 129 : 4492 - 4505 , 2019 parwani av , kronz jd , genega em , et al : prostate carcinoma with squamous differentiation : an analysis of 33 cases . 
weindorf sc , taylor as , kumar - sinha c , et al : metastatic castration resistant prostate cancer with squamous cell , small cell , and sarcomatoid elementsa clinicopathologic and genomic sequencing - based discussion . 
 major response to carboplatin in a patient with metastatic triple - negative breast cancer with somatic mutation of brca1 and loss of rad51b lor `ene seguin , md1 ; max chaffanet , phd , hdr1 ; s everine garnier , phd1 ; jos e ad elade , msc1 ; nadine carbuccia , msc1 ; arnaud guille , msc1 ; jihane pakradouni , pharmd , phd2 ; renaud sabatier , md , phd1 ; cornel popovici , md , phd2 ; daniel birnbaum , md , phd1 ; franois bertucci , md , phd1 ; and anthony goncalves , md , phd1 background triple - negative breast cancer ( tnbc ) , clinically dened as not expressing estrogen receptor , progesterone receptor , and human epidermal growth factor receptor 2 tyrosine kinase receptor , accounts for approximately 15% of breast cancers and is associated with a poor prognosis and a lack of recognized molecular targets for therapeutics.1 some 15% to 20% of tnbcs arise in patients with brca1 germline mutations , and tnbc is the most common molecular subtype in this context.2 breast cancer type 1 susceptibility protein ( brca1 ) and many other proteins , such as the dna repair protein rad 51 homolog 1 ( rad51 ) paralogs , are involved in the dna homologous recombination ( hr ) repair pathway.3 breast cancers associated with germline brca mutations display dna double - strand break repair defects , which is believed to render them particularly sensitive to dna repairtargeting drugs such as poly ( adp ) ribose polymerase ( parp ) inhibitors , 4 but also to dna - damaging agents , such as platinum analogs.5 although the presence of germline brca1 / 2 mutations was recently shown to predict benet of platinum compounds , 6 little is known about other determinants of efcacy of this class of cytotoxics . 
clinical procedures performed after molecular tumor board decision were done according to routine clinical management . in july 2015 , a 72 - year - old woman presented with a ct2n0m0 tumor of the right breast . 
biopsy showed scarff - bloom - richardson grade 3 , triple - negative invasive carcinoma , which was treated by breastconserving surgery and axillary lymph node dissection ( fig 1 )  . 
pathologic examination of surgical specimen revealed a 5 - cm invasive ductal breast carcinoma , nuclear grade 3 , with lymphovascular invasion and two of 16 axillary lymph nodes invaded by metastasis , one with extracapsular spread . immunohistochemistry did not show any expression of estrogen receptor , progesterone receptor , human epidermal growth factor receptor 2 , or cytokeratins 5 and 6 ; ki67 antigen was expressed by 50% of malignant cells . 
then , because of positive margins , a mastectomy was done , without pathologic residual tumor , followed by adjuvant radiotherapy started on february 2016 . in april 2016 , while the patient was ending radiotherapy , she presented visual troubles , dizziness , and gait disorders . 
at this time , the disease progressed in the lung and liver , with stable cranial disease , and she received three cycles of pembrolizumab between september 2016 and november 2016 in the context of a clinical trial . 
the disease progressed at both cranial and extracranial levels , and she was enrolled in november of 2016 in ( clinicaltrials.gov identier : our permed - 01 trial nct02342158 ) , whose aim is to identify targetable molecular alterations in locally advanced and metastatic tumors . 
2018 adjuvant adj rt brain relapse nodes liver , lung , nodes , brain liver , lung , nodes , brain liver , lung , nodes , brain cr ( nodes , lung , and liver ) pd in brain fec100 - wptx wbrt cape pembro eribulin re - xrt brain , carboplatin diagnosis surgery fig 1 . 
adj , adjuvant ; cape , capecitabine ; cr , complete response ; ct , computed tomography ; fec100 , uorouracil - epirubicine 100mg / m - cyclophosphamide ; mst , mastectomy ; pd , progressive disease ; pembro , pembrolizumab ; rt , radiotherapy ; wbrt , whole - brain radiation therapy ; wptx , weekly paclitaxel ; xrt , radiation therapy . genomic copy number aberrations and somatic mutation status were identied on metastatic tissue by using wholegenome array - comparative genomic hybridization ( acgh ) and targeted next - generation sequencing of 559 actionable genes , as previously described7 , 8 ( data supplement )  . 
analysis of germline dna revealed no brca mutation . in may 2017 , after an initial partial response to eribulin , the disease spread to brain ( multifocal ) , lung , mediastinum lymph nodes , and liver ( figs 3 and 4 ) , and a molecular tumor board recommended treatment with platinum derivatives . the patient started single - agent carboplatin ( area under the curve = 5 mg / ml / min ) in june 2017 . 
after three cycles of carboplatin in august 2017 , a striking partial response was observed at the extracranial level ( fig 3 ) , and a signicant partial response was observed at the brain level in december 2017 after seven cycles of carboplatin ( fig 4 )  . 
the patient was seen on february 2018 , after only one additional cycle of carboplatin ( in january 2018 ) , because of thrombocytopenia ; a complete response was still observed in lung , mediastinum , and liver . 
in april 2018 , a persistent , nearly complete response was noted at the extracranial level ( fig 3 ) , but the disease progressed in the brain , with deterioration of the patients clinical status . 
because of the small sample size of this analysis , however , relevant conclusions cannot be drawn from this small subset . germline palb2 mutations may also be associated with platinum sensitivity.10 similarly , proofs of efcacy of parp inhibitors in patients with advanced breast cancer have been restricted to patients with germline brca mutations , 11 , 12 and no clinical data exist demonstrating efcacy of these drugs in patients with somatic brca mutations . 
in addition to germline or somatic brca mutations , brca1 / 2 promoter methylation , as well as other numerous non - brca genomic alterations , may also drive hrd and the so - called brcaness phenotype . 
computed tomography scan was obtained before ( may 2017 , left panel ) and after carboplatin ( august 2017 , middle panel ; april 2018 , right panel ) showing a nearly complete response at the extracranial level . been associated with predisposition to breast cancer.13 the recruitment of rad51 to dna double - strand breaks is dependent on rad51 paralogs ( ie , rad51b , rad51c , rad51d , xrcc2 , and xrcc3 ) as well as on rad52 , the deciency of which worsens the phenotype of brca1 , brca2 , or palb2 alterations.14 interestingly , preclinical evidence shows that inactivation of rad51b increases sensitivity to dna - damaging agents , including platinum , because of both alteration in the cell cycle checkpoint response and impairment in hr repair.15 in addition , recent data indicate that the functionality of hr , as measured by rad51 foci , may predict sensitivity to parp inhibitors in brca - mutated breast cancer.16 thus , in the case presented here , loss of rad51b and somatic brca1 mutation may have cooperated to induce a brcaness phenotype , as suggested by the high hrd score identied by acgh . of note , despite experiencing initial response , the disease ultimately progressed at the brain level only , in the context of chemotherapy delay due to persistent carboplatinrelated thrombocytopenia . 
yet , at the time of this case report , parp inhibitors were not routinely available for patients with breast cancer in france . to estimate the clinical relevance of rad51b alterations , we examined their frequency in the permed trial as well as in other public databases , either alone or in combination with brca mutations . 
these results are discussed in the appendix . in conclusion , we have described a major response to carboplatin in a heavily pretreated patient with tnbc with somatic alterations in dna repair genes , suggesting that this class of potent and inexpensive cytotoxics could be used as an authentic targeted therapeutic in a precision fig 2 . 
arrowheads indicate lesions subjected to stereotactic radiation ; arrows show subcentimetric lesions not subjected to radiation but regressive after systemic treatment . to its medicine perspective using biomarkers pertinent mechanisms of action . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . renaud sabatier honoraria : novartis , astrazeneca , pzer research funding : novartis ( inst ) , eisai ( inst ) , astrazeneca ( inst ) travel , accommodations , expenses : amgen , pzer cornel popovici travel , accommodations , expenses : astrazeneca anthony goncalves research funding : msd ( inst ) , bristol - myers squibb ( inst ) , novartis ( inst ) , cascadian therapeutics ( inst ) , nektar ( inst ) , boehringer ingelheim ( inst ) , eli lilly ( inst ) , abbvie ( inst ) , genentech ( inst ) , astrazeneca ( inst ) , roche ( inst ) travel , accommodations , expenses : pzer , novartis , genentech , celgene no other potential conicts of interest were reported . acknowledgment we thank the computing facilities disc ( datacenter it and scientic computing , centre de recherche en canc erologie de marseille ) for their technical support . 
n engl j med 363 : 1938 - 1948 , 2010 bianchini g , qi y , alvarez rh , et al : molecular anatomy of breast cancer stroma and its prognostic value in estrogen receptor - positive and - negative cancers . j clin oncol 28 : 4316 - 4323 , 2010 3 . 
oncogene 22 : 7265 - 7279 , 2003 tutt a , tovey h , cheang mcu , et al : carboplatin in brca1 / 2 - mutated and triple - negative breast cancer brcaness subgroups : the tnt trial . 
nat med 24 : 628 - 637 , 2018 bertucci f , finetti p , guille a , et al : comparative genomic analysis of primary tumors and metastases in breast cancer . 
oncotarget 7 : 27208 - 27219 , 2016 gonalves a , bertucci f , guille a , et al : targeted ngs , array - cgh , and patient - derived tumor xenografts for precision medicine in advanced breast cancer : a single - center prospective study . 
oncotarget 7 : 79428 - 79441 , 2016 abkevich v , timms km , hennessy bt , et al : patterns of genomic loss of heterozygosity predict homologous recombination repair defects in epithelial ovarian cancer . 
br j cancer 107 : 1776 - 1782 , 2012 isaac d , karapetyan l , tamkus d : association of germline palb2 mutation and response to platinum - based chemotherapy in metastatic breast cancer : a case series . 
lok bh , carley ac , tchang b , et al : rad52 inactivation is synthetically lethal with deciencies in brca1 and palb2 in addition to brca2 through rad51mediated homologous recombination . 
cruz c , castroviejo - bermejo m , guti errez - enrquez s , et al : rad51 foci as a functional biomarker of homologous recombination repair and parp inhibitor resistance in germline brca - mutated breast cancer . 
lin nu , claus e , sohl j , et al : sites of distant recurrence and clinical outcomes in patients with metastatic triple - negative breast cancer : high incidence of central nervous system metastases . 
 platinum in tnbc with brca1 somatic mutation and loss of rad51b appendix can this observation be extended to other patients of our trial or other institutions ? another patient with refractory triple - negative breast cancer ( tnbc ) enrolled in the permed - 01 trial displayed rad51b homozygous deletion with high homologous recombination deciency ( hrd ) score in the biopsy of a skin metastasis ; yet , at the time of the manuscript writing , this patient did not receive platinum salt or poly ( adp ) - ribose polymerase inhibitor . 
because of its potential therapeutic interest , we assessed the frequency of rad51b homozygous deletion in the the cancer genome atlas ( tcga ; abouttcga / overview ) and genomics evidence neoplasia information exchange , version 4 ( genie ; aacr project genie consortium : cancer discov 7 : 818 - 831 , 2017 ) public databases . 
this alteration was rare , with only 21 ( approximately 0.2% ; 21 of 10 , 837 ) and 35 ( approximately 0.1% ; 35 of 35 , 498 ) cases in each database , respectively ( data supplement )  . 
in breast cancer , rad51b homozygous deletion was observed in 0.09% of cases in both databases ( one case out of 1 , 079 in tcga and four out of 4 , 421 in genie ; data supplement ) , which are exclusively or mostly composed of primary tumor samples ( appendix fig a1a )  . 
although remaining quite uncommon , the detection of this alteration in two tnbc samples out of the rst set of 183 patients with advanced breast cancer enrolled in the permed - 01 trial , including 64 tnbcs , suggests that rad51b homozygous deletion may be enriched this subtype . 
we also examined public in metastatic samples of databases for the concomitant presence of brca mutation and rad51b deletion and found it at variable frequencies in cancer : rad51b homozygous deletion combined with brca mutation was only observed in two cases , a bladder urothelial cancer ( tcga ) and a breast cancer ( genie ) , both involving brca2 and never brca1 ( data supplement )  . 
however , among 8 , 851 patients with various cancers from tcga , 8% ( 709 of 8 , 851 ) of tumor genomic proles exhibited the double event combining heterozygous mutation or loss of rad51b with heterozygous mutation or loss of brca . the top ve frequencies were 28% in ovarian serous cystadenocarcinomas ( 163 of 579 ) , 25% in uterine carcinosarcomas ( 14 of 56 ) , 19% in cholangiocarcinomas , 14% in sarcomas ( 37 of 256 ) and mesotheliomas ( 12 of 87 ) , as well as 11% in breast invasive carcinoma ( 118 of 1 , 074 ; appendix fig a1b )  . 
moreover , a similar highly signicant association was observed between the concomitant presence of double heterozygous ( rad51b loss or mutation and brca loss or mutation ) events and hrd ( p , .001 ; appendix fig a2b , right )  . 
altogether , these data suggest that combination of genomic alterations in the dna repair pathway , including heterozygous alterations , may increase hrd and thus expand the population of patients who are candidates for therapeutic targeting of this pathway . 
 ( a ) hrd score was calculated as described in abkevich9 and is presented as box plots in patients with ( left ) and without ( right ) rad51b homozygous deletion . 
 high expression of fgd3 , a putative regulator of cell morphology and motility , is prognostic of favorable outcome in multiple cancers purpose identification of single - gene biomarkers that are prognostic of outcome can shed new insights on the molecular mechanisms that drive breast cancer and other cancers . methods exploratory analysis of 20 , 464 single - gene messenger rnas ( mrnas ) in the molecular taxonomy of breast cancer international consortium ( metabric ) discovery cohort indicates that low expression of fgd3 mrna is prognostic for poor outcome . 
2017 by american society of clinical oncology licensed under the creative commons attribution 4.0 license scooter willis yuliang sun mark abramovitz teng fei brandon young xiaoqian lin min ni justin achua meredith m . 
goldstein roberto salgado sherene loi giancarlo pruneri giuseppe viale myles brown brian leyland - jones author affiliations and support information ( if applicable ) appear at the end of this article . the contents are solely the responsibility of the authors and do not necessarily represent the official views of the national cancer institute . ( continued ) introduction an increasing collection of breast cancer cohorts have been molecularly profiled on affymetrix and illumina platforms , so it is now feasible to conduct an exploratory analysis to identify single - gene biomarkers in which messenger rna ( mrna ) expression is prognostic of outcome.1 by limiting the exploratory analysis to a single gene , we intended to identify novel gene ( s ) that might provide insight into biological mechanisms that drive breast cancer metastasis.2 the starting point for this analysis was the molecular taxonomy of breast cancer international consortium ( metabric ) data set , which contains clinical traits , expression data , copy number variation profiles , and single nucleotide polymorphism genotypes derived from breast tumors collected from participants in the metabric trial.3 we also used the genomic data commons , which incorporates the cancer genome atlas ( tcga ) cancer cohorts and currently spans 21 cancer types suitable for survival analysis . 
fgd3 and susd34 cell motility genes were compared as a single - gene biomarker with proliferation genes mki67 , 5 , 6 aurka , 7 - 10 and pcna11 , 12 in six distinct breast cancer cohorts and as a pan - cancer biomarker in tcga cancer cohorts . 
fgd3 mrna expression as a biomarker for an immune response was evaluated by using tumor - infiltrating lymphocyte cells in tcga breast cancer and breast international group 1 - 98 ( big 1 - 98 ; letrozole or tamoxifen in treating postmenopausal women with breast cancer ) cohorts . 
esr1 transcriptional regulation of fgd3 mrna expression in the breast cancer cell line zr - 75 - 1 was confirmed . methods cohorts detailed description of each cohort is provided in the data supplement . survival analysis to illustrate the outcome benefit of low versus high expression , the kaplan - meier method13 was used to estimate the distribution of timeto - disease outcome end points by gene expression status bifurcated on the cohort mean and median ( data supplement )  . 
the wald - test p values from cox proportional hazards models for the association of cancer outcomes with gene expression as a continuous variable for each cohort were used to determine the stouffer weighted z - test p value . 
tumor - infiltrating lymphocytes ( tils ) were called in 389 samples from tcga breast cancer high - resolution slide images using methods previously defined by the international til working group 2014.20 tils were called using a similar methodology in 725 samples from the big 1 - 98 dasl cohort , and correlation to fgd3 mrna expression was determined by using pearsons correlation coefficient ( r ) .21 fgd3 protein expression analysis fgd3 protein expression in tumor samples was determined by immunohistochemical ( ihc ) staining . 
breast cancer samples were provided by avera cancer institute , and breast cancer tmas ( br1504a , br1505b , hbre - duc068bch - 01 , and br20837 ) were purchased from us biomax ( rockville , md )  . fgd3 protein expression was quantitatively determined in the range of 0 to 4 . 
the us biomax metadata indicates whether the patient had no regional lymph node metastasis ( n0 ) or degrees of metastasis in regional lymph nodes ( n1 to n3 )  . fgd3 expression levels for samples with n0 designation ( n = 135 ) and samples with n1 to n3 designations in metastatic tissue ( n = 98 ) were compared by using an unpaired t test . 
tissues for matched lymph node metastasis ( n = 103 ) were compared with primary tumor tissues using unpaired t test , and figures were generated using graphpad prism 7.0. 
additional details on analysis can be found in the data supplement . fgd3 mrna expression regulated by estrogen receptors breast cancer cell line zr - 75 - 1 was grown in rpmi - 1640 medium with 10% fetal bovine serufor the treatment of estrogen , cells were deprived of hormone for 3 days in phenol - free rpmi - 1640 medium with 5% charcoal - stripped fetal bovine serum and then treated with either ethanol ( vehicle ) or 1 nm 17b - estradiol ( estrogen ) for 16 hours . 
reverse transcriptase - quantitative polymerase chain reaction ( rt - qpcr ) was performed and is described in the data supplement . mrna expression of genes of interest with published data the expression atlas web site22 was used to query rna sequencing ( rna - seq ) expression levels in breast cancer cell lines . 
 used to illustrate differences in differential expression of the proliferation genes using prism 7.0. continuous and categorical variables , kaplanmeier figures split on cohort means , and expression profiles can be found in the data supplement . results discovery of fgd3 we undertook an exploratory analysis of 20 , 464 possible single - gene biomarkers as categorical variables split on the mean in the metabric discovery cohort and identified fgd3 mrna expression as the highest ranked prognostic gene based on the p value for overall survival ( os ) , which we subsequently verified as being prognostic in the metabric validation cohort ( data not shown )  . 
the hungarian academy of science ( has ) breast cancer cohort represents a collection of all publicly available breast cancer cohorts profiled on the affymetrix platforthe kaplanmeier plotter web interface allows selection of has cohorts on the basis of er status using the mrna expression level . 
hungarian academy of science breast cancer cohort kaplanmeier plots for recurrencefree survival splitting on fgd3 median messenger rna ( mrna ) expression in which estrogen receptor ( er ) positive status is derived from mrna using the kaplan - meier plotter web interface to generate graphs . 
to determine whether fgd3 was a prognostic biomarker in a specific prediction analysis of microarray 50 ( pam50 ) subtype , the has cohort was subdivided via the web interface for the kaplan - meier plotter . 
hungarian academy of science breast cancer cohort kaplan - meier plot for recurrence - free survival splitting on fgd3 median messenger rna ( mrna ) expression in the prediction analysis of microarray 50 subtype . 
seven of the 21 tcga cohorts did not have a single - gene biomarker from the list ( fgd3 , susd3 , mki67 , pcna , aurka ) that was prognostic . 
by using the biomarker p value and the number of samples in each cohort , the stouffer25 p value was calculated to rank the prognostic value as a pan - cancer biomarker . 
by using the tcga cohort , tils were called from high - resolution images , and fgd3 mrna expression did not correlate with tils evaluated on hematoxylin and eosin slides defined by using a previously published method26 in which tils represented a pre - existing antitumor t - cell response ( unpublished data )  . 
in addition , til calls from the big 1 - 98 dasl cohort did not correlate with fgd3 mrna expression . to further investigate whether fgd3 mrna expression is a feature of the tumor , breast cancer tmas were purchased from us biomax , and ihc was used to determine fgd3 protein expression levels ( scored from 0 to 4 )  . 
by using metadata provided by us biomax , fgd3 protein levels in tumors ( n = 135 ) with no regional lymph node metastasis ( n0 ) were compared with tumors with lymph node metastasis ( n1 to n3 ) and corresponding matched metastatic tissues ( fig 4 )  . an unpaired t test comparing n0 with n1 to n3 suggests that lymph node metastasis is associated with lower fgd3 protein levels ( p , 1e - 4 )  . 
benign tumors ( fig 5a ) and breast adenocarcinomas in lower stages ( fig 5b - c ) showed strong expression of fgd3 , whereas late - stage breast adenocarcinomas in higher stages ( fig 5d - f ) showed mild to weak expression . 
stage iia invasive breast cancer ( data supplement ) showed strong fgd3 expression compared with its matched metastatic carcinoma ( data supplement ) , in which fgd3 was weakly expressed . 
this is a significant finding in the tcga cohorts , considering the median survival time in these cohorts was typically less than 2 years . fgd3 has a putative guanine nucleotide exchange factor that targets cell division control protein 42 homolog ( cdc42 ) 31 and shares high sequence similarity with fgd1 in their dbl homology ( 70% ) and pleckstrin homology ( 60.6% ) domains ; however , fgd3 lacks the n - terminal proline - rich domain found in fgd1 . 
the proline - rich domain plays a crucial role in the response to extracellular signal - responsive translocation of fgd1 to the leading - edge membrane in cells facing toward a wound during the wound - healing process.32 through a highly conserved recognized destruction motif ( dsgids ) in both fgd3 and fgd1 as well as in other unrelated proteins including ikbs and b - catenin , downregulation occurs through the ubiquitin / proteasome system via phosphorylation by gsk - 3b of the serine residues in the dsgids motif.33 thus , both fgd3 and fgd1 intracellular levels are tightly regulated by the same destruction pathway . 
functionally , fgd1 is involved in the regulation of cellular structures required for invadopodia biogenesis and extracellular matrix degradation in an invasive cell model by modulating cdc42 activation.34 - 37 in addition , mutations in fgd1 are responsible for the x - linked disorder known as faciogenital dysplasia , and fgd1 is highly expressed during bone growth and mineralization.36 using the hela tet - off cell system , hayakawa et al31 showed that notwithstanding their similarity , fgd3 and fgd1 played quite different roles in regulating cellular functions . 
furthermore , inducible expression of fgd3 resulted in significant morphologic changes that included the formation of broad sheet - like protrusions known as lamellipodia when gtpbound cdc42 levels were significantly increased by the inducible expression of fgd3 , whereas high expression of fgd1 led to the formation of filopodia , which are found in migrating cells.31 thus , cell motility seemed to be inversely regulated by fgd3 and fgd1 : fgd3 inhibited cell migration and fgd1 stimulated it . the fgd3 - susd3 metagene ( these genes share the same chromosomal location directly adjacent to each other at chr9q22.31 ) was ranked with the highest concordance index38 in the sage bionetworks - dream breast cancer prognosis challenge and was a key biomarker presented by ascopubs.org / journal / po jco precision oncology 7 n1 - n3 metastatic lymph node metastatic fgd3 protein expression is inversely associated with stage . published esr1 chromatin immunoprecipitation sequencing data in breast cancer cell lines mcf - 727 and zr - 75 - 128 identified a conserved esr1 binding site within the gene locus of fgd3 ( data supplement )  . 
by using rt - qpcr , we also determined that estradiol stimulation substantially increased the mrna expression level of fgd3 , as well as the known esr1 targeted gene tff1 in the zr - 75 - 1 cell line ( data supplement )  . 
in a previously published esr1 knockdown experiment in the mcf - 7 erpositive breast cancer cell line , fgd3 was downregulated by 2.9 and susd3 by 1.3 on a log2 scale ( data supplement ) .29 cbioportal was used to query co - expression relationships in the metabric cohort , which showed a tendency toward cooccurrence with p , .001 and a log odds ratio of 1.52. the tcga breast cohort showed a tendency toward co - occurrence with p , .001 and a log odds ratio of 2.3 in tma expression data . 
surprisingly , fgd3 mrna expression in bt - 20 , a triple - negative breast cancer cell line , was upregulated to 1.99 and esr1 was upregulated to 0.47 on a log2 scale when treated with an egfr inhibitor ( data supplement ) .30 discussion the exploratory analysis of 20 , 464 possible singlegene biomarkers in the metabric discovery cohort identified fgd3 as a highly prognostic biomarker . 
 ( a ) strong fgd3 expression in benign tumor and ( b - c ) at lower cancer stages i and iia , ( d - e ) mild fgd3 expression at stages iib and iiia , and ( f ) weak fgd3 expression at stage iiib . the group submitting the winning model.39 using the metabric data set , 3 they determined that the expression value of two genes , fgd3 and susd3 , was the most prognostic molecular metagene marker associated with a good prognosis , and they referred to it as a protective metagene because it displayed a ci that was significantly less than 0.5. 
the prognostic significance of fgd3 and susd3 as single gene prognostic biomarker using cox regression models in a large collection of breast cancer cohorts and tcga cohorts has not been published . in a follow - up study , the group developed a breast cancer prognostic test , breast cancer attractor metagenes ( bcam ) , which had several molecular features , including the breast cancerspecific fgd3 - susd3 metagene , as well as tumor size , and number of positive lymph nodes.41 notably , ou yang et al41 went on to suggest that breast cancer subtype classification as well as hormone receptor and her2 status did not add additional prognostic information when expression levels of the fgd3susd3 metagene and the attractor metagenes were known and taken into consideration . in a similar manner , susd3 expression was found to be regulated by esr1 in mcf - 7 cells through direct interaction of e2 with its regulatory region . experiments in mcf - 7 cells further showed that susd3 was implicated in e2 - mediated cell proliferation , adhesion , and migration.4 however , as with fgd3 , the role that susd3 plays in er - positive breast cancer has not been fully established . on the basis of normal tissue expression profiles , fgd3 is highly expressed in t cells , natural killer cells , monocytes associated with immune response , and myeloid whole blood cells . 
a characteristic of these cell types is that they are mobile , and evidence from the hela tet - off wound healing assay suggests that high expression of fgd3 limits cell mobility.31 fgd3 mrna expression did not correlate with tils in the big 1 - 98 dasl and tcga breast cancer cohorts , suggesting that the prognostic value of fgd3 is not indicating immune cells in patients tumors . ihc data from breast cancer tmas indicates that fgd3 protein expression is a feature of the tumor , and low expression indicates a higher chance of cell migration to lymph nodes . 
big 1 - 98 , breast international group 1 - 98 [ trial ] ; e2197 , combination chemotherapy in treating women with breast cancer [ trial ] ; er , estrogen receptor ; has , hungarian academy of science ; her2 - e , human epidermal growth factor receptor 2 subtype e ; metabric , molecular taxonomy of breast cancer international consortium ; os , overall survival ; rna - seq , rna sequencing . wide range of treatment options . 
comparing the prognostic value of fgd3 in breast cancer with the prognostic value of genes associated with proliferation such as mki67 , pcna , and aurka indicates that fgd3 may offer superior disease progression metrics in all clinically relevant breast cancer subtypes ( fig 6a )  . 
overall , aurka is the most prognostic gene in the tcga cancer cohorts in which the median time of 2 years suggests that it is an indicator of early relapse as measured by os ( fig 6b )  . 
a pubmed search for fgd3 and cancer mentioned in the abstract resulted in one publication.41 repeating the pubmed search for the other proliferation genes resulted in the following publication metrics ( mki67 , 92 ; ki67 , 3 , 104 ; pcna , 2 , 741 ; and aurka , 284 )  . the key differentiator of fgd3 as a putative biomarker is that high expression indicates favorable outcome ; for other established proliferation biomarkers , high expression of mki67 , ki67 , pcna , and aurka are prognostic of poor outcome . the availability of a growing collection of cancer cohorts with outcome data has allowed for the confirmation of the clinical importance of fgd3 as a prognostic biomarker and implications that can guide treatment . 
regan , myles brown , brian leyland - jones financial support : myles brown , brian leyland - jones administrative support : roswitha kammler , joseph a . sparano , brian leyland - jones provision of study materials or patients : joseph a . 
sparano , brian leyland - jones collection and assembly of data : scooter willis , mark abramovitz , teng fei , brandon young , xiaoqian lin , min ni , justin achua , meredith m . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . scooter willis no relationship to disclose yuliang sun no relationship to disclose mark abramovitz no relationship to disclose teng fei no relationship to disclose brandon young no relationship to disclose xiaoqian lin no relationship to disclose min ni no relationship to disclose justin achua employment : avera mckennan hospital meredith m . 
regan consulting or advisory role : merck , ipsen ( inst ) research funding : veridex ( inst ) , oncogenex ( inst ) , pfizer ( inst ) , ipsen ( inst ) , novartis ( inst ) , merck ( inst ) , ferring ( inst ) , celgene ( inst ) , astrazeneca ( inst ) , pierre fabre ( inst ) , ipsen ( inst ) kathryn p . 
gray stock and other ownership interests : mdgn robert gray research funding : abbott molecular , agios , amgen , astrazeneca , bristol - myers squibb , boehringer ingelheim , celgene , genentech , genomic health , genzyme , glaxosmithkline , imclone systems , janssen - ortho , kanisa , millennium , nodality , onyx , osi pharmaceuticals , pfizer , sanofi , sequenta , syndax , novartis victoria wang no relationship to disclose bradley long no relationship to disclose roswitha kammler no relationship to disclose joseph a . 
goldstein honoraria : genentech , roche pharma ag , puma biotechnology , pfizer , glenmark consulting or advisory role : genentech , domp e farmaceutici , roche pharma ag , puma biotechnology , pfizer , merck , astrazeneca research funding : merck ( inst ) , genentech ( inst ) other relationship : roche pharma ag roberto salgado travel , accommodations , expenses : roche sherene loi research funding : genentech ( inst ) , pfizer ( inst ) , novartis ( inst ) , merck ( inst ) , puma biotechnology ( inst ) , bristol - myers squibb ( inst ) patents , royalties , other intellectual property : pi3k pathway gene signature granted by the european and us patent offices ( inst ) myles brown consulting or advisory role : novartis , gtx research funding : novartis patents , royalties , other intellectual property : : as part of my work at the dana - farber cancer institute i have made invention disclosures and the institute is filing patents on technology related to endocrine resistance in breast cancer and improved crispr dual sgrna library design . travel , accommodations , expenses : gtx brian leyland - jones stock and other ownership interests : catalyst pharmaceuticals , progenix , puma biotechnology , sucampo pharmaceuticals , ariad , zogenix consulting or advisory role : glaxosmithkline , amgen speakers bureau : genentech , exelixis research funding : takeda , tesaro expert testimony : amgen giancarlo pruneri no relationship to disclose giuseppe viale honoraria : msd oncology consulting or advisory role : dako , genentech , astrazeneca , bristol - myers squibb , astellas pharma travel , accommodations , expenses : roche , celgene scooter willis , yuliang sun , mark abramovitz , brandon young , xiaoqian lin , justin achua , casey williams , and brian leyland - jones , avera cancer institute , sioux falls , sd ; teng fei , meredith m . 
gray , robert gray , victoria wang , and myles brown , dana - farber cancer institute , boston , ma ; min ni , childrens medical center research institute , university of texas southwestern medical center , dallas , tx ; bradley long , molecular core , scripps florida , jupiter , fl ; roswitha kammler , international breast cancer study group , bern , switzerland ; joseph a . 
goldstein , fox chase cancer center , philadelphia , pa ; roberto salgado , breast cancer translational research laboratory / institut jules bordet , brussels , belgium ; sherene loi , peter maccallum cancer centre , east melbourne , vic , australia ; and giancarlo pruneri and giuseppe viale , european institute of oncology , university of milan , milan , italy . affiliations support supported by public health service grants ca23318 , ca66636 , ca21115 , ca49883 , ca14958 , ca39229 , ca16116 , ca27525 , and ca114737 ( to the e2197 study ) from the breast cancer research foundation , national cancer institute ( nci ) , national institutes of health , department of health and human services ; by the susan g . 
bullwinkel j , baron - l uhr b , l udemann a , et al : ki - 67 protein is associated with ribosomal rna transcription in quiescent and proliferating cells . 
nouri m , ratther e , stylianou n , et al : androgen - targeted therapy - induced epithelial mesenchymal plasticity and neuroendocrine transdifferentiation in prostate cancer : an opportunity for intervention . 
lv q , zhang j , yi y , et al : proliferating cell nuclear antigen has an association with prognosis and risks factors of cancer patients : a systematic review . 
salgado r , denkert c , demaria s , et al : the evaluation of tumor - infiltrating lymphocytes ( tils ) in breast cancer : recommendations by an international tils working group 2014 . 
petryszak r , keays m , tang ya , et al : expression atlas update : an integrated database of gene and protein expression in humans , animals and plants . 
gy } orffy b , surowiak p , budczies j , et al : online survival analysis software to assess the prognostic value of biomarkers using transcriptomic data in non - small - cell lung cancer . 
gyorffy b , lanczky a , szallasi z : implementing an online tool for genome - wide validation of survival - associated biomarkers in ovarian - cancer using microarray data from 1287 patients . 
denkert c , wienert s , poterie a , et al : standardized evaluation of tumor - infiltrating lymphocytes in breast cancer : results of the ring studies of the international immuno - oncology biomarker working group . 
hayakawa m , matsushima m , hagiwara h , et al : novel insights into fgd3 , a putative gef for cdc42 , that undergoes scf ( fwd1 / beta - trcp ) - mediated proteasomal degradation analogous to that of its homologue fgd1 but regulates cell morphology and motility differently from fgd1 . 
oshima t , fujino t , ando k , et al : proline - rich domain plays a crucial role in extracellular stimuli - responsive translocation of a cdc42 guanine nucleotide exchange factor , fgd1 . 
ayala i , giacchetti g , caldieri g , et al : faciogenital dysplasia protein fgd1 regulates invadopodia biogenesis and extracellular matrix degradation and is up - regulated in prostate and breast cancer . 
daubon t , buccione r , genot e : the aarskog - scott syndrome protein fgd1 regulates podosome formation and extracellular matrix remodeling in transforming growth factor b - stimulated aortic endothelial cells . 
egorov mv , capestrano m , vorontsova oa , et al : faciogenital dysplasia protein ( fgd1 ) regulates export of cargo proteins from the golgi complex via cdc42 activation . 
laetsch author affiliations and support information ( if applicable ) appear at the end of this article . creative commons attribution non commercial no derivatives 4.0 license clinical trial information : nct02637687 . corresponding author : theodore w . 
in normal development , these genes regulate the growth , differentiation , and survival of neurons.14 , 15 gene fusions that involve one of these genes ( trk fusions ) have been described in a range of pediatric and adult cancers.16 - 25 in these fusions , the 3 region of the ntrk gene , which includes the kinase domain , is joined downstream of the promoter and 5 region of an unrelated gene . 
most reported fusions in extra cranial solid tumors to date have involved either ntrk1 or ntrk3 , with ntrk2 fusions more common in primary cns tumors.26 larotrectinib is the first highly selective inhibitor of all three trk kinases to enter clinical development . 
after two cycles of chemotherapy , disease progression continued , and an aortic pseudo aneurysm developed within the mass , which led to displacement of the inferior vena cava and ureteral impingement ( fig 1b )  . 
 ( e ) after 14 months of larotrectinib treatment . the patient was subsequently referred to our institution , where surgical intervention to debulk the tumor and repair the pseudo - aneurysm was offered . 
histologically , the tumor consisted of sheets of epithelioid cells with large eccentrically placed nucleus , occasional nucleoli , and abundant eosinophilic cytoplasm , mimicking rhabdoid cells ( fig 3 )  . 
immunohistochemically , the cells showed retained ini - 1 nuclear positivity and scattered cells positive for s - 100 protein and cd34 . postoperatively , gross residual tumor remained in the vertebral bodies . 
next generation sequencing ( ngs ) of her tumor was performed using foundationoneheme ( foundation medicine , cambridge , ma ) , a combined dna and rna sequencing hybrid capture - based assay that has been validated for clinical use without requirement for an orthogonal confirmatory assay.28 sequencing revealed a novel strn - ntrk2 fusion in which the kinase domain of ntrk2 is joined in frame to strn ( figs 3e and 3f )  . 
copy number loss of cdkn2b also was identified . two months after surgery , after informed consent , the patient was enrolled in the pediatric phase i trial of larotrectinib.29 she was treated with dose level 1 ( 100 - mg adult equivalent dose by simcyp modeling [ simcyp , sheffield , uk ] ) and received larotrectinib 75 mg twice a day continuously on the basis of her age and body surface area . 
pharmacokinetic assessment after the first dose of larotrectinib revealed an estimated 24 - hour area under the plasma concentration time curve ( auc0 - 24 ) of 2 , 980 ng h / ml , which was less than the protocol - specified threshold of 3 , 500 ng h / ml that would allow intrapatient dose escalation . 
pharmacokinetics at this dose demonstrated an estimated auc0 - 24 of 3 , 830 ng h / ml . at the time of initiation of larotrectinib , the patients lansky play - performance score ( lps ) was 60 . 
by 14 days after initiation of larotrectinib , the patient was noticeably less fatigued ( lps of 70 ) , the ascites had resolved by physical examination , and her back pain had resolved ( fig 4 )  . 
 ( d ) excised tumor specimen , including the aortic bifurcation . ureter position of vertebral bodies 2 , demonstrated resolution of pet avidity of all tumors , resolution of ascites , and significant reduction in the size of the residual pulmonary metastases and retroperitoneal tumors consistent with a partial response by response evaluation criteria in solid tumors ( recist ) version 1.1 ( figs 1d and 1e )  . 
five months after starting larotrectinib , the patient underwent uncomplicated closure of her colostomy and removal of her denver shunt . despite heavy pretreatment , the patient has tolerated larotrectinib well , with the only drug related adverse events consisting of mild ( common terminology criteria for adverse events [ version 4 ] grade 1 ) fatigue and intermittent grade 1 to 2 cytopenias . 
her response continues to deepen with complete resolution of her pulmonary metastasis and only residual pet - negative tissue at the site of tumor invasion of the vertebral bodies after 22 months of larotrectinib therapy as of february 2018 . 
 currently , the patients lps is 90 , and she has returned to school . discussion we describe a patient in whom tumor sequencing led to the identification of a novel ntrk2 fusion in a chemotherapy - refractory , metastatic , unresectable , undifferentiated sarcoma and successful treatment with larotrectinib . 
the identification of an ntrk2 fusion is consistent with other reports of oncogenic fusions in this histology.13 , 30 - 39 a wide range of tumors that harbor trk fusions has been reported to respond to larotrectinib.27 the activity of larotrectinib is striking in children , with a 93% confirmed objective response rate and all patients with trk fusions experiencing tumor regression.29 this patients tumor harbored a fusion of ntrk2 , and she was the sole patient in the initial 55 - patient data set to have a fusion of this gene.27 other rare ntrk2 fusions have been described in gliomas , specifically with vcl , agbl4 , qki , and nacc2 , 20 , 40 but to our knowledge , this report is the first of an ntrk2 fusion in a pediatric extracranial solid tumor . 
 ( b ) hematoxylin and eosin stain that shows epithelioid / rhabdoid cells with eccentric , pleomorphic nuclei ; occasional nucleoli and abundant eosinophilic cytoplasm ; and a single mitosis . 
 ( f ) rna sequencing reads that support the strn - ntrk2 fusion . ntrk3 suggests that these sarcomas should be evaluated for fusions of all three ntrk genes.41 strn on chromosome 2p22.2 encodes striatin , a ubiquitously expressed calmodulin - binding protein thyroid cancer , it is a common 5 fusion partner for alk also located on 2p.42 however , strn has not previously been reported as an ntrk fusion partner , which is consistent with the broad diversity of 5 fusion partners seen in trk fusion - positive cancers27 and is an important consideration when designing testing strategies for trk fusions . 
tests such as reverse transcriptase polymerase chain reaction only detect known fusion partners and are likely to miss tumors with uncommon or unique ntrk fusion genes , which can respond to trk inhibition . 
testing that uses hybrid capturebased ngs has the potential to detect a diversity of ntrk fusion partners , but careful attention must be paid to the initial substrate ( dna v rna ) , the target enrichment strategy ( hybrid capture v amplicon v anchored multiplex polymerase chain reaction ) , and the detailed probe design . the profound clinical response seen in this strn - ntrk2 fusion patient to larotrectinib establishes that the trk fusion is the key driver for this patients tumor . 
in the latter , despite high initial response rates , nearly all patients treated with vemurafenib or dabrafenib experience disease progression within 12 to 18 months of starting therapy.43 , 44 durable responses also have been observed in patients with fusions that involve ntrk1 and ntrk3 treated with larotrectinib.27 in conclusion , ngs of the undifferentiated sarcoma in our patient was critical in identifying a highly actionable kinase fusion ( strn - ntrk2 ) , which resulted in a profound and durable clinical response on matched treatment . 
laetsch manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors veena rajaram no relationship to disclose dean c . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center lee a . 
cox employment : bayer ag , loxo oncology , merck , amgen stock and other ownership interests : loxo oncology , bayer ag , merck , amgen patents , royalties , other intellectual property : us patent 62 / 318 , 041 issued to loxo oncology ( inst ) theodore w . 
laetsch , the university of texas southwestern medical center ; tara pavlock , alison patterson , anne post , caitlyn ambrose , veena rajaram , andrew martin , steve megison , and theodore w . 
ferrari a , sultan i , huang tt , et al : soft tissue sarcoma across the age spectrum : a populationbased study from the surveillance epidemiology and end results database . 
pappo as , devidas m , jenkins j , et al : phase ii trial of neoadjuvant vincristine , ifosfamide , and doxorubicin with granulocyte colony - stimulating factor support in children and adolescents with advanced - stage nonrhabdomyosarcomatous soft tissue sarcomas : a pediatric oncology group study . 
antonescu cr , suurmeijer aj , zhang l , et al : molecular characterization of inflammatory myofibroblastic tumors with frequent alk and ros1 gene fusions and rare novel ret rearrangement . 
simon mp , pedeutour f , sirvent n , et al : deregulation of the platelet - derived growth factor b - chain gene via fusion with collagen gene col1a1 in dermatofibrosarcoma protuberans and giant - cell fibroblastoma . 
moss yp , voss sd , lim ms , et al : targeting alk with crizotinib in pediatric anaplastic large cell lymphoma and inflammatory myofibroblastic tumor : a childrens oncology group study . 
laetsch tw , roy a , xu l , et al : undifferentiated sarcomas in children harbor clinically - relevant oncogenic fusions and gene copy - number alterations : a report from the childrens oncology group . 
bourgeois jm , knezevich sr , mathers ja , et al : molecular detection of the etv6 - ntrk3 gene fusion differentiates congenital fibrosarcoma from other childhood spindle cell tumors . 
knezevich sr , garnett mj , pysher tj , et al : etv6 - ntrk3 gene fusions and trisomy 11 establish a histogenetic link between mesoblastic nephroma and congenital fibrosarcoma . 
el demellawy d , cundiff ca , nasr a , et al : congenital mesoblastic nephroma : a study of 19 cases using immunohistochemistry and etv6 - ntrk3 fusion gene rearrangement . 
laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
italiano a , sung ys , zhang l , et al : high prevalence of cic fusion with double - homeobox ( dux4 ) transcription factors in ewsr1 - negative undifferentiated small blue round cell sarcomas . 
yamada y , kuda m , kohashi k , et al : histological and immunohistochemical characteristics of undifferentiated small round cell sarcomas associated with cic - dux4 and bcor - ccnb3 fusion genes . 
li ws , liao ic , wen mc , et al : bcor - ccnb3 - positive soft tissue sarcoma with round - cell and spindle - cell histology : a series of four cases highlighting the pitfall of mimicking poorly differentiated synovial sarcoma . 
omeara e , stack d , phelan s , et al : identification of an mll4 - gps2 fusion as an oncogenic driver of undifferentiated spindle cell sarcoma in a child . 
kao yc , sung ys , zhang l , et al : recurrent bcor internal tandem duplication and ywhaenutm2b fusions in soft tissue undifferentiated round cell sarcoma of infancy : overlapping genetic features with clear cell sarcoma of kidney . 
sugita s , arai y , aoyama t , et al : nutm2a - cic fusion small round cell sarcoma : a genetically distinct variant of cic - rearranged sarcoma . 
kelly lm , barila g , liu p , et al : identification of the transforming strn - alk fusion as a potential therapeutic target in the aggressive forms of thyroid cancer . 
hauschild a , grob jj , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
 evaluation of commercial circulating tumor dna test in metastatic prostate cancer sinja taavitsainen , msc1 , 2 ; matti annala , msc1 , 2 ; elisa ledet , phd3 ; kevin beja , msc1 ; patrick j . 
each sample was analyzed using guardant360 and a research panel encompassing 73 prostate cancer genes . concordance of somatic mutation and copy number calls was evaluated between the two approaches . results targeted sequencing independently conrmed 94% of somatic mutations identied by guardant360 at an allele fraction greater than 1% . 
the research approach detected several clinically relevant dna repair gene alterations not reported by guardant360 , including four germline truncating brca2 / atm mutations , two somatic atm stop gain mutations , one brca2 biallelic deletion , 11 brca2 stop gain reversal mutations in a patient treated with olaparib , and a hypermutator phenotype in a patient sample with 42 mutations per megabase . conclusion guardant360 accurately identies somatic ctdna mutations in patients with metastatic prostate cancer , but low allele frequency mutations should be interpreted with caution . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction molecular stratication is poised to guide treatment of metastatic prostate cancer ( mpc ) , but tissue biopsies are difcult to acquire , because many patients lack soft tissue metastases . 
fortunately , circulating tumor dna ( ctdna ) can be detected in peripheral blood cellfree dna ( cfdna ) from most patients with progressive disease.1 - 4 numerous research , industry , and commercial cfdna sequencing assays have arisen , each aiming to provide a practical alternative to metastatic tissue biopsy for tumor molecular stratication . unlike many other solid cancers , where ctdna assays can rely on detection of recurrent clinically relevant mutations , 5 mpc is characterized by a low mutation rate and high prevalence of large structural rearrangements , including deletions and translocations.6 furthermore , up to 30% of patients with mpc harbor deleterious germline and / or somatic defects in dna damage repair genes , such as brca2.7 the clinical laboratory improvement amendments certied guardant360 ctdna test ( guardant health , redwood city , ca ) identies single - nucleotide variants ( snvs ) in 73 genes , insertions / deletions ( indels ) in 23 genes , copy number amplications ( cnas ) in 18 genes , and gene fusions in six genes . 
 taavitsainen et al context key objective to evaluate a commercial circulating tumor ( ctdna ) test by comparing it against a prostate cancerspecic research panel in matched same - day plasma samples from men with metastatic prostate cancer . knowledge generated high concordance between the approaches was observed for ar gene copy number calls and somatic mutations at an allele fraction greater than 1% . 
the commercial test did not report several clinically actionable dna repair defects , including brca2 somatic homozygous deletions , structural rearrangements , and germline truncating mutations . relevance our results suggest that clinicians should use caution when interpreting commercial ctdna test results , particularly in the context of low allele fraction mutations . 
test utility in prostate cancer is limited by the lack of reporting on germline mutations , somatic deletions , and structural variants . specimens to guardant360 ctdna testing and foundationone ( foundation medicine , cambridge , ma ) tumor tissue testing and also found high discordance , particularly for mutations reported at allele frequencies lower than 1% . 10 together , these results raise signicant concerns about the accuracy of ctdna testing in precision oncology and are consistent with recent consensus statements on insufcient evidence of clinical validity for ctdna assays in advanced cancer11 and lack of support for routine ctdna testing in mpc.12 given the increasing use of commercial ctdna testing , we sought to assess the strengths and limitations of guardant360 in mpc . 
raw guardant360 sequencing data were not available for bioinformatic analysis , and there was no research agreement with guardant health . matched same - day samples from the 24 patients with mpc sent for guardant360 testing were subjected to targeted cfdna and wbc sequencing using a previously published academic approach ( the vancouver panel ) .2 , 13 targeted cfdna and wbc sequencing and data analysis were performed and nalized before examination of guardant360 reports . 
approval for this study was granted by the tulane university institutional review board ( certicate m0600 ) and the university of british columbia clinical research ethics board ( certicate h18 - 00944 )  . 
the af was required to be at least 20 times higher than the average af across all wbc samples and at least three times higher than the af in the paired wbc sample . 
 evaluation of commercial ctdna test in metastatic prostate cancer and the average distance of the mutant allele from the nearest read end was required to be at least 15 bases . 
our mutation analysis pipeline was previously validated in matched tissue - cfdna cohorts13 , 18 and in dilution series experiments.2 protein - level consequences of variants were predicted using annovar.19 ctdna fractions were estimated based on somatic mutation afs as previously described.2 mutations were considered subclonal if their af was less than 0.25 times the ctdna fraction ( for autosomes ) or less than 0.5 times the ctdna fraction ( for chromosome x )  . 
this conservative threshold was determined by halving the expected af for truncal mutations . two tp53 missense mutations in the cohort had an af greater than 1% in cfdna and a similar af in the matched wbc sample . 
one of these mutations ( a tp53 p.r273h missense mutation in patient 5 ) was reported by guardant360 and is included in figures 1a and 1b and the data supplement . analysis of deleterious germline variants germline variants were called in wbc samples by searching for variants with an alternate af of at least 15% and at least eight supporting reads . 
gc fraction was calculated for all target regions , and a scatter plot was created for each sample showing target regions as dots , with coverage log ratio relative to golden reference on the y - axis and gc fraction on the x - axis . 
these conservative thresholds were determined empirically by studying a plot of coverage log ratios and heterozygous snp afs in samples with and without detectable ctdna . categorization of putative pc driver alterations the following somatic mutations detected in the cohort were considered putative pc drivers : tp53 missense and truncating mutations ; ar missense mutations in amino acids 702 , 742 , 875 , 878 , and 893 ; akt1 p.e17k missense mutations ; apc truncating mutations ; braf missense mutations in amino acids 600 and 601 ; pten missense mutations in amino acid 35 ; pik3ca missense mutations in amino acids 378 , 391 , and 1047 ; atm truncating mutations ; ctnnb1 missense mutations in amino acids 32 to 45 ; and rb1 truncating mutations and missense mutations in amino acid 661 . 
putative driver mutations were determined from review of recently published large castration - resistant mpc sequencing studies.6 , 20 , 21 analysis of serial blood collections in addition to the matched 24 same - day samples subjected to guardant360 testing and vancouver panel sequencing , guardant360 reports were available for an additional 86 blood collections from the same patients collected between august 2015 and july 2018 . 
note that throughout the course of the study time period , three versions of the guardant360 assay ( 68 - , 70 - , and 73 - gene panels ) were used , with expanding coverage of genes and alterations . 
all somatic mutations identied as discordant in this study were conrmed to have been tested with the guardant360 73 - gene panel . results concordance of somatic mutation calls our objective was to compare the guardant360 test against a pc - specic ctdna research assay ( vancouver panel ) that identies snvs , indels , amplications , deletions , and rearrangements in the exonic regions of 73 mpc - relevant genes ( data supplement ) .2 , 13 , 22 between september 2016 and april 2018 , we sent plasma from 24 patients with clinically progressive mpc for guardant360 testing and performed targeted sequencing on matched same - day samples using the vancouver panel ( median depth , 1 , 435 ; data deposited to european genome - phenome archive under accession egas00001003352 ; data supplement )  . 
across the remaining 20 patients , ctdna fractions estimated by the vancouver panel ranged between undetectable ( , 2% ) and 80% ( median , 23% ; data supplement )  . focusing on 26 genes covered by both approaches , 30 ( 94% ) of 32 somatic mutations identied by guardant360 with an af greater than 1% were independently conrmed by the vancouver panel ( figs 1a and 1b ; data supplement )  . 
 a subclonal 1 - 100 known prostate cancer driver not a known prostate cancer driver not called in mutation analysis known prostate cancer driver not a known prostate cancer driver not called in mutation analysis * * * * * * taavitsainen et al not reported by guardant360 ; allele fraction is unknown * * * * * * * atm q2414x stop gain tp53 r273h missense ( clonal hematopoiesis ) atm q2593x stop gain subclonal highest allele percentage at other time points cg > tg substitution other base substitution insertion / deletion 1 2 5 6 7 8 9 10 11 12 13 15 16 17 patient fig 1 . 
it is plausible that some mutations labeled as subclonal had a nonprostate orig ( c ) plot showing all mutations ( dots ) identied by guardant360 in the cell - free dna ( cfdna ) time points that were also analyzed with the vancouver panel , grouped by allele fraction . 
patient 6 displays a hypermutation signature enriched for somatic cg.tg transitions and insertions / deletions , consistent with an underlying mismatch repair defect . supporting reads for 24 ( 86% ) of these mutations in cfdna , but nine of the mutations were found at a similar af in matched wbcs ( which are not analyzed by guardant360 ; figs 1a and 1b )  . 
furthermore , 82% of mutations with an af lower than 1% were found to be subclonal ( figs 1a and 1b ; criteria described in patients and methods )  . 
to explore further , we examined serial guardant360 test results from the same patients and found that 96% of mutations detected at an af lower than 1% did not reach an af greater than 2% at any time point ( fig 1c ) and did not track with overall ctdna fraction ( data supplement )  . 
these data suggest that many low af mutations identied by guardant360 represent subclonal passenger events or rare somatic clones of nonprostate origin . guardant360 did not report seven of 39 somatic mutations identied by the vancouver panel at allele fractions between 6% and 14% ( median , 10% ; data supplement )  . 
 evaluation of commercial ctdna test in metastatic prostate cancer vancouver panel also detected a high somatic mutation burden ( 42 mutations per mb ) in patient 6 ( fig 1d ) , accompanied by msh2 and msh6 monoallelic losses . guardant360 does not report silent mutations or total mutation burden . 
this patient had a complete remission ( 9 months at last follow - up ) after pembrolizumab treatment . sensitivity toward somatic changes in ar the ar gene is altered in most treatment - resistant mpcs , and ar status is associated with therapy response.1 , 2 , 6 , 23 in this cohort , ar amplications were identied in 11 of 24 patients , with perfect concordance between assays . 
somatic hotspot mutations in the androgen receptor ( ar ) ligand - binding domain were also highly concordant , except for three ar mutations detected by guardant at an af lower than 0.5% ( fig 2a )  . 
these mutations had supporting reads in our assay and were likely subclonal based on the presence of other mutations at higher afs ( data supplement )  . guardant360 does not report structural variants within the ar gene . 
we identied two patients with ar ligand - binding domain rearrangements predicted to yield a constitutively active ar protein ( fig 2b ) .24 identication of actionable dna repair gene alterations deleterious alterations in homologous recombination repair genes are associated with response to poly ( adp - ribose ) polymerase ( parp ) inhibitors and platinum - based chemotherapy.7 , 25 the vancouver panel identied six patients with homologous recombination repair defects : four patients with a germline brca2 or atm truncating mutation ( independently veried by commercial germline testing ) , two patients with somatic atm stop gain mutations , and one patient with a somatic brca2 biallelic deletion ( figs 3a and 3b )  . 
 ( a ) bar plot showing allele fractions of somatic ar hotspot mutations detected by the two assays . ar amplication status is indicated by blue and red tiles in the middle . 
 ( c ) eleven brca2 stop gain reversing somatic alterations detected with the vancouver panel in cfdna from patient 17 after treatment with poly ( adp - ribose ) polymerase inhibitor olaparib . 
all deletions overlapping the stop gain mutation are multiple of 3 bp in length and therefore remove the stop gain mutation while avoiding frameshistop gainreversing base substitutions are shown in the embedded table . patient 17 was sampled after olaparib resistance in march 2018 , and his cfdna revealed 11 cancer cell populations with somatic deletions or mutations reversing the germline brca2 stop gain ( fig 3c ) .26 these alterations were not reported by guardant360 , likely because it only reports short indels . concordance of gene amplication calls amplication of chromosome 7 genes met , braf , and cdk6 is rare in mpc , although low - level gain of chromosome 7 is common.6 , 21 met , braf , and / or cdk6 was reported amplied by guardant360 in 13 patients . 
guardant360 additionally reported 12 amplications in pik3ca , ccnd1 , and myc , nine of which showed evidence consistent with single copy gaonly 11 of 40 reported non - ar amplications displayed evidence for more than a single copy gain ( fig 4b )  . 
guardant360 also reported 11 amplications in genes egfr , pdgfra , kit , and fgfr1 , which are rarely altered in tissue - based mpc studies6 and are not assessed by the vancouver panel . guardant360 does not search for alterations in mpc genes spop , cdk12 , pik3r1 , foxa1 , msh2 , msh6 , tmprss2 , and erg and does not report large somatic deletions or complex structural variants in any genes . in total , we identied potentially clinically relevant alterations that were not reported by guardant360 in 12 of 24 patients , including a tp53 inactivating rearrangement , a cdkn1b biallelic deletion , intragenic ar rearrangements in two patients , three spop mutations , and dna repair defects in seven patients ( data supplement )  . discussion the guardant360 commercial ctdna assay has improved access to genomic testing across academic and nonacademic practitioners , especially in settings where tissue biopsy is not feasible . 
as with any narrow pan - cancer assay , there are compromises for individual cancer types . overall , we found excellent concordance between guardant360 and the vancouver pc panel for high af somatic mutations . 
copy numbers were estimated based on sequencing coverage log ratio and circulating tumor ( ctdna ) fraction ( described in patients and methods ) and represent the average gene copy numbers in ctdna - shedding cancer cells . 
 ( b ) sequencing coverage log ratios of genes met , braf , cdk6 , pik3ca , myc , ccnd1 , and ar , quantied with the vancouver panel in all 24 cfdna samples . 
numbers above bars indicate the average gene copy numbers in ctdna - shedding cancer cells that would produce the observed coverage log ratio in the vancouver panel data , correcting for presence of normal cfdna ( patients and methods )  . 
first , a vast majority of these mutations were subclonal and therefore potentially poor biomarkers for therapies aiming at broad antitumor effect , although they may still be of relevance for detecting emerging resistant clones . 
 taavitsainen et al somatic alterations falsely attributed to pc - derived ctdna if the wbc fraction were not analyzed.3 because guardant360 only analyzes cfdna , the test cannot reject somatic cfdna mutations that are simultaneously detected in the blood lineage . 
consistent with these three points , a vast majority of low af mutations did not track with overall ctdna fraction and never rose to a signicant clonal fraction in longitudinal sampling . 
finally , earlier studies comparing commercial ctdna assays found large discordances in reported low af somatic mutations.10 together , these results suggest that guardant360 should consider differential reporting of low af mutations , especially for mpc . somatic changes to the ar gene , including mutations , amplications , and rearrangements resulting in constitutive activation , are primary drivers of resistance to systemic therapies targeting the androgen axis in pc24 and are under development as predictive cfdna biomarkers.2 , 29 , 30 we found near - perfect concordance between guardant360 and the vancouver panel for ar amplications and hotspot mutations , with the only limitation being that guardant360 does not currently report intragenic ar rearrangements . the vancouver panel identied two patients with a potentially ligand - independent ar in this cohort . guardant360 does not report germline alterations , somatic copy number deletions , or large structural variants in the dna damage repair genes included in its panel . 
in mpc , these classes of variants are common , especially across brca2 , and can have both prognostic and predictive implications.31 of particular relevance , biallelic brca2 defects can sensitize to parp inhibitors , whereas deletions overlapping the site of a pre - existing mutation ( ie , so - called reversion mutations ) can drive parp inhibitor resistance . 26 , 32 one quarter of the patients proled here had biologically and clinically relevant dna damage repair gene alterations identied via sequencing with the vancouver panel . 
because nongenomic specialists may not be aware of the limits of commercial assays , we caution that negative results from guardant360 should be interpreted critically ; absence of reported somatic mutation in a gene does not preclude other types of alterations ( eg , somatic biallelic brca2 deletion , rearrangement , or germline truncating mutation )  . in conclusion , we show that guardant360 and targeted ctdna sequencing with a research assay ( ie , the vancouver panel ) are highly concordant for high af mutations in mpc . however , the guardant360 test has potential limitations in its reporting of indels , rearrangements , and germline variants . 
in the future , optimal ctdna commercial assays for mpc should identify and report on all types of including deletions and rearrangesomatic alterations , include mpc - specic genes , such as foxa1 , ments ; spop , and erg ; and identify deleterious germline alterations . 
limitations of this study include the absence of matched tissue to adjudicate discordances and the lack of a standardized cohort to draw clinical outcome correlates . affiliations 1university of british columbia , vancouver , british columbia , canada 2tampere university , tampere , finland 3tulane university , new orleans , la 4british columbia cancer agency , vancouver , british columbia , canada data analysis and interpretation : sinja taavitsainen , matti annala , matti nykter , oliver sartor , alexander w . 
 evaluation of commercial ctdna test in metastatic prostate cancer research funding : bayer healthcare pharmaceuticals ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , endocyte ( inst ) , innocrin pharma ( inst ) , merck ( inst ) , invitae ( inst ) , constellation pharmaceuticals ( inst ) , advanced accelerator applications ( inst ) expert testimony : sano travel , accommodations , expenses : bayer healthcare pharmaceuticals , johnson & johnson , sano , astrazeneca , progenics alexander w . 
wyatt consulting or advisory role : genzyme speakers bureau : janssen research funding : janssen no other potential conicts of interest were reported . acknowledgment we acknowledge the csc - it center for science , espoo , finland , for providing computational resources . references romanel a , gasi tandefelt d , conteduca v , et al : plasma ar and abiraterone - resistant prostate cancer . 
sci transl med 7 : 312re10 , 2015 annala m , vandekerkhove g , khalaf d , et al : circulating tumor dna genomics correlate with resistance to abiraterone and enzalutamide in prostate cancer . cancer discov 8 : 444 - 457 , 2018 3 . 
hovelson dh , liu c - j , wang y , et al : rapid , ultra low coverage copy number proling of cell - free dna as a precision oncology screening strategy . 
genome med 10 : 85 , 2018 8 : 89848 - 89866 , 2017 corcoran rb , chabner ba : application of cell - free dna analysis to cancer treatment . 
n engl j med 379 : 1754 - 1765 , 2018 quigley da , dang hx , zhao sg , et al : genomic hallmarks and structural variation in metastatic prostate cancer [ erratum : cell 175 : 889 , 2018 ]  . 
eur urol 71 : 417 - 425 , 2017 zill oa , banks kc , fairclough sr , et al : the landscape of actionable genomic alterations in cell - free circulating tumor dna from 21 , 807 advanced cancer patients . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
scher hi , graf rp , schreiber na , et al : assessment of the validity of nuclear - localized androgen receptor splice variant 7 in circulating tumor cells as a predictive biomarker for castration - resistant prostate cancer . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
cancer discov 7 : 999 - 1005 , 2017 jaiswal s , fontanillas p , flannick j , et al : age - related clonal hematopoiesis associated with adverse outcomes . 
conteduca v , wetterskog d , sharabiani mta , et al : androgen receptor gene status in plasma dna associates with worse outcome on enzalutamide or abiraterone for castration - resistant prostate cancer : a multi - institution correlative biomarker study . 
a study of patients with myeloid malignancy compared the response rate of trametinib among patients with ras wild - type ( n = 30 ) and ras - mutated mds or aml ( n = 50 )  . 
five patients with ras - mutated mds or aml achieved a complete response ( cr ) or cr with incomplete platelet recovery compared with no patients with ras wild - type mds or aml.5 herein , we describe a patient with relapsed mds after undergoing allogeneic stem - cell transplant ( allo - sct ) who had next - generation sequencing ( ngs ) identifying map2k2 p298l , for which the patient received trametinib plus decitabine and achieved a durable cr . 
the map2k2 p298l mutation has been identified previously in a patient with lung cancer , but the functional significance at the protein level has not yet been elucidated.6 the patient is a 52 - year - old asian woman with a 12 - year history of jak2 - negative essential thrombocythemia ( et ) treated with anagrelide ( 10 years ) and hydroxyurea ( 2 years )  . 
time points indicate number of months after transplantation each next - generation sequencing panel was obtained . dnmt3a tet2 calr map2k runx1 mutations , notably runx1 s141 * ( mutation allele frequency [ maf ] , 12% ) , zmym3 g49wfs * 13 ( maf , 27% ) , calr k368rfs * 51 ( maf , 39% ) , and map2k2 p298l ( maf , 30% )  . 
after a 1 - month treatment interruption , the mucositis resolved and treatment resumed with decitabine 20 mg / m2 intravenously on days 1 through 3 of a 28 - day cycle and trametinib 2 mg daily for 21 days of a 28 - day cycle . 
after resolution , treatment with decitabine 20 mg / m2 intravenously on days 1 through 5 of a 28 - day cycle and trametinib 0.5 mg daily for 7 days of a 14 - day cycle continued without additional issues . 
instead , a benign pdgfrb t88i ( maf , 47% ) alteration and tet2 h1380y ( maf , 5% ) and dnmt3a r882s ( maf , 15% ) mutations were identified ( fig 1 ; data supplement )  . subsequently , a donor pb sample was analyzed by a clinical laboratory improvement amendments - certified moffitt 54 - genetargeted myeloid ngs panel8 with an average coverage of 11 , 987 reads . 
a benign asxl1 g652s variant was detected in the patient and the related donor ( maf , 49% ) , likely reflecting a heterozygous germline variant detected in both persons as a result of shared inheritance . 
 this acquired mutation in the patient suggests donor - derived acquisition of a chip mutation . at the time of this report , the patient was without gvhd symptoms , received a donor lymphocyte infusion ( dli ) 16 months after trametinib initiation , and remains in cr 18.5 months after trametinib initiation ( 29.5 months after allo - sct )  . 
 the primary oncologist felt that a dli may achieve the best long - term outcomes because there are no long - term efficacy data of trametinib plus a hypomethylating agent ( hma ) in relapsed mds after allo - sct . 
the patient continues to receive treatment with trametinib and decitabine without evidence of dysplasia or relapse . discussion protein function in the presence of map2k2 p298l has not been previously characterized to our knowledge . 
this map2k2 alteration is located in a proline - rich segment of the protein kinase domain , is near a map2k2 phosphorylation site , and has been observed previously in cancer.6 additionally , per the catalog of somatic mutations in cancer , the map2k2 p298l alteration had been identified as somatic and pathogenic per their prediction tool.11 despite not knowing the functional significance of the alteration , a clinical response was observed after the administration of trametinib and decitabine . 
 the 2 - year os was 12.4% and in those achieving a cr after azacitidine administration , the 2 - year os was 48.4%.12 therefore , it is difficult to determine to what degree , if any , the clinical benefit observed could be attributed to trametinib , because hmas with or without dli have demonstrated clinical efficacy in patients with relapsed mds after sct transplant . adverse effects and their management with trametinib plus decitabine has not been previously discussed to our knowledge . 
based on phase ii data , trametinib was not believed to result in the infectious complications experienced in our case.4 trametinib and decitabine were held to evaluate the etiology of the adverse effects of dermatitis and mucositis , for which a biopsy specimen demonstrated gvhd . 
kevin hicks no relationship to disclose lia perez no relationship to disclose eric padron honoraria : incyte , cell therapeutics , cell therapeutics ( inst ) research funding : incyte ( inst ) rami s . 
kim kb , kefford r , pavlick ac , et al : phase ii study of the mek1 / mek2 inhibitor trametinib in patients with metastatic braf - mutant cutaneous melanoma previously treated with or without a braf inhibitor . 
borthakur g , popplewell l , boyiadzis m , et al : activity of the oral mitogen - activated protein kinase kinase inhibitor trametinib in ras - mutant relapsed or refractory myeloid malignancies . 
hung , md , phd1 ; dora dias - santagata , phd1 ; maristela onozato , md1 ; nikunj shah , bs2 ; eric severson , md2 ; daniel duncan , md2 ; brendan j . 
we characterized molecular and clinicopathologic features of the pertinent fusion - positive patient cases . results we identied 11 patients with thymomas harboring a gene fusion of kmt2a and mastermind - like transcriptional coactivator 2 ( maml2 )  . 
the frequency of kmt2a - maml2 fusion was 4% of all thymomas ( 10 of 242 ) and 6% of thymomas of b2 or b3 histology ( 10 of 169 )  . conclusion kmt2a - maml2 represents the rst recurrent fusion described in type b thymoma . 
the identication of this fusion offers insights into the biology of thymoma and may have clinical relevance for patients with disease refractory to conventional therapeutic modalities . jco precis oncol 4 : 109 - 115 . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction thymoma , a neoplasm that arises from or exhibits thymic epithelial differentiation , is the most common tumor of the adult thymus.1 thymoma has a strong association with autoimmune diseases , particularly myasthenia gravis , which typically resolve upon successful tumor resection . 
we aim to identify recurrent genetic alterations present in this tumor . knowledge generated a subset of type b2 and b3 thymomas harbor recurrent gene fusions between lysine methyltransferase 2a ( kmt2a ) and mastermind - like transcriptional coactivator 2 ( maml2 )  . 
aside from rare case reports of hematologic neoplasms in the literature , the kmt2a - maml2 rearrangement seems specic to type b2 and b3 thymomas among human tumors . relevance the nding of recurrent kmt2a - maml2 fusion provides insights into tumor biology and potential therapeutic targets in type b2 and b3 thymomas , which are clinically aggressive with limited curative options . solid fusion assay analysis ( mgh solid fusion assay ; mgh , boston , ma ; data supplement provides list of gene targets ) and single - nucleotide variant and insertion / deletion analysis ( snapshot dna - based assay ; thermo fisher scientic , waltham , ma ; data supplement provides list of gene targets ) .7 the solid fusion assay used rna - based fusiontargeted anchored multiplex polymerase chain reaction ( archerdx primers , boulder , co ) and illumina ( san diego , ca ) sequencing . 
in brief , 60 ng of dna was extracted from 255 , 008 cancer specimens , including 242 thymoma specimens , in 40 m of formalin - xed , parafn - embedded tissue blocks . 
the samples were assayed by cgp using adaptor ligation , and hybrid capture was performed for all coding exons from 287 ( version 1 ) to 315 ( version 2 ) cancer - related genes plus select introns from 19 ( version 1 ) to 28 ( version 2 ) genes frequently rearranged in cancer ( data supplement )  . 
gtf2i included on any list of cancer - related genes . was not various samples were similarly assayed but performed in dna on 406 genes and selected introns of 31 genes involved in rearrangements ( data supplement ) and in rna on 265 genes commonly rearranged in cancer . 
sequences were analyzed for all classes of genomic alterations , including short variant alterations ( base substitutions , insertions , and deletions ) , copy - number alterations ( focal amplications and homozygous deletions ) , and select gene fusions or rearrangements by methods previously described.8 - 10 thymomas harboring a kmt2a - maml2 the cohort of fusion comprised 10 patient cases assayed with cgp ( foundation medicine ) during clinical care at other institutions . 
seven years later , the patient developed recurrent thymoma , with direct invasion of the lung , pericardium , and distal left main pulmonary artery , as well as metastasis to paratracheal lymph nodes ( fig 1a )  . the patient received induction chemotherapy and underwent surgical resection ( radical thymectomy , radical pericardiectomy , and left pneumonectomy ) , followed by paratracheal lymph node excision and radiotherapy . 
 ( a ) computed tomography of the chest from the patients rst recurrence demonstrates a 7.8 - cm anterior mediastinal mass ( arrow ) in contact with the pericardium , aorta , and portions of the main and left pulmonary arteries . 
 ( b ) histopathologic examination of the tumor shows sheets of large epithelioid cells lacking signicant lymphocytic inltration , consistent with type b3 thymoma ( hematoxylin and eosin stain ; magnication 400 )  . 
 ( d ) ihc for terminal deoxynucleotidyl lineage thymocytes associated with the tumor ( magnication 400 )  . transferase highlights scattered nuclei of t - cell recurrence of myasthenia gravis . 
the patient died as a result of complications of her thymoma 15 years after initial diagnosis . given the aggressive nature of this thymoma , molecular genetic assays were performed on the initial recurrence to lung , in an attempt to identify potentially targetable genetic alterations . 
this fusion assay result was reproduced on the patients subsequent paratracheal lymph node excision . kmt2a - maml2 fusion occurs in aggressive histologic subtypes of thymoma to determine the frequency of kmt2a - maml2 fusion in a cohort specically enriched in clinically more aggressive cases of thymoma , we reviewed a set of 242 patient cases of thymoma from the foundation medicine archives . 
the patient case was reviewed , and the original diagnosis was conrmed . the kmt2a - maml2 fusion was reamong thymomas , stricted to the most aggressive histologic thymoma subtypes , being present in 10 ( 5.9% ) of 169 thymomas that included b2 or b3 components , but 0 ( 0% ) of 64 of the remaining thymomas ( types a , ab , and b1 )  . 
no other known or likely pathogenic alterations were identied in 7 of 10 patient cases with a kmt2a - maml2 fusion , whereas a concurrent mutation in tp53 , arid1a , or sf3b1 was identied in 1 patient case each . 
of patients age at diagnosis , years final staging ( modied masaoka ) median range male female unknown histology b2 + b3 b3 + c 112 2020 by american society of clinical oncology discussion in the 243 patient cases of thymoma evaluated , we discovered a recurrent fusion of kmt2a and maml2 in 11 . this fusion seems to be highly specic to thymomas with aggressive histologic features , because all fusion - positive patient cases contained type b2 and / or b3 histology . 
the striking restriction of kmt2a - maml2 fusion to thymomas was underscored by the absence of the fusion in approximately 255 , 000 patient cases of diverse tumor types , including 366 thymic carcinomas , with the exception of a single patient case of plasmacytoma . kmt2a , rst described in 1991 , was initially termed mixedlineage leukemia - 1 because of its frequent appearance as a translocation partner in acute myeloid and lymphoid leukemias.12 the 36 - exon gene is located on chromosome 11q23 . 
the encoded protein binds dna and methylates histone h3 at lysine - 4 to regulate other genes , including several homeobox ( hox ) genes.13 kmt2a has been found to be a promiscuous translocation partner , with  . 
80 unique fusion partners identied.14 currently , there is no unifying theory on how kmt2a rearrangements lead to neoplasia.14 maml2 is a 5 - exon gene residing on chromosome 11q21 . 
maml2 and other maml family proteins are involved in notch pathwaymediated transcriptional activation.15 recurrent gene rearrangements involving maml2 have been described in mucoepidermoid carcinoma , in which fusion of the rst exon of the camp response element - binding proteinregulated transcription coactivator - 1 ( crtc1 ) with maml2 exons 2 to 5 leads to notch pathway disruption.16 the kmt2a - maml2 gene fusion results from inv ( 11 ) ( q21q23 ) , a cytogenetic abnormality rst reported in 1998 by obama et al17 in a patient with therapy - related acute myeloid leukemia . subsequent reports of the fusion are exceptionally rare and no . 
to our knowledge , only 8 patient cases have been reported , including 2 of acute myeloid leukemia , 2 of myelodysplastic syndrome , and 4 of acute lymphoblastic leukemia.17 - 22 reported fusion proteins in these patient cases involved regions similar to those identied in our cohort , with the exception of 2 patient cases reported by metlzer et al21 with maml2 breakpoints in introns 2 and 3 . prior functional studies of the kmt2a - maml2 construct have shown evidence of disrupted notch pathway signaling . 
in addition to describing the fusion in patient cases therapy - related myeloid neoplasms , nemoto et al19 the kmt2ademonstrated via luciferase assay that maml2 fusion suppresses promoter activation of the notch1 target gene hes1.19 gene expression proles from 2 patient cases of kmt2a - maml2positive t - cell acute lymphoblastic leukemia showed differential expression patterns relative to controls , suggesting activation of genes downstream of notch1.21 another study demonstrated oncogenic activity by kmt2a - maml2 fusion inserted into cell lines with sleeping - beauty vectors.23 the sum of these studies has demonstrated oncogenic function of kmt2a - maml2 fusion , likely via disruption of notch signaling . 
further study is warranted to examine the impact of this fusion on notch signaling . in patients with malignancies not amenable to traditional surgical or chemoradiotherapy protocols , targeted therapy offers an additional potential opportunity for disease control . 
early data suggest disease refractory to initial that maml2 fusionpositive mucoepidermoid carcinoma may respond to targeted therapeutics , including epidermal growth factor receptor inhibitors such as getinib.24 - 26 given the low tumor mutational burden seen in thymoma , identication of this small but genomically distinctive subset of kmt2a - maml2rearranged tumors may provide a therapeutic target in patients not responsive to traditional therapy . 
hasserjian , abner louissaint jr , erik a . williams manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors nikunj shah employment : foundation medicine eric severson employment : foundation medicine , partners healthcare stock and other ownership interests : foundation medicine daniel duncan employment : foundation medicine jeffrey s . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . dora dias - santagata consulting or advisory role : rarecyte ( i ) maristela onozato patents , royalties , other intellectual property : patent pending for multiplex fish assay , led on october 25 , 2019 ( no direct compensation related to this patent ) jo - anne vergilio employment : foundation medicine stock and other ownership interests : foundation medicine , roche valentina nardi consulting or advisory role : thermo fisher scientic ( i ) , cell signaling technology ( i ) robert p . 
hasserjian stock and other ownership interests : avanos medical , danaher , henry schein , hologic , idexx laboratories , johnson & johnson , kimberly clary , medtronic , stryker , cooper companies , thermo fisher scientic consulting or advisory role : jazz pharmaceuticals , promedior erik a . 
crit rev oncol hematol 99 : 332 - 350 , 2016 radovich m , pickering cr , felau i , et al : the integrated genomic landscape of thymic epithelial tumors . 
cancer cell 33 : 244 - 258.e10 , 2018 petrini i , meltzer ps , kim ik , et al : a specic missense mutation in gtf2i occurs at high frequency in thymic epithelial tumors . 
front oncol 4 : 103 , 2014 thomas a , rajan a , berman a , et al : sunitinib in patients with chemotherapy - refractory thymoma and thymic carcinoma : an open - label phase 2 trial . 
lancet oncol 16 : 177 - 186 , 2015 [ erratum : lancet oncol 16 : e105 , 2015 ] petrini i , rajan a , pham t , et al : whole genome and transcriptome sequencing of a b3 thymoma . 
nat med 20 : 1479 - 1484 , 2014 frampton gm , fichtenholtz a , otto ga , et al : development and validation of a clinical cancer genomic proling test based on massively parallel dna sequencing . 
ziemin - van der poel s , mccabe nr , gill hj , et al : identication of a gene , mll , that spans the breakpoint in 11q23 translocations associated with human leukemias . 
k ochert k , ullrich k , kreher s , et al : high - level expression of mastermind - like 2 contributes to aberrant activation of the notch signaling pathway in human lymphomas . 
tonon g , modi s , wu l , et al : t ( 11 ; 19 ) ( q21 ; p13 ) translocation in mucoepidermoid carcinoma creates a novel fusion product that disrupts a notch signaling pathway . 
obama k , furukawa y , tara m , et al : secondary monocytic leukemia with rearrangement of the mll gene occurring during the course of adult t - cell leukemia . int j hematol 68 : 323 - 326 , 1998 18 . 
mariani ra , silva m , caparelli e , et al : inv ( 11 ) ( q21q23 ) : kmt2a - maml2 , a recurrent genetic abnormality in t - cell therapy - related acute lymphoblastic leukemia . 
nemoto n , suzukawa k , shimizu s , et al : identication of a novel fusion gene mll - maml2 in secondary acute myelogenous leukemia and myelodysplastic syndrome with inv ( 11 ) ( q21q23 )  . 
tang g , lu x , wang sa , et al : homozygous inv ( 11 ) ( q21q23 ) and mll gene rearrangement in two patients with myeloid neoplasms . 
metzler m , staege ms , harder l , et al : inv ( 11 ) ( q21q23 ) fuses mll to the notch co - activator mastermind - like 2 in secondary t - cell acute lymphoblastic leukemia . 
chen z , chen j , gu y , et al : aberrantly activated areg - egfr signaling is required for the growth and survival of crtc1 - maml2 fusion - positive mucoe26 . 
li s , zhang z , tang h , et al : pathological complete response to getinib in a 10 - year - old boy with egfr - negative pulmonary mucoepidermoid carcinoma : a pidermoid carcinoma cells . 
bryce purpose genomic testing has increased the quantity of information available to oncologists . unfortunately , many identified sequence alterations are variants of unknown significance ( vuss ) , which thus limit the clinicians ability to use these findings to inform treatment . 
we applied a combination of in silico prediction and molecular modeling tools and laboratory techniques to rapidly define actionable vuss . materials and methods exome sequencing was conducted on 308 tumors from various origins . most single nucleotide alterations within gene coding regions were vuss . 
a subset of receptor tyrosine kinase vuss was characterized by laboratory comparison of each vus versus its wild - type counterpart in terms of expression and signaling activity . results the study identified 4 , 327 point mutations of which 3 , 833 were vuss . 
three vuss ( fgfr2 f276c , fgfr4 r78h , and kdr g539r ) showed increased basal or ligand - stimulated erk phosphorylation compared with their wild - type counterparts , which suggests that they support transformation . 
for example , braf v600e is well accepted as a therapeutic target in metastatic melanoma.7 however , a current challenge in genomic oncology care is the evaluation of the potential therapeutic significance of large numbers of uncharacterized , nonsynonymous sequence alterations referred to as variants of unknown significance ( vuss ) in potentially oncogenic proteins . when novel vuss are identified , the clinical team must try to draw conclusions about whether the variant is a driver mutation or has no significance for cancer pathogenesis . 
although some recurrent mutations within oncogenic proteins have been characterized as having an effect on protein function and thus , the promotion of transformation , novel vuss identified through clinical genomic testing often are lacking functional information . the definition of the therapeutic value of vuss is a current unmet need.8 we demonstrate how in silico analysis and experimental laboratory studies can rapidly determine the potential therapeutic value of a vus . 
by using bioinformatic analysis of exome sequencing results , a large number of potentially deleterious vuss that are therapeutically targetable were identified with a high frequency of occurrence in kinases . 
the mayo clinic irb approved the in vitro functional studies of somatic mutations identified in tumors of patients enrolled in the cim oncology service ( irb 15 - 003386 )  . 
redcap ( research electronic data capture ) hosted at the mayo clinic was used to collect and store clinical follow - up data.10 results vuss are the most common findings in tumor exome sequencing analysis targeted and exome sequencing were performed on heterogeneous solid ( 57% ) and hematologic ( 43% ) malignancies ( data supplement )  . 
vuss , which constitute mutations that are functionally uncharacterized or previously unreported in the cosmic ( catalogue of somatic mutations in cancer ) database , 11 comprised the majority ( 89% ) of the point mutations observed in this cohort ( fig 1a )  . 
obstacles to clinical use of these data resulted from large numbers of vuss identified in each patient , uncertainty whether identified vuss are potential drivers of transformation , and whether encoded proteins were therapeutically targetable . to begin to address these difficulties , vuss were filtered into a subgroup of 905 in genes that encode proteins therapeutically targetable by food and drug administrationapproved drugs or by investigational agents available through clinical trials . 
protein class analysis demonstrated that rtks and serine / threonine kinases represent the largest therapeutically targetable functional classes , with mutations in both hematologic and solid tumors ( fig 1b )  . these 905 therapeutically targetable vuss were then evaluated in silico , and those determined to be benign by two prediction tools were removed , which left 522 potentially deleterious , therapeutically targetable vuss in 226 patients ( data supplement ) or 12% of the total variants detected ( fig 1a )  . 
the distribution of protein classes represented in this deleterious , therapeutically targetable subgroup ( fig 1c ) was similar to that of the therapeutically targetable vus group ( fig 1b )  . 
 a significant findings , 11% targetable , deleterious , vuss , 12% other vuss , receptor tyrosine kinase serine / threonine kinase notch receptor dna endonuclease endocytosis nonreceptor tyrosine kinase tumor suppressor pi3k family ubiquitin ligase apoptotic regulator growth inhibition receptor tyrosine kinase serine / threonine kinase notch receptor endocytosis nonreceptor tyrosine kinase dna endonuclease pi3k family histone deacetylase tumor suppressor hormone receptor fgf receptor ubiquitin ligase growth inhibition hematologic solid no . 
 ( a ) frequency of significant findings and uncharacterized / unreported variants of unknown significance ( vuss ) in 4 , 327 point mutations reported in 308 patient tumors , including solid and hematologic malignancies . 
 ( b ) frequency of the most commonly observed protein classes in 905 therapeutically targetable vuss . with pymol software ( schrodinger , new york , ny ; data supplement ) , which predicted potentially altered function on the basis of their location within the proteins kinase domain ( data supplement )  . in silico and functional characterization of rtk vuss identified a subset of new targetable mutations ten rtk vuss from varied solid and hematologic malignancies ( data supplement ) and in reinterest were selected for gions of functional additional evaluation by in vitro testing . 
in addition , sequence alignment across species demonstrated that the wt residue that corresponded to each of the 10 vuss was completely conserved among diverse species , including mouse , rat , bovine , and human proteins . 
biochemical studies of r78h demonstrated no significant differences from wt fgfr4 in overall expression levels when expressed in kmch - 1 cholangiocarcinoma cells ( figs 2b and 2c )  . 
cellular localization of wt and r78h fgfr4 was also similar and exhibited mainly a plasma membrane distribution with intracellular labeling of probable golgi membranes ( fig 2e )  . however , r78h fgfr4 exhibited a small , but significantly elevated fgf2 - stimulated phosphoerk ( perk ) level compared with wt ( figs 2b and 2d )  . two kdr vuss , g55e and g539r , are located in the extracellular domain in proximity to amino acids that form disulfide bonds ( c53 and c530 ) ; thus , these amino acid substitutions may potentially affect neighboring disulfide bonds . 
 ( c ) frequency of the most commonly observed protein classes in 522 therapeutically targetable , potentially deleterious vuss . cells that expressed g55e kdr ( figs 3a and 3c )  . kdr variants and wt exhibited a similar punctate distribution by immunofluorescence ( fig 3d )  . vuss g251e , v484m , and t643m of pdgfra and variants v258l and v316m of pdgfrb were investigated . 
all variants fall in the extracellular domain of their respective receptor except t643m , which occurs within the pdgfrb kinase domav258l was predicted to be functionally benign but was of interest for in vitro study because of its ig3 location . 
pdgfr vuss were generally similar to their wt counterparts in terms of expression , distribution of polypeptide species on western blots , pdgf - stimulated perk levels , and cellular localization ( data supplement ) , except that pdgfra v484m was significantly lower in expression and pdgfstimulated perk levels than wt ( data supplement ) and pdgfrb v316m was significantly lower in expression than wt ( data supplement )  . f276c mutant is a new , constitutively active form of fgfr2 although predicted in silico to be benign , fgfr2 k41e , identified in an acute myeloid leukemia , was selected for additional study because of its location in the extracellular ig1 of fgfr2 and its unknown effect on ligand binding in nearby ig2 and ig3 ( data supplement )  . 
the fgfr2 f276c mutation identified here from a cholangiocarcinoma was also in a single cholangiocarcinoma in the cosmic database but has not been characterized.11 , 12 f276c is located in an extracellular , ig - like c2 - type 3 domain13 where ligand binding occurs.14 a different amino acid substitution at the same residue , f276v , has been reported in crouzon syndrome.15 modeling of wt and f276c fgfr2 showed that the extracellular receptor of fgfr2 contains an intrinsic disulfide bond between c278 and c342 in ig3 ( fig 4a , shown in gold )  . 
these data suggest that the f276c variant is functionally altered relative to the wt form . when fgfr2 proteins were expressed in kmch - 1 cells , immunofluorescence microscopy showed that the wt and k41e fgfr2 proteins were localized mainly to the cell surface and occurred on intracellular structures , likely endosomes and the golgi apparatus ( fig 4c )  . 
in contrast , the f276c variant exhibited an endoplasmic reticulumlike appearance and bright golgi - like intracellular structures in most cells , with only a minority of cells showing an obvious plasma membrane distribution ( fig 4c )  . 
each protein was expressed as an approximately 130 - kda polypeptide as detected by western blot ( fig 4d )  . however , the f276c variant was expressed at a higher level and the k41e variant at a lower level compared with wt ( fig 4d ) , although cells were transfected with equal amounts of dna for the different fgfr2 constructs . functional characteristics of fgfr2 proteins were assessed by studying perk signaling . 
because the f276c fgfr2 variant is expressed at higher levels than wt when equal amounts of dna were used , a lower ratio of f276c construct dna was used for transfection in the following experiments so that resulting levels of wt and f276c fgfr2 proteins were comparable ( figs 4e and 4f ) : kmch - 1 cells transfected with fgfr2 constructs were treated for 16 hours in serum - free media with fgf2 , lysed , and analyzed by western blot . 
the expression of wt or k41e fgfr2 in the absence of fgf2 increased perk levels beyond control levels , and treatment with fgf2 led to approximately fivefold increases in perk compared with control for both wt and k41e . 
however , expression of f276c fgfr2 significantly increased the perk level in the absence of fgf2 compared with wt fgfr2 , with little increase upon treatment with fgf2 ( figs 4e and 4g )  . 
in summary , f276c fgfr2 has high expression , altered cellular distribution , and increased constitutive activity compared with wt . finally , the sensitivity of wt and f276c fgfr2 activities to treatment with the fgfr inhibitor bgj398 were compared . 
at concentrations between 0 and 100 nm , erk phosphorylation was similarly partially inhibited by bgj398 in cells that expressed wt or f276c , and both fgfr2 forms were completely inhibited by bgj398 at 200 nm ( figs 5a and 5b )  . 
right panel : after 1 day , the cells were incubated with and without 20 ng / ml fgf2 in 0.1% bovine serum albumin / dmem for 16 hours at 37c . 
values are mean 6 se normalized to wt ( + fgf2 ) levels . bracket indicates groups within treatment types ( 2fgf or + fgf ) among fgfr4 - transfected samples that were significantly different ( p , .05 ) from each other in twotailed t tests . 
 ( e ) hucct - 1 cells were transfected with flag - tagged wt and r78h fgfr4 for 2 days and then processed for immunofluorescence by using an anti - flag antibody . 
he was originally treated in a clinical trial with gemcitabine , cisplatin , and silmitasertib , which resulted in a partial response . he remained on this treatment of 10 months , at which time his disease progressed and he was switched to capecitabine and oxaliplattwo months later , the disease became refractory to that regimen . 
after 1 day , the cells were serum starved in 0.1% bovine serum albumin / dmem overnight and then incubated with and without 25 ng / ml vascular endothelial growth factor ( vegf ) for 10 min at 37c . 
cell samples were then lysed and subjected to western blot analysis for flag - kdr , phospho - erk ( perk ) , total erk , and vinculequal amounts of total protein were loaded per lane . 
g55e expression of full - length receptor ( approximately 200 kda ) was decreased compared with wt , with the appearance of approximately 70to 80 - kda fragments , which suggested decreased stability / increased degradation of the g55e forperk was barely detectable in g55e samples and not increased by vegf treatment . 
brackets indicate groups within treatment types ( 2vegf or + vegf ) among kdr - expressing samples that were significantly different ( p , .05 ) from one another in two - tailed t tests . 
 ( d ) hucct - 1 cells were transfected with flag - tagged wt and variants of unknown significance kdr for 2 days and then processed for immunofluorescence with an anti - flag antibody . 
on the basis of this finding , the patient started on bgj398 ( clinicaltrials.gov identifier : nct02150967 ) , achieved a partial response to therapy after 2 months ( figs 5c and 5d ) , and maintained the response for an additional 4 months , at which time new lesions developed that led to discontinuation of bgj398 . 
as a result of our in vitro studies of f276c , a mechanism of action has now been correlated with this observed clinical response of the tumor to bgj398 . discussion the volume of new data from individual and group sequencing efforts ( eg , the cancer genome atlas ) has rapidly expanded the understanding of the incidence and frequency of mutations in disparate cancers . 
few mutations have extensive preclinical and clinical evidence that support the effectiveness of targeted therapies , and genomic testing often reveals that tumors have numerous vuss , including variant sequences for which no functional data are available . mutations that have not been functionally characterized present a significant and growing challenge to the treating physician . 
the extracellular receptor of fgfr2 contains an intrinsic disulfide bond between c278 and c342 in the immunoglobulin - like domain 3 ( ig3 ; shown in gold )  . residue f276 is highlighted in gray and is proximal to the disulfide bridge . 
the fgfr2 f276c variant ( highlighted in red ) may lead to the introduction of aberrant disulfide bonds that could alter the activation state of the prote ( b ) sequence alignment shows that residue f276 is highly conserved among the fgfr2 family from zebrafish to humans ( sequence alignment performed by using clustal omega [ embl - ebi , wellcome genome campus , uk ] ; uniprotkb entry numbers are shown )  . 
 ( c ) hucct - 1 cholangiocarcinoma cells transfected with the wt , k41e , and f276c fgfr2 forms for 2 days were fixed , permeabilized , and processed for immunofluorescence by using the flag antibody . 
kmch - 1 cells were transfected with fgfr2 forms by using a 3.5 / 5 ratio of f276c / wt and k41e dna to adjust expression of the f276c protein to similar levels as the wt forafter 1 day , cells were switched to serum - free medium with or without 20 ng / ml fgf2 and incubated an additional 16 hours at 37c before lysis . 
lysates were analyzed by western blot for expression of fgfr2 - flag , phospho - erk ( perk ) , total erk , and vincul ( f ) quantitation of fgfr2 levels in western blots as in ( e )  . 
brackets indicate groups within treatment types ( 2fgf or + fgf ) among fgfr2 - expressing samples that were significantly different ( p , .05 ) from one another in two - tailed t tests . 
 ( a ) kmch - 1 cells were transfected with f276c and wild type ( wt ) by using a 3.5 / 5 dna ratio , respectively , to normalize expression levels . 
values are mean 6 se and expressed as percent inhibition of perk signal compared with cells with no bgj398 . response of fgfr2 f276ccontaining tumor to bgj398 in ( c ) september 2015 ( pretreatment , with magnetic resonance imaging showing a 30.1mm tumor diameter [ red line ] ) and ( d ) october 2015 ( postinitiation of treatment , with pan - fgfr inhibitor bgj398 magnetic resonance imaging showing tumor shrinkage to an 18.2 - mm diameter [ red line ] )  . fgfr2flag perk fgfr2flag perk f276c bgj398 ( nm ) 50 100 200 f276c bgj398 ( nm ) becomes how to quickly assess the potentially deleterious effect of vuss that occur in therapeutically targetable genes . 
with multiple uncharacterized / unreported mutations returned for each patient , a method of prioritizing which variants to study in depth is necessary . we addressed this problem by developing an approach that uses an in silico filtering process to prioritize mutations of the highest biologic and clinical interest . 
of these 10 variants , seven were found to be altered in expression or activity relative to the wt protein , and three of these ( fgfr2 f276c , fgfr4 r78h , and kdr g539r ) demonstrated greater activity than their wt counterparts ( table 1 ) , which suggests that these mutations play a role in promoting oncogenesis . 
in contrast , four vuss ( fgfr4 k41e , kdr g55e , pdgfra v484m , and pdgfrb v316m ) exhibited reduced expression compared with their wt counterparts , and thus were unlikely to be involved in oncogenesis in the tumors where they occurred . 
these findings not only support the strength of our in silico analysis in predicting whether vuss are functionally altered but also point to the inability to distinguish among activating , deactivating , and destabilizing mutations . optimization of appropriate cellular models is important in methods development for functional evaluation of vuss . 
for more understanding of the functional significance of vuss , these studies should be followed by experiments that use cell types that match the vus tumor of origin and evaluate end points such as cell growth and viability . fgfr2 f276c was identified as a vus of potential interest because of the presence of several factors , including prediction of a deleterious effect by two algorithms , 3d modeling that suggests an increase in activity on the basis of its location in the ligand - binding ig3 , and proximity to a key disulfide bond . 
dashes ( ) indicate no change versus wild - type protein . abbreviation : vus , variant of unknown significance . * increases or decreases in activity ( phospho - erk levels ) indicate changes seen versus wild type upon stimulation with ligand , except for fgfr2 f276c , which exhibited increased constitutive activity . constitutive receptor dimerization and activation , which lead to a variety of skeletal and craniosynostosis disorders ( eg , crouzon and pfeiffer syndromes ) .16 - 18 our molecular modeling combined with the demonstration that f276c fgfr2 is more highly expressed and constitutively active than the wt receptor suggests that this mutation alters disulfide bonds , which alters receptor dimerization and activity similarly to the fgfr2 mutations seen in craniosynostosis syndromes . 
by using in vitro studies , we show that the f276c fgfr2 variant is sensitive to bgj398 , a panfgfr inhibitor , which was also reflected clinically in the response of a patients tumor when treated with bgj398 as part of a clinical trial ( fig 5 )  . 
however , additional studies , such as the testing of bgj398 effectiveness in impeding growth of organoids or xenografts that express wt versus f276c , are needed to confirm that fgfr2 f276c is actionable . the ability to identify potentially actionable vuss from numerous vuss for each patient tumor would simplify therapeutic choices . 
in silico analysis requires only hours to conduct and as demonstrated here , can yield a subset of vuss that encode therapeutically targetable proteins likely to be altered in function by their variant sequence . in vitro functional studies are more time consuming and may not fit practically within a patients progression timeline , but they may yield moredefinitive findings . 
gawryletz no relationship to disclose sikander ailawadhi consulting or advisory role : amgen , takeda pharmaceuticals , novartis research funding : pharmacyclics ( inst ) travel , accommodations , expenses : amgen , takeda pharmaceuticals , novartis stephen m . 
ansell honoraria : webmd , research to practice research funding : bristol - myers squibb ( inst ) , celldex therapeutics ( inst ) , seattle genetics ( inst ) , merck ( inst ) , affimed ( inst ) , trillium therapeutics ( inst ) kelly k . 
halfdanarson consulting or advisory role : lexicon ( inst ) , ipsen ( inst ) , merrimack ( inst ) research funding : esanex ( inst ) , ipsen ( inst ) , boston biomedical ( inst ) thai h . 
 research funding : merck , bristol - meyers squibb , roche ( inst ) , genentech ( inst ) , x4p pharmaceuticals ( inst ) , amgen ( inst ) prashant kapoor consulting or advisory role : sanofi ( inst ) research funding : amgen ( inst ) , takeda pharmaceuticals ( inst ) aaron s . 
mansfield consulting or advisory role : trovagene ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) travel , accommodations , expenses : bristol - myers squibb nathalie meurice no relationship to disclose amulya a . 
nowakowski consulting or advisory role : celgene ( inst ) , morphosys ( inst ) , genentech ( inst ) research funding : celgene ( inst ) animesh pardanani no relationship to disclose sameer a . 
feldman consulting or advisory role : infinity pharmaceuticals patents , royalties , other intellectual property : inventor of technology for which the mayo clinic holds an unlicensed patent or has submitted a patent application ( inst ) ramesh k . 
ramanathan honoraria : taiho pharmaceutical , cerulean pharma , pharmacyclics , insys therapeutics , novocure consulting or advisory role : cerulean pharma , novocure , insys therapeutics , pharmacyclics research funding : abbvie ( inst ) , celgene ( inst ) , merck ( inst ) , schering plough ( inst ) , merrimack ( inst ) , boston biomedical ( inst ) , berg ( inst ) , superlab far east ( inst ) steven i . 
robinson travel , accommodations , expenses : tricon pharmaceuticals raoul tibes research funding : novartis ( inst ) , merck ( inst ) , seattle genetics ( inst ) , boehringer ingelheim ( inst ) , astellas pharma ( inst ) , astex pharmaceuticals ( inst ) heidi d . 
mcwilliams consulting or advisory role : merrimack ( inst ) research funding : prism biolab ( inst ) , genentech ( inst ) , novartis ( inst ) , newlink genetics ( inst ) , eli lilly ( inst ) , aduro biotech ( inst ) , pfizer ( inst ) , sanofi ( inst ) travel , accommodations , expenses : astrazeneca mrinal m . 
wieben patents , royalties , other intellectual property : champions oncologylicensed ip - targeted therapy with abiraterone acetate ( $0 received ) , wuxi appteclicensed ip - breast cancer xenografts ( $12 , 737 to mayo clinic ; inst ) , affymetrix - licensed ip on several variants in drug processing enzymes ( $0 in past 2 years ) , life technologieslicensed ip on several variants in drug processing enzymes ( $0 in past 2 years ) tammy m . 
kennedy patents , royalties , other intellectual property : patent on unrelated work ( us patent 9 , 458 , 189 ) for ligation of stapled polypeptides issued october 4 , 2016 eric w . 
borad stock and other ownership interests : glaxosmithkline , gilead sciences consulting or advisory role : g1 therapeutics , td2 , fujifilm ( inst ) , agios ( inst ) , insys therapeutics ( inst ) , novartis ( inst ) , arqule ( inst ) , celegene ( inst ) , inspyr therapeutics , halozyme therapeutics ( inst ) research funding : boston biomedical ( inst ) , mirna therapeutics ( inst ) , senhwa biosciences ( inst ) , medimmune ( inst ) , bioline ( inst ) , agios ( inst ) , halozyme therapeutics ( inst ) , celgene ( inst ) , threshold pharmaceuticals ( inst ) , toray ( inst ) , dicerna pharmaceuticals ( inst ) , sillajen ( inst ) , eisai ( inst ) , taiho pharmaceuticals ( inst ) , emd serono ( inst ) , isis pharmaceuticals ( inst ) , incyte ( inst ) , sun biopharma ( inst ) , ariad pharmaceuticals ( inst ) , imclone systems ( inst ) travel , accommodations , expenses : arqule , celgene , astrazeneca aminah jatoi research funding : entera health , boston biologics martin e . 
kennedy , university of georgia , athens , ga . supported by the mayo clinic center for individualized medicine . presented at the science of team science 2016 conference , phoenix , az , may 16 - 19 , 2016 . support prior presentation references 35 : 49 - 62 , 2016 1 . 
horak p , fr ohling s , glimm h : integrating next - generation sequencing into clinical oncology : strategies , promises onco targets ther 9 : 7355 - 7365 , 2016 and pitfalls . 
harris pa , taylor r , thielke r , et al : research electronic data capture ( redcap ) a metadata - driven methodology and workflow process for providing translational research informatics support . 
steinberger d , vriend g , mulliken jb , et al : the mutations in fgfr2 - associated craniosynostoses are clustered in five structural elements of immunoglobulin - like domain iii of the receptor . 
lajeunie e , heuertz s , el ghouzzi v , et al : mutation screening in patients with syndromic craniosynostoses indicates that a limited number of recurrent fgfr2 mutations accounts for severe forms of pfeiffer syndrome . 
ratisoontorn c , fan gf , mcentee k , et al : activating ( p253r , c278f ) and dominant negative mutations of fgfr2 : differential effects on calvarial bone cell proliferation , differentiation , and mineralization . 
 o circulating braf v600e cell - free dna as a biomarker in the management of anaplastic thyroid carcinoma purpose anaplastic thyroid cancer ( atc ) is a deadly form of thyroid cancer . 
we explored the ability of droplet digital polymerase chain reaction ( ddpcr ) to identify this mutation in circulating cell - free dna ( cfdna ) in plasma . materials and methods the ddpcr assay was evaluated for its sensitivity , specificity for detection of braf v600e cfdna , and concordance with tumor tissue . 
the assay also was used to evaluate its potential role as a biomarker of response . results forty - four patients with atc who were tested for the braf mutation by tumor tissue dna sequencing or immunohistochemistry were included . 
in addition , cfdna levels by ddpcr were predictive of treatment response in 71% of samples . conclusion cfdna detection by ddpcr is highly sensitive , specific , and concordant with mutation status on atc tumors . 
2018 by american society of clinical oncology introduction anaplastic thyroid carcinoma ( atc ) is responsible for one third of thyroid cancer deaths and has a high mortality rate.1 , 2 braf v600e is the most common actionable driver mutation in atc , which is seen in approximately 45% of these cancers.3 , 4 indeed , targeted treatment strategies are extending patient survival , 5 - 8 and the braf plus mek inhibitor combination dabrafenib plus trametinib was recently approved by the food and drug administration for braf v600emutated atc.9 , 10 diagnosis of atc usually is made by biopsy . 
 unlike differentiated tumors , the lack of sufficient viable tissue hampers molecular diagnostic testing.2 , 11 , 12 given the rapid progression of atc , rapid testing is needed for timely therapeutic intervention . 
liquid biopsy ( mutation testing performed on blood samples ) provides a potential alternative to tissue biopsy in the management of certain malignancies.13 - 15 the detection of mutations in circulating cell - free dna ( cfdna ) , such as braf v600e , can serve as a surrogate for mutation testing on tissue biopsy , and its overall levels provide a novel marker in predicting thyroid cancer burden.16 , 17 the need for molecular testing on tissue before treatment with selective braf inhibitors may substantially delay the time to initiation of a beneficial treatment in patients with braf - mutated atc.8 , 18 - 22 we have demonstrated previously priyanka c . 
 patients with atc prospectively enrolled ( n = 58 ) excluded ( n = 14 ) did not have atc ( n = 6 ) mutation on tumor not tested ( n = 2 ) no evidence of active atc ( n = 2 ) no guardant sample drawn simultaneously ( n = 4 ) ( n = 44 ) correlation of cfdna braf status by ddpcr with tissue braf - mutated cfdna as a biomarker of response ( n = 44 ) ( n = 16 ) fig 1 . 
 in the absence of readily available tumor mutation profiling , we obtain both braf v600e by ihc on tissue biopsy and cfdna on plasma by ngs simultaneously before initiation of treatment . 
the ihc analysis antibody is anti - braf p.v600e ( clone ve1 , dilution 1 : 50 ; spring bioscience , pleasanton , ca ) and is performed on a ventana benchmark ultra autostainer ( ventana medical systems , tucson , az )  . patients who had a cfdna analysis by ngs more than 2 weeks before the research ddpcr sample draw were excluded from concordance testing . 
however , if patients tested positive for the braf v600e mutation on their tumor tissue and were receiving treatment , serial plasma samples were collected for ddpcr assay during their treatment to examine the correlation of cfdna levels with response to treatment . study population for correlation of changes in cfdna levels with response to treatment patients with tissue - positive braf v600e mutation were followed prospectively during their respective treatments to evaluate whether levels of circulating braf v600e cfdna by ddpcr could serve as a biomarker for monitoring response to therapy . 
blood samples for cfdna analysis were drawn at routinely scheduled laboratory appointments . braf v600e mutation analysis tumor tissue was tested for braf mutation status by either ihc or ngs at our center ( 50gene somatic mutation analysis panel , 25 solid tumor genomics assay version 1 that examines 134 genes , 26 or foundationone genomic test27 ) , depending on the quantity of viable tumor tissue available for testing . 
of patients median age , years ( range ) male female stage at diagnosis braf status on tumor braf v600e mutation * braf wild type method of braf analysis on tumor ihc without ngs baseline liquid biopsy sample by ngs drawn not drawn no . 
 abbreviations : ihc , immunohistochemistry ; ngs , next - generation sequencing . * of these patients , 17 ( 85% ) had tumor tissue tested by ngs and three ( 15% ) by ihc . of the five patients who were tested for the presence of the braf v600e protein by ihc , one had testing for and detection of the same mutation by single - gene polymerase chain reaction at an outside facility before referral to our center . 
two patients who had tumor tissue tested only by ihc did not have additional testing by ngs because of insufficient tumor tissue . sequencing test28 ( guardant health , redwood city , ca )  . evaluation of response to treatment a single independent radiologist reviewed the images at baseline and at the time of restaging while patients were receiving treatment . 
 we determined clinical responses by calculating the percent change ( from baseline and after / during treatment ) in the size of target lesions identified using response evaluation criteria in solid tumors ( recist ) version 1.1 , 29 but we modified slightly the definitions of response . 
for the purpose of our study , an increase in tumor size was defined as an increase in the sum of target lesions greater than or equal to 10 mrecist progression in nontarget lesions was assigned an additional 20 mm to the sum of target lesions . 
a decrease in tumor size was defined as a decrease in sum of target lesions greater than or equal to 10 m stable tumor size was defined as a change in tumor burden between 9 and 9 mm . data analysis testing for concordance between circulating v600e cfdna by ddpcr and tumor tissue and cfdna by ngs and tumor tissue . 
a false positive was defined by the presence of a mutation in cfdna when tumor tissue tested negative , and a false negative was indicated when the mutation was not detected in cfdna but tumor tissue tested positive for braf v600e mutation . concordance between braf v600e mutation in cfdna by ddpcr with braf mutation status on tumor tissue by ngs , ihc , and pcr was calculated as number of concordant samples / ( number of concordant samples + number of discordant samples )  . 
concordance also was calculated for the detection of braf mutation in cfdna samples by ngs and tumor tissue . testing for correlation of change in circulating v600e ddpcr levels with changes in tumor size . 
 in patients who were followed prospectively , concordance was calculated between the change in the level of braf - mutated cfdna by ddpcr and change in tumor size on restaging scans during treatment . 
any increase in the level of cfdna was called concordant if that correlated with an increase in tumor size of greater than or equal to 10 m similarly , any decrease in the level of cfdna was called concordant if it correlated with a decrease in tumor size of greater than or equal to 10 mif there was no change in the level of cfdna correlating with 9 to 9 mm , the sample was called concordant . 
concordance between detection of circulating braf v600e cell - free dna ( cfdna ) by droplet digital polymerase chain reaction ( ddpcr ) and next - generation sequencing ( ngs ) on liquid biopsy with mutation status on tumor . 
npv , negative predictive value ; ppv , positive predictive value . statistical tests sensitivity and specificity of detection of braf - mutated cfdna by ddpcr and by ngs were calculated and reported with exact 95% cis . 
fishers exact test was conducted to calculate concordance between cfdna levels and the corresponding radiologic events , specifically , increase in tumor size , tumor shrinkage , and stable tumor size . results fifty - eight patients with a suspected atc diagnosis were prospectively enrolled in the study . 
of the remaining 44 patients , 16 who had a braf v600e positive tumor were followed for correlation changes in cfdna with response to treatment . detection of braf v600e cfdna on liquid biopsy the lowest allelic fraction ( af ) for braf v600e detected by ddpcr was 0.07% and for cfdna by ngs , 0.1%. 
of the 20 patients who tested positive for braf mutation on tissue , 17 ( 85% ) were positive for braf v600e cfdna by ddpcr and 16 ( 80% ) were positive for cfdna by ngs ( fig 2 )  . 
detection of braf - mutated cfdna by ddpcr was 93% concordant with tumor testing , whereas detection of cfdna by ngs was 91% ( 95% ci , 8% to 14% )  . 
forty - three ( 98% ) also had blood samples sent for cfdna by ngs . correlation between changes in braf v600e cfdna by ddpcr and changes in tumor size sixteen patients whose tumors tested positive for braf mutation were prospectively followed and had plasma samples drawn during scheduled laboratory appointments before the clinic visit . 
in the three patients who tested false negative by ddpcr , tumor burden at baseline ranged from 31 to 33.3 m these patients had had their primary tumor treated with surgery ( thyroidectomy in two patients and hemithyroidectomy in one patient )  . 
the braf v600e cfdna was detectable in tumors larger than 52.5 mm , with the exception of a single patient who had an 8 - mm lung nodule that presented while he was receiving adjuvant radiation to the thyroid bed with chemotherapy . of 36 time points , 27 ( 75% ) provided concordant findings between changes in cfdna levels and response to therapy ( table 3 )  . 
we included the three patients who tested false negative by ddpcr in this group because the braf v600e cfdna levels continued to remain undetectable , which correlated with these patients continued response to treatment with braf inhibitor . 
one patient with braf positivity on tumor did not get testing done by next - generation sequencing ( ngs ) on liquid biopsy ; therefore , the analysis was done on 43 patient samples . 
because all 24 of the patients without braf mutation tested negative for cell - free dna by droplet digital polymerase chain reaction ( ddpcr ) and ngs , the receiver operating characteristic curve is degenerate . 
one patient showed an increase in cfdna levels 2 weeks after starting braf inhibitor therapy , which was consistent with the increased tumor size observed on his first restaging scans 2 months after starting this treatment . 
figure a1 shows an example of the trends in cfdna levels that correlated with changes in tumor size on imaging in a patient who was initially treated with nab - paclitaxel followed by braf and mek inhibitor therapy and then with the addition of immunotherapy ( pembrolizumab )  . 
the levels of braf cfdna trended upward despite the addition of pembrolizumab because the patient was not able to swallow the braf inhibitor , which led to nonadherence and eventual progression . discussion the braf v600e mutation is the most common actionable mutation in atc tumors . 
 recent studies have shown promising results with dabrafenib plus trametinib ( braf and mek inhibitors ) in terms of clinical response and survival , 9 , 18 , 30 and this combination is now food and drug administration approved for braf - mutated atc . 
hence , identification of this mutation for timely initiation of treatment is important . in addition to the ability to identify an actionable mutation for initiation of therapy , development of biomarkers is needed to predict and assess treatment response in atc . 
of patients median age , years ( range ) male female stage at diagnosis treatment received * surgery radiation sensitizing chemotherapy systemic therapy braf inhibitor + mek inhibitor braf inhibitor + mek inhibitor + immunotherapy no . 
patients with a braf mutation on their tumor tissue had liquid biopsy samples drawn prospectively for assessing correlation of changes in levels of circulating braf v600e cell - free dna detected by droplet digital polymerase chain reaction with response to treatment . * patients received more than one treatment modality . ( tg ) levels are a biomarker of response to therapy . 
given the successes observed for other cancers where tumor - specific biomarkers do not exist , we believe that changes in braf v600e cfdna could provide a specific biomarker for monitoring response to treatment in patients with atc.19 although response can be assessed by imaging , a marker to predict response allows sufficient time to change the treatment plan before the patient becomes too ill . in this study , we show that cfdna by ddpcr is a sensitive and highly specific technique for determining braf status in patients with atc . 
braf cfdna and rna in liquid biopsy have been shown to be useful biomarkers in patients with dtc as well as in a murine model of atc.31 , 32 the current study is the first in our knowledge to evaluate ddpcr to detect braf - mutated cfdna in the circulation of patients with atc . 
in a phase ii clinical trial in radioiodine - refractory dtc , braf v600e cfdna was detectable by ddpcr in only 35% of patients , 33 whereas in our study , it was detected in 85% of patients with atc . 
 therefore , we suggest that in patients with low measurable disease , reliance solely on cfdna for identifying the braf mutation may not be advisable , and molecular testing on tumor tissue should be awaited . a murine model of braf - mutated atc circulating rna levels has been shown to be a useful biomarker of response to therapy.32 in the current study , we show that ddpcr is a useful technique for serial monitoring of cfdna levels as a predictive biomarker in patients with atc table 3 . 
increase in tumor size was defined as any change in the sum of target lesions 10 mprogression in nontarget lesions ( ie , nonmeasurable disease ) was assigned an additional 20 mm to the sum of target lesions . 
these findings were similar to that observed in patients with melanoma.34 , 35 in patients whose braf v600e cfdna levels rise after initiating braf and mek inhibitor therapy , resistance to treatment should be considered , prompting early restaging scans and consideration of alternative treatment options upon confirmation . 
one possible explanation is that targeted treatment indeed led to a reduction in the braf v600eharboring tumor cells but led to clonal expansion of tumor cells that harbored other driver mutations as a mechanism of resistance . 
however , the small sample size limited us from evaluating the association of the af of the braf v600e cfdna with prognosis and overall survival . in conclusion , ddpcr is a novel , noninvasive technique for detecting braf v600e cfdna in patients with atc and should be considered in routine standard - of - care testing . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ramona dadu research funding : astrazeneca , merck , eisai , genentech , bristol - myers squibb mark zafereo no relationship to disclose naifa l . 
 renata ferrarotto consulting or advisory role : ayala research funding : oncomed pharmaceuticals ( inst ) , g1 therapeutics ( inst ) , astrazeneca ( inst ) , medimmune ( inst ) , emd serono ( inst ) , genentech ( inst ) , roche ( inst ) , merck serono ( inst ) vivek subbiah consulting or advisory role : medimmune research funding : novartis ( inst ) , glaxosmithkline ( inst ) , nanocarrier ( inst ) , northwest biotherapeutics ( inst ) , genentech ( inst ) , roche ( inst ) , berg ( inst ) , bayer ag ( inst ) , incyte ( inst ) , fujifilm ( inst ) , pharmamar ( inst ) , d3 oncology solutions ( inst ) , pfizer ( inst ) , amgen ( inst ) , abbvie ( inst ) , multivir ( inst ) , blueprint medicines ( inst ) , loxo oncology ( inst ) , vegenics ( inst ) , takeda pharmaceuticals ( inst ) , alfasigma ( inst ) , agensys ( inst ) , idera ( inst ) , boston biomedical ( inst ) , inhibrx ( inst ) , exelixis ( inst ) travel , accommodations , expenses : pharmamar , bayer neil gross honoraria : intuitive surgical consulting or advisory role : pds biotechnology , verb surgical ( inst ) research funding : regeneron pharmaceuticals , medimmune ( inst ) , genentech ( inst ) brandon g . 
cabanillas consulting or advisory role : loxo oncology , blueprint medicines research funding : kura oncology , eisai , roche , genentech , exelixis acknowledgment we thank the patients with atc who agreed to provide samples , karen bohannon - johnson for phlebotomy support , and clinical colleagues who provided access to their patients for this study . affiliations all authors : the university of texas md anderson cancer center , houston , tx . supported by an endocrine fellows foundation grant ( p.c.i. ) and national cancer institute grant no . 
takahashi s , kiyota n , yamazaki t , et al : phase ii study of lenvatinib in patients with differentiated , medullary , and anaplastic thyroid cancer : final analysis results . 
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cradic kw , milosevic d , rosenberg am , et al : mutant braf ( t1799a ) can be detected in the blood of papillary thyroid carcinoma patients and correlates with disease status . 
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schreuer m , meersseman g , van den herrewegen s , et al : quantitative assessment of braf v600 mutant circulating cell - free tumor dna as a tool for therapeutic monitoring in metastatic melanoma patients treated with braf / mek inhibitors . 
chen g , mcquade jl , panka dj , et al : clinical , molecular , and immune analysis of dabrafenibtrametinib combination treatment for braf inhibitor - refractory metastatic melanoma : a phase 2 clinical trial . 
 cfdna declined at the time of response to therapy correlated with tumor shrinkage from baseline , and an increase in cfdna levels at the time of progression correlated with a radiologic increase in tumor burden . - 25c nab - paclitaxel dabrafenib + trametinib + pembrolizumab time ( months ) isolation of cell - free dna for droplet digital polymerase chain reaction after obtaining patient consent , approximately 8 to 10 ml of blood were drawn into each of two edta tubes . 
plasma was separated from the cell components after centrifuging twice at 2 , 000 rpm for 10 minutes at 4c and then stored at 80c to allow for batch isolation of cell - free dna ( cfdna )  . 
the amount of dna was quantified using a qubit fluorometer ( thermo fisher scientific , waltham , ma )  . droplet digital polymerase chain reaction the detection of the braf v600e mutation was performed in a research laboratory setting using the qx200 droplet digital pcr system ( bio - rad , hercules , ca ) and the validated primepcr ddpcr mutation assay ( bio - rad ) , which was multiplexed with an assay for detection of braf unmutated codon ( wild type )  . 
the cfdna yields using this protocol ranged from 2 to 132 ng / ml when measured by qubit fluorometer , which allowed a median estimated input of 5 ng per assay . 
droplets were counted with the qx200 droplet reader , and data were analyzed using quantasoft software ( bio - rad ) , with thresholds for fam and hex detection manually set on the basis of results from the no - template control . 
 therapy - related erythroleukemia in a man with metastatic ewing sarcoma : a clinical role for advanced molecular diagnostics introduction therapy - related leukemia may be challenging to diagnose when a patient has cytopenia during treatment of another malignancy , particularly when there are few circulating leukemia cells . 
 here , we report a case of a 55 - year - old man with refractory ewing sarcoma who presented with thrombocytopenia and tumor lysis syndrome ( tls ) ; he was found to have pure erythroid leukemia ( pel ) , likely resulting from prior alkylating agent and / or topoisomerase ii inhibitor chemotherapy . 
furthermore , when patients with metastatic solid tumor have cytopenia , they may not undergo bone marrow ( bm ) evaluation if the cytopenia has already been attributed to therapies or the prior malignancy . in this case , initial diagnostics and the poorly differentiated morphology seen in the bm biopsy specimen did not readily distinguish between ewing sarcoma and acute leukemia . 
he was diagnosed with ewing sarcoma in 2011 , after a known right - side lower - lobe lung mass demonstrated increased size and malignant radiologic features on computed tomography ( ct ) imaging . 
the patient underwent right - side lower lobectomy and metastasectomy of bilateral pectoral lesions , radiation ( xrt ) to his rib , and additional chemotherapy with dactinomycin , vincristine , and cyclophosphamide , followed by xrt to his pectoral surgical bed . 
he started a trial of olaparib and temozolomide in august 2015 , which continued until october 2016 , when he was removed from protocol after ct imaging showed disease progression . 
cumulatively , he received 31 cycles of chemotherapy and four treatments of xrt . one month after stopping therapy , the patient presented with fatigue , dyspnea , fevers , bruising , and petechial rash , with no hepatosplenomegaly . 
peripheral smear revealed left - shifted myeloid cells and large basophilic cells with vacuolated cytoplasm ; these cells constituted 9% of blood leukocytes and were interpreted as either reactive atypical lymphocytes , circulating ewing sarcoma cells , or circulating blasts . 
zmynd8 exons 1 through 22 fuse with rela exons 3 through 11 to form the fusion gene zmynd8 - rela , which has been described in erythroleukemia.2 zmynd8 exons 1 - 22 zmynd8 - rela fusion chromosome 20 exons 3 - 11 rela chromosome 11 cbc counts at the ewing sarcoma diagnosis in 2011 were unavailable , cbc counts in 2013 were normal ( wbc , 4.9 103 / l ; hemoglobin , 14.0 g / dl ; platelets , 207 103 / l )  . he underwent bm biopsy and aspiration , and began treatment of tls with rasburicase , allopurinol , and normal saline . 
however , treatment was complicated by persistent cytopenia and hallucinations , likely related to ifosfamide . the bm biopsy specimen was hypercellular and revealed replacement by primitive , discohesive cells , which , by flow cytometry , were negative for cd45 , cd34 , myeloperoxidase , cd13 , and cd56 . 
by immunohistochemistry , cells were negative for cytokeratin , cd43 , and cd56 , but were positive for cd99 ( present in up to 98% of ewing sarcoma but also expressed in other cancers , including leukemia ) .3 - 6 preliminary bm karyotype identified an 11q13 abnormality , but no ewsr1 rearrangement . 
interphase fluorescent in situ hybridization study also did not reveal ewsr1 rearrangement . molecular testing was performed via heme snapshot assay , an institutional ngs platform using illumina truseq amplicon technology ( san diego , ca ) for single nucleotide variant and insertion / deletion detection in genomic dna.7 snapshot results are descriptive and cannot determine clonality , tumor - stromal percentage , or percentage of cells carrying mutations . 
 analysis was undertaken using a sequencing library generated with an oligo pool focusing on approximately 141 kb of genomic content consisting of 568 amplicons covering 15 full genes and exonic hotspots in 39 genes ( trusight myeloid sequencing panel ; illumina )  . testing identified three tp53 mutations with the following allelic frequencies : r337p , 38% ; i255f , 38% ; and y220c , 10% . 
these findings confirmed diagnosis of therapy - related pel , rather than progressive ewing sarcoma . the patient transiently improved after ifosfamide / etoposide treatment , but the leukemia ultimately progressed , at which point he opted for comfort care . 
he died 2 months after pel diagnosis . methods this anchored multiplex fusion assay is an ngs method that amplifies small amounts of nucleic acid and detects fusions without targeting specific rearrangements . 
two heme - nested pcr reactions are then performed to create a fully functional sequencing library targeting specific genes and exons ( fusionplex solid tumor kit ; archerdx , boulder , co )  . 
illumina misequation 2 147 base pairend sequencing results are aligned to the hg19 human genome reference , and a laboratory - developed algorithm is used for fusion transcript detection and annotation . 
the resulting product can then be processed for illumina or ion torrent ( thermo fisher scientific , waltham , ma ) sequencing.10 discussion this case highlights how the evolving field of molecular genetic diagnostics can help distinguish specific cancer diagnoses . 
advanced molecular testing using ngs and an rna - based solid fusion assay ultimately clarified this patients diagnosis . ewing sarcoma describes a family of cancers with fusion oncogenes involving the ewsr1 gene.13 there is a high correlation between bony metastases and bm involvement , and , to our knowledge , pel has not been described in refractory ewing sarcoma before this case report.14 - 17 therapy - related leukemia is a rare adverse effect of alkylating agents , radiotherapy , and topoisomerase ii inhibitors . 
tumor cells were positive for e - cadherin and cd71 ( not shown )  . erythroid precursors with 30% proerythroblasts.22 patients typically present with sequelae of pancytopenia from erythroid precursor proliferation . pel also has a very complex karyotype compared with other leukemias and can be difficult to diagnose , given its negativity for other markers typically expressed in aml , such as cd45 , cd13 , myeloperoxidase , and cd34.20 , 22 , 23 cd45 is commonly used to screen for hematologic neoplasms on initial pathologic staining . 
 ( megakaryoblastic anemia is another cd45 - negative leukemia . ) e - cadherin , expressed in most pel cases , helped lead us toward the correct diagnosis , as did demonstration of the rare zmynd8 - rela fusion . 
the latter is hypothesized to promote oncogenesis via constitutive nf - b activation.1 by definition , aml after exposure to cytotoxic chemotherapy or radiation is therapy - related aml , of which there are two primary etiologic subtypes : alkylating agent / radiotherapyrelated type and topoisomerase ii inhibitorrelated type.24 , 25 alkylating agents and radiotherapy exhibit dose - dependent risk of disease effected via centromeric breakage and partial or complete chromosome loss , particularly at chromosomes 5 and 7 . 
the leukemia had several balanced translocations , including t ( 11 ; 20 ) ( q12 ; q13.1 ) , and a partial deletion of chromosome 4 . mutations in tp53 , as seen in this case , are common in t - aml . 
interestingly , recent data suggest that tp53 - mutated clones may exist before the exposure to chemotherapy and expand under the selective pressure of treatment of another malignancy.27 this is the first reported case of greater than two tp53 mutations in t - aml.9 , 27 regardless of the inciting agents , t - aml is associated with dismal outcomes , such as were experienced by this patient . in patients with advanced cancers treated with alkylating agents , radiotherapy , or topoisomerase ii inhibitors , t - aml should be considered as a cause of refractory cytopenia . 
angelini df , ottone t , guerrera g , et al : a leukemia - associated cd34 / cd123 / cd25 / cd99 + immunophenotype identifies flt3 - mutated clones in acute myeloid leukemia . 
dias - santagata d , akhavanfard s , david ss , et al : rapid targeted mutational analysis of human tumours : a clinical platform to guide personalized cancer medicine . 
ok cy , patel kp , garcia - manero g , et al : tp53 mutation characteristics in therapy - related myelodysplastic syndromes and acute myeloid leukemia is similar to de novo diseases . 
green dc , deharvengt sj , de abreu fb , et al : use of anchored multiplex pcr enrichment for detection of gene fusions in solid tumors by next generation sequencing . 
thiel u , wawer a , von luettichau i , et al : bone marrow involvement identifies a subgroup of advanced ewing sarcoma patients with fatal outcome irrespective of therapy in contrast to curable patients with multiple bone metastases but unaffected marrow . 
cuneo a , van orshoven a , michaux jl , et al : morphologic , immunologic and cytogenetic studies in erythroleukaemia : evidence for multilineage involvement and identification of two distinct cytogenetic - clinicopathological types . 
kasyan a , medeiros lj , zuo z , et al : acute erythroid leukemia as defined in the world health organization classification is a rare and pathogenetically heterogeneous disease . 
olney hj , mitelman f , johansson b , et al : unique balanced chromosome abnormalities in treatment - related myelodysplastic syndromes and acute myeloid leukemia : report from an international workshop . 
in their letter , karam et al express concerns about the claims made regarding the inability of rna sequencing ( rna - seq ) to perform allele - specic quantication . however , we believe our statement that rna - seq does not allow the allele - specic quantication of normal full - length transcript is correct . the percent splicing index measures the frequency at which a given splice event occurs compared with others affecting the same site.3 as karam et al1 note , this allows one to quantify reads from aberrant transcripts relative to reference transcripts but it does not provide an allele - specic quantication of splicing . 
however , in the case of intronic variants , rnaseq cannot determine whether any of the full - length transcript is also produced by the variant allele because the variant is not part of the messenger rna sequence . 
in the absence of an additional informative variant in the exon , rna - seq cannot distinguish between a full splice defect ( no full - length transcript is made by the variant allele ) and a partial or leaky splice defect ( some full - length transcript is produced by the variant allele )  . 
as gelli et al4 noted , partial splice defects may not be pathogenic if the variant allele produces enough full - length transcript to support normal protein function . in their letter , karam et al1 highlighted a recent publication by landrith et al3 and indicated that rnaseq was used to identify partial skipping of exon 5 in the brca2 c.426 - 12_426 - 8del variant carrier and control patients . 
of note , the landrith et al denition of partial exon skipping is some portion of the exon is skipped ( ie , alternative acceptor / donor ) , 3 not as a partial splice defect . 
however , other published data do show that brca2 c.426 - 12_426 - 8del causes a partial splice defect.8 our laboratory now classies this variant as benign based on additional phenotypic and mutation co - occurrence data , 2 which suggests that the amount of normal transcript produced by the variant allele does support normal protein function . with increased use of tools such as rna - seq to aid in variant classication , physician understanding of how these tools should be used is critical to appropriate patient care . 
we would like to emphasize that we are not arguing against the use of functional rna studies in producing data to support variant classication . rather , we are promoting the need for improved guidelines for interpretation and use of such data in variant classication . 
sharing of reclassication advancements and variant classication information through publications such as the article by nix et al2 allows for dissemination of high - quality data that has passed peer review . 
nix p , mundt e , manley s , et al : functional rna studies are a useful tool in variant classication but must be used with caution : a case study of one brca2 variant . 
gelli e , colombo m , pinto am , et al : usefulness and limitations of comprehensive characterization of mrna splicing proles in the denition of the clinical relevance of brca1 / 2 variants of uncertain signicance . 
rna - seq allows the use of a method called the percent splicing index to quantify allelic expression by mapping rna - seq reads from alternate or aberrant transcripts relative to reference ( normal ) transcripts as described by schafer et al.7 we have recently published data demonstrating that the variant brca2 c.426 - 12_426 - 8delgtttt not only results in partial skipping of exon 5 ( brca2 r.426_475del ) , but this splicing event was also seen in 20 of 345 control patients.8 laboratories should proceed with caution when weighting functional evidence in variant curation , because interpretation of these results can be complex . 
in this specic case , the rna - seq results and the new clinical data prompted reassessment and resulted in reclassication of this brca2 variant . the article by nix et al6 highlights the need for laboratories to increase collaboration , particularly when siloed clinical information can shed light onto discrepant classications . 
submission of a classication and its justication to dynamic databases such as clinvar is a critical step in this process , 9 because data sharing among clinical diagnostic laboratories improves the resolution of variant interpretation differences.10 in summary , we believe that innovation , such as introduction of rna - seq to hereditary cancer clinical genetic testing as well as participation in multi - institutional efforts designed to increase transparency between laboratories , is of utmost importance for advancing variant classication that will ultimately benet patients . rachid karam , md , phd ; holly laduca , ms ; marcy e . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . rachid karam employment : ambry genetics research funding : ambry genetics travel , accommodations , expenses : ambry genetics holly laduca employment : ambry genetics stock and other ownership interests : ambry genetics marcy e . 
richardson employment : ambry genetics tina pesaran employment : ambry genetics stock and other ownership interests : ambry genetics travel , accommodations , expenses : ambry genetics elizabeth chao employment : ambry genetics no other potential conicts of interest were reported . references cummings bb , marshall jl , tukiainen t , et al : improving genetic diagnosis in mendelian disease with transcriptome sequencing . 
sci transl med 9 : eaal5209 , 2017 fr esard l , smail c , ferraro nm , et al : identication of rare - disease genes using blood transcriptome sequencing and large control cohorts . 
nat med 25 : 911 - 919 , 2019 gonorazky hd , naumenko s , ramani ak , et al : expanding the boundaries of rna sequencing as a diagnostic tool for rare mendelian disease . 
am j hum genet 104 : 466 - 483 , 2019 lee h , huang ay , wang l - k , et al : diagnostic utility of transcriptome sequencing for rare mendelian diseases . 
genet med 22 : 490 - 499 , 2020 karam r , conner b , laduca h , et al : assessment of diagnostic outcomes of rna genetic testing for hereditary cancer . 
nix p , mundt e , manley s , et al : functional rna studies are a useful tool in variant classication but must be used with caution : a case study of one brca2 variant . 
jco precis oncol 4 : 730 - 735 , 2020 schafer s , miao k , benson cc , et al : alternative splicing signatures in rnaseq data : percent spliced in ( psi )  . 
curr protoc hum genet 87 : 11.16.111.16.14 , 2015 landrith t , li b , cass aa , et al : splicing prole by capture rna - seq identies pathogenic germline variants in tumor suppressor genes . 
the precise impact of these panels on clinical decision making is not well understood . methods here , we report our institutional experience with a targeted 40 - gene panel ( myeloseq ) that is used to generate a report for both genetic variants and variant allele frequencies for the treating physician ( the limit of mutation detection is approximately one aml cell in 50 )  . results in total , 346 sequencing reports were generated for 325 patients with suspected hematologic malignancies over an 8 - month period ( august 2018 to april 2019 )  . 
to determine the inuence of genomic data on clinical care for patients with acute myeloid leukemia ( aml ) , we analyzed 122 consecutive reports from 109 patients diagnosed with aml and surveyed the treating physicians with a standardized questionnaire . 
inuences were often nuanced and extended beyond identifying actionable genetic variants with us food and drug administrationapproved drugs . conclusion this study provides insights into how physicians are currently using multigene panels capable of detecting relatively rare aml cells . 
the most inuential way to integrate these tools into clinical practice will be to perform prospective clinical trials that assess patient outcomes in response to genomically driven interventions . jco precis oncol 5 : 191 - 203 . 
some quires variant single - gene tests and two multitarget panels are currently us food and drug administration ( fda ) approved and have associated companion diagnostics that designate a specic cancer subtype and indication.2 however , the vast majority of variant identication and annotation is performed by laboratory developed tests ( ldts ) , 3 for which results are provided as a clinical report . 
these reports typically require a certain level of genomic literacy to understand and implement.4 , 5 lack of report standardization , inadequate genomic training , 6 , 7 limited infrastructure to support oncologists , 1 , 8 and limited resourcesfor example , low reimbursement rates and lack of access to clinical trialsare thought to hinder the impact of sequencing data on clinical care.9 , 10 the result is a discrepancy between the identication of clinically actionable variants11 and implementation of change in treatment decisions.1 , 12 acute myeloid leukemia ( aml ) sequencing data are particularly complex because of the genetic and clonal heterogeneity of aml cases . 
 barnell et al context key objective whereas physicians have increased the use of targeted sequencing panels to inform treatment decisions for patients with hematologic malignancies , the impact and utility of sequencing data on clinical decision making is not well understood . 
through standardized surveys , this study captured the nuanced impact of sequencing data on clinical decision making for patients with acute myeloid leukemia . knowledge generated physicians self - reported that 50 of 114 sequencing reports ( 44% ) inuenced clinical care decisions with 56 total inuences reported , 38 of which were related to therapeutic options , 10 related to risk stratication in rst clinical remission , and eight involving measuring persistent molecular disease . 
in 11% of all patients , the panel was ordered at multiple timepoints during the disease course for persistent molecular disease monitoring . relevance this study demonstrates that physicians are integrating sequencing data obtained at various points in the acute myeloid leukemia disease course into clinical decision making , mostly to determine therapy choices , stratify relapse risk , and measure persistent disease . signicance may depend on cooperating covariants in multiple other genes.14 for example , european leukemianet / national comprehensive cancer network guidelines specically mention six genes / mutations in their risk stratication guidelines , all of which must be evaluated in parallel for risk stratication.15 , 16 in addition , whereas pathogenic variants within three genesflt3 , idh2 , and idh1have been used as predictive markers for fda - approved targeted therapeutics , 17 - 19 ongoing clinical trials have demonstrated predictive utility for other pathogenic variants that do not yet have approved companion diagnostics.20 next - generation sequencing ( ngs ) data can provide information beyond therapeutic sensitivity / resistance that is not currently captured by fda - approved diagnostics . specically , quantication of the variant allele frequency ( vaf ) of tumor - associated variants has been used to detect persistent molecular disease ( pmd ) after therapies are administered , and predict both relapse risk21 and survival outcomes.22 - 24 although multipanel ldt diagnostics are being used on patients with aml to supplement treatment decisions , the utility of these reports is not well described . this study sought to better understand the extent to which genomic reports inuence clinical decision making for patients with aml . 
this paper describes physician experience with a targeted gene panel ( myeloseq ) that terrogates 40 recurrently mutated genes or gene hotspots and returns gene variant and vaf data to the treating physician . 
we determined usage patterns over an 8 - month period and surveyed treating physicians regarding how they used the panel results in clinical care . methods study design and patient eligibility this study was conducted at washington university school of medicine ( human research protection ofce #201801112 )  . 
the panel was a targeted sequencing assay that evaluated 40 genes and gene hotspots that are recurrently mutated in myeloid malignancies ( data supplement ) .25 for each patient who was found to have a denitive diagnosis of aml , a survey was sent to the treating physician . 
patients with acute promyelocytic leukemia ( m3 aml subtype ) were excluded.26 the treating physician was asked to complete a ninequestion survey to determine how the physician used the panel to inform treatment decisions ( data supplement )  . panel design and processing the panel uses an amplicon capture - based enrichment with unique molecular identiers for ultra - high variant sensitivity that targets an approximately 98 - kb space ( haloplex target enrichment system ; agilent technologies , santa clara , ca )  . 
this included evaluating bone marrow morphology , standard panels of ow cytometric markers , and a panel of routine cytogenetic and molecular marker studies , including uorescence in situ hybridization probes . target enrichment , variant calling strategies , and variant annotation methods are described in the data supplement . the median number of failed genes across all reports was two ( range , 0 to 24 genes )  . 
wt1 ( n = 211 cases ) , cux1 ( n = 197 cases ) , and cebpa ( n = 111 cases ) were genes that most frequently failed coverage requirements . 
if physicians did not respond to the initial contact , reminders were provided to increase the response rate . ethics , consent , permissions , and consent to publish this study was conducted at washington university school of medicine and was approved by the washington university human research protection ofce ( #201801112 )  . 
summary of patient , report , and physician characteristics characteristic ( n = 109 ) value median time from accessioning to report sign out , daysa 12 ( 4 - 36 ) patient ( n = 109 ) median age , years male female report ( n = 122 ) physician ( n = 14 ) mean time in practice , yearsb academic rank professor associate professor assistant professor degree type md / phd md / mba male female there were 124 reports from patients with aml . 
the reports from patients with aml , after removing patients with apl subtype ( n = 122 samples ) , were derived from 109 unique patients who were under the care of 14 physicians ( table 1 )  . 
only 13 samples had no observed variants , eight of which were acquired from patients who were determined to be in clinical remission using bone marrow biopsy . reports were ordered at various points in the disease course . 
the next most common timepoint was during disease assessment ( n = 28 of 122 ; [ 22.9% ] ) , followed by potential relapse ( n = 19 of 122 [ 15.6% ] ; fig 3a )  . 
for reports ordered during disease response assessments , seven were ordered post - induction , six were ordered after allogeneic hematopoietic cell transplant ( allohct ) , ve were ordered during ongoing treatment with a hypomethylating agent , two were ordered after consolidation with high - dose ara - c , and seven were ordered during or after salvage therapy ( fig 3b )  . 
on the basis of these data , the sequencing report was a factor in determining therapy decisions in 50 ( 43.8% ) of 114 cases ( fig 4a )  . 
the patient accepted the treatment plan 93% of the time ( n = 38 of 41 cases )  . predictive inuences in 35 of 50 reports , physicians indicated that they recommended at least one therapy on the basis of the variants identied by the sequencing panel ( fig 4b )  . 
on the basis of results35 reports with 38 corresequencing panel sponding inuencesphysicians reported recommending a hypomethylating agent in 14 patients for a tp5320 or tet228 , 29 variant , kinase inhibitors ( midostaurin or gilteritinib ) in 12 patients with a flt3 variant30 and one patient with a kit variant , 31 and idh1 / idh2 inhibitors were recommended for eight patients.32 there were three patients for whom a clinical trial was recommended on the basis of observed variants or persistent disease . 65 ( 23 - 90 ) 58 ( 53.2 ) 51 ( 46.8 ) 22 ( 8 - 44 ) 5 ( 36 ) 4 ( 29 ) 5 ( 36 ) 8 ( 57 ) 5 ( 36 ) 1 ( 7 ) 11 ( 79 ) 3 ( 21 ) note . 
of cases ( n = 122 ) flt3 internal tandem duplication splice acceptor variant frameshift variant missense variant flt3 tyrosine kinase domain splice donor variant inframe insertion negative no flt3 variant flt3 status stop gained variant type inframe deletion percentage of cases fig 2 . 
in 16 of 29 eligible cases ( two patients refused treatment ) , physicians reported the following inuences : 12 used the ngs panel to prescribe an flt3 inhibitor and four inuences were independent of flt3 status . 
in three of these four cases , patients had an flt3 inhibitor prescribed based on a previously known result from a different genetic test . there were 13 cases in which the patient had an flt3 variant , but the physician reported no inuence . 
of these 13 cases , three patients died before treatment initiation and eight had an flt3 inhibitor prescribed based on a previously known result from a different genetic test ( data supplement )  . risk stratication for transplant in first clinical remission physicians identied 10 reports that inuenced patient risk assessment and allohct recommendation ( fig 4b )  . specically , allohct was not recommended in rst complete remission in six patients , based on the presence of bialleleic cebpa variants ( n = 2 ) , kit variant status ( n = 1 ) , lack of high - risk variants ( n = 1 ) , or differential clearance of co - occurring variants after induction therapy ( n = 1 )  . 
for the latter patient , three variants were detected at diagnosis ( dnmt3a [ vaf = 42% ] , npm1 [ vaf = 38% ] , and rad21 [ vaf = 43% ] )  . 
these recommendations were based on tp53 variant status ( n = 2 ) , dnmt3a variant status ( n = 1 ) , and co - occurrence of multiple variants ( dnmt3a , npm1 , and flt3 internal tandem duplication ; n = 1 ) .14 assessment for pmd there were eight cases in which the sequencing panel was used to assess for pmd ( fig 4b )  . 
in ve cases , the physician indicated that the reports conrmed relapse / progression of aml , including one case of bone marrow negative , extramedullary relapse in the esophagus ( fig 5d )  . there were three patients who were being assessed for pmd while in an apparent clinical remission . 
two of the three patients did not show persistent aml via pmd assessment . the third patient showed three residual variants at low vaf ( cebpa [ vaf = 4% ] , smc1a [ vaf = 4% ] , and wt1 [ vaf = 3% ] ) , suggesting persistent disease . patients with no change in treatment regimens in response to sequencing panels there were 64 cases for which the physician noted no change in therapeutic plan on the basis of the report . 
the total number of eligible surveys completed by each physician and the total number of cases where the physician changed his or her plan is shown in figure 4c . the sequencing panel reports the vaf and thus can detect possible inherited variants . 
one patient was found to have a gata2 variant observed at a vaf of 52% , indicative of a possible germline variant , which prompted an action by the treating physician . 
a subsequent skin biopsy determined that the patient did not have a germline predisposition for disease . multiple sequencing panels for longitudinal disease monitoring and response therapy , there were 12 patients for whom the treating physician ordered multiple reporters during the disease course21 ( fig 5 and data supplement )  . 
after induction , despite some variants demonthe idh2 vaf of strating response to initial 39% ( 46% at diagnosis ) resulted in initiation of enasidenib . figure 5b shows a patient for whom the physician obtained three sequencing panels for longitudinal pmd monitoring . the rst report was ordered at relapse post - transplant and showed ve variants . 
a month later , the third report showed the re - emergence of three variants despite no excess blasts on the bone marrow biopsy , which resulted in a second allohct . 
figure 5c shows how a physician used sequential reports to observe the patients molecular response to a donor lymphocyte infusion and gilteritinib . figure 5d shows how the reports diagnosed extramedullary relapse in a patient with negative bone marrow biopsy ndings . 
the extramedullary disease showed the presence of some original variants ( nf1 and ezh2 ) , loss of other variants ( dnmt3a ) , and three novel variants ( cux1 , ptpn11 , and wt1 ) , some of which had clinical implications.34 , 35 additional cases with multiple reports are provided in the data supplement . reimbursement and clinical care access one of the biggest challenges for the widespread clinical implementation of ngs - based diagnostics has been inconsistent reimbursement from payers . 
coverage and reimbursement for myeloseq was divided into inpatient testing ( 26% ) and outpatient testing ( 74% ) , and 90% of outpatient testing was reimbursed across all payers . 
of these 124 cases , four were excluded ( acute promyelocytic leukemia [ apl ] subtype [ n = 2 ] ; no survey returned [ n = 2 ] )  . 
in 64 cases , physicians reported that the results did not inform decision making . ( c ) there were 14 physicians who contributed at least one survey to this study . was no specic pattern in terms of the diagnosis of rejected claims ( data supplement )  . discussion this study reports our institutions experience using a targeted capture sequencing panel to inform clinical care in patients with aml . 
 a addition of targeted therapy after lack of response to induction therapy persistent molecular disease monitoring barnell et al cebpa k302e smc1a r96h wt1 a38gfs * 69 wt1 r370pfs * 15 ezh2 k400del nf1 t2507i dnmt3a w297s dnmt3a f755 * smc1a / cepba ( 4% ) wt1 ( 3% ) wt1 ( 0% ) ( itd ) cux1 g1328s ptpn11 a72v wt1 r370pfs * 15 ezh2 k400del nf1 t2507i flt3 status enasidenib treatment ( itd ) gilteritinib new diagnosis of aml ( d0 diagnosis ) 22% blasts ( bmbx ) post 7 + 3 induction ( d49 post - diagnosis ) 3% blasts ( bmbx ) relapse ( d360 sct ) 44% blasts ( bmbx ) remission ( d426 sct ) < 1% blasts ( bmbx ) disease assessment ( d475 sct ) 0% blasts ( bmbx ) persistent molecular disease monitoring post - dli molecular diagnosis of extramedullary relapse bone marrow esophagus asxl1 g646wfs * 12 idh2 r140q runx1 l112cfs * 10 srsf2 p95h stag2 r146 * flt3 status treatment bcor t1129pfs * 30 bcorl1 q459 * dnmt3a r882h tet2 s1448n u2af1 s34f flt3 status flt3 status treatment treatment ( itd ) ( itd ) gilteritinib flt3 status treatment relapsed aml ( 1 month post - dli ) 21% blasts ( bmbx ) relapsed aml ( 3 months post - dli ) 6% blasts ( bmbx ) bone marrow ( ~ 10 yr sct ) 1% blasts ( bmbx ) esophageal tissue ( ~10 yr sct ) 1% blasts ( bmbx ) fig 5 . 
 ( b ) physician reported that the observation of persistent molecular disease at 475 days ( d ) poststem - cell transplantation ( sct ) indicated the need for a second allogeneic stem - cell transplantation despite clinical remission ( 0% blasts on bone marrow biopsy [ bmbx ] )  . 
 ( d ) extramedullary relapse was conrmed by comparing sequencing results of the original tumor and the periesophageal lesion . diagnosis , during disease assessment , and / or at multiple timepoints during the disease course . this study suggests that physicians are increasingly relying on the evaluation of multiple co - occurring variants in parallel ; therefore , simultaneous analysis of these genes is necessary . 
furthermore , pmd monitoring after cytotoxic induction therapy and transplantation21 , 36 has prognostic value ; therefore , the vafs reported on the gene panel studied here were being used to supplement existing standard - of - care mechanisms for residual disease assessment . 
although it is clear that physicians are using this test to measure and assess pmd , this test was not designed for measurable residual disease testing , and the limit of detection is not within the european leukemianet guidelines for measurable residual disease assessment.15 , 37 the prognostic information provided by the detection of persistent variants , the optimal depth of clearance , and the required limit of detection are all areas of active investigation requiring additional study in prospective clinical trials . there were several limitations associated with this study . reports were evaluated over an 8 - month period at a single academic institution among physicians with experience interpreting genomic results . 
 targeted panel inuences decision making for patients with aml were returned contemporaneously and tests were ordered at different timepoints during the disease course ( fig 3 )  . whereas the proportion of cases with inuences was not signicantly different among timepoints ( data supplement ) , inuence types might be different between timepoints and should be evaluated further to understand the impact of disease timepoint on treatment decisions . 
finally , each physician had a varied number of patients ( range , one to 18 patients ) with a large range in the number of cases reported to be inuential ( 0% to 90% )  . 
larger longitudinal , multi - institutional studies are needed to better understand interphysician variability in incorporating genomic data into clinical decision making . this study evaluated reports from the rst 8 months after launch of the diagnostic . 
the physicians were also experienced in interpreting genomic data , having participated in large genomic trials , 20 , 21 , 38 - 41 with many of them being clinical investigators themselves . 
given that the inuence of genomic data varies on the basis of physicians experience with genomic data , 6 , 7 the results presented here might not extrapolate to institutions that are unfamiliar with ordering and interpreting sequencing - based diagnostics . the sequencing panel has several additional limitations . the use of a tumor - only panelthat is , lack of a germline or reference sequenceprevented variants from normal being denitively called somatic . 
in future studies , it will be important to ascertain from physicians if any aspect of the test or the molecular report is unclear , biased , or difcult to interpret . there are several outstanding questions in the eld that could be addressed using a test similar to the one described in this paper . 
the prognostic value of residual dnmt3a , tet2 , and asxl1 mutations after treatment is incompletely understood , 21 , 36 , 42 and the difference between a residual leukemic clone versus rising clonal hematopoiesis43 needs additional study . 
our group is currently conducting a prospective clinical ( clinicaltrials.gov identier : nct02178241 ) to address some of these outstanding questions . trial in summary , the results from this study suggest that variants and associated vafs are being integrated into clinical care to inuence therapy choices , stratify relapse risk , and measure persistent disease . 
barnell employment : geneoscopy stock and other ownership interests : geneoscopy patents , royalties , other intellectual property : inventor of intellectual property in start - up company ( geneoscopy ) travel , accommodations , expenses : geneoscopy kenneth f . 
newcomer employment : geneoscopy ( i ) stock and other ownership interests : geneoscopy ( i ) patents , royalties , other intellectual property : inventor of intellectual property owned by geneoscopy ( i ) zachary l . 
oh consulting or advisory role : incyte , novartis , blueprint medicines , celgene , kartos , cti biopharma corp , pharmaessentia , disc medicine , constellation pharmaceuticals research funding : incyte ( inst ) , gilead sciences ( inst ) , cti biopharma corp ( inst ) , kartos ( inst ) , celgene ( inst ) , sierra oncology ( inst ) , blueprint medicines ( inst ) , constellation pharmaceuticals ( inst ) john s . 
stockerl - goldstein stock and other ownership interests : abbott laboratories , abbvie consulting or advisory role : celgene research funding : glaxosmithkline , takeda , biolinerx , janssen other relationship : cellerant ravi vij consulting or advisory role : bristol myers squibb , celgene , janssen , sano , karyopharm therapeutics , takeda , genentech , abbvie , oncopeptides research funding : takeda , celgene , bristol myers squibb travel , accommodations , expenses : celgene , bristol myers squibb , sano , janssen , davaoncology , karyopharm therapeutics , amgen , takeda , abbvie amanda f . 
abboud stock and other ownership interests : abbvie ( i ) , abbott laboratories ( i ) , gilead sciences ( i ) , bristol myers squibb ( i ) , johnson & johnson ( i ) honoraria : cardinal health , dova pharmaceuticals , nkartatherapeutics , archer biosciences research funding : actinium pharmaceuticals , selvita ( inst ) , allovir ( inst ) , forty - seven ( inst ) armin ghobadi honoraria : kite pharma consulting or advisory role : kite pharma , celgene , amgen , wugen speakers bureau : kite pharma , amgen geoffrey l . 
schroeder consulting or advisory role : astellas pharma , dova pharmaceuticals , flatiron health , glaxosmithkline , incyte , partners therapeutics , partners therapeutics , pzer speakers bureau : abbvie , merck , takeda john f . 
dipersio stock and other ownership interests : magenta therapeutics , wugen honoraria : incyte consulting or advisory role : cellworks , rivervest , magenta therapeutics , incyte research funding : amphivena therapeutics ( inst ) , macrogenics ( inst ) , incyte ( inst ) , wugen ( inst ) , biolinerx ( inst ) , maxcyte ( inst ) , bigelow aerospace ( inst ) patents , royalties , other intellectual property : patents : cd7 and cd2 knockout for cart to cd7 and cdl ; duvelisib for treatment of cytokine release syndrome ; nt - 17 to enhance cart survival ; novel wu mobilizing compounds ( inst ) ; selection of impdh mutant stem cells ; ifn , upregulate mhcii for relapsed aml ; dextran - based molecules to detect car - t cells ; combining integrin inhibitor with chemokine binders , 016131 ; jak and calcineurin inhibition , solid organ transplant ; vla4 , gro - b ; triple combinationcxcr2 , vla - 4 , gro - b ; targeting ifnr / cscr3 in gvhd ; wu / slu compounds vla4 and cxcr2 ( inst ) travel , accommodations , expenses : incyte , macrogenics , magenta therapeutics mary c . 
duncavage stock and other ownership interests : p&v licensing consulting or advisory role : cofactor genomics , bristol myers squibb , eli lilly open payments link : 317379 timothy j . 
additional thanks are also given to the siteman cancer center and the barnesjewish hospital foundation . 11 : 11 , 2016 368 : 2059 - 2074 , 2013 129 : 424 - 447 , 2017 netw 15 : 926 - 957 , 2017 2017 314 : 811 - 822 , 2015 references ray t : survey of precision oncology programs nds agreement on testing , divergence in care delivery . 
precision oncology news , july 19 , 2019 : precisiononcologynews.com / cancer / survey - precision - oncology - programs - nds - agreement - testing - divergence - care - delivery stone rm , mandrekar sj , sanford bl , et al : midostaurin plus chemotherapy for acute myeloid leukemia with a flt3 mutation . 
n engl j med 377 : 454 - 464 , 2017 kim as , bartley an , bridge ja , et al : comparison of laboratory - developed tests and fda - approved assays for braf , egfr , and kras testing . 
jama oncol 4 : 838 - 841 , 2018 li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
bmc med inform decis mak 18 : 107 , 2018 chow - white p , ha d , laskin j : knowledge , attitudes , and values among physicians working with clinical genomics : a survey of medical oncologists . 
j genet couns 27 : 187 - 196 , 2018 gornick mc , ryan ka , scherer am , et al : interpretations of the term actionable when discussing genetic test results : what you mean is not what i heard . j genet couns 28 : 334 - 342 , 2019 statz cm , patterson se , mockus sm : barriers preventing the adoption of comprehensive cancer genomic proling in the clinic . 
au ch , wa a , ho dn , et al : clinical evaluation of panel testing by next - generation sequencing ( ngs ) for gene mutations in myeloid neoplasms . 
marcucci g , mr ozek k , ruppert as , et al : abnormal cytogenetics at date of morphologic complete remission predicts short overall and disease - free survival , and higher relapse rate in adult acute myeloid leukemia : results from cancer and leukemia group b study 8461 . 
chen y , cortes j , estrov z , et al : persistence of cytogenetic abnormalities at complete remission after induction in patients with acute myeloid leukemia : prognostic signicance and the potential role of allogeneic stem - cell transplantation . 
j clin oncol 29 : 2507 - 2513 , 2011 ivey a , hills rk , simpson ma , et al : assessment of minimal residual disease in standard - risk aml . 
loken mr , alonzo ta , pardo l , et al : residual disease detected by multidimensional ow cytometry signies high relapse risk in patients with de novo acute myeloid leukemia : a report from childrens oncology group . 
hou h - a , chou wc , lin li , et al : characterization of acute myeloid leukemia with ptpn11 mutation : the mutation is closely associated with npm1 mutation but 35 . 
gaidzik vi , schlenk rf , moschny s , et al : prognostic impact of wt1 mutations in cytogenetically normal acute myeloid leukemia : a study of the germaninversely related to flt3 / itd . 
blood 113 : 4505 - 4511 , 2009 jongen - lavrencic m , grob t , hanekamp d , et al : molecular minimal residual disease in acute myeloid leukemia . 
schuurhuis gj , heuser m , freeman s , et al : minimal / measurable residual disease in aml : a consensus document from the european leukemianet mrd working party . 
clinical diincluding disease status , was dened by board - certied agnosis , hematopathologists . the panel uses an amplicon capture - based enrichment with unique molecular identiers for ultra - high variant sensitivity that targets an approximately 98 - kg base pair space ( haloplex target enrichment system ; agilent technologies , santa clara , ca )  . 
the panel is generally ordered for one of the following conditions : aml , mds , cytopenia , clonal cytopenia of undetermined signicance , clonal hematopoiesis of indeterminate signicance , myeloproliferative neoplasm , or other myeloid disorders . 
this included evaluating bone marrow morphology , standard panels of ow cytometric markers , and a panel of routine cytogenetic and molecular marker studies , including uorescence in situ hybridization probes . target enrichment for the panel used a commercially available , targeted , next - generation sequencing approach ( haloplexhs ; agilent technologies )  . 
preparation consisted of enzymatic fragmentation ; strand - specic ligation of sequencing primers , sample indexes , 10 - bp degenerate molecular barcodes , and biotin tagging of single dna molecules ; rapid liquid - phase enrichment of target loci using paramagnetic streptavidin - coated beads ; and on - bead polymerase chain reaction amplication . 
sequencing was performed using the illumina miniseq sequencing platform ( target depth = 50 coverage )  . variant calling for the panel was performed using a computational pipeline that employs custom - built tools created at washington university . 
overall reads were required to exceed 1 , 000 , 000 total reads with more than 98% aligned . during this process , unique molecular identier sequences are added to the binary alignment map le . 
once aligned , a custom java - based tool collapsed reads into read families using customized gatk software ( mckenna a , et al : genome res 20 : 1297 - 1303 , 2010 )  . 
collapsed binary alignment maps were used with standard variant calling tools , including varscan2 ( koboldt dc , et al : genome res 22 : 568 - 576 , 2012 ) , platypus ( rimmer a , et al : nat genet 46 : 912 - 918 , 2014 ) , and pindel ( ye k , et al : bioinformatics 25 : 2865 - 2871 , 2009 )  . 
these programs detected single - nucleotide substitutions , insertions or deletions ( indels ) up to 10 bp , and flt3 internal tandem duplication insertions between 21 and 108 bp . 
initial variant annotation was performed using the variant effect predictor tool ( mclaren w , et al : genome biol 17 ( 1 ) : 122 , 2016 )  . 
annotation was format le with variants augmented using a custom variant call identied in the aml the cancer genome atlas data set as well as variants observed in three published sequencing reports that evaluated patients with mds ( haferlach t , et al : leukemia 28 : 241 - 247 , 2014 ; papaemmanuil e , et al : blood 122 : 3616 - 3627 , quiz 3699 , 2013 ; walter mj , et al : leukemia 27 : 1275 - 1282 , 2013 )  . 
variant identication was subject to the following thresholds and cutoffs for reporting purposes : variants must be nonsynonymous , variants must have 2% minimum variant allele frequency and ve variant reads with support on each strand ( flt3 internal tandem duplication alleles require one read on each strand ) , amplicons must have at least ve reads assigned to it during consensus binary alignment map formation , and potential somatic variants must have 0.1% maximum population allele frequency ( max_af across all populations ; 1000 genomes [ v.phase3 ; 1000 genomes project consortium , et al : nature 526 : 6874 , 2015 ] and gnomad database [ v.170228 ; karczewski kj , et al : nature 581 : 434 - 443 , 2020 ] ) or presence in a custom mds / aml variant database . tier 1 ( variants with strong clinical signicance ) and tier 2 variants ( variants with potential clinical signicance ) , four ltered variants ( ie , variant allele frequency , 2% ) , and variants of unknown signicance were manually reviewed for potential clinical relevance . 
newberg , phd3 ; meagan montesion , phd3 ; and peter mu - hsin chang , md , phd1 , 2 introduction salivary gland tumors comprise a rare group of neoplasms that arise from salivary ducts , most of which are benign.1 the parotid gland is the most frequently involved site and comprises more than 80% of salivary tumors.2 of the parotid tumors , approximately 75% are benign , whereas the remaining 25% are malignant.3 the most frequent subtype of malignant salivary gland cancer is mucoepidermoid carcinoma , followed by adenoid cystic carcinoma.4 salivary gland tumors have been linked to exposure to high ultraviolet radiation.5 salivary gland cancer has a poor prognosis ( 5 - year overall survival , 50% ) and a high propensity for recurrence.6 the mainstay of treatment of salivary gland cancers is surgery in patients with early and locally advanced disease.7 in metastatic or recurrent disease , consensus is lacking on the optimal regimen for systemic chemotherapy.8 the low prevalence of this disease precludes large - scale randomized trials , and current clinical data are mostly derived from small clinical studies . 
current data , although dated , support cisplatin , anthracyclines , uorouracil , and cyclophosphamide as active agents against salivary gland cancer.9 - 11 in general , response to chemotherapy is limited ( a review of response to chemotherapy was published by laurie and licitra , 12 with response rates mostly ranging from 10% to 30% ) , and chemotherapy is mostly for palliative control.8 , 12 experts have urged a coordinated effort for clinical trials to further elucidate the role of chemotherapy in this patient group , 12 but this proves to be difcult , owing to the rarity of this cancer . the success of epidermal growth factor receptor ( egfr ) inhibitors in head and neck cancers13 and lung cancers14 has sparked hope for the possibility of use in salivary gland tumors because egfr is sometimes upregulated in this disease group.15 however , attempts to use egfr inhibitors , such as getinib and cetuximab , have largely been disappointing , with limited response.16 , 17 multiple mechanisms have been proposed for the lack of response to egfr inhibition in salivary gland cancers.18 to gain additional insight into the egfr expression pattern in salivary gland cancers , the dna and protein status of more than 800 tumor samples were analyzed for egfr gene alteration and protein levels in a retrospective study.19 the study revealed a high frequency of egfr low prevalence of egfr gene protein expression , mutation , and , more interestingly , no occurrence of egfr gene amplication . this is signicantly different from studies of head and neck squamous cell carcinomas , in which the prevalence of egfr amplication has been reported to be 17%20 and was linked to worse clinical outcome . 
interestingly , studies in colorectal cancer have shown that egfr gene amplication is linked to better outcomes and response to cetuximab.21 , 22 conversely , egfr amplication is proposed as an intrinsic resistance mechanism in lung cancer , 23 although other studies report conicting results , demonstrating egfr amplication associated with better outcomes with tyrosine kinase inhibitors ( tkis ) in patients with advanced nonsmall - cell lung cancer.24 therefore , the exact role of egfr amplication in response to egfr inhibition therapy remains to be claried . in this case report , we describe an unusual patient with a salivary gland cancer , refractory to initial chemotherapy agents but demonstrating signicant response to afatinib , an egfr and human epidermal growth factor receptor 2 tki . 
 ( c ) a computed tomography scan was performed 3 months after starting afatinib , showing marked decrease in size of the tumor ( right )  . pathology studies conrmed the diagnosis of high - grade salivary ductal carcinoma with inltration to the nontumor portion of the parotid gland . 
copy number ( cn ) plot ( top ) and minor allele frequency plot ( bottom ) showing marked increase in copy number of epidermal growth factor receptor . after discussion with the patient , the decision was made to initiate a therapeutic regimen of the egfr inhibitor afatinib ( 40 mg , every other day )  . 
written informed consent for publication of this case report was obtained from the patient . discussion afatinib is a tki that irreversibly inhibits the human egfr and human epidermal growth factor receptor 2 kinases.26 it has proven clinical activity and is approved for treatment of nonsmall - cell lung cancer with mutant egfr27 ( as shown in the lux - lung 3 and lux - lung 6 trials )  . 
interestingly , afatinib showed signicant activity against tumors harboring the deletion of exon 19 in egfr , while lacking activity against the common l858r point mutation , 27 , 28 highlighting the differences in biology between different egfr mutation types.29 afatinib was shown to be effective in advanced head and neck cancers , with benet progression - free survival30 , 31 ; however , little data exist for afatinib in salivary gland cancers . although some subtypes of salivary gland tumors exhibit egfr overexpression , 15 it is generally established that egfr inhibitors such as cetuximab are ineffective against salivary gland tumors . 
mechanistically , egfr amplication has been linked to higher spatial density of the receptor and thus linked to heightened dimerization and signaling.32 interestingly , as described in a recent case report , a patient with triple - negative breast cancer with egfr amplication was also successfully treated with cetuximab.33 a recent study retrospectively investigated a subgroup of esophageal cancers with egfr amplication.34 although previous studies have failed to demonstrate efcacy of egfr inhibition in esophageal cancers , 35 this study demonstrated a high response rate ( objective response rate , 58% ; disease control rate , 100% ) in this patient population.34 the ndings in our case report are in line with the aforementioned studies , highlighting the prognostic value of egfr amplication with treatment with egfr inhibitors . 
our patient is unique in that egfr amplication is extremely rare in salivary gland tumors , 19 compared with higher prevalence in triple - negative breast cancer ( up to 92% ) 36 or in esophageal cancer ( 7% ) .37 these reports that egfr amplication may indicate a favorsuggest able response to egfr inhibitors , regardless of the tumor site . 
this highlights the importance of genetic proling of individual tumors to determine personalized treatment of patients . in conclusion , we report a patient with a high copy number of egfr who demonstrated good response to egfr inhibition therapy . 
newberg employment : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : im on a patent stemming from research in my graduate school days related to identifying location biomarkers using imaging techniques . 
head neck surg 8 : 177 - 184 , 1986 liu y , li h , qin l , et al : prognostic factors in malignant sublingual salivary gland tumors . 
j oral maxillofac surg 75 : 1542 - 1548 , 2017 spitz mr , sider jg , newell gr , et al : incidence of salivary gland cancer in the united states relative to ultraviolet radiation exposure . 
head neck surg 10 : 305 - 308 , 1988 johnston ml , huang sh , waldron jn , et al : salivary duct carcinoma : treatment , outcomes , and patterns of failure . 
head neck 38 : e820 - e826 , 2016 ( suppl 1 ) lewis ag , tong t , maghami e : diagnosis and management of malignant salivary gland tumors of the parotid gland . 
otolaryngol clin north am 49 : 343 - 380 , 2016 aleri s , granata r , bergamini c , et al : systemic therapy in metastatic salivary gland carcinomas : a pathology - driven paradigm ? oral oncol 66 : 58 - 63 , 2017 licitra l , cavina r , grandi c , et al : cisplatin , doxorubicin and cyclophosphamide in advanced salivary gland carcinoma . 
proc natl sci counc repub china b 25 : 90 - 96 , 2001 jakob ja , kies ms , glisson bs , et al : phase ii study of getinib in patients with advanced salivary gland cancers . 
chen z , chen j , gu y , et al : aberrantly activated areg - egfr signaling is required for the growth and survival of crtc1 - maml2 fusion - positive mucoepidermoid carcinoma cells . 
temam s , kawaguchi h , el - naggar ak , et al : epidermal growth factor receptor copy number alterations correlate with poor clinical outcome in patients with head and neck squamous cancer . 
hirsch fr , herbst rs , olsen c , et al : increased egfr gene copy number detected by uorescent in situ hybridization predicts outcome in non - small - cell lung cancer patients treated with cetuximab and chemotherapy . 
nukaga s , yasuda h , tsuchihara k , et al : amplication of egfr wild - type alleles in non - small cell lung cancer cells confers acquired resistance to mutationselective egfr tyrosine kinase inhibitors . 
cappuzzo f , hirsch fr , rossi e , et al : epidermal growth factor receptor gene and protein and getinib sensitivity in non - small - cell lung cancer . 
sk alov a a , vanecek t , sima r , et al : mammary analogue secretory carcinoma of salivary glands , containing the etv6 - ntrk3 fusion gene : a hitherto undescribed salivary gland tumor entity . 
solca f , dahl g , zoephel a , et al : target binding properties and cellular activity of afatinib ( bibw 2992 ) , an irreversible erbb family blocker . 
yang jc , wu yl , schuler m , et al : afatinib versus cisplatin - based chemotherapy for egfr mutation - positive lung adenocarcinoma ( lux - lung 3 and lux - lung 6 ) : analysis of overall survival data from two randomised , phase 3 trials . 
kato t , yoshioka h , okamoto i , et al : afatinib versus cisplatin plus pemetrexed in japanese patients with advanced non - small cell lung cancer harboring activating egfr mutations : subgroup analysis of lux - lung 3 . 
kaneda t , yoshioka h , tamiya m , et al : differential efcacy of cisplatin plus pemetrexed between l858r and del - 19 in advanced egfr - mutant non - squamous non - small cell lung cancer . 
machiels jp , haddad ri , fayette j , et al : afatinib versus methotrexate as second - line treatment in patients with recurrent or metastatic squamous - cell carcinoma of the head and neck progressing on or after platinum - based therapy ( lux - head & neck 1 ) : an open - label , randomised phase 3 trial . 
clement pm , gauler t , machiels jp , et al : afatinib versus methotrexate in older patients with second - line recurrent and / or metastatic head and neck squamous cell carcinoma : subgroup analysis of the lux - head & neck 1 trial . 
suntharalingam m , winter k , ilson d , et al : effect of the addition of cetuximab to paclitaxel , cisplatin , and radiation therapy for patients with esophageal cancer : the nrg oncology rtog 0436 phase 3 randomized clinical trial . 
 parents , health care professionals , and scientists experiences of a precision medicine pilot trial for patients with high - risk childhood cancer : a qualitative study janine vetsch , phd1 , 2 ; claire e . 
ziegler , md , phd1 , 2 purpose children with high - risk cancers have low survival rates because current treatment options are limited . precision medicine trials are designed to offer patients individualized treatment recommendations , potentially improving their clinical outcomes . 
therefore , we wanted to gain an in - depth understanding of the experiences of all stakeholders involved in a new precision medicine pilot trial called target , including parents , their childs hcps , and the scientists who conducted the laboratory research and generated the data used to make treatment recommendations . methods we conducted semistructured interviews with all participants and analyzed the interviews thematically . results we interviewed 15 parents ( 9 mothers ; 66.7% bereaved ) , 17 hcps , and 16 scientists . 
we identied the following themes in parents interviews : minimal understanding and need for more information , hope as a driver of participation , challenges around biopsies , timing , and drug access , and few regrets . 
 vetsch et al context key objective what are the experiences of parents , health care professionals , and scientists participating in a precision medicine pilot trial for patients with high - risk childhood cancer ? knowledge generated parents had a minimal understanding of the trial aims . 
health care professionals and scientists embraced new technologies and collaborations but faced challenges managing families expectations , timing of testing , and drug access . relevance educating families will help them to better understand the potential benets and limitations of precision medicine trials , increase satisfaction with their childs care , and ameliorate additional long - term psychosocial burden for families already impacted by high - risk childhood cancer . 
health care professionals and scientists will also benet from further educational support so that they can prepare for the challenges of the rapidly emerging eld of precision medicine . typically securing responsible informed consent.15 previous studies suggested that poorer understanding is associated with lower socioeconomic status and having an ethnic background.6 some hcps have difculty explaining the purpose of experimental trials , which highlights the importance of ensuring that consent discussions are appropriate for parents with different educational backgrounds , languages , and cultural contexts.6 , 16 , 17 despite the fact that some hcps are concerned that parents understanding of clinical trials may be limited , hcps often share parents therapeutic optimism.17 hcps may nd it difcult to manage families expectations , including maintaining hope , while the likelihood of cure.11 , 18 for being realistic about scientists , precision medicine trials can be challenging because they represent a new way of conducting research , including adding a sense of accountability to families who are awaiting results . 
to our knowledge , scientists experiences of working on a precision medicine trial have not been assessed previously . the psychosocial with childhood cancer precision medicine trials being implemented worldwide , implications for families , hcps , and scientists need to be explored in depth . 
although some studies have examined the impact of pediatric genetic testing on families and hcps , 19 no studies have assessed the experiences of parents , hcps , and scientists participating in a precision medicine trial for patients with high - risk childhood cancer . 
therefore , we aimed to explore the experiences of parents , hcps , and scientists participating in the target study . methods participants the following three participant groups were eligible : parents ( including bereaved parents ) , hcps , and scientists . 
when families enrolled in target , they were informed that the primary objective of the trial was to assess the feasibility of a new precision medicine protocol and that personalized therapies ( if identied ) might not benet their child . 
with study progression and the establishment of the platform , results of actionable ndings were fed back to families . parents were eligible for this qualitative study if their child was enrolled in target , they provided informed consent , and they could speak conversational english . 
treating oncologists assessed all potential families for eligibility and excluded patients who were deemed to be experiencing severe mental health difculties or other conditions that may have impacted their study participation . hcps were eligible if they had been involved in the care of any target patient . 
we audio - recorded and transcribed the interviews with participants permission ( the average length of interviews was 35 minutes for parent , 27 minutes for hcps , and 31 minutes for scientists )  . 
we interviewed hcps and scientists to gain an understanding of their professional and personal experiences with target ( data supplement )  . we collected demographic data including age , sex , and education level from all participants . 
we collected clinical data from the target database ( table 1 )  . data analysis we used descriptive statistics to summarize participants demographic information using spss v25 ( ibm , armonk , ny )  . 
most children enrolled in target had a cns tumor ( seven families ) , and parents were , on average , 3.3 years from their childs initial cancer diagnosis at the time of the interview . 
numbers do not always add up as a result of missing values . abbreviation : sd , standard deviation . * includes students and homemakers . parents experiences we identied several terviews ( table 3 )  . important themes in parents minimal understanding and need for more information . parents generally recalled signing the target consent forhowever , they commonly could not recall the study aims or what their childs enrollment in target involved . of the parents who could not recall signing the consent form , they expressed confusion about the difference between target and other trials their child had participated in because [ everything ] just bleeds into one ( bereaved mother , id010 )  . 
some parents were not sure whether an additional biopsy or tissue sample was taken for target . other parents spoke of the target drug , not understanding that target was an analysis platform and not one specic drug . 
parents described their the target capacity to understand information about study as impeded by stressit just ew over the top of our heads ( bereaved father , id015 )  . 
parents also desired developmentally tailored information for their child because most parents included their children in treatment decisions . however , other parents reported not wanting any additional study information because it was too overwhelming and reminded them that their child had a terminal illness . hope as a driver of participation in target . 
target offered a sense of control to parents with minimal options , allowing them to take some sort of control of the uncontrollable ( bereaved mother , id008 )  . 
some parents whose children died found solace in the idea that their participation in target might help future patients . challenges around biopsies , timing , and drug access . parents reported feeling challenged by several ( uncontrollable ) factors , including the need for additional biopsy and conicting priorities as a result of limited available tumor tissue . 
parents queried why biopsies were not obtained and stored at the time of their childs diagnosis , and they expressed hope that this process would be in place for future patients . 
one mother explained that there was 4 2019 by american society of clinical oncology competing priority between using the biopsy for research and exploring other treatment options interstate or overseas . 
at the same time , parents were often willing for their child to undergo as many biopsies as needed to enhance their childs treatment options and contribute to research ( including being willing to consent to an autopsy after their childs death )  . parents also described challenges around timing . 
some parents expressed regret that the study was not offered earlier , particularly when they received the results either when their child was too unwell to start a new treatment or after their child had died . 
as one mother explained , its very frustrating , but youve missed an opportunity to better understand the tumor and what could reduce it ( id008 )  . another challenge described by parents was accessing the drugs identied through testing and recommended by target . 
although some parents described willingness to pay for drug costs , they were commonly advised to access the drug through an open clinical trial so that outcomes could be monitored , but this sometimes further slowed access . 
hcps valued that target gave them potential access to additional therapies not likely to be considered without the testing platforhcps highly valued that they were able to offer individualized therapies and state - of - the - art care ( hcp , their site , assisting families to avoid traveling overseas to access experimental therapies . id020 ) at challenges managing expectations , unexpected ndings , and drug access . 
im trying to remember , i dont actually remember what they said the objectives were , to be honest . i believe that the other treatment was utilising drugs that were used for a different type of leukaemia that if an all can actually sometimes look like or it will mimic , so i think the hypothesis was that the aml drugs may actually prove to respond better for [ childs ] s type of all , the infant all , and the main goal of the study was to investigate that . i know that it focuses on studying the genetic makeup of the tumor and  . 
what sort of treatment can help address genetic makeup of the tumor that she has . how long had they had the results and if they had them sooner , why the hell didnt they say , weve got the results because my thing is that if they can somehow have them on their target treatments and radiation as quickly as possible , maybe theres going to be a better result . i would quite like to have seen that all laid out with some bubbles with some arrows . 
so i could at least understand visually how it was . i just think [ sharing results ] should be one - on - one ; i didnt need ve bereaved father people there . 
 , no more resections , no more other drugs , no more radiation so might as well [ participate ]  . we enrolled [ child ] to the program not because of anything but because it was the only option we had . the hope is helping out future families . 
would be awesome if we can bring any value to anybody else whos been going through what weve been through . some drug will [ help ] so thats how you live its really important to have as much data as possible . 
i think its really important for families to participate . i think it was keep our child alive as long as we can in the hope that bereaved mother there is still hope  . 
there is still hope , mother there is still hope . challenges involving biopsies , timing , and drug access i think it would be seriously helpful though for newly diagnosed families to make sure that we get the tumor from that rst surgery . even , you know , and i know theres limited resources available to look at tumors , but theres always ways to nd somebody else to look at tumors at a cost . 
themes with representative parent quotes ( continued ) theme and quotes precisely , because the sheer quantity of tests and biopsies and treatments and scans and everything they go through already is beyond comprehension . 
so , the idea of agreeing to research that has the potential to increase that or add additional invasive procedures or negative experiences , then that would be , for me , that would be my deal breaker . 
at that point i would say , no more . so i dont know what it is , why it takes 8 weeks , if thats just literally , you know , in practical terms , how long it takes to grow and run the tests or whether its just a case of if you have more people and resources , you could do all that faster . so i didnt appreciate when she came off that drug how quickly things would move from there . 
so that would be something i would be warning people about . it was only another probably 3 weeks after [ surgery ] , that the cancer came back again anyway ! so , yeah , poor bugger had his brain surgery for nothing . it would be awesome to have more trials , more trials in australia . where you dont have to sell the house , re - mortgage the house , to go to germany or go for america and pay the bills over there just to try and get yourself enrolled in a trial that might help . 
some hcps were concerned that oncologists did not have good connections with pharmaceutical companies , which might limit access to recommended drugs for their patients . scientists experiences we identied the following themes from interviews with scientists ( illustrative quotes are provided in table 5 )  . embracing new collaborations and knowledge . 
scientists valued new interdisciplinary collaborations with clinicians and being able to learn and generate new knowledge . scientists described feeling a connection to real patients and felt that their work was meaningful , with the potential for real - life impact on families . 
themes with representative hcp quotes theme and quotes embracing new technology and collaboration so for families , i found that its made a huge difference to be able to offer them the possibility of targeted therapy , knowing that we may not nd anything for their particular child , or their particular tumor , but its made it so that we can offer something where there may , have not been anything else to be able to be offered . i have got one patient with a relapsed tumor where having access to the target has allowed us to use different drugs and those different drugs have put the patient into remission . challenges drug access if you havent got contacts within the pharmaceutical industry then thats also very difcult so at the moment im trying to get access to a drug which i cant get access to in australia so i think thats also difcult because the patient now knows theres a potential target and we wont have anything that we can give . also turnaround timesso many patients are rapidly progressing  . 
we need to still be optimistic but realistic at the same time and maybe this could give them an excess of hope , maybe thats what i consider as a problem . this has the potential to give other options and even if it doesnt give other options for them it gives potential options for the future , and as a i said , the disadvantage is that even if you were offering  . 
so its hard to give consent . theyre hoping that their child will have the one - in - a million where you nd a cure , based on their genetics . 
but from what , more than that , the vast majority of kids we either nd something thats adjuvant , like can be added in , but may not be curative , and in some patients we havent found anything thats targetable and the disappointment that comes with that . 
i dont think is a fault of the study , but comes with the territory of what it is that youve found . unexpected ndings one family who had a germline mutation , so i think that is something unexpected and it just adds another level of complexity . 
scientists expressed that target was unique compared with other studies they had worked on because of the potential for this personal psychological impact . discussion we found that many parents could not recall the specic aims of target and that hope commonly motivated participation . 
most parents desired additional , more accessible , written information about the study and valued regular updates from the treating physician . despite reporting challenges , parents did not regret participating in target . 
with this opportunity , i can interact into bigger communities across different research groups and also with some research clinicians from sydney childrens hospital . it was good , it was a really good learning experience to get a knowledge base and foundational skills in personalized medicine and research . its so rewarding doing what we do and nding things , i get a kick out of nding things that were missed by every other test before it . finding things that youd never think to look for , i think thats cool . . 
. conversely , when we get the biopsies , not getting enough sample . and we get blamed for that , and its like well were not the one that got the sample . there had been a few instances where patients had passed away and there would be an email sent out to everybody and seeingwhen you work in this sort of industry or this sort of workand you see the same names pop up , youll notice that sometimes therell be a positive reaction to treatment and its noted somewhere , but then a few months down the track , you see the names pop up again and youd be like , this persons obviously gotten worse again . there was an expectation that we would have [ the testing platform ] set up very rapidly , so that was a particular challenge to try meet those expectations and manage those expectations . 
that was quite tricky at times . drug access we always hope that something might come up but just sometimes you do get that type of result and theres nothing we can do to help with the kids and we dont  . 
scientists were challenged by time pressure and a new sense of responsibility to families , but at the same time , they valued this new connection with patients . echoing previous studies examining parents understandings of genomic tumor proling and experimental trials , 8 , 21 , 22 parents understanding of target was low . 
our results conrm that parents of children participating in clinical trials may experience therapeutic optimism.22 there is some evidence that ( potentially unrealistic ) optimism for a personal benet might be positively associated with patients mental health status throughout treatment23 ; however , long - term outcomes are unclear . 
echoing recent studies , some parents participation had a dual purpose , hoping for a benet for their child and for future patients.21 , 24 ensuring that families can make informed decisions about precision medicine will be critical for its integration into routine clinical care . 
hcps in our study reported challenges managing families expectations and avoiding false hope . the primary goal of this precision medicine trial , similar to other trials , was to benet future patients and research , with only a small proportion of current patients likely to gain medical benet.25 , 26 there is evidence that low literacy or educational attainment is associated with poorer understanding of precision medicine6 , 8 , 21 and may be more common in ethnic or racial minority groups , 6 highlighting the importance of easily understandable resources in different languages potentially supported with infographics or owcharts of trial steps.8 clinicians could consider providing families with information about the study multiple times over the course of treatment as well as offering multiple opportunities to have discussions with their treating team . although emerging literature has reected on the implications of cross - disciplinary processes inherent to precision medicine ( eg , sharing of big data sets between clinicians and researchers , the coming together of laboratories and clinics ) , 27 the experience of different stakeholders has received little attention . 
with more precision medicine trials being implemented worldwide , biopsy at diagnosis for up - front next - generation sequencing analysis will likely become standard of care for future patients with childhood cancer.28 timing was also challenging for scientists when children died before analysis of their data was completed . 
scientists should be given the opportunity to debrief and discuss their emotional reactions within the study team . a study strength was the inclusion of multiple stakeholders . parents response rate was moderate ; however , many parents were recently bereaved and were perhaps not yet ready to share their experience . 
we recruited participants from one hospital and only included english - speaking parents , which limits the generalizability of our results . participating hcps were highly interested in precision medicine , potentially limiting the generalizability of our hcp ndings . 
in addition , the change in practice over the study course needs to be considered when interpreting our results . future larger prospective trials may want to assess stakeholders experiences over the course of a precision medicine trial . parents willingly enroll their children in cancer precision medicine trials to explore all avenues of potential treatment . however , they may overestimate the likely benet for their child . 
easy - to - understand educational resources in multiple languages explaining the main concepts of precision medicine trials are needed . parents expectations should be monitored by hcps throughout their trial participation . 
tucker travel , accommodations , expenses : astrazeneca uncompensated relationships : astrazenica david malkin consulting or advisory role : bayer no other potential conicts of interest were reported . acknowledgment we thank janice yung , lianne wong , jessica deng , julie van , josh weisel , and pirathat techakesari for their contribution to this research . references eur j cancer 65 : 91 - 101 , 2016 tannock if , hickman ja : limits to personalized cancer medicine . 
harris mh , dubois sg , glade bender jl , et al : multicenter feasibility study of tumor molecular proling to inform therapeutic decisions in advanced pediatric solid tumors : the individualized cancer therapy ( icat ) study . 
jama oncol 2 : 608 - 615 , 2016 lau l , byrne j , ekert pg , et al : pilot study of a comprehensive precision medicine platform for children with high - risk cancer . 
n engl j med 372 : 855 - 862 , 2015 cousino mk , zyzanski sj , yamokoski ad , et al : communicating and understanding the purpose of pediatric phase i cancer trials . 
j clin oncol 30 : 4367 - 4372 , 2012 alderfer ma , zelley k , lindell rb , et al : parent decision - making around the genetic testing of children for germline tp53 mutations . 
cancer 121 : 286 - 293 , 2015 oberg ja , ruiz j , ali - shaw t , et al : whole - genome and whole - exome sequencing in pediatric oncology : an assessment of parent and young adult patient knowledge , attitudes , and expectations . 
beranger a , bouazza n , de haut de sigy a , et al : parents and childrens comprehension and decision in a paediatric early phase oncology trial : a prospective study . 
kass n , taylor h , fogarty l , et al : purpose and benets of early phase cancer trials : what do oncologists say ? what do patients hear ? j empir res hum res 14 . 
estlin ej , cotterill s , pratt cb , et al : phase i trials in pediatric oncology : perceptions of pediatricians from the united kingdom childrens cancer study group and the pediatric oncology group . 
marron jm , cronin am , dubois sg , et al : duality of purpose : participant and parent understanding of the purpose of genomic tumor proling research among children and young adults with solid tumors . 
harttrampf ac , lacroix l , deloger m , et al : molecular screening for cancer treatment optimization ( moscato - 01 ) in pediatric patients : a single - institutional prospective molecular stratication trial . 
chang w , brohl as , patidar r , et al : multidimensional clinomics for precision therapy of children and adolescent young adults with relapsed and refractory cancer : a report from the center for cancer research . 
although several inhibitors have been created , duvelisib and idelalisib have moved far in the clinic1 ; in fact , the latter in combination with rituximab is an approved agent for treatment of relapsed / refractory cll.2 , 3 duvelisib targets the dand g - isoforms , whereas idelalisib inhibits only the d - isoform.1 hence , we hypothesized that these inhibitors may have similar effects in downstream target proteins . 
these observations were in circulating cells after duvelisib therapy ( ie , after peripheral blood lymphocytosis ) .6 idelalisib showed a similar phenomenon during phase i , single - agent investigations.7 to test our hypothesis , we evaluated these cll lymphocytes from the peripheral blood before and after idelalisib treatment . fifteen samples from five patients were assessed ( table 1 )  . 
all these patients with cll were previously untreated and enrolled in a dana - farber cancer institute clinical trial of upfront idelalisib for 2 months followed by the addition of ofatumumab . 
all received idelalisib 150 mg twice per day as a single agent during the time these samples were collected . rppa assays were performed from these samples to determine the protein expression of the bcl - 2 family . 
the bcl - 2 family proteins are mcl - 1 , bclxl , bcl - 2 , and bcl - 2 - a1 among the antiapoptotic members ; bax and bak ( multidomain proapoptotic members ) ; and bim , bid , puma , and bad.ps155 among the bh3 - only members . 
close to 300 proteins were included in the rppa assay , which included 10 members ( blue symbols ) of the bcl - 2 family ( figs 1a and 1b )  . 
the treatment duration at the time of measurement varied , starting as early as 15 days and as late as cycle 3 day 1 ( ie , 56 days )  . 
a volcano plot demonstrates that 40 proteins after 15 or 28 days ( post - treatment t1 ; fig 1a ) and 35 proteins after two cycles ( 56 days ) of idelalisib ( post - treatment t2 ; fig 1b ) were significantly modulated . 
brown varsha gandhi qingshan yang , prexy modi , anil korkut , and varsha gandhi , the university of texas md anderson cancer center , houston , tx ; stacey m . fernandes , john hanna , and jennifer r . 
primary cll cells from five patients were isolated fresh from peripheral blood samples before treatment ( baseline , designated as d0 [ day 0 ] ) and d15 ( t1 ) or d28 ( t1 ) and d56 ( t2 ) after the start of oral idelalisib 150 mg twice per day . 
reverse phase protein array was done after lysis of cells at md anderson cancer center . the assay contained 300 proteins.8 lysates were diluted and samples probed with antibodies and visualized by colorimetric reaction . 
relative protein levels for each sample were determined by interpolation of each dilution curve from the standard curve of the slide . all data were normalized to protein loading and transformed to a linear value . 
 ( a ) volcano plot of the fold change of protein and statistical significance between pretreatment and post - treatment t1 ( d15 and d28 after start of idelalisib therapy )  . 
 ( b ) volcano plot of the fold change of protein and statistical significance between pretreatment and post - treatment t2 ( ie , d56 after start of idelalisib treatment )  . 
among the four evaluated antiapoptotic proteins , bcl - 2 was consistently increased in all patient samples at every time point ( fig 1c )  . bcl - 2 - a1 and bcl - xl generally decreased but varied . 
among proapoptotic bh3 - only domain proteins , bid remained the same , but bim was consistently increased at both evaluation times ( p 5 .01 ; fig 1c )  . 
idelalisib therapy results in an increase in bcl - 2 and bim and a decrease in mcl - 1 protebar graph of three proteins that show significant changes . primary chronic lymphocytic leukemia cells from patients were isolated fresh from peripheral blood before and after therapy and subjected to reverse phase protein array analysis as described in figure 1 . 
 ( a ) changes in the level of bcl - 2 protein after idelalisib therapy ( t1 5 15 or 28 days and t2 5 56 days after treatment )  . 
as shown in figs 2a to 2c , bcl - 2 , mcl - 1 , and bim levels were modulated in every sample , which were similar to those obtained with duvelisib.6 in general , these data suggest that bcr pathway inhibition leads to high bcl - 2 and bim protein levels and a decline in mcl - 1 protein levels in cll cells , which was also previously reported with ibrutinib therapy.11 given that the bcr axis inhibitors do not induce overt apoptosis of cll cells , strategies to combine venetoclax with idelalisib , duvelisib , or ibrutinib should result in apoptosis and removal of cll cells from peripheral blood . 
relationships are self - held unless noted . i 5 immediate family member , inst 5 my institution . relationships may not relate to the subject matter of this manuscript . for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . the following represents disclosure information provided by authors of this manuscript . 
 prexy modi no relationship to disclose anil korkut stock and other ownership interests : vivoz biolabs ( i ) patents , royalties , other intellectual property : drug combinations for treatment of melanoma and other cancers , c . 
brown honoraria : janssen pharmaceuticals , abbvie consulting or advisory role : gilead sciences , pharmacyclics , janssen pharmaceuticals , roche , genentech , celgene , sun pharma , infinity pharmaceuticals , astrazeneca , redx pharma , astellas pharma , abbvie research funding : gilead sciences varsha gandhi research funding : gilead sciences acknowledgment supported in part by an md anderson cancer center support grant , a cll global research foundation alliance grant , and sponsored research agreement from gilead to v.g. 
yang q , modi p , newcomb t , et al : idelalisib : first - in - class pi3k delta inhibitor for the treatment of chronic lymphocytic leukemia , small lymphocytic leukemia , and follicular lymphoma . 
miller bw , przepiorka d , de claro ra , et al : fda approval : idelalisib monotherapy for the treatment of patients with follicular lymphoma and small lymphocytic lymphoma . 
herman se , gordon al , wagner aj , et al : phosphatidylinositol 3 - kinase - d inhibitor cal - 101 shows promising preclinical activity in chronic lymphocytic leukemia by antagonizing intrinsic and extrinsic cellular survival signals . 
hoellenriegel j , meadows sa , sivina m , et al : the phosphoinositide 39 - kinase delta inhibitor , cal - 101 , inhibits b - cell receptor signaling and chemokine networks in chronic lymphocytic leukemia . 
patel vm , balakrishnan k , douglas m , et al : duvelisib treatment is associated with altered expression of apoptotic regulators that helps in sensitization of chronic lymphocytic leukemia cells to venetoclax ( abt - 199 )  . 
brown jr , byrd jc , coutre se , et al : idelalisib , an inhibitor of phosphatidylinositol 3 - kinase p110d , for relapsed / refractory chronic lymphocytic leukemia . 
roberts aw , seymour jf , brown jr , et al : substantial susceptibility of chronic lymphocytic leukemia to bcl2 inhibition : results of a phase i study of navitoclax in patients with relapsed or refractory disease . 
ramkissoon , md , phd5 , 6 ; and malak abedalthaga , md7 this case study demonstrates that rst - line treatment of a neurotrophic receptor tyrosine kinase ( ntrk ) fusionpositive infantile glioblastoma with larotrectinib , an ntrk inhibitor ( ntrki ) , was a safe and effective way to achieve tumor regression in our patient . 
an 18 - month - old saudi arabian female presented with a history of right - sided weakness and partial seizures . brain magnetic resonance imaging ( mri ) revealed a large left frontal complex contrast - enhancing mass . craniotomy for gross total resection ( gtr ) was performed , and histologic pathologic analysis revealed a diagnosis of glioblastoma . 
follow - up mri was performed 8 weeks after larotrectinib treatment and showed signicant tumor regression , indicating a positive response to treatment with no reported adverse effects . this patient case highlights the importance of genomic proling for pediatric brain tumors to identify targetable alterations . 
mri showed a large , heterogeneous , complex left frontotemporal mass with internal cystic and necrotic changes with mass effect and a rightward midline shift with enhancing focus at the left posterior thalamic region ( 8 7 9 cm ; fig 1a )  . whole - spine imaging was unremarkable , and the patient underwent craniotomy for gtr . 
the patient recovered well from surgery with no neurologic decits . postoperative mri conrmed gtr but did note a small focus of nodular enhancement in the left insular cortex suggestive of residual tumor ( fig 1b )  . intermixed small neuropathologic analysis of resected tissues revealed features consistent with a high - grade glioma best classied as glioblastoma ( who grade iv )  . 
the neoplastic cells were diffusely immunopositive for vimentin ; were focally positive for s100 and synaptophysin ; showed retained nuclear staining for ini1 ; and were immunonegative for sma , ema , cd99 , cd31 , cd34 , and neun ( figs 2c to 2f )  . 
genomic proling of tumor tissue revealed the presence of an etv6 - ntrk3 fusion , which creates a novel chimeric oncoprotein that results in continuous activation of the ntrk3 kinase . 
the fusion encompassed exons 1 to 5 of etv6 and exons 14 to 20 of ntrk3 , which retains the kinase domain of ntrk3 ( fig 2g )  . as a result of the poor survival rates associated with the patients family declined chemoglioblastoma , therapy or radiation therapy despite extensive counseling on standard - of - care treatment . 
 ( b ) after total surgical resection , postgadolinium axial t1 - weighted mri demonstrated total resection of the left frontal mass . ( c ) at recurrence , postgadolinium axial t1 - weighted mri demonstrated newly appearing mass within the operative bed ( arrow ) showing intermediate diffusion signal with corresponding contrast enhancement indicating recurrent tumor . 
the patient has received continuous larotrectinib therapy since october 2019 and was scheduled for her 6 - month followup mri studies in april 2020 ; however , as a result of the global covid - 19 pandemic , the patients family has deferred further nonemergent hospital visits ( including followup mris ) until the self - isolation restrictions have been lifted . 
therefore , the patient was advanced to a digital clinic visit , where she was noted to be clinically stable and neurologically intact without any evidence of adverse events or toxicities to date . 
we obtained consent from the patients guardian to publish the patients presentation and related images . methods genomic proling next - generation sequencing was performed as previously described8 using the oncomine comprehensive assay v3 system ( thermo fisher scientic , waltham , ma )  . 
assays were performed using the ion s5 system and ion 540 chip ( thermo fisher )  . discussion primary brain tumors are a leading cause of cancer - related morbidity and mortality in children.9 high - grade gliomas ( hggs ) account for approximately 10% of pediatric brain tumors and are the second most common malignant cns tumor after medulloblastoma . 
the most frequent tumors are anaplastic astrocytoma ( who grade iii ) and glioblastoma ( who grade iv ) .10 glioblastoma occurs in both children and adults and is associated with a poor prognosis . 
 ( a ) sheet of highly cellular monomorphic round primitive cells with relative demarcation from adjacent brain tissue ( hematoxylin and eosin [ he ] ; original magnication , 20 )  . 
 ( b ) heterogeneous morphologic features of the neoplasm composed of focal areas of spindle cells arranged in small fascicles and primitive round cells in myxoid background with alternating hyperand hypocellularity ( he ; original magnication , 200 )  . ( c ) higher magnication of the primitive cells in the myxoid background ( he ; original magnication , 200 )  . 
 ( g ) schematic of etv6 - ntrk3 fusion detected in patients tumor . etv6 - ntrk3 5 14 for different n - terminal chemotherapy consisting of vincristine , carboplatin , and temozolomide.12 however , progression - free survival rates remain poor for these patients , highlighting the need for new therapeutic options , including small molecules and / or immunotherapy alone or in combination with chemotherapy regimens.13 although the etiology and genomic drivers of glioblastoma are diverse , 14 - 16 a common nding in pediatric hgg , especially infantile hggs , is the presence of fusions involving ntrk , alk , and ros1 , among others . 
trk fusion proteins are oncogenic drivers that have been reported in a wide range of adult and pediatric tumors that occur at high frequencies ( 90% ) in rare cancer types.17 , 18 gene fusions involving the kinase domain of each of the 3 neurotrophin receptors ( ntrk1 , ntrk2 , and ntrk3 ) fusion partners , were identied in 4% of diffuse intrinsic pontine gliomas and 10% of nonbrain stem ( nbs ) hggs . 
notably , in one study , 4 ( 40% ) of 10 nbs - hggs in children younger than 3 years old harbored an ntrk fusion gene . the high frequency of ntrk fusions in nbs - hggs from children age 3 years and the paucity of additional mutations in these tumors strongly suggest that the fusion genes are potent oncogenic drivers in early postnatal brain tumor development.19 ntrk fusions have been identied at low frequencies in lowgrade pediatric astrocytomas and adult glioblastomas.20 , 21 trk ligands ( commonly nerve growth factor for trka , brainderived growth factor or neurotrophin 4 for trkb , and neurotrophin 3 for trkc ) bind with high afnity to the extracellular domain of the trk receptor.22 , 23 this leads to receptor activation and the induction of signal transduction pathways involved in proliferation , differentiation , and survival ( eg , mapk , pi3k , and pkc pathways ) in both normal and neoplastic cells . the activity of the rst - generation trk - selective inhibitor larotrectinib in pediatric patients with tumors harboring ntrk fusions has been explored in clinical trials , including a phase i / ii trial in pediatric patients ( scout ; clinicaltrials.gov identier : nct02637687 ) and a phase ii trial involving adults and adolescents ( navigate ; clinicaltrials.gov identier : nct02576431 )  . 
larotrectinib is a potent and selective inhibitor of all 3 trks , producing potent and well - tolerated responses in adult and pediatric patients with ntrk - rearranged tumors , with sustained tumor regression in  . 
90% of infants , children , and adolescents with trk fusions at doses of 100 mg / m2 twice a day ( maximum , 100 mg per dose ) .1 - 7 the most common adverse events include mild elevations of liver enzyme levels , cytopenias , and vomiting . 
the high solubility of larotrectinib permit its use in liquid formulations in young patients unable to swallow capsules.5 , 24 increasingly , case reports in the literature demonstrate tolerance and clinical response to ntrki in pediatric patients with hgg , even after chemotherapy and radiation treatment.25 these patient cases highlight the need for clinical trials that assess the sustained durability of response to ntrki and whether these targeted therapies should be used as monotherapy agents or in combination with chemotherapy regimens . our patient case demonstrates that trk inhibitors can be integrated as a rst - line therapy for pediatric hggs harboring trk fusions . 
we also highlight the need for the integration of genomic proling in the routine histopathologic analyses of pediatric patients with malignant primary intracranial tumors to detect any genetic mutations that can be targeted with available therapies . 
bakhsh collection and assembly of data : musa alharbi , nahla ali mobark , malak abedalthaga data analysis and interpretation : musa alharbi , nahla ali mobark , fatmah a . 
ramkissoon employment : foundation medicine stock and other ownership interests : foundation medicine no other potential conicts of interest were reported . references bielack ss , cox mc , nathrath m , et al : rapid , complete and sustained tumour response to the trk inhibitor larotrectinib in an infant with recurrent , chemotherapy - refractory infantile brosarcoma carrying the characteristic etv6 - ntrk3 gene fusion . 
lancet oncol 19 : e187 , 2018 drilon a , laetsch tw , kummar s , et al : efcacy of larotrectinib in trk fusion - positive cancers in adults and children . 
n engl j med 378 : 731 - 739 , 2018 dubois sg , laetsch tw , federman n , et al : the use of neoadjuvant larotrectinib in the management of children with locally advanced trk fusion sarcomas . cancer 124 : 4241 - 4247 , 2018 laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
lancet oncol 19 : 705 - 714 , 2018 landman y , ilouze m , wein s , et al : rapid response to larotrectinib ( loxo - 101 ) in an adult chemotherapy - naive patient with advanced triple - negative secretory breast cancer expressing etv6 - ntrk3 fusion . 
espinoza jc , haley k , patel n , et al : outcome of young children with high - grade glioma treated with irradiation - avoiding intensive chemotherapy regimens : final report of the head start ii and iii trials . 
alharbi m , ali mobark n , almubarak l , et al : durable response to nivolumab in a pediatric patient with refractory glioblastoma and constitutional biallelic mismatch repair deciency . 
nat genet 46 : 444 - 450 , 2014 jones dt , hutter b , j ager n , et al : recurrent somatic alterations of fgfr1 and ntrk2 in pilocytic astrocytoma . 
ziegler ds , wong m , mayoh c , et al : brief report : potent clinical and radiological response to larotrectinib in trk fusion - driven high - grade glioma . 
 graft - versus - host diseasefree antitumoral signature after allogeneic donor lymphocyte injection identied by proteomics and systems biology xiaowen liu , phd1 , 2 ; zongliang yue , ms3 ; yimou cao , ms1 ; lauren taylor , md2 ; qing zhang , ms4 ; sung w . 
chen , phd3 ; huanmei wu , phd1 ; and sophie paczesny , md , phd2 purpose as a tumor immunotherapy , allogeneic hematopoietic cell transplantation with subsequent donor lymphocyte injection ( dli ) aims to induce the graft - versus - tumor ( gvt ) effect but often also leads to acute graftversus - host disease ( gvhd )  . 
our novel six - step systems biology analysis involved removing common proteins and gvhd - specic proteins , creating a protein - protein interaction network , calculating relevance and penalty scores , and visualizing candidate biomarkers in gene networks . 
we then performed a second proteomics experiment in a validation set of patients who experienced gvt without acute gvhd after dli for comparison with the proteome of patients before dli . 
an independent experiment with single - cell proling in tumor antigenactivated t cells from a patient with posthematopoietic cell transplantation relapse was performed . results the approach provided a list of 46 proteins in the training set , and 30 proteins in the validation set were associated with gvt without gvhd . 
finally , the single - cell proling in activated t cells found 43 of the 61 genes . novel markers , such as rpl23 , ilf2 , cd58 , and crtam , were identied and could be extended to other antitumoral responses . conclusion our multiomic analysis provides , to our knowledge , the rst human plasma signature for gvt without gvhd . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction allogeneic hematopoietic cell transplantation ( hct ) is one of the most effective forms of tumor immunotherapy available to date . 
the lymphocytes in the donor graft recognize and eliminate residual tumoral cells through the graft - versus - tumor ( gvt ) effect , and thus , donor lymphocyte injection ( dli ) often is used at the time of relapse post - hct to induce gvt . 
despite the correlation of gvt indirect evidence for a gvt reaction and gvhd , separate from gvhd has been reported in large cohorts of hct patients or when dli is administered to induce remission in hct patients who have experienced a relapse.1 , 2 gvt activity can be increased by targeted therapy , as has been shown with sorafenib in flt3 internal tandem duplicationmutant leukemia cells.3 the gvt effect is mediated by minor histocompatibility antigens ( mihags ) on recipient leukemic cells that are recognized by donor cd4 + and cd8 + t cells.4 mihags can mediate gvt without inducing gvhd if they are only expressed by the recipient hematopoietic cells ( ie , minor h antigen [ ha ] - 1 , ha - 2 , bcl2a1 , and hb - 1 ) .5 , 6 nonhistocompatibility antigen proteins expressed by tumor cells , called tumor - associated antigens ( survivin , wilms tumor 1 , proteinase 3 ) also can mediate gvt activity.7 cytokines ( ie , interleukin - 15 [ il - 15 ] ) 3 ; checkpoint proteins , such as pd - 1 / pd - l18 ; and t - cell trafcking modulators9 are other possible mediators of gvt . our study aim was to develop a proteomic signature to identify gvt without gvhd after allogeneic dli . 
we attempted to do so through plasma proteomics and systems biology analyses of patients in relapse after hct who received donor lymphocytes as immunotherapy . knowledge generated our novel six - step systems biology analysis involved the removal of common proteins and gvhd - specic proteins , creation of a protein - protein interaction network , calculation of relevance and penalty scores , and visualization of candidate biomarkers in gene networks to dene a unique , biologically relevant 61 - protein signature of gvhd - free gvt . 
forty - three of the 61 genes also were found in an independent experiment using massive single - cell proling of tumor antigenactivated t cells from a patient who experienced post - hct relapse . relevance this multiomic analysis provides the rst human plasma signature for gvhd - free gvt to our knowledge . 
risk stratication on the basis of the gvt without gvhd protein signature would allow for customized treatment plans after hct . of 61 proteins that are signicantly expressed in the plasma of hct patients who received dli for tumor relapse . 
the methodology for this study is described in the data supplement . results plasma proteomics of gvhd - free gvt in a training set our initial approach to identifying gvt - specic biomarkers was to undertake a proteomics analysis . 
we reasoned that the best setting to observe a gvt effect without any effect of chemotherapy or preparative conditioning regimen would be after dli is given for relapse of malignant disease . 
our rst proteomics experiment ( ipas01 ) was designed to distinguish proteomes that predict gvhd - free gvt from those that predict gvt with gvhd after dli in a training set . 
we compared a pool of plasma samples taken approximately 30 days after dli from ve patients without relapse and without gvhd ( gvt - positive , gvhd - negative ) labeled with the heavy isotope and compared them with a pool of plasma samples at matched time points from 11 patients without relapse but with concomitant gvhd ( gvt - positive , gvhd - positive ) labeled with the light isotope ( fig 1 )  . 
no signicant differences between groups were observed for patient age , disease status ( all but one with morphologic relapse , and only one patient did not receive chemotherapy ) , dli donor type , and dli dose , and all patients were off immunosuppression . 
 gvhd - free antitumoral signature after donor lymphocyte injection gvt - positive , and gvhd - positive post - dli ( ipas - 01 ) gvt - positive , and gvhd - negative pre - dli ( ipas - 02 ) gvt - positive , and gvhd - negative post - dli ( ipas - 01 and - 02 ) isotopic labeling light isotopic labeling heavy immunodepletion six most abundant proteins acrylamide alkylation samples mixed fig 1 . 
the intact - protein analysis system ( ipas ) compared graft - versus ( gvt ) positive and graft - versus - host disease tumor ( gvhd ) negative postdonor lymphocyte injection ( dli ; heavy isotope ) with gvt - positive and gvhd - positive postdli ( light isotope ) samples in a training set ( ipas - 01 ) , and gvt - positive and gvhd - negative post - dli ( heavy isotope ) with gvt - positive and gvhd - negative pre - dli ( light isotope ) samples in a validation set ( ipas - 02 )  . anion - exchange chromatography ( n = 8 ) reversed - phase chromatography ( n = 60 ) liquid chromatography - ms / ms software tool ( data supplement )  . 
after this data processing , the ipas - 01 experiment provided a list of 46 proteins associated with a gvt signature without gvhd post - dli in the training set ( table 1 )  . 
although we started with ipas proteins with a heavy / light ratio greater than 1.2 , the systems biology process may have resulted in a nal score of less than 1 ; however , because all these proteins are gvt specic , they all are included in the nal gvhd - free gvt signature . 
the rst node is centered around cd8 ( cd8a ) and includes cd58 , il1a , ly75 , fas , and gpnmb and a secondary node centered around raf1 and containing guk1 , ephb4 , and cxcl12 . 
our data with the cd8a - centered node strongly suggest that gvt is majorly mediated by cd8 t cells and gvhd less so , which provides an opportunity to separate gvt and gvhd by manipulating these two t - cell subsets differently . 
as a proof of concept , we performed the experiment without applying these proteins to show that their nal scores have not been signicantly changed by the use of penalty scores ( table 1 ; data supplement )  . plasma proteomics of gvhd - free gvt in a validation set our second proteomics experiment ( ipas - 02 ) used a validation set that was designed to compare a pool of samples from ve gvt - positive , gvhd - negative ( labeled with the heavy isotope ) patients with a pool of samples from the same patients taken before dli when the patients were in relapse and thus gvt negative ( labeled with the light isotope ; fig 1 )  . 
a major cluster is constituted by centromere protein m ( cenpm ) , nup160 , wapal , dhx37 , stx7 , and il enhancer binding factor 2 ( ilf2 ) , which are all proteins implicated in the activation of cytotoxic t cells consistent with a gvt response ( table 2 )  . 
for example , cenpm ( also called pane1 ) is a known mihag expressed on b - lymphoid cells that is highly relevant to gvt - mediated post - dli.12 the protein encoded by ilf2 is a transcription factor needed for t - cell expression of il - 2.13 the second cluster is similar to the one found in ipas - 01 centered on map3k6 and dbnl . final 61 - protein gvhd - free gvt signature after dli the next step was to combine the proteins found in the training and validation sets . 
combined analysis of the two ipas experiments yielded 61 proteins : 49 with a nal combined score of greater than 1 and 12 with a nal combined score of less than 1 , all specic to gvt without gvhd ( table 1 )  . 
these include one similar to that seen in ipas - 01 centered on cd8a , one similar to that seen in ipas - 02 centered on cenpm - wapal and also containing dhx37 , and one found in both experiments and centered on map3k6 and dbnl . 
this additional cluster is centered around cse1l , which is a ras - related nuclear protein with a potential role in ras / raf / mapk signaling in t cells . 
some potential important novel markers , such as cytotoxic and regulatory t - cell molecule ( crtam ) , which has been shown to determine the cd4 + cytotoxic t - lymphocyte lineage , 14 are not part of a cluster . 
 ( a ) intact - protein analysis system ( ipas ) - 01 : geneterrain visualization shown in 2d for the graftversus - tumor ( gvt ) signature obtained by comparing gvt - positive , graft - versus - host disease ( gvhd ) negative with gvt - positive , gvhd - positive postdonor lymphocyte injection ( dli ) samples . 
a mean reads number of 381 , 079 per cell and median gene number of 1 , 091 per cell were analyzed for an average of 1 , 436 cells per condition . 
among the 61 genes identied in the proteomic gvhd - free gvt signature , 11 were more highly expressed in prame - specic t cells compared with cmvspecic t cells or nonreactive t cells . 
the expression prole of four representative gvt markers in the single - cell rna sequencing analysis of prame - specic t cells ( rpl23 , ilf2 , cd58 , and crtam ) is shown in figure 3 . 
rpl23 is a component of the 60s ribosomal subunit and has been shown to link the oncogenic ras signaling to p53 - mediated tumor suppression.15 t - cell responses to rpl23 also are increased in autoimmune diseases , 16 which suggests a role for the ras / raf / mapk pathway in t cells that is currently underexplored . 
the cd58 / cd2 axis is the primary costimulatory pathway for cd8 + t cells that lack cd28 , which suggests an alternate activation mechanism during gvt for exhausted t cells.17 crtam is upregulated in cd4 + and cd8 + t cells and encodes a type 1 transmembrane protein with v and c1 - like immunoglobulin domains.18 it has been shown to negatively regulate zeb1 ( zinc nger e - boxbinding homeobox 1 ) in t cells19 and to determine the cd4 + cytotoxic t - lymphocyte lineage , 14 and it might determine the cd8 + cytotoxic t - lymphocyte lineage as well . 
expression prole of four representative graft - versus - tumor ( gvt ) markers in single - cell rna sequencing analysis of prameand cytomegalovirus ( cmv ) pp65specic t cells . 
one systems biology novelty of our approach was the performance of a one - layer extension on ppi data using interactions one node away from the gene in the original list that are called outer genes . 
a strength of our approach is that we ltered out nonrelevant proteins using a penalty score , which led to a more - specic list of candidate proteins and avoided contaminants . 
this study favored a large - scale proteomics approach as opposed to a hypothesis - driven candidate approach.21 we have shown that for gvhd markers , this method is efcient in discovering new candidate markers.10 , 11 compared with our previous studies , we experimentally removed the gvhd proteins by assigning them the light isotope . 
of note , this approach showed that the proteins identied and their ratio have not been inuenced much by the implementation of penalty scores . in an independent experiment with single - cell proling of t cells from a patient with relapse after hct that were activated in vitro , 43 of the 61 proteomic genes also were found in activated t cells , which suggests that the proteins identied are biologically relevant in different antitumoral responses . the biology of the gvt markers not yet described is as follows . 
the function of trpc4ap ( transient receptor potential cation channel subfamily c member 4associated protein ) has been shown to be involved in the ubiquitination of e3 ligase skp222 and the activation of c - jun nh ( 2 ) terminal kinase and transcription factor ap - 1.23 guanylate kinase 1 ( guk1 ) is an enzyme that catalyzes the transfer of a phosphate group from atp to guanosine monophosphate ( gmp ) to form guanosine diphosphate ( gdp ) and is believed to be a good target for cancer chemotherapy.24 its expression on tumor - specic t cells was not previously reported . 
pin1 ( peptidylprolyl cis / trans isomerase , nimainteracting 1 ) catalyzes the cis / trans isomerization of peptidyl - prolyl peptide bonds and thus catalytically regulates the postphosphorylation conformation of its substrates and is involved in the regulation of t - cell biology . 
in particular , its implication has been shown in systemic lupus erythematosus and t - cell acute lymphoblastic leukemia progression.25 - 27 wapl cohesin release factor has been shown to restrict chromatin loop extension.28 of note , it was part of a microrna - mrna network in allogeneic t - cell responses.29 fermitin family member 3 ( fermt3 ) a member of the kindlins that mediates ppi involved in integrin activation . 
mutations in this gene cause the auadhesion deciency tosomal leukocyte syndrome - 3.30 its role in t cells has not been studied . cd160 is another surface protein tightly expressed on peripheral cytotoxic cd8 t lymphocytes and natural killer cells , 31 and soluble cd160 enhances cd8 + t cells , which results in increased interferon - , il - 2 , and tumor necrosis recessive factorsecretion as well as cytolysis against tumor cells in vitro and in vivo.32 not surprisingly , serglycin ( srgn ) , which serves as a mediator of granule - mediated apoptosis through the macromolecular complex of granzymes and perforin and determines the secretory granule repertoire of cytotoxic t lymphocytes , 33 was also upregulated in this study . 
the fas cell surface death receptor ( fas ) that plays a critical role in the activation of the death - inducing signaling complex with fas - associated death domain protein and triggers a downstream caspase cascade that leads to apoptosis34 also was upregulated . the chemokine cxcl12 has been proposed to be able to distinguish immune cells that induce gvt going to the bone marrow from immune cells that induce gvhd.35 it is one of the rare proteins for which the nal score was modied more than twice by the penalty score but is still included overall as a gvt proteseveral of the tripartite motif ( trim ) members encode for mihags.21 although trim42 , 22 , and 37 are located on chromosomes 3 , 11 , and 17 , respectively , trim39 is on chromosome 6 in the major histocompatability class i region and , in our study , showed global expression on activated t cells . 
raf1 is the cellular homolog of viral raf proto - oncogene ( v - raf ) and is also a map3k that functions downstream of the ras family of membrane - associated gtpases to which it binds directly . 
cse1l is a ras - related nuclear protein that binds strongly to nuclear localization signal - free importin - , and this complex is then released in the cytoplasm by the combined action of ranbp1 and rangap1 . 
one particular protein of nont - cell origin , il - 1 , was found to be elevated in the plasma of patients with gvt response and may play a signicant role in antitumor effects . 
of note , il - 1engineered tumor cells rarely develop into tumors , and if they do , the tumors are quickly destroyed through a mechanism that involves cd8 + t cells and natural killer cells , and il - 1 tumor immunoediting microenvironment.36 although our approach identied several proteins for gvhd - free gvt , there are limitations in this study . 
third , the systems biology pipeline relies on knowledge from the published domain , which makes the application of this method to diseases that have not been well studied , such as gvt , difcult . 
chen travel , accommodations , expenses : wuxi apptec sophie paczesny patents , royalties , other intellectual property : inventor on a patent entitled methods of detection of graft - versus - host disease ( us 20130115232a1 , wo 2013066369a3 ) no other potential conicts of interest were reported . acknowledgment the raw mass spectrometry data are publicly available at massive ( massive.ucsd.edu ) with the identication number msv000081057 . 
we thank gregory yanik , md , for providing the patient samples through a university of michigan - indiana university material transfer agreement . references ringd en o , labopin m , gorin nc , et al : is there a graft - versus - leukaemia effect in the absence of graft - versus - host disease in patients undergoing bone marrow transplantation for acute leukaemia ? br j haematol 111 : 1130 - 1137 , 2000 bar m , sandmaier bm , inamoto y , et al : donor lymphocyte infusion for relapsed hematological malignancies after allogeneic hematopoietic cell transplantation : prognostic relevance of the initial cd3 + t cell dose . 
mathew nr , baumgartner f , braun l , et al : sorafenib promotes graft - versus - leukemia activity in mice and humans through il - 15 production in flt3 - itdmutant leukemia cells . 
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leuk lymphoma 45 : 2229 - 2237 , 2004 koestner w , hapke m , herbst j , et al : pd - l1 blockade effectively restores strong graft - versus - leukemia effects without graft - versus - host disease after delayed adoptive transfer of t - cell receptor gene - engineered allogeneic cd8 + t cells . 
blood 117 : 1030 - 1041 , 2011 kim ym , sachs t , asavaroengchai w , et al : graft - versus - host disease can be separated from graft - versus - lymphoma effects by control of lymphocyte trafcking with fty720 . 
vander lugt mt , braun tm , hanash s , et al : st2 as a marker for risk of therapy - resistant graft - versus - host disease and death . 
brickner ag , evans am , mito jk , et al : the pane1 gene encodes a novel human minor histocompatibility antigen that is selectively expressed in b - lymphoid 13 . 
kao pn , chen l , brock g , et al : cloning and expression of cyclosporin aand fk506 - sensitive nuclear factor of activated t - cells : nf45 and nf90 . 
cancer res 76 : 5030 - 5039 , 2016 ito y , hashimoto m , hirota k , et al : detection of t cell responses to a ubiquitous cellular protein in autoimmune disease . 
leitner j , herndler - brandstetter d , zlabinger gj , et al : cd58 / cd2 is the primary costimulatory pathway in human cd28 - cd8 + t cells . 
yeh jh , sidhu ss , chan ac : regulation of a late phase of t cell polarity and effector functions by crtacell 132 : 846 - 859 , 2008 19 . 
bachireddy p , hainz u , rooney m , et al : reversal of in situ t - cell exhaustion during effective human antileukemia responses to donor lymphocyte infusion . blood 123 : 1412 - 1421 , 2014 21 . 
tissue antigens 81 : 183 - 193 , 2013 jamal a , swarnalatha m , sultana s , et al : the g1 phase e3 ubiquitin ligase truss that gets deregulated in human cancers is a novel substrate of the s - phase e3 ubiquitin ligase skp2 . 
soond sm , terry jl , riches dw : truss , a tumor necrosis factor receptor - 1 - interacting protein , activates c - jun nh ( 2 ) - terminal kinase and transcription factor ap - 1 . 
ruppert r , moser m , sperandio m , et al : kindlin - 3 - mediated integrin adhesion is dispensable for quiescent but essential for activated hematopoietic stem cells . j exp med 212 : 1415 - 1432 , 2015 31 . 
kotsiou e , davies jk : new ways to separate graft - versus - host disease and graft - versus - tumour effects after allogeneic haematopoietic stem cell transplantation . br j haematol 160 : 133 - 145 , 2013 36 . 
we identied , for the rst time , an epigenomic factor that can potentially complement dna mutation status in discriminating patients with lung adenocarcinoma who are less likely to benet from egfr - tki treatment , thereby leading to improved patient management in precision medicine . jco precis oncol 5 : 418 - 431 . 
inhibition of epidermal growth factor receptor ( egfr ) kinase activity by egfr - tyrosine kinase inhibitors ( tkis ) , such as erlotinib , getinib , and afatinib , was effective in patients with nsclc with egfr - activating mutations . however , despite the remarkable clinical success , the treatment efcacy was still limited to 50% - 80%.10 , 11 the sizable percentage of nonresponders ( 20% - 30% ) suggested intrinsic tki resistance and substantial heterogeneity among tumors , even among egfrmutant tumors , highlighting the need for reliable predictive biomarkers . the comprehensive molecular proling of pretreatment lung adenocarcinoma to identify inherently tkiresistant cases can aid the development of potential strategies to manage such cases . 
 dna methylation proling for egfr - tki responses context key objective a sizable portion ( 20% - 30% ) of patients with epidermal growth factor receptor ( egfr ) mutant nonsmall - cell lung cancer have no good initial clinical response to egfr - tyrosine kinase inhibitors ( tkis ) , and how to predict intrinsic drug resistance accurately is challenging . 
global dna methylation landscape of tumors from patients with lung adenocarcinoma before tki treatment was analyzed to investigate the association with egfr - tki responses . knowledge generated a total of 216 tki responseassociated methylated sites were identied , and functional analysis revealed the enrichment of homeobox genes . 
in particular , increased methylation of hoxb9 correlated with higher rate of intrinsic resistance ( ir ) to egfr - tki . relevance dna methylation provides a different dimension to complement the dna mutationbased markers for understanding the mechanism of ir . 
evaluation of the methylation level on hoxb9 may be incorporated in the management of lung adenocarcinoma to aid the prediction of egfr - tki response . egfr - tki14 suggest many dna - based biomarkers for ir prediction . 
on the other hand , tumor suppressor genes involved in the alternative mechanisms of ir may be inactivated by epigenetic mechanisms that result in phenotypic or functional changes.15 however , although studies have reported that epigenetic changes in tumor participate in the evolution of acquired drug resistance through regulating gene expression patterns , 16 epigenomic data associated with ir to tki are lacking . 
modication of methylation on dna is stable and abnormal methylation represents an early event for cancer diagnosis , making methylation aberrations equally suitable candidates for recurrence detection and prediction of patient survival.17 - 21 therefore , we undertook a genome - wide approach to investigate dna methylation patterns associated with ir to tki . dna methylation that occurs at cytosines of cpg dinucleotides , especially within cpg islands in the promoter region , can lock genes in off status , resulting in a transcriptionally silent state.22 , 23 although dna methylation is an important mechanism for maintaining normal development and cellular homeostasis , aberrant dna methylationmediated silencing of tumor suppressor genes has been reported to be associated with cell survival and progression in cancer.24 dna methylation proling of tumors , including those of glioma , acute myeloid leukemia , and colorectal and lung cancers , has aided the identication of cancer subtypes correlated with clinical outcomes.25 - 29 in this study , we aimed to identify epigenetic markers for predicting drug efcacy in patients with lung adenocarcinoma . 
we conducted genome - wide dna methylation proling of tumors from patients before their egfr - tki therapy and established a dna methylation landscape to elucidate the association of dna methylation with the egfr - tki response status of patients via a pipeline of statistical analysis , gene ontology ( go ) , and bioinformatics analysis . 
detailed accounts of sample collection and protocols for dna extraction , bisulte conversion , dna methylation analysis , pyrosequencing along with statistical analysis , bioinformatics analysis , and data availability are presented in the data supplement . results clinicopathologic features of the patients table 1 lists the clinicopathologic features of the two cohorts . 
the validation cohort consisted of 163 egfrmutant patients and the majority ( 85.28% ) were at stage iv . the tki response assessmentprogressive disease ( pd ) , stable disease ( sd ) , partial response ( pr ) , or complete response ( cr ) was determined according to the recist guidelines.30 the pd group , dened at the rst scan done at 8 weeks following the start of egfr - tki , is considered as patients with ir . 
using the top 5% coefcient of variation as the cutoff , 24 , 121 probes with the greatest variability were analyzed , and 391 probes were found correlated with egfr - tki response . 
the majority of the probes ( 203 ) had higher dna methylation in patients with a poor response than in those with a favorable response ; hypermethylation correlated with poor response . 
a global view of the dna methylation distribution contrasting the patients with pd against those with pr showed that all but 13 probes were located above the diagonal line , elucidating a clear pattern of methylation gain in patients with pd ( fig 2b - d )  . 
the tumors of patients who were more likely to be resistant to egfr - tkis tended to have higher pretreatment methylation levels . chromosomal context analysis of candidate cpg sites showed enrichment in cpg islands and gene promoter regions the cpg sites were assigned to the annotated categories according to their chromosome positions relative to the nearby transcription start sites and the closest cpg islands ( data supplement )  . 
we examined the changes in the proportion of each category during our probe selection and found an increasing trend in cpg islands and the gene promoter region tss1500 ( between 1 , 500 bp and 200 bp upstream of the transcription start site )  . 
for the 37 transcription - repressive sites , the enrichment pattern in cpg islands was retained and that in tss1500 was increased to 27.03% ( fig 2e )  . identication of transcription - repressive methylation sites we investigated the potential of the 216 methylation sites in cis - regulation of gene expression by correlating publicly accessible mrna gene expression data ( gse60644 ) with dna methylation data ( gse56044 ) in lung adenocarcinoma ( data supplement )  . 
a total of 37 sites were identied as transcription - repressive sites ( data supplement )  . functional enrichment analysis of transcript - linked methylation showed eight probes linked to tfs ( go : 0003677 ) , to evaluate the molecular function of the genes mapped by the 37 transcription - repressive sites , go enrichment analysis was conducted . 
furthermore , using animal transcription factor database ( animaltfdb ) , we found that eight of the 37 sites were annotated to ve tfs : ikzf1 , hoxb9 , sp8 , lass4 , and vax2 ( table 2 and data supplement )  . figure 2g shows the f statistic and the corresponding p value from analysis of variance for each of the eight sites , along with the location and chromosome context information . 
we found that seven of the eight tf - linked sites are located in the context of cpg islands and ve in the transcription start site ( tss ) region ( table 2 )  . 
the two vax2 methylation sites also showed a moderate ability to predict the egfr - tki response ( data supplement )  . we further performed stratication analysis by classifying patients as those with egfr - activating mutations and those increased methylation of hoxb9 without ( figs 3d - f )  . ( cg13643585 ) was observed in pd patients . 
for the egfr wild - type group , the or ( 7.59 ) was comparable , but the p value was .09 , likely because of the small sample size ( fig 3e )  . 
the data in table 3 conrmed the pattern of increased hoxb9 methylation in the egfr - tkiresistant ( pd ) group compared with the disease control group ( cr , pr , or sd )  . 
the pd group was ranked rst in each quartile , and the one - sided rank - sum test for between - group differences indicated a signicant difference ( p = .036 ) ( data supplement )  . in addition , analysis of the auroc showed that hoxb9 methylation statistically signicantly increased the predictive precision of egfr - tki resistance for the dcr ( table 3 )  . 
although signicant advances have been made in understanding acquired resistance ( ar ) , the causes of ir remain unclear.12 in addition to being classied as ar versus ir , resistance mechanisms can be classied in terms of on - target versus off - target , 31 suggesting the activation of collateral signaling . 
the patients characteristics , smoking behavior ( p1 ) , sex ( p2 ) , egfr status ( p3 ) , and egfr - tki response ( p4 ) , are shown by the bars at the top of the heatmap . 
for each cpg probe , the average beta value across patients with pd was plotted against that across patients with pr and is shown as a smooth kernel scatter plot . 
in the gradient scale , red represents the densest region , whereas purple represents the sparsest region ; pr ( red ) , sd ( yellow ) , and pd ( blue )  . 
the probe distributions in the cpg context and the gene context are shown on the left and right , respectively , for all probes in the array ( top ) , for the most variably methylated probes ( upper middle ) , for the tki responseassociated methylation sites ( lower middle ) , and for the transcription - repressive sites ( bottom )  . 
moreover , where genomic resistance has been found , epigenomic modulation has been proposed as the potential mechanism . changes in resistant phenotypes , including epithelialtransition ( emt ) and cancer stemness mesenchymal shift , have been found to be driven by epigenetic remodeling . 
tki - induced dna methylation changes have been reported in advanced egfr - mutated lung cancer.33 decitabine , the dna methyl transferase inhibitor , could reverse the sensitivity of egfr - tkiresistant nsclc cell line pc9 / gr through demethylation of rassf1a and gadd45.34 the combination of tkis with epigenetic drugs has shown in preclinical and clinical promise as a treatment studies.33 - 35 in this study , we conducted clinical oncological investigation on the potential role of dna methylation in mediating ir to egfr - tki treatment in patients with advanced lung adenocarcinoma . 
aberrant dna methylation is one of the most classical events that occurs during lung cancer development.36 many studies have shown altered methylation patterns in lung cancer , indicating roles of epigenetic biomarkers and therapeutic targets.37 - 39 earlier study by zhu et al40 focused on the methylation patterns of wnt antagonists , showing the association of methylated sfrp5 with shortened progression - free survival under egfr - tki treatment , but not with ir to tki . 
interestingly , two 428 2021 by american society of clinical oncology of those ve genes , axl1 and hoxa9 , are homeobox tfs . our pursuit of the primary egfr - tkiresistant methylation markers also identied enrichment of homeobox genes . among the 30 tki - associated methylation probes annotated to tfs , 11 accounted for nine homeobox genes ( data supplement )  . we identied and conrmed the correlation of hoxb9 dna methylation with an increased rate of ir to egfr - tkis . hoxb9 is involved in cell development and proliferation43 and is suggested to function as a tf that can induce the expression of emt genes and several angiogenic factors , such as vegf , il - 8 , and tgf , resulting in the activation of egfr and erbb2.44 - 46 egfr signaling is connected to the nf - b pathway , giving the role in ir or ar to egfr inhibitors.47 however , the molecular mechanisms by which hoxb9 contributes to carcinogenesis are debated.48 , 49 the overexpression of hoxb9 can suppress the akt / nf - b / snail pathway and inhibit the proliferation of gastric carcinoma cells.50 we analyzed the correlation between egfr signaling and nf - bdependent pathways ( gse60644 ) and found that expression of hoxb9 negatively associated with that of kiaa1199 ( cell migrationinducing hyaluronidase 1 ; data supplement )  . 
through protein - protein interaction ( ppi ) analysis , we found that hoxb9 might cross talk with both ir and ar to egfr - tki through ezh2 , sirt1 , and egr2 ( data supplement )  . 
therefore , regulation of hoxb9 is crucial in the cooperated oncogenic loops.12 our data suggested that hoxb9 hypermethylation may be a novel tumor cellular state that is useful for precise categorization of tumor heterogeneity in the study of intrinsic egfr - tki resistance via off - target effects such as redundant or compensating signaling . pattern was consistent between patients with egfr - activating mutations and patients with wild - type egfr , implying that the regulatory effect of dna methylation of hoxb9 may be independent of egfr activity . in addition , dna methylation changes can be accurately detected in tumors and liquid biopsies . 
such detection is promising for the development of biomarkers for cancer screening.51 dna methylation in distal regulatory sites , such as enhancer regions , plays important roles in gene regulation through the binding of cell typespecic tfs and interaction with promoters.52 - 54 we validated a dna methylation site in the enhancer region of hoxb9 that can help the prediction of nonresponse to egfr - tki . 
in cancer , aberrant dna methylation at enhancers couples with recruitment of coactivators or corepressors , forming networks of cancer - associated tfs and their targeted genes.55 - 57 stone et al58 dened hypermethylation enhancers that correlate with sensitivity to endocrine therapy , suggesting the impact of enhancer status on the drug treatment response . 
 dna methylation proling for egfr - tki responses the combination of genetic aberrations , gene expression , and dna methylation highlights the potential of the identied candidates in the development of biomarkers for tumor diagnosis or prognosis . 
in this study , with a focus on medical actionability , we discovered that hoxb9 methylation could be a biomarker useful for discriminating patients with tki resistance from those with tki sensitivity , especially patients whose tumors harbor egfr - activating mutations . 
although improving the sensitivity and specicity of hoxb9 methylation is recommended , our work provided a preliminary proof of concept on the usefulness of hoxb9 methylation for opening up more clinical options to manage lung adenocarcinoma . 
for example , in accordance with the current clinical standard of treating egfr - mutant patients with egfr - tki , for patients with hoxb9 hypermethylation , combination treatment such as egfr - tki plus antiangiogenic therapy59 or egfr - tki plus chemotherapy60 may be another option to overcome the resistance and improve the response rate . 
 acknowledgment the authors thank all the patients and research staff who participated in this work . su et al references siegel rl , miller kd , jemal a : cancer statistics , 2019 . 
mitsudomi t , morita s , yatabe y , et al : getinib versus cisplatin plus docetaxel in patients with non - small - cell lung cancer harbouring mutations of the epidermal growth factor receptor ( wjtog3405 ) : an open label , randomised phase 3 trial . 
lancet oncol 11 : 121 - 128 , 2010 zhou c , wu yl , chen g , et al : erlotinib versus chemotherapy as rst - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
lancet oncol 12 : 735 - 742 , 2011 rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutationpositive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
wu yl , zhou c , liam ck , et al : first - line erlotinib versus gemcitabine / cisplatin in patients with advanced egfr mutation - positive non - small - cell lung cancer : analyses from the phase iii , randomized , open - label , ensure study . 
ann oncol 26 : 1883 - 1889 , 2015 yang jch , sequist lv , geater sl , et al : clinical activity of afatinib in patients with advanced non - small - cell lung cancer harbouring uncommon egfr mutations : a combined post - hoc analysis of lux - lung 2 , lux - lung 3 , and lux - lung 6 . 
lancet oncol 16 : 830 - 838 , 2015 yang jch , wu yl , schuler m , et al : afatinib versus cisplatin - based chemotherapy for egfr mutation - positive lung adenocarcinoma ( lux - lung 3 and luxlung 6 ) : analysis of overall survival data from two randomised , phase 3 trials . 
lee ck , wu yl , ding pn , et al : impact of specic epidermal growth factor receptor ( egfr ) mutations and clinical characteristics on outcomes after treatment with egfr tyrosine kinase inhibitors versus chemotherapy in egfr - mutant lung cancer : a meta - analysis . 
lee ck , davies l , wu yl , et al : getinib or erlotinib vs chemotherapy for egfr mutation - positive lung cancer : individual patient data meta - analysis of overall survival . 
santoni - rugiu e , melchior lc , urbanska em , et al : intrinsic resistance to egfr - tyrosine kinase inhibitors in egfr - mutant non - small cell lung cancer : differences and similarities with acquired resistance . 
blakely cm , watkins tbk , wu w , et al : evolution and clinical impact of co - occurring genetic alterations in advanced - stage egfr - mutant lung cancers . 
niu x , liu f , zhou y , et al : genome - wide dna methylation analysis reveals gabbr2 as a novel epigenetic target for egfr 19 deletion lung adenocarcinoma with induction erlotinib treatment . 
nelson hh , marsit cj , christensen bc , et al : key epigenetic changes associated with lung cancer development : results from dense methylation array proling . epigenetics 7 : 559 - 566 , 2012 37 . 
zhu j , wang y , duan j , et al : dna methylation status of wnt antagonist sfrp5 can predict the response to the egfr - tyrosine kinase inhibitor therapy in nonsmall cell lung cancer . 
rauch t , wang z , zhang x , et al : homeobox gene methylation in lung cancer studied by genome - wide analysis with a microarray - based methylated cpg island recovery assay . 
zhang l , wu q , he c , et al : hoxb9 inhibits proliferation in gastric carcinoma cells via suppression of phosphorylated - akt and nf - b - dependent snail expression . 
taberlay pc , statham al , kelly tk , et al : reconguration of nucleosome - depleted regions at distal regulatory elements accompanies dna methylation of enhancers and insulators in cancer . 
h saito , t fukuhara , n furuya , et al : erlotinib plus bevacizumab versus erlotinib alone in patients with egfr - positive advanced non - squamous non - small - cell lung cancer ( nej026 ) : interim analysis of an open - label , randomised , multicentre , phase 3 trial . 
hosomi y , morita s , sugawara s , et al : getinib alone versus getinib plus chemotherapy for non - small - cell lung cancer with mutated epidermal growth factor receptor : nej009 study . 
 response to entrectinib in differentiated thyroid cancer with a ros1 fusion introduction the detection of gene fusions in cancer provides insight into tumorigenesis and in some cases reveals potential therapeutic targets.1 there are now a multitude of small - molecule inhibitors that effectively target tumors harboring specific gene fusions . 
gene fusions in ros1 , for example , predict sensitivity to the oral tyrosine kinase inhibitor crizotinib and have led to the approval of crizotinib for the treatment of nsclc with an ros1 fusion.2 ros1 fusions have also been detected in multiple other cancer types , including glioblastoma multiforme , 3 gastric cancer , 4 and acral lentiginous melanoma , 5 but response to ros1 tyrosine kinase inhibitors in tumors other than lung cancer is not well characterized . 
over the next 8 years , she was treated with radioactive iodine ( 200 mci after a radioactive iodine scan showed hilar uptake ) , stereotactic radiosurgery , and surgical resection ( including a left pneumonectomy ) , which confirmed metastatic papillary thyroid carcinoma . 
imaging then showed metastases in the thorax , rib , liver , and brashe began firstline systemic therapy with sorafenib , which she continued for 18 months , achieving a best response of stable disease . 
her thyroglobulin levels were detectable but low and did not change notably during treatment . with no established second - line agents for metastatic papillary thyroid cancer , the patient then participated in prescreening for the phase ii basket study of entrectinib , which facilitated genomic testing of her tumor sample . 
as part of that testing , mrna was isolated from a formalin - fixed paraffinembedded sample from the resected brain metastasis and a sequencing library prepared using a custom - designed anchored multiplex pcr kit ( archerdx , boulder , co ) targeting fusions in the ntrk1 / 2 / 3 , ros1 , alk , and ret genes.10 sequencing was performed on an illumina miseqdx system ( illumina , san diego , ca )  . 
this assay identified an ezr ( exon 10 ) ros1 ( exon 34 ) fusion . the patient provided informed consent , enrolled in the phase ii study of entrectinib , and started treatment in august 2016 . 
at baseline , positron emission tomography / computed tomography imaging revealed a left periaortic soft tissue nodule ( figs 1a and 1d ) and a solitary liver metastasis not well visualized with computed tomography alone ( figs 2a and 2d )  . 
after 4 weeks of therapy , the periaortic nodule was no longer visualized ( figs 1b and 1e ) and remained absent 6 months after starting therapy ( figs 1c and 1f )  . 
there is a growing body of evidence illustrating the activity of targeted agents across cancer types , underscoring the relevance of a genomic diagnosis.11 in nsclc , the presence of a pathogenic ros1 rearrangement identifies candidates for treatment with crizotinib , and targeting ros1 has been a promising strategy across fusion partners.2 , 12 - 14 ros1 gene rearrangements create fusion proteins with constitutively active kinase domains that activate downstream signaling pathways , leading to oncogenic properties in cells , including uncontrolled proliferation and resistance to cell death with prolonged tumor - cell survival . 
these pathways include rasextracellular regulated kinase for cellular proliferation and the janus kinasesignal transducers and activators of transcription and phosphatidylinositol 3 - kinase / akt pathways , which regulate cell survival ( antiapoptosis ) and proliferation . 
cancers that have these pathways activated tend to be more aggressive , with invasion and metastasis leading to poor patient survival.15 with increasing access to genomic profiling of tumors , ros1 rearrangements are now being identified in many other cancers . 
here , we report another unique event : an ezr - ros1 fusion , previously described only in nsclc.16 , 17 although identification of these genomic aberrations across disease types is of interest , there is greater value in documenting clinical response to ros1 inhibition . 
liver metastasis response to entrectinib . axial and coronal images at ( a , d ) baseline , ( b , e ) 4 weeks , and ( c , f ) 6 months . the liver metastasis ( red arrow ) was not well visualized on computed tomography images alone but was [ 18f ] fluorodeoxyglucose avid at baseline ( standardized uptake value , 12.02 ) but was not visualized at 4 weeks and remains absent . is clinically relevant only if it reveals a viable therapeutic target . 
liu consulting or advisory role : genentech , boehringer ingelheim , pfizer , ariad pharmaceuticals , celgene , eli lilly , taiho pharmaceutical , bristol - myers squibb , astrazeneca , ignyta , takeda pharmaceuticals research funding : genentech , pfizer , threshold pharmaceuticals , clovis oncology , corvus pharmaceuticals , esanex , bayer healthcare pharmaceuticals , oncomed , ignyta , merck , medimmune , lycera , astrazeneca laura a . 
imran no relationship to disclose jason christiansen employment : ignyta stock and other ownership interests : ignyta edna chow - maneval employment : ignyta zachary hornby employment : ignyta leadership : ignyta stock and other ownership interests : ignyta travel , accommodations , expenses : ignyta pratik s . 
ardini e , menichincheri m , banfi p , et al : entrectinib , a pan - trk , ros1 , and alk inhibitor with activity in multiple molecularly defined cancer indications . 
murphy da , ely ha , shoemaker r , et al : detecting gene rearrangements in patient populations through a 2 - step diagnostic test comprised of rapid ihc enrichment followed by sensitive next - generation sequencing . 
bansal p , osman d , gan gn , et al : recent advances in targetable therapeutics in metastatic non - squamous nsclc . front oncol 6 : 112 , 2016 12 . 
bos m , gardizi m , schildhaus hu , et al : complete metabolic response in a patient with repeatedly relapsed non - small cell lung cancer harboring ros1 gene rearrangement after treatment with crizotinib . 
subbiah v , hong ds , meric - bernstam f : clinical activity of ceritinib in ros1 - rearranged non - small cell lung cancer : bench to bedside report . 
li h , pan y , wang r , et al : response to crizotinib observed in metastatic mediastinum lymph node from a non - small cell lung cancer patient harboring ezr - ros1 fusion . 
kasi , mbbs , md , ms1 ; judong yang , md , ms2 ; phani keerthi surapaneni , mbbs1 ; tanios bekaii - saab , md3 ; daniel h . 
borad , md3 purpose recent advances in molecular diagnostic technologies have allowed for the evaluation of solid tumor malignancies via noninvasive blood sampling , including circulating tumor dna ( ctdna ) proling . 
after excluding variants of unknown signicance , therapeutically relevant alterations were observed in 76 patients ( 55% ) , including braf mutations , erbb2 amplications , fgfr2 fusions , fgfr2 mutations , and idh1 mutations seen in 21% of patients . 
a different spectrum of alterations was observed in patients with early - onset btc ( younger than age 50 years ) compared with older patients ( older than age 50 years )  . conclusion data on ctdna in btc is currently limited . 
intact circulating tumor cells and cell - free dna ( cfdna ) from both leukocytes and tumors ( circulating tumor dna [ ctdna ] ) can now be isolated and analyzed using advanced sequencing methods . 
ctdna has been shown to carry tumor - specic genetic or epigenetic alterations , such as point mutations , copy number variations , chromosomal rearrangements , and dna methylation patterns.1 - 4 the testing approaches in this eld are two dominant polymerase chain reaction ( pcr ) based ( digital pcr ) and next - generation sequencing ( ngs )  . 
ngs approaches have the ability to investigate a larger these number of genes simultaneously ; however , techniques have historically been limited by the need for high sensitivity and specicity and the cost associated with sequencing . 
this approach allows for agnostic analysis of large portions of the genome and can identify multiple mutations with increased sensitivity.5 evaluation of ctdna is particularly attractive as it enables the assessment of patient - specic tumoral genetic / epigenetic alterations while allowing for serial monitoring of tumor genomes in a noninvasive , convenient , and accurate manner . 
 mody et al biliary tract cancers ( btcs ) are an uncommon malignancy arising from epithelial cells that line the biliary tree and have a rapidly fatal course , with 5 - year survival rates of less than 10%.1 , 2 although relatively rare in western countries , btcs are more prevalent in southeast asia.3 in the united states , btcs account for approximately 2% of all new cancer diagnoses and have been rising in incidence during the past few decades.4 - 10 patients with cholangiocarcinoma stand to gain immensely from the use of ctdna given that diagnosis currently is more often made at advanced stages of disease ; recurrences are common , despite the pursuit of potentially curable treatments , such as surgery in a subset of patients ; biopsies are not always obtained or often yield suboptimal quantities of tumor cells for tissue - based genomic proling ; and multiple genomic alterations , which are potential therapeutic targets , are known to occur in btcs . 
genetic alterations that have been identied include activating kras mutations , tp53 mutations / deletions , idh1 and idh2 mutations , fgfr2 gene fusions , cdkn2a / b mutations / deletions , and , less commonly , ntrk gene fusions and alterations in erbb2 ( her2 ) , met , braf , nras , and pik3ca.6 , 7 therefore , the purpose of the current study was to examine the results of ctdna testing from a large cohort of patients with btc at a national cancer institute comprehensive cancer center , acquired in the course of clinical practice , and to characterize the mutational landscape of btcs using this technology . 
data analysis from this patient cohort was reviewed and approved by the mayo clinic institutional review board . demographic information and the date of blood collection were available for all patients . 
additional patient information was collected from the mayo clinic electronic medical record and included conrmation of btc diagnosis ; risk factors , including history of hepatitis a , b , or c , nonviral chronic liver disease , diabetes , obesity , or primary sclerosing cholangitis ; and pertinent clinical information , such as treatment status at the time of ctdna testing and history of liver - directed therapy . comprehensive genomic testing in plasma cfdna was extracted from whole blood collected in 10 - ml streck tubes . 
samples were shipped to a clinical laboratory improvement actcertied , college of american pathologistsaccredited laboratory ( guardant health )  . after double ultracentrifugation , 5 to 30 ng cfdna was isolated for digital sequencing . cfdna fragments , both leukocyte and tumor derived , were simultaneously sequenced . 
analytical sensitivity allowed for the detection of one to two mutant fragments in a 10 - ml blood sample ( 0.1% limit of detection ) with analytic specicity of more than 99.9999%. twelve copy number alterations were reported as the absolute gene copy number in plasma . 
as most cfdna is leukocyte derived , the gene copy number is generally 2.0. tumor - derived dna shed into the bloodstream raises this value , but , because of the relative proportions of tumorderived versus leukocyte - derived cfdna , is typically a minor contributor . 
in the 68 - gene panel , eight genes were retired from the single - nucleotide variation gene set , whereas coverage of gene amplications expanded from three to 16 genes , and the addition of detection of fusions in four genes and insertions or deletion of bases ( indels ) in one gene was made . 
the 70 - gene panel included all national comprehensive cancer network somatic genomic targets , cluding complete or critical exon coverage in 30 and 40 genes , respectively , amplications in 14 genes , fusions in six genes , and indels in three genes . 
the majority of samples in this study ( n = 122 ) were tested using the 73 - gene panel . to determine if an alteration was therapeutically relevant , we dened therapeutically relevant as any gene alteration with an oncokb level of evidence of 1 , 2a , 2b , 3a , 3b , or r1.8 oncokb is a precision oncology knowledge base that contains information about the effects and treatment implications of specic cancer gene alterations.8 oncokb contains detailed information about specic alterations in 477 cancer genes compiled from various sources , cluding guidelines from the us food and drug administration ( fda ) , national comprehensive cancer network , asco , clinicaltrials.gov , and the scientic literature . 
level 4 includes those variants that are considered predictive of response to targeted agents on the basis of compelling biologic , nonclinical evidence . by these standards , a gene is considered therapeutically relevant if there is supporting evidence that the gene is a driver of tumorigenesis , and wherein actionability of the gene can refer to either sensitivity and / or resistance to a drug ( s )  . 
in addition , there must be a clinically available agent , including clinical trials , that targets the gene / protein for a specic agent , and there must be at least preclinical evidence that supports its role in targeting the specic gene / protein . on the basis of the aforementioned criteria , the following genes were considered actionable : akt1 , alk , araf , atm , braf , brca1 , brca1 , ccnd1 , ccnd2 , cdk4 , cdk6 , cdkn2a , ctnnb1 , egfr , erbb2 , esr1 , fgfr1 , fgfr2 , gnas , idh1 , idh2 , jak2 , kras , met , map2k1 , mlh1 , mtor , myc , ntrk1 , ntrk3 , pdgfra , pik3ca , raf1 , ptpn11 , stk11 , tsc1 , and vhl . 
finally , variants found in actionable genes that did not alter the amino acid sequencethat is , synonymous mutationsand / or those that lacked any supporting functional evidence of pathogenicity were excluded . statistical analysis the distribution of each continuous variable is summarized by its mean , standard deviation , and range . 
the relationship between gene types with regard to mutation and amplication , as well as synonymous and targetable status , was evaluated using spearmans rank correlation and was displayed in the correlation matrix in which nonsignicant correlations are marked with a blank in the graph . 
a small subset of patients had underlying chronic liver disease , such as primary sclerosing cholangitis ( 8% ) or other chronic liver disease ( 6% )  . landscape of alterations among a total of 138 ctdna samples , 105 ( 76% ) of these included one or more alterations when variants of unknown signicance were excluded . 
tp53 and kras were the two most common alterations in all subtypes of disease , followed by fgfr2 in 7% ( intrahepatic subtype ) , arid1a ( extrahepatic subtype ) and cdk6 , apc , and smad4 ( gallbladder subtype )  . 
in the more prevalent of the subtypes ( intrahepatic ) in our sampleaside from fgfr2pik3ca and idh1 were fairly commonly altered . a different spectrum of alterations was observed in patients with early - onset btc ( younger than age 50 years ) compared with older patients ( older than age 50 years ) , although overall the differences were not statistically signicant ( p = .55 ; fig 3 )  . 
other alterations which were more common in younger patients included pik3ca , met , and braf . therapeutically relevant alterations after excluding variants of unknown signicance , therapeutically relevant alterations were seen in 55% ( n = 76 ) of the total cohort of samples . 
several risk factors for btc have been described , with most etiologies resulting in long - standing inammation.9 , 12 the only standard systemic therapy for the disease is gemcitabine and cisplatthere is no standard second - line therapy that has been shown to unequivocally improve survival for patients who experience disease progression on gemcitabine / cisplatin.13 btcs are traditionally classied by location as intrahepatic , extrahepatic , and gallbladder on the basis of their presumed site of origin within the biliary duct systethis 4 2019 by american society of clinical oncology mody et al 65 ( 28 - 87 ) 85 ( 69 ) 22 ( 18 ) 16 ( 13 ) 60 ( 48 ) 63 ( 52 ) 42 ( 35 ) 38 ( 30 ) 43 ( 35 ) 21 ( 17 ) 14 ( 12 ) 10 ( 8 ) 2 ( 1 ) 6 ( 5 ) 15 ( 11 ) 30 ( 22 ) 26 ( 19 ) 19 ( 14 ) 48 ( 35 ) anatomic classication has been effective in differentiating btcs with regard to epidemiology , etiology , clinical presentation , and treatment.9 early diagnosis is ideal given that surgical resection or liver transplantationfor perihilar tumorsoffers the best chance at cure ; however , majority of patients are diagnosed with advanced - stage disease precluding surgical management . 
of particular importance , pathologic tissue - based conrmation of btc can be challenging given that clinical yield is often suboptimal and insufcient , especially for dna extraction to enable genomic proling . 
this is primarily a result of the more desmoplastic nature of many btc tumors . with the availability of next - generation genomic proling in recent years , a number of genomic subtypes of btc have been described , many of which are dened by therapeutically targetable genomic alterations.7 , 14 - 18 for example , fgfr fusion rearrangements and idh1 and idh2 mutations have emerged as signicant driver mutation genomic subtypes . 
at present , several targeted drugs are in clinical development , with encouraging results thus far . for the above reasons , the potential for use of ctdna in the management of btc is of particular interest . 
investigations of the use of ctdna in cca have previously been hampered by the rarity of the disease , the relatively incomplete understanding of the genetics of this cancer , and the lack of a validated and widely used ctdna assay . 
this has now changed with recent increased focus on the disease ; recent characterization of the btc genome by several studies , including that from the cancer genome atlas ; and also with the availability of a number of commercially available ctdna assays in clinical practice.14 , 15 , 19 thus far , data on ctdna in cholangiocarcinoma have been sparse . 
andersen and jakobsen20 have demonstrated the early feasibility of a ctdna assay in btc , using a multiplex digital pcr assay to screen for 31 mutations in kras , nras , braf , and pik3ca . 
the authors then performed the assay on serum from ve patients with btc with known tumor mutations and six patients who were known to be wild type for the assayed mutations . 
the assay correctly identied the ve known mutations , whereas none of the six wild - type samples had mutations identied in cfdna . goyal and colleagues21 demonstrated the usefulness of ctdna in serial monitoring of disease and for the detection of resistance mechanisms in the setting of targeted therapy . among 32 patients enrolled in a phase ii study of the fgfr inhibitor bgj398 , nine patients ( 28% ) had fgfr2 fusions detected and four patients were enrolled in the trial . 
pivotal trials exploring inhibitors of fgfr and idh in the management of btc specically are ongoing ( clinicaltrials.gov identiers : nct02924376 , nct03230318 , nct02052778 , and nct02989857 )  . other data have highlighted the application of erbb2 and braf targeted therapies in the disease.22 - 27 for these reasons , it is critically important to identify therapeutically relevant alterations in patients with cholangiocarcinoma . we demonstrate , for the rst time to our knowledge , the ability to detect a broad array of therapeutically relevant alterations using ctdna testing at a signicant rate ( 55% ) in patients with btc . 
whereas the oncokb system is an extensive , comprehensive , and curated precision oncology knowledge base that is capable of supporting precision oncology treatment decisions , should be noted that universally accepted denitions of actionable alterations are not currently available.8 more practically , a total of 21% of patients in our cohort were cohort ; fig 3 . 
 circulating tumor dna in biliary tract cancer identied as having actionable alterations in braf , erbb2 , fgfr2 , and idh1 , for which there are dedicated clinical trials available for patients with btc or for which currently available data exist on the treatment of patients with btc with existing targeted therapies . limitations , our study does have other including the moderate sample size , its retrospective nature , and the fact that patients are derived from a single institution . 
we also have limited clinical data as a result of the retrospective nature of the study . ctdna in btc has been an underexplored area , but our study for the rst time to our knowledge demonstrates the true feasibility of ctdna testing in this disease . 
we believe there is a rationale for ctdna to be incorporated in cholangiocarcinoma trials going forward so as to further explore the technology as a means for identifying patients with actionable genomic alterations , as a biomarker of response , and for serial monitoring of disease and detection of resistance mechanisms , as well as for prognostic purposes . 
borad manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors policy , please refer to or ascopubs.org / po / authorcenter . kabir mody consulting or advisory role : celgene , genentech , merrimack pharmaceuticals , eisai , astrazeneca , vicus therapeutics research funding : fibrogen , senhwa biosciences , ariad pharmaceuticals , tracon pharma , medimmune , agios , arqule , taiho pharmaceutical pashtoon m . 
kasi consulting or advisory role : taiho pharmaceutical ( inst ) , ipsen ( inst ) , bristol - myers squibb ( inst ) , advanced accelerator applications ( inst ) , array biopharma ( inst ) , celgene ( inst ) tanios bekaii - saab consulting or advisory role : amgen ( inst ) , glenmark , ipsen ( inst ) , eli lilly ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , bayer ( inst ) , celgene ( inst ) , genentech ( inst ) , abbvie , incyte ( inst ) , imugene , immuneering other relationship : exelixis , merck , sillajen , armo biosciences daniel h . 
ahn consulting or advisory role : celltrion ( i ) , merrimack pharmaceuticals , astellas pharma , eisai , cardinal health , paradigm , lexicon amit mahipal research funding : taiho pharmaceutical jason s . 
nat med 20 : 548 - 554 , 2014 sia d , hoshida y , villanueva a , et al : integrative molecular analysis of intrahepatic cholangiocarcinoma reveals 2 classes that have different outcomes . gastroenterology 144 : 829 - 840 , 2013 valle jw , lamarca a , goyal l , et al : new horizons for precision medicine in biliary tract cancers . 
shaib yh , davila ja , mcglynn k , et al : rising incidence of intrahepatic cholangiocarcinoma in the united states : a true increase ? j hepatol 40 : 472 - 477 , 2004 11 . 
chan - on w , kuwahara k , kobayashi n , et al : cholangiocarcinomas associated with long - term inammation express the activation - induced cytidine deaminase and germinal center - associated nuclear protein involved in immunoglobulin v - region diversication . 
j gastrointest oncol 7 : 797 - 803 , 2016 javle m , bekaii - saab t , jain a , et al : biliary cancer : utility of next - generation sequencing for clinical management . 
goyal l , saha sk , liu ly , et al : polyclonal secondary fgfr2 mutations drive acquired resistance to fgfr inhibition in patients with fgfr2 fusion - positive cholangiocarcinoma . 
j clin oncol 33 , 2017 ( suppl ; abstr e15137 ) javle m , churi c , kang hc , et al : her2 / neu - directed therapy for biliary tract cancer . 
kocsis j , aroksz all asi a , andr as c , et al : combined dabrafenib and trametinib treatment in a case of chemotherapy - refractory extrahepatic braf v600e mutant cholangiocarcinoma : dramatic clinical and radiological response with a confusing synchronic new liver lesion . 
loaiza - bonilla a , clayton e , furth e , et al : dramatic response to dabrafenib and trametinib combination in a braf v600e - mutated cholangiocarcinoma : implementation of a molecular tumour board and next - generation sequencing for personalized medicine . 
golan t , raitses - gurevich m , kelley rk , et al : overall survival and clinical characteristics of brca - associated cholangiocarcinoma : a multicenter retrospective a brief review . 
oncogenic met activation results from a hijacking of various aspects of the canonical met pathway otherwise normally active in development and wound healing.2 the canonical pathway consists of hgf ligand - induced dimerization , tyrosine kinase domain activation , and the subsequent activation of a downstream signaling cascade resulting in the met - driven oncophenotype . 
shouldnt a targeted therapy be directed toward a susceptible cancer cell that harbors the target ? but what was the biomarker to reliably signify that a tumor was truly met dependent and would derive substantial benet from anti - met therapy ? the leading biomarker candidate was , and still is , met amplication , which has severalfold higher protein expression as observed by mass spectrometry compared with nonamplied tumors.8 although rare , amounting to only approximately 5% of gea ( the highest incidence of any cancer ) , met amplication has been the most consistent and reliable biomarker both of overall poor prognosis and predictive benet from agents targeting the receptor.3 , 4 , 12 - 14 however , other potential predictive biomarkers have also been proposed , including met tyrosine kinase phosphorylation ( difcult to measure ) , 15 met activating mutation or fusion ( rare ) , met exon 14 skipping or deletion ( mostly lung cancer ) , 16 high hgf tumor and / or serum levels ( not consistently demonstrated ) , and met overexpression ( in the absence of met amplication ) .17 focus on the latter overexpression ensued , likely because this was generally than the more stringent genomic more prevalent denition of amplication , making this more expedient and lucrative to study . 
what exactly is the denition of met overexpression ? met expression by immunohistochemistry ( ihc ) has many descriptions , including cellular distribution ( membranous , cytoplasmic , and / or nuclear staining ) , extensity ( the percentage of tumor cells actually staining ) , and intensity ( the semiquantied staining strength from 0 to 3 + )  . 
 catenacci death ligand 1 ( pd - l1 ) , various alterations in the scoring criteria can change a tumor from met negative to met positive , or vice versa , and dramatically alter positivity incidence with slight scoring modications . 
benet in the met - high population ( 64% incidence in that study ) hinged on a small retrospective subgroup of 47 and 21 patients receiving rilotumumab and placebo , respectively.18 unfortunately , the competition to be rst to market and , therefore , the rush to initiate phase iii studies with rilotumumab in rilomet - 1 ( international phase iii multicenter , randomized , double - blind , placebocontrolled trial of rilotumumab plus epirubicin , cisplatin , and capecitabine as first - line therapy in patients with advanced met - positive gastric or gastroesophageal junction adenocarcinoma ) and onartuzumab in metgastric ( fluorouracil , leucovorin , and oxaliplatin with or without onartuzumab in her2 - negative , met - positive gastroesophageal adenocarcinoma ) , without more attention to these issues , resulted in a fundamental lack of biomarker understanding . 
because the questions were unasked , the answers were unknown . importantly , thus , the market - based engines steamed on ahead with the following two bits of data : one patient who responded to an lbab monotherapy5 and one retrospective small subgroup analysis of a phase ii randomized study.18 unfortunately , ultimately both lbab phase iii studies were negative.10 , 11 regrettably , neither study successfully enriched for a population who would benet from met lbabs . 
notably , for the rilotumumab studies , the initial antibody prototype assay and , the actual scoring system used in the phase ii study were changed for the prospective phase iii study to ofcially codevelop a companion diagnostic assay . the assay in rilomet - 1 likely inadequately selected any optimal patient population for treatment , with most patients ( 81% ) screened considered positive for met expression using the lax criteria of greater than or equal to 1 + intensity at 25% or greater extensity staining ( hardly selecting ) and most patients having low - level expression.11 prospectively testing formalin - xed parafn - embedded ( ffpe ) freshly cut samples from recently diagnosed patients in rilomet - 1 compared with a retrospective batched archival ffpe analysis in the phase ii study may also have contributed to the incidence discrepancy between the studies , because ihc sensitivity is decreased with older ffpe samples and , when still positive in light of this , would represent those indeed , true benet randomized phase ii samples likely having the highest levels of expression to begin with . 
conversely , the metgastric study had only the slightly more stringent criteria of positivity for eligibility of greater than or equal to 1 + intensity at 50% or greater extensity staining ( ie , more cells needed to be expressing at least low - level amounts of protein )  . 
notably , in this latter underpowered subgroup analysis , the hr for overall survival was 0.64 in favor of onartuzumab ( p = .062 ) , and the median survival increased from 9.7 months to 11 months with onartuzumab.10 could this have been statistically signicant with the originally intended number of patients ? because the question was unasked ( study terminated early ) , the answer is unknown . 
in the end , the optimal met biomarker assay , scoring , and positivity criteria of expression for lbabs , if any , remain undened . nevertheless , even if we could rewind and do things differently with this hindsight ( could we perform prospective , adequately accrued , randomized phase ii and / or iii studies with only the highest ihc criteria amounting to approximately 20% to 30% of all patients with gea ? ) , the marginal absolute benets that could be realistically achieved with lbab in an optimal expressing subgroup , as exemplied by the metgastric subgroup analysis hr of 0.64 , lend pause to question whether this would really provide signicant clinical improvement . 
yet , frustratingly , met amplication , now serving as a driver oncogene in this scenario , is the biomarker subset to likely derive the most benet from targeted met receptor inhibitors . 
in comparison , pd - l1 checkpoint blockade monotherapies , despite the hysteria , ultimately demonstrated an approximate 10% response rate in the third - line or higher setting in gea all - comers , with a median progression - free survival time of 2 months , and only a 13.3% response rate ( 19 of 143 patients ) in the subset of pd - l1positive , microsatellite stable ( mss ) selected patients , with a median dor of less than 8 months ( only ve patients , or ve [ 28% ] of 19 responders or ve [ 3% ] of 143 pd - l1positive / mss patients , had dor greater than 12 months ) .25 yet on the basis of these results , pembrolizumab was recently successfully pursued for accelerated approval for the entire pd - l1positive / mss subset by the us food and drug administration.25 , 26 similar clinical outcomes are consistently reported in patients with met - amplied gea ( with comparable incidence of responses lasting greater than 12 months )  . 
in the face of being an uncommon genomic event , this discussion still matters for patients with gea with tumors harboring met amplication . this amg337 example , along with other met inhibitors , has well - elucidated reasons for perceived failure . 
these include underappreciating the general poor prognosis of met - amplied tumors in single - arm , late - line studies , intrapatient heterogeneity with regions harboring and not harboring met amplication , and the presence of concurrent genomic aberrations in some met - amplied cells . all of these factors could lead to relatively quick progression on monotherapy either outright or shortly after an initial response in most , but importantly not all , responding patients . 
however , the ideal randomized and combination therapy studies have been elusive to date because of the infeasibility of classic clinical study designs and the requirement of extraordinarily high numbers of patients screened to identify the met - amplied subset , with the consequent abandonment of additional investigation by pharma because of this apparently high - risk and low - yield scenario . 
with met , supportive evidence abounds that there are patients who derive benet from met inhibitors , particularly those with met - amplied tumors , yet to date , no met - specic inhibitor is approved by the us food and drug administration in any met - specic indication for any tumor . 
lack of progress can be attributed to a number of issues including inadequate validation of biomarker cut - offs , along with the inherent hurdles to developing drugs in lowincidence biomarker populations , coupled with complex intrapatient heterogeneous biology rendering monotherapy in late - line therapy less likely to impress , 34 and certainly so for accelerated approval paths . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . daniel catenacci honoraria : genentech , eli lilly , amgen , oncoplex diagnostics , foundation medicine , taiho pharmaceutical , genmab , nantomics , guardant health , merck , bristol - myers squibb , gritstone oncology , five prime therapeutics , astellas pharma consulting or advisory role : genentech , amgen , merck , eli lilly , taiho pharmaceutical , bristol - myers squibb , astellas pharma speakers ' bureau : guardant health , foundation medicine , genentech , eli lilly , merck references giordano s , di renzo mf , ferracini r , et al : p145 , a protein with associated tyrosine kinase activity in a human gastric carcinoma cell line . 
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hong ds , lorusso pm , hamid o , et al : phase 1 study of amg 337 , a highly selective small - molecule met inhibitor , in patients with advanced solid tumors . 
van cutsem e , karaszewska b , kang yk , et al : a multicenter phase 2 study of amg 337 in patients with met - amplied gastric / gastroesophageal junction / esophageal adenocarcinoma and other solid tumors . 
fuchs cs , doi t , jang rw , et al : safety and efcacy of pembrolizumab monotherapy in patients with previously treated advanced gastric and gastroesophageal junction cancer : phase 2 clinical keynote - 059 trial . 
catenacci dvt , park h , uronis he , et al : margetuximab ( m ) plus pembrolizumab ( p ) in erbb2 - amplied pd - l1 + gastroesophageal adenocarcinoma ( gea ) post trastuzumab ( t )  . 
lancet oncol 16 : 1276 - 1278 , 2015 joshi ss , maron sb , lomnicki s , et al : personalized antibodies for gastroesophageal adenocarcinoma ( pangea ) : a phase ii precision medicine trial ( nct02213289 )  . 
j natl cancer inst 97 : 249 - 250 , 2005 jardim dl , groves es , breitfeld pp , et al : factors associated with failure of oncology drugs in late - stage clinical development : a systematic review . 
hamid o , gajewski tf , frankel ae , et al : epacadostat plus pembrolizumab in patients with advanced melanoma : phase 1 and 2 efcacy and safety results from echo - 202 / keynote - 037 . 
long gv , dummer r , hamid o , et al : epacadostat ( e ) plus pembrolizumab ( p ) versus pembrolizumab alone in patients ( pts ) with unresectable or metastatic melanoma : results of the phase 3 echo - 301 / keynote - 252 study . 
gene amplication , or increased gene dosage , leads to increased messenger rna expression , which leads to exponential increase in the amount of met protein receptor ( green ) expression at the membrane . 
most patients present with either metastatic pdac ( 50% - 60% ) or locally advanced tumors ( 30% - 40% ) , for which the median survival is 5 - 9 months after diagnosis.1 , 2 outcomes are still suboptimal for the small subset ( 10%20% ) of patients who present with resectable tumors conned to the pancreas ; , 50% of these patients survive 5 years after surgery despite modern adjuvant chemotherapy.3 moreover , at autopsy , the disease is metastatic for 88% of recurrences , and  . 
80% have more than 10 distinct metastatic lesions4 that are genetically related to the primary tumor5 and other metastases.6 these observations indicate that majority of patients with pdac harbor nonradiographically evident , micrometastatic disease after resection and that remnant tumor cells evadeor acquire resistance toadjuvant chemotherapy . 
although tropism to specic organs during metastatic spread is still poorly understood , patients with recurrence in the liver or peritoneum7 survive signicantly shorter than patients with recurrent lung metastases.8 - 10 pdac tumors are commonly classied into two major subtypes : one that shares some features with adenosquamous tumors ( squamoid and / or basal ) and the other that retains a differentiated , glandular and / or ductal morphology ( ductal and / or classical )  . 
squamoid pdac tumors are more glycolytic , 11 , 12 more hypoxic , 13 more inammatory likely broblasts , 16 and yield a poorer prognosis than ductal tumors.17 - 21 classical subtype tumors are associated with more tumor - inltrating leukocytes , denser collagen , and better outcomes , 15 , 22 although signicant subtype heterogeneity within tumors13 complicates the relationship between subtype and outcome . to metastasize , 14 , 15 recruit more cytolytic t cells inltrate pdac tumors than most other tumors , 23 but they are ultimately insufcient to control the cancer . 
density of tumor - inltrating t cells is highly variable among pdac tumors , 24 and abundant cd8 + t cells ( along with a high number of neoantigens ) can support exceptionally long - term survival.25 however , t cellmediated tumor immunity may be restricted by several mechanisms : tumor immunosuppressive cell downregulation of hla , leukocytes , t cell proximity to tumor cells , and t cell exhaustion.26 - 30 effective t cellmediated tumor immunity is enhanced by a high diversity of functional t cell clones , tumor - specic recruitment of effector t cells , and abundant neoantigens.23 , 25 , 31 quantifying the phenotypes , functions , and locations of leukocytes is critical to identify specic tumor immunity required for exceptional positive outcomes . rare , exceptional control of pdac progression may be mediated by equally rare , idiosyncratic patient genetics , tumor - specic somatic alterations and gene expression , and / or stochastically generated tumor immunity . 
in this report , we present the cases of pt1 , who survived more than 46 months with occult , chemotherapy - resistant metastatic pdac , and her niece ( pt2 ) who succumbed to progressing metastatic disease despite aggressive treatment . 
however , during adjuvant chemotherapy , the lung lesion increased to 23 mm 18 mm , and a ct and / or pet was suspicious for malignancy with a standardized uptake value ( suv ) of 4.5. 
ca19 - 9 test results are not shown becausefor both patientsthey were reproducibly approximately 90% lower than the 37 u / ml threshold for normal , even when the primary tumor was present . 
pt1 chose to receive no further treatment and was radiographically disease - free for over 2 years ( fig 1 ) until an isolated , recurrent lung metastasis was identied by ct and fdg - pet ( suv of 9 ) and then treated by 50 gy in ve fractions using stereotactic body radiotherapy . 
pt2 died 19 months after metastatic disease recurrence . treatment a shared germline prss1 mutation and somatic alterations common to pdac we identied germline prss1 p.a16v in both patients and somatic alterations in the two most common pdac driver geneskras and tp53in both tumors from each patient ( table 1 )  . 
each scale bar is 0.5 m ( c ) pdac subtyping of each patients primary and metastatic tumors . left panel : spearman correlation coefcients for tumors from pt1 and pt2 compared with the published rank order of pdassigner genes for classical ( y - axis ) and quasimesenchymal ( x - axis ) tumors . 
both tumors from pt1 aligned well with the classical subtype , whereas the tumors from pt2 were more quasimesenchymal and / or basal with the metastasis scoring more basal than the primary tumor . leukocyte types associated with immunity in tumors from patient 1 we used a multiplex immunohistochemistry ( mihc ) workow34 to quantify the densities of tumor cells , broblasts , and 10 leukocyte subsets ( appendix table a1 )  . 
we selected regions of interest ( rois ) within each section that contained both krt + epithelial or tumor cells and cd45 + immune cells ( appendix fig a1 ) , followed by quantitative assessment of each roi . 
a detailed analysis of leukocyte subsets revealed that cd8 + t cells and cd4 + t cells were signicantly denser in the metastasis from pt1 compared with the primary tumor from pt2 ( fig 3b )  . 
 ( a ) mean cell density per roi for mutually exclusive populations of ki67 + tumor or epithelial cells , ki67neg tumor or epithelial cells , broblasts , and leukocytes . 
among subsets of cd4 + t cells , we found more pro - inammatory th1 t cells in the metastasis from pt1 than either primary tumor ( fig 3c )  . 
within cd4 + t cells , we found a greater density of both cytolytic granzyme b + ( grzb ) cells and proliferative ki67 + cells in the metastasis from pt1 than the primary tumor from pt2 and a higher density of proliferative ki67 + cells in pt1s primary tumor compared with pt2s primary tumor ( fig 3d )  . consistent with the abundant th1 - like macrophages in pt1s primary tumor , we found that the ratio of th1 - like to th2 - like macrophages was signicantly greater in pt1s primary tumor relative to the other 2 tumors ( fig 3e )  . 
a high granulocyte / neutrophil to lymphocyte ratio is associated with poor outcomes.35 , 36 consistent with this , the primary tumor from pt2 had a signicantly higher granulocyte to cd8 + t cell ratio than either tumor from pt1 ( fig 3e )  . 
in addition , across rois , there was no correlation between the densities of cd8 + t cells and granulocytes in the tumors from pt1 , but there was a signicant positive correlation in pt2s primary tumor ( p , .03 , fig 4a )  . 
furthermore , the abundant granulocytes in pt2s tumor were proximal to tumor cells and appeared within lumens ( fig 4b ) where they may contribute to pathogenesis by occluding ducts.37 we also observed tertiary lymph structures ( tlss ) at the border of both primary tumors , but these were more prevalent in the primary tumor from pt1 ( appendix fig a1 )  . 
tlss from pt1 also contained signicantly more b cells , cd4 + t cells , and cd8 + t cells ( appendix fig a2 ) as previously reported for patients with relatively positive outcomes.24 , 38 tissue acquisition and patient consent human tissues were obtained with informed consent in accordance with the declaration of helsinki and were acquired through the oregon pancreas tissue registry under oregon health & science university irb protocol #3609 . discussion we investigated multiple modalities and tumor characteristics of pdac between two related patients . 
we found several similarities between both patients cancers , cluding genes commonly altered in aggressive pdac ( kras , tp53 , and smad439 , 40 ) and a shared prss1 a16v germline mutation that may predispose to pancreatitis41 - 44 but is variably penetrant , 45 raising the possibility that this specic alteration leads to subclinical pancreatitis that accelerates tumorigenesis , consistent with pt2s early onset of disease.41 , 46 the disease course for pt1 was exceptional in the context of occult , chemotherapy - resistant metastatic disease for nearly 4 years . 
an fanca mutation in the metastasis from pt1 might have sensitized that tumor to adjuvant gemcitabine and xeloda and later to sbrt ; however , pt1s lung metastasis progressed during adjuvant chemotherapy , and no adjuvant treatment was given after surgical resection of the lung metastasis , suggesting that the indolent disease might have also been controlled by other factors . 
both tumors from pt2 contained an alteration in cdkn2a , and the metastasis from pt2 had a copy number loss of pten ; alterations in these genes are associated with poor outcomes and drug resistance.47 - 49 pt1s classical subtype tumors and metastases limited to the lungs are both favorable prognostic factors . 
specically , more prevalent tlss at the periphery of the primary tumor ( appendix fig a1 ) and denser cd8 + t cells ( fig 3b ) that did not correlate with the density of granulocytes24 , 50 ( fig 4a ) , opening the possibility that tumor cells and / or cd4 + t cells in pt1s tumors recruit fundamentally different leukocyte cell types from pt2s tumors.51 additionally , granulocytes typically promote immunosuppression in late - stage tumors , 52 consistent with the relatively low number of t cells in pt2s tumor . classical subtype pdac with lung metastases and unconventional tumor immunity may lead to exceptional outcomes . 
sears , phd , brenden - colson center for pancreatic care , oregon health and science university , 2730 s moody ave , portland , or 97201 ; e - mail : searsr@ohsu.edu. support supported by the brenden - colson foundation and nci grant u01 ca224012 to r.c. 
coussens employment : oregon health &amp ; science university ( ohsu ) honoraria : prospect creek foundation , lustgarten foundation for pancreatic cancer research , syndax pharmaceuticals , inc : external advisory board , carisma therapeutics inc : scientic advisory board , verseau therapeutics , inc , scientic advisory board , zymeworks , inc , scientic advisory board , cytomx therapeutics , inc , kineta inc , ( p30 ) koch institute for integrated cancer research , massachusetts inst . 
of tech , ( p30 ) salk institute cancer center , bloomberg - kimmel institute for cancer immunotherapy , sidney kimmel comprehensive cancer center at johns hopkins , dana farber cancer center breast spore , ( p30 ) dana farber / harvard cancer center , ( p30 ) university of california , san diego moores cancer center , starr cancer consortium , lustgarten foundation for pancreatic cancer research , therapeutics working group , nih / nci - frederick national laboratory advisory committee ( fnlac ) , susan g komen foundation , komen scholar consulting or advisory role : cell signaling technologies , pharmacyclics , cytomx therapeutics , syndax , carisma therapeutics , verseau therapeutics , zymeworks , kineta , inc , abbvie , shasqi inc research funding : syndax pharmaceuticals inc , pharmacyclics , cell signaling technologies , innate pharma , deciphera travel , accommodations , expenses : cell signaling technologies , astrazeneca , pharmacyclics , verseau , carisma therapeutics , cytomx therapeutics , zymeworks other relationship : prospect creek foundation , lustgarten foundation for pancreatic cancer research , ( p30 ) koch institute for integrated cancer research , massachusetts inst . 
n engl j med 379 : 2395 - 2406 , 2018 iacobuzio - donahue ca , fu b , yachida s , et al : dpc4 gene status of the primary carcinoma correlates with patterns of failure in patients with pancreatic cancer . j clin oncol 27 : 1806 - 1813 , 2009 yachida s , jones s , bozic i , et al : distant metastasis occurs late during the genetic evolution of pancreatic cancer . 
makohon - moore ap , zhang m , reiter jg , et al : limited heterogeneity of known driver gene mutations among the metastases of individual patients with pancreatic cancer . 
nat genet 49 : 358 - 366 , 2017 katz mhg , wang h , fleming jb , et al : long - term survival after multidisciplinary management of resected pancreatic adenocarcinoma . 
ann surg oncol 16 : 836 - 847 , 2009 downs - canner s , zenati m , boone ba , et al : the indolent nature of pulmonary metastases from ductal adenocarcinoma of the pancreas . 
j surg oncol 112 : 80 - 85 , 2015 deeb a , haque su , olowokure o : pulmonary metastases in pancreatic cancer , is there a survival inuence ? j gastrointest oncol 6 : e48 - e51 , 2015 10 . 
rashid nu , peng xl , jin c , et al : purity independent subtyping of tumors ( purist ) , a clinically robust , single - sample classier for tumor subtyping in pancreatic 34 . 
zhou y , wei q , fan j , et al : prognostic role of the neutrophil - to - lymphocyte ratio in pancreatic cancer : a meta - analysis containing 8252 patients . 
giakoustidis a , neofytou k , costa neves m , et al : identifying the role of neutrophil - to - lymphocyte ratio and platelets - to - lymphocyte ratio as prognostic markers in patients undergoing resection of pancreatic ductal adenocarcinoma . 
herman jm , jabbour sk , lin sh , et al : smad4 loss correlates with higher rates of local and distant failure in pancreatic adenocarcinoma patients receiving adjuvant chemoradiation . 
schubert s , traub f , brakensiek k , et al : cftr , spink1 , prss1 , and ctrc mutations are not associated with pancreatic cancer in german patients . 
mcwilliams rr , maisonneuve p , bamlet wr , et al : risk factors for early - onset and very - early - onset pancreatic adenocarcinoma : a pancreatic cancer casecontrol consortium ( panc4 ) analysis . 
kim m , shah a , zhang j , et al : gemcitabine resistance in cultured pancreatic tumor cells is associated with down regulation of pten and a mesenchymal phenotype . 
ferrer m , de winter jp , mastenbroek dc , et al : chemosensitizing tumor cells by targeting the fanconi anemia pathway with an adenovirus overexpressing dominant - negative fanca . 
ye k , schulz mh , long q , et al : pindel : a pattern growth approach to detect break points of large deletions and medium sized insertions from paired - end short reads . 
exome sequencing libraries were prepared with a kapa hyper prep kit , enriched using the agilent sureselectxt clinical research exome , and paired - end sequenced with an illumina hiseq 2500 to a high depth of 300  . 
rna sequencing was performed as previously reported.62 briey , rna was extracted using an rneasy kit ( qiagen ) and evaluated by the ohsu massively parallel sequencing shared resource ( mpssr ) core facility for library construction with the truseq rna access library prep kit ( illumina )  . 
30% as measured using an agilent 2100 bioanalyzer . rna was sequenced on an illumina hiseq 2500 / 4000 to generate 100 bp paired - end reads for a minimum depth of 40 million reads per sample . 
we followed the published protocol for purist subtyping33 and used the same data set as for pdassigner subtyping . tissue processing and immunostaining tumor tissue samples were xed in 10% neutral buffered formalin for 24 hours and embedded in parafn ( ffpe )  . 
ffpe sections were stained with hematoxylin and eosin , and krt5 was detected with a rabbit monoclonal antibody ( ep1601y , abcam ) and polyclonal goat anti - rabbit antibodies ( invitrogen )  . 
exposure times and signal thresholds were normalized across all images . multiplex immunohistochemistry , image acquisition , and processing multiplex ihc was performed on 5 m ffpe sections using an adapted protocol based on methodology we previously described.34 briey , slides were deparafnized and stained with hematoxylin ( s3301 , dako , santa clara , ca ) , followed by whole slide scanning at 20 magnication on an aperio at2 ( leica biosystems , wetzlar , germany )  . 
slides were digitally scanned following each chromogen development . scanned images were registered in matlab version r2018b using the surf algorithm in the computer vision toolbox ( the mathworks , inc , natick , ma )  . 
image processing and cell quantication were performed using fiji ( fiji is just imagej ) cellproler version 3.5.164 and fcs express 6 image cytometry ruo ( de novo software , glendale , ca )  . aec signal was extracted for quantication and visualization in fiji using a custom macro for color deconvolution . 
 ( a ) krt ( magenta ) and cd45 ( teal ) expression and selected rois ( yellow rectangles ) used for mihc analyses of tumors ( scale bars represent 5 mm )  . 
 predisposing germline mutations in young patients with squamous cell cancer of the oral cavity introduction squamous cell carcinoma ( scc ) of the oral cavity ( oscc ) , and especially scc of the oral tongue ( otscc ) , is a malignancy associated with poor survival rates , with established risk factors considered to include advanced age , male gender , human papillomavirus ( hpv ) infection , and tobacco and alcohol abuse.1 , 2 scc of the oral cavity has been described as part of the phenotypic spectrum of rare bone marrow failure syndromes , that is , dyskeratosis congenita ( dc ) and fanconi anemia ( fa )  . 
 in particular , among patients with fa carrying biallelic mutations in a number of genes , as well as among patients with dc carrying mutations in genes that are involved in telomere maintenance , head and neck scc ( hnscc ) is the most frequent solid tumor diagnosed.3 , 4 patients with fa , in particular , face a 100 - fold risk for scc , compared with the general population.5 , 6 although there are few reports describing familial aggregation and patients with hereditary oscc , the actual genetic predisposition of oscc has never been thoroughly assessed , especially in individuals who lack the traditional risk factors . 
 considering that early age at cancer diagnosis is a hallmark of genetic predisposition in most cancer types , we sought to elucidate the possible germline gene defects by implementation of a comprehensive cancer gene panel in a highly selected cohort of young patients diagnosed with oscc . 
the yocc study was approved by the review board of attikon university hospital and evangelismos general hospital , and the bioethics committee of the national center for scientific research demokritos in compliance with the 1975 helsinki declaration . 
patient clinical characteristics and survival status are listed in table 1 . genetic analysis genomic dna was used to produce indexed libraries to target the sequence of 94 cancer predisposing genes using the trusight cancer panel ( illumina , san diego , ca ) following manufacturers instructions . 
odds ratios were calculated using fishers exact test . results prevalence of germline loss - of - function mutations germline loss - of - function mutations in three genes , namely , cdkn2a , sdhb , and recql4 , were identified in 13.3% ( four of 30 ) of the individuals tested . 
patients were followed for a median of 40.1 months , with one third of them ( 10 of 30 ) having died or being diagnosed with a relapse . cdkn2a mutations were the most prevalent because they were detected in two nonrelated patients . 
moreover , sdhb protein expression was retained on the tumor sample of patient ot - 2 after immunohistochemistry staining , also indicating that sdhb mutation was not directly related to his cancer diagnosis . associations between detected loss - of - function alleles per gene were compared with the exac data , as already described ( results are listed in table 3 )  . 
 although our results reached statistical significance , the cis were quite wide , mainly because of a small number of patients in our study ; therefore , these associations should be considered with caution . 
its design aimed to look beyond the usual risk factors for oscc , thus investigating a selected cohort composed of young , non alcohol drinking , nonhpv - infected patients with otscc . 
approximately , one in seven patients in our cohort carried a loss - of - function mutation in genes ( cdkn2a , sdhb , and recql4 ) known to be associated with various forms of cancer , the most prevalent being cdkn2a mutations . 
although not surprising , because none of the individuals included in the study had a clinical diagnosis of fa and therefore a prior diepoxybutane induced chromosome breakage test had not been ordered , it is possible that monoallelic mutations in the fa - associated genes are not associated with higher head and neck cancer incidence . individuals with sdhb mutations are known to face a lifetime risk of developing paragangliomas reaching 70% by the age of 80 years , 9 whereas they develop renal cell carcinomas , gastrointestinal stromal tumors , and pheochromocytomas.10 however , biallelic recql4 mutations cause rothmund - thomson syndrome , mainly characterized by poikiloderma , skeletal abnormalities , and increased risk of osteosarcoma.11 to our knowledge , mutations in these genes have never been reported before in patients with oscc and of course it is likely that these findings are purely incidental . 
although a direct association with tumorigenesis cannot be made , the genomic instability caused by the malfunction of these genes can be considered of importance . germline cdkn2a mutation carriers are known to have an elevated lifetime risk of melanoma and pancreatic cancer.12 although there have been previous case reports describing individuals diagnosed with hnscc in families carrying cdkn2a mutations , 13 a clear association , followed by clinical guidelines , has never been made . 
the high rate of somatic cdkn2a mutations and the high frequency of cdkn2a disruption detected in hnscc , 14 , 15 along with its critical role in tumor suppression , further support a potential role in hnscc initiation and development , while highlighting cdkn2a as an ideal candidate for hnscc susceptibility . 
interestingly , none of the cdkn2a carriers identified in this study seem to have a local or distant recurrence after approximately 5 and approximately 8 years of follow - up . 
there is a definite association of the initial tumor staging ( both t1n0 ) with improved survival , but an association of mutation status can also be assumed , which should be investigated further . the main limitation of our study lies in the small number of patients . 
furthermore , the lack of evaluation of genes known to be associated with dc , which might be of importance in this cohort of highly selected patients , is also considered a limiting factor . this study suggests a possible genetic predisposition in a small but notable fraction of young , apparently sporadic , oral patients with scc . 
 although , through the findings of this study , cdkn2a is proposed as a candidate gene , further studies are essential to establish its possible causative role and its inclusion in genetic analysis , whereas larger - scale analyses are imperative for defining the susceptibility gene spectra for oral scc . 
patel sc , carpenter wr , tyree s , et al : increasing incidence of oral tongue squamous cell carcinoma in young white women , age 18 to 44 years . 
goldstein am , chan m , harland m , et al : high - risk melanoma susceptibility genes and pancreatic cancer , neural system tumors , and uveal melanoma across genomel . 
ricketts cj , forman jr , rattenberry e , et al : tumor risks and genotype - phenotype - proteotype analysis in 358 patients with germline mutations in sdhb and sdhd . 
gaal j , stratakis ca , carney ja , et al : sdhb immunohistochemistry : a useful tool in the diagnosis of carney - stratakis and carney triad gastrointestinal stromal tumors . 
reed al , califano j , cairns p , et al : high frequency of p16 ( cdkn2 / mts - 1 / ink4a ) inactivation in head and neck squamous cell carcinoma . 
hoang , md1 , 2 ; rui yang , md1 , 2 ; daniel weiser , md2 ; jonathan morris , md3 ; richard gorlick , md4 ; jonathan b . 
we have identied a single patient who was initially diagnosed with a benign osteoblastoma and subsequently presented years later with a high - grade osteosarcoma in the same anatomic region . 
a biopsy sample of the mass demonstrated conventional - type osteoblastoma with focal epithelioid features for which the patient underwent intralesional curettage ( fig 2 )  . subsequent imaging demonstrated a persistent abnormal signal in the sacrum , and a plan of continued surveillance was agreed upon . 
over the ensuing 4 - year imaging failed to demonstrate appreciable period , radiographic change , and the patients clinical course remained stable . five years later , the patient returned with increasing paimaging demonstrated an increase in the size of the mass , and an urgent open sacral biopsy was performed ( fig 3 )  . 
staging studies performed at that time were negative for distant disease . neoadjuvant chemotherapy was started in accordance with childrens oncology group protocol aost0331 ; however , because of severe pain , patient required semi - urgent surgical intervention and did not complete planned neoadjuvant treatment . 
the decision was made to manage conservatively , and as of july 2019 , surveillance demonstrated no evidence of disease . methods including the osteoblastoma , patient consent and institutional review board approval were obtained before study initiation . 
sequencing and data analysis were performed by novogene technology ( beijing , china ) to evaluate for structural variants , copy number variation , single nucleotide variants , and insertions / deletions . 
germline - matched comparison from each tumor was undertaken to evaluate for somatic changes . to evaluate for pathogenic variants , somatic analysis on small variants focused on changes that would elicit a coding or splice site change and were not common polymorphisms ( allele frequency , 0.01 in 1 , 000 genomes and exac databases )  . 
furthermore , we evaluated whether any variants were found in cancer mutational hotspots ( recurrence of more than ve in cosmic [ catalog of somatic mutations in cancer ] ) or were a truncating variant in a known tumor suppressor gene ( cancer gene census )  . 
 geller et al context key objective does genomic analysis of a patient who was initially diagnosed with a benign osteoblastoma and subsequently presented years later with a high - grade osteosarcoma in the same anatomic region demonstrate evidence of malignant transformation ? knowledge generated there was near - zero overlap in the somatic small variants , somatic copy number variation pattern , and predicted structural variants in the osteoblastoma compared with the osteosarcoma . 
findings from this study argue against malignant transformation as an evolving or stepwise process and conversely support two distinct neoplasms with dissimilar genetic makeups . relevance this study performed an in - depth genetic characterization of two distinct tumors that historically have been believed to be along the same spectrum of disease . 
in addition , a germline mutation in brip1 was discovered , which lends itself to additional investigation . pathogenic or likely pathogenic for a cancer predisposition syndrome . results whole - genome sequencing resulted in high - quality data , which generated an average 63 million reads per tumor , with more than 98% usable on the basis of quality metrics . 
after ltering and duplicate removal , mapping to hg19 resulted in an average sequencing depth of 29 and 32 for the benign and malignant tumors , respectively , and at least 4 coverage in more than 99% of the genome . somatic variant analysis revealed approximately 98 , 000 and 141 , 000 high - condence small variants in the benign and malignant tumor , respectively , which corresponded to somatic mutational burdens of 33 and 47 mutations / megabase ( mb )  . 
in the osteosarcoma , a single variant recurrent in cosmic of unclear oncologic signicance , znf429 p.n426k , was found as well as truncating mutations in two tumor suppressor genes , daxx and ncor1 . structural and copy number variation analysis revealed signicant alterations in both tumors . 
a striking number of somatic inversion events were found in both tumors ( approximately 1 , 750 per tumor ) , particularly compared with other structural changes , such as translocations , deletions , or tandem duplications ( each approximately 10 to 30 per tumor )  . 
 ( a ) a 2015 hematoxylin and eosinstained low - power ( 10 ) micrograph demonstrates ndings consistent with high - grade osteosarcoma , including high cellularity , multiple foci of tumor necrosis , and osteoid formation . 
 ( b ) a 2015 hematoxylin and eosinstained high - power ( 40 ) micrograph that demonstrates pleiomorphic and bizarre cellular features . overlap in the predicted structural variants in the osteoblastoma compared with the osteosarcoma . germline analysis using the methods described identied a single pathogenic germline mutation , brip1 r798x , identied with high condence in all three samples . 
a summary of genomic ndings is listed in table 1 . discussion the notion that osteoblastoma can undergo malignant transformation to osteosarcoma dates back to an original report in 1967.1 since then , 24 cases have appeared in the literature , none of which investigated the transformation event on a genomic level1 - 20 ( table 2 )  . 
given the lack of objective genetic data and short time to transformation in some cases , there is a distinct possibility that some of these reports represent coincidence or diagnostic error . a few prior reports have attempted to document malignant transformation through a limited analysis of sequential biopsies samples.4 , 18 , 21 however , these tumors were characterized only in terms of ploidy , thereby limiting understanding of the transformation process.4 , 18 , 21 although these reports suggested that transformation is associated with an increase in dna content , only one patients tumor showed an observable change in dna content over time . moreover , in the current study , we have demonstrated the benign and malignant tumors to have distinct genomic proles with almost no overlap in somatic changes . 
whether these tumors are driven in part by an unrecognized anatomic predisposition remains speculative . we also identied a germline mutation in the brip1 tumor suppressor gene , a member of the recq helicase family associated with brca1.22 , 23 brip1 mutations are associated with a predisposition to breast cancer , ovarian cancer , and fanconi anemia , 22 , 24 , 25 and brip1 is known to play a critical role in dna repair , with knockdown leading to chromosomal instability.26 of note in our patient , both the benign and the malignant tumors exhibited a higher - thantypical somatic mutation rate compared with most pediatric malignancies27 as well as a high number of structural variants with a preponderance of inversion events , which suggests a functional role of this germline nding . 
we have speculated that these changes may have accumulated because of brip1 partial dysfunction that led to chromoinstability and impaired dna crosslink repair.26 somal admittedly , denitive conclusions cannot be drawn on the basis of a single patient , and additional investigation seems warranted . although osteoblastoma infrequently has been associated with mutations involving rb , tp53 , fos , fosb , d - jun , and mdm2 , the genetic landscape of this tumor is still largely unknown.28 - 31 the osteoblastoma in this report is similar to previous reports in that we observed many structural table 1 . 
many osteosarcomas demonstrate chromosomal abnormalities that commonly involve tumor suppressor genes or dna helicases.32 , 33 however , osteosarcoma generally is recognized as exhibiting tremendous genetic complexity with no clearly identiable genetic driver . this heterogeneity may stem from chromothripsis , 34 - 36 markers of which have been described in 2% to 3% of all cancers and up to 33% of osteosarcomas . 
although the current case did not exhibit evidence of chromothripsis , it demonstrates an otherwise typical genomic prole for osteosarcoma with a high degree of chromosomal instability , increased ploidy , and truncating point mutations in several tumor suppressor genes . in some cases , in conclusion , although malignant transformation of osteoblastoma to osteosarcoma historically has been accepted , review of the literature has revealed a paucity of convincing evidence , and controversy has persisted . 
to our knowledge , this study is the rst to report an in - depth genetic characterization of two distinct tumors within the same patient and the same anatomic location . 
findings from this study argue against malignant transformation as an evolving or stepwise process and conversely supports two distinct neoplasms with dissimilar genetic makeups . this report also has uncovered a germline truncating mutation in brip1 in this patient , which raises the question of whether this serves as an underlying predisposition for both tumors . 
geller , md , monteore greene medical arts pavilion , 3400 bainbridge ave , bronx , ny 10467 ; e - mail : dgeller@monteore.org. support supported by clinical and translational science awards catalytic seed grant ul1 tr001073 ( d.s.g. ) from the national center for advancing translational sciences , a component of the national institutes of health . the content is solely the responsibility of the authors and does not necessarily represent the ofcial views of the national institutes of health . 
j bone joint surg am 57 : 424 - 426 , 1975 stutch r : osteoblastomaa benign entity ? orthopaed rev 4 : 27 , 1975 grace j , mccarthy s , stankovic r , et al : malignant transformation of osteoblastoma : study using image analysis microdensitometry . 
 genomic analysis does not support malignant transformation kunze e , enderle a , radig k , et al : aggressive osteoblastoma with focal malignant transformation and development of pulmonary metastases . 
sun x , brieo - enrquez ma , cornelius a , et al : fancj ( brip1 ) loss - of - function allele results in spermatogonial cell depletion during embryogenesis and altered processing of crossover sites during meiotic prophase i in mice . 
weber - lassalle n , hauke j , ramser j , et al : brip1 loss - of - function mutations confer high risk for familial ovarian cancer , but not familial breast cancer . 
radig k , schneider - stock r , mittler u , et al : genetic instability in osteoblastic tumors of the skeletal systepathol res pract 194 : 669 - 677 , 1998 31 . 
lorenz s , bary t , sun j , et al : unscrambling the genomic chaos of osteosarcoma reveals extensive transcript fusion , recurrent rearrangements and frequent novel tp53 aberrations . 
 contributed equally to this work . ( continued ) purpose alk ( anaplastic lymphoma kinase ) rearrangements predict for sensitivity to alk tyrosine kinase inhibitors ( tkis ) ; however , responses to alk tkis are generally short lived . 
although multiple studies support the clinical benefits of repeat tissue sampling , the clinical utility of longitudinal circulating tumor dna analysis has not been established in alk - positive lung cancer . patients and methods we used a 566 - gene hybrid - capture next - generation sequencing assay to perform a longitudinal analysis of plasma specimens from 22 alk - positive patients with acquired resistance to alk tkis to track the evolution of resistance during treatment . 
to determine tissueplasma concordance , we compared plasma findings with the results of repeat biopsies . results at disease progression , we detected an alk fusion in plasma from 19 ( 86% ) of 22 patients and identified alk resistance mutations in plasma specimens from 11 patients ( 50% )  . 
alk g1202rthe most frequent plasma mutation detected after progression on a second - generation tkiwas consistently suppressed during treatment with lorlatinib . conclusion plasma genotyping by next - generation sequencing is an effective method for detecting alk fusions and alk mutations in patients who experience disease progression on alk tkis . 
2018 by american society of clinical oncology introduction oncogenic rearrangements that result in the constitutive activation of anaplastic lymphoma kinase ( alk ) define a molecular subtype of nonsmalllung cancer ( nsclc ) that is characterized by sensitivity to alk tyrosine kinase inhibitors ( tkis ) .1 , 2 since the identification of alk rearrangements in nsclc in 2007 , four tkis have become standard therapies for patients with advanced disease.3 - 6 although these tkis have significantly improved clinical outcomes , most patients experience relapse within 1 to 2 years.1 despite a shared molecular driver , the magnitude of benefit from tki treatment varies widely between patients . 
repeat biopsies upon disease progression have been instrumental in elucidating the molecular mechanisms that drive resistance to alk inhibitors , including the distinct spectrum of alk mutations associated with resistance to each tki7 ; however , repeat biopsies may be challenging to obtain and single - site sampling may not capture the spatial heterogeneity of resistance mechanisms . analysis of circulating tumor dna ( ctdna ) is an emerging approach for tumor genotyping . 
shaw , md , phd , department of medicine , massachusetts general hospital , 32 fruit st , boston , ma 02114 ; e - mail : ashaw1@ partners.org. as plasma sampling is minimally invasive and ctdna may be derived from all metastatic sites , longitudinal monitoring of genetic alterations in ctdna may overcome many of the limitations of tissue sampling . 
 libraries were constructed with illumina truseq nano dna library prep kit ( illumina , san diego , ca ) , enriched for a 566 - gene pancancer gene panel ( data supplement ) by using agilent sureselect xt custom baits ( agilent technologies , santa clara , ca ) , and sequenced on an illumina hisequation 2500 sequencer to a median of 105 million reads , which yielded a median coverage of 1 , 195.18 sequence data were aligned to the hg19 reference genome . 
those with at least four alternate reads were retained on the basis of a calculated background mutation rate and false - positive rate of 1e - 4 and 1e - 6 , respectively . 
ctdna insufficient for analysis indicates those samples that were technically successful , but had insufficient tumor dna present in the plasma to reliably estimate underlying tumor genotype . longitudinal ctdna analysis ( n = 79 ) disease progression on study ( n = 29 ) ctdna analysis successful ( n = 22 ) ctdna insufficient for analysis ( n = 7 ) 23 repeat biopsies attempted for 20 patients * repeat biopsy not attempted ( n = 2 ) tissue insufficient ( n = 7 ) tissue sufficient ( n = 16 ) inaccessible site ( n = 1 ) patient preference ( n = 1 ) * three patients underwent tissue sampling twice during plasma surveillance patients with cns - only progression patients with isolated intrathoracic disease progression patients with isolated progression of a liver lesion ( n = 1 ) ( n = 5 ) ( n = 1 ) three of six attempted repeat biopsies sufficient for analysis results patient characteristics that were administered is depicted in the data supplement and figure 2 . plasma was longitudinally collected from 79 patients with metastatic , alk - positive nsclc ( fig 1 )  . 
as this study was primarily focused on investigating the role of ctdna analysis at disease progression , this report is limited to patients who had progressive disease and analyzable plasma specimens . 
of the seven patients who did not have detectable ctdna , one patient experienced cns - only progression , five patients had intrathoracic progression , and one patient had liver oligoprogression ( fig 1 )  . 
baseline characteristics of the 22 patients and their treatment histories are summarized in table 1 , figure 2 , and the data supplement . plasma genotyping was performed on 88 plasma samples from 22 patients . 
the temporal relationship between plasma collection and the treatments concordance between tissue and plasma genotypes we first evaluated concordance between tissue and plasma genotyping for alk fusions , alk mutations , and non - alk alterations . 
 ( % ) of alk tkis before initial plasma collection * abbreviation : alk , anaplastic lymphoma kinase ; tki , tyrosine kinase inhibitor . * the total number of alk tkis on which a patient had experienced progression before the collection of the initial plasma specimen . 
in instances where plasma was collected during sequential treatment with distinct alk inhibitors , the line of therapy at initial plasma collection is represented . ( 94% ; appendix fig a1 )  . 
among the 12 patients for whom the fusion partner was known and an alk fusion was detected in the plasma , there was 100% agreement between tissue and plasma fusion calls ( fig 3a )  . 
point mutations in the alk kinase domain were identified in plasma specimens from 11 patients ( 50% ) , five of whom had paired biopsies at the time of mutation detection ( fig 3b )  . 
three patients had multiple alk mutations . all tissue - detected alk mutations were also identified in corresponding plasma samples , and all plasma - detected alk mutations were also present in paired biopsies . 
 among 17 patients who had plasma collected during progression on a second - generation alk inhibitorthat is , ceritinib , alectinib , or brigatinibplasma alk mutations were identified in eight patients ( 47% ; data supplement ) , including i1171n ( n = 1 ) , g1202r ( n = 5 ) , i1171n / g1202r ( n = 1 ) , and e1210k ( n = 1 )  . 
 the observed frequency of plasma alk mutations is consistent with our previous analysis of resistance biopsies from patients who developed resistance to second - generation inhibitors , which included five patients from the current plasma cohort.7 non - alk alterations . 
as we did not detect any differences in tissue alterations that were identified in serial specimens from the three patients who underwent multiple biopsies , we restricted the concordance assessment to one biopsy per individual . 
although we were not able to obtain tissue after the patient had developed progression on lorlatinib , amplification was not present when a prelorlatinib liver biopsy was assessed using the same 566gene panel . 
despite high - level met amplification ( > 25 copies ) in tissue , we did not detect met amplification in the corresponding plasma specimen ; however , as the maximum allelic frequency ( af ) of detected alterations in the plasma of mgh939 was approximately 2% , the degree of amplification was below the limit of detection of the assay . evolution of resistance during molecular surveillance alk fusion kinetics and correlation with disease status . 
preclinical models and case reports suggest that the presence of a specific alk mutation in a tki - resistant tissue specimen may predict response to subsequent alk tkis1 , 7 , 23 ; therefore , we analyzed plasma specimens from patients with alk mutations who received treatment with additional alk tkis to evaluate the potential of using plasma findings to inform sequential therapies . 
during the follow - up period , seven of these patients ( 88% ) went on to receive treatment with a tki that targeted the alk mutation ( data supplement )  . 
 detected in plasma only detected in plasma and tissue mutation no paired biopsy paired biopsy available detected in plasma only detected in plasma and tissue eml4 - alk variant 1 variant 2 variant 3 variant 5 i1171n f1174c f1174l g1202r d1203n e1210k fig 3 . 
parentheses denote patients for whom the alk mutation was considered the dominant resistance mechanisfor patients without paired biopsies , alk mutations that were detected at the time of progression on an alk tyrosine kinase inhibitor are listed . 
because the mutations were separated by too many bases , the allelic relationship ( cis v trans ) could not be determined for mgh990s alk mutation . in alk i1171n af from 4.5% to undetectable after 6 weeks ( fig 4a )  . 
one patient ( mgh989 ) underwent microwave ablation to treat a liver lesion with a biopsy - proven g1202r mutation and continued treatment with alectinib for an additional 6 months . 
 mgh990 had a radiographic response to treatment , but we could not evaluate the molecular response as we were only able to collect a single plasma specimen . although the g1202r mutation was suppressed in plasma during the treatment with lorlatinib , two of the four patients with plasma - detected g1202r developed progressive disease soon after initiating lorlatinib ( appendix fig a3 )  . 
we were not able to obtain a biopsy , but plasma analysis demonstrated an increase in copy number of gnas and bcl2l1 and a marked increase in the af of mutations that involved other genes during treatment ( fig 5 )  . 
in both cases , eml4 - alk fusion af increased at progression despite the suppression of alk mutations , which supports the notion that resistance was independent of genetic alk alterations . discussion despite a shared molecular driver , the clinical course is variable for patients with alk - positive nsclc treated with alk tkis . 
our findings highlight the potential clinical utility of hybrid - capture ngs for improving our understanding of the molecular drivers of resistance . in our cohort of patients , 76% of plasma samples contained sufficient tumor - derived dna for molecular analysis compared with 65% of biopsy specimens , which confirms that both are reliable approaches . 
 furthermore , our observation that the presence of specific plasma alk mutations correlated with the response and resistance to distinct alk tkis lends support to the emerging practice of using alk mutations to inform the selection of alk tkis . although tissue sampling is the gold standard for molecular analysis , sampling a single site of disease may overestimate the contribution of a particular alteration to the resistant phenotype . 
for example , we detected an alk g1202r mutation at 50% af in a progressing liver lesion , which suggested that it was a major contributor to alectinib resistance in the case of mgh919 . 
in contrast , the plasma g1202r af of 1% was less than the af of other plasma - detected molecular alterations , including multiple non - alk alterations ( fig 5 )  . 
moreover , this case reinforces the notion that the analysis of liquid biopsies may be more informative than tissue - based genotyping in certain situations . to date , the study of resistance to alk therapeutics has primarily focused on alk mutations . 
figure illustrates the change in the allelic fraction of eml4alk and alk mutations during sequential treatment with next - generation alk inhibitors for ( a ) mgh987 and ( b ) mgh087 . 
 ( a ) allelic fraction of alk ( anaplastic lymphoma kinase ) fusion ( blue ) , alk mutations ( red and gold ) , and non - alk alterations ( gray ) during treatment with sequential alk inhibitors . 
despite these shortcomings , our data suggest that the quantitative assessment of structural variants may be clinically useful and complementary to radiographic assessment in some patients . overall , our data confirm that plasma genotyping by using hybrid - capture ngs technology can reliably detect alk fusions and alk resistance mutations in patients with alk - positive nsclc ; however , there are several limitations of this study , including the small size of our cohort , inconsistent sampling intervals that led to variation in the duration of follow - up after and before disease progression , and the inability to obtain pretreatment plasma and paired biopsies for all patients . 
furthermore , as a result of the small contribution of tumor dna to total cellfree dna in most patients , we cannot definitively exclude the presence of undetected amplification events at resistance . 
as identifying alk resistance mutations is emerging as an important consideration for the management of alk - positive nsclc , we anticipate that genotyping plasma to characterize resistance to alk tkis will also become a routine part of patient care . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ibiayi dagogo - jack consulting or advisory role : boehringer ingelheim honoraria : foundation medicine a . 
campbell employment : novartis , pfizer ( i ) manuscript writing : all authors stock and other ownership interests : novartis final approval of manuscript : all authors accountable for all aspects of the work : all authors jessica j . 
schultz no relationship to disclose jennifer ackil no relationship to disclose sara stevens no relationship to disclose leila dardaei no relationship to disclose satoshi yoda no relationship to disclose harper hubbeling no relationship to disclose subba r . 
sequist honoraria : astrazeneca consulting or advisory role : astrazeneca , genentech , bristol - myers squibb , pfizer research funding : boehringer ingelheim ( inst ) , clovis oncology ( inst ) , genentech ( inst ) , merrimack pharmaceuticals ( inst ) , novartis ( inst ) , astrazeneca ( inst ) , johnson & johnson ( inst ) , merck ( inst ) , pfizer ( inst ) inga t . 
lennes honoraria : blue cross and blue shield of massachusetts consulting or advisory role : kyruus anthony john iafrate stock and other ownership interests : archer biosciences consulting or advisory role : debiopharm group , constellation pharmaceuticals , chugai pharma , roche research funding : blueprint medicines patents , royalties , other intellectual property : archerdx exclusive license to amp technology rebecca s . 
heist consulting or advisory role : boehringer ingelheim research funding : glaxosmithkline , sanofi , abbvie , novartis , roche , incyte , celgene , mirati therapeutics , peregrine pharmaceuticals , exelixis , millennium pharmaceuticals , debiopharm group christopher g . 
azzoli consulting or advisory role : merck , ariad pharmaceuticals , takeda research funding : pharmamar ( inst ) , abbvie ( inst ) , astrazeneca ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , loxo ( inst ) , ignyta ( inst ) travel , accommodations , expenses : pharmamar , abbvie , stemcentrx jeffrey a . 
engelman employment : novartis stock and other ownership interests : loxo , agios , kura , gatekeeper pharmaceuticals , novartis consulting or advisory role : novartis , agios , loxo , clovis oncology , ventana medical systems , g1 therapeutics , sanofi , chugai pharma , warp drive bio , asana biosciences , emd serono , synta , allostery , genentech , aveo , biodesix , merck , cell signaling technology , endo pharmaceuticals , astrazeneca , glaxosmithkline , amgen , bristol - myers squibb , cancer progress research funding : novartis , jounce therapeutics , sanofi , araxes , astrazeneca , amgen ( inst ) patents , royalties , other intellectual property : coinventor on a patent application that has been licensed to ventana medical system / roche other relationship : third rock ventures jochen k . 
leary employment : novartis stock and other ownership interests : novartis patents , royalties , other intellectual property : patents , pending patents , and a royalty - sharing agreement with johns hopkins university alice t . 
shaw honoraria : pfizer , novartis , genentech , foundation medicine consulting or advisory role : pfizer , novartis , genentech , roche , ariad pharmaceuticals , ignyta , blueprint medicines , daiichi sankyo , emd serono , taiho pharmaceutical , ksq therapeutics research funding : pfizer , novartis , genentech justin f . 
gainor honoraria : merck , incyte , ariad pharmaceuticals consulting or advisory role : novartis , boehringer ingelheim , clovis oncology , genentech , bristol - myers squibb , theravance , loxo research funding : merck , novartis , genentech , bristolmyers squibb , adaptimmune , astrazeneca , ariad pharmaceuticals travel , accommodations , expenses : affymetrix anna f . 
farago honoraria : foundation medicine consulting or advisory role : pharmamar , merrimack pharmaceuticals , takeda , abbvie , intervention insights acknowledgment we also thank jeremy decker for assistance with plasma preparation and circulating tumor dna processing . 
shaw at , yeap by , mino - kenudson m , et al : clinical features and outcome of patients with nonsmall - cell lung cancer who harbor eml4 - alk . 
kim dw , mehra r , tan ds , et al : activity and safety of ceritinib in patients with alk - rearranged nonsmall - cell lung cancer ( ascend - 1 ) : updated results from the multicentre , open - label , phase 1 trial . 
shaw at , gandhi l , gadgeel s , et al : alectinib in alk - positive , crizotinib - resistant , nonsmallcell lung cancer : a single - group , multicentre , phase 2 trial . 
kim dw , tiseo m , ahn mj , et al : brigatinib in patients with crizotinib - refractory anaplastic lymphoma kinase - positive nonsmall - cell lung cancer : a randomized , multicenter phase ii trial . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
sacher ag , paweletz c , dahlberg se , et al : prospective validation of rapid plasma genotyping for the detection of egfr and kras mutations in advanced lung cancer . 
paweletz cp , sacher ag , raymond ck , et al : bias - corrected targeted next - generation sequencing for rapid , multiplexed detection of actionable alterations in cell - free dna from advanced lung cancer patients . 
schwaederl mc , patel sp , husain h , et al : utility of genomic assessment of blood - derived circulating tumor dna ( ctdna ) in patients with advanced lung adenocarcinoma . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
curigliano g , gmez pardo p , meric - bernstam f , et al : ribociclib plus letrozole in early breast cancer : a presurgical , window - of - opportunity study . 
ye k , schulz mh , long q , et al : pindel : a pattern growth approach to detect break points of large deletions and medium sized insertions from paired - end short reads . 
solomon b , bauer tm , felip e , et al : safety and efficacy of lorlatinib ( pf - 06463922 ) from the dose - escalation component of a study in patients with advanced alk + or ros1 + non - small cell lung cancer ( nsclc )  . 
 in two of the three patients for whom plasma analysis failed to detect a fusion , an eml4 - alk fusion ( variants 3 and 5 ) was identified in matching tissue . 
 c acquired resistance to immune checkpoint inhibitor therapy through outgrowth of cells lacking cd274 and pdcd1lg2 amplification introduction the recent introduction of immune checkpoint inhibitor ( icpi ) therapies has expanded effective treatment options for many patients with metastatic solid tumors , although typically acquired resistance develops over time . 
here , we present a patient with metastatic colon cancer in whom next - generation sequencing ( ngs ) demonstrated amplification of both cd274 , or programmed cell death ligand 1 ( pd - l1 ) , and pdcd1lg2 , or programmed cell death ligand 2 ( pd - l2 )  . 
ngs testing of the progressed tumor no longer demonstrated cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) amplification but did not identify any new genomic alterations compared with the initial tumor profile . 
 histologic examination revealed a stage iiib ( t4bn1mx ) colon adenocarcinoma , and a computed tomography ( ct ) scan of the chest , abdomen , and pelvis showed no evidence of metastatic disease . 
she received 12 doses of adjuvant fluorouracil plus leucovorin plus oxaliplatin chemotherapy . a repeat ct scan in july 2015 revealed development of a retroperitoneal soft tissue nodule , which was confirmed by biopsy to be metastatic colon adenocarcinoma . 
 in december 2015 , a ct scan showed interval enlargement of extraperitoneal tumor implants as well as numerous subcutaneous and muscular metastases . a commercial ngs assay ( foundation medicine , cambridge , ma ) was performed on the pretreatment adenocarcinoma sample and revealed gene amplification of both cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 )  . 
the total mutation burden was 11 mutations / mb , which falls in the intermediate burden category . in january 2016 , the patient began receiving intravenous nivolumab ( 3 mg / kg ) every 2 weeks . 
 after six doses , a repeat ct scan ( chest , abdomen , and pelvis ) in april 2016 showed resolution or considerable decrease in size of all nodules , both within and outside of the radiation field . 
a left supraclavicular lymph node core biopsy showed a poorly differentiated carcinoma consistent with spread from the patients known adenocarcinoma . ngs ( foundation medicine ) performed on the november 2017 supraclavicular lymph node biopsy specimen showed a similar genomic mutation profile as the 2014 primary tumor ; however , this sample lacked amplification of both cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) as well as flt3 amplification and stag - 2 p.w85l. 
no new alterations were reported , and the total mutation burden was 11 mutations / mb . discussion in 2017 , we first reported this patient with proficient dna mismatch repair metastatic colorectal cancer whose tumor responded dramatically to an icpi.2 icpis are now routinely used as firstor second - line metastatic disease therapies for patients with a variety of cancer types , including deficient mismatch repair expressing microsatellite instabilityhigh colorectal cancer , where the response rate is roughly 40%.3 there is existing literature that pd - l1 gene amplification can be a predictive marker for checkpoint inhibitor therapy efficacy.4 ikeda et al5 reported a patient with metastatic basal cell carcinoma to the liver who had an exceptional response to nivolumab . 
in addition , in patients with nonsmall - cell lung cancer , clav et al6 demonstrated pd - l1 gene amplification resulting in high pd - l1 expression , a confirmed biomarker for effective checkpoint inhibitor therapy . 
pd - l1 expression seen at the time of initiation of the effective checkpoint inhibitor therapy and no longer demonstrated in the progressive disease would be supportive evidence that pd - l1 gene amplification was not only a biomarker of efficacy but also related causally to the efficacy of the checkpoint inhibitor , given the mechanism of action of the checkpoint inhibitor used ( inhibiting the programmed death pathway ligand )  . we reasoned that our patients tumor responded to an icpi , because ngs testing demonstrated amplification of both cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) , and the mechanism for this therapy is to elicit a cytotoxic immune response by inhibiting the programmed death pathway ligands ( pd - l1 and pd - l2 )  . 
unlike pd - l1 protein expression , amplification of pd - l1 and pd - l2 in cancer is rare and most likely to be detected by routine clinical ngs testing rather than fluorescent in situ hybridization assays . 
routine screening for pd - l1 and pd - l2 amplification would be costly from a time , financial , and tissue perspective , only to show a low rate of cases with gene amplifications . 
the ability of any ngs assay to detect gene amplifications is dependent on the bait set design of the assay , quality of extracted dna , adequacy of tumor content , and depth of coverage . 
in cases where pd - l1 / pd - l2 amplifications are suspected but ngs quality metrics are suboptimal , fluorescent in situ hybridization testing should be considered as an orthogonal assay to confirm gene amplifications . 
for example , overman et al8 recently reported that in patients with deficient mismatch repair expressing metastatic colorectal cancers , indirect comparisons suggest combination therapy provides improved efficacy relative to anti - program death 1 monotherapy.8 ( p773 ) studies of secondary or acquired resistance to icpi therapy have been reported . 
the authors of a recent review wrote that mechanisms of resistance to icpis include somatic mutations in antigen processing and presentation as well as upregulation of genes involved in cell adhesion , angiogenesis , and extracellular matrix remodeling . 
they also note the potential to target mechanisms of resistance such as an angiogenic phenotype and defects in interferon signaling pathways.9 it seems likely that our patients cancer that progressed in the supraclavicular area was due to the selection and outgrowth of a small population of tumor cells ( subclones ) that did not harbor cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) amplification . 
during the 8 months of checkpoint inhibitor therapy , those subclones became the predominant population because , on repeat ngs testing , no additional genomic alterations were identified , and the cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) amplifications were not detected . because there has been no tumor progression outside the supraclavicular area , it is possible that the supraclavicular area was the only site of subclones lacking cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) amplifications . 
finally , we hypothesize that combination therapies targeting both cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) amplified and nonamplified cell populations might have resulted in a more durable response . in conclusion , on the basis of ngs testing of our patients progressive disease after icpi treatment , resistance to icpi therapy was likely due to the selection and outgrowth of subclones lacking cd274 ( pd - l1 ) and pdcd1lg2 ( pd - l2 ) amplifications . 
sorscher s , resnick j , goodman m : first case report of a dramatic radiographic response to a checkpoint inhibitor in a patient with proficient mismatch repair gene expressing metastatic colorectal cancer . 
inoue y , yoshimura k , mori k , et al : clinical significance of pd - l1 and pd - l2 copy number gains in non - small - cell lung cancer . 
ikeda s , goodman am , cohen pr , et al : metastatic basal cell carcinoma with amplification of pd - l1 : exceptional response to anti - pd1 therapy . 
lee ck , kim s , lee js , et al : next - generation sequencing reveals novel resistance mechanisms and molecular heterogeneity in egfr - mutant non - small cell lung cancer with acquired resistance to egfr - tkis . 
overman mj , lonardi s , wong kym , et al : durable clinical benefit with nivolumab plus instability - high metastatic in dna mismatch repair - deficient / microsatellite ipilimumab colorectal cancer . 
chen pl , roh w , reuben a , et al : analysis of immune signatures in longitudinal tumor samples yields insight into biomarkers of response and mechanisms of resistance to immune checkpoint blockade . 
 discordance in human epidermal growth factor receptor 2 ( her2 ) phenotype between primary tumor and circulating tumor cells in women with her2 - negative metastatic breast cancer purpose discordance in human epidermal growth factor receptor 2 ( her2 ) status between primary tumor and metastases might have important implications for treatment response and therapy decisions . 
here , we evaluate both the frequency of circulating tumor cells ( ctcs ) and the factors predicting her2 discordance between primary tumor and ctcs as a potential surrogate for tumor biology and tumor heterogeneity in patients with metastatic breast cancer . patients and methods the number of ctcs in 7.5 ml of peripheral blood and her2 status were evaluated in 1 , 123 women with her2 - negative metastatic breast cancer . 
2017 by american society of clinical oncology introduction circulating tumor cells ( ctcs ) are observed in early and metastatic breast cancer ( mbc ) , and their prognostic relevance has been demonstrated in both early and advanced disease.1 , 2 according to previous studies , approximately 65% to 85% of patients with mbc have detectable ctcs , and approximately half of these patients have five or more ctcs in 7.5 ml of peripheral blood.2 , 3 in addition to the prognostic value of ctcs as assessed before treatment , monitoring ctc dynamics during therapy provides important information on therapy response.4 - 7 however , valuable information with regard to therapy response and suitability of additional treatment options may be provided not only by the prevalence and changes in the number of ctcs but also by the phenotype of ctcs . 
friedl jens huober christoph scholz nikolaus de gregorio brigitte rack elisabeth trapp marianna alunni - fabbroni sabine riethdorf volkmar mueller andreas schneeweiss klaus pantel franziska meier - stiegen bernadette jaeger andreas hartkopf florin - andrei taran peter a . 
assessing ctc phenotype may be especially important in mbc , because it can be used as a noninvasive liquid biopsy to characterize the metastatic disease , thus reflecting tumor heterogeneity and possible discordance in hormone receptor and / or human epidermal growth factor receptor 2 ( her2 ) expression with potentially far - reaching implications in terms of follow - up treatment and additional targeted therapies . although discordance in her2 status among primary tumor , distant metastases , and ctcs has been described in several studies , 3 , 8 - 10 it has not been implemented in clinical practice to guide therapy decisions . 
the study concept was in accordance to the declaration of helsinki , adhered to good clinical practice and german pharmaceutical law , and was approved by the local ethic committees of the participating centers . assessment of ctc presence and her2 phenotype on ctcs from all patients , 7.5 - ml peripheral blood samples were collected , and presence and phenotype of ctcs were assessed as previously described in detail , 11 using the semiautomatic and standardized cellsearch system ( janssen diagnostics , raritan , nj ) , which is the only us food and drug administrationapproved method for the enumeration of ctcs . 
for her2 assessment , cells were also labeled with her2 antibodies , and ctcs were considered as her2 positive only if they showed a strong ihc staining intensity for her2 ( ihc score , 3 + )  . 
analyses for determining ctc prevalence and her2 phenotype of ctcs were performed by trained scientists with a peer - review system at four independent reference laboratories . statistical calculations descriptive statistics for the categorical data are provided in terms of absolute and relative frequencies . 
the non - normally distributed continuous variables age ( in years ) and time interval between primary diagnosis and screening ( in months ) are described by medians and ranges . 
associations between presence of ctcs or presence of her2 - positive ctcs and patient or tumor characteristics were evaluated using mann - whitney u tests for age and time interval between primary diagnosis and screening , and x2 tests were used for all other categorical variables . 
to assess which factors predicted discordance in the her2 phenotype between primary tumor and ctcs , we used a multivariable logistic regression model with discordance in her2 status ( yes v no ) as a binary response variable and a stepwise backward selection procedure ( significance level cutoff for exclusion , .05 [ likelihood ratio test ] )  . 
demographic and primary tumor characteristics of patients with her2negative mbc screened for ctcs within the detect study program ( n = 1 , 123 ) characteristic age at screening , years total no . 
 ( % ) of patients time between primary diagnosis and screening , months median range median range menopausal status at screening premenopausal postmenopausal unknown tumor stage unknown nodal stage unknown histologic grade unknown histologic type invasive ductal invasive lobular other hormone receptor status negative positive unknown 26 - 89 0 - 450 136 ( 12.1 ) 734 ( 65.4 ) 253 ( 22.5 ) 308 ( 27.4 ) 503 ( 44.8 ) 114 ( 10.2 ) 125 ( 11.1 ) 13 ( 1.2 ) 60 ( 5.3 ) 363 ( 32.3 ) 378 ( 33.7 ) 147 ( 13.1 ) 136 ( 12.1 ) 99 ( 8.8 ) 47 ( 4.2 ) 576 ( 51.3 ) 406 ( 36.2 ) 94 ( 8.4 ) 751 ( 66.9 ) 199 ( 17.7 ) 173 ( 15.4 ) 171 ( 15.2 ) 886 ( 78.9 ) 66 ( 5.9 ) had hormone receptorpositive invasive ductal tumors . 
median number of ctcs detected in ctc - positive patients was seven ( interquartile range , two to 30 ; range , one to 35 , 078 ctcs )  . 
frequency distribution of the number of ctcs detected is shown in appendix figure a1 . presence of at least one ctc was significantly associated with nodal stage and histologic type of the primary tumor but not with other patient or primary tumor characteristics ( table 2 )  . 
in 158 patients ( 22.2% ) , at least one ctc with an her2 2 + ihc score , but no ctcs with an her2 3 + ihc score , was detected ; these patients were not considered to have her2 - positive ctcs in the blood ( as described in patients and methods )  . 
patients with grade 3 primary tumors were less likely to have her2 - positive ctcs than patients with grade 1 or 2 primary tumors ( p = .028 ; fig 3a )  . 
patients with invasive lobular primary tumors were more likely to have her2positive ctcs than patients with other primary tumor histologic types ( p , .001 ; fig 3b ) , and patients with hormone receptorpositive primary tumors were more likely to have her2 - positive ctcs than patients with hormone receptor negative ( ie , triple negative ) primary tumors ( p , .001 ; fig 3c )  . 
of her2 - positive ctcs 6 - 10 11 - 50 > 50 predictors of discordance in her2 status between primary tumor and ctcs to evaluate which factors can independently predict discordance in her2 status between primary tumor and ctcs , we used a multivariable logistic regression model with discordance in her2 status ( yes v no ) as a binary response variable . 
patient and primary tumor characteristics included as independent factors were patient age in years , time since primary diagnosis in months , tumor stage ( pt ) , nodal stage ( pn ) , histologic grade , histologic type , and hormone receptor status . 
to account for the association between number of ctcs detected and presence of her2 - positive ctcs , we included number of ctcs ( one to four v > five ctcs ) as an additional explanatory variable . 
please note that the or for age listed in table 3 ( ie , 0.977 ) corresponded to the change of the odds of showing discordance in her2 phenotype associated with a 1 - year increase in age . discussion to our knowledge , the combined ctc screening of the detect study program provides the largest worldwide cohort of patients with mbc tested with regard to both rate of discordance in her2 phenotype between primary tumor and ctcs and possible predictors of her2 discordance . 
our analyses revealed an overall ctc prevalence of 63.3% in 1 , 123 patients with her2 - negative mbc , which is within the range reported in other studies on mbc.2 , 3 , 12 discordance in her2 phenotype between primary tumor and ctcs was observed in 18.8% of 711 ctc - positive patients and was independently predicted by histologic type and hormone receptor status of the primary tumor . 
of ctcs 11 - 50 > 50 6 - 10 11 - 25 > 25 her2 - positive ctcs ( % ) her2 status was more frequent in patients with five or more ctcs compared with patients with fewer than five ctcs . some previous studies have reported even higher discordance rates , although with considerably smaller sample sizes . 
lobular carcinomas are less cohesive tumors that are characterized by impaired cell - cell adhesion with reduced expression of the adhesion molecule e - cadherin.19 , 20 reduced cell and tissue adhesion may lead to an easier spread of tumor cells and could be one explanation for the association of presence of ctcs with lobular carcinomas . 
in general , her2 is rarely amplified or overexpressed in lobular carcinomas21 ; thus , the fact that we observed an association between presence of her2 - positive ctcs and lobular carcinomas is surprising and not easily explained . there is some evidence that lobular breast cancer shows a higher frequency of her2 mutations compared with ductal breast cancer.22 - 24 therefore , it could be speculated that the increased rate of her2 discordance observed in lobular carcinomas might be related to her2 mutations that affect her2 expression and membrane staining . the fact that hormone receptorpositive primary tumors exhibit higher rates of her2 discordance than triple - negative tumors is also a new finding that must be explored in more detail . clearly , additional investigations of tumor biology and pathogenesis of ctcs are necessary to help us understand these results . regardless of the underlying mechanisms , our findings may have implications for clinical practice . 
data on changes in her2 status during tumor progression represent crucial information for adequate patient therapy , because they may lead to modification of systemic and / or addition of targeted treatments . 
on the basis of our results , we suggest physicians consider attempting to obtain additional biopsies of metastatic lesions for detection of potential changes in her2 phenotype , especially in patients with lobular carcinomas or hormone receptorpositive primary tumors , because these are risk factors for her2 discordance identified in our study . 
prevalence of at least one human epidermal growth factor receptor 2 ( her2 ) positive circulating tumor cell ( ctc ; ie , discordance rate of her2 status [ % ] ) according to tumor characteristics of the primary tumor . 
 ( a ) prevalence of at least one her2 - positive ctc according to histologic grade of the primary tumor in 654 ctc - positive patients with her2 - negative metastatic breast cancer ( mbc ) screened for the detect study program ( for 57 patients , histologic grade of the primary tumor was unknown ; table 2 )  . 
 ( b ) prevalence of at least one her2 - positive ctc according to histologic type of the primary tumor in 711 ctc - positive patients with her2 - negative mbc screened for the detect study progra ( c ) prevalence of at least one her2positive ctc according to hormone receptor status of the primary tumor in 670 ctc - positive patients with her2 - negative mbc screened for the detect study program ( for 41 patients , hormone receptor status of the primary tumor was unknown ; table 2 )  . therapy in patients with histologically her2positive mbc revealed discordance of her2 status between tissue and ctcs in 62% of patients , and negative her2 status of ctcs was significantly associated with shorter progressionfree survival after the new line of anti - her2 therapy.25 another recent study indicated that her2 - targeted therapy with lapatinib was effective in decreasing the number of her2positive ctcs in patients with mbc.26 if additional research confirms that ctcs can be used as an easily accessible liquid biopsy to assess changes in tumor biology and her2 status of metastases , detection of her2 - positive ctcs in patients with mbc with her2negative primary tumors might even trigger the addition of her2 - targeted therapies without the need for a confirmatory biopsy of metastatic lesions . 
although primary tumors were considered her2 positive if more than 10% of tumor cells showed protein overexpression , her2 - positive ctc status was defined as presence of at least one ctc with an her2 3 + ihc score in the blood . 
furthermore , because this study was based on the initial screening results of the detect study program , and only a subsample of screened patients was recruited in one of the detect clinical trials , associations between ctc prevalence or presence of her2 - positive ctcs with metastatic disease patterns and patient outcomes could not be analyzed at this stage . 
ctc detection was based on an epithelial cell adhesion molecule selection process ; therefore , ctcs undergoing epithelial - tomesenchymal transition with phenotypic changes in terms of lacking epithelial cell adhesion molecule expression and gaining mesenchymal and / or stem - cell marker characteristics might have been missed , which could have led to falsely low rates of ctc positivity . 
furthermore , her2 status of ctcs was assessed by ihc only and was not confirmed using fish . in conclusion , discordance in her2 status between primary tumor and ctcs was observed in 18.8% of patients with her2 - negative mbc and was associated with lobular carcinomas , hormone receptorpositive primary tumors , and high ctc counts . 
moreover , the concept of liquid biopsy using ctcs as a real - time noninvasive monitoring tool to evaluate tumor biology , progression , and heterogeneity as a basis for more personalized treatment decisions should be tested in prospective randomized clinical trials . 
fasching provision of study material or patients : amelie de gregorio , jens huober , nikolaus de gregorio , brigitte rack , elisabeth trapp , andreas schneeweiss , klaus pantel , andreas hartkopf , peter a . 
fasching , tanja fehm collection and assembly of data : amelie de gregorio , christoph scholz , nikolaus de gregorio , brigitte rack , elisabeth trapp , sabine riethdorf , volkmar mueller , andreas schneeweiss , klaus pantel , franziska meier - stiegen , bernadette jaeger , andreas hartkopf , florin - andrei taran , peter a . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . amelie de gregorio consulting or advisory role : roche pharma ag thomas w.p. 
 jens huober honoraria : novartis , roche consulting or advisory role : novartis , roche travel , accommodations , expenses : novartis , roche christoph scholz consulting or advisory role : roche pharma ag research funding : novartis ( inst ) , roche pharma ag ( inst ) , janssen oncology ( inst ) nikolaus de gregorio consulting or advisory role : roche travel , accommodations , expenses : astrazeneca , tesaro brigitte rack consulting or advisory role : novartis speakers bureau : roche , pfizer research funding : sanofi ( inst ) , novartis ( inst ) , eli lilly ( inst ) , astrazeneca ( inst ) , chugai pharma ( inst ) , janssen diagnostics ( inst ) travel , accommodations , expenses : pfizer elisabeth trapp no relationship to disclose marianna alunni - fabbroni no relationship to disclose volkmar mueller consulting or advisory role : astrazeneca , celgene , daiichi sankyo , eisai , nektar , genentech , novartis travel , accommodations , expenses : pfizer , roche pharma ag andreas schneeweiss honoraria : roche pharma ag , celgene , astrazeneca , pfizer , novartis , amgen , roche pharma ag ( inst ) , pfizer ( inst ) research funding : roche pharma ag ( inst ) , celgene ( inst ) travel , accommodations , expenses : roche , celgene , amgen klaus pantel honoraria : agena bioscience consulting or advisory role : wntresearch , roche , novartis , sanofi research funding : janssen diagnostics franziska meier - stiegen consulting or advisory role : amgen bernadette jaeger no relationship to disclose andreas hartkopf no relationship to disclose florin - andrei taran no relationship to disclose peter a . 
fasching honoraria : roche , amgen , novartis , pfizer , celgene research funding : novartis ( inst ) wolfgang janni honoraria : janssen diagnostics research funding : janssen diagnostics tanja fehm consulting or advisory role : roche , novartis , amgen research funding : novartis acknowledgment we thank all the patients for participating in this study and donating their blood samples for research purposes . 
friedl , jens huober , christoph scholz , nikolaus de gregorio , and wolfgang janni , university hospital ulm , ulm ; brigitte rack , elisabeth trapp , and marianna alunni - fabbroni , hospital of ludwig - maximilians - university , munich ; sabine riethdorf , volkmar mueller , and klaus pantel , university hospital hamburg - eppendorf , hamburg ; andreas schneeweiss , university hospital heidelberg , heidelberg ; franziska meier - stiegen , bernadette jaeger , and tanja fehm , heinrichheine - university duesseldorf , duesseldorf ; andreas hartkopf and florin - andrei taran , university hospital tuebingen , tuebingen ; and peter a . 
fasching , university hospital erlangen , erlangen , germany . affiliations support the detect study program is supported by the investigator - initiated study program of janssen diagnostics , with clinical trials also supported by pierre fabre pharma , teva pharmaceuticals industries , amgen , novartis pharma , and eisai ; study medications vinorelbine , nonpegylated liposomal doxorubicin , lapatinib and everolimus , eribulin , and pertuzumab were provided free of charge by pierre fabre pharma , teva pharmaceuticals industries , novartis pharma , eisai , and roche , respectively . the funding sources had no role in study design ; data collection , analysis , or interpretation ; or writing of the report . 
bidard fc , peeters dj , fehm t , et al : clinical validity of circulating tumour cells in patients with metastatic breast cancer : a pooled analysis of individual patient data . 
fehm t , m uller v , aktas b , et al : her2 status of circulating tumor cells in patients with metastatic breast cancer : a prospective , multicenter trial . 
hayes df , cristofanilli m , budd gt , et al : circulating tumor cells at each follow - up time point during therapy of metastatic breast cancer patients predict progression - free and overall survival . 
pierga jy , hajage d , bachelot t , et al : high independent prognostic and predictive value of circulating tumor cells compared with serum tumor markers in a large prospective trial in first - line chemotherapy for metastatic breast cancer patients . 
simmons c , miller n , geddie w , et al : does confirmatory tumor biopsy alter the management of breast cancer patients with distant metastases ? ann oncol 20 : 1499 - 1504 , 2009 10 . 
ligthart st , bidard fc , decraene c , et al : unbiased quantitative assessment of her - 2 expression of circulating tumor cells in patients with metastatic and non - metastatic breast cancer . 
schramm a , friedl tw , schochter f , et al : therapeutic intervention based on circulating tumor cell phenotype in metastatic breast cancer : concept of the detect study prograarch gynecol obstet 293 : 271 - 281 , 2016 12 . 
tewes m , aktas b , welt a , et al : molecular profiling and predictive value of circulating tumor cells in patients with metastatic breast cancer : an option for monitoring response to breast cancer related therapies . 
wallwiener m , hartkopf ad , riethdorf s , et al : the impact of her2 phenotype of circulating tumor cells in metastatic breast cancer : a retrospective study in 107 patients . 
houssami n , macaskill p , balleine rl , et al : her2 discordance between primary breast cancer and its paired metastasis : tumor biology or test artefact ? insights through meta - analysis . 
aurilio g , disalvatore d , pruneri g , et al : a meta - analysis of oestrogen receptor , progesterone receptor and human epidermal growth factor receptor 2 discordance between primary breast cancer and metastases . 
sinn hp , helmchen b , heil j , et al : lobular neoplasms and invasive lobular breast cancer [ in german ] pathologe 35 : 45 - 53 , 2014 20 . 
gomes ds , porto ss , rocha rm , et al : usefulness and limitations of e - cadherin and b - catenin in the classification of breast carcinomas in situ with mixed pattern . 
ross js , wang k , sheehan ce , et al : relapsed classic e - cadherin ( cdh1 ) - mutated invasive lobular breast cancer shows a high frequency of her2 ( erbb2 ) gene mutations . 
zhang s , li l , wang t , et al : real - time her2 status detected on circulating tumor cells predicts different outcomes of anti - her2 therapy in histologically her2 - positive metastatic breast cancer patients . 
 appendix results additional data regarding both the association between hormone receptor status and histologic type and rates of human epidermal growth factor receptor 2 ( her2 ) discordance in relation to the combined hormone receptor and tumor type status are as follows : hormone receptor status and histologic type of primary tumors were significantly associated with each other ( p , .001 ; n = 670 ; 41 patient cases with missing values for hormone receptor status )  . 
frequency distribution of the number of circulating tumor cells ( ctcs ) detected in 7.5 - ml peripheral blood samples from 1 , 123 patients with human epidermal growth factor receptor 2negative metastatic breast cancer screened for the detect study program ( cutoff for ctc positivity , > one ctc )  . 6 - 10 11 - 50 > 50 no . 
 olaparib monotherapy for brip1 - mutated high - grade serous endometrial cancer kohei nakamura , md , phd1 , 2 ; eriko aimono , md1 ; shigeki tanishima , md , phd3 ; mitsuho imai , md , phd1 ; akiko kawano nagatsuma , md , phd1 ; hideyuki hayashi , md , phd1 ; yuki yoshimura , md4 ; kentaro nakayama , md , phd4 ; satoru kyo , md , phd4 ; and hiroshi nishihara , md , phd1 introduction treatment the prognosis for women with high - grade endometrial cancers is poor , with little improvement in the last two decades.1 the mainstay of is surgery lymphadenectomy . ( hysterectomy ) with or without although adjuvant radiotherapy is considered standard for high - risk endometrial cancers , the added value of chemotherapy has been the subject of recent trials . 
recently , other mutations were reported in ovarian cancers , such as those in fanconi anemia genes ( eg , palb2 [ fancn ] , brip1 [ fancj ] , and rad51c ) and other genes involved in hrr ( eg , atm , bard1 , nbn , cdk12 , tp53 , and chek2 ) .2 , 3 poly ( adp - ribose ) polymerase ( parp1 ) is a dna repair enzyme involved in base excision and single - stranded break repair pathways.4 parp1 inhibition in hrrdecient cells blocks single - stranded dna break repair pathways , leaving only double - stranded dna break repair pathways functional . 
this results in synthetic lethality from the loss of homologous recombination and base excision repair , thus activating highly error - prone dna repair pathways , eventually causing cell death.5 , 6 parp inhibitors also trap parp - dna complexes at the replication fork , increase toxic nonhomologous end joining in parp1 - decient cells , and block parp1 / pol - mediated alternative end joining.7 the us food and drug administration ( fda ) has approved three parp inhibitors ( olaparib , rucaparib , and niraparib ) as monotherapies for breast and ovarian cancers . 
after surgery , the patient received six cycles of carboplatin and paclitaxel . there was also evidence of after rst - line chemotherapy , ct indicated stable disease based on recist 1.0 criteria , with only improvements in the cardiophrenic swollen lymph node ( fig 1 )  . 
after six cycles , ct revealed essentially stable disease without iliac in the para - aortic or left improvement swollen lymph nodes ( fig 1 )  . lateral targeted next - generation sequencing of the patients blood and resected specimen was performed using an in - house assay during treatment . 
a tp53 somatic point mutation ( p.r175h ) and somatic frameshift brip1 ( p.q554hfs * 35 ) alterations were detected as pathogenic variants in the tumor ; detailed information is provided in appendix figures a1 and a2 . 
secondary germ line examination found no american college of medical genetics and genomics recommended genes for testing . given her somatic brip1 mutation and ndings indicating loh high status , the potential efcacy of the parp inhibitor olaparib was discussed with the patient . 
9 months of olaparib and showed complete response on her most recent ct . discussion endometrial cancers are categorized into two main histologic types.8 type i endometrial tumors show endometrioid histology and typically express estrogen ( er ) and progesterone ( pr ) receptors . 
in contrast , type ii endometrial tumors do not exhibit endometrioid histology ( predominantly serous histology ) and are associated with poorer prognoses , with a 5 - year overall survival rate of 55%.1 type ii tumors neither express er / pr nor respond to endocrine therapy . 
meanwhile , type i tumors exhibit signicantly more pi3k pathway alterations ( primarily pten and pik3ca mutations ) .9 , 10 in our case , next - generation target panel sequencing results reected the molecular events observed in serous endometrial cancers , such as tp53 mutations . whereas brip1 is implicated in double - stranded dna break repair via hrr pathways , the frequency of brip1 mutations in type ii endometrial tumors remains unclear . in a previous study by heeke et al , 11 the prevalence of recombinationrelated gene mutations homologous across multiple cancer types was investigated in 52 , 426 malignant tumors . 
this has promoted clinical studies of parp inhibitors in contexts other than ovarian cancer . moreover , their potential therapeutic applications might be extended from germ line brca mutations to target a more diverse group of sporadic tumors , such as those with epigenetic disruption of brca1 / 2 function or genetically or epigenetically acquired aberrations in other important hrr pathway constituents.12 there is clinical evidence to support this theory , with olaparib approved by the fda as an alternative for patients with germ line or somatic brca1 / 2 mutations and as maintenance therapy after platinumbased chemotherapy in platinum - sensitive recurrent epithelial ovarian carcinoma , regardless of brca mutation status.13 hrr alterations are associated with brca1 / 2 mutations in high - grade serous endometrial cancers ; however , parp inhibitors await fda approval for this indication , and there are currently no trials of parp inhibitors in patients with endometrial cancers with brca or other hrr - associated genealterations . accumulating evidence indicates that patients with brip1 mutations have hrr deciency and are consequently hypersensitive to parp inhibition.14 brip1 is a brca1interacting protein ( the brip1 - brca1 interaction is important for hrr ) and associates with brca1 as cells progress through the s phase of the cell cycle.15 , 16 brip1 is a dna helicase that interacts with the cooh - terminal brct repeat of brca1 . 
brip1 is associated with the gm1 / 2 checkpoint , as well as the activation of chk1 , regulation of entry into the s phase , and maintenance of genomic stability.16 thus , if the complex involving brca1 and brip1 is involved in tumor suppression , mutations in the genes that encode these proteins should be associated with altered cancer risk . 
recently , three independent dnabased measures of genomic instability reecting underlying tumor homologous recombination dna repair deciency were developed based on loh , telomeric allelic imbalance , and large - scale state transitions.17 - 19 however , we could not determine the homologous recombination deciency score , because the relevant test is not covered by insurance in japan , and therefore , we could not prove this . 
however , we can hypothesize that the brip1 mutation results in hrr deciency and subsequently causes a high loh frequency and scattered allelic imbalance , potentially resulting in good response to parp inhibitors . in conclusion , we describe the case of a 70 - year - old woman exhibiting a durable clinical radiographic response to olaparib . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . support supported by the japan agency for medical research and development under grant no . 
lancet 387 : 1094 - 1108 , 2016 somyajit k , subramanya s , nagaraju g : rad51c : a novel cancer susceptibility gene is linked to fanconi anemia and breast cancer . 
carcinogenesis 31 : 2031 - 2038 , 2010 sigurdsson s , van komen s , bussen w , et al : mediator function of the human rad51b - rad51c complex in rad51 / rpa - catalyzed dna strand exchange . genes dev 15 : 3308 - 3318 , 2001 4 . 
morales j , li l , fattah fj , et al : review of poly ( adp - ribose ) polymerase ( parp ) mechanisms of action and rationale for targeting in cancer and other diseases . crit rev eukaryot gene expr 24 : 15 - 28 , 2014 farmer h , mccabe n , lord cj , et al : targeting the dna repair defect in brca mutant cells as a therapeutic strategy . 
nature 434 : 917 - 921 , 2005 ashworth a : a synthetic lethal therapeutic approach : poly ( adp ) ribose polymerase inhibitors for the treatment of cancers decient in dna double - strand break repair . 
j clin oncol 26 : 3785 - 3790 , 2008 konstantinopoulos pa , ceccaldi r , shapiro gi , et al : homologous recombination deciency : exploiting the fundamental vulnerability of ovarian cancer . 
gynecol oncol 15 : 10 - 17 , 1983 kandoth c , schultz n , cherniack ad , et al : cancer genome atlas research network : integrated genomic characterization of endometrial carcinoma . 
sato k , koyasu m , nomura s , et al : mutation status of rad51c , palb2 and brip1 in 100 japanese familial breast cancer cases without brca1 and brca2 oncogene 26 : 2157 - 2165 , 2007 mutations . 
dong y , hakimi ma , chen x , et al : regulation of brcc , a holoenzyme complex containing brca1 and brca2 , by a signalosome - like subunit and its role in 16 . 
genomic testing was performed on a plessision internal clinical sequencing apparatus ( keio university , tokyo , japan ) , which is used for all genome sequencingrelated analyses in our hospital ( keio university hospital )  . 
this apparatus was used to extract genomic dna from tumor samples and peripheral blood mononuclear cells extracted from patients with cancer , after the provision of consent to undergo comprehensive genomic testing . 
this study was conducted in accordance with the declaration of helsinki and title 45 , us code of federal regulations , part 46 , protection of human subjects , effective december 13 , 2001 . dna quality was checked by calculating the dna integrity number ( din ) using an agilent 2000 tapestation ( agilent technologies , waldbronn , germany ) before conducting targeted amplicon exome sequencing of the 160 genes implicated in cancer using the illumina miseq sequencing platform ( illumina , san diego , ca )  . 
cancer - specic changes in somatic genes , including single - nucleotide variants , insertions / deletions , and copynumber variations were detected and used to determine the tumor mutation burden . 
these preclinical observations suggest a role for the targeted inhibitors of the bcr pathway in the treatment of dlbcl.1 dlbcl is most commonly present as malignant inltration of lymph nodes . 
the use of btk inhibitors is now incorporated into standard therapy for these conditions , and the genetic basis of acquired resistance in cll , dominated by acquired mutation of btk or plcg2 , has been well - studied.6 , 7 by contrast , the role of bcr inhibition in dlbcl remains less clear and little is known about the genetics of acquired resistance . a 75 - year - old male presented with rapidly enlarging cutaneous nodules . 
clinical examination revealed cutaneous nodules up to 25 mm in diameter affecting the feet , legs , arms , and abdomen . a repeat biopsy showed features identical to his original diagnostic biopsy ( fig 1a ) , and computed tomography scan conrmed exclusively cutaneous disease . 
the patient was managed with palliative radiotherapy . the rapid clinical response and prolonged remission , followed by later re - emergence of tumor , suggested the acquisition of new genetic alterations driving resistance to bcr inhibition . 
this study was approved by the east of england cambridge south research ethics committee ( approval reference number 07 / mre05 / 44 )  . full variant and copy number data are presented in the data supplement . 
 ( a ) histology and immunohistochemistry from tumor biopsy showing a diffuse inltration by large atypical cells with predominantly centroblast - like morphology expressing cd20 , mum1 , bcl2 , weak bcl6 , no cd10 , and mib1 proliferation fraction 90% . 
 ( b ) images of selected lesions on the forearm , hand , popliteal fossa , and abdomen taken prior to therapy ( top row ) , at 28 days ( middle row ) , and at 6 months ( bottom row ) of b cell receptortargeted therapy . 
 ( a ) summary of whole - exome sequencing of samples taken from three different timepoints ; diagnosis , prior to bcr - targeted therapy , and at the time of relapse . 
gray indicates no mutation or copy number change identied . ( b ) a simplied schematic showing the critical signaling components of the bcr pathway that converge onto activation of canonical nf - b . components targeted pharmacologically in this patient are indicated . 
we manually examined the loci of plcg2 and btk , mutations that are commonly acquired in btki - resistant cll , and conrmed both genes to be wild type at all timepoints . 
 case report in the bcr pathway to activate canonical nf - b signaling.1 activating mutation in the coiled - coil domain of card11 was previously proposed as a mechanism of resistance to bcr inhibition in mantle cell lymphoma8 and primary resistance in dlbcl.9 the acquired k215t mutation in our patient is located in the coiled - coil domain and has been previously shown to activate nf - b.10 we conrmed the near - clonal presence of the card11 k215t mutation at relapse ( variable allele frequency 40% ) but zero mutant reads at this position in either of the two pretreatment biopsies ( read depth , 180 and 210 , appendix fig a3 )  . 
taken together , these data strongly suggest that card11 mutation was the genetic driver of the acquired resistance in this case . the limited information about acquired resistance to bcr inhibition in dlbcl suggests potential differences compared with that of cll . 
the latter is predominantly associated with mutation of btk and plcg2.6 , 7 card11 identied in 10% - 15% of dlbcl at mutation is presentation11 but is rarely identied ( , 1% ) in cll.12 this suggests that the bcr signal in cll and dlbcl may be qualitatively different and therefore that genetic mechanisms of resistance to bcr inhibition may also differ . however , establishing the genetic basis of resistance to bcr inhibition in dlbcl presents specic challenges that contrast with the situation in cll . 
first , patients with dlbcl receiving bcr inhibitors are typically treated simultaneously with multiagent immunochemotherapy regimens , making it hard to establish which mutations provide resistance to which agent , or indeed if sensitivity to the bcr inhibitor ever existed in the rst place . 
combined with the biopsy - accessible cutaneous location of disease , this provided a rare opportunity to study genetic mechanisms of resistance to bcr inhibition in abc dlbcl . indeed , we have found only one other case describing the genetic basis of acquired resistance to bcr inhibition in dlbcl . 
this also involved a case of pcdlbcl - lt and also reported acquisition of card11 mutation ( interesting also k215 mutant ) in a patient who relapsed following an initial response to a btk inhibitor.13 however , the concurrent nding of nfkbie mutation and igh - irf8 translocation reported in that study might also have contributed to resistance , leaving the role of the card11 mutation uncertain . our ndings of acquired activating card11 mutation , the absence of any likely alternative genetic explanation , and the demonstrated ability of the k215t mutation to affect btki resistance in vitro strongly suggest that card11 mutation is the dominant driver of bcr independence in our case . as we move toward the introduction of precision medicine in dlbcl and the real - time monitoring of clonal evolution , it will become increasingly important to understand genetic mechanisms of drug resistance . 
our study uses the unique features of this case of cutaneous dlbcl to highlight the importance of card11 mutation as a driver of acquired resistance to bcr inhibition in dlbcl . 
hodson provision of study materials or patients : nimish shah collection and assembly of data : rebecca caeser , ieuan walker , jie gao , nimish shah , livia rasso - barnett , jose - ezequiel martin , daniel j . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . rebecca caeser consulting or advisory role : karus therapeutics nimish shah consulting or advisory role : abbvie speakers bureau : roche , janssen travel , accommodations , expenses : abbvie livia rasso - barnett leadership : cambridge pathology stock and other ownership interests : cambridge pathology honoraria : cambridge pathology consulting or advisory role : cambridge pathology daniel j . 
semin hematol 52 : 77 - 85 , 2015 swerdlow sh , campo e , pileri sa , et al : the 2016 revision of the world health organization classication of lymphoid neoplasms . 
blood 127 : 2375 - 2390 , 2016 grange f , beylot - barry m , courville p , et al : primary cutaneous diffuse large b - cell lymphoma , leg type : clinicopathologic features and prognostic analysis in 60 cases . 
mareschal s , pham - ledard a , viailly pj , et al : identication of somatic mutations in primary cutaneous diffuse large b - cell lymphoma , leg type by massive parallel sequencing . 
j invest dermatol 137 : 1984 - 1994 , 2017 pham - ledard a , prochazkova - carlotti m , andrique l , et al : multiple genetic alterations in primary cutaneous large b - cell lymphoma , leg type support a common lymphomagenesis with activated b - cell - like diffuse large b - cell lymphoma . 
j clin oncol 35 : 1437 - 1443 , 2017 ahn ie , underbayev c , albitar a , et al : clonal evolution leading to ibrutinib resistance in chronic lymphocytic leukemia . 
fox lc , yannakou ck , ryland g , et al : molecular mechanisms of disease progression in primary cutaneous diffuse large b - cell lymphoma , leg type during ibrutinib therapy . 
nagel d , spranger s , vincendeau m , et al : pharmacologic inhibition of malt1 protease by phenothiazines as a therapeutic approach for the treatment of aggressive abc - dlbcl . 
 case report chr1 chr3 chr5 chr11 chr13 chr15 chr17 chr19 chr21 chrx prdm1 tnfaip3 chr7 cdkn2a chr9 rb1 gna13 chr2 chr4 chr6 chr8 chr10 chr12 chr14 chr16 chr18 chr20 chr22 chry mir17 - 92 bcl2 malt1 tcf4 cd79a spib mir17 - 92 bcl2 malt1 tcf4 cd79a spib chr1 chr3 chr5 chr7 chr9 chr11 chr15 chr17 chr19 chr21 chrx chr2 chr4 chr6 chr8 chr10 chr12 chr14 chr16 chr18 chr20 chr22 chry prdm1 tnfaip3 rb1 chr13 gna13 appendix relapse pre - treatment diagnosis chr1 chr3 chr5 chr7 chr9 chr11 chr13 chr15 chr17 chr19 chr21 chrx chr2 chr4 chr6 chr8 chr10 chr12 chr14 chr16 chr18 chr20 chr22 chry fig a1 . 
 o genetic alterations detected in cell - free dna are associated with enzalutamide and abiraterone resistance in castration - resistant prostate cancer samantha torquato , phd1 ; aparna pallavajjala , ms1 ; alexa goldstein , ms1 ; patricia valda toro , ms1 ; john l . 
hurley , phd1 purpose androgen receptor ( ar ) gene alterations , including ligand - binding domain mutations and copy number ( cn ) gain , have yet to be fully established as predictive markers of resistance to enzalutamide and abiraterone in men with metastatic castration - resistant prostate cancer ( mcrpc )  . 
the goal of this study was to validate ar gene alterations detected in cell - free dna ( cfdna ) as markers of enzalutamide and abiraterone resistance in patients with mcrpc . methods patients with mcrpc ( n = 62 ) were prospectively enrolled between 2014 and 2018 . 
blood was collected before therapiesenzalutamide ( n = 25 ) , abiraterone ( n = 35 ) , or enzalutamide and abiraterone ( n = 2 ) and at disease progression . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction next - generation therapies that target the androgen androgen receptor ( ar ) axis , such as abiraterone and enzalutamide , have improved survival outcomes for men with metastatic castration - resistant prostate cancer ( mcrpc ) , 1 - 4 but both primary and acquired resistance to these drugs continue to be a substantial clinical challenge . 
resistance mechanisms are not fully understood ; however , some forms of resistance likely involve alterations to ar , including amplication and ligand - binding domain ( lbd ) missense mutations . 
although rare in primary prostate cancers , 5 - 7 ar gene alterations are highly prevalent in mcrpc.8 - 13 metastatic tissue biopsies as a sole means to detect and observe changes in ar status is impractical , and thus cell - free dna ( cfdna ) is gaining traction as a minimally invasive and easily obtainable tumor biopsy surrogate . 
previous studies using cfdna from the blood to evaluate the association of ar gene aberrations with resistance to abiraterone and enzalutamide are inclusive.14 - 17 ar copy number ( cn ) gain18 , 19 and / or amplication20 or detection of two or more ar mutations20 have been associated with worse outcomes to such therapies as abiraterone and enzalutamide . 
the ar splice variant ar - v7 is associated with resistance to enzalutamide and abiraterone21 - 23 and is also associated with increased ar cn.24 in addition to ar , alterations in other genes , including tumor protein p53 ( tp53 ) , phosphatase and tensin homolog ( pten ) , and breast cancer gene 2 ( brca2 ) , are enriched in lethal prostate cancer.8 - 11 studies support the idea that lineage plasticity from an ardependent to an ar - independent state through loss of tp53 and retinoblastoma - associated protein 1 ( rb1 ) mediates resistance to ar - targeted therapies.25 - 28 consistent with this , tp53 defects have been shown to be associated with worse outcomes with abiraterone and enzalutamide therapies.17 the role of brca2 and other homology - directed repair ( hdr ) genes in mediating resistance to enzalutamide and abiraterone has not been denitively determined . 
the secondary goal was to determine if alterations in other genes that are enriched in lethal prostate cancer , including tp53 , pten , and brca2 , were associated with response to enzalutamide and abiraterone . in this study , high circulating tumor dna ( ctdna ) burden was signicantly associated with prostate - specic antigen ( psa ) ( pfs ) , and overall survival ( os )  . 
study limitations , including sample size and patient heterogeneity , necessitate larger and prospective validation of the association of plasma ar status with outcomes . response , progression - free survival methods patient information , study end points , sample collection , deep next - generation sequencing ( ngs ) , sequence alignment and analysis of variants , cn variation , estimation of ctdna fraction , and statistical analyses are found in the data supplement . results patient cohort patient characteristics are listed in table 1 . 
clinvarannotated pathogenic or likely pathogenic missense mutations , truncating mutations , and / or cn alterations were detected in cfdna from 89% of patients before therapy initiation and in 92% of patients at disease progression ( figs 1a - 1d and data supplement )  . ctdna total cfdna concentration before therapy was associated with psa ( p = .002 ; data supplement )  . 
nearly all patients ( 61 of 62 ) had detectable cn variation ( s ) and / or mutation ( s ) with an allelic frequency above the 1% cutoff before therapy ( figs 1b and 1c )  . 
multivariable analyses controlled for ctdna high . abbreviations : ar , androgen receptor ; atm , ataxia - telangiectasia mutated gene ; brca1 / 2 , breast cancer gene 1 / 2 ; cn , copy number ; ctdna , circulating tumor dna ; lbd , ligand - binding domain ; or , odds ratio ; pi3k , phosphoinositide 3 - kinase ; psa , prostate - specic antigen ; rb1 , retinoblastoma - associated protein 1 ; tp53 , tumor protein 53 ; wnt , wingless - type mmtv integration site . h875y mutation had psa responses on abiraterone ( fig 2c )  . 
 ( b ) total number of protein - altering genetic changes in 46 genes detected by next - generation sequencing ( ngs ) of cfdna from 62 patients before abiraterone ( abi ) and enzalutamide ( enza ) therapy . 
 ( c ) genetic alterationscopy number ( cn ) status , clinvar pathogenic / likely pathogenic missense and germline mutations , and truncating mutationsin 46 genes detected by ngs of cfdna from 62 patients before abiraterone and enzalutamide therapy in order of best psa response . 
 ( d ) total number of genetic alterationscn , clinvar pathogenic / likely pathogenic missense and germline mutations , and truncating mutationsin 46 genes detected by ngs of cfdna from 62 patients before abiraterone and enzalutamide therapy . 
ar , androgen receptor ; ctdna , circulating tumor dna . defectspathogenic mutations and / or cn losswere not associated with psa response ( p = .602 ) or pfs ( p = .314 ; tables 2 and 3 )  . 
progression - free survival ( pfs ) : pathogenic androgen receptor ( ar ) ligand - binding domain ( lbd ) mutations are associated with a shorter time to progression . 
 ( a ) kaplan - meier method and log - rank test were used to determine median time to progression for patients who had high versus low circulating tumor dna ( ctdna ) before therapy . 
 ( b ) waterfall plot of best prostate - specic antigen ( psa ) response for all patients ( n = 62 ) after therapy as determined by best percentage fold change in psa . 
wingless - type mmtv integration site pathway defects involving genetic alterations in adenomatous polyposis colicn loss and / or truncating mutationsand - catenincn gain and pathogenic missense mutationswere detected in nearly 15% of patients before to therapy ( figs 1c and 1d )  . 
analysis of brca2 , and atm did not increase prognostic signicance . discussion liquid biopsies using cfdna as a tumor analyte are rapidly being developed for cancer diagnostics of solid tumors.35 - 37 when obtained concurrently , plasma - derived cfdna is highly concordant with tissue biopsies for tumor - specic genetic alterations.38 , 39 as a result of their advantages over traditional tissue biopsies , including the ease of accessibility for sequential monitoring of cancer dynamics and recapitulation of tumor heterogeneity , clinical development of cfdna has the potential to advance prostate cancer precision medicine.40 mechanisms of resistance to abiraterone and enzalutamide likely involve alterations to androgenar axis signaling . 
deregulation of these pathways likely mediates resistance to androgenar axis therapies . concurrent tp53 and rb1 defects are highly enriched in ar - independent neuroendocrine mcrpc compared with adenocarcinoma mcrpc.42 combined tp53 and rb1 loss has been shown to promote lineage switching from an ardependent to an ar - independent state41 , 43 , 44 and consequent resistance to ar - targeted therapies . 
similar to tp53 , genetic alterations in pten are enriched in mcrpc compared with metastatic castration - sensitive prostate cancer and localized prostate cancer.11 studies suggest that pten loss may mediate castration resistance by downregulating ar , 25 - 28 thereby supporting a rationale for combined inhibition of pi3k and arin pten - decient mcrpcs.45 , 46 association of pathogenic mutations in hdr genes with response to abiraterone and enzalutamide therapy is conicting . 
a clinical trial in patients with mcrpc suggested that genetic alterations in hdr genes that were detected in metastatic biopsy tissue may be associated with longer pfs when on abiraterone therapy.29 concordant ndings were observed in a second study that supported the idea that patients with mcrpc harboring a germline brca1 / 2 or atm mutation may also have improved outcomes to abiraterone and enzalutamide.30 in contrast , another study showed that truncating mutations in brca2 and atm detected in cfdna were associated with a shorter time to progression on abiraterone and enzalutamide therapies in treatment - nave patients with mcrpc.17 in our study , collective somatic and germline genetic alterations were also not associated with worse outcomes to enzalutamide and abiraterone . 
association differences may reect variables , such as sample size , prior treatment status , disease burden , disease heterogeneity , somatic versus germline , and single versus dual loss . 
certainly , additional prospective investigation is needed to determine the clinical signicance of hdr mutations as predictive markers to abiraterone and enzalutamide therapies . in the current study , many patients had detectable alterations that could serve as potential therapeutic targets . previous studies have shown that patients with mcrpc with either germline or somatic mutations in hdr genes achieved signicant responses to olaparib47 and to abiraterone plus veliparib.29 more than one quarter of patients in our study had a deleterious germline or somatic brca1 , brca2 , or atm mutation detected before therapy or at disease progression , which suggests that these patients may benet from therapies that target poly ( adp - ribose ) polymerase or platinum - based chemotherapy.29 , 47 , 48 in addition , immunotherapy trials have been largely unsuccessful in men with mcrpc49 ; however , rare responders have been reported.50 a seminal clinical trial demonstrated that microsatellite instable cancers caused by mismatch repair ( mmr ) gene deciency were sensitive to programmed death - 1 blockade , perhaps because of the formation of neoantigens resulting from increased mutational burden.51 inactivation of mmr genes and elevated mutational burden have been detected in some men with aggressive prostate cancers.33 , 52 , 53 one patient in our study had a detectable noncanonical mmr gene mutation in his cfdna and a correspondingly high fig 3 . 
 ( a ) kaplan - meier method and log - rank test were used to determine median os for patients who had high versus low circulating tumor dna ( ctdna ) before therapy . 
 ( b ) kaplan - meier method and log - rank test were used to determine median os for patients who had androgen receptor ( ar ) copy number ( cn ) gain before therapy . 
 ( c ) gene schematic illustrating deleterious tp53 mutations detected by deep next - generation sequencing ( ngs ) of cellfree dna ( cfdna ) before abiraterone and enzalutamide therapies and at disease progression while on therapy . 
 ( d ) kaplan - meier method and log - rank test were used to determine median os for patients who had tp53 defectscn loss and or clinvar pathogenic / likely pathogenic mutationsbefore therapy . 
 ( e ) kaplan - meier method and log - rank test were used to determine median os for patients who had both tp53 and retinoblastomaassociated protein 1 ( rb1 ) defects compared with patients who had tp53 defects but were rb1 intactcn loss and or clinvar pathogenic / likely pathogenic mutationsbefore therapy . 
 ( f ) kaplan - meier method and log - rank test were used to determine median os for patients who had pi3k pathway defectscn loss and / or truncating mutations in phosphatase and tensin homolog and / or cn gain of pik3cabefore therapy . association of pi3k defects with os controlled for ctdna burden using multivariable proportional hazards regression modeling . 
 ( g ) kaplan - meier method and log - rank test were used to determine median os for patients who had wingless - type mmtv integration site ( wnt ) pathway defectscn loss and / or truncating mutations in adenomatous polyposis coli and / or cn gain and / or pathogenic missense mutations in - cateninbefore therapy . 
consistent with other reports , patients with prior exposure to abiraterone and enzalutamide experienced worse outcomes.54 - 59 statistical signicance was not reached , likely because of the small overall sample size and the few patients with prior therapy . 
ngs protocols were adjusted on the basis of total input , but for patients with low input the lack of genetic alteration detection was considered indeterminate as opposed to negative . 
in addition , mutations in such genes as including ar - v7 , because of tp53 and atm detected in cfdna at low allelic frequencies may be false positives as a result of clonal hematopoiesis.60 corresponding tissue was not available for all samples to conrm tp53 status , and future studies will examine both prostate tumor tissue and blood leukocytes for genetic alterations . 
a nal limitation was our inability to evaluate ar the resplice variants , quirement of circulating tumor cells or whole - blood rna . the presence of ar - v7 is certainly another established mechanism of primary and acquired resistance to nextgeneration hormonal therapies.21 - 23 future studies should aim to simultaneously analyze the full complement of ar aberrations , including gene mutations , amplications , genomic structural rearrangements , and mrna splice variants , from a single liquid biopsy . in summary , our ndings indicate ctdna burden was highly associated with worse outcomes to enzalutamide and abiraterone . 
eisenberger leadership : veru stock and other ownership interests : veru honoraria : sano , pzer consulting or advisory role : astellas pharma , ipsen , bayer , sano , pzer research funding : sano , tokai pharmaceuticals , genentech travel , accommodations , expenses : bayer , astellas pharma , sano , pzer , veru emmanuel s . 
antonarakis honoraria : sano , dendreon , medivation , janssen biotech , essa pharma , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , medivation , janssen biotech , essa pharma , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : coinventor of a biomarker technology licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation bruce j . 
park leadership : loxo pharmaceuticals stock and other ownership interests : loxo pharmaceuticals consulting or advisory role : horizon discovery , foundation medicine , loxo pharmaceuticals , casdin capital , h3 biomedicine , jackson laboratory for genomic medicine , eli lilly speakers ' bureau : astrazeneca research funding : foundation medicine , abbvie , pzer patents , royalties , other intellectual property : royalties paid through inventions at johns hopkins university by horizon discovery travel , accommodations , expenses : eli lilly , loxo pharmaceuticals paula j . 
hurley stock and other ownership interests : loxo pharmaceuticals ( i ) honoraria : foundation medicine ( i ) , roche ( i ) , h3 biomedicine ( i ) , casdin capital ( i ) , loxo pharmaceuticals ( i ) , eli lilly ( i ) consulting or advisory role : loxo pharmaceuticals ( i ) , foundation medicine ( i ) , roche ( i ) , h3 biomedicine ( i ) , casdin capital ( i ) , lilly ( i ) patents , royalties , other intellectual property : cell lines at horizon ( i ) no other potential conicts of interest were reported . acknowledgment we thank the patients who consented to participate in this study . 
n engl j med 364 : 1995 - 2005 , 2011 ryan cj , smith mr , de bono js , et al : abiraterone in metastatic prostate cancer without previous chemotherapy . 
n engl j med 368 : 138 - 148 , 2013 scher hi , fizazi k , saad f , et al : increased survival with enzalutamide in prostate cancer after chemotherapy . 
n engl j med 367 : 1187 - 1197 , 2012 beer tm , armstrong aj , rathkopf de , et al : enzalutamide in metastatic prostate cancer before chemotherapy . 
cancer cell 18 : 11 - 22 , 2010 grasso cs , wu ym , robinson dr , et al : the mutational landscape of lethal castration - resistant prostate cancer . 
nature 487 : 239 - 243 , 2012 kumar a , coleman i , morrissey c , et al : substantial interindividual and limited intraindividual genomic diversity among tumors from men with metastatic prostate cancer . 
abida w , armenia j , gopalan a , et al : prospective genomic proling of prostate cancer across disease states reveals germline and somatic alterations that may affect clinical decision making . 
azad aa , volik sv , wyatt aw , et al : androgen receptor gene aberrations in circulating cell - free dna : biomarkers of therapeutic resistance in castration - resistant prostate cancer . 
annala m , vandekerkhove g , khalaf d , et al : circulating tumor dna genomics correlate with resistance to abiraterone and enzalutamide in prostate cancer . cancer discov 8 : 444 - 457 , 2018 18 . 
salvi s , casadio v , conteduca v , et al : circulating cell - free ar and cyp17a1 copy number variations may associate with outcome of metastatic castrationresistant prostate cancer patients treated with abiraterone . 
conteduca v , wetterskog d , sharabiani mta , et al : androgen receptor gene status in plasma dna associates with worse outcome on enzalutamide or abiraterone for castration - resistant prostate cancer : a multi - institution correlative biomarker study . 
qu f , xie w , nakabayashi m , et al : association of ar - v7 and prostate - specic antigen rna levels in blood with efcacy of abiraterone acetate and enzalutamide treatment in men with prostate cancer . 
antonarakis es , lu c , luber b , et al : clinical signicance of androgen receptor splice variant - 7 mrna detection in circulating tumor cells of men with metastatic castration - resistant prostate cancer treated with rstand second - line abiraterone and enzalutamide . 
cancer res 67 : 6535 - 6538 , 2007 jiao j , wang s , qiao r , et al : murine cell lines derived from pten null prostate cancer show the critical role of pten in hormone refractory prostate cancer development . 
hussain m , daignault - newton s , twardowski pw , et al : targeting androgen receptor and dna repair in metastatic castration - resistant prostate cancer : results from nci 9012 . 
antonarakis es , changxue l , luber b , et al : germline dna - repair gene mutations and outcomes in men with metastatic castration - resistant prostate cancer receiving rst - line abiraterone and enzalutamide . 
salvi s , casadio v , conteduca v , et al : circulating ar copy number and outcome to enzalutamide in docetaxel - treated metastatic castration - resistant prostate cancer . 
lallous n , volik sv , awrey s , et al : functional analysis of androgen receptor mutations that confer anti - androgen resistance identied in circulating cell - free dna from prostate cancer patients . 
na r , zheng sl , han m , et al : germline mutations in atm and brca1 / 2 distinguish risk for lethal and indolent prostate cancer and are associated with early age at death . 
de bono js , de giorgi u . , massard c , et al : pten loss as a predictive biomarker for the akt inhibitor ipatasertib combined with abiraterone acetate in patients with metastatic castration - resistant prostate cancer ( mcrpc )  . 
brahmer jr , drake cg , wollner i , et al : phase i study of single - agent anti - programmed death - 1 ( mdx - 1106 ) in refractory solid tumors : safety , clinical activity , pharmacodynamics , and immunologic correlates . 
kwon ed , drake cg , scher hi , et al : ipilimumab versus placebo after radiotherapy in patients with metastatic castration - resistant prostate cancer that had progressed after docetaxel chemotherapy ( ca184 - 043 ) : a multicentre , randomised , double - blind , phase 3 trial . 
loriot y , bianchini d , ileana e , et al : antitumour activity of abiraterone acetate against metastatic castration - resistant prostate cancer progressing after docetaxel and enzalutamide ( mdv3100 )  . 
brasso k , thomsen fb , schrader aj , et al : enzalutamide antitumour activity against metastatic castration - resistant prostate cancer previously treated with docetaxel and abiraterone : a multicentre analysis . 
maughan bl , luber b , nadal r , et al : comparing sequencing of abiraterone and enzalutamide in men with metastatic castration - resistant prostate cancer : a retrospective study . 
emamekhoo h , barata pc , edwin nc , et al : evaluation of response to enzalutamide consecutively after abiraterone acetate / prednisone failure in patients with metastatic castration - resistant prostate cancer . 
craig lockhart , md17 ; cristiana sessa , md18 ; thomas zander , md19 ; matthew ng , md , phd20 ; giuseppe curigliano , md , phd21 , 22 ; jennifer bendiske , mba23 ; xueying chen , phd23 ; somesh choudhury , phd23 ; diana graus - porta , phd24 ; nancy lewis , md23 ; jose manuel perez garcia , md , phd25 ; and mara jos e de miguel - luken , md , phd26 purpose concurrent pik3ca mutations and broblast growth factor receptor ( fgfr ) alterations occur in multiple cancer types , including estrogen receptorpositive breast cancer , bladder cancer , and endometrial cancer . 
archival tumor samples were sequenced to explore genomic correlates of response . results in combination , both agents were escalated to full , single - agent recommended doses ( alpelisib , 300 mg per day continuously ; ingratinib , 125 mg per day 3 weeks on followed by 1 week off )  . 
the toxicity prole of the combination was consistent with the established safety prole of each agent , although 71% of all patients required at least one treatment interruption or dose reduction . 
molecularly selected dose expansions in breast cancer and other solid tumors harboring pik3ca mutations , alone or in combination with fgfr alterations , identied sporadic responses , predominately in tumor types and genotypes previously dened to have sensitivity to these agents . conclusion the combination of alpelisib and ingratinib can be administered at full single - agent doses , although the high rate of dose interruption or reduction suggests long - term tolerability may be challenging . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction genome - driven oncology has been focused primarily , to date , on the targeting of individual genomic alterations present in each tumor.1 although this approach has led to the development of many highly effective therapies , 2 - 6 we now understand that most oncogenes exist within a complex genomic landscape characterized by additional alterations that may , themselves , be targetable or modify sensitivity to therapy.7 even in instances in which the paradigm of targeting an individual genomic alteration has been successful , adaptation of the tumor eventually leading to acquired resistance ultimately limits effectiveness . 
 hyman et al context key objective to determine if the - elective pi3k inhibitor alpelisib can be combined safely with the selective broblast growth factor receptor ( fgfr ) inhibitor ingratinib . knowledge generated alpelisib and ingratinib were successfully escalated in combination to full single - agent doses ; however , high rates of treatment interruption and dose reduction suggest long - term tolerability may be challenging . 
in exploratory signal - seeking cohorts of patients harboring dual pik3ca and fgfr1 - 3 alterations , no clear evidence of synergistic activity was observed . relevance additional studies are necessary to determine the potential role of combined pi3k and fgfr inhibition in treatment of various advanced solid tumors with alterations in pik3ca and / or fgfr1 - 3 . suggested that the combined inhibition of these oncogenes might be benecial.14 moreover , in breast cancer , pik3ca mutations often co - occur with fgfr1 gene amplications , indicating pik3ca and fgfr1 could cooperate as potential dual oncogenic drivers in this tumor type.12 , 15 similarly , concurrent activating pik3ca and fgfr2 mutations have been observed in endometrial carcinomas , with 90% or more fgfr2 - mutant endometrial cancers also exhibiting genomic activation of the pi3k pathway.16 - 18 taken together , these data provided a rationale for evaluating the feasibility and preliminary activity of combined fgfr and pik3ca inhibition in the clinic . to evaluate this therapeutic strategy , we studied the combination of alpelisib ( byl719 ) and ingratinib ( bgj398 )  . 
alpelisib is a selective class i pi3k inhibitor that recently demonstrated a statistically signicant and clinically relevant improvement in progression - free survival in a phase iii study ( solar - 1 ) of patients with pik3camutant , er + metastatic breast cancer.19 ingratinib is an orally bioavailable , selective pan - fgfr kinase inhibitor that has demonstrated single - agent activity in fgfr2 / 3altered bladder cancers and fgfr2 fusion - positive cholangiocarcinomas.20 , 21 we hypothesized that the combination of a selective fgfr and pik3ca inhibitors would be safe and would synergize in tumors with concurrent alteration of these oncogenes . 
dose escalation was guided by a bayesian logistic regression model with escalation with overdose control.22 in total , three arms in the expansion cohort were planned : dual pik3camutant and fgfr - altered breast ( arm 1 ) and nonbreast ( arm 2 ) cancers and pik3ca - mutant solid tumors ( arm 3 )  . because of the slow rate of accrual and overall safety prole , the study was closed before the target enrollment was completed . the primary objective was to determine the maximum tolerated dose and / or recommended dose for expansion of the combination of ingratinib and alpelisib . 
the secondary objectives included assessment of safety and tolerability of the combination , characterization of pharmacokinetic ( pk ) proles , assessment of preliminary antitumor activity as measured by overall response rate ( orr ) , and progressionfree survival ( pfs ) , per recist , version 1.1. study drug administration eligibility patients were at least 18 years of age and had advanced solid tumors with pik3ca mutation with or without fgfr genetic alteration in which standard therapy was unsuccessful . 
patients remained in the study until disease progression , unacceptable adverse investigator events ( aes ) , or withdrawal at patient or discretion . study assessments tumor responses were measured by recist , version 1.1 ( investigator assessed ) , using computed tomography or magnetic resonance imaging.23 assessments were performed at screening and every 8 weeks after rst treatment until disease progression . 
safety was monitored throughout institute the study according to the national cancer common terminology criteria for adverse events , version 4.03.24 ecgs were assessed and independently reviewed by a central laboratory . pharmacokinetic analysis during dose escalation , blood samples were collected to measure alpelisib and ingratinib plasma concentrations . samples were collected predose and 0.5 , 1 , 2 , 3 , 4 , 6 , 8 , and 24 hours postdose on cycle 1 day 1 , cycle 1 day 15 , and cycle 2 day 1 . 
drug plasma concentrations ( and active metabolites ) were measured using validated liquid chromatographytandem mass spectrometry with a lower limit of quantication of 1 ng / ml . genomic sequencing genomic alterations potentially associated with fgfr and pik3ca signaling were assessed from archival tumor specimens of fresh , pretreatment tumor biopsy specimens . for samples with sufcient tissue material ( n = 41 ) , nextgeneration sequencing ( ngs ) analysis was performed in a clinical laboratory improvement amendmentscertied laboratory ( foundation medicine , cambridge , ma ) using previously published methods.25 statistical analysis the data cutoff for all statistical analyses was august 23 , 2016 . 
the sample size for each expansion cohort was selected primarily for continued safety evaluation and was not powered for any specic efcacy end point . results patient demographics a total of 62 patients were enrolled in the study between october 2013 and august 2016 across 22 clinical centers in 12 countries . 
the median age of patients at the time of study entry was 60 ( range , 30 to 78 ) years , and all patients had an eastern cooperative oncology group performance status of 1 or less . 
patients were heavily pretreated , having received a median of three prior lines of systemic therapy . safety and tolerability dose - limiting toxicities were reported in three patients ( 10.7% ) who were included in the dose - escalation cohort ( n = 38 ) during the rst 28 days of treatment . 
dose - limiting toxicities included grade 4 hyperglycemia in one patient receiving alpelisib 300 mg and ingratinib 40 mg ; and grade 3 stomatitis in two patients ( one receiving alpelisib 300 mg and ingratinib 75 mg ; and the other receiving alpelisib 300 mg and ingratinib 100 mg )  . 
the recommended dose for expansion was determined to be alpelisib 300 mg once per day ( administered continuously ) and ingratinib 125 mg once per day ( administered on a schedule of 3 weeks on followed by 1 week off )  . overall , the safety prole of alpelisib and ingratinib was similar to the known safety proles of each agent ; no new major aes were noted ( table 2 )  . 
serious aes suspected to be drug related were reported in 12.9% of patients ( n = 8 of 62 ) overall and 16.1% ( n = 5 of 31 ) treated at the recommended dose for expansion . 
a total of 13 deaths ( 21% ) were reported during the study , including three ( 4.8% ) deaths resulting from disease progression while the patient was receiving study treatment . 
similarly , hyperglycemia , which is a biomarker of on - target pi3k inhibition , was also observed in 38.7% of all patients treated with alpelisib 200 mg or 300 mg , consistent with prior experience with this agent.27 for ingratinib , 37 patients ( 59.7% ) reported at least one dose interruption and 23 patients ( 37.1% ) reported at least one dose reduction . 
there was no or negligible pk interaction between ingratinib and alpelisib . antitumor efcacy in total , 52 patients were evaluable for response and 10 ( n = 6 in the dose escalation study ; n = 4 in the dose expansion study ) were nonevaluable on the basis of discontinuing therapy before the rst disease assessment ( table 3 )  . 
among 60 patients with a locally annotated pik3ca mutation reported , sequencing with high condence coverage was obtained centrally in 35 samples and the locally reported pik3ca variant conrmed in 80% patients ( n = 28 of 35 )  . 
 ( % ) , except where n = 0 . abbreviations : cr , complete response ; pd , progressive disease . * for patients who only had nontarget lesions at baseline and did not experience either a cr or pd , response is reported as non - cr / non - pd . patient with unknown best overall response due to ( 1 ) no valid postbaseline assessment , or ( 2 ) stable disease occurred too early ( , 6 weeks ) dened as patients who have best overall response cr , partial response , or stable disease , in which stable disease needs to occur at least 6 weeks after the rst dosing . squamous anal cancer with pik3ca e545k mutation . 
interestingly , in the patient with melanoma who had a pr , the only genomic activation of either pathway identied by central sequencing was an fgfr2 m722i mutation , an alteration not known to be recurrent or of biologic signicance.27 we also explored whether genetic alterations of the mapk pathway co - occurred with mutations in the fgfr and / or pi3k pathways and may account for lack of response , at least partially , in those settings . 
overall , ngs studies showed no clear association of alterations in the fgfr , pi3k , or mapk pathways with response . discussion to our knowledge , this is the rst study to evaluate the safety and preliminary efcacy of combined selective pi3k and fgfr inhibition in patients . 
we dened a recommended dose for expansion of alpelisib 300 mg once per day and ingratinib 125 mg once per day , 3 weeks on followed by 1 week off , which is the full single - agent dose and schedule of each drug . 
although this combination did not raise new specic safety concerns , 71% of patients required a dose interruption of alpelisib and 60% of patients reported at least one dose interruption of ingratinib during the course of treatment . 
of note , dose interruptions in the range of 50% to 70% have previously been reported with each agent when used individually , again suggesting that their combination may not be associated with signicant additive toxicity over the component parts but that long - term tolerance each drug alone can exhibit issues.20 , 28 , 29 no drug - drug interactions were reported between ingratinib and alpelisib . this study does have some important limitations . 
the relatively small number of patients treated with relevant concurrent alterations , as well as the heterogeneity of the population , do not permit a denitive assessment of synergistic efcacy . as such , any efcacy data presented from these expansions should be considered hypothesis generating only . second , we note that in the subset of 58% of patients ( n = 35 of 60 ) with tumor tissue in which successful central sequencing was completed , the pik3ca mutations were centrally conrmed in 80% of patients . 
as a result , some patients may have been enrolled on the basis of pik3ca mutations characterized by subclonality , spatial or temporal heterogeneity , or even test failures , as has been observed in prior genome - driven studies.7 finally , enrollment in the expansion cohorts for patients harboring concurrent pik3ca and fgfr1 - 3 alterations was not restricted to variants functionally characterized as activating but to regions of the affected genes that are recurrently the target of alteration . 
efcacy by ( a ) a waterfall plot depicting best percent change in the target tumor burden from baseline according to cohort and ( b ) a swimmer plot depicting progression - free survival by patients according to cohort . 
integrated genomic analysis of efcacy according to mutations in the fgfr , pi3k , and mapk pathways by central next - generation sequencing . ( * ) missing response data , as a result of discontinuation before rst response assessment . 
indel , insertion and / or deletion . fgfr amplication is partially dependent on the degree of amplication.30 both the inclusion of variants of unknown signicance as well as copy number amplications with a specic fold - change requirement may have adversely affected the observed orr by enrolling tumors without true pathway dependency on fgfr . despite these important limitations , a relatively low orr of only 9.7% across the entire study suggests that these two classes of agents may not provide synergistic activity . moreover , responses were generally observed in tumors arising from anatomic sites and harboring genetic alterations previously described as sensitizing to either alpelisib or ingratinib . 
it is also noteworthy that a signicant proportion of patients did not respond , or had stable disease as their best response , despite harboring pik3ca mutations alone or in combination with fgfr alterations . 
 hyman et al implementation has been identication of targeted therapy combinations have often been cited as a means of overcoming both intrinsic and acquired resistance , but a number of scientic , technical , and logistic impediments have made successful implementation challenging.31 , 32 perhaps the most difcult barrier to successful right drug combinations . 
enrichment for concurrent alterations of two oncogenes in one or multiple cancer types has served as one basis for selecting potential drug combinations and formed the basis of the hypothesis evaluated in this clinical study . 
recently , ndings were reported from two precision medicine studies , i - predict and winther , suggesting that a higher degree of molecular matching between somatic alterations detected at baseline and the therapy administered was associated with improved outcomes.33 , 34 although these results imply that targeting multiple oncogenic alterations with polytherapy may be a worthwhile strategy in select circumstances , the data presented here demonstrate that more rigorous evaluation of specic biomarker and drug combinations is required before the approach is more widely embraced . in conclusion , the combination of pik3ca and fgfr inhibition with alpelisib and ingratinib was feasible , although overall tolerability was limited by each agent . 
schellens , mario campone , cristiana sessa , giuseppe curigliano , jennifer bendiske , xueying chen , somesh choudhury , nancy lewis , jose manuel perez garcia , mara jos e de miguel - luken provision of study material or patients : luis paz - ares , jan h . 
craig lockhart , cristiana sessa , thomas zander , matthew ng , giuseppe curigliano , jose manuel perez garcia , mara jos e de miguel - luken collection and assembly of data : david m . 
craig lockhart , cristiana sessa , thomas zander , giuseppe curigliano , xueying chen , somesh choudhury , nancy lewis , jose manuel perez garcia , mara jos e de miguel - luken data analysis and interpretation : david m . 
schellens employment : modra pharmaceuticals stock and other ownership interests : modra pharmaceuticals honoraria : debiopharm group consulting or advisory role : debiopharm group research funding : dutch cancer society ( inst ) patents , royalties , other intellectual property : patent on oral taxanes philippe l . 
bedard research funding : bristol - myers squibb ( inst ) , sano ( inst ) , astrazeneca ( inst ) , roche ( inst ) , servier ( inst ) , glaxosmithkline ( inst ) , novartis ( inst ) , signalchem ( inst ) , ptc therapeutics ( inst ) , nektar ( inst ) , merck ( inst ) , seattle genetics ( inst ) , mersana ( inst ) , immunomedics ( inst ) , eli lilly ( inst ) mario campone honoraria : novartis , eli lilly consulting or advisory role : novartis ( inst ) , servier ( inst ) , menarini , sano ( inst ) , eli lilly ( inst ) , pzer ( inst ) , astrazeneca / medimmune ( inst ) , abbvie ( inst ) , pierre fabre ( inst ) , accord ( inst ) , sandoz - novartis ( inst ) speakers bureau : novartis , amgen research funding : novartis ( inst ) travel , accommodations , expenses : novartis , astra zeneca , pzer other relationship : roche philippe a . 
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nature 554 : 189 - 194 , 2018 [ erratum : nature 2019 ; 566 : e11 - e12 ] baselga j , campone m , piccart m , et al : everolimus in postmenopausal hormone - receptor - positive advanced breast cancer . 
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corcoran rb , atreya ce , falchook gs , et al : combined braf and mek inhibition with dabrafenib and trametinib in braf v600mutant colorectal cancer . j clin oncol 33 : 4023 - 4031 , 2015 11 . 
hortobagyi gn , chen d , piccart m , et al : correlative analysis of genetic alterations and everolimus benet in hormone receptorpositive , human epidermal growth factor receptor 2negative advanced breast cancer : results from bolero - 2 . 
nogova l , sequist lv , perez garcia jm , et al : evaluation of bgj398 , a broblast growth factor receptor 1 - 3 kinase inhibitor , in patients with advanced solid tumors harboring genetic alterations in broblast growth factor receptors : results of a global phase i , dose - escalation and dose - expansion study . 
pal sk , rosenberg je , hoffman - censits jh , et al : efcacy of bgj398 , a broblast growth factor receptor 13 inhibitor , in patients with previously treated advanced urothelial carcinoma with fgfr3 alterations . 
neuenschwander b , matano a , tang z , et al : bayesian industry approach to phase i combination trials in oncology , in zhao w , yang h , eds : statistical methods in drug combination studies . 
w ohrle s , bonny o , beluch n , et al : fgf receptors control vitamin d and phosphate homeostasis by mediating renal fgf - 23 signaling and regulating fgf - 23 expression in bone . 
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cancer discov 8 : 174 - 183 , 2018 javle m , lowery m , shroff rt , et al : phase ii study of bgj398 in patients with fgfr - altered advanced cholangiocarcinoma . 
scarlett uk , chang dc , murtagh tj , et al : high - throughput testing of novel - novel combination therapies for cancer : an idea whose time has come . 
indeed , triple - negative breast cancer ( tnbc ) , the most lethal breast cancer subgroup , has been reported to occur at a higher incidence in japan than in the united states . 
here , we sought to elucidate the geographic and ethnic diversity of breast cancer by examining actionable driver alterations in tnbc tumors from japanese patients and comparing them with the cancer genome atlas ( tcga ) database , which gathers data primarily from non - asian patients . materials and methods we performed comprehensive genomic profiling , including an analysis of 435 known cancer genes , among japanese patients with tnbc ( n = 53 ) and compared the results with independent data obtained from tcga ( n = 123 )  . results driver alterations were identified in 51 ( 96% ) of 53 japanese patients . 
by american society of clinical oncology introduction although breast cancer is one of the most frequently diagnosed cancers among women in the united states and japan , 1 , 2 its biologic characteristics may differ among different geographic or ethnic populations . 
indeed , breast cancer incidence , peak age of highest incidence , and mortality are different between women in the united states and japan.3 importantly , triple - negative breast cancer ( tnbc ) , the most lethal subgroup of breast cancer and characterized as estrogen receptor negative and progesterone receptor negative with no overexpression of human epidermal growth factor receptor 2 / neu , 4 is known to be more prevalent in japan than in the united states.5 , 6 large - scale genomic studies based on next generation sequencing ( ngs ) , such as the cancer genome atlas ( tcga ) and the international cancer genome consortium , have revealed important driver gene alterations in many types of solid tumors , 7 - 14 which have led to new targeted therapeutic strategies for precision cancer medicine.15 - 19 these studies have also highlighted the geographic and ethnic diversity in the cancer genome.20 , 21 however , most ngs - based studies have been conducted in western countries , where the asian population is a minority , and the resulting genomic information may not truly represent this population.8 for instance , only 5.5% of participants have identified themselves as asians in the tcga cohort . 
tnbc tumors in both the japanese cohort and the tcga database were defined according to previous reports.23 , 24 sequencing library preparation archival tissue in the formalin - fixed , paraffin embedded ( ffpe ) tumor obtained during routine biopsy or resection of primary tumor was used for analysis . 
all sample preparation , comprehensive genomic sequencing , and analytics were performed in a clinical laboratory improvement amendments / college of american pathologistsaccredited laboratory ( kew , cambridge , ma ) as described previously.19 comprehensive genomic sequencing ffpe genomic dna ( 50 to 150 ng ) was used to construct libraries that were enriched for 435 genes using cancerplex ( kew ) as described previously.19 the term gene alterations is used when there are genetic aberrations such as amplifications in addition to mutations . 
to compare the mutational burden of the 435 - gene panel with that of the tcga whole - exome sequencing ( wes ) data , the data set of single - nucleotide polymorphisms was downsampled to the 435 genes in the panel , and the panel mutation rate was determined , calculated as mutations per megabase , as described previously.19 results genetic alterations in japanese patients with tnbc the clinicopathologic characteristics of the patients with tnbc in the japanese and tcga cohorts are summarized in the data supplement . 
the japanese cohort included more patients with m1 disease ( 11% ) compared with the tcga cohort ( 1% ; p < .01 ) , which seemed to affect the difference in stage among the two cohorts ( data supplement )  . 
after performing comprehensive genomic sequencing on all japanese tnbc samples , we found at least one alteration in 82 of 435 cancer - associated genes ( fig 1 ; data supplement )  . 
although a total of 186 alterations were found in the 53 patients , there were only three frequently altered genes ( seen in > 10% of patients ) : tp53 , pik3ca , and pten ( fig 1 )  . 
among them , biopsy specimens of primary tumors before neoadjuvant chemotherapy were used for analysis in 11 patients , and surgical specimens of remnant primary tumors after neoadjuvant chemotherapy were used in 24 patients ( data supplement )  . 
 ( * ) p < .05 for alteration frequencies between japanese patients and the tcga cohort . genes including those for tp53 , pik3ca , and pten , were comparable between the two groups ( data supplement )  . 
of note , there were two distinct categories in the tcga cohort : tnbc based on pathologic subtyping and basal - like breast cancer based on pam50 analysis , with some overlap between the two groups . 
interestingly , the tp53 alteration rate in tnbc ( 65 [ 52.8% ] of 123 ) was relatively low in the tcga cohort , although the rate in basal - like breast cancer ( 73 [ 78.5% ] of 93 ) was much higher in the same cohort ( data supplement )  . 
generally , the gene alteration rates were comparable between japanese patients and the tcga cohort ; however , the alteration frequencies in two genes ( myc and ptk2 ) were significantly different between the two cohorts ( fig 1 ; data supplement )  . similar to that of the tcga cohort ( figs 2a to 2j )  . 
however , there were some exceptions , such as significantly more amplification of myc in the tcga cohort ( 28% ) than in japanese patients ( 6% ; p < .01 ; fig 2 )  . we found that eight patients ( 15% ) showed brca1 / 2 alterations , including five brca1 and three brca2 alterations ( figs 2a to 2j )  . 
moreover , bioinformatic analysis revealed that seven of eight alterations were possible germ line alterations , based on the allelic fraction and alteration site compared with a database , such as clinvar ( table 1 )  . 
we did not confirm the germ line alteration using patients normal tissue . genomic alterations in cancer signaling pathways tumor mutational burden and microsatellite instability in patients with tnbc we next assessed genomic alterations in major oncogenic pathways involving phosphatidylinositol 3 - kinase , the cell cycle , dna double strand break ( dsb ) repair , erbb2 / kras , and - catenin / wnt signaling and determined whether there were differences between the two cohorts ( figs 2a to 2j )  . 
overall , the gene alteration spectrum of the japanese cohort was a high tumor mutational burden ( tmb - h ) tumor is defined as a tumor with a high rate of somatic mutation . 
 ( a - e ) japanese patients ( n = 53 ) and ( f - j ) the cancer genome atlas ( tcga ) cohort ( n = 123 ) were evaluated for gene alterations in key cancer pathways : ( a , f ) phosphatidylinositol 3 - kinase ( pi3k ; 45% and 25% of patients , respectively ) , ( b , g ) cell cycle ( 26% and 29% of patients , respectively ) , ( c , h ) dna double - strand break ( dsb ) repair ( 75% and 58% of patients , respectively ) , erbb2 / kras ( 17% and 11% of patients , respectively ) , and ( e , j ) - catenin / wnt ( 11% and 29% of patients , respectively )  . 
this classification was based on our previous studies of colorectal and gastric cancers , which included a number of patients with microsatellite instability , although no microsatellite instability was observed in any of the 53 japanese patients with tnbc ( fig 3a )  . 
 ( a ) mutation rate and microsatellite instability ( msi ) in patients with triple - negative breast cancer in japan ( n = 53 ) ; three ( 5.7% ) of 53 hypermutated . 
 ( b ) mutation rate data from whole - exome sequencing ( wes ) for the cancer genome atlas cohort ( n = 123 ) were downsampled to the content of the 435 - gene panel platform ; six ( 4.9% ) of 123 hypermutated . 
cluster one ( n = 83 ; 47.2% ) , in which no common actionable alterations were seen , was the largest of the 10 identified clusters , and cluster nine ( n = 23 ; 13.1% ) , in which pik3ca alterations were common , was the second largest cluster ( fig 4b )  . 
cluster seven ( n = 16 ) was characterized by pten alterations , cluster eight ( n = 12 ) was characterized by cdkn2a and cdkn2b alterations , and clusters six ( n = 6 ) and three ( n = 6 ) were characterized by brca1 and brca2 alterations , respectively . 
moreover , cluster two ( n = 7 ) contained fgfr1 alterations , cluster four ( n = 7 ) contained ddr2 alterations , and cluster five ( n = 10 ) contained ccnd2 / 3 alterations . 
 a d0578 d0575 d0588 d0600 tcgaewa1p701 tcgaewa1p401 d0605 d0601 d0606 d0607 d0611 d0610 d0614 d0616 d0717 d0716 d0719 d0735 d0741 d0739 tcgaa2a0d001 tcgaa2a0d201 tcgaa2a0t201 tcgaa2a0st01 tcgaa2a1g601 tcgaa7a26g01 tcgaana0fx01 tcgaa8a07c01 tcgaana0g001 tcgaaoa03u01 tcgaaoa12801 tcgaaoa0j401 tcgaara0ts01 tcgaara0u101 tcgab6a0iq01 tcgaara1ay01 tcgab6a0re01 tcgab6a0rs01 tcgab6a0wx01 tcgab6a0ru01 tcgabha0av01 tcgabha0b901 tcgabha0rx01 tcgabha0bl01 tcgabha1fc01 tcgac8a26y01 tcgad8a27f01 tcgad8a1jl01 tcgad8a27m01 tcgae2a14r01 tcgae2a15801 tcgae2a14x01 tcgae2a1b601 tcgae2a1l701 tcgae2a1lk01 tcgae2a1li01 tcgae2a1ls01 tcgaewa1p101 tcgad8a1jf01 tcgaara1aq01 d0597 tcgad8a1xk01 tcgabha18t01 tcgae2a15001 tcgabha18q01 tcgad8a1jg01 tcgac8a13401 d0595 tcgaewa1p801 tcgaa7a0da01 tcgaara0tu01 tcgac8a27b01 tcgaaoa0jl01 tcgac8a26x01 d0625 d0609 tcgaa7a26i01 tcgaa8a09x01 tcgad8a14201 tcgaa7a26f01 tcgaana0fl01 tcgaa2a04q01 d0581 tcgaara1ar01 d0574 tcgaa2a0ym01 tcgabha0e601 tcgaara25601 tcgae2a1lh01 tcgae2a1lg01 tcgaana04d01 d0718 tcgaara1ai01 d0577 tcgaa7a0ce01 d0586 tcgab6a0rt01 tcgaa2a0cm01 tcgac8a1hj01 tcgad8a14701 tcgaa8a07o01 tcgabha0e001 tcgaaoa12901 tcgaa2a04t01 tcgaa1a0sk01 tcgae2a1az01 tcgae9a22g01 d0584 tcgaa1a0sp01 d0585 tcgaana0ar01 tcgaewa1ow01 tcgaaoa12f01 d0736 d0594 tcgaana0xu01 tcgabha18g01 tcgaa1a0so01 tcgabha0wa01 tcgaaoa0j201 d0738 tcgae2a15901 tcgae9a1nd01 d0580 tcgabha0b301 d0598 tcgaara0u001 d0579 d0599 tcgaewa1ov01 tcgaewa1pb01 tcgaa2a0ye01 d0590 tcgad8a13z01 tcgaa2a0t001 tcgabha0bg01 d0589 tcgabha0bw01 tcgaana0al01 d0740 tcgabha18v01 tcgaana0at01 d0604 tcgaara0u401 tcgaaqa04j01 tcgae2a1ll01 tcgaa2a04u01 tcgad8a1xq01 tcgabha1ew01 tcgad8a27h01 tcgaa2a0sx01 tcgaaoa12401 tcgac8a13101 d0596 tcgaa2a04p01 d0592 d0591 d0576 d0733 d0638 d0583 d0742 tcgaa8a08r01 tcgab6a0rg01 tcgab6a0ie01 tcgac8a12v01 tcgab6a0rn01 tcgab6a0ik01 tcgad8a14301 d0572 d0587 tcgae2a14n01 tcgaaoa0j601 d0615 d0573 d0582 donors fig 4 . 
 ( a ) a cluster analysis was performed on 176 cases of triple - negative breast cancer ( tnbc ; 53 tumors from japanese patients and 123 tumors from the cancer genome atlas [ tcga ] cohort ) by using euclidean distance and wards clustering method ( distance based on common mutated genes are colored blue to yellow )  . 
ado - trastuzumab , emtansine , lapatinib , pertuzumab , trastuzumab japanese , 3 ( 5.7% ) of 53 ; tcga , 6 ( 4.9% ) of 123 kit , pdgfr , abl imatinib japanese , 2 ( 3.8% ) of 53 ; tcga , 15 ( 12.2% ) of 123 jak1 / 2 . 
belinostat , panobinostat , vorinostat japanese , 0 ( 0% ) of 53 ; tcga , 6 ( 4.9% ) of 123 ceritinib , crizotinib , alectinib japanese , 0 ( 0% ) of 53 ; tcga , 5 ( 4.1% ) of 123 vegfr2 . 
genetic alterations in japanese patients with triple - negative breast cancer and patients in the cancer genome atlas ( tcga ) cohort potentially targetable by us food and drug administration ( fda ) approved cancer therapies . 
interestingly , we similarly analyzed the tcga cohort and found that , as with the japanese cohort , 66.7% of cases had at least one potentially actionable alteration associated with fda - approved drugs . for japanese patients , genes associated with mammalian target of rapamycin ( mtor ) , poly ( adp - ribose ) polymerase ( parp ) , and cdk4 / 6 inhibitors showed the three highest alteration rates ( fig 5 )  . 
seventeen percent of japanese patients and 22% of tcga cases had alterations in actionable genes related to the cell - cycle pathway , which could be treated by cdk4 / 6 inhibition . 
moreover , other fda - approved drugs , including multitargeted tyrosine kinase inhibitors , mek inhibitors , antihuman epidermal growth factor receptor 2 therapies , and jak inhibitors , were indicated as potential targeted therapies for japanese patients with tnbc , with even more drugs suggested for tcga cases ( fig 5 )  . 
of note , oncoprint analysis showed coalterations in many cases of tnbc in both cohorts , which may be associated with resistance to the targeted therapies ( fig 5 )  . 
however , the overall alteration spectrum of the japanese patients was similar to that of the tcga cohort.8 importantly , 66% of japanese patients , as well as 67% of tcga cases , had at least one genomic alteration in actionable genes , providing potentially new treatment strategies . we demonstrated significant differences in the frequencies of alterations in two genes : ptk2 and myc . 
it has been previously reported that myc is one of the most important driver genes , and there are known ethnic differences in myc amplification frequency.30 although we found a myc amplification rate of 5.7% in our cohort , high incidence ( 30% to 35% ) of myc amplification has been repeatedly reported from us groups , similar to tcga rates.31 - 33 a unique patient population comprises the cohort described in our study , which could be useful given the sparse genomic data from asian tnbc populations . we analyzed genomic alterations in ffpe tumor tissue from a cohort of japanese patients with tnbc by comprehensive ngs - based sequencing of a panel of 435 cancer - relevant genes , at an average 500 depth . 
method of preservation is critical for dna analysis using ffpe tissue samples , as we reported previously.34 the quality of all dna samples used in this study was confirmed to be adequate for accurate ngs analysis by strict quality control checks . 
indeed , most of the genes altered in both the japanese and tcga cohorts showed similar frequencies , consistent with previous reports , despite the different sequencing techniques used . previous comprehensive genomic profiling studies have reported that tnbc is a heterogeneous disease involving diverse genomic alterations.8 , 35 , 36 our results also demonstrated the heterogeneity of tnbc , with only three genes mutated in > 10% of patients and most of the genetic alterations differing from one another . 
 more comprehensive approach , such as the one used in this study , will be required to find actionable alterations in each patient with tnbc . to explore the clinical utility of targeted sequencing with a large panel for tnbc , we identified actionable genes that can be treated by fda - approved drugs and found that 35 japanese patients ( 66% ) had at least one such actionable gene alteration . 
we identified several signaling pathways for molecular targeted therapies , including the pi3k pathway for mtor inhibitors , the dsb repair pathway for parp inhibitors , and the cell - cycle pathway for cdk4 / 6 inhibitors ( fig 5 )  . 
although none of these patients received immune checkpoint inhibitor therapy , there is a high likelihood that these patients may have responded , given clinical data demonstrating efficacy in tmb - h patients . in our study , we found that seven ( 13% ) of 53 japanese patients with tnbc had possible germ line brca1 / 2 alterations based on bioinformatic analysis of tumor dna . 
although specific genetic tests are needed to confirm the frequency of germ line brca1 / 2 alterations , this estimated frequency is in agreement with previous reports.40 recently , germ line alteration of brca1 / 2 has attracted increasing attention because of the use of parp inhibitors . 
therefore , we considered 53 as a sufficient number for the japanese cohort , at least to the extent that the alteration rate of more than one gene was significantly different between the japanese and tcga cohorts . another limitation is that we included patients receiving neoadjuvant chemotherapy , and we cannot exclude the possibility that the neoadjuvant chemotherapy affected genomic alterations . 
however , when we compared the gene alterations between the chemotherapy - nave tissue samples ( n = 29 ) and chemotherapy affected tissue samples ( n = 24 ) , we found that gene alteration frequencies , including those for tp53 , pik3ca , and pten , were comparable between the two groups ( data supplement )  . 
 moreover , considering that we did not see major differences in genomic alterations between the japanese and tcga cohorts except for myc , it is unlikely that neoadjuvant chemotherapy dramatically influenced the landscape of driver alterations . 
although it is not easy yet in japan to recruit a large number of patients with tnbc for genomic sequencing , additional studies with a greater number of patients are warranted to confirm our findings in the future . despite these limitations , to our knowledge , this is the largest cohort of japanese patients with tnbc to undergo comprehensive genomic profiling to date , and our data provide important insights into the molecular heterogeneity underlying this aggressive disease from an ethnogeographic perspective . 
although our study indicates the possibility of targeted therapies for patients with tnbc , an accumulation of clinical evidence will be required to reveal the usefulness of each therapy for this disease . 
 are required to reveal potential treatments for patients with tnbc . in conclusion , our study revealed actionable driver alterations in japanese patients with tnbc that could potentially be treated with existing drugs . 
tsuchida j , nagahashi m , rashid om , et al : at what age should screening mammography be recommended for asian women ? cancer med 4 : 1136 - 1144 , 2015 4 . 
barnes dm , harris wh , smith p , et al : immunohistochemical determination of oestrogen receptor : comparison of different methods of assessment of staining and correlation with clinical outcome of breast cancer patients . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
rizvi na , hellmann md , snyder a , et al : cancer immunology : mutational landscape determines sensitivity to pd - 1 blockade in non - small cell lung cancer . 
parsons ha , beaver ja , cimino - mathews a , et al : individualized molecular analyses guide efforts ( image ) : a prospective study of molecular profiling of tissue and blood in metastatic triple - negative breast cancer . 
radovich m , clare se , atale r , et al : characterizing the heterogeneity of triple - negative breast cancers using microdissected normal ductal epithelium and rna - sequencing . 
 high detection rate of myd88 mutations in cerebrospinal fluid from patients with cns lymphomas jun watanabe , md1 ; manabu natsumeda , md , phd1 ; masayasu okada , md , phd1 ; daiki kobayashi , ms1 ; yu kanemaru , md1 ; yoshihiro tsukamoto , md , phd1 ; makoto oishi , md , phd1 ; akiyoshi kakita , md , phd1 ; and yukihiko fujii , md , phd1 purpose biopsy is the gold standard for the diagnosis of primary cns lymphoma ( pcnsl )  . 
furthermore , we performed dna sequencing of myd88 in 21 cases with available surgically obtained formalin - xed parafn - embedded ( ffpe ) tissue and compared the results . results the median cfdna amount extracted from 1 ml csf was 219 ng / ml ( 25th to 75th percentile , 129 to 333 ng / ml )  . 
2019 by american society of clinical oncology introduction primary cns lymphomas ( pcnsls ) are highly malignant neoplasms ; the incidence of pcnsl has been increasing , and it accounts for 4% of all primary brain tumors.1 , 2 stereotactic or open biopsies are the gold the diagnosis of pcnsl.3 however , standard for pcnsl often occurs in deep brain structures , such as the basal ganglia and brain stem , and hemorrhage as a result of biopsy may cause serious morbidity or even mortality . 
therefore , a more minimally invasive , reliable , and rapid diagnostic method is needed . there has been growing interest in cancer diagnosis using cell - free dna ( cfdna ) as a source for tumor biomarkers in cancers , including malignant lymphomas.4 , 5 systemic diffuse large b - cell lymphomas ( dlbcls ) are known to be clinically and morphologically heterogeneous.6 hans et al6 classied dlbcl into the activated b - cell type ( abc type ) and germinal center b cell type ( gcb type )  . 
in abc - type dlbcl , somatic mutations are frequent in genes in the b - cell receptor signaling pathway , the toll - like receptor / interleukin - 1 receptor pathway , and the nuclear factor - b pathway.7 of these mutations , ngo et al7 has shown that myeloid differentiation primary response 88 gene ( myd88 ) mutations are the driver mutations for dlbcl and are related to activation of nuclear factor - b pathway and janus kinase - signal transducer and activator of transcription 3 ( jakstat3 ) signaling . 
the majority of pcnsls were reported to be of abc type.8 furthermore , the prevalence of myd88 mutations is reported to be more common in pcnsl than in systemic dlbcl.9 - 15 therefore , detecting these mutations may serve as a genetic marker for the diagnosis of pcnsl and a potential basis for molecularly targeted therapy . 
 watanabe et al context key objective to date , it is not known whether myd88 mutation , an important driver mutation of primary cns lymphoma , can be reliably detected from cell - free dna ( cfdna ) taken from cerebrospinal uid ( csf )  . 
in patients with primary cns lymphoma , detection of cfdna from the blood has been reported ; however , the detection rate is low . knowledge generated we showed that myd88 mutations were detected in cfdna extracted from 1 ml of csf from 76.9% ( 20 of 26 patients ) by combination of sanger sequencing and droplet digital polymerase chain reaction . 
detection of mutation was 100% concordant with that of tumor dna taken from matched tissue in 21 available cases . relevance these results showed that tumor cfdna is abundant in the csf , and tumor cfdna taken from the csf can be used as a lessinvasive molecular diagnostic and monitoring tool . 
in the near future , patients may not need surgery for the diagnosis . to date , the detection of cfdna from cerebrospinal uid ( csf ) in pcnsl has been reported in only two cases.18 , 19 the aim of this study is to determine whether reliable detection of myd88 mutations is possible in csf taken from patients with cns lymphomas . 
this study was approved by the institutional review board , and written informed consent to use csf and resected tissue for research purposes was obtained from patients ( #g20180008 )  . 
dna was extracted from formalin - xed parafn - embedded ( ffpe ) tissue in 21 cases using the qiaamp ffpe tissue kit ( qiagen , valencia , ca )  . 
sections were incubated with the working dilution of each antibody raised against the following antigens as previously described20 : cd10 ( clone 56c6 ; leica , vienna , austria ; diluted 1 : 100 ) , bcl - 6 ( clone pg - b6p ; dako , glostrup , denmark ; diluted 1 : 50 ) , mum1 ( clone mum1p ; dako ; diluted 1 : 200 )  . 
tumors were subclassied according to the expression pattern of gcb and abc markers , using the methods published by hans et al.6 determination of tumor volume post - contrast t1 - weighted sequences were used to dene the tumor volume as the area of contrast enhancement including central necrotic tissue . 
to determine the volume , we measured the tumor area in each slice using a region - ofinterest method ( brainlab software ; brainlab , feldkirchen , germany )  . 
although volumetrics is well established , this method is highly subjective and likely underestimates the total tumor volume . statistical analysis the sample size of generated data was small , so the data were considered to have a nonparametric distribution . 
the kaplan - meier method was used to estimate progressionfree survival ( pfs ) and overall survival ( os ) , and log - rank test was used to test for signicance . 
pfs was calculated from the day of diagnosis until magnetic resonance imagingconrmed tumor progression or end of follow - up . os was dened as the interval from the day of diagnosis until death or the end of follow - up . 
l265p in exon5 was the most frequent myd88 mutation found in 19 of 20 ( 95.0% ) cases ( fig 1b ) , and s219c in exon 3 was detected in one case ( fig 1c )  . 
likewise , myd88 mutation was not detected in the six patients with myd88wild - type tumor , yielding a 100% match of myd88 detection between csf and tumor - derived biopsy specimen . comparison of sanger sequencing and ddpcr first , we performed sanger sequencing in cfdna extracted from csf . 
mutations for l265p were detected in 15 cases , and s219c mutation was detected in one case ( fig 2 )  . however , in 10 cases we found the overlapping peaks to be small or not detectable , making the determination of mutant or wild type by sanger sequencing difcult . 
in two out of four ( 50% ) cases in which mutation could be detected only by ddpcr , magnetic resonance images showed little to no contrast - enhancing lesions localized to the brainstem ( figs 4a - 4c )  . 
after incubation at 4c for 2 hours , the amount of cfdna decreased to approximately one - third compared with rapid processing ( appendix fig a3 ) , and myd88 mutation was difcult to detect even by ddpcr . definite l265p s219c ( n = 15 ) ( n = 1 ) nondefinite ( n = 10 ) discussion mutant ( n = 4 ) myd88 mutant type l265p s219c ( n = 20 ) ( n = 19 ) ( n = 1 ) ddpcr wild type ( n = 6 ) wild type ( n = 6 ) in this study , a high detection rate of myd88 mutations in csf from patients with cns dlbcls was achieved . 
in the 21 cases with sufcient surgically obtained ffpe tissue for the detection of myd88 mutation from dna analysis , cfdna was 100% consistent with that of tumor - derived dna from ffpe tissue . 
therefore , we used sanger sequencing to screen for myd88 mutations and subsequently performed ddpcr to conrm specic mutations . furthermore , we found that obtaining high concentrations of cfdna is important . 
as has already been reported in glioma and metastatic brain tumors , tumor - derived dna could be found in csf located in the proximity of neoplastic lesions.23 , 24 especially in pcnsl , in which the primary site fig 2 . 
in two cases , we analyzed the myd88 l265p mutation before and during chemotherapy . patients in cases 5 and 14 received methotrexate , procarbazine , and vincristine.21 the amount of cfdna and number of mutant droplets serially decreased with treatment ( appendix fig a1 )  . pfs and os were compared between myd88 - mutant ( n = 12 ) versus myd88wild - type cases ( n = 2 ) , and no difference was detected ( pfs : p = .831 ; os : p = .464 ; logrank test )  . 
likewise , no difference in pfs and os were detected between high ( n = 7 ) versus low ( n = 7 ) cfdna amount ( pfs : p = .252 ; os : p = .824 ; appendix fig a2 )  . because the number of newly diagnosed pcnsl cases is small ( n = 14 ) and the observation period is short , it is still difcult to draw any conclusions . cfdna stability in csf to study the stability of cfdna , we examined the concentration of cfdna and the time from csf collection to storage at 80c in two cases . 
magnetic resonance imaging showed a tumor on the left side of the midbra ( a - c ) diffusion - weighted images ( a ) and uid attenuated inversion recovery ( b ) showed high signal intensity ; however , contrast enhancement was not observed in post - contrast t1 - weighted images ( c )  . 
 ( d , e ) l265p mutation was detected by sanger method in formalin - xed parafn - embedded ( ffpe ) tissue ( d ) , whereas l265p mutation was not detected in csf by sanger sequencing ( e )  . 
 ( f ) several l265p - mutant droplets were conrmed in csf by droplet digital polymerase chain reaction ( ddpcr )  . is still controversial , future studies directly comparing matched plasma and csf cfdna concentrations are needed . 
in addition , lumbar puncture has a possibility of blood contamination . this is certainly relevant in patients with systemic lymphoma . we should also consider the clearance of cfdna in addition to release of cfdna . 
it was reported that clearance of fetal cfdna from the plasma of pregnant women had a mean half - life of 16 to 60 minutes.25 , 26 although there has been no prior study of the clearance of cfdna in csf , the present analysis showed that promptly centrifuging and storing the supernatant is important to obtain a sufcient amount of cfdna . 
as previously reported , 28 we found that isolation efciency of cfdna by the maxwell rsc machine was superior to that of traditional methods using other dna extraction kits ( data not shown )  . 
myd88 mutations have been reported so far in only b - cell malignancies such as dlbcl , waldenstrom macroglobulinemia , and igm monoclonal gammopathy.32 it has also been conrmed that myd88 mutations do not appear in gliomas , which proves useful because gliomas are often considered for differential diagnosis.13 according to a large - scale study , myd88 l265p mutation was found in only one out of 12 , 380 healthy individuals.33 myd88 mutation in dlbcl has also been reported as a negative prognostic factor for patients undergoing concurrent methotrexate - based polychemotherapy.34 , 35 with the introduction of targeted therapies , it is anticipated that myd88 mutation will become a positive predictive factor in the future.36 the bruton tyrosine kinase inhibitor ibrutinib was found to be effective in abc - type systemic dlbcl , especially in cases with myd88 l265p mutation.36 furthermore , gromme et al37 and lionakis et al38 reported that ibrutinib was also effective for relapsed pcnsl . 
detection of myd88 mutations will enable the timely commencement of treatment in mutationpositive cases and might be used for monitoring treatment response and detecting early relapse , thus potentially contributing to an improved outcome in patients with pcnsl . in conclusion , the current study shows that reliable detection of myd88 mutations in patients with cns dlbcls was possible . 
crit rev oncol hematol 113 : 97 - 110 , 2017 scherer f , kurtz dm , newman am , et al : distinct biological subtypes and patterns of genome evolution in lymphoma revealed by circulating tumor dna . 
sci transl med 8 : 364ra155 , 2016 rossi d , diop f , spaccarotella e , et al : diffuse large b - cell lymphoma genotyping on the liquid biopsy . 
hans cp , weisenburger dd , greiner tc , et al : conrmation of the molecular classication of diffuse large b - cell lymphoma by immunohistochemistry using a tissue microarray . 
nature 470 : 115 - 119 , 2011 kreher s , j ohrens k , strehlow f , et al : prognostic impact of b - cell lymphoma 6 in primary cns lymphoma . 
neuro - oncol 17 : 1016 - 1021 , 2015 gonzalez - aguilar a , idbaih a , boisselier b , et al : recurrent mutations of myd88 and tbl1xr1 in primary central nervous system lymphomas . 
yamada s , ishida y , matsuno a , et al : primary diffuse large b - cell lymphomas of central nervous system exhibit remarkably high prevalence of oncogenic myd88 and cd79b mutations . 
nakamura t , yamashita s , fukumura k , et al : genome - wide dna methylation proling identies primary central nervous system lymphoma as a distinct entity different from systemic diffuse large b - cell lymphoma . 
zheng m , perry am , bierman p , et al : frequency of myd88 and cd79b mutations , and mgmt methylation in primary central nervous system diffuse large 16 . 
fontanilles m , marguet f , bohers e , et al : non - invasive detection of somatic mutations using next - generation sequencing in primary central nervous system 17 . 
hattori k , sakata - yanagimoto m , suehara y , et al : clinical signicance of disease - specic myd88 mutations in circulating dna in primary central nervous b - cell lymphoma . 
hiemcke - jiwa ls , minnema mc , radersma - van loon jh , et al : the use of droplet digital pcr in liquid biopsies : a highly sensitive technique for myd88 p . ( l265p ) detection in cerebrospinal uid . 
zorofchian s , lu g , zhu jj , et al : detection of the myd88 p.l265p mutation in the csf of a patient with secondary central nervous system lymphoma . 
aoki h , ogura r , tsukamoto y , et al : advantages of dose - dense methotrexate protocol for primary central nervous system lymphoma : comparison of two different protocols at a single institution . 
de mattos - arruda l , mayor r , ng cky , et al : cerebrospinal uid - derived circulating tumour dna better represents the genomic alterations of brain tumours 24 . 
wang y , springer s , zhang m , et al : detection of tumor - derived dna in cerebrospinal uid of patients with primary tumors of the brain and spinal cord . 
fernando mr , chen k , norton s , et al : a new methodology to preserve the original proportion and integrity of cell - free fetal dna in maternal plasma during sample processing and storage . 
sorber l , zwaenepoel k , deschoolmeester v , et al : a comparison of cell - free dna isolation kits : isolation and quantication of cell - free dna in plasma . 
schroers r , baraniskin a , heute c , et al : detection of free immunoglobulin light chains in cerebrospinal uids of patients with central nervous system diagn 19 : 162 - 168 , 2017 lymphoma . 
schroers r , baraniskin a , heute c , et al : diagnosis of leptomeningeal disease in diffuse large b - cell lymphomas of the central nervous system by ow cytometry and cytopathology . 
hattori k , sakata - yanagimoto m , okoshi y , et al : myd88 ( l265p ) mutation is associated with an unfavourable outcome of primary central nervous system 35 . 
takano s , hattori k , ishikawa e , et al : myd88 mutation in elderly predicts poor prognosis in primary central nervous system lymphoma : multi - institutional lymphoma . 
 detection of myd88 mutations from csf in cns lymphoma appendix direct sequencing for myd88 mutations twenty nanograms of cell - free dna ( cfdna ) were amplied using primers for the detection of the myd88 mutations . 
next , we performed sequencing of other known myd88 point mutations ( s219c , m232t , v233m , d239n , p267s , i266v , t285i , c293y , t294i , t200i ) in l265p wild - type cases . the rst set of primers within exon 5 had a product of 383 bp : ( 1 ) forward 5 - gctgttgttaaccctggggttgaag - 3 and ( 1 ) reverse 5gacgtgtctgtgaagttggcatctc - 3 . 
the exon 3 primers had a product size of 310 bp : ( 3 ) forward 5 - aagccttcccatggagctctgaccac - 3 and ( 3 ) reverse 5 - gctaggaggagatgcccagtatctg - 3 . 
the 20l pcr mix , composed of 10 l of 2 ddpcr supermix for probes ( no deoxyuridine triphosphate ; bio - rad ) , 1 l ddpcr mutation assay ( bio - rad ) , and 9 l cfdna was loaded into sample wells of an eightchannel disposable droplet generator cartridge ( bio - rad )  . 
after droplet generation , droplets were transferred into a 96 - well pcr plate and proceeded to thermal cycling . amplication was carried out on the 20 - l reaction mixture on the qx200 ddpcr system ( bio - rad )  . 
after pcr , the 96 - well pcr plate was subjected to the qx - 200 droplet reader ( bio - rad ) , and data were analyzed by quantasoft analysis software ( bio - rad )  . 
myd88 l265p mutation - specic signals were generated in the 6 - uorescein amidite channel , and myd88 wild - type signals were generated in the hexachloro - uorescein channel . 
the cfdna amount at baseline and after methotrexate , procarbazine , and vincristine ( mpv ) two courses from case 5 ( b , c ) and case 14 ( e , f )  . 
this study was performed to characterize mutagenesis and mutational target genes underlying lung carcinogenesis in patients with uip . patients and methods a cohort of 691 japanese patients with lung adenocarcinoma ( ladc ) , of whom 54 had uip and 637 did not , was studied for driver oncogene aberrations . 
2018 by american society of clinical oncology introduction smoking is a major risk factor for lung cancer , 1 and its mutagenic process and mutational targets , including kras and tp53 , have been elucidated.2 smoking is also a pathogenic factor for idiopathic pulmonary fibrosis ( ipf ) , which is pathologically diagnosed as usual interstitial pneumonia ( uip ) , 3 characterized by destruction of alveolar architecture in association with fibrosis.4 uip is a strong risk factor for lung cancer independent of smoking ( relative risk , 8.25 ) 5 and increases the cumulative incidence rate of lung cancer within 10 years to 54.7%.6 notably , deleterious germline mutations in pulmonary surfactant system genes ( pssgs ) , including nkx2 - 1 / ttf1 , sftpa1 , sftpa2 , sftpb , and sftpc , have been implicated in familial neonatal respiratory failure and fibrotic lung disease , 7 as well as in lung cancer development.8 , 9 therefore , loss of function of pssgs in morphogenesis / maintenance of alveolar structure7 might also play a role in uip and subsequent development of lung cancer in individuals with germline pssg mutations . 
however , such tumors are rarely subjected to surgical resections ( 3.1% ; 1 , 300 of 41 , 742 ) , 10 largely because of the risk of acute exacerbation of interstitial pneumonia and an associated high mortality rate.10 consequently , no comprehensive genomic analysis of uip - associated lung cancers has been published to date . 
one of the few genetic characteristics of these cancers reported previously is that egfr oncogene mutations are relatively infrequent in uip - associated lung adenocarcinomas ( ladcs ) .11 - 13 in this study , we performed comparative and comprehensive genomic characterization of ladcs with and without uip . 
ladc was chosen for comparison for several reasons : it is the most common histologic type of lung cancer and frequently develops in the lungs of patients suffering from uip11 ; the genetic aberrations responsible for carcinogenesis , represented by driver oncogene aberrations , 14 - 16 have been well documented ; and mutational signature studies17 have revealed the mutational events underlying this disease , which include dna damage / adduct formation as a result of smoking , spontaneous deamination of 5 - methylcytosine , 18 and the action of apolipoprotein b mrna editing enzyme catalytic polypeptide - like cytidine deaminases.19 to deduce the mutagenic processes and elucidate commonly affected genes , we examined driver oncogene aberrations in a cohort of 691 patients with ladc , including 54 patients who were uip positive and 637 patients who were uip negative , and performed whole - exome sequencing ( wes ) analysis in 296 ladcs ( 51 uip positive and 245 uip - negative )  . 
of those , 679 were consecutive patients who underwent surgical resection between 1997 and 2008 at the national cancer center ( ncc ) hospital ( ncch ) , tokyo , and for which snap - frozen cancerous and noncancerous lung tissues suitable for genome analysis were available in the ncc biobank . 
 surgical specimens of these patients were classified as uip negative and uip positive ( 637 and 42 cases , respectively ) on the basis of previously described pathologic criteria.20 uip positivity was defined as the presence of the uip pattern ( on the basis of the 2002 american thoracic society / european respiratory society4 and 2011 ipf criteria3 )  . 
uip - positive cases were defined as those having tumorous lesions located within or adjacent to uip lesions ; tumors discontinuous to the uip lesions were excluded ( appendix )  . 
 to increase the number of uip - positive cases , an additional 12 patients who underwent surgical resection between 2011 and 2014 at ncch or tokyo medical and dental university hospital , tokyo were also studied . 
thus , the total number of uip - positive cases was 54 ( 42 + 12 )  . all patients were diagnosed according to the seventh tnm classification of malignant tumors.21 information regarding age , sex , smoking history , and clinical stage was retrospectively collected . 
 this study was approved by the institutional review boards of both the ncc and tokyo medical and dental university . driver gene aberration screening all 691 cases were screened for egfr , kras , braf , and her2 hotspot mutations by high resolution melting analysis or target sequencing analysis using the ion ampliseq cancer hotspot panel v2 ( life technologies , rockville , md )  . 
 alk , ret , and ros1 fusions were examined by reverse transcriptase polymerase chain reaction ( rt - pcr ) or molecular counting assay as previously described.15 , 22 , 23 wes analysis wes was performed for 245 uip - negative and 51 uip - positive ladcs ( 296 cases in total )  . 
 of these , 211 of the uip - negative cases and all 51 uip - positive cases were selected from the 691 patients with ladc used for driver gene aberration screening on the basis that sufficient amounts of dna were available for comprehensive genomic profiling . 
 wes was performed for cancerous and noncancerous genomic dnas using the sureselect human all exon exome capture kit ( version 4 or 5 ; agilent technologies japan , tokyo , japan ) on the illumina hisequation 2000 platform ( illumina , san diego , ca )  . 
in this condition , 10 randomly chosen snvs and 47 indels were verified at high confidence by mass - spectrometric genotyping on a massarray system ( agena bioscience , san diego , ca ) : 10 of 10 ( 100% ) for snvs and 45 of 47 ( 95.7% ) for indels , respectively ( appendix )  . 
genes recurrently affected by somatic snv and indel mutations in their coding regions were identified by mutsigcv analysis25 according to the following criterion : q value < 0.1 after adjusting for gene length and applying the benjamini - hochberg correction . 
 more detailed information about immunohistochemistry procedures is provided in the appendix . statistical analysis statistical analyses of differences were analyzed by student t test , mann - whitney u test , pearsons 2 test , or fishers exact test . 
for association studies , clinicopathological factors and mutational signatures were coded as binary or ordinal explanatory variables , and association between these signatures and clinical background was analyzed by fishers exact test and logistic regression analysis using the jmp 8.0 software ( sas institute japan , tokyo , japan )  . 
survival analysis was performed using the kaplan - meier method , and groups were compared by log - rank test using the graphpad prism 7 software ( graphpad , la jolla , ca )  . 
this result is consistent with previous reports of patients with uip3 and patients with ladc with uip.11 - 13 baseline characteristics of patients with uip - negative and - positive ladc were similar to those of previously described asian cohorts.16 , 27 , 28 driver oncogene aberrations in uip - negative cases , approximately 50% of which were egfr mutations , were similar to those of overall ladcs in east asians.16 , 28 on the other hand , the prevalence of oncogene aberrations clearly differed between uip - positive and uip - negative cases ( p < .001 by pearsons 2 ; fig 1a ; table 1 )  . 
however , the rate of egfr mutation was markedly lower in uip - positive cases than in uip - negative cases ( 1.9% [ one of 54 ] v 49.9% [ 318 of 637 ] ; p < .001 [ fishers exact test ] ) , even in heavy smokers , who have a low egfr mutation frequency30 ( 25.3% ; 38 of 150 ; p < .001 [ fishers exact test ] )  . 
 ( % ) unless otherwise noted . abbreviations : ladc , lung adenocarcinoma ; uip , usual interstitial pneumonia . * p value was derived from the comparison between the non - uip cohort and uip - ladc by mann - whitney u test , fishers exact test , or pearsons 2 test , as appropriate . invasive mucinous adenocarcinoma and colloid , fetal , and enteric carcinoma were categorized as variants of invasive adenocarcinoma , as in travis et al.29 mutational events underlying carcinogenesis deduced by mutational signatures next , we performed a genome - wide mutational analysis to deduce the mechanisms of mutagenesis during lung carcinogenesis . 
patient characteristics and driver oncogene aberrations of the uip negative cases were similar to those of the 637 uip - negative cases described above ( appendix table a1 )  . 
the median snv rates in uip positive and - negative cases were 1.43 / mb and 0.97 / mb , respectively ( p = .0044 [ mann whitney u test ] ) , whereas the median indel mutation rates in uip - positive and - negative cases were 0.25 / mb and 0.080 / mb , respectively ( p < .001 [ mann - whitney u test ] )  . 
therefore , more mutational events , including indel mutations , occurred in the genomes of uip - positive cancers . among the 296 patients , we observed cosmic signatures 4 ( smoking associated ) , 2 ( apolipoprotein b mrna editing enzyme , catalytic polypeptide - like associated ) , 1 ( age associated ) , and 16 ( unknown etiology ; appendix fig a1 )  . 
uip - negative cases were subcategorized based on smoking status : never smoker , ever smoker , and heavy smoker ( 40 pack - years [ py ] )  . 
these findings indicated that mutational events involved in the development of uip positive ladc are largely caused by smoking . significantly mutated genes in uippositive ladc mutsigcv analysis of all 296 cases revealed frequent mutations in several genes reported in previous genome - wide mutation analysis of ladc14 : egfr , kras , tp53 , stk11 , cdkn2a , ctnnb1 , and smad4 ( appendix table a3 )  . 
mutsigcv analysis of the 51 uip - positive cases revealed that tp53 ( 20 of 51 ; 39.2% ) and kras ( 10 of 51 ; 19.6% ) were the two most frequently mutated genes ( fig 1b ; appendix table a3 )  . 
mutations in other genes reported as mutated in ladc14 were also detected in patients with uip - positive ladc , albeit at lower frequencies than tp53 , kras , and nkx2 - 1 . deleterious pssg mutations in a subset of ladc the above observation prompted us to investigate whether other pssgs are mutated in ladcs . 
we found that four other pssgs , sftpa1 , sftpa2 , sftpb , and sftpc , were mutually exclusively mutated in 10 of 296 ( 3.3% ) of all ladc cases and three of 51 ( 5.9% ) of uip - positive cases ( fig 2a )  . 
most of the mutations in these pssgs were indels in the 3untranslated regions ( utrs ; fig 2b ) , consistent with a recent report that indel mutations occur preferentially in lineage - defining genes in human cancers.32 comparative genotyping of dna and cdna isolated from cancerous and noncancerous tissues revealed that the 3 - utr indel mutant alleles of sftpa1 , sftpa2 , and sftpc were expressed at significantly lower levels than the wild - type alleles ( appendix fig a2 )  . in total , 21 of 296 ladcs ( 7.1% ) had mutations in five pssgs ( nkx2 - 1 , sftpa1 , sftpa2 , sftpb , and sftpc ) , with the mutations in individual genes occurring almost mutually exclusively . 
the prevalence of indels in all cases ( 15 of 296 ; 5.1% ) and uip - positive ladc cases ( six of 51 ; 11.8% ) indicated that pssgs are a major target for indel mutagenesis ( fig 2a )  . pssg mutations define a clinically distinct subset of ladcs next , we examined the characteristics of 21 patients with ladc with pssg mutations ( table 2 )  . 
notably , 11 cases ( 52.3% ) exhibited histology corresponding to mucinous differentiation , 29 with a frequency much higher than in ladcs overall ( 6.1% to 16%29 , 33 , 34 ; appendix table a4 ; representative cases in fig 3a )  . 
most tumors with mutations in nkx2 - 1 and all tumors with mutations in sftpa1 and sftpa2 lost expression of the corresponding proteins , whereas tumors with sftpb mutations retained surfactant protein ( sp ) - b protein expression . 
patients who were uip positive with pssg mutations had shorter median overall survival : 24 months versus 125 months for patients who were uip positive without such mutations ( p = .0080 ; fig 3b )  . 
however , no such association was observed for patients with uip - negative ladc ( appendix fig 3a and 3b )  . discussion we present here the first comprehensive comparative genome profiles , to our knowledge , of ladcs with and without uip . 
 ( % ) unless otherwise noted . abbreviations : ladc , lung adenocarcinoma ; pssg , pulmonary surfactant system gene ; uip , usual interstitial pneumonia . * p value was derived from the comparison between cases with or without pssg mutation by mann - whitney u test , fishers exact test , or pearsons 2 test , as appropriate . invasive mucinous adenocarcinoma and colloid , fetal , and enteric carcinoma were categorized as variants of invasive adenocarcinoma , as in travis et al.29 profiles distinct from those of uip - negative ladcs , characterized by infrequent egfr mutations . 
furthermore , focal genome copy number gain associated with abundant transcript expression is a mode of activation of the egfr oncogene.37 uip - positive ladcs did not exhibit significant copy - number gains at egfr , whereas several uip - positive ladcs did ( appendix fig a4a - a4c )  . 
rna sequencing of representative uip - positive cases did not reveal overexpression of egfr ( appendix fig a4d - a4f ) or oncogenic egfr fusions , which have been reported as driver events in ladc.38 these results suggested that the egfr oncogene infrequently contributes to the development of uip - positive ladc . 
ladcs in east asian individuals frequently harbor egfr mutations , both in smokers and nonsmokers.39 therefore , our findings show that uip affects the molecular mechanism underlying lung carcinogenesis by changing the relative dependence of oncogene aberrations . mutational signature analysis revealed that the mutational events involved in uip - positive ladc are largely due to smoking . 
indel mutations were also frequent in uip - positive ladcs , consistent with their prevalence in smoking associated cancers.31 importantly , our results newly identify pssgs as major targets for indel mutations . 
pssg deficiency had been implicated in lung carcinogenesis on the basis of the association between deleterious germline mutations in these genes and severe familial lung diseases , such as interstitial pneumonia and lung cancer development.7 - 9 noncancerous lung tissues of patients with germline sftpb mutation and sftpc - deficient mice develop interstitial fibrosis and alveolar type ii cell dysplasia , 40 , 41 suggesting that pssg deficiency perturbs normal pneumocytic differentiation . 
 ( a ) pathologic features of pssg - mutated lung adenocarcinoma , including invasive mucinous ( case 12 ) and acinar - predominant with a mucinous cribriform pattern ( case 14 )  . 
nk2 homeobox1 ( nkx2 - 1 ) / thyroid transcription factor 1 ( ttf1 ) and surfactant protein ( sp ) - a were detected in normal pneumocytes but were undetectable in tumors with the corresponding sftpa and / or nkx2 - 1 mutations . 
hematoxylin and eosin staining ( he , upper right ) and immunohistochemistry for nkx2 - 1 / ttf1 ( lower left ) and sp - a ( lower right ) proteins , with 3 , 3 - diaminobenzidine visualization ( magnification 200 )  . 
 ( b ) kaplan - meier curve showing overall survival ( os ) of patients with usual interstitial pneumonia ( uip ) positive ladc with pssg mutation ( mutant ) and without pssg mutation ( wild type )  . 
inflammation contributes not only to tumor development but also to tumor progression , by increasing cell invasion and expanding the fraction of undifferentiated cells.43 , 44 however , pulmonary surfactant proteins play important roles in epithelial integrity and cell differentiation in the lung.7 , 45 therefore , deficiency in pulmonary surfactant protein caused by pssg mutations might increase inf lammation - driven tumor progression by disturbing epithelial integrity / differentiation . 
 pssg mutations were more likely to be present in ladcs of smokers and in egfr mutation negative ladcs , which are both associated with poor prognosis.46 , 47 in addition , the number of cases with pssg mutations was small . 
the roles of aberrations of minor driver oncogenes and pssgs should also be studied in a larger cohort , including patients with squamous cell carcinoma , to more fully elucidate lung carcinogenesis associated with uip . 
the 3 - utrs of genes play regulatory roles in the stability and abundance of mrna , and oncogenic mutations have been reported in the 3 - utrs of kras and tp53 genes.48 , 49 accordingly , functional analysis of the 3 - utr mutations in sftps is warranted . in summary , we elucidated the genomic profile of uip - ladcs and observed a predominance of smoking - related mutations in these cancers . 
 kyohei masai no relationship to disclose hirohiko totsuka employment : stagen noriko motoi honoraria : agilent , msd , novartis , astrazeneca , bristolmyers squibb japan consulting or advisory role : bristol - myers squibb , miraca life sciences , astrazeneca , chugai pharmaceuticals , research funding : roche ( inst ) yoko shimada no relationship to disclose ayaka otsuka no relationship to disclose yae kanai no relationship to disclose kenichi okubo no relationship to disclose shun - ichi watanabe no relationship to disclose masashi kobayashi no relationship to disclose takumi akashi no relationship to disclose sachiyo mimaki no relationship to disclose katsuya tsuchihara no relationship to disclose suenori chiku no relationship to disclose kouya shiraishi no relationship to disclose support references 2005 koji tsuta speakers ' bureau : msd , roche naohiko inase no relationship to disclose takashi kohno research funding : daiichi sankyo , sysmex acknowledgment we thank y . 
sakaguchi for excellent technical assistance with immunohistochemistry . affiliations takayuki honda , kouya shiraishi , yoko shimada , ayaka otsuka , and takashi kohno , national cancer center research institute , chuo - ku ; takayuki honda , hiroyuki sakashita , masashi kobayashi , takumi akashi , kenichi okubo , and naohiko inase , tokyo medical and dental university , bunkyo - ku ; kyohei masai , noriko motoi , and shun - ichi watanabe , national cancer center hospital , chuo - ku ; kyohei masai and yae kanai , keio university school of medicine , sinjuku - ku ; hirohiko totsuka , stagen , taito - ku ; suenori chiku , mizuho information and research institute , chiyoda - ku , tokyo ; sachiyo mimaki and katsuya tsuchihara , epoc , national cancer center , kashiwa , chiba ; and koji tsuta , kansai medical university , hirakata , osaka , japan . supported by the japan agency for medical research and development grant no . 
raghu g , collard hr , egan jj , et al : an official ats / ers / jrs / alat statement : idiopathic pulmonary fibrosis : evidence - based guidelines for diagnosis and management . 
fujimoto d , tomii k , otoshi t , et al : preexisting interstitial lung disease is inversely correlated to tumor epidermal growth factor receptor mutation in patients with lung adenocarcinoma . 
masai k , tsuta k , motoi n , et al : clinicopathological , immunohistochemical , and genetic features of primary lung adenocarcinoma occurring in the setting of usual interstitial pneumonia pattern . 
goldstraw p , crowley j , chansky k , et al : the iaslc lung cancer staging project : proposals for the revision of the tnm stage groupings in the forthcoming ( seventh ) edition of the tnm classification of malignant tumours . 
sunami k , furuta k , tsuta k , et al : multiplex diagnosis of oncogenic fusion and met exon skipping by molecular counting using formalin - fixed paraffin embedded lung adenocarcinoma tissues . 
travis wd , brambilla e , noguchi m , et al : international association for the study of lung cancer / american thoracic society / european respiratory society international multidisciplinary classification of lung adenocarcinoma . 
yatabe y , koga t , mitsudomi t , et al : ck20 expression , cdx2 expression , k - ras mutation , and goblet cell morphology in a subset of lung adenocarcinomas . 
tang x , kadara h , behrens c , et al : abnormalities of the titf - 1 lineage - specific oncogene in nsclc : implications in lung cancer pathogenesis and prognosis . 
hirsch fr , varella - garcia m , bunn pa jr , et al : epidermal growth factor receptor in non - smallcell lung carcinomas : correlation between gene copy number and protein expression and impact on prognosis . 
wallot m , wagenvoort c , demello d , et al : congenital alveolar proteinosis caused by a novel mutation of the surfactant protein b gene and misalignment of lung vessels in consanguineous kindred infants . 
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fujisawa t , iizasa t , saitoh y , et al : smoking before surgery predicts poor long - term survival in patients with stage i non - small - cell lung carcinomas . 
takano t , fukui t , ohe y , et al : egfr mutations predict survival benefit from gefitinib in patients with advanced lung adenocarcinoma : a historical comparison of patients treated before and after gefitinib approval in japan . 
 appendix histologic diagnosis surgically resected specimens ( ie , tissues remaining after snap - frozen tissues were set aside ) were formalin fixed by transbronchial or transpleural injection ( in an inflated state ) , cut serially into 5 - mmthick sections , and macroscopically examined . 
the reads were aligned to the reference human genome ( university of california , santa cruz , human genome 19 ; hg19 ) with the burrows wheeler aligner multi - vision software package . 
because duplicate reads were generated during the polymerase chain reaction ( pcr ) amplification process , duplicated paired - end reads that aligned to the same genomic positions were marked using picard . 
depth of coverage at capture targets in tumor samples was counted using read coverage spanning a target segment with the total number of aligned reads and proportionally calibrated to estimate the copy ratio using depths observed in a panel of normal ( noncancer ) diploid genomes . 
thresholds were as follows : board length cutoff , 0.5 chromosome arms ; confidence interval , 90% . validation of candidate mutations using mass - spectrometric genotyping validation and quantification of candidate mutations were performed by mass - spectrometric ( ms ) genotyping as previously described ( su ky , et al : j clin oncol 30 : 433 - 440 , 2012 ) according to the user instructions for the massarray system ( agena bioscience , san diego , ca )  . 
extracted dna ( 10 ng ) was amplified using specific primers ; unincorporated nucleotides were inactivated by shrimp alkaline phosphatase ; a single - base extension reaction was performed using extension primers that hybridized immediately adjacent to the mutations . 
salts were removed by addition of cation exchange resafter cleanup with spectroclean resin , samples were loaded onto the spectrochip matrix using a nanodispenser and then analyzed by matrix - assisted laser desorption ionizationtime - of - flight mass spectrometry on a bruker autoflex instrument . 
 mutational signature analysis mutational signature in this study was analyzed using nonnegative matrix factorization ( nmf ) , which was applied to the 96 possible substitutions in a trinucleotide context including the bases 5 and 3 of each substitution site , as previously described.17 , 26 nmf was applied to the 96 - substitution pattern using published software from the wellcome trust sanger institute.9 at least 2 , 400 iterations of nmf were run , and each nmf run was iterated to convergence ( 10 , 000 iterations without change ) or until 1 million iterations were performed . 
nmf runs with various numbers of signatures were tested , from one to 10 ; four was best , because signature stability remained high and the reconstruction error converged at a low value ( appendix fig a2a )  . 
 one microgram of total rna was reverse - transcribed using superscript iii first - strand synthesis system for reverse transcriptase ( rt ) pcr ( thermo fisher scientific , waltham , ma ) after dnase treatment . 
ten nanograms of genomic dna and cdna corresponding to 50 ng of rna were prepared from both cancerous and noncancerous tissues . for ms genotyping , the experimental procedures described above were applied to both genomic dna and cdna using the same primer , and mutant allele frequency ( represented as peak heights ) was calculated using the typer4 software ( agena bioscience )  . for fragment analysis , regions including mutations were amplified by pcr from genomic dna and cdna using the same primers according to the manufacturers instructions ( applied biosystems , foster city , ca )  . 
pcrs were performed in triplicate with the following conditions : 35 cycles of denaturation at 95c for 1 minute , annealing at 60c for 1 minute , and extension at 72c for 1 minute . 
mutant allele frequency ( represented as peak heights ) was calculated using the abi genemapper software ( applied biosystems )  . differences in the sftpa1 , sftpa2 , and sftpc gene expression between cancerous and noncancerous tissue were analyzed using quantitative rt - pcr . 
triplicate samples were used for all experiments described in this paragraph . rna sequencing rna - sequencing libraries were prepared from 200 ng of total rna using the truseq rna sample prep kit ( illumina )  . 
the resultant libraries were subjected to paired - end sequencing of 75 - bp reads on a hisequation 2000 ( illumina ) as previously described ( nakaoku t , et al : clin cancer res 20 : 3087 - 3093 , 2014 )  . 
egfr fusion transcripts were identified using the tophat - fusion algorithm ( kim d , et al : genome biol 12 : r72 , 2011 ) .12 expression values were normalized against the corresponding levels of a housekeeping gene ( tbp , encoding tata - binding protein ) .19 immunohistochemistry studies immunohistochemistry studies were performed on 4 - mthick , formalin - fixed , paraffin - embedded tissue sections derived from representative tumor blocks . 
3 , 3 - diaminobenzidine was used as the chromogen , and hematoxylin was used as the counterstareactions that labeled at least 5% of cells were considered positive for thyroid transcription factor 1 ( nuclear )  . 
 ( a ) mass - spectrometric genotyping of genomic dna and cdna from cancerous tissues with sftp - 3 untranslated region ( utr ) indel mutation ( mut ) and noncancerous tissue ( wt )  . 
 ( a ) kaplan - meier curve of overall survival ( os ) for patients with usual interstitial pneumonianegative lung adenocarcinoma with pulmonary surfactant system gene ( pssg ) mutation ( mutant ) and without pssg mutation ( wild type )  . 
 ( a ) copy - number analysis of usual interstitial pneumonia ( uip ) positive lung adenocarcinomas ( ladcs ; n = 51 ) in comparison with uip - negative ladcs ( n = 245 ) ; ( b ) uip - negative ladcs with egfr mutation ( n = 130 ) ; and ( c ) uip - negative ladcs without egfr mutation ( n = 115 )  . 
 ( d ) expression levels of egfr in three uip - positive ladcs in comparison with uip - negative ladcs ( n = 138 ) ; ( e ) uip - negative ladcs with egfr mutation ( n = 35 ) ; and ( f ) uip - negative ladcs without egfr mutation ( n = 103 )  . 
expression levels are shown as fold changes in fragments per kilobase of exon per milllion reads mapped , normalized against the gene encoding tata - binding protein ( tbp )  . 
identification of biomarkers predictive of a benefit from trastuzumab will minimize overtreatment and lower health care costs . methods to identify possible single - gene biomarkers , an exploratory analysis of 3 , 669 gene probes not expected to be expressed in normal breast tissue was conducted . 
 disease - free survival ( dfs ) was used as the end point in a cox regression model , with the interaction term between c8a mrna and treatment as a categorical variable split on the cohort mean . results a significant interaction between c8a mrna and treatment was detected ( p < .001 ) , indicating a predictive response to trastuzumab treatment . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction breast cancer is the leading cause of cancer death among women worldwide.1 it is a heterogeneous disease , so to maximize benefit to the patient by individualizing treatment regimens , clinicians need a sound classification syste clinicopathologic variables , including the estrogen receptor 1 , progesterone receptor , and human epidermal growth factor receptor 2 ( her2 ) , are used to classify tumors as hormone positive , her2 positive ( her2 + ) , or triple negative and to guide treatment decisions . 
pam50 , oncotype dx , and mammaprint were developed using retrospective analysis of mrna gene expression data from breast cancer cohorts . identification of single genes or gene signatures that can be used to classify a breast cancer tumor as a subtype with known treatment strategies can improve outcomes and minimize unnecessary treatment . 
the identification that 15% to 25% of breast cancer tumors overexpress the her2 protein , a transmembrane tyrosine kinase that regulates growth and cell survival , resulted in the development of monoclonal antibody therapy that targets her2 . 
 the exploratory analysis identified c8a , a member of the membrane attack complex and part of the innate immune system , which was prognostic of outcome in the observation arm and predictive of benefit from trastuzumab . 
we also characterized c8a protein expression in stable cancer cell lines . methods study population the hera trial was an international , intergroup , open - label , phase iii randomized study.5 a total of 5 , 102 women with her2 + primary breast cancer ( after a minimum of four courses of standard chemotherapy ) were enrolled and assigned randomly to one of the following three treatment arms : observation ( no trastuzumab ) and 1 or 2 years of adjuvant trastuzumab administered intravenously every 3 weeks . 
an interim analysis5 showed that patients assigned to the 1 - year trastuzumab arm experienced a significantly lower hazard of a dfs event than those in the observation arthis finding resulted in a protocol amendment that allowed for observation patients to selectively crossover to trastuzumab treatment ( 1 or 2 years ) , with the restriction of being alive and disease - free as of may 16 , 2005 . 
the transhera tissue resource consisted of 1 , 203 blocks that originated from 15 countries and were processed at royal marsden hospital in the united kingdo in addition , an extra 600 - m core was taken from each block . 
sample rna was extracted using the expressart ffpe rnaready isolation kit ( amptec , hamburg , germany ) , which is optimized for isolation of total rna specifically from ffpe tissue samples , and eluted into a volume of 20 l . 
the biotinylated cdna is then immobilized to a streptavidin - coated solid support and annealed to a dasl assay pool of gene - specific oligonucleotides for extension and ligation followed by polymerase chain reaction amplification with a biotinylated and a fluorophore - labeled universal primer . 
 control ( liver and brain ) rna samples were included for each processed batch of 48 samples to ensure that rna processing was successful and for quality control and normalization of data between assay batches . 
cubic spline has been shown to combine the positive effects of quantile normalization and to avoid the drawbacks of discontinuous mapping of intensity values and no - rank preservation.11 analysis information from the hera database , with a clinical cutoff date of april 12 , 2012 , and 8 years of median follow - up , was used in the current study.7 the primary end point was dfs , defined as the time from random assignment to first occurrence of any of the following dfs events : recurrence of breast cancer at any site ; the development of ipsilateral or contralateral breast cancer , including ductal carcinoma in situ but not lobular carcinoma in situ ; second nonbreast malignant disease other than basal - cell or squamous - cell carcinoma of the skin or carcinoma in situ of the cervix ; or death as a result of any cause without documentation of a cancer related event . exploratory analysis of possible predictive biomarkers in this exploratory analysis , 3 , 669 gene mrna probes on the illumina humanht - 12 v3 array , which are based on normal breast tissue mrna expression profiles not expected to be expressed in breast tissue , 10 were used to conduct an exploratory analysis of possible predictive biomarkers.1 each probe was used in a cox proportional hazards regression predictive model as a categorical variable bifurcated on the mean of gene mrna expression . 
the list of probes ranked by interaction p value were then used to identify c8a as a gene of interest because it is not normally expressed in breast tissue and is a member of the membrane attack complex and part of the innate immune systea volcano plot of the exploratory analysis is shown in figure 1 . 
exploratory analysis of treatment interaction p value as a categorical variable split on probe mrna expression of 3 , 669 gene probes in the herceptin adjuvant cdna - mediated annealing , selection , extension , and ligation cohort that have zero expected expression in normal breast tissue . 
in the early events analysis , only early disease - defining events were taken into account ( ie , at 2.2 years of median follow - up time ) , when almost no patient had switched from observation to trastuzumab . 
 cox models were adjusted for several clinicopathologic factors : age , pathologic tumor size , progesterone receptor local , estrogen receptor local , tumor grade , menopausal status , nodal status , prior ( neo ) adjuvant chemotherapy , eastern cooperative oncology group performance status , race , and region . 
the weights for the ipw analysis were estimated using a time - varying covariate and the following two baseline covariates : age at study entry and prior ( neo ) adjuvant chemotherapy . 
follow - up time of each eligible patient was divided into 1 - month intervals , and the time - varying covariate was estimated as the within - interval cumulative time of eligibility to cross over . prognostic her2 + gastric cancer cohort we used the publicly available data from the hungarian academy of science ( has ) gastric cancer cohort to further explore c8a as a possible biomarker in her2 + gastric cancer.12 the has gastric cancer cohort is a collection of publicly available cohorts with outcome data profiled on the affymetrix platform ( santa clara , ca )  . 
molecular signature database ( version 4.0 ) gene sets tested included immunologic signatures ( n = 1 , 910 ) , canonical pathways ( n = 1 , 320 ) , molecular gene ontology terms ( n = 1 , 454 ) , microrna ( n = 221 ) , chromosome positions ( n = 326 ) , transcription factors ( n = 615 ) , chemical genetic perturbations ( n = 3 , 402 ) , and oncogenic signatures ( n = 189 )  . c8a mrna normal and cancer tissue expression profile the gtex web portal17 was used to generate a figure for the c8a mrna expression in normal tissues . 
figures that illustrate c8a mrna expression from cancer cell lines were generated using the cancer cell line portal.18 the cancer cell line encyclopedia was used to determine the c8a mrna mean and standard deviation in 1 , 036 cancer cell lines . 
tumor cell lines , hepatocellular carcinoma ( tma809 ) , lung cancer ( dms454 ) , triple negative breast cancer ( mda - 231 ) , her2 normal breast cancer ( mda - 175 ) , and her2 + breast cancer ( sk - br - 3 ) were used for c8a ihc staining . 
 the mrna expression profile suggests that for approximately 70% of the human epidermal growth factor 2positive cohort , c8a mrna was not expressed , and 30% had high expression of c8a mrna . 
kaplan - meier curve for disease - free survival ( dfs ) in the herceptin adjuvant cdna - mediated annealing , selection , extension , and ligation cohort , where the c8a mrna split on the mean represents c8a - low and c8a - high categories . 
the c8a phenotype is illustrated in the gsea histogram shown in figure 4 , with the top 50 genes enriched in the c8a - low group versus the top 50 genes enriched in the c8ahigh group . 
c8a is part of the innate immunity and membrane attack complex and clearly differentiated the enrichment of gene sets associated with immunologic response . c8a mrna expression the c8a mrna on / off expression profile in our analysis cohort suggests that c8a may be expressed in other cancer cell lines . 
on the basis of the results presented in the data supplement , we see that c8a is highly expressed in distinct ovarian , liver , stomach , pancreatic , lung , and hematopoietic / lymphoid cancer types . 
to verify that c8a mrna results in c8a protein expression , c8a antibody was used to stain available cancer cell lines , and the results are the data supplement . discussion identification of single genes or gene signatures that can be used to classify a breast cancer tumor as a subtype with known treatment strategies can improve outcomes and minimize unnecessary treatments . 
 the immune gene list from molecular signature database ( version 4.0 ) on the right represents the top 50 enriched immune genes in c8a - low versus c8ahigh samples and the top 50 enriched immune genes in c8a - high versus c8a - low samples . 
the cancer cell line encyclopedia data show that dms454_lung , ov90_ovary , and snu719_stomach are examples that have high expression of c8a and that c8a is a feature of those immortal cancer cell lines . c8a protein is a critical component of the membrane attack complex that inserts itself into the outer membrane of target cells and anchors the recruitment of c9 proteins to form a pore that leads to cell lysis and death.20 , 21 the membrane attack complex is a component in the complement system , which is part of the innate immune system found in plant and animals and evolved before adaptive immunity.22 the innate immune system can work independently of or be triggered by the adaptive immune system and plays a role in the monitoring of host cells that are damaged or have died and should be cleared.23 the complement system proteins are synthesized by the liver and normally circulate in the blood until stimulated by complement activation . 
molecular characterization of c8a high her2 + tumors may indicate that it is a new cancer phenotype that can escape the immune response and become an important mechanism in cancer that affects survival . 
goldhirsch a , gelber rd , piccart - gebhart mj , et al : 2 years versus 1 year of adjuvant trastuzumab for her2 - positive breast cancer ( hera ) : an open - label , randomised controlled trial . 
skedgel c , rayson d , younis t : is adjuvant trastuzumab a cost - effective therapy for her - 2 / neu - positive t1bn0 breast cancer ? ann oncol 24 : 1834 - 1840 , 2013 10 . 
benita y , cao z , giallourakis c , et al : gene enrichment profiles reveal t - cell development , differentiation , and lineage - specific transcription factors including zbtb25 as a novel nf - at repressor . 
gyrffy b , lanczky a , eklund ac , et al : an online survival analysis tool to rapidly assess the effect of 22 , 277 genes on breast cancer prognosis using microarray data of 1 , 809 patients . 
gyorffy b , lnczky a , szllsi z : implementing an online tool for genome - wide validation of survival - associated biomarkers in ovarian - cancer using microarray data from 1287 patients . 
gyrffy b , benke z , lnczky a , et al : recurrenceonline : an online analysis tool to determine breast cancer recurrence and hormone receptor status using microarray data . 
said ea , dupuy fp , trautmann l , et al : programmed death - 1 - induced interleukin - 10 production by monocytes impairs cd4 + t cell activation during hiv infection . 
 c entrectinib in two pediatric patients with inflammatory myofibroblastic tumors harboring ros1 or alk gene fusions introduction inflammatory myofibroblastic tumor ( imt ) is a rare , indolent spindle cell tumor that typically affects children and young adults.1 , 2 imts occur predominantly in visceral soft tissue and are categorized as an intermediate malignancy because they have a potential for local recurrence but rarely progress to distant metastases.2 , 3 approximately 50% of imts harbor alk rearrangements , although gene fusions involving ros1 , ntrk3 , and pdgfr have also been identified.2 , 4 - 6 previously , the presence of alk gene fusions was typically identified using immunohistochemistry7 ; however , newer techniques such as hybridization capture - based next - generation sequencing ( ngs ) and ngs - based anchored multiplex polymerase chain reaction ( pcr ) testing can now be used to detect gene fusions.8 - 10 identifying patients with actionable gene fusions is important , given the availability of promising therapeutic strategies.2 , 4 surgical resection is the standard of care for patients with a solitary imt , 11 but patients with unresectable or advanced disease have limited treatment options . 
the current national comprehensive cancer network guidelines for soft tissue sarcoma recommend the use of alk inhibitors for patients with alk gene fusions12 ; however , there are no targeted agents approved specifically for use in fusion - positive imts . 
 entrectinib is an investigational , cns - active , potent , and selective inhibitor of trk , ros1 , and alk.8 , 13 , 14 in phase i trials , entrectinib demonstrated clinical efficacy in patients with different tumor types harboring ntrk , ros1 , or alk fusions , regardless of the fusion partner gene.8 a majority of the responses to entrectinib occurred in a rapid and durable manner , and some patients remained on study because they received clinical benefit , even after experiencing disease progression.8 here , we present two patients with fusion positive imts ( dctn1 - alk and tfg - ros1 ) who were enrolled in the ongoing startrk - ng phase i / ib trial ( nct02650401 : study of rxdx 101 in children with recurrent or refractory solid tumors and primary cns tumors , with or without trk , ros1 , or alk fusions ) and treated with entrectinib . 
further molecular testing using a hybrid capture - based targeted exome sequencing assay15 revealed a dctn1 - alk fusion ( fig 1a ) , which determined eligibility to enroll in the startrk - ng trial . 
 ( a ) the dctn1alk rearrangement identified in patient 1 is a deletion that results in the fusion of dctn1 exons 1 - 26 with alk exons 20 - 29 . 
 ( d ) axial t1 postcontrast image shows complete response of the tumor to entrectinib treatment ( no measurable tumor present , red arrow )  . the patient provided informed consent , and entrectinib was started in may 2017 at a dose of 550 mg / m2 taken orally once per day ( 1 cycle was 28 days )  . 
 at the time of this report , she continues daily entrectinib and has no limitations in academic or athletic activities . patient 2 is a 10 - year - old girl who presented with daily high - grade fevers , cough , weight loss , and changes in physical activity over a 2 - month period . 
hybrid capture - based targeted exome sequencing and anchored multiplex pcr as described above15 , 16 identified a tfg - ros1 gene fusion ( fig 2a ) , and she was subsequently enrolled in the startrk - ng trial . the patient provided informed consent and entrectinib was started in may 2017 at a dose of 550 mg / m2 orally once per day . 
in addition , by month 4 of treatment , the residual mass was primarily nonenhancing on contrast - enhancing magnetic resonance imaging , suggesting relative lack of activity ( fig 2b - 2c )  . 
while on treatment , she experienced constipation , mild bloating , nausea , and weight gashe also experienced nighttime urinary incontinence that was potentially related to treatment and improved with simple changes in her nighttime routine . 
both patients exhibited clinically significant responses to the investigational agent entrectinib , which was well tolerated , and the observed adverse effects were consistent with the reported safety profile of entrectinib.8 these cases are in agreement with previous reports demonstrating the clinical efficacy and tolerability of entrectinib in patients with solid tumors harboring ntrk , ros1 , or alk gene fusions , regardless of fusion partner.8 , 17 - 20 entrectinib seems to be well tolerated , as demonstrated in 203 patients treated at the recommended phase ii dose of 600 mg once per day.21 the most common treatment - related adverse events ( traes ) of any grade were dysgeusia ( 38% ) , fatigue ( 29% ) , constipation ( 23% ) , and dizziness ( 23% )  . 
in preclinical studies , entrectinib was a potent inhibitor of trk - driven neuroblastoma , 22 and it has demonstrated clinical activity in a 20 - month - old patient with infantile fibrosarcoma harboring an ntrk fusion.23 the benefit observed in the two patients reported here along with published data on the benefit of entrectinib in trk fusion - positive infantile fibrosarcoma highlight the potential of entrectinib in pediatric tumors harboring trk , ros1 , or alk fusions . 
the startrk - ng trial is currently enrolling pediatric patients with cancer , including primary cns tumors , neuroblastoma , and other non - neuroblastoma extracranial solid tumors harboring gene fusions in ntrk , ros1 , or alk , or harboring alk molecular alterations.23 these cases add to the growing body of evidence that demonstrates the diversity of gene fusion drivers in the formation of imt and underscore the importance of screening patients with imts for ntrk , ros1 , and alk gene fusions by using the best available diagnostic techniques . 
 the gene fusions present in these patients were identified by using a workflow that sequentially uses two different diagnostic platforms : a hybrid capture - based targeted exome sequencing assay ( msk - impact ) and anchored multiplex pcr ( archer fusionplex )  . 
 these cases also highlight the importance of treating patients with imts who harbor trk , ros1 , or alk fusions with drugs , such as entrectinib , that bind and inhibit the kinase domains of these fusion proteins . 
imt is often characterized by the presence of alk rearrangements ; however , additional gene fusions have also been identified in this rare cancer , including ros1 , ntrk3 , and pdgfr , 2 , 4 , 5 including a patient with etv6 - ntrk3 fusion - positive imt who is being considered for treatment with entrectinib.27 in patients with alk fusion positive imt , there have been varying efficacy results reported when patients are treated with alk inhibitors , including crizotinib , ceritinib , and alectinib.28 - 32 in addition , a recent report noted that a patient with imt harboring a tfg - ros1 fusion exhibited a poor response to crizotinib.6 there remains an unmet need in this patient population for safe and effective therapies that can treat patients across a wide range of gene fusion drivers . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . the potential benefit of entrectinib in that it inhibits select targeted kinases with high potency , allowing for the treatment of multiple distinct patient populations with one therapy . we have demonstrated clinically significant improvement in two patients with imts who harbor actionable gene fusions treated with entrectinib in the startrk - ng trial . 
basu no relationship to disclose acknowledgments the authors thank the patients who granted us consent to present their cases for the benefit of the scientific , medical , and patient communities worldwide and nick cianciola , of the lockwood group , for providing medical writing support funded by ignyta . accountable for all aspects of the work : all authors stock and other ownership interests : ignyta affiliations srikanth r . 
basu , memorial sloan kettering cancer center , new york , ny ; and edna chow - maneval , ignyta , san diego , ca . support supported by ignyta ; funded by national institutes of health national cancer institute grant no . 
antonescu cr , suurmeijer aj , zhang l , et al : molecular characterization of inflammatory myofibroblastic tumors with frequent alk and ros1 gene fusions and rare novel ret rearrangement . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multitargeted pan - trk , ros1 , and alk inhibitor entrectinib : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . 
loke bn , lee vkm , sudhanshi j , et al : novel exon - exon breakpoint in cic - dux4 fusion sarcoma identified by anchored multiplex pcr ( archer fusionplex sarcoma panel )  . 
menichincheri m , ardini e , magnaghi p , et al : discovery of entrectinib : a new 3 - aminoindazole as a potent anaplastic lymphoma kinase ( alk ) , c - ros oncogene 1 kinase ( ros1 ) , and pantropomyosin receptor kinases ( pan - trks ) inhibitor . 
ardini e , menichincheri m , banfi p , et al : entrectinib , a pan - trk , ros1 , and alk inhibitor with activity in multiple molecularly defined cancer indications . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
green dc , deharvengt sj , de abreu fb , et al : use of anchored multiplex pcr enrichment for detection of gene fusions in solid tumors by next generation sequencing . 
drilon a , li g , dogan s , et al : what hides behind the masc : clinical response and acquired resistance to entrectinib after etv6 - ntrk3 identification in a mammary analogue secretory carcinoma ( masc )  . 
sartore - bianchi a , ardini e , bosotti r , et al : sensitivity to entrectinib associated with a novel lmna - ntrk1 gene fusion in metastatic colorectal cancer . 
ahn mj , cho bc , siena s , et al : entrectinib in patients with locally advanced or metastatic ros1 fusion - positive non - small cell lung cancer ( nsclc )  . 
rangaraju s , li g , christiansen j , et al : pediatric phase 1 / 1b study of entrectinib in patients with primary brain tumors , neuroblastoma , and ntrk , ros1 , or alk fusions . 
vendrell ja , taviaux s , bganton b , et al : detection of known and novel alk fusion transcripts in lung cancer patients using next - generation sequencing approaches . 
subbiah v , mcmahon c , patel s , et al : stump unstumped : anti - tumor response to anaplastic lymphoma kinase ( alk ) inhibitor based targeted therapy in uterine inflammatory myofibroblastic tumor with myxoid features harboring dctn1 - alk fusion . 
ono a , murakami h , serizawa m , et al : drastic initial response and subsequent response to two alk inhibitors in a patient with a highly aggressive alk - rearranged inflammatory myofibroblastic tumor arising in the pleural cavity . 
mansfield as , murphy sj , harris fr , et al : chromoplectic tpm3 - alk rearrangement in a patient with inflammatory myofibroblastic tumor who responded to ceritinib after progression on crizotinib . 
 large - cell neuroendocrine carcinoma of the lung : a focused analysis of braf alterations and case report of a braf non - v600 mutated tumor responding to targeted therapy purpose in advanced stages , large - cell neuroendocrine carcinoma of the lung ( l - lcnec ) mimics small - cell lung cancer despite its traditional classification as a non small - cell lung cancer . 
here we present a focused analysis of braf mutations in this population . patients and methods comprehensive genomic profiling of tumor tissues was performed from a cohort of 300 patients with biopsy - proven l - lcnec . 
the importance of biomarker - driven therapy is subsequently highlighted with our case of a 69 - year - old man diagnosed with metastatic l - lcnec who did not respond to cisplatin plus etoposide . 
a significant durable response was then demonstrated with therapy targeted toward a braf non - v600e activating mutation ( g469r ) associated with biomarker response identified through circulating cell - free tumor dna analysis . 
giles author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : young kwang chae , md , mph , mba , northwestern medicine developmental therapeutics institute , 645 n . 
the 2015 who classification modified this outline and instead included all lung nets as a single entity , acknowledging that there exist major histologic , epidemiologic , and clinical differences between the carcinoids and high - grade l - lcnec and sclc.3 l - lcnec remains both rare and difficult to treat given the discord between its histologic and clinical characteristics . 
 chemotherapy regimens used for the treatment of sclc should be used ( etoposide and platinum combinations ) , which is reflected in national clinical cancer network ( nccn ) guidelines . 
 in the era of next - generation sequencing ( ngs ) , it is interesting to note that this strategy has yet to be adapted for the category of nonadenocarcinomas and nonsquamous cell carcinomas , which is certainly limiting in our ability to further identify these difficult - to - classify malignancies . 
nccn guidelines only mention ngs for adenocarcinomas . here we summarize the current landscape of l - lcnec and explore in detail the specific genomic alterations pertaining to braf , a member of the serine / threonine kinase raf family , in the largest cohort of patients with l - lcnec . 
 mutations and copy - number gains in the phosphatidylinositol 3 - kinase / akt / mammalian target of rapamycin pathway were detected in 15% of the tumors compared with 17% of sclc tumors.6 in another study using ngs in a cohort of 45 patient cases of l - lcnec , the most commonly altered genes similarly included tp53 ( 78% ) , rb1 ( 38% ) , stk11 ( 33% ) , keap1 ( 31% ) , and kras ( 22% )  . 
l - lcnecs with coaltered rb1 and tp53 ( 40% ) were identified as sclc - like , whereas tumors without this pattern ( 56% ) were identified as nsclc - like . 
as a whole , braf mutations are detected in 2% to 4% of lung cancers and have primarily been identified in adenocarcinomas.8 interestingly , although v600 mutations comprise the majority of braf alterations in melanoma , the v600e mutation is accountable for approximately 50% of braf mutations identified in nsclcs and up to 80% in late stages.8 as recently as late 2015 , the prognostic and biologic implications of braf mutations in nsclc were limited and controversial when evaluating the existing case series . 
subsequent studies were positive for cytokeratin 7 , thyroid transcription - 1 , synaptophysin , and chromogranin , thereby resulting in the diagnosis of metastatic , high - grade neuroendocrine carcinoma ( l - lcnec ) of lung primary ( fig 1 ; appendix ) .11 additional evaluation with brain magnetic resonance imaging and positron emission tomography ct identified a 1.4 - cm nodule in the superior segment of the left lower lobe , likely the site of the primary tumor . 
three months after rt , ct scans showed that the left hemipelvic mass had decreased in size to 3.5 4 cm , with a central area of necrosis ; however , the left lower lobe lung nodule was noted to have grown to 2 cm . ngs of tumor tissue ( foundationone ; foundation medicine , cambridge , ma ) had been performed at diagnosis and revealed mutations in braf ( g469r ) , erbb4 ( a118s ) , stk11 ( l282fs * 3 ) , and tp53 ( r248l ) ; myc amplification was also identified . 
given these molecular findings describing an activating braf mutation , treatment with trametinib ( 2 mg orally once daily ) and dabrafenib ( 150 mg orally twice daily ) was initiated at this time . 
trametinib is a mek inhibitor that prevents raf - dependent mek phosphorylation.8 dabrafenib is a braf serine / threonine kinase inhibitor that has high selectivity for braf v600emutant proteins.8 cell - free dna ( guardant360 ; guardant health , redwood city , ca ) analysis performed at diagnosis demonstrated concordance in detecting mutations in braf ( g469r ) and tp53 ( r248l ) , as well as myc amplification . 
 histology of needle core biopsy : ( c ) hematoxylin stain , 600 ; immunostains for ( d ) prostate - specific antigen , ( e ) cytokeratin 7 , ( f ) chromogranin , ( g ) synaptophysin , ( h ) thyroid transcription - 1 , and ( i ) cdx2 , 600 . expression of the patients braf g469r mutation was demonstrated , from 36.8% at time of diagnosis to nondetectable at both 5 months ( which may also have been in part a result of rt and subsequent tissue necrosis ) and 10 months after initiation of dabrafenib and trametinib ( fig 2 )  . there was an increase in other detectable alterations , which included synonymous mutations in brca1 , arid1a , and smo as well as vuss in apc , pten , fgfr1 , and pik3ca ( figs a1 - a3 )  . 
 presently , a full 15 months since initiating therapy with dabrafenib and trametinib , the patient is continuing with therapy and continues to demonstrate an eastern cooperative oncology group performance status of 0 . 
his latest ct scans ( 18 months after rt and 15 months after initiating targeted therapy ) show no residual pelvic mass and a stable left lower lobe nodule measuring 1.7 cm ( fig 3 )  . 
samples were pulled from an ngs database as part of a deidentified pool with only basic demographic information available ( required for processing the ngs order ) from many institutions . 
an inherent limitation of this pool is that we have to assume the histology of the malignancy was confirmed at each local institution . the atypical variants of braf in l - lcnec are identified as g469a , k601n , and g469r , which are all known to be activating mutations.14 - 17 there also exists g466v , which is an oncogenic kinase - impaired alteration.18 the remainder includes n581i and vus alterations e220k , w210l , g9d , and p149t . 
n581i is a known recurrently somatic braf alteration , but its effect has not been characterized ; otherwise , to our knowledge , these remaining braf mutations have not been previously identified.19 our analysis is summarized in table 1 . discussion current understanding of braf v600 mutations originated in melanoma , where they are the most commonly identified oncogenic mutations and are seen in nearly 50% of cutaneous melanomas.21 braf is an upstream effector of the mitogen - activated protein kinase pathway ( ras / raf / mek / extracellular regulated kinase ) , which plays a central role in cell growth , division , and differentiation . 
ninety percent of braf - mutated melanomas result from a substitution of glutamic acid for valine at codon 600.22 the braf v600e mutations show a 500 - fold increase in catalytic activity compared with the wild type.23 initially , selective braf inhibitors such as vemurafenib and dabrafenib were evaluated as monotherapy in patients with metastatic melanoma harboring either braf v600e or v600k mutations . 
contrast - enhanced computed tomography scans of the ( a , c , e , g ) abdomen and ( b , d , f , h ) chest of the patient ( a , b ) at diagnosis , ( c , d ) approximately 1 month after chemotherapy , ( e , f ) 3 months after radiation therapy ( rt ) directed at the left hemipelvic mass , and ( g , h ) after 15 months of targeted therapy with dabrafenib and trametinib . 
 melanoma , colorectal cancer , or nsclc , investigators concluded that kinase activity is likely to be elevated in 35% of braf mutations , impaired in 15% , and unknown in 10%.18 known nonv600e activating variants of braf that have been identified in patients with nsclc include g464v , g466a , g469a / v / r / s , and k601e . 
 mutations with impaired activity have been reported to be g466r / v , d594a / e / g / h / n / v , and g596c / r.20 interestingly , it has been identified that concomitant kras or nras mutations are more likely occur with the kinase - impaired braf mutants than the kinase - activated braf mutants.18 preclinical data have demonstrated sensitivity to treatment with dabrafenib and trametinib in hek293t cells , lung epithelial cellular models ( beas - 2b ) , and human cancer cell lines harboring non - v600 braf mutations ( both activating and kinase impaired )  . 
this same study also identified that the kinase activity of the g469s variant was comparable to that seen with the braf v600e mutation.20 this further provides a basis for the ongoing exploration of targeted therapy in non - v600 braf - mutant lung cancers . with regard to lung cancer , nccn guidelines for nsclc delineate emerging targeted therapy options for patients with genetic alterations.25 vemurafinib has been studied in multiple nonmelanoma cancers with braf v600 mutations in a basket trial design ( clinicaltrials.gov identifier nct01524978 ) ; in a cohort of 20 patients with nsclc , eight achieved partial responses with targeted braf inhibition.26 in a clinical trial studying dabrafenib plus trametinib in patients with previously treated braf v600emutant metastatic nsclc ( clinicaltrials.gov identifier nct01336634 ) , investigators reported an overall response rate of 63.2% in a cohort of 57 patients.27 this led to the recent approval of dabrafenib with trametinib as a treatment option for patients with advanced or metastatic nsclc with a braf v600 mutation by the us food and drug administration in june 2017.28 interestingly , there is minimal guidance available for non - v600 braf - mutated lung malignancies and even less information specifically focused on sclc or nets . 
remarkably when using ngs ( a broad and sensitive detection tool ) , non - v600e mutations comprise a substantial portion of the braf mutations in different tumors ( nsclc , 86% ; melanoma , 34% ; and colorectal cancer , 23% ) , as assessed in a cohort of more than 800 patients.17 this is a higher proportion of non - v600e braf mutations than identified in earlier retrospective studies with cohorts of 30 to 50 patients . 
in a retrospective study detailing the characteristics of nearly 700 patients with lung adenocarcinoma , braf mutations were present in 3% of patients ( v600e , 50% ; g469a , 39% ; and d594g , 11% )  . 
 interestingly , all of these patients were current or former smokers.29 currently , ngs assays demonstrate the best - known sensitivity and breadth of analysis for the clinical detection of braf mutations including non - v600e alterations.17 in our patient , of course , we must acknowledge the confounding variable of rt directed at the left hemipelvis in the reduction in size of the mass in this location . 
given this , in addition to the steep drop - off seen in braf circulating tumor dna , we suspect that this is a durable response to therapy . it is worth mentioning that cosmic presents information related to adenocarcinoma and squamous cell carcinoma but not l - lcnec . 
this does not reflect the scenario of a real - world stage iv malignancy . although not common , l - lcnec does seem to contain activating and thus actionable alterations as evidenced by our patient 's remaining stable with therapy focused at braf inhibition . 
 in particular , given the scope of non - v600 braf alterations , the basket trial design is ideal for furthering our understanding of the functionality of these various mutations in a histology - agnostic manner . 
the nci - match ( national cancer institute molecular analysis for therapy choice ) trial is currently under way and includes a nonv600 arm in which patients will receive trametinib . 
giles jon chung employment : foundation medicine administrative support : young kwang chae provision of study material or patients : young kwang chae , vincent miller collection and assembly of data : young kwang chae , keerthi b . 
 for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : foundation medicine xiaoqi lin no relationship to disclose vincent miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center siraj m . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome stuff in non - neoplastic disease ( i ) young kwang chae consulting or advisory role : foundation medicine , boehringer ingelheim , biodesix , counsyl , astrazeneca , guardant health speakers bureau : merck , genentech / roche travel , accommodations , expenses : hanmi francis j . 
tamragouri no relationship to disclose consulting or advisory role : novartis travel , accommodations , expenses : medimmune , novartis , foundation medicine affiliations young kwang chae , keerthi b . 
lurie comprehensive cancer center , northwestern university ; xiaoqi lin , northwestern memorial hospital , northwestern university , chicago , il ; and jon chung , vincent miller , and siraj m . 
yao jc , hassan m , phan a , et al : one hundred years after carcinoid : epidemiology of and prognostic factors for neuroendocrine tumors in 35 , 825 cases in the united states . 
travis wd , brambilla e , nicholson ag , et al : the 2015 world health organization classification of lung tumors : impact of genetic , clinical and radiologic advances since the 2004 classification . 
rekhtman n , pietanza mc , hellmann md , et al : next - generation sequencing of pulmonary large cell neuroendocrine carcinoma reveals small cell carcinoma - like and non - small cell carcinoma - like subsets . 
lin x , saad rs , luckasevic tm , et al : diagnostic value of cdx - 2 and ttf - 1 expressions in separating metastatic neuroendocrine neoplasms of unknown orig appl immunohistochem mol morphol 15 : 407 - 414 , 2007 12 . 
noeparast a , teugels e , giron p , et al : non - v600 braf mutations recurrently found in lung cancer predict sensitivity to the combination of trametinib and dabrafenib . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) - mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
 fine - needle aspiration and core - needle biopsy percutaneous fine - needle aspiration ( fna ) and core - needle biopsy ( cnb ) were performed under ultrasound guidance using a 22 - gauge needle for fna and a 20 - gauge core biopsy device for cnb.10 one fna pass was used for localization . 
airdried fna smear was stained with diff - quik stain for on - site evaluation of adequacy and immediate interpretation by a board - certified cytopathologist ( x.l. ) , and alcohol - fixed fna smear was stained with papanicolaou statwo cnb passes were obtained for histologic examination . 
immunohistochemical stains for prostate - specific antigen ( a0562 ; dakocytomation , carpinteria , ca ) , cytokeratin 7 ( ck7 ; a7018 ; dakocytomation ) , chromogranin ( 760 - 2519 ; ventana , tucson , az ) , synaptophysin ( 336a - 76 ; cell marque , rocklin , ca ) , thyroid transcription - 1 ( ttf - 1 ; 343m - 98 ; cell marque ) , and cdx2 ( mu392a - uc ; biogenex , san ramon , ca ) were performed in an automated immunostainer with appropriate positive and negative controls following manufacturers instructions , meaning that positive controls were stained positive and negative controls were stained negative . pathology results fna smears showed loosely cohesive nests or three - dimensional clusters of pleomorphic epithelial cells with focal rosette pattern ( figs a1a and a1b )  . 
the tumor cells were positive for neuroendocrine immunomarkers ( chromogranin and synaptophysin ; fig a1f and a1g ) , ck7 ( fig a1e ) , and ttf - 1 ( a marker for lung adenocarcinoma , lung neuroendocrine neoplasm , 11 and thyroid neoplasm ; fig a1h )  . 
the tumor cells were negative for prostate - specific antigen ( fig a1d ) and cdx2 ( an immunomarker for gi adenocarcinoma and neuroendocrine neoplasm arising from gi tract ; fig a1i ) .11 on the basis of the morphology and immunoprofile , a large - cell neuroendocrine carcinoma diagnosis was rendered . 
the tumor cells were also positive for ttf - 1 and ck7 and negative for cdx2 , suggesting lung origin.11 appendix sample submission time point oct - 16 ( % ) aug - 15 ( % ) pten ( q214 * ) erbb2 ( r143q ) braf ( g469r ) 36.8 mar - 17 ( % ) fig . 
miller , md4 purpose next - generation sequencing ( ngs ) of tumor and germline dna is foundational for precision oncology , with rapidly expanding diagnostic , prognostic , and therapeutic implications . 
although few question the importance of ngs in modern oncology care , the process of gathering primary molecular data , integrating it into electronic health records , and optimally using it as part of a clinical workow remains far from seamless . numerous challenges persist around data standards and interoperability , and clinicians frequently face difculties in managing the growing amount of genomic knowledge required to care for patients and keep up to date . methods this review provides a descriptive analysis of genomic data workows for ngs data in clinical oncology and issues that arise from the inconsistent use of standards for sharing data across systems . 
questions about their provenance and timeliness of updating remapotentially useful standards for sharing genomic data , such as hl7 fhir and mcode , remain primarily in the research and / or development stage . 
2019 by american society of clinical oncology introduction next - generation sequencing ( ngs ) of tumor and inherited ( germline ) genomes has revolutionized and rened cancer treatment during the past two decades and is now vital for evaluating therapeutic opportunities in many solid and hematologic malignancies.1 currently , ngs panels including sets of genes are the most widespread method of rapidly identifying sequence variation in patients with cancer . 
ngs panels provide information for a variety of purposes , cluding diagnostics ( eg , determination of sarcoma subtype ) , hereditary risk assessment ( eg , lynch syndrome ) , prognosis ( eg , kras mutations in lung adenocarcinoma ) , and treatment selection ( eg , biomarkers for immunotherapy responsiveness , such as tumor mutational burden and microsatellite instability ; therapeutic selection for clinically actionable alterations , such as braf v600e in melanoma ; and biomarkers of resistance , such as loss of b2m for immunotherapy ) .2 , 3 as a metric of the signicance of ngs in oncology care , 29 of the 43 national comprehensive cancer network clinical practice guidelines denote specic sequence - based biomarkers important for clinical care ( table 1 )  . 
of these 29 guidelines for treatment of cancer by site , 12 include both somatic and germline biomarkers , 16 include somatic only , and one includes germline only . recently , there has been an increased focus on performing ngs on matched normal samples ( either adjacent tissue or blood ) to compare with tumor biopsies . 
 conway et al context key objective the amount of molecular knowledge required for patient care is exploding , but the minimal adoption of genomic data standards in electronic health records compounds the challenges facing oncologists . 
using examples from asco cancerlinq , this review covers the current status of next - generation sequencing , describes relevant data standards , highlights the pilot of the genomic smart - on - fhir application , and provides a call to action for laboratories and electronic health record vendors to ensure that the chain of data custody for structured genomic content remains unbroken and reaches the clinician . knowledge generated several genomic knowledge bases for variant interpretation are available to support clinicians . 
nonetheless , transmitting nextgeneration sequencing results via pdf hinders the use of decision support tools intended for clinical care , including trial selection , and blocks the downstream reuse of genomic data . relevance the consistent use of evolving standards ( eg , hl7 fhir and mcode ) should improve genomic data interoperability and care quality . 
however , the full integration of genotype and phenotype will require an innovative and socially driven commitment by all oncologic ecosystem participants , beginning with sequencing laboratories , to better leverage technologic solutions . also embedded in guidelines and reimbursement for certain treatments ( eg , poly [ adp - ribose ] polymerase inhibitors for ovarian cancer )  . 
multiple molecularly targeted agents have now been incorporated into standard patient management and reected in numerous guidelines . clinical quality measures the 2019 merit - based incentive payment system ( mips ) of the centers for medicare and medicaid services quality payment program contains 24 general oncology measures , two of which involve genetic testing ( kras and nras in patients with colorectal cancer ) .14 in addition , a number of clinical quality measures in the asco quality oncology practice initiative reference ngs testing , including nonsmall - cell lung cancer ( nsclc ) measures evaluating the use and turnaround time of molecular testing in patients with adenocarcinoma histology.15 as clinical quality measurement evolves from clinicianfocused process measures to more patient - centric outcome measures , it is reasonable to expect that more measures will incorporate results from ngs panels and potentially circulating tumor - free dna testing to foster appropriate diagnostic testing and therapy selection that affect patient outcomes . molecular testing has become essential to oncology care.12 survey data from 2017 showed that more than 75% of oncologists used ngs tests to guide cancer treatment . 
inclusion of genetic testing in nccn cancer site guidelines s , g , b , or n cancer subtype details cancer site acute lymphoblastic leukemia ( adult and aya ) acute lymphoblastic leukemia ( pediatric ) acute myeloid leukemia aids - related kaposi sarcoma anal carcinoma bladder cancer bladder cancer upper tract tumors urothelial carcinoma of the prostate primary carcinoma of the urethra ewing sarcoma family of tumors giant cell tumor of the bone bone chondrosarcoma chordoma osteosarcoma breast cancer cns cancer cervical cancer lymphoma chronic myeloid leukemia colon / rectal cancer colon cancer rectal cancer chronic lymphocytic leukemia / small lymphocytic esophageal and esophagogastric junction cancers gastric cancer gestational trophoblastic neoplasia hairy cell leukemia head and neck cancers hepatobiliary cancers hodgkin lymphoma kidney cancer malignant pleural mesothelioma melanoma cutaneous melanoma uveal melanoma multiple myeloma / other plasma cell neoplasms multiple myeloma systemic light chain amyloidosis waldenstr om macroglobulinemia / lymphoplasmacytic lymphoma myelodysplastic syndromes myeloproliferative neoplasms ( continued on following page ) efciently assess eligibility criteria . 
barriers include insufcient clinician knowledge , training , and condence regarding the use of ngs results.20 , 21 although many clinicians may take laboratorybased interpretations at face value , numerous knowledge bases have been created to aid oncologists and clinical researchers in the curation and interpretation of ngs data . these were developed largely because of the recognition that institutional ( local ) knowledge based on a limited sampling of the cancer population , including that possessed by testing laboratories , would not be sufcient to type , capture the genomic diversity of any cancer common or rare . 
perhaps a surprise to clinicians , many commonly tested genes , such as brca1 and brca2 , show considerable disagreement by interpreting laboratories about the pathogenicity of genetic variants.22 one of the earliest resources to address this issue was mycancergenome , 23 created at vanderbilt university in 2009 . 
since that time , there have been numerous entrants into an increasingly crowded eld , with the most well - known publicly available resources for variant interpretation being civic , 24 oncokb , 25and clinvar , 26 the latter of which is the rst fda - recognized public genetic variant database , housing clingen expert - curated data.27 each of these efforts was developed in relative isolation and with slightly different goals , leading to a divergence of data models , evidentiary models , and user experiences . 
the variant interpretation in cancer consortium , a driver project of the global alliance for genomics and health , 28 was founded with the mission statement to help unify and harmonize the disparate interpretation in cancer data sources . 
inclusion of genetic testing in nccn cancer site guidelines ( continued ) cancer site neuroendocrine and adrenal tumors s , g , b , or n cancer subtype details neuroendocrine tumors of the gi tract , lung , and thymus ( carcinoid tumors ) neuroendocrine tumors of the pancreas adrenal gland tumors pheochromocytoma / paraganglioma men1 men2 non - hodgkins lymphomas chronic lymphocytic leukemia / small lymphocytic lymphoma b - cell lymphomas primary cutaneous b - cell lymphomas t - cell lymphomas nonmelanoma skin cancers basal cell skin cancer dermatobrosarcoma protuberans merkel cell carcinoma squamous cell skin cancer nonsmall - cell lung cancer occult primary ( cancer of unknown primary ) ovarian cancer epithelial ovarian cancer ( including fallopian tube cancer and primary peritoneal cancer ) pancreatic adenocarcinoma penile cancer prostate cancer small - cell lung cancer soft tissue sarcoma systemic mastocytosis testicular cancer thyroid carcinoma uterine neoplasms endometrial carcinoma uterine sarcoma vulvar cancer thymomas and thymic carcinomas note . 
categorization of national comprehensive cancer network ( nccn ) guideline44 by cancer site showing whether the guideline recommends somatic testing ( s ) , germline testing ( g ) , both ( b ) , or neither ( n )  . 
genetic testing refers to short variations , structural sequence variations , cytogenetic analyses , and mismatch repair assays . abbreviations : aya , adolescent or young adult ; men1 , multiple endocrine neoplasia type 1 ; men2 , multiple endocrine neoplasia type 2 . several challenges associated with knowledge bases must be considered . 
although the aforementioned knowledge bases are free to users , they 4 2019 by american society of clinical oncology are generally not integrated into the clinical workow.30 the second is trustworthiness and culpability . 
can the assertions made by knowledge bases be trusted ? if advice is erroneous , the primary responsibility clearly lies with the managing clinician , but can knowledge bases also be held culpable ? furthermore , advice can become outdated ; this must be expected to some degree , given the exponential growth of the eld and the lag between the announcement of trial results , publication of ndings , fda labeling , and revision of variant interpretations ; however , poor recency of data in knowledge bases will diminish trust . 
many knowledge bases spend much effort on attractive so - called skins and search abilities , but the degree to which clinicians nd these interfaces useful has not been extensively studied . technological challenges of data integration : opportunities with fhir and mcode integration of ngs results into the clinical workow via tackle several ehr interfaces must technologic challenges . interpreted genomic results are in particular , generally reported in pdf format , which cannot support electronic search , clinical decision support ( cds ) , or secondary use.31 moreover , the lack of a common data model for genomic testing impedes all use cases by hampering data storage and interoperability between ehr systems and / or data warehouses , thereby hindering the use of cds tools intended to assist clinicians in caring for their patients . these issues have prompted the emergence of initiatives aimed at improving genomic data standards and facilitating genomic data interoperability . 
the top section shows total count of prognostic or predictive assertions related to this gene - variant combination , the breakdown by data source ( ve are shown ) , and the breakdown by assertion type per association for molecular pathology ( amp ) / asco / college of american pathologists ( cap ) guidelines.46 the middle section cross - references drugs and diseases with the gene of interest ( rst column ) , as well as potentially related genes ( adjacent columns ) , which are automatically determined ; heatmap colors indicate the quantity of evidence for a drug - gene or diseasegene correlation . 
the vicc meta - knowledgebase user guide is available online.47 auspices of sync for genes.36 these reports were generated from proprietary pipelines used for the fmi foundationone and foundationact ngs panels . 
although customers typically receive a pdf of the ndings and interpretations , fmi also sends xml les , based on a custom internal standard used to generate the pdfs , upon request . 
these xml les include more detailed information than that presented in the pdf , some of which is for research use only , and can be parsed to generate information relevant for fhir resources and elements ( eg , variant allele fraction , sequencing depth and functional effect for mutations , absolute copy number and copy - number ratio for copy - number events , number of supporting read pairs and identity of both genes involved for rearrangements , and genomic location for all alterations )  . 
briey , clinical elds such as patient , sample , and physician information could be mapped to patient , specimen , and physician fhir resources , respectively . genomic elds such as alterations ( eg , braf p.v600e , amplication , rearrangement ) , therapies , and clinical trials were mapped to elements of the observation genetics resource , with more detailed genetic information ( eg , chromosome , start position , end position , variant allele frequency , coverage , and variant type ) mapped to the molecular sequence resource . 
the entire fmi report was represented as a diagnostic report resource , which included references to the patient , physician , specimen , observation genetics , and molecular sequence resources . 
the modular design ( fig 2 ) was architected with four major goals : assist in clinical interpretation of variants within context , provide links to external resources , facilitate point - of - care physician - patient conversations , and demonstrate that smart - on - fhir technology can be used for a clinicogenomic use case . 
cancerlinq aggregates structured and unstructured data from ehrs and other sources via direct feeds and processes the data in a series of cloud - based databases where it normalized and deidentied for secondary reuse.40 database the cancerlinq database , now representing more than 1.5 million patients , contains vast amounts of detailed longitudinal clinical data , such as demographics , diagnoses , laboratory results , and medications . 
however , a signicant volume of the data is not computable , because many critical concepts ( cancer staging , biomarkers , disease progression , and adverse events ) reside primarily in text notes and other unstructured documents and not in discrete elds . 
smart ( sustainable medical apps , reusable technology ) precision cancer medicine ( pcm ) architecture diagrathe application is designed to be modular and extensible , particularly in the ability to add presentation modules and interfaces to external data sources . 
unique text strings are shown for two well - known egfr gene variations abstracted during curation of unstructured genomic reports that were obtained from electronic health records of practices participating in cancerlinq . 
although natural language processing technology itself has not yet demonstrated sufcient precision or recall to be used as a standalone solution , it has been successfully embedded in the curation workbench used by the data abstractors , where it functions to surface putative data elements from unstructured text that can then be conrmed or disregarded . curation of genomic data from ngs panels in cancerlinq as noted , ngs panels are typically brought into the ehr as pdfs or scanned faxes and therefore are not computable . however , since 2017 , cancerlinq has been extracting high - value genomic information via user interfaceassisted data abstraction . 
cancerlinq has also obtained and processed structured genomic reports in xml format and is evaluating automated processes to scan and extract data from reports with standardized formats . the magnitude of the genomic data gap in native ehrs is considerable and shows how poorly precision oncology is supported . 
similarly , for advanced nsclc , 85.3% of curated patient records had epidermal growth factor receptor tests , but structured epidermal growth factor receptor data were found in native ehrs for only 1.7% of all records for patients with advanced nsclc . it is worth noting that although cancerlinq has developed various technical solutions to structuring genomic data as it is housed in ehrs , all ngs data are originally generated as structured data by molecular diagnostics laboratories . 
the data capture of the various chemistries that underlie ngs sequencing , as well as the components of bioinformatic pipelines ( sequence aligners , variant callers ) and even clinical report production , comprises machine - readable , structured genomic data . 
the technical solutions cancerlinq has painstakingly developed would not be necessary at all if the originally structured data were provided . a stark example of how data quality is diminished when optical character recognition , needed to parse genomic reports , is applied , particularly to scanned images ( eg , faxed reports ) and tables , is listed in table 2 . 
 conway et al of national comprehensive cancer network guidelines as well as payment incentives ( eg , mips ) and quality programs ( eg , quality oncology practice initiative )  . 
clinical trial eligibility in oncology increasingly incorporates genomic biomarkers , and the fda has been modernizing its policies and review processes for cancer , resulting in an avalanche of new agents and approved indications for targeted therapies.41 there is no dearth of cds tools to help translate patient data into quality care , nor is there a lack of technical solutions to transmit , harmonize , curate , store , or otherwise manage data . 
these problems are not primarily technical , and solving them requires a will to action , with social incentives and disincentives . for example , ngs test results that are natively structured are sent to ordering physicians and stored in their ehrs , but in a manner that requires costly and data - lossy curation to restructure back into usable information . 
considering that the genomic results are reimbursed through federal and private insurers , but the reporting format impedes their utility to clinicians , we call for all molecular diagnostic laboratories to provide structured data as part of routine reporting at the request of ordering physicians and their practices . 
this would help laboratories meet the denition of interoperability by the 21st century cures act34 to facilitate health information exchange without special effort on the part of the user while avoiding the act 's prohibition of information blocking . it is notable that on the basis of curated records , structured brca1 or brca2 gene test results are extremely underrepresented among the 10 ehrs used by the more than 50 cancerlinq practices . 
it is possible to integrate genomic and clinical data from apis externally to native ehrs , but greater cooperation is needed from vendors to export clinical data for cds use and to provide a seamless experience for the clinician , whose attention is tethered to the ehr . adoption of data standards , including hl7 fhir and mcode , by all the entities that generate , transmit , and receive health information would also facilitate the implementation of precision oncology . 
the endless customizability of ehrs is at odds with health information technology interoperability and suboptimally supports automated quality measure reporting as required by mips.42 , 43 the dearth of coding for cancer staging , laboratory data , and medications within ehrs could be rectied by adopting widely used standard vocabularies , which would facilitate the computable representation of patients oncology records as envisioned by mcode . 
miller , md , cancerlinq , american society of clinical oncology , 2318 mill rd , suite 800 , alexandria , va 22314 ; e - mail : robert.miller@asco.org. support supported by award no . 
 ngs data challenges and solutions references freedman an , klabunde cn , wiant k , et al : use of next - generation sequencing tests to guide cancer treatment : results from a nationally representative survey of oncologists in the united states . 
mol oncol 8 : 859 - 873 , 2014 kamps r , brando rd , bosch bj , et al : next - generation sequencing in oncology : genetic diagnosis , risk prediction and cancer classication . 
int j mol sci 18 : e308 , 2017 jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
sci transl med 7 : 283ra53 , 2015 cibulskis k , lawrence ms , carter sl , et al : sensitive detection of somatic point mutations in impure and heterogeneous cancer samples . 
nat biotechnol 31 : 213 - 219 , 2013 carter sl , cibulskis k , helman e , et al : absolute quantication of somatic dna alterations in human cancer . 
nat biotechnol 30 : 413 - 421 , 2012 robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . j clin oncol 33 : 3660 - 3667 , 2015 karow j : tumor - only sequencing may misguide therapy but many labs omit matched control . 
may - misguide - therapy - many - labs - omit - matched - control damodaran s , berger mf , roychowdhury s : clinical tumor sequencing : opportunities and challenges for precision cancer medicine . 
saigi m , alburquerque - bejar jj , sanchez - cespedes m : determinants of immunological evasion and immunocheckpoint inhibition response in non - small cell patterns of carcinoma evolution . 
gao p , zhang r , li j : comprehensive elaboration of database resources utilized in next - generation sequencing - based tumor somatic mutation detection . biochim biophys acta rev cancer . 
j clin oncol 32 : 1317 - 1323 , 2014 johnson l - m , valdez jm , quinn ea , et al : integrating next - generation sequencing into pediatric oncology practice : an assessment of physician condence and understanding of clinical genomics . 
lawler m , siu ll , rehm hl , et al : all the worlds a stage : facilitating discovery science and improved cancer care through the global alliance for genomics and 29 . 
hughes ks , ambinder ep , hess gp , et al : identifying health information technology needs of oncologists to facilitate the adoption of genomic medicine : recommendations from the 2016 american society of clinical oncology omics and precision oncology workshop . 
li m , datto m , duncavage e : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
ali , md2 ; luke juckett , ms2 ; funda meric - bernstam , md1 ; and vivek subbiah , md1 introduction one to two percent of nonsmall - cell lung cancers ( nsclcs ) harbor ros1 gene rearrangements.1 - 3 ros1 gene rearrangement leads to constitutive activation receptor tyrosine kinase that activates downstream mitogen - activated protein kinase , phosphoinositide - 3 kinase , signal transducer and transcription 3 , and other pathways activator of leading to oncogenesis.4 because ros1 shares 49% amino acid sequence homology with anaplastic lymphoma kinase ( alk ) in the kinase domain , ros1 rearranged ( ros1 - positive ) nsclc tends to be sensitive to alk inhibitors.5 crizotinib , a mesenchymal epithelial transition factor ( met ) / alk / ros1 tyrosine kinase inhibitor ( tki ) , is the only us food and drug administrationapproved drug for ros1 - positive nsclc.6 ceritinib and brigatinib , second - generation alk inhibitors , have demonstrated activity in crizotinib - nave ros1 - positive nsclc but lacked activity in patients who were crizotinib resistant in anecdotal cases.7 , 8 however , the efcacy of both ceritinib and brigatinib in patients who are crizotinib resistant remains unclear . 
fludeoxyglucose positron emission tomographyct scan after completing four cycles of chemotherapy showed increasing pleural nodularity . comprehensive next - generation sequencing of tumor tissue obtained revealed a cd74 - ros1 rearrangement ( fig 1b )  . 
each of the two cerebellar lesions was treated with gamma knife radiosurgery ( 20 gy to 50% isodose ) , and the patient was enrolled in an anticytotoxic t - cell lymphocyte - 4 antibody ipilimumab and radiation trial ( clinicaltrials . gov identier : nct02239900 )  . 
as per trial protocol , he received external beam radiotherapy to the rll lesion ( 60 gy in 10 fractions ) with concurrent ipilimumab . there was disease progression noted in mediastinal lymph nodes and pleural metastasis while on the aforementioned trial . 
he was then enrolled in the modular phase ii identier : basket signature ( clinicaltrials.gov nct02186821 ) trial with ceritinib for ros1 - aberrant cancers at 750 mg orally daily.11 restaging scans after two cycles and once again after four cycles conrmed a partial response ( pr ; 56% decrease ) per response evaluation criteria in solid tumors ( recist ) 1.1. 
in addition , mri showed reduction in brain metastasis . he continued to have pr while receiving ceritinib for 8 months , until it had to be held for grade 3 elevation in ast and alt . 
 ( a ) the various treatments the patient received for metastatic ros1 - positive nonsmall - cell lung cancer , along with the duration of and best response to each treatment . 
 ( c ) computed tomography and magnetic resonance images of the patients right anterior diaphragmatic lymph node , right lower lobe nodule , and left cerebellar metastases before and at the indicated times after he initiated treatment with brigatinib . 
a radiologic unconrmed partial response by response evaluation criteria in solid tumors 1.1 was achieved after 3 months in the target lesion ( right lower lobe nodule ) , with concurrent response in the right anterior diaphragmatic lymph node and stable cerebellar metastases . cr , complete response ; pd , progressive disease ; pr , partial response ; upr , unconrmed partial response ; sd , stable disease . ceritinib continued to clinically benet the patient , demonstrating both systemic and cns activity for another 17 months . 
eventually , he experienced progression in brain metastases , mediastinal lymph nodes , and rll lesions . plasma cell - free dna ( cfdna ) testing ( guardant panel , guardant health , redwood , ca ) showed notch s2435s , tp53 g245a , and p190t , as well as fbxw7 g477s mutations but no cd74 - ros1 fusions or other ros1 pathway aberrations . 
ct scan of the chest also showed 59% decrease in target lesions by recist 1.1 criteria ( unconrmed pr ) , with decrease in rll lesions and resolution of mediastinal lymphadenopathy ( fig 1c )  . 
however , owing to a signicant decline in performance status ( eastern cooperative oncology group score , 4 ) due to other comorbidities and prolonged hospitalization , he was transitioned to hospice care . discussion to our knowledge , this is the rst report of crizotinibresistant ros1 - positive nsclc responding for an extended period of time ( 25 months ) , to ceritinib9 and subsequently to brigatinib . 
mechanisms of resistance to crizotinib in ros1 - positive nsclc include mutations involving the ros1 kinase domain and activation of bypass signaling pathways.13 - 15 the most common of the ros1 resistance mutations is the g2032r solvent front mutation that causes steric interference to crizotinib binding.15 , 16 the g2032r mutation occurs in close to 50% of crizotinibresistant nsclc.15 in vitro studies have demonstrated that both ceritinib and brigatinib are unable to overcome the common g2032r resistance mutation.12 , 17 various other mutations in the ros1 kinase domain confer resistance to crizotinib.18 - 21 of these , the l2026m gatekeeper mutation maintains sensitivity to ceritinib and brigatinib.12 , 20 brigatinib is a tki that has preclinical activity against ros1.12 in an in vitro kinase inhibitory screen of more than 300 kinases , alk ( half maximal inhibitory concentration [ ic50 ] ; 0 . 6 nm ) was the only kinase inhibited with an ic50 less than 1 viability potently inhibited brigatinib nm . 
another possibility is the re - emergence of the cd74 - ros1 fusion during ipilimumab plus radiation and the subsequent 3 - month treatment hiatus because of lack of selection pressure in the absence of crizotinib , rendering the tumor sensitive to ceritinib . 
however , the lapse between ceritinib and brigatinib therapy was only 12 days , making such a phenomenon less likely . one of the major limitations of this study is the lack of onand post - progression biopsies , which are critical to understanding response and / or resistance mechanisms . these were not performed because the patient declined biopsy , considering advanced age , comorbidities , clinical treatment at progression , and the risk of urgency of pneumothorax . instead , we obtained cfdna testing ( guardant panel ) at disease progression , which was nondiagnostic , either because of ros1 cfdna suppression by ongoing ceritinib treatment or limited sensitivity of cfdna platform in detecting the ros1 fusion . 
although cns activity of brigatinib in ros1 - positive nsclc is not documented , it is likely superior to crizotinib and possibly even ceritinib , given the ndings in alk - rearranged nsclc . 
our patient was refractory to ipilimumab and radiation but responded promptly to subsequent ros1directed therapy , once again highlighting the lack of benet of second - line immune checkpoint monotherapy in patients with certain subsets of oncogene - driven nsclc.27 , 28 several ros1 - directed tkis are being studied in clinical trials ( table 1 )  . 
hong stock and other ownership interests : molecularmatch , oncoresponse , presagia honoraria : adaptimmune , baxter , merrimack pharmaceuticals , bayer consulting or advisory role : alpha insights , axiom , adaptimmune , baxter , bayer , genentech , glg pharma , group h , guidepoint global , innity , janssen pharmaceuticals merrimack , medscape , numab , pzer , seattle genetics , takeda , trieza therapeutics research funding : abbvie , adaptimmune , amgen , astra - zeneca , bayer , bms , daiichi - sankyo , eisai , fate therapeutics , genentech , genmab , ignyta , innity , kite , kyowa , lilly , loxo , merck , medimmune , mirati , mirna , molecular templates , mologen , nci - ctep , novartis , pzer , seattle genetics , takeda travel , accommodations , expenses : loxo oncology , mirna therapeutics siraj m . 
ann oncol 24 : 1822 - 1827 , 2013 yoshida a , kohno t , tsuta k , et al : ros1 - rearranged lung cancer : a clinicopathologic and molecular study of 15 surgical cases . 
am j surg pathol 37 : 554 - 562 , 2013 chin lp , soo ra , soong r , et al : targeting ros1 with anaplastic lymphoma kinase inhibitors : a promising therapeutic strategy for a newly dened molecular subset of non - small - cell lung cancer . 
j thorac oncol 7 : 1625 - 1630 , 2012 ou s - hi , tan j , yen y , et al : ros1 as a druggable receptor tyrosine kinase : lessons learned from inhibiting the alk pathway . 
n engl j med 371 : 1963 - 1971 , 2014 lim sm , kim hr , lee j - s , et al : open - label , multicenter , phase ii study of ceritinib in patients with non - small - cell lung cancer harboring ros1 rearrangement . j clin oncol 35 : 2613 - 2618 , 2017 gettinger sn , bazhenova la , langer cj , et al : activity and safety of brigatinib in alk - rearranged non - small - cell lung cancer and other malignancies : a singlearm , open - label , phase 1 / 2 trial . 
lancet oncol 17 : 1683 - 1696 , 2016 subbiah v , hong ds , meric - bernstam f : clinical activity of ceritinib in ros1 - rearranged non - small cell lung cancer : bench to bedside report . 
zhang s , anjum r , squillace r , et al : the potent alk inhibitor brigatinib ( ap26113 ) overcomes mechanisms of resistance to rstand second - generation alk inhibitors in preclinical models . 
gainor jf , tseng d , yoda s , et al : patterns of metastatic spread and mechanisms of resistance to crizotinib in ros1 - positive non - small - cell lung cancer . 
drilon a , somwar r , wagner jp , et al : a novel crizotinib - resistant solvent - front mutation responsive to cabozantinib therapy in a patient with ros1 - rearranged lung cancer . 
song a , kim tm , kim d - w , et al : molecular changes associated with acquired resistance to crizotinib in ros1 - rearranged non - small cell lung cancer . 
schrock ab , pavlick d , klempner sj , et al : hybrid capture - based genomic proling of circulating tumor dna from patients with advanced cancers of the gastrointestinal tract or anus . 
clark ta , chung jh , kennedy m , et al : analytical validation of a hybrid capture - based next - generation sequencing clinical assay for genomic proling of cell - free circulating tumor dna . 
patil t , smith de , bunn pa , et al : the incidence of brain metastases in stage iv ros1 - rearranged non - small cell lung cancer and rate of central nervous system progression on crizotinib . 
camidge dr , kim d - w , tiseo m , et al : exploratory analysis of brigatinib activity in patients with anaplastic lymphoma kinase - positive nonsmall - cell lung cancer and brain metastases in two clinical trials . 
gainor jf , shaw at , sequist lv , et al : egfr mutations and alk rearrangements are associated with low response rates to pd - 1 pathway blockade in non - small cell lung cancer : a retrospective analysis . 
lee ck , man j , lord s , et al : checkpoint inhibitors in metastatic egfr - mutated non - small cell lung cancer : a meta - analysis . 
zou hy , li q , engstrom ld , et al : pf - 06463922 is a potent and selective next - generation ros1 / alk inhibitor capable of blocking crizotinib - resistant ros1 30 . 
facchinetti f , loriot y , kuo ms , et al : crizotinib - resistant ros1 mutations reveal a predictive kinase inhibitor sensitivity model for ros1and alk - rearranged mutations . 
drilon a , ou si , cho bc , et al : repotrectinib ( tpx - 0005 ) is a next - generation ros1 / trk / alk inhibitor that potently inhibits ros1 / trk / alk solvent - front 32 . 
ardini e , menichincheri m , ban p , et al : entrectinib , a pan - trk , ros1 , and alk inhibitor with activity in multiple molecularly dened cancer indications . 
 enrichment of fgfr3 - tacc3 fusions in patients with bladder cancer who are young , asian , or have never smoked purpose fgfr3 - tacc3 ( fibroblast growth factor receptor 3transforming acidic coiled coil - containing protein 3 ) fusions have recently been identified as driver mutations that lead to the activation of fgfr3 in bladder cancer and other tumor types and are associated with sensitivity to tyrosine kinase inhibitors . 
we examined the clinical and molecular characteristics of patients with fgfr3 - tacc3 fusions and hypothesized that they are enriched in a subset of patients with bladder cancer . materials and methods we correlated somatic fgfr3 - tacc3 fusions with clinical and molecular features in two cohorts of patients with bladder cancer . 
the second cohort consisted of patients with mibc or high - grade nonmibc at the dana - farber cancer institute that had targeted capture sequencing of a selected panel of cancer genes ( n = 356 )  . 
the clinical response of one patient with fgfr3 - tacc3 bladder cancer to an fgfr3 inhibitor was investigated . results overall , 751 patients with high - grade bladder cancer without fgfr3 - tacc3 fusions and 17 with fgfr3 - tacc3 fusions were identified in the pooled analysis of the data sets from the cancer genome atlas and the dana - farber cancer institute . 
 fgfr3 - tacc3 fusions were enriched in patients age 50 years versus age 51 to 65 years versus those older than 65 years ( pooled , p = .002 ) , and were observed in four ( 12% ) of 33 patients age 50 years in the pooled analysis . 
in 2017 , 79 , 030 new cases of bladder cancer are expected to be diagnosed , and approximately 16 , 870 deaths are predicted to occur from the disease in the united states.1 , 2 compared with other cancer subtypes , advances in the management of bladder cancer have been limited in the past three decades , and there is an unmet need to develop novel therapeutic agents that target potentially actionable alterations.3 , 4 genomic alterations in fibroblast growth factor receptors ( fgfrs ) are among the most frequent events during bladder cancer development . 
fgfrs are receptor tyrosine kinases that orchestrate various cellular processes , including cell proliferation , differentiation , and survival.5 fgfr mutations lead to developmental syndromes when present in the germline , and contribute to cancer growth when acquired somatically.6 fgfr fusions with an intact kinase domain have been identified in several cancer amin h . 
consort diagram for 850 patients with bladder cancer . clinical cohort ( n = 850 ) dana - farber cancer institute ( n = 438 ) the cancer genome atlas ( n = 412 ) whole - exome sequencing ( n = 412 ) paired tumor - normal muscle - invasive bladder cancer rna sequencing for structural variant calls assessment of clinical and molecular characteristics in fgfr3 - tacc3positive versus negative bladder tumors institutional targeted next - generation sequencing assay oncopanel ( n = 438 ) computational workflow ( n = 365 ) mutational calling ( mutect ) copy number variations ( viscap - cancer ) breakmer algorithm ( structural variants ) exclusions low - grade nonmuscle invasive histology ( n = 73 ) exclusions low tumor purity ( < 20% ; n = 9 ) final analysis ( n = 356 ) assessment of clinical and molecular characteristics in fgfr3 - tacc3positive versus negative bladder tumors types , including cervical cancer , bladder carcinoma , glioblastoma multiforme , squamous lung carcinoma , and head and neck cancer.7 - 15 fgfr3 , a member of this family , has been reported to be involved in fusions with several genes in bladder carcinoma , including tacc3 ( transforming acidic coiled coil - containing protein 3 )  . 
tacc3 normally is thought to mediate the stabilization and organization of the mitotic spindle during mitosis.14 in the cancer genome atlas ( tcga ) muscle invasive bladder cancer ( mibc ) cohort , in - frame activating fgfr3 - tacc3 fusionsobserved in 10 ( 2.4% ) of 412 patientswere the most common gene fusions identified.7 fgfr3 - tacc3 fusion proteins consist of the immunoglobulin , transmembrane , and tyrosine kinase domains of fgfr3 , fused to the coiled - coil domain of tacc3 . 
through the promotion of dimerization , these fusions lead to a constitutively active fgfr3 kinase protein that has been demonstrated to promote cell proliferation in vivo and in vitro.7 - 9 , 13 phase i and ii trials of fgfr inhibitors have reported promising antitumor activity in patients with fgfr genetic alterations , especially bladder cancer.16 certain genetic alterations , particularly gene fusion events , are enriched in clinical subsets of patients with cancer . 
 patients with mibc and high - grade non - mibc were pooled together in the dfci cohort as there is substantial evidence that the two subtypes are biologically and genomically similar.21 - 23 overall , seven patients with fgfr3 - tacc3 fusions were identified in the dfci cohort using an institutional targeted next - generation sequencing assay24 ( oncopanel )  . 
figure 1 shows the sample inclusion and exclusion criteria and workflow . tissue collection and dna extraction tumor specimens and clinicopathologic information were collected with institutional review board approval at dfci . 
tumor areas that contained at least 20% of tumor cells ( mean tumor purity , 58% ; range , 20% to 100% ) were isolated from normal tissue and chosen for dna extraction . 
dna was quantified by nanodrop and pico - green assays . targeted sequencing two hundred nanograms of genomic dna from each sample was subjected to targeted exon capture and sequencing using oncopanel_v1 to v3 cancer gene panels at brigham and womens hospital ( boston , ma )  . 
the oncopanel gene panel includes capture probes for 275 to 560 cancer - associated genes , as well as intronic portions of 60 genes for rearrangement detection , including fgfr3.24 sample dna was captured using oncopanel_v1 to v3 bait sets using a solution - phase agilent sureselect hybrid capture kit ( agilent technologies , santa clara , ca )  . 
single - nucleotide variants and small indels were analyzed using mutect version 1 0.27200 ( display / cgatools / mutect ; accessed may 2013 ) and annotated by oncotator ( broadinstitute.org / oncotator ; accessed may 2013 )  . 
 copy number alterations were analyzed using a custom r - based tool26 , 27 ( viscap - cancer )  . mean depth of read coverage for the targeted genes was 283 . 
mean , median , and range of percentage of target bases with read depth > 30 was 98% , 99% , and 78% to 99% , respectively . identification of rearrangements and analysis of genomic breakpoints fgfr3 fusion sequences were identified using the breakmer algorithm28 and were manually reviewed using integrated genomic viewer29 to exclude sequencing or alignment artifacts . 
all analyses of sequencing data and mutation and fusion calls were performed blinded to clinical data . clinical response to anti - fgfr3 therapy one patient with fgfr3 - tacc3 mibc received anti - fgfr3 therapy along with docetaxel and the clinical response was monitored . statistical analysis we used fisher 's exact test for categorical data and the wilcoxon rank - sum test for quantitative data . 
 ( % ) , unless otherwise noted . abbreviations : dfci , dana - farber cancer institute ; fgfr3 , fibroblast growth factor receptor 3 ; hg , high grade ; nd , not determined ; nmibc , nonmuscle invasive bladder cancer ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; tcga , the cancer genome atlas . fusion partner fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - lmnb2 fgfr3 - tnip2 fgfr3 - fam184b fgfr3 - jakmip1 fgfr3 4 : 1808826 ; 4 : 1737404 4 : 1808771 ; 4 : 1740268 4 : 1808744 ; 4 : 1740297 4 : 1808806 ; 4 : 1741100 4 : 1808737 ; 4 : 1741297 4 : 1808690 ; 4 : 1741336 4 : 1808937 ; 4 : 1732863 4 : 1808556 ; 19 : 2436887 4 : 1808750 ; 4 : 2752213 4 : 1809003 ; 4 : 17691454 4 : 1808936 ; 4 : 6091989 fig 2 . 
schematic representation of the genomic rearrangements observed in 11 tumor samples that harbor fibroblast growth factor receptor 3 ( fgfr3 ) fusion variants identified using the oncopanel assay in the dana - farber cancer institute cohort . 
fam184b , family with sequence similarity 184 member b ; lmnb2 , lamin b2 ; jakmip1 , janus kinase and microtubule interacting protein 1 ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; tnip2 , tnfaip3 interacting protein 2 . results formalin - fixed , paraffin - embedded tumor specimens were obtained from 438 patients at dfci . 
 we excluded 82 tumors from the analysis because they were of low - grade nonmuscle invasive histology ( n = 73 ) or had low ( < 20% ) tumor purity ( n = 9 )  . 
we mapped the genomic breakpoints of fgfr3 and its corresponding fusion partners that were identified in the dfci cohort , which included four non - tacc3 fusions ( fig 2 )  . 
 ( % ) , unless otherwise noted . abbreviations : dfci , dana - farber cancer institute ; fgfr3 , fibroblast growth factor receptor 3 ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; tcga , the cancer genome atlas . patients age 50 harboring a fusion ( p = .03 ; table 2 )  . 
fgfr3 - tacc3 fusions in tcga were also more frequent in asians ( six [ 14% ] of 44 patients ) compared with other races ( p < .001 ) , as well as in never smokers ( eight [ 7.2% ] of 111 patients ) compared with ever smokers ( p < .001 ; table 2 )  . 
similarly , fgfr3 - tacc3 fusions were more common in dfci patients age 50 years ( one [ 12% ] of eight patients ) compared with other age groups ( p = .001 ; table 2 )  . 
eleven ( 65% ) of 17 patients with fgfr3tacc3 fusions were associated with least one of these three clinical characteristics , and three ( 18% ) of the 17 patients were asian never smokers age 50 years . we next examined whether tumors with fgfr3 - tacc3 fusions had molecular features that distinguished them from other tumors . 
as the oncopanel analysis was performed on tumor samples only , we excluded variants that were observed at any frequency in the exome aggregation consortium database , 30 as they were considered likely germline variants . 
the 17 patients whose tumors harbored fgfr3 - tacc3 fusions were enriched for cdkn1a mutations ( 5 [ 29% ] of 17 v 76 [ 10% ] of 751 ; p = .03 ; table 3 )  . 
conversely , fgfr3 - tacc3 fusion - positive tumors had significantly fewer tp53 mutations ( p = .02 ) , and none had rb1 mutations ( p = .054 ; table 3 )  . 
 somatic copy number alterations were also analyzed in both cohorts using criteria for loss , deletion , gain , and amplification that were developed and applied independently in the two cohorts ( table 3 )  . 
dfci cohort : amplification : log2 ( copy ratio ) > 1.8 , gain : 1.1 log2 ( copy ratio ) < 1.8 ; deletion : log2 ( copy ratio ) < 2 , loss : 2 log2 ( copy ratio ) < 1 . abbreviations : cnv , copy number variation ; dfci , dana - farber cancer institute ; fgfr3 , fibroblast growth factor receptor 3 ; snv , single nucleotide variant ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; mdm2 , murine double minute 2 ; tcga , the cancer genome atlas . mdm2 ( murine double minute 2 ) gain ( p = .04 ) , deletion of pten ( p = .02 ) , and deletion of cdk2na ( p = .0033 ; table 3 )  . as a result of differences in the extent of genome sequencing in the tcga and dfci cohorts , we analyzed the overall mutational burden in each cohort separately . 
in the tcga cohort , the nonsynonymous somatic mutation rate across 18 , 862 genes was significantly higher in patients without fgfr3 - tacc3 fusions compared with those with fusions ( median 224 v 128 ; p = 0.04 ; table 3 )  . 
 in addition , there were no significant differences in the frequency of somatic copy number alterations in either the tcga or dfci cohorts ( table 3 )  . one patient who harbored the fgfr3 - tacc3 fusion in mibc in the dfci cohort was treated with an fgfr3 inhibitor and docetaxel and experienced complete remission for approximately 10 months . discussion our results demonstrate that patients with bladder cancer with fgfr3 - tacc3 fusions have distinct clinical and molecular features compared with the general population of patients with bladder cancer . 
in addition , fgfr3tacc3 fusions were associated with a low frequency of tp53 and rb1 mutations and a higher frequency of cdkn1a mutations , fgfr3 and mdm2 amplifications , and pten deletions . 
 because fgfr3 - tacc3 fusion - positive tumors can be sensitive to fgfr inhibitors , 9 , 31 , 32 these observations suggest that molecular testing to detect fgfr3 - tacc3 fusions in bladder cancer should be prioritized for patients who are young ( age 50 years ) , of asian race , and / or who have never smoked . 
most strikingly , we observed that all patients with bladder cancer who were asian never smokers younger than age 50 years ( n = 3 ) had fgfr3 - tacc3 fusions . we emphasize that our study has significant limitations as a result of the small number of patients with fgfr3 - tacc3 fusions included ( n = 17 ) , which reflects that this is a relatively rare molecular subset of bladder cancer . 
most importantly , we strongly advocate additional studies of this association to extend and confirm these findings . in conclusion , fgfr3 - tacc3 fusion - positive bladder cancer is highly enriched in asians , never smokers , and those age 50 years . 
nassar no relationship to disclose kevin lundgren no relationship to disclose mark pomerantz honoraria : bayer eliezer van allen stock and other ownership interests : synapse , tango therapeutics , genome medical consulting or advisory role : synapse , roche , third rock ventures , takeda , novartis , genome medical , invitae speakers ' bureau : illumina research funding : bristol - myers squibb , novartis lauren harshman consulting or advisory role : medivation , astellas pharma , pfizer , genentech , theragene , kew , corvus pharmaceuticals , merck , exelixis , bayer research funding : medivation , astellas pharma ( inst ) , bayer ( inst ) , sotio ( inst ) , genentech ( inst ) , dendreon ( inst ) , bristol - myers squibb ( inst ) , takeda ( inst ) , merck ( inst ) , janssen oncology ( inst ) , pfizer ( inst ) travel , accommodations , expenses : bayer atish d . 
sonpavde honoraria : uptodate consulting or advisory role : bayer , genentech , sanofi , merck , novartis , pfizer , argos therapeutics , agensys , eisai , astrazeneca , janssen pharmaceuticals , amgen , bristolmyers squibb , exelixis speakers ' bureau : clinical care options , national comprehensive cancer network , physician education resource , onclive , research to practice research funding : onyx pharmaceuticals ( inst ) , bayer ( inst ) , boehringer ingelheim ( inst ) , celgene ( inst ) , merck ( inst ) , pfizer ( inst ) other relationship : boehringer ingelheim , astrazeneca affiliations amin h . 
1p01ca120964 : molecular pathogenesis of the hamartoma syndromes . a directly related abstract was accepted as a poster presentation in the 2018 genitourinary cancer symposium of the american society of oncology , san francisco , ca , february 8 - 10 , 2018 . support prior presentation references 1 . 
acquaviva j , he s , zhang c , et al : fgfr3 translocations in bladder cancer : differential sensitivity to hsp90 inhibition based on drug metabolis mol cancer res 12 : 1042 - 1054 , 2014 4 . 
nogova l , sequist lv , perez garcia jm , et al : evaluation of bgj398 , a fibroblast growth factor receptor 1 - 3 kinase inhibitor , in patients with advanced solid tumors harboring genetic alterations in fibroblast growth factor receptors : results of a global phase i , dose - escalation and dose - expansion study . 
shaw at , yeap by , mino - kenudson m , et al : clinical features and outcome of patients with nonsmall - cell lung cancer who harbor eml4 - alk . 
humphrey pa , moch h , cubilla al , et al : the 2016 who classification of tumours of the urinary system and male genital organs - part b : prostate and bladder tumours . 
balbs - martnez c , sagrera a , carrillo - de - santa - pau e , et al : recurrent inactivation of stag2 in bladder cancer is not associated with aneuploidy . 
lindgren d , frigyesi a , gudjonsson s , et al : combined gene expression and genomic profiling define two intrinsic molecular subtypes of urothelial carcinoma and gene signatures for molecular grading and outcome . 
garcia ep , minkovsky a , jia y , et al : validation of oncopanel : a targeted next - generation sequencing assay for the detection of somatic variants in cancer . 
tabernero j , bahleda r , dienstmann r , et al : phase i dose - escalation study of jnj - 42756493 , an oral pan - fibroblast growth factor receptor inhibitor , in patients with advanced solid tumors . 
in cohort b , the orr and disease control rate were 75% and 75% . conclusion capmatinib in combination with erlotinib demonstrated safety proles consistent with prior studies . we observed efcacy in specic patient populations . 
early studies evaluated onartuzumab ( an anti - met monoclonal antibody ) in combination the phase iii with erlotinib in recurrent nsclc.16 , 17 in the phase ii study , patients with met 2 + or 3 + by immunohistochemistry ( ihc ) demonstrated a signicant improvement in survival end points compared with low met expression . 
despite this , trial was negative.18 tivantinib , a non - atp competitive small molecule met inhibitor , was evaluated in combination with erlotinib in a phase ii trial of unselected pretreated patients . 
the combination did not meet its overall efcacy goal ; however , a planned subset analysis showed a trend toward prolonged progression - free survival ( pfs ) in patients with met amplication.19 this lack of efcacy may be due to the lack of specicity of tivantinib for the met pathway compared with other met inhibitors.20 capmatinib ( inc280 ) is a highly potent and selective oral met inhibitor that has recently been approved for the treatment of tumors with met exon 14 mutations.21 in the phase i study , antitumor activity was observed in pretreated patients with egfr wild - type ( wt ) tumors with met dysregulation . 
because of overlapping signaling pathways , we sought to determine whether the combination of capmatinib with erlotinib would be safe and demonstrate an efcacy signal in patients with egfror metaltered tumors . knowledge generated we demonstrated that the combination of capmatinib and erlotinib is safe . 
however , it restored sensitivity to erlotinib and promoted apoptosis in nsclc models rendered erlotinib resistant by hgf.23 on the basis of the data available during trial development , we propose that the combination of capmatinib plus erlotinib would be safe and show efcacy in patients with egfr - mutated tumors experiencing disease progression on erlotinib due to met activating bypass pathways . 
the initial phase of the study was a dose escalation to determine the maximum tolerated dose ( mtd ) of capmatinib plus erlotinib ; there was no intrapatient dose escalation . 
patients in cohort a must have an egfr activating mutation and a biopsy at the time of progression that shows evidence of met positivity . treatment capmatinib capsules were administered orally every 12 hours of a 28 - day cycle at 100 - 600 mg . 
a dose - limiting toxicity ( dlt ) was dened as per the study protocol ( data supplement )  . pk blood samples were collected for patients in the doseescalation cohort on cycle 1 , day 15 ; cycle 2 , days 1 and 15 ; and cycles 3 and 4 , day 1 . 
analysis of hgf levels was conducted in duplicate by enzyme - linked immunosorbent assay ( r&d systems , minneapolis , mn ; cat dhg00 ) as per the manufacturers instructions . statistical methods all patients who had at least one dose of study therapy were included in the analyses . 
twelve and ve patients were enrolled in cohorts a and b , respectively ( fig 1 )  . patient demographics and disease characteristics patient demographics and disease characteristics are listed in table 1 . 
in the doseescalation cohort and cohort a , 67% ( patients 1 and 313 ) and 92% ( all except patient 29 ) had prior treatment with at least one egfr tki . 
swimmers plot demonstrating the cohort , met , and epidermal growth factor receptor ( egfr ) status of each patient and corresponding response status and progression - free survival of each patient . 
patient 30 was found to have an egfr t790m mutation on a biopsy sample taken after egfr tyrosine kinase inhibitor ( tki ) treatment ; however , on immediate pretreatment biopsy this mutation was not detected . 
a waterfall plot of best response for all evaluable patients is shown in figure 3 . the aes that were possibly , probably , or denitely attributed to the study drugs are shown in table 2 for all dose levels . 
the most common aes of any grade were acneiform rash ( 62.9% ) , fatigue ( 51% ) , nausea ( 45.7% ) , diarrhea , lower extremity edema , vomiting , and hypoalbuminemia ( 37% each )  . 
in patients who received the recommended phase ii dose ( rp2d ) , the most common aes were acneiform rash ( 65% ) , fatigue and nausea ( both 60% ) , vomiting ( 55% ) , and hypoalbuminemia and edema ( both 50% ) ; additional aes are detailed in appendix table a1 . there were no grade 5 toxicities related to the drug combination . dlt and mtd in dose level 5 , one patient developed grade 3 neutropenia possibly related to treatment . 
dose level 6 served as the expansion of dose level 5 , given that 600 - mg capsules were previously shown to be pharmacokinetically equivalent to 400 - mg tablets . 
six patients received dose modications of capmatinib due to nausea ( 2 ) , alt abnormalities ( 1 ) , edema ( 1 ) , low neutrophil count ( 1 ) , and elevated amylase ( 1 )  . 
five patients received dose modications of erlotinib due to paronychia ( 2 ) , acneiform rash ( 1 ) , creatinine increase ( 1 ) , and diarrhea ( 1 )  . 
four patients received dose modications of both drugs for lipase elevation ( 1 ) , creatinine increase ( 1 ) , lymphopenia ( 1 ) , and lung inammation / pneumonitis ( 1 )  . the pk properties of erlotinib and capmatinib were examined during dose escalation on cycle 1 , day 15 at multiple time points after drug administration . 
the same 400mg dose of capmatinib in the tablet formulation demonstrates a higher drug exposure with greater variation ( appendix table a2 ) compared with the capsule formulation , 182 2021 by american society of clinical oncology although it was not statistically signicant . in addition , erlotinib showed a dose - dependent change of systemic drug exposure ( 150 mg v 100 mg ; appendix fig a1b and appendix table a2 ) ; coadministration with capmatinib did not have signicant impact on erlotinib pk ( appendix table a2 )  . 
overall , the range of erlotinib exposures during dose escalation was similar to previously published results.28 efcacy across all evaluable patients , the orr was 31% ( 8 / 26 ; fig 3 )  . 
among patients with pr or cr , the responses were prolonged , from patient 24 , who discontinued study after apart 3 months because of pneumonia / pneumonitis ; vestigators could not rule out possible drug - related pneumonitis , and thus the patient was discontinued from study . two responders were treatment nave ( 20 and 24 ) ; the remainder had at least one prior regimen ( table 1 )  . dose - escalation cohort fifteen of the 18 patients in the dose - escalation cohort were evaluable . 
two patients ( patients 21 and 23 ) withdrew from the study by individual choice , one patient ( patient 33 ) developed new brain metastasis and withdrew , and one patient ( patient 30 ) had a prolonged hospitalization for a cerebrovascular event deemed unrelated to study drugs . 
efcacy data across dose - escalation cohort dose level median cycles ( range ) 2 ( 2 - 4 ) 5 ( 4 - 16 ) 2 ( 1 - 7 ) 2 ( 2 - 8 ) 4 ( 1 - 10 ) 4 ( 4 - 29 ) inc280 , mg twice a day erlotinib , mg once daily evaluable patients complete response partial response stable disease progressive disease overall response rate abbreviation : inc280 , capmatinib . 1 ( 33% ) 3 ( 100% ) disease control rate 2 ( 67% ) 2 ( 67% ) 1 ( 33% ) 2 ( 67% ) 1 ( 33% ) five egfr - wt patients were enrolled in cohort b ; one patient ( patient 25 ) was not evaluable because of death during cycle 1 deemed unrelated to the study drugs . 
efcacy data across dose - expansion cohorts dosing and response groups cohort a median cycles ( range ) 2 ( 1 - 33 ) 3 ( 1 - 45 ) inc280 , mg twice daily erlotinib , mg once daily evaluable patients complete response partial response stable disease progressive disease overall response rate , % disease control rate , % cohort b abbreviations : inc280 , capmatinib ; ne , not evaluable . at the recommended phase ii dosing , responses were seen in patients with met amplication by ngs and / or 3 + ihc expression and those with met exon 14 mutations , but not in patients with 2 + ihc expression . 
a study in chinese patients with getinib plus capmatinib also reported that 2 + ihc expression was not predictive of response unless it was accompanied by a gene copy number of 5.29 the met / cen7 ratios were not fully reported in this study , but a ratio  . 
serial blood hgf levels were measured to evaluate baseline levels and treatment - related changes in patients over time ; however , no overt correlations with baseline hgf levels and treatment outcomes were observed ( data not shown )  . the patient population with the greatest potential to benet from the combination treatment was cohort a , which enrolled egfr - positive patients who had experienced progression on egfr tkis . 
additional evaluation of an egfr - tki plus a met - tki to overcome this common resistance mechanism is warranted . affiliations 1helen diller family comprehensive cancer center , university of california , san francisco , ca 2university of california davis comprehensive cancer center , sacramento , ca 3mount sinai tisch cancer institute , new york , ny subject matter of this manuscript . 
mccoach honoraria : novartis , genentech , guardant health consulting or advisory role : astrazeneca speakers bureau : novartis research funding : novartis , revolution medicine travel , accommodations , expenses : loxo , eli lilly , takeda pharmaceuticals aiming yu stock and other ownership interests : johnson & johnson patents , royalties , other intellectual property : patents : ( 1 ) yu am , wang wp , chen qx , li mm . 
gandara honoraria : astrazeneca consulting or advisory role : astrazeneca ( i ) , guardant health ( i ) , oncocyte ( i ) , amgen , io biotech ( i ) , merck , roche / genentech , boehringer ingelheim , inivata , novartis research funding : roche / genentech ( i ) , merck ( i ) , amgen ( i ) travel , accommodations , expenses : boehringer ingelheim jonathan w . 
lara consulting or advisory role : janssen research funding : aragon pharmaceuticals ( i ) , janssen biotech ( i ) , tracon pharma ( i ) , merck ( i ) , pharmacyclics ( i ) , incyte ( i ) , taiho pharmaceutical ( i ) matthew gubens consulting or advisory role : bristol myers squibb , roche / genentech , astrazeneca , heron , boehringer ingelheim , takeda pharmaceuticals , beyondspring pharmaceuticals , inivata research funding : celgene ( i ) , merck ( i ) , novartis ( i ) , roche / genentech ( i ) , oncomed ( i ) philip c . 
mack honoraria : guardant health consulting or advisory role : astrazeneca , guardant health , amgen research funding : boehringer ingelheim consulting or advisory role : roche / genentech , regeneron , abbvie , emd serono , merck , pzer , astrazeneca , novartis , symphogen , inivata , bristol myers squibb , takeda pharmaceuticals , eli lilly , amgen , genmab , targeted oncology , genentech research funding : emd serono ( i ) , genentech ( i ) , abbvie ( i ) , five prime therapeutics ( i ) , regeneron ( i ) , astellas pharma ( i ) , tizona therapeutics , ( i ) eli lilly ( i ) , novartis ( i ) , amgen ( i ) patents , royalties , other intellectual property : author royalties for uptodate , an evidence - based , peer - reviewed information resource , available via the web , desktop , and pda travel , accommodations , expenses : astrazeneca , roche / genentech , merck , regeneron , eli lilly , abbvie , emd serono no potential conicts of interest were reported . acknowledgment we thank patients and their families for participation in this study . karen kelly honoraria : merck references finocchiaro g , toschi l , gianoncelli l , et al : prognostic and predictive value of met deregulation in non - small cell lung cancer . 
ann transl med 3 : 83 , 2015 go h , jeon yk , park hj , et al : high met gene copy number leads to shorter survival in patients with non - small cell lung cancer . 
j thorac oncol 5 : 305 - 313 , 2010 dimou a , non l , chae yk , et al : met gene copy number predicts worse overall survival in patients with non - small cell lung cancer ( nsclc ) ; a systematic review and meta - analysis . 
plos one 9 : e107677 , 2014 tong jh , yeung sf , chan aw , et al : met amplication and exon 14 splice site mutation dene unique molecular subgroups of non - small cell lung carcinoma with poor prognosis . 
clin cancer res 22 : 3048 - 3056 , 2016 gherardi e , birchmeier w , birchmeier c , et al : targeting met in cancer : rationale and progress . 
nat rev cancer 12 : 89 - 103 , 2012 [ erratum : nat rev cancer 12 : 637 , 2012 ] engelman ja , zejnullahu k , mitsudomi t , et al : met amplication leads to getinib resistance in lung cancer by activating erbb3 signaling . 
science 316 : 1039 - 1043 , 2007 bean j , brennan c , shih jy , et al : met amplication occurs with or without t790m mutations in egfr mutant lung tumors with acquired resistance to getinib or erlotinib . 
proc natl acad sci usa 104 : 20932 - 20937 , 2007 cappuzzo f , j anne pa , skokan m , et al : met increased gene copy number and primary resistance to getinib therapy in non - small - cell lung cancer patients . ann oncol 20 : 298 - 304 , 2009 piotrowska z , thress ks , mooradian m , et al : met amplication ( amp ) as a resistance mechanism to osimertinib . 
le x , puri s , negrao mv , et al : landscape of egfr - dependent and - independent resistance mechanisms to osimertinib and continuation therapy beyond progression in egfr - mutant nsclc . 
drilon a , cappuzzo f , ou si , et al : targeting met in lung cancer : will expectations nally be met ? j thorac oncol 12 : 15 - 26 , 2017 15 . 
spigel dr , ervin tj , ramlau ra , et al : randomized phase ii trial of onartuzumab in combination with erlotinib in patients with advanced non - small - cell lung 18 . 
spigel dr , edelman mj , obyrne k , et al : results from the phase iii randomized trial of onartuzumab plus erlotinib versus erlotinib in previously treated stage iiib or iv non - small - cell lung cancer : metlung . 
sequist lv , von pawel j , garmey eg , et al : randomized phase ii study of erlotinib plus tivantinib versus erlotinib plus placebo in previously treated non - smallcell lung cancer . 
calles a , kwiatkowski n , cammarata bk , et al : tivantinib ( arq 197 ) efcacy is independent of met inhibition in non - small - cell lung cancer cell lines . 
liu x , wang q , yang g , et al : a novel kinase inhibitor , incb28060 , blocks c - met - dependent signaling , neoplastic activities , and cross - talk with egfr and her22 . 
bang y - j , su w - c , nam d - h , et al : phase i study of the safety and efcacy of inc280 in patients with advanced met - dependent solid tumors . 
lara ms , holland ws , chinn d , et al : preclinical evaluation of met inhibitor inc - 280 with or without the epidermal growth factor receptor inhibitor erlotinib in non - small - cell lung cancer . 
paik pk , drilon a , fan pd , et al : correction : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
cancer discov 5 : 842 - 849 , 2015 jorge se , schulman s , freed ja , et al : responses to the multitargeted met / alk / ros1 inhibitor crizotinib and co - occurring mutations in lung adenocarcinomas with met amplication or met exon 14 skipping mutation . 
fukudo m , ikemi y , togashi y , et al : population pharmacokinetics / pharmacodynamics of erlotinib and pharmacogenomic analysis of plasma and cerebrospinal uid drug concentrations in japanese patients with non - small cell lung cancer . 
wu yl , zhang l , kim dw , et al : phase ib / ii study of capmatinib ( inc280 ) plus getinib after failure of epidermal growth factor receptor ( egfr ) inhibitor therapy in patients with egfr - mutated , met factor - dysregulated non - small - cell lung cancer . 
wolf j , overbeck tr , han j , et al : capmatinib in patients with high - level met - amplied advanced nonsmall cell lung cancer ( nsclc ) : results from the phase 2 geometry mono - 1 study . 
camidge dr , otterson ga , clark jw , et al : crizotinib in patients ( pts ) with met - amplied non - small cell lung cancer ( nsclc ) : updated safety and efcacy ndings from a phase 1 trial . 
caparica r , yen ct , coudry r , et al : responses to crizotinib can occur in high - level met - amplied non - small cell lung cancer independent of met exon 14 33 . 
wolf j , seto t , han j , et al : results of the geometry mono - 1 phase ii study for evaluation of the met inhibitor capmatinib ( inc280 ) in patients with metex14 mutated advanced non - small cell lung cancer . 
yu h , ahn m , kim s , et al : ct032 tatton phase ib expansion cohort : osimertinib plus savolitinib for patients ( pts ) with egfr - mutant , met - amplied nsclc after progression on prior rst / second - generation epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitor ( tki )  . 
sequist l , lee js , han j , et al : ct033 tatton phase ib expansion cohort : osimertinib plus savolitinib for patients ( pts ) with egfr - mutant , met - amplied nsclc after progression on prior third - generation epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitor ( tki )  . 
treatment - related adverse events by cohort and dose level ( continued ) dose level 1 dose level 2 dose level 3 dose level 4 dose level 5 dose level 6 expansion adverse event gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 gr 1 / 2 gr 3 total gastroesophageal reux disease oral mucositis hyponatremia stroke proteinuria back pain peripheral sensory neuropathy abbreviations : gr , grade ; inr , international normalized ratio ; sae , signicant adverse event . 
 r fundamental concepts in the application of plasma genotyping ( liquid biopsy ) to egfr mutation detection in nonsmall - cell lung cancer plasma genotyping has rapidly evolved from an investigational technology into a standard - of - care tool used to direct therapy in metastatic nonsmall - cell lung cancer ( nsclc )  . 
the optimal use and interpretation of plasma genotyping requires understanding of cell - free dna biology , the assay characteristics of the available testing technologies , and the application of testing in each clinical scenario . 
 current recommendations for plasma genotyping in metastatic nsclc are limited to patients with newly diagnosed disease and those with acquired resistance to targeted therapy , in particular , epidermal growth factor receptor ( egfr ) kinase inhibitors . 
in newly diagnosed metastatic nsclc , under certain circumstances , plasma genotyping is useful for the detection of targetable genomic alterations or nontargetable driver alterations ( eg , kras ) that are mutually exclusive with targetable alterations . 
in patients with acquired resistance to therapy , such as egfr t790m - mediated acquired resistance to egfr kinase inhibitors , plasma genotyping may detect resistance mutations missed by standard tissue genotyping because of tumor heterogeneity . 
in both scenarios , the high specificity and positive predictive value of validated plasma genotyping assays allow for the reliable selection of therapy on the basis of a positive plasma genotyping result . 
this technology has become commonplace in prenatal research as well as cancer diagnostics and biomarker research.1 - 6 liquid biopsy has emerged as the colloquial term for the specific use of cfdna genotyping analysis to interrogate plasma , urine , and csf.7 , 8 this technology has been piloted in multiple solid tumor types to detect specific genomic alterations.2 , 4 , 5 its potential utility has been best demonstrated in lung cancer , where the rapid detection of targetable genomic alterations is key to selecting optimal systemic therapy.9 , 10 liquid biopsy technology has inarguably entered the realm of standard care in the treatment of nonsmall - cell lung cancer ( nsclc ) .11 , 12 multiple platforms for performing liquid biopsy have been evaluated for the detection of targetable genomic alterations in metastatic nsclc.9 , 10 , 12 - 20 the most rigorous of these studies have used either prospective sample testing or batched testing of samples collected from prospective clinical trials compared with standard tissue genotyping . 
 ( fda ) approval of a liquid biopsy assay using the cobas epidermal growth factor receptor ( egfr ) mutation test v2 ( roche molecular systems ) platform for the detection of egfr exon 19 del / l858r mutations as well as the egfr t790m resistance mutation constitutes the best example of the rapid transition of this technology from a research assay to a tool for guiding clinical care.21 furthermore , the commercial availability of multiple liquid biopsy assays for the detection of increasingly large panels of genomic alterations underscores the growing clinical role of this technology.22 , 23 the reliability , interpretation , and optimal use of liquid biopsy technology in lung cancer are potentially confusing , given the long history of the field and the number of testing platforms available . 
this hypotheses was confirmed by the detection of known mutations from a patients tumor in cfdna isolated from matched patient plasma.31 tumor - derived cfdna constitutes only a minor and potentially variable fraction of cfdna in a patient with an active malignancy , with the majority of the cfdna originating from normal tissue and blood cells.1 , 30 , 32 the careful isolation of cfdna from plasma as opposed to serum can potentially limit additional contamination with nontumor dna derived from the lysis of white blood cells during specimen processing.33 technical aspects of cfdna isolation , including prompt plasma processing and the use of dna - preservation tubes , may also reduce contamination with nontumor dna ( see specimen type and handling section ) .34 however , the relatively low frequency of tumor - derived cfdna present in the blood as well the short fragment length historically constituted key technical barriers to the reliable detection of tumor genomic alterations in cfdna . the advent of highly sensitive genotyping technologies now allows for the reliable genotyping of the tumor - derived component of plasma cfdna . 
a variety of highly sensitive validated platforms can detect specific genomic alterations in the small fraction of plasma cfdna that is derived from tumor cells ( see technology section ) .9 , 10 , 12 - 20 however , the fundamental limitation of any highly sensitive plasma genotyping assay is the degree to which a given tumor sheds cfdna into the peripheral circulation . 
the determinants of tumor cfdna shed are incompletely understood at present but are hypothesized to relate to both tumor burden and site of disease with tumor characteristics , which include histology , mitotic rate , and tumor vascularization.27 , 28 , 30 , 35 in studies of quantitative plasma genotyping of patients with metastatic nsclc , increasing disease burden , as measured by an increase in metastatic sites , as well as the presence of bone or liver metastases correlate with the concentration of tumor - derived cfdna.35 in all cases , the fraction of tumor - derived cfdna relative to total cfdna , and thus the degree of tumor cfdna shed , must be inferred from the detection of mutant cfdna relative to wild - type cfdna at a given genetic locus . 
the distinction between a shedding and nonshedding tumor is key to the understanding and interpretation of the results of any plasma genotyping assay in nsclc . technology the development of highly sensitive genotyping platforms propelled the analysis of the tumor - derived portion of cfdna from a laboratory curiosity to a potentially reliable clinical tool . 
however , both the presence and rate of cfdna shed vary among patients and directly affect the diagnostic sensitivity of plasma genotyping assays , which can contribute to false - negative results with these assays . circulating cell - free normal dna circulating tumor dna bloodstream normal tissue metastatic nsclc . 
however , the ability of individual plasma genotyping assays to detect specific types of genomic alterations is highly dependent on the testing platform , with the identification of complex rearrangements and copy number alterations being more difficult than the detection of point mutations . 
 analytical sensitivity and specificity refer to the technical ability of a genotyping assay to detect low levels of a given genomic alteration and distinguish it from other alterationsa metric that is most relevant for the development of laboratory tests and procedures . 
this review focuses primarily on clinical diagnostic sensitivity and specificity , which refer to the ability of an assay to accurately identify patients who have or do not have a given genomic alteration compared with a reference standardthe key criteria for using a test for making treatment decisions . cobas egfr mutation test and polymerase chain reactionbased approaches the cobas egfr mutation test is a real - time polymerase chain reaction ( pcr ) based assay originally developed for the purpose of detecting egfr sensitizing and t790m resistance mutations in tumor tissue . 
it is presently the only plasma genotyping assay with an fda indication for the detection of egfr mutations in metastatic nsclc for the purpose of initiating treatment with an egfr kinase inhibitor in both the initial and acquired resistance setting.21 the cobas assay was evaluated for these indications through retrospective testing of prospectively collected plasma samples from the ensure trial compared with standard tissue genotyping . 
 tissue biopsy negative t790m test metastatic site 1 metastatic site 2 blood draw positive t790m test egfrm - expressing tumor cell egfr - t790m - expressing tumor cell circulating cell - free normal dna t790m - negative ctdna t790m - positive ctdna circulating tumor dna circulating cell - free normal dna circulating tumor dna fig 2 . 
the presence of egfr t790m has been demonstrated to exhibit heterogeneity across metastatic sites , potentially resulting in false - negative results when performing tissue genotyping on a rebiopsy specimen taken from a nonrepresentative metastatic site . 
pooled data from these studies demonstrated a sensitivity of 61% ( 95% ci , 57% to 66% ) and specificity of 79% ( 95% ci , 70% to 85% ) for the detection of the egfr t790m mutation.38 a similar comparison was performed using prospectively collected samples from the aura3 study that randomly assigned patients with metastatic nsclc with egfr t790m mediated acquired resistance to egfr kinase inhibitors to either standard platinum - based chemotherapy or osimertinib.39 the study of the plasma cobas assay for egfr t790m in aura3 demonstrated a lower sensitivity of 51% ( 95% ci , 46% to 57% ) but similar specificity of 77% ( 95% ci , 71% to 83% ) .40 interestingly , both studies demonstrated near - perfect specificity for the detection of egfr exon 19 del and l858r , leading to suspicion that the lower specificity was secondary to heterogeneity of resistance mechanisms between metastatic sites within the same patient , thus rendering tumor tissue genotyping a nondefinitive reference standard . 
this hypothesis is supported by the finding that patients who are plasma - positive for egfr t790m exhibit clinical benefit similar to those who are tissue genotypingpositive and that repeat tissue biopsy of patients with acquired resistance led to discordant tissue genotyping results for egfr t790m but not egfr sensitizing mutations ( fig 2 ) .20 , 35 the cobas assay is the best - validated example of the use of pcr - based plasma genotyping assay to assess specific genetic hotspots corresponding to potentially targetable genomic alterations . 
 multiple other plasma genotyping assays have been evaluated for the detection of genomic alterations in metastatic nsclc in studies ranging in scope from analysis of prospectively collected banked plasma samples from large clinical trials to small retrospective series . 
these studies have demonstrated a consistent trend of high specificity but more modest sensitivity.9 , 41 , 42 plasma genotyping using pcr - based approaches is readily able to detect point mutations as well as defined stereotypical insertions and deletions . 
 however , the detection of complex rearrangements and copy number alterations using these platforms is challenging . droplet digital pcr and beads , emulsion , amplification , and magnetics genotyping emulsion digital pcr - based assays for plasma genotyping afford the ability to detect mutant cfdna in a highly sensitive but also quantitative manner . 
 study demonstrated that this assay was able to detect egfr exon 19 del and l858r mutations with a sensitivity of 82% and 74% , respectively , and a specificity of 100% . 
similar assay characteristics were reported for the detection of kras codon 12 mutations ( sensitivity 64% , specificity 100% ) .35 interestingly , similar sensitivity ( 77% ) but more modest specificity ( 63% ) was noted for the detection of egfr t790m . 
a subset of five patients initially reported as being falsely positive for egfr t790m by plasma genotyping were found to be truly positive on repeat tissue biopsy and genotyping of an alternative metastatic sitea finding not observed for any of the aforementioned driver mutations.35 this finding underscores the potentially heterogeneous nature of resistance mutations such as egfr t790m , whereby only growing sites of disease may possess the resistance mutation of interest . 
 tissue genotyping thus has the potential to be falsely negative when testing for an acquired resistance mutation , in contrast to plasma genotyping , which allows for the detection across metastatic sites within the same patient . beads , emulsion , amplification , and magnetics ( beaming ) based plasma genotyping assays have similarly been evaluated for the detection of egfr sensitizing and resistance mutations in patients with metastatic nsclc with acquired resistance to egfr kinase inhibitors . 
despite the rapid and quantitative nature of emulsion - based technologies , they are somewhat limited in terms of panel size and ability to multiplex . next - generation sequencing multiple next - generation sequencing ( ngs ) based platforms for plasma genotyping have been evaluated for the detection of genomic in nsclc.16 , 17 , 22 , 43 ngs - based alterations plasma genotyping assays have a greater ability to detect complex genomic alterations , such as complex rearrangements and high copy number alterations , that may be difficult to identify using other methods . 
a recent retrospective study of plasma samples collected in the biocast / ifct - 1002 study compared an ngsbased ( iontorrent , thermo fisher scientific , waltham , ma ) plasma genotyping assay to standard tissue genotyping in 68 matched samples of never - smokers with metastatic nsclc . 
this study demonstrated a sensitivity of 58% ( 95% ci , 43% to 71% ) and specificity of 87% ( 95% ci , 62% to 96% ) for the detection of mutations in key genes , including egfr , her2 , kras , braf , and pik3ca.16 a more recent retrospective study of 48 patients with metastatic nsclc comparing an ngs - based plasma genotyping assay performed on a miseq platform ( resolution bioscience ) to both ddpcr - based plasma genotyping and standard tissue genotyping revealed comparable sensitivity ( 77% , 48 of 62 positive cases detected ) and specificity ( 100% ; 95% ci , 90% to 100% ) , as well as the ability to reliably detect complex alterations , including alk and ros1 rearrangements.43 commercial plasma genotyping assays that use ngs - based platforms with expansive gene panels have been compared with tissue genotyping reference standard across multiple tumor types , and concordance rates between the two sample types are approximately 85% ( guardant360 , foundationact ) .22 , 23 other methods a multitude of other testing platforms have been used to develop plasma genotyping assays . 
 testing platforms are beyond the scope of this article and have been recently reviewed elsewhere . specimen type and handling careful and standardized methods for the isolation of cfdna from plasma are essential to optimize assay sensitivity and reproducibility . 
the collection of blood in a dna preservation tube , rapid sample processing , and the careful isolation of plasma in a fashion that minimizes cellular contamination ( centrifugation with double spin and disabled brake ) have been previously demonstrated to optimize sample quality for subsequent plasma genotyping.35 the use of plasma is preferable to serum , because the level of nontumor cfdna contamination is lower and less variable in plasma . 
the total cfdna level is frequently higher in serum samples , presumably because of white blood cell rupture during standard serum isolation , which requires allowing the blood sample to clot . 
plasma genotyping results can be available significantly faster compared with standard tissue genotyping for metastatic nsclc in both patients with newly diagnosed disease and those with disease progression while receiving initial targeted therapy.35 however , the optimal use and interpretation of plasma genotyping results hinges on specific details of the clinical scenario in which it is used . clinical actionability plasma genotyping assays consistently demonstrate high specificity and positive predictive value but modest sensitivity . 
the detection of a targetable genomic alteration in genes , including egfr , alk , ros1 , braf , met , ret , and her2 , provides useful information that may be directly used to select therapy . 
for instance , the detection of an egfr exon 19 del mutation in a patient with newly diagnosed metastatic nsclc may be used to initiate therapy with a firstor second - generation egfr kinase inhibitor ( eg , erlotinib , gefitinib , or afatinib )  . 
as a corollary , the detection of mutually exclusive , nontargetable driver genomic alterations ( eg , kras mutation ) is also useful because it provides reassurance that one of the aforementioned targetable genomic alterations is not present and that targeted therapy is not a therapeutic option.48 , 49 thus , plasma genotyping panels must be designed to detect clinically actionable genomic alterations as well as known nontargetable driver mutations . treatment status the established utility of plasma genotyping for the purpose of treatment selection in metastatic nsclc is limited to a small number of clinical scenarios . 
the best - evaluated use of plasma genotyping is for the selection of therapy in patients with newly diagnosed metastatic nsclc.15 , 37 validated plasma genotyping assays have been demonstrated to yield high sensitivity as well as near - perfect specificity for the detection of targetable genomic alterations in patients with newly diagnosed disease . 
plasma genotyping also has the capability to yield genotyping results with improved turnaround time and obviates the need for repeat biopsies in patients with newly diagnosed disease whose initial diagnostic biopsy samples are insufficient for tissue genotyping . patients with a targetable genomic alteration and acquired resistance to initial targeted therapy represent an additional clinical scenario in which plasma genotyping can guide therapy . 
the best - characterized example is the egfr t790m resistance mutation in metastatic nsclc that confers acquired resistance to firstand second - generation egfr kinase inhibitors but sensitivity to third - generation egfr kinase inhibitors . 
potentially targetable acquired resistance mutations , such as egfr t790m , emerge in a heterogeneous fashion in metastatic nsclc ; as a result , not all sites of disease may harbor a given resistance mutation , and thus the detection of such genomic alterations is inherently complex . plasma genotyping has also been evaluated with regard to monitoring the emergence of treatment resistance in patients already receiving therapy.50 , 51 the use of plasma genotyping in this context to detect early disease progression , in advance of clinical or radiographic evidence of progression , is presently investigational and should not be used to change treatment in the absence of objective evidence of disease progression . clinical stage the use of plasma genotyping has demonstrated utility for guiding therapy in metastatic nsclc but is investigational in nonmetastatic disease . 
the optimal use of this technology and interpretation of its results hinges on careful synthesis of three key concepts : cfdna biology , specific assay technology , and the individual clinical oncology of the individual patient ( fig 3 )  . patients with newly diagnosed disease plasma genotyping in a patient with newly diagnosed metastatic nsclc is most informative when a targetable genomic alteration ( eg , egfr , alk , ros1 , braf , met ) or a nontargetable mutually exclusive driver alteration ( eg , kras ) is found . 
the use of an fda - approved and rigorously validated plasma genotyping assay allows for immediate initiation of appropriate targeted or systemic therapy in the instance of a positive result , given the high specificity and positive predictive value of these assays . 
negative plasma genotyping results where no driver alteration is detected are not useful in guiding therapy , given the modest sensitivity of such assays , and should prompt appropriate tissue genotyping if not already initiated . 
importantly , caution must be exercised in interpreting low - level positive results near the limit of detection , particularly of nondriver alterations detected on poorly validated panels , as there exists the risk of assay artifact and a false - positive result . acquired resistance plasma genotyping should be used as the initial genotyping method in the setting of acquired resistance to targeted therapy in metastatic nsclc . 
this approach has the ability to obviate the need for repeat biopsy in many instances but also detects resistance mechanisms that may be missed on repeat tissue genotyping because of heterogeneity of resistance mechanisms . 
the absence of an identifiable resistance mutation should prompt repeat tissue biopsy and genotyping to rule out a false - negative result , as well as examine for alternative resistance mechanisms that are not easily identified through plasma genotyping , such as small - cell transformation or met amplification . 
as a corollary , a plasma genotyping result that fails to detect the original targetable alteration in a patient with acquired resistance should be considered indicative of the absence of tumor cfdna shed , and the result invariably a false negative . 
importantly , plasma testing for acquired resistance as well as repeat biopsy should only be initiated in patients with clinically or radiographically significant disease progression , to avoid inadvertently labeling a patients disease t790m negative because of testing before the emergence of clinical resistance . 
a recent retrospective study demonstrated improved sensitivity with the use of combined urine and plasma genotyping in a cohort of patients with metastatic resistant egfr - mutant nsclc.52 this finding supports the hypothesis that the use of multiple orthogonal testing strategies may be effective in enhancing overall diagnostic sensitivity . 
furthermore , the combination of plasma and tissue genotyping alone has the potential to surmount the modest sensitivity in the context of acquired resistance . the potential utility of serial quantitative plasma genotyping for the purpose of monitoring response to therapy , as well as the evolution of acquired resistance , constitutes another promising area of research . 
 therapeutic response in clinical trials of novel agents may allow for real - time monitoring of response to therapy as well as early prediction of potential mechanisms of acquired resistance . 
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thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . 
sacher a , alden r , oconnell a , et al : a prospective study of rapid plasma genotyping utilizing sequential ddpcr and ngs in newly diagnosed advanced nsclc patients . 
 cholangiocarcinoma with fgfr genetic aberrations : a unique clinical phenotype purpose fgfr genetic aberrations ( gas ) occur in an estimated 10% to 16% of intrahepatic cholangiocarcinomas ( ccas )  . 
the natural history of cca with fgfr gas , the prognostic role of coexisting gas , and the outcome with fgfr - targeted inhibitors are unknown . patients and methods patients with cca with fgfr gas were identified using next generation sequencing or fluorescence in situ hybridization from four tertiary cancer centers and compared with fgfr wild - type counterparts . 
fishers exact test , kaplan - meier plots , and log - rank tests were used for statistical analysis . results three hundred seventy - seven patients with cca were identified , and 95 had fgfr gas . 
bap1 mutation was the most common coexisting mutation without prognostic impact , whereas tp53 ( p = .04 ) and cdkn2a / b ( p = .04 ) were correlated with a shorter conclusion cca with fgfr gas represents a unique subtype occurring in younger patients with an indolent disease course . 
2018 by american society of clinical oncology introduction biliary tract cancers including intrahepatic and extrahepatic cholangiocarcinoma ( cca ) and gallbladder cancers are uncommon tumors that typically present at an advanced disease stage and are characterized by an aggressive disease course and poor clinical outcome . 
the incidence of these cancers is hard to estimate accurately because some intrahepatic ccas ( ihccas ) are still classified as cancer of unknown primary or included into the larger group of primary liver cancer . 
in 2016 , 40 , 710 primary liver cancers ( which include hepatocellular cancer and ihcca ) and 11 , 740 gallbladder and extrahepatic biliary tract cancers were diagnosed in the united states.1 the incidence of these cancers , particularly ihcca , is increasing in the western world.2 higher incident rates of cca occur in the southeast asian population as compared with the western population ( > 80 per 100 , 000 population in northeast thailand v 0.3 per 100 , 000 population in canada ) , 3 whereas gallbladder cancer occurs more commonly in south asia and latin america . 
this geographic difference can at least partly be attributed to etiologic factors such as fluke infection endemic to certain parts of asia.4 not only are there major etiologic and epidemiologic differences between the three types of apurva jain mitesh j . 
with emerging technolincluding next - generation sequencing ogies , ( ngs ) , scientists have identified actionable mutations in the isocitrate dehydrogenase 1 / 2 ( idh1 / 2 ) , fgfr2 , braf , and her2 / neu genes for targeted therapeutics in cca and gallbladder cancer.5 - 8 these studies indicate that the incidence of specific genetic differences may vary according to biliary cancer subtype . 
idh1 / 2 , fgfr2 , and braf genetic aberrations ( gas ) occur with significantly higher incidence in ihcca , whereas kras , tp53 , and cdkn2a / b are more common in extrahepatic cca and her2 / neu amplifications are more likely to occur in gallbladder cancer . 
idh1 mutations and fgfr2 fusions seem to be mutually exclusive.9 , 10 ongoing trials are investigating the impact of targeted agents against these actionable mutations with promising early results . the fibroblast growth factor receptor ( fgfr ) family consists of four transmembrane receptors ( fgfr1 to fgfr4 ) , 18 fgf ligands , and a heparan sulfate proteoglycan that stabilizes and sequesters the fgfs . 
the ligand - receptor combination is responsible for the activation of downstream ras / raf / mek , jak / stat , and pi3k / akt pathways.11 gas such as activating mutations , amplifications , or chromosomal translocations / fusions in the fgfr pathway contribute to malignant transformation . 
in ihcca , fgfr2 fusions have been observed in 10% to 16% of patients using next - generation tumor dna sequencing methods.12 , 13 however , rna sequencing studies suggest that fgfr gas occur at a higher rate of 45% in surgically resectable disease stage.14 the natural history , prognostic impact , response to fgfr - directed therapy , and clinical phenotype of cca with fgfr gas have not yet been described in detail . 
a better understanding of this subset may enable precision medicine approaches for the management of these rare , fatal cancers . university cancer center , mayo clinic , and university of californiasan francisco helen diller family comprehensive cancer center . 
 the 95 patients included in the study were those who had pathologically confirmed biliary cancer between january 2000 and december 2015 , had at least 3 months of follow up , and had fgfr gas ( fgf19 , fgfr1 , fgfr2 , fgfr3 , or fgfr4 ) on molecular testing . 
our comparison group included 282 patients with the same cancers from the same institutions without any known fgfr gas on molecular profiling with ngs using a common platform ( foundationone ; foundation medicine , cambridge , ma ) , as described in the next section . 
these data included demographic characteristics , clinical history , diagnosis and tumor location , tumor stage and grade at diagnosis , surgical procedures , radiation and systemic treatments received , and current status . targeted ngs pretreatment formalin - fixed , paraffin - embedded tissue from biopsies of primary or metastatic tumor sites or surgically resected specimens were sent for targeted ngs . 
finally , fgfr2 break apart fish probe mix ( abbott molecular diagnostics , des plaines , il ) , containing spectrumorange ( spanning 353.6 kb targeting the centromeric part of gene ) and spectrumgreen ( spanning 491.3 kb targeting the telomeric part of gene ) probes in hybridization buffer , was then applied to the etched area of the slide , and a cover slip was applied . 
these studies were performed as a part of standard management of patients with cca , and the methods have been described in detail elsewhere.13 , 16 statistical methods categorical variables such as patient sex , histologic tumor grade , and stage at diagnosis were summarized as total counts and frequencies . 
we used the log - rank test for discrete variables and the cox proportional hazards model for continuous variables to test the associations of clinical / genetic features with os and to estimate hazard ratios ( hrs ) and 95% cis . 
the median age was 61 years ( range , 22 to 85 years ) in patients with fgfr gas and 56 years ( range , 22 to 82 years ) in patients without fgfr gas . 
no differences were noted in the percentage of patients who received surgical and radiation therapy . no genetic aberration ( n = 282 ; median os , 20 months [ 95% ci , 17 to 26 months ] ) genetic aberration present ( n = 59 ; median os , 30 months [ 95% ci , 20 to 97 months ] ) time ( months ) no . 
 in patients with advanced disease ( stage iii or iv ) , patients with fgfr gas had a longer median os compared with the fgfr wt group ( 24 v 17 months , respectively ; p < .004 ; appendix fig a1 ) , suggesting that advanced cca with fgfr gas may have a more indolent course . 
kras , idh1 , and braf mutations did not coexist with the fgfr2 fusions , suggesting that these may be mutually exclusive . table 2 lists the univariable analysis results in patients with fgfr gas ( n = 95 )  . 
patients who received fgfr - directed treatment had a significantly improved os ( 44.8 months ) compared with patients who received standard treatment ( 24.3 months ; p = .01 ; fig 3 )  . 
 the majority of the patients enrolled onto clinical trials had fgfr2 fusion ( n = 27 , 75% ) ; other gas included fgfr3 ( n = 2 ) and fgf19 ( n = 1 )  . 
 our results suggest that fgfr gas may be associated with a relatively indolent disease course ( confirming earlier reports from our group ) 5 and responsiveness to targeted fgfr inhibitors . 
furthermore , the relationship between fgfr gas with tumor location ( primary tumor v metastases ) and uncommon histologies such as undifferentiated cancers and hepatocholangiocarcinoma deserves further study . several fgfr - targeted inhibitors are currently in clinical trials . 
these include multitargeted tyrosine kinase inhibitors , such as ponatinib , nintedanib , and dovitinib , and more specific fgfr - directed small - molecule tyrosine kinase inhibitors , such as bgj398 , jnj425756493 , prn1371 , arq087 , and tas - 120 . 
the overall response rate was 15% , disease control rate was 95% , and pfs was 6 months , indicating the potential of this therapy for ccas with fgfr gas.17 the more recent third - generation therapy options , including fgfr isoformspecific fgfr inhibitors ( eg , rg744 / mgfr1877s , fgf401 ) and fgfr trap molecules ( eg , gsk3052230 ) , need further investigation.18 these agents are currently being investigated in the second - line setting after prior chemotherapy . 
further investigation of these drugs in the first - line setting and concurrently with chemotherapy is required . although the majority of our patients had fgfr2 fusions ( 77% ) , the rest of the patients with other fgfr gas exhibited a clinical course similar to that of patients with fgfr2 fusions and showed response or prolonged stability ( eg , with fgf19 amplifications )  . 
bap1 mutation is associated with a poor prognosis in uveal melanoma and renal and colorectal cancer.19 - 21 coexisting bap1 mutations occurred frequently in patients with fgfr gas in our series ( n = 16 , 22% )  . 
however , these cancers in the advanced disease setting can be misclassified on radiology alone , and it is possible that the number of patients with ihcca may be higher in our study . 
furthermore , the ngs platforms have become more comprehensive with time , leading to the possibility that some patients with cca investigated using older platforms were false negative for table 3 . 
 shroff , milind javle financial support : funda meric - bernstam , milind javle administrative support : funda meric - bernstam , milind javle provision of study material or patients : robin kate kelley , funda meric - bernstam , ahmed omar kaseb , tanios bekaii - saab , rachna t . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . apurva jain no relationship to disclose tertiary care centers with availability of clinical trials of targeted therapies . despite these limitations , this study is important , as it is , to our knowledge , the first clinical and molecular characterization of a large cohort of patients with cca harboring fgfr gas . 
 funda meric - bernstam honoraria : dialecta honoraria : sumitomo group , genentech , inflection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , grail thomas deleon no relationship to disclose andrea grace bocobo no relationship to disclose research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , effective pharmaceuticals , curis , pfizer tanios bekaii - saab consulting or advisory role : amgen , celgene , national comprehensive cancer network , genentech , bayer , boehringer ingelheim , research to practice , merrimack , glenmark , ipsen ( inst ) , eli lilly , bristol - myers squibb ( inst ) keith a . 
shroff consulting or advisory role : celgene , codiak biosciences , amgen , agios , halozyme research funding : eli lilly , celgene , agios , halozyme travel , accommodations , expenses : celgene , codiak biosciences , amgen , agios , halozyme daniel h . 
ahn consulting or advisory role : celltrion ( i ) , merrimack , astellas pharma , eisai , cardinal health , paradigm milind javle no relationship to disclose affiliations apurva jain , ying wang , reham abdel - wahab , funda meric - bernstam , keith a . 
borad and thomas deleon , mayo clinic , scottsdale , az ; robin kate kelley and andrea grace bocobo , university of californiasan francisco helen diller family comprehensive cancer center , san francisco , ca ; reham abdel - wahab , assiut university hospital , assiut , egypt ; and daniel h . 
blum , michael lu , and patricia maxin funds for cholangiocarcinoma research and the international cholangiocarcinoma research network . presented , in part , at the clinical science symposium of the 52nd annual meeting of the american society of clinical oncology , chicago , il , june 3 - 7 , 2016 . support prior presentation references 1 . 
goyal l , govindan a , sheth ra , et al : prognosis and clinicopathologic features of patients with advanced stage isocitrate dehydrogenase ( idh ) mutant and idh wild - type intrahepatic cholangiocarcinoma . 
di stefano al , fucci a , frattini v , et al : detection , characterization , and inhibition of fgfr - tacc fusions in idh wild - type glioma . 
borad mj , champion md , egan jb , et al : integrated genomic characterization reveals novel , therapeutically relevant drug targets in fgfr and egfr pathways in sporadic intrahepatic cholangiocarcinoma . 
javle mm , shroff rt , zhu a , et al : a phase 2 study of bgj398 in patients ( pts ) with advanced or metastatic fgfr - altered cholangiocarcinoma ( cca ) who failed or are intolerant to platinum - based chemotherapy . 
hierro c , rodon j , tabernero j : fibroblast growth factor ( fgf ) receptor / fgf inhibitors : novel targets and strategies for optimization of response of solid tumors . 
progression - free survival ( pfs ) kaplan - meier curves for patients with and without fibroblast growth factor receptor ( fgfr ) genetic aberrations ( gas ) who received first - line chemotherapy for systemic disease . 
ileana dumbrava , md1 ; kavitha balaji , phd1 , 2 ; kanwal raghav , md1 ; kenneth hess , phd1 ; milind javle , md1 ; mariela blum - murphy , md1 ; jaffer ajani , md1 ; scott kopetz , md , phd1 ; russell broaddus , md , phd1 ; mark routbort , md , phd1 ; mehmet demirhan , md1 ; xiaofeng zheng , phd1 ; shubham pant , md1 ; apostolia m . 
piha - paul , md1 ; and funda meric - bernstam , md1 purpose human epidermal growth factor receptor 2 ( her2 ) is an effective therapeutic target in breast and gastric and gastroesophageal junction cancers . 
overexpression of her2 protein occurs through her2 gene amplication or through translational mechanisms3 other and can result in the formation of spontaneous receptor homodimers , resulting in the initiation of downstream signaling cascades and malignant transformation.4 , 5 her2 amplication is a prognostic transcriptional or biomarker for worse survival in the absence of antiher2 therapy.6 , 7 her2 is a compelling therapeutic target in patients with breast6 , 8 - 10 and gastric or gastroesophageal junction ( gej ) cancers.11 for her2 - overexpressing or her2 - amplied breast cancer , several her2 - targeted therapies are approved for use in the adjuvant and metastatic settings , including trastuzumab ( metastatic and adjuvant ) , pertuzumab ( metastatic and adjuvant ) , lapatinib ( metastatic ) , ado - trastuzumab emtansine ( metastatic ) , and neratinib ( adjuvant )  . 
 dumbrava et al context key objective our study focused on assessment of erbb2 ( her2 ) amplication in patients with solid tumors , excluding breast cancer , who underwent next - generation sequencing . 
we evaluated the clinical benet of her2 - targeted therapy by measuring the timedependent overall survival from the genomic testing results , progression - free survival ( pfs ) , and pfs during her2 - targeted therapy compared with pfs during prior therapy . knowledge generated we showed that her2 amplication is present in a clinically relevant proportion of tumors and in a variety of tumor types and that her2 - targeted therapy may confer clinical benet , with increased survival in patients with tumor types other than those for which her2 inhibitors are approved . relevance her2 is an established effective therapeutic target in breast , gastric , and gastroesophageal junction cancers ; however , less is known about the prevalence of her2 amplication and efcacy of her2 - targeted treatment in other tumors . 
validation of these results in a larger study could focus on determining the associations of copy number , simultaneous her2 mutations , and other coalterations with response to her2 - targeted therapies . agents are in development , such as the bispecic her2 antibody zw25 and the antibody - drug conjugate ds - 8201.12 , 13 targeted therapy with pfs during prior therapy . 
we also compared the overall survival ( os ) of patients who received her2 - targeted therapy with the os of patients who did not . the main mechanism of her2 overexpression is her2 gene amplication , which occurs in 18% to 20% of patients with breast cancer14 , 15 and 7% to 34% of patients with gastric or gej cancers.11 , 16 , 17 asco and the college of american pathologists recommended testing in breast and gastric or gej cancers using immunohistochemistry ( ihc ) for her2 protein expression or in situ hybridization ( uorescence in situ hybridization [ fish ] , chromogenic in situ hybridization , or silver in situ hybridization ) for her2 gene amplication.14 , 18 other techniques , such as comparative genomic hybridization , can also be used to detect copy number variations.19 - 21 however , with the development and integration of next - generation sequencing ( ngs ) in cancer care and the increasing capacity of ngs to determine copy number variations concurrently with other alterations such as mutations , ngs has become a more cost - effective and tissue - efcient alternative to current single - gene assessment methods.22 her2 amplication also occurs in other carcinomas at differing frequency.23 - 25 although relatively little is known about the role of her2 in other tumor types , emerging data indicate that her2 - targeted therapy may have efcacy in other her2 - positive tumors.26 we hypothesized that her2 - targeted therapy could be associated with clinical benet in tumor types other than breast and gastric or gej cancers . 
for the current study , the ngs analysis was performed using four platforms , including the oncomine comprehensive assay ( thermofisher , waltham , ma ) or ion ampliseq comprehensive cancer panels ( thermofisher ) performed at the university of texas md anderson cancer center molecular diagnostic laboratory , 27 foundationone or foundationone heme ( foundation medicine , cambridge , ma ) tumor testing , or guardant360 ( guardant health , redwood city , ca ) circulating cell - free dna ( cfdna ) testing . 
the genomic testing results were annotated by the precision oncology decision support system at the university of texas md anderson cancer center.28 the patients relevant clinical and molecular characteristics were collected from electronic medical records and prospectively maintained institutional databases ( table 1 )  . 
of prior lines of treatment 57 ( 11 ) 29 - 79 64 ( 52 ) 58 ( 48 ) 42 ( 34 ) 80 ( 66 ) 15 ( 12 ) 107 ( 88 ) 98 ( 80 ) 17 ( 14 ) 7 ( 6 ) abbreviations : fish , uorescent in situ hybridization ; her2 , human epidermal growth factor receptor 2 ; ihc , immunohistochemistry ; sd , standard deviation . * some patients had multiple genomic testing . for her2 amplication , was performed in some patients and was also reviewed in this study . the her2 - targeted clinical trials had been individually approved and conducted at the university of texas md anderson cancer center in accordance with institutional review board guidelines , and this reported analysis was conducted under an institutional review boardapproved protocol . her2 amplication and overexpression analysis her2 amplication determined by ngs was dened according to each platforms analytic pipeline , was based on the resulting reports and validation , and varied between greater than ve to greater than seven estimated copy numbers for reporting high - condence amplication.29 , 30 for patients who underwent cfdna analysis , digital sequencing was performed by guardant health , using a 54gene panel ( guardant360 )  . 
to determine the clinical benet of her2 - targeted therapy , we measured pfs during matched her2 - targeted therapy ( pfs2 ) and compared it with pfs during prior therapy ( pfs1 ) .32 , 33 pfs was dened as the time from the start of treatment until disease progression or death . 
response to treatment and progression were determined using response evaluation criteria in solid tumors ( recist ) version 1.1 , as measured by radiologists or investigators.34 patients who received her2 - targeted therapy as the rst systemic treatment were excluded from the pfs2 - to - pfs1 analysis . we also evaluated the os of patients who received her2targeted therapy and compared it with the os of patients who did not receive her2 - targeted therapy . 
os was calculated as a time - dependent indicator variable in both the kaplan - meier and cox proportional hazards analyses from the genomic testing result until death from any cause . 
the royal marsden hospital prognostic score for predicting survival in phase i trials35 ( including albumin , lactate dehydrogenase [ ldh ] , and number of metastatic sites ) , number of prior lines of treatment , disease stage , and eastern cooperative oncology group ( ecog ) performance status at the time of genomic testing were also analyzed . statistical analysis we used descriptive statistics to summarize the characteristics of patients with her2 amplications . 
concordance between ngs and ihc and between ngs and fish tests was calculated by dividing the number of samples that had concordant results by the total number of samples . univariable and multivariable cox proportional hazards models were t to assess the association between prognostic factors and os , in which the prognostic factors included her2 - targeted therapy , sex , age , histology , ecog performance status , number of prior therapies , number of metastatic sites , disease stage , ldh , albumin , and number of metastatic sites at time of genomic testing . 
one hundred six patients were found to have her2 amplication on tumor tissue analysis on the foundationone , oncomine comprehensive assay , or ion torrent ampliseq comprehensive cancer platforms , and 24 patients were found to have her2 amplications on cfdna analysis using guardant360 technology ( fig 1 )  . 
the most frequent her2 - amplied tumor types included gastric or gej , esophageal , endometrial , bladder , biliary or gallbladder , salivary gland , colorectal , and cervical tumors ( fig 2 )  . 
of the two patients with discordant results , one had low - level ( 1 + ) her2 amplication on cfdna , and the other had equivocal amplication on foundationone . twenty - four patients had positive her2 amplication on the guardant360 platform for cfdna . 
among these 11 patients , ve also had ihc testing , all with concordant positive her2 protein expression , and her2 amplication was conrmed in all three patients who had fish testing ( appendix table a1 )  . clinical benet of her2 - targeted therapy we studied the clinical actionability of her2 amplication and clinical benet of her2 - targeted therapy in 122 evaluable patients who had the molecular testing done more than 6 weeks from the current analysis . 
response to treatment was determined by recist version 1.1 , except in three patients who had clinical progression without radiologic documentation of progressive disease . forty - two ( 34% ) of 122 patients with her2 amplications on ngs also underwent her2 ihc testing . 
of these 42 patients , 31 ( 74% ) had her2 protein overexpression ( 3 + ) , four ( 9% ) had equivocal expression ( 2 + ) , two ( 5% ) had low expression ( 1 + ) , and ve ( 12% ) had no her2 expression . forty patients with other tumor types than the ones for which her2 inhibitors are approved ( 38% ) received at least one line of her2 - targeted therapy , with eight patients receiving more than one line of her2 - targeted therapy . most patients ( 93% ) received trastuzumab in combination foundationone or foundationone heme panels ( n = 2 , 086 ) oncomine comprehensive assay panel ( n = 2 , 494 ) ion ampliseq comprehensive cancer panel ( n = 153 ) guardant 360 panel ( n = 269 ) fig 1 . 
of patients cancer type % colorectal biliary gastric 11.9 lung endometrial bladder esophageal ovarian pancreatic salivary gland hnscc liver cervical melanoma peritoneal prostate urachal 28.6 small intestine unknown primary vulvar 10.0 6 / 116 6 / 64 5 / 307 4 / 172 4 / 86 3 / 106 3 / 173 2 / 69 1 / 346 1 / 38 1 / 192 1 / 36 1 / 58 1 / 10 foundationone oncomine cms400 guardant360 fig 2 . 
cms400 , ion ampliseq comprehensive cancer panel ; her2 , human epidermal growth factor receptor 2 ; hnscc , head and neck squamous cell carcinoma ; oncomine , oncomine comprehensive assay panel . with chemotherapy or other targeted therapies . 
across different lines of treatment , 27 patients received trastuzumab with other targeted therapies such as pertuzumab , 14 patients received trastuzumab and chemotherapy , three patients received small - molecule inhibitors targeting her2 , three patients received antibody - drug conjugates or bispecic antibodies against her2 , and two patients received trastuzumab alone . 
other factors associated with a longer os were ecog performance status of 0 or 1 , a royal marsden hospital prognostic score of 0 or 1 ( normal albumin and ldh levels and two or fewer metastatic sites ) , and colorectal cancer tumor type as compared with other histologies ( table 2 )  . among 37 patients with cancers other than gastric , gej , or esophageal cancers in whom her2 - targeted treatment was given in the second line or later and for whom previous treatment the pfs2 - to - pfs1 ratio was 1.3 or greater in 21 patients ( 57% ) , and the information was available , median pfs2 and pfs1 times were 24 and 13 weeks , respectively ( p , .001 ; fig 4 )  . twelve ( 30% ) of 40 patients with tumor types other than gastric cancer achieved an objective response as dened by complete or partial response per recist version 1.1 , with seven patients receiving trastuzumab and pertuzumab , four patients receiving trastuzumab with chemotherapy , and one patient receiving an her2 antibody - drug conjugate . 
of prior lines of treatment : 0 - 2 v 3 - 7 determinants of enrollment on her2 - targeted therapy the median time between ngs showing an her2 amplication and start of her2 - targeted therapy was 16 weeks . we investigated the reasons why 68 patients did not receive her2 - targeted therapy after their ngs results showed her2 amplication . 
the leading cause was noneligibility for an her2 - targeted clinical trial ( n = 28 ; 41% ) because of equivocal her2 amplication results , insurance denial , or clinical issues such as poor performance status , chronic tumor - related bleeding , or inadequate organ function ( appendix fig a1 )  . discussion in a large cohort of patients who underwent targeted ngs to facilitate personalized cancer treatment , we found her2 amplication in tumor types other than breast and gastric or gej cancers . 
ngs has been shown to meet the sensitivity of detection for mutations used in clinical trials , permitting simultaneous testing of copy number variations in hundreds of genes.28 , 40 , 43 currently , there are several ongoing clinical trials evaluating prevalence of her2 alterations and the benet of targeting her2 in different tumor types ( eg , clinicaltrials.gov identiers : nct02465060 , nct02675829 , nct02091141 , nct02693535 )  . 
the recently published results from the mypathway trial26 , 45 studying treatment with trastuzumab and pertuzumab in colorectal cancer showed an overall response rate of 40% in patients without kras mutations , conrming preliminary data that her2 testing could be integrated in future guidelines for biomarker testing in other tumor types , such as colorectal , 44 , 46 salivary , bladder , and biliary cancers . 
on the basis of these ndings , the national comprehensive cancer network colorectal cancer guidelines were updated recently to include pertuzumab plus trastuzumab and trastuzumab plus lapatinib as category 2b recommendations for her2 - positive colorectal cancer.47 in this study , ngs identied her2 amplication in 2.4% of patients across 20 tumor types . 
although her2 amplications were found in many different epithelial cancers , positive results were rare , and often nonexistent , in malignancies of nonepithelial origthis nding was consistent with the her2 overexpression results reported by yan et al42 in 37 , 992 patients . 
 her2 amplication identied by ngs in contrast with breast cancer , for which her2 - targeted therapies have been established for a long time with ve treatment options approved by the us food and drug administration , for gastric , gej , or esophageal cancers , less is known about the prognostic role of her2 , and therapeutic options are limited to trastuzumab in combination with chemotherapy.26 our results suggest there is a clinical benet in patients with indications beyond gastric or gej cancers . in tissue samples , the thresholds for reporting are higher for ngs than for fish ; therefore , the tissue - based ngs test used in our study may have underestimated the rate of her2 amplication . 
our results on testing for her2 status by ngs compared with ihc and fish are consistent with a previous report of high concordance between ihc and fish in colorectal cancer.49 , 50 many patients were not eligible for her2 - targeted therapies , highlighting the importance of patient selection for genomic testing . 
however , as evidence for actionability of her2 increases , her2 testing should be considered earlier in the treatment course for tumor types in which her2 is more frequently amplied ( eg , colorectal cancer )  . sequential testing by ihc and fish and further mutation analyses may lead to tissue exhaustion before the completion of all necessary testing . 
thus , early incorporation of ngs into clinical practice for diseases with frequent actionable genomic alterations has the advantage of screening for multiple therapeutic options simultaneously while sparing tissue . limit limitations that might our study has several generalizability of our ndings . 
although ngs has many advantages , samples with low tumor content , heterogeneity , and low levels of amplication may result in false - negative results where her2 amplication might have been detected on fish20 ; thus , we are likely underestimating the frequency of her2 amplication.51 a higher prevalence of her2 amplication on liquid biopsies could be , at least in part , related to a selection bias and may be consistent with emergence of her2 amplication as a mechanism of rereceptortargeted sistance to epidermal growth factor therapy , 52 - 54 explaining the higher discordance rates when compared with gold standard tissue - based tests . 
however , patients with her2 amplication detected on ngs may have higher levels of amplication and therefore may have greater benet from her2 - targeted therapy . ngs reveals her2 amplication in a clinically relevant proportion of tumors and in a variety of tumor types , and her2 - targeted therapy may confer clinical benet in tumor types beyond those for which her2 inhibitors are approved . 
further studies are needed to conrm these results and to determine the associations of copy number , simultaneous her2 mutations , and other coalterations with response to her2 - targeted therapies . 
the association of her2 amplications with genomic alterations in other oncogenic drivers provides rationale for novel therapeutic combinations . affiliations 1the university of texas md anderson cancer center , houston , tx 2lexicon pharmaceuticals , houston , tx translational sciences grant no . 
ileana dumbrava , kavitha balaji , milind javle , mariela blum - murphy , scott kopetz , russell broaddus , mark routbort , mehmet demirhan , xiaofeng zheng , vivek subbiah , david s . 
tsimberidou honoraria : covance , genentech consulting or advisory role : roche research funding : emd serono ( inst ) , baxter ( inst ) , foundation medicine ( inst ) , onyx ( inst ) , bayer ( inst ) , boston biomedical ( inst ) , placon ( inst ) , immatics ( inst ) , karus therapeutics ( inst ) , stem cells ( inst ) , obi pharma ( inst ) patents , royalties , other intellectual property : parker institute for cancer immunotherapy ( inst ) vivek subbiah consulting or advisory role : medimmune research funding : novartis ( inst ) , glaxosmithkline ( inst ) , nanocarrier ( inst ) , northwest biotherapeutics ( inst ) , genentech ( inst ) , berg pharma ( inst ) , bayer ( inst ) , incyte ( inst ) , fujilm ( inst ) , pharmamar ( inst ) , d3 oncology solutions ( inst ) , pzer ( inst ) , amgen ( inst ) , abbvie ( inst ) , multivir ( inst ) , blueprint medicines ( inst ) , loxo ( inst ) , vegenics ( inst ) , takeda ( inst ) , alfasigma ( inst ) , agensys ( inst ) , idera ( inst ) , boston biomedical ( inst ) , inhibrx ( inst ) , exelixis ( inst ) travel , accommodations , expenses : pharmamar , bayer david s . 
hong stock and other ownership interests : molecularmatch , oncorena , presagia honoraria : adaptimmune , baxter , merrimack , bayer consulting or advisory role : baxter , bayer , guidepoint global , janssen , genentech , eisai , glg , alpha insights , axiom biotechnologies , adaptimmune , grouph , merrimack , medscape , numab , pzer , seattle genetics , takeda , trieza therapeutics research funding : novartis , genentech , eisai , astrazeneca , pzer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer , bristol - myers squibb , genmab , ignyta , innity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo , medimmune , molecular templates , takeda , seattle genetics , amgen , fate therapeutics , mologen , national cancer institute cancer therapy evaluation program travel , accommodations , expenses : loxo , mirna therapeutics , genmab jordi rodon consulting or advisory role : novartis , eli lilly / imclone , servier , orion pharma , peptomyc , kelun pharmaceuticals , merck sharp & dohme , spectrum pharmaceuticals , pzer research funding : novartis , bayer kenna m . 
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wolff ac , hammond meh , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
press mf , sauter g , buyse m , et al : her2 gene amplication testing by uorescent in situ hybridization ( fish ) : comparison of the asco - college of american pathologists guidelines with fish scores used for enrollment in breast cancer international research group clinical trials . 
yeh i - t , martin ma , robetorye rs , et al : clinical validation of an array cgh test for her2 status in breast cancer reveals that polysomy 17 is a rare event . 
ross ds , zehir a , cheng dt , et al : next - generation assessment of human growth factor receptor 2 ( erbb2 ) amplication status : clinical validation in the context of a hybrid capture - based , comprehensive solid tumor genomic proling assay . 
zhao m , wang q , wang q , et al : computational tools for copy number variation ( cnv ) detection using next - generation sequencing data : features and perspectives . 
yoon hh , sukov wr , shi q , et al : her - 2 / neu gene amplication in relation to expression of her2 and her3 proteins in patients with esophageal adenocarcinoma . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecular proles : results from mypathway , an open - label , phase iia multiple basket study . 
singh rr , patel kp , routbort mj , et al : clinical massively parallel next - generation sequencing analysis of 409 cancer - related genes for mutations and copy number variations in solid tumours . 
frampton gm , fichtenholtz a , otto ga , et al : development and validation of a clinical cancer genomic proling test based on massively parallel dna se24 : 2719 - 2731 , 2018 quencing . 
press mf , pike mc , hung g , et al : amplication and overexpression of her - 2 / neu in carcinomas of the salivary gland : correlation with poor prognosis . 
gatzemeier u , groth g , butts c , et al : randomized phase ii trial of gemcitabine - cisplatin with or without trastuzumab in her2 - positive non - small - cell lung 39 . 
serrano - olvera a , dueas - gonz alez a , gallardo - rinc on d , et al : prognostic , predictive and therapeutic implications of her2 in invasive epithelial ovarian 40 . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
sartore - bianchi a , trusolino l , martino c , et al : dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - of - concept , multicentre , open - label , phase 2 trial . 
meric - bernstam f , hurwitz h , raghav kps , et al : pertuzumab plus trastuzumab for her2 - amplied metastatic colorectal cancer ( mypathway ) : an updated report from a multicentre , open - label , phase 2a , multiple basket study . 
richman sd , southward k , chambers p , et al : her2 overexpression and amplication as a potential therapeutic target in colorectal cancer : analysis of 3256 patients enrolled in the quasar , focus and piccolo colorectal cancer trials . 
seo an , kwak y , kim dw , et al : her2 status in colorectal cancer : its clinical signicance and the relationship between her2 gene amplication and 50 . 
takezawa k , pirazzoli v , arcila me , et al : her2 amplication : a potential mechanism of acquired resistance to egfr inhibition in egfr - mutant lung cancers that lack the second - site egfrt790m mutation . 
raghav kps , overman mj , yu r , et al : her2 amplication as a negative predictive biomarker for anti - epidermal growth factor receptor antibody therapy in metastatic colorectal cancer . 
negative results were dened as those with no staining ( score , 0 ) or faint or barely perceptible membranous staining ( score , 1 + ) in less than 10% of the invasive tumor cells . 
equivocal results were dened as those with weak to moderate complete , basolateral , or lateral membranous reactivity in at least 10% of invasive tumor cells ( score , 2 + )  . her2 amplication by fluorescent in situ hybridization her2 uorescent in situ hybridization was also performed in some patients , and her2 amplication was dened as an overall ratio of 2.0 or greater with an average her2 copy number of greater than 4.0 signals per cell ; an overall ratio of 2.0 or greater with an average her2 copy number of less than 4.0 signals per cell ; an average ratio of 2.0 or greater with an average her2 copy number of 4.0 or more but less than 6 signals per cell ; or an average ratio of less than 2.0 with an average her2 copy number of 6.0 or more signals per cell . the patient died before return of results insurance denial patient elected to receive a different treatment the patient was not seen back at mdacc after genomic testing 16% not eligible to enroll in her2 - targeted clinical trials 40% possible future option equivocal result fig a1 . 
dignam , phd2 in this precision oncology era , where molecular proling at the individual patient level becomes increasingly accessible and affordable , more and more clinical trials are now driven by biomarkers , with an overarching objective to optimize and personalize disease management . 
as compared with the conventional clinical development paradigms , where the key is to evaluate treatment effects in histology - dened populations , the choices of biomarker - driven clinical trial designs and analysis plans require additional considerations that are heavily dependent on the nature of biomarkers ( eg , prognostic or predictive , integral or integrated ) and the credential of biomarkers performance and clinical utility . 
here we provide a concise overview of design options for both the setting of singlebiomarker / single - disease and the setting of multiple - biomarker / multiple - disease types . 
we focus on explaining the trial design and practical considerations and rationale of when to use which designs , as well as how to incorporate various adaptive design components to provide additional exibility , enhance logistical efciency , and optimize resource allocation . 
2019 by american society of clinical oncology introduction in the past 10 to 15 years , cancer clinical trials have experienced some important paradigm changes to embrace the era of precision oncology as dened by various biomarkers . 
the central hypothesis driving this movement is that by integrating the right biomarker information we can properly select , or at least enrich , trial cohorts for patients who are most likely to benet from a particular therapy . 
multiple factors collectively contribute to this movementour knowledge about oncogenic pathways has been greatly advanced ; highthroughput screening and other drug discovery developments have made a lot more candidate agents available for evaluation ; and the rapid development of various omics - based technologies , especially the increasing availability of next - generation genomic sequencing , makes it more feasible and affordable to incorporate biomarker information into clinical trials . 
all of these call for novel biomarker - driven trial designs to expedite the clinical development of multiple treatment agents and newly dened patient populations . in this review , we use biomarker to generically describe any characterizations of biologic molecules or diagnostic tests carried out on dna , rna , proteins , and metabolites from blood , body uids , or tissues for diagnosis purposes including disease conrmation , staging , subtyping , and so on . 
under this working denition , the presence of some actionable mutation , such as a mutation in epidermal growth factor receptor ( egfr ) measured at the protein level , is viewed as a single biomarker ; a dna - based multiplex genotyping that simultaneously determines multiple actionable mutations such as egfr , kras , or eml4 - alk is viewed as multiple biomarkers . treatment benet compared with the traditional paradigm , there are even greater consequences of asking the right questions ( or wrong questions ) in these biomarker - driven clinical trials . 
for example , although often there is good biologic rationale to consider biomarker - negative ( m - negative ) patients unlikely or less likely to benet from the new ( targeted ) therapy , the clinical evidence of whether is conned only in the potential biomarker - positive ( m - positive ) patients may or may not be strong . 
moreover , the development of a validated companion biomarker , including establishing a widely accepted partition or cutoff value to determine whether the biomarker is positive or negative , is sometimes lagging behind the development of novel therapeutic agents . 
 hu and dignam context key objective in the past few decades , clinical trials have experienced a major paradigm shift , aiming to incorporate ever - growing tumor biomarker information and evaluate biomarker - dened patient cohorts , while accelerating the clinical development process simultaneously . 
what are the key considerations when designing and conducting biomarker - driven clinical trials ? knowledge generated we present an overview of the rationale , trial types , key design elements and features , and practical considerations for commonly used biomarker - driven clinical trials . 
examples of trials conducted and the lessons learned are also presented . relevance when properly designed and implemented with adequate resources , biomarker - driven clinical trials may efciently and effectively generate evidence on biomarker - based personalized disease management . 
clinicians and clinical trialists should think thoroughly and critically if and how to design and conduct these trials . properly tailor the trial designs and prioritize research questions on the basis of the development stage of the biomarker and the credentials of its clinical utility . the demand for trial development and conduct has become more daunting than ever , as high - throughput molecular proling becomes more accessible . 
rather than mounting separate trials , an important paradigm shift to expedite clinical development is to establish the so - called master protocol or platform triala program of trial development and conduct implemented with an up - front molecular screen and enrollment infrastructure into subtrials across multiple biomarkers and / or multiple disease typesto enhance logistic and regulatory efciency . some important and useful concepts in development of biomarkers for clinical utility are rst briey introduced here and expanded on in the next sections . 
throughout this review , we assume biomarkers of interest already have good analytical validity ( eg , they can be accurately , reliably , and reproducibly measured ) .1 , 2 a biomarker is called prognostic if it is associated with disease prognosis regardless of treatment type and is called predictive when it exerts prognostic inuence differentially according to different treatments . 
it is desirable to have a biomarker ( either prognostic or predictive ) with good clinical utility ( ie , the biomarker can reliably prompt clinical actions that benet patients )  . 
according to dancey et al , 3 biomarkers are integral when they are inherent in the study design from the onset and must be performed in real time to establish eligibility , identify the correct stratum for stratied enrollment , or assign treatment . 
in other words , to make a biomarker usable for clinical trial setting , an integral biomarker should be fully developed and validated ( eg , the cutoff that dichotomizes the continuous marker measurement is xed ) , with a rapid assay turnaround time . 
fast assay turnaround time is desirable but not required for integrated biomarkers . to design more efcient trials and overcome the aforementioned challenges , the idea of adaptive designs has been promoted , and aspects of this approach play an important role in virtually all existing biomarker - driven trials . although modern oncology trial design has promoted adaptive designs as a new aspect of clinical trials , we note that adaptive elements have played a long - standing role in oncology clinical trials , dating back to early multistage design concepts4 , 5 and continuing in the rich development of group sequential monitoring methods that permit early efcacy or futility stopping.6 also , both traditional and newer phase i oncology trial designs are by their nature adaptive to accumulating data . 
we will discuss the rationale and features of established as well as newer adaptive design elements as they arise in respective biomarker - driven trial designs . finally , a new nomenclature that generally describes trial constructs has been introduced , attempting to describe heuristically the structure , particularly when multiple biomarkers and / or treatment agents are considered . 
the term basket trial refers to a trial with an agent tested among multiple disease types sharing a common molecular feature or target identied by biomarker ( s )  . 
in contrast , an umbrella trial describes the case where , for a common disease entity , multiple agents may be investigated in conjunction with specic molecular targets and biomarkers . 
we note that all of these terms lack precision , and thus the specic study features will provide more detail as to the structure . this article aims to provide a concise and up - to - date overview on the current status of biomarker - driven clinical trials , with a focus on the underlying design considerations , rationale , and lessons learned . 
we organize these discussions in terms of the biomarkers role ( integral v integrated ) , number of biomarkers involved ( one v multiple ) , and trial objective ( conrmatory v discovery )  . 
interim monitoring , including but not limited to group sequential methods , provides the statistical framework to allow repeated assessments of treatment efcacy and early stopping as soon as the accumulated data already provide adequate evidence to conclude that the experimental regimen is highly likely ( efcacy monitoring ) or unlikely ( futility monitoring ) benecial . 
for example , phase ii trials traditionally have implemented a single - arm , noncomparative design , with a planned interim futility analysis , such as simons two - stage design , 7 to minimize patient exposure to ineffective regimens . 
in the late - phase setting , integrated randomized phase ii / iii design8 is a useful adaptive design that combines both screening ( phase ii component ) and conrmatory ( phase iii component ) in a single trial . 
as the data based on the the overall phase ii component are used to provisionally test the study hypothesis of the phase iii component , integrated phase ii / iii designs can effectively be viewed as phase iii studies with rather aggressive ( ie , likely to stop ) interim futility analyses . if more than one experimental regimen is of interest in the phase ii component , a plan of selecting treatment arms can also be incorporated when making the go / no - go decision from phase ii to phase iii . more formally speaking , adaptive designs are those that allow prospectively planned modications in both the statistical and scientic aspects of study designs , on the basis of accumulating data while the trials are still progress.9 adaptations to the statistical aspects of study designs arise when the primary estimand ( eg , the target of estimation ) addressing the scientic question of interest10 remains unchanged ; examples include group sequential designs , 6 sample size adaptation , 11 and , more recently ( although the concept dates back several decades ) , outcome / response - adaptive randomization.12 - 14 adaptations to the scientic aspects of study designs occur when the primary estimand does change ( eg , enriching patient population , or selecting new treatment arms or end points while the trial is still ongoing )  . 
among these adaptive design features , group sequential theorybased interim analysis and treatment assignment modication ( such as add or drop arms ) have been used most frequently , whereas other adaptive design features have not been widely adopted in practice . 
if the new agent is expected to have little effect on tumor shrinkage , or must be combined with an active agent , randomized phase ii screening designs17 with end points such as progression - free survival may be considered and provide valuable information on whether a conrmatory , randomized phase iii enrichment design should be performed . 
of note , although enrichment designs should be efcient ( a small sample size ) because we anticipate a large effect size , if the prevalence of mpositive patients is low , many patients must be screened to obtain the necessary sample size ; if the prevalence is too low , the trial may simply be infeasible . when there is strong evidence suggesting the biomarker is predictive with respect to the experimental regimen ( ie , m - positive patients benet ) , but it remains unclear whether the new treatment may also have a clinically meaningful ( but likely smaller ) benet for m - negative patients , the socalled biomarker - stratied design , which randomly assigns all patients with a valid marker result ( m - positive and m - negative ) as a stratication factor , can be considered ( fig 1b )  . 
one can also view this as an umbrella trial ( dened in a later section ) that contains two separate rcts for m - positive and m - negative subgroups . 
the key design consideration for conrmatory trials is if and how to prioritize the multiple hypotheses within the m - positive subgroup , the m - negative subgroup , or the overall population and properly power for each separately as applicable . 
 a biomarker - driven oncology clinical trial designs biomarker assay biomarker assay m - negative m - positive m - negative m - positive off study randomize randomize randomize standard rx new rx standard rx new rx standard rx new rx biomarker assay randomize biomarker assay nonmarkerbased strategy marker - based strategy marker subgroup 1 marker subgroup 2 marker subgroup 3 new rx randomize standard rx randomize new rx v standard rx standard rx m - negative , standard rx m - positive , new rx standard rx new rx fig 1 . 
m - negative , biomarker - negative ; m - positive , biomarker - positive ; rx , treatment . strategy can be considered by rst testing the m - positive subgroup at signicance level and then testing the m - negative subgroup at the same level if and only if the rst test is statistically signicant.20 an alternative approach to reect such prioritization is to split the overall unequally with a bonferroni correction ( eg , 1 = 0.04 and 2 = 0.01 for m - positive and m - negative , respectively )  . ( cid : 129 ) if the effect in the overall population is of secondary interest , the aforementioned sequential procedure needs to be modied , because the treatment effect of the overall population can still seem to be clinically meaningful even when the new treatment only works in the in the m - negative m - positive subpopulation but not subpopulation at all . 
to mitigate the potentially misleading conclusion that treatment works in all comers ( m - positive and m - negative ) , the marker sequential test design21 was proposed , which rst tests the m - positive subgroup at a reduced signicance level 1 ( , ) : if the test yields a statistically signicant result , the m - negative subgroup will be tested at level , whereas the overall population will be tested at 1 if the test among the m - negative subgroup is not signicant . ( cid : 129 ) if there is no convincing evidence suggesting a particular biomarker is predictive , a fallback strategy can be used , which rst tests the overall population at 1 ( , ) : if the result is signicant , one can claim that the treatment is effective in all patients ; if it is not signicant , then the m - positive population must meet 1 for signicance.22 although biomarker - stratied designs are typically used in the context of a conrmatory phase iii setting , randomized phase ii screening designs may still be considered if the overarching goal is to efciently inform whether to conduct a randomized phase iii enrichment design . 
when the primary interest is to evaluate whether the biomarker - based treatment assignment strategy is more effective than nonbiomarker - based treatment assignment strategy , one may consider a biomarker - strategy design , which randomly assigns all patients ( m - positive and m - negative ) to receive treatments either on the basis of or independent of biomarker status ( fig 1c )  . 
this design may also be used to evaluate whether the biomarker is predictive with some efciency loss , 16 , 23 because there can be a signicant portion of patients with the same biomarker status receiving the same treatments in both arms , reducing the treatment effect size that can realistically be specied . biomarker - directed design may be considered when it is desirable to have an integral biomarker evaluation for all patients , and there is compelling existing evidence suggesting a particular biomarker - dened subgroup should receive a certain regimen with satisfactory efcacy and safety proles ( fig 1d )  . 
in this case , like enrichment designs , a biomarker - directed design only randomizes the biomarker - dened subgroup where the biomarkers clinical utility in directing treatment decisions remains unclear ; meanwhile the other biomarker - dened subgroups are treated deterministically . 
for in tailorx ( program for the assessment of example , clinical cancer tests [ pacct - 1 ] : trial assigning individualized options for treatment ) , 24 patients with breast cancer treated with tamoxifen were classied as low , intermediate , and high risk on the basis of a 21 - gene recurrence score ( oncotype dx , genomic health , redwood city , ca )  . 
patients with intermediate risk were randomly assigned to receive hormonal therapy with or without chemotherapy , whereas lowrisk patients and high - risk patients always received only hormonal therapy with chemotherapy , respectively . in these conrmatory integral biomarker - driven trials , interim monitoring , especially futility monitoring , plays an even more critical role to help prioritize the limited resources by dropping subgroups with unpromising or unresponsive treatment benet and / or dropping ineffective experimental regimens if more than one is being investigated . 
for a biomarker classier that is based on a multiplex assay of genomic , proteomic , and transcriptomic data , the adaptive signature design29 was proposed to evaluate whether the experimental regimen is effective in the overall population or a subset of patients only while developing the biomarker classier simultaneously . 
if the treatment comparison for all patients is not signicant in the overall population at 1 ( , ) , we will either split all patients into training and testing subsets or use k - fold cross - validation30 to develop the biomarker and then evaluate efcacy in identied subgroups . 
of note , the cross - validated approach has also been shown to substantially improve the power of identifying the m - positive subgroup that benets from the new treatment . 
by transforming the multiple candidate genes to a binary classier , the approach does not suffer too much with respect to type i error control as the dimension of genes increases . 
when a biomarker or gene signature can be quantied on a continuous or ordinal scale , we can consider the biomarker - adaptive threshold design31 using a similar strategy to identify and validate an optimal cutoff point that separates m - positive and m - negative subgroups . the use of bootstrap resampling for estimation and inference of the threshold , although accounting for the multiplicity issue due to combining the tests for subgroup m - positive and overall population , has been shown to preserve the power to detect a global treatment effect while developing the biomarker . 
comparing with the conventional approaches , these methods have been shown to substantially improve the likelihood of detecting the mpositive subgroup when differential treatment effect does exist , especially when the prevalence of m - positive is low . 
for example , after the approval of vemurafenib for brafv600 mutation - positive metastatic melanoma , a nonrandomized phase ii basket trial of vemurafenib for multiple nonmelanoma cancers with brafv600 mutation was conducted , 33 with objective response as the primary end point . from a trial conduct perspective , basket trials can be more efcient than multiple histology - specic enrichment trials to carry out conducted separately and are convenient because the biomarker can ( although not necessarily ) be assessed locally at participating sites as part of the eligibility criteria screen . 
furthermore , this trial design can be quite appealing to patients because it conveniently provides access to the experimental therapy across multiple disease types , including in settings where our understanding of biomarker - treatment relationship is relatively limited . 
 molecular target a molecular target b molecular target y molecular target z targeted therapy a standard therapy targeted therapy b standard therapy targeted therapy y standard therapy targeted therapy z standard therapy biomarker - driven oncology clinical trial designs targeted therapy x tumor type a tumor type b tumor type y tumor type z biomarker assays phase iii continue to follow for definitive end point accrue additional n2 patients for definitive end point primary analysis treatment effect sufficiently large initiate phase ii trial phase ii accrue n1 patients assess stop insufficient ie activity promising ie activity run - in : randomization ( p1 = p2 ) randomization arm 1 ( p1 ) v arm 2 ( p2 ) assess interim estimate of treatment effect stop and conclude new rx better treatment effect not sufficiently large arm 1 better arm 2 better increase p1 decrease p2 increase p2 decrease p1 fig 2 . 
 hu and dignam from a scientic perspective , the underlying rationale of conducting a basket trial is that the biomarkers presence may independently predict responses attributed to the corresponding targeted therapy , regardless of histology or disease type.34 if this truly holds , it would be reasonable to redene cancer in a histology - agnostic fashion , suggesting an exciting new approach to therapy development . 
for example , in may 2017 , the us food and drug administration approved pembrolizumab for any patients with microsatellite instabilityhigh / decient dna mismatch repair regardless of histology.35 this approval was the rstever histology - agnostic indication and was partly based on a small , proof - of - concept basket trial.36 because basket trials may be viewed as a collection of enrichment trials , they also inherit all of the advantages and disadvantages , with the same practical considerations as elaborated earlier . 
one unique challenge facing basket trials is the balance between feasibility and the exchangeability ( eg , histology agnostic ) hypothesis , given the potential heterogeneity across different disease types . 
that is , if and when can we assume the molecular proling is sufcient to replace histology and pool patients together with the same biomarker ? for many biomarkers , prevalence is so low that it may be infeasible to accrue enough patients and analyze by each disease type . 
meanwhile , pooling all patients with the same biomarker can be questionable if not at all unrealistic , because the approach implies we can completely ignore the prognosis heterogeneity across different histology and assume disease subtype is not prognostic at all . 
in the case of vemurafenib for patients with brafv600 mutations , response to treatment was high when the primary site was melanoma but low when the primary site was colorectal cancer.33 a practical compromise is to combine some disease types for which prevalence is signicantly lower than others . 
in le et al , 36 patients with microsatellite instability high / decient dna mismatch repair were accrued and analyzed by colorectal and noncolorectal cohorts separately , because the prevalence in colorectal cancer is notably higher than other disease types . several novel adaptive designs have been developed to avoid separate analyses and properly share response information across disease types . 
one approach is based on preplanned interim analyses to determine the next steps.37 for example , if there is adequate evidence suggesting some histology - specic cohorts have similar and promising activities , these cohorts will be aggregated to allow more efcient statistical inference with fewer patients ; otherwise , histology - specic cohorts with exceptionally favorable response will remain separate , and cohorts with low responses will be terminated . 
the other approach is based on statistical modeling and bayesian inference , 38 , 39 which explicitly allows information sharing across different histology - specic cohorts and permits early stopping for some cohorts naturally on the basis of posterior probability of histology - specic response rates . 
nonetheless , it was argued that , for sample sizes typically used in phase ii trials and a reasonable number of cohorts / histology types under investigation , these designs that are meant to share information may not be as useful as one would hope , unless there is a strong rationale and evidence indicating uniform responses across cohorts.40 another important consideration when designing discovery basket trials is whether randomization should be used or not . 
the nonrandomized basket trial may be clearly preferred because of its feasibility and close connection to the conventional single - arm phase ii design traditionally used in early - stage development . 
however , nonrandomized basket design practically mandates objective response to be the only choice of the primary end point , because it is generally considered the only interpretable efcacy end point without a comparator . 
even with this end point , concerns may still arise regarding the relevance of historical control in at least some histology cohorts , because the biomarker likely denes a new disease subtype for which there is little or no historical information on prognosis.41 furthermore , if the experimental regimen is to be administered in combination with other active regimens , how to isolate the impacts of background treatments and properly the experimental regimens role can be chalinterpret lenging . 
in this case , because a centralized molecular screening platform is typically used , one may also view them as umbrella trials . from a pure statistical perspective , one could argue that basket trials may have multiplicity issues , because we simultaneously evaluate multiple histology - specic cohorts . pragmatically speaking , this may not be that problematic , because we are more tolerant of a higher type i error for discovery purposes ; the same issue also exists if we conduct separate trials for each cohort , and more practical concerns such as accrual feasibility often outweigh the type i error control . 
a randomized phase ii / iii trial example is alchemist ( adjuvant lung cancer enrichment marker identication and sequencing trial ) for resectable nonsmall - cell lung cancer ( nsclc ) , 42 , 43 which consists of three treatment subtrials , alchemistegfr for patients with egfr mutation ( clinicaltrials.gov identier : nct02193282 ) , alchemist - alk for patients with alk rearrangements ( clinicaltrials.gov identier : nct02201992 ) , and anvil ( clinicaltrials.gov identier : nct02595944 ) for unmatched patients ( eg , squamous histology , or nonsquamous histology and neither egfr mutation nor alk rearrangements )  . an observation cohort is also available for unmatched patients who refuse to participate in anvil . 
another prominent example is lung - map ( clinicaltrials.gov identier : nct02154490 ) , 44 which was initially for squamous lung cancer but recently was amended for all types of advanced nsclc . 
using sequential development features such as phase ii / iii designs and interim analyses that permit adaptation to ndings , these trials adaptively provide the necessary exibility for the umbrella trial objectives as a whole ( fig 2c )  . when there are multiple candidate regimens that are of interest equally for some or all biomarker cohorts , umbrella trials also can be designed solely for discovery objectives . 
for example , in the battle - 1 ( clinicaltrials.gov identier : nct00411632 , nct00409968 , nct00410059 , nct00410189 , nct00411632 , nct00411671 ) trial , patients with chemotherapy - refractory nsclc were assayed for four candidate biomarkers to be allocated to a total of ve marker strata ( including one nonmatched ) and then randomly assigned to one of four drug regimens.15 in nrglu003 ( clinicaltrials.gov identier : nct03737994 ) , an umbrella trial of previously treated patients with alk - positive lung cancer , a total of 10 marker cohorts ( including an unmatched cohort ) and up to seven new - generation alk inhibitors are to be evaluated . 
however , as the total number of possible drug - marker strata increases , the likelihood to accrue enough patients to have a reasonably accurate estimate of efcacy for each drug - biomarker stratum decreases . 
by exploiting the fact that biomarker allocation is not informative for treatment assignments , battle - 1 considered a learn - as - go approach by explicitly using a bayesian hierarchical probit model for information sharing , 45 along with outcome - adaptive randomization , 12 , 46 which allocates more patients to drug - marker strata that are more likely to have exceptional activities , to potentially provide individuals with more efcacious treatments and improve estimation precision ( fig 2d )  . 
in nrg - lu003 , for each biomarker the investigators are able to determine and prioritize the experimental regimens of interest on the basis of preclinical data , which substantially reduces the total number of drug - biomarker strata to be evaluated . 
freidlin and korn40 suggested that under typical phase ii trial design settings , both approaches may require similar resources . one implication of conducting umbrella trials is that an explicit rule governing how to match biomarkers and candidate regimens needs to be specied prospectively . 
therefore , umbrella trials also provide a unique opportunity to evaluate whether a rule - based policy that matches biomarkers and drugs is effective at all and , if so , to what extent across all genomic characterizations . 
to make such evaluation interpretable , the rule - based assignment policy should be as stable as possible during the trial conduct and ideally cover a wide range of biomarker - drug combinations.47 another unique consideration with umbrella trials is that a patient could be eligible for multiple biomarker cohort allocation because the tumor contains multiple biomarkers . 
with the emergent use of molecular proling , basket trials and umbrella trials , as well as extensions discussed here , can be collectively called master protocols or platform trials . 
more importantly , such a protocol provides substantial exibility in terms of discontinuing unpromising investigations , carrying forward favorable early results to denitive testing in a phase ii / iii framework , and introducing new subtrials as targets and agents are identied in a perpetual manner , using the aforementioned adaptive design methods for single - biomarker settings.48 in addition , the infrastructure advantages of conducting master protocols , such as centralized and streamlined trial conduct ( enrollment , informed consent ) , data collection , governance ( institutional review board , data and safety monitoring committee ) , and quality assurance ( clinical monitoring , imaging reading ) , are subtrials stantial as compared with conducting individual separately . 
when it was activated in 2015 , it started with 10 parallel biomarker - based cohorts to evaluate eight different in may 2016 , a preplanned feasibility interim analysis revealed that only 9% of patients had actionable mutations that could be matched with any of the multiple targeted therapies under investigation . 
the lower - than - expected matching success rate led to a major amendment to improve the overall matching rate by adding additional marker - specic cohorts.49 in june 2017 , when the original screening target was met ( n = 6 , 000 ) , it was found that the common molecular subtypes were rarer than expected.50 the study therefore underwent another major amendment by collapsing multiple subtype cohorts and relaxing the screening process . 
to date , the study remains open to accrual , with a total of 19 cohorts to evaluate 13 drugs.51 four lung - map was originally designed in 2014 for advanced squamous nsclc , consisting of targeted therapy subgroups and one nonmatched subgroup , each using a phase ii / iii seamless design , with progression - free survival and overall survival as primary end points , respectively.52 since 2015 , the treatment landscape of advanced nsclc has changed tremendously because of a series of approvals in immunotherapies especially for squamous and nonsquamous nsclc by the us food and drug administration , which fundamentally changed the standard of care and the study control arms . 
after multiple minor amendments for adding and closing biomarker - specic subtrials , in 2018 the study was completely revamped by expanding eligibility to all histology of advanced nsclc , using a new screening protocol and introducing new biomarker - dened subtrials.53 in summary , although conceptually offering efciency and exibility , master protocols are more prone to various factors that are unknown ( eg , low biomarker prevalence ) or cannot be foreseen ( eg , changing treatment landscape ) at the trial inilogistical tiation . 
these trials also come with substantial complications , especially when several sponsors are involved who may have conicting proprietary interests and regulatory concerns . discussion biomarker - driven clinical trials allow us to investigate patient heterogeneity on the basis of molecular proling , which consequently introduces new opportunities and challenges . 
comparing with the conventional paradigm , these trials require even more thorough planning and comprehensive evaluation on the overarching objectives ( discovery or conrmatory ) , the credential of biomarkers clinical utility , choice of adaptive design and analysis plans , knowledge of cancer biology , existing data from preclinical and early clinical trials , prevalence of each subtype population , logistic readiness to conduct immortal clinical trials , and so on . 
the success of any biomarker - driven trials therefore certainly relies on an even closer collaboration involved in advancing cancer care , including among all clinical investigators , statisticians , sponsors , regulators , drug and assay developers , and patient advocates . our discussions have been limited to phase ii and iii trial designs for discovery and conrmatory purposes . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / author - center . chen hu consulting or advisory role : merck sharp & dohme james j . 
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lih cj , sims dj , harrington rd , et al : analytical validation and application of a targeted next - generation sequencing mutation - detection assay for use in treatment assignment in the nci - mpact trial . 
peeters m , jay price tj , cervantes a : randomized phase iii study of panitumumab with uorouracil , leucovorin , and irinotecan ( folfiri ) compared with folfiri alone as second - line treatment in patients with metastatic colorectal cancer . 
herbst rs , redman mw , kim es , et al : cetuximab plus carboplatin and paclitaxel with or without bevacizumab versus carboplatin and paclitaxel with or without bevacizumab in advanced nsclc ( swog s0819 ) : a randomised , phase 3 study . 
spigel dr , ervin tj , ramlau ra , et al : randomized phase ii trial of onartuzumab in combination with erlotinib in patients with advanced non - small - cell lung cancer . 
bradley jd , paulus r , komaki r , et al : standard - dose versus high - dose conformal radiotherapy with concurrent and consolidation carboplatin plus paclitaxel with or without cetuximab for patients with stage iiia or iiib non - small - cell lung cancer ( rtog 0617 ) : a randomised , two - by - two factorial phase 3 study . 
vansteenkiste jf , cho bc , vanakesa t , et al : efcacy of the mage - a3 cancer immunotherapeutic as adjuvant therapy in patients with resected mage - a3positive non - small - cell lung cancer ( magrit ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
cobo m , isla d , massuti b , et al : customizing cisplatin based on quantitative excision repair cross - complementing 1 mrna expression : a phase iii trial in nonsmall - cell lung cancer . 
 poly ( adp - ribose ) polymerase inhibitor activity in prostate cancers harboring mutations in dna repair genes : who benets ? shridar ganesan , md , phd1 and judy garber , md , mph2 the seminal nding that cancers harboring mutations in brca1 or brca2 are often exquisitely sensitive to poly ( adp - ribose ) polymerase ( parp ) inhibition has led to the successful development of parp inhibitors as effective targeted therapies for brca1 / 2 - mutated ovarian , breast , prostate , and pancreatic cancers.1 - 7 because many other genes are indirectly or directly involved in the brca1 / 2 - associated homologous recombination ( hr ) mediated dna repair ( hrd ) pathway , there has been a great deal of interest in rationally expanding the use of parp inhibitors to include cancers harboring mutations in these related dna repair genes.8 , 9 these include genes intimately associated with the brca1 / 2 hrd pathway , such as palb2 , bard1 , brip1 , and the rad51 paralogs , as well as genes less directly involved in hrd , such as atm and chek2 . 
is there evidence of biallelic loss of function of the gene in the tumor ? both of these criteria would presumably be required for a tumor to manifest a defect in hr - mediated repair sufciently profound to lead to sensitivity to parp inhibitors . 
the second criterion is especially important because , for many dna repair genes , the heterozygous state has at most a subtle repair phenotype that would not impart sensitivity to parp inhibitors . 
even if a lossof - function mutation in a critical dna repair gene is detected in a tumor , there must also be loss of the wildtype allele or , rarely , a dominant negative heterozygous mutation or evidence of epigenetic silencing of the wildtype allele for the tumor to have a profound dna repair defect . 
similarly , for each gene considered as a biomarker of sensitivity to parp inhibitors , data regarding the functional effect of biallelic loss on the hrd pathway and subsequent relative sensitivity to parp inhibitors need to be carefully evaluated . this leads us to the recently published randomized phase iii profound study ( clinicaltrial.gov identier : nct02987543 ) of the efcacy and safety of olaparib in men with metastatic castration - resistant prostate cancer harboring germline mutations in a set of dna repair genes who experienced disease progression on initial hormonal treatment.10 all patients had an alteration in one of 15 genes ( brca1 , brca2 , atm , brip1 , bard1 , cdk12 , chek1 , chek2 , fancl , palb2 , ppp2r2a , rad51b , rad51c , rad51d , and rad54l ) and were randomly assigned in a 2 : 1 fashion to receive either the parp inhibitor olaparib or physicians choice of second - line hormonal therapy with enzalutamide or abiraterone . 
the trial was divided into two cohorts , with cohort a ( n = 245 ) having an alteration in brca1 , brca2 , or atm , and cohort b ( n = 142 ) having alterations in any of the other 12 genes . 
the key question is whether the benet of olaparib treatment seen in both cohort a and cohorts a and b overall is driven primarily by benet in patients with brca2 mutations in both instances . 
here again , analysis of high - depth sequencing data may be able to identify which brca1mutant prostate cancers have undergone loss of heterozygosity with loss of wild - type brca1 allele and are thus truly sensitive to parp inhibitors.13 some individual gene analyses were presented as exploratory analyses as well . 
cancers with mutations in rad51b and rad54l , which are genes directly involved in hrd , had some evidence of benet , but numbers are small ( see supplementary figure s6 in de bono et al10 )  . 
the rest of the genes , including palb2 , bard1 , brip1 , fancl , chek1 , rad51c , and rad51d , conferred eligibility on fewer than ve randomly assigned patients each and cannot be assessed . these data suggest that brca2 - mutant prostate cancers denitely benet from olaparib treatment , and this is a clear advance in the treatment of this subset of prostate cancers . however , it may well be that the benet seen in the brca2mutant population is driving the overall benet seen in both cohort a and the combined group of cohorts a and b in this study . 
the reason for lack of a clear signal in atm - mutant prostate cancer needs to be further investigated , and analysis of both allelic status of the mutations and molecular evidence of patterns of genomic instability associated with hrd may help resolve these issues . 
several reports have shown that atm - mutant breast cancers may not respond to parp inhibitors , 14 , 15 suggesting that atm mutation may not confer clinical sensitivity to parp inhibitors . 
different therapeutic strategies may be required to effectively treat atm - mutant prostate cancers , and other rational treatments , such as atr inhibitors , need to be investigated.16 the lack of clear signal of benet in prostate cancers harboring brca1 mutations may be a result of the small numbers and the fact that , unlike breast , ovarian , and pancreatic cancers , many brca1 - mutant prostate tumors often do not show evidence of biallelic alteration.11 , 17 although there are hints of benet in cancers harboring mutations in other genes critical for hr , including the rad51 paralogs , the numbers in this trial are too small to make any denitive conclusion . 
for example , palb2 and rad51 paralogs clearly play a central role in hrd , and there are data demonstrating that palb2 mutation in breast and prostate cancer and rad51 paralog mutation in ovarian cancer are associated with benet from parp inhibitors.14 , 15 , 18 - 20 evaluation of the landscape of other hrd gene mutations in different cancer types and data regarding the settings in which there is strong evidence of biallelic loss may help guide development of these genes as biomarkers for parp inhibitors . in designing future trials that rationally target specic dna repair defects in cancer , simply identifying a pathogenic mutation in a broad set of genes in the tumor or in germline may not be sufcient to dene the population likely to benet . 
clear evidence that loss of function of each gene of interest confers high - level sensitivity to the drugs being evaluated needs to be presented , and the allelic status of the gene in the tumor may need to be assayed . 
in some settings , such as ovarian and breast cancer , the nding of a pathogenic brca1 or brca2 mutation , either germline or somatic , is almost always associated with evidence of biallelic mutations , but in other cancers and with other dna this may not necessarily be the case.17 repair genes , evaluation of allelic status can be approached by computational methods , but there may be settings , including epigenetic silencing and dominant negative alleles , where this approach will need to be complemented by functional assays of genomic instability . 
here , assays using wholegenome sequencing or targeted sequencing may also be informative in determining whether the presence of a dna repair gene mutation is accompanied by mutation patterns consistent with a profound defect in hrd.21 - 23 the presence of reversion mutations or mutations in compensating genes also can affect sensitivity to parp inhibitors and may need to be considered.24 , 25 in summary , a more sophisticated approach to analysis of dna repair status of cancers , which includes not only identifying the presence of a pathogenic mutation , but also demonstrating that there is loss of the wild - type allele , lack of reversion mutation , and / or genomic evidence of a profound dna repair defect , may be required to optimally identify cancers that may benet from parp inhibitors and related dna - damaging agents . 
grouping together a set of related genes for pooled analysis may , given differences in prevalence of individual mutations and effect size of benet for different genes , lead to settings where the overall benet in the pool may be driven only by a subset of genes . 
if this possibility is not considered , pooled analysis could lead to approval of therapies for gene alterations when these therapies are ineffective and prevent or delay development of more effective targeted therapies for those patients . 
gene - level analysis may make trial design more difcult , but ultimately , it may lead to more precise use of therapies that target specic dna repair defects or other loss - of - function alterations in cancer . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / authors / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis , roche , foghorn therapeutics , foundation medicine , merck sharp & dohme research funding : m2gen ( inst ) patents , royalties , other intellectual property : i hold 2 patents for digital imaging that may be licensed to ibris and inspirata other relationship : national cancer institute / national institutes of health judy garber consulting or advisory role : novartis ( i ) , gtx ( i ) , helix biopharma , konica minolta , aleta biotherapeutics ( i ) , h3 biomedicine ( i ) , kronos bio ( i ) research funding : novartis ( i ) , ambry genetics , invitae genetics , myriad genetics other relationship : susan g . 
n engl j med 361 : 123 - 134 , 2009 gonz alez - martn a , pothuri b , vergote i , et al : niraparib in patients with newly diagnosed advanced ovarian cancer . 
n engl j med 381 : 2391 - 2402 , 2019 kaufman b , shapira - frommer r , schmutzler rk , et al : olaparib monotherapy in patients with advanced cancer and a germline brca1 / 2 mutation . 
moore kn , secord aa , geller ma , et al : niraparib monotherapy for late - line treatment of ovarian cancer ( quadra ) : a multicentre , open - label , single - arm , phase 2 trial . 
lancet oncol 20 : 636 - 648 , 2019 litton jk , rugo hs , ettl j , et al : talazoparib in patients with advanced breast cancer and a germline brca mutation . 
n engl j med 379 : 753 - 763 , 2018 golan t , hammel p , reni m , et al : maintenance olaparib for germline brca - mutated metastatic pancreatic cancer . 
sokol es , pavlick d , khiabanian h , et al : pan - cancer analysis of brca1 and brca2 genomic alterations and their association with genomic instability as measured by genome - wide loss of heterozygosity . 
sakamoto s , iijima k , mochizuki d , et al : homologous recombination repair is regulated by domains at the nand c - terminus of nbs1 and is dissociated with 13 . 
khiabanian h , hirsheld km , goldnger m , et al : inference of germline mutational status and evaluation of loss of heterozygosity in high - depth , tumor - only atm functions . 
gruber jj , afghahi a , hatton a , et al : talazoparib beyond brca : a phase ii trial of talazoparib monotherapy in brca1 and brca2 wild - type patients with advanced her2 - negative breast cancer or other solid tumors with a mutation in homologous recombination ( hr ) pathway genes . 
tung nm , robson me , ventz s , et al : tbcrc 048 : a phase ii study of olaparib monotherapy in metastatic breast cancer patients with germline or somatic mutations in dna damage response ( ddr ) pathway genes ( olaparib expanded )  . 
yap ta , ocarrigan b , penney ms , et al : phase i trial of rst - in - class atr inhibitor m6620 ( vx - 970 ) as monotherapy or in combination with carboplatin in patients with advanced solid tumors . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
chandran ea , kennedy i : signicant tumor response to the poly ( adp - ribose ) polymerase inhibitor olaparib in heavily pretreated patient with ovarian carcinosarcoma harboring a germline rad51d mutation . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deciency among breast cancer subtypes . 
telli ml , timms km , reid j , et al : homologous recombination deciency ( hrd ) score predicts response to platinum - containing neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
 specifying the trueand falsepositive rates in basket trials in the clinical evaluation of anticancer therapies , after identification of a recommended dose , investigators typically seek evidence of drug efficacy in populations of patients hypothesized to benefit from it . 
the purpose of these signal - finding studies is to prioritize additional development and to determine whether drugs should be tested in randomized phase iii trials and , if so , in which populations of patients . 
because these identified populations usually are small and efficacy often is substantially better than that for available therapies , conclusions from single - arm trials of this nature can be used to inform off - label treatment decisions and sometimes lead to inclusion in treatment guidelines or regulatory approvals . 
an understanding of the performance characteristics of the novel clinical trial designs commonly used in this setting is critical to avoid inappropriate clinical decision making on the basis of false - positive clinical trial results . the group of patients in whom a therapy is hypothesized to have activity can be identified in a number of ways , including genomic and proteomic profiles , and activity of the drug can be influenced by histology or the primary tumor site . 
the combination of a hypothesized mechanism of action and uncertainty around the populations of patients who would likely benefit has encouraged a trend toward more - complex earlyphase trials.1 a major challenge is the desire to study the effects of the drug simultaneously in patients with different primary sites of disease or histologies with the goal of evaluating the efficacy of the drug in these contexts , often referred to as baskets.2 - 9 a related recent trend in clinical trial design has been increasing enthusiasm for the use of adaptive designs , whereby design parameters can be changed dynamically as the trial progresses and evidence about efficacy gradually emerges.10 a final important trend has been the use of bayesian design as a tool to evaluate the emerging evidence in a formal statistical model.11 - 15 many of these methods are predicated on the underlying expectation of broadly similar efficacy across baskets because the statistical model allows the sharing of information across baskets with the purpose of completing the trial in a shorter time frame with fewer patients than a traditional strategy whereby each basket is regarded as an independent phase ii trial . 
this combination of design complexity with sophisticated statistical modeling has led to situations in which important clinical trials are being launched without a broad understanding of the implications of the novel methods used , an issue that has been identified previously in the context of novel phase i study designs.16 in this commentary , we examine the properties of a particular bayesian adaptive design that increasingly is being used in the context of basket trials , and we use the clinical setting of a completed basket trial to demonstrate that the design is heavily tilted toward positive conclusions about the efficacy of the drug.17 the complexity of these modern methods makes having a clear understanding of the properties of design , characterized by easily interpretable measures , essential when planning a new clinical trial . although bayesian statistical analyses generally focus on reporting the probability that an individual drug works ( the so - called posterior probability ) , we believe that the evaluation of properties of designs in terms of the familiar metrics used in the context of clinical trials is important . 
these properties are the true - positive rate ( the probability that a truly effective agent will be shown to be effective [ often referred to as power ] ) and the falsepositive rate ( the probability that an ineffective agent is erroneously judged to be effective [ often referred to as the type i error ] )  . 
we generally like to keep the false - positive rate low because we do not want to encourage additional study of a drug that does not work , and we want the true - positive rate to be high because we want to be confident that if the drug truly works , its effectiveness will be recognized . 
therefore , to fully understand the implications of these data - sharing methods , we must calculate a more - elaborate set of trueand false - positive rates , specifically when the drug does not work at all , when it only works in one kristen m . 
 basket , when it only works in two baskets , and so forth . as an illustration of the clinical setting , we refer to the findings of a recent basket trial that investigated the effects of vemurafenib , a selective oral inhibitor of the braf kinase.2 the trial assessed efficacy in five disease - specific baskets : nonsmallcell lung cancer , colorectal cancer , cholangiocarcinoma , erdheim - chester disease or langerhans cell histiocytosis , and anaplastic thyroid cancer . 
the investigators concluded that the drug shows promising activity in the nonsmall - cell lung cancer basket and the erdheim - chester disease or langerhans cell histiocytosis basket but that it is inactive in colorectal cancer . 
although this trial did not use the bayesian hierarchical design proposed by berry et al , 17 we use the clinical setting of the vemurafenib trial to investigate the performance of the berry design . the bayesian hierarchical model is structured to capture the correlation between the anticipated efficacies of the drug across various baskets . 
this aggregation of evidence is rooted in a key feature of bayesian methods , the prior distribution of the between - basket variability , an entity that is prespecified by the analyst . 
in the context of a basket trial , this prior distribution essentially titrates the extent to which emerging evidence of drug efficacy from one basket can be used to bolster the evidence in other baskets . 
however , they presented a sensitivity analysis that concluded that the properties are actually relatively insensitive to this choice . we evaluated the false - positive and false - negative error rates for a hypothetical trial similar in structure to the vemurafenib trial , with five baskets and null and alternative response rates of 15% and 45% , respectively . 
we simulated trials by following the bayesian hierarchical design and conducted interim analyses after the first 10 patients were accrued and then after every additional five patients until a maximum of 19 patients per basket were enrolled . 
early stopping rules terminated accrual to individual baskets if the basket - specific posterior probability that the true response rate is greater than a midlevel response rate of 30% was , 5% ( stop for futility ) or  . 
at the end of the trial , the treatment was declared efficacious in a basket if the posterior probability that the response rate that exceeded the null value of 15% was  . 
for example , in the second row ( one active basket ) , basket 1 is the one in which the drug is truly active , whereas in baskets 2 to 5 , the drug is not active . 
in this scenario , we see that a 79% chance for observing a true - positive result exists in the active basket , whereas for each nonactive basket , the false - positive rate is 18% . 
the next column on the right captures the probability that one or more of the nonactive baskets is a false - positive finding , a term usually referred to as the family - wise error rate , a key criterion for evaluating multiple hypotheses in clinical trials.18 , 19 we see that this overall false - positive rate is 37% when the drug truly works in only one basket and rises to 57% when the drug does not work in only one basket . 
although the maximum trial size was set to 95 patients , the expected trial size ranged from 59 to 84 patients , depending on the true efficacy configuration of the baskets . 
the table also lists the family - wise error rates for the setting in which each basket is regarded as an entirely independent clinical trial wherein the false - positive rate is 10% . 
each basket displays the observed response rate ( rr ) from the vemurafenib trial for a particular disease ( sample sizes in parentheses )  . ( * ) patients received combination therapy ( vemurafenib 1 cetuximab )  . 
statistical properties of bayesian hierarchical design probability drug will be declared efficacious , % family - wise error rate , % * basket 1 basket 2 basket 3 basket 4 basket 5 hierarchical independent no . 
bold represents baskets in which the drug is active ; no bold represents baskets in which the drug is not active . * the family - wise error rate represents the probability that the drug has false - positive efficacy in any one or more of the nonactive baskets ( ie , the overall false - positive rate of the design given the number of baskets in which the drug is truly active )  . 
this is shown for both the bayesian hierarchical design and the setting in which all five baskets are considered to be independent clinical trials . close examination of table 1 demonstrates two complementary results from using the bayesian design . 
although the targeted overall false - positive rate of 10% has been achieved for the setting in which the drug has no efficacy ( ie , the drug works in none of the baskets as shown in the first row ) , this standard rapidly erodes as we investigate settings in which the drug works in some baskets but not in others . for example , if we look at the two active baskets row of the table , we see a high probability ( 94% ) of declaring each of the two active baskets to be efficacious . 
consider the most extreme case ( the four active baskets row of the table ) where we see that the nonactive basket has a false - positive rate of 57% . 
in this setting , the evidence typically is dominated by strong positive results from the four baskets in which the drug is truly active , and the imposition of the prior distribution encourages the model to interpret the results from all five baskets as strongly correlated ( ie , similar in efficacy ) , which leads to a high probability that the inactive basket will be classified incorrectly as active . 
in related work , we explored in depth options for modifying the bayesian design used in our simulations by examining various choices of prior distributions and of decision rules used , demonstrating that trials can be designed on the basis of hierarchical modeling with much better control of the familywise error rates.20 we believe that straightforward reporting of the various trueand false - positive rates , as listed in table 1 , are fundamental to understanding the merits of any proposed basket study design . seemingly innocuous choices , such as the use of a prior distribution that berry et al17 characterized as weak , which allows the data to shape the amount of borrowing , can actually have a substantial influence on the real risks of obtaining false - positive results . 
hyman consulting or advisory role : atara biotherapeutics , chugai pharmaceutical , cytomx therapeutics , boehringer ingelheim , astrazeneca research funding : astrazeneca , puma biotechnology , loxo oncology gregory j . 
riely consulting or advisory role : genentech research funding : novartis ( inst ) , roche ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , infinity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : novartis , merck sharp & dohme kristen m . 
begg no relationship to disclose affiliations all authors : memorial sloan kettering cancer center , new york , ny . supported in part through national cancer institute awards ca008748 and ca163251 . support references 33 : 975 - 977 , 2015 1 . 
hyman dm , puzanov i , subbiah v , et al : vemurafenib in multiple nonmelanoma cancers with braf v600 mutations . n engl j med 373 : 726 - 736 , 2015 3 . 
eortc network of core institutions : cross - tumoral phase 2 clinical trial exploring crizotinib ( pf - 02341066 ) in patients with advanced tumors induced by causal alterations of alk and / or met ( create ) , 2013 . 
lopez - chavez a , thomas a , rajan a , et al : molecular profiling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
burris ha , hurwitz h , perez ea , et al : mypathway : an open - label phase iia study of trastuzumab / pertuzumab , erlotinib , vemurafenib , and vismodegib in patients who have advanced solid tumors with mutations or gene expression abnormalities targeted by these agents . 
iasonos a , g onen m , bosl gj : scientific review of phase i protocols with novel dose - escalation designs : how much information is needed ? j clin oncol 33 : 2221 - 2225 , 2015 17 . 
chen c , li n , shentu y , et al : adaptive informational design of confirmatory phase iii trials with an uncertain biomarker effect to improve the probability of success . 
 precision medicine for relapsed multiple myeloma on the basis of an integrative multiomics approach alessandro lagan itai beno david melnekoff violetta leshchenko deepu madduri dennis ramdas larysa sanchez scot niglio deepak perumal brian a . 
contributed equally to this work . corresponding author : alessandro lagana , 770 lexington avenue , 14 - 12 new york , ny 10065 ; twitter : @alagana1 ; e - mail : alessandro.lagana@mssm.edu. licensed under the creative commons attribution 4.0 license purpose multiple myeloma ( mm ) is a malignancy of plasma cells , with a median survival of 6 years . 
current approaches in precision oncology aim at matching specific dna mutations to drugs , but incorporation of genome - wide rna profiles has not yet been clinically assessed . methods we have developed a novel computational platform for precision medicine of relapsed and / or refractory mm on the basis of dna and rna sequencing . 
we tested our approach in a pilot precision medicine clinical trial with 64 patients with relapsed and / or refractory mm . results we generated treatment recommendations in 63 of 64 patients . 
of these , 11 received a drug that was based on rna findings , eight received a drug that was based on dna , and two received a drug that was based on both rna and dna . 
sixteen of the 21 evaluable patients had a clinical response ( ie , reduction of disease marker 25% ) , giving a clinical benefit rate of 76% and an overall response rate of 66% , with five patients having ongoing responses at the end of the trial . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction multiple myeloma ( mm ) is a mostly incurable malignancy of terminally differentiated plasma cells that affects 6.5 per 100 , 000 people per year in the united states , making it the second most common hematologic malignancy.1 typically , the trajectory of mm is characterized by a pattern of recurrent remissions and relapses , with patients becoming increasingly refractory to treatment . 
 hallmarks of mm include chromosomal translocations and copy number alterations ( cna ) .2 however , the causal drivers of mm pathogenesis are still unclear , and treatment is administered empirically on the basis of recurrence risk rather than genetic events . 
high - throughput dna sequencing of patients with mm has revealed wide and remarkable heterogeneity of the mutational spectrum across patients and a complex subclonal structure , 3 , 4 suggesting that the use of a personalized therapeutic approach is likely to improve the outcomes for myeloma.5 in the past 4 years , we have focused on the design and development of a computational platform for personalized therapy of relapsed and / or refractory mm , on the basis of a comprehensive patient profile generated from dna and rna sequencing . 
this is leading to a landmark paradigm shift in cancer therapy , in which treatment may be administered on the basis of the specific genomic alterations observed in a patients tumor , rather than on the tumor histology or tissue type . our approach to precision medicine of relapsed mm critically incorporates rna sequencing based drug repurposing . 
importantly , although our pipeline is designed and tailored for the specific needs of mm therapy , it can provide a general framework for incorporating rna sequencing based drug repurposing in oncology . methods protocol approvals and patient enrollment the patients were physician referred . 
enrollment criteria , which included relapsed myeloma , lack of food and drug administration ( fda ) approved therapeutic options , and a prognosis of 6 months of survival , were approved by the mount sinai institutional review board ( irb )  . 
the study was concluded in september 2017 . sample processing and sequencing bone marrow ( bm ) aspirates and peripheral blood ( pb ) were obtained from patients with mm in the study . 
raw sequencing data are available at national center for biotechnology information sequence read archive ( accession number : prjna474747 )  . data processing and bioinformatics analysis we designed and implemented a software framework for the definition and execution of data analysis workflows . 
extended methods are provided in the data supplement . results overview of the study and patient characteristics we developed a computational platform for personalized therapy of relapsed and / or refractory mm , on the basis of a comprehensive patient profile generated from dna sequencing and rnaseq data ( fig 1 )  . 
we evaluated the feasibility and effectiveness of our approach in an irb approved precision medicine clinical trial with 64 participants treated at mount sinai ( see methods and table 1 )  . 
 overall , the patients had received a median of seven lines of therapy , with 13 patients ( 20% ) having received > 10 lines of therapy . genomic landscape of patients with relapsed mm and actionable findings we obtained dna data , either wes or targeted sequencing or both , for 55 patients ( 86% ; data supplement )  . 
the pipeline identified a total of 21 , 166 somatic mutations in 10 , 403 genes in 54 of the 55 patients with dna data available ( data supplement )  . 
whole - exome and / or targeted panel sequencing ( seq ) is performed , and the obtained reads are mapped to the reference genome and analyzed for the identification of somatic mutations and copy number alterations , which are then prioritized on the basis of their actionability . 
we used the clinical interpretations of variants in cancer database ( org ) to identify actionable mutations ( ie , those associated with sensitivity to one or more drugs in one or more cancer types6 ; fig 2c ; data supplement )  . 
the other actionable mutations detected were associated with other hematologic malignancies or with solid cancers . cna constitute another important category of abnormalities observed frequently in mm , as well as in other cancers . 
overall , we found a total of 3 , 541 genes affected by cna in at least one patient and identified 31 actionable alterations ( fig 2d ; data supplement )  . 
we assessed concordance of wes - based cna with fluorescent in situ hybridization and cytogenetics for detection of the most recurrent and clinically relevant cna in mm ( del [ 1p ] , del [ 13q ] , del [ 17p ] , and gain [ 1q21 ] ) and observed a 69% overlap . analysis of the mm transcriptome for the identification of actionable variations rnaseq data were available for 60 patients ( 94% ) and were used to determine outlier genes and pathway activation and to perform rna drug repurposing ( data supplement )  . 
we then calculated pathway activation by single - sample gene set variation analysis7 on a set of actionable pathways relevant in mm : xbp1s activation , mammalian target of rapamycin signaling , histone deacetylase ( hdac ) , dna repair , interleukin - 6 signaling , pi3k / akt activation , hedgehog signaling , fibroblast growth factor receptor 3 , and mitogen activated protein kinase ( mapk )  . 
 ( % ) unless indicated otherwise . abbreviations : asct , autologous stem cell transplant ; iss , international staging system . ranged from 113 to 1 , 423 , with an average of 527.5 mutations per patient ( fig 2a )  . 
mutations were distributed among 14 different categories according to their nature and position in the genome , the majority of them being located in introns ( 57% ; fig 2b )  . 
 ( a ) distribution of mutational burden ( ie , number of total mutations per megabase [ mb ] detected ; n = 41 patients with whole exome sequencing [ wes ] data available )  . 
fgfr3 , fibroblast growth factor receptor 3 ; hdac , histone deacetylase ; il - 6 , interleukin - 6 ; mapk , mitogen - activated protein kinase ; mtor , mammalian target of rapamycin ; p13k akt , phosphoinositide 3 - kinase ; xbp1s , xbox binding protein 1 spliced . the l1000cds2 method , which is based on characteristic direction signatures.8 , 9 the rationale behind this approach is that a drug inducing a gene expression profile that is opposite to a patients profile might be able to revert the disease - associated signature and the phenotype . 
this approach has been demonstrated successfully in several published cases.10 - 12 figure 3d presents the distribution of fda - approved cancer drugs selected by our analysis in the cohort . 
the data supplement summarizes fda - approved noncancer drugs options that were selected for at least one patient . implemented recommendations and response to therapy our pipeline generated recommendations for 63 of 64 patients ( 98% )  . 
trametinib was recommended because of mutations in either nras or kras ; venetoclax was recommended because of high bcl2 expression in the context of all the patients analyzed ( data supplement ) ; panobinostat was recommended on the basis of rnaseq analysis indicating activation of the hdac pathway and / or by rna - based drug repurposing selecting the pan - hdac inhibitor vorinostat . 
 a - 100 ismms56 ismms43 ismms42 ismms41 ismms40 ismms36 ismms34 ismms27 ismms26 ismms25 ismms23 ismms21 ismms20 ismms19 ismms10 ismms09 ismms08 ismms07 ismms05 ismms02 ismms01 dna based rna based dna + rna based treatment ongoing ( patient still responding ) patients disease progression physicians choice adverse event remission achieved death additional drugs used treatment ongoing other therapy trametinib venetoclax panobinostat dabrafenib etoposide time ( days ) fig 4 . 
each color represents a different drug , coded as follows : trametinib ( light blue ) , venetoclax ( dark gold ) , panobinostat ( dark blue ) , dabrafenib ( salmon ) , and etoposide ( dark red )  . 
triangle indicates discontinuation of treatment , where reasons are color coded as follows : disease progression ( gold ) , physicians choice ( green ) , adverse event ( pink ) , and remission achieved ( white )  . 
of these , 11 ( 52% ) received a drug on the basis of rna profiling , eight ( 38% ) on the basis of dna profiling , and two ( 10% ) on the basis of both rna and dna profiling . 
 five patients received our recommended drugs alone , whereas for 16 patients , the drugs were either added to previous treatment ( n = 10 ) or administered in combination with other drugs on the basis of physician discretion ( n = 6 )  . 
in particular , of the 21 evaluable patients , one ( 5% ) achieved cr ; three ( 14% ) , very good partial response ; and 10 ( 47% ) , pr , to give an overall response rate of 66% . 
five patients had still ongoing responses at the end of the study ( september 1 , 2017 ) , with response durations of 235 , 182 , 150 , 172 , and 99 days , respectively ( fig 4b )  . 
significant ( grade 3 ) nonhematologic toxicities were seen in five patients ( 24% ) ; these included neutropenic fever , diarrhea , fatigue , and cardiomyopathy ( table 2 )  . case studies case 1 : patient ismms05 ( rna - based recommendation : panobinostat plus venetoclax )  . 
on the basis of these findings , she was administered venetoclax 400 mg po once daily , the hdac inhibitor panobinostat 20 mg monday , wednesday , and friday , 2 weeks on , 1 week off , and , in addition , pomalidomide 2 mg monday to friday , 3 weeks on , 1 week off . 
after relapsing after receiving multiple treatments including pomalidomide 2 mg ( immediate preceding regimen ) , his cd138 + cells and pb samples were sent for sequencing ( data supplement )  . 
before treatment , his iga and free kappa light chains measured 661 mg / dl and 576 mg / l , respectively ( free kappa / lambda ratio , 1932 )  . 
three months after treatment began , his iga had reached a nadir of 94 mg / dl , whereas his free kappa light chains had decreased to 109 mg / l . 
the patient relapsed 5 months later , with free kappa light chains rising to 390 mg / l ( iga , 187 mg / dl ; data supplement )  . case 3 : patient ismms40 ( wes + rna - based recommendation : trametinib plus venetoclax )  . 
the patient was initially administered lenalidomide and dexamethasone , which resulted in relapse and , after multiple failed regimens , his cd138 + cells and pb were sent for sequencing ( data supplement )  . 
after relapse , the patient was challenged with venetoclax 400 mg monday to friday , trametinib 2 mg monday , wednesday , friday , and carfilzomib 20 / 27 mg / m2 . 
the patient has been continuing this regimen for 3 months ( data supplement )  . discussion here , we reported our integrated multiomics approach for personalized therapy of mm and its application in a pilot precision medicine clinical trial with 64 patients with relapsed mm seen at mount sinai . 
the results of our study show how a precision medicine approach incorporating rna sequencing may identify viable and effective therapeutic options beyond the current fda - approved armamentarium in mm . 
our pipeline generated recommendations from a larger pool of fda - approved cancer drugs ( mm and non - mm ) for 63 of 64 patients in the trial ( 98% ; fig 5 )  . treatment was implemented in 40% of patients , and 81% of these were evaluable ( table 2 )  . 
 two drugs that we repurposed successfully from other cancers in our study were trametinib and venetoclax , the former selected on the basis of dna and the latter on the basis of rna findings . 
trametinib is a mek1 / 2 inhibitor approved by the fda in combination with dabrafenib for unresectable or metastatic melanoma and nonsmall - cell lung cancer carrying mutations in braf ( v600e / v600k )  . 
recent studies have shown activating mutations in nras , kras , and braf in mm , making the mapk pathway a significant therapeutic target also in mm.3 - 5 a retrospective study has demonstrated clinical activity of trametinib in patients with mm with ras - mutated tumors.14 eleven of 21 evaluable patients in our study received trametinib , either alone or in combination with other drugs . 
six of them had clinical response , with a median progression - free survival of 110 days , and two patients had ongoing responses at the end of the study . 
 bone marrow rnaseq ( 94% ) wes ( 64% ) targeted dna panel ( 53% ) analysis pipeline rx 1 rx 2 rx n drug recommendation genomics transcriptomics n = 64 pts relapsed and / or refractory mm peripheral blood n = 16 pts ( 76% ) responded ( mr ) n = 5 pts ( 24% ) did not respond ( sd ) n = 21 pts ( 81% ) evaluable dna - based ( n = 8 [ 38% ] ) rna - based ( n = 10 [ 48% ] ) dna + rna - based ( n = 3 [ 14% ] ) n = 26 pts ( 40% ) treatment implemented n = 38 pts ( 60% ) treatment not implemented no drugs no drugs identied ( 3% ) insurance denial ( 11% ) pt progression before implementation or lost to follow - up ( 86% ) possible problems potential solutions clonal heterogeneity bone marrow microenvironment bad predictions wes - based clonality assessment scrnaseq cytof scrnaseq of microenvironment in silico validation ( from proling ) in vitro / in vivo validation fig 5 . 
we obtained rna sequencing ( rnaseq ) for 94% , whole - exome sequencing ( wes ) for 64% , and targeted dna panel data for 53% of the pts . 
 according to imwg criteria , 76% of the pts had a clinical response ( mr and above , where mr = minimal response and corresponds to a 25% reduction of disease marker ) , whereas 24% of the pts had stable disease ( sd ) or worse . 
problems to address to improve recommendations include assessment of clonal heterogeneity , analysis of bone marrow microenvironment , and extension of reference data to include mm - specific drug profiles from in vitro and in vivo models . 
treatment was not implemented in 60% of the pts , because either no drugs were identified , because insurance denied the proposed drugs , or because of rapid progression of the patient before the results of sequencing were available . 
cytof , mass cytometry ; scrna , single - cell rna . progression - free survival of 161 days , and five patients had ongoing responses at the end of the study . 
overall , these results compare favorably to the efficacy seen in several novel agents for mm , including pomalidomide , daratumumab , and elotumumab , as well as targeted precision medicine approaches such as the nci - match ( national cancer institute molecular analysis for therapy choice ) trial , in which patients with specific solid tumors received treatment on the basis of actionable dna mutations.19 our trial also identified the challenges in implementing ngs - based recommendations in a real - world setting . 
in 60% of the patients with recommendations , treatment was not implemented , either because of insurance denial of the drug or because of rapid progression of disease before sequencing results were available . 
this may be more expensive initially but may become cost effective with greater use . of the 21 treated patients who were evaluable , five did not respond to the recommended therapy . 
 populations may evolve by selective pressure of therapy.5 , 20 , 21 we have recently started to investigate the impact of clonal heterogeneity on therapy selection , by extending our analysis to include clonality assessment on the basis of wes and / or single - cell rna sequencing ( scrnaseq )  . 
integration of both wes and scrnaseq may provide a more comprehensive profile of a patients tumor , enabling drug repurposing at the subclonal level . another key factor in optimal therapy prediction is the bm microenvironment . 
mm cells are strongly dependent on the surrounding microenvironment , which promotes their homing , growth , survival , and migration , as well as their resistance to drugs.22 therapies targeting both the cellular and the noncellular bm compartments are available and are currently used in mm , although not in a targeted manner . 
profiling the microenvironment by scrnaseq and / or mass cytometry , which allows simultaneous measurements of up to 50 markers at single - cell resolution , may help dissect the nontumor compartment and better inform targeted therapy . 
 we are currently investigating the feasibility of including this feature in the next generation of our platforin particular , the use of scrnaseq in clinical precision oncology is limited by several challenges , including increased cost compared with bulk sequencing ( approximately 10 times higher ) , high sensitivity to sample purity , and dropouts ( ie , undetected transcripts due to low amounts of rna sequenced within individual cells ) , as well as data processing and interpretation . 
dudley , samir parekh provision of study materials or patients : ajai chari , hearn - jay cho , deepu madduri , bart barlogie , sundar jagannath , samir parekh collection and assembly of data : alessandro lagan , violetta leshchenko , deepu madduri , dennis ramdas , larysa sanchez , scot niglio , deepak perumal , ajai chari , hearn jay cho , bart barlogie , sundar jagannath data analysis and interpretation : alessandro lagan , itai beno , david melnekoff , brian a . 
kidd , riccardo miotto , jane houldsworth , rita shaknovich manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors technology that will likely complement current precision medicine strategies in the near future . a third key factor to consider concerns the accuracy of the predictions . 
we are working on extending our knowledge base to incorporate mm specific data , including transcriptional effects of novel agents , to quickly and effectively translate robust research findings into clinical practice . 
to further improve drug recommendations , we are implementing validation of the in silico findings using both in vitro ( micro - c3 ) and in vivo ( pdx ) models.23 , 24 this will also contribute to reducing both the costs and the toxicities associated with ineffective treatments . 
finally , we are going to equip our platform with a machine learning flow , which will implement interactive learning techniques to refine the predictions on the basis of therapy outcome and physicians opinion . in conclusion , here we have described our sequencing - based precision medicine platform for relapsed and / or refractory mm and reported the results of a pilot clinical trial to assess the feasibility and usefulness of this approach . 
the trial has allowed us to test and reveal the accuracy of our platform and to understand the pitfalls and limitations of the approach , laying the foundation for our next - generation precision medicine framework . 
 david melnekoff no relationship to disclose violetta leshchenko no relationship to disclose deepu madduri employment : roivant sciences ( i ) leadership : roivant sciences ( i ) honoraria : abbvie consulting or advisory role : abbvie speakers ' bureau : baxalta / shire stock and other ownership interests : roivant sciences ( i ) patents , royalties , other intellectual property : roivant sciences ( i ) dennis ramdas employment : eli lilly ( i ) stock and other ownership interests : eli lilly ( i ) speakers ' bureau : janssen pharmaceuticals , sanofi , takeda pharmaceuticals ( i ) larysa sanchez no relationship to disclose scot niglio no relationship to disclose deepak perumal no relationship to disclose brian a . 
kidd no relationship to disclose riccardo miotto no relationship to disclose rita shaknovich employment : cgix leadership : cgix stock and other ownership interests : cgix consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca ajai chari consulting or advisory role : array biopharma , celgene , novartis , millennium pharmaceuticals , amgen , janssen oncology , adaptive biotechnologies , bayer ag , seattle genetics research funding : array biopharma , celgene , millennium pharmaceuticals , novartis , onyx pharmaceuticals , janssen pharmaceuticals , pharmacyclics , acetylon pharmaceuticals ( inst ) , biotest ( inst ) , bristol - myers squibb ( inst ) travel , accommodations , expenses : takeda pharmaceuticals , celgene , novartis , amgen , janssen oncology , bristol - myers squibb hearn jay cho honoraria : genentech / roche consulting or advisory role : janssen research & development , genentech , bristol - myers squibb research funding : agenus , janssen research & development , bristol - myers squibb travel , accommodations , expenses : roche / genentech , bristol - myers squibb bart barlogie no relationship to disclose sundar jagannath honoraria : celgene , karyopharm therapeutics consulting or advisory role : celgene , bristol - myers squibb , janssen pharmaceuticals , novartis , karyopharm therapeutics research funding : celgene ( inst ) , karyopharm therapeutics ( inst ) , bristol - myers squibb ( inst ) joel t . 
dudley consulting or advisory role : janssen pharmaceuticals , allergan research funding : astrazeneca ( inst ) samir parekh consulting or advisory role : foundation medicine acknowledgment we thank the genomics core facility at the icahn institute and the department of genetics and genomic sciences at mount sinai , the mount sinai hematological malignancies tissue bank ( hmtb ) , and the human immune monitoring core ( himc ) for their support . 
we also thank scientific computing at the icahn school of medicine at mount sinai for their computational resources and staff expertise . affiliations alessandro lagan , itai beno , david melnekoff , violetta leshchenko , deepu madduri , dennis ramdas , larysa sanchez , scot niglio , deepak perumal , brian a . 
touzeau c , dousset c , le gouill s , et al : the bcl - 2 specific bh3 mimetic abt - 199 : a promising targeted therapy for t ( 11 ; 14 ) multiple myeloma . 
kumar s , kaufman jl , gasparetto c , et al : efficacy of venetoclax as targeted therapy for relapsed / refractory t ( 11 ; 14 ) multiple myeloma . 
moreau p , chanan - khan a , roberts aw , et al : promising efficacy and acceptable safety of venetoclax plus bortezomib and dexamethasone in relapsed / refractory mm . 
pak c , callander ns , young ew , et al : microc ( 3 ) : an ex vivo microfluidic cis - coculture assay to test chemosensitivity and resistance of patient multiple myeloma cells . 
mody , md , ms2 introduction somatic mutations in b - cell lymphoma 6 ( bcl6 ) corepressor ( bcor ) are reported in solid and hematologic malignancies in adults and children . 
bcor mediates transcriptional repression through epigenetic modication believed to cause oncogenesis through both overexpression or loss of tumor suppressor function.1 it is found to affect multiple diverse downstream gene targets and plays a role in development and function across many tissue lineages , especially the cns.2 , 3 in pediatric malignancies , bcor - ccnb3 fusion is prominent in undifferentiated round cell sarcoma ( uds ) , which , until recently , was treated similarly to ewing sarcoma ( ews )  . 
now considered its own genetic entity , bcor - ccnb3 fusions are typically identied in uds using transcriptome sequencing ( rna - seq ) and are present in up to 14% of uds cases.4 , 5 internal tandem duplications in bcor are found in pediatric cns neuroepithelial tumors and clear cell sarcoma of the kidney , 6 , 7 and mutations are reported in rhabdomyosarcoma and diffuse intrinsic pontine glioma ( dipg ) .8 , 9 however , uncertainty remains regarding the genomic landscape and signicance of bcor alterations in pediatric malignancies . in this article , we describe bcor alterations identied in our integrative clinical sequencing ( ics ) cohort in patients with sarcoma and high - grade glioma ( hgg ) these alterations in and explore the landscape of publicly available databases . 
furthermore , we examine their histopathologic features and co - occurring genomic aberrations and propose prospective targeted treatment strategies . methods pediatric and young adult patients ( , 26 years ) described were consented and enrolled in a prospective , institutional review boardapproved ( hum# : ics trial pediatricmichigan oncology 00056496 ) sequencing ( peds - mioncoseq ) at c.s. 
details of the sequencing procedures and bioinformatics analyses have been previously described.10 briey , somatic mutations , copy number variants / alterations , insertions and deletions , gene fusions , and gene expression are analyzed.11 , 12 investigation of clinical relevance of somatic variants uses an integrated approach incorporating technical considerations , variant and patient - specic information , and published data . st judes pediatric cancer data portal ( pecan ) was used ( accessed january 2019 ) to explore bcor alterations in a larger cohort of pediatric patients . 
the pecan database is a pediatric cancer genome repository containing whole - genome sequencing , wholeexome sequencing , and rna - seq data on more than 4 , 300 patients . 
 mankuzhy et al of the 86 sarcoma cases sequenced at the time of this report , 18 osteosarcomas and ve malignant peripheral nerve sheath tumors did not contain bcor alterations . twenty - seven of the remaining 63 cases contained clinically relevant diagnostic fusions , one ( 3.7% ) of which ( pax3 - foxo1positive alveolar rhabdomyosarcoma ) also had a bcor alteration . 
of the 15 patients with dipg sequenced , three ( 20% ) harbored mutations in bcor . pathologic evaluation of the bcor - mutant sarcoma cases showed both round - cell ( ewing - like ) morphology and the recently recognized variant with spindle - cell sarcoma morphology.17 figure 1 shows noncohesive sheets of malignant round to ovoid cells , with primitive - appearing chromatin , high mitotic activity , and necrosis . 
there were interlacing short fascicles with whorled pattern and foci of somewhat epithelioid congurations around larger vessels , mimicking synovial sarcoma and malignant peripheral nerve sheath tumor . mitotic gures were also identied . 
vimentin immunostain was diffusely strongly positive , and cd99 was negative . review of the pecan data set revealed 16 patients with tumors harboring nonsynonymous bcor alterations , ranging in age from 2 to 21 years ( table 2 )  . 
of the nine hggs , six contained concurrent gfr alterations , including two egfr and four platelet - derived growth factor receptor a mutations . the frequency of bcor mutations of primary adult cancers in tcga was 15 of 393 ( 3.8% ) in sarcoma and two of 273 ( 0.7% ) in hgg , particularly gbm . 
in the mi - oncoseq data set with advanced or refractory adult patients , sarcoma had a bcor mutation frequency of three of 199 ( 1.5% ) and gbm one of 49 ( 2% )  . discussion through integrative analysis of a cohort of high - risk pediatric malignancies and review of other large genomic databases , our study further describes the frequency and distribution of bcor alterations in pediatric sarcoma and high - grade glial malignancies . 
we recognized a higher overall prevalence of bcor alterations in these pediatric malignancy subtypes compared with their adult counterparts , both in primary cases ( tcga ) and refractory / advanced cases ( mi - oncoseq )  . 
this could be explained by bcors role in embryonic stem - cell differentiation , hematopoiesis , and regulation of vertebrate laterality and germline bcor mutations causing lenz microphthalmia and oculofaciocardiodental syndromes , which display fig 1 . 
 ( d ) cd99 immunostain ( 20 ) is negative . phenotypically overlapping skeletal , cns , and ocular effects , supporting its pleotropic developmental function.1 , 3 , 18 our study shows relatively high prevalence of bcor alterations in pediatric hgg ( 17% ) and in pediatric sarcomas , which are negative for fusions and other pathognomonic molecular alterations ( 11% ) , emphasizing the need for ics analysis to better dene molecular subtypes of these cases . 
our study also conrms earlier observations of bcor alterations in fusion - positive and - negative alveolar rhabdomyosarcoma.19 , 20 however , our ics cohort did not detect any bcor alterations in classic ewsr1 - rearranged ews or osteosarcoma , as seen in pecan . previous research has suggested that the prognostic signicance of bcor alterations could be tissue and diagnosis specic , with bcor - mutant leukemia being associated with a worse prognosis and no survival difference detected when comparing bcor - ccnb3 and ews.4 , 21 , 22 however , because of our cohorts small sample size and a lack of availability of outcomes data in larger data sets , additional investigation is needed to truly dene prognostic signicance of bcor alterations , specically in hgg . a novel nding in our cohort is the high frequency ( 57% ) of concurrent bcor and gfr alterations . 
gfrs are typically expressed on cell surfaces and play important roles in cell growth , survival , angiogenesis , and metastasis.23 the concurrent gfr mutations seen in our cohort are all known to be gain - of - function mutations resulting in constitutive activation of the gfr pathway and increased cell proliferation.24 - 27 bcl6 depletion results in downregulation of kinases in the receptor tyrosine kinase pathway , suggesting a potential link between bcl6 and related proteins such as bcor with receptor tyrosine kinase signaling that could be further explored to determine the signicance of these mutations.28 the bcl6 / bcor previous research has suggested that complex could serve as a potential therapeutic target . reported downstream targets of bcor activity include bcl6 targets , hoxa cluster genes , notch homolog 1 targets , and sonic hedgehog effectors such as gli1 and gli2.2 , 29 - 31 bcor can interact with specic histone deacetylase of both class i and ii , which increases the repression of transcriptional activity.32 the effect of histone deacetylase inhibitors on tumors with bcor mutations warrants additional investigation to assess the biologic relevance of these interactions , particularly in patients with dipg who also harbor histone mutations . 
 bcor alterations in pediatric solid tumors molecular and genomic characterization of tumors can complement histology - based classications of human cancers.35 recognizing which alterations are clinically meaningful and developing effective targeted treatment strategies can further contribute to dening this new cancer routine genomic proling can taxonomy . identify potential drivers of oncogenesis and possible targetable aberrations that can stimulate development of novel investigations of therapeutic approaches and additional in addition , molecular mechanisms of cancer . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . chandan kumar patents , royalties , other intellectual property : royalty for um agr #3199.101 recurrent gene fusions in prostate cancer licensed to gen - probe , inc . no other potential conicts of interest were reported . references hum mol genet 16 : 1773 - 1782 , 2007 1 . 
hilton en , manson fdc , urquhart je , et al : left - sided embryonic expression of the bcl - 6 corepressor , bcor , is required for vertebrate laterality determination . gearhart md , corcoran cm , wamstad ja , et al : polycomb group and scf ubiquitin ligases are found in a novel bcor complex that is recruited to bcl6 targets . mol cell biol 26 : 6880 - 6889 , 2006 3 . 
plos one 3 : e2814 , 2008 kao yc , owosho aa , sung ys , et al : bcor - ccnb3 fusion positive sarcomas : a clinicopathologic and molecular analysis of 36 cases with comparison to morphologic spectrum and clinical behavior of other round cell sarcomas . 
am j surg pathol 42 : 604 - 615 , 2018 peters tl , kumar v , polikepahad s , et al : bcor - ccnb3 fusions are frequent in undifferentiated sarcomas of male children . 
mod pathol 28 : 575 - 586 , 2015 argani p , kao y - c , zhang l , et al : primary renal sarcomas with bcor - ccnb3 gene fusion : a report of 2 cases showing histologic overlap with clear cell sarcoma of kidney , suggesting further link between bcor - related sarcomas of the kidney and soft tissues . 
am j surg pathol 41 : 1702 - 1712 , 2017 sturm d , orr ba , toprak uh , et al : new brain tumor entities emerge from molecular classication of cns - pnets . 
cell 164 : 1060 - 1072 , 2016 cramer sl , miller al , pressey jg , et al : pediatric anaplastic embryonal rhabdomyosarcoma : targeted therapy guided by genetic analysis and a patient - derived xenograft study . 
mackay a , burford a , carvalho d , et al : integrated molecular meta - analysis of 1 , 000 pediatric high - grade and diffuse intrinsic pontine glioma . 
tirode f , surdez d , ma x , et al : genomic landscape of ewing sarcoma denes an aggressive subtype with co - association of stag2 and tp53 mutations . 
 mankuzhy et al juckett lt , lin di , madison r , et al : a pan - cancer landscape analysis reveals a subset of endometrial stromal and pediatric tumors dened by internal tandem duplications of bcor . 
li w - s , liao i - c , wen m - c , et al : bcor - ccnb3 - positive soft tissue sarcoma with round - cell and spindle - cell histology : a series of four cases highlighting the pitfall of mimicking poorly differentiated synovial sarcoma . 
shern jf , chen l , chmielecki j , et al : comprehensive genomic analysis of rhabdomyosarcoma reveals a landscape of alterations affecting a common genetic axis in fusion - positive and fusion - negative tumors . 
puls f , niblett a , marland g , et al : bcor - ccnb3 ( ewing - like ) sarcoma : a clinicopathologic analysis of 10 cases , in comparison with conventional ewing sarcoma . 
bellus ga , spector eb , speiser pw , et al : distinct missense mutations of the fgfr3 lys650 codon modulate receptor kinase activation and the severity of the skeletal dysplasia phenotype . 
de gunst mm , gallegos - ruiz mi , giaccone g , et al : functional analysis of cancer - associated egfr mutants using a cellular assay with yfp - tagged egfr 28 . 
proc natl acad sci usa 114 : 3981 - 3986 , 2017 [ erratum : proc intracellular domamol cancer 6 : 56 , 2007 natl acad sci usa 114 : e4317 , 2017 ] 29 . 
tiberi l , bonnefont j , van den ameele j , et al : a bcl6 / bcor / sirt1 complex triggers neurogenesis and suppresses medulloblastoma by repressing sonic hedgehog signaling . 
schnidar h , eberl m , klingler s , et al : epidermal growth factor receptor signaling synergizes with hedgehog / gli in oncogenic transformation via activation of the mek / erk / jun pathway . 
 ras mutations are associated with inferior progression - free survival and overall survival of patients with mcrc compared with patients with nonmutated tumors.1 it is conceivable that ras mutations are negative prognostic factors per se ; however , the availability of only one actionable molecular target , that is , the inhibition of angiogenesis , in patients with mutated tumors certainly affects survival in this subgroup of patients . 
recent studies have demonstrated that the analysis of circulating tumor dna ( ctdna ) in blood samples , through its ability to recapitulate tumor heterogeneity , is a remarkable surrogate of tumor biopsy for mutation detection.2 extensive research on liquid biopsy led to significant achievements in the comprehension of the biologic reasons behind acquired resistance to anti - egfr therapies.3 to date , studies with liquid biopsy have been selectively concentrated on the appearance of ras - mutant clones in the blood of patients with ras wild - type primary crc , as biomarkers of anti - egfr therapy resistance . 
we here report that ctdna analysis , over the course of antiangiogenic treatment , might reveal a therapeutically exploitable window of opportunity , characterized by the relative prevalence of ras wild - type clones over time . 
a whole - body contrast enhanced computed tomography ( ct ) scan revealed a left supraclavicular lymphadenopathy , transverse colon thickening ( 3 cm ) , multiple chest and abdominal lymphadenopathies , and peritoneal carcinomatosis . 
mutational analysis of the lymph node metastasis performed through real - time polymerase chain reaction ( pcr ; real - time oncoscreen nras ) revealed exon 4 nras a146t mutation at 29 cycles . 
serum tumor markers significantly decreased , with rapid negativization ( carcinoembryonic antigen [ cea ] , 1.31.23 ; ca 19 - 9 , 71.839 ; ca - 125 , 8226 )  . 
at that time , serum tumor markers increased again ( ca 19 - 9 , 530 ; cea , 9 ) , with clinical evidence of bilateral axillary lymph node enlargement . 
concurrently , the patient was enrolled in an observational study open at our institution , which aimed to serially monitor the mutational status of ctdna in patients with ras - mutant mcrc disease , before starting any new line of treatment and in course of therapy until progression . methods blood samples were prospectively collected after obtaining informed consent with ethical committee approval . 
idylla ( biocartis , nv , mechelen , belgium ) , a fully automated , realtime pcr - based molecular diagnostics system , was used to investigate ras mutational profile from plasma . 
the first allows the detection of 21 mutations in codons 12 , 13 , 59 , 61 , 117 , and 146 of the kras gene , and the second allows the detection of 18 mutations in codons 12 , 13 , 59 , 61 , 117 , and 146 of the nras gene , five mutations in codon 600 of the braf gene , and two mutations in codon 492 of the egfr gene from 1 ml of plasma . among the parameters describing the generated pcr curves , the cq value is calculated as the difference between the quantification cycle value ( cq ) of the gene control signal and the cq of the mutant signal . 
according to the manufacturer 's instructions , a cq value of the nras control of 35.5 or higher indicates that a low amount of cell - free dna is present in the sample . 
in such cases , low - frequency mutations may not be detected . results in july 2017 , a ctdna mutational analysis was performed and revealed the absence of any clinically relevant mutation in kras , nras , and braf genes . 
this new insight into the biology of the disease convinced us to take this window of therapeutic opportunity , which was not guaranteed to remain open indefinitely ; in july 2017 , the treatment was changed to the second - line combination of irinotecan and cetuximab . 
as early as after the first cycle of chemotherapy , an objective complete clinical response of the bilateral axillary adenopathy was documented , and this was confirmed at ultrasound assessment . 
restaging ct scan after eight cycles of therapy showed a partial response , with significant reduction of pleural effusion and pulmonary lymphangitic carcinomatosis and stability of peritoneal metastases ( fig 1 )  . 
a second ctdna analysis was performed on november 2017 , confirming the ras genes wild - type status ( cq of nras total : 35.5 , which might be due to a reduction in ctdna amount )  . 
 june 2017 ( before folfiri - cetuximab ) october 2017 ( after 3 months of folfiri - cetuximab ) pleural effusion pulmonary lymphangitic carcinomatosis malignant ascites peritoneal carcinosis fig 1 . 
axial computed tomography scan after eight cycles of fluorouracil , leucovorin , and irinotecan ( folfiri ) plus cetuximab shows a partial response , with significant reduction of pleural effusion and pulmonary lymphangitic carcinomatosis and stability of peritoneal metastases . 
 sequence of treatments , clinical and radiologic response to the different schedules adopted ( partial response [ pr ] is indicated by blue arrow , and progressive disease [ pd ] is indicated by red arrow ) , and molecular tests performed on tumor tissue and plasma at different time points . 
bev , bevaci zumab ; cet , cetuximab ; ctdna , circulating tumor dna ; folfiri , fluoro uracil , leucovorin , and irinotecan ; folfoxiri , fluorouracil , leucovorin , oxaliplatin , and irinotecan ; fu , fluorouracil . 
nevertheless , a146t results in increased nras activity and downstream signaling and is transforming in cell culture resulting from increased nras guanosine diphosphate / guanosine triphosphate exchange rate , 4 and consequently patients who harbor mutations in nras also have significantly inferior anti - egfr treatment outcomes benefit compared with those without any ras mutations.5 it is recommended that patients with crc being considered for anti - egfr therapy must receive ras mutational testing , including kras and nras codons 12 and 13 of exon 2 , 59 , and 61 of exon 3 and 117 and 146 of exon 4 , and that anti - egfr should only be prescribed for patients with mcrc who are wild type for all known ras - activating mutations.6 in patients with ras - mutant primary colorectal cancers , ineligible for egfr inhibitors , the importance of the egfr pathway , which indeed sustains the disease , is counterintuitive . 
international guidelines currently recommend treatment of ras mutant mcrc with bevacizumab first line , followed by chemotherapy backbone change or aflibercept / ramucirumab at disease progression.7 preclinical and clinical data , however , demonstrate that tumor angiogenesis inhibition induces biologic changes in tumor - stroma interactions , mainly derived from hypoxia . 
preclinical observations suggest that hypoxia exerts a negative selection against ras - mutant clones through a mechanism known as secretory senescence , in which ras - mutant senescent cells operate in a paracrine manner to support the growth of surrounding ras wild - type clones , leading to their relative prevalence over time.8 we here report that ctdna analysis , under table 1 . 
 antiangiogenic treatment , might reveal a therapeutically exploitable window of opportunity , characterized by the relative prevalence of ras wild - type clones , which can be converted in a clinically meaningful benefit for patients . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . paola gazzaniga no relationship to disclose cristina raimondi no relationship to disclose federica urbano no relationship to disclose the following represents disclosure information provided by authors of this manuscript . 
modest dp , ricard i , heinemann v , et al : outcome according to kras - , nrasand brafmutation as well as kras mutation variants : pooled analysis of five randomized trials in metastatic colorectal cancer by the aio colorectal cancer study group . 
sorich mj , wiese md , rowland a , et al : extended ras mutations and anti - egfr monoclonal antibody survival benefit in metastatic colorectal cancer : a meta - analysis of randomized , controlled trials . 
sepulveda ar , hamilton sr , allegra cj , et al : molecular biomarkers for the evaluation of colorectal cancer : guideline summary from the american society for clinical pathology , college of american pathologists , association for molecular pathology , and american society of clinical oncology . 
long terra lucas shreshtha madaan kristin mattie danielle mckenna susan montgomery sarah nielsen jacquelyn powers kim rainey christina rybak michelle savage christina seelaus ( continued ) purpose multigene panels ( mgps ) are increasingly being used despite questions regarding their clinical utility and no standard approach to genetic counseling . 
how frequently genetic providers use mgp testing and how patient - reported outcomes ( pros ) differ from targeted testing ( eg , brca1 / 2 only ) are unknown . methods we evaluated use of mgp testing and pros in participants undergoing cancer genetic testing in the multicenter communication of genetic test results by telephone study ( clinicaltrials.gov identifier : nct01736345 ) , a randomized study of telephone versus in - person disclosure of genetic test results . 
genetic providers offered targeted or mgp testing based on clinical assessment . results since the inclusion of mgp testing in 2014 , 395 patients ( 66% ) were offered mgp testing . 
being offered mgp testing was significantly associated with not having ashkenazi jewish ancestry , having a history of cancer , not having a mutation in the family , not having made a treatment decision , and study site . 
after demographic adjustment , patients offered mgp testing had lower general anxiety ( p = .04 ) , state anxiety ( p = .03 ) , depression ( p = .04 ) , and uncertainty ( p = .05 ) pre - disclosure compared with patients offered targeted testing . 
there was a greater increase in change in uncertainty ( p = .04 ) among patients who underwent mgp testing . conclusion mgp testing was more frequently offered to patients with lower anxiety , depression , and uncertainty and was associated with favorable outcomes , with the exception of a greater increase in uncertainty compared with patients who had targeted testing . 
delivery of genetic testing results by telephone is one of several adaptations to the traditional genetic counseling practice model that have been studied in an effort to improve counseling access through the more efficient use of resources.3 - 5 beginning in 2012 , as part of the national cancer institute funded multicenter communication of genetic test results by telephone ( cogent ) clinical trial , patients eligible for brca1 / 2 genetic testing for hereditary breast or ovarian cancer risk assessment were recruited and randomly assigned to in - person or telephone disclosure of genetic test results . 
primary outcomes of the cogent study6 have demonstrated that telephone disclosure is noninferior to in - person counseling across all primary and secondary short term outcomes . a robust literature on patient - reported outcomes ( pros ) of brca1 / 2 and targeted genetic testing exists , including two randomized studies of telephone delivery of both pretesting and post - testing genetic services for patients considering genetic testing for these genes.3 , 5 cogent is , to our knowledge , the first randomized study to examine uptake of mgp tests in the population of patients presenting for risk assessment to a tertiary high - risk clinic , as well as to report on pros among patients receiving traditional targeted gene counseling and testing compared with patients receiving counseling and testing adapted to mgps . 
 in the current study , trends in testing choices with the advent of mgp testing and across the cogent study time period and participating sites are reported , and pros previously reported in aggregate are analyzed by counseling and testing modality selected for the patient . methods study design , setting , and participants the cogent study was a multicenter , randomized , noninferiority trial comparing the psychosocial and behavioral outcomes of phone versus in - person disclosure of genetic test results . 
 initially designed to include targeted brca1 / 2 testing only , the study eligibility was adapted in may 2014 to add all clinical germline genetic testing for hereditary breast , gynecologic , and / or gi cancer syndromes , allowing individuals receiving either targeted testing or mgp testing . 
participants were recruited after in - person pretest counseling with a genetic counselor and completed pros at the time of enrollment ( after pretest counseling [ t0 ] ) and after results disclosure ( t1 )  . random assignment after completion of the survey given after pretest counseling , participants were assigned to either the in - person arm or telephone ar random assignment was stratified by study site and sex only . 
participants who did not want to receive results by telephone and thus were not willing to be randomly assigned were permitted to self - select in - person disclosure and were analyzed separately . all 22 genetic counseling professionals used a tiered and binned counseling model for pretest sessions where mgp testing was offered.7 , 8 all disclosures were made using standardized communication protocols and visual aids.7 - 9 both a genetic counseling professional and a medical provider were present when results were provided in person , whereas individuals who received results by telephone were recommended to return to their institution to meet with a medical provider . 
patients responded on a seven - item likert scale and could mark not applicable . statistical analysis for baseline analyses , we characterized variables using means , proportions , standard deviations , and ranges for age . 
variables included in the tables and regressions included age , sex , race ( white v nonwhite ) , education ( college graduate v less than a college degree ) , jewish ethnicity ( no or missing v yes ) , number of firstand second - degree relatives with cancer , known cancer mutation , treatment decision , random assignment or self - selecting for in - person disclosure arm , and study site . 
we did not include in the imputation analyses individuals missing both t0 and t1 response data because we felt that such individuals had too much missing data to reliably impute data . 
the criterion for statistical significance was p < .05. results use and predictors of mgp testing versus targeted testing in total , 600 participants were offered genetic testing after inclusion of mgp testing ; 62.7% of participants ( 376 of 600 participants ) underwent mgp testing , whereas 37.3% of participants underwent targeted testing ( fig 1 )  . 
 targeted testing was most frequently offered to patients with a known familial mutation ( 86% ) and to patients of ashkenazi jewish ancestry ( 67% ) , a population in which three founder mutations in brca1 / 2 are found at high frequency ( prevalence of approximately 1 : 40 )  . 
of note , of 395 patients offered mgp testing by the genetic counselor , a small fraction ( 19 [ 4.8% ] of 395 patients ) declined mgp testing and chose targeted testing . 
characteristics associated with being more likely to be offered mgp testing were older age , female sex , nonashkenazi jewish heritage , personal history of cancer , no known familial mutation , nonrandomization status ( ie , preference for in - person disclosure ) , and study site . the percentage of patients offered mgp testing increased over time ( from 57% in 2014 to 66% in 2015 ; p = .02 ) and was found to vary significantly by study site ( range , 46% to 81% of all tests offered ; fig 2 )  . 
identification of carriers and true - negative results were higher in the targeted testing group , which is likely secondary to a higher number of patients with a known familial mutation ( table 1 )  . 
the frequency of uncertain variants was higher in the mgp group ( 25% v 2% with targeted testing )  . pros assessed by offer of targeted testing versus mgp testing in full models , adjusting for baseline variables , pros were assessed and compared by whether patients were offered mgp testing or targeted testing . 
characteristics of participants in the cogent study after adaptation for mgp by type of testing offered offered targeted testing only ( n = 205 ) offered multigene panel testing ( n = 395 ) characteristic had mgp testing , no . 
finally , there were no significant differences in knowledge at any time point . discussion in the largest study to date of pros after mgp testing , we found that patients eligible for hereditary cancer risk assessment and offered mgp , compared with targeted testing , had similar predisclosure and postdisclosure knowledge levels but lower predisclosure anxiety , depression , and uncertainty . 
these results demonstrate that genetic counselors can incorporate mgp testing into their practice without compromising patient understanding , even when results are delivered by telephone.6 one of the concerns commonly raised with mgp testing is the possibility of knowledge deficits as a result of the complexity of information communicated . 
 the potential negative impact of information overload from mgp counseling or testing on psychological outcomes is not supported by our findings , because we found that postdisclosure anxiety and depression were similar between the mgp and targeted testing groups . 
when the lower levels of predisclosure anxiety and depression among participants offered mgp are considered , our results also suggest that counselors may be more likely to offer complex mgp testing to patients they feel are at lower risk of negative psychological outcomes . 
in this way , these findings suggest that counselors are more than just gatekeepers to genetic testing and that comprehensive counseling includes both knowledge exchange and shared decision making with patients about concerns and preferences for genetic evaluation . 
 in the higher rates of selection of in - person disclosure among patients offered mgp testing , we observe counselors and patients counterbalancing a patients ability to manage the complexity and uncertainty of mgp testing with the standard approach of in - person results disclosure . these findings suggest that telephone disclosure is readily scalable to mgp testing and thus has an important role in the future of genomic medicine . 
although other studies have previously supported the efficacy of alternative telephone - based modalities of genetics services delivery , 3 , 5 these studies have not included mgp testing and have , notably , not reported detailed pros . 
one study recruited women at increased risk of hereditary breast and / or ovarian cancer and randomly assigned participants to in - person or telephone counseling , whereas the second study randomly assigned women with at least a 10% risk of having a brca1 / 2 mutation but without cancer to telephone counseling versus usual care . 
in both studies , telephone counseling was noninferior to in - person counseling for the selected outcomes ( which included anxiety , cancer - specific distress , perceived control , and decisional conflict in one study5 and satisfaction , distress , physical functioning , decisional conflict , and knowledge at 3 months and 1 year in the other study3 ) , although these results are specific to brca1 / 2 testing . 
although pros were not ascertained , the rate of preference for and receipt of mastectomy was similar regardless of whether a brca1 / 2 pathogenic variant or a pathogenic variant in a gene other than brca1 / 2 was identified by mgp , arguing that mgp may lead to more mastectomies over time . 
pros have not been explored in other areas of medicine where mgp testing has entered clinical care . lower postdisclosure anxiety and distress among patients offered mgp testing is consistent with differences seen pre - disclosure and reflect counselorand patient - driven selection of less anxious patients toward mgp testing . 
for others , high pretest risk was secondary to a known familial mutation ; 50% of the targeted testing population had a known familial mutation compared with 4% of the mgp testing population . 
similarly , patients tested by mgp had lower pretest likelihood of a pathogenic mutation , although the risk of identifying uncertain variants was higher as a result of the larger number of genes sequenced . although no other randomized studies have been conducted involving mgp , lumish et al19 performed a post - test survey measuring pros in patients undergoing testing for hereditary breast or ovarian cancer and in whom mgp testing was performed . 
they found older age , nonwhite race or non - hispanic ethnicity , lower educational attainment , and lower knowledge to be associated with higher anxiety and adverse psychological effects from counseling . 
analyses by cancer status ( affected or unaffected ) and stratified by result also found differential impact on psychological outcomes.19 nonetheless , it remains uncertain how the differences would have changed had mgp testing been replaced by targeted testing . 
 intolerance related to genomic testing21 have shown that uncertainty intolerance is associated with impaired decision making , feelings of vulnerability , and other adverse psychological outcomes.22 overall , we found that use of mgp testing increased over the study period.23 several factors are likely driving this change , including the need for more efficient delivery of genetic services . 
 the declining costs and the competitive marketplace for commercial testing established by the us supreme courts decision against myriad genetic laboratories and gene patenting have improved access to genetic testing . 
regional and community hospitals may be particularly disadvantaged when it comes to access to genetic counseling services and thus could be the earliest beneficiaries of models that incorporate remote counseling and testing options . 
however , after accounting for nonrandom differences between the targeted and mgp testing groups , short - term postdisclosure pros were generally similar , suggesting that the benefits of counseling rest in the live conversation between the counselor and patient and not in their proximity . 
time and resource limitations have undermined the traditional rigorous preand post - test counseling model used in cogent ; for example , katz et al25 found that 47% of patients did not receive counseling . 
in addition , few cogent participants were tested to guide a breast cancer treatment decision , and a recent population - based study found that mgp testing was associated with lower rates of testing among patients with breast cancer who had preoperative testing.18 finally , it also possible that patients choosing an mgp test versus targeted testing do so with family and family cancer risks in mind , so there may be additional information on testing selection gained from studying patterns of communication of results with relatives . in summary , the world of clinical genetic testing is changing rapidly , and use of mgp testing has increased over time . 
post - test knowledge , general anxiety , and depression were no worse and state anxiety was lower among patients who received mgp testing compared with those who received targeted testing . 
 bradbury manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors the following represents disclosure information provided by authors of this manuscript . 
 stock and other ownership interests : canceriq , tempus travel , accommodations , expenses : hospital of the university of pennsylvania research funding : novartis ( inst ) other relationship : tempus , color genomics , genentech , myriad genetics , bio ventures for global health kim rainey no relationship to disclose linda j . 
domchek honoraria : astrazeneca , clovis oncology , bristol - myers squibb research funding : astrazeneca ( inst ) , clovis oncology ( inst ) , pharmamar ( inst ) kristin mattie no relationship to disclose danielle mckenna no relationship to disclose susan montgomery no relationship to disclose sarah nielsen no relationship to disclose jacquelyn powers employment : carevive systems honoraria : cureconnect consulting or advisory role : carevive systems christina rybak no relationship to disclose michelle savage no relationship to disclose christina seelaus no relationship to disclose jessica stoll no relationship to disclose jill e . 
olopade employment : canceriq ( i ) leadership : canceriq dominique fetzer no relationship to disclose amanda brandt no relationship to disclose rachelle chambers no relationship to disclose dana f . 
clark no relationship to disclose rikki gaber honoraria : canceriq cassandra gulden no relationship to disclose janice horte no relationship to disclose andrea forman consulting or advisory role : invitae , astrazeneca , ambry speakers ' bureau : astrazeneca , ambry genetics , invitae jessica m . 
daly , andrea forman , susan montgomery , kim rainey , christina rybak , and michelle savage , fox chase cancer center , temple university health system ; susan m . 
olopade , center for clinical cancer genetics and global health , the university of chicago ; pamela ganschow , rikki gaber , terra lucas , and christina seelaus , the john h . 
hospital of cook county ; rachelle chambers , cassandra gulden , shreshtha madaan , sarah nielsen , and jessica stoll , the university of chicago , chicago , il ; and generosa grana , dana f . 
clark , janice horte , kristin mattie , and xinxin ( shirley ) yao , md anderson cancer center at cooper , camden , nj . support supported by national cancer institute grant no . 
kinney ay , steffen le , brumbach bh , et al : randomized noninferiority trial of telephone delivery of brca1 / 2 genetic counseling compared with in - person counseling : 1 - year follow - up . 
bradbury ar , patrick - miller lj , egleston bl , et al : randomized noninferiority trial of telephone vs in - person disclosure of germline cancer genetic test results . 
bradbury ar , patrick - miller lj , egleston bl , et al : patient feedback and early outcome data with a novel tiered - binned model for multiplex breast cancer susceptibility testing . 
bradbury ar , patrick - miller l , long j , et al : development of a tiered and binned genetic counseling model for informed consent in the era of multiplex testing for cancer susceptibility . 
kelly k , leventhal h , marvin m , et al : cancer genetics knowledge and beliefs and receipt of results in ashkenazi jewish individuals receiving counseling for brca1 / 2 mutations . 
cella d , hughes c , peterman a , et al : a brief assessment of concerns associated with genetic testing for cancer : the multidimensional impact of cancer risk assessment ( micra ) questionnaire . 
pieterse ah , van dulmen am , beemer fa , et al : cancer genetic counseling : communication and counselees post - visit satisfaction , cognitions , anxiety , and needs fulfillment . 
biesecker bb , klein w , lewis kl , et al : how do research participants perceive uncertainty in genome sequencing ? genet med 16 : 977 - 980 , 2014 22 . 
identication and monitoring the molecular mechanisms of acquired resistance to cetuximab or panitumumab in crc is important to anticipate the failure of anti - egfr antibodies and design strategies for additional treatments . several mechanisms of acquired resistance to antiegfr have been described in metastatic crc ( mcrc )  . 
 maurel et al context key objective the key objective was to evaluate the predictive and prognostic value of ras and braf mutation dynamics in plasma from patients with metastatic colorectal cancer treated with antiepidermal growth factor receptor ( anti - egfr ) therapy within two clinical trials ( posiba and pulse )  . knowledge generated baseline mutant ras / braf circulating tumor ( ct ) dna was a negative predictive marker of response to anti - egfr therapy , as well as a poor prognostic factor . 
the emergence of ctdna ras / braf mutations had limited relevance to the time to progression to anti - egfr therapy but conferred poor prognosis . relevance this work conrms the clinical utility of ctdna for ras / braf molecular testing to guide treatment decisions in patients with metastatic colorectal cancer ; however , clinical impact of ras / braf dynamics deserves further characterization . of ras , braf , or egfr mutations that drive acquired resistance in approximately 50% of patients.5 , 6 the use of circulating tumor ( ct ) dna for genotyping the tumor ( liquid biopsy ) offers clear advantages compared with repeated tumor tissue biopsies , including the minimally invasive method and no need for a tumor lesion accessible to biopsy . 
our objective was to determine the role of ctdna ras and braf mutations at the time of progression to anti - egfr therapy . methods study design and patient population the pulse and posiba studies were both prospective biomarker - design trials . 
patients were recruited into the pulse trial from november 2010 to april 2013 in 24 spanish centers and treated with infusional uorouracil , leucovorin , and oxaliplatin ( folfox ) - 6 plus panitumumab ( 6 mg / kg )  . 
patients were recruited into the posiba trial from july 2011 to may 2015 in 28 spanish centers and treated with folfox6 or uorouracil , leucovorin , and irinotecan ( folfiri ; at the investigators choice ) plus biweekly cetuximab ( 500 mg / m2 )  . in both trials , cytotoxic drugs were administered for 6 months , and anti - egfr monotherapy was continued until pd or unacceptable toxicity occurred . 
extended ras mutational analysis ( including kras / nras exons 2 , 3 , and 4 ) started in october 2013 in the pulse trial and in october 2015 in the posiba trial after protocol amendments . 
competitive allele - specic taqman pcr ( castpcr ; thermo fisher scientic , waltham , ma ) and an ultrasensitive sequencing technique ( digital polymerase chain reaction [ pcr ] ) were used to reanalyze tissue ras determination in patients with discrepancies between basal liquid biopsy ( mutation ) and formalin - xed parafn - embedded ( ffpe ) specimens ( wt )  . ctdna ras and braf mutational analysis this was an exploratory translational study with a primary objective of investigating measurement of ras and braf v600 - mutant ctdna in patients treated in the posiba and pulse trials using the idylla ctras and ctbraf mutation assay ( biocartis , jersey city , nj )  . 
plasma samples were collected basally , and serum samples were collected every 2 months in the pulse trial and every 3 months in the posiba trial , until pd was detected according to response evaluation criteria in solid tumors ( recist ) v1.1. 
two blood samples were analyzed for each patient for this study : a baseline plasma sample and a serum sample collected at the time of the last available determination . integrated ctdna purication and allele - specic quantitative pcr followed by automated data analysis was performed using the idylla ctkras and ctnras mutation assays to detect ras exon 2 , 3 , and 4 mutations and braf v600 mutations using 0.5 to 1 ml of plasma or serum per assay . 
the investigators who performed plasma genotyping were blinded to the clinical patient information . statistical analysis imaging was performed every 8 weeks in the pulse trial and every 12 weeks in the posiba trials and response was based on recist v1.1 as assessed by the investigators . progression - free survival ( pfs ) was dened as time from enrollment to disease progression ( recist criteria ) , death , or end of follow - up , whichever came rst . 
concordance was assessed using the kappa statistic and the characteristics of the diagnostic test using the sensitivity , specicity , and positive and negative predictive values by collapsing ras plus braf versus wt . 
statistical analysis was performed with spss statistics 22 ( spss , chicago , il ) and sas 9.4 software ( sas institute , cary , nc )  . results patient characteristics and concordance of baseline ras and braf mutation determination in plasma versus tissue the study ow chart is presented in figure 1 . 
kaplan - meier estimates of ( a ) progression - free survival and ( b ) overall survival , on the basis of ( c ) solid and ( d ) liquid biopsies . 
blood extraction was performed in group 1 ( between blood extraction and pd ) with a median ( p25 to p75 ) of + 7 days ( 1 to + 23 days ) and in group 2 with a median of 157 days ( 76 to 330 days ) , with the date of progression as the index date . the emergence of ras / braf mutations in ctdna was observed in 15 patients after initiation of therapy ( 11% ; appendix table a3 , online only )  . 
however , one of 11 patients ( 9% ) with acquired mutations in ctdna received anti - egfr compounds after disease progression compared with 22 of 79 ( 27.8% ) of those who remained free of mutations , potentially contributing to improved os . discussion our study indicates that ras and braf testing in baseline if not better , pfs and os ctdna results in a similar , discrimination compared with tissue testing in patients treated with rst - line chemotherapy plus anti - egfr therapy . 
 maurel et al 20116 20601 10019 10129 10140 10039 10027 10149 23209 10090 10153 20804 10131 10082 20401 10004 10159 20602 10006 10182 20306 10124 10115 21119 10122 22008 10167 22901 20611 10174 10126 10189 10147 22001 mutational status ( os bar ) : negativitzation no change overall response rate ( pfs bar ) : metastasectomy end of treatment liquid biopsy 1 , 000 1 , 200 1 , 400 time ( days ) fig 4 . 
progression - free survival ( pfs ) and overall survival ( os ) in patients with mutant ras and braf on basal liquid biopsy ( n = 34 )  . 
in a recent study with 43 patients , oncobeam demonstrated 72.1% concordance with tissue results , whereas idylla demonstrated 46.5% concordance with kras tissue results.15 finally , we observed that the subgroup of patients who had ras or braf mutations on tissue and wt on ctdna was enriched with patients with low tumor burden ( ldh , 1 uln )  . 
our results analyzing plasma samples at baseline and serum samples at progression differ with the analysis from the aspecct third - line phase iii panitumumab study , which showed that patients with emergent ras mutations at progression had similar pfs and os versus patients whose status remained wt at progression.19 in our study , patients with ras and braf with acquired mutations that were initially 2 wt showed signicantly poorer survival than those patients who remained wt at progression ; also , patients with disappearance of mutations showed better os . 
we have to note that patients in our study had been treated in rst - line therapy ( compared with third line in the aspecct trial ) and , therefore , second - line egfr therapies in truly sensitive patients ( those with liquid biopsies that remain wt ) would affect survival . 
moreover , we could not rule out that at pd , in patients with a poor prognosis ( identied by a high level of ldh at disease progression ) , we would have more chance to detect acquired mutations in ctdna . 
our study addresses most of the potential limitations from previous analyses , such as low number of patients , treatment heterogeneity ( including type of treatment and mixed rst , second , and third lines ) , and lack of a control group ( analysis of ras and braf in samples of patients without progression or before pd )  . 
 clinical impact of circulating tumor ras and braf mutations with rst - line therapy with currently accepted schedules of chemotherapy ( folfox and folfiri ) and approved antiegfr compounds ( cetuximab and panitumumab ) to establish differences between both groups ( 14% and 8% , respectively ; p = .47 ) , and global mutation acquisition was observed in only 11% of patients . 
this suggests that other mechanisms beyond ras and braf acquired mutations will probably play an important role , not only in the subset of patients without acquired ras and braf mutations , but also in the group of patients with acquired ras and braf mutations . 
n engl j med 360 : 1408 - 1417 , 2009 van cutsem e , lenz hj , k ohne ch , et al : fluorouracil , leucovorin , and irinotecan plus cetuximab treatment and ras mutations in colorectal cancer . 
j clin oncol 33 : 692 - 700 , 2015 douillard jy , siena s , cassidy j , et al : randomized , phase iii trial of panitumumab with infusional uorouracil , leucovorin , and oxaliplatin ( folfox4 ) versus folfox4 alone as rst - line treatment in patients with previously untreated metastatic colorectal cancer : the prime study . 
j clin oncol 28 : 4697 - 4705 , 2010 douillard jy , oliner ks , siena s , et al : panitumumab - folfox4 treatment and ras mutations in colorectal cancer . 
montagut c , dalmases a , bellosillo b , et al : identication of a mutation in the extracellular domain of the epidermal growth factor receptor conferring cetuximab resistance in colorectal cancer . 
montagut c , argil es g , ciardiello f , et al : efcacy of sym004 in patients with metastatic colorectal cancer with acquired resistance to anti - egfr therapy and molecularly selected by circulating tumor dna analyses : a phase 2 randomized clinical trial . 
jama oncol 4 : e175245 , 2018 pietrantonio f , vernieri c , siravegna g , et al : heterogeneity of acquired resistance to anti - egfr monoclonal antibodies in patients with metastatic colorectal cancer . 
clin cancer res 23 : 2414 - 2422 , 2017 diaz la jr , williams rt , wu j , et al : the molecular evolution of acquired resistance to targeted egfr blockade in colorectal cancers . 
siena s , sartore - bianchi a , garcia - carbonero r , et al : dynamic molecular analysis and clinical correlates of tumor evolution within a phase ii trial of panitumumab - based therapy in metastatic colorectal cancer . 
normanno n , esposito abate r , lambiase m , et al : ras testing of liquid biopsy correlates with the outcome of metastatic colorectal cancer patients treated with rst - line folfiri plus cetuximab in the capri - goim trial . 
grasselli j , elez e , carat `u g , et al : concordance of bloodand tumor - based detection of ras mutations to guide anti - egfr therapy in metastatic colorectal cancer . 
ann oncol 29 : 1211 - 1219 , 2018 jacobs b , claes b , pomella v , et al : analytical and clinical validation of the idylla ( cid : 1 ) ctkras and ctnras - braf liquid biopsy tests identies mcrc patient groups with high and low ctdna shedding . 
ras and braf mutational status in baseline plasma sample and secondary extraction serum sample : characteristics of patients with ctdna ras / braf mutation in baseline and second liquid biopsy plasma liquid biopsy ( basal ) serum liquid biopsy ( secondary ) , no . ras mutated braf mutated patient primary side basal liquid biopsy site of metastasis response surgery of second liquid metastasis biopsy maurel et al mutated braf mutated 2 wt total rectum kras ( a146p / t / v ) plus nras ( g13r / v ) liver left colon nras ( g13r / v ) liver , lung sigmoid kras ( g12d ) liver , lung sigmoid nras ( g13r / v ) liver , peritoneum sigmoid kras ( g12v ) node right side kras ( a146p / t / v ) local relapse sigmoid kras ( k117n ) liver , lung left colon kras ( g12v ) peritoneum rectum kras ( g12r ) liver , lung rectum kras ( k117n ) liver , lung right side braf ( v600e / d ) liver , peritoneum rectum nras ( q61h ) rectum braf ( v600e / d ) right side braf ( v600e / d ) kras ( g12d ) liver liver liver liver rectum kras ( a146p / t / v ) liver , node , suprarenal  . 
ras and braf mutational status in baseline plasma sample and secondary extraction serum sample : characteristics of patients with ctdna ras / braf mutation in baseline and second liquid biopsy ( continued ) serum liquid biopsy ( secondary ) , no . 22008 10122 10115 10006 20602 10004 10082 10153 22001 10189 10174 21119 10131 10090 rectum nras ( g61k ) liver , lung sigmoid nras ( g61r ) liver , lung right side kras ( a59t / e / g ) liver rectum kras ( a146p / t / v ) liver , lung left colon nras ( g61h ) liver , node , peritoneum  . 
 no evidence of increased risk of breast cancer in women with lynch syndrome identied by multigene panel testing jessica stoll , ms , cgc1 ; eric rosenthal , scm , phd2 ; shelly cummings , ms , cgc2 ; jamie willmott , ms , cgc2 ; ryan bernhisel , mstat2 ; and sonia s . 
kupfer , md1 purpose prior estimates of breast cancer risk in women with lynch syndrome ( ls ) range from population risk to 18 - fold increased risk with reported differences by gene . 
standardized incidence ratios ( sirs ) and 95% cis of breast cancer were calculated compared with age - matched incidence in the general us female population and with women negative for pvs stratied by the test indication . results in total , 0.8% of women ( 30 , 362 of 441 , 966 women ) carried mmr gene pvs . 
women with pvs in pms2 and msh6 were tested more frequently for hboc , whereas those with pvs in mlh1 and msh2 / epcam were tested more frequently for ls . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction breast cancer risk in lynch syndrome ( ls ) has been debated , with published data indicating anywhere from no increased risk1 - 4 up to 18 - fold increased risk for women with a pathogenic variant ( pv ) in a mismatch repair ( mmr ) gene.5 - 9 a recent laboratorybased study reported a 2to 3 - fold increased incidence of breast cancer in women with pvs in msh6 and pms2 compared with the general us female population , but not in mlh1 or msh2 carriers.10 these authors used us female population data from the seer registry ; however , comparing cancer histories in a population heavily weighted toward women being assessed for hereditary breast and ovarian cancer ( hboc ) to cancer histories in the general population could result in ascertainment bias.11 - 13 specically , this approach likely increases the proportion of the sample with a personal diagnosis of breast cancer , resulting in elevated breast cancer rates regardless of mmr gene status . 
this ascertainment bias might be less evident for women with pvs in the higher penetrance mmr genes ( ie , mlh1 , msh2 , and epcam ) who are more likely to be ascertained for testing on the basis of personal or family history of early - onset colorectal or endometrial cancer or other ls - associated cancers . therefore , to properly estimate cancer risk , women with pvs should be compared with pv - negative women within the same testing population . quantifying breast cancer risk in women with ls has signicant implications for screening and risk reduction , especially for patients with ls caused by pvs in msh6 and pms2 , which are more prevalent than previously thought . 
 stoll et al context key objective using a large , laboratory - based database , we determined whether women with lynch syndrome ( ls ) are at increased risk of breast cancer compared with the general population and to a population undergoing genetic testing . knowledge generated women with ls are not at increased risk of breast cancer . 
these ndings are in line with results from the prospective ls database but contrast with other laboratory - based studies . relevance these ndings support average - risk breast cancer screening in women with ls . ascertained for suspicion of hboc and / or ls but were not found to have a pv by multigene panel testing . methods study population women tested with a single commercial laboratorys ( myriad genetic laboratories , salt lake city , ut ) multigene panel between september 2013 and november 2018 were included unless they resided in a state prohibiting use of deidentied genetic or clinical information for research . 
clinical and demographic data for participants were obtained from test request forms submitted by ordering health care providers . ls - associated cancers included colorectal , endometrial , ovarian , pancreatic , stomach , gastric , ureter , brain , small intestine , and biliary tract cancers . 
hboc - associated cancers included breast , ovarian , prostate , and pancreatic cancers . testing criteria individuals met providers indicated on the test requisition forms whether testing was ordered for suspicion of ls or hboc . 
for hboc , 2013 national comprehensive cancer network ( nccn ) guidelines were used , 14 but the contribution of prostate cancer was excluded because gleason score or metastatic disease information was not collected reliably . these exclusions were not expected to substantially inuence results but may have resulted in an underestimate of the number of women meeting hboc criteria . 
to directly evaluate rates against the recent publication that established a 2to 3fold elevated breast cancer incidence for msh6 and pms2 , 10 the us female population from the seer registry17 was used as one comparator group . 
to compensate for the ascertainment bias expected in a population selected for testing on the basis of suspicion of hereditary cancer risk , we also calculated the sirs using the following 3 additional comparator populations : women who tested negative for any pv who were ascertained for suspicion of hboc or ls ; women who were ascertained for hboc only ; and women who were ascertained for ls only . 
all analyses were performed using sas software ( sas institute , cary , nc )  . results demographic and clinical characteristics in total , 441 , 996 women met inclusion criteria ( appendix table a1 )  . 
among these , 3 , 362 women ( 0.8% ) were found to carry a single pv in an mmr gene ( mlh1 , msh2 , msh6 , pms2 , or epcam ) , and 438 , 634 women ( 99.2% ) were negative for pvs in any of the other genes included on the panel . 
epcam deletions were identied in only 11 women and therefore were included with msh2 for all analyses . demographic and clinical characteristics for women with mmr gene pv and all women tested are listed in table 1 . for women with an mmr gene pv , median age at testing was 47 years , and 56.8% of women reported white or caucasian ancestry . 
demographic and clinical characteristics of women with mmr gene pvs and all women undergoing multigene panel testing all women tested ( n = 441 , 996 ) women with mmr gene pv ( n = 3 , 362 ) characteristic age at testing , yearsa mean ( sd ) range mean ( sd ) range age at bc diagnosis , yearsb self - reported ancestry , no . 
similar differences in mutation spectrum were found for women meeting nccn testing criteria for ls versus hboc ( fig 1 )  . the majority of mlh1 and msh2 / epcam mutation carriers were ascertained for clinical suspicion of ls , whereas msh6 and pms2 mutation carriers were more commonly ascertained for suspicion of hboc ( fig 2 )  . phenotypic spectrum the majority of women with pvs in mlh1 and msh2 / epcam were affected by cancer , whereas most pms2 carriers were unaffected . 
for msh2 / epcam carriers , endometrial and colorectal cancers were the most common cancers reported ( n = 162 [ 24.8% ] and n = 150 [ 23.0% ] , respectively )  . 
carriers of mlh1 and msh2 / epcam pvs had lower rates of breast cancer , whereas there was no difference in sirs for msh6 or pms2 carriers compared with seer population breast cancer rates ( table 2 )  . table 3 lists sirs for women with mmr gene pvs compared with women with negative panel testing . 
when all women ascertained for hboc or ls were analyzed , breast cancer rates were lower in women with pvs in mmr genes . specically , breast cancer rates ranged from 22% to 50% lower than expected among the various mmr genes . 
similarly , when compared with women ascertained for suspicion of ls , breast cancer rates also did not differ between women with mmr gene pvs compared with pv - negative women . 
distribution of pathogenic variants ( pvs ) by mismatch repair gene on the basis of ascertainment for testing indicated by ordering provider and testing criteria met ( mlh1 , n = 462 ; msh2 / epcam , n = 653 ; msh6 , n = 985 ; pms2 , n = 1 , 262 )  . 
prevalence of mismatch repair pathogenic variants by ascertainment for lynch syndrome ( ls ) and hereditary breast and ovarian cancer syndrome ( hboc ) testing as indicated by ordering provider ( mlh1 , n = 462 ; msh2 / epcam , n = 653 ; msh6 , n = 985 ; pms2 , n = 1 , 262 )  . discussion data from multigene panel testing in ls have called into question the unresolved issue of whether breast cancer risk is increased in ls . 
although there is a wealth of existing literature on breast cancer in ls , data from these studies are conicting , with risk estimates ranging from no increased risk1 - 4 up to 18 - fold increased risk.5 - 9 recent studies report an increased breast cancer risk in women with pvs in msh6 and pms2 , but not in mlh1 and msh2 / epcam , 10 or an increased risk of breast cancer exclusive to msh6.19 in the present laboratory - based study , including a large sample of msh6 and pms2 pv carriers , previously published data showing an increased breast cancer risk in women with pvs in msh6 and / or pms2 were not replicated when the same methodology was used.10 moreover , the rate of breast cancer was found to be lower than expected among mlh1 and msh2 / epcam carriers . 
findings from the current study are in line with a recent report from the prospective ls database.20 the ndings in the current study likely differ from previous studies showing increased breast cancer risk in ls for several reasons . 
first , the current study includes the largest number of mmr gene pv carriers reported to date , including large numbers of msh6 and pms2 carriers , thereby increasing precision in breast cancer risk estimates compared with more moderately sized studies . 
moreover , this sample included a large proportion of women unaffected by cancer , which appropriately shifts the breast cancer estimates closer to those of the general us female population . colon endometrial breast ovarian other * unaffected mlh1 msh2 / epcam msh6 pms2 no mutation fig 3 . 
in these analyses , no difference in breast cancer incidence was found among women with or without mmr gene pvs whether they were ascertained for suspicion of hboc or ls . 
these results support current guidelines to follow average - risk breast cancer screening recommendations in all women with ls.22 consistent with ndings from other laboratory and population - based studies , these data demonstrate that pvs in msh6 and pms2 account for a much higher proportion of ls than previously estimated.10 , 23 also similar to previous studies , 23 , 24 this study found that the current ls testing criteria perform reasonably well for women with pvs in mlh1 and msh2 but miss close to half of women with pvs in msh6 and pms2 . 
 no increased breast cancer risk in lynch syndrome these results suggest that current clinical criteria are insufcient for identication of the full spectrum of patients with ls who would benet from appropriate surveillance.25 one limitation inherent to utilization of a laboratory - based testing population is that clinical information was limited to that which was included on the test requisition form as provided by ordering clinicians and therefore may not be wholly inclusive of individuals personal and family histories . 
however , we obtained essentially the same ndings through comparisons between different populations within this study , suggesting that underor overreporting of cancer history in any of these populations did not affect the ndings . 
although the study was designed specically to address ascertainment bias , the population included only women undergoing genetic testing for clinical suspicion of a hereditary cancer syndrome and may not be representative of the more general population with ls . however , this was at least in part mitigated by the fact that the comparator population was from the same testing population to ensure that any population differences between women with and without pvs were valid . in the largest study of mmr gene pv carriers identied by a multigene panel through a commercial laboratory , there was no evidence of increased breast cancer risk in women with pvs in mmr genes compared with the general us female population or with woman undergoing multigene panel testing . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . jessica stoll consulting or advisory role : invitae travel , accommodations , expenses : invitae eric rosenthal employment : myriad genetic laboratories stock and other ownership interests : myriad genetic laboratories shelly cummings employment : myriad genetics stock and other ownership interests : myriad genetics travel , accommodations , expenses : myriad genetics jamie willmott employment : myriad genetics stock and other ownership interests : myriad genetics research funding : myriad genetics travel , accommodations , expenses : myriad genetics ryan bernhisel employment : myriad genetics sonia s . 
kupfer honoraria : advance medical no other potential conicts of interest were reported . references baglietto l , lindor nm , dowty jg , et al : risks of lynch syndrome cancers for msh6 mutation carriers . 
j natl cancer inst 102 : 193 - 201 , 2010 pande m , wei c , chen j , et al : cancer spectrum in dna mismatch repair gene mutation carriers : results from a hospital based lynch syndrome registry . 
mller p , sepp al a tt , bernstein i , et al : cancer risk and survival in path_mmr carriers by gene and gender up to 75 years of age : a report from the prospective lynch syndrome database . 
gut 67 : 1306 - 1316 , 2018 therkildsen c , ladelund s , smith - hansen l , et al : towards geneand gender - based risk estimates in lynch syndrome ; age - specic incidences for 13 extracolorectal cancer types . 
 stoll et al oliveira ferreira f , napoli ferreira cc , rossi bm , et al : frequency of extra - colonic tumors in hereditary nonpolyposis colorectal cancer ( hnpcc ) and familial colorectal cancer ( fcc ) brazilian families : an analysis by a brazilian hereditary colorectal cancer institutional registry . 
fam cancer 3 : 41 - 47 , 2004 scott rj , mcphillips m , meldrum cj , et al : hereditary nonpolyposis colorectal cancer in 95 families : differences and similarities between mutation - positive and mutation - negative kindreds . 
win ak , young jp , lindor nm , et al : colorectal and other cancer risks for carriers and noncarriers from families with a dna mismatch repair gene mutation : a prospective cohort study . 
j clin oncol 30 : 958 - 964 , 2012 goldberg m , bell k , aronson m , et al : association between the lynch syndrome gene msh2 and breast cancer susceptibility in a canadian familial cancer registry . 
harkness ef , barrow e , newton k , et al : lynch syndrome caused by mlh1 mutations is associated with an increased risk of breast cancer : a cohort study . j med genet 52 : 553 - 556 , 2015 genet med 20 : 1167 - 1174 , 2018 10 . 
2018 : is breast cancer truly caused by msh6 and pms2 variants or is it simply due to a high prevalence of these variants in the population ? genet med 21 : 256 - 257 , 2019 12 . 
evans dg , woodward er , lalloo f , et al : are women with pathogenic variants in pms2 and msh6 really at high lifetime risk of breast cancer ? genet med , 2018 13 . 
dominguez - valentin m , sampson jr , sepp al a tt , et al : cancer risks by gene , age , and gender in 6350 carriers of pathogenic mismatch repair variants : findings from the prospective lynch syndrome database . 
giardiello fm , allen ji , axilbund je , et al : guidelines on genetic evaluation and management of lynch syndrome : a consensus statement by the us multisociety task force on colorectal cancer . 
 patterns of metastatic spread and mechanisms of resistance to crizotinib in ros1 - positive nonsmall - cell lung cancer purpose the ros1 tyrosine kinase is activated through ros1 gene rearrangements in 1% to 2% of nonsmall - cell lung cancers ( nsclcs ) , which confer sensitivity to treatment with the anaplastic lymphoma kinase ( alk ) / ros1 / mesenchymal - epithelial transition factor inhibitor crizotinib . 
currently , insights into patterns of metastatic spread and mechanisms of crizotinib resistance among patients with ros1 - positive disease are limited . patients and methods we reviewed clinical and radiographic imaging data of patients with ros1and alk - positive nsclc to compare patterns of metastatic spread at initial metastatic diagnosis . 
to determine molecular mechanisms of crizotinib resistance , we analyzed repeat biopsy specimens from a cohort of patients with ros1 - positive disease who progressed on crizotinib . results we identified 39 and 196 patients with advanced ros1and alk - positive nsclc , respectively . 
ros1 mutations included g2032r ( 41% ) , d2033n ( 6% ) , and s1986f ( 6% )  . conclusion compared with alk rearrangements , ros1 rearrangements are associated with lower rates of extrathoracic metastases , including fewer brain metastases , at initial metastatic diagnosis . 
2017 by american society of clinical oncology introduction treatment paradigms for advanced nonsmallcell lung cancer ( nsclc ) continue to evolve and reflect a growing understanding of the genetic underpinnings of the disease . 
subsequent work has shown that such rearrangements are present in 1% to 2% of nsclcs and define a distinct molecular subgroup.2 - 4 of note , ros1 is phylogenetically related to the anaplastic lymphoma kinase ( alk ) receptor tyrosine kinase.5 thus , like alk rearrangements in nsclc , 6 , 7 ros1 fusions confer sensitivity to the alk / ros1 / mesenchymal - epithelial transition factor inhibitor crizotinib.3 in profile 1001 ( study of oral pf - 02341066 , a c - met / hepatocyte growth factor tyrosine kinase inhibitor , in patients with advanced cancer ) , crizotinib produced an objective response rate justin f . 
shaw author affiliations and support information ( if applicable ) appear at the end of this article . presented at the 2016 american society of clinical oncology annual meeting , chicago , il , june 3 - 7 , 2016 . corresponding author : alice t . 
on the basis of this activity , the us food and drug administration expanded crizotinibs approval to include patients with advanced , ros1 - positive nsclc.12 consistent with these reports , we observed several prolonged responses to crizotinib among patients with ros1 - positive nsclc at our institution . specifically , we observed particularly durable responses among patients with intrathoracic - only disease ( ie , m1a disease ) , 3 which led us to hypothesize that differences in malignant phenotypes between ros1 and alk rearrangements , including differences in patterns of metastatic spread , affect therapeutic outcomes . 
in one early study , doebele et al13 reported that alk rearrangements are associated with pericardial , pleural , and liver metastases compared with an egfr / kras / alk wild - type cohort . 
outside this report , however , few studies have evaluated patterns of metastatic spread according to molecular genotype in nsclc , and none have focused on ros1.14 , 15 in this study , we investigated the distribution of malignant disease at initial metastatic diagnosis and evaluated associations with clinical outcomes in ros1 - positive nsclc . 
data were updated as of january 2016 . all studies were performed under an institutional review boardapproved protocol . pfs was measured from the time of crizotinib initiation to investigator - assessed , radiographic progression or death in the absence of documented progression . 
overall survival ( os ) was measured from initiation of crizotinib until death . patients without a known date of death were censored at the time of last follow - up . in addition , patients with ros1 - positive nsclc who underwent repeat biopsies / resection of progressing lesions on crizotinib between july 2012 and december 2016 were identified . 
age and lines of therapy were analyzed by wilcoxon rank sum test . the kaplan - meier method was used to estimate pfs and os medians and probabilities , and the log - rank test was used to compare their differences between groups . 
no significant differences in baseline clinicopathologic characteristics were observed between groups ( data supplement ) , including no difference in the median number of prior lines of therapy before crizotinib ( median , 1 ; data supplement )  . 
to address whether this difference was confounded by prior therapy , we examined pfs among patients who received second - line crizotinib ( ie , after one prior therapy ) because this was the most common line of crizotinib in both cohorts ( ros1 , 60% ; alk , 42% )  . 
of note , 101 patients with alk - positive nsclc ( 58% ) received secondor thirdgeneration alk inhibitors after crizotinib , whereas only seven patients with ros1 - positive nsclc ( 23% ) received additional ros1 inhibitors ( p , .001 ; data supplement )  . 
thus , the longer median pfs with crizotinib among patients with ros1 - positive disease may have been partly offset by greater access to next - generation targeted therapies among patients with alk - positive disease . sites of metastatic disease to determine whether these clinical outcomes may have also been affected by distribution of metastatic disease , we compared sites of disease at initial metastatic diagnosis among patients with alkand ros1 - positive nsclc . 
metastatic involvement of a given anatomic site was determined on the basis of clinical staging ( tnm seventh edition ) .30 positron emission tomography - computed tomography ( ct ) and ct scans of the chest , abdomen , and pelvis were performed in 72% and 26% of patients with alk - positive nsclc and 82% and 18% of patients with ros1 - positive nsclc , respectively ( table 1 )  . 
brain magnetic resonance imaging ( alk , 76% ; ros1 , 82% ) or a head ct scan with intravenous contrast ( alk , 9% ; ros1 , 10% ) were also performed in most patients . 
in addition to having a lower rate of brain metastases at initial diagnosis , fewer patients with ros1 - positive nsclc developed brain metastases over time compared with those with alk - positive nsclc . 
the cumulative incidence of brain metastasis among patients with alkand ros1 - positive disease was 73% and 34% , respectively , at 5 years after initial metastatic diagnosis ( p , .001 ; fig 3a )  . 
percentages may not add to 100 because of rounding . abbreviations : ct , computed tomography ; ecog , eastern cooperative oncology group ; mri , magnetic resonance imaging ; pet , positron emission tomography . * includes one patient with adenosquamous histology . on the basis of performance status at initial metastatic presentation or at the first documented assessment . 
performance status was not available in four patients with alk - positive disease and one patient with ros1 - positive disease . systemic staging and neuroimaging studies were not done or were not available for review in five and 35 patients with alk - positive disease , respectively . 
four patients with alk - positive disease had both a brain mri and a head ct scan . neuroimaging studies were not done or not available for review in three patients with ros1 - positive disease . time was also greater among those with alkpositive disease ( 56% v 22% at 5 years ; p = .001 ; fig 3b )  . 
of note , 101 patients with alk - positive nsclc ( 58% ) received next - generation alk inhibitors ( ceritinib , 40% ; alectinib , 27% ; brigatinib , 3% ) after crizotinib ( data supplement ) ; however , 93% of these patients received such agents after the initial development of brain metastases . 
collectively , these findings suggest that alk - positive cancers have an increased tropism for the brain compared with ros1 - positive nsclcs . next , we evaluated outcomes of crizotinib treatment according to the presence of extrathoracic metastases ( ie , m1a v m1b disease )  . 
thus , this difference in pfs for crizotinib treatment outcomes between patients with alkand ros1 - positive nsclc in the overall study population may have been partly driven by the higher frequency of m1a disease among those with ros1 - positive disease because this group appears to derive greater benefit with crizotinib . ros1 : crizotinib resistance despite the effectiveness of crizotinib in alkand ros1 - positive nsclc , most patients acquire resistance . 
to investigate potential mechanisms of resistance to crizotinib in ros1 - positive nsclc , we analyzed postprogression biopsy specimens from patients with ros1 - positive disease who progressed on crizotinib treatment . 
all patients underwent tissue sampling within 7 days of crizotinib discontinuation . persistence of the original ros1 rearrangement was observed in nine ( 100% ) of nine postcrizotinib specimens available for testing ( repeat fish [ n = 2 ] , rt - pcr [ n = 5 ] , or ngs [ n = 2 ] )  . 
 ( d ) os as measured from the time of crizotinib initiation in the second - line setting . time since crizotinib initiation ( months ) time since crizotinib initiation ( months ) no . 
thus , ros1 resistance mutations were detected in a majority ( 10 [ 62.5% ] of 16 ) of patients with crizotinib resistance . because crizotinib has limited blood - brain barrier penetration , 31 we analyzed crizotinib - resistant samples by site of disease . 
among non - cns specimens ( n = 14 ) , the frequency of ros1 resistance mutations was 64% ( appendix fig a2 ) , with 50% of specimens harboring the ros1 g2032r mutation . 
among six specimens that underwent targeted ngs with the mgh snapshot platform , none was found to have high - level copy number changes in any analyzed gene ( data supplement )  . 
 a mgh047 - 5 ros1 g2032r mgh9018 - 1 ros1 wt biopsy ros1 wt ros1 wt ros1 g2032r ros1 g2032r ros1 g2032r ros1 s1986f ros1 g2032r * ros1 wt ros1 wt ros1 wt * mgh070 - 1 mgh096 - 1 mgh077 - 1 mgh080 - 2 mgh998 - 1 mgh508 - 1 mgh095 - 1 mgh996 - 1 mgh943 - 1 mgh995 - 1 mgh933 - 1 mgh081 - 1 mgh968 - 1 mgh986 - 1 fig 4 . 
mgh , massachusetts general hospital ; wt , wild type . g2032r ros1 d2033n ros1 wt ( 2 sites ) ros1 g2032r s1986f d2033n progression - free survival ( months ) ros1 g2032r discussion we observed that despite shared clinical features between ros1and alk - positive nsclcs , these genetic alterations were associated with different patterns of metastatic spread . 
although the shorter pfs with crizotinib treatment among patients with alk - positive nsclc may have been an influence in this series , we observed significantly higher rates of brain metastases at initial diagnosis ( ie , before exposure to crizotinib ) in this group . together , these observations suggest that alkrearranged nsclcs have a greater tropism for the cns . 
the majority of patients with alkpositive disease who developed brain metastases did so before receiving more cns penetrable , next - generation alk inhibitors , which provides an additional rationale for investigating the upfront use of next - generation alk inhibitors to prevent or delay the emergence of brain metastases . 
several ongoing first - line studies are comparing crizotinib with second - generation alk inhibitors ( eg , alex [ study comparing alectinib with crizotinib in treatment - naive anaplastic lymphoma kinasepositive advanced nonsmall cell lung cancer participants ] , alta - 1l [ phase iii study of brigatinib versus crizotinib in alk - positive advanced non small - cell lung cancer patients ] ) and have generally incorporated secondary end points focused on intracranial disease activity . one limitation of this analysis is that we observed a relatively higher frequency of baseline brain metastases in the alk - positive cohort than had other studies.6 , 13 although this observation may reflect differences in local imaging practices or referral patterns , such factors would have likely affected both alk and ros1 cohorts . 
nonetheless , several other studies have shown a comparable pfs to our series.8 - 11 of note , although patients with ros1 - positive disease had a longer median pfs with crizotinib treatment than patients with alk - positive disease , no difference in os was found between cohorts . 
we cannot exclude the possibility that this was due to unaccounted - for differences in patient characteristics , although the higher rates of next - generation targeted therapy use among patients with alk - positive disease may have offset the longer pfs with crizotinib treatment among patients with ros1positive disease . despite the significant activity of crizotinib , acquired resistance remains a challenge for patients with alkand ros1 - positive nsclc alike.16 , 43 - 45 thus far , insights into the mechanisms of resistance to crizotinib among those with ros1 - positive disease have been limited and generally consist of isolated case reports , small series , and preclinical evaluations.16 - 19 , 46 to date , seven different ros1 resistance mutations have been described.16 - 19 , 46 in addition , upregulation of bypass signaling pathways ( eg , egfr , ras , kit ) have also been reported.20 - 22 , 47 to our knowledge , we present the largest study of crizotinib resistance in ros1 - positive nsclc to date , which has found ros1 resistance mutations in a majority of specimens . 
 emerged through selection of pre - existing clones or through genetic evolution of drugtolerant cells.48 despite similarities between alk and ros1 , each has a different frequency and spectrum of on - target mechanisms of crizotinib resistance . 
indeed , patients with ros1 - positive nsclc have a much higher frequency of on - target resistance mutations , but such mutations are concentrated in a narrower segment of the kinase , which perhaps reflects the greater potency of crizotinib for ros1 than for alk . potential limitations of this analysis are that several different genotyping platforms were used . 
thus , we may have overlooked ros1 mutations outside this region . however , all specimens that underwent sanger sequencing and / or deep sequencing ( n = 8 ) were evaluated for mutations across the entire ros1 kinase domaanother important limitation is that we were unable to identify a mechanism of crizotinib resistance in all patients . 
thus , additional studies are necessary to elucidate other potentially target - independent mechanisms of crizotinib resistance . in alk - positive nsclc , second - generation alk inhibitors demonstrate significant activity in the crizotinib - resistant setting largely as a result of their greater potency against alk compared with crizotinib . 
beyond cabozantinib and tpx - 0005 , several other agents with ros1 activity are being evaluated , including entrectinib ( clinicaltrials.gov identifier nct02097810 ) , 53 ds - 6051b ( clinicaltrials.gov identifier nct02279433 ) , and lorlatinib ( clinicaltrials.gov identifier nct01970865 ) , 50 , 54 but these agents have not demonstrated clinical activity against ros1 g2032r to date ( data supplement )  . in summary , despite a shared susceptibility to crizotinib , alk and ros1 rearrangements differ in distributions of metastatic disease . 
nonetheless , acquired resistance to crizotinib remains a significant challenge for both molecular subsets . among patients with ros1 - positive nsclc , ros1 mutations ( most notably g2032r ) are the predominant mechanisms of resistance to crizotinib , which underscores the need for clinical development of next - generation ros1 inhibitors with activity against this mutation . 
provisional application to the us patent and trademark office ( application number 61817229 ) satoshi yoda no relationship to disclose ibiayi dagogo - jack no relationship to disclose luc friboulet no relationship to disclose jessica j . 
hubbeling no relationship to disclose leila dardaei no relationship to disclose james hardwick employment : pfizer stock and other ownership interests : pfizer travel , accommodations , expenses : pfizer donghui huang employment : pfizer stock and other ownership interests : pfizer travel , accommodations , expenses : pfizer mari mino - kenudson consulting or advisory role : merrimack , h3 biomedicine , acd pharmaceuticals , roche , genentech a . 
john iafrate stock and other ownership interests : archer biosciences consulting or advisory role : debiopharm group , constellation pharmaceuticals , chugai pharma , roche research funding : blueprint medicines patents , royalties , other intellectual property : archerdx exclusive license to amp technology anna f . 
farago honoraria : foundation medicine consulting or advisory role : pharmamar , merrimack , takeda pharmaceuticals , abbvie , intervention insights travel , accommodations , expenses : pharmamar , abbvie , stemcentrx aaron n . 
ferris no relationship to disclose zofia piotrowska consulting or advisory role : boehringer ingelheim , astrazeneca , ariad pharmaceuticals , takeda pharmaceuticals , superdimension research funding : guardant health ( inst ) alice t . 
shaw honoraria : pfizer , novartis , roche , genentech , foundation medicine consulting or advisory role : pfizer , novartis , genentech , roche , ariad pharmaceuticals , ignyta , blueprint medicines , daiichi sankyo , emd serono , taiho pharmaceutical , ksq therapeutics research funding : pfizer , novartis , roche , genentech acknowledgment we thank cyril h . 
shaw at , kim dw , nakagawa k , et al : crizotinib versus chemotherapy in advanced alk - positive lung cancer . med 371 : 2167 - 2177 , 2014 n engl j med 368 : 2385 - 2394 , 2013 8 . 
moro - sibilot d , faivre l , zalcman g , et al : crizotinib in patients with advanced ros1 - rearranged nonsmall - cell lung cancer ( nsclc ) : preliminary results of the acse phase ii trial . 
goto k , yang j , kim d , et al : phase ii study of crizotinib in east asian patients ( pts ) with ros1 - positive advanced nonsmall - cell lung cancer ( nsclc )  . 
russo a , franchina t , picone a , et al : different metastatic pattern according to the egfr mutational status in a cohort of lung adenocarcinomas ( adcs ) : a single - institution report . 
facchinetti f , loriot y , kuo ms , et al : crizotinib - resistant ros1 mutations reveal a predictive kinase inhibitor sensitivity model for ros1and alk - rearranged lung cancers . 
drilon a , somwar r , wagner jp , et al : a novel crizotinib - resistant solvent - front mutation responsive to cabozantinib therapy in a patient with ros1 - rearranged lung cancer . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
shaw at , yeap by , mino - kenudson m , et al : clinical features and outcome of patients with nonsmall - cell lung cancer who harbor eml4 - alk . 
goldstraw p , crowley j , chansky k , et al : the iaslc lung cancer staging project : proposals for the revision of the tnm stage groupings in the forthcoming ( seventh ) edition of the tnm classification of malignant tumours . 
gainor jf , ou sh , logan j , et al : the central nervous system as a sanctuary site in alk - positive nonsmall - cell lung j clin oncol 29 : e443 - e445 , 2011 cancer . 
soria jc , tan ds , chiari r , et al : first - line ceritinib versus platinum - based chemotherapy in advanced alkrearranged nonsmall - cell lung cancer ( ascend - 4 ) : a randomised , open - label , phase 3 study . 
gadgeel sm , shaw at , govindan r , et al : pooled analysis of cns response to alectinib in two studies of pretreated patients with alk - positive nonsmall - cell lung cancer . 
crin `o l , ahn mj , de marinis f , et al : multicenter phase ii study of whole - body and intracranial activity with ceritinib in patients with alk - rearranged nonsmall - cell lung cancer previously treated with chemotherapy and crizotinib : results from ascend - 2 . 
woo cg , seo s , kim sw , et al : differential protein stability and clinical responses of eml4 - alk fusion variants to various alk inhibitors in advanced alk - rearranged nonsmall cell lung cancer . 
huber kv , salah e , radic b , et al : stereospecific targeting of mth1 by ( s ) - crizotinib as an anticancer strategy . nature 508 : 222 - 227 , 2014 42 . 
shaw a , camidge d , engelman j , et al : clinical activity of crizotinib in advanced nonsmall - cell lung cancer ( nsclc ) harboring ros1 gene rearrangement . 
zou hy , li q , engstrom ld , et al : pf - 06463922 is a potent and selective next - generation ros1 / alk inhibitor capable of blocking crizotinib - resistant ros1 mutations . 
cui j , rogers e , zhai d , et al : ending the endless acquired tyrosine kinase resistance mutationsdesign of tpx0005 , a multi - target alk / ros1 / trk inhibitor with broad spectrum activity against wild - type and mutants including alk g1202r , ros1 g2032r , and trka g595r . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multi - targeted pan - trk , ros1 , and alk inhibitor entrectinib ( rxdx - 101 ) : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . cancer discov 7 : 400 - 409 , 2017 54 . 
solomon b , bauer t , felip e , et al : safety and efficacy of lorlatinib ( pf - 06463922 ) from the dose - escalation component of a study in patients with advanced alk + or ros1 + nonsmall - cell lung cancer ( nsclc )  . 
progressionfree survival ( pfs ) of alkand ros1 - positive patients with ( a ) m1a and ( b ) m1b disease . time since crizotinib initiation ( months ) time since crizotinib initiation ( months ) no . 
fish , phd1 , 3 , 4 introduction immune checkpoint inhibitors ( icis ) have signicantly improved advanced cancer outcomes.1 , 2 although icis unleash antitumor immune responses , negating natural immune inhibitory mechanisms can result in the development of self - reactive immune cells and an array of immune - related adverse events ( iraes ) .3 although reports of serious myocarditis have emerged , 4 - 9 data on long - term outcomes following an episode of ici - associated myocarditis are limited and molecular analyses on surviving patients are lacking . 
here , we report a case of recurrent myocarditis in a patient previously treated with a programmed death ligand 1 ( pd - l1 ) inhibitor ( durvalumab ) , an ici that blocks the binding of pd - l1 to programmed cell death protein 1 and cd80.10 molecular investigations revealed cytokine modulations suggestive of a sustained t - helper 1 ( th1 ) - like cellular immune response as well as unique antigen - bound serum autoantibodies , highlighting a induction of potential autoantibody production in iraes . role for th1 - cell - dependent case initial presentation a 67 - year - old woman presented to the emergency department with severe sudden - onset chest pain 2 days after receiving the 12th cycle of pd - l1 inhibitor ( 48 weeks after starting ici ) for the treatment of metastatic urothelial carcinoma ( fig 1a )  . 
she was previously treated for remote triple - negative right - sided breast invasive ductal carcinoma with surgery ; cyclophosphamide , epirubicin , and 5 - uorouracil chemotherapy ; and radiation . 
her treatment was largely uneventful , with only a noted diagnosis of hypothyroidism after receiving the 7th cycle of pd - l1 inhibitor , which was treated with hormone replacement therapy without interruption of ici . although the patient was hemodynamically stable , cardiac laboratory investigations revealed high - sensitivity troponin i levels were elevated at 4 , 114 ng per l ( reference range , , 26 ng per l ) , and brain natriuretic peptide levels ( bnp ) were elevated at 2 , 275 pg per ml ( reference range , , 100 pg per ml ) ( figs 1b and 1c , data supplement )  . 
2d echocardiogram demonstrated severely decreased biventricular systolic function , with a left ventricular ejection fraction ( lvef ) of 20% , right ventricular ( rv ) fraction area change of 22% , and a left ventricular ( lv ) thrombus ( fig 1d and video 1 )  . 
with a history of ici treatment , together with clinical , ecg ( fig 2a ) , and imaging ndings , a diagnosis of ici - associated myocarditis was made . 
treatment with intravenous methylprednisolone ( 2 mg / kg / d ) , furosemide , betablocker , angiotensin - converting enzyme inhibitor , and low - molecular - weight heparin was initiated . 
cardiovascular magnetic resonance ( cmr ) imaging conrmed severe biventricular dysfunction , mild pericardial effusion , and demonstrated late gadolinium enhancement ( lge ) involving the basal and apical segments predominantly in a subepicardial distribution ( video 2 , data supplement )  . 
follow - up ecg remained abnormal with low - voltage qrs complex as well as persistent st elevation ( fig 2b )  . the patient was discharged home in stable condition on 90 mg oral prednisone with a plan to taper and discontinue in 8 weeks . 
 echocardiogram ( apical the patient demonstrating four chamber view ) of biventricular dysfunction as well as a focused apex view with contrast showing a thrombus ( admission )  . case report evidence of pulmonary emboli , whereas whole - body computed tomography scanning showed no evidence of metastatic disease . 
there was signicant clinical recovery 1 month after discharge , with echocardiography revealing partial recovery of lv function ( lvef = 40% ; global longitudinal strain = 17.1% ) ; however , rv systolic function remained severely reduced ( rv fraction area change 17% , data supplement )  . 
ecg remained abnormal with low - voltage qrs , however , now with right bundle branch block ( fig 2c )  . recurrent presentation four months after the initial event , and without resumption of ici treatment , the patient presented to the cardiology clinic with extreme fatigue . 
she was admitted and a subsequent cmr conrmed the severity of lv dysfunction , multiple new lv thrombi , larger pericardial effusion , and a mild interval worsening of nonischemic pattern lge ( data supplement )  . a cardiac biopsy ( figs 2e and 2f ) conrmed the diagnosis of myocarditis with predominantly t cells ( fig 2g ) and macrophages ( fig 2h ) ; polymerase chain reaction was negative for cardiotropic viruses.11 given the biopsy result , she was diagnosed with recurrence of ici - associated myocarditis . 
she deteriorated and subsequently succumbed to heart failure a year - and - a - half later . methods the patient was enrolled in this research ethics boardapproved case report at the university health network after obtaining informed written consent . 
next - generation sequencing ( immunoseq ) , cytokine multiplex assays , targeted microrna proling , and a mass spectrometry - based assay to identify serum autoantibody complexes with their cognate antigens were performed ( for a detailed description of the methods , see the data supplement )  . results analysis of the distribution , clonality , and diversity of t - cell receptors pre - recurrence ( january ) and during treatment for recurrence of myocarditis ( march onward ) with immunosuppressants revealed limited clonal modulation ( data supplement )  . 
multiplex analysis of cytokines ( luminex , austin , tx ) in serum revealed remarkably high concentrations of t - cellderived cytokines during recurrence despite withdrawal of ici therapy and initiation of immunosuppressants . 
substratifying by t - helper ( th ) cell subtype revealed that there was an apparent dominance of th1 - cellenriched cytokines over th2 - cellenriched cytokines ( figs 3a and 3b ; data supplement )  . quantication of 92 micrornas ( fluidigm , san francisco , ca ) with known inammatory and cardiac roles revealed two micrornas ( mir - 130a - 3p and mir - 122 - 5 ) that displayed consistent upregulation and downregulation , respectively , in parallel with circulating cytokine abundance . 
increases in mir - 130a - 3p ( figs 3b and 3c ) appeared to correlate with declines in interleukin ( il ) - 4 , 12 whereas decreases in mir122 - 5p , a noted negative regulator of il - 1 , appeared to be associated with elevations in il - 1 ( figs 3a and 3c ) .13 principal component and pathway analysis of differentially regulated micrornas ( cross - timepoint comparison ) revealed modulation during treatment course ( data supplement )  . to assess the downstream effects of a potentially aberrant th1 cell response , we examined antigen - bound serum autoantibodies . 
it was noteworthy that the patient experienced hypothyroidism after receiving ici as we identied antithyroglobulin autoantibody across all sample collection points ( roche electrochemiluminescent assay ) ( data supplement )  . 
a mass spectrometry - based assay14 - 16 to identify serum autoantibodies complexed with their cognate antigens detected thirteen autoantibodies related to cardiac and coagulative pathway ( fig 3d ; data supplement )  . 
by contrast , the recurrent presentation , although displaying low ejection fraction and elevated bnp ( c and d ) , did not display markedly elevated troponin levels ( b )  . 
follow - up ecg after initial presentation shows persistence of st elevation and development of low - voltage ecg ( b )  . ecg one month after initial presentation shows low - voltage ecg and development of right bundle branch block ( rbbb , c )  . 
myocardial biopsy ( e ) demonstrated mixed inammation ( yellow arrow ) with some associated myocyte damage ( orange arrow ) and some healing injury ( green star ) near relatively uninvolved myocardium ( cyan star ) ; higher - power image is also shown ( f ) ; hematoxylin and eosin staining ; digital acquisition ; scale bars as shown = 100 m . immunohistochemistry demonstrated that most of this inltrate was composed of cd3positive t cells ( g , stained cells in brown ) and cd68 - positive macrophages ( h , stained cells in brown )  . 
avr , augmented vector right ; avl , augmented vector left ; avf , augmented vector foot . cmr showing the presence of severe biventricular dysfunction , mild pericardial effusion , and a short axis late gadolinium enhancement ( lge ) stack showing lge in a subepicardial distribution involving the basal and apical segments ( admission )  . although iraes often develop within the rst few weeks to months after initiation of treatment , these events can present at any time , including after cessation of ici therapy . 
luminex - based analysis of circulating inammatory cytokines revealed consistently elevated responses enriched in th1 cell cytokines ( a ) in contrast to th2 cell cytokines ( b )  . two mirs related to cardiac function and inammation displayed consistent trends in expression with mir - 130 - 3p trending upward and mir - 122 - 5p trending downward ( c )  . 
serum autoantibody complexes were observed consistently in the programmed cell death protein - 1 ligand 1induced fulminant myocarditis patient compared to ageand sex - matched control patients ( n = 7 ) , and a patient with myocarditis from systemic lupus erythematosus ( n = 1 ; d )  . serum autoantibody complex data are displayed as relative expression ( average protein intensity ) with data presented as the mean 6 the standard deviation . 
 case report surveillance after an episode of myocarditis , and the necessity for rapid and effective immunosuppression.4 treatment with high - dose glucocorticoids and mmf appeared to improve symptomology ; however , it may have failed to affect the underlying etiology as bnp levels remained marginally abnormal while high levels of inammatory cytokines and autoantibodies persisted . 
it is possible that in addition to generating autoreactive t cells against cardiac epitopes ( a proposed cause of ici - mediated myocarditis ) , icis may also induce th1 - dependent pathogenic autoantibody production ( data supplement )  . patients presenting with symptoms suggestive of ici - related myocarditis present a signicant diagnostic challenge . cardiac troponins can be negative in cases of myocarditis.20 indeed , in this case , troponins were only intermittently and mildly elevated during myocarditis recurrence . 
the diagnostic value of echocardiography and ecg is often limited , with ndings suggestive of myocarditis either absent initially or lacking specicity.4 , 6 the addition of cmr may be to detect benecial owing to its potential inammation , edema , and brosis within myocardial tissue . 
however , lge alone has low sensitivity and accuracy in diagnosing chronic or recurrent myocarditis , and cmr is difcult in hemodynamically unstable patients.21 although the recovery of lv function and resolution of symptoms followed by a separate recurrence of symptoms consistent with acute myocarditis is suggestive of a distinct myocarditis event , one other possibility could include the persistence of subclinical inammation between episodes , leading to smouldering myocarditis and subsequent heart raises awareness that serious iraes can occur after ici discontinuation , and without re - exposure , reinforcing the importance of cardiovascular surveillance after an episode of ici - associated myocarditis along with detailed diagnostic work - ups . 
fish provision of study materials or patients : nazanin aghel , paaladinesh thavendiranathan collection and assembly of data : nazanin aghel , dakota gustafson , ashley di meo , milena music , michael a . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . support preparation of this paper used the resources of the toronto general hospital research institute , university health network , toronto , canada . 
hansen consulting or advisory role : merck , glaxosmithkline , bristol - myers squibb , eisai research funding : karyopharm therapeutics , merck , bristol - myers squibb , boehringer ingelheim , glaxosmithkline , roche / genentech , janssen , astrazeneca / medimmune , astellas pharma , macrogenics paaladinesh thavendiranathan honoraria : amgen no other potential conicts of interest were reported . acknowledgment the authors would like to thank the peter munk cardiac centre cardiovascular biobank for the assistance provided with the clinical sample storage , maintenance , and retrieval . references antonia sj , villegas a , daniel d , et al : durvalumab after chemoradiotherapy in stage iii non - small - cell lung cancer . 
n engl j med 377 : 1919 - 1929 , 2017 larkin j , chiarion - sileni v , gonzalez r , et al : combined nivolumab and ipilimumab or monotherapy in untreated melanoma . 
n engl j med 373 : 23 - 34 , 2015 puzanov i , diab a , abdallah k , et al : managing toxicities associated with immune checkpoint inhibitors : consensus recommendations from the society for immunotherapy of cancer ( sitc ) toxicity management working group . 
j am coll cardiol 71 : 1755 - 1764 , 2018 l aubli h , balmelli c , bossard m , et al : acute heart failure due to autoimmune myocarditis under pembrolizumab treatment for metastatic melanoma . j immunother cancer 3 : 11 , 2015 8 . 
mir h , alhussein m , alrashidi s , et al : cardiac complications associated with checkpoint inhibition : a systematic review of the literature in an important emerging area . 
hsu sh , wang b , kota j , et al : essential metabolic , anti - inammatory , and anti - tumorigenic functions of mir - 122 in liver . 
ohyama k , yoshimi h , aibara n , et al : immune complexome analysis reveals the specic and frequent presence of immune complex antigens in lung cancer patients : a pilot study . 
in this article , we cover topics related to the analysis of prognostic factors , centering on factors that are both relevant at the time of diagnosis or initial treatment and during treatment . 
we then review the state - of - the art methods for dynamic prediction and compare the strengths and limitations of these methods . although static models will continue to play an important role in oncology , developing and validating dynamic models of clinical outcomes need to take a higher priority . 
2019 by american society of clinical oncology introduction the identication of prognostic factors and building of risk assessment prognostic models will continue to play a major role in 21st century medicine in patient management and decision making.1 prognostic factors in oncology associate host and tumor variables treatment.2 with clinical outcomes independent of gospodarowicz et al3 classied factors as either tumor related , host , or environmental . 
tumor - related factors are variables related to the tumor and reveal the tumor biology and pathology , such as size of tumor , lymph node involvement , presence of metastasis , and molecular markers ( overexpression of pten gene , presence of androgen receptor variant ar - v7 )  . 
finally , environmental factors are external to the patient , such as access to health care.3 prognostic models are increasingly used in the design , conduct , and analysis of clinical trials . for example , trials of prostate cancer , randomization was stratied by the predicted survival probability determined by the prognostic model of overall survival.4 - 7 in the tailorx trial , oncotype dx , a 21 - gene score that predicts the likelihood of in several recurrence , is used to classify women with breast cancer by their risk group of recurrence.8 prognostic factors also have been used for enriching the patient population in trials with targeted therapies . 
for example , in the toga trial , patients with human epireceptor 2positive gastric dermal growth factor cancer were randomly assigned to either trastuzumab plus chemotherapy or chemotherapy alone.9 in this article , we cover topics that are related to the analysis of prognostic factors , centering on factors that are relevant both at the time of diagnosis or initial treatment and during treatment or follow - up . 
we make a distinction between static and dynamic predictive models and provide a review of the state - of - the - art methods for dynamic predictive models to promote them for future use . knowledge generated to date , most risk assessment models in oncology have been based on static prognostic models . 
in patients with advanced cancer , the disease has substantially evolved race , age , performance status , body mass index , host factors tumor factors psa , ldh , alkaline phosphatase , p53 , etc clinical outcomes overall survival progression - free survival objective response rate prediction window all available information up to t timeline study baseline landmark time horizon time fig 1 . 
 developing and validating risk assessment models and has a heterogeneous presentation within the patient.10 the interand intrapatient variability should be taken into account in statistical modeling.11 , 12 dynamic prediction incorporates time - dependent covariates so that risk prediction would be continually updated with new observations to reect the patients prognosis . we dene terminology that is typically used in dynamic risk prediction . 
standard variable selection approaches , such as forward selection , backward selection , and so forth , with logistic regression for binary end points , 13 and proportional hazards regression for timeto - event end points , 14 have been applied . 
criticism for the stepwise variable selection has been well documented.15 , 16 of note , classication trees , such as recursive partitioning for both binary and time - to - event end points , 17 - 20 frequently have been used.2 , 21 - 26 we concentrate on penalized methods that t and shrink p predictors and in doing so , reduce the variance of the coefcient estimates.27 thus , these methods would improve the accuracy of the model.28 the least absolute shrinkage and selection operator ( lasso ) and adaptive lasso ( alasso ) have been widely used to develop prognostic models of clinical outcomes.29 , 30 we will briey describe ridge regression and penalized methods . 
ridge regression minimizes the residual sum of squares function , but a caveat is that it does not reduce all the coefcients exactly to 0.28 let yi be the response , xij the jth covariate value ( j = 1 , 2 , , p ) corresponding to the ith individual , j the regression coefcient jth covariate , and a tuning parameter . 
similar to ridge regression , the rst term in lasso is the residual sum of squares , and lasso minimizes this function subject to the l1 penalty ( eq 1 ) : ( cid : 1 ) i ( cid : 1 ) 1 yi ( cid : 1 ) j ( cid : 1 ) 1 j xij ( cid : 2 ) + ( cid : 1 ) ( cid : 2 ) j ( cid : 2 ) ( cid : 2 )  . j ( cid : 1 ) 1 a large tuning parameter causes the coefcient estimates to be equal to 0 , thus the lasso will have the sparsity property.28 lasso is an improvement over ridge regression , although it has the main limitation of tending to select too many unimportant variables , and it performs poorly in situations when p  . 
the alasso enjoys the oracle property.30 , 34 elastic net regression uses a combination of l1 penalty and ridge l2 penalty and is a compromise between lasso and ridge regression . 
n is that it retains more than n variables in the model.35 hastie et al28 provided a thorough comparison of these shrinkage techniques . we applied lasso and alasso from calgb 90401 , a phase iii clinical trial in advanced prostate cancer , with the overall goal of building a model of overall survival.5 we had 22 variables that were common between calgb 90401 and the enthuse trial ( external data set ) .36 because of missing data in the covariates , we used methods to impute them as described by white and royston.37 the regressions estimates from the cox proportional hazards model , lasso , and alasso , are listed in table 1 . 
we considered lasso and alasso and applied both the akaike information criterion and the bayesian information criterion to choose the optimal model of overall survival . lasso and alasso selected eight and nine variables , respectively ( table 1 )  . 
figure 2 shows the solution lactate depath for alasso , and we observe that hydrogenase ( ldh ) greater than the upper limit of normal and eastern cooperative oncology group ( ecog ) performance status were selected early in the l1 path compared with the other variables . 
this is followed by visceral disease , alkaline phosphatase , albumin , hemoglobin , pain , bone metastases , and then psa ( the bayesian information criterion stopped at psa )  . 
the nal model selected the following prognostic factors : ldh greater than the upper limit of normal , ecog performance status , metastatic site ( presence of visceral disease , presence of bone metastases ) , psa , alkaline phosphatase , albumin , hemoglobin , and analgesic opioid use . we have focused on variable selection when the number of predictors is small relative to the sample size . 
in recent years , a few statistical studies extended the penalized method for the joint modeling of longitudinal data and survival outcomes.42 , 43 the general idea is to postulate the joint likelihood linking the two submodels through latent random variables and to add shrinkage operators to select xed and random effects . 
while these methods have not been implemented in oncology , the 4 2019 by american society of clinical oncology heterogeneity of treatment effect ( hte ) is another important area to consider when building prognostic models . hte is the nonrandom , explainable variability in the direction and magnitude of treatment effects for individuals within a population.44 there are different sources for hte , and hte may arise from an underlying causal mechanism , artifacts , measurements , or methods.45 , 46 one main goal of hte analyses is to predict whether a patient might benet from a treatment . 
when we turned to our prognostic model of overall survival in prostate cancer , we computed a risk score from the estimated regression coefcients and the predicted survival at 24 months using the baseline cumulative hazard . 
we observe that patient 2 had a worse predicted survival probability at 24 months than patient 1 . another important task in static predictive modeling is to construct prognostic risk groups , which can be formed on the basis of their quantiles from the estimated linear predictor . 
t , we can update the risk prediction by calculating i * ( ut ( cid : 5 ) )  . there are two general dynamic risk prediction frameworks : joint modeling and landmark analysis . 
joint modeling comprises two linked submodels , one for the longitudinal process and one for the time - to - event data , and both depend on a common set of latent random variables.54 , 55 in particular , the longitudinal data usually are modeled by a linear mixed - effects model . 
the cox regression coefcient quanties the association between the latent longitudinal process and the hazard rate at time t . the longitudinal process and the event time process are assumed to be independent given the latent random effects , and the joint likelihood can be derived . 
the model can be estimated either using a frequentist approach that attains maximum likelihood through an expectationmaximization algorithm54 , 56 - 58 or a bayesian approach that uses markov chain monte carlo to obtain posterior means.59 - 61 while assuming that the parameters are readily estimated from the observed data , the conditional probability i * ( ut ) can be computed . 
a monte carlo estimate of i * ( ut ) can be obtained by sampling the random effects and the parameters from the corresponding distributions.62 on the other hand , landmarking63 - 66 consists of a series of related cox regression models , where each one is dened at a distinct landmark time t.63 - 66 for each pair of { u , t } , a separate model is tted to the individuals who remain in the study and have not yet experienced the event of interest . 
joint modeling models the dual distribution of the longitudinal process and the failure times and hence satises the consistency conditions for dynamic prediction.68 moreover , it exploits the full information of collected data and takes into account the measurement error of the longitudinal data . 
joint modeling also takes a considerable amount of effort to estimate the parameters , and the computational cost is high because it involves complicated joint distribution and numerical integration . landmarking circumvents the aforementioned model assumptions and computational burden , but it is not a comprehensive probability model of in contrast , the longitudinal process and failure times and , as such , does not satisfy the consistency conditions . 
another major shortcoming is that landmarking only considers the patients at risk at the landmark time and does not fully explore the information . several articles have focused on the comparison of joint modeling and landmarking . 
ferrer et al71 compared the two approaches in the case of model misspecication , and they aimed for predicting competing risks of prostate cancer from psa history . dynamic risk prediction ( joint modeling ) relies on model assumptions , and hence , its performance suffers from model misspecication . 
we have previously explored whether psa decline at different landmark times is prognostic for overall survival in patients with advanced prostate cancer.79 fontein et al80 developed a dynamic model for predicting overall survival in patients with breast cancer . 
other applications of dynamic models have been implemented to prostate cancer82 - 85 and colorectal cancer.86 we demonstrated the application of dynamic risk prediction using the datatop study , 87 a clinical trial that examined the benets of deprenyl and - tocopherol in slowing the progression of parkinson disease ( pd ) .88 multiple longitudinal biomarkers were collected in the datatop study , including unied pd rating scale total score , modied hoehn and yahr scale , and schwab and england activities of daily living . 
 developing and validating risk assessment models trajectories ( fig 3a ) and risk of functional disability ( fig 3b )  . patient 169 , who had more severe disease with earlier development of functional disability , and patient 718 , who had less severe disease , were selected to illustrate the patient - specic predictions at clinically relevant future time points conditional on their available longitudinal measurements . 
 ( a ) predicted unied parkinson disease rating scale ( updrs ) trajectories and ( b ) predicted conditional failure probabilities for patient 169 ( top rows ) and patient 718 ( bottom rows )  . 
 halabi , li , and luo joint modeling , our major interest was to predict probability of functional disability after visits at time t given the patients longitudinal proles and event - free status up to time t . 
overtting occurs when a high predictive accuracy is estimated from a model that has been applied to the training set but has low accuracy when assessed in an independent data set.90 a good example of overtting is provided in halabi and owzar.2 the validation of a prognostic model is considered a critical step after a risk assessment model has been built . 
there are two types of validation : external and internal.16 , 89 , 90 external validation , where the frozen model from the training data is applied to an independent data set , is the most rigorous approach . 
of note , other types of resampling methods , such as cross - validation , bootstrapping , and bootstrapping using 0.632 + , are considered appropriate approaches to model validation.32 , 53 , 91 , 92 investigators plot assessment of the models performance usually is conducted by examining the calibration and discriminative ability of the model . 
using data from two phase iii clinical trials , we evaluated the overall survival model for calibration at different landmarks.36 , 93 figure 4a shows that the predicted survival probabilities at 18 months in the enthuse 33 trial were close to the proportion of patients who survived 18 months . 
the rst two points ( circles ) show that the model overpredicted the proportion of patients who survived 12 months , whereas the third and fth data points show that the model underpredicted the proportion of patients who survived 12 months . discrimination describes the ability of a prognostic model to distinguish between patients with and without the outcome of interest.16 several metrics are used to report the performance of a model . 
these models are anticipated to be implemented in both the design and the conduct of future trials . although static models will continue to play an important role in oncology , developing and validating dynamic models of clinical outcomes need to take a higher priority . 
one of the limitations is that modelers may be constrained by the lack of access to the longitudinal biomarker data ; therefore , the next generation of risk assessments are highly recommended to take into consideration the longitudinal biomarker data and outcomes so that predictions are updated . in summary , risk assessment will remain an important research task in precision oncology . 
calibration of the overall survival model for observed and predicted survival probability at ( a ) 18 months and ( b ) 12 months . pertinent to patient outcomes , dene the primary end point a priori , justify the sample size , and describe the appropriate methods for variable selection and model assessment . 
lastly , they should be validated using external data sets if available . an understanding of the longitudinal relationship between host and tumor - related factors and their impact on clinical outcomes is critical . 
we expect to see an upsurge in dynamic risk assessments in oncology , and as such , the american joint committee on cancer and the transparent reporting of a multivariable prediction model for individual prognosis or diagnosis guidelines should be extended to dynamic predictive modeling . 
regardless of whether static or dynamic modeling is the primary objective , we envision that this review will bridge gaps in knowledge and motivate investigators to take risk assessment as a discipline by itself . 
 halabi , li , and luo references osullivan b , brierley j , gospodarowicz m : prognosis and classication of cancer , in osullivan b , brierley jd , dcruz ak , et al : uicc manual of clinical oncology ( ed 9 )  . 
halabi s , lin cy , kelly wk , et al : updated prognostic model for predicting overall survival in rst - line chemotherapy for patients with metastatic castrationresistant prostate cancer . 
j clin oncol 32 : 671 - 677 , 2014 kelly wk , halabi s , carducci m , et al : randomized , double - blind , placebo - controlled phase iii trial comparing docetaxel and prednisone with or without bevacizumab in men with metastatic castration - resistant prostate cancer : calgb 90401 . 
morris mj , heller g , bryce ah , et al : alliance a031201 : a phase iii trial of enzalutamide ( enz ) versus enzalutamide , abiraterone , and prednisone ( enz / aap ) for metastatic castration resistant prostate cancer ( mcrpc )  . 
j clin oncol 37 , 2019 ( suppl ; abstr 5008 ) sparano ja , gray rj , makower df , et al : adjuvant chemotherapy guided by a 21 - gene expression assay in breast cancer . 
n engl j med 379 : 111 - 121 , 2018 bang yj , van cutsem e , feyereislova a , et al : trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of her2 - positive advanced gastric or gastro - oesophageal junction cancer ( toga ) : a phase 3 , open - label , randomised controlled trial . 
miller kd , oneill a , gradishar w , et al : double - blind phase iii trial of adjuvant chemotherapy with and without bevacizumab in patients with lymph nodepositive and high - risk lymph node - negative breast cancer ( e5103 )  . 
rudloff u , jacks lm , goldberg ji , et al : nomogram for predicting the risk of local recurrence after breast - conserving surgery for ductal carcinoma in situ . 
fizazi k , higano cs , nelson jb , et al : phase iii , randomized , placebo - controlled study of docetaxel in combination with zibotentan in patients with metastatic castration - resistant prostate cancer . 
halabi sp , pi l : statistical considerations for developing and validating prognostic models of clinical outcomes , in kelly do , kevin w , halabi s ( eds ) : oncology clinical trials : successful design , conduct , and analysis ( ed 2 )  . 
gabler nb , duan n , liao d , et al : dealing with heterogeneity of treatment effects : is the literature up to the challenge ? trials 10 : 43 , 2009 46 . 
dane a , spencer a , rosenkranz g , et al : subgroup analysis and interpretation for phase 3 conrmatory trials : white paper of the efspi / psi working group on 51 . 
kattan mw , hess kr , amin mb , et al : american joint committee on cancer acceptance criteria for inclusion of risk models for individualized prognosis in the practice of precision medicine . 
rizopoulos d , hateld la , carlin bp , et al : combining dynamic predictions from joint models for longitudinal and time - to - event data using bayesian model averaging . 
yao f , m uller hg , clifford aj , et al : shrinkage estimation for functional principal component scores with application to the population kinetics of plasma folate . biometrics 59 : 676 - 685 , 2003 74 . 
yan f , lin x , li r , et al : functional principal components analysis on moving time windows of longitudinal data : dynamic prediction of times to event . 
halabi s , conaway mr , small ej , et al : serum prostate specic antigen as a predictor of survival in prostate cancer patients treated with second - line hormonal 80 . 
proust - lima c , taylor jm : development and validation of a dynamic prognostic tool for prostate cancer recurrence using repeated measures of posttreatment psa : a joint modeling approach . 
s `ene m , taylor jm , dignam jj , et al : individualized dynamic prediction of prostate cancer recurrence with and without the initiation of a second treatment : development and validation . 
kr ol a , ferrer l , pignon jp , et al : joint model for left - censored longitudinal data , recurrent events and terminal event : predictive abilities of tumor burden for cancer evolution with application to the ffcd 2000 - 05 trial . 
moons kg , altman dg , reitsma jb , et al : transparent reporting of a multivariable prediction model for individual prognosis or diagnosis ( tripod ) : explanation checklist . 
petrylak dp , vogelzang nj , budnik n , et al : docetaxel and prednisone with or without lenalidomide in chemotherapy - naive patients with metastatic castrationresistant prostate cancer ( mainsail ) : a randomised , double - blind , placebo - controlled phase 3 trial . 
halabi s , pi l , lin c - y : developing and validating prognostic models of clinical outcomes , in halabi s , michiels s ( eds ) : textbook of clinical oncology : a statistical perspective . 
 c acquired ctnnb1 mutation drives immune checkpoint inhibitoracquired resistance in a microsatellite instabilityhigh gastroesophageal adenocarcinoma with brain metastases introduction the landscape of advanced gastric and esophageal adenocarcinomas continues to evolve , partly owing to improved molecular characterization identifying genomically defined subgroups that may benefit from matched therapies.1 - 3 the keynote - 059 and attraction - 2 trials have demonstrated efficacy for the antiprogrammed death - 1 ( pd - 1 ) antibodies pembrolizumab and nivolumab in gastroesophageal adenocarcinomas ( geas ) after two or more prior lines of therapy.3 , 4 the keynote - 059 study population included seven known patients with microsatellite instabilityhigh ( msi - h ) tumors , among whom the response rate was 57% . 
outside of msi - h tumors , changes in neoantigen landscape , acquired jak1 mutations , mhc - i loss , beta - 2microglobulin mutations affecting antigen presentation , and expression of alternate checkpoints have been shown to mediate acquired resistance to immune checkpoint blockade.9 - 12 with the tumor agnostic approval of pembrolizumab for msi - h tumors in 2017 , a better understanding of acquired resistance is increasingly important . 
 standard - of - care human epidermal growth factor receptor 2 immunohistochemical testing was negative , and he received first - line fluorouracil and oxaliplatin with palliative radiotherapy to a painful bone metastasis with a best response of stable disease . 
at the time of first - line progression , his liver biopsy was screened for microsatellite instability , found to be msi - h , and he was enrolled in a clinical trial of ipilimumab 1 mg / kg and nivolumab 3 mg / kg ( table 1 )  . 
after complete radiographic response of distant disease lasting 18 months , he received palliative radiotherapy ( 0.414 gy ) concurrent with nivolumab every 2 weeks for endoscopically improved , but residual , disease and remained in the trial . 
genomic alterations with preclinical and / or clinical evidence supporting resistance to immune checkpoint inhibitors are shown in bold . abbreviations : gej , gastroesophageal junction ; msi - h , microsatellite instabilityhigh ; mut , mutation ; tmb , tumor mutation burden ; wt , wild type . the resection specimen revealed persistence of an 8.5 - cm segment of poorly differentiated gej adenocarcinoma positive for lymphovascular invasion . all lymph nodes were negative , and evidence of significant treatment effect was seen ( tumor regression grade 2 ) , overall staged as ypt3ypn0 with negative margins . 
the surgical specimen was subjected to hybrid - capture comprehensive genomic profiling using a commercial assay ( foundationone , foundation medicine , cambridge , ma ) , which confirmed msi - h ( table 1 )  . 
during the treatment time encompassing stereotactic brain radiotherapy and nivolumab , washout biopsy samples were taken from a stable subcutaneous scalp metastasis , and an intramuscular rectus femoris lesion reappeared on restaging imaging ( table 1 )  . 
in an effort to explore putative resistance mechanisms after excellent durable response to ipilimumab and nivolumab , the samples were all subjected to the same hybrid - capture comprehensive genomic profiling assay ( table 1 ; fig 1 )  . 
after stereotactic brain radiotherapy , the patient went on to enroll in a third - line trial of paclitaxel in combination with the anti - dkk1 monoclonal antibody dkn - 01 ( clinicaltrials . gov identifier : nct02013154 ) and achieved stable disease lasting 4 months , ultimately , with progression in the brain and extracranial sites concurrently . 
clonal divergence and acquired ctnnb1 in a patient with microsatellite instabilityhigh ( msi - h ) gastroesophageal junction adenocarcinoma with disease progression while receiving ipilimumab in combination with nivolumab after a durable response . 
however , the sampled site of cns progression contained private alterations known or suspected to mediate immuno oncology resistance not seen at other disease sites ( fig 1 )  . 
the ctnnb1 t41a and d32y mutations are known ( t41a ) or predicted ( d32y ) stabilizing mutations that lead to t - cell exclusion and resistance to antiprogrammed death - ligand 1 therapies in preclinical models.17 although less well studied , the d32y mutation should increase stability owing to proximity to the cki and gsk3b phosphorylation sites and is a part of the recognition motif for b - trcp ( e3 ligase for b - catenin )  . 
the additional ctnnb1 n387k is not well characterized functionally , although there is some evidence for it leading to increased b - catenin activity in liver cancer.18 stabilizing or gain - of - function ctnnb1 alterations are recurrent in gea and other tumor types and may be associated with a worse outcome , although clinical immunotherapy - specific outcome data are lacking ( fig 3 ) .2 , 19 , 20 it is also possible that the blood - brain barrier may have reduced the efficacy of checkpoint blockade , allowing for the tissue - specific development of the ctnnb1 alterations we observed . 
however , because our methods are limited to dna - based assessment , we cannot exclude nongenomic mediators of acquired resistance that are known to exist.24 overall , our patient may add early support to the possibility of tissue - contextspecific acquired resistance under selective pressure of immune checkpoint inhibitors , although we cannot draw significant conclusions from a single patient . 
in an analogy to oncogene - driven gea , intertumoral heterogeneity may emerge as an acquired resistance mechanism in msi - driven gea.2 in fact , a recent correlative article from a phase ii trial of pembrolizumab in advanced gea identified intratumoral msi heterogeneity in a patient refractory to therapy.6 if further validated , our observation may have implications beyond gea and inform rational , and perhaps individualized , salvage strategies for msi - h tumors progressing while the patient is taking checkpoint inhibitor therapy . 
klempner stock and other ownership interests : tp therapeutics speakers ' bureau : foundation medicine research funding : leap therapeutics ( inst ) , astellas pharma ( inst ) travel , accommodations , expenses : eli lilly alexa b . 
ali employment : foundation medicine leadership : incysus stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health on microbiome stuff in non - neoplastic disease ( i ) charlotte d . 
kubicky consulting or advisory role : bristol - myers squibb , eisai , array biopharma , loxo , bayer , arqule , blueprint medicines , novartis speakers ' bureau : bristol - myers squibb , eisai consulting or advisory role : eli lilly , boston biomedical , astellas pharma matthew h . 
fuchs cs , doi t , jang rw , et al : safety and efficacy of pembrolizumab monotherapy in patients with previously treated advanced gastric and gastroesophageal junction cancer : phase 2 clinical keynote - 059 trial . 
kang yk , boku n , satoh t , et al : nivolumab in patients with advanced gastric or gastrooesophageal junction cancer refractory to , or intolerant of , at least two previous chemotherapy regimens ( ono - 4538 - 12 , attraction - 2 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
janjigian yy , bendell j , calvo e , et al : checkmate - 032 study : efficacy and safety of nivolumab and nivolumab plus ipilimumab in patients with metastatic esophagogastric cancer . 
overman mj , lonardi s , wong kym , et al : durable clinical benefit with nivolumab plus instability - high metastatic in dna mismatch repair - deficient / microsatellite ipilimumab colorectal cancer . 
shitara k , zgrolu m , bang yj , et al : pembrolizumab versus paclitaxel for previously treated , advanced gastric or gastro - oesophageal junction cancer ( keynote - 061 ) : a randomised , openlabel , controlled , phase 3 trial . 
smyth ec , wotherspoon a , peckitt c , et al : mismatch repair deficiency , microsatellite instability , and survival : an exploratory analysis of the medical research council adjuvant gastric infusional chemotherapy ( magic ) trial . 
this study was performed to characterize mutagenesis and mutational target genes underlying lung carcinogenesis in patients with uip . patients and methods a cohort of 691 japanese patients with lung adenocarcinoma ( ladc ) , of whom 54 had uip and 637 did not , was studied for driver oncogene aberrations . 
2018 by american society of clinical oncology introduction smoking is a major risk factor for lung cancer , 1 and its mutagenic process and mutational targets , including kras and tp53 , have been elucidated.2 smoking is also a pathogenic factor for idiopathic pulmonary fibrosis ( ipf ) , which is pathologically diagnosed as usual interstitial pneumonia ( uip ) , 3 characterized by destruction of alveolar architecture in association with fibrosis.4 uip is a strong risk factor for lung cancer independent of smoking ( relative risk , 8.25 ) 5 and increases the cumulative incidence rate of lung cancer within 10 years to 54.7%.6 notably , deleterious germline mutations in pulmonary surfactant system genes ( pssgs ) , including nkx2 - 1 / ttf1 , sftpa1 , sftpa2 , sftpb , and sftpc , have been implicated in familial neonatal respiratory failure and fibrotic lung disease , 7 as well as in lung cancer development.8 , 9 therefore , loss of function of pssgs in morphogenesis / maintenance of alveolar structure7 might also play a role in uip and subsequent development of lung cancer in individuals with germline pssg mutations . 
however , such tumors are rarely subjected to surgical resections ( 3.1% ; 1 , 300 of 41 , 742 ) , 10 largely because of the risk of acute exacerbation of interstitial pneumonia and an associated high mortality rate.10 consequently , no comprehensive genomic analysis of uip - associated lung cancers has been published to date . 
one of the few genetic characteristics of these cancers reported previously is that egfr oncogene mutations are relatively infrequent in uip - associated lung adenocarcinomas ( ladcs ) .11 - 13 in this study , we performed comparative and comprehensive genomic characterization of ladcs with and without uip . 
ladc was chosen for comparison for several reasons : it is the most common histologic type of lung cancer and frequently develops in the lungs of patients suffering from uip11 ; the genetic aberrations responsible for carcinogenesis , represented by driver oncogene aberrations , 14 - 16 have been well documented ; and mutational signature studies17 have revealed the mutational events underlying this disease , which include dna damage / adduct formation as a result of smoking , spontaneous deamination of 5 - methylcytosine , 18 and the action of apolipoprotein b mrna editing enzyme catalytic polypeptide - like cytidine deaminases.19 to deduce the mutagenic processes and elucidate commonly affected genes , we examined driver oncogene aberrations in a cohort of 691 patients with ladc , including 54 patients who were uip positive and 637 patients who were uip negative , and performed whole - exome sequencing ( wes ) analysis in 296 ladcs ( 51 uip positive and 245 uip - negative )  . 
of those , 679 were consecutive patients who underwent surgical resection between 1997 and 2008 at the national cancer center ( ncc ) hospital ( ncch ) , tokyo , and for which snap - frozen cancerous and noncancerous lung tissues suitable for genome analysis were available in the ncc biobank . 
 surgical specimens of these patients were classified as uip negative and uip positive ( 637 and 42 cases , respectively ) on the basis of previously described pathologic criteria.20 uip positivity was defined as the presence of the uip pattern ( on the basis of the 2002 american thoracic society / european respiratory society4 and 2011 ipf criteria3 )  . 
uip - positive cases were defined as those having tumorous lesions located within or adjacent to uip lesions ; tumors discontinuous to the uip lesions were excluded ( appendix )  . 
 to increase the number of uip - positive cases , an additional 12 patients who underwent surgical resection between 2011 and 2014 at ncch or tokyo medical and dental university hospital , tokyo were also studied . 
thus , the total number of uip - positive cases was 54 ( 42 + 12 )  . all patients were diagnosed according to the seventh tnm classification of malignant tumors.21 information regarding age , sex , smoking history , and clinical stage was retrospectively collected . 
 this study was approved by the institutional review boards of both the ncc and tokyo medical and dental university . driver gene aberration screening all 691 cases were screened for egfr , kras , braf , and her2 hotspot mutations by high resolution melting analysis or target sequencing analysis using the ion ampliseq cancer hotspot panel v2 ( life technologies , rockville , md )  . 
 alk , ret , and ros1 fusions were examined by reverse transcriptase polymerase chain reaction ( rt - pcr ) or molecular counting assay as previously described.15 , 22 , 23 wes analysis wes was performed for 245 uip - negative and 51 uip - positive ladcs ( 296 cases in total )  . 
 of these , 211 of the uip - negative cases and all 51 uip - positive cases were selected from the 691 patients with ladc used for driver gene aberration screening on the basis that sufficient amounts of dna were available for comprehensive genomic profiling . 
 wes was performed for cancerous and noncancerous genomic dnas using the sureselect human all exon exome capture kit ( version 4 or 5 ; agilent technologies japan , tokyo , japan ) on the illumina hisequation 2000 platform ( illumina , san diego , ca )  . 
in this condition , 10 randomly chosen snvs and 47 indels were verified at high confidence by mass - spectrometric genotyping on a massarray system ( agena bioscience , san diego , ca ) : 10 of 10 ( 100% ) for snvs and 45 of 47 ( 95.7% ) for indels , respectively ( appendix )  . 
genes recurrently affected by somatic snv and indel mutations in their coding regions were identified by mutsigcv analysis25 according to the following criterion : q value < 0.1 after adjusting for gene length and applying the benjamini - hochberg correction . 
 more detailed information about immunohistochemistry procedures is provided in the appendix . statistical analysis statistical analyses of differences were analyzed by student t test , mann - whitney u test , pearsons 2 test , or fishers exact test . 
for association studies , clinicopathological factors and mutational signatures were coded as binary or ordinal explanatory variables , and association between these signatures and clinical background was analyzed by fishers exact test and logistic regression analysis using the jmp 8.0 software ( sas institute japan , tokyo , japan )  . 
survival analysis was performed using the kaplan - meier method , and groups were compared by log - rank test using the graphpad prism 7 software ( graphpad , la jolla , ca )  . 
this result is consistent with previous reports of patients with uip3 and patients with ladc with uip.11 - 13 baseline characteristics of patients with uip - negative and - positive ladc were similar to those of previously described asian cohorts.16 , 27 , 28 driver oncogene aberrations in uip - negative cases , approximately 50% of which were egfr mutations , were similar to those of overall ladcs in east asians.16 , 28 on the other hand , the prevalence of oncogene aberrations clearly differed between uip - positive and uip - negative cases ( p < .001 by pearsons 2 ; fig 1a ; table 1 )  . 
however , the rate of egfr mutation was markedly lower in uip - positive cases than in uip - negative cases ( 1.9% [ one of 54 ] v 49.9% [ 318 of 637 ] ; p < .001 [ fishers exact test ] ) , even in heavy smokers , who have a low egfr mutation frequency30 ( 25.3% ; 38 of 150 ; p < .001 [ fishers exact test ] )  . 
 ( % ) unless otherwise noted . abbreviations : ladc , lung adenocarcinoma ; uip , usual interstitial pneumonia . * p value was derived from the comparison between the non - uip cohort and uip - ladc by mann - whitney u test , fishers exact test , or pearsons 2 test , as appropriate . invasive mucinous adenocarcinoma and colloid , fetal , and enteric carcinoma were categorized as variants of invasive adenocarcinoma , as in travis et al.29 mutational events underlying carcinogenesis deduced by mutational signatures next , we performed a genome - wide mutational analysis to deduce the mechanisms of mutagenesis during lung carcinogenesis . 
patient characteristics and driver oncogene aberrations of the uip negative cases were similar to those of the 637 uip - negative cases described above ( appendix table a1 )  . 
the median snv rates in uip positive and - negative cases were 1.43 / mb and 0.97 / mb , respectively ( p = .0044 [ mann whitney u test ] ) , whereas the median indel mutation rates in uip - positive and - negative cases were 0.25 / mb and 0.080 / mb , respectively ( p < .001 [ mann - whitney u test ] )  . 
therefore , more mutational events , including indel mutations , occurred in the genomes of uip - positive cancers . among the 296 patients , we observed cosmic signatures 4 ( smoking associated ) , 2 ( apolipoprotein b mrna editing enzyme , catalytic polypeptide - like associated ) , 1 ( age associated ) , and 16 ( unknown etiology ; appendix fig a1 )  . 
uip - negative cases were subcategorized based on smoking status : never smoker , ever smoker , and heavy smoker ( 40 pack - years [ py ] )  . 
these findings indicated that mutational events involved in the development of uip positive ladc are largely caused by smoking . significantly mutated genes in uippositive ladc mutsigcv analysis of all 296 cases revealed frequent mutations in several genes reported in previous genome - wide mutation analysis of ladc14 : egfr , kras , tp53 , stk11 , cdkn2a , ctnnb1 , and smad4 ( appendix table a3 )  . 
mutsigcv analysis of the 51 uip - positive cases revealed that tp53 ( 20 of 51 ; 39.2% ) and kras ( 10 of 51 ; 19.6% ) were the two most frequently mutated genes ( fig 1b ; appendix table a3 )  . 
mutations in other genes reported as mutated in ladc14 were also detected in patients with uip - positive ladc , albeit at lower frequencies than tp53 , kras , and nkx2 - 1 . deleterious pssg mutations in a subset of ladc the above observation prompted us to investigate whether other pssgs are mutated in ladcs . 
we found that four other pssgs , sftpa1 , sftpa2 , sftpb , and sftpc , were mutually exclusively mutated in 10 of 296 ( 3.3% ) of all ladc cases and three of 51 ( 5.9% ) of uip - positive cases ( fig 2a )  . 
most of the mutations in these pssgs were indels in the 3untranslated regions ( utrs ; fig 2b ) , consistent with a recent report that indel mutations occur preferentially in lineage - defining genes in human cancers.32 comparative genotyping of dna and cdna isolated from cancerous and noncancerous tissues revealed that the 3 - utr indel mutant alleles of sftpa1 , sftpa2 , and sftpc were expressed at significantly lower levels than the wild - type alleles ( appendix fig a2 )  . in total , 21 of 296 ladcs ( 7.1% ) had mutations in five pssgs ( nkx2 - 1 , sftpa1 , sftpa2 , sftpb , and sftpc ) , with the mutations in individual genes occurring almost mutually exclusively . 
the prevalence of indels in all cases ( 15 of 296 ; 5.1% ) and uip - positive ladc cases ( six of 51 ; 11.8% ) indicated that pssgs are a major target for indel mutagenesis ( fig 2a )  . pssg mutations define a clinically distinct subset of ladcs next , we examined the characteristics of 21 patients with ladc with pssg mutations ( table 2 )  . 
notably , 11 cases ( 52.3% ) exhibited histology corresponding to mucinous differentiation , 29 with a frequency much higher than in ladcs overall ( 6.1% to 16%29 , 33 , 34 ; appendix table a4 ; representative cases in fig 3a )  . 
most tumors with mutations in nkx2 - 1 and all tumors with mutations in sftpa1 and sftpa2 lost expression of the corresponding proteins , whereas tumors with sftpb mutations retained surfactant protein ( sp ) - b protein expression . 
patients who were uip positive with pssg mutations had shorter median overall survival : 24 months versus 125 months for patients who were uip positive without such mutations ( p = .0080 ; fig 3b )  . 
however , no such association was observed for patients with uip - negative ladc ( appendix fig 3a and 3b )  . discussion we present here the first comprehensive comparative genome profiles , to our knowledge , of ladcs with and without uip . 
 ( % ) unless otherwise noted . abbreviations : ladc , lung adenocarcinoma ; pssg , pulmonary surfactant system gene ; uip , usual interstitial pneumonia . * p value was derived from the comparison between cases with or without pssg mutation by mann - whitney u test , fishers exact test , or pearsons 2 test , as appropriate . invasive mucinous adenocarcinoma and colloid , fetal , and enteric carcinoma were categorized as variants of invasive adenocarcinoma , as in travis et al.29 profiles distinct from those of uip - negative ladcs , characterized by infrequent egfr mutations . 
furthermore , focal genome copy number gain associated with abundant transcript expression is a mode of activation of the egfr oncogene.37 uip - positive ladcs did not exhibit significant copy - number gains at egfr , whereas several uip - positive ladcs did ( appendix fig a4a - a4c )  . 
rna sequencing of representative uip - positive cases did not reveal overexpression of egfr ( appendix fig a4d - a4f ) or oncogenic egfr fusions , which have been reported as driver events in ladc.38 these results suggested that the egfr oncogene infrequently contributes to the development of uip - positive ladc . 
ladcs in east asian individuals frequently harbor egfr mutations , both in smokers and nonsmokers.39 therefore , our findings show that uip affects the molecular mechanism underlying lung carcinogenesis by changing the relative dependence of oncogene aberrations . mutational signature analysis revealed that the mutational events involved in uip - positive ladc are largely due to smoking . 
indel mutations were also frequent in uip - positive ladcs , consistent with their prevalence in smoking associated cancers.31 importantly , our results newly identify pssgs as major targets for indel mutations . 
pssg deficiency had been implicated in lung carcinogenesis on the basis of the association between deleterious germline mutations in these genes and severe familial lung diseases , such as interstitial pneumonia and lung cancer development.7 - 9 noncancerous lung tissues of patients with germline sftpb mutation and sftpc - deficient mice develop interstitial fibrosis and alveolar type ii cell dysplasia , 40 , 41 suggesting that pssg deficiency perturbs normal pneumocytic differentiation . 
 ( a ) pathologic features of pssg - mutated lung adenocarcinoma , including invasive mucinous ( case 12 ) and acinar - predominant with a mucinous cribriform pattern ( case 14 )  . 
nk2 homeobox1 ( nkx2 - 1 ) / thyroid transcription factor 1 ( ttf1 ) and surfactant protein ( sp ) - a were detected in normal pneumocytes but were undetectable in tumors with the corresponding sftpa and / or nkx2 - 1 mutations . 
hematoxylin and eosin staining ( he , upper right ) and immunohistochemistry for nkx2 - 1 / ttf1 ( lower left ) and sp - a ( lower right ) proteins , with 3 , 3 - diaminobenzidine visualization ( magnification 200 )  . 
 ( b ) kaplan - meier curve showing overall survival ( os ) of patients with usual interstitial pneumonia ( uip ) positive ladc with pssg mutation ( mutant ) and without pssg mutation ( wild type )  . 
inflammation contributes not only to tumor development but also to tumor progression , by increasing cell invasion and expanding the fraction of undifferentiated cells.43 , 44 however , pulmonary surfactant proteins play important roles in epithelial integrity and cell differentiation in the lung.7 , 45 therefore , deficiency in pulmonary surfactant protein caused by pssg mutations might increase inf lammation - driven tumor progression by disturbing epithelial integrity / differentiation . 
 pssg mutations were more likely to be present in ladcs of smokers and in egfr mutation negative ladcs , which are both associated with poor prognosis.46 , 47 in addition , the number of cases with pssg mutations was small . 
the roles of aberrations of minor driver oncogenes and pssgs should also be studied in a larger cohort , including patients with squamous cell carcinoma , to more fully elucidate lung carcinogenesis associated with uip . 
the 3 - utrs of genes play regulatory roles in the stability and abundance of mrna , and oncogenic mutations have been reported in the 3 - utrs of kras and tp53 genes.48 , 49 accordingly , functional analysis of the 3 - utr mutations in sftps is warranted . in summary , we elucidated the genomic profile of uip - ladcs and observed a predominance of smoking - related mutations in these cancers . 
 kyohei masai no relationship to disclose hirohiko totsuka employment : stagen noriko motoi honoraria : agilent , msd , novartis , astrazeneca , bristolmyers squibb japan consulting or advisory role : bristol - myers squibb , miraca life sciences , astrazeneca , chugai pharmaceuticals , research funding : roche ( inst ) yoko shimada no relationship to disclose ayaka otsuka no relationship to disclose yae kanai no relationship to disclose kenichi okubo no relationship to disclose shun - ichi watanabe no relationship to disclose masashi kobayashi no relationship to disclose takumi akashi no relationship to disclose sachiyo mimaki no relationship to disclose katsuya tsuchihara no relationship to disclose suenori chiku no relationship to disclose kouya shiraishi no relationship to disclose support references 2005 koji tsuta speakers ' bureau : msd , roche naohiko inase no relationship to disclose takashi kohno research funding : daiichi sankyo , sysmex acknowledgment we thank y . 
sakaguchi for excellent technical assistance with immunohistochemistry . affiliations takayuki honda , kouya shiraishi , yoko shimada , ayaka otsuka , and takashi kohno , national cancer center research institute , chuo - ku ; takayuki honda , hiroyuki sakashita , masashi kobayashi , takumi akashi , kenichi okubo , and naohiko inase , tokyo medical and dental university , bunkyo - ku ; kyohei masai , noriko motoi , and shun - ichi watanabe , national cancer center hospital , chuo - ku ; kyohei masai and yae kanai , keio university school of medicine , sinjuku - ku ; hirohiko totsuka , stagen , taito - ku ; suenori chiku , mizuho information and research institute , chiyoda - ku , tokyo ; sachiyo mimaki and katsuya tsuchihara , epoc , national cancer center , kashiwa , chiba ; and koji tsuta , kansai medical university , hirakata , osaka , japan . supported by the japan agency for medical research and development grant no . 
raghu g , collard hr , egan jj , et al : an official ats / ers / jrs / alat statement : idiopathic pulmonary fibrosis : evidence - based guidelines for diagnosis and management . 
fujimoto d , tomii k , otoshi t , et al : preexisting interstitial lung disease is inversely correlated to tumor epidermal growth factor receptor mutation in patients with lung adenocarcinoma . 
masai k , tsuta k , motoi n , et al : clinicopathological , immunohistochemical , and genetic features of primary lung adenocarcinoma occurring in the setting of usual interstitial pneumonia pattern . 
goldstraw p , crowley j , chansky k , et al : the iaslc lung cancer staging project : proposals for the revision of the tnm stage groupings in the forthcoming ( seventh ) edition of the tnm classification of malignant tumours . 
sunami k , furuta k , tsuta k , et al : multiplex diagnosis of oncogenic fusion and met exon skipping by molecular counting using formalin - fixed paraffin embedded lung adenocarcinoma tissues . 
travis wd , brambilla e , noguchi m , et al : international association for the study of lung cancer / american thoracic society / european respiratory society international multidisciplinary classification of lung adenocarcinoma . 
yatabe y , koga t , mitsudomi t , et al : ck20 expression , cdx2 expression , k - ras mutation , and goblet cell morphology in a subset of lung adenocarcinomas . 
tang x , kadara h , behrens c , et al : abnormalities of the titf - 1 lineage - specific oncogene in nsclc : implications in lung cancer pathogenesis and prognosis . 
hirsch fr , varella - garcia m , bunn pa jr , et al : epidermal growth factor receptor in non - smallcell lung carcinomas : correlation between gene copy number and protein expression and impact on prognosis . 
wallot m , wagenvoort c , demello d , et al : congenital alveolar proteinosis caused by a novel mutation of the surfactant protein b gene and misalignment of lung vessels in consanguineous kindred infants . 
oshima h , nakayama m , han t - s , et al : suppressing tgf signaling in regenerating epithelia in an inflammatory microenvironment is sufficient to cause invasive intestinal cancer . 
fujisawa t , iizasa t , saitoh y , et al : smoking before surgery predicts poor long - term survival in patients with stage i non - small - cell lung carcinomas . 
takano t , fukui t , ohe y , et al : egfr mutations predict survival benefit from gefitinib in patients with advanced lung adenocarcinoma : a historical comparison of patients treated before and after gefitinib approval in japan . 
 appendix histologic diagnosis surgically resected specimens ( ie , tissues remaining after snap - frozen tissues were set aside ) were formalin fixed by transbronchial or transpleural injection ( in an inflated state ) , cut serially into 5 - mmthick sections , and macroscopically examined . 
the reads were aligned to the reference human genome ( university of california , santa cruz , human genome 19 ; hg19 ) with the burrows wheeler aligner multi - vision software package . 
because duplicate reads were generated during the polymerase chain reaction ( pcr ) amplification process , duplicated paired - end reads that aligned to the same genomic positions were marked using picard . 
depth of coverage at capture targets in tumor samples was counted using read coverage spanning a target segment with the total number of aligned reads and proportionally calibrated to estimate the copy ratio using depths observed in a panel of normal ( noncancer ) diploid genomes . 
thresholds were as follows : board length cutoff , 0.5 chromosome arms ; confidence interval , 90% . validation of candidate mutations using mass - spectrometric genotyping validation and quantification of candidate mutations were performed by mass - spectrometric ( ms ) genotyping as previously described ( su ky , et al : j clin oncol 30 : 433 - 440 , 2012 ) according to the user instructions for the massarray system ( agena bioscience , san diego , ca )  . 
extracted dna ( 10 ng ) was amplified using specific primers ; unincorporated nucleotides were inactivated by shrimp alkaline phosphatase ; a single - base extension reaction was performed using extension primers that hybridized immediately adjacent to the mutations . 
salts were removed by addition of cation exchange resafter cleanup with spectroclean resin , samples were loaded onto the spectrochip matrix using a nanodispenser and then analyzed by matrix - assisted laser desorption ionizationtime - of - flight mass spectrometry on a bruker autoflex instrument . 
 mutational signature analysis mutational signature in this study was analyzed using nonnegative matrix factorization ( nmf ) , which was applied to the 96 possible substitutions in a trinucleotide context including the bases 5 and 3 of each substitution site , as previously described.17 , 26 nmf was applied to the 96 - substitution pattern using published software from the wellcome trust sanger institute.9 at least 2 , 400 iterations of nmf were run , and each nmf run was iterated to convergence ( 10 , 000 iterations without change ) or until 1 million iterations were performed . 
nmf runs with various numbers of signatures were tested , from one to 10 ; four was best , because signature stability remained high and the reconstruction error converged at a low value ( appendix fig a2a )  . 
 one microgram of total rna was reverse - transcribed using superscript iii first - strand synthesis system for reverse transcriptase ( rt ) pcr ( thermo fisher scientific , waltham , ma ) after dnase treatment . 
ten nanograms of genomic dna and cdna corresponding to 50 ng of rna were prepared from both cancerous and noncancerous tissues . for ms genotyping , the experimental procedures described above were applied to both genomic dna and cdna using the same primer , and mutant allele frequency ( represented as peak heights ) was calculated using the typer4 software ( agena bioscience )  . for fragment analysis , regions including mutations were amplified by pcr from genomic dna and cdna using the same primers according to the manufacturers instructions ( applied biosystems , foster city , ca )  . 
pcrs were performed in triplicate with the following conditions : 35 cycles of denaturation at 95c for 1 minute , annealing at 60c for 1 minute , and extension at 72c for 1 minute . 
mutant allele frequency ( represented as peak heights ) was calculated using the abi genemapper software ( applied biosystems )  . differences in the sftpa1 , sftpa2 , and sftpc gene expression between cancerous and noncancerous tissue were analyzed using quantitative rt - pcr . 
triplicate samples were used for all experiments described in this paragraph . rna sequencing rna - sequencing libraries were prepared from 200 ng of total rna using the truseq rna sample prep kit ( illumina )  . 
the resultant libraries were subjected to paired - end sequencing of 75 - bp reads on a hisequation 2000 ( illumina ) as previously described ( nakaoku t , et al : clin cancer res 20 : 3087 - 3093 , 2014 )  . 
egfr fusion transcripts were identified using the tophat - fusion algorithm ( kim d , et al : genome biol 12 : r72 , 2011 ) .12 expression values were normalized against the corresponding levels of a housekeeping gene ( tbp , encoding tata - binding protein ) .19 immunohistochemistry studies immunohistochemistry studies were performed on 4 - mthick , formalin - fixed , paraffin - embedded tissue sections derived from representative tumor blocks . 
3 , 3 - diaminobenzidine was used as the chromogen , and hematoxylin was used as the counterstareactions that labeled at least 5% of cells were considered positive for thyroid transcription factor 1 ( nuclear )  . 
 ( a ) mass - spectrometric genotyping of genomic dna and cdna from cancerous tissues with sftp - 3 untranslated region ( utr ) indel mutation ( mut ) and noncancerous tissue ( wt )  . 
 ( a ) kaplan - meier curve of overall survival ( os ) for patients with usual interstitial pneumonianegative lung adenocarcinoma with pulmonary surfactant system gene ( pssg ) mutation ( mutant ) and without pssg mutation ( wild type )  . 
 ( a ) copy - number analysis of usual interstitial pneumonia ( uip ) positive lung adenocarcinomas ( ladcs ; n = 51 ) in comparison with uip - negative ladcs ( n = 245 ) ; ( b ) uip - negative ladcs with egfr mutation ( n = 130 ) ; and ( c ) uip - negative ladcs without egfr mutation ( n = 115 )  . 
 ( d ) expression levels of egfr in three uip - positive ladcs in comparison with uip - negative ladcs ( n = 138 ) ; ( e ) uip - negative ladcs with egfr mutation ( n = 35 ) ; and ( f ) uip - negative ladcs without egfr mutation ( n = 103 )  . 
expression levels are shown as fold changes in fragments per kilobase of exon per milllion reads mapped , normalized against the gene encoding tata - binding protein ( tbp )  . 
 o programmed cell death 1 ( pd - 1 ) ligand ( pd - l1 ) expression in solid tumors as a predictive biomarker of benefit from pd - 1 / pd - l1 axis inhibitors : a systematic review and meta - analysis monica khunger adrian v . 
pennell james stevenson sanjay mukhopadhyay kurt schalper vamsidhar velcheti monica khunger , sagar rakshit , sanjay mukhopadhyay , cleveland clinic ; adrian v . hernandez , university of connecticut / hartford hospital , universidad peruana de ciencias aplicades ; vinay pasupuleti , case western reserve university school of medicine ; nathan a . pennell , james stevenson and vamsidhar velcheti , taussig cancer center , cleveland , oh ; and kurt schalper , yale university school of medicine , new haven , ct . corresponding author : vamsidhar velcheti , md , facp , center for immuno - oncology research , cleveland clinic , cleveland , oh 44195 ; e - mail : velchev@ ccf.org. purpose drugs targeting the programmed cell death 1 ( pd - 1 ) / programmed cell death ligand 1 ( pd - l1 ) pathway show significant clinical activity across several tumor types . 
use of biomarker assays to predict response to these agents is an active area of research ; however , the predictive value of pd - l1 immunohistochemistry ( ihc ) assays is largely inconsistent across clinical trials . 
in this meta - analysis of clinical trials of pd - 1 / pd - l1targeted agents , we evaluate the predictive value of a tumor and tumor - infiltrating immune cell pd - l1 ihc assay as a biomarker for objective response to pd - 1 / pd - l1 inhibitors . methods we searched databases ( pubmed , medline , asco abstracts , european society for medical oncology abstracts , and scopus ) up until december 2016 for clinical trials using pd - 1 / pd - l1 inhibitors with reported pd - l1 biomarker data . 
objective response rates ( primary end point ) from all phase i to iii trials investigating nivolumab , pembrolizumab , atezolizumab , durvalumab , and avelumab in advanced solid tumors were collected . 
odds ratios ( ors ) for response in pd - l1positive patients compared with pd - l1negative patients were calculated using the dersimonian - laird random effects model to combine trials . 
we performed metaanalysis as per the preferred reporting items for systematic reviews and meta - analyses guidelines . results forty - one distinct trials with 6 , 664 patients were identified . 
2017 by american society of clinical oncology introduction tumors often evade the immune system by either ineffective antigen presentation or by using mechanisms to thwart an effector response.1 - 3 programmed cell death 1 ( pd - 1 ) is a negative regulator or checkpoint receptor on t cells that is a key determinant of induction of immune tolerance in the tumor microenvironment . 
pd - l1 and pd - l2 expression in the normal tissues is a major mechanism of physiologic peripheral immune tolerance to dampen tissue autoimmune responses after a sustained inflammatory response to tissue damage . 
pdl1 is upregulated in various tumor types including melanoma , nonsmall - cell lung cancer ( nsclc ) , and squamous cell head and neck carcinomas and is a major mechanism of immune evasion . 
in early trials with these agents , pd - l1 expression on tumor cells ( tcs ) , measured by immunohistochemistry ( ihc ) assay , was thought to be an important biomarker for predicting response to these agents.4 however , subsequent trials , particularly atezolizuincorporated both tc and tumormab trials , infiltrating immune cell ( ic ) pd - l1 expression , and this combined pd - l1 expression was also associated with significantly higher objective response rates ( orrs ) in clinical trials . 
pharmaceutical companies have developed different pd - l1 ihc assays , and their comparability and equivalence are the subject of active research.5 , 6 however , most such studies have included relatively small numbers of patients and have not used response or outcome as an end point . 
the databases searched included pubmed , medline , embase , asco abstracts , european society for medical oncology abstracts , google scholar , and scopus . the dates searched were from the inception of each database to december 4 , 2016 . 
the search terms included the following keywords : pd - 1 , pd - l1 , cd274 , programmed cell death receptor 1 , programmed cell death receptor ligand , immune checkpoint inhibitor , nivolumab , bms936558 , pembrolizumab , mk - 3475 , mpdl3280a , atezolizumab , avelumab , msb0010718c , durvalumab , medi - 4736 , predictive biomarker , and cancer immunotherapy . 
the following information was extracted : study design , study population and setting , mean patient age , type of cancer , type of treatment , pd - l1 expression cutoff values , and follow - up time . 
pd - l1 clones used for the evaluation of pd - l1 expression varied across different trials ; 16 studies used 28 - 8 , seven studies used 22c3 , 10 studies used sp142 , three studies used sp263 , and five studies used dako clone 73 - 10 ( dako , carpinteria , ca )  . 
among all of the included studies , 10 were randomized clinical trials , whereas the rest were single - arm trials . data synthesis and analysis study quality analysis some degree of heterogeneity was expected , and random - effects meta - analyses were performed using dersimonian - laird random effects models.10 to consider the sources of heterogeneity , the following two subgroup meta - analyses were prespecified : type of cancer and type of pd - l1 ihc assay . we used the inverse variance method to calculate pooled odds ratios ( ors ) and their 95% cis . 
i2 values of 30% to 60% represented a moderate level of heterogeneity . we used review manager ( revman 5.3 ; cochrane collaboration , copenhagen , denmark ) for our statistical analyses . results eligible studies our search retrieved 3 , 542 publications . 
the majority of the studies had high risk of bias on performance bias and detection bias . meta - analyses of the association between pd - l1 expression and orr no evidence of publication bias was observed in the funnel plot ( eggers test p = .4 ; appendix fig a2 , online only )  . 
there was low heterogeneity of effects across studies in all categories ( fig 2 )  . we performed a subgroup analysis across all nsclc trials simultaneously assessing cutoff values of 1% , 5% , and 10% for pd - l1positive tcs to identify the optimal ihc cutoff threshold . this analysis included the following four trials : brahmer et al , 14 borghaei et al , 15 rizvi et al , 17 and gettinger et al.20 all of these trials included patients with nsclc ( both squamous and nonsquamous histology ) treated with nivolumab and used the dako 28 - 8 antibody for pd - l1 ihc . 
there was limited heterogeneity of effects across studies in all subgroups ( figs 3a - c )  . an additional subgroup analysis was performed across different pd - l1 ihc assays ( fig 4 )  . 
forest plots representing odds ratios of objective response in programmed cell death ligand 1 ( pd - l1 ) positive patients compared with pd - l1negative patients across different cancer types . 
however , because of the paucity of data and power limitations , we could not compare tc and ic subgroups separately . a major objective of our study was to identify the optimal pd - l1 cutoff value associated with maximum objective response . 
this was achieved by performing a subgroup analysis of four trials simultaneously reporting objective response data for three different cut points ( 1% , 5% , and 10% ) in nsclc.14 , 15 , 17 , 20 we restricted the analysis to these four trials to remove heterogeneity associated with tumor type , treatment agents , and pdl1 antibody used for ihc assay . 
all four trials assessed patients with nsclc ( both squamous and nonsquamous histology ) treated with nivolumab and used the 28 - 8 ( dako ) clone for pd - l1 ihc . 
unfortunately , because of power limitations , we were unable to assess the optimal ihc cutoff points of the us food and drug administrationapproved pd - l1 antibodies 22c3 and sp142 . 
these issues may be significant and require additional study . a standardized biomarker such as tc and ic pdl1 expression can identify patients who will derive maximum benefit from these novel agents , sparing others from potentially harmful immune - related toxicities and elevated costs . 
 a vexing issue is the finding that , in some studies , patients respond to pd - 1 / pd - l1 axis inhibitors despite negative tumor pd - l1 expression . 
this assumes special importance in the current scenario of synergistic treatment combinations to enhance therapeutic response to antipd - 1 therapy . some other limitations to using tumor pd - l1 as a standardized biomarker include different collection times of the pathology specimen and the dynamic nature of the tumor microenvironment . 
pd - l1 staining in most cases is performed on archival formalin - fixed , paraffinembedded tissue , because fresh biopsies just before or close to treatment are often not available . 
it has been suggested that previous lines of therapy might alter tumor pd - l1 expression and may explain some of the confounding results across different trials.11 however , we believe this may not have been a significant confounder in our meta - analysis because , more recently , pd - 1 / pd - l1 inhibitor trials have included fresh biopsy specimens ( within 6 months of starting treatment ) , especially many of the recent trials with pd - 1 / pd - l1 inhibitors in the front - line setting.58 tumor pd - l1 expression  . 
the response rate and progressionfree survival ( primary end point of the study ) were higher in the pembrolizumab group than in the chemotherapy group ( orr , 44.8% in pembrolizumab arm v 27.8% in chemotherapy arm )  . 
this is in stark contrast to the results of the checkmate - 26 trial ( nivolumab v platinum - based chemotherapy in the front - line setting ) , which included treatment - nave patients with advanced nsclc and allowed a more liberal inclusion criterion of  . 
these studies further highlight the importance of incorporating pd - l1 expression into future trials of pd - 1 / pd - l1 moabs , especially in the front - line setting where patients have multiple treatment options . we used objective response as the primary end point of our analysis to ensure inclusion of maximum patients , because mature survival data were not available for many of the recent trials . 
for instance , in the checkmate 17 , checkmate 57 , poplar , and oak trials , objective response did not improve as much as the os in the pd - 1 / pd - l1 arm , suggesting postprogression survival advantage.14 , 15 , 49 , 50 however , this should not significantly affect our aim of establishing the validity of pd - l1 expression as a biomarker because orr is commonly used as a surrogate biomarker for clinical benefit in oncology . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . vinay pasupuleti no relationship to disclose sagar rakshit no relationship to disclose nathan a . 
pennell consulting or advisory role : boehringer ingelheim , astrazeneca , eli lilly , regeneron research funding : genentech ( inst ) , newlink genetics ( inst ) , clovis oncology ( inst ) , astex pharmaceuticals ( inst ) , celgene ( inst ) , astrazeneca ( inst ) , pfizer ( inst ) , merck james stevenson research funding : merck sharp & dohme ( inst ) , bayer ( inst ) , bristol - myers squibb ( inst ) sanjay mukhopadhyay research funding : philips healthcare other relationship : phillips kurt schalper honoraria : takeda research funding : vasculox , tesaro , onkaido therapeutics , genoptix , takeda vamsidhar velcheti honoraria : novartis , foundation medicine , merck , bristolmyers squibb , genentech consulting or advisory role : clovis oncology , genentech , bristol - myers squibb , merck , celgene , foundation medicine , astrazeneca / medimmune , genoptix research funding : genentech ( inst ) , trovagene ( inst ) , eisai ( inst ) , oncoplex diagnostics ( inst ) , alkermes ( inst ) , nantomics ( inst ) , genoptix ( inst ) , altor bioscience ( inst ) , merck ( inst ) , bristol - myers squibb ( inst ) , atreca ( inst ) , heat biologics ( inst ) , leap therapeutics ( inst ) travel , accommodations , expenses : astrazeneca / medimmune , eisai 1 . 
hirsch f , mcelhinny a , stanforth d , et al : pd - l1 immunohistochemistry assays for lung cancer : results from phase 1 of the blueprint pd - l1 assay comparison project . 
gettinger sn , horn l , gandhi l , et al : overall survival and long - term safety of nivolumab ( anti - programmed death 1 antibody , bms - 936558 , ono - 4538 ) in patients with previously treated advanced nonsmall - cell lung cancer . 
borghaei h , paz - ares l , horn l , et al : nivolumab versus docetaxel in advanced nonsquamous nonsmall - cell lung 2018 - 2028 , 2015 in cancer patients . 
antonia s , kim s , spira a , et al : safety and clinical activity of durvalumab ( medi4736 ) , an anti - pd - l1 antibody , in treatment - nave patients with advanced nonsmall - cell lung cancer . 
rizvi na , mazi`eres j , planchard d , et al : activity and safety of nivolumab , an anti - pd - 1 immune checkpoint inhibitor , for patients with advanced , refractory squamous nonsmall - cell lung cancer ( checkmate 063 ) : a phase 2 , single - arm trial . 
verschraegen c , chen f , spigel d , et al : avelumab ( msb0010718c ; anti - pd - l1 ) as a first - line treatment for patients with advanced nsclc from the javelin solid tumor phase 1b trial : safety , clinical activity , and pd - l1 expression . j clin oncol 34 , 2016 ( suppl ; abstr 9036 ) 19 . 
herbst rs , baas p , kim d - w , et al : pembrolizumab versus docetaxel for previously treated , pd - l1 - positive , advanced nonsmall - cell lung cancer ( keynote - 010 ) : a randomised controlled trial . 
weber js , dangelo sp , minor d , et al : nivolumab versus chemotherapy in patients with advanced melanoma who progressed after anti - ctla - 4 treatment ( checkmate 037 ) : a randomised , controlled , open - label , phase 3 trial . lancet oncol 16 : 375 - 384 , 2015 22 . 
larkin j , chiarion - sileni v , gonzalez r , et al : combined nivolumab and ipilimumab or monotherapy in untreated med 372 : 320 - 330 , 2015 melanoma . 
hamid o , sosman ja , lawrence dp , et al : clinical activity , safety , and biomarkers of mpdl3280a , an engineered pd - l1 antibody in patients with locally advanced or metastatic melanoma ( mm )  . 
hodi fs , kluger h , sznol m , et al : long - term survival of ipilimumab - nave patients ( pts ) with advanced melanoma ( mel ) treated with nivolumab ( anti - pd - 1 ; bms - 936558 , ono - 4538 ) in a phase 1 trial . 
ribas a , puzanov i , dummer r , et al : pembrolizumab versus investigator - choice chemotherapy for ipilimumabrefractory melanoma ( keynote - 002 ) : a randomised , controlled , phase 2 trial . 
daud ai , wolchok jd , robert c , et al : programmed death - ligand 1 expression and response to the anti - programmed death 1 antibody pembrolizumab in melanoma . 
topalian sl , hodi fs , brahmer jr , et al : safety , activity , and immune correlates of anti - pd - 1 antibody in cancer . 2521 - 2532 , 2015 n engl j med 366 : 2443 - 2454 , 2012 30 . 
choueiri tk , fishman mn , escudier bj , et al : immunomodulatory activity of nivolumab in previously treated and untreated metastatic renal cell carcinoma ( mrcc ) : biomarker - based results from a randomized clinical trial . 
mcdermott df , sosman ja , sznol m , et al : atezolizumab , an antiprogrammed death - ligand 1 antibody , in metastatic renal cell carcinoma : long - term safety , clinical activity , and immune correlates from a phase ia study . 
plimack e , bellmunt j , gupta s , et al : pembrolizumab ( mk - 3475 ) for advanced urothelial cancer : updated results and biomarker analysis from keynote - 012 . 
apolo ab , infante jr , hamid o , et al : safety , clinical activity , and pd - l1 expression of avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in patients with metastatic urothelial carcinoma from the javelin solid tumor phase ib trial . 
massard c , gordon ms , sharma s , et al : safety and efficacy of durvalumab ( medi4736 ) , an anti - programmed cell death ligand - 1 immune checkpoint inhibitor , in patients with advanced urothelial bladder cancer . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
balar av , galsky md , rosenberg je , et al : atezolizumab as first - line treatment in cisplatin - ineligible patients with locally advanced and metastatic urothelial carcinoma : a single - arm , multicentre , phase 2 trial . 
sharma p , callahan mk , bono p , et al : nivolumab monotherapy in recurrent metastatic urothelial carcinoma ( checkmate 032 ) : a multicentre , open - label , two - stage , multi - arm , phase 1 / 2 trial . 
segal n , ou s , balmanoukian a , et al : safety and efficacy of medi4736 , an anti - pd - l1 antibody , in patients from a squamous cell carcinoma of the head and neck ( scchn ) expansion cohort . 
le dt , bendell jc , calvo e , et al : safety and activity of nivolumab monotherapy in advanced and metastatic ( a / m ) gastric or gastroesophageal junction cancer ( gc / gec ) : results from the checkmate - 032 study j clin oncol 34 , 2016 ( suppl 4s ; abstr 6 ) 43 . 
nishina t , shitara k , iwasa s , et al : safety , pd - l1 expression , and clinical activity of avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in japanese patients with advanced gastric or gastroesophageal junction cancer . 
chung hc , arkenau h - t , wyrwicz l , et al : safety , pd - l1 expression , and clinical activity of avelumab ( msb0010718c ) , an anti - pd - l1 antibody , in patients with advanced gastric or gastroesophageal junction cancer . 
kaufman hl , russell j , hamid o , et al : avelumab in patients with chemotherapy - refractory metastatic merkel cell carcinoma : a multicentre , single - group , open - label , phase 2 trial . 
nghiem pt , bhatia s , lipson ej , et al : pd - 1 blockade with pembrolizumab in advanced merkel - cell carcinoma . n engl j med 374 : 2542 - 2552 , 2016 47 . 
antonia sj , l opez - martin ja , bendell j , et al : nivolumab alone and nivolumab plus ipilimumab in recurrent small - cell lung cancer ( checkmate 032 ) : a multicentre , open - label , phase 1 / 2 trial . 
wakelee h , patel jd , heist r , et al : phase ii trial of atezolizumab for patients with pd - l1 - selected advanced nsclc ( birch ) : updated efficacy and exploratory biomarker results : topic : medical oncology . 
rittmeyer a , barlesi f , waterkamp d , et al : atezolizumab versus docetaxel in patients with previously treated nonsmall - cell lung cancer ( oak ) : a phase 3 , open - label , multicentre randomised controlled trial . 
fehrenbacher l , spira a , ballinger m , et al : atezolizumab versus docetaxel for patients with previously treated nonsmall - cell lung cancer ( poplar ) : a multicentre , open - label , phase 2 randomised controlled trial . 
spiegel dr , chaft je , gettinger sn , et al : clinical activity and safety from a phase ii study ( fir ) of mpdl3280a ( anti - pdl1 ) in pd - l1selected patients with non - small cell lung cancer ( nsclc )  . 
carbognin l , pilotto s , milella m , et al : differential activity of nivolumab , pembrolizumab and mpdl3280a according to the tumor expression of programmed death - ligand - 1 ( pd - l1 ) : sensitivity analysis of trials in melanoma , lung and genitourinary cancers . 
aguiar pn jr , santoro il , tadokoro h , et al : the role of pd - l1 expression as a predictive biomarker in advanced nonsmall - cell lung cancer : a network meta - analysis . 
socinski m , creelan b , horn l , et al : nsclc , metastaticcheckmate 026 : a phase 3 trial of nivolumab vs investigators choice ( ic ) of platinum - based doublet chemotherapy ( pt - dc ) as first - line therapy for stage iv / recurrent programmed death ligand 1 ( pd - l1 ) - positive nsclc . 
 efcacy of lorlatinib in primary crizotinib - resistant adult neuroblastoma harboring alk y1278s mutation antoine vasseur , md1 ; luc cabel , md1 ; romain geiss , md1 ; gudrun schleiermacher , md , phd1 ; ga elle pierron , phd1 ; maud kamal , phd1 ; nina jehanno , md1 ; guillaume bataillon , md1 ; jean - marc guinebretiere , md1 ; and laurence bozec , md1 introduction anaplastic lymphoma kinase ( alk ) encodes a highly conserved receptor tyrosine kinase described as an oncogene in anaplastic large - cell lymphoma and other cancers.1 alk fusions ( mostly alk - eml4 ) represent 3% to 7% of all nonsmall - cell lung cancers ( nsclcs ) , and these tumors are generally sensitive to crizotinib ( a tyrosine kinase inhibitor [ tki ] targeting alk ) as rstline therapy in the metastatic setting.2 neuroblastoma harbors activating somatic alk mutations in 8% to 9% of patients ( up to 14% of high - risk neuroblastomas ) , with mutations occurring in the tyrosine kinase domain at three key positions ( f1174 , f1245 , and r1275 ) , which account for approximately 85% of all alk mutations in neuroblastoma.3 activation of alk may also occur by genomic amplication in 3% to 4% of patients , and it has been suggested that patients with neuroblastoma who have genetic alterations of alk could also be treated with crizotinib.4 in this article , we report , to our knowledge for the rst time , the case of an adult patient with ganglioneuroblastoma harboring a somatic alk y1278s mutation with primary resistance to crizotinib , but which was highly sensitive to lorlatinib , a third - generation tki targeting alk genomic alterations . 
computed tomography ( ct ) the chest , abdomen , and pelvis showed scan of disseminated lymph node and vertebral bone lesions . 123i - metaiodobenzylguanidine ( 123i - mibg ) scintigraphy was positive with bone and lymph node metastases . 
laboratory tests showed normal lactate dehydrogenase levels and increased urinary catecholamines ( normetanephrine , 40 , 825 nmol / l ; metanephrine , 572 nmol / l )  . the patient received rst - line induction chemotherapy according to the rapid cisplatin , vincristine , carboplatin , etoposide , and cyclophosphamide ( cojec ) regimen.5 after eight cycles , stable disease was observed in lymph nodes , and progression was observed in bone lesions . 
four months after chemotherapy , clinical disease progression was observed with bone pain , and urinary catecholamines were increased ( normetanephrine , 104 , 651 nmol / l ; metanephrine , 1 , 208 nmol / l ) despite stable mibg scintigraphy and ct scan . a lymphadenectomy ( left subclavicular lymph node ) was performed before second - line therapy with topotecan and cyclophosphamide was started for complementary molecular and immunohistochemistry analyses . immunohistochemistry revealed expression of alk by 100% of tumor cells . 
targeted next - generation in alk , sequencing found a pathogenic variant ptyr1278ser , with an allelic frequency of 23% ( fig 1 )  . the patient was included in the french acs e protocol ( nct02034981 ; phase 2 study assessing efcacy and safety of crizotinib in patients harboring an alteration on alk , met or ros1 ) , and crizotinib was initiated in june 2017 ( 250 mg taken orally twice per day )  . 
treatment was stopped in october 2017 after rapid progression of symptomatic bone metastasis conrmed by mibg scintigraphy , with marked general physical deterioration ( eastern cooperative oncology group [ ecog ] performance status 3 ) , asthenia , anorexia , and weight loss . 
lorlatinib was then obtained from a pzer compassionate - use program and was initiated ( 100 mg taken orally once per day ) in november 2017 , with a signicant clinical benet after 2 weeks of treatment . after 2 months , the patient was asymptomatic with marked improvement of performance status ( from ecog 3 to ecog 0 )  . 
alk positivity by ( a ) immunochemistry and ( b ) next - generation sequencing . partial reossication of bone metastases in favor of treatment response ( left subclavicular lymph node , largest lymph node target lesion ; fig 2 )  . 
after 10 months , 123i - mibg scintigraphy re - evaluation of treatment showed a good partial metabolic response of the left supraclavicular lymph node inltration as seen on the single photon emission computed tomography scan associated with partial response of bone inltration . 
international society of pediatric oncology europe neuroblastoma group ( siopen ) score for bone extension6 , 7 was 30 on baseline scintigraphy , which decreased to a siopen score of 15 on the re - evaluation scintigraphy ( 50% decrease ; relative mibg score of 0.5 ; fig 3 )  . 
overall response according to the international neuroblastoma response criteria consensus was assessed as a partial response.8 after 12 months ( last evaluation in november 2018 ) , the clinical benet was maintained ( ct scan showed a partial reduction of 33% in tumor size [ recist1.1 ] corresponding to the nadir ; left subclavicular lymph node ; fig 2 )  . 
no toxicity was reported during treatment with lorlatinib except for grade 1 hypertriglyceridemia and grade 1 edema of the lower limbs ( common terminology criteria for adverse events [ ctcae ] v5 )  . discussion to our this case report of adult neuroblastoma shows , knowledge for the rst time , that lorlatinib , unlike crizotinib , can be effective in patients harboring an alk y1278s mutation . 
the most common resistance mutations after crizotinib therapy are the l1196m ( 5% to 10% ) and g1269a ( , 5% ) mutations , 9 and many other mutations have also been reported . 
these mutations confer various mechanisms of resistance , such as catalytic domain alteration , which causes atp competitive inhibitor resistance , as t790m mutation in the epidermal growth factor receptor ( egfr ) mutation alters the conformation and / or the atp - binding afnity of the kinase.10 lorlatinib , a third - generation alk inhibitor that also targets ros1 , is an attractive tki in patients with nsclc pretreated with rstor second - generation alk inhibitors because of its activity against most alk resistance mutations , such as g1202r mutations11 ( fig 4b )  . 
lorlatinib has demonstrated high clinical activity in alkor ros1 - rearranged nsclc in treatment - naive or crizotinib pretreated patients.12 in nsclc , the y1278s alk mutation has not been described in the clinical setting , and the efcacy of lorlatinib in nsclc remains unknown . 
however , a different mutation at the same position , y1278h , has been reported in nsclc cell lines that have the alk - eml4 fusion exposed to accelerated mutagenesis , 13 which was resistant to crizotinib . neuroblastoma is the most common solid tumor in children , but adult patients are exceptional , because fewer than 0.3 patients are diagnosed per million people per year.14 crizotinib has been shown to be less effective in neuroblastoma than in nsclc , in which alk mutations , rather than alk fusions , are a major oncogenic event in nearly 10% of the patients , 15 and alk is the most common somatically mutated gene . 
in a phase i / ii trial ( nct00939770 ; crizotinib in treating younger patients with relapsed or refractory solid tumors or anaplastic large cell lymphoma ) , 11 patients with alk - mutated neuroblastoma were treated with crizotinib . 
crystal structure of ( a ) crizotinib / alk and ( b ) lorlatinib / alk . in neuroblastoma reported that y1278s is oncogenic ( ligand - independent activation ) and that crizotinib is inlines effective in vitro and in vivo in neuroblastoma cell harboring the alk y1278s mutation , whereas lorlatinib seemed to be highly effective.19 y1278s is located in the the alk activation loop . 1278 - yrasyy - 1283 motif of donella - deana et al20 demonstrated the important role of initial phosphorylation of tyrosine y1278 for the a - loop activation in alk - npm fusion . 
a study of the crystal structure of alk conrmed this role and highlighted a tight interaction in the inactive form of alk between the unphosphorylated y1278 and a cysteine at position 1097.21 in our patient , a y1278 mutation from tyrosine to serine the phosphorylation and thus the alk should inhibit activation , 20 but guan et al19 showed in a preclinical study that y1278 phosphorylation in neuroblastomas was not for alk activation ( unlike phosphorylation of essential y1283 , which is essential )  . 
however , this hypothesis was not conrmed , so the mechanism of alk activation with y1278s mutation is controversial.19 the y1278s mutation seems to be a rare mutation , but it has been reported in six neuroblastoma patients ( catalogue of somatic mutation in cancer [ cosmic ] database ) .17 , 22 - 24 no clinical data regarding the efcacy of alk inhibitors were reported in these six tumors harboring a y1278s alk mutation , but in two patients , preclinical data showed an in vitro resistance to crizotinib ( high concentration that inhibits 50% [ ic50 ] )  . 
note that a clinical trial of lorlatinib for patients with alk - driven relapsed or refractory neuroblastoma is ongoing as part of the new approaches to neuroblastoma therapy ( nant ) consortium ; this trial ( nct03107988 ; study of lorlatinib [ pf - 06463922 ] , an oral small molecule inhibitor of alk / ros 1 , for patients with alk - driven relapsed or refractory neuroblastoma ) is not yet recruiting in europe , and results are pending . in conclusion , we show that lorlatinib is effective against the alk y1278s mutation in neuroblastoma , whereas this mutation confers primary resistance to crizotinib . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . gudrun schleiermacher honoraria : bristol - myers squibb research funding : bristol - myers squibb ( inst ) , pzer ( inst ) , msdavenir ( inst ) , roche ( inst ) travel , accommodations , expenses : roche no other potential conicts of interest were reported . references chiarle r , voena c , ambrogio c , et al : the anaplastic lymphoma kinase in the pathogenesis of cancer . 
nat rev cancer 8 : 11 - 23 , 2008 solomon bj , mok t , kim dw , et al : first - line crizotinib versus chemotherapy in alk - positive lung cancer . 
moss e yp , lim ms , voss sd , et al : safety and activity of crizotinib for paediatric patients with refractory solid tumours or anaplastic large - cell lymphoma : a childrens oncology group phase 1 consortium study . 
lancet oncol 14 : 472 - 480 , 2013 pearson ad , pinkerton cr , lewis ij , et al : high - dose rapid and standard induction chemotherapy for patients aged over 1 year with stage 4 neuroblastoma : a randomised trial . 
lancet oncol 9 : 247 - 256 , 2008 lewington v , lambert b , poetschger u , et al : 123i - mibg scintigraphy in neuroblastoma : development of a siopen semi - quantitative reporting , method by an international panel . 
matthay kk , shulkin b , ladenstein r , et al : criteria for evaluation of disease extent by ( 123 ) i - metaiodobenzylguanidine scans in neuroblastoma : a report for the international neuroblastoma risk group ( inrg ) task force . 
br j cancer 102 : 1319 - 1326 , 2010 park jr , bagatell r , cohn sl , et al : revisions to the international neuroblastoma response criteria : a consensus statement from the national cancer institute clinical trials planning meeting . 
shaw at , felip e , bauer tm , et al : lorlatinib in non - small - cell lung cancer with alk or ros1 rearrangement : an international , multicentre , open - label , singlearm rst - in - man phase 1 trial . 
yoda s , lin jj , lawrence ms , et al : sequential alk inhibitors can select for lorlatinib - resistant compound alk mutations in alk - positive lung cancer . 
cancer discov 8 : 714 - 729 , 2018 3 : 108ra114 , 2011 cell 26 : 682 - 694 , 2014 infarinato nr , park jh , krytska k , et al : the alk / ros1 inhibitor pf - 06463922 overcomes primary resistance to crizotinib in alk - driven neuroblastoma . 
donella - deana a , marin o , cesaro l , et al : unique substrate specicity of anaplastic lymphoma kinase ( alk ) : development of phosphoacceptor peptides for the assay of alk activity . 
lee cc , jia y , li n , et al : crystal structure of the alk ( anaplastic lymphoma kinase ) catalytic domabiochem j 430 : 425 - 437 , 2010 22 . 
de brouwer s , de preter k , kumps c , et al : meta - analysis of neuroblastomas reveals a skewed alk mutation spectrum in tumors with mycn amplication . 
clin cancer res 16 : 4353 - 4362 , 2010 janoueix - lerosey i , lequin d , brugi `eres l , et al : somatic and germline activating mutations of the alk kinase receptor in neuroblastoma . 
cgp altered physician treatment selection in 25% of evaluable patients ( n = 7 of 28 ) and was associated with improved progression - free survival . conclusion to our knowledge , this is the largest technical evaluation of the performance of cgp in sarcoma . cgp was effectively performed in the vast majority of sarcoma samples and altered physician treatment selection . 
2020 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction sarcomas are uncommon , highly morbid cancers that constitute approximately 1% of all adult malignancies . currently , more than 70 recognized histologic subtypes exist , which makes them extremely challenging to accurately diagnosis and treat.1 sarcomas have multiple genomic alterations , including copy number changes , point mutations , insertions and deletions , and fusions.2 - 4 thus , detailed rna and dna sequence analysis is key for diagnosis as well as for treatment decision - making.5 is not surprising , that comprehensive therefore , genomic proling ( cgp ) is increasingly being used in the evaluation and management of bone and soft tissue sarcomas . 
cgp is the sequencing of dna and rna from tumor samples , which enables the identication of known and novel alterations that may drive inherent oncogenicity.6 - 9 cgp may rene the histologic tumor diagnosis , with its management.10 , 11 indeed , in a study by groisberg et al1 specic to sarcomas , the authors found 61% of 102 patients in a retrospective cohort had a potentially actionable genomic target . ramications despite the potential role that cgp may have in the treatment of sarcoma , the impact of dnaand rnabased cgp on physician decision - making is poorly documented.12 , 13 similarly , it is equally unclear what factors may contribute to the success or failure of cgp in an outpatient clinical setting . 
 challenges in sarcoma comprehensive genomic proling as mentioned previously is unknown ; neither are the relative contributions of biopsy site ( bone v soft tissue ) and methods ( ie , computed tomography [ ct ] - guided core needle biopsy v open excisional biopsy )  . 
to answer these questions , we herein report the results of two studies : the rst is a prospective clinical trial examining the impact of dnaand rna - based cgp on physician decision - making . the second is a retrospective analysis of the success and failure rates of cgp in an even larger patient cohort , which includes the aforementioned patients . methods sarcoma decision impact clinical trial study design . 
to examine the effects of cgp on physician decision - making , a prospective clinical trial ( the ohio state university [ osu ] institutional review board approval no . osu - 12067 ) was performed in collaboration with foundation medicine . 
the primary objectives of the study were to assess the feasibility and logistics associated with a clinical trial using a commercially available cgp platform ( foundationoneheme ; foundation medicine , cambridge , ma ) in an academic clinical setting and to determine the proportion of patients who would receive a cancer - related therapy based on cgp results . 
progression - free survival ( pfs ) was summarized using kaplan - meier survival analysis . the ohio state retrospective sarcoma study data following : date of sample procurement , method of specimen procurement ( eg , excisional biopsy , needle core biopsy , ne needle aspiration ) , biopsy site , specimen source ( hospital ) , and pathology classication by osu . 
the foundation medicine records were interrogated for all sarcoma samples sent by osu and the following information was compiled : specimen type ( formalin - xed parafn - embedded tissue blocks v unstained slides ) , morphologic tumor purity , dna and rna extraction yield , sequencing metrics , and the nature of the released report ( ie , pass , fail , or qualied )  . 
a qualied report indicates a sample for which it was unable to complete the entire cgp process ( eg , rna extraction , low tumor purity ) but for which some genomic information was obtained . in contrast , a passed report indicates a sample for which dna and rna proling was completed successfully . 
2 analysis was used to calculate the signicance of intergroup alterations . results physician decision - making was prospectively altered for 25% of patients with sarcoma who underwent cgp as part of a decision impact trial , patients with sarcoma whose disease had not yet progressed on the current line of therapy were approached to undergo cgp as part of the study . 
treating oncologists were blinded to cgp results time of progression ( based on imaging results )  . until treating oncologists rst documented their treatment decision for the patient with sarcoma without cgp results . cgp data were then released for review and the treating oncologist would note whether their treatment decision had been altered by the cgp results . 
 a hay et al patients with sarcoma diagnosis ( n = 34 ) treatment recommendations chosen before cgp patients with liposarcoma ( n = 15 ) patients with nonliposarcomatous sarcoma ( n = 19 ) no data on whether recommendation changed ( n = 3 ) did not switch therapy on the basis of cgp results ( n = 8 ) switched therapy on the basis of cgp results ( n = 4 ) no data on whether recommendation changed ( n = 3 ) did not switch therapy on the basis of cgp results ( n = 13 ) switched therapy on the basis of cgp results ( n = 3 ) patients assessed for eligibility ( n = 493 ) excluded ( n = 31 ) misdiagnosed or miscategorized tumors excluded ( n = 16 ) duplicates or no clinical data available excluded ( n = 41 ) samples that failed initial cgp remaining individuals evaluated ( n = 408 ) patients included in analysis ( n = 392 ) patients with preliminary reports ( n = 351 ) total no . 
of patients for whom full cgp analysis was completed ( n = 297 ) qualified ( n = 54 ) samples for which cgp could not be completed fig 1 . 
 ( % ) male female mean age ; median ( range ) , years data 14 ( 50 ) 14 ( 50 ) 57 ; 62 ( 2480 ) no change ( n = 12 ) changed ( n = 5 ) p = .03 altered , six patients received the selected treatment ; one patient died before initiating therapy . 
as an exploratory end point , we noted that the median pfs in the cgp - selected group was 124 days versus 54 days in the noncgpselection group ( p = .03 ; fig 2 )  . cgp was performed on almost 400 patients with sarcoma a total of 392 patients representing 413 unique samples were proled over 3 years . 
l - type sarcomas ( ie , leiomyosarcoma , liposarcoma ) constituted the greatest proportion of cases , and this is indicative by the preponderance of tp53 , rb1 alterations and mdm2 and cdk4 amplications ( table 3 )  . fifty - six of the 413 samples ( 13.6% ) had reports qualied for low tumor purity , failed rna extraction , or suboptimal sequencing metrics , whereas 10.7% ( n = 44 of 413 ) samples failed testing . 
examining sarcoma subtypes individually , leiomyosarcomas ( 74.0% ; n = 57 of 77 ) and liposarcomas ( 79.4% ; n = 50 of 63 ) had proportionally higher pass rates than did bone - based sarcomas . 
chordomas had the lowest successful initial genomic proling rate , with a 43% initial pass rate ( table 3 )  . biopsy site and method inuence successful cgp completion biopsy sites . 
the other category encompassed an array of sites , including , but not limited to , brain , eye , epicardium , aorta , lymph node , submandibular gland , bladder , prostate , testes , ovary , cervix , and vagina . 
this was partially due to nding duplicate patients ( ie , some data were obtained with patients identities removed , because they were included in the decision impact trial , which was blinded ; in unblinding , we found some individuals had been included twice )  . 
other reasons included being unable to locate individuals within ihis ( ohio state universitys electronic medical record ) and data necessary for additional analysis ( including biopsy location and method ) were unavailable . 
breakdown of the most common sarcomas subtypes proled sarcoma subtype qualied passed failed total bone - based chondrosarcoma osteosarcoma ewing chordoma soft tissue based leiomyosarcoma liposarcoma spindle cell liposarcoma myxoid liposarcoma pleomorphic liposarcoma well - differentiated liposarcoma dedifferentiated liposarcoma gist synovial myxobrosarcoma angiosarcoma fibromatosis dscrt epithelioid epithelioid hemangioendothelioma solitary brous tumor abbreviations : dscrt , desmoplastic small round cell tumor ; gist , gi stromal tumor . 180 2020 by american society of clinical oncology in conclusion , to our knowledge , this study is the only prospective evaluation of dnaand rna - based cgp in sarcoma on physician decision - making and the largest indepth evaluation of success of cgp in sarcoma to date . 
we note in this cohort that cgp in sarcoma is successful in a large majority of patients and alters physician treatment decision - making in an estimated 25% of patients . 
furthermore , this percentage may have been driven by the fact that the study data were from the era when cdk4 inhibitors were just starting to be considered for use off - label in adipocytic tumors , and conrmation of cdk4 amplication was critical for this drug selection . 
we would anticipate , as time progresses , the types of tumor for which there are dened targetable alterations will increase and thus there would be an increase in physician treatment - decision changes . 
a classic example would be that of gi tumors for which kit / pdgfr sequencing is now considered standard of care for determining whether a patient has these alterations and , if so , whether the patient has resistance alterations.17 a developing example would be that in leiomyosarcoma , where we have previously reported that homologous recombination alterations are a common feature of uterine leiomyosarcomas and may be amenable to parp inhibition.18 tumor location and tissue subtype signicantly clearly , inuence proling success , likely secondary to preanalytic variables that inuence quality of dna and rna , such as decalcication , tumor cellularity , and available tissue volume . 
of note , of the 36 bone biopsy samples that were collected in this study , pathology reports for only 13 mentioned the sample underwent decalcication ; however , no specications regarding the decalcication agent used or the xation times were documented in the report . 
protocols to prevent decalcication during sample processing may aid in yielding higher cgp success rates.19 , 20 in addition , obtaining excisional biopsy specimens rather than imaged - guided biopsy specimens seems to lead to greater likelihood of cgp success . in these studies , it should be mentioned that germline aberrations were not evaluated , because foundation medicine does not test for these . 
 challenges in sarcoma comprehensive genomic proling causes of sample failure causes of sample qualification low cellularity rna failure dna and rna failure dna failure unknown contamination rna failure failed rna metrics low tumor purity noisy cna data contamination rna failure and noisy cna data failed rna metrics and contamination low dna coverage unknown n = 44 samples n = 56 samples fig 3 . 
also , many of our samples are often obtained at outside hospitals , and there is no standardization of pathology report contents . in summary , sarcoma cgp appears to alter physician decision - making regarding treatment and may affect the ultimate outcome of the patient . 
chen consulting or advisory role : novartis , immune design , syapse speakers bureau : novartis , foundation medicine , eisai patents , royalties , other intellectual property : matchtx . no other potential conicts of interest were reported . references groisberg r , hong ds , holla v , et al : clinical genomic proling to identify actionable alterations for investigational therapies in patients with diverse sarcomas . oncotarget 8 : 39254 - 39267 , 2017 abeshouse a , adebamowo c , adebamowo sn , et al : comprehensive and integrated genomic characterization of adult soft 171 : 950 - 965.e28 , 2017 yakirevich e , madison r , fridman e , et al : comprehensive genomic proling of adult renal sarcomas provides insight into disease biology and opportunities for targeted therapies . 
cancer res 76 : 3690 - 3701 , 2016 fang w , ma y , yin jc , et al : comprehensive genomic proling identies novel genetic predictors of response to anti - pd - ( l ) 1 therapies in non - small cell lung cancer . 
clin cancer res 25 : 5015 - 5026 , 2019 chung jh , dewal n , sokol e , et al : prospective comprehensive genomic proling of primary and metastatic prostate tumors . 
jco precis oncol 3 : 1 - 23 , 2019 al - rohil rn , tarasen aj , carlson ja , et al : evaluation of 122 advanced - stage cutaneous squamous cell carcinomas by comprehensive genomic proling opens the door for new routes to targeted therapies . 
ross js , gay lm , wang k , et al : comprehensive genomic proles of metastatic and relapsed salivary gland carcinomas are associated with tumor type and reveal new routes to targeted therapies . 
rodriguez - rodriguez l , hirsheld km , rojas v , et al : use of comprehensive genomic proling to direct point - of - care management of patients with gynecologic 14 . 
thway k , rockcliffe s , gonzalez d , et al : utility of sarcoma - specic fusion gene analysis in parafn - embedded material for routine diagnosis at a specialist 16 . 
thway k , wren d , lee j , et al : evaluation of the optimal provision of formalin - xed , parafn - embedded material for reverse transcription - pcr in soft - tissue 21 : 1315 - 1325 , 2016 cancers . 
singh vm , salunga rc , huang vj , et al : analysis of the effect of various decalcication agents on the quantity and quality of nucleic acid ( dna and rna ) recovered from bone biopsies . 
choi s - e , hong sw , yoon so : proposal of an appropriate decalcication method of bone marrow biopsy specimens in the era of expanding genetic molecular study . 
this article describes medical oncologists condence with genomic testing and the association between genomic condence and test use . methods we used data from the 2017 national survey of precision medicine in cancer treatment to characterize oncologists condence with genomic testing . 
genomic condence was examined separately by type of test user : next - generation sequencing ( ngs ) only , gene expression ( ge ) only , both ngs and ge , or nonuser . predictors of genomic condence were examined with multinomial logistic regression . 
the association between genomic condence and test use was examined with multivariable linear regression . results more than 75% of genomic test users were either moderately or very condent about using results from multimarker tumor panel tests to guide patient care . 
condence with using multimarker tumor panel tests was highest among both ngs and ge test users , with 60.1% very condent in using test results , and lowest among ngs - only test users , with 38.2% very condent in using test results . 
oncologists were most condent in using single - gene tests and least condent in using whole - genome or - exome sequencing to guide patient care . genomic condence was positively associated with self - reported test use . 
in adjusted models , training in genomics , larger patient volume , and treating patients with solid tumors predicted higher genomic condence . onsite pathology services and receipt of electronic medical record alerts for genomic testing predicted lower genomic condence . conclusion oncologists condence varies by testing platform , patient volume , genomic training , and practice infrastructure . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction the landscape of cancer care has changed dramatically over the past decade as therapies are increasingly personalized to the molecular characteristics of a patients tumor.1 whereas genomic testing in oncology started with testing for single mutations in specic genes , advances in molecular proling has spurred the development and now widespread use of multimarker tumor panels.2 , 3 these panels assess different types of genomic alterations commonly detected through nextgeneration sequencing ( ngs ) and gene expression ( ge ) proles . 
such testing can identify therapeutic targets that can be treated with particular anticancer agents and determine when individuals are at higher risk for recurrence and may need therapy.3 , 4 although not standard practice as of yet , whole - genome or whole - exome sequencing is a newer technology that shows promise in informing patient care.4 the rapid proliferation of genomic testing has outpaced the development of practice guidelines on their appropriate use.5 , 6 multimarker tumor panel tests generate vast data about the biology of a patients tumor . 
in cases where the tumor can be successfully sequenced , an actionable target is identied for 39%90% of patients , a wide range that varies by patient population and the size of the panel test.7 - 10 although testing reports typically highlight multimarker panel potentially benecial therapies and relevant clinical trials , individual providers must navigate the process of communicating results to their patients and selecting an appropriate targeted therapy . 
furthermore , multimarker panel testing frequently identies variants of unknown signicance or germline variants , which can further complicate interpretation and care management.11 - 13 very few studies have examined providers attitudes about genomic testing . 
 oncologist condence in genomic testing context key objective this article provides unique data about oncologists in the united states and their condence in using results from commercially available multimarker tumor panel tests to guide decisions about patient treatment and management . knowledge generated oncologists who used both next - generation sequencing ( ngs ) and gene expression tests reported the highest condence in using multimarker tumor panel results to guide patient care ; oncologists who only used ngs tests had the lowest condence . 
oncologists with higher condence were more likely to report using results from multimarker tumor panels to inform patient care . relevance these ndings underscore the importance of genomic training and suggest other providerand practice - level factors that can be leveraged to build oncologists condence in using genomic testing . providers lack condence in using new genomic tests , which could limit the extent to which new tests are appropriately applied in practice.5 , 6 , 14 , 15 for example , providers report less condence in using multimarker tumor panels compared with single - gene tests , which are well established for certain patient populations.6 in addition , providers vary in their understanding of how to interpret and act upon results from whole - genome sequencing , which is not available outside of clinical trials.16 given the potential of precision oncology , there is a need to better understand oncologists attitudes and experiences with genomic testing and to identify factors that foster genomic testing condence . this article builds upon previous studies by describing oncologists condence with genomic testing and the association between condence and genomic test use over the past 12 months . 
oncologists condence in using multimarker tumor panels was rst examined in relation to their condence in using single - gene somatic tests and whole - genome or - exome sequencing . 
oncologists condence was then further characterized by exploring the individualand practice - level characteristics associated with condence and assessing whether their condence was associated with their use of multimarker tumor panels in practice . methods data and study population this study uses data from the national survey of precision medicine in cancer treatment , a nationally representative study of how oncologists use genomic testing in practice . eligible providers were identied from the american medical association physician masterle and selected using multistage probability sampling . 
additional information about the study design and methods have been published elsewhere.17 the survey is available upon request . measures the national survey of precision medicine in cancer treatment collected detailed data about oncologists condence in using genomic testing ; their genomic test use ; and demographics , specialty , and practice characteristics . 
condence was assessed for genomic tests for individual genes or chromosomal alterations ( referred to as single - gene tests ) , commercially available multimarker tumor panel tests , and whole - genome or - exome sequencing . 
response options were very condent , moderately condent , a little condent , or not at all condent . type of genomic test user was determined on the basis of oncologists reported use of 18 specic multimarker tumor panels in the past 12 months . 
the multimarker tumor panel tests included commercially available ge tests ( eg , oncotype dx breast ; genomic health , redwood city , ca ) , commercially available ngs tests ( eg , foundationone ; foundation medicine , cambridge , ma ) , and noncommercial panels performed at an academic medical center . 
training in genomics was also captured and dened as any formal training ( eg , instruction during residency / fellowship , professional lectures or seminars , symposiums , conferences , continuing medical education ) in the use of genomic testing . practice setting information was assessed with questions about the number of unique patients with cancer treated per month . 
responses were categorized as academic medical center or medical school and nonacademic setting . infrastructure to support precision medicine was assessed with a series of questions about whether the respondents primary practice had the following genomic testing services : onsite pathology , internal policies or protocols for use of genomic and biomarker testing , an electronic medical record ( emr ) that alerts when a genomic test is recommended , or a genomic / molecular tumor board . 
response options were categorized as yes and no or do not know . analysis weighted percentages were calculated to describe the sample and provider condence in using single - gene tests , multimarker tumor panel tests , and whole - genome or - exome sequencing . 
two sets of models were examined : one that adjusted for type of genomic test user and a second that simultaneously adjusted for type of genomic test user and the other physician and practice characteristics in the model . 
results are presented as odds ratios and adjusted percentages , also referred to as predicted margins.19 multivariable linear regression was then used to assess whether condence was associated with the percentage of patients for whom multimarker panel test results guided patient care in the past 12 months . 
multivariable models adjusted for years since graduation , sex , race , census region , specialty , training in genomics , practice setting , patient volume , and infrastructure for precision medicine . 
results are presented as adjusted percentages.19 all analyses were conducted using sudaan release 11.0 statistical software ( rti international , research triangle park , nc ) and weighted to account for the complex sampling approach and survey nonresponse . results sample characteristics the sample comprised 1 , 281 oncologists ( table 1 )  . 
participants reported a range of institutional resources to support precision medicine , with onsite pathology and internal policies or protocols for use of genomic and biomarker testing reported most frequently . genomic test use was reported by 95.4% of the sample , with 58.6% using both ngs and ge tests , 26.4% using only ngs tests , and 10.3% using only ge tests . condence using genomic tests in practice condence using multimarker tumor panel tests to guide decisions about patient treatment and management was highest among ngs and ge users , with 60.1% very condent and 35.6% moderately condent in using test results . 
even among oncologists who did not use multimarker tumor panel tests in the past 12 months , 27.1% were very condent and 37.8% were moderately condent in using test results ( fig 1b )  . in contrast to multimarker tumor panel tests , oncologists were more condent in using somatic single - gene tests and less condent in using whole - genome or - exome sequencing ( figs 1a and 1c )  . 
30 female male race white asian other region midwest northeast south west specialty solid and hematologic malignancies hematologic malignancies only solid tumors only training in genomics practice setting practice afliation academic medical center or medical school other practice settingb no . 
percentages may not sum to 100 because of missing data . bother settings include a medical center not afliated with a medical school , community hospital , ofce - based practice , health maintenance organization or integrated health care system , and other . guide decisions about patient treatment and management . in the fully adjusted models ( table 2 ) and in models that only adjusted for the type of genomic test user ( appendix table a1 ) , oncologists with training in genomics had higher condence than those who did not . 
likewise , oncologists who treated 100 patients per month had higher condence than those who treated , 49 patients per month . compared with oncologists who treated both solid and hematologic malignancies , those who only treated solid tumors were more condent , whereas those who treated only hematologic malignancies were less condent in using results of multimarker panel tests to guide patient care . oncologists who practice in institutions with onsite pathology or emr alerts for recommended genomic tests had lower condence than those who practice in institutions without onsite pathology or emr alerts . 
for example , ngs and ge users who were very condent used multimarker panel test results to inform care for 30.97% of their patients ( who had received testing ) compared with 18.44% among ngs and ge users who were not at all or a little condent . 
oncologists condence in using results from ( a ) single - gene tests , ( b ) commercially available multimarker somatic panels , and ( c ) whole - genome or - exome sequencing to guide decisions about patient treatment and management ( n = 1 , 281 )  . 
on the basis of 2 tests for independence , overall differences in condence among 4 types of genomic test users were statistically signicant at p , .001 for single - gene tests , multimarker tumor panels , and whole - genome or - exome sequencing . discussion the current study adds to the literature on provider attitudes about genomic testing . 
most ge panel tests are used to inform the treatment of patients with breast cancer , and there are clear guidelines for test results.20 , 21 for users of other multimarker tumor panel tests , the application of test results to patient management is guideline endorsed for a limited set of clinical indications . testing and the interpretation of tumor panel tests to inform care is more complicated than using single - gene tests . 
at the time the survey was conducted , there were only consensus recommendations for multimarker tumor panel testing in treating nonsmall - cell lung cancer.23 despite this , providers condence using multimarker tumor panel tests was relatively high , with  . 75% of genomic test users reporting that they were either moderately or very condent in using results to guide patient care . 
these ndings are consistent with other studies of provider condence.15 , 24 - 26 oncologists condence also varied by test type , which is consistent with previous research.6 single - gene tests have been used for several decades as companion diagnostics to targeted therapies ; thus , clinical appropriateness and utility are well prescribed.22 even among genomic test nonusers , more than half reported being very condent in using single - gene tests to guide patient care . 
presented are adjusted percentages from multivariable linear regression models that were adjusted for years since graduation , sex , race , census region , specialty , training in genomics , practice setting , and infrastructure for precision medicine . 
historically , providers who treat patients with a hematologic malignancy have technologies ( eg , ow cytometry for relied on different immunophenotyping ) or single - gene somatic tests to identify relevant targeted therapies.27 in contrast , use of multimarker tumor panel tests has been more common in the treatment of solid tumors.23 the importance of experience was also highlighted in our ndings that providers who treat  . 
100 patients per month had higher condence than providers who treat , 50 . providers in high - volume clinics have more opportunity to encounter patients for whom multimarker tumor panel tests are warranted . 
indeed , patient volume has been associated with better treatment outcomes in other settings.28 providers in lower - volume clinics may benet from additional resources , including clinical decision support , to strengthen evidence - based use of genomic testing in treatment planning.29 our ndings underscore the importance of genomic training to increase provider condence in using multimarker panel tests to guide patient care . 
training was dened broadly and included any instruction during residency or fellowship , professional lectures , conferences , or continuing medical education in the use of genomic testing . additional research should identify the specic competencies needed by different types of oncologists and be tailored to support providers who demonstrate relatively low condence in using genomic testing in practice . 
several categories of training could be pursued , including revision of the curricula of medical and nursing schools to provide training in genomics ; advanced training of physicians and other practitioners in genomics ; and continuing medical education to help practicing clinicians to stay up to date on advances in the eld.30 , 31 strategies such as case - based learning , clinical decision - support tools , administrative support for prior authorization , and clinical trial matching may be helpful in strengthening provider condence around genomic testing at the point of care and supporting successful implementation of precision medicine programs.29 genomic testing services available in an oncologists primary practice were either not associated with provider condence or , paradoxically , associated with lower condence . 
oncologists who reported that their practice had onsite pathology spent a lower percentage of time in delivering patient care ( data not shown ) , which could have inuenced their condence in using genomic test results to guide treatment decisions . 
oncologists in settings with onsite pathology could also have been more likely to have a research focus outside of genomics , although that is not something we can explore with our data . in addition , it is possible that other features of the practice setting or availability of appropriate training were more important drivers of provider condence . 
this work should address both the knowledge and the skills to use genomic testing appropriately and to act on test results as well as system - level resources to support precision oncology . our study results should be considered in light of a few limitations . 
first , providers were asked generally about their condence in using genomic test results to guide patient care ; we do not know how condence with a particular testing approach may vary on the basis of specic patient subgroups or clinical scenarios . 
however , participants are representative of practicing oncologists in the united states in terms of age , sex , and geographic location , and all analyses were weighted to adjust estimates for survey nonresponse . 
de moor , phd , mph , healthcare delivery research program , division of cancer control and population sciences , national cancer institute , 9609 medical center dr , room 3e438 , rockville , md 20850 ; e - mail : demoorjs@mail.nih.gov. support supported by the national cancer institute ( nci ) , national human genome research institute , and american cancer society through nci contract no . 
gray stock and other ownership interests : magenta therapeutics ( i ) consulting or advisory role : grail industries , magenta therapeutics ( i ) expert testimony : riley and associates no other potential conicts of interest were reported . references kalia m : biomarkers for personalized oncology : recent advances and future challenges . 
morganti s , tarantino p , ferraro e , et al : complexity of genome sequencing and reporting : next generation sequencing ( ngs ) technologies and implementation of precision medicine in real life . 
crit rev oncol hematol 133 : 171 - 182 , 2019 el - deiry ws , goldberg rm , lenz hj , et al : the current state of molecular testing in the treatment of patients with solid tumors , 2019 . 
bmc health blazer kr , nehoray b , solomon i , et al : next - generation testing for cancer risk : perceptions , experiences , and needs among early adopters in community healthcare settings . 
genet test mol biomarkers 19 : 657 - 665 , 2015 tan o , shrestha r , cunich m , et al : application of next - generation sequencing to improve cancer management : a review of the clinical effectiveness and costeffectiveness . 
j clin oncol serv res 9 : 131 , 2009 33 : 2753 - 2762 , 2015 johnson db , dahlman kh , knol j , et al : enabling a genetically informed approach to cancer medicine : a retrospective evaluation of the impact of comprehensive tumor proling using a targeted next - generation sequencing panel . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
freedman an , klabunde cn , wiant k , et al : use of next - generation sequencing tests to guide cancer treatment : results from a nationally representative survey of oncologists in the united states . 
duffy mj , harbeck n , nap m , et al : clinical use of biomarkers in breast cancer : updated guidelines from the european group on tumor markers ( egtm )  . 
godin g , b elanger - gravel a , eccles m , et al : healthcare professionals intentions and behaviours : a systematic review of studies based on social cognitive theories . 
implement sci 3 : 36 , 2008 johnson lm , valdez jm , quinn ea , et al : integrating next - generation sequencing into pediatric oncology practice : an assessment of physician condence and understanding of clinical genomics . 
allegretti m , fabi a , buglioni s , et al : tearing down the walls : fda approves next generation sequencing ( ngs ) assays for actionable cancer genomic 33 . 
pennell na , mutebi a , zhou z - y , et al : economic impact of next - generation sequencing versus single - gene testing to detect genomic alterations in metastatic nonsmall - cell lung cancer using a decision analytic model . 
unadjusted models of provider and practice characteristics associated with condence in using genomic test results to guide patient management not at all or a little condent moderately condent very condent moderately v not at all or a little condent very condent v not at all or a little condent total wtd % 95% ci wtd % 95% ci wtd % 95% ci 95% ci 95% ci overall p characteristic provider years since graduation 10 11 - 20 21 - 30  . 
unadjusted multinomial logistic regression models controlled for type of genomic test use , which was dened according to the multimarker somatic panel tests each oncologist used in the past 12 months . 
 about ras mutation clearance in plasma ctdna from ras - mutant colorectal cancer patients bouchahda et al1 recently published in your journal . authors conducted a pilot study aimed to investigate the efcacy and safety of antiegfr - targeted therapy added to chemotherapy in patients with unresectable metastatic colorectal cancer with raswild - type circulating tumor dna ( ctdna ) but ras - mutant primary tumor . 
we would like to emphasize the following . in 2017 , our group for the rst time started to investigate the clearance of ras - mutant clones in plasma , supporting an unexpected negative selection of rasmutant clones during the clonal evolution of rasmutant metastatic colorectal cancer ( mcrc ) .2 one year later , we reported that ve patients with rasmutant ras ( ras - mt ) mcrc who switched to wildtype ras ( wt - ras ) in plasma ctdna received egfr inhibitors as a second - line treatment , achieving a durable clinical benet , 3 thus suggesting that ctdna analysis might reveal a therapeutically exploitable window of opportunity , characterized by the prevalence of wt - ras clones , which can be converted in a clinically meaningful benet for patients . 
we published a detailed case report4 in which we described the study of a patient with a primary n - ras - mutant colorectal cancer , who received second - line treatment with antiegfr , after failure of rst - line triplet chemotherapy plus bevacizumab , according to the absence of any clinically relevant mutation of ras genes in blood , achieving a partial response . 
with this background , we designed the currently ongoing kairos trial ( eudract number : 2019 - 001328 - 36 ) , aimed to investigate the efcacy and safety of second - line cetuximab plus chemotherapy treatment in initially ras - mt mcrc patients who converted to raswt at the time of rst progression.3 , 4 we regret having to note that bouchahda et al1 have not cited neither our publications nor have they named the kairos trial in their entire discussion . 
in fact , the authors state that the team of raimondi et al5 recently reported the disappearance of ras - mt clones in ctdna after tumor progression while receiving bevacizumab and chemotherapy in four patients with ras - mt mcrc . 
this last information is incorrect in that we prospectively enrolled mcrc patients at the time of progression of disease and the mutational status of ctdna was assessed before initiating a further line of therapy ( as far as we underthe same inclusion criteria as reported by stand , bouchahda et al1 in their study )  . 
furthermore , bouchahda et al strongly limited the discussion of our data to the number of patients who converted to wt - ras in plasma , omitting to specify that these patients were then treated with egfr blockade based on the results obtained in ctdna . 
in these patients , the introduction of anti - egfr agents , which would have not been supported by international guidelines , allowed to achieve a 12 - month , 10 - month , and 6 - month pfs in three patients treated in second - line setting and a pfs of 4 months in patients treated in fourth - line.5 these data should have been included and discussed . 
finally , the authors state that studies with liquid biopsy have been to date selectively focused on the early detection of the appearance of ras - mt clones in tumor deposits by analyzing ctdna in blood samples from patients with raswt primary tumors . 
bouchahda m , saffroy r , karaboue a , et al : undetectable rasmutant clones in plasma : possible implication for anti - egfr therapy and prognosis in patients with ras - mutant metastatic colorectal cancer . 
gazzaniga p , raimondi c , urbano f , et al : second line egfr - inhibitors in ras mutant metastatic colorectal cancer : the plasma ras wild type window of opportunity . 
gazzaniga p , raimondi c , urbano f , et al : egfr inhibitor as second - line therapy in a patient with mutant ras metastatic colorectal cancer : circulating tumor dna to personalize treatment . 
raimondi c , nicolazzo c , belardinilli f , et al : transient disappearance of ras mutant clones in plasma : a counterintuitive clinical use of egfr inhibitors in ras mutant metastatic colorectal cancer . 
nicolazzo c , belardinilli f , caponnetto s , et al : why the therapeutic impact of ras mutation clearance in plasma ctdna deserves to be further explored in metastatic colorectal cancer . 
 o prospective feasibility study for using cell - free circulating tumor dnaguided therapy in refractory metastatic solid cancers : an interim analysis purpose retrospective studies have demonstrated that cell - free circulating tumor dna ( ctdna ) hotspot testing predicts matched therapy response to firstand second - line therapies in patients with advanced nonsmall - cell lung cancer ( nsclc )  . 
however , no prospective outcomes studies have evaluated ctdna - guided matched therapy decision making on the basis of comprehensive plasma genomic testing including all four major classes of alterations . 
here , we report the clinical utility of this approach in advanced solid tumor cancers . patients and methods we conducted a multiple parallel cohort , open - label , clinical trial using ctdna - guided matched therapy when tissue was insufficient or unobtainable for next - generation sequencing . 
patients with prespecified targetable alterations in metastatic nsclc , gastric cancer ( gc ) , and other cancers were matched to several independent targeted agent trials at a tertiary academic center . results somatic alterations were detected in 59 patients with gc ( 78% ) , and 25 patients ( 33% ) had targetable alterations ( erbb2 , n = 11 ; met , n = 5 ; fgfr2 , n = 3 ; pik3ca , n = 6 )  . 
2017 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the national comprehensive cancer network guidelines recommend genotyping in seven solid tumor cancers ( nonsmall - cell lung cancer [ nsclc ] , breast , gastric , esophageal , colorectal , melanoma , and gi stromal tumors ) for 11 genomic targets ( gts ) to inform targeted therapy selection.1 - 6 however , biopsy specimens can be inadequate for comprehensive profiling in 25% to 50% of patients , 7 - 10 leading to incomplete genotyping or repeat invasive biopsy to obtain more tissue . 
repeat biopsy is also recommended at progression in patients with breast cancer and nsclc to capture targetable genomic changes such as erbb2 ( human epidermal growth factor receptor 2 [ her2 ] ) copy number amplification ( cna ) or egfr and alk resistance mutations , respectively.4 , 5 , 11 comprehensive ctdna testing covering point mutations , insertions / deletions ( indels ) , fusions , seung tae kim kimberly c . 
 and cna may obviate the need for repeat invasive biopsies for genotyping when tissue is of insufficient quantity or unobtainable at initial diagnosis or at progression.12 , 13 in general , next - generation sequencing ( ngs ) seems to detect more actionable variants in target genes than non - ngs methods ( hotspot testing ) such as polymerase chain reaction ( pcr ) , immunohistochemistry ( ihc ) , or fluorescence in situ hybridization.14 - 18 beyond the benefits of invasive biopsy avoidance and higher sensitivity compared with nonngs methods , comprehensive ctdna ngs may provide a global summary of multiple lesions , whereas tissue genotyping of small biopsies may fail to capture intraand intertumor heterogeneity.19 - 21 retrospective studies in nsclc using ctdna genotyping for egfr mutations in the firstline ( egfrl858r / exon19del ) 22 and second - line ( egfrt790m ) 23 , 24 settings have produced response rates similar to studies of therapies directed by tissue - based genotyping . 
the study was conducted in accordance with the current ethical principles outlined in the declaration of helsinki and good clinical practice guidelines . patients eligible patients were older than age 20 years with histologically confirmed metastatic cancer , who had sufficient tumor tissue to test cancer - specific biomarkers but not to undergo comprehensive genomic profiling ( ngs )  . 
rr and disease control rate ( dcr = rr + stable disease ) were centrally adjudicated in accordance with response evaluation criteria in solid tumors ( recist ) version 1.1.28 statistical analysis descriptive statistics were calculated for demographics , ctdna alteration detection rate , and substudy matching . 
after double ultracentrifugation , 5 to 30 ng of cfdna was isolated for digital sequencing as previously described.12 , 26 , 29 all exons in 30 genes and critical exons ( those known to harbor somatic mutations ) of 40 genes were completely sequenced . 
sequencing data were analyzed using a custom bioinformatics pipeline to identify single nucleotide variants ( snvs ) in 70 genes ( 150 - kb panel footprint ) , cnas in 18 genes , indels in three genes ( egfr and erbb2 exons 19 and 20 ; met exon 14 ) , and alk , ret , ros1 , ntrk1 , fgfr2 , and fgfr3 fusions ( appendix fig a2 )  . 
tumor - derived dna shed into the bloodstream increases this value but , as a result of the relative proportions of tumorderived versus leukocyte - derived cfdna , typically a minor contributor . 
90th percentiles , respectively , of all cna calls in the guardant360 database . results patient enrollment and demographics from august 2014 to february 2016 , informed consent was obtained from 210 consecutive patients with metastatic cancer whose tissue was available for cancer - specific biomarker testing , but insufficient for ngs , at initial diagnosis or at progression . 
sixteen patients were lost to follow - up or withdrew consent , leaving 194 patients molecularly profiled by ctdna ngs ( appendix fig a3 )  . median age was 60 years ( range , 28 to 78 years ) for nsclc and 57 years ( range , 23 to 82 years ) for gc , melanoma , and other cancers ; 43% , 58% , 56% , and 89% of patients with these cancers were male , respectively ( table 1 )  . 
newly diagnosed ( firstline ) patients composed 29% of patients with nsclc , 37% of those with gc , 68% of those with melanoma , and 11% of those with other table 1 . 
erbb2 ( her2 ) cna was identified in two patients at progression ( one co - occurring with egfrt790m and one with the erbb2 g778_p780dup ) , and met was amplified in four patients at progression ( one with erbb2 insertion and three with egfrt790m )  . 
however , cnas in nsclc were not prespecified gts . on the basis of rolling substudy availability , inclusion criteria , and patient comorbidities , 10 ( 40% ) of the 25 patients with gc ( erbb2 , n = 6 ; met , n = 1 ; fgfr2 , n = 1 ; and pik3ca , n = 2 ) and 17 ( 50% ) of the 34 patients with nsclc ( egfr , n = 7 ; egfrt790m , n = 7 ; and alk , n = 1 ) with prespecified gts were matched to a molecularly targeted therapy ( tables 2 and 3 )  . 
one patient with gc and two patients with nsclc were lost to follow - up , leaving nine patients ( 90% ) and 15 patients ( 88% ) evaluable for response , respectively . ctdna - guidable targeted therapies and response by cancer type in gc , cnas in erbb2 ( n = 5 ) , fgfr2 ( n = 1 ) , and met ( n = 1 ) and snvs in pik3ca ( n = 2 ) were targeted with one patient achieving complete response ( cr ) , five partial response ( pr ) , and three stable disease ( sd ) for an rr of 67% ( 95% ci , 31% to 91% ) and dcr of 100% ( 95% ci , 63% to 100% ; table 4 , fig 2a )  . 
of patients ctdna alterations detected patients with prespecified second line of therapy third or greater line of therapy treated with matched therapy evaluable for response treated with matched therapy evaluable for response treated with matched therapy evaluable for response treated with matched therapy evaluable for response abbreviations : ctdna , circulating tumor dna ; gt , genomic target . erbb2 amplification amplification fgfr2 amplification pik3ca mutation no . 
one patient with ctdna - detected erbb2 ( her2 ) amplification ( + + + ) achieved complete remission after six cycles of capecitabine , oxaliplatin , and lapatinib ( fig 2b )  . in nsclc , egfrexon19del ( n = 5 ) , egfrl858r ( n = 2 ) , egfrt790m ( n = 7 ) , and alk fusion ( n = 1 ) were targeted , with 13 patients achieving pr and two sd for a rr of 87% ( 95% ci , 58% to 98% ) and a dcr of 100% ( 95% ci , 75% to 100% ; table 4 , fig 2c )  . 
of the seven patients receiving first - line epidermal growth factor receptor inhibitors ( egfri ) , six achieved pr on afatinib , erlotinib , or gefitinib , whereas the one patient with sd received rociletinib . 
similarly , six egfrt790m patients achieving pr were treated with osimertinib or olmutinib , whereas the patient with sd was treated with afatinib plus insulin - like growth factor ligand monoclonal antibody . 
% clinical status at time of ctdna collection new diagnosis treated with matched therapy evaluable for response second line of therapy treated with matched therapy evaluable for response treated with matched therapy evaluable for response treated with matched therapy evaluable for response abbreviations : ctdna , circulating tumor dna ; gt , genomic target . third or greater line of therapy all patients discussion to our knowledge , this is the first prospective ctdna - guided molecular testing program with objective response evaluated in solid tumors . 
this program guided patients in whom biopsy was not readily available or in whom tumor material was not sufficient for comprehensive sequencing to genomically matched therapies available in practice or clinical trials . 
of 194 patients , 30 ( 15.5% ) were successfully enrolled onto one of the ongoing matched therapy clinical trials , a rate comparable to tumor sequencing - based trials . responses to ctdna - guided matched therapy in gc and nsclc were similar to those published in tissue - based matched therapy studies , although the sample sizes here are modest . in gc , cnas were found in erbb2 ( her2 ) , met , and fgfr2 in 31% of our patients , split evenly between newly diagnosed and pretreated patients , consistent with previous primary tumor estimates of these cnas at 20% to 22%.30 , 31 significantly , four ( 80% ) of five patients with erbb2 ( her2 ) - amplified gc responded , including one cr ( fig 2a ) , with all achieving clinical benefit ( cr , pr , or sd )  . 
the one patient with gc with erbb2 cna without pr ( but with sd ) was on lapatinib monotherapy , raising the question of whether chemotherapy produced most of the benefit here . 
however , addition of lapatinib to chemotherapy did produce a significant overall survival benefit in asian patients in the lapatinib optimization study in her2 - positive gastric cancer ( logic ) study.32 in addition , a patient with refractory colon cancer with erbb2 cna achieved sd as best response ( table 4 )  . 
matched therapy response and disease control rate by cancer cohort response gc ( n = 78 ) nsclc ( n = 73 ) melanoma ( n = 34 ) other ( n = 9 ) no . 
thus , an advantage of ctdna over tissue genotyping is that quantitation of the relative vafs can provide an indication of the subclonality and potentially predict treatment response , in contrast to a binary positive or negative result . 
however , a ratio , 10% may be misleading if there is focal amplification of the egfr driver mutation and not egfrt790m.42 beyond t790m , recent reports suggest that comprehensive profiling at progression may be important in nsclc given the multiple other resistance mechanisms after egfri therapy.43 these include non - egfrt790m on - target point mutations , as well as bypass mutations in braf , kras , mek , and pik3ca ; cnas in met and erbb2 ; fusions in alk ; or rb1 inactivation heralding epithelial to mesenchymal cell transition.34 , 44 - 47 because egfrt790m is the resistance mechanism in only half of patients experiencing progression on firstline egfri , a comprehensive ctdna ngs test covering all major types of genomic alterations is particularly relevant . small sample sizes for targeted therapy in melanoma and colon cancer limit the conclusions that can be drawn in those cohorts ; however , the rr cis in gc and nsclc are consistent with tissue - guided matched therapy rrs . 
single - arm objective rrs exceeding 30% have led to us food and drug administration regulatory approval of matched therapies.48 , 49 the rrs to ctdna - detected alterations in this interim analysis ( 67% [ 95% ci , 31% to 91% ] for gc and 87% [ 95% ci , 58% to 98% ] for nsclc ) support clinical utility for guardant360 in patients with advanced nsclc and gc in whom tissue is insufficient or inaccessible and build upon previous validation studies of the diagnostic test used herein.12 , 26 because this study was not randomized , its primary limitation is the potential for selection bias to enroll patients more likely to benefit . 
not all patients with targetable alterations could receive matched therapy because of the various requirements of the multiple parallel matched therapy substudy protocols , performance status , or loss to follow - up . 
future studies should examine ctdnaguided matched therapy outcomes in more racially diverse cohorts . to our knowledge , this is the first prospective study to examine the clinical utility of comprehensive ctdna genomic testing to guide matched therapy selection . 
lanman , amirali talasaz , keunchil park , jeeyun lee financial support : young suk park , amirali talasaz administrative support : young suk park , amirali talasaz provision of study materials or patients : seung tae kim , se hoon park , joon oh park , young suk park , ho yeong lim , won ki kang , amirali talasaz , keunchil park , jeeyun lee collection and assembly of data : seung tae kim , kimberly c . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . ho yeong lim no relationship to disclose won ki kang no relationship to disclose seung tae kim no relationship to disclose kimberly c . 
banks employment : guardant health stock and other ownership interests : guardant health se - hoon lee honoraria : astrazeneca / medimmune , roche , bristol - myers squibb , merck consulting or advisory role : pfizer , novartis , astrazeneca , bristol - myers squibb travel , accommodations , expenses : novartis kyung kim no relationship to disclose joon oh park honoraria : celgene consulting or advisory role : celgene speakers bureau : celgene research funding : celgene , astrazeneca se hoon park no relationship to disclose young suk park no relationship to disclose richard b . 
lanman employment : guardant health , veracyte leadership : guardant health stock and other ownership interests : guardant health , veracyte research funding : guardant health amirali talasaz employment : guardant health leadership : guardant health stock and other ownership interests : guardant health research funding : guardant health patents , royalties , other intellectual property : guardant health travel , accommodations , expenses : guardant health keunchil park consulting or advisory role : astellas pharma , astrazeneca , boehringer ingelheim , clovis oncology , eli lilly , hanmi , kyowa hakko kirin , novartis , ono pharmaceutical , roche speakers bureau : boehringer ingelheim research funding : astrazeneca jeeyun lee no relationship to disclose affiliations support seung tae kim , se hoon park , kyung kim , joon oh park , se - hoon lee , young suk park , ho yeong lim , won ki kang , keunchil park , and jeeyun lee , samsung medical center , sungkyunkwan university school of medicine , seoul , korea ; and kimberly c . 
j natl compr canc netw 13 : 448 - 475 , 2015 von mehren m , randall rl , benjamin rs , et al : gastrointestinal stromal tumors , version 2.2014. 
sundaresan tk , sequist lv , heymach jv , et al : detection of t790m , the acquired resistance egfr mutation , by tumor biopsy versus noninvasive blood - based analyses . 
thompson jc , yee ss , troxel ab , et al : detection of therapeutically targetable driver and resistance mutations in lung cancer patients by next - generation sequencing of cell - free circulating tumor dna . 
novello s , barlesi f , califano r , et al : metastatic non - small - cell lung cancer : esmo clinical practice guidelines for diagnosis , treatment and follow - up . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
lebofsky r , decraene c , bernard v , et al : circulating tumor dna as a non - invasive substitute to metastasis biopsy for tumor genotyping and personalized medicine in a prospective trial across all tumor types . 
lim sm , kim ey , kim hr , et al : genomic profiling of lung adenocarcinoma patients reveals therapeutic targets and confers clinical benefit when standard molecular testing is negative . 
schrock ab , frampton gm , herndon d , et al : comprehensive genomic profiling identifies frequent drug - sensitive egfr exon 19 deletions in nsclc not identified by prior molecular testing . 
ali sm , hensing t , schrock ab , et al : comprehensive genomic profiling identifies a subset of crizotinib - responsive alkrearranged non - small cell lung cancer not detected by fluorescence in situ hybridization . 
rozenblum ab , ilouze m , dudnik e , et al : clinical impact of hybrid capture - based next - generation sequencing on changes in treatment decisions in lung cancer . 
karachaliou n , mayo - de las casas c , queralt c , et al : association of egfr l858r mutation in circulating free dna with survival in the eurtac trial . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced non - small - cell lung cancer . 
liang dh , ensor je , liu z - b , et al : cell - free dna as a molecular tool for monitoring disease progression and response to therapy in breast cancer patients . 
kim st , lee w - s , lanman rb , et al : prospective blinded study of somatic mutation detection in cell - free dna utilizing a targeted 54 - gene next generation sequencing panel in metastatic solid tumor patients . 
zill oa , mortimer sa , banks kc , et al : somatic genomic landscape of over 15 , 000 patients with advanced - stage cancer from clinical next - generation sequencing analysis of circulating tumor dna . 
zill oa , greene c , sebisanovic d , et al : cell - free dna next - generation sequencing in pancreatobiliary carcinomas . cancer discov 5 : 1040 - 1048 , 2015 30 . 
deng n , goh lk , wang h , et al : a comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co - occurrence among distinct therapeutic targets . 
hecht jr , bang y - j , qin sk , et al : lapatinib in combination with capecitabine plus oxaliplatin in human epidermal growth factor receptor 2 - positive advanced or metastatic gastric , esophageal , or gastroesophageal adenocarcinoma : trio - 013 / logica randomized phase iii trial . 
arrieta o , cardona af , martn c , et al : updated frequency of egfr and kras mutations in nonsmall - cell lung cancer in latin america : the latin - american consortium for the investigation of lung cancer ( clicap )  . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as first - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
sequist lv , yang jc - h , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
vallee a , audigier - valette c , herbreteau g , et al : rapid clearance of circulating tumor dna during treatment with azd9291 of a lung cancer patient presenting the resistance egfr t790m mutation . 
marchetti a , palma jf , felicioni l , et al : early prediction of response to tyrosine kinase inhibitors by quantification of egfr mutations in plasma of nsclc patients . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a third - generation egfr inhibitor . 
liang w , he q , chen y , et al : metastatic eml4 - alk fusion detected by circulating dna genotyping in an egfrmutated nsclc patient and successful management by adding alk inhibitors : a case report . 
stewart el , tan sz , liu g , et al : known and putative mechanisms of resistance to egfr targeted therapies in nsclc patients with egfr mutations : a review . 
 discordance in human epidermal growth factor receptor 2 ( her2 ) phenotype between primary tumor and circulating tumor cells in women with her2 - negative metastatic breast cancer purpose discordance in human epidermal growth factor receptor 2 ( her2 ) status between primary tumor and metastases might have important implications for treatment response and therapy decisions . 
here , we evaluate both the frequency of circulating tumor cells ( ctcs ) and the factors predicting her2 discordance between primary tumor and ctcs as a potential surrogate for tumor biology and tumor heterogeneity in patients with metastatic breast cancer . patients and methods the number of ctcs in 7.5 ml of peripheral blood and her2 status were evaluated in 1 , 123 women with her2 - negative metastatic breast cancer . 
2017 by american society of clinical oncology introduction circulating tumor cells ( ctcs ) are observed in early and metastatic breast cancer ( mbc ) , and their prognostic relevance has been demonstrated in both early and advanced disease.1 , 2 according to previous studies , approximately 65% to 85% of patients with mbc have detectable ctcs , and approximately half of these patients have five or more ctcs in 7.5 ml of peripheral blood.2 , 3 in addition to the prognostic value of ctcs as assessed before treatment , monitoring ctc dynamics during therapy provides important information on therapy response.4 - 7 however , valuable information with regard to therapy response and suitability of additional treatment options may be provided not only by the prevalence and changes in the number of ctcs but also by the phenotype of ctcs . 
friedl jens huober christoph scholz nikolaus de gregorio brigitte rack elisabeth trapp marianna alunni - fabbroni sabine riethdorf volkmar mueller andreas schneeweiss klaus pantel franziska meier - stiegen bernadette jaeger andreas hartkopf florin - andrei taran peter a . 
assessing ctc phenotype may be especially important in mbc , because it can be used as a noninvasive liquid biopsy to characterize the metastatic disease , thus reflecting tumor heterogeneity and possible discordance in hormone receptor and / or human epidermal growth factor receptor 2 ( her2 ) expression with potentially far - reaching implications in terms of follow - up treatment and additional targeted therapies . although discordance in her2 status among primary tumor , distant metastases , and ctcs has been described in several studies , 3 , 8 - 10 it has not been implemented in clinical practice to guide therapy decisions . 
the study concept was in accordance to the declaration of helsinki , adhered to good clinical practice and german pharmaceutical law , and was approved by the local ethic committees of the participating centers . assessment of ctc presence and her2 phenotype on ctcs from all patients , 7.5 - ml peripheral blood samples were collected , and presence and phenotype of ctcs were assessed as previously described in detail , 11 using the semiautomatic and standardized cellsearch system ( janssen diagnostics , raritan , nj ) , which is the only us food and drug administrationapproved method for the enumeration of ctcs . 
for her2 assessment , cells were also labeled with her2 antibodies , and ctcs were considered as her2 positive only if they showed a strong ihc staining intensity for her2 ( ihc score , 3 + )  . 
analyses for determining ctc prevalence and her2 phenotype of ctcs were performed by trained scientists with a peer - review system at four independent reference laboratories . statistical calculations descriptive statistics for the categorical data are provided in terms of absolute and relative frequencies . 
the non - normally distributed continuous variables age ( in years ) and time interval between primary diagnosis and screening ( in months ) are described by medians and ranges . 
associations between presence of ctcs or presence of her2 - positive ctcs and patient or tumor characteristics were evaluated using mann - whitney u tests for age and time interval between primary diagnosis and screening , and x2 tests were used for all other categorical variables . 
to assess which factors predicted discordance in the her2 phenotype between primary tumor and ctcs , we used a multivariable logistic regression model with discordance in her2 status ( yes v no ) as a binary response variable and a stepwise backward selection procedure ( significance level cutoff for exclusion , .05 [ likelihood ratio test ] )  . 
demographic and primary tumor characteristics of patients with her2negative mbc screened for ctcs within the detect study program ( n = 1 , 123 ) characteristic age at screening , years total no . 
 ( % ) of patients time between primary diagnosis and screening , months median range median range menopausal status at screening premenopausal postmenopausal unknown tumor stage unknown nodal stage unknown histologic grade unknown histologic type invasive ductal invasive lobular other hormone receptor status negative positive unknown 26 - 89 0 - 450 136 ( 12.1 ) 734 ( 65.4 ) 253 ( 22.5 ) 308 ( 27.4 ) 503 ( 44.8 ) 114 ( 10.2 ) 125 ( 11.1 ) 13 ( 1.2 ) 60 ( 5.3 ) 363 ( 32.3 ) 378 ( 33.7 ) 147 ( 13.1 ) 136 ( 12.1 ) 99 ( 8.8 ) 47 ( 4.2 ) 576 ( 51.3 ) 406 ( 36.2 ) 94 ( 8.4 ) 751 ( 66.9 ) 199 ( 17.7 ) 173 ( 15.4 ) 171 ( 15.2 ) 886 ( 78.9 ) 66 ( 5.9 ) had hormone receptorpositive invasive ductal tumors . 
median number of ctcs detected in ctc - positive patients was seven ( interquartile range , two to 30 ; range , one to 35 , 078 ctcs )  . 
frequency distribution of the number of ctcs detected is shown in appendix figure a1 . presence of at least one ctc was significantly associated with nodal stage and histologic type of the primary tumor but not with other patient or primary tumor characteristics ( table 2 )  . 
in 158 patients ( 22.2% ) , at least one ctc with an her2 2 + ihc score , but no ctcs with an her2 3 + ihc score , was detected ; these patients were not considered to have her2 - positive ctcs in the blood ( as described in patients and methods )  . 
patients with grade 3 primary tumors were less likely to have her2 - positive ctcs than patients with grade 1 or 2 primary tumors ( p = .028 ; fig 3a )  . 
patients with invasive lobular primary tumors were more likely to have her2positive ctcs than patients with other primary tumor histologic types ( p , .001 ; fig 3b ) , and patients with hormone receptorpositive primary tumors were more likely to have her2 - positive ctcs than patients with hormone receptor negative ( ie , triple negative ) primary tumors ( p , .001 ; fig 3c )  . 
of her2 - positive ctcs 6 - 10 11 - 50 > 50 predictors of discordance in her2 status between primary tumor and ctcs to evaluate which factors can independently predict discordance in her2 status between primary tumor and ctcs , we used a multivariable logistic regression model with discordance in her2 status ( yes v no ) as a binary response variable . 
patient and primary tumor characteristics included as independent factors were patient age in years , time since primary diagnosis in months , tumor stage ( pt ) , nodal stage ( pn ) , histologic grade , histologic type , and hormone receptor status . 
to account for the association between number of ctcs detected and presence of her2 - positive ctcs , we included number of ctcs ( one to four v > five ctcs ) as an additional explanatory variable . 
please note that the or for age listed in table 3 ( ie , 0.977 ) corresponded to the change of the odds of showing discordance in her2 phenotype associated with a 1 - year increase in age . discussion to our knowledge , the combined ctc screening of the detect study program provides the largest worldwide cohort of patients with mbc tested with regard to both rate of discordance in her2 phenotype between primary tumor and ctcs and possible predictors of her2 discordance . 
our analyses revealed an overall ctc prevalence of 63.3% in 1 , 123 patients with her2 - negative mbc , which is within the range reported in other studies on mbc.2 , 3 , 12 discordance in her2 phenotype between primary tumor and ctcs was observed in 18.8% of 711 ctc - positive patients and was independently predicted by histologic type and hormone receptor status of the primary tumor . 
of ctcs 11 - 50 > 50 6 - 10 11 - 25 > 25 her2 - positive ctcs ( % ) her2 status was more frequent in patients with five or more ctcs compared with patients with fewer than five ctcs . some previous studies have reported even higher discordance rates , although with considerably smaller sample sizes . 
lobular carcinomas are less cohesive tumors that are characterized by impaired cell - cell adhesion with reduced expression of the adhesion molecule e - cadherin.19 , 20 reduced cell and tissue adhesion may lead to an easier spread of tumor cells and could be one explanation for the association of presence of ctcs with lobular carcinomas . 
in general , her2 is rarely amplified or overexpressed in lobular carcinomas21 ; thus , the fact that we observed an association between presence of her2 - positive ctcs and lobular carcinomas is surprising and not easily explained . there is some evidence that lobular breast cancer shows a higher frequency of her2 mutations compared with ductal breast cancer.22 - 24 therefore , it could be speculated that the increased rate of her2 discordance observed in lobular carcinomas might be related to her2 mutations that affect her2 expression and membrane staining . the fact that hormone receptorpositive primary tumors exhibit higher rates of her2 discordance than triple - negative tumors is also a new finding that must be explored in more detail . clearly , additional investigations of tumor biology and pathogenesis of ctcs are necessary to help us understand these results . regardless of the underlying mechanisms , our findings may have implications for clinical practice . 
data on changes in her2 status during tumor progression represent crucial information for adequate patient therapy , because they may lead to modification of systemic and / or addition of targeted treatments . 
on the basis of our results , we suggest physicians consider attempting to obtain additional biopsies of metastatic lesions for detection of potential changes in her2 phenotype , especially in patients with lobular carcinomas or hormone receptorpositive primary tumors , because these are risk factors for her2 discordance identified in our study . 
prevalence of at least one human epidermal growth factor receptor 2 ( her2 ) positive circulating tumor cell ( ctc ; ie , discordance rate of her2 status [ % ] ) according to tumor characteristics of the primary tumor . 
 ( a ) prevalence of at least one her2 - positive ctc according to histologic grade of the primary tumor in 654 ctc - positive patients with her2 - negative metastatic breast cancer ( mbc ) screened for the detect study program ( for 57 patients , histologic grade of the primary tumor was unknown ; table 2 )  . 
 ( b ) prevalence of at least one her2 - positive ctc according to histologic type of the primary tumor in 711 ctc - positive patients with her2 - negative mbc screened for the detect study progra ( c ) prevalence of at least one her2positive ctc according to hormone receptor status of the primary tumor in 670 ctc - positive patients with her2 - negative mbc screened for the detect study program ( for 41 patients , hormone receptor status of the primary tumor was unknown ; table 2 )  . therapy in patients with histologically her2positive mbc revealed discordance of her2 status between tissue and ctcs in 62% of patients , and negative her2 status of ctcs was significantly associated with shorter progressionfree survival after the new line of anti - her2 therapy.25 another recent study indicated that her2 - targeted therapy with lapatinib was effective in decreasing the number of her2positive ctcs in patients with mbc.26 if additional research confirms that ctcs can be used as an easily accessible liquid biopsy to assess changes in tumor biology and her2 status of metastases , detection of her2 - positive ctcs in patients with mbc with her2negative primary tumors might even trigger the addition of her2 - targeted therapies without the need for a confirmatory biopsy of metastatic lesions . 
although primary tumors were considered her2 positive if more than 10% of tumor cells showed protein overexpression , her2 - positive ctc status was defined as presence of at least one ctc with an her2 3 + ihc score in the blood . 
furthermore , because this study was based on the initial screening results of the detect study program , and only a subsample of screened patients was recruited in one of the detect clinical trials , associations between ctc prevalence or presence of her2 - positive ctcs with metastatic disease patterns and patient outcomes could not be analyzed at this stage . 
ctc detection was based on an epithelial cell adhesion molecule selection process ; therefore , ctcs undergoing epithelial - tomesenchymal transition with phenotypic changes in terms of lacking epithelial cell adhesion molecule expression and gaining mesenchymal and / or stem - cell marker characteristics might have been missed , which could have led to falsely low rates of ctc positivity . 
furthermore , her2 status of ctcs was assessed by ihc only and was not confirmed using fish . in conclusion , discordance in her2 status between primary tumor and ctcs was observed in 18.8% of patients with her2 - negative mbc and was associated with lobular carcinomas , hormone receptorpositive primary tumors , and high ctc counts . 
moreover , the concept of liquid biopsy using ctcs as a real - time noninvasive monitoring tool to evaluate tumor biology , progression , and heterogeneity as a basis for more personalized treatment decisions should be tested in prospective randomized clinical trials . 
fasching provision of study material or patients : amelie de gregorio , jens huober , nikolaus de gregorio , brigitte rack , elisabeth trapp , andreas schneeweiss , klaus pantel , andreas hartkopf , peter a . 
fasching , tanja fehm collection and assembly of data : amelie de gregorio , christoph scholz , nikolaus de gregorio , brigitte rack , elisabeth trapp , sabine riethdorf , volkmar mueller , andreas schneeweiss , klaus pantel , franziska meier - stiegen , bernadette jaeger , andreas hartkopf , florin - andrei taran , peter a . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . amelie de gregorio consulting or advisory role : roche pharma ag thomas w.p. 
 jens huober honoraria : novartis , roche consulting or advisory role : novartis , roche travel , accommodations , expenses : novartis , roche christoph scholz consulting or advisory role : roche pharma ag research funding : novartis ( inst ) , roche pharma ag ( inst ) , janssen oncology ( inst ) nikolaus de gregorio consulting or advisory role : roche travel , accommodations , expenses : astrazeneca , tesaro brigitte rack consulting or advisory role : novartis speakers bureau : roche , pfizer research funding : sanofi ( inst ) , novartis ( inst ) , eli lilly ( inst ) , astrazeneca ( inst ) , chugai pharma ( inst ) , janssen diagnostics ( inst ) travel , accommodations , expenses : pfizer elisabeth trapp no relationship to disclose marianna alunni - fabbroni no relationship to disclose volkmar mueller consulting or advisory role : astrazeneca , celgene , daiichi sankyo , eisai , nektar , genentech , novartis travel , accommodations , expenses : pfizer , roche pharma ag andreas schneeweiss honoraria : roche pharma ag , celgene , astrazeneca , pfizer , novartis , amgen , roche pharma ag ( inst ) , pfizer ( inst ) research funding : roche pharma ag ( inst ) , celgene ( inst ) travel , accommodations , expenses : roche , celgene , amgen klaus pantel honoraria : agena bioscience consulting or advisory role : wntresearch , roche , novartis , sanofi research funding : janssen diagnostics franziska meier - stiegen consulting or advisory role : amgen bernadette jaeger no relationship to disclose andreas hartkopf no relationship to disclose florin - andrei taran no relationship to disclose peter a . 
fasching honoraria : roche , amgen , novartis , pfizer , celgene research funding : novartis ( inst ) wolfgang janni honoraria : janssen diagnostics research funding : janssen diagnostics tanja fehm consulting or advisory role : roche , novartis , amgen research funding : novartis acknowledgment we thank all the patients for participating in this study and donating their blood samples for research purposes . 
friedl , jens huober , christoph scholz , nikolaus de gregorio , and wolfgang janni , university hospital ulm , ulm ; brigitte rack , elisabeth trapp , and marianna alunni - fabbroni , hospital of ludwig - maximilians - university , munich ; sabine riethdorf , volkmar mueller , and klaus pantel , university hospital hamburg - eppendorf , hamburg ; andreas schneeweiss , university hospital heidelberg , heidelberg ; franziska meier - stiegen , bernadette jaeger , and tanja fehm , heinrichheine - university duesseldorf , duesseldorf ; andreas hartkopf and florin - andrei taran , university hospital tuebingen , tuebingen ; and peter a . 
fasching , university hospital erlangen , erlangen , germany . affiliations support the detect study program is supported by the investigator - initiated study program of janssen diagnostics , with clinical trials also supported by pierre fabre pharma , teva pharmaceuticals industries , amgen , novartis pharma , and eisai ; study medications vinorelbine , nonpegylated liposomal doxorubicin , lapatinib and everolimus , eribulin , and pertuzumab were provided free of charge by pierre fabre pharma , teva pharmaceuticals industries , novartis pharma , eisai , and roche , respectively . the funding sources had no role in study design ; data collection , analysis , or interpretation ; or writing of the report . 
bidard fc , peeters dj , fehm t , et al : clinical validity of circulating tumour cells in patients with metastatic breast cancer : a pooled analysis of individual patient data . 
fehm t , m uller v , aktas b , et al : her2 status of circulating tumor cells in patients with metastatic breast cancer : a prospective , multicenter trial . 
hayes df , cristofanilli m , budd gt , et al : circulating tumor cells at each follow - up time point during therapy of metastatic breast cancer patients predict progression - free and overall survival . 
pierga jy , hajage d , bachelot t , et al : high independent prognostic and predictive value of circulating tumor cells compared with serum tumor markers in a large prospective trial in first - line chemotherapy for metastatic breast cancer patients . 
simmons c , miller n , geddie w , et al : does confirmatory tumor biopsy alter the management of breast cancer patients with distant metastases ? ann oncol 20 : 1499 - 1504 , 2009 10 . 
ligthart st , bidard fc , decraene c , et al : unbiased quantitative assessment of her - 2 expression of circulating tumor cells in patients with metastatic and non - metastatic breast cancer . 
schramm a , friedl tw , schochter f , et al : therapeutic intervention based on circulating tumor cell phenotype in metastatic breast cancer : concept of the detect study prograarch gynecol obstet 293 : 271 - 281 , 2016 12 . 
tewes m , aktas b , welt a , et al : molecular profiling and predictive value of circulating tumor cells in patients with metastatic breast cancer : an option for monitoring response to breast cancer related therapies . 
wallwiener m , hartkopf ad , riethdorf s , et al : the impact of her2 phenotype of circulating tumor cells in metastatic breast cancer : a retrospective study in 107 patients . 
houssami n , macaskill p , balleine rl , et al : her2 discordance between primary breast cancer and its paired metastasis : tumor biology or test artefact ? insights through meta - analysis . 
aurilio g , disalvatore d , pruneri g , et al : a meta - analysis of oestrogen receptor , progesterone receptor and human epidermal growth factor receptor 2 discordance between primary breast cancer and metastases . 
sinn hp , helmchen b , heil j , et al : lobular neoplasms and invasive lobular breast cancer [ in german ] pathologe 35 : 45 - 53 , 2014 20 . 
gomes ds , porto ss , rocha rm , et al : usefulness and limitations of e - cadherin and b - catenin in the classification of breast carcinomas in situ with mixed pattern . 
ross js , wang k , sheehan ce , et al : relapsed classic e - cadherin ( cdh1 ) - mutated invasive lobular breast cancer shows a high frequency of her2 ( erbb2 ) gene mutations . 
zhang s , li l , wang t , et al : real - time her2 status detected on circulating tumor cells predicts different outcomes of anti - her2 therapy in histologically her2 - positive metastatic breast cancer patients . 
 appendix results additional data regarding both the association between hormone receptor status and histologic type and rates of human epidermal growth factor receptor 2 ( her2 ) discordance in relation to the combined hormone receptor and tumor type status are as follows : hormone receptor status and histologic type of primary tumors were significantly associated with each other ( p , .001 ; n = 670 ; 41 patient cases with missing values for hormone receptor status )  . 
frequency distribution of the number of circulating tumor cells ( ctcs ) detected in 7.5 - ml peripheral blood samples from 1 , 123 patients with human epidermal growth factor receptor 2negative metastatic breast cancer screened for the detect study program ( cutoff for ctc positivity , > one ctc )  . 6 - 10 11 - 50 > 50 no . 
the aim is to characterize the availability and scope of economic evidence . materials and methods we searched medline ( pubmed ) , embase ( ovid ) , and web of science databases for english - language full - text peer - reviewed articles published between 2000 and 2016 . 
we found testing was frequently used to predict prognosis ( 67% ) , to diagnose patients ( 24% ) , or to identify targeted therapeutic options ( 7% )  . 
deterministic and probabilistic analyses were typically used to characterize parameter and decision uncertainty ( 91% and 75% )  . conclusion although the availability of economic evidence examining precision oncology increased over time , methods used often did not align with current guidelines . 
regier , ma , phd , bc cancer research centre , 675 west 10th ave , vancouver , british columbia , canada , v5z 1l3 ; e - mail : dregier@bccrc.ca. introduction precision oncology is transforming routine cancer care . 
historically , cancers have been classified and treated according to their anatomic site of origin.1 now , precision oncology is shifting focus to the individual by using information on a patients genomic profile to better prevent , treat , and prognosticate disease.2 - 4 precision oncology tests range from single - gene tests to more comprehensive strategies involving next - generation sequencing ( ngs ) technologies . 
although recent scientific advances have resulted in improvements in speed and throughput of ngs technologies , 5 the state of current economic evidence supporting resource allocation decisions in cancer control is unknown . past studies reviewing economic evaluations surrounding personalized medicine found that few tests had been formally evaluated for their cost effectiveness as of 2013.6 - 8 the majority of reviewed studies examined the trade off between costs and effectiveness of older single - gene tests . 
 determine expression profiles for large numbers of genes . proponents of precision oncology report that genomic testing has the potential to reduce health system costs and improve patients health through targeted therapies and treatment stratification.11 , 12 yet , genomic testing will also involve significant expenditures that may challenge the affordability of adopting ngs technologies in routine practice . 
in text : precision * or personalized * or individualized * or sequenc * or next generation or genetic * or genom * or companion diag * or predictive testing or gene or genotype or mutation and 3 . 
in text : oncology or cancer these search terms were developed on the basis of relevant articles identified in exploratory searches and search terms used in prior systematic reviews of economic evaluations of personalized medicine and ngs technologies.6 - 8 after initial identification , we imported all articles into endnote x6 ( reuters , new york )  . 
 quality assessment of the studies was restricted to analyzing transparency . given the differences across included studies , we summarized cost - effectiveness findings according to ngs technology , test strategy , and cancer type . 
we compared incremental cost effectiveness , expressed in terms of cost per quality adjusted life - year ( qaly ) gained separately from incremental cost effectiveness expressed in terms of cost per life - year gained ( lyg )  . 
all monetary outcomes were converted to 2016 us dollars using country - specific inflation and exchange rates . results search results the database search identified 1 , 350 records , of which 577 were duplicates . 
ngs , next - generation sequencing . records identified through database searching ( n = 1 , 350 ) additional records identified through other sources ( n = 6 ) records after duplicates removed ( n = 779 ) records excluded ( conference abstracts ; n = 238 ) records screened for eligibility ( n = 541 ) records excluded ( unrelated to ngs or evaluation incomplete ; n = 446 ) full - text articles assessed for eligibility ( n = 95 ) studies included in qualitative synthesis ( n = 55 ) full - text articles excluded ( n = 40 ) unable to access or not in english ( n = 5 ) evaluation incomplete ( n = 10 ) not ngs ( n = 24 ) reported duplicate results ( n = 1 ) most common reasons for exclusion were that studies did not focus on ngs technologies ( n = 24 ) or did not include full economic evaluations comparing costs and health consequences of two or more competing technologies ( n = 10 )  . 
approximately 20% to 25% metastasize to distant sites and are generally associated with poor response to treatment.1 outcomes with systemic chemotherapy have historically been poor.2 with improved understanding of molecular biology of these tumors , we are beginning to identify promising potential therapeutic targets . in particular , the human epidermal growth factor receptor 2 / neu ( her2 / neu ) oncogene , one of the tyrosine kinase receptors , is overexpressed in salivary duct carcinomas ( 44% ) , salivary gland adenocarcinomas ( 21% ) , and adenoid cystic carcinomas ( 2% ) , among other subtypes.3 trastuzumab , a monoclonal antibody that binds to the extracellular domain of her2 / neu , inhibits the proliferation of tumor cells that overexpress her2 / neu.4 patients with her2 / neu - overexpressing sgns are often treated with trastuzumab - containing regimens with encouraging results , but disease progression is inevitable , even with a favorable initial response . 
the antibody - drug conjugate adotrastuzumab emtansine ( t - dm1 ) is currently approved for treating her2 - positive metastatic breast cancer that has progressed on therapy with trastuzumab . this antibody - drug conjugate selectively directs the cytotoxic drug emtansine to tumor cells with her2 / neu expression , thereby minimizing systemic toxicities.5 results favorable given the seen with adotrastuzumab emtansine in patients with breast cancer , it is logical to consider administering it to patients with sgns that overexpress her2 / neu after they have progressed on trastuzumab with or without chemotherapy . 
sequential her2 / neu - directed therapy has been successfully used with sustained clinical benet , albeit in a single patient.6 here we report on the clinical outcomes of seven patients with metastatic sgns who were treated at our institution with adotrastuzumab emtansine ( table 1 ) , and we summarize the clinical course and response to therapy of one patient . a 45 - year - old man presented with a painless right neck mass in late 2013 . 
fine - needle aspiration revealed a high - grade carcinoma and positron emission tomography / ct ( pet / ct ) showed multiple uorodeoxyglucose ( fdg ) - avid lymph nodes in the right cervical region . 
surgical pathology revealed a 3.9 - cm high - grade salivary duct carcinoma that was positive for androgen receptor ( ar ) and her2 / neu ( 3 + ) by immunohistochemistry ( ihc ) staining . 
because of the high - risk features of extracapsular nodal extension and close margins , he received adjuvant chemotherapy with cisplatin and radiation therapy once per week in october 2014 . 
 ( c ) restaging scan in june 2018 after ado - trastuzumab emtansine shows a complete metabolic response of previously noted metastatic lymphadenopathy . currently a void in the therapeutic guidelines for managing this disease . 
standard treatment of sgns involves surgical resection with or without adjuvant radiation therapy . locoregional recurrence and metastases are common , at which time palliative chemotherapy is considered , but response rates are generally poor , and the duration of response is brief without a clear favorable impact on survival . 
given the aggressive nature of these tumors and the limited treatment options upon relapse and metastasis , there has been an increased interest in developing targeted therapies . two such targets , the ar and her2 / neu receptor tyrosine kinase , are currently used in clinical practice with variable results.7 a relatively large retrospective case series has reported favorable outcomes using androgen deprivation therapy in ar - positive sgns with good tolerability and an overall survival benet.8 the success of her2 / neu - directed therapy in breast cancer has resulted in multiple case reports that show benet from using trastuzumab - based regimens in treating sgns.4 , 9 despite initial success with targeted therapy , however , progression is inevitable . mechanisms of resistance have not been extensively explored . 
therefore , it seems reasonable to consider the use of ado - trastuzumab emtansine upon progression on trastuzumab , drawing on its demonstrated activity and clinical benet in the analogous clinical scenario in patients with advanced her2 / neu - positive breast cancer.10 by contrast to the previous reports , we describe one of the largest single - institution experiences with her2 / neutargeted therapy in patients with metastatic sgns . 
most of our patients ( n = 6 of 7 ) experienced progression after trastuzumab , which highlights the role of sequential her2 / neu therapy described by almquist et al.6 all of our patients tumors demonstrated her2 / neu overexpression , and most had a high degree of her2 / neu receptor positivity . in our retrospective case series , there was variability in the methods for her2 / neu testing that reect the natural evolution of institutional testing practices . 
nevertheless , clinical benet was seen regardless of the method of testing diagnosed with high - grade right parotid salivary carcinoma solitary liver metastasis retroperitoneal lymph node metastases progression of retroperitoneal lymph node metastases surgical resection with modied radical neck dissection left hepatic lobectomy cisplatin and rt bicalutamide and leuprolide carboplatin and paclitaxel ado - trastuzumab emtansine trastuzumab and pertuzumab maintenance time ( months ) fig 2 . 
 swed , cohen , and aggarwal ( ihc , uorescence in situ hybridization , or next - generation sequencing ) , conrming the role of a her2 / neu - targeted approach . 
for example , the patient discussed here initially experienced a complete metabolic and radiographic response and derived a sustained clinical benet with a progression - free survival of 29 months that is ongoing . progression - free survival in all of our patients ranged from 6 to 29 months , and overall survival ranged from 9 to 33 months . 
all of the patients experienced varying degrees of neuropathy , which proved to be dose - limiting in patient 2 . thrombocytopenia was another adverse effect of therapy , which led to interruption of therapy in one patient . 
cohen honoraria : bristol - myers squibb consulting or advisory role : heat biologics , takeda pharmaceuticals , cerulean pharma , kolltan pharmaceuticals , zymeworks , pzer research funding : heat biologics ( inst ) , macrogenics ( inst ) , merck ( inst ) , takeda pharmaceuticals ( inst ) , cleave biosciences ( inst ) , celldex ( inst ) travel , accommodations , expenses : heat biologics takeda pharmaceuticals , kolltan pharmaceuticals , cerulean pharma , zymeworks , bristol - myers squibb , pzer charu aggarwal consulting or advisory role : genentech , bristol - myers squibb , eli lilly , celgene , medimmune research funding : genentech ( inst ) , incyte ( inst ) , macrogenics ( inst ) , merck sharp & dohme ( inst ) , astrazeneca / medimmune ( inst ) no other potential conicts of interest were reported . references bradley pj : distant metastases from salivary glands cancer . 
otolaryngol head neck surg 154 : 1041 - 1046 , 2016 alotaibi am , alqarni ma , alnobi a , et al : human epidermal growth factor receptor 2 ( her2 / neu ) in salivary gland carcinomas : a review of literature . 
j clin diagn res 9 : ze04 - ze08 , 2015 limaye sa , posner mr , krane jf , et al : trastuzumab for the treatment of salivary duct carcinoma . 
oncologist 18 : 294 - 300 , 2013 girish s , gupta m , wang b , et al : clinical pharmacology of trastuzumab emtansine ( t - dm1 ) : an antibody - drug conjugate in development for the treatment of her2 - positive cancer . 
cancer chemother pharmacol 69 : 1229 - 1240 , 2012 almquist d , umakanthan jm , ganti ak : sequential her2 - targeted therapy in salivary ductal carcinoma with her2 / neu overexpression and a concomitant erbb2 mutation . 
head neck pathol 12 : 95 - 104 , 2018 boon e , van boxtel w , buter j , et al : androgen deprivation therapy for androgen receptor - positive advanced salivary duct carcinoma : a nationwide case series of 35 patients in the netherlands . 
head neck 40 : 605 - 613 , 2018 van boxtel w , boon e , weijs wlj , et al : combination of docetaxel , trastuzumab and pertuzumab or treatment with trastuzumab - emtansine for metastatic salivary duct carcinoma . 
baron jm , boster bl , barnett cm : ado - trastuzumab emtansine ( t - dm1 ) : a novel antibody - drug conjugate for the treatment of her2 - positive metastatic breast cancer . 
hyman , md1 , 2 purpose matching patients to investigational therapies requires new tools to support physician decision making . we designed and implemented precision insight support engine ( precise ) , an automated , just - in - time , clinical - grade informatics platform to identify and dynamically track patients on the basis of molecular and clinical criteria . 
median time from sequencing to enrollment was 163 days ( interquartile range , 66 to 357 days ) , and from precise identication to enrollment 87 days ( interquartile range , 37 to 180 days )  . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction genomic data are increasingly used to guide both routine and investigational treatment decisions for patients with cancer . 
simultaneously , clinically validated broad next - generation sequencing platforms that permit the detection of multiple potentially actionable alterations are now accessible at the point of care.1 , 2 these improvements , however , have not been accompanied by commensurate advancements in the systems that are available to help physicians interpret and act on these data . indeed , previous experience with patients with advanced solid tumor who undergo genome proling suggests that only a minority5% to 24% , depending on the breadth of sequencing and practice settingare subsequently enrolled in genome - matched trials.3 - 8 numerous challenges exist in identifying and enrolling patients in appropriate genome - driven clinical trials . clinicians must correctly interpret sequencing data not only at the time of the initial results , but also longitudinally , as our understanding of genomic biomarkers and associated clinical evidence continuously evolves.9 enrolling patients in trials also requires access to , and up - to - date knowledge of , a changing portfolio of studies , each with its own study - specic eligibility criteria and dynamic slot availability . 
finally , all of this information must be readily accessible to the clinician at critical decision points in a patients care . to address these challenges , multiple strategies have emerged to facilitate matching patients to genomedriven clinical trials ( appendix table a1 )  . 
 tao et al context key objective new strategies to facilitate matching patients to genome - driven trials are needed to support physician decision making . precision insight support engine ( precise ) is an automated , just - in - time , clinical - grade informatics platform that identies and dynamically tracks patients on the basis of molecular and clinical criteria . 
to our knowledge , this represents the rst effort to evaluate outcomes of a bioinformatics patienttrial matching platform . knowledge generated precise identied nearly one half ( 43% ) of all enrollment in early - phase , genome - driven studies across a wide variety of tumor types and molecular alterations , with a 5 - month median time from sequencing to enrollment . 
a major area for improving matching efcacy is better integration of nonstructured , clinical eligibility criteria . relevance use of automated bioinformatics platforms represents an important means by which to increase clinical trial accrual and deliver precision oncology care to patients . straightforward of these approaches involves directly annotating molecular sequencing reports at initial sign - out to indicate the clinical signicance of each alteration and list potentially suitable clinical trials . 
multiple initiatives are underway to harmonize the annotation of individual variants and incorporate multitiered levels of evidence for actionability.10 - 12 some commercial laboratories and academic institutions have created on - demand molecular tumor boards that review molecular sequencing reports to make treatment recommendations and manually curate existing clinical trials for alterations of interest.13 all of these approaches have potential limitations . 
similarly , molecular tumor boards are time consuming , difcult to scale , and potentially inuenced by participants knowledge base and anecdotal experience . in response to these limitations and to address the ongoing unmet need of matching patients to clinical trials at our center , we created precision insight support engine ( precise ) , an automated , just - in - time , clinical - grade informatics platform to identify and dynamically track patients on the basis of molecular and clinical criteria . precise was designed to empower clinical investigators to proactively identify and recruit optimal candidates to their genome - driven trials . 
initially , limited proling data were generated via a mass spectrometrybased hotspot assay covering eight genes ( massarray ; sequenom , san diego , ca ) or an amplicon - based next - generation sequencing test covering 48 genes ( truseq amplicon cancer panel ; illumina , san diego , ca ) .14 a customized hybrid capture - based next - generation sequencing assay ( mskimpact ) was later performed per previously published methods.15 msk - impact can identify all classes of genomic alterationssingle - nucleotide variants , indels , copy number alterations , and select structural rearrangementsin up to 468 genes , depending on the assay version . 
these data are used for clinical report sign - out and delivery to the data warehouse that precise uses for patient identication.16 , 17 sequenced patients had cancer types for which proling was considered routine at the time performed or underwent clinical testing under a prospective institutional review boardapproved protocol that was designed to evaluate the utility of proling in these cancer types ( clinicaltrials.gov identier : nct01775072 )  . precise platform the precise platform was available to any principal investigator of an irb - approved therapeutic study that included molecular eligibility criteria . 
 outcomes of a physician support system for genome - driven oncology the functionality of the precise platform evolved during the study period on the basis of user feedback ( fig 1 )  . 
beginning in 2014 , precise was enhanced to offer notications , customized per study , of potentially clinically important events that could prompt a treatment change , such as upcoming appointments or restaging scans . 
for most of the study duration , precise notications were provided directly to the research team , which empowered them to further screen potential patients for appropriateness and notify treating physicians accordingly . 
use of this direct - to - primary oncologist notication function was at the discretion of the research teaall notications to the research team and the primary oncologist were generated as emails and did not directly integrate with the electronic medical record . cohort eligibility , data collection , and statistical analysis all precise cohorts for early - phase studiespilot , phase i , and phase i and iithat included at least one genomic eligibility criterion and that were created after april 16 , 2014 , were included for analysis . 
an internally developed mpath application was used to obtain the date that sequencing data was signed out and entered into the medical record for each patient , as well as the specic qualifying genomic alteration present . the msk institutional review board evaluated and approved a retrospective research protocol to evaluate precise platform outcomes . 
primary outcome measure was to determine what proportion of patients who were enrolled in the evaluated genome - driven studies was facilitated by precise . for the purpose of this analysis , enrollment was considered to be facilitated if precise identied the patient as eligible and generated a notication to either the research team or the primary oncologist before the enrollment date . 
to identify areas for future precise functionality enhancement , reasons for the failure of precise identify eligible patients before study enrollment were also explored through manual record review . in the relevant results study characteristics a total of 41 therapeutic trials used precise for genomic matching during the study period ( table 1 )  . 
the initial iteration ( version 1 ) of precise involved generating cohorts on the basis of complex genetic and clinical criteria dened by the studys principal investigator ( pi ) , which could then be sent to the pi at dened intervals . 
the capability of precise was later enhanced ( version 2 ) to enable pi notications triggered by certain events of interest , such as an upcoming patient appointment or computed tomography scan . 
present day ( version 3 ) precise can also incorporate a patients prior treatment history and allows for direct notication of the patients treating oncologist that a patient may be eligible for a study , often prompting an exchange between the treating oncologist and pi that initiates the patients future enrollment . 
of investigational agents antibody ( nonimmunotherapy ) therapeutic class * small molecule immunotherapy tumor type eligibility multiple breast lung ( nonsmall cell ) lymphoma mesothelioma glioma sarcoma prostate thoracic breast 5 - 10 10 - 15  . 
eight of 41 trials used the direct - to - oncologist notication system . principal investigator characteristics the 41 therapeutic trials were led by 19 unique principal investigators ( pis ) who individually led between one and ve studies ( table 1 )  . 
median time since the completion of terminal subspecialty training for pis was 7 years ( range , 2 to 27 years )  . patient matching during the study period , a total of 755 patients who were treated primarily by 150 unique oncologists were enrolled in 41 trials . 
precise prospectively identied 43% ( 327 of 755 ) of cases before patient enrollment , successfully notifying study investigators and / or the primary oncologist of the potential match ( fig 2 )  . 
reecting eligibility criteria among the trials , breast cancer ( 76 [ 23% ] of 327 ) and lung cancer ( 55 [ 17% ] of 327 ) were the most common tumor types among enrolled patients identied by precise . 
accounting for patients with more than one eligible molecular alteration , erbb2 ( 71 [ 21% ] of 335 ) was the most common genomic alteration , followed by pik3ca ( 47 [ 14% ] of 335 )  . at the individual protocol level , the percent of patients identied by precise before enrollment ranged from 0% to 100% . 
patients in whom the genomic alteration that ultimately led to enrollment did not meet the pre - established precise molecular criteria , as dened by the investigator , accounted for 33% ( 140 of 428 ) of missed cases . 
a lack of internal sequencing at the time of accrual accounted for 30% ( 127 of 428 ) of missed cases , predominantly among patients who enrolled on the basis of genomic proling that was performed outside the institution and was therefore not available for parsing by precise . 
another 23% ( 100 of 428 ) of cases was missed because precise cohort criteria that would have included the patient were amended only after the time of patient enrollment . 
several other technical and clinical reasons accounted for the remaining 14% ( 61 of 428 ) of cases , the majority of which ( 50 of 61 ) consisted of patients who did not meet clinical criteria available for * the total adds up to more than 41 as studies may include more than one agent class . twelve principal investigators had dual afliations with a diseasespecic group and the phase i group . one half ( 22 [ 54% ] of 41 ) of studies were phase i , and 61% ( 25 of 41 ) included multiple tumor types . 
of diseasespecic studies , the most common tumor types included breast cancer ( ve [ 12% ] of 41 ) and nonsmall - cell lung cancer ( four [ 10% ] of 41 )  . 
 ( b ) each column depicts patient enrollments by study principal investigator , with patient enrollment facilitated by precise shaded in blue and patient enrollment not facilitated by precise shaded in red . 
 ( c ) each column represents a unique study , with the absolute number of patients in each category labeled above ( non - precise ) and below ( precise enrollment ) each column . capture by precise , such as presence of triple - negative breast cancer , which was not always readily documented in the medical record . to further understand how physicians and patients use tumor genomic data to guide investigational treatment decisions , we evaluated the timing of enrollment relative to two important milestones : the completion of sequencing and the initial precise identication . 
upon evaluation of the 327 patients who were identied by precise and successfully enrolled in a genome - driven study , there was signicant variability in time intervals between these three events at the individual patient level . 
median time from sequencing to therapeutic enrollment was 163 days ( interquartile range , 66 to 357 days ; range , 5 to 1 , 281 days ) and from precise identication to enrollment 87 days ( interquartile range , 37 to 180 days ; range , 1 to 850 days ; fig 3 )  . 
reasons for delay from sequencing and precise identication to study enrollment included the availability of alternative routine therapy or a lack of need for treatment among patients without evidence of active disease . causes of patient attrition before enrollment to better understand the reasons why patients who were identied by precise did not subsequently enroll in the relevant therapeutic study , a representative cohort involving a multitumor phase i and ii expansion study of a targeted small molecule was selected for manual record review . 
of these 98 patients , 22 were immediately determined to be permanently ineligible or excluded as a result of a static characteristic that rendered the patient ineligible for the trial indenitely . 
these included having a second primary cancer ( n = 6 ) , a nonqualifying malignancy ( n = 6 ) , being deceased but not listed as such in the medical record ( n = 5 ) , and other reasons ( n = 5 )  . 
another 45% ( 10 of 22 ) involved a data element that was sometimes availablesecond primary cancer , prohibited prior therapy , and hiv / aidsfor use but not under all circumstances . 
for example , exclusions on the basis of prior therapy will miss agents administered at other medical centers or some oral anticancer agents , especially if dispensed by third - party pharmacies . after permanent exclusions , 76 potentially eligible patients remained . 
upon manual review , 78% ( 59 of 76 ) of patients did not immediately qualify for treatment at the time of the initial precise identication on the basis of not requiring active therapy ( n = 44 ) or ongoing response to current therapy ( n = 15 )  . 
collectively , 84% ( 59 of 70 ) of these temporary exclusion criteria are not consistently available for use by precise , primarily because the current disease status of the patient is not captured as a structured data element in the medical record . 
 a 2 , 000 1 , 500 1 , 000 500 1 , 000 1 , 500 outcomes of a physician support system for genome - driven oncology 1 , 400 1 , 200 1 , 000 sequencing to enrollment identification to enrollment patient sequencing identified by precise enrollment fig 3 . 
each series of three dots on a single vertical axis represents a single patients course , from initial sequencing ( blue dot ) to identication by precise ( precision insight support engine ; red dot ) to enrollment in the study ( gray dot )  . 
 ( b ) box and whisker plot showing the interval of time from sequencing to enrollment in the study ( left ; median , 163 days ) and from identication by precise to enrollment in the study ( right ; median , 87 days )  . therapies , rapidly deteriorating , or deemed inappropriate because of other issues , such as prior nonadherence . 
reasons for permanent or temporary exclusion from study qualication are depicted in blue ( criteria that is available for use by precise ) , red ( criteria that is sometimes available and could potentially be captured as an extractible structured data element ) , or teal ( criteria that is not yet available for use by precise )  . 
to our knowledge , this report represents the rst effort to evaluate real - world outcomes of an automated , just - in - time , clinicalgrade informatics platform to facilitate patient matching . we also discovered that a signicant time interval often elapses between the initial generation of tumor genomic data and subsequent enrollment in a matched study . specically , among those who ultimately accrue to a matched study , median duration from data generation to enrollment was 5 months , with some outliers enrolling up to 42 months later . 
these data emphasize the importance of supporting physician decision making longitudinally through a patients entire treatment . although these pilot data are encouraging , our analysis also identied areas of ongoing challenge for such matching systems as precise . 
of importance , nearly three quarters of initially identied patients were not immediately eligible on the basis of clinical factors that were not readily available for use by precise , most commonly related to challenges in algorithmically dening patient disease status . 
the result is that precise had a high false - positive rate that may ultimately limit the utility of this system for some indications , particularly for recruiting patients with more prevalent genomic alterations . 
indeed , a previous analysis of overall match rates at our institution that was conducted during roughly the same time period found a match rate of only 11% , despite 37% of patients harboring a potentially actionable alteration.5 taken together , these data demonstrate that even with the use of a sophisticated decision support system , there is an ongoing need for additional improvement in the methodologies to match patients to clinical trials on the basis of tumor genomic and clinical information . 
this requires developing agreed - upon standards , including discrete , structured criteria , for extracting clinical data from the electronic medical record . in the future , leveraging natural language processing and information extraction technologies may also enhance the ability to accurately capture unstructured data . this analysis has some important limitations . 
foremost , we considered any patient about whom precise successfully notied the pi or treating physician of potential eligibility before enrollment as an accrual that was potentially facilitated by the systehowever , we cannot determine exactly how many of these enrollments might have occurred without the use of this systeindeed , our study was retrospective in design and we cannot denitively make conclusions on the incremental value of precise . 
moreover , this analysis represents real - world use of precise by each pi , who were responsible for setting his or her own cohort criteria and using the results as he or she felt best complimented the practice . 
additional evaluation is needed to determine how the utility of this system is affected by recent features , such as full automation of direct - to - treating physician alerts triggered by critical events , like scans that show progression or rising tumor markers . precise is not the only system designed to address the emerging need of matching patients to relevant clinical trials on the basis of the patients genomic prole . 
several other centers have developed strategies by which to achieve this goal that range from on - site or virtual molecular tumor boards to automated matching platforms13 , 18 - 23 ( appendix table a1 )  . 
potential advantages of an automated informatics approach include scalability and the ability to track patients longitudinally and respond to changing molecular and clinical data . in summary , this pilot study of real - world use of precise to guide enrollment in genome - driven studies suggests that this type of real - time decision support system can meaningfully facilitate patient enrollment . 
harding consulting or advisory role : bristol - myers squibb , cytomx therapeutics , eli lilly , eisai research funding : bristol - myers squibb ( inst ) , pzer ( inst ) , eli lilly ( inst ) , novartis ( inst ) , incyte ( inst ) , calithera biosciences ( inst ) , polaris ( inst ) lillian m . 
smyth honoraria : astrazeneca , pzer consulting or advisory role : astrazeneca , genentech research funding : astrazeneca ( inst ) , genentech ( inst ) , puma biotechnology ( inst ) travel , accommodations , expenses : pzer , genentech , puma biotechnology research funding : novartis ( inst ) , genentech ( inst ) , debio pharmaceuticals ( inst ) , adc therapeutics ( inst ) , pzer ( inst ) , novita pharmaceuticals ( inst ) , clovis oncology ( inst ) , eli lilly ( inst ) , zymeworks ( inst ) travel , accommodations , expenses : taiho pharmaceutical , jounce therapeutics , pzer , astrazeneca other relationship : novartis , pzer , taiho pharmaceutical , jounce therapeutics alexander drilon honoraria : medscape , onclive , peervoice , physicians education resources , targeted oncology , more health , research to practice , foundation medicine , peerview consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pzer , blueprint medicines , genentech , helsinn therapeutics , beigene , hengrui therapeutics , exelixis , bayer , tyra biosciences , verastem , takeda , ariad pharmaceuticals , millennium pharmaceuticals , bergenbio , more health , eli lilly research funding : foundation medicine patents , royalties , other intellectual property : wolters kluwer ( royalties for pocket oncology ) other relationship : merck , glaxosmithkline , teva pharmaceuticals , taiho pharmaceutical , pzer , pharmamar , puma biotechnology marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / astrazeneca tagrisso rfp advisory committee , takeda , bristol - myers squibb , bayer , merck ( i ) research funding : loxo ( inst ) , helsinn therapeutics david b . 
solit stock and other ownership interests : loxo consulting or advisory role : pzer , loxo , illumina , intezyne technologies , vivideon therapeutics travel , accommodations , expenses : merck michael f . 
jhaveri consulting or advisory role : novartis , pzer , spectrum pharmaceuticals , astrazeneca , taiho pharmaceutical , jounce therapeutics , adc therapeutics , synthon , intellisphere , bristol - myers squibb acknowledgment the authors thank alisa pinkhasik for assistance with study data . 
for providing inspiration for this report . references 33 : 2753 - 2762 , 2015 schram am , berger mf , hyman dm : precision oncology : charting a path forward to broader deployment of genomic proling . 
plos med 14 : e1002242 , 2017 cheng ml , berger mf , hyman dm , et al : clinical tumour sequencing for precision oncology : time for a universal strategy . 
nat rev cancer 18 : 527 - 528 , 2018 jordan ej , kim hr , arcila me , et al : prospective comprehensive molecular characterization of lung adenocarcinomas for efcient patient matching to approved and emerging therapies . 
j clin oncol zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
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mantripragada kc , olszewski aj , schumacher a , et al : clinical trial accrual targeting genomic alterations after next - generation sequencing at a non - national cancer institute - designated cancer prograj oncol pract 12 : e396 - e404 , 2016 8 . 
massard c , michiels s , fert e c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . cancer discov 7 : 586 - 595 , 2017 schram am , reales d , galle j , et al : oncologist use and perception of large panel next - generation tumor sequencing . 
taylor ad , micheel cm , anderson ia , et al : the path ( way ) less traveled : a pathway - oriented approach to providing information about precision cancer medicine on my cancer genome . 
mateo j , chakravarty d , dienstmann r , et al : a framework to rank genomic alterations as targets for cancer precision medicine : the esmo scale for clinical actionability of molecular targets ( escat )  . 
ann oncol 29 : 1895 - 1902 , 2018 johnson a , zeng j , bailey am , et al : the right drugs at the right time for the right patient : the md anderson precision oncology decision support platfordrug discov today 20 : 1433 - 1438 , 2015 14 . 
rekhtman n , paik pk , arcila me , et al : clarifying the spectrum of driver oncogene mutations in biomarker - veried squamous carcinoma of lung : lack of egfr / kras and presence of pik3ca / akt1 mutations . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
lindsay j , fitz cdv , zwiesler z , et al : matchminer : an open source computational platform for real - time matching of cancer patients to precision medicine clinical trials using genomic and clinical criteria . 
tao j , eubank mh , pamer e , et al : precise : a clinical - grade automated molecular eligibility screening and just - in - time ( jit ) physician decision support solution for molecularly - selected oncology trials . 
notications are generated from scheduled queries and use an open - source java e - mail package implemented as a database user - dened function to send emails from the sql statement . 
a web application using open - source javascript libraries allows system administrators to capture cohort logic and settings and provides end users the ability to annotate patient status for their study . 
 ( a ) each column depicts patient enrollments by study pi , with pis with the most years in practice on the left and the fewest years in practice on the right . 
 ntrk alterations in pediatric highrisk malignancies identied through european clinical sequencing programs constitute promising drug targets over the last 2 years , two neurotrophic - tropomyosin receptor tyrosine kinase ( ntrk ) inhibitors have been approved for a tissue - agnostic indication in adults and children , namely , larotrectinib and entrectinib both in the united states and europe . 
although ntrkfusionpositive malignancies are rare , patients with tumors harboring this alteration may greatly benet from those innovative targeted therapies . molecular characterization platforms have been set up in europe over the last 5 years to identify targetable alterations in tumors of individual pediatric patients and to guide therapeutic prioritization . 
mappyacts , coordinated in france ( molecular proling for pediatric and young adult cancer treatment stratication ; clinicaltrials.gov identier : nct02613962 ) , and in ( individualized form , coordinated in germany therapy for relapsed malignancies in childhood ; eudract number : 2018 - 000127 - 14 ) , are the largest european efforts , offering real - time clinical sequencing to relapsed or refractory or very high - risk pediatric patients from 13 european countries.1 - 3 they are part of the innovative therapies for children with cancer ( itcc ) precision medicine and new drug development program , matching patients tumor molecular proles to new drugs in early clinical trials . alterations of the ntrk 1 - 3 were recently investigated in approximately 3 , 500 pediatric tumor samples across tumor types , with fusions involving these genes being detected in 0.34% of samples and amplication , mutation , and mrna overexpression occurring less frequently.4 although ntrk fusions are druggable by selective ( eg , larotrectinib and entrectinib ) and less specic small molecules , 4 - 11 reports on response of nonfusion ntrk alterations to ntrk inhibitors ( ntrki ) are lacking to date.4 since its initiation in january 2016 until july 2020 , approximately 690 patients with relapsed , refractory , or very high - risk pediatric cancer have been screened through mappyacts , whereas approximately 1 , 100 patients were screened through the inform registry from february 2015 until july 2020 . 
apart in mappyacts patients inform who were included because of being very high risk at rst diagnosis , all other tumor samples were obtained at relapse or progression ( table 1 )  . ntrk fusions were the most frequent alterations ( n = 25 ) , with ntrk1 , 2 , 3 being involved in 9 / 25 , 8 / 25 , and 8 / 25 patients , respectively . 
even for previously not described fusions , the similar structure to known ntrk fusions , with conservation of the tyrosine kinase domain , supports the hypothesis of an activation of the tyrosine kinase domain of ntrk . single nucleotide variants ( snvs ) were detected in 14 tumors ( 3 ntrk1 , 7 ntrk2 , and 4 ntrk3 ) , with six snvs being located in the kinase domain of the respective protein , one snv each in the immunoglobulin i - set domain and the leucine - rich domain , respectively , and the remaining six snvs falling outside of annotated functional domains . two cases harbored a focal amplication of ntrk1 genomic locus . a total of 17 patients with tumors harboring an ntrk fusion were treated with the specic ntrki larotrectinib . 
of these , four patients from germany , four patients from sweden , four patients from france , and one patient from poland were enrolled in an early phase clinical trial . 
complete resection of the tumor , stabilization with conventional therapy , missing availability of the drug ( before the initiation of pediatric trials ) , and loss to follow - up were stated as reasons not to treat with ntrki . 
one patient with ntrk1 amplication as nonfusion ntrk alteration received larotrectinib in a clinical trial setting . through this pan - european initiative , we demonstrate the feasibility and value of next - generation sequencing to identify children and adolescents with an ntrk tumor alteration - harboring malignancy ( across all types ) who may be eligible for ntrki therapy . addition , it allows the capture of all potential ntrk fusion partners and novel snvs in functionally relevant domains of ntrk . 
the current development of additional pediatric sequencing programs ( ie , smpaeds in the united kingdom , ither in the netherlands , and the danish program ) as part of the itcc strategy will provide an expanded access to targeted agents for children and adolescents across europe . elke pfaff , md hopp childrens cancer center heidelberg ( kitz ) , heidelberg , germany ; pediatric glioma research group , german cancer research center ( dkfz ) , heidelberg , germany ; department of pediatric oncology , hematology and immunology , heidelberg university hospital , heidelberg , germany tiphaine adam de beaumais , md clinical research department , gustave roussy cancer center , villejuif , france antonin marchais , phd bioinformatics and inserm u1015 , gustave roussy cancer center , university paris - saclay , villejuif , france cornelis m . 
van tilburg , md hopp childrens cancer center heidelberg ( kitz ) , heidelberg , germany ; department of pediatric oncology , hematology and immunology , heidelberg university hospital , heidelberg , germany ; clinical cooperation unit pediatric oncology , german cancer research center ( dkfz ) , heidelberg , germany german cancer consortium ( dktk ) , germany ; kitz clinical trial unit , hopp childrens cancer center heidelberg ( kitz ) , german cancer research center ( dkfz ) and heidelberg university hospital , heidelberg , germany mirjam blattner - johnson , phd hopp childrens cancer center heidelberg ( kitz ) , heidelberg , germany ; pediatric glioma research group , german cancer research center ( dkfz ) , heidelberg , germany uta dirksen , md german cancer consortium ( dktk ) , partner essen , germany ; university hospital essen , pediatrics iii , hematology and oncology , west german cancer centre , essen , germany ingrid ra , md , phd department of pediatric oncology and hematology , karolinska university hospital , solna , sweden ; skane university hospital , lund , sweden birgit geoerger , md , phd department of pediatric and adolescent oncology , gustave roussy cancer center , inserm u1015 , university parissaclay , villejuif , france gudrun schleiermacher , md equipe siric rtop recherche translationelle en oncologie p ediatrique , institut curie , paris , france ; siredo : care , innovation and research for children , adolescents and young adults with cancer , institut curie , paris , france stefan m . 
 correspondence hematology and immunology , heidelberg university hospital , heidelberg , germany ; division of pediatric neurooncology , german cancer consortium ( dktk ) and german cancer research center ( dkfz ) , heidelberg , germany data analysis and interpretation : elke pfaff , antonin marchais , ingrid ra , birgit geoerger , gudrun schleiermacher , stefan m . 
the inform project is nancially supported by the german consortium for translational cancer research ( dktk ) , german cancer aid , the german childhood cancer foundation , the german cancer research center ( dkfz ) , bild e.v. 
pster provision of study materials or patients : elke pfaff , uta dirksen , ingrid ra , birgit geoerger , olaf witt collection and assembly of data : elke pfaff , tiphaine adam de beaumais , antonin marchais , cornelis m . 
van tilburg consulting or advisory role : novartis , bayer uta dirksen consulting or advisory role : lilly , ipsen ingrid ra consulting or advisory role : bayer birgit geoerger consulting or advisory role : roche or genentech , merck kgaa , boehringer ingelheim , bayer , azd , novartis gudrun schleiermacher honoraria : bristol - myers squibb research funding : bristol - myers squibb , pzer , msdavenir , roche travel , accommodations , expenses : roche stefan m . 
pster research funding : lilly , bayer , roche , pharmamar , pzer patents , royalties , other intellectual property : patent on utilizing dna methylation proling for tumor classication olaf witt consulting or advisory role : novartis , astrazeneca , janssen research & development , bristol - myers squibb , roche , bayer , dayonetx research funding : biomed valley discoveries david t.w. 
worst bc , van tilburg cm , balasubramanian gp , et al : next - generation personalised medicine for high - risk paediatric cancer patients : the inform pilot study . 
harttrampf ac , lacroix l , deloger m , et al : molecular screening for cancer treatment optimization ( moscato - 01 ) in pediatric patients : a singleinstitutional prospective molecular stratication trial . 
 correspondence berlanga p , pierron g , lacroix l , et al : can pediatric and adolescent patients with recurrent tumors benet from a precision medicine program ? the european mappyacts experience . 
j clin oncol 37 , 2019 ( suppl ; abstr 10018 ) okamura r , boichard a , kato s , et al : analysis of ntrk alterations in pan - cancer adult and pediatric malignancies : implications for ntrk - targeted therapeutics . 
cancer discov 7 : 400 - 409 , 2017 laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
lancet oncol 19 : 705 - 714 , 2018 konicek bw , capen ar , credille km , et al : merestinib ( ly2801653 ) inhibits neurotrophic receptor kinase ( ntrk ) and suppresses growth of ntrk fusion bearing tumors . 
oncotarget 9 : 13796 - 13806 , 2018 van tilburg cm , dubois sg , albert cm , et al : larotrectinib efcacy and safety in pediatric trk fusion cancer patients . 
j clin oncol 37 , 2019 ( suppl ; abstr 10010 ) robinson gw , gajjar aj , gauvain km , et al : phase 1 / 1b trial to assess the activity of entrectinib in children and adolescents with recurrent or refractory solid tumors including central nervous system ( cns ) tumors . 
hong ds , dubois sg , kummar s , et al : larotrectinib in patients with trkfusionpositive solid tumours : a pooled analysis of three phase 1 / 2 clinical trials . 
steensma , md6 ; amy dezern , md7 ; gail roboz , md8 ; guillermo garcia - manero , md9 ; harry erba , md , phd10 ; benjamin l . 
maciejewski , md , phd1 purpose we developed an unbiased framework to study the association of several mutations in predicting resistance to hypomethylating agents ( hmas ) in patients with myelodysplastic syndromes ( mds ) , analogous to consumer and commercial recommender systems in which customers who bought products a and b are likely to buy c : patients who have a mutation in gene a and gene b are likely to respond or not respond to hmas . methods we screened a cohort of 433 patients with mds who received hmas for the presence of common myeloid mutations in 29 genes that were obtained before the patients started therapy . 
the association between mutations and response was evaluated by the apriori market basket analysis algorithrules with the highest condence ( condence that the association exists ) and the highest lift ( strength of the association ) were chosen . we validated our biomarkers in samples from patients enrolled in the s1117 trial . results among 433 patients , 193 ( 45% ) received azacitidine , 176 ( 40% ) received decitabine , and 64 ( 15% ) received hma alone or in combination . 
the median number of mutations per sample was three ( range , zero to nine ) , and 176 patients ( 41% ) had three or more mutations per sample . 
these molecular signatures were present in 30% of patients with three or more mutations / sample with an accuracy rate of 87% in the training cohort and 93% in the validation cohort . conclusion genomic biomarkers can identify , with high accuracy , approximately one third of patients with mds who will not respond to hmas . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the hypomethylating agents azacitidine ( aza ) and decitabine ( dac ) have been approved by the food and drug administration and the european medicine agency for patients with myelodysplastic syndromes ( mds ) .1 - 4 although treatment with these agents is well tolerated , only 30% to 40% of patients will respond to therapy , with the majority achieving hematologic improvement in blood counts and only a minority ( 10% to 15% ) achieving a complete response , the response criterion most reliably associated with improvement in overall survival ( os ) .1 - 4 more importantly , it may take up to six cycles of treatment for patients to achieve their best response.5 given the limited number of patients who benet from these agents and the long administration of identifying biotheir treatment , markers that can predict resistance is essential , because it can prevent prolonged exposure to ineffective therapy and unnecessary toxicities and treatment costs can be avoided . because clinical variables and patient characteristics have not consistently predicted response to hypomethylating agents ( hmas ) , molecular data represent a biologic opportunity6 - 8 to enhance patient response rates and outcomes . 
because identifying a single gene or comutated genes is unlikely to yield an understanding of how these mutations dene disease biology or phenotype , an unbiased approach is needed to study the relationship of these abnormalities to each other and to mds biology . in this study , we used unbiased , machine learning approaches ( a recommender system similar to that used by netix or amazon.com ) to assess the impact of molecular data on resistance to hmas in a large cohort of patients treated with hmas at different academic institutions , and we validated our results in a population treated in a contemporary prospective clinical trial of hma therapy15 of aza alone and in combination . methods patients for the training cohort , patients treated with either azaor dac - based regimens were included in this study : 230 patients were treated at cleveland clinic ( between 2002 and 2012 ) ; 203 were from other academic institutions ( dana - farber cancer institute [ 2003 to 2010 , n = 42 ] and md anderson cancer center [ 2003 to 2010 , n = 103 ] ) or were part of the daco - 020 clinical trial ( adopt [ 2005 to 2006 , n = 58 ] ) .11 all patients consented to blood or bone marrow samples at each institution under institutional review boardapproved protocols in accordance with each institution policy and the declaration of helsinki . 
more information regarding the patient cohort , response criteria , and validation cohort is included in the data supplement . dna sequencing and mutational analysis a panel of 29 genes that are commonly mutated in mds and myeloid malignancies was evaluated ( data supplement )  . 
more information regarding sequencing method is included in the data supplement . statistical analyses test variables were compared using the wilcoxon rank sum test and fishers exact for continuous and categorical variables , respectively . 
os was calculated from the date of diagnosis to the date of last follow - up or death ( whichever came rst ) , and survival curves were constructed using the kaplan - meier method and compared using the log - rank test . 
mutation distribution among responders versus nonresponders total responders non - responders nazha et al mutations asxl1 tet2 srsf2 runx1 dnmt3a sf3b1 tp53 u2af1 bcor ezh2 nras idh2 phf6 npm1 jak2 zrsr2 etv6 prpf8 idh1 prpn11 suz12 kras gata2 cebpa received dac ( 176 [ 86% ] alone and 29 [ 14% ] in combination with other agents )  . 
cytogenetic analyses per international prognostic scoring system ( ipss ) revised ( r ) criteria16 included 234 patients ( 54% ) with very good or good risk , 66 ( 15% ) with intermediate risk , 33 ( 8% ) with poor risk , 66 ( 15% ) with very poor risk , and 34 ( 8% ) not documented ( table 1 )  . 
the frequency of these mutations in our patient cohort was similar to those identied in other mds cohorts , with the exception of asxl1 , which was slightly higher because it was overrepresented in one cohort11 ( 203 patients from other academic institutions )  . 
patterns of mutation association were also similar to those in previous reports ( fig 1 )  . asxl1 mutations were commonly commutated with tet2 in 42 patients ( 10% ) , and with srsf2 38 ( 9% ) , runx1 35 ( 8% ) , u2af1 24 ( 6% ) , and dnmt3a 21 ( 5% ; fig 1 )  . overall , 367 patients ( 85% ) in the training cohort had a mutation in at least one gene . 
the graph is separated to show the spectrum of mutations in responders compared with nonresponders . ( 4% ) partial remission ( pr ) , 59 ( 14% ) hematologic improvement ( hi ) , 142 ( 33% ) stable disease , and 107 ( 24% ) progressive disease . in general , clinical characteristics such as age , cytopenias , and treatment regimens did not affect response , with the exception of the median blast percentage in the bone marrow , which was higher among responders compared with nonresponders ( 9% v 2% , p = .02 ; table 1 )  . 
risk stratications per ipss and ipss - r did not affect the overall response rate ( table 1 )  . idh1 and ezh2 , no single gene mutation was signicantly associated with response and resistance to hmas in univariate analyses , with the exception of respectively ( table 2 )  . 
the number of mutations per sample also did not affect response , with patients with three or more mutations having similar response rates to those with fewer than three mutations ( table 1 )  . 
genomic biomarkers dened by the recommender system association rules for resistance to hmas asxl1 , nf1 asxl1 , ezh2 , tet2 asxl1 , ezh2 , runx1 ezh2 , srsf2 , tet2 asxl1 , ezh2 , srsf2 asxl1 , runx1 , srsf2 asxl1 , tet2 , srsf2 asxl1 , bcor , runx1 the impact of mutations on response was assessed after controlling for clinical variables such as age and ipss - r scoring system , using logistic regression analyses . 
no mutation was associated with overall resistance or response to hmas , even after adjustment for clinical variables ( age , ipss - r , and sex ; data supplement )  . recommender system genomic biomarkers that predict response to build strong association rules ( associations between genes and outcomes [ response v no response ] ) , we used strict criteria to identify rules with the highest support ( how many times the rules appeared in the data set ) , high condence ( the condence of the algorithm in the association rule was set at 95% ) , and higher lift ( a measure that is reected in the strength of the association : the higher the lift is , the stronger is the association ) in the training cohort . 
when the rules were applied to our patient cohort , they predicted resistance to hmas correctly in 46 of 53 patients ( 87% ) with relevant molecular mutations . among the 105 patients with lower - risk disease by ipss - r ( low and very low risk groups ) , 62 ( 59% ) did respond to hmas . 
the difference in the presence of the biomarkers in lowerversus higher - risk mds is related to the higher percentage of patients with three or more mutations / sample in the higher - risk ( 42% ) versus the lower - risk ( 30% ) group . association with overall survival survival data were available for 375 patients from the training cohort . 
genomic biomarkers of resistance to aza were present in 14 of 39 samples ( 35% ) with three or more mutations ; 13 of 14 of these patients ( 93% ) did not respond to therapy . discussion predicting response or resistance to our currently available standard hma therapy in mds remains a signicant clinical challenge . 
identifying patients up front who may not respond to hmas can potentially improve outcome , decrease unnecessary adverse effects , and save money , especially when current recommendations are for a minimum of 6 months of treatment before deeming it a failure . 
although it is tempting to identify an isolated molecular abnormality or a pair of mutations that can predict hma resistance , this approach does not allow for the complexity and evolution of the genomic landscape in mds . in this study , we developed an unbiased framework using a machine learning , recommender system algorithm to identify highly sensitive genomic associations ( molecular signatures or genomic biomarkers ) that can predict resistance to hmas with high accuracy . 
these associations were validated in an independent cohort in samples from patients enrolled in a randomized phase ii / iii clinical trial . although our biomarkers were identied in only 25% of patients , their presence predicted resistance in almost all patients who had these mutations . 
by denition , a biomarker can be present in a small subset of patients , but when present can predict , with high accuracy and reliability , response or resistance to a therapy . 
detecting these biomarkers in 29% of patients suggests that other biologic mechanisms ( eg , changes in gene expression or epigenetic changes ) or clinical characteristics may contribute more to hma response and failure than does genomics . 
our ndings conrm that genomic associations may lead to different gene expressions and / or epigenetic changes that contribute to the response or resistance and thus , identifying one or two genes that can predict response may not be sufcient to build reliable and predictable models . although we included patients who received hmas in combination with other investigational agents , these combinations did not affect the response or resistance rate or os ; thus , their impact on the output of our recommender system algorithms is negligible . 
furthermore , neither ipss nor ipss - r predicted response or resistance to hmas in our study in accordance with prior reports.1 , 15 prior studies have attempted to use genomic data to predict response or resistance to hmas . 
for example , some studies have shown that tp53 mutations may predict response to hmas , whereas others did not conrm that nding.13 , 17 in a small study of 84 patients with acute myeloid leukemia ( aml ) and mds treated with a 10 - day dac course , a small subset of patients with tp53 mutations had a higher response rate to dac compared with tp53 wild - type patients . furthermore , the median os for tp53 mutated patients who received dac and underwent an allogeneic stem - cell transplantation was similar to that of patients with wild - type tp5317 . 
contrary to this nding , in a study of 71 patients with aml , there was no difference in overall response rate and survival among patients who received 5 days of dac compared with those who had a 10 - day schedule . 
 genomic biomarkers for resistance in mds with variant allele frequency greater than 10% may predict response to hmas , especially in patients with wild - type asxl1 mutations , but this nding was not validated in our study.11 the discrepancy in the results of these studies could be related to sample size , the number of genes tested , and the statistical approach that was used to analyze the data . 
it is also possible that genomic changes in themselves are not the drivers of response to hmas but rather , changes in the gene expression and methylation prole that are derived from the combination of these mutations . 
in a study of whole - genome sequencing , rna sequencing , and methylation prole of samples from patients with chronic myelomonocytic leukemia , a serial sequencing demonstrates that the response to hypomethylating agents is associated with changes in dna methylation and gene expression , without any decrease in the mutation allele burden or prevention of new genetic alteration occurrence.18 if eligible , directly , without this study includes several areas of innovation . 
for example , if a patient with mds with higher - risk disease carries one of these biomarkers , he or she should be encouraged to enroll in a clinical trial with a novel therapy or to proceed with an allogeneic stem - cell transplantation , the use of hmas , because the response to such therapy is predicted to be low . 
although all patients with mds should be encouraged to enroll in a clinical trial with novel therapies , having biomarkers that accurately predict resistance may ease the conversation with some patients who are hesitant to try newer approaches and prefer food and drug administrationapproved therapies.19 alternatively , patients with higher - risk disease and a high blast percentage may consider intensive , aml - type chemotherapy before allogeneic stem - cell transplantation , as opposed to an hma that is predicted to do little to affect the disease in the absence of other biomarkers that could predict resistance to chemotherapy , such as complex karyotype cytogenetics , and the presence of tp53 mutations and the absence of targetable mutations such as idh1 and idh2 . 
because the optimal timing for patients with mds with lower - risk disease can be challenging and because these genomic biomarkers predicted poor outcome even in patients with lower - risk disease . 
these biomarkers could be used as a justication to proceed with allogeneic stem - cell transplantation early in the disease course , especially if the patient has a lower blast percentage . 
in addition , identifying , with high accuracy , patients who may or may not respond to therapy can prevent prolonged exposure to ineffective therapy and can lead to lower cost without decreasing value or changing patient outcomes . 
introducing these biomarkers into normal hematopoietic cells using crispr / cas9 may offer an opportunity to model and understand hma resistance to develop novel drugs to overcome this resistance . our study highlights the importance of machine learning algorithms such as the recommender system in translating genomic data into useful clinical tools that can be used by physicians in the clinic.20 nevertheless , some limitations to our approach exist . 
it is possible that the response to hmas is derived mainly from epigenetic changes and is not dependent on the genomic changes that we studied here . in summary , our study identied genomic abnormalities that predict response or resistance to hmas in patients with mds , and we validated our results in an independent patient cohort treated in a randomized clinical trial . 
identication of biomarkers that can provide personalized treatment approaches that can predict response or resistance to cancer therapy remains an important clinical challenge , and future drug development should focus on identifying the subgroup of patients who may benet the most from any given cancer therapy . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . open payments is a public database containing information reported by companies about payments made to us - licensed physicians open payments . aziz nazha honoraria : dci consulting or advisory role : karyopharm therapeutics , tolero pharmaceuticals speakers bureau : novartis , incyte research funding : jazz pharmaceuticals mikkael a . 
sekeres consulting or advisory role : celgene , millennium pharmaceuticals , syros pharmaceuticals research funding : takeda pharmaceuticals ( inst ) , pzer ( inst ) rafael bejar honoraria : celgene , alexion pharmaceuticals , abbvie / genentech , astex pharmaceuticals , neogenomics laboratories , daiichi sankyo , forty seven consulting or advisory role : celgene , foundation medicine , neogenomics laboratories , abbvie / genentech , astex pharmaceuticals , daiichi sankyo research funding : celgene , takeda pharmaceuticals travel , accommodations , expenses : celgene megan othus consulting or advisory role : celgene , glycomimetics , cascadia laboratories rami s . 
komrokji stock and other ownership interests : abbvie consulting or advisory role : celgene , novartis , daiichi sankyo , pzer , janssen pharmaceuticals , agios , incyte speakers bureau : novartis , alexion pharmaceuticals , jazz pharmaceuticals travel , accommodations , expenses : celgene , incyte , alexion pharmaceuticals , novartis , jazz pharmaceuticals , daiichi sankyo david p . 
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blood 117 : 403 - 411 , 2011 takahashi k , patel k , bueso - ramos c , et al : clinical implications of tp53 mutations in myelodysplastic syndromes treated with hypomethylating agents . oncotarget 7 : 14172 - 14187 , 2016 9 . 
sekeres ma , othus m , list af , et al : randomized phase ii study of azacitidine alone or in combination with lenalidomide or with vorinostat in higher - risk myelodysplastic syndromes and chronic myelomonocytic leukemia : north american intergroup study swog s1117 . 
short nj , kantarjian hm , loghavi s , et al : treatment with a 5 - day versus a 10 - day schedule of decitabine in older patients with newly diagnosed acute myeloid leukaemia : a randomised phase 2 trial . 
we sought to identify the molecular alterations associated with mpmri - invisible tumors and determine whether mpmri visibility is associated with pca prognosis . methods discovery and validation cohorts included patients who underwent mpmri before radical prostatectomy and were found to harbor both mpmri - visible ( prostate imaging and reporting data system 3 to 5 ) and - invisible ( prostate imaging and reporting data system 1 or 2 ) foci on surgical pathology . 
next - generation sequencing was performed to determine differential gene expression between mpmri - visible and - invisible foci . a genetic signature for tumor mpmri visibility was derived in the discovery cohort and assessed in an independent validation cohort . 
its association with long - term oncologic outcomes was evaluated in a separate testing cohort . results the discovery cohort included 10 patients with 26 distinct pca foci on surgical pathology , of which 12 ( 46% ) were visible and 14 ( 54% ) were invisible on preoperative mpmri . 
a nine - gene signature ( composed largely of cell organization / structure genes ) associated with mpmri visibility was derived ( area under the curve = 0.89 ) , and the signature predicted mri visibility with 75% sensitivity and 100% specicity ( area under the curve = 0.88 ) in the validation cohort . 
recent efforts to overcome this have involved the development and optimization of several diagnostic strategies , including multiparametric magnetic resonance imaging ( mpmri )  . identication of areas that are mpmri permits visual suggestive for intermediate to high - grade cancer . 
the emergence of various mri / ultrasound fusion biopsy platforms has led to increased detection of aggressive pca by facilitating targeted biopsy of visible lesions.1 - 6 as a result , mpmri is now widely used in guiding treatment decisions in men with clinically localized disease , especially when selecting patients suitable for active surveillance or potentially focal therapy.7 - 10 the prevailing view is that only mpmri - visible cancers require clinical action . however , use of mpmri in the evaluation of men with pca is limited by cancer multifocality and interfocal disease heterogeneity . 
individual patients are known to harbor multiple spatially distinct pca foci with varying clinical , radiographic , and pathologic characteristics.11 - 15 up to 55% of all pca foci and 35% of clinically signicant foci are not visible on mpmri.3 , 16 , 17 furthermore , more than 35% of lesions 1 cm or larger are missed by mpmri.17 although some studies have demonstrated that up to 50% of mpmriinvisible pca may harbor relevant genomic alterations , the clinical and prognostic signicance of mpmriinvisible pca remains unknown.18 an improved understanding of the molecular characteristics and clinical trajectories of mpmri - visible and - invisible cancers could facilitate more optimal treatment allocation . 
 salami et al context key objective what is the molecular basis for prostate cancer visibility on multiparametric magnetic resonance imaging ( mpmri ) , and do mpmri - invisible tumors harbor any clinical or biologic signicance compared with visible tumors ? knowledge generated mpmri - visible tumors demonstrated underexpression of genes associated with cellular organization and structure . 
using a novel genetic signature for tumor visibility on mpmri , patients with predicted mpmri - visible and - invisible tumors did not experience signicant differences in biochemical recurrence , distant metastasis , or cancer - specic mortality during followrelevance prostate cancers that are mpmri invisible have similar clinical behavior to mpmri - visible tumors . 
negative mpmri seems insufcient to rule out clinically relevant prostate cancer , and patients at increased risk should be considered for additional testing or systematic prostate biopsy . to be biologically indolent , those with a known diagnosis of low - grade disease and a negative mpmri could be directed toward active surveillance . 
in addition , we test the prognostic signicance of our mpmri - derived genomic signature after radical prostatectomy ( rp )  . methods study design the study used three independent patient populations : discovery , validation , and testing cohorts . 
first , we identied patients with clinically localized disease who the university of underwent preoperative mpmri at michigan in 2015 to 2016 and were subsequently found to harbor multifocal pca at rp . 
the validation cohort from cedars - sinai medical center included patients with either mpmri - visible or - invisible foci , as previously described.19 the testing cohort was composed of patients from the decipher grid pca database treated at johns hopkins medical institute and mayo clinic ( clinicaltrials.gov identier : nct02609269 ) who underwent genome - wide expression proling after rp.20 , 21 preoperative prostate mpmri and pathologic evaluation in the discovery and validation cohorts , mpmri comprising t2 - weighted imaging , diffusion - weighted imaging , and dynamic contrast - enhanced imaging was obtained . 
all mpmri results were re - reviewed and coregistered with whole - mount formalin - xed parafn - embedded rp specimens to delineate mpmri - visible ( prostate imaging and reporting data system [ pi - rads ] version 2 ; score , 3 to 5 ) and - invisible foci . 
our targeted ngs assays were designed to assess relevant pca genomic and transcriptomic alterations and derive clinically available prognostic tests.15 the details of rna sequencing in the validation cohort and genome - wide expression proling in the testing cohorts have been previously described.19 , 24 bioinformatic analysis of the discovery cohort ngs data analysis was performed using torrent suite ( 4.2.0 ; thermo fisher scientc , waltham , ma ) and the coverage analysis plug - ins v.5.0.4. 
details regarding targeted ngs techniques , quality control parameters , dna copy number alterations and variant calls , fusion isoform and partner level analysis , androgen receptor ( ar ) and arsplice variants detection , and prognostic scores derivation have been previously described and summarized in the data supplement.15 , 25 , 26 differential gene expression analysis of mpmri - visible and - invisible cancer foci to determine gene expression differences between mpmri - visible and - invisible tumors , we analyzed rnaseq data from the discovery cohort using two approaches differential expression ( de ) analysis and random forest ( rf ) classieras described in the data supplement . 
 ( a ) cartoon depicting multifocal prostate cancer ( pca ) with both multiparametric magnetic resonance imaging ( mpmri ) visible ( solid black , left ) and invisible ( gray with black discontinuous borders , right ) lesions . 
 salami et al prognostic signicance of mpmri - based gene expression signature 55 ( 14.7% ) developed metastasis , and 28 ( 7.5% ) died as a result of pca ( data supplement )  . a total of 375 patients with genome - wide expression proles were pooled from two independent case - cohort studies20 , 21 to constitute the testing cohort . 
kaplanmeier curves and cox proportional hazard regression were used to evaluate the performance of this signature in predicting oncological outcomes : biochemical recurrencefree survival ( bfs ) , distant metastasisfree survival ( dmfs ) , and pca - specic mortality ( pcsm )  . 
multivariable analyses were performed to evaluate this signature as an independent predictor of oncological outcomes after adjusting for relevant clinicopathological variables , including preoperative prostate - specic antigen , pathologic grade group ( gg ) , surgical margins , extraprostatic extension , seminal vesicle invasion , and lymph node invasion . spearman correlation analysis was performed to measure the association of the gene signature with cellular organization pathway activity . 
among the 14 mpmri - invisible foci ( 54% ) , ve ( 36% ) were gg2 and the remainder were gg1 ( fig 1c and data supplement )  . 
there were 16 patients in the validation cohort , of whom eight ( 50% ) had mpmri - invisible cancer lesions , and two of these ( 25% ) were gg2 ( data supplement )  . 
during follow - up , 136 ( 36.3% ) patients experienced biochemical recurrence , detection of mutations and copy number alterations in the discovery cohort we detected high - condence mutations in 14 of 26 ( 54% ) tumor foci ; six ( 43% ) of the mutations were identied in mpmri - invisible lesions . 
we detected pten one copy number loss in 25% ( three of 12 ) and 14.3% ( two of 14 ) of mpmri - visible and - invisible foci , respectively ( fig 1c )  . discovery and validation of a nine - gene expression signature for mpmri visibility of the 26 total tumor foci in the discovery cohort and 306 amplicons on the rnaseq panel , 24 samples and 74 amplicons , respectively , passed quality control parameters and underwent de analysis ( data supplement )  . 
using de analysis ( data supplement ) and rf classier ( data supplement ) to identify candidate differentially expressed genes , we interrogated four separate logistic regression models for predicting mpmri tumor visibility status using the 19 de analysis genes , 20 rf genes , 11 shared genes between the de analysis and rf gene sets , and 11 shared genes combined with the mutually exclusive genes ( data supplement )  . 
a multivariable rnaseq - based logistic regression model with the best performance for predicting mpmri visibility status , comprising a nine - gene expression signature , was developed from the intersection of the de analysis and rf gene sets ( fig 2a ; data supplement )  . 
this signature correctly predicted seven ( 70% ) of the mpmrivisible and 13 ( 93% ) of the mpmri - invisible foci in the discovery cohort , yielding an area under the curve of 0.89. the optimal probability cutoff for predicting mpmri - visible tumor was greater than 0.46 , with a sensitivity and specicity of 80% and 86% , respectively , in the discovery cohort ( figs 2a and 2b )  . 
we observed underexpression of seven of the nine genes in mpmri - visible tumors , the majority of which were stromal , cellular organization , and structure genes ( fig 2a ; data supplement )  . the nine - gene expression signature was then evaluated in the independent validation cohort ( cedars - sinai medical center ) using the predetermined optimal probability cutoff ( from the discovery cohort ) to predict mpmri visibility status . 
pten one copy number loss was observed in 25% ( three of 12 ) and 14.3% ( two of 14 ) of mpmri - visible and invisible cancer foci , respectively ( false discovery rate , less than 5% )  . 
comparisons of observed ( rst row ) versus predicted ( second row ) mpmri visibility using the nine - gene signature are shown in the annotation , as well as international society of urological pathology grade group . 
 ( b ) receiver operating characteristic curves for the signature in the discovery ( university of michigan [ um ] ) versus the validation ( cedars - sinai medical center [ csmc ] ) cohorts . 
the optimal probability cutoff for predicting mpmri - visible tumor was greater than 0.46 , with a sensitivity and specicity of 75% and 100% in the validation cohort , respectively . for predicting mpmri visibility status were 75% and 100% , respectively , in the validation cohort . 
notably , the signature correctly predicted two gg2 cancers that were mpmri invisible in the validation cohort . prognostic signicance of the nine - gene mpmri visibility expression signature the distribution of each gene composing the nine - gene signature in the normalized microarray data ( testing cohort ) from the decipher grid mapped to the cancer genome atlas prostate adenocarcinoma ( tcga - prad ) rnaseq closely resemble that of the discovery cohort ( data supplement )  . 
prognostic signicance of predicted multiparametric magnetic resonance imaging ( mpmri ) visibility status . patients ( n = 375 ) in the testing cohort were pooled from two independent case - cohort studies ( johns hopkins medical institute [ n = 260 ] and mayo clinic [ n = 235 ] ) to test the capacity of predicted mpmri visibility status to predict ( a ) biochemical recurrence - free survival ( bfs ) , ( b ) distant metastasis - free survival ( dmfs ) , and ( c ) prostate cancerspecic mortality ( pcsm )  . 
normalization was performed to match the distribution of the genomic data from this cohort to the cancer genome atlas prostate adenocarcinoma rnaseq data , as described in methods , to facilitate testing of the rnaseq - based nine - gene signature to predict mpmri - visible tumors ( data supplement )  . 
similar results were obtained using the affymetrix microarray data that were not matched to the distribution of the the cancer genome atlas prostate adenocarcinoma rnaseq data ( data supplement )  . underexpression of seven of the nine genes in mpmrivisible tumors , the majority of which were stromal , cellular organization , and structure genes ( fig 2a ; data supplement )  . 
multivariable analysis to assess the prognostic signicance of predicted multiparametric magnetic resonance imaging ( mpmri ) visibility status . using data from the testing cohort described in figure 3 ( affymetrix microarray data matched to the distribution of the the cancer genome atlas prostate adenocarcinoma rnaseq data ; n = 375 ) , multivariable cox proportional hazard models were developed to assess the capacity of predicted mpmri visibility status to predict : ( a ) biochemical recurrence - free survival ( bfs ) , ( b ) distant metastasisfree survival ( dmfs ) , and ( c ) prostate cancerspecic mortality ( pcsm ) , adjusting for relevant clinicopathological variables . 
epe , extraprostatic extension ; gg , grade group ; hr , hazard ratio ; lni , lymph node invasion ; psa , prostate - specic antigen ; sm , surgical margins ; svi , seminal vesical invasion . using a targeted multiplex ngs approach . 
using robust biostatistic methods , we developed and validated a novel nine - gene signature to predict pca mpmri visibility status . interrogation of this signature in a distinct cohort with longterm follow - up revealed no signicant association with bfs , dmfs , or pcsm . 
taken together , these ndings indicate that mpmri - invisible cancer foci harbor many of the same aggressive molecular features as mpmrivisible foci and may also be clinically signicant . the molecular basis of pca visibility on mpmri is poorly understood . 
 ( a ) box plots of derived prolaris cell cycle progression ( mxccp ) score , oncotype dx genomic prostate score ( mxgps ) , and decipher genomic classier ( mxgc ) stratied by mpmri visibility status in the discovery cohort ( n = 10 patients ; 26 cancer foci )  . 
box plots of derived mxgps androgen , cellular organization , and stromal submodules stratied by mpmri visibility status are shown , with each point representing an individual cancer focus colored according to gg . 
only the cellular organization submodule had a signicant difference in mean expression ( p = .014 ) , suggesting that at the rna expression level mpmri visibility is related to underlying cellular organization of the tumor . explain cancer visibility on mpmri.28 in a recent report , li et al19 observed signicant fold changes of differentially expressed genes on the basis of mpmri visibility regardless of gleason score or tumor size , including genes involved in cytoskeleton organization . 
 molecular basis and prognosis of mri - invisible prostate cancer mpmri - visible foci in the discovery cohort demonstrated pten one copy number loss compared with 14% in mpmri - invisible foci . 
although pca is multifocal and mpmri may miss up to 35% of intermediateto high - grade pca , the absence of visible lesions on mpmri has been proposed as a reason to defer conrmatory biopsy when considering active surveillance.1 , 3 , 16 , 17 in addition , mpmri is increasingly being used to identify the index or dominant cancer foci for focal therapy . 
to be sure , although size and grade are believed to be important , how best to dene the biologically dominant cancer in multifocal disease is not known.35 to date , no study has demonstrated the clinical trajectory of mpmri - visualized lesions . 
such a study would be a challenge to perform , given the long duration of follow - up required and the multifocal nature of pca , with frequent coexistence of mpmri - visible and - invisible cancers within the same gland.31 salmasi et al36 reported that the pi - rads ( a grading system for mpmri lesion visibility ) was not a signicant predictor of adverse pathology at the time of rp . 
similarly , parry et al18 found that 50% of mpmri - invisible cancers harbored one or more genetic alterations commonly observed in metastatic castrate - resistant pca , suggesting that mpmri - invisible tumors may be as important as visible ones . 
in the study by li et al , 19 a four - gene signature comprising genes differentially expressed between mpmri - visible and - invisible pca was shown to predict bfs in two external data sets . 
however , this signature was not developed as a predictor of or a surrogate for mpmri cancer visibility , but rather it was selected on the basis of their common association with mpmri visibility and metastasis . 
by contrast , in this rst study of its kind to our knowledge , using a validated novel mpmri - based rnaseq signature as a surrogate instrument for mpmri visibility status , we have demonstrated that predicted mpmri visibility status was not associated with bfs , dmfs , or pcsm during long - term follow - up . 
put another way , mpmriinvisible pca does not seem to represent purely indolent disease ; mpmri - invisible lesions may be just as clinically relevant as mpmri - visible disease . 
first , in the diagnostic setting , these data corroborate ndings from several institutions indicating that a negative mpmri does not rule out the presence of clinically signicant pca3 , 17 , 31 and should therefore not preclude a prostate biopsy without consideration of clinical risk.37 , 38 second , in the setting of active surveillance , our ndings underscore the potential mpmri - invisible cancer foci to harbor similar biologic trajectories as mpmri - visible disease . 
although additional studies are needed to delineate the utility of mpmri in reducing the frequency of surveillance biopsies , the current literature supports systematic in addition to targeted biopsies in men undergoing active surveillance.3 , 6 last , for men considering focal therapy , our data demonstrate that mpmri alone is not sufcient to rule out the presence of a potentially lethal , nondominant cancer focus . our study has several limitations . 
however , our novel rnaseq signature demonstrated high accuracy for predicting mpmri visibility in the validation cohort , including 19% gg5 lesions . moreover , gg4 and 5 lesions are generally mpmri visible , and such patients routinely undergo whole - gland therapy . fourth , the discovery cohort was made up of a relatively small sample , with low proportion of erg - positive tumors . nonetheless , we similarly observed high test performance in the validation cohort with erg overexpression in 31% of samples . 
to facilitate reproducibility , all lesions in the current study were scored according to the validated pi - rads v2 systepi - rads 1 and 2 lesions were classied as mpmri invisible , and pi - rads 3 to 5 were classied as mpmri visible . 
thus , additional studies are needed to delineate the prognostic signicance of mpmri - invisible pca in a prospective clinical cohort . discerning aggressive from indolent disease remains a signicant clinical challenge in the evaluation and management of men with primary pca . 
our ndings indicate that mpmri - invisible cancers were no less likely to harbor lethal biologic potential than visible tumors , highlighting the limitation of using mpmri alone to guide patient management or delineate specic index cancer foci for ablative therapy . 
morgan consulting or advisory role : myriad genetics , terumo bct research funding : myriad genetics ( inst ) , mdxhealth ( inst ) , genomedx ( inst ) arvin k . 
tomlins employment : strata oncology leadership : strata oncology stock and other ownership interests : strata oncology consulting or advisory role : abbvie , janssen , astellas medivation , strata oncology , sano , almac diagnostics research funding : astellas medivation ( inst ) , genomedx ( inst ) patents , royalties , other intellectual property : i am a coauthor on a patent issued to the university of michigan on ets gene fusions in prostate cancer . 
the diagnostic eld of use has been licensed to hologic / genprobe , who has sublicensed some rights to ventana medical systems / roche . travel , accommodations , expenses : strata oncology hyung l . 
palapattu stock and other ownership interests : nantkwest consulting or advisory role : janssen scientic affairs research funding : minomic patents , royalties , other intellectual property : implantable nanotechnology for long - term testosterone delivery functionalized ducial marker for drug delivery no other potential conicts of interest were reported . references kasivisvanathan v , rannikko as , borghi m , et al : mri - targeted or standard biopsy for prostate - cancer diagnosis . 
n engl j med 378 : 1767 - 1777 , 2018 ahmed hu , el - shater bosaily a , brown lc , et al : diagnostic accuracy of multi - parametric mri and trus biopsy in prostate cancer ( promis ) : a paired validating conrmatory study . 
lancet 389 : 815 - 822 , 2017 filson cp , natarajan s , margolis dja , et al : prostate cancer detection with magnetic resonance - ultrasound fusion biopsy : the role of systematic and targeted biopsies . 
cancer 122 : 884 - 892 , 2016 salami ss , ben - levi e , yaskiv o , et al : in patients with a previous negative prostate biopsy and a suspicious lesion on magnetic resonance imaging , is a 12 - core biopsy still necessary in addition to a targeted biopsy ? bju int 115 : 562 - 570 , 2015 salami ss , vira ma , turkbey b , et al : multiparametric magnetic resonance imaging outperforms the prostate cancer prevention trial risk calculator in predicting clinically signicant prostate cancer . 
cancer 120 : 2876 - 2882 , 2014 siddiqui mm , rais - bahrami s , turkbey b , et al : comparison of mr / ultrasound fusion - guided biopsy with ultrasound - guided biopsy for the diagnosis of prostate cancer . 
jama 313 : 390 - 397 , 2015 ahmed hu , hindley rg , dickinson l , et al : focal therapy for localised unifocal and multifocal prostate cancer : a prospective development study . 
j urol 196 : 68 - 75 , 2016 ahmed hu , dickinson l , charman s , et al : focal ablation targeted to the index lesion in multifocal localised prostate cancer : a prospective development study . eur urol 68 : 927 - 936 , 2015 10 . 
guillaumier s , peters m , arya m , et al : a multicentre study of 5 - year outcomes following focal therapy in treating clinically signicant nonmetastatic prostate cancer . 
cooper cs , eeles r , wedge dc , et al : analysis of the genetic phylogeny of multifocal prostate cancer identies multiple independent clonal expansions in neoplastic and morphologically normal prostate tissue . 
j urol 193 : 87 - 94 , 2015 johnson dc , raman ss , mirak sa , et al : detection of individual prostate cancer foci via multiparametric magnetic resonance imaging . 
ross ae , johnson mh , youse k , et al : tissue - based genomics augments post - prostatectomy risk stratication in a natural history cohort of intermediateand 21 . 
karnes rj , bergstralh ej , davicioni e , et al : validation of a genomic classier that predicts metastasis following radical prostatectomy in an at risk patient high - risk men . 
hovelson dh , mcdaniel as , cani ak , et al : development and validation of a scalable next - generation sequencing system for assessing relevant somatic variants in solid tumors . 
erho n , crisan a , vergara ia , et al : discovery and validation of a prostate cancer genomic classier that predicts early metastasis following radical prostatectomy . plos one 8 : e66855 , 2013 466 : 297 - 311 , 2015 25 . 
palapattu gs , salami ss , cani ak , et al : molecular proling to determine clonality of serial magnetic resonance imaging / ultrasound fusion biopsies from men on active surveillance for low - risk prostate cancer . 
klein ea , cooperberg mr , magi - galluzzi c , et al : a 17 - gene assay to predict prostate cancer aggressiveness in the context of gleason grade heterogeneity , tumor multifocality , and biopsy undersampling . 
truong m , hollenberg g , weinberg e , et al : impact of gleason subtype on prostate cancer detection using multiparametric magnetic resonance imaging : correlation with nal histopathology . 
vargas ha , akin o , shukla - dave a , et al : performance characteristics of mr imaging in the evaluation of clinically low - risk prostate cancer : a prospective study . radiology 265 : 478 - 487 , 2012 30 . 
hurrell sl , mcgarry sd , kaczmarowski a , et al : optimized b - value selection for the discrimination of prostate cancer grades , including the cribriform pattern , using diffusion weighted imaging . 
salmasi a , khoshnoodi p , felker er , et al : a 17 - gene genomic prostate score assay provides independent information on adverse pathology in the setting of combined multiparametric magnetic resonance imaging fusion targeted and systematic prostate biopsy . 
a recent retrospective analysis found a clear association of improved survival with continuation of endocrine therapy upon diagnosis of brain metastases.10 remarkably , the cdk4 / 6 - inhibitor abemaciclib had a clinical benet rate of 25%.11 preclinical models of bc brain metastases suggest pi3k pathway inhibition may be effective for treatment of brain metastases.12 notably , both sandpiper and solar - 1 excluded patients with untreated or active cns metastases6 , 7 ; however , the precursor to alpelisib , buparlisib , did have brain penetration , which was thought to be the cause for the higher incidence of mood disorders.13 an increase in depression has distinctly not been seen with the - specic pi3kinhibitor alpelisib and , in preclinical animal models with intact blood - brain barrier , no signicant distribution into the brain was seen ( unpublished data )  . thus , the activity of alpelisib in brain metastases is unknown . herein , we report a case series of 4 patients with er + / progesterone receptorpositive ( pr + ) / her2 metastatic bc with progressive brain metastases ( fig 1 ) treated with alpelisib . 
all patients provided consent to publish their information and images . case 1 a 55 - year - old woman presented with a large breast ulceration , biopsy specimendiagnosed invasive ductal carcinoma ( idc ) , grade 3 , er + / pr + / her2 . computed tomography ( ct ) scan revealed pulmonary nodules , osseous lesions , and hypodense lesions within the right hepatic lobe . 
brain magnetic resonance imaging ( mri ) showed a 10 - mm mass in the left cerebellar hemisphere ; this was treated with stereotactic radiosurgery with initial shrinkage to 8 mm and stabilization on follow - up . 
brain mri showed an increase of the left cerebellar lesion to 12 mm , judged by neuroradiology and radiation oncology to be more compatible with progression than with radiation - induced tissue necrosis . 
the patients body mass index ( bmi ) was 25 ( calculated as kilograms divided by square of height in meters ) and eastern cooperative oncology group ( ecog ) performance status ( ps ) score of 0 . 
brain mri after 6 weeks showed a reduction in the left cerebellar lesion to 9 mm ( 62% reduction of bidimensional areas , 35% reduction of sum of longest distances )  . 
follow - up mri 2 months later revealed stability of the cns lesion . subsequent brain mri at 3 , 4 , and 6 months showed stable disease without changes in measurements . 
this was compatible with a partial response per response in neuro - oncology brain metastases assessment ( rano - bm ) criteria.14 case 2 a 71 - year - old woman was diagnosed in 2010 with pt2n0 idc of the right breast , grade 3 , er + / pr + / her2 . 
in 2017 , she had a recurrence in the right breast , pleural effusion , and bone metastases and was treated with multiple regimens : letrozole and palbociclib , fulvestrant and palbociclib , and capecitabine and paclitaxel . 
she was serially treated with fulvestrant and palbociclib , radiation to the base of skull to treat cranial nerve symptoms , and with exemestane and everolimus , capecitabine , and abemaciclib . 
for the rst time , brain mri demonstrated multiple parenchymal metastases and she was treated with hippocampal - sparing wbrt . subsequently , treatment was changed from abemaciclib to liposomal doxorubicin for progression in the brain , followed by gemcitabine . 
brain mri 6 weeks later demonstrated a 14% reduction in the sum of longest distances of measurable brain metastases ( 24% reduction in bidimensional areas ) and regressions of nonmeasurable brain metastases . 
the most recent brain mri at the 6 - month mark revealed progressive parenchymal disease requiring change of therapy . case 4 a 70 - year - old woman was diagnosed in 2013 with t1n1 idc of the right breast , grade 3 , er + / pr + / her2 . 
she was treated with breast - conserving surgery , adjuvant docetaxel plus cyclophosphamide , radiation , and anastrozole . 2018 , metastatic disease developed to the lung , liver , and bone while she received adjuvant anastrozole . 
follow - up mri demonstrated at least 15 new intraparenchymal lesions and several progressing dural - based lesions , so the patient proceeded to undergo wbrt and restarted capecitabine therapy . 
examination of a liquid biopsy specimen revealed multiple pi3k mutations ( pik3ca : h1047r , e81k , and e563k ) and she was administered alpelisib ( 300 mg ) table 1 . 
restaging after 6 weeks of therapy revealed substantial disease regression in the lungs and liver as well as interval resolution of punctate cerebellar and cerebral metastasis and reduction of a dural metastasis ( appendix fig a1 ) , compatible with stable disease per rano - bm criteria.14 repeated brain mri at the 3and 5month marks showed stable disease . discussion activating pik3ca mutations occur early in breast carcinogenesis and are typically not lost or acquired during clonal evolution in later stages of the diseasefeatures that suggest these are driver mutations . 
table 1 provides a summary of mutational prole and previous treatments . cases 1 and 2 harbored the activating mutation pik3ca h1047r in the coding exon 20 , a kinase - activating mutation and the most common mutation in bc.14 case 1 also had pik3c2b amplication , which occurs in 13% to 25% of patients.15 pik3c2b is a class ii pi3 - kinase.16 whether its amplication in conjunction with pik3ca mutation deepens or attenuates pi3k - pathway dependence of cancer and whether pik3c2bs kinase activity is inhibited by alpelisib is unknown . 
however , understanding this relationship appears to be important because activating pik3ca mutations and copy number gain of pik3c2b do co - occur in bc.15 case 3 harbored the pik3ca e545k mutation , affecting the helical domain of p110that activates signaling because of its detachment from the inhibitory p85 subunit of pi3k.17 helical domain mutations are the second most frequent in bc , with an incidence of 6.4%.14 case 4 had 3 mutations in pik3ca ; e81k and h1047r are activating mutations and e563k is novel . 
this combination of a major ( h1047r ) and a minor ( e81k ) pik3ca mutation is thought to amplify pi3k signaling and predict for responsiveness to pi3k inhibition.18 this patient had a comutation of pik3ca mutations and esr1 . 
the earlier pan - pi3k inhibitor buparlisib was tested in 4 patients with treatment - refractory cns lymphoma , 1 of whom achieved a partial remission.23 in animal models , systemically administered buparlisib showed activity against bc brain metastases.24 - 26 patients with active brain metastases were excluded from the pivotal solar - 1 and sandpiper studies.6 , 7 conclusions from our observations are limited by the small number of patients selected on the basis of their surprising response . 
the rano - bm criteria consider lesions , 10 mm as nonmeasurable.14 here , we show examples with resolution of small lesions , which are clinically meaningful but classied as stable disease per the criteria . 
additional investigation to prospectively evaluate alpelisib in patients with bc and cns involvement may be justied . in conclusion , we have described cases of regression or stabilization of progressive cns lesions in patients with hr + / her2 metastatic bc treated with the pi3k inhibitor alpelisib . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . stacy moulder research funding : oncothyreon ( inst ) , pzer ( inst ) , novartis ( inst ) , genentech ( inst ) , takeda ( inst ) , bayer ( inst ) , emd serono ( inst ) , genentech ( inst ) eric p . 
winer stock and other ownership interests : verastem honoraria : roche , genomic health consulting or advisory role : leap therapeutics , seattle genetics , jounce therapeutics , glaxosmithkline , carrick therapeutics , eli lilly , genomic health , g1 therapeutics research funding : genentech ( inst ) , novartis ( inst ) hope s . 
rugo consulting or advisory role : ionis , celtrion research funding : macrogenics ( inst ) , obi pharma ( inst ) , eisai ( inst ) , pzer ( inst ) , novartis ( inst ) , eli lilly ( inst ) , genentech ( inst ) , merck ( inst ) , immunomedics ( inst ) , odonate therapeutics ( inst ) , daiichi sankyo ( inst ) , seattle genetics ( inst ) travel , accommodations , expenses : pzer , puma biotechnology , mylan , amgen , astrazeneca , macrogenics , daiichi sankyo , merck , novartis , obi pharma open payments link : nancy u . 
lin consulting or advisory role : roche , seattle genetics , puma biotechnology , novartis , daiichi sankyo research funding : genentech , pzer , seattle genetics , merck patents , royalties , other intellectual property : royalties for chapter in upto - date regarding management of breast cancer brain metastases , royalties from jones & bartlett gerburg m . 
wulf stock and other ownership interests : selecta biosciences ( i ) research funding : merck patents , royalties , other intellectual property : pin1 as a marker for abnormal cell growth ( patent no . : 8129131 ) no other potential conicts of interest were reported . references cancer genome atlas network : comprehensive molecular portraits of human breast tumours . 
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genes chromosomes cancer 52 : 69 - 80 , 2013 ramirez - ardila de , helmijr jc , look mp , et al : hotspot mutations in pik3ca associate with rst - line treatment outcome for aromatase inhibitors but not for tamoxifen . 
breast cancer res treat 139 : 39 - 49 , 2013 kalinsky k , jacks lm , heguy a , et al : pik3ca mutation associates with improved outcome in breast cancer . 
clin cancer res 15 : 5049 - 5059 , 2009 baselga j , cortes castan j , de laurentiis m , et al : sandpiper : phase iii study of the pi3 - kinase ( pi3k ) inhibitor taselisib ( gdc - 0032 ) plus fulvestrant in patients ( pts ) with oestrogen receptor ( er ) - positive , her2 - negative locally advanced or metastatic breast cancer ( bc ) enriched for pts with pik3ca - mutant tumours . 
ann oncol 27 : vi99 , 2016 ( suppl 6 ) andr e f , ciruelos e , rubovszky g , et al : alpelisib for pik3ca - mutated , hormone receptor - positive advanced breast cancer . 
n engl j med 380 : 1929 - 1940 , 2019 adamo b , deal am , burrows e , et al : phosphatidylinositol 3 - kinase pathway activation in breast cancer brain metastases . 
breast cancer res 13 : r125 , 2011 fitzgerald dm , muzikansky a , pinto c , et al : association between pik3ca mutation status and development of brain metastases in hr + / her2metastatic breast cancer . 
bergen es , berghoff as , medjedovic m , et al : continued endocrine therapy is associated with improved survival in patients with breast cancer brain metastases . clin cancer res 25 : 2737 - 2744 , 2019 11 . 
tolaney sm , lin nu , thornton d , et al : abemaciclib for the treatment of brain metastases ( bm ) secondary to hormone receptor positive ( hr + ) , her2 negative breast cancer . 
j clin oncol 35 : 1019 , 2017 ( 15 suppl ) ippen fm , alvarez - breckenridge ca , kuter bm , et al : the dual pi3k / mtor pathway inhibitor gdc - 0084 achieves antitumor activity in pik3ca - mutant breast cancer brain metastases . 
campone m , im s - a , iwata h , et al : buparlisib plus fulvestrant versus placebo plus fulvestrant for postmenopausal , hormone receptor - positive , human epidermal growth factor receptor 2 - negative , advanced breast cancer : overall survival results from belle - 2 . 
takeshita t , yamamoto y , yamamoto - ibusuki m , et al : analysis of esr1 and pik3ca mutations in plasma cell - free dna from er - positive breast cancer patients . 
study_list = brca_igr_2015%2cbrca_mbcproject_wagle_2017&case_set_id = all&data_priority = 0&gene_list = esr1%253amut%250apik3ca%253amut& geneset_list = %20&prolefilter = 0&tab_index = tab_visualize juric d , castel p , grifth m , et al : convergent loss of pten leads to clinical resistance to a pi ( 3 ) k inhibitor . 
grommes c , pentsova e , nolan c , et al : phase ii study of single agent buparlisib in recurrent / refractory primary ( pcnsl ) and secondary cns lymphoma 24 . 
maira s - m , pecchi s , huang a , et al : identication and characterization of nvp - bkm120 , an orally available pan - class i pi3 - kinase inhibitor . 
 germline and somatic smoothened mutations in nonsmall - cell lung cancer are potentially responsive to hedgehog inhibitor vismodegib introduction smoothened ( smo ) is a seven - membrane spanning receptor involved in the hedgehog signaling pathway and is directly inhibited by patched ( ptch ) .1 in the absence of ptch inhibition , smo activates gli family transcription factors and subsequently regulates stemand progenitor cell differentiation . 
dysregulation and activation of the hedgehog pathway are associated with carcinogenesis.2 smo has been identified as an oncogene with activating mutations in sporadic basal cell carcinomas ( bccs ) 1 and medulloblastomas.3 activating smo mutations are highly relevant targets for therapy , because oral smo inhibitors , such as vismodegib ( erivedge ; genentech , san francisco , ca ) , have had proven success in antitumor activity.4 , 5 in nonsmall - cell lung cancer ( nsclc ) , neither somatic nor germline smo mutations have previously been characterized . 
 we discovered a novel germline smo p641a mutation in a patient with refractory nsclc who responded to vismodegib therapy for several months . the patient was a 69 - year - old nonsmoking man ( patient a ) with a prior fully resected bcc who developed widely metastatic nsclc . 
 none of the other first - degree relatives reported a malignancy history , and none carried the p641a mutation . we subsequently identified two additional patients ( patients b and c ) with metastatic nsclc who had smo mutations by our routine genetic profile of 50 genes via the md anderson cancer center molecular diagnostics laboratory and treated them with vismodegib . 
patient b ( adenocarcinoma ) was also found to carry the germline smo p641a mutation ; however , despite initial stabilization of his rapidly growing disease , he stopped vismodegib at 14 weeks because of grade 3 fatigue , experienced rapid disease progression , and died . 
 ( a ) radiographic images of patient a at baseline with images of lung and liver metastases and restaging chest and abdominal imaging of lung metastases after 6 weeks of vismodegib . 
all patient and family members signed informed consent for participation in this analysis within institutional review boardapproved protocol pa2014 - 0455 . results we determined the incidence of somatic smo mutations to be 2.6% in the lung adenocarcinoma cohort and found one case ( d209y ) in the squamous cohort from tcga ( n = 230 and 178 , respectively )  . 
eight germline smo p641a mutation cases ( variant frequency , 0.11% ) were identified in various cancer types , whereas none of the control germline cohort individuals had smo p641a mutation . 
similar results were obtained using additional lung cancer cell lines and the hedgehog inhibitor cyclopamine ( appendix fig a1 , online only )  . we hypothesized that ptch1 may interact with smo in the cytoplasmic domains and that smo p641a mutation disrupts smo / ptch1 interactions and releases smo suppression . 
although multiple models propose how ptch1 suppresses smo activity , 8 the binding affinity of ptch1 to smo is approximately 2 nm.9 on the basis of our in silico models of the cytoplasmic domain structures of both ptch1 and smo using our previously described approach of homology modeling and structural refinement , 10 - 12 we determined that smo p641 is located in the cytoplasmic domain on a loop between two beta sheets , in the area where smo and ptch1 interact ( fig 3 )  . computational alanine scanning and mutabind13 suggest that smo p641 destabilizes ptch1 binding with loss of binding energy and is a hotspot residue ( g > 1.5 kcal / mol )  . 
loss of the proline - aromatic interactions ( pro641 v phe1264 ) , which are critical in protein stability and protein - protein interactions , partly contributes to the binding reduction.14 , 15 once mutated to alanine , the smo loop can change conformation easily and potentially cause steric hindrance with another hotspot residue : val639 of smo ( g = 3.7 kcal / mol )  . 
computational alanine scanning showed that smo p641a mutation disfavors smo and ptch1 binding , leading to loss of binding energy of 2.3 kcal / mol , suggesting smo p641 is a hotspot residue ( g > 1.5 kcal / mol ) on the binding interface . 
this reduction in binding is partially because of the loss of proline - aromatic interactions ( pro641 v phe1264 ) , which are critical in protein stability and protein - protein interactions.14 , 15 in addition , the prolyl ring restricts and maintains the smo loop conformation and drives formation of the ring - ring stacking interactions of pro641 and phe1264 . 
also , smo p641a causes the side chain of ptch1 phe1264 to swing away because of the loss of interaction with proline , and this new position causes some steric hindrance with another hotspot residue : val639 of smo ( g = 3.7 kcal / mol )  . 
multiple proteins , including 2cz9 , 2no4 , and 4b3h structures , were used as the template for smo , and 2hg4 , 2q7v , 4xyc , and 5bwi were used for ptch1 . 
our structural modeling of smo p641a suggests that the conformational changes prevent or significantly limit ptch binding to smo , which leads to constitutive activation of downstream hedgehog signaling and dysregulated growth . 
this model does not preclude the possibility of catalytic regulation of smo by ptch1 via diffusion of a second messenger molecule , 8 where the diminished interaction would reduce smo translocation to the membrane for activation . in our analysis of the tcga databases , somatic smo mutations are rare , occurring in 1.7% of patients with nsclc . 
germline smo p641a mutations were not observed in patients with nsclc in the tcga database , but in the overall tcga database they were observed in 0.11% of patients with cancer , compared with 0% in individuals without cancer . 
 larger studies are needed to further investigate this hypothesis . it is possible that germline smo p641a mutation may be a precursor mutation that requires an additional alteration , such as tp53 mutation , to induce full carcinogenesis . 
in support of this hypothesis , both our patients with smo p641amutated nsclc had concomitant ( but different ) somatic tp53 mutations in their lung cancers , but not in their germline analyses . 
for example , it was reported16 , 17 that hedgehog pathway signaling via mutant smo constitutive activation can prevent p53 accumulation by enhancing p53 binding to mdm2 for ubiquitination , thus potentially leading to acceleration of carcinogenesis . 
additional studies will be needed to investigate the possible interactions between these pathways and determine whether , in the context of hedgehog pathway activation from smo mutations , p53 loss or mutation may serve as a protumorigenic second hit . in conclusion , we identified and treated a patient with a germline smo p641a mutation with vismodegib and achieved a significant response . 
 for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . evidence that smo mutations may be a heritable driver not only of bcc but potentially of nsclc as well . 
however , the specific role of germline and somatic smo alterations in promoting carcinogenesis , interactions with p53 , and other oncogenic alterations and the responsiveness of different smo mutations to hedgehog inhibitors are important questions that merit further investigation . 
 lixia diao no relationship to disclose jing wang no relationship to disclose vassiliki papadimitrakopoulou consulting or advisory role : clovis oncology , genentech , merck , biothera , eli lilly , janssen , gensignia life sciences , astrazeneca , ariad pharmaceuticals , nektar research funding : merck ( inst ) , novartis ( inst ) , celgene ( inst ) , clovis oncology ( inst ) , bayer healthcare pharmaceuticals ( inst ) , bristol - myers squibb ( inst ) , astrazeneca ( inst ) , pfizer ( inst ) , janssen oncology ( inst ) , acea biosciences ( inst ) myvizhi esai selvan no relationship to disclose zeynep h . 
heymach stock and other ownership interests : cardinal spine , bio - tree consulting or advisory role : astrazeneca , abbvie , boehringer ingelheim , bristol - myers squibb , medivation , ariad pharmaceuticals , synta , oncomed , novartis , genentech , calithera biosciences research funding : astrazeneca ( inst ) acknowledgment we thank fred de sauvage , md , emily roarty , phd , li xu , and robert klein for contributing to the project . ximing tang no relationship to disclose wei lu no relationship to disclose humam kadara no relationship to disclose dimitry n . 
tsao , ignacio wistuba , dianren xia , lauren byers , lixia diao , jing wang , vassiliki papadimitrakopoulou , ximing tang , wei lu , zhi tan , shuxing zhang , monique nilsson , and john v . 
heymach , the university of texas md anderson cancer center , houston , tx ; humam kara , american university of beirut , beirut , lebanon ; and dimitry n . 
chen l , du - cuny l , moses s , et al : novel inhibitors induce large conformational changes of gab1 pleckstrin homology domain and kill breast cancer cells . 
 appendix mutation and sequencing analysis archival tumor tissue dna was extracted using the generead dna formalin - fixed , paraffin - embedded ( ffpe ) kit ( qiagen , hilden , germany )  . 
surveying of mutations in hotspot regions of 46 cancer - related genes including smo was performed via ion ampliseq cancer panel ( life technologies , carlsbad , ca )  . 
the details for these methods using ampliseq cancer panel have been described previously ( singh rr , et al : j mol diagn 15 : 607 - 622 , 2013 )  . 
from the barcoded library , a manual emulsion polymerase chain reaction was performed , followed by sequencing of eight multiplexed samples using the ion personal genome machine on ion 318 chips . 
 torrent suite software ( version 2.0 ; thermo fisher ) was used for analysis of the sequence generated . for the germline and validation tumor analyses , a custom ampliseq panel targeting the coding regions of smo and p53 was designed on ampliseq.cothe smo / p53 panel was then used to prepare libraries for 24 dna samples from ffpe tissue , saliva , and blood with a modified protocol of the ion ampliseq library kit 2.0 ( life technologies )  . 
the target amplification step for each of the two primer pools was carried out in a half - volume reaction and combined after thermal cycling to create a single - volume reaction used in the rest of the preparation . 
the barcoded libraries were quantitated with quantitative polymerase chain reaction using the ion library taqman quantitation kit ( life technologies )  . the libraries were then pooled for 12 samples per chip , and the equivalent of 7 l of a 100 - pm solution was used to prepare template with the ion pi template ot2 200 kit ( version 3 ; life technologies ) according to manufacturer protocol . 
the template was then loaded onto an ion pi chip ( version 2 ; life technologies ) and sequenced on an ion proton sequencer with the sequencing reagents provided in the ion pi sequencing 200 kit ( version 3 ; life technologies ) as per manufacturer instructions . a bed file provided from ampliseq.com for the smo / p53 panel was used to generate a sequencing report in the ion torrent browser ( version 4.2 ) for use in assessing the quality of the libraries , chips , and reagents during the sequencing process . 
it was deparaffinized with deparaffinization solution at 56c for 3 minutes and digested with proteinase k at 56c for 1 hour ; nucleic acid was reverse formaldehyde modified at 90c for 1 hour , and artificially induced uracils were removed with the enzyme uracil - n glycosilase at 50c for 1 hour in a thermomixer . 
dna was quantified with nanodrop ( nd1000 spectrophotometer ; wilmington , de ) and the qubit dsdna hs assay ( life technologies )  . dna isolated from saliva saliva was collected with the ogr - 500 kit ( dna genotek ) , and dna was extracted with the prepit.l2p kit ( dna genotek )  . 
clear supernatant was transferred to a fresh 15 - ml centrifuge tube , to which 1.2 volume of room - temperature 100% ethanol was added , and mixed ; the mixture was then left to stand at room temperature for 10 minutes . 
these rare smo variants were scored for functional deleteriousness with combined annotation dependent depletion ( kircher m , et al : nat genet 46 : 310 - 315 , 2014 ) and kept if phred score 20 for subsequent variant frequency estimates . cell viability assays tumor cells were plated at a ratio of 2 , 000 cells per well in 96 - well plates and were treated with 10% fetal bovine serum media with increasing concentrations of vismodegib or cyclopamine . 
 ( a ) western blot demonstrating expression of gli1 and ptch1 / 2 in h1437 ( left ) and hcc4006 ( right ) nonsmall - cell lung cancer ( nsclc ) cells expressing smo wild type ( wt ) or smo p461a . 
giannetta , md1 ; gianluca tomasello , md1 ; stefano stabile , phd1 ; valentina motta , phd1 ; spyridon alexiadis , md1 ; francesco scaglione , md , phd1 , 2 ; angelo vanzulli , md1 , 2 ; massimo torre , md1 ; emanuela bonoldi , md1 ; silvio m . 
veronese , phd1 ; salvatore siena , md1 , 2 ; and andrea sartore - bianchi , md1 , 2 introduction epidermal growth factor receptor ( egfr ) gene mutations are strong oncogenic drivers in a subset of nonsmall - cell lung cancer ( nsclc )  . 
their inhibition with specic tyrosine kinase inhibitors ( tkis ) represents a successful example of precision medicine.1 nevertheless , disease progression almost invariably occurs after 9 - 14 months of treatment with either getinib , erlotinib , or afatinib ( rstand second - generation tkis ) 2 - 4 and after 19 months with osimertinib ( a thirdgeneration tki ) 5 because of the development of acquired therapeutic resistance . several mechanisms of tki resistance have been reported , with different mechanisms for rst - , second - , 6 and third - generation tkis.7 the acquisition of t790m mutation in exon 20 of egfr represents the most frequent mechanism ( more than 50% of patients ) of disease progression with getinib , erlotinib , or afatinib , which can be overcome by osimertinib and other thirdgeneration inhibitors . 
however , a frequent cause of third - generation tki resistance is the development of mutations at the egfr c797 codon , because they prevent binding to the egfr active site.8 , 9 in these patients , preclinical studies have shown that c797s mutation can be found in the same ( in cis ) or different ( in trans ) t790m - mutated alleles , or in other patients the t790m mutation can be lost.10 in clinical practice , resistant mechanisms to different tkis can be detected on disease progression through tissue rebiopsy . 
the isolation and analysis of circulating tumor dna ( ctdna ) through liquid biopsy is also recommended and widely used for identication of acquired resistance mutations of egfr.11 however , not only target - dependent resistance mechanisms can occur . 
after 9 months , the patient experienced disease progression in the liver ( data supplement ) , and a liquid biopsy revealed the acquisition of egfr t790m mutation ( fig 1b ; table 1 )  . 
almost 12 months later , dyspnea worsened , with evidence of increased right pleural effusion and disease progression in the lung , lymph nodes , and liver ( data supplement )  . a new liquid biopsy identied persistence of t790m plus the acquisition of c797s in trans conformation ( table 1 ; fig 1 - c )  . 
synopsis of therapeutic history and histologic and molecular analysis of the present patient showing tumor evolution toward small - cell lung cancer ( sclc ) transformation and accumulation of epidermal growth factor receptor ( egfr ) genetic abnormalities . 
in the case of sclc transformation , a favorable response to etoposide and platinum can be expected25 ; therefore , a rebiopsy should be performed when a histologic transformation is suspected ( eg , aggressive progression )  . in this case report , which describes a representative patient , different subclones harboring distinct resistance mechanisms coexisted . 
the initial ratio of t790m / activating mutation was below the threshold of 0.05 and , according to the ndings of chabon et al , 24 the response to osimertinib was limited to a stable disease by recist criteria . 
this ratio deeply decreased ( table 1 ) at progression after 12 months of therapy with osimertinib when c797s appeared concomitantly with a small - cell transformation , after a total of 20 months of treatment with tkis . 
at this time point , we observed a reduction of t790m / del19 ratio in ctdna , which was similar to the c797s / del19 ratio ( table 1 )  . 
 pizzutilo et al in conclusion , our case report underlines the importance of monitoring the evolution of tissue rebiopsy for identifying heterogeneous resistance mechanisms , especially in patients with aggressive progression , the disease and of to better dene potential treatment modications . 
pizzutilo , calogero lauricella , giulio cerea , massimo torre , salvatore siena , andrea sartore - bianchi financial support : salvatore siena provision of study materials or patients : elio g . 
giannetta , stefano stabile , valentina motta , spyridon alexiadis , angelo vanzulli , emanuela bonoldi , silvio m . veronese , salvatore siena , andrea sartore - bianchi data analysis and interpretation : elio g . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . angelo vanzulli travel , accommodations , expenses : bracco diagnostics , ge healthcare emanuela bonoldi consulting or advisory role : bayer silvio m . 
mitsudomi t , morita s , yatabe y , et al : getinib versus cisplatin plus docetaxel in patients with non - small - cell lung cancer harbouring mutations of the epidermal growth factor receptor ( wjtog3405 ) : an open label , randomised phase 3 trial . 
lancet oncol 11 : 121 - 128 , 2010 rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutationpositive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
lancet oncol 13 : 239 - 246 , 2012 sequist lv , yang jc - h , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
j clin oncol 31 : 3327 - 3334 , 2013 soria j - c , ohe y , vansteenkiste j , et al : osimertinib in untreated egfr - mutated advanced non - small - cell lung cancer . 
 case report thress ks , paweletz cp , felip e , et al : acquired egfr c797s mutation mediates resistance to azd9291 in non - small cell lung cancer harboring egfr t790m . nat med 21 : 560 - 562 , 2015 10 . 
niederst mj , hu h , mulvey he , et al : the allelic context of the c797s mutation acquired upon treatment with third - generation egfr inhibitors impacts sensitivity to subsequent treatment strategies . 
rolfo c , mack pc , scagliotti gv , et al : liquid biopsy for advanced non - small cell lung cancer ( nsclc ) : a statement paper from the iaslc . 
tan dsw , yom ss , tsao ms , et al : the international association for the study of lung cancer consensus statement on optimizing management of egfr mutation - positive non - small cell lung cancer : status in 2016 . 
j thorac oncol 11 : 946 - 963 , 2016 jukna a , montanari g , mengoli mc , et al : squamous cell carcinoma transformation concurrent with secondary t790m mutation in resistant egfr - mutated adenocarcinomas . 
yu ha , arcila me , rekhtman n , et al : analysis of tumor specimens at the time of acquired resistance to egfr - tki therapy in 155 patients with egfr - mutant 75ra26 , 2011 lung cancers . 
oxnard gr , hu y , mileham kf , et al : assessment of resistance mechanisms and clinical implications in patients with egfr t790m - positive lung cancer and acquired resistance to osimertinib . 
yang z , yang n , ou q , et al : investigating novel resistance mechanisms to third - generation egfr tyrosine kinase inhibitor osimertinib in non - small cell lung cancer patients . 
leone a : c797s and t790m egfr mutations in non - small cell lung cancer : in trans or in separate clones ? j thorac oncol 13 : e21 - e22 , 2018 19 . 
wang z , yang j - j , huang j , et al : lung adenocarcinoma harboring egfr t790m and in trans c797s responds to combination therapy of rstand thirdgeneration egfr tkis and shifts allelic conguration at resistance . 
zhou z , zhao y , shen s et al : durable clinical response of lung adenocarcinoma harboring egfr 19del / t790m / in trans - c797s to combination therapy of rstand third - generation egfr tkis . 
minari r , bordi p , del re m , et al : primary resistance to osimertinib due to sclc transformation : issue of t790m determination on liquid re - biopsy . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a third - generation egfr inhibitor . 
marcoux n , gettinger sn , okane g , et al : egfr - mutant adenocarcinomas that transform to small - cell lung cancer and other neuroendocrine carcinomas : clinical outcomes . 
the patient experienced progression on trametinib 0.5 mg per day , which is 25% of the clinically recommended dose and a dose likely insufficient to inhibit erk signaling . a previous publication2 and our experiences in the clinic suggest that pulsatile dosing may maintain the mek inhibitor dose to inhibit erk signaling sufficiently in the tumor and allow normal tissues to recover from toxic effects . 
in addition , preclinical data with raf inhibitors in melanoma models suggest that intermittent treatment may extend the period of response and forestall the development of lethal drug - resistant disease.3 we have treated two patients with colorectal tumors with the triplet combination of raf , mek , and egfr inhibitors who experienced dose - limiting drug toxicity attributable to mek inhibitors and continued to have difficulty tolerating treatment despite a reduction of one dose level . 
one patient had a partial response to vemurafenib , cobimetinib , and cetuximab lasting 16 months while taking cobimetinib on a dose schedule of 40 mg once per day , with 1 week on and 3 weeks off , as a result of grade 2 myalgias and grade 3 creatine phosphokinase elevations ( creatine phosphokinase > 1 , 000 iu / l ) ; the reduction of the cobimetinib dose to 40 mg occurred 2 weeks after initiation of treatment . 
the other patient has had ongoing stable disease for 12 months on dabrafenib , trametinib , and panitumumab , with a trametinib dose of 1 mg once daily , with 4 days on and 3 days off , as a result of intolerable , grade 2 acneiform rash ; the dose modification of the mek inhibitor occurred 4 weeks after the initiation of treatment . 
 one of our patients with melanoma treated from the start with an intermittent schedule of both dabrafenib and trametinib continues treatment after 3 years with dabrafenib 150 mg twice per day ( 2 weeks on and 2 weeks off ) and trametinib 8 mg once per day for the first 3 days of every other 4 - week cycle ; this patient has tolerated treatment well and experienced a sustained complete response of his tumor . 
kim kb , semrad r , schrock ab , et al : significant clinical response to a mek inhibitor therapy in a patient with metastatic melanoma harboring an raf1 fusion . 
 exceptional response to 177lutetium prostate - specic membrane antigen in prostate cancer harboring dna repair defects megan crumbaker , mbbs1 , 2 , 3 ; louise emmett1 , 3 ; lisa g . 
psma - targeted small molecules bound to 177lutetium ( 177lu ) , a medium - energy b - emitter , have been administered as a targeted therapy for metastatic prostate cancer ; the psma - targeted small molecule binds to psma on the cancer cell surface and is internalized , leading to delivery of a potent but targeted dose of radiation to the cell . 
a small molecule commonly used for this purpose is psma - 617 , a human psma - targeting ligand that can be conjugated to 177lu . 177lupsma - 617 therapy has shown great promise in early - phase trials , with a prostate - specic antigen ( psa ) response rate of 57% in a phase ii prospective study , 1 and randomized trials are currently recruiting internationally . de novo and acquired resistance are common , however , and biomarkers are needed to guide patient selection and rationalize combinatorial approaches . 177lupsma - 617 induces cell death through doublestrand dna breaks.2 mechanisms to repair doublestrand dna breaks are decient or absent in cells with mutations in homologous repair genes such as brca1 or brca2 , and such mutations are increasingly recognized in metastatic castration - resistant prostate cancer ( mcrpc ) .3 , 4 thus , a deciency in homologous repair may render a tumor more sensitive to 177lupsma - 617 and be relevant in crpc . 
postoperative radiotherapy was withheld because of a history of colorectal carcinoma treated with surgical resection followed by adjuvant radiotherapy 25 years prior . soon after his radical prostatectomy , he biochemically relapsed and was treated with intermittent androgen deprivation therapy . 
he eventually developed overt metastatic disease , with a perihilar mass found on a computed tomography ( ct ) scan of the chest , abdomen , and pelvis after 10 years of hormone manipulation . a nuclear medicine bone scan was negative , but an 18f - labeled uorodeoxyglucose positron emission tomography ( pet ) scan showed low - grade uptake in the mass , which was conrmed to be metastatic prostate cancer on biopsy . 
a choline pet was undertaken to assess the extent of his disease and revealed uptake in his left hilar nodes with inltration in the lingula and involvement of right paratracheal nodes . given the extent of disease across both hemithoraces , he commenced enzalutamide . 
his psa continued to increase ( fig 1 ) despite 8 weeks of treatment , and additional radiologic progression with impending bronchial obstruction prompted radiotherapy to his hilar disease . his psa initially decreased after radiotherapy but began to increase soon after . 
he then received two cycles of cabazitaxel , after which a restaging ct scan showed enlargement of his liver metastases and development of new pelvic nodal metastases . having progressed through all standard lines of therapy , this patient was enrolled in a clinical trial of 177lupsma - 617 therapy and received 4 6.5 gigabecquerel doses once every 6 weeks ( anzctr identier : actrn12615000912583 )  . 
plot of prostate - specic antigen ( psa ) values over time . treatment regimens : cabazi , cabazitaxel ; doce , docetaxel ; enz , enzalutamide ; lupsma , 177lutetium prostate - specic membrane antigen ; rt , radiotherapy . time ( months ) the return of his right upper quadrant abdominal pahe was consented for prescreening of his circulating tumor dna ( ctdna ) for a poly adp - ribose polymerase ( parp ) inhibitor trial , but while awaiting this result , his pain increased signicantly , with derangement of his liver function tests and a further increase in his psa . 
he was approved for an additional two compassionate 7.0 - gigabecquerel doses of 177lupsma - 617 ; he received these with clinical and radiologic responses associated with a psa response from 169 to 43 after the rst dose . a resolution bioscience targeted ctdna analysis for dna repair defects revealed abnormalities in three homologous fig 2 . 
to assess his germline , we performed targeted sequencing of coding regions and splice sites of atm , brca1 , brca2 , brip1 , cdh1 , cdkn2a , chek2 , hoxb13 , palb2 , pten , rad51c , rad51d , stk11 , and tp53 on dna extracted from blood ; this conrmed a frameshift mutation in exon 11 of the brca2 gene . 
up - front resistance and early relapses are common , however , signifying the need for strategies to improve patient selection and / or test rational combination approaches . as a form of ionizing radiation , 177lupsma - 617 induces double - strand dna breaks , which are believed to be the main lethal event in most exposed cells . 
preclinical and clinical studies have identied an association between cancers with homologous recombination defects and increased radiation sensitivity.8 germline mutations in genes that encode and mediate key enzymes for dna repair pathways , such as brca2 and atm , occur in approximately 11.8% of men with metastatic prostate cancer and somatic mutations in at least 23% of patients with mcrpc , 3 , 4 rendering many prostate cancers homologous recombination decient . homologous recombination deciency has been associated with responses to parp inhibition and platinum - based chemotherapy , 9 , 10 but these treatments may cause signicant toxicity . this patients germline mutation likely predisposed him to more aggressive disease , 11 and he was resistant to not only enzalutamide but also two lines of taxane - based chemotherapy . 
after his 177lupsma - 617 treatment , he also responded to carboplatin chemotherapy and a parp inhibitor . is biologically plausible that this gentlemans aberrations in homologous repair pathways enhanced his susceptibility to the radiation effects of 177lupsma - 617 therapy . 
we hypothesize that patients with mutations in dna repair pathway genes would be especially responsive to peptide receptor radionuclide therapy because of their inability to overcome dna breaks induced by the treatment . 
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eur urol 73 : 656 - 661 , 2018 emmett l , willowson k , violet j , et al : lutetium 177 psma radionuclide therapy for men with prostate cancer : a review of the current literature and discussion of practical aspects of therapy . 
pomerantz mm , spis ak s , jia l , et al : the association between germline brca2 variants and sensitivity to platinum - based chemotherapy among men with 11 . 
castro e , goh c , olmos d , et al : germline brca mutations are associated with higher risk of nodal involvement , distant metastasis , and poor survival outcomes metastatic prostate cancer . 
 s use of real - world data for the research , development , and evaluation of oncology precision medicines although randomized controlled trials remain the scientific ideal for determining the efficacy and safety of new treatments , they are sometimes insufficient to address the evidentiary requirements of regulators and payers . 
this is particularly the case when it comes to precision medicines because trials are often small , deliver incomplete insights into outcomes of most interest to policymakers ( eg , overall survival ) , and may fail to address other complex diagnostic and treatment - related questions . 
a number of modified earlyand latephase trial designs have been proposed to better support earlier biomarker validation , patient identification , and selection for regulatory studies , but there is still a need for confirmatory evidence from real - world data sources . 
these data are usually provided through observational , postapproval , phase iiib and iv studies , which rely heavily on registries and other electronic data setsmost notably data from electronic health records . 
notable examples include imatinib for the treatment of chronic myeloid leukemia , gefitinib for egfr mutationpositive nonsmall - cell lung cancer , and olaparib for patients with germline brca mutationpositive ovarian cancer . however , it is not always easy to assess the impact of new targeted cancer medicines and determine what , if any , benefit they have over existing therapies.1 - 3 table 1 lists some of the challenges of generating evidence in precision oncology . in part , this difficulty is because the types of large randomized trials that have successfully generated evidence to support blockbuster drugs are not well suited to generating evidence about targeted therapies . 
this raises a number of significant challenges to the generation and assessment of evidence . first , simply by virtue of their size , trials of precision medicines frequently do not generate the kind of evidence about overall survival that regulators and payers may demand.3 the difficulty in assessing overall survival is exacerbated by the ethical imperative to allow crossover among biomarker - positive patients , particularly when targeted agents are being assessed as alternatives to more toxic chemotherapy treatments . these challenges were evident in phase iii studies of imatinib in chronic myeloid leukemia , 4 of gefitinib5 and erlotinib6 in nonsmall - cell lung cancer , and more recently , of olaparib in advanced breast cancer in women with a known germline brca1 or brca2 gene mutation.7 the olaparib study , which recently reported improved progression - free survival with olaparib compared with chemotherapy , has thus far been unable to demonstrate an overall survival advantage . 
although this may be because such an advantage does not exist , it may also be because of crossover of patients receiving chemotherapy to olaparib , both during active monitoring and after completion of the study . 
challenges of generating evidence in precision oncology challenges small and geographically spread study populations ethical imperative to allow crossover within studies epidemiologic characterization of biomarker - defined populations evolution of disease biology leading to changes in molecular targets complexity , resource intensity , and cost of studies , particularly with adaptive trial designs failure to capture some clinically significant outcome measures need to simultaneously evaluate companion diagnostics conduct of studies only in high - income / resource - rich settings and countries unclear generalizability of data from study to target populations introduced by investigator behaviors ( eg , more frequently approaching patients with family histories or disease characteristics with known links to a biomarker ) may obscure their true prevalence and distribution . 
furthermore , more detailed knowledge about the true distribution of biomarkers by age , sex , response to prior therapies , geographies , and ethnicity is similarly difficult to obtain if the only data generated comes from screening limited numbers of patients as part of enrollment onto a single or small number of randomized controlled trials . closely aligned with this challenge is that of simultaneously assessing companion diagnostics that will eventually be used for the identification of biomarker - positive patients . 
adaptive trials may , for example , assign patients to randomly selected initial treatment groups , followed by additional testing for relevant biomarkers and appropriate stratification over the course of a trial.18 the advantages of these adaptive methods is that they can accommodate emerging information about biomarkers , changes in disease biology , and different patterns of treatment responsiveness among subsets of patients.19 two examples of adaptive studies that have been used in the develinclude the opment of precision medicines biomarker - integrated approaches of targeted therapy for lung cancer elimination ( battle ) trial , a nonsmall - cell lung cancer umbrella trial with four phase ii protocols , and i - spy2 , a breast cancer trial comparing novel drugs in combination with standard chemotherapy to standard therapy alone . and small size of trials of precision medicines may also make it more difficult to detect infrequent but serious adverse effects.8 second , although all trials face problems of generalizability ( as a result of , for example , the limited size of trial populations , effects of selection criteria , close monitoring of compliance , and frequency of clinical monitoring ) , 9 trials of targeted cancer therapies raise additional issues because patients enrolled onto such trials may be selected on the basis of biomarkers that are not routinely used in clinical practice . 
furthermore , because trials of precision medicines are expensive , sponsors may frequently choose to recruit the smallest numbers of patients required to deliver a statistically significant result , raising additional questions about the clinical significance of trial results.10 third , as in any trial , the statistical power assigned secondary end points is often considerably less than that given to primary objectives . 
this is exacerbated when secondary end points are used in trials of precision medicines because of their size , their complexity ( eg , allowing crossover ) , and the impact of both known and unknown differences between study and real - world populations . 
in the absence of postapproval follow - up studies involving large numbers of patients , drug labels are likely to be highly restricted . finally , even if a targeted therapy can be shown to be sufficiently efficacious and safe in a small trial , it can be extremely difficult to determine which patients should subsequently be screened for biomarkers and potentially offered treatment . 
 however , adaptive trials are methodologically and logistically complex and rely upon close collaboration between clinician - researchers and industry across multiple sites and geographic regions.20 they also do not address the full range of challenges associated with evidence development in precision medicine . 
in this context , physicians often prescribe medicines off - label ( ie , for indications other than those approved by the regulator ) or seek individual patient access to unregistered medicines on compassionate grounds , particularly when these seem promising based on phase i and ii studies . the problem with using off - label prescribing and patient - by - patient compassionate access as means of providing access to new medicines is that they tend to be ad hoc , inequitable , and driven more by compassion and desperation than by evidence . 
in an effort to overcome these problems , numerous formal approaches to accelerated access have been developed around the world ( eg , by the fda , the european medicines agency , health canada , and singapores health sciences authority ) .24 these programs both speed up access and enable approval based on limited data . 
examples of cancer medicines that have recently been approved in the united states on the basis of phase ii data include olaparib , in 2014 , for the management of metastatic ovarian cancer and brigatinib , in 2017 , for patients with nonsmall - cell lung cancer who have experienced progression after initially responding to crizotinib , which was itself approved via accelerated approval in 2011.25 the difficulty with accelerated access programs is that they generally mitigate against the collection of high - quality , standardized data , in part because there is no financial incentive on the part of industry and clinicians to generate additional data once a medicine is on the market and in part because patients are unwilling to enroll onto phase iii trials when they have other , guaranteed means of access and ongoing supply.10 in the long run , this creates sustained uncertainties and may place patients at risk ; we know that medicines approved through accelerated access schemes are more likely to have health warnings related to unanticipated toxicities and more likely to be subsequently withdrawn.26 , 27 accelerated access may also encourage more widespread off - label prescribing , as in the case of vemurafenib , a kinase inhibitor indicated for the treatment of metastatic melanoma with activating braf v600e mutation , which has been used off - label for refractory braf v600e mutation positive hairy cell leukemia in the absence of formal phase iii studies of its use for this indication.28 given the challenges associated with accelerated access , regulators and funders often request additional evidence of safety and / or effectiveness after registration or subsidization . 
these enable approval subject to ongoing data collection and , ideally , review of registration and subsidization decisions based on these data.2 evidence to support accelerated access and managed entry schemes may be generated through controlled trials , cohort studies , registries , and the like , all of which depend to a significant degree on the ongoing collection of clinical data regarding patient outcomes using real - world data ( rwd ) sources . 
in part , this is because they contain a vast array of different types of data including quantitative data ( eg , laboratory values ) , qualitative data ( eg , text - based documents and demographics ) , and transactional data ( eg , records of medication delivery ) , 29 all of which can be repurposed for clinical and health services research . 
 databases , pharmacies , insurance claims , disease registries , bio - repositories , public health databases , census records , and social media , which can be additional sources of data . importantly , data from ehrs may be used to assess whether the results of randomized controlled trials are generalizable to real - world populations who may differ in many ways from study populations ( eg , according to age , comorbidity , concurrent therapies ) 30 ; may identify other factors that modify clinical outcomes , including treatment availability and clinician preferences ; and may reveal patterns in treatment responsiveness and adverse effects.31 , 32 furthermore , large volumes of electronic clinical information may offer insights into potential new indications for drugs.33 in addition , where linked bio - specimens are available , data from ehrs may help to characterize genotype - phenotype associations.34 if , for example , one wished to gain a greater understanding of the efficacy and safety of poly ( adp - ribose ) polymerase inhibitors in women with breast cancer , one could ask how and when olaparib might be used with routinely available treatments , such as tamoxifen in the management of hormone receptor and brca gene mutationpositive breast cancer , or whether comorbidities that typically exclude patients from participating in regulatory phase iii clinical trials , such as liver or renal impairment , really do influence the clinical effectiveness of treatment or increase toxicities . recognition of the importance of rwd in general , and ehrs in particular , is evident in recent initiatives such as the asco - sponsored cancerlinq and the international registry to improve outcomes in men with advanced prostate cancer ( ironman )  . the asco 2017 report on the state of oncology practice in the united states , for example , notes that : learning health care systems that are based on big sets of routine clinical practice data offer great potential for improving both patient care and research , and the benefits of these systems may have particular importance for cancer care . 
the fda appears to have taken this on board , with asco recently announcing : under the new collaboration , fda plans to use cancerlinqs repository of real - world evidence on patient treatment and outcomes to track how genomically targeted drugs and newer immunotherapies are used in clinical practice , comparing their impact to what has been seen in clinical trials , and tracing their use by physicians either according to , or in spite of , their labelling information.37 enthusiasm for rwd has led numerousprofessional , commercial , and not - for - profit organizations38 - 45 to develop expertise in the collection , linkage , and use of rwd to support cancer research , and there are now examples of cancer studies that have used rwd to understand biomarker prevalence and influence on clinical outcomes , 46 - 48 validate standards of care , 49 assess the generalizability of randomized controlled trial outcomes , 50 and conduct comparative effectiveness research.51 however , despite the promise of using rwd to support research , there are considerable epistemic , social , and ethical challenges to its effective and responsible use . 
potential opportunities and challenges associated with the use of ehr - generated real - world data identification of clinically relevant study compatibility of ehr platforms for data populations exchange potential opportunity access to large populations , including via linkage of ehrs to administrative and research data sets inclusion of patients usually excluded from rcts ( eg , older patients , patients with hepatic impairment ) identification and accurate determination of biomarker prevalence among patient ( as opposed to study ) populations ability to account for differing treatment lines and sequences of therapies ability to collect outcome data relating to standard - of - care treatments not selected as comparators in rcts ability to quantify survival impact that may be obscured by crossover , either within clinical trials or after poststudy exposure to an investigational agent potential for long - term follow - up challenges data quality and compatibility issues , including accuracy , completeness , clarity , provenance , detail , and consistency in methods of measurement generation and harmonization of standards for data collection and analytical methodologies funding and resources for establishment , maintenance , and use of ehrs systematic exclusion of countries and settings that lack ehr systems data custodianship and patient privacy consent to secondary use in research of clinical data acceptance of data and methodologies among professional groups , regulators , and payers abbreviations : ehr , electronic health record ; rct , randomized controlled trial . defined rwd , can be challenging because , although data might be more complete and fit for purpose , the very process of controlling and cleaning data sets can compromise the authenticity and applicability of the research.66 , 67 although there is no doubt that it would help to build consensus about methods of data collection , curation , and analysis , 45 it may never be possible to completely standardize rwd because requirements for each study may be profoundly different and it is impossible to predict the data requirements for every potential study . 
different interventions will require specific and disparate evidence needs and thus demand the collection of different types of data , and each may require unique study protocols , clinical report forms , participant information and consent forms , and so on . 
standardization is also challenged by the nuances and complexity of multidisciplinary cancer management.68 for these reasons , asco has supported development of a framework for oncology data exchange based on a document markup standard known as high level 7 clinical document architecture ( hl7 cda )  . 
the position that has underpinned research ethics for more than 50 years is that consent from patients is required for research of any kind , and lawmakers and health care service providers generally hold the same views . 
the issues in relation to rwd are whether , and to what extent , patients should have control over information about their health care and whether accessing information without consent would constitute a breach of privacy . 
although autonomy is highly valued , the need to obtain explicit patient consent for the use of routine clinical data can be resource intensive and lead to biases as a result of differences between consenters and nonconsenters , 89 including those related to sex , socioeconomic status , or health status.90 this is particularly relevant where studies seek to assess the survival of a particular group of patients for future comparison with newer treatments in similar clinical settings . assessment of survival is likely to be further confounded if data can only be collected from living patients . 
this public opinion seems to support the view that respect for autonomy and privacy is not absolute and that public benefit is important enough and institutions are trustworthy enough to allow individuals health - related data to be used in specific situations either without consent or with broad consent . 
a study conducted after the establishment of the united kingdom national cancer registry , for example , suggested that the public does not necessarily consider the confidential use of personal information for public health research and surveillance to be an invasion of privacy.91 other studies have demonstrated public support for data linkage , with the caveat of adequate measures being in place to protect privacy.92 new policies and guidelines for researchers and human ethics committees are providing direction on whether consent is required before the use of rwd for research . 
in general , the need for consent depends on the level of risk to patients privacy , whether data can be anonymized , and the reason provided for analyzing patient data . 
additional considerations include practical difficulties associated with obtaining consent , the epidemiologic necessity for comprehensive data , the importance of the research ( public interest ) , and whether the researchers wanting access to data have commercial interests ( in most cases , waivers of consent do not apply when commercial entities seek access to data )  . it is also generally accepted that where consent cannot be waived , open - ended ( as distinct from repeated , project - specific ) consent is sufficient.93 importantly , consent may be sought not simply for use by a single researcher or research group but also for data sharing with additional researchers or research networks concurrently or in the future . research that encompasses long - term storage and recurring use of personal data will thus inevitably raise issues about access , including access by commercial entities and those located internationally.76 , 94 , 95 the issue here is that those who collect data lose control and may have to relinquish custodianship altogether . 
the sharing of data also brings to the fore questions about the degree of personal control people should have over their data and how this control should be realized.95 - 100 innovative models of consent , such as dynamic consent , supported by web - based information technologies , may help to facilitate the use of information from ehrs in ways that provide a range of ethical safeguards . 
 are being considered include open consent ( obtained once from consenters for all future research uses of genetic and other data ) , meta consent ( for use of retrospective and prospective data after being informed about the types of research these data might be used to conduct ) , and portable legal consent ( a system through which users can donate their data to databases that remove identifying details , such as name and e - mail address ) .77 , 87 , 88 , 101 , 102 more effective and efficient data linkage and networking of databases and information from other sources ( eg , biobanks , registries , and clinical trials ) , along with greater regulatory harmonization , may also improve processes for using rwd in the development of precision medicines . 
existing processes for regulatory oversight might be complemented by the establishment of independent authorities with appropriate legal , scientific , and technical expertise who could work as coordinators , receivers , and custodians of rwd . maintaining patient confidentiality and privacy the size , complexity , possible linkage , long - term storage , and potential commercialization of ehrgenerated data add significant complexity to efforts to ensure confidentiality of health - related information . 
lewis data analysis and interpretation : all authors manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors to the research question being asked but might have clinical significance for the research participant . 
the dilemma here is that , although informing participants of such findings might enable them to prevent or respond more rapidly to disease , the clinical significance of findings is not always obvious . 
the problem with promising to return individual results is that their clinical significance is often unclear , the clinical validity of findings generated in research laboratories is often uncertain , and people might not want to receive such information no matter how clinically significant it might be . 
regulators and payers have begun to acknowledge the need to establish new ways of generating and evaluating evidence , 110 and systems have developed to facilitate alternative , including real - world , methods of data collection and evidence generation . 
although these methods have the potential to transform hospitals and health care systems into learning health care systems , they raise their own technical , scientific , organizational , economic , ethical , and legal issues . 
lewis employment : astrazeneca ian kerridge no relationship to disclose wendy lipworth employment : msd animal health ( i ) affiliations all authors : sydney health ethics , university of sydney , sydney , new south wales , australia . references lewis j , lipworth w , kerridge i : ethics , evidence and economics in the pursuit of personalized medicine . 
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lewis jrr , lipworth w , kerridge i , et al : dilemmas in the compassionate supply of investigational cancer drugs . intern med j 44 : 841 - 845 , 2014 23 . 
alsop k , fereday s , meldrum c , et al : brca mutation frequency and patterns of treatment response in brca mutation - positive women with ovarian cancer : a report from the australian ovarian cancer study group . 
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abbing - karahagopian v , kurz x , de vries f , et al : bridging differences in outcomes of pharmacoepidemiological studies : design and first results of the protect project . 
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coloma pm , schuemie mj , trifir `o g , et al : combining electronic healthcare databases in europe to allow for largescale drug safety monitoring : the eu - adr project . 
suissa s , henry d , caetano p , et al : cnodes : the canadian network for observational drug effect studies . open med 6 : e134 - e140 , 2012 45 . 
garrison lp jr , neumann pj , erickson p , et al : using real - world data for coverage and payment decisions : the ispor real - world data task force report . 
wang li , shewade a , lambert p , et al : characteristics of advanced non - small cell lung cancer ( ansclc ) patients ( pts ) receiving molecular diagnostic ( md ) testing in us routine clinical practice . 
he ky , zhao y , mcpherson ew , et al : pathogenic mutations in cancer - predisposing genes : a survey of 300 patients with whole - genome sequencing and lifetime electronic health records . 
feinberg ba , kish jk , garofalo d , et al : evaluation of real - world electronic medical record ( emr ) treatment outcome data compared to clinical trial data for an advanced breast cancer treatment . 
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n engl j med 370 : 2161 - 2163 , 2014 van staa t - p , dyson l , mccann g , et al : the opportunities and challenges of pragmatic point - of - care randomised trials using routinely collected electronic records : evaluations of two exemplar trials . 
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hemkens lg , contopoulos - ioannidis dg , ioannidis jpa : agreement of treatment effects for mortality from routinely collected data and subsequent randomized trials : meta - epidemiological survey . 
science 346 : 1054 - 1055 , 2014 ioannidis jpa , trikalinos ta : early extreme contradictory estimates may appear in published research : the proteus phenomenon in molecular genetics research and randomized trials . 
sboner a , mu xj , greenbaum d , et al : the real cost of sequencing : higher than you think ! genome biol 12 : 125 , 2011 75 . 
hill em , turner el , martin rm , et al : lets get the best quality research we can : public awareness and acceptance of consent to use existing data in health researcha systematic review and qualitative study . 
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makady a , ham rt , de boer a , et al : policies for use of real - world data in health technology assessment ( hta ) : a comparative study of six hta agencies . 
van gent , phd1 , 2 ; and agnes jager , md , phd3 purpose biomarkers that predict response to poly ( adp - ribose ) polymerase inhibitors ( parpis ) are required to detect parpi sensitivity beyond germline brca - mutated ( gbrcam ) cancers and parpi resistance among reverted gbrcam cancers . 
therefore , we previously developed the repair capacity ( recap ) test , a functional homologous recombination ( hr ) assay that exploits the formation of rad51 foci in proliferating cells after ex vivo irradiation of fresh primary breast cancer tissue . 
the aim of the current study was to validate the feasibility of this test on histologic biopsy specimens from metastatic breast cancer and to explore the utility of the recap test as a predictive tool for treatment with dna - damaging agents , such as parpis . methods fresh tissue biopsies from easily accessible metastatic lesions from patients with locally advanced or metastatic breast cancer were irradiated with 5 gy and cultured for 2 hours followed by detection of rad51 foci presence ( hr procient ) or absence ( hr decient [ hrd ] )  . 
although hrd was detected in 13 ( 32% ) of 41 specimens , only ve showed a gbrcain three patients with gbrcam , post - treatment recap tests showed hr phenotype reversion after in vivo progressive disease on platinum and parpi treatment , which was explained in one patient by a secondary brca1 mutation . conclusion the recap test , which reects real - time hr status regardless of brca mutations , is feasible in metastatic breast cancer biopsy specimens . 
2019 by american society of clinical oncology introduction tumors developed among germline brca1 / 2 mutation ( gbrcam ) carriers have a defect in homologous recombination ( hr ) and are therefore highly sensitive to poly ( adp - ribose ) polymerase inhibitors ( parpis ) and dna double - strand break ( dsb ) inducing chemotherapies.1 - 4 recently , food and drug administration approval was obtained for the use of olaparib in advanced gbrcam breast cancer.3 until now , gbrcam status is the only predictive biomarker for response to parpi therapy . 
however , evidence is emerging that parpis also are effective in cancers with hr deciency ( hrd ) caused by other mechanisms than gbrcam , such as somatic brca1 / 2 mutations or mutations of other hr genes.5 several different hrd tests have been designed to identify hrd tumors in addition to gbrcam tumors to enlarge the population of patients with breast cancer who could benet from treatments that target the hr pathway.6 - 10 however , a gold standard test for predicting response to parpi therapy is not yet available . 
most hrd tests are based on specic genomic or transcriptomic patterns derived from gbrcam tumors , which also occur in sporadic cancers ( brcaness ) .6 - 10 these tests measure the accumulation of mutations and chromosomal aberrations over time ; thus , they do not necessarily reect the real - time hr status of the tumor . 
 meijer et al context key objective to determine whether the repair capacity ( recap ) test is feasible in histologic biopsy specimens from metastatic breast cancer and to explore the predictive value of the recap test for double - strand break ( dsb ) inducing therapies . knowledge generated the recap test is feasible in metastatic biopsy specimens . 
although 13 ( 32% ) of 41 specimens were found to be homologous recombination ( hr ) decient , only ve had a germline brca mutation ( gbrcam )  . 
in three patients with gbrcam with progressive disease on dsb - inducing therapies , post - treatment recap tests showed hr status reversion , which was explained by a secondary brca1 mutation in one of these patients . relevance the recap test reects real - time hr status regardless of brca mutations . 
therefore , recap is expected to predict sensitivity to dsb - inducing treatment more precisely than germline mutation analysis only . proliferating cells after ex vivo irradiation of fresh breast cancer tissue , was developed previously for primary breast cancer ( n = 148 ) .12 , 13 in the current study , we aimed to show feasibility of this test on biopsy specimens from metastatic breast cancer lesions to enhance the diagnostic potential and clinical applicability of the recap test . 
next , we aimed to nd a molecular explanation for the observed hrd phenotype , and we explored the utility of the recap test as a predictive tool for treatment with dsb - inducing agents , such as parpis , in this setting . methods biopsy specimens patients with locally advanced or metastatic breast cancer with metastatic lesions amenable for biopsy and who were planned to start systemic treatment were eligible . 
patients with pulmonary and / or bone metastasis only were excluded because of the risk of pneumothorax and technical difculties with experimental procedures caused by calcications ( data supplement )  . 
patients were to have a bilirubin level less than 1.5 the upper limit of normal and both ast and alt levels less than ve times the upper limit of normal in case a liver biopsy was scheduled . 
platelets were to be greater than 100 109 / l and international normalize ratio less than 1.5 , unless platelet and international normalized ratio values were not necessary according to local protocols or after consent of the interventional radiologist for that particular biopsy site ( eg , breast )  . 
after registration and written informed consent , each patient was scheduled for a biopsy performed by a ( interventional ) radiologist according to local protocols . for distant metastases , a core needle biopsy with a minimum of an 18 - gauge and maximum of a 12 - gauge needle was performed under imaging guidance . 
in brief , presence of rad51 foci was determined in geminin ( gmn ) positive , least 30 gmn - expressing cells were counted per tumor sample . a cell was considered rad51 positive when at least ve rad51 foci were detected . 
tumors were classied as hr procient ( hrp ) , hrd , or hr intermediate ( hri ) when more than 50% , less than 20% , or 20% to 50% of gmnpositive cells showed ve or more rad51 foci , respectively . thus actively proliferating , cells only . 
at brca1 / 2 analyses and rad51 assay on cell lines see data supplement . statistical analysis the aim of the study was to show feasibility of the recap test on biopsy specimens from metastatic breast cancer . the primary end point was the proportion of patients with metastatic breast cancer with a successful recap test result . 
in total , 47 biopsy specimens were obtained from 44 patients , of which three did not contain tumor cells , resulting in 44 representative specimens . the recap test could be performed successfully in 41 ( 93% ; 95% ci , 86% to 100% ) of the 44 biopsied metastatic lesions ( p , .001 ; fig 1a )  . 
the reason for unsuccessful testing in three biopsy specimens was an insufcient number of proliferating ( ie , gmn - positive ) tumor cells ( fewer than 30 gmn - positive in m189 , m250 , and m332 )  . 
m250 and m332 contained six and 19 gmn - positive cells , respectively , of which all were rad51 positive . biopsy specimens were derived from several metastatic sites ( fig 1b )  . 
the recap test could be performed on core needle biopsy ( n = 37 ) as well as on punch biopsy ( n = 4 ) specimens of skin metastases . 
in 19 specimens ( four triplenegative breast cancer [ tnbc ] , four human epidermal growth factor receptor 2positive , and 11 estrogen receptor [ er ] / progesterone receptor positive ) , we determined whether standard er , progesterone receptor , and human epidermal growth factor receptor 2 immunohistochemistry analyses could be performed on the recap biopsy specimen . 
in one specimen , which was originally scored as tnbc , we found a 10% er expression in the recap specimen , which is just above the threshold for er positivity ( ie , greater than or equal to 10% in the netherlands )  . among the 41 successful recap test results , we identied 13 hrd , two hri , and 26 hrp tumor samples ( fig 1 )  . recap status was independent of histopathologic characteristics of the tumors , biopsy type , and localization of the metastatic lesion ( data supplement )  . molecular defects in hrd tumors the 13 hrd tumors were analyzed further to nd a molecular explanation for the observed hrd phenotype ( table 1 )  . 
five ( 38% ) of 13 of hrd tumors harbored gbrcam of which one harbored a brca2 variant of unknown signicance that was functionally validated for affecting hr.14 in two hrd tumors ( 15% ) , somatic brca2 variants of unknown signicance were found , which are predicted to be nonpathogenic . 
brca1 promotor hypermethylation was identied in one hrd tumor , and brca1 rna was indeed absent in this tumor as assessed by rna in situ hybridization ( data supplement )  . 
thus , the hrd phenotype was explained by a brca defect in six tumors ( 46% ) , which left seven ( 54% ) of the 13 hrd tumors to be non - brca related . 
one non - brcarelated hrd tumor harbored a germline mutation in palb2 . change of hrd phenotype in response to dsb - inducing therapy next , we explored the added value of the recap test as a predictive biomarker to select patients for parpi treatment in the metastatic setting . 
the patient was treated consecutively with capecitabine , carboplatin and gemcitabine , and low - dose cisplatin in combination with nivolumab , on which she developed pd after six cycles . 
the second specimen was very heterogeneous , harboring both hrd ( rad51 - negative ) and hrp ( rad51 - positive ) cells , which overall resulted in an hri phenotype . 
 hrd reversal after dna damaging chemotherapy patient 1 : brca2 vus 06 - 2014 primary brc 12 - 2014 lumpectomy 02 - 2016 07 - 2016 12 - 2016 02 - 2017 11 - 2015 mastitis carcinomatosa / metastasis 4x ddac 12x paclitaxel capecitabine carboplatin + gemcitabine 2x cisplatin + 6x nivolumab olaparib biopsy m222 rad51 negative biopsy m298 rad51 intermediate patient 2 : brca1 mutation 03 - 2014 primary brc lumpectomy 03 - 2016 locoregional recurrence 02 - 2017 04 - 2017 3x fec 3x docetaxel carboplatin + paclitaxel and veliparib capecitabine biopsy m242 rad51 negative biopsy m303 rad51 positive patient 3 : brca2 mutation 05 - 2007 primary brc ablation 05 - 2013 bone metastases 04 - 2015 01 - 2016 03 - 2017 5x fec + tamoxifen 3x fac + anastrozol tamoxifen carboplatin + paclitaxel and veliparib biopsy m234 rad51 negative biopsy m319 rad51 positive m222 m242 m234 pretreatment post - treatment dapi geminin rad51 overlay dapi geminin rad51 overlay m298 15 m m303 m319 10 m fig 2 . 
 ( a ) an additional point mutation ( ofcially , 4327_ 4329delinstgg ) was acquired next to the original 4327c.t mutation , which resulted in restoration of the open reading frame disrupted by the original mutation and , consequently , full - length brca1 protein production . 
 ( b ) fluorescence in situ hybridization analysis showed that both preand posttreatment biopsy specimens harbored two copies of brca1 , which indicates that the original mutated allele was duplicated . 
of note , both tumors developed an hrp phenotype after they had developed resistance in response to the combination of carboplatin , paclitaxel , and veliparib ( parpi ) within a clinical trial . 
these three patients had been previously treated with anthracycline - based therapy , which also induces dsb but did not lead to hr phenotype reversion . preand post - treatment biopsy specimens , loss of heterozygosity was observed . 
fluorescence in situ hybridization analysis showed that both preand post - treatment specimens harbored two copies of brca1 , which indicates that the original mutated allele was duplicated ( fig 3b )  . thus , the tumor became hrp as a result of reversion of one mutant brca1 copy . to unravel the molecular mechanisms that lead to resistance in these patients , we searched for secondary brca1 / 2 mutations in the post - treatment tumor biopsy specimens . 
patient 2 acquired an additional point mutation , that is , 4329a.g ( ofcially , 4327_4329delinstgg ) next to the original 4327c.t mutation , which resulted in restoration of the open reading frame disrupted by the original mutation and , consequently , full - length brca1 protein production ( fig 3a )  . 
other mechanisms for parpi resistance have been proposed , such as loss of 53bp1 proteloss of 53bp1 was examined but not found in any resistant tumor ( data supplement )  . 
brc , breast cancer ; dapi , 4 ( cid : 2 ) , 6 - diamidino - 2 - phenylindole ; edu , 5 - ethynyl - 2 ( cid : 2 ) deoxyuridine ; fac , uorouracil , doxorubicin , and cyclophosphamide ; ir , irradiated ; loh , loss of heterozygosity ; pd , progressive disease . 20 m when this patient showed pd after 5 months of carboplatin treatment ; however , pretreatment hr and paclitaxel status remains unknown because a fresh pretreatment biopsy specimen was not available for this patient ( fig 4 )  . 
because this tumor might have developed reversal of the hrd phenotype , both preand posttreatment tumor material ( 70% tumor ) were sequenced . the germline brca2 mutation was present at an maf of 41% and 34% , respectively , and secondary mutations were not present . 
 meijer et al brca2 mutation suggested that the brca2 wild - type allele was still present in the tumor , which was conrmed by uorescence in situ hybridization ( fig 4b )  . 
chek2 is a known breast cancer susceptibility gene , but the direct effect of chek2 mutations on hr status remains elusive . therefore , the hr status of sum102pt cells , which harbor the exact same c.1100delc mutation in chek2 as found in this patient , was determined , and the chek2 c.1100delc mutation did not cause hrd ( fig 4d )  . 
she showed pd after the rst response evaluation at 8 weeks , which corresponded to the outcome of the recap test ( hrp ; fig 4a )  . discussion this study shows that the recap test is feasible ( 93% successful ) in metastatic breast cancer biopsy specimens , which greatly enhances its diagnostic potential and clinical applicability . 
the functional recap test is robust , and its applicability extends from core needle biopsy specimens of different metastatic sites to punch biopsy specimens of skin metastases , and test results are available within 1 week . hrd was detected in 13 ( 32% ) of 41 tumors . 
among 13 hrd tumors , only ve showed a gbrcam , which indicates that the recap test may identify twice as many candidates for parpi treatment as gbrca analysis . we believe that this study provides the rst evidence that the hr phenotype , measured by a functional hr test , changes over time in patients with gbrcam as a result of previous therapies . 
within the current cohort , reversion of the hr phenotype was detected in three patients with gbrcam tumors after developing in vivo resistance to dsb - inducing therapies ( carboplatin and cisplatin or parpi )  . 
another gbrcam patient with a brca - procient tumor showed resistance to dsb - inducing agents and was refractory to olaparib , a nding concordant with the result of the recap test ( hrp )  . 
these ndings highlight the need for hr tests that are based on the phenotype , such as the recap test , especially in the advanced setting . the molecular mechanism that leads to resistance and reversion of the hrd phenotype was explained in one of three patients by a secondary mutation in brca1 . 
this is unique because for breast cancer , most reversion mutations are described within brca2 , and a brca1 reversion has been described only once before.15 the incidence of brca1 / 2 secondary mutations within resistant tumors is not yet clear because most are described in case reports or studies with small sample sizes . 
in 26 patients who had platinum - resistant recurrent ovarian cancer , the incidence of brca1 / 2 secondary mutations was 46.2%.16 in two ( 40% ) of ve patients with gbrcam with platinum and parpi therapy - resistant metastatic breast cancer , secondary brca2 mutations were detected in circulating tumor dna.17 several case reports have highlighted that brca1 / 2 secondary mutations are a universal resistance mechanism for various tumor types ( eg , prostate , pancreatic ) with germline or somatic loss - of - function mutations.18 - 21 however , because not all resistant patients harbor secondary mutations , detection of parpi - resistant tumors by screening for secondary brca mutations would lead to an underestimation and only identify a subgroup of resistant tumors . 
the recap test , however , detects resistant tumors regardless of the exact underlying resistance mechanism . we show a case of coincidence of both germline brca2 and chek2 c.1100delc mutations in a patient with an hrp breast tumor . 
the driver mutation of this tumor was chek2 instead of brca2 , which highlights two important issues : first , breast cancer that arises in a patient with gbrcam is not necessarily brca associated , and second , the chek2 c.1100delc mutation does not cause hrd . 
furthermore , the recap test does not depend on high tumor percentage in a sample because the microscopic readout allows differentiation between tumor and stromal cells . another advantage is its broad applicability : where many hrd tests focus specically on tnbcs , the recap test detects hrd regardless of histologic grade and subtype . because recap procedures ( irradiation and 2 hours of inuence standard hormone receptor culturing ) do not analyses , the fresh biopsy specimen used for recap testing also could be used for diagnostic pathology analyses , which thereby limits the amount of tissue needed . 
first , functional testing requires fresh ( instead of parafn - embedded ) tumor specimens , and for the recap test in particular , ex vivo dna damage is induced by x - ray or gamma irradiation . 
 hrd reversal after dna damaging chemotherapy moreover , reversion of the hr phenotype is detected by recap , which identies patients with gbrcam who will no longer benet from parpi or dsb - inducing agents as a result of resistance . 
the functional recap test , which determines the real - time hr status independent of gbrcam status , shows great potential as a predictive biomarker for parpi treatment of metastatic breast cancers . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . hendrikus - jan dubbink consulting or advisory role : pzer , personal genome diagnostics research funding : astrazeneca winand n.m. 
dinjens consulting or advisory role : amgen , bristol - myers squibb , astrazeneca ( inst ) , roche no other potential conicts of interest were reported . acknowledgment we thank the medical oncologists of erasmus mc for informing patients about the trial and other activities that led to patient enrollment . 
hollestelle , phd , for providing the t47d , mm463 , and sum102pt cell lines . references audeh mw , carmichael j , penson rt , et al : oral poly ( adp - ribose ) polymerase inhibitor olaparib in patients with brca1 or brca2 mutations and recurrent ovarian cancer : a proof - of - concept trial . 
lancet 376 : 245 - 251 , 2010 ledermann j , harter p , gourley c , et al : olaparib maintenance therapy in patients with platinum - sensitive relapsed serous ovarian cancer : a preplanned retrospective analysis of outcomes by brca status in a randomised phase 2 trial . 
lancet oncol 15 : 852 - 861 , 2014 robson m , im sa , senkus e , et al : olaparib for metastatic breast cancer in patients with a germline brca mutation . 
n engl j med 377 : 523 - 533 , 2017 tutt a , robson m , garber je , et al : oral poly ( adp - ribose ) polymerase inhibitor olaparib in patients with brca1 or brca2 mutations and advanced breast cancer : a proof - of - concept trial . 
lancet 376 : 235 - 244 , 2010 den brok wd , shrader ka , sun s , et al : homologous recombination deciency in breast cancer : a clinical review . 
br j cancer 107 : 1776 - 1782 , 2012 birkbak nj , wang zc , kim jy , et al : telomeric allelic imbalance indicates defective dna repair and sensitivity to dna - damaging agents . 
cancer discov 2 : 366 - 375 , 2012 davies h , glodzik d , morganella s , et al : hrdetect is a predictor of brca1 and brca2 deciency based on mutational signatures . 
nat med 23 : 517 - 525 , 2017 joosse sa , van beers eh , tielen ih , et al : prediction of brca1 - association in hereditary non - brca1 / 2 breast carcinomas with array - cgh . 
konstantinopoulos pa , spentzos d , karlan by , et al : gene expression prole of brcaness that correlates with responsiveness to chemotherapy and with outcome in patients with epithelial ovarian cancer . 
j clin oncol 28 : 3555 - 3561 , 2010 incorvaia l , passiglia f , rizzo s , et al : back to a false normality : new intriguing mechanisms of resistance to parp inhibitors . 
afghahi a , timms km , vinayak s , et al : tumor brca1 reversion mutation arising during neoadjuvant platinum - based chemotherapy in triple - negative breast cancer is associated with therapy resistance . 
weigelt b , comino - m endez i , de bruijn i , et al : diverse brca1 and brca2 reversion mutations in circulating cell - free dna of therapy - resistant breast or ovarian j clin oncol 29 : 3008 - 3015 , 2011 cancer . 
carneiro ba , collier ka , nagy rj , et al : acquired resistance to poly ( adp - ribose ) polymerase inhibitor olaparib in brca2 - associated prostate cancer resulting from biallelic brca2 reversion mutations restores both germline and somatic loss - of - function mutations . 
cheng hh , salipante sj , nelson ps , et al : polyclonal brca2 reversion mutations detected in circulating tumor dna after platinum chemotherapy in a patient with metastatic prostate cancer . 
banda k , swisher em , wu d , et al : somatic reversion of germline brca2 mutation confers resistance to poly ( adp - ribose ) polymerase inhibitor therapy . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
zhu xd , k uster b , mann m , et al : cell - cycle - regulated association of rad50 / mre11 / nbs1 with trf2 and human telomeres . 
voss ( continued ) purpose with prospective clinical sequencing of tumors emerging as a mainstay in cancer care , an urgent need exists for a clinical support tool that distills the clinical implications associated with specific mutation events into a standardized and easily interpretable format . 
to this end , we developed oncokb , an expert - guided precision oncology knowledge base . methods oncokb annotates the biologic and oncogenic effects and prognostic and predictive significance of somatic molecular alterations . 
potential treatment implications are stratified by the level of evidence that a specific molecular alteration is predictive of drug response on the basis of us food and drug administration labeling , national comprehensive cancer network guidelines , disease - focused expert group recommendations , and scientific literature . results to date , > 3 , 000 unique mutations , fusions , and copy number alterations in 418 cancerassociated genes have been annotated . 
with the shift from single analyte tests and small hotspot panels to larger gene panels and whole - exome and - genome platforms , interpretation of the clinical significance of the increasing number of genomic alterations identified in individual tumors has become a challenge . 
a smaller subset are known or suspected functionally significant mutations with no clear therapeutic implications , and the smallest subset consists of known driver mutations that are clinically actionable . the information that discriminates whether an alteration is clinically actionable can reside in various silos , including us food and drug administration ( fda ) labeling , national comprehensive cancer network ( nccn ) guidelines , conference proceedings , disease - focused expert group recommendations , and the scientific literature . 
therefore , an urgent need exists for a clinical support tool that distills this information into a standardized and easily interpretable format that democratizes its access to clinicians of all knowledge levels and at all centers . 
to address these limitations , we describe oncokb , a comprehensive precision oncology knowledge base that offers oncologists detailed , evidence - based information about individual somatic mutations and structural alterations present in patient tumors to support optimal treatment decisions . 
oncokb content is supervised by a dedicated panel of physicians and cancer biologists who review and edit biomarker - associated investigational therapeutic strategies ( data supplement )  . through continual dialogue with the scientific and medical community , oncokb integrates clinical best practices as defined by institutionwide , multidisciplinary disease management teams ( fig 1 )  . 
oncokb communicates information on the biomarker - guided use of fdaapproved therapies and investigational agents under evaluation in clinical trials and highlights negative clinical results to discourage off - label use of expensive targeted therapies shown to be ineffective in specific mutational contexts . methods oncokb includes biologic , clinical , and therapeutic information curated from multiple unstructured information resources , including guidelines and recommendations derived from fda labeling , nccn guidelines , other diseasespecific expert and advocacy group recommendations , and the medical literature ( fig 1 )  . with recognition that clinical implications vary substantially on the basis of specific alterations within a gene and tumor context , information in oncokb is hierarchically organized by gene , alteration , tumor type , and clinical implication ( fig 1 )  . 
oncokb information is publicly available through an interactive web site19 and incorporated into the cbioportal for cancer genomics , 20 - 22 where patient genomic alterations are annotated with information from oncokb and their biologic effects and clinical implications are summarized , which facilitates cancer researcher and clinician interpretation of complex genomic data ( fig 1 )  . 
3 , 000 alterations in 418 cancer - associated genes ( table 1 )  . levels of evidence to communicate the clinical utility of individual mutant alleles consistently , a level of evidence classification system was developed ( fig 2 ) that takes into account the site of tumor origin by recognizing that the effects of targeted inhibitors vary by tumor lineage , even in cancers that share the same mutant allele ( fig 3 )  . 
potentially actionable alterations in a specific cancer type are assigned to one of four levels that are based on the strength of evidence that the mutation is a predictive biomarker of drug sensitivity to fdaapproved or investigational agents for a specific indication . 
level 1 includes genes for which specific alterations have been recognized by the fda as predictive of response to an fda - approved drug in a particular disease context ( data supplement )  . examples include braf v600e and either vemurafenib or dabrafenib as monotherapy or in combination with the mek inhibitors cobimetinib or trametinib in melanoma ; egfr l858r and erlotinib , afatinib , or gefitinib in nonsmall - cell lung cancer ( nsclc ) ; and mutations in exons 9 and 11 of kit and imatinib , sunitinib , and regorafenib in gi stromal tumors . 
in total , 82 alterations in 12 genes are considered level 1 ( data supplement )  . in recognition that some alterations in what would be considered a level 1 gene are intrinsically resistant to currently available fda - approved drugs or fall outside explicit fda approval , oncokb assigns individual alterations to a level of evidence as opposed to the entire gene . 
 variant databases gene alteration tumor type clinical implications incorporation of feedback onc kb oncokb.org web site statistical recurrence treatment guidelines akt1 scientific literature data sources breast cancer ovarian cancer lung cancer e17k e40k l52r q79k amplification prevalence prognosis nccn guidelines standard therapy clinical genomics annotation committee oncokb api cbioportal msk clinical reports investigational therapy curation review variant curation oncokb access fig 1 . 
data sources : alterations are identified by their recurrence18 from public variant databases ( cbioportal , cosmic [ catalogue of somatic mutations in cancer ] , the memorial sloan kettering [ msk ] impact internal clinical sequencing cohort ) , and by prior knowledge available in the literature . biologic and clinical therapeutic implications of alterations are curated from several public resources , including disease - specific treatment guidelines ; abstracts from major conference proceedings , such as asco , european society of medical oncology , and american association for cancer research ; and the scientific literature through pubmed . 
level 2a includes alterations that are not fda - recognized biomarkers but are considered standard care predictive biomarkers of response to an fda - approved therapy in specific cancer types . 
these alterations are highlighted in expert panel guidelines , such as the nccn compendium and asco clinical practice guidelines . several level 2a associations involve rare cancer types ( eg , braf v600e mutant histiocytosis ) or small subpopulations of common cancers ( eg , braf v600e mutant lung cancer ) , and therefore , accrual to a prospective randomized phase iii clinical study may not be feasible . 
because the total number of patients affected often is small , an application for an fda indication may never be filed , but disease experts consider the biomarker - drug association as a standard off - label use . 
in total , 11 genes with 85 alterations are currently considered level 2a ( data supplement )  . as an example , met exon 14 alterations are present in approximately 3% of nsclc27 and represent a distinct , molecularly defined subpopulation of lung adenocarcinomas that are mutually exclusive with tumors that harbor activating mutations in egfr and kras and fusions of alk , ros1 , and ret.28 - 30 an adequately powered randomized trial that compares the met inhibitor crizotinib with other standard approaches , such as chemotherapy and immunotherapy , has not yet been performed partly because of the rarity of these alterations . 
however , durable complete or partial responses to crizotinib and cabozantinib in patients with met exon 14altered lung cancers have been reported.27 , 31 although widely available as a result of its fda approval for use in alk fusionpositive nsclc , crizotinib is not explicitly fda approved in the setting of met exon 14altered nsclc . 
because the nccn guidelines consider off - label prescription of crizotinib a standard treatment approach for patients with lung cancer with met exon 14 alterations , 32 they are classified as level 2a ( fig 2 )  . 
although vemurafenib is not fda approved for use in patients with these specific braf v600e mutant indications , the off - label use of vemurafenib is a well - supported treatment option included in the nccn guidelines on the basis of compelling clinical data33 - 35 ( fig 3 )  . level 2b includes alterations that are standard predictive biomarkers of drug sensitivity in other tumor types but for which data in the tumor in question are either lacking or negative to date . 
for example , braf v600e mutations have been identified in several cancer types , including urothelial carcinomas and germ cell tumors , 36 , 37 for which no clinical response data are reported in the literature . 
in these tumors , the use of raf inhibitors in patients with braf mutant tumors remains investigational , and braf v600e is therefore classified as level 2b36 ( fig 3 )  . 
in patients with braf v600e mutant colorectal cancer , braf inhibitors , such as vemurafenib , have been tested with disappointing results.38 such negative data are referenced in oncokb and argue against the use of raf inhibitor monotherapy in patients with braf v600e colorectal cancers . 
level 3a includes mutations that are candidate predictive biomarkers of drug response on the basis of off - label use of fdaapproved drugs or investigational agents not yet fda approved for any indication . 
for the former , the evidence that supports the predictive value of the alteration is not considered sufficient to warrant a change in standard clinical practice , and disease experts would consider the use of the fda - approved drug in this context to be investigational . 
 into oncokb in real time . oncokb access : oncokb data are available for public use through an interactive web site19 and the cbioportal for cancer genomics22 and are used internally to annotate msk clinical reports . 
api , application program interface ; nccn , national comprehensive cancer network . activity has been reported , and the mutation - drug association is classified as level 3b in all other tumor types . 
fifty - five alterations in 25 genes are considered level 3 ( data supplement )  . a representative example of a level 3 alteration is akt1 e17k ( fig 3 )  . 
promising clinical activity consistent with preclinical studies of this compound has been reported with the investigational panakt inhibitor azd5363 in patients with akt1 e17k mutant breast , lung , cervical squamous , and endometrial cancers.40 - 42 on the basis of these emerging clinical data , akt1 e17k is classified as a level 3a mutation in breast , cervical , endometrial , ovarian , and lung cancers . 
a more complex example of level 3 alterations are erbb2 missense mutations that are present in a minority of a broad range of human cancers43 and that often arise in patients without erbb2 amplification or human epidermal growth factor receptor 2 ( her2 ) protein overexpression.44 these erbb2 mutants demonstrate varying degrees of sensitivity to her2 - selective kinase inhibitors , such as lapatinib and neratinib44 ( fig 3 )  . 
level 4 alterations are candidate predictive biomarkers of response to either fdaapproved or investigational agents on the basis of compelling laboratory data and an absence of substantiating compelling clinical data . 
although anecdotal responses to targeted agents may have been demonstrated in individual patients whose tumor harbored a level 4 alteration , the data are not sufficiently robust to indicate that the presence of the mutation is associated with significantly greater activity than tumors that lack the alteration . 
for example , although studies in mouseand patient - derived xenograft models have suggested that mammalian target of rapamycin or akt - targeted inhibitors may be effective in pten - null tumors , 46 the clinical data that support pten loss as a predictive biomarker of response to phosphatidylinositol 3 - kinase , akt , or mammalian target of rapamycin inhibitors in patients are limited and conflicting.47 - 52 therefore , classification of loss - of - function pten alterations as a level 4 alteration indicates that patients with pten - deficient tumors would be rational candidates for a clinical trial of investigational phosphatidylinositol 3 - kinase pathway inhibitors alone or in combination with other agents , but that the use of such agents outside the context of a clinical trial is not yet supported by the sum of the clinical data . 
additional examples of level 4 alterations include nf1 inactivating alterations , which may be predictive of response to mek1 / 2 inhibitors , 53 and egfr exon 20 insertions in lung adenocarcinomas that respond poorly to erlotinib54 , 55 but which may be sensitive to ap32788 , an investigational inhibitor of egfr and her256 ( fig 3 )  . 
because oncokb levels are dynamic , mutations currently classified as level 4 may be reclassified as level 3 or higher if additional compelling clinical data emerge . levels of resistance ( levels r1 to r3 )  . 
oncokb classifies mutations that have been shown to confer resistance to specific targeted therapies into one of three levels on the basis of the strength of the evidence that the mutation is predictive of treatment resistance ( fig 2 )  . 
level r1 includes mutational events for which there is sufficient evidence to recommend routine testing for the mutation to identify , with a high likelihood , patients who will not respond to a standard therapy . identification of r1 mutations , therefore , would lead to a recommendation that the associated therapy be withheld in patients whose tumors harbor the mutation . 
by definition , level r1 mutations predict for resistance to fda - approved drugs , and testing for such mutations is typically recommended by expert guidelines , such as those published by the nccn . 
level r1 alterations include activating ras mutations in colorectal cancer , which predict for resistance to the egfr - targeted monoclonal antibodies cetuximab and panitumumab57 , 57a ; egfr t790m mutations in nsclc , which predict for intrinsic and acquired resistance to the egfr tyrosine kinase inhibitors ( tkis ) erlotinib , afatinib , and gefitinib58 ; and pdgfra d842v , which predicts for oncokb annotation metric no . 
 level level level level level level level level level fda - recognized biomarker predictive of response to an fdaapproved drug in this indication standard care biomarker predictive of response to an fdaapproved drug in this indication * standard care biomarker predictive of response to an fdaapproved drug in another indication but not standard care for this indication compelling clinical evidence supports the biomarker as being predictive of response to a drug in this indication , but neither biomarker nor drug is standard care compelling clinical evidence supports the biomarker as being predictive of response to a drug in another indication , but neither biomarker nor drug is standard care compelling biologic evidence supports the biomarker as being predictive of response to a drug , but neither biomarker nor drug is standard care standard care biomarker predictive of resistance to an fda - approved drug in this indication compelling clinical evidence supports the biomarker as being predictive of resistance to a drug , but neither biomarker nor drug is standard care compelling biologic evidence supports the biomarker as being predictive of resistance to a drug , but neither biomarker nor drug is standard care standard therapeutic implications * includes biomarkers that are recommended as standard care by the nccn or other expert panels but not necessarily fda recognized for a particular indication investigational therapeutic implications possibly directed to clinical trials hypothetical therapeutic implications on the basis of preliminary , nonclinical data standard therapeutic implications hypothetical therapeutic implications on the basis of preliminary , nonclinical data fig 2 . 
standard therapeutic implications include food and drug administration ( fda ) recognized biomarkers that are predictive of response to an fda - approved drug in a specific indication ( level 1 ) and standard care biomarkers that are predictive of response to an fda - approved drug in a specific indication ( level 2a )  . 
investigational therapeutic implications include fda - approved biomarkers predictive of response to an fdaapproved drug detected in an off - label indication ( level 2b ) , fdaor nonfda - recognized biomarkers that are predictive of response to novel targeted agents that have shown promising results in clinical trials ( level 3a ) , and nonfdarecognized biomarkers that are predictive of response to novel targeted agents on the basis of compelling biologic data ( level 4 )  . 
nccn , national comprehensive cancer network . resistance to imatinib in patients with gi stromal tumors.59 alterations classified as levels r2 and r3 have hypothetical therapeutic implications and include alterations that are predictive of drug resistance on the basis of clinical and biologic data , respectively , but their use in guiding treatment decisions is considered investigational ( fig 2 )  . 
for example , although multiple strategies to reverse the oncogenic effects of tp53 loss have been explored in laboratory studies and early - phase clinical trials , 61 , 62 the agents tested do not directly target tp53 , their activity is typically not restricted to tp53 mutant models , and clinical trials that test these agents either have been aborted because of lack of efficacy or do not use tp53 status as a selection criterion.63 thus , although genomic alterations in tp53 are typically oncogenic , oncokb does not consider them therapeutically actionable . 
90% of alterations in oncokb have curated biologic effects and are classified as oncogenic but are not associated with actionability . actionable alterations across cancer types although targeted inhibitors have been shown to improve clinical outcomes in melanoma and lung cancer among others , 64 the broader clinical utility of large panel or whole - exome testing remains undefined . 
implicit in the designation of a level of evidence for each branch is whether the biomarker is food and drug administration ( fda ) recognized standard care or investigational and whether it is predictive of response to a drug that is fda approved or currently being tested in clinical trials . 
90% of samples harbored at least one known oncogenic mutation , only 41% had one or more alterations for which compelling clinical data currently exist to justify the use of a standard or an investigational agent ( levels 1 to 3b ) ( fig 4a )  . 
level 1 and 2a alterations were most common in melanoma ( 44% ) , ovarian cancer ( 21% , which includes 65 of 312 samples that have either germline or somatic brca1or brca2 - inactivating mutations ) , soft tissue sarcomas ( 19% on the basis of cdk4 amplifications , which predict response to palbociclib in welldifferentiated and dedifferentiated liposarcomas but not in other soft tissue sarcomas ) , nsclc ( 14% ) , esophagogastric cancer ( 13% ) , and breast cancer ( 12% )  . 
however , whereas 44% of melanomas had mutations that predict for clinical benefit with standard therapies in patients with melanoma , the majority of actionable alterations in lgg were associated with only investigational implications , with the most common mutation being idh1 r132c ( 77% of lgg samples ) , a level 3b alteration that is based on promising clinical data with the idh1 inhibitor ag - 120 in patients with acute myeloid leukemia ( figs 4a and 4b )  . 
in total , just over 10% of all samples had a level 3a mutation as their highest actionable alteration , a cohort of patients for which enrollment in a clinical trial would represent a compelling treatment option after standard treatments . 
in addition , approximately 15% of samples had level 3b alterations as their highest actionable event , ie , alterations for which promising clinical data have been observed in an investigational setting in another cancer type . on average , there were approximately three oncogenic mutations per sample , and the number of known oncogenic mutations per sample in tumor types was independent of overall mutation burden ( fig 4c )  . 
for example , although renal cell cancers had , on average , one oncogenic mutation per sample , these mutations were typically inactivating in tumor suppressors , such as vhl and pbrm1 , which are not clinically actionable at this time . 
in contrast , although thyroid cancers also on average had approximately one oncogenic mutation per sample ( fig 4c ) , these alterations were typically actionable , such as ret fusions and braf and nras mutations . 
frequencies of level of evidence 1 to 3 assignments in the cancer genome atlas cohorts . patient samples from 19 cancer types ( the cancer genome atlas ) are classified by the alteration that carries the highest level of evidence . 
 ( a ) inset pie chart : fraction of samples across all cancer types that carry a mutation considered actionable according to the levels of evidence , oncogenic but not actionable , or variants of unknown significance ( vus )  . 
cell color as shown in the key for the inset pie chart ( a )  . columns indicate sample tumor type , rows indicate gene alteration present in sample , and numbers indicate the percentage of samples per tumor type that harbor an alteration in each gene . 
 ( c ) each patient sample was classified by the number of oncogenic alterations or the number of actionable alterations . shown is the mean number of actionable ( black ) , oncogenic ( dark gray ) , or total ( gray ) mutations per sample per tumor type . 
 ( d ) each tumor type was evaluated for the percentage of samples that carry zero , one , two , three , or four or more actionable mutations per sample ( indicated in shades of blue )  . 
 mutations ( 31% , 25% , and 22% , respectively ) , which is consistent with data that demonstrate that these tumor types are driven by multiple oncogenic mutations in nonredundant pathways65 - 68 ( fig 4d ) and may explain why targeted monotherapies have shown disappointing results to date in some of these cancer types.69 , 70 discussion since the introduction of imatinib for chronic myeloid leukemia more than a decade ago , 71 , 72 a growing number of drugs that target specific genetic alterations required for tumor initiation and progression have been shown to significantly improve outcomes in molecularly defined populations of patients with cancer.64 , 73 - 74a although tumor genetic testing is now part of routine patient care in an increasing number of tumor types , interpretation of variants remains an important challenge , and in major academic cancer centers , a significant proportion of physicians report low confidence in their ability to make optimal treatment recommendations on the basis of genomic information.75 although multiple classification systems exist for the annotation of germline variants , 76 , 77 efforts to define the clinical utility of somatic alterations have been limited to established biomarkers , 78 - 80 and prior efforts often have classified actionability as a binary variable that results in the grouping of biomarkers that are fda recognized with those that are nonactionable but oncogenic . 
to this end , we assigned each mutation to one of four levels that are based on available clinical and laboratory data that support the use of the mutation as a predictive biomarker . 
standard therapeutic implications are classified as either level 1 or 2a to recognize that not all mutation - drug associations used in standard practice have been recognized by the fda . 
moreover , there are cases where off - label use of an fda - approved drug is explicitly not warranted because of existing data that argue against the use of a targeted agent in a specific cancer type . 
for example , although the braf inhibitor vemurafenib is a standard treatment option for patients with braf v600e mutant melanoma or nsclc , robust clinical reports from multiple independent centers demonstrated that patients with braf v600e mutant colorectal cancer do not respond to raf inhibitors , at least as monotherapy.38 , 84 similarly , although erbb2 amplification predicts for the clinical utility of her2 - targeted therapies in breast and esophagogastric cancers , the clinical activity of trastuzumab in erbb2 - amplified lung cancers has been disappointing.85 braf v600e and erbb2 amplification are , therefore , level 2b when detected in colorectal cancers . 
 individual mutant alleles within a single gene may be functionally distinct , with different predictive value and , therefore , individual therapeutic implications , which complicates the development of clinical decision support tools , particularly in the context of often - vague fda labeling and expert guidelines , such as those provided by the nccn , that may not define at a granular level whether specific mutations within a gene are predictive of drug response . 
to address this complexity , oncokb groups mutations in level 1 genes , such as egfr and kit , according to whether they are biologically active , whether there are preclinical data to suggest that the allele is sensitive or resistant to the matched targeted agents , and whether there are clinical data to suggest clinical sensitivity or intrinsic resistance to the approved targeted therapy . 
the challenge of rare drug - sensitive variants in level 1 genes also highlights the need for consortia efforts , such as the american association for cancer research project genie ( genomics evidence neoplasia information exchange ) , which should allow for the collection of clinical response data for rare alleles to help to guide the treatment of patients with these less common mutations . although new laboratory and clinical data are continually generated , fda labels and professional guidelines are updated at irregular intervals . 
for example , although explicit fda approval of crizotinib in ros1 - rearranged nsclc did not occur until march 2016 , offlabel use of crizotinib in patients with ros1 fusion - positive lung cancers has been considered standard of care by several expert groups for some time.86 - 88 as another example , whereas kras was initially considered a level 3a alteration in nsclc on the basis of promising data from the randomized phase ii study that supplemented standard chemotherapy with a mek inhibitor , 89 the subsequent phase iii trial showed no survival benefit with this combination , 90 which is consistent with negative data associated with mek inhibitor use in kras mutant pancreatic and colorectal cancers.91 , 92 nonetheless , anecdotal clinical and compelling preclinical data support the use of kras as a predictive biomarker of sensitivity to novel mek and erk inhibitors alone or in combination with other agents.93 - 97 oncokb thus recognizes and reassigns the level of evidence of mutational events , if appropriate , on the basis of newer , moredefinitive , and negative randomized clinical data , which take precedence over prior preliminary clinical findings . to incorporate new clinical and research findings , we have made the oncokb annotation available publically through an interactive web site19 and through the cbioportal for cancer genomics.22 both systems include a comment feature to facilitate crowdsourcing curation of this knowledge base . 
user suggestions are evaluated by the scientific team and incorporated into oncokb through periodic updates . oncokb is also an active member in efforts to promote harmonization of variant annotation across existent knowledge bases and is participating in both clingen and the global alliance for genomic health through the variant interpretation cancer consortium . in the future , we will curate information about mutational signatures , such as overall mutation burden and the possible link to immunotherapy , mutational clonality , and the impact on drug sensitivity of co - occurrence of specific oncogenic and actionable mutations . 
rudolph , ederlinda paraiso collection and assembly of data : debyani chakravarty , jianjiong gao , sarah phillips , ritika kundra , hongxin zhang , tara soumerai , moriah h . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . debyani chakravarty no relationship to disclose jianjiong gao no relationship to disclose sarah phillips no relationship to disclose ritika kundra no relationship to disclose hongxin zhang no relationship to disclose jiaojiao wang no relationship to disclose julia e . 
chang no relationship to disclose rona yaeger consulting or advisory role : glaxosmithkline , advaxis sarat chandarlapaty honoraria : chugai pharmaceutical , foresite capital , astrazeneca , sermonix pharmaceuticals , macrogenics , agendia research funding : eli lilly ( inst ) , novartis ( inst ) travel , accommodations , expenses : chugai pharmaceutical , macrogenics , astrazeneca tiffany a . 
traina consulting or advisory role : genentech , roche , eisai , mundipharma , medivation , pfizer , astrazeneca , bayer ag , immunomedics , merck research funding : medivation , eisai , pfizer , novartis , myriad genetics , innocrin pharmaceuticals , astrazeneca paul k . 
paik honoraria : celgene , bristol - myers squibb , eli lilly , ariad pharmaceuticals consulting or advisory role : celgene , eli lilly , ariad pharmaceuticals , bristol - myers squibb , celgene research funding : celgene , emd serono travel , accommodations , expenses : emd serono alan l . 
ho consulting or advisory role : oncology consortium , bristol - myers squibb , eisai , genzyme , merck , novartis , sun pharmaceutical industries , kura oncology speakers bureau : medscape , omniprex america , eli lilly , genentech , roche , astrazeneca , bayer ag , kura oncology , kolltan pharmaceuticals , eisai , astrazeneca travel , accommodations , expenses : janssen pharmaceuticals , merck , kura oncology feras m . 
hantash employment : quest diagnostics stock and other ownership interests : quest diagnostics patents , royalties , other intellectual property : patents on molecular methods , but not related to manuscript andrew grupe employment : quest diagnostics stock and other ownership interests : quest diagnostics patents , royalties , other intellectual property : patents or patent applications travel , accommodations , expenses : quest diagnostics shrujal s . 
danila honoraria : astellas pharma , angle , bayer ag , janssen pharmaceuticals consulting or advisory role : angle , bayer ag research funding : prostate cancer foundation , genentech , janssen pharmaceuticals ( inst ) patents , royalties , other intellectual property : gene expression profile associated with prostate cancer travel , accommodations , expenses : cambridge healthtech institute , prostate cancer foundation , angle , bayer ag , american austrian foundation open medical institute , global technology community , janssen pharmaceuticals , oncology education mrinal gounder honoraria : amgen , daiichi sankyo , karyopharm therapeutics , tracon pharmaceuticals , amgen consulting or advisory role : daiichi sankyo , karyopharm therapeutics , epizyme speakers bureau : amgen travel , accommodations , expenses : amgen travel , accommodations , expenses : daiichi sankyo , karyopharm therapeutics james j . 
harding no relationship to disclose dana rathkopf consulting or advisory role : janssen pharmaceuticals research funding : janssen pharmaceuticals ( inst ) , medivation ( inst ) , celgene ( inst ) , takeda pharmaceuticals ( inst ) , millennium pharmaceuticals ( inst ) , ferring pharmaceuticals ( inst ) , novartis ( inst ) , taiho pharmaceutical ( inst ) , astrazeneca ( inst ) , genentech ( inst ) , roche ( inst ) , tracon pharmaceuticals ( inst ) alexander n . 
shoushtari consulting or advisory role : vaccinex , castle biosciences , immunocore research funding : bristol - myers squibb , immunocore travel , accommodations , expenses : bristol - myers squibb neerav shukla no relationship to disclose martin h . 
voss honoraria : novartis consulting or advisory role : novartis , calithera biosciences , natera , glaxosmithkline , exelixis , pfizer , alexion pharmaceuticals research funding : pfizer , bristol - myers squibb , genentech , roche travel , accommodations , expenses : novartis , takeda pharmaceuticals matthew d . 
hellmann consulting or advisory role : bristol - myers squibb , merck , genentech , astrazeneca , medimmune , novartis , janssen pharmaceuticals research funding : bristol - myers squibb , genentech , roche ederlinda paraiso no relationship to disclose ahmet zehir no relationship to disclose gopa iyer no relationship to disclose yelena y . 
levine stock and other ownership interests : critical outcome technologies consulting or advisory role : clovis oncology , mtrap , biodesix , tesaro maeve lowery consulting or advisory role : agios , celgene antonio omuro consulting or advisory role : stemline therapeutics , juno therapeutics , bristol - myers squibb , oxigene , alexion pharmaceuticals , astrazeneca , inovio pharmaceuticals , merck michael a . 
postow honoraria : bristol - myers squibb , merck consulting or advisory role : amgen , bristol - myers squibb , novartis research funding : bristol - myers squibb ( inst ) , novartis ( inst ) , array biopharma ( inst ) , infinity pharmaceuticals ( inst ) travel , accommodations , expenses : bristol - myers squibb leonard b . 
riely consulting or advisory role : novartis , genentech research funding : novartis ( inst ) , roche ( inst ) , genentech ( inst ) , millennium pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , infinity pharmaceuticals ( inst ) , ariad pharmaceuticals ( inst ) patents , royalties , other intellectual property : patent application submitted that covers pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : novartis marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network , boehringer ingelheim , astrazeneca research funding : loxo oncology ( inst ) david m . 
 jos e baselga leadership : infinity pharmaceuticals , varian medical systems , grail , foghorn stock or other ownership : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , varian medical systems , tango , foghorn , aura biomedical , apogen , northern biologics honoraria : pmv pharma , juno therapeutics , infinity pharmaceuticals , grail , northern biologics consulting or advisory role : eli lilly , novartis , grail patents , royalties , other intellectual property : combination therapy using pdk1 and pi3k inhibitors . 
may 16 travel , accommodations , expenses : roche / genentech paul sabbatini research funding : bristol - myers squibb ( inst ) , ludwig institute for cancer research ( inst ) david b . 
solit honoraria : loxo oncology , pfizer consulting or advisory role : pfizer , loxo oncology nikolaus schultz no relationship to disclose acknowledgment we thank the following individuals for serving as oncokb curators : andrew intlekofer , eric smith , piro lito , jaclyn hechtman , dmitriy zamarin , wassim abida , mythili koneru , weiyi toy , pedram razavi , philip iaquinta , byron lee , martin dalin , matthew jones , elizabeth adams , karuna ganesh , olga guryanova , carolyn jackson , william terry , yu chen , ping chi , eduard reznik , aphrothiti hanrahan , sevin turcan , philip watson , neeman mohibullah , elena goldberg , aaron viny , emily foley , samuel kaffenberger , andrew winer , connie batlevi , helen won , lindsay saunders , kinisha gala , philip jonsson , fiona brown , eneda toska , i~nigo landalopez , and tripti shrestha - bhattarai . affiliations debyani chakravarty , jianjiong gao , sarah phillips , ritika kundra , hongxin zhang , jiaojiao wang , julia e . 
j am med inform assoc 10.1093 / jamia / ocw148 [ epub ahead of print on october 27 , 2016 ] institute of precision medicine : welcome to the precision medicine knowledgebase . 
kim kb , kefford r , pavlick ac , et al : phase ii study of the mek1 / mek2 inhibitor trametinib in patients with metastatic braf - mutant cutaneous melanoma previously treated with or without a braf inhibitor . 
paik pk , drilon a , fan pd , et al : response to met inhibitors in patients with stage iv lung adenocarcinomas harboring met mutations causing exon 14 skipping . 
ma pc , jagadeeswaran r , jagadeesh s , et al : functional expression and mutations of c - met and its therapeutic inhibition with su11274 and small interfering rna in non - small cell lung cancer . 
ma pc , kijima t , maulik g , et al : c - met mutational analysis in small cell lung cancer : novel juxtamembrane domain mutations regulating cytoskeletal functions . 
frampton gm , ali sm , rosenzweig m , et al : activation of met via diverse exon 14 splicing alterations occurs in multiple tumor types and confers clinical sensitivity to met inhibitors . 
planchard d , besse b , groen hj , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
davies br , greenwood h , dudley p , et al : preclinical pharmacology of azd5363 , an inhibitor of akt : pharmacodynamics , antitumor activity , and correlation of monotherapy activity with genetic background . 
hyman dm , smyth l , bedard pl , et al : abstract b109 : azd5363 , a catalytic pan - akt inhibitor , in akt1 e17k mutation positive advanced solid tumors . 
hyman d , piha - paul s , rod on j , et al : abstract pd5 - 05 : neratinib for erbb2 mutant , her2 non - amplified , metastatic breast cancer : preliminary analysis from a multicenter , open - label , multi - histology phase ii basket trial . cancer res 76 : pd5 - 05 , 2016 46 . 
lin j , sampath d , nannini ma , et al : targeting activated akt with gdc - 0068 , a novel selective akt inhibitor that is efficacious in multiple tumor models . 
clin cancer res 19 : 1760 - 1772 , 2013 de bono js , de giorgi u , massard c , et al : pten loss as a predictive biomarker for the akt inhibitor ipatasertib combined with abiraterone acetate in patients with metastatic castration - resistant prostate cancer ( mcrpc )  . 
ma cx , luo j , naughton m , et al : a phase i trial of bkm120 ( buparlisib ) in combination with fulvestrant in postmenopausal women with estrogen receptor - positive metastatic breast cancer . 
rodon j , bra~na i , siu ll , et al : phase i dose - escalation and - expansion study of buparlisib ( bkm120 ) , an oral panclass i pi3k inhibitor , in patients with advanced solid tumors . 
yang l , clarke mj , carlson bl , et al : pten loss does not predict for response to rad001 ( everolimus ) in a glioblastoma orthotopic xenograft test panel . 
naidoo j , sima cs , rodriguez k , et al : epidermal growth factor receptor exon 20 insertions in advanced lung adenocarcinomas : clinical outcomes and response to erlotinib . 
yasuda h , park e , yun ch , et al : structural , biochemical , and clinical characterization of epidermal growth factor receptor ( egfr ) exon 20 insertion mutations in lung cancer . 
gonzalvez f , zhu x , huang w - s , et al : abstract 2644 : ap32788 , a potent , selective inhibitor of egfr and her2 oncogenic mutants , including exon 20 insertions , in preclinical models . 
druker bj , sawyers cl , kantarjian h , et al : activity of a specific inhibitor of the bcr - abl tyrosine kinase in the blast crisis of chronic myeloid leukemia and acute lymphoblastic leukemia with the philadelphia chromosome . n engl j med 344 : 1038 - 1042 , 2001 72 . 
druker bj , talpaz m , resta dj , et al : efficacy and safety of a specific inhibitor of the bcr - abl tyrosine kinase in chronic myeloid leukemia . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
macarthur dg , manolio ta , dimmock dp , et al : guidelines for investigating causality of sequence variants in oncol 32 : 1317 - 1323 , 2014 human disease . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
simon rm , paik s , hayes df : use of archived specimens in evaluation of prognostic and predictive biomarkers . j natl cancer inst 101 : 1446 - 1452 , 2009 81 . 
conti rm , bernstein ac , villaflor vm , et al : prevalence of off - label use and spending in 2010 among patentprotected chemotherapies in a population - based cohort of medical oncologists . 
langer cj , stephenson p , thor a , et al : trastuzumab in the treatment of advanced non - small - cell lung cancer : is there a role ? focus on eastern cooperative oncology group study 2598 . 
j clin oncol 22 : 1180 - 1187 , 2004 85a . jordan ej , kim hr , arcila me , et al : prospective comprehensive molecular characterization of lung adenocarcinomas for efficient patient matching to approved and emerging therapies . 
cell 131 : 1190 - 1203 , 2007 janne pa , shaw at , pereira jr , et al : selumetinib plus docetaxel for kras - mutant advanced non - small - cell lung cancer : a randomised , multicentre , placebo - controlled , phase 2 study . 
clin lung cancer 17 : e1 - e4 , 2016 infante jr , fecher la , falchook gs , et al : safety , pharmacokinetic , pharmacodynamic , and efficacy data for the oral mek inhibitor trametinib : a phase 1 dose - escalation trial . 
rinehart j , adjei aa , lorusso pm , et al : multicenter phase ii study of the oral mek inhibitor , ci - 1040 , in patients with advanced non - small - cell lung , breast , colon , and pancreatic cancer . 
hu - lieskovan s , mok s , homet moreno b , et al : improved antitumor activity of immunotherapy with braf and mek inhibitors in braf ( v600e ) melanoma . 
kakavand h , wilmott js , menzies am , et al : pd - l1 expression and tumor - infiltrating lymphocytes define different subsets of mapk inhibitor - treated melanoma patients . 
loi s , dushyanthen s , beavis pa , et al : ras / mapk activation is associated with reduced tumor - infiltrating lymphocytes in triple - negative breast cancer : therapeutic cooperation between mek and pd - 1 / pd - l1 immune checkpoint inhibitors . 
yoon yk , kim hp , han sw , et al : kras mutant lung cancer cells are differentially responsive to mek inhibitor due to akt or stat3 activation : implication for combinatorial approach . 
 o androgen receptor immunohistochemistry as a companion diagnostic approach to predict clinical response to enzalutamide in triple - negative breast cancer purpose the androgen receptor ( ar ) is increasingly recognized as a potential biomarker for identifying a subset of patients with possible hormonally driven triple - negative breast cancer ( tnbc )  . 
thus , we evaluated ar expression by immunohistochemistry in patients with advanced tnbc before treatment with the ar inhibitor enzalutamide . methods we optimized and validated immunohistochemistry assays in breast and prostate cancer cell lines and tissues using two commercial ar monoclonal antibodies ( sp107 and ar441 )  . 
ar expression was then examined in patients with advanced tnbc enrolled in a phase ii study of enzalutamide ( clinicaltrials.gov identifier : nct01889238 ) on archived or fresh tissue before treatment . 
association with clinical response was assessed by sensitivity , specificity , positive predictive value ( ppv ) , drop - out rate , and survival . results ar expression was detected in 80% and 63% of breast cancer tissue using sp107 and ar441 , respectively . 
2017 by american society of clinical oncology introduction breast cancer is a heterogeneous disease characterized by distinct molecular and genetic subtypes.1 , 2 recent progress in gene expression studies has identified major breast cancer subtypesthe estrogen receptor ( er ) or progesterone receptor ( pgr ) positive ( er + or pgr + ) luminal a and luminal b , human epidermal growth factor receptor 2 ( her2 ) positive ( her2 + ) , and basal - like breast cancers , most of which express neither er , pgr , nor her2 and are referred to as triple - negative breast cancer ( tnbc ) .1 - 4 in clinical settings , targeted therapies play a critical role in the treatment of patients diagnosed with er + or pgr + and her2 + breast cancer . 
more than 77% of invasive breast tumors are defined as ar positive ( ar + ) when 10% or more ar nuclear staining is present in cancer cells as shown by immunohistochemistry ( ihc ) 9 , 10 ; however , ar oncogenic activity in breast cancer is poorly understood.11 , 12 enzalutamide significantly inhibited tumor growth in a xenograft model13 and , compared with other antiandrogen agents , also showed stable disease and antitumor response in clinical settings.14 - 16 in this study , we evaluated the use of the ar as a putative biomarker , using ihc to identify a subset of patients with tnbc who could benefit from enzalutamide . targeted ar therapy requires the appropriate selection of patients with breast cancer . 
breast carcinoma cell lines ( ar strongly positive t - 47d and ar + mcf7 ) and prostate carcinoma cell lines ( ar + lncap and ar - negative [ ar ] du145 ) were used to confirm staining procedures . 
accuracy , sensitivity , and specificity were calculated for both antibodies . tissue evaluation for protocol optimization was performed on commercial breast tissue ( normal and tumor ) and prostate tumors . 
formalin - fixed paraffin - embedded blocks of 4to 10 - mm sections on slides were shipped in kits provided by a central laboratory ( covance , princeton , nj ) from multiple clinical trial sites to clarient diagnostic services . 
all stained slides were evaluated for nuclear staining and were scored for ar expression by a trained pathologist using bright field microscopy ( data supplement )  . all ihc staining resulted in two scores : a staining intensity ranging from 0 to 3 ( 0 = not detectable , 1 = translucent , 2 = opaque , 3 = solid ) and the percentage of cells staining positively at each level of staining intensity . 
in addition to the total staining score , we evaluated other ihc scoring functions , including the h score , to determine whether they may perform better in classifying responders . 
the h score is a widely used , semiquantitative measure that considers both the cell staining intensity and the percentage of cells stained positively.17 the score is obtained by the equation , 3 3 the percentage of solid - staining nuclei ( score at 3 ) + 2 3 the percentage of opaque - staining nuclei ( score at 2 ) + the percentage of translucent - staining nuclei ( score at 1 ) , yielding results in a range of 0 to 300 , which are then normalized to a scale of 0% to 100% . to validate the optimized procedures , 93 independent breast carcinoma tissue samples and 10 independent prostate carcinoma tissue samples in a microarray format were then stained with the optimized protocol for sp107 . 
slides stained using the optimized sp107 and ar441 procedures and clia - compliant ar441 reference assay were scored for ar expression by the pathologist , using a standard bright field microscope ( appendix table a1 )  . phase ii clinical trial mdv3100 - 11 was a simon two - stage , single - arm , open - label phase ii trial to evaluate the efficacy and safety of enzalutamide in patients with locally advanced or metastatic ar + tnbc ( clinicaltrials.gov identifier : nct01889238 ) .18 the study was conducted in accordance with the principles of the declaration of helsinki and good clinical practice . 
all patients provided written informed consent before any study - related procedures . the intention - to - treat patients with advanced tnbc , defined as , 1% staining by ihc for er and pgr and 0 to 1 + by ihc for her2 or negative for her2 amplification by in situ hybridization for 2 + ihc , and 0.05% or more ar + staining were enrolled and treated with enzalutamide ( 160 mg / d )  . 
the association between ar expression and progression - free survival ( pfs ) and overall survival ( os ) was analyzed using cox proportional hazards regression models and was presented as kaplan - meier estimates with hazard ratio ( hr ) and 95% ci . 
for sp107 , antigen retrieval was optimized for 64 minutes at standard high ph ( appendix fig a2 ) , and primary antibody incubation was optimized without dilution for 24 minutes . 
the primary antibody was incubated at a 1 : 800 dilution for 30 minutes . the optimized ihc conditions were then verified on breast carcinoma tissue , normal breast tissue , and two breast carcinoma cell lines known to express the ar ( t - 47d and mcf719 )  . 
the staining patterns clearly indicated that sp107 displayed more intense ar expression than did ar441 ( fig 1 and appendix fig a3 )  . breast and prostate carcinoma tissues microarrays were used to optimize the ihc staining procedures . 
however , we observed that sp107 had a more robust staining signal compared with ar441 regardless of whether slides were collected after a shorter or a longer time ( appendix tables a2 and a3 )  . interestingly , when comparing the incidence of ar positivity ( defined as expression in > 10% of cells ) with the rate reported in the literature , ar + detection rates with ar441 were lower overall for breast and prostate carcinoma . 
for example , in prostate cancer samples , ar incidence was 80% ( eight of 10 ) and 44% ( four of nine ) with sp107 and ar441 , respectively . to further assess the performance of the ihc conditions , we compared the results from the current ihc methods with an ihc assay validated in a clia - certified laboratory to determine accuracy , sensitivity , and specificity . 
the optimized sp107 conditions were used to stain 46 breast carcinoma tissues in microarray format , and the optimized ar441 conditions ( table a1 ) were used to stain 43 breast carcinoma tissues in microarray format . 
the sensitivity was 100% for both , and the specificity was 42% and 57% for sp107 and ar441 , respectively . sp107 had higher positivity rates of 78% compared with ar441 , which had 70% positivity rates . 
importantly , the positivity rates for these optimized conditions were much higher than the rates from the clia - certified assay , which were 48% and 47% in the sp107 and ar441 sample sets , respectively . 
rate of ar expression in breast and prostate carcinoma compared with literature 10% of cells ar + , n of n ( % ) literature reports tissue type tnbc sp107 ar441 antibody clone ( source ) 9 of 26 ( 35 ) 6 of 15 ( 40 ) ar441 ( thermo scientific ) ar27 ( novocastra ) ar441 ( dako ) er + and / or pgr + breast carcinoma 50 of 50 ( 100 ) 19 of 25 ( 76 ) ar441 ( thermo scientific ) her2 + breast carcinoma 15 of 17 ( 88 ) 10 of 16 ( 63 ) ar27 ( novocastra ) breast carcinoma , any subtype 74 of 93 ( 80 ) 35 of 56 ( 63 ) ar411 ( dako ) prostate carcinoma 8 of 10 ( 80 ) 4 of 9 ( 44 ) ar441 ( dako ) cutoff for positivity ( % ) > 10  . 
of these prescreened patients , 118 with advanced tnbc met the other eligibility criteria and were enrolled in the trial . clinical outcomes from the phase ii trial have been reported.18 with clinical benefit rate at 16 weeks as the primary end point , 29 of 118 enrolled intentionto - treat patients ( 24.6% ) were responders to enzalutamide . 
the maximum ppv of 39.6% was reached at a high cutoff value of 80% , with a dr of 55.1% and a lost responder rate of 27.6% ( eight of 29 )  . 
importantly , a lower cutoff decreased ppv from 40% to 30% , but it increased the sensitivity and reduced the dr substantially , suggesting that a lower threshold may be favorable . we also explored the h score to evaluate the number of patients with ar + tnbc , responders , ppv , and dr at different thresholds of 0% , 10% , 30% , 50% , and 80% ( methods , appendix fig a6a , and appendix table a4 )  . 
the 10% cutoff has the potential to capture 56% of total patients with tnbc ( appendix fig a7 ) , which may translate to nearly 138 , 000 patients globally . 
in addition , not all ar + tnbc tumors accurately represent the tumor molecular biology of an ar - driven disease . thus , a genomic signaturebased approach independent of ar expression level may better identify patients . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . iulia cristina tudor employment : medivation , pfizer stock and other ownership interests : medivation , pfizer travel , accommodations , expenses : medivation amy peterson employment : beigene , medivation leadership : beigene stock and other ownership interests : beigene , medivation , loxo patents , royalties , other intellectual property : patent for identifying patients with tnbc who may benefit from enzalutamide travel , accommodations , expenses : beigene , medivation hirdesh uppal employment : medivation stock and other ownership interests : medivation patents , royalties , other intellectual property : patents related to patient selection varun kumar no relationship to disclose jianjun yu employment : predicine , novartis ( i ) , medivation / pfizer stock and other ownership interests : medivation / pfizer , predicine , novartis ( i ) vernon phan employment : medivation / pfizer stock and other ownership interests : medivation / pfizer travel , accommodations , expenses : medivation / pfizer affiliations all authors : medivation , san francisco , ca . acknowledgment medical writing and editorial support was provided by stephanie vadasz and paula stuckart of ashfield healthcare communications . 
the sponsors were responsible for the study design , data collection and analysis , decision to publish , and preparation of the manuscript . support supported by medivation and astellas pharma , the co - developers of enzalutamide . 
collins lc , cole ks , marotti jd , et al : androgen receptor expression in breast cancer in relation to molecular phenotype : results from the nurses health study . 
gucalp a , tolaney s , isakoff sj , et al : phase ii trial of bicalutamide in patients with androgen receptor - positive , estrogen receptor - negative metastatic breast cancer . 
phan vt , protter aa , peterson ac , et al : a novel diagnostic androgen receptor gene signature links clinical outcomes and preclinical response to enzalutamide , paclitaxel or the combination in triple - negative breast cancer [ abstract ]  . cancer res 76 : p2 - 07 - 04 , 2016 17 . 
traina ta , miller k , yardley da , et al : results from a phase 2 study of enzalutamide ( enza ) , an androgen receptor ( ar ) inhibitor , in advanced ar + triple - negative breast cancer ( tnbc )  . 
magklara a , brown tj , diamandis ep : characterization of androgen receptor and nuclear receptor co - regulator expression in human breast cancer cell lines exhibiting differential regulation of kallikreins 2 and 3 . 
anestis a , karamouzis mv , dalagiorgou g , et al : is androgen receptor targeting an emerging treatment strategy for triple negative breast cancer ? cancer treat rev 41 : 547 - 553 , 2015 27 . 
hickey te , robinson jl , carroll js , et al : minireview : the androgen receptor in breast tissues : growth inhibitor , tumor suppressor , oncogene ? mol endocrinol 26 : 1252 - 1267 , 2012 29 . 
process flow diagraclia , clinical laboratory improvement amendments . dako ( ar441 ) ventana ( sp107 ) protocol optimization protocol verification with cell lines reproducibility and repeatability studies to compare both ventana and dako methods stability studies to compare both methods correlation analysis with clia - compliant ar441 - based method fig a2 . 
white lines indicate medians , and gray dotted line indicates average age of all patients . the average age of responders is approximately 9.5% higher than the average age of nonresponders . 
 ( a ) bar plot of the number of diagnostic positives and true - positives for selected h - score thresholds . positive predictive value ( ppv ; gray ) and drop - out rate ( dr ; red ) were plotted as lines . 
the overall prevalence rate of ar + patients is approximately 56% at an optimal 10% threshold selected in this study ( ar , > 10% )  . color by 10% cutoff 30% cutoff 50% cutoff 80% cutoff sp107 total nuclear ar % sp107 nuclear h score sum sp107 nuclear ar 3 + , 2 + sum sp107 nuclear 3 + table a1 . 
other listed variants were reported by foundation medicine as variants of unknown signicance . abbreviations : chip , clonal hematopoiesis of indeterminate potential ; mtb , molecular tumor board ; total depth , total depth of sequencing reads . tumor , whereas the pten variant was at an allele frequency compatible with being homozygous in the tumor as a result of loss of heterozygosity or gene conversion to inactivate the second wild - type allele . 
these observations , in addition to the kit mutation having an allele fraction of 0.23% , raised the possibility that the lower allele fraction alterations may be arising from the patients melanoma ( fig 2 )  . 
several studies have shown that ctdna correlates with tumor burden , and it may be that the only melanoma tissue mass in this patient was in his brain.2 , 3 the reex testing of the patients colon cancer and melanoma was performed using the illumina trusight tumor 15 gene panel ( illumina , san diego , ca ) , with results masked to only report out specic genes depending on the indication ( ie , kras , nras , and braf for colon cancer and braf , nras , and kit for melanoma )  . 
studies have shown that clonal mutations in the hematopoietic compartment may be detected on tumor tissue testing.4 , 5 the results suggest that ctdna analysis in this patient identied not only clonal dna from two separate solid tumors , but also an additional third clonal mutation in the hematopoietic compartment , as has been recently described.6 the patient was evaluated at rutgers cancer institute of new jersey and provided informed consent to participate in a prospective study trial for tumor genomic proling ( clinicaltrials.gov identier : nct02688517 )  . 
the results of genomic proling , clinical course , and pathology were reviewed at the rutgers cancer institute of new jersey molecular tumor board ( mtb ) , which was approved by the rutgers university new brunswick health sciences institutional review board ( pro2012002075 )  . 
because the alteration occurred in a homopolymer region and brca2 is a large gene , this may have been a passenger alteration as a result of the tumor being decient in mmr . 
 detection of three distinct clonal populations using ctdna determine whether both alleles were inactivated , the mtb suggested that platinum drugs or poly ( adp - ribose ) polymerase inhibitors could be effective . 
recent work has shown that cdk12 regulates dna damage response genes , including brca1 , and is sensitive to dna - damaging agents and poly ( adpribose ) polymerase inhibitors.11 , 12 the mtb suggested that these agents may be an option with the potential to target both the brca2 truncating mutation and the cdk12 inactivating mutation . 
in addition , during the mtb meeting , accumulating evidence suggesting that loss of genes involved in dna damage repair , such as brca2 or cdk12 , may have a role in sensitivity to immune checkpoint inhibitors was presented.13 , 14 it is unusual that three truncating apc mutations that likely arose from the patients colon cancer at heterozygous levels were identied . 
apc mutations are typically correlated with microsatellite - stable colon cancer , whereas one mutation of each allele would be sufcient to inactivate the proteit may be that the colon cancer initially developed along the microsatellite - stable pathway with biallelic inactivation of apc before acquiring an additional frameshift mutation as a result of loss of mmr function , with apc being particularly susceptible to being damaged by a loss of mmr because it is a large gene . 
shortly after , the patient became septic , developed endocarditis , and ultimately died during an operation to remove the aortic valve . after the mtb meeting , pms2 ihc was performed on the melanoma from the craniotomy , which showed intact pms2 ( fig 1b )  . 
therefore , the ve lower allele frequency variants showing alterations in homopolymer regions most likely represent subclonal alterations in the colon cancer as a result of the defect in mmr . 
also after the mtb meeting , sequencing of a lymph node negative for tumor from the patients original sentinel lymph node dissection on the illumina trusight tumor 15 gene panel was performed . 
in addition , because the lymph node was removed 18 months before the patients blood was sequenced , the tp53 mutation may not have even been present at that time or present at even lower levels . 
in both cases , tp53 was negative in tumor cells , although melanin and occasional tp53 - positive cells were observed in the melanoma ( figs 1a and 1b )  . 
tp53 somatic missense mutations in cancer are generally reported to be positive by ihc , and p.g244c was reported to be positive in 17 of 18 samples.15 in total , the negative sequencing and ihc the tp53 results strongly suggest p.g244c mutation having arisen in the hematopoietic compartment . the possibility of in summary , ctdna proling identied alterations at different allele frequencies that seemed to correspond with mutations present in his colon cancer and melanoma . remarkably , there was a tp53 mutation identied in the liquid biopsy , with subsequent sequencing and ihc results indicating it was unlikely to be present in either of the solid tumors and suggesting a third clonal mutation in the hematopoietic compartment . 
when ctdna analysis is performed , knowledge of genomic alterations in the primary cancer may not be available , and occasionally , there may be a second unknown primary cancer . 
mehnert , hossein khiabanian , shridar ganesan administrative support : hossein khiabanian provision of study materials or patients : elizabeth poplin , roman groisberg , hossein khiabanian collection and assembly of data : gregory m . 
mehnert honoraria : emd serono , pzer consulting or advisory role : amgen , boehringer ingelheim , array biopharma , merck sharp & dohme research funding : merck ( inst ) , sano ( inst ) , novartis ( inst ) , polynoma ( inst ) , immunocore ( inst ) , amgen ( inst ) , astrazeneca ( inst ) , incyte ( inst ) , macrogenics ( inst ) , bristol - myers squibb ( inst ) travel , accommodations , expenses : emd serono , merck sharp & dohme , array biopharma , bristol - myers squibb other relationship : amgen , emd serono , merck , boehringer ingelheim , array biopharma roman groisberg honoraria : guidepoint global shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis , roche , foghorn therapeutics , foundation medicine patents , royalties , other intellectual property : i hold two patents for digital imaging that may be licensed to ibris and inspirata travel , accommodations , expenses : inspirata no other potential conicts of interest were reported . references khiabanian h , hirsheld km , goldnger m , et al : inference of germline mutational status and evaluation of loss of heterozygosity in high - depth , tumor - only sequencing data . 
j clin oncol 32 : 579 - 586 , 2014 dawson sj , tsui dw , murtaza m , et al : analysis of circulating tumor dna to monitor metastatic breast cancer . 
n engl j med 368 : 1199 - 1209 , 2013 severson ea , riedlinger gm , connelly cf , et al : detection of clonal hematopoiesis of indeterminate potential in clinical sequencing of solid tumor specimens . blood 131 : 2501 - 2505 , 2018 riedlinger g , hadigol m , khiabanian h , et al : association of jak2 - v617f mutations detected by solid tumor sequencing with coexistent myeloproliferative neoplasms . 
clin cancer res 24 : 4437 - 4443 , 2018 overman mj , lonardi s , wong kym , et al : durable clinical benet with nivolumab plus ipilimumab in dna mismatch repair - decient / microsatellite instabilityhigh metastatic colorectal cancer . 
hodi fs , corless cl , giobbie - hurder a , et al : imatinib for melanomas harboring mutationally activated or amplied kit arising on mucosal , acral , and chronically sun - damaged skj clin oncol 31 : 3182 - 3190 , 2013 9 . 
blazek d , kohoutek j , bartholomeeusen k , et al : the cyclin k / cdk12 complex maintains genomic stability via regulation of expression of dna damage response joshi pm , sutor sl , huntoon cj , et al : ovarian cancer - associated mutations disable catalytic activity of cdk12 , a kinase that promotes homologous recombination repair and resistance to cisplatin and poly ( adp - ribose ) polymerase inhibitors . 
ahluwalia , md5 ; howard colman , md , phd6 ; geoffrey fell , ms1 ; evanthia galanis , md7 ; john de groot , md8 ; jan drappatz , md9 ; andrew b . 
wen , md1 purpose adequately prioritizing the numerous therapies and biomarkers available in late - stage testing for patients with glioblastoma ( gbm ) requires an efcient clinical testing platforwe developed and implemented insight ( individualized screening trial of innovative glioblastoma therapy ) as a novel adaptive platform trial ( apt ) to develop precision medicine approaches in gbm . methods insight compares experimental arms with a common control of standard concurrent temozolomide and radiation therapy followed by adjuvant temozolomide . 
at the initiation of insight , three experimental arms ( neratinib , abemaciclib , and cc - 115 ) , each with a proposed genomic biomarker , are tested simultaneously . 
as the trial progresses , randomization probabilities adapt on the basis of accumulating results using bayesian estimation of the biomarker - specic probability of treatment impact on progression - free survival . treatment arms may drop because of low probability of treatment impact on overall survival , and new arms may be added . 
detailed information on the statistical model and randomization algorithm is provided to stimulate discussion on trial design choices more generally and provide an example for other investigators developing apts . conclusion insight ( nct02977780 ) is an ongoing novel biomarker - based , bayesian apt for patients with newly diagnosed unmethylated gbm . 
clinical trials in the era of precision medicine must consider how to develop biomarker data during the trials , make efcient use of multiplexed biomarker screening , and develop assignment algorithms for patients positive for more than one biomarker . 
 alexander et al master protocols and adaptive platform trials ( apts ) have been proposed as attractive solutions to efciently address multiple therapeutic and biomarker hypotheses.5 - 7 we developed insight ( individualized screening trial of innovative glioblastoma therapy ) , a multisite investigator - initiated phase ii screening apt , as a solution to precision medicine development challenges for patients with gbm . 
insight was specically designed to enable efcient use of randomly assigned controls , generate information to support genomic biomarker development , and leverage the xed cost of trial development across more experimental therapies . methods eligibility patients are eligible for insight if they have newly diagnosed gbm with unmethylated o6 - methylguanine dna methyltransferase ( mgmt ) gene promoters and negative idh1 r132h mutationspecic immunohistochemistry . 
the marginal benet of temozolomide ( tmz ) in patients with unmethylated mgmt promoters8 offers the opportunity to test experimental therapies without combinations with tmz.9 , 10 this potentially accelerates the overall time for drug development ( by not needing prior separate phase i studies with tmz ) and eliminates the potential for subtherapeutic dose of the experimental agent as a result of overlapping toxicity with tmz.2 , 3 insight therefore can support experimental arms with tmz combinations or with the experimental agent alone . 
experimental therapies may also replace tmz in the concurrent radiation therapy ( rt ) portion ( if there is a compelling radiosensitizing hypothesis ) , the adjuvant portion , or both . a pure radiosensitizing agent or experimental rt regimen could theoretically replace standard rt / tmz while keeping the adjuvant tmz intact . eligibility for insight requires sufcient genotyping data to dene the predetermined biomarker categories for arms currently in the trial . 
additional details regarding the initial experimental arms and biomarkers are included in the data supplement . statistical considerations operating characteristics , and secondary analyses use the proportional hazards ( ph ) model for both pfs and os . there are several arguments to support the use of different outcomes for adaptive randomization ( pfs ) and nal efcacy evaluation ( os )  . 
the relationship between accrual rate and event timing is crucial for response - adaptive trials , because effective variation of randomization probabilities requires rapid generation of treatment effect estimates on the basis of an adequate number of individual outcomes . 
in addition , treatment effects may have a stronger signal on pfs , a relationship illustrated previously.12 finally , potential issues with pseudoprogression and pseudoresponse13 , 14 are mitigated by preserving os as the foundation for stopping rules and nal efcacy analyses . that is , promising early results of an experimental treatment accelerate the accrual rate of the corresponding arm without reducing the nal sample size of the other experimental arms . group - specic adaptive randomization probabilities . 
patients are randomly assigned using an adaptive algorithm that updates randomization probabilities for the various arms in each biomarker group monthly.15 the algorithm uses available information generated by insight ( the individual biomarker groups combined with individual pfs ) to determine the randomization probabilities that will be used to allocate patients for the subsequent month . 
the hazard function for each patient assigned to an experimental arm is modeled , rescaling the baseline by a factor that depends on treatment ( main effect ) , biomarker - specic coefcients , and biomarker - treatment interaction terms . 
we previously described the use of ph models for the computation of randomization probabilities.17 we indicate the individual prole withx ( cid : 1 ) ( x1 , x2 , x3 )  . 
the hazard function x , a ( t ) for the timeto - event outcome of a patient with biomarker prole x , randomly assigned to experimental arm a , is proportional to the baseline ( t )  . 
insight will randomly assign a maximum of 70 patients to each experimental arthe sample size for the initial set of arms is 70 patients per arm across four arms , for a total of 280 patients , but there are early stopping rules for futility in each arm , and other arms may be added as the trial is ongoing . 
such an increase will depend on the number of experimental arms added and the time at which they will start enrollment . the later new arms start enrolling , the larger the corresponding sample size expansion will be . 
indeed , when a new experimental arm is added , the design increases the control - specic sample size to guarantee enrollment of 70 patients in the control after the addition of a novel arwe previously described the adjustment of the control sample size with the addition of novel arms and potential futility early stopping of experimental arms in platforms.18 operating characteristics of outcome adaptive randomization are related to the accrual rate relative to the event rate , because information from events is used to alter probability of random assignment for newer patients . 
biomarker frequencies were assumed on the basis of data from prior genomic proling.19 monthly updates of the randomization probabilities are combined with a sequential decision rule that drops experimental arms when there is insufcient preliminary evidence to warrant additional investigation of the treatment based on the primary end point ( os )  . 
we describe a linear boundary that provides thresholds for predictive probabilities to dene the decision rule . 2 of the main effect prior normal distributions were used for the regression parameters  . 
they are a priori independent , and the variance a a is set to have the 80th and 20th percentiles that correspond to ( log [ 2 ] ; duplication of the hazard ) and ( log [ 1 / 2 ] )  . 
 alexander et al whereas for a hypothetic arm added later during the study , it increases with the number of patients randomly assigned to the novel arm and the concomitant random assignments to the control aradaptive randomization intervenes only after the initial burn - in period . as we discussed previously , 17 , 20 to preserve the power of detecting treatment effects , it is important to guarantee sufcient enrollment in the control arrandomization probabilities for the control are obtained by matching ( under the hypothesis that all the active arms will complete accrual and will not be stopped for futility ) the expected number of patients randomly assigned to the control and the planned sample size specic to the control . 
for example , if after 10 enrollments two patients have been assigned to the control , then the 11th patient is assigned to the control with a probability of ( 70 2 ) / ( 280 10 )  . 
the same approach is used if one experimental arm is dropped for futility or a novel arm is added , with the consequence of an expansion of the control sample size.18 burn - in randomization . 
this is an important difference with respect to other adaptive designs , which include a component of competition and negative correlation with the nal number of patients enrolled by different experimental arms . 
the accrual can be stopped earlier for an experimental arm ( before this maximum is reached ) only when the likelihood of a positive nal result becomes insufcient and triggers the early stopping on the basis of futility . 
as a consequence , the adaptive algorithm has a substantial impact on the duration the arm - specic accrual period , which tends to be shortened for the arms with positive treatment effects , with little effect on other operating characteristics . 
bayesian randomization can only modify the enrollment rate and accelerate accrual to the most promising arms , particularly for the patients who are more likely to benet from these treatments . 
we also predict future biomarker proles x using a standard dirichlet conjugate model . monthly , bayesian sampling is used to generate nal trial data from the predictive distribution , including the enrollment of future patients , and pfs and os outcomes , both for patients previously enrolled and for those who have not yet been enrolled . 
using bayesian terminology , we sample multiple times from the predictive distribution every month . these data sets , including the actual data generated up to a time point by the trial and a complementary component of probabilistically imputed data , describe expectation and uncertainty on how we predict the data to look at completion of the study ( including censored data points ) on the the available information . 
these computations basis of assume that the open arms will reach the nal sample size of 70 patients and allow us to derive a single predictive probability of interest for each experimental arm , at each interim analysis , of a well - dened event . 
prediction ( the probability that the arm - specic result will be signicant ) is used monthly to decide either to continue or to discontinue the study of the experimental ara key step of the process is the simulation of the baseline and the ph model parameters from the posterior at each interim analysis . 
these steps are iterated so that the relative frequency of generated arm - specic p values below the signicance threshold approximates the targeted prediction probability . the arm is stopped if the prediction probability of a positive result becomes small . 
a linear boundary that increases with the number of enrollments from 0 at the onset of the study up to 0.1 is used to dene monthly the cutoff for discontinuing or proceeding with the study of the experimental treatment . 
in the comparison of these simulations with a balanced design , keeping the described early stopping mechanism for futility , enrollment in arms with positive treatment effects was completed faster , with an average time reduction between 16% and 27% across simulation scenarios . a similar power analysis like that for pfs was repeated for os . 
although the power to reject the null was of course considerably the power to detect a signicant biomarker / reduced , treatment interaction ( null hypothesis : no treatment effect in the cdk - positive group ) in the secondary analyses was higher ( 0.66 ; table 2 )  . 
the noncompeting maximum number of patients ( ie , 70 ) per arm maintained the power of detecting a positive treatment effect for each experimental arm stable with respect to the presence of treatment effects on the remaining arms . sensitivity to pfs and os correlation seemed limited . 
we considered both different magnitudes of pfs and os hrs contrasting an experimental treatment and a control ( appendix table a2 ) and various pfs - os correlation degrees at the individual level . 
additional sensitivity analyses , including the probability of reporting a positive treatment effect for the biomarker - positive group under selected scenarios ( appendix table a4 ) , the power for arms added later during the course of the platform trial ( appendix table a5 ) , and the power assuming different possible accrual rates ( appendix table a6 ) , are included in the appendix . 
in contrast to alternative response - adaptive designs , the low correlation of accrual rate with nal armspecic sample size ( which , as described in methods , can be fewer than 70 patients only as a result of early stopping for futility ) induces little variations of power estimates across table 2 . 
in the middle column , only a single arm has positive treatment effects restricted to a single biomarker - positive subpopulation ( prevalence , 0.5 ) and hazard ratios ( hrs ) of 1 for the rest of the patients . 
accrual rate therefore correlates with time required to complete the arm evaluation , but it does not correlate with power . discussion clinical trials under master protocols have been proposed as a methodologic innovation to more efciently answer therapeutic development questions.6 , 7 , 22 such innovations are particularly important in the era of precision medicine , where biomarker testing adds complexity by increasing the testable hypotheses . 
platform trials under number of master protocols are intended to study multiple targeted therapies in the context of a single disease in a perpetual manner , with therapies allowed to enter or leave the platform on the basis of a decision algorithm.7 ( p63 ) potential efciencies include the conservation of control arms , multiplexed biomarker screening data , and reduced downtime because the trial infrastructure is maintained as treatment arms enter or leave the trial . 
platforms also enable innovative statistical approaches to increase efciency.23 - 27 insight is the rst biomarker - based apt designed to apply these general solutions to specic problems in therapeutic development for gbm.28 late - stage clinical trial failures are a major issue for therapeutic development in general1 and in gbm specically.2 , 3 failure in phase iii may be linked to erroneous go / no - go decisions on the basis of phase ii results that have different end points than the desired pivotal trial , overestimate treatment effects on the basis of comparisons with historical controls , or both . 
prior data have shown that effects on imaging - based end points such as response rate and pfs may not translate to effects on os.4 , 13 , 29 - 31 furthermore , comparison of end points like pfs and os with historical controls may overestimate treatment effects through selection bias , temporal drift , and failure to account for control variability.4 for these reasons , we chose to use os as the primary end point of in unmethylated gbm , the trial . survival postprogression is generally short , and there are no proven effective therapies at recurrence that increase the chance of detecting a true therapeutic impact on os.12 we included a randomly assigned control arm to avoid the pitfalls associated with comparison with historical controls for os in gbm.4 the platform design affords considerable efciency by using a single control arm for comparison against multiple therapies and offers patients a higher probability of being randomly assigned to an experimental arfurthermore , we use bayesian rar17 based on accumulating pfs results to increase the probability of random assignment to arms that showed more promise.28 , 32 we had previously shown that rar using an os end point was possible for recurrent gbm17 and additionally supported this approach in our simulations during the development of insight . 
however , to increase efciency , we opted to use pfs , because earlier end point assessment can more rapidly inuence randomization.16 if we were to nd a discordance between therapeutic impact on pfs and os , randomization probability would be altered , but decision making on the primary end point would remain unchanged . another advantage of platform trials is the efcient use of multiplexed genomic biomarker data for treatment assignments . 
gbm is characterized by redundant and overlapping alterations in several molecular pathways rather than mutually exclusive driver mutations.33 as such , patients can be positive for multiple genomic biomarkers . some platform trials like nci - match ( national cancer institute molecular analysis for therapy choice ) , 34 lung map ( lung cancer master protocol ) , 35 battle ( biomarkerintegrated approaches of targeted therapy for lung cancer elimination ) , 36 and n2m2 ( national center for tumor diseases neuro master match ) 37 generally deal with this situation through an assignment algorithm on the basis of relative evidence of biomarker - specic accrual and / or therapeutic efcacy . i - spy 2 ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) , in contrast , uses biomarker subgroupspecic randomization probabilities to allow data generated during the trial to drive the biomarker specicity of arm assignments.38 insight does the latter , starting with equal randomization among the experimental arms and allowing the rar procedure to prioritize randomization in a biomarker - specic way . 
for example , if only patients with egfr amplication in the neratinib arm were living longer than those in the control , the randomization algorithm would increase the probability of egfr - amplied patients assigned to neratinib ( regardless of their other biomarkers ) while potentially reducing assignment to neratinib for egfr wild - type patients . in fact , this situation occurred in i - spy 2 , where the adaptive randomization algorithm stopped assigning patients with human epidermal growth factor receptor 2 ( her2 ) negative / hormone receptorpositive cancer and those with her2negative / hormone receptornegative cancer to neratinib during the course of the trial , even as it reached the prespecied efcacy threshold in the her2 - positive / hormone receptor negative signature.39 this strategy may be optimal when there are limited pretrial data or a weak hypothesis suggesting a biomarker - specic effect . 
in these situations , more biomarker specicity may be desired from the start of the trial , and we have suggested ways to integrate this into a platform design.40 more generally , adding future biomarkers specic to additional experimental arms increases design complexity and requires appropriate denitions of the randomization probabilities . 
even though insight used randomization , we queried clinically annotated genomic data33 , 43 to investigate the possibility that the biomarkers we used had prognostic signicance or a variable relationship between pfs and os and found no such associations.19 although the perpetual clinical provided by the apt framework can provide signicant efciencies , it can create additional challenges as well . maintaining ongoing operations requires both nancial framework that trial models that support ongoing concerns and active pipeline development to maintain a regular ow of experimental arms . 
more complex bayesian designs require engaged clinical and statistical investigators and new ways of determining operating characteristics through simulation.44 reporting of trial results is complicated because of the separation between the master protocol and the armspecic data . 
arms that leave the trial because of success or failure need to be reported while the overall trial is still ongoing , which does not lend itself to traditional trial reporting best practices like consort . 
two recent publications from i - spy 2 are examples.39 , 45 conversely , reporting on the overall master protocol does not have a natural time point , although most groups publish a general description of the overall trial structure without results.35 , 36 , 38 , 41 in conclusion , insight is an ongoing novel biomarkerbased bayesian apt for patients with newly diagnosed unmethylated gbm . 
ahluwalia stock and other ownership interests : mimivax honoraria : prime oncology , elsevier , itamar medical ( i ) consulting or advisory role : monteris medical , astrazeneca , bristol - myers squibb , abbvie , cbt pharmaceuticals , kadmon , vbi vaccines research funding : novartis , tracon pharma , novocure , spectrum pharmaceuticals , eli lilly / imclone , boehringer ingelheim , astrazeneca howard colman honoraria : merck sharp & dohme consulting or advisory role : genentech , roche , novocure , omniox , insys therapeutics , abbvie research funding : newlink genetics , plexxikon , kadmon , orbus therapeutics , merck , dnatrix , abbvie , beigene evanthia galanis consulting or advisory role : genentech / roche ( inst ) , abbvie ( inst ) , oncorus research funding : genentech / roche ( inst ) , merck ( inst ) john de groot employment : helsinn therapeutics ( i ) , ziopharm oncology ( i ) leadership : ziopharm oncology ( i ) stock and other ownership interests : gilead sciences , ziopharm oncology ( i ) consulting or advisory role : celldex , deciphera , vascular biogenics , foundation medicine , genentech / roche , omniox , oxigene , abbvie , novogen , kadmon , merck , five prime therapeutics , insys therapeutics , astrazeneca , boston biomedical , gw pharmaceuticals , carthera research funding : deciphera , novartis , eli lilly , sano , emd serono , mundipharma patents , royalties , other intellectual property : sano , research support ; astrazeneca , research support ; emd serono , research support ; eli lilly , research support ; novartis , research support ; deciphera pharmaceuticals , research support jan drappatz employment : via oncology stock and other ownership interests : exelixis , bristol - myers squibb honoraria : uptodate , via oncology consulting or advisory role : oncorus , immunomix patents , royalties , other intellectual property : uptodate andrew b . 
burt nabors consulting or advisory role : bristol - myers squibb speakers bureau : merck / schering plough sandro santagata consulting or advisory role : rarecyte david schiff consulting or advisory role : orbus therapeutics , monteris medical , cavion ( inst ) research funding : bayer healthcare pharmaceuticals ( inst ) mary r . 
wen consulting or advisory role : abbvie , genentech / roche , agios , astrazeneca , karyopharm therapeutics , vivus , monteris medical , aurora biopharma , vascular biogenics , kadmon , ziopharm oncology , gw pharmaceuticals , eli lilly , immunomic therapeutics speakers bureau : merck , agios ( inst ) , abbvie ( inst ) , angiochem ( inst ) , genentech / roche ( inst ) , glaxosmithkline ( inst ) , astrazeneca ( inst ) , immunocellular therapeutics ( inst ) , karyopharm therapeutics ( inst ) , merck ( inst ) , novartis ( inst ) , oncoceutics ( inst ) , sano ( inst ) , ariad pharmaceuticals ( inst ) , vascular biogenics ( inst ) , eli lilly no other potential conicts of interest were reported references thomas dw , burns j , audette j , et al : clinical development success rates 2006 - 2015 . 
j clin oncol 35 : 2402 - 2409 , 2017 vanderbeek am , rahman r , fell g , et al : the clinical trials landscape for glioblastoma : is it adequate to develop new treatments ? neuro oncol 20 : 1034 - 1043 , 2018 grossman sa , schreck kc , ballman k , et al : point / counterpoint : randomized versus single - arm phase ii clinical trials for patients with newly diagnosed glioblastoma . 
nat rev clin oncol 9 : 199 - 207 , 2011 berry sm , connor jt , lewis rj : the platform trial : an efcient strategy for evaluating multiple treatments . 
n engl j med 377 : 62 - 70 , 2017 stupp r , hegi me , mason wp , et al : effects of radiotherapy with concomitant and adjuvant temozolomide versus radiotherapy alone on survival in glioblastoma in a randomised phase iii study : 5 - year analysis of the eortc - ncic trial . 
alexander bm , trippa l : getting it rst versus getting it right : weighing the value of and evidence for progression - free survival as a surrogate endpoint for overall survival in glioblastoma . 
han k , ren m , wick w , et al : progression - free survival as a surrogate endpoint for overall survival in glioblastoma : a literature - based meta - analysis from 91 trials . neuro - oncol 16 : 696 - 706 , 2014 30 . 
herbst rs , gandara dr , hirsch fr , et al : lung master protocol ( lung - map ) : a biomarker - driven protocol for accelerating development of therapies for squamous cell lung cancerswog s1400 . 
pfaff e , kessler t , balasubramanian gp , et al : feasibility of real - time molecular proling for patients with newly diagnosed glioblastoma without mgmt promoter hypermethylation : the nct neuro master match ( n2m2 ) pilot study . 
the phosphatidylinositol 3 - kinase ( pi3k ) / akt / mtor signaling axis plays a central role in cell growth , survival , motility , and metabolism in a variety of cancers ( fruman da , et al : nat rev drug discov 13 : 140 - 156 , 2014 ; engelman ja : nat rev cancer 9 : 550 - 562 , 2009 ) , including glioblastoma ( gbm ; brennan cw , et al : cell 155 : 462 - 477 , 2013 )  . 
dna - dependent protein kinase is a serine / threonine kinase involved in the repair of dna double - strand breaks ( collis sj , et al : oncogene 24 : 949 - 961 , 2005 ) , which are considered to be the most lethal dna lesions and the main driver of cellular death after treatment with ionizing radiation therapy ( rt )  . 
therefore , beyond its hypothesized growth - inhibitory effect as monotherapy , cc - 115 has the potential to be a radiation - sensitizing agent in the treatment of gbm ( zhao y , et al : cancer res 66 : 5354 - 5362 , 2006 )  . 
one phase ia / ib multicenter open - label clinical study established 10 mg twice per day as the recommended dose for cohort expansion and phase ii with near - maximal inhibition of phosphorylated akt and partial inhibition of phosphorylated 4ebp ( munster pn , et al : j clin oncol 34 , 2016 [ suppl ; abstr 2505 ] )  . 
because this dose has never been combined with rt , the treatment arm will start with a safety lead - in with the combination before expansion to the full phase ii setting . abemaciclib retinoblastoma ( rb ) protein is a key tumor suppressor that inhibits progression through the g1 checkpoint ( sherr cj : science 274 : 16721677 , 1996 )  . 
abemaciclib is a highly specic atp - competitive cdk4 / 6 inhibitor that induces reversible g1 phase cell - cycle arrest in rb - procient tumor models and is approved for hormone receptorpositive , human epidermal growth factor receptor 2 ( her2 ) negative advanced or metastatic breast cancer . orally dosed abemaciclib achieved brain exposures in excess of the concentrations required for cdk4 / 6 inhibition in an orthotopic rat gbm model and signicantly increased survival alone or in combination with tmz ( raub tj , et al : drug metab dispos 43 : 1360 - 1371 , 2015 )  . 
neratinib , an orally available potent irreversible small - molecule panerbb family tyrosine kinase inhibitor that targets the intracellular tyrosine kinase domains in egfr , is approved for her2 - positive breast cancer ( martin m , et al : lancet oncol 18 : 1688 - 1700 , 2017 ; cancer discov 7 : of1 , 2017 ) 39 and has shown activity in controlling and delaying cns progression of breast cancer metastases ( awada a , et al : jama oncol 2 : 1557 - 1564 , 2016 )  . 
in preclinical gbm studies , neratinib was shown to selectively cause cell death in cell lines harboring genetic activation of egfr and was more effective than other egfr inhibitors in lines harboring the extracellular domain mutations seen in gbm ( vivanco i , et al : cancer discov 2 : 458 - 471 , 2012 )  . 
neratinib has also been shown to exhibit potential for potent inhibition of amplied egfrvii and egfrviii in gbm patient - derived cell - line models ( francis jm , et al : cancer discov 4 : 956 - 971 , 2014 )  . 
neratinib is signicantly more potent than lapatinib in limiting the growth of primary gbm cell lines , and this increased potency is an attractive feature , given that negative clinical trials for lapatinib have been attributed to inadequate tumor concentrations of the drug ( vivanco i , et al )  . 
neratinib will be administered in place of tmz after standard concurrent rt / tmz . biomarkers prospective patients may have biomarker data already available from academic or commercial sources , or they may take advantage of a companion consortium ( abc2 allele consortium ) that generates free portable genotyping data using whole - exome sequencing and copy array testing performed in a clinical laboratory improvement amendmentscertied clinical laboratory for patient use in clinical trials . 
the biomarkers determined are as follows : egfr positive dened as patients with egfr amplication or mutation ; pi3k positive dened as patients with pik3ca mutation / amplication , pik3r1 mutation , akt3 amplication , pik3c2b  . 
one copy gain , or pten dual allele inactivation through either homozygous deletion or deletion plus an inactivating mutation ; and cdk positive dened as patients with rb1 wild type and cdk4 amplication , cdk6 amplication , or cdkn2a or cdkn2b  . 
one copy loss , or cdkn2a or cdkn2b one copy loss plus an inactivating mutation . for amplications listed , the genotyping report must state clear gene amplication and not gain , which is typically greater than a log2 ratio of + 2.0. 
copy number losses would be values of , 0.3 , and more than single copy deletions are inferred relative to baseline for the chromosome on which they are located ( eg , single copy chromosome 9 loss with additional loss of cdkn2a / b below this level in focal region )  . 
ve prior events reported in cosmic or are well - established hotspots known to be activating or inactivating mutations through experimental data or novel mutations that are predicted to be clearly inactivating , such as nonsense and frameshift mutations . 
 reliable pan - cancer microsatellite instability assessment by using targeted next - generation sequencing data purpose microsatellite instability ( msi ) / mismatch repair ( mmr ) status is increasingly important in the management of patients with cancer to predict response to immune checkpoint inhibitors . 
we determined msi status from large - panel clinical targeted next - generation sequencing ( ngs ) data across various solid cancer types . methods the msi statuses of 12 , 288 advanced solid cancers consecutively sequenced with memorial sloan kettering - integrated mutation profiling of actionable cancer targets clinical ngs assay were inferred by using msisensor , a program that reports the percentage of unstable microsatellites as a score . 
of 9 , 591 non - crc / uec tumors with mss msisensor status , 456 ( 4.8% ) had slightly elevated scores ( 3 and < 10 ) of which 96.6% with available material were confirmed to be mss by msi pcr . 
msisensor correctly scored all 15 polymerase ultra - mutated cancers as negative for msi . conclusion msi status can be reliably inferred by msisensor from large - panel targeted ngs data . 
these sites are prone to dna replication errors as a result of dna polymerase slippage , which is effectively corrected through the mismatch repair ( mmr ) systedeficiencies in mmr result in increased variation at genomic loci with mononucleotide repeats . 
 drug approved for any solid tumor with a specific genetic feature ( msi - high [ msi - h ] status ) on the basis of new data that confirm its activity across 12 different cancer types , with complete responses observed in 21% of patients.5 until now , the gold standard for assessment of msi , a reliable screen for functional mmr status , has been concurrent analysis of patient tumor and normal dna for five mononucleotide microsatellite loci with pcr . 
in recent years , reports have shown that next - generation sequencing ( ngs ) facilitates identification of patients with deficiencies in the mmr pathway by comparing sequencing reads around microsatellite regions in the tumor and the matched normal or by counting mutations identified in exons . 
hause et al6 identified msi / mmr across a wide spectrum of tumor types surveyed by the cancer genome atlas but with limited validation data available in only a subset of crc / uecs and stomach cancers . 
msk - impact is an ngs assay that uses tumor and matched normal dna to identify somatic mutations , structural variants , and copy number alterations in all coding regions and select introns of 341 ( version 1 ) , 410 ( version 2 ) , or 468 ( version 3 ) cancer - related genes.7 tumor purity ( tp ) was estimated with a combination of median variant allele frequency of mutations identified in each sample and microscopic analysis of hematoxylin and eosinstained specimens . sufficient coverage in a tumor / normal pair where it identifies deletion length variation . 
x2 test is used to identify the significantly varied loci , and the percentage of unstable loci , after multiple testing correction is performed on the p values , is reported as an msisensor score ; additional details have been previously published.9 this score was used to infer msi / mmr status from ngs data in the current study . 
non - neoplastic colonic mucosa and colorectal tumors known to be deficient of mlh1 , msh2 , msh6 , and pms2 were used as external positive and negative controls , respectively . 
retained expression of each protein was defined by nuclear ihc reactivity of tumor cells , whereas loss of expression for each protein was defined by the complete absence of nuclear ihc reactivity of tumor cells . 
for the purposes of this study , all tumors with fewer than two unstable loci were interpreted as microsatellite stable ( mss )  . msisensor score analysis and cutoff determination proper detection of msi - h / mmr - d status from ngs data by using msisensor depends on whether the tumor is analyzed against its matched normal sample , because analysis with an unmatched sample results in significant inflation of the msisensor scores ( p , .001 ; appendix fig a1 )  . 
alignment files generated from the msk - impact pipeline in binary alignment map format were analyzed by using msisensor on all matched tumor - normal pairs and then separately on all unmatched tumor samples to generate the score . 
msisensor was run at the following successive dilutions : 100% tumor dna , 50% tumor dna and 50% normal dna , 25% tumor dna and 75% normal dna , 12% tumor dna and 88% normal dna , and 6% tumor dna and 94% normal dna . 
we used a total tp threshold of > 25% for this application of msisensor . mutation burden and mutational signatures tumor mutation burden ( tmb ) was calculated by dividing the total number of reported mutations by the genomic area where mutations were reported for each sample . 
these mutations were resampled 1 , 000 times and then subjected to decomposition analysis in which the kullback - leibler divergence is minimized between the sample signature and the approximation built up from 30 signatures such that each signature is assigned a weight that corresponds to the percentage of mutations explained by each given signature . 
40% of observed mutations were attributable to that signature.10 survival analysis time from procedure date to last follow - up was used for survival analysis among patients whose biopsy date and sequencing date were within 1 year of each other . 
the survival package in r version 3.2 was used for the survival analysis . results validation of msisensor in crc and uec samples one hundred thirty - eight crc and 40 uec samples with matched normals were selected for orthogonal msi / mmr status by pcr / ihc and used as the training data set for msisensor score threshold determination . 
 ( a ) green points indicate samples where orthogonal methodology indicated microsatellite stable ( mss ) phenotype ; red points indicate samples where a microsatellite instabilityhigh ( msi - h ) phenotype is observed . 
 ( c ) a poorly differentiated crc ( hematoxylin and eosin [ he ] stain ) with ( d ) mlh1 and ( e ) pms2 loss only had one unstable locus , ( f ) mono - 27 ( arrows ) , and was not msi - h by polymerase chain reaction , whereas ( g ) msisensor detected msi - h status with > 10% of loci with instability . 
from 10 , 900 patients , 11 , 553 samples had sufficient coverage of 2003 and tp of > 25% [ as described in analytic ( technical ) sensitivity ] and matched normal samples for analysis . 
among the patients without crc / uec , bladder cancer ( 11 [ 3.1% ] of 355 ) , esophagogastric carcinoma ( seven [ 2.5% ] of 282 ) , and prostate cancer ( 12 [ 1.7% ] of 722 ) had msi - h incidence . 
forty - six were concordant ( pcr , n = 39 ; ihc , n = 7 ) , whereas three were msi low ( msi - l ) by pcr but were mmr - d by ihc ( figs 1c - 1g ) , including a carcinoma of unknown primary with 16 mutations , a squamous cell carcinoma with 65 mutations , and a prostate carcinoma with 44 mutations . 
of note , use of the msisensor on targeted panel ngs data had higher clinical sensitivity as a screen for mmr - d than msi pcr . exome data and validated at a cutoff score of 3.5 from an average of 10 , 000 evaluable microsatellites per sample.9 msk - impact covers less of the genome with higher coverage , with approximately 1 , 000 evaluable microsatellites per sample . this number has increased with the addition of genes to the msk - impact panel ( appendix fig a3 )  . 
with consideration of the different cutoffs between the present and previous studies , we also evaluated the 456 ( 4.8% ) of 9 , 591 msk - impact non - crc / uecs with slightly elevated msisensor scores ( > 3 and , 10 )  . 
of note , three samples ( a germ cell tumor with two mutations , a cancer of unknown primary with 16 mutations , and a uterine sarcoma with 19 mutations ) that were msi - h by both msisensor and pcr had , 20 exonic mutations in mskimpact , a cutoff shown to be highly predictive of msi - h in crc samples.9 analysis of msi status in unmatched tumors because most clinical laboratories that offer ngs testing use a pooled unrelated normal rather than a matched normal , we investigated whether and at what cutoff msisensor could be used for unmatched tumors . 
 colorectal cancer ( n = 1 , 030 ) endometrial cancer ( n = 270 ) prostate cancer ( n = 820 ) bladder cancer ( n = 369 ) esophagogastric carcinoma ( n = 302 ) cancer of unknown primary ( n = 254 ) nonsmall - cell lung cancer ( n = 1 , 619 ) small bowel cancer ( n = 32 ) head and neck carcinoma ( n = 210 ) pancreatic cancer ( n = 578 ) skin cancer , nonmelanoma ( n = 133 ) biliary cancer ( n = 242 ) germ cell tumor ( n = 298 ) uterine sarcoma ( n = 99 ) gi neuroendocrine tumor ( n = 46 ) mesothelioma ( n = 127 ) renal cell carcinoma ( n = 380 ) small - cell lung cancer ( n = 94 ) soft tissue sarcoma ( n = 478 ) thyroid cancer ( n = 238 ) breast carcinoma ( n = 1 , 498 ) ovarian cancer ( n = 240 ) melanoma ( n = 420 ) adrenocortical carcinoma ( n = 30 ) glioma ( n = 628 ) gestational trophoblastic disease ( n = 13 ) gi stromal tumor ( n = 165 ) meningothelial tumor ( n = 33 ) osteosarcoma ( n = 56 ) salivary carcinoma ( n = 116 ) chordoma ( n = 20 ) embryonal tumor ( n = 91 ) ependymomal tumor ( n = 18 ) hepatocellular carcinoma ( n = 115 ) histiocytosis ( n = 22 ) nerve sheath tumor ( n = 21 ) sellar tumor ( n = 7 ) sex cord stromal tumor ( n = 21 ) validation status validated msi - h / mmr - d validated mss / mmr - p not validated msisensor score fig 2 . 
validation showed high concordance , with only two cancers with msi - h / mismatch repair deficiency status by polymerase chain reaction / ihc that were , 10 by msisensor . 
mmr - d , mismatched repair deficient ; mmr - p , mismatched repair proficient ; mss , microsatellite stable . known hotspot mutations in pole12 ( table 2 )  . 
our analysis of survival status for msi - h compared with mss in cancer types where we identified at least 10 patients with msi - h status showed no significant difference after adjusting for age ( fig 4 )  . 
 ( a ) for cancers with high tmb and microsatellite stable results on the basis of msisensor , ( b ) other signatures were identified , including uv exposure , apobec deficiency , smoking , temozolomide ( tmz ) treatment , and polymerase e ( pole ) deficiency . 
 ( c ) on the other hand , mismatch repair - deficient ( mmr - d ) / microsatellite instabilityhigh ( msi - h ) samples showed similar rates of tmb . 
although colorectal cancer ( crc ) showed a trend of better survival for patients with msi - h status ( p = .057 ) , other tumor types did not show a significant association between msi status and survival . 
although the bias in our data set may underestimate the total number of msi - h tumors across all patients with cancer , it gives a more accurate estimate of the proportion of patients with advanced solid cancers who may be eligible for immune checkpoint inhibition on the basis of msi - h status . although mutation rate has been used to infer msi status in crc , 10 , 14 various other hypermutation signatures ( pole , uv , smoking , temozolomide ) also are associated with an increased mutation rate in other tumor types . 
klimstra provision of study material or patients : liying zhang , justyna sadowska , jinru shia collection and assembly of data : sumit middha , liying zhang , khedoudja nafa , gowtham jayakumaran , justyna sadowska , deborah f . 
delair , ahmet zehir , jaclyn f . hechtman data analysis and interpretation : sumit middha , liying zhang , khedoudja nafa , gowtham jayakumaran , donna wong , hyunjae r . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . sumit middha no relationship to disclose liying zhang no relationship to disclose khedoudja nafa no relationship to disclose gowtham jayakumaran no relationship to disclose donna wong no relationship to disclose hyunjae r . 
berger consulting or advisory role : cancer genetics , sequenom zsofia stadler consulting or advisory role : allergan ( i ) , genentech ( i ) , roche ( i ) , regeneron pharmaceuticals ( i ) , optos ( i ) , adverum biotechnologies ( i ) david s . 
klimstra stock and other ownership interests : paige.ai consulting or advisory role : wren laboratories , ipsen marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network / boehringer ingelheim afatinib targeted therapy advisory committee , national comprehensive cancer network / astrazeneca tagrisso rfp advisory committee research funding : loxo ( inst ) ahmet zehir no relationship to disclose jaclyn f . 
hechtman jf , middha s , stadler zk , et al : universal screening for microsatellite instability in colorectal cancer in the clinical genomics era : new recommendations , methods , and considerations . 
ribic cm , sargent dj , moore mj , et al : tumor microsatellite - instability status as a predictor of benefit from fluorouracil - based adjuvant chemotherapy for colon cancer . 
le dt , durham jn , smith kn , et al : mismatch repair deficiency predicts response of solid tumors to pd - 1 blockade . 2520 , 2015 science 357 : 409 - 413 , 2017 6 . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
stadler zk , battaglin f , middha s , et al : reliable detection of mismatch repair deficiency in colorectal cancers using mutational load in next - generation sequencing panels . 
metrics table with number of tumors , median msisensor score , and median number of exonic mutations all samples ( 10 ) mss ( msisensor < 10 ) msi - h ( msisensor 10 ) general tumor type frequency median exonic mutation median no . 
metrics table with number of tumors , median msisensor score , and median number of exonic mutations ( continued ) all samples ( 10 ) mss ( msisensor < 10 ) msi - h ( msisensor 10 ) general tumor type frequency median exonic mutation median no . 
 ras mutations are associated with inferior progression - free survival and overall survival of patients with mcrc compared with patients with nonmutated tumors.1 it is conceivable that ras mutations are negative prognostic factors per se ; however , the availability of only one actionable molecular target , that is , the inhibition of angiogenesis , in patients with mutated tumors certainly affects survival in this subgroup of patients . 
recent studies have demonstrated that the analysis of circulating tumor dna ( ctdna ) in blood samples , through its ability to recapitulate tumor heterogeneity , is a remarkable surrogate of tumor biopsy for mutation detection.2 extensive research on liquid biopsy led to significant achievements in the comprehension of the biologic reasons behind acquired resistance to anti - egfr therapies.3 to date , studies with liquid biopsy have been selectively concentrated on the appearance of ras - mutant clones in the blood of patients with ras wild - type primary crc , as biomarkers of anti - egfr therapy resistance . 
we here report that ctdna analysis , over the course of antiangiogenic treatment , might reveal a therapeutically exploitable window of opportunity , characterized by the relative prevalence of ras wild - type clones over time . 
a whole - body contrast enhanced computed tomography ( ct ) scan revealed a left supraclavicular lymphadenopathy , transverse colon thickening ( 3 cm ) , multiple chest and abdominal lymphadenopathies , and peritoneal carcinomatosis . 
mutational analysis of the lymph node metastasis performed through real - time polymerase chain reaction ( pcr ; real - time oncoscreen nras ) revealed exon 4 nras a146t mutation at 29 cycles . 
serum tumor markers significantly decreased , with rapid negativization ( carcinoembryonic antigen [ cea ] , 1.31.23 ; ca 19 - 9 , 71.839 ; ca - 125 , 8226 )  . 
at that time , serum tumor markers increased again ( ca 19 - 9 , 530 ; cea , 9 ) , with clinical evidence of bilateral axillary lymph node enlargement . 
concurrently , the patient was enrolled in an observational study open at our institution , which aimed to serially monitor the mutational status of ctdna in patients with ras - mutant mcrc disease , before starting any new line of treatment and in course of therapy until progression . methods blood samples were prospectively collected after obtaining informed consent with ethical committee approval . 
idylla ( biocartis , nv , mechelen , belgium ) , a fully automated , realtime pcr - based molecular diagnostics system , was used to investigate ras mutational profile from plasma . 
the first allows the detection of 21 mutations in codons 12 , 13 , 59 , 61 , 117 , and 146 of the kras gene , and the second allows the detection of 18 mutations in codons 12 , 13 , 59 , 61 , 117 , and 146 of the nras gene , five mutations in codon 600 of the braf gene , and two mutations in codon 492 of the egfr gene from 1 ml of plasma . among the parameters describing the generated pcr curves , the cq value is calculated as the difference between the quantification cycle value ( cq ) of the gene control signal and the cq of the mutant signal . 
according to the manufacturer 's instructions , a cq value of the nras control of 35.5 or higher indicates that a low amount of cell - free dna is present in the sample . 
in such cases , low - frequency mutations may not be detected . results in july 2017 , a ctdna mutational analysis was performed and revealed the absence of any clinically relevant mutation in kras , nras , and braf genes . 
this new insight into the biology of the disease convinced us to take this window of therapeutic opportunity , which was not guaranteed to remain open indefinitely ; in july 2017 , the treatment was changed to the second - line combination of irinotecan and cetuximab . 
as early as after the first cycle of chemotherapy , an objective complete clinical response of the bilateral axillary adenopathy was documented , and this was confirmed at ultrasound assessment . 
restaging ct scan after eight cycles of therapy showed a partial response , with significant reduction of pleural effusion and pulmonary lymphangitic carcinomatosis and stability of peritoneal metastases ( fig 1 )  . 
a second ctdna analysis was performed on november 2017 , confirming the ras genes wild - type status ( cq of nras total : 35.5 , which might be due to a reduction in ctdna amount )  . 
 june 2017 ( before folfiri - cetuximab ) october 2017 ( after 3 months of folfiri - cetuximab ) pleural effusion pulmonary lymphangitic carcinomatosis malignant ascites peritoneal carcinosis fig 1 . 
axial computed tomography scan after eight cycles of fluorouracil , leucovorin , and irinotecan ( folfiri ) plus cetuximab shows a partial response , with significant reduction of pleural effusion and pulmonary lymphangitic carcinomatosis and stability of peritoneal metastases . 
 sequence of treatments , clinical and radiologic response to the different schedules adopted ( partial response [ pr ] is indicated by blue arrow , and progressive disease [ pd ] is indicated by red arrow ) , and molecular tests performed on tumor tissue and plasma at different time points . 
bev , bevaci zumab ; cet , cetuximab ; ctdna , circulating tumor dna ; folfiri , fluoro uracil , leucovorin , and irinotecan ; folfoxiri , fluorouracil , leucovorin , oxaliplatin , and irinotecan ; fu , fluorouracil . 
nevertheless , a146t results in increased nras activity and downstream signaling and is transforming in cell culture resulting from increased nras guanosine diphosphate / guanosine triphosphate exchange rate , 4 and consequently patients who harbor mutations in nras also have significantly inferior anti - egfr treatment outcomes benefit compared with those without any ras mutations.5 it is recommended that patients with crc being considered for anti - egfr therapy must receive ras mutational testing , including kras and nras codons 12 and 13 of exon 2 , 59 , and 61 of exon 3 and 117 and 146 of exon 4 , and that anti - egfr should only be prescribed for patients with mcrc who are wild type for all known ras - activating mutations.6 in patients with ras - mutant primary colorectal cancers , ineligible for egfr inhibitors , the importance of the egfr pathway , which indeed sustains the disease , is counterintuitive . 
international guidelines currently recommend treatment of ras mutant mcrc with bevacizumab first line , followed by chemotherapy backbone change or aflibercept / ramucirumab at disease progression.7 preclinical and clinical data , however , demonstrate that tumor angiogenesis inhibition induces biologic changes in tumor - stroma interactions , mainly derived from hypoxia . 
preclinical observations suggest that hypoxia exerts a negative selection against ras - mutant clones through a mechanism known as secretory senescence , in which ras - mutant senescent cells operate in a paracrine manner to support the growth of surrounding ras wild - type clones , leading to their relative prevalence over time.8 we here report that ctdna analysis , under table 1 . 
 antiangiogenic treatment , might reveal a therapeutically exploitable window of opportunity , characterized by the relative prevalence of ras wild - type clones , which can be converted in a clinically meaningful benefit for patients . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . paola gazzaniga no relationship to disclose cristina raimondi no relationship to disclose federica urbano no relationship to disclose the following represents disclosure information provided by authors of this manuscript . 
modest dp , ricard i , heinemann v , et al : outcome according to kras - , nrasand brafmutation as well as kras mutation variants : pooled analysis of five randomized trials in metastatic colorectal cancer by the aio colorectal cancer study group . 
sorich mj , wiese md , rowland a , et al : extended ras mutations and anti - egfr monoclonal antibody survival benefit in metastatic colorectal cancer : a meta - analysis of randomized , controlled trials . 
sepulveda ar , hamilton sr , allegra cj , et al : molecular biomarkers for the evaluation of colorectal cancer : guideline summary from the american society for clinical pathology , college of american pathologists , association for molecular pathology , and american society of clinical oncology . 
genomic profiling was performed on 703 appendiceal cancer specimens to compare the mutation profiles of appendiceal subtypes to crc and other cancers , with the ultimate aim to identify potential biomarkers and novel therapeutic targets . methods tumor specimens were submitted to a clinical laboratory improvement amendmentscertified laboratory ( foundation medicine , cambridge , ma ) for hybrid - capturebased sequencing of 3 , 769 exons from 315 cancer - related genes and 47 introns of 28 genes commonly rearranged in cancer . 
kras ( 35% to 81% ) and gnas ( 8% to 72% ) were the most frequent alterations in epithelial cancers ; apc and tp53 mutations were significantly less frequent in appendiceal cancers relative to crc . 
the mutation status of gnas and tp53 strongly predicted os ( median , 37.1 months for tp53 mutant v 75.8 gnas - tp53 wild type v 115.5 gnas mutant ; log - rank p = .0031 ) and performed as well as grade in risk stratifying patients . conclusion epithelial appendiceal cancers and goblet cell carcinoids show differences in kras and gnas mutation frequencies and have mutation profiles distinct from crc . 
2018 by american society of clinical oncology introduction the rarity of appendiceal neoplasms has made it difficult to conduct prospective or randomized clinical trials to guide therapy for these tumors . 
 the small number of appendiceal tumors that are detected , in many cases as an incidental finding in < 1% of appendectomy specimens , 1 comprise multiple histopathologic subtypes , including noninvasive mucinous neoplasms , mucinous and nonmucinous adenocarcinomas , carcinoids , goblet cell carcinoids ( gccs , now also called goblet cell tumors ) , and signet ring cell carcinomas.2 early - stage cancers can be treated definitively with surgery , and selected patients derive long - term benefit from cytoreductive surgery and heated intraperitoneal chemotherapy ( hipec ) .3 however , there is no standard of care for the systemic treatment of advanced , unresectable disease . in the absence of randomized phase iii data , the majority of medical oncologists use colorectal cancer ( crc ) chemotherapy regimens for the treatment of unresectable epithelial appendiceal neoplasms , as is currently recommended by the national comprehensive cancer network guidelines . 
clinical and demographic patient characteristics by subtype median age ( years ) sex ratio m : f subtype mucinous adenocarcinoma adenocarcinoma goblet cell carcinoid pseudomyxoma peritonei signet ring carcinoma 43 : 57 42 : 58 36 : 64 46 : 54 49 : 51 mutation analysis revealed kras to be the most frequently mutated gene in mad ( 77% ) , ad ( 56% ) , and pmp ( 81% ) and the second most frequently mutated gene in srcc ( 35% )  . 
in contrast , kras mutations were significantly less frequent in gccs ( 13% ; 2 p < .001 ) , where tp53 ( 33% ) was the most frequently mutated gene ( fig 1b ; appendix fig a1a )  . 
braf , brca1 , cdkn1b , cdkn2a , myc , pten , and tgfbr2 mutations were present in < 10% of cases across all subtypes ( table 2 )  . 
gnas and kras were the only gene pair significantly comutated ( odds ratio , 6.8 ; bonferroni corrected p = 8.6x10 - 17 ) ; gnas and tp53 were the only gene pair significantly mutually exclusive ( odds ratio , 0.20 ; bonferroni corrected p = 6.7x10 - 13 ; fig 1c ; data supplement )  . pathway - based analysis of mutation profiles genetic aberrations were subsequently grouped by signaling pathway ( appendix table a1 )  . 
 components of the ras / raf signaling pathway ( ie , braf , hras , kras , and nras ) were the most frequently altered genes in epithelial appendix cancers , occurring in > 80% of mads and pmps , 60% of ads , but only 33% of gccs ( 2 p < .001 ; fig 1d )  . 
alterations in homologous recombination deficiency genes were observed in > 50% of all subtypes but were most prevalent in srcc ( 80% ) fluorouracil , leucovorin , and oxaliplatin ; fluorouracil , leucovorin , and irinotecan ; and targeted agents in appendiceal adenocarcinomas compared with crc , 8 , 9 it is known that appendiceal neoplasms have a better prognosis after cytoreductive surgery with hipec treatment.10 there is also a growing body of data showing that there are clear molecular differences between appendiceal and colorectal cancers.11 - 14 here we present a cohort of 703 molecularly profiled appendiceal neoplasms , the largest such cohort to date in this rare disease . 
comparing the mutational landscapes across histologic subtypes we find significant differences in kras , gnas , and fat3 mutation prevalence and confirm that mutational profiles of appendiceal neoplasms are distinct from crc and other gi cancers . 
 in addition , we identify that patients can be risk stratified using the combined mutation status of gnas and tp53 and that outcomes are favorable for patients with kras wild - type disease when treated with irinotecan . results mutation landscape of appendiceal neoplasms the 703 cases were categorized into four different histopathological subtypes consistent with the recently updated consensus classification from the peritoneal surface oncology group international ; in addition , cases of pseudomyxoma peritonei ( pmp ) were included , because this syndrome usually arises from the appendix.2 the majority were either mucinous adenocarcinomas ( mad , 46% ) or adenocarcinomas ( ad , 30% ) , with the rest being gccs ( 12% ) , pmps ( 7.7% ) , or signet ring cell carcinoma ( srcc , 5.3% ; appendix ; table 1 )  . 
the majority of specimens submitted for sequencing came from intraperitoneal metastatic deposits , although there were also primary appendiceal tumors and a small number of lung , liver , and bone metastases ( fig 1a )  . 
data presented as % frequency . abbreviations : ad , adenocarcinoma ; crc , colorectal cancer ; gcc , goblet cell carcinoid ; mad , mucinous adenocarcinoma ; msi - h , microsatellite instability - high ; pdac , pancreatic ductal adenocarcinoma ; pmp , pseudomyxoma peritonei . comparison of genomic aberrations in appendix , colorectal , and pancreas cancers given the clinical practice of treating metastatic appendiceal cancers with crc regimens , we compared genomic alteration profiles of the appendiceal subtypes with those of 10 , 000 crcs profiled by the same laboratory ( table 2 )  . 
the high frequency of kras mutations observed in multiple appendiceal subtypes prompted inquiry into possible parallels with ( pdac ) , pancreatic ductal adenocarcinoma which harbors kras mutations in up to 95% of cases.16 sequencing of 2 , 800 pancreatic tumors revealed kras mutations in 87% of pdacs . 
there tended to be a higher frequency of microsatellite unstable or tumor mutational burdenhigh srccs and ads compared with mads ( table 2 ; appendix fig a1e )  . histopathologic and molecular features predictive of survival to determine the influence of histologic and molecular features on clinical outcomes , a retrospective review of a single - institution case series was performed . 
similar to the full 703 - patient cohort , the majority of cases were either ads ( n = 17 ) or mads ( n = 33 ) , with fewer low - grade appendiceal mucinous neoplasms that manifested as pmps ( n = 13 ) and few srccs ( n = 9 )  . 
data for chemotherapy treatment were available for 60 patients , showing that the majority were treated with a fluoropyrimidine and either oxaliplatin or irinotecan ( appendix ; table 3 )  . overall survival ( os ) , determined from time of initial diagnosis , was similar for ad and mad ( logrank p = .29 ; appendix fig a2a ) , so these groups were combined in subsequent analyses . 
 ( % ) unless otherwise noted . abbreviations : egfr , epidermal growth factor receptor ; hipec , heated intraperitoneal chemotherapy ; lamn , low - grade appendiceal mucinous neoplasms ; pd1 , programmed cell death protein 1 ; pd - l1 , programmed death ligand 1 ; pmp , pseudomyxoma peritonei ; sd , standard deviation ; vegf , vascular endothelial growth factor . for srccs ( p = .11 ; fig 2a )  . 
 however , use of irinotecan in any line of therapy was associated with a survival advantage in kras wild - type tumors ( log - rank p = .041 ; fig 2f ) but not in kras mutant tumors ( log - rank p = .32 ; appendix fig a2b )  . 
low - grade tumors were enriched for gnas mutations ( 72% v 18% for high grade ; 2 p < .001 ; appendix fig a3a ) , consistent with our prior report , 14 whereas highgrade tumors were enriched for tp53 mutations ( 56% v 6.9% for low grade ; 2 p < .001 ; appendix fig a3b )  . to assess the relative contributions of mutation and grade to the observed os differences , a cox proportional hazard analysis was performed including age , sex , kras , gnas , tp53 , and grade as covariates . 
however , the effect of tp53 mutation on survival was independent of grade , with the rare low - grade , tp53 - mutant tumors having os similar to other tp53 - mutant tumors ( median , 24.6 months ; fig 3b )  . 
at risk : irinotecan 8 no irinotecan 15 time ( months ) the mutational profile of 703 appendix neoplasms provides insight into the molecular aberrations that differentiate histologic subtypes and identifies putative prognostic and predictive biomarkers that may help guide treatment in this rare malignancy . 
compared with ad , mad , and pmp , kras and gnas mutations were much less frequent in gccs , whereas mutations in fat3 and arid1a were more frequent ( figs 1b and 1c )  . 
 these differences were also seen in the pathway analysis , in which gccs had less - frequent alterations of the ras / raf pathway relative to epithelial appendiceal cancers ( fig 1d )  . 
at risk : gnas mut 28 tp53 mut 25 neither 18 high - gnas mutant moderate - gnas mutant p = .011 low - gnas mutant time ( months ) no . 
these data also show that all of the appendiceal subtypes are molecularly distinct from crc , with more frequent gnas mutation and significantly lower prevalence of apc and tp53 mutations , which are key pathogenic alterations in crc . 
 the mutation profiles of ad and srcc bore the most resemblance to crc , with ad and crc sharing similar frequencies of mutation in kras , smad4 , and arid1a ; of note , appendiceal ads have been referred to as colonic - type adenocarcinoma , given clinical behavior more similar to crc.20 , 27 in this series , srcc had the worst prognosis of the epithelial appendiceal tumors and also has a clinical course similar to crc.28 the frequent comutation of kras and gnas in mad , ad , and pmp parallels the molecular profile of intraductal papillary mucinous neoplasms.14 , 29 notably , both intraductal papillary mucinous neoplasms and , in particular , gnas mutant appendiceal cancers are characterized by mucin production and a generally indolent clinical course . 
the differences in mutation profiles between the epithelial appendiceal tumors can be at least partially explained by grade , with significant association of gnas mutation with low - grade tumors and tp53 mutation with highgrade tumors ( appendix figs a3a and a3b )  . 
 consistent with this is the higher incidence of tp53 mutation and lower incidence of gnas mutation in srccs , which are by definition all high grade . histologic grade was also a strong predictor of survival ( fig 2b ) , consistent with prior reports.17 , 30 we did not observe a significant difference in os between ad and mad ; however , the distribution of tumor grade was similar between these two subtypes in our study . 
 conversely , tp53 mutation was an independent predictor of poor survival , with low - grade , tp53 - mutant tumors having survival similar to that of high - grade tumors . 
in addition , because appendiceal tumors are so rare , they are difficult to diagnose pathologically and are frequently overinterpreted by community pathologists.31 although gnas mutation is not an independent predictor of survival , because gnas and tp53 mutations occur mutually exclusive of each other and are associated with lowand high - grade tumors , respectively , the two genes can be substituted for grade to predict survival . 
the survival stratification achieved with the gnas - tp53 biomarker is similar to grade , an important observation , given that it is now much easier to obtain a mutation profile than an expert pathology review in the community oncology setting . the absence of a gnas mutation in the majority of high - grade tumors and the mutual exclusivity of tp53 and gnas mutations both strongly suggest that most high - grade appendiceal tumors occur de novo , rather than progressing from low - grade tumors , confirming , on a larger scale , our previous observations.14 however , there were a minority of tumors with both tp53 and gnas mutation ( n = 41 ; 6.7% ) , suggesting that transformation from low grade to high grade can occur . 
serial biopsy or serial measurement of circulating tumor dna would be needed to confirm that these tp53 mutations did in fact occur after the formation of a low - grade , gnas mutant tumor . 
however , given the low propensity for appendiceal tumors to spread beyond the abdominal cavity , there may be limited tumor dna in circulation , potentially making bloodbased tumor detection difficult . 
indeed , three of the four university of california , san diego , patients who underwent circulating tumor dna sequencing had no reportable alterations . regarding predictive biomarkers , kras wildtype status was associated with better survival in the subset of patients treated with irinotecan . 
a retrospective study in metastatic crc reported better response to irinotecan in patients with wild - type versus mutant plasma kras.32 however , a larger prospective study found that mutant kras was associated with poor survival but not with response to irinotecan in crc.33 regarding targeted therapies , there are unfortunately few clinically actionable mutations in appendiceal cancers , although the ras / raf signaling pathway is frequently altered in epithelial appendiceal cancers . 
data on therapeutic targeting of the ras / raf cascade in appendiceal tumors are limited , although a recent case report described clinical benefit in a patient with appendiceal mad harboring a gnas r201h mutation who was treated with trametinib.34 because only eight patients in this cohort received an anti - egfr antibody , we were unable to assess interactions between kras mutation status and response to these agents . a major limitation of this study is its retrospective design . 
with regard to the 703 - patient cohort , clinical information such as precise tnm stage was not available , but the fact that > 80% of specimens submitted came from metastases indicates that the majority of patients had stage iv disease . 
although specimens were independently reviewed by pathologists to confirm the diagnosis before undergoing sequencing , subtype definitions are potentially subject to variability and overlap , because there was no consensus classification system for appendiceal neoplasms and pmp until recently.2 for example , pmp is an inherently imprecise term used to describe the clinical syndrome of mucinous peritoneal dissemination from an appendiceal neoplas pmp encompasses a spectrum of both highand low - grade lesions but does not reference the histopathologic characteristics of the appendiceal primary from which it arises . 
 newer classification schemes separate pmps with low - grade and high - grade features ( also known as disseminated peritoneal adenomucinosis and peritoneal mucinous carcinomatosis , respectively35 ) and pmp with signet ring cells.2 because this study did not distinguish between these subtypes , we are unable to report on genomic differences associated with grade in the larger 70 - patient cohort . 
in addition , analysis of interactions between genotype and specific drugs are confounded by the fact that most patients received multiple lines of therapy . this study of unprecedented size in this rare disease highlights important molecular differences between different subtypes of appendix cancer and identifies gnas and tp53 mutation status as a prognostic biomarker . 
this comprehensive portrait of the molecular landscape of appendix cancer will help with the design of future clinical studies to develop and test therapeutic strategies specific to this disease . in conclusion , appendiceal neoplasms have molecular profiles that are distinct from crc and are characterized by frequent gnas and kras mutations , especially in low - grade tumors . 
ross employment : foundation medicine leadership : foundation medicine financial support : john paul shen , paul fanta , trey ideker administrative support : john paul shen , paul fanta stock and other ownership interests : foundation medicine provision of study material or patients : john paul shen , jeffrey s . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center miriam t . 
ali employment : foundation medicine leadership : incyte stock and other ownership interests : exelixis , blueprint medicines , agios pharmaceuticalas , genocea biosciences patents , royalties , other intellectual property : patents via foundation medicine and seres health joel baumgartner research funding : merck andrew lowy consulting or advisory role : halozyme , merck research funding : mitsubishi tanabe pharma , syros pharmaceuticals expert testimony : merck ascopubs.org / journal / po jco precision oncology 9 justin k . 
 paul fanta no relationship to disclose trey ideker leadership : data4cure consulting or advisory role : ideaya biosciences , genetic modifiers newco , merck , la jolla institute for allergy and immunology research funding : pfizer travel , accommodations , expenses : sage bionetworks sherri z . 
chen , david xu , joel baumgartner , andrew lowy , paul fanta , trey ideker , and olivier harismendy , university of california , san diego , la jolla , ca ; jeffrey s . 
carr nj , cecil td , mohamed f , et al : a consensus for classification and pathologic reporting of pseudomyxoma peritonei and associated appendiceal neoplasia : the results of the peritoneal surface oncology group international ( psogi ) modified delphi process . 
sugarbaker ph , bijelic l , chang d , et al : neoadjuvant folfox chemotherapy in 34 consecutive patients with mucinous peritoneal carcinomatosis of appendiceal origj surg oncol 102 : 576581 , 2010 5 . 
farquharson al , pranesh n , witham g , et al : a phase ii study evaluating the use of concurrent mitomycin c and capecitabine in patients with advanced unresectable pseudomyxoma peritonei . 
garin l , corbinais s , boucher e , et al : adenocarcinoid of the appendix vermiformis : complete and persistent remission after chemotherapy ( folfox ) of a metastatic case . 
tejani ma , ter veer a , milne d , et al : systemic therapy for advanced appendiceal adenocarcinoma : an analysis from the nccn oncology outcomes database for colorectal cancer . 
johncilla m , stachler m , misdraji j , et al : mutational landscape of goblet cell carcinoids and adenocarcinoma ex goblet cell carcinoids of the appendix is distinct from typical carcinoids and colorectal adenocarcinomas . 
borazanci e , millis sz , kimbrough j , et al : potential actionable targets in appendiceal cancer detected by immunohistochemistry , fluorescent in situ hybridization , and mutational analysis . 
alakus h , babicky ml , ghosh p , et al : genome - wide mutational landscape of mucinous carcinomatosis peritonei of appendiceal orig genome med 6 : 43 , 2014 [ erratum : genome med 6 : 53 , 2014 ] 15 . 
reid md , basturk o , shaib wl , et al : adenocarcinoma ex - goblet cell carcinoid ( appendicealtype crypt cell adenocarcinoma ) is a morphologically distinct entity with highly aggressive behavior and frequent association with peritoneal / intra - abdominal dissemination : an analysis of 77 cases . 
singhi ad , davison jm , choudry ha , et al : gnas is frequently mutated in both low - grade and high - grade disseminated appendiceal mucinous neoplasms but does not affect survival . 
mccusker me , cot tr , clegg lx , et al : primary malignant neoplasms of the appendix : a population - based study from the surveillance , epidemiology and end - results program , 19731998 . 
asare ea , compton cc , hanna nn , et al : the impact of stage , grade , and mucinous histology on the efficacy of systemic chemotherapy in adenocarcinomas of the appendix : analysis of the national cancer data base . 
 appendix tumor tissue from 703 patients with appendiceal cancer was submitted to a clinical laboratory improvement amendments certified laboratory ( foundation medicine , cambridge , ma ) for dna sequencing and variant calling . 
a minimum of 50 ng of dna was extracted and a hybrid - capture method used to capture 3 , 769 exons from 315 cancer - related genes and 47 introns of 28 genes commonly rearranged in cancer ; this material was then sequenced to high ( average , 756x ) uniform coverage allowing for evaluation of genomic alterations , including base substitutions , indels , amplifications , copy number alterations , and fusions / rearrangements . 
clinical characteristics and outcomes , including tumor histology , grade , stage , overall survival ( os ) , and chemotherapy given were determined from review of the electronic medical record . 
sequencing failed quality control in two cases , and two patients with only blood - based cell - free dna sequencing were excluded , leaving 76 patients available for analysis . 
because there were only four goblet cell carcinoids , these were removed from survival analysis . for mutual exclusivity and comutation analysis , goblet cell carcinoid tumors and microsatellite instability - high tumors were removed , and a fishers exact test was performed for all gene combinations , followed by bonferroni multiple hypothesis correction . 
 inherited mutations in men undergoing multigene panel testing for prostate cancer : emerging implications for personalized prostate cancer genetic evaluation see accompanying editorial doi : purpose multigene panels are commercially available for the evaluation of prostate cancer ( pca ) predisposition , which necessitates tailored genetic counseling ( gc ) for men . 
here we describe emerging results of genetic evaluation of men , prospective multigene testing study in pca to inform personalized genetic counseling , with emerging implications for referrals , cancer screening , and precision therapy . patients and methods eligibility criteria for men affected by or at high risk for pca encompass age , race , family history ( fh ) , and pca stage / grade . 
 pca20 - 24 along with risk for multiple additional cancers , including colorectal , endometrial , ovarian , and pancreatic.25 , 26 in addition , a recurrent mutation in hoxb13 has been identified to predispose to hereditary pca ( hpc ) , and confers an approximate twoto eightfold increased risk for pca and twoto 10 - fold increased risk for earlyonset disease , 27 - 34 consistent with the longdescribed phenotype of hpc.35 thus , inherited pca may be suspected on the basis of an fh of pca , fh of multiple other cancers , or young age at diagnosis of pca . 
this multigene testing capability raises the importance of tailoring genetic counseling ( gc ) for men and their families to make informed decisions about proceeding with genetic testing.39 , 40 because genetic testing guidelines for pca are limited , lack of clinical genetic data exists on potential rates of mutations , family cancer risks relevant to both sexes , variant of uncertain significance ( vus ) rates , concordance of mutations with personal / fh , and cancer screening impact , all of which are important to gc and informed genetic testing.39 , 40 robust data from clinical genetic testing , therefore , are needed to address this gap in gc practice and responsibly implement multigene panel testing for the evaluation of inherited pca . the genetic evaluation of men ( gem ) study was developed with three main goals : implement prospective multigene panel testing for inherited pca in the context of gc ; characterize the genetic variant spectrum in clinically available cancer risk genes to inform men and their families about cancer risks , screening , and precision treatment ; and develop a registry of men with and without pca that encompasses detailed personal / fh of cancer , diet , exercise , and exposures that are not usually available from commercial genetic testing laboratory databases . 
the study has plans to recruit additional sites pending institutional review board approvals . referrals and recruitment referrals come from treatment clinics for men with pca and men without pca enrolled in screening efforts . 
at the sidney kimmel cancer center , referrals also come from the genitourinary multidisciplinary clinic where men with pca receive multidisciplinary evaluation , treatment planning , and an opportunity to engage in gc.41 eligibility criteria eligibility criteria for gem were intended to be broad to encompass inclusion of a spectrum of risk for pca ( young age of cancer diagnoses , 19 , 26 , 42 , 43 african american race , 44 - 46 fh of pca , 47 fh of hcs - associated cancers , 19 , 25 , 26 and fh that meets strict criteria for hcss19 , 35 , 48 ) and are modeled on evaluation of other cancers.19 , 26 personal / fh of cancers associated with specific hcss include hboc ( breast , ovarian , pancreatic , and prostate cancers and melanoma ) , ls ( colorectal , ovarian , endometrial , upper gi , pancreatic , and upper urinary tract cancers and sebaceous carcinoma ) , and hpc ( pca )  . 
furthermore , with emerging insights into germline mutations in metastatic pca , 36 , 37 eligibility criteria also included metastatic pca as well as higher gleason score and t3 disease to explore mutation rates in advanced / high - risk disease . 
prap eligibility criteria include age < 69 years and any of the following : fdr with pca , two sdrs with pca on the same side of the family , and african american race . 
individuals who consented to prap participation were offered genetic evaluation of men study participation . genetic test multigene panel testing initially included 25 cancer risk genes : apc , brca1 , brca2 , mlh1 , msh2 , pms2 , msh6 , cdh1 , pten , stk11 , tp53 , atm , bard1 , bmpr1a , brip1 , cdk4 , cdkn2a , chek2 , epcam , mutyh , nbn , palb2 , rad51c , rad51d , and smad4 . 
subsequently , three more genes related to colon polyposis were added to the panel : pold1 , pole , and grem1 ( appendix table a1 ; details for variant detection provided in the appendix )  . 
discussion includes an overview of medical history and a review of pedigrees , test results , and personalized recommendations about cancer risk , screening , and personalized management for each participant and his blood relatives . post - test genetic disclosure post - test discussion focuses on cancer screening , risk reduction strategies , and further gc / testing in the family on the basis of test results ( positive for pathogenic variant , negative for any pathogenic variants , or vus [ full details provided in the appendix ] ; appendix table a1 )  . 
participants with vus also receive information for the prospective registry of multiplex testing ( promptstudy.info ) for contributing to the clarification of vus.49 statistical methods mutation rates were summarized by eligibility criteria . 
in such cases , the participant is included in the mutation rate calculation for multiple eligibility criteria . fh was summarized as the number of men who reported a history of cancer in first - degree relatives ( fdrs ) , second - degree relatives , and thirddegree relatives as well as the number of affected family members . 
furthermore , fh was summarized for five specific cancer sites of primary interestprostate , breast , ovarian , colon , and pancreaticinvolved in hcs and in which pca has been implicated . 
hcss were classified based on the participant or fh meeting criteria for hboc , ls , or hpc.19 , 35 , 48 in addition to fh , demographic information ( race , hispanic ethnicity , ashkenazi jewish ancestry ) and pca information for affected men ( stage , gleason score , age at diagnosis ) was collected . unadjusted mutation rates were compared across fh in fdrs , fh in any relatives , presence of hcs , and pca status for all men using fishers exact test . 
an examination of broader fh showed that participants with an fh of any relative with breast cancer had a higher rate of mutations ( 10.3% ) than those with no fh of breast cancer ( p = .004 ; table 3 )  . 
concordance was defined as having a personal history or any fdr , second - degree relative , or third - degree relative with a cancer in the spectrum linked with the gene mutation ( descriptive examples provided in the appendix )  . 
of the nine mutation carriers , 44.4% received their pca diagnosis at age younger than 60 years , 66.7% had a gleason score > 7 , and 44.4% had a gleason score > 8 . 
all chek2 ( ile157thr ) carriers had a personal / fh of pca , and three of four had an fh of breast and / or colon cancers consistent with the current chek2 - associated cancer spectrum . precision gc model for pca in current gc for pca , a void of information exists with regard to expected mutation and vus rates from multigene testing , potential findings and concordance of mutations , and cancer risks for patients and their families ; such information is needed for informed decision making about genetic testing.39 , 40 the current emerging results are being used to tailor gc for men concerned about inherited pca ( table 5 )  . discussion implications for precision gc the findings of this study begin to fill a practice gap for gc to inform men about potential multigene test results before proceeding with genetic testing , which is important to report at this time because of the current commercial availability of pca gene panels ( table 5 )  . 
the gem study implements multigene panel testing for evaluation of inherited pca and was intended to include a broad group of men to comprehensively uncover and characterize mutations and variants to inform genetic evaluation strategies in this underdeveloped area pertinent to pca . 
the cohort is heterogeneous and includes men with and without pca who also have personal or familial features of risk for pca , including young age at cancer diagnosis , african american race , metastatic pca , and fh of cancer . 
the chance of a genetic finding not consistent with a personal / fh also needs to be discussed due to cancer screening and management implications for patients and their families . the results reveal a proportionately higher rate of germline mutations in dna repair genes among men with a strong fh of cancer , particularly for breast cancer , with mutations identified in men without evidence of metastatic disease . 
precision genetic counseling for prostate cancer finding highlights the importance of germline genetic testing to be considered not only for men with metastatic pca but also for those with early - stage disease , particularly with a strong fh of cancer . 
oncologic , urologic , and primary care providers must be aware of the need for full intake of fh ( maternal and paternal ) , including all cancers for appropriate referrals of men for genetic evaluation . the overall mutation rate of 5.5% is comparable to non - brca mutation rates in breast and ovarian cancers where guidelines exist for genetic if we include chek2 testing.19 , 50 however , ( ile157thr ) as pathogenic , the overall prevalence of mutations in the current cohort approaches 7.5%. 
we chose to include mutation counts as stringently as possible that are based only on clinical report interpretation of a variant as pathogenic , thus excluding chek2 ( ile157thr ) at this time from mutation prevalence estimation . in castration - resistant pca and in the setting of deleterious germline brca2 mutations.51 , 52 in addition , a phase ii clinical trial suggested that a common subset of metastatic pcas , characterized by defects in dna repair , can be molecularly stratified for treatment with parp inhibitors , with a notable response seen in patients whose tumors had atm alterations and brca2 loss.38 therefore , the current findings become particularly important for men with advanced or metastatic disease who may be eligible for targeted therapy with parp inhibition . 
furthermore , as dna repair germline mutations are identified in early - stage disease , there may be an added rationale to develop trials of targeted / tailored management of these individuals , which widens the role of genetic testing for treatment and management decision making along the pca stage spectrum . implications for unaffected men at high - risk for pca implications for men with pca the identification of dna repair germline mutations in men with pca , particularly those with metastatic disease , is of high clinical importance . data suggest a potential role for parp inhibitors current national comprehensive cancer network guidelines only address pca screening in the context of brca1 / 2 mutations , 19 with a need to expand genetically informed pca screening . 
risks for colon cancer , pancreatic cancer , melanoma , and male breast cancer in men with or at risk for pca have been identified , which necessitates guidelines - based screening / management or referral for discussion of screening options.19 , 25 , 26 furthermore , male and female blood relatives of all participants now have insight into which specific mutations may predispose to cancer risk in their family and can pursue site - specific mutation testing through guidelines - based cancer screening approaches.19 , 25 , 26 consideration of study results there are some limitations when considering study results . 
although genetic mutations identified in this study inform risks for several cancers , the majority of mutations ( with the exception of brca1 and brca2 ) currently provide limited information about pca penetrance and highlight the need for additional functional studies of their role in pca predisposition . in conclusion , this study supports a comprehensive approach to genetic evaluation for pca and highlights the need to consider multiple types of cancers in families of men concerned about inherited pca risk . 
hegarty no relationship to disclose susan montgomery no relationship to disclose andrea forman consulting or advisory role : invitae speakers bureau : invitae ruth bingler no relationship to disclose william k . 
chen employment : tenet healthcare ( i ) stock and other ownership interests : pfizer ( i ) consulting or advisory role : argos therapeutics travel , accommodations , expenses : argos therapeutics costas d . 
gomella patents , royalties , other intellectual property : nuview ( inst ) , nuview travel , accommodations , expenses : abbvie , bayer ag , astellas pharma , janssen pharmaceuticals acknowledgment myriad genetics provided genetic testing free of cost to study participants . 
giusti rm , rutter jl , duray ph , et al : a twofold increase in brca mutation related prostate cancer among ashkenazi israelis is not associated with distinctive histopathology . 
leongamornlert d , mahmud n , tymrakiewicz m , et al : germline brca1 mutations increase prostate cancer risk . br j cancer 106 : 1697 - 1701 , 2012 10 . 
eerola h , pukkala e , pyrh onen s , et al : risk of cancer in brca1 and brca2 mutation - positive and - negative breast cancer families ( finland )  . 
castro e , goh c , olmos d , et al : germline brca mutations are associated with higher risk of nodal involvement , distant metastasis , and poor survival outcomes in prostate cancer . 
edwards sm , kote - jarai z , meitz j , et al : two percent of men with early - onset prostate cancer harbor germline mutations in the brca2 gene . 
engel c , loeffler m , steinke v , et al : risks of less common cancers in proven mutation carriers with lynch syndrome . j clin oncol 30 : 4409 - 4415 , 2012 553 - 557 , 2014 oncol 31 : 1713 - 1718 , 2013 21 . 
ryan s , jenkins ma , win ak : risk of prostate cancer in lynch syndrome : a systematic review and meta - analysis . cancer epidemiol biomarkers prev 23 : 437 - 449 , 2014 24 . 
xu j , lange em , lu l , et al : hoxb13 is a susceptibility gene for prostate cancer : results from the international consortium for prostate cancer genetics ( icpcg )  . 
shang z , zhu s , zhang h , et al : germline homeobox b13 ( hoxb13 ) g84e mutation and prostate cancer risk in european descendants : a meta - analysis of 24 , 213 cases and 73 , 631 controls . 
laitinen vh , wahlfors t , saaristo l , et al : hoxb13 g84e mutation in finland : population - based analysis of prostate , breast , and colorectal cancer risk . 
kote - jarai z , mikropoulos c , leongamornlert da , et al : prevalence of the hoxb13 g84e germline mutation in british men and correlation with prostate cancer risk , tumour characteristics and clinical outcomes . 
powell ij , bock ch , ruterbusch jj , et al : evidence supports a faster growth rate and / or earlier transformation to clinically significant prostate cancer in black than in white american men , and influences racial progression and mortality disparity . 
balma~na j , digiovanni l , gaddam p , et al : conflicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
sandhu sk , omlin a , hylands l , et al : poly ( adp - ribose ) polymerase ( parp ) inhibitors for the treatment of advanced germline brca2 mutant prostate cancer . 
sandhu sk , schelman wr , wilding g , et al : the poly ( adp - ribose ) polymerase inhibitor niraparib ( mk4827 ) in brca mutation carriers and patients with sporadic cancer : a phase 1 dose - escalation trial . 
bancroft ek , page ec , castro e , et al : corrigendum to targeted prostate cancer screening in brca1 and brca2 mutation carriers : results from the initial screening round of the impact study [ eur urol 2014 ; 66 : 489 - 99 ]  . 
eur urol 67 : e126 , 2015 before the genetics appointment , participants receive questionnaires on medical history , family history ( fh ) , and risk factors for clinical and study purposes . 
genetic counseling ( gc ) involves a detailed intake of medical history , prostate cancer ( pca ) features ( eg , age at diagnosis , gleason score , treatment ) , fh of cancer , and cancer - related risk factors . 
the discussion involves basic principles of disease inheritance , genetic test options ( single - gene testing versus multigene testing ) , genespecific cancer risks , types of test results ( pathogenic variant , variant of uncertain significance [ vus ] , or no pathogenic variant ) , potential management implications , genetic discrimination laws , and reproductive implications . 
pretest counseling is done in person by a cancer genetics provider ( sidney kimmel cancer center ) and by a video session designed for this study by a genetic counselor ( a.f. ) at fox chase cancer center with support by study staff . 
the myrisk test initially included 25 cancer - risk genes : apc , brca1 , brca2 , mlh1 , msh2 , pms2 , msh6 , cdh1 , pten , stk11 , tp53 , atm , bard1 , bmpr1a , brip1 , cdk4 , cdkn2a , chek2 , epcam , mutyh , nbn , palb2 , rad51c , rad51d , and smad4 . 
per laboratory protocol , all genes are sequenced as well as assessed for deletion / duplication except for epcam ( large rearrangement only ) , pole and pold1 ( sequencing of select regions ) , and grem1 ( large rearrangement analysis )  . 
additional discussion includes psychosocial supports and connection of family members with gc services as needed . individual characteristics of mutation carriers detailed characteristics for each participant with regard to mutations identified , pca status and features , fh of cancer , and concordance of mutation with personal / fh were assessed to inform gc ( appendix table a3 )  . 
concordance was defined as a personal history or any first - , second - , or third - degree relative with a cancer in the spectrum linked with the aforementioned gene mutations . 
in contrast , participant 5 had a brip1 mutation but no fh of ovarian cancer , which is the only cancer in the brip1 cancer - associated spectrum at this time . 
current myrisk panel from myriad genetics . abbreviations : br , breast ; co , colon ; en , endometrial ; fap , familial adenomatous polyposis ; ga , gastric ; hboc , hereditary breast and ovarian cancer ; hdgs , hereditary diffuse gastric cancer syndrome ; hht , hereditary hemorrhagic telangiectasia ; jps , juvenile polyposis syndrome ; ls , lynch syndrome ; lfs , li - fraumeni syndrome ; map , myh - associated polyposis ; mcs , melanoma cancer syndrome ; me , melanoma ; m - pcs , melanoma - pancreatic cancer syndrome ; oc , other cancers ; ov , ovarian ; pa , pancreatic ; phts , pten hamartoma tumor syndrome ; pjs , peutz - jeghers syndrome ; pr , prostate . 
 significant clinical response to a mek inhibitor therapy in a patient with metastatic melanoma harboring an raf1 fusion introduction systemic therapy for metastatic melanoma has changed dramatically since the development of targeted drugs for braf - mutant melanoma and immune checkpoint inhibitors . 
the overall survival duration of those with advanced melanoma has improved significantly with these novel drugs , with the median survival duration now reaching nearly 2 years.1 - 3 the checkpoint inhibitors ( anti cytotoxic t - cell lymphocyte - 4 antibodies and anti - programmed cell death - 1 [ pd - 1 ] antibodies ) produce antitumor response through their ability to activate cytotoxic t - lymphocytes . 
although many of these clinical responses are durable , the median progression - free survival durations are approximately 2 to 3 months and 5 to 6 months with anti - ctla4 antibody and ipilimumab , respectively.4 - 7 a combination of nivolumab and ipilimumab improves the overall response rate and progression - free survival compared with anti - ctla4 antibody alone.7 for patients with metastatic v600 braf - mutant melanoma , combinations of a braf inhibitor and a mek inhibitor have been established as a standard therapy because of a high response rate and superior survival over single - agent braf inhibitors.1 - 3 however , approximately 50% of melanomas do not harbor a v600 braf mutation and therefore do not benefit from braf inhibitor therapy.8 for these patients with wildtype braf , the identification of relevant and actionable genetic alterations and the development of effective matched therapies are urgently needed . 
recently , next - generation sequencing ( ngs ) analyses have revealed a multitude of less frequent and less well - characterized genetic alterations in melanoma , and these findings could lead to the development of effective treatments . 
in october 2014 , he had recurrent melanoma in the right cervical lymph node , and by december 2014 , his disease had progressed in the cervical and intrathoracic lymph nodes and the liver . 
in january 2015 , the patient started treatment with the combination of nivolumab and ipilimumab , but the treatment was discontinued after two doses because of the development of diabetic ketoacidosis . 
from august 2015 to march 2016 , he was treated with single - agent nivolumab and subsequently nivolumab in combination with intralesional talimogene laherparepvec injection to the right cervical nodes , but by march 2016 , the disease had progressed in the right neck nodes and liver . 
 in april 2016 , he underwent a debulking radical right neck lymph node dissection for a palliative purpose . in october 2016 , the patient developed a painful right neck mass , and his performance status worsened ( eastern cooperative oncology group performance status of 2 )  . 
he was found to have rapid disease progression in the right supraclavicular , mediastinal , gastrohepatic , and portocaval lymph nodes ; the liver ; the spleen ; and the t - 12 spine . 
 melanoma specimen from the right neck node was analyzed for genetic alterations using a hybrid - capturebased ngs assay ( foundationone ) .9 the results were wild type for braf , nras , and kit ; however , a number of genetic alterations , including a ano10 - raf1 fusion , flt1 r281q , notch3 splice site 4404 - 1g > a , arid2 q760fs * 7 , pbrm1 loss , spta1 q1720 * , and tert promoter - 146c > t , were detected . 
because of the development of significant skin toxicity , the dose was reduced to 1.5 mg / d after 4 weeks and further down to 1 mg / d in january 2017 . 
the patients pain in the right neck and shoulder improved dramatically with the treatment , his performance status improved , and a computed tomography scan performed at 10 weeks showed significant regression of the metastatic lesions in the right supraclavicular , mediastinal , gastrohepatic , and portocaval lymph nodes ; the liver ; and the spleen ( fig 1 )  . 
treatment with another mek inhibitor was discussed with the patient , but because of rapid clinical deterioration and the concern for significant skin toxicity , he decided on palliative care , and he died in june 2017 . discussion in this article , we describe , to our knowledge , the first case of clinical benefit from an mek inhibitor in a patient with metastatic melanoma harboring an ano10 - raf1 fusion . 
the patients tumor did not harbor a v600 braf mutation , and therefore , selective braf inhibitors or mek inhibitors were not clinically indicated at the time of the treatment . 
without the comprehensive genomic testing capable of detecting gene fusions and rearrangements in addition to mutations and copy number changes , we could have missed the great response witnessed with the mek inhibitor , underscoring the importance of ngs analysis . 
it is not clear whether the tumor progression was caused by true acquired resistance to mek inhibition or by suboptimal dosing of the treatment because of the intolerable cutaneous toxicity . although a single base substitution at codon 600 is the most common genetic alteration in raf genes in melanoma , other raf gene alterations have been observed , with various functional consequences.10 many of the non - v600 braf mutations do not activate the mitogen - activated protein kinase ( mapk ) signaling pathway in as robust a manner as do v600 mutations , and they are largely insensitive to the braf v600 specific inhibitors dabrafenib and vemurafenib.11 genetic mutations in the other raf genes , such as araf and craf ( raf1 ) , are relatively rare.12 abnormal rearrangements of raf1 , including raf1 fusions , occur in approximately 1% of cutaneous melanomas , 13 and their prognostic significance is not known . 
some of these genetic alterations , such as esrp1 - raf1 fusion , were found to activate the mapk pathway and are capable of transforming cells.10 palanisamy et al10 showed that prostate epithelial cells expressing an esrp1 - raf1 fusion were sensitive to a combination of a raf inhibitor ( sorafenib ) and a mek inhibitor ( u0126 ) in vitro . 
although the function of ano10 - raf1 fusion , as found in our case , has not been described , it is likely that this alteration activates the mapk pathway because mek protein inhibition caused significant tumor regression in our case . 
the breakpoint in this case is in raf1 exon 7 and in the fact that the resulting in - frame fusion retains the raf1 kinase domain while removing the n - terminal auto - inhibitory domain ( fig 2 )  . 
this case , together with ours , strongly suggests the clinical relevance of raf gene fusions in melanoma and offers mek inhibitors as a potential therapeutic option for patients with raf fusionpositive tumors . 
for patients with melanoma harboring a braf fusion , there is a phase ii study of trametinib ( the national cancer institute molecular analysis for therapy choice [ nci - match ] trial [ clinicaltrials . gov identifier : nct02465060 ] ) ; however , at this time there is no specific trial for patients with raf1 fusionpositive melanoma . 
in addition to the clinical investigation of mek inhibitors , clinical studies of pan - raf inhibitors , such as sorafenib and regorafenib , should be encouraged on the basis of their preclinical antitumor activity in raf1 fusionassociated cells . furthermore , a mek inhibitorbased combination approach may lead to more durable disease control . 
several groups have demonstrated potential mechanisms of resistance to mek inhibition , including induction of immunoglobulin transcription factor 2 , 15 induction of signal transducer and activator of transcription 3 , 16 and amplification of cyclin - dependent kinase 4 and 6 , 17 among others . 
 furthermore , there is increasing evidence that mek inhibition leads to antigen - specific cd8 + t cells proliferation within the tumor and pro motes the survival of tumor - infiltrating cd8 + t cells.18 these phenomena were corroborated by experiments in which the addition of an mek inhibitor to an anti pd - 1 ( or pro grammed death - ligand 1 [ pd - l1 ] ) antibody resulted in durable and synergistic tumor regression.18 several clinical trials are evaluating the clinical efficacy of an mek inhibitor in combination with the checkpoint inhibitors in patients with melanoma ( clinicaltrials.gov identifiers : nct03149029 , nct03178851 , and nct02910700 )  . in conclusion , the ngs analysis of the melanoma lesion in our patients tumor was essential in identifying the clinically relevant genetic alteration , ano10 - raf1 fusion , and in selecting a mek inhibitor treatment that resulted in brief , but significant , tumor regression and symptom improvement . 
kim honoraria : genentech , glaxosmithkline , novartis , foundation medicine consulting or advisory role : genentech , glaxosmithkline , novartis , foundation medicine speakers ' bureau : bristol - myers squibb , merck , novartis research funding : glaxosmithkline ( inst ) , novartis ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , amgen , immune design ( inst ) travel , accommodations , expenses : genentech , bristol - myers squibb , merck , novartis thomas semrad consulting or advisory role : amgen , genentech , onyx pharmaceuticals , celgene , eisai , genzyme ( i ) research funding : eisai ( inst ) , millennium pharmaceuticals ( inst ) , novartis ( inst ) alexa b . 
ali employment : foundation medicine honoraria : emd merck serono research funding : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome stuff in non - neoplastic disease ( i ) mark singer no relationship to disclose jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine honoraria : pfizer mohammed kashani - sabet stock and other ownership interests : melanoma diagnostics , dnarx honoraria : cepheid consulting or advisory role : castle biosciences research funding : merck patents , royalties , other intellectual property : myriad genetics affiliations kevin b . 
kim , mark singer , and mohammed kashani - sabet , california pacific medical center research institute , san francisco ; thomas semrad , gene upshaw memorial tahoe forest cancer center , truckee , ca ; alexa b . 
long gv , stroyakovskiy d , gogas h , et al : dabrafenib and trametinib versus dabrafenib and placebo for val600 braf - mutant melanoma : a multicentre , double - blind , phase 3 randomised controlled trial . 
weber js , dangelo sp , minor d , et al : nivolumab versus chemotherapy in patients with advanced melanoma who progressed after anti - ctla - 4 treatment ( checkmate 037 ) : a randomised , controlled , open - label , phase 3 trial . 
bid hk , kibler a , phelps da , et al : development , characterization , and reversal of acquired resistance to the mek1 inhibitor selumetinib ( azd6244 ) in an in vivo model of childhood astrocytoma . 
ebert pjr , cheung j , yang y , et al : map kinase inhibition promotes t cell and anti - tumor activity in combination with pd - l1 checkpoint blockade . 
at result reporting , the variant had not been described previously and was interpreted as nonactionable , despite the well - described role of fgfr2 fusion proteins in cholangiocarcinoma1 , 2 and preliminary evidence of efcacy of fgfr2 inhibitors in this context.3 , 4 by the time he was evaluated in the clinic , even greater evidence that an fgfr2 inhibitor was likely to be effective had emerged.2 , 3 , 5 - 9 enrollment into the national cancer institute ( nci ) match ( molecular analysis for therapy choice ) fgfr arm ( subprotocol k - 2 ) and matching with erdatinib was sought . 
because the fgfr2 - bend3 fusion had not previously been described , approval of the variant as a novel actionable mutation of interest ( amoi ) was required by the nci before enrollment . 
numerous logistical issues ensued , summarized in figure 1 . discussion of the case an overwhelming minority of tumors have amois , 10 - 13 and few amois would not have been identied as part of standard molecular subtyping workup ( eg , egfr , alk , ros , met in nonsmall - cell lung cancer ) .14 in the rare circumstances where amois are identied by nonstandard testing , the expected marginal benet of targeted therapy over conventional chemotherapy to most patients is not of great magnitude.15 others have posited that even exceptional responses to off - label targeted therapy may be as a result of a tumors inherent susceptibility to all therapies.16 - 20 finally , the value of whole - genome or exome sequencing to into our knowledge been dividual patients has not stringently assessed by , for example , value of information analysis.21 - 23 on the basis of the available data , then , it is difcult to justify broad sequencing of tumors as a cost - effective approach at any line in therapy , even in an age of rapidly declining costs of sequencing.24 , 25 despite the absence of evidence , the heuristic of population - level prospective sequencing and matching generates excitement , is used with increasing frequency , and carries cachet in the eld , driven by the hope that maximal precision in diagnostics will lead to accuracy in therapeutics . precision in the modern era reects an underlying desire to proceed with maximal exactitude . 
in the case of diagnosis , this means demonstrating the molecular lesion ( s ) driving a given cancers growth , and in the case of therapeutics , to specically inhibit this offending mechanism with a treatment . 
in doing so , the goal is to meaningfully affect the natural history of diseasethe sine qua non of accurate treatment . although it is tempting to linearly connect precision with accuracy , in practice the two concepts must be kept distinct.14 precise treatments are not always accurate . 
highly precise body surface areabased dosing of chemotherapeutic agents lacks evidence demonstrating benet or reduction in harms when compared with less - precise dosing approaches.26 , 27 accurate therapies do not always require precision , even in the era of targeted agents : in certain contexts , the off - target effects ( imprecision ) of pantyrosine kinase inhibitors are a feature rather than a bug , such that these accurate treatments do not require or even benet from precise diagnosis . furthermore , therapies that are both precise and accurate do not necessarily require precise diagnosis . 
given the overwhelming pretest probability of philadelphia chromosome positivity , chronic myelogenous leukemia could be treated with inhibitors of the bcr - abl fusion protein tyrosine kinase without molecular testing . 
a successful therapeutic trial is diagnostic , and the efcacy of philadelphia chromosomenegative chronic myelogenous leukemia treatments is limited at best.28 - 30 finally , the most likely result of an individual sequencing panel is discovering an absence of amois or identifying molecular drivers that cannot be targeted , 31 , 32 situations in which the genetic test has failed to provide diagnostic or therapeutic value . 
unclear at this time whether the rejection is on scientific or logistical grounds . back - channel communication with high - ranking nih official : the entire problem in this case is that [ referring laboratory ] cannot provide the actual breakpointsthis is not an isolated incident and all referring labs know that we need this data to be able to enter the patient . " contact chief medical officer of referral laboratory requesting exact breakpoint sequences . referral laboratory : needs legal clearance ( new roi ) to provide breakpoint data . referral laboratory sends fgfr2 and bend3 breakpoints . 
we must use our usual channels as directed by the ncimatch protocol . referral laboratory : in summary , it is [ referral laboratory ] 's understanding that were waiting on the determination decision from the nci . referral laboratory : we have just received clarification on what genomic data the nci needs to proceed with the review of this case . 
timeline of novel actionable mutation of interest ( amoi ) approval processes of national cancer institute ( nci ) match ( molecular analysis for therapy choice ) and asco targeted agent and proling utilization registry ( tapur ) in the documented case . 
in both cases , patients are exposed to a matched therapy if their tumor contains any one putative driver mutation from a preapproved list of amois . there is no comparison group in either trial . 
the outcome measures of interest are different between the two trials . match aims to maximize each arms response rate.10 , 34 as such , the question being addressed in match is , using the example of our patient with fgfr2 fusion , do patients whose advanced cancers harbor particular fgfr2 mutations and fusions respond to treatment with erdatinib at a rate sufcient to generate interest for subsequent randomized study ? success in the study is achieving ve of 31 responses ( 95% ci , 5% to 34% ) , and anything less is failure . 
given the recent history of larotrectinibs fast - tracked approval , it is possible , although remote , that drugs could become approved by the us food and drug administration for tissue - agnostic indications on the basis of match . 
in contrast , tapur aims to identify signals by maximizing the number of patients who benet from matched therapy.35 the question thus addressed in tapur is , as in our example , are there responses to sunitinib among patients whose advanced biliary carcinomas harbor fgfr2 mutation or amplication ? success in the study is not so rigorously dened , with maximization of the total number of responseshelping patientsbeing the overarching goal . 
 precision and accuracy in basket trials what of the situations in which an moi seems pathogenic but is not on the list ? in the context of a clinical trial , reproducible methods to evaluate and approve or reject novel amois , then , are critical to the scientic integrity and generalizability of these trials . 
not surprisingly , approval processes are a function of the trials purpose . as detailed in figure 1 , in the case of match this means in - depth centralized review of data not available to patients or treating physicians and provided only by partner private referral laboratories . 
clearly , as our experience shows , the goals and , consequently , the designs of precision medicine basket trials are not equal , but our hope is that all can agree on a shared set of values . certain principles ought to be adhered to in any novel amoi approval process . 
statistical purists could trials eligibility credibly say that changing a clinical criteria as it progresses limits validity and generalizability a shaky foundation from which to launch a large , expensive randomized study . 
even when a signal is seen in a given match basket ( which , curiously , sometimes consists of both mutations and fusions ) , delineation of the responding amois in a subsequent randomized study would be required . 
in tapur , increased heterogeneity of the study population would not be a fatal aw and may even enhance the possibility of identifying new signals . second , if we fail to account for the known unknowns of a cancerits temporal and spatial heterogeneity36then even the best - intentioned and well - reasoned therapy may fall short of the mark . 
nonstandard information is needed for approval of a novel amoi in match , and neither match nor tapur incorporates quantication of heterogeneity or subsequent evaluation of genetic biomarkers . returning to the case of fgfr2 fusion in cholangiocarcinoma , if investigators had previously identied divergent signals within the fgfr2 arm of the study , then there would be cause for requesting specic fusion breakpoints before attempting therapy . finally , if novel amois are to be included in a precision medicine basket trial , then the referral process should be transparent . 
an open referral process maximizes the opportunity for benecence and minimizes injustices by reducing the chance of two mutationally equivalent prospective enrollees having different clinical outcomes strictly as a result of the differential data - sharing behaviors of private companies . 
in the case of match , by virtue of the private - public partnership that now serves as the foundation of the trial , the process is heterogeneous , and the subsequent analysis of nucleotide - level data is not transparent . 
expertise is needed to interpret tumor sequencing data , but there is no evidence that a group of experts , even at high - volume centers , is better than a single individual physician who is experienced in reviewing sequencing reports and the relevant literature regarding targeted therapies . 
there are not , to our knowledge , data demonstrating that mtbs improve patient outcomes.37 , 38 moreover , there are real questions about the reproducibility of mtbs from institution to institution . 
ultimately , the novel amoi approval process matters , insofar as it is a manifestation of the research question and a litmus test for a basket trials prioritization of accuracy and precision . 
rigor in our case also applies to the original biomarker , fgfr2 , and combining fusions and point mutations fails to yield generalizable conclusions or provide reassuring negative truth claims . our elds bias toward conating precision and accuracy carries risks , especially in the context of precision medicine trials . 
as early precision medicine trials begin to read out , we must be willing to entertain the possibilities that an overemphasis on precision in design fails to generate knowledge useful for the individual patient case and risks making false - negative conclusions . 
going forward , we recommend sober consideration of the goals of a clinical trialthe best - intentioned attempts to open trials to novel amois can inherently defeat the overarching purpose of a trial . 
finally , in the spirit of understanding that each patient represents a unique opportunity for learning , we should ask ourselves the bigger question : is an essentially hypothesisfree basket trial the best use of nite resources , rare genetic events , and patient effort ? the case , continued at the rst sign of logistical issues , the patient was referred , in parallel , to a local nonacademic center with access to the tapur study , for consideration of sunitinib through that studys fgfr2 arsix weeks after presentation to the developmental therapeutics clinic , the novel amoi was approved by the nci . 
 strohbehn and ratain had been evaluated at the tapur referral site and enrolled in a different clinical trial of fgfr2 inhibitor tas - 120 ( foenix - 101 ; clinicaltrials.gov identier : nct02052778 ) the day prior , within 10 days of his presentation to the tapur referral site . 
ratain consulting or advisory role : ascentage pharma , cyclacel , aptevo therapeutics , shionogi research funding : dicerna ( inst ) , abbvie ( inst ) , genentech ( inst ) patents , royalties , other intellectual property : royalties related to ugt1a1 genotyping for irinotecan , royalties related to ugt1a1 genotyping for irinotecan ( inst ) , pending patent related to a genomic prescribing system , pending patent related to a genomic prescribing system ( inst ) expert testimony : testimony and patent litigation consulting on behalf of multiple generic pharmaceutical companies other relationship : value in cancer care consortium , beigene no other potential conicts of interest were reported . references arai y , totoki y , hosoda f , et al : fibroblast growth factor receptor 2 tyrosine kinase fusions dene a unique molecular subtype of cholangiocarcinoma . hepatology 59 : 1427 - 1434 , 2014 jusakul a , cutcutache i , yong ch , et al : whole - genome and epigenomic landscapes of etiologically distinct subtypes of cholangiocarcinoma . 
cancer discov 7 : 1116 - 1135 , 2017 javle m , lowery m , shroff rt , et al : phase ii study of bgj398 in patients with fgfr - altered advanced cholangiocarcinoma . 
mazzaferro a , el - rayes bf , cotsoglou c , et al : arq 087 , an oral pan - broblast growth factor receptor ( fgfr ) inhibitor , in patients ( pts ) with advanced intrahepatic cholangiocarcinoma ( icca ) with fgfr2 genetic aberrations . 
j clin oncol 35 , 2017 ( suppl 15 , abstr 4017 ) deleon tt , ahn dh , bogenberger jm , et al : novel targeted therapy strategies for biliary tract cancers and hepatocellular carcinoma . 
future oncol 14 : 553 - 566 , 2018 egan jb , marks dl , hogenson tl , et al : molecular modeling and functional analysis of exome sequencing - derived variants of unknown signicance identify a novel , constitutively active fgfr2 mutant in cholangiocarcinoma . 
clin cancer res 24 : 847 - 857 , 2018 sia d , losic b , moeini a , et al : massive parallel sequencing uncovers actionable fgfr2 - pphln1 fusion and araf mutations in intrahepatic cholangiocarcinoma . 
wang y , ding x , wang s , et al : antitumor effect of fgfr inhibitors on a novel cholangiocarcinoma patient derived xenograft mouse model endogenously expressing an fgfr2 - ccdc6 fusion protecancer lett 380 : 163 - 173 , 2016 10 . 
tuxen iv , rohrberg ks , oestrup o , et al : copenhagen prospective personalized oncology ( coppo ) - clinical utility of using molecular proling to select patients 13 . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular proling of patients tumors to nd potential targets and select treatments for their 33 : 2753 - 2762 , 2015 to phase i trials . 
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bellmunt j , mullane sa , werner l , et al : association of pd - l1 expression on tumor - inltrating mononuclear cells and overall survival in patients with urothelial carcinoma . 
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wimberly h , brown jr , schalper k , et al : pd - l1 expression correlates with tumor - inltrating lymphocytes and response to neoadjuvant chemotherapy in breast 21 . 
carlson jj , thariani r , roth j , et al : value - of - information analysis within a stakeholder - driven research prioritization process in a us setting : an application in cancer . 
phillips ka , ann sakowski j , trosman j , et al : the economic value of personalized medicine tests : what we know and what we need to know . 
bins s , ratain mj , mathijssen rh : conventional dosing of anticancer agents : precisely wrong or just inaccurate ? clin pharmacol ther 95 : 361 - 364 , 2014 27 . 
ratain mj : body - surface area as a basis for dosing of anticancer agents : science , myth , or habit ? j clin oncol 16 : 2297 - 2298 , 1998 28 . 
giri s , pathak r , martin mg , et al : characteristics and survival of bcr / abl negative chronic myeloid leukemia : a retrospective analysis of the surveillance , epidemiology and end results database . 
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ghazani aa , oliver nm , st pierre jp , et al : assigning clinical meaning to somatic and germ - line whole - exome sequencing data in a prospective cancer precision board . 
however , the interpretation of unexpected cdh1 mutations identified in patients who do not meet igclc criteria or do not have phenotypes suggestive of hereditary diffuse gastric cancer is clinically challenging . 
this study aims to describe phenotypes of cdh1 mutation carriers identified through multigene panel testing ( mgpt ) and to offer informed recommendations for medical management . patients and methods this cross - sectional prevalence study included all patients who underwent mgpt between march 2012 and september 2014 from a commercial laboratory ( n = 26 , 936 ) and an academic medical center cancer genetics clinic ( n = 318 ) to estimate cdh1 mutation prevalence and associated clinical phenotypes . 
cdh1 mutation carriers were classified as igclc positive ( met criteria ) , igclc partial phenotype , and igclc negative . results in the laboratory cohort , 16 ( 0.06% ) of 26 , 936 patients were identified as having a pathogenic cdh1 mutation . 
all three cdh1 mutation carriers who had risk - reducing gastrectomy had pathologic evidence of diffuse gastric cancer despite not having met igclc criteria . conclusion the majority of cdh1 mutations identified on mgpt are unexpected and found in individuals who do not fit the accepted diagnostic testing criteria . 
2017 by american society of clinical oncology introduction mutations in the cdh1 gene cause hereditary diffuse gastric cancer ( hdgc ) , which confers up to an 80% lifetime risk of diffuse gastric cancer ( dgc ) and up to a 60% lifetime risk of female invasive lobular carcinoma ( ilc ) , with the average age at diagnosis being 38 and 53 years , respectively.1 - 3 these high risks , coupled with the difficulty of diagnosing early - stage dgc and current clinical recommendations to consider prophylactic gastrectomy in cdh1 carriers , 4 , 5 highlight the importance and clinical challenges of identifying and managing individuals with cdh1 mutations ( cdh1 + )  . traditionally , genetic testing for cancer susceptibility is performed after the development of a differential diagnosis , including mendelian syndromes caused by a few highly penetrant genes suggested by personal / family history . 
with the advent of multigene panel testing ( mgpt ) , clinicians are able to analyze multiple genes simultaneously , including those lower on the differential diagnosis or not considered at all . 
the international gastric cancer linkage consortium ( igclc ) published guidelines in 2010 ( updated in 2015 ) for identifying individuals as appropriate for cdh1 gene testing4 , 5 ( table 1 ) ; however , multigene panels are now used to test increasing numbers of individuals for cdh1 . we describe a cross - sectional prevalence study of cdh1 + individuals identified by mgpt . 
a retrospective review of two cohorts was performed : the laboratory cohort included all probands , unrelated to our knowledge , who underwent mgpt for cdh1 ( genes analyzed , five to 43 ) at ambry genetics between march 16 , 2012 , and september 30 , 2014 ( n = 26 , 936 ) , and the clinic cohort consisted of all patients who underwent mgpt with cdh1 included in the panel ( genes analyzed , five to 110 ) from april 15 , 2013 , to may 29 , 2014 , at usc ( n = 318 )  . 
for all the patients in the clinic cohort , mgpt was ordered because one or more of the genes included in the panel was the primary target and part of the differential diagnosis . 
no overlap existed between the cohorts in patients who tested positive for cdh1 , and patients who tested negative for cdh1 mutations shared by usc and ambry were excluded from ambrys count . 
for the laboratory cohort , data were abstracted from test requisition forms and by contacting the ordering provider to obtain further pathology , personal and family history , testing information on family members , and outcomes data . 
subsequent blinded classifications were repeated by clinicians at ambry and usc . cdh1 + cases were classified into three categories on the basis of the 2010 igclc guidelines4 : igclc positive ( iglcc - pos ) was defined as mutation carriers who met igclc criteria ; igclc partial phenotype ( igclc - pp ) was defined as mutation carriers who did not meet igclc criteria , but hdgc was in their differential diagnosis because of the presence of gastric cancer , age older than 40 years , or ilc at any and igclc negative ( igclc - neg ) was defined as mutation carriers who did not meet igclc criteria and had no gastric cancer or ilc present in the family . 
myrisk manufactured by myriad genetics ( salt lake city , ut ) ; colonext , brcaplus , breastnext , and cancernext manufactured by ambry genetics ( aliso viejo , ca )  . abbreviations : bc , breast cancer ; bil breast , bilateral breast cancer ; crc , colorectal cancer ; gf , grandfather ; ggf , great grandfather ; ggm , great grandmother ; gm , grandmother ; gyn , gynecologic cancer ; h / n , head and neck cancer ; idc , invasive ductal breast cancer ; igclc , international gastric cancer linkage consortium ; lcis , lobular carcinoma in situ ; mat , maternal ; neg , negative ; nos , not otherwise specified ; pat , paternal ; pos , positive ; pp , partial phenotype ; rcc , renal cell carcinoma ; ua , unaffected . * family members are untested unless otherwise indicated . 
unaffected relatives who tested negative were excluded from this table . case was further reviewed on the basis of the 2015 guidelines.5 e - cadherin immunohistochemistry ( ihc ) staining was conducted on invasive ductal carcinoma ( idc ) tissue when feasible . results in the laboratory cohort , 0.06% ( 16 of 26 , 936 ) of patients were cdh1 +  . 
case cc4 was classified as igclc - pos as a result of family history ; however , the probands presentation was atypical because she was given a diagnosis of idc at age 44 years . 
 a breast 25 colon / rectum 70 ovary 29 breast 48 stomach 66 cdh1 + stomach 52 stomach stomach 71 ovary 40 colon / rectum 71 breast 44 cdh1 + cdh1 + breast 44 cdh1 + prostate 44 stomach 46 stomach 38 colon / rectum 43 cdh1 + clinic case 1 ( cc1 ) classification : igclc - neg result : cdh1 del exons 1 - 2 medical management : recommended prophylactic gastrectomy deferred until completion of breast cancer treatment pathology : ductal breast cancer ihc : expression of cdh1 clinic case 2 ( cc2 ) classification : igclc - pp result : cdh1 c.2164 + 1g > a pathology : lobular breast cancer medical management : prophylactic gastrectomy identified stage i diffuse gastric cancer clinic case 4 ( cc4 ) classification : igclc - pos result : cdh1 c.504del medical management : recommended prophylactic gastrectomy not completed initial pathology : ductal breast cancer ihc : lack of expression of cdh1 ; breast cancer reclassified as lobular e - cadherin immunostain : tumor cells strongly positive for e - cadherin e - cadherin immunostain : negative in tumor cells with positive internal control fig 1 . 
two cases were igclc - pp , and one was igclc - neg because the proband had idc ( confirmed on ihc ) , no family history of cancer , and complete family structure ( fig 1 )  . overall , 20 pathogenic cdh1 mutations were identified . 
one of the probands was unaffected . of patients with cancer , 42% ( n = 8 ) presented with ilc and 21% ( n = 4 ) with gastric cancer consistent with the expected phenotype ; however , 21% ( n = 4 ) presented with idc , 5% ( n = 1 ) with idc with lobular features , 5% ( n = 1 ) with breast neoplasm not otherwise specified , and 5% ( n = 1 ) with colon cancer ( fig 2a )  . 
cases were reviewed to determine whether they met the 2015 guidelines , and case lc17 , initially classified as igclc - pp , met the revised testing criteria as a result of a diagnosis of bilateral ilc at age 45 years.5 therefore , 65% of cases did not meet the 2015 guidelines for consideration of testing . mutation description sixteen distinct pathogenic / likely pathogenic cdh1 alterations were detected in 20 cdh1 + probands , with three recurrent mutations identified ( fig 3 ; data supplement )  . 
a variety of mechanisms lead to pathogenicity , including nonsense - mediated decay6 of mrnas that contain premature termination codons.7 , 8 for cdh1 , nonsense - mediated decay has been shown to cause downregulation of alleles , which results in loss of function.7 of the mutations described , seven are novel to our knowledge ( fig 3 )  . 
both canonical variants are predicted to abolish the native donor splice site by four different splicing prediction tools ( human splicing finder [ hsf ] , maxentscan , berkeley drosophila genome project [ bdgp ] , and esefinder ) , and were classified as likely pathogenic as a result of lack of additional clinical evidence . the six previously described mutations were classified as pathogenic . 
the four different splicing prediction tools ( hsf , maxentscan , bdgp , and esefinder ) predict that these two variants will abolish the native donor site , but we cannot exclude that the use of alternative cryptic donor sites may affect the expressivity of the phenotype in these cases . we detected four multiexon deletions : three ( 59utr_in2del and ex1_2del twice ) include the transcription and translation start sites , and the fourth ( in2_ex5del ) is predicted to include 1 , 237 nucleotides of coding sequence and to be out of frame . 
two different deletions encompassing exons 1 to 2 were previously reported in three families with hdgc ; however , we cannot confirm whether the deletions of this region in the current cohort have the same breakpoints as those previously reported.18 to our knowledge , these deletions contain the only functional translation start sites in the gene and therefore are predicted to abrogate protein synthesis . 
the two families in this cohort with the deletion of exons 1 to 2 were classified as igclc - neg , the family with the deletion that spans from the 59utr through intron 2 was classified as igclc - pp , and the family with the intron 2 through exon 5 deletion was classified as igclc - pos ( data supplement )  . clinical follow - up all cdh1 + clinic cohort patients underwent a discussion of management consistent with hdgc guidelines , 5 and the testing of at - risk family members for the cdh1 mutation was recommended ( subsequent family testing data listed in table 2 )  . one of the four clinic cohort patients elected to proceed with prophylactic gastrectomy . 
for the other three clinical cases , two patients declined prophylactic surgery at this time , and one elected to wait until cancer treatment was completed to make a decision about prophylaxis . 
for one of the laboratory cohort patients who underwent a prophylactic gastrectomy , a family member was seen at usc after identification of the mutation , which allowed additional information to be obtained ( lc12 )  . 
in 15% of patients ( three of 20 [ cc2 , lc12 , and lc6 ] ) , either the proband or the family member is known to have pursued prophylactic gastrectomy and were found to have dgc ( table 3 )  . 
patient lc12 ( proband had idc at age 36 years ) was initially classified as igclc - neg on the basis of a family history of lobular carcinoma in situ in a seconddegree relative ( maternal aunt ) with unknown age of onset and no documented family history of gastric cancer . 
although some of the mutations in the current study have been documented in highly penetrant families , others have not and , therefore , may represent less - penetrant mutations . 
because the threshold for testing for cdh1 changes over time , it is reasonable to anticipate that the cancer risks will have a wider range as families who present outside the high - risk criteria are ascertained , which is consistent with what has been derived in other well - studied cancer predisposition syndromes , such as hereditary breast and ovarian cancer syndrome.25 variable expressivity for cdh1 mutations has been demonstrated in studies of cdh1 + patients with ilc and / or a family history of ilc in the absence of dgc.9 , 14 , 26 consideration of ilc was added to the revised guidelines published in 20155 ( table 1 )  . 
detailed family histories that require deep investigation and retrieval of pathology reports from distant or deceased relatives are helpful when available , and post hoc review of family histories in this study identified previously unconfirmed gastric cancer and lobular breast cancers that changed the classification of risk for some patients who had undergone testing . current management guidelines encourage prophylactic gastrectomy between ages 20 and 30 years and annual breast magnetic resonance imaging starting at age 30 years.4 , 5 these recommendations are based on the cancer risk estimates derived from high - penetrance cdh1 + families . the unexpected cdh1 mutations may reflect an table 3 . 
counseling and support balanced by considerations of risks , benefits , and costs are integral to partnering with these patients for shared decision making about optimal management strategies and their timing . 
the option of gastrectomy in igclc - pp families typically is framed in the context of the family history of cancer , which underscores the importance of obtaining a complete family history and review of pathology reports when available . 
as genomics is further integrated into clinical practice , the gathering of families into research registries is important for long - term follow - up to expand the clinical understanding of cdh1 mutations , including range of cancer risk , and appropriate medical management across the phenotypic spectrum . in conclusion , mgpt identifies cdh1 + individuals who do not meet criteria for cdh1 testing . 
mgpt may provide an opportunity to identify individuals with an increased risk for a highly morbid cancer ( dgc ) before they present with advanced disease , even in the absence of suggestive family history . many of these families presented with cancer histories more suggestive of hereditary breast and ovarian cancer because of early - onset idc , and testing previously may have been limited to the brca genes , which raises the question of whether genetic testing criteria should be broadened to identify more cdh1 + patients . 
at this time , whether the cancer risks in the incidentally identified carriers match the levels reported for classic hdgc families is unclear , although in this series , 100% of cdh1 + patients who underwent gastrectomy had gastric cancer . 
in the absence of comprehensive data on penetrance , we currently recommend classic hdgc management guidelines for all cdh1 mutation carriers.4 , 5 published online on po.ascopubs.org on march 29 , 2017 . immediate family member , inst = my institution . 
espenschied employment : ambry genetics duveen sturgeon no relationship to disclose charit e ricker no relationship to disclose rachid karam employment : ambry genetics research funding : ambry genetics holly laduca employment : ambry genetics julie o . 
 elizabeth chao employment : ambry genetics leadership : ambry genetics stock and other ownership interests : ambry genetics consulting or advisory role : premier genomics julia sturgeon no relationship to disclose virginia speare employment : ambry genetics yanling ma no relationship to disclose kerry kingham no relationship to disclose affiliations marilena melas no relationship to disclose gregory e . 
pharoah pd , guilford p , caldas c : incidence of gastric cancer and breast cancer in cdh1 ( e - cadherin ) mutation carriers from hereditary diffuse gastric cancer families . 
j med genet 47 : 436 - 444 , 2010 [ erratum : j med genet 48 : 216 , 2011 ] van der post rs , vogelaar ip , carneiro f , et al : hereditary diffuse gastric cancer : updated clinical guidelines with an emphasis on germline cdh1 mutation carriers . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
karam r , carvalho j , bruno i , et al : the nmd mrna surveillance pathway downregulates aberrant e - cadherin transcripts in gastric cancer cells and in cdh1 mutation carriers . 
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suriano g , yew s , ferreira p , et al : characterization of a recurrent germ line mutation of the e - cadherin gene : implications for genetic testing and clinical management . 
norton ja , ham cm , van dam j , et al : cdh1 truncating mutations in the e - cadherin gene : an indication for total gastrectomy to treat hereditary diffuse gastric cancer . 
kim s , chung jw , jeong td , et al : searching for e - cadherin gene mutations in early onset diffuse gastric cancer and hereditary diffuse gastric cancer in korean patients . 
brooks - wilson ar , kaurah p , suriano g , et al : germline e - cadherin mutations in hereditary diffuse gastric cancer : assessment of 42 new families and review of genetic screening criteria . 
antoniou a , pharoah pd , narod s , et al : average risks of breast and ovarian cancer associated with brca1 or brca2 mutations detected in case series unselected for family history : a combined analysis of 22 studies . 
 evolving landscape of molecular prescreening strategies for oncology early clinical trials rodrigo dienstmann , md1 ; elena garralda , md , msc2 ; susana aguilar , phd1 ; gemma sala , msc2 ; cristina viaplana , msc1 ; fiorella ruiz - pace , msc1 ; jenifer gonz alez - zorelle , bsc1 , 3 ; deborah grazia logiacco , phd3 ; zighereda ogbah , bsc3 ; laia ramos masdeu , phd3 ; francesco mancuso , bsc3 ; roberta fasani , md4 ; jose jimenez , bsc4 ; paola martinez , bsc4 ; ana oaknin , md , phd2 ; cristina saura , md , phd2 ; mafalda oliveira , md , phd2 ; judith balmaa , md , phd2 ; joan carles , md , phd2 ; teresa macarulla , md , phd2 ; elena elez , md , phd2 ; maria alsina , md , phd2 ; irene braa , md , phd2 ; enriqueta felip , md , phd2 ; josep tabernero , md , phd2 ; jordi rodon , md , phd2 , 5 ; paolo nuciforo , md , phd4 ; and ana vivancos , phd3 most academic precision oncology programs have been designed to facilitate enrollment of patients in early clinical trials with matched targeted agents . 
we started with a tumor - agnostic hotspot mutation panel plus in situ hybridization and immunohistochemistry of selected markers and subsequently transitioned to tumor - specic amplicon - based next - generation sequencing ( ngs ) tests together with custom copy number , fusion , and outlier gene expression panels . 
in parallel , biomarker - matched trials evolved from a scenario of few targets and large populations ( such as pi3k inhibitors in pik3ca mutants ) to a complex situation with many targets and small populations ( such as multiple targetable fusion events )  . 
the substantial increase of immunotherapy trials had a major impact in target prioritization and guided clinical implementation of new markers , such as tumor mutational burden , with larger exonbased ngs assays and gene expression signatures to capture microenvironment inltration patterns . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction during the last decade , when targeted agents entered the phase i clinical trial arena and next - generation sequencing ( ngs ) became a standard molecular prescreening test to identify actionable alterations , oncologists experienced a major shift toward biomarkerdriven drug development.1 there was a lot of enthusiasm with this approach , which culminated with the approval of many targeted drugs in molecularly selected patients on the basis of nonrandomized data . 
more recently , another important milestone was reached with the approval of tissue - agnostic therapies in biomarker - selected population , rst the immune checkpoint inhibitor pembrolizumab in microsatellite instable ( msi ) tumors and then trk inhibitors larotrectinib and entrectinib in cancers harboring ntrk fusions . 
given these exciting advances , many reference institutions initiated precision oncology programs with longitudinal patient cohorts undergoing tumor molecular proling nested to early clinical trials with matched targeted agents.2 in parallel , as advances in immuno - oncology are changing the standard of care of many cancer types , the phase i oncology community experienced another paradigm shift in drug development , with an unprecedented number of new investigational agents entering clinical testing.3 not only different antipd - 1 / l1 inhibitors but also multiple combination regimens are being investigated in early clinical trials . 
more recently , genomic biomarkers are inclusion criteria to select patients for immune checkpoint inhibitor therapy , such as tumor mutation burden ( tmb ) and mutations in dna damage repair ( ddr ) pathway genes . in this evolving scenario , early clinical trial units had to constantly adapt to new biomarker - drug codevelopment trends . 
because the molecular prescreening program was established at our institution , we customized the techniques and procedures to accurately identify molecular alterations in tumors from patients eligible for early clinical trials . 
the team meets periodically to discuss existing molecular tests and new biomarkers of interest to be added to our prescreening progracancer biologists and genomicists participate in weekly molecular tumor board meetings with medical oncologists to provide guidance on the interpretation of ngs results and discuss new markers for clinical testing in patients eligible for early clinical trials . as detailed in figure 1a , we started with a targeted single base extension mutation assay covering hotspot events in 20 oncogenes and tumor suppressor genes ( sequenom ) plus uorescent in situ hybridization ( fish ) or immunohistochemistry ( ihc ) analysis of selected genes and proteins . 
in 2013 we implemented an ncounter rna platform ( nanostring ) fusions and gene expression ( gex ) analysis of 26 genesfusion and gex ncounter . in 2014 we substituted the hotspot mutation panel with a custom amplicon - based ngs assay covering 59 genes ( miseq ) , and 1 year later we replaced the fish analysis with a targeted copy number ncounter dna panel of 44 genescna ncounter . 
during 2015 we also added brca1 / brca2 genes to the ngs panel , introduced pdl1 ihc and msi testing by ihc ( with polymerase chain reactionbased test in equivocal cases )  . 
in 2018 we developed an exonbased ngs assay ( hiseq ) with 420 genes , encompassing ddr plus epigenetic pathway genes and ne - tuned for tmb quantication and other genomic signatures , such as msi . 
so far , this assay is limited to selected cases of particular interest , as per discussions in weekly molecular tumor boards , but will eventually replace the amplicon ngs and nanocopy dna panels in the coming year . 
to identify patients eligible for antibody - drug conjugates , different ihc assays were developed in collaboration with pharmaceutical companies , which allowed local testing instead of sample shipment for central proling . 
most pharmaceutical companies also accept our in - housedeveloped genomic testing as screening for biomarker - guided trials , but we noticed that a growing number of early clinical trials mandate central ngs companion diagnostic tests , specically in lung , bladder , and biliary tract cancers . all assays were optimized for archived formalin - xed parafn - embedded tumor tissues . 
importantly , ngs assays had frequent modications in gene coverage to capture emerging biomarkers being investigated in clinical trials at our institution , such as the recent additions of notch family genes to the mutation panel , ntrk breakpoints to the fusion assay , and cd274 ( pd - l1 ) to the cna ncounter test . 
in 2018 , the amplicon - based ngs panel was tailored as multiple tumortypespecic panels , with coverage limited to genes that have been previously found to be mutated in each malignancy . 
finally , circulating tumor dna ( ctdna ) mutation detection panels are under development but still limited to patient cohorts with predened tumor types participating in validation studies . each oncologist has the responsibility to dene a patients eligibility for molecular prescreening on the basis of clinical features , tumor type , and disease setting . 
cna ncounter , copy number alteration nanostring panel ; fish , uorescent in situ hybridization ; fusion and gex ncounter , fusion and gene expression nanostring panel ; ihc , immunohistochemistry ; msi , microsatellite instability ; ngs , next - generation sequencing . yield ( combined prevalence of targetable molecular alterations ) exceeds 3% . 
depending on the tumor type , molecular tests are performed up front ( such as in lung cancer when sufcient tissue is available for ngs ) , while patients receive standard - of - care chemotherapies ( such as biliary tract cancer and hormone receptorpositive breast cancer ) , or after progression to approved regimens ( such as cervical cancer )  . 
we educate clinicians not to indicate ngs as a rescue diagnostic test to identify targets for experimental therapies when patients have fast clinical deterioration , but also to avoid the all - comers up - front strategy , given the potential reduced cost effectiveness of this approach for all advanced tumor types . 
 dienstmann et al after the patient signs informed consent for broad tumor molecular proling , requests are submitted to the molecular oncology unit for sample retrieval , qualication , and preparation , and to perform ihc / fish tests . 
turnaround time is , 1 week for ihc or fish tests and approximately 2 weeks for the amplicon - based ngs panel ; ncounter results are reported within 2 - 3 weeks and exon - based ngs panel in 3 - 4 weeks . 
depending on the assays coverage , it serves as a substitute for the internal program . our molecular prescreening program is free of charge to patients and nanced with both internal resources acquired through competitive grants or donations ( institutional patronage ) and external funds from agreements with pharmaceutical companies running early clinical trials with mandatory biomarker matches . 
in the latter case , which represents 15% of total budget , the conancing models can be a molecular prescreening fee for each patient recruited in the trial or a pay - per - test fee while the trial is recruiting patients ( with monthly reports detailing number of tests performed and positive results )  . as shown in figure 1b , close to 2 , 500 molecular tests were performed in 2018 , a 10 - fold increase as compared with 2010 . 
in 2010 , most early therapeutic trials tested pi3k pathway inhibitors ( n = 11 ) , whereas in 2018 , immunotherapy trials represented the great majority ( n = 75 ) , followed by antibody - drug conjugates ( n = 9 ) , epigenetics ( n = 9 ) , fgfr inhibitors ( n = 9 ) , pi3k pathway inhibitors ( n = 8 ) , mek / erk inhibitors ( n = 8 ) , and egfr / erbb2 inhibitors ( n = 7 )  . 
regarding phase i trials with targeted drugs ( fig 2a ) , we observed a gradual increase in the number of targets of interest for clinical development from 2010 to 2016 , including alk / ros1 , fgfr1 - 3 , braf , met , notch1 - 2 , ddr pathways alterations , and others ( hdm2 , kit , pdgfr , idh1 - 2 , ret , ntrk1 - 3 , cyclin , and wnt pathways )  . 
this was accompanied by a major increase in the number of immunooncology trials , which escalated since 2015 ( fig 2b )  . the criteria for patient enrollment in a given trial go beyond genomic markers . 
in cases of borderline evidence of clinical actionability of molecular targets ( enrichment criteria ) or no oncogene alteration , alternative therapies are considered , type and taking into consideration tumor availability of slots in trials with immunotherapies and other drugs . 
more recently , immune - related markers are used as positive selection criteria for clinical trials with novel immune - oncology drugs and combinations . out of 161 early clinical trials actively recruiting patients in 2018 , 57 investigated targeted agents ( fig 2a ) , 24 of them ( 42% ) were combination regimens , and 48 ( 84% ) had mandatory or enrichment molecular inclusion criteria , the most common being fgfr , mapk , pi3k , egfr / erbb2 , and ddr pathway alterations . 
regarding immunotherapy trials , 57 out of 75 ( 76% ) were combination regimens and 32 ( 43% ) had mandatory or enrichment molecular criteria for recruitment , with pd - l1 expression and msi status being the most common biomarkers ( figs 2b and 2d )  . 
we also gradually increased the number of clinical trials testing antibody - drug conjugates , most of them with mandatory ihc analysis for patient selection , and epigenetic targets , rarely recruiting patients on the basis of genomic proling ( as brd4 - nut fusions for bet inhibitors )  . inclusions in clinical trials with targeted agents uctuated from 2010 to 2018 ( fig 2c )  . 
the multiplicity of drug targets under investigation coupled with a growing number of molecular tests being performed during this period allowed recruitment of more patients in phase i including trials assessing novel biomarkers , fgfr1 - 3 , notch1 - 2 alterations , and brca1 - 2 mutations , among others . 
we observed a major decrease in recruitment rates in phase i trials with targeted agents in 2017 , in part related to lower interest in some targets , such as pi3k pathway inhibitors , but also a 3 - fold increase in the number of patients referred to phase ii or iii trials with molecular matches , from 84 in 2016 to 224 in 2018 . 
chemo , chemotherapy ; immuno , immunotherapy ; msi , microsatellite instability . 306 patients recruited in immunotherapy trials during 2018 , 92 ( 30% ) were based on biomarkers . to investigate the clinical utility of our program , we assessed how the results of proling ( both in - house and external ) affected the immediate treatment decision of each patient . 
the most common tumor types undergoing molecular proling in the last 3 years are shown in figure 3a . in 2018 , we noticed an increase in lung , breast , and pancreatobiliary cancers being tested in line with major advances in precision cancer therapy across these tumor types . 
it is important to emphasize that these represent patients not eligible for standard - of - care genomically guided therapy , such as braf inhibitors in brafv600emutated melanomas , or her2 - targeted therapy in erbb2amplied breast cancer . 
 a 2016 ( n = 1 , 281 ) 18 19 26 dienstmann et al 2017 ( n = 1 , 218 ) 15 22 18 1 , 104 2018 ( n = 1 , 416 ) 18 12 18 colorectal lung breast pancreatobiliary gynecologic gastric head and neck other brain urinary sarcoma skin endocrine inner ring no trial immunotherapy nonimmunotherapy matched phase 1 - 3 trial outer ring biomarker mandatory biomarker enrichment fig 3 . 
 ( b ) recruitment in biomarker - guided ( mandatory or enrichment ) and other alternative trials ( immunotherapy or nonimmunotherapy )  . guided targeted agents , antibody - drug conjugates , and immunotherapies . discussion the vall dhebron institute of oncology ( vhio ) molecular prescreening program is constantly adapting to the needs of our early clinical trial portfolio . 
we observed a dramatic change in the landscape of phase i clinical trials , now focused on targeted agents for rare molecular alterations , immunotherapy combinations , antibody - drug conjugates , and epigenetic agents . 
in parallel , different ngs assays were developed for accurate detection of rare actionable mutations , copy number alterations , fusion events , and novel ihc tests were introduced . from the beginning , we followed a personalized prescreening approach , whereby oncologists are empowered to decide which patients are eligible for testing based on clinicopathological features and which molecular tests are indicated in each disease setting . 
by avoiding the one - testfor - all strategy , we were able to optimize the use of our prescreening program and educate the clinicians on molecular epidemiology of each tumor type as well as emerging diagnostic tests . 
the decision to transition from smaller tumor - specic panels to a larger exon - based ngs that covers both mutation and copy number tests is related to the need to accommodate emerging biomarkers in the ddr and epigenetic pathways as well as tmb quantication . 
overall , 1 out of 10 patients proled are ultimately enrolled in matched targeted trials , which is in line with other academic molecular prescreening programs with nested clinical studies.4 regarding germline sequencing , we follow guideline - directed testing and have regular meetings with genetic counselors to discuss secondary incidental ndings in tumor sequencing.5 in the last decade , biomarker - matched trials evolved from a scenario of few targets and large populations to a complex situation with many targets and small populations . 
even with a growing number of targets being investigated in phase i trials , and the multiplicity of trials per target , we observed a relative reduction in the number of patients enrolled in molecularly guided trials in the last years . 
this is the result of shifting interests in drug development and a clear focus on a limited number of promising biomarkers , such as rare fusion events in fgfr1 - 3 , ret , and ntrk1 - 3 genes . 
in this scenario , liquid biopsies for target identication are becoming quite useful , which has guiding our current development of a ctdna ampliconbased ngs test and prompted collaborations with commercial partners for molecular prescreening . the substantial increase in immunotherapy trials had a major impact on trial prioritization . 
inclusion criteria of immuno - oncology phase i trials are frequently limited to tumor type and treatment line , with few trials having a mandatory molecular match , which facilitates patient recruitment . 
we noticed an increase in biomarker - guided immunotherapy trial recruitment in 2018 , which is guiding implementation of a multimodality biomarker strategy that moves beyond tmb quantication , such as immune cytotoxic / suppressive microenvironment signatures measured through the gex ncounter panel , 6 as well as multiplex ihc panels.7 to conclude , we believe that to accelerate progress in precision oncology , clinical trials with adaptive designs to enroll patients on the basis of multiomics enrichment criteria are needed . 
the previous era of molecularly guided targeted agents is restrictive , and larger portfolios of drugs that include immunotherapeutic and antibody - drug conjugates with recruitment guided by molecular tests must be pursued . 
in our view , the future of cancer drug development will encompass sequential genomic proling to guide matched targeted therapies , complex multimodality biomarkers for immune - oncology agents , individualized immunotherapeutics , novel combination regimens with epigenetic drugs , and antibody - drug conjugates . 
as precision oncology becomes a more paved road , clinicians in the community oncology setting must be cognizant of its full potential and reference institutions must establish patient referral networks to increase the access to innovative experimental therapies . 
 dienstmann et al speakers bureau : msd , roche , thermo fisher scientic research funding : novartis , roche ( inst ) , thermo fisher scientic ( inst ) travel , accommodations , expenses : bristol - myers squibb , menarini , glycotope , merck sharp & dohme ana oaknin consulting or advisory role : roche , astrazeneca , pharmamar , clovis oncology , tesaro , immunogen , genmab research funding : abbvie deutschland ( inst ) , ability pharmaceuticals ( inst ) , advaxis ( inst ) , aeterna zentaris ( inst ) , amgen ( inst ) , aprea therapeutics ( inst ) , clovis oncology ( inst ) , eisai ( inst ) , f . 
mandelker d , donoghue m , talukdar s , et al : germline - focussed analysis of tumour - only sequencing : recommendations from the esmo precision medicine working group . 
lu s , stein je , rimm dl , et al : comparison of biomarker modalities for predicting response to pd - 1 / pd - l1 checkpoint blockade : a systematic review and meta - analysis . 
calvo f , apolone g , baumann m , et al : cancer core europe : a european cancer research alliance realizing a research infrastructure with critical mass and programmatic approach to cure cancer in the 21st century . 
we then used polymerase chain reaction to quantify gene expression in diagnostic biopsy tissue across a prospectively designed archival cohort of 754 consecutive thinand intermediate - thickness primary cutaneous melanomas . 
a penalized maximum likelihood estimation algorithm was used to train logistic regression models in a repeated cross - validation scheme to predict the presence of sln metastasis from molecular , clinical , and histologic variables . results expression of genes with roles in epithelial - to - mesenchymal transition ( glia - derived nexin , growth differentiation factor 15 , integrin - 3 , interleukin 8 , lysyl oxidase homolog 4 , transforming growth factorreceptor type 1 , and tissue - type plasminogen activator ) and melanosome function ( melanoma antigen recognized by t cells 1 ) were associated with sln metastasis . 
per current guidelines ( table 1 ) , slnb is not recommended if the risk of nodal metastasis is , 5% , as in melanoma with a breslow thickness of , 0.8 mm and no adverse features . 
the key objective of this study was to identify primary melanoma clinicopathologic ( cp ) variables and a gene expression prole ( gep ) that associate with a low risk of sln metastasis . knowledge generated cp variables in combination with an eight - gene gep tied to epithelial - to - mesenchymal transition as a biologic process inherent to metastasis effectively stratied melanoma according to its likelihood of sln metastasis . relevance our cp - gep model promises to work as an sln biopsy reduction tool . 
10% risk of shortand long - term complications , including bleeding , infection , lymphocele , lymphatic stula , pain , neuropathy , and lymphedema , 7 as well as an up to 5% risk of hospital readmission within 30 days because of postsurgical complications.8 better methods are needed to identify patients whose risk of nodal metastasis is so low that they may safely forgo slnb . 
here , we report the design of a model that combines established clinicopathologic ( cp ) variables with a gene expression prole ( gep ) to identify patients who have , on average , a risk of nodal metastasis of , 5% . 
of the 754 patients in this cohort , 373 were included in a previously published cohort.10 all specimens were analyzed by quantitative polymerase chain reaction ( pcr ) between february 2018 and october 2018 . eligibility was determined on the basis of histopathology data derived from patient medical records and established by two or more board - certied mayo clinic dermatopathologists . inclusion was determined by the ajcc 7th edition on the basis of institutional practice guidelines of the mayo clinic for recommending slnb , which were based on breslow thickness , ulceration , mitoses , and age . 
 molecular model to assess sentinel lymph node metastasis risk exclusion criteria were m1 disease within 90 days of primary diagnosis ; insufcient primary tumor diagnostic biopsy tissue ; inadequate rna harvested ; and , for minnesota , denial of access to medical records for research purposes ( per minnesota state law )  . 
because there is an ongoing debate about the relevance of , 0.1 mm metastasis in sln ( ie , isolated tumor cells [ itcs ] and cell clusters , 0.1 mm in diameter ) , patients with , 0.1 mm metastasis were excluded from model development . 
isolated benign melanocytes and histiocytic melanophages can be present elsewhere in the sln and mimic itcs.13 some authors cautioned against hidden tumor burden in , 0.1 mm metastatic sln and highlighted the need for enhanced pathology assessment protocols.14 , 15 others found that , 0.1 mm metastasis has no impact on prognosis compared with negative slns.16 , 17 enrollment of patients and inclusion and exclusion criteria are summarized in appendix figure a1 . 
this study was approved by the mayo clinic institutional review board . gene expression by quantitative pcr see the appendix for details . statistical methods logistic regression and least absolute shrinkage and selection operator . 
features with a tolerance 0.15 were removed from the input data set ( the tolerance represents the fraction of variance in the kth feature that cannot be accounted for by other features )  . 
the output of logistic regression models estimated the probability of sln metastasis and was converted into binary results : samples with a probability of metastasis greater than the cutoff were classied as positive , whereas samples with a probability lower than the cutoff were classied as negative . 
the performance metrics of the classiers are listed in appendix table a2 and are cutoff specic , except the area under the receiver operating characteristic curve ( auc )  . double - loop cross - validation . 
however , splitting the available data just once into a training set and a test set may be viewed as inefcient.19 a better solution is to estimate the average performance of the model by repeated cross - validation or bootstrapping . 
here , we opted for a repeated crossvalidation scheme ( ie , double - loop cross - validation [ dlcv ] ) .20 the key idea of dlcv is to get a reliable estimate of the outof - sample performance of a classier by averaging the performance of multiple classiers trained in cross - validation a number of times ( appendix fig a2 )  . 
see the appendix for details . memorial sloan kettering cancer center nomograsee the appendix for details . results epithelial - to - mesenchymal transition in high - risk melanoma to identify candidate genes tied to biologic processes inherent to metastasis and differentially expressed between metastatic and nonmetastatic melanoma , we rst reviewed rna sequencing data obtained previously.10 genes with a false discovery rate of , 0.01 in a comparison of either benign nevi and cutaneous melanoma or cutaneous melanoma with and without sln metastasis were selected for further qualication . 
a total of 194 candidate biomarkers and 3 control genes were screened for performance in breslow thickness and age - matched case - control studies by quantitative pcr ( appendix table a3 )  . 
we noted that genes predictive of nodal metastasis had been associated with epithelial - to - mesenchymal transition ( emt ) , a biologic process known to promote metastasis in primary cutaneous melanoma.21 our prospectively designed archival cohort22 comprised 754 patients with thinand intermediate - thickness primary cutaneous melanoma who underwent an slnb within 90 days of diagnosis ( table 2 )  . 
of 754 patients , 128 ( 17% ) were sln positive , in agreement with the typical prevalence in an slnb - eligible population.3 our approach was to develop models of the likelihood of sln metastasis on the basis of either cp variables ( cp models ) or geps of the primary tumor ( gep models ) and then to assess the performance of a combined model of cp and gep factors ( cpgep models )  . 
 ( % ) characteristic other mixed not documented negative ( n = 626 ) positive ( n = 128 ) 4 of 626 ( 0.6 ) 6 of 626 ( 1.0 ) 31 of 626 ( 5.0 ) 2 of 128 ( 1.6 ) 6 of 128 ( 4.7 ) abbreviations : sd , standard deviation ; slnb , sentinel lymph node biopsy . acomparisons of patients with slnb - negative and - positive outcomes were performed using the 2 test for categorical variables , the twosample t test for patient age , and the wilcoxon rank sum test for all other variables . using gene expression to predict sln metastasis dlcv and lasso were used to identify a gep dened from 11 genes that differentiated the patients with and without nodal metastasis detected by slnb within 90 days of primary diagnosis : adam metallopeptidase domain 12 ( adam12 ) , interleukin 8 ( cxcl8 ) , growth differentiation factor 15 ( gdf15 ) , integrin - 3 ( itgb3 ) , galectin 1 ( lgals1 ) , lysyl oxidase like 4 ( loxl4 ) , melanoma antigen recognized by t cells 1 ( mlana ) , tissue - type plasminogen activator ( plat ) , protein kinase c ( prkcb ) , glia - derived nexin ( serpine2 ) , and transforming growth factor ( tgf ) receptor 1 ( tgfbr1 )  . 
finally , logistic regression modeling was used to develop a novel model combining cp factors ( ie , breslow thickness and patient age ) and a gep . the combined cp - gep model was based on the expression of mlana , a melanosome marker , 23 and seven genes functionally linked to emt and with specic roles in angiogenesis / hypoxia and coagulation : gdf15 , 24 - 26 cxcl8 , 27 , 28 loxl4 , 29 , 30 tgfbr1 , 31 , 32 itgb3 , 33 - 36 plat , 37 , 38 and serpine239 , 40 ( table 3 )  . 
the cp - gep model , therefore , promised to work as an slnb reduction tool : patients with a negative test may forgo slnb because their risk of nodal metastasis is , on average , , 5% , a reduction from the pre - test probability41 ( table 1 )  . for a predictor of sln status to be clinically relevant , it must change the pretest probability within each t category of melanoma . 
the high slnb reduction rate for t1b melanoma is particularly meaningful in light of the increasing incidence of thinner melanoma , 42 for which cp variables are less predictive.5 to further dene the clinical relevance of the cp - gep model , we compared cp - gep performance to the wellknown memorial sloan kettering cancer center ( mskcc ) nomogram for predicting sln metastasis . 
shown are the models that are based on the mskcc nomogram , clinicopathologic variables ( cp model ) , and gene expression prole ( gep ) and cp variables combined ( cp - gep model )  . 
curves are averages over 100 repeats obtained by concatenating the threefold crossvalidation test results . that the mskcc nomogram performed similarly to the cp model but was outperformed by the cp - gep model in auc ( appendix fig a5 ) and slnb reduction rate ( fig 2 )  . discussion while completion lymphadenectomy for which slnb was a key determinant has fallen out of favor , 43 , 44 slnb continues to determine patient eligibility for adjuvant therapy . unfortunately , the majority of slnb procedures performed today are negative , which conrms only the low - risk nature of the primary tumor without inuencing decision making toward adjuvant therapy . 
here , we present a model that considers gene expression and cp variables ( ie , breslow thickness and patient age ) to assess the likelihood of sln metastasis in patients diagnosed with thinand intermediate - thickness primary cutaneous melanoma . 
the ability to characterize melanoma at the molecular level reduces the need for slnb , a surgical procedure that carries a risk of complications.7 our approach of combining cp factors with molecular proling better identies patients who may forgo the slnb procedure because of their low risk of metastasis . for melanoma with a 5% - 10% chance of sln metastasis ( breslow thickness , 0.8 - 1 mm ) , slnb is optional but should be discussed with the patient.45 even though slnb in this risk group is optional ,  . 
50% of affected patients in the united states undergo slnb.46 the majority of these patients have negative slnb ndings , which highlights our current dilemma with melanoma risk stratication and the limitations of histopathology alone as a predictor of regional metastasis . 
multivariable models have used breslow thickness , tumor ulceration , and patient age to predict sln status , with age being a negative predictor and breslow thickness as well as tumor ulceration being strong positive predictors.47 - 50 angiolymphatic invasion was also found to positively correlate with sln metastasis in some models.5 , 51 the most ambitious cp models , such as those developed from a large bi - institutional series , achieved slnb reduction rates of 18% - 30% , with a negative predictive value table 4 . 
in comparison , the cp plus molecular model developed here showed an slnb reduction rate of 42% at a negative predictive value of 96% ( appendix table a4 )  . 
there seems to be a clear limit in the ability of cp factors to predict sln metastasis . to improve the performance of predictive models , we developed a gep from primary diagnostic biopsy tissue . gep has been used successfully in breast cancer to individualize therapy.52 previous research on gene expression in invasive breast cancer , 53 prostate cancer , 54 colon cancer , 55 melanoma , 10 and other solid cancers56 has consistently demonstrated the upregulation of adhesion receptors and secreted factors that remodel the tumor microenvironment and are involved in emt.10 , 53 - 57 here , we have conrmed this upregulation and found genes involved in emt with specic roles in angiogenesis ( growth differentiation factor 15 , 25 interleukin 8 , 28 lysyl oxidase homolog 4 , 58 tgfreceptor type 1 , 32 and integrin 334 ) and coagulation ( tissue - type plasminogen activator , 38 and gliaderived nexin40 ) as well as the melanosome biogenesis marker melanoma antigen recognized by t cells 123 to be associated with sln metastasis ( table 3 )  . 
the functional roles of these genes have been demonstrated by genetic approaches32 , 34 , 38 , 59 and pharmacologic efcacy studies where the inhibition of integrin - 3 by cyclic peptide , 60 tgfreceptor type 1 by kinase inhibitor , 61 and interleukin 8 by neutralizing antibody62 reduced tumor angiogenesis , tumor growth , and metastasis . 
tumor vascularity in melanoma diagnostic biopsy tissue is well known to associate with nodal and distant metastasis but has been difcult quantify in the past.63 likewise , constitutive brinolytic activity in tumor tissue has been described as early as 191164 and attributed largely to plasminogen activators38 and other serine proteases , such as glia - derived nexin , 65 which promote metastasis , 66 disseminated intravascular coagulation , and bleeding in patients with metastatic cancer.67 a drawback of the simultaneous selection of cp variables and genes by our feature selection algorithm is the absence of established variables easily recognizable by clinicians , such as ulceration , in the cp - gep model . 
moreover , we excluded t4 lesions ( ie , melanoma with a breslow thickness , 4 mm ) because the pretest probability of regional metastasis for these patients is very high . 
for example , 21 ( 70% ) of 30 patients with t4 lesions in our cohort presented with regional metastasis , which is well above the recommend threshold for recommending slnb . 
finally , eligibility of patients with t1 melanoma was determined by the mayo clinic institutional practice guidelines for recommending slnb , which select for higher - risk patients , such as those , 40 years of age and with t1b melanoma . 
however , slnb to slnb metastasis risk was only , 5% if cohorts were enriched for a priori low - risk cases , such as by including t1a melanoma or restricting the analysis to patients  . 
previous attempts to develop molecular risk factors have been limited by small cohort sizes , incomplete tnm staging data , or limited clinical utility of the resulting models.49 , 69 , 70 our approach of combining cp factors and gene expression variables improved the performance of cp factors alone by outperforming current clinical practice and important benchmarks , such as the mskcc nomograthe combined cp - gep model maintained an average negative predictive value of  . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . domenico bellomo employment : skylinedx stock and other ownership interests : synlogic , skylinedx patents , royalties , other intellectual property : gene signatures for predicting metastasis of melanoma julia s . 
van vliet employment : skylinedx stock and other ownership interests : skylinedx patents , royalties , other intellectual property : named inventor on patents in the multiple myeloma eld jvalini dwarkasing employment : skylinedx stock and other ownership interests : skylinedx alexander meves research funding : skylinedx patents , royalties , other intellectual property : mayo clinic has led several patent applications on which i am listed as an inventor ; technologies are in the area of wound healing and skin cancer ( inst ) open payments link : 478139 no other potential conicts of interest were reported . acknowledgment we thank vera j . 
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zhang m , kleber s , r ohrich m , et al : blockade of tgfsignaling by the tgfr - i kinase inhibitor ly2109761 enhances radiation response and prolongs clin cancer res 11 : 6270 - 6279 , 2005 survival in glioblastoma . 
huang s , mills l , mian b , et al : fully humanized neutralizing antibodies to interleukin - 8 ( abx - il8 ) inhibit angiogenesis , tumor growth , and metastasis of human 63 . 
boulaftali y , ho - tin - noe b , pena a , et al : platelet protease nexin - 1 , a serpin that strongly inuences brinolysis and thrombolysis . 
 molecular model to assess sentinel lymph node metastasis risk appendix methods quantitative polymerase chain reaction ( pcr ) was performed as previously described.10 rna purication was from formalin - xed parafn - embedded tissue ( qiagen , hilden , germany )  . 
gene expression was corrected by the mean of housekeeping genes ( rlp0 , rlp8 , and - actin ) using the ct method . statistical methods double - loop cross - validation . 
in the inner loop ( 10 - fold cross - validation ) , we optimized the parameter by determining the number of features ( ie , the weight of the least absolute shrinkage and selection operator penalty term ) , and in the outer loop ( threefold cross - validation ) , we designed a classier on the training set ( two of the three folds )  . 
next , we assessed the performance of the trained classier on the remaining fold ( test set ) , with the parameter xed to the value estimated in the training set . 
the nal classiers were trained on the entire data set using the average ? parameter over 300 runs . memorial sloan kettering cancer center nomograthe majority of online tools for melanoma provide prognostic information47 ( zabor et al : ann surg oncol 25 : 2172 - 2177 , 2018 )  . 
the memorial sloan kettering cancer center ( mskcc ) nomogram , in contrast , is a tool specically designed to predict the probability of primary cutaneous melanoma metastasis to sln.23 the nomogram corresponds to a logistic regression model that is based on ve clinicopathologic variables : age ( range , 20 - 95 years ) , breslow thickness ( range , 0.1 - 10 mm ) , clark level ( ii , iii , iv , or v ) , biopsy location ( trunk , extremity , or head and neck ) , and tumor ulceration ( yes or no )  . 
while attempting to apply the nomogram to our cohort , we could not calculate the probability of sln metastasis for 16 patients because of missing values or because the values were outside the allowable range for the nomograsix patients were , 20 years of age , seven had a missing clark level ( one of whom was also , 20 years of age ) , and four did not have ulceration status available . 
study ow diagrathe gure depicts the enrollment of patients , inclusion and exclusion criteria , and other potential sources of retrospective bias such as the absence of research consent , the unavailability of tissue for molecular analysis , or failed gene expression proling ( gep )  . 
 molecular model to assess sentinel lymph node metastasis risk x 10 cvs x 100 repeats x 3 cvs train train test train test train average test performance test train train select optimal for lasso penalty fig a2 . 
the dlcv consists of two nested cross - validation loops : in the inner loop ( tenfold cross - validation ) , we estimate the optimal parameter , namely , the weight of the lasso penalty term ( ie , optimal feature selection ) ; in the outer loop ( threefold cross - validation ) , we assess the performance of the classier on each test set , with the parameter as determined in the training set . 
moreover , in each training set of the outer loop , we choose and x an operating point on the receiver operating characteristic curve , and we assess the performance of the classier at that operating point in the corresponding test set . 
the cross - validation procedure has been repeated 100 times , and unless otherwise stated , we reported the average performance over 300 test sets ( three test sets per outer loop , repeated 100 times )  . 
lasso , least absolute shrinkage and selection operator . cp1 ; auc , 0.78 cp2 ; auc , 0.78 cp3 ; auc , 0.78 cp4 ; auc , 0.77 cp5 ; auc , 0.77 cp6 ; auc , 0.77 false - positive rate fig a3 . 
 bellomo et al cp model ; auc , 0.78 gep model ; auc , 0.78 combined cp - gep model ; auc , 0.82 false - positive rate fig a4 . 
blue line , model for predicting sentinel based on cp variables ( cp model ) ; red line , model based on gene expression prole ( gep model ) ; teal line , model based on combined gep and cp variables ( cp - gep model )  . 
curves are averages over 300 double loop crossvalidationgenerated test sets . mskcc nomogram ; auc , 0.77 cp model ; auc , 0.78 combined cp - gep model ; auc , 0.82 false - positive rate fig a5 . 
orange line , model based on mskcc nomogram ; blue line , model based on cp variables ( cp model ) ; teal line , model based on gene expression and cp variables combined ( cp - gep model )  . 
clinicopathologic variables available for statistical modeling clinicopathologic variable age categorical biopsy location biopsy location mskcc breslow thickness breslow thickness categorical mitotic rate categorical clark level ulceration regression tumor - inltrating lymphocytes microsatellitosis angiolymphatic invasion histology type abbreviation : mskcc , memorial sloan kettering cancer center . head and neck , trunk , upper extremity , lower extremity , acral value female , male years 15 - 39 years , 40 - 59 years , 60 years head and neck , trunk , extremity millimeters , 1 mm , 1 - 2 mm , 2 - 4 mm 0 / mm2 , 1 - 6 / mm2 ,  . 
6 / mm2 , not determined ii , iii , iv , v yes , no , not determined yes , no , not determined absent , nonbrisk , brisk , not determined yes , no , not determined yes , no , not determined supercial spreading , nodular , desmoplastic , lentigo maligna , acral lentiginous , spindled , dermal , spitzoid , nevoid , unclassied , other , mixed , not determined table a2 . 
average performance of the cp , gep , and combined cp - gep models were trained in double - loop cross - validation 300 times . performance is shown for the 754 - patient cohort assembled on the basis of inclusion criteria and devoid of patients with equivocal sln metastasis ( ie , patients with , 0.1 mm metastatic disease )  . 
 o evaluation of the her / pi3k / akt family signaling network as a predictive biomarker of pathologic complete response for patients with breast cancer treated with neratinib in the i - spy 2 trial purpose in the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) , the panerythroblastic oncogene b inhibitor neratinib was available to all hormone receptor ( hr ) / human epidermal growth factor receptor 2 ( her2 ) subtypes and graduated in the hr - negative / her2 - positive signature . 
we hypothesized that neratinib response may be predicted by baseline her2 epidermal growth factor receptor ( egfr ) signaling activation / phosphorylation levels independent of total levels of her2 or egfr proteins . materials and methods complete experimental and response data were available for between 130 and 193 patients . 
in qualifying analyses , which used logistic regression and treatment interaction analysis , 18 protein / phosphoprotein , 10 mrna , and 12 dna biomarkers that related to her family signaling were evaluated . 
 exploratory analysis of her family signaling in patients with triple - negative ( tn ) disease found that activation of egfr y1173 ( p = .005 ) and her2 y1248 ( pher2 ) ( p = .019 ) were positively associated with pathologic complete response . 
exploratory analysis in this pegfr / pher2activated tn subgroup identified elevated levels of estrogen receptor ( p < .006 ) in these patients . conclusion activation of her family phosphoproteins associates with response to neratinib , but only egfr y1173 and stmn1 appear to add value to the graduating signature . 
 introduction the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ; clinicaltrials.gov identifier : nct01042379 ) is a phase ii , adaptive neoadjuvant therapy trial in which the primary goal was to determine the predictive probabilities of phase iii trial success for various targeted therapeutics . 
patients with locally advanced , high - risk breast cancer had their diseases assigned to one of eight subtypes on the basis of hormone receptor ( hr ) , human epidermal growth factor receptor 2 ( her2 ) , and mammaprint - based high1 / ( ultra ) high2 risk statuses.1 - 3 neratinib , a pan - erythroblastic oncogene b ( erbb ) inhibitor , was available to patients with all tumor subtypes in the i - spy 2 trial , and the agent availability was graduated in the hr negative / her2 - positive signature.4 neratinib has shown activity against her2 - positive metastatic breast cancer , and there is also evidence for activity against her2 - negative tumor cells in vitro.5 , 6 because neratinib was available to all patients in the trial , this study provided an opportunity to test the efficacy of the drug in patients with her2 - negative tumors . cell linebased preclinical studies have implicated alterations in her / akt / mtor family genes on the dna , mrna , or protein level as predictive of neratinib response.7 - 11 however , recent her2 therapybased clinical trials in which her family biomarkers at the total protein and / or mrna level were analyzed for response prediction found that none provided predictive value compared with the conventional , us food and drug administrationapproved immunohistochemistry ( ihc ) / fluorescence in situ hybridizationbased her2 / estrogen receptor ( er ) testing methods.12 - 14 previous work with the i - spy 1 trial cohort revealed that her2 phosphorylation was highly concordant with her2 expression.15 that study identified a subpopulation of patients who had her2 negative disease by standard testing yet had her2 phosphorylation levels similar to patients with her2 - positive disease . 
the her2 activation seen in these patients in the her2 - negative subtype appeared coincident with epidermal growth factor receptor ( egfr ) activation . on the basis of the mechanism of action of neratinib as a potent her family kinase inhibitor combined with observations of i - spy 1 trial results , we postulated that her2 and egfr activation / phosphorylation may be predictive of neratinib response independent of total her2 status in the i - spy 2 trial ; this hypothesis was motivation for an exploratory analysis within the her2 - negative and triple - negative ( tn ) subpopulation . 
our analysis of her / phosphoinositide - 3 - kinase ( pi3k ) / akt signaling family components in pretreatment samples from the neratinib and concurrent control arms of the i - spy 2 trial was performed at a unique multiomic level . 
we report results from the following : ( 1 ) assessment of selected mutation / copy number alterations by exome sequencing , ( 2 ) mrna expression levels by expression microarrays , and ( 3 ) analysis of protein / phosphoprotein levels by reverse phase protein arrays ( rppas ) as specific biomarkers of neratinib response . 
rppa analysis assessed the ability of 18 protein / phosphoproteins that comprise the known drug targets of neratinib ( egfr , her2 ) and downstream effector molecules , such as shc transforming protein 1 ( shc ) and mammalian target of rapamycin ( mtor ) / ak thyoma ( akt ) signaling components to predict complete pathologic response ( pcr ) to neratinib . 
 patients randomly assigned to the experimental arm were treated with neratinib in addition to standard chemotherapy ( neratinib + t > ac ) .4 in patients with her2 - positive disease , neratinib was administered in place of trastuzumab ( appendix fig a1 )  . 
consort diagram that outlines the number of patients included in the neratinib and control arms of the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) and those included in the subsequent analyses . 
cnv , copy number variation ; rppa , reverse phase protein array . primary efficacy analysis cohort neratinib concurrent control pretreatment expression data available neratinib concurrent control ( n = 193 ) ( n = 115 ) ( n = 78 ) ( n = 193 ) ( n = 115 ) ( n = 78 ) withdrew consent for use of tissue ( n = 2 ) pretreatment samples available for additional biomarker assessment ( n = 191 ) neratinib concurrent control ( n = 115 ) ( n = 76 ) insufficient material ( n = 23 ) insufficient material ( n = 61 ) rppa data available ( n = 168 ) neratinib ( n = 106 ) concurrent control ( n = 62 ) somatic mutation and cnv data available neratinib concurrent control ( n = 168 ) ( n = 78 ) ( n = 52 ) expression by using agilent 44k expression arrays ( agendia , irvine , ca ) , signaling protein activation by rppa , and dna sequencing ( approximately 2 , 000 - gene mini - cancer genome ; utrecht , the netherlands )  . 
details of sample preparation and data processing are provided in the data supplement . in our prespecified analysis plan , 16 logistic regression was used to assess association with pcr in the control and neratinib treated populations individually . 
relative biomarker performance between arms ( biomarker - by - treatment interaction ) was assessed with a logistic model ( pcr approximately equaled treatment + biomarker + [ treatment biomarker ] )  . 
 if a continuous biomarker did not follow a normal distribution , we applied a nonparametric method that discretized the score by using a series of cut points , and we applied logistic modeling for the dichotomized biomarker at each cut point ; significance was assessed by permutation testing . 
for significant biomarkers , bayesian logistic regression analysis was performed , as previously described , with the following model : pcr hr + her2 + biomarker + treatment + ( treatment hr ) + ( treatment her2 ) + ( treatment biomarker ) .16 in additional analyses , parametric t tests ( for normally distributed data ) or nonparametric wilcoxon rank sum tests ( for non - normally distributed data ) were used to assess association of protein end points with pcr in the control and neratinib - treated populations individually . 
hr , hormone receptor ; tn , triple negative . curves were generated for end points associated with pcr in the neratinib - treated arm of the trial to identify potential cut points for biomarker positivity rates within selected patient subtypes . 16 patients with mutated pik3ca achieved pcr in the neratinib arm compared with 24 ( 39% ) of 62 patients with wild - type pik3ca . 
however , pik3ca mutation status did not show a significant biomarker - by - treatment interaction . results evaluation of her family gene point mutations and dna amplification / loss as predictors of neratinib sensitivity we evaluated somatic mutations and copy number variations ( cnvs ) in 12 her family linked signaling pathway genesegf , egfr , her2 , nrg1 , igf1r , pik3ca , akt1 , pten , stmn1 , and mtorby targeting exome sequencing across all evaluable patients . 
 consistent with publications that link pik3ca mutation with resistance to neratinib and other her2 - targeted agents , 14 , 17 - 19 only two ( 13% ) of association of her family gene expression with response to neratinib we evaluated 10 predefined her family signaling genes as expression biomarkers of neratinib response in all evaluable patients ( appendix table a1 )  . 
her2 expression was significantly associated with sensitivity to neratinib combination therapy ( and in the her2 - positive subpopulation ) , and igf1r , to resistance ; neither gene was associated with response in the control arm of the trial ( appendix tables a1 and a2 )  . 
within the her2 negative subset , stmn1 was associated with response to neratinib ( p = .0023 ) and not control , and this result showed a significant biomarker - by - treatment interaction ( p = .0036 ; fig 3a ; appendix table a3 )  . 
 2 neratinib arm : her2 control arm : her2 hr + her2 no pcr no pcr her2 subset stmn1 - low stmn1 - high unselected her2 her2 / stmn1 - high pcr probability pcr probability fig 3 . 
 ( d ) bayesian estimated pcr probability distributions in ( left ) the unselected her2 - negative subset and ( right ) the her2 - negative / stmn1 - high subset in the control ( blue ) and neratinib ( gold ) arms . of patients with her2 - negative disease ( 29 of 106 patients ) had stmn1 - high status ( fig 3b - c )  . 
by using bayesian modeling , the estimated pcr rate of patients with her2 negative / stmn1 - high status in the treatment arm was 57% compared with 17% in the control arm ( fig 3d ) ; the predictive probability of phase iii success in this subset was 97% . her family protein signaling activation as predictors of neratinib sensitivity we evaluated 18 her family signaling proteins / phosphoproteins as biomarkers of neratinib response by using rppa data from pretreatment , laser capture microdissection ( lcm ) purified tumor epithelia across all evaluable patients in the neratinib and concurrent control arms . 
six of the 18 her family biomarkers tested ( egfr y1068 , egfr y1173 , egfr y992 , her2 total , her2 y1248 , and shc y317 ) were associated with pcr in neratinib - treated patients but not in concurrent control - arm patients in the trial ( table 1 )  . 
we dichotomized patients by their egfr y1173 intensity values into high and low groups ( optimal cut point of 4 , 501 , which maximized the significance of the biomarker - by - treatment interaction term ) , and we evaluated the distribution of pcr rates ( table 2 )  . 
bold indicates p < 0.05. the predictive probability of phase iii success ( appendix table a4 )  . comparison of her family gene expression , protein , phosphoprotein , and mutation data unsupervised clustering revealed that total protein levels of her - family genes clustered with its gene expression level , whereas phosphoprotein levels were more highly correlated to one another than to their respective gene or total protein expression levels ( fig 4 )  . 
pik3ca mutations ( 28 of 130 patients ) were not associated with altered levels of pik3ca expression of protein / phosphoprotein ; however , they were associated with lower levels of stmn1 and egfr gene expression and higher levels of the phosphoproteins pten s380 and akt s473 ( data not shown )  . exploratory analysis of her family signaling in patients with tn disease although neratinib graduated in the hr negative / her2 - positive signature , this signature was characterized by ihc / f luorescence in situ hybridizationbased analysis of total her2 expression and did not measure her2 or egfr phosphorylation . 
pcr rates for egfr y1173 and her2 y1248 biomarker high / low groups by hr / her2 subtype in neratinib - treated and control groups subtype neratinib ( n = 106 ) control ( n = 62 ) egfr y1173 ( riu > 4501 cutoff ) egfr y1173 high egfr y1173 low egfr y1173 high egfr y1173 low no . 
two - way plots of egfr y1173 and her2 y1248 for neratinib treated and concurrent controls demonstrated that nine ( 82% ) of 11 patients with tn disease who exhibited elevated phospho - egfr ( pegfr ) and phospho - her2 ( pher2 ) levels experienced a pcr in response to neratinib treatment compared with four ( 36% ) of 11 with tn disease among the concurrent controls ( table 2 ; fig 5a - b )  . 
bayesian evaluation of egfr y1173 and her2 y1248 as biomarkers for neratinib response in the tn population revealed a comparable probability of success in a phase iii trial to that of the graduated hr negative / her2 - positive population ( fig 5c ; appendix tables a4 and a5 )  . 
in this pegfr / pher2 - high group of tn tumors , 16 ( 76% ) of 21 patients had erlevels greater than the median value for the tn population compared with 11 ( 37% ) of 30 patients in the rest of the tn population ( fig 5d )  . 
in the neratinib - treated population alone , 11 ( 35% ) of 31 patients had pegfr / pher2 - high status , and nine ( 82% ) of 11 patients had total er levels greater than the tn population median . discussion as precision cancer medicine evolves into concomitant processes of discovery , validation , and development of biomarkers predictive of therapeutic response alongside the clinical assessment of drug efficacy , there is increasing emphasis on identification of predictive biomarker candidates as early as possible . 
the subset of biomarkers represented include phosphoproteins associated with response to neratinib , and their associated mrna and total protein levels ( scaled to a median of 0 and standard deviation of 1 )  . 
 egfr , epidermal growth factor receptor ; erbb , erythroblastic oncogene b ; her2 , human epidermal growth factor receptor 2 ; hr , hormone receptor ; na , not available ; shc , shc transforming protein ; tn , triple negative . neratinib arm control arm treatment receptor subtype pten loss pik3ca mut egf mut her2 mut egfr total egfr mrna stmn1 mrna erbb3 total erbb3 mrna egfr y1068 egfr y1173 her2 y1248 shc y317 egfr y992 erbb3 y1289 her2 total her2 mrna no pcr no pcr treatment receptor subtype mutation status heatmap color key neratinib control hr / her2 + hr + / her2 + hr + / her2 mutated wild type 3 2 1 0 1 2 3 value proteomic / phosphoproteomic biomarkers were measured in all pretreatment biopsy samples . 
given that her2 total protein levels do not strictly correlate with her2 phosphorylation in the her2 - negative setting , 15 and given that the phosphorylation status of her2 protein ( compared with total her2 ) provides significant information on breast cancer survival , 23 - 27 we postulated that phosphorylation levels of the neratinib drug targets her2 and egfr in pretreatment biopsy specimens would correlate with pcr in both her2 - positive and her2 negative tumors . our data revealed that coactivation of her2 and egfr correlated with pcr in both her2 positive and tn tumors . 
the pcr rate in the pegfr / pher2 - high tn population , according to an optimal cut point for both markers , was 82% ( nine of 11 patients ) in the treatment arm , compared with 36% ( four of 11 patients ) with pcr in the control ar although these data are exploratory , this pcr rate was higher than the 55% of patients who had a complete response observed in the graduated hr negative / her2 - positive arm for neratinib.4 in keeping with these results , in which phosphorylated egfr levels rather than total egfr were predictive for pcr , phosphorylated egfr has been shown to be a potential predictive marker for anti - egfr therapies in other tumors , such as nonsmall - cell lung cancer.28 , 29 also , our expression analysis produced only one predictive biomarker for neratinib sensitivity , stmn1 , a gene implicated in her2 pathway signaling and chemotherapy sensitivity in non - her2 amplified cell lines.30 - 33 although our data indicate that phosphorylation levels of her2 and egfr correlate with pcr in neratinib - treated patients with breast cancer , a number of caveats in the study limit generalizability . 
the adaptive design of the trial allowed for efficient and quick graduation ( or termination ) of agent / marker combinations on the basis of their estimated likelihood of phase iii success . 
analysis of epidermal growth factor receptor ( egfr ) y1173 and human epidermal growth factor receptor 2 ( her2 ) y1248 as biomarkers for neratinib response in patients with triple - negative ( tn ) disease enrolled in the i - spy 2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 )  . 
 ( a ) and ( b ) two - way plots of egfr y1173 and her2 y1248 intensities for tn ( a ) control group and ( b ) neratinib - treated patients . 
other studies with her family inhibitors have shown that neratinib , in combination with insulin - like growth factor receptor ( igfr ) inhibitors had antiproliferative effects in her2 non - overexpressing breast cancer cell lines , and pilot clinical studies of lapatinib treatment in various metastatic cancers showed a correlation of pher2 with lapatinib response.37 , 38 what is the basis for her2 and egfr activation in the tn subpopulation ? the frequency of her2 and egfr mutations in the neratinib cohort is too small ( n = 4 and 3 , respectively ) to be a contributing factor . 
in the absence of genomic alterations related to her family signaling when her activation is seen , a logical postulate is that the process is mediated by ligand - driven events . 
recently , it has been shown that neuregulin 1 ( nrg1 or heregulin ) and her2 phosphorylation coincidentally occurred in a subset of her2 - negative tumors and that inhibition of egfr or her2 or both receptors reduced breast cancer stem cell survival and self - renewal.39 although we evaluated nrg1 in our study and did not find any correlation with pcr or her2 activation status ( table 1 ) , we did explore the possibilities of other ligand - driven events underpinning the her2 and egfr activation observed in tn tumors , namely estrogen signaling . 
estrogen can exert nongenomic activity called membrane - initiated steroid signaling through binding with er at low concentrations40 ; er may exist in a signalsome complex with a variety of receptor tyrosine kinases , such as igfr , 41 egfr , 42 , 43 or her2 , 44 , 45 and lead to activation of egfr , her2 , and igfr121 in the absence of gene transcription . 
 we found that erlevels in the tn cohort were higher in pegfr / pher2 - high tumors than in tumors that were not her2 / egfr activated ( fig 5 )  . 
this result could provide a potential explanation for the paradoxical finding of her2 / egfr activation in tn cancers in the absence of her2 genomic alterations and must be confirmed in independent study sets . the lcm - rppa workflow used in this study provides a powerful and unique approach to quantitatively measure the activated signaling architecture of a large number of cancer - related pathways , including the her family , from microscopic quantities of tissue . 
this technology and workflow is especially well suited for clinical sample assessment.46 , 47 past studies have revealed the need for lcm to accurately assess phosphorylated and total protein levels , and to facilitate biomarker evaluation in the context of high and low tumor cell content.48 moreover , unlike ihc - based approaches that can be adversely effected by choice of antigen retrieval method , the rppa technique utilizes fully denatured protein in which phospho - epitopes are fully linearized and recognized by the cognate primary antibody . patients with tn breast cancer have a paucity of targeted therapeutic options available . 
given the pcr rate observed and biomarker positive prevalence we found in the tn setting , we believe these data provide a strong molecular rationale to consider prospective validation of the findings in patients with tn disease who received neratinib . 
to our knowledge , this study is the first of its kind to quantitatively assess activated her family signaling in the context of clinical response to her - directed therapies in a tn population . 
 the biomarker findings , although prespecified , ultimately are based on small numbers of patients and must be confirmed with larger patient populations in independent clinical studies to validate fig 5 . 
wulfkuhle honoraria : dava oncology patents , royalties and other intellectual property : coinventor on filed george mason universityassigned patents related to phosphorylated her2 and egfr response predictors for her family directed therapeutics . 
gallagher no relationship to disclose lamorna brown - swigart no relationship to disclose gillian hirst no relationship to disclose laura esserman consulting or advisory role : blue cross blue shield association research funding : merck travel , accommodations , expenses : blue cross blue shield association donald berry employment : berry consultants leadership : berry consultants stock and other ownership interests : berry consultants consulting or advisory role : berry consultants travel , accommodations , expenses : berry consultants minetta liu research funding : eisai ( inst ) , seattle genetics ( inst ) , novartis ( inst ) , roche ( inst ) , genentech ( inst ) , grail ( inst ) , merck ( inst ) , janssen diagnostics ( inst ) travel , accommodations , expenses : grail , mreck , celgene , agena bioscience , menarini silicon biosystems , cynvenio biosystems john w . 
park stock and other ownership interests : merrimack consulting or advisory role : genentech ( inst ) speakers ' bureau : genentech , pfizer , agendia ( i ) lodewyk f.a. 
petricoin iii leadership : perthera , ceres nanosciences stock and other ownership interests : perthera , ceres nanosciences , avant diagnostics consulting or advisory role : perthera , ceres nanosciences , azgen , avant diagnostics research funding : ceres nanosciences ( inst ) , glaxosmithkline ( inst ) , abbvie ( inst ) , symphony evolution ( inst ) patents , royalties , other intellectual property : national institutes of health patents licensing fee distribution / royalty . 
6 - 10 , 2016 , and the annual meeting of the american society for clinical oncology , chicago , il , may 29 - june 2 , 2015 . support prior presentation references 1 . 
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loibl s , majewski i , guarneri v , et al : pik3ca mutations are associated with reduced pathological complete response rates in primary her2 - positive breast cancer : pooled analysis of 967 patients from five prospective trials investigating lapatinib and trastuzumab . 
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wang f , wang s , wang z , et al : phosphorylated egfr expression may predict outcome of egfr - tkis therapy for the advanced nsclc patients with wild - type egfr . 
saal lh , johansson p , holm k , et al : poor prognosis in carcinoma is associated with a gene expression signature of aberrant pten tumor suppressor pathway activity . 
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chakraborty a , hatzis c , digiovanna mp : co - targeting the her and igf / insulin receptor axis in breast cancer , with triple targeting with endocrine therapy for hormone - sensitive disease . 
lee cy , lin y , bratman sv , et al : neuregulin autocrine signaling promotes self - renewal of breast tumor - initiating cells by triggering her2 / her3 activation . 
arpino g , wiechmann l , osborne ck , et al : crosstalk between the estrogen receptor and the her tyrosine kinase receptor family : molecular mechanism and clinical implications for endocrine therapy resistance . 
song rx , barnes cj , zhang z , et al : the role of shc and insulin - like growth factor 1 receptor in mediating the translocation of estrogen receptor to the plasma membrane . 
pietras rj , arboleda j , reese dm , et al : her - 2 tyrosine kinase pathway targets estrogen receptor and promotes hormone - independent growth in human breast cancer cells . 
akbani r , becker kf , carragher n , et al : realizing the promise of reverse phase protein arrays for clinical , translational , and basic research : a workshop report : the rppa ( reverse phase protein array ) society . 
i - spy2 trial ( investigation of serial studies to predict your therapeutic response with imaging and molecular analysis 2 ) schema for patients in the control and experimental therapy arms . 
 molecular characterization and clinical outcomes of primary gleason pattern 5 prostate cancer after radical prostatectomy pedro isaacsson velho , md1 ; david lim , ms1 ; hao wang , phd1 ; jong chul park , md1 ; harsimar b . 
lotan , md1 purpose very high - risk prostate cancer ( pc ) is associated with poor response to local and systemic treatments ; however , few cases have been molecularly proled . 
clinicopathologic and genomic parameters were correlated with biochemical relapse , metastasis - free survival , time to castration resistance , and overall survival using cox proportional hazards models . results of patients with somatic sequencing data and clinical follow - up , 34% had dna repair gene mutations , including 22% ( 11 of 49 ) with homologous recombination and 12% ( six of 49 ) with mismatch repair gene alterations . 
these data are retrospective and hypothesis generating . conclusion potentially actionable homologous recombination and mismatch repair alterations are observed in a signicant proportion of patients with very high - risk pc at the time of radical prostatectomy . 
2019 by american society of clinical oncology introduction the national comprehensive cancer network very high - risk prostate cancer ( pc ) subset includes patients with t3b to t4 disease or more than four biopsy cores with gleason score 8 to 10 ( grade group 4 / 5 ) or those presenting with gleason score 5 + 5 = 10 or 5 + 4 = 9 ( primary gleason pattern 5 [ pg5 ] ; grade group 5 ) .1 these patients have the poorest oncologic outcomes , with higher relapse rates , frequent development of distant metastasis , poor response to systemic treatments , and short survival.2 - 4 previous studies have suggested that the proportion of gleason pattern 5 tumor on biopsy or surgical specimen denes a subset with independent prognostic implications and distinct outcomes after local and systemic treatments.5 - 8 although we have a wealth of data substantiating the poor prognosis of patients with predominant or pg5 , the molecular we know surprisingly little about alterations in these poorly differentiated tumors . among the 333 primary prostate tumors proled for the cancer genome atlas ( tcga ) , only eight patient cases ( 2% ) had pg5.9 because the prevalence of targetable alterations is relatively increased in other aggressive histologic subtypes of pc , 10 - 12 it is critically important to ll in these gaps in our molecular characterization of this disease . evolving data on metastatic castration - resistant pc ( mcrpc ) have demonstrated that druggable genomic alterations are not uncommon . 
 isaacsson velho et al context key objective we performed an integrated clinical and genomic analysis of prostate tumors with primary gleason pattern 5 at radical prostatectomy to identify potentially actionable alterations . knowledge generated in this very high - risk patient subset , adverse pathologic ndings and common molecular alterations , such as tp53 mutation , pten loss , and erg expression , were associated with poor outcomes . 
importantly , one third of patients had pathogenic mutations in dna repair genes , including in the homologous repair and mismatch repair pathways . relevance these data support the notion that aggressive subsets of primary prostate cancer are enriched for actionable genomic alterations and could inform the design of prospective clinical trials in this population . ( pd - 1 ) inhibitors.18 yet how these results in mcrpc might translate into treatment for clinically localized disease remains unclear . 
several clinical trials evaluating perioperative therapies in patients with high - risk localized including androgen - deprivation therapy ( adt ) , 19 antiandrogens , 20 and docetaxel , 21 have failed to demonstrate relevant benet . 
however , the utility of neoadjuvant and / or adjuvant parp and pd - 1 inhibitors has not yet been studied , in large part because of the relative rarity of these alterations in primary pc cohorts . here , we assembled a consecutive cohort of clinically localized prostate tumors with pg5 and long - term clinical follow - up after radical prostatectomy ( rp )  . 
to maximize duration of oncologic follow - up with the most recent pathologic specimens possible to preserve dna quality , we queried the pathology database for consecutive rps with pg5 from 2005 to 2015 and identied 60 patient cases with available tissue and clinical follow - up ( appendix fig a1 )  . immunohistochemistry tissue microarrays were constructed as previously reported.11 immunostaining for erg , pten , and p53 status was performed using previously reported and genetically validated rabbit monoclonal antibodies and staining and scoring protocols.22 - 26 punches from regions with the highest percentage of gleason pattern 5 tumor . 
dna was extracted from formalin - xed parafn - embedded material as previously described.11 next - generation tumor sequencing targeted next - generation deep sequencing to evaluate 262 cancer - related genes at a 500 average depth was performed using uw - oncoplex ( university of washington , seattle , wa ) as previously described.27 reported alterations were limited to those deemed pathogenic or likely pathogenic in the clinvar database . 
germline mutations were inferred by expert molecular pathologist review through cross - referencing against the clinvar database and by variant allele fraction in the context of tumor content , ploidy , and loss of heterozygosity status.28 , 29 two patients ( two of 49 ) did not have tumor dna available for uwoncoplex but had prior somatic sequencing performed using a clinical platform for clinical care purposes ( pgdx ; foundation medicine , cambridge , ma , and baltimore , md ) and were included in the analysis . 
patient cases in which tumor purity and / or dna quality was not high enough to exclude false - negative results are listed in the data supplement . germline sequencing altogether , 55% patient cases ( 27 of 49 ) underwent germline sequencing ( data supplement )  . 
 ( % ) a conrmatory test , 31 and metastasis - free survival ( mfs ) , dened as the time from rp to the rst detection of distant metastasis on imaging or death resulting from any cause , whichever occurred rst . 
time to castration resistance ( tcr ) , dened as the time from adt to two consecutive elevations in psa at least 4 weeks apart , and overall survival ( os ) , dened as the time from rp to death , were also assessed . 
univariable and multivariable cox proportional hazards models were used to estimate hazard ratios ( hrs ) and corresponding 95% cis and test for the association of the variables with clinical outcomes . 
because this study was hypothesis generating , we did not perform corrections for multiple comparisons . results baseline characteristics demographic , clinical , and pathologic characteristics of the pg5 cohort ( n = 60 ) at rp are listed in table 1 . 
at surgery , most patients had pathologic evidence of locally advanced disease , including nonorgan - conned ( pt3 / t4 ) tumors ( 54 [ 90% ] of 60 ) , seminal vesicle invasion ( svi ) ( 35 [ 58% ] of 60 ) , positive lymph nodes ( 16 [ 27% ] of 60 ) , and positive surgical margins ( 28 [ 47% ] of 60 )  . 
of the 37 patients who received either salvage or adjuvant radiation therapy , 27 ( 73% ) also received adjuvant adt . also , of the 16 patients who had positive lymph nodes ( pn + ) , 11 ( 69% ) received adjuvant adt . prevalence of gene mutations overall , 81.7% ( 49 of 60 ) of patients had available sequencing data on somatic genomic alterations ( data supplement ) , and 35% ( 17 of 49 ) of these had at least one pathogenic mutation in a gene involved in dna repair ( table 2 ; data supplement )  . 
overall , 55% ( 27 of 49 ) had germline sequencing results available , including six patients with presumed germline homologous recombination alterations on the basis of somatic sequencing , all of which were conrmed on germline sequencing ( brca2 , n = 3 ; brca1 , chek2 , and palb2 , n = 1 each )  . 
in addition to these alterations in homologous recombination genes , mmr deciency was found in 12% ( six of 49 ) of patients ( all in msh2 and included in our previous immunohistochemistry [ ihc ] study11 )  . other mutations common in pc were also identied ( data supplement )  . 
of 57 patients who had tumors evaluated by ihc , 51% ( 29 of 57 ) had pten protein loss . foxa1 mutations were seen in 12% ( six of 49 ) of patients , and spop mutations were seen in 8% ( four of 49 ) of patients . 
several pathologic characteristics were associated with increased risk of bcr on univariable analysis , including svi ( appendix table a1 ; appendix fig a2a ) and presence of ductal or intraductal histology ( appendix table a1 ; appendix fig a2b )  . 
multivariable models were t separately for each genomic alteration , adjusting for ductal or intraductal histology and svi ; however , none of the genomic alterations remained signicantly associated with bcr ( appendix table a2 )  . overall , 43% ( 26 of 60 ) of the cohort developed metastasis , with a median mfs of 86.4 months ( 95% ci , 40.7 months to not reached )  . 
visceral disease was seen in 31% of patients who developed metastasis , with liver ( 23% ) and lung ( 19% ) the most common sites . among clinicopathologic factors on univariable analysis , presence of svi ( table 3 ; fig 1a ) and ductal or intraductal histology ( table 3 ; fig 1b ) , along with patient age , psa , and nodal status , were both associated with increased risk of metastasis ( fig 1b )  . 
kaplan - meier analysis of metastasis - free survival in primary gleason pattern 5 cohort by ( a ) seminal vesicle invasion ( svi ) status , ( b ) ductal or intraductal ( doi ) histology status , ( c ) tp53 mutation status , and ( d ) pten protein status using immunohistochemistry . 
we chose a subset of patients with established unfavorable clinical outcomes who were diagnosed before evidence of metastatic disease and received the same initial local treatment to minimize potential biases associated with extent of disease . 
almost all patients had nonorganconned disease , more than half had svi , and a quarter had node - positive disease , demonstrating the aggressive behavior of these poorly differentiated tumors . the prevalence of genomic abnormalities in the dna repair pathway in clinically localized pg5 seems to be comparable to or perhaps even higher than that in patients with mcrpc . pritchard et al13 showed that 12% of patients with mcrpc table 5 . 
abnormalities in homologous recombination and mmr genes could have potential therapeutic implications for the treatment of all stages of pc , including the design of adjuvant and neoadjuvant trials in the pg5 population . 
in addition , our ndings have important implications for the families of patients with very high - risk disease , given that 82% of patients with homologous recombination mutations in this study had apparent underlying germline mutations . 
these ndings clearly support the recent national comprehensive cancer network guidelines , which recommend genetic testing in all patients with high - risk or very high - risk pc . our results show that there are pathologic and molecular features that are useful for risk stratication after rp . 
patients with svi or ductal or intraductal histology have more than four times greater risk of metastasis , and tp53 mutation , pten loss , and erg expression were associated with increased risk of biochemical failure and metastasis . 
notably , our study validates current clinicopathologic variables used for risk stratication and suggests that pathologic ndings after rp may be more signicant for risk prediction than molecular alterations in multivariable models . 
however , where full pathologic data are not available ( eg , in patients who do not undergo rp ) , molecular alterations could be of added value . future studies should evaluate prospectively the utility of tp53 mutation and pten loss in well - designed biomarkerdriven clinical trials cohorts , particularly in the biopsy setting . in addition , although we believe that our data are unique and informative , these results should be viewed as preliminary because of relatively the small numbers and multiplicity of clinical , pathologic , and molecular data points , which limit the power of the observations with regard to outcomes . 
it is likely that a prospective evaluation with additional numbers and follow - up time will allow for a more precise study of the prognostic signicance of clinicopathologic and molecular parameters in this group of patients . the pivotal role of adt in pc with gleason scores 9 to 10 has been called into question in recent years.8 a recent large retrospective study of patients undergoing external - beam radiation therapy in combination with adt compared outcomes of patients with gleason score 8 versus 9 to 10 , suggesting that those in the higher gleason group may derive less benet than patients with gleason score 8.8 recent studies have shown that the addition of either docetaxel21 , 32 or abiraterone33 , 34 improves os in the locally advanced or metastatic hormone - sensitive setting , with higher benet among high - risk patients , including those with high disease burden , 32 t3 to t4 disease , 21 , 34 psa greater than 40 ng / ml , 21 , 34 and gleason score 8 to 10.21 , 33 , 34 our data suggest that compared with lower - grade tumors , pg5 tumors may be less dependent on androgens and potentially more dependent on alternative oncogenic drivers , including defects in dna repair pathways . limitations of the study include the fact that it was retrospective , and clinical follow - up and dna sequencing were available only for a subset of patients , although the clinicopathologic parameters of patients with and without follow - up and sequencing were not signicantly different ( appendix fig a1 )  . 
also , the quality of the archival dna and tumor purity were not uniformly high , and false negatives at sequencing could not be excluded in all patient cases , suggesting that our results may actually underestimate the prevalence of dna repair alterations among pg5 tumors . 
 isaacsson velho et al in conclusion , we performed the rst integrated clinical and genomic analysis to our knowledge of pg5 prostate tumors at rp , a subset that has not been well represented in other sequencing efforts . 
clinical outcomes and response to conventional treatment are worse compared with lower - risk groups , and adverse pathologic ndings and common molecular alterations such as tp53 mutation , pten loss , and erg expression are associated with poor outcomes . 
the relatively high incidence of hrd and mmr deciency observed herein could inform the design of multimodal clinical trials employing parp inhibitors or pd - 1 / pd - 1 ligand monoclonal antibodies in very high - risk patients with clinically localized disease . 
contributed equally to this work . support supported by the patrick walsh research fund ; by national cancer institute ( nci ) , national institutes of health , prostate specialized program of research excellence grant no . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . travel , accommodations , expenses : astrazeneca , astellas pharma , pzer , merck serono , merck michael a . 
carducci consulting or advisory role : astellas pharma , abbvie , roche / genentech , pzer , foundation medicine research funding : bristol - myers squibb ( inst ) , pzer ( inst ) , astrazeneca ( inst ) , gilead sciences ( inst ) , emd serono ( inst ) , effector therapeutics ( inst ) samuel r . 
antonarakis honoraria : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : coinventor of biomarker technology licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation mario a . 
eisenberger leadership : veru stock and other ownership interests : veru honoraria : sano , pzer consulting or advisory role : astellas pharma , ipsen , bayer healthcare pharmaceuticals , sano , pzer research funding : sano , tokai pharmaceuticals , genentech travel , accommodations , expenses : bayer healthcare pharmaceuticals , astellas pharma , sano , pzer , veru pedro isaacsson velho honoraria : bayer healthcare pharmaceuticals speakers bureau : astrazeneca , pzer , bristol - myers squibb research funding : bristol - myers squibb , pzer ( inst ) expert testimony : bayer healthcare pharmaceuticals tamara l . 
prostate cancer 2018 : 151 epstein ji , zelefsky mj , sjoberg dd , et al : a contemporary prostate cancer grading system : a validated alternative to the gleason score . 
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clin cancer res 23 : 6863 - 6874 , 2017 isaacsson velho p , silberstein jl , markowski mc , et al : intraductal / ductal histology and lymphovascular invasion are associated with germline dna - repair gene mutations in prostate cancer . 
powell ij , tangen cm , miller gj , et al : neoadjuvant therapy before radical prostatectomy for clinical t3 / t4 carcinoma of the prostate : 5 - year followup , phase ii southwest oncology group study 9109 . 
vale cl , burdett s , rydzewska lhm , et al : addition of docetaxel or bisphosphonates to standard of care in men with localised or metastatic , hormone - sensitive prostate cancer : a systematic review and meta - analyses of aggregate data . 
tosoian jj , almutairi f , morais cl , et al : prevalence and prognostic signicance of pten loss in african - american and european - american men undergoing 23 . 
lotan tl , wei w , ludkovski o , et al : analytic validation of a clinical - grade pten immunohistochemistry assay in prostate cancer by comparison with pten radical prostatectomy . 
maughan bl , guedes lb , boucher k , et al : p53 status in the primary tumor predicts efcacy of subsequent abiraterone and enzalutamide in castration - resistant prostate cancer . 
pritchard cc , salipante sj , koehler k , et al : validation and implementation of targeted capture and sequencing for the detection of actionable mutation , copy number variation , and gene rearrangement in clinical cancer specimens . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
na r , zheng sl , han m , et al : germline mutations in atm and brca1 / 2 distinguish risk for lethal and indolent prostate cancer and are associated with early age 31 . 
cookson ms , aus g , burnett al , et al : variation in the denition of biochemical recurrence in patients treated for localized prostate cancer : the american urological association prostate guidelines for localized prostate cancer update panel report and recommendations for a standard in the reporting of surgical outcomes . 
n engl j med 377 : 352 - 360 , 2017 james nd , de bono js , spears mr , et al : abiraterone for prostate cancer not previously treated with hormone therapy . 
pathology database query for consecutive radical prostatectomies ( rps ) with primary gleason score 5 ( pg5 ) from 2005 to 2015 , where 60 patient cases were identied with available tissue and clinical follow - up . 
this model combines the expression of eight genes in primary melanoma with breslow thickness and patient age to identify patients who may forgo a sentinel lymph node biopsy ( slnb ) because of their low risk of nodal metastasis . 
cp - gep can guide physicians on slnb referrals and reduce the frequency of slnb surgeries.4 the authors of both commentaries acknowledge the need for a tool to reduce the frequency of slnb procedures . 
bartlett et al1 appreciated our approach of incorporating cp variables into our model because it ensures transparency on the added value of the gep , and they nd the comparison of cp - gep and cp models appropriate . 
the authors of both commentaries reected on the evidence that supports the utility of the cp - gep model in clinical practice and elaborated on some methodologic considerations . both commentaries rightfully emphasized the need for adequately sized external validation and additional clinical utility studies before widespread clinical adoption of cp - gep . 
we agree that extensive validation in diverse patient populations and different geographical contexts is critical . for example , we recently validated the cp - gep model in a dutch retrospective patient cohort ( n = 211 ) 5 in which patient selection , surgical procedures , and pathologic assessment of slnb are signicantly different from clinical practice in the united states . 
cp - gep achieved an slnb reduction rate ( rr ) of 41% in t1 / t2 melanoma at a negative predictive value ( npv ) of 90.7%.5 additional studies are underway to elucidate cp - gep as an slnb reduction tool . 
slnb recommendations were made on the basis of individualized considerations and within the framework of institutional practice guidelines . we , in turn , derive institutional practice guidelines from established national and international guidelines . 
moreover , in terms of net benet , the cp - gep model is consistently superior to the cp model across a range of clinically reasonable risk thresholds with a more substantial gain for higher risk thresholds . varey et al2 rightfully observe that the npv is a function of the prevalence of slnb positivity in the population and , in particular , that npv decreases as the prevalence increases . 
second , the risk of metastasis to the sentinel lymph node ( sln ) ; as reected by npv and positive predictive value ( ppv ) upon taking a test is a clinically relevant metric in the process of making a decision for or against an slnb , as indicated by national comprehensive cancer network guidelines . 
furthermore , in a previous publication by mocellin et al , 9 team members thompson and scolyer themselves recommended building predictive models for sln metastasis with the aim of maximizing the npv and reducing the rate of slnb procedures through minimizing the error rate . 
in a consensus statement on the development of gep in cutaneous melanoma , grossman et al10 recently commented that gep - based tests should add to the npv of current models while minimizing false - negative predictions . bartlett et al discuss the stratication of the results by t categories . 
after consulting with dermatopathologists at mayo clinic , we concluded that the 140 excluded patients could results stratied by t category , and we hope that our data will enable physicians to critically assess the potential of cp - gep . 
knowing model performance within each t category ( as opposed to overall performance ) is likely to gain importance because the distribution of melanoma t categories is expected to change over time with more melanomas diagnosed at earlier t categories . 
we further sought to limit variability in our data by requiring slnb to be performed within 90 days of the diagnosis of primary melanoma.3 from our point of view , combining end points such as slnb status and regional recurrence can be problematic , because they occur on different time scales and vary in their methods of detection . 
the relatively high rate of patients who develop regional recurrences after negative slnb , however , highlights the need for better , more sensitive staging tools , such as the cp - gep model . 
accordingly , and to avoid missing stage iii disease , too many patients undergo invasive and costly slnb , which highlights the need for an slnb reduction tool . varey et al2 from the melanoma institute australia ( mia ) recently published a cp nomogram to predict the risk of sln metastasis.12 the mia nomogram is based on six cp variables : patient age , breslow thickness , ulceration , histologic subtype , mitotic rate , and lymphovascular invasion . in their commentary , the authors speculate that the mia nomogram outperforms the cp - gep model . 
therefore , since the mia nomogram is available online , we sought to assess the performance of the mia nomogram in our cohort.3 we found that the mia nomogram risk score could not be calculated for approximately 19% of the patients ( 143 of 754 ) in our cohort . 
of the 143 patients excluded , 140 were not suitable for the nomogram because of histologic type , and three patients were excluded because they were younger than age 18 years at biopsy . 
shown are models based on the mia nomogram , clinicopathologic variables ( cp model ) , and cp variables and a gene expression prole ( cp - gep )  . 
 correspondence not be consistently reclassied into the ve histologic types available for the mia nomograit is likely that in clinical practice , we would encounter a similar number of patients who are difcult to classify for the mia nomograit is important to note that 16.4% ( 23 ) of the 140 excluded patients showed sln metastasis . 
more data are needed to characterize our model fully , and to this end , we are currently implementing a comprehensive validation plan . domenico bellomo , phd skylinedx , rotterdam , the netherlands alina g . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . domenico bellomo employment : skylinedx stock and other ownership interests : synlogic , skylinedx patents , royalties , other intellectual property : gene signatures for predicting metastasis of melanoma tina j . 
hieken research funding : genentech ( inst ) alexander meves research funding : skylinedx ( inst ) patents , royalties , other intellectual property : mayo clinic has led several patent applications on which i am listed as an inventor . 
mulder eeap , dwarkasing jt , hollestein d , et al : validation of a clinicopathological and gene expression prole ( cp - gep ) model for sentinel lymph node metastasis in primary cutaneous melanoma . 
bioinformatics 21 : 3755 - 3762 , 2005 steyerberg ew , harrell fe jr , borsboom gj , et al : internal validation of predictive models : efciency of some procedures for logistic regression analysis . 
mocellin s , thompson jf , pasquali s , et al : sentinel node status prediction by four statistical models : results from a large bi - institutional series ( n = 1132 )  . 
 analysis of ntrk alterations in pan - cancer adult and pediatric malignancies : implications for ntrk - targeted therapeutics purpose fusions that involve neurotrophic - tropomyosin receptor kinase ( ntrk ) genes are known drivers of oncogenesis . 
among 31 adult samples carrying ntrk fusions , co - alterations occurred often and usually involved the downstream phosphoinositide - 3 - kinase signaling pathway , cell - cycle machinery , other tyrosine kinase receptors , and mitogen - activated protein kinase signals . conclusion whereas ntrk fusions are exceedingly rare , other ntrk abnormalities affect 14% of patients with cancer . 
2018 by american society of clinical oncology introduction ntrk1 , ntrk2 , and ntrk3 genes encode the neurotrophic - tropomyosin receptor tyrosine kinases ( ntrks ) trka ( ntrk1 ) , trkb ( ntrk2 ) , and trkc ( ntrk3 )  . 
 nerve growth factor ( ngf ) binds to ntrk1 ; brain - derived neurotrophic factor ( bdnf ) and neurotrophin - 4 ( nt - 4 ) and nt - 5 bind to ntrk2 ; and nt - 3 binds both ntrk1 and ntrk3.1 binding of neurotrophic factors to their receptors activates the downstream effectors of ntrk : phospholipase c - , mitogen - activated protein kinase ( mapk ) , and phosphatidylinositol 3 - kinase ( pi3k ) / akt pathways . 
p75ntr is a positive regulator of the ngf / ntrk1 system that reduces ligand induced receptor ubiquitination and delays receptor internalization and degradation.2 ntrk receptors promote the proliferation and survival of neuronal cells3 - 8 ( fig 1 )  . 
the ligands nerve growth factor ( ngf ) , brain - derived neurotrophic factor ( bdnf ) , neurotrophin 3 ( nt - 3 ) , and nt - 4 bind to their receptors , namely ntrk1 ( tropomyosin receptor kinase a or trka ) , ntrk2 ( tropomyosin receptor kinase b or trkb ) , and ntrk3 ( tropomyosin receptor kinase c or trkc )  . 
several signaling cascades are further activatedphospholipase c ( plc - ) , mitogen - activated protein kinase ( mapk ) , and phosphoinositide - 3 - kinase ( pi3k ) and are converging to protumorigenic cell processes , such as proliferation , survival invasion , or differentiation . 
the hyperactivation of the ntrk signaling pathway induced by ntrk alterations fusions or point mutations can be overcome by the use of ntrk antagonists ( eg , ana - 12 and cyclotraxin b ) or small - molecule tyrosine kinase inhibitors ( eg , larotrectinib and entrectinib )  . 
these drive ntrk mrna and protein overexpression , which further leads to constitutive activation of downstream signaling.12 the prevalence of ntrk fusions is low , but can reach more than 80% in some rare tumors , such as mammary - analog secretory carcinoma of the salivary gland , secretory breast carcinoma , and infantile congenital fibrosarcoma.12 - 20 ntrk fusions are also found in 40% of pediatric non - brainstem high - grade glioma.21 among all alterations in ntrk genes , transcript fusions are currently the best characterized and the most pharmacologically tractable . 
nonfusion ntrk alterationsfor example , mutation or amplificationhave been associated with a lack of response with some ntrk inhibitors.22 because ntrk fusions are rare , the number of patients who can benefit from drugs that target ntrk receptors is relatively low , but the antitumor activity of such agents is remarkable.23 , 24 indeed , larotrectinib , a pan - ntrk inhibitor , demonstrated a response rate of 76% in patients with ntrk fusionpositive tumors ( 17 cancer types ) .15 , 18 tumor regression has been maintained for more than 1 year in 71% of patients . 
entrectinib , an oral pan - ntrk , ros1 , and alk inhibitor demonstrated a 79% objective response in patients with ntrk , ros1 , or alk fusions.22 in may 2017 , a new precedent was set when an immune checkpoint inhibitorpembrolizumab was approved by the us food and drug administration ( fda ) for use in a tissue - agnostic fashion on the basis of a genomic biomarker ( mismatch repair gene deficiency ) .25 ntrk - selective inhibitors represent another pharmacology class that has been developed on the sole basis of somatic molecular patterns . 
all data used in this study respected the tcgas human subjects protection and data access policies31 and the st jude cloud terms of use.32 lists of significant variants were generated using whole - genome somatic mutation data and the mutsig2cv algorithm ( org / cancer / cga / mutsig ) , taking into account the somatic background mutation rate for each gene and its neighbor genes.33 focal copy number variations that correspond to genome - wide single - nucleotide polymorphism array data were normalized and assessed at the gene level using the gistic2 protocol , 34 where a deep loss was documented by the value ( 2 ) , a single - copy loss by the value ( 1 ) , a low - level gain by the value ( + 1 ) , and an amplification by the value ( + 2 )  . 
only ntrk - related gene amplifications were kept for the analysis . sequencing - based mrna expression signals were integrated and normalized for each gene per sample using the rna - sequencing by expectation maximization protocol . 
the standard score ( z - score ) for each gene per sample was calculated using the mean values and standard deviation found in all similar tumors same tumor typethat are diploid for the said gene . 
in adults , co - alterations within signaling cascades , such as tp53 , mapk , pi3k , tyrosine kinase receptor , or cell - cycle signaling pathways , were curated from tcga . 
all nonsynonymous missense , nonsense , nonstop , deletion / insertions , frameshift , or splicing site mutations within the genes of interest , as well as deep losses or amplifications and mrna under or overexpressions , were kept for analysis . results prevalence of ntrk fusions in tcga ( adult ) and st jude pecan ( pediatric ) databases fusion frequency in adults of the 9 , 966 adult tumor samples in the tcga database , 0.31% ( n = 31 samples ) presented an ntrk fusion . 
 ( there were 5 , 023 patient samples with these 22 ntrk fusion negative tumor types [ samples per tumor type = 36 to 541 ]  . ) ntrk3 fusions were the most common ( n = 16 ) , followed by ntrk1 ( n = 9 ) and ntrk2 ( n = 6 ) fusions in adults ( table 1 )  . fusion frequency in children of the 3 , 501 pediatric tumor samples ( st jude pecan database ) , 0.34% ( n = 12 ) presented an ntrk fusion . 
frequency of ntrk receptor transcript fusions in tcga ( n = 9 , 966 adult tumor samples ) and st jude pediatric cancer database ( n = 3 , 501 pediatric tumor samples ) , and specific tumors with high incidence of ntrk fusions in the literature no . 
sixteen molecules are currently being evaluated in clinical trials , with the most advanced being larotrectinib ( loxo oncology , stamford , ct ; ic50 for ntrk1 , ntrk2 , and ntrk3 fusions ranging from 4 to 9 nm )  . 
the new drug application was submitted to the fda in december 2017 and granted priority review status on the basis of remarkable clinical activity23 ( table 2 )  . types of ntrk - related alterations in adult and pediatric tumors and sensitivity to ntrk inhibitors to understand the potential benefits of selective ntrk inhibitors for the treatment of adult and pediatric patients with cancer , we first aimed to describe the prevalence and type of ntrk activating pathway alterations , including point mutations , gene copy number amplifications , and mrna overexpression of ntrk receptors , co - receptor , and ligands , within a large cohort of pan - cancer samples ( figs 1 and 2 )  . 
the number of samples with comprehensive data for this analysis was 11 , 621 ( 9 , 966 adults and 1 , 655 children )  . alterations in ntrk receptors and ligands genomic and / or transcriptomic ntrk receptor alterations were found in 14.2% ( 1 , 648 of 11 , 621 ) of samples , with gene amplification and mrna overexpression being the most frequent alterations . 
transcript fusions were observed in ntrk receptor genes only , with the exception of two samples that presented one transcript fusion of bdnf ligand and one transcript fusion of p75ntr ( positive regulator of the ngf / ntrk1 machinery ; fig 2 )  . - transcript fusion types ntrk - transcript fusions that were observed in the pan - cancer cohort and / or described in the literature are listed in table 3 . 
this variant is a known biomarker of sensitivity to larotrectinib and entrectinib.71 , 72 variants tpm3ntrk1 ( 0.04% ) , irf2bp2 - ntrk1 ( < 0.01% ) , and sqstm1 - ntrk1 ( < 0.01% ) are also sensitive to larotrectinib ; however , the sensitivity of the remaining 22 unique variants observed in the pan - cancer cohort is not currently known . 
nine rearrangements previously described in the literature were not found in the tcga and st jude pecan databases ( table 3 )  . point mutations several point mutations are acquired resistant variants to first - generation ntrk inhibitors ( larotrectinib or entrectinib ) , but not to loxo - 195 , specifically designed to overcome secondary resistance . 
these variants , namely ntrk1 g595r , ntrk1 g667c , ntrk3 g696a , and ntrk3 g623r , were not observed in any of the 13 , 467 combined adult and pediatric tumors reviewed ( treatment - nave samples ; table 3 )  . co - alterations observed in ntrk fusionpositive adult tumor samples among 31 adult tumors presenting ntrk fusions , 61.3% ( 19 of 31 ) harbored one or more co alteration that activated the downstream pi3k signaling pathway ; 58.1% ( 18 of 31 ) harbored one or more co - alteration within cell - cycleassociated genes ; 58.1% ( 18 of 31 ) harbored one or more co - alteration within other tyrosine kinase receptors ; 32.2% ( 10 of 31 ) harbored one or more co - alteration within the mapk signaling pathway ; and 35.5% ( 11 of 31 ) harbored one or more co - alteration within tp53 - associated genes . 
 nf2 - activating mutations were associated with ntrk fusions in 42% ( 13 of 31 ) of samples , and tp53 ( 10 of 31 ) , rb1 ( six of 31 ) and cdkn2a ( five of 31 ) occurred in more than 15% of the ntrk fusionpositive samples ( fig 3 and appendix table a1 )  . 
 ( adequate data to comprehensively assess co - alteration data in children was not available . ) samples bearing ntrk fusions were significantly associated with ntrk mrna overexpression compared with samples without the fusion ( appendix fig a1 )  . 
distribution of molecular alterations leading to the hyperactivation of the neurotrophic - tropomyosin receptor tyrosine kinase ( ntrk ) signaling pathway in human tumors ( n = 11 , 621 samples with comprehensive molecular data )  . 
all samples that presented a nonsilent mutation , gene copy amplification , gene fusion , or mrna overexpression of ntrk receptors ( ntrk1 , ntrk2 , and ntrk3 ) , co - receptor ( p75ntr ) , or ligands ( nerve growth factor [ ngf ] , brain - derived neurotrophic factor [ bdnf ] , neurotrophin 3 [ nt - 3 ] , and nt - 4 ) were retrieved from a large adult and pediatric pan - cancer cohort ( the cancer genome atlas and st judes pecan databases ; n = 11 , 621samples )  . 
among the ntrk fusion cases ( n = 31 from tcga cohort ) , four cases had concomitant alteration within the genes that code the ntrk pathway membersligands , co - receptor , and receptorsas follows : low - grade glioma , ntrk3 fusion plus ntf3 amplification ( n = 1 ) ; low - grade glioma , ntrk1 fusion plus ntrk1 amplification ( n = 1 ) ; glioblastoma , ntrk1 fusion plus ntrk1 amplification ( n = 1 ) ; head and neck squamous cell carcinoma , ntrk3 fusion plus ntrk3 amplification ( n = 1 )  . we reviewed data from 13 , 467 tumor samples in the tcga ( adult tumors ) and st jude pecan ( pediatric tumors ) databases and found ntrk fusions in 0.3% of pan - cancer tumors ( table 1 )  . 
 although the prevalence of these alterations is low , ntrk fusions are more often found in specific and rare tumors , such as mammary - analog secretory carcinoma of the salivary gland ( 93% to 100% of tumors presenting an etv6 - ntrk3 fusion ) , secretory breast carcinoma ( etv6ntrk3 fusions in 92% of tumors ) , infantile congenital fibrosarcoma ( etv6 - ntrk3 fusions in 86% to 91% of tumors ) , and pediatric non brainstem high - grade glioma14 - 21 ( 40% of tumors presenting an ntrk fusion ; table 1 )  . of importance , various ntrk inhibitors are in clinical development and have differential activities ( table 2 )  . 
drugs with established clinical trial data and the ability to affect ntrk1 , ntrk2 , and ntrk3 fusions at low ic50 include , but are not limited to , larotrectinib ( 76% response rate in diverse malignancies bearing ntrk fusions ) and entrectinib , which also affects alk and ros1 rearrangements ( 79% response rate ) , and some of these responses are durable and occur with remarkable speed22 , 23 ( table 2 )  . 
furthermore , five of these small inhibitors are already approved by the fda for other indications : cabozantinib ( ic50 against ntrk2 , 7 nm ) , crizotinib ( ic50 against ntrk1 and ntrk2 , 1 nm ) , midostaurin ( ic50 against ntrk1 , - 2 , and - 3 ranging from 11 to 51 nm ) , nintedanib ( ic50 against ntrk1 , - 2 , amd - 3 ranging from 17 to 264 nm ) , and regorafenib ( ic50 against ntrk1 , 74 nm )  . 
 ntrk mutations that are associated with larotrectinib or entrectinib resistance include ntrk1 f589l g595r , g667c , g667s , v573m , and ntrk3 g696a , g623r ( table 3 )  . 
 ( these mutations were not detected in tcga , likely because these patients had not been previously treated with ntrk inhibitors . ) the resistant alterations are targetable with loxo - 195 , a next - generation , selective ntrk inhibitor with promising preliminary clinical activity50 ( fig 2 )  . 
in the current study , ntrk - associated co - alterations were commonly discerned in genes that are involved in pi3k signaling ( 61% of patient samples ) , tyrosine kinase families ( 58% of patient samples ) , cell - cycle machinery ( 58% of patient samples ) , and mapk pathways ( 32% of patient samples ; fig 3 and appendix table a1 )  . 
frequencies of alterations were computed using a large adult and pediatric pan - cancer cohort ( the cancer genome atlas and st judes pecan databases ; n = 13 , 467 samples )  . 
sensitivity and resistance criteria presented in this table correspond to objective clinical responses or nonresponses observed in fusion - positive or mutation - positive patients who received the drug . abbreviations : na , not available ; ntrk , neurotrophic - tropomyosin receptor tyrosine kinase . drilon et al , 50 wei et al77 drilon et al , 50 hyman et al , 71 russo et al78 drilon et al , 50 russo et al78 drilon et al , 50 wei et al77 drilon et al , 50 wei et al77 drilon et al50 drilon et al , 50 , 79 hyman et al71 fusions were significantly associated with ntrk mrna overexpression ( appendix fig a1 ) , which is consistent with a previous report.101 of interest , in the adult cohort , ntrk fusionpositive samples were significantly associated with a lower mutational burden compared with fusion - negative tumors ( p < .001 ; appendix fig a2 )  . 
this observation echoes a previous report that demonstrated that tumors harboring a driver fusion tend to have a lower number of point mutations.101 in contrast , high microsatellite unstable metastatic colorectal tumors have been shown to preferentially bear alk , ros1 , or nrtk fusions.102 in our cohort , three ntrk fusionpositive colon cancer samples were observed and two of them presented with microsatellite instability - high status ( data not shown )  . 
finally , we found that nonfusion ntrk gene alterations , such as mutation , amplification , and mrna overexpression , were found in approximately 14% of pan - cancer samples ( fig 2 )  . 
all samples that presented a gene fusion of ntrk receptorsntrk1 , ntrk2 , and ntrk3were retrieved from a large adult pan cancer cohort ( the cancer genome atlas database ; n = 9 , 966 samples )  . 
despite these limitations , the current report provides a comprehensive portrait of the genomic landscape of ntrk alterations among pan - cancer tumors using large databases . in conclusion , ntrk fusions were observed in 0.31% ( 31 of 9 , 966 ) of adult tumors and 0.34% ( 12 of 3 , 501 ) of pediatric cancers , mostly in ntrk3 ( 0.16% of adult tumors ) and ntrk1 ( 0.14% of pediatric tumors ) ; however , some tumor types had more frequent ntrk fusions ( table 1 )  . 
genomic co alterations were commonly observed in ntrk fusionpositive cancers , including in genes involved in pi3k signaling , tyrosine kinase families , cell - cycleassociated regulators , and the mapk pathway ( fig 3 )  . 
furthermore , it would be of interest to determine whether the salutary effects of ntrk inhibitors in patients who harbor cancers with ntrk fusions can be extended via rational compound design to any of the more common ntrk alterations , such as mutation , amplification , and overexpression . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . ryosuke okamura no relationship to disclose amlie boichard no relationship to disclose jason k . 
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drilon a , li g , dogan s , et al : what hides behind the masc : clinical response and acquired resistance to entrectinib after etv6 - ntrk3 identification in a mammary analogue secretory carcinoma ( masc )  . 
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 predictive biomarkers in metastatic colorectal cancer : a systematic review juan ruiz - baobre , md1 , 2 , 3 ; raju kandimalla , phd2 ; and ajay goel , phd2 purpose the development and use of predictive biomarkers to guide treatment decisions are paramount not only for improving survival in patients with metastatic colorectal cancer ( mcrc ) , but also for sparing them from unnecessary toxicity and reducing the economic burden of expensive treatments . 
we conducted a systematic review of published studies and evaluated the predictive biomarker landscape in the mcrc setting from a molecular and clinical viewpoint . methods studies analyzing predictive biomarkers for approved therapies in patients with mcrc were identied systematically using electronic databases . 
of all the biomarkers analyzed , 1.4% ( two of 148 ) were explored in a prospective manner , whereas 98.6% ( 146 of 148 ) were evaluated in retrospective studies . 
of the latter group , 78.8% ( 115 of 146 ) were not tested in subsequent phases , 9.6% ( 14 of 146 ) were tested in other retrospective cohorts , 8.9% ( 13 of 146 ) were retrospectively tested in at least one or more randomized cohorts , and only 2.7% ( four of 146 ) were prospectively tested in a clinical trial . 
2019 by american society of clinical oncology introduction colorectal cancer ( crc ) remains the third leading cause of cancer - related deaths in the western world . despite ongoing efforts aimed at increased population screening and improved early detection strategies , approximately 20% of patients still present with metastatic disease at diagnosis , and approximately 35% of those who undergo curative surgeries for a localized disease relpase.1 during the past three decades , the median overall survival ( os ) of patients with metastatic crc ( mcrc ) has gradually increased because of the implementation of combined chemotherapy regimens as well as targeted molecular therapies against egfr and angiogenic factors.2 since the identication of ras mutations as a negative predictive marker , antiegfr therapy has had the greatest impact on the management of patients with mcrc ; nonetheless , the response rates of these treatments remain only approximately 40% to 60% . 
in addition , the recognition landscape for immunotherapy in the treatment patients with microsatellite instability - high ( msi - h ) or dna decient mismatch - repair ( dmmr ) mcrc has been encouraging for this subset of patients . 
crc , colorectal cancer ; mcrc , metastatic colorectal cancer ; neoadjuvant - crt , neoadjuvant chemoradiotherapy . 2 2019 by american society of clinical oncology conventional chemotherapy and triuridine / tipiracil the backbone of treatment in patients with mcrc has historically been chemotherapy , and several chemotherapeutic agents are now approved in this setting : uoropyrimidines ( uorouracil [ fu ] and capecitabine ) , oxaliplatin , irinotecan , and since 2015 , triuridine / tipiracil ( tas - 102 )  . fluoropyrimidine - based chemotherapy and tas - 102 . 
studies of the role of thymidylate synthase ( ts ) in uoropyrimidine - based therapy ( primarily fu plus leucovorin ) in various retrospective and prospective studies have yielded discordant results . 
in this regard , multiple studies have shown that low levels of ts expression in metastatic tumor tissues generally correlate with higher overall response rate ( orr ) .3 - 6 surprisingly , such a correlation was not evident when ts levels were measured in primary tumor tissues.4 , 7 similarly , low levels of ts and dihydropyrimidine dehydrogenase in metastatic tumor tissues were associated with a favorable response to fu in patients with mcrc8 ; however , a subsequent report in 2006 did not validate these ndings.9 likewise , the role of thymidine phosphorylase as a predictive biomarker was also investigated , but the results remain inconclusive.10 , 11 in 2009 , a meta - analysis of ve studies examining a total of 861 patients with mcrc concluded that compared with microsatellite - stable patients , msi - h patients did not achieve a statistically signicant better response rate to fu - based chemotherapy.12 similarly , while investigating the relationship between msh2 gene expression and capecitabine efcacy in patients with mcrc , jensen et al13 observed that a higher msh2 expression was associated with a better response . 
in 2015 , hamauchi et al30 found that patients who develop grade 3 or 4 neutropenia during the rst cycle of tas - 102 treatment had a smaller risk of disease progression . 
selected biomarkers the nal analysis . distribution of biomarkers by individual treatment group . ( b ) distribution of biomarkers by study design . antipd - 1 , antiprogrammed cell death - 1 drugs ; fu , uoropyrimidine - based chemotherapy ; irinotecan , irinotecan - based chemotherapy ; msi , microsatellite instability ; oxaliplatin , oxaliplatin - based chemotherapy ; tas - 102 , triuridine / tipiracil . 
 ( * ) predictive biomarker for anti - egfr drugs ( cetuximab / panitumumab ) ; ( ) predictive biomarker for antipd - 1 drugs ( pembrolizumab and nivolumab alone or in combination with ipilimumab )  . testing in 1 randomized cohorts ( n = 13 ; 8.9% ) ras mutations * testing in a clinical trial ( n = 4 ; 2.7% ) msi status oxaliplatin - based chemotherapy . 
the most notable attempts in this regard have been for the ercc1 gene , and as reported from the mavericc ( marker evaluation for avastin research in crc ) trial , intratumoral ercc1 gene expression failed to predict response to oxaliplatin treatment.17 another gene evaluated in this setting was the x - ray repair cross - complementing group 1 ( xrcc1 ) gene , a base excision repair modulator , wherein a polymorphism in this gene ( xrcc1 - 839 arg / gln or gln / gln ) correlated with worse orr to fu / oxaliplatin.18 interestingly , several micrornas ( mirnas ) have been explored for their predictive response potential to fu , leucovorin , and oxaliplatin ( folfox ) or capecitabine plus oxaliplatin ( capeox ) based regimens . 
using a proteomic approach in 2010 , aoyagi et al32 reported that lower levels of plasma soluble vascular endothelial growth factor ( vegf ) receptor 1 were associated with improved disease control in a subset of 46 patients treated with modied fu , leucovorin , and oxaliplatin ( mfolfox6 ) plus bevacizumab . 
in the same year , another study identied a signicant correlation between low angiopoetin - 2 serum levels and better survival outcomes in a cohort of patients with mcrc treated with bevacizumab - based therapy.33 conversely , the correlation between vegf - a levels and the clinical benet of bevacizumab - based chemotherapy is still under evaluation . 
perhaps in the near future , mavericc trial results will offer more insights into the usefulness of plasma vegf - a levels in this setting.17 with regard to the predictive role of ras , in a subset of 230 patients with mcrc treated in a phase iii randomized clinical trial with either irinotecan , fu , and leucovorin ( ifl ) plus placebo , or ifl plus bevacizumab , only the wild - type kras subset of patients obtained a signicantly higher response rate in the bevacizumab arm.35 in addition to the molecular markers listed previously , a few clinical factors have been studied in relation to bevacizumab response . 
two retrospective studies based on the data from the correct ( patients with metastatic colorectal cancer treated with regorafenib or placebo after failure of standard therapy ) and consigna ( regorafenib in subjects with metastatic colorectal cancer who have progressed after standard therapy ) trials have evaluated the usefulness of different computed tomography scan based parameters in predicting the clinical benet of regorafenib therapy . 
one of the rst studies , in 2016 , reported a correlation between improved pfs and lung metastases cavitation before therapy initiation and even at week 8.38 in this study , baseline lung metastases cavitation and changes in the sum of target lesion diameters were deemed to be predictors for improved os in the multivariate analysis . 
a year later , the correct trial also demonstrated a signicant association between survival ( pfs and os ) and several radiologic parameters such as response or stable disease in size and density of lung metastases.39 likewise , highlighting the use of dynamic contrast - enhanced magnetic resonance imaging , a recent study reported that a  . 
these and other potential predictive biomarkers for anti - egfr therapy are summarized in table 3 and in the data supplement . antiprogrammed cell death - 1 drugs : pembrolizumab and nivolumab in may and july of 2017 , the us food and drug administration approved pembrolizumab and nivolumab for the treatment of patients with msi - h mcrc in whom the disease has progressed after treatment with uoropyrimidine , oxaliplatin , and irinotecan therapies . 
almost a year later , in july 2018 , a nivolumab plus ipilimumab combined regimen was approved , which opened up three novel treatment options for patients with msi - h or dmmr mcrc , who represent approximately 5% of all patients with mcrc.23 the belief is that , despite their worse prognosis , a large prolymphocytic inltration and the presence of portion of mutation - associated neoantigens61 confer to patients with msi - positive mcrc the clinical benet they derive from antiprogrammed cell death - 1 ( pd - 1 ) therapy.62 - 65 this exciting discovery has now led to universal msi testing for the management of patients with mcrc . disease monitoring by liquid biopsies recently , liquid biopsies have emerged as powerful tools for monitoring disease evolution and therapeutic response through the analysis of cell - free dna and rna biomarkers in bodily uids . 
one of the rst studies , in 1979 , which reported that a gradual decrease in carcinoembryonic antigen ( cea ) levels during chemotherapy was signicantly associated with better survival rates , was the basis for this concept.66 such a correlation between cea are and improved pfs and os was conrmed a few years later in a subset of 670 patients with mcrc undergoing rst - line chemotherapy.67 although cea is not a crc - specic biomarker , cea monitoring in blood , alone or in addition to ca 19 - 9 , 68 is still performed commonly in routine clinical practice . 
in this context , the accuracy of cea change in predicting disease progression has been demonstrated recently in a study involving 2 , 828 patients from seven rstline clinical trials.69 in addition to this , other analyses of circulating tumor cells70 and endothelial cells71 in mcrc have been undertaken by several groups . 
in 2015 , hansen et al72 reported that circulating levels of mirna - 126 in a subset of 68 patients with mcrc were predictive of tumor response to bevacizumab - based chemotherapy . 
since then , multiple studies have reported distinct genetic alterations in ctdna from patients with primary disease or acquired resistance to antiegfrbased therapies in genes such as kras , nras , met , erbb2 , flt3 , egfr , and map2k1 by droplet digital polymerase chain reaction , beaming , and next - generation sequencing methodologies.74 , 75 using a massively parallel sequencing - based assay in a prospective cohort of 53 patients with mcrc , it was shown that early changes in ctdna during rst - line standard chemotherapy can also predict subsequent radiologic response.76 similarly , 2017 , a study demonstrated a signicant correlation between the decrease in ras mutant clones in blood after 8 weeks of therapy and improved pfs and os in a cohort of patients treated with regorafenib.40 intriguingly , clonal evolution is a dynamic process , yet the emergence of drugresistant clones in circulation increases during treatment , whereas drug withdrawal results in a decrease of such clones . 
the understanding of this fact has paved a path for novel treatment strategies that are already under evaluation as part of the rasintro ( ras mutations in ctdna and anti - egfr reintroduction in mcrc ) study ( clinicaltrials . gov identier : nct03259009 ) and the chronos ( rechallenge with panitumumab driven by ras dynamic of resistance ) trial ( clinicaltrials.gov identier : nct03227926 ) , which are evaluating the predictive impact of ctdna ras mutations on the efcacy of anti - egfr monotherapy rechallenge in patients with ras wild - type mcrc whose disease has progressed after anti - egfrfree chemotherapy . 
in addition , a ve - gene methylation panel for monitoring tumor burden in liquid biopsies using a methylbeaming assay was described recently77 in 182 patients with mcrc treated with chemotherapy and / or targeted therapy , in which the authors discovered a signicant correlation between the dynamics of methylation markers and orr and pfs . discussion despite the tremendous body of effort devoted to the identication of predictive biomarkers for various treatments used in patients with mcrc , thus far only two of such markers have been translated into routine clinical practice . the rst one , the mutations in the ras gene , serves as a negative predictive biomarker that is present in approximately 55% of patients with mcrc78 and correlates with the lack of efcacy of anti - egfr antibody treatments . 
the exciting result of the association between msi - h and response to nivolumab in the rst - in - human clinical trial ( clinicaltrials . gov identier : nct00441337 ) led to two subsequent phase ii clinical trials , which were instrumental in the approval of antipd - 1 drugs ( pembrolizumab or nivolumab ) alone or in combination with ipilimumab ( nivolumab plus ipilimumab ) as a treatment option for patients with msi - h or dmmr mcrc.63 - 65 , 79 other well - described predictive biomarkers used in the management of several tumor types have shown promising usefulness in selecting patients with mcrc for various targeted therapy - based regimens . 
results from two clinical trials in patients with braf v600epositive mcrc have highlighted this mutation as a predictive biomarker for braf inhibitorbased regimens ( data supplement ) .80 , 81 regarding the role of human epidermal growth factor receptor 2 ( her2 ) amplication or overexpression as a predictive biomarker results of two phase ii clinical trials evaluating the dual her2 blockade in a biomarker - selected subset of heavily pretreated patients with mcrc , with either trastuzumab plus lapatinib ( heracles [ her2 amplication for colorectal cancer enhanced stratication ] trial ) or with pertuzumab and trastuzumab ( mypathway trial ) , demonstrate an impressive orr of approximately 30% to 40% ( data supplement ) .82 , 83 for anti - her2based therapies , nonetheless , the discovery and validation of novel predictive biomarkers that can assist in decision making has been a challenging endeavor , resulting in a long list of failed predictive markers . 
in crc , because the use of single - agent chemotherapeutic regimens has shown limited efcacy , and the majority of current treatment options include various combinations of drugs , biomarker discovery for specic drugs is more complicated , not surprisingly , because of the interactions among different cytotoxic agents.84 similar concerns remain regarding developing predictive biomarkers for therapeutic response to bevacizumab , because ( 1 ) it is also not used as a single agent in the clinic , 84 ( 2 ) its mechanisms of action are poorly understood , 85 and ( 3 ) angiogenesis is an intriguingly adaptive process that involves numerous factors.86 presumably , the inherent complexity of angiogenesis has been a substantial hurdle in the attempts to develop responsepredictive biomarkers for other multitargeted antiangiogenic drugs such as aibercept or regorafenib . 
 predictive biomarkers in metastatic colorectal cancer a possible source of discrepancy even when the molecular marker is analyzed in a different region of the same source.88 besides their spatial heterogeneity , tumors are dynamic entities that continue to evolve over time , especially if they are under selective pressure.89 for this reason , the time from sample acquisition to biomarker analysis is of clinical relevance ; however , overlooked in most studies . 
because only approximately 20% of patients with crc present with metastatic disease at the time of diagnosis , it is often the practice or only option available to analyze archival tissues from the primary tumor to identify biomarkers , which is not always optimal.90 this is an issue that patient selection is gaining importance , which is evidenced by the recent initiative , the us national cancer institutes exceptional responder program.91 consideration of extreme phenotypes such as long - term responders and extremely early progressors for biomarker discovery can facilitate successful identication of molecular alterations that better correlate with clinical phenotypes . 
for instance , in the majority of studies presented in this article , there was no consideration of pfs as a selection criterion , and many studies included in the nonresponders patients with stable disease . 
in general , improved orr and longer pfs are superior indicators of the true efcacy of any drug intervention , whereas inclusion of gain in os as a selection feature may inadvertently introduce bias . 
in addition , new biomarker - driven study designs such as basket or umbrella trials , which assign a treatment according to tumor molecular characteristics , not only are going to improve clinical drug development , but also will facilitate improved biomarker validation . 
besides the examples already described previously in the text , new drugs that target tyrosine kinase fusions in genes such as nrtk1 / 2 / 3 , ret , alk , and ros1 are emerging with promising preliminary results in phase i and ii clinical trials that include patients with crc ( data supplement ) .92 - 97 although analysis of clinical specimens with robust followup data from retrospective series or randomized trials are of tremendous value , subsequent prospective clinical cohorts using longitudinally collected specimens are much needed to establish clinically translatable predictive biomarkers . 
in addition , although many surgical specimens are of suitable quality , needle biopsyderived metastatic lesions often yield lower amounts of dna and rna than that required for robust sequencing experiments98 , 99 ; having access to liquid biopsybased predictive markers would be transformative in overcoming this limitation in patients with mcrc . 
furthermore , liquid biopsy biomarkers will improve patient compliance and eliminate the concerns surrounding intratumor heterogeneity associated with tumor or biopsy specimens and may also help in disease monitoring as well as in predicting secondary resistance . the international community has to consolidate initiatives to improve biomarker development studies and , more importantly , undertake conscious efforts to validate the results gathered from retrospective studies in prospective randomized multicenter cohorts . 
last , the implementation of novel high - throughput molecular analytic techniques and the integration of multiomic approaches with clinical and epidemiologic data using machine - learning algorithms will denitely hasten biomarker development in the coming years.100 despite many attempts over the past decades , there remain only two well - established predictive biomarkers , mutations in the ras gene and msi status , that currently guide treatment decisions in patients with mcrc . 
 ruiz - baobre , kandimalla , and goel juan ruiz - baobre travel , accommodations , expenses : bristol - myers squibb , merck sharp & dohme , ipsen , pharmamar no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
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 erbb3 - activating mutations in small bowel adenocarcinomas purpose functional studies have demonstrated that some mutations of erbb3 , which encodes for human epidermal growth factor receptor ( her ) 3 , are oncogenic via activation of the erbb family signaling pathway . 
this study was designed to report the rate of activating erbb3 mutations in small bowel adenocarcinoma ( sba ) , a rare tumor type in which we previously reported a high rate ( 12% ) of erbb2 - activating mutations . materials and methods dna from 74 sbas , previously characterized for erbb2 mutations and mismatch repair status , was submitted for sequencing of erbb3 exons 3 , 6 , 7 , 8 , and 23 . 
mutant allelic frequencies suggested that both mutations were shared by the same clone rather than being harbored by mutually exclusive tumor subclones . conclusion sbas display a high rate of erbb3 - activating mutations , which have been shown to be targetable by anti - her2 therapies . 
2018 by american society of clinical oncology human epidermal growth factor receptor ( her ) 3 is a tyrosine kinase transmembrane receptor and a member of the her receptor family , which consists of four members : epidermal growth factor receptor ( egfr ) , her2 , her3 , and her4 , which are encoded by the egfr , erbb2 , erbb3 , and erbb4 genes , respectively . 
 unlike other members of this family , her3 has an impaired intracellular kinase domain1 and must heterodimerize with egfr , her2 , or her4 to initiate an intracellular signal , which activates downstream survival signaling such as the phosphoinositide 3 - kinase ( pik3ca ) pathway.2 in 2013 , a first report established that erbb3 displays recurrent hotspot mutations in several cancers , especially in colorectal , gastric , 3 and lobular breast cancer4 ; the most frequent amino acid change ( p.v104m / l ) is related to a single nucleotide variation hotspot located in exon 3 . 
sba is usually treated the same way as colorectal cancer , but few studies have been devoted to this cancer type.8 a first report from our team addressing the specific genomic landscape of sba was published by laforest et al , 9 in which 83 sba samples were subjected to targeted panel sequencing ( 46 genes , ion ampliseq cancer hotspot panel v2 )  . 
this study , which was performed before the discovery of erbb3 activating mutations , reported eight genes that were mutated in more than 5% of sba cases : kras , tp53 , apc , smad4 , pik3ca , erbb2 , braf , and fbxw7 . 
errb2 alterations were highly prevalent : 10 tumors ( 12% ) presented either erbb2 - activating point mutations ( n = 7 ) or erbb2 amplifications ( n = 3 )  . 
2 ethics committee under id - rcb number 2008a01058 - 47 . sample preparation tumor samples were collected as described elsewhere.9 briefly , using a 1.0 - mm punch , paraffin - embedded tissues from all cases were sampled from representative areas containing more than 50% of tumor cells . 
sequencing products were purified with sephadex gel ( ge healthcare , vlizy villacoublay , france ) before running them on a 3500 genetic analyzer ( applied biosystems , foster city , ca )  . 
sequencing data were visualized using finch tv ( geospiza , seattle , wa ) with a detection sensitivity of 10% mutated cells . next - generation sequencing ( ngs ) targeted ngs ( a panel of 39 genes ) was performed on samples with co - occurrence of erbb2 and erbb3 . 
of patients ( % ) 74 ( 100 ) median age in years , range 62 years , 32 - 98 male female tumor stage ( tnm classification ) primary tumor site duodenum jejunum ileum dmmr status msi - h histologic grading 40 ( 54 ) 34 ( 46 ) 1 ( 1 ) 25 ( 34 ) 27 ( 37 ) 19 ( 25 ) 2 ( 3 ) 36 ( 49 ) 26 ( 35 ) 12 ( 16 ) 17 ( 23 ) 57 ( 77 ) 20 ( 27 ) 23 ( 31 ) 30 ( 41 ) 1 ( 1 ) abbreviations : dmmr , mismatch repairdeficient ; msi , microsatellite instability ; mss , microsatellite stable ; na , not available raw reads were aligned on the reference human genome hg19 using the tmap aligner v0.3.7 ( life technologies )  . 
only studies with more than 100 patients and an erbb2 / erbb3 mutation rate higher than 5% ( including putative driver or passenger mutations and at least one erbb3 driver mutation ) were taken into account , with the exception of the mutation rate in the genie cohort . 
after combining erbb3 data with the previous genotyping data , a significant correlation was observed with erbb2 mutation three of the four erbb3 - mutated sba samples also displayed an erbb2 - activating mutation . 
 because the activation of two oncogenes in the same pathway is unusual , this finding was validated by subjecting two samples with sufficient dna to another ngs assay targeting both erbb2 and erbb3 to investigate whether these mutations were restricted to tumor subclones . 
in addition to confirming that erbb2 and erbb3 mutations co - occurred in the same tumor , mafs suggested a clonal distribution , ie , that both mutations were indeed harbored by the same tumor cells . erbb3 mutations , mismatch repair ( mmr ) status , and erbb2 mutations in other tumor types we investigated whether the correlation among erbb3 - activating mutations , erbb2 mutations , and msi - h status was also observed in other tumor types by performing in silico analysis of publicly available data . 
 ( * ) p < .01 between msi - h and microsatellite stable ( mss ) cancers . in 1% to 3% of the following cancer types : lobular breast , gastric , colorectal , endometrial , and cervix adenocarcinoma , together with cholangiocarcinoma and bladder cancer.3 , 4 , 11 - 18 this spectrum of erbb3 - mutated cancers overlaps with that of erbb2 - mutated and erbb2 amplified cancers , supporting the biologic concept of her2 - driven cancer because erbb3 activating mutations act via her2 signaling . 
 because sba is the most common form of erbb2 - mutated cancer ( as initially reported by laforest et al9 ) , we hypothesized that erbb3 sequencing would detect a high rate of erbb3 mutations . 
in more detail , three of the four mutated sba samples harbored the most frequent hotspot mutation of erbb3 ( v104m ) , whereas one sample harbored the e928g mutation , which has been mainly described in lobular breast adenocarcinoma18 and found in only one case in the two largest series of colorectal cancer sequencing.17 , 19 a striking finding of this study was the significant co - occurrence of erbb2 and erbb3 mutations across tumor samples . 
oncogenic mutations that activate the same signaling pathway are usually distributed according to a mutually exclusive mode in a given cancer type , eg , kras , nras , and braf mutations in colorectal cancers.17 in breast cancer , the study of heterogeneous erbb2 - amplified tumors ( a rare phenotype ) has shown that erbb2 - amplified subclones coexisted with her2 - mutated subclones.20 however , the ngs targeted analysis performed in the current study on two of the three cases with both erbb3 and erbb2 mutations did not demonstrate any significant differences between their allelic frequencies . 
the three sba samples with both erbb2 and erbb3 mutations exhibited microsatellite instability and likely had a high mutational load , 21 suggesting a possible causality that has yet to be investigated . more recently , a study performed genomic profiling of 317 sba cases , using colorectal and gastric cancers as controls.22 the reported overall erbb3 mutation rate was 6.3% , similar to that observed in our study , and was significantly higher than that observed in colorectal ( p = .001 ) and gastric ( p = .02 ) cancers in their cohort . 
this previous report provided no data regarding erbb3 and erbb2 mutation co - occurrence or the association between erbb3 mutation and msi - h . in 2017 , the food and drug administration granted accelerated approval to an immune checkpoint inhibitor ( pembrolizumab , an anti pd - 1 antibody ) for the treatment of patients with unresectable or metastatic msi - h solid tumors , regardless of the histology , on the basis of the impressive results observed in these tumors.23 for patients with concomitant msi - h tumors and erbb2 / 3 mutations , anti - her2 and antipd - 1 drugs can therefore both be considered as treatment options . 
in view of the clearly demonstrated benefit of antipd - 1 drugs in this setting , 23 , 24 which can achieve long - lasting complete responses , although anti - her2 / 3 drugs are not currently approved in this setting , anti pd - 1 drugs should probably be preferred . 
studies testing the toxicity and efficacy of immune checkpoint inhibitors and anti - her2 / 3 targeted therapies could be particularly relevant for msi - h erbb2 / 3 - mutated cancers . finally , we acknowledge that our study has several limitations . 
these include the limited sample size resulted in large cis for estimation of mutation rates , the lack of fresh frozen material prevented the performance of more comprehensive whole - exome sequencing , and , in cases with dual erbb2 / erbb3 mutations , the absence of single cell sequencing did not allow the demonstration of epistatic interactions between erbb2 and erbb3 mutations . 
hyman dm , piha - paul sa , rodon j , et al : abstract ct001 : neratinib in her2 or her3 mutant solid tumors : summit , a global , multi - histology , open - label , phase 2 basket study . 
pereira b , chin s - f , rueda om , et al : the somatic mutation profiles of 2 , 433 breast cancers refines their genomic and transcriptomic landscapes . 
ng cky , martelotto lg , gauthier a , et al : intra - tumor genetic heterogeneity and alternative driver genetic alterations in breast cancers with heterogeneous her2 gene amplification . 
 response to selective ret inhibition with loxo - 292 in a patient with ret fusion - positive lung cancer with leptomeningeal metastases robin guo , md1 ; mark schreyer , ms1 ; jason c . 
hyman , md1 , 4 ; and alexander drilon1 , 4 introduction the development of leptomeningeal metastases is a poor prognostic factor in patients with advanced cancers.1 - 3 in nonsmall - cell lung cancers ( nsclcs ) , median overall survival of patients from the diagnosis of leptomeningeal disease is 1 to 2 months without treatment and up to 8 months with systemic therapy.4 - 6 furthermore , patients with leptomeningeal disease have historically had limited access to novel therapies in clinical trials . 
recent efforts from many groups , including the european society for medical oncology and the us food and drug administration ( fda ) , have encouraged the inclusion of patients with leptomeningeal metastases in clinical trials , in addition to promoting standardization of intracranial response assessments.7 - 9 these efforts are crucial given that many investigational agents have substantial cns activity and may improve outcomes in driver - positive cancers with leptomeningeal involvement.5 , 10 ret fusions are actionable oncogenic drivers that are identied in 1% to 2% of nsclcs.11 , 12 to date , chemotherapy and / or immunotherapy remain the only approved systemic therapies for these cancers . 
although these agents were found to be active in these patients , outcomes are modest a subset of compared with targeted therapies in other driverpositive lung cancers , and intracranial activity is poor.13 , 14 selective ret inhibitors currently in development , such as loxo - 292 and blu - 667 , have improved outcomes for patients with ret fusion - positive cancers because of increased potency and less offtarget toxicity.15 , 16 in september of 2018 , loxo - 292 received breakthrough therapy designation from the fda for treatment of patients with metastatic ret fusion - positive nsclcs ( as well as ret fusion - positive thyroid cancers and ret - mutant medullary thyroid cancer )  . 
in addition , conrmed intracranial responses and durable disease control have been achieved in patients with brain metastases in an ongoing phase i / ii trial of loxo - 292 for patients with ret fusion - positive cancers.15 its activity in leptomeningeal disease , however , has not previously been characterized . 
computed and positron - emission tomography imaging revealed a hypermetabolic 4.8lobe mass , mediastinal and hilar cm right adenopathy , and osseous metastases involving l1 , the sacrum , and the left anterolateral sixth rib . 
magnetic resonance imaging ( mri ) of the brain showed three subcentimeter enhancing foci in the right precentral lobe . gyrus , right parietal endobronchial biopsy of an r4 lymph node revealed adenocarcinoma with signet ring cell features ( fig 1a )  . tumor cells were positive for ttf - 1 and negative for p40 by immunohistochemistry . 
broad , hybrid capture based next - generation sequencing using the memorial sloan kettering integrated mutation proling of actionable cancer targetsmsk - impactand illumina hiseq 2500 ( illumina , san diego , ca ) 17 identied an eml4 - ret fusion ( fig 1b ) in addition to a tp53 p.p142tfs * 5 frameshift mutation . 
this eml4 - ret fusion was conrmed using a targeted rna - based anchored multiplex polymerase chain reaction archer fusion assay ( archer , boulder , co )  . with identication of the ret fusion , the patient was treated with the investigational anti - ret multikinase inhibitor rxdx - 105.18 , 19 although a conrmed partial response was initially achieved ( a near - complete response in her brain metastases ) , her course was marked by isolated asymptomatic intracranial progression requiring multiple radiation treatments . 
 guo et al eml4 ( nm_019063.3 ) ret ( nm_020630.4 ) 8 9 10 1112 13 14 15 16 1718 1912 13 1415 1617 18 ence eml4 ( + ) nm_019063.3|exon : 19 ret ( + ) nm_020630.4|exon : 12 fig 1 . 
 ( a ) a hematoxylin and eosinstained section from a cell block of a ne - needle aspiration specimen from a lower paratracheal lymph node conrmed a diagnosis of lung adenocarcinoma . 
clusters of malignant epithelial cells with signet - ring cell morphology ( eccentrically placed nuclei , focally prominent nucleoli , and abundant amount of cytoplasm containing grayish - blue mucin ) are shown . 
 ( b ) an in - frame ret fusion containing the ret tyrosine kinase domain was identied in extracted dna from this sample by broad , hybrid capturebased next - generation sequencing using the memorial sloan kettering integrated mutation proling of actionable cancer targetsmsk - impact and illumina hiseq 2500 ( illumina , san diego , ca )  . exon 19 of the 5 ( cid : 1 ) upstream gene partner eml4 was fused to exon 12 of 3 ( cid : 1 ) ret . 
this eml4 - ret fusion was conrmed using an rna - based anchored multiplex polymerase chain reaction ( archer , illumina miseq [ archer , boulder , co ] )  . four months later , the patient developed symptomatic progression of brain metastases and new leptomeningeal disease . 
she presented with left facial , tongue , and upper extremity tingling and worsening neck pathese symptoms were deemed to be secondary to leptomeningeal disease that was identied radiologically in the right hemisphere , predominantly in the right parietal lobe ( fig 2a ; top panel ) , recognizing that nonradiologically apparent disease was likely present in other areas.8 multiple brain metastases had also increased ( largest measuring 2.7 cm in the right frontal lobe ; fig 2a ; bottom panel )  . 
a cant lumbar puncture was recommended , but the patient declined ; a brain biopsy to potentially determine the mechanism of resistance to rxdx - 105 was not deemed safe . extracranial imaging again showed no evidence of disease . given that the patient was highly symptomatic with progressive symptoms , a single - patient use protocol of loxo - 292 was approved by the fda and institutional review board . 
magnetic resonance imaging axial brain images are shown ( a ) at baseline , ( b ) 5 weeks , and ( c ) 21 weeks after the initiation of loxo - 292 therapy in a patient with an eml4ret fusion - positive lung cancer . 
a representative right superior medial and right lower frontal intraparenchymal metastasis ( green arrows ) regressed with loxo - 292 therapy , along with several other metastases followed on serial intracranial response by recist ( response evaluation criteria in solid tumors ) v1.1 and a complete response in leptomeningeal disease by response assessment in neuro - oncology were achieved . 
a conrmed partial patient provided written informed consent before enrollment , and loxo - 292 was administered orally at 160 mg twice daily . this dose was selected based on preliminary safety and efcacy results from an ongoing phase i / ii trial of the drug ( clinicaltrials.gov identier : nct03157128 )  . imaging assessments ( mri of the brain and computed tomography of the chest , abdomen , and pelvis ) were performed every 8 weeks . response was assessed by recist ( response evaluation criteria in solid tumors ) version 1.1.20 response of leptomeningeal metastases was assessed in accordance with response assessment in neuro - oncology criteria.8 additional volumetric three - dimensional imaging was performed on subsequent scans ( sloan kettering advanced imaging lab , sail ; figs 3b and 3c )  . a clinical response to therapy was achieved within the rst week of therapy , with improvement and subsequent resolution of the patients neurologic symptoms . 
in addition , loxo - 292 therapy achieved complete resolution of leptomeningeal in neuroenhancement , with a response assessment oncology leptomeningeal score dropping from 1 at baseline to 0 at 8 weeks . 
volumetric assessment revealed a continued decrease in the total volume of signicant intracranial disease ( leptomeningeal and parenchymal ) , with a maximal shrinkage of 65% ( from 20.1 cm3 at baseline to 7 cm3 ) at 5 months ( fig 3c )  . the patient continues to receive therapy with loxo - 292 at 10.8 months , with ongoing radiologic disease control and no neurologic symptoms . 
volumetric three - dimensional magnetic resonance imaging analyses were performed on serial imaging performed at ( a ) baseline , ( b ) 5 weeks , and ( c ) 21 weeks . 
maximal volumetric disease regression of 65% was achieved at 21 weeks in the graph of total volume over time on loxo - 292 therapy as shown in the bottom panel . 
in nsclcs with leptomeningeal metastases , there is no consensus on the use of wholebrain radiotherapy , because it has not been shown to consistently improve survival.1 , 3 although systemic chemotherapy with more contemporary regimens ( including pemetrexed and / or bevacizumab ) and intrathecal chemotherapy have been shown to improve outcomes in select series , the development of new agents with higher response rates and more durable disease control continues to represent an unmet need for many patients.4 , 6 this report represents the rst description , to our knowledge , of leptomeningeal metastases responding to any systemic therapy in a patient with a ret fusion - positive cancer . 
a brisk and durable ongoing response to loxo - 292 was achieved in a patient with a ret fusion - positive lung cancer who had notable disease progression while 4 2019 by american society of clinical oncology receiving a prior multikinase inhibitor and multiple prior stereotactic radiosurgery treatments . 
in preliminary data from trial ( clinicaltrials.gov identier : an ongoing phase i / ii nct03157128 ) , all four patients with untreated measurable parenchymal metastases had conrmed intracranial responses to therapy accompanied by overall disease control.15 durable intracranial and extracranial disease control was likewise established in several other patients with untreated nonmeasurable brain metastases before loxo - 292 therapy . the activity of loxo - 292 in the cns can be attributed to several factors . 
the drug is active preclinically , with oral dosing in an orthotopic mouse model of a ret fusionpositive patient - derived tumor implanted into the brain.21 , 22 its potency and selectivity for ret are also likely contributory . 
using a highly active agent in the cns is crucial in ret fusion - positive lung cancers , because close to 25% of patients present with intracranial disease at baseline , whereas the lifetime prevalence of brain metastases approaches 50%.14 in addition , loxo - 292 was designed to target potential resistance mechanisms that can emerge from prior multikinase inhibitor use , such as ret v804m / l gatekeeper substitutions . 
 response to loxo - 292 in ret - rearranged leptomeningeal disease fusions are also identied in papillary thyroid , anaplastic thyroid , colorectal , pancreatic , and breast cancers ; spitzoid neoplasms ; and chronic myeloproliferative neoplasms.11 somatic and germline - activating ret mutations are likewise actionable drivers of oncogenesis that are identied in medullary thyroid cancers and potentially other malignancies.33 although the frequency at which intracranial metastases present is lower for many of these other cancers compared with nsclcs , metastatic disease in the cns can occur in some cases.34 in conclusion , selective ret inhibition with loxo - 292 achieved a clinically meaningful and conrmed response in a patient with a ret fusion - positive lung cancer with leptomeningeal disease and heavily pretreated brain metastases . 
although additional conrmation of this activity will help elucidate overall intracranial disease outcomes , this report underscores the potential of selective ret inhibition as a means of treating and preventing the occurrence of disease in the cns in patients with ret - dependent cancers of any histology . affiliations 1memorial sloan kettering cancer center , new york , ny 2loxo oncology , stamford , ct 3new york university langone medical center , new york , ny 4weill cornell medical college , new york , ny s . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . dahlia henry employment : loxo stock and other ownership interests : loxo , allergan , axovant sciences , palatin technologies mark g . 
kris consulting or advisory role : astrazeneca , regeneron , pzer travel , accommodations , expenses : astrazeneca , genentech other relationship : memorial sloan kettering cancer center robert j . 
young stock and other ownership interests : agios , alexion pharmaceuticals , biogen , celgene , gilead sciences , karyopharm therapeutics , spark therapeutics , regeneron , stemline therapeutics , vertex consulting or advisory role : agios , puma biotechnology , nordicneurolab , icon clinical research research funding : agios ( inst ) david m . 
future oncol 14 : 391 - 407 , 2018 omuro am , kris mg , miller va , et al : high incidence of disease recurrence in the brain and leptomeninges in patients with nonsmall cell lung carcinoma after response to getinib . 
cancer 103 : 2344 - 2348 , 2005 lee sj , lee ji , nam dh , et al : leptomeningeal carcinomatosis in non - small - cell lung cancer patients : impact on survival and correlated prognostic factors . j thorac oncol 8 : 185 - 191 , 2013 li ys , jiang by , yang jj , et al : leptomeningeal metastases in patients with nsclc with egfr mutations . 
j thorac oncol 11 : 1962 - 1969 , 2016 park jh , kim yj , lee jo , et al : clinical outcomes of leptomeningeal metastasis in patients with non - small cell lung cancer in the modern chemotherapy era . lung cancer 76 : 387 - 392 , 2012 kim es , bruinooge ss , roberts s , et al : broadening eligibility criteria to make clinical trials more representative : american society of clinical oncology and friends of cancer research joint research statement . 
neuro - oncol 19 : 484 - 492 , 2017 le rhun e , weller m , brandsma d , et al : eano executive board and esmo guidelines committee : eano - esmo clinical practice guidelines for diagnosis , treatment and follow - up of patients with leptomeningeal metastasis from solid tumours . 
liao bc , lee jh , lin cc , et al : epidermal growth factor receptor tyrosine kinase inhibitors for non - small - cell lung cancer patients with leptomeningeal carcinomatosis . 
aisner dl , sholl lm , berry ld , et al : the impact of smoking and tp53 mutations in lung adenocarcinoma patients with targetable mutations - the lung cancer mutation consortium ( lcmc2 )  . 
drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 14 . 
oxnard gr , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer : an update from asco 2018 . 
subbiah v , taylor m , lin j , et al : highly potent and selective ret inhibitor , blu - 667 , achieves proof of concept in a phase i study of advanced , ret - altered solid tumors . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
drilon ae , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
yang jc - h , cho bc , kim d - w , et al : osimertinib for patients ( pts ) with leptomeningeal metastases ( lm ) from egfr - mutant nonsmall cell lung cancer ( nsclc ) : updated results from the bloom study . 
reungwetwattana t , nakagawa k , cho bc , et al : cns response to osimertinib versus standard epidermal growth factor receptor tyrosine kinase inhibitors in patients with untreated egfr - mutated advanced nonsmall - cell lung cancer . 
wu yl , ahn mj , garassino mc , et al : cns efcacy of osimertinib in patients with t790m - positive advanced nonsmall - cell lung cancer : data from a randomized 28 . 
costa db , shaw at , ou sh , et al : clinical experience with crizotinib in patients with advanced alk - rearranged nonsmall - cell lung cancer and brain phase iii trial ( aura3 )  . 
gadgeel s , peters s , mok t , et al : alectinib versus crizotinib in treatment - naive anaplastic lymphoma kinase - positive ( alk + ) non - small - cell lung cancer : cns efcacy results from the alex study . 
shaw at , kim tm , crin `o l , et al : ceritinib versus chemotherapy in patients with alk - rearranged non - small - cell lung cancer previously given chemotherapy and crizotinib ( ascend - 5 ) : a randomised , controlled , open - label , phase 3 trial . 
camidge dr , kim dw , tiseo m , et al : exploratory analysis of brigatinib activity in patients with anaplastic lymphoma kinase - positive nonsmall - cell lung cancer and brain metastases in two clinical trials . 
solomon bj , besse b , bauer tm , et al : lorlatinib in patients with alk - positive non - small - cell lung cancer : results from a global phase 2 study . 
 o genomic resistance patterns to second - generation androgen blockade in paired tumor biopsies of metastatic castration - resistant prostate cancer purpose patients with castration - resistant prostate cancer ( crpc ) receive second - generation androgen - deprivation therapy , but frequently experience relapse or do not respond . 
understanding the genetic mechanisms of resistance will help to identify strategies and biomarkers that are essential for the next line of therapy . patients and methods we analyzed whole exomes of patient - matched preand post - treatment tumors from patients with crpc . 
these patients had received the secondary androgendeprivation therapy agent , abiraterone , which suppresses androgens to below castration levels , or enzalutamide , which competitively inhibits the key androgen signaling effector , androgen receptor . results we observed that abiraterone - resistant tumors harbored alterations in ar and myc , whereas enzalutamide - resistant tumors gained alterations in cell - cycle pathway genes , such as mutation in cyclin - dependent kinase n2a ( cdkn2a ) or amplification of cdk6 . 
experimentally , overexpressing cell - cycle kinases promoted enzalutamide resistance in androgen - sensitive lncap cells that was mitigated via cdk4 / 6 blockadepalbociclib and ribociclib . conclusion cdk4 / 6 - mediated resistance observed in preclinical experiments suggests that cdk4 / 6 amplifications may sufficiently promote enzalutamide resistance in crpc , and that these patients may respond to palbociclib or ribociclib . 
2017 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction prostate cancer is among the most prevalent adult malignancies in men.1 patients with metastatic prostate cancer receive primary androgen - deprivation therapy ( adt ) , and whereas many patients achieve a response , almost all develop castration - resistant prostate cancer ( crpc ; fig 1a )  . 
for patients with crpc , the standard of care includes secondgeneration inhibitors of androgen receptor ( ar ) signaling , including abiraterone2 and enzalutamide.3 these agents effectively prolong survival , but all patients eventually develop resistance . moreover , considering the potential wider usage of abiraterone from recent findings on the benefit of adding abiraterone and prednisone to primary adt in hormone - sensitive advanced prostate cancer , 4 understanding the resistance mechanisms that are specific to these agents is even more critical . previous studies have identified several mechanisms of primary or secondary adt resistance : ar activation , ar bypass , and resistance independent of the ar signaling axis.5 ar - activating alterations include amplifications , 6 mutations , 7 and splicing variants.8 multiple studies of patients with crpc at single time points identified alterations in other pathways , including dna repair9 and cell - cycle pathways , 6 although their specific g . 
patients with resistance to nextgeneration androgendeprivation therapy ( adt ) can be classified according to acquired and intrinsic mechanisms using prostate - specific antigen ( psa ) level change . ( a ) schematic overview of paired ( preand posttreatment ) tumor biopsy collection in the context of next - generation adt , abiraterone , and enzalutamide , followed by whole - exome sequencing and computational analysis to investigate clinical resistance mechanisms . ( b ) change in psa levels between the start of treatment ( at the time of pretreatment biopsy , day 0 ) and the end ( at the time of post - treatment biopsy ) of treatment . 
crpc , castration - resistant prostate cancer . primary prostate crpc germline pretreatment biopsy next - generation ( abiraterone / enzalutamide ) postrelapse biopsy resistant time clinical information psa level patient history radiographic images post whole - exome sequencing identify resistanceassociated alterations clinical resistance mechanisms 6 months patients abi - 1 abi - 2 abi - 3 abi - 4 enza - 1 enza - 2 enza - 3 acquired resistance intrinsic resistance psa50 psa75 psa88 time of treatment ( days ) relationship to treatment resistance has been incompletely characterized . whereas genomic studies of metastatic prostate cancer have demonstrated genomic alterations in ar and its pathway , the genomic characterization of paired biopsy samples from living patients with crpc before secondary adt initiation and at the time of resistance have been limited as a result of the logistical challenges of obtaining repeated tumor biopsies and tumor heterogeneity in metastatic prostate cancer . 
after assessment of pathology and whole - exome sequencing quality metrics ( appendix ) for the 15 patients who were included in this clinical series , results from seven patients were available for analysis ( data supplement )  . 
we also examined clinical information for each patient ( data supplement ) , including prostate - specific antigen ( psa ) levels ( fig 1b ) , treatment history , and radiographic images ( data supplement )  . 
we primarily used therapy duration and changes in psa level to define clinical response.10 we confirmed soft tissue progression using response evaluation criteria in solid tumors ( recist v1.1 ) 11 criteria and bone disease progression using protocol by prostate cancer working group 212 criteria ( appendix )  . 
6 months , with the remaining patients being intrinsically resistant ( fig 1b )  . by this measure , three patients ( abi - 1 , enza - 1 , and enza - 3 ) exhibited acquired resistance , and four patients ( abi - 2 , abi - 3 , abi - 4 , and enza - 2 ) were intrinsically resistant . we then performed mutation , copy number , and phylogenetic analyses of these tumors to nominate putative genetic correlates of resistance by therapeutic class ( appendix )  . 
in abiraterone patients , one patient ( abi - 2 ) , who was clinically classified as intrinsically resistant , harbored a wellcharacterized ar resistance mutation ( l702h ) 13 , 14 in the post - treatment sample that was not detected in the pretreatment sample ( 0 of 62 reads and 17 of 46 reads in preand post - treatment tumors , respectively ; fig 2 )  . 
in two additional intrinsic patients ( abi - 3 and abi - 4 ) , both preand abi - 2 rac1 lmna jak1 tp53 myo5a pretreatment allelic fraction chrx : 66 , 931 , 463 reference : 62 variant : 0 ar p.l702h ( t > a ) reference : 46 variant : 17 fig 2 . 
 ( a and b ) ar , myc amplification , and abiraterone resistance . copy number profile of paired samples of patients abi - 1 , abi - 3 , and abi - 4 across the genome ( top ) are depicted , and the status of chrx and chr8 is displayed for respective patients ( bottom )  . 
vertical bars and alternating colors demarcate the borders between chromosomes . both preand posttreatment samples from abi - 3 and abi - 4 harbored ar amplifications , whereas samples from abi - 1 harbored pre - existing ar amplification but obtained a focal gain of myc in the resistant sample . 
although our observations associate ar with abiraterone resistance , one patient with pre - existing ar focal amplification ( abi - 1 ) demonstrated an initial 50% decrease in psa level response before ultimately developing resistance ( fig 1b )  . 
white line represents the needle used to withdraw tumor tissue . ( b ) in patient enza - 1 , the fraction of mutations unique to the pretreatment and post - treatment states are shown in blue and red , respectively . 
cancer cell fractions ( ccf ) for mutations in the pretreatment ( x - axis ) and post - treatment ( y - axis ) tumors are compared . selected cancer genes are annotated in the ccf plots . ( c ) p81l mutation of cdkn2a , found only in the post - treatment tumor , is visualized in the integrated genomics viewer ( igv ) browser . 
change of nucleotide , amino acid , and number of reads in reference and variant alleles are shown in the box . enza - 1 post enriched in posttreatment tumor tp53 shared by both tumor samples cdkn2a enriched in pretreatment tumor pre - ccf chr9 : 21 , 971 , 116 p81l ( g > a ) reference : 140 variant : 0 p81l ( g > a ) reference : 39 variant : 9 cdkn2a resistance to ar suppression and bicalutamide.15 , 16 our result associates myc with abiraterone resistance independent of ar status , which suggests that genetic changes beyond ar may also contribute to clinical abiraterone resistance . we then examined genetic evolution in the context of clinical resistance to enzalutamide . 
in one patient ( enza - 1 ) with paired biopsy samples that were obtained from the same site ( fig 4a ) , a p81l mutation in cdkn2a was only detected in the resistant tumor ( figs 4b and 4c and data supplement )  . 
this is a clinically observed cancer mutation17 that is also adjacent to a hotspot location ( r80 ) .18 in addition , relative to wild - type cdkn2a , p81l is functionally defective when overexpressed in melanoma cells.19 the posttreatment tumor from a second enzalutamideresistant patient ( enza - 2 ) had chr7q ( spanning cdk6 ) , whereas ar amplification was detected at both time points ( fig 5 )  . 
because the genetic loss of all rb family members promotes the constitutive activation of cdk signaling , we also investigated alterations of rb family proteins ( rb1 , rbl1 , and rbl2 ; data supplement )  . 
in the last acquired - resistance patient ( enza - 3 ) , we did not detect alterations in cell - cycle genes or oncogenic pathways that had been previously associated with adt resistance . the observation of cell - cycle up - regulation specifically from these enzalutamide - resistant patients suggests the activity of cell - cycle kinases in enzalutamide resistance . 
we followed the schematics in figure 6a and used open reading frames that contained cdk4 or cdk6 to overexpress these genes in enzalutamide - sensitive lncap cells.20 , 21 lncap cells were used to examine the efficacy of enzalutamide in preclinical applications , 20 and have recently been used to study acquired resistance to enzalutamide.21 after confirming overexpression by immunoblotting ( data supplement ) , we mimicked adt by first culturing each resulting cell line in media that was supplemented with androgenfree media ( charcoal - stripped serum [ css ] ) for 3 days and , subsequently , in both css and enzalutamide . 
we observed significant differences in adt proliferation , as cdk4 / 6 - expressing cells continued to proliferate , whereas luciferaseexpressing negative control cells failed to do so ( p , .005 ; two - tailed t test ; fig 6b )  . in combination with the estrogen inhibitor letrozole , the cdk4 / 6 inhibitor palbociclib has recently been approved by the us food and drug administration for treatment of estrogen receptorpositive breast cancers.22 another cdk4 / 6 inhibitor , ribociclib , has demonstrated efficacy in rb wildtype23 and ar mutant prostate cancer cells.24 in two clinical trials , cdk4 / 6 inhibition was thought to benefit prostate cancers that express wild - type rb ( clinicaltrials.gov identifiers : nct02059213 and nct02555189 )  . 
copy number profiles of paired samples of patient enza - 2 across the genome ( top ) are depicted , and the status of chr7 is displayed ( bottom )  . 
to test the clinical potential of combining adt with cdk4 / 6 inhibitors specifically in enzalutamide - resistant crpcs with cdk4 / 6 amplifications , we again used our preclinical model in which cdk4 / 6 sufficiently promoted enzalutamide resistance . 
the average of three experiments is plotted and error bars represent standard deviation . ( * ) overexpression of a gene led to a significant difference compared with luciferase control cells . 
 ( ) cell - cycle inhibitor treatment led to a significant reduction of proliferation ( p , .005 , two - tailed t test )  . enzalutamide - resistant metastatic crpcs that have cdk4 / 6 amplifications in patient cases of clinical resistance that are either intrinsic or acquired . discussion in summary , we used a paired biopsy approach and have associated the clinical resistance of abiraterone with ar alterations and , in one patient , with myc . 
two enzalutamide - resistant patients harbored aberrations in cell - cycle pathway genes . our preclinical data demonstrate that cdk4 / 6 overexpression sufficiently drove enzalutamide resistance , but this phenotype was abrogated by cdk4 / 6 inhibitors . 
for enzalutamide - resistant patients , we identify the specific cell - cycle mutations , cdkn2a and cdk4 / 6 , as biomarkers that may predict whether an enzalutamide - resistant patient could benefit from combination therapy that involves cdk4 / 6 inhibition and enzalutamide . 
in this study , we do not disambiguate enzalutamide resistance from general adt resistance ; however , other forms of adt resistance , including ar - splice variants , that promote enzalutamide resistance22 , 25 , 26 and general castration resistance27 demonstrate a challenge in mechanistically discerning treatment - specific or class - wide resistance mechanisms . 
addressing differences via expanded clinical cohorts and diverse preclinical models may determine strategies by which patients with such resistance may be treated . although two patients were classified as intrinsically resistant by clinical parameters , paired analysis demonstrated clinically relevant alterations in ar and cell - cycle genes only in the resistant tumor . 
in addition , difficulties in consistently obtaining anatomically matched biopsies at two time points for a subset of this cohort make definitive conclusions about resistance mechanisms or tumor heterogeneity difficult to tease apart . 
mechanistically , we speculate that adt - resistant clonal evolution can rapidly occur ; therefore , matched tissue and / or blood - based biopsies sampled at more finite intervals , along with rna analysis for ar splicing and transcriptional changes , if available , may inform us of the dynamic selection of resistant subclones and patients who were not explained solely by bulk tumor biopsies . 
hahn , mary - ellen taplin financial support : mary - ellen taplin administrative support : mary - ellen taplin provision of study materials or patients : zhenwei zhang , glenn j . 
balk honoraria : janssen pharmaceuticals consulting or advisory role : sanofi patents , royalties , other intellectual property : license to nkt therapeutics for an antibody expert testimony : astellas medivation travel , accommodations , expenses : janssen pharmaceuticals william c . 
ca cancer j clin 66 : 7 - 30 , 2016 de bono js , logothetis cj , molina a , et al : abiraterone and increased survival in metastatic prostate cancer . 
scher hi , halabi s , tannock i , et al : design and end points of clinical trials for patients with progressive prostate cancer and castrate levels of testosterone : recommendations of the prostate cancer clinical trials working group . j clin oncol 26 : 1148 - 1159 , 2008 13 . 
comstock ces , augello ma , goodwin jf , et al : targeting cell cycle and hormone receptor pathways in cancer . 2016 oncogene 32 : 5481 - 5491 , 2013 24 . 
antonarakis es , lu c , wang h , et al : ar - v7 and resistance to enzalutamide and abiraterone in prostate cancer . n engl j med 371 : 1028 - 1038 , 2014 26 . 
hu r , dunn ta , wei s , et al : ligand - independent androgen receptor variants derived from splicing of cryptic exons signify hormone - refractory prostate cancer . 
cancer res 69 : 16 - 22 , 2009 patients who were eligible for this analysis had metastatic castration - resistant prostate cancer ( crpc ) and were being considered for next - generation androgen - deprivation therapy ( adt ) using abiraterone acetate or enzalutamide . 
all patients provided written informed consent to obtain metastatic tumor biopsies and for molecular profiling of preand post - treatment tumor and germline samples . biopsies and pathology review paired biopsies were collected as outlined in the protocols of the clinical trials described above and in a prior study ( mckay rr , et al : clin cancer res 23 : 935 - 945 , 2017 )  . 
pretreatment baseline biopsies were obtained before starting therapy , and post - treatment progression biopsies were obtained at the time of radiographic progression ( fig 1a ) while the patients were still on treatment . 
matched trios of germline , pre - , and post - treatment tumor samples were obtained for all patients , and seven patients who were treated with abiraterone ( n = 4 ) or enzalutamide ( n = 3 ) among an initial 15 patients passed the quality control . 
clinical responses to therapy were determined using the response evaluation criteria in solid tumors ( recist v1.1 ) 11 for soft tissue progression and prostate cancer working group 212 for bone disease progression . participants were evaluated every 4 weeks by prostate - specific antigen and every 12 weeks by computed tomography and bone scan and were not taken off treatment until documented symptomatic progression or progression by imaging as protocol defined by recist ( v1.1 ) and prostate cancer working group 2 . whole - exome sequencing and sequence data processing whole - exome sequencing was performed on extracted dna using illumina ( san diego , ca ) and agilent technologies ( santa clara , ca ) platforms . 
exome sequencing data were processed using established analytic pipelines at the broad institute of mit and harvard ( cambridge , ma ; van allen em , et al : nat med 20 : 682 - 688 , 2014 )  . 
bam files were produced via the picard pipeline ( picard.sourceforge.net / ) , uploaded , and processed through the firehose pipeline ( cga / firehose )  . bam files are currently in process for submission to the database of genotypes and phenotypes . data availability sequencing quality control exome sequence data processing and analysis were performed using pipelines at the broad institute . 
from the patients we examined , individuals with immediate cessation of therapy , with low coverage ( germline , 350 , tumor , 3100 ) in one or more tumors , or those who experienced the failure of manual copy number profile inspection were filtered out ( data supplement )  . 
furthermore , individuals with tumor purity of > 0.15 for all matched trios of germline , pre - , and posttreatment tumor samples were obtained , which resulted in seven individuals for additional analyses . 
no additional selection process was used to identify the seven individuals for analysis . variant calling and phylogenetic analysis to identify somatic single - nucleotide variants , mutect ( cibulskis k , et al : nat biotechnol 31 : 213 - 219 , 2013 ) was applied and reviewed with integrated genomics viewer ( igv ; robinson jt , et al : nat biotechnol 29 : 24 - 26 , 2011 )  . 
artifacts from dna oxidation during sequencing were removed using a filtered - based method ( costello m , et al : nucleic acids res 41 : e67 , 2013 )  . 
 variants in cancer genes reported from the cosmic cancer gene census ( cancer.sanger.ac.uk / census ; futreal pa , et al : nat rev cancer 4 : 177 - 183 , 2004 ) bona fide cancer genes that are causally implicated in cancersare shown in allelic frequency scatter plots as in figure 1d . probability distributions of possible cancer cell fractions of point mutations were calculated on the basis of local copy number and the estimated sample purity was inferred using absolute ( carter sl , et al : nat biotechnol 30 : 413 - 421 , 2012 )  . copy number analysis copy ratios were segmented using the circular binary segmentation algorithm ( olshen ab , et al : biostatistics 5 : 557 - 572 , 2004 )  . 
rescaled copy numbers for each genomic segment were calculated using absolute ( carter sl , et al : nat biotechnol 30 : 413 - 421 , 2012 ) to correct copy ratios for variations in sample purity and ploidy . 
to classify segments into categories , including high - level amplification , amplification , homozygous deletion , and no alteration , the focality of each genomic segment was calculated as previously described ( brastianos pk , et al : cancer discov 5 : 1164 - 1177 , 2015 )  . 
after the change of copy number alterations was computed , we selected copy number alterations , such as gained high amplification and gained amplification categories , that were present in the post - treatment tumor only . 
after 4 days of selection , cell lysates were collected and expressions of open reading frames were determined using immunoblots with cdk4 and cdk6 antibodies ( cell signaling technology , danvers , ma )  . 
after confirming their respective expression , each cell line was cultured in androgen - free media for 3 days , and vi - cell was used to count and seed 100 , 000 cells in quadruplicates in a 12 - well plate for 14 days in androgenfree media ( charcoal - stripped serum ; atlanta biologicals , atlanta , ga ) with enzalutamide 2.5 mm and either ribociclib 500 nm , palbociclib 500 nm ( selleck chemicals , houston , tx ) , or dmso control . 
lncap cells are not among the cell lines that are easily misidentified as described by the international cell line authentication committee . these cells are purchased directly from american type culture collection ( manassas , va ) , which maintains authenticated cell lines by sequencing and comparing short tandem repeats to parental lncap cells in their database . 
before the experiments , cells were tested for several strains of mycoplasma contamination using mouse / rat comprehensive clear panel w / corynebacterium bovis from charles river laboratories ( wilmington , ma )  . 
 comprehensive analysis of the unfolded protein response in breast cancer subtypes purpose triple - negative breast cancers ( tnbcs ) are associated with a worse prognosis and patients with tnbc have fewer therapeutic options than patients with non - tnbc . 
recently , the ire1a - xbp1 branch of the unfolded protein response ( upr ) was implicated in tnbc prognosis on the basis of a relatively small patient population , suggesting the diagnostic and therapeutic value of this pathway in tnbcs . 
in addition , the ire1a - xbp1 and hypoxia - induced factor 1 a ( hif1a ) pathways have been identified as interacting partners in tnbc , suggesting a novel mechanism of regulation . 
to comprehensively evaluate and validate these findings , we investigated the relative activities and relevance to patient survival of the upr and hif1a pathways in different breast cancer subtypes in large populations of patients . materials and methods we performed a comprehensive analysis of gene expression and survival data from large cohorts of patients with breast cancer . 
the patients were stratified based on the average expression of the upr or hif1a gene signatures . results we identified a strong positive association between the xbp1 gene signature and estrogen receptorpositive status or the hif1a gene signature , as well as the predictive value of the xbp1 gene signature for survival of patients who are estrogen receptor negative , or have tnbc or her2 +  . 
2017 by american society of clinical oncology introduction triple - negative breast cancers ( tnbcs ) represent a breast cancer subpopulation lacking estrogen receptor ( er ) , progesterone receptor ( pr ) , and her2 expression.1 patients with tnbc have a worse prognosis than those with non - tnbc , suggesting more aggressive biologic behavior . 
the unfolded protein response ( upr ) is an adaptive process to alleviate endoplasmic reticulum stress during tumor growth and proliferation.2 one major upr signaling pathway , ire1a leading to activation of xbp1 , is implicated in multiple types of cancers , including breast cancer.3 a recent study reported that tnbc cell lines and primary tumor samples from patients with tnbc express higher levels of the activated form of xbp1 than non - tnbc.4 furthermore , this study also revealed that in tnbc cells , xbp1 coregulates hif1a target genes , and that both xbp1 and hif1a gene signatures were associated with poor prognosis in tnbc , but not in patients with er + breast cancer . 
for example , the expression of esr1 , gata3 , and xbp1 were highly correlated in breast cancer.5 , 6 in addition , xbp1 enhances the transactivation activity of era7 and was identified as an estrogenresponsive gene.8 recently , our laboratory identified that doxorubicin , a widely used chemotherapeutic agent in breast cancer treatment , is a potent inhibitor of xbp1 activation.9 therefore , clarifying the role of xbp1 in breast cancer prognosis would not only improve the application of existing treatment strategy but also would dadi jiang brandon turner jie song ruijiang li maximilian diehn quynh - thu le purvesh khatri albert c . 
using the same four luminal and six basal - like cell lines reported by chen et al , 4 ( a ) average expression of the xbp1 gene signature was higher in the luminal type , although not statistically significant , whereas ( b ) average expression of the atf4 / chop signature was significantly higher in the basal - like type . 
the cell line collection consists of 19 estrogen receptor ( er ) + and 32 er , or 25 triple - negative breast cancer ( tnbc ) and 26 non - tnbc cell lines defined on the basis of mrna / protein levels of er / progesterone receptor / her2 . 
 ( e ) the same analysis on microarray data of patients with breast cancer from the cancer genome atlas database ( n = 404 er + and n = 118 er , or n = 91 tnbc and n = 431 non - tnbc )  . 
 support the preclinical development of therapy on the basis of modulating xbp1 activity.10 , 11 in this study , we comprehensively investigated the activity of xbp1 , its relationship with the er status as well as the hif1a pathway , and its prognostic value in a large group of patients with breast cancer . 
the rnaseq ( n = 1 , 182 ; illumina hiseq ; illumina , san diego , ca ) and microarray ( n = 597 , a subset of the 1 , 182 patients ; agilentg4502a_07_3 array ; agilent technologies , santa clara , ca ) data with the clinical information of the patients with breast cancer were downloaded from the cancer genome atlas ( tcga ) database through the university of california santa cruz cancer browser . 
all signature and expression data were normalized as z - scores with a mean of 0 and standard deviation of 1 . differences in average expression ( microarray or rnaseq ) level of the gene signatures by er and tnbc status were assessed using the nonparametric wilcoxon rank - sum test . 
mrna expression levels of foxa1 , esr1 , and gata3 were first individually normalized ( mean , 0 ; standard deviation , 1 ) and then averaged together before comparing with either the xbp1 gene signature expression or xbp1 gene expression using regression . 
cox proportional hazards regression models were fit to breast cancer survival data , and the nonparametric log - rank test was used to test for significant differences in relapse - free survival ( rfs ) between subtypes of patients with high or low levels of average xbp1 , atf4 / chop , or hif1a gene signature expression . 
patient survival data up to 150 months were used for the analysis . cell culture and viability assay mda - mb - 231 , hs578t , mda - mb - 468 , mcf7 , t47d , and bt474 cells were purchased from american type culture collection ( manassas , va ) and maintained in dmem supplemented with 10% fetal bovine serum and 1% penicillinstreptomycin , and cells were cultured at 37c with 5% co2 . 
after 72 hours of treatment , xtt reagent ( american type culture collection ) was added to the wells , then cells were incubated for 2 hours , and cell viability was calculated with the following formula : absorbance = a475nm ( test ) a475nm ( blank ) a660nm ( test ) using a biotek synergy h1 plate reader ( biotek , winooski , vt )  . results first , we tested the initial conclusion of the previous study4 that basal - like breast cancer cell lines , which consist primarily of tnbc cells , express higher levels of the spliced / activated form of xbp1 compared with those of the luminal type , which consist primarily of er + cells.4 we found the average expression of the same xbp1 gene signature used by the previous investigators to measure xbp1 activity4 was actually higher in the same set of luminal ( n = 4 ) than basal - like ( n = 6 ) cell lines , albeit without statistical significance ( fig 1a )  . 
 2 average expression of the xbp1 gene signature was significantly higher in er + compared with cell lines , consistent with previous reports ( fig 1c ) .5 - 8 however , there was no statistically significant difference in the xbp1 signature between tnbc and non - tnbc cell lines ( fig 1c )  . in contrast , expression of the atf4 / chop sigor tnbc than in er + or nature was higher in er non - tnbc cell lines , respectively ( fig 1c )  . in established cell these observations lines prompted us to evaluate these pathways in tumor samples from patients with breast cancer . 
we performed the same analyses on 1 , 182 patients with breast cancer from tcga , on the basis of rnaseq ( fig 1d ) , 5 or a subset of 597 patients on the basis of microarray ( fig 1e ) , as well as 1 , 809 curated microarray gene expression profiles ( fig 1f ) .14 in each comparison , we found expression of the xbp1 gene signature was significantly higher in er + or non - tnbc than in er or tnbc tumor samples , respectively . 
overall , we identified a strong correlation between the expression of xbp1 , which is also a transcriptional target of activated xbp1 itself , 4 and er pathway genes ( ie , esr1 , gata3 , and foxa1 ; fig 2a and 2b )  . 
this relationship was also significant when we correlated the average expression of the xbp1 gene signature with the average er pathway gene expression ( fig 2c and 2d )  . these data are consistent with a previous report of xbp1 playing a crucial role in 17 - b - estradiolinduced growth of er + breast cancer cells.15 to test the reported coregulation of target gene expression by activated xbp1 and hif1a4 in a large cohort of patients with breast cancer , we performed similar correlation analysis using the tcga dataset . 
overall , we found a strong correlation between the xbp1 and hif1a gene signatures in patients either er + or er , and with non - tnbc or tnbc , who were from tcga ( fig 2e and 2f )  . 
this result confirms the molecular - level interaction between the two pathways with large - scale gene - expression data from patients and suggests the xbp1 and hif1a pathways are highly correlated in breast cancer regardless of the subtypes . to assess the influence of the upr and hif1a pathways on survival of patients with breast cancer and extend the analysis of the previous study4 to larger patient cohorts , we performed survival analyses of the 1 , 809 - patient data set , using the same high - low expression cutoff ( 58th percentile ) as previously reported.4 surprisingly , the xbp1 signature was not associated with worse rfs in the whole population of patients with breast cancer ( fig 3a , left )  . 
however , when the patient population was further stratified into tnbc versus , or her2 + versus non - tnbc , er + versus er , higher expression of the xbp1 signature her2 was associated with worse rfs in tnbc ( fig 3b , ( fig 3c , left ) , or her2 + ( fig 3d , left ) left ) , er patients , but not in patients positive for er ( fig 3c , left ) or negative for her2 ( fig 3d , left )  . 
interestingly , the atf4 / chop signature was not associated with rfs ( fig 3a , middle ) , even after stratification into either tnbc / non - tnbc , er + / 2 her2 + / 2 status ( fig 3b - 3d , middle )  . 
in contrast , the hif1a signature was significantly associated with rfs regardless of how the patients were stratified ( fig 3a - 3d , right )  . to evaluate whether using gene signature expression cutoffs at the extremes would reveal stronger association , we applied quartile ( the highest 25% v the lowest 25% ) cutoff and performed the same survival analysis . 
the atf4 / chop signature became significantly associated with rfs in the whole population ( data supplement ) and the xbp1 signature became significantly associated ( data with rfs in patients who were her2 supplement )  . 
however , the positive association between the xbp1 signature and rfs in the patients with non - tnbc using the 58th percentile cutoff became negative when using the quartile cutoff , which likely was due to the reduced number of patients in the new categories ( data supplement )  . 
nevertheless , the major conclusions of the current study remain unchanged . discussion in summary , on the basis of a comprehensive analysis on large cohorts of patients with breast cancer , our findings confirm the initial observations from chen et al4 that xbp1 activity was associated with a worse prognosis in tnbc , but not er + patients , and extend this relationship to ( fig 3c , left )  . 
correlation of xbp1 mrna expression and the xbp1 gene signature with estrogen receptor ( er ) pathway gene expression and correlation of the xbp1 and hif1a gene signatures in the the cancer genome atlas ( tcga ) breast cancer data set . 
correlation analysis of expression of the xbp1 gene and the average of three er pathway genes ( esr1 , foxa1 , and gata3 ) using ( a ) rnaseq or ( b ) microarray data from 1 , 182 patients with breast cancer in tcga breast cancer database and the same correlation analysis of the average expression of the xbp1 gene signature and the three er pathway genes on the basis of ( c ) rnaseq or ( d ) microarray data in the tcga database . 
 ( e , f ) correlation of the average expression of the xbp1 and hif1a gene signatures in the groups of patients with breast cancer , on the basis of the rnaseq data in the tcga database : ( e ) er + ( n = 600 patients , gold ) and er ( n = 179 patients , blue ) ; and ( f ) triple - negative breast cancer ( tnbc ; n = 125 patients , blue ) and non - tnbc ( n = 647 patients , gold )  . 
kaplan - meier graphs showing relapse - free survival ( rfs ) of the different subtypes of patients with breast cancer stratified by the xbp1 , atf4 / chop , or hif1a gene signatures . 
kaplan - meier graphs of rfs of ( a ) the total of 1 , 640 patients , ( b ) 225 patients with triple - negative breast cancer ( tnbc ) and 1 , 415 with non - tnbc , ( c ) 1 , 286 who are estrogen receptor ( er ) + and 354 who are er with rfs < 150 months separated by high and low ( with the 58th percentile cutoff used previously4 ) levels of the average expression of the xbp1 ( left column ) , atf4 / chop ( middle column ) , or hif1a ( right column ) gene signature . 
this may partially explain those who are her2 why the xbp1 - rfs association is stronger in than in those with tnbc patients who are er ( fig 3b and 3c , left ) , because some of the patients / her2 + are included in the patients who are er but not in the patients with tnbc . who are er however , through analyzing large - scale gene expression profiles , we identified that average expression of the same xbp1 gene signature reported by chen et al4 was higher in er + or non - tnbc or tnbc cell lines or patients , respecthan er tively ( fig 1c - 1f ) , to correct the initial conclusion by chen et al.4 these data are consistent with other previous studies . 
our findings suggest that , albeit with higher xbp1 activities , patients who are er + , and other patients with non - tnbc ( excluding her2 + ) , may not benefit from therapeutic strategies targeting xbp1 activity . 
the design and aims of the current study are summarized in the schematic shown in the data supplement . recently , we have shown that doxorubicin blocks xbp1 activation through the inhibition of ire1a rnase activity.9 these data suggest that pa , and possibly tients with tnbc , who are er those who are her2 + , may benefit the most from anthracycline - based therapies . 
davies mp , barraclough dl , stewart c , et al : expression and splicing of the unfolded protein response gene xbp - 1 are significantly associated with clinical outcome of endocrine - treated breast cancer . 
finlin bs , gau cl , murphy ga , et al : rerg is a novel ras - related , estrogen - regulated and growth - inhibitory gene in breast cancer . 
j biol chem 276 : 42259 - 42267 , 2001 jiang d , lynch c , medeiros bc , et al : identification of doxorubicin as an inhibitor of the ire1a - xbp1 axis of the unfolded protein response . 
jiang d , niwa m , koong ac : targeting the ire1a - xbp1 branch of the unfolded protein response in human diseases . semin cancer biol 33 : 48 - 56 , 2015 11 . 
gy orffy b , lanczky a , eklund ac , et al : an online survival analysis tool to rapidly assess the effect of 22 , 277 genes on breast cancer prognosis using microarray data of 1 , 809 patients . 
sengupta s , sharma cg , jordan vc : estrogen regulation of x - box binding protein - 1 and its role in estrogen induced growth of breast and endometrial cancer cells . 
lacroix m , leclercq g : about gata3 , hnf3a , and xbp1 , three genes co - expressed with the oestrogen receptoralpha gene ( esr1 ) in breast cancer . 
tozlu s , girault i , vacher s , et al : identification of novel genes that co - cluster with estrogen receptor alpha in breast tumor biopsy specimens , using a large - scale real - time reverse transcription - pcr approach . 
andres sa , wittliff jl : relationships of esr1 and xbp1 expression in human breast carcinoma and stromal cells isolated by laser capture microdissection compared to intact breast cancer tissue . 
wang dy , fulthorpe r , liss sn , et al : identification of estrogen - responsive genes by complementary deoxyribonucleic acid microarray and characterization of a novel early estrogen - induced gene : eeig1 . 
karn t , metzler d , ruckhaberle e , et al : data - driven derivation of cutoffs from a pool of 3 , 030 affymetrix arrays to stratify distinct clinical types of breast cancer . 
wirth , md1 ; takashi kohno , phd2 ; hibiki udagawa , md , phd3 ; shingo matsumoto , md , phd3 ; genichiro ishii , md , phd3 ; kevin ebata , phd4 ; brian b . 
michael rothenberg , md , phd4 ; and koichi goto , md , phd3 introduction the ret receptor tyrosine kinase is oncogenically activated by ret gene fusions in 1% to 2% of nonsmall - cell lung cancers ( nsclc ) and by ret gene mutations in most medullary thyroid cancers ( mtc ) .1 although multikinase inhibitors ( mkis ) with nonspecic anti - ret activity are approved for the treatment of mtc irrespective of ret mutation status , their investigational use for patients with ret fusion - positive nsclc has been limited by substantial off - target adverse effects that lead to dose reductions and inadequate ret - specic inhibition.2 - 7 as a result , tumor responses to mkis have been infrequent and short lived , and a comprehensive molecular understanding of mki response and resistance is lacking . in contrast to the mkis , loxo - 292 is a highly selective , small molecule ret tyrosine kinase inhibitor ( tki ) with nanomolar potency against diverse ret alterations , favorable pharmacokinetic ( pk ) properties , and signicant cns penetration.8 in an ongoing , phase i / ii identier : study of loxo - 292 ( clinicaltrials.gov nct03157128 ) , conrmed partial responses ( prs ) were achieved in most ret - altered patients across different tumor histologies and diverse ret gene fusions and mutations . 
a 42 - yearold woman with nsclc had received nine prior systemic therapy regimens , including approved chemotherapy , immunotherapy , and investigational tkis , before the identication of a kif5b - ret fusion in a sample from a recurrent pleural fusion ( fig 1a , data supplement )  . 
she received alectinib and additional chemotherapy and then vandetanib ( fig 1a ) .6 she experienced a conrmed pr by response evaluation criteria in solid tumors ( recist ) 1.1 with vandetanib treatment , with improvement in multiple lung and pleural - based lesions . 
targeted ret gene sequencing of a biopsy specimen from a progressing right lung lesion identied a ret valine - to - leucine ( v804l ) gatekeeper mutation absent from a pretreatment tumor sample ( fig 1a , data supplement )  . v804l allele frequency in the progression sample was 15% by next - generation sequencing ( 120 of 799 reads ) compared with 0% in the pretreatment sample ( 0 of 847 reads ; data supplement )  . the patient received additional systemic chemotherapy with pemetrexed and amrubicin but experienced continued disease progression . 
after providing written informed consent , she started treatment with loxo292 in the phase i portion of the phase i / ii clinical trial at the recommended phase ii dose of 160 mg twice a day . 
 ( a ) various treatments the patient received for metastatic , kif5b - ret fusion - positive nonsmall - cell lung cancer are shown , together with the levels of carcinoembryonic antigen ( cea ; red diamonds ) and the sum of target lesions by response evaluation criteria in solid tumors ( recist ) 1.1 ( blue squares ) over time during treatment . 
the estimated levels of ret target inhibition at the 50% inhibitory concentration ( ic50 ) and 90% inhibitory concentration ( ic90 ) for kif5b - ret and kif5b - ret - v804l were modeled using actual patient human pharmacokinetic parameters ( data supplement )  . 
 ( c ) computed tomographic images of the patients metastatic lung and liver disease before and at the indicated times after initiating treatment with vandetanib ( left three pairs of panels ) or loxo - 292 ( right two pairs of panels )  . 
consistent with this , she experienced a rapid clinical and biochemical response to loxo - 292 , with decreased shortness of breath and reduction in serum carcinoembryonic antigen ( fig 1a )  . repeat imaging after 8 weeks of treatment demonstrated a 48% decrease in measurable tumor burden by recist 1.1 that was maintained after 16 weeks , indicating a conrmed pr ( figs 1a and 1c )  . 
the patient has received loxo - 292 for more than 11 months , is still receiving treatment , and is tolerating therapy well , without dose interruption , and with all treatment - emergent adverse events grade 1 or 2 . case 2 : hereditary ret v804m mtc . 
a 50 - year - old man with hereditary ret v804m multiple endocrine neoplasia 2a and mtc developed primary disease progression despite previous treatment with three anti - ret mkis ( fig 2a )  . before treatment with loxo - 292 , he was highly symptomatic , with abdominal pain from tumor inltration of the liver and severe tumor - related diarrhea . 
consistent with this , serum carcinoembryonic antigen and calcitonin levels decreased rapidly , together with resolution of diarrhea , abdominal distension , and abdominal parepeat imaging after 8 weeks of treatment indicated a complete response by recist 1.1 , which was conrmed after 12 weeks of treatment , with complete resolution of target lymph node lesions and nontarget liver memediastinal tastases and normalization of serum tumor markers ( figs 2c and 2d )  . 
the patients dose was increased to 160 mg twice a day as allowed by the protocol , with doseproportional increases in exposure and continuous more than ic90 ret v804m target coverage ( fig 2b ) , continued complete response , and continued normalization of tumor markers ( fig 2c )  . 
the patient experienced three adverse events : transient grade 3 altered mental status ( sedation ) , judged by the investigator to be related to concomitant treatment with anxiolytic medications and unrelated to loxo - 292 ; grade 1 constipation ; and grade 2 nausea . 
he remains in complete response and is still receiving treatment at more than 20 months after the start of loxo - 292 . loxo - 292 but not anti - ret mkis maintain inhibitory activity against ret gatekeeper mutations preclinically . 
in contrast to mkis , loxo - 292 is predicted to better accommodate the bulky leucine and methionine side chains in the gatekeeper residues without any steric interactions ( fig 3b )  . to determine the impact of ret kinase domain resistance mutations on inhibitor activity , loxo - 292 , vandetanib , and cabozantinib were tested in vitro against the puried wildtype and mutant ret kinase domains ( fig 3c )  . 
at physiologic ( 1 mm ) atp concentration , loxo - 292 had potent inhibitory activity against wild - type ret , ret v804l , and ret v804m kinases . the anti - ret mkis , in contrast , vandetanib and cabozantinib , displayed signicantly reduced activity against ret v804l / m compared with wildtype ret . 
these data demonstrate that loxo - 292 , but not the mkis vandetanib or cabozantinib , maintain potent inhibitory activity against ret gatekeeper mutations . discussion selective tkis targeting actionable kinase alterations have transformed the treatment landscape for several human cancers . 
although acquired resistance to tkis is universal , a detailed molecular understanding of resistance has led to the development of next - generation tkis that have extended disease control and clinical benet in resistant patients.16 , 17 in several instances , initial treatment with the next - generation inhibitor has led to more durable treatment responses than treatment with the rstgeneration tki and has become standard upfront systemic therapy.18 , 19 loxo - 292 combines features of both rstand nextgeneration tkis used to treat other single kinase - driven cancers . 
it is highly potent against and selective for diverse founder activating ret alterations in human cancers , and in preclinical experiments , it overcomes ret v804 gatekeeper mutations , which have been identied in rare patients with acquired resistance to anti - ret mkis . 
for both patients , inhibiintegration of preclinical ret target tory activity with the actual exposures safely achieved at the recommended phase ii dose of 160 mg twice a day allowed more than ic90 calculated target coverage of both wild - type and gatekeeper - mutated ret in patients ( figs 1b and 2b )  . 
 ( b ) pharmacokinetic analysis at steady state after 8 days of treatment with loxo - 292 at a dose of 80 mg , 120 mg , and 160 mg twice a day . 
the estimated levels of ret target inhibition at the 50% inhibitory concentration ( ic50 ) and 90% inhibitory concentration ( ic90 ) for wild - type ( wt ) ret and ret v804m were modeled as in fig 1b . 
the red arrows indicate diffuse inltration of the liver by tumor . lenvat , lenvatinib ; rt , radiation treatment ; vande , vandetanib . treatment with loxo - 292 after the prior mkis has signicantly extended the period of durable clinical and biochemical response and disease control . 
 wirth et al hibiki udagawa honoraria : astrazeneca , chugai pharmaceutical , bristol - myers squibb , ono pharmaceutical , msd , taiho pharmaceutical , amco , abbvie , boehringer ingelheim , daiichi sankyo consulting or advisory role : abbvie , boehringer ingelheim research funding : msd , abbvie , daiichi sankyo , amgen shingo matsumoto honoraria : pzer , novartis , chugai pharma , astrazeneca research funding : chugai pharma ( inst ) , novartis ( inst ) , lilly ( inst ) , merck serono ( inst ) , merck sharp & dohme ( inst ) kevin ebata employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology brian b . 
tuch employment : loxo oncology stock and other ownership interests : loxo oncology consulting or advisory role : kezar life sciences patents , royalties , other intellectual property : biomarkers for ntrk inhibition ; biomarkers for proteasome inhibition edward y . 
zhu employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology michele nguyen employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology steve smith consulting or advisory role : loxo oncology , various patents , royalties , other intellectual property : various patents and applications travel , accommodations , expenses : various lauren m . 
burkard employment : array biopharma , university of colorado hospital ( i ) stock and other ownership interests : array biopharma , pzer , pzer ( i ) james f . 
blake employment : array biopharma stock and other ownership interests : array biopharma patents , royalties , other intellectual property : i am listed as a co - author on approximately 46 patents ( inst ) kevin r . 
brandhuber employment : loxo oncology stock and other ownership interests : loxo oncology , array biopharma travel , accommodations , expenses : loxo oncology steve andrews employment : loxo oncology leadership : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology s . 
michael rothenberg employment : loxo oncology stock and other ownership interests : loxo oncology travel , accommodations , expenses : loxo oncology koichi goto honoraria : bristol - myers squibb , astrazeneca , pzer , chugai pharmaceutical , taiho pharmaceutical , ono pharmaceutical , novartis , eli lilly , boehringer ingelheim , quintiles , merck serono , life technologies , msd , abbvie , riken genesis , nippon kayaku , takeda pharmaceuticals , otsuka pharmaceutical , srl diagnostics consulting or advisory role : otsuka pharmaceutical research funding : msd , astrazeneca , taiho pharmaceutical , chugai pharmaceutical , boehringer ingelheim , ono pharmaceutical , sumitomo dainippon , takeda pharmaceuticals , novartis , daiichi sankyo , kyowa hakko kirin , astellas pharma , eisai , eli lilly , pzer , riken genesis , bristol - myers squibb , merck serono , ignyta , life technologies , research triangle institute d / b / a rti health solutions , janssen , xcoo , loxo oncology no other potential conicts of interest were reported . references ji jh , oh yl , hong m , et al : identication of driving alk fusion genes and genomic landscape of medullary thyroid cancer . 
wells sa jr , robinson bg , gagel rf , et al : vandetanib in patients with locally advanced or metastatic medullary thyroid cancer : a randomized , double - blind phase iii trial . 
j clin oncol 30 : 134 - 141 , 2012 drilon a , rekhtman n , arcila m , et al : cabozantinib in patients with advanced ret - rearranged non - small - cell lung cancer : an open - label , single - centre , phase 2 , single - arm trial . 
lancet oncol 17 : 1653 - 1660 , 2016 lin jj , kennedy e , sequist lv , et al : clinical activity of alectinib in advanced ret - rearranged non - small cell lung cancer . 
j thorac oncol 11 : 2027 - 2032 , 2016 yoh k , seto t , satouchi m , et al : vandetanib in patients with previously treated ret - rearranged advanced non - small - cell lung cancer ( luret ) : an open - label , multicentre phase 2 trial . 
lancet respir med , 5 : 42 - 50 , 2017 lee sh , lee jk , ahn mj , et al : vandetanib in pretreated patients with advanced non - small cell lung cancer - harboring ret rearrangement : a phase ii clinical trial . 
ann oncol 28 : 292 - 297 , 2017 brandhuber bb , haas j , tuch bb , et al : ena - 0490 the development of loxo - 292 , a potent , kdr / vegfr2 - sparing ret kinase inhibitor for treating patients with ret - dependent cancers . 
aacr - nci - eortc international conference on molecular targets and cancer therapeutics , munich , germany , november 29 - december 2 , 2016 oxnard gr , subbiah v , park k , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret fusion + non - small cell lung cancer : an update from asco 2018 . 
wirth lj , cabanillas me , sherman ej , et al : clinical activity of loxo - 292 , a highly selective ret inhibitor , in patients with ret - altered thyroid cancers : an update from asco 2018 . 
drilon ae , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
yang , m , cai j , guo s , et al : rapid conversion to resistance , of a colon pdw with ret - fusion , by ponatinib treatment could potentially be attributed to the introduction of the gate keeper mutation , v804m . 
dagogo - jack i , stevens se , lin jj , et al : emergence of a ret v804m gatekeeper mutation during treatment with vandetanib in ret - rearranged nsclc . j thorac oncol 13 : e226 - e227 , 2018 15 . 
nat commun 9 : 625 , 2018 j anne pa , yang jc , kim dw , et al : azd9291 in egfr inhibitor - resistant non - small - cell lung cancer . 
ou sh , ahn js , de petris l , et al : alectinib in crizotinib - refractory alk - rearranged non - small - cell lung cancer : a phase ii gobal study . 
pao w , miller va , politi ka , et al : acquired resistance of lung adenocarcinomas to getinib or erlotinib is associated with a second mutation in the egfr kinase 2016 293 : 876 - 880 , 2001 domaplos med 2 : e73 , 2005 22 . 
katayama r , khan tm , benes c , et al : therapeutic strategies to overcome crizotinib resistance in non - small cell lung cancers harboring the fusion oncogene eml4 - alk . 
 intratumoral cd3 + and cd8 + t - cell densities in patients with dna mismatch repairdecient metastatic colorectal cancer receiving programmed cell death - 1 blockade sakti chakrabarti , md1 ; lucas j . 
sinicrope , md1 introduction the programmed cell death - 1 ( pd - 1 ) pathway represses type 1 t - helper cell cytotoxic immune responses and is upregulated in many tumors and in their microenvironment . 
blockade of this pathway with antibodies to pd - 1 has led to robust clinical responses in patients with many tumor types , including a subset of metastatic colorectal cancers ( mcrcs ) with decient dna mismatch repair ( dmmr ) .1 the clinical benet of pd - 1 blockade by pembrolizumab in dmmr mcrc was rst reported in a phase ii study in which the objective response rate ( orr ) and immunerelated progression - free survival rate at 20 weeks were 40% ( four of 10 patients ) and 78% ( seven of nine patients ) , respectively.2 expansion of this cohort to 40 patients indicated an orr of 52%.1 among dmmr tumors , mechanisms underlying responsiveness or resistance to pd - 1 blockade remain unknown , 1 and a predictive biomarker has not been identied within this tumor subtype . colorectal cancers ( crcs ) with dmmr have high microsatellite instability ( msi - h ) and are associated with a high mutational burden , neoantigen load , and typically a dense lymphocytic inltrate.3 in a recent report , the densities of cd3 + and cd8 + t cells were found to be signicantly more heterogeneous in dmmr versus procient mismatch repair ( pmmr ) colon cancers and were shown to prognostically stratify patients with both dmmr and pmmr tumors.4 , 5 on the basis of these data , we hypothesized that the responsiveness of dmmr mcrcs to immunotherapy may be related to the extent of inltration . 
tumor response was assessed by radiographic studies using response evaluation criteria in solid tumors ( recist ) version 1.1.6 the study was approved by the institutional review board of mayo clinic . informed consent was obtained from all patients before collection of data and tumor specimens for analysis . tumors were analyzed for mmr protein ( mlh1 , msh2 , msh6 , and pms2 ) expression by immunohistochemistry ( ihc ) or using a polymerase chain reactionbased assay for msi.7 in archival primary colorectal tumor tissues , cd3 + and cd8 + t - lymphocyte staining was performed by ihc ( ventana medical systems , tucson , az ) , and t - cell densities were determined in tumor core ( ct ) and invasive margin ( im ) by automated image analysis ( appendix fig a1 )  . 
analyses of cd3 + and cd8 + density scores and programmed death ligand 1 ( pd - l1 ) expression were performed by investigators blinded to clinical characteristics and patient outcomes . 
density values for cd3 + and cd8 + t cells , calculated by dividing the cell count by the area ( square millimeters ) within ct or im compartments , were used to calculate a density score ( 0 to 100 ) for each marker by compartment ( cd3 + im , cd3 + ct , cd8 + im , and cd8 + ct ) , as previously described.5 pd - l1 protein expression in tumor cells and in tumor - inltrating immune cells was determined by ihc using ventana pd - l1 ( sp263 ) rabbit monoclonal antibody and was graded according to the percentage of tumor cells with membranous pdl1 expression or as the percentage of positive immune cells in the inammatory inltrate.8 patient and tumor characteristics , details of prior treatment , and pembrolizumab response data are listed in table 1 . 
box plots illustrating the distribution of cd3 + and cd8 + t - cell density ( score range , 0 to 100 ) at the tumor core ( ct ) and the invasive margin ( im ) among the responders and nonresponders . 
responders are dened as patients with complete responses ( crs ) and partial responses ( prs ) ; nonresponders are dened as those with stable disease ( sd ) or progressive disease ( pd )  . regimens received was one ( range , one to four regimens ; one regimen in seven patients , two regimens in three patients , and four regimens in two patients )  . 
median follow - up time of the study cohort since initiation of pembrolizumab was 19.5 months ( range , 9 to 41 months ) in all patients , 21 months ( range , 16 to 24 months ) in nonresponders , and 16 months ( range , 9 to 41 months ) in responders . patient radiographic response data were as follows : two complete responses ( crs ) , ve partial responses ( prs ) , four patients with stable disease , and one patient with progressive disease . 
among pembrolizumab - treated patients who had a cr or pr ( n = 7 ) , the median time to response was 12 weeks ( range , 6 to 40 weeks )  . to examine the relationship between t - cell density scores and treatment response , patients were divided into responders ( cr and pr , n = 7 ) and nonresponders ( stable disease and progressive disease , n = 5 ) to pembrolizumab . median values and ranges of cd3 + and cd8 + t - cell density scores at the ct ( cd3 + ct and cd8 + ct ) and im ( cd3 + im and cd8 + im ) in each response category are provided in figure 1 and table 2 . 
all median t - cell density scores were higher in responders than in nonresponders , with score for cd3 + ct ( 74 v 52 , differences that were greatest respectively ) and cd8 + ct ( 88 v 37 , respectively ) , as shown in figure 1 . 
all median t - cell density scores were higher in the patient group in whom disease control was achieved for more than 12 months ( n = 8 ) , with the greatest score difference seen for cd8 + ct ( 88 v 36 for patients with disease control for more than 12 months v less than 12 months , respectively )  . median tumor cell pd - l1 expression was 2% ( range , 1% to 40% ) among responders and 1% ( range , 0% to 60% ) among nonresponders . 
median pd - l1 expression in intratumoral immune cells was 5% for both responders ( range , 2% to 25% ) and nonresponders ( range , 1% to 10% )  . 
of the ve nonresponding patients , one patients tumor underwent testing for a jak2 mutation , which was not detected . discussion the ability to distinguish high versus low immunogenic tumors could enable selection of patients who are more likely to benet from immunotherapy . 
we used an automated analysis of cd3 + and cd8 + tumor - inltrating lymphocyte density quantitation that was initially reported in stage ii colon cancers and found to be signicantly prognostic independent of mmr status.9 more recently , we validated this platform in nearly 600 stage iii colon cancers from a clinical trial of folfox - based adjuvant chemotherapy where cd3 + and cd8 + t - cell densities were shown to prognostically stratify patients with both dmmr and pmmr colon cancers.5 we found that both cd3 + and cd8 + t - cell density scores in ct and im were higher in patients with dmmr tumors who beneted from pembrolizumab , both in terms of objective response rate and duration of disease control . despite variability observed in our small patient cohort , median density scores of t - cell markers were higher in responders versus nonresponders and in those in whom disease control was achieved for more than versus less than 12 months . 
conversely , these response data suggest that lower t - cell densities are associated with immunotherapy resistance in dmmr tumors and are consistent with the reported nding that lower t - cell densities are associated with worse survival in patients with dmmr stage iii colon cancers receiving cytotoxic chemotherapy.5 our data are consistent with the ndings that increased intratumoral cd8 + t cells can predict response to immunotherapy in patients with metastatic melanoma10 and in patients with head and neck cancers.11 median follow - up of 21 months among nonresponders exceeded the median follow - up time of 12.5 months that was reported in the largest published series of patients with dmmr mcrcs treated with pd - 1 blockade.1 in that study , the mean time to the best radiographic response was 7 months , 1 suggesting that our study follow - up time was of sufcient duration to detect response outcomes . studies have shown higher expression of tumor pd - l1 protein in dmmr versus pmmr crcs , 3 and our analysis of the cancer genome atlas database revealed higher pd - l1 mrna levels in dmmr versus pmmr primary colon cancers ( unpublished data )  . 
in the current study of patients with dmmr and msi - h crcs , we found similar median levels of pd - l1 expression on tumor cells and on inltrating immune cells in responders versus nonresponders . studies of crc , expression of pd - l1 has not been shown to be a predictive biomarker , in contrast to data in patients with nonsmall - cell lung cancer . 
furthermore , a phase ii study of patients with dmmr mcrcs treated with pembrolizumab found that the expression of pd - l1 was not signicantly associated with progression - free survival or overall survival.2 insight into responses to antipd - 1 blockade in dmmr colon cancers is suggested by functional analysis in a responding patient in which rapid in vivo expansion of neoantigen - specic t - cell clones that were reactive to mutant neopeptides were found in the tumor.1 immune inltration may reect the tumors clonal evolution during treatment . 
potential causes of immunotherapy resistance include 2 - microglobulin and jak1 / 2 mutations , 12 and in our study , only one of ve nonresponders was tested for a jak2 mutation , which was not detected . 
other potential biomarkers in dmmr tumors such as the elimination of neoepitopes and differences in t - cell clonal diversity and tumor microenvironment proles warrant additional study . it is important to recognize that dmmr and msi - h are predictive biomarkers for responsiveness to immune checkpoint inhibitors . 
tumor mutation burden ( tmb ) may be a promising biomarker and has been studied in relationship to a t - cellinamed gene expression prole across 22 tumor types.13 although tmb and t - cell gene expression signature were poorly correlated , their combination jointly predicted responders to pembrolizumab , suggesting that features of neoantigenicity and t - cell activation.13 using tmb as a biomarker for immunotherapy responsiveness has important limitations in that not all mutations generate neoantigens , the correlation of tmb with neoantigen load is variable , and an established cutoff point remains unresolved.14 they may capture distinct in summary , we observed that higher cd3 + and cd8 + t - cell densities were associated with higher objective response rates and duration of disease control in patients with dmmr mcrc treated with pembrolizumab . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . andrea muranyi employment : roche stock and other ownership interests : roche patents , royalties , other intellectual property : roche travel , accommodations , expenses : roche june clements employment : ventana medical systems stock and other ownership interests : ventana medical systems research funding : ventana medical systems shalini singh employment : ventana medical systems stock and other ownership interests : ventana medical systems patents , royalties , other intellectual property : method of identifying treatment - responsive nonsmall - cell lung cancer using alk as a marker ( inst ) joleen m . 
hubbard consulting or advisory role : bayer ( inst ) research funding : boston biomedical ( inst ) , senhwa biosciences ( inst ) , bayer ( inst ) , merck ( inst ) , taiho pharmaceutical ( inst ) , treosbio ( inst ) , effector therapeutics ( inst ) robert r . 
mcwilliams consulting or advisory role : merrimack ( inst ) , zeno pharmaceuticals , newlink genetics ( inst ) research funding : prism biolab ( inst ) , genentech ( inst ) , novartis ( inst ) , newlink genetics ( inst ) , eli lilly ( inst ) , aduro biotech ( inst ) , pzer ( inst ) , sano ( inst ) , merck ( inst ) , bristol - myers squibb ( inst ) kandavel shanmugam employment : ventana medical systems stock and other ownership interests : roche patents , royalties , other intellectual property : patents ( inst ) travel , accommodations , expenses : ventana medical systems frank a . 
sinicrope stock and other ownership interests : illumina honoraria : imedex , american society of clinical oncology consulting or advisory role : roche ( inst ) , bristol - myers squibb ( inst ) , ventana medical systems ( inst ) , haliodx ( inst ) research funding : ventana medical systems ( inst ) travel , accommodations , expenses : ventana medical systems no other potential conicts of interest were reported . references le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 le dt , uram jn , wang h , et al : pd - 1 blockade in tumors with mismatch - repair deciency . 
n engl j med 372 : 2509 - 2520 , 2015 llosa nj , cruise m , tam a , et al : the vigorous immune microenvironment of microsatellite instable colon cancer is balanced by multiple counter - inhibitory checkpoints . 
cancer discov 5 : 43 - 51 , 2015 pag `es f , mlecnik b , marliot f , et al : international validation of the consensus immunoscore for the classication of colon cancer : a prognostic and accuracy study . 
lancet 391 : 2128 - 2139 , 2018 yoon hh , shi q , heying en , et al : intertumoral heterogeneity of cd3 + and cd8 + t - cell densities in the microenvironment of dna mismatch - repair - decient colon cancers : implications for prognosis . 
eur j cancer 45 : 228 - 247 , 2009 sinicrope fa , mahoney mr , smyrk tc , et al : prognostic impact of decient dna mismatch repair in patients with stage iii colon cancer from a randomized trial of folfox - based adjuvant chemotherapy . 
j clin oncol 31 : 3664 - 3672 , 2013 el jabbour t , ross js , sheehan ce , et al : pd - l1 protein expression in tumour cells and immune cells in mismatch repair protein - decient and - procient colorectal cancer : the foundation study using the sp142 antibody and whole section immunohistochemistry . 
j clin pathol 71 : 46 - 51 , 2018 gibbs ph , hutchinson r , tran b , et al : immune prole and survival outcomes in stage 2 colon cancer . 
partlov a s , bou cek j , kloudov a k , et al : distinct patterns of intratumoral immune cell inltrates in patients with hpv - associated compared to non - virally induced head and neck squamous cell carcinoma . 
 ( a ) hematoxylin and eosin ( he ) stained whole - tissue sections were manually annotated to outline the entire tumor region ( red line ) and demarcate the invasive margin ( orange line )  . 
 ( b and c ) annotations were transferred onto adjacent cd3 + and cd8 + ihc images with an algorithm outlining the invasive margin ( im ; green line ) and core of the tumor ( ct ; red line )  . 
 repeated abscopal effect with radiotherapy and programmed death 1 blockade in mismatch repairdeficient endometrial cancer introduction radiotherapy for cancer has long been valued for its ability to target specific lesions to achieve tumor regression and improve patient symptoms . 
though the effect of radiotherapy is typically limited to its targeted fields , reports have described response in distant tumors a phenomenon termed the abscopal effect.1 prior studies have demonstrated that this effect may be mediated by an enhanced immune response against tumors , 2 possibly elicited by tumor specific antigens released by cancer cells exposed to radiation.3 interest in leveraging the abscopal effect has been revived by recent advances in immunotherapy.4 inhibitors of immune checkpoints , including cytotoxic t - lymphocyteassociated protein 4 ( ctla - 4 ) , programmed death 1 ( pd - 1 ) , and programmed death ligand 1 ( pd - l1 ) , have been shown to induce a strong clinical response in multiple cancer types.5 - 8 also , the us food and drug administration has approved pd - 1 inhibitors for use against any solid tumors that have deficiencies in dna mismatch repair ( mmr ) .9 these treatments block signaling pathways that normally suppress the immune system and thus can unleash a potent antitumor immune response.8 it has been hypothesized that immunotherapies , given their immune - based mechanisms , might synergize with radiotherapy and induce a more consistent and intense abscopal effect . in one early report , a patient with metastatic melanoma was treated with ipilimumab , a ctla - 4 inhibitor , and treatment resulted in significant regression in multiple areas of cancer after radiation was administered to a paraspinal mass.10 the patient had temporally associated increases in activated cd4 + t cells and antibodies against cancer antigens , which supports an immunologic basis for this effect . 
pathology demonstrated grade 1 endometrial adenocarcinoma with myometrial invasion and abnormal peritoneal washings , consistent with stage iiic2 disease per the international federation of gynecology and obstetrics staging syste of note , immunohistochemical studies showed absent expression of the mmr proteins mlh1 and pms2 ( fig 1 )  . the patient was given adjuvant paclitaxel 175 mg / m2 and an area under the curvebased carboplatin target dose of 5 for six cycles , but a subsequent ct scan revealed progression of disease . 
she received six cycles of doxorubicin ( reduced to 50 mg / m2 per cycle for severe neutropenia ) , but the follow - up ct scan showed enlarged pelvic lymph nodes . 
oh young kwang chae author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : young kwang chae , md , mph , mba , department of medicine , northwestern university feinberg school of medicine , robert h . 
at this time , immunotherapy was considered because of data to suggest its efficacy in mmr - deficient tumors.14 meanwhile , the patients performance status deteriorated rapidly , and she was no longer able to ambulate without assistance , in part because cutaneous metastases presented as large fungating masses on her left thigh . 
ultimately , she started nivolumab 3 mg / kg every 2 weeks ; the first cycle occurred 23 months after surgery . two months after nivolumab treatment initiation , a ct scan demonstrated a mixed response , with improved pulmonary metastatic disease but increased pelvic lymph nodes and a nodule of the sigmoid mesentery . 
because of worsening leg pain , the patient was referred to a radiation oncologist and received palliative radiation to her left thigh , which consisted of 25 gy in five fractions via en face photon beams . 
notably , she also experienced decreased size of hepatic masses , sigmoid nodule , and retroperitoneal and pelvic lymphadenopathy . ct obtained 2 months afterward concerningly showed progression of the sigmoid nodule and pelvic lymphadenopathy as well as marked growth of a splenic lesion and a 7 - cm l3 vertebral metastasis that was causing significant back pa the patient was again referred for palliative radiotherapy and received 20 gy to the lumbar spine in five fractions using conventional anterior - posterior / posterior - anterior ( appa ) technique . 
clinically , the patients back pain significantly improved ; with the aid of physical therapy , she was able to ambulate independently agahowever , the patient developed recurrent difficulties with walking , and progression of a nodal mass in the left external iliac chain was discovered . 
a repeat ct scan showed reduction in this mass as well as response in the hepatic and splenic masses to near resolution . by this time , it was noted that the patient had exhibited a presumed abscopal effect after each of her radiation treatments ( fig 2 )  . 
 ( a ) metastases targeted by radiotherapy ( rt ) were in the ( 1 ) left thigh ; ( 2 ) l3 vertebra ; ( 3 , 4 ) left external iliac chain ; and ( 5 ) bladder , as identified by red circles on computed tomography ( ct ) images . 
 ( b ) ct images of liver metastases ( gold circle and arrow ) , which were located on an axial plane distinct from any radiation fields , showed response to rt treatments ( numbered as in [ a ] )  . 
the patient did develop hematuria and dysuria consistent with radiation - induced grade 2 cystitis , but she otherwise continues to tolerate nivolumab without high - grade toxicities . discussion we describe here the case of a patient with widely metastatic endometrial cancer who exhibited abscopal responses after multiple rounds of palliative radiotherapy while on nivolumab . 
this patient experienced disease response to five separate radiotherapy treatments with concurrent pd - 1 blockade , which yielded an ongoing survival benefit that lasted longer than 28 months as of this writing . abscopal effects are difficult to clearly identify , because multiple factors affect patient response . 
 for example , tumor shrinkage after the first radiotherapy treatment may have represented a delayed effect of nivolumab , which can cause pseudoprogression before a definite clinical response.15 the repeated benefit with radiotherapy in this case , however , suggests the presence of a true abscopal effect . 
however , one clinical trial showed that the use of ipilimumab with pelvic radiotherapy for prostate cancer did not result in a greater than - expected increase in toxicities.16 a retrospective analysis of 133 patients with various cancer types who received both immunotherapy and radiotherapy similarly did not uncover an increase in major adverse effects.17 thoughtful and judicious use of these treatments , even in a repeated fashion , may be tolerated by many patients . not all patients treated with radiotherapy exhibit an abscopal effect , and such an effect may be dependent on patient - specific immune parameters . 
for example , this patients primary tumor exhibited mmr deficiency , which is a possible sensitizing factor to radiotherapy , 18 presumably because the ability of cancer cells to repair dna damage inflicted by radiation is reduced.19 in addition , mmr deficiency has been associated with an increase in tumor mutations and tumor - specific neoantigens.9 this attribute may be beneficial in the context of a desired abscopal effect , because radiotherapy could amplify the immunogenic stimulus provided by these neoantigens . 
 relevant studies have almost exclusively been performed in preclinical models , but this evidence suggests that concurrent radiotherapy and immunotherapy is more beneficial than sequential administration.20 the ideal dosing regimen to achieve an abscopal effect also remains undetermined , but one study that used mouse models of breast and colon cancer showed that a fractionated strategy was superior to a single large dose.21 although these approaches certainly were effective in our patient , forthcoming data from prospective trials are awaited.22 our report adds to the overall evidence in support of an abscopal effect , and it raises the possibility that immunotherapy can be periodically boosted by radiotherapy ; however , additional studies are needed to validate such an approach . 
sharabi ab , nirschl cj , kochel cm , et al : stereotactic radiation therapy augments antigenspecific pd - 1 - mediated antitumor immune responses via cross - presentation of tumor antigen . 
herbst rs , baas p , kim d - w , et al : pembrolizumab versus docetaxel for previously treated , pdl1 - positive , advanced nonsmall - cell lung cancer ( keynote - 010 ) : a randomised controlled trial . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinumbased chemotherapy : a single - arm , multicentre , phase 2 trial . 
kwon ed , drake cg , scher hi , et al : ipilimumab versus placebo after radiotherapy in patients with metastatic castration - resistant prostate cancer that had progressed after docetaxel chemotherapy ( ca184 - 043 ) : a multicentre , randomised , double - blind , phase 3 trial . 
bang a , wilhite tj , pike lrg , et al : multicenter evaluation of the tolerability of combined treatment with pd - 1 and ctla - 4 immune checkpoint inhibitors and palliative radiation therapy . 
martin lm , marples b , coffey m , et al : dna mismatch repair and the dna damage response to ionizing radiation : making sense of apparently conflicting data . 
dewan mz , galloway ae , kawashima n , et al : fractionated but not single - dose radiotherapy induces an immune - mediated abscopal effect when combined with antictla - 4 antibody . 
it also re - examines some of the conventional wisdom that previously dominated clinical trial design and discusses development and internal validation of a predictive biomarker as a new paradigm for optimizing the intended - use subset for a treatment . 
some previous paradigms for clinical trial design can limit the development of more effective methods on the basis of prospectively planned adaptive methods , but useful new methods have been developed for analysis of genome - wide data and for the design of adaptively enriched studies . 
in many cases , the heterogeneity of populations eligible for clinical trials as traditionally dened makes it unlikely that molecularly targeted treatments will be effective for a majority of the eligible patients . 
with the completion of the human genome project and the initiation of large dna sequencing of human tumors , somatic mutations were discovered that accounted for the invasion and progression of cancers . 
it became evident that the traditional tumor classications on the basis of site and histologic type were inadequate for developing therapeutics . the discovery of somatic mutations led to major changes in the development of oncology drugs . 
the focus of oncology drug development switched to developing inhibitors of mutated protein kinases and blocking the protein products of amplied receptors . the new strategies of drug discovery required new strategies for clinical trial design . 
the traditional assumption that qualitative interactions are unlikely was frequently shown to be wrong . at about the same time , new whole - genome assays such as rna transcript microarrays , copy number microarrays , and methylation arrays were becoming available . 
the resulting statistical methods were based on classication and prediction , which enabled the development of classiers on the basis of high - dimensional assays for predicting prognosis and response to therapy for individual patients.3 , 4 this article will highlight some of the important developments in clinical trial design and classication analysis that have been stimulated by the dramatic changes in oncology drug development . 
 simon context key objective to describe new and innovative methods for discovering and using predictive biomarkers to develop effective treatments in the presence of patient heterogeneity . knowledge generated a method was developed for discovering and validating therapeutically relevant patient subsets using a new paradigm on the basis of predictive classication rather than multiple hypothesis testing . 
with the development of drugs targeted to specic genomic alterations , attention has shifted to phase ii studies with eligibility determined by specic genomic alterations rather than histologic type , the so - called basket clinical trial.5 - 9 large basket trials include multiple drugs , each with a targeted genomic alteration . 
patients have their tumors sequenced , and then they are assigned the drug appropriate to the genomic alteration found in their tumor . basket trials have generally been sized by using standard methods either for inference on the basis of all patients with the genomic alteration histologic type or for separate inference for each histologic type . 
recently , bayesian designs have been developed that attempt to share response information among histology baskets for patients whose tumor contains the same genomic alteration.10 some of these are based on hierarchical models of treatment effects . 
however , cunanan11 has shown that the prior distributions for such designs must be chosen carefully or the false - positive error for some histology baskets may be highly inated . 
if the accumulating information indicates homogeneity of response probabilities , then the baskets are essentially pooled and a small sample size sufces . cunanan12 developed a frequentist design on the basis of two - stage sampling . 
otherwise , sampling and inference are conducted independently for the baskets . the platform design is for settings with multiple treatments and multiple candidate biomarker strata.13 the design is based on the assumption that the candidate biomarkers are the same for each drug , which somewhat limits the realm of applications . 
most platform designs are bayesian designs and the term promising is interpreted to mean that the posterior probability of a positive phase iii trial is at least 80% . in a platform design , a patient is initially randomly assigned with equal probability to receive any of the drugs . 
the objective is to nd candidates for phase iii trials with a smaller total sample size than would be required for conducting a separate simon two - stage optimal trial in each of the strata.14 the bayesian models used are generally based on hierarchical modeling.13 , 15 freidlin et al16 developed a simpler phase ii trial design for a single drug with a single binary biomarker . 
 statistical methods for biomarker - driven clinical trials simon and maitournam17 , 18 studied the number of patients needed to screen and randomize for the enrichment design compared with a standard design , in which the assay is not performed . 
they found that the enrichment design generally requires many fewer randomly assigned patients . they showed that the ratio of number of required randomly assigned patients was approximately ( cid : 1 ) nenrichment nstandard ( cid : 1 ) te + + ( 1 ) te ( cid : 3 ) 2 where te + and te are the treatment effects in mutationpositive and mutation - negative patients , respectively , and denotes the proportion of mutation - positive patients . 
this formula indicates that the randomization ratio equals the reciprocal of the square of the treatment effects in the two trial designs . if the treatment effect in mutation - negative patients is zero , then the randomization ratio equals 2 . 
if the treatment effect in the mutation - negative patients equals half that in mutationpositive patients , then the randomization ratio becomes { + ( 1 ) / 2 } 2 , so if = 0.5 , then the randomization ratio equals 9 : 16 , and the enrichment design requires slightly more than one half the number of patients as the standard design . adaptive determination of the intended - use population the efciency of the enrichment design highlights the critical relationship between the required size of a phase iii clinical trial and the target treatment effect . 
simon et al19 developed a focused approach for using such archived tissues called the prospective - retrospective study design , which was used for establishing that patients with advanced colorectal cancer do not benet from anti - egfr antibodies if their tumors contain a mutation in the kras gene.20 this approach was also used in a structured manner in the development of the oncotype dx recurrence score as a prognostic and predictive signature for patients with stage i and stage ii breast cancer.21 in addition to using archived samples from a failed randomized controlled trial ( rct ) , adaptive methods have been developed for prospective design of an rct in a statistically rigorous way to adaptively identify the subset of patients who benet from the test treatment . 
some of these adaptive methods will be discussed , but their use has required regulators and clinical trialists to accept that the intended - use population need not be the full eligible population . by prospectively allocating some of the type i error rate to a planned subset analysis , 22 we do not need to use the convention that subset analysis should be performed only if the all - comers analysis is signicant or if there is a statistically signicant interaction . 
statisticians and clinical investigators have sometimes been slow to shed some of the conventional wisdom of the previous paradigm , such as the requirement that the intended - use population must be the eligible population . adaptive enrichment single binary candidate biomarker . 
the most common type of adaptive enrichment in phase iii trials involves whether to use a binary candidate biomarker to restrict eligibility . initially patients are characterized with regard to the biomarker and then randomly assigned to the test treatment or control , but the biomarker is not used to restrict eligibility . 
at some point during the trial an interim analysis is performed and one of three decisions is made : ( 1 ) the entire trial is closed for futility , ( 2 ) the trial continues accruing without any restriction on eligibility until its originally planned sample size is reached , or ( 3 ) accrual is continued only for biomarker - positive patients . 
in the third case , the total target accrual may be increased to adequately power the nal analysis for biomarker - positive patients . several authors have proposed designs for the binary biomarker case described previously.23 - 32 they contain multiplicity adjustments to account for the fact that inferences are being made for the treatment effect overall and for biomarker - positive patients . 
in many cases , there is a quantitative or semiquantitative biomarker that is thought to be predictive of which patients are most likely to benet . often , previous studies have not reliably established the relationship between biomarker value and likelihood of benet , and there is no adequately determined cut point for positivity . 
a recent example is the programmed deathligand 1 ( pd - l1 ) level of expression on nonsmall - cell lung tumors as a predictor of response to t - cell checkpoint therapy . because of regulators requirements that sponsors demonstrate statistically signicant effectiveness of the treatment of an intended - use population , most sponsors want to have the intended - use population dened at the outset . this may require using a cut point selected on the basis of inadequate phase ii trials . 
 simon of the relationship between biomarker level and treatment effectiveness . biomarkers , not for settings in which whole - genome data are used for classier development . there are only a few cases in which investigators use an adaptive design to determine an optimal cut point on the basis of interim data , perhaps because they are unaware of the new statistical designs that may achieve this in a statistically valid manner . jiang et al34 showed how one could test the null hypothesis of no treatment effect using a minimal p value statistic for which a p value for treatment effect is computed for the cases above each of the candidate cut points . 
their proposed analysis is performed at the end of the trial using the full data set and is based on the null distribution of the min - p - value statistic . 
this approach is easy to implement because it does not require any changes during the trial . the intended - use population is adaptively determined at the end of the trial . is adaptive in that simon and simon35 illustrated the use of their adaptive enrichment approach for modifying eligibility during the trial on the basis of an interim analysis of the relationship of biomarker value to treatment effect . 
the signicance test preserves the type i error , regardless of the strategy used for modifying eligibility . although the method is frequentist , they advocate using a bayesian model for selecting features and building the classier at interim analyses.33 the bayesian model can also be used for selecting an intended - use population . one of the questions about using adaptive enrichment is how to estimate the treatment effect in the adaptively selected intended - use population in an unbiased manner . simon and simon36 described how to use bootstrap resampling in an unbiased manner to estimate treatment effects for the intended - use population using data from periods that also determined how to modify eligibility . 
one approach involves developing separate prognostic scores for the active treatment group ( eg , h ( x ; a ) for the log hazard ratio relative to baseline hazard for a patient with covariate vector x receiving the active treatment ) and the control group ( h ( x ; c ) )  . 
that is , if the hazard of a failure event on treatment a is less than the hazard of that event on the control by a tolerance of at least c for a patient with baseline covariate vector x , then the predictive biomarker is considered to have value 1 , and otherwise to have value 0 . 
instead of using proportional hazards modeling as suggested here , one could use other methods such as random forest modeling37 or any other method of prognostic modeling . a major feature of the new paradigm for subset analysis introduced by the adaptive signature design ( asd ) is that nding an appropriate intent - to - treat subpopulation should be treated as a classication problem , not as a hypothesistesting problefinding a subset with a large apparent treatment effect is of little value because the resubstitution estimate of treatment effect is so often optimistically biased . the asd and cross - validated asd ( cv - asd ) provide unbiased estimates and tests of such treatment effects . simon38 described sensitivity , specicity , positive predictive value ( ppv ) , and negative predictive value ( npv ) for predictive classiers with survival time outcome . 
when the survival time for active treatment versus control has proportional hazards for classier - positive and classier - negative patients , then the ppv can be written38 ppv ( cid : 1 ) 1 + + where + denotes the hazard ratio of control versus active treatment of classier - positive patients . 
us food and drug administration ( fda ) guidance on the use of enrichment strategies describes the asd in a positive manner.42 practical experience in designing a clinical trial using the asd is described by sher et al , 43 simon , 44 and mi.45 where + denotes the prevalence of classier - positive patients . 
the asd and cv - asd to be described in a later section were originally described in terms of a specic kind of classier for gene expression data , but the concept is quite general and will be described here in its generality . 
it is not limited to high - dimension genomic data or signatures of gene expression measurements ; is best used with a moderate number of candidate predictive biomarkers . in fact , at the nal analysis , the patients randomly assigned in the clinical trial are randomly partitioned into a training set and a validation set . 
a predictive classier is developed by using only training set data . with the asd , however , one is permitted to develop only a single predictive classier , and it must be completely specied before the validation set data are used in any way . finally , the patients in the validation set are classied as likely to benet from the active treatment ( f ( x ) = 1 ) or not ( f ( x ) = 0 )  . 
the set of covariate vectors for which f ( x ) = 1 is considered the intended - use subset s : s = { x : f ( x ) = 1 }  . although the asd provides a new paradigm for subset analysis of rcts , its statistical power is limited because of the sample splitting . 
freidlin et al46 introduced an improved method called the cv - asd with improved power establishing the signicance of the treatment effect in the adaptively determined intended - use subset . 
we denote the resulting predictive classier as c ( a , d ) where d denotes the complete data set . the resubstitution estimator of treatment effect is denoted ( c ( a , d ) , d ) where the operator computes the empirical treatment effect on the subset of d for which classier c is positive . 
this new training starts from scratch ; that is , it does not use the feature selection steps of development of the full sample classier c . let ck ( a , dk ) denote the classier developed on dk . 
i is the prevalidation classication of patient i . having developed a single predictive classier using training data , the next step is to evaluate the treatment effect for patients in the validation set with covariate vectors in s . 
outcomes of those who received active treatment are compared with outcomes of those who received the control . because the validation set was not used to develop the classier , this comparison of outcomes is unbiased . after completing all k - folds of the cross - validation , all of the cases have been classied once . 
these { i } are called prevalidated indicators of the intended - use subset.47 let iu = { i : i = 1 } , the intended - use subset on the basis of the prevalidated predictive classications . 
 simon empirical treatment effect in iu , and take that as an approximation for the treatment effect in using the full sample classier c ( a , d ) with new cases in the future . 
simulation studies have shown that this estimator is much better than the resubstitution estimator but somewhat conservative.46 a statistical signicance test for treatment effect among future patients classied positive using c ( a , d ) is approximated by computing the permutation distribution of ( iu )  . for each permutation of the treatment labels , the crossvalidation procedure is repeated giving a new iu , say iu ( cid : 4 ) , and a new value of ( iu )  . 
with many permutations of the treatment labels , one can approximate the null distribution . the null hypothesis here is that there is no subset for which there is a positive treatment effect . 
zhang et al48 describe an alternative approach to de - biasing the resubstitution estimator ( c ( a , d ) , d ) using bootstrap sampling instead of using prevalidated classication . other phase iii designs zhao et al49 describe a method for using the results of a previous clinical trial of a treatment and control to select a subset of patients for a new rct . 
for higher - dimensional data , the authors recommend sample splitting or cross - validation to separate the development of predictive scores from the evaluation of the outcome difference in the selected patients . 
the authors assume that feature selection does not use the clinical trial data because a partial cross - validation approach in which feature selection is not repeated for each resampling is described and can be highly biased when feature selection uses the data.50 foster et al37 describe a method very similar to the cv - asd for binary outcome data in which the random forest method is used for developing prognostic prediction function in the active treatment and control groups . 
they also investigate bootstrap resampling to estimate the treatment effect in the selected subset . cv - asds are quite general with regard to the type of models used for predicting difference in expected outcome between treatment groups as a function of the covariate vector . 
these treatment effect estimates may be biased if the assumed parametric model is misspecied , however . outcome weighted learning is an approach to developing approximately optimum individualized treatment rules that are robust to model misspecication.51 , 52 sequentially adaptive interventions are multistage treatto tailor a sequence of ment strategies that attempt treatment interventions to the characteristics of individual patients and their responses to previous treatments . 
such a score can be based on the difference between a prognostic risk function ft ( x ) trained on the treatment group and a prognostic risk function fc ( x ) trained on the control group , where x denotes the vector of measured covariates . 
using the k - fold cross - validation approach of the cv - asd , these functions can be developed on dk training sets and used to compute prevalidated predictive scores ft ( xi ; dk ) fc ( xi ; dk ) for the cases in the withheld sets dk . 
these prevalidated predictive scores si being quantiles are thus in the range ( 0 , 1 )  . matsui et al55 suggest that these prevalidated scores be used as the independent variable in a proportional hazards model containing a main effect of the treatment and an interaction between treatment and prevalidated predictive score quantile . 
for any test statistic involving the estimated treatment effect scores , the null hypothesis of no treatment effect can be performed by permuting the treatment labels and repeating the cross - validation procedure . 
predictions for future patients require rst computing the predictive index quantile score for the new patient using quantiles of the full data set and then plugging that value into the tted proportional hazards model . cai et al56 described a two - stage procedure for estimating a predictive score . 
for high dimensional their approach is probably best used with covariates , prevalidated predictive scores . discussion the development of personalized oncology has been a consequence of the discovery of somatic driver mutations in tumors . 
development of drugs and companion diagnostics for inhibiting driver mutations has provided many two decades . therapeutic successes during the past complex statistical methods have not been necessary for developing predictive biomarkers in these cases because the presence of is the biomarker . the mutation itself however , most somatic mutations are not driver mutations , and identication of predictive biomarkers in those cases can be much more difcult . 
consequently , the fda developed a regulatory pathway in which the diagnostic was not labeled as distinguishing patients who are likely to benet from the drug from those who are not , but rather for identifying patients who have a tumor containing the mutation that makes them eligible for the approved drug . 
during the past two decades , numerous drugs and companion diagnostics for patients with cancer have been approved on the basis of the enrichment design . the question of whether to restrict eligibility to a phase iii trial on the basis of a binary biomarker or on the basis of the value of a quantitative biomarker frequently arises in the design of pivotal trials . 
having larger phase ii trials would provide better evidence for designing phase iii trials , but often the phase iii design decisions are made on the basis of insufcient phase ii data . 
the adaptive designs described in which eligibility is not initially restricted but may subsequently be restricted to biomarker - positive patients on the basis of a prespecied interim analysis are widely applicable . 
more general adaptive enrichment designs with multiple candidate biomarkers can be effective if markers are sufciently powerful their effects on outcome can be discovered at interim analyses . that the asd and cv - asd are easy to use because they do not require any eligibility changes during the course of the trial . they are adaptive in the sense that the intended - use population is adaptively determined by the trial data . however , because they do not adapt eligibility , the opportunity for power gains is limited . 
the cv - asd has much better power and is appropriate for settings in which strong candidate biomarkers are not known at the start of the trial . analyzing phase iii trials by using a continuous score biomarker that reects relative treatment effectiveness can provide medically useful information without the arbitrariness of specifying a cut point . 
it is important , however , to internally validate the calibration of the scoring function by using resampling methods as described here . trials for nding optimal dynamic regimes for clinical multistage decision making have not yet found much application in oncology but have been used effectively in other areas . some of the conventional wisdom that has guided the design and analysis of phase iii trials is undergoing reevaluation . 
for example , the paradigm of broad eligibility and the use of subset analysis on the basis of multiple hypothesis testing require re - evaluation . is not always for molecularly targeted treatments , reasonable to expect a signicant treatment effect for all eligible patients dened by using conventional histology and stage criteria . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . richard simon consulting or advisory role : abbvie pharmaceuticals , amgen biotechnology , janssen pharmaceuticals , bristol - myers squibb , pzer , onconano medicine travel , accommodations , expenses : amgen references talpaz m , silver rt , drucker bj , et al : imatinib induces durable hematologic and cytogenic responses in patients with accelerated phase chronic myeloid leukemia : results of a phase 2 study . 
blood 99 : 1928 - 1937 , 2002 slamon dj , leyland - jones b , shak s , et al : use of chemotherapy plus a monoclonal antibody against her2 for metastatic breast cancer that overexpresses her2 . 
new york , ny , chapman and hall / crc , 2015 antonijevic z , beckman ra ( eds ) : platform trial designs in drug development : umbrella trials and basket trials . 
new york , ny , chapman and hall / crc , 2018 berry sm , broglio kr , groshen s , et al : bayesian hierarchical modeling of patient subpopulations : efcient designs of phase ii oncology clinical trials . 
clin trials 10 : 720 - 734 , 2013 simon rm : primary site independent clinical trials in oncology , in antonijevic z , beckman ra : platform trial designs in drug development : umbrella trials and basket trials . 
bokemeyer c , kohne c , rougier p , et al : cetuximab with chemotherapy ( ct ) as rst - line treatment for metastatic colorectal cancer ( mcrc ) : analysis of the crystal and opus studies according to kras and braf mutation status . 
paik s , tang g , shak s , et al : gene expression and benet of chemotherapy in women with node - negative , estrogen receptor - positive breast cancer . 
biom j 51 : 358 - 374 , 2009 jenniso c , turnbull bw : conrmatory seamless phase ii / iii clinical trials with hypotheses selection at interim : opportunities and limitations . 
stat med 32 : 2695 - 2714 , 2013 jenkins m , stone a , jennison c : an adaptive seamless phase ii / iii design for oncology trials with subpopulation selection using correlated survival endpoints . pharm stat 10 : 347 - 356 , 2011 30 . 
biostatistics 19 : 27 - 41 , 2018 jiang w , freidlin b , simon r : biomarker - adaptive threshold design : a procedure for evaluating treatment with possible biomarker - dened subset effect . 
bai x , tsiatis aa , lu w , et al : optimal treatment regimes for survival endpoints using a locally - efcient doubly - robust estimator from a classication perspective . 2003 lifetime data anal 23 : 585 - 604 , 2017 52 . 
a recent retrospective analysis found a clear association of improved survival with continuation of endocrine therapy upon diagnosis of brain metastases.10 remarkably , the cdk4 / 6 - inhibitor abemaciclib had a clinical benet rate of 25%.11 preclinical models of bc brain metastases suggest pi3k pathway inhibition may be effective for treatment of brain metastases.12 notably , both sandpiper and solar - 1 excluded patients with untreated or active cns metastases6 , 7 ; however , the precursor to alpelisib , buparlisib , did have brain penetration , which was thought to be the cause for the higher incidence of mood disorders.13 an increase in depression has distinctly not been seen with the - specic pi3kinhibitor alpelisib and , in preclinical animal models with intact blood - brain barrier , no signicant distribution into the brain was seen ( unpublished data )  . thus , the activity of alpelisib in brain metastases is unknown . herein , we report a case series of 4 patients with er + / progesterone receptorpositive ( pr + ) / her2 metastatic bc with progressive brain metastases ( fig 1 ) treated with alpelisib . 
all patients provided consent to publish their information and images . case 1 a 55 - year - old woman presented with a large breast ulceration , biopsy specimendiagnosed invasive ductal carcinoma ( idc ) , grade 3 , er + / pr + / her2 . computed tomography ( ct ) scan revealed pulmonary nodules , osseous lesions , and hypodense lesions within the right hepatic lobe . 
brain magnetic resonance imaging ( mri ) showed a 10 - mm mass in the left cerebellar hemisphere ; this was treated with stereotactic radiosurgery with initial shrinkage to 8 mm and stabilization on follow - up . 
brain mri showed an increase of the left cerebellar lesion to 12 mm , judged by neuroradiology and radiation oncology to be more compatible with progression than with radiation - induced tissue necrosis . 
the patients body mass index ( bmi ) was 25 ( calculated as kilograms divided by square of height in meters ) and eastern cooperative oncology group ( ecog ) performance status ( ps ) score of 0 . 
brain mri after 6 weeks showed a reduction in the left cerebellar lesion to 9 mm ( 62% reduction of bidimensional areas , 35% reduction of sum of longest distances )  . 
follow - up mri 2 months later revealed stability of the cns lesion . subsequent brain mri at 3 , 4 , and 6 months showed stable disease without changes in measurements . 
this was compatible with a partial response per response in neuro - oncology brain metastases assessment ( rano - bm ) criteria.14 case 2 a 71 - year - old woman was diagnosed in 2010 with pt2n0 idc of the right breast , grade 3 , er + / pr + / her2 . 
in 2017 , she had a recurrence in the right breast , pleural effusion , and bone metastases and was treated with multiple regimens : letrozole and palbociclib , fulvestrant and palbociclib , and capecitabine and paclitaxel . 
she was serially treated with fulvestrant and palbociclib , radiation to the base of skull to treat cranial nerve symptoms , and with exemestane and everolimus , capecitabine , and abemaciclib . 
for the rst time , brain mri demonstrated multiple parenchymal metastases and she was treated with hippocampal - sparing wbrt . subsequently , treatment was changed from abemaciclib to liposomal doxorubicin for progression in the brain , followed by gemcitabine . 
brain mri 6 weeks later demonstrated a 14% reduction in the sum of longest distances of measurable brain metastases ( 24% reduction in bidimensional areas ) and regressions of nonmeasurable brain metastases . 
the most recent brain mri at the 6 - month mark revealed progressive parenchymal disease requiring change of therapy . case 4 a 70 - year - old woman was diagnosed in 2013 with t1n1 idc of the right breast , grade 3 , er + / pr + / her2 . 
she was treated with breast - conserving surgery , adjuvant docetaxel plus cyclophosphamide , radiation , and anastrozole . 2018 , metastatic disease developed to the lung , liver , and bone while she received adjuvant anastrozole . 
follow - up mri demonstrated at least 15 new intraparenchymal lesions and several progressing dural - based lesions , so the patient proceeded to undergo wbrt and restarted capecitabine therapy . 
examination of a liquid biopsy specimen revealed multiple pi3k mutations ( pik3ca : h1047r , e81k , and e563k ) and she was administered alpelisib ( 300 mg ) table 1 . 
restaging after 6 weeks of therapy revealed substantial disease regression in the lungs and liver as well as interval resolution of punctate cerebellar and cerebral metastasis and reduction of a dural metastasis ( appendix fig a1 ) , compatible with stable disease per rano - bm criteria.14 repeated brain mri at the 3and 5month marks showed stable disease . discussion activating pik3ca mutations occur early in breast carcinogenesis and are typically not lost or acquired during clonal evolution in later stages of the diseasefeatures that suggest these are driver mutations . 
table 1 provides a summary of mutational prole and previous treatments . cases 1 and 2 harbored the activating mutation pik3ca h1047r in the coding exon 20 , a kinase - activating mutation and the most common mutation in bc.14 case 1 also had pik3c2b amplication , which occurs in 13% to 25% of patients.15 pik3c2b is a class ii pi3 - kinase.16 whether its amplication in conjunction with pik3ca mutation deepens or attenuates pi3k - pathway dependence of cancer and whether pik3c2bs kinase activity is inhibited by alpelisib is unknown . 
however , understanding this relationship appears to be important because activating pik3ca mutations and copy number gain of pik3c2b do co - occur in bc.15 case 3 harbored the pik3ca e545k mutation , affecting the helical domain of p110that activates signaling because of its detachment from the inhibitory p85 subunit of pi3k.17 helical domain mutations are the second most frequent in bc , with an incidence of 6.4%.14 case 4 had 3 mutations in pik3ca ; e81k and h1047r are activating mutations and e563k is novel . 
this combination of a major ( h1047r ) and a minor ( e81k ) pik3ca mutation is thought to amplify pi3k signaling and predict for responsiveness to pi3k inhibition.18 this patient had a comutation of pik3ca mutations and esr1 . 
the earlier pan - pi3k inhibitor buparlisib was tested in 4 patients with treatment - refractory cns lymphoma , 1 of whom achieved a partial remission.23 in animal models , systemically administered buparlisib showed activity against bc brain metastases.24 - 26 patients with active brain metastases were excluded from the pivotal solar - 1 and sandpiper studies.6 , 7 conclusions from our observations are limited by the small number of patients selected on the basis of their surprising response . 
the rano - bm criteria consider lesions , 10 mm as nonmeasurable.14 here , we show examples with resolution of small lesions , which are clinically meaningful but classied as stable disease per the criteria . 
additional investigation to prospectively evaluate alpelisib in patients with bc and cns involvement may be justied . in conclusion , we have described cases of regression or stabilization of progressive cns lesions in patients with hr + / her2 metastatic bc treated with the pi3k inhibitor alpelisib . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . stacy moulder research funding : oncothyreon ( inst ) , pzer ( inst ) , novartis ( inst ) , genentech ( inst ) , takeda ( inst ) , bayer ( inst ) , emd serono ( inst ) , genentech ( inst ) eric p . 
winer stock and other ownership interests : verastem honoraria : roche , genomic health consulting or advisory role : leap therapeutics , seattle genetics , jounce therapeutics , glaxosmithkline , carrick therapeutics , eli lilly , genomic health , g1 therapeutics research funding : genentech ( inst ) , novartis ( inst ) hope s . 
rugo consulting or advisory role : ionis , celtrion research funding : macrogenics ( inst ) , obi pharma ( inst ) , eisai ( inst ) , pzer ( inst ) , novartis ( inst ) , eli lilly ( inst ) , genentech ( inst ) , merck ( inst ) , immunomedics ( inst ) , odonate therapeutics ( inst ) , daiichi sankyo ( inst ) , seattle genetics ( inst ) travel , accommodations , expenses : pzer , puma biotechnology , mylan , amgen , astrazeneca , macrogenics , daiichi sankyo , merck , novartis , obi pharma open payments link : nancy u . 
lin consulting or advisory role : roche , seattle genetics , puma biotechnology , novartis , daiichi sankyo research funding : genentech , pzer , seattle genetics , merck patents , royalties , other intellectual property : royalties for chapter in upto - date regarding management of breast cancer brain metastases , royalties from jones & bartlett gerburg m . 
wulf stock and other ownership interests : selecta biosciences ( i ) research funding : merck patents , royalties , other intellectual property : pin1 as a marker for abnormal cell growth ( patent no . : 8129131 ) no other potential conicts of interest were reported . references cancer genome atlas network : comprehensive molecular portraits of human breast tumours . 
nature 490 : 61 - 70 , 2012 loi s , michiels s , baselga j , et al : correction : pik3ca genotype and a pik3ca mutation - related gene signature and response to everolimus and letrozole in estrogen receptor positive breast cancer . 
genes chromosomes cancer 52 : 69 - 80 , 2013 ramirez - ardila de , helmijr jc , look mp , et al : hotspot mutations in pik3ca associate with rst - line treatment outcome for aromatase inhibitors but not for tamoxifen . 
breast cancer res treat 139 : 39 - 49 , 2013 kalinsky k , jacks lm , heguy a , et al : pik3ca mutation associates with improved outcome in breast cancer . 
clin cancer res 15 : 5049 - 5059 , 2009 baselga j , cortes castan j , de laurentiis m , et al : sandpiper : phase iii study of the pi3 - kinase ( pi3k ) inhibitor taselisib ( gdc - 0032 ) plus fulvestrant in patients ( pts ) with oestrogen receptor ( er ) - positive , her2 - negative locally advanced or metastatic breast cancer ( bc ) enriched for pts with pik3ca - mutant tumours . 
ann oncol 27 : vi99 , 2016 ( suppl 6 ) andr e f , ciruelos e , rubovszky g , et al : alpelisib for pik3ca - mutated , hormone receptor - positive advanced breast cancer . 
n engl j med 380 : 1929 - 1940 , 2019 adamo b , deal am , burrows e , et al : phosphatidylinositol 3 - kinase pathway activation in breast cancer brain metastases . 
breast cancer res 13 : r125 , 2011 fitzgerald dm , muzikansky a , pinto c , et al : association between pik3ca mutation status and development of brain metastases in hr + / her2metastatic breast cancer . 
bergen es , berghoff as , medjedovic m , et al : continued endocrine therapy is associated with improved survival in patients with breast cancer brain metastases . clin cancer res 25 : 2737 - 2744 , 2019 11 . 
tolaney sm , lin nu , thornton d , et al : abemaciclib for the treatment of brain metastases ( bm ) secondary to hormone receptor positive ( hr + ) , her2 negative breast cancer . 
j clin oncol 35 : 1019 , 2017 ( 15 suppl ) ippen fm , alvarez - breckenridge ca , kuter bm , et al : the dual pi3k / mtor pathway inhibitor gdc - 0084 achieves antitumor activity in pik3ca - mutant breast cancer brain metastases . 
campone m , im s - a , iwata h , et al : buparlisib plus fulvestrant versus placebo plus fulvestrant for postmenopausal , hormone receptor - positive , human epidermal growth factor receptor 2 - negative , advanced breast cancer : overall survival results from belle - 2 . 
takeshita t , yamamoto y , yamamoto - ibusuki m , et al : analysis of esr1 and pik3ca mutations in plasma cell - free dna from er - positive breast cancer patients . 
study_list = brca_igr_2015%2cbrca_mbcproject_wagle_2017&case_set_id = all&data_priority = 0&gene_list = esr1%253amut%250apik3ca%253amut& geneset_list = %20&prolefilter = 0&tab_index = tab_visualize juric d , castel p , grifth m , et al : convergent loss of pten leads to clinical resistance to a pi ( 3 ) k inhibitor . 
grommes c , pentsova e , nolan c , et al : phase ii study of single agent buparlisib in recurrent / refractory primary ( pcnsl ) and secondary cns lymphoma 24 . 
maira s - m , pecchi s , huang a , et al : identication and characterization of nvp - bkm120 , an orally available pan - class i pi3 - kinase inhibitor . 
 o next - generation sequencing of advanced gi tumors reveals individual treatment options michael bitzer , md1 , 2 , 5 ; leonie ostermann1 ; marius horger , md3 ; saskia biskup , md , phd4 ; martin schulze , dsc4 ; kristina ruhm , msc5 ; franz hilke , msc6 ; oznur oner , msc5 ; konstantin nikolaou , md , mba2 , 3 ; christopher schroeder , md6 ; olaf riess , md6 ; falko fend , md7 , 8 ; daniel zips , md8 , 9 ; martina hinterleitner , md10 ; lars zender , md2 , 8 , 10 ; ghazaleh tabatabai , md , phd2 , 8 , 11 ; janina beha , phd5 ; and nisar p . 
malek , md1 , 2 , 5 , 8 purpose precision oncology connects highly complex diagnostic procedures with patient histories to identify individualized treatment options in interdisciplinary molecular tumor boards ( mtbs )  . 
follow - up data and a response assessment that was based on radiologic imaging were recorded . results ninety - six patients were presented to the mtb of tuebingen university hospital . 
patients with pr or sd in the course of mtb - recommended treatments seemed to benet with respect to pfs and os . jco precis oncol 4 : 258 - 271 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction the challenge of precision oncology is to connect highly complex diagnostic procedures with individual patient histories to identify optimal treatments . 
detailed data on mtbguided treatment suggestions , and specically the outcomes of patients , have only been reported for nonselected patient groups , including for a variety of different tumors.1 - 4 however , each tumor entity , including gi cancers , harbors unique features that will have to be considered to identify the patients who will benet the most from such an approach.4 recent reports highlight the experiences of mtbs in everyday practice . 
a series from the md anderson cancer center that examined hot - spot regions in 11 to 50 genes for 2 , 000 cancer tissues found actionable mutations for 39% of patients.2 only 11% of these selected patients could be enrolled in genotype - matched clinical trials.2 a report from the mayo clinic identied actionable mutations in 65% of 141 patients , but only 29 ( 21% ) were subsequently treated in clinical trials or with targeted food and drug administration ( fda ) approved drugs , with an objective response or stable disease ( sd ) for 4 months in 10 patients.3 freiburg university reported 104 patients with recommendations that were based on diagnostic tests that ranged from an 8 - gene panel to whole - exome sequencing ( wes ) .1 thirty - three patients received a recommended treatment ; 11 had an objective response , and 8 additional patients reached sd at 10 weeks . 
 molecular tumor board for advanced gi cancers context key objectives academic molecular tumor boards ( mtbs ) bridge the gap between a growing complexity in diagnostic procedures and clinicians at the bedside . 
this retrospective study investigated the course of patients with advanced gastrointestinal ( gi ) cancers that have been considered for personalized treatment options , including the outcome receiving mtb - guided treatment . knowledge generated next - generation sequencing ( ngs ) revealed a relevant number of germline variants , suggesting genetic counseling . 
responding patients with prolonged disease stabilization seemed to derive a meaningful survival benet from cancer genome sequencing and matched treatments . relevance patients with gi cancers can benet from currently available ngs sequencing procedures . 
in perspective , a continued improvement of mtb recommendations and the inclusion of additional complex diagnostic procedures might substantively enhance treatment opportunities in everyday clinical practice for these patients in the near future . the sequencing of matched tumor and normal tissue is an important procedure for the precise identication of potentially actionable genes.5 , 6 this inevitably leads to the detection of germline alterations . 
a recent investigation in 10 , 389 patients across 33 cancer types detected pathogenic or likely pathogenic germline variants in 8% of all patients with cancer and in 8.8% of patients with gi tumors.7 the frequency of germline mutations varied greatly across cancer types in general but also across different gi cancers , ranging from 2.2% for cholangiocarcinoma to 14.1% for pancreatic cancer ( pc ) .7 to our knowledge , our experience with gi tumors in an academic mtb is to date the largest reported series of this group with detailed information of comprehensive sequencing data , subsequent board recommendations , and documented outcome . 
the mtb consists of an interdisciplinary team coordinated by the tuebingen center for personalized medicine and includes experts in clinical and translational oncology , pathology , bioinformatics , molecular biology , radiology , and human genetics . 
an electronic web - based platform ( mtb platform ) was established to introduce patients to the mtb team with all necessary information to prepare and follow up the weekly face - to - face meetings and subsequently document treatment outcomes ( data supplement )  . 
best response assessment was based on radiologic imaging in line with recist 1.1 , for checkpoint inhibitor therapy , irecist , or for hepatocellular carcinomas ( hcc ) , mrecist criteria.8 - 10 genetic tumor / normal characterization tumor and normal tissues were genetically characterized either by ngs panel sequencing of full coding sequences or by wes ( more information in data supplement )  . 
off - label use refers to the administration of an fda / european medicines agency - approved drug outside its approved indication . for recommended off - label therapies , an application for reimbursement was submitted to the patients health individual treatment describes insurance . 
patients treated within a heilversuch have been registered at the local authority , in this case the regierungspr asidium tuebingen . statistical analysis progression - free survival ( pfs ) and overall survival ( os ) were analyzed with the kaplan - meier method dependent on the treatment response ( sd and pr v progressive disease [ pd ] ) compared by log - rank testing . 
btc , biliary tract cancer ; crc , colorectal cancer ; gc , gastric cancer ; hcc , hepatocellular carcinoma ; net , neuroendocrine tumor ; pc , pancreatic cancer ; ugc , upper gi tract cancer . results diagnostic procedure and clinical work - up ninety - six patients received ngs of advanced gi tumors and were presented to the mtb . 
this cohort included 32 colorectal cancer ( crc ) , 22 pc , 19 biliary tract cancer ( btc ) , 11 hcc , 9 upper gi tract cancer ( ugc ) , and 3 neuroendocrine tumors ( net ; fig 1a )  . 
the mean number of systemic anticancer pretreatments was 2.8 ( fig 1b )  . ninety - one patients received a gene panel analysis that examined between 337 and 710 genes , and 5 patients had wes ( fig 1c )  . 
genes represented in the different panels are summarized in the data supplement , together with the total size and the average and median coverage of the 649 and 710 gene panels . germline variants in gi cancers germline ndings were ranked according to a 5 - tiered classication.11 , 12 sixteen patients ( 17% ) had germline variants classied as pathogenic or likely pathogenic ( figs 1d - 1f ) , and in 1 patient with gastric cancer , 2 likely pathogenic variants were detected ( palb2 and fancm )  . five patients ( 5% ) had pathogenic or likely pathogenic germline variants in one of the brca2 , msh6 , or sdhb genes . 
these alterations belong to a list of secondary ndings that should be reported because of the possibility for interventions to signicantly reduce morbidity and mortality.13 in addition , 3 patients showed germline variants in pharmacologically relevant genes , 2 in dpyd and 1 in g6pd ( data supplement ) without showing unusual adverse reactions during chemotherapy . 
this variant has been reported with classications ranging from variant of unknown signicance to pathogenic.14 a germline alteration was directly responsible for mtb recommendations for 5 patients ( 5% ) : brca2 for poly ( adpribose ) - polymerase ( parp ) inhibition ( 3 pc ) , chek2 combined with 2 somatic atm truncations for atr - inhibition and carboplatin ( 1 crc ) , and msh6 and therefore a resulting high tumor mutational burden ( tmb ) for pembrolizumab ( 1 crc )  . 
 molecular tumor board for advanced gi cancers frequency of germline mutations ( n = 96 ) presentation of ngs for gi tumors ( n = 96 ) molecular target identification ( n = 96 ) patients with clinically relevant ( n = 19 [ 20% ] ) germline mutations patients with pathogenic or likely pathogenic ( n = 16 ) variants patients with pharmacogenomic relevant variants ( n = 3 ) patients with at least 1 molecular target ( n = 47 [ 49% ] ) patients without mtb recommendation ( n = 6 ) no progression under last line treatment ( n = 4 ) complete tumor resection ( n = 2 ) patients not treated with recommendation ( n = 16 ) patients with poor performance status ( n = 15 ) patients not evaluable ( n = 5 ) without imaging for response monitoring ( n = 3 ) died within 21 days after treatment start ( n = 2 ) patient not evaluable ( n = 1 ) alternative therapy before response monitoring patients with mtb treatment recommendation ( n = 41 [ 43% ] ) patients received the suggested treatment ( n = 25 [ 26% ] ) patients with colorectal cancer ( n = 11 ) patients with pancreatic cancer ( n = 7 ) patients with biliary tract cancer ( n = 4 ) patients with upper gi tract cancer ( n = 2 ) patient with hepatocellular carcinoma ( n = 1 ) patients evaluable for best response and os ( n = 20 [ 21% ] ) patients pr ( n = 3 [ 15% of 20 patients ] ) patients sd ( n = 6 [ 30% of 20 patients ] ) patients pd ( n = 11 [ 55% of 20 patients ] ) fig 2 . 
 ( b ) frequency of potential target identication by the molecular tumor board ( mtb ) , patients with target identication but no treatment , and patients with mtb - recommended treatment initiation . 
btc , biliary tract cancer ; crc , colorectal cancer ; hcc , hepatocellular carcinoma ; net , neuroendocrine tumor ; pc , pancreatic cancer ; ugc , upper gi tract cancer ; w / o , without . pharyngeal , or bladder cancer ; and the patient with a chek2 mutation had a rst - degree relative with ovarian cancer . 
eight of these 10 patients were also tested for msi , but only 2 patients were found to have a msi - high tumor . tmb is currently regarded as relevant in predicting therapeutic success with checkpoint inhibitors beyond tumors with mismatch repair deciency.15 - 18 this has been shown for patients with crc and ugc , 18 but is less clear for hepatobiliary cancer and pc . 
for tumors known to have a low tmb in general , those with values molecular target identication by the mtb at least 1 potential molecular target was identied in 47 of 96 patients ( 49% ; figs 2b and 3b )  . 
the frequency of target identication varied among tumor types ( fig 3c , table 2 ) , with 74% for btc , 56% for upper gi cancers , 50% for pc , 44% for crc , and 27% for hcc . 
the most frequently altered genes with single - nucleotide variants or copy number variants were cdkn2a / b , brca2 , idh1 , erbb2 , myc , fgf3 , fgf4 , flt3 , fgfr4 , cdk6 , braf , and atm ( table 2 ; data supplement )  . 
target identication per tumor type ( continued ) diagnosis patients tested ( no . ) molecular target frequency erbb2 braf brd4 cdkn2a / b chek2 fgf3 / 4 / 19a flt1 / 3 mlh1 msh6 fgfr2 - bicc1 idh1 braf brca1 brca2 cdkn2a fgfr1 fgfr2b fgfr4 fgfr2 - prkcq fgfr2 - ahcyl2 cdkn2a / b brca2 cdk6 erbb3 nrg3 nrg1 - cdh6 tmem66 - nrg1 cdkn2a / b cdk6 fgf3 / 4 idh1 idh1 abbreviations : btc , biliary tract cancer ; crc , colorectal cancer ; hcc , hepatocellular carcinoma ; pc , pancreatic cancer ; tmb , tumor mutational burden . afgf3 / fgf4 / fgf19 cluster amplication . bcoincident fgfr2 mutation in tumor with fgfr2_ahcyl2 fusion gene . cdkn2a / b alterations , 6 were detected in pc , 2 in ugc , 1 in btc , and 1 in crc . 
three out of 4 brca2 alterations were detected in pc , and 1 in btc ( table 2 )  . outcome and clinical course of patients the course of all patients presented to the mtb is shown in fig 2b . 
mtb recommendations for matched treatments were given for 41 patients ( 43% )  . twenty - ve patients with a mean of 3.4 previous anticancer treatments received the suggested medication ( 61% of patients with mtb recommendation ; 26% of the whole cohort )  . 
the alterations in included cdkn2a / b this subgroup without treatment deletions , braf mutations , brca deletions , flt1 / 3 amplication , fgfr2 fusion , idh mutation , and high tmb ( data supplement )  . treatment was initiated in 11 patients with crc ( 34% of patients with crc ) , 7 patients with pc ( 32% of patients with pc ) , 4 patients with btc ( 21% of patients with btc ) , 2 patients with ugc ( 22% of patients with ugc ) , and 1 patient with hcc ( 9% of patients with hcc )  . 
the applied drugs were either used in - label , used off - label , obtained via a clinical study , or supplied for a matched experimental treatment ( table 1 , drug availability column )  . 
 molecular tumor board for advanced gi cancers patients who reached either sd or pr were treated with pd1 blocking antibodies ( high tmb ) , atr inhibitor with carboplatin ( simultaneous mutations in atm , chek2 , and tp53bp1 ) , trastuzumab with lapatinib ( erbb2 amplication ) , pertuzumab with erlotinib ( nrg1 fusion , high - expression erbb3 and nrg3 ) , idh1 inhibitor bay 1436032 ( idh1 mutation ) , or lenvatinib ( fgfr2 fusion gene ; table 1 )  . 
1 year after treatment initiation reached either sd or pr ( data supplement )  . therefore , as a surrogate end point to estimate whether patients might benet from the mtb - recommended treatment , the achievement of sd for at least 3 months or even pr as best response was compared with pd in a kaplan - meier estimation for pfs and os . 
in several studies , the inclusion of germline ndings enabled a more comprehensive characterization of tumor biology , potential resistances , or even treatment opportunities.22 , 23 in this study , germline variants classied as pathogenic , likely pathogenic , or pharmacogenomic could be identied in 19 patients ( 20% )  . 
these numbers are higher than in a recent investigation that reported pathogenic or likely pathogenic germline predisposition variants in 8.8% of gi tumors , 7 and could be mainly a result of the smaller sample size in our study . 
for example , for brca mutations , the tumor lineage indeed seems to determine the therapeutic benet of parp inhibition.24 conversely , emerging data suggest that patients with germline mutations that are not typically associated with a diagnosed cancer might nevertheless benet from drugs that target this alteration.25 germline variant reporting and the inclusion of experts in clinical genetics , should therefore be a prerequisite for mtbs.22 , 23 , 26 in predicting therapeutic tmb is regarded as relevant outcome with checkpoint inhibitors.15 - 18 the minimum size of tumor panels to reliably calculate tmb was suggested to include at least 300 genes , or more precisely , 1.5 mb of the target region , 21 , 27 , 28 which is met in our approach . 
one patient with crc and high tmb ( 118 var / mb ) who showed progression under pd - 1 inhibition even responded after the addition of ctla4 inhibition on progression . 
in the 4 patients who did not show any response to checkpoint inhibition , the molecular analysis did not reveal one of the currently discussed mechanisms of resistance.29 of note , only a minority of patients with high tmb also had msi - high tumors . 
this observation is in line with an investigation in a broad range of different tumor types , showing that only 16% with high tmb were classied as msi high.21 another study in 6 , 004 patients with crc identied 465 patients with high tmb ; however , only 65% of these could be classied as msi high.30 these observations suggest that a reliable method for tmb estimation should be used if patients with gi tumors are evaluated for personalized treatment options . of 96 patients with advanced gi tumors , mtb treatment recommendations were given for 41 ( 43% ) , which means an additional therapy option beyond established treatment lines for 4 out of 10 patients . 
14 months in our cohort , compared with patients with pd as best response ( fig 4d ) , is remarkable ; however , it has to be interpreted with caution and should be conrmed in larger patient populations with gi or other cancers . 
if this observation could be conrmed , 1 goal in the constant improvement of mtb recommendations should be to gradually increase the percentage of patients who reach disease control of at least 3 months in advanced cancers . early cohorts with molecular - matched therapies have been reported for crc31 and btc.32 in the rst study , 68 out of 254 patients with advanced crc received selected matched therapies to kras / braf / pik3ca mutations , pten , or phosphorylated met expression . 
a subgroup with btc from the moscato - 01 trial reported molecular targets in 23 of 34 patients , with 18 receiving matched therapies ( 53% ) .32 the overall response rate and pfs of 6 months in that study were 33% and 37% , respectively . 
several techniques , such as transcriptome34 , 35 and epigenome36 analysis or wholegenome37 and single - cell sequencing , are expected to improve tumor characterization up front.38 such a constant evolution will require more specialists in these methods to join academic mtbs , which means a new era of terdisciplinary patient care to bridge the gap between a growing complexity in diagnostic procedures and clinicians at the bedside . 
 ( a ) progression - free survival ( pfs ) , dened as the time from start of an mtb - recommended treatment to radiographic progression or death , and ( b ) overall survival ( os ) , dened as the time from start of an mtbrecommended treatment to death as a result of any cause , in days . 
recent examples in crc are pd - l1 and ctla - 4 inhibition in msi - high cancers41 or the combination of a braf inhibitor , mek inhibitor , and antiepidermal growth factor receptor antibody in braf v600e mutated cancers.42 third , a reduction in dropout rates might be achieved with more focused and earlier patient selection for ngs - based diagnostic procedures and a shortening of time intervals to get access to suggested drugs . 
fourth , each patient who is treated according to an mtb recommendation outside clinical trials should be regarded as an n - of - 1 trial.43 this implies a thorough documentation of adverse events and a reliable response assessment along a predened routine . in conclusion , gi tumors are an important group in the eld of personalized medicine . 
malek provision of study material or patients : michael bitzer , falko fend collection and assembly of data : michael bitzer , leonie ostermann , marius horger , saskia biskup , kristina ruhm , oznur oner , christopher schroeder , olaf riess , falko fend , daniel zips , martina hinterleitner , lars zender , janina beha data analysis and interpretation : michael bitzer , leonie ostermann , marius horger , saskia biskup , martin schulze , franz hilke , konstantin nikolaou , christopher schroeder , olaf riess , daniel zips , martina hinterleitner , lars zender , janina beha , nisar p . 
 bitzer et al falko fend consulting or advisory role : roche , eusa pharma daniel zips research funding : elekta ( inst ) , siemens ( inst ) , sennewald ( inst ) travel , accommodations , expenses : elekta ( inst ) martina hinterleitner travel , accommodations , expenses : novartis / ipsen lars zender leadership : heparegenix gmbh consulting or advisory role : boehringer ingelheim research funding : heparegenix gmbh patents , royalties , other intellectual property : patent on mkk4 inhibition for the treatment of acute and chronic liver diseases travel , accommodations , expenses : ipsen ghazaleh tabatabai honoraria : abbvie , bayer , medac , novocure ( inst ) consulting or advisory role : abbvie , bayer travel , accommodations , expenses : novocure ( inst ) nisar p . 
hoefin r , geiler a - l , fritsch r , et al : personalized clinical decision making through implementation of a molecular tumor board : a german single - center experience . 
j clin oncol 33 : 2753 - 2762 , 2015 bryce ah , egan jb , borad mj , et al : experience with precision genomics and tumor board , indicates frequent target identication , but barriers to delivery . oncotarget 8 : 27145 - 27154 , 2017 zehir a , benayed r , shah rh , et al : mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10 , 000 patients . 
nat med 23 : 703 - 713 , 2017 [ erratum : nat med , 2017 ] jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
sci transl med 7 : 283ra53 , 2015 cheng dt , prasad m , chekaluk y , et al : comprehensive detection of germline variants by msk - impact , a clinical diagnostic platform for solid tumor molecular oncology and concurrent cancer predisposition testing . 
eur j cancer 45 : 228 - 247 , 2009 seymour l , bogaerts j , perrone a , et al : irecist : guidelines for response criteria for use in trials testing immunotherapeutics . 
plon se , eccles dm , easton d , et al : sequence variant classication and reporting : recommendations for improving the interpretation of cancer susceptibility j hepatol 66 : 1166 - 1172 , 2017 genetic test results . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
n engl j med 377 : 2500 - 2501 , 2017 jenkins rw , thummalapalli r , carter j , et al : molecular and genomic determinants of response to immune checkpoint inhibition in cancer . 
fabrizio da , george tj jr , dunne rf , et al : beyond microsatellite testing : assessment of tumor mutational burden identies subsets of colorectal cancer who may respond to immune checkpoint inhibition . 
verlingue l , malka d , allorant a , et al : precision medicine for patients with advanced biliary tract cancers : an effective strategy within the prospective moscato - 01 trial . 
overman mj , lonardi s , wong kym , et al : durable clinical benet with nivolumab plus ipilimumab in dna mismatch repair - decient / microsatellite instabilityhigh metastatic colorectal cancer . 
ferguson , mbbs , mrcp , frcr4 ; alessandra curioni - fontecedro , md , pd1 ; martin zoche , phd1 ; holger moch , md1 ; and bart vrugt , md , phd1 introduction malignant mesothelioma ( mm ) is a rare neoplasm arising from the mesothelial cell lining of the pleura ( 80% to 90% ) , but it can also develop in the peritoneum ( 10% to 15% ) , pericardium , and tunica vaginalis.1 , 2 because of the long latency of the disease , the age at diagnosis ranges from 54 to 65 years3 - 5 ; thus , mm rarely occurs in young patients and children . the frequency of both pleural and peritoneal mm is almost equal in patients younger than age 40 years . 
in addition , previous asbestos exposure is less common in peritoneal compared with pleural mm.6 peritoneal mesothelioma commonly presents with vague and unspecic symptoms , including abdominal distension and weight loss.7 consequently , the diagnosis of peritoneal mesothelioma generally is made at an advanced stage of the disease , 8 which partly explains the poor clinical outcome , even after optimal oncologic and surgical treatment . 
the median survival is less than 12 months in the majority of patients.9 , 10 patients with mm are not routinely analyzed for the presence of potentially drug - targetable gene mutations , including anaplastic lymphoma tyrosine kinase ( alk )  . 
by using targeted next - generation sequencing of tumor dna and rna , hung et al11 recently identied alk rearrangements with three novel alk fusion partners in a small subgroup of patients with peritoneal mm . 
the alk breakpoint was mapped to intron 19 in all three cases , the strn breakpoint to intron 3 , the atg16l1 breakpoint to intron 2 , and the tpmi1 breakpoint to the beginning of exon 9 . here we report a 13 - year - old girl with peritoneal mesothelioma harboring an strn - alk gene fusion , which was identied by comprehensive genomic proling ( cgp )  . 
images before treatment showed large - volume ascites , bilateral hydrotissue nephrosis , and widespread peritoneal soft deposits particularly within the pelvis and around the liver with scalloping of the liver margin ( fig 1 )  . 
she had no history of asbestos or radiation exposure . peritoneal biopsies were obtained by an explorative laparoscopy and submitted for a histologic and molecular work - up . pathology multiple peritoneal biopsies revealed a tumor with a mixed tubulopapillary and solid growth pattern . immunohistochemistry with positivity for ck5 / 6 and calretinin in the absence of expression of the epithelial marker berep - 4 and claudin - 4 conrmed the mesothelial origin of the tumor . 
even though necrosis and mitotic activity ( less than 1 mitosis per 10 high - power elds ) were not evident , growth pattern , cytonuclear atypia of the tumor cells , and immune prole fullled the criteria for malignant epithelioid mesothelioma ( figs 2a and 2b )  . 
images before treatment demonstrate large - volume ascites , bilateral hydronephrosis , and widespread peritoneal soft tissue deposits particularly within the pelvis ( all ndings marked by green arrows )  . 
 ( b ) schematic representation of the strn - alk fusion showing the 700 - amino - acid ( aa ) - long fusion gene , with 137 aas originating from the n terminus of strn and the remaining 562 aas originating from the c terminus of alk . 
 ( a ) immunohistochemical staining showing strong expression of alk protein ( original magnication 40 )  . ( b ) alk uorescent in situ hybridization break - apart probes showing one fused red - green signal and one red signal in 96% of the tumor cells compatible with 5 ( cid : 1 ) alk deletion ( original magnication 100 )  . for a transient and self - limiting rise in alanine aminotransferase ( alt ) , no adverse effects were noted . discussion we report a dramatic tumor regression after the rst cycle of ceritinib in a 13 - year - old girl with alk - rearranged peritoneal mm . 
the alk receptor can be translocated , mutated , or overexpressed in non - squamous nonsmall - cell lung cancer , inammatory myobroblastic tumors ( imts ) , and anaplastic large - cell lymphomas ( alcls ) .14 it is well known that pediatric patients with imts or alcl can show strong and sustained clinical response to the inhibitory effects of the alk - targeting drug crizotinib.15 peritoneal mm is an extremely rare tumor in children , but an almost complete response to an alk - targeting drug has never been described before . 
recently , loharamtaweethong et al16 reported a 10 - year - old girl with an alk - translocated peritoneal mm detected by fish and immunohistochemistry , but the exact fusion partner was not determined . 
genetic alterations frequently seen in pleural and peritoneal mesothelioma , including cdkn2a , bap - 1 , nf2 , and setd2 , are not detected in patients with alk - rearranged disease.11 even though the prevalence of alk - rearranged peritoneal mesotheliomas is low , alk alterations seem to be restricted to peritoneal mesothelioma only and do not occur in pleural mm . 
this is consistent with our observation , because we were unable to demonstrate alk expression in a tissue microarray containing tumor samples from 221 patients with pleural mesothelioma , including 22 females of whom three were younger than age 40 years ( unpublished data )  . in our patients tumor sample , we identied a rare alk fusion by cgp . 
the platform used in this study can detect all alk alterations ( including atg16l1 and tpm1 fusions ) and has been extensively validated.12 even in alk fishnegative patients , alk rearrangements could be identied by using this method.18 in our patient , we detected an strn - alk fusion with similar breakpoints but with a fusion in the alk - rearranged patient protein identical described by hung et al.11 the strn - alk fusion was an inframe alteration with breakpoints for strn in intron 3 and alk in intron 19 . to that patients with alk - rearranged mm cannot be distinguished from their conventional counterparts , but the differences in clinical presentation ( young patients with no history of asbestos exposure ) and the detection of isolated alk mutations would justify a separate tumor entity of alk - rearranged mesothelioma . 
in the absence of genetic alterations of cdkn2a , bap - 1 , nf2 , and setd2 , it is tempting to speculate that fusions involving the alk gene may represent the predominant oncogenic driver in peritoneal mm in young female patients . 
on the basis of the success of therapeutic alk inhibition in our patient , alk fusion screening by cgp is highly advised in peritoneal mms , especially in young patients . 
the promising response in our patient also stresses the need for investigations involving a larger cohort of young female patients with alkrearranged peritoneal mm to determine the efcacy and durability of alk inhibition . 
r uschoff , elise gradhand , alessandra curioni - fontecedro , martin zoche , holger moch , bart vrugt administrative support : holger moch provision of study materials or patients : elise gradhand , helen rees , martin zoche , bart vrugt collection and assembly of data : elise gradhand , abdullah kahraman , helen rees , jane l . 
hoffmann - la roche holger moch honoraria : roche consulting or advisory role : roche , deniens research funding : roche ( inst ) travel , accommodations , expenses : roche pharma travel , accommodations , expenses : deniens no other potential conicts of interest were reported . references 20 : 935 - 944 , 2009 ray m , kindler hl : malignant pleural mesothelioma : an update on biomarkers and treatment . 
cancer causes control beebe - dimmer jl , fryzek jp , yee cl , et al : mesothelioma in the united states : a surveillance , epidemiology , and end results ( seer ) - medicare investigation of treatment patterns and overall survival . 
eur j gynaecol oncol 18 : 141 - 143 , 1997 asensio ja , goldblatt p , thomford nr : primary malignant peritoneal mesothelioma : a report of seven cases and a review of the literature . 
arch surg 125 : 1477 - 1481 , 1990 thomas a , chen y , yu t , et al : distinctive clinical characteristics of malignant mesothelioma in young patients . 
tumori 89 : 269 - 273 , 2003 kaya h , sezgi c , tanrikulu ac , et al : prognostic factors inuencing survival in 35 patients with malignant peritoneal mesothelioma . 
fabrizio da , george tj jr , dunne rf , et al : beyond microsatellite testing : assessment of tumor mutational burden identies subsets of colorectal cancer who may respond to immune checkpoint inhibition . 
moss e yp , voss sd , lim ms , et al : targeting alk with crizotinib in pediatric anaplastic large cell lymphoma and inammatory myobroblastic tumor : a childrens oncology group study . 
loharamtaweethong k , puripat n , aoonjai n , et al : anaplastic lymphoma kinase ( alk ) translocation in paediatric malignant peritoneal mesothelioma : a case report of novel alk - related tumour spectruhistopathology 68 : 603 - 607 , 2016 17 . 
ali sm , ou shi , he j , et al : identifying alk rearrangements that are not detected by fish with targeted next - generation sequencing of lung carcinoma . 
an endobronchial biopsy showed an adenocarcinoma consistent with a lung primary ( thyroid transcription factor 1 positive , napsin a positive , and cytokeratin 7 positive by immunohistochemistry ; figs 1a and 1b )  . targeted exon sequencing of 468 genes with memorial sloan kettering integrated mutation proling of actionable cancer targets ( msk - impact ) was negative for known mitogenic drivers , including kras , egfr , braf , met , and erbb2 mutations and alk , ros1 , and ret rearrangements . 
photomicrographs of ( a ) cytology from the patients lung adenocarcinoma and ( b ) positive immunohistochemistry results remarkable for cytoplasmic and membranous staining using a pan - trk antibody are shown . 
this identied a novel activating trk fusion ( in - frame fusion between eps15 exon 21 and ntrk1 exon 10 ; figs 1c and 1d )  . the patient consented to receive larotrectinib in a basket study for trk fusion - positive cancers ( navigate ; clinicaltrials.gov identier : nct02576431 )  . 
a brisk partial response to therapy was achieved at 4 weeks , which was subsequently conrmed at 8 weeks ( 34% by response evaluation criteria in solid tumors [ recist ] version 1.1 ; fig 2 ) , with regression of all areas of disease . 
this included near total resolution of all brain metastases at 8 weeks ( 95% reduction in aggregate tumor volume ) and subsequently , a complete intracranial response by 16 weeks ( fig 3 )  . 
pathology showed a stage iiic ( t1cn3m0 ) multifocal invasive ductal carcinoma ; the largest lesion measured 1.8 cimmunohistochemistry was positive for estrogen and progesterone receptors and negative for human epidermal growth factor receptor 2 . 
she was treated initially with adjuvant dose - dense doxorubicin , cyclophosphamide , plus paclitaxel and radiotherapy , after which she received anastrozole followed by bilateral salpingo - oophorectomy . the patient developed recurrent , metastatic disease approximately 17 months after completing adjuvant radiolymph node biopsy conrmed therapy . 
sequencing of an abdominal lymph node and a subsequently biopsied liver metastasis using msk - impact revealed the previously reported fusion between lmna exons 1 and 20 and ntrk1 exons 11 and 17 , which was veried using targeted multiplex rna sequencing . the patient consented to receive larotrectinib in the same basket study for trk fusion - positive cancers ( navigate )  . at enrollment , her disease was widely metastatic to liver , adrenal gland , lymph nodes , and bone . 
a brisk and conrmed partial response by recist version 1.1 ( 32% , 47% , and 56% at 4 , 8 , and 16 weeks , respectively ) was achieved . 
of note , her cns metastases likewise regressed at the rst follow - up assessment at 4 weeks , with a complete response in the cns at 8 weeks ( fig 4 )  . 
axial contrastenhanced t1 - weighted images at ( a ) baseline ( brain metastases highlighted by circles ) , ( b ) 8 weeks , and ( c ) 16 weeks after treatment with larotrectinib was initiated demonstrate decreased and then resolved metastases in the right - side insula and left - side occipital lobe . 
three - dimensional models at ( d ) baseline and ( e ) post - treatment at 8 weeks and ( f ) post - treatment at 16 weeks conrmed decreased burden of metastatic intracranial disease ( segmented in green voxels and quantied at bottom )  . 
response to larotrectinib in a patient with a trk fusion - positive metastatic breast cancer . baseline axial computed tomography imaging of the brain was performed with the addition of iodinated contrast that showed ( a ) metastatic brain disease ( circles ) and after 8 weeks of treatment with larotrectinib , ( b ) complete response . 
 rosen et al discussion to our knowledge , this report is the rst to showcase the intracranial efcacy of larotrectinib in metastatic trk fusion - positive cancers of any histology . 
these cases demonstrate that larotrectinib can achieve clinically relevant cns exposure , which highlights its role in the management of trk fusion - positive cancers with intracranial disease . beyond nsclcs and breast cancers , other trk fusionpositive tumors have a proclivity for brain metastases.1 the intracranial activity featured here is consistent with prior work that did not identify cns metastasis as a site of progression on larotrectinib across multiple tumor types4 and with a report that showed a response to larotrectinib in a trk fusion - positive glioma.5 additional clinical experience in patients with trk fusion - positive cancers with cns involvement ultimately will delineate the overall activity and durability of larotrectinib within the cns . although this article represents what is to our knowledge the rst report of intracranial responses to a sein patients with trk fusionlective trk inhibitor positive cancers and brain metastases , intracranial disease control also has been reported with multikinase trk inhibitors . 
entrectinib , a multikinase trk , ros1 , and alk inhibitor , displayed activity in a patient with a trk fusion - positive lung cancer and brain metastases6 and in ros1 fusion - positive lung cancers with intracranial disease.7 repotrectinib , a multikinase trk , ros1 , and alk inhibitor , achieved intracranial disease regression in untreated brain metastases in a patient with a ros1 fusion - positive nsclc.8 finally , this report represents the rst description of the novel eps15 - ntrk1 fusion . 
young stock and other ownership interests : agios , alexion pharmaceuticals , biogen , celgene , gilead sciences , karyopharm therapeutics , spark therapeutics , regeneron pharmaceuticals , stemline therapeutics , vertex consulting or advisory role : agios , puma biotechnology , nordicneurolab , icon clinical research research funding : agios ( inst ) jaclyn f . 
shu research funding : celgene ( inst ) , genentech ( inst ) , roche ( inst ) , janssen pharmaceuticals ( inst ) , medimmune ( inst ) travel , accommodations , expenses : genentech , roche nora c . 
 cns efcacy of larotrectinib in trk fusion - positive solid tumors travel , accommodations , expenses : novartis ( i ) , biotheranostics ( i ) , pzer ( i ) , amgen ( i ) , genentech ( i ) , roche ( i ) , astrazeneca ( i ) , macrogenics ( i ) , peregrine pharmaceuticals ( i ) , pierian bioscience ( i ) david m . 
ziegler ds , wong m , mayoh c , et al : brief report : potent clinical and radiological response to larotrectinib in trk fusion - driven high - grade glioma . 
drilon a , siena s , ou s - hi , et al : safety and antitumor activity of the multi - targeted pan - trk , ros1 , and alk inhibitor entrectinib ( rxdx - 101 ) : combined results from two phase 1 trials ( alka - 372 - 001 and startrk - 1 )  . 
doebele r , ahn m , siena s , et al : oa02.01 : efcacy and safety of entrectinib in locally advanced or metastatic ros1 fusion - positive non - small cell lung cancer 8 . 
drilon a , ou si , cho bc , et al : repotrectinib ( tpx - 0005 ) is a next - generation ros1 / trk / alk inhibitor that potently inhibits ros1 / trk / alk solvent - front 9 . 
 rationale and design of the targeted agent and profiling utilization registry study purpose case reports and small prospective trials suggest that administering targeted therapies to patients with advanced cancer and an identified genomic target may be associated with clinical benefit . 
the targeted agent and profiling utilization registry ( tapur ) study , a phase ii prospective , nonrandomized , multibasket pragmatic clinical trial , aims to identify signals of drug activity when us food and drug administration approved drugs are matched to prespecified genomic targets in patients with advanced cancer , outside of approved indications . methods patients eligible to participate in tapur are age 12 years and have advanced measurable or evaluable solid tumors , multiple myeloma , or b - cell non - hodgkin lymphoma . 
secondary end points include safety , progression - free survival , and overall survival . results more than 1 , 000 participants have thus far been registered , and more than 800 have been treated with a tapur study drug . 
two study cohorts have permanently closed to enrollment because of lack of antitumor activity , and 12 have expanded to the second stage of enrollment after promising preliminary activity . conclusion the tapur study will describe the efficacy and toxicity of the targeted drugs used outside of their approved indications when matched to a somatic genomic variant . evidence is building through reports of clinical trials , case reports , and clinical anecdotes to suggest that patient outcomes may be improved when a targeted agent is matched to a genomic alteration present in a patients tumor.1 - 6 clinical reports to date suggest that 30% to 80% of advanced solid tumors harbor potentially actionable genomic variants.7 - 10 in a meta - analysis of 570 phase ii studies of new anticancer agents , schwaederle et al11 examined response rate ( rr ) , progression - free survival ( pfs ) , and overall survival ( os ) for 32 , 149 patients who received a personalized treatment strategy versus those who did not . 
 of the md anderson cancer center experience of genomic profiling of patients with solid tumors with advanced disease , the impact ( initiative for molecular profiling and advanced cancer therapy ) study . 
the moscato - 01 ( molecular screening for cancer treatment optimization ; clinicaltrials.gov identifier : nct01566019 ) trial enrolled patients with treatment - resistant progressive metastatic cancers with lesions accessible to biopsy to perform genomic profiling.14 this study compared pfs using therapy based on genomic assessment with pfs for the most recent therapy during which the patient had experienced disease progression . 
le tourneau et al17 published the results of a randomized phase ii trial comparing therapy on the basis of tumor molecular profiling versus physician choice of therapy in patients with refractory cancer . 
this article will describe the rationale and design of the targeted agent and profiling utilization registry ( tapur ) study , a large pragmatic precision medicine basket trial with the overarching goal of describing the efficacy and toxicity of targeted anticancer drugs used outside of their approved indications for treatment of patients with advanced cancer based on a tumor genomic profile . methods objectives the primary objective of tapur is to evaluate the antitumor activity of commercially available targeted anticancer drugs used outside of their fda - approved indications for treatment of patients with advanced solid tumors , multiple myeloma , or b - cell non - hodgkin lymphoma with a genomic alteration known to be a drug target . 
secondary objectives include determination of pfs , os , and safety . design the tapur study is a phase ii prospective , nonrandomized , open - label clinical trial that aims to define signals of drug activity . 
list of available tapur study treatments for adults and pediatric patients study drug population to which available adults and children age 12 - 17 years adults only adults and children age 12 - 17 years adults and children age 16 - 17 years adults and children age 13 - 17 years adults and children age 12 - 17 years adults and children age 16 - 17 years adults only adults and children age 12 - 17 years adults and children age 12 - 17 years adults and children age 12 - 17 years nivolumab + ipilimumab adults only pembrolizumab adults and children age 12 - 17 years axitinib bosutinib cetuximab crizotinib dasatinib erlotinib olaparib palbociclib regorafenib sunitinib temsirolimus trastuzumab + pertuzumab adults only vemurafenib + cobimetinib adults only vismodegib adults and children age 12 - 17 years note . 
the study includes participants as young as 12 years of age with a tumor harboring a genomic alteration known to be a target of or to predict sensitivity to at least one of the 16 therapeutic options available in the study ( table 1 )  . 
eligible participants must have a tumor genomic variant identified on a test performed in a laboratory that has certification under the clinical laboratory improvement amendments and accreditation by the college of american pathologists . 
patients are matched to at least one of the available study treatments through a set of protocol - defined genomic matching rules or after review of a participant case by the tapur molecular tumor board ( mtb )  . 
the study uses simons optimal two - stage design for cohort analysis . tapur was designed independently by asco staff and volunteer leaders , with input from patient advocates , community - based investigators , the initial collaborating pharmaceutical companies , and the asco cancer research committee . 
the study was registered on clinicaltrials.gov ( nct02693535 ) before study launch . a data and safety monitoring board ( dsmb ) , consisting of a group of independent experts not involved in the conduct of tapur , meets biannually to monitor the study data and outcomes . 
 their primary functions include assessing the safety and efficacy of study treatments , safeguarding the interests and safety of trial participants , and ensuring that study results are both credible and reported to the medical community in a timely manner . 
for expanded cohorts , it will review all final cohort analyses and make recommendations regarding release of the cohort data . study population and recruitment the pragmatic approach of tapur allows for broad eligibility criteria , including eastern cooperative oncology group performance status of 0 to 2 , age 12 years , prior malignancies or positive hiv status , and previously treated but clinically stable brain metastases . 
tapur inclusion and exclusion criteria comport fully with recently published recommendations by asco and friends of cancer research for broadening eligibility criteria for cancer clinical trials.23 participating sites include both academic and community centers . study treatment decision once a potential participant is identified , the clinical site obtains informed consent and registers the participant in the tapur electronic data capture ( edc ) platform as shown in figure 1 . 
if a study drug is identified and the drug - specific inclusion and exclusion criteria are met , the clinical site completes the drug specific informed consent process and enrolls the participant in the study . 
 a screening consent general eligibility criteria met registration treatment 1 treatment 2 , continued tapur matching to study drug ( s ) based on genomic criteria ( or approved by mtb ) treatment decision by treating physician target variant 1 target variant 2 screening continued drug - specific eligibility criteria met tumor type 1 tumor type 2 tumor type 1 tumor type 2 enrolled and placed into cohorts enrollment cohort 1 cohort 2 cohort 3 cohort 4 fig 1 . 
the mtb , composed of clinical oncologists , molecular pathologists , and patient advocates , reviews the genomic test results , pathology reports , and clinical histories of submitted patient cases and identifies potential treatment matches among the study treatments . 
of the patient cases reviewed by the mtb , approximately 65% resulted in identification of a study drug option . permitted at the discretion of the treating physician in accordance with the recommended dose modifications contained in the approved prescribing information . 
management of aes is performed according to institutional standards of care , informed by the package insert . tumor measurements and radiologic evaluations and evaluation of clinical disease status are performed every 8 weeks after initiation of treatment for the first 16 weeks , and then every 12 weeks if the treatment continues , and at the end of study treatment , if possible . 
study treatment is continued until progressive disease is documented . after progression of disease during any study treatment , participants may be reassessed to determine eligibility for treatment with another study drug after a minimum of 30 days has elapsed from the last dose of the previous drug and any aes have resolved to grade 2 or stabilized . 
all general and drug - specific eligibility criteria must be reconfirmed , and the participant must sign a new drug - specific consent form . treatment schedule and interval of evaluations ae and sae criteria study treatments are administered according to the recommended starting dose and schedule described in the package insert of each drug . 
events not resolved at the end of study treatment require follow - up every 30 days until the event resolves to ctcae grade 2 . tapur requires reporting of ctcae grade 3 to 4 aes that are possibly , probably , or definitely related to the study treatment , whether expected or not . 
all saes , regardless of grade , relatedness to study drug , or expectedness , must also be reported , including all deaths . end points the primary end point is objective response at 8 weeks or sd documented at 16 weeks . 
tapur study milestones date milestone march 14 , 2016 study launch at 37 clinical site locations with 14 study drugs first participant registered ( consented ) first participant enrolled ; two additional drugs added for total of 16 study drugs additional drug added for total of 17 study drugs 100th participant registered november 2016 100th participant enrolled march 2016 april 2016 may 2016 august 2016 april 2017 june 2017 august 2017 september 2017 november 2017 december 2017 february 2018 march 2018 33 clinical sites added for total of 70 locations 500th participant registered additional therapy added for 19 study drugs first cohort reaches stage one 500th participant enrolled 1 , 000th participant registered 10th cohort reaches stage one 43 clinical sites added for total of 113 locations abbreviation : tapur , targeted agent and profiling utilization registry . the basis of the presence , absence , or unequivocal progression of the lesions . 
participants who have no tumor evaluation beyond baseline and are alive with no signs of progressive disease at the time of leaving the study will be replaced in their cohort with another participant . secondary end points include grade 3 to 5 aes and saes , pfs , response duration , and os . 
the null hypothesis is that the probability of objective response or sd of at least 16 weeks duration is 15% , versus the alternative hypothesis that it is at least 35% . 
after 28 participants in the cohort have been observed for the primary outcome , if seven or more participants achieve objective response or sd of at least 16 weeks duration , the null hypothesis will be rejected , and we will declare that the study drug is active in the cohort of participants defined by tumor type and genomic alteration . 
this design has a 54% chance of early stopping if the null hypothesis is true . estimates of the rr and 95% ci will be presented for each cohort upon closure ( at either stage one or stage two ) .24 the kaplan - meier method will be used to estimate the duration of response , pfs , and os distributions . results table 3 summarizes key study milestones . 
figure 2 also shows the distribution of genomic targets by tumor type ( fig 2b ) and study drug ( fig 2c ) , highlighting the heterogeneity of genomic targets and tumor types , resulting in 336 unique cohorts at the time of this writing . 
targeted agent and profiling utilization registry ( tapur ) study registration , enrollment , and cohort creation by ( a ) month , ( continued on next page ) many cancers that are driven by specific molecular alterations that can be targeted with drugs that inhibit aberrant signaling pathways in tumor cells . 
thus , the targeting of bcr - abl alterations in chronic myeloid leukemia , flt3 alterations in acute myeloid leukemia , egfr mutations and alk translocations in nonsmallcell lung cancer , braf mutations in melanoma and nonsmall - cell lung cancer , and human epidermal growth factor receptor 2 overexpression in breast and gastric cancers , among others , represent examples of the successful application of precision medicine approaches in clinical oncology that have extended the lives of many patients.1 , 25 - 30 interest in precision medicine has been further fueled by reported responses ranging from modest to exceptional when targeted treatments are selected based on large - scale genomic tumor profiling.5 the widespread availability of commercial next generation sequencing tests presents opportunities for patients who have exhausted standard treatment options to pursue treatments with investigational agents or approved drugs prescribed outside of their labeled indications . the tapur study stemmed from the recognition that the rapid dissemination of genomic profiling provides an opportunity to learn from the application of precision cancer medicine in practice while at the same time providing a framework for clinical decision support for clinical oncologists who are struggling to interpret the complex genomic data they now confront in practice . 
 b vegfr3 ( flt4 ) mutation , amplification , or overexpression vegfr1 ( flt1 ) mutation , amplification , or overexpression smo mutation lck mutation prkdc mutation pold1 mutation msh2 mutation vegfr3 ( flt4 ) mutation or amplification ewsr1nrya3 fusion cdk12 mutation ccnd3 bcr - abl mutation alk fusion or mutation msi high status egfr mutation rictor amplification vegfr1 ( flt1 ) mutation or amplification csf1r mutation or amplification vegfr2 ( kdr ) mutation , amplification , or overexpression vhl mutation or amplification ptch1 deletion or inactivating mutation mlh1 mutation tsc2 mutation pdgfra mutation or amplification palb2 mutation stk11 mutation vegfr2 ( kdr ) mutation or amplification ret mutation or amplification pdgfr ? mutation or amplification kit mutation atm mutation tsc1 mutation pole mutation fgfr3 mutation or amplification cdk6 amplification raf1 mutation or amplification pten mutation kit mutation or amplification braf mutation or amplification akt1 mutation flt3 mutation or amplification brca1 / brca2 mutation met amplification or mutation pik3ca mutation mtor mutation fgfr2 mutation or amplification ccnd1 amplification fgfr1 mutation or amplification cdk4 amplification atm mutation or deletion braf_v600e / d / k / r mutation erbb2 / erbb3 mutation , amplification , or overexpression kras , nras , and braf wild type ( all must be wild type ) germline or somatic brca1 / brca2 inactivating mutations high tumor mutational burden cdkn2a loss or mutation total fig 2 . 
 ( a ) april 2018 registration , enrollment , and cohort creation in progress at the time of this report ; ( b , c ) the number in each box indicates the number of patients . 
 c vegfr3 ( flt4 ) mutation , amplification , or overexpression vegfr1 ( flt1 ) mutation , amplification , or overexpression smo mutation lck mutation prkdc mutation pold1 mutation msh2 mutation vegfr3 ( flt4 ) mutation or amplification ewsr1nrya3 fusion cdk12 mutation ccnd3 bcr - abl mutation alk fusion or mutation msi high status egfr mutation rictor amplification vegfr1 ( flt1 ) mutation or amplification csf1r mutation or amplification vegfr2 ( kdr ) mutation , amplification , or overexpression vhl mutation or amplification ptch1 deletion or inactivating mutation mlh1 mutation tsc2 mutation pdgfra mutation or amplification palb2 mutation stk11 mutation vegfr2 ( kdr ) mutation or amplification ret mutation or amplification pdgfr ? mutation or amplification kit mutation atm mutation tsc1 mutation pole mutation fgfr3 mutation or amplification cdk6 amplification raf1 mutation or amplification pten mutation kit mutation or amplification braf mutation or amplification akt1 mutation flt3 mutation or amplification brca1 / brca2 mutation met amplification or mutation pik3ca mutation mtor mutation fgfr2 mutation or amplification ccnd1 amplification fgfr1 mutation or amplification cdk4 amplification atm mutation or deletion braf_v600e / d / k / r mutation erbb2 / erbb3 mutation , amplification , or overexpression kras , nras and braf wild type ( all must be wild type ) germline or somatic brca1 / brca2 inactivating mutations high tumor mutational burden cdkn2a loss or mutation total fig 2 . 
 ( continued ) ( c ) ibrance ( pfizer , new york , ny ) , lynparza ( astrazeneca , wilmington , de ) , sutent ( pfizer ) , keytruda ( merck , kenilworth , nj ) , torisel ( pfizer ) , erbitux ( eli lilly , indianapolis , in ) , perjeta ( genentech , south san francisco , ca ) , herceptin ( genentech ) , cotellic ( genentech ) , zelboraf ( genentech ) , opdivo ( bristol - myers squibb , new york , ny ) , yervoy ( bristol - myers squibb ) , stivarga ( bayer , whippany , nj ) , xalkori ( pfizer ) , sprycel ( bristol - myers squibb ) , erivedge ( genentech ) , inlyta ( pfizer ) , bosulif ( pfizer ) , and tarceva ( genentech )  . 
tapur study initial cohort expansions and closures study drug tumor type variant ovarian cancer kras , nras , and braf wild type colorectal cancer braf_v600e / d / k / r mutation breast cancer colorectal cancer germline or somatic brca1 / brca2 inactivating mutations atm mutation or deletion head and neck cancer soft tissue sarcoma malignant neoplasm of bronchus and lung cdkn2a loss or mutation cdk4 amplification cdkn2a loss or mutation breast cancer colorectal cancer uterine cancer high tumor mutational burden high tumor mutational burden high tumor mutational burden colorectal cancer erbb2 / erbb3 mutation , amplification , or overexpression expansion to stage two cetuximab cobimetinib + vemurafenib olaparib palbociclib pembrolizumab pertuzumab + trastuzumab sunitinib closed at stage one palbociclib breast cancer fgfr1 mutation or amplification pancreatic cancer malignant neoplasm of gallbladder and bile ducts cdkn2a loss or mutation abbreviation : tapur , targeted agent and profiling utilization registry . data collection , and discretion left to the treating physician regarding choice of which tumor biospecimen to interrogate and which genomic profiling test to use . 
however , tapur uses standard treatment response and toxicity criteria for assessment of efficacy and toxicity outcomes , structured data collection , protocol - specified evaluation times , and a standard simons twostage statistical design to assess the primary end point as well as an independent dsmb to provide recommendations on cohort expansion and closure . 
importantly , the study also provides educational opportunities and clinical decision support tools to treating physicians in the form of protocol - specified genomic matching rules and access to an mtb to assist in interpretation of genomic test reports . although study results are not yet available , preliminary information about the status of certain cohorts suggests that the study can provide meaningful information . 
 enrollment rates when the frequency of genomic targets was not well defined for many tumor types , identifying clinical launch sites that routinely used genomic profiling , arranging for drug distribution , and building an experienced clinical trial management team to operate the study . 
mangat no relationship to disclose susan halabi consulting or advisory role : tokai pharmaceuticals consulting or advisory role : eisai , bayer healthcare pharmaceuticals travel , accommodations , expenses : bayer healthcare pharmaceuticals suanna s . 
bruinooge no relationship to disclose elizabeth garrett - mayer stock and other ownership interests : abbott laboratories , abbvie consulting or advisory role : tactical therapeutics , okava pharmaceuticals ajjai alva consulting or advisory role : eisai , astrazeneca , genentech / roche speakers bureau : astrazeneca research funding : genentech ( inst ) , novartis ( inst ) , bristol - myers squibb ( inst ) , bind biosciences ( inst ) , acerta pharma ( inst ) , merck sharp & dohme ( inst ) , prometheus laboratories ( inst ) , covance ( inst ) , mirati therapeutics ( inst ) , united biosource ( inst ) , ariad pharmaceuticals ( inst ) , astrazeneca ( inst ) , pfizer ( inst ) , genentech / roche ( inst ) , hoosier cancer research network ( inst ) , bayer healthcare pharmaceuticals ( inst ) katherine a . 
stella no relationship to disclose emile voest consulting or advisory role : interna , biogeneration ventures research funding : novartis ( inst ) , glaxosmithkline ( inst ) , genentech / roche ( inst ) , pfizer ( inst ) , astrazeneca ( inst ) , eisai ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) kathleen j . 
kim honoraria : celgene , eli lilly , astrazeneca , boehringer ingelheim consulting or advisory role : eli lilly , celgene , astrazeneca , boehringer ingelheim travel , accommodations , expenses : eli lilly , celgene , astrazeneca , boehringer ingelheim richard l . 
kim , carolinas healthcare systems levine cancer institute , charlotte , nc ; ajjai alva , university of michigan ; jane perlmutter , gemini group , ann arbor ; philip j . 
janeway , data - farber / boston childrens cancer and blood disorders center , boston , ma ; emile voest , netherlands cancer institute , amsterdam , the netherlands ; and navin pinto , seattle childrens hospital , seattle , wa . 
wagle n , grabiner bc , van allen em , et al : activating mtor mutations in a patient with an extraordinary response on a phase i trial of everolimus and pazopanib . 
cobain ef , robinson dr , wu y - m , et al : clinical impact of high - throughput sequencing in patients with advanced cancer : lessons learned from the michigan oncology sequencing center . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
massard c , michiels s , fert c , et al : high - throughput genomics and clinical outcome in hardto - treat advanced cancers : results of the moscato 01 trial . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , openlabel , proof - of - concept , randomised , controlled phase 2 trial . 
cheson bd , fisher ri , barrington sf , et al : recommendations for initial evaluation , staging , and response assessment of hodgkin and non - hodgkin lymphoma : the lugano classification . 
barrington sf , mikhaeel ng , kostakoglu l , et al : role of imaging in the staging and response assessment of lymphoma : consensus of the international conference on malignant lymphomas imaging working group . 
kim es , bruinooge ss , roberts s , et al : broadening eligibility criteria to make clinical trials more representative : american society of clinical oncology and friends of cancer research joint research statement . 
druker bj , talpaz m , resta dj , et al : efficacy and safety of a specific inhibitor of the bcr - abl tyrosine kinase in chronic myeloid leukemia . 
slamon dj , leyland - jones b , shak s , et al : use of chemotherapy plus a monoclonal antibody against her2 for metastatic breast cancer that overexpresses her2 . 
bang yj , van cutsem e , feyereislova a , et al : trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of her2 - positive advanced gastric or gastrooesophageal junction cancer ( toga ) : a phase 3 , open - label , randomised controlled trial . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecular profiles : results from mypathway , an open - label , phase iia multiple basket study . 
butler , mph ; kuo guo , ms ; molly holoubek , ccrn ; samiha islam ; linda miller , msn , rn , ocn ; shamika ranasinghe , ms ; brittany m . 
precursors and carcinomas were immunohistochemically compared and analyzed for mutations , gene amplications , microsatellite instability , and tumor mutational burden using an next - generation sequencing panel containing 523 cancer - related genes . 
in addition , presence of fusion genes was analyzed using a panel of 55 genes . results sixty percent of neuroendocrine cases ( 6 / 10 ) presented with a precursor lesion , either intracholecystic papillary neoplasm ( n = 3 ) or biliary intraepithelial neoplasia ( n = 3 )  . 
moreover , nearly half of the ne gbcs carried at least one potentially actionable molecular alteration , highlighting the importance of molecular testing in this highly lethal cancer . jco precis oncol 5 : 473 - 484 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction neuroendocrine neoplasms ( nens ) can arise from almost any anatomical site including , but not limited to , the lung , the prostate , and throughout the gi and hepatobiliary tract . 
two major categories of nens have been described : well - differentiated neuroendocrine tumors ( nets ) and poorly differentiated neuroendocrine carcinomas ( necs ) , the latter being high grade by denition.1 morphologically , necs are classied as either pure small - cell or large - cell nec , and they might also be present together with an adenocarcinoma ( ac ) component . 
they nonneuroendocrine neoplasms ( minens ) when both the neuroendocrine component ( generally nec ) and the non - neuroendocrine component ( generally ac ) comprise at least 30% of the neoplasm.2 regardless of the anatomical site , necs and minens are highly aggressive tumors and carry a dismal prognosis . neuroendocrine as mixed classied necs can either arise de novo or during progression of an epithelial neoplasm , for example , because of a therapy resistance mechanism.3 the molecular features of necs have been best described in lung , pancreas , and prostate , but the cell of origin of necs has been a matter of controversy , specically in tumors with a mixed phenotype ( ie , minens )  . 
this study was approved by the radboud university medical center medical ethics committee ( 2018 - 4126 )  . histopathologic review formalin - xed parafn - embedded ( ffpe ) blocks were selected on the basis of pathology reports and histopathologic review . 
histologic typing and grading , including description of a precursor lesion ( either bilin or icpn ) , was performed using the who histologic classication of tumors of the gallbladder ( fth edition ) .2 t classication was performed using the american joint committee on cancer tumor - node - metastasis classication system ( eighth edition ) .12 additionally , presence of vascular , lymphatic , and perineural invasion was assessed . immunohistochemistry immunohistochemistry ( ihc ) was performed on 4 - mm whole - slide ffpe sections semiautomated using the lab vision autostainer ( immunologic , duiven , the netherlands ) for muc2 , muc5ac , muc6 , and ttf - 1 essentially as described before13 or fully automated using tissue - tek genie ( sakura finetek , torrance , ca ) for chromogranin a , cd56 , ck7 , ck20 , ki - 67 , ema ( muc1 ) , p53 , and synaptophysin with ready - to - use reagents . 
discrepancies in scoring were reevaluated until agreement . nucleic acid extraction for molecular analyses , dna and rna were isolated from ffpe - derived tumor tissue and the precancerous lesion if available . 
dna was isolated , quantied , and precipitated manually as described before.14 after precipitation , the nal concentration was determined using the qubit high sensitivity kit ( thermo fisher scientic , waltham , ma )  . rna was isolated using the reliaprep ffpe total rna miniprep system ( promega , madison , wi ) according to the manufacturers protocol , omitting the dnase treatment step . 
 histologic and molecular features of ne gallbladder cancer subsequently , 60 ng of either dna or rna was used as input for the library preparation . library preparation dna and rna library preparations were performed separately using the hybrid capture - based trusight oncology ( tso ) 500 dna and rna library preparation kits , respectively ( illumina , san diego , ca ) according to the manufacturers protocol essentially as described before.15 the tso500 dna assay targets 523 cancer - related genes for assessment of singleand multiple - nucleotide variants , gene amplications , tumor mutational burden ( tmb ) , and microsatellite instability ( msi ) , whereas the rna kit targets 55 genes for fusion gene analyses ( data supplement )  . 
in short , dna samples were fragmented , and rna samples were used for rstand second - strand cdna synthesis . next , samples underwent end - repair and a - tailing , followed by unique molecular identier ligation and barcoding . two target capture and purication steps , allowing for maximal target enrichment , were followed by polymerase chain reaction amplication and purication . 
libraries were quantied and normalized for uniform library representation . sequencing and data analysis sequencing was performed on a nextseq 500 system ( illumina ) , with 10 dna libraries on a nextseq high - output cassette or 16 rna libraries on a nextseq mid - output cassette . 
the number of gene copies in the tumor cells was estimated on the basis of the relative coverage corrected for the percentage of neoplastic cells in the sample . variant annotation was performed as described before via an in - housedeveloped pipeline.17 variants were ltered by exclusion of ( 1 ) variants outside exons and splice site regions ( 8 / + 8 ) except those in the tert promoter region , ( 2 ) synonymous variants , unless present in a splice site region , ( 3 ) variants present with a frequency of  . 
0.1% in the exac ( version 0.2 ) database , ( 4 ) variants with a variant allele frequency ( vaf ) of , 5% , and ( 5 ) variants with , 5 variant reads . 
remaining variants were manually inspected and curated and classied into ve classes on the basis of their level of evidence for pathogenicity , largely on the basis of american college of medical genetics / association for molecular pathology guidelines18 , 19 : class 1 , not pathogenic ; class 2 , unlikely pathogenic ; class 3 , possibly pathogenic ; class 4 , likely pathogenic ; and class 5 , pathogenic . 
potential effects on splicing were evaluated on the basis of the majority vote of splicesitefinder - like , maxentscan , nnsplice , and genesplicer ( all available from alamut visual version 2.13 [ sophia genetics , lausanne , switzerland ] )  . 
details on classes and their interpretation are provided in figure a1 , online only . variant - specic level 1 , 2 , 3 , or 4 evidence for actionability across all tumor types was derived from oncokb.21 level 1 and 2 biomarkers are dened as fda - recognized or standard care biomarkers , respectively , that are predictive of response to fda - approved drugs in specic tumor types . for level 3a biomarkers , there is compelling clinical evidence of drug response in a specic indication , and level 3b alterations are predictive of response to an fdaapproved or investigational drug in another indication . level 4 alterations comprise alterations for which there is compelling biological evidence that predicts response to a drug . 
seven cases ( 70% ) were pure high - grade net or nec , whereas three tumors ( 30% ) showed both ac and nec features and were classied as minens . 
data on type of systemic therapy are not available . tumors ( 50% ) were large - cell nec , four cases ( 40% ) were small - cell nec , and one case ( 10% ) was a net grade 3 , hereafter collectively referred to as ne gbc . 
in 90% of cases , at least one tumor component ( either nec or , if present , ac ) showed angioinvasion ; lymphatic invasion and perineural invasion were observed in 80% and 30% of cases , respectively . neuroendocrine expression with synaptophysin , chromogranin a , and cd56 conrmed neuroendocrine histology and was absent in the precancerous lesions ( table 2 and fig 1 )  . 
tumor characteristics case diagnosis ptnm ( m location ) icpn ( mixed type ) with nec ( sc ) t2anx bilin with nec ( sc ) t3nx nec ( sc ) t3n2m1 ( liver ) icpn ( intestinal type ) with nec ( lc ) t3n1 icpn ( biliary type ) with minen ( lc ) t2an1 bilin with minen t3nx ( lc ) nec ( lc ) nec ( lc ) t2nx t3nxm1 ( peritoneum ) 476 2021 by american society of clinical oncology abbreviations : + ,  . 
neuroendocrine marker expression with synaptophysin was positive in the nec and negative in the icpn and ac ( chromogranin a and cd56 were comparable ; table 2 ) , whereas epithelial marker expression ( ck 7 ) was positive in the icpn and ac and negative in the nec ( ck20 - negative in all three ; table 2 )  . 
since tp53 is frequently altered in necs of other anatomical origin , case 5 served as an exemplary case for which p53 ihc was performed next to a molecular screening , which was done for all cases . 
both the ac and nec components showed aberrant p53 expression , whereas the icpn component showed predominantly a normal p53 expression with only a small region with overexpression ( fig 1 )  . 
 de bitter et al molecular characteristics discussion for each case , dna and rna were isolated from the precursor lesion , the nec component and , if available , the ac component . 
quality control parameters of dna and rna libraries including reference values are listed in the data supplement . for case 1 , both the nec and icpn components did not meet quality control for msi , tmb , and cnv assessment . all likely pathogenic and pathogenic singleand multiplenucleotide variants ( classes 4 and 5 ) were considered potentially clinically relevant and are listed in figure 2 and the data supplement . 
a variety of other genes harbored potentially clinically relevant mutations in individual cases . mutations in tp53 were shared among the different precursor , ac , and nec components in all but one case ( case 8 ) , where two different mutations were observed in the ac versus the nec . 
interestingly , the icpn of case 5 did share the same tp53 mutation with the invasive tumor components , albeit with a low vaf ( 8.7% ) , reecting the limited region with p53 overexpression ( fig 1 )  . 
three cases ( 30% ) harbored potentially actionable variants ( level 1 ) in atm , brca2 , and rad54l , albeit with a low vaf for the atm variant of case 4 . in six cases , gene amplications were observed in a variety of genes including potentially actionable amplications of erbb2 ( level 1 ) and mdm2 ( level 3a ) , the latter being in a case without a tp53 mutation ( fig 2 )  . 
whereas the majority of mutations were shared among different precancerous , ac , and nec components , for gene amplications this was for a cnne1 amplication that not observed , except was shared between the ac and nec , but not the icpn , of case 5 . a fusion involving fgfr3 and tacc3 genes was observed in all three components of case 5 ( fig 2 )  . 
despite these phenotypical differences , the shared tp53 mutation in the different components in ve of six cases strongly suggests a common origin for neuroendocrine and epithelial components of ne gbc . 
in addition , 50% of the cases also had cholelithiasis , which is a well - known risk factor for pure gallbladder ac , 26 and may further reinforce the concept of a common origother studies of digestive system necs also support the lineage transformation hypothesis with molecular analyses.5 , 27 , 28 nearly all cases had multiple pathogenic or likely pathogenic mutations in a variety of genes with tp53 , ctnnb1 , rb1 , and atm being the most frequently involved . 
our ndings are largely in line with observations in lung , prostate , and pancreatic necs , where tp53 and rb1 are altered in roughly 80% of cases.3 interestingly , also pure gallbladder ac is molecularly highly heterogeneous with tp53 as the most frequently mutated gene ( 47.1% - 59% of cases ) .29 however , large - scale molecular data remain scarce and are mainly derived from endemic regions , which could hamper the extrapolation of ndings to nonendemic regions . gene amplications ( n = 6 cases ) were observed in a subset of cases and were in all but one case not shared between the different components . 
this suggests that , in contrast to mutations that are shared between the precursor and invasive components , oncogenic amplications typically occur as a later event in carcinogenesis , which has been observed before in esophageal ac.30 in case 5 , a ccne1 amplication was shared between the ac and nec , but not the icpn . 
potentially clinically relevant mutations ( class 4 and class 5 ) , gene amplications , fusion genes , microsatellite status , and total tumor mutational burden , identied by tso500 . 
another limitation of this study is the limited information on used therapeutic regimens , such as the type and outcome of adjuvant systemic therapy received by three of the patients , because of the retrospective anonymized nature of this study . in conclusion , we provide a comprehensive histopathologic and molecular overview of a very rare and understudied tumor type . 
ligtenberg employment : synthon ( i ) honoraria : astrazeneca ( inst ) , msd ( inst ) consulting or advisory role : astrazeneca ( inst ) , bayer ( inst ) , bristol - myers squibb ( inst ) , janssen ( inst ) , merck sharp and dohme ( inst ) , novartis ( inst ) , roche ( inst ) , lilly ( inst ) research funding : astrazeneca ( inst ) , bristol - myers squibb ( inst ) no other potential conicts of interest were reported . acknowledgment we would like to thank mandy hermsen , lisa plettenburg , and chinook ophelders for technical assistance ; palga and the ncr for providing data ; and pathology laboratories ( pathan , gelre hospitals , olvg , meander medical center , and martini hospital ) for providing tumor tissue . references rindi g , klimstra ds , abedi - ardekani b , et al : a common classication framework for neuroendocrine neoplasms : an international agency for research on cancer ( iarc ) and world health organization ( who ) expert consensus proposal . 
mod pathol 31 : 1770 - 1786 , 2018 klimstra ds , lam ak , paradis v , et al : tumours of the gallbladder and extrahepatic bile ducts , in who classication of tumours , 5th edition : digestive system tumours . 
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j clin oncol 26 : 3063 - 3072 , 2008 sciarra a , missiaglia e , trimech m , et al : gallbladder mixed neuroendocrine - non - neuroendocrine neoplasm ( minen ) arising in intracholecystic papillary neoplasm : clinicopathologic and molecular analysis of a case and review of the literature . 
meguro y , fukushima n , koizumi m , et al : a case of mixed adenoneuroendocrine carcinoma of the gallbladder arising from an intracystic papillary neoplasm associated with pancreaticobiliary maljunction . 
acosta am , hamedani fs , kajdacsy - balla a , et al : primary mixed adenoneuroendocrine carcinoma of the gallbladder in a 55 - year - old female patient : a case report and review of the literature . 
de bitter tjj , van der linden rla , van vliet s , et al : colorectal metastasis to the gallbladder mimicking a primary gallbladder malignancy : histopathological and molecular characteristics . 
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scardoni m , vittoria e , volante m , et al : mixed adenoneuroendocrine carcinomas of the gastrointestinal tract : targeted next - generation sequencing suggests a monoclonal origin of the two components . 
voss mh , hierro c , heist rs , et al : a phase i , open - label , multicenter , dose - escalation study of the oral selective fgfr inhibitor debio 1347 in patients with advanced solid tumors harboring fgfr gene alterations . 
we completely agree with the authors that better ways of selecting patients with melanoma for snb are required , because approximately 80% of patients who currently have an snb are found to be sn negative . 
improved methods of identifying those at low risk of being sn positive are needed so that they are not unnecessarily subjected to the procedure , while those at higher risk are not excluded . bellomo et al1 propose that using their gene expression prole ( gep ) test will achieve greater accuracy , but we are not convinced that this is correct . 
first , we have several concerns about the statistical methodology used in their study to support the claim that a combination of two clinicopathologic ( cp ) features and an eight - gene test ( a cp - gep model ) improves the accuracy of selecting patients for snb . and second , we have evidence that prognostic estimates of sn status equivalent to or better than those provided by the cp - gep model of bellomo et al1 can be achieved using readily available cp parameters only . one of our statistical concerns is that the study had a relatively small sample size of patients who underwent snb ( n = 754 ) and only 128 were sn positive . the small sample size used for model development may explain why there was no apparent improvement in performance when more complex cp models were used compared with the use of breslow thickness and age only . another statistical concern is that the model reported by bellomo et al1 was assessed only by internal crossvalidation , and external validation was not performed . this is important , because there is a high probability that external validation using an unrelated data set will demonstrate a reduced discrimination ( c statistic ) compared with the development set because models tend to overt the data set on which they were developed.2 the apparent gain in discrimination achieved by the cp - gep model relative to the memorial sloan kettering cancer center ( mskcc ) nomogram ( from 77% to 82% ) is therefore likely to be is externally validated . reduced when the model furthermore , the c statistics had considerable overlap , and there is no evidence that there was a statistically signicant improvement . the 95% cis of in addition , the reported snb reduction rate reported by bellomo et al1 is based upon a negative predictive value ( npv ) threshold of 95% . 
however , the npv of any test decreases as the prevalence of the condition increases ; thus , in practice , it cannot be xed.3 therefore , it would be more informative for both clinicians and patients to indicate the rate reductions of snb with individual risk thresholds rather than the npv . the above statistical concerns , regardless of question of whether the gep test improved prognostic accuracy remains . 
it should be noted that the c statistic obtained by using the mskcc nomogram was considerably higher in the report by bellomo et al1 than in both our study and the original mskcc study , 5 which probably reects selection bias in their study sample that excluded thick tumors . 
the 5% absolute improvement in the c statistic reported in their study combining cp parameters ( two only ) and molecular risk factors ( an eight - gene test ) is less than the 6.2% achieved by our new model , which used cp parameters only . for all of the above reasons , we are not convinced that the addition of gep to cp parameters improves the reliability of sn - positivity estimates . 
scolyer , phd melanoma institute australia and faculty of medicine and health , the university of sydney , sydney , and department of tissue oncology and diagnostic pathology , royal prince alfred hospital and nsw health pathology , camperdown , nsw , australia john f . 
scolyer employment : royal prince alfred hospital consulting or advisory role : bristol myers squibb , glaxosmithkline , merck sharp & dohme , neracare , novartis amgen , myriad genetics , qbiotics research funding : the ainsworth foundation ( inst ) , national health and medical research council travel , accommodations , expenses : bristol myers squibb , novartis john f . 
bellomo d , arias - mejias sm , ramana c , et al : model combining tumor molecular and clinicopathologic risk factors predicts sentinel lymph node metastasis in primary cutaneous melanoma . 
lo sn , ma j , scolyer ra , et al : improved risk prediction calculator for sentinel node positivity in patients with melanoma : the melanoma institute australia nomograj clin oncol 38 : 2719 - 2727 , 2020 5 . 
wong sl , kattan mw , mcmasters km , et al : a nomogram that predicts the presence of sentinel node metastasis in melanoma with better discrimination than the american joint committee on cancer staging systeann surg oncol 12 : 282 - 288 , 2005 6 . 
scolyer ra , judge mj , evans a , et al : data set for pathology reporting of cutaneous invasive melanoma : recommendations from the international collaboration on cancer reporting ( iccr )  . 
the authors stated that there are currently no trials of parp inhibitors in endometrial carcinoma , mainly because mutations in brip1 , brca1 , brca2 , and other homologous recombination ( hr ) related genes are too rare , being reported overall in , 5% of cases.2 in fact , the french group gineco ( groupe dinvestigateurs nationaux pour letude des cancers ovariens ) is conducting a national randomized phase ii trial evaluating olaparib as maintenance therapy in platinumsensitive advanced uterine carcinoma ( utola trial ; clinicaltrials.gov identier : nct03745950 ; fig 1 ) versus placebo . 
we anticipate that patients with endometrial tumors might benet from a parp inhibitor , even in cases of no brca or related genetic mutations . the hr - decient ( hrd ) phenotype was initially characterized in approximately 50% of high - grade serous ovarian carcinomas , and 20% to 25% of these had no brca1 or brca2 mutations.3 importantly , this phenotype is associated with clinical activity of platinum and parp inhibitors in platinumsensitive ovarian carcinomas regardless of brca mutations.4 , 5 according to the cancer genome atlas data , the hrd phenotype was also recently reported in 25% of uterine endometrial carcinomas.6 it is almost exclusively found in the serous - like , tp53 - mutated subtype , in which it represents nearly 50% of cases.7 molecular alterations responsible for the hrd phenotype in endometrial carcinoma have not been largely explored and remain to be identied , because brca1 promoter methylation seems uncommon.7 finally , hr deciency could be induced by platinum - based chemotherapy ; a recent study showed decreased expression of rad51 protein , a key partner of hr , after neoadjuvant chemotherapy in a subset of patients with ovarian cancer.8 in tp53 wild - type endometrioid carcinoma , common molecular alterations such as pten or arid1a loss have been also associated in vitro with signicant parp inhibitor activity.9 , 10 according to these preliminary data , inclusion criteria in the utola trial are not restricted to specic molecular alterations ; rather , patients could be enrolled if their disease is platinum sensitive , a well - recognized landmark of the hrd phenotype . 
patients are stratied according to mrr and tp53 immuno - phenotypes , and a large screening of molecular alterations , including hrd prole , will be conducted to determine the best candidates for parp inhibitor maintenance . in conclusion , we agree with nakamura et al1 that parp inhibitors should be explored in patients with advanced endometrial carcinoma , beyond those with rare mutations in brca or related genes . 
the secondary end points are overall survival , response rate , quality of life , safety , time from random assignment to rst and second subsequent therapies , and time from random assignment to second disease progression or death . 
exploratory analyses included homologous recombinationdecient ( hrd ) phenotype and multiple - gene next - generation sequencing , including brca1 and brca2 and other hrd - related genes ( tp53 , pten , pole , and arid1a ) , and microsatellite instability status . 
nature 474 : 609 - 615 , 2011 [ erratum : nature 490 : 298 , 2012 ] ray - coquard i , pautier p , pignata s , et al : olaparib plus bevacizumab as rstline maintenance in ovarian cancer . 
marquard am , eklund ac , joshi t , et al : pan - cancer analysis of genomic scar signatures associated with homologous recombination deciency suggests novel indications for existing cancer drugs . 
biomark res 3 : 9 , 2015 de jonge mm , auguste a , van wijk lm , et al : frequent homologous recombination deciency in high - grade endometrial carcinomas . 
clin cancer res 25 : 1087 - 1097 , 2019 kubelac p , genestie c , auguste a , et al : changes in dna damage response markers with treatment in advanced ovarian cancer . 
cancers ( basel ) 12 : 707 - 719 , 2020 dedes kj , wetterskog d , mendes - pereira am , et al : pten deciency in endometrioid endometrial adenocarcinomas predicts sensitivity to parp inhibitors . 
the patient , a 33 - year - old man , presented with a primary tumor in the pancreatic tail and metastatic disease in regional and distant lymph nodes ( retroperitoneal , hilar , mediastinal , left supraclavicular ) , liver , and lungs . 
a supraclavicular lymph node core biopsy showed sheets and acini composed of epithelial cells that strongly expressed keratins by immunohistochemistry and had periodic acidschiffpositive diastase - resistant apical granularity . zymogen granules were seen with electron microscopy , consistent with pacc . 
some tumor cells expressed synaptophysin and had electron microscopydetected neurosecretory granules , suggesting possible neuroendocrine differentiation , but this was not conrmed because of limited tumor quantity . multiple lines of cytotoxic therapy were trialed over a 3 - month period because of rapid disease progression and a lack of clinical response . 
concurrently , molecular testing of tumor dna involving the targeted sequencing analysis of 386 cancer - related genes was performed with informed consent ( approval , peter maccallum cancer centre human research ethics committee 17 / 94 )  . testing detected a gatm ( exons 1 - 2 ) - raf1 ( exons 10 - 17 ) fusion that was conrmed by reverse transcriptase polymerase chain reaction / sanger quencing . 
concurrent biallelic cdkn2a - cdkn2b deletion was detected . at the time of obtaining the molecular results , mek inhibitors were reported to be effective against pacc with braf fusions in vitro4 and clinically effective in a melanoma with an raf1 fusion in our institute.3 because cytotoxic chemotherapy had proven ineffective , the patient started receiving trametinib 2 mg orally once daily . 
over a period of 4 weeks , no clinical response was observed , and the patient continued to deteriorate . sorafenib was briey trialed , but the patient had entered the terminal phase of his illness and died 5 months after diagnosis . unlike previously reported patients with oncogenic raf1 fusions , where rapid clinical improvement and tumor regression were observed after mek inhibitor treatment , 1 - 3 the response in this patient was transient and partial . 
available research is conned to case reports or retrospective series , and in the metastatic setting , survival outcomes are generally poor.5 , 6 targetable genomic alterations , such as raf fusions , promise to offer new treatment opportunities . a study of 44 paccs identied raf fusions in 10 patients ( 23% ) , 4 and although in vitro susceptibility to mek inhibition was demonstrated , the clinical efcacy of mek inhibitors or sorafenib has not previously been reported . 
to our knowledge , this study is notable as the rst clinical evaluation of an mek inhibitor in a pacc with a previously unreported gatm - raf1 fusion . biallelic loss of cdkn2a was found in this patient and in two previous raf fusion - positive patients who responded to mek inhibitors.2 , 3 concurrent cdkn2acdkn2b deletion and raf fusions were reported in a subset of paccs4 and anaplastic pleomorphic xanthoastrocytomas.7 it seems that raf fusion - driven mapk activation is commonly associated with both cell cycle dysregulation and p53 - dependent apoptosis because of loss of p16ink4a , p15ink4b , and p14arf . despite this , combined mek and cdk4 / 6 inhibition failed to control disease progression in this patient . potential explanations for this patients lack of response include activation of downstream effectors such as erk , 8 a possible component of neuroendocrine carcinoma or ductal adenocarcinoma lacking the gatm - raf1 fusion , the advanced state of the disease , limited medication absorption due to marked gut dysfunction , and potential impact of the gatm fusion partner . 
mcevoy , phd peter maccallum cancer centre , melbourne , victoria , australia damien kee , mbbs , dmedsc peter maccallum cancer centre , melbourne , and the walter and eliza hall institute of medical research , parkville , victoria , australia owen w.j. 
clay , mbbs ( hons ) , dmedsc st john of god subiaco hospital , subiaco , western australia , australia clare scott , md , phd the walter and eliza hall institute of medical research , parkville , victoria , australia anastasia backhouse , mbbs australian clinical labs , subiaco , western australia , australia stephen b . 
clay honoraria : mundipharma , merck serono , novartis , pzer , roche , astrazeneca speakers bureau : merck sharp & dohme , astrazeneca , novartis travel , accommodations , expenses : merck sharp & dohme , astrazeneca , genentech , bristol - myers squibb clare scott research funding : genentech , clovis oncology , sierra oncology , eisai patents , royalties , other intellectual property : royalty agreement for venetoclax ( inst ) expert testimony : astrazeneca travel , accommodations , expenses : astrazeneca other relationship : clovis oncology anastasia backhouse employment : australian clinical laboratories stephen b . 
kim kb , semrad t , schrock ab , et al : signicant clinical response to a mek inhibitor therapy in a patient with metastatic melanoma harboring an raf1 fusion . 
chmielecki j , hutchinson ke , frampton gm , et al : comprehensive genomic proling of pancreatic acinar cell carcinomas identies recurrent raf fusions and frequent inactivation of dna repair genes . 
brunetti o , aprile g , marchetti p , et al : systemic chemotherapy for advanced rare pancreatic histotype tumors : a retrospective multicenter analysis . pancreas 47 : 759 - 771 , 2018 6 . 
corcoran rb , ebi h , turke ab , et al : egfr - mediated re - activation of mapk signaling contributes to insensitivity of braf mutant colorectal cancers to raf inhibition with vemurafenib . 
guideline - aligned biomarker testing rates for ras , braf , and microsatellite instability / mismatch repair deciency over this study period were 41% , 43% , and 51% , respectively . 
patients were more likely to have guideline - aligned testing for ras and braf if they were treated at an academic center , were diagnosed with de novo metastatic disease , and were female . 
of the 177 patients ( 12% of cohort ) who received antiepidermal growth factor receptor therapy , only 50 ( 28% ) had complete guideline - aligned biomarker testing . conclusion despite guideline recommendations and signicant therapeutic implications , overall biomarker testing rates in mcc remain suboptimal . 
2019 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction the promise of precision oncology requires the application of biomarker testing to direct appropriate clinical care . 
among patients with metastatic colorectal cancer ( mcrc ) , genomic proling may identify somatic mutations that are prognostic for outcomes and / or predictive of response to approved treatments . in 2009 , asco and the national comprehensive cancer network ( nccn ) published guidelines recommending that patients with mcrc undergo testing for activating mutations in codons 12 and 13 of kras exon 2 on the basis of data that patients with these mutations do not derive clinical benet from the antiepidermal growth factor receptor ( anti - egfr ) monoclonal antibody ( mab ) therapies cetuximab and panitumumab.1 , 2 kras exon 2 mutation testing allows oncologists to avoid the use of ineffective anti - egfr therapy in approximately 40% of patients with mcrc who may otherwise receive these drugs as second - line therapy.3 over the subsequent 10 years , biomarker testing guidelines have been expanded ( fig 1 )  . 
testing for mutations in kras exons 3 or 4 and nras exons 2 , 3 , or 4 nds 20% more ras mutations than exon 2 testing alone , adding another 8% of patients with mcrc who will have poor responses to anti - egfr therapy ( fig 2 ) .3 , 4 braf mutations , specically v600e , predict lack of response to cetuximab and panitumumab in another 9%.5 , 6 erbb2 ( her2 ) amplication , present in approximately 2% of mcrc , is also a negative predictor of anti - egfr mab response , increasing the percentage of patients with mcrc in whom these ineffective agents could be avoided to almost 60%.7 , 8 in addition to their clinical utility as negative predictors of cetuximab and panitumumab response , braf mutations and her2 overexpression are positive predictors of response to targeted therapy . 
 gutierrez et al context key objective how often are patients with metastatic colon cancer ( mcc ) receiving guideline - aligned biomarker testing ? knowledge generated this retrospective medical record review of patients treated at academic and community centers in the united states demonstrates that only 40% of patients with mcc received guideline - aligned biomarker testing between 2013 and 2017 . patients were more likely to receive guideline - aligned biomarker testing if they were female , diagnosed at , 65 years of age , treated at an academic center , and diagnosed with de novo metastatic disease . relevance biomarker testing plays an increasingly important role in treatment selection in mcc , and exploring new approaches to increase genotyping rates is essential for improved patient outcomes . response and disease control populations.9 - 12 rates in these specic microsatellite instability ( msi ) is an important predictive biomarker for response to immune checkpoint blockade ( icb ) .13 , 14 in 2018 , the tumor - agnostic approval of pembrolizumab for the treatment of patients with unresectable or metastatic msi high ( msi - h ) solid tumors after progression on prior approved therapies established this critical biomarker to guide icb therapy selection.15 it is also an important screening test for the hereditary cancer syndrome , lynch syndrome , and a prognostic marker in stage ii crc . 
50 years of age in 2011 , and then for patients with mcrc at any age in 2015.16 , 17 although biomarker testing has been advocated for a decade in mcrc guidelines , published testing rates remain low . 
20 , 000 patients in the seer database reported only 30% of patients diagnosed with mcrc in 2010 were tested for kras.19 shaikh et al20 reported 28.2% of patients diagnosed with mcrc between 2010 and 2012 had testing for dmmr . we hypothesize that genomic testing rates for guidelinerecommended biomarkers have improved over time . 
at the time of data extraction , the cota database included demographic , diagnostic , treatment , and quality - of - care information for patients with colon cancer abstracted from the electronic health records from 23 practices including 258 oncologists in arkansas , maryland , michigan , new jersey , new york , and tennessee who contribute data under business associate agreements . 
the electronic exempt medical records of each patient ( all clinical progress notes , laboratory reports , and pathology reports ) were reviewed by trained cota abstractors for any mention of biomarker testing ( including results placed in the record in both structured and unstructured formats , such as scanned pdf les )  . 
we dened a patient as receiving extended ras testing if the laboratory or pathology report indicated analysis of exons 2 , 3 , and 4 for both kras and nras and as limited ras testing if analysis was anything less than exons 2 , 3 , and 4 in both kras and nras . 
fu , uorouracil ; ihc , immunohistochemistry ; mmr , mismatch repair ; msi , microsatellite instability ; msi - h , microsatellite instability high ; nccn , national comprehensive cancer network ; ngs , next - generation sequencing ; pts , patients ; wt , wild type . testing for a given biomarker was considered guideline aligned if the nccn guidelines recommended testing for that biomarker for the entire year being analyzed . guideline - aligned testing in 2013 and 2014 included testing for kras by any methodology , in 2015 included extended testing of nras and kras , and in 2016 and 2017 included extended testing of both kras and nras , braf testing by any methodology , and msi / dmmr analysis by any methodology . 
because the cota database captures limited family history data , we did not include msi / dmmr in the guideline - aligned genotyping analysis until it was recommended for all patients regardless of age or family history . results patient demographics a total of 1 , 497 patients with mcc were identied in the observational database ( table 1 )  . 
of these patients , 1 , 325 ( 89% ) had de novo presentation of metastatic disease , and 172 ( 11% ) had been previously diagnosed with earlier stage colon cancer and became metastatic during the study time frame . 
the patients were treated at 23 centers , including 1 , 152 ( 77% ) at academic cancer centers and 345 ( 23% ) at community cancer centers . overall guideline - aligned biomarker testing guideline - aligned biomarker testing was completed in 40% of patients in this study ( 601 of 1 , 497 )  . 
 ( a ) frequency of mutations identied in expanded ras testing.4 , 20 , 21 ( b ) approximately 60% of patients with metastatic colorectal cancer ( mcrc ) will have a genetic alteration that may predict poor response to anti - egfr monoclonal antibody ( mab ) therapies cetuximab and panitumumab . 
most of these nonresponders will have kras exon 2 mutations , but expanded ras , braf , and erbb2 analysis identies an additional 20% of patients who will not benet from therapy . nras testing by any methodology , with 7% of tested patients harboring an nras mutation ( fig 3 )  . braf testing rates guideline - aligned braf testing was completed in 43% of patients ( 235 of 546 ) in 2016 - 2017 when braf testing was guideline recommended . 
although pcr was the most common testing methodology for kras in 2013 , ngs was the dominant testing methodology for kras after 2013 and for nras and braf throughout this study . 
the the entire period of proportion of patients who had testing for kras , nras , and braf by ngs increased each year over the course of the study ( fig 4 )  . use of anti - egfr therapy in this study , 177 ( 11.8% ) patients received cetuximab or panitumumab between 2013 and 2017 . 
of these patients , 50 ( 28% ) had guideline - aligned testing for ras and braf . sixty - three ( 36% ) were tested for kras by any methodology , 37 ( 21% ) were tested for nras by any methodology , and 44 ( 26% ) were tested for braf by any methodology . 
it is not known whether ras testing occurred before or after initiation of therapy . msi and dmmr testing discussion guideline - aligned dmmr testing was completed in 51% of patients ( 276 of 546 ) in 2016 - 2017 when dmmr testing was recommended for all patients with mcc . 
although the proportion of patients tested for individual markers increased , because guidelines signicantly expanded between 2013 and 2017 , the number of patients receiving guideline - aligned genotyping in 2017 was lower than it was at the start of the study . 
 variable patients female male age groupa , 65 years 65 years race white black asian other 2013 2014 2015 2016 2017 0 - iii stage at diagnosis practice type academic community ras , raf , and mmr biomarker testing in metastatic colon cancer table 1 . 
observed undergenotyping rates in this analysis are consistent with previous reports of kras testing rates ( 30% - 48% ) between 2008 and 2013.18 , 19 , 21 undergenotyping for guideline - recommended biomarkers may place patients at risk for receiving ineffective antiegfr mab therapy and / or missing the opportunity to receive appropriate immunotherapy options . 
however , in this cohort , 72% of patients receiving cetuximab and / or panitumumab were undergenotyped , providing evidence against the hypothesis that low testing rates are explained by patients not being considered for anti - egfr therapy . using the observed real - world mutation rates for kras , nras , and braf ( 62% , 7% , 17% ) , we estimated the proportion of patients who would have been considered candidates for anti - egfr therapies had all patients undergone complete biomarker testing . 
giving anti - egfr therapy to patients who are ras / raf positive poses risks to patients , in particular severe infusion reactions , which occur in 3% of patients given cetuximab and 1% of patients given panitumumab.22a in addition , mab therapies are expensive relative to testing costs . 
guideline - aligned testing in 2013 - 2014 included testing for kras by any methodology , in 2015 included extended testing of nras and kras , and in 20162017 included extended testing of both kras and nras , braf testing by any methodology , and microsatellite instability / mismatch repair deciency ( dmmr ) analysis by any methodology . 
mcc , metastatic colon cancer . although nccn guidelines do not specify a preferred methodology for biomarker testing , a sequential approach to testing multiple biomarkers amplies challenges with tissue insufciency , turnaround time , and cost.23 we saw increased use of ngs for biomarker testing between 2013 and 2017 for kras , nras , and braf . 
if every patient in this study who was tested for at least one biomarker had a tissueor plasma - based ngs panel with comprehensive coverage of 2013 2014 2015 2016 2017 extended ras , braf , and msi , we would have observed a nearly 50% increase in the percentage of patients who had guideline - aligned biomarker testing ( from 40% to 59% )  . 
therefore , additional barriers must exist , preventing adoption of testing in mcc . tissue - based biomarker barriers to molecular testing in mcc have not been well turnaround studied but may include tissue availability , time , physician education / knowledge , cost / insurance coverage , patient preference , and patient eligibility for therapy on the basis of performance status and comorbidities.18 , 24 a qualitative study of oncologists perspectives on kras testing in 2010 found all participating clinicians reported ordering kras testing and endorsed the value of testing , but there was a lack of consensus on test timing and confusion about what tissue sample to test ( fresh v archival and primary v metastatic ) .25 a 2018 survey of us oncologists , pathologists , and surgeons about msi / dmmr testing practices in mcrc found 84% were aware of published guidelines for dmmr / msi testing in patients with mcrc , and 78% followed published guidelines . 
although the majority of physicians ( 69% ) stated they perform universal testing for all patients with mcrc , nearly 30% of physicians selected patients for testing on an individualized basis . 
 ras , raf , and mmr biomarker testing in metastatic colon cancer current study , guideline - aligned testing was signicantly more likely if the patient was diagnosed with de novo metastatic disease . 
more complete testing in patients with de novo metastatic disease versus patients who experienced progression from an earlier stage may suggest challenges in obtaining archival tissue specimens or patient or physician resistance to repeat tissue biopsy related to complication risks or nancial pressures . several well - validated plasma - based ngs assays that include comprehensive analysis of biomarkers from circulating tumor dna ( ctdna ) have demonstrated high sensitivity , specicity , and concordance with tissue genotyping . 
as with tissue genotyping , ctdna testing can predict response to targeted therapies ( msi - high , braf v600e mutated , erbb2 amplied , ntrk fusions ) and lack of response to anti - egfr treatment but may also reduce barriers associated with obtaining archival tissue or rebiopsy ( gupta et al , manuscript in review ) .25a , 26 - 35 given the relative ease of use and rapid turnaround time , plasmabased ngs offers one method of overcoming barriers associated with tissue testing , but other strategies to reduce undergenotyping must be explored , including physician education , implementation of testing protocols like universal msi / dmmr screening , and use of electronic health records to identify patients who require genotyping . there are multiple limitations of this study . 
mainly , the study relied on medical record input for database review . patients whose genomic testing was not documented in the medical record could have led to errors of omission . 
it is also possible that patients had biomarker testing before being referred to the centers included in this data set , and this testing was not documented in the record . 
in addition , data were collected only on patients with colon cancer . guideline recommendations for kras , nras , braf , and msi all specify testing for metastatic colorectal cancer . 
prior studies suggest that patients with rectal cancer are tested less frequently than those with colon cancer.19 therefore , true testing rates for mcrc may be lower than what is presented in this mcc study . 
this is an important factor that should be further explored in diverse patient cohorts . mutation - positive rates reported for kras , nras , and braf in this study were higher than previously published literature , including a large cohort of mcrc tumors sequenced by msk - impact , which cites kras , nras , and braf mutation rates of 45% , 4% , and 12% , respectively.36 we acknowledge a potential for positive result bias , with physicians documenting positive results in their clinical notes more often than negative results . 
there may have been factors such as treatment ineligibility or refusal that contributed to undergenotyping rates . the results of this study indicate that adherence to evidence - based biomarker testing guidelines in mcc remains poor in both academic and community settings in the united states , with only 40% of patients completing guideline - aligned biomarker testing . 
 gutierrez et al open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . consulting or advisory role : forward medical research funding : guardant health martin e . 
gutierrez stock and other ownership interests : cota healthcare honoraria : foundation medicine , guardant health consulting or advisory role : exenex speakers bureau : bristol - myers squibb , merck , eli lilly research funding : bristol - myers squibb ( inst ) , merck ( inst ) , incyte ( inst ) , nextcure ( inst ) , pzer ( inst ) , genentech ( inst ) , boehringer ingelheim ( inst ) , gsb pharma ( inst ) , moderna therapeutics ( inst ) , eisai ( inst ) , silenseed ( inst ) , seattle genetics ( inst ) , regeneron ( inst ) , sano ( inst ) , johnson & johnson ( inst ) , medimmune ( inst ) , checkpoint therapeutics ( inst ) travel , accommodations , expenses : guardant health kristin s . 
nagy employment : guardant health stock and other ownership interests : guardant health irfan shah employment : cota healthcare stock and other ownership interests : guardant health michael mulcahy employment : cota healthcare andrew d . 
goldberg employment : cota healthcare stock and other ownership interests : cota healthcare research funding : celator pharmaceuticals ( inst ) , bristol - myers squibb ( inst ) , novartis ( inst ) no other potential conicts of interest were reported . references allegra cj , jessup jm , somereld mr , et al : american society of clinical oncology provisional clinical opinion : testing for kras gene mutations in patients with metastatic colorectal carcinoma to predict response to anti - epidermal growth factor receptor monoclonal antibody therapy . 
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 phase i study of the braf inhibitor vemurafenib in combination with the mammalian target of rapamycin inhibitor everolimus in patients with braf - mutated malignancies vivek subbiah shiraj sen kenneth r . 
are co - first authors and contributed equally to this work . the funders had no role in the design of the study ; the collection , analysis , and interpretation of the data ; the writing of the article ; and the decision to submit the article for publication . corresponding author : vivek subbiah , md , department of investigational cancer therapeutics ( phase i clinical trials program ) , unit ( continued ) purpose parallel activation of the phosphatidylinositol 3 - kinasemammalian target of rapamycin pathway represents a mechanism of primary and acquired resistance to braf - targeted therapy , but the two pathways have yet to be cotargeted in humans . 
we performed a phase i study to evaluate the safety and activity of the braf inhibitor vemurafenib in combination with the mammalian target of rapamycin inhibitor everolimus in braf - mutated advanced solid tumors . patients and methods we performed a 3 + 3 dose - escalation study with escalating doses of both oral ( po ) vemurafenib administered twice a day and po everolimus administered daily . results twenty patients with advanced cancers were enrolled . 
 patients were heavily pretreated with prior braf or mek inhibitors ( n = 11 ) , phase i clinical trial therapy ( n = 10 ) , surgery ( n = 18 ) , radiation therapy ( n = 11 ) , and chemotherapy ( n = 13 )  . 
one of the two pediatric patients initially experienced grade 3 rash , but after dermatologic intervention , the patient remains on trial with partial response and no dose reduction at time of analysis . 
one pediatric patient with pleomorphic xanthroastrocytoma remains on protocol with continued clinical response after 38 cycles . conclusion the combination of vemurafenib 720 mg po twice a day and everolimus 5 mg po daily is safe and well tolerated and has activity across histologies , with partial responses noted in advanced nonsmall - cell lung cancer , melanoma , optic nerve glioma , and xanthroastrocytoma , including patients who previously experienced progression on braf and / or mek inhibitor therapy . 
a recent basket study of vemurafenib demonstrated clinical activity in patients with advanced nonmelanoma cancers.8 unfortunately , many patients exhibited primary and acquired resistance to therapy . reactivation of mapk signaling and activation of alternative parallel signaling pathways such as the phosphatidylinositol 3 - kinase ( pi3k ) mammalian target of rapamycin ( mtor ) pathway have been hypothesized to contribute to primary and acquired resistance to braf - targeted therapy.9 , 10 specifically , akt mutation , 9 pten deficiency , 11 and downstream mtor activation have been implicated in resistance to both vemurafenib and dabrafenib in metastatic melanoma , both clinically and in preclinical models.12 , 13 preclinical studies have demonstrated efficacy in dual targeting of both the mapk and pi3kmtor pathways in various tumor types.14 , 15 we also recently identified a strong association between co - occurring pi3k - mtor pathway aberrations and primary resistance to braf targeted therapy . 
all patients were treated at the clinical center for targeted therapy at the university of texas md anderson cancer center from september 2013 to august 2015 and met all the eligibility criteria . 
patients who had a myocardial infarction within 3 months before starting treatment , who were pregnant or breastfeeding , or who had undergone a major surgical procedure within 28 days were excluded . 
palliative radiation therapy was allowed during the study treatment . study design and treatment this study was a nonrandomized , open - label , standard 3 + 3 dose - escalation study of oral ( po ) vemurafenib , starting at a dose of 720 mg daily , and po everolimus , starting at a dose of 5 mg daily , for 28 days . 
the primary objectives were to determine the safety , mtd , and dose - limiting toxicity ( dlt ) of the combination of vemurafenib and everolimus in patients with braf - mutated advanced cancer . 
 two pediatric patients were enrolled onto this study and were treated with vemurafenib po 480 mg daily and everolimus po 2.5 mg daily , per body surface areabased dose adjustment . if a patient experienced new grade 3 or greater toxicity , treatment was withheld until the condition was addressed and it recovered to grade 1 or baseline . 
the patients continued treatment until they experienced disease progression or intolerable toxicities , until the treating physician or patient felt that it was not in the patients best interest to continue for any reason , or until consent was withdrawn for any other reason . all patients were evaluated for dlts during the first 28 days and evaluated in clinic every 28 days before initiation of each subsequent cycle . 
dlts were treatment - related grade 3 or 4 nonhematologic toxicities , as defined by the national cancer institute common terminology criteria for adverse events version 3.0 , or grade 4 hematologic toxicities lasting > 7 days or accompanied by fever or bleeding during the first 4 weeks of therapy . 
clinical laboratory improvement amendments ( clia ) certified next generation sequencing data were collected for each patient . response to therapy was assessed using response evaluation criteria in solid tumors ( recist ) version 1.1. 
median time to disease progression and os duration were determined using the kaplan - meier method . circulating tumor dna three patients agreed to have an optional blood draw to measure circulating tumor dna ( ctdna ) at baseline and at each restaging . 
at least 8 ng of unamplified cell - free dna were tested with a droplet digital polymerase chain reaction brafv600e mutationspecific assay and / or multiplex brafv600 screening kit ( bio - rad , hercules , ca ) to distinguish the wild - type allele from the three most common mutations ( brafv600e , brafv600k , and brafv600r ) using the qx200 droplet digital pcr system ( bio - rad ) according to the manufacturers standard protocol . 
planned dose schedule in patients who received the combination of vemurafenib and everolimus in a phase i study dose level vemurafenib orally twice a day ( mg ) everolimus orally once a day ( mg ) * body surface area - based dose adjustment was made ( level 1 ) for pediatric patients dose level 1 was the recommended phase ii dose . frequency for the multiplexed screening assay and < 0.1% mutant allele frequency per single well for the mutation - specific assays . results patient characteristics the demographics and clinical characteristics of the 20 patients who received at least one dose of vemurafenib and everolimus and completed the dlt window are listed in table 2 . 
the most common tumor types were melanoma ( n = 7 ) , glioma ( n = 5 ) , and thyroid cancer ( n = 4 ) , and one patient each had appendiceal cancer , colorectal cancer , nsclc , and unknown primary cancer . 
patients were heavily pretreated with prior therapies , including braf or mek inhibitor therapy ( n = 11 ) , prior phase i clinical trial therapy ( n = 10 ) , surgery ( n = 18 ) , radiotherapy ( n = 11 ) , and chemotherapy ( n = 13 )  . 
one patient had measurable disease but not evaluable disease , and a second patient was not evaluable as a result of withdrawing consent before the first restaging , but both patients cleared the toxicity window and therefore are included in the toxicity evaluation but not in the response evaluation . safety all 20 patients were evaluated for dlts . 
 five patients ( 25% ) had everolimus dose reductions throughout their therapy as a result of toxicity , and one patient had the vemurafenib dose reduced as a result of renal insufficiency . 
two patients without dlts withdrew consent before disease progression . response of the 18 patients evaluable for response , 11 patients ( 61% ) had objective tumor volume reduction as best response . 
two patients were not evaluable for response ; one patient had measurable but not evaluable disease and a second patient completed the dlt window but withdrew consent before restaging . prs were seen in patients with nsclc , melanoma , optic nerve glioma , and pleomorphic xanthroastrocytoma . 
of the nine patients who had disease progression on braf or mek inhibitors before enrolling onto this study , two ( 22% ) had prs and five ( 56% ) had stable disease with vemurafenib and everolimus . at the time of analysis , 14 patients ( 78% ) had discontinued therapy because of disease progression . 
 ( b ) representative restaging images of a patient with metastatic melanoma and a pten ( p95s ) mutation who had a partial response on vemurafenib and everolimus after disease progression on vemurafenib and px866 , an investigational pi3k inhibitor . 
astro , anaplastic astrocytoma ; at , anaplastic thyroid ; crc , colorectal cancer ; cup , cancer of unknown primary ; glio , glioblastoma ; glioma , optic nerve glioma ; mel , melanoma ; pt , papillary thyroid . prior braf or mek inhibitor use no prior braf or mek inhibitor use still on trial without progression pleomorphic xanthroastrocytoma remains on protocol with continued clinical response after 38 cycles . genomic profiling all evaluable patients underwent clia - certified clinical next - generation sequencing of at least 50 genes before trial enrollment . 
among the four patients who achieved pr , a patient with metastatic melanoma who had previously experienced progression on vemurafenib plus an investigational pi3k inhibitor ( px866 ) had a concurrent pten ( p95s ) mutation . 
a patient with nsclc whose tumor harbored an idh1 ( r132c ) mutation , arid2 alteration ( splice site 92 + 1 g > a ) , and ppp1r2a mutation ( r183w ) achieved a pr after previously experiencing progression on dabrafenib . 
all concurrent molecular aberrations and best response to therapy for each patient are listed in table 4 . circulating tumor dna patients enrolled onto this study were offered an optional blood draw to measure ctdna throughout the course of the study . 
 a third patient with a brafv600e mutation had detectable ctdna levels , which were measured at four time points throughout therapy and are depicted in figure 2 alongside the patients scans . 
dlts included fatigue ( 20% ) and rash ( 15% ) , but both were present in only one patient at the mtd and recommended phase ii dose of vemurafenib 720 mg twice daily and everolimus 5 mg daily . 
 the patient with glioblastoma who experienced a grade 3 rash had a resolution of his rash after initial everolimus discontinuation and was able to resume everolimus at a dose of 2.5 mg daily without toxicity . 
 the use of nonpharmacologic approaches , such as physical and mindfulness - based exercise therapy , 20 , 21 and pharmacologic approaches , such as corticosteroids22 in treating cancerand therapy related fatigue , has recently demonstrated efficacy in randomized controlled trials and may benefit these patients moving forward . we observed only one metabolic adverse event ( hypertriglyceridemia and hyperglycemia ) , which is attributed to mtor inhibitors . 
overall , most patients at the recommended phase ii dose tolerated the treatment well . our trial also demonstrates that the addition of an mtor inhibitor to everolimus treatment is able to overcome resistance to braf and / or mek inhibition in a subset of patients with braf - mutant advanced cancers . 
graphical depiction of a patients circulating tumor dna level of brafv600e ( shown as copies per milliliter of plasma ) while on treatment with vemurafenib plus everolimus with representative restaging scans and response to therapy , per response evaluation criteria in solid tumors ( recist ) 1.1. 
pd , progression of disease ; pr , partial response . baseline baseline july 16 , 2014 october 14 , 2014 november 12 , 2014 december 10 , 2014 the 20 patients in this study had a pr to therapy . 
 next - generation sequencing performed at the time of initial diagnosis revealed idh1 ( r132c ) , arid2 ( splice site 92 + 1 g > a ) , and ppp1r2a ( r183w ) aberrations . 
unfortunately , no molecular profiling was available at the time the patient experienced progression on dabrafenib immediately before enrolling onto this trial . a second patient with metastatic melanoma and a pten ( p95s ) mutation who had recently had disease progression on vemurafenib and px866 , an investigational pi3k inhibitor , also achieved a pr on our trial ( fig 1b )  . 
in vivo , pten - deficient , braf - mutated mouse models treated with vemurafenib and pi3k inhibitors also demonstrate synergistic antitumor activity.23 interestingly , this patient experienced progression on the vemurafenib and investigational pi3k inhibitor combination but responded with a pr to vemurafenib and everolimus . 
a 78 - year - old patient with metastatic papillary thyroid cancer whose tumor harbored a pik3ca ( h1047r ) mutation had 7 months of stable disease with a 27% reduction in tumor burden before having any disease progression . 
both of these patients had no co occurring genomic alterations identified on their tumors other than the brafv600e mutation , illustrating the fact that although co - occurring alterations may lead to activation of parallel signaling pathways that increase resistance to therapy in some patients , they may render other tumors susceptible to therapy when actionable . we have previously reported our institutions experience with implementing multiplex hotspot testing and the need to enroll patients onto genotype - matched trials when feasible.24 a number of the responders on this trial further support the hypothesis that the identification of actionable alterations can help guide the right patient to the right targeted therapy . 
all nonresponders were either previously treated with braf or mek inhibitor or harbored non - v600 braf mutations . in the patient with metastatic melanoma with measurable ctdna , the level of mutated brafv600e copies per milliliter decreased with clinical response and increased before subsequent restaging that demonstrated disease progression . 
previous studies have identified an association between detection and levels of circulating tumor dna and disease burden and survival across braf and mek inhibitor trials.27 it is plausible that this may explain why only wildtype braf was detectable in the plasma of these two patients . vitro data suggest that the combination of mek and mtor inhibition may be more effective than braf and mtor inhibition in activating bax and caspase - 3 and inducing caspase - dependent apoptosis in melanoma cell lines.31 future studies to investigate the safety and effectiveness of combining everolimus with both braf and mek inhibitors together are being planned . our study has several limitations , including a small patient population and the variety of molecular profiling platforms used . 
although all patients underwent clia - certified next generation sequencing of at least 40 genes , including those in the pi3k - mtor pathway , some patients underwent more extensive 400gene profiling . 
ideally , all patients should have a broader panel of testing to identify all actionable aberrations , both at the time of study initiation and at disease progression , to better understand the clonal evolution of tumors treated with vemurafenib and everolimus . 
 sherman , patrick hwu manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors in conclusion , the combination of vemurafenib and everolimus is safe and well tolerated and has clinical activity across histologies , with prs noted in patients with advanced nsclc , melanoma , optic nerve glioma , and xanthroastrocytoma . 
our results do not support the addition of everolimus based solely on alterations in the pi3k - mtor pathway ; however , given the responders who did harbor concurrent mutations in this pathway , further investigation in a larger cohort of molecularly matched patients with uniform genomic profiling is warranted . 
hess no relationship to disclose filip janku stock and other ownership interests : trovagene consulting or advisory role : deciphera , trovagene , novartis , sequenom , foundation medicine , guardant health , immunome research funding : novartis , biomed valley discoveries , roche , agios , astellas pharma , deciphera , symphony evolution , plexxikon , piqur , fujifilm other relationship : bio - rad david s . 
hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack , bayer consulting or advisory role : baxter , bayer , guidepoint global , janssen speakers ' bureau : genentech , janssen oncology research funding : novartis , genentech , eisai , astrazeneca , pfizer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer , bristol - myers squibb , genmab , ignyta , infinity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo , medimmune , molecular templates , takeda travel , accommodations , expenses : loxo , mirna therapeutics other relationship : oncorena , eisai soumen khatua no relationship to disclose research funding : phosplatin therapeutics travel , accommodations , expenses : phosplatin therapeutics javier munoz consulting or advisory role : kite pharma , pfizer , pharmacyclics , bayer , alexion pharmaceuticals , bristolmyers squibb , janssen , seattle genetics , gilead sciences , kyowa hakko kirin speakers ' bureau : kite pharma gerald s . 
falchook employment : sarah cannon research institute , healthone research funding : millennium , emd serono , celgene , medimmune , genmab , vegenics , novartis , astrazeneca , incyte , armo biosciences , kolltan pharmaceuticals , 3 - v biosciences , abbvie , aileron therapeutics , delmar pharmaceuticals , effector therapeutics , strategia therapeutics , fujifilm , hutchison medipharma , regeneron , biothera , curegenix , curis , eli lilly , jounce therapeutics , oncomed , precision oncology , syndax , taiho pharmaceutical , tesaro , takeda , beigene , ignyta , merck , rgenix , tarveda therapeutics , tocagen patents , royalties , other intellectual property : handbook of targeted cancer therapy travel , accommodations , expenses : millennium , sarah cannon research institute , emd serono , bristol - myers squibb roman groisberg no relationship to disclose apostolia m . 
tsimberidou consulting or advisory role : roche research funding : emd serono ( inst ) , baxter ( inst ) , foundation medicine ( inst ) , onyx ( inst ) , bayer ( inst ) , boston biomedical ( inst ) , placon ( inst ) , immatics ( inst ) , karus therapeutics ( inst ) , stem cells ( inst ) , obi pharma ( inst ) steven i . 
 support prior presentation presented in part at the 52nd annual meeting of the american society of clinical oncology , chicago , il , june 3 - 7 , 2016 . references 417 : 949 - 954 , 2002 1 . 
turski ml , vidwans sj , janku f , et al : genomically driven tumors and actionability across histologies : braf - mutant cancers as a paradigmol cancer ther 15 : 533 - 547 , 2016 3 . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) - mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
subbiah v , kreitman rj , wainberg za , et al : dabrafenib and trametinib treatment in patients with locally advanced or metastatic braf v600 - mutant anaplastic thyroid cancer . 
nazarian r , shi h , wang q , et al : melanomas acquire resistance to b - raf ( v600e ) inhibition by rtk or n - ras upregulation . 
gopal yn , rizos h , chen g , et al : inhibition of mtorc1 / 2 overcomes resistance to mapk pathway inhibitors mediated by pgc1 and oxidative phosphorylation in melanoma . 
greger jg , eastman sd , zhang v , et al : combinations of braf , mek , and pi3k / mtor inhibitors overcome acquired resistance to the braf inhibitor gsk2118436 dabrafenib , mediated by nras or mek mutations . 
faber ac , coffee em , costa c , et al : mtor inhibition specifically sensitizes colorectal cancers with kras or braf mutations to bcl - 2 / bcl - xl inhibition by suppressing mcl - 1 . 
sen s , meric - bernstam f , hong ds , et al : co - occurring genomic alterations and association with progression - free survival in brafv600 - mutated nonmelanoma tumors . 
subbiah v , westin sn , wang k , et al : targeted therapy by combined inhibition of the raf and mtor kinases in malignant spindle cell neoplasm harboring the kiaa1549 - braf fusion protej hematol oncol 7 : 8 , 2014 20 . 
yennurajalingam s , frisbee - hume s , palmer jl , et al : reduction of cancer - related fatigue with dexamethasone : a double - blind , randomized , placebo - controlled trial in patients with advanced cancer . 
bonnevaux h , lemaitre o , vincent l , et al : concomitant inhibition of pi3k and braf or mek in pten - deficient / braf - mutant melanoma treatment : preclinical assessment of sar260301 oral pi3k - selective inhibitor . 
santiago - walker a , gagnon r , mazumdar j , et al : correlation of braf mutation status in circulating - free dna and tumor and association with clinical outcome across four brafi and meki clinical trials . 
janku f , claes b , huang hj , et al : braf mutation testing with a rapid , fully integrated molecular diagnostics systeoncotarget 6 : 26886 - 26894 , 2015 29 . 
penna i , molla a , grazia g , et al : primary cross - resistance to brafv600e - , mek1 / 2and pi3k / mtor - specific inhibitors in braf - mutant melanoma cells counteracted by dual pathway blockade . 
 o development and validation of a clinical polygenic risk score to predict breast cancer risk elisha hughes , phd1 ; placede tshiaba , ms1 ; shannon gallagher , mph1 ; susanne wagner , phd1 ; thaddeus judkins , ms1 ; benjamin roa , phd1 ; eric rosenthal , phd , ms1 ; susan domchek , md2 ; judy garber , md , mph3 ; johnathan lancaster , md , phd1 ; jeffrey weitzel , md4 ; allison w . 
lanchbury , phd1 ; alexander gutin , phd1 ; and mark robson , md6 purpose women with a family history of breast cancer are frequently referred for hereditary cancer genetic testing , yet , 10% are found to have pathogenic variants in known breast cancer susceptibility genes . 
largescale genotyping studies have identied common variants ( primarily single - nucleotide polymorphisms [ snps ] ) with individually modest breast cancer risk that , in aggregate , account for considerable breast cancer susceptibility . 
candidate polygenic risk scores ( prss ) as predictors of personal breast cancer history were developed through multivariable logistic regression models adjusted for age , cancer history , and ancestry . 
an optimized prs was validated in 2 independent cohorts ( n = 13 , 174 ; n = 141 , 160 )  . results within the training cohort ( n = 24 , 259 ) , 4 , 291 women ( 18% ) had a personal history of breast cancer and 8 , 725 women ( 36% ) reported breast cancer in a rst - degree relative . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction although breast cancer ranks among the cancer types with the highest heritability , 1 characterization of the incomplete . 
pathounderlying genetic causes is still genic variants in high - penetrance genes ( eg , brca1 , brca2 , palb2 ) associated with substantial increases in risk are individually rare in the general population.2 - 4 all known highand moderate - penetrance breast cancer susceptibility genes are estimated to account for a combined 20% of familial relative risk.5 as a result , most women who are referred for hereditary cancer genetic testing are negative for a pathogenic variant and without a clear understanding of the magnitude of their risk.6 genome - wide association studies ( gwas ) have identied several hundred , common , single - nucleotide polymorphisms ( snps ) as breast cancer susceptibility variants.7 - 11 although their individual contribution to risk is minor , polygenic risk scores ( prss ) of such variants can dene variant combinations with potentially actionable clinical risk.9 , 11 together , pathogenic variants in highand moderate - risk genes and panels of snps are estimated to explain up to 40% of the familial risk for developing breast cancer.11 the rst well - characterized prs combined 77 snps ( prs77 ) and was evaluated in  . 
this prs was highly predictive of breast cancer in two independent validation cohorts . relevance prss that aggregate genotypes from common variants have emerged as a new approach to improve breast cancer risk assessment . 
we developed and validated an 86 - snp score that was adjusted for family breast cancer history and was highly predictive of breast cancer risk , making it appropriate for clinical use to identify women at increased risk of developing breast cancer . recently , a polygenic score of 313 snps was deduced from the same gwas and then validated in an independent population cohort.11 the same study also supported previous work indicating snp - based risk scores may have to be optimized depending on breast cancer estrogenreceptor ( er ) status . 
composition and individual contribution of variants of the ideal snp - based breast cancer risk score remain to be dened . family history ( fh ) of breast cancer , a combination of biologic , social , and environmental factors , includes a genetic component that is expected to overlap with snpbased risk.9 , 11 to avoid double counting of risk due to correlation between genetic components of fh and prs , joint modeling of both genetic factors is required . 
here , we describe the development and validation of a prs in which we co - estimate snp - based risk and familial risk to obtain effect sizes independent of fh . 
additional details are provided in the data supplement . snp genotyping amplicons for 94 snp markers published at the time of this study were incorporated into a next - generation sequencing panel.8 , 9 two markers failed design due to their location within repetitive elements , leaving 92 markers for evaluation . 
clinical information from provider - completed test request forms included ancestry , personal and family cancer history , cancer type ( s ) , and age ( s ) at diagnosis . 
 clinical polygenic risk score for breast cancer previous work supports a multiplicative model as the best method for capturing the combined snp effects.9 , 11 we centered the multiplicative model according to generalpopulation allele frequencies so the or for an individual patient represents the fold - change in risk relative to the general population . 
patient clinical characteristics validation study tested the association of the prs with invasive breast cancer after adjusting for age , personal and family cancer history , and ancestry . in exploratory analyses , we assessed the predictive ability of the optimized prs compared with a previously described prs77 by adding both to a multivariable model . 
the observed versus theoretical effect of the prs on breast cancer risk under the multiplicative polygenic model was assessed by comparing ors from the continuous prs with those obtained from analysis of patients binned in categories according to prs percentiles . 
heterogeneity of the prs effect size according to age , ancestry , and fh of breast cancer was evaluated by tting additional interaction terms and by repeating the primary analysis restricted to subcohorts stratied by age , ancestry , and fh severity . 
overall , 8 , 725 patients ( 36% ) reported a breast cancer diagnosis in 1 rst - degree relative and 13 , 230 ( 55% ) had no rst - degree relatives with breast or ovarian cancer . effect sizes and population frequencies were used to rank 92 susceptibility variants by their informativeness and to construct a polygenic score by successive addition of the most informative variant . 
distribution of relative risks , or fold changes , in breast cancer risks due to the 86 - snp score in unaffected women was similar between the rst and second validations ( data supplement figures s1 and s2 )  . 
ors for developing breast cancer by 86 - snp score percentile in each of the two validation cohorts are given in table 2 . consistently , women in the top 95th percentile of the 86snp score distribution had a more than 2 - fold higher risk of breast cancer development than women with an average 80 86 snps ranked by informativeness * fig 1 . 
effect sizes of the 86 - snp score were consistent across subcohorts stratied by age ( table 3 ; data supplement figure s4 ) , ancestry ( data supplement table s3 ) , and fh ( table 4 ; data supplement figure s5 ) in both validation cohorts . 
these results indicate the simple multiplicative model remains the best method for capturing the risk conferred by the combined effects of snps after accounting for family cancer history . discussion prss aggregating genotypes from common variants offer new ways to improve breast cancer risk assessment and can contribute to better understanding of breast cancer risk in all women . 
modication of risk estimates by prs - based stratication has been shown in a variety of clinical settings , including women who carry a pathogenic variant , high - risk women , and population cohorts.11 , 15 - 17 these novel tools , however , are of particular interest to women who present for genetic risk assessment with increased risk due to a fh of breast cancer . 
fh and susceptibility variants contribute independently to risk prediction , yet the approximately 13% reduction in the or for fh when adjusted for the prs77 ( or prs313 ) indicates an overlapping contribution to risk.9 , 11 , 18 adjustment for this correlation between snps and fh can be achieved by co - estimating ors from multivariable models . 
the reported interaction was only signicant in er - positive disease , a subanalysis not available in our data set.11 since the inception of this study , additional breast cancer risk variants have been described , and expanded breast cancer prss have been evaluated and validated in independent data sets.10 , 11 the enlarged prss are estimated to account for a larger fraction of familial risk and promise observed theoretical observed theoretical > 1 - 5 5 - 10 10 - 20 20 - 40 40 - 60 60 - 80 80 - 90 90 - 95 95 - 99 > 99 > 1 - 5 5 - 10 10 - 20 20 - 40 40 - 60 60 - 80 80 - 90 90 - 95 95 - 99 > 99 percentiles of the 86 - snp score percentiles of the 86 - snp score fig 2 . 
the approach described here of co - estimation in multivariate models could be applied to any emerging prs , irrespective of number of variants or ancestral origin . among the strengths of this study are the use of large , contemporary , and fully independent cohorts for development and 2 validation studies . 
thus , to our knowledge , the 86 - snp score is the rst prs with an snp component adjusted for fh and , as such , would be an appropriate addition to conventional clinical models . limitations of the study include the inability to apply the 86snp score to patients of non - european ancestry because changes in genetic structure and linkage disequilibrium may affect the predictive ability of individual risk variants when present in a different ancestral background . 
although association studies with equivalent explanatory power in other ancestries have yet to be described , they are the subject of ongoing research and the expansion of breast cancer prs to other ancestries is a high priority . 
however , previous studies have demonstrated that unbiased risk estimates can be obtained from analysis of a clinical testing population through multivariable adjustment for the factors related to ascertainment.14 , 19 although the 86 - snp score described here adjusted for fh , genetic factors are not the sole contributors to breast cancer risk , even in cohorts with exceptional fh . 
validated clinical risk models incorporate variables such as body mass index , age at menarche , parity , age at rst birth and hormone replacement therapy use , as well as details of fh.20 - 23 other important risk factors , such as mammographic density and diet , are not taken into account here.24 - 26 more studies will be needed to accommodate these additional variables and to determine their dependent contributions . 
lanchbury data analysis and interpretation : elisha hughes , placede tshiaba , shannon gallagher , susanne wagner , benjamin roa , eric rosenthal , susan domchek , judy garber , jeffrey weitzel , allison w . 
komen for the cure ( i ) , american association for cancer research , diane helis henry medical foundation , james p . wilmot foundation ( i ) , adrienne helis malvin medical research foundation ( i ) , breast cancer research foundation , facing our risk of cancer empowered johnathan lancaster employment : myriad genetics , regeneron stock and other ownership interests : myriad genetics , regeneron jeffrey weitzel speakers bureau : astrazeneca allison w . 
jama 315 : 68 - 76 , 2016 peto j , collins n , barfoot r , et al : prevalence of brca1 and brca2 gene mutations in patients with early - onset breast cancer . 
j natl cancer inst 91 : 943 - 949 , 1999 anglian breast cancer study group : prevalence and penetrance of brca1 and brca2 mutations in a population - based series of breast cancer cases . 
 hughes et al collaborative group on hormonal factors in breast cancer : familial breast cancer : collaborative reanalysis of individual data from 52 epidemiological studies including 58 , 209 women with breast cancer and 101 , 986 women without the disease . 
j mammary gland biol neoplasia 9 : 221 - 236 , 2004 desmond a , kurian aw , gabree m , et al : clinical actionability of multigene panel testing for hereditary breast and ovarian cancer risk assessment . 
michailidou k , beesley j , lindstrom s , et al : genome - wide association analysis of more than 120 , 000 individuals identies 15 new susceptibility loci for breast cancer . 
am j hum genet 104 : 21 - 34 , 2019 judkins t , leclair b , bowles k , et al : development and analytical validation of a 25 - gene next generation sequencing panel that includes the brca1 and brca2 genes to assess hereditary cancer risk . 
li h , feng b , miron a , et al : breast cancer risk prediction using a polygenic risk score in the familial setting : a prospective study from the breast cancer family 17 . 
n aslund - koch c , nordestgaard bg , bojesen se : common breast cancer risk alleles and risk assessment : a study on 35 441 individuals from the danish registry and kconfab . 
cuzick j , brentnall ar , segal c , et al : impact of a panel of 88 single nucleotide polymorphisms on the risk of breast cancer in high - risk women : results from two randomized tamoxifen prevention trials . 
lindstr om s , thompson dj , paterson ad , et al : genome - wide association study identies multiple loci associated with both mammographic density and breast cancer risk . 
 high - content biopsies facilitate molecular analyses and do not increase complication rates in patients with advanced solid tumors purpose precision oncology relies on frequent pathologic , molecular , and genomic assessments of tumor tissue to guide treatment selection , evaluate pharmacodynamic effects of novel agents , and determine drug resistance mechanisms . 
it remains unknown how the need for serial biopsies with large numbers of tumor cores relates to tissue yields and biopsy complication rates . materials and methods in this study , we performed a retrospective analysis of 199 focal liver biopsies performed in 143 patients in the setting of oncologic research protocols ( research biopsy group ) over a 4 - year period at a single - intervention oncology service . 
practice patterns and complication rates were compared with those related to 1 , 522 consecutive biopsies performed in 1 , 154 patients in whom two cores were obtained for standard clinical management of patients ( standard biopsy )  . results in the research biopsy group , 1 , 100 tissue cores ( average , 5.5 cores per procedure ) were harvested and distributed to trial sponsors , internal research laboratories , and pathology services . 
in the standard biopsy control group , major complications were observed in 1.4% of procedures ( 22 of 1 , 522 ) and minor complications in 0.2% ( three of 1 , 522 )  . 
2017 by american society of clinical oncology introduction precision oncology aims to adapt treatment decisions based on the molecular characteristics of an individual tumor , thereby increasing the chance for a successful clinical outcome.1 tumors are increasingly being classified into subsets based on molecular profile with corresponding tailored treatment . 
there are substantial data demonstrating metastatic tissue can harbor unique genomic alterations compared with the primary tumor , and heterogeneity can also be seen among different metastatic sites in the same patient.2 , 3 it is generally accepted that the use of genomics and biomarkers substantially increases the success rate of clinical trials while lowering their cost.4 despite the rapid emergence of liquid biopsies ( eg , circulating tumor dna , 5 exosomes , circulating tumor cells ) , image - guided , minimally invasive biopsies remain the gold standard in procuring sufficient malignant tissue for molecular analysis . there are several reasons for sampling increasing amounts of tissue more frequently : the realization that tumors can adapt rapidly to therapeutic pressures and that molecular analysis of progression site biopsy , rather than primary specimen , is crucial to identify mechanisms of resistance ; the nathan e . 
 increasing use of immunotherapy trials where treatment response assessment can be difficult by imaging ( eg , pseudoprogression ) ; the emergence of more sophisticated analytic models , including patient - derived tumor cell lines and xenografts , requiring additional tissue ; the fact that a single biopsy core ( 10 mm3 ) maximally contains 30 million cells but often much fewer because of stroma and other factors ; and as a precautionary method to ensure that genomic analysis is indeed possible , because results can help with potential selection of matched targeted therapy . 
for example , in a large recent federal trial of personalized cancer medicine , 13% of tumor biopsy samples could not be used for genomic analysis.6 a recent trend in image - guided biopsies has therefore been to collect more cores ( four to 10 cores ) than necessary for traditional pathology workup ( eg , one to two cores )  . additional cores can be harvested with the use of coaxial systems that allow repeat 18 - gauge samples to be obtained through a hollow needle placed under image guidance . 
with such an approach , consecutive tissue fragments can then be used for immunohistochemistry , fluorescence in situ hybridization analysis , genomic analysis , protein and phosphoprotein biomarker testing , and establishment of patient - derived models , including cell lines , organoids , and mouse xenografts.7 these multicore biopsies , which we herein term highcontent biopsies ( hcbx ) , are thus attractive in initiating and evaluating genotype - centric drug trials and may be critically important for comprehensive genomic and proteomic analyses . 
with increased core sampling , a critical question remains : is there an increased complication rate associated with more extensive tissue harvesting ? data on the safety of research biopsies are limited , 8 , 9 in part because such data are typically not reported in clinical trials , and there is no standard consensus for the reporting of adverse events.10 the technical success rates of obtaining adequate cores after repeat sampling are largely unpublished , although anecdotal reports describe potential reduction in sample quality after repeat sampling.11 furthermore , performing biopsies within research protocols requires more complex logistics , with dedicated personnel and workflows . the main goal of this study was to evaluate if the increased number of cores obtained for research biopsies was associated with increased complication rates or decreased sample quality . 
to address these questions , we performed a retrospective analysis of focal tumor biopsies in the liver performed in the setting of specific oncologic research protocols at a single institution over a 4 - year period . 
practice patterns and complication rates were compared with those of 1 , 522 consecutive biopsies performed in 1 , 154 patients for standard clinical management during the same time period . 
of these , 199 biopsies were performed in 143 patients in the setting of oncologic research protocols ( research biopsy group ) ; 1 , 522 were performed in 1 , 154 patients for standard clinical management ( standard biopsy group )  . in the standard biopsy group , patients were referred from their oncologists directly to the interventional oncology service . 
these cores were placed in formalin and sent to pathology for standard processing : hematoxylin and eosin staining , immunohistochemistry as needed , and , more recently , molecular testing ( snapshot or foundation medicine [ fm ] , as discussed in pathology analysis ) when requested by referring oncologists . for research biopsies , however , a dedicated staff research coordinator was responsible for coordinating the entire process : arranging for the biopsy scheduling , determining and discussing the number of cores needed with the interventional radiologist , and collecting the samples and distributing them to their appropriate destinations . 
this was performed according to a standard operating procedure ( sop ) associated with each research study in which these patients were enrolled and was prospectively logged in an institutional database . 
for research biopsies , a dedicated staff member ( biopsy coordinator ) is responsible for coordinating the entire process : arranging for the scheduling , discussing the number of cores , and collecting the samples and distributing them to their appropriate destinations . the most common workflow involves obtaining five cores : in formalin for pathology , including mutational analyses ; fixed in formalin for 6 to 24 hours and subsequently transferred to ethanol , to be sent to trial sponsor ; in fetal bovine serum ( fbs ) , for development of patientderived models and drug testing ; in formalin for intrainstitutional research laboratories ; and snap frozen for tissue bank . prior imaging coaxial biopsy research / clinical trial biopsy > 5 cores formalin formalin formalin snap frozen patient 1 - 2 cores analysis of : size location growth approach routine pathology tissue type ihc mutations analysis of : tissue type pathway analysis mutations drug response oncologist interventional radiologist biopsy coordinator the fourth in formalin for intra - institutional research laboratories ; and the fifth , which was snap frozen ( fig 1 )  . 
patients in the research group were consented for additional risk of bleeding and other complications . image - guided biopsy procedures all procedures were performed using 18 - gauge coaxial , semiautomatic needle biopsy cutting needles ( bard mission ; bard biopsy systems , tempe , az ) under imaging guidance . 
50 , 000 / ml and an international normalized ratio of prothrombin time , 1.5 for all patients undergoing liver biopsy . in the research biopsies , 54.3% of the procedures were performed using ultrasound guidance ( supersonic imagine , aix - en - provence , france ; hitachi aloka medical , tokyo , japan ) , and 45.7% were performed using computed tomography guidance ( general electrics , fairfield , ct )  . 
a total of 193 procedures were performed using moderate sedation ( intravenous use of fentanyl and midazolam ) , three biopsies were performed with general anesthesia or monitored anesthesia care , and three procedures were performed with local anesthetic only ( lidocaine )  . complication rates were determined by review of medical notes and imaging studies obtained up to 30 days after the procedure ( research biopsies ) and of a prospectively maintained departmental database ( research and standard biopsies ; hi - iq ; conexsys , lincoln , ri )  . 
complications were classified as major ( including all patients who required more therapy other than clinical support , required hospitalization , or experienced an unplanned increase in the level of care , permanent adverse sequelae , or death ) or minor ( others ) .13 we did not record intraprocedural pain scores , because a majority of patients received conscious sedation in a patient - focused manner and by different care providers . 
all patient cases with negative results were reviewed , and clinical and imaging follow - up was used to determine whether they were true or false negatives . pathology analysis a negative biopsy was defined as 0% tumor cells . when rare tumor cells were present , they were noted , and the diagnosis was positive for malignancy . 
this was performed in house with polymerase chain reaction ( pcr ) based assay ( pcr - snapshot14 ) or targeted nextgeneration sequencing ( ngs ) tumor genotyping assay ( ngs - snapshot ) .15 selected samples were sent to fm for a different comprehensive genomic profiling using ngs.16 statistical analysis descriptive statistics were used to summarize results . 
table 1 summarizes patient demographics . because of heterogeneity among the clinical trial protocols , the mean number of cores obtained in the research cohort varied ( fig 3a )  . 
for a majority of procedures ( n = 186 of 199 ; hcbx ) , a larger number of cores ( range , four to 10 ; mean , 5.7 cores ) was obtained . 
in a smaller characteristic age , years mean range male female cancer type breast lung colorectal other primary stage * complication minor major 57.9 28 - 84 60 ( 30.2 ) 139 ( 69.8 ) 68 ( 34.2 ) 55 ( 27.6 ) 26 ( 13.1 ) 50 ( 25.1 ) 1 ( 0.5 ) 5 ( 2.5 ) 3 ( 1.5 ) 190 ( 95.5 ) 2 ( 1.0 ) 1 ( 0.5 ) * patient cases of stage i to iii disease correspond to cases of intrahepatic cholangiocarcinoma or hepatocellular carcinoma ; patient cases of stage iv disease represent all other neoplasms . number of procedures ( n = 13 of 199 ) , fewer cores ( range , two to three ; mean , 2.8 cores ) were sufficient to satisfy trial requirements and / or research needs . sample processing and analysis the 1 , 100 cores were distributed to their appropriate destination by the research biopsy coordinator according to the sop of each study ( fig 3b ) ; 229 cores ( from 127 procedures ) were sent to trial sponsors , 121 cores ( from 110 procedures ) were sent for development of patient - derived cell lines , 466 cores ( from 192 procedures ) were sent to other in - house research laboratories for various studies , and 284 cores ( from 174 procedures ) were sent to standard pathology . 
among the procedures from which samples were sent to standard pathology ( n = 174 ) , molecular analysis was attempted on 73 : multiplex pcr - based snapshot in 13 , ngs - based snapshot in 39 , and foundationone in 19 ; two samples had insufficient tissue for molecular analysis . the success rates of different analyses for research biopsies are summarized in figure 3c . 
 ( a ) distribution of number of cores per biopsy ( median , five ; mean , 5.5 6 standard deviation , 1.5 ; range , two to 10 cores )  . 
of these , four were shown to be true negatives ( ie , no evidence of metastasis or persistent local response after treatment on followup ) and were excluded from the analyses of success for the different tests . 
of the evaluated parameters ( table 2 ) , none were clearly associated with either satisfactory or nondiagnostic samples . the complication rates in the standard biopsy cohort were similar , with major complications observed in 1.4% of procedures ( 22 of 1 , 522 )  . the major complications were hematomas requiring transfusion or intervention ( n = 15 ) , pneumothorax requiring chest tube ( n = 1 ) , hemobilia requiring endoscopic retrograde cholangiopancreatogram ( n = 1 ) , infection requiring admittance ( n = 1 ) and / or percutaneous drainage ( n = 1 ) , and death ( n = 3 ; all secondary to bleeding )  . 
the minor complication rate was 1.0% ( n = 2 ; both were hematomas managed conservatively : one patient with metastatic breast cancer [ seven cores ] and one with colorectal cancer [ five cores ] )  . image - guided biopsies have long played an important role in the management of cancer . 
these findings are not entirely unexpected , because we used a coaxial biopsy technique that allows for multiple cores to be harvested through a single coaxial needle , therefore minimizing the number of capsular punctures probably a factor for decreasing the risk of complications in biopsies.24 one evident finding of our study is the progressive increase of research biopsies over the study period . this is consistent with the increasing popularity of molecularly targeted trials , as well as the realization that hcbx are technically feasible and safe . 
it has already been reported that genetic analysis is contingent on sufficient material.6 accordingly , different methods of molecular analysis in our data had results that ranged from 79% ( fm ) to 100% ( pcr - based snapshot )  . although ngs can more efficiently detect a wider range of molecular aberrations , more material is needed compared with older pcrbased techniques . to streamline research biopsies and accommodate larger numbers of procedures , we implemented a specific workflow with dedicated staff for efficient communication among clinicians , researchers , trial sponsors , and interventional radiologists , as well as collection and distribution of samples . 
although we did not measure the exact length of time required for the procedures in this study , we had previously determined that additional core sampling only required a few minutes longer , unless the coaxial needle had to be repositioned because of poor sample material ( eg , necrotic core , cystic tumor , fragmented specimen )  . 
interestingly , in our experience , the order in which cores were harvested was not associated with lower success rates for pathology , contrary to prior published reports.11 the samples sent for cell - line creation had a lower success rate . 
although this may have been related to the sample volume , it may also have resulted from other variables beyond our control ( amount of tumoral cells required for successful cell - line creation , timing , distance , or personnel , among others )  . 
interestingly , however , within the samples that were used for cell - line creation , the number of cores was not associated with cellline creation success rate . our study was designed to answer simple questions : how successful are hcbx , and what is their complication rate ? this is of timely interest ; data on the safety of research biopsies are limited , because they are often not reported in clinical trials.10 as such , our study focused on so - called all comers in a large oncologic interventional care setting rather than on specific subsets of patients , biopsy sites , or operators . 
 3% pi3k - akt signaling pathway fgfr1 / 2 / 3 / 4 and fgf familiy mapk / ras signaling pathway cyclin - dependent kinase related tp53 egfr esr1 other negative fig 4 . 
the genomic abnormalities detected in our study were similar to those found in several large studies17 and reflect the study population involving breast , lung , and colorectal cancer and cholangiocarcinoma trials at our institution . 
mapk , mitogen - activated protein kinase ; pi3k , phosphatidylinositol 3 - kinase . thoracic lesions , and similar studies may be warranted for those cohorts . our study has several limitations . 
medical records were reviewed for complications exclusively in the research biopsy group , although this would , if anything , overestimate the relative risk of complications compared with that of standard biopsies . 
only data on liver biopsies were reviewed , and therefore , additional studies are required to verify if the conclusions apply to other organs frequently biopsied , such as lungs , lymph nodes , and bones . 
vadvala , aditya bardia , jeffrey engelman , peter r . mueller , dejan juric , ralph weissleder financial support : dejan juric , ralph weissleder administrative support : dejan juric , ralph weissleder provision of study material or patients : laura spring , dejan juric collection and assembly of data : nathan e . 
frenk , laura spring , alona muzikansky , mari mino - kenudson , amy ly , aditya bardia , dianne finkelstein , dejan juric , ralph weissleder manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors the field of blood - based biomarkers in oncology for disease monitoring and molecular analysis is rapidly evolving . 
liquid biopsies can be used to detect circulating extracellular vesicles25 or tumor cells within a blood specimen , providing a tool to monitor cancer noninvasively.26 similarly , a number of technologies have also been developed to identify and track tumor - specific mutations via circulating free dna in the blood and urine.5 as these technologies are further developed and validated , they might replace some of the tissue biopsies in certain research and clinical settings . however , tissue biopsies allow for sampling of specific lesions and evaluation of tissue architecture and the tumor microenvironment , including proteins , phosphoproteins , and varied cytokines . image - guided biopsies will therefore continue to remain important for phenotyping tumor responses , identifying tumor heterogeneity , identifying therapeutic resistance , and characterizing host responses in the era of immunotherapy and targeted therapies . 
additional advances in image - guided tumor sampling , including lower computed tomography doses , shorter image acquisition times , and systems for acquiring , processing , and analyzing smaller samples may further expand the use of hcbx . 
mueller consulting or advisory role : cook medical patents , royalties , other intellectual property : royalties from cook ( percutaneous catheters ) dejan juric consulting or advisory role : novartis , emd serono , eisai ralph weissleder consulting or advisory role : moderna therapeutics , alivio therapeutics , tarveda therapeutics , lumicell , t2 biosystems , bioanalytix acknowledgment we thank all members of the division of interventional and abdominal radiology who contributed to the review of cases and / or performing of biopsies , in particular steven dawson , md , ashraf thabet , md , ronald arellano , md , suvranu ganguli , md , avinash kambadakone , md , michael zalis , md , and omar zurkiya , md , phd . 
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im h , shao h , park yi , et al : label - free detection and molecular profiling of exosomes with a nano - plasmonic sensor . nat biotechnol 32 : 490 - 495 , 2014 26 . 
 exceptional response to 177lutetium prostate - specic membrane antigen in prostate cancer harboring dna repair defects megan crumbaker , mbbs1 , 2 , 3 ; louise emmett1 , 3 ; lisa g . 
psma - targeted small molecules bound to 177lutetium ( 177lu ) , a medium - energy b - emitter , have been administered as a targeted therapy for metastatic prostate cancer ; the psma - targeted small molecule binds to psma on the cancer cell surface and is internalized , leading to delivery of a potent but targeted dose of radiation to the cell . 
a small molecule commonly used for this purpose is psma - 617 , a human psma - targeting ligand that can be conjugated to 177lu . 177lupsma - 617 therapy has shown great promise in early - phase trials , with a prostate - specic antigen ( psa ) response rate of 57% in a phase ii prospective study , 1 and randomized trials are currently recruiting internationally . de novo and acquired resistance are common , however , and biomarkers are needed to guide patient selection and rationalize combinatorial approaches . 177lupsma - 617 induces cell death through doublestrand dna breaks.2 mechanisms to repair doublestrand dna breaks are decient or absent in cells with mutations in homologous repair genes such as brca1 or brca2 , and such mutations are increasingly recognized in metastatic castration - resistant prostate cancer ( mcrpc ) .3 , 4 thus , a deciency in homologous repair may render a tumor more sensitive to 177lupsma - 617 and be relevant in crpc . 
postoperative radiotherapy was withheld because of a history of colorectal carcinoma treated with surgical resection followed by adjuvant radiotherapy 25 years prior . soon after his radical prostatectomy , he biochemically relapsed and was treated with intermittent androgen deprivation therapy . 
he eventually developed overt metastatic disease , with a perihilar mass found on a computed tomography ( ct ) scan of the chest , abdomen , and pelvis after 10 years of hormone manipulation . a nuclear medicine bone scan was negative , but an 18f - labeled uorodeoxyglucose positron emission tomography ( pet ) scan showed low - grade uptake in the mass , which was conrmed to be metastatic prostate cancer on biopsy . 
a choline pet was undertaken to assess the extent of his disease and revealed uptake in his left hilar nodes with inltration in the lingula and involvement of right paratracheal nodes . given the extent of disease across both hemithoraces , he commenced enzalutamide . 
his psa continued to increase ( fig 1 ) despite 8 weeks of treatment , and additional radiologic progression with impending bronchial obstruction prompted radiotherapy to his hilar disease . his psa initially decreased after radiotherapy but began to increase soon after . 
he then received two cycles of cabazitaxel , after which a restaging ct scan showed enlargement of his liver metastases and development of new pelvic nodal metastases . having progressed through all standard lines of therapy , this patient was enrolled in a clinical trial of 177lupsma - 617 therapy and received 4 6.5 gigabecquerel doses once every 6 weeks ( anzctr identier : actrn12615000912583 )  . 
plot of prostate - specic antigen ( psa ) values over time . treatment regimens : cabazi , cabazitaxel ; doce , docetaxel ; enz , enzalutamide ; lupsma , 177lutetium prostate - specic membrane antigen ; rt , radiotherapy . time ( months ) the return of his right upper quadrant abdominal pahe was consented for prescreening of his circulating tumor dna ( ctdna ) for a poly adp - ribose polymerase ( parp ) inhibitor trial , but while awaiting this result , his pain increased signicantly , with derangement of his liver function tests and a further increase in his psa . 
he was approved for an additional two compassionate 7.0 - gigabecquerel doses of 177lupsma - 617 ; he received these with clinical and radiologic responses associated with a psa response from 169 to 43 after the rst dose . a resolution bioscience targeted ctdna analysis for dna repair defects revealed abnormalities in three homologous fig 2 . 
to assess his germline , we performed targeted sequencing of coding regions and splice sites of atm , brca1 , brca2 , brip1 , cdh1 , cdkn2a , chek2 , hoxb13 , palb2 , pten , rad51c , rad51d , stk11 , and tp53 on dna extracted from blood ; this conrmed a frameshift mutation in exon 11 of the brca2 gene . 
up - front resistance and early relapses are common , however , signifying the need for strategies to improve patient selection and / or test rational combination approaches . as a form of ionizing radiation , 177lupsma - 617 induces double - strand dna breaks , which are believed to be the main lethal event in most exposed cells . 
preclinical and clinical studies have identied an association between cancers with homologous recombination defects and increased radiation sensitivity.8 germline mutations in genes that encode and mediate key enzymes for dna repair pathways , such as brca2 and atm , occur in approximately 11.8% of men with metastatic prostate cancer and somatic mutations in at least 23% of patients with mcrpc , 3 , 4 rendering many prostate cancers homologous recombination decient . homologous recombination deciency has been associated with responses to parp inhibition and platinum - based chemotherapy , 9 , 10 but these treatments may cause signicant toxicity . this patients germline mutation likely predisposed him to more aggressive disease , 11 and he was resistant to not only enzalutamide but also two lines of taxane - based chemotherapy . 
after his 177lupsma - 617 treatment , he also responded to carboplatin chemotherapy and a parp inhibitor . is biologically plausible that this gentlemans aberrations in homologous repair pathways enhanced his susceptibility to the radiation effects of 177lupsma - 617 therapy . 
we hypothesize that patients with mutations in dna repair pathway genes would be especially responsive to peptide receptor radionuclide therapy because of their inability to overcome dna breaks induced by the treatment . 
hofman ms , sandhu s , eu p , et al : 785olutetium - 177 psma ( lupsma ) theranostics phase ii trial : efcacy , safety and qol in patients with castrate - resistant prostate cancer treated with lupsma . 
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eur urol 73 : 656 - 661 , 2018 emmett l , willowson k , violet j , et al : lutetium 177 psma radionuclide therapy for men with prostate cancer : a review of the current literature and discussion of practical aspects of therapy . 
pomerantz mm , spis ak s , jia l , et al : the association between germline brca2 variants and sensitivity to platinum - based chemotherapy among men with 11 . 
castro e , goh c , olmos d , et al : germline brca mutations are associated with higher risk of nodal involvement , distant metastasis , and poor survival outcomes metastatic prostate cancer . 
 circulating tumor dna analysis in colorectal cancer : from dream to reality carlotta antoniotti , md1 , 2 ; filippo pietrantonio , md3 , 4 ; salvatore corallo , md3 ; filippo de braud , md3 , 4 ; alfredo falcone , md1 , 2 ; and chiara cremolini , md , phd1 , 2 liquid biopsy is a minimally invasive approach to obtain circulating materials that originate from tumor cells through the sampling of body uids , mainly peripheral blood . 
because of its abilities to detect tumor - derived nucleic acids and proteins and to characterize tumor - specic genomic abnormalities , liquid biopsy has emerged as an approach to orient care of patients with colorectal cancer ( crc )  . 
second , the reliability of studies that evaluate the concordance of ras testing between tissue and plasma samples is impaired by the adoption of assays with heterogeneous analytical sensitivity and coverage of genomic regions . 
there are now several commercially available methods for ctdna assessment and technology platforms based on digital polymerase chain reaction or next - generation sequencing approacheseach one with specic sensitivity , specicity , throughput , gene coverage , costs , and potential clinical applications.12 among them , three test kits are ce - marked in vitro diagnostic devices for detection of ras and braf mutations on ctdna in crc.13 - 16 third , some clinicopathologic variables are likely to affect the amount of tumor - released ctdna.5 , 6 , 8 , 10 , 11 whereas liver involvement and tumor burden are positively associated with the ras mutant allele fraction ( the proportion of mutant dna fragments at a given locus ) , peritoneal , nodal , and lung metastases and mucinous histology are linked to low ras inuence ctdna ctdna detection . 
 antoniotti et al ras wild - type cases , as assessed on ctdna , negligible . is not the parallel assessment of the mutant allele fractions of other key genomic tumor alterations may help solve challenging cases that have undetectable ras mutations and ctdna levels at or lower than the analytic sensitivity of adopted assays . 
to overcome these issues , preanalytic procedures should be standardized , a threshold of detectable mutation rate that confers intrinsic resistance to egfr inhibition should be set and prospectively validated , investigation to understand when plasma and additional and tissue tests are interchangeable and to improve assay sensitivities is warranted . meanwhile , the ras status assessment to address the use of anti - egfr agents must be performed as the gold standard on tumor specimens.3 , 4 , 17 , 18 only when tissuebased testing is technically or logistically unfeasible could it be replaced by ctdna analysis.4 ctdna to estimate prognosis and detect minimal residual disease retrospective studies have focused on the prognostic impact of the quantitative analysis of ctdna . 
in the metastatic setting , a correlation between ctdna concentration and survival has been described , but the independent weight of ctdna quantication when the relative impact of other well - known prognostic factors is taken into account has not been claried ( appendix table a2 )  . the role of the quantitative assessment of ctdna in monitoring response during treatment must be dened in the light of its potential added value when compared with easily available and well - established markers , including carcinoembryonic antigen or early radiologic disease reassessment . 
recently , ctdna has been proposed to detect , measure , and monitor residual disease after radical interventions . a series of proof - of - concept studies reported that liquid biopsy could disclose the persistence of minimal residual disease ( mrd ) through the detection of ctdna in patients with crc who underwent potentially curative surgery ( resection of primary tumor in early - stage crc or radical resection of metastases ) even in the absence of clinical or radiologic signs of residual disease ( appendix table a2 )  . by identifying incomplete eradication of disease after a curative treatment , detectable ctdna predicts an increased risk of relapse regardless of the exposure to an adjuvant treatment . 
the development of such a sensitive tool might improve the risk estimation of disease relapse after a curative intervention to properly stratify clinical trials in early - stage crc and to accordingly drive the therapeutic management . theoretically , two applications of the detection of mrd in this setting may be foreseen : to offer chemotherapy to all postoperative ctdna - positive patients , including those with no histopathologic risk factors to reduce their risk of progressionindeed , ctdna positivity invariably means residual diseaseand to avoid useless adjuvant therapies in postoperative ctdna - negative patients . 
in early - stage crc , ctdna is detected at a lower rate than in the advanced disease.1 therefore , highly sensitive techniques are needed to achieve appropriate accuracy to detect mrd . most available data have been achieved through a twothe identication of specic somatic step procedure : abnormalities in tissue samples , followed by the search for the same alteration in ctdna . 
only trials that aim to optimize the treatment of all postoperative ctdna - positive patients , independent of traditional histopathologic factors , are ethically acceptable . ctdna to track tumor response and resistance to therapy whereas tissue biopsies catch single snapshots of the tumor in a specic spatiotemporal fragment , liquid biopsy may more comprehensively depict the intrinsic and dynamic intratumoral heterogeneity . 
the heterogeneity and dynamism of the tumor clonal evolution under the pressure of targeted treatments are conrmed by the emergence of multiple alterations in the mitogenactivated protein kinase pathway effectors , including ras and mek mutations and kras , brafv600e , and met amplication , during the treatment with braf / egfr , braf / mek and braf / egfr / mek inhibitors in patients with brafv600e - mutant mcrc.23 - 27 two novel ntrk1 mutations have been detected as a potential mechanism of acquired resistance to entrectinib , a tyrosine kinase receptor inhibitor , in a patient with lmna - ntrk1rearranged mcrc.34 nevertheless , some steps should be covered to translate liquid biopsy from the investigational setting into clinical practice . available data indicate that the frequency of molecular alterations in ctdna at the time of disease progression is inconsistent among different series , even when the same methods for plasma ctdna analysis is applied ( table 1 )  . this inconsistency impairs the reliability of adopted techniques and the reproducibility of the ndings . 
setting and validation of a quantitative threshold to dene the clinical relevance of each detectable molecular alteration as clearly associated with a lack of benet from ongoing therapies may be relevant to biologically guide therapeutic decisions . currently , no prospective data are available about usefulness of discontinuing ongoing therapy and initiation of a tailored treatment when signals of acquired resistance emerge in ctdna before clinical or imaging - based disease progression is noted . the co - occurrence of multiple and / or subclonal molecular alterations at the time of acquired resistance highlights an increase in tumor heterogeneity , which complicates the denition of clinical value of each identied alteration as therapeutic target for subsequent tailored strategies . 
in other words , how to therapeutically target the heterogeneous mechanisms of resistance and the subclonal patterns of tumor cell populations that emerge upon drug selection is today still challenging . 
in this proof - ofconcept study , patients who are candidates for anti - egfr rechallenge are eligible only if a notable decrease in ras fractional mutational abundance occurs from the time of disease progression after a rst - line anti - egfrcontaining therapy to the time of rechallenge . liquid biopsy has emerged as a minimally invasive tool to genotype tumors , to assess patient prognosis and detect mrd , to monitor treatment efcacy , and to track the dynamism of clonal evolution over time and therapies . 
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tsuji y , shitara k , yamanaka t , et al : reverce : randomized phase ii study of regorafenib followed by cetuximab versus the reverse sequence for metastatic colorectal cancer patients previously treated with uoropyrimidine , oxaliplatin , and irinotecanbiomarker analysis . 
montagut c , argil es g , ciardiello f , et al : efcacy of sym004 in patients with metastatic colorectal cancer with acquired resistance to anti - egfr therapy and molecularly selected by circulating tumor dna analyses : a phase 2 randomized clinical trial . 
santini d , vincenzi b , addeo r , et al : cetuximab rechallenge in metastatic colorectal cancer patients : how to come away from acquired resistance ? ann oncol 23 : 4602 - 4616 , 2017 23 : 2313 - 2318 , 2012 49 . 
parseghian cm , loree jm , morris vk , et al : anti - egfr resistant clones decay exponentially after progression : implications for anti - egfr re - challenge . 
cremolini c , rossini d , dellaquila e , et al : rechallenge for patients with ras and braf wild - type metastatic colorectal cancer with acquired resistance to rstline cetuximab and irinotecan : a phase 2 single - arm clinical trial . 
 aggressive - variant microsatellitestable pole mutant prostate cancer with high mutation burden and durable response to immune checkpoint inhibitor therapy the increasing application of next - generation tumor dna sequencing may define molecular subsets of prostate cancer for which precision medicine approaches are enabled . 
transrectal ultrasound guided needle biopsy demonstrated gleason 4 + 5 = 9 ( grade group 5 ) adenocarcinoma in 12 of 12 cores involving 95% to 100% of each core with perineural invasion . 
tumor cells stained positive for psa and negative for chromogranin and synaptophys radiologic staging studies indicated bilateral external iliac , common iliac , and retroperitoneal adenopathy without definitive evidence of bone metastases . 
with persistent bulky disease in the prostate on digital rectal examination at 12 weeks from the start of hormonal therapy , a repeat biopsy was performed , which demonstrated gleason 4 + 5 = 9 adenocarcinoma with focal synaptophysin expression . 
restaging studies showed only modest regression in pelvic adenopathy discordant with the brisk decline in psa , with tumor infiltrating the bladder base and seminal vesicles , and abutting the rectum with a preserved fat plane on magnetic resonance imaging . 
pathologic examination indicated a high - grade tumor with morphologic and immunohistochemical evidence of neuroendocrine differentiation ( synaptophysin and chromogranin expression ) with lymphocytic infiltration ( fig 1 ; appendix fig a1 )  . 
seminal vesicle involvement was absent , but there was extensive extraprostatic extension and multiple positive surgical margins including the bladder neck , and one of eight lymph nodes were involved.the patient did well in the postoperative period , with early recovery of continence ; however , restaging studies showed progressive retroperitoneal and pelvic adenopathy . 
repeat radiologic imaging after an interval on observation again demonstrated progressive pelvic adenopathy ( fig 2a )  . methodology genomic sequencing studies on the primary tumor were performed with the foundationone assay1 ( foundation medicine , cambridge , ma ) , and the tumor mutation burden was estimated as previously described.2 mutations of the androgen receptor , pten , tp53 , and atm , which have been previously implicated in the genomic landscape of prostate cancer , 3 , 4 were identified , along with a pole v511l mutation ( appendix table a1 )  . 
using all nondriver and nongermline missense mutations , we found that 77% of the alterations in the sample were attributable to the pole signature , making this the dominant signature over other lesions identified in the sample that have been implicated in dna repair , including tp53 , atm , or pten ( appendix table a1 )  . 
germline screens for inherited mutations included a screen for brca1 and brca2 ( ambry genetics , aliso viejo , ca ) and a breast - ovarian panel ( genedx , gaithersburg , md )  . 
infiltrating cd4 + and cd8 + lymphocytes were observed in a three to one ratio.the patients family history raised concerns of an autosomal - dominant inherited risk of prostate and breast cancer . 
his father had been diagnosed with high - grade prostate cancer at 76 years of age , and his two brothers had screen - detected low - risk prostate cancer at 54 and 48 years of age , respectively . 
one sister had died of triple - negative metastatic breast cancer at 45 years of age , and another was diagnosed with ductal carcinoma in situ at 55 years of age . 
 was identified in the father in brip1 ( c2392c > t [ p . arg798ter ] ) , along with a brip1 variant of uncertain significance ( c.3710c > a [ p.ser1237tyr ] ) ; the latter alone was found in the patient and two living siblings ( appendix fig a2 )  . 
given the early castration - resistant and chemotherapy - resistant progression of the patients disease and the high tumor mutation burden identified , he was started on immune checkpoint inhibitor blockade with pembrolizumab therapy 200 mg every 3 weeks intravenously . 
sixteen months later , he has remained without evidence of disease progression after 24 cycles of therapy , with residual subcentimeter pelvic nodes , a normal testosterone level without hormonal therapy , and an eastern cooperative oncology group performance score of zero . discussion to our knowledge , this first report in prostate cancer indicates the presence of a mutation in the highly conserved exonuclease domain of dna polymerase ( pole ) 7 in an aggressive - variant metastatic prostate cancer8 that presented with a bulky primary tumor , early castration , and chemotherapy resistance but with an excellent and durable subsequent response to immune checkpoint blockade . 
pole mutant cancers constitute a unique genomic subset of cancers described previously in colorectal and endometrial cancers.9 the somatic v411l mutation of pole has been associated with impaired dna proofreading repair and the generation of ultramutated tumor phenotypes that are microsatellite stable.9 , 10 mutations that could contribute to castration resistance ( androgen receptor , pten ) or dna damage repair insufficiency ( atm , tp53 ) were also identified , consistent with the known genomic landscape of prostate cancer.3 however , two methods of analyzing genomic signatures were used that implicate the pole lesion as the dominant source of the hypermutated phenotype in this case . 
 hypermutated phenotypes in prostate cancer are uncommon and were first identified in 12% of tumors ( 7 of 60 ) sourced from patient - derived xenografts and a rapid autopsy series.11 in this study set , hypermutated tumors , defined as > 300 somatic protein - altering mutations , were universally associated with micro satellite instability largely secondary to msh2 and msh6 structural rearrangements and not mlh1 epigenetic silencing , as is more commonly seen in colorectal and endometrial cancers with dna mismatch repair deficiency . 
 our case report suggests that microsatellite stable pole mutant prostate cancer represents a distinct , albeit exceedingly rare , genomic subset of highmutation - burden prostate cancers with demonstrable potential for high - quality and durable response to immune checkpoint blockade , similar to that reported in endometrial and colorectal pole mutant cancers.12 , 13although responses to immune checkpoint inhibitors in castration resistant prostate cancer have been uncommon to date , 14 - 16 in one study , three of 10 enzalutamide resistant tumors responded to pembrolizumab therapy.17 one evaluable tumor was found to be microsatellite unstable , and a second was microsatellite stable . 
to our knowledge , other that this case report , there are no data that link the control of prostate cancer with immune checkpoint inhibitors to genomically defined highmutation - burden subsets of prostate cancers , whether microsatellite stable or unstable . 
more studies will be required to establish whether high - quality and durable responses to immune checkpoint inhibitors as single agents will be confined to prostate tumors with high mutation burdens . 
hotspot germline genomic sequencing using commercially available assays via clinical genetics consultation did not identify a pathogenic lesion in the patient and two of the living siblings with cancer diagnoses , but his father was identified with a pathogenic brip1 variant along with the brip1 variant of uncertain significance found in his children . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . lisa lee no relationship to disclose elizabeth genega no relationship to disclose dallas reed no relationship to disclose ethan sokol no relationship to disclose paul mathew honoraria : exelixis patents , royalties , other intellectual property : patent pending on new therapeutic invention travel , accommodations , expenses : exelixis affiliations lisa lee , elizabeth genega , dallas reed , and paul mathew , tufts medical center , boston ; siraj ali and ethan sokol , foundation medicine , cambridge , references 1 . 
graff jn , puri s , bifulco cb , et al : sustained complete response to ctla - 4 blockade in a patient with metastatic , castration - resistant prostate cancer . 
kwon ed , drake cg , scher hi , et al : ipilimumab versus placebo after radiotherapy in patients with metastatic castration - resistant prostate cancer that had progressed after docetaxel chemotherapy ( ca184 - 043 ) : a multicentre , randomised , double - blind , phase 3 trial . 
kote - jarai z , jugurnauth s , mulholland s , et al : a recurrent truncating germline mutation in the brip1 / fancj gene and susceptibility to prostate cancer . 
 legend prostate cancer squamous cell carcinoma colorectal cancer thyroid cancer melanoma basal cell cancer breast cancer 61 years brip1 c.3710c > a ( p.ser1237tyr ) ; likely benign variant prostate cancer , 59 years gleason 9 60 years breast cancer ( unilateral ) , 54 years brip1 c.3710c > a , p.ser1237tyr ; likely benign variant 53 years prostate cancer , 52 years melanoma 49 years prostate cancer , 48 years basal cell cancer d . 
87 years colorectal cancer , 87 years 85 years brip1 c.2392c > t ( p.arg798ter ) ; pathogenic prostate cancer , 79 years squamous cell carcinoma 83 years thyroid cancer , 40s fig a2 . 
steensma , md6 ; amy dezern , md7 ; gail roboz , md8 ; guillermo garcia - manero , md9 ; harry erba , md , phd10 ; benjamin l . 
maciejewski , md , phd1 purpose we developed an unbiased framework to study the association of several mutations in predicting resistance to hypomethylating agents ( hmas ) in patients with myelodysplastic syndromes ( mds ) , analogous to consumer and commercial recommender systems in which customers who bought products a and b are likely to buy c : patients who have a mutation in gene a and gene b are likely to respond or not respond to hmas . methods we screened a cohort of 433 patients with mds who received hmas for the presence of common myeloid mutations in 29 genes that were obtained before the patients started therapy . 
the association between mutations and response was evaluated by the apriori market basket analysis algorithrules with the highest condence ( condence that the association exists ) and the highest lift ( strength of the association ) were chosen . we validated our biomarkers in samples from patients enrolled in the s1117 trial . results among 433 patients , 193 ( 45% ) received azacitidine , 176 ( 40% ) received decitabine , and 64 ( 15% ) received hma alone or in combination . 
the median number of mutations per sample was three ( range , zero to nine ) , and 176 patients ( 41% ) had three or more mutations per sample . 
these molecular signatures were present in 30% of patients with three or more mutations / sample with an accuracy rate of 87% in the training cohort and 93% in the validation cohort . conclusion genomic biomarkers can identify , with high accuracy , approximately one third of patients with mds who will not respond to hmas . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the hypomethylating agents azacitidine ( aza ) and decitabine ( dac ) have been approved by the food and drug administration and the european medicine agency for patients with myelodysplastic syndromes ( mds ) .1 - 4 although treatment with these agents is well tolerated , only 30% to 40% of patients will respond to therapy , with the majority achieving hematologic improvement in blood counts and only a minority ( 10% to 15% ) achieving a complete response , the response criterion most reliably associated with improvement in overall survival ( os ) .1 - 4 more importantly , it may take up to six cycles of treatment for patients to achieve their best response.5 given the limited number of patients who benet from these agents and the long administration of identifying biotheir treatment , markers that can predict resistance is essential , because it can prevent prolonged exposure to ineffective therapy and unnecessary toxicities and treatment costs can be avoided . because clinical variables and patient characteristics have not consistently predicted response to hypomethylating agents ( hmas ) , molecular data represent a biologic opportunity6 - 8 to enhance patient response rates and outcomes . 
because identifying a single gene or comutated genes is unlikely to yield an understanding of how these mutations dene disease biology or phenotype , an unbiased approach is needed to study the relationship of these abnormalities to each other and to mds biology . in this study , we used unbiased , machine learning approaches ( a recommender system similar to that used by netix or amazon.com ) to assess the impact of molecular data on resistance to hmas in a large cohort of patients treated with hmas at different academic institutions , and we validated our results in a population treated in a contemporary prospective clinical trial of hma therapy15 of aza alone and in combination . methods patients for the training cohort , patients treated with either azaor dac - based regimens were included in this study : 230 patients were treated at cleveland clinic ( between 2002 and 2012 ) ; 203 were from other academic institutions ( dana - farber cancer institute [ 2003 to 2010 , n = 42 ] and md anderson cancer center [ 2003 to 2010 , n = 103 ] ) or were part of the daco - 020 clinical trial ( adopt [ 2005 to 2006 , n = 58 ] ) .11 all patients consented to blood or bone marrow samples at each institution under institutional review boardapproved protocols in accordance with each institution policy and the declaration of helsinki . 
more information regarding the patient cohort , response criteria , and validation cohort is included in the data supplement . dna sequencing and mutational analysis a panel of 29 genes that are commonly mutated in mds and myeloid malignancies was evaluated ( data supplement )  . 
more information regarding sequencing method is included in the data supplement . statistical analyses test variables were compared using the wilcoxon rank sum test and fishers exact for continuous and categorical variables , respectively . 
os was calculated from the date of diagnosis to the date of last follow - up or death ( whichever came rst ) , and survival curves were constructed using the kaplan - meier method and compared using the log - rank test . 
mutation distribution among responders versus nonresponders total responders non - responders nazha et al mutations asxl1 tet2 srsf2 runx1 dnmt3a sf3b1 tp53 u2af1 bcor ezh2 nras idh2 phf6 npm1 jak2 zrsr2 etv6 prpf8 idh1 prpn11 suz12 kras gata2 cebpa received dac ( 176 [ 86% ] alone and 29 [ 14% ] in combination with other agents )  . 
cytogenetic analyses per international prognostic scoring system ( ipss ) revised ( r ) criteria16 included 234 patients ( 54% ) with very good or good risk , 66 ( 15% ) with intermediate risk , 33 ( 8% ) with poor risk , 66 ( 15% ) with very poor risk , and 34 ( 8% ) not documented ( table 1 )  . 
the frequency of these mutations in our patient cohort was similar to those identied in other mds cohorts , with the exception of asxl1 , which was slightly higher because it was overrepresented in one cohort11 ( 203 patients from other academic institutions )  . 
patterns of mutation association were also similar to those in previous reports ( fig 1 )  . asxl1 mutations were commonly commutated with tet2 in 42 patients ( 10% ) , and with srsf2 38 ( 9% ) , runx1 35 ( 8% ) , u2af1 24 ( 6% ) , and dnmt3a 21 ( 5% ; fig 1 )  . overall , 367 patients ( 85% ) in the training cohort had a mutation in at least one gene . 
the graph is separated to show the spectrum of mutations in responders compared with nonresponders . ( 4% ) partial remission ( pr ) , 59 ( 14% ) hematologic improvement ( hi ) , 142 ( 33% ) stable disease , and 107 ( 24% ) progressive disease . in general , clinical characteristics such as age , cytopenias , and treatment regimens did not affect response , with the exception of the median blast percentage in the bone marrow , which was higher among responders compared with nonresponders ( 9% v 2% , p = .02 ; table 1 )  . 
risk stratications per ipss and ipss - r did not affect the overall response rate ( table 1 )  . idh1 and ezh2 , no single gene mutation was signicantly associated with response and resistance to hmas in univariate analyses , with the exception of respectively ( table 2 )  . 
the number of mutations per sample also did not affect response , with patients with three or more mutations having similar response rates to those with fewer than three mutations ( table 1 )  . 
genomic biomarkers dened by the recommender system association rules for resistance to hmas asxl1 , nf1 asxl1 , ezh2 , tet2 asxl1 , ezh2 , runx1 ezh2 , srsf2 , tet2 asxl1 , ezh2 , srsf2 asxl1 , runx1 , srsf2 asxl1 , tet2 , srsf2 asxl1 , bcor , runx1 the impact of mutations on response was assessed after controlling for clinical variables such as age and ipss - r scoring system , using logistic regression analyses . 
no mutation was associated with overall resistance or response to hmas , even after adjustment for clinical variables ( age , ipss - r , and sex ; data supplement )  . recommender system genomic biomarkers that predict response to build strong association rules ( associations between genes and outcomes [ response v no response ] ) , we used strict criteria to identify rules with the highest support ( how many times the rules appeared in the data set ) , high condence ( the condence of the algorithm in the association rule was set at 95% ) , and higher lift ( a measure that is reected in the strength of the association : the higher the lift is , the stronger is the association ) in the training cohort . 
when the rules were applied to our patient cohort , they predicted resistance to hmas correctly in 46 of 53 patients ( 87% ) with relevant molecular mutations . among the 105 patients with lower - risk disease by ipss - r ( low and very low risk groups ) , 62 ( 59% ) did respond to hmas . 
the difference in the presence of the biomarkers in lowerversus higher - risk mds is related to the higher percentage of patients with three or more mutations / sample in the higher - risk ( 42% ) versus the lower - risk ( 30% ) group . association with overall survival survival data were available for 375 patients from the training cohort . 
genomic biomarkers of resistance to aza were present in 14 of 39 samples ( 35% ) with three or more mutations ; 13 of 14 of these patients ( 93% ) did not respond to therapy . discussion predicting response or resistance to our currently available standard hma therapy in mds remains a signicant clinical challenge . 
identifying patients up front who may not respond to hmas can potentially improve outcome , decrease unnecessary adverse effects , and save money , especially when current recommendations are for a minimum of 6 months of treatment before deeming it a failure . 
although it is tempting to identify an isolated molecular abnormality or a pair of mutations that can predict hma resistance , this approach does not allow for the complexity and evolution of the genomic landscape in mds . in this study , we developed an unbiased framework using a machine learning , recommender system algorithm to identify highly sensitive genomic associations ( molecular signatures or genomic biomarkers ) that can predict resistance to hmas with high accuracy . 
these associations were validated in an independent cohort in samples from patients enrolled in a randomized phase ii / iii clinical trial . although our biomarkers were identied in only 25% of patients , their presence predicted resistance in almost all patients who had these mutations . 
by denition , a biomarker can be present in a small subset of patients , but when present can predict , with high accuracy and reliability , response or resistance to a therapy . 
detecting these biomarkers in 29% of patients suggests that other biologic mechanisms ( eg , changes in gene expression or epigenetic changes ) or clinical characteristics may contribute more to hma response and failure than does genomics . 
our ndings conrm that genomic associations may lead to different gene expressions and / or epigenetic changes that contribute to the response or resistance and thus , identifying one or two genes that can predict response may not be sufcient to build reliable and predictable models . although we included patients who received hmas in combination with other investigational agents , these combinations did not affect the response or resistance rate or os ; thus , their impact on the output of our recommender system algorithms is negligible . 
furthermore , neither ipss nor ipss - r predicted response or resistance to hmas in our study in accordance with prior reports.1 , 15 prior studies have attempted to use genomic data to predict response or resistance to hmas . 
for example , some studies have shown that tp53 mutations may predict response to hmas , whereas others did not conrm that nding.13 , 17 in a small study of 84 patients with acute myeloid leukemia ( aml ) and mds treated with a 10 - day dac course , a small subset of patients with tp53 mutations had a higher response rate to dac compared with tp53 wild - type patients . furthermore , the median os for tp53 mutated patients who received dac and underwent an allogeneic stem - cell transplantation was similar to that of patients with wild - type tp5317 . 
contrary to this nding , in a study of 71 patients with aml , there was no difference in overall response rate and survival among patients who received 5 days of dac compared with those who had a 10 - day schedule . 
 genomic biomarkers for resistance in mds with variant allele frequency greater than 10% may predict response to hmas , especially in patients with wild - type asxl1 mutations , but this nding was not validated in our study.11 the discrepancy in the results of these studies could be related to sample size , the number of genes tested , and the statistical approach that was used to analyze the data . 
it is also possible that genomic changes in themselves are not the drivers of response to hmas but rather , changes in the gene expression and methylation prole that are derived from the combination of these mutations . 
in a study of whole - genome sequencing , rna sequencing , and methylation prole of samples from patients with chronic myelomonocytic leukemia , a serial sequencing demonstrates that the response to hypomethylating agents is associated with changes in dna methylation and gene expression , without any decrease in the mutation allele burden or prevention of new genetic alteration occurrence.18 if eligible , directly , without this study includes several areas of innovation . 
for example , if a patient with mds with higher - risk disease carries one of these biomarkers , he or she should be encouraged to enroll in a clinical trial with a novel therapy or to proceed with an allogeneic stem - cell transplantation , the use of hmas , because the response to such therapy is predicted to be low . 
although all patients with mds should be encouraged to enroll in a clinical trial with novel therapies , having biomarkers that accurately predict resistance may ease the conversation with some patients who are hesitant to try newer approaches and prefer food and drug administrationapproved therapies.19 alternatively , patients with higher - risk disease and a high blast percentage may consider intensive , aml - type chemotherapy before allogeneic stem - cell transplantation , as opposed to an hma that is predicted to do little to affect the disease in the absence of other biomarkers that could predict resistance to chemotherapy , such as complex karyotype cytogenetics , and the presence of tp53 mutations and the absence of targetable mutations such as idh1 and idh2 . 
because the optimal timing for patients with mds with lower - risk disease can be challenging and because these genomic biomarkers predicted poor outcome even in patients with lower - risk disease . 
these biomarkers could be used as a justication to proceed with allogeneic stem - cell transplantation early in the disease course , especially if the patient has a lower blast percentage . 
in addition , identifying , with high accuracy , patients who may or may not respond to therapy can prevent prolonged exposure to ineffective therapy and can lead to lower cost without decreasing value or changing patient outcomes . 
introducing these biomarkers into normal hematopoietic cells using crispr / cas9 may offer an opportunity to model and understand hma resistance to develop novel drugs to overcome this resistance . our study highlights the importance of machine learning algorithms such as the recommender system in translating genomic data into useful clinical tools that can be used by physicians in the clinic.20 nevertheless , some limitations to our approach exist . 
it is possible that the response to hmas is derived mainly from epigenetic changes and is not dependent on the genomic changes that we studied here . in summary , our study identied genomic abnormalities that predict response or resistance to hmas in patients with mds , and we validated our results in an independent patient cohort treated in a randomized clinical trial . 
identication of biomarkers that can provide personalized treatment approaches that can predict response or resistance to cancer therapy remains an important clinical challenge , and future drug development should focus on identifying the subgroup of patients who may benet the most from any given cancer therapy . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . open payments is a public database containing information reported by companies about payments made to us - licensed physicians open payments . aziz nazha honoraria : dci consulting or advisory role : karyopharm therapeutics , tolero pharmaceuticals speakers bureau : novartis , incyte research funding : jazz pharmaceuticals mikkael a . 
sekeres consulting or advisory role : celgene , millennium pharmaceuticals , syros pharmaceuticals research funding : takeda pharmaceuticals ( inst ) , pzer ( inst ) rafael bejar honoraria : celgene , alexion pharmaceuticals , abbvie / genentech , astex pharmaceuticals , neogenomics laboratories , daiichi sankyo , forty seven consulting or advisory role : celgene , foundation medicine , neogenomics laboratories , abbvie / genentech , astex pharmaceuticals , daiichi sankyo research funding : celgene , takeda pharmaceuticals travel , accommodations , expenses : celgene megan othus consulting or advisory role : celgene , glycomimetics , cascadia laboratories rami s . 
komrokji stock and other ownership interests : abbvie consulting or advisory role : celgene , novartis , daiichi sankyo , pzer , janssen pharmaceuticals , agios , incyte speakers bureau : novartis , alexion pharmaceuticals , jazz pharmaceuticals travel , accommodations , expenses : celgene , incyte , alexion pharmaceuticals , novartis , jazz pharmaceuticals , daiichi sankyo david p . 
blood 123 : 829 - 836 , 2014 fenaux p , mufti gj , hellstrom - lindberg e , et al : efcacy of azacitidine compared with that of conventional care regimens in the treatment of higher - risk myelodysplastic syndromes : a randomised , open - label , phase iii study . 
lancet oncol 10 : 223 - 232 , 2009 l ubbert m , suciu s , baila l , et al : low - dose decitabine versus best supportive care in elderly patients with intermediateor high - risk myelodysplastic syndrome ( mds ) ineligible for intensive chemotherapy : final results of the randomized phase iii study of the european organisation for research and treatment of cancer leukemia group and the german mds study group . 
j clin oncol 29 : 1987 - 1996 , 2011 steensma dp , baer mr , slack jl , et al : multicenter study of decitabine administered daily for 5 days every 4 weeks to adults with myelodysplastic syndromes : the alternative dosing for outpatient treatment ( adopt ) trial . 
leuk res 41 : 43 - 47 , 2016 zeidan am , sekeres ma , garcia - manero g , et al : comparison of risk stratication tools in predicting outcomes of patients with higher - risk myelodysplastic syndromes treated with azanucleosides . 
leukemia 30 : 649 - 657 , 2016 itzykson r , th epot s , quesnel b , et al : prognostic factors for response and overall survival in 282 patients with higher - risk myelodysplastic syndromes treated with azacitidine . 
blood 117 : 403 - 411 , 2011 takahashi k , patel k , bueso - ramos c , et al : clinical implications of tp53 mutations in myelodysplastic syndromes treated with hypomethylating agents . oncotarget 7 : 14172 - 14187 , 2016 9 . 
sekeres ma , othus m , list af , et al : randomized phase ii study of azacitidine alone or in combination with lenalidomide or with vorinostat in higher - risk myelodysplastic syndromes and chronic myelomonocytic leukemia : north american intergroup study swog s1117 . 
short nj , kantarjian hm , loghavi s , et al : treatment with a 5 - day versus a 10 - day schedule of decitabine in older patients with newly diagnosed acute myeloid leukaemia : a randomised phase 2 trial . 
 significant tumor response to the poly ( adp - ribose ) polymerase inhibitor olaparib in heavily pretreated patient with ovarian carcinosarcoma harboring a germline rad51d mutation introduction brca1 and brca2 are the best - known examples of proteins that contribute to repair of double - strand dna breaks via the homologous recombination repair ( hrr ) pathway . the rad51 paralogs rad51b , rad51c , and rad51d are proteins that are also involved in the hrr pathway . 
parp inhibitors are rationally designed drugs that inhibit parp1 by trapping the inactivated enzyme onto the single - strand break , generating a potential block for cellular dna replication.5 - 7 trapped parp - dna complexes can lead to the stalling and / or collapse of replication forks , resulting in the generation of more deleterious double - strand breaks.8 in cells unable to carry out hrr because of brca mutation , the added genotoxic stress of inhibition of single - strand repair is cytotoxic and referred to as synthetic lethality.5 , 7 in vitro and mice studies support the use of parp inhibition , not only in the presence of brca mutation but also in malignancy with other genetic defects that affect hrr , such as rad51 deletion.9 given the rarity of rad51 mutations , there is limited clinical evidence in this context . we describe a heavily pretreated patient with ovarian carcinosarcoma , with known germline rad51d mutation , that exhibited a remarkable and durable response to parp inhibitor therapy . 
subsequently the patient experienced remissions of varying degrees and durations , with additional lines of therapy including paclitaxel , cisplatin , ifosfamide , and doxorubictwo years before presentation of this case report , the patient was enrolled in a phase i clinical trial using a novel pd - 1 inhibitor . 
 a writing , the patient continues to take olaparib , with no evidence of disease regrowth . discussion synthetic lethality is a term used to describe the combination of two defects that do not affect cell viability when each occurs individually but are cytotoxic when they occur simultaneously in a single cell.7 , 10 parp inhibitors have been used to exploit synthetic lethality in brca1and brca2 - mutant ovarian , breast , prostate , and other cancers . 
 however , hrr deficiency extends beyond cancers harboring brca1 / 2 mutations , and the term brcaness has been coined to describe the clinical and biologic features of such tumors . 
 this not only includes similar histomorphological features such as basal - like phenotype in breast cancers or high - grade serous morphology in ovarian cancers , but also similar immunophenotypic profile ( eg , triple - negative breast cancers ) , drug sensitivity ( eg , to platinum agents and parp inhibitors ) , as well as prognosis.11 - 13 the brcaness phenotype is seen in tumors with loss - of - function mutations involving other hrr pathway genes , including atm , atr , bard1 , brip1 , mre11a , palb2 , rad50 , rad51d , rad54 , nbs1 , chek1 , and chek2 , as well as components of the fanconi anemia repair pathway.13 , 14 in vitro and mice studies have demonstrated efficacy of parp inhibitors against cancer cells with defects in rad51 . 
separate studies by shah et al , cruz et al , and wang et al found that breast or ovarian cancer cells with absent or low levels of rad51 were sensitive to parp inhibitors.15 - 17 another study observed that parp inhibitor sensitivity was increased by 1 , 000 - fold in cells that are rad51 knockdown.14 cruz et al and wang et al additionally demonstrated that the presence of rad51 conferred resistance to parp inhibitors in these cells.16 , 17 in their experiments on triple - negative breast cancer cells , wang et al postulated that it may be possible to expand the sensitivity of triple - negative breast cancer to parp inhibitors by targeting rad51.17 other studies found increased sensitivity to parp inhibition when rad51 inhibitors were coadministered.10 , 18 interestingly , falchi et al found the addition of a brca2 - rad51 disruptor to parp inhibition to be synergistic , rather than merely additive , which is probably a consequence of fig 1 . 
 ( a ) baseline computed tomography ( ct ) scan of pelvis , demonstrating heterogeneous mass ( arrowhead ) , ( b ) ct scan after 8 weeks on olaparib , showing excellent partial response in pelvic mass ( arrowhead ) , and ( c ) ct scan after 16 weeks on olaparib , showing additional disease response ( arrowhead )  . disease response for 16 months , followed by rapid and significant tumor regrowth ( fig 1a )  . the patient had previously been determined to have a germline mutation in rad51d , evidenced by a heterozygous variant c.263 + 1g > a . 
 this mutation has previously been described in ovarian cancer.4 with the possibility of defective hrr in the patients tumor as the result of loss of the remaining functional rad51d allele , a therapeutic trial of olaparib was initiated . 
we are not aware of other case reports that have demonstrated disease response to parp inhibitors in tumors with an underlying rad51d mutation . our clinical experience is consistent with preclinical models and adds to the current limited clinical evidence of benefit of parp inhibition in the context of rad51 mutations . 
chandran no relationship to disclose ian kennedy no relationship to disclose the simultaneous inhibition of two dna - repair mechanisms.10 a 2016 phase ii study ( ariel2 ; a study of rucaparib in patients with platinum - sensitive , relapsed , high - grade epithelial ovarian , fallopian tube , or primary peritoneal cancer ) used the parp inhibitor rucaparib in recurrent , platinum - sensitive , high - grade ovarian carcinoma . 
 of 206 patients , there were seven with rad51 mutations : one patient with rad51b mutation with stable disease , who was receiving rucaparib ; four patients with rad51c mutations ( three partial responses and one patient with stable disease ) ; and two patients with rad51d mutation , both with stable disease.19 using baseline and postprogression biopsy samples from the same study , kondrashova et al reported that in five of six patients with rad51c and rad51d truncation mutations that subsequently developed resistance to rucaparib , there were one or more secondary mutations restoring the open reading frame . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
song h , dicks e , ramus sj , et al : contribution of germline mutations in the rad51b , rad51c , and rad51d genes to ovarian cancer in the population . 
tan dsp , rothermundt c , thomas k , et al : brcaness syndrome in ovarian cancer : a casecontrol study describing the clinical features and outcome of patients with epithelial ovarian cancer associated with brca1 and brca2 mutations . 
mccabe n , turner nc , lord cj , et al : deficiency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
shah mm , dobbin zc , nowsheen s , et al : an ex vivo assay of xrt - induced rad51 foci formation predicts response to parp - inhibition in ovarian cancer . 
cruz c , castroviejo - bermejo m , gutirrez - enrquez s , et al : rad51 foci as a functional biomarker of homologous recombination repair and parp inhibitor resistance in germline brca - mutated breast cancer . 
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 r predictive biomarkers in metastatic colorectal cancer : a systematic review juan ruiz - baobre , md1 , 2 , 3 ; raju kandimalla , phd2 ; and ajay goel , phd2 purpose the development and use of predictive biomarkers to guide treatment decisions are paramount not only for improving survival in patients with metastatic colorectal cancer ( mcrc ) , but also for sparing them from unnecessary toxicity and reducing the economic burden of expensive treatments . 
we conducted a systematic review of published studies and evaluated the predictive biomarker landscape in the mcrc setting from a molecular and clinical viewpoint . methods studies analyzing predictive biomarkers for approved therapies in patients with mcrc were identied systematically using electronic databases . 
of all the biomarkers analyzed , 1.4% ( two of 148 ) were explored in a prospective manner , whereas 98.6% ( 146 of 148 ) were evaluated in retrospective studies . 
of the latter group , 78.8% ( 115 of 146 ) were not tested in subsequent phases , 9.6% ( 14 of 146 ) were tested in other retrospective cohorts , 8.9% ( 13 of 146 ) were retrospectively tested in at least one or more randomized cohorts , and only 2.7% ( four of 146 ) were prospectively tested in a clinical trial . 
2019 by american society of clinical oncology introduction colorectal cancer ( crc ) remains the third leading cause of cancer - related deaths in the western world . despite ongoing efforts aimed at increased population screening and improved early detection strategies , approximately 20% of patients still present with metastatic disease at diagnosis , and approximately 35% of those who undergo curative surgeries for a localized disease relpase.1 during the past three decades , the median overall survival ( os ) of patients with metastatic crc ( mcrc ) has gradually increased because of the implementation of combined chemotherapy regimens as well as targeted molecular therapies against egfr and angiogenic factors.2 since the identication of ras mutations as a negative predictive marker , antiegfr therapy has had the greatest impact on the management of patients with mcrc ; nonetheless , the response rates of these treatments remain only approximately 40% to 60% . 
in addition , the recognition landscape for immunotherapy in the treatment patients with microsatellite instability - high ( msi - h ) or dna decient mismatch - repair ( dmmr ) mcrc has been encouraging for this subset of patients . 
crc , colorectal cancer ; mcrc , metastatic colorectal cancer ; neoadjuvant - crt , neoadjuvant chemoradiotherapy . 2 2019 by american society of clinical oncology conventional chemotherapy and triuridine / tipiracil the backbone of treatment in patients with mcrc has historically been chemotherapy , and several chemotherapeutic agents are now approved in this setting : uoropyrimidines ( uorouracil [ fu ] and capecitabine ) , oxaliplatin , irinotecan , and since 2015 , triuridine / tipiracil ( tas - 102 )  . fluoropyrimidine - based chemotherapy and tas - 102 . 
studies of the role of thymidylate synthase ( ts ) in uoropyrimidine - based therapy ( primarily fu plus leucovorin ) in various retrospective and prospective studies have yielded discordant results . 
in this regard , multiple studies have shown that low levels of ts expression in metastatic tumor tissues generally correlate with higher overall response rate ( orr ) .3 - 6 surprisingly , such a correlation was not evident when ts levels were measured in primary tumor tissues.4 , 7 similarly , low levels of ts and dihydropyrimidine dehydrogenase in metastatic tumor tissues were associated with a favorable response to fu in patients with mcrc8 ; however , a subsequent report in 2006 did not validate these ndings.9 likewise , the role of thymidine phosphorylase as a predictive biomarker was also investigated , but the results remain inconclusive.10 , 11 in 2009 , a meta - analysis of ve studies examining a total of 861 patients with mcrc concluded that compared with microsatellite - stable patients , msi - h patients did not achieve a statistically signicant better response rate to fu - based chemotherapy.12 similarly , while investigating the relationship between msh2 gene expression and capecitabine efcacy in patients with mcrc , jensen et al13 observed that a higher msh2 expression was associated with a better response . 
in 2015 , hamauchi et al30 found that patients who develop grade 3 or 4 neutropenia during the rst cycle of tas - 102 treatment had a smaller risk of disease progression . 
selected biomarkers the nal analysis . distribution of biomarkers by individual treatment group . ( b ) distribution of biomarkers by study design . antipd - 1 , antiprogrammed cell death - 1 drugs ; fu , uoropyrimidine - based chemotherapy ; irinotecan , irinotecan - based chemotherapy ; msi , microsatellite instability ; oxaliplatin , oxaliplatin - based chemotherapy ; tas - 102 , triuridine / tipiracil . 
 ( * ) predictive biomarker for anti - egfr drugs ( cetuximab / panitumumab ) ; ( ) predictive biomarker for antipd - 1 drugs ( pembrolizumab and nivolumab alone or in combination with ipilimumab )  . testing in 1 randomized cohorts ( n = 13 ; 8.9% ) ras mutations * testing in a clinical trial ( n = 4 ; 2.7% ) msi status oxaliplatin - based chemotherapy . 
the most notable attempts in this regard have been for the ercc1 gene , and as reported from the mavericc ( marker evaluation for avastin research in crc ) trial , intratumoral ercc1 gene expression failed to predict response to oxaliplatin treatment.17 another gene evaluated in this setting was the x - ray repair cross - complementing group 1 ( xrcc1 ) gene , a base excision repair modulator , wherein a polymorphism in this gene ( xrcc1 - 839 arg / gln or gln / gln ) correlated with worse orr to fu / oxaliplatin.18 interestingly , several micrornas ( mirnas ) have been explored for their predictive response potential to fu , leucovorin , and oxaliplatin ( folfox ) or capecitabine plus oxaliplatin ( capeox ) based regimens . 
using a proteomic approach in 2010 , aoyagi et al32 reported that lower levels of plasma soluble vascular endothelial growth factor ( vegf ) receptor 1 were associated with improved disease control in a subset of 46 patients treated with modied fu , leucovorin , and oxaliplatin ( mfolfox6 ) plus bevacizumab . 
in the same year , another study identied a signicant correlation between low angiopoetin - 2 serum levels and better survival outcomes in a cohort of patients with mcrc treated with bevacizumab - based therapy.33 conversely , the correlation between vegf - a levels and the clinical benet of bevacizumab - based chemotherapy is still under evaluation . 
perhaps in the near future , mavericc trial results will offer more insights into the usefulness of plasma vegf - a levels in this setting.17 with regard to the predictive role of ras , in a subset of 230 patients with mcrc treated in a phase iii randomized clinical trial with either irinotecan , fu , and leucovorin ( ifl ) plus placebo , or ifl plus bevacizumab , only the wild - type kras subset of patients obtained a signicantly higher response rate in the bevacizumab arm.35 in addition to the molecular markers listed previously , a few clinical factors have been studied in relation to bevacizumab response . 
two retrospective studies based on the data from the correct ( patients with metastatic colorectal cancer treated with regorafenib or placebo after failure of standard therapy ) and consigna ( regorafenib in subjects with metastatic colorectal cancer who have progressed after standard therapy ) trials have evaluated the usefulness of different computed tomography scan based parameters in predicting the clinical benet of regorafenib therapy . 
one of the rst studies , in 2016 , reported a correlation between improved pfs and lung metastases cavitation before therapy initiation and even at week 8.38 in this study , baseline lung metastases cavitation and changes in the sum of target lesion diameters were deemed to be predictors for improved os in the multivariate analysis . 
a year later , the correct trial also demonstrated a signicant association between survival ( pfs and os ) and several radiologic parameters such as response or stable disease in size and density of lung metastases.39 likewise , highlighting the use of dynamic contrast - enhanced magnetic resonance imaging , a recent study reported that a  . 
these and other potential predictive biomarkers for anti - egfr therapy are summarized in table 3 and in the data supplement . antiprogrammed cell death - 1 drugs : pembrolizumab and nivolumab in may and july of 2017 , the us food and drug administration approved pembrolizumab and nivolumab for the treatment of patients with msi - h mcrc in whom the disease has progressed after treatment with uoropyrimidine , oxaliplatin , and irinotecan therapies . 
almost a year later , in july 2018 , a nivolumab plus ipilimumab combined regimen was approved , which opened up three novel treatment options for patients with msi - h or dmmr mcrc , who represent approximately 5% of all patients with mcrc.23 the belief is that , despite their worse prognosis , a large prolymphocytic inltration and the presence of portion of mutation - associated neoantigens61 confer to patients with msi - positive mcrc the clinical benet they derive from antiprogrammed cell death - 1 ( pd - 1 ) therapy.62 - 65 this exciting discovery has now led to universal msi testing for the management of patients with mcrc . disease monitoring by liquid biopsies recently , liquid biopsies have emerged as powerful tools for monitoring disease evolution and therapeutic response through the analysis of cell - free dna and rna biomarkers in bodily uids . 
one of the rst studies , in 1979 , which reported that a gradual decrease in carcinoembryonic antigen ( cea ) levels during chemotherapy was signicantly associated with better survival rates , was the basis for this concept.66 such a correlation between cea are and improved pfs and os was conrmed a few years later in a subset of 670 patients with mcrc undergoing rst - line chemotherapy.67 although cea is not a crc - specic biomarker , cea monitoring in blood , alone or in addition to ca 19 - 9 , 68 is still performed commonly in routine clinical practice . 
in this context , the accuracy of cea change in predicting disease progression has been demonstrated recently in a study involving 2 , 828 patients from seven rstline clinical trials.69 in addition to this , other analyses of circulating tumor cells70 and endothelial cells71 in mcrc have been undertaken by several groups . 
in 2015 , hansen et al72 reported that circulating levels of mirna - 126 in a subset of 68 patients with mcrc were predictive of tumor response to bevacizumab - based chemotherapy . 
since then , multiple studies have reported distinct genetic alterations in ctdna from patients with primary disease or acquired resistance to antiegfrbased therapies in genes such as kras , nras , met , erbb2 , flt3 , egfr , and map2k1 by droplet digital polymerase chain reaction , beaming , and next - generation sequencing methodologies.74 , 75 using a massively parallel sequencing - based assay in a prospective cohort of 53 patients with mcrc , it was shown that early changes in ctdna during rst - line standard chemotherapy can also predict subsequent radiologic response.76 similarly , 2017 , a study demonstrated a signicant correlation between the decrease in ras mutant clones in blood after 8 weeks of therapy and improved pfs and os in a cohort of patients treated with regorafenib.40 intriguingly , clonal evolution is a dynamic process , yet the emergence of drugresistant clones in circulation increases during treatment , whereas drug withdrawal results in a decrease of such clones . 
the understanding of this fact has paved a path for novel treatment strategies that are already under evaluation as part of the rasintro ( ras mutations in ctdna and anti - egfr reintroduction in mcrc ) study ( clinicaltrials . gov identier : nct03259009 ) and the chronos ( rechallenge with panitumumab driven by ras dynamic of resistance ) trial ( clinicaltrials.gov identier : nct03227926 ) , which are evaluating the predictive impact of ctdna ras mutations on the efcacy of anti - egfr monotherapy rechallenge in patients with ras wild - type mcrc whose disease has progressed after anti - egfrfree chemotherapy . 
in addition , a ve - gene methylation panel for monitoring tumor burden in liquid biopsies using a methylbeaming assay was described recently77 in 182 patients with mcrc treated with chemotherapy and / or targeted therapy , in which the authors discovered a signicant correlation between the dynamics of methylation markers and orr and pfs . discussion despite the tremendous body of effort devoted to the identication of predictive biomarkers for various treatments used in patients with mcrc , thus far only two of such markers have been translated into routine clinical practice . the rst one , the mutations in the ras gene , serves as a negative predictive biomarker that is present in approximately 55% of patients with mcrc78 and correlates with the lack of efcacy of anti - egfr antibody treatments . 
the exciting result of the association between msi - h and response to nivolumab in the rst - in - human clinical trial ( clinicaltrials . gov identier : nct00441337 ) led to two subsequent phase ii clinical trials , which were instrumental in the approval of antipd - 1 drugs ( pembrolizumab or nivolumab ) alone or in combination with ipilimumab ( nivolumab plus ipilimumab ) as a treatment option for patients with msi - h or dmmr mcrc.63 - 65 , 79 other well - described predictive biomarkers used in the management of several tumor types have shown promising usefulness in selecting patients with mcrc for various targeted therapy - based regimens . 
results from two clinical trials in patients with braf v600epositive mcrc have highlighted this mutation as a predictive biomarker for braf inhibitorbased regimens ( data supplement ) .80 , 81 regarding the role of human epidermal growth factor receptor 2 ( her2 ) amplication or overexpression as a predictive biomarker results of two phase ii clinical trials evaluating the dual her2 blockade in a biomarker - selected subset of heavily pretreated patients with mcrc , with either trastuzumab plus lapatinib ( heracles [ her2 amplication for colorectal cancer enhanced stratication ] trial ) or with pertuzumab and trastuzumab ( mypathway trial ) , demonstrate an impressive orr of approximately 30% to 40% ( data supplement ) .82 , 83 for anti - her2based therapies , nonetheless , the discovery and validation of novel predictive biomarkers that can assist in decision making has been a challenging endeavor , resulting in a long list of failed predictive markers . 
in crc , because the use of single - agent chemotherapeutic regimens has shown limited efcacy , and the majority of current treatment options include various combinations of drugs , biomarker discovery for specic drugs is more complicated , not surprisingly , because of the interactions among different cytotoxic agents.84 similar concerns remain regarding developing predictive biomarkers for therapeutic response to bevacizumab , because ( 1 ) it is also not used as a single agent in the clinic , 84 ( 2 ) its mechanisms of action are poorly understood , 85 and ( 3 ) angiogenesis is an intriguingly adaptive process that involves numerous factors.86 presumably , the inherent complexity of angiogenesis has been a substantial hurdle in the attempts to develop responsepredictive biomarkers for other multitargeted antiangiogenic drugs such as aibercept or regorafenib . 
 predictive biomarkers in metastatic colorectal cancer a possible source of discrepancy even when the molecular marker is analyzed in a different region of the same source.88 besides their spatial heterogeneity , tumors are dynamic entities that continue to evolve over time , especially if they are under selective pressure.89 for this reason , the time from sample acquisition to biomarker analysis is of clinical relevance ; however , overlooked in most studies . 
because only approximately 20% of patients with crc present with metastatic disease at the time of diagnosis , it is often the practice or only option available to analyze archival tissues from the primary tumor to identify biomarkers , which is not always optimal.90 this is an issue that patient selection is gaining importance , which is evidenced by the recent initiative , the us national cancer institutes exceptional responder program.91 consideration of extreme phenotypes such as long - term responders and extremely early progressors for biomarker discovery can facilitate successful identication of molecular alterations that better correlate with clinical phenotypes . 
for instance , in the majority of studies presented in this article , there was no consideration of pfs as a selection criterion , and many studies included in the nonresponders patients with stable disease . 
in general , improved orr and longer pfs are superior indicators of the true efcacy of any drug intervention , whereas inclusion of gain in os as a selection feature may inadvertently introduce bias . 
in addition , new biomarker - driven study designs such as basket or umbrella trials , which assign a treatment according to tumor molecular characteristics , not only are going to improve clinical drug development , but also will facilitate improved biomarker validation . 
besides the examples already described previously in the text , new drugs that target tyrosine kinase fusions in genes such as nrtk1 / 2 / 3 , ret , alk , and ros1 are emerging with promising preliminary results in phase i and ii clinical trials that include patients with crc ( data supplement ) .92 - 97 although analysis of clinical specimens with robust followup data from retrospective series or randomized trials are of tremendous value , subsequent prospective clinical cohorts using longitudinally collected specimens are much needed to establish clinically translatable predictive biomarkers . 
in addition , although many surgical specimens are of suitable quality , needle biopsyderived metastatic lesions often yield lower amounts of dna and rna than that required for robust sequencing experiments98 , 99 ; having access to liquid biopsybased predictive markers would be transformative in overcoming this limitation in patients with mcrc . 
furthermore , liquid biopsy biomarkers will improve patient compliance and eliminate the concerns surrounding intratumor heterogeneity associated with tumor or biopsy specimens and may also help in disease monitoring as well as in predicting secondary resistance . the international community has to consolidate initiatives to improve biomarker development studies and , more importantly , undertake conscious efforts to validate the results gathered from retrospective studies in prospective randomized multicenter cohorts . 
last , the implementation of novel high - throughput molecular analytic techniques and the integration of multiomic approaches with clinical and epidemiologic data using machine - learning algorithms will denitely hasten biomarker development in the coming years.100 despite many attempts over the past decades , there remain only two well - established predictive biomarkers , mutations in the ras gene and msi status , that currently guide treatment decisions in patients with mcrc . 
 ruiz - baobre , kandimalla , and goel juan ruiz - baobre travel , accommodations , expenses : bristol - myers squibb , merck sharp & dohme , ipsen , pharmamar no other potential conicts of interest were reported . references siegel rl , miller kd , jemal a : cancer statistics , 2018 . 
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cancer discov 7 : 400 - 409 , 2017 amatu a , somaschini a , cerea g , et al : novel cad - alk gene rearrangement is drugable by entrectinib in colorectal cancer . 
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j natl cancer inst 109 ( 12 ) : djx089 , 2017 kris mg , johnson be , berry ld , et al : using multiplexed assays of oncogenic drivers in lung cancers to select targeted drugs . 
 clinicopathologic features of non small - cell lung cancer harboring an ntrk gene fusion purpose gene rearrangements that involve ntrk1 / 2 / 3 can generate fusion oncoproteins that contain the kinase domains of trka / b / c , respectively . 
despite the potential benefit of identifying these fusions , the clinicopathologic features of ntrk fusion - positive nsclcs are not well characterized . methods we compiled a database of patients with nsclcs that harbor ntrk fusions . 
 we characterized clinical , molecular , and histologic features with central review of histology . results we identified 11 patients with nsclcs that harbor ntrk gene fusions verified by next - generation sequencing and with available clinical and pathologic data . 
nine patients had adenocarcinoma , including two with invasive mucinous adenocarcinoma and one with adenocarcinoma with neuroendocrine features ; one had squamous cell carcinoma ; and one had neuroendocrine carcinoma . 
2018 by american society of clinical oncology introduction the neurotrophin kinase ( ntrk ) genes ntrk1 , ntrk2 , and ntrk3 encode the tropomyosin receptor tyrosine kinases trka , trkb , and trkc , respectively , which function during normal neuronal development and maintenance . 
of patients male female smoking history , pack - years median pack - years of smoking ( range ) stage at diagnosis ( ajcc seventh edition , criteria ) 5 - 20 > 20 bone lung liver brain histology ( local assessment ) adenocarcinoma squamous cell carcinoma neuroendocrine carcinoma no . 
 ( % ) 48 ( 25 - 86 ) 6 ( 55 ) 5 ( 45 ) 8 ( 73 ) 3 ( 27 ) 0 ( 0 - 58 ) 2 ( 18 ) 1 ( 9 ) 8 ( 73 ) 9 ( 82 ) 1 ( 9 ) 1 ( 9 ) trk signaling in preclinical models results in cell death and tumor regression.4 in early - phase clinical trials , solid tumors that harbor ntrk gene rearrangements have been highly sensitive to selective trk tyrosine kinase inhibitors ( tkis ) , including larotrectinib , which is selective for trka / b / c , and entrectinib , which targets trka / b / c as well as alk and ros1 . 
among four patients with nsclc , response evaluation criteria in solid tumors ( recist ) responses were seen in three , and the fourth had an approximately 20% reduction in tumor size . 
one of four ntrk - rearranged tumors treated with entrectinib in an adult phase i trial was nsclc , and this patient had a partial response , including a complete response in the cns.9 despite the potent activity of trk inhibitors , the clinical and pathologic features of ntrk - rearranged nsclcs are poorly defined . 
 we show that ntrk fusions occur across age and smoking status and suggest that all patients with nsclc be screened for fusions by using a multiplexed next - generation sequencing ( ngs ) assay . methods physicians across seven institutions contributed de - identified patients with nsclc to an ntrk fusion nsclc database . 
assays used identified fusions through a variety of technologies : rna - based fusion - targeted anchored multiplex polymerase chain reaction ( pcr ) and illumina ( san diego , ca ) sequencing10 ( massachusetts general hospital [ mgh ] solid fusion assay , memorial sloan kettering [ msk ] solid fusion assay , archerdx fusionplex performed at caris life sciences [ irving , tx ] ) ; dna hybridization capture with intron tiling and illumina sequencing ( foundationone11 [ foundation medicine , cambridge , ma ] , msk - integrated mutation profiling of actionable cancer targets [ impact ] 12 , 13 ) , total nucleic acid extraction , pcr amplification , and ion torrent sequencing ( pcdx14 ; paradigm , phoenix , az )  . the kaplan - meier method was used to obtain estimates of overall survival from diagnosis of stage iv disease to death or last follow - up ( censored )  . 
data collection and analysis were performed under institutional review boardapproved protocols . results we reached out to physicians at 47 institutions in the united states who were actively participating in a trk inhibitor clinical trial that enrolled adult patients and invited them to contribute data on living or deceased patients with nsclcs that harbored an ntrk gene rearrangement . 
candidate fusions initially were identified by using a combination of rnaand dna - based ngs assays , with validation by one or more of rna - based ngs , fluorescent in situ hybridization , and reverse transcription pcr on a patient - by - patient basis . 
 among these patients , in - frame trk fusions that contained the kinase domain were verified in 11 , which formed the study cohort . of note , three patients were excluded from the study cohort for the following reasons . 
note that exons are drawn at a larger scale than introns and that introns are not drawn to the same scale for each gene ( ntrk1 locus is approximately 21 kilobases [ kb ] , ntrk2 is approximately 358 kb , and ntrk3 is approximately 384 kb )  . 
this group includes patients 1 to 4 , 11 , and s1 to s6 . abbreviations : mgh , massachusetts general hospital ; mskcc , memorial sloan kettering cancer center ; nsclc , nonsmall - cell lung cancer . fusion assay , an rna - based fusion - specific targeted ngs assay that uses anchored multiplex pcr.10 the candidate fusion contained p2ry8 exon 2 fused with ntrk1 exons 1 to 5 . 
the second patient had an ntrk2 intragenic deletion that disrupted the exon 18 3 splice site , which is predicted to disrupt the kinase domain and , therefore , to be inactivating . 
this patient also had a concurrent her2 l755p mutation , which is predicted to be activating.15 the clinical characteristics of the 11 patients in the study cohort are listed in table 1 . 
patient 4 had a candidate ntrk1 fusion detected by msk - impact with an equivocal partner , and the correct fusion partner was determined using the msk solid fusion assay . 
all ntrk fusions couple the kinase domain of ntrk1 or ntrk3 ( with or without the membrane - spanning helix ) to an n - terminal gene fusion partner with domains known or predicted to mediate dimerization or oligomerization ( table 2 ; fig 1 )  . 
in all patients tested , potential oncogenic alterations in the following genes , when interrogated , were not detected : kras ( zero of 10 ) , egfr ( zero of 11 ) , alk ( zero of 11 ) , ros1 ( zero of 11 ) , braf ( zero of 11 ) , pik3ca ( zero of 10 ) , her2 ( zero of eight ) , and met ( zero of eight )  . to estimate the overall frequency of ntrk fusions in nsclc , we reviewed consecutively tested patients with nsclc from mgh and the msk cancer center , where ngs screening of 4 , 872 unique patients identified 11 ntrk fusions ( 0.23% ; table 3 )  . 
five of these patients had available clinical and pathologic data for inclusion in the study cohort , and we report the molecular details of the additional six patients ( s1 to s6 ; appendix table a1 )  . 
we diagram the fusion positions of all 17 of these patients ( study cohort patients 1 to 11 plus patients s1 to s6 ) in figure 1 . we next examined the histologic features of the 11 patients who formed the study cohort . 
among the patients with adenocarcinoma , we observed a range of histologic subtypes , including adenocarcinoma with neuroendocrine features ( patient 2 ; fig 2a ) , poorly differentiated adenocarcinoma with solid pattern and signet ring cells ( patient 1 ; fig 2b ) , and invasive mucinous adenocarcinoma ( patients 4 and 6 ; fig 2c )  . 
 ( a ) patient 2 had an adenocarcinoma with solid growth pattern , diffuse neuroendocrine differentiation , and signet ring cells ; inset shows high magnification ( x400 )  . 
 ( e ) patient 11 had neuroendocrine carcinoma with well - differentiated morphology and increased mitotic activity ( left ) ; high magnification ( x400 ) shown in middle . ttf1 chromogranin mucicarmine ttf1 ttf1 synaptophysin absence of ttf1 ( patient 8 ; fig 2d )  . 
patient 11 ( fig 2e ) had a morphologically well - differentiated neuroendocrine tumor ( equivalent to atypical carcinoid ) with an increased mitotic index of 12 per 10 high - power fields and a brain metastasis ; this tumor was classified as large - cell neuroendocrine carcinoma in accordance with current who criteria.16 although analysis of the cohort is limited by size and the fact that this review is retrospective across multiple institutions , we sought to describe clinical outcomes in these patients . 
the median overall survival of the 10 patients with metastatic disease was 40.8 months ( 95% ci , 0.79 months to not reported ) , with a median follow - up of 52.8 months ( fig 3 )  . three patients had early - stage disease at the time of diagnosis . 
patient 4 had stage iib ( t3n0 ) disease at diagnosis , was treated with surgery followed by adjuvant cisplatin and pemetrexed , and remained recurrence free at the most recent follow - up 30.0 months after initial diagnosis . 
patient 6 had stage iia ( t1bn1 ) disease at diagnosis , was treated with surgery followed by cisplatin and pemetrexed , and developed metastatic disease 24.5 months after initial diagnosis . 
we describe the clinicopathologic features of a cohort of 11 patients with nsclcs harboring ntrk gene rearrangements that resulted in the fusion of the trk tyrosine kinase domain with a dimerization - inducing partner . 
these are predicted or previously have been reported to be activating.4 , 17 the current cohort includes both men and women across a range of ages , histologies , and smoking histories . 
 although the cohort is small , the only defining pattern of clinical characteristics that emerges is the lack of an alternate canonical driver mutation in all patients , similar to others with kinase fusion - positive nsclcs.18 of note , ntrk rearrangements were identified in patients with and without a history of smoking ; although the majority of patients ( eight [ 73% ] of 11 ) had a minimal to never smoking history , three of the 11 had a history of 30 pack - years . 
similarly , alk - , ros1 - , and ret - driven nsclcs are enriched in never - smokers but can be seen in current and former smokers as well.5 , 19 , 20 nine of the 11 patients had adenocarcinoma that tended to be mucinous or poorly differentiated , including one with a tpr - ntrk1 fusion with fig 3 . 
however , other histologies also were observed , including one squamous cell carcinoma with an etv6 - ntrk3 fusion and one neuroendocrine carcinoma with an sqstm1 - ntrk3 fusion . ascertainment bias as a result of selective testing has historically limited an accurate assessment of frequency of ntrk fusions in nsclc . 
 these assays generally are used at the time of tissue diagnosis in both institutions ; therefore , this population likely represents a previously unscreened group in which patients were not already selected to be negative for other known driver mutations in lung cancer . 
we note that cancers selected for molecular testing may be enriched for patients with metastatic disease because no established role exists for targeted therapies in early - stage lung cancer to date . 
 although ntrk fusions are rare in lung cancer , we estimate that with approximately 234 , 000 new nsclc diagnoses annually in the united states , > 500 of these patients may be candidates for highly effective trk inhibitor therapy . 
 significantly more patients with ntrk fusion nsclc may exist when considering the global incidence of lung cancer . the natural history of ntrk fusion nsclcs , compared with nsclcs in general , is not well established . 
although we observed a median overall survival of 40.8 months among the 10 patients with metastatic disease , we acknowledge the small size of this retrospective cohort , among whom eight received at least one trk tki . 
the observation that one of two patients diagnosed at stage ii and one at stage iii developed relapsed metastatic disease is consistent with the natural history of nsclcs in general , although selection bias may have existed against screening patients with early - stage cancer who did not develop metastatic disease . because there seems to be no uniform defining clinical or pathologic feature of ntrk fusion positive nsclcs , we recommend screening all nsclcs for ntrk gene rearrangements . 
 advantages over dna - based methods , including high sensitivity , confident identification of breakpoints and in - frame fusions , and deeper coverage.10 three patients with predicted nonfunctional ntrk alterations also were identified in this study , which emphasizes the added value of ngs - based sequencing and attention to the breakpoints . 
although immunohistochemical assays for the detection of trk expression are in development , 21 allocation of an unstained slide for trk immunohistochemistry may be impractical given the need to test for a wide range of molecular alterations on often - limited tissue samples . 
similarly , given the seeming lack of concurrent canonical driver mutations in these patients , consideration of an initial dna - based ngs for mutational profiling may be reasonable , with reflex multiplexed fusion - targeted rna - based ngs in tumors that lack such a driver . 
however , sequential testing for possible gene alterations can delay the ultimate molecular diagnosis , may be problematic for small samples , and relies on mutual exclusivity of a kinase fusion and oncogenic driver mutation . 
therefore , we favor concurrent ngs - based mutational analysis with multiplexed ngs - based targeted rna sequencing for the identification of gene fusions in nsclc rather than sequential mutation testing or immunohistochemistry , which consumes more time and tissue . 
ou , mari mino - kenudson research funding : pharmamar ( inst ) , abbvie ( inst ) , bristol - myers squibb ( inst ) , merck ( inst ) , loxo oncology ( inst ) , ignyta ( inst ) travel , accommodations , expenses : pharmamar , abbvie , stemcentrx martin s . 
doebele stock and other ownership interests : rain therapeutics honoraria : pfizer , astrazeneca , ariad pharmaceuticals , guardant health , takeda pharmaceuticals , spectrum pharmaceuticals , trovagene consulting or advisory role : pfizer , oncomed pharmaceuticals , trovagene , ignyta , greenpeptide , astrazeneca patents , royalties , other intellectual property : licensing fees from abbott molecular for patent pct / us2013 / 057495 , licensing fees from ignyta for biologic materials ( inst ) travel , accommodations , expenses : ignyta , ariad pharmaceuticals , guardant health provision of study materials or patients : anna f . 
le stock and other ownership interests : archerdx speakers bureau : astrazeneca , roche , genentech , takeda pharmaceuticals travel , accommodations , expenses : astrazeneca , roche , genentech , takeda pharmaceuticals , tp therapeutics shivaani kummar consulting or advisory role : corvus pharmaceuticals , medtree ( i ) , nodus therapeutics research funding : bristol - myers squibb ( inst ) , dynavax technologies ( inst ) , pfizer ( inst ) , loxo oncology ( inst ) , corvus pharmaceuticals ( inst ) , plexxikon ( inst ) , jounce therapeutics ( inst ) , adc therapeutics ( inst ) , advenchen laboratories ( inst ) alexander i . 
spira research funding : roche ( inst ) , astrazeneca ( inst ) , boehringer ingelheim ( inst ) , astellas pharma ( inst ) , medimmune ( inst ) , novartis ( inst ) , newlink genetics ( inst ) , incyte ( inst ) , abbvie ( inst ) , ignyta ( inst ) , lam therapeutics ( inst ) , trovagene ( inst ) , takeda pharmaceuticals ( inst ) , macrogenics ( inst ) , cytomx therapeutics ( inst ) theresa a . 
haura consulting or advisory role : bristol - myers squibb , janssen pharmaceuticals research funding : eli lilly , ignyta , janssen pharmaceuticals , boehringer ingelheim , forma therapeutics patents , royalties , other intellectual property : patent pending on proximity ligation assay technology related to kinase inhibitor sensitivity biomarkers travel , accommodations , expenses : bristol - myers squibb , roche maria e . 
aisner honoraria : astrazeneca , clovis oncology consulting or advisory role : inivata , abbvie , bristolmyers squibb research funding : genentech ( inst ) , roche ( inst ) patents , royalties , other intellectual property : patent pending for pneumatic cell collection device travel , accommodations , expenses : seracare life sciences nora k . 
horick no relationship to disclose consulting or advisory role : archerdx patents , royalties , other intellectual property : coinventor of the anchored multiplex pcr technology , which is licensed to archerdx and receive royalty payments for this patent travel , accommodations , expenses : archerdx a . 
john iafrate stock and other ownership interests : archerdx consulting or advisory role : debiopharm group , chugai pharmaceutical , roche research funding : blueprint medicines patents , royalties , other intellectual property : archerdx exclusive license to amp technology sai - hong i . 
ou stock and other ownership interests : tp therapeutics honoraria : pfizer , roche , genentech , ariad pharmaceuticals , takeda pharmaceuticals , novartis , astrazeneca , foundation medicine consulting or advisory role : pfizer , roche , genentech , novartis , astrazeneca , takeda pharmaceuticals , foundation medicine , tp therapeutics , ignyta speakers bureau : genentech , astrazeneca , takeda pharmaceuticals research funding : pfizer ( inst ) , roche ( inst ) , astrazeneca ( inst ) , medimmune ( inst ) , clovis oncology ( inst ) , ariad pharmaceuticals ( inst ) , ignyta ( inst ) , peregrine pharmaceuticals ( inst ) , glaxosmithkline ( inst ) , astellas pharma ( inst ) , chugai pharmaceutical ( inst ) alice t . 
shaw at , yeap by , mino - kenudson m , et al : clinical features and outcome of patients with nonsmall - cell lung cancer who harbor eml4 - alk . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multitargeted pan - trk , ros1 , and alk inhibitor entrectinib : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
weiss gj , hoff br , whitehead rp , et al : evaluation and comparison of two commercially available targeted next - generation sequencing platforms to assist oncology decision making . 
rekhtman n , pietanza mc , hellmann md , et al : next - generation sequencing of pulmonary large cell neuroendocrine carcinoma reveals small cell carcinoma - like and non - small cell carcinoma - like subsets . 
ardini e , bosotti r , borgia al , et al : the tpm3 - ntrk1 rearrangement is a recurring event in colorectal carcinoma and is associated with tumor sensitivity to trka kinase inhibition . 
gainor jf , varghese am , ou sh , et al : alk rearrangements are mutually exclusive with mutations in egfr or kras : an analysis of 1 , 683 patients with non - small cell lung cancer . 
gautschi o , milia j , filleron t , et al : targeting ret in patients with ret - rearranged lung cancers : results from the global , multicenter ret registry . 
hyman dm , laetsch tw , kummar s , et al : the efficacy of larotrectinib ( loxo - 101 ) , a selective tropomyosin receptor kinase ( trk ) inhibitor , in adult and pediatric trk fusion cancers . 
 therapy - related erythroleukemia in a man with metastatic ewing sarcoma : a clinical role for advanced molecular diagnostics introduction therapy - related leukemia may be challenging to diagnose when a patient has cytopenia during treatment of another malignancy , particularly when there are few circulating leukemia cells . 
 here , we report a case of a 55 - year - old man with refractory ewing sarcoma who presented with thrombocytopenia and tumor lysis syndrome ( tls ) ; he was found to have pure erythroid leukemia ( pel ) , likely resulting from prior alkylating agent and / or topoisomerase ii inhibitor chemotherapy . 
furthermore , when patients with metastatic solid tumor have cytopenia , they may not undergo bone marrow ( bm ) evaluation if the cytopenia has already been attributed to therapies or the prior malignancy . in this case , initial diagnostics and the poorly differentiated morphology seen in the bm biopsy specimen did not readily distinguish between ewing sarcoma and acute leukemia . 
he was diagnosed with ewing sarcoma in 2011 , after a known right - side lower - lobe lung mass demonstrated increased size and malignant radiologic features on computed tomography ( ct ) imaging . 
the patient underwent right - side lower lobectomy and metastasectomy of bilateral pectoral lesions , radiation ( xrt ) to his rib , and additional chemotherapy with dactinomycin , vincristine , and cyclophosphamide , followed by xrt to his pectoral surgical bed . 
he started a trial of olaparib and temozolomide in august 2015 , which continued until october 2016 , when he was removed from protocol after ct imaging showed disease progression . 
cumulatively , he received 31 cycles of chemotherapy and four treatments of xrt . one month after stopping therapy , the patient presented with fatigue , dyspnea , fevers , bruising , and petechial rash , with no hepatosplenomegaly . 
peripheral smear revealed left - shifted myeloid cells and large basophilic cells with vacuolated cytoplasm ; these cells constituted 9% of blood leukocytes and were interpreted as either reactive atypical lymphocytes , circulating ewing sarcoma cells , or circulating blasts . 
zmynd8 exons 1 through 22 fuse with rela exons 3 through 11 to form the fusion gene zmynd8 - rela , which has been described in erythroleukemia.2 zmynd8 exons 1 - 22 zmynd8 - rela fusion chromosome 20 exons 3 - 11 rela chromosome 11 cbc counts at the ewing sarcoma diagnosis in 2011 were unavailable , cbc counts in 2013 were normal ( wbc , 4.9 103 / l ; hemoglobin , 14.0 g / dl ; platelets , 207 103 / l )  . he underwent bm biopsy and aspiration , and began treatment of tls with rasburicase , allopurinol , and normal saline . 
however , treatment was complicated by persistent cytopenia and hallucinations , likely related to ifosfamide . the bm biopsy specimen was hypercellular and revealed replacement by primitive , discohesive cells , which , by flow cytometry , were negative for cd45 , cd34 , myeloperoxidase , cd13 , and cd56 . 
by immunohistochemistry , cells were negative for cytokeratin , cd43 , and cd56 , but were positive for cd99 ( present in up to 98% of ewing sarcoma but also expressed in other cancers , including leukemia ) .3 - 6 preliminary bm karyotype identified an 11q13 abnormality , but no ewsr1 rearrangement . 
interphase fluorescent in situ hybridization study also did not reveal ewsr1 rearrangement . molecular testing was performed via heme snapshot assay , an institutional ngs platform using illumina truseq amplicon technology ( san diego , ca ) for single nucleotide variant and insertion / deletion detection in genomic dna.7 snapshot results are descriptive and cannot determine clonality , tumor - stromal percentage , or percentage of cells carrying mutations . 
 analysis was undertaken using a sequencing library generated with an oligo pool focusing on approximately 141 kb of genomic content consisting of 568 amplicons covering 15 full genes and exonic hotspots in 39 genes ( trusight myeloid sequencing panel ; illumina )  . testing identified three tp53 mutations with the following allelic frequencies : r337p , 38% ; i255f , 38% ; and y220c , 10% . 
these findings confirmed diagnosis of therapy - related pel , rather than progressive ewing sarcoma . the patient transiently improved after ifosfamide / etoposide treatment , but the leukemia ultimately progressed , at which point he opted for comfort care . 
he died 2 months after pel diagnosis . methods this anchored multiplex fusion assay is an ngs method that amplifies small amounts of nucleic acid and detects fusions without targeting specific rearrangements . 
two heme - nested pcr reactions are then performed to create a fully functional sequencing library targeting specific genes and exons ( fusionplex solid tumor kit ; archerdx , boulder , co )  . 
illumina misequation 2 147 base pairend sequencing results are aligned to the hg19 human genome reference , and a laboratory - developed algorithm is used for fusion transcript detection and annotation . 
the resulting product can then be processed for illumina or ion torrent ( thermo fisher scientific , waltham , ma ) sequencing.10 discussion this case highlights how the evolving field of molecular genetic diagnostics can help distinguish specific cancer diagnoses . 
advanced molecular testing using ngs and an rna - based solid fusion assay ultimately clarified this patients diagnosis . ewing sarcoma describes a family of cancers with fusion oncogenes involving the ewsr1 gene.13 there is a high correlation between bony metastases and bm involvement , and , to our knowledge , pel has not been described in refractory ewing sarcoma before this case report.14 - 17 therapy - related leukemia is a rare adverse effect of alkylating agents , radiotherapy , and topoisomerase ii inhibitors . 
tumor cells were positive for e - cadherin and cd71 ( not shown )  . erythroid precursors with 30% proerythroblasts.22 patients typically present with sequelae of pancytopenia from erythroid precursor proliferation . pel also has a very complex karyotype compared with other leukemias and can be difficult to diagnose , given its negativity for other markers typically expressed in aml , such as cd45 , cd13 , myeloperoxidase , and cd34.20 , 22 , 23 cd45 is commonly used to screen for hematologic neoplasms on initial pathologic staining . 
 ( megakaryoblastic anemia is another cd45 - negative leukemia . ) e - cadherin , expressed in most pel cases , helped lead us toward the correct diagnosis , as did demonstration of the rare zmynd8 - rela fusion . 
the latter is hypothesized to promote oncogenesis via constitutive nf - b activation.1 by definition , aml after exposure to cytotoxic chemotherapy or radiation is therapy - related aml , of which there are two primary etiologic subtypes : alkylating agent / radiotherapyrelated type and topoisomerase ii inhibitorrelated type.24 , 25 alkylating agents and radiotherapy exhibit dose - dependent risk of disease effected via centromeric breakage and partial or complete chromosome loss , particularly at chromosomes 5 and 7 . 
the leukemia had several balanced translocations , including t ( 11 ; 20 ) ( q12 ; q13.1 ) , and a partial deletion of chromosome 4 . mutations in tp53 , as seen in this case , are common in t - aml . 
interestingly , recent data suggest that tp53 - mutated clones may exist before the exposure to chemotherapy and expand under the selective pressure of treatment of another malignancy.27 this is the first reported case of greater than two tp53 mutations in t - aml.9 , 27 regardless of the inciting agents , t - aml is associated with dismal outcomes , such as were experienced by this patient . in patients with advanced cancers treated with alkylating agents , radiotherapy , or topoisomerase ii inhibitors , t - aml should be considered as a cause of refractory cytopenia . 
angelini df , ottone t , guerrera g , et al : a leukemia - associated cd34 / cd123 / cd25 / cd99 + immunophenotype identifies flt3 - mutated clones in acute myeloid leukemia . 
dias - santagata d , akhavanfard s , david ss , et al : rapid targeted mutational analysis of human tumours : a clinical platform to guide personalized cancer medicine . 
ok cy , patel kp , garcia - manero g , et al : tp53 mutation characteristics in therapy - related myelodysplastic syndromes and acute myeloid leukemia is similar to de novo diseases . 
green dc , deharvengt sj , de abreu fb , et al : use of anchored multiplex pcr enrichment for detection of gene fusions in solid tumors by next generation sequencing . 
thiel u , wawer a , von luettichau i , et al : bone marrow involvement identifies a subgroup of advanced ewing sarcoma patients with fatal outcome irrespective of therapy in contrast to curable patients with multiple bone metastases but unaffected marrow . 
cuneo a , van orshoven a , michaux jl , et al : morphologic , immunologic and cytogenetic studies in erythroleukaemia : evidence for multilineage involvement and identification of two distinct cytogenetic - clinicopathological types . 
kasyan a , medeiros lj , zuo z , et al : acute erythroid leukemia as defined in the world health organization classification is a rare and pathogenetically heterogeneous disease . 
olney hj , mitelman f , johansson b , et al : unique balanced chromosome abnormalities in treatment - related myelodysplastic syndromes and acute myeloid leukemia : report from an international workshop . 
mcgowan , phd1 , 2 purpose although analyzing germline and tumor samples concurrently provides the best opportunity for differentiating between germline and somatic mutations , tumor - only sequencing is becoming increasingly common in clinical care . 
with limited professional society guidance on how to manage pathogenic mutations identied via tumor - only sequencing , this study contemplates the professional knowledge and skills necessary to have represented on an mgtb to interpret these results in context of potential germline ndings . methods qualitative interviews with mgtb members and an ethnographic case study of a breast cancer mgtb at a national cancer institute cancer center were examined . results this mgtb discussed 34 cases of women with advanced - stage breast cancer over 13 months . interviews and observations of mgtb meetings indicated that members of the mgtb contemplated whether variants were germline or somatic and potential for identication of germline cancer predisposition . 
however , the mgtb only referred 11 patients ( 61% ) for additional germline testing , and the remaining seven patients ( 39% ) were not referred , raising questions about the kind of genomic expertise needed on an mgtb to optimize results interpretation and referrals . conclusion to ensure adequate interpretation , recommendation , and communication of tumor sequencing results , an mgtb should include professionals with knowledge and experience in clinical translation of tumor sequencing , testing methodology , molecular pathology , cancer biology , genomic pathways , germline variant interpretation , evaluation of family history , and application of professional recommendations for germline testing after tumor - only sequencing . 
 fishler et al context key objective : how are tumor - only sequencing results interpreted by a multidisciplinary genomic tumor board ( mgtb ) ? which professional expertise ought to be represented when discussing these results and recommendations ? knowledge generated : commercial laboratories provision of tumor - only sequencing without germline reference samples can complicate the ability of an mgtb to interpret patients genomic sequencing results and make recommendations for targeted treatment and referrals for additional genetic testing . 
providers on an mgtb questioned whether a known or likely pathogenic tumor sequencing variant was germline or somatic , sometimes overlooked known / likely pathogenic mutations in cancer susceptibility genes other than brca1 / 2 , and recognized the necessity of varied professional expertise when interpreting tumor - only sequencing results . relevance : to ensure appropriate interpretation of tumor - only sequencing and identication of patients who ought to be referred to genetics , an mgtb should include individuals with expertise in clinical translation of tumor sequencing , testing methodology , molecular pathology , cancer biology and genomic pathways , germline variant interpretation , evaluation of personal and family history , and application of professional guidelines for germline testing . 
to mitigate provider deliberation and genomic knowledge necessary to determine if additional germline testing is necessary , genetics professional societies and clinical laboratories ought to consider whether tumor - only sequencing should be routinely paired with germline samples to facilitate standardized reporting of germline variants . the basis of tumor - only sequencing results , even when combined with their family history . a previously published study from a breast cancer mgtb revealed that decisions about which patients received genetics referrals were not standardized.10 this prior analysis did not explore the factors the mgtb used to determine which patients received genetics referrals after tumor - only sequencing . 
our study aimed to identify these factors and to explore which professionals ought to be involved on an mgtb to ensure adequate interpretation , clinical application , and referral for additional germline testing when appropriate . each interview ranged in length from 25 to 49 minutes . 
all mgtb members signed a written informed consent , which allowed for recording , transcription , and analysis of the meeting minutes and interview data . data were collected using standard qualitative research including ethnography and in - depth inmethods , interviews and mgtb meetings were audio terviews . recorded and transcribed verbatim by a medical transcriptionist . 
participants in this study included 22 members of a breast cancer mgtb at one urban national cancer institute cancer center . methods included an ethnographic case study of mgtb meetings and interviews with mgtb members . 
this group met monthly from october 2013 to november 2014 to discuss results of tumor - only sequencing ordered for patients with advanced - stage breast cancer in a clinical setting . mgtb members were invited to participate in a semistructured interview regarding their opinions about a tumor board approach to interpreting tumor sequencing results . in total , 12 members of the board were interviewed by the research team , including treating physicians ( n = 6 ) , bioinformaticians ( n = 3 ) , a pathologist ( n = 1 ) , a medical geneticist ( n = 1 ) , and an administrator ( n = 1 ) .10 all patients discussed by this mgtb were women with advanced - stage breast cancer and tumor - only sequencing performed as part of their clinical care ( n = 34 )  . 
the mgtb discussed all of the hospitals patients with breast cancer who underwent tumor sequencing during the study period . all patient samples were sent to the same commercial laboratory for sequencing and analysis . the laboratory - generated tumor sequencing report suggested on - label / off - label treatments and clinical trial options on the basis of known / likely pathogenic mutations . pathogenic and likely pathogenic results were listed separately from vus results . 
as published in the preliminary analysis , mgtb recommendations included genetics referrals for suspected germline variants , clinical trial recommendations , us food and drug administrationapproved on - label therapies , androgen receptor testing , and repeat human epidermal growth factor receptor 2 testing . 
 underlying germline variants in tumor - only sequencing leaderships commitment to adherence with evidencebased medicine and bioethical principles of benecence and nonmalecence.10 of the 34 patients tumor sequencing results that the mgtb reviewed during the study period , 18 patients met nccn criteria for additional germline testing on the basis of their personal history , including type of breast cancer , age of onset , and / or the identication of a known / likely pathogenic tumor mutation in a cancer susceptibility gene . 
the remaining seven patients ( 39% ) represent missed opportunities for additional germline testing on the basis of the patients personal history , prior germline testing , and / or tumor - only sequencing result ( table 2 )  . 
five of these patients were missed on the basis of a combination of these factors ; two were missed on the basis of personal history alone . through analysis of mgtb member interview transcripts and mgtb meetings , three themes emerged : provider confusion about whether a variant identied by tumoronly sequencing was germline or somatic , potential for tumor - sequencing identication of germline cancer predisposition , and genetics expertise necessary for inclusion on an mgtb . provider confusion about whether a mutation was germline or somatic one key question raised by mgtb members was whether the variants listed on tumor sequencing reports were germline or somatic . 
on the basis of the way mgtb members managed the referral process , it became apparent that they disagreed about their role as evaluators of tumor - only sequencing results , including determining whether follow - up with additional germline testing was necessary . 
for example , one medical oncologist mentioned that all mutations relevant treatment were listed on the rst page of the patients report and that if we dont have a lot of time , we may not ip through the rest to see what else might be listed there . in contrast , another oncologist advocated for a more active interpretation : we cant role in report take what [ commercial vendor ] recommends as gospel truth and say okay , this is what were going to go with , because they recommended itthe interpretation needs to happen from our end . just result in addition to differing perspectives about terpretation , there was confusion among the mgtb members regarding whether the reported mutations were somatic or germline . 
a discussion about a patient with a reported mutation in fancc highlights this confusion , which affected their thoughts about whether the patient should receive a genetics referral ( table 3 )  . 
of times reason was discussed during the mgtb meetings patient referrals for additional germline testing on the basis of personal history triple - negative cancer and age of diagnoses , 60 years diagnosis of bilateral breast cancer on the basis of results of tumor - only sequencing report for parp inhibitors identication of known / likely pathogenic fancc mutation identication of known / likely pathogenic chek2 mutation identication of known / likely pathogenic mlh1 mutation identication of known / likely pathogenic nf1 mutation identication of known / likely pathogenic mutation or vus in brca1 / 2 to determine eligibility on the basis of personal history and of tumor - only sequencing report re - evaluation of brca1 / 2 status for parp inhibitors because of prior negative germline results and negative tumor sequencing results for brca1 / 2 identication of known / likely pathogenic tp53 mutation on tumor sequencing and age of diagnoses note . 
missed opportunities for referral for additional germline testing ( n = 7 ) fishler et al missed opportunity on the basis of personal history on the basis of tumor - only sequencing report identication of known / likely pathogenic pten variant on the basis of personal history and tumor - only sequencing report triple - negative breast cancer , rst breast cancer diagnoses , 60 years , and no prior germline genetic testing personal diagnosis of lobular breast cancer and identication of known / likely pathogenic cdh1 variant on the basis of previous genetic test results and tumor - only sequencing report negative brca1 / 2 germline testing before availability of bart testing , no mutation in brca1 / 2 gene identied on tumor negative brca1 / 2 germline testing before availability of bart testing , pten mutation identied on tumor sequencing sequencing total no . 
the tumor - only report does not distinguish variants that are reported pathogenic from variants that are reported likely pathogenic . they are reported as one category on the front page of the report . 
seven patients out of 18 discussed at the mgtb did not receive a genetics referral for additional germline testing , although it would have been indicated by nccn criteria or a known / likely pathogenic mutation identied in a cancer susceptibility gene by tumor - only sequencing . 
at the time of the study of this mgtb , nccn criteria recommended that patients with negative brca1 / 2 sequencing before 2006 have bart testing and women with triple - negative breast cancer and their rst breast cancer diagnoses before age 60 years have brca1 / 2 germline testing . 
in addition , the american college of medical genetics and genomics recommended that pathogenic germline mutations associated with hereditary cancer syndromes be returned to patients ( such as pten and cdh1 )  . abbreviations : bart , brac analysis rearrangement test ; mgtb , multidisciplinary genomic tumor board ; nccn , national comprehensive cancer network . testing , some of the medical oncologists were reluctant , because the gene was not directly related to hereditary breast and ovarian cancer syndrome . 
mgtb interviewees indicated lack of education regarding medical genetics as a limitation of the mgtb , which is a recognized barrier to autonomous use of genetic testing by ordering physicians.2 , 12 potential for identication of germline cancer predisposition consistent with the mgtbs focus on identifying treatment options , 10 members of this mgtb were most concerned about whether a patient had a brca1 / 2 mutation to determine their eligibility for treatment with poly ( adp - ribose ) table 3 . 
vignette : confusion about somatic versus germline mutations vignette medical oncologist 7 : it says in the report that germline mutations in fancc cause fanconi anemia , a clinical heterogeneous disorder , and that appropriate clinical testing [ to detect ] the presence of a germline mutation is recommended . 
whenever we see a mutation , we have to make sure that we realize its one test and we would need it to be validated , but does it have relevance for treatment ? ( talking about prior treatment responses and discussion about parp inhibitor recommendations ) medical oncologist 7 : and she was germline brca tested and all thats negative ? medical oncologist 1 : yeah , she was brca negative . medical oncologist 2 : should we refer to genetics about this fancc thing ? medical oncologist 1 : you think we should refer ? is there a reason to think about it ? medical oncologist 7 : the only way you can test it is on those panels . 
every genetics has a panel where you can test for fanconi anemia genesi dont know how much breast cancer risk or other risks [ are associated with variants in this gene ]  . 
 underlying germline variants in tumor - only sequencing polymerase inhibitors , which gained traction as a mutationguided treatment option during the study period.13 , 14 thus , all patients with tumor - only sequencing results that included a vus or known / likely pathogenic mutation in brca1 / 2 were referred to genetics ( n = 4 )  . patients with known / likely pathogenic mutations in other cancer susceptibility genes ( such as pten ) were not routinely referred to genetics ( table 2 )  . 
at the time of this study , american college of medical genetics and genomics recommended that when analyzing a tumor and paired germline sample , such results should be conrmed and communicated to patients as secondary ndings , because of their association with a hereditary cancer syndrome . however , nccn guidelines did not include a recommendation for additional germline testing for mutations in genes on the secondary ndings list , 7 which may have contributed to inconsistent referral patterns , especially given that the mgtb was reviewing tumor - only sequencing results . two additional patients who met nccn guidelines for germline testing on the basis of their personal history were not referred for germline testing ( table 2 )  . 
at the time of the study of this mgtb , nccn recommended bart ( brac analysis rearrangement test ) testing for patients who had received negative brca1 / 2 germline test results before 2006.7 two patients with negative brca1 / 2 tumor - only sequencing results and negative brca1 / 2 germline test results before the availability of bart testing were not referred to genetics , although a genetics referral would have been indicated by nccn guidelines . 
in discussing how well individual disciplines were represented on the mgtb , a medical oncologist who co - led the mgtb recognized the value of genetics expertise in interpreting whether certain mutations were common or rare and how to manage referrals on the basis of a variants likelihood of being germline . 
explicitly , she noted that knowledge and experience with specic gene pathways enhanced the variant interpretation and productivity of the discussions about treatment options and result interpretation during the mgtb meetings . 
she also described disappointment that a medical geneticist and genetic counselors were invited , but that a medical geneticist only attended one mgtb meeting over the 13 - month study period and no genetic counselors participated . 
however , the other medical oncologist who co - led the mgtb mentioned that scheduling posed a barrier to genetic counselors attendance . mgtb members discussed the limitations of the test throughout the entire study period . 
the pathologist cautioned during her interview that not all providers who order tumor - only sequencing may understand the limitations of the test in terms of identifying germline variants : its hard to speak for other doctors , other community doctors . 
furthermore , at one meeting , the medical geneticist explained sequencing methodology , utility of bart testing for patients who have previously tested negative for brca1 / 2 , and guidelines for germline testing on the basis of a patients personal history , including age and triple - negative diagnosis . 
this information shifted the conversation from discussion of clinical trial options for a patient with triple - negative breast cancer who previously tested negative for mutations in brca1 / 2 to clarication of other germline testing options including bart testing , in accordance with nccn recommendations.7 during his interview , the medical geneticist stressed the value of genetics professionals who can address psychosocial concerns with patients during result return when a germline mutation is suspected . 
he noted that this skill was outside of his scope of practice and was one of the most difcult parts of result return . discussion for patients discussed by this mgtb , tumor sequencing was performed as part of clinical care . 
members of this mgtb , including medical oncologists , questioned whether the results of tumor sequencing were somatic or germline and queried what resources were available to them to clarify this information . 
the medical geneticist was the only mgtb member who was board certied in medical genetics . however , he was not present at the majority of mgtb meetings to provide clarication regarding whether a patient discussed on the mgtb should receive additional germline genetic testing . 
other mgtb members without medical genetics board certication may have qualied as a commission on cancer ( coc ) dened genetics professional by providing cancer risk assessment on a regular basis.15 ( p51 ) a key question that emerged through this analysis is whether these criteria are sufcient to ensure optimal implementation and interpretation of tumor sequencing by an mgtb and how best to support clinicians as they move into using new genomic technologies in their practices . nccn currently recommends genetic risk evaluation for patients with a known / likely pathogenic variant identied in a cancer susceptibility gene via tumor sequencing . 
perceived value of types genetics expertise on an mgtb perceived value by mgtb members member illustrative quote medical oncologists identication of clinical trials evaluation of treatment options medical oncologist : i can look and see if that [ three prior investigational studies ] will exclude her from [ clinical trials ] in the area , but that would sort of be my preference would be to put her on the phase i while looking for regional studies , and ill contact [ name ] and look on clinicaltrials.gov. 
and i guess were not recommending treatment off study with one of these m2r inhibitors ? basic scientists evaluation of functional studies radiation oncologist : someone who has more expertise in the basic science stuffwith better knowledge about genomic pathways understanding of mechanisms of the different mutations and how that may or may not translate into something that the drug might actually work for . medical evaluation of testing geneticists methodology variant classication genetic evaluation of family history counselors variant classication psychosocial counseling during result return medical geneticist : it is still not clear using next - generation sequencing whether a negative result is [ a true negative ] , because you have to look at the coverage across each position and the number of reads theyre reporting . 
second , rearrangements can be missed , so wed want to have her get bartshe should get the [ germline ] testingjust given her age of diagnosis and the fact that its triple - negative . medical geneticist : the most challenging patient encounters ive had is telling a mom that shes passed [ the mutation ] along to her daughter , and having the daughter understand that her mom just passed along a gene that basically assures her that shell get breast cancer in her lifebut it is very challenging , the psychosocial aspect . abbreviations : bart , brac analysis rearrangement test ; mgtb , multidisciplinary genomic tumor board . family history to determine whether people with known / likely pathogenic mutations in cancer susceptibility genes should receive additional germline testing . 
when clinical sequencing laboratories do not compare variants identied in a tumor sample with a germline sample , ordering providers are responsible for lling this gap in professional recommendations by recognizing when clinical germline testing is indicated on the basis of the combination of personal history , tumor sequencing results , and family history . currently , there are no guidelines or recommendations for which professionals or types of genomic expertise should be included by an mgtb to ensure adequate interpretation , recommendation , and communication of genomic test results . 
the coc denes certain roles within a cancer center and provides guidelines for the frequency and format of multidisciplinary tumor boards.15 however , it does not dene what disciplines should be included to constitute an mgtb , nor does it specify guidelines for tumor boards that evaluate tumor - only sequencing . 
the coc denes a genetics professional in a cancer center as someone who provides cancer risk assessment on a regular basis15 ( p51 )  . although multiple clinicians on this mgtb may have met this coc denition , many expressed confusion regarding benets and limitations of genetic testing and genetic risk assessment as well as knowledge deciencies surrounding testing methodology and result interpretation . 
this suggests that the genetics expertise pertinent for interpreting tumor - only sequencing results may be partial or unevenly distributed among those who were tapped to lend their expertise to an mgtb . on the basis of the results of this single - site case study , when considering how denitions of a genetic professional may be applied to mgtbs , providing cancer risk assessment on a regular basis is insufcient for conferring expertise for implementing tumor sequencing in clinical care . to ensure appropriate interpretation of tumor sequencing and identication of patients who ought to be referred to genetics , an mgtb should include individuals with expertise in clinical translation of tumor sequencing , testing methodology , molecular pathology , cancer biology and genomic pathways , germline variant interpretation , evaluation of personal and family history , and application of professional guidelines for germline testing . 
 underlying germline variants in tumor - only sequencing societies and organizations and clinical laboratories ought to consider whether tumor - only sequencing should be routinely paired with germline samples to facilitate standardized reporting of germline variants . given that the mgtb under study was primarily focused on treatment and clinical trial recommendations on the basis of results of tumor sequencing , it may not have been the optimal setting to discuss a patients personal history , including prior genetic testing and / or potentially pathogenic variants in cancer susceptibility genes lacking treatment implications . 
however , to ensure comprehensive referrals for additional germline sequencing after tumor - only sequencing , ordering providers ought to interpret the patients personal history in combination with their tumor - only sequencing results , as discussed by the mgtb . 
for two patients with negative brca1 / 2 tumor - only sequencing results and negative brca1 / 2 germline testing before the availability of bart testing , negative brca1 / 2 tumor - only sequencing results may have been falsely reassuring for these providers , especially considering the possibility that other cancer susceptibility genes may have been responsible for the cause of their cancer . is possible that provider deliberation about whether certain patients should be referred to genetics on the basis of these factors , not specic to the purpose of convening the mgtb the mgtb , may have occurred outside of meetings and would not have been captured by this analysis . 
in a climate where there is a paucity of genetic counselors and medical geneticists , creative strategies for engaging genetics professionals formally and informally in mgtb deliberations should be considered to optimize interpretation of tumor sequencing results . 
this study was limited by the information discussed as part of the mgtb meetings focused on patients with advanced breast cancer and interviews with mgtb members at a single national cancer institutedesignated cancer center . 
thus , possible that there were additional patients with known / likely pathogenic variants in genes associated with an inherited cancer predisposition syndrome that were not captured by this analysis , or that geneticists or genetic counselors may have been consulted about interpretation of laboratory reports outside of the mgtb context . 
fishler research funding : illumina ( inst ) lauren walters - sen employment : invitae stock and other ownership interests : invitae consulting or advisory role : ischemia care no other potential conicts of interest were reported . acknowledgment we thank roselle ponsaran , tracie baker , rebecca sisson , and the multidisciplinary genomic tumor board members for their time and contribution to this study . 
 fishler et al references schwaederle m , parker ba , schwab rb , et al : molecular tumor board : the university of california - san diego moores cancer center experience . 
oncologist 19 : 631 - 636 , 2014 tafe lj , gorlov ip , de abreu fb , et al : implementation of a molecular tumor board : the impact on treatment decisions for 35 patients evaluated at dartmouthhitchcock medical center . 
ann oncol 27 : 795 - 800 , 2016 jones s , anagnostou v , lytle k , et al : personalized genomic analyses for cancer mutation discovery and interpretation . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
mcgowan ml , ponsaran rs , silverman p , et al : a rising tide lifts all boats : establishing a multidisciplinary genomic tumor board for breast cancer patients with advanced disease . 
catenacci dv , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 13 . 
 next - generation rapid autopsies enable tumor evolution tracking and generation of preclinical models purpose patients with cancer who graciously consent for autopsy represent an invaluable resource for the study of cancer biology . 
to advance the study of tumor evolution , metastases , and resistance to treatment , we developed a next - generation rapid autopsy program integrated within a broader precision medicine clinical trial that interrogates preand postmortem tissue samples for patients of all ages and cancer types . materials and methods one hundred twenty - three ( 22% ) of 554 patients who consented to the clinical trial also consented for rapid autopsy . 
this report comprises the first 15 autopsies , including patients with metastatic carcinoma ( n = 10 ) , melanoma ( n = 1 ) , and glioma ( n = 4 )  . whole - exome sequencing ( wes ) was performed on frozen autopsy tumor samples from multiple anatomic sites and on non - neoplastic tissue . 
tissue was also used for the development of preclinical models , including tumor organoids and patient - derived xenografts . results three hundred forty - six frozen samples were procured in total . 
mutational profiles of primary tumors and metastases yielded candidate mediators of metastatic spread and organotropism including cul9 and pigm in metastatic ependymoma and ankrd52 in metastatic melanoma to the lung . 
rna - seq data identified novel gene fusion candidates . conclusion a next - generation sequencingbased autopsy program in conjunction with a premortem precision medicine pipeline for diverse tumors affords a valuable window into clonal evolution , metastasis , and alterations underlying treatment . 
the goal of the caryl and israel englander institute for precision medicine ( ipm ; new york , ny ) is to harness as much information as possible from an individual patients tumor tissue not only in an effort to benefit the patient during life , 1 but also to develop preclinical platforms2 and coclinical trials with the potential to benefit larger populations . 
an important arm of our precision medicine program permits postmortem tissue donation linked to robust downstream applications through a dedicated autopsy program . institutional rapid autopsy programs have been well described1 , 3 - 12 and have previously led to significant advances in cancer research in the areas of prostate , 1 , 3 , 4 , 6 , 7 , 11 pancreas , 10 breast , 8 and pediatric brain tumors.5 , 9 , 12 this program builds on prior autopsy programs by enrolling patients of all ages and cancer types , capturing samples throughout a patients disease course , and leveraging multiple parallel platforms to generate high - throughput sequencing data and robust preclinical tumor models . 
we highlight our initial experience with 15 patients who underwent rapid autopsy and emphasize the following three themes : capturing the molecular status of a diverse set of neoplasms at the end point in disease progression relative to ascopubs.org / journal / po jco precision oncology david j . 
at our institution , the generic hospital autopsy consent form must also be signed by the next of kthis institutional review boardapproved autopsy tissue donor program is based in part on protocols developed at the university of michigan by drs mark a . 
once the treating physician notifies a contact member of a patients death by pager , a robotic calling system is activated to alert the autopsy teaattending and resident autopsy pathologists , an autopsy technical assistant , and two to four members of the ipm laboratory are available at all times . 
total rna was prepared for rna sequencing ( rnaseq ) in accordance with the standard illumina mrna sample preparation protocol ( illumina )  . paired - end rna - seq at read lengths of 50 or 51 base pairs was performed with the hisequation 2000 ( illumina )  . 
tumor samples are represented in a phylogenetic tree as nodes with no children , whereas the internal nodes model inferred tumor cell populations on the basis of observed single nucleotide variants using the parsimony ratchet method.21 , 22 see data supplement for gene clonality assessment . rna - seq data analysis all reads were independently aligned with star_2.4.0f123 for sequence alignment against the human genome build hg19 , downloaded via the university of california santa cruz genome browser . 
for fusion analysis , we used star - fusion ( star - fusion_v0.5.1 ) , 24 , 25 fusioncatcher ( v0.99.3e ) , 26 and fusionseq.27 - 31 nucleic acid extraction dna extraction and whole - exome and wholegenome sequencing . 
sequencing is performed using illumina hisequation 2500 rapid run mode ( 23101bp ; illumina , san diego , ca )  . patient - derived , tumor organoid , and xenograft development platform as previously described , 2 fresh tumor tissue is dissociated before seeding cells into growth factor reduced matrigel ( corning , corning , ny )  . 
 with matrigel in the flanks of nu / nu nude mice ( charles rivers laboratories , wilmington , ma )  . were variably treated with prior surgery , radiation , and / or chemotherapeutic agents ( data supplement )  . results consent one hundred twenty - three ( 22% ) of 554 patients who consented to the clinical trial have also consented for rapid autopsy . 
of those patients for whom we have documented death in addition to premortem consent , we have performed autopsy on approximately 54% ( see materials and methods for details on consent )  . diversity of tumor types and metastatic sites the first 15 autopsies performed comprise a diverse set of neoplasms and metastatic sites ( fig 1 )  . primary tumors were available in 12 ( 80% ) of 15 patients from prior surgical resections and / or from recurrent or residual primary tumors obtained at autopsy . 
in patients with known metastatic disease before death , matched primary and metastatic tumor from individual patients was available in 10 ( 77% ) of 13 patients , and metastatic disease was collected at autopsy in 100% ( n = 13 ) of these patients . 
transport was successfully managed from up to 50 miles from our manhattanbased institution . this initial cohort yielded a total of 346 frozen aliquots over 131 distinctly annotated anatomic sites , of which 310 contained tumor upon histologic review of frozen sections ( fig 1b )  . 
one hundred thirteen distinct samples underwent whole - exome sequencing ( wes ) , including 82 frozen tumor and 10 frozen non - neoplastic control tissue samples obtained at autopsy , six samples derived from peripheral blood , and 15 formalin - fixed paraffinembedded or frozen samples from prior surgical procedures . 
in addition to wes , rnaseq was performed on a subset of samples ( n = 72 )  . data regarding rna concentration , rna integrity number values , 260 / 280 values , and 260 / 230 values over all rna samples are provided in the data supplement . 
despite transporting the patient from an outside institution , our pmi for this patient was only 2 hours , and the effort led to viable cell cultures . tumor clonal architecture and evolution autopsy material in combination with premortem surgical material is crucial to the study of the spatiotemporal evolution of cancer . 
in one illustrative patient ( wcm419 ) , a young girl with recurrent anaplastic ependymoma , material was available from eight distinct surgical resection procedures spanning more than 5 years in addition to material obtained at autopsy ( fig 2 )  . multiple sites of disease were available for study including the posterior fossa ( the primary site ) , metastatic lesions within the spinal cord , and a metastatic deposit involving the lateral ventricle obtained at autopsy ( figs 2a to 2c )  . 
histologic examination of all tumor material showed prominent perivascular pseudorosette formation ( fig 2d )  . wes was performed on formalin - fixed paraffinembedded material derived from prior surgical specimens as well as frozen autopsy tissue from two distinct sites ( figs 2e and 2f )  . 
reconstruction of the evolutionary tree of this tumor revealed a complex branching pattern where several mutations ( erbb3 , dnmt3a , brca1 , notch1 , and runx1t1 ) in the primary tumor samples were not shared at different time points ( 0 to 64 months ) or with descendent clones ( fig 2g )  . 
moreover , we identified two genes , cul9 and pigm , as harboring alterations specific to three or greater metastatic sites of disease and absent from all tissues resected from the primary site of disease . molecular features among multiple metastatic sites even in the absence of a definitive primary site , it is possible to gain insights into the evolutionary dynamics of tumor growth in distinct anatomic compartments . 
a case in point is wcm642 , a 50 - year - old male patient who presented with disseminated disease from a primary tumor of unknown origin ( fig 3 )  . 
prior biopsy demonstrated an epithelioid neoplasm without a definitive diagnosis . at autopsy , tumor was frozen from 15 distinctly annotated anatomic locations including adrenal gland and three distinct lobes of the lungs ( figs 3a and 3b ) , parietal pleura , omentum , lymph nodes ( three distinct sites ) , small intestine , large intestine , liver ( two distinct lobes ) , gallbladder , and pancreas . diagnosis of this tumor was only ascertained at autopsy . 
at autopsy , cells demonstrated both epithelioid and sarcomatoid morphology ( figs 3c and 3d ) and focal positive staining for s100 ( not shown ) , which had been negative in the biopsy . sequencing revealed mutations in nras and idh1 ( fig 3e ) and contributed to the final diagnosis of malignant melanoma . reconstruction of the clonal architecture of eight metastases from this patient demonstrated several mutations that were shared in all samples ( mllt4 , idh1 , aff3 , arid2 , ect2l , and nras ) , as well as mutations restricted to particular metastatic sites ( eg , apc in an lm and smad4 in lung ; fig 3f )  . remarkably , the branch points of the phylogenetic tree reflect the anatomic distribution of metastases , with those encompassing the digestive system grouped separately from those to the adrenal gland and lungs . 
 a wcm419 cul9 pigm runx1t1 notch1 brca1 dnmt3a erbb3 mutated wild type anaplastic ependymoma 1 - 5 : posterior fossa primary 6 : spinal thoracic met 7 : spinal thoracic met 8 : lateral ventricle met 9 : spinal met 10 : spinal met 9 10 runx1t1 shared in more than one sample but not all samples private primary private metastatic notch1 brca1 msh2 dnmt3a erbb3 spec id# months location pf , lv fig 2 . 
multiple sites of disease were available for study , including ( a and b ) the posterior fossa ( primary site ; [ a ] ventral surface of the whole brain with exophytic tumor component indicated by the arrow ; [ b ] metastatic deposits within the supratentorial compartment involving the lateral ventricle and subventricular brain parenchyma , and lesions within the spinal cord ( not shown ) , ( c ) axial cross - section through the pons and cerebellum )  . 
 ( f ) whole - exome sequencing was performed on prior surgical resection formalin - fixed paraffin - embedded specimens including primary tumor in posterior fossa ( samples 1 , 3 , 4 , and 5 ) and metastases to spinal cord ( samples 6 , 7 , 9 , and 10 ) , as well as on frozen autopsy tissue from two distinct sites , including recurrent primary tumor in the posterior fossa ( sample 2 ) and metastasis to the lateral ventricle ( sample 8 )  . 
both the color - coded bar on the right and the phylogenetic tree below indicate whether mutations are private to primary or private to metastases or shared in more than one sample . 
several mutations ( erbb3 , dnmt3a , brca1 , notch1 , and runx1t1 ) in the primary tumor samples are not shared either between them at different time points ( 0 to 64 months ) or with descendent clones . 
in particular , for both of these patients , genes were identified that showed consistent overexpression across metastatic tumors for each patient at the transcriptional level relative to the expression of these genes over a large set of rna - seq samples . 
for wcm772 , these data correlated with evidence of amplification of the met gene derived from wes , whereas for wcm0 , no such correlation was observed ( data supplement )  . additional rna - seq analysis of wcm0 samples identified novel gene fusion candidates such as znf526 - megf8 ( figs 4b to 4d )  . 
in addition , wgs on two lms from this patient yielded additional candidates , including the discovery of a gene fusion involving styk1 , a putative serine / threonine and tyrosine receptor protein kinase of potential clinical significance in castrate - resistant prostate cancer32 ( fig 5 )  . tumor organoid , pdx , and cell line development pdxs and cell lines are the most frequently used models in cancer research and anticancer drug screening . 
 a mutated wild type melanoma 1 : liver right met 2 : lung left upper lobe met 3 : lung left upper lobe met 4 : lung right upper lobe 5 : small intestine met 6 : large intestine met 7 : adrenal left met 8 : pancreas met shared in all samples shared in more than one sample but not all samples private metastatic wcm642 1 2 3 4 5 6 7 8 smad4 mllt4 idh1 aff3 arid2 ect2l nras mllt4 idh1 aff3 arid2 ect2l nras ankrd52 smad4 fig 3 . 
a 50 - year - old male patient presented with disseminated disease from primary tumor of unknown origa previous biopsy ( not shown ) showed an unclassified malignant and epithelioid neoplasm . at autopsy , tissue samples from 17 distinct anatomic locations were snap frozen , including ( a ) adrenal gland and ( b ) lung . 
both the colorcoded bar on the right and the phylogenetic tree below indicate whether mutations are private to any metastatic site or are shared in more than one sample or in all samples . 
few mutations are shared in more than one sample but not all samples ( eg , apc in right liver metastasis ( met ) ; smad4 in left upper lobe of lung )  . 
scale bars = ( a and b ) , 1 cm ; ( c and d ) , 50 mm . in vivo biologic processes and may provide a new avenue for personalized cancer care.33 , 34 as demonstrated in patient wcm331 , despite a delayed pmi of 6.5 hours as a result of transportation from an outside hospital , tumor organoid development of ovarian serous adenocarcinoma was achieved . 
viable organoids histologically comparable to metastatic autopsy tissue were produced and consistent with ovarian serous adenocarcinoma ( figs 6b to 6d )  . wes was performed on a metastatic omental lesion biopsied 2 years before autopsy , on several metastatic lesions obtained at autopsy , and on the tumor organoid material derived from a peritoneal nodule obtained at autopsy . 
reconstruction of the clonal architecture of metastatic samples and tumor organoid demonstrates that ptprb mutation is shared across all samples , whereas foxo1 mutation is present in one metastasis ( to small bowel serosa ) and the tumor organoid only . 
alterations restricted to the tumor organoid material only ( eg , prdm16 and kmt2a ) may reflect either additional tumor heterogeneity or alterations arising in vitro . another example of patient - derived preclinical model development from rapid autopsy tissue is illustrated in a patient with colon adenocarcinoma ( wcm715 ; fig 6g ) for whom both tumor organoid ( figs 6h and 6i ) and downstream pdx models ( fig 6j ) were established . 
 a lm1 coverage [ 0 93 ] lm1 junctions lm2 coverage [ 0 75 ] lm2 junctions pm1 coverage [ 0 48 ] pm1 junctions pm2 coverage [ 0 59 ] pm2 junctions t24 coverage [ 0 53 ] t24 junctions t5 coverage [ 0 85 ] t5 junctions t16 coverage [ 0 50 ] t16 junctions refseq cdkn2c cdkn2c cdkn2c cdkn2c cdkn2c wcm0 wcm772 [ 0 93 ] [ 0 75 ] [ 0 48 ] [ 0 59 ] [ 0 53 ] [ 0 85 ] [ 0 50 ] znf526 megf8 fig 4 . 
 ( a ) gene expression outlier analysis across 300 rna sequencing samples derived from a diversity of tumors within the institute for precision medicine cohort highlights wcm0 ( small - cell carcinoma of prostate ) and wcm772 ( pleomorphic carcinoma of lung ) , two patients who show cdkn2c and met as recurrent outliers in distinct anatomic samples , respectively . 
z scores were calculated for 70 druggable cancer genes , and outliers were selected at a cutoff of z score greater than 2.5 and fragments per kilobase million greater than 50 . 
 ( b ) rna sequencing analysis by fusioncatcher and fusionseq allows for the identification of novel gene fusion candidates . schematic of the fusion between znf526 and megf8 in wcm0 showing the connected exons . 
 a ybx3 chr12 styk1 lm1 coverage lm1 junctions lm2 coverage lm2 junctions pm1 coverage pm1 junctions pm2 coverage pm2 junctions t24 coverage t24 junctions t5 coverage t5 junctions t16 coverage t16 junctions refseq fig 5 . 
a 55 - year - old male patient status post prostatectomy presented with local recurrence , metastases in the pelvis and liver , and cushing syndrome in the month before death . 
overexpression of styk1 may serve as a potential molecular target in castrate - resistant prostate cancer.32 discussion tissue procurement from patients with cancer at autopsy and within the context of a pan - cancer precision medicine clinical trial captures biologic data at a state in disease progression that is rarely studied . 
in contrast to previously reported autopsy programs , we have incorporated data analysis and development of preclinical models using multiple platforms , 2 clinical - grade assays , 13 and computational algorithms , 13 , 35 , 36 leveraging the infrastructure of ipm . 
here , we illustrate a proof of principle in developing a powerful model for interrogating a diverse set of primary tumor types and metastatic sites , including newly generated tumor organoids , pdx models , and cell culture . 
indeed , with just the first 15 autopsies , we have revealed novel genetic candidates as potential mediators of metastatic spread in both ependymoma and melanoma , as well as provided the foundation for additional work investigating treatment effect in metastatic urothelial carcinoma . as a testament to our ability to track patients through their disease course , we analyzed primary tumor samples in 77% of patients for whom metastatic disease was procured at autopsy and in 80% of patients overall . 
 a wcm331 prdm16 kmt2a foxo1 ptprb foxo1 kmt2a prdm16 shared in all samples shared in more than one sample but not all samples private metastatic ptprb serous ovarian carcinoma 1 : omentum met 2 : diaphragm met 3 : small intestine met 4 : organoid from peritoneal met mutated wild type fig 6 . 
 ( d ) cytologic comparison of these tumor organoids with representative sections from metastatic autopsy tissue revealed morphologically similar cells ( diff - quik stain , 3400 original magnification )  . 
 ( e ) whole - exome sequencing was performed on formalin - fixed paraffin - embedded material derived from an omental metastasis biopsied 2 years before autopsy ( sample 1 ) , on frozen material from two metastases obtained at autopsy ( samples 2 and 3 ) , and on tumor organoid material derived from a peritoneal nodule obtained at autopsy ( sample 4 )  . 
both the color - coded bar on the right and the phylogenetic tree below indicate whether mutations are private to the metastatic sites or are shared in more than one sample or in all samples . 
 ( f ) in the absence of material from the primary tumor , partial reconstruction of the clonal evolution of metastatic samples ( including the tumor organoid as surrogate of one of the metastasis at autopsy ) demonstrates that ptprb mutation is shared in all samples and foxo1 mutation is present in two metastases . 
 ( g ) in case wcm715 , an he - stained section of a liver metastasis obtained at autopsy showed metastatic mucinous adenocarcinoma of the colon ( 3200 original magnification )  . 
 ( j ) he - stained section of patient - derived xenograft derived from organoid implantation in mouse demonstrates comparable histomorphology with original liver metastasis and derived tumor organoid ( 3200 original magnification )  . 
for example , analysis of wcm419 revealed alterations in cul9 and pigm that were present in most or all spatiotemporally distinct metastatic sites of ependymoma but absent from multiple resections at the primary site . 
 whereas pigm encodes a mannosyltransferase involved in glycosylphosphatidylinositol - anchor biosynthesis.38 in addition , we have identified gene candidates for further study that may mediate organotropism of metastases in melanoma ; for example , we found that ankrd52 mutations were restricted to lung metastases in a patient with widely metastatic melanoma . 
finally , additional work on two patients from within this cohort ( wcm117 and wcm259 ) has already yielded further insights into chemotherapy - resistant urothelial carcinoma , demonstrating enrichment in clonal alterations including targetable mutations ( eg , l1cam and integrin signaling pathways ) .21 comparison of wes between primary tumors , metastatic sites , and preclinical in vitro models of disease also enables an assessment of the extent to which critical molecular features of a tumor are reiterated , for example , in tumor organoids . 
the latter seem to recapitulate the patients metastatic disease at the exome level , representing an opportunity to develop coclinical trials and other clinically relevant applications ( discussed in additional detail by pauli et al39 )  . 
in addition , investigation of wgs and rna - seq data including gene expression outlier analysis across our precision medicine cohort has allowed the identification of novel gene fusions and overexpression of certain transcripts across metastatic sites with potential clinical relevance . we have set the foundation to investigate several critical questions over a diverse set of neoplasms , including the temporal evolution of tumors , the clonal evolution of tumors with respect to widely disseminated metastatic disease sites , and the production and examination of tumor organoid models derived from these specimens . 
robinson , alexandros sigaras , rema rao , bishoy faltas , rohan bareja , prajwal rajappa , jeffrey greenfield , anne - katrin emde , nicolas robine , olivier elemento , andrea sboner , francesca demichelis , himisha beltran , mark a . rubin , juan miguel mosquera manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors david j . 
robinson stock and other ownership interests : metastat , consulting or advisory role : progenics pharmaceuticals patents , royalties , other intellectual property : methods for diagnosing and treating prostate cancer david m . 
tagawa consulting or advisory role : medivation , astellas pharma , dendreon , janssen , bayer , genentech , sanofi , endocyte , immunomedics speakers bureau : amgen research funding : eli lilly ( inst ) , sanofi ( inst ) , janssen ( inst ) , astellas pharma ( inst ) , progenics ( inst ) , millennium ( inst ) , amgen ( inst ) , bristol - myers squibb ( inst ) , dendreon ( inst ) , rexahn pharmaceuticals ( inst ) , bayer ( inst ) , genentech ( inst ) , newlink genetics ( inst ) , inovio pharmaceuticals ( inst ) , astrazeneca ( inst ) , immunomedics ( inst ) , novartis ( inst ) , aveo ( inst ) , rexahn pharmaceuticals ( inst ) , boehringer ingelheim ( inst ) , merck ( inst ) , stem centrx ( inst ) travel , accommodations , expenses : sanofi jeffrey greenfield no relationship to disclose anne - katrin emde no relationship to disclose nicolas robine no relationship to disclose olivier elemento no relationship to disclose andrea sboner no relationship to disclose alexandros sigaras employment : weill cornell medical college mark a . 
rubin research funding : eli lilly , janssen francesca demichelis patents , royalties , other intellectual property : coinventor on a patent filed by the university of michigan and the brigham and womens hospital covering the diagnostic and therapeutic fields for ets fusions in prostate cancer . 
the diagnostic field has been licensed to gen - probe . himisha beltran consulting or advisory role : bayer , janssen oncology , genzyme research funding : astellas pharma ( inst ) , eli lilly ( inst ) , janssen ( inst ) , millennium ( inst ) , stemcentryx abbvie juan miguel mosquera no relationship to disclose acknowledgment we thank our patients and their families for participation in this study . 
we also acknowledge douglas scherr , md , and christopher barbieri , md , for contributing samples ; to yasmin khakoo , md , and our other referring clinicians ; to our clinical pathology fellows for their assistance during rapid autopsies ; to terra mcnary , loredana puca , mirjam blattner , uday bhanu maachani , nector garcia , anvioris taveras , and yelena churakova for technical assistance ; to funeral home transport personnel ; to autopsy and laboratory personnel involved in this project ; and to rogerio paulo da silva for art design . myriam kossai no relationship to disclose jacqueline fontugne no relationship to disclose robert kim no relationship to disclose rema rao no relationship to disclose danielle pancirer no relationship to disclose bishoy faltas no relationship to disclose rohan bareja no relationship to disclose ana m . 
shah rb , mehra r , chinnaiyan am , et al : androgen - independent prostate cancer is a heterogeneous group of diseases : lessons from a rapid autopsy progracancer res 64 : 9209 - 9216 , 2004 5 . 
zarghooni m , bartels u , lee e , et al : whole - genome profiling of pediatric diffuse intrinsic pontine gliomas highlights platelet - derived growth factor receptor alpha and poly ( adp - ribose ) polymerase as potential therapeutic targets . j clin oncol 28 : 1337 - 1344 , 2010 6 . 
esgueva r , park k , kim r , et al : next - generation prostate cancer biobanking : toward a processing protocol amenable for the international cancer genome consortiudiagn mol pathol 21 : 61 - 68 , 2012 7 . 
udager am , shi y , tomlins sa , et al : frequent discordance between erg gene rearrangement and erg protein expression in a rapid autopsy cohort of patients with lethal , metastatic , castration - resistant prostate cancer . 
prostate 74 : 1199 - 1208 , 2014 juric d , castel p , griffith m , et al : convergent loss of pten leads to clinical resistance to a pi ( 3 ) ka inhibitor . 
xie t , musteanu m , lopez - casas pp , et al : whole exome sequencing of rapid autopsy tumors and xenograft models reveals possible driver mutations underlying tumor progression . 
hoffman lm , dewire m , ryall s , et al : spatial genomic heterogeneity in diffuse intrinsic pontine and midline highgrade glioma : implications for diagnostic biopsy and targeted therapeutics . 
rennert h , eng k , zhang t , et al : development and validation of a whole - exome sequencing test for simultaneous detection of point mutations , indels and copy - number alterations for precision cancer care . 
quail ma , kozarewa i , smith f , et al : a large genome centers improvements to the illumina sequencing systenat methods 5 : 1005 - 1010 , 2008 med genomics 8 : 9 , 2015 2015 17 . 
sboner a , habegger l , pflueger d , et al : fusionseq : a modular framework for finding gene fusions by analyzing paired - end rna - sequencing data . 
derrien t , johnson r , bussotti g , et al : the gencode v7 catalog of human long noncoding rnas : analysis of their gene structure , evolution , and expression . 
chung s , tamura k , furihata m , et al : overexpression of the potential kinase serine / threonine / tyrosine kinase 1 ( styk 1 ) in castration - resistant prostate cancer . 
demichelis f , greulich h , macoska ja , et al : snp panel identification assay ( spia ) : a genetic - based assay for the identification of cell lines . 
 large - cell neuroendocrine carcinoma of the lung : a focused analysis of braf alterations and case report of a braf non - v600 mutated tumor responding to targeted therapy purpose in advanced stages , large - cell neuroendocrine carcinoma of the lung ( l - lcnec ) mimics small - cell lung cancer despite its traditional classification as a non small - cell lung cancer . 
here we present a focused analysis of braf mutations in this population . patients and methods comprehensive genomic profiling of tumor tissues was performed from a cohort of 300 patients with biopsy - proven l - lcnec . 
the importance of biomarker - driven therapy is subsequently highlighted with our case of a 69 - year - old man diagnosed with metastatic l - lcnec who did not respond to cisplatin plus etoposide . 
a significant durable response was then demonstrated with therapy targeted toward a braf non - v600e activating mutation ( g469r ) associated with biomarker response identified through circulating cell - free tumor dna analysis . 
giles author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : young kwang chae , md , mph , mba , northwestern medicine developmental therapeutics institute , 645 n . 
the 2015 who classification modified this outline and instead included all lung nets as a single entity , acknowledging that there exist major histologic , epidemiologic , and clinical differences between the carcinoids and high - grade l - lcnec and sclc.3 l - lcnec remains both rare and difficult to treat given the discord between its histologic and clinical characteristics . 
 chemotherapy regimens used for the treatment of sclc should be used ( etoposide and platinum combinations ) , which is reflected in national clinical cancer network ( nccn ) guidelines . 
 in the era of next - generation sequencing ( ngs ) , it is interesting to note that this strategy has yet to be adapted for the category of nonadenocarcinomas and nonsquamous cell carcinomas , which is certainly limiting in our ability to further identify these difficult - to - classify malignancies . 
nccn guidelines only mention ngs for adenocarcinomas . here we summarize the current landscape of l - lcnec and explore in detail the specific genomic alterations pertaining to braf , a member of the serine / threonine kinase raf family , in the largest cohort of patients with l - lcnec . 
 mutations and copy - number gains in the phosphatidylinositol 3 - kinase / akt / mammalian target of rapamycin pathway were detected in 15% of the tumors compared with 17% of sclc tumors.6 in another study using ngs in a cohort of 45 patient cases of l - lcnec , the most commonly altered genes similarly included tp53 ( 78% ) , rb1 ( 38% ) , stk11 ( 33% ) , keap1 ( 31% ) , and kras ( 22% )  . 
l - lcnecs with coaltered rb1 and tp53 ( 40% ) were identified as sclc - like , whereas tumors without this pattern ( 56% ) were identified as nsclc - like . 
as a whole , braf mutations are detected in 2% to 4% of lung cancers and have primarily been identified in adenocarcinomas.8 interestingly , although v600 mutations comprise the majority of braf alterations in melanoma , the v600e mutation is accountable for approximately 50% of braf mutations identified in nsclcs and up to 80% in late stages.8 as recently as late 2015 , the prognostic and biologic implications of braf mutations in nsclc were limited and controversial when evaluating the existing case series . 
subsequent studies were positive for cytokeratin 7 , thyroid transcription - 1 , synaptophysin , and chromogranin , thereby resulting in the diagnosis of metastatic , high - grade neuroendocrine carcinoma ( l - lcnec ) of lung primary ( fig 1 ; appendix ) .11 additional evaluation with brain magnetic resonance imaging and positron emission tomography ct identified a 1.4 - cm nodule in the superior segment of the left lower lobe , likely the site of the primary tumor . 
three months after rt , ct scans showed that the left hemipelvic mass had decreased in size to 3.5 4 cm , with a central area of necrosis ; however , the left lower lobe lung nodule was noted to have grown to 2 cm . ngs of tumor tissue ( foundationone ; foundation medicine , cambridge , ma ) had been performed at diagnosis and revealed mutations in braf ( g469r ) , erbb4 ( a118s ) , stk11 ( l282fs * 3 ) , and tp53 ( r248l ) ; myc amplification was also identified . 
given these molecular findings describing an activating braf mutation , treatment with trametinib ( 2 mg orally once daily ) and dabrafenib ( 150 mg orally twice daily ) was initiated at this time . 
trametinib is a mek inhibitor that prevents raf - dependent mek phosphorylation.8 dabrafenib is a braf serine / threonine kinase inhibitor that has high selectivity for braf v600emutant proteins.8 cell - free dna ( guardant360 ; guardant health , redwood city , ca ) analysis performed at diagnosis demonstrated concordance in detecting mutations in braf ( g469r ) and tp53 ( r248l ) , as well as myc amplification . 
 histology of needle core biopsy : ( c ) hematoxylin stain , 600 ; immunostains for ( d ) prostate - specific antigen , ( e ) cytokeratin 7 , ( f ) chromogranin , ( g ) synaptophysin , ( h ) thyroid transcription - 1 , and ( i ) cdx2 , 600 . expression of the patients braf g469r mutation was demonstrated , from 36.8% at time of diagnosis to nondetectable at both 5 months ( which may also have been in part a result of rt and subsequent tissue necrosis ) and 10 months after initiation of dabrafenib and trametinib ( fig 2 )  . there was an increase in other detectable alterations , which included synonymous mutations in brca1 , arid1a , and smo as well as vuss in apc , pten , fgfr1 , and pik3ca ( figs a1 - a3 )  . 
 presently , a full 15 months since initiating therapy with dabrafenib and trametinib , the patient is continuing with therapy and continues to demonstrate an eastern cooperative oncology group performance status of 0 . 
his latest ct scans ( 18 months after rt and 15 months after initiating targeted therapy ) show no residual pelvic mass and a stable left lower lobe nodule measuring 1.7 cm ( fig 3 )  . 
samples were pulled from an ngs database as part of a deidentified pool with only basic demographic information available ( required for processing the ngs order ) from many institutions . 
an inherent limitation of this pool is that we have to assume the histology of the malignancy was confirmed at each local institution . the atypical variants of braf in l - lcnec are identified as g469a , k601n , and g469r , which are all known to be activating mutations.14 - 17 there also exists g466v , which is an oncogenic kinase - impaired alteration.18 the remainder includes n581i and vus alterations e220k , w210l , g9d , and p149t . 
n581i is a known recurrently somatic braf alteration , but its effect has not been characterized ; otherwise , to our knowledge , these remaining braf mutations have not been previously identified.19 our analysis is summarized in table 1 . discussion current understanding of braf v600 mutations originated in melanoma , where they are the most commonly identified oncogenic mutations and are seen in nearly 50% of cutaneous melanomas.21 braf is an upstream effector of the mitogen - activated protein kinase pathway ( ras / raf / mek / extracellular regulated kinase ) , which plays a central role in cell growth , division , and differentiation . 
ninety percent of braf - mutated melanomas result from a substitution of glutamic acid for valine at codon 600.22 the braf v600e mutations show a 500 - fold increase in catalytic activity compared with the wild type.23 initially , selective braf inhibitors such as vemurafenib and dabrafenib were evaluated as monotherapy in patients with metastatic melanoma harboring either braf v600e or v600k mutations . 
contrast - enhanced computed tomography scans of the ( a , c , e , g ) abdomen and ( b , d , f , h ) chest of the patient ( a , b ) at diagnosis , ( c , d ) approximately 1 month after chemotherapy , ( e , f ) 3 months after radiation therapy ( rt ) directed at the left hemipelvic mass , and ( g , h ) after 15 months of targeted therapy with dabrafenib and trametinib . 
 melanoma , colorectal cancer , or nsclc , investigators concluded that kinase activity is likely to be elevated in 35% of braf mutations , impaired in 15% , and unknown in 10%.18 known nonv600e activating variants of braf that have been identified in patients with nsclc include g464v , g466a , g469a / v / r / s , and k601e . 
 mutations with impaired activity have been reported to be g466r / v , d594a / e / g / h / n / v , and g596c / r.20 interestingly , it has been identified that concomitant kras or nras mutations are more likely occur with the kinase - impaired braf mutants than the kinase - activated braf mutants.18 preclinical data have demonstrated sensitivity to treatment with dabrafenib and trametinib in hek293t cells , lung epithelial cellular models ( beas - 2b ) , and human cancer cell lines harboring non - v600 braf mutations ( both activating and kinase impaired )  . 
this same study also identified that the kinase activity of the g469s variant was comparable to that seen with the braf v600e mutation.20 this further provides a basis for the ongoing exploration of targeted therapy in non - v600 braf - mutant lung cancers . with regard to lung cancer , nccn guidelines for nsclc delineate emerging targeted therapy options for patients with genetic alterations.25 vemurafinib has been studied in multiple nonmelanoma cancers with braf v600 mutations in a basket trial design ( clinicaltrials.gov identifier nct01524978 ) ; in a cohort of 20 patients with nsclc , eight achieved partial responses with targeted braf inhibition.26 in a clinical trial studying dabrafenib plus trametinib in patients with previously treated braf v600emutant metastatic nsclc ( clinicaltrials.gov identifier nct01336634 ) , investigators reported an overall response rate of 63.2% in a cohort of 57 patients.27 this led to the recent approval of dabrafenib with trametinib as a treatment option for patients with advanced or metastatic nsclc with a braf v600 mutation by the us food and drug administration in june 2017.28 interestingly , there is minimal guidance available for non - v600 braf - mutated lung malignancies and even less information specifically focused on sclc or nets . 
remarkably when using ngs ( a broad and sensitive detection tool ) , non - v600e mutations comprise a substantial portion of the braf mutations in different tumors ( nsclc , 86% ; melanoma , 34% ; and colorectal cancer , 23% ) , as assessed in a cohort of more than 800 patients.17 this is a higher proportion of non - v600e braf mutations than identified in earlier retrospective studies with cohorts of 30 to 50 patients . 
in a retrospective study detailing the characteristics of nearly 700 patients with lung adenocarcinoma , braf mutations were present in 3% of patients ( v600e , 50% ; g469a , 39% ; and d594g , 11% )  . 
 interestingly , all of these patients were current or former smokers.29 currently , ngs assays demonstrate the best - known sensitivity and breadth of analysis for the clinical detection of braf mutations including non - v600e alterations.17 in our patient , of course , we must acknowledge the confounding variable of rt directed at the left hemipelvis in the reduction in size of the mass in this location . 
given this , in addition to the steep drop - off seen in braf circulating tumor dna , we suspect that this is a durable response to therapy . it is worth mentioning that cosmic presents information related to adenocarcinoma and squamous cell carcinoma but not l - lcnec . 
this does not reflect the scenario of a real - world stage iv malignancy . although not common , l - lcnec does seem to contain activating and thus actionable alterations as evidenced by our patient 's remaining stable with therapy focused at braf inhibition . 
 in particular , given the scope of non - v600 braf alterations , the basket trial design is ideal for furthering our understanding of the functionality of these various mutations in a histology - agnostic manner . 
the nci - match ( national cancer institute molecular analysis for therapy choice ) trial is currently under way and includes a nonv600 arm in which patients will receive trametinib . 
giles jon chung employment : foundation medicine administrative support : young kwang chae provision of study material or patients : young kwang chae , vincent miller collection and assembly of data : young kwang chae , keerthi b . 
 for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : foundation medicine xiaoqi lin no relationship to disclose vincent miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan kettering cancer center siraj m . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome stuff in non - neoplastic disease ( i ) young kwang chae consulting or advisory role : foundation medicine , boehringer ingelheim , biodesix , counsyl , astrazeneca , guardant health speakers bureau : merck , genentech / roche travel , accommodations , expenses : hanmi francis j . 
tamragouri no relationship to disclose consulting or advisory role : novartis travel , accommodations , expenses : medimmune , novartis , foundation medicine affiliations young kwang chae , keerthi b . 
lurie comprehensive cancer center , northwestern university ; xiaoqi lin , northwestern memorial hospital , northwestern university , chicago , il ; and jon chung , vincent miller , and siraj m . 
yao jc , hassan m , phan a , et al : one hundred years after carcinoid : epidemiology of and prognostic factors for neuroendocrine tumors in 35 , 825 cases in the united states . 
travis wd , brambilla e , nicholson ag , et al : the 2015 world health organization classification of lung tumors : impact of genetic , clinical and radiologic advances since the 2004 classification . 
rekhtman n , pietanza mc , hellmann md , et al : next - generation sequencing of pulmonary large cell neuroendocrine carcinoma reveals small cell carcinoma - like and non - small cell carcinoma - like subsets . 
lin x , saad rs , luckasevic tm , et al : diagnostic value of cdx - 2 and ttf - 1 expressions in separating metastatic neuroendocrine neoplasms of unknown orig appl immunohistochem mol morphol 15 : 407 - 414 , 2007 12 . 
noeparast a , teugels e , giron p , et al : non - v600 braf mutations recurrently found in lung cancer predict sensitivity to the combination of trametinib and dabrafenib . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) - mutant metastatic non - small cell lung cancer : an open - label , multicentre phase 2 trial . 
 fine - needle aspiration and core - needle biopsy percutaneous fine - needle aspiration ( fna ) and core - needle biopsy ( cnb ) were performed under ultrasound guidance using a 22 - gauge needle for fna and a 20 - gauge core biopsy device for cnb.10 one fna pass was used for localization . 
airdried fna smear was stained with diff - quik stain for on - site evaluation of adequacy and immediate interpretation by a board - certified cytopathologist ( x.l. ) , and alcohol - fixed fna smear was stained with papanicolaou statwo cnb passes were obtained for histologic examination . 
immunohistochemical stains for prostate - specific antigen ( a0562 ; dakocytomation , carpinteria , ca ) , cytokeratin 7 ( ck7 ; a7018 ; dakocytomation ) , chromogranin ( 760 - 2519 ; ventana , tucson , az ) , synaptophysin ( 336a - 76 ; cell marque , rocklin , ca ) , thyroid transcription - 1 ( ttf - 1 ; 343m - 98 ; cell marque ) , and cdx2 ( mu392a - uc ; biogenex , san ramon , ca ) were performed in an automated immunostainer with appropriate positive and negative controls following manufacturers instructions , meaning that positive controls were stained positive and negative controls were stained negative . pathology results fna smears showed loosely cohesive nests or three - dimensional clusters of pleomorphic epithelial cells with focal rosette pattern ( figs a1a and a1b )  . 
the tumor cells were positive for neuroendocrine immunomarkers ( chromogranin and synaptophysin ; fig a1f and a1g ) , ck7 ( fig a1e ) , and ttf - 1 ( a marker for lung adenocarcinoma , lung neuroendocrine neoplasm , 11 and thyroid neoplasm ; fig a1h )  . 
the tumor cells were negative for prostate - specific antigen ( fig a1d ) and cdx2 ( an immunomarker for gi adenocarcinoma and neuroendocrine neoplasm arising from gi tract ; fig a1i ) .11 on the basis of the morphology and immunoprofile , a large - cell neuroendocrine carcinoma diagnosis was rendered . 
the tumor cells were also positive for ttf - 1 and ck7 and negative for cdx2 , suggesting lung origin.11 appendix sample submission time point oct - 16 ( % ) aug - 15 ( % ) pten ( q214 * ) erbb2 ( r143q ) braf ( g469r ) 36.8 mar - 17 ( % ) fig . 
suarez , md1 introduction genomic sequencing of colorectal cancers reveals that 16% have a very high tumor mutation burden ( tmb ) .1 three quarters of such tumors display microsatellite instability ( msi ) associated with silencing or somatic mutation of mismatch repair ( mmr ) genes . 
among advanced colorectal cancers , prevalence of pole mutations remains unknown , but only 3.5% are defective in mmr.2 pole proofreading and mmr act in concert to correct replication errors . because mmr - decient tumors often respond to therapy , 3 - 5 pole - mutated tuimmune checkpoint mors might also respond . 
pathology revealed moderately differentiated adenocarcinoma with two involved lymph nodes , classied as stage iiic disease ( pt4bn1b according to the american joint committee on cancer staging system , eighth edition )  . 
after adjuvant chemotherapy with uorouracil and oxaliplatin , computerized tomography ( ct ) scan showed no evidence of disease . three years later , biopsy of an enlarging left supraclavicular lymph node revealed a kras - mutated mss adenocarcinoma with abundant extracellular mucin and a lack of programmed death ligand 1 ( pd - l1 ) tumor cell expression by both e1l3n and sp263 antibody clones . 
the tumor - inltrating lymphocytes ( tils ) could not be assessed , because this was a lymph node metastasis and the primary tumor was unavailable . the patient received uorouracil and irinotecan plus bevacizumab . 
treatment was complicated by a small bowel stula , which required discontinuation of bevacizumab , partial small bowel resection , takedown of an enterorectal stula , and placement of a permanent rectal tube . after a 3 - month recovery from surgical complications , imaging showed new pulmonary metastases . 
the enlarging left supraclavicular nodal mass led to horner syndrome with ptosis and near syncope , which required palliative radiation . the left supraclavicular lymph node specimen obtained 3 years after surgery displayed approximately 20% tumor purity by histology . 
genomic proling with the stanford solid tumor actionable mutation panel , a hybrid capturebased next - generation sequencing assay , revealed an ultra - high tmb relative to colorectal carcinomas analyzed on the same panel ( fig 1b )  . additional testing demonstrated intact expression of mmr proteins as well as mss by polymerase chain reaction . 
the boxplot shows the median , interquartile range , and standard deviation for the tmb in 82 microsatellite - stable ( mss ) colorectal cancers ( crcs ) detected by the stanford solid tumor actionable mutation panel at the time of patient testing . 
the gray dots indicate tmb for those pole - mutated tumors reported to have responded to programmed death 1 ( pd - 1 ) blockade : two crcs and two endometrial cancers ( ecs )  . 
the box plots show the tmb for a survey of 859 tumors with likely driver mutations in mismatch repair genes that would produce microsatellite instability ( msi ) and 102 tumors with known or likely functional pole mutations ( adapted from chalmers et al16 )  . 
on the basis of the ultra - high tmb , estimated at 200 mutations / mb ( fig 1c ) , our molecular tumor board recommended immunotherapy with an immune checkpoint inhibitor . pembrolizumab was obtained for compassionate use . treatment led to a transient increase in the carcinoembryonic antigen ( cea ) from 2 , 742 ng / ml to a peak of 3 , 727 ng / ml followed by a decline to a plateau of 57 to 83 ng / ml which was maintained through 25 months of treatment and an additional 3 months of follow - up ( fig 2a )  . this was associated with resolution of pain and normalization of performance status from eastern cooperative oncology group status of 2 to 0 . 
bars above the graph indicate periods of treatment with uorouracil and irinotecan ( folfiri ) , uorouracil and oxaliplatin ( folfox ) , regorafenib , triuridine ( tfd ) and tipiracil ( tpi ) , radiation therapy ( xrt ) to the left supraclavicular mass , and the programmed death 1 ( pd - 1 ) inhibitor pembrolizumab . 
the delayed response was consistent with slow clearance of mucin after tumor cell death . the patient experienced a brief episode of localized herpes zoster and later a brief episode of asymptomatic grade 1 transaminitis . 
each episode was addressed by withholding one cycle of pembrolizumab , and each quickly resolved without sequelae . discussion in recent years , immune checkpoint blockade has emerged as a safe and effective treatment of many solid tumors . 
in particular , tumors with high level of msi and mismatch repair deciency have shown dramatic responses to treatment with inhibitors.4 , 5 similarly , accumulating immune checkpoint evidence suggests that tmb alone , independent of mmr status , correlates with response to immune checkpoint blockade for some tumor types.3 , 6 - 9 hence , mss tumors with an ultra - mutated phenotype as a result of mutations in pole or pold110 , 11 represent an intriguing subset of tumors that may also respond to immune checkpoint inhibitors . the case presented here adds to the few reports of polemutated tumors that responded to pd - 1 checkpoint blockade . 
by contrast , the responsive tumors were inconsistent in pd - l1 expression ( fig 1d )  . unlike patients in the other cases , the patient in this report began treatment with the greatest extent of disease and enjoyed the longest sustained response ( which continued beyond 28 months )  . 
radiologic density of tumors failed to change signicantly for 8 months before nally disappearing at 28 months . the dramatic response in this patient shows the potential benet of evaluating mss tumors for pole and possibly pold1 mutations . 
however , it is important to realize that some pole or pold1 mutations , particularly previously uncharacterized mutations , may prove to be passenger alterations with no effect on tmb.10 a prospective analysis of 80 , 853 patients with advanced solid tumors revealed known genomic alterations in pole in only 259 patients ( 0.3% ) , with a median tmb of 31 mutations / mb.17 the most common mutation was p.r446q ( n = 77 ) , which is uncharacterized , associated with low tmb ( less than ve mutations / mb ) , and predominantly germline . 
the two nextmost - common mutations , p.p286r ( n = 41 ) and p.v411l ( n = 29 ) , are both functional , associated with high tmb ( greater than 20 mutations / mb ) , predominantly somatic , and enriched in colorectal cancer and endometrial carcinoma . 
these were the mutations present in the four polemutant tumors that have responded to pd - 1 checkpoint blockade in this and other published reports ( fig 1d )  . however , not all pole - mutated tumors respond to checkpoint blockade . 
two colorectal cancers with the p.p286r mutation showed progressive and stable disease after 1 and more than 10 months of follow - up.15 both cases showed low levels of cd8 + tils . 
lo employment : genentech , roche stock and other ownership interests : genentech , roche gilbert chu patents , royalties , other intellectual property : rapid small volume detection of blood ammonia , patent no . 
nature 487 : 330 - 337 , 2012 koopman m , kortman ga , mekenkamp l , et al : decient mismatch repair system in patients with sporadic advanced colorectal cancer . 
br j cancer 100 : 266 - 273 , 2009 rizvi na , hellmann md , snyder a , et al : mutational landscape determines sensitivity to pd - 1 blockade in nonsmall - cell lung cancer . 
science 348 : 124 - 128 , 2015 le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
science 357 : 409 - 413 , 2017 le dt , uram jn , wang h , et al : pd - 1 blockade in tumors with mismatch - repair deciency . 
n engl j med 372 : 2509 - 2520 , 2015 snyder a , makarov v , merghoub t , et al : genetic basis for clinical response to ctla - 4 blockade in melanoma . 
n engl j med 371 : 2189 - 2199 , 2014 goodman am , kato s , bazhenova l , et al : tumor mutational burden as an independent predictor of response to immunotherapy in diverse cancers . 
mol cancer ther 16 : 2598 - 2608 , 2017 . kowanetz m , zou w , shames d , et al : oa20.01 : tumor mutation burden ( tmb ) is associated with improved efcacy of atezolizumab in 1l and 2l + nsclc patients . 
santin ad , bellone s , buza n , et al : regression of chemotherapy - resistant polymerase ( pole ) ultra - mutated and msh6 hyper - mutated endometrial tumors with nivolumab . 
wang c , gong j , tu ty , et al : immune proling of microsatellite instability - high and polymerase ( pole ) mutated metastatic colorectal tumors identies predictors of response to antipd - 1 therapy . 
schrock ab , fabrizio d , he y , et al : analysis of pole mutation and tumor mutational burden ( tmb ) across 80 , 853 tumors : implications for immune checkpoint inhibitors ( icpis )  . 
 expanded analysis of secondary germline findings from matched tumor / normal sequencing identies additional clinically signicant mutations ecaterina ileana dumbrava , md1 ; lauren brusco , phd1 ; molly s . 
mills , md1 ; ken chen , phd1 ; and funda meric - bernstam , md1 purpose next - generation sequencing ( ngs ) for tumor molecular proling can reveal secondary germline likely pathogenic and pathogenic variants ( lpv / pv )  . 
the american college of medical genetics and genomics ( acmg ) recommends return of secondary results for a subset of 59 genes , but other genes with evidence of clinical utility are emerging . 
five mutations in highpenetrance hereditary cancer predisposition genes were selected to be returned to patients or their representatives : bap1 , cdh1 , cdkn2a , egfr , and smarca4 . conclusion broader genomic testing is likely to identify additional secondary pathogenic germline alterations , some with potential clinical utility for return to patients and their relatives . 
2019 by american society of clinical oncology introduction with the exponential development of next - generation sequencing ( ngs ) , specically the ability to sequence larger panels of genes in more depth , molecular proling increasingly is being integrated into oncology practice.1 , 2 the main goal of ngs is to identify actionable genomic alterations in the tumor to target by matched drugs in efforts to personalize treatment.3 in addition , ngs can be used for testing of prognostic biomarkers of disease progression and metastasis , testing of cancer predisposition genes , and cancer risk assessment for at - risk asymptomatic family members . sequencing matched tumor and normal tissue samples from the same patient can assist in more - accurate calling of somatic variants.4 - 6 often , germline variants are subtracted and ignored ; however , analysis of secondary germline ndings might identify variants associated with an increased susceptibility to develop cancer or other diseases . 
 ileana dumbrava et al solicit patients preference with regard to the return of pathogenic germline alterations before testing.9 however , the systematic return of germline alterations found during ngs requires implementation of bioinformatics programs for variant detection , curation , and annotation ; such implementation increases the required resources , time , and costs.9 , 10 in this study , we sought to determine whether ngs of matched tumor and normal samples revealed secondary germline pv and likely pathogenic variants ( lpv ) in genes beyond those currently recommended by the acmg . 
patients also were offered possible secondary germline mutation testing in a companion institutional review boardapproved protocol.11 the patients relevant clinical characteristics were collected from electronic medical records and prospectively maintained institutional databases . matched tumor / normal dna sequencing paired tumor / normal dna - targeted exome sequencing of 201 genes was performed in a research laboratory ( data supplement ) .12 tumor samples were acquired as formalinxed parafn - embedded slides in which the tumor area the tumorwas circled to facilitate macrodissection of containing region . 
the key elements of ngs , including dna extraction , library preparation , target enrichment , sequencing , and variant calling , were performed on tumor / normal tissue samples . 
alignment of the sequenced data to human reference assembly hg19 and variant calling of the sequencing reads have been described previously.13 - 15 single nucleotide variants and small indels were called using the genome analysis tool kit ( broad institute , cambridge , ma )  . 
loss of the normal allele in the tumor ( loss of heterozygosity ) was evaluated in the analyzed genes . selection of genes for analysis for secondary germline findings our group previously published the germline lpv / pv results for 18 of 56 genes recommended by acmg that were included in our 201 - gene panel.11 palb2 also was included in a previous secondary germline analysis because of its strong association with hereditary breast cancer.16 after a thorough literature search and evaluation of relevant databases , 17 - 19 we selected 54 additional genes from our panel for which we analyzed germline lpv / pv . 
these genes were selected on the basis of the mode of inheritance and known penetrance for disease phenotype , including genes previously described as hereditary - cancer susceptibility ; genes currently tested in commercially available hereditary panels ; cancer - related genes often tested on matched normal / tumor panels , however with the mode of inheritance nonconsistent with phenotypic expression in patients ; and noncancer - related genes with suggested familial heritance ( data supplement )  . 
on the basis of the mode of inheritance , known penetrance for a disease phenotype , and presence or absence of management guidelines , the identied lpv / pv were grouped into ve categories ( data supplement ) : ( 1 ) established hereditary cancer susceptibility genes ( not in the acmg recommended genes in 2015 , which were previously reported by our group11 ) and smad4 ( which was added to the recommended genes in 2016 ) , ( 2 ) hereditary cancer susceptibility genes with moderate penetrance included in available genetic testing panels with suggested management guidelines ( atm and chek2 ) , ( 3 ) genes wherein somatic variants are associated with cancer but germline mutations are associated with noncancer phenotypes , ( 4 ) other cancer - related genes with unknown clinical validity of pathogenic germline alterations , and ( 5 ) hereditary noncancer susceptibility genes with other possible clinical utility . clinical signicance interpretation of variants variant clinical signicance classication was assigned according to acmg guidelines.20 , 21 the online tools and databases used to classify the clinical signicance of the remaining variants are detailed in figure 1 . 
the clinical signicance annotation of all variants in the 54 additional genes analyzed in this study were independently analyzed using intervar , a bioinformatics software tool that uses an annotated le generated from annovar22 and classies each variant on the basis of the association of molecular pathology / acmg 2015 guidelines , 20 and by a scientist with germline variants annotation expertise from the institute for personalized cancer therapy at the university of texas md anderson cancer center . 
 ileana dumbrava et al recommendation for cancer somatic variant evaluation , we focused on tier i and ii variants , which include lpv / pv.21 furthermore , personal and family history of cancer was reviewed for all patients with identied lpv / pv . determination of which results to return to patients a committee of oncologists , a genetic counselor , molecular pathologists , an ethicist , and behavioral scientists developed criteria for return of results to patients . 
the lpv / pv in wellestablished hereditary cancer predisposition genes with high penetrance for which management recommendations were available were recommended to be returned to patients who expressed interest in knowing about secondary germline ndings . 
variants selected to be returned to patients or their personal representative , were validated with an orthogonal assay in a clinical laboratory improvement amendmentscertied laboratory using the same deidentied research specimen before formal genetic counseling and genetic testing . results study population among the 1 , 000 patients who underwent matched tumor / normal dna sequencing for personalized cancer therapy in the clearinghouse protocol , the most frequent tumor types were breast ( 25.3% ) and colorectal ( 15.6% ) cancers , glioblastoma ( 15.1% ) , melanoma ( 14.3% ) , and sarcoma ( 10.2% ; fig 2 )  . 
four patients had a personal history of a previous malignancy ( data supplement )  . we identied two patients who had two germline lpv / pv ( one mutation from the acmg - recommended return of results list that was found previously and one from the list of genes described here )  . 
the second patient was a 13 - year - old girl who had a solid pseudopapillary neoplasm of the pancreas with two deleterious germline mutations ( msh6 and ercc3 ) , and although she had no relevant family history , previous genetic testing revealed a germline mutation in msh6 suggestive of lynch syndrome . of the 46 patients with lpv / pv , only 11 ( 24% ) had been referred previously for genetic counseling . 
the most frequent lpv / pv were identied in the following genes : 10 chek2 mutations ( 1% ) , ve ar mutations ( 0.5% ) , four atm mutations ( 0.4% ) , four ercc3 mutations ( 0.4% ) , four mitf mutations ( 0.4% ) , four pkhd1 muthree nf1 mutations ( 0.3% ) , and two tations ( 0.4% ) , chek1 mutations ( 0.2% ; fig 3 )  . 
on the basis of currently available drugs ( food and drug administration approved or currently in clinical trials ) , 26 lpv / pv were found in eight potentially therapeutically actionable genes ( chek2 , ar , atm , nf1 , cdkn2a , egfr , hras , ptch1 )  . lpv / pv were found in several tumor types , most frequently breast cancer , colorectal cancer , glioblastoma , melanoma , sarcoma , and ovarian cancer ( table 2 )  . 
among the 10 patients with breast cancer with lpv / pv , 10 variants were observed in eight genes ( data supplement )  . of the 46 lpv / pv , 20 ( 44% ) were known to be pathogenic and previously reported in clinvar23 and related to an increased risk of cancer or other diseases . 
twenty - six variants were identied as lpv on the basis of the effect / location of the genomic change on the protein function or the databases and online tools shown in figure 1 . 
in cases of low median allele fraction , the results were rechecked and validated to be of germline origfour patients ( 8.7% ) presented loss of heterozygosity in the same genes as the identied germline lpv / pv ( two patients with nf1 mutation , one with atm mutation , and one with smarca4 mutation )  . concordance of manual and automatic variant interpretation variant clinical signicance was determined using databases and online tools ( fig 1 )  . 
all variants also were annotated using intervar.24 we compared manual annotations with the automatic annotation tool and observed concordance rates between 88% and 98% , which depended on the type of alteration analyzed ( point v truncating mutations )  . return of results to patients or their personal representative the committee decided that germline lpv / pv in the following established hereditary cancer predisposition genes with high penetrance should be returned to patients : bap1 , cdh1 , cdkn2a , egfr , and smarca4 ( appendix fig a1 )  . all these results were previously unknown to the patient , and none of the ve patients had been previously referred to genetic counseling or underwent prior genetic testing . all ve lpv / pv were conrmed using de - identied samples in a clinical laboratory improvement amendments certied laboratory using a different platform ( 100% concordance obtained )  . 
the patient underwent formal genetic testing and genetic counseling , and the cdkn2a p.g101w mutation was conrmed ; she was enrolled in a pancreatic cancer screening program in addition to dermatologic surveillance because of her history of metastatic melanoma , which is currently without evidence of disease . 
indeed , a recent study showed that more than one half of patients with deleterious secondary germline ndings would not have been tested using current clinical guidelines.27 in the current study , from the additional genes tested , only the nf1 mutations had been identied before the matched normal / tumor dna sequencing , which indicates that important cancer predisposition genes may be missed by current criteria for referral to a genetic counselor and genetic testing . 
furthermore , in addition to colon , breast , and ovarian cancers , we identied lpv / pv in melanoma , glioblastoma , sarcoma , and pancreatic and gastric cancers . the 2016 acmg recommendations changed the terminology to secondary ndings instead of incidental ndings because the genes were intentionally analyzed . 
 secondary germline findings on matched tumor discussion in the return of secondary germline findings committee about which germline lpv or pv should be reported confirmation of the result in clia - approved laboratory ( if initial testing done in a research laboratory ) genetic counseling ( initial visit ) patient or personal representative ( if patient deceased ) informed by genetic counselor and physician of secondary germline findings genetic counseling ( follow - up visit ) discussion of results of the genetic testing ( confirmation or not of germline secondary finding ) formal clinical genetic testing for suspected hereditary syndrome for patients ( after informed consent ) assessment and management of second primary cancer risk family risk assessment and guidance personalized targeted treatment determination establishment of germline knowledge database participant informed consent for : tumor profiling companion germline variants analysis return of results of secondary germline findings tumor and normal sample sequencing somatic molecular profile report germline sequence annotation fig 4 . 
clia , clinical laboratory improvement amendments ; lpv / pv , likely pathogenic and pathogenic variants . likely will evolve continuously as more knowledge about hereditary syndromes is accumulated and as ngs is integrated into oncology practice , which thus will increase the likelihood of detecting secondary germline ndings.8 the cancer risk predictions associated with our gene classications is based on highly penetrant families . 
lpv / pv in hereditary cancer susceptibility genes also are present in the general population at a very low frequency , and whether these ndings will have the same implications in patients without signicant family histories is unknown . although established public knowledgebases of lpv / pv , such as clinvar , 23 are helpful in determining the clinical signicance of germline mutations , this might have conicting results from different sources , and many variants are not yet described . 
to improve these databases , we need to share the results and establish guidelines for return of secondary germline ndings.35 the potential effect of reporting secondary germline ndings in cancer - related genes presents signicant opportunities to assess and manage the risk of second primary cancers , assess familial risk , and provide targeted treatment options . 
although the clinical utility of germline lpv / pv in some genes outside the acmg list is still unknown , rapid advances of biologic knowledge and new drug development could aid in identifying new actionable alterations to serve as the basis for future clinical trial design and personalized cancer therapy.36 , 37 increasing patient interest exists in knowing about secondary germline ndings ; however , which results should be returned remains controversial . 
in this study , a committee of oncologists , a genetic counselor , molecular pathologists , an ethicist , and behavioral scientists believed that in the absence of signicant cancer family history , the clinical utility of pathogenic secondary germline ndings in moderate penetrance genes like chek2 remains with many uncertainties and knowledge gaps ; thus , moderate penetrance genes were not returned . 
this decision was made , in part , because the patients were deceased , which made it difcult to denitively conrm results because they were obtained in the research environment . 
our process for identifying , conrming , and returning secondary germline ndings is summarized in figure 4 . results cases , 40 but this might be overcome with the integration of new variant analysis tools and education programs to ll the knowledge gap among treating cancer care providers and patients . the current study is that one limitation of the patient population was from an academic center where many patients were referred for consideration of clinical trials ; this population may inuence the overall results / detection of germline lpv / pv in particular tumor types . 
in addition , our return - of - results efforts did not include variants of unknown signicance that might have clinical implications in the future with the rapidly evolving eld . important barriers left to be overcome when disclosing germline deleterious variants are psychological outcomes and family communication barriers.38 , 39 in deceased patients , identication and contact of a personal representative and making the information on secondary germline ndings available but allowing the right to decline represent other barriers in return of results.25 currently , only 5% of genetic counselors feel prepared to handle tumor proling in conclusion , secondary germline ndings identied on tumor / normal dna proling could have implications in the assessment and management of second primary cancer risk ; family risk assessment and guidance ; and most importantly , personalized treatment determination . 
most patients would like to know about these secondary germline ndings for themselves and their families , 41 but some barriers remain to be overcome , such as the determination of which results to disclose and how to disclose them as well as the burdens that this process would place on the cancer care prograa systematic analysis of germline variants could increase the cost and time involved in dna sequencing and the interpretation of clinical signicance . 
hong , jordi rodon , scott kopetz , funda meric - bernstam collection and assembly of data : ecaterina ileana dumbrava , lauren brusco , chetna wathoo , kenna r . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . lauren brusco employment : celgene jennifer litton consulting or advisory role : pzer , astrazeneca , medivation speakers bureau : physicians education resource , uptodate , med learning group , medscape research funding : novartis ( inst ) , bristol - myers squibb ( inst ) , genentech ( inst ) , pzer ( inst ) , emd serono ( inst ) , jounce therapeutics ( inst ) , glaxosmithkline ( inst ) , medivation ( inst ) patents , royalties , other intellectual property : uptodate travel , accommodations , expenses : physicians education resource , med learning group , medscape sarina a . 
 secondary germline findings on matched tumor vivek subbiah consulting or advisory role : medimmune research funding : novartis ( inst ) , glaxosmithkline ( inst ) , nanocarrier ( inst ) , northwest biotherapeutics ( inst ) , genentech ( inst ) , roche ( inst ) , berg ( inst ) , bayer ag ( inst ) , incyte ( inst ) , fujilm ( inst ) , pharmamar ( inst ) , d3 oncology solutions ( inst ) , pzer ( inst ) , amgen ( inst ) , abbvie ( inst ) , multivir ( inst ) , blueprint medicines ( inst ) , loxo oncology ( inst ) , vegenics ( inst ) , takeda pharmaceuticals ( inst ) , alfasigma ( inst ) , agensys ( inst ) , idera pharmaceuticals ( inst ) , boston biomedical ( inst ) , inhibrx ( inst ) , exelixis ( inst ) travel , accommodations , expenses : pharmamar , bayer ag david s . 
hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack , bayer ag consulting or advisory role : baxter , bayer ag , guidepoint global , janssen pharmaceuticals , genentech , eisai , glg pharma research funding : novartis , genentech , eisai , astrazeneca , pzer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer ag , bristol - myers squibb , genmab , ignyta , innity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo oncology , medimmune , molecular templates , takeda pharmaceuticals , seattle genetics , amgen travel , accommodations , expenses : loxo oncology , mirna therapeutics jordi rodon consulting or advisory role : novartis , eli lilly , imclone systems , servier , orion , peptomyc , kelun pharmaceutical , merck sharp & dohme , spectrum pharmaceuticals , pzer research funding : novartis , bayer ag scott kopetz stock and other ownership interests : molecularmatch , navire pharma consulting or advisory role : roche , genentech , emd serono , merck , karyopharm therapeutics , amal therapeutics , biocartis , navire pharma , symphogen research funding : amgen ( inst ) , sano ( inst ) , biocartis ( inst ) , guardant health ( inst ) , array biopharma ( inst ) , genentech ( inst ) , roche ( inst ) , emd serono ( inst ) , medimmune ( inst ) , novartis ( inst ) john mendelsohn stock and other ownership interests : merrimack patents , royalties , other intellectual property : royalty payments from university of california , san diego gordon b . 
mills stock and other ownership interests : catena pharmaceuticals , spindletop capital , immunome , signalchem , tarveda therapeutics honoraria : nuevolution , astrazeneca , tarveda therapeutics , tesaro , symphogen , immunome consulting or advisory role : astrazeneca , catena pharmaceuticals , critical outcome technologies , signalchem , tarveda therapeutics , symphogen , takeda pharmaceuticals , millennium pharmaceuticals , ion pharmaceuticals , immunome research funding : miriam and sheldon g . 
adelson medical research foundation , astrazeneca , nanostring technologies , breast cancer research foundation , karus therapeutics , immunome , ion pharmaceuticals , komipharm , ovarian cancer research foundation , pzer , prospect creek foundation , tarveda pharmaceuticals , millennium pharmaceuticals patents , royalties , other intellectual property : hrd assay to myriad genetics travel , accommodations , expenses : astrazeneca , pzer , immunome , symphogen funda meric - bernstam honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwinhealth , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer ag , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pzer , effector therapeutics , abbvie , boehringer ingelheim ( i ) no other potential conicts of interest were reported . acknowledgment we thank bryan tutt in the department of scientic publications , the university of texas md anderson cancer center , for editorial assistance . references 33 : 2753 - 2762 , 2015 cummings ca , peters e , lacroix l , et al : the role of next - generation sequencing in enabling personalized oncology therapy . 
sci transl med 7 : 283ra53 , 2015 gray pn , vuong h , tsai p , et al : tumornext : a comprehensive tumor proling assay that incorporates high resolution copy number analysis and germline status to improve testing accuracy . 
oncotarget 7 : 68206 - 68228 , 2016 christoforides a , carpten jd , weiss gj , et al : identication of somatic mutations in cancer through bayesian - based analysis of sequenced genome pairs . 
bmc genomics 14 : 302 , 2013 green rc , berg js , grody ww , et al : acmg recommendations for reporting of incidental ndings in clinical exome and genome sequencing . 
genet med 19 : 249 - 255 , 2017 [ erratum : genet med 19 : 484 , 2017 ] robson me , bradbury ar , arun b , et al : american society of clinical oncology policy statement update : genetic and genomic testing for cancer susceptibility . j clin oncol 33 : 3660 - 3667 , 2015 10 . 
hegde m , santani a , mao r , et al : development and validation of clinical whole - exome and whole - genome sequencing for detection of germline variants in inherited disease . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
tung n , lin nu , kidd j , et al : frequency of germline mutations in 25 cancer susceptibility genes in a sequential series of patients with breast cancer . 
kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identies pathogenic germline mutations , and directs targeted therapy . 
boland g , piha - paul s , subbiah v , et al : clinical next generation sequencing to identify actionable alterations in a phase i prograoncotarget 6 : 20099 - 20110 , 37 . 
the patient declined surgery , and the centrally located rll tumor was treated with stereotactic body radiation therapy ( sbrt ) at a dose of 50 gy in five fractions . 
 six months later , the patient presented with a 3 - month history of right hip and left shoulder pain , which was a biopsy - proven recurrence of the rll primary with diffuse bony metastases . 
 the patient consented to an institutional review boardapproved protocol ( #226210 at the university of california , davis )  . tumor and germline genomic sequencing assays plasma ctdna was isolated from 10 ml of whole blood drawn in streck cell - free dna tubes , enriched by hybrid capture to target exons of 70 genes and critical introns of six genes , and sequenced to an average depth of approximately 15 , 000 on an illumina nextseq500 ( guardant360 assay ; guardant health , redwood , ca ) at a clinical laboratory improvement actcertified commercial laboratory.6 germline dna was isolated from the patients pbmcs and enriched for targeted regions using a hybridization - based protocol and was sequenced with 50 or greater depth using illumina technology at a commercial genetic testing laboratory ( invitae , san francisco , ca )  . 
 methods for in vitro studies are described in detail in the data supplement . this patients family history suggests a hereditary predisposition to lung cancer : three other individuals across three generations had a history of lung cancer ( data supplement )  . 
tumor genomic profiling of plasma ctdna with the guardant360 assay identified concurrent low ( 0.3% ) mutation allelic frequency ( maf ) of egfr l858r and high ( 51% ) maf of egfr t790m ( fig 1a - 1b )  . 
 the patient was referred to a genetic counselor , and germline dna sequencing confirmed that this patient carried a germline egfr t790m mutation . we determined the in vitro cytotoxicity of egfr tkis on this patients pbmcs using a permanent epstein barr virustransformed lymphoblastoid cell line , a good surrogate for the patients germline genomic materials , 11 , 12 established before initiation of any systemic treatment . 
we found that the lymphoblastoid cells ( fig 2a ) and the patients pbmcs ( fig 2b ) were resistant to all first - , second - , and third - generation egfr tkis tested . 
consistent with previous reports , 13 h3255 cells ( which harbored only an oncogenic egfr l858r mutation ) were sensitive to all egfr tkis ( fig 2c ) , whereas h1975 cells ( which harbored both oncogenic egfr l858r and t790m mutations ) were resistant to erlotinib but sensitive to afatinib and osimertinib ( fig 2d )  . 
we found that the patients pbmcs and pbmc - derived cells did not express egfr and akt protein , the two key signaling molecules that mediate the downstream oncogenic signaling pathways in h3255 and h1975 cells , by western blots ( fig 2e )  . 
we also confirmed that there was no egfr mrna expression in patients pbmcs or in the patient - derived ebv - transformed lymphoblastoid cell line ( data supplement )  . 
thus , afatinib and osimertinib could be used safely in this patient with a germline egfr t790 mutation . during the in vitro studies , the patient first received palliative radiation for the right hip pa he had stable disease after first - line combination chemotherapy with carboplatin , pemetrexed , and bevacizumab for four cycles , and he experienced tumor progression at the primary rll and metastatic bony lesions after maintenance treatment with pemetrexed and bevacizumab for four cycles . 
a restaging positron emission tomography ( pet ) / ct scan 2 months after afatinib treatment began revealed extensive tumor progression in the primary rll tumor and multiple bone metastases . 
serial guardant360 assays revealed that the changes in the maf of egfr l858r in plasma ctdna correlated with the tumor responses to chemotherapy , afatinib , and osimertinib ; the maf of egfr t790m remained at approximately 50% ( fig 1a - 1b )  . 
time points ( ie , dates ) were selected on the basis of radiographic assessments at baseline and after each treatment according to recist version 1.1 during the entire disease course . 
targeted ngs of malignant cells in pleural effusion by foundationone ( foundation medicine , cambridge , ma ) revealed multiple genomic alterations , including egfr l858r and t790m ( fig 1c )  . 
similar to plasma ctdna analysis , egfr genotyping of the patients tumor dna by droplet digital polymerase chain reaction revealed that the maf of egfr l858r in tumor dna increased with tumor progression , whereas the maf of egfr t790m remained at approximately 60% ( fig 1c )  . 
the patient did not tolerate subsequent treatment on a clinical trial and died on hospice approximately 3 months later . discussion routine clinical application of multiplex tumor genomic profiling has increased the detection rate of rare germline mutations that may affect the patients clinical care and that raise concerns for cancer risks in family carriers.15 , 16 the maf of a somatic mutation in the plasma ctdna is usually much lower than that of archived tumor dna , whereas the maf of germline egfr t790m remains at 50% to 60% in plasma ctdna and tumor dna . 
results from the inherit study ( nct01754025 ) , which provided free genetic counseling and tested for lung cancer in patients and family members with an egfr t790m mutation at diagnosis and at longitudinal surveillance with serial ct scans , 17 are highly anticipated . patients with lung cancer who have a germline egfr t790m usually harbor a distinct spectrum of one or more concurrent oncogenic egfr mutations ( data supplement )  . 
the median progression - free survival was 4.9 months in the pooled analysis of patients ( the data supplement ) , whereas the median progression - free survival was 9 to 13 months in patients with egfr tkisensitive somatic egfr mutations.18 furthermore , data from our patient and the patients in the data supplement also revealed less clinical benefit from chemotherapy and radiation , which suggests tumor resistance to these standard therapeutic strategies . 
stollenwerk , tianhong li provision of study material or patients : debbie lewis , yanhong zhang , jamie hung , jenna welborn , tianhong li data analysis and interpretation : weijie ma , jidong shan , wenwu xiao , yanhong zhang , sixi wei , kit s . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . weijie ma no relationship to disclose jay gong no relationship to disclose jidong shan no relationship to disclose debbie lewis no relationship to disclose wenwu xiao no relationship to disclose elizabeth h . 
moore no relationship to disclose yanhong zhang no relationship to disclose jamie hung no relationship to disclose patents , royalties , other intellectual property : patent for device and method for assessing beam quality in computed tomography by measuring the half - value layer ( inst ) sixi wei no relationship to disclose jeanna welborn no relationship to disclose nicholas s . 
lam leadership : lamnotherapeutics stock and other ownership interests : lamnotherapeutics , lp therapeutics , cardioprobe patents , royalties , other intellectual property : i have more than 20 issued patents , many with the university of california , davis ( no royalty received in the past 2 years )  . tianhong li consulting or advisory role : foundation medicine , takeda , puma research funding : foundation medicine ( inst ) , pfizer ( inst ) , astrazeneca ( inst ) , hengrui ( inst ) acknowledgment we dedicate this work to the late jeannine h . 
mans stock and other ownership interests : concert pharmaceuticals , corcept therapeutics , varex imaging , verasterm , ziopharm oncology affiliations weijie ma , jay gong , wenwu xiao , elizabeth h . 
3 - ( 4 , 5 - dimethylthiazol - 2 - yl ) - 5 - ( 3 - carboxymethoxyphenyl ) - 2 - ( 4 - sulfophenyl ) - 2h - tetrazolium assay for ebv - transformed lymphoblastoid cell line established from ( a ) this patient , ( b ) the patients pbmcs , ( c ) h3255 , and ( d ) h1975 . 
 ( e ) the expression of egfr and downstream signaling molecules in the ebv - transformed lymphoblastoid cells and pbmcs from this patient , h3255 , and h1975 are shown . 
mulloy r , ferrand a , kim y , et al : epidermal growth factor receptor mutants from human lung cancers exhibit enhanced catalytic activity and increased sensitivity to gefitinib . 
lanman rb , mortimer sa , zill oa , et al : analytical and clinical validation of a digital sequencing panel for quantitative , highly accurate evaluation of cell - free circulating tumor dna . 
ancevski hunter k , friedland dm , villaruz lc , et al : first - line osimertinib in patients with treatment - naive somatic or germline egfr t790m - mutant metastatic nsclc . 
hussain t , kotnis a , sarin r , et al : establishment and characterization of lymphoblastoid cell lines from patients with multiple primary neoplasms in the upper aero - digestive tract & healthy individuals . 
li d , shimamura t , ji h , et al : bronchial and peripheral murine lung carcinomas induced by t790m - l858r mutant egfr respond to hki - 272 and rapamycin combination therapy . 
meric - bernstam f , brusco l , daniels m , et al : incidental germline variants in 1 , 000 advanced cancers on a prospective somatic genomic profiling protocol . 
hu y , alden rs , odegaard ji , et al : discrimination of germline egfr t790m mutations in plasma cell - free dna allows study of prevalence across 31 , 414 cancer patients . 
oxnard gr , heng jc , root ej , et al : initial results of a prospective , multicenter trial to study inherited lung cancer risk associated with germline egfr t790m : inherit egfr . 
kris mg , natale rb , herbst rs , et al : efficacy of gefitinib , an inhibitor of the epidermal growth factor receptor tyrosine kinase , in symptomatic patients with non - small cell lung cancer : a randomized trial . 
 oncologists use of genomic sequencing data to inform clinical management purpose to determine whether oncologists intended to change treatment as a result of tumor sequencing , and subsequently , whether patients experienced an alteration of clinical management or derived clinical benefit . patients and methods a prospective survey of oncologists referring adult patients with rare , advanced , or refractory cancer to the michigan oncology sequencing program was conducted from june 2014 to march 2015 to assess the use of and intent to disclose sequencing findings . 
medical records were reviewed retrospectively to determine if clinical management was informed or changed by sequencing results . results oncologists ( response rate , 93% ) referring 112 consecutive patients were surveyed . 
2018 by american society of clinical oncology introduction clinical implementation of tumor genomic sequencing is emerging as a promising strategy to improve patient outcomes in oncology.1 integrating an individuals clinical history with genomic data can inform both diagnostic and treatment strategies , potentially suggesting therapies that are tailored to the patients tumor mutational landscape.2 there are several ongoing national efforts to evaluate the effectiveness of treating cancers with targeted therapies informed by alterations in patients tumors . 
the national cancer institute 's molecular analysis for therapy choice ( match ) is a basket study matching patients with metastatic solid tumor malignancies to food and drug administrationapproved or experimental drugs on the basis of specific tumor alterations.3 the tumor agent and profiling utilization registry study ( tapur ) , sponsored by asco , matches patients to commercially available targeted antineoplastic agents on the basis of potentially actionable tumor events.4 the initiative for molecular profiling in advanced cancer therapy ( impact ) program in the phase i clinic at md anderson cancer center matches targeted agents with tumor molecular alterations in patients with advanced cancer.5 evaluating the evidence for improved outcomes for patients with cancer matched to targeted agents is an essential first step . 
scott roberts author affiliations and support information ( if applicable ) appear at the end of this article . the study funders had no role in the design of the study ; the collection , analysis , or interpretation of the data ; the writing of the manuscript ; or the decision to submit the manuscript for publication . corresponding author : michele c . 
furthermore , there is debate among medical professionals about what should be considered clinically actionable and what types of findings from clinical sequencing should be disclosed to patients.6 - 12 still , it is common for studies that use sequencing results to match patients with targeted therapy to report the frequency of actionable results.13 however , few report what percentages of these actionable results were eventually acted on in clinical practice . currently , most commercially available tumor testing platforms focus on targetable alterations in a limited set of genes . 
in contrast , the michigan oncology sequencing ( mi - oncoseq ) program has adopted a more comprehensive approach by sequencing the genome , exome , and transcriptome of tumors , as well as a matched normal sample , in an effort to characterize novel variants that may increase cancer risk . 
 this has led to the identification of alterations with important clinical implications , such as the activation of esr1 mutations in patients with estrogen receptor - positive metastatic breast cancer refractory to hormonal therapies , implicating these mutations as a likely mechanism of resistance to endocrine therapy.3 furthermore , novel fibroblast growth factor receptor fusions , potentially targetable with fibroblast growth factor receptor inhibitors currently being studied in clinical trials , have been identified across a diverse range of cancer types.4 these discoveries highlight how taking a comprehensive approach to identifying therapeutic targets for individual patients with cancer can expand the molecular taxonomy of cancer . 
to address whether oncologists are using sequencing findings to change a patients clinical management , and to what extent potentially actionable findings are being acted on , we surveyed oncologists referring patients with rare , advanced , or refractory cancer to the mi - oncoseq program , a precision oncology research study at university of michigan comprehensive cancer center.14 we also examined whether there was concordance between an oncologists intention to disclose the finding and the referred patients perception of a disclosure of results . 
detailed information on the program , including patient eligibility criteria , have been reported previously.14 results were generated within approximately 6 to 8 weeks , and potentially actionable findings were discussed at an institutional precision medicine tumor board ( pmtb ) composed of members with expertise in medical oncology , hematology , clinical pathology , cancer genetics and genetic counseling , bioinformatics , and bioethics . 
the mi - oncoseq program received institutional review board approval from the university of michigan . framework for classification of genomic alterations to determine the clinical relevance or potential actionability of comprehensive sequencing results , the study team developed a post hoc clinical tiering system to allow for a uniform and scalable approach for classifying alterations for research purposes ( table 1 )  . tier 1 alterations represent the highest level of clinical evidence and are generally incorporated into national comprehensive cancer net work guidelinebased recommendations for the treatment of malignancies . 
this includes food and drug administrationapproved therapies in the context of a molecular biomarker that predicts therapeutic response to a drug , pathogenic germline alterations conferring increased cancer risk , or sequencing information that contributed to a change in cancer diagnosis for tumors of unknown primary orig tier 2 alterations represent the identification of molecular alterations that meet the enrollment criteria for a clinical trial or registry study of a targeted therapeutic agent . 
potentially actionable genomic alteration classification tier 1 approved biomarker predictive of therapeutic response to an approved drug in that disease for example : brafv600e mutation , vemurafenib , melanoma germline alteration conferring increased cancer risk for example : pathogenic germline brca1 alteration change in cancer diagnosis for example : cup determined to be nsclc tier 2 rationale for enrollment in a clinical trial or registry study ( tapur ) for example : fgfr2 fusion in cholangiocarcinoma , fgfr inhibitor bgj398 tier 3 a . 
alteration in known oncogene or tumor suppressor for example : apc mutation abbreviations : cup , carcinoma of unknown primary ; fgfr , fibroblast growth factor receptor ; nsclc , nonsmall - cell lung cancer ; tapur , tumor agent and profiling utilization registry study ; vegfr , vascular endothelial growth factor receptor . particular molecular alteration with regard to tumor pathogenesis , but are not considered to be clinically actionable . oncologist survey after receiving the pmtb report , oncologists were surveyed about their intended use of sequencing information . 
each oncologist received a survey for every patient he or she referred during the 9 - month period , and therefore , the same oncologist may have completed multiple surveys . 
for example , oncologists were asked , will you make any changes to this patients cancer treatment based on pmtb and / or the mi - oncoseq report ? ( response options were yes , no , not sure . ) if the oncologist selected yes , he or she was asked , what changes will you make ? if the oncologist endorsed no or not sure , he or she was asked , what is your reasoning for not making any changes ? additional items asked about intention to disclose the findings to patients as well as how and when this communication would occur . 
 patient surveys patients enrolled in the mi - oncoseq program were administered surveys after they consented to participate in the study and after the referring oncologist received the pmtb report . 
 at baseline , a 23 - item survey assessed patients knowledge and expectations regarding genomic sequencing , including beliefs about incidental findings , and preference for the return of results . 
 a follow - up survey mailed approximately 2 weeks after the referring oncologist received the results assessed patients fulfillment of expectations , decisional regret , satisfaction with results , and behavioral changes . concordance between oncologist and patient responses to assess gaps in the communication process , we compared items about an oncologists intention to disclose the sequencing results with the patients recollection of a results disclosure discussion . 
 specifically , will you share the genetic sequencing results with this patient ? ( response options were yes , no , not sure . ) similarly , in their follow - up survey , patients were asked , since you began participating in this research study , has your doctor ( s ) discussed one or more of your genome sequencing test results with you ? ( response options were yes , no , not sure . ) next , we conducted a content analysis of patients medical records to find documentation of a disclosure discussion . 
outcomes assessed included whether treatment was altered on the basis of results , the type of treatment or change in management , and the identification of a germline alteration with implications for management of patient or family member care ( eg , cascade testing )  . data analysis descriptive data , including frequencies and percentages , were calculated for demographic variables and responses to the survey questions for both the referring oncologists and the patients . 
whether survey participants characteristics and responses predicted intention to change clinical management and report of a results discussion were compared using fishers exact tests for categorical variables for low cell counts . 
all analyses were conducted using spss version 22 ( spss , chicago , il )  . results oncologist and patient surveys forty - three oncologists referring 112 patients to the mi - oncoseq study between june 2014 and march 2015 completed the survey ( response rate , 93% )  . 
approximately one half ( 52% ) of the oncologists surveyed referred three or more patients ( median , two patients ; range , one to 12 patients )  . of the 112 patients , the mean age was 57 years ( sd , 12.7 years ) , 51.8% were female , 94.6% self - reported as being white , and 32.1% were college graduates ( table 2 )  . 
the oncologists had no plans to change the treatment of 51% of patients ( n = 60 ) , or were not sure if they were going to make any treatment changes for 28 patients . 
 the most frequently endorsed reasons for not changing clinical management were a lack of locally available trials offering therapies relevant to the findings ( 59% ) , findings not actionable ( ie , not enough clinical evidence or results not clinically significant ; 27.4% ) , and the effectiveness of a patients current treatment ( 12% )  . regardless of an intention to change treatment , oncologists intended to share sequencing results with 94 of the 112 patients ( 84% )  . 
several indicated that they would disclose results by telephone ( 20% ) or before the patients next visit ( 24% )  . intention to change treatment and the mode of communication of findings were stratified by the median number of patients referred and the patient diagnosis . 
no variables significantly predicted intention to change treatment ( fig 1 )  . concordance between oncologist and patient responses of the 94 patients for whom an oncologist intended to share results , 57 completed the follow - up survey . 
oncologist and patient survey respondent characteristics respondent year medical training completed , median ( range ) 1993 ( 1969 - 2013 ) hematology and medical oncology oncologist primarily sees patients at an academic medical center no . 
 ( % ) unless indicated otherwise . * includes physicians referring patients to the study between june 2014 and february 2015 ; 94% response rate . and a documented note in their medical record supported their response . 
controlling for referring oncologist or cancer type did not significantly predict report of a results discussion . actionability classification of tumor genomic alterations , and patient outcomes on the basis of the retrospective chart review , nine of 24 patients had actual changes in clinical management informed by sequencing results . 
 on the basis of a review of medical records , these reasons included patient barriers ( eg , unable to travel to referred trial ) , insurance or cost ( eg , phase i clinical trial not covered ) , ineligibility for an identified study ( eg , impaired liver or renal function ) , and loss to follow - up or patient deceased . discussion comprehensive genomic sequencing offers the opportunity to characterize somatic and germline alterations for patients who have exhausted standard therapies and to potentially inform patients of additional treatment options . 
in this study , we found that oncologists reported intentions to make changes to treatment on the basis of genomic findings for 24 of 112 patients with rare or refractory cancers . 
these findings demonstrate both the potential benefit that can result from taking a comprehensive approach to identify targeted therapies tailored to a patients mutational landscape and the barriers to implementation of tumor - related genomic results into clinical management . 
significant obstacles include , but are not limited to , the need for additional educational support for both clinicians and patients , the need to define what constitutes an actionable finding , lack of access to clinical trials and off label therapies , and the need for future research to develop improved patient - provider communication mechanisms . our findings are consistent with those of other studies that have reported notable barriers to the integration of sequencing results into clinical practice.15 , 16 we found several instances that suggested a need for educational resources to support both the patient and the clinician . 
 example , patients with advanced or rare disease , such as the patients in this study , often join multiple research studies , go through multiple treatments regimens in a brief timeframe , and meet with several providers . 
it is reasonable that patients might not remember the specific study being discussed , be fatigued from treatments and appointments , or be confused by complex medical terminology . defining what constitutes an actionable finding is often challenging when multiple stakeholders are involved . 
of cases ( n = 112 ) abbreviations : cmml , chronic myelomonocytic leukemia ; dlbcl , diffuse large b - cell lymphoma ; nsclc , nonsmall - cell lung cancer ; scc , squamous cell carcinoma . the need for improved and better - designed test reports . discordance between an oncologist and a patients perceptions of a disclosure of results suggests the need for improvements in patient provider communication as a point of intervention . 
for referred to mi - oncoseq ( n = 122 ) completed survey ( n = 112 ) planned to share results with patients ( n = 94 ) did not plan or unsure of plan to share results with patients ( n = 18 ) completed follow - up survey ( n = 57 ) loss to follow - up ( n = 19 ) deceased or hospice ( n = 18 ) completed follow - up survey ( n = 7 ) loss to follow - up ( n = 4 ) deceased or hospice ( n = 7 ) had a discussion with physician ( n = 23 ) did not have a discussion with physician ( n = 34 ) had a discussion with physician ( n = 1 ) did not have a discussion with physician ( n = 6 ) medical chart review ( n = 57 ) documented disclosure discussion ( n = 14 ) discussion after follow up survey ( n = 5 ) no documentation of disclosure ( n = 15 ) ascopubs.org / journal / po jco precision oncology 7 fig 1 . 
 actionable can mean different things to different individuals on the care tea therefore , establishing a clear framework for defining actionable findings is critical to the implementation of comprehensive genomic sequencing information in clinical management . 
our attempt to address this barrier was the tiering scalable framework for classification of alterations to be implemented in future test reports . other prominent barriers patients and oncologists faced included uncertainty about locally available clinical trials and the lack of access to off - label therapies . 
these barriers include a lack of information about existing trials and therapies , a lack of resources to identify trial eligibility , inability to obtain approval for compassionate use for off - label drugs , and logistical challenges for the patient ( travel , lack of insurance coverage , or financial constraints )  . our study sample is not representative of oncologists in general given its over - representation of practitioners in an academic medical center . 
in addition , because medical record information is not always complete and may not accurately capture the existence or nature of discussions with patients , the verification of disclosures and outcomes was limited to a subset of individuals . 
le no relationship to disclose natalie bartnik no relationship to disclose elena stoffel research funding : cancer prevention pharmaceuticals ( inst ) scott schuetze consulting or advisory role : emd serono , janssen pharmaceuticals , daiichi sankyo research funding : ab science ( inst ) , janssen pharmaceuticals ( inst ) , amgen ( inst ) , biomed valley discoveries ( inst ) , cytrx ( inst ) , plexxikon ( inst ) , eli lilly ( inst ) , karyopharm therapeutics ( inst ) , adaptimmune ( inst ) moshe talpaz consulting or advisory role : gilead sciences , cti biopharma , nynex research funding : gilead sciences , incyte , cti biopharma , ariad pharmaceuticals , novartis , aptose biosciences , pfizer , sanofi expert testimony : bristol - myers squibb canada arul chinnaiyan consulting or advisory role : tempus j . 
tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
scheuner mt , peredo j , benkendorf j , et al : reporting genomic secondary findings : acmg members weigh genet med 17 : 27 - 35 , 2015 7 . 
brandt ds , shinkunas l , hillis sl , et al : a closer look at the recommended criteria for disclosing genetic results : perspectives of medical genetic specialists , genomic researchers , and institutional review board chairs . 
townsend a , adam s , birch ph , et al : i want to know whats in pandoras box : comparing stakeholder perspectives on incidental findings in clinical whole genomic sequencing . 
middleton a , morley ki , bragin e , et al : attitudes of nearly 7000 health professionals , genomic researchers and publics toward the return of incidental results from sequencing research . 
although survival from any pediatric cancer has improved dramatically during past decades , a number of cancers continue to yield dismal prognoses , which has motivated the continued study of novel therapeutic strategies . 
furthermore , even patients cured of pediatric cancer often experience severe adverse effects of treatment and other long - term health implications , such as cardiotoxicity or loss of fertility . 
fortunately , pediatric cancers are rare overall , but even among patients with the same narrow cancer type , there is often broad heterogeneity in terms of prognosis , molecular features or pathology , current treatment strategies , and scientic objectives . 
as a result , the design of clinical trials in the pediatric cancer setting is challenged by a number of practical issues that must be addressed to ensure trial feasibility for this vulnerable group of patients . 
in this review , we discuss some of the unique trial design considerations often encountered in any rare tumor setting through the lens of our experiences as faculty statisticians for the childrens oncology group , the largest organization in the world dedicated exclusively to pediatric cancer research and clinical trials . these topics include risk stratication within individual trials , relaxation of trial operating characteristics and parameters , use of historical controls , and address of noninferiority - type objectives in small cohorts . 
2019 by american society of clinical oncology introduction overview of pediatric cancer and current directions in the united states , cancer remains the leading cause of disease - related death in children.1 , 2 although the prognosis for most pediatric patients has improved dramatically during the past several decades to achieve an overall 5 - year survival rate of 84% , pediatric cancer truly comprises many heterogenous diseases with a great deal of variability in expected survival outcomes and current scientic objectives.3 , 4 among the childhood cancer types with the best prognosis ( thanks in large part to decades of therapeutic intensication trials for improved survival ) , achievement of an incremental improvement upon current outcomes remains a key objective of most pediatric trials alongside objectives and novel treatment strategies intended to minimize short - term treatment - related toxicities and improve longer - term considerations , such as fertility , cardiac health , and quality of life.5 - 9 for other childhood cancers , such as acute myelogenous leukemia , high - risk neuroblastoma , and brainstem glioma , progress has been more limited , with 50% or more patients eventually succumbing to their disease . 
in those diseases , the study of novel therapeutic strategies to improve overall survival ( os ) remains the highest priority.10 , 11 role of the childrens oncology group the childrens oncology group ( cog ) , a member of the national clinical trials network supported by the national cancer institute , is the worlds largest organization devoted exclusively to childhood and adolescent cancer research . 
the current organizational structure of cog was established in the year 2000 as the result of a voluntary merger of its four predecessor groups : the childrens cancer study group ( ccg ) , pediatric oncology group ( pog ) , intergroup rhabdomyosarcoma study group , and national wilms tumor study group . 
more than 90% of the 14 , 000 children and adolescents newly diagnosed with cancer each year in the united states are cared for at cog these member institutions , with more than half of patients historically enrolling in cog therapeutic clinical trials . 
 renfro et al context challenges . key objective clinical trials in pediatric cancer and other rare diseases often include unique statistical features or design knowledge generated in the pediatric setting , common design components include use of prognostic risk stratication and use of data from historical controls . 
statistical challenges include maintaining power or addressing noninferiority - type hypotheses when only a limited population of patients is available to enroll . relevance we provide an overview of these features and challenges and describe existing approaches in the literature as well as those used in example trials from the childrens oncology group . active follow - up in cog studies at more than 220 leading childrens hospitals , universities , and cancer centers across the united states , canada , australia , and new zealand . pediatric cancer as a rare disease with trial planning implications fortunately , even the most common pediatric cancers occur only rarely in the general population , representing only 1% of new cancer diagnoses in the united states.12 also fortunate is the current availability of effective therapies for most of these patients . 
however , both the rarity of pediatric cancers and their generally favorable outcomes present unique challenges to clinical trial design , where improving outcomes and lessening the burden of treatment remain critically important . in some pediatric malignancies , it is not feasible to conduct a randomized phase iii clinical trial to detect a modest , yet clinically relevant improvement in outcome with high statistical power and a low type i error rate . 
furthermore , with targeted therapies now increasingly regarded as promising treatment strategies for patients whose tumors harbor particular molecular features or mutations , the already small disease populations that currently comprise pediatric cancer are becoming even smaller as a result of additional molecular characterization , thereby exacerbating some of the usual trial design challenges inherent in any rare disease . 
in addition , for those pediatric cancer subtypes where exceptional prognosis or cure can now reasonably be expected with standard treatment , current and future trials likely will be designed to answer questions such as whether historically toxic treatments can be safely reduced or altered in some way without negatively affecting outcomes . these next - generation questions , although important to answer , generally necessitate noninferiority ( ni ) - type trial design , which on average , requires a far greater sample size than a traditional phase iii randomized trial . in this article , we highlight several trial design features and challenges that are common to pediatric cancer trials and , in some cases , are broadly applicable to trials for any rare cancer . 
these include risk stratication as a design component , relaxation of trial operating characteristics to maintain feasibility , alternative approaches to testing nitype hypotheses , and use of historical controls . 
these risk groups might be derived from a number of patient and disease factors , such as age of the patient , size or local stage of the tumor , tumor histology , molecular biomarkers , or other features that have been previously shown to predict patients natural course of disease or response to standard treatments . 
in most cog trials where upfront risk stratication takes place , patients assigned to different strata ( eg , low risk , intermediate risk , high risk ) will go on to receive ( or be randomly assigned to ) treatment strategies of increasing intensity , depending on the severity of their initial risk assignment . 
in some pediatric cancer types , therapeutic deintensication is the main objective for those known to be at low or very low risk of adverse outcomes , such as disease recurrence or progression . challenges for risk stratication in rare diseases although risk stratication offers a logical and feasible approach to studying prognostically different cancer stages or subtypes under a unied protocol , this practice presents some challenges . 
first , it is common in pediatric cancers for stratum - specic risk classications to change over time because knowledge of the individual diseases and their corresponding standard treatments continue to evolve . 
 trial design for precision oncology in rare tumors group of patients considered to be very low risk during one era of treatment trials of a given cancer might be redened to become more inclusive in the next era , whereas discovery of a new negatively prognostic biomarker present across all risk groups might add a layer of upstaging from lowerto higher - risk groups across the board . 
another challenge of risk stratication is that introduction of a new risk factor or threshold to distinguish lower - risk from higher - risk patients might be based on limited patient numbers or incomplete clinical evidence ( eg , a biomarker collected for only a subset of patients ) , which precludes a statistically rigorous evaluation of the risk classication system in question and leaves much to the discretion and instincts of study investigators . 
even the methodology originally used to determine that a particular patient or disease feature is sufciently prognostic to map a patient to a different risk level ( and thus treatment assignment ) , such as whether a patients age is above or below some threshold at the time of diagnosis , might be questioned or re - evaluated after more data become available . 
modications , updates , or other inconsistencies between risk classications from one generation of trials to the next within a single disease type can lead to challenges in dening risk groupspecic historical controls when planning the next generation of trials , particularly when available cohorts of reference patients are already small or systematically different in some other way ( historical controls will be discussed subsequently in this article )  . nonetheless , risk stratication remains central to many pediatric cancers , and thus , the development of optimal approaches for risk stratication in clinical trials remains of critical interest to cog researchers . examples of risk stratication in cog trials hepatoblastoma . 
on the basis of these ndings , cog opened the hepatoblastoma studies int - 009815 in 1989 and p964516 in 1999 , using resectability at exploratory surgery and histology information to dene a risk stratication framework . 
in the early 2000s , the radiologybased pretreatment extent of disease ( pretext ) staging factor in risk stratication system became a dominant because exploratory surgery was no longer routinely supported with the advent of advanced radiographic imaging techniques . 
in 2009 , cog opened a new hepatoblastoma study , ahep0731 that ( clinicaltrials.gov identier : nct00980460 ) , that incorporated pretext and - fetoprotein in the risk stratication . as noted previously , the performance of direct comparisons of patient outcomes from trials or groups that use dissimilar risk classication strategies is challenging , and such was the case in hepatoblastoma . 
to address this issue , the childhood hepatic tumor international consortium established a database that consists of 1 , 605 patients from eight prior studies from cog , the international childhood liver tumors strategy group , the german society for pediatric oncology and haematology , and the japanese study group for pediatric liver tumors.17 the goal was to develop a common risk stratication system for pediatric hepatic tumors . 
figure 1 illustrates the details of this new risk stratication tool , which has been implemented in the pediatric hepatic malignancy international therapeutic trial ( phitt ) with participants from cog , the international childhood liver tumors strategy group , and the japanese study group for pediatric liver tumors . 
acute lymphoblastic leukemia ( all ) is the most common cancer diagnosed in children , with an estimated 3 , 500 diagnoses per year in persons younger than 20 years of age in the united states.18 in the current era , overall cure rates for children with newly diagnosed all are approaching 85%.19 although survival gains during the past four decades are noteworthy , many children predicted to be at low risk of relapse at initial diagnosis ultimately experience treatment failure . 
all other patients were classied as nci standard risk . yes is dened as the presence of double trisomy 4 and 10 or etv6 - runx1 fusion . consists of patients with cns3 , hypodiploidy ( , 44 chromosomes and / or dna index , 0.81 ) , intrachromosomal amplication of chromosome 21 , induction failure ( m3 marrow day 29 ) , or kmt2a ( mll ) rearrangement ( not kmt2a deletion )  . 
bcr - abl1positive patients are eligible for a separate , dedicated philadelphia chromosomepositive acute lymphoblastic leukemia study , aall1122 or aall1631 ( if open )  . includes four nci standard - risk and high - risk patients with testicular disease . group classication protocol aall03b1 , formed the basis for the renement of the risk stratication algorithm subsequently used in aall08b1 . initial registration and risk stratication in after aall08b1 , patients could be deemed eligible for a cog frontline all treatment trial as follows . 
additional studies performed at local and cog reference laboratories at the time of initial diagnosis and at dened time points during induction were used to rene postinduction therapy . patients with national cancer institute standard - risk and high - risk20 b - lymphoblastic leukemia ( b - all ) 21 were then distributed among the following four risk groups after induction : low risk , average risk , high risk , and very high risk ( table 1 )  . 
although a welcome problem is that children with cancer are living longer than ever before , a lower event rate within a given disease setting directly reduces the statistical power of a clinical trial , unless the sample size is increased ( which may or may not be feasible )  . 
during the past 50 years , the 5 - year survival rate for pediatric cancers has risen dramatically from 10% to 83% , which makes future clinical trials in pediatric cancers more challenging to design.24 , 25 taking standard - risk all as an example , the cure rate is 90% or greater for children in the general population.26 yet another challenge in rare and pediatric cancers is the advent of stratied or precision medicine , with an everincreasing number of new targeted therapies available for testing within narrowly dened risk - stratied or molecularly dened cohorts . 
even among pediatric cancers with the highest incidence rates ( eg , all , which accounts for approximately 30% of all cancers in children ) , most trials are conducted within far - smaller cohorts dened by risk stratication systems wherein a given risk stratum has unique objectives and possible treatment assignments , as described in the risk stratication section . 
 renfro et al a setting , even a common cancer usually is studied as a series of essentially independent , smaller trials and is therefore subject to many of the same design challenges as rarer cancers.27 , 28 when layered upon the general rare cancer issues previously described , precision medicine creates an additional urgency at the design stage to strike a balance between what is statistically rigorous and what is acceptable to support feasibility . rationale for relaxing operating characteristics / design parameters and common approaches under current conventions , a typical two - arm randomized phase iii clinical trial that tests a superiority hypothesis often uses a two - sided 5% type i error rate ( which corresponds to a one - sided 2.5% type i error rate ) and power in the range of 80% to 90% to detect a clinically relevant difference in outcome between treatment arms . 
for example , assuming a cancer with a baseline cure rate of 50% where improvement to 65% cure is desired but only 40 patients per year will likely enroll , a two - arm randomized trial would require the recruitment of 360 patients accrued during 9 years to detect the desired improvement with 80% power and a 5% type i error rate.23 in pediatric cancer , an accrual rate of 20 to 50 patients per year is common , such as in the setting of risk - stratied relapsed all . 
although a prolonged trial achieves the typical type i and type ii error rates and increases our condence in the conclusions we obtain from a completed trial , it limits the number of trials we can conduct in the long run and reduces the number of new treatment strategies or agents that we can test . 
in addition , a treatment can become irrelevant after a long duration , and a long trial can become obsolete before it completed.23 , 29 therefore , other designs are considered for clinical trials in small populations.30 at cog and in other groups that study rare diseases , a number of approaches commonly are used to minimize the overall sample size required for a trial and are subject to context - specic constraints . 
when the enrollment in a trial is not sufcient to achieve the sample size that an ideal design would require , one option is to target a larger effect size than the smallest effect that would be clinically relevant ( eg , to detect a hazard ratio [ hr ] of 0.60 [ 40% risk reduction ] rather than a more modest hr of 0.80 [ 20% risk reduction ] )  . 
in doing so , the required trial sample size is reduced as one raises the bar of the expected treatment benet under the alternative hypothesis.27 , 31 - 37 particularly in low - incidence cancer settings where only one novel therapy can be studied at a time ( to avoid splitting the population between competing trials ) , it can be reasonable to power a trial to detect a large treatment effect so long as such an effect is believed to be feasible given the type of treatment under study and the intended population.34 when the cohort to be studied is so small as to preclude formal hypothesis testing , a primary objective may instead be to enroll as many patients as possible within a given time frame and estimate the outcomes of interest ( eg , efs at 3 years )  . 
another sample size reduction approach particularly common in phase ii and some phase iii trials is a relaxation ( an increase ) of the maximum allowable rate of type i error or the probability of a false - positive result.23 , 27 - 29 , 33 - 35 , 38 , 39 a conventional rule of thumb for many clinical studies ( not just clinical trials ) is to specify a two - sided type i error rate of 5% to control the probability false - positive results when the null hypothesis ( no treatment effect ) is true . 
a third approach to reducing sample size ( albeit less common at cog ) is to relax or decrease the amount of power or probability with which the targeted effect size will be detected if it is true ( a power less than 80% usually is not considered )  . 
although each of these adjustments comes with some corresponding statistical sacrice , a compromise among the three objectives of low type i error , high power , and a reasonable targeted effect is often possible and straightforward to implement ; thus , these approaches remain popular in rare disease settings.23 , 27 - 39 guidance for relaxing operating characteristics and trial parameters . 
when trials include most of the patients in the target population , sposto and stram23 investigated the relationship between type i error , sample size , trial duration , patient accrual rate , and therapeutic innovation rate and the increase in treatment efcacy achieved after a series of two - treatment randomized phase iii trials . 
they proposed that a more appropriate view of trial design in lowincidence cancer settings is in the overall context of the research setting and long - term goals rather than in the narrow context of the current single trial . ( p1183 ) sposto and stram concluded that judicious choice of type i error and accrual duration will result in a larger average gain in treatment efcacy as measured by improvements in cure rates over the long term , especially in low - incidence disease , than would use of small type i error and high power for small differences . 
strauss and simon29 considered the optimum allocation of patient resources to maximize success rates in a phase ii context and had similar conclusions ( ie , more frequent , smaller trials are warranted in settings where patient resources are limited )  . 
these articles support the notion that performance of a series of small trials with relaxed operating characteristics over a long - term research horizon leads ( on average ) to larger survival benets . 
an optimal choice of design parameters can be selected to maximize the expected total survival benet by considering factors such as accrual rate , therapeutic innovation rate , and disease severity.23 , 28 , 39 despite the justications , the targeting of a larger effect size or relaxing of type i error has some disadvantages . 
targeting a larger effect size with the type ii error rate of 20% could lead to underpowered studies for new treatments associated with smaller , but still clinically meaningful benets and , hence , increases the risk of missing a moderate or small treatment effect.31 , 33 use of larger type i error rates and / or shorter trials is associated with worse apparent treatment efcacy in the long term and an increased likelihood of ultimately selecting an inferior treatment compared with standard larger trials with lower type i error , 23 and increasing type i error ( one - sided ) above 20% generally is not recommended.23 , 28 , 39 examples of relaxed design constraints and solutions from cog trials at cog , many phase ii and some phase iii randomized studies were designed with relaxed type i error rates ( onesided 5% , 10% , or 15% ) or were powered to target a larger effect size with a reduced statistical power of 80% . 
table 2 lists some of these trials and includes their specic objectives and operating characteristics as examples . among these is the study design for low - risk patients with relapsed b - all enrolled in the cog trial aall1331 ( clinicaltrials.gov identier : nct02101853 )  . 
the cohortspecic objective was to compare disease - free survival ( dfs ) between patients randomly assigned to chemotherapy alone ( control arm ) or chemotherapy plus blinatumomab ( a bispecic single - chain antibody that targets the cd19 antigen ) after re - induction . 
the corresponding study was designed to have 80% power to detect an hr of 0.55 using a log - rank test with 5% one - sided type i error , which corresponds to an increase in the 3 - year dfs rate from 73% in the control arm to 84% in the experimental arthe b - all cohort was expected to accrue during 5.6 years to reach 206 eligible patients , with the analysis requiring 3 years of additional follow - up after completion of enrollment . 
common objectives in randomized pediatric oncology trials include the comparison of drug combinations , altered doses , or adjuvant therapies against standard therapeutic backbones , with trials powered to detect improved outcomes in the experimental arms versus the control aralso common in pediatric trials are situations where the goal is not to prove superiority but to show that a new experimental therapy is not statistically inferior to an active control or standard of care and retains most ( if not all ) of the controls therapeutic benet . 
in this case , factors such as potential improvements in safety , tolerability , cost , convenience , availability , or other secondary factors are used to justify the study of the experimental regimen . 
despite their relevance in situations such as those just described , ni trials are often more challenging to design than superiority trials , and a number of factors must be considered during the planning stages to ensure a feasible trial capable of answering the ni - type question of interest.41 , 42 planning and design considerations for ni trials overview of randomized ni designs using time - to - event end points . 
as such , the results presented usually include a signicance test for differences between groups ( eg , a log - rank test ) and a numerical summary of that difference ( eg , the hr estimated from a cox proportional hazards regression model )  . 
in the randomized ni trial setting with a time - to - event outcome , however , interest lies in determining whether the estimated hr and its ci fall in such a region that inferiority of the experimental arm can be statistically ruled out . 
at the time of the nal analysis , if this condition is met , ni ( or a stronger conclusion such as superiority ) can be claimed for the experimental treatment ( fig 2 )  . general cautions about ni designs . 
first , conclusions about the ni of a new regimen versus an active control are not particularly useful if the control was never established as best care in prior research.43 , 44 in addition , if outcomes in the control group are better than anticipated during trial planning , a resulting ni study could be underpowered ( even when the treatment arms are equivalent ) because of an overall shortage of events among the enrolled patients . 
a typical ni design is powered under the assumption of risk equality between groups , although this can be adjusted in some cases ( see herein the challenges with conducting ni designs in rare disease settings and some ad hoc and literature - based solutions section )  . 
in many cases , futility monitoring can be incorporated to halt the ni trial if it becomes evident that the therapy is truly inferior , although specic experimental testing approaches and decision rules should be considered carefully.45 - 47 challenges with conducting ni designs in rare disease settings and some ad hoc and literature - based solutions as is often the case in rare disease settings , the design of randomized ni trials for cog studies requires extra consideration and some degree of compromise to increase trial feasibility . 
within cog , all aspects of statistical design and supporting clinical rationale ultimately undergo several layers of review , during which the benets and caveats are evaluated carefully with respect to the realistic constraints imposed by treatment options , the patient population , and other resources . relaxation of type i error . 
ideally , ni trials , especially those for regulatory indications , would specify no greater than a one - sided type i error rate of 2.5% by default to retain a high degree of rigor and safeguard against false - positive conclusions.44 , 52 as in the superiority setting , a smaller type i error requires a larger sample size and widens the ci for the hr , making an ni conclusion much less likely to be a false - positive result . 
within cog , ni trials usually are motivated by the desire to reduce treatment intensity in groups of patients with established good prognoses , thereby reducing shortor long - term toxicities among children expected to be cured . 
in this context , there is precedent for conducting ni trials with a one - sided type i error rate of 5% ( or even more relaxed ; see relaxing trial operating characteristics and design parameters section ) , which strikes a compromise between error rate conservation and simple feasibility . literature - proposed solutions for ni hypotheses in rare diseases . 
freidlin et al53 adapted the ni design to allow for sample size calculations in situations where the assumed hr for the power calculation is not equal to 1 ( equivalence ) but reects modest superiority for the experimental treatment ( ie , hr slightly less than 1 )  . 
 renfro et al enhanced when a small improvement in outcome truly exists for the experimental arthis is often a welcome compromise when the experimental arm already offers less toxicity or other advantages . 
in rare disease settings , such as pediatric cancer trials conducted by cog , this design often is considered when small provements are deemed plausible or likely ( see example trials from cog testing ni - type hypotheses section for examples )  . 
in the same article , freidlin et al also described a sequential testing procedure that can be applied when a test for ni followed by a test for superiority ( a higher bar ) is desired . treatment example trials from cog testing ni - type hypotheses one recently opened cog trial with an ni design is aall1631 ( clinicaltrials.gov identier : nct03007147 ) , an international collaborative study of the ni of an experimental , less - toxic postinduction treatment in patients with standard - risk philadelphia chromosomepositive all.54 the 3 - year using historical data during trial planning , dfs rate was predicted to be 70% in the control arm , and m = 1.43 was set to correspond to a minimally reduced 3 - year dfs rate of 60% in the experimental group . assuming 6 years of accrual and a minimum of 3 years of follow - up , random assignment of 475 patients will yield 80% power to conclude ni using a one - sided type i error rate of 5% . 
for patients with low - grade gliomas , the question of treatment de - intensication to avoid harmful adverse effects without sacricing efcacy is highly relevant . however , given the rarity of this patient population , in addition to proposing a larger - than - usual ni margin ( hr of 1.7 ) and somewhat inated type i error rate of 10% , these two studies have used the design proposed by freidlin et al53 and described here in the challenges with conducting ni designs in rare disease settings and some ad hoc and literature - based solutions section to make these rare cancer ni trials more feasible because superiority is possible . 
in addition , availability of individual patient data from the potential historical trials or data sources is key so that the formal cohort that resembles the control arm can be tailored to t the current trials eligibility criteria and other characteristics . 
in cases where large historical control cohorts with adequate patient - level data are available , these designs can serve as an effective alternative to randomized trials in the context of signal nding . 
our sense is that such approaches work best in circumstances where the outcome is dismal , the targeted efcacy signal is large , and the historical cohort available is deemed to be sufciently similar to a cohort that would be enrolled if a concurrent control arm were included in the trial design . review of trial designs using historical controls dixon and simon62 described an initial approach to designing phase ii studies using historical controls ; however , it was subsequently shown by korn and freidlin63 that this method does not adequately protect against type i or ii errors . 
instead , korn and freidlin proposed a two - sample randomized design approach with adjusted allocation to the size of the historical cohort , which optimizes estimation of the median sample size and controls the type i and ii errors effectively . 
a drawback , however , is that the design is conservative in the sense that the number of events in the control cohort is almost always larger because of follow - up in the historical control being longer than what would have been observed with concurrent random assignment to cohorts of equal sample size . another drawback of this approach is that calculation of accumulating end point information during the trial for the purposes of timing interim analyses is not readily possible as with traditional designs . 
both drawbacks are addressed in an article by wu and xiong64 that focused on the median sample size as the primary parameter to be optimized on the basis of the one - sided sequential log - rank test . 
overall survival ( os ) outcomes for historical childrens oncology group studies in newly diagnosed diffuse intrinsic pontine glioma displayed ( a ) by study and ( b ) combined . a transformed information time to accommodate appropriately the information from the historical control and experimental group together to enable interim analyses . work by wu and li ( manuscript submitted for publication ) further extends this method for use with interim analyses on the basis of the alpha and beta spending functions of lan and demets . end point of this trial is progression - free survival , and the efcacy comparison is based on a historical control cohort constructed from prior cog studies , including acns0423 ( clinicaltrials.gov identier : nct00100802 ) and acns0822 ( clinicaltrials.gov identier : nct01236560 ) , as well as global meta - analysis cohorts where tumors received similar molecular annotation.65 example trials from cog using historical controls recommendations for use of historical controls a phase ii study currently in development for newly diagnosed diffuse intrinsic pontine glioma will use pooled historical data from several similar completed studies as the comparison cohort , where the primary end point of interest is os . 
using the methodology described in wu and xiong64 and the empirical kaplan - meier estimate to model the combined os distribution ( fig 3b ) , a reasonable phase ii design will require 45 patients to target an hr of 0.60 with 80% power and maintain less than a 5% type i error rate using a one - sided log - rank test . this hr translates to an approximately 18% net provement in 1 - year os rate ( 42% to 60% )  . 
because the study accrual duration is expected to be 1 to 1.5 years , the design will require 1 year of additional follow - up for all patients after accrual completion . 
a similar approach also has been used for acns1721 ( clinicaltrials.gov identier : nct03581292 ) , which enrolls newly diagnosed patients with high - grade glioma at least 3 years of age whose tumors are risk stratied by molecular criteria at initial study screening . 
the primary although phase ii designs that are based on historical control cohorts have desirable properties that support feasibility in rare disease settings , they are most useful when the available historical control group is relatively large . 
when the sample size and / or the number of events in the historical control cohort are small , the designs outlined here may not be feasible because the sample size in the proposed trial may not be able to compensate for the lack of patients / events supporting the historical cohort . 
on the other hand , if the historical control cohort is very large , then the design essentially reduces to a literature - controlled design where the comparison is against a xed rate at a specied time point . 
more sophisticated approaches for borrowing information from historical controls while simultaneously randomly assigning a small subset of patients to a control arm also have been described.67 discussion in this article , we highlighted some of the most prominent features and challenges that affect clinical trials designed for the pediatric oncology setting . 
renfro , phd , childrens oncology group , 222 e huntington dr , monrovia , ca 91016 ; twitter : @lindsayrenfro ; e - mail : lrenfro@ childrensoncologygroup.org. support supported by the national cancer institute ( 1u10ca180899 - 05 )  . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . arzu onar - thomas honoraria : eli lilly research funding : novartis ( inst ) , apexigen ( inst ) , pzer ( inst ) , celgene ( inst ) , merck ( inst ) travel , accommodations , expenses : eli lilly john a . 
kairalla stock and other ownership interests : johnson & johnson , sophiris bio no other potential conicts of interest were reported . acknowledgment we acknowledge the childrens oncology group committees associated with the examples cited in this article ( acute lymphatic leukemia , cns , neuroblastoma , acute myeloid leukemia , and rare tumors )  . references siegel r , naishadham d , jemal a : cancer statistics , 2012 . 
nat rev cancer 12 : 776 - 782 , 2012 bhatia s , meadows at : long - term follow - up of childhood cancer survivors : future directions for clinical care and research . 
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evans ae , land vj , newton wa , et al : combination chemotherapy ( vincristine , adriamycin , cyclophosphamide , and 5 - uorouracil ) in the treatment of children with malignant hepatoma . 
ortega ja , douglass ec , feusner jh , et al : randomized comparison of cisplatin / vincristine / uorouracil and cisplatin / continuous infusion doxorubicin for treatment of pediatric hepatoblastoma : a report from the childrens cancer group and the pediatric oncology group . 
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clin trials 8 : 270 - 276 , 2011 jung sh , kang sj , mccall lm , et al : sample size computation for two - sample noninferiority log - rank test . 
fangusaro j , onar - thomas a , young - poussaint t , et al : a phase ii prospective study of selumetinib in children with recurrent or refractory low - grade glioma ( lgg ) : a pediatric brain tumor consortium ( pbtc ) study . 
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mackay a , burford a , carvalho d , et al : integrated molecular meta - analysis of 1 , 000 pediatric high - grade and diffuse intrinsic pontine glioma . 
 complete response to pd - 1 inhibition in an adolescent with relapsed clear cell adenocarcinoma of the cervix predicted by neoepitope burden and apobec signature anya levinson , md1 ; alex g . 
alejandro sweet - cordero , md1 , 2 ; and elliot stieglitz , md1 , 2 introduction utilization of checkpoint inhibition therapy in the management of malignant diseases is increasing . however , response to these therapies is highly variable , and robust predictive markers remain elusive . identication of predictive biomarkers is crucial considering the toxicities and high nancial cost associated with this approach . 
here , we report an adolescent with relapsed clear cell adenocarcinoma of the cervix ( ccac ) who experienced a complete response to checkpoint blockade despite not exhibiting positive pd - l1 immunohistochemical ( ihc ) staining , microsatellite instability ( msi ) , or a high tumor mutational burden ( tmb )  . 
biopsy of an exophytic mass protruding into the vagina conrmed a human papillomavirus / p16 - negative ccac ( fig 1 )  . family history was notable for paternal clear cell renal carcinoma . 
sixteen months after entering remission , surveillance positron emission tomography ( pet ) computed tomography ( ct ) revealed new hypermetabolic disease , including a new right upper lobe ( rul ) pulmonary nodule , enlarged prevascular right internal mammary , and right paratracheal nodes ( fig 2a ) and a left supraclavicular node . 
biopsy of the supraclavicular node conrmed recurrence of ccac ( fig 3 )  . her relapsed tumor exhibited 0% staining for pd - l1 by ihc , microsatellite stability ( 1 , 149 of 1 , 157 tested microsatellite regions were stable ) , and a low tmb ( 1.9 single nucleotide variants per megabase on wgs , less than the pediatric threshold of 2 ; appendix )  . 
genomic assays performed included targeted dna sequencing , wgs , and rna - seq ( appendix table a1 )  . a targeted institutional dna - seq panel assaying 479 cancer - relevant genes4 showed that both diagnostic and relapsed tumors had a broad approximately 11 - fold amplication on chromosome 20 containing aurora kinase a as a putative driver.5 the diagnostic sample also displayed a chromosome 1p deletion containing arid1a , a gene frequently mutated in cervical cancer , 6 which was absent at relapse . no pathogenic point mutations , insertions / deletions ( indels ) , or germline alterations were detected on this panel at diagnosis or relapse . 
pathologic conrmation of clear cell carcinoma of the cervix . ( a ) primary clear cell carcinoma of the cervix , showing hyperchromatic tumor cell nests in the stroma at left and normal endocervical glandular epithelium at the right ( 40 )  . 
 ( c ) an immunohistochemical stain for hepatocyte nuclear factor 1 - , which is a marker of clear cell carcinoma , shows strong positive nuclear staining in the tumor cells , a positive test result ( 200 )  . the rul pulmonary nodule and the prevascular lymph lymph nodes denode ( fig 2b )  . 
the median age was 53 years , and only three patients were , 30 years of age , 13 making the patient presented here one of the youngest patients ever reported with idiopathic ccac . 
 ( a ) patient developed a new hypermetabolic pulmonary nodule in the right upper lobe ( blue arrow ) , along with prominent hypermetabolic prevascular nodes ( red arrow )  . 
 ( b ) after initial nivolumab therapy , patients right upper lobe nodule decreased in size ( blue arrow ) , and the prevascular node had nearly resolved ( red arrow )  . 
 ( c ) approximately 16 months after initial recurrent disease , the pulmonary nodule has nearly completely resolved ( blue arrow ) , and no new pathologic nodes have developed . known biomarkers for response to checkpoint inhibition are ihc staining for pd - l1 , presence of msi , and high tmb . this patient , who achieved a complete and durable remission from checkpoint inhibition without any of these markers , highlights the need for additional biomarkers . 
we sought to analyze the genomics of her tumors to explain her dramatic response . somatic variations that give rise to amino acid substitutions in tumors yield neoepitopes , or mutated , tumor - specic peptides on the surface of cancer cells that can serve as neoantigens for the adaptive immune system , even if they are not oncogenic . 
determinants of neoantigen tness are the likelihood of their presentation by the major histocompatibility complex and of subsequent t - cell recognition.16 the number of neoepitopes per tumor can be more functionally relevant than the tmb . 
biopsy of supraclavicular node conrms metastatic disease . ( a ) metastatic clear cell carcinoma in a supraclavicular lymph node . the tumor cells line glands or grow in nests and are surrounded by lymphocytes , seen at the lower left ( 200 )  . ( b ) metastatic clear cell carcinoma in a supraclavicular lymph node . 
an immunohistochemical stain for pd - l1 shows minimal staining in the tumor cells and staining of scattered lymphoid cells around the tumor ( 200 )  . patients relapsed tumor , higher than that of available ( although biologically distinct ) comparison cohorts , supporting the idea that high neoepitope burden may predict favorable response to immunotherapy . 
of these , signatures 1 ( aging ) and 3 ( homologous recombination deciency ; appendix fig a4 ) are commonly found in cancer.18 , 19 signatures 2 and 13 represent activity of the aid / apobec family of enzymes.18 , 19 is associated with expression of apobec , a family of zinc - coordinating enzymes that convert cytosines to uracils , has been implicated in mutagenesis of nonsmall - cell lung cancer . 
systematic cancer genomic and transcriptomic association studies have shown that overexpression of one of the family members , apobec3b , immune genes and known immunotherapy response biomarkers such as pd - l1.20 a positive correlation was recently documented between strength of the apobec signature and the neoepitope burden in many cancers , including cervical.21 the authors also found that this mutational signature corresponded to increased abundance of tumorinltrating lymphocytes in some cancers , 21 although these were absent in this case . 
clinically , the apobec mutational signature is enriched in patients with durable clinical benet after immunotherapy , and an apobec signature may be better than tmb in predicting immunotherapy response.22 , 23 finally , there was a small contribution from signature 8 of uncertain etiology ( it is perhaps related to nucleotide excision repair deciency ) .24 the present patient is of interest for several reasons . 
box - and - whisker plots display the interquartile range ( box ) and outlier thresholds ( whiskers ) for the therapeutically applicable research to generate effective treatments neuroblastoma and the cancer genome atlas prostate adenocarcinoma data sets . 
although there may be other factors that contributed to the patients dramatic response , this case supports emerging evidence that a high neoepitope burden and an apobec mutational signature response to are potentially actionable biomarkers of checkpoint blockade . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . jessica van zife employment : adaptive biotechnologies ( i ) stock and other ownership interests : adaptive biotechnologies ( i ) patents , royalties , other intellectual property : adaptive biotechnologies ( i ) benjamin laguna leadership : sira medical stock and other ownership interests : sira medical stanley g . 
leung stock and other ownership interests : illumina , pzer , thermo fisher jacob pfeil employment : abbvie no other potential conicts of interest were reported . acknowledgment we thank the patient and her family for their willingness to share their experience using an unconventional treatment approach . 
naumann rw , hollebecque a , meyer t , et al : safety and efcacy of nivolumab monotherapy in recurrent or metastatic cervical , vaginal , or vulvar carcinoma : results from the phase i / ii checkmate 358 trial . 
european society for medical oncology meeting , barcelona , spain , september 27 - october 1 , 2019 ( abstr lba62 ) kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identies pathogenic germline mutations , and directs targeted therapy . 
curr oncol rep 15 : 566 - 572 , 2013 cho h , kim js , chung h , et al : loss of arid1a / baf250a expression is linked to tumor progression and adverse prognosis in cervical cancer . 
n engl j med 377 : 1345 - 1356 , 2017 rao aa , madejska aa , pfeil j , et al : protect : prediction of t - cell epitopes for cancer therapy . 
reich o , tamussino k , lahousen m , et al : clear cell carcinoma of the uterine cervix : pathology and prognosis in surgically treated stage ib - iib disease in women not exposed in utero to diethylstilbestrol . 
thomas mb , wright jd , leiser al , et al : clear cell carcinoma of the cervix : a multi - institutional review in the post - des era . 
boyd j , takahashi h , waggoner se , et al : molecular genetic analysis of clear cell adenocarcinomas of the vagina and cervix associated and unassociated with diethylstilbestrol exposure in utero . 
turajlic s , litcheld k , xu h , et al : insertion - and - deletion - derived tumour - specic neoantigens and the immunogenic phenotype : a pan - cancer analysis . 28 : 15 - 17 , 2019 lancet oncol 18 : 1009 - 1021 , 2017 18 . 
wang s , jia m , he z , et al : apobec3b and apobec mutational signature as potential predictive markers for immunotherapy response in non - small cell lung cancer . 
chen z , wen w , bao j , et al : integrative genomic analyses of apobec - mutational signature , expression and germline deletion of apobec3 genes , and immunogenicity in multiple cancer types . 
chen pl , roh w , reuben a , et al : analysis of immune signatures in longitudinal tumor samples yields insight into biomarkers of response and mechanisms of resistance to immune checkpoint blockade . 
boichard a , tsigelny if , kurzrock r : high expression of pd - 1 ligands is associated with kataegis mutational signature and apobec3 alterations . oncoimmunology 6 : e1284719 , 2017 jager m , blokzijl f , kuijk e , et al : deciency of nucleotide excision repair is associated with mutational signature observed in cancer . 
the lymph node from the patient was snap frozen and ffpe into optimal cutting temperature ( oct ) mediuall tissues were sectioned to a depth of 5 m and stained with hematoxylin and eossamples were evaluated for tumor content by a certied pathologist . 
rna integrity was quantied with the high sensitivity rna kit dnf - 472 ( advanced analytical technologies , orangeburg , ny ) on the fragment analyzer ( advanced analytical technologies )  . 
immunohistochemical pd - l1 staining was performed on tumor cells with the us food and drug administrationapproved pd - l1 28 - 8 pharmdx antibody for opdivo ( neogenomics laboratories , fort myers , fl )  . whole blood was collected during lymph node metastasectomy in a 4ml edta vacutainer . 
germline dna was extracted using the dneasy blood and tissue kit 69504 ( qiagen )  . dna was quantied using the nanodrop 2000 ( thermo fisher , waltham , ma ) and qubit high sensitivity dsdna assay q32851 ( thermo fisher ) and integrity quantied using the high sensitivity gdna kit dnf488 ( advanced analytical technologies ) on the fragment analyzer ( advanced analytical technologies )  . 
libraries from ffpe samples were made using the truseq rna access kit ( rs - 301 - 2001 ; illumina , san diego , ca ) with an input of 100 ng in accordance with manufacturers instructions . libraries from ffpe samples were made using the truseq stranded mrna kit ( rs - 122 - 2101 ; illumina ) with an input of 400 ng in accordance with manufacturers instructions . 
outliers ( ie , underor overexpression ) were identied using tukey outlier denition . targeted dna sequencing an institutional dna sequencing panel assaying 479 cancer - related genes was used.4 as per kline et al , 4 genomic dna was extracted from peripheral blood and tumor tissue microdissected from ffpe blocks . 
capture - based next - generation sequencing ( ngs ) was performed at the university of california , san francisco ( ucsf ) clinical cancer genomics laboratory , using an assay targeting the coding regions of these genes , tert promoter , select introns from 40 genes ( for detection of gene fusions and other structural variants ) , and intergenic regions at regular intervals along each chromosome ( for chromosomal copy number assessment ) , altogether with a total sequencing footprint of 2.8 mb ( ucsf500 cancer gene panel , appendix fig a2 )  . 
a list of genes included can be found at the following url ( although some genes may have been added or deleted since this patients analysis in 2017 ) : gene - panel - test - ucsf500 - uc500 . whole - genome sequencing libraries were generated using the truseq nano kit fc - 121 - 4001 ( illumina ) with a 350 - bp insert , per manufacturers instructions . 
libraries were made using 200 - ng input gdna , and then quantied on the tapestation 4200 ( agilent , santa clara , ca ) and sequenced on the hiseq x ten ( illumina ) using 2 150 bp paired - end reads . 
nonsynonymous variants were annotated using variant effect predictor ( mclaren w , et al : genome biol 17 : 122 , 2016 )  . predicted tumor neoepitope analysis we used the prediction of t - cell epitopes for cancer therapy ( protect ) pipeline v 2.6.18 to investigate the patients neoepitope burden . 
we compared the patients tumor mutation and neoepitope burden to publicly available protect data for the therapeutically applicable research to generate effective treatments neuroblastoma ( pmid : 23334666 ) and the cancer genome atlas prostate adenocarcinoma data sets ( pmid : 26544944 ) and assessed for signicance using tukeys outlier denition . apobec signature analysis single base substitution mutational signatures were extracted from the samples wgs data using deconstructsigs ( rosenthal r , et al : genome biol 17 : 31 , 2016 ) , with default parameters . 
the patients sample is notable for a signature 3 ( homologous recombination deciency [ hrd ] ) signature . violin plot of the fraction of mutations in each sample from ma et al11 attributed to signature 3 . 
a biopsy specimen of the liver lesion revealed a poorly differentiated carcinoma , with tumor cells displaying a partly pleomorphic , signet ring or spindle cell appearance , fitting to the metastatic presentation of either a carcinoma of the bile duct or pancreatico - biliary syste additional staging procedures indicated a large mass in the head of the pancreas . 
biopsy of this region identified tumor cells that resembled the previous liver lesion . after comprehensive review of all data , our interdisciplinary tumor board diagnosed a hepatically metastasized pancreatic ductal adenocarcinoma ( pdac ) and recommended palliative chemotherapy with gemcitabine and nanoparticle albumin bound paclitaxel . 
after an additional four cycles of gemcitabine monotherapy , overt progression was observed with only minor growth of the primary tumor in the pancreas but newly diagnosed small metastases in the liver . to obtain information about the molecular profile of the tumor , genomic dna was isolated from the liver metastasis of the pancreatic carcinoma , and a blood sample from the patient was used as a reference . 
the samples were enriched for whole - exome sequencing and sequenced on an illumina hiseq next - generation sequencing platform ( illumina , san diego , ca ) by cegat ( tuebingen , germany )  . 
the most relevant somatic driver mutations were a loss - of - function stop mutation within fancb ( e472 * ) and an activating mutation in braf ( v600e )  . 
the patient also had no germline mutations in known cancer susceptibility genes . because of the remarkably high tmb and to directly interfere with the driver mapk / erk signaling pathway , the patient was offered a personalized off - label therapy with the intravenous immune checkpoint pd - 1 antibody pembrolizumab ( 200 - mg flat dose ) in combination with the oral mek inhibitor trametinib ( 2 mg daily )  . 
 the mapk / erk pathway has been implicated in the immune resistance of tumors , and inhibition of this pathway can lead to an increased infiltration of the tumor by cd8 - positive t cells in preclinical models.1 furthermore , mek inhibition promotes t - cell activity , eliciting a synergistic effect with checkpoint blockage.2 although trametinib therapy had to be terminated after 3 months because of severe adverse effects , including edema and fatigue , the immunotherapy was well tolerated and continued for another 6 months . 
the only relevant immune - related adverse event was a suppression of the endogenous level of cortisol ( hypocortisolism ) , resulting in the need of permanent oral replacement therapy . 
surveillance positron emission tomography computed tomography scans after eight cycles of chemotherapy ( a ) before change to immunotherapy and mek inhibition , and ( b ) 5 months and ( c ) 9 months after change to immunotherapy . 
 ( a ) during chemotherapy , positron emission tomographycomputed tomography scan reveals progression of the primary tumor in the pancreas ( ) and of the hypermetabolic solitary metastasis of the liver ( * )  . 
 ( c ) metabolic activity in both lesions considerably decreased . surveillance positron emission tomography computed tomography scans revealed declining disease according to positron emission tomography response criteria in solid tumors , regarding the size of the masses in the pancreas and liver , as well as their metabolic activity , providing clear evidence for an explicit and sustainable response to the personalized therapy ( figs 1a - 1c )  . to change the therapeutic concept from palliative to potentially curative , exploratory laparotomy was performed 18 months after primary diagnosis . 
instead , the tumor was irradiated with a total dose of 54 gy administered over 6 weeks to promote local control , while pembrolizumab administration was discontinued to avoid additive toxicity to the gi tract in combination with irradiation . histologic analysis of the resected liver tissue led to the diagnosis of a metastasized , poorly differentiated , in parts undifferentiated / anaplastic pancreatic adenocarcinoma , which represents a variant of pdac . 
a moderate number of cd3 - positive t cells were observed within the tumor tissue ( approximately 20 t cells per 100 nucleated cells ) , including equal amounts of cd8 - positive and cd4 - positive cells , with a moderately higher density at the tumor margin ( figs 2e and 2f )  . 
mmr and additional dna repair proteins such as atm , atr , and brca1 were regularly expressed by the tumor cells ( not shown )  . the prognosis of undifferentiated pancreatic adenocarcinoma is usually worse than that of conventional pdac , with distant metastases frequently present at the time of diagnosis.3 however , our patient still is in good condition with no evidence of relapse 2 years after primary diagnosis . discussion in pdac , only minimal progress has been made so far in identifying therapies targeted toward altered signaling pathways , and single - agent therapy with antictla - 4 or antipd - 1 antibodies was found to be ineffective in early clinical trials.4 instead , chemotherapeutic selection on the basis of histopathologic analysis alone remains the standard of care.5 here , we report the case of a patient with a metastasized , undifferentiated pdac with a high tmb who is experiencing durable remission to single - agent checkpoint inhibition . the tmb has already been correlated with clinical benefits of antipd - 1 and antictla - 4 therapy in various tumor types , including melanoma , 6 , 7 nonsmall - cell lung cancer , 8 and several dna repairdeficient tumors.9 - 11 however , no generally agreed - on definition of hypermutation has been postulated yet . 
in a recent study based on > 80 , 000 tumors , the threshold for hypermutation was set to 10 mutations / mb.12 this value coincides with the median tmb of patients previously reported to respond to checkpoint inhibition.8 , 13 in pdac , a high tmb is usually rare . 
 ( a ) moderately to poorly differentiated adenocarcinoma consistent with a metastasis of a pancreatic ductal adenocarcinoma ( hematoxylin and eosin staining [ h&e ] ; magnification , 100 )  . 
 ( b ) tumor heterogeneity : undifferentiated component ( left ) and a highly regressive carcinoma component ( right ) showing fibrosis and myxoid change ( h&e ; magnification , 100 )  . 
it was also shown recently that high levels of microsatellite instability are mostly restricted to tumors in the range of 10 to 100 mutations / mb.12 however , the tumor of the patient in this report was microsatellite stable . 
 instead , we found a loss - of - function stop mutation within the fanconi anemia complementation group b ( fancb ) gene ( e472 * ) and an activating mutation in braf ( v600e )  . 
somatic mutations in the fa gene family can be found in approximately 13% of pancreatic tumors.17 , 18 recently , chalmers et al19 identified > 100 somatic mutations significantly associated with increased tmb , including missense mutations in the fa pathway genes fancd2 and fancj , providing evidence that the loss - offunction fancb mutation might contribute to the high tmb in our patient . the mapk / erk pathway is also often altered in pdac . 
the braf gene is mutated in one - third of pancreatic cancers with known wild - type kras.20 it has been suggested that the kras and braf oncogenes function in a mutually exclusive manner in the transformation and carcinogenesis of pancreatic cancer . 
to block the mutationally activated cellular pathway and to increase the immune effect in the typical desmoplastic stroma within pancreatic cancers , we combined pembrolizumab with the oral mek inhibitor trametinib . 
however , the latter had to be terminated prematurely after 3 months because of intolerable adverse effects ; its relative contribution to the patients response cannot be addressed precisely . in conclusion , our data suggest that whole exome sequencing has the potential to identify a small but clinically meaningful subgroup of pdac with a high tmb . 
liu l , mayes pa , eastman s , et al : the braf and mek inhibitors dabrafenib and trametinib : effects on immune function and in combination with immunomodulatory antibodies targeting pd - 1 , pd - l1 , and ctla - 4 . 
ebert pjr , cheung j , yang y , et al : map kinase inhibition promotes t cell and anti - tumor activity in combination with pd - l1 checkpoint blockade . 
howitt be , shukla sa , sholl lm , et al : association of polymerase e - mutated and microsatelliteinstable endometrial cancers with neoantigen load , number of tumor - infiltrating lymphocytes , and expression of pd - 1 and pd - l1 . 
strickland kc , howitt be , shukla sa , et al : association and prognostic significance of brca1 / 2 - mutation status with neoantigen load , number of tumor - infiltrating lymphocytes and expression of pd - 1 / pd - l1 in high grade serous ovarian cancer . 
the patient subsequently underwent neoadjuvant radiation in addition to receiving weekly carboplatin and paclitaxel , followed by esophagogastrectomy.7 pathology revealed moderately differentiated adenocarcinoma invading the adventitia ( pt3 ) , but none of the 14 lymph nodes were involved ( pn0 )  . 
one and a half years after resection , surveillance imaging revealed new concerning hypodensity in the liver , accompanied by an increase in the carcinoembryonic antigen ( cea ) levels . 
next - generation sequencing ( ngs ) was performed on biopsies from the time of initial and recurrent liver metastasis using the commercially available comprehensive genomic proling ( cgp ) assay from foundation medicine ( cambridge , ma ; table 1 )  . 
serial blood collections were also obtained to determine the presence of ctdna using a tumorinformed multiplex polymerase chain reaction - ngs assay from natera ( san carlos , ca ) designed from tumor genomic alterations ( table 1 )  . 
at the time of disease recurrence in the liver , the tumor - informed assay with an established analytical sensitivity5 revealed elevated levels of ctdna , measured in mean tumor molecules / ml of plasma ( fig 1 )  . the patient underwent the patient approximately 760 days postdiagnosis , received 6 cycles ( c6 ) of uorouracil ( fu ) , leucovorin , and oxaliplatin ( mfolfox6 ) , with radiographic response in the liver lesion . 
after another year ( approximately 1 , 490 days postdiagnosis ) , the patient developed a new fdgavid mass in the ablation cavity , accompanied by an increase in cea level . 
the patient received 1 cycle ( c1 ) of fu and leucovorin ( fu / lv ; approximately 1 , 520 days postdiagnosis ) , complicated by oral mucositis , followed by resection of the liver mass ( approximately 1 , 580 days postdiagnosis ) , and pathologically conrmed to be metastatic eac . 
after metastasectomy , surveillance imaging showed no evidence of recurrence , ctdna levels became negative , and the patient remains in remission , currently 11 months ( approximately 320 days ) postmetastasectomy . 
the use of more sensitive cancer detection methods may help optimize treatment approaches ( escalation or de - escalation of therapies ) in the localized setting . in this case study , the patient experienced oligometastatic recurrence despite aggressive trimodality therapy . 
although we were unable to assess ctdna in the localized setting for this patient , a recent study investigated ctdna in the context of neoadjuvant chemoradiation for localized esophageal cancer and showed that detectable ctdna levels postchemoradiation , along with metabolic imaging analysis , predicted tumor progression with 100% sensitivity versus ctdna alone ( 71% ) and imaging alone ( 57% ) .15 thus , detectable , ctdna could help clarify ambiguous ndings ( as observed in this case study ) and could help identify high - risk patients with mrd who could be upper limit of normal cea 1 , 000 0.01 1 , 370 1 , 523 1 , 677 1 , 826 1 , 219 time since diagnosis ( days ) 1 , 066 no evidence of disease or disease response ctdna - positive ( mtm / ml ) liver metastasis suspicious finding , subsequently resolved or stable ctdna - negative ( mtm / ml ) mfolfox6 suspicious finding , subsequently confirmed cea ( ng / ml ) fluorouracil / leucovorin fig 1 . 
another study evaluated prognosis based on the presence of detectable ctdna after neoadjuvant chemotherapy prior to cystectomy in patients with bladder cancer.3 the preoperative ctdna status was 100% sensitive in predicting pathologic complete response , suggesting that trials could strategize testdeferred surgery in patients with undetectable ctdna postneoadjuvant therapy . in this case study , the initial plan was to proceed with chemotherapy ( mfolfox6 ) , followed by metastasectomy for removal of any residual disease ; however , the latter was delayed because of the ambiguous ndings that showed enlarged pulmonary / soft tissue nodules ( table 2 ; fig 1 ) , requiring further follow - up . 
retrospectively , serial ctdna analysis suggested that chemotherapy was more effective than rfa in reducing the tumor burden , and thus , consideration of consolidation metastasectomy in lieu ofor soon afterrfa could have prevented the second local recurrence . 
 ( * ) brd4 and smad4 have 3 missing data points between september 2017 and june 2018 . mfolfox6 , 6 cycles of uorouracil , leucovorin , and oxaliplatin . this case study illustrates the potential advantage of using ctdna as a conrmatory , adjunctive surveillance tool . 
the early and continued increase in ctdna post - rfa showed the sensitivity and specicity of the ctdna assay in predicting disease recurrence by a lead time of 174 days compared with cea and 350 days before radiographic conrmation . 
cea is known to be a lagging indicator of disease and is relatively insensitive , nonspecic , and can be confounded by acute or chronic inammation , smoking , liver disease , and diabetesall common comorbidities in this patient population.16 in this particular case , the multiple postresection complications confounded the interpretation of an increase in cea , an increase that ultimately attenuated and has not translated into relapse by imaging or ctdna with 11 months of follow - up . 
this could be a faster and more accurate measure than following the standard approach of using radiographic progression - free survival alone . it is important to note that the tumor - informed ctdna assay is a personalized method that requires separate whole - exome sequencing of the tumor tissue to develop patient - specic primers . 
the customized design of this assay targeting a set of clonal mutations known to be present in the specic tumor leads to its high sensitivity and specicity ; it is not intended to be a discovery assay for assessment of actionable genomic targets , but rather , a tool for detecting mrd . 
it was notable to observe that genomic alterations in the primary tumor were detectable with the tumor - informed ctdna assay at the time of relapse , and they all appeared to track in parallel ( fig 2 )  . 
we did not observe evidence of signicant selection for or against clones harboring any of the genomic targets tested during treatment , but we cannot rule out the acquisition of additional subclonal genomic alterations . our study has certain limitations . 
another aspect is how often and how long a patient should be monitored in this setting . although tumor burden may be undetectable by the ctdna assay , the patient is still at risk and needs surveillance . however , given the features described , it is reasonable to test this assays utility in multiple disease settings as part of clinical trials in esophageal and other cancers . 
einstein research funding : trovagene ( inst ) , bristol - myers squibb ( inst ) nathan liang employment : natera stock and other ownership interests : natera meenakshi malhotra employment : natera stock and other ownership interests : natera alexey aleshin employment : natera stock and other ownership interests : natera consulting or advisory role : mission bio solomon moshkevich employment : natera , evidation health ( i ) stock and other ownership interests : natera patents , royalties , other intellectual property : named as inventor on a patent led by natera travel , accommodations , expenses : natera paul r . 
billings employment : natera leadership : trovagene , biological dynamics , omniseq , alveo biotechnologies stock and other ownership interests : natera , trovagene , biological dynamics , omniseq , alveo biotechnologies consulting or advisory role : bethesda group , guidepoint global eirini pectasides consulting or advisory role : clovis oncology research funding : bristol - myers squibb no other potential conicts of interest were reported . references shah m , denlinger cs : optimal post - treatment surveillance in cancer survivors : is more really better ? oncology ( williston park ) 29 : 230 - 240 , 2015 2 . 
natl j maxillofac surg 7 : 17 - 20 , 2016 christensen e , birkenkamp - demtr oder k , sethi h , et al : early detection of metastatic relapse and monitoring of therapeutic efcacy by ultra - deep sequencing of plasma cell - free dna in patients with urothelial bladder carcinoma . 
j clin oncol 37 : 1547 - 1557 , 2019 abbosh c , birkbak nj , wilson ga , et al : phylogenetic ctdna analysis depicts early - stage lung cancer evolution . 
nature 545 : 446 - 451 , 2017 [ erratum : nature 554 : 264 , 2018 ] coombes c , page k , salari r , et al : personalized detection of circulating tumor dna antedates breast cancer metastatic recurrence . 
clin cancer res 25 : 14255 - 4263 , 2019 reinert t , henriksen tv , christensen e , et al : analysis of plasma cell - free dna by ultradeep sequencing in patients with stages i to iii colorectal cancer . 
jama oncol 5 : 1124 - 1131 , 2019 shapiro j , van lanschot jjb , hulshof mccm , et al : neoadjuvant chemoradiotherapy plus surgery versus surgery alone for oesophageal or junctional cancer ( cross ) : long - term results of a randomised controlled trial . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
arch pathol lab med 142 : 1242 - 1253 , 2018 araujo dv , bratman sv , siu ll : designing circulating tumor dna - based interventional clinical trials in oncology . 
bray f , ferlay j , soerjomataram i , et al : global cancer statistics 2018 : globocan estimates of incidence and mortality worldwide for 36 cancers in 185 countries . 
 prospective longitudinal ctdna workow reveals clinically actionable alterations in ovarian cancer jaana oikkonen , phd1 ; kaiyang zhang , msc1 ; liina salminen , md2 ; ingrid schulman1 ; kari lavikka1 ; noora andersson , phd1 ; erika ojanper a1 ; sakari hietanen , md , phd2 ; seija gr enman , md , phd2 ; rainer lehtonen , phd1 ; kaisa huhtinen , phd3 ; olli carp en , md , phd1 , 3 , 4 ; johanna hynninen , md , phd2 ; anniina f arkkil a , md , phd1 , 4 , 5 ; and sampsa hautaniemi , d tech1 purpose circulating tumor dna ( ctdna ) detection is a minimally invasive technique that offers dynamic molecular snapshots of genomic alterations in cancer . 
although ctdna markers can be used for early detection of cancers or for monitoring treatment efcacy , the value of ctdna in guiding treatment decisions in solid cancers is controversial . 
we applied the workow to a prospective cohort consisting of 78 ctdna samples from 12 patients with high - grade serous ovarian cancer before , during , and after treatment . these longitudinal data sets were analyzed using our open - access ctdna - tailored bioinformatics analysis pipeline and in - house translational oncology knowledgebase to detect clinically actionable genomic alterations . 
the alterations were ranked according to the european society for medical oncology scale for clinical actionability of molecular targets . results our results show good concordance of mutations and copy number alterations in ctdna and tumor samples , and alterations associated with clinically available drugs were detected in seven patients ( 58% )  . treatment of one chemoresistant patient was changed on the basis of detection of erbb2 amplication , and this ctdna - guided decision was followed by signicant tumor shrinkage and complete normalization of the cancer antigen 125 tumor marker . conclusion our results demonstrate a proof of concept for using ctdna to guide clinical decisions . 
analysis of circulating tumor dna ( ctdna ) is an approach with the potential of overcoming all three obstacles.1 indeed , ctdna sampling is a clinically attractive , minimally invasive technique that is based on the observation that tumor cells leak dna to the bloodstream , where it can be captured by genomic assays . 
 oikkonen et al context key objective the aim of the study was to identify the clinical usefulness of circulating tumor dna ( ctdna ) in the treatment of high - grade serous ovarian cancer ( hgsoc ) and to provide a clinical workow for reliable detection of ctdna alterations . knowledge generated we show that longitudinal ctdna sampling can be used to detect response to platinum - taxane primary therapy after the rst cycles of chemotherapy and to identify clinically applicable mutations and copy number alterations . 
in one patient with chemoresistant hgsoc , ctdna - guided treatment including trastuzumab was administered during tumor progression and yielded tumor shrinkage . relevance the early detection of poor - responding patients allows the design of alternative treatment strategies in hgsoc . 
especially for platinum - resistant patients who have limited treatment options , rapid discovery of resistant cell populations can provide an early opportunity to interfere with the development of recurrence . 
this is a substantial improvement in the management of recurrent solid cancers , where tumors are not usually sampled either because of the risk of potential intervention complications or simply because the sample could be insufcient or not representative of the disease . ctdna analysistailored bioinformatics pipelines , and a translational oncology knowledgebase to identify clinically actionable mutations and copy number alterations ( cnas )  . 
we demonstrate the usefulness of this approach in high - grade serous ovarian cancer ( hgsoc ) , which is the most common and aggressive form of epithelial ovarian cancer , with a 5 - year survival rate of 43%.7 the current standard - of - care therapy for advanced hgsoc consists of cytoreductive surgery and platinum - paclitaxel chemotherapy.8 although the initial response to standard - of - care therapy is usually good , nearly all patients eventually relapse and have limited treatment options . 
the samples were stored at 80c as 1 to 2 ml aliquots frozen less than 2 hours after collection to avoid lysis of the white blood cells.1 cell - free dna ( cfdna ) was extracted from plasma samples and subjected to 1000 targeted illumina hi - seq sequencing at bgi ( bgi europe a / s , copenhagen , denmark ) using the oseq solid cancer panel with more than 500 clinically actionable genes ( data supplement )  . dna was isolated from 21 liquid ln2 snap - frozen tumor tissue and ascites samples ( data supplement ) , as well as from whole blood ( germline ) buffy coat samples , and was sequenced using the oseq panel with coverage of 200 . mutation and copy number detection mutation detection was performed in the computational ecosystem anduril10 using the ctdna data analysis pipeline , which is based on best practices for sequencing data analysis ( data supplement )  . 
filtering steps included detection of likely spurious mutations by identifying clusters of variants shared between patients but not known in cancer , 12 and functionally irrelevant variants by a combined annotation dependent depletion13 score of less than 15 . 
to estimate the change in mutational proles , we identied the largest proportion of signicantly decreased variants during treatment compared with the pretreatment sample ( p , .01 , fishers exact test )  . 
because of varying numbers of mutations in the pretreatment samples , the proportion of signicantly decreased variants was corrected for mutation counts . pathway analysis was performed for genes with a nondecreasing mutation frequency ( p , .01 , fishers exact test ; data supplement ) using the consensuspathdb15 algoriththe consensuspathdb integrates data from 32 databases and allows comprehensive over - representation analysis for mutations . immunohistochemistry and in situ hybridization potentially clinically actionable alterations were validated through immunohistochemistry ( ihc ) and in situ hybridization for alterations classied as most prominent ( escat , the european society for medical oncology scale for clinical actionability of molecular targets ) 16 and shown to exist in patients tumor tissue ( data supplement )  . results ctdna panel reliably captures mutations and cnas we collected 78 longitudinal ctdna samples and 21 tumor tissue samples from 12 unselected patients with hgsoc ( data supplement )  . 
we applied a sequencing panel of more than 500 genes , followed by variant and cna calling , ltering , and prioritization of clinically relevant aberrations as shown in fig 1a and the data supplement . 
altogether , 265 mutations in 185 genes ( data supplement ) and cna aberrations in 113 genes ( data supplement ) passed our calling and ltering criteria . the median concordance of mutations detected from plasma to tumor tissue samples from the same patient was 79% ( fig 1b ; data supplement )  . 
 oikkonen et al 12 patients with hgsoc variant and cna calling targeted sequencing mutation discovery filtering plasma , sampled longitudinally cancer gene panel cna detection germline dna tumor tissue validation clinical application interpretation prioritization early response monitoring vaf dynamics drug relevance translational oncology knowledgebase tumor burden and mutational composition during therapy plasma only shared tissue only patient 12 months 12 months fig 1 . 
pfi , platinum - free interval . ctdna mutation proles reect long - term treatment response and reveal targetable pathways in patients with aggressive hgsoc ctdna allows several ways to monitor treatment response . for hgsoc , parkinson et al4 suggested the use of tp53 measured from ctdna in disease monitoring . 
we observed that , consistent with their results , tp53 vaf was below 0.5% in all except one patient during primary chemotherapy and was increased in all patients at disease progression ( fig 2 )  . 
these results suggest that the changes in vafs detected from ctdna samples can be used for the early identication of patients with poor response to chemotherapy . we hypothesized that genes whose mutation vafs remained stable or increased during treatment in poor responders could reveal pathways crucial for chemoresistance . 
pathways enriched in the poor - responding patients in comparison with the good - responding patients included transcription , p53 , and chromatin regulatory pathways and dna double - strand break repair pathways ( data supplement )  . 
these alterations are predicted to cause sensitivity to cdk2 / 425 and / or cdk4 / 6 inhibitors.26 regardless of the presence of hr - deciencyconferring alterations , this patient , who had no residual tumor after surgery , progressed 8.9 months after the last platinum cycle . ctdna identies actionable mutations in patients with hgsoc we prioritized and interpreted all 265 mutations and 113 cnas using the translational oncology knowledgebase , which integrates information from 11 databases and 14 scientic articles ( data supplement )  . 
the knowledgebaseprioritized mutations and cnas revealed four major targetable processes : mammalian target of rapamycin ( mtor ; patients eoc429 , eoc49 ) , dna repair ( patients eoc429 , eoc677 , and eoc1067 ) , epidermal growth factor receptor ( egfr ; patients eoc587 , eoc736 , and eoc568 ) , and cyclin dependent kinases ( cdks ; patient eoc1067 )  . the highest allele frequency mutations matching tumor content were detected in pten ( patient eoc49 ) and nf1 ( patient eoc429 ) , which cause overactivation of the mtor pathway.20 , 22 patients with the activated mtor pathway have been shown to be responsive to phosphatidylinositol 3 - kinase / mtor inhibitors.22 we validated overactivity of the mtor pathway in the two patients with ihc from tumor tissue samples ( fig 3 ; data supplement )  . 
in patient eoc49 , pten mutation vaf in omentum ( 8% and 6% for pretreatment and interval samples , respectively ) and plasma matched the pattern of tp53 mutation , indicating that tumor cells and presents an early event in tumor evolution ( data supplement )  . 
pten was detected in a follow - up sample at 8 months after primary treatment with vaf of 0.1% , conrming its persistence during therapy . the pten mutation exists in all we observed mutations and cnas in genes associated with dna repair in three patients . 
in patient eoc677 , we detected mutations in brca2 and stag2 , which potentially confer homologous recombination ( hr ) dna repair deciency and sensitivity to poly - adp ribose polymerase ( parp ) inhibitors . however , the frequencies of these mutations were low in the tumor tissues ( 0.2% for brca2 and 3.1% for stag2 ) , suggesting subclonal events . 
in patient eoc429 , we detected a germline deletion in rad51c from plasma , which has been shown to confer hr deciency and parp inhibitor sensitivity , 21 and , consistent with this , the patient had a prolonged response to platinum - based chemotherapy . 
we also detected a somatic deletion of fanca in patient three patients had mutations or cnas associated with sensitivity to drugs targeting the epidermal growth factor receptor ( egfr ) pathway . 
patient eoc568 had an erbb4 mutation , which is predicted to confer sensitivity to egfr inhibitors.27 patient eoc587 had a mapk mutation and a simultaneous mapk1 amplication , which are associated with resistance to the egfr targeting therapies.28 , 29 we detected a high copycount erbb2 amplication in the ctdna in patient eoc736 . the erbb2 locus is amplied in 3% to 11% of hgsocs30 , 31 and is a predictive biomarker for trastuzumab . 
the erbb2 amplication was validated in primary omentum tissue using snp genotypebased cna detection and in the tumor tissue sample from interval debulking surgery with in situ hybridization and ihc ( figs 4a and 4b )  . patient eoc736 was treated with nact , and she participated in a clinical trial after primary treatment , receiving maintenance bevacizumab and olaparib or placebo ( fig 4c )  . 
although she had a clinical and radiologic complete response to primary therapy , tp53 vaf remained detectable throughout the treatment , which , on the basis of our ndings , indicates a poor response to platinum taxane ( data supplement )  . 
this patient also suffered from severe paclitaxel - induced neuropathy after primary treatment , and therefore , pegylated liposomal doxorubicin ( pld ) was started at the rst relapse instead of dose - dense paclitaxel therapy . 
pld was discontinued after four cycles because of constantly rising ca125 ( from 193 to 769 ) and progression in lymph nodes as evidenced by a computed tomography scan . the erbb2 amplication detected in on the basis of ctdna , treatment of patient eoc736 was changed to trastuzumab 600 mg subcutaneously once every 3 weeks , combined with reduced doses of carboplatin ( auc4 ) and dose - dense paclitaxel ( 80 mg / m2 on days 1 and 8 )  . 
the patient responded to this combination well , and a biochemical complete response ( ca - 125 value reduced from 840 iu / ml to 19 iu / ml ) was achieved after only three treatment cycles ( fig 4c )  . 
pathogenic mutation in nf1 was detected in circulating tumor dna ( ctdna ) , leading to functionally overactive mammalian target of rapamycin ( mtor ) signaling in the tumor tissue . 
 ( a ) mutational frequencies in a good - responding patient ( eoc429 ) during primary treatment and follow - up . variant allele frequency ( vaf ) values are normalized for the frequency level to show relative changes in the levels . 
 ( b ) mtor pathway activation was detected in primary tumor tissue with higher staining for phosphorylated mtor ( pmtor ) and e4 - bp1 compared with normal ovarian tissue . 
scale bar , 100 m ( c ) in addition to having a complete response on the basis of recist 1.1 , the response to primary therapy was good , as indicated by cancer antigen 125 ( ca - 125 ) values that stayed low during treatment and follow - up . 
cadd , combined annotation dependent depletion ; hgsoc , high - grade serous ovarian cancer ; pte , primary treatment end ; 4e - bp , 4e - binding protein . sequencing of more than 500 genes from liquid biopsies , a ctdna data analysis pipeline , and a translational oncology knowledgebase to enable longitudinal analysis of ctdna during therapy and guide personalized cancer treatment decisions . 
the ctdna analysis pipeline and translational oncology knowledgebase are open - source and available with documentation ( data supplement )  . we detected high ctdnatumor congruence , which , together with the absence of alterations from the blood cells used as germline samples and comprehensive ltering of mutations through clustering , maximizes the likelihood that the reported alterations originated from tumor and not from other sources , such as clonal hematopoiesis.1 indeed , our ltering approach using longitudinal samples removed false - positive alterations in all patients . 
rara was within the amplied region in plasma but not in primary omentu ( b ) erbb2 protein was overexpressed in cancer tissue ( arrowheads ) in immunohistochemistry ( ihc ) and the erbb2 gene was amplied in dna in situ hybridization ( ish ) analysis ( scale bars , 20 mm )  . 
the most informative comparisons for predicting treatment outcome are samples at the preoperative stage , after two cycles of chemotherapy , and after debulking surgery , because they provide information on treatment response and on persisting tumor subclones we identied potentially clinically applicable mutations or cnas in more than one half of the patients with hgsoc . these included two patients with mtor pathwayactivating mutations that were validated . 
both patients had a good response to the platinum - based rst - line therapy , but in the case of relapse they could most likely benet from mtor inhibitors alone or in combination with chemotherapy.22 in patient eoc429 , we identied alterations conferring both mtor pathway activation and hr deciency , which suggests potential benet from combination treatment with , for example , mtor inhibition and parp inhibition . 
in addition , two patients had more than one concurrent , potentially targetable alteration . patient eoc1067 progressed after 9 months of platinum - based therapy despite the fanca deletion conferring hr deciency , potentially because of the contribution of the cdk alterations on cell - cycle regulation and tumor progression.32 on the basis of the concurrent ckdn1b and ckdn2b deletions , this patient could potentially benet from a combination targeting both pathways , for instance , parp inhibitor and cdk4 / 6 inhibitor . these results indicate that longitudinal ctdna sampling can detect and monitor a relapse at an early stage and identify potentially effective drug combinations . we identied a high - condence erbb2 amplication in the ctdna of a patient with platinum - resistant hgsoc and used this information to change the patients treatment to include trastuzumab with reduced doses of platinum and paclitaxel . 
thus , rapid response to the ctdna - guided treatment , detected by complete normalization of ca - 125 values within 2 months after starting the combination treatment , was surprising . 
earlier studies that have combined erbb2 inhibitors with platinum and paclitaxel report similar encouraging responses for relapsed patients with advanced hgsoc.31 although the number of patients in these studies and our study remains small because of the low number of patients with erbb2 - amplied hgsoc , these results warrant testing erbb2 amplication from relapsed hgsoc patients with advanced disease . ctdna sampling and sequencing with a large panel offers several benets to physicians . 
for a detailed description of the disclosure categories , or for more information about ascos conict of interest policy , please refer to or po.ascopubs.org / site / ifc sakari hietanen consulting or advisory role : tesaro , astrazeneca travel , accommodations , expenses : roche pharma ag olli carp en stock and other ownership interests : orion corporation honoraria : merck kgaa , roche pharma ag sampsa hautaniemi stock and other ownership interests : nanostring technologies no other potential conicts of interest were reported . acknowledgment we thank the patients who participated in this study , dr tuulia vallius and dr zoltan maliga for critical review of the manuscript , ma tiia pelkonen for proof reading , and the csc - it center for science ltd . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
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 o duodenal - jejunal flexure gi stromal tumor frequently heralds somatic nf1 and notch pathway mutations purpose gi stromal tumors ( gists ) are commonly associated with somatic mutations in kit and pdgfra . 
we define the anatomic distribution of nf1 alterations in gist . methods we describe the demographic / clinicopathologic features of 177 patients from two institutions whose gists underwent next - generation sequencing of 315 cancer - related genes . results we initially identified six ( 9.7% ) of 62 gists with nf1 genomic alterations from the first cohort . 
of the five djf gists with any nf1 alteration , three ( 60% ) had kit mutations , and three ( 60% ) had notch pathway mutations ( notch2 , maml2 , cdc73 )  . 
we validated these findings in a second cohort of 115 gists , where two ( 40% ) of five unifocal nf1 - mutated gists arose at the djf , and one of these also had a notch pathway mutation ( ep300 )  . conclusion broad genomic profiling of adult gists has revealed that nf1 alterations are enriched in djf gists . 
 ( ie , kras , nras , hras ) by increasing the catalytic conversion of the active form ( ras - gtp ) to the inactive form ( ras - gdp ) .14 pathogenic nf1 variants disrupt the normal function of neurofibromin and result in constitutive ras activation.15 this activation increases downstream signaling through braf / craf - mediated activation of the mitogen - activated protein kinase pathway and hence , facilitates tumor initiation and progression.16 until recently , nf1 mutations in gist were believed to be primarily of germline origin , associated with clinical nf - 1 , and combined with a second somatic mutation in the tumor . 
thus , our understanding of nf1 in gist continues to evolve . approximately 30% of all gists occur in the small intestine , 1 which measures approximately 5 to 6 m in length.18 most small bowel gists are associated with somatic kit mutations , whereas a subset is associated with nf1 mutations.19 the small bowel is divided into three anatomically , histologically , and functionally distinct segments , namely the duodenum , jejunum , and ileum.18 although some studies distinguish duodenal gists from other small bowel gists , most combine them and do not characterize the biology of tumors on the basis of these distinct locations . 
moreover , the exact transition from jejunum to ileum is somewhat arbitrary , but the duodenal - jejunal flexure ( djf ) , also known as the ligament of treitz , represents a clear anatomic site that marks the transition from duodenum to jejunuto date , no study of gists has specifically characterized tumors that arise from the djf . 
the current study , however , started with presumably sporadic gists , which led to the unexpected finding that somatic nf1 mutations in gists are more prevalent than previously suspected and that they are enriched in tumors that arise from the djf . methods primary study population patient demographic and tumor clinicopathologic data were retrospectively collected in an unbiased fashion from every patient with pathologically confirmed gist seen within the university of california , san diego ( ucsd ) , health system from january 1 , 2000 , to april 30 , 2017 , under a ucsd institutional review boardapproved protocol . 
available operating notes or imaging reports were reviewed for these 165 patients to distinguish the primary site of origin of any small bowel gist as duodenal , djf , jejunal , or ileal . comprehensive genomic profiling of the 165 patients with gist in the cohort , 62 underwent next - generation sequencing ( ngs ) of coding regions of cancer - related genes . 
dna was extracted from formalin - fixed paraffin - embedded ( ffpe ) sections that contained a minimum of 20% tumor tissue and were used for comprehensive genomic profiling with hybridization - captured , adaptor ligationbased libraries . 
the number of genes in the foundationone panel has evolved over time as new data on cancer - related genes have been published and currently includes 315 cancerrelated genes plus select introns from 28 genes often rearranged or altered in solid tumor cancers . however , all versions of the assay simultaneously analyze the extracted dna for base substitutions , short insertions and deletions , amplifications and homozygous deletions , and gene rearrangements with > 99% sensitivity.20 specimens submitted to the ucsd clinical genomics laboratory underwent ngs of the exons of 397 genes involved in pathways that control growth or differentiation and are known to be frequently mutated in solid tumors . 
coverage depth ranged from 2833 to 8303 across all sequenced tumor samples from both the foundationone and the ucsd assays . nontumor tissue sequencing patients found to have nf1 mutations in their tumor tissue were also tested for germline nf1 mutation . four samples tested by using dna extracted from ffpe sections of adjacent normal tissue or peripheral blood underwent ngs cancer - related mutation panel testing by the ucsd clinical genomics laboratory as just described . 
one additional sample was tested by using commercially available targeted sequencing of the nf1 gene from peripheral blood by arup laboratories ( salt lake city , ut )  . secondary study population a confirmatory cohort of  . 
1 , 000 patients with pathologically confirmed gists from memorial sloan kettering cancer center ( mskcc ) with retrospectively collected patient demographic and tumor clinicopathologic data also were analyzed under an institutional review boardapproved protocol . 
data included age , sex , primary gist site , tumor size , and pathologic characteristics . one hundred fifteen patients with gists had ngs results available in the msk - impact ( integrated mutation profiling of actionable cancer targets ) platform , which characterized frozen or ffpe tumor specimens for somatic dna mutations , copy number alterations , and select rearrangements of 341 cancer - associated genes.21 statistical analysis all statistical analyses were performed with stata 9.0 software ( statacorp , college station , tx )  . comparisons between groups were performed by using the two - sample test of proportions . 
none of these patients had previously known clinical manifestations of nf - 1 ( eg , cafe au lait spots ; axillary / inguinal freckling ; dermal neurofibromas ; lisch nodules ; iris hamartomas ; nervous system tumors , including malignant peripheral nerve sheath tumors [ mpnsts ] , pancreatic neuroendocrine tumors , pheochromocytomas , or other sarcomas ] ) .10 therefore , the application of expanded ngs panels to characterize the mutational profile of gists identified an unappreciated subset of patients with nf1 genomic alterations in their tumors but no clinical evidence of nf - 1 . nf1 genomic alterations in gist frequently occur at the djf of the six patients with gist for whom we identified nf1 genomic alterations , five ( 83.3% ) had unifocal tumors at the djf , and one ( 16.7% ) had a unifocal tumor in the stomach ( fig 1a )  . 
the demographic , clinicopathologic , and genomic characteristics of these nine patients with djf tumors are listed in table 1 ( n = 7 ngs gists ) and the data supplement ( n = 2 non - ngs gists )  . 
given the infrequency of nf1 genomic alterations in gist , the djf appears to be an over - represented focus of nf1 mutant tumors . nf1 genomic alterations in gist are primarily somatic but can herald mild neurofibromatosis nf1 genomic alterations for each patient are listed in table 2 . 
although none of the patients had known prior clinical evidence of nf - 1 , we next obtained nontumor dna from blood or nontumor tissue to determine whether any of these patients had germline nf1 mutations . 
 ( a ) from a total of 165 patients ( university of california , san diego [ ucsd ] ) with pathologically confirmed gists , 62 had available next generation sequencing ( ngs )  . 
this finding is consistent with the mild phenotype / low penetrance reported in other patients with this germline nf1 mutation.22 nf1 genomic alterations in gists are associated with other cancer - related mutations at the genomic level , the ucsd cohort ngs data generally parallel the known distribution of driver mutations in gists ( fig 2 )  . 
of the 65 driver mutations identified in the 62 gists , oncogenic kit ( 63% ) , pdgfra ( 11% ) , and sdh subunit ( 11% ) mutations were most frequent , whereas braf and kras mutations were less common . moreover , nf1 mutations ( six of 65 ) represented 9% of total genomic alterations . 
the loss of the nf1 tumor suppressor gene often leads to additional chromosomal alterations , but second - hit mutations and / or loss of heterozygosity are necessary to promote tumorigenesis.23 therefore , we analyzed a cohort of five patients with nf1 mutant djf gists for additional cancer - related gene mutations . 
demographic and clinicopathologic characteristics of these two patients are listed in table 3 , with the characteristics of the remaining five patients without djf and / or multifocal gists listed in the data supplement . 
in addition to an nf1 mutation , one patient had a concomitant mutation in ep300 , which encodes a histone acetyltransferase / transcriptional coactivator that has been previously reported to interact with maml1 and maml2 to potentiate notch signaling.24 this supports our earlier observation that unifocal nf1 mutant djf gists also can have impaired notch signaling . 
in summary , 40% of unifocal nf1 mutant gists in the mskcc cohort were localized at the djf , which corroborates the high rate ( 83.3% ) of similar tumors in the ucsd cohort . 
we now show in two single - institution cohorts of patients with gists that 6.1% ( mskcc , seven of 115 ) to 9.7% ( ucsd , six of 62 ) have nf1 alterations . 
if we exclude the 17 patients who overlap with our previous study ( two of whom have nf1 mutations [ ucsd patients 3 and 5 in the current study ] ) , we show that 8.9% ( four of 45 ) of patients with gists have nf1 alterations . 
taken together , nf1 mutation frequencies range from 6% to 10% in gist and are higher than previously appreciated but similar to our recent analysis.7 for the first time in our knowledge , we show that broad genomic profiling of djf or ligament of treitz gists in adults reveals frequent nf1 alterations ( somatic and / or germline ) that occur even in the absence of clinical nf - 1 . 
 yes high high high high pathologic feature tumor resection yes tumor size , cm 13 mitotic index / 5 mm2 high cellular morphology mixed spindle / epithelioid histologic grade g2 immunostain positivity dog - 1 genomic alterations somatic kit ( af ) kit exon somatic nf1 ( af ) ( 30% ) none other somatic alterations ( af ) none table 2 . 
of the 62 patients with gi stromal tumors with available next generation sequencing , 65 known driver mutations were identified : 41 in kit , seven in pdgfra , six in nf1 , seven in succinate dehydrogenase ( sdh ) subunits ( a , b , c , or d ) , two in braf , and two in kras . awareness of the risk of additional tumors ( eg , dermal neurofibromas , nervous system tumors [ including mpnsts , pancreatic neuroendocrine tumors , pheochromocytomas , and other sarcomas ] ) 10 and allows for earlier screening of these nf - 1associated tumors , although whether different malignancies and gists have unique presentation patterns remains to be determined ; and diagnosis of nf - 1 allows for genetic counseling and testing of potentially affected family members . 
of note , individuals can have segmental mosaicism of nf - 1 , which occurs when an nf1 somatic mutation occurs early in embryonic development such that only the tissues derived from the nf1 - mutated cell carry the mutation while the remaining tissues are wild type.26 as with ucsd patient 2 , a clinical genetics work - up may be indicated for patients with nf1 mutations on tumor profiling that could indicate a germline rather than a somatic origin . tumor development in the setting of nf1 genomic alterations is associated with additional second - hit mutations.23 we now have shown that djf tumors with nf1 genomic alteration also can harbor concurrent kit mutations . 
in general , most kit mutations portend imatinib sensitivity , whereas nf1 mutations do not.3 , 27 consistent with this aforementioned drug sensitivity , tumors with a high risk of recurrence are recommended for adjuvant imatinib on the basis of the american college of surgeons oncology group z900128 and scandinavian sarcoma group xviii / aio29 trials where cumulative results demonstrated improved relapse - free survival ( rfs ) and overall survival with 36 months of adjuvant imatinib in patients with high - risk disease . 
in our cohort , three patients with djf gists had a high risk of recurrence by validated risk assessment models.30 , 31 ucsd patient 4 lacked a kit mutation and was predicted to not respond to imatinib therapy ; instead , this patient could experience toxicity . 
this approach was supported by eortc - 62005 and southwest oncology group s0033 / cancer and leukemia group b 150105 phase iii trials that collectively demonstrated improved response rates and rfs in patients with advanced gists and kit exon 9 mutations treated with high - dose imatinib ( 800 mg daily ) compared with standard - dose imatinib ( 400 mg daily ) .32 the patient also had a germline nf1 variant and ultimately developed a local recurrence after 5 years of adjuvant imatinib therapy . ucsd patient 3 had a known kit exon 11 mutation and was treated with dose - escalated imatinib followed by the multikinase inhibitor sunitinib for metastatic disease . 
a brief trial of the mammalian target of rapamycin inhibitor everolimus in combination with imatinib was attempted to block parallel signaling pathways , but the patient rapidly succumbed to the disease . much like patients with metastatic colorectal cancer who are tested for pan - ras mutations before treatment targeting upstream cell surface receptors ( ie , epidermal growth factor receptor ) , 33 , 34 we propose that patients with djf gists be tested for nf1 ( which would activate ras ) and braf v600e genomic alterations ( which two of the patients with djf gists also harbored ) before being offered imatinib therapy , which targets upstream kit . we have recently shown that notch1 can be mutated in both wild - type and nonwild - type gists.7 we now add evidence that implicates the notch signaling pathway in gists . 
we identified another tumor with a mutation in cdc73 , which encodes the rna polymerase iiassociated factor complex protein parafibromin and was recently reported to potentiate notch signaling by binding to the nicd.36 we also found an ep300 mutation in the validation cohort that could abrogate signaling of the notch transcriptional complex . of note , notch signaling was reported to have a tumor suppressor function in gist by downregulating kit mrna expression.37 this prior study also demonstrated that patients with gists with low hes1 expression had shorter rfs times than those with high hes1 expression . whether loss - of - function mutations in notch pathway genes that lead to decreased hes1 expression contribute to gist tumorigenesis remains to be determined . 
nf1 regulates mek / smad3 / jagged1 / hes1dependent glial and neuronal differentiation.38 notch has also been reported to mediate transformation of benign plexiform neurofibromas into mpnsts in the setting of nf - 1 , 39 which suggests an alternate oncogenic role of notch in nf - 1 . 
more studies are required to elucidate the biologic significance of notch pathway mutations in gist , including nf - 1associated gist . finally , the mechanism by which nf1 mutations lead to gists that specifically arise at the djf remains unclear . 
summary of duodenal - jejunal flexure genomic alterations . tumor size , mitotic index ( mi ) , and genomic alterations for patients with duodenal - jejunal flexure gi stromal tumors ( gists ) from both cohorts are presented and organized by known driver genes and notch pathway alterations . somatic and germline mutations are annotated by color for mutation type . snp , single nucleotide polymorphism . cdc73 ep300 notch2 maml2 asxl1 men1 erbb4 tsc2 bcor ( per 5 mm2 ) high unknown genomic alteration nonsense frameshift missense in - frame indel deletion splicing ( somatic ) ( germline ) ( somatic ) braf ( somatic ) arid1a ( somatic ) notch pathway other pacemaker activity.42 one could postulate that this region of chromatin on 17q is open and transcriptionally active at the djf . 
belinsky no relationship to disclose margaret von mehren consulting or advisory role : cytrx , blueprint medicines , janssen pharmaceuticals , deciphera pharmaceuticals research funding : arqule travel , accommodations , expenses : janssen pharmaceuticals , blueprint medicines , novartis , arog pharmaceuticals other relationship : national comprehensive cancer network john a . 
thorson no relationship to disclose lisa madlensky employment : janssen pharmaceuticals ( i ) patents , royalties , other intellectual property : husband has patents through his employment with janssen pharmaceuticals ; these are methods patents and not related to any therapeutics ( i ) timothy bowler employment : regenxbio ( i ) stock and other ownership interests : regenxbio ( i ) francesco dangelo no relationship to disclose dwayne g . 
sicklick , university of california , san diego , la jolla , ca ; martina de siena and francesco dangelo , sapienza e universit `a di roma , rome , italy ; benjamin medina , timothy bowler , and ronald p . 
ma gl , murphy jd , martinez me , et al : epidemiology of gastrointestinal stromal tumors in the era of histology codes : results of a population - based study . 
hechtman jf , zehir a , mitchell t , et al : novel oncogene and tumor suppressor mutations in kit and pdgfra wild type gastrointestinal stromal tumors revealed by next generation sequencing . 
burgoyne am , somaiah n , sicklick jk : gastrointestinal stromal tumors in the setting of multiple tumor syndromes . curr opin oncol 26 : 408 - 414 , 2014 11 . 
belinsky mg , rink l , cai kq , et al : somatic loss of function mutations in neurofibromin 1 and myc associated factor x genes identified by exome - wide sequencing in a wild - type gist case . 
miettinen m , fetsch jf , sobin lh , et al : gastrointestinal stromal tumors in patients with neurofibromatosis 1 : a clinicopathologic and molecular genetic study of 45 cases . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
messiaen l , vogt j , bengesser k , et al : mosaic type - 1 nf1 microdeletions as a cause of both generalized and segmental neurofibromatosis type - 1 ( nf1 )  . 
dematteo rp , ballman kv , antonescu cr , et al : adjuvant imatinib mesylate after resection of localised , primary gastrointestinal stromal tumour : a randomised , double - blind , placebo - controlled trial . 
gastrointestinal stromal tumor meta - analysis group ( metagist ) : comparison of two doses of imatinib for the treatment of unresectable or metastatic gastrointestinal stromal tumors : a meta - analysis of 1 , 640 patients . 
pietrantonio f , cremolini c , petrelli f , et al : first - line anti - egfr monoclonal antibodies in panras wild - type metastatic colorectal cancer : a systematic review and meta - analysis . 
sorich mj , wiese md , rowland a , et al : extended ras mutations and anti - egfr monoclonal antibody survival benefit in metastatic colorectal cancer : a meta - analysis of randomized , controlled trials . 
hansen , md , phd1 , 2 ; lars henrik jensen , md , phd1 , 2 ; and anders jakobsen , dmsc1 , 2 purpose analysis of circulating tumor dna ( ctdna ) is a potential improvement in precision medicine . 
plasma samples represented healthy donors and localized and metastatic crcs . results the level of neuropeptide ymethylated dna in the tissue cohorts differed between nonmalignant and malignant / premalignant tissues with minimal overlap . 
furthermore , meth - ctdna was detected in plasma from 100% of patients with metastatic disease , compared with 67% of those with localized disease and 8% of healthy donors . 
2019 by american society of clinical oncology introduction circulating tumor - specic dna ( ctdna ) is an attractive biomarker for obvious reasons , such as easily repeated access , better reection of overall tumor biology , and timely correct tumor mutational status . 
consequently , the era is marked by enthusiasm , but it should be noted that its clinical utility , with few exceptions , remains to be proven.1 ctdna can be determined by the presence of tumorspecic genetic or epigenetic alterations . 
ngs allows identication of mutations of interest and is a relatively broad approach applicable in the identication of mutational patterns and quantication of specic mutations , but this method is time and resource consuming . 
different platforms may lead to contradictive results , as shown in a recent report , with only 60% agreement between analyses of the same mutations.2 the second method relies on pcr with analysis of specic mutations . 
compared with ngs , pcr , especially digital pcr , has a faster data turnaround time3 and lower costs , but direct pcr is only applicable in the fraction of patients with known specic mutations . in colorectal cancer ( crc ) , ras / raf mutations are of interest , because their presence in tumor tissue contraindicates treatment with monoclonal antibodies cetuximab and panitumumab . 
multiplex technology allows for screening of 27 mutations in the same analysis , 4 but even so , only approximately 60% of patients present with a ras / raf - mutated tumor . 
 thomsen et al context key objective can circulating tumor - specic methylated dna serve as a universal biomarker in colorectal cancer ? knowledge generated methylated dna was tumor specic in different cohorts including tissue as well as plasma . 
high correlation was found between mutated and methylated dna in both localized and metastatic disease . relevance circulating tumor - specic methylated dna holds promise as a universal colorectal cancer marker that can be analyzed in a simple , highly reproducible approach . most of these patients , the same tumor - specic mutation is detectable in ctdna ( mut - ctdna )  . 
dna was eluted in 50 ml of nuclease - free water and further diluted with nuclease - free water , if necessary . aberrant methylation is an early event in carcinogenesis and occurs in almost all malignant tumors as methylation of promoter regions causing inactivation of genes . 
this , along with the stability of methylation changes , makes it a relevant biomarker for early diagnosis.5 analysis of abnormally methylated dna in plasma ( meth - ctdna ) has been proposed for screening , 6 and a test for crc has been approved by the us food and drug administration.7 however , because of insufcient sensitivity and specicity , it has not been generally accepted . 
the neuropeptide y gene ( npy ) has been correlated with invasion and proliferation.8 , 9 exogenous npy has been shown to inuence the growth of malignant cholangiocarcinoma cells in vitro and inhibit invasion of crc cells . 
in this disease , hypermethylation of the npy promoter region has been correlated with inactivation of gene expression and therefore carcinogenesis , and currently , hypermethylation of the npy gene is suggested as a blood - based biomarker.10 - 12 the purpose of our study was to compare mutated dna with methylated dna in malignant and nonmalignant colorectal tissue and plasma with the aim of determining a method applicable in all patients with crc . plasma sampling and purication in edta tubes , 9 - ml blood samples were collected from donors and different cohorts of patients . 
plasma was centrifuged again at 10 , 000 g for 10 minutes before purication , and cysteine - rich polycomb - like protein 1 ( cpp1 ) dna fragments were added as exogenous internal control.13 dna from patients was puried from 2 2 or 2 4 ml of plasma on the qiasymphony sp instrument using the qiasymphony circulating nucleic acid kit ( qiagen , hilden , germany ) according to manufacturer instructions . dna from healthy donors was puried from 1 4 ml of plasma . dna was eluted in 60 ml of the supplied buffer and water added to 400 ml . 
three 15 - mm slices of ffpe tissue were subjected to 180 ml of incubation buffer and 20 ml of protein kinase k overnight at 70c ; 400 ml of lysis buffer adenomas and tumor tissue samples were screened for ras / raf mutations as previously described.14 samples from adjacent tissue and plasma were analyzed for the specic mutation by droplet digital pcr in two wells . positive controls for each mutation ( gblocks ; idt , carolville , ia ) or mutated fragments generated according to spindler et al , 15 genomic donor dna , and water were included in the analyses as controls . 
patients with mcrc had plasma analyzed both at baseline and after the rst treatment cycle . tissue methylation in 25 nonneoplastic specimens , all but one were nonmethylated ( 4% were npy positive )  . 
figure 1 shows the results of the tissue npy methylation analysis , with methylated npy presented as actual clearly shows that the level of npy methylation was different in malignant and nonmalignant tissues . 
the range of npy fractions . mutated and methylated dna in colorectal cancer methylation analysis tumor - specic methylated dna was dened as dna with methylation of the npy gene.12 before droplet digital pcr methylation analysis , bisulte conversion of circulating and ffpe - isolated dna was performed as recommended by the manufacturer ( zymo research , irvine , ca )  . 
water and a pool of lymphocyte dna from cancer - free individuals were included in each round of analyses as negative controls ; universal human methylated control dna ( zymo research ) and epitech control dna ( qiagen ) were included as positive controls . 
the upper limit of the 95% ci was 1.8% , and therefore , the cutoff value was set to 2% . limit of blank in plasma limit of blank ( lob ) in the mutation analysis was determined by donor controls . 
because fewer than two fampositive droplets were observed in all analyses of the genomic donor dna controls and plasma dna from healthy individuals as previously described , 16 plasma samples with more than two fam - positive droplets in two wells were classied as positive . lob in the methylation analysis was dened as the quantity of npy droplets counted in control dna samples from a test cohort of healthy individuals ( n = 50 )  . 
correlations are also illustrated in the scatter plots shown in figures 3 , 4a , and 4b , which represent correlation between meth - ctdna and mut - ctdna in the localized and metastatic settings at baseline and in the metastatic setting after the rst treatment cycle , respectively . discussion our study on tissue and plasma samples from donors and different stages of crc indicates that meth - ctdna correlated with mut - ctdna across the cohorts and that methctdna was detectable in cases without activating dna mutations . 
therefore , meth - ctdna may be a universal biomarker in crc from the perspectives of detection and monitoring . key challenges in cancer management are early diagnosis and close monitoring during treatment and follow - up with minimal harm to the patients . 
in the landscape of tumor markers , ctdna represents a relatively new approach with the potential for progress in cancer management , because it contains the same molecular alterations as the corresponding tumor and potential metastases . 
even so , clinical utility has been limited . recently , presence of ctdna was conrmed in wt patients using epigenetic modications such as hypermethylation.17 - 19 meth - ctdna seems to represent tumor - specic dna and is found in nearly all colorectal adenocarcinomas , 10 as opposed to ctdna based on ras / raf mutations . 
three recent studies have suggested that hypermethylation of the npy gene may serve as a biomarker for monitoring the treatment of crc , 10 , 11 , 20 but a detailed comparison of mutated and methylated dna motivated our study . the level of methylation varied among different cohorts with malignant and nonmalignant tissues , the latter in general being negative . 
fifty healthy donors were only analyzed for methylated ctdna ( methctdna ) , and 20 healthy donors were analyzed for kras g12d mutated ctdna ( mut - ctdna )  . 
plasma was drawn from patients with localized ras / raf - mutated tumors ( n = 27 ) and metastatic ras / rafmutated tumors ( n = 20 ) and analyzed for the same specic mutations and methylation . methylation in tumors did not overlap that of nonmalignant npy methylation , except in three cases ( 3% )  . plasma methylation figure 2 shows the plasma analysis of different cohorts . samples from healthy donors showed that four ( 8% ) of 50 had detectable meth - ctdna above the lob . 
furthermore , the analysis showed that 67% ( 18 of 27 ) of patients with localized crc had mut - ctdna , compared with 52% ( 14 of 27 ) with meth - ctdna . 
scatter plot showing correlation of methylated circulating tumor dna ( ctdna ) and mutated ctdna ( mut - ctdna ) in localized disease . almost complete separation of malignant and nonmalignant tissues based on the statistical variation of the observed frequencies in healthy individuals . 
adjacent tissue showed npy hypermethylation in one third of the samples , although they were just positive ; none were mutated , despite ras / raf mutations in the nearby tumor . 
scatter plots showing correlation of methylated circulating tumor dna ( ctdna ) and mutated ctdna ( mut - ctdna ) in metastatic colorectal cancer ( a ) at baseline and ( b ) after one cycle of treatment . furthermore methylation is an early event in carcinogenesis , 22 which may represent a potential universal biomarker.23 all tumor tissue samples were hypermethylated irrespective of mutational status and to the same extent as ras / raf - mutated adenomas . 
this indicates that aberrant methylation takes place as an early part of cancer progression , which can predispose to additional genetic alterations.24 possibly , these epigenetic changes give an important and early window for therapeutic interventions in patients with crc . plasma analyses showed that the frequency of patients with ctdna varied depending on disease stage . 
lob of two positive droplets per reaction determined in a test cohort of 50 healthy donors seems in good agreement with previous results reporting an lob of 3.30 on the basis of 17 control dna samples without hypermethylated npy.11 the two self - reported healthy donor cohorts with 4% ( two of 50 ) and 8% ( four of 50 ) of patients having more than two positive droplets per reaction indicate good agreement . 
therefore , occurrence of aberrant methylation with increasing age does not seem to be a major problethe false - positive rate may be acceptable for patients with advanced disease , and therefore , clinical application of meth - ctdna in metastatic disease seems encouraging . 
in localized tumors , two thirds of patients harbored mut - ctdna and meth - ctdna , which is in accordance with current literature.10 in the metastatic setting , all indicating its potential as patients had meth - ctdna , a general biomarker . 
they found that 77% had detectable ctdna at baseline , assessed by mut - ctdna and meth - ctdna . boeckx et al11 reported that 87.5% of all baseline plasma samples were positive for npy methylation in 24 patients with mcrc . 
varying methods of analysis , which lack standardization throughout the eld of research in ctdna , are one obvious reason for the lower frequency of patients with detectable ctdna compared with our ndings . correlation between mut - ctdna and meth - ctdna was investigated to compare the two potential biomarkers . 
this is in agreement with previous studies concluding that methylated markers in ctdna could replace tumor - specic mutations in the blood.10 this conclusion was based on a correlation coefcient of r = 0.94 between mut - ctdna ( kras , braf , and tp53 ) and meth - ctdna ( npy )  . 
we did not investigate the potential role of meth - ctdna in monitoring wt patients , but we found a strong correlation between mut - ctdna and meth - ctdna after one cycle of treatment , which emphasizes the role of meth - ctdna in treatment monitoring . 
taken together , the current literature indicates high agreement between mut - ctdna and meth - ctdna , 10 , 11 , 20 further supported by our results . a minor disadvantage in the methylation assays is the need for bisulte conversion , which can degrade dna and therefore requires additional material . 
however , the need for prior establishment of mutation status , as with mutctdna , is bypassed , and therefore , meth - ctdna is applicable in nearly all patients with crc . 
it should be noted that meth - ctdna is not relevant in the selection of patients for targeted treatment with epidermal growth factor receptor inhibitors . in conclusion , to our knowledge , our study represents the rst detailed comparison of methylated and mutated dna in normal tissue as well as in localized and metastatic tumors . 
this indicates that hypermethylated npy in plasma is applicable as a universal biomarker in all patients with mcrc , but further investigation of clinical utility is warranted . affiliations 1danish colorectal cancer center south , vejle hospital , vejle , denmark 2university of southern denmark , odense , denmark relationships are self - held unless noted . 
all relationships are considered compensated . lars henrik jensen research funding : merck sharp & dohme ( inst ) travel , accommodations , expenses : bayer healthcare pharmaceuticals no other potential conicts of interest were reported . acknowledgment we thank the study participants and the staff at vejle hospital who collected samples for this study . 
merker jd , oxnard gr , compton c , et al : circulating tumor dna analysis in patients with cancer : american society of clinical oncology and college of american pathologists joint review . 
jama oncol 4 : 868 - 870 , 2018 thierry ar , el messaoudi s , mollevi c , et al : clinical utility of circulating dna analysis for rapid detection of actionable mutations to select metastatic colorectal patients for anti - egfr treatment . 
front mol biosci 2 : 13 , 2015 church tr , wandell m , lofton - day c , et al : prospective evaluation of methylated sept9 in plasma for detection of asymptomatic colorectal cancer . 
boeckx n , op de beeck k , beyens m , et al : mutation and methylation analysis of circulating tumor dna can be used for the follow - up of metastatic colorectal cancer patients . 
roperch jp , incitti r , forbin s , et al : aberrant methylation of npy , penk , and wif1 as a promising marker for blood - based diagnosis of colorectal cancer . 
spindler kl , pallisgaard n , vogelius i , et al : quantitative cell - free dna , kras , and braf mutations in plasma from patients with metastatic colorectal cancer during treatment with cetuximab and irinotecan . 
thomsen cb , hansen tf , andersen rf , et al : monitoring the effect of rst line treatment in ras / raf mutated metastatic colorectal cancer by serial analysis of tumor specic dna in plasma . 
garlan f , laurent - puig p , sefrioui d , et al : early evaluation of circulating tumor dna as marker of therapeutic efcacy in metastatic colorectal cancer patients ( placol study )  . 
step two was 44 cycles at 95c for 15 seconds and 56c for 1 minute , with a 1.5c per second ramp rate . step three was at 98c for 10 minutes . 
 c subgrouping of unfavorable histology neuroblastomas with immunohistochemistry toward precision prognosis and therapy stratication naohiko ikegaki , phd1 and hiroyuki shimada , md , phd2 , for the international neuroblastoma pathology committee introduction neuroblastoma , as well dened by willis , 1 is an embryonal tumor of neural crest origtumors of the neuroblastoma group include neuroblastoma , ganglioneuroblastoma , and ganglioneuroma . 
we believe that all ganglioneuromas were once neuroblastomas in the early stage of tumor development.1 , 2 they are collectively called peripheral neuroblastic tumors ( pnts ) and are known to present with a wide range of clinical behavior , from spontaneous regression and tumor maturation to aggressive progression that is refractory to intensive treatment . 
these observations have led us to seek additional immunohistochemical biomarkers that are tightly associated with aggressive behaviorsthat is , unresponsiveness or resistance to the current intensive multimodal therapyof certain uh tumors . 
to address this problem , we and others have sought and identied the expression of potentially drug - targetable proteins that are responsible for their aggressive progression in the uh group . 
when we seek such biomarkers , they are preferably actionable / druggable by existing pharmaceutical agents , us food and drug administration approved , or currently tested in human clinical trials . 
of note , these three types of highly aggressive neuroblastomasthat is , myc - driven neuroblastoma , alt phenotype neuroblastoma because of atrx loss , and tert - overexpressing neuroblastoma with gene rearrangementare mutually exclusive and seem to comprise the majority of therapy - resistant or refractory uh neuroblastomas . these three markersthat is , myc family proteins , tert , and atrx can be the subjects of immunohistochemical assay and potentially incorporated in future inpc . it should be noted that other than the above gene and expression alterations found in aggressive uh neuroblastomas , alk mutations and amplication are found in approximately 10% of sporadic neuroblastoma cases.20 , 21 it was also found that alk gene amplication and f1174 mutations are associated with mycn amplication.22 moreover , alk overexpression as a result of alk amplication / mutations seems to be responsible for its oncogenic activity23 ; however , the prognostic signicance of alk mutations / overexpression has been controversial , as some reports suggest an association of alk mutations / overexpression with fatal outcomes of the disease , whereas others suggest otherwise.22 , 23 in particular , regairaz et al24 showed immunohistochemically that expression of alk and its active form palk was observed in many neuroblastomas independent of alk mutation / amplication . 
in this regard , myc / mycn and tert overexpression26 - 29 has been linked to the stemness of tumor cells , and direct and indirect therapeutic targeting of these alterations suppresses the stemness of aggressive and therapy - resistant uh neuroblastomas . 
similarly , alt is linked to tumor stem cells.30 , 31 these observations allow us to incorporate the information into the inpc toward the goal of precision prognosis and therapy stratication . our plan is to rene the uh neuroblastoma stratication using immunohistopathologic analysis with antipan - myc antibody ( or anti - mycn and anti - myc ) , anti - tert antibody , and anti - atrx antibody . 
it is expected that the nonresponder to current high - risk therapymyc , tert , and atl subgroups could be separated from the possible respondernull subgroupwith a high probability before the initiation of therapy : myc subgroup : myc - driven neuroblastoma shows augmented expression of mycn protein and / or myc proteas myc family protein overexpression stimulates rrna synthesis and protein translation , neuroblastoma cells in this subgroup often exhibit prominent nucleolar formationnucleolar hypertrophyand hypertrophic cell morphology.13 , 14 because of the presence of one to a few prominent nucleoli , myc - driven neuroblastoma is cytologically distinguishable from the conventional small blue - cell neuroblastoma with salt - and - pepper nuclei . myc - driven neuroblastomas , which comprise more than 50% of high - risk neuroblastomas , includes rare and unique tumor , named large - cell neuroblastoma , characterized by the bulls eye appearance of enlarged and uniquely open euchromatin - rich nuclei that contain highly conspicuous nucleoli.33 most large - cell neuroblastomas overexpress higher levels of mycn or myc protein than other myc - driven neuroblastomas . 
their euchromatin - rich open nuclei suggest the stem celllike nature of the tumor cells.29 a considerable number of myc - driven neuroblastomas are also associated with tert overexpression , as tert is a direct transcriptional target of myc family proteins . 
tert can also stabilize myc protein via its noncanonical enzymatic function , creating a positive feedback loop between mycn / myc and tert expression.34 , 35 tert subgroup : tert is the protein component of telomerase , which also includes terc , the telomerase rna component . 
immunohistochemical grading of tert is performed in essentially the same way as that of myc family proteins . estimated survival of each subgroup is based on wang et al12 and valentijn et al.18 to exclude the possibility of overlooking alt cases with atrx point mutations with no atrx loss and / or rare daxx mutations , patients older than age 5 years in the null group can be subjected to additional screening by either rdna32 or telomeric uorescence in situ hybridization assay.32a likely a result of long - range genomic rearrangements but not to promoter mutations in neuroblastoma.36 tert promoter hypermethylation may also be involved in its activating mechanism.37 , 38 alt subgroup : atrx loss results in the alt phenotype . atrx mutation is rarely observed in the myc and tert subgroups , and loss of atrx is exclusively observed in patients with neuroblastoma older than age 5 years.17 because a normal atrx function is to insert the variant histone h3 , namely h3.3 , in concert with daxx , into chromatin to maintain transcriptionally active euchromatin , 39 atrx loss may result in a more transcriptionally inactive heterochromatic state . 
thus , histologic / cytologic appearance of the alt subgroup could be the conventional type with salt - and - pepper nuclei . null subgroup : there are still uh neuroblastomas without myc family protein overexpression , tert overexpression , and atrx loss . 
strategies under consideration include , but are not limited to , transcriptional repression of myc and mycn genes by g - quadruplex ( g4 ) stabilizers , 42 , 43 bromodomain and extraterminal protein inhibitors , 44 , 45 and inhibitors of a transcriptional cyclin - dependent kinase 746 , 47 ; destabilization of mycn by aurora kinase a inhibitors48 and of myc and mycn proteins by ras signaling pathway inhibitors49 - 51 ; and translational blockade of myc mrna by eif4f inhibition and stabilization of rna g4 by rna g4 ligands.52 , 53 we recognize that uh tumors with high - level myc family protein expression tend to exhibit hypertrophic nucleoli , 13 , 14 which indicates that they are highly active in rrna synthesis and protein translation . 
small - molecule inhibitors , including cx - 5461 , an rna polymerase i inhibitor , and halofuginone , a protein translation inhibitor , could therefore effectively target these pathophysiologic features . as we have shown , these inhibitors in fact downregulate myc family protein expression in neuroblastoma cells.13 for those patients with tert - overexpressing neuroblastoma , telomerase inhibitors can be considered . 
if so , is there any other way by which the alt phenotype can be suppressed ? to address this question , we need to understand the mechanism of how atrx loss leads to alt . 
it has become evident that the acquisition of the alt phenotype uses the dna replication stress response , 30 which involves a cascade of events , including the obligatory activation of atr ( ataxia telangiectasia and rad3 related ) kinase . azd6738 is a novel potent and selective inhibitor of atr kinase with ic50 values of less than 1 mm in cell - based assays58 and would effectively target alt tumor cells . conclusion prognosis and therapy stratication of neuroblastomas have steadily improved since the introduction of the evans staging system59 with age used as a prognostic factor60 ; however , 5 - year survival of patients with high - risk neuroblastoma , dened by the international neuroblastoma risk group system ( inrg ) , remains at approximately 40% or lower.61 , 62 the same is true for the uh neuroblastoma group , which essentially overlaps high - risk neuroblastomas.8 , 63 unfortunately , no additional renement for the inrg has been proposed since 2009.61 the proposed histologic subgrouping of uh neuroblastomas represents a practical and immediately implementable approach with which to create the category leading to the most devastating clinical outcome , namely extremely unfavorable histology ( euh ) neuroblastoma . 
we expect that conventional uh neuroblastoma tumorsthat is , the null subgroupwould , we hope , respond to the current multimodal high - intensity therapy designed for high - risk neuroblastoma , whereas euh tumorsthat is , those of the myc , tert , and alt subgroupswould not . 
for those euh tumors , appropriate therapy protocols will have to be designed and tested . on the basis of our ndings , 12 myc family protein immunohistochemistry is already incorporated in the childrens oncology group pathology analysis as an integrated biomarker of neuroblastoma . 
similar attempts are now underway for tert and atrx immunohistochemistry for precision prognosis and the stratication of neuroblastoma . furthermore , we are planning to perform correlative studies between tert protein expression and tert gene rearrangements and between atrx protein loss and atrx gene mutations / deletions . 
for more information about ascos conict of interest policy , please refer to or po.ascopubs.org / site / ifc . no potential conicts of interest were reported . references willis r : neuroblastoma and ganglioneuroma . 
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 o graft - versus - leukemia effect of allogeneic stem - cell transplantation and minimal residual disease in patients with acute myeloid leukemia in first complete remission purpose the detection of minimal residual disease ( mrd ) in patients with acute myeloid leukemia ( aml ) may improve future risk - adapted treatment strategies . 
we assessed whether mrd - positive and mrd - negative patients with aml benefit differently from the graft - versusleukemia effect of allogeneic hematopoietic stem - cell transplantation ( allohsct )  . methods a total of 1 , 511 patients were treated in subsequent dutch - belgian hemato - oncology cooperative group and the swiss group for clinical cancer research aml trials , of whom 547 obtained a first complete remission , received postremission treatment ( prt ) , and had available flow cytometric mrd before prt . 
prt consisted of allohsct ( n = 282 ) , conventional prt by a third cycle of chemotherapy ( n = 160 ) , or autologous hematopoietic stem - cell transplantation ( n = 105 )  . results mrd was positive in 129 patients ( 24% ) after induction chemotherapy before proceeding to prt . 
2017 by american society of clinical oncology introduction acute myeloid leukemia ( aml ) is a heterogeneous malignancy characterized by a variety of underlying cytogenetic and molecular aberrations , which are associated with distinct prognostic features.1 although current treatment approaches induce high percentages of hematologic remission , relapse rates are high and vary according to the underlying risk profile.2 recently , the european leukemianet ( eln ) developed an updated classification on the basis of cytogenetic and molecular aberrancies distinguishing patients with a favorable , intermediate , jurjen versluis burak kalin wendelien zeijlemaker jakob passweg carlos graux markus g . 
therefore , we evaluated whether and to what extent allohsct quantitatively reduces relapse compared with conventional prt in upfront - treated patients with mrd - positive or mrd - negative aml in first cr ( cr1 )  . assessed for eligibility hovon - sakk aml42a hovon - sakk aml92 hovon - sakk aml102 ( n = 1 , 511 ) ( n = 511 ) ( n = 142 ) ( n = 858 ) excluded obtained no cr received no prt no available mrd ( n = 964 ) ( n = 255 ) ( n = 234 ) ( n = 475 ) patients eligible for analysis ( n = 547 ) mrd negative ct auto allo ( n = 418 ) ( n = 118 ) ( n = 89 ) ( n = 211 ) mrd positive ct auto allo ( n = 129 ) ( n = 42 ) ( n = 16 ) ( n = 71 ) methods patients patients participated in three prospective , consecutive dutch - belgian hemato - oncology cooperative group and the swiss group for clinical cancer research ( hovon - sakk ) collaborative group trials ( aml42 , aml92 , and aml102 ; the netherlands trial register numbers ntr230 , ntr1446 , and nrt2187 , respectively ) , for whom assessment of mrd after induction therapy and before prt by allohsct , chemotherapy , or autologous hsct ( autohsct ) was performed.25 , 26 the results of the aml92 trial have not yet been published , but trial information is available in the netherlands trial register ( ntr1446 )  . 
patients were excluded if cr1 did not occur after two induction cycles of chemotherapy ( n = 255 ; 17% ) or the patient did not receive prt after obtaining cr1 ( n = 234 ; 15% )  . 
in addition , a total of 475 patients ( 31% ) received prt in cr1 ; however , their mrd status was not available within a time window of 4 months before prt . 
patients were classified by aml prognostic risk on the basis of the cytogenetic and molecular profile of the underlying aml , according to the eln2017 risk classification.3 molecular analysis was available for the majority of patients , specifically for npm1 ( 93% ) ; fms - like tyrosine kinase 3 internal tandem duplication ( flt3 - itd ; 91% ) , including the flt3 - itd mutant to wild - type ratio ( 86% ) ; evi1 ( 79% ) ; asxl1 ( 83% ) ; runx1 ( 47% ) ; and tp53 ( 47% )  . 
patient characteristics mrd negative ( n = 418 ) mrd positive ( n = 129 ) wbc count at diagnosis , 109 / l cytogenetics of aml cytogenetic abnormalities monosomal karyotype characteristic male female age , years median range < 100  . 
prt included a third cycle of chemotherapy with mitoxantrone and etoposide , high - dose chemotherapy with busulfan and cyclophosphamide followed by autohsct , or allohsct after either myeloablative conditioning or reduced intensity conditioning ( ric )  . 
the myeloablative conditioning regimen contained high - dose cyclophosphamide with at least 8 gy total body irradiation ( tbi ) in 83 patients ( 76% ) ; the remainder of the patients received busulfan with cyclophosphamide . 
although ric regimens varied , the majority contained low - dose ( 2 or 4 gy ) tbi preceded by fludarabine ( n = 126 ; 77% ) , whereas 23% of the patients received fludarabine with busulfan . 
these different prt modalities were applied according to a riskadapted strategy : patients with aml classified as favorable risk , according to cytogenetic and molecular analysis , were planned for a third cycle of chemotherapy ; intermediate - risk patients were preferentially treated with allohsct using an hla - matched sibling donor or a fully hlamatched unrelated donor , if available ; patients with adverse - risk aml proceeded to allohsct using a sibling donor , an unrelated donor , or cord blood grafts ; and patients alternatively received autohsct or a third cycle of chemotherapy if no suitable donor was available.25 - 28 mrd detection and sample selection mrd flow cytometric analysis was performed in a two - step procedure , as previously described.18 in summary , the immunophenotype was determined on blasts defined by cd45 expression with a low sideward scatter . 
mrd percentage was defined as the percentage of laip cells within the wbc compartment multiplied by the correction factor ( 100% divided by the percentage of laippositive blasts at diagnosis )  . 
patient characteristics ( continued ) characteristic year of prt median range mrd negative ( n = 418 ) mrd positive ( n = 129 ) p = .11 2011 2006 - 2014 2010 2006 - 2014 abbreviations : aml , acute myeloid leukemia ; cn - x - y , cytogenetically normal or only loss of x or y chromosome ; cr , complete remission ; eln2017 , european leukemianet 2017 ; hsct , hematopoietic stem - cell transplantation ; iqr , interquartile range ; flt3 - itd , fms - like tyrosine kinase 3 internal tandem duplication ; mrd , minimal residual disease ; npm1 , nucleophosmin - 1 ; prt , postremission treatment . * the cutoff of the flt3 - itd ratio is defined as 0.50. number of induction courses ( ie , i or ii ) was performed to allow the baseline hazard to differ between these two patient groups . 
all analyses were performed with stata software ( release 13.1 ; stata corporation , college station , tx )  . results patient characteristics a total of 547 patients with aml in cr1 and available mrd status proceeded to prt with either allohsct ( n = 282 ) , chemotherapy ( n = 160 ) , or autohsct ( n = 105 )  . 
patients with mutated npm1 were more frequently mrd negative , whereas mrd - positive patients more frequently tended to obtain a late cr1 ( ie , after induction cycle 2 )  . 
the eln2017 risk classification was similarly distributed among the mrd - negative and mrd - positive patients . interestingly , the time interval from cr1 to prt for patients with mrd - positive aml was shorter compared with their negative counterparts , which was mainly apparent in favorablerisk patients with aml . 
no other differences with regard to donor source , conditioning , cytomegalovirus serostatus , and european group for blood and marrow transplantation ( ebmt ) risk score were apparent between mrd - negative and mrdpositive patients . 
patients with a high risk of nrm according to the ebmt risk score32 ( > 3 points ) represented 45% of the patients who underwent transplantation . treatment outcome os and rfs were significantly better in patients without mrd before prt compared with mrdpositive patients ( 65% 6 2% v 50% 6 5% at 4 years ; p = .002 ; and 58% 6 3% v 38% 6 4% ; p , .001 , respectively ; figs 2a and 2b )  . 
the sample with the shortest time interval between prt and the date of collection was selected for analysis . end points the primary end point of the study was the cumulative incidence of relapse . 
the cumulative risks of relapse and nrm over time were calculated as competing risks with actuarial methods , where patients alive in continuing cr1 were censored at the date of last contact . statistical methods a time - dependent analysis of prt was performed as described previously28 , 29 by applying multivariable cox regression with allohsct as the timedependent covariable . 
in both the multivariable analysis and the estimation of the survival curves , these patients were counted as at risk in the chemotherapy group from the start of prt until allohsct and after that as at risk in the allohsct group . 
more detailed outcome estimates according to mrd status , type of prt , and risk of nrm on the basis of the ebmt risk score are presented in the data supplement . the cumulative incidence of relapse was significantly lower in patients without mrd receiving allohsct compared with chemotherapy or autohsct ( 26% 6 3% v 38% 6 3% at 4 years ; p = .027 , respectively ; fig 3a )  . 
the cumulative incidence of relapse in mrd - positive patients is estimated to be 45% 6 6% compared with 66% 6 6% at 4 years ( p = .058 ) for recipients of allohsct compared with recipients of chemotherapy or autohsct , respectively ( fig 3b )  . 
rfs after allohsct proved similar compared with prt with chemotherapy or autohsct in patients without mrd before prt ( 58% 6 4% v 58% 6 4% at 4 years ; p = .99 , respectively ; fig 3c )  . 
rfs after allohsct in mrd - positive patients before prt was 44% 6 6% compared with 31% 6 6% at 4 years ( p = .20 ) after chemotherapy or autohsct , respectively ( fig 3d )  . 
only 46 of relapsing patients ( 22% ) proceeded to allohsct after obtaining a second cr . multivariable analysis the following variables significantly predicted for relapse in the univariable analysis : mrd status , type of prt , age , wbc category , flt3 - itd category , year of prt , time from diagnosis to cr , time from cr to prt , cytogenetics , number of cycles to cr , eln2017 risk classification , npm1 mutation , evi1 overexpression , and cebpa double mutation . 
after forward selection , the multivariable analysis was performed , stratified by the total number of induction courses with adjustment for mrd status , type of prt , age , wbc category at diagnosis , flt3 - itd , eln2017 risk classification , number of cycles to cr , and year of prt ( table 3 )  . 
different variables in the multivariable model were significantly associated with relapse , with the eln2017 risk classification , flt3 - itd mutant to wild - type ratio , number of cycles to reach cr , and type of prt being the most important variables . discussion the development of treatment approaches in patients with aml is increasingly personalized by using genetic and molecular leukemia characteristics at diagnosis and individual treatment response.3 - 6 response and especially mrd , detected by either multiparametric flow cytometry or quantitative polymerase chain reaction , has become an important parameter in a more precise treatment approach for patients with aml.10 - 24 currently , it is unknown whether and how the presence or absence of mrd should guide the application of allohsct as prt . 
recently , the quantitative detection of mutated npm1 has been shown to have high predictive value , and recommendations to tailor the application of allohsct by mrd were made.10 - 12 balsat et al10 suggested refraining from allohsct in npm1 mrdnegative patients and to selectively proceed to allohsct as prt in cr1 in mrd - positive patients or adverse - risk patients on the basis of karyotype or the presence of flt3 - itd . 
kaplan - meier estimates of the cumulative incidence ( ci ) of relapse in ( a ) minimal residual disease ( mrd ) negative patients ; ( b ) ci of relapse in mrdpositive patients ; ( c ) relapse - free survival ( rfs ) in mrd - negative patients ; and ( d ) rfs in mrdpositive patients by type of prt in patients with acute myeloid leukemia in first complete remission from start of prt . 
nevertheless , the advantages of personalized treatment are obvious and continuously being refined by updated and better methods of risk assessment . also , new technologies to better define mrd , such as quantification of leukemic stem - cell content , standardized protocols and antibody panels , and novel software possibilities , are emerging.45 - 47 a personalized approach including mrd identifies patients with a high risk of relapse who qualify for allohsct , but who might benefit from attempts to induce mrd negativity before transplantation . 
previously , a number of investigators reported that patients in cr1 with persistence of mrd before allohsct have worse survival compared with recipients of allohsct with an mrd - negative cr1.17 , 19 - 24 although allohsct is clearly indicated in mrd - positive patients , it is important to study the value of approaches intended to induce mrd negativity before allohsct . 
it has been suggested that continued chemotherapy with one or two consolidation cycles may not be the preferred strategy to obtain an mrd - negative cr before allohsct , 48 but several new drugs are currently being developed and evaluated for aml.49 possible other strategies may include efforts to improve allogeneic immunotherapy by early tapering of immunosuppression and / or preemptive donor lymphocyte infusions , which also could be guided by mrd . 
of events / patients allo ct / auto hr & 95% ci ( ct / auto : allo ) reduction ( sd ) mrd status ( cut - off 0.1 ) negative positive 93 / 207 40 / 58 90 / 211 40 / 71 total 133 / 265 ( 50% ) 130 / 282 ( 46% ) allo better ct / auto better 45% ( 8 ) reduction 2p < .001 collectively , our study shows that the gvl effect was strikingly similar in mrd - positive and mrdnegative patients . 
additional prospective studies are needed to evaluate whether the conversion of mrd positivity into an mrd - negative remission before allohsct further optimizes outcome , and how the gvl effect after allohsct can be optimized . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . jurjen versluis no relationship to disclose burak kalin no relationship to disclose wendelien zeijlemaker patents , royalties , other intellectual property : i have a patent for a laboratory test to identify specific leukemia cells that can be used in patients with acute myeloid leukemia . 
manz consulting or advisory role : amgen , novartis , roche , pfizer marie - christiane vekemans consulting or advisory role : amgen ( inst ) , celgene ( inst ) , bristol - myers squibb ( inst ) , janssen ( inst ) , takeda ( inst ) travel , accommodations , expenses : amgen , bristol - myers squibb , teva , janssen bart j . 
bargetzi no relationship to disclose juergen kuball employment : gadeta stock and other ownership interests : gadeta consulting or advisory role : gadeta , novartis ( inst ) speakers bureau : gadeta research funding : gadeta , miltenyi biotec , novartis patents , royalties , other intellectual property : multiple patents on gamma - delta t cell receptor sequences isolation strategies and targets in combination with gamma - delta t cell receptor sequences travel , accommodations , expenses : gadeta , novartis , miltenyi biotec harry c . 
van der velden consulting or advisory role : celgene ( inst ) research funding : bd biosciences ( inst ) patents , royalties , other intellectual property : patent for euroflow mrd antibody tubes . 
janssen honoraria : bristol - myers squibb netherlands , pfizer europe consulting or advisory role : pfizer europe , novartis research funding : novartis travel , accommodations , expenses : novartis thomas pabst no relationship to disclose bob lowenberg consulting or advisory role : astex pharmaceuticals , clear creek bio , agio pharmaceuticals , celgene mojca jongen - lavrencic no relationship to disclose gerrit jan schuurhuis research funding : becton dickinson ( inst ) gert ossenkoppele honoraria : roche consulting or advisory role : celgene , sunesis pharmaceuticals , janssen , novartis , cti , amgen , pfizer , roche research funding : amgen ( inst ) , janssen ( inst ) , celgene ( inst ) travel , accommodations , expenses : roche jan j . 
cornelissen no relationship to disclose acknowledgment following dutch - belgian hemato - oncology cooperative group and the swiss group for clinical cancer research ( hovon - sakk ) publication rules , coauthorship was offered to centers contributing the highest number of patients . nevertheless , the authors highly appreciate the contribution of many physicians and data managers throughout hovonsakk , who made this analysis possible . affiliations jurjen versluis , burak kalin , bob lowenberg , mojca jongen - lavrencic , and jan j . 
van der velden , erasmus university medical center , rotterdam ; wendelien zeijlemaker , jeroen j.w.m. janssen , gerrit jan schuurhuis , and gert ossenkoppele , vu university medical center ; bart j . 
wijermans , haga hospital , the hague ; mels hoogendoorn , medical center leeuwarden , leeuwarden ; juergen kuball , university medical center utrecht , utrecht ; harry c . schouten , maastricht university medical center , maastricht , the netherlands ; jakob passweg , university hospital basel , basel ; markus g . 
grimwade d , hills rk , moorman av , et al : refinement of cytogenetic classification in acute myeloid leukemia : determination of prognostic significance of rare recurring chromosomal abnormalities among 5876 younger adult patients treated in the united kingdom medical research council trials . 
d ohner h , estey eh , amadori s , et al : diagnosis and management of acute myeloid leukemia in adults : recommendations from an international expert panel , on behalf of the european leukemianet . 
cornelissen jj , gratwohl a , schlenk rf , et al : the european leukemianet aml working party consensus statement on allogeneic hsct for patients with aml in remission : an integrated - risk adapted approach . 
ossenkoppele g , schuurhuis gj : mrd in aml : does it already guide therapy decision - making ? hematology ( am soc hematol educ program ) 2016 : 356 - 365 , 2016 8 . 
grimwade d , freeman sd : defining minimal residual disease in acute myeloid leukemia : which platforms are ready for prime time ? blood 124 : 3345 - 3355 , 2014 9 . 
buccisano f , walter rb : should patients with acute myeloid leukemia and measurable residual disease be transplanted in first complete remission ? curr opin hematol 24 : 132 - 138 , 2017 10 . 
balsat m , renneville a , thomas x , et al : postinduction minimal residual disease predicts outcome and benefit from allogeneic stem cell transplantation in acute myeloid leukemia with npm1 mutation : a study by the acute leukemia french association group . 
kr onke j , schlenk rf , jensen ko , et al : monitoring of minimal residual disease in npm1 - mutated acute myeloid leukemia : a study from the german - austrian acute myeloid leukemia study group . 
freeman sd , virgo p , couzens s , et al : prognostic relevance of treatment response measured by flow cytometric residual disease detection in older patients with acute myeloid leukemia . 
schnittger s , kern w , tschulik c , et al : minimal residual disease levels assessed by npm1 mutation - specific rq - pcr provide important prognostic information in aml . 
shayegi n , kramer m , bornhauser m , et al : the level of residual disease based on mutant npm1 is an independent prognostic factor for relapse and survival in aml . 
jourdan e , boissel n , chevret s , et al : prospective evaluation of gene mutations and minimal residual disease in patients with core binding factor acute myeloid leukemia . 
araki d , wood bl , othus m , et al : allogeneic hematopoietic cell transplantation for acute myeloid leukemia : time to move toward a minimal residual disease - based definition of complete remission ? j clin oncol 34 : 329 - 336 , 2016 18 . 
bastos - oreiro m , perez - corral a , martnez - laperche c , et al : prognostic impact of minimal residual disease analysis by flow cytometry in patients with acute myeloid leukemia before and after allogeneic hemopoietic stem cell transplantation . 
walter rb , buckley sa , pagel jm , et al : significance of minimal residual disease before myeloablative allogeneic hematopoietic cell transplantation for aml in first and second complete remission . 
walter rb , gooley ta , wood bl , et al : impact of pretransplantation minimal residual disease , as detected by multiparametric flow cytometry , on outcome of myeloablative hematopoietic cell transplantation for acute myeloid leukemia . 
zhou y , othus m , araki d , et al : preand post - transplant quantification of measurable ( minimal ) residual disease via multiparameter flow cytometry in adult acute myeloid leukemia . 
l owenberg b , pabst t , maertens j , et al : therapeutic value of clofarabine in younger and middle - aged ( 18 - 65 years ) adults with newly diagnosed aml . 
cornelissen jj , versluis j , passweg jr , et al : comparative therapeutic value of post - remission approaches in patients with acute myeloid leukemia aged 40 - 60 years . 
versluis j , hazenberg cl , passweg jr , et al : post - remission treatment with allogeneic stem cell transplantation in patients aged 60 years and older with acute myeloid leukaemia : a time - dependent analysis . 
buccisano f , maurillo l , piciocchi a , et al : pre - transplant persistence of minimal residual disease does not contraindicate allogeneic stem cell transplantation for adult patients with acute myeloid leukemia . 
cornelissen jj , breems d , van putten wl , et al : comparative analysis of the value of allogeneic hematopoietic stemcell transplantation in acute myeloid leukemia with monosomal karyotype versus other cytogenetic risk categories . j clin oncol 30 : 2140 - 2146 , 2012 35 . 
lamers ch , wijers r , van bergen ca , et al : cd4 + t - cell alloreactivity toward mismatched hla class ii alleles early after double umbilical cord blood transplantation . 
norde wj , overes im , maas f , et al : myeloid leukemic progenitor cells can be specifically targeted by minor histocompatibility antigen lrh - 1 - reactive cytotoxic t cells . 
terwey th , hemmati pg , martus p , et al : a modified ebmt risk score and the hematopoietic cell transplantationspecific comorbidity index for pre - transplant risk assessment in adult acute lymphoblastic leukemia . 
sorror ml , maris mb , storb r , et al : hematopoietic cell transplantation ( hct ) - specific comorbidity index : a new tool for risk assessment before allogeneic hct . 
sorror ml , sandmaier bm , storer be , et al : comorbidity and disease status based risk stratification of outcomes among patients with acute myeloid leukemia or myelodysplasia receiving allogeneic hematopoietic cell transplantation . 
versluis j , labopin m , niederwieser d , et al : prediction of non - relapse mortality in recipients of reduced intensity conditioning allogeneic stem cell transplantation with aml in first complete remission . 
shouval r , labopin m , bondi o , et al : prediction of allogeneic hematopoietic stem - cell transplantation mortality 100 days after transplantation using a machine learning algorithm : a european group for blood and marrow transplantation acute leukemia working party retrospective data mining study . 
zeijlemaker w , kelder a , oussoren - brockhoff yj , et al : a simple one - tube assay for immunophenotypical quantification of leukemic stem cells in acute myeloid leukemia . 
flores - montero j , sanoja - flores l , paiva b , et al : next generation flow for highly sensitive and standardized detection of minimal residual disease in multiple myeloma . 
cornelissen jj , van norden y , van gelder m , et al : early post - transplant epigenetic therapy by panobinostat and decitabine followed by donor lymphocyte infusion ( dli ) : interim results of the hovon - 116 phase i / ii feasibility study in poor - risk aml recipients of allogeneic stem cell transplantation ( allohsct )  . 
bug g , burchert a , wagner e , et al : phase i / ii study of the deacetylase inhibitor panobinostat as maintenance therapy after an allogeneic stem cell transplantation in patients with high - risk mds or aml : the panobest - trial . 
stone rm , mandrekar s , sanford bl , et al : the multi - kinase inhibitor midostaurin prolongs survival compared with placebo in combination with daunorubicin / cytarabine induction , high - dose c consolidation , and as maintenance therapy in newly diagnosed acute myeloid leukemia ( aml ) patients age 18 - 60 with flt3 mutations : an international prospective randomized - controlled double - blind trial ( calgb 10603 / ratify [ alliance ] )  . 
dinardo c , de botton s , pollyea da , et al : molecular profiling and relationship with clinical response in patients with idh1 mutation - positive hematologic malignancies receiving ag - 120 , a first - in - class potent inhibitor of mutant idh1 , in addition to data from the completed dose escalation portion of the phase 1 study . 
 plasma dna - based molecular diagnosis , prognostication , and monitoring of patients with ewsr1 fusion - positive sarcomas purpose ewing sarcoma ( es ) and desmoplastic small round cell tumors ( dsrcts ) are aggressive sarcomas molecularly characterized by ewsr1 gene fusions . 
as pathognomonic genomic events in these respective tumor types , ewsr1 fusions represent robust potential biomarkers for disease monitoring . methods to investigate the feasibility of identifying ewsr1 fusions in plasma - derived cell - free dna ( cfdna ) from patients with es and dsrct , we evaluated two complementary approaches in samples from 17 patients with radiographic evidence of disease . 
the first approach involved identification of patient - specific genomic ewsr1 fusion breakpoints in formalin - fixed , paraffinembedded tumor dna using a broad , hybridization capture - based next - generation sequencing ( ngs ) panel , followed by design of patient - specific droplet digital polymerase chain reaction ( ddpcr ) assays for plasma cfdna interrogation . 
2017 by american society of clinical oncology introduction ewing sarcoma ( es ) and desmoplastic small round cell tumor ( dsrcts ) are aggressive sarcomas with peak incidences in adolescence and young adulthood.1 both are characterized by fusions involving the ewsr1 gene on chromosome 22q12.2 , 3 the fusions in es involve ewsr1 and a member of the ets family . 
most commonly , the partner gene is ets family member fli1 , with alternative genes such as erg , etv1 , etv4 , and fev less commonly observed.4 in dsrcts , the fusion involves ewsr1 and the wilms tumor gene wt1 . 
given their exquisite specificity for es and dsrct , respectively , the detection of these fusions in a tumor biopsy has become a standard part of the diagnostic assessment of patients with these sarcomas . over the past several decades , numerous trials for es have been conducted , leading to current therapeutic standards of care that result in long - term cure for approximately 75% of patients who present with localized disease but only approximately 25% in patients who present with metastatic disease.5 , 6 dsrct was only recognized as a distinct malignancy 25 years ago , with the characterization of its pathognomonic oncogenic fusion following several years later.3 , 7 despite intensive regimens evaluating combinations of chemotherapy , aggressive debulking surgical approaches , neerav n . 
 radiation therapy , and autologous stem cell rescue , outcomes for dsrct remain poor , with locoregional recurrences representing the most common type of relapse.8 the establishment of clinically valid prognostic and predictive biomarkers has been challenging in es and largely unstudied in dsrct.9 specifically , numerous studies have been conducted in an effort to establish platforms to identify and follow subclinical levels of disease burden.10 - 14 the two strategies most commonly used have been reverse transcription polymerase chain reaction ( rtpcr ) evaluation for the ewsr1 fusion transcript from cellular rna extracted from peripheral blood and / or bone marrow , or , for es , flow cytometric evaluation of peripheral blood and / or bone marrow cells on the basis of a cd99 + gating strategy . 
these studies have had varying results and , to date , have not satisfied criteria as suitable clinical biomarkers . more recently , studies in various cancer types have demonstrated the potential use of identifying and following tumor - specific mutations in cell - free dna ( cfdna ) isolated from plasma as a marker for subclinical disease.15 - 17 a study of various different cancer types by bettegowda et al18 demonstrated highly variable levels of mutations in baseline cfdna in patients with different tumor types , suggesting that the use of cfdna as a clinically relevant signal for subclinical disease will be partly based on the cancer type itself . 
these studies all rely on the ability to identify tumorspecific aberrations as a marker of disease burden . tumors such as es and dsrcts have low mutational burdens , because it is believed that the pathognomonic ewsr1 fusions are the primary driving oncogenic lesions in these tumor types , with few recurrent secondary alterations.19 therefore , the identification of tumor - specific ewsr1 fusions in cfdna as a marker for active disease is an especially attractive option , given that these tumors are defined by these translocations . 
moreover , issues such as clonal evolution , which can affect the detection of certain mutations in cfdna in other tumor types , are less pertinent , because these sarcomas maintain these specific fusions through an individuals disease course . 
importantly , even identical ewsr1 fusion transcripts are the result of genomic breakpoints in the corresponding introns that are unique to each patient.20 although a genomic dna - based clinical assay to monitor these translocations in plasma cfdna should be more robust than rna - based assays in this context , the heterogeneity of intronic breakpoint regions between tumors from different patients had previously presented a major challenge for the design and routine application of such a dna - based assay , a hurdle now overcome by the application of more powerful sequencing approaches . in this study , we directly compared two strategies to identify baseline ewsr1 genomic rearrangements in cfdna of patients with es and dsrct . the first approach uses droplet digital pcr ( ddpcr ) of cfdna to detect fusions identified by targeted next - generation sequencing of formalinfixed paraffin - embedded tumor biopsy material.21 this approach has been successfully used in numerous studies of other tumor types . 
the second approach uses next - generation sequencing ( ngs ) via a modified hybridization capture approach to identify ewsr1 fusions as well as potentially prognostic mutations in cfdna samples . 
the primary aim of this study was to evaluate each platform , ddpcr and ngs , on paired cfdna samples from patients with es and dsrct with confirmed radiographic evidence of disease . methods patient population between august 2014 and january 2016 , patients with a confirmed diagnosis of es or dsrct and formalin - fixed paraffin - embedded clinical tumor material available for memorial sloan kettering integrated mutation profiling of actionable cancer targets ( msk - impact ) tumor genotyping were eligible to enroll on this study . 
for each patient , at least one baseline 10 - ml blood sample was collected in streck blood collection tubes ( bcts ; streck , la vista , ne )  . msk - impact tumor ngs genomic dna from tumor tissue and patientmatched normal blood were subjected to targeted sequencing using msk - impact , a custom , deepcoverage targeted sequencing assay approved by the new york state department of health as a clinical test.21 , 22 tumors were sequenced to an average coverage depth of 7663 ( range , 4053 to 1 , 2513 ) in the clinical laboratories of the memorial sloan kettering cancer center molecular diagnostics service . 
 cancer - associated genes using bioinformatics pipelines previously described.21 gene fusions involving ewsr1 were identified in all patients included in this study using delly.23 , 24 plasma cfdna extraction and analyses whole blood collected in 10 - ml cell - free dna bcts ( streck ) was centrifuged in two steps to separate plasma from cells . 
in step 2 , separated plasma was further centrifuged in a high - speed microcentrifuge at 18 , 000 3 g for 10 minutes ( ambient temperature )  . cell - free plasma was aliquoted and frozen at 280c until ready to extract . 
extraction of cfdna was performed using a fully automated qiagen platform , qiasymphony sp , and qiasymphony dsp virus / pathogen midi kit ( catalog #937055 ; qiagen , valencia , ca )  . 
quality and quantity of cfdna was evaluated with automated electrophoresis using either tapestation with high sensitivity d1000 screentape and reagents ( agilent technologies , santa clara , ca ) or fragment analyzer with high sensitivity genomic dna analysis kit ( advanced analytical , ankeny , ia )  . breakpoint - specific ddpcr for each sample , a fusion - specific assay was designed using primer3plus and ordered through biorad ( hercules , ca )  . 
pcr reactions contained fusion - specific primers and probes , biorad validated copy number control primers and probes , and digital pcr supermix for probes ( no 2 / - deoxyuridine 59 - triphosphate ) and circulating free dna . 
emulsified reactions were amplified on a 96 - well thermal cycler using cycling conditions identified during the optimization step ( 95c 109 ; 40 cycles of 94c 3099 58c 19 , 98c 109 , 4c hold )  . 
plates were read and analyzed with the quantasoft software to assess the number of droplets positive for mutant dna , wild - type dna , both , or neither . the assay threshold sensitivity was set at two mutant droplets . targeted plasma ngs cell - free dna ( cfdna ) from plasma was extracted using the qiasymphony sp system ( qiagen )  . sequencing libraries were prepared according to the kapa hyper protocol ( kapa biosystems , wilmington , ma ) with the ligation of illumina sequence adaptors followed by pcr amplification and clean - up . 
custom dna probes targeting all coding exons of stag2 and tp53 and selected introns of ewsr1 ( intron 7 to 13 ) were synthesized by idt ( integrated dna technologies , coralville , ia )  . 
an equal amount of each dna library ( 200 ng per sample ) was pooled for hybridization capture using a customized double - capture protocol modified from the nimblegen seqcap target enrichment system ( roche sequencing solutions , pleasanton , ca )  . 
after pcr clean - up , the captured target library was processed by a secondary capture ( using the same custom dna probes ) incubated at 65c for 4 hours and followed by postcapture washes and three to five cycles of pcr amplification . 
the pooled , cleaned - up libraries containing captured dna fragments were sequenced on the illumina hiseq system with paired end reads ( 2 3 100 bp )  . analysis was performed using the same bioinformatics pipeline as for msk - impact tissue sequencing . 
sequence alignment and mutation calling were performed on reads from all tumor samples , normals , and cfdna samples simultaneously to ensure consistent realignment around indels and consistent annotation of shared mutations . the scatterplot for concordance between ngs and ddpcr measurement of fusion molecules was generated using the r package ggplot2 . 
clinical features of patients with es in the study patient id sex age at dx ( years ) disease type fusion partner gene disease status primary tumor location metastatic site ( s ) at diagnosis site of recurrence es - 3 right chest wall n / a left lung fli1 fli1 fli1 fli1 fli1 fli1 fli1 fli1 newly diagnosed , right fibula newly diagnosed , right scapula multiple bones , bone multiple bones marrow newly diagnosed , left femur multiply recurrent , right chest wall multiple bones lungs , multiple newly diagnosed , left chest wall lungs multiply recurrent , pelvis vertebrae , lungs lungs bones lungs lungs pelvis lungs left ankle lungs left tibia lungs , multiple bones , multiple bones bone marrow left chest wall pleura , abdomen localized metastatic recurrent , metastatic localized metastatic metastatic metastatic recurrent , metastatic recurrent , metastatic recurrent , metastatic recurrent , metastatic abbreviations : dx , diagnosis ; es , ewing sarcoma ; id , identification ; n / a , not applicable . disease were analyzed by both ddpcr and custom capture ngs ( tables 1 and 2 )  . 
all patients with dsrct had abdominal / pelvic disease involvement , being the characteristic clinical presentation of this sarcoma , and four out of six patients also had metastatic disease involving the mediastinum . tumor - specific ewsr1 fusions were successfully identified by msk - impact in all 17 tumor biopsyderived dna samples ( table 3 ; data supplement )  . 
no false positives were detected in 165 , 000 wild - type copies . we identified tumor - specific fusions as evidence of circulating tumor dna ( ctdna ) in all 11 baseline plasma samples from patients with es ( table 3 )  . 
we also identified ewsr1 - wt1 fusions in five out of six dsrct baseline plasma samples . using our custom capture ngs assay involving ewsr1 , tp53 , and stag2 , we sequenced parallel cfdna samples from the cohort of 17 patients to a mean total depth of coverage of 147 , 5493 ( mean unique coverage , 3 , 7543 after removing inferred pcr duplicates )  . 
by achieving such deep coverage , we achieved high sensitivity for detecting different ewsr1 fusions in a single universal assay , regardless of the precise location of the genomic breakpoint in ewsr1 . fusions were detected in 14 out of 17 patients ( table 3 ) , including 10 of 11 patients with ewing sarcoma and four of six patients with dscrt . 
as a complementary approach , cfdna samples were also directly profiled using a custom capturetargeted ngs assay designed to identify alterations in ewsr1 , tp53 , stag2 , and cdkn2a . dna extraction msk - impact breakpoint identication tumor blood cfdna extraction personalized ddpcr primers ddpcr assay targeted ngs prior knowledge from sequencing the tumor tissue ( data supplement )  . 
this is the first report to our knowledge to directly compare two complementary methodologies , ddpcr and hybrid - capture ngs , to evaluate tumor - specific ewsr1 fusions in cfdna from patients with es and dsrct . tumor - specific fusions are particularly attractive target substrates for mutation - based biomarker studies of ewsr1 translocation - associated sarcomas . 
although tumor cfdna studies typically target oncogene point mutations , we previously demonstrated the relative scarcity of such recurrent somatic mutations in fusion - associated sarcomas.19 specifically , in 75 es and 24 dsrct samples screened for 275 recurrent point mutations in 29 oncogenes frequently mutated across different cancer types , mutations were identified in only 4% of es samples , and none of the dsrct samples . 
recent comprehensive wholeexome and whole - genome sequencing studies of es tumor specimens have validated this finding.26 - 28 conversely , ewsr1 fusions are defining molecular features of es and dsrcts and have never been reported to undergo modification or clonal evolution through a disease course . previous studies using rt - pcr to identify ewsr1 fusion transcripts in peripheral blood or bone marrow samples from patients with es report successful identification in , 50% of patients.10 , 11 , 13 it is perhaps not surprising that the cfdna - based approach used in our study yielded more sensitive results , because previous studies attempted to identify rare occult tumor cells through the identification of cellular ewsr1 fusion transcripts . 
recent studies have established the increased sensitivity of plasma - derived cfdna assays as compared with circulating tumor cell assays for blood - based identification of disease.18 a similar sensitivity advantage of cfdna over cell - free rna is also likely . 
mu , mutant droplets ; wt , wild - type droplets . ddpcr ( mu / ( mu + wt ) ) rt - pcr methodologies used rna as a substrate , which undergoes rapid degradation leading to potential false - negative results if samples are not processed immediately . 
finally , previous attempts at using rt - pcr used primers for only the most common transcripts seen in es tumors among the many reported ewsr1 - fli1 fusion types.20 therefore , a subset of patients whose tumors harbored less common ewsr1 - fli1 fusion types or other ewsr1 fusion partners was uncaptured , reducing the clinical sensitivity of the assay . in this study , both platforms were highly sensitive at detecting ewsr1 fusions in baseline cfdna samples , although ddpcr demonstrated increased sensitivity and was able to detect levels < 0.1%. 
the characterization of tp53 alterations as an adverse prognostic finding was proposed on the basis of several retrospective studies29 - 32 but was not confirmed in a recent prospective study.33 however , another recent large - scale genomic profiling study of es identified tumors with comutation of stag2 and tp53 as defining a particularly high - risk subset of patients.28 it is therefore important future biomarker studies continue to collect these mutational data in an effort to establish more definitively their clinical use . that a significant advantage of the ngs approach is that it can be performed directly on cfdna without a priori knowledge of tumor - specific mutations . 
this is a particularly attractive aspect of this methodology , because reliable acquisition of baseline tumor tissue has proven difficult in north american cooperative group es banking studies.34 in this study , we demonstrated the ability to identify fusion breakpoint sequences in the majority of plasma cfdna samples , along with potentially prognostic alterations in tp53 and stag2 . 
although ngs was successful at identifying fusions in the majority of baseline cfdna samples , there were several examples in which ddpcr was able to identify a low level of fusion positivity that was not identified by ngs . 
a similar ngs - based approach was recently described in patients with advanced lung cancer , with 88% and 100% sensitivity and specificity , respectively , for detecting previously charat 0.1% allele acterized mutations present frequency or higher.35 the higher sensitivity of a ddpcr approach is potentially clinically important for identifying early evidence of relapse in followup samples during and after therapy . our study highlights the advantages of both platforms . 
furthermore , ngs provides the ability to capture the heterogeneity of a patients disease more completely than ddpcr , as reflected in the patient cfdna sample ( es - 2 ) with multiple tp53 mutations . 
nonetheless , these results provide important data for the establishment of an optimal strategy for future cooperative group prospective biomarker studies of ewsr1 - defined sarcomas . given these findings , we propose a hybrid approach for future clinical trials ( fig 3 )  . 
this will also allow for identification of the precise fusion breakpoint as well as additional tp53 and stag2 mutational status on the majority of patients , without the need to profile tumor material . 
proposed schema for prospective ewsr1 fusion - based cell - free dna ( cfdna ) studies . the depicted proposed schema for future prospective studies evaluating the use of cfdna as a marker for subclinical disease in ewing sarcoma or desmoplastic small round cell tumors incorporates the advantages of each methodology ( nextgeneration sequencing [ ngs ] and downstream droplet digital polymerase chain reaction [ ddpcr ] )  . breakpoint determination , as well as quantification of ewsr1 fusion , and identification of additional mutation data are identifiable on the majority of baseline plasma cfdna samples using a targeted custom - capture ngs approach . 
 ( * ) for cases where ngs fails to identify genomic fusion sequences , tissue samples will need to be collected for breakpoint determination through tumor profiling . baseline cfdna extraction follow - up blood cfdna extraction targeted ngs breakpoint determination * quantication of fusion additional mutation detection ddpcr assay biomarker development in rare cancer types , and certain characteristics are imperative for the successful development of predictive markers in this clinical context.9 our proposed approach is especially compelling given these criteria . 
first , our approach should capture almost 100% of patients with es and dsrct , because the platforms are designed to capture any ewsr1 fusion type , including those with rare variant ewsr1 translocations . 
cell - free specific bcts contain stabilizing reagents , which have been shown to minimize both ctdna degradation and sample contamination with blood cellderived genomic dna.36 , 37 this is particularly important for potential biomarkers in rare diseases , where cooperative group studies require long - distance sample deliveries , necessitating strategies to eliminate the issue of substrate degradation . 
ddpcr has been established as an attractive platform for circulating nucleic acids on the basis of the ease of quantitation of mutant fragments as compared with realtime pcr.38 furthermore , broad , hybrid - capture ngs platforms are becoming increasingly used for clinical use , as exemplified by the msk - impact sequencing platform , with well over 10 , 000 patient tumor samples studied to date , 39 and even greater numbers studied by similar ngs - based assays at commercial reference laboratories . our primary aim in this study was to establish a robust methodology suitable for the unique and stringent requirements for biomarker development in prospective studies of rare diseases . 
 heather magnan no relationship to disclose ahmet zehir no relationship to disclose daoqi you no relationship to disclose jiabin tang no relationship to disclose fanli meng no relationship to disclose aliaksandra samoila no relationship to disclose emily k . 
fletcher c , bridge j , hogendoorn p , et al ( eds ) : world health organization classification of tumours : pathology and genetics of tumours of soft tissue and bone ( ed 4 )  . 
lessnick sl , ladanyi m : molecular pathogenesis of ewing sarcoma : new therapeutic and transcriptional targets . 2837 - 2840 , 1994 annu rev pathol 7 : 145 - 159 , 2012 5 . 
womer rb , west dc , krailo md , et al : randomized controlled trial of interval - compressed chemotherapy for the treatment of localized ewing sarcoma : a report from the childrens oncology group . 
kolb ea , kushner bh , gorlick r , et al : long - term event - free survival after intensive chemotherapy for ewings family of tumors in children and young adults . 
desai nb , stein nf , laquaglia mp , et al : reduced toxicity with intensity modulated radiation therapy ( imrt ) for desmoplastic small round cell tumor ( dsrct ) : an update on the whole abdominopelvic radiation therapy ( wap - rt ) experience . 
zoubek a , ladenstein r , windhager r , et al : predictive potential of testing for bone marrow involvement in ewing tumor patients by rt - pcr : a preliminary evaluation . 
schleiermacher g , peter m , oberlin o , et al : increased risk of systemic relapses associated with bone marrow micrometastasis and circulating tumor cells in localized ewing tumor . 
ash s , luria d , cohen ij , et al : excellent prognosis in a subset of patients with ewing sarcoma identified at diagnosis by cd56 using flow cytometry . 
roschewski m , dunleavy k , pittaluga s , et al : circulating tumour dna and ct monitoring in patients with untreated diffuse large b - cell lymphoma : a correlative biomarker study . 
hyman dm , diamond el , vibat cr , et al : prospective blinded study of brafv600e mutation detection in cell - free dna of patients with systemic histiocytic disorders . 
dawson sj , tsui dw , murtaza m , et al : analysis of circulating tumor dna to monitor metastatic breast cancer . n engl j med 368 : 1199 - 1209 , 2013 18 . 
shukla n , ameur n , yilmaz i , et al : oncogene mutation profiling of pediatric solid tumors reveals significant subsets of embryonal rhabdomyosarcoma and neuroblastoma with mutated genes in growth signaling pathways . 
plougastel b , zucman j , peter m , et al : genomic structure of the ews gene and its relationship to ewsr1 , a site of tumor - associated chromosome translocation . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
huang hy , illei pb , zhao z , et al : ewing sarcomas with p53 mutation or p16 / p14arf homozygous deletion : a highly lethal subset associated with poor chemoresponse . 
tsuchiya t , sekine k , hinohara s , et al : analysis of the p16ink4 , p14arf , p15 , tp53 , and mdm2 genes and their prognostic implications in osteosarcoma and ewing sarcoma . 
lerman dm , monument mj , mcilvaine e , et al : tumoral tp53 and / or cdkn2a alterations are not reliable prognostic biomarkers in patients with localized ewing sarcoma : a report from the childrens oncology group . pediatr blood cancer 62 : 759 - 765 , 2015 34 . 
integrative genomics viewer screenshot of es - 2 bam file showing tp53 r280k ( right ; frequency , 0.04 ; identified in plasma ) and e285k ( left ; frequency , 0.44 ; identified in both plasma and tissue ) mutations . 
paweletz cp , sacher ag , raymond ck , et al : bias - corrected targeted next - generation sequencing for rapid , multiplexed detection of actionable alterations in cell - free dna from advanced lung cancer patients . 
denis mg , knol ac , theoleyre s , et al : efficient detection of braf mutation in plasma of patients after long - term storage of blood in cell - free dna blood collection tubes . 
 detection of circulating tumor dna in patients with leiomyosarcoma with progressive disease purpose leiomyosarcoma ( lms ) is a soft - tissue sarcoma characterized by multiple copy number alterations ( cnas ) and without common recurrent single - nucleotide variants . 
 we evaluated the feasibility of detecting circulating tumor dna ( ctdna ) with next generation sequencing in a cohort of patients with lms whose tumor burden ranged from no evidence of disease to metastatic progressive disease . patients and methods we evaluated cell - free dna in plasma samples and paired genomic dna from resected tumors from patients with lms by ultra - low passage whole genome sequencing . 
sequencing reads were aligned to the human genome and cnas that were identified in cell - free dna and tumor dna by ichorcna software to determine the presence of ctdna . 
clinical data were reviewed to assess disease burden and clinicopathologic features . results we identified lms ctdna in 11 ( 69% ) of 16 patients with disease progression and total tumor burden greater than 5 csixteen patients with stable disease or low disease burden at the time of blood draw were found to have no detectable ctdna . 
ctdna levels declined after resection of progressive disease in one case and became detectable upon disease relapse in another individual patient . conclusion these results suggest that ctdna , assayed by a widely available sequencing approach , may be useful as a biomarker for a subset of patients with uterine and extrauterine lms . 
2018 by american society of clinical oncology introduction leiomyosarcoma ( lms ) is a malignant neoplasm derived from smooth muscle that represents one of the most common subtypes of soft - tissue sarcoma.1 , 2 although the majority of lms cases are sporadic , predisposing factors include li fraumeni syndrome , hereditary retinoblastoma , and radiation exposure.3 , 4 there are no oncogenic single - nucleotide variants ( snvs ) that characterize lms , although loss of tumor suppressors , including tp53 , rb1 , and pten , are commonly observed , as are multiple copy number alterations ( cnas ) .5 - 8 lms is frequently a clinically aggressive disease , and patients are at high risk for local and metastatic relapse after initial complete resection.9 , 10 efforts to improve outcomes for patients would benefit from more reliable indicators of high - risk disease and biomarkers of response to therapy . detection of circulating tumor dna ( ctdna ) has emerged as a new approach for identifying oncogenic mutations , measuring disease burden , clinical prognostication , and assessing tumor response to therapy.11 , 12 most ctdna assays matthew l . 
 have been developed to detect snvs that are highly recurrent in many types of carcinomas.13 although the lack of recurrent snvs in lms limits efforts at targeted sequencing , the numerous cnas that are characteristic of this disease represent an ideal target for detection . 
 a next - generation sequencing approach using ultra - low passage whole - genome sequencing ( ulp - wgs ) can detect cnas in cell - free dna , which indicates the tumor fraction of ctdna present in blood.14 , 15 previous studies have shown that ctdna can be detected in cell - free dna samples that are sequenced at a minimum coverage of 0.1 across the whole genome.14 sequencing for ulp - wgs uses the standard illumina next - generation sequencing platform without modifications or special adaptions ( illumina , san diego , ca )  . 
the ichorcna algorithm is used to detect megabase - scale cnas from ulp - wgs data in which ctdna comprise as little as 3% of the total cell - free dna extracted from a plasma sample.14 in the current study , we evaluated plasma from patients with uterine and extrauterine lms for the presence of ctdna using ulp - wgs . 
paired resected tumors from each patient were also sequenced when available ( 29 of 30 patients ) , which enabled the identification and comparison of cnas between primary tumors and ctdna . 
high - molecular - weight dna contamination of cell - free dna was determined by bioanalyzer ( agilent technologies , santa clara , ca ) and size selection was performed if necessary ( ampure xp beads ; beckman coulter , brea , ca )  . 
up to 40 ng of cell - free dna , 100 ng of dna from fresh frozen tissue , and 200 ng of dna from ffpe tissue were used for kapa hyper library preparation ( kapa biosystems , wilmington , ma )  . 
 after bioruptor sonication ( diagenode ) of formaldehyde - fixed fresh frozen sample , with library preparation using a thruplex dna sequencing kit ( rubicon ) and sequencing on an illumina nextseq 500 . 
this higher sequencing coverage did not alter downstream analyses or data interpretation . sequencing results were demultiplexed , aligned , and processed using picard , burrows - wheeler alignment tool , 17 and genome analysis toolkit.18 , 19 to assess for cnas in tumor and cellfree dna and determine tumor fraction or percentage of ctdna in cell - free dna , we used ichorcna software14 with manual curation of results as necessary to confirm tumor percentages . 
previous studies have demonstrated that this technique can be used to identify and quantitate ctdna that constitutes as little as 3% of the cell - free dna in a sample.14 copy number analysis copy number segments and estimates of tumor fraction and ploidy were generated by ichorcna . 
this analysis was performed separately on tumor resection samples , including the eight samples for which plasma was not available , and on plasma samples that were positive for detectable levels of ctdna . statistical analysis group comparisons between patients with lms with active or indolent disease at the time of plasma collection was performed by nonparametric mann - whitney test , and we performed pearson correlation coefficient between tumor fraction or cell - free dna and tumor burden using graphpad prism ( version 7.0 ; graphpad software , la jolla , ca )  . 
one was added to integer values before log2 transformation to generate non - negative values for data representation . results detection of lms ctdna we retrospectively identified 30 patients who were diagnosed with metastatic lms who had plasma banking performed at variable time points in their treatment history between january 2007 and november 2017 . 
median age at diagnosis was 51 years , most patients were female , the most common primary tumor location was the uterus ( n = 16 ) followed by the retroperitoneum ( n = 8 ) , and most tumors were originally of intermediate or high grade ( table 1 )  . 
twenty - nine of 30 patients had a tumor resection sample available for comparison with cell - free dna . in review of clinical data at the time of plasma banking , the cases could be divided into active disease or indolent disease groups on the basis of tumor volume and evidence of disease progression . 
the active disease group consisted of 16 patients and was defined by having a total tumor burden greater than 5 cm in greatest diameter and progressive disease at the time of blood draw on the basis of imaging or clinical determination . 
in contrast , 16 patients in the indolent disease group had stable disease at the time of blood draw and / or tumor burden less than 5 camong the active disease group , 11 ( 69% ) of 16 patients had detectible ctdna , including patients with both uterine and extrauterine primary tumors . 
none of the samples obtained from the indolent disease group had detectible ctdna ( fig 1a )  . when comparing the amount of ctdna measured as a fraction of total cell - free dna in the plasma sample to the volume of tumor burden reported by computed tomography scan , there was a significant association between higher ctdna levels and increasing tumor burden ( fig 1b )  . 
 abbreviations : a , abdomen ; b , bone ; c , chest ; ctdna , circulating tumor dna ; f , female ; hpf , high - power field ; l , liver ; m , male ; na , not available ( data not reported during pathology review ) ; p , pelvis ; st , soft tissue , including subcutaneous , muscle , and paraspinal locations . cna concordance between lms tumors and ctdna in the 11 plasma samples with detectible levels of ctdna , there was a high concordance of cnas between the tumor sample and ctdna ( figs 2a - 2d ) , with blood collection occurring less than 2 years apart from resection of the matched tumor specimen . 
the active disease group consists of patients with tumors > 5 cm in size and with progressive disease at the time of blood draw as indicated by computed tomography ( ct ) scan or clinical report . 
labels indicate the active disease subgroup ( red ) with tumor size > 5 cm and progressive disease ( n = 16 ) , or indolent disease subgroups ( gray ) with tumor size > 5 cm and stable disease ( n = 2 , diamond ) , tumor size < 5 cm and progressive disease ( n = 4 ; triangle ) , and tumor size < 5 cm and stable disease ( n = 10 ; circle )  . 
overall , recurrent cnas from tumors in this cohort are remarkably similar to those found in prior studies.5 , 8 the most significantly amplified genomic region was found on chromosome 17p , which includes the transcriptional regulator myocd ( copy gained in 20 of 37 tumors )  . 
this gene has previously been reported as significantly amplified in lms and is associated with smooth muscle differentiation.22 additional putative oncogenic and lms associated genes that were recurrently amplified include hdgf in 20 , myc in 14 , cthrc1 in 17 , tnfrsf19 in 10 , and myh2 in 16 of 37 tumors ( fig 3a )  . 
copy gains in these genes were also observed in a portion of cell - free dna samples with detectable ctdna ( myocd in four , hdgf in six , myc in eight , cthrc1 in nine , tnfrsf19 in three , and myh2 in four of 11 ctdna - positive samples ) ; however , the number of evaluable samples was too small for any copy gains of these genes to reach statistical significance ( fig 3b )  . 
from tumor samples , recurrent deletions in tumor suppressors were found , which are characteristic of lms , 5 , 8 , 23 including pten deletions in 27 , rb1 in 27 , and tp53 in 11 of 37 tumors profiled ( fig 3c )  . 
deletions that involved these genes were also detected in ctdna ( pten in eight , rb1 in six , and tp53 in two of 11 ctdna - positive samples ) , but sample size was too small for many of these deletions to reach significance ( fig 3d )  . 
 thus , ulp - wgs is capable of detecting recurrent cnas characteristic of lms , and these methods may be helpful in identifying genelevel cnas in ctdna . ctdna longitudinally correlates with disease status to determine whether ctdna levels change in agreement with longitudinal disease status , we evaluated serial plasma samples in two patients after either resection of localized lms or with disease recurrence after surgery . 
in contrast , in the patient with disease recurrence 32 months after surgical resection , cell - free dna tumor fraction increased from undetectable postoperatively to detectable at the time of disease recurrence ( fig 4b )  . 
 ( a - e ) copy number plots generated from ultra - low passage whole - genome sequencing of five representative tumor surgical ( left panels ) and plasma ( right panels ) sample pairs . 
tumor fraction is indicated for each plot . discussion in the current study , we analyzed cell - free dna from the plasma of patients with lms for evidence of ctdna . 
a significant association between tumor burden and the amount of ctdna was identified , which suggests that larger and actively growing tumors are more likely to release tumor dna into circulation . 
 ( a - d ) gistic2.0 analysis identifying recurrent focal amplified ( a and b ) and deleted ( c and d ) regions in lms tumors ( n = 37 ; left panels ) and cell - free dna samples with detectable circulating tumor dna ( n = 11 ; right panels )  . 
the green line indicates an fdr of 0.25. tumor cell - free dna amplifications tnfrsf19 myocd myh2 amplifications cthrc1 6 7 8 9 10 chromosome 12 14 16 18 20 x 12 14 16 18 20 6 7 8 9 10 chromosome deletions hdlbp deletions cdkn2aip brca2 tp53 pten tsc1 ypel3 12 14 16 18 20 x 12 14 16 18 20 x 6 7 8 9 10 chromosome 6 7 8 9 10 chromosome 10 - 1 0.25 10 - 2 10 - 1 0.25 less than 5 cm in size , regardless of evidence of disease progression , which may represent a technologic sensitivity threshold . 
we further found that ctdna levels decline with resection of disease and increase with disease recurrence in individual patients , which indicates that these methods may be useful for supporting a diagnosis of disease recurrence or response to therapy . sequencing of snvs in cell - free dna has proven clinical utility in detecting resistance mutations to targeted therapies and directing treatment strategies.24 emerging use of whole - genome sequencing to identify and quantify cnas from tumor - derived dna circulating in patients with cancer has been evaluated in a number of cancer types.14 , 25 - 27 this noninvasive approach can be useful in the genomic characterization of malignancy and provide diagnostic and prognostic information relevant for clinical care.15 , 21 , 28 in a recent study of patients with lms , a highly customized lms - specific assay ( cancer personalized profiling by deep sequencing , or cappseq ) was designed to detect selected snvs and combined with cna analysis to identify and quantify ctdna in patients with progressive disease.29 in this study , the investigators found that approximately 20% of patients ( two of nine ) had tumors that did not have somatic events that were detectable by the assay . 
in contrast , we found that tumors from 100% of cases had cnas that were detectable by ulp - wgs , which suggests that ulp - wgs may be more broadly applicable for patients with lms . 
 the interval between surgical date and cell - free dna collection is indicated . in six of seven baseline samples of patients who were eligible for study ( 86% ) and had a sensitivity of 68% among all samples tested from their cohort . 
although these numbers are small , this suggests that capp - seq may have a higher sensitivity for ctdna , which might be expected given the deep sequencing coverage used in this assay . 
for example , our recent study in osteosarcoma demonstrated that pretreatment ctdna levels detected by ulpwgs are prognostic , 28 whereas a more sensitive assay , such as capp - seq , may be advantageous in the setting of disease surveillance.29 there are several potential clinical uses of ctdna in the diagnosis and management of patients with lms . 
crompton strategies for uterine tumors that could potentially harbor lms.32 second , there is significant clinical uncertainty regarding which patients with lms derive benefit from adjuvant chemotherapy and radiation.10 , 33 , 34 should ctdna levels bear prognostic significance for tumors that are at highest risk of recurrence or identify the presence of residual disease , their measurement may help guide clinical decisions regarding adjuvant therapies . 
finally , ctdna levels may be a useful indicator of response to systemic therapy and provide an early indication for switching or intensifying treatment regimens used in this disease.3 , 35 together with technologic improvements in sensitivity and throughput , these initial reports that identify ctdna in lms may quickly evolve to transform clinical practice . 
andersen no relationship to discloses edwin thai no relationship to discloses suzanne george stock and other ownership interests : abbott laboratories , abbvie ( i ) , allergan ( i ) consulting or advisory role : blueprint medicines , deciphera , astrazeneca , blueprint medicines , bayer , eli lilly research funding : pfizer ( inst ) , novartis ( inst ) , bayer ( inst ) , ariad pharmaceuticals ( inst ) , blueprint medicines ( inst ) , deciphera ( inst ) patents , royalties , other intellectual property : uptodate expert testimony : bayer other relationship : research to practice brian d . 
crompton , broad institute of massachusetts institute of technology and harvard , cambridge , ma ; and gavin ha , fred hutchinson cancer research center , seattle , wa . supported by the american society of oncology conquer cancer foundation young investigator award ( m.l.h. ) , national institutes of health grant no . 
toro jr , travis lb , wu hj , et al : incidence patterns of soft tissue sarcomas , regardless of primary site , in the surveillance , epidemiology and end results program , 1978 - 2001 : an analysis of 26 , 758 cases . 
ducimetire f , lurkin a , ranchre - vince d , et al : incidence of sarcoma histotypes and molecular subtypes in a prospective epidemiological study with central pathology review and molecular testing . 
hensley ml , ishill n , soslow r , et al : adjuvant gemcitabine plus docetaxel for completely resected stages i - iv high grade uterine leiomyosarcoma : results of a prospective study . 
oxnard gr , paweletz cp , kuang y , et al : noninvasive detection of response and resistance in egfr - mutant lung cancer using quantitative next - generation genotyping of cell - free plasma dna . 
klega k , imamovic - tuco a , ha g , et al : detection of somatic structural variants enables quantification and characterization of circulating tumor dna in children with solid tumors . 
mermel ch , schumacher se , hill b , et al : gistic2.0 facilitates sensitive and confident localization of the targets of focal somatic copy - number alteration in human cancers . 
stover dg , parsons ha , ha g , et al : association of cell - free dna tumor fraction and somatic copy number alterations with survival in metastatic triple - negative breast cancer . 
oxnard gr , thress ks , alden rs , et al : association between plasma genotyping and outcomes of treatment with osimertinib ( azd9291 ) in advanced nonsmall - cell lung cancer . 
van roy n , van der linden m , menten b , et al : shallow whole genome sequencing on circulating cell - free dna allows reliable noninvasive copy - number profiling in neuroblastoma patients . 
heitzer e , ulz p , belic j , et al : tumor - associated copy number changes in the circulation of patients with prostate cancer identified through whole - genome sequencing . 
shulman ds , klega k , imamovic - tuco a , et al : detection of circulating tumour dna is associated with inferior outcomes in ewing sarcoma and osteosarcoma : a report from the childrens oncology group . 
hensley ml , wathen jk , maki rg , et al : adjuvant therapy for high - grade , uterus - limited leiomyosarcoma : results of a phase 2 trial ( sarc 005 )  . 
reed ns , mangioni c , malmstrm h , et al : phase iii randomised study to evaluate the role of adjuvant pelvic radiotherapy in the treatment of uterine sarcomas stages i and ii : an european organisation for research and treatment of cancer gynaecological cancer group study ( protocol 55874 )  . 
 translating in vivo metabolomic analysis of succinate dehydrogenasedeficient tumors into clinical utility purpose mutations in the mitochondrial enzyme succinate dehydrogenase ( sdh ) subunit genes are associated with a wide spectrum of tumors , including pheochromocytomas and paragangliomas , gi stromal tumors , renal cell carcinomas , and pituitary adenomas . 
our aim was to investigate the potential clinical applications of proton - 1 magnetic resonance spectroscopy ( 1h - mrs ) in a range of suspected sdh related tumors . patients and methods fifteen patients were recruited to this study . 
sequential imaging in a patient with a metastatic abdominal paraganglioma demonstrated loss of the succinate peak after four cycles of [ 177lu ] dotatate , with a corresponding biochemical response in normetanephrine . conclusion this study has demonstrated the translation into clinical practice of in vivo metabolomic analysis using 1h - mrs in patients with sdh - deficient tumors . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the succinate dehydrogenase ( sdh ) enzyme is composed of four subunits ( a to d ) and plays a key role in the krebs cycle and oxidative phos phorylation.1 in the past two decades , germ line mutations in the genes encoding the four sdh subunits ( sdha , sdhb , sdhc , and sdhd ) , collectively known as sdhx , have emerged as an important cause of human neoplasia and a par adigm for the role of disordered cellular meta bolism in oncogenesis.27 sdhx mutations were described initially in association with head and neck paragangliomas ( pgls ; derived from para sympathetic ganglia ) and in pheochromocytomas and pgls ( ppgls ; derived from sympathetic ganglia and often secreting catecholamines ) .2 , 3 it is now recognized that approximately 40% of patients with ppgls harbor germ line muta tions in inherited ppgl genes , and sdhx mutations comprise the most common cause of ppgl predisposition.8 in addition , germ line sdhb mutations are associated with a high risk of malignancy in ppgls.9 other tumor types associated with sdhx mutations include gi stromal tumors ( gists ) and renal cell car cinomas ( rccs ) .1013 gists are mesenchymal tumors of the gi tract and in adults are usually associated with somatic activating mutations in ruth t . 
 the kit or pdgfra gene.4 , 11 however , gists without kit or pdgfra gene mutations , 4 known as wildtype gists ( wtgists ) , account for 15% of adult and 85% of pediatric gists , and recent studies suggest that up to 88% of wtgists are sdh deficient.11 a wtgist with sdh deficiency may harbor a germ line sdhx mutation ( 75% of cases ) or an sdhc gene epi mutation with hypermethylation of the pro moter region.11 only approximately one third of patients with sdhdeficient wtgists achieve disease stabilization with imatinib therapy , 12 and the risk of metastatic disease is higher with sdhdeficient gists compared with conven tional gists.11 , 12 sdhx - associated rcc may present in patients with a personal or family his tory of ppgl or may present with an rcconly phenotype.13 finally , germ line sdhx mutations have been described in rare patients with pitu itary adenomas.10 despite recent advances in the understanding of the sdhx genes , there are many areas of unmet clinical need , including a lack of robust biomarkers to predict aggressive biologic behavior and inform clinical surveil lance and management.14 succinate has been shown to be elevated by 100fold in sdhxmutated ppgls ex vivo compared with nonsdhxmutated ppgls.15 recently , in vivo detection of succinate by mag netic resonance spectroscopy ( mrs ) was reported in two patient cohorts with sdhdeficient ppgls.16 , 17 similarly , the noninvasive detec tion of 2hydroxyglutarate with proton1 mrs ( 1hmrs ) has been demonstrated within glio mas in patients with gainoffunction mutations in another citric acid cycle enzyme , isocitrate dehydrogenase 1.18 the ability to measure succi nate in vivo has a number of important potential clinical applications , including early identifica tion of sdh deficiency , which could enable tai lored patient surveillance and management . 
suitable patients were identi fied based on sdhx germ line status , suspicious clinical phenotype ( metastatic ppgl , pgl , or wtgist ) , and / or immunohistochemistry of tumor tissue showing absent sdhb immuno staining . 
all participants provided written informed consent , and the study was approved by the cambridge south research ethics committee . mrs analysis both sage ( ge healthcare , waukesha , wi ) and lcmodel ( sprovencher.com ) 19 spectros copy analysis programs were used to recon struct , analyze , and display spectra . 
 ( c ) axial fused [ 18f ] fluorodeoxyglucose ( [ 18f ] fdg ) positron emission tomography ( pet ) / computed tomography ( ct ) image demonstrating an [ 18f ] fdgavid carotid body paraganglioma after sdh deficiency was demonstrated on proton1 mr spectroscopy ( 1hmrs )  . 
three patients had multicentric primary tumors , including patient 5 , who presented with a metastatic wtgist and was subsequently diagnosed with a 1.9cm carotid body pgl ( fig 1d ) ; patient 9 , with an abdominal pgl and a small leftsided 1.5cm carotid pgl ( fig 2b ) ; and patient 8 , with a large leftsided glomus pgl and a 2cm prolactin secreting pituitary adenoma ( data supplement )  . 
 genotype a germ line mutation in an sdhx gene was iden tified in nine ( 60% ) of 15 patients : five in sdhb ( four missense variants and one truncating vari ant ) and four in sdha ( one missense and three truncating )  . 
two additional patients were found to have somatic sdhc epimutations ( table 1 )  . 1h - mrs succinate analysis the 1hmrs characteristics of the 15 patients are listed in the data supplement . 
the liver was the most common site to be assessed ( n = 6 ) , but goodquality spectra were also obtained from a pituitary tumor ( n = 1 ) and ppgls ( n = 5 )  . 
patient 4 had a met astatic wtgist with no detectable germ line sdhx mutation and preserved sdhb protein expression in the tumor tissue ; choline was con fidently fitted on lcmodel , but no succinate was seen . 
patient 6 demonstrated a goodquality spectrum from the remnant pituitary adenoma ; choline was detected on lcmodel and sage processing , but no succinate was detected , and this finding was consistent with the preserva tion of sdhb protein expression in the pitu itary tumor by immunohistochemistry ( fig 4 )  . 
patient 12 demonstrated no reliable detection of succinate or choline because of motion artifact and a low signaltonoise ratio ( snr ) , which probably resulted from inconsistent breathing , because the voxel was at the edge of the liver . 
a metastasis on the edge of the liver was imaged in patient 14 , where again incon sistent respiration probably led to displace ment of the voxel into adjacent adipose tissue . 
 ( a ) t2weighted magnetic resonance image from patient 1 and ( b ) t1weighted image from patient 3 demonstrating liver metastases from which spectra were acquired in the locations indicated by the white arrows . 
after four cycles of treatment , a repeat 1hmrs examina tion on the same pelvic nodal metastases revealed a choline peak but no succinate peak ( fig 5c )  . 
 although the magnetic resonance imaging fea tures of the metastatic lesions were unchanged pre and posttreatment , the loss of a succi nate peak was correlated with a reduction in plasma normetanephrine levels ( from 1 , 861 to 1 , 193 pmol / l ) and tumor avidity on [ 18f ] fluo rodeoxyglucose ( [ 18f ] fdg ) positron emission tomography ( pet ) / computed tomography ( ct ; standardized uptake value : pretreatment , 16.1 ; posttreatment , 9.3 ; figs 5d to 5f )  . 
the detec tion of choline on the acquired spectra both before and after treatment indicates that tumor necrosis is unlikely to account for the absent suc cinate peak posttreatment . a sequential 1hmrs study was performed for patient 5 because of evidence of progressive disease on surveillance ct , despite treatment with a multikinase inhibitor , regorafenib . 
the results for scr were almost identical in these two patients , suggesting good test reproducibility ( data supplement )  . discussion this proofofprinciple study demonstrates that detection of a succinate peak and an increased scr was specific for a variety of sdhdeficient tumor types . 
all six tumors with a positive suc cinate peak and elevated scr were associated with a germ line sdhx mutation ( n = 4 ) or an sdhc epimutation ( n = 2 )  . 
 ( c ) succinate dehydrogenase b ( sdhb ) immunohistochemistry demonstrating preserva tion of the sdhb protein performed on a section of tumor tissue debulked from the pituitary tumor . adequate 1hmrs demonstrated preservation of sdhb expression in the tumors analyzed . 
our findings are complementary to a previous study in which 1hmrs was applied in nine patients with pgls , and succinate peaks were detected in all five with sdhx mutations but not in the four patients without mutations.16 we demonstrate for the first time to our knowledge that 1hmrs can also be used to determine the sdh status of gists and pituitary adenomas and that succinate peaks can be detected in sdhdeficient tumors with epigenetic inactivation of sdhc . 
potential diagnostic applications of this new approach include : assessing the pathoge nicity of patients with germ line sdhx variants of uncertain significance and potentially sdh related tumors ; investigating possible metastatic lesions ( eg , in the liver ) in patients with germ line sdhx mutations and primary sdhdeficient tumors ; assessing patients with multiple pri mary tumors to determine if all are sdh defi cient ; identifying patients without detectable germ line sdhx mutations who might benefit from specialist genetic investigations , such as sdhc promoter methylation status ; and assess ing sdh tumor status preoperatively , particu larly for patients with possible wtgists , because standard adjuvant treatment with imatinib has proven to be less effective in patients with sdh deficient disease.12 notably , here we use the presence of a choline signal as an internal control for viable tissue to discriminate technical failures from a negative finding . 
 this trend is the opposite of what would be expected if necrosis were artificially lowering the overall succinate levels in large tumors and therefore suggests that the method is measuring real differences in succinate , which are indepen dent of tumor size . 
 ( b ) spectra acquired before treatment illustrating succi nate accumulation at 2.4 pp ( c ) spectra ac quired after four cycles of [ 177lu ] dotatate with no detectable succinate peak at 2.4 pp ( d ) plasma metanephrine and methoxytyramine levels before and after treatment with [ 177lu ] dotatate . 
as a consequence , sdhdeficient tumors demonstrate epigenetic abnormalities and activated hypoxic gene responses , and more recently , evidence has suggested that succinate may have a paracrine effect on stromal tis sue.2022 understanding the molecular mech anisms of sdhrelated tumorigenesis provides a rationale for novel therapeutic interventions such as reversing the epigenetic abnormalities or exploiting metabolic vulnerabilities , similar to the recent discovery that tumoral 2hydroxyglutarate accumulation may increase responsiveness to olapa rib , a poly ( adpribose ) polymerase inhibitor.23 the availability of sensitive noninvasive bio markers would greatly facilitate precision medicinebased clinical trials . 
1hmrs is highly specific and allows in vivo detection of individual metabolites without the use of ionizing radiation ; however , 1hmrs is significantly less sensitive than pet , which could limit the detection of low levels of succinate , and it can be challenging to differen tiate intracellular from extracellular metabolites . 
 in the future , 1hmrs may be complemented by other techniques , such as hyperpolarized car bon13 mrs , which can increase 13mrs snr by several orders of magnitude , allowing assess ment of enzyme flux in vivo.26 we show that 1hmrs could be a valuable tool for the assessment of tumor response in the con text of radionuclide and other therapies , because alterations in succinate levels were detected despite stable appearance of the tumor diam eters . 
this important application of 1hmrs could be expanded to include other tumors with specific metabolic defects , including fuma rate hydratasedeficient tumors , 27 idh1mutant tumors , 18 and the recently identified malate dehydrogenase 2deficient tumors.28 however , important limitations of in vivo metabolomic analysis using 1hmrs were also revealed by our study ; for example , spectral quality was poor in close proximity to metal dental work , in areas adjacent to air spaces such as the lung , and in bone metastases and was susceptible to motion artifact . 
in this study , the technical failure rate was 26% , which is similar to the failure rate reported in previous studies using 1hmrs.16 importantly , no patient cases were excluded from this prospective study , with the intention that this would inform the translation of this imaging modality into clinical practice . 
on the basis of the evidence from this exploratory study , we recommend that tumors be selected for 1hmrs analysis based on the following : ideally the largest tumor deposit but at least > 2 cm in size ; tumors located close to bone or lung should be avoided ; tumors with significant necrosis or hemorrhage should be avoided ; superficial tumor deposits should be selected preferentially ; and respiratorytriggered acquisition should be used for tumors in the upper abdomen , such as hepatic metastases . although the use of 1hmrs as a diagnos tic tool is likely to be limited to specialist cen ters , the number of scan averages in our study during spectral acquisition was less than half those reported in a previous study16 ( 200 v 512 ) , without demonstrating a reduction in sensi tivity . 
furthermore , this imaging modal ity could be used to investigate other metaboli cally driven tumors . in conclusion , this study is the largest to date to our knowledge to evaluate 1hmrs in patients with sdh deficiency . 
it reveals that 1hmrs has the potential to be used as a noninvasive biomarker in the precision management of sdhdeficient disease and could have a role as a biomarker of successful treatment response . 
mclean stock and other ownership interests : veryan medical patents , royalties , other intellectual property : patent for stent design for arterial bypass graft basetti madhu no relationship to disclose benjamin g . 
challis no relationship to disclose rogier ten hoopen no relationship to disclose thomas roberts no relationship to disclose consulting or advisory role : bayer healthcare pharmaceuticals , ariad pharmaceuticals speakers bureau : pfizer travel , accommodations , expenses : pierre fabre , teva pharmaceuticals europe helen l . 
bulusu honoraria : pierre fabre kieran allinson no relationship to disclose lisa happerfield no relationship to disclose soo - mi park no relationship to disclose alison marker no relationship to disclose olivier giger stock and other ownership interests : cambridge pathology eamonn r . 
xekouki p , stratakis ca : succinate dehydrogenase ( sdhx ) mutations in pituitary tumors : could this be a new role for mitochondrial complex ii and / or krebs cycle defects ? endocr relat cancer 19 : c33c40 , 2012 7 . 
boikos sa , pappo as , killian jk , et al : molecular subtypes of kit / pdgfra wildtype gastrointestinal stromal tumors : a report from the national institutes of health gastrointestinal stromal tumor clinic . 
holdsworth ch , badawi rd , manola jb , et al : ct and pet : early prognostic indicators of response to imatinib mesylate in patients with gastrointestinal stromal tumor . 
 o comparative analysis of durable responses on immune checkpoint inhibitors versus other systemic therapies : a pooled analysis of phase iii trials elvire pons - tostivint , md1 , 2 ; aur elien latouche , phd3 ; pauline vaard , md1 ; francesco ricci , md , phd1 ; delphine loirat , md , phd1 ; s egol `ene hescot , md , phd1 ; marie - paule sablin , md1 ; roman rouzier , md , phd3 , 4 ; maud kamal , phd1 ; claire morel , msc1 ; charlotte lecerf , msc1 ; vincent servois , md1 ; xavier paoletti , phd5 ; and christophe le tourneau , md , phd1 , 3 , 6 purpose immune checkpoint inhibitors ( icis ) have been demonstrated to improve overall survival ( os ) in several tumor types . 
the proportion of patients who experienced an os that exceeded two times the median os of the whole patient population also was estimated . results nineteen studies involving 11 , 640 patients treated in 42 treatment arms ( 26 ici and 16 non - ici arms ) were included . 
the mean proportion of patients who experienced a durable response was 2.3 times higher in those treated with an ici compared with those treated in the control arms ( 25% v 11% )  . 
durable responses were more frequent in patients treated with antipd - 1 / pd - l1 agents than in patients treated with antictla - 4 agents ( 28% v 18% )  . 
the mean proportion of patients who had an os that exceeded two times the median os was also higher in those treated with icis than in those treated in the control arms ( 30% v 23% )  . 
2019 by american society of clinical oncology introduction immune checkpoint inhibitors ( icis ) that target cytotoxic t - lymphocyte protein - 4 ( ctla - 4 ) and programmed cell death protein 1 ( pd - 1 ) and its ligand pd - l1 have been demonstrated to improve overall survival ( os ) in several tumor types.1 - 12 in 2011 , ipilimumab , a fully human immunoglobulin g1 monoclonal antibody that targets ctla - 4 , was the rst ici to be approved by the food and drug administration for the treatment of patients with previously treated advanced melanoma because of a signicant improvement in os in two randomized phase iii clinical trials.8 , 13 antipd - 1 icis , including nivolumab and pembrolizumab , and antipd - l1 icis , including atezolizumab , avelumab , and durvalumab , were subsequently approved by the food and drug administration not only in recurrent melanoma but also in several other tumor types , including nonsmall - cell lung cancer ( nsclc ) , renal cell carcinoma , head and neck squamous cell carcinoma , urothelial carcinoma , merkel cell carcinoma , and hodgkin lymphoma . patients with cancer with recurrent and / or metastatic disease usually have been considered as being incurable . 
when a duplicate publication of the same trial was found , the study with the most complete and updated report was included . selection criteria studies meeting all of the following criteria were selected : prospective randomized phase iii trials of icis in patients with cancer treated in the recurrent and / or metastatic setting , trials with os and / or progression - free survival ( pfs ) as a primary end point , and availability of the os and pfs kaplan - meier survival curves in the publications . 
finally , trials were excluded if the follow - up was insufcient to estimate the proportion of patients who experienced a durable response ( see statistical analyses )  . data extraction data extracted from eligible trials were tumor type , class of drugs in each treatment arm , number of patients in each treatment arm , number of previous lines of treatment in the recurrent and / or metastatic setting , median pfs , median os , the proportion of patients with a pfs exceeding three times the median pfs in each arm , and the proportion of patients with an os exceeding two times the median os in each arm ( fig 1 )  . statistical analyses because no denition of durable response existed , we arbitrarily dened as a durable response for a specic patient a pfs that exceeded three times the median pfs of all patients treated with the same drugs in the same trial . 
we also estimated the proportion of patients who experienced an os that exceeded two times the median os of all patients treated with the same drugs in the same trial . 
using digitizelt software ( digitzeit , braunschweig , germany ) , proportions of patients who experienced a pfs / os that exceeded three / two times the median pfs / os in each arm were measured directly from the extracted kaplan - meier curves.17 , 18 proportions were compared using the mannwhitney u test and represented using graphpad ( graphpad software , la jolla , ca )  . 
twelve of these were excluded for the following reasons : absence of a monotherapy ici arm ( n = 3 ) , adjuvant setting ( n = 3 ) , duplicate trials ( n = 5 ) , and insufcient follow - up ( n = 1 )  . 
the 19 remaining phase iii trials involved 11 , 640 patients treated in 42 different treatment arms ( table 1 )  . tumor types included melanoma ( seven trials ) , 8 - 12 , 23 , 24 nsclc ( ve trials ) , 1 - 3 , 19 urothelial carcinoma ( two trials ) , 6 , 20 prostate cancer ( two trials ) , 21 , 22 head and neck squamous cell carcinoma ( one trial ) , 4 gastric cancer ( one trial ) , 5 and renal cancer ( one trial ) .7 a total of 7 , 769 patients were randomly assigned to an ici treatment in 26 arms . 
the remaining 3 , 871 patients were treated with chemotherapy ( 11 arms ) , a molecularly targeted agent ( one arm ) , a vaccine ( one arm ) , and a placebo ( three arms )  . 
twelve ( 63% ) of the 19 trials were conducted in patients having received at least one prior line of treatment in the recurrent and / or metastatic setting , whereas patients were treated in the rst - line recurrent and / or metastatic setting in ve trials ( 26% ) and without restriction in terms of prior treatments in the two remaining trials ( 11% )  . 
crossover from the control arm to the ici arm was allowed in ve trials ( 26% )  . proportion of durable responses the mean of the median follow - ups was 15.7 months ( range , 5 to 38 months )  . 
the mean proportion of patients who experienced an os that exceeded two times the median os was 30% ( 95% ci , 28% to 32% ) in the ici arms versus 23% ( 95% ci , 21% to 26% ) in the other arms ( p , .001 , mann - whitney u test ; fig 3b ; table 2 )  . predictors of durable responses because durable responses were well reported in patients with melanoma treated with icis , 15 we compared the proportion of durable responses in patients with and without melanoma . 
estimated proportion of patients with a survival probability that exceeded two times the median survival in each treatment arm . articles that did not match the selection criteria ( n = 322 ) phase iii randomized trials that involved at least one immune checkpoint inhibitor arm ( n = 31 ) combination trials adjuvant setting duplicate insufficient follow - up ( n = 3 ) ( n = 3 ) ( n = 5 ) ( n = 1 ) subgroup of patients with nsclc , given the high number of trials in this latter tumor type . 
nonmelanoma trials involved 6 , 991 patients treated in 13 ici arms and 12 non - ici arms ( table 1 )  . the mean proportion of patients in the ici arms who had a pfs that exceeded three times the median pfs was 28% ( 95% ci , 22% to 34% ) in the melanoma trials versus 23% ( 95% ci , 20% to 26% ) in the nonmelanoma trials ( p not signicant , mann - whitney u test ; fig 4a ; table 2 )  . 
the mean proportion of patients in the ici arms who experienced an os that exceeded two times the median os was 30% ( 95% ci , 26% to 33% ) in the melanoma trials versus 30% ( 95% ci , 26% to 33% ) in the nonmelanoma trials ( p not signicant ; mann - whitney u test )  . 
results were similar when the subgroup of nonmelanoma trials was restricted to nsclc trials ( table 2 )  . we then evaluated whether the number of previous lines of treatment in the recurrent and / or metastatic setting affected the results . 
trials beyond the rst - line recurrent and / or metastatic setting involved 6 , 991 patients treated in 14 ici arms and 12 non - ici arms ( table 1 )  . 
the mean proportion of patients in the ici arms who had a pfs that exceeded three times the median pfs was 30% ( 95% ci , 20% to 40% ) in the rst - line trials versus 23% ( 95% ci , 19% to 26% ) in the beyond - the - rst - line trials ( p not signicant , mann - whitney u test ; fig 4b ; table 2 )  . 
the mean proportion of patients who had an os that exceeded two times the median os in the rst - line setting could not be calculated because of a too - short follow - up . we nally evaluated whether the proportion of durable responses depended on the target of the icis ( pd - 1 / pd - l1 v ctla - 4 )  . 
the mean proportion of patients treated with an antipd - 1 / pd - l1 agent who had a pfs that exceeded three times the median pfs was 28% ( 95% ci , 24% to 31% ) versus 18% ( 95% ci , 15% to 21% ) for patients treated with an antictla - 4 agent ( p , .001 , mann - whitney u test ; fig 4c ; appendix table a1 )  . 
the mean proportion of patients who had an os that exceeded two times the median os was 31% ( 95% ci , 28% to 34% ) in patients treated with an antipd - 1 / pd - l1 agent compared with 29% ( 95% ci , 26% to 32% ) in patients treated with an antictla - 4 agent ( p not signicant , mann - whitney u test ; appendix table a1 )  . the effect of in multivariable analysis , treatment with antipd - 1 / pd - l1 agents ( p , .001 ) and the effect of rstline treatment ( p = .02 ) were statistically associated with a higher mean proportion of durable responses ( appendix table a2 )  . discussion our study conrms that a higher proportion of patients experience durable responses to icis than to other drug classes ( 25% v 11% )  . 
proportion of patients who had ( a ) a progression - free survival ( pfs ) that exceeded three times the median pfs and ( b ) an overall survival ( os ) that exceeded two times the median os according to drug classes . 
these results are of primary importance because it cannot be excluded that some patients who experience a durable response might be cured of their recurrent and / or metastatic cancer , which represents the overarching goal of cancer research . 
estimation of the proportion of patients with a pfs that exceeds three times the median pfs of the whole cohort of patients treated with the same drugs instead of arbitrarily dening a minimum pfs is an elegant way not to be biased by heterogeneity in terms of the natural history of the disease , clinical setting , and drugs used . 
we selected a threshold of at least two times the median for os because the followup was insufcient in most of the trials to get the information for three times the median os . 
using durable response as we dened it provides additional information that is not given by any other classic end point , such as duration of response or pfs because it is calculated on the basis of the median pfs of the whole treatment arit gives an insight into the proportion of patients who experience durable responses and takes into account the natural history of the disease and the overall activity of the treatment . 
whether this measure correlates with os , which can be evaluated only with individual data , remains to be determined . twenty - ve percent of patients treated with icis in the trials retrieved for our study had a durable response according to our denition . 
although the proportion of durable responses is high and conrms one of the specicities of icis , 11% of patients treated with other drug classes , including chemotherapy and targeted therapy , also experienced durable responses , which means that this phenomenon is not unique to immunotherapy . 
how the results of our study would have been affected by such patient populations remains to be determined . the proportion of patients who had an os that exceeded two times the median os was also higher in patients treated with an ici compared with those treated with other drug classes , although to a lesser extent ( 30% v 23% )  . 
this difference might be explained by two factors . first , the threshold chosen of two times the median was lower for os than for pfs ( for the reasons explained at the beginning of the discussion )  . 
proportion of patients who had a progression - free survival ( pfs ) that exceeded three times the median pfs according to ( a ) tumor type ( melanoma v nonmelanoma ) , ( b ) clinical setting ( rst v second line or greater of treatment ) , and ( c ) drug classes ( antiprogrammed cell death 1 [ pd - 1 ] / programmed death - ligand 1 [ pd - l1 ] v anticytotoxic t - cell lymphocyte - 4 [ ctla - 4 ] agents )  . 
for example , 58% of patients crossed over in the nivolumab versus chemotherapy nsclc trial.19 reporting of long - term os data will be key to estimate the real effect on os . one of the limitations of our study is the small number of non - ici arms , which hampered the separate evaluation of the proportion of durable responses in patients treated in the various control arms . 
we attempted as well to include in our study phase iii trials that did not involve ici arms to have a better representation of patients treated with chemotherapy and targeted therapy . 
however , the lower proportion of patients who experienced durable responses to other drugs than icis in our study conrms the usual short - lived responses reported with chemotherapy and targeted therapy ( mainly those related to the occurrence of resistance mutations in this latter case )  . 
finally , we restricted our analysis to trials with sufcient follow - up to estimate the proportion of patients who experienced a durable response , as dened in patients and methods under statistical analyses , which means that the use of our end point cannot be generalized to all trials . in conclusion , our pooled analysis of randomized phase iii trials objectively conrms that durable responses are more frequent with icis than with other drug classes , especially with icis that target pd - 1 and pd - l1 . 
our study also shows that durable responses according to our denition are not specic to icis because this phenomenon also exists with targeted therapies and chemotherapy , although to a lower extent . 
the identication of predictive biomarkers of efcacy , and especially durable response , is of upmost importance to select patients who will need only a single - agent ici and patients for whom a drug combination will be necessary . 
horn l , spigel dr , vokes ee , et al : nivolumab versus docetaxel in previously treated patients with advanced nonsmall - cell lung cancer : two - year outcomes from two randomized , open - label , phase iii trials ( checkmate 017 and checkmate 057 )  . 
herbst rs , baas p , kim d - w , et al : pembrolizumab versus docetaxel for previously treated , pd - l1 - positive , advanced non - small - cell lung cancer ( keynote010 ) : a randomised controlled trial . 
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lancet 389 : 255 - 265 , 2017 ferris rl , blumenschein g jr , fayette j , et al : nivolumab for recurrent squamous - cell carcinoma of the head and neck . 
n engl j med 375 : 1856 - 1867 , 2016 kang y - k , boku n , satoh t , et al : nivolumab in patients with advanced gastric or gastro - oesophageal junction cancer refractory to , or intolerant of , at least two previous chemotherapy regimens ( ono - 4538 - 12 , attraction - 2 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
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larkin j , minor d , dangelo s , et al : overall survival in patients with advanced melanoma who received nivolumab versus investigators choice chemotherapy in checkmate 037 : a randomized , controlled , open - label phase iii trial . 
lee ck , davies l , wu y - l , et al : getinib or erlotinib vs chemotherapy for egfr mutation - positive lung cancer : individual patient data meta - analysis of overall survival . 
in patients with stage iii or iv melanoma , early changes in ctdna within 1 month after initiation of treatment correctly predicted recist response categories in 19 of 20 patients . 
 braune et al context key objective we evaluated ctdna in stage iii and iv melanoma to detect active disease and to predict response to treatment . knowledge generated ctdna had superior sensitivity to ldh and s100 in detecting active disease in stage iv melanoma . 
written informed consent was obtained from all patients . isolation and quantitation of ctdna from plasma blood samples were collected in edta tubes ( sarstedt , n umbrecht , germany ) and centrifuged twice within the 2 hours after collection . 
the supernatant was stored at 80c . cell - free ctdna was extracted from 2 ml using the qiasymphony circulating dna kit ( qiagen , hilden , germany ) according to the manufacturers instructions and was eluted in 60 l of elution buffer . 
the limit of blank , limit of detection , and lowest detectable copy ratio were determined for each assay ( data supplement )  . imaging analysis imaging and quantitative analyses were performed by a single radiologist blinded to results of the ctdna analyses . 
workows for ct and magnetic resonance imaging are capable of automated segmentation and volume measurements . pet imaging and quantication 18f - uorodeoxyglucose scans were performed with a 64 - slice gemini tf positron emission tomography ( pet ) / ct scanner or a 16 - slice gemini tf big bore pet / ct scanner ( philips healthcare for both ) .17 a contrast - enhanced diagnostic ct ( 120 kvp , 100 , 400 mas , dose modulation applied ) or a low - dose ct ( 120 kvp , 25 mas ) scan was performed for attenuation correction and spatial allocation . 
for each pet study , a quantitative analysis was performed using rover v2.1.12 ( abx , radeberg , germany ) .18 , 19 a threshold of 40% of maximum standardized uptake value was chosen for the determination of the metabolic tumor volume ( mtv ) .20 statistical analysis data analysis was performed separately by stage for all eligible patients . 
correlations were calculated by using a log scale , and ldh and s100 measurements below the standard value were set to the standard value . within - patient correlation was accounted for in the correlation analysis and in the estimation of the progression - free survival ( pfs ) hazard ratio ( hr ) in stage iv patients . 
patient characteristics ( continued ) characteristic 66 ( 28 - 92 ) tissue mutation status braf exon 15 v600e v600k v600r k601n d594g l597s w604c nras q61 q61k q61r total patients female male age , years median ( range ) 60  . 
60 stage stage iii newly diagnosed previous treatment treatment after inclusion surgery surgery radiation systemic treatment relapsed previous treatment of relapse treatment of relapse after inclusion surgery radiation systemic treatment no . 
of previous lines of therapy stage iv mean ( range ) treatment at inclusion braf / mek inhibitor immunotherapy treatment after inclusion immunotherapy braf / mek inhibitor radiotherapy surgery interferon vaccination ( continued in next column ) 1.7 ( 0 - 7 ) * systemic treatment after progression to stage iv . three patients received systemic treatment for unresectable stage iii melanoma , and three patients received systemic treatment after progression to stage iv melanoma . total number of tissue mutations is 64 . 
patient 62 was tissue positive for nras q61r and braf w604c , patient 55 had resection of two different melanomas before inclusion in the study ( one was positive for braf v600e , and the other was positive for nras q61k )  . 
the mean number of samples was 6.8 ( range , 1 to 15 samples ) per patient with stage iii disease , and the mean was 5.8 ( range , 1 to 27 samples ) for stage iv patients . in patients with stage iii disease , 10 ( 83.3% ) of 12 were positive for ctdna at least once ; for patients with stage iv disease , 44 ( 88% ) of 50 patients were positive for ctdna at least once ( table 2 )  . 
s100 and ldh are indicated as being increased when level is above the normal range of , 0.105 mg / l for s100 and 135 to 225 u / l for ldh . 
we identied 10 stage iii and 30 stage iv patients with 56 samples obtained up to 30 days before surgery , initiation of systemic treatment , or change in systemic treatment . 
even when they were combined , ldh and s100 detected measurable disease in only 34 ( 60.7% ) of 56 samples before initiation of treatment ( table 3 ; fig 1c )  . 
thus , ctdna detected a higher proportion of patients with active disease . amount of mutated ctdna correlates with ldh and s100 to compare ctdna with the established biomarkers ldh and s100 , we studied measurement pairs obtained at the same time points . 
ctdna strongly correlated with s100 ( r = 0.64 based on 278 measurement pairs from 62 patients ) and ldh ( r = 0.50 based on 288 measurement pairs from 61 patients )  . ctdna reects tumor volume and metabolic activity we next asked whether mutant ctdna levels correlate with tumor burden . 
analysis was performed according to change in the sum of the diameters of target tumor lesions from baseline to rst ( fig 2a ) and subsequent ( fig 2b ) follow - up imaging scans according to recist 1.1. 
 ( a ) percentage of positive ( ctdna ) or increased ( lactate dehydrogenase [ ldh ] , s100 ) samples from 274 time points with matched ctdna , ldh , and s100 samples for stage iii and stage iv patients , respectively . 
red lines indicate the mean value for ctdna , ldh , or s100 . dotted lines indicate the thresholds of ldh ( 225 u / l ) and s100 ( 0.105 ug / l ) above which values are stated as being increased . 
 ( c ) sensitivity of ctdna , ldh , and s100 to detect disease within 30 days before surgery , initiation of treatment , or change in treatment ( see table 3 for details )  . 
of note , one patient who displayed a new lesion despite favorable ctdna course had an additional braf w604c mutation detectable at baseline that converted from negative at day 43 to positive at day 91 . 
conversely , all nine patients with partial response according to recist had a positive - to - negative conversion , had a decrease in ctdna , or remained ctdna negative . thus , early ctdna dynamics correctly predicted progressive disease or partial response according to recist in 21 of 24 patients . 
the remaining patient had a ctdna - positive sample available 1 day after imaging ( patient 60 ; fig 2c )  . ctdna predicts outcome we analyzed stage iii patients with a ctdna measurement within 30 days after surgery or at initiation of systemic therapy . 
four patients did not meet these criteria because they had no samples within 30 days after surgery ( n = 3 ) or at the initiation of systemic treatment ( n = 1 )  . 
thus , the higher levels of ctdna that appeared early after initiation of treatment or change in treatment indicated inferior pfs . dynamic ctdna proles of individual patients results of biomarker assessment in individual patients demonstrate that ctdna analysis over time is informative with respect to tumor dynamics as shown in the data supplement . 
ctdna demonstrated a superior dynamic signal range compared with ldh and s100 , and ctdna detected progression whereas ldh ( data supplement ) or ldh and s100 ( fig 1c , g ) failed to detect progression . 
of note , the combination of all three biomarkers provides an 8.9% increase in sensitivity to ctdna alone . thus , ctdna might be used together with ldh and s100 in a combined biomarker score . 
we observed a signicant association of ctdna at baseline with ldh , s100 , tumor size , and mtv ( r2 = 0.87 ) , the latter displaying the strongest correlation . 
this is in agreement with two other studies demonstrating a strong correlation between the number of ctdna copies and mtv in melanoma ( r = 0.63 , 23 and r2 = 0.6949 , 24 respectively )  . 
 ( d ) correlation between ctdna and ( continued on following page ) recist 1.1 , ( e ) tumor volume at baseline assessed by radiologic analysis , and ( f ) tumor metabolic activity , assessed by positron emission tomography / computed tomography ( pet / ct ) scan and expressed as the mean total lesion glycolysis ( tlg ) in [ g / ml x ccm ]  . 
the tlg in the equation [ g / ml x ccm ] was calculated by multiplying the lesion volume with the mean standardized uptake value in the volume of interest . 
eleven patients with stage iii and 22 with stage iv disease with a baseline ctdna sample , radiographic imaging before intervention , and a ctdna sample taken within 30 days after initiation of treatment or change in treatment were analyzed . 
 ( a ) waterfall plot showing the change in sum of diameter ( sod ) of target tumor lesions from baseline to rst follow - up imaging according to recist 1.1 in relation to early changes in ctdna . 
t0 denotes baseline ctdna sample , and t1denotes rst sample after baseline at day 8 to 28 after initiation of or change in treatment with ctdna detectable ( + ) or not detectable ( )  . 
dotted lines represent 20% increase in sod , which indicated progressive disease ( pd ) , or 30% decrease , which indicated partial response ( pr ) according to recist 1.1. 
 ( b ) spider plot showing changes in sod from baseline to rst and subsequent follow - up imaging according to early ctdna dynamic changes from baseline to rst sample after baseline taken within 28 days after institution of or change in treatment . 
cr , complete response ; sd , stable disease . importantly , early changes in ctdna levels were superior to ldh and s100 for early assessment of treatment response . of all the patients who achieved partial response , 76.9% had favorable ctdna dynamics as early as 8 to 28 days after initiation of or change in treatment . 
in line with these observations , detectable ctdna as early as within 30 days after initiation of or change to therapy predicted inferior pfs for patients with stage iii or iv disease . 
in stage iv disease , ctdna with more than 10 copies per ml within 30 days after initiation of or change in treatment indicated a population with a particularly short pfs of only 4 months . 
we included patients who were alive and free of progression 1 month after surgery or at the start of systemic therapy and who had a ctdna measurement within 1 month . 
pfs was dened as the time from initiation of treatment to rst reported progression or to the most recent visit . progression events included progression as dened by recist 1.1 , clinical progression , or melanoma - specic death . 
 ( a ) pfs in eight patients with stage iii disease alive and free of progression after 1 month with a ctdna measurement within 1 month after surgery or start of systemic treatment . 
 ( b - c ) pfs in 36 patients with stage iv disease with 46 pfs sections , alive and free of progression at 1 month by the rst ctdna value taken within 30 patients with days ( median , day 22 ; range , days 1 to 30 ) after start of or change in systemic treatment with a ctdna measurement within 1 month , by ( b ) positive v negative , and ( c ) negative or 10 or fewer copies per ml v more than 10 copies per ml . 
our data suggest that ctdna dynamics allow prediction of response and pfs within in the rst month after implementing braf / mek inhibitors or immunotherapy . in contrast to previous reports , 27 - 30 ctdna at baseline was not a prognostic marker for pfs in patients with stage iv disease in our cohort , whereas the level of ctdna at rst measurement after baseline was clearly predictive for pfs , most likely as an expression of response to treatment . notably in the aforementioned studies , most patients were treated with braf / mek inhibitors whereas the majority of our patients received immunotherapy . 
in two other studies of patients with or without melanoma who were receiving pd - 1 antibodies , there was no association between baseline ctdna and pfs.25 , 31 however , subgroup analyses did not reveal signicant differences because this study was not designed to examine the signicance of baseline ctdna in patients treated with braf / mek inhibitors versus immunotherapy . 
 braune et al nras mutations.27 , 32 this is a possible explanation for the increasing copies of nras - mutated ctdna detected in patient 53 after changing the treatment to dabrafenib and trametinib , which suggests selection of a subclonal mutation that mediates resistance to treatment with braf / mek inhibitors . 
nevertheless , previous studies have demonstrated tumor interand intraheterogeneity involving additional genetic events that lead to mapk or pi3k / pten / akt reactivation when disease progresses during treatment with braf inhibitors.33 , 34 few studies address the use of ctdna as a biomarker in stage iii melanoma . 
but in one recent study , ctdna positivity within 12 weeks after surgery indicated adverse disease - free survival and os.35 in our cohort , ctdna positivity after resection of the primary tumor and within 1 month after denitive locoregional treatment or start of systemic therapy predicted a poor pfs . 
with adjuvant therapies showing benet for high - risk stage iii melanoma , 9 , 10 ctdna positivity might help to stratify patients for adjuvant treatment . one limitation of this study is the small sample size . 
validation in a larger prospective trial is required , especially for detection of minimal residual disease in stage iii and to examine whether changes of ctdna early after the start of treatment constitute an independent marker for pfs and os for braf / mek inhibitor treatment versus immunotherapy . 
although mutationspecic assays might be most suitable for monitoring response and minimal residual disease , a broader sequencing approach using next - generation sequencing might be used in previously treated patients to track subclonal mutations to understand treatment resistance and to guide further therapy.34 in addition , including tert promoter mutations present in 70% of melanomas36 could increase coverage when added to brafand nrasspecic ctdna assays.37 in conclusion , our results demonstrate that ctdna is superior to ldh and s100 for detecting active disease and suggest that changes in ctdna early after initiation of treatment predict response to treatment and pfs . 
 ctdna as a biomarker in malignant melanoma dagmar von bubnoff honoraria : roche , iomedico travel , accommodations , expenses : bristol - myers squibb frank meiss honoraria : bristol - myers squibb , novartis , pierre fabre consulting or advisory role : bristol - myers squibb , novartis , pierre fabre , roche pharma ag speakers bureau : bristol - myers squibb travel , accommodations , expenses : novartis , bristol - myers squibb , pierre fabre nikolas von bubnoff honoraria : astrazeneca , amgen , bristol - myers squibb , novartis consulting or advisory role : novartis ( inst ) research funding : novartis ( inst ) no other potential conicts of interest were reported . acknowledgments the authors thank renata koch and aurelia winter for sample collection , patient management , and administrative support . references cancer genome atlas network : genomic classication of cutaneous melanoma . 
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 precision oncology strategy in trastuzumab - resistant human epidermal growth factor receptor 2positive colon cancer : case report of durable response to ado - trastuzumab emtansine introduction colorectal cancer is the third most common cancer and the fourth leading cause of cancer death worldwide.1 metastatic disease is ultimately identified in the majority of patients with colorectal cancer and , with rare exceptions , is considered incurable . 
the treatment of metastatic colorectal cancer ( mcrc ) has historically included the use of fluorouracil in combination with other chemotherapeutic agents , including oxaliplatin or irinotecan . the addition of the antivascular endothelial growth factor antibody , bevacizumab , to standard chemotherapy regimens has improved the progression - free and overall survival of patients with mcrc and has signaled a shift toward the addition of biologic and targeted agents in the treatment of advanced cancer.2 , 3 the transition toward molecularly targeted therapies has gained additional momentum with the us food and drug administration approval of the antiepidermal growth factor receptor agents cetuximab and panitumumab for the treatment of kras wild - type colorectal cancers.4 , 5 unfortunately , many patients with mcrc progress through these therapies , or are not candidates to receive them on the basis of the molecular profile of their particular tumor , and are left with few treatment options . 
 the tumor exhibited normal expression of the mismatch repair genes mlh1 , msh2 , msh6 , and pms2 . shortly after diagnosis , the patient began palliative chemotherapy with capecitabine and oxaliplatin every 3 weeks . 
however , follow - up imaging 6 months after treatment initiation identified progressive disease in the liver and lung , as well as a new adrenal gland metastasis . the patients treatment was then changed to capecitabine plus irinotecan and , ultimately , capecitabine , irinotecan , plus cetuximab , but his tumor continued to progress through each of these regimens , as determined by an increasing size of multiple hepatic metastases ( table 1 )  . 
we used a standard set of her2 - specific taqman primers and probes ( thermo fisher scientific , foster city , ca ) compared with standard references using an ultraconserved region on chromosome 1 . 
briefly , taqman pcr reaction mixtures were assembled using 2x ddpcr supermix for probes , 20x assays ( 18 mm primers and 5 mm probe ) and restriction digested dna samples ( bio - rad )  . 
this standard reference assay used the following primers : forward primer : 59 - tgagggattcggcagatgttg - 39 ; reverse primer : 59 - ctgaaaggctggacttgacaga - 39 ; and probe : 59 - vic - actgtgtgctggacctmgb - 39 . 
all assay primers were ordered from integrated dna technologies ( coraville , ia )  . thermal cycling conditions were 95c for 10 minutes ( 1 cycle ) ; 94c for 30 seconds and 60c for 60 seconds ( 40 cycles ) ; 98c for 10 minutes ( 1 cycle ) , and a 12c hold . 
her2 copy number per cell was estimated as the ratio of the her2 and rna polymerase 30 ( rpp30 ) concentrations multiplied by two to account for the two copies of rpp30 that are expected per diploid genome . 
quadruplicate ddpcr wells were analyzed for each sample . results in the absence of additional treatment options , and given the patients good performance status , another liver biopsy was performed and nextgeneration sequencing was completed in a certified laboratory , which identified several tumor - specific somatic mutations , including apc r232 * , tp53 splice site 97_1g.a , and her2 amplification . the patients case and tumor genomics were then presented to a multi - institutional molecular tumor board for interpretation . the identification of a mutation in the adenomatous polyposis coli ( apc ) gene was expected and consistent with previous reports in which up to 85% of spontaneous colorectal cancers harbor somatic mutations in the classic tumor suppressor.16 a splice site mutation in the tp53 gene was equally unsurprising , given the relative frequency of tp53 mutations in human cancers.17 , 18 the molecular tumor board considered neither the apc nor tp53 mutations clinically actionable . treatment duration , months best outcome table 1 . 
cross - reference with the cancer genome atlas confirmed that approximately 4% to 5% of spontaneous colorectal cancers harbor high - level her2 amplifications , 19 and preclinical data predicted that anti - her2 therapy might be clinically effective , particularly when used in a combinatorial approach ( table 2 ) .20 , 21 gene alteration r232 * tp53 splice site 97_1g > a erbb2 amplification fig 1 . 
tumor - specific somatic alterations and quantification of the her2 copy number alteration . ( a ) next - generation sequencing identified three validated alterations in the patients hepatic metastatic colon cancer . 
 ( b ) using a droplet digital polymerase chain reaction assay , the total copies of her2 per genome in the patients metastatic tumor ( blue dot ) were measured and compared with the total copies of her2 in the patients germline ( peripheral blood , gold dot )  . 
error bars represent standard error of the mean . peripheral blood tumor to further characterize the her2 amplification and to validate the finding using an orthogonal method , a ddpcr assay was used . 
in contrast , a control gene , rpp30 , had the expected diploid copy number of two ( fig 1 )  . given the genomic findings and the patients clinical circumstances , treatment with trastuzumab was initiated . 
follow - up ct imaging , compared with baseline evaluation , revealed disease progression in the liver , with the largest lesion measuring 5.8 cm ( figs 2a and 2b )  . trastuzumab treatments were discontinued and the patient then received trastuzumab - emtansine ( t - dm1 ) infusions every 21 days for three total treatments . 
follow - up imaging revealed the largest hepatic metastasis measured 4.6 cm , compared with 5.3 cm at the initiation of t - dm1 ( fig 2c )  . three additional infusions at 21 - day intervals with subsequent imaging yielded ongoing disease response , with the largest hepatic mass measuring 3.2 cm ( fig 2d )  . 
the patient ultimately received t - dm1 infusions every 21 days for 15 months without any discernible negative clinical effect . the largest hepatic metastasis decreased to 2.1 cm ( fig 2e ) and two other metastases responded completely . 
the use of next - generation sequencing panels to identify actionable mutations and guide treatment has become increasingly scrutinized as a potentially viable approach for improving outcomes in a variety of cancer subtypes , including lung cancer and melanoma . 
these findings are bolstered by an interim analysis report from the mypathway study2 investigating the use of the combination of trastuzumab plus pertuzumab in various solid tumors , including mcrc . the case reported here suggests that genomicsbased analysis of refractory colorectal cancer can lead to effective targeted treatments . 
the expected progression - free survival and overall survival of a patient with mcrc with refractory disease is approximately 1.7 and 5 months , respectively , 25 in contrast to the 15 - month progression - free survival observed in this case . additional data and outcomes are required to confirm that precision oncology routinely yields superior outcomes ; however , this report illustrates an additional treatment option in patients with refractory disease who have exhausted all of the commonly used therapeutics for their respective disease and yet retain an acceptable performance status and desire additional treatmenta common clinical scenario . 
kamangar f , dores gm , anderson wf : patterns of cancer incidence , mortality , and prevalence across five continents : defining priorities to reduce cancer disparities in different geographic regions of the world . 
saltz lb , clarke s , daz - rubio e , et al : bevacizumab in combination with oxaliplatin - based chemotherapy as first - line therapy in metastatic colorectal cancer : a randomized phase iii study . 
douillard jy , siena s , cassidy j , et al : randomized , phase iii trial of panitumumab with infusional fluorouracil , leucovorin , and oxaliplatin ( folfox4 ) versus folfox4 alone as first - line treatment in patients with previously untreated metastatic colorectal cancer : the prime study . 
slamon dj , clark gm , wong sg , et al : human breast cancer : correlation of relapse and survival with amplification of the her - 2 / neu oncogene . 
sartore - bianchi a , trusolino l , martino c , et al : dual - targeted therapy with trastuzumab and lapatinib in treatmentrefractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - ofconcept , multicentre , open - label , phase 2 trial . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors based on molecular profiles : early results from mypathway , an open - label , phase iia umbrella basket study . 
richman sd , southward k , chambers p , et al : her2 overexpression and amplification as a potential therapeutic target in colorectal cancer : analysis of 3256 patients enrolled in the quasar , focus and piccolo colorectal cancer trials . 
sartore - bianchi a , ardini e , bosotti r , et al : sensitivity to entrectinib associated with a novel lmna - ntrk1 gene fusion in metastatic colorectal cancer . 
bertotti a , migliardi g , galimi f , et al : a molecularly annotated platform of patient - derived xenografts ( xenopatients ) identifies her2 as an effective therapeutic target in cetuximab - resistant colorectal cancer . 
parikh a , atreya c , korn wm , et al : prolonged response to her2 - directed therapy in a patient with her2amplified , rapidly progressive metastatic colorectal cancer . 
bensch f , van rooijen jm , schr oder cp , et al : a 21 - year - old patient with a her2 - positive colorectal cancer . discov 5 : 832 - 841 , 2015 gastroenterology 148 : 20 - 21 , 2015 cancer . 
grothey a , van cutsem e , sobrero a , et al : regorafenib monotherapy for previously treated metastatic colorectal cancer ( correct ) : an international , multicentre , randomised , placebo - controlled , phase 3 trial . 
 impact of variable rna - sequencing depth on gene expression signatures and target compound robustness : case study examining brain tumor ( glioma ) disease progression alexey stupnikov paul g . 
mcart , phd , msc , bioinformatics group , health sciences ( continued ) purpose gene expression profiling can uncover biologic mechanisms underlying disease and is important in drug development . 
the impact of sequencing depth alteration on rna - seqbased downstream analyses such as gene expression connectivity mapping is not known , where this method is used to identify potential therapeutic compounds for repurposing . methods in this study , published rna - seq profiles from patients with brain tumor ( glioma ) were assembled into two disease progression gene signature contrasts for astrocytoma . 
gene signatures were subsampled to simulate sequencing alterations and analyzed in connectivity mapping to investigate target compound robustness . results data loss to gene signatures led to the loss , gain , and consistent identification of significant connections . 
 building , centre for cancer research and cell biology , queens university belfast , 97 lisburn rd , belfast , bt9 7bl , united kingdom ; twitter : @drdmcart ; e - mail : d.mcart@qub.ac.uk. measurement is rna sequencing ( rna - seq ) of cdna transcripts in a high - throughput manner . 
rna - seq has wider analytical capabilities , including single nucleotide variants , insertion - deletions , gene splice variants , post - transcriptional modifications , and gene fusion detection , but remains costly.6 , 7 experimental techniques developed to minimize sequencing costs include sample multiplexing . 
 multiplexing involves labeling each sample library with a barcode identifier , allowing multiple libraries to be pooled and sequenced simultaneously , reducing costs.7 - 10 smaller volumes of rna are analyzed for multiplexed samples ; thus , the downside to multiplexing is reduced sequencing depth for this library type . accurate assessment of transcripts depends on length , abundance , and mappability to the reference and sufficient sequencing depth , particularly for genes with low transcript abundance.11 , 12 sequencing depth alterations can affect the detection of differentially expressed genes ( degs ) and potentially the accuracy of rna - seqbased downstream analysis . 
few studies have assessed the impact of sequencing depth alterations on rna - seq downstream applications.13 more studies are required , particularly to assess applications that rely on precise gene signatures , informative in classifying cancer subtypes and improved prognostic and predictive outcomes.14 , 15 a gene signature is summarized by degs that collectively represent the most prominent features of a cancer subtype or disease progression phenotype . 
this could be particularly problematic for connectivity mapping that examines a gene expression signature contrast with the aim of predicting potentially therapeutic us food and drugapproved target compounds for repurposing.16 there is urgent need for new targeted therapies for gliomas , which are the most common form of primary brain tumor . 
gliomas can be classified from grade i to iv on the basis of histologic and molecular information.17 depending on the cell of origin , each neoplasm is classified as an astrocytoma , oligodendroglioma , or ependymoma . 
herein , reference gene signatures were compiled from publically available sequenced tumors for astrocytoma disease progression.2 subsampling was applied to simulate sequencing depth alterations of gene signatures , and the performance of connectivity mapping was assessed . 
results reveal that information loss to gene signatures significantly affects target compound robustness . methods published whole transcriptome sequencing data of brain tumor biopsy specimens from adults ( accession : gse48865 ; bao et al2 ) was downloaded from the sequence read archive.25 on average , samples had 50 million reads each . 
reads were quality controlled using trimmomatic software26 and aligned using bowtie2 , 27 allowing one mismatch against the human genome version hg38.28 aligned reads were mapped to genes from the grch38.81 annotation29 using samexplorer software.30 , 31 to benchmark a diverse range in performance of the rna - seq analysis , mapped reads were subsampled to simulate samples with a range of lower cdna library sequencing depths using a bioinformatics pipeline32 ( appendix fig a1 ; data supplement )  . 
the impact of information loss to gene signatures for degs , gene ontology ( go ) terms , and target compound detection was assessed using differential expression , go , and gene expression connectivity mapping analysis , respectively , with deseq2 , goseq , and the qub accelerated drug and transcriptomic connectivity ( quadratic ) software33 - 35 ( data supplement )  . 
the reproducibility of significant connections to the library of integrated cellular signatures identified for all cell lines and neuronal specific cell lines ( data supplement ) by quadratic was investigated16 , 36 - 38 ( data supplement )  . 
results and associated false discovery rates ( fdrs ) were visualized using the r packages venndiagram and ggplot2.39 , 40 results assessment of the l - h and h - h gene expression signatures l - h ( dataset_i ) and h - h ( dataset_ii ) gene signature contrasts comprised 47 and 33 patients , respectively ( data supplement )  . 
 when data input was reduced , the fdr for the number of degs detected increased linearly and by approximately the same amount for both data sets ( appendix fig a2 )  . 
dataset_i gene signature therefore demonstrated better resilience to data loss for deg detection compared with dataset_ii . for the full data set ( f = 1.0 ) , > 200 go terms described the functions of the degs identified for dataset_i ( appendix fig a3a )  . 
given this low number , which reduced to zero on f = 0.5 , go results for subsampled dataset_ii are not depicted . impact of information loss to gene signatures used in gene expression connectivity mapping for the full data set , a greater number of significant reverse ( rev ) and progress ( prog ) connections were identified for dataset_i compared with dataset_ii ( fig 2a )  . 
effect of decreased cdna library sequencing depth on the number of differentially expressed genes ( degs ) detected from ( a ) dataset_i , and ( b ) dataset_ii gene signatures ( data supplement )  . 
visualization of the global stratification ability of ( c ) dataset_i , low to high ( l - h ) , and ( d ) dataset_ii , high to high ( h - h ) gene signatures . 
heatmap was generated using unsupervised hierarchical clustering with the full rna - seq data ( f = 1 ) and depicts the gene expressional patterns of the top 100 differentially expressed genes identified between the gene signature contrast groups . 
the who disease grades of samples as determined by bao et al2 are overlaid . target compound identification , dataset_i was therefore more resilient to alterations in cdna sequencing depth compared with dataset_ii . the impact of data loss to gene signatures and the reproducibility of connectivity mapping is presented in figures 3 - 5 . 
for example , 3 , 135 rev connections were identified for dataset_i using f = 1.0 ; this increased to approximately 5 , 000 when subsampled to f = 0.01 , but approximately 60% of compounds were infrequently detected ( figs 3b and 3c )  . 
for dataset_i , when 50% of reads were removed , approximately 62.5% rev ( approximately 2 , 500 of 4 , 000 ) and approximately 50% prog significant connections ( approximately 1 , 500 of 3 , 000 ) were identified with every iteration ( fig 3 )  . 
for dataset_ii , when 50% of reads were removed , just approximately 13% rev ( approximately 400 of 3 , 000 ) and 9% prog significant connections ( approximately 180 of 2 , 000 ) were identified with every iteration ( fig 4 )  . 
 significant connections that potentially could progress ( prog ) or reverse ( rev ) the disease phenotype and fdrs are plotted against the data fraction included in the analysis ( f )  . 
when affected by data loss , connectivity mapping results were more robust for dataset_i compared with the dataset_ii gene signature . reducing data to the gene signature led to the loss , gain , and consistent identification of significant connections to target compounds ( fig 5 )  . 
for dataset_i , a large proportion of the significant connections across all cell lines ( 69% ; 2 , 195 of 3 , 135 ) and neuronal - specific cell lines ( 70% ; 144 of 205 ) were detected with all data fractions . 
similarly for dataset_ii , a proportion of the significant connections across all cell lines ( 7% ; 100 of 1 , 339 ) and neuronal specific cell lines ( 5% ; nine of 172 ) were detected with all data fractions . 
for example , 350 and 105 compounds were detected across all cell lines for dataset_i , f = 0.01 , that were not identified by the full data set ( fig 5a )  . 
when 50% of the reads were removed , nine and 27 target compounds identified for neuronal specific cell lines were lost , respectively , for dataset_i and ii ( figs 5c and 5d ; table 1 )  . 
thus , for dataset_ii , more target compounds identified by the full gene signature were lost , and some of these included compounds of potential clinical utility for glioma , such as suramin and dasatinib ( table 1 )  . 
a comparison of the rate of impact of data loss on go terms and significant connections detection for dataset_i can be seen by comparing figures a3 and 2a . discussion understanding molecular pathways and regulatory networks driving cancer is essential for the development of new therapies . 
gene expression profiling using rna - seq has led to the development of clinically relevant gene signatures that are informative for cancer subtypes.14 , 15 rnaseq experimental approaches such as sample multiplexing reduce cdna sequencing depth and potentially affect gene signature accuracy . 
significant connections to target compounds identified from the neuronal derived cell lines using ( c ) dataset_i and ( d ) dataset_ii across gene signatures are also compared . more patient gene expression profiles matched their who grade classifications . 
results support the subjective nature of tumor classification , which has interobserver variability.41 gene signatures provided a framework to assess connectivity mapping output for a well - performing accurate versus a poorer - performing less accurate contrast . characterization of the disease progression gene signatures revealed they differed in biologic complexity . 
thus , the l - h gene signature was more resilient to data loss for deg detection and had greater test sensitivity compared with the h - h gene signature . 
overall , the number of significant connections detected for the l - h gene signature was greater , most likely explained by the heterogeneous biologic mechanisms involved in lowto high - grade astrocytoma transition . 
with data loss , this fdr threshold was reached by the l - h and h - h gene signatures , respectively , when 70% and just 1% of reads were removed . 
thus , the l - h gene signature was more resilient to data loss for the detection of significant connections to target compounds using connectivity mapping . subsampling of gene signatures for connectivity mapping revealed that the suite of significant connections to target compounds became modified with data loss . 
compounds lost by the h - h gene signature ( who grade iii to iv ) included suramin , lopinavir , dasatinib , and vincristine , which have already been considered as glioma treatments . 
suramin , an anticancer agent , inhibits the binding of growth factors understood to play a role in glioma progression , angiogenesis , and radioresistance and has been used to treat newly diagnosed gbms.42 , 43 lopinavir , a protease inhibitor , has reached phase ii clinical trials for the treatment of high - grade glioma.44 dasatinib , a kinase inhibitor that acts on members of the src family of kinases , is well studied in glioma and has shown preclinical promise.45 vincristine , a spindle poison , is used in combination with procarbazine and lomustine to treat high - grade glioma and has also been successful in a phase iii trial for the treatment of low - grade gliomas.22 , 46 , 47 reductions in transcript abundance probably led to the loss of low - abundance genes from the full gene signature and altered the degs detected , leading to the loss of these connectivity mapping connections . 
fewer significant connections identified by the full data sets were lost by the l - h gene signature compared with the h - h gene signature , suggesting it was more resilient to data loss . 
similarly , in another subsampling rna - seq study of healthy organisms from multiple taxa , highly expressed genes regulating metabolism and pathogenesis of disease were consistently identified even when downsampling rna - seq reads to only 1 million reads , 13 thereby corroborating our findings from diseased tumors . results highlight the need for determining the optimal cdna sequencing depth for accurately identifying degs when compiling gene signatures . 
in the future , rna standard and spike - in controls may be useful to inform rna - seq best practices.48 the accuracy of a gene signature was particularly important when carrying out additional downstream analyses , such as connectivity mapping . 
given the instability of gene expression , perhaps using ontology types or ontotypes49 to characterize contrast phenotypes may be a more reliable approach compared with gene lists in connectivity mapping . 
other target compounds sensitive to data loss are being tested for their biologic efficacy against glioma stem cells using clonogenic cell survival assays and western blot analyses in ongoing studies by this research group . 
roddy no relationship to disclose manuel salto - tellez consulting or advisory role : philips healthcare , visiopharm , bristol - myers squibb , merck patents , royalties , other intellectual property : co - inventor of qupath ( open - source system for digital pathology analysis ) darragh g . 
mcart , queens university belfast ; tom flannery , estelle healy , and manuel salto - tellez , belfast health and social care trust , belfast , united kingdom ; alexey stupnikov , johns hopkins university , baltimore , md ; hayley p . 
 kurian , brain tumour research centre , university of bristol , bristol , united kingdom ; and frank emmert - streib , tampere university of technology , tampere , finland . supported by funding from the brainwaves northern ireland charity ( registered charity number : nic103464 )  . 
bao zs , chen hm , yang my , et al : rna - seq of 272 gliomas revealed a novel , recurrent ptprz1 - met fusion transcript in secondary glioblastomas . 
verhaak rg , hoadley ka , purdom e , et al : integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
wang l , si y , dedow lk , et al : a low - cost library construction protocol and data analysis pipeline for illumina - based strand - specific multiplex rna - seq . 
liu y , zhou j , white kp : rna - seq differential expression studies : more sequence or more replication ? bioinformatics 30 : 301 - 304 , 2014 13 . 
turkington rc , hill la , mcmanus d , et al : association of a dna damage response deficiency ( ddrd ) assay and prognosis in early - stage esophageal adenocarcinoma . 
lamb j , crawford ed , peck d , et al : the connectivity map : using gene - expression signatures to connect small molecules , genes , and disease . 
okamoto y , di patre pl , burkhard c , et al : population - based study on incidence , survival rates , and genetic alterations of low - grade diffuse astrocytomas and oligodendrogliomas . 
ziu m , kalkanis sn , gilbert m , et al : the role of initial chemotherapy for the treatment of adults with diffuse low grade glioma : a systematic review and evidence - based clinical practice guideline . 
stupp r , hegi me , mason wp , et al : effects of radiotherapy with concomitant and adjuvant temozolomide versus radiotherapy alone on survival in glioblastoma in a randomised phase iii study : 5 - year analysis of the eortc - ncic trial . 
takano s , gately s , engelhard h , et al : suramin inhibits glioma cell proliferation in vitro and in the braj neurooncol 21 : 189 - 201 , 1994 44 . 
yu mk , kramer m , dutkowski j , et al : translation of genotype to phenotype by a hierarchy of nat rev genet 18 : 473 - 484 , 2017 cell subsystems . 
effect of decreased cdna library sequencing depth on the number of gene ontology ( go ) terms identified for ( a ) dataset_i and ( b ) the false discovery rate ( fdr ) for the number of go terms identified . 
 combined targeted therapy for braf - mutant , treatment - related acute myeloid leukemia a 44 - year - old woman with a prior history of myxoid liposarcoma who was previously treated with radiation , chemotherapy , and resection , was admitted with syncope and pancytopenia . she was diagnosed with a high - grade therapy - related myelodysplastic syndrome and treated with decitabine . 
she was treated with cytotoxic chemotherapy including cytarabine and topotecan , but she was not a candidate for further anthracycline exposure given her prior treatment for sarcoma and concern for cardiotoxicity . 
her aml was refractory to two sequential induction regimens . given that targeted genomic sequencing had revealed a braf v600e mutation with a high allelic fraction , she was then placed on combined targeted braf / mek therapy with dabrafenib and trametinib for her refractory disease . 
this resulted in a dramatic response with clearance of circulating myeloblasts , restoration of normal hematopoiesis , a significant decrease in marrow leukemic burden , and a concordant decrease in the braf v600e allelic burden . 
it emerges spontaneously or from antecedent myeloid neoplasms , such as myelodysplastic syndromes ( mdss ) .1 mds and aml can be related to prior chemotherapy or radiotherapy , in which case they have a worse prognosis . 
substantial molecular heterogeneity underlies myeloid malignancies , 2 - 5 and the presence of certain mutations has an impact on prognosis and response to treatment.6 for aml , npm1 , cebpa , and flt3 mutations are incorporated into clinical practice as important prognostic characteristics . such alterations reflect only a subset of the genomic heterogeneity underlying aml , and additional mutational abnormalities may soon influence treatment selection and prognostication.7 across malignancies , focus has shifted toward a genomics - driven framework promoting therapies that target specific molecular alterations . 
this personalized approach contrasts with traditional treatment with indiscriminately cytotoxic agents.8 therapies targeting the braf pathway are pervasive in melanoma , in which activating mutations are common.9 most alterations involve a substitution of glutamic acid for valine at position 600 ( v600e ) within the activation loop , causing constitutive activation and signaling through the mek / erk pathway . 
in metastatic melanoma , combinatorial regimens targeting braf and mek have demonstrated superiority to braf inhibitors alone in the phase iii setting and are approved by the us food and drug administration.10 braf mutations have also been noted in colorectal and nonsmall - cell lung cancers , gastric carcinomas , 11 and in virtually all patients with hairy cell leukemia in whom therapeutic responses are noted with braf inhibition.12 - 14 braf mutations are much less common in myeloid malignancies . 
in a study of more than 1 , 500 patients with aml , braf mutations were rare ( nine individuals [ , 1% ] ) , but their presence was associated with worse prognosis.15 in another series of 140 patients with therapy - related myeloid neoplasms , three braf mutations were po.ascopubs.org po precision oncology seth a . 
she had received neoadjuvant chemotherapy and radiation therapy 20 months earlier as treatment for sarcoma , including three cycles of doxorubicin , ifosfamide , and mesna ( aim )  . 
resection was followed by three additional cycles of aim . one year later , after presenting with the aforementioned symptoms , laboratories revealed pancytopenia , with white blood cell count ( wbc ) of 1 , 620 / ml , neutrophil count of 370 / ml , hemoglobin of 4.9 g / dl , and platelet count of 21 , 000 / ml . 
two weeks later , another marrow sample revealed persistent disease , with myeloblast involvement above 80% . her disease thereafter progressed , with wbc and circulating blast percentage reaching peaks of 9 , 530 / ml and 69% , respectively . 
although no pathogenic genomic variants were reported at initial diagnosis of therapy - related mds , a braf v600e mutation was identified ( at an allelic fraction of approximately 43% ; fig 1 ) upon leukemic progression . 
 therapy - related mds sample revealed that this braf variant had indeed been present , but at a variant allelic frequency ( vaf ) below detection threshold ( four reads , , 2% vaf ; fig 1 ; table 1 )  . no additional pathogenic mutations were present according to our institutions sequencing platform . because of rapid and refractory aml progression and the unique genomic data noted above , she was initiated on combined targeted braf / mek inhibition . 
she received dabrafenib ( 150 mg twice per day ) and trametinib ( 2 mg once per day ) , per established regimens for braf - mutant melanoma.17 two weeks later , her wbc had decreased to 500 / ml , and circulating blasts had disappeared . 
retrospective identification of a small population of braf - mutant cells in the original mds sample likely reflects the presence of an early subclone that expanded under the selective pressure of conventional treatment . because of limited therapeutic options and a wealth of clinical experience with braf / mek blockade in melanoma , she was treated with dabrafenib and trametinib . 
a dramatic clinical response was noted , with clearance of circulating myeloblasts , restoration of hematopoiesis , decrease in marrow leukemic burden , and a concordant decrease in the braf v600e vaf . 
of note , the braf v600e vaf rose at the time of progression because the acquisition of novel kras subclones ( all of which also harbored the original braf v600e mutation ) drove resistance and outgrowth . mechanisms governing resistance to braf / mek inhibition have been well characterized in cell culture models , xenografts , and patients.18 primary resistance to braf blockade in colorectal and papillary thyroid cancers has been attributed to loss of erk - dependent negative feedback on other oncogenic signaling pathways , table 1 . 
 ( c ) hematoxylin and eosin staining on continued braf / mek - directed therapy demonstrating hypocellular marrow with regenerating erythroid elements and several blasts . ( d ) terminal deoxynucleotidyl transferase dutp nick - end labeling staining of ( top ) pretreatment bone marrow sample showing no staining of the leukemic blasts and ( bottom ) first posttreatment bone marrow sample showing scattered positive apoptotic cells . including those involving egfr and her2 / 3 receptor tyrosine kinases.19 - 21 acquired resistance to braf blockade , also described in translational studies , does not seem to be the result of gatekeeper mutations in the braf kinase , as seen with other kinase inhibitors.22 instead , bypass mechanisms activate the map kinase pathway through mutations that activate key enzymes , such as nras , mek1 , or mek2.23 - 25 upregulation of pi3k / akt or her2 pathways have also been implicated as mechanisms of acquired resistance , 26 , 27 as have amplification of braf v600e , novel mek2 variants , and activating nras mutations via study of therapy - resistant tissue samples.28 - 30 in the presented case , four kras mutations were identified at disease progression . 
resistance to vemurafenib exposure co - occurred with spontaneous acquisition of a kras g12d activating mutation in papillary thyroid carcinoma cells in vitro.31 in recent clinical studies of vemurafenib in hairy cell leukemia , a patient with resistant disease acquired two subclonal kras mutations ( g12d and k117n ) .32 there have also been reports of rasdependent tumor outgrowth after treatment with braf inhibitors . 
additional work will be necessary to validate this assumption in cellular models . braf mutations are rare in mds and aml . nevertheless , it is intriguing that all braf - mutant cases among the previously published cohort of patients with therapy - related disease , like our case , harbored a concurrent t ( 9 ; 11 ) ( p22 ; q23 ) mll rearrangement.16 in a large cohort of patients with mll - rearranged aml , ras signaling alterations were identified in 50% of patients ( 59 of 118 ) , three of whom harbored braf mutations.35 the presence of a braf or ras mutation may interact with the mll - rearranged protein to drive leukemic genesis and evolution in this population and could contribute to decreased therapeutic responsiveness and poor prognosis . 
such a potential interaction requires further study . therapy in mds or aml leading to an impressive antileukemic response , as well as the first description of convergent kras mutations in aml at the time of therapeutic resistance . although braf and mek inhibitors hold tremendous promise in various malignancies , divergent mechanisms of resistance have been described , many of which rely upon constitutive activation of ras kinases and related pathways . 
hasserjian stock and other ownership interests : cerner , gilead pharmaceuticals , halyard health , healthcare services group , johnson & johnson , medtronic , novo nordisk , perrigo consulting or advisory role : amgen , celgene , promedior kwadwo oduro no relationship to disclose krzysztof glomski no relationship to disclose valentina nardi no relationship to disclose gregory m . 
cote research funding : pharmamar ( inst ) , epizyme ( inst ) , boston biomedical ( inst ) , agios pharmaceuticals ( inst ) , macrogenics ( inst ) timothy a . 
graubert stock and other ownership interests : biogen idec ( i ) , vertex ( i ) , bristol - myers squibb , express scripts consulting or advisory role : biogen idec ( i ) , novartis ( i ) , agios pharmaceuticals , juno therapeutics andrew m . 
chen consulting or advisory role : insys therapeutics , incyte , takeda pharmaceuticals , regimmune , seattle genetics research funding : seattle genetics , novartis , bayer healthcare pharmaceuticals , celgene amir t . 
mardis er , ding l , dooling dj , et al : recurring mutations found by sequencing an acute myeloid leukemia genome . n engl j med 361 : 1058 - 1066 , 2009 3 . 
papaemmanuil e , gerstung m , bullinger l , et al : genomic classification and prognosis in acute myeloid leukemia . 2847 - 2855 , 2016 n engl j med 374 : 2209 - 2221 , 2016 16 . 
christiansen dh , andersen mk , desta f , et al : mutations of genes in the receptor tyrosine kinase ( rtk ) / ras - braf signal transduction pathway in therapy - related myelodysplasia and acute myeloid leukemia . 
long gv , weber js , infante jr , et al : overall survival and durable responses in patients with braf v600 - mutant metastatic melanoma receiving dabrafenib combined with trametinib . 
corcoran rb , ebi h , turke ab , et al : egfr - mediated re - activation of mapk signaling contributes to insensitivity of braf mutant colorectal cancers to raf inhibition with vemurafenib . 
montero - conde c , ruiz - llorente s , dominguez jm , et al : relief of feedback inhibition of her3 transcription by raf and mek inhibitors attenuates their antitumor effects in braf - mutant thyroid carcinomas . 
nazarian r , shi h , wang q , et al : melanomas acquire resistance to b - raf ( v600e ) inhibition by rtk or n - ras x274 - x279 , 2006 upregulation . 
emery cm , vijayendran kg , zipser mc , et al : mek1 mutations confer resistance to mek and b - raf inhibition . proc natl acad sci usa 106 : 20411 - 20416 , 2009 25 . 
villanueva j , vultur a , lee jt , et al : acquired resistance to braf inhibitors mediated by a raf kinase switch in melanoma can be overcome by cotargeting mek and igf - 1r / pi3k . 
wagle n , van allen em , treacy dj , et al : map kinase pathway alterations in braf - mutant melanoma patients with acquired resistance to combined raf / mek inhibition . 
long gv , fung c , menzies am , et al : increased mapk reactivation in early resistance to dabrafenib / trametinib combination therapy of braf - mutant metastatic melanoma . 
danysh bp , rieger ey , sinha dk , et al : long - term vemurafenib treatment drives inhibitor resistance through a spontaneous kras g12d mutation in a braf v600e papillary thyroid carcinoma model . 
andrews mc , behren a , chionh f , et al : braf inhibitor - driven tumor proliferation in a kras - mutated colon carcinoma is not overcome by mek1 / 2 inhibition . 
callahan mk , rampal r , harding jj , et al : progression of ras - mutant leukemia during raf inhibitor treatment . n engl j med 367 : 2316 - 2321 , 2012 35 . 
staining was performed by using an anti - braf v600e mouse monoclonal antibody ( clone ve1 , ventana medical systems , tucson , az , catalog #790 - 4855 )  . 
terminal deoxynucleotidyl transferasemediated dutp nick - end labeling detection was completed manually by using millipore apoptag in situ detection kit ( emd millipore , darmstadt , germany , s7100 ) and visualized with diaminobenzidine substrate ( dako agilent pathology solutions , santa clara , ca , k4000 )  . this next - generation sequencing assay ( snapshot ) , using a multiplex polymerase chain reaction technology called anchored multiplex pcr ( amp ; zheng z , et al : nat med 20 : 1479 - 1484 , 2014 ) for single nucleotide variant ( snv ) and insertion / deletion ( indel ) detection , was used . 
briefly , genomic dna was isolated from blood or marrow aspirate . genomic dna was sheared with the covaris m220 instrument , followed by end - repair , adenylation , and ligation with an adapter . 
illumina misequation 2 3 147 base - paired end - sequencing results were aligned to the hg19 human genome reference using bwa - mem ( li h and durbin r : bioinformatics 25 : 1754 - 1760 , 2009 )  . 
mutect ( cibulskis k , et al : nat biotechnol 31 : 213 - 219 , 2013 ) and a laboratory - developed indel analysis algorithm were used for snv and indel variant detection , respectively . 
 acquired alk and ret gene fusions as mechanisms of resistance to osimertinib in egfr - mutant lung cancers introduction approximately 20% of patients with metastatic lung adenocarcinoma have somatic activating mutations in the epidermal growth factor receptor ( egfr ) gene , egfr . 
1 patients with egfr - mutant lung adenocarcinomas have a 70% response rate to first - line egfrtyrosine kinase inhibitor ( tki ) therapy ( ie , erlotinib , gefitinib , or afatinib ) .2 egfr t790m is the dominant resistance mechanism to earlier - generation egfr - tkis.3 osimertinib is approved by the us food and drug administration for the treatment of egfr - mutant lung cancers that have an acquired egfr t790m after failure of a previous egfr - tki4 and now is approved in the first - line setting as well.5 response to osimertinib eventually is followed by progression with known resistance mechanisms , including small - cell transformation3 , 6 ; acquired egfr mutations , including g796 / c797 , l792 and l718 / g7197 ; and non - egfr mediated resistance , including alterations / amplification in met , her2 , braf , mek , kras , and pik3ca . 
ngs with archerdx and msk - impact confirmed an acquired eml4 - alk fusion ( eml4 exons 1 through 6 fused with alk exons 20 through 29 ; c.667 + 516 : eml4_c.3173 - 415 : alkinv ) in addition to the egfr exon19del and t790m mutations . 
the patient started combination treatment with osimertinib 80 mg daily and crizotinib 200 mg twice daily , remained on treatment with stable disease ( by recist version 1.1 ) , and continued to receive clinical benefit from treatment , with no report of toxicity . 
the preosimertinib biopsy was a fine - needle aspiration ( fna ) and was partially fragmented on staining , whereas the acquired resistance ( ar ) sample was a core - needle biopsy . 
the pretreatment egfr exon19del staining was performed with epidermal growth factor receptor ( egfr ) e746 ; the post - treatment ihc stained more diffusely for egfr exon19del , likely related to the egfr amplification ( fold change : 3.0 ) noted on next - generation sequencing with msk - impact . 
 the ihc data suggest the presence of the alk rearrangement and egfr mutation within the same cell ( however , this cannot be confirmed by targeted next - generation sequencing because of technical limitations )  . 
 case 2 a 68 - year - old woman , who was never a smoker , presented with a 9 - cm right apical lung mass , right hilar lymphadenopathy , and a left temporal lobe mass ( staging t4n1m1b )  . 
 ( of note , no alk rearrangement was detected on ngs or fish . ) the patient started treatment with osimertinib and had an initial disease response , but oligoprogression occurred in the lung after 6 months . 
 ( a ) osimertinib and crizotinib in patient case 1 after one cycle ( 28 days ) of treatment ; image shows overall stable disease ( 0% best response )  . 
 ( b ) osimertinib and alectinib in patient case 2 after one cycle ( 28 days ) of treatment ; image shows regression of the dominant right upper lobe mass ( 25% reduction )  . precombination targeted therapy postcombination targeted therapy precombination targeted therapy postcombination targeted therapy l858r and t790m mutations as well as the new eml4 - alk rearrangement ( eml4 exons 1 through 2 fused to alk exons 20 through 29 ; c.208 + 4890 : eml4_c.3173 - 373 : alkinv ; fig 3b ; appendix table a2 )  . 
the patient started treatment with alectinib 300 mg twice daily and osimertinib 80 mg daily ; the first interval scan showed a decrease in the dominant right lung mass ( 25% reduction by recist version 1.1 ) as well as ongoing clinical benefit and no report of toxicity at the last follow - up . 
a right lung biopsy showed the known egfr l747s and l858r mutations as well as a new ncoa4 - ret fusion on msk - impact ; the fusion was confirmed by archerdx . 
 ( * ) treatment ongoing as of april 1 , 2018 . which showed that the fusion partner did not influence ret activity in cell lines.19 , 20 each condition was assayed in triplicate in at least two independent experiments . 
the pc9 cells were used to assess the effect of ret fusions on sensitivity of growth and apoptosis ( caspase 3 / 7 activity ) in the presence of osimertinib and cabozantinib . 
however , erk1 / 2 phosphorylation was not sensitive to osimertinib treatment in pc9 - pcx4.1ccdc6 - ret cells but was diminished with cabozantinib treatment ( fig 4b )  . 
these results suggest that ret rearrangements can cause bypass activation of growth - promoting pathways in cells that express oncogenic egfr . growth of pc9 cells that stably expressed ccdc6 - ret or kif5b - ret rearrangements was at least 10 - fold less sensitive to osimertinib than pc9 - pcx4.1empty cells were ( 50% inhibitory concentrations described in fig 4e )  . 
expression of ret fusions in pc9 cells prevented osimertinib - induced activation of caspase 3 / 7 , similar to the effect on growth rate ( fig 4f [ left panel ] )  . 
treatment of control - group pc9 cells or pc9 - ret cells with cabozantinib did not lead to activation of caspase 3 / 7 ( fig 4f [ left panel ] )  . 
these results suggest that ret rearrangements can induce resistance to osimertinib in cells that have egfr mutations and that response to osimertinib is restored when it is used in combination with cabozantinib . in conclusion , osimertinib is now a first - line treatment for metastatic egfr - mutant lung cancers.5 although potential resistance mechanisms to osimertinib have been identified , these have primarily been observed after later - line osimertinib in the setting of egfr t790m mutations and have focused on ctdna.9 - 11 many alterations identified as potential resistance mechanisms are seen concurrently with egfr in pretreatment samples , including amplifications of met and her2 as well as pik3ca mutations , which makes the comparison with pretreatment tissue critical to identify truly acquired alterations.13 as ngs becomes standard of care , it is feasible and fruitful to molecularly profile tumors broadly before treatment and at progression to identify acquired alterations that mediate resistance . it remains unclear whether mechanisms of resistance to first - line osimertinib will differ from mechanisms of resistance to later - line osimertinib or earlier - generation egfr - tkis . 
osimertinib is a potent mutant - egfr inhibitor that inhibits egfr t790m , so there is a potential to see novel on - target21 , 22 and off - target23 - 25 resistance mechanisms . 
this is corroborated by the low frequency ( 15% to 25% ) of egfr c797s and other acquired egfr alterations after osimertinib use compared with 60% frequency of acquired egfr t790m after use of earlier generation egfr - tkis.9 , 13 , 22 we may see new acquired alterations not previously seen or seen rarely with earlier - generation egfr - tkis . 
 moreover , although cabozantinib can inhibit growth of egfrand ret - mutant / rearranged cell lines , a combination of osimertinib and cabozantinib induced apoptosis . at our institution , among 174 patients with egfr - mutant lung cancer in whom ngs was performed on tumor tissue after progression developed during treatment with erlotinib or afatinib , we found no alk or ret fusions . 
it is unknown whether this potential enrichment of acquired fusions is related to the more potent egfr inhibition of osimertinib or to the later - line setting after multiple lines of egfr inhibition . 
pc9 cells were infected with lentivirus that harbored an empty plasmid ( pcx4.1 - empty ) or pcx4.1 with either ccdc6 - ret or kif5b - ret complementary dna ( cdna ) , and cells that expressed the plasmids were selected to generate stable cell lines . 
 ( a ) cell extracts were immunoblotted ( indicated by ib ) for ( left panel ) total ret ( left panel ) or ( right panel ) phosphorylated ret . 
 ( b ) cell lines were treated with either osimertinib 0.05 m or cabozantinib or 0.25 m for 1 h ; cell extracts were prepared and then immunoblotted for the indicated proteins . 
 ( c ) cells were treated with increasing concentrations ( as indicated on the figure ) of ( left panel ) osimertinib or ( right panel ) cabozantinib for 96 h , and then growth was determined . 
 ( f ) cells were treated with the indicated concentrations of ( left panel ) osimertinib or ( right panel ) cabozantinib for 48 hours , and then caspase 3 / 7 enzymatic activity determined . 
 ( g ) pc9 cells that expressed either pcx4.1 - empty vector or pcx4.1ccdc6 - ret were treated with the indicated concentrations of cabozantinib in the presence of osimertinib 0.1 m for 48 h , and then caspase 3 / 7 enzymatic activity was determined . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . michael offin no relationship to disclose romel somwar research funding : helsinn healthcare travel , accommodations , expenses : helsinn healthcare natasha rekhtman no relationship to disclose ryma benayed no relationship to disclose jason c . 
li consulting or advisory role : roche , biosceptre international , thermofisher scientific , mersana , guardant health research funding : roche ( inst ) , genentech ( inst ) , illumina ( inst ) , biomed valley discoveries ( inst ) , astrazeneca ( inst ) , grail ( inst ) gregory j . 
riely research funding : novartis ( inst ) , roche ( inst ) , genentech ( inst ) , millenium ( inst ) , glaxosmithkline ( inst ) , pfizer ( inst ) , infinity pharmaceuticals ( inst ) , ariad ( inst ) patents , royalties , other intellectual property : patent application submitted covering pulsatile use of erlotinib to treat or prevent brain metastases ( inst ) travel , accommodations , expenses : merck sharp & dohme charles m . 
kris consulting or advisory role : astrazeneca , regeneron william travis speakers ' bureau : genentech alexander drilon consulting or advisory role : ignyta , loxo , tp therapeutics , astrazeneca , pfizer , blueprint medicines , genentech , roche , takeda , helsinn therapeutics , beigene maria e . 
arcila consulting or advisory role : astrazeneca travel , accommodations , expenses : astrazeneca , invivoscribe , raindance technologies marc ladanyi honoraria : merck ( i ) consulting or advisory role : national comprehensive cancer network , boehringer ingelheim , astrazeneca ( tagrisso rfp advisory committee ) research funding : loxo ( inst ) helena a . 
jui , the chinese university of hong kong , sha tin new town , hong kong special administrative region , china . supported in part by the national cancer institute of the national institutes of health grants no . 
jnne pa , wang xf , socinski j , et al : randomized phase ii trial of erlotinib ( e ) alone or in combination with carboplatin / paclitaxel ( cp ) in never or light former smokers with advanced lung adnocarcinoma : calgb 30604 trial . 
yang z , yang n , ou q , et al : investigating novel resistance mechanisms to third - generation egfr tyrosine kinase inhibitor osimertinib in nonsmall - cell lung cancer patients . 
yang jc , ahn mj , kim dw , et al : osimertinib in pretreated t790m - positive advanced non small - cell lung cancer : aura study phase ii extension component . 
yu ha , suzawa k , jordan e , et al : concurrent alterations in egfr - mutant lung cancers associated with resistance to egfr kinase inhibitors and characterization of mtor as a mediator of resistance . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
jackman d , pao w , riely gj , et al : clinical definition of acquired resistance to epidermal growth factor receptor tyrosine kinase inhibitors in nonsmall - cell lung cancer . 
national cancer institute : osimertinib and necitumumab in treating patients with egfr - mutant stage iv or recurrent nonsmall - cell lung cancer who have progressed on a previous egfr tyrosine kinase inhibitor ( nct02496663 )  . 
okamoto k , kodama k , takase k , et al : antitumor activities of the targeted multi - tyrosine kinase inhibitor lenvatinib ( e7080 ) against ret gene fusiondriven tumor models . 
arai s , kita k , tanimoto a , et al : in vitro and in vivo anti - tumor activity of alectinib in tumor cells with ncoa4 - ret . 
klempner sj , mehta p , schrock ab , et al : cis - oriented solvent - front egfr g796s mutation in tissue and ctdna in a patient progressing on osimertinib : a case report and review of the literature . 
ou si , horn l , cruz m , et al : emergence of fgfr3 - tacc3 fusions as a potential bypass resistance mechanism to egfr tyrosine kinase inhibitors in egfr - mutated nsclc patients . 
detailed molecular and immunohistochemical characterization of patient case 1 presented timing of molecular test diagnosis type of molecular test result tissue pcra impactb 15base pair egfr exon 19 deletion detected egfr exon19 p.e746_a750del ; tp53 exon10 p.r337l ; atr exon41 p.d2331y detected erlotinib progression cfdnac egfr t790m detected ( 0.79% ) d tissue pcrc egfr t790m detected ( 15.15% ) d alk : negative ; egfr exon 19 deletion : positive osimertinib + necitumumab ihce alk : positive ; egfr exon 19 deletion : positive progression impactb ihce impactb archerdxf fishg egfr exon19 p.e746_a750del ; egfr exon20 p.t790m ; kmt2c exon38 p.d2690n ; rad51b exon7 p.l209v detected no alk fusion detected no evidence of alk rearrangement . 
the single base extension product is detected by tandem mass - spectrometry on a sequenom massarray spectrometer ( sequenom , san diego , ca )  . bmsk - impact ( integrated mutation profiling of actionable cancer targets ) was used to identify specific mutations in 468 genes . cdigital pcr of cfdna and / or tissue amplification of part of egfr exon 20 in the presence of fluorescent probes specific to the wild - type and mutant alleles . dratio of mutant allele / ( mutant + wild - type allele )  . eimmunohistochemistry ( ihc ) for pertinent proteins performed with the following clones : egfr - exon19del ( egfr - e746 ) : clone 6b6 ; alk : clone d5f3 . farcher fusionplex custom solid panel ( archer fusionplex , boulder , co ) uses the anchored multiplex pcr used to detect gene fusions in tumor samples consisting of 62 cancer - related genes previously reported to be involved in chromosomal rearrangements . 
the single base extension product is detected by tandem mass - spectrometry on a sequenom massarray spectrometer . carcher fusionplex custom solid panel uses the anchored multiplex pcr used to detect gene fusions in tumor samples consisting of 62 cancer - related genes previously reported to be involved in chromosomal rearrangements . 
 mithat g onen lipika goyal stacy gray patrick grohar william grubb joshua gruber michael hall balazs halmos heather hampel sigurdis haraldsdottir derrick haslem aaron hata robert hayashi matthew hellmann andrew hendifar brian henick daniel hertz j . 
kevin hicks cinta hierro masahiro hiratsuka kim hirshfield eran hodis david hong david hsu eric huang hatim husain david hyman david ilson steven isakoff haruka itakura gopa iyer katherine janeway fabrice jardin russell jenkins lingyun ji chris jones goran jonsson mark kelley jonathan killian won kim hyunjae kim kevin kim randall kimple eric klein samuel klempner todd knepper andrew ko rachel koff wendy kohlmann tomonobu koizumi jill kolesar carl koschmann vessela kristensen rajiv kumar shaji kumar shivaani kummar pamela kunz allison kurian kwong kwok wong norman lacayo joseph lasky ulrik lassen josh lauring christophe le tourneau sarah leary adrian lee j . 
jack lee jochen lennerz mark lewis jessica lin carol liu charles lopez patricia lorusso christine lovly ying lu cynthia ma anant madabhushi subha madhavan michael maitland xavier maldonado david malka diana mandelker aaron mansfield richard marais laetitia marisa renato martins daniela matei joaquin mateo jes sloth mathiesen ignacio matos caroline mccoach rohit mehra diana miao james miser irvin modlin todd morgan alessandro morotti jean mulcahy levy peter m uller arno mundt katherine nathanson j.t. 
raymond , ms3 ; eduardo vilar , md , phd1 ; michael overman , md1 ; bryan kee , md1 ; cathy eng , md1 ; kanwal raghav , md1 ; and scott kopetz , md , phd1 purpose atypical , non - v600 braf ( abraf ) mutations represent a rare molecular subtype of metastatic colorectal cancer ( mcrc )  . 
preclinical data are used to categorize abraf mutations into class ii ( intermediate to high levels of kinase activity , ras independent ) and iii ( low kinase activity level , ras dependent )  . 
among patients with abraf ras wild - type mcrc who received anti - egfr antibodies ( monotherapy , n = 1 ; combination therapy , n = 10 ) , no responses to anti - egfr therapy were reported , and six patients ( four with class iii abraf mutations , one with class ii , and one unclassied ) achieved stable disease as best response . 
in the ctdna cohort , there was an increased prevalence of abraf mutations and subclonal abraf mutations ( p , .001 for both ) among predicted anti - egfr exposed compared with nonexposed patients . conclusion efcacy of anti - egfr therapy is limited in class ii and iii abraf mcrc . 
2019 by american society of clinical oncology introduction brafv600e missense mutations are present in 6% to 10% of patients with metastatic colorectal cancer ( mcrc ) .1 , 2 within the braf kinase domain , substitution of a valine to glutamic acid at position 600 manifests as constitutive activation and oncogenic signaling along the mitogenactivated protein kinase ( mapk ) pathway.1 brafv600e mcrc represents an aggressive molecular subtype of colorectal cancer inherently refractory to standard chemotherapy ; thus , tremendous research focus has been directed toward novel therapeutic development.2 because of increased use of next - generation sequencing ( ngs ) in the management of mcrc , various mutational hotspots of clinical signicance have emerged within interest , such as expanded ras testing . genes of however , with such broad testing including circulating tumor dna ( ctdna ) , alterations of evolving signicance without clear predictive , prognostic , or therapeutic implications have also been identied . 
atypical , non - v600 braf ( abraf ) mutations that occur outside of codon 600 are one example of an emerging molecular subtype in colorectal cancer . abraf mutations were retrospectively studied at two large centers comprehensively describing the clinical , pathologic , and survival implications of these mutations in patients with mcrc.3 a total of 9 , 643 patients with mcrc underwent ngs testing and 208 patients with abraf mutations were identied , representing 2.2% of all patients tested . 
 johnson et al context key objective to determine if atypical , non - v600 braf ( abraf ) mutations , stratied by class , affect outcomes with anti - egfr therapy and , secondarily , if acquisition of abraf mutations imparts resistance to egfr inhibition . knowledge generated clinical outcomes on the basis of functional class and their effect on anti - egfr efcacy for abraf metastatic colorectal cancer ( mcrc ) have not been dened . 
in patients with abraf wild - type ras mcrc who received anti - egfr antibodies , there were no responses among class ii or iii abraf mcrc , with stable disease as best response in our internal cohort . evaluation of a large external cohort of patients with circulating tumor dna interrogated by an anti - egfr exposure score revealed increased prevalence of abraf and subclonal abraf mutations among predicted anti - egfr exposed compared with nonexposed patients , suggesting an acquired mechanism of resistance to egfr inhibition . relevance anti - egfr therapy is limited in abraf mcrc , with class ii abraf mutations emerging as a negative predictive biomarker . detection of abraf mutations in ctdna may represent a novel mechanism of resistance warranting additional investigation . can be used sequentially throughout the course of the disease . although brafv600e mcrc is known to be predictive of poor response to anti - egfr therapy , the clinical utility of egfr inhibition in abraf mcrc remains unclear.4 , 5 of note , previous retrospective work investigating a cohort of 150 patients with refractory mcrc identied seven patients with abraf mutations and reported poor progression - free survival when they were exposed to anti - egfr therapy in comparison with a cohort with ras / raf wild - type ( ras / rafwt ) mcrc.6 preclinical work has highlighted unique biology among traditional brafv600e mutations ( class i ) and abraf mutations ( classes ii and iii ) .7 , 8 brafv600e mutations , designated as class i , result in feedback inhibition of gtp - bound ras , are ras independent , and signal as active monomers . 
in contrast , class ii abraf mutations have intermediate to high levels of kinase activity , are ras independent , signal as constitutive dimers , and are resistant to vemurafenib , whereas class iii abraf mutations have low or absent kinase activity and are primarily ras dependent and sensitive to erk - dependent feedback of ras.7 , 8 these tumors bind more tightly to ras - gtp than do wild - type braf tumors , and binding to wild - type craf is enhanced , resulting in increased erk signaling.8 these stark differences in underlying tumor biology may explain the varying response to therapy , specically the potential limitations to anti - egfr inhibition in abraf mcrc . 
cohort 1 included patients with stage iv colorectal cancer who were seen at mdacc between march 1 , 2012 , and june 27 , 2017 , and underwent targeted exome sequencing . 
all clinical and outcomes data were derived from this cohort . cohort 2 included patients with mcrc who underwent a targeted ngs ctdna assay ( guardant360 ; guardant health , redwood city , ca ) as part of their care between june 1 , 2014 , and december 26 , 2017 , at multiple institutions . 
 abraf mutations as a mechanism of resistance to egfr inhibition frequencies for both cohorts of abraf mutations : predicted anti - egfr exposed and nonexposed . statistical analysis clinicopathologic features were compared by 2 test or fishers exact test for categorical variables and assessment of odds ratios for associations as appropriate , as well as by t test to compare continuous variables . 
matched analysis adjusted by age and sidedness was undertaken to compare os among all molecular classes . 2 or fishers exact tests , as well as t test , were used to evaluate the adequacy of the matching . 
statistical analyses were performed using graphpad prism , version 6.07 ( graphpad software , la jolla , ca ) , and spss , version 23.0 ( ibm , armonk , ny )  . 
among 36 patients with abraf mcrc , 19 ( 53% ) had left - sided primary tumors and 24 ( 67% ) had microsatellite stable ( mss ) disease and were a median age of 56 years ( table 1 )  . 
of note , in contrast to brafv600e mcrc , which is mutually exclusive with ras mutations , 12 patients with abraf mcrc had ras mutations ( class iii , n = 7 of 21 [ 33% ] ; class ii , n = 5 of 10 [ 50% ] )  . 
among these , one patient with class ii abraf mcrc also had microsatellite instabilityhigh ( msi - h ) disease . for a more accurate comparison of survival outcomes among respective molecular classes , we performed a matched analysis by age and sidedness among the 36 patients with abraf mcrc compared with 36 patients with brafv600e mcrc and 36 with ras / rafwt disease ( fig 3 ; appendix table a1 )  . 
 ( % ) unless otherwise indicated . abbreviations : , not applicable ; abraf , atypical , non - v600 braf ; msi - h , microsatellite instabilityhigh ; mss , microsatellite stable ; wt , wild exposed to anti - egfr therapy in their treatment course . among patients with abraf raswt mcrc , 11 ( 50% ) received anti - egfr monoclonal antibodies ( mabs ; monotherapy , n = 1 , combination therapy , n = 10 ; class iii , n = 7 of 14 [ 50% ] , class ii , n = 3 of 5 [ 60% ] , unclassied , n = 1 )  . there were no responses reported , and six patients ( class iii , n = 4 ; class ii , n = 1 ; unclassied , n = 1 ) achieved stable abraf ( n = 36 ) brafv600e ( n = 221 ) wild - type braf ( n = 438 ) time ( months ) fig 2 . 
in line with previous reports , patients with class i or brafv600e mcrc had worse survival outcomes when exposed to egfr inhibition ( fig 4 )  . abraf mutations as a potential mechanism of resistance to anti - egfr therapy to understand our institutional ndings of limited efcacy of anti - egfr therapy in abraf mcrc , we analyzed an external ctdna cohort of 5 , 257 samples ( cohort 2 ) from 4 , 465 patients with mcrc . 
 abraf mutations as a mechanism of resistance to egfr inhibition abraf ( n = 36 ) brafv600e ( n = 36 ) wild - type braf ( n = 36 ) time ( months ) fig 3 . 
abraf , atypical , nonv600 braf . cohort , after excluding ras and brafv600e mutations , we applied a previously validated anti - egfr exposure score to divide patients into predicted prior exposure to anti - egfr ( n = 644 ) versus predicted nonexposed ( n = 2 , 880 ) .10 this revealed that the prevalence of abraf mutations increased from 3.99% among patients predicted to have no prior antiegfr exposure to 8.38% among those with predicted antiegfr exposure ( p , .001 ; fig 5a )  . as a sensitivity analysis , we evaluated the prevalence of abraf mutations among patients with egfr ectodomain mutations , compared with those without , because egfr ectodomain mutations are unequivocally present only after exposure to egfr inhibition . 
class ii activating g469a mutations ( p , .001 ) and class iii d594n ( p , .001 ) were the most common alterations among patients with predicted antiegfr exposure ( fig 5c )  . 
agents such as vemurafenib are not active , because the drug is designed to target the shape of the v600e - mutated protein and is more than 10 - fold less active against nonmutated forms . 
 ( a ) ctdna prevalence of abraf ( 3.99% ) among non - exposed patients ( n = 2 , 880 ) v ctdna prevalence of abraf ( 8.38% ) among predicted anti - egfr exposed ( n = 644 )  . 
schematic gure of the conserved region3 ( cr3 ) of the braf protein , also known as the braf kinase domain ( amino acids 457 to 717 ) , and the location of the class ii and iii hotspot mutations . 
the kinase domain contains the p - loop ( amino acids 464 - 471 ) , the c helix ( amino acids 492 - 504 ) , the dimerization interface ( dif , amino acids 504 - 511 ) , the catalytic loop ( cl , amino acids 574 - 581 ) , the dfg motif ( amino acids 594 - 596 ) , and the activation segment ( as , amino acids 594 - 623 )  . 
class ii , activating g469a mutations ( p , .001 ) and class iii , d594n ( p , .001 ) were the most common , respectively , among predicted anti - egfr exposed patients . 
although previous reports have suggested class iii abraf mcrc may achieve responses with antiegfr therapy owing to ras dependency , our cohort , albeit small , only revealed stable disease as best response.6 , 8 , 12 - 15 , 19 these results support the ndings of the breac study , which revealed no responses in six patients with abraf mcrc ( n = 2 each with class ii , class iii , and unclassied ) .6 of note , the nding of concomitant ras mutations with abraf mcrc in tissue , conrmed in our external ctdna cohort , clearly precludes the use of egfr inhibition for all patients , highlighting the need for novel combination strategies that consider this distinct signaling biology.20 , 21 in our internal and external cohorts , we did not nd a difference between patients with class ii and class iii abraf mcrc in regard to the presence of concurrent ras mutations . 
 abraf mutations as a mechanism of resistance to egfr inhibition in our mdacc internal cohort , four patients had unclassied disease ( y656d , a415v , k752r , f109i ) and had poor survival outcomes . 
in the external ctdna cohort , we found numerous unclassied abraf mutations that are yet to be functionally described ; most were commonly comutated with ras , pik3ca , and egfr . development of acquired ras and subclonal egfr ectodomain mutations are known mechanisms of resistance to anti - egfr therapy in raswt mcrc.22 - 26 considering the limitation of egfr inhibition noted in our internal cohort , the emergence of abraf potentially reects whether a novel mechanism of acquired resistance to egfr inhibition was investigated . 
analysis of our ctdna cohort showed statistically signicant increases in the prevalence of abraf mutations , subclonal abraf mutations , and multiple abraf mutations in individual ctdna samples among patients predicted to be exposed to egfr inhibition versus those predicted to be nonexposed . 
it is important to note that the rate of abraf mutation in our ctdna cohort was higher than in our internal cohort , as well as higher than what has been published in tissue - based testing.3 these ndings highlight the potential of abraf mutations as a novel acquired resistance mechanism to egfr inhibition and warrant additional prospective investigation . of note , in patients with egfr - mutant nonsmall - cell lung cancer , abraf mutations have been reported as a mechanism of acquired resistance to egfr tyrosine kinase inhibition.27 our results underscore the need for innovative combinatorial targeted approaches for abraf mutations exploiting class biology . 
data suggest that downstream signaling with novel inhibitors of mek or erk may be useful , because the pathway is still active.20 furthermore , because both class ii and class iii mutations signal through braf and / or craf target didimers , next - generation raf inhibitors that merization is of interest in combination with these agents as a rationale next step for therapeutic intervention.21 of note , regimen using safety lead - in data for a novel triplet encorafenib , binimetinib , and cetuximab for refractory brafv600e mcrc have been published showing impressive response rates and signicant in survival outcomes.28 subsequent studies will need to investigate whether this novel triplet combination strategy can also enhance optimal mapk inhibition and provide durable benet in patients with abraf mcrc . improvement there are limitations to this study . 
second , considering the rarity of abraf mcrc , we were only able to identify 36 patients in our internal cohort , of whom 30% received egfr inhibition therapy . third , detailed clinical annotation is not available for the external ctdna cohort , and we were unable to conrm that these patients had received prior anti - egfr therapy . therefore , we applied a previously validated and published anti - egfr exposure score to identify patients predicted to have anti - egfr exposure versus patients predicted to be nonexposed to conduct our ctdna analysis . our results suggest selection criteria for the use of antiegfr therapy in abraf - mutated mcrc should be based not only on raswt status but also the functional class of the atypical variant . 
in our cohort , although limited by sample size , ndings continue to generate more hypotheses in that class ii abraf mutations may represent a negative predictive biomarker of egfr inhibition , and exposure to anti - egfr mabs may adversely affect survival outcomes , whereas efcacy of egfr inhibition was limited in patients with class iii abraf mcrc . 
increased subclonal abraf mutations and prevalence of class ii and class iii variants in ctdna among patients with predicted anti - egfr exposure suggest a novel mechanism of resistance warranting additional prospective investigation . also , our data support the clinical utility of comprehensive genomic proling ( both tissue and ctdna ) in the management of advanced mcrc , because standard hotspot polymerase chain reaction testing would not capture emerging clinically signicant alterations . 
loree , kanwal raghav , scott kopetz provision of study material or patients : all authors collection and assembly of data : all authors data analysis and interpretation : benny johnson , alexandre a . 
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br j cancer 117 : 1450 - 1458 , 2017 yao z , torres nm , tao a , et al : braf mutants evade erk - dependent feedback by different mechanisms that determine their sensitivity to pharmacologic inhibition . 
cancer cell 28 : 370 - 383 , 2015 yao z , yaeger r , rodrik - outmezguine vs , et al : tumours with class 3 braf mutants are sensitive to the inhibition of activated ras . 
nature 548 : 234 - 238 , 2017 strickler jh , loree jm , ahronian lg , et al : genomic landscape of cell - free dna in patients with colorectal cancer . 
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parseghian cm , loree jm , morris vk , et al : anti - egfr resistant clones decay exponentially after progression : implications for anti - egfr re - challenge . 
cremolini c , di bartolomeo m , amatu a , et al : braf codons 594 and 596 mutations identify a new molecular subtype of metastatic colorectal cancer at favorable prognosis . 
sullivan rj , infante jr , janku f , et al : first - in - class erk1 / 2 inhibitor ulixertinib ( bvd - 523 ) in patients with mapk mutant advanced solid tumors : results of a phase i dose - escalation and expansion study . 
rankin a , klempner sj , erlich r , et al : broad detection of alterations predicted to confer lack of benet from egfr antibodies or sensitivity to targeted therapy in 19 . 
schirripa m , biason p , cortiula f , et al : clinico - pathological and molecular characterization of braf mutant metastatic colorectal cancer ( mcrc ) : are all advanced colorectal cancer . 
yu ha , suzawa k , jordan e , et al : concurrent alterations in egfr - mutant lung cancers associated with resistance to egfr kinase inhibitors and characterization of mtor as a mediator of resistance . 
distribution of abraf ( atypical , non - v600 braf ) mutations in cohort 1 ( n = 36 )  . abraf mutation class appendix johnson et al table a1 . 
faden , md1 , 2 ; roberto gomez - casal , ms3 ; diego alvarado , phd4 ; and umamaheswar duvvuri , md , phd3 introduction the epidermal growth factor receptor / human epidermal growth factor receptor ( her ) family plays a critical role in the growth of numerous human cancers . multiple therapeutics targeted to members of the her family have been developed , including the epidermal growth factor receptortargeting monoclonal antibody cetuximab , which is fda approved for treatment of head and neck squamous cell carcinoma ( hnscc )  . her3 / erbb3 is expressed in most solid tumors , including hnscc , and has been shown to correlate with a poor prognosis.1 , 2 phosphorylation of erbb3 ( perbb3 ) affects numerous pathways , including activation of the pi3k / akt pathway , driving cell survival and growth . 
for this reason , blocking erbb3 activity could be an effective strategy to decrease tumor growth and resistance to other tyrosine kinase inhibitors.3 - 5 cdx - 3379 is a human immunoglobulin g1 lambda monoclonal antibody that binds erbb3 and inhibits its activity by multiple mechanisms . 
after pathologic conrmation by biopsy , informed consent was obtained , the patient was enrolled in nct02473731 and given two 1 , 000 mg intravenous doses of cdx - 3379 . 
a signiresponse was noted within the rst cant clinical 48 hours after administration of the rst dose , with concomitant reduction in pain from 8 of 10 to 2 of 10 . on examination before surgical extirpation , the primary tumor was found to have a nearly complete response , demonstrating a 92% reduction in greatest dimension . 
tumor and germline dna underwent whole exome sequencing ( wes ) library construction with the illumina truseq kit ( san diego , ca ) , with exonic regions captured using agilent sureselect v4 ( santa clara , ca )  . 
rna underwent library preparation with the illumina truseq rna access kit followed by pairedend ( 2 76 ) sequencing on an illumina nextseq 500 , with average coverage of 45 million reads per sample . primary processing of sequence data was performed using illumina casava software v1.8. 
somatic mutations and copy number variants ( cnvs ) were identied by variantdx as previously described.10 all nonsynonymous coding variants , splice site variants , indels , and cnvs above or below 2.0 were considered potentially deleterious . 
after adapter trimming with cutadapt v1.5 , reads were mapped to the human reference genome grch37 / 38 using hisat2 v2.0.4 , and gene expression was quantitated using htseq v0.9. 
differential gene expression was performed using edger v3.20.9. quantitative real - time polymerase chain reaction total rna was isolated from human hnscc cell lines ( te6 , kyse510 , te9 , fadu , pecapj34 , cal33 , scc4 , bhy , osc19 , scc25 ) using the qiagen rneasy kit . 
 faden et al real - time polymerase chain reaction ( pcr ) was performed using the bio - rad iq sybr green supermix and applied biosystems 7900ht fast real - time pcr systethe following primers were used to detect fzd3 mrna : 5 ( cid : 2 ) - gcttccacagtgacacaagg - 3 ( cid : 2 ) and 5 ( cid : 2 ) - accatacactgccagccata - 3 ( cid : 2 )  . to detect erbb3 mrna , the following primers were used : 5 ( cid : 2 ) - actctccatatcccttcctctc - 3 ( cid : 2 ) and 5 ( cid : 2 ) - gtttcctccctttcctctct - 3 ( cid : 2 )  . pcr amplications were run in triplicate for each cell line . comparative quantication of gene expression was performed using the ct method , and values were referenced to gapdh mrna expression . erbb3 phosphorylation erbb3 phosphorylation was measured by veratag assay ( san francisco , ca ) on ffpe tissue.6 colony - formation assays five thousand cells per well were seeded in six - well plates and allowed to attach overnight . 
the area covered by stained cells was measured using imagej . statistical analysis was performed using graphpad prism 7 . perbb3 was assessed by veratag assay to examine changes in activated erbb3 pretreatment to post - treatment , revealing a 69% decrease from 0.45 to less than 0.14 ( lower limit of quantitation of the assay ) , demonstrating successful blockage of erbb3 activation by cdx - 3379 . 
we hypothesized that loss of somatic alterations from pretreatment to post - treatment , in combination with a signicant reduction in clinical tumor volume , could represent selective killing of clones more sensitive to cdx - 3379 and thus give insight terrogating the list of alterations that were present in the tumor pretreatment but not post - treatment ( on the basis of known mechanisms of action of each gene ) identied amplication of fzd3 ( frizzled class receptor 3 ) , a receptor in the wnt signaling pathway , as a possible candidate conferring sensitivity to cdx - 3379 ( table 1 )  . 
rna - seq demonstrated a 2.5 - foldhigher expression of fzd3 pretreatment versus post - treatment ( p , 4.5e - 13 ) , consistent with the 3.0 amplication identied on wes in the pre ( fig 1a )  . 
six percent ( 28 of 496 ) of hnsccs in tcga possess an fzd3 alteration that could result in an increase in downstream wnt signaling , consistent with the case reported here ( one amplication and 27 mrna upregulations )  . 
patients with hnsccs from tcga that possess an fzd3 alteration have poorer overall survival , suggesting that alterations in this gene may be important in the biology of a subset of hnsccs ( fig 1b )  . tumor to explore the possibility that fzd3 plays a role in sensitivity to erbb3 inhibition , we examined fzd3 mrna expression lines , by quantitative real - time pcr in 10 hnscc cell nding high variability among cell lines ( fig 1c )  . 
to test the hypothesis that increased fzd3 expression could render cells more sensitive to cdx - 3379 , akin to the pretreatment tumor , we performed colony - formation assays with table 1 . 
the role of wnt signaling pathways in cancer is well established.11 fzd upregulation has been identied in numerous cancers , correlates with poor outcomes , and is an active area of investigation for targeted therapeutics.11 , 12 fzd3 , in particular , is believed to play a role in both the canonical and noncanonical wnt pathways and has been found to be upregulated in lung , esophageal , and colon cancers.13 - 15 here , we report fzd3 gene amplication and overexpression in pretreatment but not post - treatment tumor from an exceptional responder to cdx - 3379 . 
review of fzd3 in hnsccs from tcga supports the potential biologic importance of alterations in this gene . we further demonstrate that fzd3 expression levels correlate with sensitivity to cdx - 3379 and that activation of fzd3 by its ligand wnt3a further potentiates the effects of cdx - 3379 . 
the mechanism by which fzd3 confers sensitivity to erbb3 inhibition is unclear ; however , the wnt and erbb pathways have been reported to closely interact and collude in tumorigenesis.16 , 17 it remains to be seen whether this is by convergence on a common downstream molecule , such as - catenin , 18 or via effects on different target genes . 
in breast cancer , wnt overexpression activates signaling via erbb.19 , 20 interestingly , we identied a tight correlation between erbb3 and fzd3 mrna expression levels in hnscc cell lines , suggesting a similar relationship and highlighting the interconnected nature of these singling pathways . 
images of a representative colony formation ( top ) with quantication of stained area represented in bar graph ( middle ) and culture additives ( bottom ) p , .001 for all comparisons by one - way analysis of variance . 
semin cell dev biol 21 : 944 - 950 , 2010 takikita m , xie r , chung jy , et al : membranous expression of her3 is associated with a decreased survival in head and neck squamous cell carcinoma . 
j transl med 9 : 126 , 2011 lee - hoeich st , crocker l , yao e , et al : a central role for her3 in her2 - amplied breast cancer : implications for targeted therapy . 
cancer res 68 : 5878 - 5887 , 2008 sergina nv , rausch m , wang d , et al : escape from her - family tyrosine kinase inhibitor therapy by the kinase - inactive her3 . 
nature 445 : 437 - 441 , 2007 brand tm , hartmann s , bhola ne , et al : cross - talk signaling between her3 and hpv16 e6 and e7 mediates resistance to pi3k inhibitors in head and neck cancer . 
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j clin oncol 34 , 2016 ( suppl ; abstr 2501 ) duvvuri u , george j , kim s , et al : molecular and clinical activity of cdx - 3379 , an anti - erbb3 monoclonal antibody , in head and neck squamous cell carcinoma : a preoperative window of opportunity study . 
schroeder ja , adriance mc , mcconnell ej , et al : erbb - beta - catenin complexes are associated with human inltrating ductal breast and murine mammary tumor virus ( mmtv ) - wnt - 1 and mmtv - c - neu transgenic carcinomas . 
faivre ej , lange ca : progesterone receptors upregulate wnt - 1 to induce epidermal growth factor receptor transactivation and c - src - dependent sustained activation of erk1 / 2 mitogen - activated protein kinase in breast cancer cells . 
these preclinical observations suggest a role for the targeted inhibitors of the bcr pathway in the treatment of dlbcl.1 dlbcl is most commonly present as malignant inltration of lymph nodes . 
the use of btk inhibitors is now incorporated into standard therapy for these conditions , and the genetic basis of acquired resistance in cll , dominated by acquired mutation of btk or plcg2 , has been well - studied.6 , 7 by contrast , the role of bcr inhibition in dlbcl remains less clear and little is known about the genetics of acquired resistance . a 75 - year - old male presented with rapidly enlarging cutaneous nodules . 
clinical examination revealed cutaneous nodules up to 25 mm in diameter affecting the feet , legs , arms , and abdomen . a repeat biopsy showed features identical to his original diagnostic biopsy ( fig 1a ) , and computed tomography scan conrmed exclusively cutaneous disease . 
the patient was managed with palliative radiotherapy . the rapid clinical response and prolonged remission , followed by later re - emergence of tumor , suggested the acquisition of new genetic alterations driving resistance to bcr inhibition . 
this study was approved by the east of england cambridge south research ethics committee ( approval reference number 07 / mre05 / 44 )  . full variant and copy number data are presented in the data supplement . 
 ( a ) histology and immunohistochemistry from tumor biopsy showing a diffuse inltration by large atypical cells with predominantly centroblast - like morphology expressing cd20 , mum1 , bcl2 , weak bcl6 , no cd10 , and mib1 proliferation fraction 90% . 
 ( b ) images of selected lesions on the forearm , hand , popliteal fossa , and abdomen taken prior to therapy ( top row ) , at 28 days ( middle row ) , and at 6 months ( bottom row ) of b cell receptortargeted therapy . 
 ( a ) summary of whole - exome sequencing of samples taken from three different timepoints ; diagnosis , prior to bcr - targeted therapy , and at the time of relapse . 
gray indicates no mutation or copy number change identied . ( b ) a simplied schematic showing the critical signaling components of the bcr pathway that converge onto activation of canonical nf - b . components targeted pharmacologically in this patient are indicated . 
we manually examined the loci of plcg2 and btk , mutations that are commonly acquired in btki - resistant cll , and conrmed both genes to be wild type at all timepoints . 
 case report in the bcr pathway to activate canonical nf - b signaling.1 activating mutation in the coiled - coil domain of card11 was previously proposed as a mechanism of resistance to bcr inhibition in mantle cell lymphoma8 and primary resistance in dlbcl.9 the acquired k215t mutation in our patient is located in the coiled - coil domain and has been previously shown to activate nf - b.10 we conrmed the near - clonal presence of the card11 k215t mutation at relapse ( variable allele frequency 40% ) but zero mutant reads at this position in either of the two pretreatment biopsies ( read depth , 180 and 210 , appendix fig a3 )  . 
taken together , these data strongly suggest that card11 mutation was the genetic driver of the acquired resistance in this case . the limited information about acquired resistance to bcr inhibition in dlbcl suggests potential differences compared with that of cll . 
the latter is predominantly associated with mutation of btk and plcg2.6 , 7 card11 identied in 10% - 15% of dlbcl at mutation is presentation11 but is rarely identied ( , 1% ) in cll.12 this suggests that the bcr signal in cll and dlbcl may be qualitatively different and therefore that genetic mechanisms of resistance to bcr inhibition may also differ . however , establishing the genetic basis of resistance to bcr inhibition in dlbcl presents specic challenges that contrast with the situation in cll . 
first , patients with dlbcl receiving bcr inhibitors are typically treated simultaneously with multiagent immunochemotherapy regimens , making it hard to establish which mutations provide resistance to which agent , or indeed if sensitivity to the bcr inhibitor ever existed in the rst place . 
combined with the biopsy - accessible cutaneous location of disease , this provided a rare opportunity to study genetic mechanisms of resistance to bcr inhibition in abc dlbcl . indeed , we have found only one other case describing the genetic basis of acquired resistance to bcr inhibition in dlbcl . 
this also involved a case of pcdlbcl - lt and also reported acquisition of card11 mutation ( interesting also k215 mutant ) in a patient who relapsed following an initial response to a btk inhibitor.13 however , the concurrent nding of nfkbie mutation and igh - irf8 translocation reported in that study might also have contributed to resistance , leaving the role of the card11 mutation uncertain . our ndings of acquired activating card11 mutation , the absence of any likely alternative genetic explanation , and the demonstrated ability of the k215t mutation to affect btki resistance in vitro strongly suggest that card11 mutation is the dominant driver of bcr independence in our case . as we move toward the introduction of precision medicine in dlbcl and the real - time monitoring of clonal evolution , it will become increasingly important to understand genetic mechanisms of drug resistance . 
our study uses the unique features of this case of cutaneous dlbcl to highlight the importance of card11 mutation as a driver of acquired resistance to bcr inhibition in dlbcl . 
hodson provision of study materials or patients : nimish shah collection and assembly of data : rebecca caeser , ieuan walker , jie gao , nimish shah , livia rasso - barnett , jose - ezequiel martin , daniel j . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . rebecca caeser consulting or advisory role : karus therapeutics nimish shah consulting or advisory role : abbvie speakers bureau : roche , janssen travel , accommodations , expenses : abbvie livia rasso - barnett leadership : cambridge pathology stock and other ownership interests : cambridge pathology honoraria : cambridge pathology consulting or advisory role : cambridge pathology daniel j . 
semin hematol 52 : 77 - 85 , 2015 swerdlow sh , campo e , pileri sa , et al : the 2016 revision of the world health organization classication of lymphoid neoplasms . 
blood 127 : 2375 - 2390 , 2016 grange f , beylot - barry m , courville p , et al : primary cutaneous diffuse large b - cell lymphoma , leg type : clinicopathologic features and prognostic analysis in 60 cases . 
mareschal s , pham - ledard a , viailly pj , et al : identication of somatic mutations in primary cutaneous diffuse large b - cell lymphoma , leg type by massive parallel sequencing . 
j invest dermatol 137 : 1984 - 1994 , 2017 pham - ledard a , prochazkova - carlotti m , andrique l , et al : multiple genetic alterations in primary cutaneous large b - cell lymphoma , leg type support a common lymphomagenesis with activated b - cell - like diffuse large b - cell lymphoma . 
j clin oncol 35 : 1437 - 1443 , 2017 ahn ie , underbayev c , albitar a , et al : clonal evolution leading to ibrutinib resistance in chronic lymphocytic leukemia . 
fox lc , yannakou ck , ryland g , et al : molecular mechanisms of disease progression in primary cutaneous diffuse large b - cell lymphoma , leg type during ibrutinib therapy . 
nagel d , spranger s , vincendeau m , et al : pharmacologic inhibition of malt1 protease by phenothiazines as a therapeutic approach for the treatment of aggressive abc - dlbcl . 
 case report chr1 chr3 chr5 chr11 chr13 chr15 chr17 chr19 chr21 chrx prdm1 tnfaip3 chr7 cdkn2a chr9 rb1 gna13 chr2 chr4 chr6 chr8 chr10 chr12 chr14 chr16 chr18 chr20 chr22 chry mir17 - 92 bcl2 malt1 tcf4 cd79a spib mir17 - 92 bcl2 malt1 tcf4 cd79a spib chr1 chr3 chr5 chr7 chr9 chr11 chr15 chr17 chr19 chr21 chrx chr2 chr4 chr6 chr8 chr10 chr12 chr14 chr16 chr18 chr20 chr22 chry prdm1 tnfaip3 rb1 chr13 gna13 appendix relapse pre - treatment diagnosis chr1 chr3 chr5 chr7 chr9 chr11 chr13 chr15 chr17 chr19 chr21 chrx chr2 chr4 chr6 chr8 chr10 chr12 chr14 chr16 chr18 chr20 chr22 chry fig a1 . 
 role of community - based genomics programs see accompanying article doi : increasingly , genomic changes in patients tumors are used to inform individualized management , although the optimal approach and impact of tumor profiling on cancer care , especially in the community setting , remain important research questions.1 , 2 challenges in applying precision medicine approaches include cost and access to genomic testing and to indicated therapies , lack of actionable gene alterations , education of all stakeholders , patient expectations , complexity of interpretation of data , access to big data solutions , and expansion of physicians comfort zones . 
arguably , the latter represents the most formidable challenge . in the article accompanying this editorial , burkard et al3 address many of these challenges in their report , implementation and clinical utility of an integrated academic - community regional molecular tumor board . 
the implementation of a novel wisconsin state - wide model , including a precision - medicine molecular tumor board ( pmmtb ) , an institutional review boardapproved registry protocol , and a journal club , allows for addressing many of the challenges of precision medicine . 
the authors point out that in the united states , much of precision medicine is implemented in an academic - center context , often in conjunction with robust clinical trial platforms , to include big data analytic informatics solutions . conversely , most patients are cared for outside of such academic systems.4 the challenge is to provide patients access , through their community - based providers , to the potential benefits of precision medicine . 
the described model is an academic and community partnership that allows for nextgeneration sequencing ( ngs ) through any clinical laboratory improvement amendmentscertified laboratory , and uses as its cornerstone a twiceweekly web - based pmmtb teleconference , provided as a free service . 
as with most molecular tumor boards ( mtbs ) , the focus is on prioritizing labeled and off - label therapies , as well as clinical trial options , on the basis of biologic profiling of the patients tumor . 
the model addresses the increasingly dynamic nature of the molecular pathology report with its interpretation of a specific genotype and its clinical importance often becoming outdated in the short term . the presence of an institutional review board approved registration trial assists in observing the clinical course of patients to include relevant outcomes . 
patients may have molecular profiling performed early in their clinical course ; thus , long - term follow - up allows for evaluating the downstream impact of the original molecular profiling or that of any subsequent repeat molecular profiling . this type registry is especially important given the uncertainties regarding the value proposition of precision medicine in daily practice . 
the construct of this tripartite model seeks to address the challenges of precision medicine , though the results reported by burkard et al3 emphasize the remaining barriers to successful implementation of precision medicine platforms in community settings and beyond . over approximately 1 year , a modest number of patients with metastatic / incurable cancer ( n 5 74 ) were presented at the pmmtb ; only 38 evaluable patients were enrolled in the registration trial , and some of these were enrolled retrospectively . 
 actionable target ( ie , molecularly targeted clinical trial and / or off - trial treatment ) was identified in 32 patients , with treatment accepted in only nine patients ( 28% )  . 
only one patient was enrolled in an instate clinical trial , although a total of 14 patients had clinical trial options within the state , and no patients were enrolled in out - of - state clinical trials . 
during much of the reported period in the registry trial , the national cancer institute molecular analysis for therapy choice ( match ) basket trial was on hold , and there was no access to the asco targeted agent and profiling utilization registry ( tapur ) basket trial . 
clinical benefit was seen in three of eight ( 38% ) evaluable patients , with a response evaluation criteria in solid tumors ( recist ) - defined response in one patient . this novel precision - medicine model aims at networking academic and community providers to deliver genomically driven care to patients closest to where they live and under the care of their community physicians . 
what role does cost play with regard to accessing ngs testing and targeted drugs ? given the wide range of ngs testing platforms , how is quality assured ? this is especially important because clinical laboratory improvement amendments certification does not address many quality dimensions inherent to ngs testing . in this report , the mean number of prior therapies for patients was two . 
when is the most effective time to perform ngs testing during a patients clinical course : earlier or later ? similarly , a range of ngs panel sizes was used , with a not - surprising suggestion that larger comprehensive panels are more frequently associated with treatment options . where does cost effectiveness guide us in selecting ngs panel size ? with regard to actionable gene alterations , it is remarkable that by recent analysis , the us food and drug administration has only approved 22 gene alterations with associated biomarkers.7 , 8 the key to defining labeled indications for targeted therapies is participation in clinical trials such as match and tapur . additional clinical trial approaches include prospective registration - type trials that contain detailed data elements , including demographic data , clinical outcomes measures , and quality - of - life and economic metrics that allow for long - term follow - up and planned statistical analyses . one aspect not referenced in the burkard et al3 report is the underlying informatics platforthe scalability of such a platform , as well as its interfacing capabilities , along with its analytic functions , are key , especially across a multisite network . 
in particular , a clinical - trials matching function that allows for prioritizing variables such as geographic distance and relevance to an individual patients unique characteristics , and those of their tumor , will facilitate identification of the most promising clinical trials for a given patient . 
in addition , engaging busy clinicians is always a challenge , and one presumed solution is to have approaches and platforms that align with their daily work flow , including integration into existing informatics platforms , most especially the electronic medical record , along with automatic extraction of data elements from existing electronic databases , which limits the need for form completion , whether electronic or manual . 
for example , maximal use of high quality databases , such as tumor registries or the seer program database , can help overcome the challenges of relying on semistructured data within the electronic medical record . the demonstration of the value proposition for precision medicine is a work in progress . 
it will require clinical trial experience with genomically driven therapies across a broad population of patients with varied tumor types , cared for by a range of providers , and in varied settings , to include the broad variety of community practices . 
the newer formulation of clinical trial design , whether the basket or umbrella type design or that of sophisticated registry trials , such as those described by burkard et al , will substantially facilitate the access to targeted therapy trials in the community setting.9 , 10 these trials provide guidance for community physicians in identifying gene alterations or biomarkers with appropriate targeted therapies and provide access to off - label targeted therapies . 
brown td , tittel pd , gold pj , et al : impact of a personalized medicine research program ( pmrp ) , using targeted tumor profiling and a cloud based clinical trials matching platform , on clinical decision - making . 
 effects of molecular heterogeneity on survival of patients with brafv600 - mutated melanoma treated with vemurafenib with or without cobimetinib in the cobrim study purpose the treatment of advanced brafv600 - mutated melanomas with braf inhibitors ( brafi ) has improved survival , but the efficacy of brafi varies among individuals and the development of acquired resistance to brafi through reactivation of mitogen activated protein kinase ( mapk ) signaling is common . 
we performed an exploratory , retrospective analysis to investigate the effects of brafv600 allelic balance , coexisting oncogene mutations , cell proliferation signaling levels , and loss of pten expression on progression - free survival ( pfs ) in patients in the phase iii cobrim study , which compared the combination of the mek inhibitor cobimetinib with the brafi vemurafenib versus vemurafenib as monotherapy . methods baseline tumor samples from the intention - to - treat population were analyzed by targeted deep sequencing at a median coverage of 3 , 600 and by immunohistochemistry for cell proliferation markers , brafv600e , and pten . 
gene expression in relation to loss of pten was profiled by rna sequencing in 205 patient samples and 42 brafv600 - mutated melanoma cell lines . results neither brafv600 allelic balance nor coexisting mutations in the ras / raf / rtk pathway affected pfs in either treatment group . 
loss of function of the tumor suppressor pten ( via both genetic alterations and other mechanisms such as epigenetic silencing ) occurs in > 20% of patients with brafv600 - mutated melanoma.15 - 17 loss of functional pten has been associated with a shorter pfs response to braf inhibition , 17 , 18 reduced overall survival , and a shorter time to the development of brain metastases.15 , 19 pten / akt signaling is known to interact with mapk signaling . 
for example , meki have been shown to enhance epidermal growth factorinduced akt activation , and mutations that activate pi3k / akt signaling reduce mapk signaling.20 to understand the impact of baseline tumor heterogeneity on the efficacy of treating advanced melanoma with meki and brafi , we systematically examined the effect of braf allelic balance , coexisting oncogene mutations , and cell proliferation signaling levels on pfs in all evaluable cobrim study participants . 
here , we report the results of this retrospective , exploratory analysis . methods analysis population samples for biomarker analysis were collected from patients with unresectable locally advanced or metastatic brafv600 - mutated melanoma in the cobrim study of cobimetinib combined with vemurafenib versus vemurafenib monotherapy , 6 with the aim of exploring intrinsic mechanisms of resistance to mek and braf inhibition . 
brafv600 allelic balance , coexisting oncogene mutations , cell proliferation biomarkers , and loss of pten expression were analyzed in samples from the cobrim intention - to - treat ( itt ) population . 
most analyses could not be performed on the complete itt population ( n = 495 ) because of insufficient tissue availability or assay failure . genetic marker analysis archival formalin - fixed paraffin - embedded ( ffpe ) melanoma tumor samples , biopsy specimens of accessible tumor lesions , and blood samples were obtained from consenting patients at study entry ( baseline )  . 
rna was extracted using the high pure rna paraffin isolation kit ( roche diagnostics , indianapolis , in )  . from the 495 patients in the cobrim itt population , 400 pretreatment tumor samples were evaluable by targeted next - generation sequencing . 
 ( a ) distribution of variant allele frequency ( vaf ; ratio of mutant to wild type [ wt ] ) in brafv600 in 400 baseline tumor samples from cobrim study patients . 
 ( b ) impact on progression - free survival ( pfs ) indicated by kaplan - meier plots of pfs in patients grouped by vaf above or below the median for each treatment ar ( c ) immunohistochemistry of brafv600e protein levels in tumor samples with a range of vafs ; increased vaf was associated with greater staining intensity . 
cobi , cobimetinib ; pbo , placebo ; vem , vemurafenib . mutations ( appendix table a1 ) was performed for a focused panel of 17 oncogenes ( suraseq targeted next - generation sequencing assay ; asuragen , austin , tx ) 21 at a median coverage of 3 , 600 . 
different cutoff points were explored earlier in the analysis and gave results similar to those shown here using the median vaf as the high and low cutoff ( appendix fig a1 )  . 
the median was chosen to be representative of the overall range of cutoff points . analysis of pten copy number and methylation status in 42 brafv600 - mutant melanoma cell lines was performed as described by haverty et al.22 analysis of methylation status was performed in bisulfite - treated genomic dna using the illumina 450k array ( infinium humanmethylation450 beadchip kit ; illumina , san diego , ca )  . 
methylation data were analyzed using the methyanalysis package for r.23 gene expression in relation to loss of pten was profiled by rna sequencing in 205 patient samples and in 42 braf v600 - mutant melanoma cell lines . 
rna was prepared for high throug hput sequencing with the truseq rna access library prep kit ( illumina ) , and 40 million 2 100 - bp reads were sequenced per sample using illumina hiseq . 
coexisting oncogene mutations and impact on progression - free survival ( pfs ) in patients treated with cobimetinib ( cobi ) combined with vemurafenib ( vem ) or vem monotherapy . 
 ( b ) pfs in patients with or without ras / raf / rtk mutations ( both treatment arms were combined to give sufficient numbers of patients with ras / raf / rtk mutations for statistical analysis )  . 
 ( c ) patients with coexisting ras / raf / rtk mutations had elevated levels of phosphorylated extracellular regulated kinase ( perk ) , measured by immunohistochemistry , compared with patients with wild - type ( wt ) ras / raf / rtk , indicating greater mitogen - activated protein kinase signaling pathway activity . 
 defined by the molecular signatures database emt hallmark collection , 24 was compared by z - score ( sum of log2 reads per kilobase of transcript per million mapped reads for all genes on the emt hallmark collection ) between samples with functional and nonfunctional pten . and immunohistochemical markers and a pfs data cutoff date of january 16 , 2015 . 
 expression levels were quantified by histo - score ( h - score ) , and samples were grouped as high or low , depending on whether the h - score was above or below the median , respectively . 
in a subset of samples , brafv600e expression was also evaluated by ihc ( antibrafv600e [ ve1 ] mouse monoclonal primary antibody ; ventana [ n = 39 ] )  . in vitro studies the effect of pten loss on drug sensitivity was evaluated in 42 brafv600 - mutant melanoma cell lines by analyzing cell viability after vemurafenib treatment . 
 in all samples , > 95% of tumor cells stained positive for brafv600e mutation , suggesting that differences in vaf reflect cells across the tumor rather than indicate a subclonal mutation , and that increased vaf was associated with greater staining intensity ( fig 1c )  . 
similar results were seen in a set of four melanoma cell lines ( appendix fig a2 )  . association between oncogene mutations and pfs to explore potential drivers of brafi resistance affecting survival , in addition to previously identified mechanisms such as mek mutation , 27 coexisting mutations in a panel of 17 oncogenes21 ( appendix table a1 ) were assayed in baseline braf - mutated tumor tissue from 400 of 495 patients in the cobrim itt population and were identified in 43 patients ( 11% ; fig 2a )  . 
h - score , histo - score ; mut , mutation ; pbo , placebo ; pd , progressive disease ; pr , partial response ; sd , stable disease . 
cell proliferation biomarkers and impact on progression - free survival ( pfs ) in patients treated with cobimetinib ( cobi ) combined with vemurafenib ( vem ) or vem monotherapy . 
 ( a ) kaplan - meier plots of pfs in patients grouped by high ( above the population median histo - score [ h - score ] of 40 ) or low ( below the population median ) phosphorylated extracellular regulated kinase ( perk ) levels . 
 ( b ) kaplan - meier plots of pfs in patients grouped by high or low baseline proliferation index , measured by the protein encoded by themki67gene ( ki - 67 ) immunohistochemistry ( population median ki - 67 level is 20% ) or ( c ) phosphorylated s6 immunohistochemistry ( ps6 ; population median h - score is 71 )  . 
 ( c ) rna sequencing profiling of melanoma samples from cobrim comparing the epithelial - mesenchymal transition ( emt ) gene expression signatures in tumors with pten loss versus tumors with normal pten levels . 
patient characteristics were similar between patients with and without loss of pten expression in the cobimetinib combined with vemurafenib and the vemurafenib monotherapy cohorts , with the exception that more patients with loss of pten expression had elevated lactate dehydrogenase in the cobimetinib combined with vemurafenib arm ( appendix table a3 )  . 
 ( b ) rna sequencing profiling of braf - mutant melanoma cell lines with or without pten loss comparing the epithelial - mesenchymal transition ( emt ) gene expression signatures . 
 loss of pten expression was associated with upregulation of the emt gene expression signature in these melanoma cell lines ( fig 5b ) , similar to that seen in the baseline tumor samples . 
when tested in an in vitro wound healing assay , in the absence of vemurafenib or cobimetinib , cell lines with loss of pten showed a higher capacity for migration ( fig 5c ) , consistent with observed clinical manifestations and previous preclinical findings.28 , 29 attempts to analyze whether vemurafenib or cobimetinib combined with vemurafenib affected the increased cell migration behavior associated with loss of pten were confounded by their effect on cell viability . discussion to our knowledge , this retrospective biomarker analysis of brafv600 - mutated melanoma samples from the cobrim study is the largest such study to date . 
although there was an association between signaling pathway activity and pfs in patients treated with vemurafenib monotherapy , increased mapk signaling and cell proliferation did not affect pfs in patients treated with a combination of cobimetinib and vemurafenib . 
 the combination of mek and braf inhibition thus seems to override the poor prognostic effect of increased mapk pathway activation . loss of pten expression is linked to reduced survival in advanced melanoma , most likely as a result of suppression of apoptosis and enhanced cell survival mediated by hyperactivation of pi3k / akt signaling.17 , 18 our analysis suggests that combined mek and braf inhibition can overcome the effect of loss of pten on pfs . 
 loss of pten function in addition to brafv600 mutation has been linked to the rapid development of brain metastases in advanced melanoma , which may also contribute to reduced pfs.15 , 26 our analysis confirms that brafv600 - mutated melanoma cells with loss of pten function have a higher expression of genes associated with emt , as well as enhanced migration . 
functional pten inhibits cell migration through dephosphorylation of focal adhesion kinase ( fak ) ; loss of pten relieves this inhibition.29 in prostate cancer models , ras / mapk activation cooperated with pten loss to promote emt and metastasis , and mek inhibition was able to reduce metastatic progression in these models.30 mek can also activate fak to promote cell migration , and mek inhibition could therefore downregulate fak - mediated migration , 31 addition to reducing the cell survival resulting from ras / mapk activation in brafv600 - mutated melanoma . 
this suggests a potential mechanism by which cobimetinib combined with vemurafenib could contribute to a survival benefit in patients with braf v600 - mutated melanoma and loss of pten . the large patient cohort available for analysis was a significant strength of this study ; however , the analysis was limited by the inability to evaluate baseline tumor samples for approximately 20% of patients included in the cobrim study . additional investigation of the mechanisms underlying intrinsic and acquired resistance is warranted . 
 the molecular mechanisms at work in patients with prolonged responses to combination therapy with cobimetinib and vemurafenib are still under investigation but may involve regulation of the host antitumour immune response.33 the overall findings of this study suggest that deeper inhibition of the mapk pathway through combined inhibition of both mek and braf overrides the effects of molecular heterogeneity to provide a survival benefit to all patients . 
 this both supports and provides a rationale for the greater efficacy of combination therapy with braf and meki , which has become the standard of care , compared with braf inhibition alone . 
ascierto , brigitte drno , anna maria di giacomo , claus garbe , ilsung chang , jessie hsu , hartmut koeppen , james larkin , yibing yan , grant a . 
wongchenko employment : genentech / roche stock and other ownership interests : genentech / roche , ariad pharmaceuticals antoni ribas stock and other ownership interests : compugen , flx bio , cytomx therapeutics , five prime therapeutics , advaxis , arcus biosciences , tango therapeutics , pact pharma consulting or advisory role : merck , amgen , genentech / roche , novartis paolo a . 
 james larkin honoraria : eisai , bristol - myers squibb , msd , glaxosmithkline , pfizer , novartis , genentech / roche , sectra , pierre fabre , eusa pharma , consulting or advisory role : eisai , bristol - myers squibb , msd , glaxosmithkline , pfizer , novartis , genentech / roche , sectra , pierre fabre , eusa pharma research funding : pfizer ( inst ) , novartis ( inst ) , msd ( inst ) , bristol - myers squibb ( inst ) travel , accommodations , expenses : bristol - myers squibb , pfizer , novartis , genentech / roche yibing yan employment : genentech / roche stock and other ownership interests : genentech / roche patents , royalties , other intellectual property : genentech / roche grant a . 
wongchenko , ilsung chang , jessie hsu , isabelle rooney , william lu , hartmut koeppen , and yibing yan , genentech , south san francisco ; antoni ribas , jonsson comprehensive cancer center at the university of california , los angeles , los angeles , ca ; paolo a . 
pascale , naples ; anna maria di giacomo , azienda ospedaliera universitaria senese , siena , italy ; brigitte drno , nantes university , nantes , france ; claus garbe , university of tbingen , tbingen , germany ; james larkin , the royal marsden hospital , london , united kingdom ; grant a . 
ascierto pa , mcarthur ga , drno b , et al : cobimetinib combined with vemurafenib in advanced braf ( v600 ) - mutant melanoma ( cobrim ) : updated efficacy results from a randomised , doubleblind , phase 3 trial . 
hauschild a , grob j - j , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
wilmott js , menzies am , haydu le , et al : braf ( v600e ) protein expression and outcome from braf inhibitor treatment in braf ( v600e ) metastatic melanoma . 
wagle n , van allen em , treacy dj , et al : map kinase pathway alterations in braf - mutant melanoma patients with acquired resistance to combined raf / mek inhibition . 
bucheit ad , chen g , siroy a , et al : complete loss of pten protein expression correlates with shorter time to brain metastasis and survival in stage iiib / c melanoma patients with brafv600 mutations . 
xing f , persaud y , pratilas ca , et al : concurrent loss of the pten and rb1 tumor suppressors attenuates raf dependence in melanomas harboring ( v600e ) braf . 
nathanson kl , martin a - m , wubbenhorst b , et al : tumor genetic analyses of patients with metastatic melanoma treated with the braf inhibitor dabrafenib ( gsk2118436 )  . 
latham g , hough j , sah s , et al : suraseq targeted ngs assays : integrated , cross - platform reagents that enable accurate detection of cancer gene mutations in residual clinical ffpe , fna , and biofluid biopsies . 
mcarthur ga , larkin j , ascierto pa , et al : impact of baseline allelic frequencies of brafv600 mutation and coexisting oncogenic mutations on progression - free survival from the cobrim phase 3 study evaluating cobimetinib + vemurafenib in advanced brafv600 - mutated melanoma . 
larkin jmg , yan y , mcarthur ga , et al : update of progression - free survival ( pfs ) and correlative biomarker analysis from cobrim : phase iii study of cobimetinib ( cobi ) plus vemurafenib ( vem ) in advanced braf - mutated melanoma . 
tamura m , gu j , takino t , et al : tumor suppressor pten inhibition of cell invasion , migration , and growth : differential involvement of focal adhesion kinase and p130cas . 
mulholland dj , kobayashi n , ruscetti m , et al : pten loss and ras / mapk activation cooperate to promote emt and metastasis initiated from prostate cancer stem / progenitor cells . 
wongchenko mj , mcarthur ga , drno b , et al : gene expression profiling in braf - mutated melanoma reveals patient subgroups with poor outcomes to vemurafenib that may be overcome by cobimetinib plus vemurafenib . 
exploration of the impact of variant allele frequency ( vaf ) on progression - free survival ( pfs ) indicated by kaplan - meier plots of pfs in patients grouped by vaf above or below cutoff points of ( a ) 25% and ( b ) 50% for each treatment arfor the analysis , the median was chosen to be representative of the overall range of cutoff points . 
cell viability of 42 brafv600 - mutant melanoma cell lines treated with vemurafenib , stratified by expression versus loss of expression of pten . pten + ( n = 20 ) pten loss ( n = 22 ) table a1 . 
leach , ms , lgc1 ; jessica marquard , ms , lgc1 ; manmeet ahluwalia , md1 ; hetty carraway , md , mba1 ; petros grivas , md , phd2 ; davendra p.s. 
recent data sets indicate that the incidence of hereditary cancer may be as high as 17.5% in patients with cancer , and a notable subset is missed if screening is solely by family history and current syndrome - based testing guidelines . identication of germline variants has implications for both patients and their families . 
we aimed to summarize genes linked to hereditary cancer and the somatic and germline panels that include such genes . methods germline predisposition genes were chosen if commercially available for testing . 
penetrance was dened as low , moderate , or high according to whether the gene conferred a 0% to 20% , 20% to 50% , or 50% to 100% lifetime risk of developing the cancer or , when percentages were not available , was estimated on the basis of existing literature descriptions . results we identied a total of 89 genes linked to hereditary cancer predisposition , and we summarized these genes alphabetically and by organ systewe considered four germline and six somatic commercially available panel tests and quantied the coverage of germline genes across thecomparison between the number of genes that had germline importance and the number of genes included in somatic testing showed that many but not all germline genes are tested by frequently used somatic panels . conclusion the inclusion of cancer - predisposing genes in somatic variant testing panels makes incidental germline ndings likely . 
2019 by american society of clinical oncology introduction cancer is a genetically driven disease triggered by the accumulation of variants in genes responsible for regulation of cell growth , invasion , survival , and migration . 
most cancers are sporadic and result from acquired genetic changes known as somatic variants , which are caused by stochastic events that accumulate over time as well as by specic environmental factors , such as smoking and ultraviolet radiation , among others.1 precision oncology currently consists of an effort to understand the acquired genetic variants that underlie each patients cancer , which thus allows the opportunity to tailor therapy to a patients individual tumor biology.2 although tumor testing previously involved sequencing of individual genes or short hotspot fragments of dna , recent advances in next - generation sequencing ( ngs ) technology have enabled much more frequent and precise identication of pathogenic variants.2 , 3 such sequencing platforms are rapidly becoming faster and cheaper , which makes them as available and as popular as many other clinical testing tools.4 , 5 germline variants occur in germ cells , which are responsible for reproduction . 
although somatic variants occur in a single cell and are passed down only to that cells offspring , germline variants exist in all somatic cells and can inuence cancer susceptibility by affecting multiple cellular processes ( eg , cancer clone growth , somatic variant acquisition rates , and carcinogen metabolism ) .1 discovery and understanding of germline variants are of major clinical importance to the patient diagnosed with a hereditary cancer ; the identication of an inherited genetic variant often has therapeutic and prognostic value for a patient undergoing therapy . 
 akras et al showing promise in the context of both somatic and germline variants in brca and other homologous repair genes and represent a breakthrough niche in precision oncology.7 therapeutic consequences of other germline ndings are also expanding ; this is best highlighted by the recent nding that lynch syndromerelated cancers are exquisitely sensitive to programmed cell death - 1 inhibition.8 finally , a germline nding is clinically important in that members of the patients broader family who also carry inherited pathogenic variants will be at an increased risk of cancer as well.9 targeted surveillance is important for all carriers of germline pathogenic variants , whether they are cancer survivors or asymptomatic relatives ; the vast majority of inherited cancer predisposition syndromes increase the risk of multiple cancers , and targeted surveillance for the discrete subset of cancers associated with that particular gene should be undertaken . 
in addition , data support that gene - specic , directed cancer surveillance programs can be life - saving for carriers.10 , 11 thus , identication of pathogenic variants in the germline is critical for the improvement of health outcomes in cancer treatment and prevention . previously , it had been estimated that a small minority of cancers ( 5% to 10% ) are a result of inherited germline pathogenic variants.9 emerging data sets in the post - ngs era indicate that the incidence of hereditary cancer may be as high as 17.5% in patients who carry a diagnosis of cancer and even higher in specic histologic types , such as ovarian cancer and urothelial carcinoma.12 - 14 multiple studies have shown that somatic tumor dna sequencing may lead to incidental ndings of hereditary risk.15 , 16 this realization magnies the potential impact of somatic testing and prompts the need for a re - evaluation of companion germline diagnostic methodology . 
in this review , we provide a summary of genes related to hereditary cancer and assess the comprehensiveness of somatic and germline panels that test them . genes with germline implications table 1 catalogs cancer predisposition genes organized by tumor type ; each row lists all associated germline genes for a given tumor type . 
as an alternate reference , table 2 lists cancer predisposition genes in alphabetical order ; each row lists associated cancers and the estimated penetrance of these cancers for that particular gene . 
the dual table organization allows an oncologist to use either the clinical presentation or the results of somatic genetic testing as a screening tool to understand if a patients family history or somatic genetic testing result , respectively , may represent a germline variant . reviewed genes were chosen on the basis of their identication as cancer - susceptibility genes for which commercial germline testing is available from the four major germline testingfocused companies in the united states . 
for each cancer predisposition gene in table 2 , associated cancers are broadly categorized by the estimated penetrance categories ( high , medium , and low penetrance ) for that gene . 
penetrance was dened as low , moderate , or high , according to a 0% to 20% , 20% to 50% , or 50% to 100% lifetime chance of developing that particular cancer or , when percentages were unavailable , an estimate based on descriptions in the existing literature.17 it is important to note that different studies may declare varying penetrance rates for a gene , so we aimed to reect the ndings of the literature at large . as seen in table 2 , cancer - associated genes have greatly varying penetrance rates for different phenotypes ( ie , different types of cancer )  . 
for example , pathogenic variants in lynch syndrome genes ( ie , epcam , mlh1 , msh2 , msh6 , pms2 ) are not highly penetrant for pancreatic cancer but are for colorectal cancer . 
these differences in penetrance also underscore the importance of gene - based , rather than syndromic or histology - based , interpretations , given the unique physiology that underlies specic variants . in addition , several germline variants confer an increased risk only if they are biallelic ( ie , both alleles of the gene carry pathogenic variants )  . 
if genes are not marked as such , they can be assumed to confer risk when monoallelic ( ie , only one allele is altered )  . in the appropriate scenario , these tables can be used to guide genetic testing and counseling ; however , they should the current clinical be used with an understanding of limitations of such data . 
cancer subtypes and associated hereditary genes that confer risk ( continued ) cancer type associated germline genes skin ( scc ) small bowel ( ac ) thyroid acd , blm , cdkn2a , fancc , recql4 , terc , tert , tp53 apc , bmpr1a , epcam , mlh1 , msh2 , msh6 , mutyh , pms2 , smad4 , stk11 apc ( ptc ) , hras , mutyh , pten ( ftc , ptc ) , ret ( mtc ) , wrn ( ftc , ptc ) abbreviations : ac , adenocarcinoma ; acc , adrenocorticocarcinoma ; all , acute lympocytic leukemia ; aml , acute myeloid leukemia ; bcc , basal cell carcinoma ; cel , chronic eosinophilic leukemia ; cll , chronic lymphocytic leukemia ; cmml , chronic myelomonocytic leukemia ; eoc , epithelial ovarian cancer ; erms , embryonal rhabdomyosarcoma ; ftc , follicular thyroid cancer ; gbm , glioblastoma multiforme ; gist , gi stromal tumor ; hb , hepatoblastoma ; hcc , hepatocellular carcinoma ; lam , lymphangioleiomyomatosis ; mds , myelodysplastic syndrome ; mel , melanoma ; mtc , medullary thyroid cancer ; nb , nephroblastoma ; nsclc , nonsmall - cell lung cancer ; pnet , pancreatic neuroendocrine tumors ; ppb , pleuropulmonary blastoma ; ptc , papillary thyroid cancer ; rcc , renal cell carcinoma ; scc , squamous cell carcinoma ; sccoht , small - cell carcinoma of the ovary , hypercalcemic type ; scst , sex cord stromal tumors ; sctat , sex cord tumors with annular tubules ; seb , sebaceous gland carcinoma ; sega , supependymal giant cell astrocytoma ; tcc , transitional cell carcinoma ; t - pll , t - cell prolymphocytic leukemia . clinical benet to the patient . 
testing relatives can help identify those at an increased risk of developing similar cancers ; however , a challenge to counseling still exists , because these variants lack the cohesive screening guidelines of their high - penetrance counterparts , and they may require a more individualized plan . 
differences between the number of genes currently tested in widely available germline panels , even compared with the number of genes linked to cancer predisposition as listed in table 2 , underscore the rapidly shifting understanding of clinically pertinent germline genes and the wide differences in opinion about what constitutes a clinically useful gene list . variants noted as rare ( labeled - r in table 2 ) are included for a more comprehensive guide to known germline - related malignancies . 
given the young age at which cancers develop in these patients or the other profound organ dysfunction associated with the respective syndromes , germline variants in such genes are unlikely to be carried through generations . furthermore , these syndromes often have clearly associated features that readily identify them clinically , and genetic testing only conrms a suspected diagnosis . 
one such example is wrn , the gene implicated in werner syndrome ; individuals with this disease display severe growth retardation , lipodystrophy , and progeria that would be obvious on examination . 
although familial inheritance of these genes has on occasion been described , such cases should be regarded as the rare exception rather than the rule . currently available somatic variant panels somatic variant panels test many more genes than their germline counterparts do . 
some prominent somatic tests are caris molecular intelligence ( caris life sciences , irving , tx ) , foundationone cdx ( foundation medicine , cambridge , ma ) , genpath onkosight ( genpath oncology , elmwood park , nj ) , msk - impact ( memorial sloan kettering cancer center , new york city , ny ) , omniseq comprehensive ( omniseq corporation , buffalo , ny ) , and tempus xt ( tempus labs , chicago , il )  . 
table 4 lists the number of genes in these somatic panels and the number of genes in each panel with germline implications ( according to table 2 ) at the time of publication . 
in general , a notable number of genes with germline implications are sequenced within common somatic panels . importantly , however , no somatic panel covers all known genes of germline importance , and sizeable numbers of cancer - susceptibility genes are excluded . currently available germline variant panels discussion several companies offer panels that test genes linked to hereditary cancer for various body systems . 
well - established companies with longer commercial track records include ambry genetics ( aliso viejo , ca ) , genedx ( gaithersburg , md ) , invitae ( san francisco , ca ) , and myriad genetics ( salt lake city , ut )  . 
criteria for inclusion of a company in this summary were a primary focus in commercial clinical laboratory improvement amendmentscertied germline testing and exclusion of direct - to - consumer testing or testing several cancer - related genes hold germline implications , and these genes are not uniformly included in currently available germline panel tests ( table 3 )  . 
given the state of current germline testing guidelines , which are syndrome based , and available commercial germline panels , which increasingly are organ - system based , a degree of disconnect between what is clinically relevant and what is offered with germline panels is to be expected . 
our group found that tumor sequencing had a notable number of potential germline variants and that referrals based on somatic variant sequencing could reveal otherwise unknown germline variants.22 within the 315 - gene panel used for the initial 222 - patient cohort , 41 genes ( 13% ) were classied as genes known to cause cancer susceptibility when mutated in the germline . 
coverage of genes within comprehensive or body systemspecic panel offerings from each major germline testing company ambry cancer type genedx invitae myriad * breast / gynecologic colorectal melanoma pancreatic prostate renal frequently somatically mutated in tumors , including tp53 , apc , and cdkn2a , were excluded , 91 patients ( 41% ) had a potential germline variant . 
twenty - three patients ( 10% ) were evaluated by genetics professionals ; three genetics referrals resulted directly from somatic testing results , which ultimately yielded one previously unknown germline variant . 
with formal integration of medical genetics into somatic testing review by the genomics tumor board at our institution , the overall percentage of referrals to genetics increased from 15% to 33% , and 41% of those referrals were the direct result of a somatic test review.23 in another study , speare et al24 reviewed 74 germline tests that followed identication of somatic variants in the tumor specimens of 54 patients and found that 10 variants ( 13.5% ) were conrmed in the germline . 
last , schrader et al25 surveyed germline variants in 187 genes that overlapped with a concurrent 341 - gene tumor somatic panel and identied pathogenic germline variants in 246 ( 15.7% ) of 1 , 566 patients . 
moreover , of the 198 individuals with variants in genes specically associated with increased cancer risk , only 81 of these germline changes ( 40.9% ) were concordant with the tumor type . 
that is , more than half of the patients who had pathogenic germline variants likely would not have had a recommendation for germline testing of that particular gene on the basis of their cancer type alone . 
in our own data , a high proportion of patients who were discovered by somatic tumor testing alone to carry a germline pathogenic variant ( ve of seven patients , or 71.4% ) did not meet any guidelinebased genetic testing criteria.23 together , these data demonstrate that somatic variant sequencing can inform germline testing and act as a screening tool for inherited germline carrier status , which suggests an additional clinical purpose for somatic variant testing separate from the intended goal of screening for possible targeted therapies . * myriad myrisk simultaneously tests 28 genes linked to hereditary cancers in various body systems . 
although some of these tests ask for blood or saliva samples and can test germline variants , they are primarily advertised as panels used to test tumor samples for somatic variants . abbreviation : mskcc , memorial sloan kettering cancer center . in a 1 , 000 - patient cohort with tumor and normal dna sequenced with a 202 - gene panel , meric - bernstam et al20 reported 43 patients ( 4.3% ) with potentially germline variants . 
more than half of these germline variantpositive individuals ( 101 patients ) would not have met guideline - based criteria for clinical germline testing . these studies add credence to the idea that the identication of germline variants from somatic testing can benet patients who would not otherwise have been identied by means of striking personal or family histories and would likely identify inherited cancer susceptibility in additional patients that targeted germline panel or syndrome testing alone may miss . although somatic variant testing can unearth germline variants that traditional means of screening have not , it is important to point out that some common types of germline variants are not picked up with the current technology used for somatic sequencing . 
large rearrangements , inversions , promoter variants , and pseudogene differentiation are not consistently addressed with current somatic sequencing . thus , a germline variant that involves a large rearrangement of brca or is within pms2 , which is notoriously difcult to distinguish from its pseudogene , may be missed these genes or misinterpreted despite the inclusion of within the somatic test panel.26 , 27 despite technical differences between germline and somatic testing , somatic sequencing still has promise as a clinically useful , but not independently adequate , tool for the screening of inherited cancer predisposition . 
somatic tumor sequencing may be considered additive to a proper family history and of particular utility in screening the subset of patients whose family or tumor histology would not otherwise meet traditional germline genetic testing criteria . tables 3 and 4 demonstrate the complexity of current offerings in germline and somatic variant testing . 
even within the category of commercial germline testing , the composition of clinically relevant genes within panels designed for the same organ ( eg , breast ) varies widely from company to company . 
these tables underscore the difculty of interpreting exactly which genes are clinically relevant , whether in a germline or somatic setting , and in some ways reect the issues of offering tests in a eld with a rapidly expanding knowledge base . 
correspondingly , one of the largest challenges in the writing of this review was the expansive and rapidly changing nature of both genes and tumors , which require multidisciplinary expertise and multiple revisions to interpret emerging data . although these tables are designed as a foundational primer specically for the oncologist and should serve well as a quick reference in clinic , the involvement of genetic counselors whenever available in the interpretation of germline implications of somatic testing and the orders for follow - up germline testing is recommended . in conclusion , although family history remains the most reliable screening tool for inherited cancer predisposition syndromes , several studies suggest that a clinically notable subset of germline carriers would be missed by family history alone . because limited family history or an incomplete gene penetrance can result in ambiguity , family historybased germline testing alone may be inadequate to completely assess a patients , and the familys , hereditary cancer risk . 
the plethora of cancer susceptibility genes tested in widespread somatic testing tumor panels makes incidental germline ndings likely , and numerous studies have conrmed that somatic testing can be a useful , but not fully adequate , screen for germline variants . 
sohal , pauline funchain collection and assembly of data : zade akras , brandon bungo , brandie h . leach , jessica marquard , manmeet ahluwalia , hetty carraway , davendra p.s. 
leach consulting or advisory role : invitae speakers ' bureau : myriad genetics references manmeet ahluwalia stock and other ownership interests : mimivax honoraria : prime oncology , elsevier , itamar medical ( i ) consulting or advisory role : monteris medical , astrazeneca , bristol - myers squibb , abbvie , cbt pharmaceuticals , kadmon , vbi vaccines research funding : novartis , tracon pharma , novocure , spectrum pharmaceuticals , lilly , imclone , boehringer ingelheim , astrazeneca hetty carraway consulting or advisory role : amgen , agios , myriad genetics , celgene speakers ' bureau : baxalta , celgene , novartis , jazz pharmaceuticals research funding : celgene travel , accommodations , expenses : celgene , agios , jazz pharmaceuticals , novartis , baxalta petros grivas consulting or advisory role : genentech , merck , bristol - myers squibb , astrazeneca , biocept , clovis oncology , emd serono , seattle genetics , foundation medicine , driver , pzer , qed therapeutics , heron speakers ' bureau : genentech , bristol - myers squibb research funding : mirati therapeutics ( inst ) , genentech ( inst ) , roche ( inst ) , merck ( inst ) , oncogenex ( inst ) , bayer ( inst ) , pzer ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) davendra p.s. 
sohal honoraria : foundation medicine consulting or advisory role : perthera research funding : novartis ( inst ) , celgene ( inst ) , oncomed ( inst ) , bayer ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) travel , accommodations , expenses : foundation medicine pauline funchain consulting or advisory role : eisai no other potential conicts of interest were reported stratton mr : exploring the genomes of cancer cells : progress and promise . 
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carlo mi , zhang l , mandelker d , et al : cancer predisposing germline mutations in patients ( pts ) with urothelial cancer ( uc ) of the renal pelvis ( r - p ) , ureter ( u ) and bladder ( b )  . 
catenacci dvt , amico al , nielsen sm , et al : tumor genome analysis includes germline genome : are we ready for surprises ? int j cancer 136 : 1559 - 1567 , 2015 16 . 
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klek s , heald b , milinovich a , et al : genetic counseling ( gc ) and germline ( gl ) testing rates after adoption of an integrated clinical cancer genetics ( ccg ) approach to genomics tumor board ( gtb )  . 
 e introducing the jco precision oncology molecular tumor board case discussion series see accompanying article doi : as the idea and application of precision oncology gains momentum among cancer practitioners , the need for evidence - based guidelines and expert opinions is essential . 
many challenges exist for implementing precision oncology , but knowledge gaps in the interpretation of cancer variants and off - label access to approved agents or experimental drugs in clinical trials are major barriers faced by medical oncologists . 
a cancer genome interpreter must deal with the huge amount of unstructured information on effectiveness of therapies matched to driver alterations that is being generated constantly by clinical trials and preclinical experiments . 
moreover , potential and confirmed germline genomic events identified during tumor and / or normal dna sequencing may pose significant challenges for oncologists who are not prepared to handle incidental findings that have therapeutic effect on the individual patient with cancer and clinical implications for at - risk family members . mtbs bridge this gap by facilitating the exchange of information among a wide range of experts ( eg , medical oncologists , cancer geneticists and biologists , molecular pathologists , genetic counselors , bioinformaticians ) who review patients medical histories and cancer genomic profiles to guide treatment options . 
ford research funding : myriad genetics ( inst ) , natera ( inst ) author affiliations and support information ( if applicable ) appear at the end of this article . corresponding author : james m . 
ford md , fasco , stanford university school of medicine , 1115 ccsr , 269 campus dr , stanford , ca 94305 ; e - mail : jmf@ stanford.edu. the following represents disclosure information provided by authors of this manuscript . 
others have an intermediate phenotype and are classified as glomus tumors of uncertain malignant potential ( gt - ump ) .3 herein , we present a case of an 18 - year - old patient with two glomus tumors involving the lateral and posterior cords of the right brachial plexus . 
physical examination demonstrated no neurologic deficit . imaging mr imaging of the right upper extremity demonstrated two distinct brachial plexus lesions , one emanating from the distal aspect of the lateral cord and the other from the posterior cord ( fig 1 )  . 
after extensive discussion with the neurosurgeon , the patient opted for surgical exploration with open biopsy and possible removal of the infraclavicular tumors to provide a histologic diagnosis and guidance on further management . intraoperative findings open exploration of the right infraclavicular brachial plexus was performed . 
these were gently mobilized but did not stimulate and were divided , allowing the lesion to be removed en bloc and sent for histopathological analysis . in the posterior cord region , the axillary nerve was clearly enlarged with tumor . 
 ( a ) on coronal fluid - sensitive magnetic resonance sequence through the chest , the right brachial plexus demonstrates asymmetric hyperintensity and thickening of the c5 , c6 , c7 , and t1 nerve roots and upper trunk ( not shown ) in addition to two discrete masses arising from the distal brachial plexus involving the posterior ( short arrow ) and lateral ( long arrow ) cords . 
 ( c ) on diffusion weighted imaging with apparent diffusion coefficient mapping , there is qualitative and quantitative restricted diffusion ( apparent diffusion coefficient [ adc ] values range from 0.6 to 1 103 mm2 / s in the larger mass and 0.9 to 1 103 mm2 / s in the smaller mass )  . 
on frozen section , this tumor appeared relatively benign , but given its widespread involvement with the axillary nerve , further aggressive dissection of the remaining tumor was deferred to avoid morbid neurologic deficits . histopathology and molecular analysis histopathologic analysis revealed a well circumscribed proliferation of relatively monomorphic cells with round nuclei and abundant eosinophilic cytoplasm ( figs 2a and 2b )  . 
mart1 was faint , caldesmon was focal , cd34 highlighted blood vessels , ini - 1 expression was intact , and ki - 67 proliferation index was mild to moderate . 
these findings together led to the diagnosis of malignant glomus tumor per current criteria.3 molecular genetic analysis using polymerase chain reactionbased sequencing of braf exon 15 revealed the braf v600e mutation at a mutant allele frequency of 40% . 
 to support this finding , we performed immunohistochemical analysis using antibodies directed against phosphoextracellular signal - regulated kinase ( erk ) ; this revealed variable immunostaining , with both cytoplasmic and nuclear immunoreactivity . 
in addition to isolated braf testing , a conventional cytogenetic analysis of the tumor revealed a normal 46 xx karyotype in all cells examined . therapeutic management management of this patients malignant tumor was discussed at the johns hopkins hospital multidisciplinary sarcoma tumor board . 
 ( a ) low - power view of glomus tumor associated with peripheral nerve fascicles , hematoxylin and eosin sta ( b ) tumor cells had ample eosinophilic cytoplasm and evident mitotic activity . 
mr imaging and 18f - fluorodeoxy - d - glucose positron emission tomographycomputed tomography obtained 2 weeks after the addition of trametinib demonstrated interval decrease in tumor size ( table 1 )  . 
 mr imaging at 3 and 6 months after initiating raf inhibitor therapy showed continued decrease in tumor size ( figs 3 and 4 ) and at 9 months showed no further change in size or imaging characteristics relative to most recent prior imaging . 
she experiences no pain , and the extremity function is normal . discussion the ras - raf - mek - erk signaling pathway is a frequent site of oncogenic mutations , with approximately 30% of human cancer harboring at least one mutation that results in its dysregulation . 
activating braf mutations are found in approximately 7% of cancers , roughly half of malignant melanomas , 5 and in other tumors , including colorectal , ovarian , papillary thyroid , and nonsmall - cell lung cancers , gliomas , and histiocytic disorders.6 - 12 the most common mutation , v600e , results in constitutive activation of the erk pathway . small molecule inhibitors of raf kinase were first studied in clinical trials of patients with melanoma . 
to determine whether the benefit of targeted raf inhibition would extend to nonmelanoma tumors with braf v600e , a phase ii basket trial explored the use of vemurafenib in patients selected for this mutation . 
this study demonstrated modest antitumor activity , although not all tumors with braf mutation responded , thus enforcing that a single driver oncogene may be associated with a nonuniform response to targeted therapy.16 braf mutations also occur rarely in a wide spectrum of cancers , including 1.4% of soft tissue sarcomas.17 a single patient with braf - mutated clear cell sarcoma was treated in the vemurafenib basket trial and sustained a partial response.16 the role of raf inhibitors in other sarcomas , however , has not been explored . glomus tumors are mesenchymal neoplasms that are rare and generally benign.18 they can occur as solitary or multiple soft tissue tumors and are most commonly located on the digits , supporting early hypotheses about their origin in the temperature - sensing glomus body . 
in a targeted sequencing analysis , three of 28 glomus tumors were found to harbor braf v600e mutations and a single tumor mutation in kras.19 a single case of a glomus tumor of the median nerve was found by next - generation sequencing to harbor a braf v600e mutation.20 this patient , and those in the retrospective analysis of 28 cases , was treated surgically without consideration for systemic therapy . 
finally , in a collection of 102 glomus tumors ( 56% benign , 15% gt - ump , and 29% malignant ) braf v600e mutation was detected in six tumors ( 6% ) , all of which were classified as either malignant glomus tumor or gt - ump ( and 0 of 57 benign glomus tumors harbored braf mutations ) .21 these data , although reflective of an overall small sample size , are suggestive of braf mutation as a predictor of more aggressive clinical behavior . 
 interestingly , glomus tumor has previously been associated with neurofibromatosis type 1 , 22 suggesting a shared terminal event in activation of erk signaling in these tumors . our patients response to targeted braf inhibition is an extraordinary one and highlights promise for future use in sarcomas with this mutation . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . andrea cuviello no relationship to disclose aviad zick research funding : merck ( inst ) , eli lilly ( inst ) shivani ahlawat no relationship to disclose fausto j . 
folpe al , fanburg - smith jc , miettinen m , et al : atypical and malignant glomus tumors : analysis of 52 cases , with a proposal for the reclassification of glomus tumors . 
kimura et , nikiforova mn , zhu z , et al : high prevalence of braf mutations in thyroid cancer : genetic evidence for constitutive activation of the ret / ptc - ras - braf signaling pathway in papillary thyroid carcinoma . 
mcarthur ga , chapman pb , robert c , et al : safety and efficacy of vemurafenib in braf ( v600e ) and braf ( v600k ) mutation - positive melanoma ( brim - 3 ) : extended follow - up of a phase 3 , randomised , open - label study . 
hauschild a , grob jj , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
dahlin lb , scherman p , besjakov j , et al : intraneural glomus tumor of uncertain malignant potential and with braf mutation in the median nerve an unusual case . 
karamzadeh dashti n , bahrami a , lee sj , et al : braf v600e mutations occur in a subset of glomus tumors , and are associated with malignant histologic characteristics . 
dahlin lb , mller g , anagnostaki l , et al : glomus tumours in the long finger and in the thumb of a young patient with neurofibromatosis - 1 ( nf - 1 )  . 
i believe there are two other important aspects of the us food and drug administration ( fda ) approval not mentioned in her editorial . first , haraldsdottir described this as fda approval , although in fact this was an fda accelerated approval . 
as a result , the fda requires the sponsor to do additional studies involving patients with different tumor types.2 the different tumor types studied should be tumors derived from different tissues , and studies should include dmmr / msi - h tumors derived from the same tissue of origin to determine whether additional molecular markers might predict which patients with dmmr / msi - h tumors are among the roughly 40% of patients whose tumors do respond or the 60% of patients whose dmmr / msi - h tumors do not respond to pembrolizumab . 
seventy - eight percent of the roughly 40% of patients whose tumors responded to pembrolizumab in the key study were still responding or had stable disease for at least 6 months from the initiation of pembrolizumab.2 the likelihood of durable responses among responders to checkpoint inhibitors does seem to distinguish the benefit of these drugs from that typically seen in patients responding to chemotherapy . 
other molecular markers harbored in dmmr / msi - h tumors might further distinguish which patients with dmmr / msi - h tumors are more likely to have durable responses . biomarkers have long been used as predictors of response to specific therapies . 
 targeted therapy for colorectal cancers with non - v600 braf mutations : perspectives for precision oncology braf mutations are found in up to 10% of colorectal cancers ( crc )  . 
it has been established that braf v600e mutations in crc predict unresponsiveness to epidermal growth factor receptor ( egfr ) inhibitioncetuximab and / or panitumumabas a result of the constitutive activation of the mitogen - activated protein kinase pathway downstream of egfr signaling . 
in many instances , clinicians may be hesitant to use egfr inhibitors for these patients , as it is largely assumed that tumors with non - v600 braf mutations activate the mitogen activated protein kinase pathway in a similar manner to ras or braf v600e mutations and would therefore be equally refractory to egfr inhibition ; however , the evidence that currently exists to substantiate this claim is mixed and incomplete . 
preclinical data and several case reports suggest that a subset of braf non - v600 mutations that impair the protein 's kinase activity may in fact confer heightened sensitivity to egfr inhibition because of dependency on upstream receptor tyrosine kinase signaling . 
 ( a ) in braf wild - type ( wt ) tumors , braf signals downstream from receptor tyrosine kinases ( rtks ) and ras as a dimer with braf or craf . 
it signals downstream to mitogen - activated protein kinase kinase 1 / 2 ( mek1 / 2 ) and extracellular regulated kinase 1 / 2 ( erk1 / 2 ) , sustaining cell survival and proliferation . 
for this reason , targeting them with egfr and mek inhibitors is the optimal combination of approved agents , but may be improved upon with the development of next - generation pan - raf and erk inhibitors . 
jones et al2 identified an impressive cohort of 208 patients with braf non - v600 mutant crc , which accounted for 2.2% of patients in their crc cohort and 22% of patients with braf mutations . 
among non - v600 mutants , class ii mutations were found in eight patients ( 22% of non - v600 mutants ) , class iii mutations in 17 patients ( 46% ) and unknown braf mutations in 12 patients ( 32% )  . 
it is likely that the prevalence of non - v600 mutants compared with v600e braf mutants is overestimated in this population because braf v600e is associated with microsatellite instability high ( msi - h ) tumor status.4 together , these data imply that non - v600 braf mutations are present in 2% to 3% of crc , which makes them more prevalent than was previously speculated.29 in addition to the prevalence of non - v600 mutations in crc , these studies also revealed important insights into the characteristics of patients with braf mutant crc . 
braf v600 mutant tumors are commonly right sided , of high clinical grade , msi - h , and experience inferior survival compared with both braf wild - type and non - v600 mutants.2 , 4 , 30 meanwhile , braf non - v600 mutant tumors tend to be found in younger patients with left - sided disease who experience a more indolent disease course than patients with either braf v600e or braf wild - type mutant tumors.2 , 30 these data clearly segregate braf v600 and non - v600 mutant tumors as distinct clinical entities . 
while jones et al2 did not observe differences between class ii and class iii mutants in these characteristics , results from yaeger et al4 suggest that class ii mutants may cluster more closely with class i mutants than class iii mutants as a result of their common right - sided frequency and mutual exclusivity from complimentary genetic lesions in the mapk pathway . 
 this result was underwhelming compared with the response rates observed in patients with melanoma and later with nonsmall - cell lung cancer.37 , 39 a subsequent study evaluated combined inhibition of brafvemurafeniband egfr panitumumabfor the treatment of patients with braf v600e mutant crc . 
the results of this trial showed modest efficacy for a small number of patients , with responses seen in two of 15.40 similar response rates were observed in braf plus egfr inhibited arms of more recent trials . 
encorafenib and cetuximab elicited responses in 19% of patients , 41 whereas 10% of dabrafeniband panitumumab - treated patients experienced a response.42 given that braf v600e is a strong predictor of nonresponsiveness to egfr inhibition , 10 , 43 - 45 these studies are successful in demonstrating that braf inhibition can sensitize braf v600e crc to egfr inhibitors . 
however , it is clear that this strategy is still insufficient at effectively inhibiting the mapk pathway and achieving responses in a majority of patients . safety lead - in data from 30 patients in an ongoing clinical trial using encorafenib ( braf inhibitor ) , binimetinib ( mek inhibitor ) , and cetuximab ( egfr inhibitor ) indicate the strongest results with targeted therapy for braf v600e crc thus far , achieving response rates of 48%.46 this is in contrast with a completed study by corcoran et al42 that used dabrafenib ( braf inhibitor ) , trametinib ( mek inhibitor ) , and panitumumab ( egfr inhibitor ) which only achieved a response rate of 21% . 
whereas it is difficult to make cross - study comparisons , both studies had similar patient characteristics , which makes it possible to speculate that this large discrepancy between trials comes from differences between the drugs themselves . 
panitumumab and cetuximab are considered similarly effective agents , and different mek inhibitors have been shown to be highly similar mechanistically.47 , 48 for this reason , the differences between encorafenib and dabrafenib may account for the improved outcomes in the beacon safety lead - in data . 
in braf class i mutant metastatic melanoma , treatment with encorafenib plus binimetinib has produced higher response rates and progression - free survival compared with what has been previously reported with dabrafenib plus trametinib.49 this suggests that these new agents may be superior in their ability to sustain the inhibition of the mapk pathway in braf v600e mutant cells . 
 this approach is currently under exploration in melanoma.64 , 65 given that combinations of targeted therapies are beginning to elicit encouraging responses in braf v600 mutant microsatellite stable crc , additional studies that explore novel combinations are expected to continue . 
additional preclinical studies that explore patient - derived crc cell lines and xenografts may help to determine which , if any , of the nonv600 braf mutations confer increased sensitivity to egfr inhibition . 
 important areas of preclinical research include understanding the oncogenic potential of these mutations to assign them to class ii , class iii , or as passenger mutations of no significance . as the development of novel targeted agents , such as erk inhibitors and next - generation raf inhibitors , reach clinical trials , it will be important to assess their potential for patients with crc with non - v600 braf mutations . 
furthermore , preclinical research in understanding the mechanisms that underlie co - occurrence of non - v600 braf mutations with other lesions in the mapk pathway may provide important insights into the pathogenesis and vulnerabilities of these tumors . 
as the field refines targeted therapies for braf v600e crc , it is likely that more effective treatment strategies will become understood and available for crc with non - v600 braf mutations . 
seligmann jf , fisher d , smith cg , et al : investigating the poor outcomes of braf - mutant advanced colorectal cancer : analysis from 2530 patients in randomised clinical trials . 
shitara k , yonesaka k , denda t , et al : randomized study of folfiri plus either panitumumab or bevacizumab for wild - type kras colorectal cancer - wjog 6210g . 
de roock w , claes b , bernasconi d , et al : effects of kras , braf , nras , and pik3ca mutations on the efficacy of cetuximab plus chemotherapy in chemotherapy - refractory metastatic colorectal cancer : a retrospective consortium analysis . 
shinozaki e , yoshino t , yamazaki k , et al : clinical significance of braf non - v600e mutations on the therapeutic effects of anti - egfr monoclonal antibody treatment in patients with pretreated metastatic colorectal cancer : the biomarker research for anti - egfr monoclonal antibodies by comprehensive cancer genomics ( breac ) study . 
shen y , wang j , han x , et al : effectors of epidermal growth factor receptor pathway : the genetic profiling of kras , braf , pik3ca , nras mutations in colorectal cancer characteristics and personalized medicine . 
corcoran rb , ebi h , turke ab , et al : egfr - mediated re - activation of mapk signaling contributes to insensitivity of braf mutant colorectal cancers to raf inhibition with vemurafenib . 
herr r , halbach s , heizmann m , et al : braf inhibition upregulates a variety of receptor tyrosine kinases and their downstream effector gab2 in colorectal cancer cell lines . 
planchard d , kim tm , mazieres j , et al : dabrafenib in patients with braf ( v600e ) - positive advanced nonsmall - cell lung cancer : a single - arm , multicentre , open - label , phase 2 trial . 
cremolini c , di bartolomeo m , amatu a , et al : braf codons 594 and 596 mutations identify a new molecular subtype of metastatic colorectal cancer at favorable prognosis . 
schirripa m , biason p , cortiula f , et al : clinico - pathological and molecular characterisation of braf mutant metastatic colorectal cancer ( mcrc ) : are all mutations created equal ? j clin oncol 36 : 3590 , 2018 ( suppl ) 32 . 
planchard d , besse b , groen hjm , et al : dabrafenib plus trametinib in patients with previously treated braf ( v600e ) - mutant metastatic nonsmall - cell lung cancer : an open - label , multicentre phase 2 trial . 
van geel rmjm , tabernero j , elez e , et al : a phase ib dose - escalation study of encorafenib and cetuximab with or without alpelisib in metastatic braf - mutant colorectal cancer . 
guren tk , thomsen m , kure eh , et al : cetuximab in treatment of metastatic colorectal cancer : final survival analyses and extended ras data from the nordic - vii study . 
price tj , peeters m , kim tw , et al : panitumumab versus cetuximab in patients with chemotherapy - refractory wild - type kras exon 2 metastatic colorectal cancer ( aspecct ) : a randomised , multicentre , open - label , non - inferiority phase 3 study . 
dummer r , ascierto pa , gogas hj , et al : encorafenib plus binimetinib versus vemurafenib or encorafenib in patients with braf - mutant melanoma ( columbus ) : a multicentre , openlabel , randomised phase 3 trial . 
niessner h , sinnberg t , kosnopfel c , et al : braf inhibitors amplify the pro - apoptotic activity of mek inhibitors by inducing er stress in nras - mutant melanoma . 
pietrantonio f , oddo d , gloghini a , et al : met - driven resistance to dual egfr and braf blockade may be overcome by switching from egfr to met inhibition in braf - mutated colorectal cancer . 
ahronian lg , sennott em , van allen em , et al : clinical acquired resistance to raf inhibitor combinations in braf - mutant colorectal cancer through mapk pathway alterations . 
sinicrope fa , mahoney mr , smyrk tc , et al : prognostic impact of deficient dna mismatch repair in patients with stage iii colon cancer from a randomized trial of folfox - based adjuvant chemotherapy . 
tran b , kopetz s , tie j , et al : impact of braf mutation and microsatellite instability on the pattern of metastatic spread and prognosis in metastatic colorectal cancer . 
overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - deficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
donia m , fagone p , nicoletti f , et al : braf inhibition improves tumor recognition by the immune system : potential implications for combinatorial therapies against melanoma involving adoptive t - cell transfer . 
hu - lieskovan s , mok s , homet moreno b , et al : improved antitumor activity of immunotherapy with braf and mek inhibitors in braf ( v600e ) melanoma . 
sullivan rj , gonzalez r , lewis kd , et al : atezolizumab ( a ) + cobimetinib ( c ) + vemurafenib ( v ) in brafv600 - mutant metastatic melanoma ( mel ) : updated safety and clinical activity . 
miller wh , kim tm , lee cb , et al : atezolizumab ( a ) + cobimetinib ( c ) in metastatic melanoma ( mel ) : updated safety and clinical activity . 
bahadoran p , allegra m , le duff f , et al : major clinical response to a braf inhibitor in a patient with a braf l597r - mutated melanoma . 
noeparast a , teugels e , giron p , et al : non - v600 braf mutations recurrently found in lung cancer predict sensitivity to the combination of trametinib and dabrafenib . 
sullivan rj , infante jr , janku f , et al : first - in - class erk1 / 2 inhibitor ulixertinib ( bvd - 523 ) in patients with mapk mutant advanced solid tumors : results of a phase i dose - escalation and expansion study . 
de roock w , de vriendt v , normanno n , et al : kras , braf , pik3ca , and pten mutations : implications for targeted therapies in metastatic colorectal cancer . 
hampson , phd1 ; bjoern bornkamp , phd1 ; antonella maniero , msc2 ; frank bretz , phd1 ; and emmanuel zuber , phd1 the diversity of patient journeys can raise fundamental questions regarding the evaluation of drug effects in clinical trials to inform clinical practice . 
when dening the treatment effect of interest in a trial , the researcher needs to account for events occurring after treatment initiation , such as the start of a new therapy , before observing the end point . 
this estimand framework provides a structured approach to discuss how to account for intercurrent events that occur after random assignment and may affect the assessment or interpretation of the treatment effect . 
on the basis of the patients clinical and pathologic ndings , he is offered entry into a randomized trial of a new drug plus standard - of - care therapy ( soc ) versus soc alone . 
the examples provided earlier include discontinuation of treatment as a result of an adverse reaction , start of a new anticancer regimen before observing the end point of interest ( eg , progression - free survival [ pfs ] or overall survival [ os ] ) , or death of a patient while on treatment . some of these events may reect a desired or undesired activity of the treatment , which is not directly captured by the end point ; some may prevent observation of the end point ; and still others may complicate interpretation of the end point . 
 degtyarev et al context key objective a clinical researcher is confronted with unique challenges when dening the treatment effect of interest in oncology clinical trials as a result of the diversity of patient journeys . 
in this article , the relationship between patient journeys and treatment effects is highlighted , and it is illustrated how the newly introduced estimand framework can structure discussions among interdisciplinary teams regarding the design and interpretation of oncology trials . knowledge generated the estimand framework facilitates a precise denition of the scientic question of interest accounting for different patient journeys . 
all parties involved in the design of clinical trials need to consider how to dene the treatment effect of interest in the study population , along with the relevant end point and data analysis , to adequately address the trial objective in the presence of intercurrent events . understanding the treatment effect measured in a clinical trial will be important for oncologists so that they can make informed treatment decisions . the international council for harmonization of technical requirements for pharmaceuticals for human use ( ich ) aims to align the development of new medicinal products in europe , japan , and the united states . 
the ich e9 note for guidance focuses on the design , conduct , analysis , and reporting of conrmatory clinical trials . however , there is a growing awareness that an imprecise denition of the scientic question of the trial may create a misalignment between its objectives and analysis and confuse its interpretation . 
in response to this , in 2017 , the ich released a draft addendum1 to its e9 guideline.2 this proposes a structured framework for clinical researchers to better align trial objectives , design , analysis , and interpretation , in view of the diversity of patient journeys and intercurrent events . 
the addendum introduces the concept of an estimand to precisely describe the treatment effect of interest in terms of the following four attributes : the target population ; the end point ( or variable ) to be obtained for each patient ; a specication of how to account for intercurrent events ; and a population - level summary for the variable , such as the hazard ratio for pfs . these four attributes are always interlinked . 
for those three patients , events occurring after random assignment either prevent the observation of the end point ( patient 2 : how long would the pfs be otherwise ? ) or raise important questions on its interpretation ( patient 1 : is the observed pfs a result of the effect of the investigational treatment or of the new therapy ? patient 2 : is the withdrawal of consent indicative of any treatment effect ? patient 3 : is death a random event , or is it indirectly related to the disease or treatment ? )  . 
eot , end of treatment ; soc , standard of care . a change in anticancer treatment reect the reality of clinical practice , including the possible impact of the investigated treatment on the choice or activity of subsequent therapies . 
for example , estimand 3 ( table 1 ) targets the effect of the studied treatment on pfs as if no alternative therapy existed ( ie , excluding its possible impact )  . 
this has implications for how we dene the end point , as well as how we collect and analyze the data . for example , for estimands 2 and 3 , collection of tumor assessments after the start of new therapy is not required , whereas this is necessary for estimand 1 . 
the choice of the estimand will be informed by discussions between all parties involved in the clinical trial , the disease cluding sponsor and regulators , about setting , the anticipated mode of action of the treatment , and the relevance of intercurrent events . example with os table 1 lists the four attributes ( population , end point , intercurrent events , and summary ) of several estimands for the lung cancer trial , each of which is dened with a pfs end point . 
it is interesting to further illustrate how the estimand framework can accommodate a patients journey when os ( ie , time to all - cause mortality ) is the end point of interest . 
how the treatment effect denition drives the choice of end point and handling of an intercurrent event in the estimand framework for the lung cancer trial example attributes of the estimand description per ich e9 addendum estimand 3 estimand 2 estimand 1 population variable ( end point ) intercurrent event : start new therapy population - level summary prolonging time to progression or death prolonging time to progression , death , or new therapy prolonging time to progression or death if new therapy is not initiated because none is available population according to targeted indication pfs based on progression death as event new time to event end point considering progression , death , or new therapy as event pfs based on progression or death as event treatment policy composite hypothetical hazard ratio note . 
the intercurrent event addressed here is the start of a new anticancer therapy before the assessment of tumor progression ( as illustrated by patient 1 in fig 1 )  . 
the treatment policy strategy ignores the event , and the end point is expected to be assessed and analyzed regardless of its occurrence ; traditionally , this was addressed in the analysis by not censoring observations at the start of new therapy . 
the estimand framework allows clarication of how different choices of strategy to account for intercurrent events affect the end point denition , assessment , and analysis , and consequently , the interpretation of trial results with respect to the treatment effect of interest . 
note that in all three estimands , the intercurrent event of death ( as for patient 3 in fig 1 ) is incorporated in the variable using a composite strategy . abbreviations : ich , international council for harmonization of technical requirements for pharmaceuticals for human use ; pfs , progression - free survival . if one assumes that patient journeys observed in the trial after treatment discontinuation reect real - world clinical practice , the treatment effect of interest can be dened as follows : does the investigational treatment prolong survival compared with soc , regardless of treatment discontinuation ? this reects a treatment policy strategy for handling intercurrent events such as the start of new therapy . 
this denes the estimand typically used with os in oncology trials . however , it is debatable whether this estimand with os always yields a clinically meaningful comparison of treatments , in particular if the assumption that subsequent new therapies reect that clinical practice is violated . 
even if it does become available ( eg , after regulatory approval based on pfs results ) , the investigational treatment would likely be used in lieu of soc , rather than after disease progression on soc . 
a similar situation arises when patients randomly assigned to soc have access , upon tumor progression , to other therapies outside the trial with the same mechanism of action ( moa ) as the investigational treatment . 
 estimands and the patient journey example in the adjuvant treatment setting a 70 - year - old woman with a 2.0 - cm adenocarcinoma of the breast and no involved lymph nodes comes to her oncologist for treatment . 
in her seventh year after random assignment , the patient dies from complications after a myocardial infarction . the scientic question of interest in this adjuvant trial is whether the new treatment prolongs patients disease - free survival time . 
should the appearance of a contralateral breast cancer be considered as disease recurrence ? and what about another primary cancer or death not related to breast cancer ? such discussions may further rene the scientic question . 
for example , the researcher may choose between the following three questions to dene the objective of this trial : does the drug delay relapse , secondary malignancy , or death from any cause ? does the drug delay relapse or death from any cause ? does the drug delay relapse or disease - related death ? the choice of scientic question should be informed by a treatments moa and the specic disease setting . 
for instance , published data suggest that adjuvant hormone therapies for breast cancer may effectively reduce the risk of contralateral breast cancer but increase the risk of other primary malignancies.14 - 16 therefore , in this setting , the effect of treatment on the risk of developing these secondary malignancies seems to be relevant . 
consequently , the composite strategy could be applied to include these secondary malignancies in the denition of the end point . the researcher would select the rst question ( does the drug delay relapse , secondary malignancy , or death from any cause ? ) as the primary treatment effect of interest for the study . such discussions are not new in oncology , and efforts have been undertaken in the adjuvant setting to standardize end points and handle intercurrent events without using the ich e9 terminology . 
hudis et al8 ( p2127 ) noted that standardized denitions of breast cancer clinical trial end points must be adopted to permit the consistent interpretation and analysis of breast cancer clinical trials and to facilitate cross - trial comparisons and meta - analyses . 
recommendations for breast cancer were provided as part of the denition for the assessment of time - to - event end points in cancer trials initiative , further distinguishing between different types of relapses and secondary malignancies.17 the authors also recognized that handling intercurrent events differently may require new end points . 
alternatively , she could receive an investigational personalized therapy , a chimeric antigen receptor t - cell therapy ( car - t ) , currently approved to treat patients with diffuse large b - cell lymphoma in a later setting.18 , 19 the oncologist anticipates the different journeys this patient could encounter on each of the treatment options . if the patient is to receive soc , she will initially receive salvage chemotherapy . 
the best soc therapy after rituximab plus cyclophosphamide , doxorubicin , vincristine , and prednisone is high - dose chemotherapy followed by asct for patients who achieve a deep remission on salvage chemotherapy . 
if a deep remission is not obtained after two to three cycles of a rst salvage chemotherapy ( approximately 6 weeks ) , the patient will receive a new salvage therapy ( second salvage ) , still with the goal to achieve a deep remission and subsequently receive transplantation . 
in this situation , the car - t therapy could be offered because it is approved in this later setting . alternatively , the patient may receive car - t immediately , as an experimental option in this earlier setting . 
she might then require chemotherapy to control the disease and prevent rapid progression ( bridging chemotherapy ) during the approximate 4 to 6 weeks required to manufacture and deliver the car - t therapy to the clinic . 
however , in general and in contrast with the administration of asct in the soc option , tumor response or progression before cart infusion is not relevant for the administration of car - t and , at this stage , would not constitute a nal outcome for the patient . 
if there is no improvement of disease after approximately 12 weeks into the journey , then the strategy of car - t administration would be deemed to have failed , and other treatment options would need to be considered . adopting now the perspective of the researcher who wants to compare both options in a randomized clinical study , a review of the different patient journeys just described raises a number of challenges to identify the adequate research question and the treatment effect of interest for this trial . 
those challenges that need to be addressed to design a study enabling a scientically sound and interpretable comparison are as follows . first , the therapies to be compared represent two treatment strategies , not simply two different treatments . 
during the manufacturing period , patients may take bridging therapy . their tumor may progress or respond to the bridging therapy , but the tumor response status before car - t infusion is not relevant for the initiation of car - t . 
therefore , the treatment effect of the car - t strategy relative to the soc strategy is not expected to manifest fully during the waiting period . finally , car - t may be administered after failure of the soc treatment strategy . 
for patients receiving the soc treatment strategy , once two lines of salvage therapy have failed to be effective , patients become eligible to receive the car - t therapy , which has already been approved in that setting . 
this means that the patient outcome observed afterward in the soc treatment group may not reect the effect of the soc strategy alone , but also the effect of this crossover . the estimand framework helps to address the challenges raised by the complexity of patient journeys on both arms . 
the researcher will be able to give a more precise description of the treatment effect of interest using the language offered by the estimand framework , starting with the two treatment strategies to be a description of compared . treatment strategies to be compared the study could evaluate the effect of car - t against asct administration only , focusing on the possibly curative component of each treatment strategy . 
this would ideally be studied by randomly assigning patients only when they would be ready for both the administration of car - t ( ie , after successful car - t manufacturing ) and asct ( ie , after reaching a sufcient remission from salvage therapy )  . 
in this case , patients would be randomly assigned to receive either car - t or asct , with all necessary preparatory steps in their therapeutic journey being part of a common run - in phase before random assignment . however , the population for the comparison would then constitute only a subset of the population initially considered eligible to receive the car - t or soc treatment strategies . 
this would not address the following scientic question of interest : what is the relative clinical benet across the entire patient journey once a car - t or soc treatment strategy is prescribed ? therefore , it seems of interest to compare the entirety of both treatment strategies instead , including all possible paths as dened in the patient journeys . 
this also corresponds to clinical practice , where not all patients will receive all components of the treatment . population aligned with the denition of the treatment strategies described earlier , the population of interest includes all patients eligible to receive either car - t or soc treatment strategies , to be further specied with adequate inclusion and exclusion criteria . variable typically in this disease setting , the primary variable , or end point , is event - free survival ( efs ) , representing the time from random assignment to failure of the treatment strategy . 
intercurrent events affecting the comparison of the treatment strategies , with their respective handling strategy intercurrent event handling strategy justication manufacturing failure in car - t arm or failing treatment policy intrinsic to treatment strategy : those events to receive asct in soc arm reect the clinical reality of the treatment strategy new cancer therapy before observing efs event hypothetical not part of treatment strategy , and affecting the sd / pd at week 6 treatment policy observation and interpretation of further assessments does not reect an outcome of treatment strategy ; only used for treatment decision in soc arm ; not used for car - t arm abbreviations : asct , autologous stem - cell transplantation ; car - t , chimeric antigen receptor t - cell therapy ; efs , event - free survival ; pd , progressive disease ; sd , stable disease ; soc , standard of care . constitute a failure of a treatment strategy if observed at or after the week 12 assessment . 
however , death represents the most informative and denitive outcome of either treatment strategy , which can be observed regardless of when it occurs . new cancer therapy started before observing efs event . 
if a patient takes an unplanned anticancer therapy before his or her assigned treatment strategy reaches failure , it will be difcult to interpret the outcome as reecting the effect of that treatment strategy . 
this intercurrent event can be handled using the hypothetical strategy ( ie , to evaluate the effect had patients not been offered such an alternative treatment )  . insufcient remission ( stable disease or progressive disease ) at week 6 . 
they are ignored , following the treatment policy strategy , as reected in the variable denition . intercurrent events table 2 lists the intercurrent events affecting the comparison of the two treatment strategies and the estimand strategy used to handle each of them . summary measure manufacturing failure in the car - t arm or failing to receive asct in the soc arthe patient may not receive the nal treatment ( car - t infusion or asct ) as a result of the nature of both treatment strategies . 
following the treatment policy strategy , such events should be ignored , and patients should still be observed until the nal event of interest . the summary measure often used to quantify the relative treatment effect on efs in a randomized study is the hazard ratio . 
in addition , both car - t and asct are population variable ( cid : 129 ) patients with dlbcl who have experienced relapse or are refractory after first - line therapy ( cid : 129 ) event - free survival with sd / pd on or after week 12 or death at any time as event treatment strategies ( cid : 129 ) soc : salvage therapy followed by asct ( cid : 129 ) car - t : optional bridging therapy and lymphodepleting therapy followed by car - t infusion ( cid : 129 ) hazard ratio summary measure ( cid : 129 ) failure / delay to receive final treatment ( cid : 129 ) sd / pd at week 6 ( cid : 129 ) new therapy intercurrent events fig 2 . 
in the soc arm , patients receive up to two salvage chemotherapies , with the aim to receive autologous stem - cell transplantation ( asct ) when disease responds to chemotherapy . 
if no sufcient response to the rst round of chemotherapy is achieved in soc patients , car - t is manufactured in parallel to the patient receiving a new round of chemotherapy . 
birc , blinded independent review committee ; cr , complete response ; lymphoma ; pd , progressive disease ; pet , positron ct , computed tomography ; dlbcl , diffuse large b - cell emission tomography ; pr , partial response ; r , random assignment ; sd , stable disease . potentially curative therapies , and hence , a proportion of patients may have a similar outcome when they are cured . 
alternative summary measures to quantify treatment effects in the presence of nonproportional hazards are currently being investigated.20 - 22 having dened the treatment strategies to be compared , together with the four other attributes of the primary estimand , as summarized in figure 2 , the study design presented in figure 3 could be proposed . conclusion patients with cancer experience different journeys , and researchers need to account for this diversity when dening the treatment effect of interest in a clinical trial . 
various events occurring after random assignment may affect the assessment and interpretation of the treatment effect of interest . the estimand framework provides a structured approach to transparently discuss and account for different patient journeys . 
identifying an estimand leads to a precise denition of the scientic question of interest and to tailored study designs and data analyses.23 , 24 experience with the estimand framework in clinical research is still limited , 25 and its use in oncology is being explored in dedicated regulatory and industry forums and working groups . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . evgeny degtyarev employment : novartis stock and other ownership interests : novartis yiyun zhang employment : novartis kapildeb sen employment : novartis stock and other ownership interests : novartis david lebwohl employment : novartis , semma therapeutics stock and other ownership interests : novartis , semma therapeutics expert testimony : novartis mouna akacha employment : novartis stock and other ownership interests : novartis lisa v . 
hampson employment : novartis , astrazeneca stock and other ownership interests : novartis bjoern bornkamp employment : novartis stock and other ownership interests : novartis , alcon travel , accommodations , expenses : novartis antonella maniero employment : novartis , bristol - myers squibb stock and other ownership interests : novartis , bristol - myers squibb travel , accommodations , expenses : novartis frank bretz employment : novartis stock and other ownership interests : novartis travel , accommodations , expenses : novartis emmanuel zuber employment : novartis , novartis ( i ) stock and other ownership interests : novartis , alcon , air liquide , novartis ( i ) , alcon ( i ) travel , accommodations , expenses : novartis , novartis ( i ) no other potential conicts of interest were reported . acknowledgment we thank aby buchbinder for his enlightening critical review of the rst version of this article . 
we are indebted to ying lu , md , and jack lee , md , for inviting us and gratefully appreciate the opportunity to contribute this review article . references international council for harmonization of technical requirements for pharmaceuticals for human use : e9 ( r1 ) draft guideline : estimands and sensitivity analysis in clinical trials . 
international council for harmonization of technical requirements for pharmaceuticals for human use : e9 guideline : statistical principles in clinical trials . rubach k : treatment effect quantication for time - to - event endpoints : estimands , analysis strategies , and beyond . 
pharm stat 18 : 145 - 165 , 2019 bengoudifa b - r , weber h , gathmann i , et al : estimand framework in aml based on a randomized , placebo - controlled , phase 3 study investigating the effect of adding midostaurin to standard chemotherapy in patients with newly diagnosed aml without a flt3 mutation . 
j clin oncol 27 : 2874 - 2880 , 2009 korn el , freidlin b , abrams js : overall survival as the outcome for randomized clinical trials with effective subsequent therapies . 
j clin oncol 29 : 2439 - 2442 , 2011 saad ed , buyse m : overall survival : patient outcome , therapeutic objective , clinical trial end point , or public health measure ? j clin oncol 30 : 1750 - 1754 , 2012 8 . 
hudis ca , barlow we , costantino jp , et al : proposal for standardized denitions for efcacy end points in adjuvant breast cancer trials : the steep systej clin oncol 25 : 2127 - 2132 , 2007 larkin j , minor d , dangelo s , et al : overall survival in patients with advanced melanoma who received nivolumab versus investigators choice chemotherapy in checkmate 037 : a randomized , controlled , open - label phase iii trial . 
rittmeyer a , barlesi f , waterkamp d , et al : atezolizumab versus docetaxel in patients with previously treated non - small - cell lung cancer ( oak ) : a phase 3 , open - label , multicentre randomised controlled trial . 
reck m , rodr guez - abreu d , robinson ag , et al : treatment switchingadjusted overall survival ( os ) in keynote - 024 : first - line pembrolizumab versus chemotherapy in patients with advanced non - small cell lung cancer ( nsclc )  . 
sternberg cn , hawkins re , wagstaff j , et al : a randomised , double - blind phase iii study of pazopanib in patients with advanced and / or metastatic renal cell carcinoma : final overall survival results and safety update . 
motzer rj , escudier b , oudard s , et al : phase 3 trial of everolimus for metastatic renal cell carcinoma : final results and analysis of prognostic factors . 
goss pe , ingle jn , martino s , et al : a randomized trial of letrozole in postmenopausal women after ve years of tamoxifen therapy for early - stage breast cancer . 116 : 4256 - 4265 , 2010 n engl j med 349 : 1793 - 1802 , 2003 15 . 
gourgou - bourgade s , cameron d , poortmans p , et al : guidelines for time - to - event end point denitions in breast cancer trials : results of the datecan initiative ( denition for the assessment of time - to - event endpoints in cancer trials )  . 
saad ed , zalcberg jr , p eron j , et al : understanding and communicating measures of treatment effect on survival : can we do better ? j natl cancer inst 21 . 
royston p , parmar mk : restricted mean survival time : an alternative to the hazard ratio for the design and analysis of randomized trials with a time - to - event outcome . 
 functional rna studies are a useful tool in variant classication but must be used with caution : a case study of one brca2 variant paola nix , phd1 ; erin mundt , ms1 ; susan manley , ms / cgc , mba1 ; bradford coffee , phd1 ; and benjamin roa , phd1 the use of genetic testing to evaluate hereditary cancer risk is increasing , because it can inform clinical management and cancer treatment decisions . 
a germline pathogenic variant in one of these genes is associated with an increased risk of cancer and therefore merits altered including increased surveilmedical management , lance and the option of risk - reducing surgeries.1 in addition , the identication of a pathogenic brca1 or brca2 variant may affect treatment decisions and clinician recommendations for women with breast and / or ovarian cancer.1 - 4 given these clinical implications , laboratories accurately that classify variants as part of hereditary cancer genetic testing . is essential although established guidelines from the american college of medical genetics ( acmg ) and association for molecular pathology ( amp ) provide a framework to help with variant classication , 5 there may be challenges interpreting the available evidence for some variants.6 , 7 this includes some sequence variants that have the potential to affect mrna splicing . 
a notable fraction of disease - causing variants in cancer predisposition genes affect splicing.8 - 10 many of these occur at the 5 ( cid : 1 ) and 3 ( cid : 1 ) exon - intron boundaries , and the potential impact on splicing is well established , based on the expected sequence at the canonical splice donor and acceptor ( 6 1 , 2 splice sites ) .5 however , sequence variants located beyond these canonical splice sites may also alter mrna processing . 
pathogenicity for these variants is more difcult to assess , and additional functional evidence is often required to determine the actual impact of the variants on splicing . clinical laboratories commonly use functional rna studies to aid in the classication of variants that may affect splicing . 
although these studies can provide useful evidence about the pathogenicity of such variants , there are important caveats to consider , and care must be taken in both how the studies are performed and how the data are interpreted.11 , 12 one important consideration when using rna analysis to classify variants that may affect splicing is that the observation of a splice defect alone may not be sufcient evidence for classication . 
aberrant splicing may result either in no normal transcript produced by the variant allele ( complete splice defect ) or in some residual normal transcript produced by the variant allele.13 these partial , or leaky , splice defects may result in enough functional transcript being produced to support normal protein function . 
therefore , it is essential to quantify any aberrant splice product and determine whether the variant allele produces any normal transcript when using rna analysis in variant classication . functional rna studies often involve reverse transcription polymerase chain reaction ( rt - pcr ) analysis of rna extracted from a patient blood sample or lymphoblastoid cell line . 
one method to distinguish variant - specic transcripts is to use informative single nucleotide in the same pcr polymorphisms ( snps ) present amplicon as the putative spliceogenic variant being tested ( ie , tag snps )  . 
in the case of a heterozygous variant carrier , these tag snps can differentiate the transcripts produced by the normal allele versus the variant allele , especially when the variant allele is located in the intron and not present in the processed mrna . 
rt - pcr products representing these transcripts can be cloned into a vector system or used directly as templates for sequencing analysis . laboratories that do not require rna analysis to include allele - specic transcript quantication for variant classication , either as part of their own studies or from published studies , may misclassify splice - related variants and potentially report false - positive results . 
in addition , care must be taken in assigning pathogenicity if a variant allele has been shown to produce functional transcript , because it may be unclear whether the amount transcript could support normal protein function . 
 commentary splice variants causing brca2 exon 3 skipping , a variant allele may express up to 20% aberrant product yet not be associated with even a moderate risk of cancer . case study of brca2 c.426 - 12_426 - 8del one example of a splice variant with a complex interpretation is brca2 c.426 - 12_426 - 8delan intronic variant resulting in the deletion of ve nucleotides from the dna sequence adjacent to the splice acceptor site of exon 5 . 
published functional studies support this prediction , with studies by zhang et al in 200916 and sanz et al in 201017 demonstrating that this variant causes skipping of exon 5 , which is out of frame . 
however , both studies also noted that the variant allele produces full - length transcript , indicating a partial splice defect . the variant recently published rna analyses from one clinical testing laboratory showed that brca2 c.426 - 12_426 - 8del caused aberrant splicing , resulting in the deletion of exon 5.18 , 19 there was no allele - specic quantication of however , normal transcripts to determine how much , if any , was produced from the variant allele . 
still , the authors concluded that this variant could be classied as likely pathogenic in accordance with acmg / amp guidelines5 on the basis of rna studies demonstrating abnormal splicing from ( evidence category ps3 ) , absence of population controls ( evidence category pm2 ) , and in silico splicing models predicting a weakening of the native site ( evidence category pp3 ) .18 conversely , our laboratory initially classied brca2 c.42612_426 - 8del as a vus on the basis of the evidence available at the time ( fig 1 )  . 
this evidence included the 2 previously published functional studies showing that the variant allele produced some normal transcript.16 , 17 these functional data alone are not sufcient to determine whether the variant is associated with increased cancer risk , because there is uncertainty in how much normal transcript must be expressed by the variant allele to support normal brca2 function . 
although population databases and in silico modeling can provide useful evidence for classication , these tools also must be considered carefully . benign variants also can be rare ( eg , absent from population controls ) , and in silico splicing models cannot discriminate between a full or partial splice defect . 
as a result , this body of evidence was not sufcient for our laboratory to classify brca2 c.42612_426 - 8del as likely pathogenic . our laboratory was later able to reclassify brca2 c.42612_426 - 8del from vus to benign using additional clinical evidence . 
this included evidence from a validated history weighting algorithm ( hwa ) that scores a variant on the basis of the personal and family histories of multiple individuals who carry the specic variant of interest.20 the variant - specic score is compared with matched pathogenic controls ( individuals with known pathogenic variants in brca2 ) and matched benign controls ( individuals with only benign variants in brca2 and other breast and ovarian cancer - risk genes ; appendix fig a1 )  . 
in this case , the hwa called brca2 c.426 - 12_426 - 8del benign , indicating that carriers did not have a personal or family in brca2 history consistent with a pathogenic variant ( appendix fig a1 )  . in addition , co - occurrence of a vus with known pathogenic variants in the same gene can provide evidence that a variant is benign on the basis of associated clinical phenotypes . 
this provides additional evidence that time of brca2 c.426 - 12_426 - 8del hwa and co - occurrence data are consistent with a benign classication and suggest the variant allele does produce enough functional transcript to support normal brca2 function . 
the recent uptake in laboratories performing their own functional rna studies for variant classication can lead to denitive , actionable ndings for more patients ; however , it is critical that rna analysis be held to a high standard to ensure that variant classications also retain a high level of accuracy . to this end , there are several important considerations in the classication of variants in cancer predisposition genes that may affect splicing . 
snp , single - nucleotide polymorphism . some functional transcript , additional clinical evidence may be needed to determine whether the variant is pathogenic . the importance of this additional clinical evidence is exemplied by brca2 c.426 - 12_426 - 8del . 
karam et al18 came to the conclusion that the variant was likely pathogenic on the basis of rna analysis that identied aberrant splicing , in combination with population frequency and in silico modeling data ; however , the rna analysis performed in that study did not elucidate whether the transcript . 
the variant allele produced any functional previously published rna analyses were considered insufcient for a pathogenic classication by our laboratory because of evidence that the variant allele does produce some normal transcript . 
previous studies have highlighted the complex situation that discordant classications create for patients and providers regarding patient management and the potential for discordant test results for family members tested at different laboratories.6 , 7 second , classications made without careful consideration of rna analysis performed by the laboratory or from published studies may result in a false - positive test result . 
professional societies provide recommendations for the medical management of patients with a pathogenic variant in brca2 , including consideration of risk - reducing surgical interventions and eligibility for cancer drug therapies.1 - 4 the example of brca2 c.426 - 12_426 - 8del highlights the need for caution when interpreting functional evidence from rna analysis for variants that may affect splicing to avoid potential mismanagement and inappropriate medical intervention . in this case , variant classication made without full the partial splice defect consideration of resulted in a classication of likely pathogenic for a variant that our laboratory classied as benign when assessed with additional clinical evidence . acmg / amp guidelines provide useful guidance for variant classication5 but do not inform on every caveat or complexity that may be encountered during variant classication . given the severity of the potential clinical consequences of incorrectly classifying a benign variant as pathogenic , additional guidance for interpreting rna sequencing data may be necessary to enhance accurate classication of splicerelated variants . 
this could involve a stepwise process until sufcient data ( from functional rna studies and other sources ) are obtained to accurately perform variant classication ( fig 1 )  . 
for example , the rna transcripts observed in a patient who carries a sequence variant should be compared with the range of full - length and alternative transcripts that naturally occur in normal controls . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . erin mundt employment : myriad genetics stock and other ownership interests : myriad genetics susan manley employment : myriad genetics stock and other ownership interests : myriad genetics bradford coffee employment : myriad genetic laboratories stock and other ownership interests : myriad genetics benjamin roa employment : myriad genetics leadership : myriad genetics stock and other ownership interests : myriad genetics research funding : myriad genetics patents , royalties , other intellectual property : intellectual property held by employer myriad genetics ( inst ) travel , accommodations , expenses : myriad genetics no other potential conicts of interest were reported . acknowledgment we thank krystal brown , phd , and stephanie meek , phd , for their assistance in preparing the manuscript . references daly mb , pilarski r , berry mp et al : nccn clinical practice guidelines in oncology : genetic / familial high - risk assessment : breast , ovarian , and pancreatic ( version 1.2020 ) , nccn clinical practice guidelines in oncology , 2020 . 
 nix et al armstrong d , plaxe s , alvarex r , et al : nccn clinical practice guidelines in oncology : ovarian cancer including fallopian tube cancer and primary peritoneal cancer , version 4.2017. 
curr oncol 25 : s151 - s160 , 2018 richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
genet med 17 : 405 - 424 , 2015 gradishar w , johnson k , brown k , et al : clinical variant classication : a comparison of public databases and a commercial testing laboratory . 
oncologist 22 : 797 - 803 , 2017 balmaa j , digiovanni l , gaddam p , et al : conicting interpretation of genetic variants and cancer risk by commercial laboratories as assessed by the prospective registry of multiplex testing . 
j clin oncol 34 : 4071 - 4078 , 2016 rhine cl , cygan kj , soemedi r , et al : hereditary cancer genes are highly susceptible to splicing mutations . 
whiley pj , de la hoya m , thomassen m , et al : comparison of mrna splicing assay protocols across multiple laboratories : recommendations for best practice in 12 . 
brnich se , abou tayoun an , couch fj , et al : recommendations for application of the functional evidence ps3 / bs3 criterion using the acmg / amp sequence standardized clinical testing . 
gelli e , colombo m , pinto am , et al : usefulness and limitations of comprehensive characterization of mrna splicing proles in the denition of the clinical relevance of brca1 / 2 variants of uncertain signicance . 
sanz dj , acedo a , infante m , et al : a high proportion of dna variants ofbrca1 and brca2 is associated with aberrant splicing in breast / ovarian cancer patients . 
pruss d , morris b , hughes e , et al : development and validation of a new algorithm for the reclassication of genetic variants identied in the brca1 and brca2 genes . 
 prospective feasibility study for using cell - free circulating tumor dnaguided therapy in refractory metastatic solid cancers : an interim analysis purpose retrospective studies have demonstrated that cell - free circulating tumor dna ( ctdna ) hotspot testing predicts matched therapy response to firstand second - line therapies in patients with advanced nonsmall - cell lung cancer ( nsclc )  . 
however , no prospective outcomes studies have evaluated ctdna - guided matched therapy decision making on the basis of comprehensive plasma genomic testing including all four major classes of alterations . 
here , we report the clinical utility of this approach in advanced solid tumor cancers . patients and methods we conducted a multiple parallel cohort , open - label , clinical trial using ctdna - guided matched therapy when tissue was insufficient or unobtainable for next - generation sequencing . 
patients with prespecified targetable alterations in metastatic nsclc , gastric cancer ( gc ) , and other cancers were matched to several independent targeted agent trials at a tertiary academic center . results somatic alterations were detected in 59 patients with gc ( 78% ) , and 25 patients ( 33% ) had targetable alterations ( erbb2 , n = 11 ; met , n = 5 ; fgfr2 , n = 3 ; pik3ca , n = 6 )  . 
2017 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the national comprehensive cancer network guidelines recommend genotyping in seven solid tumor cancers ( nonsmall - cell lung cancer [ nsclc ] , breast , gastric , esophageal , colorectal , melanoma , and gi stromal tumors ) for 11 genomic targets ( gts ) to inform targeted therapy selection.1 - 6 however , biopsy specimens can be inadequate for comprehensive profiling in 25% to 50% of patients , 7 - 10 leading to incomplete genotyping or repeat invasive biopsy to obtain more tissue . 
repeat biopsy is also recommended at progression in patients with breast cancer and nsclc to capture targetable genomic changes such as erbb2 ( human epidermal growth factor receptor 2 [ her2 ] ) copy number amplification ( cna ) or egfr and alk resistance mutations , respectively.4 , 5 , 11 comprehensive ctdna testing covering point mutations , insertions / deletions ( indels ) , fusions , seung tae kim kimberly c . 
 and cna may obviate the need for repeat invasive biopsies for genotyping when tissue is of insufficient quantity or unobtainable at initial diagnosis or at progression.12 , 13 in general , next - generation sequencing ( ngs ) seems to detect more actionable variants in target genes than non - ngs methods ( hotspot testing ) such as polymerase chain reaction ( pcr ) , immunohistochemistry ( ihc ) , or fluorescence in situ hybridization.14 - 18 beyond the benefits of invasive biopsy avoidance and higher sensitivity compared with nonngs methods , comprehensive ctdna ngs may provide a global summary of multiple lesions , whereas tissue genotyping of small biopsies may fail to capture intraand intertumor heterogeneity.19 - 21 retrospective studies in nsclc using ctdna genotyping for egfr mutations in the firstline ( egfrl858r / exon19del ) 22 and second - line ( egfrt790m ) 23 , 24 settings have produced response rates similar to studies of therapies directed by tissue - based genotyping . 
the study was conducted in accordance with the current ethical principles outlined in the declaration of helsinki and good clinical practice guidelines . patients eligible patients were older than age 20 years with histologically confirmed metastatic cancer , who had sufficient tumor tissue to test cancer - specific biomarkers but not to undergo comprehensive genomic profiling ( ngs )  . 
rr and disease control rate ( dcr = rr + stable disease ) were centrally adjudicated in accordance with response evaluation criteria in solid tumors ( recist ) version 1.1.28 statistical analysis descriptive statistics were calculated for demographics , ctdna alteration detection rate , and substudy matching . 
after double ultracentrifugation , 5 to 30 ng of cfdna was isolated for digital sequencing as previously described.12 , 26 , 29 all exons in 30 genes and critical exons ( those known to harbor somatic mutations ) of 40 genes were completely sequenced . 
sequencing data were analyzed using a custom bioinformatics pipeline to identify single nucleotide variants ( snvs ) in 70 genes ( 150 - kb panel footprint ) , cnas in 18 genes , indels in three genes ( egfr and erbb2 exons 19 and 20 ; met exon 14 ) , and alk , ret , ros1 , ntrk1 , fgfr2 , and fgfr3 fusions ( appendix fig a2 )  . 
tumor - derived dna shed into the bloodstream increases this value but , as a result of the relative proportions of tumorderived versus leukocyte - derived cfdna , typically a minor contributor . 
90th percentiles , respectively , of all cna calls in the guardant360 database . results patient enrollment and demographics from august 2014 to february 2016 , informed consent was obtained from 210 consecutive patients with metastatic cancer whose tissue was available for cancer - specific biomarker testing , but insufficient for ngs , at initial diagnosis or at progression . 
sixteen patients were lost to follow - up or withdrew consent , leaving 194 patients molecularly profiled by ctdna ngs ( appendix fig a3 )  . median age was 60 years ( range , 28 to 78 years ) for nsclc and 57 years ( range , 23 to 82 years ) for gc , melanoma , and other cancers ; 43% , 58% , 56% , and 89% of patients with these cancers were male , respectively ( table 1 )  . 
newly diagnosed ( firstline ) patients composed 29% of patients with nsclc , 37% of those with gc , 68% of those with melanoma , and 11% of those with other table 1 . 
erbb2 ( her2 ) cna was identified in two patients at progression ( one co - occurring with egfrt790m and one with the erbb2 g778_p780dup ) , and met was amplified in four patients at progression ( one with erbb2 insertion and three with egfrt790m )  . 
however , cnas in nsclc were not prespecified gts . on the basis of rolling substudy availability , inclusion criteria , and patient comorbidities , 10 ( 40% ) of the 25 patients with gc ( erbb2 , n = 6 ; met , n = 1 ; fgfr2 , n = 1 ; and pik3ca , n = 2 ) and 17 ( 50% ) of the 34 patients with nsclc ( egfr , n = 7 ; egfrt790m , n = 7 ; and alk , n = 1 ) with prespecified gts were matched to a molecularly targeted therapy ( tables 2 and 3 )  . 
one patient with gc and two patients with nsclc were lost to follow - up , leaving nine patients ( 90% ) and 15 patients ( 88% ) evaluable for response , respectively . ctdna - guidable targeted therapies and response by cancer type in gc , cnas in erbb2 ( n = 5 ) , fgfr2 ( n = 1 ) , and met ( n = 1 ) and snvs in pik3ca ( n = 2 ) were targeted with one patient achieving complete response ( cr ) , five partial response ( pr ) , and three stable disease ( sd ) for an rr of 67% ( 95% ci , 31% to 91% ) and dcr of 100% ( 95% ci , 63% to 100% ; table 4 , fig 2a )  . 
of patients ctdna alterations detected patients with prespecified second line of therapy third or greater line of therapy treated with matched therapy evaluable for response treated with matched therapy evaluable for response treated with matched therapy evaluable for response treated with matched therapy evaluable for response abbreviations : ctdna , circulating tumor dna ; gt , genomic target . erbb2 amplification amplification fgfr2 amplification pik3ca mutation no . 
one patient with ctdna - detected erbb2 ( her2 ) amplification ( + + + ) achieved complete remission after six cycles of capecitabine , oxaliplatin , and lapatinib ( fig 2b )  . in nsclc , egfrexon19del ( n = 5 ) , egfrl858r ( n = 2 ) , egfrt790m ( n = 7 ) , and alk fusion ( n = 1 ) were targeted , with 13 patients achieving pr and two sd for a rr of 87% ( 95% ci , 58% to 98% ) and a dcr of 100% ( 95% ci , 75% to 100% ; table 4 , fig 2c )  . 
of the seven patients receiving first - line epidermal growth factor receptor inhibitors ( egfri ) , six achieved pr on afatinib , erlotinib , or gefitinib , whereas the one patient with sd received rociletinib . 
similarly , six egfrt790m patients achieving pr were treated with osimertinib or olmutinib , whereas the patient with sd was treated with afatinib plus insulin - like growth factor ligand monoclonal antibody . 
% clinical status at time of ctdna collection new diagnosis treated with matched therapy evaluable for response second line of therapy treated with matched therapy evaluable for response treated with matched therapy evaluable for response treated with matched therapy evaluable for response abbreviations : ctdna , circulating tumor dna ; gt , genomic target . third or greater line of therapy all patients discussion to our knowledge , this is the first prospective ctdna - guided molecular testing program with objective response evaluated in solid tumors . 
this program guided patients in whom biopsy was not readily available or in whom tumor material was not sufficient for comprehensive sequencing to genomically matched therapies available in practice or clinical trials . 
of 194 patients , 30 ( 15.5% ) were successfully enrolled onto one of the ongoing matched therapy clinical trials , a rate comparable to tumor sequencing - based trials . responses to ctdna - guided matched therapy in gc and nsclc were similar to those published in tissue - based matched therapy studies , although the sample sizes here are modest . in gc , cnas were found in erbb2 ( her2 ) , met , and fgfr2 in 31% of our patients , split evenly between newly diagnosed and pretreated patients , consistent with previous primary tumor estimates of these cnas at 20% to 22%.30 , 31 significantly , four ( 80% ) of five patients with erbb2 ( her2 ) - amplified gc responded , including one cr ( fig 2a ) , with all achieving clinical benefit ( cr , pr , or sd )  . 
the one patient with gc with erbb2 cna without pr ( but with sd ) was on lapatinib monotherapy , raising the question of whether chemotherapy produced most of the benefit here . 
however , addition of lapatinib to chemotherapy did produce a significant overall survival benefit in asian patients in the lapatinib optimization study in her2 - positive gastric cancer ( logic ) study.32 in addition , a patient with refractory colon cancer with erbb2 cna achieved sd as best response ( table 4 )  . 
matched therapy response and disease control rate by cancer cohort response gc ( n = 78 ) nsclc ( n = 73 ) melanoma ( n = 34 ) other ( n = 9 ) no . 
thus , an advantage of ctdna over tissue genotyping is that quantitation of the relative vafs can provide an indication of the subclonality and potentially predict treatment response , in contrast to a binary positive or negative result . 
however , a ratio , 10% may be misleading if there is focal amplification of the egfr driver mutation and not egfrt790m.42 beyond t790m , recent reports suggest that comprehensive profiling at progression may be important in nsclc given the multiple other resistance mechanisms after egfri therapy.43 these include non - egfrt790m on - target point mutations , as well as bypass mutations in braf , kras , mek , and pik3ca ; cnas in met and erbb2 ; fusions in alk ; or rb1 inactivation heralding epithelial to mesenchymal cell transition.34 , 44 - 47 because egfrt790m is the resistance mechanism in only half of patients experiencing progression on firstline egfri , a comprehensive ctdna ngs test covering all major types of genomic alterations is particularly relevant . small sample sizes for targeted therapy in melanoma and colon cancer limit the conclusions that can be drawn in those cohorts ; however , the rr cis in gc and nsclc are consistent with tissue - guided matched therapy rrs . 
single - arm objective rrs exceeding 30% have led to us food and drug administration regulatory approval of matched therapies.48 , 49 the rrs to ctdna - detected alterations in this interim analysis ( 67% [ 95% ci , 31% to 91% ] for gc and 87% [ 95% ci , 58% to 98% ] for nsclc ) support clinical utility for guardant360 in patients with advanced nsclc and gc in whom tissue is insufficient or inaccessible and build upon previous validation studies of the diagnostic test used herein.12 , 26 because this study was not randomized , its primary limitation is the potential for selection bias to enroll patients more likely to benefit . 
not all patients with targetable alterations could receive matched therapy because of the various requirements of the multiple parallel matched therapy substudy protocols , performance status , or loss to follow - up . 
future studies should examine ctdnaguided matched therapy outcomes in more racially diverse cohorts . to our knowledge , this is the first prospective study to examine the clinical utility of comprehensive ctdna genomic testing to guide matched therapy selection . 
lanman , amirali talasaz , keunchil park , jeeyun lee financial support : young suk park , amirali talasaz administrative support : young suk park , amirali talasaz provision of study materials or patients : seung tae kim , se hoon park , joon oh park , young suk park , ho yeong lim , won ki kang , amirali talasaz , keunchil park , jeeyun lee collection and assembly of data : seung tae kim , kimberly c . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . ho yeong lim no relationship to disclose won ki kang no relationship to disclose seung tae kim no relationship to disclose kimberly c . 
banks employment : guardant health stock and other ownership interests : guardant health se - hoon lee honoraria : astrazeneca / medimmune , roche , bristol - myers squibb , merck consulting or advisory role : pfizer , novartis , astrazeneca , bristol - myers squibb travel , accommodations , expenses : novartis kyung kim no relationship to disclose joon oh park honoraria : celgene consulting or advisory role : celgene speakers bureau : celgene research funding : celgene , astrazeneca se hoon park no relationship to disclose young suk park no relationship to disclose richard b . 
lanman employment : guardant health , veracyte leadership : guardant health stock and other ownership interests : guardant health , veracyte research funding : guardant health amirali talasaz employment : guardant health leadership : guardant health stock and other ownership interests : guardant health research funding : guardant health patents , royalties , other intellectual property : guardant health travel , accommodations , expenses : guardant health keunchil park consulting or advisory role : astellas pharma , astrazeneca , boehringer ingelheim , clovis oncology , eli lilly , hanmi , kyowa hakko kirin , novartis , ono pharmaceutical , roche speakers bureau : boehringer ingelheim research funding : astrazeneca jeeyun lee no relationship to disclose affiliations support seung tae kim , se hoon park , kyung kim , joon oh park , se - hoon lee , young suk park , ho yeong lim , won ki kang , keunchil park , and jeeyun lee , samsung medical center , sungkyunkwan university school of medicine , seoul , korea ; and kimberly c . 
j natl compr canc netw 13 : 448 - 475 , 2015 von mehren m , randall rl , benjamin rs , et al : gastrointestinal stromal tumors , version 2.2014. 
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lim sm , kim ey , kim hr , et al : genomic profiling of lung adenocarcinoma patients reveals therapeutic targets and confers clinical benefit when standard molecular testing is negative . 
schrock ab , frampton gm , herndon d , et al : comprehensive genomic profiling identifies frequent drug - sensitive egfr exon 19 deletions in nsclc not identified by prior molecular testing . 
ali sm , hensing t , schrock ab , et al : comprehensive genomic profiling identifies a subset of crizotinib - responsive alkrearranged non - small cell lung cancer not detected by fluorescence in situ hybridization . 
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kim st , lee w - s , lanman rb , et al : prospective blinded study of somatic mutation detection in cell - free dna utilizing a targeted 54 - gene next generation sequencing panel in metastatic solid tumor patients . 
zill oa , mortimer sa , banks kc , et al : somatic genomic landscape of over 15 , 000 patients with advanced - stage cancer from clinical next - generation sequencing analysis of circulating tumor dna . 
zill oa , greene c , sebisanovic d , et al : cell - free dna next - generation sequencing in pancreatobiliary carcinomas . cancer discov 5 : 1040 - 1048 , 2015 30 . 
deng n , goh lk , wang h , et al : a comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co - occurrence among distinct therapeutic targets . 
hecht jr , bang y - j , qin sk , et al : lapatinib in combination with capecitabine plus oxaliplatin in human epidermal growth factor receptor 2 - positive advanced or metastatic gastric , esophageal , or gastroesophageal adenocarcinoma : trio - 013 / logica randomized phase iii trial . 
arrieta o , cardona af , martn c , et al : updated frequency of egfr and kras mutations in nonsmall - cell lung cancer in latin america : the latin - american consortium for the investigation of lung cancer ( clicap )  . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as first - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
sequist lv , yang jc - h , yamamoto n , et al : phase iii study of afatinib or cisplatin plus pemetrexed in patients with metastatic lung adenocarcinoma with egfr mutations . 
vallee a , audigier - valette c , herbreteau g , et al : rapid clearance of circulating tumor dna during treatment with azd9291 of a lung cancer patient presenting the resistance egfr t790m mutation . 
marchetti a , palma jf , felicioni l , et al : early prediction of response to tyrosine kinase inhibitors by quantification of egfr mutations in plasma of nsclc patients . 
piotrowska z , niederst mj , karlovich ca , et al : heterogeneity underlies the emergence of egfrt790 wild - type clones following treatment of t790m - positive cancers with a third - generation egfr inhibitor . 
liang w , he q , chen y , et al : metastatic eml4 - alk fusion detected by circulating dna genotyping in an egfrmutated nsclc patient and successful management by adding alk inhibitors : a case report . 
stewart el , tan sz , liu g , et al : known and putative mechanisms of resistance to egfr targeted therapies in nsclc patients with egfr mutations : a review . 
most prostate cancers that develop resistance to abiraterone or enzalutamide have active ar signaling , and amplication of the ar gene or its enhancer is thought to be a common resistance mechanism.2 - 4 in the jayaram et al study , plasma was collected before starting treatment from one of four clinical cohorts that used either abiraterone plus low - dose steroid or enzalutamide for treatment of metastatic castration - resistant prostate cancer ( mcrpc ) ( pcr2023 cohort , clinicaltrials.gov identier : nct01867710 ; premier cohort , clinicaltrials.gov identier : nct02288936 ; british columbia cohort , clinicaltrials.gov identier : nct02125357 ; and cohort a , which was on biospecimen collection protocols )  . 
the investigators used droplet digital polymerase chain reaction and / or targeted next - generation sequencing to determine cn gain of the ar gene within the cell - free dna ( cfdna ) in plasma . 
their study adds support for a noninvasive prognostic factor to improve the management of mcrpc . not surprisingly , the rate of ar gain ( 16.5% ) identied in the jayaram et al1 study and in other evaluations of plasma ar status5 , 6 is signicantly lower than what has been found in tissue ( 70% ) , 3 which is even higher when including gain of the ar enhancer ( 81% )  . 
this suggests that the prognostic value of detecting ar gain may be as much in its indication of high ctdna fractionlikely a reection of tumor burdenas in the identication of a putative resistance mechanisindeed , plasma ar gain has been associated with worse os in patients receiving docetaxel8 and worse os and pfs in patients receiving cabazitaxel.9 concentration of cfdna alone is predictive and prognostic in the setting of taxane therapy.10 the authors should be commended for acknowledging a prognostic bias of tumor burden . 
vanderweele research funding : prostate cancer foundation , department of defense - prostate cancer research program , astrazeneca ( inst ) , fortis ( inst ) travel , accommodations , expenses : genzyme no other potential conicts of interest were reported . references jayaram a , wingate a , wetterskog d , et al : plasma androgen receptor copy number status at emergence of metastatic castrationresistant prostate cancer : a pooled multicohort analysis . 
j transl med 12 : 313 , 2014 salvi s , casadio v , conteduca v , et al : circulating cell - free ar and cyp17a1 copy number variations may associate with outcome of metastatic castration - resistant prostate cancer patients treated with abiraterone . br j cancer 112 : 1717 - 1724 , 2015 conteduca v , wetterskog d , sharabiani mta , et al : androgen receptor gene status in plasma dna associates with worse outcome on enzalutamide or abiraterone for castration - resistant prostate cancer : a multiinstitution correlative biomarker study . 
ann oncol 28 : 1508 - 1516 , 2017 annala m , vandekerkhove g , khalaf d , et al : circulating tumor dna genomics correlate with resistance to abiraterone and enzalutamide in prostate cancer . 
cancer discov 8 : 444 - 457 , 2018 conteduca v , jayaram a , romero - laorden n , et al : plasma androgen receptor and docetaxel for metastatic castration - resistant prostate cancer . eur urol 75 : 368 - 373 , 2019 conteduca v , castro e , wetterskog d , et al : plasma ar status and cabazitaxel in heavily treated metastatic castration - resistant prostate cancer . eur j cancer 116 : 158 - 168 , 2019 10 . 
these results highlight the importance of screening for ntrk fusions as part of the tumor genomic proling for patients with pediatric cancer . jco precis oncol 5 : 204 - 214 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction rearrangements involving the neurotrophic tyrosine receptor kinase ( ntrk ) genes ntrk1 , ntrk2 , and ntrk3 encode fusion proteins containing the intact ntrk kinase domain that are oncogenic drivers of a histologically diverse group of tumors . 
 ntrk fusions in pediatric tumors : frequency , partner , and outcome content key objective ntrk fusions are tumor - agnostic or age - independent biomarkers that identify patients suitable for treatment with the us food and drug administrationapproved trk inhibitors . 
this single institutional study examined the frequency , fusion partner , and clinical outcome of ntrk fusions in a large cohort of unselected patients with pediatric cancer . knowledge generated our study demonstrated that ntrk fusions are more frequent in pediatric tumors and involve a broader panel of fusion partners and a wider range of tumors those than previously recognized and highlights pediatric cancers in which ntrk fusions are more or less likely to occur . relevance this study provided important ndings regarding ntrk fusionpositive pediatric cancers and cancers where ntrk fusions are rarely seen . 
immunohistochemistry was performed in a subset of cases using pan - trk antibody ( abcam , cambridge , uk , 1 : 100 dilution ) ( table 1 )  . fusion gene detection was performed using the chop cancer fusion panel as previously described.15 briey , targetspecic primers covering 673 exons were custom designed to identify known fusion genes and potential novel fusion genes associated with 110 cancer genes using anchored multiplex polymerase chain reaction ( pcr ) technology ( archerdx , inc , boulder , co )  . 
all fusions , when identied in our laboratory for the rst time , were conrmed by nested pcr followed by sanger sequencing . mutations ( single nucleotide variants [ snvs ] and small insertion / deletions [ indels ] ) and copy number alterations ( cnas ) were evaluated by using the chop hematological malignancy panel ( chmp ) or solid tumor panel ( cstp ) as described previously.16 briey , genomic dna was extracted from the tumor samples . 
libraries were prepared using probes targeting 118 genes ( chmp ) or 238 genes ( cstp ) , respectively , and sequenced on illumina hiseq platform using 150 bp paired - end sequencing . 
sequence data were analyzed using the home brew software concords v2 ( for snvs and indels ) and nextgene v2 next - generation sequencing analysis software ( for cnas ; softgenetics , llc , state college , pa )  . 
clinically signicant variants including indels , and cnas were conrmed by sanger sesnvs , quencing , multiplex ligation - dependent probe amplication ( mlpa ) , real - time pcr , or droplet digital pcr ( ddpcr ) when necessary . 
by contrast , different ntrk fusions were present in tumors with the same histological diagnosis , such as kctd16 - ntrk2 and trim24 - ntrk2 in two male patients of similar age with ganglioglioma , who grade i ( table 1 )  . 
in ptc , tumorigenesis is associated with constitutive activation of the mapk and pi3k signaling pathways secondary to somatic point mutations in braf , pten , dicer1 , and ras as well as fusions involving ret , alk , and ntrk.3 , 23 gene fusions have been reported in both sporadic and radiation - induced ptcs and are more common in pediatric ( 50% - 60% ) compared with adult tumors ( approximately 15% ) .2 , 23 ret and ntrk fusions are the most common , reported in 25%30% and approximately 10% ( range , 0% - 26% ) of pediatric ptcs , respectively.2 , 23 ntrk3 fusions are usually observed more commonly in ptcs than ntrk1 fusions , 2 , 23 which is similar to what we observed in our patient cohort . 
all the ptcs in our cohort were sporadic , none associated with ntrk1 ntrk2 ntrk3 snvs / indels cnas 10 - 15 16 - 20 gender female male snvs and indels missense frameshift inframe cnas gain loss gain and loss cnloh fig 1 . 
case 17 demonstrates a low - grade tumor with strn3 - ntrk3 showing moderately cellular spindle to round cell proliferation with prominent vascular proliferation ( c , h&e , 200 )  . 
case 21 shows widely invasive follicular variant of papillary thyroid carcinoma with etv6 - ntrk3 demonstrating extrathyroidal extension and angioinvasion ( d , h&e , 50 ) and nuclear features of papillary thyroid carcinoma ( inset , 400 )  . 
two cases demonstrate the diffuse sclerosing variant of papillary thyroid carcinoma showing solid and papillary groups inltrating the thyroid parenchyma with numerous psammomatous calcications ( e , h&e , 100 )  . 
the data are limited but suggest that the presence of an ntrk fusion may have diagnostic , prognostic , and therapeutic signicance in ptcs and may hold clinical utility for stratifying surgical and medical care . 
standard therapy for advanced ptcs in children involves surgical resection of gross disease followed by radioactive - iodide ( rai ) therapy . in a recent multicenter , open - label phase i or ii study of larotrectinib for the treatment of pediatric patients with solid tumors , two children with advanced ptcs were treated for  . 
7 months and remained progression - free , although , unfortunately , the objective response to treatment was not reported.25 ntrk fusions in pediatric cns tumors all the cns tumors identied with ntrk fusions were either gliomas or mixed neuronal glial tumors . 
four of the six ntrk2 fusions were novel fusions at the time of discovery with different 5 ( cid : 1 ) - partner genes including kank1 , c2orf4 , kctd16 , and specc1l . 
ntrk fusion genes have been described in pediatric lowand highgrade gliomas at a low prevalence , 26 although one study reported a nding of 40% of nonbrainstem high - grade gliomas in children younger than 3 years old containing an ntrk fusion gene ( n = four of the 10 samples ) .27 six of the 7 ntrk fusionpositive cns tumors were low - grade gliomas ( lgg ) , which may be partially due to the higher frequency of lgg in our unselected pediatric cohort ( approximately 45% of all cns tumors )  . 
although the duration of follow - up in our study is limited , the majority of patients underwent standard of care for their cns tumor subtype with resection of the primary tumor without recurrence . 
larotrectinib and entrectinib have shown antitumor effect for both primary brain tumors and solid tumors with brain metastases with systemic administration suggesting adequate penetration of the blood - brain barrier.11 in a study of nine patients with primary cns tumors treated with ntrk inhibitors , disease control was observed in all evaluable patients with stable disease in seven patients . 
some tumors exhibited typical age , morphology , and etv6 - ntrk3 fusion compatible with if , showing densely cellular fascicular growth of primitive ovoid cells and inltration of surrounding tissue ( cases 13 and 14 )  . 
clinical classication and treatment based on histology only , particularly in soft - tissue tumors with spindle morphology , have proven to be challenging in some cases because of variable histologic features and immunohistochemical patterns.30 as more tumors are being studied for fusions , the morphologic spectrum is expanding , such that the fifth edition of the soft tissue and bone tumors who classication31 now includes an emerging entity titled ntrk - rearranged spindle cell neoplasm to encompass spindle cell soft - tissue tumors with ntrk gene rearrangements ( other than if )  . 
it remains to be seen if soft - tissue histologic classication , molecular classication , or some combination of both will provide clinicians with the most accurate information for personalized treatment . 
magnetic resonance imaging at diagnosis ( a ) , 1 month post - targeted therapy ( b ) , and 5 months post - therapy ( c ) showing marked tumor shrinkage . 
at diagnosis , the tumor contained densely cellular areas with spindled to round cells and increased mitosis ( d , h&e 400 ) with cytoplasmic and membranous pan - trk immunohistochemistry ( inset )  . 
ccd , coiled - coil domain ; chd , calponin homology domain ; ecd - lb , extracellular ligand binding domain ; h&e , hematoxylin and eosin staining ; pkt , protein tyr kinase ; tm , transmembrane domain ; ss , signal sequence . ntrk fusions facilitate precision diagnosis , prognosis , and therapy follow - up information is available for all patients , and follow - up times ranged from 6 to 46 months . 
in almost all cases , the detection of an ntrk fusion conrmed the morphologic diagnosis , and in ve cases , the nal tumor diagnosis was largely based on the discovery of an ntrk fusion ( excluding other differential diagnostic considerations )  . 
one exception was the case of secretory carcinoma , which was initially diagnosed as mucoepidermoid carcinoma , but later changed to secretory carcinoma following the detection of the etv6 - ntrk3 and additional immunohistochemical evaluation ( case 10 )  . 
collectively , we analyzed 261 common embryonal solid tumors ( 79 neuroblastomas , 29 medulloblastoteratoid / rhabdoid mas , 28 wilms tumors , 13 atypical tumors , and 11 hepatoblastomas ) , bone tumors ( 27 osteosarcomas and 24 ewing sarcomas ) , and skeletal muscle tumors ( 50 rhabdomyosarcomas ) , and none had ntrk fusions . 
thus , although it is difcult to exclude the possibility that ntrk fusions might occur in individual tumors of these subtypes , which accounted for about one third of all solid tumors in this cohort , they are likely to be rare . case 15 was a 6 - month - old male infant with a left upper extremity mass . 
prospectively , the rest of the patients who survived with the standard therapy may also benet from trk inhibitor therapy if their tumors progress or recur . received neoadjuvant we assessed the clinical outcome of all ntrk fusionpositive patients for up to 46 months ( median 21 months )  . 
the median follow - up time for patients with cns tumors was 21 months . the majority of ntrk - positive lgg demonstrated superb outcome with gross total resection without additional therapy . one patient with congenital glioblastoma and an etv6ntrk3 fusion died 3 months after birth , and the tumor specimen was obtained via autopsy . 
our review of 1 , 217 patients showed that ntrk fusions are more frequently seen in pediatric tumors than in adult tumors and involve a broader panel of fusion partners and a wider range of pediatric tumors than previously recognized . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / cci / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . elizabeth fox other relationship : helsinn therapeutics gerald b . 
wertheim employment : johnson & johnson stock and other ownership interests : johnson & johnson vinodh pillai consulting or advisory role : foundation medicine travel , accommodations , expenses : foundation medicine jennifer e . 
genes ( basel ) 10 : 723 , 2019 prasad ml , vyas m , horne mj , et al : ntrk fusion oncogenes in pediatric papillary thyroid carcinoma in northeast united states . 
hsiao sj , zehir a , sireci an , et al : detection of tumor ntrk gene fusions to identify patients who may benet from tyrosine kinase ( trk ) inhibitor therapy . 
nat rev clin oncol 15 : 731 - 747 , 2018 suurmeijer aj , dickson bc , swanson d , et al : the histologic spectrum of soft tissue spindle cell tumors with ntrk3 gene rearrangements . 
papadopoulos kp , gandhi l , janne pa , et al : first - in - human study of ds - 6051b in patients ( pts ) with advanced solid tumors ( ast ) conducted in the us . 
drilon a , ou si , cho bc , et al : repotrectinib ( tpx - 0005 ) is a next - generation ros1 / trk / alk inhibitor that potently inhibits ros1 / trk / alk solventfront mutations . 
lopez gy , perry a , harding b , et al : cdkn2a / b loss is associated with anaplastic transformation in a case of ntrk2 fusion - positive pilocytic astrocytoma . neuropathol appl neurobiol 45 : 174 - 178 , 2019 19 . 
surrey lf , jain p , zhang b , et al : genomic analysis of dysembryoplastic neuroepithelial tumor spectrum reveals a diversity of molecular alterations dysregulating the mapk and pi3k / mtor pathways . 
tuttle rm , haugen b , perrier nd : updated american joint committee on cancer / tumor - node - metastasis staging system for differentiated and anaplastic thyroid cancer ( eighth edition ) : what changed and why ? thyroid 27 : 751 - 756 , 2017 25 . 
laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , 26 . 
okamura r , boichard a , kato s , et al : analysis of ntrk alterations in pan - cancer adult and pediatric malignancies : implications for ntrk - targeted theropen - label , phase 1 / 2 study . 
nat genet jones ka , bossler ad , bellizzi am , et al : bcr - ntrk2 fusion in a low - grade glioma with distinctive morphology and unexpected aggressive behavior . 
robinson gw , gajjar aj , gauvain km , et al : phase 1 / 1b trial to assess the activity of entrectinib in children and adolescents with recurrent or refractory solid tumors including central nervous system ( cns ) tumors . 
 o persistent severe hyperlactatemia and metabolic derangement in lethal sdhb - mutated metastatic kidney cancer : clinical challenges and examples of extreme warburg effect see accompanying editorial doi : purpose to describe the unique clinical features , determine the genomics , and investigate the metabolic derangement of an extremely rare form of a hereditary lethal kidney cancer syndrome . patients and methods three patients with lethal kidney cancer ( age 19 , 20 , and 37 years ) exhibiting persistent ( 1 to 3 months ) extremely high levels of blood lactate ( > 5 mm ) despite normal oxygen perfusion , highly avid tumors on [ 18f ] fluorodeoxyglucose positron emission tomography ( pet ) , and pleomorphic histopathologic features were identified and treated in a single institute . 
integrated studies including whole - genome sequencing ( wgs ) , targeted sequencing , immunohistochemistry , cell - based assays , and 18f - glutamine pet imaging were performed to investigate this rare kidney cancer syndrome . results all three patients with kidney cancer were initially given various diagnoses as a result of diverse tumor histopathology and atypical clinical presentations . 
genomic studies of the blood and tumors of these patients identified three different kinds of germline lossof - function mutations in the sdhb gene and the common loss of heterozygosity in the remaining sdhb allele thorough somatic chromosome 1p deletion . 
in one patient , wgs revealed that a germline mutation of sdhb coupled with loss of heterozygosity was the sole genetic event . cancer evolution analysis of sdhb tumors based on wgs demonstrated that sdhb in kidney epithelium fulfills the knudson two - hit criteria as a major tumor suppressor gene . 
right panels are corresponding blood lactate levels over the monitoring period for patients 1 , 2 , and 3 . mutated gene in sdh - rcc is sdhb ( 83% ) .18 - 20 as a result of its rarity and recent designation , clinical and molecular features associated with aggressive sdhb - deficient rcc are unknown . the aerobic glycolysis warburg effect in cancer was recognized by otto warburg , 21 , 22 who first described a phenomenon where glucose undergoes lactic acid fermentation in lieu of aerobic respiration despite normal oxygen tension , providing adaptive advantages for proliferating cancer cells.23 - 26 direct investigation of the warburg effect in human cancer remains a challenge.27 , 28 the increased activity detected by [ 18f ] fluorodeoxyglucose ( fdg ) positron emission tomography ( pet ) reflects glucose uptake and thereby renders indirect evidence of aerobic glycolysis . 
cb - 839 was provided by calithera biosciences ( south san francisco , ca )  . germline dna analysis germline dna was purified from blood and subjected to sequencing on all coding exons of the sdhb , sdhc , sdhd , and af2 genes by genedx ( elmwood park , nj ) .45 histopathology and immunohistochemistry immunohistochemistry for sdhb was performed using anti - shdb antibody ( ab14714 , clone 21a11 ; abcam , cambridge , united kingdom ) .20 normal pair samples were prepared from the primary kidney tumor of patient 1 and the primary tumor and metastases of patient 3 . 
paired - end 2 3 100 base pair sequence reads were performed using illumina hisequation 2500 instruments ( illumina , san diego , ca ) , mapped using the burrows - wheeler aligner , and processed with the genome analysis toolkit . 
target - specific probes for hybrid selection were designed to capture all protein - coding exons of 341 cancer genes.48 metabolic assessment of patient - derived sdhb - deficient cancer cells short - term primary cell cultures were established from patient 1s tumor ( sdhb2 / 2 tumor ) , patient 1s tumor - adjacent tissue ( sdhb + / 2 cells ) , and an unrelated patients tumor - adjacent normal kidney tissues ( normal kidney )  . 
metabolites were extracted by 80% methanol , and count values were normalized to cell number . whole - genome sequencing 18f - glutamine pet whole - genome sequencing ( wgs ) was performed at the new york genome center ( new york , ny )  . 
 [ 18f ] fdg - pet confirmed extensive metastatic lesions and noted additional involvement of the parietal lobe and cranium ( maximum suv , 44.1 ; fig 1 )  . 
his hospital course was complicated by multiple unexplainable hemolytic and thrombotic events , including pulmonary emboli , numerous cerebral vascular events , and infarction of the superior mesenteric artery necessitating exploratory laparotomies for small bowel and colon resections . 
the increasing blood lactate was associated with increasing tumor burden . patient 3 had persistently elevated lactate levels with a baseline of 4.4 mm / l and a peak of 7.5 mm / l ( fig 1 )  . 
as a result of the high blood lactate level and suspicion of sdhbdeficient rcc based on fdg - pet images , an arterial blood gas was obtained ( ph , 7.43 ; partial pressure of carbon dioxide , 28.6 mm hg ; bicarbonate , 19.3 meq / l ; and oxygen saturation , 98% ; fig 1 )  . diverse histopathology of sdhb - deficient the histopathologic features varied significantly among our patients with sdhb - deficient cancer , making the initial diagnosis challenging . 
 1 7 3 4 4 0 0 0 17352000 17360000 17368000 sdhb exons 4 - 5 patient 1 260 substitutions 72 deletions and insertions 7 rearrangements complex insertion deletion other deletion repeat deletion m - homology t . 
common histology described for sdhbdeficient renal tumors , such as bubbly eosinophilic cytoplasm and cytoplasmic inclusions , 56 was detected only in patient 1s primary tumor but not in the tumors of patients 2 and 3 . loss of sdhb staining in tumors as a result of unusual clinical and histopathologic presentations , sdhb - deficient rcc was suspected in these patients . 
 the two innermost tracks depict the copy number changes ( red , increase ; blue , decrease ; purple , allelic imbalance , one allele amplified or deleted ) in the tumor when compared with the normal for patient 1 . the outermost track shows the intermutation distance for substitutions each plotted according to the type of nucleotide change . the middle track shows the genomic positions of the small insertion ( green ) and deletion ( red ) along the genome . 
immunohistochemistry stain for sdhb protein was subsequently established at memorial sloan kettering cancer center , demonstrating the loss of sdhb staining in cancer but not adjacent non - neoplastic cells ( fig 2a )  . 
as a control , oncocytoma , a kidney tumor with wild - type sdhb , showed strong sdhb staining ( fig 2a )  . patient 1s family pedigree the young age of patient 1 and the unusual histopathologic features of his tumor were concerning for a hereditary rcc . 
accordingly , germline dna analysis was performed by direct sequencing of the sdhb , sdhc , sdhd , and af2 genes , 45 which revealed a germline exon 45 deletion within the sdhb gene in patient 1 ( fig 2b )  . 
germline duplication in sdhb and somatic loss of 1p , where sdhb resides ( 1p36 ) , resulted in complete genetic loss of sdhb in patient 2s tumor ( fig 2b )  . wgs of patient 1s primary tumor to determine genetic events contributing to the pathogenesis of sdhb - deficient rcc , wgs of patient 1s tumor and matched normal tissue was performed to mean haploid coverage of approximately 903 with greater than 96% of the genome at > 303 . 
wgs identified only a single nonsynonymous somatic substitution ( srebf1 p.d329y ) with no significant impact based on functional prediction.57 copy number the tumor revealed few genomic analysis of alterations including loss of the short arm of chromosome 1 where sdhb resides ( fig 3 )  . 
furthermore , close examination of the sdhb locus in the retained allele found that both tumor and normal tissue have the same deletion spanning exons 4 and 5 of the sdhb coding sequence ( chr1 : 17 , 353 , 986 to 17 , 359 , 321 ; fig 3 ) , resulting in a frameshift mutation . 
altogether , a germline intragenic deletion in sdhb and a somatic loss of 1p resulted in complete loss of sdhb in the tumor ( fig 2b )  . wgs and clonal evolution of patient 3s primary and metastatic tumors wgs was performed on patient 3s primary kidney tumor as well as his metastatic liver and scapula bone lesions ( fig 4 and data supplement )  . 
of note , the same sdhb mutation has been reported in patients with gi stromal tumor and paraganglioma.58 detailed characterization of the subclonal structure using the substitution data established a long trunk with 5 , 198 of 8 , 047 substitutions in 100% of cells across tumor sites . 
the second largest subclone supported by 820 substitutions was present in approximately 55% and 100% of cells in the liver and bone metastases , respectively , likely reflecting tumor heterogeneity.46 overall , subclonal relationship among the three tumor sites suggests relatively late metastasis during clonal evolution . disruption of mitochondrial architecture in sdhb - deficient cancer cells because sdhb encodes a tca cycle protein , we examined the mitochondria morphology of patient 1s sdhb - deficient primary tumor cells under electron microscopy . 
 primary tumor 5 , 809 substitutions liver metastasis 0 10 20 30 40 50 60 5 , 916 substitutions 394 deletions and insertions 50 100 150 200 ( most recent common ancestor ) 81 rearrangements patient 3 mrca complex insertion deletion other deletion repeat deletion m - homology t . 
duplication deletion inversion translocation 50 100 150 99 rearrangements 0 10 20 30 40 50 60 70 8 , 817 substitutions 679 deletions and insertions complex insertion deletion other deletion repeat deletion m - homology t . 
whole - genome sequencing and clonal evolution analysis of patient 3s paired primarymetastatic kidney tumors . mrca denotes the most recent common ancestor cell identified during the cancer evolution of individual tumors.46 loh , loss of heterozygosity ; mtor , mammalian target of rapamycin . electron transport chain ( etc ) complex v , was used to inhibit mitochondrial oxygen consumption , thereby activating glycolysis , and carbonyl cyanide - 4 - ( trifluoromethoxy ) phenylhydrazone ( fccp ) , an uncoupler of the mitochondrial proton gradient , was used to induce maximum mitochondrial oxygen consumption . 
 ( d ) relative succinate levels . intracellular succinate was quantified by gas chromatographymass spectrometry and then normalized to cell number . error bars indicate standard deviation ( n = 3 )  . fccp , carbonyl cyanide4 - ( trifluoromethoxy ) phenylhydrazone . primary cell production at baseline as a result of the preexisting defect in oxidative respiration . 
measurement of intracellular metabolites showed that sdhb2 / 2 kidney cancer cells had increased succinate compared with sdhb + / 2 cells and rcc4 and a498 ( fig 5d ) , suggesting that loss of both copies of sdhb resulted in succinate accumulation . glutamine uptake in the sdhb - deficient kidney cancer to determine whether the use of other carbon sources was altered in sdhb - deficient kidney cancer , an 18f - glutamine pet was used to measure glutamine uptake in patient 2 ( fig 6a )  . patient 2s tumors exhibited elevated 18fglutamine uptake , implicating increased dependence on glutamine metabolisusing primary sdhb2 / 2 tumor cells from patient 1 , glutamine deprivation resulted in decreases in glutamate and succinate , which are downstream catabolites of glutamine ( fig 6b )  . 
similarly , lactate downstream of glucose metabolism was unaffected by glutamine deprivation ( fig 6b )  . furthermore , prolonged glutamine deprivation in sdhb2 / 2 tumor cells resulted in increased cell death ( fig 6c )  . discussion here we report three patients with sdhbdeficient lethal rcc . 
annexin v staining of apoptotic cells was determined in sdhb2 / 2 culture after 72 hours of glutamine deprivation . error bars indicate standard deviation ( n = 3 )  . ( d ) model depicts the increased glucose flux and lactate production in sdhb - deficient cancer cells . 
all three individuals carry distinct germline mutations in one copy of the sdhb gene , and through chromosome 1p loss , the remaining copy of sdhb is lost in their tumors , consistent with the knudson two - hit hypothesis.59 mitochondrion generates atp and provides biosynthetic intermediates via two interlinked processes ( ie , etc and tca cycle )  . 
unlike the other dedicated tca cycle enzymes , the sdh enzyme also functions as complex ii in etc , coupling oxidation of succinate to fumarate in the tca cycle with electron transfer to ubiquinone in the etc . 
sdh enzyme is highly conserved and consists of a , b , c , and d subunits , with sdha and sdhb as the catalytic subunits extending into the mitochondrial matrix and anchored to its inner membrane with sdhc and sdhd ( fig 6d )  . 
of note , homozygous mutations in sdha cause severe neurologic defects in infants , known as leigh syndrome , characterized by subacute necrotizing encephalomyelopathy , failure to thrive , ataxia , seizures , and severe lactic acidosis.37 to our knowledge , the association between chronic hyperlactatemia and overt metastatic sdhb kidney cancer has never been reported . metabolic assessment of patient 1s sdhb2 / 2 tumor cells demonstrated the uncoupling between etc and tca , manifested by the lack of oxidative phosphorylation , the overproduction of lactate , and the dependence on aerobic glycolysis , exemplifying the extreme warburg effect in human cancer ( fig 6d )  . 
the mechanisms by which sdhb loss might contribute to tumorigenesis have been investigated using cell - based assays and mouse paraganglioma models.60 - 63 these studies highlighted the role of accumulated succinate as an oncometabolite that inhibits a - ketoglutaratedependent dioxygenases , resulting in metabolic and epigenetic changes.60 - 63 in fact , our genomic study of these patients demonstrated that the complete loss of sdhb constitutes the first event in the pathogenesis of sdhbdeficient kidney cancer . from 2011 to 2015 , 4 , 328 patients were diagnosed with rcc at memorial sloan kettering cancer center , among whom eight ( 0.18% ) have sdhb - deficient rcc . 
limited clinical data presented in our small series suggested varied treatment benefit with vascular endothelial growth factor and possibly mammalian target of rapamycin inhibitors , and the use of glutaminase inhibitor in this rare disease deserves further investigation . 
hsieh honoraria : novartis , pfizer , chugai , eisai , cancer genomics consulting or advisory role : novartis , pfizer , chugai , eisai , cancer genomics research funding : novartis , pfizer , chugai , eisai , cancer genomics acknowledgment we dedicate this article to the patients and their families and are forever grateful for their inspirational courage instilled upon us when fighting against this deadly disease . ying - bei chen no relationship to disclose justin r . 
cheng no relationship to disclose ramaprasad srinivasan no relationship to disclose dayna oschwald no relationship to disclose affiliations support chung - han lee , gunes gundem , william lee , ying - bei chen , justin r . 
moch h , cubilla al , humphrey pa , et al : the 2016 who classification of tumours of the urinary system and male genital organspart a : renal , penile , and testicular tumours . 
hsieh jj , manley bj , khan n , et al : overcome tumor heterogeneity - imposed therapeutic barriers through convergent genomic biomarker discovery : a braided cancer river model of kidney cancer . 
ricketts cj , forman jr , rattenberry e , et al : tumor risks and genotype - phenotype - proteotype analysis in 358 patients with germline mutations in sdhb and sdhd . 
williamson sr , eble jn , amin mb , et al : succinate dehydrogenase - deficient renal cell carcinoma : detailed characterization of 11 tumors defining a unique subtype of renal cell carcinoma . 
lu j , tan m , cai q : the warburg effect in tumor progression : mitochondrial oxidative metabolism as an antimetastasis mechaniscancer lett 356 : 156 - 164 , 2015 27 . 
fraley ds , adler s , bruns fj , et al : stimulation of lactate production by administration of bicarbonate in a patient with a solid neoplasm and lactic acidosis . 
friedenberg as , brandoff de , schiffman fj : type b lactic acidosis as a severe metabolic complication in lymphoma and leukemia : a case series from a single institution and literature review . 
martinez - outschoorn ue , whitaker - menezes d , valsecchi m , et al : reverse warburg effect in a patient with aggressive b - cell lymphoma : is lactic acidosis a paraneoplastic syndrome ? semin oncol 40 : 403 - 418 , 2013 36 . 
xu j , pham cg , albanese sk , et al : mechanistically distinct cancer - associated mtor activation clusters predict sensitivity to rapamycj clin invest 126 : 3526 - 3540 , 2016 45 . 
miyakita h , tokunaga m , onda h , et al : significance of 18f - fluorodeoxyglucose positron emission tomography ( fdg - pet ) for detection of renal cell carcinoma and immunohistochemical glucose transporter 1 ( glut - 1 ) expression in the cancer . 
ho cl , chen s , ho km , et al : dual - tracer pet / ct in renal angiomyolipoma and subtypes of renal cell carcinoma . clin nucl med 37 : 1075 - 1082 , 2012 53 . 
voss mh , molina am , chen yb , et al : phase ii trial and correlative genomic analysis of everolimus plus bevacizumab in advanced non - clear cell renal cell carcinoma . 
collins n , dietzek a : contiguous bilateral head and neck paragangliomas in a carrier of the sdhb germline mutation . nucleic acids res 39 : e118 , 2011 j vasc surg 55 : 216 - 219 , 2012 59 . 
letouze e , martinelli c , loriot c , et al : sdh mutations establish a hypermethylator phenotype in paraganglioma . cancer cell 23 : 739 - 752 , 2013 61 . 
xiao m , yang h , xu w , et al : inhibition of a - kg - dependent histone and dna demethylases by fumarate and succinate that are accumulated in mutations of fh and sdh tumor suppressors . 
craig lockhart , md17 ; cristiana sessa , md18 ; thomas zander , md19 ; matthew ng , md , phd20 ; giuseppe curigliano , md , phd21 , 22 ; jennifer bendiske , mba23 ; xueying chen , phd23 ; somesh choudhury , phd23 ; diana graus - porta , phd24 ; nancy lewis , md23 ; jose manuel perez garcia , md , phd25 ; and mara jos e de miguel - luken , md , phd26 purpose concurrent pik3ca mutations and broblast growth factor receptor ( fgfr ) alterations occur in multiple cancer types , including estrogen receptorpositive breast cancer , bladder cancer , and endometrial cancer . 
archival tumor samples were sequenced to explore genomic correlates of response . results in combination , both agents were escalated to full , single - agent recommended doses ( alpelisib , 300 mg per day continuously ; ingratinib , 125 mg per day 3 weeks on followed by 1 week off )  . 
the toxicity prole of the combination was consistent with the established safety prole of each agent , although 71% of all patients required at least one treatment interruption or dose reduction . 
molecularly selected dose expansions in breast cancer and other solid tumors harboring pik3ca mutations , alone or in combination with fgfr alterations , identied sporadic responses , predominately in tumor types and genotypes previously dened to have sensitivity to these agents . conclusion the combination of alpelisib and ingratinib can be administered at full single - agent doses , although the high rate of dose interruption or reduction suggests long - term tolerability may be challenging . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction genome - driven oncology has been focused primarily , to date , on the targeting of individual genomic alterations present in each tumor.1 although this approach has led to the development of many highly effective therapies , 2 - 6 we now understand that most oncogenes exist within a complex genomic landscape characterized by additional alterations that may , themselves , be targetable or modify sensitivity to therapy.7 even in instances in which the paradigm of targeting an individual genomic alteration has been successful , adaptation of the tumor eventually leading to acquired resistance ultimately limits effectiveness . 
 hyman et al context key objective to determine if the - elective pi3k inhibitor alpelisib can be combined safely with the selective broblast growth factor receptor ( fgfr ) inhibitor ingratinib . knowledge generated alpelisib and ingratinib were successfully escalated in combination to full single - agent doses ; however , high rates of treatment interruption and dose reduction suggest long - term tolerability may be challenging . 
in exploratory signal - seeking cohorts of patients harboring dual pik3ca and fgfr1 - 3 alterations , no clear evidence of synergistic activity was observed . relevance additional studies are necessary to determine the potential role of combined pi3k and fgfr inhibition in treatment of various advanced solid tumors with alterations in pik3ca and / or fgfr1 - 3 . suggested that the combined inhibition of these oncogenes might be benecial.14 moreover , in breast cancer , pik3ca mutations often co - occur with fgfr1 gene amplications , indicating pik3ca and fgfr1 could cooperate as potential dual oncogenic drivers in this tumor type.12 , 15 similarly , concurrent activating pik3ca and fgfr2 mutations have been observed in endometrial carcinomas , with 90% or more fgfr2 - mutant endometrial cancers also exhibiting genomic activation of the pi3k pathway.16 - 18 taken together , these data provided a rationale for evaluating the feasibility and preliminary activity of combined fgfr and pik3ca inhibition in the clinic . to evaluate this therapeutic strategy , we studied the combination of alpelisib ( byl719 ) and ingratinib ( bgj398 )  . 
alpelisib is a selective class i pi3k inhibitor that recently demonstrated a statistically signicant and clinically relevant improvement in progression - free survival in a phase iii study ( solar - 1 ) of patients with pik3camutant , er + metastatic breast cancer.19 ingratinib is an orally bioavailable , selective pan - fgfr kinase inhibitor that has demonstrated single - agent activity in fgfr2 / 3altered bladder cancers and fgfr2 fusion - positive cholangiocarcinomas.20 , 21 we hypothesized that the combination of a selective fgfr and pik3ca inhibitors would be safe and would synergize in tumors with concurrent alteration of these oncogenes . 
dose escalation was guided by a bayesian logistic regression model with escalation with overdose control.22 in total , three arms in the expansion cohort were planned : dual pik3camutant and fgfr - altered breast ( arm 1 ) and nonbreast ( arm 2 ) cancers and pik3ca - mutant solid tumors ( arm 3 )  . because of the slow rate of accrual and overall safety prole , the study was closed before the target enrollment was completed . the primary objective was to determine the maximum tolerated dose and / or recommended dose for expansion of the combination of ingratinib and alpelisib . 
the secondary objectives included assessment of safety and tolerability of the combination , characterization of pharmacokinetic ( pk ) proles , assessment of preliminary antitumor activity as measured by overall response rate ( orr ) , and progressionfree survival ( pfs ) , per recist , version 1.1. study drug administration eligibility patients were at least 18 years of age and had advanced solid tumors with pik3ca mutation with or without fgfr genetic alteration in which standard therapy was unsuccessful . 
patients remained in the study until disease progression , unacceptable adverse investigator events ( aes ) , or withdrawal at patient or discretion . study assessments tumor responses were measured by recist , version 1.1 ( investigator assessed ) , using computed tomography or magnetic resonance imaging.23 assessments were performed at screening and every 8 weeks after rst treatment until disease progression . 
safety was monitored throughout institute the study according to the national cancer common terminology criteria for adverse events , version 4.03.24 ecgs were assessed and independently reviewed by a central laboratory . pharmacokinetic analysis during dose escalation , blood samples were collected to measure alpelisib and ingratinib plasma concentrations . samples were collected predose and 0.5 , 1 , 2 , 3 , 4 , 6 , 8 , and 24 hours postdose on cycle 1 day 1 , cycle 1 day 15 , and cycle 2 day 1 . 
drug plasma concentrations ( and active metabolites ) were measured using validated liquid chromatographytandem mass spectrometry with a lower limit of quantication of 1 ng / ml . genomic sequencing genomic alterations potentially associated with fgfr and pik3ca signaling were assessed from archival tumor specimens of fresh , pretreatment tumor biopsy specimens . for samples with sufcient tissue material ( n = 41 ) , nextgeneration sequencing ( ngs ) analysis was performed in a clinical laboratory improvement amendmentscertied laboratory ( foundation medicine , cambridge , ma ) using previously published methods.25 statistical analysis the data cutoff for all statistical analyses was august 23 , 2016 . 
the sample size for each expansion cohort was selected primarily for continued safety evaluation and was not powered for any specic efcacy end point . results patient demographics a total of 62 patients were enrolled in the study between october 2013 and august 2016 across 22 clinical centers in 12 countries . 
the median age of patients at the time of study entry was 60 ( range , 30 to 78 ) years , and all patients had an eastern cooperative oncology group performance status of 1 or less . 
patients were heavily pretreated , having received a median of three prior lines of systemic therapy . safety and tolerability dose - limiting toxicities were reported in three patients ( 10.7% ) who were included in the dose - escalation cohort ( n = 38 ) during the rst 28 days of treatment . 
dose - limiting toxicities included grade 4 hyperglycemia in one patient receiving alpelisib 300 mg and ingratinib 40 mg ; and grade 3 stomatitis in two patients ( one receiving alpelisib 300 mg and ingratinib 75 mg ; and the other receiving alpelisib 300 mg and ingratinib 100 mg )  . 
the recommended dose for expansion was determined to be alpelisib 300 mg once per day ( administered continuously ) and ingratinib 125 mg once per day ( administered on a schedule of 3 weeks on followed by 1 week off )  . overall , the safety prole of alpelisib and ingratinib was similar to the known safety proles of each agent ; no new major aes were noted ( table 2 )  . 
serious aes suspected to be drug related were reported in 12.9% of patients ( n = 8 of 62 ) overall and 16.1% ( n = 5 of 31 ) treated at the recommended dose for expansion . 
a total of 13 deaths ( 21% ) were reported during the study , including three ( 4.8% ) deaths resulting from disease progression while the patient was receiving study treatment . 
similarly , hyperglycemia , which is a biomarker of on - target pi3k inhibition , was also observed in 38.7% of all patients treated with alpelisib 200 mg or 300 mg , consistent with prior experience with this agent.27 for ingratinib , 37 patients ( 59.7% ) reported at least one dose interruption and 23 patients ( 37.1% ) reported at least one dose reduction . 
there was no or negligible pk interaction between ingratinib and alpelisib . antitumor efcacy in total , 52 patients were evaluable for response and 10 ( n = 6 in the dose escalation study ; n = 4 in the dose expansion study ) were nonevaluable on the basis of discontinuing therapy before the rst disease assessment ( table 3 )  . 
among 60 patients with a locally annotated pik3ca mutation reported , sequencing with high condence coverage was obtained centrally in 35 samples and the locally reported pik3ca variant conrmed in 80% patients ( n = 28 of 35 )  . 
 ( % ) , except where n = 0 . abbreviations : cr , complete response ; pd , progressive disease . * for patients who only had nontarget lesions at baseline and did not experience either a cr or pd , response is reported as non - cr / non - pd . patient with unknown best overall response due to ( 1 ) no valid postbaseline assessment , or ( 2 ) stable disease occurred too early ( , 6 weeks ) dened as patients who have best overall response cr , partial response , or stable disease , in which stable disease needs to occur at least 6 weeks after the rst dosing . squamous anal cancer with pik3ca e545k mutation . 
interestingly , in the patient with melanoma who had a pr , the only genomic activation of either pathway identied by central sequencing was an fgfr2 m722i mutation , an alteration not known to be recurrent or of biologic signicance.27 we also explored whether genetic alterations of the mapk pathway co - occurred with mutations in the fgfr and / or pi3k pathways and may account for lack of response , at least partially , in those settings . 
overall , ngs studies showed no clear association of alterations in the fgfr , pi3k , or mapk pathways with response . discussion to our knowledge , this is the rst study to evaluate the safety and preliminary efcacy of combined selective pi3k and fgfr inhibition in patients . 
we dened a recommended dose for expansion of alpelisib 300 mg once per day and ingratinib 125 mg once per day , 3 weeks on followed by 1 week off , which is the full single - agent dose and schedule of each drug . 
although this combination did not raise new specic safety concerns , 71% of patients required a dose interruption of alpelisib and 60% of patients reported at least one dose interruption of ingratinib during the course of treatment . 
of note , dose interruptions in the range of 50% to 70% have previously been reported with each agent when used individually , again suggesting that their combination may not be associated with signicant additive toxicity over the component parts but that long - term tolerance each drug alone can exhibit issues.20 , 28 , 29 no drug - drug interactions were reported between ingratinib and alpelisib . this study does have some important limitations . 
the relatively small number of patients treated with relevant concurrent alterations , as well as the heterogeneity of the population , do not permit a denitive assessment of synergistic efcacy . as such , any efcacy data presented from these expansions should be considered hypothesis generating only . second , we note that in the subset of 58% of patients ( n = 35 of 60 ) with tumor tissue in which successful central sequencing was completed , the pik3ca mutations were centrally conrmed in 80% of patients . 
as a result , some patients may have been enrolled on the basis of pik3ca mutations characterized by subclonality , spatial or temporal heterogeneity , or even test failures , as has been observed in prior genome - driven studies.7 finally , enrollment in the expansion cohorts for patients harboring concurrent pik3ca and fgfr1 - 3 alterations was not restricted to variants functionally characterized as activating but to regions of the affected genes that are recurrently the target of alteration . 
efcacy by ( a ) a waterfall plot depicting best percent change in the target tumor burden from baseline according to cohort and ( b ) a swimmer plot depicting progression - free survival by patients according to cohort . 
integrated genomic analysis of efcacy according to mutations in the fgfr , pi3k , and mapk pathways by central next - generation sequencing . ( * ) missing response data , as a result of discontinuation before rst response assessment . 
indel , insertion and / or deletion . fgfr amplication is partially dependent on the degree of amplication.30 both the inclusion of variants of unknown signicance as well as copy number amplications with a specic fold - change requirement may have adversely affected the observed orr by enrolling tumors without true pathway dependency on fgfr . despite these important limitations , a relatively low orr of only 9.7% across the entire study suggests that these two classes of agents may not provide synergistic activity . moreover , responses were generally observed in tumors arising from anatomic sites and harboring genetic alterations previously described as sensitizing to either alpelisib or ingratinib . 
it is also noteworthy that a signicant proportion of patients did not respond , or had stable disease as their best response , despite harboring pik3ca mutations alone or in combination with fgfr alterations . 
 hyman et al implementation has been identication of targeted therapy combinations have often been cited as a means of overcoming both intrinsic and acquired resistance , but a number of scientic , technical , and logistic impediments have made successful implementation challenging.31 , 32 perhaps the most difcult barrier to successful right drug combinations . 
enrichment for concurrent alterations of two oncogenes in one or multiple cancer types has served as one basis for selecting potential drug combinations and formed the basis of the hypothesis evaluated in this clinical study . 
recently , ndings were reported from two precision medicine studies , i - predict and winther , suggesting that a higher degree of molecular matching between somatic alterations detected at baseline and the therapy administered was associated with improved outcomes.33 , 34 although these results imply that targeting multiple oncogenic alterations with polytherapy may be a worthwhile strategy in select circumstances , the data presented here demonstrate that more rigorous evaluation of specic biomarker and drug combinations is required before the approach is more widely embraced . in conclusion , the combination of pik3ca and fgfr inhibition with alpelisib and ingratinib was feasible , although overall tolerability was limited by each agent . 
schellens , mario campone , cristiana sessa , giuseppe curigliano , jennifer bendiske , xueying chen , somesh choudhury , nancy lewis , jose manuel perez garcia , mara jos e de miguel - luken provision of study material or patients : luis paz - ares , jan h . 
craig lockhart , cristiana sessa , thomas zander , matthew ng , giuseppe curigliano , jose manuel perez garcia , mara jos e de miguel - luken collection and assembly of data : david m . 
craig lockhart , cristiana sessa , thomas zander , giuseppe curigliano , xueying chen , somesh choudhury , nancy lewis , jose manuel perez garcia , mara jos e de miguel - luken data analysis and interpretation : david m . 
schellens employment : modra pharmaceuticals stock and other ownership interests : modra pharmaceuticals honoraria : debiopharm group consulting or advisory role : debiopharm group research funding : dutch cancer society ( inst ) patents , royalties , other intellectual property : patent on oral taxanes philippe l . 
bedard research funding : bristol - myers squibb ( inst ) , sano ( inst ) , astrazeneca ( inst ) , roche ( inst ) , servier ( inst ) , glaxosmithkline ( inst ) , novartis ( inst ) , signalchem ( inst ) , ptc therapeutics ( inst ) , nektar ( inst ) , merck ( inst ) , seattle genetics ( inst ) , mersana ( inst ) , immunomedics ( inst ) , eli lilly ( inst ) mario campone honoraria : novartis , eli lilly consulting or advisory role : novartis ( inst ) , servier ( inst ) , menarini , sano ( inst ) , eli lilly ( inst ) , pzer ( inst ) , astrazeneca / medimmune ( inst ) , abbvie ( inst ) , pierre fabre ( inst ) , accord ( inst ) , sandoz - novartis ( inst ) speakers bureau : novartis , amgen research funding : novartis ( inst ) travel , accommodations , expenses : novartis , astra zeneca , pzer other relationship : roche philippe a . 
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all four patients received selpercatinib ( capsule or liquid formulation ) orally in continuous 28 - day cycles at a starting dose of 90 mg / m2 twice per day . this dose was intended to deliver exposure equivalent to the recommended adult phase ii dose of 160 mg twice per day . 
one patient was enrolled to the 80 - mg cohort of trial ( clinicaltrials.gov identier : nct03157128 ) and underwent intrapatient dose escalation to 160 mg per protocol . the ongoing selpercatinib phase i / ii pharmacokinetic analysis serial blood samples were collected for pharmacokinetic analyses . 
molecular analysis showed that the tumor harbored an ret exon 6 deletion ( d378_ g685.e ) , and the patient was treated sequentially with four multitargeted kinase inhibitors : vandetanib , sunitinib , cabozantinib , and lenvatinib , which were each discontinued because of either adverse events or lack of efcacy . 
a 7 - year - old boy with neonatal hypotonia , abdominal pain , hollow feet , and unexplained laryngeal spasms was referred for diagnostic exome sequencing of genomic dna ( sureselect xt clinical research exome , agilent , santa clara , ca )  . 
this revealed a constitutional de novo ret m918t mutation , a pathogenic variant associated with men2b that confers the highest risk of early onset mtc.16 the patient was subsequently diagnosed with an mtc and underwent thyroidectomy with tracheostomy followed by vandetanib therapy , which was discontinued because of the onset of grade 3 colitis . selpercatinib was subsequently initiated at 90 mg twice per day . 
magnetic resonance imaging demonstrated new lung nodules indicative of metastatic disease . an rna - based next - generation sequencing ( ngs ) fusion assay ( solid fusion assay v2 ; archerdx , boulder , co ) indicated that the tumor harbored an myh10 - ret gene fusion . 
the patient was started on vandetanib and achieved a partial tumor response by response evaluation criteria in solid tumors ( recist ) 1.1.22 however , after 4 months of treatment , she developed disease progression at the primary site . 
repeat imaging after 6 months of treatment showed complete resolution of the paraspinal mass and a 50% decrease in the size of the retroperitoneal , pelvic , and lumbosacral mass ( fig 2a - d )  . 
during repair of congenital bilateral inguinal hernias , a 2 - month - old girl was found to have a right renal mass , and she underwent a right nephrectomy . 
patient 1 : magnetic resonance imaging scans of ( a ) right lateral and ( b ) left anterior liver metastatic lesions at baseline and after 22 months of treatment with selpercatinib of ( c ) right lateral and ( d ) left anterior in a heavily pretreated patient with ret - mutated medullary thyroid cancer . 
patient 3 : ( a , c ) computed tomography ( ct ) scans of the abdomen at baseline and ( b , d ) after 6 months of treatment with selpercatinib , revealing multiple paraspinal retroperitoneal and pelvic lesions in a patient with infantile myobroma / hemangiopericytoma harboring an myh10 - ret fusion . 
a partial response was observed after one cycle of selpercatinib ; after six cycles , the paraspinal lesion had completely resolved , and the patient regained lower extremity neurologic function . 
patient 4 : ct scans at baseline of ( e ) the lungs and ( g ) brain and after 8 months of treatment with selpercatinib of ( f ) the lungs and ( h ) brain in a patient with an specc1l - ret fusionpositive congenital mesoblastic nephroma and infantile brosarcoma . 
patient 5 : ct scans ( i , k ) at baseline and ( j , l ) after 2 months of treatment with selpercatinib of the left foot in a patient with an ncoa4 - ret fusionpositive lipobromatosis . 
abdominal ultrasound and chest x - ray identied a mass in the left kidney and a large left lower lung mass ; computed tomography imaging conrmed these lesions and identied additional , multiple small lung lesions . 
biopsy of a lung mass revealed high - grade spindle cell sarcoma consistent with an infantile brosarcoma ; pathology review of the original right nephrectomy specimen conrmed the initial diagnosis of mesoblastic nephroma . 
the patient received additional chemotherapy with cyclophosphamide and topotecan , but treatment was complicated by febrile neutropenia and enterococcus faecalis ventriculitis . dna - based ngs ( using memorial sloan kettering integrated mutation proling of actionable cancer targets [ msk - impact ] ) of the tumor from the renal and lung masses identied the same specc1l - ret gene fusion , and the patient initiated treatment with selpercatinib . after two cycles , a partial response was observed with a 41% tumor reduction , ( fig 2e - h )  . 
a selpercatinib concentration of 4.5 ng / ml was achieved in cerebrospinal uid at a dose level of 48 mg twice per day ( 90 mg / m2 per dose )  . upon detection and resection of an isolated metastasis at the right posterior temporal occipital junction , the dose of selpercatinib was increased to 94 mg ( 180 mg / m2 ) twice per day , raising the concentration of the drug to 16 ng / ml in the cerebrospinal uid . 
 selpercatinib in pediatric ret - altered cancer libretto - 001 ( 160 mg , day 8 ) patient 3 patient 4 patient 5 6 , 000 4 , 000 2 , 000 time ( hours ) fig 3 . 
plasma samples from three patients revealed that adequate plasma concentrations of selpercatinib were achieved ( greater than ret wild - type concentration that inhibits 90% [ ic90 ] ) , which were within the range seen in adult patients treated with the recommended dose of 160 mg in the libretto - 001 trial . 
the gray area represents the 95% cis for the median plasma concentrations observed in patients treated in the libretto - 001 trial ( red circles )  . fusion , which was conrmed by whole genome and transcriptome analysis . 
selpercatinib was initiated , and imaging after 2 months revealed a partial response by recist 1.1 , with a 59% reduction in tumor volume and resolution of tumor inltration of the metatarsals ( fig 2i - l )  . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . sandya govinda raju employment : loxo oncology dahlia henry employment : loxo oncology stock and other ownership interests : loxo oncology , allergan , axovant sciences , palatin technologies steve smith consulting or advisory role : various , loxo oncology patents , royalties , other intellectual property : various patents and applications travel , accommodations , expenses : various s . 
cox employment : bayer , loxo oncology , merck kgaa , amgen , day one biopharmaceuticals stock and other ownership interests : loxo oncology , bayer , merck kgaa , amgen , day one biopharmaceuticals patents , royalties , other intellectual property : us patent 62 / 318 , 041 issued to loxo oncology ( inst ) julia glade bender consulting or advisory role : abbvie ( inst ) research funding : celgene ( inst ) , merck ( inst ) , pzer ( inst ) , amgen ( inst ) , ignyta ( inst ) , bristol - myers squibb ( inst ) , eisai ( inst ) , novartis ( inst ) , eli lilly ( inst ) , loxo oncology ( inst ) , genentech ( inst ) travel , accommodations , expenses : novartis , amgen , merck , bayer , genentech uncompensated relationships : springworks therapeutics , bristol - myers squibb a . 
lindsay frazier stock and other ownership interests : decibel therapeutics consulting or advisory role : decibel therapeutics peter anderson stock and other ownership interests : healios consulting or advisory role : enlivity patents , royalties , other intellectual property : patent for glutamine and trehalose compositions ; priority date 13 september 2013 ; app 14 / 470 , 545 , led august 27 , 2014 ; patent 61 / 878 , 084 issued december 26 , 2017 other relationship : enlivity alberto s . 
pappo honoraria : bayer , roche consulting or advisory role : merck , loxo oncology / bayer , eusa pharma no other potential conicts of interest were reported . acknowledgments we thank the patients and their families and contributing clinical staff across all sites . 
medical writing services were provided by jim heighway of cancer communications and consultancy , knutsford , united kingdom , and were funded by loxo oncology , stamford , ct . references kato s , subbiah v , marchlik e , et al : ret aberrations in diverse cancers : next - generation sequencing of 4 , 871 patients . 
clin cancer res 23 : 1988 - 1997 , 2017 ceccherini i , pasini b , pacini f , et al : somatic in frame deletions not involving juxtamembranous cysteine residues strongly activate the ret proto - oncogene . oncogene 14 : 2609 - 2612 , 1997 prescott jd , zeiger ma : the ret oncogene in papillary thyroid carcinoma . 
nat commun 9 : 4821 , 2018 ferrara r , auger n , auclin e , et al : clinical and translational implications of ret rearrangements in non - small cell lung cancer . 
j thorac oncol 13 : 27 - 45 , 2018 cordioli mi , moraes l , bastos au , et al : fusion oncogenes are the main genetic events found in sporadic papillary thyroid carcinomas from children . 
thyroid 27 : 182 - 188 , 2017 fenton cl , lukes y , nicholson d , et al : the ret / ptc mutations are common in sporadic papillary thyroid carcinoma of children and young adults . 
j clin endocrinol metab 85 : 1170 - 1175 , 2000 prasad ml , vyas m , horne mj , et al : ntrk fusion oncogenes in pediatric papillary thyroid carcinoma in northeast united states . 
cancer 122 : 1097 - 1107 , 2016 vanden borre p , schrock ab , anderson pm , et al : pediatric , adolescent , and young adult thyroid carcinoma harbors frequent and diverse targetable genomic alterations , including kinase fusions . 
carvalho d , mackay a , bjerke l , et al : the prognostic role of intragenic copy number breakpoints and identication of novel fusion genes in paediatric high 11 . 
al - ibraheemi a , folpe al , perez - atayde ar , et al : aberrant receptor tyrosine kinase signaling in lipobromatosis : a clinicopathological and molecular genetic grade glioma . 
antonescu cr , suurmeijer aj , zhang l , et al : molecular characterization of inammatory myobroblastic tumors with frequent alk and ros1 gene fusions and rare novel ret rearrangement . 
elisei r , cosci b , romei c , et al : prognostic signicance of somatic ret oncogene mutations in sporadic medullary thyroid cancer : a 10 - year follow - up study . j clin endocrinol metab 93 : 682 - 687 , 2008 16 . 
latteyer s , klein - hitpass l , khandanpour c , et al : a 6 - base pair in frame germline deletion in exon 7 of ret leads to increased ret phosphorylation , erk activation , and men2a . 
wirth lj , kohno t , udagawa h , et al : emergence and targeting of acquired and hereditary resistance to multikinase ret inhibition in patients with ret - altered 20 . 
drilon ae , subbiah v , oxnard gr , et al : a phase 1 study of loxo - 292 , a potent and highly selective ret inhibitor , in patients with ret - altered cancers . 
antonescu cr , dickson bc , swanson d , et al : spindle cell tumors with ret gene fusions exhibit a morphologic spectrum akin to tumors with ntrk gene 26 . 
wells sa jr , robinson bg , gagel rf , et al : vandetanib in patients with locally advanced or metastatic medullary thyroid cancer : a randomized , double - blind 28 . 
schlumberger m , jarzab b , cabanillas me , et al : a phase ii trial of the multitargeted tyrosine kinase inhibitor lenvatinib ( e7080 ) in advanced medullary thyroid 30 . 
gautschi o , milia j , filleron t , et al : targeting ret in patients with ret - rearranged lung cancers : results from the global , multicenter ret registry . 
yoh k , seto t , satouchi m , et al : vandetanib in patients with previously treated ret - rearranged advanced non - small - cell lung cancer ( luret ) : an open - label , multicentre phase 2 trial . 
 emerging role for precision therapy through next - generation sequencing for sarcomas see accompanying article doi : sarcomas are rare malignancies , collectively accounting for only 1% of adult and 15% of pediatric cancers . 
there are at least 100 different histologic subtypes of bone and soft tissue cancers , and significant genetic and biologic heterogeneity exists within the more common subtypes , such as high - grade pleomorphic sarcomas , liposarcomas , and leiomyosarcomas.1 as a result , development of novel therapies for sarcoma has been slow , because of the difficulty in conducting large clinical trials for rare and heterogeneous populations . 
particularly in smaller phase ii trials , signals of activity can be diluted by the inclusion of many different sarcoma histologies , with limited power to detect predictive biomarkers for patients likely to respond . 
 although cytotoxic chemotherapies have greatly improved cure rates for localized pediatric sarcomas , such as ewing sarcoma , rhabdomyosarcoma , and osteosarcoma , metastatic sarcomas remain incurable in most cases , with median overall survival of 12 to 18 months.2 thus , novel therapies are desperately needed for this challenging group of cancers . recently , wu et al3 presented a pediatric patient with an aggressive , poorly differentiated retroperitoneal sarcoma found to harbor a fusion of ntrk2 . 
shortly thereafter , the patient was enrolled in a clinical trial using larotrectinib , which subsequently led to a dramatic and prolonged clinical improvement of her cancer symptoms , with a near - complete response that has lasted more than 1 year . 
she exhibited an early and dramatic clinical tumor response . the tropomyosin - related kinase ( trk ) family of proteins are receptor tyrosine kinases encoded by the neurotrophic receptor tyrosine kinase 1 , 2 , and 3 ( ntrk1 , 2 , and 3 ) that are activated by their ligands : nerve growth factor , brain - derived growth factor , and neurotrophin 3 / 4.5 there have been many different fusion partners that seem to drive the development of cancers , with several drugs currently in development that target these fusions , including larotrectinib and entrectenib.6 , 7 these drugs have had astonishing efficacy and , importantly , seem to have activity regardless of cancer subtype . 
for example , larotrectinib showed a 75% response rate and 13% complete response rate in ntrk - associated tumors , with median durations of response and median progression - free survival not reached in this study.6 although incidence of these fusions in most cancers is low , the importance of finding these alterations cannot be overemphasized . in the last 20 years , cancer therapy has dramatically evolved by advances in genetics and molecular biology . 
 facilitated diagnostic capabilities in cases where immunohistochemistry and pathology review have been indeterminate . in the article that accompanies this editorial , boddu et al8 present their data on a single institution experience using ngs in patients with sarcoma . 
from a total population of 114 patients , they report a median of three ( range , zero to 19 ) driver variants per tumor tested , with the most common variants being found in tp53 , cdkn2a / b , cdk4 , mdm2 , atrx , and rb1 . 
 perhaps more importantly , five patients ( 4.4% ) ended up having a change in their pathology on the basis of sequencing findings ( including a new diagnosis of a desmoid tumor , synovial sarcoma , and several more specific subtypes of small round blue cell tumors )  . gounder et al9 recently reported a retrospective analysis of more than 5 , 700 patients who underwent ngs with the foundation medicine genomic profiling platforthe results of genomic profiling changed or refined the pathologic diagnosis in 8% of patients . 
in addition , 8% of patients were found to have genetic mutations that were already biomarkers for approved drugs for sarcoma , whereas an additional 9% of patients had genetic biomarkers associated with approved drugs for other cancers . 
overall , for the majority of patients , genetic profiling identified potential therapeutic options either as standard of care or clinical trial opportunities . in some sarcoma subtypes , targeted therapies have shown remarkable efficacy and have become the standard - of - care approach over traditional chemotherapy ( table 1 )  . 
in 2000 , gastrointestinal stromal tumors ( gists ) were first identified to carry activating mutations in kit , and clinical trials of imatinib produced remarkable and durable responses in these sarcomas that were completely resistant to cytotoxic chemotherapy . 
however , although 70% of gists will carry exon 11 mutations , up to 10% of gists have now been shown to be driven from other genetic mutations , many of which are resistant to imatinib.10 to avoid futile therapy at diagnosis , the national comprehensive cancer network guidelines recommend mutation testing for all patients who are planned to be treated with imatinib . 
novel kit inhibitors are being rationally designed to target these mutations ; thus , biopsy at relapse may allow more strategic enrollment in clinical trials , with agents likely to target the specific alterations identified . despite the advances for these subtypes , the majority of mutations and abnormalities identified in metastatic sarcomas are still lacking effective therapies . 
in a recently published analysis from the cancer genome atlas network , multiplatform genomic characterization of 206 soft tissue sarcomas ( leiomyosarcomas , pleomorphic sarcomas , dedifferentiated liposarcomas , myxofibrosarcomas , synovial sarcoma , and malignant peripheral nerve sheath tumors ) revealed that the majority of tumors are characterized predominantly by copy - number changes , with low mutational loads and only a few conserved recurrent genetic mutations across subtypes , including tp53 , atrx , and rb1.11 however , in some subsets , clustering was able to identify genetic signatures associated with prognosis and potentially allow for better stratification of patients for future clinical trials . 
for example , in dedifferentiated liposarcomas , somatic copy - number alteration analysis and dna methylation data revealed three distinct clusters : k1 ( jun amplified ) , k2 ( tert amplified and chromosomally unstable ) , and k3 ( 6q25.1 amplified with fewer unbalanced segments )  . 
 efforts to develop validation trials on the basis of these and other identified genetic subsets will be critical to better customize therapy and improve outcomes . in summary , better understanding of key oncogenic driver mutations and fusions along with development of potent , specific inhibitors is creating meaningful treatment options for patients who do not respond to traditional therapies . 
selected examples of targeted therapy options for sarcomas and other bone / soft tissue tumors sarcoma histologic subtype genetic driver therapies gi stromal tumor c - kit exon 11 ( 70% ) exon 9 ( 10% ) exon 13 / 14 / 17 ( < 1% ) pdgfr ( 10% ) exon 12 exon 18 d842v sdh deficient raf v600e nf - 1 pi3k igf - 1r overexpression ntrk fusions imatinib 400 mg imatinib 800 mg imatinib resistant panotinib * imatinib imatinib resistant crenolanib or avapritinib * sunitinib or regorafenib raf inhibitor raf inhibitor * raf / mek inhibitors * pi3k inhibitors igf - 1r inhibitors * larotrectinib * dermatofibrosarcoma protuberans t ( 17 ; 22 ) ( fusion col1a1 / pdgfb ) > pdgf - b imatinib alveolar soft part sarcoma cediranib , sunitinib , pazopanib t ( 17 ; x ) ( fusion asps1 / tfe3 ) > vegf cofactors tsc1 / tsc2 mutations > mtorch1 activation perivascular epithelial cell tumor ( pecoma ) sirolimus , temsirolimus desmoid fibromatosis giant cell tumor of bone notch signaling gamma secretase inhibitors * rank / rank ligand overexpression denosumab pigmented villonodular synovitis t ( 1 ; 2 ) translocation ( collagen / ) csf1 > csf1 csf1r inhibitors * inflammatory myofibroblastic tumor alk rearrangements dedifferentiated liposarcomas cdk4 / mdm2 amplification solitary fibrous tumor epithelioid sarcoma chondrosarcomas ewing sarcoma ini1 loss idh1 / idh2 mutations ews - fli1 translocation crizotinib palbociclib ezh2 inhibitors idh inhibitors * nab2 - stat6 translocation > vegf temozolomide / bevacizumab abbreviations : csf1r , colony stimulating factor 1 receptor ; igfr1 , insulin growth factor receptor 1 ; vegf , vascular endothelial growth factor . * being explored in ongoing clinical trials . tk - 216 ( disrupts binding of fusion protein to rna helicase a ) * alterations such as ntrk fusions in sarcomas remains relatively low , the potential benefit for this subset of patients is without question . 
wu lw , pavlock t , patterson a , et al : durable clinical response to larotrectinib in an adolescent patient with an undifferentiated sarcoma harboring an strn - ntrk2 fusion . 
doebele rc , davis le , vaishnavi a , et al : an oncogenic ntrk fusion in a soft tissue sarcoma patient with response to the tropomyosin - related kinase ( trk ) inhibitor loxo - 101 . 
drilon a , siena s , ou s - hi , et al : safety and antitumor activity of the multi - targeted pan - trk , ros1 , and alk inhibitor entrectinib ( rxdx - 101 ) : combined results from two phase 1 trials ( alka - 372 - 001 and startrk - 1 )  . 
gounder mm , ali sm , robinson v , et al : impact of next - generation sequencing ( ngs ) on diagnostic and therapeutic options in soft - tissue and bone sarcoma . 
blay jy , le cesne a , cassier pa , et al : gastrointestinal stromal tumors ( gist ) : a rare entity , a tumor model for personalized therapy , and yet ten different molecular subtypes . 
donahue , md , memorial sloan kettering cancer center , department of surgery , 353 east 68th st , new york , ny 10065 ; e - mail : donahuet@mskcc.org. purpose patients with lynch syndrome ( ls ) have a significantly increased risk of developing upper - tract urothelial carcinoma ( utuc )  . 
here , we sought to identify differences in the patterns of mutational changes in ls - associated versus sporadic utucs . patients and methods we performed targeted sequencing of 17 utucs from patients with documented ls - associated germline mutations ( ls - utucs ) using the memorial sloan kettering integrated molecular profiling of actionable cancer targets targeted exon capture assay and compared the results with those from a recently characterized cohort of 82 patients with sporadic utuc . results patients with ls - utuc were significantly younger , had had less exposure to tobacco , and more often presented with a ureteral primary site compared with patients with sporadic utuc . 
although fgfr3 mutations were identified in both cohorts , the r248c hotspot mutation was highly enriched in ls - utuc . conclusion lsand sporadic utucs have overlapping but distinct genetic signatures . 
2018 by american society of clinical oncology introduction lynch syndrome ( ls ) is an autosomal dominant cancer predisposition syndrome caused by germline mutations in the mismatch repair ( mmr ) genes mlh1 , msh2 , msh6 , or pms2 . 
 patients with ls have an increased risk of developing a variety of tumors , particularly those arising in the colon , but also extracolonic cancers , including urothelial carcinomas ( ucs ) .1 - 3 uc is the third most frequent malignancy in ls , occurring in approximately 5% of patients.3 , 4 patients with ls have up to a 22 - fold greater risk of developing upper - tract urothelial carcinoma ( ls - utuc ) over the general population and a median age of onset 10 to 15 years earlier than patients with sporadic utuc.2 - 5 although both uc of the bladder ( ucb ) and utuc are believed to arise from a common precursor cell population within the urothelium , increasing evidence suggests that these two malignancies represent different disease entities from both clinicopathologic and genetic perspectives.6 - 10 in support of this concept , tumor genomic sequencing of ucb and utuc has identified distinct mutational profiles between these two urothelial malignancies.11 , 12 here , we sought to determine whether patients with utuc with known germline mutations uniformly harbored loss of heterozygosity of the wild - type allele of the gene that was the basis of their ls diagnosis and whether their tumors exhibited a pattern of hypermutation consistent with mmr deficiency . 
the ccfr activities are conducted across six multipleprincipal investigator sites and six subaward sites : university of melbourne ( melbourne , victoria , australia ) , fred hutchinson cancer research center ( seattle , wa ) , sinai health system ( comprising mount sinai hospital and lunenfeld tanenbaum research institute [ toronto , ontario , canada ] ) , mayo clinic ( mayo clinic arizona [ scottsdale , az ] with a subaward to mayo clinic minnesota [ rochester , mn ] ) , cedars - sinai consortium ( comprising cedars - sinai medical center [ los angeles , ca ] with subawards to cleveland clinic [ cleveland , oh ] , university of minnesota [ minneapolis , mn ] , dartmouth college [ hanover , nh ] , and university of virginia [ charlottesville , va ] ) , and university of hawaii ( university of hawaii medical center [ honolulu , hi ] with a subaward to cancer prevention institute of california [ fremont , ca ] )  . 
a previously characterized cohort of 82 patients with presumed sporadic utuc treated with radical nephroureterectomy was used as a comparison group.11 germline dna was extracted from peripheral blood lymphocytes provided by the ccfr for each patient . 
when not provided by the ccfr , dna was extracted from paraffin sections as previously described.12 clinical and demographic information were obtained from the prospectively maintained registry of the ccfr . targeted sequencing all protein - coding exons of 341 cancer - associated genes were sequenced using the memorial sloan kettering integrated molecular profiling of actionable cancer targets ( msk - impact ) assay as previously described ( data supplement ) .14 all candidate mutations and indels were reviewed manually . 
the quasi p value for a particular signature was calculated as the fraction of samples with a signature proportion greater than a precalculated noise threshold ( 1 105 )  . 
all analyses were conducted using r software ( version 2.13.1 ; r foundation , vienna , austria )  . results genomic characterization of ls - utuc of the 21 tumors analyzed , four were reclassified as renal cell carcinoma ( rcc ) on central pathologic review . 
genomic dna from all 21 sample tumors ( ls - utuc , n = 17 ; rcc , n = 4 ) and matched normal peripheral blood lymphocytes were analyzed for alterations in 341 cancer - associated genes . 
 thirteen ( 76% ) of 17 patients had loss of heterozygosity in the dna repair genes that corresponded to the germline alterations identified in their germline dna ( fig 1a ; appendix fig a1 )  . a total of 1 , 834 somatic coding alterations were identified across all patients with ls - utuc , involving 300 different genes ( data supplement )  . 
characteristic of mmr - deficient neoplasms , the mean msisensor score was high ( median , 25.1 ; range , 6 to 37.7 ) , with an excess of frameshift mutations ( 142 [ 8% ] in 1 , 834 ) , whereas copy - number alterations were uncommon.19 using mutational decomposition analysis in samples with 10 somatic mutations , we identified evidence of msi / mmr signatures in seven tumors , whereas the mitotic clock / aging signature was predominant in nine ( fig 1b )  . 
notably , the four rccs found to arise in the patients with ls had low mutation rates ( median , two ; range , one to nine ) , low msisensor scores ( median , 4.7 ; range , 3 to 11.6 ) , and no evidence of loss of heterozygosity of their ls associated germline mutation , suggesting that the pathogenesis of these tumors was biologically independent of their ls diagnosis . the most frequently mutated genes in the 17 ls - utuc tumors ( present in > 10 patients ) in decreasing frequency were kmt2d , crebbp , arid1a , smarca4 , cic , fat1 , fgfr3 , foxp1 , kmt2c , notch1 , and notch3 ( appendix fig a2 )  . 
with the exception of cic , foxp1 , and kmt2c , these genes were also those with the highest mutation rate ( > 0.002 mutations per nucleotide ; data supplement )  . 
 tp53 was mutated in a smaller subset of carcinomas ( five [ 29% ] of 17 ) , and in four of these , the tp53 mutation co - occurred with fgfr3 mutations . 
moreover , cdkn1b amplification showed a tendency toward mutual exclusivity with both fgfr3 and tp53 mutations . comparison of genomic profiles of ls - utuc and sporadic utuc to identify potential differences in the mutational landscape between ls - utuc and sporadic utuc , we compared the results of the ls - utuc cohort with those from a previously reported analysis by our group of 82 patients with sporadic utuc . 
one patient in this prior cohort had an ultramutated phenotype ( 422 mutations and no focal copy - number alterations ) attributable to a hotspot mutation in pole.11 patient demographic and clinicopathologic characteristics of the two groups are listed in table 1 . 
 this revealed that , although the mutational landscapes overlapped , some genes were targets of somatic alteration in both cohorts ; however , the frequency of alteration was significantly higher in ls - utuc ( ie , kmt2d , crebbp , arid1a , and smarca4 )  . 
when adjusting for grade , most of the differences between the two cohorts remained significant , although the frequency of gene alterations was different between lowand high - grade tumors ( table 2 )  . finally , we noted that both cohorts had similar frequencies of fgfr3 mutations ( ls - utuc , 11 [ 65% ] of 17 v sporadic utuc , 41 [ 50% ] of 82 ; p = .269 ; appendix fig a3 )  . 
 however , whereas the most prevalent fgfr3 hotspot mutation in sporadic utuc was s249c ( 26 [ 63% ] of 41 mutations ; 13 of 22 and 13 of 19 for lowand high - grade tumors , respectively ) , in ls - utuc , the fgfr3 mutations noted were predominantly r248c ( nine [ 82% ] of 11 mutations ; four of four and five of seven for lowand high - grade tumors , respectively ) and to a lesser extent g380r ( four [ 36% ] of 11 mutations ; two of four and two of seven for lowand high - grade tumors , respectively ; fig 2a )  . given this unexpected finding , we rereviewed all 41 fgfr3 mutations in our sporadic cohort of 82 utucs and identified two carcinomas with an fgfr3 r248c mutation . 
however , their msisensor scores were low ( 0 and 0.11 ) , and the mutational decomposition analysis revealed an aid / apobec signature . validation of fgfr3 r248c as marker of ls - utuc to determine the extent to which the presence of an fgfr3 r248c mutation may be associated with ls or an ls - like hypermutator phenotype , we queried 14 , 800 tumors prospectively sequenced as part of clinical care at memorial sloan kettering cancer center using the msk - impact assay . 
twenty - three patients had an fgfr3 r248c mutation , corresponding to 11 utucs , nine ucbs , and three tumors with other primary sites ( one squamous cell carcinoma of the lung , one lung metastasis from breast carcinoma , and one squamous cell carcinoma of the tongue ; fig 3 )  . 
 of the nine evaluable patients with presumed sporadic utuc and an fgfr3 r248c hotspot mutation , seven displayed germline evidence of ls ( six germline mutations in msh2 and one in msh6 )  . 
upwards of 80% of patients with ls will develop a malignancy , with colorectal cancer being the most common.20 uc is the third most common site of extracolonic malignancy in the ls spectrum and occurs in approximately 5% of patients . 
few studies to date have sought to define the somatic mutational profile of mmr - deficient urothelial tumors , in part because of the perception that the high mutational load would limit the ability to identify true driver events.19 in this study , we performed targeted sequencing of utuc from 17 patients with known germline mutations in an ls - associated gene to characterize the genomic landscape of these tumors and compared the results with those from a cohort of 82 patients with clinically presumed sporadic utuc . next - generation sequencing ( ngs ) can be used to discover novel , targetable , or pathogenic somatic alterations and identify patients with mutations for which therapies already exist . 
 a fgfr3 ls - utuc ( n = 17 ) presumed sporadic utuc ( n = 81 ) sporadic utuc with pole mutation ( n = 1 ) fgfr3 r248c fgfr3 s249c fgfr3 other mutation fgfr3 wild type p < .001 patients r248c s249c mutation fig 2 . 
 ( a ) number of somatic alterations in lynch syndromeassociated upper - tract urothelial carcinoma ( ls - utuc ) and sporadic utuc tumors and their association with fgfr3 mutation status . 
 ( b ) total mutation count in patients with somatic fgfr3 r248c and fgfr3 s249c mutations . the ls and sporadic utuc cohorts tended to be similar ( fgfr3 , kdm6a , pic3ca , and tp53 ) , differences in the genomic profiles were observed . 
of note , however , hypermutation or loss of heterozygosity of the ls germline mutation was not noted in the four rcc samples collected from patients with ls , suggesting that the pathogenesis of these tumors was unrelated to the ls diagnosis . although we were able to identify somatic alterations in most patients driving loss of heterozygosity in the germline ls genes relevant to each corresponding patient , four patients with ls had germline mutations without evidence of loss of heterozygosity as detectable by tumor dna sequencing . 
flow chart of identification of the patients with fgfr3 r248c mutation in the clinical memorial sloan kettering integrated molecular profiling of actionable cancer targets ( msk - impact ) cohort . 
 signatures consistent with msi , suggesting that these patients may have had transcriptional silencing by promoter hypermethylation , as previously reported.21 regarding the mutational decomposition analysis , only seven ls - utuc tumors had an mmr / msi signature . 
this mutational decomposition analysis only uses single - nucleotide polymorphisms , and these are not the most prevalent type of mutation present in msi / mmr cases.19 this may partially explain why the decomposition analysis did not identify a strong msi / mmr signature in some patient cases , including many with high msisensor scores . among the most striking findings in our study was the identification of an r248c hotspot mutation in fgfr3 that may serve as a potential biomarker for ls in patients with utuc . 
activating mutations of fgfr3 are particularly common in low - grade ucs.22 , 23 fgfr3 r248c leads to increased fgfr3 dimer stability and constitutive receptor activation in the absence of ligand , resulting in activation of the phosphatidylinositol 3 - kinaseakt and mitogen - activated protein kinase signaling pathways.24 , 25 this mutation has already been described in ucb , 26 but its presence in utuc was highly associated with a significantly increased median number of somatic mutations . some hereditary cancers are misclassified as sporadic , although their identification might have consequences for both patients and their family members , because this information would prompt germline testing and , if positive , screening for ls - related malignancies.27 our data suggest that the finding of an fgfr3 r248c somatic mutation is a potential biomarker for ls and its identification in a patient should prompt germline testing for ls . 
lindor tumors with mmr deficiency are more responsive to immune checkpoint blockade than mmr proficient tumors.28 it is possible that patients with ls - utuc may derive greater benefit from anti pd - 1 therapy , suggesting an immediate clinical implication for screening and potential personalization of therapy in these patients . one potential limitation of our study was the use of a targeted sequencing approach focusing on a panel of 341 cancer - related genes . 
recently , the analysis of 28 samples of sporadic utuc identified four rna expression profiles with different clinical characteristics , and it would be biologically important to study how ls - utucs cluster within this classification.29 additionally , although ours is the largest series to date to our knowledge profiling ls - utuc using ngs , the sample size remains small , and a larger study may have revealed other significant patterns of comutated genes . 
consequently , there is a need for a larger cohort with external validation . in conclusion , we performed targeted ngs of 17 utucs that arose in patients with ls to compare the genetic characteristics of such tumors with those of sporadic utuc tumors . 
although the spectrums of mutated genes showed some similarities , ls - utucs were characterized by a unique genetic signature , consisting of hypermutation and frequent hotspot mutations at fgfr3 r248c . 
 for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . christophe rosty no relationship to disclose daniel d . 
sfakianos consulting or advisory role : emd serono speakers bureau : astellas medivation dahlia sperling employment : next generation stock and other ownership interests : pharma ( i ) consulting or advisory role : next generation travel , accommodations , expenses : next generation hikmat al - ahmadie consulting or advisory role : bristol - myers squibb , emd serono mark clendenning no relationship to disclose zsofia k . 
stadler consulting or advisory role : allergan ( i ) , genentech / roche ( i ) , regeneron ( i ) , optos , ( i ) , adverum ( i ) gopa iyer no relationship to disclose barry taylor no relationship to disclose jonathan coleman no relationship to disclose noralane m . 
lindor consulting or advisory role : uptodate patents , royalties , other intellectual property : royalties as editor for section in uptodate ; royalties as editor for section in uptodate ( i ) travel , accommodations , expenses : intercept pharmaceuticals ( i ) david b . 
lynch ht , smyrk tc , watson p , et al : genetics , natural history , tumor spectrum , and pathology of hereditary nonpolyposis colorectal cancer : an updated review . 
rink m , ehdaie b , cha ek , et al : stage - specific impact of tumor location on oncologic outcomes in patients with upper and lower tract urothelial carcinoma following radical surgery . 
wagle n , berger mf , davis mj , et al : high - throughput detection of actionable genomic alterations in clinical tumor samples by targeted , massively parallel sequencing . 
duperret ek , oh sj , mcneal a , et al : activating fgfr3 mutations cause mild hyperplasia in human skin , but are insufficient to drive benign or malignant skin tumors . 
juanpere n , agell l , lorenzo m , et al : mutations in fgfr3 and pik3ca , singly or combined with ras and akt1 , are associated with akt but not with mapk pathway activation in urothelial bladder cancer . 
al - ahmadie ha , iyer g , janakiraman m , et al : somatic mutation of fibroblast growth factor receptor - 3 ( fgfr3 ) defines a distinct morphological subtype of high - grade urothelial carcinoma . 
audenet f , colin p , yates dr , et al : a proportion of hereditary upper urinary tract urothelial carcinomas are misclassified as sporadic according to a multi - institutional database analysis : proposal of patient - specific risk identification tool . 
moss tj , qi y , xi l , et al : comprehensive genomic characterization of upper tract urothelial engl j med 372 : 2509 - 2520 , 2015 carcinoma . 
oncoprint of the most frequent genes altered in the lynch cohort . kmt2d crebbp arid1a smarca4 fat1 fgfr3 foxp1 kmt2c notch1 notch3 kdm6a pik3ca cdkn1b tp53 tsc1 genetic alterations truncating mutation inframe mutation missense mutation ( putative driver ) missense mutation ( putative passenger ) amplification i - set pkinase_tyr lynch 806 aa fgfr3 fgfr3 r248c g380r s249c i - set i - set fig a3 . 
 frequent molecular subtype switching and gene expression alterations in lung and pleural metastasis from luminal atype breast cancer max klebe , ms1 ; carlo fremd , md2 ; mark kriegsmann , md1 ; katharina kriegsmann , md3 ; thomas albrecht , md1 ; verena thewes , phd2 , 6 ; martina kirchner , phd1 ; pornpimol charoentong , phd2 , 6 ; nadine volk , phd1 , 2 ; johannes haag , md4 ; ralph wirtz , phd5 ; thordur oskarsson , phd6 ; alexandra schulz , ms1 ; j org heil , md7 ; andreas schneeweiss , md8 ; hauke winter , md4 ; and peter sinn , md1 purpose conversion of tumor subtype frequently occurs in the course of metastatic breast cancer but is a poorly understood phenomenon . 
in luma cancers , 62 genes were identied with differential expression in metastatic versus primary disease , compared with only 10 differentially expressed genes in lumb , human epidermal growth factor receptor 2 ( her2 ) enriched , and basal subtypes combined . gene expression changes in luma cancers affected not only the repression of the estrogen receptor pathway and cell cyclerelated genes but also the wnt pathway , proteinases ( mme , mmp11 ) , and motility - associated cytoskeletal proteins ( ck5 , ck14 , ck17 )  . 
this involved 83 notable gene expression changes . conclusion our results indicate that gene expression changes and subsequent subtype conversion occur on a large scale in metastatic luminal atype breast cancer compared with other molecular subtypes . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction visceral metastases often occur as late events in the course of metastatic breast cancer and are generally followed by a rapidly fatal outcome . 
we examined changes in pam50 gene signatures in a matched - pair series of 57 breast cancer primaries and corresponding lung or pleural metastases to determine the nature and extent of tumor subtype conversion . knowledge generated subtype conversion to pam50 luminal b subtype was observed in the majority of luminal atype breast cancers . 
only few cases of primary luminal b , human epidermal growth factor receptor 2enriched , and basal - like subtypes converted to another pam50 category in metastasis . relevance pam50 - based subtype classication of breast cancer lung and pleural metastases may be different than that seen in the primary tumor , especially in primary luminal a cancers . 
this change in pam50 classication between primary and metastatic disease may affect response to systemic therapy and must be investigated . other three subtypes by tissue microarray analysis , 7 and basal subtypes in particular were more frequent than expected.9 in this study , we included patients with invasive breast cancer of all molecular subtypes and metachronous breast cancer with lung or pleural metastasis ( bclpm ) to provide insights into the upand downregulation of genes during the course of the disease . 
therefore , we retrospectively examined gene expression proles in a wellcharacterized , prospectively assembled group of patients with breast cancer and metachronous lung or pleural metastasis ( data supplement 2 , fig s1 )  . 
exclusion criteria included no availability or insufciency of tumor tissue from pbc or bclpm tumor tissue ( n = 11 ) , primary lung cancer after review of patient records ( n = 2 ) , and low rna content or not meeting quality control criteria of rna data ( n = 11 )  . gene expression analysis for the selection of tumor tissue for rna extraction , ffpe tissue blocks from the pbc and metastatic lesions were selected after reviewing all original tissue slides and were recut for hematoxylin & eosin sections , to be used for reference and to determine tumor cell content ( tumor surface area )  . 
microdissection was performed in most cases to avoid normal breast tissue contamination . a minimum of approximately 50 ng of total rna was used . hybridization time per cartridge was 16 hours before measurement . rna expression analysis was performed by measuring a custom panel of 269 breast cancerrelated genes and 11 housekeeping genes ( data supplement 2 , table s2 ) , using the ncounter platform ( nanostring technologies , seattle ca ) according to the manufacturers instructions . 
the gene panel cludes 25 published gene signatures with prognostic or predictive properties in luminal - type breast cancer with the aim to determine their role in metastatic disease ( data supplement 2 , table s3 )  . 
the selection of gene signatures covered by this list of genes includes nine proliferationrelated signatures , four estrogen receptorrelated signatures , one immune - related signature , and 11 signatures related to cancer pathways . 
for gene function , david bioinformatics resources were used ( version 6.8 ) , 17 , 18 and functional annotation analysis in the biological process category and kegg pathway enrichment were computed . 
all statistical calculations , except gene function analysis , were done using r , version 3.6.1.20 additional information is available in data supplement 1 . results patient characteristics a total of 57 patients with bclpm were included in this study . 
pam50 molecular subtype conversion occurred in the majority of luminal atype pbc ( n = 16 ; 57.1% ) , evolving mostly into luminal btype or her2 - type metastasis ( table 1 ; fig 1b )  . 
gene expression clustering of bclpm was clearly different from pbc in the low - risk category but not with cancers of high - risk subtypes ( figs 2a - 2b )  . this indicates a similar tumor biology of bclpm and pbc for tumors of high - risk subtypes but a different biology in the low - risk ( luminal a ) category . 
by tnm classication luma lumb her2 basal ( range ) initial metastatic site before the treatment of metastatic breast cancer lung or pleural metastasis endocrine therapy at time of metastatic other unknown biopsy yes , tamoxifen yes , aromatase inhibitor yes , gnrha no . 
similarly , heatmap clustering conrmed separate luminal a clusters for primary tumors and metastases ( fig 3 )  . pgr was signicantly downregulated ( p = .0015 , wilcoxon rank - sum test ) , and mki67 was not signicantly increased ( data supplement 2 , fig s5 )  . differential gene expression analysis to characterize which genes are involved in the process of bclpm , differential gene expression analysis was performed . 
these included 3 cytoskeletal proteins ( krt14 , krt17 , krt5 ) , 2 matrix metalloproteinases ( mmp11 , mme ) , and ankrd30a . the latter is a breast differentiation gene that is frequently expressed in the breast and in receptor - positive breast cancer.22 other molecular changes in metastases were linked to proliferation ( cdc6 , ccnb1 , mki67 , top2a , aurkb , pttg1 ) , cell cycle checkpoints ( brca2 , bub1 , bub1b , chek1 ) , and epithelial - mesenchymal transition ( emt ) genes . 
among the genes most relevant for therapy in breast cancer ( esr1 , pgr , her2 , mki67 ) , the expressions of esr1 and her2 were unaffected in bclpm , but subtype - specic changes the pam50 subtypes of pbc showed marked variation with regard to the extent of differential gene expression of this gene panel in bclpm . 
the greatest number of differentially expressed genes was seen in luminal atype breast cancer , with 47 and 11 downand upregulated genes , respectively , compared with fewer expression changes in metastatic high - risk tumors ( luminal b , her2 - enriched , basal - like ) , with six and four downand upregulated genes , respectively ( figs 4a - 4b )  . 
only 1 gene was downregulated in bclpm that was her2 enriched , and no genes reached signicance after adjustment for multiple testing in the basal - like subtype , which in part may be attributed to the comparably small sample sizes of 6 and 7 , respectively ( data supplement 2 , table s6 )  . 
of the genes repressed in luminal a metastases , several are associated with emt . four of these ( twist2 , twist1 , zeb1 , tgfb3 ) are key regulators of emt . 
multidimensional scaling ( umap ) of gene expression , showing ( a ) gene expression in primary versus metastatic cancers , and ( b ) pam50 subtypes of the primary and metastatic tumors . 
for luminal a ( luma ) subtype , two subtype clusters can be distinguished , ( bottom ) one for primary breast cancers , and ( top ) the smaller one representing lung metastases . 
lumb , luminal b ; her2 , human epidermal growth factor rector 2enriched ; basal , basal - like ; normal , normal - like subtype . with bclpm ( figs 2a - 2b ) , and the magnitude and type of gene expression changes in lung metastasis ( table 1 )  . 
thirty - four and 49 genes were signicantly upand downregulated , respectively , in bclpm from luminal a cancers with subtype switch ( adjusted p , .05 ) compared with only 7 genes downregulated and none upregulated in the nonsubtype switch group ( figs 4c - 4d )  . 
in luminal a cancers , subtype switch affected cell cycle and cell proliferation genes ( mitotic cell cycle checkpoint , sister chromatid cohesion , mitotic nuclear division , cell division ) and the p53 - signaling as well as progesterone - signaling pathways ( data supplement 2 , figs 4a and 4b )  . clustering of gene expression in luminal atype cancers to better characterize the phenomenon of subtype conversion in luminal a cancers , we set up a logistic model for the assessment of differential gene expression with and without subtype conversion . 
in the group of 28 luminal asubtype tumors , a subtype conversion was more likely to occur when genes involved in certain growth factors , nuclear proteins , and signaling molecules were upregulated ( gnaz , hoxb13 , vegfa ) and some genes involved in immune response and inammation ( foxp3 , cd8a , cd68 , csf1r ) were downregulated ( fig 5a )  . 
this included 10 genes of various functions with downregulation in metastases and 52 genes , also of diverse functions , that were upregulated after subtype switch ( fig 5b )  . 
this upregulation of a substantial number of genes suggests a common mechanism of gene regulation that is involved in subtype switching . comparison of gene signatures in luminal a and btype cancers for additional insight into the classes of genes involved in subtype switching , a couple of well - characterized gene signatures for estrogen receptor signaling , tumor proliferation , and hallmarks of cancer were analyzed in bclpm ( data supplement 2 , figs s6a and s6b )  . 
interestingly , and despite the different genes involved in these signatures , all 4 tumor proliferation signatures tested showed similar patterns of gene expression in metastases derived from luminal atype tumors with and without subtype switch . 
 klebe et al subtype luminal a luminal b basal - like her2 - enriched normal - like site breast primary lung metastasis expression subtype site brca2 diaph3 chek2 ccne2 aurka bub1 mki67 rrm2 cenpa exo1 mybl2 cep55 plk1 pttg1 cdc6 top2a tyms hif1a flvcr2 cd44 rragd uchl1 scrg1 qsox2 oxct1 krt7 cd24 fgfr4 phgdh cdca7 adgrg6 prkcb pim2 ptgds zeb2 tp53 il17rb rbbp8 krt5 krt14 krt17 tspyl5 elf5 vgll1 prom1 sfrp1 mmp12 mmp9 igfbp5 cxcl14 abl1 zeb1 twist2 twist1 snai2 aldh1a1 slc2a3 csnk1d fam213b fzr1 bbc3 rassf7 plau mmp11 tgfb3 ankrd30a tmem45b pik3ca col4a2 cdc42bpa gstm1 esm1 csnk1e znf703 ccnd1 ebf4 esr1 thsd4 tbc1d9 gata3 cxxc5 ca12 tff1 tff3 foxa1 spdef krt18 pak1 blvra cdk7 stk32b bcl2 stc2 greb1 mapt scube2 igf1r slc39a6 siah2 krt19 cldn4 ddr1 azgp1 fig 3 . 
tumors are discriminated according to their molecular subtype , with separation of metastatic luminal a tumors from primary luminal a cancers ( shown as blue bars across top )  . 
different patterns of gene expression changes are observed , with ( a ) signicantly more changes in the luminal a subtype compared with ( b ) high - risk tumors ( lumb , human epidermal growth factor receptor 2 ( her2 ) enriched , basal - like )  . 
within the luminal a subtype , gene expression changes were mostly conned to ( c ) tumors with subtype switch in lung metastasis compared with ( d ) nonswitched metastases . intrinsic tumor subtype as subtype conversion or subtype switch.26 our results indicate that evolution within cancer cell populations during metastasis leads to more transcriptomic and phenotypic changes than might be expected from the acquisition of genetic events . 
 molecular subtype switching in luminal atype breast cancer the pam50 subtype , subtype conversion only partly reects the changes occurring in tumor evolution , and our data indicate that , even the molecular without change of phenotype may still be different in the metastasis , especially in low - grade tumors . 
in multidimensional scaling , tumors of luminal a subtype in bclpm form a different cluster than luminal a subtype in the primary ( fig 2 ) , and , in the differential expression heatmap , they cluster with more aggressive subtypes ( fig 3 )  . 
along that line , relevant gene expression changes in brain metastases were found without change of pam50 subtype.28 when pam50 subtype conversion occurs , it can be regarded as an indicator of genetic remodeling in metastasis and as a risk factor of additional disease progression . 
of note , although estrogen receptor and her2 statuses as predictive clinical markers remained unchanged in this group , the proliferation rate greatly increased , and breast hormone receptor signaling declined . 
as such , although therapeutically relevant markers were unaltered upon subtype switch , remarkable changes occurred that are generally associated with a worsened malignant behavior and prognostic impact . the metastatic tumor cell the gene expression changes that were evident across all subtypes included evidence for increased mobility and invasive behavior of through downregulation of cytokeratins ( krt5 / 14 ) 29 ; tumor activation through downregulation of mmp1130 , 31 ; and deactivation of estrogen receptordependent pathways , as indicated by the downregulation of the progesterone receptor and the ankyrin repeat - domain gene ( ankrd30a )  . conversely , genes involved in emt and growth signaling were upregulated in all molecular subtypes ( data supplement 2 , fig s3 )  . 
as far as datasets are comparable , most changes found in bclpm have been reported to occur also in other metastatic sites , 27 , 32 with the exception of her2 , which was demonstrated to be upregulated in the brain28 ; however , it was not in our dataset . luminal a cancers undergoing a subtype switch were characterized by a much higher variability in gene expression in bclpm compared with high - risk carcinomas . this variability affected various molecular pathways . 
from gene expression data alone , it appears not possible to name a common denominator for the changes in metastasis of luminal a cancers that affected several dozens of genes . 
when trying to dissect the alterations that occur in subtype conversion , we found that primary tumors with low expression of inammation - related genes but increased expression of growth signalingassociated genes were more likely to undergo subtype conversion . 
in the metastatic tumor cell , the subtype switch was characterized by quite extensive gene expression changes of various molecular pathways , similar to the nding of important gene expression changes in  . 
100 genes in brain metastasis.29 no hypothesis about the root cause of changes for subtype conversion can be put forward , but the manifold changes of expression status in bclpm from luminal a cancers do indicate a major reprogramming of the tumor cell . limitations of this study include the use of a curated gene list . 
last but not least , although the discrimination of patients with breast cancer into specic cancer subtypes is a widely applied clinical concept with profound prognostic implications , luminal a and b cancers may much more represent a continuum rather than true distinct subtypes from a biologic point of view . in conclusion , we have shown that luminal atype breast cancer is most affected by subtype conversion and differential gene expression in matched metastases to lung or pleura involving but not limited to estrogen receptor signaling ( downregulation ) and tumor proliferation ( upregulation )  . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . carlo fremd honoraria : roche , pzer , celgene , astrazeneca , amgen consulting or advisory role : roche , pzer travel , accommodations , expenses : celgene , roche ralph wirtz employment : stratifyer molecular pathology gmbh stock and other ownership interests : stratifyer molecular pathology gmbh consulting or advisory role : janssen oncology ( inst ) , biontech ag ( inst ) research funding : janssen research & development ( inst ) patents , royalties , other intellectual property : royalties from biontech ( inst ) ; royalties from qiagen ( inst ) thordur oskarsson stock and other ownership interests : neovasc , cyclacel pharmaceuticals , windtree therapeutics , enzon pharmaceuticals patents , royalties , other intellectual property : migrastatins and uses thereof . 
description : the present invention provides compounds , pharmaceutically acceptable compositions thereof , and methods of using the same . other relationship : genentech j org heil honoraria : roche , siemens healthcare diagnostics , bard consulting or advisory role : roche , siemens healthcare diagnostics research funding : bard travel , accommodations , expenses : celgene andreas schneeweiss honoraria : roche pharma ag , celgene , astrazeneca , pzer , novartis , msd oncology , lilly , tesaro research funding : roche pharma ag ( inst ) , celgene ( inst ) , abbvie , molecular partners expert testimony : roche , astrazeneca travel , accommodations , expenses : roche , celgene hauke winter expert testimony : astrazeneca travel , accommodations , expenses : astrazeneca peter sinn honoraria : nanostring technologies , roche pharma ag research funding : roche pharma ag travel , accommodations , expenses : nanostring technologies no other potential conicts of interest were reported . references vanharanta s , massagu e j : origins of metastatic traits . 
j surg oncol 23 : 175 - 180 , 1983 van den hurk cj , eckel r , van de poll - franse lv , et al : unfavourable pattern of metastases in m0 breast cancer patients during 1978 - 2008 : a population - based analysis of the munich cancer registry . 
smyth gk : limma : linear models for microarray data , in gentleman r , carey v , dudoit s , et al ( eds ) : bioinformatics and computational biology solutions using r and bioconductor . 
aomatsu e , takahashi n , sawada s , et al : novel scrg1 / bst1 axis regulates self - renewal , migration , and osteogenic differentiation potential in mesenchymal stem cells . 
thompson am , jordan lb , quinlan p , et al : prospective comparison of switches in biomarker status between primary and recurrent breast cancer : the breast recurrence in tissues study ( brits )  . 
this , in turn , leads to a profound defect in homology - mediated dna repair and inappropriate use of error - prone repair pathways , which result in gross genomic instability that contributes to tumorigenesis.1 , 2 this dna - repair defect in brca1 / 2 - mutant cancers renders them exquisitely vulnerable to certain kinds of dna damage , including those caused by poly ( adp - ribose ) polymerase ( parp ) inhibitors and certain classic chemotherapy agents , including platinum.3 the vulnerabilities of brca1 / 2 - mutant cancers to these agents have been translated successfully into treatment approaches . 
parp inhibitors are now approved by the us food and drug administration for treatment of brca1 / 2 mutant ovarian cancers , 4 and data are accumulating that suggest that parp inhibitors are likely active in brca1 / 2 - mutant cancer regardless of the tissue of origparp inhibitors are thought to be toxic to brca1 / 2 - mutant cancers not only because of their catalytic inhibition of parp but by their ability to trap parp - 1 enzyme on dna.5 , 6 the most potent parp inhibitors that induce cell death in brca1 / 2 - mutant cells are those that most efficiently trap parp protein on dna , creating a bulky protein dna adduct.7 in this sense , parp inhibitors work similarly to topoisomerase inhibitors , which trap topoisomerases to create a bulky protein dna adduct . 
other dna - damaging agents including platinum , mitomycin c , and topoisomerase inhibitors , that also induce dna adducts , are also effective in the treatment of brca1 / 2 - mutant cancers in animal models and clinically . given the widespread use of germline and tumor sequencing , and recent us food and drug administration approval of parp inhibitors , more patients who have tumors with pathogenic brca1 / 2 mutations are being treated with parp inhibitors and / or platinum agents . 
one important mechanism of acquired resistance is reversion mutations in brca1 or brca2 that partly restore wild - type gene function.8 , 9 the three reports10 - 12 of reversion mutations in brca2 in breast and prostate cancers that accompany this editorial highlight the importance and increasing awareness of this mechanism of resistance . 
the presence of reversion mutations in brca1 / 2 also reveals some insights about the role of brca1 / 2 function in tumorigenesis and chemosensitivity . most pathogenic mutations in brca1 and brca2 are small insertion / deletions that result in a frameshia frameshift will introduce a premature stop codon , which leads to a truncated , nonfunctional protein product . 
often , frameshift mutations lead to effective null mutations , because rna transcripts harboring premature stop codons can be recognized and degraded by the nonsense - mediated decay pathway.13 reversion mutations are secondary mutations , often small deletions , in a mutant brca1 / 2 allele that convert the initial frameshift mutation into an in - frame internal deletion that still produces a partly functional protein product . 
 complex rearrangements or abnormal use of alternative start sites that bypass the frameshift mutation may also occur.14 rarely , there is full reversion of the pathogenic mutation with restoration of the full wild - type sequence , as seen in the article by banda et al.10 reversion mutations can occur in the setting of either germline or somatic brca1 / 2 mutations , as demonstrated by carneiro et al , 12 and can lead to acquired resistance not only to parp inhibitors but to other classes of dna - damaging agents , such as platinum11 . intriguingly , the mechanism underlying many reversion mutations is inappropriate use of the nonhomologous end - joining pathway , resulting in small deletions , as seen by presence of microhomology at junction sequences.15 longer deletions associated with single - strand annealing may also be present but more difficult to detect . 
it is possible that reversion mutations may already be present in a small population of cells , especially if there is high tumor burden as seen , for example , in ovarian cancer , and are simply selected with ongoing treatment . reversion mutations can be difficult to detect by standard sequencing methods . 
large deletions may be completely missed by short - read sequencing , and even small deletions have to be carefully curated to determine in which allele they originate , and the effect on the final reading frame . 
some full reversions to wild - type sequence may only be detected by careful analysis of tumor purity and mutant allele frequencies in serial samples over time , as demonstrated by banda et al.10 heterogeneity of reversion mutations may also hinder detection . 
analysis of circulating - cell free dna , such as reported by cheng et al11 and carneiro et al , 12 can detect multiple reversion mutations simultaneously at the time of clinical resistance to parp inhibitors or platinum , each restoring the reading frame and arising from a different small tumor - cell population.16 it is possible that only a fraction of reversion mutations in brca1 / 2 are being identified by current sequencing methods . 
new technologies , such as long - read sequencing , and higher depth sequencing may allow more robust detection of reversion mutations and better define their frequency . the selection for reversion mutations in brca1 / 2 under certain treatments does give us some insights into the biology of brca1 . 
 the induction of reversion mutations by platinum is clear genetic evidence that this agent acts on the dna - repair defect associated with brca1 / 2 loss and exerts direct selection pressure to restore brca1 / 2 function . 
this finding also suggests that perhaps , in general , dna - damaging chemotherapies function not as gross metabolic poisons but as targeted therapies for cancers with underlying defects in dna repair and / or checkpoint control . 
if this is true , we may need to reconsider how to optimally dose and schedule platinum and other chemotherapy agents , especially in the setting of cancers with underlying dna - repair defects . the presence of reversion mutations demonstrates that loss of brca1 or brca2 function and the associated dna - repair defect is only required for initiation of tumorigenesis and is not required for maintenance of the cancer phenotype . 
 this feature can be labeled tumor - suppressor tolerance to place it in contrast to oncogene addiction . tumor - suppressor tolerance may operate in cancers that have underlying mutations in genes critical for genomic stability . 
loss of tumor - suppressor function of these genes may only be required for initial tumorigenesis ; once the tumor is established , there may be selection pressure to restore the tumor - suppressor function and reestablish dna - repair function . 
in brca1 - mutant cancers , resistance to parp inhibitors can occur not only by reversion mutations that directly restore brca1 function but also by compensating mutations in other genes such as 53bp1 and its downstream factors such as rif1 , ptip and rev7 , which also can restore homology mediated repair pathways independent of functional brca1.21 - 25 similarly , loss of ptip and chd4 may allow brca2 - mutant cells to reestablish replication fork stability and become resistant to cisplatin and parp inhibitors.26 these findings suggest that to better predict sensitivity to parp inhibitors and platinum , we will need to develop assays capable of distinguishing a cancer with ongoing genomic instability from a cancer with just a history of genomic instability followed by functional reversion of a dna - repair defect . with increasing use of parp inhibitors and platinum for targeted therapy of brca1 / 2 - mutant cancers , we will likely see increased incidence of acquired resistance that exploits tumor - suppressor tolerance and restores brca1 / 2 function . 
it is possible that some hypomorphic alleles of brca1 and brca2 that arise by reversion mutation may still have some targetable vulnerability.27 alternatively , parp inhibitors , or other dna - damaging agents such as platinum , will need to be combined with other drugs that target a different vulnerability in these cancers . 
carneiro b , et al : acquired resistance to the parp inhibitor olaparib in brca2 - associated prostate cancer due to biallelic brca2 reversion mutations restoring both germline and somatic loss of function mutations . 
perrin - vidoz l , sinilnikova om , stoppa - lyonnet d , et al : the nonsense - mediated mrna decay pathway triggers degradation of most brca1 mrnas bearing premature termination codons . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
escribano - daz c , orthwein a , fradet - turcotte a , et al : a cell cycle - dependent regulatory circuit composed of 53bp1 - rif1 and brca1 - ctip controls dna repair pathway choice . 
bouwman p , aly a , escandell jm , et al : 53bp1 loss rescues brca1 deficiency and is associated with triple - negative and brca - mutated breast cancers . 
chapman jr , barral p , vannier jb , et al : rif1 is essential for 53bp1 - dependent nonhomologous end joining and suppression of dna double - strand break resection . 
 o genomic characterization of erbb2 - driven biliary cancer and a case of response to ado - trastuzumab emtansine sebastian mondaca , md1 ; pedram razavi , md , phd1 , 2 ; chongrui xu , md , phd1 ; michael ofn , md1 ; mackenzie myers , ms1 ; maurizio scaltriti , phd1 ; jaclyn f . 
abou - alfa , md , mba1 , 2 purpose biliary tract cancers ( btcs ) , which include intrahepatic cholangiocarcinoma ( icc ) , extrahepatic cholangiocarcinoma ( ehc ) , and gallbladder cancer ( gbc ) , have limited treatment options . 
twenty - eight patients ( 5.4% ) had erbb2 alterations , including 2.7% with erbb2 gene amplication , 2.3% with erbb2 mutation , and 0.4% with concurrent amplication and mutation . 
frequent co - altered genes in this cohort were tp53 ( 54% ) , pik3ca ( 21% ) , and cdkn2a ( 18% ) ; kras amplication / mutation was found in 7% of patients . 
2019 by american society of clinical oncology introduction biliary tract cancer ( btc ) comprises three clinically and molecularly distinct entities , intrahepatic cholangiocarcinoma ( icc ) , extrahepatic cholangiocarcinoma ( ehc ) , and gallbladder cancer ( gbc )  . 
genomic proling of btcs with next - generation sequencing ( ngs ) platforms has shown that the three clinical subtypes have signicant molecular differences.5 whereas all three have a high prevalence of tp53 and cdkn2a mutations , genomic alterations in fgfr2 and idh1 are mostly limited to icc ( approximately 20% each )  . 
 mondaca et al context key objective to describe the landscape of erbb2 genomic alterations in biliary tract cancer and illustrate a case of a patient who responded to antihuman epidermal growth factor receptor 2 ( her2 ) targeted therapy . knowledge generated erbb2 amplication or mutations were identied in 28 ( 5.4% ) of 517 patients with biliary tract cancer . 
erbb2 - driven biliary tract tumors had higher concurrent alterations of tp53 and pik3ca , while kras alterations seemed to be less common . one patient with erbb2 - amplied extrahepatic cholangiocarcinoma had a partial response to the her2 - targeted antibodydrug conjugate ado - trastuzumab emtansine . relevance potentially targetable erbb2 amplication and mutation are present in a signicant group of biliary tract tumors , particularly in gallbladder cancer . 
this study supports prospective testing for erbb2 alterations to develop novel anti - her2 strategies in this population . rst - line chemotherapy compared with patients with erbb2 wild type . on the basis of demonstrated improved os in pivotal phase iii trials , drugs that target her2 are standard treatment in her2 - overexpressed breast and gastric cancers.9 , 10 given the low incidence of btcs , the clinical characterization of relevant molecular subgroups , such as erbb2 - amplied or erbb2 - mutant btcs , has been limited , and the clinical experience with anti - her2 agents in this group has been largely anecdotal . 
a recent basket trial showed objective response in four ( 36% ) of 11 patients with erbb2amplied or erbb2 - mutant btc treated with the combination of the anti - her2 antibodies trastuzumab and pertuzumab.11 the aim of the current study was to comprehensively describe the clinical and molecular characteristics of erbb2 - amplied or erbb2 - mutant btcs identied within the context of a prospective tumor proling initiative at memorial sloan kettering ( msk ) cancer center . we also report a durable response to the her2 - targeted antibody - drug conjugate ado - trastuzumab emtansine ( t - dm1 ) in a patient with erbb2 - amplied btc enrolled in a basket trial ( clinicaltrials.gov identier : nct02675829 )  . methods patients demographic data and treatment histories were collected for all patients with erbb2 - altered btc who consented for prospective tumor genomic proling using the us food and drug administrationauthorized msk - impact assay between february 2014 and june 2018 . 
informed consent for tumor proling and clinical data collection was obtained under the genomic proling in cancer patients protocol ( clinicaltrials.gov identier : nct01775072 ) , which was approved by the msk institutional review board . data collection clinical data were extracted from electronic medical records . variables collected were demographic characteristics ( age , sex , race ) , eastern cooperative oncology group performance status , tumor type ( icc , ehc , gbc ) , metastatic sites , systemic treatments received , and clinical outcomes . 
all tumors were prospectively reviewed to conrm histology and to estimate tumor purity . molecular proling and genomic analysis memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) was performed as previously described in a clinical laboratory improvement amendmentscertied laboratory.12 , 13 msk - impact sequences at high coverage all exons and selected intronic and noncoding regions of up to 468 cancer - associated genes . 
baseline characteristics characteristic illustrative case one patient with metastatic erbb2 - amplied ehc was treated with t - dm1 in a basket trial at msk for patients with her2 - amplied or her2 - mutant cancers in the cohort of other solid tumors . 
methods and partial results of this trial have been presented previously , 15 , 16 but to our knowledge , this would be the rst publication about the patient with btc from the basket trial . 
this study was approved by the msk institutional review board , and all patients signed informed consent in accordance with the precepts of the declaration of helsinki . results patients and molecular prole during the period considered in this study , 517 patients with btc underwent msk - impact testing . 
in the subset of patients with btc with erbb2 - amplied or erbb2 - mutant tumors , the median age at diagnosis was 64 years ( range , 27 - 82 years ) , and the most frequent stage of presentation was stage iv ( 50% )  . 
the most frequently mutated domain of her2 was the extracellular domain ( 32% ) , and all mutations in this region arose at the s310 codon ( fig 1 )  . missense mutations represented the most common alteration in the mutated group ( 94% )  . 
of patients age , years median ( range ) male female race white asian black unknown primary tumor stage at diagnosis genomic alteration erbb2 amplication erbb2 mutation erbb2 amplication / mutation first sites of metastasis liver lung bone peritoneum other btc , no . 
the patient then received adjuvant gemcitabine , but within 3 months of initiation of systemic chemotherapy , imaging showed progression of disease in the posterior mediastinum , liver , and peritoneua biopsy specimen of the table 3 . 
aa , amino acid ; furin - like , furin - like cysteine - rich region ; gf_recept - iv , growth factor receptor domain iv ; pkinase_tyr , protein tyrosine kinase domain ; recep_l , receptor l domain . mediastinal metastasis conrmed recurrence ; immunohistochemistry revealed 3 + her2 protein overexpression . the patient was then treated with t - dm1 3.6 mg / kg once every 21 days in a basket trial and achieved a conrmed partial response after 12 weeks of treatment ( fig 3 )  . 
despite ongoing treatment with t - dm1 , the patients disease progressed after 8.6 months with the development of a new 2.2 - cm ( short - axis ) retrocaval lymph node . 
cancer antigen 19 - 9 was 10 , 700 u / ml before starting t - dm1 and decreased to 73 u / ml after achieving a conrmed partial response , with cancer antigen 19 - 9 remaining stable at the time of disease progression ( 62 u / ml )  . 
however , with the development of a new site of disease , t - dm1 was discontinued . discussion this study reports that potentially targetable erbb2 amplication or mutation was present in 5.4% of a cohort of 517 patients with btc who underwent prospective tumor molecular characterization at our institution . 
a similar gradient was described in a previous study that reported 16% , 11% , and 3% of erbb2 amplication in gbc , ehc , and icc , respectively.5 we also found that msi - high tumors were more frequent in the erbb2 - altered cohort compared with tumors without these alterations . 
similar ndings have been described in erbb2 - mutant colon cancer17 ; however , it is not clear whether this represents a biologically meaningful association or passenger erbb2 mutations are more frequent in tumors with an increased tumor mutational burden . 
erbb2activating mutations have been previously described to be present in 1% to 8% of btcs ; the potential therapeutic signicance of these mutations is an active area of research.5 as an example , 20 patients with her2 - mutant btc were enrolled in a basket trial of the pan - her tyrosine kinase inhibitor neratinib ( clinicaltrials.gov identier : nct01953926 ) , with two ( 10% ) achieving a partial response.18 this trial the clinical activity of found that neratinib varied as a function of tumor site , with the most promising clinical activity observed in her2 - mutant breast cancer ( 32% ) but no recist responses in several other cancer types , including bladder and colon cancers.19 the likelihood of clinical response to neratinib also varied as a function of mutation type . 
in another basket study , the response rate of patients with her2 - mutant nonsmall - cell lung cancer to t - dm1 was 44%.15 it remains unknown whether her2targeted antibody drug conjugates would have similar activity in her2 - mutant btc . we report here a patient with erbb2 - amplied btc who achieved a partial response to the her2 - targeted antibodydrug conjugate t - dm1 . 
 mutation count mutation spectrum msi type cancer type sample type erbb2 egfr erbb3 erbb4 fgfr2 pik3ca akt1 tsc2 tp53 mdm2 smad4 arid1a arid1b arid2 kmt2c kras cdkn2a idh1 bap1 mondaca et al stable indeterminate instable primary metastatic female male 100% genomic alterations missense mutation ( putative driver ) missense mutation ( unknown significance ) truncating mutation in - frame mutation fusion amplification deletion no alterations fig 2 . 
ehc , extrahepatic cholangiocarcinoma ; gbc , gallbladder cancer ; icc , intrahepatic cholangiocarcinoma ; msi , microsatellite instability . basket trials , conduct of dedicated trials that include an erbb2 - altered btc cohort has been more challenging . currently , a phase ii trial in china is evaluating the combination of gemcitabine plus oxaliplatin and trastuzumab in erbb2 - amplied btc ( clinicaltrials.gov identier : nct02836847 )  . 
her2 overexpression by immunohistochemistry and uorescence in situ hybridization has been pivotal for the approval of her2 - targeted therapies in breast and gastric cancers.9 , 10 however , tissuebased ngs analyses can identify both mutation and amplication along with other potential actionable targets . given the good correlation for amplication among these methods14 and the increasing clinical use of ngs , we believe that this approach represents an appropriate inclusion criterion in clinical trials . 
first , the cohort represents a selected population treated at a single academic cancer center that favors clinical trial enrollment ; hence , the patients with btc studied may have had different characteristics compared with those being treated in a community setting . 
 erbb2 amplication and mutation in biliary tract cancer baseline 3 months 8.6 months 30% present 80% present new retrocaval ln target lesions ( liver ) nontarget lesions new lesions 10 , 000 8 , 000 6 , 000 4 , 000 2 , 000 months fig 3 . 
ca , cancer antigen ; ln , lymph node . reported treatment is greater than 1.3 times the pfs on the prior line of therapy , the reported treatment can be considered benecial.26 in the case presented here , the patient progressed within 3 months after starting adjuvant chemotherapy and had a pfs of 8.6 months on rst - line t - dm1 , which supports a clinically meaningful benet . 
abou - alfa , md , memorial sloan kettering cancer center , 300 e 66th st , new york , ny 10065 ; twitter : @gaboualfa , @sloan_ kettering ; e - mail : abou - alg@mskcc.org. support supported by national institutes of health memorial sloan kettering cancer center core grant no . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . sebastian mondaca consulting or advisory role : foundation medicine pedram razavi consulting or advisory role : novartis research funding : grail ( inst ) , illumina ( inst ) chongrui xu honoraria : astrazeneca , boehringer ingelheim , eli lilly , msd , novartis , pzer , roche consulting or advisory role : boehringer ingelheim , pzer travel , accommodations , expenses : astrazeneca , boehringer ingelheim , eli lilly , novartis , pzer , roche , bristol - myers squibb , msd michael ofn consulting or advisory role : pharmamar , novartis , targeted oncology travel , accommodations , expenses : bristol - myers squibb , merck sharp & dohme maurizio scaltriti stock and other ownership interests : loxo oncology honoraria : menarini , adc therapeutics consulting or advisory role : menarini research funding : menarini ( inst ) , immunomedics ( inst ) , targimmune therapeutics ( inst ) , puma biotechnology ( inst ) , daiichi sankyo ( inst ) patents , royalties , other intellectual property : pi3k inhibitors and uses thereof , us provisional application no . 
62 / 742 , 163 , inventors : maurizio scaltriti , dan heller , jos e baselga , yosef shamay , carles monterrubio , amaia arruabarrena ( inst ) ; methods for detecting her2 dimerization in patients with her2 mutant lung cancers and predicting responsiveness to ado - trastuzumab emtansine therapy , sk2018038 - 01 , inventors : maurizio scaltriti , bob t . 
solit stock and other ownership interests : loxo oncology consulting or advisory role : pzer , loxo oncology , illumina , intezyne technologies , vivideon therapeutics , eli lilly travel , accommodations , expenses : merck kgaa bob t . 
li consulting or advisory role : roche , biosceptre international , thermo fisher scientic , mersana , guardant health , hengrui therapeutics research funding : roche ( inst ) , genentech ( inst ) , illumina ( inst ) , biomed valley discoveries ( inst ) , astrazeneca ( inst ) , grail ( inst ) , daiichi sankyo ( inst ) , hengrui therapeutics ( inst ) , guardant health ( inst ) , amgen ( inst ) ghassan k . 
n engl j med 362 : 1273 - 1281 , 2010 okusaka t , nakachi k , fukutomi a , et al : gemcitabine alone or in combination with cisplatin in patients with biliary tract cancer : a comparative multicentre study in japan . 
br j cancer 103 : 469 - 474 , 2010 lamarca a , palmer d , wasan h , et al : abc - 06 | a randomised phase iii , multi - centre , open - label study of active symptom control ( asc ) alone or asc with oxaliplatin / 5 - fu chemotherapy ( asc + mfolfox ) for patients ( pts ) with locally advanced / metastatic biliary tract cancers ( abc ) previously - treated with cisplatin / gemcitabine ( cisgem ) chemotherapy . 
j clin oncol 37 , 2019 ( suppl ; abstr 4003 ) javle m , bekaii - saab t , jain a , et al : biliary cancer : utility of next - generation sequencing for clinical management . 
cancer 122 : 3838 - 3847 , 2016 roa i , de toro g , schalper k , et al : overexpression of the her2 / neu gene : a new therapeutic possibility for patients with advanced gallbladder cancer . gastrointest cancer res 7 : 42 - 48 , 2014 galdy s , lamarca a , mcnamara mg , et al : her2 / her3 pathway in biliary tract malignancies ; systematic review and meta - analysis : a potential therapeutic target ? cancer metastasis rev 36 : 141 - 157 , 2017 lowery ma , ptashkin r , jordan e , et al : comprehensive molecular proling of intrahepatic and extrahepatic cholangiocarcinomas : potential targets for intervention . 
clin cancer res 24 : 4154 - 4161 , 2018 slamon dj , leyland - jones b , shak s , et al : use of chemotherapy plus a monoclonal antibody against her2 for metastatic breast cancer that overexpresses her2 . 
bang yj , van cutsem e , feyereislova a , et al : trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of her2 - positive advanced gastric or gastro - oesophageal junction cancer ( toga ) : a phase 3 , open - label , randomised controlled trial . 
lancet 376 : 687 - 697 , 2010 javle mm , hainsworth jd , swanton c , et al : pertuzumab + trastuzumab for her2 - positive metastatic biliary cancer : preliminary data from mypathway . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
ross ds , zehir a , cheng dt , et al : next - generation assessment of human epidermal growth factor receptor 2 ( erbb2 ) amplication status : clinical validation in the context of a hybrid capture - based , comprehensive solid tumor genomic proling assay . 
li bt , shen r , buonocore d , et al : ado - trastuzumab emtansine for patients with her2 - mutant lung cancers : results from a phase ii basket trial . 
ross js , fakih m , ali sm , et al : targeting her2 in colorectal cancer : the landscape of amplication and short variant mutations in erbb2 and erbb3 . 
harding j , cleary j , shapiro g , et al : o - 005 : treating her2 - mutant advanced biliary tract cancer with neratinib : benets of her2 - directed targeted therapy in the phase 2 summit basket trial . 
nature 554 : 189 - 194 , 2018 [ erratum : nature 566 : e11 - e12 , 2019 ] janjigian yy , sanchez - vega f , jonsson p , et al : genetic predictors of response to systemic therapy in esophagogastric cancer . 
cancer discov 8 : 49 - 58 , 2018 iwata h , tamura k , doi t , et al : trastuzumab deruxtecan ( ds - 8201a ) in subjects with her2 - expressing solid tumors : long - term results of a large phase 1 study with multiple expansion cohorts . 
park h , doi t , modi s , et al : oa02.07 : updated results of phase 1 study of ds - 8201a in her2 - expressing or mutated advanced non - small - cell lung cancer . 
meric - bernstam f , beeram m , mayordomo ji , et al : single agent activity of zw25 , a her2 - targeted bispecic antibody , in heavily pretreated her2 - expressing 25 . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular proling of patients tumors to nd potential targets and select treatments for their thorac oncol 13 : s324 , 2018 cancer res 77 , 2017 ( suppl ; abstr 31 ) cancers . 
rod rassekh , md , mhsc5 ; rebecca deyell , md5 ; jennifer rauw , md1 ; meg knowling , md2 ; kong khoo , md6 ; ursula lee , md6 ; krista noonan , md6 ; jason hart , md1 ; r . 
taylor2 ; simon chan , msc2 ; karen mungall2 ; eric chuah2 ; yongjun zhao , dvm2 ; andrew mungall , phd2 ; richard moore , phd2 ; howard lim , phd2 ; daniel j . 
jones , phd2 ; marco marra , phd2 ; and janessa laskin , md2 purpose this study investigated therapeutic potential of integrated genome and transcriptome proling of metastatic sarcoma , a rare but extremely heterogeneous group of aggressive mesenchymal malignancies with few systemic therapeutic options . methods forty - three adult patients with advanced or metastatic non - gi stromal tumor sarcomas of various histology subtypes who were enrolled in the personalized oncogenomics program at bc cancer were included in this study . 
fresh tumor tissues along with blood samples underwent whole - genome and transcriptome sequencing . results the most frequent genomic alterations in this cohort are large - scale structural variation and somatic copy number variation . 
outlier rna expression as well as somatic copy number variations , structural variations , and small mutations together suggest the presence of one or more potential therapeutic targets in the majority of patients in our cohort . 
point mutations or deletions in known targetable cancer genes are rare ; for example , tuberous sclerosis complex 2 provides a rationale for targeting the mammalian target of rapamycin pathway , resulting in a few patients with exceptional clinical benet from everolimus . 
2019 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction adult sarcoma is one of the most difcult cancer types to study in the clinical trial setting , owing to its rarity along with complexity and heterogeneity in histology , tissue origin , and molecular subtypes . 
although improved survival is seen over time in metastatic sarcoma , the prognosis continues to be poor , with a median overall survival of approximately 18 months.1 the genomic prole of adult sarcomas was recently unveiled by a comprehensive genomic study published by the cancer genome atlas ( tcga ) consortium.2 unlike other cancer types , adult sarcomas are characterized by a predominance of copy number variations ( cnvs ) , with relatively few single - nucleotide variants ( snvs ) .2 however , these data were limited to localized primary disease in only six major sarcoma subtypes and did not explore any direct correlation with potential targeted therapies . targeted oncological therapeutics based on genomic proling ( ie , personalized cancer medicine ) , despite many controversies , seem to improve clinical outcome of patients with multiple cancer types . 
 feng et al context key objective using whole - genome and transcriptome sequencing technology , we attempt a systemic analysis of comprehensive proling on a cohort of 43 patients with metastatic non - gi stromal tumor sarcomas to identify therapeutic implication . knowledge generated our data showed large - scale structural variant aberration is the primary mechanism of mutagenesis in metastatic sarcoma . 
in addition , we reported cases of clinical outcomes of personalized oncogenomicsdirected therapy and demonstrated the clinical utility of genomic proling in metastatic sarcomas . furthermore , we reported several novel mutational signatures in metastatic sarcomas , one of which is homologous recombination deciency signature that may associate with superior sensitivity to double - strand dnadamaging agents in several sarcoma subtypes . relevance our results support the use of genomic data in precision medicine and clinical trial design to improve care for patients with metastatic sarcoma . 19 distinct types of advanced metastatic sarcoma as part of the personalized oncogenomics ( pog ) project ( clinicaltrials.gov identier : nct02155621 ) at bc cancer in canada . 
these represent cases refractory to standard therapies that were genomically analyzed with the aim to identify molecular aberrations amenable to a clinically approved targeted therapy or a theoretical targeted therapy under investigation in clinical trials . 
clinical benet of pogdirected therapy was determined by radiographic response on the basis of response evaluation criteria in solid tumors ( recist ; version 1.1 ) and / or progression - free survival of 6 months or more . methods patient samples as previously described , 5 , 6 candidate patients enrolled in pog underwent metastatic tumor biopsies and peripheral blood collection for comparison with detected somatic alterations . 
genome libraries from tumors and blood samples ( normal control ) as well as transcriptome libraries from tumors were constructed using protocols previously described.7 , 8 all patients provided written informed consent for tumor biopsies , blood sample collection , genomic proling , data analysis , and publication of results as part of pog of british columbia approved by the university of british columbia research ethics committee ( reb# h12 - 00137 ) and registered ( clinicaltrials.gov identier : nct02155621 )  . 
raw sequence data and downstream analytics were maintained within a secure computing environment . whole - genome and transcriptome sequencing and bioinformatics paired - end reads from all libraries were generated on illumina hiseq2000 or hiseq2500 sequencer ( illumina , san diego , ca )  . 
determination of somatic snvs , structural variants ( svs ) , cnvs , and gene expression was performed as previously described.5 , 6 transcript outlier expression was determined either by a greater than or a less than two - fold change against tumor illumina bodymap ( arrayexpress id : e - mtab - 513 ) or percentile less than 10% or greater than 90% ( tumor v compendium of tcga ; nih.gov / tcga / )  . 
for gene expression clustering , data were t using the deseq2 package , and hierarchical clustering of log - transformed reads per kilobase of transcript per million mapped reads was performed for genes signicant at an adjusted p value threshold of .01 ( euclidean distance , complete linkage clustering )  . 
the common histologies in this cohort were leiomyosarcoma ( lms ; nongynecologic : n = 7 [ 16% ] and gynecologic : n = 3 [ 7% ] ) , osteosarcoma ( osa ; n = 5 [ 12% ] ) , undifferentiated pleomorphic sarcoma ( ups ; n = 5 [ 12% ] ) , dedifferentiated liposarcoma ( ddlps ; n = 4 [ 9% ] ) , and ewing sarcoma ( n = 3 [ 7% ] ; table 1 )  . 
there were 29 male patients ( 67% ) and 14 female patients ( 33% ) , with a median age at time of metastatic diagnosis of 55 years ( range , 18 to 79 years )  . 
in this cohort , 28 of 43 patients ( 65% ) had received one standard systemic treatment of advanced metastatic disease at the time of sequencing biopsy , and 15 of 43 patients ( 35% ) had received multiple lines ( range , 2 to 7 )  . 
details of standard systemic treatments received in this cohort are described in appendix table a1 . at the time of data analysis , 26 of 43 patients ( 60% ) were deceased , and 17 of 43 ( 40% ) were still alive . potentially targetable alterations in a heterogeneous sarcoma cohort we sought to systematically characterize the genomic landscapes of adult metastatic sarcomas in this heterogeneous cohort and explore how these landscapes relate to therapeutic approaches . 
however , this level of information can potentially be used to inform treatment options for therapies currently available . overall clinical outcome of pog - directed therapy of 42 patients with potentially targetable alterations , 18 ( 43% ) patients attempted pog - directed therapies either in the clinical trial setting or through a compassionate access these , eight of 18 patients ( 44% ) program ( cap )  . 
of derived clinical benet from pog - directed therapy ( table 2 ) and are described in case series of patients who derived clinical benet from pog - directed therapy . response could not be assessed in four cases ( 22% ) owing to short duration ( 2 weeks ) on pog - directed toxicities and / or deterioration of therapies because of performance status ( appendix table a2 )  . 
there were six patients ( 33% ) considered nonresponders to pogdirected therapies , including tyrosine kinase inhibitors , histone deacetylase inhibitors , and immunotherapies ( appendix table a2 )  . 
this result is comparable to a recent study using genomic proling in the clinical setting.15 case series of patients who derived clinical benet from pog - directed therapy infrequent tsc2 mutation / deletion has cases 1 and 2 : therapeutic implications for mammalian target of rapamycin inhibitors . 
case 1 is a 62 - year - old male who presented with recurrent metastatic renal epithelioid angiomyolipoma with lung , liver , peritoneum , and bone metastases ( table 2 )  . 
pog identied a tsc2 pathologic truncating mutation , a relatively well - known event.18 everolimus was given through cap , yielding prolonged partial response ( pr ; appendix fig a3 ) as predicted and continued to show response at 15 months of therapy at the time of analysis . case 2 is a 57 - year - old female who presented with a large right upper lobe mass with mediastinal / hilar lymphadenopathy and pleural effusion and was diagnosed with undifferentiated round cell sarcoma . 
however , the above two cases suggest that the landscape of small mutations and deletions , although rare , has therapeutic relevance in some sarcoma subtypes . our systematic analysis of somatic events based on wholegenome sequencing reveals that the most frequent recurrent alterations in this cohort of adult metastatic sarcomas occur through large - scale structural changes in the genome ( fig 2a ) , rather than through point mutations or small deletions that are frequent in many other cancer types , 20 with a few exceptions of known tumor suppressor genes including tp53 ( approximately 30% ; 13 of 43 ) , atrx ( approximately 12% ; ve of 43 ) , and rb1 ( approximately 7% ; three of 43 ; fig 2b )  . 
 personalized oncogenomics of adult metastatic sarcoma case 3 : targeting common oncogenic amplications such as mouse double minute 2 homolog and cyclin - dependent kinase 4 may have therapeutic implications . 
she subsequently had a pr to a combination of mdm2 and cdk4 inhibitors in a phase ib / ii clinical trial ( clinicaltrials.gov identier : nct02343172 ) and continued to receive therapy for approximately 1 year before death as a result of disease progression . 
although the synergistic effect of mdm2 and cdk4 inhibitors remains controversial22 , 23 pending ongoing clinical trials , the case of this exceptional responder provides rationale for investigating and targeting these genomic abnormalities in this tumor and possibly other sarcoma types . recurrent amplications have been described as a common feature in genomically complex sarcoma subtypes.2 , 24 the canonical 12q13 - 15 amplications targeting mdm2 / cdk4 were observed in ddlps , with an additional case of highgrade osa also harboring this event , suggestive of a dedifferentiated osa arising from a low - grade osa with mdm2 amplication.25 amplication of the oncogene myc on 8q24 was also observed in three of 43 sarcomas . 
the most common region of amplication across this adult sarcoma cohort is 17p11 - 12 altered in 42% ( 18 of 43 ) of cases ( figs 3a and 3b )  . 
strikingly , when we examined the frequency of our recurrent amplication events across tcga cancer types , the amplication on 17p11 - 12 was found to be highly sarcoma specic , which is rarely observed in other tumor types ( fig 3c )  . 
furthermore , the 17p11 - 12 amplicon has been previously described only in osa26 , 27 and lms.28 in our study , this amplicon is observed in a variety of sarcoma subtypes , including ddlps , pleomorphic liposarcoma , osa , lms , chordoma , ups , and undifferentiated endometrial sarcoma ( ues ) , suggesting it harbors an oncogene that is important for sarcoma tumorigenesis . myocd , pmp22 , and cops3 are believed to be potential oncogenic targets within this amplicon in lms and osa.26 - 28 we examined transcriptome expression data for potential oncogenic targets in this region ( fig 3d )  . 
myocd and pmp22 are both within the region most frequently amplied in this cohort , with myocd showing particularly higher expression in amplied samples and pmp22 showing higher expression overall and compared with many other in addition , adora2b was noted as having tumors . amplicon - associated expression ; this gene has not previously been examined as a potential target for this amplicon , but it has been reported to have growth - promoting properties in oral and breast cancers.29 , 30 this analysis suggests that additional functional analysis of genes within this amplicon is required to clearly dene the oncogenic target ( s )  . there are few therapies available that to date , target common amplications in metastatic sarcomas . 
the future development of therapies targeting recurrent amplications such as 17p11 - 12 may be warranted , potentially improving therapeutic options in this disease . case 4 , 5 , and 6 : mutation signatures and homologous recombination deciency may delineate sarcoma subtypes and indicate sensitivity to certain dna - damaging agents . mutation signatures are characteristic patterns of mutation , which may result from specic cellular or environmental pressures and may have implications for therapy.12 the most comprehensive validated set of mutation signatures described to date is reported in cosmic ( sanger.ac.uk / cosmic / signatures )  . 
on the basis of singlenucleotide alterations , we performed mutation signature detection in our sarcoma cohort and identied eight signatures through this de novo process , denoted v1 to v8 ( appendix fig a6 )  . 
comparison of discovered sarcoma signatures to the 30 previously described mutation signatures reported in cosmic31 revealed that sarcoma signatures v1 , v3 , v4 , v5 , v6 , and v8 matched signatures 30 , 5 , 2 , 1 , 8 , and 9 , respectively ( fig 4 )  . 
for example , ddlps possessed similar rearrangement proles , with elevated signature r1 and high mutation burden . signatures v6 and v7 matched signatures 3 and 8 , both of which are associated with hrd signature , 31 also known as brcaness , which has been well described in breast , fig 2 . 
genomic structural complexity is calculated as the average of the proportion of copy segments that are nondiploid and the proportion of the genome represented in nondiploid copy segments , similar to that per the cancer genome atlas research network.2 ( b ) oncoprint of recurrent somatic dna alterations in cancer - related genes observed in sarcomas , grouped by sarcoma subtype . 
types of gene alterations include amplication ( red ) , homozygous deletion ( blue ) , gene fusion ( purple ) , truncating mutation ( black ) , or missense mutation ( green )  . 
 personalized oncogenomics of adult metastatic sarcoma ovarian , and other relatively common cancer types32 including osa.33 we further computed hrd indices and found that in addition to osa , high hrd scores were also seen in lms , ues , and a few other sarcoma subtypes ( fig 4 )  . 
the brcaness phenotype in lms that we observed is consistent with a recent report.34 interestingly , we did not observe deleterious genomic or transcriptomic aberrations of genes such as brca1 and brca2 , which have been described as accounting for the majority of hrd signatures in other tumor types . 
we do observe losses , svs , or downregulated expression of various components implicated in the homologous recombination repair pathway , such as pten , atm , and rad51 ( data not shown ) , suggesting potential alternative contributions to the hrd signature . 
a clear - cut relationship between genetic aberrations and hrd signature is also not observed in other studies.12 , 31 case 4 is a 44 - year - old woman who presented with metastatic ues with lung metastasis . 
the response to ifosfamide was not long - lasting , like all other chemotherapies , and both patients eventually experienced progression , did not respond to any additional treatment , and died as a result of disease progression . 
the hrd signature or brcaness phenotype is associated with therapeutic response to dna - damaging agents , including platinum - based chemotherapies.12 although platinums are not generally used in metastatic soft tissue sarcomas , the dna damaging chemotherapeutic agent ifosfamide has similar , though less - pronounced , dna crosslinking effects . although ifosfamide is an active drug in various sarcoma subtypes , with an overall response rate between 10% and 40% depending on dosing schedule , single - agent response is generally considered low ( , 10% ) , especially in the third - line setting or beyond for sarcomas aside from synovial sarcoma.35 we speculate that the response may relate to partial dna cross - linking property of ifosfamide alkylating agent , which may have therapeutic advantage in hrd tumors . case 6 is 53 - year - old man who presented with recurrent metastatic splenic vein lms with liver and lung metastasis . his disease progressed through docetaxel plus gemcitabine treatment . 
because of a similar hrd signature identied through pog study , he was enrolled in a phase i clinical trial ( clinicaltrials.gov identier : nct02873975 ) investigating an experimental drug ( prexasertib ) targeting hrd tumors . 
these cases support the clinical utility of genomic analysis of hrd and mutation signatures across sarcoma subtypes . case 7 and 8 : potentially targetable aberrations identied solely through transcriptome / expression analysis . 
case 7 is a 77 - year - old male presenting with recurrent multiple intraabdominal ups , which progressed through two cycles of doxorubichis tumors exhibited high rna expression of various tyrosine kinase receptors , such as plateletderived growth factor receptors ; therefore , sunitinib was attempted through cap . 
he then received pog - directed therapy in the form of sunitinib on the basis of his tumor exhibiting high rna expression of fms - like tyrosine kinase 3 and colony - stimulating factor 1 receptor . 
expression in amplicon refers to log ( reads per kilobase of transcript per million mapped reads ) ; increase in amplied samples is measured as expression in amplied samples divided by expression in nonamplied samples in this cohort ; expression percentile is determined relative to all tcga tumors ( see methods )  . 
 ( a ) structural variant ( sv ) mutation signatures ( r1 to r4 ) and single - nucleotide variant ( snv ) mutation signatures ( v1 to v8 ) were deciphered de novo from metastatic sarcomas . 
three dedifferentiated liposarcomas demonstrated high sv and snv burden , with similar r1 rearrangement signature and signatures v4 , v5 , and v6 . signature v4 matched catalogue of somatic mutations in cancer ( cosmic ) signature 2 and is known to be associated with apobec deamination . 
 ( b ) three sarcoma cases ( labeled in red ) with elevated homologous recombination deciency ( hrd ) score and / or the hrd - associated signature 3 demonstrated response to double - strand dnadamaging chemotherapy . 
 ( c ) mutation signatures deciphered de novo from sarcomas were compared against 30 canonical signatures from the cosmic using the cosine similarity metric . signatures that map most closely to a cosmic signature are highlighted . 
 personalized oncogenomics of adult metastatic sarcoma selection who had these two histology subtypes.36 , 37 taken together , these results support the notion that drug efcacy may be dictated by biology measurable through gene expression biomarkers in addition to histology subtype . furthermore , these data support additional research on these putative biomarkers in the context of a complex signaling network , which may help advance the drug development of various tyrosine kinase inhibitors in future sarcoma clinical trials . immune landscape of sarcoma subtypes despite being regarded as a poorly immunogenic tumor because of relatively low mutation burden compared with other cancer types , 2 checkpoint inhibitor immunotherapies have produced promising durable response in a few sarcoma histology subtypes such as ups and alveolar soft part sarcoma thus far.38 , 39 pd - l1 expression has been correlated with efcacy of immunotherapy in some , but not all , cancer types40 and reported as a prognostic marker in soft tissue and bone sarcoma , 41 , 42 but it has not yet been shown to correlate with immunotherapy sensitivity in sarcoma.43 the tumor immune microenvironment plays a key role in determining immunotherapy sensitivity , and emerging data demonstrated a positive correlation between clinical response and preexisting tumor immune microenvironment.44 we examined immune inltration on the basis of gene expression proles ( see methods ) and observed that a subset of tumors show high iiss ( fig 5 ; appendix fig a9 )  . 
we did not observe any correlation between high level of pd - l1 expression and immunotherapy response in a small number of cases ( n = 4 ) within our cohort . interestingly , of the four patients in our cohort treated with immunotherapies , the only patient ( case 8 , lms ) who exhibited some response to immunotherapy also demonstrated an unusually high iis ( fig 5 ; table 2 )  . 
two other cases with high iis , both ups , were not treated with immunotherapy , and two other sarcomas that were treated with immunotherapy , an lms and an osa , had low iis and did not respond . 
overall , our experience suggests that although iis alone may not be sufcient as a predictive biomarker for immunotherapy in investigation , all sarcoma types , particularly in lms . it warrants additional cases 9 and 10 : detection of fusion genes assists in sarcoma diagnosis and therapeutic intervention . 
t - cell inltration score is the sum of all t - cell subtypes excluding regulatory t cells , which are negative modulators . immune inltration score is the sum of scores for all 22 immune cell types proled . 
arms , alveolar rhabdomyosarcoma ; asps , alveolar soft part sarcoma ; ccs , clear cell sarcoma ; chsa , chondrosarcoma ; ddlps , dedifferentiated liposarcoma ; eaml , epithelioid angiomyolipoma ; ews , ewing sarcoma ; mlps , myxoid liposarcoma ; mpnst , malignant peripheral nerve sheath tumor ; msft , malignant solitary brous tumor ; osa , osteosarcoma ; other , groups urs , plps , mlps , ccs , mpnst , eaml , arms , ss , chsa , asps , and sef ; plps , pleomorphic liposarcoma ; sef , sclerosing epithelioid brosarcoma ; ss , synovial sarcoma ; stlms , nongynecologic leiomyosarcoma ; ues , undifferentiated endometrial sarcoma ; ulms , gynecologic leiomyosarcoma ; ups , undifferentiated pleomorphic sarcoma ; urs , undifferentiated round cell sarcoma . sarcoma and change to standard alternating multi - agent chemotherapies with substantial pr . 
her systemic disease also responded to second - line and third - line standard chemotherapies for ewing sarcoma , but she eventually developed brain metastasis and died as a result of disease progression . case 10 is a 68 - year - old man presenting with recurrent metastatic osa ( initial pathologic diagnosis ) of the right femur with lung metastasis . 
 feng et al rapid deterioration shortly after this diagnosis was made from genomic analysis and died as a result of disease progression . within our cohort , in all cases where a fusion would be expected based on pathologic features , we observed a fusion consistent with the sarcoma type ( appendix table a3 )  . the exceptional above two cases , where we identied fusions that had not initially been expected based on pathology , support the utility of genomic proling in rening sarcoma diagnosis and therapeutic intervention , echoing the results of a large retrospective study.17 conclusion our data lend additional support to the current literature data showing that sv and cnv are the primary mechanisms of mutagenesis in sarcomas , as opposed to single - nucleotide alteration . 
we provide anecdotal evidence showing the potential of genomic alterations , such as loss of tsc2 and amplication of mdm2 / cdk4 , to predict exceptional response to targeted treatments . 
overall , we were able to identify potentially actionable genomic alterations in the majority of cases , largely on the basis of outlier rna expression and cnv and sv aberrations . 
renouf , karen gelmon , stephen yip , marco marra , janessa laskin data analysis and interpretation : xiaolan feng , erin pleasance , eric y . zhao , tony ng , jasleen k . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . xiaolan feng honoraria : astrazeneca , nanostring / innomar strategies consulting or advisory role : astrazeneca , ipsen , genomic health , nanostring / innomar strategies , roche tony ng honoraria : nanostring technologies travel , accommodations , expenses : nanostring technologies sara k . 
 personalized oncogenomics of adult metastatic sarcoma krista noonan consulting or advisory role : merck , sano canada , bristol - myers squibb , janssen , pzer , astrazeneca speakers bureau : merck stephen yip consulting or advisory role : bayer , pzer , roche research funding : pzer , bayer , roche , foundation medicine travel , accommodations , expenses : bayer , roche , pzer jason hart honoraria : novartis martin jones employment : qiagen , thermo fisher scientic ( i ) howard lim honoraria : eli lilly / imclone systems , ipsen , merck , roche canada , eisai , taiho pharmaceutical , bristol - myers squibb canada travel , accommodations , expenses : eisai , taiho daniel j . 
renouf honoraria : celgene , servier , taiho pharmaceutical , ipsen , shire research funding : bayer ( inst ) , astrazeneca ( inst ) karen gelmon honoraria : astrazeneca , merck sharp & dohme consulting or advisory role : pzer , novartis , astrazeneca , merck , eli lilly , bristol - myers squibb , nanostring technologies , genomic health , janssen oncology , roche , mylan research funding : pzer ( inst ) , bristol - myers squibb ( inst ) , astrazeneca ( inst ) , roche ( inst ) expert testimony : genentech marco marra travel , accommodations , expenses : roche canada janessa laskin honoraria : boehringer ingelheim , roche canada , astrazeneca , pzer research funding : astrazeneca ( inst ) , roche canada ( inst ) no other potential conicts of interest were reported . acknowledgment we thank katherine mui , jessica nelson , and lindsay zibrik from the personalized oncogenomics ( pog ) program for coordinating our study . this work would not be possible without the participation of our patients and families , the entire pog team , and the generous support of the bc cancer foundation and genome british columbia ( project b20pog )  . 
cell 171 : 950 - 965.e28 , 2017 schwaederle m , zhao m , lee jj , et al : impact of precision medicine in diverse cancers : a meta - analysis of phase ii clinical trials . 
j clin oncol 33 : 3817 - 3825 , 2015 schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
jama oncol 2 : 1452 - 1459 , 2016 jones mr , lim h , shen y , et al : successful targeting of the nrg1 pathway indicates novel treatment strategy for metastatic cancer . 
ann oncol 28 : 3092 - 3097 , 2017 laskin j , jones s , aparicio s , et al : lessons learned from the application of whole - genome analysis to the treatment of patients with advanced cancers . 
cold spring harb mol case stud 1 : a000570 , 2015 shefeld bs , tinker av , shen y , et al : personalized oncogenomics : clinical experience with malignant peritoneal mesothelioma using whole genome sequencing . 
plos one 10 : e0119689 , 2015 jamshidi f , pleasance e , li y , et al : diagnostic value of next - generation sequencing in an unusual sphenoid tumor . 
oncologist 19 : 623 - 630 , 2014 gao j , aksoy ba , dogrusoz u , et al : integrative analysis of complex cancer genomics and clinical proles using the cbioportal . 
timms km , abkevich v , hughes e , et al : association of brca1 / 2 defects with genomic scores predictive of dna damage repair deciency among breast cancer 15 . 
breast cancer res 16 : 475 , 2014 oncotarget 8 : 39254 - 39267 , 2017 italiano a , khalifa e , laizet y , et al : genetic landscape of soft - tissue sarcomas : moving toward personalized medicine . 
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cytogenet genome res 150 : 52 - 59 , 2016 van dartel m , redeker s , bras j , et al : overexpression through amplication of genes in chromosome region 17p11.2 approximately p12 in high - grade osteosarcoma . 
lee sh , chang mh , baek kk , et al : high - dose ifosfamide as secondor third - line chemotherapy in refractory bone and soft tissue sarcoma patients . 
mahmood st , agresta s , vigil ce , et al : phase ii study of sunitinib malate , a multitargeted tyrosine kinase inhibitor in patients with relapsed or refractory soft tissue sarcomas . 
tawbi ha , burgess m , bolejack v , et al : pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , 39 . 
kim jr , moon yj , kwon ks , et al : tumor inltrating pd1 - positive lymphocytes and the expression of pd - l1 predict poor prognosis of soft tissue sarcomas . 
wei s , shreiner ab , takeshita n , et al : tumor - induced immune suppression of in vivo effector t - cell priming is mediated by the b7 - h1 / pd - 1 axis and transforming growth factor beta . 
the number of potentially targetable alterations was determined by comparing observed somatic mutations and gene expression alterations to a database of events that have clinical or preclinical evidence of potential therapeutic targeting , on the basis of therapeutics currently available or in development . mutation copy number expression only samples with potentially targetable alterations ( % ) fig a2 . 
samples with potentially targetable alterations were determined by comparing observed somatic mutations and gene expression alterations to a database of events that have clinical or preclinical evidence of potential for therapeutic targeting , on the basis of therapeutics currently available or in development . 
 feng et al baseline before standard chemotherapy ( april 2016 ) progression after standard chemotherapy ( august 2016 ) response to pog - directed therapy ( july 2017 ) fig a3 . 
 personalized oncogenomics of adult metastatic sarcoma baseline before standard chemotherapy ( january 2015 ) progression after standard chemotherapy ( may 2015 ) response to pog - directed therapy ( december 2015 ) fig a4 . 
annotation tracks show exposure values calculated from mutation analysis ( structural variant [ sv ] , single - nucleotide variant [ snv ] burden ) , clinical covariates , and histologic properties of the sarcoma cohort . 
 feng et al baseline before standard chemotherapy ( august 2015 ) progression after standard chemotherapy ( july 2016 ) response to pog - directed therapy ( october 2016 ) fig a7 . 
 personalized oncogenomics of adult metastatic sarcoma baseline ( feb 2015 ) progression after standard chemotherapy ( april 2015 ) response to pog - directed therapy ( october 2015 ) fig a8 . 
other than undifferentiated pleomorphic sarcoma ( ups ) , some leiomyosarcoma ( lms ) and dedifferentiated liposarcoma ( ddlps ) and one case of synovial sarcoma ( ss ) seem to have relatively high iis compared with others . 
 precision oncology strategy in trastuzumab - resistant human epidermal growth factor receptor 2positive colon cancer : case report of durable response to ado - trastuzumab emtansine introduction colorectal cancer is the third most common cancer and the fourth leading cause of cancer death worldwide.1 metastatic disease is ultimately identified in the majority of patients with colorectal cancer and , with rare exceptions , is considered incurable . 
the treatment of metastatic colorectal cancer ( mcrc ) has historically included the use of fluorouracil in combination with other chemotherapeutic agents , including oxaliplatin or irinotecan . the addition of the antivascular endothelial growth factor antibody , bevacizumab , to standard chemotherapy regimens has improved the progression - free and overall survival of patients with mcrc and has signaled a shift toward the addition of biologic and targeted agents in the treatment of advanced cancer.2 , 3 the transition toward molecularly targeted therapies has gained additional momentum with the us food and drug administration approval of the antiepidermal growth factor receptor agents cetuximab and panitumumab for the treatment of kras wild - type colorectal cancers.4 , 5 unfortunately , many patients with mcrc progress through these therapies , or are not candidates to receive them on the basis of the molecular profile of their particular tumor , and are left with few treatment options . 
 the tumor exhibited normal expression of the mismatch repair genes mlh1 , msh2 , msh6 , and pms2 . shortly after diagnosis , the patient began palliative chemotherapy with capecitabine and oxaliplatin every 3 weeks . 
however , follow - up imaging 6 months after treatment initiation identified progressive disease in the liver and lung , as well as a new adrenal gland metastasis . the patients treatment was then changed to capecitabine plus irinotecan and , ultimately , capecitabine , irinotecan , plus cetuximab , but his tumor continued to progress through each of these regimens , as determined by an increasing size of multiple hepatic metastases ( table 1 )  . 
we used a standard set of her2 - specific taqman primers and probes ( thermo fisher scientific , foster city , ca ) compared with standard references using an ultraconserved region on chromosome 1 . 
briefly , taqman pcr reaction mixtures were assembled using 2x ddpcr supermix for probes , 20x assays ( 18 mm primers and 5 mm probe ) and restriction digested dna samples ( bio - rad )  . 
this standard reference assay used the following primers : forward primer : 59 - tgagggattcggcagatgttg - 39 ; reverse primer : 59 - ctgaaaggctggacttgacaga - 39 ; and probe : 59 - vic - actgtgtgctggacctmgb - 39 . 
all assay primers were ordered from integrated dna technologies ( coraville , ia )  . thermal cycling conditions were 95c for 10 minutes ( 1 cycle ) ; 94c for 30 seconds and 60c for 60 seconds ( 40 cycles ) ; 98c for 10 minutes ( 1 cycle ) , and a 12c hold . 
her2 copy number per cell was estimated as the ratio of the her2 and rna polymerase 30 ( rpp30 ) concentrations multiplied by two to account for the two copies of rpp30 that are expected per diploid genome . 
quadruplicate ddpcr wells were analyzed for each sample . results in the absence of additional treatment options , and given the patients good performance status , another liver biopsy was performed and nextgeneration sequencing was completed in a certified laboratory , which identified several tumor - specific somatic mutations , including apc r232 * , tp53 splice site 97_1g.a , and her2 amplification . the patients case and tumor genomics were then presented to a multi - institutional molecular tumor board for interpretation . the identification of a mutation in the adenomatous polyposis coli ( apc ) gene was expected and consistent with previous reports in which up to 85% of spontaneous colorectal cancers harbor somatic mutations in the classic tumor suppressor.16 a splice site mutation in the tp53 gene was equally unsurprising , given the relative frequency of tp53 mutations in human cancers.17 , 18 the molecular tumor board considered neither the apc nor tp53 mutations clinically actionable . treatment duration , months best outcome table 1 . 
cross - reference with the cancer genome atlas confirmed that approximately 4% to 5% of spontaneous colorectal cancers harbor high - level her2 amplifications , 19 and preclinical data predicted that anti - her2 therapy might be clinically effective , particularly when used in a combinatorial approach ( table 2 ) .20 , 21 gene alteration r232 * tp53 splice site 97_1g > a erbb2 amplification fig 1 . 
tumor - specific somatic alterations and quantification of the her2 copy number alteration . ( a ) next - generation sequencing identified three validated alterations in the patients hepatic metastatic colon cancer . 
 ( b ) using a droplet digital polymerase chain reaction assay , the total copies of her2 per genome in the patients metastatic tumor ( blue dot ) were measured and compared with the total copies of her2 in the patients germline ( peripheral blood , gold dot )  . 
error bars represent standard error of the mean . peripheral blood tumor to further characterize the her2 amplification and to validate the finding using an orthogonal method , a ddpcr assay was used . 
in contrast , a control gene , rpp30 , had the expected diploid copy number of two ( fig 1 )  . given the genomic findings and the patients clinical circumstances , treatment with trastuzumab was initiated . 
follow - up ct imaging , compared with baseline evaluation , revealed disease progression in the liver , with the largest lesion measuring 5.8 cm ( figs 2a and 2b )  . trastuzumab treatments were discontinued and the patient then received trastuzumab - emtansine ( t - dm1 ) infusions every 21 days for three total treatments . 
follow - up imaging revealed the largest hepatic metastasis measured 4.6 cm , compared with 5.3 cm at the initiation of t - dm1 ( fig 2c )  . three additional infusions at 21 - day intervals with subsequent imaging yielded ongoing disease response , with the largest hepatic mass measuring 3.2 cm ( fig 2d )  . 
the patient ultimately received t - dm1 infusions every 21 days for 15 months without any discernible negative clinical effect . the largest hepatic metastasis decreased to 2.1 cm ( fig 2e ) and two other metastases responded completely . 
the use of next - generation sequencing panels to identify actionable mutations and guide treatment has become increasingly scrutinized as a potentially viable approach for improving outcomes in a variety of cancer subtypes , including lung cancer and melanoma . 
these findings are bolstered by an interim analysis report from the mypathway study2 investigating the use of the combination of trastuzumab plus pertuzumab in various solid tumors , including mcrc . the case reported here suggests that genomicsbased analysis of refractory colorectal cancer can lead to effective targeted treatments . 
the expected progression - free survival and overall survival of a patient with mcrc with refractory disease is approximately 1.7 and 5 months , respectively , 25 in contrast to the 15 - month progression - free survival observed in this case . additional data and outcomes are required to confirm that precision oncology routinely yields superior outcomes ; however , this report illustrates an additional treatment option in patients with refractory disease who have exhausted all of the commonly used therapeutics for their respective disease and yet retain an acceptable performance status and desire additional treatmenta common clinical scenario . 
kamangar f , dores gm , anderson wf : patterns of cancer incidence , mortality , and prevalence across five continents : defining priorities to reduce cancer disparities in different geographic regions of the world . 
saltz lb , clarke s , daz - rubio e , et al : bevacizumab in combination with oxaliplatin - based chemotherapy as first - line therapy in metastatic colorectal cancer : a randomized phase iii study . 
douillard jy , siena s , cassidy j , et al : randomized , phase iii trial of panitumumab with infusional fluorouracil , leucovorin , and oxaliplatin ( folfox4 ) versus folfox4 alone as first - line treatment in patients with previously untreated metastatic colorectal cancer : the prime study . 
slamon dj , clark gm , wong sg , et al : human breast cancer : correlation of relapse and survival with amplification of the her - 2 / neu oncogene . 
sartore - bianchi a , trusolino l , martino c , et al : dual - targeted therapy with trastuzumab and lapatinib in treatmentrefractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - ofconcept , multicentre , open - label , phase 2 trial . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors based on molecular profiles : early results from mypathway , an open - label , phase iia umbrella basket study . 
richman sd , southward k , chambers p , et al : her2 overexpression and amplification as a potential therapeutic target in colorectal cancer : analysis of 3256 patients enrolled in the quasar , focus and piccolo colorectal cancer trials . 
sartore - bianchi a , ardini e , bosotti r , et al : sensitivity to entrectinib associated with a novel lmna - ntrk1 gene fusion in metastatic colorectal cancer . 
bertotti a , migliardi g , galimi f , et al : a molecularly annotated platform of patient - derived xenografts ( xenopatients ) identifies her2 as an effective therapeutic target in cetuximab - resistant colorectal cancer . 
parikh a , atreya c , korn wm , et al : prolonged response to her2 - directed therapy in a patient with her2amplified , rapidly progressive metastatic colorectal cancer . 
bensch f , van rooijen jm , schr oder cp , et al : a 21 - year - old patient with a her2 - positive colorectal cancer . discov 5 : 832 - 841 , 2015 gastroenterology 148 : 20 - 21 , 2015 cancer . 
grothey a , van cutsem e , sobrero a , et al : regorafenib monotherapy for previously treated metastatic colorectal cancer ( correct ) : an international , multicentre , randomised , placebo - controlled , phase 3 trial . 
johnson , phd1 purpose given regulatory approval of immune checkpoint inhibitors in patients with mismatch repairdecient ( mmr - d ) cancers agnostic to tumor type , it has become important to characterize occurrence of mmr - d and develop cost - effective screening approaches . 
using a next - generation sequencing ( ngs ) panel ( oncopanel ) , we developed an algorithm to identify mmr - d frequency in tumor samples and applied it in a clinical setting with pathologist review . methods to predict mmr - d , we adapted methods described previously for use in ngs panels , which assess patterns of single base - pair insertion or deletion events occurring in homopolymer regions . 
for tumors tested after june 2017 , sequencing results were presented to pathologists in real time for clinical mmr determination , in the context of tumor mutation burden , other mutational signatures , and clinical data . results of 20 , 301 tumors sequenced , 2.7% ( 553 ) were retrospectively classied as mmr - d by the algorithm . of 4 , 404 samples with pathologist sign - out of mmr status , the algorithm classied 147 ( 3.3% ) as mmr - d : in 116 cases , mmr - d was conrmed by a pathologist , ve cases were overruled by the pathologist , and 26 were assessed as indeterminate . 
overall , the highest frequencies of oncopanel - inferred mmr - d were in endometrial ( 21% ; 152 / 723 ) , colorectal ( 9.7% ; 169 / 1 , 744 ) , and small bowel ( 9.3% ; 9 / 97 ) cancers . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction as regulatory approvals for immunotherapy agents expand across tumor types , efforts to identify predictive biomarkers of response or resistance to treatment are similarly expanding . 
comprehensive analysis of colorectal cancers has shown that tumors with defects in mismatch repair ( mmr ) , resulting in microsatellite instability ( msi ) , have elevated lymphocytic inltration.1 in addition , tumors with msi demonstrate upregulated expression of inhibitory immune checkpoints , including pd - l1 , on tumorinltrating lymphocytes and myeloid cells . 
overall , the algorithm classied 2.7% of samples as mmr - d . relevance we show the value of using a routine ngs panel to identify new , clinically relevant biomarkers that might otherwise not be assessed because of low prevalence in certain tumor types and to identify potential candidates for immunotherapy . testing using ihc or pcr is not routinely pursued in clinical practice in other tumor types , despite national comprehensive cancer network testing recommendations for the rectal , endometrial , following cancers : cervical , colon , esophageal , gastroesophageal junction , gastric carcinoma , gallbladder , intrahepatic cholangiocarcinoma , extrahepatic cholangiocarcinoma , neuroendocrine , ovarian , pancreatic , prostate , testicular , and vulvar . 
broad implementation of a targeted , tumor - only next - generation sequencing ( ngs ) assay ( oncopanel ) for patients at dana - farber cancer institute ( dfci ) , brigham and womens hospital ( bwh ) , and boston childrens hospital ( bch ) allowed us to assess whether bioinformatic analysis of oncopanel7 data could characterize the prevalence of mmr - d / msi - h ( hereafter mmr - d ) across tumors and increase the number of patients who could be considered for immunotherapy . methods such as msings , 8 msi - sensor9 and cell - free dna10 have previously been reported for detection of mmr - d . 
however , given the wide implementation and relatively low cost of tumor - only ngs , it is important to develop approaches suited for this paradigm and understand potential differences in results . 
it is also critical to better characterize the frequency of mmr - d across tumors to inform selective use of ihc , pcr , or ngs assays in clinical settings where ngs panels and mmr testing are used less frequently . 
this study expands on previous work to develop oncopanel for clinical assessment of mmr - d using ihc and pcr for validation11 and to characterize mmr status in 645 upper gi tract cancers12 and 304 sarcomas.13 here we describe a bioinformatics algorithm that infers mmr status using an institution - wide ngs panel and report the prevalence of mmr - d across  . 
of these tumors , 4 , 488 were sequenced after the implementation on june 27 , 2017 of a process for pathologist sign - out of ngsbased , mmr - d assessment , described in more detail below . 
a total of 4 , 404 of these 4 , 488 tumors met criteria for mmr assessment via the oncopanel algorithm , which measures insertion or deletion ( indel ) events within homopolymeric microsatellite loci to infer mmr status , and were presented for nal interpretation by a molecular pathologist . 
signed - out oncopanel reports , including mmr - d calls , were returned to physicians for clinical use . patients from the aforementioned study of 304 sarcomas13 are also included in the summary data here , although with different subclassications . 
here , we used the original pathologists diagnoses as recorded at oncopanel sign - out , rather than more detailed subclassication of sarcomas using chart review . sequencing from august 2013 to july 2014 , patient samples were tested with oncopanel version 1 , which covers 0.753334 mb and the full coding regions of 275 genes , plus selected intronic regions of 30 genes for rearrangement detection . 
at the time of clinical pathology assessment for mmr deciency ( on or after june 27 , 2017 ) , all samples were being sequenced using oncopanel version 3.14 variants observed in public genome databases at a frequency of  . 
finally , variants were tiered and reported based on clinical significance by a molecular pathologist using methods previously described.16 all testing was conducted in a clinical laboratory improvement amendmentscertied environment . mmr algorithm on the basis of methods described previously for identifying mmr - d in colorectal cancer using oncopanel versions 1 - 2 , 11 an internally developed algorithm was adjusted to predict mmr status across all tumor types . 
only single base - pair patterns of single base - pair indels in homopolymers were considered ( with a minimum threshold of 1.5 / mb ) , and tumor mutational burden ( tmb ) was ignored . possible values resulting from the oncopanel algorithm are procient ( mmr - p ) , decient ( mmr - d ) , and cannot assess ( for tumors with , 12 variants ) , although a pathologist may override algorithmic calls or mark a tumor indeterminate . for the 4 , 488 samples where mmr results were communicated to the ordering physician , a pathologist manually reviewed the algorithmic mmr status to assign nal status . 
pathologists interpreted the algorithmic mmr determination in the context of tmb , other mutational signatures validated on the platform ( uv [ ultraviolet ] , tobacco , apobec [ apolipoprotein b mrna editing enzyme , catalytic polypeptide - like ] , temozolomide , and pole [ dna polymerase epsilon catalytic subunit ] ) , and existing clinical data such as mmr protein expression , when available . 
recognizing that the positive and negative predictive values of the mmr algorithm are lower near the dened cutoff , and that patterns of mmr - d are not well dened for tumors outside of colon and endometrium , the pathologist could elect to override the algorithmic classication . 
possible reasons for overriding the classication included homopolymer indel rates near the cutoff , low tmb for that tumor type , or no mmr gene alterations in the sequencing data . the treating clinician was also encouraged to seek conrmatory testing with ihc or pcr in this setting when clinically relevant . tmb was calculated by including all nonsynonymous mutations in coding regions of the genome covered by oncopanel . 
we reported three tmb metrics for each tumor : mutations per megabase , percentile of tmb across all tumors sequenced in the current oncopanel version , and percentile of tmb across tumors of each cancer type . orthogonal testing twelve of the 26 tumor samples with discrepant calls between algorithm and pathologist , specically those with algorithm - predicted mmr - d , a pathologist call of indeterminate , and sufcient leftover dna , underwent orthogonal , tumor - only pcr testing . 
overall , among 3 , 779 noncolorectal , nonendometrial samples for which oncopanel results were returned to clinicians , 43 ( 1.14% ) tumors were detected as msi - h / mmr - d , and results were reported to the patients treating clinicians . without another indication for clinical msi / mmr testing , these 43 patients are unlikely to have been tested outside of the oncopanel program . across the 816 pediatric tumors proled , eight were predicted as mmr - d algorithmically . 
pcr - based orthogonal validation was performed on the small bowel case to conrm msi - h status , and msi was detected for three of four microsatellite markers . we identied two adult appendiceal tumors with predicted mmr - d : one predicted by the algorithm in the historical cohort and the other identied by a pathologist during routine clinical sign - out . 
17 - 465 all represents the overall oncopanel cohort using algorithm prediction , and 17 - 465 pathologist assessed represents the subset with pathology sign - out . abbreviations : mmr - d , mismatch repair deciency ; n / a , tumor type not assessed or specied . mmr - d has not been reported previously in appendiceal cancer . 
in addition , we found one thymic mmr - d tumor among ve cases ( 20% ) , indicating that thymic cancers too can be mmr - d , corroborating a recent report.20 the cancer genome atlas ( tcga ) and therapeutically applicable research to generate effective treatments ( target ) projects20 reported msi - h status in 3.8% of tumors , using paired tumor - normal sequencing across cancer types and the algorithm mantis , 40 and identied in 27 cancer types ( see discussion )  . 
one factor among many that could play a role in discordance between algorithmic prediction and pathologist assessment ( table 5 ) is tmb , which was relatively high in concordant mmr - d cases ( mean tmb , 55.8 mut / mb )  . 
for the 4 , 404 we found 2.72% of 20 , 301 tumor samples to be mmr - d across a wide range of adult and pediatric malignancies using a bioinformatics algorithm to process tumor - only ngs data . 
mapping of tumor types from sources original tumor type mapped tumor type colon adenocarcinoma rectal adenocarcinoma colorectal adenocarcinoma barret esophagus adenocarcinoma esophageal carcinoma gastric adenocarcinoma stomach or gastric adenocarcinoma esophagogastric junction carcinoma pancreatic adenocarcinoma uterine carcinosarcoma kidney chromophobe kidney renal clear cell carcinoma kidney renal papillary cell carcinoma kidney cancer sarcoma glioblastoma multiforme lower - grade or low - grade glioma merkel cell carcinoma colorectal cancer colorectal cancer colorectal cancer esophagogastric carcinoma esophagogastric carcinoma esophagogastric carcinoma esophagogastric carcinoma esophagogastric carcinoma pancreatic cancer uterine sarcoma renal cell carcinoma renal cell carcinoma renal cell carcinoma renal cell carcinoma soft tissue sarcoma glioma glioma skin cancer , nonmelanoma small intestinal malignancies small bowel cancer extrahepatic bile duct adenocarcinoma biliary cancer malignant solitary brous tumor of the pleura soft tissue sarcoma ovarian surface epithelial carcinoma nonepithelial ovarian cancer ovarian cancer ovarian cancer cervical squamous cell carcinoma / endocervical cervical cancer adenocarcinoma pediatric acute myeloid leukemia acute myeloid leukemia pediatric high - risk wilms tumor wilms tumor poorly differentiated carcinoma , nos cancer of unknown combined small - cell lung carcinoma lung bronchioloalveolar carcinoma thyroid carcinoma thymic carcinoma head and neck squamous carcinoma nut midline carcinoma of the head and neck prostatic adenocarcinoma primary small - cell lung cancer nonsmall - cell lung cancer thyroid cancer thymic tumor head and neck carcinoma head and neck carcinoma prostate cancer abbreviations : nos , not otherwise specied ; nut , nuclear protein in testis . agreement between purely algorithmic calls and formal pathologist classication . 
it should be noted that these two measures are not independent , because the pathologists included the algorithmic calls as a part of their assessment , along with tmb , results of other mutational signatures , and existing clinical data . 
orthogonal laboratory validation of tumors predicted to be mmr - d but signed out as indeterminate demonstrated the value of manual pathologist review as a nal step in the mmr - d classication process and suggests that inclusion of other data types could improve future algorithms . conrming prior clinical observations , frequencies of predicted mmr - d were in endometrial and colorectal cancers , but mmr - d was also observed in many different cancer types not commonly assessed for mmr - d in routine clinical practice , including appendiceal cancer and nonmelanoma skin cancer . the highest further manual review of predicted mmr - d tumors signed out as indeterminate highlighted the tendency for tumors with a pattern of indels in homopolymer regions but low tmb to be called indeterminate . 
our results suggest conrmatory laboratory testing should continue to be used , especially when borderline ngs results are obtained or mmr - d is predicted in a tumor with low mmr - d prevalence . 
correlation between high tmb and msi - h has been reported in other ngs studies , including in prostate cancer , where 71% of 111 tumors with high tmb ( 20 mut / mb ) were msi - h , 41 and in adrenocortical carcinoma ( n = 92 ) and cervical squamous cell and cervical adenocarcinoma ( n = 305 ) .20 in a larger ngs panel study ( n = 11 , 000 ) , only 27% of tumors with high tmb ( dened as 17 mut / mb ) were msi - h ( 46 altered microsatellite loci / mb ) , whereas 70% of msi - h cases had high tmb.21 as exemplied in these studies , however , there is signicant variability in the denitions of high tmb and the methodologies used to measure it.42 recent fda approval of pembrolizumab for high - tmb tumors dened high tmb as 10 mut / mb , with a targeted gene panel as a companion diagnostic . 
 clinical assessment of mmr deciency using targeted ngs measure names oncopanel pathologist oncopanel all bonneville middha vanderwalde dudley colorectal cancer endometrial cancer esophagogastric carcinoma head and neck carcinoma hepatocellular carcinoma prostate cancer renal cell carcinoma soft tissue sarcoma thyroid cancer fig 1 . 
across all studies described in table 3 , 18 - 39 the frequency of mmr - d or msi - h was reported across all six cohorts in nine tumor types : colorectal , endometrial , esophagogastric , head and neck , hepatocellular , prostate , renal cell carcinoma , thyroid cancer , and soft tissue sarcoma . 
hepatocellular carcinoma and thyroid cancer had considerably higher msi - h rates reported in the review by dudley et al.19 it is encouraging , however , that mmr - d prevalence in most tumor types across independent studies was generally consistent ( fig 1 ) , especially for other ngs - based table 4 . 
mean tmb across 4 , 404 oncopanel tumors , subcategorized by algorithm - predicted mmr status and pathologist - assessed mmr status pathologist assessment algorithm mmr - d algorithm mmr - p pathologist mmr - d pathologist mmr - p pathologist indeterminate 54.96 ( 116 ) 17.34 ( 5 ) 17.61 ( 26 ) 47.36 ( 147 ) mean tmb 72.24 ( 6 ) 7.58 ( 4 , 213 ) 22.71 ( 38 ) 8.40 ( 4 , 257 ) 55.81 ( 122 ) 7.59 ( 4 , 218 ) 20.64 ( 64 ) 8.99 ( 4 , 404 ) note . 
across tumor types , it remains unclear which methodology to determine mmr status provides greater accuracy , and ngs computational algorithms may improve identication of these tumors compared with tmb , pcr , or ihc testing . 
it will also be important for future studies to measure the impact of mmr - d assessment on treatment decisions and patient outcomes . given the low overall frequency of mmr - d across most noncolorectal , nonendometrial tumors , we believe our algorithm provides a cost - effective initial screening tool to identify patients for pcror ihc - based testing . 
from a clinical implementation standpoint , rather than testing all patients with cancer with pcr or ihc to identify the , 3% of patients who may be candidates for immune checkpoint inhibitors on the basis of mmr - d , implementing the algorithm in the context of an existing , multipurpose ngs tumor - only panel , can provide an efcient initial screen and allow clinicians to select only those tumors most likely to be mmr - d for further testing . 
biomarker studies in patients with mmr - d tumors treated with immune checkpoint inhibition will provide further insight . in the near future , combined testing of many biomarkers across a large panel of genes as described here may be more efcient in cost , time , and sample material than sequential or more selective biomarker testing , and it also offers the ability to quickly incorporate new biomarker discoveries into clinical practice and bring effective treatments to patients who would otherwise not benet from these discoveries . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / authors / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . mayur amonkar employment : merck stock and other ownership interests : merck alanna j . 
church honoraria : biorad laboratories , jackson laboratories consulting or advisory role : alphasights , samba scientic , perceptive advisors , jackson laboratories , bayer travel , accommodations , expenses : jackson laboratories , bayer adem albayrak employment : health catalyst stock and other ownership interests : health catalyst honoraria : bc platforms research funding : merck ( inst ) travel , accommodations , expenses : health catalyst other relationship : guidepoint marios giannakis research funding : bristol myers squibb , merck renato umeton consulting or advisory role : health catalyst patents , royalties , other intellectual property : patent : portable medical device and method for quantitative retinal image analysis through a smartphone ; patent : epstein barr virus genotypic variants and uses thereof as risk predictors , biomarkers , and therapeutic targets of multiple sclerosis elizabeth h . 
johnson consulting or advisory role : novartis , foundation medicine , hengrui therapeutics , daiichi sankyo , chugai pharmaceuticals , lilly , checkpoint therapeutics research funding : toshiba ( inst ) , novartis ( inst ) , novartis patents , royalties , other intellectual property : dana - farber cancer institute kai - li liaw employment : merck sharp & dohme stock and other ownership interests : merck sharp & dohme research funding : merck sharp & dohme travel , accommodations , expenses : merck sharp & dohme katherine a . 
nowak patents , royalties , other intellectual property : provisional patent application involving novel methods for characterizing immune cell distributions in solid tumors . lynette sholl honoraria : astrazeneca consulting or advisory role : loxo oncology , emd serono research funding : roche / genentech nancy u . 
lin consulting or advisory role : seattle genetics , puma biotechnology , daiichi sankyo , california institute for regenerative medicine , denali therapeutics research funding : genentech , pzer , seattle genetics , merck patents , royalties , other intellectual property : royalties for chapter in upto - date regarding management of breast cancer brain metastases ; royalties , jones & bartlett jason m . 
johnson consulting or advisory role : ucb , patientslikeme research funding : merck travel , accommodations , expenses : ucb no other potential conicts of interest were reported . acknowledgment we thank kaitlyn t . 
bifolck , ba , for her editorial support . references llosa nj , cruise m , tam a , et al : the vigorous immune microenvironment of microsatellite instable colon cancer is balanced by multiple counter - inhibitory checkpoints . 
newsroom / pressannouncements / ucm560167.htm. le dt , durham jn , smith kn , et al : mismatch repair deciency predicts response of solid tumors to pd - 1 blockade . 
murphy km , zhang s , geiger t , et al : comparison of the microsatellite instability analysis system and the bethesda panel for the determination of microsatellite instability in colorectal cancers . 
am j cancer res 8 : 1977 - 1988 , 2018 salipante sj , scroggins sm , hampel hl , et al : microsatellite instability detection by next generation sequencing . 
nowak ja , yurgelun mb , bruce jl , et al : detection of mismatch repair deciency and microsatellite instability in colorectal adenocarcinoma by targeted nextres 25 : 7035 - 7045 , 2019 generation sequencing . 
christakis ag , papke dj , nowak ja , et al : targeted cancer next - generation sequencing as a primary screening tool for microsatellite instability and lynch syndrome in upper gastrointestinal tract cancers . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
vanderwalde a , spetzler d , xiao n , et al : microsatellite instability status determined by next - generation sequencing and compared with pd - l1 and tumor mutational burden in 11 , 348 patients . 
glavac d , volavsek m , potocnik u , et al : low microsatellite instability and high loss of heterozygosity rates indicate dominant role of the suppressor pathway in squamous cell carcinoma of head and neck and loss of heterozygosity of 11q14.3 correlates with tumor grade . 
chiappini f , gross - goupil m , saffroy r , et al : microsatellite instability mutator phenotype in hepatocellular carcinoma in non - alcoholic and non - virally infected normal livers . 
murphy ma , wentzensen n : frequency of mismatch repair deciency in ovarian cancer : a systematic review this article is a us government work and , as such , is in the public domain of the united states of america . 
hammerschmied c , stoehr r , walter b , et al : the role of elevated microsatellite alterations at selected tetranucleotides ( emast ) in renal cell carcinoma ( rcc )  . cancer res 67 , 2007 ( abstr 1934 ) 35 . 
palmieri g , ascierto pa , cossu a , et al : assessment of genetic instability in melanocytic skin lesions through microsatellite analysis of benign naevi , dysplastic naevi , and primary melanomas and their metastases . 
cesinaro am , ubiali a , sighinol p , et al : mismatch repair proteins expression and microsatellite instability in skin lesions with sebaceous differentiation : a study in different clinical subgroups with and without extracutaneous cancer . 
reuschenbach m , sommerer c , hartschuh w , et al : absence of mismatch repair deciency - related microsatellite instability in non - melanoma skin cancer . j invest dermatol 132 : 491 - 493 , 2012 39 . 
vokes ni , liu d , ricciuti b , et al : harmonization of tumor mutational burden quantication and association with response to immune checkpoint blockade in non - small - cell lung cancer . 
boland cr , thibodeau sn , hamilton sr , et al : a national cancer institute workshop on microsatellite instability for cancer detection and familial predisposition : development of international criteria for the determination of microsatellite instability in colorectal cancer . 
comparison of oncopanel mmr algorithm with historical clinical msi / mmr testing laboratory assessment algorithm mmr - d algorithm mmr - p total laboratory msi - h laboratory mss total note . 
 clinical use of precision oncology decision support purpose precision oncology is hindered by the lack of decision support for determining the functional and therapeutic significance of genomic alterations in tumors and relevant clinically available options . 
to bridge this knowledge gap , we established a precision oncology decision support team that provides annotations at the alteration level and subsequently determined whether clinical decision making was influenced . methods genomic alterations were annotated to determine actionability on the basis of a variants known or potential functional and / or therapeutic significance . 
a webbased survey was implemented to capture the reasons genotype - matched therapies were not pursued . results the precision oncology decision support team processed 1 , 669 requests for annotation of 4 , 084 alterations ( 2 , 254 unique ) across 49 tumor types for 1 , 197 patients . 
sixty - six percent of patients had at least one actionable / potentially actionable alteration , and 20.6% of patients ( 110 of 535 ) annotated enrolled in a genotype - matched trial . 
clinicians cited a variety of reasons that patients with actionable alterations did not enroll in trials . conclusion over half of alterations annotated were of unknown significance or nonactionable . physicians were more likely to enroll a patient in a genotype - matched trial when an annotation supported actionability . 
 research indicates that clinicians are unlikely to use sources that take longer than 30 seconds to retrieve data10 and that information presented in graphical summaries enhances interpretation , improving health care quality.11 , 12 second , limited information may be exposed because these web sites are public facing . 
third , novel alterations continue to be discovered , and information is rapidly evolving , generally outpacing the rate of updates . thus , there is a need for an on - demand , real - time clinical interpretation service that annotates all requested alterations , beyond those available within accessible knowledge bases , to determine their actionability . the precision oncology decision support system ( pods ) was established at the university of texas md anderson cancer center in recognition of these needs.9 herein , we report our experience with large - scale , institution - wide decision support and its initial clinical utility . 
all requestors indicating the same physician as the contact for correspondence were considered a teastatistical significance was evaluated by a x2 test . annotation process and return of reports pods scientists receive requests , access our knowledge base of variant annotations , and review and update content as applicable.9 , 13 reports consist of a data summary with references and alteration frequency from external ( cbioportal , cosmic [ catalogue of somatic mutations in cancer ] ) and internal databases . 
in 2015 , reports evolved to routinely contain a functional significance , gene , and alteration - level actionability call ( table 1 ) .7 , 12 all reports are reviewed by the medical director and returned via e - mail . 
starting in august 2015 , reports referencing clia - validated panels were deposited within md andersons electronic health record ( ehr )  . manual review of clinical data medical records of 539 patients annotated in 2015 through clinician - initiated requests or for treatment planning conferences were reviewed for the presence of a clinical trial entrance note in the patients ehr . 
potential matches between the annotated variants and targeted therapy used within the trial were manually recorded . clinical decision follow - up surveys a web - based survey was initiated in 2015 , and 236 surveys were sent to annotation requestors with a 1 - month postannotation delivery date to ascertain whether the patient matched to genomically guided therapy . 
for patients not enrolled to receive therapy on the basis of the annotation provided , the survey inquired as to the reasons why . results patient annotation requests the pods team processed 1 , 669 requests for 1 , 197 patients , most in 2014 and 2015 ( data supplement )  . 
multiple requests for the same patient may have been due to additional alterations requested for annotation , different clinicians requesting annotation of the same molecular report , or the same molecular report requested for different venues in which the patient was evaluated ( eg , clinic visit v treatment planning conference )  . 
clinician - initiated requests originated from treating physicians and team members for point - of - care decisions on the basis of molecular testing or from clinical trial teams screening for patients to enroll in genotype - matched trials . fifty - six physician teams initiated requests for 724 patients and ranged from one to 176 per team , with two requests being the median ( data supplement )  . 
because not all aspects of protein function can possibly be determined , the functional significance is likely benign there is peer - reviewed published literature showing that the alteration has an inactivating or inferred inactivating effect on an oncogene . there is peer - reviewed published literature showing that the alteration has an activating or inferred activating effect on a tumor suppressor that enhances its function as a tumor suppressor overall , 4 , 084 variant - level annotations were provided for 2 , 254 unique alterations . 
genes most commonly annotated as part of a full panel request included tp53 , kras , and pik3ca , representing the three most commonly mutated genes in the genome ( fig 1c )  . 
the percentage of requests is shown for ( a ) each indicated tumor type ( top 25 ) and ( b ) annotation type ( full panel or select alterations )  . 
genes with 20 or more annotations are shown . actionable genes and alterations a gene is actionable if there are clinically available therapies that directly or indirectly targe alterations in the gene and / or there are clinical trials selecting for alterations in the gene . of the 4 , 084 annotations , 3 , 166 ( 78% ) were within a gene defined as actionable at the time of annotation ( fig 2a ; data supplement )  . 
in 2015 , annotation reports evolved to contain an actionable variant call describing the alterations functional and therapeutic significance , with classification into four broad categories actionable ( further subcategorized by source : literature based , inferred , or functional genomics ) , potentially actionable , unknown , and nonactionable ( table 1 ) 9which was provided with 2 , 444 annotations delivered for 669 patients . 
a total of 794 ( 32.5% ) annotations were actionable , 230 ( 9.4% ) were potentially actionable , 725 ( 29.7% ) were unknown , and 697 ( 28.4% ) were not actionable ( fig 2b )  . 
the total number of annotations in 2015 and the subset that was actionable / potentially actionable are shown per the patients tumor type ( fig 2e and data supplement , respectively )  . 
the actionability of kras has been controversial , particularly in colorectal cancer.14 - 16 when excluding kras as actionable , most actionable annotations were provided for breast cancer patients ( n = 90 ; data supplement )  . clinical utility of annotations we then asked whether physicians acted more often on alterations with evidence of actionability ( data supplement )  . 
we manually recorded clinical follow - up data by accessing the ehrs of 539 patients requested for annotation by clinicians or for treatment planning conferences . four patients were excluded : two had mutations that were actionable only for resistance to therapy , and two because of insufficient follow - up since physician notification . 
for the remaining 535 patients , variant annotation data were filtered , such that each patient in the data set is represented by a single alteration ( fig 3a )  . 
the fraction of patients represented by the highest variant call ( yellow column ) and the corresponding fraction of patients with that call enrolled in a trial ( gray column )  . 
the fraction of patients represented by the highest variant call ( yellow column ) and the corresponding fraction of patients with that call enrolled in a trial ( gray column )  . 
of patients with variant call enrolled in a trial ( % ) yes : literature based 214 ( 40.0 ) 49 ( 22.9 ) yes : inferred 54 ( 10.1 ) 26 ( 48.1 ) potentially 65 ( 12.1 ) 17 ( 26.2 ) unknown 136 ( 25.4 ) 16 ( 11.8 ) no ( nonactionable ) 66 ( 12.3 ) 2 ( 3 ) p < .001 actionable / potentially actionable alterations unknown alterations nonactionable alterations actionable variant classification total no . 
alterations of 214 patients ( 40% ) were classified into the yes : literature based category ; 54 ( 10.1% ) were classified into the yes : inferred category ; 65 ( 12.1% ) were classified into the potentially category ; 136 ( 25.4% ) were classified into the unknown category ; and 66 ( 12.3% ) were classified into the no ( nonactionable ) category ( fig 3a , yellow column )  . 
patients with actionable alterations in pten ( n = 20 ) , pik3ca ( n = 11 ) , and erbb2 ( n = 10 ) most frequently enrolled in a trial ( fig 4 ) , paralleling the data showing a large number of actionable / potentially actionable annotations delivered for pik3ca and pten ( fig 2d ; data supplement )  . to understand why physicians may not have acted on potentially actionable alterations , we introduced a web - based survey in 2015 to accompany physician - initiated requests . 
a combination of survey responses and manual review revealed that 26.8% of annotations ( 59 of 221 ) led to a genotypematched trial ( fig 3c , gray column )  . 
the latter had another well - characterized oncogenic variant ( idh1 r132c , akt1 e17k , or fgf3 and fgf4 amplifications ) or an alteration clearly inferable as actionable ( early truncating ptch1 mutation ) , where either decision support was not needed or was previously supplied outside the survey group . finally , three patients ( 3.3% ) elected to be treated elsewhere . among 161 patients with variants classified as yes : literature based and yes : inferred , there were fig 4 . 
reasons patients did not enroll in genotype - matched trials after precision oncology decision support annotations , as stated by the survey respondents patients ( n = 161 ) patients with yes : literature based and yes : inferred variants ( n = 42 ) patients with variants annotated as potentially actionable ( n = 29 ) patients with variants annotated as unknown and no for actionability ( n = 90 ) 71 ( 44.1 ) 5 ( 11.9 ) 9 ( 31.0 ) 57 ( 63.3 ) reasons patient did not enroll in trial physician stated annotation does not support trial enrollment , no . 
reasons included another alteration pursued ( two patients ) , the patient was responding to current therapy ( six patients ) , and the patient elected treatment elsewhere ( nine patients )  . 
other reasons included nongenotype - matched treatment options pursued ( five patients ) and ineligibility ( 11 patients )  . in five instances , physicians indicated that the annotation did not support trial enrollment , which we investigated further . 
 toxicity - related deaths in patients treated with targeted therapies.17 - 20 however , few biomarkers have an indication for treatment with a food and drug administrationapproved drug specific to the patients tumor type , 21 - 27 and a limited number of patients with potentially actionable alterations receive genotype - matched therapies in experimental contexts.3 - 7 one contributing factor may be a lack of decision support , as suggested by the cancer genome evaluation committee , which found that physicians are often overwhelmed by data of uncertain significance and that sound guidelines are essential for determining clinical action.28 moreover , we previously reported modest differences in trial enrollment between patients with or without potentially actionable alterations.3 assessing a new population of patients where decision support was provided , we observed that physicians acted more often when the function of the alteration was known . the necessity for real - time decision support is clear from the large volume of requests received from numerous physicians ( data supplement ) treating patients with diverse tumor types for alterations in a range of genes . 
however , bias likely exists toward physicians leading targeted therapy trials and for genes targeted by those therapies . the pods team is frequently asked to provide an annotation for sequencing reports from commercial vendors that produce end - to - end reports , some already containing alteration - level annotations . distinguishing factors of pods reports are a clear call of functional effect9 ( eg , activating , inactivating , unknown ) , a range of variant - level actionability categories on the basis of experimental evidence , and inclusion of all md anderson genotype - matched clinical trials in current reports . previous studies reported high rates of alterations in actionable genes , 4 , 29 - 33 and we provided an annotation in at least one actionable gene for 97% of patients in our cohort . 
using the target ( tumor alterations relevant for genomics - driven therapy ) database and phial ( precision heuristics for interpreting the alteration landscape ) algorithm to rank alterations followed by manual annotation for only selected patients , a study showed that 90% of patients have clinically relevant alterations.34 conversely , we found that 66% of patients annotated have at least one potentially actionable alteration on the basis of manual curation of all aberrations . 
potential differences between the studies include ( 1 ) the inclusion of potentially actionable diagnostic or prognostic alterations by van allen et al34 and not in our study ; ( 2 ) we provided annotations for only requested alterations , and few annotation requests were obtained for well - established alterations ( eg , braf v600e ) ; and ( 3 ) the difference in the number of patients assessed by manual curation in the two studies . among all annotations with an actionable variant call , only 32.5% were classified as actionable , with another 9.4% classified as potentially actionable . even within genes that are considered actionable , 47.4% of the annotations either had no evidence to support actionability or were not actionable . moreover , 58% of the genomic alterations annotated and evaluable for frequency have not been reported in the cosmic database ( data supplement )  . 
these data highlight the need to define actionability at the variant , rather than gene , level . to determine whether physicians acted according to the evidence presented in the pods reports , we followed 535 patients . 
thus , physicians more often act on alterations when sufficient evidence is provided that they may be driver events . the most often - cited reason that patients did not enroll in genotype - matched trials was that the annotation did not support trial enrollment . 
mills shaw , john mendelsohn , funda meric - bernstam provision of study materials or patients : sarina piha - paul , vivek subbiah , david hong , kenna r . 
mills shaw , funda meric - bernstam data analysis and interpretation : amber johnson , yekaterinab . khotskaya , lauren brusco , jia zeng , vijakumar holla , ann m . bailey , md abu shufean , russell broaddus , gordon b . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . jia zeng stock and other ownership interests : amgen , mckesson , mylan , adamas pharmaceuticals amber johnson no relationship to disclose yekaterina b . 
s anchez no relationship to disclose md abu shufean no relationship to disclose sarina piha - paul consulting or advisory role : genentech research funding : glaxosmithkline , xuanzhu , puma biotechnology , novartis , merck sharp & dohme , curis , principa biopharma , biomarin , helix biopharma , bayer , abbvie , incyte , five prime therapeutics , cerulean pharma , medimmune , medivation vivek subbiah research funding : novartis , glaxosmithkline , nanocarrier , northwest biotherapeutics , roche / genentech , bergpharma , bayer , incyte , fujifilm , pharmamar , d3 , pfizer , amgen , abbvie , multivir , bluprint medicines travel , accommodations , expenses : novartis , pharmamar , fujifilm david hong stock and other ownership interests : molecularmatch , oncorena honoraria : adaptimmune , baxter , merrimack , bayer consulting or advisory role : baxter , bayer research funding : novartis , genentech , eisai , astrazeneca , pfizer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly travel , accommodations , expenses : loxo , mirna therapeutics other relationship : oncorena mark routbort no relationship to disclose russell broaddus no relationship to disclose kenna r . 
stockley tl , oza am , berman hk , et al : molecular profiling of advanced solid tumors and patient outcomes with genotype - matched clinical trials : the princess margaret impact / compact trial . 
j pers med 3 : 306 - 325 , 2013 johnson a , zeng j , bailey am , et al : the right drugs at the right time for the right patient : the md anderson precision oncology decision support platfordrug discov today 20 : 1433 - 1438 , 2015 10 . 
forsman j , anani n , eghdam a , et al : integrated information visualization to support decision making for use of antibiotics in intensive care : design and usability evaluation . 
rinehart j , adjei aa , lorusso pm , et al : multicenter phase ii study of the oral mek inhibitor , ci - 1040 , in patients with advanced non - small - cell lung , breast , colon , and pancreatic cancer . 
bennouna j , lang i , valladares - ayerbes m , et al : a phase ii , open - label , randomised study to assess the efficacy and safety of the mek1 / 2 inhibitor azd6244 ( arry - 142886 ) versus capecitabine monotherapy in patients with colorectal cancer who have failed one or two prior chemotherapeutic regimens . 
schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
van allen em , wagle n , stojanov p , et al : whole - exome sequencing and clinical interpretation of formalin - fixed , paraffin - embedded tumor samples to guide precision cancer medicine . 
this , in turn , leads to a profound defect in homology - mediated dna repair and inappropriate use of error - prone repair pathways , which result in gross genomic instability that contributes to tumorigenesis.1 , 2 this dna - repair defect in brca1 / 2 - mutant cancers renders them exquisitely vulnerable to certain kinds of dna damage , including those caused by poly ( adp - ribose ) polymerase ( parp ) inhibitors and certain classic chemotherapy agents , including platinum.3 the vulnerabilities of brca1 / 2 - mutant cancers to these agents have been translated successfully into treatment approaches . 
parp inhibitors are now approved by the us food and drug administration for treatment of brca1 / 2 mutant ovarian cancers , 4 and data are accumulating that suggest that parp inhibitors are likely active in brca1 / 2 - mutant cancer regardless of the tissue of origparp inhibitors are thought to be toxic to brca1 / 2 - mutant cancers not only because of their catalytic inhibition of parp but by their ability to trap parp - 1 enzyme on dna.5 , 6 the most potent parp inhibitors that induce cell death in brca1 / 2 - mutant cells are those that most efficiently trap parp protein on dna , creating a bulky protein dna adduct.7 in this sense , parp inhibitors work similarly to topoisomerase inhibitors , which trap topoisomerases to create a bulky protein dna adduct . 
other dna - damaging agents including platinum , mitomycin c , and topoisomerase inhibitors , that also induce dna adducts , are also effective in the treatment of brca1 / 2 - mutant cancers in animal models and clinically . given the widespread use of germline and tumor sequencing , and recent us food and drug administration approval of parp inhibitors , more patients who have tumors with pathogenic brca1 / 2 mutations are being treated with parp inhibitors and / or platinum agents . 
one important mechanism of acquired resistance is reversion mutations in brca1 or brca2 that partly restore wild - type gene function.8 , 9 the three reports10 - 12 of reversion mutations in brca2 in breast and prostate cancers that accompany this editorial highlight the importance and increasing awareness of this mechanism of resistance . 
the presence of reversion mutations in brca1 / 2 also reveals some insights about the role of brca1 / 2 function in tumorigenesis and chemosensitivity . most pathogenic mutations in brca1 and brca2 are small insertion / deletions that result in a frameshia frameshift will introduce a premature stop codon , which leads to a truncated , nonfunctional protein product . 
often , frameshift mutations lead to effective null mutations , because rna transcripts harboring premature stop codons can be recognized and degraded by the nonsense - mediated decay pathway.13 reversion mutations are secondary mutations , often small deletions , in a mutant brca1 / 2 allele that convert the initial frameshift mutation into an in - frame internal deletion that still produces a partly functional protein product . 
 complex rearrangements or abnormal use of alternative start sites that bypass the frameshift mutation may also occur.14 rarely , there is full reversion of the pathogenic mutation with restoration of the full wild - type sequence , as seen in the article by banda et al.10 reversion mutations can occur in the setting of either germline or somatic brca1 / 2 mutations , as demonstrated by carneiro et al , 12 and can lead to acquired resistance not only to parp inhibitors but to other classes of dna - damaging agents , such as platinum11 . intriguingly , the mechanism underlying many reversion mutations is inappropriate use of the nonhomologous end - joining pathway , resulting in small deletions , as seen by presence of microhomology at junction sequences.15 longer deletions associated with single - strand annealing may also be present but more difficult to detect . 
it is possible that reversion mutations may already be present in a small population of cells , especially if there is high tumor burden as seen , for example , in ovarian cancer , and are simply selected with ongoing treatment . reversion mutations can be difficult to detect by standard sequencing methods . 
large deletions may be completely missed by short - read sequencing , and even small deletions have to be carefully curated to determine in which allele they originate , and the effect on the final reading frame . 
some full reversions to wild - type sequence may only be detected by careful analysis of tumor purity and mutant allele frequencies in serial samples over time , as demonstrated by banda et al.10 heterogeneity of reversion mutations may also hinder detection . 
analysis of circulating - cell free dna , such as reported by cheng et al11 and carneiro et al , 12 can detect multiple reversion mutations simultaneously at the time of clinical resistance to parp inhibitors or platinum , each restoring the reading frame and arising from a different small tumor - cell population.16 it is possible that only a fraction of reversion mutations in brca1 / 2 are being identified by current sequencing methods . 
new technologies , such as long - read sequencing , and higher depth sequencing may allow more robust detection of reversion mutations and better define their frequency . the selection for reversion mutations in brca1 / 2 under certain treatments does give us some insights into the biology of brca1 . 
 the induction of reversion mutations by platinum is clear genetic evidence that this agent acts on the dna - repair defect associated with brca1 / 2 loss and exerts direct selection pressure to restore brca1 / 2 function . 
this finding also suggests that perhaps , in general , dna - damaging chemotherapies function not as gross metabolic poisons but as targeted therapies for cancers with underlying defects in dna repair and / or checkpoint control . 
if this is true , we may need to reconsider how to optimally dose and schedule platinum and other chemotherapy agents , especially in the setting of cancers with underlying dna - repair defects . the presence of reversion mutations demonstrates that loss of brca1 or brca2 function and the associated dna - repair defect is only required for initiation of tumorigenesis and is not required for maintenance of the cancer phenotype . 
 this feature can be labeled tumor - suppressor tolerance to place it in contrast to oncogene addiction . tumor - suppressor tolerance may operate in cancers that have underlying mutations in genes critical for genomic stability . 
loss of tumor - suppressor function of these genes may only be required for initial tumorigenesis ; once the tumor is established , there may be selection pressure to restore the tumor - suppressor function and reestablish dna - repair function . 
in brca1 - mutant cancers , resistance to parp inhibitors can occur not only by reversion mutations that directly restore brca1 function but also by compensating mutations in other genes such as 53bp1 and its downstream factors such as rif1 , ptip and rev7 , which also can restore homology mediated repair pathways independent of functional brca1.21 - 25 similarly , loss of ptip and chd4 may allow brca2 - mutant cells to reestablish replication fork stability and become resistant to cisplatin and parp inhibitors.26 these findings suggest that to better predict sensitivity to parp inhibitors and platinum , we will need to develop assays capable of distinguishing a cancer with ongoing genomic instability from a cancer with just a history of genomic instability followed by functional reversion of a dna - repair defect . with increasing use of parp inhibitors and platinum for targeted therapy of brca1 / 2 - mutant cancers , we will likely see increased incidence of acquired resistance that exploits tumor - suppressor tolerance and restores brca1 / 2 function . 
it is possible that some hypomorphic alleles of brca1 and brca2 that arise by reversion mutation may still have some targetable vulnerability.27 alternatively , parp inhibitors , or other dna - damaging agents such as platinum , will need to be combined with other drugs that target a different vulnerability in these cancers . 
carneiro b , et al : acquired resistance to the parp inhibitor olaparib in brca2 - associated prostate cancer due to biallelic brca2 reversion mutations restoring both germline and somatic loss of function mutations . 
perrin - vidoz l , sinilnikova om , stoppa - lyonnet d , et al : the nonsense - mediated mrna decay pathway triggers degradation of most brca1 mrnas bearing premature termination codons . 
quigley d , alumkal jj , wyatt aw , et al : analysis of circulating cell - free dna identifies multiclonal heterogeneity of brca2 reversion mutations associated with resistance to parp inhibitors . 
kondrashova o , nguyen m , shield - artin k , et al : secondary somatic mutations restoring rad51c and rad51d associated with acquired resistance to the parp inhibitor rucaparib in high - grade ovarian carcinoma . 
escribano - daz c , orthwein a , fradet - turcotte a , et al : a cell cycle - dependent regulatory circuit composed of 53bp1 - rif1 and brca1 - ctip controls dna repair pathway choice . 
bouwman p , aly a , escandell jm , et al : 53bp1 loss rescues brca1 deficiency and is associated with triple - negative and brca - mutated breast cancers . 
chapman jr , barral p , vannier jb , et al : rif1 is essential for 53bp1 - dependent nonhomologous end joining and suppression of dna double - strand break resection . 
 duality of purpose : participant and parent understanding of the purpose of genomic tumor profiling research among children and young adults with solid tumors purpose increasing use of genomic tumor profiling may blur the line between research and clinical care . 
we aimed to describe perspectives of research participants about the purpose of genomic tumor profiling research in pediatric oncology . methods we surveyed 45 participants ( response rate , 85% ) in a pilot study of genomic profiling in pediatric solid tumors at four academic cancer centers after the return of sequencing results . 
we defined understanding according to a one - item ( basic ) definition ( recognition that the primary purpose was not to improve the patients treatment ) and a four - item ( comprehensive ) definition ( primary purpose was not to improve patients treatment ; primary purpose was to improve treatment of future patients ; there may not be direct medical benefit ; most likely result of participation was not increased likelihood of cure )  . results sixty - eight percent of respondents ( 30 of 44 respondents ) demonstrated basic understanding of the study purpose ; 55% ( 24 of 44 respondents ) demonstrated comprehensive understanding . 
ninety - three percent of respondents who believed the primary purpose was to improve the patients care simultaneously stated that the research also aimed to benefit future patients . conclusion most participants in pediatric tumor profiling research understand that the primary goal of this research is to improve care for future patients , but many express dual goals when they participate in sequencing research . 
2019 by american society of clinical oncology introduction parents of children with cancer1 , 2 and adults with cancer3 - 5 often fail to understand the purpose of clinical trials in which they participate . 
understanding the distinction between the goals of research and clinical care is of particular importance in early - phase oncology trials , in which response rates approximate 10%.6 , 7 up to 60% of research participants demonstrate evidence of therapeutic misconception , 3 , 4 , 8 , 9 the belief that the primary purpose of research is therapeutic in nature rather than acquisition of generalizable knowledge.10 , 11 the precision medicine era invites new exploration of these findings . 
 among adults16 , 17 and children.17 - 20 although advances in targeted therapeutics generate great excitement , they may also blur the line between research and clinical care.21 , 22 young adult patients and parents of children with cancer have high hopes / expectations for tumor sequencing , 23 , 24 though only a minority experience clinical benefit.25 - 29 this mirrors findings among adult patients with cancer30 - 33 and highlights the need for a deeper understanding of the tumor profiling consent process . 
furthermore , many participants simultaneously identified dual purposes for genomic tumor profiling research in pediatric oncology . relevance consenting clinicians should query and explore participant goals during presequencing counseling to identify both ( 1 ) those who do not recognize that the primary purpose of research sequencing is to generate knowledge to help future patients and ( 2 ) those who report dual purposes for this research . 
additional work is necessary to better understand the perspectives and motivations of those who express this duality and to develop and test interventions to improve equitable understanding of the purpose of genomic tumor profiling research in pediatric oncology . methods we surveyed consenting participants in the icat ( individualized cancer therapy ) pilot study of genomic profiling in children with relapsed , recurrent , and high - risk solid tumors ( clinicaltrials.gov identifier : nct01853345 ) .25 participants were approached at dana - farber / boston childrens cancer and blood disorders center ( boston , ma ) , university of california at san francisco ( san francisco , ca ) , columbia university medical center ( new york , ny ) , and childrens national medical center ( washington , dc )  . 
the study was approved by the institutional review board of all participating institutions . individualized cancer therapy study icat study procedures have been reported previously.25 all patients receiving care at participating institutions were eligible for enrollment if they were age 30 years or younger at enrollment and had a recurrent , refractory , or high - risk ( expected likelihood of cure < 25% ) extracranial solid tumor with sufficient tumor for submission . 
the study consent document described the purpose of the study as follows : to determine how often the panel of experts can [ use tumor sequencing results to ] make an individual treatment recommendation and to use this information to help future patients with cancer . 
 consent discussions were not standardized , nor were data collected on the content of these discussions . enrolled participants underwent tumor profiling via targeted next - generation sequencing and copy number assessment or a sequenom assay . 
survey items for assessment of participant understanding of the purpose of genomic profiling research in pediatric oncology question stem answer choice agree unsure * disagree * the main reason this study was done was to improve the treatment of myself / my child . the main reason this study was done was to improve the treatment of future patients with cancer . there may not have been direct medical benefit to me / my child from participation . what of the following did you think was most likely to happen because of your participation in this research study ? agree * unsure * disagree agree * unsure * disagree i / my child would have a better chance of being cured . doing this testing would give me peace of mind . * doctors would be better able to find cures for future patients . * doctors would be able to learn more about my / my childs cancer . * i / my child would have a greater number of treatment options . * nothing was likely to happen as a result of this research . * i would learn about my / my childs genes . * i would learn about my familys genes . * other * alterations for which a matched targeted therapy was available via clinical trial or us food and drug administrationapproved medication ; the recommendation described actionable alteration ( s ) found and strength of evidence for each treatment recommendation . study population icat participants were offered a self - administered written survey after return of study results to the patients oncologist . 
surveys were offered in english to the consenting individual : the patient if he / she was age 18 years or older at enrollment , or the patients parent / guardian if the patient was younger than age 18 years at enrollment . 
 surveys were not offered if the patient died between the time of enrollment and approach by the study team ( n = 41 ) ; the patient / parent did not understand english sufficiently to complete the survey ( n = 3 ) ; the patient / parent declined additional contact from study investigators after enrollment ( n = 0 ) ; and / or the oncologist did not permit approach by the study team ( n = 4 )  . survey methods survey procedures have been reported previously.24 surveys consisted of 103 items and included scales that addressed participant understanding of the purpose of clinical research , 34 genetic knowledge , 35 and the short form - 36 general health perceptions question . 
secondary outcomes were participant - level predictors of understanding ( demographic characteristics , genetic knowledge , experience with genetics , clinical status , receipt of icat recommendation / targeted therapy )  . 
participants were enrolled between september 2012 and november 2013 ; surveys were administered between september 2014 and july 2015 . participant understanding of the purpose of research sequencing we assessed participant understanding with four independent items ( table 1 )  . 
three items were adapted from the quality of informed consent measurea validated measure to assess understanding of the purpose of oncology clinical trials , 34 by adult patients with cancer and further validated in parents of children with cancer1 ; answer choices were agree , unsure , and disagree.34 the fourth item offered respondents multiple choices about their perceived most likely result of study participation . participants were asked how well they understood conversation ( s ) they had with the doctor about the icat study and the testing involved in it , and responses were collected on a 5 - point likert scale ( responses of extremely well , well , moderately , poorly , extremely poorly )  . 
 to measure patient knowledge about genetics / genomics.24 , 36 , 37 respondents were asked if they had regular exposure to genetics and / or genetic information through their job and if they had ever attended any classes / lectures on genes / genetics . statistical methods understanding of the purpose of the study was defined in two ways . 
 comprehensive understanding was defined as an understanding of all four of the following : ( 1 ) the primary purpose was not to improve their / their childs treatment ; ( 2 ) the primary purpose was to improve treatment of future patients with cancer ; ( 3 ) there may not have been direct medical benefit to them / their child ; and ( 4 ) the most likely result of participation was not an increased likelihood of cure for themselves / their child . 
for example , if a participant identified that the primary purpose of the study was not to improve her childs treatment , he or she demonstrated basic understanding of the studys purpose . 
to be as inclusive as possible , and because of the complexity and uncertainty inherent in tumor profiling research , responses of unsure to any of the first three items were coded as consistent with understanding . 
for the fourth item , only responses that the most likely result of participation in the study was cure were coded as inconsistent with understanding ; all other responses , including answers of other , were coded as understanding . 
missing responses to any of the four understanding items were excluded from analysis of comprehensive understanding ; only those that were missing the first item were excluded from analysis of basic understanding . self - report of degree of understanding of the consent conversation ( s ) was dichotomized as well or extremely well ( coded as good self reported understanding ) versus all others . 
those who answered extremely true or very true to the item about how helpful participation was to them / their child were coded as feeling the study to have been helpful , and those who answered with the other answer choices were coded as feeling it was not . experience with genetics was defined as an affirmative response to questions of regular exposure to genetics or experience with genetics / genetic information and / or enrollment in any classes / lectures on genes or genetics . 
high genetic knowledge was defined as correct answers of all four items from the gki.35 those who answered fewer than four gki items correctly were coded as having low genetic knowledge . respondent demographics and clinical characteristics and understanding of results and the purpose of testing were evaluated using descriptive statistics . 
item nonresponse was less than 10% , and participants with nonresponse to an item were excluded from analyses of that ite all analyses were performed using stata , version 13.1 ( statacorp , college station , tx )  . results respondent characteristics of 101 participants who underwent profiling on the icat study , 53 were eligible for survey administration . 
characteristics of survey respondents are listed in table 2 for the overall cohort and are subdivided into patient ( n = 11 ; 24% ) and parent / guardian ( n = 34 ; 76% ) respondents . 
participant and patient demographics , overall and separately , according to whether the survey was completed by the patients parent / guardian or by the patient himself or herself overall ( n = 45 ) patient respondents ( n = 11 ) no . 
participant and patient demographics , overall and separately , according to whether the survey was completed by the patients parent / guardian or by the patient himself or herself ( continued ) overall ( n = 45 ) patient respondents ( n = 11 ) no . 
sixty - eight percent of respondents ( 30 of 44 respondents ) recognized that the primary reason the study was performed was not to improve the treatment of them / their child , which met our definition of basic understanding of the purpose of the study . 
no significant differences were seen according to respondent age , sex , or race / ethnicity ; according to self - reported health status or likelihood of cure , receipt of an icat treatment recommendation or matched targeted therapy ; or according to participant - identified understanding of what they were told about the study . 
 results were similar when responses of unsure were excluded from analysis ( appendix fig a1 )  . similar results were seen with understanding defined by the composite four - item scale . 
comprehensive understanding of the purpose of genomic profiling research was seen with statistically greater frequency among those with at least a college education ( 73% v 28% ; p = .01 ) and with higher genetic knowledge ( 71% v 23% ; p = .01 ) and among white / non - hispanic respondents ( 68% v 37% ; p = .07 ) , though the comparison by race / ethnicity was not statistically significant . 
similarly , no statistical difference in understanding was seen according to receipt of an icat treatment recommendation or matched targeted therapy or according to whether the respondent reported a good understanding of what they were told about the study / testing . 
among those who mistakenly identified the primary purpose as improvement of their / their childs treatment , 93% ( 13 of 14 respondents ) simultaneously recognized that it aimed to benefit future patients . 
twenty - eight percent ( 12 of 43 respondents ) of those who identified that the primary purpose was to benefit future patients also reported that the primary purpose was to improve their / their childs treatment . discussion in this multi - institutional study that examined the role of molecular profiling of pediatric solid tumors , nearly all participants recognized that the primary purpose was to benefit future patients . 
 however , approximately one third of respondents believed that the primary purpose of the trial was to improve their / their childs treatment , and nearly one fifth expected participation to impart a greater chance of cure . although these responses raise concerns about the quality of informed consent for tumor fig 1 . 
relationship between participant demographics and understanding of purpose of research tumor profiling ( continued ) helpfulness of participating in the study not helpful to myself / my child helpful note . 
 ( % ) 17 ( 71 ) 7 ( 35 ) sequencing , they must be considered in context of a complex technology with an evolving role in clinical care . 
this duality is echoed by the american society of clinical oncology , which states that early - phase clinical trials in oncology simultaneously generate new knowledge and provide participants the opportunity for psychological and clinical benefit.22 , 38 oncologists often balance dual goals for patients by recommending enrollment in a phase i trial while hoping for patient benefit or by simultaneously providing palliative and cancer - directed ( ie , blended ) care.39 in the era of precision cancer medicine , it is reasonable that patients / families might perceive such dualities as well . this duality has important clinical implications . 
however , an initial approach could be to discuss the primary goal of the study as gaining new knowledge to help future patients , followed by an acknowledgment , tempered with realistic expectations , that many patients / parentsand many clinicianshold hope that the child will also benefit from participation . 
in the case of next - generation sequencing , for example , it is important to note that the number of patients who experience direct benefit via receipt of a targeted therapy is quite low , likely in the range of 3% to 19%.25 - 29 our results also underscore the importance of hope among patients and parents of children with cancer in clinical and research settings.40 - 42 hopeful thinking may partially explain why participants who felt the study had helped them / their child and those who were receiving cancer directed therapy at the time of survey completion less frequently demonstrated understanding of the purpose of research tumor sequencing . in this cohort , understanding was observed more frequently in those with at least a college education and those with good genetic knowledge . 
 this finding , also reported elsewhere , 23 is not surprising , given the complexity of these concepts and the expected link between understanding and health literacy / numeracy.43 understanding also varied according to race / ethnicity , consistent with similar work in the pediatric oncology phase i literature , 2 although the difference did not reach statistical significance in this pilot study . 
these disparities underscore the importance of attention to the needs of vulnerable populations when they are counseled about genomic results ; however , the optimal mechanism for such counseling remains unclear.44 prior work in pediatric oncology has identified that refinement of the consent process may improve understanding , 45 but optimal strategies to adequately convey the complexities of tumor sequencing and support fully informed consent for participation in sequencing research are not yet known . 
a follow - up study is in development to examine the benefit of such an intervention for those who demonstrate less than comprehensive understanding , as defined in this cohort . 
patients / parents may have better understood the purpose of profiling closer to the time of consent , but understanding did not vary statistically with time to survey completion in this cohort . 
many study participants died before surveys could be administered ; however , demographic and clinical characteristics of respondents mirrored those of the overall cohort.25 finally , participants were enrolled at four large academic centers , so results may not be generalizable to those from smaller and / or community centers . 
this could , for example , explain the unexpectedly high genetic knowledge and experience seen in this cohort . although some participants misidentified the primary goal of tumor profiling research as therapeutic in nature , participant views are nuanced . 
dubois honoraria : loxo consulting or advisory role : loxo research funding : millennium ( inst ) , merck ( inst ) , novartis ( inst ) , roche ( inst ) , genentech ( inst ) , lilly ( inst ) , curis ( inst ) , loxo ( inst ) travel , accommodations , expenses : loxo , roche , genentech julia glade - bender research funding : bristol - myers squibb ( inst ) , pfizer ( inst ) , novartis ( inst ) , ignyta ( inst ) , amgen ( inst ) , celgene ( inst ) , eisai ( inst ) , lilly ( inst ) , merck ( inst ) travel , accommodations , expenses : novartis , amgen , merck aerang kim no relationship to disclose brian d . 
weinfurt kp , seils dm , lin l , et al : research participants high expectations of benefit in earlyphase oncology trials : are we asking the right question ? j clin oncol 30 : 4396 - 4400 , 2012 6 . 
italiano a , massard c , bahleda r , et al : treatment outcome and survival in participants of phase i oncology trials carried out from 2003 to 2006 at institut gustave roussy . 
druker bj , sawyers cl , kantarjian h , et al : activity of a specific inhibitor of the bcr - abl tyrosine kinase in the blast crisis of chronic myeloid leukemia and acute lymphoblastic leukemia with the philadelphia chromosome . 
kantarjian hm , shah np , cortes je , et al : dasatinib or imatinib in newly diagnosed chronicphase chronic myeloid leukemia : 2 - year follow - up from a randomized phase 3 trial ( dasision )  . 
wagle n , grabiner bc , van allen em , et al : activating mtor mutations in a patient with an extraordinary response on a phase i trial of everolimus and pazopanib . 
kushner bh , cheung nv , modak s , et al : a phase i / ib trial targeting the pi3k / akt pathway using perifosine : long - term progression - free survival of patients with resistant neuroblastoma . 
laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , open - label , phase 1 / 2 study . 
weber js , levit la , adamson pc , et al : reaffirming and clarifying the american society of clinical oncologys policy statement on the critical role of phase i trials in cancer research and treatment . 
oberg ja , ruiz j , ali - shaw t , et al : whole - genome and whole - exome sequencing in pediatric oncology : an assessment of parent and young adult patient knowledge , attitudes , and expectations . 
marron jm , dubois sg , glade bender j , et al : patient / parent perspectives on genomic tumor profiling of pediatric solid tumors : the individualized cancer therapy ( icat ) experience . 
harris mh , dubois sg , glade bender jl , et al : multicenter feasibility study of tumor molecular profiling to inform therapeutic decisions in advanced pediatric solid tumors : the individualized cancer therapy ( icat ) study . 
chang w , brohl as , patidar r , et al : multidimensional clinomics for precision therapy of children and adolescent young adults with relapsed and refractory cancer : a report from the center for cancer research . 
harttrampf ac , lacroix l , deloger m , et al : molecular screening for cancer treatment optimization ( moscato - 01 ) in pediatric patients : a single - institutional prospective molecular stratification trial . 
miller fa , hayeems rz , bytautas jp , et al : testing personalized medicine : patient and physician expectations of next - generation genomic sequencing in late - stage cancer care . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental findings : results from the canseq study . 
carere da , couper mp , crawford sd , et al : design , methods , and participant characteristics of the impact of personal genomics ( pgen ) study , a prospective cohort study of direct - to - consumer personal genomic testing customers . 
weber js , levit la , adamson pc , et al : american society of clinical oncology policy statement update : the critical role of phase i trials in cancer research and treatment . 
ferrell br , temel js , temin s , et al : integration of palliative care into standard oncology care : american society of clinical oncology clinical practice guideline update . 
sensitivity analyses for the relationship between participant demographics and understanding of the purpose of research tumor profiling basic understanding ( n = 33 ) comprehensive understanding ( n = 26 ) variable survey respondent characteristic no . 
 ( % ) respondent attitudes about icat study understanding of icat information poor self - reported understanding good self - reported understanding helpfulness of participating in icat study not helpful to myself / my child helpful basic understanding ( n = 33 ) comprehensive understanding ( n = 26 ) 10 ( 77 ) 9 ( 45 ) 11 ( 69 ) 8 ( 47 ) 8 ( 80 ) 8 ( 50 ) 10 ( 77 ) 6 ( 46 ) note . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction as our knowledge of hereditary cancer risk has testing of cancer preevolved , multigene panel disposition genes has become an important component of patient care . 
the national comprehensive cancer network provides gene - specic recommendations for changes in medical management on the basis of the identication of pathogenic variants.1 to this end , accurate and denitive variant classication is a critical component of clinical genetic testing . 
the american college of medical genetics and genomics ( acmg ) and the association for molecular pathology ( amp ) provide guidelines for clinical variant classication2 ; however , there is often insufcient evidence to support a denitive classication of pathogenic or benign when a variant is rst detected . 
as a result , testing laboratories may vary in their clinical terpretation of acmg / amp guidelines for hereditary cancer genetic testing and , ultimately , in their variant classications.3 - 6 with the increased use of multigene panels , number of variants of uncertain signicance ( vuss ) detected has also increased.7 , 8 in addition to a larger number of genes , many cancer predisposition genes have been more recently incorporated into clinical testing , and there is less evidence available to support variant classication . 
 evolution of cancer gene variant reclassication context key objective with the increasing use of hereditary cancer genetic testing and introduction of multigene panels , robust and accurate methods for variant re / classication of cancer predisposition genes are of utmost importance . 
laboratory - developed methods were the most common lines of evidence used in variant reclassication , with pheno analysis ( a clinical history weighting algorithm ) being used in approximately 40% of cases . relevance many tools traditionally used for variant re / classication are not informative for rare variants ; however , rare variants collectively affect millions of patients . 
this was followed by testing for lynch syndrome ( mlh1 , msh2 , msh6 , and pms2 ) and melanoma - pancreatic cancer syndrome ( cdkn2a ) in 2002 and for familial adenomatous polyposis ( fap ) / attenuated fap / mutyh - associated polyposis ( apc and mutyh ) in 2003 . 
in 2013 , a hereditary cancer multigene panel was introduced , which was analytically validated and described in detail previously.9 the panel included 25 genes : apc , atm , bard1 , bmpr1a , brca1 , brca2 , brip1 , cdh1 , cdk4 , cdkn2a ( p16ink4a and p14arf ) , chek2 , epcam , mlh1 , msh2 , msh6 , mutyh , nbn , palb2 , pms2 , pten , rad51c , rad51d , smad4 , stk11 , and tp53 . 
individuals who had single - site or founder mutation testing were reclassication program the reclassication program used by this testing laboratory included a multidisciplinary committee of laboratory directors , genetic counselors , phd - level scientists , and supporting variant specialists . 
variant classication and reclassication followed a stringent , welldocumented protocol as previously described.13 on the basis of acmg / amp guidelines , variants were classied into ve categories of increasing clinical severity : benign ( b ) , likely benign ( lb ) , vus , likely pathogenic ( lp ) , and pathogenic ( p ) .2 , 14 , 15 automated processes proactively monitored and gathered all available evidence to expedite reclassication . 
multiple classication tools could have been used to evaluate the pathogenicity of a variant at the time of original classication and / or if a variant was reclassied , an reclassication ( fig 1 )  . amended report was sent to health care providers for all patients who were carriers of the variant . 
 esterling et al pheno ( n = 56 , 596 ) clinical history weighting algorithm to assess phenotype severity for variant carriers v carriers of pathogenic and benign variants pt / ha ( n = 36 , 314 ) phase testing or haplotype analysis for genes associated with embryonic lethality or severe clinical phenotypes because of homozygosity or compound heterozygosity homozygosity confirmed continuous evidence evaluation threshold reached population frequency ( n = 17 , 664 ) threshold reached allele frequency from exac and gnomad functional or clinical evidence literature ( n = 4 , 509 ) expert review of automated search results and curated repository structure disrupted structural analysis ( n = 850 ) using validated protein structures mco ( n = 12 , 753 ) likelihood of co - occuring pathogenic variants in the same gene or in genes associated with the same hereditary cancer syndrome threshold reached cosegregation in multiple families segregation analysis ( n = 8 , 255 ) published pedigrees and provider communications rna analysis ( n = 610 ) in - house comprehensive rna analysis to directly assess rna splicing effects splicing disrupted splicing analysis ( n = 3 , 148 ) functional data and expert review other ( n = 4 , 598 ) knowledge of similar variants , species conservation in conjunction with structural analysis , additional statistical analysis , and classification / reclassification protocol refinements evidence queuing for review based on variant type and new evidence multiple expert reviews evidence insufficient wait for additional evidence committee discussion variant reclassified amended reports fig 1 . 
phase testing / homozygosity analysis ( pt / ha ) was only applied to genes associated with autosomal dominant cancer risks that may also be associated with embryonic lethality or severe clinical phenotypes in individuals carrying pathogenic variants in the affected gene on different parental chromosomes as a result of either homozygosity or compound heterozygosity . 
common single nucleotide polymorphisms ( snps ) observed in the patient population were used to develop gene - specic haplotypes , which were automatically assigned to determine the variants phase ( ie , in cis or in trans ) , whenever possible . 
mutation co - occurrence ( mco ) analysis was based on an assumption of a low likelihood that an individual will carry two autosomal dominant pathogenic variants that cause an increased risk for the same or a similar cancers.18 mco analysis measured the statistical signicance of a variant co - occurring multiple times with one or more pathogenic variants in the same patient ( in the same gene or in a different gene for the same syndrome )  . 
99.5%. rna splicing analysis and protein structural analysis . assessment of in silico rna splicing predictions was used to initially evaluate the potential effects of a variant on rna splicing.19 published reports of biochemical splicing analysis , which used high - quality data and appropriate controls , were considered for variant classication . 
in some cases where evidence was unavailable or of insufcient quality or detail to be conclusive , quantitative rna splicing analyses were performed in house , using informative snps , to assess potential rna splicing effects resulting from the variant of interest.20 expert protein structural analysis was also used to assess the impact of variants predicted to affect protein structure at the amino acid level . 
jack lee , phd2 precision oncology exploits genomic , immunologic , and other biomarkers to drive discovery , drug development , and clinical care for patients with cancer . precision oncology helps devise individualized treatment strategies and therapies on the basis of a patients specic characteristics , such as genetic information , health history , environmental exposure , and needs and preferences , to guide discovery of effective drugs and treatment interventions . 
because precision oncology research raises so many interesting and challenging clinical and statistical questions that require new approaches to statistical thinking , design , and analysis , it is critical that multidisciplinary teams include clinicians , basic scientists , and statisticians who can collaborate on study design , analysis , and interpretation . statistical methods play an important role in discovering signals and ltering out noises embedded in the rich sources of high - dimensional - omics data , but they must also contend with the complexity of cancer biology and medical conditions . 
for example , the umbrella trial design was used in battle1 ( clinicaltrials.gov identier : nct00409968 ) and i - spy 2 ( clinicaltrials.gov identier : nct01042379 ) 2 trials , and it greatly improved efciency in these phase ii cancer trials , which screened drugs for efcacy signals . 
a basket trial design was used successfully in a trial of vermurafenib3 in multiple non - melanoma cancers with braf v600 mutations ( clinicaltrials.gov identier : nct01524978 )  . master protocols have been developed for the lungmap ( clinicaltrials.gov identier : nct02154490 ) trial4 and nci - match ( clinicaltrials.gov identier : nct02465060 ) trial , among others.5 , 6 in recent years , statisticians have worked closely with oncologists to develop new statistical methods that will provide scientically rigorous answers to research questions and substantially improve the efciency of the drug development process and the feasibility of doing the research . 
for this reason , jco precision oncology has organized this special series of tutorial and review articles on statistical methods for precision oncology that will serve as a bridge between the clinical researcher and statistician communities , will help facilitate the application of new methods , and will stimulate the development of more and better methods to address various needs in precision oncology research . the journal solicited 13 papers from well - known statisticians who are developers of novel statistical methods for precision oncology or are experts in their application . 
some articles introduce and review various methods for developing precision drugs in oncology , and some provide expert opinions on discoveries , precision oncology care , and decision making . cluded here are articles on drug discoveries , earlyphase dose determination , phase ii biomarker - driven trials , phase iii trials , companion and predictive diagnoses , master protocols for basket trials and umbrella trials , selection of estimands for clinical trials , and clinical trials for pediatric cancer . 
the following are brief descriptions of highlights from each article . high - dimensional data have much promise in advancing precision oncology , whereas data on individual biomarkers contribute relatively small amounts of information on complex diseases . 
newly developed statistical tools allow researchers to aggregate pathwaylevel information from multiple relatively weak signals . zhao , chang , and long7 provide a comprehensive review of knowledge - guided statistical supervised and unsupervised learning methods for - omics data . 
the review of recent developments in risk assessment models of clinical outcomes by halabi , li , and luo8 covers a topic that is identifying new prognostic factors and critical building new risk assessment prognostic models for managing patients and decision making . 
in precision oncology , evaluating treatment effects in populations dened by their histology , choosing biomarker - driven clinical trial designs , and planning analyses require additional considerations , depending on the nature and utility of the biomarkers . simon9 gives a historical account of the evolution of trial design in precision oncology and provides a review of new biomarker - driven clinical trial designs that can be used for various purposes , including adaptive validation of companion diagnostic tests for targeted treatments . polley and cheung10 have reviewed the concepts and methodology of early - phase cancer trial designs with a focus on dose nding and treatment screening . 
because most cancer trial designs have been developed for cytotoxic targeted cancer therapies , the authors discussed the relevance of these time - tested design principles in the context of platform trials for targeted cancer therapies . 
yuan , lee , and hilsenbeck11 introduce and review a new class of model - assisted designs to combine the transparency and simplicity of conventional algorithm - based designs with the superiority and rigorousness of novel model - based designs . thall12 reviews two clinical trial designs that help researchers make subgroup - specic decisions and compare each of them to a simpler design that ignores patient heterogeneity . 
these trial designs illustrate the benets of prospectively accounting for treatment - subgroup interactions and show how utilities may be used to quantify riskbenet trade - offs . several articles also discuss newly developed methods that can be used in later - phase trials of drug efcacy and can also be used to identify subgroups dened by predictive biomarkers . 
they then discuss the adaptive enrichment design , which uses subgroup analysis to inform random assignments to various treatments . progress in the areas of genomics , disease pathways , and in clinical and drug discovery is beginning to be felt trials have been translational cancer research . 
the article by kaizer et al14 provides a comprehensive review of basket trial designs in oncology settings and discusses several issues that arise with their design and methods of analysis . hu and dignam15 provide a comprehensive overview of the design elements , types , features , and practical considerations of master protocols for multiagent and / or multihistology master protocol trials . 
polley , korn , and freidlin provide an updated review of commonly used biomarkerbased randomized clinical trial design for a single agent and subpopulation for simultaneous inferences , with a particular focus on design efciency.16 ou et al17 provide case studies of ve types of trial designs for selecting patruly benet from a target therapy and tients who will discuss the advantages and disadvantages of each design . renfro et al18 discuss the unique challenges often encountered in any rare tumor setting and the best practices used by the childrens oncology group to address these challenges . 
now that clinical trials can use precision oncology to dene molecular subtypes of cancers and specic targeted treatments , those trials increasingly encounter the same challenges as those faced by the childrens oncology group . 
thus , their solutions to these challenges are highly relevant beyond pediatric oncology trials . one of the challenges in evaluating precision oncology agents is the diversity of each patients journey in clinical practice . 
degtyarev et al19 address the estimand framework , which provides a structured approach for discussing how to account for intercurrent events that occur after random assignment and may affect the assessment or interpretation of the treatment effect . 
they illustrate this framework by using a trial for chimeric antigen receptor t - cell therapy . the main purpose of this collection of tutorial and review articles is to inform clinical researchers about statistical concerns that should be considered in their research projects and to encourage professional statisticians to use cutting - edge methods in their analyses . 
because the authors of this collection are leading developers of these methods , it is also a great resource for statisticians who are interested in learning about oncology research by providing a succinct overview of the literature . although there are many novel statistical methods currently being developed to address the challenges of precision oncology , they are published primarily in statistical it is important to increase awareness of these methods among clinical researchers so that theory can be brought into practice . 
we hope this series will serve as a bridge between clinical researchers and statisticians and will help disseminate information and transfer knowledge so these powerful designs and methods can be used to advance precision oncology . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . ying lu consulting or advisory role : paxvax , nektar therapeutics , zap surgical systems , abeona therapeutics ( inst ) research funding : merck ( inst ) j . 
jack lee consulting or advisory role : abbvie no other potential conicts of interest were reported . references liu s , lee jj : an overview of the design and conduct of the battle trials . 
n engl j med 375 : 83 - 84 , 2016 diamond el , subbiah v , lockhart ac , et al : vemurafenib for braf v600 - mutant erdheim - chester disease and langerhans cell histiocytosis : analysis of data from the histology - independent , phase 2 , open - label ve - basket study . 
herbst rs , gandara dr , hirsch fr , et al : lung master protocol ( lung - map ) : a biomarker - driven protocol for accelerating development of therapies for squamous cell lung cancerswog s1400 . 
n engl j med 377 : 62 - 70 , 2017 chen ap , eljanne m , harris l , et al : national cancer institute basket / umbrella clinical trials : match , lungmap , and beyond . 
cancer j 25 : 272 - 281 , 2019 zhao y , chang c , long q : knowledge - guided statistical learning methods for analysis of high - dimensional - omics data in precision oncology . 
renfro la , ji l , piao j , et al : trial design challenges and approaches for precision oncology in rare tumors : experiences of the childrens oncology group . 
 prevalence of homologous recombinationrelated gene mutations across multiple cancer types purpose the prevalence of homologous recombination dna damage repair ( hr - ddr ) deficiencies among all tumor lineages is not well characterized . 
therapy directed toward homologous recombination ddr deficiency ( hrd ) is now approved in ovarian and breast cancer , and there may be additional opportunities for benefit for patients with other cancers . 
comprehensive evaluations for hrd are limited in part by the lack of a uniform , cost - effective method for testing and defining hrd . methods molecular profiles of 52 , 426 tumors were reviewed to identify pathogenic mutations in the hr - ddr genes arid1a , atm , atrx , bap1 , bard1 , blm , brca1 / 2 , brip1 , chek1 / 2 , fanca / c / d2 / e / f / g / l , mre11a , nbn , palb2 , rad50 , rad51 , rad51b , or wrn . 
 a total of 17 , 566 tumors were sequenced with ngs600 ( n = 592 genes ) , and 34 , 860 tumors underwent hotspot illumina miseq platform testing ( n = 47 genes )  . results of the tumors that underwent ngs600 testing , the overall frequency of hrddr mutations detected was 17.4% , and the most commonly mutated lineages were endometrial ( 34.4% ; n = 1 , 475 ) , biliary tract ( 28.9% ; n = 343 ) , bladder ( 23.9% ; n = 201 ) , hepatocellular ( 20.9% ; n = 115 ) , gastroesophageal ( 20.8% ; n = 619 ) , and ovarian ( 20.0% ; n = 2 , 489 )  . 
germline mutations in one or both of these genes place patients at heightened risk for development of breast , 1 - 6 ovarian , 1 - 6 prostate , 7 - 9 melanoma , 7 , 10 and pancreatic cancers7 , 10 - 12 during their lifetime . 
it has become apparent that brca interacts with a number of other dna repair proteins to form a complex system for ddr , including atm , rad51 , palb2 , mre11 , rad50 , nbn , and the fanconi anemia proteins.13 , 14 recent evidence suggests mutations in palb2 , atm , and the genes responsible for the mrn complex , rad50 , mre11 , and nbn , play a role in hereditary cancers.15 , 16 for example , palb2 mutation carriers have a lifetime risk of breast cancer development of approximately 50% , 17 , 18 and atm mutation carriers are at higher risk for development of breast , 19 , 20 pancreatic , 21 , 22 and prostate cancers.23 , 24 arielle l . 
in germline brca1 / 2 mutation carriers , exposure to platinum chemotherapy led to improved objective response rates in advanced triple - negative breast cancer versus taxanes ( 68% v 33% ) , 25 and overall survival in pancreatic cancer versus other nonplatinum chemotherapy ( 22 months v 9 months ) .26 mychoice hr - ddr deficiency ( hrd ) score - high triple - negative breast cancer responded better to platinum - based neoadjuvant therapy , with pathologic complete response ( cr ) rates of 27.5% versus 0% in the hr - ddrproficient cohort.27 the mychoice hrd score is frequently used to identify patients with hrd . 
it is a proprietary diagnostic test to assess a hrd phenotype , including an evaluation of loss of heterozygosity , telomeric allelic imbalance , and large - scale state transitions . on exposure to another class of dna - damaging agents , poly - adp ribose polymerase ( parp ) inhibitors , patients with germline or somatic deleterious mutations in the hr - ddr pathway have also achieved favorable responses . 
in this study , three patients had germline brca2 mutations , three patients had germline atm mutations , and the remaining responders had tumor expression of a deleterious mutation ( including palb2 , brca2 , brca1 , chek2 , fanca , and atm ) .35 all germline mutation carriers except for one patient with atm mutation responded to therapy . despite the exciting therapeutic potential of dna - damaging agents in patients with broader evidence of hrd , the prevalence of hrd among all tumors is largely unknown . 
the aim of our study was to determine the prevalence of hr - ddr pathogenic or presumed pathogenic mutations detected on tumor next - generation sequencing ( ngs ) testing across multiple cancer lineages , using commercially available dna sequencing ( ngs or sanger sequencing panel testing , multiplatform profiling ; caris life sciences [ caris ] , irving , tx ) to better define the proportion of patients who may benefit from such therapy . methods study design approval for this study was obtained from the georgetown university institutional review board . 
we defined hrd on tumor ngs testing as a mutation in the following genes , each of which has some activity within the hr - ddr pathway36 - 45 and has been included previously in hr - ddr biomarker clinical trials : arid1a , atm , atrx , bap1 , bard1 , blm , brca1 / 2 , brip1 , chek1 / 2 , fanca / c / d2 / e / f / g / l , mre11a , nbn , palb2 , rad50 , rad51 , rad51b , or wrn . 
frequencies of each mutation were determined for the total cohort , as well as for each cancer lineage ( biliary tract , bladder , breast , cervix , colorectal [ crc ] , endometrial , gastro esophageal [ ge ] , gastrointestinal stromal [ gist ] , glioma , head and neck , hepatocellular [ hcc ] , melanoma , neuroendocrine / small cell lung , nonsmall - cell lung [ nsclc ] , ovarian , pancreas , prostate , renal , sarcoma , thyroid , and unknown primary )  . ngs testing platforms hr - ddr mutation analysis from solid tumor biopsy specimens was determined by ngs at caris , a clinical laboratory improvement amendmentscertified laboratory . 
while 17 , 566 tumors were sequenced with ngs600 , 34 , 860 tumors underwent hotspot illumina miseq platform testing ( illumina truseq amplicon cancer hotspot panel , evaluating 47 genes including the hr - ddr genes atm , brca1 , and brca2 ; illumina , san diego , ca )  . 
tumor enrichment was achieved by harvesting targeted tissue by manual microdissection performed on all cases before molecular testing . the pathogenicity of gene variants identified were interpreted by board - certified molecular geneticists and categorized as pathogenic , presumed pathogenic , variant of unknown significance , presumed benign , or benign , according to american college of medical genetics and genomics standards on the basis of the level of evidence of published studies on the identified variants.46 , 47 only pathogenic or presumed pathogenic mutations were considered deleterious ; variants of unknown significance and variants that have not been previously reported in individuals affected by cancer in the literature were excluded . 
 deleterious mutations reported included frameshift mutations , premature stop codons , mutations shown to disrupt natural splicing , as well as point mutations ; deleterious mutations included those that have and have not been reported as causal for hereditary cancers . statistical analysis the proportion of pathogenic or presumed pathogenic mutations identified from all tumor specimens tested for each specific mutation were calculated for the total cohort and for each cancer lineage investigated . 
the total frequency of hr - ddr mutations in the complete cohort and per cancer lineage was calculated by dividing the number of tumors carrying at least one mutation by the total number of tumors tested , to avoid counting tumors carrying more than one hr - ddr mutation multiple times . 
the 95% cis were computed using the pearson - klopper exact method using r ( org / ) , and the graphics were generated by spss statistics , version 24 ( ibm , armonk , ny )  . results we evaluated 52 , 426 solid tumor pathologic specimens that underwent extended ngs for hrd . 
molecular profiling was performed on the primary tumor in 47.9% of cases ( n = 25 , 102 ) , and on a metastatic site of disease in 41.9% ( n = 21 , 956 )  . 
 within the tumor lineages , the frequencies of mutations varied ( tables 2 and 3 ; fig 2 )  . hr gene mutation frequency overall , pathogenic mutations within the homologous recombination pathway were seen in 17.4% of the 17 , 566 tumors tested with ngs600 , and 8.3% of the 52 , 426 solid tumors overall ( including 34 , 860 tumors that were evaluated for atm , brca1 , and brca2 mutations only on the hotspot panel )  . 
 brca1 / 2 mutations were seen predominately in ovarian and breast cancers , though pathogenic brca2 mutations were seen in high frequencies among gi and nonovarian genitourinary malignancies , as well . 
although palb2 mutations were less common overall and appreciated in only 0.6% of tumors tested , a significant proportion of palb2 mutations was found in bladder , breast , and gi malignancies . 
no pathogenic mutations were identified in bard1 , chek1 , fanca / d2 / e / f / g / l , rad51 , or rad51b ( table 4 )  . hr - ddr gene mutations were appreciated in both primary and metastatic lesions , though with different patterns . 
the remaining mutated hr - ddr genes ( blm , brip1 , chek2 , fancc , mre11a , nbn , palb2 , rad50 , and wrn ) had similar frequencies among primary and metastatic tissue evaluations . tumors with multiple hr gene mutations of the 17 , 566 tumors that underwent extended molecular profiling with the ngs600 platform , 362 were found to carry more than one hr - ddr pathway mutation , including 112 endometrial ( 7.6% ; n = 1 , 475 ) , 75 crc ( 3.1% ; n = 2 , 454 ) , 34 ovarian ( 1.4% ; n = 2 , 489 ) , 29 nsclc ( 0.9% ; n = 3 , 245 ) , 23 ge ( 3.7% ; n = 619 ) , 20 breast ( 1.2% ; n = 1 , 625 ) , and 15 biliary tract ( 4.4% ; n = 343 ) tumors . 
total bar height represents the overall frequency of hr - ddr deficient tumors within each lineage ; colored bar length represents the relative mutation frequency of individual genes in each cancer type . 
summary of homologous recombination dna damage repair mutations identified * overall , % ngs600 , % hotspot , % mutation arid1a brca2 brca1 atrx chek2 bap1 palb2 brip1 fancc rad50 mre11a abbreviation : n / a , not applicable . * no mutations identified : bard1 , chek1 , fanca / d2 / e / f / g / l , rad51 , rad51b . in this large - scale study of ngs molecular profiling of solid tumor samples across multiple cancer lineages , we confirmed hrd is common and was observed in 17.4% of the solid tumors evaluated by the ngs600 platform ( spanning 21 cancer lineages )  . 
in a recent evaluation of brca1 / 2 mutational patterns , for example , a model to detect brca1 / 2 deficiency failed to correlate brca1 / 2 mutational patterns with pathogenic mutations in several additional hr - ddr pathway genes , including atm , atr , chek2 , the fanc group of genes , palb2 , pten rad50 , and rad51c.48 the unique genetic signatures across the breadth of hr - ddr pathway genes are not well characterized , and , as such , it is unknown if the lack of a brca - like mutational pattern is associated with altered responses to parp inhibitors and dna - damaging chemotherapy . our reported frequencies of hrd are similar to previously published work , though a range of frequencies is appreciated ( table 5 )  . 
because there is not yet an established way to measure hrd , and previous studies have measured hrd by an hrd assay assessing large - scale transition scores and telomere allelic imbalances , germline mutations , somatic mutations , brca - like genetic signatures , or a combination of these methods , the differences in hrd prevalence may be related to nonuniformity of assessment . 
in addition , significant variation will occur between whole - exome sequencing versus use of hotspot panels , with the identification of hrd more common among studies that used whole - exome sequencing . 
within our study , 17 , 566 tumors ( 33.5% of the total 52 , 426 tumors tested ) underwent sequencing with the targeted whole - exome sequencing platform ngs600 , which evaluated tumors for 592 genes , assuming dna was sufficient . 
consequently , studies including an evaluation for pten mutations are expected to report higher frequencies of hrd . it is also possible frequencies of hrd may differ across studies as a result of differences in patient population . 
patients with tumors harboring hr - ddr pathway mutations may be more sensitive to dna - damaging chemotherapy and therefore less likely to recur after initial treatment of localized disease . 
although the clinical stage of patients included in our analysis at the time of tissue acquisition ( and if tissue was obtained at presentation ) was unknown , it is possible our population was enriched with patients with metastatic disease without hrd who were less likely to respond favorably to frontline treatment and , therefore , recurred . looking forward , classifying tumors as hr - ddr deficient will likely become increasingly important , as we now appreciate that hrd is common and has been associated with improved outcomes in some patients treated with dna - damaging therapies . 
several clinical trials are assessing in part the role of hrd in response to anticancer therapies and outcomes , including treatment with parp inhibitor therapy alone , but also in combinations with chemotherapy , radiation therapy , or immunotherapy to enhance antitumor efficacy . 
in tandem , it will be important to generate a consensus regarding uniform testing to identify appropriate patients for these tailored therapies . there are some limitations of this study to note . 
given the nature of the study , we evaluated patients tumor tissue for the presence of hr - ddr mutations and thus are unable to distinguish whether a given mutation was a somatic or germline mutation . 
we were also unable to assess tumors for epigenetic modifications such as dna methylation , which could also lead to significant and clinically relevant alterations in gene expression affecting functions of the hr pathway.57 , 58 in addition , hrd is defined by currently available literature regarding the suspected pathogenicity of each mutation . 
it is certainly possible that mutations labeled as a variant of unknown significance may prove important in the future , although the majority are reclassified as benign polymorphisms.59 - 61 we also recognize our results are influenced by the overrepresentation of certain cancer lineages , including ovarian ( n = 9 , 630 ) , nsclc ( n = 8 , 119 ) , crc ( n = 6 , 650 ) , breast ( n = 5 , 910 ) , and endometrial ( n = 5 , 540 ) cancers in the caris database . 
baker employment : caris life sciences , roche travel , accommodations , expenses : caris life sciences , roche honoraria : roche , amgen , bayer / onyx , taiho pharmaceutical , caris life sciences , celgene consulting or advisory role : roche , amgen , bayer / onyx , taiho pharmaceutical , caris life sciences , celgene speakers ' bureau : roche , amgen , bayer / onyx , celgene , taiho pharmaceutical research funding : bayer / onyx ( inst ) , roche ( inst ) , pfizer ( inst ) , amgen ( inst ) , boehringer ingelheim ( inst ) , medimmune ( inst ) claudine isaacs honoraria : roche , astrazeneca , pfizer , novartis , syndax , nanostring technologies consulting or advisory role : pfizer , roche , novartis , astrazeneca , medivation , nanostring technologies , syndax speakers ' bureau : genentech , pfizer , astrazeneca research funding : novartis ( inst ) , pfizer ( inst ) , genentech ( inst ) , tesaro patents , royalties , other intellectual property : uptodate , mcgraw hill publishing affiliations arielle l . 
antoniou a , pharoah pd , narod s , et al : average risks of breast and ovarian cancer associated with brca1 or brca2 mutations detected in case series unselected for family history : a combined analysis of 22 studies . 
van der kolk dm , de bock gh , leegte bk , et al : penetrance of breast cancer , ovarian cancer and contralateral breast cancer in brca1 and brca2 families : high cancer incidence at older age . 
kote - jarai z , leongamornlert d , saunders e , et al : brca2 is a moderate penetrance gene contributing to young - onset prostate cancer : implications for genetic testing in prostate cancer patients . 
casadei s , norquist bm . , walsh t , et al : contribution to familial breast cancer of inherited mutations in the brca2 - interacting protein palb2 to familial breast cancer . 
telli ml , timms km , reid j , et al : homologous recombination deficiency ( hrd ) score predicts response to platinum - containing neoadjuvant chemotherapy in patients with triple - negative breast cancer . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
oza am , tinker av , oaknin a , et al : antitumor activity and safety of the parp inhibitor rucaparib in patients with high - grade ovarian carcinoma and a germline or somatic brca1 or brca2 mutation : integrated analysis of data from study 10 and ariel2 . 
mccabe n , turner nc , lord cj , et al : deficiency in the repair of dna damage by homologous recombination and sensitivity to poly ( adp - ribose ) polymerase inhibition . 
aarts m , bajrami i , herrera - abreu mt , et al : functional genetic screen identifies increased sensitivity to wee1 inhibition in cells with defects in fanconi anemia and hr pathways . 
pennington kp , walsh t , harrell mi , et al : germline and somatic mutations in homologous recombination genes predict platinum response and survival in ovarian , fallopian tube , and peritoneal carcinomas . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
yap kl , kiyotani k , tamura k , et al : whole - exome sequencing of muscle - invasive bladder cancer identifies recurrent mutations of unc5c and prognostic importance of dna repair gene mutations on survival . 
stjepanovic n , kim rh , wilson m , et al : clinical outcome of patients with advanced triple negative breast cancer with germline and somatic variants in homologous recombination gene . 
shahda s , timms k , ibrahim a , et al : homologous recombination deficiency ( hrd ) in patients with pancreatic cancer ( ps ) and response to chemotherapy . 
bang yj , im sa , lee kw , et al : randomized , double - blind phase ii trial with prospective classification by atm protein level to evaluate the efficacy and tolerability of olaparib plus paclitaxel in patients with recurrent or metastatic gastric cancer . 
easton df , deffenbaugh am , pruss d , et al : a systematic genetic assessment of 1 , 433 sequence variants of unknown clinical significance in the brca1 and brca2 breast cancer - predisposition genes . 
dabrafenib , a braf inhibitor , and pazopanib , a multikinase inhibitor that targets vascular endothelial growth factor and platelet - derived growth factor , have not been combined previously . 
this phase i study was designed to evaluate the safety , pharmacokinetics , and pharmacodynamics of the combination . patients and methods patients with any advanced braf mutated malignancy with adequate organ function were eligible . 
dosages started at dabrafenib 50 mg twice a day and pazopanib 400 mg daily on dose level ( dl ) 1 , with maximum dosages of 150 mg twice a day and 800 mg daily on dl5 . 
pharmacokinetics and braf v600e plasma clone were measured , and efficacy was evaluated by imaging and tumor markers every 8 weeks . results twenty - three patients with 11 different tumor histologies were enrolled in five dls . 
common drug - related adverse events included nausea ( 52% ) , skin papules ( 43% ) , diarrhea ( 39% ) , hand - foot syndrome ( 30% ) , anemia ( 26% ) , rash ( 22% ) , vomiting ( 22% ) , hypophosphatemia ( 22% ) , and transaminitis ( 22% )  . 
five patients ( 22% ) experienced a partial response , including low - grade ovarian serous carcinoma , thyroid cancer , and glioblastoma multiforme , and two patients ( appendiceal and thyroid cancer ) had stable disease > 6 months . 
2018 by american society of clinical oncology introduction considered driver mutations in some tumor types , braf mutations are found in several types of cancer , 1 including melanoma , papillary thyroid cancer , 2 colorectal cancer , 3 and low - grade serous ovarian cancer ( lgsoc ) .4 braf inhibitor therapy is associated with an impressive , albeit shortlived , response rate in the treatment of malignant melanoma.5 in other malignancies , the activity of single - agent braf inhibitor is mixed . 
for example , limited efficacy was observed in colorectal cancer , 6 but favorable activity was shown in non small - cell lung cancer.7 mechanisms of resistance differ by tumor type . 
in melanoma , upregulation of the mitogen - activated protein kinase ( mapk ) pathway via mutations in alternate splicing of nras , mek , and braf leads to primary resistance.8 - 10 in addition , upregulation of platelet - derived growth factorin melanoma tumors from patients and in melanoma cell lines has been observed.11 in colorectal cancer , primary resistance seems to be via upregulation of the epidermal growth factor receptor and the mapk pathway , 12 , 13 although increased platelet - derived growth factor ( pdgf - b ) and signal transducer and activator of transcription 3 ( stat - 3 ) phosphorylation have also been sigurdis haraldsdottir filip janku ming poi cynthia timmers susan geyer larry j . 
an example of a fruitful attempt is the combination of dabrafenib , a braf inhibitor , with trametinib , a mek 1 / 2 inhibitor , in melanoma.16 collectively , it is compelling to combine therapies that target the aforementioned pathways with a braf inhibitor to synergize the effects of the agents and enhance the durability of response by abating drug resistance . we conducted an investigator - initiated multicenter phase i clinical trial that combined dabrafenib and pazopanib in the treatment of advanced braf mutated malignancies . 
eligibility criteria included any advanced malignant tumor carrying a mutation in the braf gene for which no standard curative or palliative measures existed , no treatment within 2 weeks of study enrollment , eastern cooperative oncology group performance status of 2 , life expectancy > 12 weeks , age 18 years , no prior use of dabrafenib or pazopanib , no more than three prior multikinase inhibitor regimens , normal organ function defined by an absolute neutrophil count of 1 , 500 / ml , hemoglobin 9 g / dl , and a platelet count of 100 , 000 / ml , as well as normal renal function ( creatinine 1.5 upper limit of normal and urine protein to creatinine ratio < 1 ) , hepatic function ( alt / ast 2.5 upper limit of normal and bilirubin 1.5 upper limit of normal ) , and cardiac function ( left ventricular ejection fraction 50% )  . 
patients with symptomatic , untreated brain metastases , hiv , hepatitis b or c , poorly controlled hypertension ( defined as systolic blood pressure 140 mm hg and / or diastolic blood pressure 90 mm hg measured on more than one occasion and not responsive to antihypertensives ) , qt interval > 480 ms , or who received excluded medications ( warfarin , antiepileptics , and / or antifungals , among others ) were excluded . 
braf mutation testing for study entry must have been performed at a clinical laboratory improvement amendmentscertified laboratory . dose escalation and administration dose escalation was performed on the basis of a standard cohorts - of - 3 designdose level 1 ( dl1 ) was dabrafenib 50 mg twice a day and pazopanib 400 mg daily ; dl2 was dabrafenib 50 mg twice a day and pazopanib 600 mg daily ; dl3 was dabrafenib 100 mg twice a day and pazopanib 600 mg daily ; dl4 was dabrafenib 100 mg twice a day and pazopanib 800 mg daily ; and dl5 was dabrafenib 150 mg twice a day and pazopanib 800 mg daily , administered in 28 - day cycles without interruption . 
all patients who were treated within a dl had to complete 28 days of therapy before escalation to the next dl and had to receive 80% of the doses of each drug ( or else they were replaced with another enrolled study patient )  . safety and efficacy assessments after drug initiation , patients were assessed on days 8 , 15 , 22 , 29 , and 43 , then every 4 weeks for adverse events , vital signs , hematology , chemistries , prothrombin time / partial thromboplastin time , urinalysis , and spot urine protein - to creatinine ratio . 
 dlts included grade 3 hematologic toxicities ( except grade 3 that resolved 7 days of stopping drugs or grade 3 lymphopenia ) ; fever 38.5c associated with dehydration , hypotension , or renal insufficiency ( two or more occasions ) ; grade 2 proteinuria ( unresolved 2 weeks of holding drugs ) ; grade 2 valvular toxicities ; asymptomatic decrease in left ventricular ejection fraction 10% that resulted in left ventricular ejection fraction at or below the institutional lower limit of normal ; symptomatic hypertension or recurring 160 / 100 mm hg despite antihypertensive medication ; and any grade 3 nonhematologic toxicities , excluding nausea , vomiting , diarrhea , electrolyte disturbance , fatigue , rash , or acute kidney injury that resolved 7 days of holding drugs . radiologic assessment was performed by computed tomography or magnetic resonance imaging ( as long as the same consistent measure was used serially ) every 8 weeks , and responses were measured according to recist 1.1. 
tumor markers , if applicable , were measured every 8 weeks . pharmacokinetic studies a single dose of dabrafenib was administered on cycle 1 , day 1 ( c1d1 ) , and a single dose of pazopanib on c1d2 . 
blood samples for dabrafenib and pazopanib pks were obtained predose , at 0.5 , 1 , 2 , 3 , 4 , 6 , 8 0.5 hours , and at 24 1 hours after drug administration on c1d1 , c1d2 , c1d3 , and c2d1 . 
 noncompartmental analysis of concentration time data were performed using phoenix winnonlin ( version 6.3 ; pharsight corporation , mountain view , ca )  . pharmacodynamic studies correlative studies included the quantification of the copy number of the braf v600e mutant allele in cell - free dna that was purified from plasma . 
we performed cell - free dna analysis on plasma samples that were collected at c1 to c6 and every other cycle beyond c6 using an allele - specific digital polymerase chain reaction assay on the qx200 droplet digital polymerase chain reaction system ( bio - rad laboratories , hercules , ca )  . 
archival formalin - fixed , paraffin embedded tumor tissue was collected , and dna was extracted to sequence the coding exons of 409 tumor suppressor and oncogenes using the ion torrent comprehensive cancer panel ( thermo fisher scientific , waltham , ma )  . 
maximum grade , frequency , and perceived attribution of adverse events were summarized across and within dls per national cancer institute common terminology criteria for adverse events criteria ( version 4 )  . 
per these criteria , toxicity was defined as an adverse event that was at least possibly related to treatment . in an exploratory manner , clinical outcomes were summarized , including overall response , time to progression ( ttp ) , and duration of response , and were based on recist criteria . 
of note , two patients on dl5 ( patients 5b and 5f ) received < 80% of drug doses and were replacedone patient experienced rapid disease progression with new brain metastasis , the other developed radiation recall after 3 days of therapy . 
two dlts were observed , which included grade 3 bowel perforation on dl3 , which was attributed to pazopanib , and grade 3 arthralgias on dl5 , which was attributed to dabrafenib . 
therapy was discontinued in three patients because of adverse events that included grade 3 bowel perforation that developed 4 days after therapy initiation , grade 2 radiation recall that developed 3 days after therapy initiation , 17 and grade 2 uveitis that developed 10 months after therapy initiation . 
serious adverse events possibly related to study drugs that led to hospital admission included a grade 3 to 4 pulmonary emboli , grade 3 abdominal pain , grade 2 intracranial hemorrhage , and grade 2 fever . response rate and ttp five ( 22% ; 95% ci , 7% to 44% ) of 23 patients achieved partial responses after 2 to 4 months of therapy ( fig 1 )  . 
 ( % ) , unless otherwise noted . abbreviations : ecog , eastern cooperative oncology group ; q , quartile . * nineteen patients with available data . the study and enrolled them in five dls ( table 1 )  . 
 grade grade grade toxicity ophthalmologic floaters photosensitivity uveitis skin skin papule or tag palmar - plantar erythrodysesthesia syndrome rash maculopapular dry skin actinic keratosis pruritus radiation recall reaction rash acneiform skin hyperpigmentation skin induration treatment - related secondary malignancy ( melanoma ) miscellaneous acute kidney injury dysmenorrhea flank pain menorrhagia oral pain thromboembolic event total events 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 10 ( 43 ) 7 ( 30 ) 4 ( 17 ) 3 ( 13 ) 2 ( 9 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) 1 ( 4 ) abbreviation : dl , dose level . * expanded to six patients ( two patients on dl5 had < 80% of doses and were replaced )  . grade 4 or 5 events were not observed . pk parameters of first - dose and steady - state pazopanib and dabrafenib are listed in tables 3 and 4 , respectively . 
appendix figures a1 and a2 ( online only ) depict mean plasma concentration time profiles stratified by dl for first - dose ( monotherapy ) and steady - state ( combination ) pazopanib and dabrafenib , respectively . 
 papillary thyroid cancer ( follicular variant ) ovarian cancer ( low grade , serous ) papillary thyroid cancer ae , papillary thyroid cancer papillary thyroid cancer appendiceal adenocarcinoma ovarian cancer ( low grade , serous ) glioblastoma multiforme * hrthle cell thyroid cancer cholangiocarcinoma nonsmall - cell lung cancer * parotid gland carcinoma melanoma melanoma bladder cancer melanoma colon cancer nonsmall - cell lung cancer papillary thyroid cancer melanoma ae , neuroendocrine carcinoma of colon * patient withdrawal , colon cancer ae , nonsmall - cell lung cancer time on treatment ( months ) time to response time to off treatment fig 1 . 
 ( * ) found to have discordance in braf mutation testing . concentrationtime profiles stratified by dl on c1d2 , whereas appendix figure a4b shows the predicted mean steady - state on the basis of firstdose pazopanib monotherapy pk data in the absence of drug interaction . 
only 39% and 20% of patients had a trough pazopanib concentration of > 17.5 g / ml on c1d15 and at steady state ( c2d1 ) , and only 13% of patients had a trough pazopanib concentration of > 20.5 g / ml at steady state ( c2d1 )  . 
samples from 16 patients were collected for both dabrafenib and pazopanib 24 - hour profile pharmacokinetics analysis on c2d1 . abbreviations : auc ( 0 - ) , observed area under the curve from 0 to infinity ; cmax , maximum observed concentration ; cssavg , average steady - state concentration ; cl / f , clearance ; fd , first dose ; ss , steady state ; t1 / 2 , terminal phase elimination half - life ; v / f , apparent volume of distribution on the basis of terminal phase . * the accumulation of dabrafenib is insignificant ; therefore , auc0is presented here for first dose and steady state for direct comparison . pharmacodynamics / braf v600e plasma measurements fig 2 . 
log ratio of braf v600e / braf wild type is depicted before therapy , lowest value on therapy , and value upon progression for patients who remained on therapy for more than two cycles . we measured braf v600e copies in circulating tumor dna in 19 patients . 
changes in copies along with tumor measurements and / or tumor markers in patients in the study for more than two cycles are shown in appendix figure a5 ( online only )  . 
the most common adverse events included nausea , vomiting , diarrhea , transaminitis , arthralgia , and skin toxicities , but the combination did not increase toxicities compared with the administration of either agent alone.18 , 19 two dltsa grade 3 bowel perforation on dl3 and grade 3 arthralgia on dl5were observed . 
 long - term toxicities were not prohibitive , as six patients were on therapy for > 6 months . ideally , time - dependent pks would have been measured with a run - in , with each drug measuring single dose and steady state , but given the refractory study population , a single drug run - in was not considered feasible . 
dabrafenib mean terminal half - lives grew shorter with repeated dosing at steady state , and mean auc ratios of c2d1 : c1d1 were < 1.0 , which suggests autoinduction of the drug.20 this correlates with previous reports in monotherapy studies.21 , 22 pk parameters for first single - dose pazopanib were overall consistent with previously published data from pazopanib monotherapy studies23 - 25 ; however , the steady - state concentration of pazopanib was lower than expected . 
in preclinical models , a steady - state concentration of > 17.5 g / ml was required for in vivo activity of pazopanib , 26 and a target pazopanib trough concentration of > 20.5 g / ml is associated with improved efficacy in patients with renal cell carcinoma.21 only 20% of patients in this study reached trough pazopanib concentrations of > 17.5 g / ml at steady state ( c2d1 ) , and only 13% of the patients achieved a trough pazopanib concentration of > 20.5 g / ml at steady state ( c2d1 )  . 
 the efficacy of single - agent multikinase inhibitors in thyroid cancer is well known , 30 - 32 with two agentssorafenib and lenvatinibapproved by the us food and drug administration . 
dabrafenib demonstrated partial responses in 33% of patients with braf mutated papillary thyroid carcinoma.33 , 34 braf mutations are found in 36% of patients with lgsoc tumors.4 two case reports of the administration of a braf inhibitor in heavily pretreated patients with unresectable lgsoc demonstrated a long lasting response.35 , 36 both patients with lgsoc in this trial were heavily pretreated and one had received an mek inhibitor as well as sorafenib / vemurafenib combination therapy . 
approximately 2% of glioblastomas have braf mutations , 37 and a response to vemurafenib was observed in a basket trial that included glioblastoma.36 we did not observe any activity in four patients with melanoma who had previously experienced progression on vemurafenib . 
it is possible that the combination does not target resistance mechanisms that promote progression on prior braf inhibitor therapy . measurements of the plasma braf v600e clone were positive in 58% of patients at baseline . 
this suggests that this type of monitoring could be used to determine clinical efficacy but should be undertaken in a larger trial . tumor heterogeneity was observed in three nonresponding patients with discordant outside braf testing that was obtained after coming off the trial . 
furthermore , we allowed tumor types with non - v600 braf mutations in this study , as dabrafenib does not exclusively inhibit braf v600 mutations , but we did not observe any activity in these patients . 
tumor sequencing of 409 tumor suppressor and oncogenes did not reveal any other significant findings . strengths of our study include the robust pk data that were obtained as well as assessment of braf v600e plasma clone levels during therapy and upon progression . 
therefore , a randomized phase ii trial is warranted in certain tumor types to determine whether the combination is superior to single - agent therapy or combination braf / mek inhibitor therapy . 
shah ming poi stock and other ownership interests : immunomedics , cti biopharma , juno therapeutics , propanc biopharm , pfizer , merck consulting or advisory role : salveo health communications , sandoz - novartis financial support : manisha h . 
shah collection and assembly of data : sigurdis haraldsdottir , filip janku , cynthia timmers , jennifer sexton , lai wei , jennifer thurmond , vivianne velez - bravo , erin m . 
schaaf , lai wei , kari kendra , amir mortazavi , vivek subbiah , mitch phelps manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors cynthia timmers no relationship to disclose susan geyer no relationship to disclose larry j . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : abbott nutrition research funding : medimmune ( inst ) , pfizer ( inst ) , bristol - myers squibb ( inst ) , ignyta ( inst ) patents , royalties , other intellectual property : us and foreign patents travel , accommodations , expenses : medimmune sigurdis haraldsdottir no relationship to disclose filip janku stock and other ownership interests : trovagene consulting or advisory role : deciphera , trovagene , novartis , sequenom , foundation medicine , guardant health , immunome research funding : novartis , biomed valley discoveries , roche , agios , astellas pharma , deciphera , symphony evolution , plexxikon , piqur , fujifilm other relationship : bio - rad vivianne velez - bravo no relationship to disclose vanda m . 
shah consulting or advisory role : eisai , loxo , novartis research funding : eisai , merck , loxo amir mortazavi honoraria : motive medical intelligence consulting or advisory role : genentech research funding : acerta pharma ( inst ) , genentech ( inst ) , merck ( inst ) , novartis ( inst ) , seattle genetics ( inst ) vivek subbiah consulting or advisory role : medimmune research funding : novartis ( inst ) , glaxosmithkline ( inst ) , nanocarrier ( inst ) , northwest biotherapeutics ( inst ) , genentech ( inst ) , berg pharma ( inst ) , bayer ( inst ) , incyte ( inst ) , fujifilm ( inst ) , pharmamar ( inst ) , d3 oncology solutions ( inst ) , pfizer ( inst ) , amgen ( inst ) , abbvie ( inst ) , multivir ( inst ) , blueprint medicines ( inst ) , loxo ( inst ) , vegenics ( inst ) , takeda ( inst ) , alfasigma ( inst ) , agensys ( inst ) , idera ( inst ) , boston biomedical ( inst ) travel , accommodations , expenses : pharmamar , bayer affiliations sigurdis haraldsdottir , ming poi , cynthia timmers , susan geyer , larry j . 
shah , ohio state university medical center , columbus , oh ; sigurdis haraldsdottir , stanford university , stanford , ca ; filip janku , vivianne velez - bravo , vanda m . 
stepanek , and vivek subbiah , university of texas md anderson cancer center , houston , tx ; and susan geyer , university of south florida , tampa , fl . funded by national comprehensive cancer network oncology research program from general research support provided by novartis , the sidney kimmel foundation for cancer research , a 2015 university of texas brain seed grant , and the glioblastoma moonshot translational research on brain tumors grant . presented at the asco annual meeting , chicago , il , may 30 - june 3 , 2014 , and the 26th european organisation for research and treatment of cancer national cancer instituteamerican association for cancer research symposium on molecular targets and cancer therapeutics , barcelona , spain , november 18 - 21 , 2014 . support prior presentation references 417 : 949 - 954 , 2002 1 . 
nikiforova mn , kimura et , gandhi m , et al : braf mutations in thyroid tumors are restricted to papillary carcinomas and anaplastic or poorly differentiated carcinomas arising from papillary carcinomas . 
sieben nl , macropoulos p , roemen gm , et al : in ovarian neoplasms , braf , but not kras , mutations are restricted to low - grade serous tumours . 
planchard d , kim tm , mazieres j , et al : dabrafenib in patients with braf ( v600e ) - positive advanced nonsmall - cell lung cancer : a single - arm , multicentre , open - label , phase 2 trial . 
nazarian r , shi h , wang q , et al : melanomas acquire resistance to b - raf ( v600e ) inhibition by rtk or n - ras upregulation . 
wagle n , van allen em , treacy dj , et al : map kinase pathway alterations in braf - mutant melanoma patients with acquired resistance to combined raf / mek inhibition . 
ahronian lg , sennott em , van allen em , et al : clinical acquired resistance to raf inhibitor combinations in braf - mutant colorectal cancer through mapk pathway alterations . 
long gv , stroyakovskiy d , gogas h , et al : dabrafenib and trametinib versus dabrafenib and placebo for val600 braf - mutant melanoma : a multicentre , double - blind , phase 3 randomised controlled trial . 
hauschild a , grob jj , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
ouellet d , gibiansky e , leonowens c , et al : population pharmacokinetics of dabrafenib , a braf inhibitor : effect of dose , time , covariates , and relationship with its metabolites . 
shibata si , chung v , synold tw , et al : phase i study of pazopanib in patients with advanced solid tumors and hepatic dysfunction : a national cancer institute organ dysfunction working group study . 
kumar r , knick vb , rudolph sk , et al : pharmacokinetic - pharmacodynamic correlation from mouse to human with pazopanib , a multikinase angiogenesis inhibitor with potent antitumor and antiangiogenic activity . 
lawrence sk , nguyen d , bowen c , et al : the metabolic drug - drug interaction profile of dabrafenib : in vitro investigations and quantitative extrapolation of the p450 - mediated ddi risk . 
goh bc , reddy nj , dandamudi ub , et al : an evaluation of the drug interaction potential of pazopanib , an oral vascular endothelial growth factor receptor tyrosine kinase inhibitor , using a modified cooperstown 5 + 1 cocktail in patients with advanced solid tumors . 
brose ms , nutting cm , jarzab b , et al : sorafenib in radioactive iodine - refractory , locally advanced or metastatic differentiated thyroid cancer : a randomised , double - blind , phase 3 trial . 
brose ms , cabanillas me , cohen ee , et al : vemurafenib in patients with braf ( v600e ) positive metastatic or unresectable papillary thyroid cancer refractory to radioactive iodine : a non - randomised , multicentre , open - label , phase 2 trial . 
combe p , chauvenet l , lefrre - belda ma , et al : sustained response to vemurafenib in a low grade serous ovarian cancer with a braf v600e mutation . 
 ( a through g ) patients who were on study for more than two cycles with measurable braf v600e plasma clone levels ( gold ) are depicted along with recist measurements ( sum of target lesions in centimeters depicted as blue columns , if disease was measurable ) and tumor marker ( gray , if measurable )  . 
in three patients with a partial response ( 3c , 4c , and 5e ) , plasma copies decreased , and in two patients ( 3c and 4c ) they became undetectable . 
two patients with stable disease > 6 months ( 2c and 5h ) had a decrease in copies ( one to undetectable levels , rising again upon progression )  . 
patient and tumor characteristics , tumor shrinkage , and tumor mutations in patients with partial responses and stable disease > 6 months patient id cancer type and time since diagnosis of metastatic disease until trial entry ( months ) appendiceal adenocarcinoma ( 44 ) lgsoc ( 6 ) lgsoc ( 105 ) ptc ( 119 ) ptc ( 24 ) gbm ( 45 ) follicular variant ptc ( 3 ) no . 
of prior therapies * 5 ( mek inhibitor , sorafenib + vemurafenib ) none none 1 ( sunitinib ) 3 ( vemurafenib ) shrinkage , sd ( nm ) tumor mutations ( deleterious ) braf v600e , ep400 , braf v600e sd ( nm ) braf v600e braf v600e , ddb2 braf v600e braf v600e time since acquiring tissue for testing until trial entry , months abbreviations : gbm , glioblastoma multiforme ; lgsoc , low - grade serous ovarian cancer ; mek , mitogen - activated pathway kinase kinase ; nm , nonmeasurable ; nt , not tested ; ptc , papillary thyroid cancer ; sd , stable disease . 
one year later , endometrial adenocarcinoma , endometrioid type international federation of gynecology and obstetrics grade 2 ( figo ; stage ii1 ) was diagnosed and treated with total abdominal hysterectomy and bilateral salpingo oophorectomy , followed by postoperative external beam radiotherapy and high - dose vaginal brachytherapy . 
immunohistologic studies for dna mismatch repair proteins on the endometrial adenocarcinoma revealed loss of expression of mlh1 and pms2 , and mlh1 promoter hypermethylation analysis was positive . another year later , positron emission tomography computed tomography scans indicated bilateral lung metastases suggestive of metastatic endometrial adenocarcinoma and a left axillary hypermetabolic lymph node suggestive of metastatic breast adenocarcinoma ( estrogen receptor negative , progesterone - receptor negative [ 1 + , 10% ] , and her2 negative )  . 
a biopsy specimen was taken of the chest wall lesion , which was found to be consistent with metastatic carcinoma most likely of breast origin , based on immunohistochemical and clinical findings . 
 follow - up magnetic resonance imaging testing showed metastases to bone and bra because of systemic progression , tumor molecular profiling for one of the chest wall lesions was performed using the stanford actionable mutation panel ( stamp ) assay , which is a 198 gene , hybrid - capturebased , solid - tumor , next generation sequencing panel . 
the case was discussed by the molecular tumor board ; the molecular profiling was considered to be suggestive of endometrial origin rather than breast orig given that the primary endometrial adenocarcinoma had been microsatellite unstable , microsatellite instability ( msi ) testing was recommended on the metastasis to enable the potential use of immune - checkpoint inhibitors , if positive . 
msi testing by polymerase chain reaction demonstrated that the tumor was msi high . after liposomal doxorubicin chemotherapy , stereotactic radiotherapy for the brain metastases , and palliative radiation therapy to a painful right acetabulum metastasis , the patient started treatment with pembrolizumab on a compassionate use basis because she did not qualify for current open trials ( having two active cancers ) , and this was before food and drug administration approval of immunotherapies for msi tumors . 
hence , although nonspecific , the - catenin ( ctnnb1 ) somatic mutation ( as opposed to an amplification ) is virtually never seen in ductal breast carcinoma and thus was a unique finding suggesting that the molecular signature of the biopsy specimen was more consistent with an endometrial adenocarcinoma origin than that of a breast adenocarcinoma . to more convincingly distinguish the tissue of origin of the patients metastatic disease , the molecular tumor board members recommended testing of mismatch repair protein status by polymerase chain reaction and agreed that if the tumor demonstrated microsatellite instability , the patient would be eligible to receive pembrolizumab as a participant in a local clinical trial or off label ( this was before the food and drug administration approval of pembrolizumab for msi - high tumors )  . discussion of possible alternatives to immune checkpoint inhibitors included therapeutic routes focused on targeting the akt - mtor pathway , because of pten and pik3ca mutations . 
 which has been demonstrated to respond to immunotherapy.6 published online on ascopubs.org / journal / po on september 19 , 2018 . rochelle reyes no relationship to disclose meredith mills research funding : myriad genetics ( inst ) recipient : natera ( inst ) james l . 
zehnder no relationship to disclose george sledge leadership : syndax stock and other ownership interests : syndax honoraria : symphony evolution consulting or advisory role : symphony evolution , coherus biosciences , radius health , peregrine pharmaceuticals , taiho pharmaceutical research funding : roche ( inst ) travel , accommodations , expenses : radius health , taiho pharmaceutical christina curtis consulting or advisory role : grail james m . 
 validation of her2 amplification as a predictive biomarker for anti epidermal growth factor receptor antibody therapy in metastatic colorectal cancer purpose her2 amplification has been implicated in resistance to therapy with anti epidermal growth factor receptor antibodies ( anti - egfrabs ) in metastatic colorectal cancer ( mcrc )  . 
the purpose of the study was to validate the predictive impact of her2 amplification in mcrc . patients and methods we analyzed patients with ras / braf wild - type mcrc across two distinct cohorts . 
 cohort 2 ( n = 70 ) included 16 patients with her2 amplification and 54 her2 nonamplified controls identified by next - generation sequencing ( her2 amplification : four or more copies ) who had received prior anti - egfrabs . 
2019 by american society of clinical oncology introduction antiepidermal growth factor receptor ( egfr ) antibodies ( anti - egfrabs ) , cetuximab and panitumumab , are routinely used , either alone or in combination with chemotherapy , in the treatment of metastatic colorectal cancer ( mcrc )  . 
 activating mutations in ras ( kras and nras ) genes are the only validated predictive biomarker of resistance to these agents.1 therefore , current practice guidelines recommend restricting anti - egfrab use to patients with ras wild - type tumors , which compose 45% to 50% of the population with mcrc.2 even among this kanwal raghav jonathan m . 
 select group , many patients do not derive clinical benefit from treatment with anti - egfrabs as a result of diverse inherent and acquired resistance mechanisms.3 amplification in the her2 ( human epidermal growth factor receptor 2 ) gene ( also known as erbb2 ) is one such mechanisher2 amplification has been implicated in therapeutic resistance to anti - egfrab therapy in preclinical studies in mcrc.4 , 5 aberrant her2 signaling results in bypass activation of the ras - mek - erk signaling pathway , thereby blunting the effect of egfr blockade.4 although the clinical significance and therapeutic potential of her2 amplification is well established in breast and gastric cancer , its characterization in mcrc remains deficient . 
her2 amplification is seen in a small subset of mcrc , predominantly in kras wildtype tumors , for which anti - egfrabs are used as targeted therapies.6 , 7 limited retrospective evidence shows that her2 amplification is associated with poor survival outcomes with anti - egfrabbased regimens.4 , 5 , 8 given the preliminary nature of these studies , these findings need additional clinical corroboration . accordingly , we systematically analyzed two distinct cohorts of patients with mcrc to validate the impact of her2 amplification on anti egfrabbased therapy . 
our in situ hybridization ( ish ) cohort ( cohort 1 ) included 98 sequential patients with ras / braf wild - type mcrc who were enrolled on a molecular screening program at the university of texas md anderson cancer center ( mdacc ; data supplement ) between august 2010 and june 2015 ( fig 1 ; data supplement ) .1 , 9 in this cohort , we identified 13 her2 - amplified and 85 her2 - nonamplified patients . 
among these patients , the 12 her2 amplified patients and 65 her2 - nonamplified patients who had received anti - egfrab in the secondor third - line setting after treatment on a nonanti - egfr regimen in the first - line setting were used for primary analyses ( fig 1 )  . 
 our next - generation sequencing ( ngs ) cohort ( cohort 2 ) comprised 16 patients with ras / braf wild - type mcrc with her2 amplification and 54 patients with ras / braf wild - type mcrc without her2 amplification who were identified by an ngs platform at mdacc and city of hope cancer center and had received prior treatment with anti - egfrabs in a second or third - line setting after treatment on a non anti - egfr regimen in the first - line setting , similar to cohort 1 ( fig 1 ; data supplement )  . 
 data on patient and tumor characteristics , treatment course , and vital status were collected from a prospectively maintained database and electronic medical records ( data supplement )  . the primary objective was to compare the efficacy of anti - egfrab therapy in the secondor third - line setting after treatment on prior therapy without anti - egfrab between patients with her2 - amplified and her2 - nonamplified mcrc . 
the choice of this specific line of therapy was based on practice patterns of treating mcrc ; anti - egfrab therapy is most commonly used as secondor third - line therapy.10 her2 amplification testing and interpretation pretreatment formalin - fixed paraffin - embedded archival tumor tissues were used for her2 testing . 
focal her2 amplification was defined as an her2 / cep17 ratio of 2.0 or greater , as per asco / college of american pathologists clinical practice guidelines for her2 testing in breast and gastric cancer ( data supplement ) .11 , 12 her2 amplification status in cohort 2 was determined with ngs . 
 a cohort 1 ( ish cohort ) cohort 2 ( ngs cohort ) patients with mcrc enrolled in attacc molecular prescreening protocol ( n = 747 ) systematic search of patients with mcrc who had ngs under clia excluded patients kras mutant nras mutant ras unknown braf mutant ( n = 489 ) ( n = 368 [ 49% ] ) ( n = 28 [ 4% ] ) ( n = 41 [ 6% ] ) ( n = 52 [ 7% ] ) patients excluded as a result of absence of necessary tissue for her2 dual ish evaluation ( n = 160 ) patients eligible for her2amp testing ( n = 258 ) ras / braf wild - type patients with successful her2amp testing ( n = 98 ) step 1 identification of patients step 2 identification of controls patients satisfying all of following criteria : her2 amp detected no ras mutations no braf mutation patients satisfying all of following criteria : no her2 amp detected no ras mutations no braf mutation patients were excluded if patients either had : not received any anti - egfr therapy received anti - egfr therapy in first - line setting her2 - amplified mcrc ( n = 13 ) her2 - nonamplified mcrc ( n = 85 ) patients : her2 - amplified mcrc ( n = 16 ) controls : her2 - nonamplified mcrc ( n = 54 ) anti - egfrbased therapy used in second or third - line setting * ( n = 12 ) ( n = 65 ) fig 1 . 
the analyses to determine the impact of her2 amplification ( her2amp ) on progression - free survival with antiepidermal growth factor receptor ( egfr ) therapy was tested in two independent cohorts of patients with metastatic colorectal cancer ( mcrc )  . 
 ( a ) cohort 1 consisted of patients with ras / braf wild - type mcrc with adequate tissue available for her2 testing using dual in situ hybridization ( ish )  . 
 ( b ) cohort 2 consisted of patients with ras / braf wild - type mcrc with her2amp detected on next - generation sequencing ( ngs ) and matched controls with her2 - nonamplified tumors who underwent similar sequencing and were treated with an anti - egfr therapy regimen in a similar setting . 
at time of database lock , 21 patients had received either no anti - egfr therapy ( n = 20 ) or anti - egfrbased therapy in the first - line setting ( n = 1 )  . 
attacc , assessment of targeted therapies against colorectal cancer ; clia , clinical laboratory improvement amendments ; pep , primary end point . using the hybrid capturebased foundationone assay ( data supplement ) .14 all testing was performed in clinical laboratory improvement amendmentscertified laboratories . statistical analysis the primary end point was progression - free survival ( pfs ) in patients treated with anti egfrabbased therapy in the secondor thirdline setting . 
to ascertain the predictive value of her2 amplification , we then compared the pfs of these patients on a regimen devoid of anti egfrabs ( nonanti - egfrabbased regimen in first - line setting )  . 
we also performed additional analyses to ascertain whether the reduction in pfs in her2 - amplified patients is exclusively a result of rapid progression on treatment with anti - egfrabs or whether these patients are rapid progressors irrespective of type of therapy by using the pfs ratio ( ratio of pfs on antiegfrbased therapy in secondor third - line setting to pfs on nonanti - egfr regimen in first - line setting )  . 
key secondary end points were overall survival and time to treatment failure ( defined as time from start of treatment to discontinuation of treatment for any reason or death )  . 
baseline characteristics and treatment variables were well balanced between cohorts 1 and 2 ( data supplement ) and between her2 - amplified and nonamplified subsets in both cohorts ( table 1 )  . 
in cohort 1 , cetuximab was the most commonly administered anti - egfr agent ( 88% of patients ) , and irinotecan was the most common cytotoxic chemotherapy backbone ( 88% ) used with anti - egfrabs . 
likewise , in cohort 2 , cetuximab and an irinotecan - based regimen were used in 79% and 87% of patients , respectively . her2 amplification and pfs on treatment with anti - egfrabbased therapy to evaluate the impact of her2 amplification on efficacy of anti - egfrabs , we first compared pfs of her2 - amplified and her2 - nonamplified patients receiving these agents in the secondor third - line setting . 
in both ( a ) cohort 1 and ( b ) cohort 2 , her2amp was associated with shorter median pfs ( mpfs ) on anti epidermal growth factor receptor ( egfr ) antibody ( anti - egfrab ) therapy compared with the her2 - nonamplified ( her2na ) group . 
in contrast , there was no difference in mpfs on therapy devoid of anti - egfrabs between her2amp and her2na groups in both ( c ) cohort 1 and ( d ) cohort 2 . 
 ( e and f ) in addition , the pfs ratio ( ratio of pfs on anti - egfrab therapy [ pfs2 ] to pfs on nonanti - egfrab therapy [ pfs1 ] ) for individual patients is lower for her2amp patients compared with her2na patients . 
the direction and magnitude of differences between her2 - amplified and nonamplified patients on anti - egfrab and non anti - egfrab therapy were comparable to the previously presented results in both cohorts ( data supplement )  . 
 is a pivotal step in refining the risk - benefit profile of anti - egfrabs and toward the eventual goal of true personalized therapy in mcrc . this clinical analysis was performed to determine the role of her2 amplification as a predictive biomarker . 
using two distinct cohorts , we showed that when patients with ras wild - type mcrc are treated with anti - egfrabbased regimens , the pfs of her2 - amplified patients is significantly shorter ( less than 3 months ) compared with the pfs of her2 - nonamplified patients ( 8 to 9 months )  . in addition to corroborating our findings in two independent cohorts , our complementary analysis helped to assess the predictive nature of this finding in the absence of an observation or placebo arm.15 the precept underlying this approach was that if the poor pfs seen with anti egfrabbased regimen is a result of poor prognostic impact of her2 amplification , then we would expect a similar lower pfs in these her2 amplified patients irrespective of type of therapy.16 however , we found that the pfs of these patients on therapy devoid of anti - egfrabs was similar to that of her2 - nonamplified patients . 
 we also found that the ratio of pfs on antiegfr therapy to pfs on nonanti - egfr therapy in her2 - amplified patients was lower , indicating that her2 - amplified patients had relatively better pfs on nonanti - egfr therapy . 
thus , we demonstrated that poorer survival found in her2 - amplified patients compared with her2 - nonamplified patients was uniquely associated with anti - egfr therapy ( data supplement ) .1 our findings are comparable to and confirm other smaller series reported in literature . 
our study included two independent groups , and in addition , our analysis uniquely explored the predictive value of her2 amplification by comparing the effect of her2 amplification on nonanti - egfrab therapy . 
preclinical data have shown that activating genetic aberrations in her2 overcome efficacy of anti - egfrabs by either bypassing egfr signaling and activating pi3k / akt / mtor and ras / raf / mapk cascade or by heterodimerization with egfr.18 using a large xenograft cohort derived from patients with mcrc ( n = 85 ) , bertotti et al5 showed that her2 amplifications were enriched in a subset of cetuximab - resistant , kras / nras / braf / pik3ca wild - type patients and caused resistance to anti egfrab therapy . 
together , these robust preclinical and clinical data strengthen the hypothesis that her2 amplifications are negative predictors of response to anti - egfr therapy.4 , 5 the prevalence of her2 amplifications and the appropriate setting and optimal methodology for testing are critical concerns moving forward . 
we performed her2 amplification analyses in cohort 1 using dual ish , as was done in the her2 amplification for colorectal cancer enhanced stratification ( heracles ) study ( fig 3 ) .22 in cohort 2 , ngs was used for her2 amplification determination , as was done in the my pathway study.21 our analysis shows comparable impact of her2 amplification on pfs with anti - egfr therapy , irrespective of the methodology used . 
representative photomicrographs of colorectal cancer ( crc ) samples with ( a ) her2 protein expression using immunohistochemistry ( ihc ; scores of 0 , 1 + , 2 + , and 3 + ) and ( b ) her2amp using dual in situ hybridization ( ish ; gene status expressed as her2 / cep17 ratio )  . 
 additional studies in colon cancer are needed for cross - validation of these methodologies to assess concordance between ish and ngs and to determine the optimal platform ; however , both platforms supported similar findings of predictive impact in our study . the discovery of her2 amplification in a patient with mcrc has implications beyond identification of a negative predictive factor . 
 unlike patients with ras - mutant tumors where we struggle from the lack of therapies that target the ras pathway , myriad agents ( eg , trastuzumab , lapatinib , pertuzumab , trastuzumab emtansine , neratinib ) that target her2 exist . 
 these have shown favorable clinical activity in her2 - amplified tumor types such as breast cancer and gastric cancer.24 - 27 her2 - amplified patient - derived xenografts resistant to cetuximab show rapid and dramatic tumor shrinkage with dual anti - her2 inhibition by combination therapy with pertuzumab and lapatinib.5 in line with these preclinical findings , two distinct proof - of - concept , single - arm , phase ii studies using dual anti - her2 targeting in patients with her2 - amplified refractory mcrc have shown promising preliminary results . 
however , given the lack of major differences between the her2 - amplified and nonamplified patients , the relatively large size of this cohort of a rare subset of mcrc , the strength of the observed effect , and the clear imitation in a second independent data set , this study indicates strong evidence for this predictive effect . 
additional study of her2 amplifications in tissue specimens from randomized prospective cohorts such as the swog 80405 trial may provide a higher level of validation , although the low prevalence of this biomarker makes this challenging . 
despite these limitations , we consider these findings to be representative of this subset of patients with mcrc , and although not definitive , the findings strongly indicate that her2 amplification is a negative determinant of response to anti - egfrabbased therapy in mcrc . 
we propose that although the level of evidence is insufficient to completely forego therapy with anti - egfrabs in these patients , the limited benefit with these agents in this population argues in favor of using her2 testing for facilitating anti - egfr treatment decision making and for clinical trial actionability . her2 amplification is not the only resistance mechanism to anti - egfr therapy . 
 loree , david menter , shalini singh , riham katkhuda , kandavel shanmugam , scott kopetz administrative support : david menter provision of study materials or patients : michael j . 
shaw , riham katkhuda , dipen maru , marwan fakih , scott kopetz studies have implicated other alterations , such as her2 mutations and met amplification , in this resistance.29 , 30 emerging data have also shown that acquired resistance as a result of her2 amplifications occurs in a small subset of patients ( three [ 14% ] of 22 patients ) .31 follow - up studies are necessary to assess the role of these acquired her2 amplifications in resistance to anti - egfrabs . 
activation as measured by phosphoher2 and downstream effector pik3 / akt pathway in amplified tumors and in tumors where it occurs independent of amplification ( data supplement ) may predict response to her2 - targeted therapies , as is the case with breast cancer.32 , 33 in conclusion , her2 amplifications predict a lack of response to anti - egfrab therapy in patients with mcrc . 
early integration of her2 testing for patients with ras / braf wild - type mcrc can allow for a more informed discussion with patients regarding risks and benefit of anti - egfrabs , adding a layer of personalization to therapy in this subset of patients with mcrc . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . kanwal raghav consulting or advisory role : genentech ( inst ) , bayer ( inst ) travel , accommodations , expenses : tracon pharma jonathan m . 
overman consulting or advisory role : bristol - myers squibb , genentech , gritstone oncology , medimmune research funding : bristol - myers squibb , merck , roche , medimmune ruoxi yu no relationship to disclose funda meric - bernstam honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inflection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pfizer , effector therapeutics , abbvie , boehringer ingelheim ( i ) , guardant health ( inst ) david menter no relationship to disclose krittiya korphaisarn no relationship to disclose brian kee stock and other ownership interests : medtronic stock and other ownership interests : roche patents , royalties , other intellectual property : roche travel , accommodations , expenses : roche shalini singh employment : ventana medical systems stock and other ownership interests : ventana medical systems patents , royalties , other intellectual property : method of identifying treatment - responsive nonsmall - cell lung cancer using alk as a marker ( inst ) mark routbort no relationship to disclose ken chen no relationship to disclose kenna r.m. 
shaw no relationship to disclose riham katkhuda no relationship to disclose kandavel shanmugam employment : ventana medical systems stock and other ownership interests : roche patents , royalties , other intellectual property : patents ( inst ) travel , accommodations , expenses : ventana medical systems dipen maru no relationship to disclose marwan fakih consulting or advisory role : amgen , array biopharma , genentech speakers ' bureau : amgen , taiho pharmaceutical research funding : novartis ( inst ) , amgen ( inst ) , astrazeneca ( inst ) scott kopetz stock and other ownership interests : molecularmatch , navire pharma consulting or advisory role : roche , genentech , emd serono , merck , karyopharm therapeutics , amal therapeutics , navire pharma , symphogen , holy stone , biocartis , amal therapeutics , amgen , novartis research funding : amgen ( inst ) , sanofi ( inst ) , biocartis ( inst ) , guardant health ( inst ) , array biopharma ( inst ) , genentech ( inst ) , emd serono ( inst ) , medimmune ( inst ) , novartis ( inst ) affiliations kanwal raghav , jonathan m . 
allegra cj , rumble rb , hamilton sr , et al : extended ras gene mutation testing in metastatic colorectal carcinoma to predict response to anti - epidermal growth factor receptor monoclonal antibody therapy : american society of clinical oncology provisional clinical opinion update 2015 . 
misale s , di nicolantonio f , sartore - bianchi a , et al : resistance to anti - egfr therapy in colorectal cancer : from heterogeneity to convergent evolution . 
bertotti a , migliardi g , galimi f , et al : a molecularly annotated platform of patient - derived xenografts ( xenopatients ) identifies her2 as an effective therapeutic target in cetuximabresistant colorectal cancer . 
richman sd , southward k , chambers p , et al : her2 overexpression and amplification as a potential therapeutic target in colorectal cancer : analysis of 3256 patients enrolled in the quasar , focus and piccolo colorectal cancer trials . 
martin v , landi l , molinari f , et al : her2 gene copy number status may influence clinical efficacy to anti - egfr monoclonal antibodies in metastatic colorectal cancer patients . 
overman mj , morris v , kee b , et al : utility of a molecular prescreening program in advanced colorectal cancer for enrollment on biomarker - selected clinical trials . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
bartley an , washington mk , ventura cb , et al : her2 testing and clinical decision making in gastroesophageal adenocarcinoma : guideline from the college of american pathologists , american society for clinical pathology , and american society of clinical oncology . 
jeong jh , kim j , hong ys , et al : her2 amplification and cetuximab efficacy in patients with metastatic colorectal cancer harboring wild - type ras and braf . 
hurwitz h , raghav kps , burris ha , et al : pertuzumab + trastuzumab for her2 - amplified / overexpressed metastatic colorectal cancer ( mcrc ) : interim data from mypathway . 
ross ds , zehir a , cheng dt , et al : next - generation assessment of erbb2 ( human epidermal growth factor receptor 2 ) amplification status : clinical validation in the context of a hybrid capture - based , comprehensive solid tumor genomic profiling assay . 
bang yj , van cutsem e , feyereislova a , et al : trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of her2 - positive advanced gastric or gastrooesophageal junction cancer ( toga ) : a phase 3 , open - label , randomised controlled trial . 
sartore - bianchi a , trusolino l , martino c , et al : dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - of - concept , multicentre , open - label , phase 2 trial . 
raghav k , morris v , tang c , et al : met amplification in metastatic colorectal cancer : an acquired response to egfr inhibition , not a de novo phenomenon . 
wulfkuhle jd , yau c , wolf dm , et al : evaluation of the her / pi3k / akt family signaling network as a predictive biomarker of pathologic complete response for patients with breast cancer treated with neratinib in the i - spy 2 trial . 
pathologic examination showed a 2.9 - cm collecting duct carcinoma ( cdc ) with metastases in eight of 15 resected hilar , suprahilar , and periaortic lymph nodes . after surgery , the patient was initiated on therapy with cisplatin and gemcitabine on a dosing schedule of once every 3 weeks . 
cytologic examination of pleural fluid retrieved during thoracentesis confirmed malignant pleural effusions . given the absence of any standard second - line treatment of cdc , comprehensive genomic profiling ( cgp ) was performed using a commercially available assay in a clinical laboratory improvement amendmentscertified , college of american pathologistsaccredited laboratory ( foundation medicine ; cambridge , ma )  . 
formalin - fixed paraffin - embedded tumor derived from the original nephrectomy specimen was analyzed by hybridization capture of all coding exons from 315 cancerrelated genes and select introns of 28 genes commonly rearranged in cancer . 
sequencing and bioinformatics methods for characterization of genomic alterations ( ga ) have previously been described in detail.1 the sole ga observed in this case was homozygous deletion of cdkn2a / b . 
multiple variants of unknown significance were identiincluding bard1 ( p358_s364del ) , brip1 fied , ( r264w ) , crlf2 ( e213k ) , dicer1 ( v594i ) , fgf6 ( n113k ) , igf1r ( p190s ) , mll2 ( r1292c ) , notch1 ( v1232m ) , pdgfrb ( s408c ) , ros1 ( e401k ) , socs1 ( a44_v45insvp ) , and tet2 ( e1405q )  . 
cdkn2a alteration has been suggested to be a potential predictive biomarker for cdk4 / 6 inhibitors.2 , 3 in light of loss of cdkn2a / b , the patient was offered therapy with the cdk4 / 6 inhibitor palbociclib . 
chung , foundation medicine , cambridge ; and toni k . choueiri , dana - farber cancer institute / brigham and womens cancer center , boston , ma corresponding author : sumanta k . 
the genomic landscape of cdc was defined in a previous report from our group.11 potential biomarkers for response to cdk4 / 6 inhibitors such as palbociclib include alterations in genes involved in the regulation of cdk4 / 6cyclin d kinase complexes , 2 , 3 such as cdk4 amplification , and palbociclib has demonstrated encouraging activity in phase 2 studies of patients with liposarcoma who harbor this driver.12 , 13 although preclinical studies of cell lines from multiple cancer types , including rcc , have reported that cdkn2a / p16ink4a loss of function is associated with sensitivity to cdk4 / 6 inhibitors , 14 - 18 there is limited clinical evidence supporting cdkn2a as a predictive biomarker , with one case study reporting that a patient with uterine leiomyosarcoma harboring cdkn2a homozygous deletion and a concurrent nf2 mutation experienced 4 months of stable disease on palbociclib treatment . in contrast , for patients with advanced breast cancer , for which palbociclib is approved with either letrozole or fulvestrant , cdkn2a loss ( assessed by fluorescent in situ hybridization ) was not associated with further benefit from palbociclib in combination with letrozole , in the palbociclib ongoing trials in the management of breast cancer ( paloma ) - 1 trial for patients with er + / her22 breast cancer.19 similarly , in a basket trial of the cdk4 / 6 inhibitor ribociclib , no responses were observed among the 73 patients with cancer whose tumor harbored a cdkn2a ga , as assessed by cgp.20 in this context and that of limited single - agent efficacy of cdk4 / 6 inhibitors in unselected populations , 19 , 20 the partial response to palbociclib experienced here by a patient with metastatic refractory cdc harboring cdkn2a / b homozygous deletion is unusual . 
in a series of 17 patients with cdc assessed by cgp , the most frequently identified gas were in nf2 ( 29% ) , setd2 ( 24% ) , smarcb1 ( 18% ) , and cdkn2a / b ( 12% , including homozygous deletion and mutation )  . 
characteristics for cases with cdkn2a or cdkn2a / b homozygous deletion characteristic total cases , no . total cases with cdkn2a or cdkn2a / b homozygous deletion , no . cases with cdkn2a or cdkn2a / b homozygous deletion and no co - occurring alteration , no . characteristics of patients with cdkn2a or cdkn2a / b homozygous deletion and no co - occurring alteration female male age , years , median ( range ) median tumor mutational burden , no . 
cdkn2a ( or cdkn2a / b ) homozygous deletion was identified as the sole driver alteration in 1.2% ( 16 of 1 , 322 ) rcc cases and also in other disease types , including 15.2% of salivary gland acinic cell tumors , 14.3% of bone giant - cell tumors , and 11.3% of bone chordomas ( table 1 )  . 
it is conceivable , however , that some of these cases with cdkn2a homozygous deletion as the sole known ga may harbor concurrent driver alterations that have not yet been discovered . 
a larger subset of cases ( 16% ) had homozygous deletion of this locus as well as other gas in other genes ( table 1 ) , and additional cases had loss of heterozygosity of cdkn2a with the remaining allele mutated . 
more investigation is also required to understand how responses to cdk4 / 6 inhibitors for patients with cdkn2a alteration may be modulated by the presence or absence of different driver gene alterations . for patients with cdc , additional genomic profiling studies are needed , given the response to palbociclib observed in this study , which suggests that cdk4 / 6 inhibitors should be further explored for patients with cdkn2a - altered cdc . 
more broadly , this study identifies cdkn2a homozygous deletion as the sole known ga in a small subset ( 0.25% ) of advanced cancer cases and at higher frequency in specific tumor types ( table 1 )  . 
 patents , royalties , other intellectual property : patents via foundation medicine , seres health on microbiome research in non - neoplastic disease ( inst ) genentech , eisai , foundation medicine , cerulean pharma , astrazeneca , peloton therapeutics , exelixis , prometheus , alligent jeffrey ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine honoraria : pfizer , emd merck serono research funding : foundation medicine toni k . 
choueiri honoraria : national comprehensive cancer network , uptodate consulting or advisory role : pfizer , bayer , novartis , glaxosmithkline , merck , bristol - myers squibb , roche / research funding : pfizer ( inst ) , novartis ( inst ) , merck ( inst ) , exelixis ( inst ) , tracon pharma ( inst ) , glaxosmithkline ( inst ) , bristol - myers squibb ( inst ) , astrazeneca ( inst ) , peloton therapeutics ( inst ) , roche / genentech ( inst ) , celldex ( inst ) , agensys ( inst ) travel , accommodations , expenses : advisory boards / consultancy jon h . 
curr oncol 20 : e223 - e232 , 2013 von der maase h , hansen sw , roberts jt , et al : gemcitabine and cisplatin versus methotrexate , vinblastine , doxorubicin , and cisplatin in advanced or metastatic bladder cancer : results of a large , randomized , multinational , multicenter , phase iii study . 
miyake h , haraguchi t , takenaka a , et al : metastatic collecting duct carcinoma of the kidney responded to sunitinib . int j clin oncol 16 : 153 - 155 , 2011 10 . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
dickson ma , tap wd , keohan ml , et al : phase ii trial of the cdk4 inhibitor pd0332991 in patients with advanced cdk4 - amplified well - differentiated or dedifferentiated liposarcoma . 
logan je , mostofizadeh n , desai aj , et al : pd - 0332991 , a potent and selective inhibitor of cyclin - dependent kinase 4 / 6 , demonstrates inhibition of proliferation in renal cell carcinoma at nanomolar concentrations and molecular markers predict for sensitivity . 
young rj , waldeck k , martin c , et al : loss of cdkn2a expression is a frequent event in primary invasive melanoma and correlates with sensitivity to the cdk4 / 6 inhibitor pd0332991 in melanoma cell lines . 
finn rs , crown jp , lang i , et al : the cyclin - dependent kinase 4 / 6 inhibitor palbociclib in combination with letrozole versus letrozole alone as first - line treatment of oestrogen receptor - positive , her2 - negative , advanced breast cancer ( paloma - 1 / trio - 18 ) : a randomised phase 2 study . 
peguero ja , oneil bh , sohal d , et al : genomic mutation profiling ( gmp ) and clinical outcome in patients ( pts ) treated with ribociclib ( cdk4 / 6 inhibitor ) in the signature prograj clin oncol 34 , 2016 ( suppl ; abstr 2528 ) 21 . 
wang j , papanicolau - sengos a , chintala s , et al : collecting duct carcinoma of the kidney is associated with cdkn2a deletion and slc family gene up - regulation . 
 translating gene signatures into a pathologic feature : tumor necrosis predicts disease relapse in operable and stage i lung adenocarcinoma purpose the high 5 - year disease relapse rate in patients with stage i lung adenocarcinoma indicates the need for additional risk stratification parameters . 
this study assessed whether gene signatures translate into a pathologic feature for better disease stratification . materials and methods the mutual interdependence and risk stratification power of three gene signatures , cell cycle , hypoxia , and mammalian target of rapamycin ( mtor ) , were investigated in nine cohorts of patients with lung adenocarcinoma and five cohorts of patients with lung squamous cell carcinoma . 
the translation of signature score to pathway activity was further investigated by integrative analyses using the cancer genome atlas and the cancer protein atlas lung adenocarcinoma data sets . results the results showed that the three gene signatures were mutually interdependent in lung adenocarcinoma but not in lung squamous cell carcinoma . 
2018 by american society of clinical oncology introduction nonsmall - cell lung cancers ( nsclcs ) account for 85% of lung cancer cases and are the leading cause of cancer - related death worldwide.1 - 4 although a high proportion of nsclcs are diagnosed at advanced stages , the percentage of patients with early stage disease is increasing with the implementation of lung cancer screening programs.5 nevertheless , although surgical resection may increase the potential cure for patients with early stage disease , tumor recurrence is an almost inevitable outcome in reality , including those with stage i tumors . 
the 5 - year survival rate after potential curative resection is approximately 73% for stage ia and 58% for stage ib disease.6 current evidence shows that adjuvant chemotherapy is detrimental to patients with stage ia disease and is beneficial to patients with stage ib disease only among those with primary tumor size > 4 cm.7 - 9 despite numerous studies in the field of prognostic biomarkers for better patient stratification during the past decade , t stage remains the only available parameter . 
 the new - generation adjuvant trials are evaluating drugs beyond chemotherapy.10 advances in cancer genomics have led to the generation of several prognostic gene expression signatures.11 , 12 although these signature - based biomarkers represent a new milestone in lung cancer biomarker research , the sophisticated processing procedures limit their feasibility in clinical use . 
however , several retrospective clinicopathologic studies suggested that tumor necrosis serves as an additional stratification factor for stage i disease.13 - 16 nevertheless , somewhat discrepant results from these studies precluded the consensus for adopting tumor necrosis as an additional parameter . from the biologic aspect , tumor necrosis is the end result of dysregulated cell proliferation that occurs in a hypoxic tumor microenvironment poor with nutrient supply.17 depletion of intracellular atp levels switches apoptotic cell death to necrotic cell death.18 poly ( adp - ribose ) polymerase - 1 interacts with hypoxia - inducible factors , and its overactivation leads to a massive intracellular atp depletion that results in necrotic cell death.19 , 20 the mammalian target of rapamycin ( mtor ) kinase integrates signals from nutrients , growth factors , energy , and stress to regulate cell growth.18 autophagy is a cellular machinery that antagonizes necrotic cell death , and the mtor signaling pathway has been shown to promote necrotic cell death via suppression of autophagy.21 balance among apoptosis , necrosis , and autophagy determines the ultimate destiny of the cell.18 this study investigated the association between tumor necrosis and clinical prognosis of patients with lung adenocarcinoma as well as the association between tumor necrosis and three prognostic gene expression signatures in lung adenocarcinoma . 
the mutual interdependence of three gene signatures , representing cell cycle activity , tissue hypoxia , and nutrient balance , was assessed , as was the ability of these signatures to predict risk in patients with lung adenocarcinomas . 
 lung squamous cell carcinoma gene signatures were analyzed in four clinical cohorts : gse8894 , gse11969 , gse4573 , and tcga lung squamous cell carcinoma data sets ( data supplement )  . 
the tcga data set was downloaded from the tcga web site , and other data sets were downloaded from the gene expression omnibus database.22 the reverse phase protein array data of lung adenocarcinoma data sets were downloaded from the cancer protein atlas ( tcpa ) web site.23 determination of gene signatures three gene signatures , the cell - cycle , hypoxia , and mtor signatures , were used in this study . 
 the cell - cycle signature is composed of genes whose expression levels were altered during synchronized cell cycle phase.24 the hypoxia signature consists of hif targeted genes identified as core responders to hypoxia.25 the mtor signature consists of genes downregulated after rapamycin treatment of human bjab lymphoma cells.26 , 27 the genes involved in these three signatures are listed in the data supplement . 
the r values derived then served as the null distribution for evaluating the significance of our observation . statistical analysis differences in signature scores between two groups , such as normal and tumor samples , were estimated by t tests . 
the results were considered statistically significant when two - tailed p values were < .05. results three mutually interdependent gene signatures active in operable lung adenocarcinomas bearing areas of necrosis assessment of the gse11969 lung adenocarcinoma cohort showed that overall survival was significantly shorter in necrosis - positive than necrosis - negative tumors ( p = .04 ; fig 1a )  . 
three gene signatures , cell cycle , hypoxia , and mtor , were selected to estimate the activities of three corresponding processes in tumor biology : cell proliferation , tissue hypoxia , and nutrient balance , respectively . 
evaluation of the gse11969 cohort showed that each gene signature possessed significantly higher activity in necrosis - positive than in necrosis - negative tumors ( p < .001 each ; fig 1a ) and was predictive of the presence of necrosis ( area under the curve > 0.7 each ; data supplement )  . 
each of these three gene signatures also showed higher activities in the sample containing tumor cells than in adjacent normal areas ( p < .001 each ; data supplement )  . to determine whether these three gene signatures were mutually interdependent , they were evaluated in six clinical cohorts : the shedden cohort , gse8894 , gse31210 , gse20853 , gse13213 , and gse11969 . 
these results showed that the three gene signatures were mutually interdependent and possessed higher activities in necrosis - positive than necrosis - negative operable lung adenocarcinomas . three gene signatures stratify patients with operable lung adenocarcinoma into different risk groups we next investigated whether the three interdependent gene signatures correlated with overall or relapse - free survival in patients with operable lung adenocarcinoma . 
five data sets , the shedden cohort of michigan , gse8894 of korea , gse11969 , gse31210 , and gse13213 of japan , were included in univariable cox regression analysis . 
for every gene signature selected , the signature activity was positively associated with shorter overall ( the shedden cohort , gse11969 , and gse13213 ) or relapse - free ( gse8894 and gse31210 ) survival in almost all study cohorts ( data supplement )  . 
these cohorts , the shedden cohort ( n = 442 ) and the gse11969 , gse31210 , and gse13213 cohorts ( total n = 453 ) , included a total of 895 patients from both western and asian populations . 
the only exception was the hypoxia signature , with which the association did not reach statistical significance when it was applied to the gse11969 ( p = .31 ) and gse13213 ( p = .09 ) cohorts ( table 1 )  . 
 however , the unit - weighted composite score derived from the hypoxic and mtor signatures predicted overall and relapse - free survival ( all p < .05 ) in all cohorts ( data supplement )  . in addition , the predictive power of these three gene signatures was independent of patient age and tumor stage , with gene signature tending to be a stronger predictor of overall survival than clinical stage ( table 1 )  . 
in the shedden cohort , for example , the three gene signatures stratified adenocarcinoma patients into two groups with different overall survival times on the basis of kaplan - meier survival analyses ( fig 2a )  . 
high signature activity was defined when the signature score was weighted in the upper half of the distribution , whereas low signature activity was defined when the signature score was weighted in the lower half of the distribution . 
stratification of stage ii and stage iii patients by signature activities showed that the survival curve of patients with stage ii and high activity almost overlapped with that of patients with stage iii and low activity . 
taken together , the results showed that the three gene signatures were significantly associated with overall and relapse - free survival in patients with operable lung adenocarcinoma , with predictive powers independent of and somewhat stronger than clinical stage . three gene signatures predict disease relapse in patients with stage i lung adenocarcinoma to determine whether the three gene signatures were associated with overall and relapsefree survival in patients with stage i disease , patients with stage i disease in the gse13213 cohort were examined . 
to further determine whether these gene signatures predicted relapse - free survival , the okayama cohort ( gse31210 ) , which includes 162 patients with stage i adenocarcinoma and information on clinical stage , age , and relapse - free survival , was evaluated by multivariable cox regression analysis . 
significant associations between signature scores and relapse - free survival time were observed , with similar results observed with all three gene signatures ( data supplement ; fig 3a )  . three gene signatures are indicative of pathologic tumor necrosis , which predicts disease relapse in patients with stage i lung adenocarcinoma a gene signature is composed of gene sets that react to biologic stimulation and is more representative of a biologic function than a single gene . 
the results showed that the signature score correlated with the expression level of the representative protein ( cell cycle versus cyclin b1 , hypoxia versus pai1 , and mtor versus mtor - ps2448 ) , which implicated the activity of each pathway ( data supplement ) .28 , 29 the biologic meanings of these signatures were found to converge into one pathologic feature , tumor necrosis . 
in the japanese gse11969 cohort , tumor necrosis was associated with shorter overall survival and higher signature activities . these findings were independently validated using the tcga lung adenocarcinoma data set . 
the three gene signatures were mutually interdependent and associated with overall and relapse - free survival in patients with operable and stage i lung adenocarcinomas ( data supplement )  . 
 ( a ) kaplan - meier survival analysis showing that tumor necrosis was associated with poor overall survival in the gse11969 cohort ( log - rank p = .04 , right upper panel )  . 
 ( b ) kaplan - meier analysis showing that stratification of patients with stage ii and stage iii disease by signature activities resulted in the survival curve of patients with stage ii disease with high activity almost overlapping with that of patients with stage iii disease with low activity . 
mtor , mammalian target of rapamycin . between mtor signature activity and relapsefree survival in patients with stage i disease , in which the differences did not reach statistical significance ( data supplement )  . compatible with what was observed in the gse11969 cohort , tumor necrosis was associated with higher signature activities ( p < .001 ; fig 3b ) and shorter overall as well as relapsefree survival ( p < .05 ; fig 3c )  . 
although signature activities were associated with the presence of necrosis , the signatures remained prognostic , even in patients with necrosis - negative tumors , indicating the prognostic value of the gene signatures by themselves ( data supplement )  . 
in addition , because the three gene signatures were interdependent and associated with the presence of necrosis , we further included a proliferative marker , the cyclin b1 , as a surrogate for ki - 67 in our multivariable cox regression analyses with the tcga and tcpa data sets . 
the independent validation results supported the role of tumor necrosis as the pathologic sum of the three gene signatures combined . three gene signatures are not interdependent or predictive of risk in lung squamous cell carcinoma adenocarcinoma and squamous cell carcinoma are both categorized as nsclcs and share the same tnm classification criteria . 
 ( c ) tumor necrosis predicts overall and relapse - free survival in patients with operable and stage i lung adenocarcinoma of tcga lung adenocarcinoma cohort . study showed that tumor size matters differently in these two cancer types.30 we therefore evaluated whether the three gene signatures play a role in squamous cell carcinoma similar to that in adenocarcinoma . 
assessment of four cohorts , the gse11969 , gse4573 , gse8894 , and tcga data sets , showed that the three gene signatures were no longer interdependent , with the only correlation between the cell - cycle and mtor signatures ( fig 4a )  . 
 ( c ) inability of the three gene signatures to predict overall survival in patients with lung squamous cell carcinoma . the three gene signatures were unable to stratify patients with squamous cell carcinoma into different risk groups in regard to overall survival ( fig 4c )  . 
these findings provide further evidence that lung adenocarcinoma and squamous cell carcinoma are two distinct disease entities with different biologic behavior . discussion proper risk stratification in patients with stage i lung adenocarcinoma is important for postoperative treatment strategy decisions , because it may influence the long - term outcome of patients . 
 in patients with stage ib disease with tumors > 4 cm.8 on the basis of these two studies , t stage seems to be the only available risk stratification parameter for stage i disease . ironically , approximately 30% to 50% of patients with stage i disease died as a result of disease relapse within 5 years after potential curative surgery.6 , 32 , 33 this fact indicates that a substantial percentage of stage i tumors are more aggressive than thought , which is compatible with the results obtained from the uracil - tegafur and calgb 9633 trials.8 , 31 the issue of how we can identify these high - risk individuals , for whom postoperative adjuvant therapy will do good more than bad , remains . 
genomically , the cell - cycle , hypoxia , and mtor signatures were found to be mutually interdependent , more active in necrosis - positive than necrosis negative tumors , and associated with overall and relapse - free survival independent of clinical stage . 
in contrast , the three gene signatures were no longer mutually interdependent and lost their risk stratification power in patients with lung squamous cell carcinoma . although genome - wide approaches have been used for risk stratification of biomarkers , the comprehensive process of gene signature derivation limits their clinical application . 
therefore , translation from sophisticated cancer genomics to corresponding pathologic features that can be applied in routine clinical practice would be especially important . although limited by its retrospective nature , this study showed that gene signatures could be translated into a pathologic feature . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . konan peck no relationship to disclose takashi takahashi no relationship to disclose pan - chyr yang honoraria : astrazeneca , novartis , merck , ono pharmaceutical speakers ' bureau : astrazeneca , roche , novartis , merck , ono pharmaceutical acknowledgment the authors thank the laboratory of takashi takahashi , md , phd , for preparing the information needed in analyzing data sets gse11969 and gse13213 . 
lozano r , naghavi m , foreman k , et al : global and regional mortality from 235 causes of death for 20 age groups in 1990 and 2010 : a systematic analysis for the global burden of disease study 2010 . 
morgensztern d , ng sh , gao f , et al : trends in stage distribution for patients with non - small cell lung cancer : a national cancer database survey . 
travis wd , brambilla e , noguchi m , et al : international association for the study of lung cancer / american thoracic society / european respiratory society international multidisciplinary classification of lung adenocarcinoma . 
goldstraw p , chansky k , crowley j , et al : the iaslc lung cancer staging project : proposals for revision of the tnm stage groupings in the forthcoming ( eighth ) edition of the tnm classification for lung cancer . 
pisters km , evans wk , azzoli cg , et al : cancer care ontario and american society of clinical oncology adjuvant chemotherapy and adjuvant radiation therapy for stages i - iiia resectable non small - cell lung cancer guideline . 
crin l , weder w , van meerbeeck j , et al : early stage and locally advanced ( non - metastatic ) non - small - cell lung cancer : esmo clinical practice guidelines for diagnosis , treatment and follow - up . 
shedden k , taylor jm , enkemann sa , et al : gene expression - based survival prediction in lung adenocarcinoma : a multi - site , blinded validation study . 
yoshizawa a , motoi n , riely gj , et al : impact of proposed iaslc / ats / ers classification of lung adenocarcinoma : prognostic subgroups and implications for further revision of staging based on analysis of 514 stage i cases . 
duhig ee , dettrick a , godbolt db , et al : mitosis trumps t stage and proposed international association for the study of lung cancer / american thoracic / european respiratory society classification for prognostic value in resected stage 1 lung adenocarcinoma . 
wu yt , tan hl , huang q , et al : activation of the pi3k - akt - mtor signaling pathway promotes necrotic cell death via suppression of autophagy . 
benita y , kikuchi h , smith ad , et al : an integrative genomics approach identifies hypoxia inducible factor - 1 ( hif - 1 ) - target genes that form the core response to hypoxia . 
ebi h , tomida s , takeuchi t , et al : relationship of deregulated signaling converging onto mtor with prognosis and classification of lung adenocarcinoma shown by two independent in silico analyses . 
liao h , hyman mc , lawrence da , et al : molecular regulation of the pai - 1 gene by hypoxia : contributions of egr - 1 , hif - 1alpha , and c / ebpalpha . 
sawabata n , asamura h , goya t , et al : japanese lung cancer registry study : first prospective enrollment of a large number of surgical and nonsurgical cases in 2002 . 
 multigene hereditary cancer panels reveal high - risk pancreatic cancer susceptibility genes purpose the relevance of inherited pathogenic mutations in cancer predisposition genes in pancreatic cancer is not well understood . 
we aimed to assess the characteristics of patients with pancreatic cancer referred for hereditary cancer genetic testing and to estimate the risk of pancreatic cancer associated with mutations in panel - based cancer predisposition genes in this high - risk population . methods patients with pancreatic cancer ( n = 1 , 652 ) were identified from a 140 , 000 patient cohort undergoing multigene panel testing of predisposition genes between march 2012 and june 2016 . 
gene - level mutation frequencies relative to exome aggregation consortium and genome aggregation database reference controls were assessed . results the frequency of germline cancer predisposition gene mutations among patients with pancreatic cancer was 20.73%. 
mutations in atm , brca2 , cdkn2a , msh2 , msh6 , palb2 , and tp53 were associated with high pancreatic cancer risk ( odds ratio , > 5 ) , and mutations in brca1 were associated with moderate risk ( odds ratio , > 2 )  . 
in a logistic regression model adjusted for age at diagnosis and family history of cancer , atm and brca2 mutations were associated with personal history of breast or pancreatic cancer , whereas palb2 mutations were associated with family history of breast or pancreatic cancer . conclusion these findings provide insight into the spectrum of mutations expected in patients with pancreatic cancer referred for cancer predisposition testing . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction pancreatic cancer ( pc ) is the fourth most common cause of death resulting from cancer in the united states.1 epidemiologic studies have suggested that 10% to 20% of pcs are associated with an inherited component , with familial pc , defined as kindreds containing at least two affected first - degree relatives , as an established entity of inherited disease.2 pc is a component of hereditary breast - ovarian cancer syndrome , 3 , 4 lynch syndrome , 5 , 6 familial adenomatous polyposis , 7 familial atypical multiple mole melanoma syndrome , 8 hereditary pancreatitis , 9 peutz - jeghers syndrome , 10 and li - fraumeni syndrome.11 recent studies involving familial pc kindreds have further characterized the role of brca1 / 2 , cdkn2a , atm , and palb2 in pc susceptibility.12 - 14 until recently , germline studies of pcs have focused on single cancer predisposition genes.15 , 16 the first panel - based study of 13 cancer predisposition genes among patients with pc identified 11 mutations ( 3.8% ) in atm , brca1 / 2 , mlh1 , msh2 , msh6 , and tp53 , 17 whereas a 22 - gene panelbased study identified atm , brca1 / 2 , chek2 , and palb2 mutations in 13% of 96 sequentially collected pcs.18 a majority of these mutations were identified in pcs with a family history of pancreatic , breast , ovarian , or colorectal cancer , suggesting that a better understanding of pc risk will depend on evaluation of families with broad constellations of tumors.18 more recently , panel - based approaches identified germline chunling hu holly laduca hermela shimelis eric c . 
 mutations in 4% ( 33 of 854 ) of patients with apparently sporadic pc19 and in 25% ( 44 of 176 ) of patients with advanced pc.20 here , we report results from panel - based clinical testing of 1 , 652 patients with pc from a large cohort of > 140 , 000 patients evaluated by a single diagnostic laboratory and calculate gene - specific risks of pc by comparison with exome aggregation consortium ( exac ) and genome aggregation database ( gnomad ) reference controls.21 , 22 methods study population patients with pc ( n = 1 , 819 ) were identified from a large cohort of > 140 , 000 patients undergoing multigene panel testing of seven to 49 cancer predisposition genes between march 2012 and june 2016 at ambry genetics23 ( aliso viejo , ca ; appendix table a1 )  . 
exclusion criteria , including the presence of neuroendocrine tumors or intraductal papillary mucinous neoplasms , reduced the number of patients for analysis ( n = 1 , 652 ; appendix )  . 
 the study was approved by the western institutional review board . multigene panel testing mutation testing was performed by sequencing of targeted custom capture products from several multigene panels and targeted chromosomal microarray analysis , as previously described.24 genomic dna was isolated from each patients blood or saliva specimen using a standardized methodology ( qiagen , valencia , ca )  . 
sequence enrichment was performed by incorporating the genomic dna into microfluidics chip or microdroplets along with primer pairs or by a bait - capture methodology using long biotinylated oligonucleotide probes ( raindance technologies , billerica , ma ; integrated dna technologies , san diego , ca ) , followed by polymerase chain reaction and then next - generation sequencing analysis ( illumina , san diego , ca ) of all coding exons plus at least five bases into the 5 and 3 ends of all the introns and untranslated regions . 
all mutations identified by ambry genetics are submitted to the clinvar public database . statistical methods the observed frequency of all pathogenic mutations within each gene in white patients with pc was compared with the frequency of pathogenic mutations in the exac non - finnish european ( nfe ) nonthe cancer genome atlas ( tcga ) reference control after data cleaning and filtering ( appendix ) as previously described.23 copy number variants in all genes and mutations in pseudogene homology regions ( pms2 exons 9 and 11 to 15 ) were excluded from cases and controls for risk estimation , because these alterations were not individually validated in exac or gnomad controls . 
although these gnomad controls partially overlap with exac nfe non - tcga controls , the substantially increased number along with updated variant calling algorithms identified gnomad as an independent reference control data set . 
 ( % ) patients of all ethnicities ( n = 1 , 652 ) white patients ( n = 1 , 256 ) age at pc diagnosis were evaluated using the kolmogorov - smirnov test . 
 compared with a median age at pc diagnosis of 70 years in surveillance , epidemiology , and end results registries between 2010 and 2014 , 26 the median age at diagnosis was 63 years among patients with pc . 
among white patients with pc , 38.1% had a firstor second - degree relative with pc , and 48.8% had a family history of breast cancer ( table 1 )  . 
similar frequencies were observed for patients with pc of all races and ethnicities . pathogenic mutations among patients with pc the combined frequency of mutations in genes from all hereditary cancer testing panels was 20.73% for patients with pc of any race or ethnicity and 21.12% for white patients ( appendix table a2 )  . 
brca2 was the most frequently mutated predisposition gene ( 4.64% ) among patients diagnosed at age 63 years , and atm was most frequently mutated ( 4.03% ) in patients with pc diagnosed at age > 63 years ( appendix table a4 )  . 
association analyses using gnomad reference controls confirmed all significant associations , and gene - specific risk estimates were highly similar , except for slightly attenuated risk for palb2 mutations and increased risk for tp53 ( appendix table a6 )  . the same genes were associated with increased pc risk when considering patients of all races and ethnicities compared with exac all race and ethnicity controls ( appendix table a7 ) and after excluding those who had previously tested negative for brca1 / 2 mutations before panel testing ( appendix table a8 )  . 
risk estimates for most genes were slightly diminished when including only those patients with pc for whom pc was the first cancer diagnosis , although msh2 and tp53 mutations were no longer significantly associated with moderate risk of pc because of the decreased number of mutations in patients with pc , and the modest or associated with chek2 was marginally significant ( appendix table a9 )  . 
in contrast , analyses using only exac nfe non - tcga variants in the high - quality pass category marginally increased the ors for each gene ( appendix table a10 )  . 
mutations in atm , brca2 , and palb2 were also more frequent in patients with pc with a family history of breast cancer ( first or second - degree relative ; table 3 )  . 
in contrast , only palb2 and msh2 displayed a substantial increase in mutation frequency among patients with a family history of pc , and only chek2 , msh2 , and tp53 had increased frequencies of mutation among patients with pc with a family history of colorectal cancer ( table 3 )  . 
 family history of pc ( p = .029 ) or breast cancer ( p = .0056 ) and the association of chek2 mutations with family history of colorectal cancer ( p = .014 ; table 4 )  . performance of genetic testing criteria among mutation carriers consensus clinical genetic testing guidelines include pc as a component tumor for seven of the confirmed pc genes in this study ( brca1 / 2 , msh2 , msh6 , atm , palb2 , and cdkn2a ) .27 - 29 clinical histories of patients with mutations in these genes were evaluated to determine whether the respective genetic testing criteria were met ( table 5 )  . 
although a majority of brca1 / 2 and all msh2 mutation carriers displayed histories consistent with testing criteria , 50.0% of atm , cdkn2a , palb2 , and msh6 carriers met criteria . 
in addition , no cdkn2a families met diagnostic criteria for familial atypical multiple mole melanoma syndrome , 30 and 38.9% ( seven of 18 ) did not report any personal or family history of melanoma . discussion here we report a study of cancer predisposition gene mutations among patients with pc on the basis of a cohort of individuals undergoing hereditary cancer multigene panel testing from a single clinical laboratory . 
results from case control studies of the pc cases and exac reference controls identified six genes associated with high risk ( or , > 5 ) of pc ( atm , brca2 , cdkn2a , msh6 , palb2 , and tp53 ) , consistent with previous smaller studies and segregation studies from pc families . 
msh2 was also associated with a high risk of pc ; however , additional studies are needed to confirm these findings , because this association was based on a limited number of mutations detected among pc cases . 
 here we show that brca1 mutations are associated with a moderate risk ( or , > 2 ) of pc , even in a series of sensitivity analyses accounting for potential modifying effects of other cancers . 
 chek2 mutations were also associated with a moderate risk of pc ; however , this association was either diminished ( or , < 2 ) or nonsignificant in several sensitivity analyses . 
one likely explanation is that stk11 mutations are unlikely to occur in the absence of pathognomonic clinical characteristics associated with peutz - jeghers syndrome , and therefore , patients with suspected peutz - jeghers syndrome may be referred for single - gene testing more often than multigene testing . 
pathogenic mutations in other panel genes were still sufficiently uncommon to allow assessment of associations with risk ( eg , apc , mlh1 )  . the risk estimates for pc associated with each of these established predisposition genes will help improve clinical pc risk assessment . 
for some genes , these results offer more precise estimates than previously reported , whereas for others , such as palb2 and atm , we are the first to characterize the level of risk , to our knowledge . 
 it should be noted that the interpretation of the risks reported here is specific to patients referred for hereditary cancer genetic testing based on a personal or family history of cancer ( at least one diagnosis of pc in the family ) , and thus , these data may not be applicable to the general population or unselected pc cohorts . 
despite the enrichment for cases with personal or family history of cancer , these risks are derived from a broader clinical cancer testing cohort compared with previous studies selected for classic syndromic phenotypes such as fammm and therefore demonstrate that pc risk from syndromic genes remains high across a range of clinical histories . 
furthermore , this enrichment presented an opportunity to explore predictors of germline mutations . in total , 13% of patients had mutations in genes significantly associated with increased risk for pc across a range of sensitivity analyses ( atm , brca1 , brca2 , cdkn2a , msh6 , palb2 , and tp53 )  . 
family history of breast , pancreatic , or colorectal cancer was a significant predictor of positive results , suggesting that histories of these cancers should specifically be considered as genetic testing guidelines evolve for pc . 
the remaining 9% ( 15 of 173 ) of mutations were found in the approximately 65% of patients with pc without a family history of these cancers , suggesting a mutation rate of only 2.1% in white patients with pc without a family history of cancer ( 15 mutations in 698 ) in the clinically tested cohort . 
additional studies of population - based series of patients with pc are needed to determine whether clinical panel testing should be considered for patients with pc unselected for family history . in practice , patients with pc may not benefit directly from genetic testing because of the high mortality rate for this cancer . 
however , knowledge of mutation status for genes such as brca1 / 2 and palb2 with respect to clinical trial eligibility for targeted agents such as poly ( adp - ribose ) polymerase inhibitors may make genetic testing more appealing . 
in addition , mutation - positive family members can significantly benefit from knowledge of increased risk for a variety of cancers , including pc , and mutation - negative family members can also adjust their cancer screening protocols accordingly . 
in addition , the international cancer of the pancreas screening consortium and the american college of gastroenterology 29 , 31 recommend that pc surveillance , including annual endoscopic ultrasound and / or magnetic resonance imaging , be considered for individuals with > 5% lifetime or relative risk for pc . 
in addition , although brca1 mutation carriers with a firstor second - degree relative with pc are included in the list of patients for whom pc screening should be considered , the moderate pc risk categorization for brca1 in this study suggests this may not be clinically indicated . exac nfe non - tcga controls were used in this study because of the lack of a large series of matched controls . 
although the use of large reference data sets is not ideal , the large sample size allows precise estimation of the frequency of mutations in individuals without cancer and is likely reflective of the general population . 
in addition , we applied many data cleaning steps and used consistent criteria for selection of mutations in the clinical cohort of patients with pc and the exac controls to ensure that the data sets were adequately normalized for case - control association analyses . 
in a recent assessment of the quality of clinical history information for patients undergoing hereditary cancer panel testing , pedigrees and / or clinic notes were provided for 46% of randomly selected patient cases ( unpublished data )  . 
 when compared with pedigrees and clinic notes , a vast majority of proband cancers were reported completely ( 95% ) and accurately ( > 99% ) on test requisition forms . 
among family members , 76% of melanomas and > 80% of breast , ovarian , colorectal , endometrial , and pancreatic cancers were reported with 98% accuracy on test requisition forms . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . stock and other ownership interests : ambry genetics chunling hu no relationship to disclose holly laduca employment : ambry genetics hermela shimelis no relationship to disclose eric c . 
lee no relationship to disclose brigette tippin davis employment : ambry genetics stock and other ownership interests : ambry genetics research funding : ambry genetics ( inst ) travel , accommodations , expenses : ambry genetics mary helen black employment : ambry genetics research funding : ambry genetics travel , accommodations , expenses : ambry genetics tina pesaran employment : ambry genetics stock and other ownership interests : ambry genetics travel , accommodations , expenses : ambry genetics david e . 
rahib l , smith bd , aizenberg r , et al : projecting cancer incidence and deaths to 2030 : the unexpected burden of thyroid , liver , and pancreas cancers in the united states . 
risch ha , mclaughlin jr , cole de , et al : population brca1 and brca2 mutation frequencies and cancer penetrances : a kin - cohort study in ontario , canada . 
ruijs mw , verhoef s , rookus ma , et al : tp53 germline mutation testing in 180 families suspected of li - fraumeni syndrome : mutation detection rate and relative frequency of cancers in different familial phenotypes . 
mandelker d , zhang l , kemel y , et al : mutation detection in patients with advanced cancer by universal sequencing of cancer - related genes in tumor and normal dna vs guideline - based germline testing . 
laduca h , stuenkel aj , dolinsky js , et al : utilization of multigene panels in hereditary cancer predisposition testing : analysis of more than 2 , 000 patients . 
canto mi , harinck f , hruban rh , et al : international cancer of the pancreas screening ( caps ) consortium summit on the management of patients with increased risk for familial pancreatic cancer . 
 appendix patient cases of pancreatic cancer a total of 1 , 819 patients with pancreatic cancer were identified in a cohort of 140 , 449 individuals undergoing clinical germline cancer panel testing between march 2012 and june 2016 at a clinical testing laboratory ( ambry genetics , aliso viejo , ca )  . 
all variants classified by ambry were submitted to clinvar . exome aggregation consortium reference controls the exome aggregation consortium ( exac ) contains exome sequence data from 60 , 706 unrelated individuals sequenced as part of various disease - specific and population genetic studies . 
exclusion of sequence data from these patient cases yielded exac non - nfe non - tcga reference controls . genome aggregation database reference controls the genome aggregation database ( gnomad ) contains sequencing data of 123 , 136 exomes and 15 , 496 genomes from unrelated individuals sequenced as part of various disease - specific and population genetic studies . 
 gnomad data cleaning and filtering restricted to gnomad nfe exome data combined with gnomad ashkenazi jewish exome data . genomics viewer and by frequency in control data from dbsnp . pathogenic variant classification rules : same as in exac rules 1 to 8 . review variants with allele count 15 by integrative allele number was calculated as average of all variants within the coding region of a gene of interest . 
we previously reported our prospective experience of precision oncology in solid tumors , and here we report our longitudinal experience , focusing on therapeutic impact . patients and methods we conducted a retrospective review of 600 consecutive patients seen at cleveland clinic from 2013 to 2016 for treatment of incurable solid tumor malignancies for whom tumor genomic profiling was ordered using foundationone ( cambridge , ma )  . 
 after results , 313 patients ( 52.2% ) started any subsequent therapy ; of these , 95 ( 30% ; 15.8% overall ) received genomics - driven therapy ( g ) , and 218 ( 70% ) received non genomics - driven treatment ( ng )  . 
for the g versus ng group , the on - label , off - label , and clinical trial therapy breakdowns were 23% versus 88% , 47% versus 3% , and 30% versus 9% , respectively . 
more patients received treatment via clinical trials in the g cohort , and although not statistically significant , there was a trend toward increased os in the g ( v ng ) group . 
2018 by american society of clinical oncology introduction the sequencing of the human genome in the early 21st century ushered in the era of precision oncology , an era of tailoring anticancer treatments to individual patients by targeting the specific molecular alterations in their tumors.1 , 2 notable examples include pembrolizumab for microsatellite instability ( msi ) high tumors , vemurafenib for braf v600e alterations in melanoma , and olaparib for brca - positive ovarian cancer . 
however , clinical data supporting precision oncology in its broadest sense ( ie , applying these methods across a variety of solid tumors in large patient cohorts ) remain sparse . 
obstacles to generating real - world applications in precision oncology include small study populations , unclear distribution of biomarkers in various subsets , ethical considerations or treatment crossover , cost and availability of resources , and limitations in external validity . 
delays in accessing new treatments for our patients have also been a dilemma , frequently leading to off - label prescribing or use on compassionate grounds , which feed into the lack of available data . 
the study did not receive any external funding . patients and procedures all consecutive adult patients with a diagnosis of an incurable solid tumor malignancy who were seen at the cleveland clinic between january 1 , 2013 , and december 31 , 2016 , and underwent tumor genomic profiling were eligible for inclusion in this study . 
 briefly , this assay is capable of detecting any of the four classes of alterations in > 300 genes , including > 25 introns that are commonly altered in solid tumor malignancies . 
the assay has > 99% specificity , and results include msi and tumor mutational burden.4 all patients undergoing such testing are presented at our biweekly , multidisciplinary genomics tumor board ( gtb ) , composed of clinical oncologists , genetic counselors , pathologists , and patient care coordinators . 
next - generation sequencing ( ngs ) reports for each patient were reviewed comprehensively , and therapeutic treatment recommendations , made on the basis of reviewed literature , abstract presentations , and clinical trial availability , were discussed . 
all recommendations were documented in the electronic medical record system and were communicated directly to the treating oncologist . criteria for actionability of genomic alterations gtb considered an alteration to be actionable if one of the following criteria was met : ( 1 ) the target had a food and drug administration ( fda ) approved drug available for the specific tumor type ( on - label use ) , ( 2 ) the target had a drug approved by the fda for a different tumor type ( off - label use ) , or ( 3 ) the target had a drug available via clinical trial ( available at either the home institution or other institutions )  . 
when outside clinical trials were recommended , they were generally within approximately 200 miles of the patients primary residence . germline mutations predisposing patients to hereditary cancer syndromes and standardof - care alterations , such as her2 amplification , braf , alk fusions , or egfr mutations identified previously through routine testing for currently approved indications , were not considered to be actionable . 
however , if standard - of - care alterations had not been tested previously or the results of such testing performed at outside institutions were not available , then the gtb made appropriate on - label recommendations for such findings . study measurements clinical and pathologic information was acquired from electronic medical record review . 
demographics ( age , sex , ethnicity ) , date of diagnosis , location of primary malignancy , treatment history , gtb recommendations made on the basis of ngs results , treatment received after gtb recommendations were made , reason for non genomics - based treatment ( if known ) , date of last contact , and date of death ( if applicable ) were all collected . 
all data were entered into a secure electronic database for analysis . statistical analysis study data were collected and managed using redcap ( research electronic data capture ) tools hosted at cleveland clinic . 
overall survival ( os ) was calculated as time from date of gtb discussion of the case to either date of death or date of last contact ( the latter cases were censored for os calculation )  . 
 ( % ) unless indicated otherwise . 79% of patients had received two or more prior lines of therapy . on the basis of sequencing results , targeted therapy was recommended in 310 patients ( 51.7% ) , 95 of whom received more than one recommendation . 
of all gtb recommendations ( n = 405 ) , 32 ( 7.9% ) were for on - label treatment , 42 ( 10.4% ) were for off - label treatment , and 331 ( 81.7% ) were for clinical trials . 
for genomics - driven versus nongenomics - driven groups , the distributions of on - label , off - label , and clinical trial therapy received were 23% versus 88% , 47% versus 3% , and 30% versus 9% , respectively . 
the use of genomics - driven treat ment increased from 13% ( 29 of 223 ) in the first cohort ( reported earlier ) 3 to 18% ( 66 of 377 ) in the subsequent cohort . 
of note , of the 33 patients with cancer of unknown primary , the gtb was able to determine the primary origin in eight of these cases : three lung , two cholangiocarcinoma , and one each of colorectal , gastric , and pancreas . discussion this study represents one of the largest cohorts of patients with multiple types of incurable solid - tumor malignancies who had ngs performed to determine therapeutic options . 
 awareness and use of precision medicine ; and ( 5 ) although not statistically significant , there was a trend toward longer os in the genomics - driven versus nongenomics - driven treatment group ; however , this finding may also be related to unmeasured confounders . a review of the current literature indicated that a few other studies at various institutions have analyzed actionability and the percentage of patients who receive genomics - driven therapy . 
one such study was conducted at johns hopkins with 155 patients ; 85% of these patients received a treatment recommendation , and 24 ( 15% ) went on to receive genomics - driven therapy.5 although , in comparison , 51.7% of our cohort received recommendations , it is important to keep in mind our exclusion , in many cases , of germline mutations and alterations known to exist from standard - of - care testing in approved indications ( such as her2 in breast cancer )  . 
as in our findings , the researchers at johns hopkins commented on poor performance status being a limiting factor to clinical trial enrollment in addition to the unavailability of local trials . 
the md anderson cancer center reported on 2 , 000 patients who underwent ngs , of whom 789 ( 39% ) were found to have an actionable alteration and 83 ( 4.1% ) enrolled in genomics - driven trials.6 another study , of 1 , 932 patients with ngs testing , found that management was altered in 21% of patients ( 331 of 1 , 593 ) in need of a treatment change , as reported by the treating physicians.7 although our cohort was smaller , we were still able to find an increased percentage of patients who were provided with gtb recommendations and a similar , if not also increased , percentage of those receiving genomics - driven treatment . it is also important to note that the benchmark of precision oncology ( actionability ) is a fluid concept itself.8 it depends on the availability of clinical trials , locally , regionally , and nationally . 
 data on molecular markers and targeted therapy emerge rapidly , requiring up - to - date searches and algorithms to keep up with the literature.9 as more evidence accumulates and drugs receive regulatory approval , off - label use may shift to on label . 
for example , our data set predates the blanket approval of pembrolizumab for msi high or mismatch repair deficient tumors ; msi results on ngs are now increasingly being used to determine the use of immune checkpoint inhibitors , which is likely to increase the proportion of patients receiving genomics - driven therapy . 
 similarly , after additional evidence , other agents such as braf and alk inhibitors may move from the off - label to the on - label arena in additional tumor types over time . 
although the reasons are beyond the scope of this discussion , it leads to more on - label recommendations and has contributed somewhat to increased actionability over time in our cohort as well . an interesting point to note is the large cohort of patients not receiving genomics - driven therapy because of physician preference . 
of the cases found to have actionable alterations by expert curators , physicians were able to identify actionable alterations in 81% ( 362 of 445 ) .7 this finding showed that clinicians have substantial awareness of actionability . 
 the os benefit of genomics - driven therapy has been evaluated only in a limited number of studies , the largest being the impact ( initiative for molecular profiling and advanced cancer therapy ) study.12 this retrospective analysis included a cohort of 1 , 436 patients , of whom 637 ( 44.4% ) were found to have one or more clinically actionable alterations . 
the impact trial researchers used their institutions in - house ngs ; however , recommendations for treatment were not reviewed individually at a multidisciplinary gtb , as they were in our case , making the definition we used for a clinically actionable alteration more stringent . 
 although the impact trial compared survival among patients who were all determined to have clinically actionable alterations , we compared survival between those who received genomics driven treatment and those who did not ( 54.1% of whom did not have a clinically actionable target or receive a gtb recommendation ) ; our approach was to evaluate the overall impact of precision oncology in all comers . 
the shiva trial was an open - label randomized controlled phase ii trial that spanned eight french hospitals to produce a cohort of 195 patients ; 99 were randomly assigned to the experimental group ( who received molecularly targeted therapy ) and 96 were randomly assigned to the control group ( who received treatment at physicians choice )  . 
of these , 22 patients received genomics - driven therapy and the other half received standard chemotherapy ( n = 17 ) or best supportive care ( n = 5 )  . 
although the treatment of every patient with cancer is certainly individualized , it is evident from the data that most patients get such testing performed only after they have progressed on multiple lines of treatment . 
in addition , given that trial ineligibility secondary to poor performance status is a deterrent to patients receiving genomics - driven therapy as recommended by the gtb , it could be suggested that patients would benefit from having ngs performed earlier in the course of their disease . it is notable that a number of different ngs platforms exist using diverse assays and gene panels , introducing a degree of variability in the field ; we report results that are based on a specific assay , which is now fda approved . 
relevant additional parameters to take into account and discuss with patients when ordering ngs testing include turnaround time , cost , and the possibility of identifying an incidental germline mutation . 
because the implications of the latter can be dire , pretest awareness and the need for genetic counseling for the patient and more broadly , for the family , before and after testing , is crucial.15 given that this was a retrospective study , we were reliant on medical record review to determine the reason behind treatment decisions ; this approach has inherent putative selection and confounding biases . 
although real - world analyses of the benefit of precision oncology are required , they are obviously limited by heterogeneity , with a mixture of histologies , prior therapies , various performance statuses , and a slew of different tumor - specific prognostic features . 
last but not least , the vast majority of patients in our cohort were white , highlighting the need to generate more data that include other racial and ethnic populations , which is actually aligned with the priorities of the national cancer institute regarding equity in cancer care delivery and health care disparities . 
in that regard , our group has launched a prospective study evaluating ngs testing in underserved populations . tumor genomic profiling influenced treatment in 15.8% of patients in this cohort , and its use has increased over time . 
more patients received treatment via clinical trials in the genomics driven treatment cohort , and although not statistically significant , there was a trend toward longer os in the genomics - driven versus the nongenomics - driven treatment group . 
 sohal amy pritchard no relationship to disclose administrative support : amy pritchard provision of study material or patients : all authors collection and assembly of data : all authors data analysis and interpretation : meena sadaps , davendra p.s. 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . meena sadaps no relationship to disclose pauline funchain consulting or advisory role : eisai haider mahdi no relationship to disclose petros grivas consulting or advisory role : genentech , dendreon , exelixis , merck , bristol - myers squibb , astrazeneca , biocept , clovis oncology , emd serono , seattle genetics , foundation medicine , driver speakers ' bureau : genentech , bristol - myers squibb research funding : mirati therapeutics ( inst ) , genentech / roche ( inst ) , merck ( inst ) , oncogenex ( inst ) , bayer ag ( inst ) , pfizer ( inst ) , astrazeneca ( inst ) stefan klek no relationship to disclose bassam estfan no relationship to disclose jame abraham honoraria : pfizer , genentech / roche speakers ' bureau : pfizer g . 
thomas budd research funding : genentech / roche ( inst ) , eisai ( inst ) , cytrx corporation ( inst ) , tracon pharma ( inst ) , threshold pharmaceuticals ( inst ) james p . 
pennell consulting or advisory role : astrazeneca , eli lilly , regeneron , cota healthcare research funding : genentech ( inst ) , celgene ( inst ) , astrazeneca ( inst ) , pfizer ( inst ) , merck alok a . 
khorana honoraria : janssen pharmaceuticals , halozyme , pfizer , bayer ag , angiodynamics , pharmacyte biotech consulting or advisory role : sanofi , janssen , halozyme , bayer ag , pfizer , pharmacyte biotech research funding : amgen ( inst ) travel , accommodations , expenses : janssen , pfizer , bayer ag brian j . 
sohal honoraria : foundation medicine consulting or advisory role : perthera research funding : novartis ( inst ) , celgene ( inst ) , oncomed ( inst ) , bayer ag ( inst ) , genentech ( inst ) , bristolmyers squibb ( inst ) travel , accommodations , expenses : foundation medicine affiliations meena sadaps , pauline funchain , haider mahdi , amy pritchard , stefan klek , bassam estfan , jame abraham , g . 
tsimberidou a - m , hong ds , ye y , et al : initiative for molecular profiling and advanced cancer therapy ( impact ) : an md anderson precision medicine study . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , openlabel , proof - of - concept , randomised , controlled phase 2 trial . 
genomics - driven therapy received after gtb recommendations ( n = 95 ) ( continued ) histology drug therapy type target os ( months ) pancreatobiliary idh1 inhibitor clinical trial idh1 prostate prostate prostate prostate prostate renal sarcoma sarcoma temsirolimus olaparib everolimus + bicalutamide trastuzumab olaparib + bicalutamide cabozantinib palbociclib sunitinib unknown primary lenvatinib unknown primary trastuzumab + folfox unknown primary idh1 inhibitor unknown primary trastuzumab + pertuzumab unknown primary everolimus unknown primary trastuzumab abbreviations : gtb , genomics tumor board ; os , overall survival . 
the latest innovations in clinical trials have followed with master protocols , which are dened by inclusive eligibility criteria and devised to interrogate multiple therapies for a given tumor histology and / or multiple histologies for a given therapy under one protocol . 
conventionally conducted within the phase ii setting , basket designs have become popular as drug developers seek to effectively evaluate and identify preliminary efcacy signals among clinical indications identied as promising in preclinical study . 
the latest innovations in clinical trials have followed with master protocols , which are dened by inclusive eligibility criteria and devised to interrogate multiple therapies for a given tumor histology and / or multiple histologies for a given therapy under one protocol.1 , 2 the use of master protocols for oncology has become more common with the desire to improve the efciency of clinical research and accelerate overall drug development . 
the lung - map study , for example , used a master protocol for a phase ii / iii comparative trial designed to evaluate biomarkermatched therapies in patients with previously treated advanced squamous nonsmall - cell lung cancer.3 shortly after initiation , the us food and drug administration approved a new immunotherapy for the same population . 
the designs exibility facilitated subsequent modication of the standard of care , which preserved the relevance of the study.1 a second example includes the create study master protocol , which evaluated the efcacy of crizotinib in patients with alk or met mutations among six different tumor histologies , where each histology constituted a subtrial of alk / met - positive or alk / met - negative tumors.2 emerging cancer therapies may target relatively rare molecular subtypes , which poses practical challenges to completing a clinical trial devised to enroll a single clinical indication . 
second , biomarkerguided treatment selection supersedes traditional clinical indicators for the studied populations such that the presence of a molecular marker predicts response to a targeted therapy irrespective of tumor histology.2 , 4 , 5 thus , basket trials are designed to enroll multiple clinical subpopulations in whom it is assumed that the therapy in question offers benecial efcacy in the presence of the targeted molecular prole . 
most often conducted within the phase ii setting , basket designs have become popular as drug developers seek to effectively evaluate and identify preliminary efcacy signals among clinical indications identied as promising in preclinical study.6 - 8 in certain circumstances , however , evidence acquired from a basket trial has served as the basis for regulatory approval.9 , 10 the framework also poses new challenges to statistical analysis . 
 kaizer et al context key objective describe recent developments in the design of basket trials for oncology studies and elucidate several issues that pertain to their statistical analysis and design . knowledge generated basket trials have evolved from their initial use in exploratory contexts to conrmatory , randomized , and platform trials . 
the context of each trial requires consideration of statistical properties for trial design ( strength and type of type i error control and implications for power ) and methods for analysis ( to pool clinical indications with a common target or accommodate the potential for heterogeneous activity among tumor histologies )  . relevance advances in genomics , disease pathways , and drug discovery have progressed into clinical cancer research . 
innovations in trial design with basket trials facilitate interrogations of multiple therapies for a given tumor histology and / or multiple histologies for a given therapy - target combination that bridges aspects of translational and clinical research paradigms . 
molecularly targeted treatment strategies may not offer acceptable efcacy to all putatively promising clinical indications . proliferation rates of tumor cells are known to vary within and between tumor types.11 moreover , contemporary sequencing methodologies have revealed extensive genetic variation among different types of cancer . 
as drug developers pursue drug approvals with broad labels ( eg , pembrolizumab for which indication was expanded in 2017 to include any unresectable or metastatic solid tumors with microsatellite instability , 12 larotrectinib in 2018 for adults and children who harbor ntrk gene fusion without a known acquired resistance mutation13 ) , trials will evaluate multiple disease indications for agnostic effects . 
for these trials , subpopulation analysis becomes central to the study design and should be considered in the evaluation of trial operating characteristics . trials , discusses this article reviews designs of basket several issues that arise with their implementation , and examines the statistical criteria considered in the development of such trials . 
this section discusses examples of exploratory trials designed as basket trials and introduces recent extensions that convey the evolving landscape of basket trial design in oncology . exploratory designs most basket trials have been conducted within exploratory settings to evaluate agent - specic estimates of tumor response . 
cunanan et al5 described three studies implemented in oncology settings that extend the basic formulation of a basket trial to multiple targets and / or agent combinations . the nci - match trial used a master protocol to enroll participants into drugand mutation - specic baskets while also incorporating genetic screening . 
a basket trial approach was selected to accommodate the rare disease setting , which is limited by traditional large prospective trials.14 the custom trial was a phase ii study with a two - stage design that aimed to identify molecular biomarkers and determine their clinical relevance in patients expected to benet from multiple targeted therapies.15 these trials facilitated the study of less common types of malignancies . 
in addition , these studies were devised to identify potential baskets in which the respective therapies demonstrated promising efcacy and , thus , were exploratory . extensions to randomized , conrmatory designs the methodology for basket trials has been extended to accommodate a wide variety of potential motivations beyond exploratory studies . 
one such extension includes randomized design such that participants are randomly assigned to either a standard - of - care arm without regard to specic genetic mutations or to an arm where a specic mutation is hypothesized to be susceptible to targeted treatment.16 , 17 these designs test the hypothesis that biomarker - guided selection demonstrates benecial treatment efcacy . 
 basket designs : statistical considerations for oncology trials fusion of basket and platform trials may accommodate exploratory and conrmatory study.18 one example of this approach is the signature program , which included a series of eight agent - specic , open - label , phase ii basket trials under a single overarching master protocol.21 the signature program was tissue agnostic and driven by molecular indications with the intention to demonstrate the feasibility of rapid signal nding across multiple tumors . 
molecularly targeted treatment strategies , however , may not offer acceptable efcacy to all putatively promising clinical trials pose challenges to the traditional paradigm for trial design and analysis , which assumes that individual patients who enroll in the same clinical study represent exchangeable units that can be averaged . 
imatinib , for example , was shown to be efcacious in treating malignancies , such as philadelphia chromosomepositive chronic myelogenous leukemia , through the dysregulation of imatinib - sensitive protein tyrosine kinases.23 to determine whether other malignancies with similar kinases respond to treatment , a single - arm , open - label , phase ii study was conducted with inclusive enrollment across 40 different pathologic diagnoses.24 neither the number of indications was constrained nor the design devised to examine subpopulation - specic effects . 
the study represents an example of the challenges posed by indication heterogeneity with conventional study design ( eg , see lacombe et al25 ) , the prediction of which may not be feasible in advance of a studys implementation . the opposite end of the spectrum is dened by studies that evaluate the effectiveness of a treatment strategy for a given subpopulation independent of the evidence acquired from patients in differing patient subsets . 
subpopulation - specic inference also fails to delineate which patient subtypes should be considered nonexchangeable on the basis of the observed data . for example , upon establishing that melanomas that exhibit braf v600 mutations respond to vemurafenib , 26 a basket trial was designed to evaluate the effectiveness of vemurafenib in patients without melanoma , with baskets dened by primary tumor origthe study was devised to interrogate the effectiveness of vemurafenib independently among patients who harbor braf v600 mutations within several prespecied tumor organ sites.5 , 9 despite having designed the study with success criteria that were invariant by tumor indication , the studys analysis plan evaluated evidentiary measures of effectiveness independently for each basket . 
with some baskets having observed low accrual and others yielding one or no response , overall conclusions are difcult to ascertain.27 the polarities of independence and pooling require strong a priori assumptions , which yield poor statistical designs when violated . 
these include multistage designs that merge subtypes at interim analyses28 or bayesian adaptive designs with hierarchical modeling strategies.29 hobbs and landin30 adapted the multisource exchangeability model ( mem ) , 31 which facilitates bayesian inference with respect to all possible pairwise exchangeability relationships among the studied subpopulations . 
the design enables the identication of disjointed subpopulations that comprise meta - subtypes or singleton subtypes on the basis of accumulating evidence during the course of study . design criteria and operating characteristics a basket designs operating characteristics should be determined by the trials intention and phase of development . control of falsely concluding that an inferior experimental therapy offers benet to any clinical indication should be emphasized for conrmatory trials that enroll multiple indications . 
statistical designs of clinical studies are conventionally devised in consideration of distributions of test statistics that measure the extent of evidence acquired against a prespecied null hypothesis upon repeated sampling of the trial data for a given decision rule . 
for hypotheses of superiority , null hypotheses dene value ( s ) of statistical parameters for which the underlying true state of nature is characterized by the absence of treatment effectiveness . 
for one - sample the null often is represented by a xed , prestudies , specied value that represents an expected response rate considered inadequately low to justify additional investigation . 
the decision rule determines the extent to which the trials conclusions could be explained as a result of chance . in this context , a type i error occurs when the null hypothesis is true but the trial yields data for which the decision rule rejects the null hypothesis in favor of a positive nding . 
for basket trials designed to examine multiple indications , the possibility of committing a type i error may occur for tests of each subpopulation , yielding two types of false conclusions : marginal type i error rates estimate the type i error rate for each indication separately , whereas family - wise type i error rates consider the entire trial violation if a single indication falsely rejects the null hyrepresents stronger pothesis . 
when selecting a statistical design devised to enroll and evaluate multiple indications , trialists must synthesize the trials operating characteristics with respect to a diverse array of possible trial outcomes , which we denote hereafter as scenarios . 
the strongest control is therefore conferred by the scenario with only one null indication . decisions that pertain to statistical approaches for analysis of multiple subpopulations , expected enrollment distribution , type i error method , and the strength of type i error control have implications for a designs statistical power . 
in the absence of heterogeneity among indications , the pooling of data acquired from all indications has the potential to increase statistical power ( identify smaller effect sizes )  . 
in addition , increasing imbalance among subpopulation sample sizes may reduce power and / or inate bias under strategies that enable data pooling . hierarchical models devised to share information across indications in relation to estimates of statistical exchangeability have been proposed by various authors18 , 35 - 38 with the intention of increasing statistical power while controlling bias . 
hierarchical models were calibrated for strong control of type i error such that marginal type i error was controlled under scenarios for which only one ( of ve or 10 ) subpopulation was truly ineffective . 
it should be noted , however , that under scenarios with multiple null subpopulations , the designs that resulted from hierarchical models demonstrated both commensurate power and reduced type i error when compared with subpopulation - specic analyses . 
in some cases , drastic reductions in type i error were observed for hierarchical models , such as the global null scenario , where strong borrowing reduced the type i error rate from a target of 10% to approximately 1% when considering 10 indications.39 moreover , the authors failed to adjust frequentist tests for multiple comparisons , which would have attenuated their power . 
in the presence of limited or imbalanced enrollment , however , one may wish to combine subpopulations or use statistical methods to facilitate information sharing among patient subpopulations.5 , 30 guidelines for evaluating the operating characteristics of subpopulation analyses are needed for both conrmatory and nonconrmatory settings.33 , 34 to provide an illustration of the existing strategies and their trade - offs , a simulation study was completed for a xedsample basket trial with ve indications each enrolling 25 patients . 
type i error , however , inates quickly to unacceptable levels in the presence of basket heterogeneity . the independent analysis approach , which adjusts for multiplicity , maintains family - wise error rates , 5% , but it is at the expense of power ( only 0.66 probability of identifying any active basket as efcacious )  . 
finally , the analysis of each basket independently and failure to adjust for multiple comparisons yielded high power ( 0.91 ) with large familywise error rates for all scenarios except the one with four active baskets ( ie , one null basket )  . the method for calibrating basket results for the bayesian model are provided for three posterior probability decision thresholds to illustrate the exibility of trials of various types . 
calibration 1 maintains a marginal type i error at 10% with no active baskets as well as increased probability for identifying effective baskets relative to independent approaches with two or more active baskets . family - wise error and marginal type i error rates are inated with fewer active baskets , however . 
reported is the basket - specic probability of being declared efcacious for null ( nonbold ) and active ( bold ) baskets for multisource exchangeability models ( mems ) with different pp threshold calibrations . 
this stands in contrast multiplicity ( low power of 0.66 ) or do not adjust for multiplicity ( higher power at the expense of higher family - wise error rates of 40% )  . 
the three calibrations presented were selected to demonstrate acceptable designs for different types of basket trials , with calibrations 1 and 2 formulated for exploratory settings and calibration 3 appropriate for conrmatory trials . discussion subpopulation heterogeneity is intrinsic to evaluations of cancer therapies that emerge within the evolving oncology landscape . 
basket trials provide a natural framework for studying molecularly targeted treatment strategies in several potentially promising clinical subpopulations while acknowledging the possibility of heterogeneous results . initiated in exploratory settings , basket designs have evolved to include randomization , enrichment of the enrolled population , and incorporation to platform trials and even acquire conrmatory evidence . 
further innovations and renements may make it possible to use the framework across the full spectrum of clinical translation with seamless design.19 as our simulation study demonstrates , basket trials should require analysis strategies and designs that acknowledge the potential for subpopulation effects . 
several aspects of basket trials , including the recommendations for weak versus strong control of type i error and adjustment for multiplicity , require additional consideration and guidance from academic and regulatory leaders to promote best practices for each stage of the research process.33 as basket trials evolve from simple exploratory trialists trials to increasingly complex master protocols , should avoid simple replication of designs from prior study and instead adapt the trial to its context with appropriate assumptions for the phase of inquiry . our simulation study demonstrates that nave pooling of all subpopulations results in unacceptable type i error , whereas independent examination of each basket without correction for multiplicity may result in inated type i error or , conversely , decreased power to detect efcacious baskets when correcting for multiplicity . 
the mem was evaluated with three different posterior probability threshold calibrations , each demonstrating appropriate operating characteristics for basket trials devised for exploratory and conrmatory settings . further improving their accessibility is the availability of the basket package in r to implement the symmetric mem approach.41 these results stand in contrast to challenges and limitations to information sharing previously reported.34 , 39 one should note a few limitations , however , that remain unresolved by the basket trial framework . 
patients described by a common subpopulation may exhibit sources of heterogeneity on the basis of other important considerations , such as immune prole , prior treatment histology , informatics that redemographics , or additional clinical quire patient - level data analysis . 
for a single tumor histology , this can yield insufcient efcacy not because the drug is necessarily ineffective for the indication but because the subtype in the trial happened to enroll a disproportionate number of patients with refractory disease.27 in settings where indication heterogeneity is not only known but also well understood , an effective means for addressing this type of heterogeneity is to construct baskets derived from information contained in clinical and auxiliary data sources . 
given sufcient enrollment , an indication can be partitioned into prognostic subpopulations and thereby provide new avenues for delineating drug versus prognostic effects at the subpopulation level without randomization . basket trials , like many master protocols , require tissue analysis and molecular proling before registration , which often limits their scope to a small number of leading academic institutions . 
molecular match rates for trials of targeted therapies have been reported to be as low as 4%.42 a single - institution study of the msk - impact assay evaluated 1 , 932 patients and a span of 49 cancer types in the real - world setting and in a matched found that 13% of patients were enroll study.43 by facilitating a centralized platform for acquiring and processing genomic data in conjunction with their functional and therapeutic implications , basket trials may overcome such deciencies . 
this has prompted interrogations of electronic health recordderived measures of real - world progression as alternatives to the response evaluation criteria in solid tumors ( recist ) .44 with the emergence of data science and machine learning , pathologic and radiologic data may offer new avenues for rapid , noninvasive patient proling . 
innovations in radiomics , for example , have effectively yielded prognostic signatures from informatics acquired from scanning technologies used routinely in clinical settings.45 - 48 to address the potential for heterogeneity within a clinical indication , innovations that facilitate use of noninvasive biomedical informatics and algorithms should be pursued with the aim of developing prognostic models in concert with the trials design . 
koopmeiners patents , royalties , other intellectual property : listed as an inventor for us patent 9 , 858 , 665 , which describes a computer - aided design system for predicting prostate cancer using magnetic resonance imaging satrajit roychoudhury employment : pzer leadership : pzer stock and other ownership interests : pzer , novartis david s . 
hong stock and other ownership interests : molecularmatch , oncorena , presagia honoraria : adaptimmune , baxter , merrimack , bayer ag consulting or advisory role : baxter , bayer ag , guidepoint global , janssen pharmaceuticals , genentech , eisai , glg , alpha insights , axiom biotechnologies , adaptimmune , grouph , merrimack , medscape , numab , pzer , seattle genetics , takeda pharmaceuticals , trieza therapeutics research funding : novartis , genentech , eisai , astrazeneca , pzer , mirna therapeutics , amgen , daiichi sankyo , merck , mirati therapeutics , eli lilly , adaptimmune , abbvie , bayer ag , bristol - myers squibb , genmab , ignyta , innity pharmaceuticals , kite pharma , kyowa hakko kirin , loxo oncology , medimmune , molecular templates , takeda pharmaceuticals , seattle genetics , amgen , fate therapeutics , mologen , nci - ctep travel , accommodations , expenses : loxo oncology , mirna therapeutics , genmab brian p . 
n engl j med 377 : 62 - 70 , 2017 renfro l , sargent d : statistical controversies in clinical research : basket trials , umbrella trials , and other master protocols : a review and examples . 
ann oncol 28 : 34 - 43 , 2017 steuer ce , papadimitrakopoulou v , herbst rs , et al : innovative clinical trials : the lung - map study . 
clin pharmacol ther 97 : 488 - 491 , 2015 redig aj , j anne pa : basket trials and the evolution of clinical trial design in an era of genomic medicine . 
j clin oncol 33 : 975 - 977 , 2015 cunanan km , gonen m , shen r , et al : basket trials in oncology : a trade - off between complexity and efciency . 
nakamura y , komatsu y , kato k , et al : btmb - high basket trial : a multicenter phase ii trial of nivolumab monotherapy in patients with advanced gastrointestinal cancers with high blood tumor mutational burden ( btmb )  . 
j clin oncol 37 , 2019 ( suppl ; abstr tps179 ) diamond el , subbiah v , lockhart ac , et al : vemurafenib for braf v600 - mutant erdheim - chester disease and langerhans cell histiocytosis : analysis of data from the histology - independent , phase 2 , open - label ve - basket study . 
sch offski p , wozniak a , escudier b , et al : crizotinib achieves long - lasting disease control in advanced papillary renal - cell carcinoma type 1 patients with met mutations or amplication . 
lopez - chavez a , thomas a , rajan a , et al : molecular proling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
chen c , li x , yuan s , et al : statistical design and considerations of a phase 3 basket trial for simultaneous investigation of multiple tumor types in one study . 
heinrich mc , joensuu h , demetri gd , et al : phase ii , open - label study evaluating the activity of imatinib in treating life - threatening malignancies known to be associated with imatinib - sensitive tyrosine kinases . 
freidlin b , korn el : borrowing information across subgroups in phase ii trials : is it useful ? clin cancer res 19 : 1326 - 1334 , 2013 40 . 
grifth sd , tucker m , bowser b , et al : generating real - world tumor burden endpoints from electronic health record data : comparison of recist , radiologyanchored , and clinician - anchored approaches for abstracting real - world progression in non - small cell lung cancer . 
yu w , tang c , hobbs bp , et al : development and validation of a predictive radiomics model for clinical outcomes in stage i non - small cell lung cancer . 
lacking multivariable specication of relationships among subpopulations , conventional analysis strategies represent the extremes of either pooling all indications or analyzing each indication independently of the evidence acquired for other indications . 
more specically , pooling in this context refers to an analysis strategy devised to evaluate evidence of effectiveness for all indications through statistical inference of a single response rate that is estimated using data from all indications . 
by relying on only one test , marginal and family - wise type i error rates are identical for the pooled approach . at the other extreme , independent analyses infer a total of ve response rates estimated from the data observed within specic indications . 
our simulation study considers the constrained empirical bayes ( ceb ) priors for symmetric mems described by hobbs and landin.30 briey , unconstrained empirical bayes approach to prior specication identies and conditions the analysis with respect to the mem that maximizes the marginal data likelihood . 
while acknowledging the uncertainty about identifying the true mem from the marginal likelihood , the ceb prior constrains shrinkage using an upper bound ( ub ) on the prior probability of inclusion for each source . 
for the basket trial with ve indications , there are six possible scenarios that range from all indications being null ( scenario 1 ) to all indications being alternative ( scenario 6 ) and four intermediate combinations ( scenarios 2 to 5 )  . 
for the bayesian mem approach with ub = 0.10 , posterior probability thresholds were identied that maintained the basket - specic ( marginal ) type i error rate under the global null scenario , the type i error rate for the scenario with one null basket , and the family - wise type i error rate for the global null scenario . 
the other two articles are case reports of breast and gastroesophageal cancer with mismatch repair deficiency ( dmmr ) where immunotherapy resulted in remarkable responses . these articles are highly relevant because the us food and drug administration ( fda ) approved pembrolizumab in may 2017 for the treatment of all unresectable or metastatic cancer with msi / dmmr irrespective of tissue origit was the first time that any therapy had been approved for cancers that share a specific genetic feature irrespective of site of origfurthermore , in late july , nivolumab was approved for msi / dmmr metastatic colorectal cancer . 
the fda approvals are based on studies showing disease control rates of 70% to 90% in patients with colorectal cancer and noncolorectal msi / dmmr cancers , most of whom with disease that was refractory to standard chemotherapy upon entering these trials.1 - 3 these trials had not reached median progression - free survival1 , 2 or overall survival1 - 3 at the time of publication , indicating that the responses are durable . msi is defined as a difference in length of microsatellites ( dna nucleotide repeats ) when comparing tumor dna with normal dna from the same individual . 
deficiency in the mmr system , a dna repair system in charge of correcting errors during dna replication , causes a distinct accumulation of errors in microsatellites , as well as a hypermutated phenotype . 
the mmr system is most commonly inactivated in tumors by either somatic inactivation via methylation of the mlh1 gene , 4 germline mutations in the mmr genes ( mlh1 , msh2 , msh6 , and pms2 [ lynch syndrome ] ) , 5 or , more rarely , somatic mmr mutations.6 , 7 dmmr can be detected by two widely implemented methods : immunohistochemistry ( tumor is stained for the four mmr proteins ) and msi testing via polymerase chain reaction ( pcr )  . 
these two methods have a high concordance.8 traditionally , msi testing has been done via pcr focusing on five predefined microsatellites ( monoor dinucleotide microsatellites ) , which were initially chosen during a meeting in bethesda in 1997.9 , 10 with the advent of ngs with targeted gene sequencing or whole exome / genome sequencing , myriad microsatellites can now be investigated simultaneously with computational tools . 
at least four different computational tools have been developed : msings , 11 msisensor , 12 mantis , 13 and mosaic.14 so how common is msi / dmmr in cancer ? it is well known that the highest msi / dmmr incidences are observed in endometrial cancer ( 20% to 30% ) , 15 - 17 colorectal cancer ( 12% to 15% ) , 18 , 19 and gastric cancer ( 15% to 20% ) , 20 although rates may be lower when focusing on metastatic disease ( 4% to 5% in colorectal cancer in populationbased studies ) .21 , 22 bonneville et al23 examined msi with mantis software in 11 , 139 tumors ( 39 cancer types ) , mostly derived from the cancer genome atlas , using whole exome sequencing data ( including 2 , 530 microsatellites )  . 
the study by middha et al24 describes lower rates of msi compared with bonneville et al , 23 but it is probably as a result of the more advanced stages examined in the study by middha et al . 
both studies looked at mutational burden and found that msi tumors have a significantly higher mutational burden compared with microsatellite stable ( mss ) tumors . do msi cases found via msi - ngs always signify tumors with dmmr ? or could they have other etiologies causing msi ? mantis had previously been validated against samples with msi by pcr in colorectal cancer , endometrial cancer , gastric cancer , esophageal cancer , and prostate cancer , as well as uterine carcinomasarcoma.13 in the study by bonneville et al , 23 the investigators examined ngs data of the mmr genes and found mmr mutations in some cases , but do not have data on mlh1 hypermethylation , which is the most common reason for msi . 
in the study by middha et al , 24 the msi status was validated in 138 colorectal and endometrial cancer cases by performing mmr immunohistochemistry and conventional msi by pcr . 
they found a high concordance between the methods ( 99.4% ) , and msi by ngs seems slightly more sensitive than msi by pcr because they discovered three msi cases by msisensor that scored as msi - low or mss on pcr but were dmmr on immunohistochemistry . 
furthermore , they investigated 456 other cancer cases that scored low ( 3 to 10 ) on msisensor and found that only 3.5% were discordant ( msi by pcr ) , reflecting the fact that most cases with low msi are not truly dmmr.10 ideally , validation would be done for every tumor type to ensure that msi is detected across a range of different cancers and truly represents dmmr . 
in the study by middha et al , 24 one case with a pole mutation was msh6 deficient and msi ; all other pole - mutated cases were mss by msisensor and had normal mmr immunohistochemistry , suggesting that msi in pole - mutated cases is secondary to mutations in mmr genes . other studies have described similar findings.6 , 25 the case reports are great examples of how tumors that are not typically associated with msi status can respond dramatically to immunotherapy . 
in the study by kok et al , 26 a 69 - year - old patient with metastatic breast cancer responded to nivolumab , with complete resolution of a malignant gastric ulcer after three cycles and an ongoing response after 12 cycles of nivolumab . 
in the study by klempner et al , 27 an 85 - yearold patient with stage iii gastroesophageal adenocarcinoma , deemed not a surgical candidate , had a complete response to pembrolizumab , with an ongoing response for 8 months . 
because mlh1 - hypermethylated tumors are more commonly observed in older patients , 16 , 20 , 28 a patients age should not deter physicians from investigating msi / dmmr . with the fdas recent approval of immunotherapy in msi / dmmr advanced cancers , and the finding of this molecular signature across a broad range of tumor types , screening all metastatic cancer cases for msi should become standard practice . 
companies and / or institutions who offer multiple gene sequencing panels should strongly consider integrating msi analysis into their existing ngs protocols and include this as part of their reporting . 
some panels are already reporting this , such as the foundation one platform . it is unclear how many of the msi cases found in the studies by bonneville et al23 and middha et al24 were caused by lynch syndrome . 
in prior studies , 10% to 15% of msi / dmmr colorectal cancer cases and 10% of msi / dmmr endometrial cancer cases were caused by lynch syndrome.21 , 22 , 29 lynch syndrome can increase the risk of many of the malignancies found to be msi in the studies presented in jco precision oncology ; thus it is important for physicians to refer patients with msi / dmmr cancers to the genetics clinic ( the exception being mlh1 / pms2 - absent cancers that test positive for mlh1 hypermethylation , because most of these cases are somatic )  . 
overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - deficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
kane mf , loda m , gaida gm , et al : methylation of the hmlh1 promoter correlates with lack of expression of hmlh1 in sporadic colon tumors and mismatch repair - defective human tumor cell lines . 
haraldsdottir s , hampel h , tomsic j , et al : colon and endometrial cancers with mismatch repair deficiency can arise from somatic , rather than germline , mutations . 
bartley an , luthra r , saraiya ds , et al : identification of cancer patients with lynch syndrome : clinically significant discordances and problems in tissue - based mismatch repair testing . 
boland cr , thibodeau sn , hamilton sr , et al : a national cancer institute workshop on microsatellite instability for cancer detection and familial predisposition : development of international criteria for the determination of microsatellite instability in colorectal cancer . 
billingsley cc , cohn de , mutch dg , et al : polymerase e ( pole ) mutations in endometrial cancer : clinical outcomes and implications for lynch syndrome testing . 
 o comparative analysis of public knowledge bases for precision oncology steffen pallarz , phd1 ; manuela benary , phd1 , 2 ; mario lamping , md2 ; damian rieke , md2 , 3 ; johannes starlinger , md2 ; christine sers , phd2 , 4 ; david luis wiegandt1 ; marc seibert1 ; jurica seva , phd1 ; reinhold sch afer , phd2 , 4 ; ulrich keilholz , md2 ; and ulf leser , phd1 purpose precision oncology depends on the availability of up - to - date , comprehensive , and accurate information about associations between genetic variants and therapeutic options . 
we performed a quantitative and qualitative comparison of clinical interpretations of variants in cancer , oncokb , cancer gene census , database of curated mutations , cgi biomarkers ( the cancer genome interpreter biomarker database ) , tumor alterations relevant for genomics - driven therapy , and the precision medicine knowledge base . methods we downloaded each kb and restructured their content to describe variants , genes , drugs , and genedrug associations in a common format . 
for the analysis of clinically relevant gene - drug associations , we obtained lists of genes affected by genetic alterations and putative drug therapies for 113 patients with cancer whose cases were presented at the molecular tumor board ( mtb ) of the charit e comprehensive cancer center . results our analysis revealed that the kbs are largely overlapping but also that each source harbors a notable amount of unique information . 
the relative importance of a kb in terms of cancer genes was assessed in more detail by logistic regression , which revealed that all but one source had a notable impact on result quality . 
we conrmed these ndings using a second data set obtained from an independent mtb . conclusion to date , none of the existing publicly available kbs on gene - drug associations in precision oncology fully subsumes the others , but all of them exhibit specic strengths and weaknesses . 
2019 by american society of clinical oncology introduction precision oncology ( po ) is based on the molecular characterization of tumors and the integration of these data into clinical decision making.1 molecular characterizations typically are based on the identication of genomic variants by genomic sequencing , which results in patient - specic variant proles of single nucleotide variants , small insertions or deletions , copy number variations , and gene fusion load of the events . 
this bottleneck of clinical interpretation in po currently is based mostly on manual work and still lacks standardization.2 clinical variant interpretation must be based on published information.3 however , such information currently is dispersed across a number of databases , repositories , and web sites . 
 pallarz et al context key objective several knowledge bases that support the clinical evaluation of genetic variants in patients with cancer have emerged during the past years , but their mutual overlaps and extents are unknown . knowledge generated we compared seven knowledge bases and found that they share information only to a moderate extent and that they altogether lack important data . 
also , none of the knowledge bases is clearly more comprehensive than the others . relevance the creation of structured and easy - to - use knowledge bases to support precision oncology has made notable progress in the past years , yet the current systems remain incomplete and inhomogeneous . 
our results underline the necessity that , to obtain comprehensive information , oncologists must interrogate multiple knowledge bases and search relevant literature directly . we compared these kbs by measuring their mutual overlap of genes , drugs , and gene - drug associations and , if possible , by comparing each kbs content to actual treatment recommendations for 113 patients with cancer whose cases were discussed at the molecular tumor board ( mtb ) of the charit e comprehensive cancer center . 
results were conrmed using a second , independent set of recommendations for 10 patients with cancer . methods we performed pubmed searches and expert interviews to obtain a list of seven publicly available knowledge bases that aim at supporting medical decision making in precision oncology ( po - kb ) by providing structured information regarding the relationship between genes , variants , cancer entities , and therapies . 
specically , we used ( 1 ) civic ( clinical interpretations of variants in cancer ) , ( 2 ) oncokb , ( 3 ) cgc ( cancer gene census ) , ( 4 ) docm ( database of curated mutations ) , ( 5 ) cgi biomarkers ( the cancer genome interpreter biomarker database ) , ( 6 ) target ( tumor alterations relevant for genomics - driven therapy ) , and ( 7 ) pmkb ( the precision medicine knowledge base )  . 
the technical data integration procedure and normalization methods we developed for genes , variants , and drugs can be found in the data supplement . overlap comparison for a quantitative comparison , we computed the mutual overlap of all sources with regard to the set of genes , variants , drugs , and gene - drug associations they contain and visualized them using upset diagrams.12 for clustering of po - kbs , we rst computed pairwise distances using jaccards formula for set similarity and then applied hierarchical clustering ( data supplement )  . comparison of clinically relevant gene - drug associations we compared the content of each po - kb alone and in combinations versus recommendations of the charit e comprehensive cancer centers mtb ( n = 113 patient cases ) , at which results of comprehensive molecular table 1 . 
diagrams show the overlap between different precision oncology knowledge bases ( po - kbs ; identied by colors ) the matrices in the lower panels indicate po - kbs involved in an intersection , and the bar plots show the number of elements in this intersection . 
cgi , cgi biomarkers ( the cancer genome interpreter biomarker database ) ; civic , clinical interpretations of variants in cancer ; db , database ; docm , database of curated mutations ; pmkb , precision medicine knowledge base ; target , tumor alterations relevant for genomics - driven therapy . analysis ( whole - exome or panel sequencing , rna sequencing , immunohistochemical validations ) from patients with advanced cancer are discussed on a weekly basis . clinical interpretation of molecular alterations in the mtb is performed by a trained physician3 , 13 ; the data supplement contains details on this process . 
we measured the overlap between this reference set and different combinations of po - kbs for each patient using the metrics precision ( percentage of associations of a [ set of ] po - kb that is also contained in the reference ) , recall ( percentage of associations in the reference that is also contained in a [ set of ] po - kb ) and f1 measure ( harmonic mean between precision and recall )  . 
these measures are visually displayed later in the results , and more details can be found in the data supplement . to assess the predictive power of the different po - kbs , we proceeded as follows : for each association present in any of the po - kbs , a vector representation was constructed to encode its coverage by civic , cgi biomarkers , target , and oncokb , respectively . 
every gene - drug association that also was listed in the mtb associations was considered positive ( association relevant ; n = 345 cases ) , and all others were considered negative ( association not relevant ; n = 808 cases )  . 
 ( a ) percentage of patients for which any gene - drug associations were found when their presence was required in one to four po - kbs ( y - axis )  . 
each dot represents one patient , and only patients for whom at least one gene - drug association had been found were used . a 10 - fold cross - validation scheme to compute the out - ofsample error . 
eventually , a new model was trained on the entire training set to take this error into account ( using r package caret ) ; we report the results of the second model when applied on the test set . to validate our ndings , we used a second data set , which described treatment recommendations for patients with cancer , as derived at the molecularly aided stratication for tumor eradication ( masters ) 14 program at the national center for tumor diseases in heidelberg ( n = 10 ) and obtained from perera - bel et al.15 the normalization of gene and drug names for both data sets is described in the data supplement . 
to make results comparable to our rst data set , we removed all affected genes for which we did not have a single association in any of the po - kbs or for which no drug recommendation had been provided . 
to compensate for the positive bias in this set , we then added twice the number of genes chosen randomly from those we removed before . results overlap of studied kbs we downloaded and normalized seven publicly available databases that aim to support clinical decision making in po . we found that all databases overlap to a certain degree in the information they provide but also that each provided unique information . 
civic ( n = 89 genes ) and oncokb ( n = 86 genes ) have the second largest number of unique genes not mentioned in any other po - kb ; 49 genes were contained in all seven databases . 
the data supplement shows a hierarchical clustering of po - kbs on the basis of their overlaps in genes , variants , and gene - drug associations . although civic , oncokb , and pmkb share a highly similar goal and creation process and also obtain their data from the same origin ( scientic publications ) , each of them contains a substantial amount of unique genes . 
the most probable reason for this observation is that all po - kbs are small compared with the huge amounts of published data . the data supplement lists all genes contained in one or more of the databases . 
in addition , the four sources that contain drug information provide both shared and unique information ( fig 1b ) : 17 drugs are mentioned in all sources , and civic has the largest number of unique drugs ( n = 223 )  . 
similarly , civic shows the largest number of unique gene - drug associations ( n = 698 ; fig 1c )  . comparison of clinically relevant gene - drug associations we next compared the content of each po - kb and combinations thereof versus expert considerations for the 113 patients discussed at the charit e mtb at the level of genedrug associations . 
the number of drugs is high , because , for the analysis , drug classes ( eg , mammalian target of rapamycin inhibitors ) were expanded to all drugs of the respective class to match the granularity of information in different data sets . 
we analyzed which patients for whom the associations presented to the mtb also were contained in different po - kbs ( fig 2 ) and which fractions of gene - drug associations presented in the mtbs also would be found by specic combinations of po - kbs ( fig 3 )  . overall , the mtb discussed 203 different genes and 245 different drugs , of which 152 and 176 , respectively , were found in at least one po - kb . 
this implies that 25% of genes and 28% of drugs discussed in the mtb could not be found by our software in any of the po - kbs we considered . 
next , we computed the set of prioritized genes per patient and checked for how many of those had associations with drugs in at least one , two , three , or four po - kbs . 
 comparison of knowledge bases for precision oncology precision true positives ( tp ) false negatives ( fn ) recall false positives ( tn ) true negatives ( tn ) in po - kbs precision recall no . 
 ( b ) median precision ( blue ) , recall ( red ) and f1 ( harmonic mean between precision and recall ) score ( gray ) when considering an increasing number of precision oncology knowledge bases ( po - kbs ) to support gene - drug associations discussed by the molecular tumor board ( mtb ) experts . 
 ( c ) precision and ( d ) recall obtained by using different combination of po - kbs as boxplots ( median , 25th and 75th percentiles ; whiskers extend to the maximum values within 1.5 the interquartile range ; dots represent outliers )  . 
cgi , cgi biomarkers ( the cancer genome interpreter biomarker database ) ; civic , clinical interpretations of variants in cancer ; pr , precision and recall ; target , tumor alterations relevant for genomics - driven therapy . gene - drug association , the number of patients decreases to 42 . 
figure 2b shows that the number of potential suggestions per patient drops sharply with the required number of supporting po - kbs : when support by any two po - kbs was required , we obtained a median of ve associations per patient . 
the median increased to 12 if only one po - kb was required and decreased to two for three po - kbs and zero for four po - kbs . next , we considered the mtb associations as reference and the contents of the four po - kbs that contained genedrug associations as predictors . 
when the mtb reference gene - drug association was required to be contained in only one po - kbsthat is , the union of all po - kbs was used as predictorthe median recall for all patients reached approximately 46% ( fig 3b , blue line ) , whereas the median precision was low because of the large number of associations found in the po - kbs that were not discussed in the mtb ( fig 3b , orange line ; data supplement contains evaluation metrics )  . 
intuitively , this means that searching in more than one po - kb in our evaluation always led to nding more relevant data but at the cost of also nding more data that are irrelevant for the concrete patient according to the mtb . finally , we trained a logistic regression classier on evidence from all po - kbs using mtb associations as ground truth . 
on our withheld test set ( n = 288 gene - drug associations ) , this model reached an f1 score of 43% ( precision , 64% ; recall , 33% )  . 
on the nct data set , this model reached a precision of 100% at a recall of 38% , which resulted in a higher f1 score of 56% . the data supplement contains an interactive html page with the complete list of gene - drug associations of the berlin and the heidelberg data sets together with the information about which of the po - kbs contains which reference associations . discussion we performed a quantitative and qualitative comparison of the current content ( february 2019 ) of seven knowledge bases specialized in po . 
our results indicate that the pokbs have partly overlapping and partly unique results . compared with associations discussed for 113 patients in an mtb of a comprehensive cancer center at a university clinic , we found that po - kbs contain relevant information not present in any of the others . 
however , we also want to point out some limitations of our work that warrant additional studies . even after careful normalization of gene and drug names in all po - kbs ( data supplement ) , 809 of the 1 , 154 gene - drug associations of the mtb data set were not found in any of the po - kbs . 
possible reasons for their absence are that these genes are simply not yet curated , are grossly misspelled , or designate gene families rather than individual genes and so could not be matched by our normalization procedure . 
similarly , 157 associations with 69 unique drugs were not found because these drugs are not contained in any of the kbs ; 383 associations were missing because none of the po - kbs reported this particular association , although both the genes and the drugs were found in principle . our analysis showed that civic has the highest recall and f1 score compared with mtb associations when data from only one po - kb are considered ( ie , no combinations were allowed )  . 
these submissions could be the reason for the higher recall of po - kb combinations contained in civic ( fig 3d ) ; however , civic also simply contains the highest number of gene - drug associations among all po - kbs considered , which also positively inuences recall . 
separation of these two effects is difcult , but we note that regression results on the heidelberg data set , for which no bias toward civic exists , are even better than for the mtb data set . 
on both data sets , removal of civic from the training data left the precision of the learned model unchanged but induced a notable decrease in recall ( mtb , 33% decreased to 19% ; heidelberg , 38% decreased to 21% ) and , thus , in the f1 score ( mtb , 43% decreased to 29% ; heidelberg , 56% decreased to 35% )  . 
the fact that the decrease in recall was comparable in both data sets is an argument against a strong bias of the charit e mtb analysis toward civic ; the overall strong decrease originates from the large number of gene - drug associations only contained in civic . as reported , we trained a classier on combinations of the different po - kbs using the mtb associations as ground truth . 
however , we note that the reported results in terms of prediction accuracy cannot be considered as the ability to predict treatments in a clinical decision support setting for multiple reasons . 
second , we considered all associations in the mtb data as relevant without taking into account the nal decision of the mtb , which could be the recommendation of a single drug , could be a combination of drugs , or could disregard all discussed associations . 
fifth , the patient cases presented in the mtb represent a large variety of different tumor types , such as breast cancer , pancreatic cancer , leiomyosarcoma , ovarian cancer , liposarcoma , and neuroendocrine tumors ( data supplement )  . our analysis ignored the information on cancer types , because this level of detail frequently is missing in the po - kbs and , when present , uses a highly idiosyncratic nomenclature . 
note that analysis of recommendations derived from genomic information across different cancer types is commonplace in current studies about po.16 , 17 in conclusion , we here report a quantitative and qualitative comparison of precision oncology knowledge databases . our analysis shows that each of the databases contains , besides a rather small common core , a relevant amount of unique information . 
when we compared po - kb contents with gene - drug associations discussed in two mtbs , we found that a considerable fraction of information indeed can be found in some po - kbs but also that many presumably clinically relevant associations are not yet contained in any of them and that relevant information often is dispersed across different po - kbs . 
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perera - bel j , hutter b , heining c , et al : from somatic variants towards precision oncology : evidence - driven reporting of treatment options in molecular tumor boards . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular proling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
massard c , michiels s , fert e c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . cancer discov 7 : 586 - 595 , 2017 18 . 
chinnaiyan , md , phd4 , 5 case description in january 2018 , a 79 - year - old man was referred to our genitourinary medical oncology clinic for management of his prostate adenocarcinoma metastatic to multiple bones . 
his prostate cancer spread to additional bony sites , which were likewise treated with radiation , including radiation to the thoracic spine in july 2017 and the proximal humerus in august 2017 , rather than any systemic in december 2017 , he had prophylactic therapy . nipple irradiation to prevent gynecomastia in preparation for noncastrating medical therapy with singleagent bicalutamide . 
on meeting the patient for the rst time in january 2018 , we elected to continue with the plan for single - agent bicalutamide 50 mg per day , given the patients preference and the uncertain prognosis from his metastatic melanoma . 
his prostatespecic antigen ( psa ) was 30.8 ng / ml at the time of treatment initiation and responded rapidly to bicalutamide , reaching a nadir of 1.1 ng / ml in september 2018 ( fig 1a )  . his melanoma was diagnosed from a shave biopsy of the right superior lateral lower back in august 2015 as localized ulcerated malignant melanoma , unclassied , with nevoid features . 
he subsequently had a microstaging excision and a right back excision with a negative sentinel lymph node in the right groin 2017 , the patient noticed a new lump on his right lower back scar in 2017 . 
in november 2017 , excisional biopsies of his right lower back and right groin both showed metastatic melanoma , as conrmed by immunohistochemistry ( ihc ) showing positive staining for sox - 10 and mart - 1 . 
a 7 - mm lesion was also detected on his posterior scalp and was also visible on magnetic resonance imaging of his brain and metabolically active on positron emission tomography ( pet ) / computed tomography ( ct ) ; hence , it was diagnosed as stage iv melanoma . 
he began treatment of his metastatic melanoma with pembrolizumab 200 mg intravenous every 3 weeks and received four treatments before the pembrolizumab was stopped because of the development of pneumonitis . 
his pneumonitis was treated with a taper of prednisone , which was reduced to physiologic dosing by august 2018 . however , despite evidence of response in his melanoma by physical examination , there was concern for progression on pet / ct in june 2018 , with fdg update in the descending colon / small bowel wall , perisplenic region , a mildly fdg - avid left internal iliac lymph node , and a right external iliac nodal conglomerate encasing the right ureter , 4.1 cm in diameter and with an suv max of 11.7. 
 case report systemic therapy : gem - carbo docetaxel bicalutamide pembro bicalutamide leuprolide 1.1 ureter stent and pelvic mass biopsy abdominal wall excisional biopsy psa : ( ng / ml ) 30.8 event : date : 1 / 2018 6 / 2018 1 / 2019 6 / 2019 1 / 2020 6 / 2020 before gem - carbo after gem - carbo before docetaxel after docetaxel fig 1 . 
psa , prostate - specic antigen . pelvic mass was judged to be atypical for either prostate cancer or melanoma , it was biopsied by pelvic laparoscopy in november 2018 and was found on surgical pathology assessment to be consistent with a high - grade carcinoma with squamous features ( fig 2a )  . 
we performed exome sequencing using the university of michigan oncoseq panel ( mi - oncoseq ) and whole transcriptome analysis on formalin - xed parafn - embedded tissue from this biopsy . 
all patients enrolled in the mi - oncoseq study provided written informed consent approved by the university of michigan institutional review board . consent is inclusive of publishing information and / or images from participants ( or their designate )  . 
because the pelvic mass was causing pain and urinary obstruction , we elected to treat it with a platinum doublet active in urothelial carcinoma and carcinoma of unknown primary , despite not knowing the tissue of origin january 2019 , we began carboplatin area under the curve 5 mg / ml / minute on day 1 and gemcitabine 1 , 000 mg / m2 on days 1 and 8 of 21 - day cycles , and we completed six cycles before stopping because of progressive fatigue . 
 ( d ) ihc for erg of the primary prostate tumor showing strong labeling . ( e ) h&e histology of the abd wall nodule biopsy specimen used for molecular analysis . 
 ( f ) ihc for erg of the abd wall nodule showing much weaker labeling . in june 2019 , while being treated only with bicalutamide , the patient was noted on ct scan as having a 1.4 - cm nodule in the supercial anterior abdominal wall , which subsequently became easily palpable and caused skin together with smaller adjacent erythema . 
this nodule , nodules , was removed by excisional biopsy in july 2019 , where surgical pathology assessment demonstrated tumor features consistent with metastatic squamous cell carcinoma ( fig 2b )  . 
a fresh portion of this specimen was sent for analysis using the mi - oncoseq platforthis specimen showed a much higher tumor content of 54% , allowing the discovery of additional molecular alterations . precision medicine tumor board discussion results were discussed at the university of michigan precision medicine tumor board in september 2019 . somatic aberrations detected in the previous sample were detected in the new biopsy specimen , suggesting clonal relatedness , and additional alterations consistent with the increased tumor content were noted as well ( table 2 )  . 
for prostate adenocarcinoma , the addition of medical castration , likely in addition to either abiraterone and prednisone or a nonsteroidal second - generation antiandrogen , would have been a reasonable next line of therapy . 
however , the transcriptomics data of the mi - oncoseq platform showed low expression of the androgen receptor and androgen responsive genes klk2 , klk3 ( psa ) , tmprss2 , acpp , and slc45a3 ( fig 3b )  . 
therefore , we did not plan chemotherapy with a regimen such as carboplatin and etoposide , which is active against small - cell neuroendocrine carcinomas . we examined the remainder of the molecular results in an effort to nd alternative , clinically actionable molecular targets . 
however , overall , the results for mtor inhibitors in prostate cancer have been disappointing.3 some randomized data support the use of pi3k inhibitors in metastatic castration - resistant prostate cancer.4 however , this was in combination with abiraterone , which made pi3k inhibitors less attractive in this case , given the patients near total lack of androgen signaling . 
however , we decided against this option because cdk4 / 6 inhibitors have thus far shown disappointing results in prostate cancer.5 therefore , we elected to treat with docetaxel , the most common cytotoxic chemotherapy drug for castration - resistant prostate cancer . at this point , the patients lung nodules , which were previously indeterminate , had enlarged greatly ( fig 1d )  . 
we started treatment with docetaxel at 75 mg / m2 for one cycle , then decreased the dose to 60 mg / m2 because of fatigue , and completed three more cycles . 
ct completed after three cycles showed an interval decrease in the size of multiple bilateral lung nodules , and a decrease in size of his right pelvic mass , compatible with a therapeutic response ( fig 1e )  . discussion in this case , we used next - generation sequencing to determine that the patients squamous cell carcinoma was actually of prostate origin , because of the presence of a gene fusion between tmprss2 and erg . 
 case report prostate cancer subtypes has become more common since the development of abiraterone and nonsteroidal secondgeneration antiandrogens , 6 possibly as a means to escape continual selective pressure against androgen signaling , a phenomenon that had been described rarely in the past.9 some of these double - negative prostate cancer ( dnpc ) tumors seem to be driven by broblast growth factor ( fgf ) alterations , and trials of fgf inhibitors have recently begun in advanced prostate cancer.10 our patient did not have an fgf abnormality . 
in the current case , despite having squamous differentiation , this patient had only stable disease in response to platinum - based chemotherapy . after using whole exome sequencing and rna sequencing to identify this tumor as a squamous neoplasm of prostate origin , we elected to treat him with an agent approved for prostate cancer ( docetaxel ) , an agent we would not have elected to use without knowing the tissue of origwe elected not to pursue the therapies that could target molecular alterations in his tumor because of the known survival benet of docetaxel in men with advanced prostate cancer , but therapies targeting his tumors molecular alterations remain options down the road if his disease progresses . 
alumkal consulting or advisory role : merck sharp & dohme , dendreon research funding : aragon pharmaceuticals ( inst ) , astellas pharma ( inst ) , zenith epigenetics ( inst ) , gilead sciences ( inst ) travel , accommodations , expenses : astellas pharma , merck sharp & dohme other relationship : astellas pharma arul chinnaiyan stock and other ownership interests : oncopia , tempus , esanik , oncofusion therapeutics , medsyn consulting or advisory role : tempus patents , royalties , other intellectual property : co - inventor on a patent on the detection of ets gene fusions in prostate cancer issued to the university of michigan . no other potential conicts of interest were reported . acknowledgment we thank the mi - oncoseq clinical sequencing team , leslie fecher , md , jeff montgomery , md , and michael sabel , md , for collaborative clinical care and discussion ; alex hopkins for assistance with gures ; and jyoti athanikar for assistance with scientic editing and manuscript preparation . 
cell 161 : 1215 - 1228 , 2015 [ erratum : cell 162 : 454 , 2015 ] statz cm , patterson se , mockus sm : mtor inhibitors in castration - resistant prostate cancer : a systematic review . 
target oncol 12 : 47 - 59 , 2017 de bono js , de giorgi u , rodrigues dn , et al : randomized phase ii study evaluating akt blockade with ipatasertib , in combination with abiraterone , in patients with metastatic prostate cancer with and without pten loss . 
clin cancer res 25 : 928 - 936 , 2019 clinicaltrials.gov : a phase ii study of androgen deprivation therapy with or without palbociclib in rb - positive metastatic prostate cancer . 
gov / ct2 / show / nct02059213 bluemn eg , coleman im , lucas jm , et al : androgen receptor pathway - independent prostate cancer is sustained through fgf signaling . 
cancer cell 32 : 474 - 489.e6 , 2017 labrecque mp , coleman im , brown lg , et al : molecular proling straties diverse phenotypes of treatment - refractory metastatic castration - resistant prostate cancer . 
j clin invest 129 : 4492 - 4505 , 2019 parwani av , kronz jd , genega em , et al : prostate carcinoma with squamous differentiation : an analysis of 33 cases . 
weindorf sc , taylor as , kumar - sinha c , et al : metastatic castration resistant prostate cancer with squamous cell , small cell , and sarcomatoid elementsa clinicopathologic and genomic sequencing - based discussion . 
with the recent increase in integrative clinical sequencing for pediatric patients with cancer , our understanding of the dicer1 syndrome continues to evolve , as new and rare pathogenic variants are reported . 
as the frequency of integrative clinical sequencing increases , discussions regarding challenges encountered in the interpretation of sequencing results are essential to continue to advance the eld of cancer predisposition . 
the purpose of this work was to identify patients with somatic and / or germline dicer1 variants in our patient population and to discuss sequencing interpretation and the clinical recommendations that result from the integrative clinical sequencing results . methods patients were enrolled in the peds - mioncoseq study . 
2019 by american society of clinical oncology introduction the dicer1 gene is located on chromosome 14 ( 14q32.13 ) and encodes the dicer protedicer is an rnase iii enzyme functioning in micro - rna ( mirna ) processing . 
mirnas are single - stranded , noncoding rnas that target mrnas by binding to complementary mrna sequences , increasing their degradation and suppressing translation.1 through its ability to regulate mirna processing , dicer1 plays a critical role in cellular mrna expression and in early development.1 , 2 with respect to human disease , more than 130 germline and 95 somatic dicer1 mutations have been reported.2 the majority of somatic dicer1 mutations are hotspot mutations in the rnase iiib domain ; however , somatic mutations are reported to be elsewhere , including the domain of unknown function.2 germline dicer1 mutations have been reported in all of the 10 major domains and spanning regions.3 dicer1 syndrome , caused by pathogenic variants in dicer1 , is an inherited condition associated with an increased risk of developing pleuropulmonary blastoma ( ppb ) , multinodular goiter , cystic nephroma , sertoli - leydig cell tumors of the ovary , and other rare tumors . 
 bailey et al context the goal of this work was to describe sequencing interpretation challenges and clinical recommendations in patients with dicer1 somatic and / or germline variants identied on integrative sequencing . this work suggests that postzygotic mosaicism may play a signicant role in the development of dicer1 - associated tumors . furthermore , we report a patient with a dicer1 variant of uncertain signicance whose clinical course and response to treatment was highly unusual , suggesting this variant could be clinically meaningful . the use of integrative clinical sequencing has signicantly expanded in pediatric oncology in the past 5 years . 
reports also include a dicer1 syndrome family with both somatic and germline pathogenic variants found in family members with different types of dicer1 - related cancers.15 to our knowledge , our group reported the rst real - time , integrative clinical sequencing ( ics ) study in the pediatric oncology population in 2015.16 since that time , the role of real - time ics of tumors and germline samples in the pediatric oncology population has continued to expand.17 - 19 however , the interpretation of genetic variants and their translation into the clinical setting remain challenging . when sequencing results identify germline dicer1 variants in pediatric oncology patients , counseling and screening implications for family members are affected . 
the purpose of this work was to highlight ( 1 ) somatic and / or germline dicer1 pathogenic variants identied in our pediatric oncology sequencing cohort , ( 2 ) challenges encountered with sequencing result interpretation with respect to dicer1 , and ( 3 ) current patient and family screening recommendations . methods patients the pediatric patients described were treated at c.s. 
patients were enrolled in a prospective , institutional review boardapproved ics trial ( peds - mioncoseq ) 16 and underwent paired tumor / normal whole - exome sequencing and tumor transcriptome sequencing . 
peds - mioncoseq is an ongoing precision oncology cohort and focused on enrolling highrisk , relapsed / refractory , and rare pediatric and young adult ( younger than 25 years of age ) patients with cancer . integrative clinical sequencing specics of the sequencing procedure and bioinformatics analyses have been previously described.16 briey , germline sequence and copy number variants , as well as somatic mutations , copy number alterations / variants , insertions and deletions , gene fusions , and gene expression , were identied.20 , 21 pathogenicity of germline variants was determined through a review of the published literature and publically available databases ( ie , clinvar )  . clinical relevance of somatic variants was investigated using an integrated approach incorporating technical considerations ( eg , recurrence , variant allele fraction , expression levels , and predictive algorithms for pathogenicity ) , variant - specic information ( ie , clinvar , published literature , and curated gene - specic resources ) , and published correlations of drug and variant sensitivity proles . results four patients with somatic and / or germline dicer1 pathogenic variants were identied among the rst 300 patients enrolled in peds - mioncoseq ( table 1 )  . 
we detail the patient presentations , diagnoses , variant terpretation , and clinical actions taken on the basis of these results . patient 1 : a patient with a hotspot somatic variant and a germline pathogenic dicer1 variant patient 1 presented at 3 years of age with a history of left arm and abdominal paan abdominal x - ray was performed , and a left - sided pleural effusion was incidentally noted . 
surveillance for dicer1 - related tumors was initiated for the patients sister ( 6 years old at time of genetic testing ) and included baseline chest ct ( to screen for ppb ) , with a chest x - ray at 8 years of age , annual ultrasound scans of the abdomen and neck ( to screen for ovarian and kidney tumors and thyroid tumors , spectively ) , and annual serum markers to screen for ovarian tumors . 
the father received an annual ultrasound scan of the thyroid gland only , because dicer1 - associated cancers affecting males primarily present in childhood . the bony metastatic lesions completely responded to chemotherapy , and the patient underwent primary mass resection followed by two more cycles of chemotherapy . the resected mass showed mostly viable ppb , with malignant cartilaginous nodules overrun by an anaplastic prostate cancer multinodular goiter s / p thyroidectomy prostate cancer fig 1 . 
patient 1 continued to have disease progression despite chemotherapy , and the decision was made to transition to comfort care . patient 2 : a patient with a germline dicer1 variant of unknown signicance patient 2 initially presented at 3 years of age with a left lower quadrant / pelvic mass . 
remarkably , the patient had an excellent response to therapy and was deemed disease free at age 5 years . at 19 years of age , patient 2 presented to our medical center with severe abdominal and back paimaging revealed concern for new / recurrent widely metastatic disease , because a pelvic mass was noted along with multiple spine and liver lesions . 
palliative radiation was initiated for pain control , and the patient enrolled in the peds - mioncoseq study . sequencing results revealed a germline dicer1 variant of uncertain signicance ( vus ) ( table 1 )  . 
sequencing of the original tumor ( from 3 years of age ) was attempted for comparison / to determine whether this was a metachronous tumor ; however , only sparse , poor - quality material was available , and sequencing could not be performed . 
although vuss are not disclosed per the pedsmioncoseq protocol , at times , a recommendation for clinical germline genetic testing may be made for patients with striking personal / family histories . 
the majority of vuss will be reclassied as likely benign / benign , 22 but for those that are reclassied as likely pathogenic / pathogenic , there can be signicant implications for patients and their relatives . 
patient 2 died at 20 years of age as a result of metastatic disease . patient 3 : a patient with low - level dicer1 mosaicism patient 3 initially presented at 22 months of age with a leftsided pneumonia and pneumothorax . 
a persistent air - lled cystic cavity was present in the left chest and observed with imaging for approximately 3 months before a diserial agnosis of ppb was made after resection of the left lower lobe of the lung . 
regardless , clinical germline genetic testing of dicer1 was recommended but not pursued because of the out - of - pocket cost . approximately 6 months later , patient 3 was enrolled in the peds - mioncoseq study . 
 ( a ) he image ( 40 ) of the original tumor showing mixed morphology with alveolar pattern in the top half and more abundant rhabdomyoblastic differentiation in the lower half . ( b ) he image ( 400 ) of the late recurrence tumor showing spindle - shaped and round cell tumor cells with focal rhabdomyoblastic differentiation . 
as such , no signicant somatic copy number variations , point mutations , indels , or gene fusions were able to be called . no germline variants were considered reportable at this time . this patient also enrolled in the national institutes of healths ( nihs ) pleuropulmonary blastoma dicer1 syndrome study , which includes germline and somatic sequencing , approximately 1 year after initial diagnosis . germline sequencing identied a mosaic germline dicer1 pathogenic variant ( table 1 ; fig 3 ) in 2% of the allelic reads in the patients blood sample . 
both parents enrolled in the study , and their germline testing was negative for the dicer1 pathogenic variant , consistent with the low - level mosaicism detected in the patients blood sample . 
this somatic variant is commonly seen in dicer1 syndromeassociated tumors and involves the rnase iiib domain of dicer1 . analysis of the raw data available from the peds - mioncoseq the germline dicer1 pathogenic study indicates that variant identied by the nih was present in 2% of germline variant reads in our study as well . 
this patient continues to receive annual chest ct scans with no evidence of disease and undergoes annual kidney ultrasound scans , thyroid examinations , and targeted physical examinations as screening for other potential tumors . patient 4 : a patient with a rare dicer1 - associated tumor patient 4 presented at 3 years of age with headaches , photophobia , and hydrocephalus . 
the patient received ve cycles of chemotherapy , consisting of vincristine , etoposide , cyclophosphamide , and cisplatin , with tumor resection performed after the second cycle because of an increase in tumor size . 
the patient also underwent autologous bone marrow transplantation . a year later , an mri scan revealed an enhancing mass overlying the left middle cerebellar peduncle , suggestive of recurrent disease . 
in a previous study , 25 low - level mosaicism in four children with multiple dicer1 - associated tumors in whom no germline dicer1 variant had been identied by conventional sequencing techniques was observed . 
patient 4 contributes to the literature on dicer1 syndrome and illustrates how ics can be useful in identifying germline variants in individuals with rare cancers . from a cancer treatment perspective , all four of these challenging patients revealed dicer1 variants ; however , to date , there are no there are no clinically available pediatric therapies targeting specic mirnas . 
the possibility of targeting mirnas and dicer function in the future is currently being explored.26 from a genetic counseling standpoint , once a germline dicer1 pathogenic variant is identied , germline genetic testing is recommended for rst - degree relatives . 
approximately 13% to 20% of individuals with detectable germline dicer1 pathogenic variants have de novo variants , whereas 80% to 87% are inherited.9 , 27 germline genetic testing can provide tumor risk information to probands and their relatives and provide information regarding recurrence risk for future pregnancies . 
in families where the dicer1 variant is inherited , reports indicate it is uncommon to have multiple individuals diagnosed with ppb ; however , there may be higher penetrance of other manifestations , including goiters and benign lung cysts . 
family members lacking the familial dicer1 mutation do not need surveillance , whereas those who have inherited this variant should be observed according to current surveillance recommendations . screening recommendations at our institution evolved over time and are based on literature review , expert opinion , and patient preferences . 
beyond this age , for female adolescent and adult patients , we discuss symptoms and signs of hormone excess related to sex cordstromal tumors , such as hirsutism , virilization , and menstrual abnormalities . 
for all other manifestations , we recommended a detailed physical examination . recently , consensus guidelines for surveillance were published by the international ppb registry , which are largely in accordance with our institutions age - specic recommendations . 
these guidelines were developed at the rst international dicer1 symposium in may 2016.7 recommendations for surveillance begin in the prenatal period , with a third - trimester ultrasound for detection of large lung cysts that require intervention at birth . 
these differences reect the natural uncertainty in screening approaches for a recently described hereditary tumor syndrome , which aim to integrate the morbidity and the unknown mortality of syndrome - associated tumors , incidence in the target population , and presumed cost effectiveness and patient burden . least 10 years of age and do not tumor and germline sequencing in the pediatric oncology patient population has rapidly expanded in recent years . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . no potential conicts of interest were reported . references peng y , croce cm : the role of micrornas in human cancer . 
nat rev cancer 14 : 662 - 672 , 2014 kurzynska - kokorniak a , koralewska n , pokornowska m , et al : the many faces of dicer : the complexity of the mechanisms regulating dicer gene expression and enzyme activities . 
nucleic acids res 43 : 4365 - 4380 , 2015 kim j , field a , schultz kap , et al : the prevalence of dicer1 pathogenic variation in population databases . 
int j cancer 141 : 2030 - 2036 , 2017 slade i , bacchelli c , davies h , et al : dicer1 syndrome : clarifying the diagnosis , clinical features and management implications of a pleiotropic tumour predisposition syndrome . 
hum mutat 32 : 1381 - 1384 , 2011 schultz kap , williams gm , kamihara j , et al : dicer1 and associated conditions : identication of at - risk individuals and recommended surveillance strategies . clin cancer res 24 : 2251 - 2261 , 2018 8 . 
science 325 : 965 , 2009 brenneman m , field a , yang j , et al : temporal order of rnase iiib and loss - of - function mutations during development determines phenotype in pleuropulmonary blastoma / dicer1 syndrome : a unique variant of the two - hit tumor suppression model . 
schultz ka , pacheco mc , yang j , et al : ovarian sex cord - stromal tumors , pleuropulmonary blastoma and dicer1 mutations : a report from the international pleuropulmonary blastoma registry . 
schultz ka , yang j , doros l , et al : dicer1 - pleuropulmonary blastoma familial tumor predisposition syndrome : a unique constellation of neoplastic conditions . dev pathol 18 : 504 - 511 , 2015 pediatr blood cancer 61 : 1695 - 1697 , 2014 pathol case rev 19 : 90 - 100 , 2014 22 : 564 - 567 , 2014 14 . 
fern andez - martnez l , villegas ja , santamara i , et al : identication of somatic and germ - line dicer1 mutations in pleuropulmonary blastoma , cystic nephroma and rhabdomyosarcoma tumors within a dicer1 syndrome pedigree . 
kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identies pathogenic germline mutations , and directs targeted therapy . 
marks lj , oberg ja , pendrick d , et al : precision medicine in children and young adults with hematologic malignancies and blood disorders : the columbia university experience . 
messinger yh , stewart dr , priest jr , et al : pleuropulmonary blastoma : a report on 350 central pathology - conrmed pleuropulmonary blastoma cases by the international pleuropulmonary blastoma registry . 
therefore , less is known about the prevalence and extent of msi among other types of cancer . methods using our recently published msi - calling software , mantis , we analyzed wholeexome data from 11 , 139 tumor - normal pairs from the cancer genome atlas and therapeutically applicable research to generate effective treatments projects and external data sources across 39 cancer types . 
within a subset of these cancer types , we assessed mutation burden , mutational signatures , and somatic variants associated with msi . results we identified msi in 3.8% of all cancers assessedpresent in 27 of tumor typesmost notably adrenocortical carcinoma ( acc ) , cervical cancer ( cesc ) , and mesothelioma , in which msi has not yet been well described . 
in addition , msi - high acc and cesc tumors were observed to have a higher average mutational burden than microsatellite - stable acc and cesc tumors . conclusion we provide evidence of as - yet - unappreciated msi in several types of cancer . 
2017 by american society of clinical oncology introduction large - scale sequencing projects of cancer genomes have opened the door to studies that have identified putative biomarkers with potential clinical and therapeutic value , among them the presence or absence of microsatellite instability ( msi )  . 
microsatellites are defined as 10 to 60 base pair regions that contain multiple repeats of 1 to 5 base pair motifs.1 microsatellites occur at microsatellite loci , which are widely dispersed throughout the human genome . 
in normal cells , repeat count of microsatellites is verified and maintained during cell division by the mismatch repair ( mmr ) system , 2 , 3 one of many cellular dna repair mechanisms . 
after multiple cycles of cell division , cells with an impaired mmr system will develop varying lengths in their microsatellite sequences . mismatch repair deficiency is known to occur in some tumors , 2 either by somatic hypermutation of mmr genes , most commonly , mlh14 , 5 ; an inherited germline mmr pathway mutation , such as in lynch syndrome6 , 7 ; or double somatic mutations in mmr genes . 
 durable responses and a statistically significant improvement in overall survival.12 msi polymerase chain reaction ( pcr ) and immunohistochemistry are two molecular biology based methods that are in routine use for clinical msi testing . 
msi - pcr analyzes the distribution of microsatellite lengths at five standardized loci ( bethesda panel ) , 14 and immunohistochemistry detects the presence or absence of four proteins that are involved in the mmr pathway ( msh2 , msh6 , mlh1 , and pms2 )  . 
examples of such software include msings , 15 msisensor , 16 and mantis.17 a recent study by our group17 demonstrated that mantis achieves high sensitivity ( 97% ) and specificity ( 99% ) across six cancer typestested using samples with known msi status by msipcrand provides stable performance with varying numbers of microsatellite loci . 
because of this , mantis is particularly well suited for application to a wider variety of cancer types . as clinical msi testing is routinely performed only on colorectal and endometrial tumors , 18 the prevalence of msi in many other cancer types has been less well described . 
in addition , evidence exists that msi - pcr may be less accurate in other cancer types.19 a recent study by hause et al20 developed and applied the msi detection tool , mosaic , to perform a detailed survey of msi across 18 cancer types ( n = 5 , 930 cases ) ; however , many other cancer types have yet to be analyzed for msi . 
the ability to detect msi in novel cancer types would permit the investigation of immuneenhancing therapies in these cancers , with the potential to benefit previously unknown subsets of patients with cancer with msi . to perform a more comprehensive assessment of msi across many additional cancer types than those analyzed by hause et al , our study determined the prevalence of msi in 39 distinct cancer types ( n = 11 , 139 tumors from 11 , 080 patients ) by using our previously published msi - calling tool , mantis . methods data preprocessingthe cancer genome atlas and therapeutically applicable research to generate effective treatments for analysis , 10 , 701 cases of paired tumor - normal whole - exome sequencing data were obtained from the cancer genome atlas ( tcga ) 21 - 44 and therapeutically applicable research to generate effective treatments ( target ) 45 , 46 projects . 
data from all of these cases , with the exception of diffuse large b - cell lymphoma ( dlbcl ) were processed via our in - house automated pipeline , l - map ( landscape microsatellite analysis pathway )  . 
l - map is implemented in python and mysql and was run on the oakley supercomputer at the ohio supercomputing center.47 first , the metadata for all dna whole - exome bam files were downloaded from the genomic data commons ( gdc ) 48 and were converted to sql database entries . 
premarked duplicate reads were removed as above . data preprocessingother sources four hundred thirty cases of paired tumor - normal whole - exome sequencing data were obtained from the sequence read archive51 : 338 chronic lymphocytic leukemia cases from 279 patients from landau et al , 52 32 cutaneous t - cell lymphoma cases from choi et al , 53 51 nasopharyngeal carcinoma cases from zheng h et al , 54 and 8 cholangiocarcinoma cases from ong et al.55 fifteen additional cholangiocarcinoma cases were obtained from the european nucleotide archive56 from chan - on et al.57 all sample identifiers used are available in the data supplement . these cases were processed via l - map . 
coordinates for 2 , 539 microsatellite loci within or near the exomeoriginally introduced by salipante et al15 and used by later studies17 were converted from hg19 to hg38 by using liftover.61 nine unlifted loci were discarded , which left 2 , 530 regions that were used for analysis with mantis in all cohorts , with the exception of dlbcl ( data supplement )  . 
mantis was run with authorrecommended settings for whole - exome data minimum read quality , 20 ; minimum locus quality , 25 ; minimum locus coverage , 20 ; minimum repeat reads , one ; all other settings left at defaults . eight samples were observed to have fewer than 10 loci sufficiently covered and were dropped . 
variant annotation was performed by using annovar ( version 201602 - 01 ) 63 and gnu parallel.64 somatic mutations in the repair genes msh2 , msh6 , mlh1 , pms2 , exo1 , pold1 , and pole were determined by filtering variants with a dann68 , 69 pathogenicity score greater than 0.96 ( included in annovar )  . this threshold for dann was chosen as it was previously shown to provide optimal sensitivity and specificity.69 mutational signature calling was performed by using the tool deconstructsigs70 with the nature 2013 signatures set , which contains 27 signatures , 71 and the exome2genome normalization method . 
of 2 , 530 loci , we identified 22 loci that , within at least five cohorts , had an msi - h versus mss difference score greater than 0.75 and were sufficiently covered by at least 50% of samples in the cohort ( appendix table a2 )  . 
note that for chronic lymphocytic leukemia ( cll ) , the listed msi prevalence in panel a is out of 279 patients , and all 338 tumors are shown in panel b . 
acc , adrenocortical carcinoma ; aml , pediatric acute myeloid leukemia ( target ) ; blca , bladder carcinoma ; brca , breast carcinoma ; cesc , cervical squamous cell carcinoma and endocervical adenocarcinoma ; chol , cholangiocarcinoma ; coad , colon adenocarcinoma ; ctcl , cutaneous t - cell lymphoma ; dlbc , diffuse large b - cell lymphoma ; esca , esophageal carcinoma ; gbm , glioblastoma multiforme ; hnsc , head and neck squamous cell carcinoma ; kich , kidney chromophobe ; kirc , kidney renal clear cell carcinoma ; kirp , kidney renal papillary cell carcinoma ; laml , acute myeloid leukemia ( tcga ) ; lgg , lower - grade glioma ; lihc , liver hepatocellular carcinoma ; luad , lung adenocarcinoma ; lusc , lung squamous cell carcinoma ; meso , mesothelioma ; nbl , pediatric neuroblastoma ; npc , nasopharyngeal carcinoma ; ov , ovarian serous cystadenocarcinoma ; paad , pancreatic adenocarcinoma ; pcpg , pheochromocytoma and paraganglioma ; prad , prostate adenocarcinoma ; read , rectal adenocarcinoma ; sarc , sarcoma ; skcm , skin cutaneous melanoma ; stad , stomach adenocarcinoma ; tcgt , testicular germ cell tumor ; thca , thyroid carcinoma ; thym , thymoma ; ucec , uterine corpus endometrial carcinoma ; ucs , uterine carcinosarcoma ; uvm , uveal melanoma ; wt , wilms tumor . were within the set of 22 top - performing loci . these results indicate a striking heterogeneity of msi patterns across various types of cancer . all four disease types with the highest rates of msi prevalence were lynch syndromeassociated tumor types that have been previously known to exhibit msi : endometrial carcinoma , colon adenocarcinoma , gastric adenocarcinoma , and rectal adenocarcinoma . 
somatic variant calling was performed on whole - exome samples from these four cancer types , and the mean absolute number of somatic mutationsboth nonsynonymous and synonymouswas found to be increased among msi - h versus mss tumors within their own cohorts ( fig 3 )  . 
p values were calculated by using two - sided fishers exact test ( using signature presence or absence ) , with benjamini correction for multiple hypotheses.78 mmr pathway alterations msi - h lynch syndromeassociated tumors are known to lack the expression or function of at least one mmr protein ; therefore , we analyzed somatic mutations that were predicted to be deleterious ( by dann68 ) in the mmr genes msh2 , msh6 , mlh1 , pms2 , and exo1 , and the proofreading dna polymerases pold1 and pole , among msi - h and mss samples within acc , cesc , and meso ( appendix table a3 ; data supplement )  . 
although pold and pole are not considered mmr proteins , mutations in these genes have been shown to lead to somatic hypermutation.22 , 79 within these cohorts , 64% of msi - h cases and 7% of mss cases were found to contain at least one predicted deleterious somatic mutation in at least one of these genes ; however , given that these samples were sequenced with potentially different exome captures , together with the increased mutational burden of msi - h tumors , we could not determine the statistical significance of this finding . discussion in this study , we have performed , to our knowledge , the largest analysis of msi in human cancer exomes to date , including 11 , 139 whole - exome tumor - normal pairs from 39 types of cancer . compared with a study by hause et al , 20 we mantis score mantis score mantis score ascopubs.org / journal / po jco precision oncology 5 fig 2 . 
kernel density plots of mantis scores within ( a ) adrenocortical carcinoma ( acc ) , ( b ) cervical squamous cell carcinoma and endocervical adenocarcinoma ( cesc ) , and ( c ) mesothelioma ( meso )  . 
somatic mutational burden correlates with microsatellite instability high ( msi - h ) status within adrenocortical carcinoma ( acc ) and cervical squamous cell carcinoma and endocervical adenocarcinoma ( cesc )  . mutational burden is listed for ( a ) acc , ( b ) cesc , and ( c ) mesothelioma ( meso )  . 
previous studies of msi in acc have implicated lynch syndrome as a risk factor for familial acc80 , 81 ; however , to our knowledge , ngs - based msi analysis has not yet been applied to acc . msi - h colorectal tumors have been previously shown to be exceptionally sensitive to therapy with pd - 1 immune checkpoint inhibitors.12 identification of msi in novel tumor types may lead to an expanded role for immunotherapy and a broader scope of clinical msi testing.82 in addition , msi is known to be prognostic within colorectal cancer , 83 which may apply in other cancer types as well . 
clinical trials of immune checkpoint inhibitors are beginning or are underway in acc ( clinicaltrials.gov identifier : nct02673333 ) , cesc ( clinicaltrials.gov identifier : nct02635360 ) , and meso ( clinicaltrials.gov identifiers : nct02784171 , nct02991482 , nct02707666 , and nct02399371 ) , and a previous study of dendritic cell immunotherapy in acc84 demonstrated tumor marker but not clinical response . these studies may benefit from the retrospective evaluation of msi - h as a biomarker . 
prospective expansion of clinical msi testing to other cancer types may enlighten the prognostic and predictive value of msi - h for noncolorectal cancers . mmr deficiency is well recognized as the predominant cause of msi within colorectal , endometrial , and gastric cancers . 
if future studies indicate that msi in acc , cesc , and / or meso is indeed a result of mmr deficiency , the findings of this study may implicate previously unappreciated cancer types as being part of lynch syndrome . 
compared with germline alterations in mmr genes , somatic events are most often a result of hypermethylation of cpg islands in the promoter region of mlh1.4 additional investigation is needed to elucidate other molecular mechanisms that can lead to msi , as well as the downstream effects of msi on tumor - specific biology . 
in addition , of 9 , 569 tumors assessed in this study not within colorectal , endometrial , or gastric cancer , 77 ( 0.8% ) were msi - h . 
only 14 of these were within acc , cesc , or meso , which compromised the statistical power of our mutational signature analysis . a larger cohort of msi - h tumors would permit more comprehensive studies , including correlation with clinical data . in summary , we have detected msi in multiple cancer types , including acc , cesc , and meso , which indicates that msi may affect nonlynch syndrome tumor types . 
kautto no relationship to disclose affiliations all authors : the ohio state university , columbus , oh . support sameek roychowdhury stock and other ownership interests : johnson & johnson ( i ) research funding : takeda , ignyta acknowledgment we thank current and past members of the roychowdhury laboratory for their helpful insight and discussion . 
the chronic lymphocytic leukemia sequencing data ( dbgap : phs000922.v1.p1 ) used in this work was supported by national human genome research institute large - scale sequencing program grant no . 
kane mf , loda m , gaida gm , et al : methylation of the hmlh1 promoter correlates with lack of expression of hmlh1 in sporadic colon tumors and mismatch repair - defective human tumor cell lines . 
study of two large midwestern kindreds . 812 - 816 , 1993 arch intern med 117 : 206 - 212 , 1966 imai k , yamamoto h : carcinogenesis and microsatellite instability : the interrelationship between genetics and epigenetics . 
boland cr , thibodeau sn , hamilton sr , et al : a national cancer institute workshop on microsatellite instability for cancer detection and familial predisposition : development of international criteria for the determination of microsatellite instability in colorectal cancer . 
niu b , ye k , zhang q , et al : msisensor : microsatellite instability detection using paired tumor - normal sequence data . chem 60 : 1192 - 1199 , 2014 bioinformatics 30 : 1015 - 1016 , 2014 17 . 
giardiello fm , allen ji , axilbund je , et al : guidelines on genetic evaluation and management of lynch syndrome : a consensus statement by the us multi - society task force on colorectal cancer . 
faulkner rd , seedhouse ch , das - gupta ep , et al : bat - 25 and bat - 26 , two mononucleotide microsatellites , are not sensitive markers of microsatellite instability in acute myeloid leukaemia . 
cancer genome atlas research network : comprehensive genomic characterization of squamous cell lung cancers . nature 489 : 519 - 525 , 2012 [ erratum : nature 491 : 288 , 2012 ] 24 . 
hoadley ka , yau c , wolf dm , et al : multiplatform analysis of 12 cancer types reveals molecular classification within and across tissues of origcell 158 : 929 - 944 , 2014 33 . 
zheng s , cherniack ad , dewal n , et al : comprehensive pan - genomic characterization of adrenocortical carcinoma . cancer cell 29 : 723 - 736 , 2016 [ erratum : cancer cell 30 : 363 , 2016 ] 42 . 
zheng h , dai w , cheung akl , et al : whole - exome sequencing identifies multiple loss - of - function mutations of nf - kb pathway regulators in nasopharyngeal carcinoma . 
chan - on w , nairismagi m - l , ong ck , et al : exome sequencing identifies distinct mutational patterns in liver flukerelated and non - infection - related bile duct cancers . 
oleary na , wright mw , brister jr , et al : reference sequence ( refseq ) database at ncbi : current status , taxonomic expansion , and functional annotation . 
quang d , chen y , xie x : dann : a deep learning approach for annotating the pathogenicity of genetic variants . bioinformatics 31 : 761 - 763 , 2015 69 . 
bacher jw , flanagan la , smalley rl , et al : development of a fluorescent multiplex assay for detection of msi - high 1113 - 1120 , 2013 tumors . 
gatalica z , vranic s , xiu j , et al : high microsatellite instability ( msi - h ) colorectal carcinoma : a brief review of predictive biomarkers in the era of personalized medicine . 
challis bg , kandasamy n , powlson as , et al : familial adrenocortical carcinoma in association with lynch syndrome . j clin endocrinol metab 101 : 2269 - 2272 , 2016 81 . 
patterns of mutational signatures ( s ) across microsatellite instability cancers : ( a ) adrenocortical carcinoma ( acc ) , ( b ) cervical squamous cell carcinoma and endocervical adenocarcinoma ( cesc ) , and ( c ) mesothelioma ( meso )  . 
listed are the number of samples ( mss or msi - h ) with at least one predicted deleterious mutation in msh2 , msh6 , mlh1 , pms2 , exo1 , pold1 , and pole . mutations were called by using mutect ( variant calling in methods ) and included in this table if the dann pathogenicity score was  . 
velez - velez1 ; horacio asbun , md1 ; and gerardo colon - otero , md1 introduction solid pseudopapillary neoplasms ( spns ) of the pancreas are rare , accounting for between 1% and 2% of all pancreatic tumors.1 - 5 these tumors are primarily seen in young women between the ages of 20 and 40 years who usually present with large pancreatic masses.1 , 2 surgical resection is highly effective , with 5 - year survival rates of 95% in patients able to have a complete resection.3 - 5 a recent retrospective review of spn cases treated surgically in the united states from 2004 to 2013 as part of the national cancer database identied 369 cases , with a 9.6% incidence of positive surgical margins and a 95.5% 5 - year overall survival.6 an english medical literature review up to december 2003 found a total of 718 well - documented published cases of spn of the pancreas.5 among 497 cases with adequate data , 97 ( 19.5% ) had evidence of either metastasis or local invasion.5 the most common sites of invasion or metastasis were the liver ( n = 27 ) , portal vein ( n = 26 ) , and spleen ( n = 17 ) .5 radiation is frequently used when margins of surgical resection are positive . 
surgical resection of metastasis is recommended whenever feasible , given the frequently indolent nature of the disease , with long - term diseasefree survival noted.6 - 8 given the rarity of this disease and the highly favorable outcomes with complete surgical resection , there is no standard of care for the systemic management of unresectable recurrent or metastatic disease.7 hao et al9 recently reported a meta - analysis of all aggressive spn cases , including locally invasive , recurrent , or metastatic tumors , reported in the english medical literature.9 a total of 59 patients were included in this review , most of whom ( 91.5% ) were able to undergo a curative resection . 
a 5 - year disease - free survival rate of 26.8% with a 5 - year overall survival of 71.1% was noted in this series.9 the presence of unresectable disease at presentation and recurrence within 3 years of initial diagnosis correlated with worse outcomes.9 we report a case of a patient with unresectable spn , treated with neoadjuvant chemotherapy followed by attempt at surgery and radiation therapy , who developed rapidly progressing biopsy - proven liver metastasis . 
an ultrasound - guided biopsy of the mass was positive for neoplasm and showed cells positive for cd10 and - catenin and negative for cytokeratin 7 , cam5.2 , p16 , pax - 8 , chromogranin , and synaptophysin , thus conrming the diagnosis of spn . involvement of blood vessels , the tumor was considered unresectable . 
there was some mild reduction in the tumor , which was followed by a pyloricpreserving total pancreatectomy with vascular construction of the superior mesenteric vein ( smv ) and the portal veat the time of surgery , the pancreatic mass was readily evident and was noted to involve the transverse colon mesentery , which was subsequently resected . 
 jorgensen et al context key objective is everolimus of potential benet in the treatment of patients with unresectable metastatic solid pseudopapillary neoplasms ( spns ) of the pancreas ? knowledge generated a patient with aggressive metastatic spn of the pancreas to the liver with ctnnb1 and pten mutations had a sustained signicant response to everolimus treatment , with excellent tolerability . 
a review of the literature shows no data on the frequency of pten mutations in spn tumor of the pancreas and no previous reported cases of everolimus treatment of spns . 
there are limited data on the effectiveness of systemic treatments in this rare tumor . relevance given the lack of standard treatments for metastatic unresectable spn of the pancreas , this case illustrates the potential role for genomic testing in this rare cancer . 
vascular reconstruction of the smv and the portal vein was performed using an 8 - mm ringed polytetrauoroethylene graft . mri of the abdomen and pelvis taken 6 weeks postoperatively showed recurrent tumor in the midabdomen with encasement of the sma and both replaced hepatic arteries ( fig 2 )  . 
a computed tomography scan performed 9 months postoperatively was consistent with liver metastases , which were conrmed on biopsy ( fig 3a )  . comprehensive genomic proling was performed on the primary tumor specimen using foundationone ( foundation medicine , cambridge , ma ) that revealed the following genomic alterations : ctnnb1 d32y and pten g165fs * 2 , y16fs * 1 pathogenic mutations . 
figure 4 summarizes the evaluation and treatment timeline . discussion spns are uncommon pancreatic neoplasms that typically present with localized disease , with excellent long - term prognosis after complete surgical resection . 
 ( c ) ct scan taken 18 months postoperatively showing continued response . current literature providing specic details on systemic treatments for unresectable , recurrent and / or metastatic spns of the pancreas is mostly limited to case reports ( table 1 )  . 
responses in single - case reports have been described with a combination chemotherapy regimen of ifosfamide , cisplatin , and etoposide , 11 with hyperthermic intraperitoneal chemotherapy with oxaliplatin and irinotecan , and with infusional uorouracil , leucovorin , and oxaliplatin ( folfox ) .12 , 13 selective intrahepatic radiation therapy was successful in controlling hepatic metastasis in a patient with recurrent disease.14 tamoxifen has been associated with stable disease in one case report.15 isolated case reports of different combination chemotherapy regimens listed in table 1 had failed to show signicant responses.13 , 16 a patient with metastatic disease responded to folfox chemotherapy.13 neoadjuvant treatment of unresectable spns with singleagent gemcitabine , with a combination of cisplatin , ifosfamide , etoposide , and vincristine , and with concomitant uorouracil and radiation therapy , have been shown to be effective in single - case reports.11 , 18 , 19 these treatment approaches resulted in signicant tumor size reductions , making surgical resection possible . 
in another report of a patient with unresectable hepatic metastases , treatment with intrahepatic perfusions with melphalan resulted in stable disease for 10 months.21 another report of a patient with multiple liver metastases after surgical resection of spn treated with intra - arterial chemotherapy ( cisplatin , doxorubicin , and uorouracil ) and systemic therapy with gemcitabine and erlotinib failed to provide long - lasting responses.2 a liver transplantation was ultimately performed in this patient , with no recurrence on follow - up 1 year after transplantation.2 in the case reported here , comprehensive genomic prole of the tumor revealed ctnnb1 and pten pathogenic mutations . 
 jorgensen et al ( 83% ) , and 14 of 14 ( 100% ) spn tumors analyzed , for an average of 90.3% ; therefore , ctnnb1 alterations have been implicated in the pathogenesis of spns.24 - 26 besides the wnt / - catenin pathway , whole - genome mrna expression analyses of 14 spn tumors by kim et al6 showed that genes involved in activation of the hedgehog and androgen receptor signaling pathways are also differentially up - regulated in spns compared with pancreatic adenocarcinomas , neuroendocrine tumors , and non - neoplastic pancreatic tissues . 
a proteomic analysis demonstrated upregulation of proteins that directly interact with the key proteins of notch , hedgehog , and androgen receptor signaling pathways.27 these ndings have paved the way to the development of many preclinical and clinical studies exploring cancer therapies that aim to exploit loss of pten function and investigating the role of pten loss in tumorigenesis and resistance to cancer therapy.25 there are limited data available on the frequency of pten mutations in spn tumors . 
pten was not listed as one of the genes that was down regulated in spn in the studies reported by kim et al6 and cavard et al.28 although inhibitors of the mtor pathway , such as everolimus , have been effective in decreasing growth of pten - decient tumors in preclinical studies , clinical studies in several tumor subtypes have yielded mixed results.29 the phosphatase and tension homolog ( pten ) tumor suppressor gene is a potent regulator of the phosphatidylinositol 3 - kinase / akt / mammalian target of rapamycin ( mtor ) pathway , which stimulates cell growth , proliferation , and survival . 
deciencies in pten due to mutations or homozygous loss , as in the case reported here , tumor subtypes . are frequently found across different everolimus ( rad - 001 [ 40 - o - ( 2 - hyrdoxyethyl ) - rapamycin ] ) is an orally administered rapamycin analog with various indications approved by the us food and drug administration , including advanced renal cell carcinoma , progressive pancreatic neuroendocrine tumors , renal angiomyolipoma , and subependymal giant cell astrocytoma associated with tuberous sclerosis.30 - 32 everolimus table 1 . 
 everolimus in spn pancreas adverse effects include stomatitis , rash , fatigue , infection , pulmonary toxicities , hyperglycemia , anemia , and thrombocytopenia.31 because genetic alterations or loss of pten have been proposed as predictors of sensitivity to everolimus independently of advanced tumor type , we hypothesized that the spn recurrence in our patient might be responsive to everolimus.30 , 32 the effective use of everolimus on the basis of low level of pten expression has also been reported in a patient with metastatic renal medullary carcinoma , another rare type of tumor without well - dened management.33 moreover , a study using a mouse model with a gain - of - function mutation in the - catenin gene and homozygous deletion of pten in cells of the mouse ovary to study ovarian endometrioid adenocarcinoma showed that dysregulation of wnt and pten signaling pathways resulted in increased mtor activity and more aggressive tumors.34 the same group showed that mtor inhibition with rapamycin reduced tumor growth in these mice . these data and our patients ndings suggest that the pten mutation may have contributed to the aggressiveness of her tumor . 
recently , results from a phase ii trial provided encouraging evidence that treatment with the mtor inhibitor temsirolimus in combination with chemotherapy improves progression - free survival in patients with advanced endometrial cancer with identied tsc2 somatic mutations.35 similar to oncogenic alterations in pten , tsc2 mutations are also known to cause aberrant activation of the phosphatidylinositol 3 - kinase / akt / mtor pathway . 
these data suggest that the combination of bevacizumab and everolimus might be of added benet in tumors with ctnnb1 and pten mutations like our patients tumor . in summary , this unique patients experience suggests that metastatic spn tumors with pathogenic mutations of ctnnb1 and pten may have signicant long - term benet from treatment with everolimus . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . gerardo colon - otero research funding : novartis ( inst ) no other potential conicts of interest were reported . references reddy s , cameron jl , scudiere j , et al : surgical management of solid - pseudopapillary neoplasms of the pancreas ( franz or hamoudi tumors ) : a large singleinstitutional series . 
j am coll surg 208 : 950 - 957 , discussion 957 - 959 , 2009 dovigo ag , daz mb , g utierrez mg , et al : liver transplantation as treatment in a massive metastasis from gruber - frantz pancreatic tumor : a case report . transplant proc 43 : 2272 - 2273 , 2011 vollmer cm , jr . , dixon e , grant dr : management of a solid pseudopapillary tumor of the pancreas with liver metastases . 
hpb 5 : 264 - 267 , 2003 casanova m , collini p , ferrari a , et al : solid - pseudopapillary tumor of the pancreas ( frantz tumor ) in children . 
med pediatr oncol 41 : 74 - 76 , 2003 papavramidis t , papavramidis s : solid pseudopapillary tumors of the pancreas : review of 718 patients reported in english literature . 
j am coll surg 200 : 965 - 972 , 2005 leraas hj , kim j , sun z , et al : solid pseudopapillary neoplasm of the pancreas in children and adults : a national study of 369 patients . 
j pediatr hematol oncol 40 : e233 - e236 , 2018 kim cw , han dj , kim j , et al : solid pseudopapillary tumor of the pancreas : can malignancy be predicted ? surgery 149 : 625 - 634 , 2011 lubezky n , papoulas m , lessing y , et al : solid pseudopapillary neoplasm of the pancreas : management and long - term outcome . 
hao eu , hwang hk , yoon d - s , et al : aggressiveness of solid pseudopapillary neoplasm of the pancreas : a literature review and meta - analysis . 
gao h , gao y , yin l , et al : risk factors of the recurrences of pancreatic solid pseudopapillary tumors : a systematic review and meta - analysis . 
rebhandl w , felberbauer fx , puig s , et al : solid - pseudopapillary tumor of the pancreas ( frantz tumor ) in children : report of four cases and review of the 12 . 
krug s , bartsch dk , schober m , et al : successful selective internal radiotherapy ( sirt ) in a patient with a malignant solid pseudopapillary pancreatic neoplasm 15 . 
hofmann h , von haken r , werner j , et al : unresectable isolated hepatic metastases from solid pseudopapillary neoplasm of the pancreas : a case report of chemosaturation with high - dose melphalan . 
abraham sc , klimstra ds , wilentz re , et al : solid - pseudopapillary tumors of the pancreas are genetically distinct from pancreatic ductal adenocarcinomas and almost always harbor beta - catenin mutations . 
lee l , ito t , jensen rt : everolimus in the treatment of neuroendocrine tumors : efcacy , side - effects , resistance , and factors affecting its place in the treatment sequence . 
lipkin js , rizvi sm , gatalica z , et al : therapeutic approach guided by genetic alteration : use of mtor inhibitor in renal medullary carcinoma with loss of pten 8 : 55582 - 55592 , 2017 expression . 
tanwar ps , zhang l , kaneko - tarui t , et al : mammalian target of rapamycin is a therapeutic target for murine ovarian endometrioid adenocarcinomas with dysregulated wnt / - catenin and pten . 
these results highlight the importance of screening for ntrk fusions as part of the tumor genomic proling for patients with pediatric cancer . jco precis oncol 5 : 204 - 214 . 
2021 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction rearrangements involving the neurotrophic tyrosine receptor kinase ( ntrk ) genes ntrk1 , ntrk2 , and ntrk3 encode fusion proteins containing the intact ntrk kinase domain that are oncogenic drivers of a histologically diverse group of tumors . 
 ntrk fusions in pediatric tumors : frequency , partner , and outcome content key objective ntrk fusions are tumor - agnostic or age - independent biomarkers that identify patients suitable for treatment with the us food and drug administrationapproved trk inhibitors . 
this single institutional study examined the frequency , fusion partner , and clinical outcome of ntrk fusions in a large cohort of unselected patients with pediatric cancer . knowledge generated our study demonstrated that ntrk fusions are more frequent in pediatric tumors and involve a broader panel of fusion partners and a wider range of tumors those than previously recognized and highlights pediatric cancers in which ntrk fusions are more or less likely to occur . relevance this study provided important ndings regarding ntrk fusionpositive pediatric cancers and cancers where ntrk fusions are rarely seen . 
immunohistochemistry was performed in a subset of cases using pan - trk antibody ( abcam , cambridge , uk , 1 : 100 dilution ) ( table 1 )  . fusion gene detection was performed using the chop cancer fusion panel as previously described.15 briey , targetspecic primers covering 673 exons were custom designed to identify known fusion genes and potential novel fusion genes associated with 110 cancer genes using anchored multiplex polymerase chain reaction ( pcr ) technology ( archerdx , inc , boulder , co )  . 
all fusions , when identied in our laboratory for the rst time , were conrmed by nested pcr followed by sanger sequencing . mutations ( single nucleotide variants [ snvs ] and small insertion / deletions [ indels ] ) and copy number alterations ( cnas ) were evaluated by using the chop hematological malignancy panel ( chmp ) or solid tumor panel ( cstp ) as described previously.16 briey , genomic dna was extracted from the tumor samples . 
libraries were prepared using probes targeting 118 genes ( chmp ) or 238 genes ( cstp ) , respectively , and sequenced on illumina hiseq platform using 150 bp paired - end sequencing . 
sequence data were analyzed using the home brew software concords v2 ( for snvs and indels ) and nextgene v2 next - generation sequencing analysis software ( for cnas ; softgenetics , llc , state college , pa )  . 
clinically signicant variants including indels , and cnas were conrmed by sanger sesnvs , quencing , multiplex ligation - dependent probe amplication ( mlpa ) , real - time pcr , or droplet digital pcr ( ddpcr ) when necessary . 
by contrast , different ntrk fusions were present in tumors with the same histological diagnosis , such as kctd16 - ntrk2 and trim24 - ntrk2 in two male patients of similar age with ganglioglioma , who grade i ( table 1 )  . 
in ptc , tumorigenesis is associated with constitutive activation of the mapk and pi3k signaling pathways secondary to somatic point mutations in braf , pten , dicer1 , and ras as well as fusions involving ret , alk , and ntrk.3 , 23 gene fusions have been reported in both sporadic and radiation - induced ptcs and are more common in pediatric ( 50% - 60% ) compared with adult tumors ( approximately 15% ) .2 , 23 ret and ntrk fusions are the most common , reported in 25%30% and approximately 10% ( range , 0% - 26% ) of pediatric ptcs , respectively.2 , 23 ntrk3 fusions are usually observed more commonly in ptcs than ntrk1 fusions , 2 , 23 which is similar to what we observed in our patient cohort . 
all the ptcs in our cohort were sporadic , none associated with ntrk1 ntrk2 ntrk3 snvs / indels cnas 10 - 15 16 - 20 gender female male snvs and indels missense frameshift inframe cnas gain loss gain and loss cnloh fig 1 . 
case 17 demonstrates a low - grade tumor with strn3 - ntrk3 showing moderately cellular spindle to round cell proliferation with prominent vascular proliferation ( c , h&e , 200 )  . 
case 21 shows widely invasive follicular variant of papillary thyroid carcinoma with etv6 - ntrk3 demonstrating extrathyroidal extension and angioinvasion ( d , h&e , 50 ) and nuclear features of papillary thyroid carcinoma ( inset , 400 )  . 
two cases demonstrate the diffuse sclerosing variant of papillary thyroid carcinoma showing solid and papillary groups inltrating the thyroid parenchyma with numerous psammomatous calcications ( e , h&e , 100 )  . 
the data are limited but suggest that the presence of an ntrk fusion may have diagnostic , prognostic , and therapeutic signicance in ptcs and may hold clinical utility for stratifying surgical and medical care . 
standard therapy for advanced ptcs in children involves surgical resection of gross disease followed by radioactive - iodide ( rai ) therapy . in a recent multicenter , open - label phase i or ii study of larotrectinib for the treatment of pediatric patients with solid tumors , two children with advanced ptcs were treated for  . 
7 months and remained progression - free , although , unfortunately , the objective response to treatment was not reported.25 ntrk fusions in pediatric cns tumors all the cns tumors identied with ntrk fusions were either gliomas or mixed neuronal glial tumors . 
four of the six ntrk2 fusions were novel fusions at the time of discovery with different 5 ( cid : 1 ) - partner genes including kank1 , c2orf4 , kctd16 , and specc1l . 
ntrk fusion genes have been described in pediatric lowand highgrade gliomas at a low prevalence , 26 although one study reported a nding of 40% of nonbrainstem high - grade gliomas in children younger than 3 years old containing an ntrk fusion gene ( n = four of the 10 samples ) .27 six of the 7 ntrk fusionpositive cns tumors were low - grade gliomas ( lgg ) , which may be partially due to the higher frequency of lgg in our unselected pediatric cohort ( approximately 45% of all cns tumors )  . 
although the duration of follow - up in our study is limited , the majority of patients underwent standard of care for their cns tumor subtype with resection of the primary tumor without recurrence . 
larotrectinib and entrectinib have shown antitumor effect for both primary brain tumors and solid tumors with brain metastases with systemic administration suggesting adequate penetration of the blood - brain barrier.11 in a study of nine patients with primary cns tumors treated with ntrk inhibitors , disease control was observed in all evaluable patients with stable disease in seven patients . 
some tumors exhibited typical age , morphology , and etv6 - ntrk3 fusion compatible with if , showing densely cellular fascicular growth of primitive ovoid cells and inltration of surrounding tissue ( cases 13 and 14 )  . 
clinical classication and treatment based on histology only , particularly in soft - tissue tumors with spindle morphology , have proven to be challenging in some cases because of variable histologic features and immunohistochemical patterns.30 as more tumors are being studied for fusions , the morphologic spectrum is expanding , such that the fifth edition of the soft tissue and bone tumors who classication31 now includes an emerging entity titled ntrk - rearranged spindle cell neoplasm to encompass spindle cell soft - tissue tumors with ntrk gene rearrangements ( other than if )  . 
it remains to be seen if soft - tissue histologic classication , molecular classication , or some combination of both will provide clinicians with the most accurate information for personalized treatment . 
magnetic resonance imaging at diagnosis ( a ) , 1 month post - targeted therapy ( b ) , and 5 months post - therapy ( c ) showing marked tumor shrinkage . 
at diagnosis , the tumor contained densely cellular areas with spindled to round cells and increased mitosis ( d , h&e 400 ) with cytoplasmic and membranous pan - trk immunohistochemistry ( inset )  . 
ccd , coiled - coil domain ; chd , calponin homology domain ; ecd - lb , extracellular ligand binding domain ; h&e , hematoxylin and eosin staining ; pkt , protein tyr kinase ; tm , transmembrane domain ; ss , signal sequence . ntrk fusions facilitate precision diagnosis , prognosis , and therapy follow - up information is available for all patients , and follow - up times ranged from 6 to 46 months . 
in almost all cases , the detection of an ntrk fusion conrmed the morphologic diagnosis , and in ve cases , the nal tumor diagnosis was largely based on the discovery of an ntrk fusion ( excluding other differential diagnostic considerations )  . 
one exception was the case of secretory carcinoma , which was initially diagnosed as mucoepidermoid carcinoma , but later changed to secretory carcinoma following the detection of the etv6 - ntrk3 and additional immunohistochemical evaluation ( case 10 )  . 
collectively , we analyzed 261 common embryonal solid tumors ( 79 neuroblastomas , 29 medulloblastoteratoid / rhabdoid mas , 28 wilms tumors , 13 atypical tumors , and 11 hepatoblastomas ) , bone tumors ( 27 osteosarcomas and 24 ewing sarcomas ) , and skeletal muscle tumors ( 50 rhabdomyosarcomas ) , and none had ntrk fusions . 
thus , although it is difcult to exclude the possibility that ntrk fusions might occur in individual tumors of these subtypes , which accounted for about one third of all solid tumors in this cohort , they are likely to be rare . case 15 was a 6 - month - old male infant with a left upper extremity mass . 
prospectively , the rest of the patients who survived with the standard therapy may also benet from trk inhibitor therapy if their tumors progress or recur . received neoadjuvant we assessed the clinical outcome of all ntrk fusionpositive patients for up to 46 months ( median 21 months )  . 
the median follow - up time for patients with cns tumors was 21 months . the majority of ntrk - positive lgg demonstrated superb outcome with gross total resection without additional therapy . one patient with congenital glioblastoma and an etv6ntrk3 fusion died 3 months after birth , and the tumor specimen was obtained via autopsy . 
our review of 1 , 217 patients showed that ntrk fusions are more frequently seen in pediatric tumors than in adult tumors and involve a broader panel of fusion partners and a wider range of pediatric tumors than previously recognized . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / cci / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . elizabeth fox other relationship : helsinn therapeutics gerald b . 
wertheim employment : johnson & johnson stock and other ownership interests : johnson & johnson vinodh pillai consulting or advisory role : foundation medicine travel , accommodations , expenses : foundation medicine jennifer e . 
genes ( basel ) 10 : 723 , 2019 prasad ml , vyas m , horne mj , et al : ntrk fusion oncogenes in pediatric papillary thyroid carcinoma in northeast united states . 
hsiao sj , zehir a , sireci an , et al : detection of tumor ntrk gene fusions to identify patients who may benet from tyrosine kinase ( trk ) inhibitor therapy . 
nat rev clin oncol 15 : 731 - 747 , 2018 suurmeijer aj , dickson bc , swanson d , et al : the histologic spectrum of soft tissue spindle cell tumors with ntrk3 gene rearrangements . 
papadopoulos kp , gandhi l , janne pa , et al : first - in - human study of ds - 6051b in patients ( pts ) with advanced solid tumors ( ast ) conducted in the us . 
drilon a , ou si , cho bc , et al : repotrectinib ( tpx - 0005 ) is a next - generation ros1 / trk / alk inhibitor that potently inhibits ros1 / trk / alk solventfront mutations . 
lopez gy , perry a , harding b , et al : cdkn2a / b loss is associated with anaplastic transformation in a case of ntrk2 fusion - positive pilocytic astrocytoma . neuropathol appl neurobiol 45 : 174 - 178 , 2019 19 . 
surrey lf , jain p , zhang b , et al : genomic analysis of dysembryoplastic neuroepithelial tumor spectrum reveals a diversity of molecular alterations dysregulating the mapk and pi3k / mtor pathways . 
tuttle rm , haugen b , perrier nd : updated american joint committee on cancer / tumor - node - metastasis staging system for differentiated and anaplastic thyroid cancer ( eighth edition ) : what changed and why ? thyroid 27 : 751 - 756 , 2017 25 . 
laetsch tw , dubois sg , mascarenhas l , et al : larotrectinib for paediatric solid tumours harbouring ntrk gene fusions : phase 1 results from a multicentre , 26 . 
okamura r , boichard a , kato s , et al : analysis of ntrk alterations in pan - cancer adult and pediatric malignancies : implications for ntrk - targeted theropen - label , phase 1 / 2 study . 
nat genet jones ka , bossler ad , bellizzi am , et al : bcr - ntrk2 fusion in a low - grade glioma with distinctive morphology and unexpected aggressive behavior . 
robinson gw , gajjar aj , gauvain km , et al : phase 1 / 1b trial to assess the activity of entrectinib in children and adolescents with recurrent or refractory solid tumors including central nervous system ( cns ) tumors . 
mandrekar , phd1 with the launch of the national cancer institutes precision medicine initiative in 2015 , there has been a shift to trial designs that tailor health care solutions to individual patients by using a screening platform and by moving away from the one - trial / one - biomarker - at - a - time approach . 
2019 by american society of clinical oncology introduction precision medicine takes into account the variability of an individual patients genes , environment , and lifestyle when deciding the best approach for disease prevention and treatment.1 since the rst publication of the human genome in february 2001 , 2 scientists have made great progress in understanding inherited differences in genes , making precision medicine a tangible reality . 
even though precision medicine is a relatively new term , tailoring intervention on the basis of a patients specic features is not a new idea . many currently available us food and drug administration ( fda ) approved therapies are based on specic patient subgroups . 
for example , rituximab , the rst monoclonal antibody treatment for cancer , was approved by the fda in 1997 for patients with relapsed or refractory cd20 + , b - cell , low - grade , or follicular non - hodgkin lymphoma . 
the addition of cetuximab to rst - line chemotherapy in patients with kras wild - type metastatic colorectal cancer has been shown to signicantly improve treatment outcomes compared with chemotherapy alone in two randomized clinical trials , crystal ( clinicaltrials.gov identier : nct00154102 ; cetuximab combined with irinotecan in first - line therapy for metastatic colorectal cancer ) 3 and opus ( clinicaltrials.gov identier : nct00125034 ; oxaliplatin and cetuximab in first - line treatment of metastatic colorectal cancer [ mcrc ] ) .4 erlotinib and crizotinib are fda - approved therapies for patients with advanced lung cancer who test positive for an epidermal growth factor receptor ( egfr ) mutation and the alk rearrangement , respectively . 
it was later found that patients with higher programmed death - ligand 1 expression treated with pembrolizumab had longer progression - free survival ( pfs ) and overall survival ( os ) .5 most recently , on may 23 , 2017 , the fda granted accelerated approval to pembrolizumab as the treatment for adult and pediatric patients with unresectable or metastatic microsatellite instability - high or mismatch repair decient solid tumors , 6 which is the rst time that the fda has approved a cancer treatment for an indication on the basis of a common biomarker rather than the primary site or origin ( ie , tissue agnostic ) .7 there are continuing efforts in drug development to move away from the one - size - ts - all approach and toward precision medicine . in this article , we aim to introduce novel trial designs by using case studies as examples . 
 ou et al context key objective to discuss types of clinical trial designs for accelerating development of new drugs in the era of precision medicine . knowledge generated clinical trial designs ( such as umbrella , basket , and subgroup ) that evaluate multiple hypotheses are efcient precision medicine initiatives . 
other designs include enrichment designs for validating the efcacy of an agent in biomarker - driven subgroups and window of opportunity designs to help understand the antitumor activity of an agent in a treatment - naive patient population . relevance the clinical trial designs discussed in this article are practical and relevant for precision medicine trials . 
several case studies are provided to demonstrate the utility of these clinical trial designs . the results of tumor gene sequencing or other testing techniques , such as polymerase chain reaction , ow cytometry , uorescence in situ hybridization ( fish ) , chromogenic in situ hybridization , and immunohistochemistry . 
specic to genotype - driven trials , patients will be matched to trials that are developed on the basis of prior understanding of certain molecular aberrations that may determine sensitivity to certain therapies . 
if a patient is eligible for more than one genotype - driven trial , the trial will be selected by the treating physician on the basis of the totality of information , such as the patients preferences and status , expected benets , and molecular characteristics . 
enrichment designs test selective therapeutic options for matching patients that can result in better patient outcomes.9 the genotype - driven trial mentioned in the case study is one type of enrichment design ; other types of enrichment , such as that based on the epigenome , is also appropriate . 
enrichment trial design is best suited when the rationale for the trial strongly suggests that the agent would be effective in a specic biomarkerdened patients with a specific tumor type with biomarker status unknown may be part of the trial protocol biomarker profiling with targeted biomarker trial enrollment with targeted therapy without targeted biomarker standard of care fig 1 . 
it is particularly advantageous if the biomarker used to dene the patient population is considered soc ; if so , the trial design does not need to take into account the molecular testing because the information would be available for all patients . 
highly specic screening tests are required to identify the low - prevalence molecular prole and to avoid assigning patients who tested false positive to treatment options that may not be efcacious . 
finally , certain molecular proles may have low prevalence and may result in a large proportion of screened patients receiving the soc , which can be inefcient ( eg , if the prevalence of the molecular prole of interest is only 5% , 500 patients will need to be proled to identify 25 patients who are potentially eligible )  . umbrella design umbrella trials include patients with a single tumor type or disease and for which several biomarkers have been identied and used to dene disease subtypes.10 patients are screened for a panel of biochemical , genetic , and / or immunologic markers associated with their disease and , on the basis of the markers detected , assigned to a biomarkerdriven treatment strategy or targeted therapy that is most likely to result in favorable outcomes . 
thus , an umbrella trial consists of multiple substudies , each with independent subgroups of patients receiving different therapies and with the option of assuming different statistical parameters for independent designs . 
the substudies , however , exist under an overarching master protocol that uses a common infrastructure for screening and treatment assignment to reduce the cost and time associated with enrollment to unrelated and often sequential biomarker - informed studies . 
lung - map ( clinicaltrials.gov identier : nct03851445 ; a master screening protocol previously - treated non - small cell lung cancer ) is an example of a phase ii / iii umbrella study in solid tumors.11 lung - map opened to accrual in 2014 for patients with advanced squamous cell carcinoma ( scc ) of the lung . similar to aml , scc of the lung is a biologically complex disease . 
roughly 60% of patients with lung scc harbor genetic abnormalities that might be targeted with therapy.14 lung - map provided a common infrastructure to test patient samples for multiple biomarkers , which informed therapy assignment within 10 to 14 days . 
patients were assigned to a substudy according to a predened algorithm that used specic genetic abnormalities detected via ngs in patients with a specific tumor type biomarker profiling targeted biomarker 1 targeted biomarker 2 targeted biomarker 3 targeted biomarker n no actionable biomarker regimen a regimen b regimen c regimen n standard of care or non - targeted regimen fig 2 . 
a substudy of new therapy versus soc remained open for patients without an actionable biomarker . lung - map was designed to test new therapies against soc for a particular subgroup using multiple , randomized phase ii trials with pfs as the primary end point . 
within a substudy , if a new therapy met criteria that suggested large the substudy was expanded to improvements in pfs , a phase iii study with pfs and os as co - primary end points . patients who were part of the phase ii interim analysis were included in the phase iii assessment . 
with a well - established screening platform in place , an umbrella trial design can be quite efcient in directing patients into different treatment regimens and accelerating the drug development process . 
the concept of umbrella trials can be applied in any disease setting , but it is most appropriate when there is a strong scientic rationale informing which therapies might work best in biomarker - dened subgroups . 
although not used in beat aml or lung - map , adaptive randomization can be applied within a substudy that has multiple arms to assign patients to a therapy that shows the most favorable outcome , given the data already collected.1 , 15 , 16 bayesian posterior probabilities that compare efcacy of experimental therapy with soc can be used in decision making . umbrella trials are exible and have the ability to open or close new substudies with different targeted therapies or statistical designs if appropriate . basket design basket trials are an efcient way of screening experimental therapeutics across patients with a variety of tumor types and / or histology under one master trial . 
basket trials involve several biomarker proles whereby patients are assigned to treatments based on the molecular alterations their tumors contain , regardless of the histologic type of the tumor.17 , 18 the basic premise for this trial design is that the average response to one or more experimental treatments is expected to vary across these different biomarker proles . like umbrella trials , there may be a common genetic screening platform , especially if the cohorts dened by the study are histology - independent and dened only by the presence of a single molecular aberration . 
figure 3 provides a generic representation of a basket trial design schema . basket trial designs may be appropriate when there is reason to believe that one or more experimental treatments may be effective across a range of primary tumor sites or histologies , and in particular , when patients with specic biomarker proles are expected to respond well to a particular treatment , regardless of their specic disease or histology . 
one such design is the bayesian basket design.20 in this design , a bayesian approach is used to model the response probabilities for the various histologic strata , and two hypotheses are considered : ( 1 ) the response probabilities for a particular targeted agent are equal across the corresponding histologic strata , and ( 2 ) the activity of the drug is independent across these strata . 
a hierarchical bayesian design has recently been proposed for randomized phase ii trials with multiple groups ( or baskets ) , allowing for information sharing across baskets while at the same time having the ability to help with decision making for each individual trial or basket.21 within the hierarchical bayesian design framework , the estimate of the treatment effect for each phase ii trial basket within this master protocol shrunk toward the overall mean treatment effect , which alleviates concerns regarding randomness across the trials or baskets.21 , 22 this approach is most powerful when the treatment effects are heterogeneous across the different baskets and inates the type i error in the inferior treatment effect groups or baskets in the case of heterogeneous treatment effects across baskets . 
it has been noted that the results of a basket trial can be heavily tilted toward positive conclusions , 23 even with specication of weak priors in a bayesian setting . 
the goal of this study , as noted in the publication , was to identify molecular biomarkers and determine their frequency and clinical relevance in patients with advanced nonsmall - cell lung cancer , and thymic malignancies and to evaluate the efcacy of multiple targeted therapies in specic molecular subsets of patients.27 ( p1001 ) a limitation of this trial was the lack of the lung cancer , small - cell adaptive trial feature , because seamless addition of new treatment arms for molecular targets or replacing treatments for a particular molecular subtype was not possible . another issue was the timeliness of the availability of some of the core molecular proling results , which had an impact on enrollment to the trial.27 acs e and tapur case studies . 
the french national cancer institutes acs e initiative ( secured access to innovative therapies ) 28 and ascos tapur trial ( clinicaltrials.gov identier : nct02693535 ; testing the use of food and drug administration [ fda ] approved drugs that target a specic abnormality in a tumor gene in people with advanced stage cancer ) 29 are examples of large - scale trials with basket - type design that evaluate the safety and efcacy prole of approved agents in other indications ( ie , tumor types )  . 
the goals of these trials are to provide patients with advanced diseases ( without promising treatment options ) off - label access to approved agents and to evaluate the safety and efcacy of these agents outside their approved indications . 
the acs e - crizotinib trial ( clinicaltrials.gov identier : nct02034981 ; phase 2 study assessing efcacy and safety of crizotinib in patients harboring an alteration on alk , met or ros1 ) is the rst trial coordinated by the acs e prograit includes patients with various solid and hematologic malignancies . 
basket designs test a single agent in different histologic subtypes , which can be efcient if the goal is to screen for antitumor activity of the agent in different disease settings . 
for example , only two ( nsclc with egfr mutations and nsclc with kras or braf mutations ) of the 15 substudies in the custom trial completed accruing ; accrual was unsuccessful for the other 13 rare histologic subtypes . 
 ou et al experimental therapy in the subgroup of patients positive for the biomarker as well as in either the subgroup of patients negative for the biomarker or in all patients . 
with co - primary objectives , the signicance level ( ) is allocated or split between the two objectives to maintain an acceptable overall type i family - wise error rate using a conservative bonferroni correction or a less conservative correction that considers the correlation between the two tests.31 in the case with co - primary objectives dened for the biomarker - positive subgroup and all patients , the design can be subgroup focused or all - population focused.32 a subgroup - focused design is most appropriate when there is evidence that the experimental therapy will be most effective in patients with the biomarker of interest , but it could also have a broad impact in the general disease population . 
a design with an all - population focus is most appropriate when there is less evidence that the experimental therapy will be most effective in patients with the biomarker of interest but could be effective in the general disease population . 
with an accrual goal of 618 patients egfr - positive by fish , there was 92% power to detect a hazard ratio of 0.75 for pfs in the cetuximab arm relative to the control arm with a type i error rate ( ) of 2% . 
with an accrual goal of 1 , 546 total patients , there was 86% power to detect a hazard ratio of 0.83 for os in the cetuximab arm relative to the control arm with a one - sided of 1.5%. 
because of slow accrual and a lower - than - expected percentage of patients who were egfr positive , the study was amended to 400 egfrpositive patients to detect planned differences in pfs with 80% power . 
 case studies for innovative trial designs multiple hypotheses in a subgroup design allows formal testing of efcacy for a biomarker - dened subgroup of patients and the overall patient population . 
by testing multiple hypotheses , the power for testing a specied effect in the overall population is reduced.32 furthermore , in a subgroup - focused design , as the prevalence of a biomarker decreases , the total sample size increases.32 costs also increase because tissue procurement and biomarker testing is required for all patients to reach the target number of subgroup patients.33 these additional resources can be offset by testing for larger treatment effects in the biomarker - dened subgroup.32 window of opportunity design the primary goal of window of opportunity ( woo ) design , is to unalso known as window or phase 0 design , derstand the antitumor activity of an agent in a disease state that is not disrupted by previous or simultaneous treatments . 
these trials occur between patient diagnosis and initiation of standard treatment and typically have a clinical end point such as tumor response or pfs at a predened early time point , often assessed by radiographic imaging ( figure 5 )  . 
woo designs are distinct from neoadjuvant trial settings , in which an investigational agent is commonly given preoperatively along with cytotoxic chemotherapy or hormonal therapy for a longer period of time than in a woo trial . 
woo trials have recently gained attention , specically in the context of evaluating molecular agents or in early advanced or metastatic disease in which the tumor may not be resistant to selective inhibition of a novel cancer target.38 evaluating molecular end points can be hindered by difculties in procuring tumor tissue before and after drug administration and by heterogeneity in previous exposure to cancer therapies . 
woo trials help to overcome these difculties by enrolling treatment - nave patients , including a translational research component , and occurring in a short time frame before the initiation of the standard treatment of the disease . 
the ultimate hope of woo trials is that they can expedite the drug development process by improving understanding of an agents biologic effect early in its development , validating markers that may predict subsets of patients who will benet , and targeting select short courses of experimental treatment diagnosis of disease standard of care ( eg , surgery ) standard treatment option fig 5 . 
it is a design best suited for trials in which the treatment cycles are short , and a short - term outcome ( eg , biomarker change ) is the end point of interest . 
in addition , although it is not yet documented , there is the theoretical possibility that the investigational agent may in fact induce resistance to subsequent therapies . logistically , woo trials require careful coordination among members of a multidisciplinary study team because diagnosis , workup , and study treatment must all be arranged in a short time frame . 
furthermore , tumor heterogeneity can be an issue , and thus it is essential to have the infrastructure capable of performing a centralized and high - quality review of all biomarkers.40 woo trials were initially used to inform a go / no - go decision in development of anticancer agents , to expose a small number of patients to a limited duration and dose of a drug and subsequently proceed to phase i / ii trials on the basis of the results.41 ( p2574 ) woo trials may not be advantageous in settings in which an agent has already been well - studied in other disease setfor which the toxicity prole is already welltings , understood , or even for which little safety data are available regarding the risk of delaying surgery.40 despite these concerns and considerations , woo trials have proved benecial in some settings . 
 ou et al active in untreated patients.42 , 43 woo trials should therefore be considered as a promising alternative trial design . discussion with the ability to simultaneously evaluate the effects of therapies on multiple biomarkers and diseases , umbrella and basket trial designs can help accelerate the discovery of targeted therapy . 
because each substudy of the umbrella and basket trials is essentially an enrichment trial design , we would expect a larger effect size , given the available prior knowledge of certain genotype proles and their sensitivity to therapy . 
woo trials allow investigators to understand the antitumor activity of an agent in the de novo disease setting . trial designs in the precision medicine era require a platform to carry out the biomarker proling . 
given the advances in liquid biopsies , cell - free dna from plasma may provide a minimally invasive alternative to standard tumor biopsies.44 even though we have more options for proling patients , the proling is not without challenge . 
at the same time , a screening cut point will need to be established and validated to ensure the cut point value ( ie , the high and low levels of the biomarker value to predict the response to treatment ) is appropriate.45 in an early work , mandrekar et al46 outlined the criteria for choice of phase ii designs for initial validation of a predictive marker in a review article that considered assay performance , turnaround time , preliminary evidence , and marker prevalence . with the advances in targeted therapy , we now have many therapeutic options for specic targeted biomarkers ; however , mutations that have high prevalence in a certain disease may not be common in another ( for example , human epidermal growth factor receptor 2 overexpression has been reported in approximately 15%47 of patients with breast cancer but only approximately 2% of patients with colorectal cancer ) .48 designing a trial with a biomarker target with extremely low prevalence is a challenge because it is difcult to obtain a sufcient number of patients to properly power the study . 
a statistical trial design that uses small sample sizes is needed to tackle this issue , as well as potentially international partnerships . in this article , we have focused our discussion on trial designs that are better suited for phase ii and iii studies . 
seamless phase i / ii designs , which blur the distinction between dose selection and efcacy evaluation , are one such design . hobbs et al49 provided an overview of the use of seamless designs in rst - in - human studies based on abstracts submitted to asco annual meetings from 2010 to 2017 and provided guidance on the design and conduct of such trials . 
to validate biomarker associations identied from such studies , sufcient statistical rigor is still required , such as clear denition of the primary end point , a prespecied interim and nal analysis plan , and well - dened safety monitoring rules . with immunotherapy gaining traction in oncology , it uncertain whether the current designs can adequately address the needs for these agents . 
if the primary objective is to show efcacy in a biomarker - dened , tumor - specic patient population , then both enrichment design and umbrella design ( ie , as one of the substudies ) are applicable . 
as mentioned in the introduction , pembrolizumab received the rst tissue - agnostic fda approval , and there may be several factors that could have contributed to successfully ling for approval of pembrolizumab.50 first , the tissue collection in the initial randomized pembrolizumab trials allowed investigators to retrospectively test the tissue - agnostic hypothesis . 
second , immunotherapies are designed with a strong foundation of preclinical data . third , multiple prospective clinical trials have veried the hypotheses generated by the retrospective data that contributed to its approval . 
in the case of pembrolizumab , approval was based on the data from ve different trials in which patients were retrospectively identied from two studies and prospectively enrolled in three studies.7 because this design is the rst of its kind , it is unclear which design discussed in this article will be best suited for future agents targeting tissue - agnostic indications . 
nature 409 : 860 - 921 , 2001 van cutsem e , k ohne ch , hitre e , et al : cetuximab and chemotherapy as initial treatment for metastatic colorectal cancer . 
n engl j med 360 : 1408 - 1417 , 2009 bokemeyer c , bondarenko i , makhson a , et al : fluorouracil , leucovorin , and oxaliplatin with and without cetuximab in the rst - line treatment of metastatic colorectal cancer . 
j clin oncol 27 : 663 - 671 , 2009 daud ai , wolchok jd , robert c , et al : programmed death - ligand 1 expression and response to the anti - programmed death 1 antibody pembrolizumab in melanoma . 
clin cancer res [ epub ahead of print on february 20 , 2019 ] zardavas d , maetens m , irrthum a , et al : the aurora initiative for metastatic breast cancer . 
br j cancer 111 : 1881 - 1887 , 2014 tsimberidou am , wen s , hong ds , et al : personalized medicine for patients with advanced cancer in the phase i program at md anderson : validation and landmark analyses . 
herbst rs , gandara dr , hirsch fr , et al : lung master protocol ( lung - map ) : a biomarker - driven protocol for accelerating development of therapies for squamous cell lung cancerswog s1400 . 
burd a , levine rl , shoben a , et al : initial report of the beat aml umbrella study for previously untreated aml : evidence of feasibility and early success in molecularly driven phase 1 and 2 studies . 
lopez - chavez a , thomas a , rajan a , et al : molecular proling and targeted therapy for advanced thoracic malignancies : a biomarker - derived , multiarm , multihistology phase ii basket trial . 
herbst rs , redman mw , kim es , et al : cetuximab plus carboplatin and paclitaxel with or without bevacizumab versus carboplatin and paclitaxel with or without bevacizumab in advanced nsclc ( swog s0819 ) : a randomised , phase 3 study . 
herbst rs , kelly k , chansky k , et al : phase ii selection design trial of concurrent chemotherapy and cetuximab versus chemotherapy followed by cetuximab in advanced - stage non - small - cell lung cancer : southwest oncology group study s0342 . 
kim es , moon j , herbst rs , et al : phase ii trial of carboplatin , paclitaxel , cetuximab , and bevacizumab followed by cetuximab and bevacizumab in advanced nonsquamous non - small - cell lung cancer : swog s0536 . 
lynch tj , patel t , dreisbach l , et al : cetuximab and rst - line taxane / carboplatin chemotherapy in advanced nonsmall - cell lung cancer : results of the randomized multicenter phase iii trial bms099 . 
pirker r , pereira jr , von pawel j , et al : egfr expression as a predictor of survival for rst - line chemotherapy plus cetuximab in patients with advanced nonsmall - cell lung cancer : analysis of data from the phase 3 flex study . 
machiels jp , bossi p , menis j , et al : activity and safety of afatinib in a window preoperative eortc study in patients with squamous cell carcinoma of the head 40 . 
schmitz s , caballero c , locati ld : perspectives on window of opportunity trials in head and neck cancer : lessons from the eortc 90111 - 24111 - noci - hncg and neck ( scchn )  . 
clark pi , slevin ml , joel sp , et al : a randomized trial of two etoposide schedules in small - cell lung cancer : the inuence of pharmacokinetics on efcacy and 44 . 
our real - time tumor sequencing program , which makes precision treatment decisions for patients with cancer , produces matched germline information , providing a unique opportunity to efficiently implement pharmacogenetics and benefit patients . methods the germline genetic database from the michigan oncology sequencing ( mi - oncoseq ) program was searched for 21 clinically actionable polymorphisms in five cancer - relevant genes : tpmt , dpyd , cyp2c19 , cyp3a5 , and ugt1a1 . 
the medical records of mi - oncoseq patients with actionable phenotypes were searched for receipt of relevant drugs and to determine whether having genetic information at the time of treatment would have led to a treatment recommendation . results all nine variants in tpmt , dpyd , and cyp2c19 that were detected in mi - oncoseq were confirmed by external genotyping . 
on the basis of retrospective assessment of 115 adult and pediatric patient records , 4.3% ( n = 5 ) had a potentially clinically actionable phenotype for tpmt , dpyd , or cyp2c19 and received a relevant medication . 
 after accounting for differences in adult and pediatric recommendations , three of these patients could have received a treatment recommendation at the time of prescribing . conclusion germline genotype determinations for tpmt , dpyd , and cyp2c19 can be used to make evidence - based treatment recommendations in mi - oncoseq patients . 
 although the proportion of patients for whom recommendations can be made is small , this added value to mi - oncoseq and patient care comes at no additional genotyping cost . 
2018 by american society of clinical oncology introduction the genomes of patients ( germline ) and their tumors ( somatic ) each provide useful information to guide precision medicine in oncology . 
vali dated pharmacogenetic associations exist for several germline polymorphisms with com monly used cancer treatments , including thiopu rines ( tpmt ) , 1 fluorouracil ( fu ) / capecitabine ( dpyd ) , 2 irinotecan ( ugt1a1 ) , 3 and tacrolimus ( cyp3a5 ) .4 additionally , there are several known associations with supportive care agents com monly used in patients during treatment , such fungal prophylaxis with voriconazole ( cyp2c19 ) 5 and antiemetic treatment with ondansetron ( cyp2d6 ) .6 despite their established clinical validity , few of these associations have been implemented into clinical practice . 
st jude childrens research hospital has led the way , implementing pre emptive pharmacogenetic testing to guide per sonalized treatment of several genedrug pairs.7 the experiences of early adopters has identified formidable challenges to implementing phar macogenetics into clinical practice , 8 , 9 which require substantial investment and expertise.10 , 11 daniel l . 
mody arul chinnaiyan author affiliations and support information ( if applicable ) appear at the end of this article . the content is solely the responsibility of the authors and does not necessarily represent the official views of the national institutes of health . corresponding author : daniel l . 
although there is debate about the necessity and feasibility of demon strating clinical utility for pharmacogenetic implementation , 12 , 13 the lack of uptake indicates that health systems are not willing to incur the costs of pharmacogenetic implementation for unproven clinical benefit . 
however , available germline genetic information should be con sidered when making treatment decisions.14 in anticipation of a time when genetic informa tion is available for many patients , perhaps as a result of the proliferation of directtoconsumer genotyping , 15 the pharmacogenetic community has developed evidencebased pharmacogenetic treatment guidelines.3 , 16 in oncology , there has been a tremendous expan sion in the availability of genetic information as a result of the proliferation of tumor sequenc ing programs that use somatic genetic informa tion to personalize selection of targeted cancer treatments.17 although some programs analyze only the somatic genome , others have found that matched germline analysis improves quality control18 and enables simultaneous assessment of familial predisposition to cancer.19 this cre ates a unique situation in which germline genetic information for clinically relevant pharmaco genes is freely available.20 however , the oppor tunity to use these data in clinical practice has not yet been capitalized upon . the michigan oncology sequencing ( mi oncoseq ) program at the university of michi gan comprehensive cancer center ( umccc ) performs targeted sequencing of somatic and matched germline dna , in addition to somatic wholetranscriptome analysis . 
21 the targeted sequencing panel includes approximately 100 pharmacogenes that could be used to provide evidencebased pharmacogenetic treatment rec ommendations , if the accuracy of the germline genetic determinations are verified . 
detailed study information including inclusion and exclusion criteria , data analysis and processing , and return of results has been pre viously published.2123 briefly , patients treated at umccc with refractory tumors are invited to participate in a research protocol in which they provide tumor and blood samples for matched genetic sequencing , among other somatic anal yses . 
 since the initiation of mioncoseq , the dna sequencing platform has transitioned from wholeexome sequencing to a targeted exon sequencing panel , and sequencing methods have been previously described in detail.21 , 23 this tar geted panel sequences primarily exonic regions of approximately 1 , 700 genes , including approx imately 100 pharmacogenes selected based on curation within pharmgkb ( appendix table a1 )  . 
these five genes were selected based on their relevance to cancer treatment or sup portive care , likelihood of clinician interest in prospective implementation of the genedrug pairs , and existence of evidencebased treatment guidelines from the clinical pharmacogenet ics implementation consortium ( cpic ) 16 or the dutch pharmacogenetics working group ( dpwg ) .3 the polymorphisms in each gene were selected based on the validated variant lists within each guideline . 
note that ugt1a1 * 28 ( rs8175347 ) and * 80 ( rs887829 ) were both included to represent the ugt1a1 * 28 geno type , because they are highly linked , and * 80 is often substituted for * 28 as a result of its relative ease of genotyping.24 the mioncoseq germ line genetic database was screened to identify all variant calls at any of these polymorphisms for all patients sequenced on onco1700_v4 , and variant calls were compiled in a single data set for further analysis . confirmatory genotyping genotype determinations from onco1700 were manually screened for potentially unreliable calls by assessing standard sequencing quality con trol parameters , including read depth . 
in the second stage , polymor phisms with > five but < 30 occurrences were selected , by prioritizing patients who also car ried a variant at one of the common snp posi tions . 
finally , as many samples as necessary were selected that carried these common variants so that each variant was represented in five samples . selected samples were sent for college of american pathologistsaccredited , clinical lab oratory improvement amendmentsapproved genotyping at genelex laboratories ( seat tle , wa )  . 
genotypes were obtained using a laboratorydeveloped , multiplex polymerase chain reactionbased test followed by single base primer extension for variant detection by mass spectrometry ( massarray analyzer 4 system ; agena bioscience , san diego , ca )  . 
percent concordance for each snp was calculated as the number of concordant genotypes divided by the total number of samples compared . retrospective analysis of clinically actionable phenotypes patient genotypes were translated to activity phenotypes based on the appropriate cpic26 or dpwg3 guidelines ( appendix table a2 )  . 
genotype data for ugt1a1 * 28 ( * 80 ) and cyp3a5 * 3 was only available for the 25 samples sent for confirma tory genotyping ; therefore , these patients and genotypes were included in assessments of clin ical usefulness . 
medical record screening was performed using an automated screening tool ( emerse27 ) that searches the text of notes in michart , the version of epic used at mich igan medicine . 
text used to screen the medical records included all generic and brand drug names and commonly used acronyms ( eg , fu for fluourouracil )  . a pharmacy student , in consultation with a phar macist with oncology pharmacogenomic expertise , manually reviewed the electronic medical record for each patient who had an actionable pheno type and received the relevant drug to determine whether a treatment modification would have been recommended had this genetic information been available to the clinician before treatment initia tion . 
these patients represent the diversity of the mioncoseq cohort , including adult ( n = 82 ; 71% ) and pediatric patients ( n = 33 ; 29% ) who were evenly divided between male ( n = 58 ; 50% ) and female sex ( n = 57 ; 50% ) , were primarily white ( n = 97 ; 84% ) , and had a variety of solid ( n = 80 ; 70% ) and liquid tumor types ( n = 35 ; 30% )  . no genotype determinations for cyp3a5 * 3 , ugt1a1 * 28 , or ugt1a1 * 80 were made by onco1700 because of low read depth ( cyp3a5 * 3 and ugt1a1 * 80 ) or sequence repeat misalign ment ( ugt1a1 * 28 ) ; therefore , these polymor phisms were excluded from genotype concordance analyses . 
across the 18 remaining snps , a total of 139 variant calls were made in these 115 samples , and nine unique snps were detected in at least one patient ( table 1 )  . 
the frequency of actionable phenotypes was highest for cyp2c19 ( 43.5% ) , followed by cyp3a5 ( 20% ) , ugt1a1 ( 20% ) , and tpmt ( 13% ) , and lowest for dpyd ( 3.5% ) , as expected . the electronic medical record for each patient carrying an actionable phenotype was screened for relevant drugs . 
one patient with cyp2c19 rapid metabolizer phenotype never received voriconazole ; two patients with cyp2c19 rapid metabolizer phenotype received voriconazole treatment , but they were pediatric patients , so no dose adjustment is recommended per cpic guidelines5 ; and one patient with ugt1a1 poor metabolizer phenotype treated with irinotecan received a standard pediatric dose ( 49 mg / m2 ) , which is below the recommended threshold for dose adjustment based on dpwg guidelines.3 three patients with actionable phenotypes who received the relevant drug , in whom a treatment recommendation could have been made , were identified . 
one patients dose was held after 5 days because of neutro penia ( absolute neutrophil count [ anc ] , 200 ) , and the second patients dose was reduced to 70% of the standard dose after 7 days because of neutropenia ( anc , 500 )  . 
 are many challenges to pharmacogenetic imple mentation , 10 but perhaps the primary challenge is the current lack of evidence of clinical util ity to justify the upfront cost of establishing a pharmacogenetic service.31 , 32 in anticipation of a future in which genomic information is more readily available , cpic and other groups have published evidencebased treatment recommen dations for patients with known genotypes.3 , 16 there is a unique opportunity to integrate evidencebased pharmacogenetic treatment into tumor sequencing programs that analyze germline genetic information , 20 such as the mioncoseq program at umccc.21 the objective of this analysis was to confirm the accuracy of germ line genotype determinations produced during mioncoseq sequencing and then to retrospec tively assess the clinical usefulness of integrating pharmacogenetics into mioncoseq . attempted confirmatory genotyping of 21 clin ically actionable snps in five cancerrelevant pharmacogenes confirmed genotyping accu racy for common and uncommon variants in three genes ( tpmt , dpyd , and cyp2c19 ) but revealed an inability to genotype common vari ants in cyp3a5 and ugt1a1 . 
this finding is easily explained by the targeted exonic coverage of onco1700 and the location of these polymor phisms at a splice site ( cyyp3a5 * 3 , rs776746 ) and in the promoter region ( ugt1a1 * 28 , rs8175347 )  . 
other variants that were not detected are extremely rare , and several have not been found in white patients . prior studies have estimated that > 90% of the population has an actionable phenotype of at least one candidate gene33 , 34 ; however , this is only relevant if the patient is treated with the drug of interest and the guidelines apply to the patient . 
 in our cohort , 4% ( five of 115 ) of patients had a potentially actionable phenotype in cyp2c19 , tpmt , or dpyd and received the relevant drug , and in 2.6% ( three of 115 ) of patients , a guideline based treatment recommendation could have been made . manual review of these three patients identified several interesting findings . 
despite tpmt gen otype information available at the time of treat ment , two patients with heterozygous genotypes initiated treatment at standard mercaptopurine doses , per the childrens oncology group protocols on which they were enrolled . 
cpic recommends a preemptive 30% to 70% dose decrease with enhanced monitoring and titration based on tolerability.1 although germline tpmt determination from mioncoseq would not have changed these patients treatment in any way , it would have prevented external genetic testing , resulting in cost savings to the health systethe third patient carried a dpyd geno type that confers risk of severe toxicity with fu , which was not known at the time of treatment . 
 cpic guidelines recommend a preemptive dose reduction of 50% with monitoring and titra tion.2 although it is impossible to attribute tox icity to any single factor , it is interesting that two patients experienced toxicity requiring a reactive dose reduction , which may have been prevented if care had been based on cpic guidelines . the 2% to 4% absolute increase in the propor tion of patients with clinically actionable findings from germline pharmacogenetics represents a minimal estimate , because the emerse screen ing tool does not automatically screen prescrib ing data , and there is some chance that a patient with an actionable phenotype received a relevant medication that was never mentioned in a clini cal note . 
regardless , this represents a meaning ful increase in the clinically actionable findings from our tumor sequencing program.35 in addi tion to its usefulness for quality control , 18 , 36 matched germline analysis identifies validated cancer predisposition variants in an estimated 15% of patients.19 several tumor sequencing programs , including mioncoseq , 21 use their matched germline dna for this purpose.37 , 38 our results represent a critical first step toward integration of germline pharmacogenetics into mioncoseq . although several programs have reported that pharmacogenetics is considered in their deci sion making , 39 , 40 we are not aware of any detailed reports of the integration of pharmacogenetics into these programs . 
 used to inform irinotecan treatment decisions3 or how the incidental finding of gilberts syn drome would be conveyed to the patient.42 , 43 generalization of our estimate of the proportion of patients who could benefit from pharmacog enetic implementation in other tumor sequenc ing programs is challenging for several reasons . 
 first , there are differences in the frequencies of clinically actionable alleles or phenotypes among racial cohorts.44 additionally , institutional differ ences in the distribution of tumors that are treated and sent for sequencing could dramatically affect this estimate . 
 pharmacogenetic integration would be most ben eficial in programs that sequence tumors early in treatment , particularly at institutions that treat many pediatric patients with all . the proportion of patients who would benefit from pharmacogenetic implementation could be increased in several ways . 
mody , arul chinnaiyan substantial upfront investment to build and maintain clinical decision support within the electronic health record , hire or train individu als with pharmacogenetic expertise , and provide clinician and patient education . 
pharmacoge netic implementation within tumor sequencing programs that analyze matched germline dna is particularly efficient because there is no geno typing cost and the bioinformatic workflow to detect actionable germline phenotypes can be integrated into the existing infrastructure . 
additional work is necessary to develop infrastructure to embed active clini cal decision support into the electronic health record so that actionable phenotypes can be stored and used indefinitely.7 , 11 in conclusion , onco1700 produces reliable germline pharmacogenetic information for three clinically relevant pharmacogenes ( tpmt , dpyd , and cyp2c19 )  . 
elliott ls , henderson jc , neradilek mb , et al : clinical impact of pharmacogenetic profiling with a clinical decision support tool in polypharmacy home health patients : a prospective pilot randomized controlled trial . 
caudle ke , dunnenberger hm , freimuth rr , et al : standardizing terms for clinical pharmacogenetic test results : consensus terms from the clinical pharmacogenetics implementation consortium ( cpic )  . 
hanauer da , mei q , law j , et al : supporting information retrieval from electronic health records : a report of university of michigans nineyear experience in developing and using the electronic medical record search engine ( emerse )  . 
luzum ja , pakyz re , elsey ar , et al : the pharmacogenomics research network translational pharmacogenetics program : outcomes and metrics of pharmacogenetic implementations across diverse healthcare systems . 
ji y , skierka jm , blommel jh , et al : preemptive pharmacogenomic testing for precision medicine : a comprehensive analysis of five actionable pharmacogenomic genes using nextgeneration dna sequencing and a customized cyp2d6 genotyping cascade . 
stockley tl , oza am , berman hk , et al : molecular profiling of advanced solid tumors and patient outcomes with genotypematched clinical trials : the princess margaret impact / compact trial . 
crews kr , gaedigk a , dunnenberger hm , et al : clinical pharmacogenetics implementation consortium ( cpic ) guidelines for codeine therapy in the context of cytochrome p450 2d6 ( cyp2d6 ) genotype . 
hicks jk , bishop jr , sangkuhl k , et al : clinical pharmacogenetics implementation consortium ( cpic ) guideline for cyp2d6 and cyp2c19 genotypes and dosing of selective serotonin reuptake inhibitors . 
elvin , md , phd1 purpose vulvar squamous cell carcinoma ( vscc ) encompasses two predominant variants : one associated with detectable high - risk strains of human papillomavirus ( hrhpv ) and a second form often occurring in the context of chronic dermatitis in postmenopausal women . 
sixty - one percent of hpv + vsccs had a pathogenic alteration in the pi3k / mtor pathway , whereas hpv vsccs showed alterations in tp53 , tertp , cdkn2a , ccnd1 , and egfr , and biomarkers associated with responsiveness to immunotherapy . jco precis oncol 4 : 647 - 661 . 
90% of vulvar cancers and nearly 5% of all gynecologic cancers.1 , 2 radical excision imposes high morbidity , and one third of patients have been shown to experience recurrence after primary treatment.3 recent reports have shown durable responses with denitive or neoadjuvant chemoradiation for unresectable cancers.4 , 5 for patients with recurrence or distant metastasis , prognosis is poor , with an overall 2 - year survival rate of less than 15%.6 there is a critical need to improve our understanding of the molecular pathogenesis of vscc to provide insights that may guide more effective therapies . vscc develops through two distinct oncogenic pathways . 
this subgroup often associates with usual - type vulvar intraepithelial neoplasia ( vin ) , also known as high - grade squamous intraepithelial lesion.7 although other anogenital squamous cell neoplasms have  . 
 williams et al context key objective previous analyses have suggested genetic differences in vulvar squamous cell carcinoma based on human papillomavirus ( hpv ) status , but restricted sample volume and testing platforms have limited comprehensive identication of statistically signicant differences . 
in a large - scale comparative genomic study , what undiscovered genomic alterations distinguish high - risk hpv - driven versus dystrophic / inammatory - associated vulvar squamous cell carcinoma ? knowledge generated we identify signicantly different molecular proles based on hpv status . 
for genomic analyses , 60 ng of dna was extracted from 40 - m sections of 255 , 008 tumor samples , including 280 vscc specimens and 1 , 031 cervical squamous cell carcinoma ( cscc ) , each from a different patient , in formalin - xed parafnembedded ( ffpe ) tissue blocks . 
hpv genome sequences were detected by de novo assembly of nonhuman sequencing reads and nucleotide basic local alignment search tool ( blastn ) comparison against all viral nucleotide sequences in the national center for biotechnology information refseq database . 
hpv types identied in this study were stratied according to the hpv classication described by muoz et al , 8 with hpv 16 , 18 , 31 , 33 , and 58 labeled hrhpv + and hpv 6 labeled low risk . 
sequencing was performed on the primary tumor in 200 patients and on metastases in 80 ( 57 regional lymph nodes and 23 distant sites )  . hpv status and typing were determined on all 280 patient samples ; 102 / 280 vsccs ( 36% ) contained hrhpv sequences , predominantly hpv 16 ( 88% ; table 1 )  . 
for the 177 hpv vsccs , 137 were sequenced using the original primary tumors and 40 from metastatic site biopsies ( 10 distant , including seven lung , one pleural , one abdominal , and one to bone )  . comprehensive genomic proling figure 1 displays the distribution of gas by hpv status . 
the only specic point mutation with a signicant difference between hpv + and hpv was pik3ca e545k , an activating mutation that was signicantly enriched in hpv + vsccs ( table 2 )  . 
of vsccs cell - free circulating tumor dna ( ctdna ) was evaluated from blood specimens collected from 10 patients with vscc ( liquid biopsy ) using the hybrid capture - based illumina hi - seq ( illumina , san diego , ca ) technology . 
maximum somatic allele frequency was used to estimate the fraction of ctdna per methods previously described.30 , 31 mutational signatures mutational signatures were assessed for all tumor samples with at least 20 nondriver somatic missense alterations . signatures were given by analysis of the trinucleotide context and proled using the sanger cosmic signatures of mutational processes in human cancer.32 a positive signature required a sample to have at least a 40% t to a characterized mutational process , including apobec overexpression , exposure to ultraviolet light , hypofunction of the brca tumor suppressor , and defects in mismatch repair.32 immunohistochemistry programmed death - ligand 1 ( pd - l1 ) immunohistochemistry ( ihc ) was performed regularly in tandem with cgp to guide patient selection for immunotherapy . 
pd - l1 protein expression was assessed by ihc on 5 - micron ffpe tissue sections using the dako pd - l1 ihc22c3 pharmdx assay ( agilent ; santa clara , ca ; n = 52 vsccs ) or the ventana ( oro valley , az ) pd - l1 ( sp142 ) assay ( n = 21 vsccs ) , following each manufacturers instructions . 
dako pd - l1 expression was reported as a tumor proportion score , and ventana pd - l1 was reported as percent tumor area covered by positively staining tumor cells and immune cells . less than 1% staining was dened as negative , 1% - 49% was dened as low positive , and 50% was dened as high positive . clinicopathologic analysis of the vscc cohort a total of 280 vsccs were assayed with cgp ( foundation medicine ) , using material sent from treating institutions , from 2014 to 2019 . 
human investigations were performed after approval by a local human investigations committee and in accordance with an assurance led with and approved by the department of health and human services , where appropriate . 
amp , amplication ; mb , megabase ; msi , microsatellite instability ; msi - h , microsatellite instability - high ; mss , microsatellite stable ; mut , mutation ; pd - l1 , programmed death - ligand 1 ; tmb , tumor mutation burden . of each ga in the hpv and hpv + cohorts is included in appendix figures a2a and a2b , respectively . in the entire cohort : an hpv 16 ( + ) vscc with an mlh1 splice site mutation . frequencies of specic biomarkers associated with responsiveness to immunotherapy differed between the vscc subgroups ( fig 2 )  . 
all other gas , as well as age and pd - l1 ihc staining , showed no signicant differences between primary versus metastatic samples controlled for hpv status . comparison of hpv 16 with other hrhpv subtypes revealed no signicant differences in demographics , tmb , or sequenced site . 
thirty - three ( 12.6% ) were identied with an apobec ( apolipoprotein b mrna - editing enzyme , catalytic polypeptide - like ) signature ( 12 hpv + and 21 hpv ) , two with brca signature ( one hpv + , one hpv ) , seven with mismatch repair ( two hpv + , ve hpv ) , and a single tumor with ultraviolet signature ( hpv )  . 
three of four liquid biopsies showed at least one pathogenic ga present in the associated tissue biopsy ( appendix table a2 )  . separate from our 280 patients in the vscc cohort , ctdna was evaluated on six patients with known vscc but without tissue biopsy sequencing data . 
gas were detected in ve of six of these patients ( appendix table a2 )  . hpv + cscc ( n = 864 ) showed gas that were largely similar to what we found in hpv + vscc ( n = 103 ; appendix table a3 )  . 
although low in frequency , gas in kdm6a , ar , and cdk12 were signicantly higher in vscc versus cscc ( appendix table a3 )  . discussion in this study , hybrid capture - based dna sequencing was applied to a large series of patient tumors to better characterize the genomic landscape of vscc and to identify important genetic differences between hpv + and hpv disease . 
consistent with prior studies , a high rate of mutation was identied overall , with 98% of tumors in the analysis containing one or more known oncogenic mutations.17 , 18 mutational proles sharply differentiated hpv + and hpv disease . 
hpv + vscc showed mutations in the pi3k / mtor pathway , with 61% of tumors containing gas in the pathway , with the majority of gas showing signicant association with hpv + status ( table 2 )  . 
choschzick et al22 specically examined ccnd1 copy number changes in 183 vsccs and identied amplications in 22% , with a signicant association with hpv tumors.23 growdon pd - l1 ihc negative low positive high positive genomic alterations rearrangement short variant deletion not performed amplification fig 2 . 
of the 73 vulvar squamous cell carcinoma for which pd - l1 ihc was performed , 33% of hpv - negative and 9% of hpv - positive were pd - l1 tumor high - positive ; p = .04. 
histopathology of vulvar squamous cell carcinoma ranged from ( a ) well differentiated with abundant keratin to ( b ) poorly differentiated ( hematoxylin and eosin stains , 400 )  . 
 ( c ) programmed death - ligand 1 ( pd - l1 ) staining of human papillomavirus ( hpv ) negative vsccs showed signicantly higher frequency of high - positive tumors , whereas ( d ) hpvpositive disease was largely negative for pd - l1 stain ( pd - l1 immunohistochemistries , 400 )  . et al24 evaluated egfr amplication in 51 vsccs , and identied amplication in 12% of tumors , with signicant association with poor prognosis and hpv status . 
zie ba et al19 performed sequencing of 81 vsccs with a 50 - gene panel , and the results differed from other studies , most strikingly in the absence of clear genomic differences between hpv + and hpv disease . 
the authors reported tp53 and cdkn2a mutations in both hpv + and hpv vscc , whereas mutations in pik3ca , fbxw7 , hras , fgfr3 , stk11 , akt1 , smad4 , and pten were found at low frequencies in both types of vscc.19 zie ba et al19 noted , however , that the 2 hpv tests that they used gave highly inconsistent results and that those hpv tests had not been developed for analyzing tissue - derived dna.19 these difculties in identifying hpv + and hpv disease may account for the divergence of their results from several prior studies.16 - 18 , 20 in our study , hpv status clearly divided our large cohort into two signicantly different genomic - dened diseases . pi3k / mtor pathway mutations , including stk11 , a negative regulator of mtor signaling , have been described in a wide range of hpv - driven cancers.33 , 34 in our cohort , a signicantly higher rate of stk11 gas was observed in hpv + tumors sequenced from metastases , compared with hpv + tumors sequenced from the primary site . stk11 has been previously correlated with poor response to antiprogrammed death - 1 therapy in kras - mutant lung adenocarcinoma.35 it is conceivable that a similar role could exist in hpv + vscc as a putative tumor immuneescape mechanism , but additional studies are needed . a minority of vsccs showed distinctive mutational signatures . 
this signature reects apobec cytidine deaminase dna - editing activity36 , 37 and has been noted to be important in development of thoracic cancers , with possible implications for predicting response to immunotherapy.38 , 39 several of the gas observed to be signicantly enriched in the hpv cohort are in pathways functionally relevant to hpv pathogenesis . 
tp53 , tert , and cdkn2a are deregulated by hpv e6 and / or e7 , whereas egfr recycling is altered by hpv e5.40 - 42 beyond specic gas , key differences were identied in tmb and pd - l1 ihc staining patterns . 
hpv induces genomic instability , which may account for the increased tmb in the primary hpv + cohort.43 in addition , hpv infection reduces the cellular immune response by decreasing the interferon antiviral response.44 cgp may reveal opportunities for targeted therapies to be tested in clinical trials . 
kmt2d , an epigenetic modier , and transcription factor sox2 can activate and interact with the pi3k pathway.49 - 51 gas in both are enriched in hpv + vscc ( table 2 )  . 
tumors with gas in kmt2d may be sensitive to aurora kinase inhibition.52 in light of the many recent successes of immune checkpoint inhibitors , a careful approach to patient selection for clinical trials of these agents may be valuable . 
in our cohort , hpv vsccs showed a signicantly higher rate of pd - l1 ihc highpositive tumor staining , a higher rate of pdl1 amplication , and signicantly lower rates of stk11 alterations . 
vsccs in this category may benet from novel targeted therapeutics.53 other identied potential therapeutic targets include gas in receptor tyrosine kinases , cell cycle regulation , and the mapk pathway . 
early work in gas that affect epigenetic regulation indicates ezh2 inhibitors may be a viable therapeutic strategy.54 , 55 our study also provides a proof of concept that liquid biopsy detects ctdna in vscc , with three of four demonstrating at least one pathogenic ga detected in the tissue biopsy from the same patient . 
liquid biopsy may be a valuable method in vscc , and additional investigation is warranted . limitations in the study include the distinct patient population . tumor samples undergoing cgp are usually sent by clinicians seeking targeted therapy for patients with advanced disease . an additional limitation is the inadequate data on treatment history of the patients before tumor sequencing ; controls for tmb and resistance gas that may have arisen from local radiation or systemic treatment were not available . 
future work is needed to correlate genetic ndings with treatment exposure and follow - up data , which are not included in this study . in this study , we provided evidence that hpv + and hpv vscc are two distinct diseases , each with a characteristic molecular prole . 
 genomics of hpv + versus hpv vulvar squamous cell carcinoma rachel erlich employment : foundation medicine stock and other ownership interests : foundation medicine kevin jon williams stock and other ownership interests : hygieia stock and other ownership interests : gemphire therapeutics consulting or advisory role : gemphire therapeutics , inc . research funding : novo nordisk jeff m . 
venstrom employment : genentech , foundation medicine leadership : genentech stock and other ownership interests : genentech research funding : genentech , foundation medicine travel , accommodations , expenses : genentech brian m . 
alexander employment : foundation medicine leadership : foundation medicine stock and other ownership interests : roche research funding : eli lilly ( inst ) , puma ( inst ) , celgene ( inst ) open payments link : 854258 / summary nikunj shah employment : foundation medicine natalie danziger employment : foundation medicine eric a . 
severson employment : foundation medicine , partners healthcare stock and other ownership interests : foundation medicine jonathan keith killian employment : foundation medicine stock and other ownership interests : foundation medicine douglas i . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine consulting or advisory role : celsius therapeutics research funding : foundation medicine julie y . 
hemmerich employment : foundation medicine stock and other ownership interests : foundation medicine ( inst ) acknowledgment we thank our colleagues for their helpful comments during the preparation of this article . references judson pl , habermann eb , baxter nn , et al : trends in the incidence of invasive and in situ vulvar carcinoma . 
moore dh , ali s , koh wj , et al : a phase ii trial of radiation therapy and weekly cisplatin chemotherapy for the treatment of locally - advanced squamous cell carcinoma of the vulva : a gynecologic oncology group study . 
n engl j med 348 : 518 - 527 , 2003 alemany l , saunier m , alvarado - cabrero i , et al : human papillomavirus dna prevalence and type distribution in anal carcinomas worldwide . 
adv anat pathol 24 : 201 - 214 , 2017 van der avoort ia , shirango h , hoevenaars bm , et al : vulvar squamous cell carcinoma is a multifactorial disease following two separate and independent pathways . 
virgili a , borghi a , toni g , et al : prospective clinical and epidemiologic study of vulvar lichen sclerosus : analysis of prevalence and severity of clinical features , together with historical and demographic associations . 
weberpals ji , lo b , duciaume mm , et al : vulvar squamous cell carcinoma ( vscc ) as two diseases : hpv status identies distinct mutational proles including oncogenic broblast growth factor receptor 3 . 
trietsch md , nooij ls , gaarenstroom kn , et al : genetic and epigenetic changes in vulvar squamous cell carcinoma and its precursor lesions : a review of the current literature . 
swarts dra , voorham qjm , van splunter ap , et al : molecular heterogeneity in human papillomavirus - dependent and - independent vulvar carcinogenesis . cancer med 7 : 4542 - 4553 , 2018 24 . 
halec g , alemany l , lloveras b , et al : pathogenic role of the eight probably / possibly carcinogenic hpv types 26 , 53 , 66 , 67 , 68 , 70 , 73 and 82 in cervical 9 : 34 , 2017 cancer . 
sakamoto j , kamiura s , okayama k , et al : single type infection of human papillomavirus as a cause for high - grade cervical intraepithelial neoplasia and invasive cancer in japan . 
clark ta , chung jh , kennedy m , et al : analytical validation of a hybrid capturebased next - generation sequencing clinical assay for genomic proling of cell - free circulating tumor dna . 
gregg jp , li g , pavlick d , et al : comprehensive genomic proling of ctdna in patients with colon cancer and its delity to the genomics of the tumor biopsy . j clin oncol 36 : 569 , 2018 ( 4 ; suppl ) 32 . 
wang s , jia m , he z , et al : apobec3b and apobec mutational signature as potential predictive markers for immunotherapy response in non - small cell lung cancer . 
gameiro sf , kolendowski b , zhang a , et al : human papillomavirus dysregulates the cellular apparatus controlling the methylation status of h3k27 in different human cancers to consistently alter gene expression regardless of tissue of origoncotarget 8 : 72564 - 72576 , 2017 42 . 
zhang b , srirangam a , potter da , et al : hpv16 e5 protein disrupts the c - cbl - egfr interaction and egfr ubiquitination in human foreskin keratinocytes . oncogene 24 : 2585 - 2588 , 2005 43 . 
song d , li h , li h , et al : effect of human papillomavirus infection on the immune system and its role in the course of cervical cancer . 
tinker av , ellard s , welch s , et al : phase ii study of temsirolimus ( cci - 779 ) in women with recurrent , unresectable , locally advanced or metastatic carcinoma of the cervix . 
oncol lett 12 : 4107 - 4116 , jung k , kang h , mehra r : targeting phosphoinositide 3 - kinase ( pi3k ) in head and neck squamous cell carcinoma ( hnscc )  . 
pi3k pathway regulates er - dependent transcription in breast cancer through the epigenetic regulator kmt2d . oncogene 37 : 1354 - 1368 , 2018 science 355 : 1324 - 1330 , 2017 51 . 
kalu nn , mazumdar t , peng s , et al : comprehensive pharmacogenomic proling of human papillomavirus - positive and - negative squamous cell carcinoma identies sensitivity to aurora kinase inhibition in kmt2d mutants . 
strauss j , heery cr , schlom j , et al : phase i trial of m7824 ( msb0011359c ) , a bifunctional fusion protein targeting pd - l1 and tgfb , in advanced solid tumors . clin cancer res 24 : 1287 - 1295 , 2018 idris s , lindsay c , kostiuk m , et al : investigation of ezh2 pathways for novel epigenetic treatment strategies in oropharyngeal cancer . 
lindsay cd , kostiuk ma , harris j , et al : efcacy of ezh2 inhibitory drugs in human papillomavirus - positive and human papillomavirus - negative oropharyngeal squamous cell carcinomas . 
 hpv negative ( n = 177 ) hpv positive ( n = 103 ) rearrangement short variant deletion amplification multiple rearrangement short variant deletion amplification multiple williams et al fig a2 . 
30 years ago with the identication of the reciprocal translocation , t ( 11 ; 22 ) ( q24 ; q12 ) , otherwise known as ews - fl1.1 , 2 in the time since , multiple other fusion partners with ews have been identied that t a similar ewing sarcoma phenotype.3 , 4 when ews fusions are not identied , tumors with histologic features of ewing sarcoma have been labeled as primitive neuroectodermal tumors . 
in 2012 , pierron et al5 identied a subset of ewing - like tumors harboring paracentric inversion on the short arm of chromosome x , resulting in the fusion of the bcor and ccnb3 genes.5 since that discovery , several small case series have further elucidated the clinical , morphologic , and genomic differences that make this diagnosis distinct from other round cell sarcomas , most notably ewing sarcoma.6 - 8 though distinct from ewing sarcoma , most bcorccnb3fused sarcomas ( bcs ) are treated with upfront compressed chemotherapy with vincristine , doxorubicin , cyclophosphamide , ifosfamide , and etoposide plus local control with surgery and / or radiation . bcs shares similar event - free and overall survival rates with the standard ews - fli1fused ewing sarcoma using this treatment strategy.6 - 8 despite the growing knowledge base related to bcs , little is known about potential drug targets related to this disease entity , especially with regard to treatment of disease recurrence . 
we highlight the treatment of a young patient who had multiply - relapsed disease with the us food and drug administrationapproved cyclindependent kinase 4 / 6 ( cdk4 / 6 ) inhibitor palbociclib ; the tumor harbored a bcor - ccnb3 fusion and a germline variant in cdkn2b , and treatment resulted in a complete response and no evidence of disease 25 months into therapy . case history our male patient initially presented in 2010 at 1 year of age with a xed mass on his back . 
a core needle biopsy was performed , which revealed a malignant , small , round , blue cell tumor along with small amounts of benign brofatty tissue and skeletal muscle . 
immunohistochemical stains were positive for cd99 , fli1 , and vimentin and were negative for nse , synaptophysin , myf4 , gaf , cd45rb , and tdt consistent with a primitive neuroectodermal tumor . 
the patient started chemotherapy per childrens oncology group protocol aews0031 , regimen b2 , with ifosfamide , etoposide , vincristine , doxorubicin , and cyclophosphamide . gross total resection was not feasible at the time per neurosurgery , and the patient received 57.6 gy of proton beam radiation in october 2010 . 
2 years but then developed multiple local recurrences without metastases from 2013 to 2017 and underwent numerous surgeries , along with multiple different early - phase childrens oncology group therapeutic studies , as outlined in the timeline in figure 1a . 
after the most recent recurrence in october 2016 , the patient was referred to our pediatric cancer precision genomics prograbecause of the ndings outlined here in the results , we chose to start palbociclib in february 2017 . 
 diagnosis radiation debulking surgeries ( n = 4 ) case report molecular tumor analysis debulking surgery debulking surgery april 2010 2010 july 2013 2014 2015 2016 june 2016 2016 2016 2017 march 2019 initial therapy aews0031 arm b : vincristine , doxorubicin , cyclophosphamide , ifosfamide , etoposide cog phase i advl1212 : crizotinib , cyclophosphamide , topotecan phase ii advl1322 : pazopanib phase i advl1315 : axitinib metronomic therapy molecular - guided therapy palbociclib initial diagnosis before palbociclib 2 cycles of palbociclib 3 cycles of palbociclib 2 years of palbociclib fig 1 . 
there was concern for progression after 2 cycles of palbociclib , but there was a 2 - month lag between the before palbociclib scan and actually starting drug , so interval progression likely occurred in this timeframe . 
ned , no evidence of disease . results whole - genome sequencing , rna sequencing ( rna - seq ) analysis , germline exome sequencing , and protein evaluation were performed at the clinical laboratory improvement amendment ( clia ) approved laboratory , nantomics ( culver city , ca )  . 
the mutational burden of the tumor was relatively low at 75 , 046 somatic mutations , with only 88 somatic mutations mapping to protein coding regions ( circos plot in fig 2a )  . 
additionally , an undescribed somatic mutation in the smo gene ( smo n476s ) was identied in the tumor , and germline sequencing revealed a cdkn2b n41d missense variant , which was heterozygous in both the germline and tumor genomes of this patient . 
rna - seq was also performed by nantomics , and mrna transcripts were ranked by abundance , which could be associated with increased pathway activity and sensitivity to a targeted drug . 
with the exception of the destruction box in ccnb3 , all functional domains from each encoded protein remain intact in the bcor - ccnb3 fusion prote ( c ) the cdk4 / 6 pathway is a gene regulatory program controlled by multiple tiers of protein kinases and transcriptional regulators . increases in cyclin - d or cdk4 or 6 protein can lead to phosphorylation of the rb1 - e2f tumor suppressor complex . 
upon phosphorylation of rb1 , the e2f1 - 3 transcription factors are released from the complex and are able to bind to the promoters of target genes , driving activation of transcription . 
in the several case series describing bcs , the median age of diagnosis is in the teenage years , with the youngest patient recorded at age 2.5 - 8 , 11 again , because of the age of presentation , one could be concerned about an inherited cancer syndrome . 
this congenital tumor also harbored a smarcb1 / ini1 gene deletion common to malignant rhabdoid tumor , epithelioid sarcomas , and epithelioid malignant peripheral nerve sheath tumor that also , table 1 . 
overexpression of relevant tumor - promoting pathways gene status gene function ccnd1 ccnd2 cdk4 e2f1 e2f2 e2f3 cdc25a cdc25c cdc25b top2a bub1 bub1b overexpressed activating cyclin for cdk4 and cdk6 overexpressed activating cyclin for cdk4 and cdk6 overexpressed rb1 protein kinase overexpressed rb1 - regulated transcription factor overexpressed rb1 - regulated transcription factor overexpressed rb1 - regulated transcription factor overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene overexpressed e2f - regulated gene note . 
the expression status for a gene was classied as overexpressed if its tpm exceeded the genes upper 5th percentile.30 abbreviations : cdk , cyclin - dependent kinase ; e2f , e2 transcription factor ; rb1 , retinoblastoma gene ; tpms , transcripts per million . when found germline , is known to cause rhabdoid tumor predisposition syndrome.12 - 16 in the case reported by alfaro - cervello et al , 12 ini1 germline analysis was not performed . 
our patient also harbored a germline heterozygous missense variant , cdkn2b n41d . is unclear what role this germline cdkn2b n41d variant could play in sarcomagenesis , as cancer risks associated with cdkn2a / b gene variants include melanoma , pancreatic cancer , and astrocytomas.17 , 18 there is a recent short report from jouenne et al19 that found an increased risk of soft tissue sarcoma development with germline loss of cdkn2a , though no data exist conrming this risk with cdkn2b variants . 
sunita et al20 showed that the specic cdkn2b n41d variant , which encodes p15 ( ink4b ) , is unable to bind to the cdk6 protein , leading to loss of function of cdkn2b , which could lead to dysregulated control of s - phase entry . 
though this variants contribution to tumorigenesis is intriguing , ckdn2b was normally expressed in our patients tumor , and there are no data suggesting that this impaired binding to cdk6 leads to mrna overexpression along multiple levels of the cdk4 / 6 pathway . despite discovering alterations of several key regulators of the cdk4 / 6 pathway in this tumor , none have been proven to serve as clinical biomarker for sensitivity to cdk4 / 6 inhibitors.21 in a preclinical ewing sarcoma orthotopic xenograft model with cdkn2a deletion , palbociclib was able to greatly suppress growth despite doxorubicin resistance of this model.22 in other sarcoma subtypes , palbociclib reduced tumor burden in murine preclinical models.23 - 25 clinically , there is phase ii evidence of palbociclibs efcacy in adults with liposarcoma26 , 27 and leiomyosarcoma.28 despite growing evidence in these sarcomas , there are no published data testing cdk4 / 6 inhibitors in bcs . 
for our patient with bcs , the expression status for a gene was classied as overexpressed if its tpm exceeded the genes upper 5th percentile of per - gene rna - seq by expectation - maximization ( rsem ) transcript - per - million ( tpm ) values for a collection of rna sequencing ( rna - seq ) datasets from the cancer genome atlas normal samples . 
in the study by pierron et al , 5 10 bcs tumors were analyzed for certain mrna expression ; overexpression was determined as described in pierron manuscript methods . abbreviations : bcs , bcor - ccnb3fused sarcomas ; nd , not disclosed . pathway , and ( 3 ) the presence of a germline cdkn2b variant . 
ferguson , md , ms , 705 riley hospital dr , ri 4340 , indianapolis , in 46202 ; twitter : @rileychildrens ; e - mail : micjferg@iu.edu. support supported by grant no . 
cancer genet cytogenet 21 : 185 - 208 , 1986 turc - carel c , aurias a , mugneret f , et al : chromosomes in ewings sarcoma : i . 
an evaluation of 85 cases of remarkable consistency of t ( 11 ; 22 ) ( q24 ; q12 )  . cancer genet cytogenet 32 : 229 - 238 , 1988 ginsberg jp , de alava e , ladanyi m , et al : ews - fli1 and ews - erg gene fusions are associated with similar clinical phenotypes in ewings sarcoma . 
j clin oncol 17 : 1809 - 1814 , 1999 shing dc , mcmullan dj , roberts p , et al : fus / erg gene fusions in ewings tumors . 
cancer res 63 : 4568 - 4576 , 2003 pierron g , tirode f , lucchesi c , et al : a new subtype of bone sarcoma dened by bcor - ccnb3 gene fusion . 
nat genet 44 : 461 - 466 , 2012 peters tl , kumar v , polikepahad s , et al : bcor - ccnb3 fusions are frequent in undifferentiated sarcomas of male children . 
mod pathol 28 : 575 - 586 , 2015 puls f , niblett a , marland g , et al : bcor - ccnb3 ( ewing - like ) sarcoma : a clinicopathologic analysis of 10 cases , in comparison with conventional ewing sarcoma . 
am j surg pathol 38 : 1307 - 1318 , 2014 kao , yc , owosho aa , sung ys , et al : bcor - ccnb3 fusionpositive sarcomas : a clinicopathologic and molecular analysis of 36 cases with comparison to morphologic spectrum and clinical behavior of other round cell sarcomas . 
riggi n , suv `a ml , suv `a d , et al : ews - fli - 1 expression triggers a ewings sarcoma initiation program in primary human mesenchymal stem cells . 
matsuyama a , shiba e , umekita y , et al : clinicopathologic diversity of undifferentiated sarcoma with bcor - ccnb3 fusion : analysis of 11 cases with a reappraisal of the utility of immunohistochemistry for bcor and ccnb3 . 
chan ak , han sj , choy w , et al : familial melanoma - astrocytoma syndrome : synchronous diffuse astrocytoma and pleomorphic xanthoastrocytoma in a patient with germline cdkn2a / b deletion and a signicant family history . 
campa d , pastore m , gentiluomo m , et al : functional single nucleotide polymorphisms within the cyclin - dependent kinase inhibitor 2a / 2b region affect pancreatic cancer risk . 
oncotarget 7 : 57011 - 57020 , 2016 jouenne f , chauvot de beauchene i , bollaert e , et al : germline cdkn2a / p16ink4a mutations contribute to genetic determinism of sarcoma . 
agarwal sk , mateo cm , marx sj : rare germline mutations in cyclin - dependent kinase inhibitor genes in multiple endocrine neoplasia type 1 and related states . j clin endocrinol metab 94 : 1826 - 1834 , 2009 21 . 
murakami t , singh as , kiyuna t , et al : effective molecular targeting of cdk4 / 6 and igf - 1r in a rare fus - erg fusion cdkn2a - deletion doxorubicin - resistant ewings sarcoma patient - derived orthotopic xenograft ( pdox ) nude - mouse model . 
perez m , muoz - galv an s , jim enez - garca mp , et al : efcacy of cdk4 inhibition against sarcomas depends on their levels of cdk4 and p16ink4 mrna . oncotarget 6 : 40557 - 40574 , 2015 24 . 
vlenterie m , hillebrandt - roeffen mh , schaars ew , et al : targeting cyclin - dependent kinases in synovial sarcoma : palbociclib as a potential treatment for synovial sarcoma patients . 
b ohm mj , marienfeld r , j ager d , et al : analysis of the cdk4 / 6 cell cycle pathway in leiomyosarcomas as a potential target for inhibition by palbociclib . 
dickson ma , tap wd , keohan ml , et al : phase ii trial of the cdk4 inhibitor pd0332991 in patients with advanced cdk4 - amplied well - differentiated or dedifferentiated liposarcoma . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
elvin ja , gay lm , ort r , et al : clinical benet in response to palbociclib treatment in refractory uterine leiomyosarcomas with a common cdkn2a alteration . oncologist 22 : 416 - 421 , 2017 1072 - 1074 , 2015 29 . 
 development and validation of a clinical polygenic risk score to predict breast cancer risk elisha hughes , phd1 ; placede tshiaba , ms1 ; shannon gallagher , mph1 ; susanne wagner , phd1 ; thaddeus judkins , ms1 ; benjamin roa , phd1 ; eric rosenthal , phd , ms1 ; susan domchek , md2 ; judy garber , md , mph3 ; johnathan lancaster , md , phd1 ; jeffrey weitzel , md4 ; allison w . 
lanchbury , phd1 ; alexander gutin , phd1 ; and mark robson , md6 purpose women with a family history of breast cancer are frequently referred for hereditary cancer genetic testing , yet , 10% are found to have pathogenic variants in known breast cancer susceptibility genes . 
largescale genotyping studies have identied common variants ( primarily single - nucleotide polymorphisms [ snps ] ) with individually modest breast cancer risk that , in aggregate , account for considerable breast cancer susceptibility . 
candidate polygenic risk scores ( prss ) as predictors of personal breast cancer history were developed through multivariable logistic regression models adjusted for age , cancer history , and ancestry . 
an optimized prs was validated in 2 independent cohorts ( n = 13 , 174 ; n = 141 , 160 )  . results within the training cohort ( n = 24 , 259 ) , 4 , 291 women ( 18% ) had a personal history of breast cancer and 8 , 725 women ( 36% ) reported breast cancer in a rst - degree relative . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction although breast cancer ranks among the cancer types with the highest heritability , 1 characterization of the incomplete . 
pathounderlying genetic causes is still genic variants in high - penetrance genes ( eg , brca1 , brca2 , palb2 ) associated with substantial increases in risk are individually rare in the general population.2 - 4 all known highand moderate - penetrance breast cancer susceptibility genes are estimated to account for a combined 20% of familial relative risk.5 as a result , most women who are referred for hereditary cancer genetic testing are negative for a pathogenic variant and without a clear understanding of the magnitude of their risk.6 genome - wide association studies ( gwas ) have identied several hundred , common , single - nucleotide polymorphisms ( snps ) as breast cancer susceptibility variants.7 - 11 although their individual contribution to risk is minor , polygenic risk scores ( prss ) of such variants can dene variant combinations with potentially actionable clinical risk.9 , 11 together , pathogenic variants in highand moderate - risk genes and panels of snps are estimated to explain up to 40% of the familial risk for developing breast cancer.11 the rst well - characterized prs combined 77 snps ( prs77 ) and was evaluated in  . 
this prs was highly predictive of breast cancer in two independent validation cohorts . relevance prss that aggregate genotypes from common variants have emerged as a new approach to improve breast cancer risk assessment . 
we developed and validated an 86 - snp score that was adjusted for family breast cancer history and was highly predictive of breast cancer risk , making it appropriate for clinical use to identify women at increased risk of developing breast cancer . recently , a polygenic score of 313 snps was deduced from the same gwas and then validated in an independent population cohort.11 the same study also supported previous work indicating snp - based risk scores may have to be optimized depending on breast cancer estrogenreceptor ( er ) status . 
composition and individual contribution of variants of the ideal snp - based breast cancer risk score remain to be dened . family history ( fh ) of breast cancer , a combination of biologic , social , and environmental factors , includes a genetic component that is expected to overlap with snpbased risk.9 , 11 to avoid double counting of risk due to correlation between genetic components of fh and prs , joint modeling of both genetic factors is required . 
here , we describe the development and validation of a prs in which we co - estimate snp - based risk and familial risk to obtain effect sizes independent of fh . 
additional details are provided in the data supplement . snp genotyping amplicons for 94 snp markers published at the time of this study were incorporated into a next - generation sequencing panel.8 , 9 two markers failed design due to their location within repetitive elements , leaving 92 markers for evaluation . 
clinical information from provider - completed test request forms included ancestry , personal and family cancer history , cancer type ( s ) , and age ( s ) at diagnosis . 
 clinical polygenic risk score for breast cancer previous work supports a multiplicative model as the best method for capturing the combined snp effects.9 , 11 we centered the multiplicative model according to generalpopulation allele frequencies so the or for an individual patient represents the fold - change in risk relative to the general population . 
patient clinical characteristics validation study tested the association of the prs with invasive breast cancer after adjusting for age , personal and family cancer history , and ancestry . in exploratory analyses , we assessed the predictive ability of the optimized prs compared with a previously described prs77 by adding both to a multivariable model . 
the observed versus theoretical effect of the prs on breast cancer risk under the multiplicative polygenic model was assessed by comparing ors from the continuous prs with those obtained from analysis of patients binned in categories according to prs percentiles . 
heterogeneity of the prs effect size according to age , ancestry , and fh of breast cancer was evaluated by tting additional interaction terms and by repeating the primary analysis restricted to subcohorts stratied by age , ancestry , and fh severity . 
overall , 8 , 725 patients ( 36% ) reported a breast cancer diagnosis in 1 rst - degree relative and 13 , 230 ( 55% ) had no rst - degree relatives with breast or ovarian cancer . effect sizes and population frequencies were used to rank 92 susceptibility variants by their informativeness and to construct a polygenic score by successive addition of the most informative variant . 
distribution of relative risks , or fold changes , in breast cancer risks due to the 86 - snp score in unaffected women was similar between the rst and second validations ( data supplement figures s1 and s2 )  . 
ors for developing breast cancer by 86 - snp score percentile in each of the two validation cohorts are given in table 2 . consistently , women in the top 95th percentile of the 86snp score distribution had a more than 2 - fold higher risk of breast cancer development than women with an average 80 86 snps ranked by informativeness * fig 1 . 
effect sizes of the 86 - snp score were consistent across subcohorts stratied by age ( table 3 ; data supplement figure s4 ) , ancestry ( data supplement table s3 ) , and fh ( table 4 ; data supplement figure s5 ) in both validation cohorts . 
these results indicate the simple multiplicative model remains the best method for capturing the risk conferred by the combined effects of snps after accounting for family cancer history . discussion prss aggregating genotypes from common variants offer new ways to improve breast cancer risk assessment and can contribute to better understanding of breast cancer risk in all women . 
modication of risk estimates by prs - based stratication has been shown in a variety of clinical settings , including women who carry a pathogenic variant , high - risk women , and population cohorts.11 , 15 - 17 these novel tools , however , are of particular interest to women who present for genetic risk assessment with increased risk due to a fh of breast cancer . 
fh and susceptibility variants contribute independently to risk prediction , yet the approximately 13% reduction in the or for fh when adjusted for the prs77 ( or prs313 ) indicates an overlapping contribution to risk.9 , 11 , 18 adjustment for this correlation between snps and fh can be achieved by co - estimating ors from multivariable models . 
the reported interaction was only signicant in er - positive disease , a subanalysis not available in our data set.11 since the inception of this study , additional breast cancer risk variants have been described , and expanded breast cancer prss have been evaluated and validated in independent data sets.10 , 11 the enlarged prss are estimated to account for a larger fraction of familial risk and promise observed theoretical observed theoretical > 1 - 5 5 - 10 10 - 20 20 - 40 40 - 60 60 - 80 80 - 90 90 - 95 95 - 99 > 99 > 1 - 5 5 - 10 10 - 20 20 - 40 40 - 60 60 - 80 80 - 90 90 - 95 95 - 99 > 99 percentiles of the 86 - snp score percentiles of the 86 - snp score fig 2 . 
the approach described here of co - estimation in multivariate models could be applied to any emerging prs , irrespective of number of variants or ancestral origin . among the strengths of this study are the use of large , contemporary , and fully independent cohorts for development and 2 validation studies . 
thus , to our knowledge , the 86 - snp score is the rst prs with an snp component adjusted for fh and , as such , would be an appropriate addition to conventional clinical models . limitations of the study include the inability to apply the 86snp score to patients of non - european ancestry because changes in genetic structure and linkage disequilibrium may affect the predictive ability of individual risk variants when present in a different ancestral background . 
although association studies with equivalent explanatory power in other ancestries have yet to be described , they are the subject of ongoing research and the expansion of breast cancer prs to other ancestries is a high priority . 
however , previous studies have demonstrated that unbiased risk estimates can be obtained from analysis of a clinical testing population through multivariable adjustment for the factors related to ascertainment.14 , 19 although the 86 - snp score described here adjusted for fh , genetic factors are not the sole contributors to breast cancer risk , even in cohorts with exceptional fh . 
validated clinical risk models incorporate variables such as body mass index , age at menarche , parity , age at rst birth and hormone replacement therapy use , as well as details of fh.20 - 23 other important risk factors , such as mammographic density and diet , are not taken into account here.24 - 26 more studies will be needed to accommodate these additional variables and to determine their dependent contributions . 
lanchbury data analysis and interpretation : elisha hughes , placede tshiaba , shannon gallagher , susanne wagner , benjamin roa , eric rosenthal , susan domchek , judy garber , jeffrey weitzel , allison w . 
komen for the cure ( i ) , american association for cancer research , diane helis henry medical foundation , james p . wilmot foundation ( i ) , adrienne helis malvin medical research foundation ( i ) , breast cancer research foundation , facing our risk of cancer empowered johnathan lancaster employment : myriad genetics , regeneron stock and other ownership interests : myriad genetics , regeneron jeffrey weitzel speakers bureau : astrazeneca allison w . 
jama 315 : 68 - 76 , 2016 peto j , collins n , barfoot r , et al : prevalence of brca1 and brca2 gene mutations in patients with early - onset breast cancer . 
j natl cancer inst 91 : 943 - 949 , 1999 anglian breast cancer study group : prevalence and penetrance of brca1 and brca2 mutations in a population - based series of breast cancer cases . 
 hughes et al collaborative group on hormonal factors in breast cancer : familial breast cancer : collaborative reanalysis of individual data from 52 epidemiological studies including 58 , 209 women with breast cancer and 101 , 986 women without the disease . 
j mammary gland biol neoplasia 9 : 221 - 236 , 2004 desmond a , kurian aw , gabree m , et al : clinical actionability of multigene panel testing for hereditary breast and ovarian cancer risk assessment . 
michailidou k , beesley j , lindstrom s , et al : genome - wide association analysis of more than 120 , 000 individuals identies 15 new susceptibility loci for breast cancer . 
am j hum genet 104 : 21 - 34 , 2019 judkins t , leclair b , bowles k , et al : development and analytical validation of a 25 - gene next generation sequencing panel that includes the brca1 and brca2 genes to assess hereditary cancer risk . 
li h , feng b , miron a , et al : breast cancer risk prediction using a polygenic risk score in the familial setting : a prospective study from the breast cancer family 17 . 
n aslund - koch c , nordestgaard bg , bojesen se : common breast cancer risk alleles and risk assessment : a study on 35 441 individuals from the danish registry and kconfab . 
cuzick j , brentnall ar , segal c , et al : impact of a panel of 88 single nucleotide polymorphisms on the risk of breast cancer in high - risk women : results from two randomized tamoxifen prevention trials . 
lindstr om s , thompson dj , paterson ad , et al : genome - wide association study identies multiple loci associated with both mammographic density and breast cancer risk . 
van zogchel , md1 , 3 ; jalenka van wijk , msc1 , 2 ; ilse timmerman , phd1 , 3 ; ngoc - kim vo1 ; lily zappeij - kannegieter1 ; boris decarolis , md4 ; thorsten simon , md4 ; max m . 
studies have found that neuroblastoma tissue contains adrenergic ( adrn ) and mesenchymal ( mes ) cells ; the latter express low levels of commonly used markers for minimal residual disease ( mrd )  . 
after selecting a panel of markers , serial bone marrow , peripheral blood , and peripheral blood stem cell samples were obtained from patients with high - risk neuroblastoma and tested for marker expression ; survival analyses were also performed . results prrx1 , postn , and fmo3 mrnas were used as a panel for specically detecting mes mrna in patient samples . 
mes mrna was detected only rarely in peripheral blood ; moreover , the presence of mes mrna in peripheral blood stem cell samples was associated with low event - free survival and overall survival . 
 van wezel et al context key objective the aim of this study was to identify a panel of markers to detect mesenchymal ( mes ) neuroblastoma mrna and to study these markers dynamics in patients with high - risk neuroblastoma . knowledge generated we identied a panel of mrna markers ( prrx1 , postn , and fmo3 ) to specically detect mes mrna in peripheral blood , bone marrow ( bm ) , and peripheral blood stem cell samples . 
in contrast to the frequently used adrenergic ( adrn ) mrna markers in real - time quantitative polymerase chain reaction studies , mes mrna increased during therapy in bm , which supports the idea that mes neuroblastoma cells have a different response to therapy than adrn neuroblastoma cells . furthermore , mes mrna was more frequently detected in bm and peripheral blood stem cells of patients with adverse outcomes . relevance neuroblastoma cells that undergo epithelial to mes transition are believed to become more chemoresistant and give rise to relapse . 
clinical samples were collected in edta tubes , processed within 24 hours , transferred to paxgene blood rna tubes ( qiagen , venlo , the netherlands ) , and stored at 20 c . 
dna was isolated from mononuclear cells stored in 10% dimethylsulfoxide at 180 c , and hypermethylated rassf1a rt - qpcr was performed as described previously.34 control samples and isolation of nonpathologic cell subsets to assess expression patterns of candidate markers in control tissue , pediatric bm samples of patients with leuleast 3 months after kemia in molecular remission ( at therapy ; n = 48 ) , pb samples from healthy volunteers ( n = 104 ) , and pbsc samples from children treated for a disease other than neuroblastoma ( n = 29 ) were tested as described previously.28 different pb populations were isolated as described previously.10 cultured mscs35 were provided by carlijn voermans , phd , at the department of hematopoiesis , sanquin blood supply foundation ( amsterdam , the netherlands )  . 
all samples were obtained with informed consent . rna extraction and rt - qpcr rna was isolated from clinical and control samples using the paxgene blood rna kit ( qiagen )  . 
expression was normalized to gusb expression using the following equation : normalized threshold cycle ( dct ) = ( ctgusb ctmarker )  . data analysis for the newly identied mes markers , a threshold for positivity in control bm , pb , and pbsc samples was determined on the basis of their expression in each sample ( see results )  . in the pbsc cohort , survival was analyzed using the kaplanmeier method , and signicant differences between the estimated survival curves were analyzed using the log - rank test . fishers exact test was used to analyze the differences in mes marker positivity between the relapse and survivor groups . 
subsequently , we ltered for genes with a minimal expression level in pb data sets , which resulted in an initial list of 14 candidate genes ( fig 2a )  . 
although prrx1 was not included in this initial list because its expression in 700 - mes cells was less than 400 , we included this gene in our additional analyses because prrx1 was reported as an immunohistochemistry marker for mes neuroblastoma.24 validation of candidate markers using rt - qpcr with sybr green i dye ( applied biosystems , foster city , ca ) , we examined the expression of all 15 candidate markers in mes cells ( 691 - mes and shep2 ) , adrn cells ( 691 - adrn , sh - sy5y , and imr - 32 ) , and a control pb sample ( data supplement )  . 
our analysis revealed three genes with high expression in mes cells , a signicant difference in expression between the mes and adrn cell lines , and either low or no measurable expression in the control pb these three genes were postn , prrx1 , and sample ; col3a1 , which encode the proteins periostin , paired related homeobox 1 , and collagen type iii 1 , respectively . rt - qpcr using taqman probes validated expression of these markers , which demonstrated high postn , prrx1 , and col3a1 expression in 691 - mes and sh - ep2 and low expression in 691 - adrn , sh - sy5y , and imr - 32 ( fig 3a )  . col3a1 was then excluded because it did not adequately discriminate between adrn and mes cell lines and was detected in the control pb samples . next , to set thresholds for dening positivity , we measured the expression of postn and prrx1 in normal hematologic cells : control bm samples ( n = 48 ) , pb samples ( n = 104 ) , and pbscs ( n = 29 )  . 
however , because both postn and prrx1 were expressed at variable levels in the control bm and pb samples ( fig 3b ) , we examined their expression levels in several subsets of hematologic cells and in mscs ( fig 3c )  . 
blue circles , sh - ep2 ; blue squares , 691 - mes ; red squares , 691 - adrn ; red circles , sh - sy5y ; red diamonds , imr - 32 . robustly expressed in mscs and , to a lesser extent , in t cells ; in contrast , postn was expressed at extremely low levels in b cells . 
taken together , these results suggest that the presence of both postn and prrx1 in control bm and pb samples is likely the result of their expression in mscs . identication of an msc - discriminating marker next , we searched for a marker that can be used to discriminate between mscs and mes mrna . 
microarray analysis identied 14 candidate genes that were highly expressed in mscs but poorly expressed both in mes cell lines and in hematologic cells ( not containing mscs ; fig 4a ; data supplement )  . 
the specicity of these markers was then tested using mscs obtained from healthy individuals ( n = 2 ) , neuroblastoma cell lines ( n = 5 ) , and control pb samples ( n = 2 ) using sybr green i dye ( data supplement )  . our analysis revealed that the fmo3 gene ( encoding avincontaining monooxygenase 3 ) was the most promising marker for discriminating between mscs and mes cells . testing using an fmo3 - specic taqman subsequent probe conrmed high expression in mscs ( comparable to the expression levels of prrx1 and postn ) , low expression ( or no expression ) in all neuroblastoma cell lines ( fig 4b ) , and no expression in hematologic subsets that lacked mscs . threshold for positivity in bm , pb , and pbscs because mscs , and to a lesser extent , b cells and t cells , express low levels of postn and prrx1 , we established a threshold for positivity for mes mrna detection in control bm , pb , and pbsc samples . 
 ( b ) heat map that shows the expression proles of the indicated 35 genes with high expression ( red ) in mes cell lines ( right ) and low expression ( green ) in adrenergic ( adrn ) cell lines ( left ) ; shown underneath are genes that are commonly used for mrd testing in neuroblastoma . 
 ( a ) the indicated genes were measured in mes cell lines ( shown in blue ) and adrenergic ( adrn ) cell lines ( shown in red )  . 
 ( b ) normalized expression ( dct = ctgusb ctmarker ) of postn and prrx1 measured in control bone marrow ( bm ) , peripheral blood ( pb ) , and peripheral blood stem cell ( pbsc ) samples . 
on the basis of these results , the positivity threshold for postn and prrx1 was set to a dct value greater than 9 between postn / prrx1 and gusb and a dct value greater than 3 between postn / prrx1 and fmo3 ( fig 4c )  . 
the threshold for positivity for pb was determined using 104 control pb samples ( data supplement ) and was set to a dct value greater than 12 for prrx1 and a dct value greater than 10 for postn , with no measurable expression of fmo3 . 
because the background expression of both postn and prrx1 was extremely low in control pbsc samples , each pbsc sample was scored as r2 microarray mscs neuroblastoma mes cell lines 74 genes r2 and haematlas no or low expression in whole blood hematologic subgroups 14 genes candidate msc marker negative fmo3 postn prrx1 phox2b postn prrx1 ctgusb ctpostn > 9 and ctfmo3 ctpostn > 3 ctgusb ctpostn > 10 and fmo3 negative ctgusb ctprrx1 > 9 and ctfmo3 ctpostn > 3 ctgusb ctprrx1 > 12 and fmo3 negative pbsc quantifiable range and fmo3 negative quantifiable range and fmo3 negative fig 4 . 
 van wezel et al positive for mes mrna if the ct value was within the quantitative range , 38 with no measurable expression of fmo3 ( fig 4c )  . 
phox2b mrna was detected in all diagnostic samples ; this expression decreased to undetectable levels in most patients during induction chemotherapy ( ic ) and was detected again at relapse . 
in contrast , mes mrna was detected in only six samples ; ve of these samples were pbscs , and of note , these pbsc samples were negative for phox2b mrna . next , we examined pbsc samples obtained from 53 patients with high - risk neuroblastoma who were previously studied using adrn mrna39 ( data supplement )  . 
mes mrna and adrn mrna were detected in 15 ( 28% ) and six ( 11% ) of 53 samples , respectively , with little overlap ( both mes and adrn mrna were detected in only one sample )  . 
we previously reported that adrn mrna positivity is not correlated with outcome.39 however , here we found that the presence of postn and / or prrx1 mrna in pbsc samples was signicantly associated with low eventfree survival ( p = .045 ) and low overall survival ( p = .047 ; fig 5 ; data supplement )  . 
specically , we compared phox2b mrna with mes mrna measured in 95 serial bm samples collected at diagnosis , during therapy , during follow - up , and ( where applicable ) during relapse ( fig 6 ; data supplement )  . 
phox2b mrna was detected in all 27 diagnostic bm samples ; this expression decreased during ic treatment and was undetectable by the end of ic in most patients ( nine of 10 patients with complete remission and 10 of 15 patients who experienced relapse )  . 
in the patients with recurrent disease , phox2b mrna was detected again in 75% ( nine of 12 patients ) with systemic relapse ( three of the 15 patients with recurrent disease had a local relapse )  . 
 a negative mesenchymal minimal residual disease panel in neuroblastoma n716 asct relapse g04 survivor asct time since diagnosis ( days ) time since diagnosis ( days ) negative negative negative diagnosis mid - induction end - induction after asct relapse n = 13 n = 14 n = 10 n = 16 n = 10 n = 15 n = 12 both adrn negative s urviv ors r ela pse s urviv ors r ela pse s urviv ors r ela pse s urviv ors r ela pse r ela pse negative fig 6 . 
 ( c ) summary of the results obtained from all serial samples obtained from patients who ultimately experienced relapsed and patients who remained in complete remission ( survivors )  . 
 ( d ) a peripheral blood stem cell sample obtained from patient 774 and two bm samples obtained from patients 576 and 690 were measured for phox2b ( squares ) , postn ( lled circles ) , prrx1 ( triangles ) , and hypermethylated rassf1a ( open circles )  . 
we found that gd2s is expressed at high levels in both mes and adrn cell lines ; however , specicity is limited because of its relatively high expression in normal hematologic cells.10 to study the expression of mes - specic markers at the time of diagnosis as well as the dynamic expression pattern during follow - up , we identied a panel of markers that includes postn and prrx1 , which have been linked to emt in several cancer types.24 , 40 - 44 an mrd marker ideally should be expressed at extremely low levels in normal hematologic cells . 
however , a possible limitation of this approach is that dependent on the platform used , the actual gene expression levels can be underestimated , for example , as in the case of prrx1 expression in one cell line used in our study . 
of note , although we ascribed the expression of postn and prrx1 in control bm samples to mscs , we cannot rule out the possibility that other cell types , such as osteoblasts , may also contribute to this expression . 
nevertheless , because we established strict thresholds for dening positivity , we believe that we avoided detection of normal stromal cells as well as other cell types . because mes mrna was rarely detected in pb samples obtained from patients with high - risk neuroblastoma , its clinical relevance remains unclear , and these results need to be conrmed using a larger cohort . 
in contrast , mes mrna was detected in 28% of the pbsc samples obtained from 53 patients and was signicantly associated with low event - free survival and overall survival . 
of note , we previously reported a relatively low prevalence ( 9% ) of adrn mrna in pbscs obtained from this cohort , and the presence of adrn mrna was not associated with either low event - free survival or low overall survival.39 therefore , we speculate that the mes cells that reside in the bm circulate during stem - cell mobilization . by focusing on serial bm samples in high - risk patients , we found that mes mrna and adrn mrna have distinct temporal dynamics . 
specically , adrn mrna levels were high at diagnosis and during relapse but decreased during treatment , whereas mes mrna levels increased during treatment and were associated with patients who ultimately had a relapse . 
this nding suggests that mes cells may respond differently to therapy compared with adrn neuroblastoma cells and may play an important role in disease progression and / or recurrence ; this notion is consistent with reports that demonstrated the importance of emt in disease progression and treatment resistance.24 , 45 moreover , our nding that mes mrna was detected in only 14 of 27 patients at diagnosis ( and only rarely at relapse ) is consistent with the hypothesis that metastatic cells can undergo an mes - to - epithelial conversion and thus revert to an adrn phenotype.46 the relatively small size of our patient cohorts precluded extensive multivariable analyses of survival ; however , these exploratory ndings suggest that detection of mes markers in the bm and pbscs during treatment may have prognostic value . dna markers for mrd ( and recently , circulating cell - free dna markers ) have been shown to provide added value when combined with rna - based methods for monitoring mrd and for measuring tumor - derived genetic aberrations.34 , 47 - 49 on the other hand , we previously reported discrepancies between rna - based and dna - based markers using either methylated rassf1a or patientspecic dna markers.34 , 47 we hypothesize that these discrepancies reect mes neuroblastoma cells that express reduced levels of adrn markers but can still be detected using dna markers . in conclusion , we report that postn , prrx1 , and fmo3 mrna can be used to detect mes neuroblastoma cells in bm and pbscs in patients with high - risk neuroblastoma . 
moreover , although the mes markers are more prevalent in the bm of patients who will ultimately experience relapse , they are rarely present at the actual time of relapse . 
van zogchel , jalenka van wijk , ngoc - kim vo , lily zappeij - kannegieter , boris decarolis , thorsten simon , rogier versteeg , jan koster , johan van nes data analysis and interpretation : esther m . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . thorsten simon consulting or advisory role : eusa pharma ( inst ) consulting or advisory role : merck kgaa ( inst ) huib n . 
caron employment : roche stock and other ownership interests : roche travel , accommodations , expenses : roche no other potential conicts of interest were reported . references laprie a , michon j , hartmann o , et al : high - dose chemotherapy followed by locoregional irradiation improves the outcome of patients with international neuroblastoma staging system stage ii and iii neuroblastoma with mycn amplication . 
matthay kk , villablanca jg , seeger rc , et al : treatment of high - risk neuroblastoma with intensive chemotherapy , radiotherapy , autologous bone marrow transplantation , and 13 - cis - retinoic acid . 
n engl j med 341 : 1165 - 1173 , 1999 yu al , gilman al , ozkaynak mf , et al : anti - gd2 antibody with gm - csf , interleukin - 2 , and isotretinoin for neuroblastoma . 
n engl j med 363 : 1324 - 1334 , 2010 seeger rc , reynolds cp , gallego r , et al : quantitative tumor cell content of bone marrow and blood as a predictor of outcome in stage iv neuroblastoma : a childrens cancer group study . 
j clin oncol 18 : 4067 - 4076 , 2000 beiske k , burchill sa , cheung iy , et al : consensus criteria for sensitive detection of minimal neuroblastoma cells in bone marrow , blood and stem cell preparations by immunocytology and qrt - pcr : recommendations by the international neuroblastoma risk group task force . 
stutterheim j , gerritsen a , zappeij - kannegieter l , et al : detecting minimal residual disease in neuroblastoma : the superiority of a panel of real - time quantitative 11 . 
stutterheim j , zappeij - kannegieter l , versteeg r , et al : the prognostic value of fast molecular response of marrow disease in patients aged over 1 year with pcr markers . 
burchill sa , lewis ij , abrams kr , et al : circulating neuroblastoma cells detected by reverse transcriptase polymerase chain reaction for tyrosine hydroxylase mrna are an independent poor prognostic indicator in stage 4 neuroblastoma in children over 1 year . 
marachelian a , villablanca jg , liu cw , et al : expression of ve neuroblastoma genes in bone marrow or blood of patients with relapsed / refractory neuroblastoma provides a new biomarker for disease and prognosis . 
hartomo tb , kozaki a , hasegawa d , et al : minimal residual disease monitoring in neuroblastoma patients based on the expression of a set of real - time rt - pcr markers in tumor - initiating cells . 
hirase s , saitoh a , hartomo tb , et al : early detection of tumor relapse / regrowth by consecutive minimal residual disease monitoring in high - risk neuroblastoma patients . 
viprey vf , gregory wm , corrias mv , et al : neuroblastoma mrnas predict outcome in children with stage 4 neuroblastoma : a european hr - nbl1 / siopen 19 . 
burchill sa , beiske k , shimada h , et al : recommendations for the standardization of bone marrow disease assessment and reporting in children with neuroblastoma on behalf of the international neuroblastoma response criteria bone marrow working group . 
debruyne dn , bhatnagar n , sharma b , et al : alk inhibitor resistance in alk ( f1174l ) - driven neuroblastoma is associated with axl activation and induction of emt . 
piskareva o , harvey h , nolan j , et al : the development of cisplatin resistance in neuroblastoma is accompanied by epithelial to mesenchymal transition in vitro . cancer lett 364 : 142 - 155 , 2015 [ erratum : cancer lett 369 : 428 , 2015 ] 28 . 
burchill sa , bradbury fm , smith b , et al : neuroblastoma cell detection by reverse transcriptase - polymerase chain reaction ( rt - pcr ) for tyrosine hydroxylase oncol 26 : 5443 - 5449 , 2008 mrna . 
bate - eya lt , ebus me , koster j , et al : newly - derived neuroblastoma cell lines propagated in serum - free media recapitulate the genotype and phenotype of primary neuroblastoma tumours . 
eur j cancer 50 : 628 - 637 , 2014 van nes j , chan a , van groningen t , et al : a notch3 transcriptional module induces cell motility in neuroblastoma . 
kraal kc , bleeker gm , van eck - smit bl , et al : feasibility , toxicity and response of upfront metaiodobenzylguanidine therapy therapy followed by german pediatric oncology group neuroblastoma 2004 protocol in newly diagnosed stage 4 neuroblastoma patients . 
maijenburg mw , noort wa , kleijer m , et al : cell cycle and tissue of origin contribute to the migratory behaviour of human fetal and adult mesenchymal stromal cancer res 18 : 808 - 814 , 2012 cells . 
cheung iy , lo piccolo ms , kushner bh , et al : quantitation of gd2 synthase mrna by real - time reverse transcriptase polymerase chain reaction : clinical utility in evaluating adjuvant therapy in neuroblastoma . 
viprey vf , lastowska ma , corrias mv , et al : minimal disease monitoring by qrt - pcr : guidelines for identication and systematic validation of molecular markers prior to evaluation in prospective clinical trials . 
gabert j , beillard e , van der velden vh , et al : standardization and quality control studies of real - time quantitative reverse transcriptase polymerase chain reaction of fusion gene transcripts for residual disease detection in leukemiaa europe against cancer prograleukemia 17 : 2318 - 2357 , 2003 van wezel em , stutterheim j , vree f , et al : minimal residual disease detection in autologous stem cell grafts from patients with high risk neuroblastoma . 
wu sq , lv ye , lin bh , et al : silencing of periostin inhibits nicotine - mediated tumor cell growth and epithelial - mesenchymal transition in lung cancer cells . 
j clin invest 119 : 1420 - 1428 , 2009 van wezel em , zwijnenburg d , zappeij - kannegieter l , et al : whole - genome sequencing identies patient - specic dna minimal residual disease markers in neuroblastoma . 
chicard m , colmet - daage l , clement n , et al : whole - exome sequencing of cell - free dna reveals temporo - spatial heterogeneity and identies treatmentresistant clones in neuroblastoma . 
 mesenchymal minimal residual disease panel in neuroblastoma appendix microarray analysis mesenchymal ( mes ) - specic candidate markers were identied by comparing gene expression proles ( human genome u133 plus 2.0 array ; affymetrix , santa clara , ca ) among the following isogenic pairs of adrenergic ( adrn ) and mes cell lines : 691 - mes / 691b - adrn , sh - ep2 ( mes ) / sh - sy5y ( adrn ) , 700 - mes / 700 - adrn.24 specically , we screened for genes with a 1 log - fold or more difference in expression ( within each isogenic pair ) and an expression level greater than 400 units , thereby selecting only highly expressed marker genes . 
to identify discriminating markers for normal mesenchymal stromal cells ( mscs ) , the top 300 genes with the highest expression were used ( gene expression omnibus : gse68374 ) ; the genes with the highest fold difference between mscs and mes neuroblastoma cell lines were then selected . 
for each analysis , each genes expression was compared with its corresponding expression level in reference blood samples obtained from ve different data sets ( gse13159 , gse17186 , gse10715 , gse8121 , and gse6575 ) ; only genes that are not expressed in hematologic cell types ( using haematlas ; watkins et al : blood 113 : e1 - e9 , 2009 ) were selected . 
the reverse transcription was then heat inactivated , and the reaction volume was increased to 100 to 150 l . primers and probes were designed using primer express version 1.5 software ( applied biosystems , foster city , ca ) or oligo 6 ( molecular biology insights , colorado springs , co ) and synthesized by eurogentec ( li `ege , belgium ; data supplement )  . 
the primer / probe combinations for glucuronidase ( gusb ) , - 1 , 4 - n - acetylgalactosaminyltransferase 1 ( b4galnt1 , also known as gd2s ) , paired - like homeobox 2b ( phox2b ) , tyrosine hydroxylase ( th ) , dopa decarboxylase ( ddc ) , growth - associated protein 43 ( gap43 ) , cholinergic receptor nicotinic 3 ( chrna3 ) , and dopamine - hydroxylase ( dbh ) have been published previously10 , 36 , 37 ( beillard et al : leukemia 17 : 2474 - 2486 , 2003 )  . 
the initial screening for candidate molecular markers was performed using sybr green i dye ( applied biosystems ) combined with a melting curve analysis followed by specic taqman probes ( eurogentec )  . 
 effects of molecular heterogeneity on survival of patients with brafv600 - mutated melanoma treated with vemurafenib with or without cobimetinib in the cobrim study purpose the treatment of advanced brafv600 - mutated melanomas with braf inhibitors ( brafi ) has improved survival , but the efficacy of brafi varies among individuals and the development of acquired resistance to brafi through reactivation of mitogen activated protein kinase ( mapk ) signaling is common . 
we performed an exploratory , retrospective analysis to investigate the effects of brafv600 allelic balance , coexisting oncogene mutations , cell proliferation signaling levels , and loss of pten expression on progression - free survival ( pfs ) in patients in the phase iii cobrim study , which compared the combination of the mek inhibitor cobimetinib with the brafi vemurafenib versus vemurafenib as monotherapy . methods baseline tumor samples from the intention - to - treat population were analyzed by targeted deep sequencing at a median coverage of 3 , 600 and by immunohistochemistry for cell proliferation markers , brafv600e , and pten . 
gene expression in relation to loss of pten was profiled by rna sequencing in 205 patient samples and 42 brafv600 - mutated melanoma cell lines . results neither brafv600 allelic balance nor coexisting mutations in the ras / raf / rtk pathway affected pfs in either treatment group . 
loss of function of the tumor suppressor pten ( via both genetic alterations and other mechanisms such as epigenetic silencing ) occurs in > 20% of patients with brafv600 - mutated melanoma.15 - 17 loss of functional pten has been associated with a shorter pfs response to braf inhibition , 17 , 18 reduced overall survival , and a shorter time to the development of brain metastases.15 , 19 pten / akt signaling is known to interact with mapk signaling . 
for example , meki have been shown to enhance epidermal growth factorinduced akt activation , and mutations that activate pi3k / akt signaling reduce mapk signaling.20 to understand the impact of baseline tumor heterogeneity on the efficacy of treating advanced melanoma with meki and brafi , we systematically examined the effect of braf allelic balance , coexisting oncogene mutations , and cell proliferation signaling levels on pfs in all evaluable cobrim study participants . 
here , we report the results of this retrospective , exploratory analysis . methods analysis population samples for biomarker analysis were collected from patients with unresectable locally advanced or metastatic brafv600 - mutated melanoma in the cobrim study of cobimetinib combined with vemurafenib versus vemurafenib monotherapy , 6 with the aim of exploring intrinsic mechanisms of resistance to mek and braf inhibition . 
brafv600 allelic balance , coexisting oncogene mutations , cell proliferation biomarkers , and loss of pten expression were analyzed in samples from the cobrim intention - to - treat ( itt ) population . 
most analyses could not be performed on the complete itt population ( n = 495 ) because of insufficient tissue availability or assay failure . genetic marker analysis archival formalin - fixed paraffin - embedded ( ffpe ) melanoma tumor samples , biopsy specimens of accessible tumor lesions , and blood samples were obtained from consenting patients at study entry ( baseline )  . 
rna was extracted using the high pure rna paraffin isolation kit ( roche diagnostics , indianapolis , in )  . from the 495 patients in the cobrim itt population , 400 pretreatment tumor samples were evaluable by targeted next - generation sequencing . 
 ( a ) distribution of variant allele frequency ( vaf ; ratio of mutant to wild type [ wt ] ) in brafv600 in 400 baseline tumor samples from cobrim study patients . 
 ( b ) impact on progression - free survival ( pfs ) indicated by kaplan - meier plots of pfs in patients grouped by vaf above or below the median for each treatment ar ( c ) immunohistochemistry of brafv600e protein levels in tumor samples with a range of vafs ; increased vaf was associated with greater staining intensity . 
cobi , cobimetinib ; pbo , placebo ; vem , vemurafenib . mutations ( appendix table a1 ) was performed for a focused panel of 17 oncogenes ( suraseq targeted next - generation sequencing assay ; asuragen , austin , tx ) 21 at a median coverage of 3 , 600 . 
different cutoff points were explored earlier in the analysis and gave results similar to those shown here using the median vaf as the high and low cutoff ( appendix fig a1 )  . 
the median was chosen to be representative of the overall range of cutoff points . analysis of pten copy number and methylation status in 42 brafv600 - mutant melanoma cell lines was performed as described by haverty et al.22 analysis of methylation status was performed in bisulfite - treated genomic dna using the illumina 450k array ( infinium humanmethylation450 beadchip kit ; illumina , san diego , ca )  . 
methylation data were analyzed using the methyanalysis package for r.23 gene expression in relation to loss of pten was profiled by rna sequencing in 205 patient samples and in 42 braf v600 - mutant melanoma cell lines . 
rna was prepared for high throug hput sequencing with the truseq rna access library prep kit ( illumina ) , and 40 million 2 100 - bp reads were sequenced per sample using illumina hiseq . 
coexisting oncogene mutations and impact on progression - free survival ( pfs ) in patients treated with cobimetinib ( cobi ) combined with vemurafenib ( vem ) or vem monotherapy . 
 ( b ) pfs in patients with or without ras / raf / rtk mutations ( both treatment arms were combined to give sufficient numbers of patients with ras / raf / rtk mutations for statistical analysis )  . 
 ( c ) patients with coexisting ras / raf / rtk mutations had elevated levels of phosphorylated extracellular regulated kinase ( perk ) , measured by immunohistochemistry , compared with patients with wild - type ( wt ) ras / raf / rtk , indicating greater mitogen - activated protein kinase signaling pathway activity . 
 defined by the molecular signatures database emt hallmark collection , 24 was compared by z - score ( sum of log2 reads per kilobase of transcript per million mapped reads for all genes on the emt hallmark collection ) between samples with functional and nonfunctional pten . and immunohistochemical markers and a pfs data cutoff date of january 16 , 2015 . 
 expression levels were quantified by histo - score ( h - score ) , and samples were grouped as high or low , depending on whether the h - score was above or below the median , respectively . 
in a subset of samples , brafv600e expression was also evaluated by ihc ( antibrafv600e [ ve1 ] mouse monoclonal primary antibody ; ventana [ n = 39 ] )  . in vitro studies the effect of pten loss on drug sensitivity was evaluated in 42 brafv600 - mutant melanoma cell lines by analyzing cell viability after vemurafenib treatment . 
 in all samples , > 95% of tumor cells stained positive for brafv600e mutation , suggesting that differences in vaf reflect cells across the tumor rather than indicate a subclonal mutation , and that increased vaf was associated with greater staining intensity ( fig 1c )  . 
similar results were seen in a set of four melanoma cell lines ( appendix fig a2 )  . association between oncogene mutations and pfs to explore potential drivers of brafi resistance affecting survival , in addition to previously identified mechanisms such as mek mutation , 27 coexisting mutations in a panel of 17 oncogenes21 ( appendix table a1 ) were assayed in baseline braf - mutated tumor tissue from 400 of 495 patients in the cobrim itt population and were identified in 43 patients ( 11% ; fig 2a )  . 
h - score , histo - score ; mut , mutation ; pbo , placebo ; pd , progressive disease ; pr , partial response ; sd , stable disease . 
cell proliferation biomarkers and impact on progression - free survival ( pfs ) in patients treated with cobimetinib ( cobi ) combined with vemurafenib ( vem ) or vem monotherapy . 
 ( a ) kaplan - meier plots of pfs in patients grouped by high ( above the population median histo - score [ h - score ] of 40 ) or low ( below the population median ) phosphorylated extracellular regulated kinase ( perk ) levels . 
 ( b ) kaplan - meier plots of pfs in patients grouped by high or low baseline proliferation index , measured by the protein encoded by themki67gene ( ki - 67 ) immunohistochemistry ( population median ki - 67 level is 20% ) or ( c ) phosphorylated s6 immunohistochemistry ( ps6 ; population median h - score is 71 )  . 
 ( c ) rna sequencing profiling of melanoma samples from cobrim comparing the epithelial - mesenchymal transition ( emt ) gene expression signatures in tumors with pten loss versus tumors with normal pten levels . 
patient characteristics were similar between patients with and without loss of pten expression in the cobimetinib combined with vemurafenib and the vemurafenib monotherapy cohorts , with the exception that more patients with loss of pten expression had elevated lactate dehydrogenase in the cobimetinib combined with vemurafenib arm ( appendix table a3 )  . 
 ( b ) rna sequencing profiling of braf - mutant melanoma cell lines with or without pten loss comparing the epithelial - mesenchymal transition ( emt ) gene expression signatures . 
 loss of pten expression was associated with upregulation of the emt gene expression signature in these melanoma cell lines ( fig 5b ) , similar to that seen in the baseline tumor samples . 
when tested in an in vitro wound healing assay , in the absence of vemurafenib or cobimetinib , cell lines with loss of pten showed a higher capacity for migration ( fig 5c ) , consistent with observed clinical manifestations and previous preclinical findings.28 , 29 attempts to analyze whether vemurafenib or cobimetinib combined with vemurafenib affected the increased cell migration behavior associated with loss of pten were confounded by their effect on cell viability . discussion to our knowledge , this retrospective biomarker analysis of brafv600 - mutated melanoma samples from the cobrim study is the largest such study to date . 
although there was an association between signaling pathway activity and pfs in patients treated with vemurafenib monotherapy , increased mapk signaling and cell proliferation did not affect pfs in patients treated with a combination of cobimetinib and vemurafenib . 
 the combination of mek and braf inhibition thus seems to override the poor prognostic effect of increased mapk pathway activation . loss of pten expression is linked to reduced survival in advanced melanoma , most likely as a result of suppression of apoptosis and enhanced cell survival mediated by hyperactivation of pi3k / akt signaling.17 , 18 our analysis suggests that combined mek and braf inhibition can overcome the effect of loss of pten on pfs . 
 loss of pten function in addition to brafv600 mutation has been linked to the rapid development of brain metastases in advanced melanoma , which may also contribute to reduced pfs.15 , 26 our analysis confirms that brafv600 - mutated melanoma cells with loss of pten function have a higher expression of genes associated with emt , as well as enhanced migration . 
functional pten inhibits cell migration through dephosphorylation of focal adhesion kinase ( fak ) ; loss of pten relieves this inhibition.29 in prostate cancer models , ras / mapk activation cooperated with pten loss to promote emt and metastasis , and mek inhibition was able to reduce metastatic progression in these models.30 mek can also activate fak to promote cell migration , and mek inhibition could therefore downregulate fak - mediated migration , 31 addition to reducing the cell survival resulting from ras / mapk activation in brafv600 - mutated melanoma . 
this suggests a potential mechanism by which cobimetinib combined with vemurafenib could contribute to a survival benefit in patients with braf v600 - mutated melanoma and loss of pten . the large patient cohort available for analysis was a significant strength of this study ; however , the analysis was limited by the inability to evaluate baseline tumor samples for approximately 20% of patients included in the cobrim study . additional investigation of the mechanisms underlying intrinsic and acquired resistance is warranted . 
 the molecular mechanisms at work in patients with prolonged responses to combination therapy with cobimetinib and vemurafenib are still under investigation but may involve regulation of the host antitumour immune response.33 the overall findings of this study suggest that deeper inhibition of the mapk pathway through combined inhibition of both mek and braf overrides the effects of molecular heterogeneity to provide a survival benefit to all patients . 
 this both supports and provides a rationale for the greater efficacy of combination therapy with braf and meki , which has become the standard of care , compared with braf inhibition alone . 
ascierto , brigitte drno , anna maria di giacomo , claus garbe , ilsung chang , jessie hsu , hartmut koeppen , james larkin , yibing yan , grant a . 
wongchenko employment : genentech / roche stock and other ownership interests : genentech / roche , ariad pharmaceuticals antoni ribas stock and other ownership interests : compugen , flx bio , cytomx therapeutics , five prime therapeutics , advaxis , arcus biosciences , tango therapeutics , pact pharma consulting or advisory role : merck , amgen , genentech / roche , novartis paolo a . 
 james larkin honoraria : eisai , bristol - myers squibb , msd , glaxosmithkline , pfizer , novartis , genentech / roche , sectra , pierre fabre , eusa pharma , consulting or advisory role : eisai , bristol - myers squibb , msd , glaxosmithkline , pfizer , novartis , genentech / roche , sectra , pierre fabre , eusa pharma research funding : pfizer ( inst ) , novartis ( inst ) , msd ( inst ) , bristol - myers squibb ( inst ) travel , accommodations , expenses : bristol - myers squibb , pfizer , novartis , genentech / roche yibing yan employment : genentech / roche stock and other ownership interests : genentech / roche patents , royalties , other intellectual property : genentech / roche grant a . 
wongchenko , ilsung chang , jessie hsu , isabelle rooney , william lu , hartmut koeppen , and yibing yan , genentech , south san francisco ; antoni ribas , jonsson comprehensive cancer center at the university of california , los angeles , los angeles , ca ; paolo a . 
pascale , naples ; anna maria di giacomo , azienda ospedaliera universitaria senese , siena , italy ; brigitte drno , nantes university , nantes , france ; claus garbe , university of tbingen , tbingen , germany ; james larkin , the royal marsden hospital , london , united kingdom ; grant a . 
ascierto pa , mcarthur ga , drno b , et al : cobimetinib combined with vemurafenib in advanced braf ( v600 ) - mutant melanoma ( cobrim ) : updated efficacy results from a randomised , doubleblind , phase 3 trial . 
hauschild a , grob j - j , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
wilmott js , menzies am , haydu le , et al : braf ( v600e ) protein expression and outcome from braf inhibitor treatment in braf ( v600e ) metastatic melanoma . 
wagle n , van allen em , treacy dj , et al : map kinase pathway alterations in braf - mutant melanoma patients with acquired resistance to combined raf / mek inhibition . 
bucheit ad , chen g , siroy a , et al : complete loss of pten protein expression correlates with shorter time to brain metastasis and survival in stage iiib / c melanoma patients with brafv600 mutations . 
xing f , persaud y , pratilas ca , et al : concurrent loss of the pten and rb1 tumor suppressors attenuates raf dependence in melanomas harboring ( v600e ) braf . 
nathanson kl , martin a - m , wubbenhorst b , et al : tumor genetic analyses of patients with metastatic melanoma treated with the braf inhibitor dabrafenib ( gsk2118436 )  . 
latham g , hough j , sah s , et al : suraseq targeted ngs assays : integrated , cross - platform reagents that enable accurate detection of cancer gene mutations in residual clinical ffpe , fna , and biofluid biopsies . 
mcarthur ga , larkin j , ascierto pa , et al : impact of baseline allelic frequencies of brafv600 mutation and coexisting oncogenic mutations on progression - free survival from the cobrim phase 3 study evaluating cobimetinib + vemurafenib in advanced brafv600 - mutated melanoma . 
larkin jmg , yan y , mcarthur ga , et al : update of progression - free survival ( pfs ) and correlative biomarker analysis from cobrim : phase iii study of cobimetinib ( cobi ) plus vemurafenib ( vem ) in advanced braf - mutated melanoma . 
tamura m , gu j , takino t , et al : tumor suppressor pten inhibition of cell invasion , migration , and growth : differential involvement of focal adhesion kinase and p130cas . 
mulholland dj , kobayashi n , ruscetti m , et al : pten loss and ras / mapk activation cooperate to promote emt and metastasis initiated from prostate cancer stem / progenitor cells . 
wongchenko mj , mcarthur ga , drno b , et al : gene expression profiling in braf - mutated melanoma reveals patient subgroups with poor outcomes to vemurafenib that may be overcome by cobimetinib plus vemurafenib . 
exploration of the impact of variant allele frequency ( vaf ) on progression - free survival ( pfs ) indicated by kaplan - meier plots of pfs in patients grouped by vaf above or below cutoff points of ( a ) 25% and ( b ) 50% for each treatment arfor the analysis , the median was chosen to be representative of the overall range of cutoff points . 
cell viability of 42 brafv600 - mutant melanoma cell lines treated with vemurafenib , stratified by expression versus loss of expression of pten . pten + ( n = 20 ) pten loss ( n = 22 ) table a1 . 
konat e , phd1 ; biswajit das , phd3 ; chris karlovich , phd3 ; chih - jian lih , phd3 ; eric polley , phd9 ; richard simon , dsc1 ; ming - chung li , phd1 ; richard piekarz , md , phd1 ; and james h . 
although patients and physicians were blinded to the sequencing and random assignment results , a higher pretreatment dropout rate was observed in the control arm ( 22% ) compared with the experimental arm ( 6% ; p = .038 ) , suggesting that some patients may have had prior tumor mutation proling performed that led to a lack of participation in the control arm . conclusion further investigation , better annotation of predictive biomarkers , and the development of more effective agents are necessary to inform treatment decisions in an era of precision cancer medicine . 
increasing prevalence of tumor mutation proling and preference for targeted therapy make it difcult to use a randomized phase ii design to evaluate targeted therapy efcacy in an advanced disease setting . jco precis oncol 5 : 133 - 144 . 
to explore this , we conducted a randomized , histology - agnostic clinical to examine whether patients with advanced , refractory cancer who had a tumor mutation in a gene in one of three signaling pathways ( dna repair , pi3k , or ras / raf / mek ) were more likely to derive clinical benet if treated with regimens targeting that pathway ( the experimental arm ) than if they were treated with regimens that did not ( the control arm )  . 
 chen et al context key objective a molecular aberration in a patients tumor is expected to render the tumor susceptible to a drug targeting that aberration , but randomized , controlled , blinded phase ii trials conrming the efcacy of this precision medicine approach are both sparse and challenging to design . knowledge generated efcacy in patients with study - dened actionable mutations in the dna repair , ras / raf / mek , or akt / pi3k / mtor pathways either did not achieve the target objective response rate ( trametinib or adavosertib with carboplatin ) or indicated futility despite accrual challenges ( everolimus or veliparib with temozolomide )  . 
patients randomly assigned to the nontargeted control arm had a higher pretreatment dropout rate than the experimental arm , suggesting a preference for targeted therapy based on prestudy genetic proling . relevance the prevalence of genetic data makes it challenging to randomly assign patients to a nontargeted control arbetter geneand variant - specic biomarkers that predict response to drugs are needed for patients with cancer . patients were required to have measurable disease , be willing to undergo tumor biopsy to establish presence of a study - dened actionable mutation of interest ( amoi ) , and have tumor amenable to interventional radiologyguided percutaneous biopsy with a 16to 18 - gauge neeindicated and dle ; excisional biopsy was allowed if evaluable . 
patients who had prior treatment with any of the investigational agents were eligible to participate but were not assigned that same agent . agent - specic eligibility criteria are included in the data supplement . this trial was conducted under a national cancer institute ( nci ) - sponsored investigational new drug application with institutional review board approval . 
protocol design and conduct followed all applicable regulations , guidances , and local policies ( clinicaltrials.gov identier : nct01827384 )  . the investigators obtained informed consent from each participant . trial design this was a multihistology , multicenter , randomized phase ii study of four investigational drug regimens demonstrated to inhibit the dna repair pathway , ras / raf / mek pathway , or akt / pi3k / mtor pathway . 
eligible patients with an amoi detected were randomly assigned 2 : 1 to receive the recommended phase ii dose of either ( 1 ) a predened targeted regimen based on mutation status ( experimental arm ) or ( 2 ) a regimen , chosen from the four study regimens , that did not target their amois ( control arm )  . 
the specic study amois ( data supplement ) were selected on the basis of published functional evidence or implications for protein translation and pathway function ; they were detected in patient samples via a clinical laboratory improvement amendments ( clia ) sequencing assay developed and validated by the molecular characterization laboratory at the frederick national laboratory for cancer research , as previously described.5 patient eligibility determination and randomized treatment assignment were performed with the genemed informatics system as described.6 if more than one amoi was detected for a patient randomly assigned to the experimental arm , the targeted treatment was based on the selection of higher allele frequency ; if allele frequencies were within 15% , the patient was assigned to the targeted treatment cohort with the fewest patients enrolled ( with the option to receive the other treatment regimen upon disease progression )  . 
if a patient randomly assigned to the control arm had multiple nontargeted treatment options , their regimen was chosen based on the proportions of treatment assignments on the experimental arm , so as to balance the two arms with respect to proportions receiving each of the four regimens . for the purpose of assessing the primary end point of this trial , only response to the rst regimen was used . 
adverse events ( aes ) were graded according to nci common toxicity criteria version 4.0 until march 31 , 2018 , when version 5.0 was implemented ; all aes were mapped to version 5.0 before the nal analysis . 
 random assignment and clinical outcome on the nci - mpact trial study agents veliparib ( abt - 888 ; nsc 737664 ) , adavosertib ( azd1775 ; nsc 751084 ) , trametinib ( nsc 763093 ) , and everolimus ( nsc 733504 ) were supplied by the division of cancer treatment and diagnosis , nci , under collaborative research and development agreements with abbvie ( north chicago , il ) , astrazeneca ( cambridge , united kingdom ) , glaxosmithkline ( brentford , united kingdom ) , and novartis ( basel , switzerland ) , respectively . 
study drugs were administered at the recommended phase ii doses and schedules ( data supplement )  . statistical study design the accrual ceiling for each regimen cohort of the experimental arm was set at 30 patients to discriminate between tumor response rates of 20% versus 5% . 
the design included n = 198 enrolled n = 5 did not have biopsy n = 193 had biopsy collected n = 13 insufficient tumor or dna n = 1 declined to participate detceted ioma on dah 17 = n detceted ioma na dah 801 = n n = 7 had no targeted regimen n = 5 had no control regimen but were offered treatment n = 64 randomly assigned to targeted arm n = 32 randomly assigned to control arm n = 10 assigned everolimus n = 25 assigned trametinib n = 3 assigned veliparib plus tmz n = 10 assigned everolimus n = 10 assigned trametinib n = 2 assigned veliparib plus tmz n = 26 assigned adavosertib plus carboplatin n = 10 assigned adavosertib plus carboplatin n = 7 clinically excluded n = 4 died n = 4 declined to participate n = 7 clinically excluded n = 1 died n = 7 declined to participate n = 6 received adavosertib plus carboplatin n = 8 received everolimus n = 20 received trametinib n = 3 received veliparib plus tmz n = 3 received everolimus n = 6 received trametinib n = 2 received veliparib plus tmz n = 8 off treatment : n = 2 death ( pd ) n = 4 pd n = 1 toxicity n = 1 withdrew n = 20 off treatment : n = 19 pd n = 1 withdrew n = 3 off treatment : n = 3 pd n = 3 off treatment : n = 3 pd n = 6 off treatment : n = 5 pd n = 1 withdrew n = 2 off treatment : n = 1 pd n = 1 withdrew n = 6 off treatment : n = 5 pd n = 1 toxicity n = 18 received adavosertib plus carboplatin n = 18 off treatment : n = 13 pd n = 1 intercurrent illness n = 3 toxicity n = 1 withdrew fig 1 . 
seven patients had an amoi but could not be randomly assigned because they were ineligible for the targeted treatment ( six patients : pancreatic cancer with an ras mutation ; one patient : unknown reason )  . 
 chen et al an interim futility analysis ; if no objective responses were observed among the initial 12 patients in each experimental cohort , the cohort was to be terminated early ( with 54% likelihood under the null hypothesis ) , with 93% condence that the response rate would be lower than the target 20% rate . 
this design yields at least 84% power to detect a true objective response rate of at least 20% and at least 0.94 probability of a negative result if the true objective response rate was no more than 5% . 
four - month progression - free survival ( pfs ) , dened as the time from random assignment to progression or death from any cause ( whichever comes rst ) , was evaluated as a secondary end point using kaplan - meier estimates and cis calculated using greenwoods formula . 
twelve or more instances of 4 - month pfs ( at least 40% ) among the 30 patients in an experimental cohort was to be considered promising ; this would occur with 90% likelihood if the true 4 - month pfs rate is 50% ( median pfs of 4 months ) and with 5% likelihood if the true 4 - month pfs rate is 25% ( median pfs of 2 months )  . results enrollment and treatment assignment one hundred ninety - eight patients who met study eligibility criteria were enrolled from january 2014 to april 2018 ( fig 1 , table 1 , data supplement ) , 108 ( 55% ) of whom underwent a tumor biopsy procedure and ultimately had a study - actionable mutation detected ( fig 2a )  . 
patient characteristics characteristic patients enrolled median age , years ( range ) sex ( female / male ) median number of prior lines of therapy ( range ) a patients with karnofsky performance status ( % ) dna repair pi3k ras / raf / mek patients with an amoi in a targeted pathwayb number 60 ( 23 - 83 ) 109 / 89 4 ( 1 - 12 ) abbreviations : amoi , actionable mutation of interest . areported for patients who received at least one dose of study agent on nci - mpact . breported for all patients with an amoi detected on nci - mpact . 
patients with an amoi in more than one pathway are counted here for each affected pathway . 136 2021 by american society of clinical oncology the genes with highest frequency of study amois were tp53 and kras ( 56% and 46% of patients with an amoi , respectively ) ( fig 2c , data supplement )  . 
all patients assigned to the two dna repair pathway cohorts of the experimental arm had a tp53 mutation and 75% of patients assigned to the trametinib experimental cohort had a kras mutation . 
the majority of amois were nonsynonymous single - nucleotide variants ( data supplement )  . toxicity thirty ( 45% ) of the 66 patients who received at least one dose of study agent ( s ) experienced an ae of grade 3 or greater that was considered at least possibly related to study treatment ( data supplement )  . 
seven patients died within 30 days of their last dose of study drugs but none of the on - study deaths were considered related or likely related to the study treatments . treatment compliance interim analysis revealed unanticipated differences in compliance for patients who were assigned to targeted versus nontargeted therapy ( fig 3a )  . 
the overall percentage of patients assigned to the control arm who never initiated treatment was 47% ( 15 / 32 ) , signicantly higher than the rate for patients assigned to the experimental arm ( 23% ; 15 / 64 ; p = .034 , two - sided , by fishers exact test )  . 
evaluation of the reasons why patients came off study , as documented in the clinical database , reveals that a signicantly higher percentage of the patients randomly assigned to the control arm chose not to start treatment ( 22% [ 7 / 32 ] ) compared with the percentage of patients in the experimental arm who chose not to start treatment ( 6% [ 4 / 64 ] ; p = .038 , two - sided , by fishers exact test )  . interim futility analysis accrual to the veliparib plus tmz and everolimus cohorts was slow such that accrual did not reach the 12 - patient threshold for interim analysis of the primary end point , objective response rate ; no responses were measured on either regimen ( fig 3b )  . 
slow accrual to the veliparib plus tmz arm was because of the fact that every dna repair pathway amoi detected on study was within tp53 ; on the basis of preclinical evidence that loss - of - function mutations in tp53 affect regulation of cell cycle progression , patients who were randomly assigned to the experimental arm with these mutations were assigned adavosertib plus carboplatin as their rst - line study treatment if eligible , not veliparib plus tmz . 
pfs events were experienced by 12 / 17 randomly assigned and treated patients in the control arm ; among the patients randomly assigned to the experimental cohorts , pfs events were documented in 6 of 8 treated with everolimus , 20 of 20 treated with trametinib , 13 of 18 treated with adavosertib plus carboplatin , and 3 of 3 treated with veliparib plus tmz . 
caution must be used in comparing the individual experimental cohorts to the control arm as the restriction of an experimental cohort to a particular target may be prognostic of better ( or worse ) pfs . 
 ( a ) nci - mpact treatment compliance rates : the percent of randomly assigned patients who initiated their assigned study treatment or did not start treatment because of death , clinical exclusion that developed after enrollment , or patient choice . 
 ( b ) the proportions of randomly assigned and treated patients who experienced objective response ( complete response or conrmed partial response ) are presented by arm or targeted treatment cohort . 
none of the three patients in the experimental veliparib plus tmz cohort were progressionfree at 4 months ( ci not provided because of small sample size )  . two patients experienced sustained stable disease ( sd ) for a noteworthy 24 cycles of targeted treatment ( fig 5 )  . one patient with endometrial cancer and pik3ca h1047l and pten r130 * amois received everolimus and experienced sd for 24 cycles before progressing . 
the other patient , a 52 - year - old woman with low - grade ovarian cancer with an nras q61r amoi , experienced sd for 27 cycles of trametinib treatment before her disease progressed . 
in the experimental adavosertib plus carboplatin cohort , one patient with endometrial carcinoma and tp53 r213 * and pik3ca c420r amois had an unconrmed pr before coming off treatment because of toxicity . 
none of the patients who crossed over at disease progression from the control arm to a targeted treatment or from one targeted treatment to another experienced clinical benet on the crossover regimen ( data supplement )  . discussion highly effective , tailored therapy targeting specic genetic aberrations is a primary goal of precision medicine.1 , 2 reports of exceptional responders , retrospective studies , and several nonrandomized trials indicate clinical benet for genome - driven treatments , prompting optimism and discussion about the appropriate evidence framework for precision oncology.3 , 8 - 24 the results of our study , which was important considerdesigned in 2012 , highlight several ations for randomized precision oncology studies in the advanced disease setting that have evolved since then.25 - 28 with the greater prevalence of genetic tests and emphasis on precision medicine , it may be very challenging to randomly assign patients to a nontargeted control arour data suggest that some patients and physicians may have had prior tumor mutation prole knowledge and , when randomly assigned to the control arm , appeared to show a bias favoring the presumed precision medicine approach , declining to participate in the study . 
the low dropout rate on the similarly designed shiva trial may be explained by having the patients randomly assigned to a physicians choice control arm ; results from the shiva trial also did not demonstrate the superiority of molecularly targeted agents over the control treatment.25 the results of the winther and coppo trials , two nonrandomized studies , describe clinical benet for a small number of patients with personalized treatment but the pfs - based end point was not met in either study.29 , 30 our results are similar in that the two statistically evaluable experimental cohorts indicate that neither trametinib nor adavosertib plus carboplatin was more effective than standard therapy at achieving objective response when assigned to target nci - mpact - dened amois in ras / raf / mek or dna repair pathways ( eg , kras gain of function or tp53 loss of function mutations , respectively )  . 
 random assignment and clinical outcome on the nci - mpact trial experimental arm control arm 120 - day rate median 120 - day rate median 100 150 200 250 300 350 100 150 200 250 300 350 days since random assignment days since random assignment number at risk number at risk everolimus experimental cohort trametinib experimental cohort 120 - day rate median 120 - day rate median 100 150 200 250 300 350 days since random assignment number at risk 100 150 200 250 300 350 days since random assignmentt number at risk ( b ) control arm , fig 4 . 
 chen et al x age at dx prior disease category cycles best response werdhtiw yticixot withdrew toxicity illness toxicity werdhtiw female genitourinary genitourinary lower gi breast lower gi female genitourinary gender female male female male female female female male female female male male female female female female male female male male female female male male female female female female female male female male male female female female female female male male male female female male female female female male male male female male female male male male male female female female female elamef genitourinary head and neck genitourinary sarcoma genitourinary lower gi lower gi lower gi lung upper gi genitourinary neuroendocrine lower gi genitourinary lower gi lower gi lower gi lower gi lower gi breast sarcoma lower gi genitourinary gi upper head and neck breast lower gi melanoma lower gi breast sarcoma lower gi lower gi genitourinary genitourinary lower gi lung lower gi lower gi lower gi lower gi lower gi breast lower gi lower gi lung lower gi lower gi lower gi lower gi lower gi lower gi female genitourinary lower gi melanoma melanoma lung genitourinary female genitourinary fig 5 . 
each patients detected nci - mpact amois are listed and color - coded to indicate the level of evidence that the mutation is susceptible to the assigned nci - mpact treatment ( based on the information in the oncokb and civic precision oncology knowledge bases at the time of writing )  . 
where available , the results of whole exome sequencing are presented as the number of genetic alterations detected that are annotated in oncokb as either oncogenic ( # oncogenic mutations ) or as oncogenic and actionable with available therapeutic agents ( # oncokb mutations )  . 
 random assignment and clinical outcome on the nci - mpact trial medicine approach , the lack of signicant response on the experimental arm argues for need of better therapies and further validation . 
extensive genetic sequencing and clinical trials evaluating broader aspects of pathway alterations may reveal additional information about actionable sensitivity markers . the targeted treatment assignments in nci - mpact were made based on molecular aberrations that were expected to confer therapeutic sensitivity at the level of a signaling pathway . 
since the trials initiation , the cancer research community has been engaged in an ongoing effort identify geneand variant - specic biomarkers that predict response to drugs.31 - 37 retrospective review of two precision oncology knowledge bases , oncokb and civic , suggests that there is little curated evidence to support many of the amoi - drug associations targeted in the ncimpact trial , which is consistent with the lack of clinical activity . 
for example , tp53 mutations , which were detected in every nci - mpact patient randomly assigned to a targeted dna repair inhibitor cohort , are understood to be oncogenic but have remained largely undruggable.38 the experimental trametinib cohort is the exception in that for each ras / mek / erk pathway amoi that was detected , there is evidence curated in oncokb or civic suggesting effective inhibition by trametinib . 
notably , all three patients who were treated with trametinib to target an nras q61r mutation experienced clinical benet , in line with published clinical evidence of mek inhibitor activity in patients carrying an nras q61 mutation.39 most of the patients treated in the experimental trametinib arm carried an amoi in kras . 
although there is preclinical support for treating kras amois with an mek inhibitor , the results of that approach were modest in this study , perhaps because of reported mechanisms of kras mutant resistance to atpnoncompetitive mek inhibitors.40 - 42 the presence of a therapy - targeted amoi furthermore , in a patient tumor does not indicate whether the amoi is a driver or passenger mutation.43 , 44 in nci - mpact , the most frequently detected amoisthose in tp53 and kraswere detected in all four treatment cohorts and might have contributed to disease progression in cases where treatment was assigned to target an amoi in a different pathway ( eg , akt / pi3k / mtor pathway )  . 
treatment assignment in such cases was made based on the amoi with the highest allele frequency but there is precedent for subclonal molecular alterations driving disease progression.45 - 48 two of the three patients who tolerated everolimus treatment and had amois conned to only the pi3k pathway experienced prolonged sd ( 10 cycles )  . it is important to note that we were able to achieve a successful biopsy collection rate of  . 
90%.49 even with a turnaround time of 10 days for sequencing results , 5 19 biopsied patients ( 10% ) progressed to the point of ineligibility or death before treatment initiation , reecting the advanced disease status of this patient population . 
biopsy sampling could not have identied spatially or temporally isolated tumor subclones that may have been driving tumor growth or conferring resistance in these patients , 43 , 44 , 50 , 51 challenges that can be explored further in preclinical studies as can the presence of putative driver mutations in other signaling pathways . we are completing the analysis of a preclinical study performed in parallel with the nci - mpact trial using xenograft models derived from the tumors of cancer patients to overcome the hurdles inherent to clinical investigations of molecularly targeted treatment response ( manuscript in preparation )  . 
our preliminary data suggest that functional in vivo evidence of activity in molecularly dened models should be the basis on which to evaluate clinical benet of targeted agents in specied patient subgroups . 
chen , md , national cancer institute , 31 center drive , room 3a44 , bethesda , md 20814 ; twitter : @ncitreatment ; e - mail : chenali@ mail.nih.gov. support this project has been funded in whole or in part with federal funds from the national cancer institute , national institutes of health , under contract no . 
mickey williams , richard piekarz , james h . doroshow provision of study materials or patients : shivaani kummar , geraldine osullivan coyne , funda meric - bernstam , stephen leong , chris karlovich collection and assembly of data : alice p . 
konat e , biswajit das , chris karlovich , chih - jian lih , eric polley , richard simon , ming - chung li , richard piekarz , james h . 
mickey williams research funding : illumina patents , royalties , other intellectual property : i was a co - inventor of the dlbcl cell of origin patent recently led by the nih kanwal p . 
trends mol med 23 : 874 - 898 , 2017 tate jg , bamford s , jubb hc , et al : cosmic : the catalogue of somatic mutations in cancer . 
nucleic acids res 47 : d941 - d947 , 2019 lih c - j , sims dj , harrington rd , et al : analytical validation and application of a targeted next - generation sequencing mutation - detection assay for use in treatment assignment in the nci - mpact trial . 
j mol diagn 18 : 51 - 67 , 2016 zhao y , polley ec , li m - c , et al : genemed : an informatics hub for the coordination of next - generation sequencing studies that support precision oncology clinical trials . 
eur j cancer 45 : 228 - 247 , 2009 ottmann og , druker bj , sawyers cl , et al : a phase 2 study of imatinib in patients with relapsed or refractory philadelphia chromosome - positive acute lymphoid leukemias . 
blood 100 : 1965 - 1971 , 2002 sawyers cl , hochhaus a , feldman e , et al : imatinib induces hematologic and cytogenetic responses in patients with chronic myelogenous leukemia in myeloid blast crisis : results of a phase ii study . 
obrien sg , guilhot f , larson ra , et al : imatinib compared with interferon and low - dose cytarabine for newly diagnosed chronic - phase chronic myeloid leukemia . 
fukuoka m , wu yl , thongprasert s , et al : biomarker analyses and nal overall survival results from a phase iii , randomized , open - label , rst - line study of getinib versus carboplatin / paclitaxel in clinically selected patients with advanced non - small - cell lung cancer in asia ( ipass )  . 
rosell r , carcereny e , gervais r , et al : erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutationpositive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
hauschild a , grob jj , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . lancet 380 : 358 - 365 , 2012 16 . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
massard c , michiels s , ferte c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . cancer discov 7 : 586 - 595 , 2017 19 . 
hainsworth jd , meric - bernstam f , swanton c , et al : targeted therapy for advanced solid tumors on the basis of molecular proles : results from mypathway , an open - label , phase iia multiple basket study . 
freidlin b , allegra cj , korn el : moving molecular proling to routine clinical practice : a way forward ? j natl cancer inst 112 : 773 - 778 , 2019 25 . 
le tourneau c , delord j - p , gonalves a , et al : molecularly targeted therapy based on tumour molecular proling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
herbst rs , gandara dr , hirsch fr , et al : lung master protocol ( lung - map ) - a biomarker - driven protocol for accelerating development of therapies for squamous cell lung cancer : swog s1400 . 
goncalves a , bachelot t , lusque a , et al : high - throughput genome analysis and therapeutic decision for patients with her2 - negative metastatic breast cancer : first feasibility and molecular results of the randomized phase ii study safir02 breast ( ucbg - 0105 / 1304 )  . 
tuxen iv , rohrberg ks , oestrup o , et al : copenhagen prospective personalized oncology ( coppo ) clinical utility of using molecular proling to select patients to phase i trials . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
dummer r , schadendorf d , ascierto pa , et al : binimetinib versus dacarbazine in patients with advanced nras - mutant melanoma ( nemo ) : a multicentre , open - label , randomised , phase 3 trial . 
ferry - galow kv , datta v , makhlouf hr , et al : what can be done to improve research biopsy quality in oncology clinical trials ? j oncol pract 14 : e722 - e728 , 2018 50 . 
the aim of our study was to investigate whether ctdna can be used for response monitoring in neuroblastoma . methods one hundred forty - nine plasma samples from 56 patients were analyzed by quantitative polymerase chain reaction ( qpcr ) for total cell free dna ( cfdna ; albumin and - actin ) and ctdna ( hypermethylated rassf1a )  . 
ctdna results were compared with mrna - based minimal residual disease ( qpcr ) in bone marrow ( bm ) and blood and clinical patient characteristics . results ctdna was detected at diagnosis in all patients with high - risk and stage m neuroblastoma and in 3 of 7 patients with localized disease . 
the discrepancies indicated either low - level bm inltration ( ctdna negative / mrna positive ) or primary tumor / soft tissue lesions with no bm involvement ( ctdna positive / mrna negative )  . conclusion ctdna can be used for monitoring disease in patients with neuroblastoma . 
it is likely that ctdna can originate from both primary tumor and metastases and may be of special interest for disease monitoring in patients who experience relapse in other organs than bm . jco precis oncol 4 : 291 - 306 . 
2020 by american society of clinical oncology creative commons attribution non - commercial no derivatives 4.0 license introduction neuroblastoma is the most common extracranial solid tumor of childhood . in approximately 50% , patients present with high - risk ( hr ) disease and are treated with intensive multimodality treatment protocols that encompass induction therapy , primary tumor surgery , myeloablative chemotherapy with autologous stem - cell rescue , local irradiation , and anti - gd2based immunotherapy1 ( appendix fig a1 )  . 
despite this intensive therapy , in approximately one half of hr patients , the tumor will relapse and result in a fatal outcome.2 assessment of treatment response is based on the international neuroblastoma response criteria . 
meta - iodobenzylguanidine ( mibg ) scintigraphy , imaging ( magnetic resonance imaging / positron emission tomography scans ) , and bone marrow ( bm ) examinations by histology or ( immuno ) cytology are combined to assess the extent of disease.3 because the median age at diagnosis is 18.8 months , 4 response evaluation that is based on imaging and bm testing often must be performed under general anesthesia . 
 van zogchel et al context key objective can hypermethylated rassf1a be used as a circulating tumor dna ( ctdna ) marker for minimal residual disease detection in neuroblastoma ? knowledge generated when testing cell free dna , we were able to detect tumor - derived hypermethylated rassf1a in all patients with stage m disease at diagnosis . 
comparison between ctdna and bloodor bone marrow ( bm ) derived mrna revealed that discrepancies were found when bm inltration was low or when there were primary tumor lesions without bm involvement . relevance ctdna is an interesting source for monitoring disease in patients with neuroblastoma . 
our data indicate that testing of both ctdna and mrna increases the sensitivity of molecular disease monitoring . several studies have shown the feasibility of detecting mutations or tumor - specic translocations in the ctdna by high - depth targeted sequencing or mutation - specic pcr to monitor disease in various types of adult cancer.13 - 19 however , neuroblastoma tumors , like many pediatric tumors , lack recurrent mutations and translocations . 
broader analysis , such as whole - exome sequencing ( wes ) and shallow whole - genome sequencing ( swgs ) , to detect tumor - specic mutations or copy number alterations have been performed successfully using cfdna of patients with neuroblastoma at diagnosis and relapse.20 - 26 nevertheless , these techniques are only informative when the ctdna content is approximately 10%27 and are , therefore , less suited for the detection of mrd , when the tumor burden is low . in contrast to the copy number alterations and tumorspecic mutations , a methylation - specic qpcr assay could potentially be a more general and sensitive ctdna marker . 
hypermethylated rassf1a ( rassf1am ) can be detected in bm with a similar sensitivity as mrna and has shown added value in mrna - negative bm.28 in addition , rassf1am already has been described as a prognostic ctdna marker at diagnosis.29 the aim of this study was to investigate the feasibility of using ctdna ( rassf1am in plasma ) to monitor treatment response in patients with hr / stage m neuroblastoma . 
we retrospectively performed qpcr for rassf1am on cfdna from stored remains of previously collected plasma samples of patients with localized or metastatic neuroblastoma at diagnosis and for patients with hr / stage m neuroblastoma during treatment and at relapse . 
to test the additional value of ctdna monitoring , we compared it with other techniques for disease monitoring : mibg scans , urinary catecholamines , immunocytology , and rt - qpcr rna - based mrd detection in bm and peripheral blood ( pb )  . methods between 2013 and 2016 , from all consecutively diagnosed patients who were included in this study ( n = 56 ) , 149 pb samples for mrna and cfdna and 105 bm samples for mrna were tested . 
pediatric pb control samples were collected from the amsterdam umc ( appendix table a1 )  . sample collection , dna isolation , bisulte conversion , and real - time qpcr methods for sample collection , dna isolation , bisulte conversion , and real - time qpcr for rassf1am28 and mrna markers31 can be found in the appendix and appendix table a2 . data analysis total cfdna was quantied by qpcr for albumin ( alb ) or - actin ( actb )  . 
all statistical analyses were performed with spss version 23 ( ibm corporation , chicago , il ) or graphpad prism 8 ( graphpad software , la jolla , ca ) software . results patients and samples from 48 patients with hr and / or stage m and 8 patients with non - hr neuroblastoma , 149 samples were tested in this study ( fig 1 )  . 
six of the 149 patient samples and 12 of 73 healthy control samples were not included for rassf1am qpcr because too much dna had been lost during bisulte conversion ( fig 1 )  . 
flowchart of samples tested for total cell free dna ( cfdna ) , number of samples excluded after too much dna had been lost after bisulte conversion , and number of samples tested for circulating tumor dna ( ctdna ) by hypermethylated rassf1a ( rassf1am )  . 
the percentage of ctdna of total cfdna , calculated with the equation [ rassf1am / ( rassf1am + unmethylated rassf1a ) 100 ] , was 94% ( range , 82% - 98% ) in the 14 diagnostic samples from patients with stage m disease . 
compared with the individual mrna markers , rassf1am was more often positive , but the combined mrna markers identied the same positive samples as rassf1am ( appendix table a4 )  . in 93 matched bm mrna and ctdna ( pb ) samples , double - negative or double - positive results were found in 77% ( fig 3b )  . 
in contrast to pb , the bm mrna panel identied more positive samples than ctdna , and the individual markers phox2b and th correlated best with rassf1am ( appendix table a4 )  . discrepant findings between ctdna and pb or bm mrna mrd discrepant results between ctdna and mrna were detected in 27 pb and 21 bm samples , respectively , and listed in table 3 and appendix table a4 . 
from 3 of 5 bm mrna - negative / ctdnapositive samples , cryopreserved bm cells were available and tested all negative for rassf1ain some patients ( n850 , n865 , n732 ) , the high levels of ctdna probably correlated with the large primary or local relapse tumors , and these patients had no or very little bm inltration . in the ctdna - negative samples , in general , the cfdna levels were lower , with a median of 6.1 ng / ml for the bm mrna - positive / ctdna - negative and 1.52 ng / ml for the pb mrna - positive / ctdna - negative samples . 
from 15 of negative samples , cryopreserved cells were available and tested for rassf1am ; of the 5 positive samples , 4 were not in the quantitative range , which indicated low levels of bm inltration . in the samples from patients n777 , n798 , n2011 , n2014 , and n802 , no ctdna was detected . 
begin induction indicates until 2 courses of induction therapy ; mid - induction indicates after 3 - 5 courses of induction chemotherapy , unless additional courses were given after 6 courses , and samples before last course were also included at this time point ; end induction indicates at the end of induction therapy ; surveillance indicates during follow - up or at relapse suspicion ; and event indicates relapse or progression . 
of samples diagnosis samples localized and stage ms stage m follow - up samples beginning of induction therapy mid - induction therapy end of induction therapy postconsolidation surveillance progression relapse / refractory disease relapse therapy note . 
positive indicates that rassf1am circulating tumor dna was detected and quantied , and negative indicates that no rassf1am circulating tumor dna was detected . abbreviations : pnq , positive not quantiable ; rafssf1am , hypermethylated rafssf1a . complete remission at that time . 
patient n802 was treated for an isolated cns relapse . in the samples from patients n2012 , n2013 , n2016 , n2024 , n2029 , and n2031 , no ctdna was detected , while low amounts of mrna were detected in the bm . in the case of restricted , minimal bm disease , mrna detection was more sensitive than ctdna ( appendix table a4 )  . 
however , in some patients , a primary tumor was still present ( median , 50 mm ) while ctdna was negative ( table 3 )  . discussion ctdna in plasma is a powerful source for the detection of tumor - derived aberrations in a minimally invasive setting . many ctdna studies in adults for the detection of mrd are based on detection of tumor - specic mutations by targeted sequencing or digital droplet pcr ( ddpcr ) .12 , 16 , 17 because recurrent mutations are not common in neuroblastoma , 32 tumor - specic aberrations need to be characterized before they can be used as an mrd marker . 
however , temporospatial heterogeneity has been reported in neuroblastoma by several studies , 20 , 26 which raises the question of whether we should only use the small part of the tumor that is derived from the biopsy to design tumor - specic mrd markers . 
first , it is a sensitive marker , with a sensitivity of 1 tumor cell in 105 mononuclear cells.28 second , rassf1am qpcr can be used in all patients with stage m neuroblastoma because it has been shown that rassf1a is hypermethylated in all previously tested stage m neuroblastoma tumors.28 third , detection of rassf1am is less costly compared with wes and even swgs ( approximately 40and 10 - fold less expensive , respectively )  . 
hypermethylation of rassf1a has been described in several types of cancer and in physiologic circumstances in placental cells.33 rassf1a is not methylated in normal hematologic cells.28 , 33 , 34 however , in 2 of 61 samples from healthy individuals , we detected very low , nonquantiable levels of rassf1ain diagnosis or relapse other diagnosis or relapse other n = 11 n = 12 n = 23 n = 16 n = 12 n = 124 positive negative positive negative n = 66 n = 12 n = 4 n = 36 n = 4 n = 1 negative ctdna ( rassf1am ) positive negative ctdna ( rassf1am ) positive fig 3 . 
 van zogchel et al addition , in other studies , infrequent detection of rassf1am has been observed in plasma samples from healthy control participants.35 , 36 therefore , when detecting verylow levels of rassf1am in patients with neuroblastoma ( indicated as pnq range ) , results should be analyzed with caution . it has been shown that neuroblastoma tumors shed high amounts of ctdna in the plasma.25 , 26 , 37 in the current study , we found a median cfdna concentration of 73.1 ng / ml at diagnosis for patients with stage m disease . 
however , the levels we found are lower compared with previously published studies.25 , 26 , 37 this inconsistency may be due to differences in isolation of cfdna because we did not use a circulating nucleic acid kit or to differences in quantication methods . 
we found the majority of the cfdna ( 94% at diagnosis ) to be tumor derived in patients with stage m or hr disease , which is also supported by previous research.26 , 37 we tested 143 samples from 54 patients with neuroblastoma and detected ctdna in 57 samples . 
ctdna was detected at diagnosis in all 14 patients with stage m and 4 of 8 patients with localized and stage ms neuroblastoma . misawa et al29 described detection of rassf1am at diagnosis in the serum of 17 of 68 patients ( all stages ) and in 11 of 18 patients with stage m disease . 
there are two likely causes for the increased ctdna detection in our study . first , we used plasma , whereas misawa et al tested serum , which is known to be more contaminated by genomic dna originated from leukocytes during ex vivo clotting.38 second , misawa et al used conventional pcr , which is less sensitive than qpcr . 
our group has previously described that hypermethylation of rassf1a is variable in tumors of patients with stage ms ( median , 65% ) and localized ( median , 30% ) disease28 ; therefore , the level of ctdna can be slightly underestimated in these patients when using rassf1am as marker . we compared the performance of ctdna with pb and bm mrna in 128 and 93 samples , respectively . 
most patients in whom we detected relatively high levels of ctdna compared with pb or bm mrnas still had considerable tumor volumes or negative or low mibg scores ( data not shown ) ; therefore , it is likely that the ctdna in these patients originated from the primary tumor . 
two of these patients were in complete remission but in the other 15 patients , considerable tumor volumes were detected on imaging or urine catecholamines were still positive , which indicate the need to optimize pre - analytic sample handling and prospective study of cfdna kinetics in well - characterized patient cohorts with available paired ( nuclear ) imaging and bm assessment . while the detection of ctdna is very promising for future mrd studies , the current study has some limitations . stored remains were used , which resulted in missing samples and paired clinical data . 
for detection and quantication of low levels of ctdna in the plasma , dna extraction methods can be optimized with an isolation method specic for cfdna , and ddpcr39 may be a more suited technique compared with qpcr.40 moreover , large amounts of cfdna ( up to 96% ) could be destroyed during bisulte conversion41 ; therefore , we are investigating alternative methylation - specic ddpcr methods . 
previous studies showed that rassf1a was the most frequent hypermethylated tumor suppressor gene in neuroblastoma as well as identied other hypermethylated tumor suppressor genes , and inclusion of these genes as mrd markers might increase the sensitivity.42 , 43 in this study , we used rassf1am as a ctdna marker . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . no potential conicts of interest were reported . references pinto nr , applebaum ma , volchenboum sl , et al : advances in risk classication and treatment strategies for neuroblastoma . 
j clin oncol 33 : 3008 - 3017 , 2015 park jr , kreissman sg , london wb , et al : effect of tandem autologous stem cell transplant vs single transplant on event - free survival in patients with high - risk neuroblastoma : a randomized clinical trial . 
jama 322 : 746 - 755 , 2019 park jr , bagatell r , cohn sl , et al : revisions to the international neuroblastoma response criteria : a consensus statement from the national cancer institute clinical trials planning meeting . 
j clin oncol 35 : 2580 - 2587 , 2017 london wb , castleberry rp , matthay kk , et al : evidence for an age cutoff greater than 365 days for neuroblastoma risk group stratication in the childrens oncology group . 
j clin oncol 23 : 6459 - 6465 , 2005 viprey vf , gregory wm , corrias mv , et al : neuroblastoma mrnas predict outcome in children with stage 4 neuroblastoma : a european hr - nbl1 / siopen study . 
j clin oncol 32 : 1074 - 1083 , 2014 cheung nk , ostrovnaya i , kuk d , et al : bone marrow minimal residual disease was an early response marker and a consistent independent predictor of survival after anti - gd2 immunotherapy . 
j clin oncol 33 : 755 - 763 , 2015 kreissman sg , seeger rc , matthay kk , et al : purged versus non - purged peripheral blood stem - cell transplantation for high - risk neuroblastoma ( cog a3973 ) : a randomised phase 3 trial . 
lancet oncol 14 : 999 - 1008 , 2013 burchill sa , beiske k , shimada h , et al : recommendations for the standardization of bone marrow disease assessment and reporting in children with neuroblastoma on behalf of the international neuroblastoma response criteria bone marrow working group . 
cancer 123 : 1095 - 1105 , 2017 stutterheim j , zappeij - kannegieter l , versteeg r , et al : the prognostic value of fast molecular response of marrow disease in patients aged over 1 year with stage 4 neuroblastoma . 
gormally e , caboux e , vineis p , et al : circulating free dna in plasma or serum as biomarker of carcinogenesis : practical aspects and biological signicance . mutat res 635 : 105 - 117 , 2007 2017 12 . 
mcbride dj , orpana ak , sotiriou c , et al : use of cancer - specic genomic rearrangements to quantify disease burden in plasma from patients with solid tumors . genes chromosomes cancer 49 : 1062 - 1069 , 2010 16 . 
tsao sc , weiss j , hudson c , et al : monitoring response to therapy in melanoma by quantifying circulating tumour dna with droplet digital pcr for braf and 18 . 
van roy n , van der linden m , menten b , et al : shallow whole genome sequencing on circulating cell - free dna allows reliable noninvasive copy - number proling in neuroblastoma patients . 
chicard m , colmet - daage l , clement n , et al : whole - exome sequencing of cell - free dna reveals temporo - spatial heterogeneity and identies treatmentresistant clones in neuroblastoma . 
yanik ga , parisi mt , shulkin bl , et al : semiquantitative mibg scoring as a prognostic indicator in patients with stage 4 neuroblastoma : a report from the 31 . 
stutterheim j , gerritsen a , zappeij - kannegieter l , et al : detecting minimal residual disease in neuroblastoma : the superiority of a panel of real - time quantitative 32 . 
chan kc , ding c , gerovassili a , et al : hypermethylated rassf1a in maternal plasma : a universal fetal dna marker that improves the reliability of noninvasive prenatal diagnosis . 
scheffer pg , de haas m , van der schoot ce : the controversy about controls for fetal blood group genotyping by cell - free fetal dna in maternal plasma . 
white he , dent cl , hall vj , et al : evaluation of a novel assay for detection of the fetal marker rassf1a : facilitating improved diagnostic reliability of noninvasive opin hematol 18 : 467 - 473 , 2011 prenatal diagnosis . 
wong fc , sun k , jiang p , et al : cell - free dna in maternal plasma and serum : a comparison of quantity , quality and tissue origin using genomic and epigenomic approaches . 
 circulating tumor dna in neuroblastoma appendix sample collection clinical samples were collected in edta tubes and processed within 24 hours , and 2 ml peripheral blood ( pb ) or 0.5 ml bone marrow ( bm ) was transferred to paxgene blood rna tubes ( qiagen , venlo , the netherlands ) and stored at 20c . 
mononuclear cells were isolated from the remaining bm sample by ficoll density centrifugation and cryopreserved in 10% dimethyl sulfoxide . dna isolation and bisulte conversion dependent on the available plasma volume , dna was extracted by using the qiaamp dna mini blood kit ( qiagen ) for 200 l plasma , or the magna pure 96 isolation robot ( roche , basel , switzerland ) for 500 - 1 , 000 l plasma and eluted in h2o . 
converted dna samples were used directly or stored at 20c . real - time quantitative polymerase chain reaction real - time quantitative polymerase chain reaction ( qpcr ) was performed as previously described ( van wezel em , et al : j mol diagn 17 : 43 - 52 , 2015 )  . 
primer and probe sequences have been described previously28 ( scheffer pg , et al : bjog 118 : 1340 - 1348 , 2011 ) and are listed in appendix table a2 . 
qpcr for alb , actb , and unmethylated rassf1a was performed in duplicate ; hypermethylated rassf1a was tested in triplicate . pb and bm mrna reverse transcriptase qpcr total rna from whole blood and bm samples was extracted using the paxgene blood rna kit ( qiagen ) according to the manufacturers instructions . 
cdna was synthesized and reverse transcriptase ( rt ) qpcr , with a maximum of 50 cycles was performed for - glucuronidase ( gusb ) , paired ctdna in neuroblastoma like homeobox 2b ( phox2b ) , tyrosine hydroxylase ( th ) , dopa decarboxylase ( ddc ) , growth - associated protein 43 ( gap43 ) , cholinergic receptor nicotinic - 3 ( chrna3 ) , and dopamine - hydroxylase ( dbh ) , as has been described previously.31 expression was normalized to gusb expression using the following equation : [ normalized threshold cycle ( ct ) = ( ctgusb ctmarker ) ]  . 
samples were scored for positivity according to previously published thresholds9 , 31 ( stutterheim j , et al : j clin oncol 26 : 5443 - 5449 , 2008 )  . 
we examined the frequency and characteristics of braf - mutated lgsc and described the response to treatment with braf inhibitors . patients and methods mutations were assessed in lgsc ( n = 65 ) by using targeted , exome , and whole - genome sequencing . 
braf inhibitors were trialed in two patients with a somatic braf v600e mutation : one patient received dabrafenib monotherapy and was monitored clinically , biochemically ( cancer antigen [ ca ] - 125 levels ) , and with positron emission tomography ( pet ) imaging . 
expression of the braf v600e protein in this patient was assessed by immunohistochemistry . results among patients with lgsc , nine ( 13.8% ) of 65 had a somatic braf mutation . 
two patients with braf v600e mutation received braf inhibitors at relapse and both achieved durable responses . conclusion braf mutations are not uncommon in patients with lgsc and should be routinely tested , because braf inhibitors can be an effective treatment for these patients . 
2018 by american society of clinical oncology introduction epithelial ovarian cancer ( eoc ) is a heterogeneous disease composed of several histologic and molecular subtypes , and emerging molecular analyses are challenging longstanding clinical treatment paradigms . 
eoc subtypes are characterized by different gene expression and somatic mutation patterns and by varying degrees of sensitivity to current standard carboplatin - paclitaxel combination chemotherapy.1 - 3 the predominant type of eoc is serous carcinoma , which accounts for approximately 80% of occurrences . 
 serous carcinoma is then classified into two main subtypes : the more common and better characterized high - grade serous carcinoma , and the less common low - grade serous carcinoma ( lgsc )  . 
lgsc generally is not responsive to standard platinum - based chemotherapy , 4 , 5 and the outcome is poor in women who have residual disease after debulking surgery , 6 - 8 which underscores the need for alternative therapeutic options . lgsc is molecularly distinct from high - grade serous carcinoma and is characterized by activating mutations of the ras sarcomamitogen - activated protein kinase ( ras - mapk ) pathway . 
 the mapk pathway and can be found in several cancer types , most often in melanoma.13 the reported frequency of braf mutations in lgsc varies from 2% to 33%11 , 14 - 16 and these mutations also are found in up to 46% of serous borderline tumors.17 , 18 clinical trials have shown impressive response rates to braf inhibitors in braf - mutant melanoma , and braf inhibitor use in metastatic melanoma is now considered standard of care.19 , 20 responses in other tumor types , including gastrointestinal stromal tumor , thyroid papillary cancer , hairy cell leukemia , and high - grade colorectal neuroendocrine tumors , also have been reported.21 - 26 however , some cancer types , such as colorectal adenocarcinoma , have much lower response rates to braf inhibitors despite the presence of the same somatic braf mutations.27 - 29 thus , although oncogenic braf represents a potential therapeutic target , responses vary according to tumor type , and clinical benefit is not always achieved . 
 we incorporated the shift from a three - tier grading system to a two - tier grading system , as recommended in the 2014 who classification of ovarian tumors.31 patient cases of lgsc were identified from review of diagnostic pathology reports and independent review of hematoxylin and eosinstained diagnostic slides by expert gynepathologists . 
in addition , grade 2 occurrences were screened for tp53 mutations , and only those that were wild type , consistent with a molecular classification of lgsc , were included in the lgsc cohort . clinical definitions progression - free survival was calculated as the time interval from date of histologic or cytologic diagnosis to the date of first progression based on gynecologic cancer intergroup ( gcig ) criteria.32 overall survival was calculated from date of diagnosis to date of death as a result of any cause . 
treatment response was assigned according to gcig cancer antigen ( ca ) 125 criteria.32 briefly , 50% or greater reduction in serum ca - 125 from an elevated pretreatment level , confirmed and maintained for at least 28 days , was considered a response . 
the aocs was approved by the human research ethics committee at the peter maccallum cancer centre , queensland institute of medical research , westmead hospital , and at all other participating hospitals . 
the gynbiobank and this study were approved by the western sydney local health district human research ethics committee . written informed consent was obtained from the patient treated with dabrafenib to include clinical information and imaging . 
this process also was approved by the western sydney local health district human research ethics committee . sequencing and immunohistochemistry frozen or fixed tumor samples were sectioned , and hematoxylin and eosin stains were used to assess tumor content before and after serial sectioning for nucleic acid extraction . 
for samples that contained less than 70% tumor , needle dissection of tumor cells was performed on sections of up to 50 10 extractions were performed using the dneasy blood and tissue kit or qiaamp dna mini kit ( qiagen , hilden , germany )  . 
mutations in exon 15 of braf , exon 2 of kras , exon 20 of erbb2 , and exons 2 to 11 of tp53 were screened by high - resolution melt analysis and validated by direct sequencing , as previously described.8 , 9 a subset of cases was screened by next - generation sequencing . 
target enrichment of the dna samples was performed according to the manufacturers protocol.34 the polymerase chain reactions for each sample were pooled , and target enriched dna samples were purified with agencourt ampure xp beads ( beckman coulter , indianapolis , in )  . 
the dna libraries were prepared according to qiagen protocols.35 dna libraries ( > 4 nm ) were sequenced on a miseq ( illumina , san diego , ca ) at the australian genome research facility ( melbourne , victoria , australia ) , with a read length of 2 150 base pairs . 
samples of the ovarian tumor from the primary surgery specimen and in biopsies at disease relapse were stained for mutated braf v600e with a mutation - specific monoclonal antibody ( mouse antihuman braf v600e monoclonal antibody , clone ve1 ; spring biosciences , pleasanton , ca ) by using the ventana benchmark ultra immunohistochemistry staining module ( ventana medical systems , tucson , az ) with a 1 - in - 200 antibody dilution . 
most ( eight [ 89% ] of nine ) were braf v600e mutations , a shared hot - spot mutation locus found in diverse cancer types ; one was a braf l597r mutation , an uncommon missense variant ( table 1 )  . in three braf - mutant tumors , additional variants identified by wes and wgs predicted alteration in the protein sequence ( range , 13 to 30 variations per patient case ; table 2 ) at lower allele frequencies than the braf mutations , which suggests subclonal events.8 , 37 there was no evidence of additional driver mutations , and no genes with deleterious mutationsother than brafwere common to the three patient cases . clinical features of braf mutation positive lgsc occurrences among patients with braf - mutation positive lgsc , age at diagnosis ranged from 22 to 77 years ( median , 51 years ; table 1 )  . 
the majority had international federation of gynecology and obstetrics ( figo ) stage iii or iv disease at diagnosis ( seven [ 78% ] of nine patients )  . all patients with braf - mutated lgsc had surgery as part of primary treatment , and most tumors ( seven [ 78% ] of nine ) were optimally debulked to no macroscopic residual disease . 
 the median follow - up time was 61.5 months , and five ( 56% ) of the nine patients remained progression free ( table 1 )  . treatment and clinical course in patients with braf mutationpositive lgsc after disease progression four patients experienced progression , and all four had relatively short progression - free survival ( table 1 ; fig 2 )  . 
sections ( 4 m ) from formalin - fixed , paraffin - embedded tumor tissue blocks were stained with hematoxylin and eos ( a ) patient case 1 , publishing id 65928 ; ( b ) patient case 2 , publishing id 11368 ; ( c ) patient case 3 , publishing id 5711 ; ( d ) patient case 4 , publishing id 65917 ; ( e ) patient case 5 , publishing id 65854 ; ( f ) patient case 6 , publishing id 10693 ; ( g ) patient case 7 , publishing id 9125 ; ( h ) patient case 8 , publishing id 11014 ; and ( i ) patient case 9 , publishing id 66198 . progression and died 2 months after the completion of treatment . 
overall survival was less than 2 years from her initial diagnosis . patient case 8 was diagnosed with stage iv ovarian cancer at age 31 years ( fig 2b )  . 
at additional disease progression , the patient entered a phase i trial of the braf inhibitor dabrafenib21 ( glaxosmithkline , sydney , australia ) and received 100 mg twice daily . 
the serum cancer antigen ( ca ) - 125 levels and treatment throughout the clinical course of patients : ( a ) patient case 6 , publishing id 10693 ; ( b ) patient case 8 , publishing id 11014 ; ( c ) patient case 4 , publishing id 65917 ; and ( d ) patient case 9 , publishing id 66198 . which promptly decreased after resumption of dabrafenib . 
expression of braf v600e in patient case 4 : immunohistochemical staining that used an antibody specific for braf v600e in formalin - fixed , paraffin - embedded tumor tissue sections of ( a ) left ovarian tumor from the primary surgical specimen , ( b ) left supraclavicular fossa lymph node core biopsy before second dabrafenib treatment at 78 months , and ( c ) left para - aortic lymph node core biopsy before second dabrafenib treatment at 78 months . 
the bar indicates a 50 - m scale . during treatment with dabrafenib 150 mg twice daily ( 50% higher than her previous dose ) , there was an impressive clinical response , which included reduced analgesic requirements , improved well - being , and marked reduction in the palpable supraclavicular lymph node . 
a positron emission tomography / computed tomography scan confirmed a significant partial radiologic response to treatment ( 63% decrease in sum of diameters of measured lesions ) and significantly fewer metabolically active lesions throughout almost all nodal regions and pulmonary nodules ( fig 4 )  . at the time of censoring , the patient continued to receive dabrafenib , and her ca125 had remained within normal range for 4 months . 
with disease progression , she was enrolled into a braf inhibitor basket trial ( desai et al , manuscript in preparation ) and has received treatment for more than 12 months . 
this patient experienced a partial radiologic response ( bo gao , personal communication , december 2017 ) and normalization of her ca - 125 level with treatment with a braf inhibitor ( fig 2d )  . discussion here , we report clinical outcomes in , to our knowledge , one of the largest series of patients with braf mutationpositive lgsc reported to date . 
we also report the first , to our knowledge , response to the braf inhibitor dabrafenib in a patient who has lgsc with a somatic braf v600e mutation . lgsc typically is tp53 wild type and commonly harbors ras and raf pathway mutations.9 , 14 , 18 this finding has led to clinical trials to evaluate mapk / erk kinase ( mek ) inhibitor activity . 
 a phase ii trial to evaluate the response to the mek inhibitor selumetinib in lgsc reported a promising response rate of 15%.39 response was not associated with known braf / kras mutation status , although this may be due to the small number of cases with known mutations in the trial . 
it is unclear whether all mutation subtypes of lgsc respond similarly to mek inhibition . we found braf mutations in 13.8% ( nine of 65 ) of patients with lgsc , which falls within the broad range reported previously ( 2% to 33% ) .11 , 14 - 16 , 40 this was similar to the 17.9% rate ( 10 of 56 patients ) reported by xing et al40 in a similarly sized cohort and was slightly higher than rate in the american association for cancer research genie project database , for which the frequency of patients with braf mutations in lgsc was four ( 7% ) of 56 patients.41 the genie project contains genomic records generated in clia / isocertified laboratories obtained at multiple tertiary referral centers41 and may be enriched for patients with late - stage disease who seek biomarker - driven clinical trials , whereas patients enrolled in this study were prospectively recruited from clinics . some studies have suggested that braf v600e mutations in lgsc are rare and are associated with early - stage disease and improved prognosis.15 , 16 , 42 however , we found that most women with a braf mutationpositive carcinoma were diagnosed at an advanced stage . 
 [ 18f ] - fluorodeoxyglucose ( 18f - fdg ) pet / ct ( siemens biograph mct , knoxville , tn ) images ( a , b , and c ) before and ( d , e , and f ) after 7 months of second dabrafenib treatment that indicated response to treatment with decrease in size and metabolic activity of lesions . 
the right common iliac node ( c ) before and ( f ) after 7 months of second treatment with dabrafenib . before dabrafenib 7 months on dabrafenib to no residual disease , which is associated with improved prognosis . 
 two others received braf inhibitors , and both achieved sustained response . patient case 4 initially received dabrafenib as part of a dose - finding phase i trial , 21 and , although some response was observed with deceased serum ca - 125 levels , a much more profound response was seen when the patient was retreated with dabrafenib 46 months later . 
 the explanation for the improved response with subsequent dabrafenib treatment is potentially multifactorial and may include the increased dosage , in line with current melanoma dosing guidelines , which suggests that her original dose was subtherapeutic.43 the patient also had a 25 - kg weight loss between dabrafenib treatment periods , although there is no evidence to date that the dabrafenib dose requires adjustment for weight.43 there also is emerging evidence that braf inhibitors may act in part via an effect on host immunity , 44 , 45 and it is possible that an uncharacterized immunologic component contributed to the response in this patient . consistent with our findings , responses to another braf inhibitor , vemurafenib , have been reported in lgsc . 
 the only patient with lgsc in a basket trial of a novel braf inhibitor ( desai et al , manuscript in preparation ) ; her disease has shown a sustained response , which provides additional evidence that braf v600e mutationpositive tumors in lgsc are broadly responsive to braf inhibition . in conclusion , recurrent lgsc is relatively chemotherapy resistant , and targeted treatment may play an important role in improvement of patient outcomes . 
our results are consistent with recent reports of response to braf inhibition in at least two other studies30 , 46 and suggest that braf inhibitors may be an effective option in patients with relapsed , braf mutationpositive lgsc . 
wain , russell hogg , sian fereday , nadia traficante , alexander dobrovic , anna defazio data analysis and interpretation : tania moujaber , dariush etemadmoghadam , yoke - eng chiew , rosemary l . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . tania moujaber no relationship to disclose dariush etemadmoghadam no relationship to disclose catherine saunders employment : macquarie medical imaging yoke - eng chiew no relationship to disclose rosemary l . 
wain no relationship to disclose bo gao no relationship to disclose russell hogg no relationship to disclose sivatharsny sirangan no relationship to disclose casina kan no relationship to disclose sian fereday research funding : astrazeneca ( inst ) nadia traficante research funding : astrazeneca ( inst ) ann - marie patch no relationship to disclose john v . 
 alexander dobrovic honoraria : astrazeneca , amgen consulting or advisory role : astrazeneca , amgen research funding : astrazeneca ( inst ) patents , royalties , other intellectual property : hold a patent related to a novel treatment target in ovarian cancer david d.l. 
we also thank georgina long , bsc , phd , mbbs , fracp , a primary investigator on the phase i dabrafenib trial ; glaxosmithkline and novartis oncology for providing the treatment drug , dabrafenib , on a compassionate use basis ; the american association for cancer research ( aacr ) for its financial and material support in the development of the aacr project genie registry ; and members of the consortium for their commitment to data sharing . 
bowtell , dariush etemadmoghadam , and alexander dobrovic , university of melbourne ; alexander dobrovic , olivia newton john cancer research institute , heidelberg ( melbourne ) , and la trobe university , bundoora , victoria ; ann - marie patch , john v . 
12 / rig / 1 - 17 and 15 / rig / 1 - 16 and is a member bank of the australasian biospecimens network - oncology , funded by nhmrc nos . 
damd17 - 01 - 1 - 0729 , the cancer council victoria , queensland cancer fund , the cancer council new south wales , the cancer council south australia , the cancer foundation of western australia , the cancer council tasmania , and the nhmrc nos . 
seidman jd , horkayne - szakaly i , haiba m , et al : the histologic type and stage distribution of ovarian carcinomas of surface epithelial origint j gynecol pathol 23 : 41 - 44 , 2004 2 . 
schmeler km , sun cc , bodurka dc , et al : neoadjuvant chemotherapy for low - grade serous carcinoma of the ovary or peritoneugynecol oncol 108 : 510 - 514 , 2008 5 . 
grabowski jp , harter p , heitz f , et al : operability and chemotherapy responsiveness in advanced low - grade serous ovarian cancer : an analysis of the ago study group metadatabase . 
emmanuel c , chiew ye , george j , et al : genomic classification of serous ovarian cancer with adjacent borderline differentiates ras pathway and tp53 - mutant tumors and identifies nras as an oncogenic driver . 
singer g , sthr r , cope l , et al : patterns of p53 mutations separate ovarian serous borderline tumors and lowand high - grade carcinomas and provide support for a new model of ovarian carcinogenesis : a mutational analysis with immunohistochemical correlation . 
grisham rn , iyer g , garg k , et al : braf mutation is associated with early stage disease and improved outcome in patients with low - grade serous ovarian cancer . 
anglesio ms , arnold jm , george j , et al : mutation of erbb2 provides a novel alternative mechanism for the ubiquitous activation of ras - mapk in ovarian serous low malignant potential tumors . 
sieben nl , macropoulos p , roemen gm , et al : in ovarian neoplasms , braf , but not kras , mutations are restricted to low - grade serous tumours . 
hauschild a , grob j - j , demidov lv , et al : dabrafenib in braf - mutated metastatic melanoma : a multicentre , open - label , phase 3 randomised controlled trial . 
falchook gs , long gv , kurzrock r , et al : dabrafenib in patients with melanoma , untreated brain metastases , and other solid tumours : a phase 1 dose - escalation trial . 
falchook gs , trent jc , heinrich mc , et al : braf mutant gastrointestinal stromal tumor : first report of regression with braf inhibitor dabrafenib ( gsk2118436 ) and whole exomic sequencing for analysis of acquired resistance . 
klempner sj , gershenhorn b , tran p , et al : brafv600e mutations in high - grade colorectal neuroendocrine tumors may predict responsiveness to braf - mek combination therapy . 
mao m , tian f , mariadason jm , et al : resistance to braf inhibition in braf - mutant colon cancer can be overcome with pi3k inhibition or demethylating agents . 
rustin gj , vergote i , eisenhauer e , et al : definitions for response and progression in ovarian cancer clinical trials incorporating recist 1.1 and ca 125 agreed by the gynecological cancer intergroup ( gcig )  . 
farley j , brady we , vathipadiekal v , et al : selumetinib in women with recurrent low - grade serous carcinoma of the ovary or peritoneum : an open - label , single - arm , phase 2 study . 
gershenson dm , sun cc , wong kk : impact of mutational status on survival in low - grade serous carcinoma of the ovary or peritoneubr j cancer 113 : 1254 - 1258 , 2015 43 . 
castelli c , rivoltini l , rodolfo m , et al : modulation of the myeloid compartment of the immune system by angiogenicand kinase inhibitor - targeted anti - cancer therapies . 
combe p , chauvenet l , lefrre - belda ma , et al : sustained response to vemurafenib in a low grade serous ovarian cancer with a braf v600e mutation . 
bowtell , peter maccallum cancer centre , east melbourne and university of melbourne , parkville , victoria , australia ; and imperial college london , london , england , united kingdom ; g . 
 treatment of patients with lobular breast cancer harboring human epidermal growth factor receptor 2 mutation with her2 - directed therapy introduction human epidermal growth factor receptor 2 ( her2 ) is a tyrosine kinase encoded by the erbb2 gene . 
mutations in cdh1 have been reported in 62% to 100% of cases of invasive lobular carcinoma , and many investigators consider a mutation in cdh1 to represent a genomic alteration characteristic of lobular carcinoma.5 mutations in erbb2 have been reported in six of 22 ( 27% ) cdh1 - mutated lobular carcinomas.5 the presence of activating somatic mutations in erbb2 could provide a rationale for her2 targeted therapy , 4 , 6 and there have now been several case reports of successful treatment of patients with such mutations with her2 targeted therapy.7 - 10 we initially identified a patient with progressive metastatic lobular carcinoma resistant to chemotherapy and hormonal regimens , whose liver metastasis harbored both cdh1 and erbb2 mutations . 
on the basis of the presence of the erbb2 mutation , we elected to treat the patient with her2 - targeted therapy , and she has achieved significant and durable responses to three consecutive her2 - targeted therapies during a 2.5year period of time , despite the lack of erbb2 amplification . after our experience with this patient , we then reviewed all of our patients with metastatic lobular carcinoma of the breast for whom next generation sequencing had been obtained . 
on the basis of reports that erbb2 exon 20 insertion has been shown to confer sensitivity to trastuzumab and tyrosine kinase inhibitors , we elected to treat the patient with dual her2 blockade with the combination of trastuzumab and pertuzumab.2 , 3 treatment was continued for 8 months , with major subjective clinical improvement , which included better appetite and resolution of abdominal pa clinical response was confirmed by ct scan on april 4 , 2016 showing a significant decrease in hepatic lesions , which has been maintained ( fig 2 )  . 
by july 2017 , the carcinoembryonic antigen , ca19 - 9 , and alkaline phosphatase increased aga ado - trastuzumab emtansine was discontinued , and she was started on third - line anti - her2directed therapy with lapatinib and capecitabine in july 2017 . she once again demonstrated significant response in all four tumor markers as well as her liver enzymes ( figs 3 and 4 )  . 
 only one of the five was also her2 amplified and had received prior her2 - directed therapy . all five patients have received her2 - targeted therapy for their metastatic disease , and four have achieved clinical responses as defined by response evaluation criteria in solid tumors ( recist ; tables 1 and 2 )  . 
liver biopsy showing infiltrating cords and nests of tumor cells ( july 2011 )  . in december 2010 , tumor markers were noted to be elevated , and a magnetic resonance imaging scan of the abdomen demonstrated hepatic metastases . 
 subsequent positron emission tomography / computed tomography ( ct ) scan showed progression of her liver lesions , and an ultrasound guided biopsy of the liver in july 2011 confirmed metastatic lobular carcinoma ( fig 1 )  . 
as with the primary tumor , the tumor specimen from liver biopsy was estrogen receptor and progesterone receptor positive and her2 negative by ihc . during the next 2 years she was treated with several chemotherapy regimens , including carboplatin and gemcitabine , capecitabine , and eribul she experienced progression on these regimens after initial responses of approximately 6 months , and progression of liver metastases was seen in august of 2014 . eribulin was then discontinued and she was started on tamoxifen , followed by exemestane and everolimus . 
her disease did not respond to these treatments , and she presented to cancer treatment centers of america at midwestern regional medical center for a second opinion in march of 2015 with extensive hepatic and bone metastases . 
comprehensive metabolic panel : alkaline phosphatase , ast , and alt . has received only two cycles of treatment , and it is too early to evaluate for radiologic response , although her tumor markers have fallen significantly . discussion we have identified erbb2 mutations in five of 16 patients ( 31% ) with cdh1 - mutated metastatic lobular carcinoma , an incidence similar to that previously reported.5 our experience suggests that such patients may well respond favorably to her2 - targeted therapy despite the absence trastuzumab and pertuzumab of her2 amplification . 
if the prevalence of erbb2 mutations is confirmed in larger studies , it would indicate that a significant number of patients with metastatic lobular carcinoma are likely to benefit from her2 - targeted therapy . 
this , together with the fact that one patient ( patient 3 ) had received no systemic treatment before biopsy , suggests that erbb2 mutation may be an intrinsic characteristic of lobular carcinoma of the breast and does not necessarily arise from prior systemic therapy . there is currently considerable interest in the possibility that patients with her2 - mutated breast cancer can be successfully treated with drugs already approved by the us food and drug administration for her2 - amplified disease . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . speakers ' bureau : astrazeneca , pfizer , r - pharm us , agendia bradford a . 
ali employment : foundation medicine leadership : incyte stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health on microbiome in non - neoplastic disease ( i ) ankur r . 
parikh consulting or advisory role : foundation medicine maurie markman employment : cancer treatment centers of america consulting or advisory role : amgen , celgene , crititech , pfizer , myriad genetics , merck , clovis oncology dennis l . 
 expert testimony : actavis , acorn research , apotex , emcure pharmaceuticals , dr reddy 's laboratories , fresenius kabi , hikma pharmaceuticals , hospira , pharma international , sagent pharmaceuticals , strides arcolab , sun pharma , wockhardt jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine references stock and other ownership interests : foundation medicine research funding : foundation medicine arun kadamkulam syriac no relationship to disclose sara j . 
wolff ac , hammond me , hicks dg , et al : recommendations for human epidermal growth factor receptor 2 testing in breast cancer : american society of clinical oncology / college of american pathologists clinical practice guideline update . 
ross js , slodkowska ea , symmans wf , et al : the her - 2 receptor and breast cancer : ten years of targeted anti - her - 2 therapy and personalized medicine . 
ross js , wang k , sheehan ce , et al : relapsed classic e - cadherin ( cdh1 ) - mutated invasive lobular breast cancer shows a high frequency of her2 ( erbb2 ) gene mutations . 
ali sm , alpaugh rk , downing sr , et al : response of an erbb2 - mutated inflammatory breast carcinoma to human epidermal growth factor receptor 2 - targeted therapy . 
chumsri s , weidler j , ali s , et al : prolonged response to trastuzumab in a patient with her2nonamplified breast cancer with elevated her2 dimerization harboring an erbb2 s310f mutation . 
ben - baruch ne , bose r , kavuri sm , et al : her2 - mutated breast cancer responds to treatment with single - agent neratinib , a second - generation her2 / egfr tyrosine kinase inhibitor . 
shih j , bashir b , gustafson ks , et al : cancer signature investigation : erbb2 ( her2 ) - activating mutation and amplification - positive breast carcinoma mimicking lung primary . 
hyman dm , piha - paul sa , rodon j , et al : neratinib in her2 or her3 mutant solid tumors : summit , a global , multi - histology , open - label , phase 2 basket study . 
 loss of g2032r resistance mutation upon chemotherapy treatment enables successful crizotinib rechallenge in a patient with ros1 - rearranged nsclc sebastian michels matthias scheffler svenja wagener dennis plenker andreas scheel lucia nogov anne schultheis rieke n . 
sos reinhard bttner jrgen wolf author affiliations and support information ( if applicable ) appear at the end of this article . licensed under the creative commons attribution 4.0 license correspondence author : jrgen wolf , md , lung cancer group cologne , department i for internal medicine , center for integrated oncology , university hospital of cologne ; kerpener str . 
lacking targeted treatment options at that time , we treated him for approximately 3 months within a clinical phase i trial testing a combination of nintedanib and everolimus , without radiographic response of the disease . while on treatment , an extended molecular profiling was performed of a tumor sample collected 4 years after first diagnosis . 
a break - apart fluorescence in - situ hybridization assay ( zytovision , bremerhaven , germany ) revealed a rearrangement of ros1 in 100% of the tumor cells ( baseline ) .10 massively parallel sequencing ( mps ) and further alk fluorescence in - situ hybridization assays revealed no co - occurring genetic aberration ( fig 2 )  . 
disease progression in january 2015 most notably became apparent by a new ascites ( t1 ) , of which a sample was collected for molecular analyses and for the establishment of a patient - derived tumor model using the conditionally reprogramming of cells ( crc ) protocol established by liu et al.11 , 12 the culture was positive for malignant cells by immunohistochemical analysis , and ros1 fish confirmed the high level of rearrangement in the native ascites as well as the crc model ( fig 2 )  . 
because our mps panel did not cover the ros1 gene , sanger sequencing of ros1 exons 34 to 41 ( exon 38 forward primer sequence : 5 - actccataaagaccctcggc - 3 ; reverse primer sequence : 5 - gttttaccactgcagcctattaa - 3 ) was performed on an eight - capillary 3500 genetic analyzer ( thermo fisher scientific ) and showed a g2032r substitution in exon 38 in the ascites and in the derived cells ( fig 2 ) .7 to assess whether the g2032r mutation was acquired during treatment with crizotinib , we additionally sequenced the pretreatment biopsy specimen , which did not harbor any point mutation in ros1 . 
treatment of the crc with crizotinib and cabozantinib showed a shift of the half maximal growth - inhibitory dose ( gi50 ; cabozantinib , 0.3 m ; crizotinib , 1.2 m ) for crizotinib toward higher concentrations , as compared with cabozantinib in the viability assay ( fig 2d )  . 
 ( a ) table listing the results of the molecular pathological analyses before first crizotinib treatment ( baseline ) , at resistance to first crizotinib treatment ( t1 ) , and at progression to chemotherapy , before the initiation of the second crizotinib treatment ( t2 ) period . 
 ( b ) ros1 mutation status as determined by sanger sequencing of exons 34 to 41 at baseline , t1 , and t2 , revealing the substitution c.6094g > a / p.g2032r. 
 ( c ) magnifications of hematoxylin and eosin ( h&e ) staining , ttf1 and calretinin immunohistochemistry ( ihc ) , and ros1 break - apart fluorescence in situ hybridization ( fish ) of the patients conditionally reprogramming of cells ( crc ) tissue collected at t1 . 
the first 18f - labeled fluorodeoxyglucose positron emission tomographycomputed tomography ( ct ) scan at week 4 of treatment showed a dramatic metabolic and morphologic response with a reduction of the largest dimension of target lesions by 41.2% and a reduction of maximum standardized uptake value of the single hottest lesion by 45.9%. 
another ct scan 4 weeks later confirmed the partial response and , at time of data cutoff for this report ( december 2017 ) , the patient has continued treatment of almost 1 year . discussion this case is a proof of concept that rechallenge with crizotinib after intervening chemotherapy is feasible in ros1 - rearranged nsclc with acquired resistance . 
 it is commonly thought that darwinian selection underlies the emergence of resistant clones during targeted therapy , 4 such as those that carry the ros1 p.g2032r resistance mutation , like in our case . 
a similar phenomenon has been described in vitro in egfr p.t790mpositive cells that grew slower than did cells with sensitizing egfr mutations only.14 otherwise , crizotinib - resistance mutations in alk - rearranged cell - line models seem to induce an increased proliferation rate.15 also , studies proving a higher sensitivity toward chemotherapy of ros1 p.g2032positive cells have not been reported . 
thus , our finding needs to be interpreted with caution , and comprehensive studies are required to explain this observation . apart from the clinical findings , this case also illustrates the feasibility and the viability of crc establishment for individual patients to guide treatment decisions . 
sos , reinhard bttner , jrgen wolf administrative support : sebastian michels , reinhard bttner provision of study material or patients : sebastian michels , matthias scheffler , lucia nogov , wolfgang baus , sabine merkelbach - bruse , reinhard bttner , jrgen wolf collection and assembly of data : sebastian michels , matthias scheffler , svenja wagener , dennis plenker , andreas scheel , lucia nogov , rieke n . 
 abdulla , carsten kobe , wolfgang baus , sabine merkelbachbruse , reinhard bttner , jrgen wolf sensitive to treatment with cabozantinib , which is consistent with the clinical loss of crizotinib efficacy . 
tpx0005 , a next - generation ros1 / alk inhibitor , has promising activity in the presence of these mutations , including g2032r and is in early clinical development.17 our theoretical understanding of the evolutionary dynamics in cancer has impressively improved , and it seems that clonal evolution under therapy follows deterministic and stochastic forces . 
 in particular , in the patient in this case report who has been treated sequentially with targeted and nontargeted therapy , a precise allocation to one of these mechanisms may not be possible . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . sebastian michels honoraria : novartis , pfizer , astrazeneca , boehringer ingelheim , roche pharma consulting or advisory role : boehringer ingelheim , pfizer , roche pharma research funding : pfizer ( inst ) , novartis ( inst ) , bristolmyers squibb ( inst ) travel , accommodations , expenses : novartis matthias scheffler honoraria : healthcare consulting cologne , boehringer ingelheim , takeda consulting or advisory role : boehringer ingelheim , takeda travel , accommodations , expenses : boehringer ingelheim svenja wagener no relationship to disclose dennis plenker stock and other ownership interests : roche , foundation medicine patents , royalties , other intellectual property : a patent of nrg1 fusions has been filed . andreas scheel honoraria : msd , bristol - myers squibb , roche , dako / agilent technologies consulting or advisory role : msd , bristol - myers squibb , roche , dako / agilent technologies lucia nogov honoraria : pfizer , celgene , pfizer , novartis consulting or advisory role : roche , novartis , boehringer ingelheim , bristol - myers squibb research funding : pfizer ( inst ) , bristol - myers squibb ( inst ) , novartis ( inst ) , msd ( inst ) travel , accommodations , expenses : novartis , pfizer , celgene , boehringer ingelheim anne schultheis consulting or advisory role : novartis research funding : roche research funding : bristol - myers squibb ( inst ) , msd ( inst ) diana s.y. 
abdulla honoraria : boehringer ingelheim , roche pharma , bristolmyers squibb , merck consulting or advisory role : boehringer ingelheim , roche pharma , novartis research funding : bristol - myers squibb ( inst ) , pfizer ( inst ) , novartis ( inst ) travel , accommodations , expenses : bristol - myers squibb , roche pharma , boehringer ingelheim , novartis , loxo , merck richard riedel consulting or advisory role : boehringer ingelheim , novartis , eli lilly travel , accommodations , expenses : loxo anne bunck no relationship to disclose carsten kobe no relationship to disclose wolfgang baus travel , accommodations , expenses : novartis ( i ) sabine merkelbach - bruse honoraria : astrazeneca , bristol - myers squibb , novartis consulting or advisory role : bristol - myers squibb , novartis martin l . 
sos research funding : novartis reinhard bttner stock and other ownership interests : cofounder and chief scientific officer for targos molecular pathology ( kassel , germany ) and tamp ( atlanta , ga ) honoraria : astrazeneca , abbvie , bayer , bristol - myers squibb , boehringer ingelheim , merck serono , msd , novartis , qiagen , pfizer , roche research funding : roche ( inst ) jrgen wolf honoraria : abbvie , astrazeneca , bristol - myers squibb , boehringer ingelheim , msd , novartis , roche consulting or advisory role : abbvie , astrazeneca , bristol - myers squibb , boehringer ingelheim , chugai pharma , ignyta , eli lilly , msd oncology , novartis , pfizer , roche research funding : bristol - myers squibb , novartis , pfizer affiliations all authors : university hospital of cologne ; martin l . 
gainor jf , tseng d , yoda s , et al : patterns of metastatic spread and mechanisms of resistance to crizotinib in ros1 - positive nonsmall - cell lung cancer . 
facchinetti f , loriot y , kuo ms , et al : crizotinib - resistant ros1 mutations reveal a predictive kinase inhibitor sensitivity model for ros1and alk - rearranged lung cancers . 
shaw at , felip e , bauer tm , et al : lorlatinib in non - small - cell lung cancer with alk or ros1 rearrangement : an international , multicentre , open - label , single - arm first - in - man phase 1 trial . 
cui jj , zhai d , deng w et al : abstract b185 : tpx - 0005 , a supreme ros1 inhibitor , overcomes crizotinib - resistant ros1 mutations including solvent front mutation g2032r and gatekeeper mutation l2026m . 
 tumor - infiltrating lymphocyte function predicts response to neoadjuvant chemoradiotherapy in locally advanced rectal cancer purpose the presence of tumor - infiltrating lymphocytes ( tils ) in tumors is superior to conventional pathologic staging in predicting patient outcome . 
here we developed an assay that tests til cytotoxicity in patients with locally advanced rectal cancer before definitive treatment , identifying those who will obtain a pathologic complete response ( pcr )  . 
we also used the assay to demonstrate the rescue of til function after checkpoint inhibition blockade ( cib )  . patients and methods thirty - four consecutive patients were identified initially , with successful completion of the assay before surgery in those 17 patients who underwent full treatment . 
cib ( antiprogrammed cell death protein 1 [ antipd - 1 ] antibody ) response was also assessed in a subset of patient specimens . results six of the 17 patients achieved an objective pcr on final evaluation of the resected specimen after neoadjuvant chemoradiotherapy . 
assessment of the effectiveness of cib revealed partial restoration of cytotoxicity in tils with increased pd - 1 expression with antipd - 1 antibody exposure . conclusion evaluating til function can be undertaken within weeks of the diagnostic biopsy , affording the potential to alter patient management decisions and refine selection for a watch - and - wait protocol . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license introduction the patients immune system plays a vital role in tumor eradication.1 this has been demonstrated by gene expression studies of colorectal cancer ( crc ) , identifying tumor - infiltrating lymphocytes ( tils ) , associated cytokines such as interferon gamma ( ifn - ) , and cytolytic granules ( granzyme b ) , correlating with a good prognosis.2 subsequent validation by immunohistochemistry ( ihc ) defined cd8 + ( cytotoxic ) tils to be a superior predictive marker to tnm staging.3 similarly , the immune landscape in rectal cancer before neoadjuvant chemoradiotherapy ( nacrt ) is well characterized , with high densities of cd8 + tils seeming to be an enticing arbiter of good tumor regression grade.4 - 6 although the location of tils correlates with outcome , this is not to an extent whereby management can be confidently altered . 
inclusion criteria were patients with t3 to t4 and / or n1 to n2 rectal cancer who were scheduled for long - course nacrt , had no or solitary hepatic metastasis amenable to surgery , and had subsequent total mesorectal excision surgery with curative intent performed at least 10 to 12 weeks from the last crt dose . 
patients were excluded if they were younger than 18 years of age or if they had received short - course , or failed to complete long - course , crt . 
the study was approved by the peter maccallum cancer centre human research ethics committee , and written consent was obtained from each patient according to national health and medical research council guidelines . clinical assessment each patient was treated by a specialist lower gi cancer multidisciplinary board consisting of a nuclear medicine physician , two radiologists , two medical oncologists , two radiation oncologists , two pathologists , and four colorectal trained surgeons and research scientists . 
radiotherapy took place during a period of 5 weeks , for a total of 45 gy in 25 fractions to the pelvis , followed by a 5.4 gy boost in three fractions . histology was examined by two gi oncology specialist - pathologists . 
 if no tumor was identified macroscopically , the whole tumor bed was examined . pretreatment immune cytotoxicity measurement collection of biopsy specimens to derive tumoroids and tils was performed by one of the five scientists , after 3 months of training . 
experimental assessors were blinded to clinical outcomes . tumoroid and til expansion tumoroids are an established in vitro model.20 , 27 fresh tumor biopsy specimens were collected at the time of endoscopy , with a proportion of the specimens processed into tumoroids.27 their origin was confirmed by short tandem repeat analysis by the australian genomics research foundation , melbourne , and by staining for cdx2 and ck20 ( data supplement )  . 
 a portion of the endoscopic biopsy specimen was used for the expansion of tils , using a modified protocol.28 tils were analyzed for t - cell subsets ( cd3 + , cd4 + , cd8 + , foxp3 + , and cd56 + cells ) using a fluorescence - activated cell sorting ( facs ) platform ( bd lsrfortessa x - 20 , north ryde , australia ) at days 0 and 14 ( data supplement )  . multiplex ihc , imaging , spectral unmixing , and phenotyping multiplex ihc staining was performed using the perkinelmer opal 6 - color kit ( perkinelmer , waltham , ma ) as per manufacturers instructions . 
representative images , detailed methodology , and a list of antibodies can be found in the data supplement . immune cytotoxicity assay analysis a comprehensive protocol is reported in the data supplement . 
briefly , tumoroids were expanded over two passages and were plated onto an ibidi 96 - well microscopy - grade plate in their third passage and allowed to grow for 5 to 10 days to a size of > 50 each well contained 10 to 500 tumoroids with the appropriate media included during their coculture with matched tils . 
two fluorescent dyes were added to the wells : an apoptotic marker ( thermo fisher , scoresby , australia cellevent caspase - 3 / 7 - green readyprobes reagent ) and a cell death marker ( themo fisher propidium iodide [ pi ] ) activated by nucleic acid binding . 
 tumoroids death was quantified by measuring the mean fluorescence intensity ( mfi ) of pi only , given the stability of the dye . four wells , consisting of two negative controls with tumoroids alone and two test wells , cocultured with matched tils , were used for each experiment . 
tumoroids at the matrigel periphery ( < 100 m from the edge ) were viewed at random , with at least 10 tumoroids imaged every 2 hours for 48 hours . 
the images were then analyzed by measuring the maximum mfi for each tumoroid ( overall fluorescence intensity emitted / surface area of tumoroid ) to obtain a mean for the 10 + tumoroids . 
morphologic killing was examined by scanning electron microscopy ( scem ; jcm - 6000 , jeol , frenchs forest , australia ; at 15 kv under high vacuum )  . 
cultivation of tils in tumoroid media had no effect on the viability or the capacity to respond to activation stimuli ( data supplement )  . results study participants thirty - four consecutive patients consented , with completion of the cytotoxic assay before surgery in 17 . 
after additional optimization , we eliminated in vitro culture infection and , with sufficient tumor tissue , achieved a culture success rate of 87% ( 19 of 22 patients )  . 
an additional four had disease progression and thus were not amenable to surgery , two patients had immediate surgery , and one patient was excluded because of poor tolerance to nacrt and proceeded to surgery . 
the mean number of sections examined for patients with pcr was 6.8 , and the mean number of lymph nodes inspected was 19.5 ( table 1 )  . functional immune cytotoxicity assay we compared tumor sections and matched embedded tumoroids by costaining with cdx2 and ck20 antibodies ( fig 1a )  . 
to show that tils were capable of interaction with tumoroids , we used scem to visualize the morphologic integrity of the tumoroids with and without their matched tils ( fig 1c )  . 
patient - specific tils of those who eventually achieved a pcr , initiated tumor cell killing ( apoptosis by activated caspase3 / 7green fluorescence [ data supplement ] ) and subsequent tumoroid death ( pi red fluorescence ) as shown in figs 1d - 1f . 
in those patients who did not respond to nacrt , their tils did not induce substantive tumoroid death , whereas some tumoroids are intrinsically resistant to immune attack and / or the tils lack cytotoxic activity ( figs 1g - 1i ; data supplement )  . implicit to the concept of til - mediated cytotoxicity is that by increasing the ratio of effector cells to target cells , it would be expected that the kinetics of til killing would accelerate . 
by monitoring the pi fluorescence of 10 to 30 tumoroids over time , it was apparent that there was a range of til - induced tumoroid deaths across patient samples ( fig 2b )  . prospective patient cohort and matched primary and metastasis assays the prospective recruitment of patients with rectal cancer afforded an opportunity to explore the predictive power of our assay without modifying the patient treatment course . 
when the results are presented as a box plot of for maximum killing ( fig 3c ) , an unambiguous difference ( p < .001 ) between pcr and incomplete response at 48 hours is evident ( mean pcr mfi of 27 , 982 [ 95% ci , 25 , 340 to 30 , 625 ] compared with 12 , 428 [ 95% ci , 9 , 434 to 15 , 423 ] ) for incomplete response . 
 we also evaluated the percentage of tumoroids killed by exposure to tils in the pcr group ( mean sem , 85% 5% ) versus incomplete response ( 32% 7% ) on the basis of morphologic disruption ( bright field microscopy ) as well as pi uptake ( fluorescence microscopy ) , finding a highly significant difference by this measure ( p < .0001 , two - tailed t test )  . 
 in parallel , we showed that the primary tumor tils kill primary tumorderived tumoroids , whereas the liver tumoroids are not killed readily by their matched tils ( data supplement )  . 
 in one patient , we propagated sufficient tils to add primary tils to metastasis tumoroids to find that these have a slightly greater capacity to kill than do metastasis tils . 
on antipd - 1 antibody treatment , the increase in cytokine production tracks with improved cytotoxicity of the increased pd - 1expressing tils in one patient ( figs 5d , 5g ) partial improvement in another ( figs 5e , 5h ) , and no improvement in a third ( figs 5f , 5i )  . 
facs separation of til subsets cd8 + , cd4 + , cd56 + / cd8 ( natural killer cells ) , and cd8 + / cd56 + ( natural killer t ) was performed to distinguish the cytotoxic effect of each in the assay ( data supplement )  . 
visualization of the killing capacity of cd8 + / cd56 tils compared with the other subpopulations is documented in fig 4d , whereas production of ifnor tumor necrosis factor ( tnf - ) did not discriminate between groups ( data supplement )  . data from this prospective study advance the concept that it is possible to assess til cytotoxicity and that measuring the function of patient specific tils accurately predicts pcr in patients with locally advanced rectal cancer undegoing nacrt . 
this study has demonstrated the functional characterization of individual patient - specific tils against matched primary or metastatic tumor cells . our study ensured that all eligible patients received standardized treatment without variation , including an interval time to surgery of at least 10 weeks ( from the last radiation dose )  . 
 ( b ) tumoroids ( approximately 500 cells ) embedded in matrigel are readily generated ex vivo from surgical biopsy specimens and can be combined with patient - matched tils to allow measurement of patient - specific cytotoxicity . 
the addition of tils ( rendered pink on the basis of characteristic cell size ; pink arrows ) to patient - matched tumoroids leads to morphologic irregularities on the tumoroid surface and progressive structural disruption ( images at 8 hours )  . 
 ( d ) tumoroids ( black arrow ) at time 0 show no uptake of propidium iodide ( pi ) as indicated by red fluorescence , or activation of caspase - 3 / 7 ( apoptosis ) as indicated by green fluorescence in the absence of tils . 
 ( gi ) not all tumoroids ( white arrow ) are subject to til - mediated killing , as demonstrated in this series of images , suggesting that intrinsic resistance to immune - mediated killing is a characteristic in some patients with rectal cancer . 
 assessment was performed by two independent , blinded pathologists across the entire irradiated tumor bed to ensure reporting consistency . the usefulness of tumoroid models lies in their resemblance to the original tumor in terms of tissue architecture , mutations , and heterogeneity.30 the restoration of tils in this model activated caspase 3 / 7 target : effector ratios 12 h 20 h 48 h 12 h 20 h 12 h killing 1 : 10 1 : 10 30 , 000 25 , 000 20 , 000 15 , 000 10 , 000 5 , 000 8 12 16 20 24 28 32 36 40 44 48 time ( hours ) fig 2 . 
 ( a ) target effector ratios of tumoroid cells ( stained blue with hoechst 33258 ) to matched tils measured by activated caspase 3 / 7 fluorescence ( green ) demonstrates that til - mediated killing is effector cell density dependent . 
 ( b ) cytotoxic assays measured in six patient samples by propidium iodide uptake ( mean fluorescence intensity [ mfi ] ) in rectal tumoroids and patient - matched tils at a 1 : 10 ratio demonstrate patient - to - patient heterogeneity in terms of kinetics and extent of killing of tumoroids ( mfi of 30 to 100 tumoroids / patient tracked over time ; six patient samples ; means depicted )  . partially recapitulates the tumor microenvironment . 
of greatest importance , the rapid establishment of tumoroids and tils within a clinically relevant timeline ( 3 to 4 weeks of patient biopsy ) lends this assay to multiple applications . phenotypic characterization of tils identified cd8 + tils as a key arbiter of good tumor regression grade.4 - 6 , 31 - 34 however , quantification of tils is limited by an inability to predict response accurately and thereby allows treatment decisions to be altered.5 , 6 our study advances the phenotypic characterization to include functional evaluations , reaffirming that cd8 + tils are the predominant t cells responsible for cytotoxicity . 
importantly , the assay uses the same ratio of tils to target cells across samples , further emphasizing that til density alone does not predict response , rather , their functional quality . to determine whether tils have the ability to migrate toward and interact with patientmatched tumoroids , we performed scem of mixed cultures of matched tils and tumoroids . 
by staining tils with nucleic acid binding fluor - syto11 , we tracked the migration of patient - matched peripheral blood mononuclear cells through matrigel ( data supplement ) and identified tumoroids that are intrinsically resistant to immune attack ( data supplement )  . 
 ( b ) by measuring the cytotoxicity of tils against matched tumoroids ( that contain approximately 500 cells ) over a 48 - hour period with an effector - to - target ratio of 10 : 1 , distinct killing profiles were ascertained . 
 ( d ) pretreatment biopsy tissue blocks were processed for immune makers by multiplex immunohistochemistry ( ihc ) and digitally evaluated for immune cells subsets within the tumor and the treg / cd8 + cell ratio ( e ) for the cohort of patients achieving a pcr ( four ) and incomplete responses ( six ) whereby no significant differences were observed . 
 the addition of antipd - 1 antibody into this setting partially rescued killing activity for two of three patient samples , despite increases in ifn and tnfrelease in all three . 
this uncoupling has been reported by others , who showed that there can be target engagement by cytotoxic t cells but failure to kill , which in turn leads to chronic cytokine production.41 interestingly , despite having a greater proportion of cd8 + tils , our crossover study in one patient with synchronous primary and metastatic liver tumors showed a decreased killing efficacy of met - tils compared with primary tils . 
however , met - cd8 + tils also displayed a higher proportion of pd - 1expressing cells and showed the same , but no greater , killing efficacy as primary tils on addition of antipd - 1 antibody . 
 ( ac ) tils were fluorescence - activated cell sortingenriched to generate different subsets ( cd4 + / cd56 , cd8 + / cd56 , cd8 / cd56 + , and cd8 + / cd56 + ) to identify the cell types responsible for the killing of patient - matched rectal tumoroids . 
mfi , mean fluorescence intensity . including receptor and ligand expression by ihc , have had low yield in predicting response to immunotherapy.26 in conclusion , others have recently explored the usefulness of examining patient - derived organotypic tumor spheroids or tumor organoidlike cultures in combination with other microenvironment components in the setting of cib treatments , 42 as well as peripheral blood - derived cells from the same patient.43 the relative merits of our assay platform are tabulated in the data supplement . 
it is instructive that this assay is performed before the effects of the tumor cell damage induced by nacrt are presented to the immune milieu and that measuring de novo immune competency appears to predict response to treatment . 
 ( ac ) pd - 1 ( programmed cell death protein 1 ) expression of cultured tils is induced after 2 days of exposure to anti - cd3 / cd28 dynabeads ( blue bar ) compared with unstimulated ( gray bar ) ; shown for three patient samples . 
mfi , mean fluorescence intensity . thus , in some patients , the immune microenvironment is poised to take advantage of the effects of nacrt to achieve a pcr , and this implies , but does not prove , that the quality of the tils affects the multiple actions of nacrt ; these are issues for future evaluation . 
this pretreatment biomarker has the potential to influence the management of patients with rectal cancer by improving the accuracy of patient selection for a watch - and - wait protocol . 
 alexander graham heriot no relationship to disclose robert george ramsay honoraria : merck serono research funding : merck serono , targovax , fisher and paykel travel , accommodations , expenses : fisher and paykel acknowledgment we thank rebecca abbot for her assistance in tissue culture , pasquale petrone and heloise halse for their assistance in multiplex immunohistochemistry data acquisition and initial til analysis respectively , and chad johnson , jill dane , and sarah ellis for their guidance and assistance in the usage of high - resolution fluorescence microscopy instruments . affiliations joseph cherng huei kong , glen robert guerra , rosemary magdalena millen , sara roth , huiling xu , paul joseph neeson , phillip kevin darcy , michael henry kershaw , shienny sampurno , jordane malaterre , david shi hao liu , toan duc pham , vignesh narasimhan , minyu wang , yu - kuan huang , jacob mccormick , andrew craig lynch , satish warrier , michael michael , jayesh desai , william murray , catherine mitchell , samuel ngan , wayne allen phillips , alexander graham heriot , and robert george ramsay , peter maccallum cancer centre , university of melbourne , melbourne ; and kumar visvanathan and rosemary magdalena millen , st vincents hospital , east melbourne , australia . supported by the colorectal surgical society of australia , the new zealand foundation , the royal australasian college of surgeons foundation for surgery , the national health and medical research council of australia , and the victorian cancer agency . presented in part at the american society for clinical oncology annual meeting , chicago , il , june 2 - 6 , 2017 . support prior presentation references 1 . 
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dalton rs , velineni r , osborne me , et al : a single - centre experience of chemoradiotherapy for rectal cancer : is there potential for nonoperative management ? colorectal dis 14 : 567 - 571 , 2012 39 . 
maas m , lambregts dm , nelemans pj , et al : assessment of clinical complete response after chemoradiation for rectal cancer with digital rectal examination , endoscopy , and mri : selection for organ - saving treatment . 
perez ro , habr - gama a , gama - rodrigues j , et al : accuracy of positron emission tomography / computed tomography and clinical assessment in the detection of complete rectal tumor regression after neoadjuvant chemoradiation : long - term results of a prospective trial ( national clinical trial 00254683 )  . 
jenkins mr , rudd - schmidt ja , lopez ja , et al : failed ctl / nk cell killing and cytokine hypersecretion are directly linked through prolonged synapse time . 
tsai s , mcolash l , palen k , et al : development of primary human pancreatic cancer organoids , matched stromal and immune cells and 3d tumor microenvironment models . 
 drug - related pneumonitis in the era of precision cancer therapy drug - related pneumonitis as a result of novel cancer therapy provides new challenges for providers of cancer care in the era of precision medicine . 
here , we provide a detailed review of drug - related pneumonitis that develops during precision cancer therapies using immune - checkpoint inhibitors and molecular targeting agents , and we summarize the emerging data that have been obtained by recent investigations to provide a state - of - the - art overview for clinicians involved in cancer care . we focus on immune - checkpoint inhibitorrelated pneumonitis , which is an immune - related adverse event of growing interest and increasing clinical significance in current oncology practice that has rapidly expanding access to these agents . 
clinical characteristics , radiographic spectrum , and risk factors and outcome of pneumonitis are described for each class of agents , and current treatment guidelines and monitoring recommendations are discussed . 
with recent advances in precision cancer therapy using molecular targeting agents and immune - checkpoint inhibitors ( icis ) , pneumonitis in patients who are treated with novel anticancer agents is increasingly recognized as a significant clinical challenge . 
in addition , rapidly expanding access to icis , such as programmed death 1 ( pd - 1 ) and programmed death - ligand 1 ( pd - l1 ) inhibitors has brought new and emerging challenges . 
recent studies of pneumonitis in patients who are treated with these novel agents have provided important new knowledge and insight that are relevant to cancer care providers across disciplines . this review focuses on drug - related pneumonitis during precision cancer therapies , including icis and molecular targeting agents , and provides an overview for clinicians who are involved in the care of patients with cancer . 
the spectrum of radiographic manifestations of pneumonitis is presented in the context of patient management . we also provide up - to - date guidelines and recommendations for the treatment and monitoring of pneumonitis during these therapies . 
 been made to characterize the radiographic patterns of pneumonitis caused by various therapeutic agents.1 , 2 several recent reports have indicated that the radiographic patterns of drug - related pneumonitis may be categorized according to patterns that correspond to american thoracic society / european respiratory society ( ats / ers ) classifications of idiopathic interstitial pneumonias and related disorders , 3 which are based on ct findings and their extent and distributions on imaging.2 , 4 - 8 in these studies of pneumonitis that developed during treatment with molecular targeting agents and icis , the commonly noted radiographic patterns of pneumonitis included cryptogenic organizing pneumonia ( cop ) pattern , nonspecific interstitial pneumonia ( nsip ) pattern , hypersensitivity pneumonitis ( hp ) pattern , and acute interstitial pneumonia ( aip ) / acute respiratory distress syndrome ( ards ) pattern2 , 4 - 10 ( table 1 )  . 
radiographic patterns of pneumonitis have been shown to correlate with the toxicity grades assessed by the common terminology criteria for adverse events.5 recent advances in precision cancer therapy have brought the new and emerging challenges of pneumonitis as a result of treatment with novel agents . 
regulatory approvals for these agents have recently been granted , including nivolumab for melanoma , nonsmall - cell lung cancer ( nsclc ) , renal cell carcinoma ( rcc ) , and hodgkin lymphoma ; pembrolizumab for melanoma , nsclc , hodgkin lymphoma , and squamous cell head and neck cancer ; and atezolizumab for urothelial carcinoma and nsclc . 
combination therapy of nivolumab and ipilimumab , a cytotoxic t - lymphocyte - associated protein 4 inhibitor , has also been approved for treatment of advanced melanoma and is actively investigated in nsclc and other malignancies . as a result , these agents are rapidly expanding their treatment roles in clinical oncology practice , and more agents are in the drug development and testing pipeline . immune - checkpoint inhibition of these agents is associated with a unique set of toxicities that are known as immune - related adverseevents ( iraes ) .11 - 14 among a variety of iraes that can affect organs from head to toe , ici - related pneumonitis is a clinically significant and potentially life - threatening irae and is therefore recognized as an event of special interest . phase i trials of pd - 1 inhibitors have resulted in pneumonitis - related deaths in patients with advanced solid tumors , including nsclc , melanoma , and colorectal cancer.15 - 18 in a report of long - term safety in a nsclc cohort that was treated in a phase i trial , pneumonitis occurred in 7% ( 9 of 129 patients ) , with three pneumonitisrelated deaths.15 in a phase ii trial of nivolumab in squamous nsclc , pneumonitis was one of the most common iraes , occurring in 5% of patients ( 6 of 117 patients ) , including four patients with grade 3 pneumonitis.19 more recent data suggest that pneumonitis can be an even more significant issue in patients who are treated with combination therapies . 
radiographic pattern was associated with clinical severity of pneumonitis represented by toxicity grades , where aip / ards pattern had the highest grade , followed by cop pattern , whereas nsip pattern and hp pattern had lower grade ( median grade : 3 , 2 , 1 , 1 ) .5 results indicate that the radiographic patternbased approach , in addition to early and accurate diagnosis , may help guide patient management and follow - up in the setting of pneumonitis . 
another recent study of pd - 1 / pd - l1 inhibitor - related pneumonitis has also reported the diverse radiographic and pathologic features of the entity , 25 further indicating the importance of a standardized common language to describe the findings of ici - related pneumonitis.10 treatment , clinical course , and management guidelines treatment of ici - related pneumonitis consists mainly of holding back on the use icis and administering corticosteroids ; however , some cases may be refractory to corticosteroids and require additional treatment . 
 ( d ) aip / ards pattern is characterized by diffuse or multifocal ggos or consolidations , along with lung volume loss and traction bronchiectasis . ( n = 12 ) or as intravenous therapy ( n = 5 )  . 
although the cause of death was solely attributed to pneumonitis in one patient alone , the serious outcome in 12% ( 5 of 43 ) of patients again emphasizes the clinical significance of the entity.25 twelve patients were retreated with icis after complete clinical resolution of initial pneumonitis , and three patients experienced recurrent pneumonitis , which again resolved by drug holding ( n = 1 ) or oral corticosteroids ( n = 2 ) as in the course of their initial pneumonitis treatment.25 a recently published guideline of pneumonitis management is in agreement with the observations in these reports.31 the guideline recommends oral corticosteroid treatment , including prednisone 1 to 2 mg / kg / d or methylprednisolone 0.5 to 1 mg / kg / d in mild to moderate cases . 
in mild to moderate cases , bronchoscopy is recommended to exclude infectious etiologies before starting immunosuppression.31 in severe cases , hospitalization is necessary , with treatment to include high - dose corticosteroids , such as methylprednisolone 2 to 4 mg / kg / d , and additional immunosuppression , including mycophenolate mofetil , cyclophosphamide ; infliximab can be administered if necessary.31 although limited to a small percentage of patients , an additional unique phenomenon of pneumonitis flare has been reported where ici - related pneumonitis recurs after the termination of corticosteroid taper and in the absence of ici retreatment after the initial episode of pneumonitis has been successfully treated ( fig 2 )  . 
this was first reported in a patient with nsclc who was treated with commercial nivolumab and who experienced pneumonitis.6 the patient was successfully treated with corticosteroids for the initial pneumonitis ; however , the patient experienced another episode of pneumonitis after completing corticosteroid taper without resuming pd - 1 inhibitor therapy or starting any other therapy , indicating a pneumonitis flare.6 although similar to the initial presentation both clinically and radiographically , flare pneumonitis tends to be more severe and extensive than the initial episode . 
such a phenomenon has not been described in the setting of pneumonitis related to other anticancer agents and this that indicates the clinical course of icirelated pneumonitis may be more complex than other drug - related pneumonitis in some patients . in a series of 20 patients with ici - related pneumonitis , one patient with lymphoma experienced two episodes of pneumonitis flare in which pneumonitis came back with similar but more extensive radiographic presentations compared with the initial episode after completion of corticosteroid taper without pd - 1 retreatment5 ( fig 2 )  . 
this observation further confirms the phenomenon , which is likely unique to iraes and may involve autoimmune mechanisms . unmet clinical needs that require additional investigations although several recent reports provide important knowledge and observations of ici - related pneumonitis , significant knowledge gaps still exist for this emerging entity . 
because early and accurate diagnosis is key for this mostly treatable conditionwith good response to corticosteroids in the majority of the casesadditional studies are needed to identify risk factors and early markers for pneumonitis to improve diagnostic accuracy . treatment and clinical management guidelines need to be further optimized as the immuneoncology community accumulates the experience of this entity . 
pneumonitis with a cryptogenic organizing pneumonia ( cop ) pattern in a 33 - year - old female with hodgkin lymphoma who was treated with nivolumab and ipilimumab combination therapy , with a recurrence during retreatment ( 2a ; ah ) and two episodes of pneumonitis flare after completion of corticosteroid taper ( 2b ; ah )  . 
reprinted with permission from nishino et al.5 2a : ( a and b ) computed tomography ( ct ) scan of the chest at 1.4 months of therapy demonstrated ground - glass and reticular opacities and consolidations with multifocal distribution , which are indicative of a cop pattern of pneumonitis ( arrowheads )  . 
 ( 2b : a and b ) the patient completed 2 months of corticosteroid taper , and after 1 month , experienced another episode of pneumonitis with a similar radiographic pattern , without nivolumab retreatment or other systemic therapy , which indicated a pneumonitis flare . 
 ( 2b : e and f ) the 2.7 - month course of corticosteroid taper was completed , and after 2 weeks , the patient again developed a pneumonitis flare with a similar radiographic pattern as prior episodes . 
findings included lymphocyte - predominant interstitial pneumonitis ( arrowhead , 2b [ g ] , hematoxylin and eosin stain , 3200 ) with rare eosinophils ( arrow , 2b [ g ] ) , and areas of organizing pneumonia with fibroblast plugs and foamy macrophages filling the airspaces ( asterisks , 2b [ h ] , hematoxylin and eosin stain , 3200 )  . 
the patient started another course of prednisone taper with subsequent clinical improvement and is schedule for a follow - up ct scan . in addition , awareness of pneumonitis related to icis other than pd - 1 / pd - l1 inhibitors is becoming increasingly important . 
everolimus is approved for the treatment of several cancers , including advanced rcc , advanced pancreatic neuroendocrine tumors ( nets ) , subependymal giant cell astrocytomas , and advanced hormone receptorpositive , human epireceptor 2negative dermal growth factor breast cancer ( in combination with exemestane )  . 
temsirolimus is approved for the treatment of advanced rcc . drug - related pneumonitis is a recognized class effect toxicity of mtor inhibitors and has been described in detail in the context of advanced rcc treatment . 
in a study by maroto et al , 34 among 178 patients with rcc who were treated with singleagent temsirolimus , 52 ( 29% ) had radiographically identified drug - related pneumonitis . 
of these , 16 patients ( 31% ) had respiratory symptoms at the time of the onset of radiographically detected pneumonitis , whereas others ( 36 of 52 ; 69% ) were asymptomatic and thus may not be clinically diagnosed for pneumonitis . 
the estimated cumulative probability of radiologically identified drug - related pneumonitis was 21% ( 95% ci , 15% to 29% ) at 8 weeks , 31% ( 95% ci , 24% to 40% ) at 16 weeks , and 45% ( 95% ci , 36% to 57% ) at 13 months.34 another study of 46 patients with rcc who were treated with temsirolimus or everolimus reported that 14 patients ( 30% ) developed drug - related pneumonitis.35 median time of the onset of radiologic manifestations of pneumonitis was 56 days ( range , 31 to 214 days )  . 
these 14 patients more frequently achieved stable disease than did others , which indicates a possibility of pneumonitis as a treatment benefit marker.35 reports of mtor inhibitorrelated pneumonitis in tumors other than rcc indicate a somewhat different incidence of pneumonitis according to tumor types . 
radiographic patterns of mtor inhibitorrelated pneumonitis have been characterized in patients with wm and in those with advanced net.7 , 8 in both cohorts , the most common findings were bilateral ground - glass opacities ( ggos ) and reticular opacities , sometimes with consolidations , in a peripheral and lower distribution . 
cop pattern was the leading pattern observed in the majority of cases ( 70% in wm and 57% in net ) , followed by nsip pattern ( 30% in wm and 36% in net ) , whereas one patient in the net cohort demonstrated the hp pattern.7 , 8 similar imaging manifestations are noted in other cohorts with mtor inhibitor related pneumonitis.34 , 35 recognition of the characteristic radiographic patterns of pneumonitis during mtor inhibitor therapy helps with the early detection and accurate diagnosis of this entity . clinical management of mtor inhibitorrelated pneumonitis mostly depends on the severity of clinical symptoms . 
egfr - tki therapy should be discontinued , and systemic corticosteroids are usually administered.49 although egfr - tkirelated pneumonitis has mostly been a specific concern among the japanese population and has often had a low clinical impact in other populations , a recent observation from a trial of a novel ici and third - generation egfr - tki , osimertinib , raises a new concern in the setting of combination therapy . 
 agents may limit , in part , the destructive remodeling of the lung and impair the lungs ability to respond to injury.37 , 49 , 52 these possible mechanisms are also likely modified by various host and environmental factors , which further complicates the issue.52 likewise , risk factors for pneumonitis need to be defined , especially for ici - related pneumonitis , to allow for optimal patient selection with regard to treatment safety . 
the risk of recurrent pneumonitis after reintroduction of therapy is another important debate for these agents , as they may be the only available or effective therapy for patients with advanced cancers.5 , 37 the impact of radiotherapy on pneumonitis is a major topic , given a number of ongoing combination therapy trials that use ici and radiotherapy.53 in some studies of patients with advanced nsclc who were treated with egfr - tkis , prior thoracic irradiation and concomitant radiotherapy have been noted as risk factors for pneumonitis.49 , 54 although the exact effect of radiotherapy on ici - related pneumonitis awaits additional data , prior chest radiation has influenced the radiographic appearance of pd - 1 pneumonitis in patients with lymphoma , which indicates a need for caution in treatment monitoring.30 prior reports have often focused on radiation to the chest ; however , radiotherapy in the extrathoracic sites may require more attention given the concept of abscopal effects , which are increasingly discussed in the context of ici and radiation treatment.53 in the clinical setting , drug - related pneumonitis is ultimately a diagnosis of clinical correlation and exclusion , and there is no specific test for the entity.55 among various lung conditions that can affect patients with advanced cancer who undergo systemic therapy , infection is an important differential diagnosis that should be excluded before starting corticosteroid therapy . 
fiberoptic bronchoscopy is helpful for this purpose as it allows for targeted and deep sampling of specimens for microbiology , cytology , and histology via bronchoalveolar lavage and transbronchial biopsy.55 a minority of patients may present with respiratory distress in the absence of radiographic confirmation , thereby leading to delays in appropriate management . 
of note , some of the findings of pneumonitis , such as ggos , are not adequately evaluated on chest radiographs , and thus diagnostic chest ct scans are needed to sensitively detect and fully characterize the lung abnormalities in the setting of suspected pneumonitis . in conclusion , knowledge of drug - related pneumonitis has increasingly emerged in recent investigations , providing important clues for accurate diagnosis , patient management , and monitoring . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . mizuki nishino honoraria : bayer yakuhin consulting or advisory role : bristol - myers squibb , worldcare clinical , toshiba medical systems research funding : merck ( inst ) drug - related pneumonitis in the era of precision cancer therapy the following represents disclosure information provided by authors of this manuscript . 
stephen hodi employment : dana - farber cancer institute consulting or advisory role : merck sharp & dohme , novartis , genentech , amgen , emd serono research funding : bristol - myers squibb ( inst ) , merck sharp & dohme ( inst ) , genentech ( inst ) , novartis ( inst ) patents , royalties , other intellectual property : patent pending as per institutional policy , patent pending royalties received on mica - related disorders application to institution per institutional policy travel , accommodations , expenses : novartis , bristol - myers squibb other relationship : bristol - myers squibb , genentech nikhil h . 
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ghobrial im , gertz m , laplant b , et al : phase ii trial of the oral mammalian target of rapamycin inhibitor everolimus in relapsed or refractory waldenstr om macroglobulinemia . 
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min jh , lee hy , lim h , et al : drug - induced interstitial lung disease in tyrosine kinase inhibitor therapy for nonsmall cell lung cancer : a review on current insight . 
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 o inference of germline mutational status and evaluation of loss of heterozygosity in high - depth , tumor - only sequencing data purpose inherited germline defects are implicated in up to 10% of human tumors , with particularly well - known roles in breast and ovarian cancers that harbor brca1 / 2 mutated genes . 
however , because of the frequent lack of patient matched control normal dna and / or low tumor purity , there is limited ability to determine the genomic status of these alterations ( germline v somatic ) and to assess the presence of loss of heterozygosity ( loh )  . 
these analyses , especially when applied to genes such as brca1 / 2 , can have significant clinical implications for patient care . materials and methods lohgic ( loh - germline inference calculator ) is a statistical model selection method to determine somatic versus germline status and predict loh for mutations identified via clinical grade , high - depth , hybrid capture , tumor - only sequencing . 
lohgic incorporates statistical uncertainties inherent to high - throughput sequencing as well as specimen biases in tumor purity estimates , which we used to assess brca1 / 2 mutations in 1 , 636 specimens sequenced at rutgers cancer institute of new jersey . results evaluation of lohgic with available germline sequencing from brca1 / 2 testing demonstrates 93% accuracy , 100% precision , and 96% recall . 
2018 by american society of clinical oncology introduction inherited germline genomic alterations contribute to the pathogenesis of 5% to 10% of cancers.1 , 2 hereditary breast and ovarian cancer ( hboc ) is one of the most common familial cancer syndromes , with a prevalence of one in 400 to 500 people in the general population2 and a higher ocurrence in specific ethnic and racial groups.3 women harboring germline mutations in the brca1 and brca2 genes have a significantly increased lifetime risk of developing hboc.4 , 5 mutations in these genes increase the risk of other cancers , including fallopian tube and peritoneal cancers in women , 6 prostate and breast cancers in men , 7 , 8 and pancreatic cancer in both sexes9 ; they are also associated with subtypes of fanconi anemia.10 , 11 brca1 and brca2 are tumor - suppressor genes that encode two proteins involved in homologous recombination ( hr ) mediated dna repair . 
tumors that arise in patients with germline brca1 / 2 mutations often lose the wildtype allele through additional somatic mutations or copy number changes that result in loss of hossein khiabanian kim m . 
us food and drug administration approval of olaparib is only for germline brca1 / 2 mutations , because response to both chemotherapy and targeted therapy is affected by their presence.16 second is continued cancer risk . 
relatives of patients with germline brca1 / 2 mutations may benefit from genetic testing to assess risk.17 for patients with cancer who may possess inherited brca1 / 2 alterations , the standard approach to investigate mutational status has been sequenc ing normal tissue , such as peripheral blood lymphocytes or buccal swabs.18 , 19 with the availability of high - quality assays , tumoronly sequencing is being performed on more patients , 20 , 21 and pathogenic mutations in genes associated with hereditary cancer syndromes , such as brca1 / 2 , can be unexpectedly detected.22 the identification of brca1 / 2 variants in tumor - only data raises two important questions . 
 is the variant acquired somatically in the tumor , or is it in the germline ? and is loh affecting brca1 / 2 loci , suggesting a role for targeted therapy ? the latter question , specifically , cannot be answered by routine germline testing . 
 for example , if a male patient with a known pathogenic germline brca2 mutation develops a tumor not typically associated with the brca2 tumor syndrome ( eg , lung cancer ) , standard approaches cannot determine whether the cancer cells have undergone loh at the brca2 locus and thus may be susceptible to treatment with parp inhibitors . 
similarly , in the setting of a somatic pathogenic brca1 / 2 mutation , determining the loh status can resolve whether the alteration is a heterozygous passenger mutation or whether it has led to a true loss of brca1 / 2 function and , hence , susceptibility to parp inhibitors . 
because loh is the most common mechanism for biallelic inactivation , 23 , 24 its identification in a tumor may also help classify variants of unknown significance . analysis of variant allele frequencies ( vafs ) coupled with robust estimates of copy number changes and tumor purity can be used to infer loh status . 
in this study , we address this problem and introduce lohgic ( loh - germline inference calculator ) to assess germline versus somatic status of mutations and predict presence of loh in tumor - only deep - sequencing data . 
all classes of genomic alterations , including substitutions , small indels , rearrangements , and copy number changes , were determined for each sample , as previously described.26 each tumor sample was analyzed alongside a process - matched normal control ( an internally validated mixture of 10 heterozygous diploid hapmap samples ) , which allowed normalizing sequence coverage distribution across baited targets.26 purity and base ploidy were derived using empirical bayesian sampling methodologies . 
 ( a ) a tumor specimen consists of both cancer cells ( brown ) , normal stromal cells ( gray ) , and possibly normal lymphocytes ( light red )  . 
observed variant allele frequency ( vaf ) of a mutation in hybrid capture dna sequencing depends on various factors including depth of sequencing and chromosomal copy number ( cn ; ploidy ) at its locus , as well as specimen purity ( see materials and methods )  . 
 the brca1 / 2 mutations were classified as candidate pathogenic when they were reported in clinvar or other brca1 / 2 mutation classification databases , 29 , 30 were listed as verified mutations in the catalogue of somatic mutations in cancer database , 31 or were truncating indels or nonsense substitutions in functional protein domains of the genes . lohgics mutational status modeling assuming tumor purity of p and a mutations chromosomal copy number of two in normal cells and ploidy of y in tumor cells , the expected vaf for a somatic variant is given by vaf = c mut p _____________ 2 ( 1 p ) + y p , where c mut is the variant alleles unknown copy number . 
akaike information criterion ( aic ) can then be used to compare these likelihoods.32 because there is one fitted parameter in a binomial distribution , aic ( f , d ) = 2 log l ( f , d ) + 2  . 
to select the most consistent model for each variant , w for a c mut estimate and mutational status were computed across purity and vaf cis and were then summed . 
the ratio of w or sums of ws for a set of models indicates their relative strength of evidence.33 thus , aggregate weights , wgerm and wsom , were calculated by summing all germline and all somatic models , respectively . 
similarly , aggregate weights for loh status in germline and somatic models were calculated independently ; wloh > 0.5 was considered as significant presence of loh in tumors . results modeling mutational status of substitution and small indels observed vaf of a mutation in hybrid capture dna sequencing depends on the relative number of cancer cells compared with normal cells ( tumor purity ) in a specimen ( fig 1a )  . 
 however , for germline models , the mutant allele is present in both normal and tumor cells ( fig 1c )  . lohgic is developed on a model - selection scheme using aic weighting.33 lohgic infers the most consistent model describing the germline versus somatic mutational status with the corresponding number of mutated copies for each mutation . 
loh events , especially at the brca1 / 2 loci , can occur by either deletion of the wild - type allele ( ie , reduction to copy number one ) or duplication of mutant allele with loss of the wild - type under copy - neutral loh ( gene conversion or isodisomy ) .34 in our approach , models for all these mechanisms are evaluated . 
 biallelic mutations are considered if more than one pathogenic mutation is detected ; however , lohgic cannot infer rare rearrangements in the second allele or focal deletions aic weights can be interpreted as likelihoods for mutational status and presence of loh and strongly rely on the statistical confidence in assessing vaf and tumor purity . 
appendix figures a1 , a2 , and a3 illustrate the changes in aic weights at higher ploidy and across possible models , indicating how some combinations of vaf and tumor purity will not permit the selection of one model out of several , yielding ambiguous calls . 
moreover , because accuracy in vaf estimates depends on sequencing depth , inferring loh is statistically robust at depths that provide sufficient confidence in measuring vaf within 1% to 5% . lohgic is available at the khiabanian lab web site ( html )  . 
given confidences in these measurements , lohgic reports and visualizes aic weights for all possible mutational models . mutational status of brca1 / 2 alterations we identified 64 patients with cancer with candidate pathogenic brca1 / 2 mutations , detected by hybrid capture , tumor - only sequencing , in a set of 1 , 636 sequenced specimens at the rutgers cancer institute ( data supplement )  . 
in a sample with purity of 60% , sequenced at 1 , 000 , akaike information criterion ( aic ) weights ( w ) are shown across the variant allele frequencys ( vaf ) 99% ci . 
 used lohgic and predicted germline versus somatic mutational status of the brca1 / 2 mutant alleles with high confidence in 88% of patients ( 56 of 64 patients ) , 66% of whom ( 37 of 56 patients ) had germline aic weights > 0.7 and 34% of whom ( 19 of 56 patients ) had somatic aic weights > 0.7. 
our predictions significantly corroborated these data , showing 93% accuracy , 100% positive predictive value ( precision ) , 96% true - positive rate ( recall ) , 75% negative predictive value , and 25% false omission rate ( table 1 )  . 
 in only one patient , lohgic could not correctly genotype a previously validated germline brca2 mutation ; this single nucleotide deletion had a vaf of 35% ( depth , 844 ; purity , 29% )  . 
 further inspection of raw sequencing reads at the position of the deletions revealed the presence of a somatic reversion mutation ( insertion of a guanine ) that restored the reading frame and thus affected the vaf of the germline thymine deletion ( appendix fig a4 )  . six patients had data from multiple sequenced specimens . 
in 33% of these patients ( two of six patients ) , lohgics predictions agreed with genetic testing for one specimen while remaining ambiguous for the other ( table 2 )  . evaluating the loss of wild - type allele and we predicted the presence of loh when the sum of aic weights for germline or somatic models with loh was > 0.5. 
as expected for pathogenic brca1 / 2 mutations , we found loh to be prevalent in our cohort ; loh was present in 76% of patients ( 28 of 37 patients ) inferred to have a germline mutation and in 63% of patients ( 12 of 19 patients ) inferred to have a table 1 . 
in two patients , we observed two brca2 mutations ; one patient ( patient 31 ) harbored both a somatic and a germline ( without loh ) mutation , and the other patient ( patient 60 ) harbored one somatic mutation , whereas the inference of his second mutation was ambiguous ( data supplement )  . prevalence and sex specificity of brca1 / 2 mutations germline brca1 mutations were exclusively found in tumors arising in women , 87% of whom ( 13 of 15 patients ) were diagnosed with hboc or fallopian tube cancers . 
germline brca2 mutations were observed equally in cancers occurring in men and women , each at 50% ( 11 of 22 patients ) , with a wide range of tumor types . 
graphs represent the relationship between the expected vaf and purity for each model ( see materials and methods ) ; the shaded gray area represents vaf and purity cis , within which w is calculated . 
further inspection of the data from the second breast tumor indicated low purity of the sequenced specimen , which prohibited robust assessment of loh status . discussion inherited mutations in the brca1 / 2 genes contribute to 1% to 5% of breast cancers . 
these tumors almost invariably undergo loh with the loss of the wild - type allele and are shown to be sensitive to parp inhibitor and platinum treatment.13 - 15 parp inhibitors and platinum are also selectively effective in other cancers harboring mutations in brca1 / 2.35 therefore , early detection of these mutations and precise determination of their germline versus somatic status and loh is extremely important to therapeutic approaches.36 germline genetic testing men with malignancies in the prostate ( three patients ) , pancreas ( two patients ) , lung ( one patient ) , and breast ( one patient )  . 
in the setting of somatic brca2 mutation , presence of loh was inferred in 67% of patients ( 10 of 15 patients ) , uncorrelated with sex . co - mutations in patients with brca1 / 2 mutations the most common genomic alterations in brca1 / 2 - mutated tumors were tp53 mutations ( 67% ; 43 of 64 patients ) , myc amplifications ( 17% ; 11 of 64 patients ) , and cdkn2a / b deletions ( 17% ; 11 of 64 patients )  . 
tp53 mutations were present in 87% of patients ( 13 of 15 patients ) with germline brca1 mutations , co - occurring in 100% of patients ( 11 of 11 patients ) with inferred loh . 
 cnv , copy number variant ; f , female ; gist , gi stromal tumor ; m , male ; snv , single nucleotide variant ; na , not available ( lack of testing results )  . primary tumor tissue somatic brca1 heterozygous somatic brca1 with loh germline brca1 heterozygous germline brca1 with loh ambiguous brca1 somatic brca2 heterozygous somatic brca2 with loh germline brca2 heterozygous germline brca2 with loh ambiguous brca2 genetic testing patients sex tp53 mutation myc amplification cdkn2a / b deletion no . 
however , various ethical complications , uninformative family histories , and / or miscommunication between patients , families , and health care providers may result in missed opportunities to incorporate brca1 / 2 mutational status , and that of related genes , in treatment and prevention of future cancers.37 with the advent of precision oncology and implementation of high - depth sequencing in the clinic , it is now possible to partially resolve the genetic profile of tumors and their prognostic mutations soon after disease diagnosis . 
in the absence of normal dna controls , computational analysis of tumor - only genetic data are essential for identifying patients who may harbor germline brca1 / 2 mutations and prioritizing them for germline testing.38 here , we presented lohgic , which statistically infers mutational status and predicts the loss of wild - type allele under loh from deep - sequencing data . 
lohgic predictions are strongly concordant with independent germline genetic testing results and provide additional information on the likely presence of loh at brca1 / 2 in tumor cells ; patient - matched control dna genotyping is required to further support lohgics results . this analysis highlights differences in the tumor spectrum associated with the brca1 / 2 mutations . 
tumors arising in the setting of germline brca1 mutations with loh were all found in women and were exclusively breast cancer or of mllerian origmoreover , they universally harbored pathogenic tp53 mutations . 
in contrast , tumors showing germline brca2 mutation with loh had a much wider spectrum of cancers , were seen in both sexes , and did not frequently harbor tp53 mutations . 
tumors with evidence of germline brca1 / 2 mutation , but without loh , may represent sporadic tumors that arose in mutation carriers ; however , careful molecular analysis is required to rule out the presence of reversion mutations or other mechanisms including epigenetic silencing of the wild - type allele.24 , 39 haploinsufficiency may also play a role in tumorigenesis in some settings.40 in the case of somatic brca1 / 2 alterations , most were in the setting of a relatively high mutation burden , suggesting their heterozygous passenger status that may not confer defects in hr and thus sensitivity to parp inhibitors or platinum until biallelic inactivation occurs . 
although these tumors are predicted not to harbor genomic signatures of brca1 / 2 loss , deficiency in hr cannot be completely ruled out.23 , 24 our analysis may be confounded by low tumor purity and insufficient sequencing data . 
the presence of reversion mutations in brca1 / 2 , which occur under acquired resistance to platinum and parp inhibitors , 41 can also lead to incorrect or ambiguous inference . 
in our data set , a somatic reversion mutation in one patient and low tumor purity in another led to discrepant results , further illustrating the importance of incorporating statistical variations in vaf , depth , and purity , especially considering inherent biases in high - throughput sequencing . 
of note , the requirement for robust vaf determination limits this approach to hybrid capture based sequencing , because interpreting vaf in amplicon - based assays can be confounded by polymerase chain reaction efficiency . in summary , lohgic , which is freely available for academic use , will facilitate investigating the molecular epidemiology of brca1 / 2 and hr - associated mutations . 
 hirshfield , shridar ganesan deborah toppmeyer employment : novartis ( i ) leadership : novartis ( i ) financial support : hossein khiabanian , shridar ganesan stock and other ownership interests : novartis ( i ) serena wong no relationship to disclose nancy chan no relationship to disclose kalyani dhar no relationship to disclose jinesh gheeya no relationship to disclose hetal vig no relationship to disclose mohammad hadigol no relationship to disclose dean pavlick no relationship to disclose sepand ansari no relationship to disclose administrative support : lorna rodriguez - rodriguez , shridar ganesan provision of study material or patients : kim m . 
 hirshfield , mendel goldfinger , mark stein , joseph aisner , deborah toppmeyer , serena wong , nancy chan , kalyani dhar , jinesh gheeya , hetal vig , lorna rodriguez rodriguez , shridar ganesan collection and assembly of data : hossein khiabanian , kim m . 
hirshfield , mendel goldfinger , mark stein , joseph aisner , deborah toppmeyer , serena wong , nancy chan , kalyani dhar , jinesh gheeya , hetal vig , dean pavlick , siraj ali , lorna rodriguez - rodriguez , shridar ganesan data analysis and interpretation : hossein khiabanian , kim m . 
 for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . siraj ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine ; patents via seres health on microbiome stuff in non - neoplastic disease ( i ) bing xia no relationship to disclose lorna rodriguez - rodriguez no relationship to disclose shridar ganesan employment : merck ( i ) stock and other ownership interests : ibris , inspirata , merck ( i ) consulting or advisory role : inspirata , novartis patents , royalties , other intellectual property : i hold two patents for digital imaging that may be licensed to ibris and inspirata travel , accommodations , expenses : inspirata hossein khiabanian no relationship to disclose kim m . 
hirshfield , mendel goldfinger , simon bird , mark stein , joseph aisner , deborah toppmeyer , serena wong , nancy chan , kalyani dhar , jinesh gheeya , hetal vig , mohammad hadigol , sepand ansari , bing xia , lorna rodriguez - rodriguez , and shridar ganesan , rutgers cancer institute of new jersey , rutgers university ; hossein khiabanian , kim m . 
samimi g , bernardini mq , brody lc , et al : traceback : a proposed framework to increase identification and genetic counseling of brca1 and brca2 mutation carriers through family - based outreach . 
finch a , beiner m , lubinski j , et al : salpingo - oophorectomy and the risk of ovarian , fallopian tube , and peritoneal cancers in women with a brca1 or brca2 mutation . 
giri vn , obeid e , gross l , et al : inherited mutations in men undergoing multigene panel testing for prostate cancer : emerging implications for personalized prostate cancer genetic evaluation . 
de bono j , ramanathan rk , mina l , et al : phase i , dose - escalation , two - part trial of the parp inhibitor talazoparib in patients with advanced germline brca1 / 2 mutations and selected sporadic cancers . 
wagle n , berger mf , davis mj , et al : high - throughput detection of actionable genomic alterations in clinical tumor samples by targeted , massively parallel sequencing . 
alexandrova em , mirza sa , xu s , et al : p53 loss - of - heterozygosity is a necessary prerequisite for mutant p53 stabilization and gain - of - function in vivo . 
christie el , fereday s , doig k , et al : reversion of brca1 / 2 germline mutations detected in circulating tumor dna from patients with high - grade serous ovarian cancer . 
 ploidy 1 or 2 ploidy 3 somatic loh cnmut = 1 germline loh cnmut = 1 somatic loh cnmut = 1 germline loh cnmut = 1 somatic , cnmut = 1 germline , cnmut = 1 somatic , cnmut = 1 germline , cnmut = 1 somatic loh , cnmut = 2 germline loh , cnmut = 2 somatic loh , cnmut = 2 germline loh , cnmut = 2 somatic loh , cnmut = 3 germline loh , cnmut = 3 somatic loh , cnmut = 3 germline loh , cnmut = 3 depth : 1000 purity 0.60 depth : 1000 purity 0.60 somatic loh cnmut = 1 germline loh cnmut = 1 somatic loh cnmut = 1 germline loh cnmut = 1 somatic , cnmut = 1 germline , cnmut = 1 somatic , cnmut = 1 germline , cnmut = 1 somatic loh , cnmut = 2 germline loh , cnmut = 2 somatic loh , cnmut = 2 germline loh , cnmut = 2 somatic loh , cnmut = 3 germline loh , cnmut = 3 somatic loh , cnmut = 3 germline loh , cnmut = 3 fig a2 . 
similar to the models shown in figure 1 , here , the sum of aic weights across vaf and purity cis ( shown in parentheses ) larger than 0.7 indicates unambiguous prediction of a model . 
expected variant allele frequency ( vaf ) versus specimen purity for all possible models is shown at mutational ploidy of ( a ) one and two and ( b ) three . 
akaike information criterion weights for a sample with purity of 60% , sequenced at 1 , 000 are shown at ploidy of ( c ) one and two and ( d ) three . 
overlapping regions show how some combinations of tumor purity , ploidy , and sequencing depth may not permit the selection of one model out of several , resulting in ambiguous results . 
pathology demonstrated metastatic colloid / mucinous adenocarcinoma ( stage pt4a , pn2b , pm1c )  . immunohistologic testing for dna mismatch repair ( mmr ) proteins on tissue biopsy specimen showed preservation of muts protein homolog 2 ( msh2 ) and muts homolog 6 ( msh6 ) , but loss of mutl homolog 1 ( mlh1 ) and mismatch repair endonuclease pms2 ( pms2 ) , consistent with mmr deciency . 
initially , the patient was treated with four doses of uorouracil , leucovorin , oxaliplatin , and irinotecan ( folfoxiri ) until computed tomography scanning revealed an increase in peritoneal masses and liver metastases . 
he then was treated with pembrolizumab on the basis of mmr deciency ; however , this was discontinued after three doses when scans revealed progressive disease , and a doubling of carcinoembryonic antigen since initiation was noted ( 401 ng / ml to 848 ng / ml )  . 
all patient information was curated under an institutional review board protocol ( mcc 19161 ) , which was formally reviewed and granted approval by moftt cancer center ( mcc )  . 
this institutional review board protocol includes a waiver of consent , because no identifying information is reported in the case . a foundationone cdx test ( foundation medicine , cambridge , ma ) was ordered on the diagnosed omental tissue with subsequent review by the personalized medicine clinical service ( pmcs ) at mcc for guidance regarding future therapeutic options ( table 1 )  . 
the molecular tumor board ( mtb ) discussion focused on approaches for targeted therapeutic considerations in a patient with high tumor mutation burden ( tmb ) after disease progression on an immune checkpoint inhibitor . the patient had 93 reported alterations ; the foundationone cdx report provided interpretive content for 26 of them for correlated therapies with clinical benet , clinical trials , or therapies with a lack of response . 
in a patient with high tmb status and microsatellite instability ( msi ) , the likelihood of an individual alteration primarily driving the cancer is difcult to ascertathe pmcs categorized alterations into common repair / signaling pathways , associating the alterations with possible therapies and ranking therapeutic options on the available evidence ( table 1 )  . 
figure 1 and appendix table a1 illustrate the workow taken by the pmcs to identify and prioritize treatment options . of the 26 alterations for which foundationone cdx provided interpretive content , impaired homologous repair ( hr ) was a commonly altered pathway . 
highlight alterations with targeted therapies tmb : high ( 105 muts / mb ) microsatellite status : unstable kras a59t atm r2227c brca2 n319fs * 8 nf1 i679fs * 21 ptch1 r1308fs * 64 akt1 e17k msh6 f1088fs * 2 men1 r612h mtor a469t apc h298fs * 28 apc r1114 * apc v2194fs * 5 arid1a g889fs * 2 asxl1 g646fs * 12 bcorl1 p1681fs * 20 ctcf t204fs * 18 keap1 f478fs * 2 mll2 p2354fs * 30 notch3 a1701v notch3 g2035fs * 60 notch3 p1317fs * 103 pbrm1 w992fs * 23 ptpn11 s502p qki k134fs * 14 setd2 f1650v sox9 v306fs * 77 pold1 r17q flt1 s733del 66 vus 2 . 
categorize by mechanism tmb - high msh6 arid1a brca2 akt1 kras * nf1 * mmr deficiency mmr deficiency mmr deficiency hr deficiency hr deficiency hr deficiency akt activation ras activation ras activation 3 . 
correlate mechanisms to therapies parp or atr inhibitor second line of immunotherapy ( combination therapy or novel agent on trial ) pi3k - akt - mtor inhibitor arid1a brca2 tmb - high msh6 arid1a brca2 akt1 4 . 
 ( 3 ) correlating grouped repair / signaling mechanisms from step 2 with possible targeted therapy options assists collecting and correlating supporting evidence to be considered by a molecular tumor board ( mtb )  . 
 ( 4 ) the mtb reviewed the evidence and prioritized therapy options according to the patients current disease state , current failed line of therapy , patient preference , strength of evidence associated with an alteration and therapy option , and available clinical trials . 
nct03188965 ( first - in - human study of atr inhibitor bay1895344 in patients with advanced solid tumors and lymphomas ) was recruiting patients with atm alterations and was further supported by clinical , in vivo , and in vitro data . 
 ( * ) the kras a59t and nf1 i679fs * 21 alterations produced conicting likelihoods of response to epidermal growth factor receptor ( egfr ) inhibitors and were based on minimal case report data . 
 nelson et al ( parp ) inhibitors or immunotherapy.2 , 3 parp inhibition in the context of brca alterations has demonstrated clinical benet in breast , ovarian , and prostate cancer and has produced discussion of expansion to other ddr deciencyrelated alterations.4 atm encodes a protein kinase that plays a key role in dna repair , cell cycle checkpoints , and apoptosis in response to dna damage.5 the atm r2227c alteration is clinically relevant , because it produces a missense alteration in the frap - atm - trrap ( fat ) domain , has been categorized as deleterious in breast cancer and adenoid cystic carcinoma , and is classied as pathogenic by clinvar ( clinvar / )  . 
in a phase ii trial of patients with ddr - defective metastatic castrate - resistant prostate cancer receiving olaparib , patients with germline or somatic alterations in genes involved in ddr showed signicantly increased activity , with responses occurring in 14 out of 16 patients ( 88% ) .6 , 7 the at - rich interactive domain - containing protein 1a ( arid1a ) g889fs * 2 alteration is likely inactivating ( catalogue of somatic mutations in cancer mutation id : cosm6911235 )  . arid1a is a subunit of the chromatin remodeling complex swi / snf that is involved in facilitating access of proteins to dna , and inactivating alterations are common across various cancer types.8 pathways involved in ddr have been shown to interact with arid1a , including msh2 . 
during dna replication , it has been demonstrated that arid1a recruits msh2 to chromatin and promotes mmr.8 thus , inactivation of arid1a has been shown to impair mmr . arid1a deciency has demonstrated sensitization to parp inhibitors in vitro and in vivo.9 atr , another important genetic component of ddr , has been the target of novel investigational drugs that inhibit atr and arid1a signaling in vitro and in vivo.5 , 10 collectively , arid1a , atm , and brca2 produce a common theme of ddr / hr deciency , which leads to atr or parp inhibition alone or in combination with platinum or another dna - damaging chemotherapy agent in an off - label or ( more preferred ) clinical trial setting were recommended as viable options . akt1 e17k has been reported as a missense alteration that occurs in the pleckstrin homology domain of rac - alpha serine / threonine - protein kinase ( akt1 ) and activates akt signaling leading to inhibition of cell apoptosis and promotion of cellular proliferation.11 this alteration is therefore considered oncogenic and is well described in the literature . 
in a phase i , dose - escalation trial of the pan - akt inhibitor azd5363 , 58 patients with solid tumor found to have somatic akt1 e17k alterations were enrolled . 
the median progression - free survival was 5.5 months for patients with estrogen - positive breast cancer , 6.6 months for patients with gynecologic disease , and 4.2 months for patients with other solid tumors , including two patients with colorectal cancer ( crc ) .12 however , in a patient with a high tmb and msi , the value of this akt1 e17k mutation as a clinically relevant driver is unclear . 
in case the clinical team decided to target akt , clinical trials , including nct02465060 ( nci - match - arm z1k ) , nct03310541 , or nct02761694 , could be considered . finally , the kras a59t alteration is less common than other known activating kras alterations but has been reported as resulting in increased activation of the map kinase and pi3k pathways in vivo.13 interestingly , this alteration may demonstrate an exception to the observation that patients with kras - mutated metastatic crc do not receptor respond to epidermal growth factor ( egfr ) targeted monoclonal antibodies cetuximab or panitumumab . 
there is one case report of a patient with metastatic crc and the kras a59t alteration who was treated with panitumumab plus uorouracil , leucovorin , and irinotecan and experienced a partial radiographic response ( 36% decrease per response evaluation criteria in solid tumors 1.1 ) , stable carcinoembryonic antigen biomarker , and decreased size of metastases for an 8 - month duration.14 the patient showed no other alterations in exons 2 and 3 of kras , nras , and hras genes ; exon 15 of braf ; and exons 2 , 5 , 9 , 10 , 20 , and 21 of pik3ca . this seems to be the rst observed documentation of the a59t allele not producing resistance to egfr - targeting monoclonal antibodies and may provide a potential future consideration for our patient.14 however , there is limited evidence that the nf1 frame shift may predict poorer response to cetuximab or panitumumab therapy on the basis of a small case series of four chinese patients with metastatic crc who were kras g12 and g13 wt but found to have inactivating nf1 alterations . 
the alterations involved in hr deciency ( brca2 , atm , and arid1a inactivation ) provided the most robust combined evidence of predicted response to future therapy options . the akt1 e17k alteration is known to be activating , but its importance in a highly mutated , unstable tumor was less well dened . 
 therapy option prioritization in crc with high mutation burden follow - up of the patients case , unfortunately , showed that after three treatments of pembrolizumab , there was no sign of response , which led the clinical team to refer back to the above options to consider treatment beyond immunotherapy . 
the clinical team discussed the predominant grouping of alterations ( arid1a , atm , and brca2 ) with the common theme of ddr / hr deciency and ultimately decided to enroll the patient in a clinical trial ( clinicaltrials.gov identier : nct03188965 ) investigating the atr inhibitor bay1895344 in patients with solid tumor with atm loss . the lesson learned with this patient was one of categorizing a large list of alterations and prioritizing each according to therapeutic targets on the basis of dominant signaling / repair pathways and strength of available evidence . 
in doing so , the pmcs was able to provide the treating physician with a succinct , prioritized grouping of alterations validating the initial line of therapy and considerations for future therapeutic options , which led to the patient being enrolled in a clinical trial with the greatest anticipated therapeutic benet . 
walko , pharmd , 12902 magnolia dr , tampa , fl 33612 ; twitter : @mofttnews ; e - mail : christine.walko@moftt.org. support supported in part by national cancer institute comprehensive cancer center support grant no . 
mcleod leadership : cancer genetics stock and other ownership interests : cancer genetics , interpares biomedicine honoraria : genentech , illumina consulting or advisory role : gentris , cancer genetics , saladax biomedical , national institutes of health / national cancer institute , admera health , evicore healthcare , pharmazam speakers bureau : genentech christine m . 
walko employment : mission healthcare stock and other ownership interests : alexion pharmaceuticals ( i ) consulting or advisory role : foundation medicine , jackson laboratory for genomic medicine , intermountain precision genomics other relationship : mission hospital no other potential conicts of interest were reported . references cerniglia m , xiu j , grothey a , et al : association of dna damage response and repair genes ( ddr ) mutations and microsatellite instability ( msi ) , pd - l1 expression , tumor mutational burden ( tmb ) in gastroesophageal cancers . 
j clin oncol 37 , 2019 ( suppl 4 ; abstr 60 ) overman mj , mcdermott r , leach jl , et al : nivolumab in patients with metastatic dna mismatch repair - decient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
lancet oncol 18 : 1182 - 1191 , 2017 ghiringhelli f , richard c , chevrier s , et al : efciency of olaparib in colorectal cancer patients with an alteration of the homologous repair proteworld j gastroenterol 22 : 10680 - 10686 , 2016 pili e pg , gay cm , byers la , et al : parp inhibitors : extending benet beyond brca - mutant cancers . 
clin cancer res 25 : 3759 - 3771 , 2019 shiloh y , ziv y : the atm protein kinase : regulating the cellular response to genotoxic stress , and more . 
n engl j med 373 : 1697 - 1708 , 2015 shen j , ju z , zhao w , et al : arid1a deciency promotes mutability and potentiates therapeutic antitumor immunity unleashed by immune checkpoint blockade . 
nat med 24 : 556 - 562 , 2018 shen j , peng y , wei l , et al : arid1a deciency impairs the dna damage checkpoint and sensitizes cells to parp inhibitors . 
banerji u , dean ej , p erez - fidalgo ja , et al : a phase i open - label study to identify a dosing regimen of the pan - akt inhibitor azd5363 for evaluation in solid tumors and in pik3ca - mutated breast and gynecologic cancers . 
mei z , shao yw , lin p , et al : smad4 and nf1 mutations as potential biomarkers for poor prognosis to cetuximab - based therapy in chinese metastatic colorectal cancer patients . 
ninety - three alterations were reported on the foundationone cdx report ( including variants of known and unknown signicance )  . twenty - six of the alterations had interpretive content for correlated therapies with clinical benet , clinical trials , or therapies with a lack of response . 
twenty - seven alterations had potentially relevant information ( maf , listed in exac , protein domain location , in oncokb and others ) as reported in the initial screening of ndings . 
 enrichment of fgfr3 - tacc3 fusions in patients with bladder cancer who are young , asian , or have never smoked purpose fgfr3 - tacc3 ( fibroblast growth factor receptor 3transforming acidic coiled coil - containing protein 3 ) fusions have recently been identified as driver mutations that lead to the activation of fgfr3 in bladder cancer and other tumor types and are associated with sensitivity to tyrosine kinase inhibitors . 
we examined the clinical and molecular characteristics of patients with fgfr3 - tacc3 fusions and hypothesized that they are enriched in a subset of patients with bladder cancer . materials and methods we correlated somatic fgfr3 - tacc3 fusions with clinical and molecular features in two cohorts of patients with bladder cancer . 
the second cohort consisted of patients with mibc or high - grade nonmibc at the dana - farber cancer institute that had targeted capture sequencing of a selected panel of cancer genes ( n = 356 )  . 
the clinical response of one patient with fgfr3 - tacc3 bladder cancer to an fgfr3 inhibitor was investigated . results overall , 751 patients with high - grade bladder cancer without fgfr3 - tacc3 fusions and 17 with fgfr3 - tacc3 fusions were identified in the pooled analysis of the data sets from the cancer genome atlas and the dana - farber cancer institute . 
 fgfr3 - tacc3 fusions were enriched in patients age 50 years versus age 51 to 65 years versus those older than 65 years ( pooled , p = .002 ) , and were observed in four ( 12% ) of 33 patients age 50 years in the pooled analysis . 
in 2017 , 79 , 030 new cases of bladder cancer are expected to be diagnosed , and approximately 16 , 870 deaths are predicted to occur from the disease in the united states.1 , 2 compared with other cancer subtypes , advances in the management of bladder cancer have been limited in the past three decades , and there is an unmet need to develop novel therapeutic agents that target potentially actionable alterations.3 , 4 genomic alterations in fibroblast growth factor receptors ( fgfrs ) are among the most frequent events during bladder cancer development . 
fgfrs are receptor tyrosine kinases that orchestrate various cellular processes , including cell proliferation , differentiation , and survival.5 fgfr mutations lead to developmental syndromes when present in the germline , and contribute to cancer growth when acquired somatically.6 fgfr fusions with an intact kinase domain have been identified in several cancer amin h . 
consort diagram for 850 patients with bladder cancer . clinical cohort ( n = 850 ) dana - farber cancer institute ( n = 438 ) the cancer genome atlas ( n = 412 ) whole - exome sequencing ( n = 412 ) paired tumor - normal muscle - invasive bladder cancer rna sequencing for structural variant calls assessment of clinical and molecular characteristics in fgfr3 - tacc3positive versus negative bladder tumors institutional targeted next - generation sequencing assay oncopanel ( n = 438 ) computational workflow ( n = 365 ) mutational calling ( mutect ) copy number variations ( viscap - cancer ) breakmer algorithm ( structural variants ) exclusions low - grade nonmuscle invasive histology ( n = 73 ) exclusions low tumor purity ( < 20% ; n = 9 ) final analysis ( n = 356 ) assessment of clinical and molecular characteristics in fgfr3 - tacc3positive versus negative bladder tumors types , including cervical cancer , bladder carcinoma , glioblastoma multiforme , squamous lung carcinoma , and head and neck cancer.7 - 15 fgfr3 , a member of this family , has been reported to be involved in fusions with several genes in bladder carcinoma , including tacc3 ( transforming acidic coiled coil - containing protein 3 )  . 
tacc3 normally is thought to mediate the stabilization and organization of the mitotic spindle during mitosis.14 in the cancer genome atlas ( tcga ) muscle invasive bladder cancer ( mibc ) cohort , in - frame activating fgfr3 - tacc3 fusionsobserved in 10 ( 2.4% ) of 412 patientswere the most common gene fusions identified.7 fgfr3 - tacc3 fusion proteins consist of the immunoglobulin , transmembrane , and tyrosine kinase domains of fgfr3 , fused to the coiled - coil domain of tacc3 . 
through the promotion of dimerization , these fusions lead to a constitutively active fgfr3 kinase protein that has been demonstrated to promote cell proliferation in vivo and in vitro.7 - 9 , 13 phase i and ii trials of fgfr inhibitors have reported promising antitumor activity in patients with fgfr genetic alterations , especially bladder cancer.16 certain genetic alterations , particularly gene fusion events , are enriched in clinical subsets of patients with cancer . 
 patients with mibc and high - grade non - mibc were pooled together in the dfci cohort as there is substantial evidence that the two subtypes are biologically and genomically similar.21 - 23 overall , seven patients with fgfr3 - tacc3 fusions were identified in the dfci cohort using an institutional targeted next - generation sequencing assay24 ( oncopanel )  . 
figure 1 shows the sample inclusion and exclusion criteria and workflow . tissue collection and dna extraction tumor specimens and clinicopathologic information were collected with institutional review board approval at dfci . 
tumor areas that contained at least 20% of tumor cells ( mean tumor purity , 58% ; range , 20% to 100% ) were isolated from normal tissue and chosen for dna extraction . 
dna was quantified by nanodrop and pico - green assays . targeted sequencing two hundred nanograms of genomic dna from each sample was subjected to targeted exon capture and sequencing using oncopanel_v1 to v3 cancer gene panels at brigham and womens hospital ( boston , ma )  . 
the oncopanel gene panel includes capture probes for 275 to 560 cancer - associated genes , as well as intronic portions of 60 genes for rearrangement detection , including fgfr3.24 sample dna was captured using oncopanel_v1 to v3 bait sets using a solution - phase agilent sureselect hybrid capture kit ( agilent technologies , santa clara , ca )  . 
single - nucleotide variants and small indels were analyzed using mutect version 1 0.27200 ( display / cgatools / mutect ; accessed may 2013 ) and annotated by oncotator ( broadinstitute.org / oncotator ; accessed may 2013 )  . 
 copy number alterations were analyzed using a custom r - based tool26 , 27 ( viscap - cancer )  . mean depth of read coverage for the targeted genes was 283 . 
mean , median , and range of percentage of target bases with read depth > 30 was 98% , 99% , and 78% to 99% , respectively . identification of rearrangements and analysis of genomic breakpoints fgfr3 fusion sequences were identified using the breakmer algorithm28 and were manually reviewed using integrated genomic viewer29 to exclude sequencing or alignment artifacts . 
all analyses of sequencing data and mutation and fusion calls were performed blinded to clinical data . clinical response to anti - fgfr3 therapy one patient with fgfr3 - tacc3 mibc received anti - fgfr3 therapy along with docetaxel and the clinical response was monitored . statistical analysis we used fisher 's exact test for categorical data and the wilcoxon rank - sum test for quantitative data . 
 ( % ) , unless otherwise noted . abbreviations : dfci , dana - farber cancer institute ; fgfr3 , fibroblast growth factor receptor 3 ; hg , high grade ; nd , not determined ; nmibc , nonmuscle invasive bladder cancer ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; tcga , the cancer genome atlas . fusion partner fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - tacc3 fgfr3 - lmnb2 fgfr3 - tnip2 fgfr3 - fam184b fgfr3 - jakmip1 fgfr3 4 : 1808826 ; 4 : 1737404 4 : 1808771 ; 4 : 1740268 4 : 1808744 ; 4 : 1740297 4 : 1808806 ; 4 : 1741100 4 : 1808737 ; 4 : 1741297 4 : 1808690 ; 4 : 1741336 4 : 1808937 ; 4 : 1732863 4 : 1808556 ; 19 : 2436887 4 : 1808750 ; 4 : 2752213 4 : 1809003 ; 4 : 17691454 4 : 1808936 ; 4 : 6091989 fig 2 . 
schematic representation of the genomic rearrangements observed in 11 tumor samples that harbor fibroblast growth factor receptor 3 ( fgfr3 ) fusion variants identified using the oncopanel assay in the dana - farber cancer institute cohort . 
fam184b , family with sequence similarity 184 member b ; lmnb2 , lamin b2 ; jakmip1 , janus kinase and microtubule interacting protein 1 ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; tnip2 , tnfaip3 interacting protein 2 . results formalin - fixed , paraffin - embedded tumor specimens were obtained from 438 patients at dfci . 
 we excluded 82 tumors from the analysis because they were of low - grade nonmuscle invasive histology ( n = 73 ) or had low ( < 20% ) tumor purity ( n = 9 )  . 
we mapped the genomic breakpoints of fgfr3 and its corresponding fusion partners that were identified in the dfci cohort , which included four non - tacc3 fusions ( fig 2 )  . 
 ( % ) , unless otherwise noted . abbreviations : dfci , dana - farber cancer institute ; fgfr3 , fibroblast growth factor receptor 3 ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; tcga , the cancer genome atlas . patients age 50 harboring a fusion ( p = .03 ; table 2 )  . 
fgfr3 - tacc3 fusions in tcga were also more frequent in asians ( six [ 14% ] of 44 patients ) compared with other races ( p < .001 ) , as well as in never smokers ( eight [ 7.2% ] of 111 patients ) compared with ever smokers ( p < .001 ; table 2 )  . 
similarly , fgfr3 - tacc3 fusions were more common in dfci patients age 50 years ( one [ 12% ] of eight patients ) compared with other age groups ( p = .001 ; table 2 )  . 
eleven ( 65% ) of 17 patients with fgfr3tacc3 fusions were associated with least one of these three clinical characteristics , and three ( 18% ) of the 17 patients were asian never smokers age 50 years . we next examined whether tumors with fgfr3 - tacc3 fusions had molecular features that distinguished them from other tumors . 
as the oncopanel analysis was performed on tumor samples only , we excluded variants that were observed at any frequency in the exome aggregation consortium database , 30 as they were considered likely germline variants . 
the 17 patients whose tumors harbored fgfr3 - tacc3 fusions were enriched for cdkn1a mutations ( 5 [ 29% ] of 17 v 76 [ 10% ] of 751 ; p = .03 ; table 3 )  . 
conversely , fgfr3 - tacc3 fusion - positive tumors had significantly fewer tp53 mutations ( p = .02 ) , and none had rb1 mutations ( p = .054 ; table 3 )  . 
 somatic copy number alterations were also analyzed in both cohorts using criteria for loss , deletion , gain , and amplification that were developed and applied independently in the two cohorts ( table 3 )  . 
dfci cohort : amplification : log2 ( copy ratio ) > 1.8 , gain : 1.1 log2 ( copy ratio ) < 1.8 ; deletion : log2 ( copy ratio ) < 2 , loss : 2 log2 ( copy ratio ) < 1 . abbreviations : cnv , copy number variation ; dfci , dana - farber cancer institute ; fgfr3 , fibroblast growth factor receptor 3 ; snv , single nucleotide variant ; tacc3 , transforming acidic coiled - coil - containing protein 3 ; mdm2 , murine double minute 2 ; tcga , the cancer genome atlas . mdm2 ( murine double minute 2 ) gain ( p = .04 ) , deletion of pten ( p = .02 ) , and deletion of cdk2na ( p = .0033 ; table 3 )  . as a result of differences in the extent of genome sequencing in the tcga and dfci cohorts , we analyzed the overall mutational burden in each cohort separately . 
in the tcga cohort , the nonsynonymous somatic mutation rate across 18 , 862 genes was significantly higher in patients without fgfr3 - tacc3 fusions compared with those with fusions ( median 224 v 128 ; p = 0.04 ; table 3 )  . 
 in addition , there were no significant differences in the frequency of somatic copy number alterations in either the tcga or dfci cohorts ( table 3 )  . one patient who harbored the fgfr3 - tacc3 fusion in mibc in the dfci cohort was treated with an fgfr3 inhibitor and docetaxel and experienced complete remission for approximately 10 months . discussion our results demonstrate that patients with bladder cancer with fgfr3 - tacc3 fusions have distinct clinical and molecular features compared with the general population of patients with bladder cancer . 
in addition , fgfr3tacc3 fusions were associated with a low frequency of tp53 and rb1 mutations and a higher frequency of cdkn1a mutations , fgfr3 and mdm2 amplifications , and pten deletions . 
 because fgfr3 - tacc3 fusion - positive tumors can be sensitive to fgfr inhibitors , 9 , 31 , 32 these observations suggest that molecular testing to detect fgfr3 - tacc3 fusions in bladder cancer should be prioritized for patients who are young ( age 50 years ) , of asian race , and / or who have never smoked . 
most strikingly , we observed that all patients with bladder cancer who were asian never smokers younger than age 50 years ( n = 3 ) had fgfr3 - tacc3 fusions . we emphasize that our study has significant limitations as a result of the small number of patients with fgfr3 - tacc3 fusions included ( n = 17 ) , which reflects that this is a relatively rare molecular subset of bladder cancer . 
most importantly , we strongly advocate additional studies of this association to extend and confirm these findings . in conclusion , fgfr3 - tacc3 fusion - positive bladder cancer is highly enriched in asians , never smokers , and those age 50 years . 
nassar no relationship to disclose kevin lundgren no relationship to disclose mark pomerantz honoraria : bayer eliezer van allen stock and other ownership interests : synapse , tango therapeutics , genome medical consulting or advisory role : synapse , roche , third rock ventures , takeda , novartis , genome medical , invitae speakers ' bureau : illumina research funding : bristol - myers squibb , novartis lauren harshman consulting or advisory role : medivation , astellas pharma , pfizer , genentech , theragene , kew , corvus pharmaceuticals , merck , exelixis , bayer research funding : medivation , astellas pharma ( inst ) , bayer ( inst ) , sotio ( inst ) , genentech ( inst ) , dendreon ( inst ) , bristol - myers squibb ( inst ) , takeda ( inst ) , merck ( inst ) , janssen oncology ( inst ) , pfizer ( inst ) travel , accommodations , expenses : bayer atish d . 
sonpavde honoraria : uptodate consulting or advisory role : bayer , genentech , sanofi , merck , novartis , pfizer , argos therapeutics , agensys , eisai , astrazeneca , janssen pharmaceuticals , amgen , bristolmyers squibb , exelixis speakers ' bureau : clinical care options , national comprehensive cancer network , physician education resource , onclive , research to practice research funding : onyx pharmaceuticals ( inst ) , bayer ( inst ) , boehringer ingelheim ( inst ) , celgene ( inst ) , merck ( inst ) , pfizer ( inst ) other relationship : boehringer ingelheim , astrazeneca affiliations amin h . 
1p01ca120964 : molecular pathogenesis of the hamartoma syndromes . a directly related abstract was accepted as a poster presentation in the 2018 genitourinary cancer symposium of the american society of oncology , san francisco , ca , february 8 - 10 , 2018 . support prior presentation references 1 . 
acquaviva j , he s , zhang c , et al : fgfr3 translocations in bladder cancer : differential sensitivity to hsp90 inhibition based on drug metabolis mol cancer res 12 : 1042 - 1054 , 2014 4 . 
nogova l , sequist lv , perez garcia jm , et al : evaluation of bgj398 , a fibroblast growth factor receptor 1 - 3 kinase inhibitor , in patients with advanced solid tumors harboring genetic alterations in fibroblast growth factor receptors : results of a global phase i , dose - escalation and dose - expansion study . 
shaw at , yeap by , mino - kenudson m , et al : clinical features and outcome of patients with nonsmall - cell lung cancer who harbor eml4 - alk . 
humphrey pa , moch h , cubilla al , et al : the 2016 who classification of tumours of the urinary system and male genital organs - part b : prostate and bladder tumours . 
balbs - martnez c , sagrera a , carrillo - de - santa - pau e , et al : recurrent inactivation of stag2 in bladder cancer is not associated with aneuploidy . 
lindgren d , frigyesi a , gudjonsson s , et al : combined gene expression and genomic profiling define two intrinsic molecular subtypes of urothelial carcinoma and gene signatures for molecular grading and outcome . 
garcia ep , minkovsky a , jia y , et al : validation of oncopanel : a targeted next - generation sequencing assay for the detection of somatic variants in cancer . 
tabernero j , bahleda r , dienstmann r , et al : phase i dose - escalation study of jnj - 42756493 , an oral pan - fibroblast growth factor receptor inhibitor , in patients with advanced solid tumors . 
 use of a targeted exome next - generation sequencing panel offers therapeutic opportunity and clinical benet in a subset of patients with advanced cancers scott kopetz , md , phd1 ; kenna r . 
jack lee , md1 ; jiexin zhang , ms1 ; beate litzenburger , phd1 ; vijaykumar holla , phd1 ; walter kinyua , ms1 ; emily broaddus1 ; molly s . 
broaddus , md , phd1 purpose smaller hotspot - based next - generation sequencing ( ngs ) panels have emerged to support standard of care therapy for patients with cancer . 
survival and the impact of matched therapy use were determined by kaplan - meier estimate , log - rank test , and cox proportional hazards regression . results the larger ngs panel identied at least one alteration in an actionable gene not previously identied in the smaller sequencing panel in 214 ( 41% ) of 521 of enrolled patients . 
with current clinical molecular diagnostics , sequencing is faster , uses less tumor dna , and costs less when genes are multiplexed into small next - generation sequencing ( ngs ) panels . 
historically , the focus was often on the identication of mutations found in hotspotsareas of the genome where known drivers are frequently mutated , many of which can be mapped to therapeutic intervention . 
these panels typically emphasize genes that are recommended by cancer treatment guidelines . an emerging utility of ngs is the screening of other types of cancers for mutations in clinically actionable genes that can be targeted therapeutically . 
such treatment approaches are associated with improved in retrospective analyses screening , 1 prosurvival spective trials , 2 - 4 and meta - analyses , 5 - 7 but this approach is not universally embraced.8 , 9 an important issue in these studies is the low number of patients who benet from this approach . 
 kopetz et al context key objective can additional actionable information be identied by expanding sequencing coverage to the full exome of hundreds of genes beyond hotspot analysis and , secondarily , does that additional information affect patient outcomes ? knowledge generated only a small number of genes have alterations that are specically listed in a us food and drug administrationapproved indication that would match a patient with cancer to a specic actionable agentfor example , braf v600e to vemurafenib . 
limited access to targeted therapy trials is an issue , as some trials enroll only certain tumor types or are only active in a few geographic sites . in patients with advanced cancer that is refractory to standard treatment , any benet gained from the detection of mutations in clinically actionable genes beyond those detected using focused hotspot sequencing panels remains unknown . 
hotspot - focused ngs panels fail to robustly identify copy number alterations or mutations that are found outside commonly altered loci , which would represent an advantage of larger ngs initiative was to panels . 
enrollment criteria included the following : adult patient with pathologic documentation of a single solid tumor malignancy ; completed frontline treatment and any standard treatments that extended life by at least 3 months ; eastern cooperative oncology group performance status of 0 or 1 ; no active brain metastases ; and completed tumor testing using a smaller sequencing panel and either disease progression on a matched therapy that targeted a previously identied actionable nding or no clinically actionable mutations detected . molecular assays and decision support that consisted of hotspot mutation testing was primarily performed on archival formalin - xed , parafn - embedded primary and metastatic cancers acquired during the course of routine clinical care using a 46or 50 - gene ngs panel described previously10 ( actionable genes summarized in the data supplement )  . 
subsequent testing used a larger ngs the entire coding regions of panel 409 cancer - related genes with methodologies previously detailed11 ( actionable genes and details of larger ngs panel provided in the data supplement )  . 
the protocol did not provide for image - guided biopsies of the most recent metastasis for testing ; median time since tissue acquisition to ngs was 467 days ( appendix fig a1 )  . relevant germline ndings were reported to the referring oncologist.12 for comparisons with protocol patients , the cancer genome atlas ( tcga ) datagene mutations and gene amplicationsfor the same 409 genes from 316 ovarian high - grade serous carcinomas , 212 colorectal adenocarcinomas , and 230 lung adenocarcinomas were extracted using cbioportal.org. 
for patients with colorectal cancer , mismatch repair was assessed as part of routine clinical care.13 somatic mutations and amplications that were reported for each patient were reviewed by the precision oncology decision support team.14 , 15 this involved annotation for function and potential clinical trial matching for actionability . 
characteristics for patients enrolled and tested in the prospective protocol characteristic female male performance status missing race asian black white hispanic other unknown tumor type bladder breast colorectal endometrial hawaiian / pacic islander gastric / gastroesophageal junction germ cell tumor head and neck lung neuroendocrine others ovarian prostate renal sarcoma thyroid age , years 20 20 - 30 30 - 40 40 - 50 50 - 60 60 - 70  . 
for the smaller 46and 50 - gene ngs panel , 34 and 38 genes , respectively , were considered actionable , whereas for the larger 409 - gene ngs panel , 96 genes were actionable ( data supplement )  . statistical analysis study sample size was dictated by the capacity of the clinical laboratory improvement amendmentscertied clinical molecular diagnostics laboratory that performed the 409 - gene ngs panel , estimated to be 25 cases per week . with a target of 600 patients , it was determined a priori that the rate of identication of alterations in actionable genes could be estimated with a standard error of no more than 0.02. 
we used fishers exact test to assess whether the gene mutation frequency was signicantly different between protocol patients with colorectal adenocarcinoma , lung adenocarcinoma , or ovarian high - grade serous carcinoma and corresponding tcga data sets . 
the probability of overall survival was determined by kaplan - meier estimate , and we used a log - rank test to assess the statistical signicance of the difference between patient groups . 
to evaluate the effect of clinical variables on overall survival , we performed multivariable survival analysis using a cox proportional hazards regression model that included variables that were signicant ( p , .05 ) in a univariable analysis . results characteristics of the patient population enrolled in the protocol a total of 675 patients were enrolled , with large - panel testing completed in 569 patients . 
five hundred twenty - one patients who received at least 6 months of follow - up or who died within 6 months were included in the analysis ( appendix fig a2 )  . colorectal cancer , sarcoma , head and neck cancer , ovarian cancer , and breast cancer were the most frequently represented cancers in the cohort ( table 1 ) , but the protocol enrolled patients with a broad spectrum of cancer types . sequencing results once material was received by the molecular diagnostics laboratory , a median of 13 days passed before the molecular reports were nalized and entered into the electronic medical record ( appendix fig a3 )  . 
of the 521 patients who were tested with the 409 - gene ngs assay , 214 ( 41% ) had at least one tumor alteration in an actionable gene that was not identied in a prior assay using a smaller ngs panel ( figs 1a and 1b )  . full 409 - gene ngs assay results are summarized for all patients in the data supplement . 
not counting the sequencing results from the smaller panel , the mean number of alterations detected in actionable genes in the 409 - gene panel was 1.0 ( range , 0 to 66 ; fig 1c )  . 
after the application of decision support , 201 ( 41% ) of 495 alterations in actionable genes were considered to affect the function of the gene and were deemed actionable ( mean per patient , 0.4 ; range , 0 to 5 ; fig 1d )  . 
the rate of detection of an alteration in an actionable gene with additional testing was dependent on tumor type , with low rates observed in thyroid and ovarian cancers ( fig 2a )  . 
alterations in a variety of actionable genes from the 409 - gene panel were identied , with the most common mutations in genes nf1 , mdm2 , atm , kdr , notch2 , erbb2 , mtor , and pten ( fig 2b )  . matching tested patients to targeted therapy of the 214 patients who had alterations in actionable genes in the large ngs platform that were not detected in the previous small - panel ngs testing , 40 ( 19% ) were matched gender race male female unknown other hispanic hawaiian / pacific islander white black asian disease site others thyroid sarcoma renal ovarian lung colorectal breast age , years > q3 : 65 - 85 q2 - q3 : 56 - 65 q1 - q2 : 46 - 56 < q1 : 18 - 46 fig 1 . 
on average , only one alteration in an actionable gene per tumor was detected . ( d ) on average , only 0.4 actionable alterationsmutation or amplication in an actionable gene that is known or has inferred biologic functionwere detected per tumor . 
 ( a ) stacked bar chart shows the percent of cases for each broad class of tumor type listed with 0 , 1 , 2 , or 3 or more alterations in actionable genes not detected in the smaller testing panel . data are shown for tumor types in which at least 10 patient tumors were sequenced . 
these patients had mutations in actionable genes that were classied as actionable , potentially actionable , or a variant of unknown signicance but the oncologist chose a therapy that was not a match to the gene alterations treating with matched therapy found . 
reasons for not protocols were similar to those from a previously reported patient population18 and included declining performance status , a desire to seek treatment closer to home , or an oncologist who did not consider the gene mutation clinically actionable or the targeted therapy sufciently active in the given tumor type ( data supplement )  . decision support decision support was critical as alterations were detected in a number of actionable genes that were less familiar to oncologists , and the availability of matching clinical trials varied during the study period . 
given the hypermutated nature of this patients tumor , it was felt that none of the mutations would act as a driver or represented a good target for matched therapy ; thus , they were not annotated ( fig 3a )  . 
not counting the sequencing results from the smaller panel , nearly 70% of tumor alterations were identied in patients with tumors that were found to be in the top quartile of overall tumor mutation burden . 
 kopetz et al ( n = 201 ; 41% ) yes : inferred ( n = 35 ; 17% ) potentially ( n = 81 ; 40% ) yes : literature based ( n = 85 ; 42% ) ( n = 66 ; 13% ) ( n = 11 ; 2% ) unknown ( n = 21 ; 44% ) all gene alterations ( n = 2 , 673 ) bottom quartile 3rd quartile 2nd quartile top quartile alterations in actionable genes ( n = 495 ) actionable alterations ( n = 201 ) bottom quartile 3rd quartile bottom quartile 2nd quartile top quartile 3rd quartile top quartile 2nd quartile fig 3 . 
forty - four percent of the alterations found in actionable genes were variants of unknown signicance ( unknown ) , and 13% were not annotated because they were all from one hypermutated patient ( na )  . 
of the alterations with known function , 2% are known to be benign or not actionable ( no ) , with the remainder having some annotated function on the basis of the existing literature . 
presence of clinically actionable alterations was not related to high overall tumor mutation burden . application of decision support , the number of actionable alterations was poorly correlated with mutation burden , as less than 50% of actionable alterations in actionable genes are in the top quartile of mutation load ( fig 3b )  . 
thus , tumor mutation burden was not a good predictor of the presence of a clinically actionable alteration . patient outcomes neither the number of overall gene alterations in the tumor , nor the presence of alterations in actionable genes signicantly inuenced patient survival ( figs 4a and 4b )  . 
survival was assessed by manual curation of the medical record along with the date when a patient was last known to be alive as documented by a physician note or date of death provided by obituary , tumor registry , or reported by a family member . 
this study is limited by the lack of randomization ; however , comparison of matched and unmatched patients helps to minimize concerns related to comorbidities or declining performance status as an explanation for the differences in outcomes observed in figures 4c and 4d , as all patients in this analysis received another line of therapy , including participation in clinical trials . two patients were found to have deleterious germline mutations that were not previously known to the patient or oncologistpatient management was not altered in either case . 
 ( a - d ) kaplan - meier plots for overall survival by ( a ) total number of alterations ( actionable and nonactionable ) detected , ( b ) whether the patient had a tumor with an alteration in an actionable gene , ( c ) type of therapy and absence of alterations in actionable genes , and ( d ) whether the patient had a tumor with an alteration in an actionable gene on the 409 - genes next - generation sequencing panel received matched treatment . 
only treatment with matched targeted therapy ( c and d ) was associated with signicantly improved survival ( p = .017 compared with patients treated with nonmatched therapy )  . 
tcga did not select for patients with advanced cancers ; therefore , we compared mutation frequencies in our cohort with those of the tcga for colorectal adenocarcinoma , lung adenocarcinoma , and ovarian high - grade serous carcinoma.19 - 21 these three cancers were examined because of their relatively homogeneous histology and sufcient representation in the study . 
for colorectal cancer , kras mutation frequency was higher in our patient population , which was consistent with their resistance to epidermal growth factor receptordirected therapy22 ( data supplement )  . 
protocol patients also had a signicantly higher incidence of tp53 mutations ( 72% v 52% ; p = .004 ; data not shown )  . only 3% of protocol colorectal cancers were microsatellite instabilityhigh compared with 13% in tcga . 
at risk : wild type 507 439 315 197 112 508 440 318 198 113 508 439 319 199 114 time ( months ) time ( months ) time ( months ) mutation mutation mutation no . 
 ( a - j ) kaplan - meier plots for overall survival for nine actionable genes commonly altered in clinical protocol patients ( a - i ) and for the most common cancer types represented in the protocol ( j )  . 
only two clinically actionable genescdkn2a and cdkn2bhad lower frequencies of alteration in protocol patients with lung adenocarcinoma ( data supplement )  . discussion survival for the overall cohort was poor in this institutionwide prospective protocol that enrolled patients with advanced solid tumor malignancies refractory to treatment . for 41% of these patients , we identied an alteration in a clinically actionable gene that was not detected by previous small - panel testing . 
the overall utility of singleas opposed to sequential smallpanel , then large - panel testinglarge - panel ngs testing combined with decision support can be estimated by combining the 11% enrollment in clinical trials from our prior 46and 50 - gene panel study18 with the 8% derived from the incremental addition of the large - panel testing in this study . 
as metastases can accumulate mutations over time , this represents another potential reason for limited patient benet . with increasing gene targets and matched drugs , it is becoming increasingly difcult for an individual physician to reasonably interpret the molecular ndings from larger ngs panels . 
the importance of decision support a comprehensive precision medicine strategy is highlighted by the fact that less than one half of actionable alterations in actionable genes had been reported previously in the literature . 
over time , at least some of these variants of undetermined signicance may be found to be activating mutations after they are examined in functional assays . examples of variants that have been reclassied as activating mutations in a functional genomics platform26 include pdgfra k385m , pik3ca e110del , and ret d627n . 
the reliability of quality decision support is crucial as patients with advanced cancers have a nite lifespan . patients with advanced cancers that are refractory to standard therapy may have mutational frequencies of individual genes that differ from published frequencies derived from unselected patients . 
this was apparent in patients with colorectal cancer and ovarian high - grade serous carcinoma in whom frequencies likely reected a bias toward more clinically aggressive or treatment - resistant tumor biology . frontline treatment of ovarian cancer is for example , platinum - based chemotherapy ; is possible that , by selecting for patients with platinum - resistance , the protocol also selected for patients with ovarian cancers with therapydriven alterations in the molecular landscape . 
the phenomenon is supported by the comparison of survival populations from stage - matched patients in tcga and clinical trials , where patient survival from clinical trials was substantially lower.27 patients with advanced cancers may have higher incidences of mutations associated with other forms of treatment resistance , such as egfr t790m and esr1 mutations.28 the potentially unique molecular features in patients with advanced , chemotherapy - resistant cancers may represent one factor that contributes to the the matched targeted therapy low success rate of approach . treatment directed against actionable genes remains suboptimal . 
pathways that were previously thought to be universally targetable have proven to be difcult to treat , such as the phosphatidylinositol 3 - kinase / akt pathway , 29 or subject to variation in results by tumor type , such as braf30 or her2 / 3 mutations.31 , 32 in protocol patients , we were unable to ascertain any strong individual signals of activity for particular alterations in specic tumor types in part because of insufcient numbers of patients . in conclusion , these results demonstrate the utility of largepanel ngs testing when combined with decision support . the derived benet is realized in only a small subset of patients . 
future efforts should emphasize high - quality and timely decision support and minimize barriers to patient enrollment , with the ultimate goal of broadly delivering precision medicine to patients with solid tumor malignancies . 
broaddus , md , phd , department of pathology , unit 85 , university of texas md anderson cancer center , 1515 holcombe blvd , houston , tx 77030 ; twitter : @mdandersonnews ; e - mail : rbroaddus@ mdanderson.org. support supported , in part , by undesignated donor funds from the md anderson annual funds program provided by the provosts ofce , khalifa bin zayed al nahyan foundation , cancer prevention research institute of texas grant no . 
for more information about asco 's conict of interest policy , please refer to or po.ascopubs.org / site / ifc . scott kopetz stock and other ownership interests : molecularmatch , navire consulting or advisory role : roche , genentech , emd serono , merck , karyopharm therapeutics , amal therapeutics , navire pharma , symphogen , holy stone , biocartis , amgen , novartis research funding : amgen ( inst ) , sano ( inst ) , biocartis ( inst ) , guardant health ( inst ) , array biopharma ( inst ) , genentech ( inst ) , emd serono ( inst ) , medimmune ( inst ) , novartis ( inst ) j . 
jack lee consulting or advisory role : abbvie kopetz et al beate litzenburger employment : qiagen funda meric - bernstam honoraria : sumitomo group , dialectica consulting or advisory role : genentech , inection biosciences , pieris pharmaceuticals , clearlight diagnostics , darwin health , samsung bioepis , spectrum pharmaceuticals , aduro biotech , origimed , xencor , debiopharm group research funding : novartis , astrazeneca , taiho pharmaceutical , genentech , calithera biosciences , debiopharm group , bayer , aileron therapeutics , puma biotechnology , cytomx therapeutics , jounce therapeutics , zymeworks , curis , pzer , effector therapeutics , abbvie , boehringer ingelheim ( i ) , guardant health ( inst ) no other potential conicts of interest were reported . references tsimberidou am , iskander ng , hong ds , et al : personalized medicine in a phase i clinical trials program : the md anderson cancer center initiative . 
massard c , michiels s , fert e c , et al : high - throughput genomics and clinical outcome in hard - to - treat advanced cancers : results of the moscato 01 trial . 
cancer discov 7 : 586 - 595 , 2017 radovich m , kiel pj , nance sm , et al : clinical benet of a precision medicine - based approach for guiding treatment of refractory cancers . 
cancer res 76 : 3690 - 3701 , 2016 jardim dl , schwaederle m , wei c , et al : impact of a biomarker - based strategy on oncology drug development : a meta - analysis of clinical trials leading to fda approval . 
j natl cancer inst 107 : djv253 , 2015 schwaederle m , zhao m , lee jj , et al : impact of precision medicine in diverse cancers : a meta - analysis of phase ii clinical trials . 
j clin oncol 33 : 3817 - 3825 , 2015 schwaederle m , zhao m , lee jj , et al : association of biomarker - based treatment strategies with response rates and progression - free survival in refractory malignant neoplasms : a meta - analysis . 
singh rr , patel kp , routbort mj , et al : clinical validation of a next - generation sequencing screen for mutational hotspots in 46 cancer - related genes . 
singh rr , patel kp , routbort mj , et al : clinical massively parallel next - generation sequencing analysis of 409 cancer - related genes for mutations and copy number variations in solid tumours . 
bartley an , luthra r , saraiya ds , et al : identication of cancer patients with lynch syndrome : clinically signicant discordances and problems in tissue - based mismatch repair testing . 
cancer prev res ( phila ) 5 : 320 - 327 , 2012 johnson a , zeng j , bailey am , et al : the right drugs at the right time for the right patient : the md anderson precision oncology decision support platfordrug discov today 20 : 1433 - 1438 , 2015 15 . 
liang h , cheung lw , li j , et al : whole - exome sequencing combined with functional genomics reveals novel candidate driver cancer genes in endometrial cancer . genome res 22 : 2120 - 2129 , 2012 33 : 2753 - 2762 , 2015 18 . 
andr e f , bachelot t , commo f , et al : comparative genomic hybridisation array and dna sequencing to direct treatment of metastatic breast cancer : a multicentre , prospective trial ( safir01 / unicancer )  . 
hyman dm , piha - paul sa , rodon j , et al : neratinib for erbb2 mutant , her2 non - amplied , metastatic breast cancer : preliminary analysis from a multicenter , open - label , multi - histology phase ii basket trial . 
 t clinical benet of larger ngs panels assessed for eligibility ( n = 675 ) excluded ( n = 101 ) died before testing declined to return to the institution for treatment insufficient tissue for testing ngs testing ( n = 574 ) final analysis ( n = 521 ) excluded ( n = 53 ) no death within 6 months follow - up < 6 months cms46 / 50 testing ( n = 507 ) without cms46 / 50 ( n = 14 ) no actionable gene found ( n = 371 ) actionable gene found , then progression ( n = 78 ) actionable gene found , no progression ( n = 58 ) cms400 testing ( n = 507 ) no actionable genes in cms400 that are not identified in cms46 / 50 ( n = 301 ) no actionable gene identified in cms400 ( n = 6 ) cms400 testing ( n = 14 ) 1 actionable gene in cms400 not identified in cms46 / 50 ( n = 206 ) no additional actionable gene identified in cms400 ( n = 307 ) 1 actionable gene identified in cms400 ( n = 8 ) 1 actionable gene in cms400 not in previous panel ( n = 214 ) matched therapy ( n = 40 ) nonmatched therapy ( n = 108 ) no therapy ( n = 66 ) fig a2 . 
summary of the turnaround time ( in days ) for large panel next - generation sequencing testing to be nalized once tissue was received by the clinical molecular diagnostics lab . 
we then used polymerase chain reaction to quantify gene expression in diagnostic biopsy tissue across a prospectively designed archival cohort of 754 consecutive thinand intermediate - thickness primary cutaneous melanomas . 
a penalized maximum likelihood estimation algorithm was used to train logistic regression models in a repeated cross - validation scheme to predict the presence of sln metastasis from molecular , clinical , and histologic variables . results expression of genes with roles in epithelial - to - mesenchymal transition ( glia - derived nexin , growth differentiation factor 15 , integrin - 3 , interleukin 8 , lysyl oxidase homolog 4 , transforming growth factorreceptor type 1 , and tissue - type plasminogen activator ) and melanosome function ( melanoma antigen recognized by t cells 1 ) were associated with sln metastasis . 
per current guidelines ( table 1 ) , slnb is not recommended if the risk of nodal metastasis is , 5% , as in melanoma with a breslow thickness of , 0.8 mm and no adverse features . 
the key objective of this study was to identify primary melanoma clinicopathologic ( cp ) variables and a gene expression prole ( gep ) that associate with a low risk of sln metastasis . knowledge generated cp variables in combination with an eight - gene gep tied to epithelial - to - mesenchymal transition as a biologic process inherent to metastasis effectively stratied melanoma according to its likelihood of sln metastasis . relevance our cp - gep model promises to work as an sln biopsy reduction tool . 
10% risk of shortand long - term complications , including bleeding , infection , lymphocele , lymphatic stula , pain , neuropathy , and lymphedema , 7 as well as an up to 5% risk of hospital readmission within 30 days because of postsurgical complications.8 better methods are needed to identify patients whose risk of nodal metastasis is so low that they may safely forgo slnb . 
here , we report the design of a model that combines established clinicopathologic ( cp ) variables with a gene expression prole ( gep ) to identify patients who have , on average , a risk of nodal metastasis of , 5% . 
of the 754 patients in this cohort , 373 were included in a previously published cohort.10 all specimens were analyzed by quantitative polymerase chain reaction ( pcr ) between february 2018 and october 2018 . eligibility was determined on the basis of histopathology data derived from patient medical records and established by two or more board - certied mayo clinic dermatopathologists . inclusion was determined by the ajcc 7th edition on the basis of institutional practice guidelines of the mayo clinic for recommending slnb , which were based on breslow thickness , ulceration , mitoses , and age . 
 molecular model to assess sentinel lymph node metastasis risk exclusion criteria were m1 disease within 90 days of primary diagnosis ; insufcient primary tumor diagnostic biopsy tissue ; inadequate rna harvested ; and , for minnesota , denial of access to medical records for research purposes ( per minnesota state law )  . 
because there is an ongoing debate about the relevance of , 0.1 mm metastasis in sln ( ie , isolated tumor cells [ itcs ] and cell clusters , 0.1 mm in diameter ) , patients with , 0.1 mm metastasis were excluded from model development . 
isolated benign melanocytes and histiocytic melanophages can be present elsewhere in the sln and mimic itcs.13 some authors cautioned against hidden tumor burden in , 0.1 mm metastatic sln and highlighted the need for enhanced pathology assessment protocols.14 , 15 others found that , 0.1 mm metastasis has no impact on prognosis compared with negative slns.16 , 17 enrollment of patients and inclusion and exclusion criteria are summarized in appendix figure a1 . 
this study was approved by the mayo clinic institutional review board . gene expression by quantitative pcr see the appendix for details . statistical methods logistic regression and least absolute shrinkage and selection operator . 
features with a tolerance 0.15 were removed from the input data set ( the tolerance represents the fraction of variance in the kth feature that cannot be accounted for by other features )  . 
the output of logistic regression models estimated the probability of sln metastasis and was converted into binary results : samples with a probability of metastasis greater than the cutoff were classied as positive , whereas samples with a probability lower than the cutoff were classied as negative . 
the performance metrics of the classiers are listed in appendix table a2 and are cutoff specic , except the area under the receiver operating characteristic curve ( auc )  . double - loop cross - validation . 
however , splitting the available data just once into a training set and a test set may be viewed as inefcient.19 a better solution is to estimate the average performance of the model by repeated cross - validation or bootstrapping . 
here , we opted for a repeated crossvalidation scheme ( ie , double - loop cross - validation [ dlcv ] ) .20 the key idea of dlcv is to get a reliable estimate of the outof - sample performance of a classier by averaging the performance of multiple classiers trained in cross - validation a number of times ( appendix fig a2 )  . 
see the appendix for details . memorial sloan kettering cancer center nomograsee the appendix for details . results epithelial - to - mesenchymal transition in high - risk melanoma to identify candidate genes tied to biologic processes inherent to metastasis and differentially expressed between metastatic and nonmetastatic melanoma , we rst reviewed rna sequencing data obtained previously.10 genes with a false discovery rate of , 0.01 in a comparison of either benign nevi and cutaneous melanoma or cutaneous melanoma with and without sln metastasis were selected for further qualication . 
a total of 194 candidate biomarkers and 3 control genes were screened for performance in breslow thickness and age - matched case - control studies by quantitative pcr ( appendix table a3 )  . 
we noted that genes predictive of nodal metastasis had been associated with epithelial - to - mesenchymal transition ( emt ) , a biologic process known to promote metastasis in primary cutaneous melanoma.21 our prospectively designed archival cohort22 comprised 754 patients with thinand intermediate - thickness primary cutaneous melanoma who underwent an slnb within 90 days of diagnosis ( table 2 )  . 
of 754 patients , 128 ( 17% ) were sln positive , in agreement with the typical prevalence in an slnb - eligible population.3 our approach was to develop models of the likelihood of sln metastasis on the basis of either cp variables ( cp models ) or geps of the primary tumor ( gep models ) and then to assess the performance of a combined model of cp and gep factors ( cpgep models )  . 
 ( % ) characteristic other mixed not documented negative ( n = 626 ) positive ( n = 128 ) 4 of 626 ( 0.6 ) 6 of 626 ( 1.0 ) 31 of 626 ( 5.0 ) 2 of 128 ( 1.6 ) 6 of 128 ( 4.7 ) abbreviations : sd , standard deviation ; slnb , sentinel lymph node biopsy . acomparisons of patients with slnb - negative and - positive outcomes were performed using the 2 test for categorical variables , the twosample t test for patient age , and the wilcoxon rank sum test for all other variables . using gene expression to predict sln metastasis dlcv and lasso were used to identify a gep dened from 11 genes that differentiated the patients with and without nodal metastasis detected by slnb within 90 days of primary diagnosis : adam metallopeptidase domain 12 ( adam12 ) , interleukin 8 ( cxcl8 ) , growth differentiation factor 15 ( gdf15 ) , integrin - 3 ( itgb3 ) , galectin 1 ( lgals1 ) , lysyl oxidase like 4 ( loxl4 ) , melanoma antigen recognized by t cells 1 ( mlana ) , tissue - type plasminogen activator ( plat ) , protein kinase c ( prkcb ) , glia - derived nexin ( serpine2 ) , and transforming growth factor ( tgf ) receptor 1 ( tgfbr1 )  . 
finally , logistic regression modeling was used to develop a novel model combining cp factors ( ie , breslow thickness and patient age ) and a gep . the combined cp - gep model was based on the expression of mlana , a melanosome marker , 23 and seven genes functionally linked to emt and with specic roles in angiogenesis / hypoxia and coagulation : gdf15 , 24 - 26 cxcl8 , 27 , 28 loxl4 , 29 , 30 tgfbr1 , 31 , 32 itgb3 , 33 - 36 plat , 37 , 38 and serpine239 , 40 ( table 3 )  . 
the cp - gep model , therefore , promised to work as an slnb reduction tool : patients with a negative test may forgo slnb because their risk of nodal metastasis is , on average , , 5% , a reduction from the pre - test probability41 ( table 1 )  . for a predictor of sln status to be clinically relevant , it must change the pretest probability within each t category of melanoma . 
the high slnb reduction rate for t1b melanoma is particularly meaningful in light of the increasing incidence of thinner melanoma , 42 for which cp variables are less predictive.5 to further dene the clinical relevance of the cp - gep model , we compared cp - gep performance to the wellknown memorial sloan kettering cancer center ( mskcc ) nomogram for predicting sln metastasis . 
shown are the models that are based on the mskcc nomogram , clinicopathologic variables ( cp model ) , and gene expression prole ( gep ) and cp variables combined ( cp - gep model )  . 
curves are averages over 100 repeats obtained by concatenating the threefold crossvalidation test results . that the mskcc nomogram performed similarly to the cp model but was outperformed by the cp - gep model in auc ( appendix fig a5 ) and slnb reduction rate ( fig 2 )  . discussion while completion lymphadenectomy for which slnb was a key determinant has fallen out of favor , 43 , 44 slnb continues to determine patient eligibility for adjuvant therapy . unfortunately , the majority of slnb procedures performed today are negative , which conrms only the low - risk nature of the primary tumor without inuencing decision making toward adjuvant therapy . 
here , we present a model that considers gene expression and cp variables ( ie , breslow thickness and patient age ) to assess the likelihood of sln metastasis in patients diagnosed with thinand intermediate - thickness primary cutaneous melanoma . 
the ability to characterize melanoma at the molecular level reduces the need for slnb , a surgical procedure that carries a risk of complications.7 our approach of combining cp factors with molecular proling better identies patients who may forgo the slnb procedure because of their low risk of metastasis . for melanoma with a 5% - 10% chance of sln metastasis ( breslow thickness , 0.8 - 1 mm ) , slnb is optional but should be discussed with the patient.45 even though slnb in this risk group is optional ,  . 
50% of affected patients in the united states undergo slnb.46 the majority of these patients have negative slnb ndings , which highlights our current dilemma with melanoma risk stratication and the limitations of histopathology alone as a predictor of regional metastasis . 
multivariable models have used breslow thickness , tumor ulceration , and patient age to predict sln status , with age being a negative predictor and breslow thickness as well as tumor ulceration being strong positive predictors.47 - 50 angiolymphatic invasion was also found to positively correlate with sln metastasis in some models.5 , 51 the most ambitious cp models , such as those developed from a large bi - institutional series , achieved slnb reduction rates of 18% - 30% , with a negative predictive value table 4 . 
in comparison , the cp plus molecular model developed here showed an slnb reduction rate of 42% at a negative predictive value of 96% ( appendix table a4 )  . 
there seems to be a clear limit in the ability of cp factors to predict sln metastasis . to improve the performance of predictive models , we developed a gep from primary diagnostic biopsy tissue . gep has been used successfully in breast cancer to individualize therapy.52 previous research on gene expression in invasive breast cancer , 53 prostate cancer , 54 colon cancer , 55 melanoma , 10 and other solid cancers56 has consistently demonstrated the upregulation of adhesion receptors and secreted factors that remodel the tumor microenvironment and are involved in emt.10 , 53 - 57 here , we have conrmed this upregulation and found genes involved in emt with specic roles in angiogenesis ( growth differentiation factor 15 , 25 interleukin 8 , 28 lysyl oxidase homolog 4 , 58 tgfreceptor type 1 , 32 and integrin 334 ) and coagulation ( tissue - type plasminogen activator , 38 and gliaderived nexin40 ) as well as the melanosome biogenesis marker melanoma antigen recognized by t cells 123 to be associated with sln metastasis ( table 3 )  . 
the functional roles of these genes have been demonstrated by genetic approaches32 , 34 , 38 , 59 and pharmacologic efcacy studies where the inhibition of integrin - 3 by cyclic peptide , 60 tgfreceptor type 1 by kinase inhibitor , 61 and interleukin 8 by neutralizing antibody62 reduced tumor angiogenesis , tumor growth , and metastasis . 
tumor vascularity in melanoma diagnostic biopsy tissue is well known to associate with nodal and distant metastasis but has been difcult quantify in the past.63 likewise , constitutive brinolytic activity in tumor tissue has been described as early as 191164 and attributed largely to plasminogen activators38 and other serine proteases , such as glia - derived nexin , 65 which promote metastasis , 66 disseminated intravascular coagulation , and bleeding in patients with metastatic cancer.67 a drawback of the simultaneous selection of cp variables and genes by our feature selection algorithm is the absence of established variables easily recognizable by clinicians , such as ulceration , in the cp - gep model . 
moreover , we excluded t4 lesions ( ie , melanoma with a breslow thickness , 4 mm ) because the pretest probability of regional metastasis for these patients is very high . 
for example , 21 ( 70% ) of 30 patients with t4 lesions in our cohort presented with regional metastasis , which is well above the recommend threshold for recommending slnb . 
finally , eligibility of patients with t1 melanoma was determined by the mayo clinic institutional practice guidelines for recommending slnb , which select for higher - risk patients , such as those , 40 years of age and with t1b melanoma . 
however , slnb to slnb metastasis risk was only , 5% if cohorts were enriched for a priori low - risk cases , such as by including t1a melanoma or restricting the analysis to patients  . 
previous attempts to develop molecular risk factors have been limited by small cohort sizes , incomplete tnm staging data , or limited clinical utility of the resulting models.49 , 69 , 70 our approach of combining cp factors and gene expression variables improved the performance of cp factors alone by outperforming current clinical practice and important benchmarks , such as the mskcc nomograthe combined cp - gep model maintained an average negative predictive value of  . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . domenico bellomo employment : skylinedx stock and other ownership interests : synlogic , skylinedx patents , royalties , other intellectual property : gene signatures for predicting metastasis of melanoma julia s . 
van vliet employment : skylinedx stock and other ownership interests : skylinedx patents , royalties , other intellectual property : named inventor on patents in the multiple myeloma eld jvalini dwarkasing employment : skylinedx stock and other ownership interests : skylinedx alexander meves research funding : skylinedx patents , royalties , other intellectual property : mayo clinic has led several patent applications on which i am listed as an inventor ; technologies are in the area of wound healing and skin cancer ( inst ) open payments link : 478139 no other potential conicts of interest were reported . acknowledgment we thank vera j . 
simon , and the mayo clinic gene expression core facility for excellent technical assistance . references saranga - perry v , ambe c , zager js , et al : recent developments in the medical and surgical treatment of melanoma . 
ca cancer j clin 64 : 171 - 185 , 2014 chang jm , kosiorek he , dueck ac , et al : stratifying sln incidence in intermediate thickness melanoma patients . 
n engl j med 370 : 599 - 609 , 2014 gershenwald je , scolyer ra , hess kr , et al : melanoma staging : evidence - based changes in the american joint committee on cancer eighth edition cancer staging manual . 
hieken tj , grotz te , comfere ni , et al : the effect of the ajcc 7th edition change in t1 melanoma substaging on national utilization and outcomes of sentinel lymph node biopsy for thin melanoma . 
eur j surg oncol 43 : 270 - 277 , 2017 ascha m , ascha ms , gastman b : identication of risk factors in lymphatic surgeries for melanoma : a national surgical quality improvement program review . 
ann plast surg 79 : 509 - 515 , 2017 oude ophuis cmc , verhoef c , rutkowski p , et al : the interval between primary melanoma excision and sentinel node biopsy is not associated with survival in sentinel node positive patients an eortc melanoma group study . 
fahy as , grotz te , keeney gl , et al : frozen section analysis of slns in trunk and extremity melanoma has a high false negative rate but can spare some patients 13 . 
mahmood mn , lee mw , linden md , et al : diagnostic value of hmb - 45 and anti - melan a staining of sentinel lymph nodes with isolated positive cells . 
murali r , desilva c , mccarthy sw , et al : sentinel lymph nodes containing very small ( , 0.1 mm ) deposits of metastatic melanoma cannot be safely regarded as 33 : 2509 - 2515 , 2015 121 : 1628 - 1636 , 2015 a second operation . 
ann surg oncol 15 : 1547 - 1548 , 2008 van akkooi ac , de wilt jh , verhoef c , et al : clinical relevance of melanoma micrometastases ( , 0.1 mm ) in sentinel nodes : are these nodes to be considered negative ? ann oncol 17 : 1578 - 1585 , 2006 18 . 
alonso sr , tracey l , ortiz p , et al : a high - throughput study in melanoma identies epithelial - mesenchymal transition as a major determinant of metastasis . epidemiol 54 : 774 - 781 , 2001 21 : 3755 - 3762 , 2005 cancer res 67 : 3450 - 3460 , 2007 22 . 
subramanian j , simon r : what should physicians look for in evaluating prognostic gene - expression signatures ? nat rev clin oncol 7 : 327 - 334 , 2010 23 . 
hoashi t , watabe h , muller j , et al : mart - 1 is required for the function of the melanosomal matrix protein pmel17 / gp100 and the maturation of melanosomes . 
mullican se , lin - schmidt x , chin cn , et al : gfral is the receptor for gdf15 and the ligand promotes weight loss in mice and nonhuman primates . 
fernando ri , castillo md , litzinger m , et al : il - 8 signaling plays a critical role in the epithelial - mesenchymal transition of human carcinoma cells . 
yang j , shultz rw , mars wm , et al : disruption of tissue - type plasminogen activator gene in mice reduces renal interstitial brosis in obstructive nephropathy . j clin invest 110 : 1525 - 1538 , 2002 38 . 
mocellin s , thompson jf , pasquali s , et al : sentinel node status prediction by four statistical models : results from a large bi - institutional series ( n = 1132 )  . 
wong sl , faries mb , kennedy eb , et al : sentinel lymph node biopsy and management of regional lymph nodes in melanoma : american society of clinical oncology and society of surgical oncology clinical practice guideline update . 
hayek sa , munoz a , dove jt , et al : hospital - based study of compliance with nccn guidelines and predictive factors of sentinel lymph node biopsy in the setting of thin melanoma using the national cancer database . 
kather jn , charoentong p , zoernig i , et al : prognostic value of histopathological tumor - stroma ratio and a stromal gene expression signature in human solid tumors . 
nat rev cancer 18 : 533 - 548 , 2018 [ erratum : nat rev cancer 19 : 179 , 2019 ] jiang wp , sima zh , wang hc , et al : identication of the involvement of loxl4 in generation of keratocystic odontogenic tumors by rna - seq analysis . 
zhang m , kleber s , r ohrich m , et al : blockade of tgfsignaling by the tgfr - i kinase inhibitor ly2109761 enhances radiation response and prolongs clin cancer res 11 : 6270 - 6279 , 2005 survival in glioblastoma . 
huang s , mills l , mian b , et al : fully humanized neutralizing antibodies to interleukin - 8 ( abx - il8 ) inhibit angiogenesis , tumor growth , and metastasis of human 63 . 
boulaftali y , ho - tin - noe b , pena a , et al : platelet protease nexin - 1 , a serpin that strongly inuences brinolysis and thrombolysis . 
 molecular model to assess sentinel lymph node metastasis risk appendix methods quantitative polymerase chain reaction ( pcr ) was performed as previously described.10 rna purication was from formalin - xed parafn - embedded tissue ( qiagen , hilden , germany )  . 
gene expression was corrected by the mean of housekeeping genes ( rlp0 , rlp8 , and - actin ) using the ct method . statistical methods double - loop cross - validation . 
in the inner loop ( 10 - fold cross - validation ) , we optimized the parameter by determining the number of features ( ie , the weight of the least absolute shrinkage and selection operator penalty term ) , and in the outer loop ( threefold cross - validation ) , we designed a classier on the training set ( two of the three folds )  . 
next , we assessed the performance of the trained classier on the remaining fold ( test set ) , with the parameter xed to the value estimated in the training set . 
the nal classiers were trained on the entire data set using the average ? parameter over 300 runs . memorial sloan kettering cancer center nomograthe majority of online tools for melanoma provide prognostic information47 ( zabor et al : ann surg oncol 25 : 2172 - 2177 , 2018 )  . 
the memorial sloan kettering cancer center ( mskcc ) nomogram , in contrast , is a tool specically designed to predict the probability of primary cutaneous melanoma metastasis to sln.23 the nomogram corresponds to a logistic regression model that is based on ve clinicopathologic variables : age ( range , 20 - 95 years ) , breslow thickness ( range , 0.1 - 10 mm ) , clark level ( ii , iii , iv , or v ) , biopsy location ( trunk , extremity , or head and neck ) , and tumor ulceration ( yes or no )  . 
while attempting to apply the nomogram to our cohort , we could not calculate the probability of sln metastasis for 16 patients because of missing values or because the values were outside the allowable range for the nomograsix patients were , 20 years of age , seven had a missing clark level ( one of whom was also , 20 years of age ) , and four did not have ulceration status available . 
study ow diagrathe gure depicts the enrollment of patients , inclusion and exclusion criteria , and other potential sources of retrospective bias such as the absence of research consent , the unavailability of tissue for molecular analysis , or failed gene expression proling ( gep )  . 
 molecular model to assess sentinel lymph node metastasis risk x 10 cvs x 100 repeats x 3 cvs train train test train test train average test performance test train train select optimal for lasso penalty fig a2 . 
the dlcv consists of two nested cross - validation loops : in the inner loop ( tenfold cross - validation ) , we estimate the optimal parameter , namely , the weight of the lasso penalty term ( ie , optimal feature selection ) ; in the outer loop ( threefold cross - validation ) , we assess the performance of the classier on each test set , with the parameter as determined in the training set . 
moreover , in each training set of the outer loop , we choose and x an operating point on the receiver operating characteristic curve , and we assess the performance of the classier at that operating point in the corresponding test set . 
the cross - validation procedure has been repeated 100 times , and unless otherwise stated , we reported the average performance over 300 test sets ( three test sets per outer loop , repeated 100 times )  . 
lasso , least absolute shrinkage and selection operator . cp1 ; auc , 0.78 cp2 ; auc , 0.78 cp3 ; auc , 0.78 cp4 ; auc , 0.77 cp5 ; auc , 0.77 cp6 ; auc , 0.77 false - positive rate fig a3 . 
 bellomo et al cp model ; auc , 0.78 gep model ; auc , 0.78 combined cp - gep model ; auc , 0.82 false - positive rate fig a4 . 
blue line , model for predicting sentinel based on cp variables ( cp model ) ; red line , model based on gene expression prole ( gep model ) ; teal line , model based on combined gep and cp variables ( cp - gep model )  . 
curves are averages over 300 double loop crossvalidationgenerated test sets . mskcc nomogram ; auc , 0.77 cp model ; auc , 0.78 combined cp - gep model ; auc , 0.82 false - positive rate fig a5 . 
orange line , model based on mskcc nomogram ; blue line , model based on cp variables ( cp model ) ; teal line , model based on gene expression and cp variables combined ( cp - gep model )  . 
clinicopathologic variables available for statistical modeling clinicopathologic variable age categorical biopsy location biopsy location mskcc breslow thickness breslow thickness categorical mitotic rate categorical clark level ulceration regression tumor - inltrating lymphocytes microsatellitosis angiolymphatic invasion histology type abbreviation : mskcc , memorial sloan kettering cancer center . head and neck , trunk , upper extremity , lower extremity , acral value female , male years 15 - 39 years , 40 - 59 years , 60 years head and neck , trunk , extremity millimeters , 1 mm , 1 - 2 mm , 2 - 4 mm 0 / mm2 , 1 - 6 / mm2 ,  . 
6 / mm2 , not determined ii , iii , iv , v yes , no , not determined yes , no , not determined absent , nonbrisk , brisk , not determined yes , no , not determined yes , no , not determined supercial spreading , nodular , desmoplastic , lentigo maligna , acral lentiginous , spindled , dermal , spitzoid , nevoid , unclassied , other , mixed , not determined table a2 . 
average performance of the cp , gep , and combined cp - gep models were trained in double - loop cross - validation 300 times . performance is shown for the 754 - patient cohort assembled on the basis of inclusion criteria and devoid of patients with equivocal sln metastasis ( ie , patients with , 0.1 mm metastatic disease )  . 
 year 1 in the molecular era of pediatric brain tumor diagnosis : application of universal clinical targeted sequencing in an unselected cohort of children purpose next - generation sequencing is gaining acceptance as a clinical tool to aid diagnosis and guide treatment of pediatric cancer . 
here , we report an unselected prospective cohort study to evaluate the clinical use of universal targeted sequencing in pediatric patients with brain tumors . methods we applied a universal sequencing protocol for all tumors of the cns undergoing diagnostic workup at seattle childrens hospital during the study period of november 2015 to november 2016 . 
all tumors were sequenced using the uw - oncoplex platform , which is a multiplexed targeted deep gene sequencing panel that detects genetic alterations in 262 cancer - related genes performed in a college of american pathologists accredited clinical laboratory improvements amendmentscertified laboratory . results eighty - eight patients underwent diagnostic evaluation during the study period , of which 85 tumors ( 95% ) yielded sufficient dna for sequencing , including 59 newly diagnosed and 26 relapsed . 
of these , 57 ( 67% ) had disease - defining or disease - modifying mutations , 44 ( 52% ) had potentially targetable mutations , and 31 ( 36% ) had mutations requiring germline follow - up . 
2018 by american society of clinical oncology introduction high - throughput genomic and epigenomic technologies have recently been used to thoroughly describe the genomic landscape of pediatric brain tumors.1 - 3 this work has transformed our understanding of the molecular basis of these diseases , 4 which are the leading cause of pediatric cancer death.5 the current challenge for the field of pediatric neuro - oncology is to translate this knowledge into clinical practice . the 2016 revision of the who classification of cns tumors has begun to incorporate molecular findings into tumor diagnosis in addition to traditional histopathology.6 however , there is currently no consensus regarding best - practice diagnostics for routine clinical practice . 
recently , a few institutions have reported the use of clinically validated next generation sequencing ( ngs ) panels to identify molecular alterations in selected subsets of pediatric patients with brain tumors.7 - 10 these studies demonstrated that molecular profiling is bonnie l . 
atrt , atypical teratoid rhabdoid tumor ; dnet , dysembryoplastic neuroepithelial tumor ; etmr , embryonal tumor with multilayer rosettes ; gg , ganglioglioma ; nos , not otherwise specified ; pxa , pleomorphic xanthoastrocytoma . feasible and that clinically relevant genetic alterations may be identified . methods instability the uw - oncoplex version 5 test is a multiplex gene sequencing panel used to detect alterations in 262 cancer - related genes , including single nucleotide variants , small insertions or deletions , amplifications , selected translocations , and microsatellite ( washington.edu / tests / genetics / uw - oncoplex )  . 
in a retrospective pilot study using this test , sequencing identified a large proportion of targetable mutations in high - grade supratentorial tumors.11 we hypothesized that the use of a selected or convenience cohort in our retrospective pilot as well as all prior studies may have identified a higher proportion of actionable findings that would not necessarily be applicable to the wider population of all patients undergoing pathologic diagnosis of pediatric brain tumor.7 - 12 we designed this follow - up , prospective , unselected cohort study to evaluate the feasibility and impact of the universal application of molecular tumor testing on routine pediatric brain tumor diagnosis and to also assess how molecular results may alter medical management . all tumors of the cns undergoing diagnostic evaluation at seattle childrens hospital from november 2015 to november 2016 were included in this study . 
details of the laboratory workflow and methods are included in the data supplement . results demographics and sample characteristics we identified 88 patients who met the clinical and diagnostic inclusion criteria ( fig 1 )  . 
 of these , 97% ( 85 of 88 ) had sufficient dna obtained for sequencing , and only three patients did not have adequate tissue in formalin - fixed paraffin - embedded ( ffpe ) blocks to perform ngs . 
of patients ( % ) * targeted agent braf inhibitor mek inhibitor fgfr inhibitor braf v600e , brafpa598t599insv ganglioglioma , pleomorphic xanthoastrocytoma , pilocytic astrocytoma , desmoplastic infantile ganglioglioma / astrocytoma kiaa1549 - braf fusion , nf1 mutations and deletions , ptpn11 mutation pilocytic astrocytoma , anaplastic astrocytoma , pleomorphic xanthoastocytoma fgfr1 mutations and duplication , fgfr3 fusions pilocytic astrocytoma , dysembryoplastic neuroepithelial tumor , diffuse astrocytoma , ganglioglioma mtor pathway inhibitor mtor , fbxw7 diffuse midline glioma , medulloblastoma smo inhibitor ptch1 mutations medulloblastoma pd1 / pdl1 inhibitor biallelic msh2 loss , pms2 mutation with loh anaplastic astrocytoma , medulloblastoma pdgfra inhibitor pdgfra amplification diffuse midline glioma met inhibitor kit inhibitor met amplification kit amplification diffuse midline glioma diffuse midline glioma cdk4 / 6 inhibitor cdk4 amplification glioblastoma ezh2 inhibitor loss of smarcb1 atypical teratoid rhabdoid tumor * ten patients had more than one targetable mutation in their tumors . 10 ( 12 ) 18 ( 21 ) 10 ( 12 ) 3 ( 4 ) 3 ( 4 ) 2 ( 2 ) 2 ( 2 ) 2 ( 2 ) 2 ( 2 ) 1 ( 1 ) 1 ( 1 ) were sequenced , including 59 newly diagnosed tumors and 15 tumors from patients with a radiologic relapse during the time of this study . 
 eleven additional patients had sequencing of newly resected recurrent tumors . patients were a median age of 10 years ( range , 3 months to 22 years ) and 49% female ( 42 of 85 )  . 
medical history included only three patients with previously known cancer predisposition syndrome ; two patients had neurofibromatosis type 1 and one had neurofibromatosis type 2 . genetic results the average depth of sequencing coverage was 441 ( range , 102 to 1 , 112 )  . 
five reports with turnaround times of > 60 days were from patients with minimal tissue that required cutting additional ffpe sections with subsequent repeat dna extraction . genetic result details are shown in data supplement 1 , and criteria for tiers of alterations are listed in appendix table a1 . 
genetic alterations were found to be disease defining or modifying in 67% ( n = 57 ) , targetable with an available therapeutic drug in 52% ( n = 44 ; table 1 ) , and potentially germline associated with cancer predisposition in 36% ( n = 31 )  . 
as of the last follow - up , seven patients ( 8% of total , 16% of those with an identified molecular target ) had been prescribed targeted agents ; molecularly targeted agents were obtained through insurance - approved off - label use in five patients and through enrollment in a clinical trial in two patients . analysis of tumor subtypes tumors were analyzed separately as high - grade glioma ( hgg ) , low - grade glioma ( lgg ) , medulloblastoma , and other rare pediatric cns tumors . 
 medulloblastoma ngs results were correlated with traditional histology , immunohistochemistry , and fluorescence in situ hybridization studies.6 , 13 all 20 medulloblastomas were able to be classified into subgroups as defined by the who , 6 , 14 including a wingless ( wnt ; n = 1 ) , sonic hedgehog ( shh ; n = 7 ) , or non - wnt / non - shh group ( n = 12 ; fig 3 )  . 
for example , one patient with a wnt pathway medulloblastoma had only weak nuclear beta catenin staining ; in this patient , the finding of a ctnnb1 mutation and copy loss consistent with monosomy 6 by ngs helped place this tumor firmly in the wnt - activated subgroup . 
in another instance , an shh group medulloblastoma that was gab1 immunopositive displayed ambiguous p53 immunohistochemical staining of approximately 40% of tumor cell nuclei ; ngs not only confirmed the shh subgroup by finding sufu mutations , but also confirmed that this tumor contained a tp53 mutation . 
as of the last follow - up , two patients in the relapsed shh group with ptch1 mutations had been prescribed smo inhibitors , one of whom experienced a partial response to treatment . forty - four lggs were analyzed ( fig 4 )  . 
 a , high - grade astrocytoma ; aa , anaplastic astrocytoma ; apa , anaplastic pilocytic astrocytoma ; dipg , diffuse intrinsic pontine glioma ; gbm , glioblastoma ; hgg , high - grade glioma , not otherwise specified . pik3ca pten smarcb1 msh2 idh1 pdgfra h3f3a atrx cdk6 cdkn2a tp53 ptpn11 v600 mutations and 10 braf - kiaa translocations . 
 twenty - nine patients with lgg had targetable mutations , and at the last follow - up , three patients had been prescribed targeted therapy with a braf inhibitor for braf v600e mutation , two at the time of recurrence and one as initial therapy for unresectable brainstem tumor . 
 three patients with lgg were confirmed to have germline mutations , including the two known patients with nf1 and one patient with a recurrent pleomorphic xanthoastrocytoma who was confirmed to have a germline tp53 mutation in addition to a braf v600e mutation in the tumor ; the patient was treated with a braf inhibitor instead of radiation for recurrent tumor and continues without disease progression with > 12 months of receiving targeted therapy . 
molecular profiling did not alter treatment of the 17 patients in the lgg group with completely resected primary tumors . eleven other uncommon tumors were evaluated ( fig 5 ) , including six nonmedulloblastoma embryonal tumors , choroid plexus carcinoma , choroid plexus papilloma , vestibular schwannoma , rhabdoid meningioma , and chordoma . 
one patient had a known nf2 mutation , and the other two patients tested negative for smarcb1 ( atypical teratoid rhabdoid tumor ) and tp53 ( choroid plexus carcinoma )  . analysis of primary versus recurrent tumors considering newly diagnosed patients , 85% ( n = 50 of 59 ) had clinically relevant mutations , including disease - defining or disease - modifying mutations in 76% of tumors ( n = 45 ) , targetable mutations in 46% of tumors ( n = 27 ) , and potentially germline mutations in 41% of tumors ( n = 24 )  . of the 15 primary tumors sequenced at the time of radiologic relapse , 10 ( 67% ) were found to have clinically significant molecular alterations considered disease defining , and nine ( 60% ) identified molecular targets for therapy . 
 of 11 tumors sequenced using newly resected tumor obtained at the time of recurrence , clinically significant alterations were identified in eight ( 73% )  . discussion germline sequencing germline dna was not collected at the time of somatic sequencing in this study . 
however , somatic sequencing identified mutations considered to be potentially germline in 31 of 85 of tumor samples ( 36% ) on the basis of variant interpretation , which led to initiation of clinical follow - up and genetic counseling to recommend germline evaluation . 
in this population , germline sequencing has been performed on 13 patients , and germline mutations were confirmed in nine patients ( 75% of those tested ; 10.6% of the study population ) as of the last follow - up . 
 one patient had ctnnb1 mutation with monosomy of chromosome six diagnostic of wingless ( wnt ) subgroup , seven had either ptch1 or sufu mutations characteristic of sonic hedgehog ( shh ) subgroup , and the other 12 were non - shh / nonwnt group ; three of our seven shh group tumors were tp53 mutant . 
in the group of newly diagnosed patients , alterations were identified in 85% of patients ( n = 50 of 59 ) , a finding that was contrary to our hypothesis that selected cohorts previously reported by our group and others may have been limited by a selection bias increasing the likelihood of clinically relevant findings.7 , 8 , 11 , 12 targetable mutations were identified in 44 tumors ( 52% ) , and seven of these patients ( 8% ) have been prescribed targeted therapeutic agents to date . 
this number likely underestimates the longer - term use of targeted therapy because the study has a relatively short follow - up period and there are effective standard treatment regimens of cytotoxic therapy for most diagnoses . 
if successful , the routine use of targeted agents will greatly increase in patients with pediatric brain tumors . the main aims of cancer genomic profiling tests are to identify somatic mutations . 
it is crucial to include genetic counseling in oncology care , ideally with a geneticist or genetic counselor embedded into the pediatric oncology clinic.15 in this study , we identified 31 patients ( 36% ) with potential germline mutations . 
 be difficult to overstate in a patient for whom radiation therapy is being considered , because the long - term second malignancy rate in these patients who undergo therapeutic irradiation approaches 100%.16 molecular profiling is important for the diagnosis and management of pediatric patients with brain tumors , 6 although at present , there are several competing platforms and currently no diagnostic gold standard . 
whatever platform is used must be clinically validated and should balance cost , turnaround time , and ability to identify clinically relevant mutations in small samples , which is no small task . 
 alternatively , many research studies have argued the advantages of potentially subclassifying pediatric brain tumors primarily by rna - based gene expression17 or methylation analyses.18 however , these types of platforms are difficult to establish fig 4 . 
the majority of low - grade gliomas in our series had dysregulated braf signaling , which included 10 ( 26% ) with braf fusions and 10 ( 26% ) with codon 600 mutations ; these alterations were considered both targetable and either disease defining or modifying . 
ag , angiocentric glioma ; da , diffuse astrocytoma ; dig / dia , desmoplastic infantile ganglioglioma or desmoplastic infantile astrocytoma ; dnet , dysembryoplastic neuroepithelial tumor ; ep , ependymoma ; gg , ganglioglioma ; lgg , low - grade glioma , not otherwise specified ; o , oligodendroglioma ; pa , pilocytic astrocytoma ; pma , pilomyxoid astrocytoma ; pxa , pleomorphic xanthoastrocytoma . atrx cdk6 cdkn2a tp53 ptpn11 fgfr3 fgfr1 braf with the degree of reliability that clinical testing requires for use on a single - patient basis , and even if molecular classification was established , expression or methylation analysis might not identify candidates for targeted therapy . 
as an example , although shh pathway medulloblastoma may be reliably identified with immunohistochemistry , 13 nanostring , 17 or methylation profiling , 18 none of these platforms is specific for the site of mutation , which is required for consideration of therapy with a smoothened inhibitor that would be predicted to be effective in ptch1 mutant tumors but unlikely to be effective in the case of downstream alterations , such as gli1 amplification . 
 similarly , braf inhibitor therapy is indicated in braf v600 mutant tumors but contraindicated in braf fusion.19 the detection of fusions such as braf using a dna - based platform such as uw - oncoplex requires the specific inclusion of intronic regions in sequencing . 
alternatively , rna - based sequencing analysis may have an advantage in identifying fusions and splice variants that would be missed on a dnabased platform that does not include intronic sequencing . although 80% of our patients had clinically relevant mutations identified , this means that 20% of tumors sequenced did not have clinically relevant mutations . 
one limitation of this study and other similar studies is that not all known clinically relevant genetic alterations are yet able to be identified on any one clinically validated panel . 
for example , the angiocentric glioma would be expected to have an myb fusion , 20 embryonal tumor with multilayer rosettes would be expected to have mir c19 cluster amplification , 21 and a subset of midline gliomas would be expected to have acvr1 alterations , which are not yet included in this version of the test.22 one advantage of using a targeted sequencing panel is the ability to add and validate targets rapidly with minimal increase in cost . 
however , turnaround time can be shortened with experience , because it is most dependent on clinical interpretation and data generation may be relatively short . another question that our study did not address was the cost comparison between sequential single - gene sequencing in specific diagnostic entities . 
although single - gene testing for the most common variations costs less than a panel , it is not clear that the overall cost of sequential sequencing would be decreased for the population . 
if even a small minority of patients required three - gene testing or subsequent biopsy if tissue were depleted , then there may be a benefit to the population from an initial multiplexed approach . molecular profiling may be particularly useful in patients in whom the histologic diagnosis is unclear . 
 mutations in smarcb1 ( p.p374rfs * 100 ) , bap1 ( p.q392 * ) , pten ( p.g36e ) , nf2 ( p.q319 * ) , and tp53 ( p.r175h ) were all considered both disease defining and potentially germline . 
because only two of our h3f3a k27m mutant diffuse midline gliomas were classic radiologic diffuse intrinsic pontine gliomas , it is important to evaluate for this diagnostic entity whenever a diffuse midline glial neoplasm is encountered . this study provides rigorous evidence regarding the use of routine molecular profiling of an unselected cohort of pediatric brain tumors . 
 on the basis of the analysis presented here , we recommend incorporation of routine molecular profiling into standard clinical practice for all newly diagnosed pediatric hggs , medulloblastomas , and incompletely resected lggs . 
this may be especially important in patients who have undergone stereotactic biopsy in which tumor tissue is severely limited . there was one subgroup in which sequencing did not affect medical care . 
lockwood travel , accommodations , expenses : cambridge healthtech institute shannon stasi no relationship to disclose jeffrey stevens stock and other ownership interests : seattle genetics amy lee no relationship to disclose jeffrey g . 
leary no relationship to disclose acknowledgment we extend our deepest thanks to michael astion , md , medical director of seattle childrens hospital department of laboratories , for his tireless support of this project . 
kool m , korshunov a , remke m , et al : molecular subgroups of medulloblastoma : an international meta - analysis of transcriptome , genetic aberrations , and clinical data of wnt , shh , group 3 , and group 4 medulloblastomas . 
kline cn , joseph nm , grenert jp , et al : targeted next - generation sequencing of pediatric neuro - oncology patients improves diagnosis , identifies pathogenic germline mutations , and directs targeted therapy . 
ramkissoon sh , bandopadhayay p , hwang j , et al : clinical targeted exome - based sequencing in combination with genome - wide copy number profiling : precision medicine analysis of 203 pediatric brain tumors . 
bandopadhayay p , ramkissoon la , jain p , et al : myb - qki rearrangements in angiocentric glioma drive tumorigenicity through a tripartite mechanisnat genet 48 : 273 - 282 , 2016 21 . 
patients with medulloblastoma were subgrouped on the basis of both histology and standard immunohistochemistry methods for beta - catenin ( dako 1 : 200 ) , gab1 ( santa cruz 1 : 100 ) , and p53 ( protein tech 1 : 50 ) .13 the study pathologist estimated the percentage of tumor and selected appropriate formalin - fixed paraffin - embedded ( ffpe ) blocks for testing . 
it was collected at a separate encounter only if a possible deleterious germline mutation was detected that needed to be investigated further . template preparation , gene capture , massively parallel sequencing , and bioinformatics . sequencing was preformed using a clinically validated method performed in a college of american pathologistsaccredited clinical laboratory improvements amendmentscertified laboratory as previously reported ( pritchard et al , j mol diagn 16 : 56 - 67 , 2014 )  . 
sequencing libraries were prepared from dna samples and hybridized to a custom set of complementary rna biotinylated oligonucleotides targeting the exons of 262 genes and select intronic regions , for a total of > 1.4 mb of targeted dna sequenced ( agilent sureselect ; agilent technologies , santa clara , ca )  . 
uw - oncoplex assay version 5 is a targeted , massively parallel gene sequencing assay that detects mutations in 262 cancer - related genes ( washington.edu / uw - oncoplex )  . 
the test uses next - generation deep sequencing to detect mutations , including single nucleotide variants ( snvs ) , insertions and deletions ( indels ) , copy number changes including gene amplifications , selected structural rearrangements such as gene fusions , and microsatellite instability . 
uw - oncoplex was performed on samples from the seattle childrens hospital cohort , as previously described ( pritchard et al , j mol diagn 16 : 56 - 67 , 2014 ; salipante et al , clin chem 60 : 1192 - 1199 , 2014 )  . dna was extracted from ffpe solid tumor tissue samples using the gentra puregene dna isolation kit ( catalog #158489 ; qiagen , valencia , ca )  . 
hematoxylin and eosinstained slides were reviewed before dna extraction for all ffpe samples , and when feasible , macrodissection of tumor - containing regions was performed to enrich tumor cellularity . 
sequencing libraries were constructed from a minimum of 200 ng of dna using kapa hyper prep kits ( kapa biosystems , wilmington , ma ) , and hybridization was performed with custom agilent sureselect probes ( agilent technologies , santa clara , ca )  . 
dna sequencing was performed on a hiseq2500 sequencing system ( illumina , san diego , ca ) with 2 101bp , paired - end reads , and on a nextsequation 500 ( illumina ) with 2 150bp , paired - end reads according to the manufacturers instructions . 
for copy number variation ( cnv ) analysis , copy number states for individual probes were initially called using contra version 2.0.5 ( files ) with reference to a cnv control comprising reads from two independent rounds of library preparation and sequencing of the hapmap individual na12878 . 
adjacent exons were merged into larger segments if the read depths of their component baits were not significantly different ( p > .001 ) by students t test , and read - depth statistics were recalculated for the larger segments . 
filters are applied to exclude variants extremely unlikely to be clinically significant , including variants in intergenic dna , and variants are removed that are present at > 1% frequency in general population databases ( as reported by the exome variant server , 1000 genomes , and the exome aggregation consortium )  . 
variants of interest are subsequently evaluated in conjunction with a combination of multiple external databases ( cosmic , iarc , insight , clinvar ) , literature review ( for newly described mutations ) , and algorithms ( splice prediction tools )  . three separate expert molecular oncology reviewers independently cull data to a list of potentially reportable variants and review quality of data for variant calls by examining genotype quality score metrics , evaluating base call quality , assessing mapping quality , and evaluating other quality assessments as indicated for specific alterations . 
 once the molecular oncology experts agree on a final list of reportable variants , one laboratory director composes a fully customized , formal report that is available in the electronic health record . 
the shh subgroup was initially identified by mutations ( snvs , indels , structural alterations , and copy number alterations ) in ptch1 , smo , sufu , and copy loss for genes on the long arm of chromosome 10 . 
each month , all new patients were systematically reviewed in a presentation format consisting of clinical features and magnetic resonance imaging presented by a neuro - oncologist ( s.e.s.l. ) , histologic findings and photomicrographs by a pediatric pathologist ( b.l.c. ) , molecular results by a molecular pathologist ( c.m.l. ) followed by group discussion . 
the molecular tumor board welcomed rotating trainees from all disciplines and included attendance of trainees from oncology , neurosurgery , pathology , laboratory medicine , medical genetics , and medical students . 
when applicable , a new final integrated diagnosis was reported in the pathology addendum . genetic alterations were considered to be clinically significant as defined by meeting criteria for at least one of the following three categories : ( 1 ) alterations that define a diagnosis or molecular subtype , for example , an activating beta - catenin mutation in wnt - subtype medulloblastoma ; ( 2 ) alterations that identify a proven therapeutic target , such as braf v600e ; and / or ( 3 ) alterations that identify possible deleterious germline mutation associated with cancer predisposition syndrome , such as tp53 . 
with consideration of the variant allele fraction as well as previously described genes associated with cancer predisposition , additional constitutional follow - up testing was recommended for the patients with potential germline mutations , which was coordinated by a genetic counselor . 
 o personalized clinical decision making through implementation of a molecular tumor board : a german single - center experience rouven hoefflin anna - lena geiler ralph fritsch rainer claus julius wehrle patrick metzger meike reiser leman mehmed lisa fauth dieter henrik heiland thalia erbes friedrich stock agnes csanadi cornelius miething britta weddeling frank meiss dagmar von bubnoff christine dierks isabell ge volker brass steffen heeg henning schfer martin boeker justyna rawluk gian kayser simone hettmer hauke busch christoph peters martin werner justus duyster tilman brummer melanie boerries ( continued ) purpose dramatic advances in our understanding of the molecular pathophysiology of cancer , along with a rapidly expanding portfolio of molecular targeted drugs , have led to a paradigm shift toward personalized , biomarker - driven cancer treatment . 
here , we report the 2 - year experience of the comprehensive cancer center freiburg molecular tumor board ( mtb ) , one of the first interdisciplinary molecular tumor conferences established in europe . 
the role of the mtb is to recommend personalized therapy for patients with cancer beyond standard - of - care treatment . methods this retrospective case series includes 198 patients discussed from march 2015 through february 2017 . 
the mtb guided individual molecular diagnostics , assessed evidence of actionability of molecular alterations , and provided therapy recommendations , including approved and off - label treatments as well as available matched clinical trials . results the majority of patients had metastatic solid tumors ( 73.7% ) , mostly progressive ( 77.3% ) after a mean of 2.0 lines of standard treatment . 
 treatment recommendations were implemented in 33 of 104 patients ( 31.7% ) , of whom 19 ( 57.6% ) showed stable disease or partial response , including 14 patients ( 7.1% of the entire population ) receiving off - label treatments . conclusion personalized extended molecular - guided patient care is effective for a small but clinically meaningful proportion of patients in challenging clinical situations . 
2018 by american society of clinical oncology licensed under the creative commons attribution 4.0 license personalized cancer medicine uses molecular biomarkers for standard - of - care treatment stratification , such as activating braf mutations for the treatment of melanoma with braf inhibitors.1 in parallel , it has become evident that therapeutic strategies with targeted drugs are no longer specific for the treatment of distinct entities but rather for particular molecular profiles across different cancers.2 - 4 thus , testing for single - drug targets can provide therapeutic information , but its predictive value may vary between entities . 
although an activating braf v600e mutation will predict response to braf inhibitors in melanoma , 1 it may not do so in colorectal cancers because of epidermal growth factor receptor ( egfr ) feedback activation with requirement of additional egfr targeting.5 , 6 moreover , non - v600 braf mutations might not be responsive to braf inhibition at all.7 thus , one - mutationone - drug approaches may be ineffective , especially in heavily pretreated patients with cancer . 
examples include the selection of ras mutant clones in colorectal cancer treated with egfr antibodies , such as cetuximab or panitumumab , 11 or the acquisition of a secondary egfr t790m kinase domain mutation mediating resistance to egfr kinase inhibitors , such as gefitinib or erlotinib in non small - cell lung cancer.12 , 13 this increasing amount of complexity requires tools to translate individual information into personalized treatment concepts . 
the initial discussion includes a clinical case presentation , review of the pathology data and the tumor - specific genetic landscape , known molecular predictive or prognostic markers , active clinical trials , and potential inand off - label molecular targeted treatments . 
 diagnostic results are presented to the mtb by the molecular pathology and / or the computational biologist teaafter discussion , treatment recommendations are given and are supported by levels of evidence ( data supplement )  . 
these are based on published molecular biomarker recommendations.14 patients and patient informed consent all patients discussed ( n = 198 ) were included in this retrospective single - center case series . 
patients with individual or family history indicative of germline disease - causing mutations were referred to the institute of human genetics for counseling and possibly germline genetic analyses . diagnostic molecular pathology appropriate tissues were subjected to molecular analyses as recommended by the mtb ( fig 1 )  . 
 a molecular diagnostic tests 36 16 immunohistochemistry per case 15 6 ddseq ( exon / hotspot ) hpv testing tngs rna - seq ( total = 867 ) ( total = 492 ) 7 - 8 antibodies ( total = 139 ) type of tngs 48 - gene panel 8 - gene panel brca1 / brca2 54 - gene myeloid panel 1 antibody 2 antibodies 3 antibodies 4 antibodies 5 antibodies 6 antibodies not annotated cosmic ( no hotspot ) hotspot ( not actionable ) actionable ( sensitizing ) actionable ( resistence ) tumor entities brain colorectal melanoma thyroid other gastrointestinal fig 1 . 
 ( a ) the panels depict the type of molecular diagnostic testing performed ( left panel ) and specify the number of immunohistochemical stains ( one to eight antibodies ) per case ( middle panel ) as well as the type of targeted next - generation sequencing ( tngs ) library sequenced ( right panel )  . 
tngs was performed either by a custom panel ( eight - gene panel ) , a 48 - gene panel ( truseq amplicon cancer panel , illumina , san diego , ca ) , a 54 - gene myeloid panel ( trusight myeloid sequencing panel , illumina ) or a custom brca1 / 2 consortium panel . 
differentially expressed genes were identified using the limma voom package from r / bioconductor.34 , 35 results from march 2015 through february 2017 , 49 mtb meetings were attended by a median of 16 physicians and scientists , ensuring continuous interdisciplinary data interpretation and discussions with diagnostic and therapeutic decision making . 
the workflow of the mtb included a case and literature review , molecular diagnostic recommendations , and follow - up discussions of the molecular diagnostic results , including treatment recommendations ( appendix fig a1 )  . 
these included 305 diagnostic and 104 treatment recommendations . patient characteristics the average patient age at the time of the initial mtb presentation was 58 years ( range , 1 to 85 years )  . 
the majority of patients ( n = 146 ; 73.7% ) suffered from metastatic disease , and 77.3% ( n = 153 ) showed disease progression while receiving the standard treatment ( table 2 )  . 
of all diagnostic recommendations , 234 ( 76.7% ) were implemented , resulting in 867 single diagnostic tests ( mean , five per patient ) , including 815 routine molecular tests and 52 extended genetic analyses ( fig 1a , left panel )  . routine molecular diagnostics included immunohistochemical ( ihc ) staining for biomarkers ( n = 492 ; fig 1a , middle panel ) , such as programmed death - ligand 1 ( pd - l1 ) and mismatch repair proteins , in situ hybridizations ( ish ) for gene copy number analyses ( n = 92 ) , and testing for microsatellite instability and / or gene hotspot variations ( n = 89 ) and tngs ( n = 139 ; fig 1a )  . 
the most frequent cosmic annotated sequence variants detected by tngs occurred in tp53 , brca1 , kdr , kit , kras , pik3ca , brca2 , and braf ( fig 1b ; data supplement )  . 
therapeutically relevant mutations in hotspot regions were identified in 41 of 139 patients ( 29.5% ) , including drug - sensitizing variants in braf , pik3ca , idh1 , egfr , and kit , as well as drug resistance variants in kras and nras . extended genetic analyses including exome and transcriptome assays were performed for 36 patients ( 18.2% ; wes and rna - seq : n = 35 ; rna - seq only : n = 1 )  . 
patient characteristics characteristic total , no . female male ( range ) tumor type soft tissue unknown primary site colorectal urogenital thyroid breast lung skin hepatobiliary upper gi tract hematologic neuroendocrine pediatric head and neck others complete remission localized disease metastatic disease 2 to 3 rare tumor others solid tumors ( n = 189 ) : stage at presentation no . 
ninety of 104 treatment recommendations ( 86.5% ) were either off - label therapies ( n = 77 ) or trial inclusions ( n = 13 )  . the implementation rate of treatment recommendations was 31.7% ( 33 of 104 )  . 
in - label recommendations were pursued in nine of 14 cases ( 64.3% ) , whereas off - label recommendations and trial inclusions were implemented in only 28.6% ( 22 of 77 ) and 15.4% ( two of 13 ) of the cases , respectively . 
intended trial inclusion in 11 patients failed because of poor performance status or patient death ( n = 5 ) , closed trial arm ( n = 4 ) , or patient will ( n = 2 )  . 
main reasons for nonimplementation of treatment recommendations included loss to follow - up ( 22.5% ) , recommendation in the future ( 19.7% ) , patient death ( 16.9% ) , patient will ( 14.1% ) , and medical reasons ( 14.1% ; data supplement )  . 
of note , evidence level of individual off - label recommendations did not affect implementation rates ( data not shown )  . clinical outcome dgi and target databases , respectively ( data supplement )  . 
 the disease impact of non - hotspot mutations is more difficult to evaluate ; however , it can lead to in 33 patients with implemented treatment recommendations , partial remissions ( pr ) and stable diseases ( sd ) were seen in 11 ( 33.3% ) and eight patients ( 24.2% ; table 1 ) , respectively . 
of 14 responders receiving off - label therapies , eight ( 57.1% ) showed a progression - free survival ( pfs ) ratio ( pfs2 / pfs1 ; pfsr ) > 1.3 , supporting the impact of the recommended therapies.36 three patients had a pfsr < 1.3 with ongoing responses , meaning that their pfsr is still increasing . 
to assess whether implementation of treatment recommendations affected overall survival from first mtb discussion , we analyzed all patients with stage iv malignancies according to three subgroups ( n = 148 ; fig 3 )  . 
the median survival was not reached for patients with implemented treatment recommendations ( n = 33 recommendations pursued ; 95% ci , 9 months to not reached ) , 8 months for patients for whom treatment recommendations were not implemented ( n = 43 recommendations not pursued ; 95% ci , 3 to 10 months ) , and 10 months for patients who did not receive a treatment recommendation ( n = 72 no recommendations ; 95% ci , 7 to 17 months )  . 
predictive biomarkers for individualized immunotherapies are emerging and changing rapidly , with strong differences between entities.44 here , we used ihc for programmed cell death protein 1 ( pd - 1 ) / pd - l1 , tumor - infiltrating lymphocytes , microsatellite instability testing , and mutational burden assessment as predictive biomarkers . 
in the near future , identifying individual cancer neoantigens might allow a more precise prediction of responses to immunotherapies.45 this highlights the importance of an interdisciplinary mtb team that analyzes and interprets biomarkers to identify patients who might benefit from off label immuno - oncology treatments . in an mtb workflow , the portfolio of molecular diagnostic tests , as well as criteria to match and prioritize targeted therapies to molecular biomarkers , affects the probability to identify patients with actionable targets . 
our approach shares similarities with memorial sloan kettering integrated mutation profiling of actionable cancer targets ( msk - impact ) , focusing on therapeutically targetable biomarkers for fast clinical decision making and referral of patients to available clinical trials.51 targeted drug combinations might offer better dcr over single - agent therapies.52 - 55 in part , this is due to crosstalk between signaling pathways as well as spatial and temporal clonal heterogeneity , especially in patients with advanced cancer who failed standard - of - care treatment.56 , 57 most current programs for precision oncology use prespecified , genetically matched , single - agent treatments ( nci - match , clinicaltrials.gov identifier : nct02465060 ; or targeted agent and profiling utilization registry [ tapur ] , clinicaltrials.gov identifier : nct02693535 )  . 
these patients did not suffer from grade 3 to 4 adverse effects , although treatment combinations may bear a higher risk of toxicity.58 earlier referral to an mtb ( eg , after failure of first - line treatment ) might prevent the institution of ineffective treatments , improve the implementation rate , and increase the likelihood of success of molecular biomarkermatched treatments . 
 because of the low sample size and the heterogeneous composition of patients in the cohorts , the validity of this survival analysis is limited . access to molecular biomarkermatched , off label agents for cancer treatment is limited . 
in a recent single - center study , only 5% of molecular biomarkermatched treatment recommendations were implemented , mainly because of limited access to clinical trials or to restricted use of drugs outside their marketed label.59 thus , it is crucial to build up platforms for patients and treating physicians to link individual molecular information of the tumor to appropriate nonapproved drugs and available clinical trials . 
in rare entities , and especially in the setting of treatment - refractory cancers , precision oncology networks should allow hypothesis - driven in vitro studies and validation in small sets of individuals . 
thus , within the concept of patient - centric , biomarker - driven trial designs , 60 an mtb might constitute a critical tool to identify informative patients for clinical trials of targeted therapies in rare molecular subgroups . in summary , this mtb experience illustrates that patient management , on the basis of individual molecular biomarker profiling and analysis , is feasible in patients beyond standard - of - care treatment . 
 hauke busch no relationship to disclose christoph peters leadership : university medical center freiburg honoraria : university medical center freiburg travel , accommodations , expenses : novartis martin werner honoraria : diakovere consulting or advisory role : roche , novartis , johnson & johnson research funding : agilent ( inst ) , novartis ( inst ) , roche ( inst ) justus duyster honoraria : novartis , genentech , pfizer consulting or advisory role : novartis , roche travel , accommodations , expenses : novartis tilman brummer no relationship to disclose melanie boerries no relationship to disclose silke lassmann honoraria : novartis , astrazeneca travel , accommodations , expenses : novartis , astrazeneca nikolas von bubnoff honoraria : astrazeneca , amgen , bristol - myers squibb consulting or advisory role : novartis research funding : novartis travel , accommodations , expenses : novartis acknowledgment we thank the team of the genomics and proteomics core facility , german cancer research center / dkfz , heidelberg , germany , for their sequencing service . affiliations all authors : university of freiburg , freiburg ; ralph fritsch , julius wehrle , cornelius miething , christoph peters , martin werner , justus duyster , tilman brummer , melanie boerries , silke lassmann , and nikolas von bubnoff , german cancer consortium , partner site freiburg , and german cancer research center , heidelberg ; rainer claus , augsburg medical center , augsburg ; and hauke busch , university of lbeck , lbeck , germany . supported by comprehensive cancer center freiburg and by deutsches konsortium fr translationale krebsforschung grant no . 
hoadley ka , yau c , wolf dm , et al : multiplatform analysis of 12 cancer types reveals molecular classification within and across tissues of origcell 158 : 929 - 944 , 2014 3 . 
hong ds , morris vk , el osta b , et al : phase ib study of vemurafenib in combination with irinotecan and cetuximab in patients with metastatic colorectal cancer with brafv600e mutation . 
goss g , tsai cm , shepherd fa , et al : osimertinib for pretreated egfr thr790met - positive advanced non - small - cell lung cancer ( aura2 ) : a multicentre , open - label , single - arm , phase 2 study . 
li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
kovaleva v , geissler al , lutz l , et al : spatio - temporal mutation profiles of case - matched colorectal carcinomas and their metastases reveal unique de novo mutations in metachronous lung metastases by targeted next generation sequencing . 
kumar p , henikoff s , ng pc : predicting the effects of coding non - synonymous variants on protein function using the sift algorithnat protoc 4 : 1073 - 1081 , 2009 32 . 
von hoff dd , stephenson jj jr , rosen p , et al : pilot study using molecular profiling of patients tumors to find potential targets and select treatments for their refractory cancers . 
johnson db , dahlman kh , knol j , et al : enabling a genetically informed approach to cancer medicine : a retrospective evaluation of the impact of comprehensive tumor profiling using a targeted next - generation sequencing panel . 
massard c , michiels s , fert c , et al : high - throughput genomics and clinical outcome in hardto - treat advanced cancers : results of the moscato 01 trial . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
tos , tumorboard online system . online registration ( tos ) > 5 days prior to mtb treating physician analysis : adherence to recommendation entity expert review literature check trial availability molecular pathology review pathology review biomarkers treatment decision patient analysis : outcome 1 . 
 genomic and immune proling of a patient with triple - negative breast cancer that progressed during neoadjuvant chemotherapy plus pd - l1 blockade david casadevall , md1 , 2 ; xiaotong li , phd1 ; ryan l . 
wali , phd1 ; natalia buza , md1 ; vasiliki pelekanou , md , phd1 ; arjun dhawan , md1 ; julia foldi , md , phd1 ; borbala szekely , md , phd1 , 3 ; francesc lopez - giraldez , phd4 ; christos hatzis , phd1 ; and lajos pusztai , md , dphil1 introduction preliminary results from neoadjuvant trials combining immune checkpoint blockade ( icb ) with standardof - care chemotherapy suggest high pathologic complete response rates that range between 50% and 80% in triple - negative breast cancer ( tnbc ) .1 - 3 adding atezolizumab to nab - paclitaxel for rst - line treatment of metastatic tnbc signicantly improved response rate and progression - free survival compared with nabpaclitaxel alone , suggesting synergy between icb and chemotherapy.4 however , not all patients respond to icb , and a minority exhibit rapid progression of their disease.5 patients who experience exceptionally favorable or unfavorable responses provide unique opportunities for studying disease biology and for identifying response markers . 
progression during neoadjuvant chemotherapy is a rare event in tnbc . here , we report results from the molecular analysis of a tnbc that rapidly progressed during neoadjuvant chemotherapy plus programmed death - ligand 1 ( pdl1 ) blockade in a clinical trial neoadjuvant medi4736 concomitant with weekly nab - paclitaxel and dosedense ac for stage i - iii triple negative breast cancer ( clinicaltrials.gov identier : nct02489448 )  . 
baseline tumor - inltrating lymphocyte ( til ) count was 10% ( cd4 , 5% ; cd8 , 5% ; and cd20 , 1% ) , macrophage ( cd68 ) was 1% , and tumor cellularity was 50% . 
the patient agreed to participate in a neoadjuvant phase i / ii clinical trial that combined durvalumab ( 10 mg / kg once every 2 weeks ) with once - per - week nabpaclitaxel ( 100 mg / m2 ) for 12 cycles and dosedense doxorubicin plus cyclophosphamide ( ddac ) for 4 cycles . 
after 8 weeks of nab - paclitaxel plus durvalumab , physical examination showed increased tumor size and new skin edema conrmed by repeat mammogram and ultrasonograrepeat cnb showed 60% tumor cellularity but also an increase in til count to 20% ( cd4 , 10% to 15% ; cd8 , 5% ; and cd20 , 0% ) and an increase in macrophages ( cd68 , 20% )  . 
nab - paclitaxel was stopped but because of the increased immune inltration , durvalumab was continued , and the patient was administered ddac , which led to disease stabilization after four courses of therapy . 
because of the apparent clinical benet , she received two additional courses of ddac without durvalumab off protocol and underwent right skin - sparing mastectomy and lymph node dissection . pathology showed extensive multifocal disease ( largest focus , 2.4 cm ; tumor cellularity , 40% ) with lymphovascular invasion in the breast and more than 10 positive axillary lymph nodes ( ypt2 , ypn3 )  . 
immune cell proportions in the mastectomy were tils , 20% ; cd4 , 10% ; cd8 , 10% ; cd20 , 1% ; and cd68 , 10% . dna and rna were extracted from formalin - xed parafn - embedded sections of tumor samples obtained at baseline , at week 8 , and from the mastectomy . 
til counts and immune cell subtypes were determined by routine pathology and immunohistochemistry . when we compared our patients baseline expression of 26 immune cell types and 100 immune function metagenes with those in the reference cohort , her neutrophil metagene expression was below the 2.5th percentile , whereas the cell cycle and immunosuppression metagenes were above the 97.5th percentile of the reference distribution ( fig 1a ) , indicating a highly proliferative tumor with an immunosuppressed microenvironment . 
the tumor also showed low expression of two previously validated immunotherapy predictive gene signatures , 8 , 9 indicating low probability of response to icb ( fig 1b )  . 
single - gene level analysis revealed signicantly low expression of 27 genes including pdcd1 , cd8a , and klrc2 ( fig 1c ) , suggesting impaired t - cell and natural killer ( nk ) cell activity . 
in addition , we found high exincluding tgfb , hla - g , cd63 , pression of 33 genes , ccl28 , and cxcl16 ( fig 1d ) , which are associated with an immune evasive phenotype , increased cell motility , and invasion . 
overall , greater changes were observed between week 8 and mastectomy ( ddac treatment ) than between baseline and week 8 ( nab - paclitaxel treatment )  . we observed upregulation of fos , abcb1 , kir3dl3 , gzma , and gzmk in the mastectomy ( single - gene and metagene expression changes are provided in the data supplement )  . 
to study this further , we next analyzed t - cell exclusion and dysfunction features using the tumor immune dysfunction and exclusion ( tide ) method ( data supplement ) .10 in concordance with our previous ndings , cytotoxic t - cell inltration increased during the second period . 
however , this was accompanied by an increase in t - cell dysfunction score , indicating an ineffective immune response ( fig 2b )  . we also performed whole - exome sequencing of baseline and mastectomy specimens . 
other mutations with the highest variant allele frequency at baseline included znf385c , cacna1e , nxpe1 , and dync1h1 , which have poorly understood functions in cancer ( fig 2c ; data supplement )  . 
we also detected amplications in fgfr1 , fgf2 , fgf3 , myc , mcl1 , ccnd1 , and tgfb2 and deletions in cdkn2a and cdkn2b ( data supplement )  . 
by using sciclone ( waltham , ma ) 11 and clonevol , 12 we identied four distinct tumor clones , all present at baseline and in the mastectomy specimen , with little evidence for clonal selection during therapy ( figs 2c - d )  . 
compound heterozygous inactivating mutations cause severe combined immune deciency.14 discussion this cancer showed primary resistance to nab - paclitaxel and ddac chemotherapy concurrent with an anti - pd - l1 agent . 
the tumor harbored several poor prognostic genomic alterations at diagnosis , including a p53 mutation and coamplication of myc and mcl1 , both of which are implicated in chemotherapy resistance.15 , 16 the expression of permeability glycoprotein ( p - glycoprotein ; abcb1 ) , a drugefux transporter that mediates taxane and anthracycline resistance in vitro , also increased during treatment.17 we observed a measurable increase in intratumor ammatory response by the end of the treatment ( data supplement ) , but unfortunately this did not translate into clinical antitumor activity . 
tgf activation in cancers has been linked to primary chemotherapy resistance and also to immune evasion and resistance to pd - l1 blockade in multiple experimental systems.18 - 21 furthermore , r175h p53 mutation that this cancer harbored has been shown to render cancers insensitive to the growth inhibitory effects of tgf.22 on the basis of these ndings , we hypothesize that the high expression of tgfb2 by this tumor may have contributed to its immune escape and its resistance to chemotherapy . 
another notable feature of this cancer was the low level of expression of programmed cell death protein 1 ( pd1 ) at the time of diagnosis and the high level of expression of hla - g . 
categories in which our patients score is above the 97.5th percentile ( red dots ) or below the 2.5th percentile ( teal dots ) are highlighted , are shown as bold numbers , and are described in the legend key . 
finally , genes for which our patient had expression values below the 2.5th ( panel c , teal squares ) or above the 97.5th ( panel d , red squares ) bootstrap distribution percentiles are shown . 
legend boxes and bold numbers show categories for which we observed an increase or decrease of 0.5 log2 fold change between either baseline and 8 weeks ( rst period ) and / or 8 weeks and mastectomy ( second period )  . 
 ( b ) tumor immune dysfunction and exclusion ( tide ) - based ( data supplement ) t - cell dysfunction and exclusion shown together with correlation coefcients of the gene expression values for our patient with cancer - associated broblast ( caf ) , myeloid - derived suppressor cell ( mdsc ) , and m2 tumor - associated macrophages ( tam m2 ) signatures . 
 ( c ) variant allele frequency ( vaf ) plot ( left ) and shplot ( right ) illustrating the clonal architecture and evolution ( based on sciclone [ waltham , ma ] and clonevol tools ; data supplement ) of the tumor between baseline and mastectomy time points . 
ifng , interferon gamma signature ; math , mutant allele tumor heterogeneity ; til , tumor - inltrating lymphocyte ; tlr , toll - like receptor . contributed to the poor outcome . 
however , the ndings pose at least one testable therapeutic hypothesis : tgf - targeting therapies ( eg , galunisertib , m7824 , tew7197 , ly - 3200882 , fresolimumab , and nis793 ) may have improved the efcacy of pd - l1 blockade in this particular individual . in summary , this case demonstrates the complexity of chemotherapy and immunotherapy resistance mechanisms and suggests that multiple different biologic processes may contribute to disease progression during treatment . we nd it reassuring that previously published icb response signatures predicted low sensitivity to pd1 / pd - l1 blockade for this patient . 
for more information about asco 's conict of interest lajos pusztai honoraria : merck , astrazeneca / medimmune , pzer , syndax pharmaceuticals , almac diagnostics , pieris pharmaceuticals , genentech , immunomedics , eisai , seattle genetics / astellas pharma , biotheranostics consulting or advisory role : h3 biomedicine , merck , novartis , pieriandx , seattle genetics , syndax pharmaceuticals , athenex research funding : merck , genentech , seattle genetics , astrazeneca no other potential conicts of interest were reported . acknowledgment we thank erika esteve , md , for her invaluable support throughout the study period ; xavier monzonis , md , and santiago balseiro , md , for their insightful suggestions ; tao qing and michal marczyk for their frequent inputs regarding methodologic and technical aspects of the manuscript ; and jeremia walah ( developer of structural variation and indel analysis by assembly ) and peng jiang ( developer of tumor immune dysfunction and exclusion score ) for their feedback regarding the use and interpretation of their tools . references pusztai l , hofstatter ew , chung gg , et al : durvalumab ( medi4736 ) concurrent with nab - paclitaxel and dose dense doxorubicin cyclophosphamide ( ddac ) as neoadjuvant therapy for triple negative breast cancer ( tnbc )  . 
j clin oncol 36 , 2018 ( suppl ; abstr 586 ) loibl s , untch m , burchardi n , et al : randomized phase ii neoadjuvant study ( geparnuevo ) to investigate the addition of durvalumab to a taxane - anthracycline containing chemotherapy in triple negative breast cancer ( tnbc )  . 
nanda r , liu mc , yau c , et al : pembrolizumab plus standard neoadjuvant therapy for high - risk breast cancer ( bc ) : results from i - spy 2 . 
j clin oncol 35 , 2017 ( suppl ; abstr 506 ) schmid p , adams s , rugo hs , et al : atezolizumab and nab - paclitaxel in advanced triple - negative breast cancer . 
n engl j med 379 : 2108 - 2121 , 2018 ferrara r , mezquita l , texier m , et al : hyperprogressive disease in patients with advanced non - small cell lung cancer treated with pd - 1 / pd - l1 inhibitors or with single - agent chemotherapy . 
ann oncol 29 : 2232 - 2239 , 2018 shi w , jiang t , nuciforo p , et al : pathway level alterations rather than mutations in single genes predict response to her2 - targeted therapies in the neo - altto trial . 
ann oncol 28 : 128 - 135 , 2017 ayers m , lunceford j , nebozhyn m , et al : ifn - - related mrna prole predicts clinical response to pd - 1 blockade . 
j clin invest 127 : 2930 - 2940 , 2017 fehrenbacher l , spira a , ballinger m , et al : atezolizumab versus docetaxel for patients with previously treated non - small - cell lung cancer ( poplar ) : a multicentre , open - label , phase 2 randomised controlled trial . 
lancet 387 : 1837 - 1846 , 2016 jiang p , gu s , pan d , et al : signatures of t cell dysfunction and exclusion predict cancer immunotherapy response . 
ann oncol 28 : 3076 - 3082 , 2017 imamura t , takase m , nishihara a , et al : smad6 inhibits signalling by the tgf - beta superfamily . 
lee k , giltnane jm , balko jm , et al : myc and mcl1 cooperatively promote chemotherapy - resistant breast cancer stem cells via regulation of mitochondrial oxidative phosphorylation . 
noonan , mbbchbao , msc1 - 3 ; sagar sardesai , md1 - 3 ; jeffrey vandeusen , md , phd1 - 3 ; robert wesolowski , md1 - 3 ; nicole williams , md1 - 3 ; clara n . 
we evaluated three prespecied questions to assess patients perceptions of genomic testing . results in all , 100 patients underwent genomic testing , with a median of ve mutations ( range , 0 to 13 mutations ) detected per patient . 
genomic testing revealed one or more potential therapies in 98% of patients ( 98 of 100 ) , and 60% of patients ( 60 of 100 ) had one or more recommended treatments with level i / ii evidence for actionability . 
we did not detect a statistically signicant difference in time - to - treatment failure ( log - rank p = .87 ) or overall survival ( p = .71 ) among patients who had treatment change supported by genomic testing versus those who had no treatment change . 
this study provides a prospective analysis of physician decision making and outcomes of patients receiving tumor sequencing as part of mbc clinical care . knowledge generated genomic testing revealed that most patients ( 60% ) had at least one recommended treatment with level i / ii evidence for actionability ; however , only a subset of patients were given a recommendation for a change in treatment , and even fewer actually changed therapy on the basis of genomic testing results . 
patients whose therapy did not change on the basis of genomic testing had a decrease in condence of treatment success . relevance even though standard of care is improving , relatively few patients with mbc changed therapy on the basis of genomic testing in this prospective study . 
this suggests a need to better understand barriers to implementation of mutation - directed therapy as well as a need for improved understanding of patient perception of somatic genomic testing . ( ia ) , pik3ca hotspot - activating missense mutations ( ia ) , microsatellite instability ( ic ) , ntrk fusions ( ic ) , esr1 hotspot - activating missense mutations ( iia ) , pten loss ( iia ) , akt1 mutations ( iib ) , and erbb2 hotspot - activating missense mutations ( iib ) .16 although genomic testing is promising for improving treatment efcacy , it is unclear how frequently it changes treatment.17 - 19 complex interactions between choice of genomic testing and patient perception of care make it imperative to understand the impact of genetic sequencing in clinical oncology.17 , 20 , 21 to date , we have little understanding of how patients perceive the value or accuracy of genomic testing , and whether changes in treatment recommendation based on genomic testing affect patients perceptions of care . 
there are discrepancies between cancer patient and physician expectations of therapy efcacy ; patients demonstrate greater optimism about therapy efcacy.22 - 25 expectations of patients with mbc and their motivations for undergoing somatic genetic testing have not yet been explored . clinical tumor genomic analyses typically rely on targeted next - generation sequencing ( ngs ) of a panel of specic , typically actionable cancer - related genes to analyze somatic gene alterations from biopsy specimens . 
most commercial targeted panel sequencing approaches , including foundationone cdx ( foundation medicine , cambridge , ma ) in this study , provide treatment suggestions that are based on literature.26 we genomic alterations and available clinical hypothesized that prospective implementation of foundationone cdx testing into clinical care for patients with mbc will identify patient - specic approaches that offer improved patient outcomes and perceptions of care . 
in this study , patients with mbc received foundationone cdx testing when a new treatment was initiated and genomic testing results released to the provider at the next progression event . 
the study was approved by the ohio state university institutional review board and informed consent was obtained from all patients . testing was performed by using foundationone cdx , formalin - xed parafnwhich used ngs on patients embedded tumor tissue . 
the foundationone cdx results were then released to the provider . survey measures physicians received a ve - item questionnaire after the foundationone cdx report was released to assess whether their treatment recommendation should be changed on the basis of those results . 
the questionnaire asked how the physician used the foundationone cdx test ( multiple choice ) and what else they would like to see in the report ( multiple choice plus an open - ended other option )  . 
attitudes toward foundationone cdx testing were assessed with three items : ( 1 ) by having the test , i will feel more condent of my treatments success , ( 2 ) i will trust the test results , and ( 3 ) i think the test results will be accurate . 
patient motivation and expectations for study participation were assessed with 15 questions using a ve - point likert scale that ranged from strongly disagree to strongly agree ( data supplement )  . because of small numbers in each group , these questions were assessed as a three - level outcome ( agree v neutral v disagree ) and as a binary outcome ( agree v neutral and disagree )  . statistical and survival analyses mcnemars test of agreement ( 2 level or 3 level ) was used to compare preand post - test survey responses and preversus post - test survey agreement by foundationone cdxsupported treatment change results from the physician questionnaire . 
the offstudy date was dened as the date of the patients second progression ( rst while on study ) , second treatment change ( rst while on study ) , death , or loss to follow - up . 
patients still alive on december 18 , 2018 , were censored as of this date . all statistical analyses were performed using sas version 9.4 ( sas institute , cary , nc ) and r version 3.4.1 , and survival curves were created using the packhv package.27 results study population a total of 142 patients with mbc provided consent and were assessed for eligibility ( fig 1 )  . 
patients were excluded from analysis if there was no available tissue , insufcient tissue , or poor dna quality ( n = 21 ) , died before the foundationone cdx report was released ( n = 13 ) , did not receive foundationone cdx testing within 10 weeks of starting their current line of therapy ( n = 4 ) , were lost to follow - up ( n = 2 ) , withdrew consent ( n = 1 ) , or had a biopsy that revealed no metastatic disease ( n = 1 )  . 
of these samples , 71% ( 71 of 100 ) were metastatic biopsies and 29% ( 29 of 100 ) were primary tumors ( breast or axillary lymph node )  . 
the study population was predominantly age 55 years or older , white , and collegeeducated with a high income ( table 1 )  . foundationone cdx genomic testing results among the 100 patients with successful foundationone cdx ngs testing , the number of mutations identied per patient ranged from 0 to 13 with a median of ve mutations ( data supplement )  . 
as anticipated , the most common mutations were missense or frameshift mutations in tp53 ( n = 49 ) and pik3ca ( n = 40 ) or amplication of myc ( n = 20 ; fig 2a )  . 
among er - positive / her2 - negative patients , 10 ( 16.7% ) of 63 harbored an esr1 mutation . in terms of therapy recommendations , 98 ( 98.0% ) of 100 patients had at least one potential therapy identied on foundationone cdx testing , with a median of nine potential treatments ( range , 0 to 35 potential treatment ; fig 2b )  . 
the most commonly recommended therapy based on a genomic alteration was an mtor inhibitor ( everolimus or temsirolimus ) for pik3ca mutations ( data supplement )  . among all patients , 60 ( 60% ) of 100 had at least one recommended treatment with level i / ii evidence ( not including erbb2 amplications ) , 16 with a median of one potential treatment with level i / ii evidence ( range , 0 to 2 potential treatments ; fig 2b )  . potential germline alterations in somatic tumor testing a known challenge in somatic tumor sequencing is potential identication of germline alterations.28 - 32 among the 100 total patients , 14 had alterations identied in brca1 ( n = 4 ) , brca2 ( n = 8 ) , or palb2 ( n = 2 )  . 
of these six patients with no prior knowledge of germline mutations , two had germline alterations conrmed ( one brca1 and one brca2 ) and one underwent germline testing in which no alterations were identied ( presumed somatic brca2 mutation )  . 
the six patients whose foundationone cdx reports were not therapy without proreleased remained on their initial gression as of september 1 , 2018 ; ve of these patients had er - positive / her2 - negative and one had er - positive / her2 - positive breast cancer . 
across the study population , 10 ( 10.0% ) of 100 total patients or 10 ( 11.5% ) of 87 patients with physician questionnaire data experienced a treatment change supported by foundationone cdx data . 
physicians described not changing treatment because the patient could not be enrolled on a clinical trial ( ie , the recommended trial closed , the patient did not want to enroll , or the patient was ineligible ; n = 10 ) , patient hospitalization ( n = 3 ) , insurance denied treatment charges ( n = 2 ) , patient transferred care to other provider ( n = 1 ) , or patient pursued a nonrecommended trial ( n = 1 ; data supplement )  . genomic alterations and survival among 76 patients evaluable for ttf analysis , there was no signicant difference in ttf ( log - rank p = .87 ) by foundationone cdx - supported treatment change status ( fig 3a )  . 
despite a high frequency of mutation , there was no signicant difference in os by pik3ca mutation status among er - positive / her2 - negative patients ( p = .18 ) or tnbc patients ( p = .66 ) , or when evaluating alterations that could activate the pi3k pathway ( pik3ca mutation , pten loss , or akt1 mutation ) among er - positive / her2 - negative patients ( p = .60 ) or tnbc ( p = .81 ) patients ( data supplement )  . 
in the msk - impact study ( clinicaltrials.gov identier : nct01775072 ) , hrpositive / her2 - negative patients with detected tumor mutations in esr1 , map kinase pathway , or myc or other transcription factors genes had a worse response to aromatase inhibitor these alterations.15 we evaluated the association of these alterations with os and found no signicant difference among the four groups ( fig 3d )  . therapy than patients without patients perceptions of genetic testing a total of 58 ( 58.0% ) of the 100 evaluable patients completed at least a portion of the survey at enrollment ( pretest ) , and 40 ( 40.0% ) completed at least a portion of the survey at study conclusion ( post - test )  . 
in the pretest survey , most patients strongly agreed or somewhat agreed that by having the genetic testing they would feel more condent in their treatments success ( 36 [ 65.5% ] of 55 ) , whereas at study completion , a minority of patients ( 12 [ 30.8% ] of 39 ) felt more condent in their treatments success by having the genetic testing . 
there was no signicant difference in patients trust of test results or thinking the results were accurate ( mcnemars p = .06 for both questions )  . foundationone cdx - supported treatment change status ( fig 3b )  . 
by subtype , there were signicant differences in os ( log - rank p = .01 ) ; patients who had tnbc had worse os than er - positive / her2 - negative patients , as anticipated ( data supplement )  . among genomic alterations , we evaluated several mutations known to be prognostic ( esr1 mutations ) or potentially predictive of outcomes ( pik3ca )  . 
in msk - impact ( a targeted tumor - sequencing assay developed at memorial sloan kettering cancer center [ msk ] termed integrated mutation proling of actionable cancer targets [ impact ] ) , there was evidence that patient response to aromatase inhibitor therapy was signicantly worse for patients whose tumors harbored one of several alterations.15 among we then assessed whether pretest and post - test survey results were associated with treatment change on the basis of foundationone cdx results in patients who completed both the pretest and post - test survey questions of interest . for treatment condence , we found that patients who did not have a treatment change supported by foundationone cdx data were signicantly more likely to change their response from agree to neutral or disagree ( mcnemars test of agreement p = .001 ; fig 4 )  . 
of potential therapies with level i / ii evidence 50 40 30 20 10 0 % mutant tp53 pik3ca cdh1 znf703 esr1 ccnd1 fgfr1 fgf4 fgf19 gata3 fgf3 map2k4 znf217 pten mcl1 brca2 erbb2 map3k1 arid1a smad4 myst mdm2 mutations or potential therapies for each patient fig 2 . 
comut plot created by using the genvisr package.47 ( b ) for each patient ( n = 100 ) , the graph shows number of detectable mutations , number of potential therapies identied , and number of potential therapies with level i / ii evidence for actionability in breast cancer based on condorelli , et al.16 ( * ) indicates patients whose treatment was changed based on genomic testing results . treatment ( data supplement )  . 
 ( a ) kaplan - meier plot of time to treatment failure stratied by patients with treatment change based on genomic testing ( red line ) v no treatment change . 
time to treatment failure dened as time from release of foundationone cdx results to the off - study date , dened as date of second progression or treatment change ( rst during the study period ) , death , or loss to follow - up . 
 ( c ) kaplan - meier plot of overall survival for patients with estrogen receptor ( er ) positive / human epidermal growth factor receptor 2 ( her2 ) negative metastatic breast cancer , stratied by presence or absence of mutation in esr1 . 
we prospectively evaluated the impact of ngs on mbc treatment decisions and potential associations with patient outcomes and their perceptions of genomic testing . in this study , more than 60% of patients had a genomic alteration associated with level i or ii evidence for actionability ( not including her2 amplication ) based on a recent consensus panel16an impressive number that emphasizes the potential for widespread use of ngs . 
a total of 37 patients answered the question both before ( pre - genomic test survey ) and after ( post - genomic test survey ) genomic test results were shared with physicians . 
this is consistent with a previous study that identied barriers such as trial ineligibility , distance to trial , and physical / emotional exhaustion.18 treatment change was not signicantly associated with ttf or os ; however , the small number of patients experiencing treatment change limits the conclusions that can be drawn from these analyses . this is the rst study to our knowledge to prospectively evaluate the inuence of somatic ngs on patient perception of care and it provides important initial data , but the lower patient survey response rate limits denitive conclusions . 
when comparing study surveys at admission to surveys at conclusion , patients seemed less condent in their treatment , particularly those whose treatment was not changed by foundationone cdx results . 
this is consistent with other studies that suggest genetic testing may increase negative emotions in patients with metastatic cancer , 18 although most studies evaluated effects from germline testing.36 - 40 our data preliminarily suggests that there may be ramications of somatic genomic testing for patients despite its known utility in selecting therapy for mbc . because negative emotions are associated with decreased quality of life and potentially with survival , 41 - 44 the possible negative implications of broadly integrating ngs into clinical practice should be considered . furthermore , pretest survey data suggest that patients have misconceptions about what somatic mutation testing can inforwe found that patients had overly optimistic expectations for somatic tumor ngs : almost half believed the test would tell them which medication to take whereas only 11.5% of the total patients switched therapy on the basis of foundationone cdx reports . 
this is similar to previous studies that demonstrate that patients have greater optimism regarding treatment efcacy than physicians do , 24 possibly because physicians provide patients with more optimistic information than their true assessment.45 in addition , most patients incorrectly believed the test would predict future genetic mutations , assess childrens disease risk , or estimate treatment success , despite the informed consent stating that participants would rarely benet personally or therapeutically from this study . 
therefore , this supports further exploration of the readability of consent forms , an area currently under investigation.46 we hypothesize that patients limited knowledge of genetics may explain their decreased condence after genomic testing , 17 - 19 and we also hypothesize that improved decision support for genomic testing for patients will improve condence in their treatment , particularly in the context of increases in available targeted treatments for mbc . there are known limitations to our study that prevent us from making denitive conclusions . 
furthermore , unlike the methodologies in the existing literature , we used a unique prospective and longitudinal methodology to evaluate patient perceptions . future studies may benet by including patient interviews to assess the experience of somatic ngs . 
furthermore , the potential treatments identied by foundationone cdx test results reect drugs approved for any indication , not necessarily for mbc , and therapies available at the time of the test . 
for example , both everolimus and temsirolimus were reported as potential therapies for patients with alterations in nf1 , pten , ak1 , pik3r1 , rptor , akt3 , fbxw7 , kit , pdgfra , stk11 , and vhl ; however , only everolimus is approved by the us food and drug administration for mbc . 
in addition , since this study was completed , multiple new therapies approved by the us food and drug administration have not been considered , suggesting that clinical implications of ngs should be assessed regularly . in conclusion , our ndings suggest that ngs by tools such as foundationone cdx may provide valuable insight for physicians and patients when determining the best treatment option for patients with mbc upon disease progression . 
there are clear clinical challenges involved with integrating ngs into the framework of mbc care , including barriers to preferred treatment options and complex interactions between genomic testing and patient perceptions , which warrant further study . affiliations 1the ohio state university college of medicine , columbus , oh 2the ohio state university comprehensive cancer center , columbus , oh 3stefanie spielman comprehensive breast center , columbus , oh 4the ohio state university , columbus , oh 5foundation medicine , cambridge , ma 6the ohio state university college of public health , columbus , oh 7mt . 
chen consulting or advisory role : novartis , immune design , syapse speakers bureau : novartis , foundation medicine research funding : eisai patents , royalties , other intellectual property : matchtx , a genomics software package that helps researchers , oncologists , and clinical trial managers identify the full set of biomarkers that collectively predict the outcome of patients with cancer to treatment siraj mahamed ali employment : foundation medicine leadership : incysus stock and other ownership interests : exelixis , blueprint medicines , agios , genocea biosciences consulting or advisory role : revolution medicines , azitra ( i ) , princeps tx ( i ) patents , royalties , other intellectual property : patents via foundation medicine and via seres health on microbiome in non - neoplastic disease ( i ) anne m . 
noonan consulting or advisory role : helsinn healthcare , qed therapeutics sagar sardesai consulting or advisory role : novartis speakers bureau : immunomedics travel , accommodations , expenses : novartis jeffrey vandeusen stock and other ownership interests : immunomedics robert wesolowski consulting or advisory role : pzer ( inst ) , puma biotechnology research funding : acerta pharma , astrazeneca travel , accommodations , expenses : pzer , puma biotechnologybhuvaneswari ramaswamy consulting or advisory role : pzer maryam b . 
lustberg consulting or advisory role : tempus , pledpharma other relationship : hologic / cynosure no other potential conicts of interest were reported . references oshaughnessy j : extending survival with chemotherapy in metastatic breast cancer . 
condorelli r , mosele f , verret b , et al : genomic alterations in breast cancer : level of evidence for actionability according to esmo scale for clinical actionability 17 . 
gray sw , park er , najita j , et al : oncologists and cancer patients views on whole - exome sequencing and incidental ndings : results from the canseq study . of molecular targets ( escat )  . 
gollust se , gray sw , carere da , et al : consumer perspectives on access to direct - to - consumer genetic testing : role of demographic factors and the testing 21 . 
meropol nj , weinfurt kp , burnett cb , et al : perceptions of patients and physicians regarding phase i cancer clinical trials : implications for physician - patient communication . 
lux mp , bayer cm , loehberg cr , et al : shared decision - making in metastatic breast cancer : discrepancy between the expected prolongation of life and treatment efcacy between patients and physicians , and inuencing factors . 
parsons dw , roy a , plon se , et al : clinical tumor sequencing : an incidental casualty of the american college of medical genetics and genomics recommendations for reporting of incidental ndings . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation proling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
tanioka m , fan c , parker js , et al : integrated analysis of rna and dna from the phase iii trial calgb 40601 identies predictors of response to trastuzumabbased neoadjuvant chemotherapy in her2 - positive breast cancer . 
bakos ad , hutson sp , loud jt , et al : brca mutation - negative women from hereditary breast and ovarian cancer families : a qualitative study of the brca37 . 
hay jl , meischke hw , bowen dj , et al : anticipating dissemination of cancer genomics in public health : a theoretical approach to psychosocial and behavioral negative experience . 
collins vr , meiser b , ukoumunne oc , et al : the impact of predictive genetic testing for hereditary nonpolyposis colorectal cancer : three years after testing . genet med 9 : 290 - 297 , 2007 40 . 
hendriks ks , hendriks mm , birnie e , et al : familial disease with a risk of sudden death : a longitudinal study of the psychological consequences of predictive testing for long qt syndrome . 
chida y , hamer m , wardle j , et al : do stress - related psychosocial factors contribute to cancer incidence and survival ? nat clin pract oncol 5 : 466 - 475 , 2008 42 . 
giese - davis j , collie k , rancourt km , et al : decrease in depression symptoms is associated with longer survival in patients with metastatic breast cancer : a secondary analysis . 
perni s , rooney mk , horowitz dp , et al : assessment of use , specicity , and readability of written clinical informed consent forms for patients with cancer undergoing radiotherapy . 
 o implementation and clinical utility of an integrated academiccommunity regional molecular tumor board see accompanying editorial doi : purpose precision oncology develops and implements evidence - based personalized therapies that are based on specific genetic targets within each tumor . 
however , a major challenge that remains is the provision of a standardized , up - to - date , and evidenced - based precision medicine initiative across a geographic region . materials and methods we developed a statewide molecular tumor board that integrates academic and community oncology practices . 
the precision medicine molecular tumor board ( pmmtb ) has three components : a biweekly web - based teleconference tumor board meeting provided as a free clinical service , an observational research registry , and a monthly journal club to establish and revise evidence - based guidelines for off - label therapies . 
the pmmtb allows for flexible and rapid implementation of treatment , uniformity in practice , and the ability to track outcomes . results we describe the implementation of the pmmtb and its first year of activity . 
nine subjects ( 28% ) received recommended therapy with a response rate of 17% ( one of six ) and a clinical benefit rate ( partial response + stable disease ) of 38% ( three of eight )  . 
today , next - generation sequencing assays are widely available and considered to be part of the standard of care in specific clinical situations.1 , 2 at the same time , precision medicine promises to match patients to gene - targeted treatments.3 however , many challenges exist in implementing precision medicine , including knowledge gaps , privacy , systems barriers , and reimbursement issues.4 , 5 the knowledge gaps arise from the extensive breadth and depth of knowledge required to effectively use genomic information , which is compounded by tumor complexity and the wide variation of genomic landscapes in tumors.6 , 7 to meet this challenge , knowledge in genomic technologies , cancer biology , human pathology , pharmacology , clinical patient care , and often detailed knowledge of gene structure and function are required . molecular tumor boards ( mtbs ) address gaps in knowledge and clinical utility by providing a forum for individuals with wide - ranging expertise to review patient medical histories and mutation profiles to guide patient - specific treatment options.8 - 12 in contrast to organ - specific tumor boards , mtbs consider patients with diverse mark e . 
rehrauer jill kolesar author affiliations appear at the end of this article . supported by national cancer institute grant no . p30 ca014520 to the university of wisconsin carbone cancer center . corresponding author : mark e . 
although mtbs have been established at academic institutions , they are largely unavailable at nonacademic sites . to expand access to mtbs , we have partnered with community practitioners at other health networks to develop an integrated mtb available to any provider in our geographic region , the precision medicine molecular tumor board ( pmmtb )  . 
in addition to its regional scope , the pmmtb is novel in its tripartite structure by separating clinical service , a registry protocol , and a journal club to establish parameters for evidencebased use of off - label therapies . 
moreover , some patients are prospectively consented to the registry at the time that molecular testing and biopsy are performed ; these patient cases are later presented at the tumor board . the third part of the structure is a monthly journal club meeting . 
at the conclusion of the journal club , the tumor board decides whether to adopt or reject the proposed drug - biomarker pair and to update the guidance document that specifies when offlabel therapies will be recommended . 
in addition , periodic review of cases in the tumor registry ineffective treatment approaches , may reveal which in turn will trigger a journal club to seek to retract a previously issued criterion in the guidance document . tumor board the first part of the pmmtb structure consists of a twice - monthly tumor board convened through web - based teleconference . 
participants are experts in diverse fields that span basic cancer biology , medical / clinical genetics , molecular pathology , surgical pathology / cytopathology , pharmacology , medical oncology , and radiation oncology . 
molecular test results from a clinical laboratory improvement amendmentscertified laboratory are included with the case submission information . up to six cases are discussed per 1 - hour meeting ; when additional cases are submitted , review is either postponed or performed administratively by the pmmtb chairs . 
the molecular pathology team reviews alterations and assesses their analytic validity , that is , whether a particular mutation is likely to alter gene function on the basis of site and allele frequency or whether an amplicon encompasses many reported genes . 
 are systematically discussed in the context of cancer databases ( cancer gene census / cosmic [ catalogue of somatic mutations in cancer ] ) , the cancer genome atlas , and human polymorphism databases ( dbsnp , 1000 genomes project , esp6500 ) along with knowledge tools ( cbioportal , my cancer genome , targeted cancer care , personalized cancer therapy ) .13 - 18 the board identifies and discusses possible clinical trials and off - label targeted therapies . 
final recommendations are provided in the form of a formal letter to the submitting physician , with acceptance at the discretion of the treating clinician ( data supplement )  . journal club the pmmtb considers targeted food and drug administrationapproved drugs that are not labeled for use in that particular patients tumor type according to a guidance document . 
the guidance document includes , for example , the targeting of oncogenes with known activating mutations by using drugs that directly inhibit their activity , combination therapies for braf mutations , and specific criteria for using genomic decisions for immune checkpoint inhibitors . 
during the meeting , up to three studies , including human and preclinical evidence , are provided and the pmmtb decide reviewed ; members of whether to amend the guidance document , to provisionally amend it ( if human data are extremely limited ) , or to reject it . 
in this manner , all decisions to recommend off - label therapies are based on careful , but timely review of evidence . registry patients are enrolled in a registry to allow for the tracking of outcomes . 
the registry protocol was approved by our institutional review board ( university of wisconsin [ uw ] hs - irb approval #2015 - 1370 ) and was conducted in accordance with the declaration of helsinki . 
all clinical laboratory improvement amendments certified genomic tumor profiling assays are allowed , including commercial tests , tests performed at outside academic facilities , and tests performed at the uw collaborative genomics core . subjects registered and presented at the pmmtb were followed for acceptance of recommendations , treatment , and disease response or progression . 
the primary objective of this study was to assess the the pmmtb , defined as clinical utility of the frequency of recommendation acceptance . descriptive summaries of response to therapy , disease status , and demographic information are provided . 
for nonmeasurable tumors , stable disease versus partial response was reported on the basis of radiologic follow - up and clinical assessment of the treating physician at the follow - up study performed 2 to 4 months after baseline . results participant and disease characteristics because registry consent was not a prerequisite to pmmtb presentation , overlap was incomplete between patient cases presented and subjects enrolled . 
seventy - seven patient cases were submitted to the tumor board between september 17 , 2015 , and september 1 , 2016 : 74 were presented to the board , and three were reviewed administratively . 
four registered patients who had planned genomic testing were not presented at the tumor board because molecular analysis of their tumor was not complete ( eg , insufficient tissue )  . 
of the 44 patient cases presented , 38 were deemed to have adequate followup by september 1 , 2016 , to report results here . table 1 includes demographics and other baseline characteristics for these 38 patients . 
the most common genomic test used was the foundationone ( foundation medicine , cambridge , ma ) assay , followed by the uw collaborative genomics core 50 - gene panel . pmmtb recommendations and acceptance figure 3 depicts recommendations and acceptance of the 38 patient cases . 
an actionable target was defined as one that allowed identification of a molecular - targeted clinical trial or off - trial treatment that is based on the pmmtb guidance document . 
the area of the circle is proportional to the number of patient cases presented from that health system . uwccc , university of wisconsin carbone cancer center . actionable target was found in 32 ( 84% )  . 
treatment was accepted for nine ( 28% ) of these 32 and not accepted for 11 ( 34% ) , and the remainder of patients continued on standard - of - care therapy , pending progression . 
in general , we found that patients were able to obtain these drugs when recommended by the pmmtb , which highlights the access that physicians and patients have to off - label therapies . 
the pmmtb may have facilitated this access by establishing and implementing a uniform set of criteria and recommendations provided as an official letter ( data supplement )  . although clinical trials were preferentially recommended , they were rarely accepted . 
for clinical trials available outside the state , no patients enrolled . the major reason was that patients with metastatic cancer often were unable or unwilling to travel long distances for investigational therapy . within the state , restrictive and often unanticipated eligibility criteria prohibited enrollment . for example , one patient was ineligible because of a recent amendment that precluded any history of drug allergy . 
molecular - targeted basket studies were largely unavailable in the region partly because of a national hold placed on the national cancer institute molecular analysis for therapy choice ( nci - match ) trial during most of the period covered . 
these findings highlight poor access to clinical trials of precision medicines and the need for local availability of clinical trials with minimal eligibility restrictions and fast startup . in the first year of the pmmtb , journal clubs primarily were used to expand the guidance document ( data supplement )  . 
in this diagram , some samples were tested for large gene sets ( foundationone , including gray boxes for nonaltered genes ) and others for limited gene sets through the uw collaborative genomics core 50 - gene panel or subset ; genes not tested are depicted as white areas . 
additional genes identified in these subjects are listed in the data supplement . the pmmtb identified treatment options that targeted 18 distinct genes in these patients ( red boxes )  . 
more treatment options were identified for tumors tested with comprehensive panels . with the inclusion of both trial and nontrial treatments , we identified a mean of 1.7 treatment options with the 405 - gene panel versus 1.1 with a more - restrictive panel of < 50 genes . 
of the remaining eight patients who received the recommended therapy , the clinical benefit rate was 38% ( three of eight ) and the response rate was 17% ( one of six ) by central review . 
the pmmtb recommended genetic counseling for three patients , and two received this counseling . discussion olaparib for brca1 / 2 mutant cancers and pembrolizumab for tumors with mismatch repair deficiency confirmed by immunohistochemistry or microsatellite testing . 
for example , vandetanib was adopted provisionally for the treatment of tumors with fumarate hydratase loss - of - function mutations , which led to an updated recommendation issued at the next pmmtb meeting . 
to bridge this gap , mtbs that comprise experts with a diverse knowledge base have been established at academic institutions8 - 11 but remain largely inaccessible to community oncologists and their patients . 
 patients ( n = 38 ) no treatment identified ( n = 6 ) treatment recommendation ( n = 32 ) accepted ( n = 9 ) not accepted ( n = 11 ) waiting for progression ( n = 12 ) condition deteriorated physician discretion unable to travel trial unavailable ( n = 6 ) ( n = 3 ) ( n = 1 ) ( n = 1 ) fig 3 . 
identification and acceptance of precision medicine molecular tumor board recommendations . to develop and implement the tripartite pmmtb . by separating the clinical service from the registry , we were able to rapidly launch and provide service across the region , although this method partially limited the number of reportable patients . 
moreover , the pmmtb used a separate decisionmaking process ( journal club ) for standardizing recommendations for off - label therapy , which allowed the board to focus on clinical cases rather than on time - consuming excursions to the clinical / preclinical literature . 
moreover , the monthly journal club allowed for a timely and careful review of conditions for which off - label therapies are reasonably expected to be effective . most previously described mtbs appear to be focused on a single institution or a single precision medicine clinic within the institution.8 - 12 such centralization can standardize clinical practice and facilitate access to clinical trials . 
despite this limitation , the decentralized approach is expected to be superior in fostering regional collaboration and access of patients to precision medicine . we found actionable mutations in 86% of the selected cohort . 
although this number appears high , we note that the number of patients with actionable mutations depends on the particular definition of actionable as well as on the clinical trials and approved off - label drugs available at that time . 
in addition , this statistic can be biased because physicians are expected to select for submission patient cases with actionable alterations . moreover , although we were able to identify molecular - based clinical trials for many patients , a number of these were inaccessible to patients unable to travel . 
if we limit the data by excluding out - ofstate trials , the rate of actionable mutations becomes 63% , which is similar to the 71% reported by a another tumor board.9 an important finding of this study is that clinical trials often are unavailable for patients . 
although this registry study was launched contemporaneously with nci - match , the expected competition for the two approaches was not realized partly because of the relative complexity of match and the clinical hold on accruals . 
nevertheless , our experience and that of others suggest that off - trial therapies will remain an important component of an mtb.3 thus , the tracking of patient outcomes is important to provide data on treatment outcomes by molecular profile . on the basis of our experience and that reported by others , 3 , 8 - 10 continued identification of food and drug administrationapproved therapies and maintenance of a registry that tracks patient outcomes will be important . 
 # genes osimertinib everolimus enzalutamide pd dabrafenib dabrafenib + trametinib everolimus everolimus enzalutamide everolimus key : tumor type key : genomic profile lung mutation amplification recommendation breast other deletion no alteration treated fig 4 . 
the genes with identified alterations are displayed as columns , with rows displaying the tumor profile for a given subject . areas shown in white organize genomic data and matched clinical outcomes will facilitate national efforts , such as cancerlinq , 19 , 20 the american association for cancer research genie ( genomics evidence information exchange ) project , 21 neoplasia orien ( oncology research information exchange network ) , commercial databases , and anticipated nci / moonshot data banks . few trials have compared molecular - targeted therapies versus standard of care to determine the benefit of genome sequencing . 
cancer type by color code is shown on the right , as are the number of clinical trials and nontrial treatments recommended by the precision medicine molecular tumor board , the response to therapy , and the treatment given . the chart on the bottom displays the frequency of alterations in each gene shown at the top by tumor type . 
a , adenoid cystic ; m , melanoma ; o , papillary serous ovary ; p , prostate ; s , alveolar rhabdomyosarcoma ; u , carcinoma of unknown primary . expression of hormone receptors , assigned treatments on the basis of amplifications , and used single - agent targeted therapies . 
by contrast , other studies have reported improved outcomes and enhanced cost effectiveness through a precision medicine approach.12 , 23 similarly , clinical benefit of adaptable use of nonstandard molecular - targeted therapy has been seen in lung cancer24 , 25 and by other mtbs.9 , 10 , 12 we observed a 13% objective response rate by standardized criteria and a clinical benefit rate of 38% ( partial response plus stable disease )  . 
although modest with a small sample , the observed rate compares favorably with the 5% response reported for unmatched phase i trials and the 4% to 16% response rate reported for secondline chemotherapy for colorectal cancer.26 , 27 similarly , a retrospective analysis has found improved progression - free survival without increased cost when patients are treated with a precision medicine approach.23 thus , our initial findings are consistent with these observations and can be improved by experience . this work has some limitations . 
the study was observational with a small sample size and patient responses were assessed by their treating physicians as part of standard - of - care evaluations . in addition , the majority of patients presented were of advanced - stage disease and had limited standard - of - care treatment options , which suggests that these results may not be generalizable to patients earlier in the course of their disease . 
local access to molecularly targeted therapies is the most pressing need for our patients with advanced cancer . in conclusion , we have developed and implemented a regional mtb that integrates clinical service , a registry , and a journal club . 
the principal weaknesses are that the registry is observational , largely retrospective , and does not include all patient cases presented at the tumor board . our experience demonstrates that we can identify actionable mutations for a high proportion of patients and identify off - trial targeted therapies . 
kruglyak km , lin e , ong fs : next - generation sequencing in precision oncology : challenges and opportunities . expert rev mol diagn 14 : 635 - 637 , 2014 2 . 
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tafe lj , gorlov ip , de abreu fb , et al : implementation of a molecular tumor board : the impact on treatment decisions for 35 patients evaluated at dartmouth - hitchcock medical center . 
ortiz mv , kobos r , walsh m , et al : integrating genomics into clinical pediatric oncology using the molecular tumor board at the memorial sloan kettering cancer center . 
johnson a , zeng j , bailey am , et al : the right drugs at the right time for the right patient : the md anderson precision oncology decision support platfordrug discov today 20 : 1433 - 1438 , 2015 17 . 
shah a , stewart ak , kolacevski a , et al : building a rapid learning health care system for oncology : why cancerlinq collects identifiable health information to achieve its vision . 
le tourneau c , delord jp , gonalves a , et al : molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer ( shiva ) : a multicentre , open - label , proof - of - concept , randomised , controlled phase 2 trial . 
haslem ds , van norman sb , fulde g , et al : a retrospective analysis of precision medicine outcomes in patients with advanced cancer reveals improved progression - free survival without increased health care costs . 
kaderbhai cg , boidot r , beltjens f , et al : use of dedicated gene panel sequencing using next generation sequencing to improve the personalized care of lung cancer . 
johnson be , kris mg , berry ld , et al : a multicenter effort to identify driver mutations and employ targeted therapy in patients with lung adenocarcinomas : the lung cancer mutation consortium ( lcmc )  . 
tsimberidou a - m , iskander ng , hong ds , et al : personalized medicine in a phase i clinical trials program : the md anderson cancer center initiative . 
 genomic profiling to expand management options for locally advanced esophagogastric cancers : a proof of principle case introduction the management of locally advanced esophageal and gastric cancer is an evolving field , but despite improvement in response rates and surgical techniques , recurrence rates for stage iii disease remain high.1 , 2 surgical resection is potentially curative and associated with established morbidity and mortality risk , limiting surgery to medically fit patients . 
emerging data suggest a role for positron emission tomography ( pet ) adaptive treatment strategies and possibly incorporation of trastuzumab in neoadjuvant therapy for patients with human epidermal growth factor receptor 2 ( her2 ) positive disease.3 , 4 however , additional tumor biologic features are not incorporated routinely in the management of locally advanced disease . 
large collaborative molecular characterization efforts , including the cancer genome atlas , the asian cancer research group , and commercial sequencing databases , have highlighted genomically defined subgroups.5 - 9 within gastric and esophageal cancers , 4% to 22% are reportedly microsatellite instable ( msi - h ) , a subgroup that has demonstrated significant responsiveness to immune checkpoint inhibitors ( icpis ) in small metastatic data sets.10 , 11 the potential to incorporate this approach in earlier - stage disease is understudied , and , to our knowledge , we report the first case describing a complete response to pembrolizumab in an msi - h stage iii gastroesophageal junction ( gej ) adenocarcinoma with persistent disease after definitive chemoradiotherapy ( crt )  . 
staging petcomputed tomography ( ct ) demonstrated a large and intensely avid mass at the gej ( standardized uptake value of 20.3 ) with no evidence of distant disease ( fig 2 )  . 
pet - ct scanning was repeated 10 weeks after crt completion , demonstrating partial response with residual pet - avid mass at the gej ( standardized uptake value of 7.1 ) , confirmed by endoscopic evidence of persistent disease and symptomatic dysphagia ( fig 2 )  . 
to explore additional therapeutic options , the original gej biopsy was submitted for comprehensive genomic profiling ( foundationone ) , which revealed msi - h , a high tumor mutational burden ( tmb ) of 36 mutations per dna megabase , an absence of erbb2 ( her2 ) alterations , and several additional genomic alterations ( appendix table a1 )  . 
orthogonal immunohistochemical mismatch repair testing confirmed loss of mlh1 and pms2 , and mlh1 promoter polymerase chain reaction testing confirmed mlh1 promoter hypermethylation , all consistent with a sporadic msi - h tumor ( fig 1 )  . 
 ( a ) scattered luminal necrosis as well as punctate single cell apoptoses and frequent mitoses are visible . mismatch repair immunohistochemistry demonstrates loss of ( b ) mlh1 and ( c ) pms2 , with intact ( d ) msh6 and ( e ) msh2 . 
 ( a ) scattered tumor infiltrating lymphocytes were present , at a density of approximately one lymphocyte per five to 10 tumor cells . response with resolution of pet - avid gej mass ( fig 2 )  . 
at the time of submission , he continues on pembrolizumab and remains clinically asymptomatic with ongoing complete response now over 8 months . discussion the ability to identify the optimal therapy for each patient is the hallmark of the precision medicine paradigm but has largely remained elusive in esophagogastric cancers to date . 
in the nonmetastatic setting , attempts to incorporate biologic agents , including the antiepidermal growth factor receptor monoclonal antibodies and antiangiogenesis agents , have not improved outcomes.12 , 13 the fully accrued radiation therapy oncology group ( rtog ) - 1010 trial examining a role for trastuzumab in combination with crt in locoregional esophageal / gej adenocarcinoma may ultimately be the first to identify a molecularly selected group to derive benefit from a biologic agent during neoadjuvant therapy for resectable disease . 
however , at the present time , patients with persistent disease after definitive crt who are unfit for resection represent a difficult clinical scenario with limited established approaches and 3 - year survival less than 10% in some series.14 , 15 although only a single case is presented herein , we suggest that in locally advanced unresectable esophagogastric cancer there may be clinical utility to molecular profiling to expand potential treatment options . 
the cancer genome atlas data sets for gastric and esophageal cancer are almost exclusively derived from nonmetastatic surgical samples and report rates of msi - h of 22% and 0% , respectively ( 0% for confirmed esophageal adenocarcinoma , although three of 36 among gej tumors not clearly of esophageal origin ) .5 , 6 this differs somewhat from the 6% rate of msi - h reported from the capecitabine and oxaliplatin adjuvant study in stomach cancer ( classic ) trial analysis of resected stage ii to iii gastric cancer and the 6.7% rate of msi - h identified in the european medical research council adjuvant gastric infusional chemotherapy ( magic ) trial of resectable gastroesophageal cancer.16 in both data sets , msi - h appears to confer a favorable prognosis and unclear benefit from adjuvant or perioperative chemotherapy , analogous to stage ii colon cancer.17 - 19 although analyses from ongoing metastatic and locoregional trials will refine the incidence of msi - h tumors , a portion will be msi - h and thus will be optimal candidates for immunotherapy consideration as supported by our case . 
complete resolution of [ 18f ] fluorodeoxyglucose activity was observed after three doses of pembrolizumab , and imaging is shown in coronal , sagittal , and axial planes for reference . pretreatment 10 weeks postchemoradiotherapy 10 weeks postpembrolizumab start strong biologic rationale , including in nonmetastatic locally advanced unresectable patients who have progressed on prior therapy.20 the ongoing checkmate - 577 trial ( nct02743494 ) will be important to more clearly establish the role of icpis in the adjuvant / locoregional setting after concurrent crt and surgery with persistent disease , and analyses for msi testing as well as tmb will be important.21 importantly , there is scientific rationale for moving these agents into the true neoadjuvant setting when the primary tumor remains.22 , 23 notably , our patient was not deemed a surgical candidate and would not be eligible for this trial . additional small studies incorporating programmed death - 1 inhibitors into concurrent crt will likely add more details , and there is strong scientific rationale for this approach ( nct03044613 ) .22 more broadly , predictive biomarkers for icpis are critical to identify patients who are most likely ( or least likely ) to benefit from icpi incorporation . not surprisingly , our patient harbored an elevated tmb at 36 mutations / dna megabase . 
however , a fraction of microsatellite stable gi cancers have also been shown to have high tmb.24 next - generation sequencingderived tmb has emerged as a robust biomarker for icpi benefit across several tumor types.25 - 27 in a small retrospective series of esophagogastric cancers , it was suggested that msi - h or tmb of > 14 mutations / megabase was associated with icpi benefit , although larger series will be critical to refine tmb in esophago - gastric cancers ( note that tmb determination was slightly different in this study ) .28 overall , our case highlights the potential role for genomic profiling in this nonmetastatic clinical situation and suggests a possible treatment approach . 
klempner consulting or advisory role : eli lilly , boston biomedical , celgene , astellas pharma speakers bureau : foundation medicine travel , accommodations , expenses : eli lilly the following represents disclosure information provided by authors of this manuscript . 
schrock employment : foundation medicine stock and other ownership interests : foundation medicine joseph chao consulting or advisory role : eli lilly , bayer , five prime therapeutics , boston biomedical , merck research funding : merck ( inst ) , novonco therapeutics ( inst ) siraj m . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health on microbiome stuff in non - neoplastic disease ( i ) affiliations samuel j . 
klempner , cedars - sinai medical center ; winnie wu , providence saint johns hospital , los angeles ; joseph chao , city of hope comprehensive cancer center , duarte , ca ; and alexa b . 
oppedijk v , van der gaast a , van lanschot jj , et al : patterns of recurrence after surgery alone versus preoperative chemoradiotherapy and surgery in the cross trials . 
smyth ec , fassan m , cunningham d , et al : effect of pathologic tumor response and nodal status on survival in the medical research council adjuvant gastric infusional chemotherapy trial . 
lordick f , ott k , krause bj , et al : pet to assess early metabolic response and to guide treatment of adenocarcinoma of the oesophagogastric junction : the municon phase ii trial . 
goodman ka niedzwiecki d , hall n , et al : initial results of calgb 80803 ( alliance ) : a randomized phase ii trial of pet scan - directed combined modality therapy for esophageal cancer . 
ali sm , sanford em , klempner sj , et al : prospective comprehensive genomic profiling of advanced gastric carcinoma cases reveals frequent clinically relevant genomic alterations and new routes for targeted therapies . 
gainor jf , tan ds , de pas t , et al : progression - free and overall survival in alk - positive nsclc patients treated with sequential crizotinib and ceritinib . 
le dt , durham jn , smith kn , et al : mismatch - repair deficiency predicts response of solid tumors to pd - 1 blockade . science 357 : 409 - 414 , 2017 12 . 
cunningham d , stenning sp , smyth ec , et al : peri - operative chemotherapy with or without bevacizumab in operable oesophagogastric adenocarcinoma ( uk medical research council st03 ) : primary analysis results of a multicentre , open - label , randomised phase 2 - 3 trial . 
intergroup phase iii trial of neo - adjuvant chemotherapy , followed by chemoradiation and surgery with and without cetuximab in locally advanced esophageal carcinoma : first results from the sakk 75 / 08 trial . 
smyth ec , wotherspoon a , peckitt c , et al : mismatch repair deficiency , microsatellite instability , and survival : an exploratory analysis of the medical research council adjuvant gastric infusional chemotherapy ( magic ) trial . jama oncol 3 : 1197 - 1203 , 2017 17 . 
bang yj , kim yw , yang hk , et al : adjuvant capecitabine and oxaliplatin for gastric cancer after d2 gastrectomy ( classic ) : a phase 3 open - label , randomised controlled trial . 
kelly rj , lockhart ac , jonker dj , et al : checkmate 577 : a randomized , double - blind , phase 3 study of adjuvant nivolumab ( nivo ) or placebo in pts with resected esophageal ( e ) or gastroesophageal junction ( gej ) cancer . 
rosenberg je , hoffman - censits j , powles t , et al : atezolizumab in patients with locally advanced and metastatic urothelial carcinoma who have progressed following treatment with platinum - based chemotherapy : a single - arm , multicentre , phase 2 trial . 
ku gy , sanchez - vega f , chatila w , et al : correlation of benefit from immune checkpoint inhibitors with next gen sequencing ( ngs ) profiles in esophagogastric cancer ( egc ) patients . 
 clinical utility of real - time targeted molecular proling in the clinical management of ovarian cancer : the allocate study olga kondrashova , phd1 , 2 , 3 ; gwo - yaw ho , mbchb2 , 4 , 5 ; george au - yeung , mbbs , phd1 , 5 ; leakhena leas1 ; tiffany boughtwood , mba1 ; kathryn alsop , phd5 ; giada zapparoli , msc6 , 7 ; alexander dobrovic , phd1 , 6 , 7 ; yi - an ko , msc5 ; arthur l . 
wakeeld , phd1 , 2 ; orla mcnally , mbbao , mbbch1 , 4 ; michael quinn , mbchb , mgo4 ; sumitra ananda , mbbs1 , 2 , 4 , 5 ; deborah neesham , mbbs4 ; anne hamilton , mbbs1 , 4 , 5 ; marisa grossi , mbbs5 ; alison freimund , mbbs1 , 5 ; yada kanjanapan , mbbs5 ; danny rischin , md5 ; nadia tracante5 ; david bowtell , phd1 , 5 ; clare l . 
targeted molecular and methylation proling of fresh biopsy and archived tumor samples were performed by screening for mutations or copynumber variations in 44 genes and for promoter methylation of brca1 and rad51c . results somatic genomic or methylation events were identied in 85% of all patient cases , with potentially actionable events with dened targeted therapies ( including four resistance events ) detected in 60% of all patient cases . 
on the basis of these ndings , six patients received molecularly guided therapy , three patients had unsuspected germline cancerassociated brca1 / 2 mutations and were referred for genetic counseling , and two intermediate differentiated ( grade 2 ) serous ovarian carcinomas were reclassied as low grade , leading to changes in clinical management . 
additionally , secondary reversion mutations in brca1 / 2 were identied in fresh biopsy samples of two patients , consistent with clinical platinum / poly ( adp - ribose ) polymerase inhibitor resistance . 
these include histopathologic features , gene expression patterns , driver mutations , copy - number variations ( cnvs ) , and mutational signatures.1 - 4 the survival rates for ovarian cancer have remained largely unchanged during the past three decades , despite increasing knowledge of the molecular and genetic mechanisms underlying most subtypes of ovarian cancer.5 , 6 there is , therefore , an urgent need to rapidly translate this knowledge into improved clinical outcomes . molecular proling of cancer has become increasingly helpful not only in diagnosis , disease monitoring , and prognostication but also in identication of patients who may benet from molecularly guided treatments.7 the feasibility of molecular proling in routine clinical practice has now been evaluated in unselected cancer cohorts8 and in a number of cancer types , such as lung , brain , and pancreatic cancers9 - 11 as well as ovarian cancer.12 , 13 the allocate ( australian ovarian cancer assortment trial evaluation ) study was designed to assess the feasibility of real - time multimodal molecular proling of recurrent and advanced ovarian cancers in routine clinical practice . 
 kondrashova et al context key objective this study was designed as a pilot to assess the feasibility and potential clinical utility of multimodal real - time molecular proling in the clinical management of ovarian cancer . knowledge generated we showed that molecular proling was technically possible and acceptable to patients and has a potential place in clinical management of ovarian cancer . 
we also showed that factors like timely reporting of results , availability of matched clinical trials , and early referral for patients with platinum - resistant cancers are important in achieving the maximum clinical benets of molecular proling . relevance real - time molecular proling should play a role in the clinical management of ovarian and multiple other cancer types . 
eligibility criteria included recurrent ovarian , fallopian tube , or primary peritoneal cancer of serous , mucinous , or clear cell histology , eastern cooperative oncology group performance status of 2 or less , life expectancy of 3 months or longer , suitability for enrollment in clinical trials , and residency in the state of victoria . 
informed consent was obtained from all patients , and all analyses were performed according to the national health and medical research council of australia human ethics guidelines . sample collection matched tumor ( either snap - frozen biopsies , ascites , or formalin - xed parafn - embedded [ ffpe ] samarchival ples ) and peripheral blood samples were obtained from all patients . 
a pathologist examined a hematoxylin and eosin section from the same tumor fragment to assess sample suitability and determine the proportion of neoplastic cells . unsuitable patient cases were excluded from the study ( appendix fig a1 )  . clinical data collection clinical history and follow - up data were collected where possible ( 88 of 99 patients ) from medical records and an internal hospital database . 
dna quality of ffpe samples was assessed by genomic dna fragment size analysis ( labchip ; perkinelmer , waltham , ma ) or by pothe gene gapdh lymerase chain reaction ( pcr ) of ( appendix fig a2 )  . 
custom - designed truseq amplicon ( version 1.0 ) or dual - stranded truseq amplicon low input ( version 1.5 ; illumina , san diego , ca ) ovarian cancer panels were used to assess somatic and germline mutations in 29 and 38 genes , respectively ( appendix table a1 )  . both panels underwent thorough analytic validation and accreditation to conrm that they were suitable for diagnostic purposes . 
variant effect predictor was used for variant annotation and ltering.16 analysis was restricted to variants within coding exons with 20 bp of anking intronic sequences within the genes of interest . 
droplet digital pcr was performed on the bio - rad qx - 200 system ( bio - rad , hercules , ca )  . results patient demographics between december 2013 and october 2016 , 113 patients with advanced or recurrent ovarian cancer were recruited to the allocate study from two tertiary hospitals : rwh and pmcc ( appendix fig a1 )  . 
a total of 14 patient cases ( 12.4% ) were excluded from the study , mostly because of insufcient neoplastic cellularity or poor dna quality in the tumor samples available for analysis ( appendix fig a1 )  . multiple histopathologic subtypes were analyzed in the study , which included 69 cases of hgsoc ( grade 2 to 3 ) and eight cases of lgsoc ( grade 1 ) ; the remaining subtypes included mucinous , clear cell , carcinosarcoma , transitional cell carcinoma , mixed histology , and unknown primary peritoneal carcinoma ( table 1 )  . clinical history and poststudy follow - up data were collected for 88 patients , with the data cutoff date set to october 1 , 2018 . 
on average , patients had received between one and two lines of treatment prior to their enrollment in the study ( fig 1b )  . median time from obtaining the patient samples to the reporting of mutation assay results was 87 days ( range , 11 to 357 days )  . 
tumor biopsies were attempted on 36 of the total 113 study patients ( 31.9% ) where the patient had consented and where it was possible to perform the biopsy safely . 
of these , 28 biopsies ( 77.8% ) obtained sufcient tissue for successful molecular proling , and eight failed because of insufcient neoplastic cellularity of less than 10% , as estimated by the pathologist . for the archival ffpe samples ( n = 69 ) , the level of dna fragmentation was assessed by genomic dna fragment size analysis or by pcr of the gene gapdh ( appendix fig a2 )  . 
nonconventional therapies ( eg , naturopathic therapies ) are not shown as lines of treatment . poor quality ( highly fragmented ) and were excluded from the mutation analysis . molecular and methylation proling one or more genomic variants were detected in 86.9% of all screened patient cases by mutation and cnv proling , with 85% of these being somatic . 
not all samples were tested with all three assays ( mutations , copy - number variations [ cnvs ] , and methylation ) because of dna fragmentation or limited amounts . the assays used for each particular patient case are marked with triangles above each testing panel . 
germline and somatic likely pathogenic ( 4 ) and pathogenic ( 5 ) variants , as well as somatic variants of uncertain signicance ( vus ; 3 ) , are shown . 
brca1 and brca2 class 4 or 5 mutations were detected in nine ( 9.6% ) and eight ( 8.5% ) of all screened cases ( n = 94 ) , respectively ; 12 of these were germline , and ve were somatic . 
an additional seven patients had somatic class 3 variants of uncertain signicance ( including one somatic heterozygous brca2 exon 2 to 27 deletion )  . variants in other homologous recombinationrelated genes , including palb2 , chek2 , atr , fanca , and rad51 , were identied in 10 patient cases . 
after adjusting the methylation proportions by percentage of neoplastic cells , two of the brca1 - methylated patient cases were predicted to have heterozygous methylation19 and ve were predicted to have homozygous methylation ; the rest could not be determined accurately ( appendix table a3 )  . potential clinical impact we assessed the potential clinical utility of the allocate study by annotating the detected mutations , cnvs , or methylation events using the oncokb database.22 a total of 78 potentially actionable events and four resistance events were detected in 60% ( 60 of 99 ) of the patients ( table 2 )  . the indicated targeted therapies included poly ( adpribose ) polymerase ( parp ) inhibitors for 31 detected events , including brca1 / 2 mutations ( evidence level 1 ) , brca1 or rad51c methylation ( level 3a ) , and other homologous recombination pathway events ( level 4 ) ; phosphatidylinositol 3 - kinase / mammalian target of rapamycin / akt inhibitors for four pik3ca hotspot mutations ( level 3b ) and 12 pten or arid1a mutations ( level 4 ) ; cdk2 / wee1 inhibitors for 11 ccne1 amplications ( level 4 ) ; human epidermal growth factor receptor 2 inhibitors for six erbb2 amplications ( level 4 ) ; mek inhibitors for eight kras or nf1 mutations ( level 4 ) ; ttk inhibitors for three ctnnb1 mutations ( level 4 ) ; braf inhibitors for two braf v600e mutations ( level 4 ) ; and alk / met inhibitors for one met amplication ( level 4 ; table 2 )  . improving selection of patients to determine which patients were most or least likely to benet from molecular proling , we assessed a number of including the number of potentially actionable criteria , events detected and the overall median survival in the patient cohort . 
likewise , stratication of patients by the histopathologic subtypes of their tumors did not greatly affect the number of potentially actionable events detected by the allocate testing ( fig 3c )  . clinical utility the primary aim of this study was to assess the feasibility and potential clinical utility of the molecular proling of ovarian cancer and not to determine the direct clinical benet that any patient or the cohort may derive , because the study was not directly linked to clinical trials for targeted therapies . 
nevertheless , a number of patients enrolled in the study went on to receive molecularly matched treatments on the basis of the results of the molecular proling of their tumors . as a result of molecular proling and subsequent pathology two of eight grade 2 serous carcinomas were review , reclassied from hgsoc to lgsoc , because in both cases a somatic kras mutation was detected with no tp53 mutation . 
one of these patients was subsequently enrolled in a phase ii clinical trial of anastrozole , an aromatase inhibitor , and achieved a partial response ( fig 4a )  . 
an additional six patients received matched therapy on the basis of the allocate results : one patient with high - level erbb2 amplication was treated with trastuzumab but did not respond ; one patient with lgsoc with a braf mutation was enrolled in a braf and epidermal growth factor receptor inhibitor combination clinical trial and achieved a partial response ( fig 4b ) ; and four patients with somatic ( n = 3 ) or germline ( n = 1 ) brca1 / 2 mutations were treated with parp inhibitors ( appendix table a4 )  . 
furthermore , a germline brca1 / 2 mutation was detected in three patients with hgsoc who had not previously undergone the genetic testing that has become routine for all patients with newly diagnosed hgsoc . 
these patients were subsequently referred to a familial cancer clinic for further management and cascade testing . in two of nine patients with brca1 / 2 mutations , where a recurrent fresh sample was tested , secondary mutations in brca1 / 2 were identied ( figs 4c to 4d ; appendix table a5 )  . 
 ( a ) kaplan - meier overall survival analysis of the patients from the time of referral to the allocate study stratied by duration of the primary platinum - free interval ( pfi ; n = 84 ) , where pfi could be determined . 
 ( b ) percentage of patient cases with potentially actionable events , as dened by oncokb , detected in the patients stratied by primary pfi ( n = 84 )  . 
 ( c ) percentage of patient cases with potentially actionable events identied by the allocate testing stratied by histologic subtype ( n = 99 )  . brca1 / 2 function and thereby caused platinum and parp inhibitor resistance , as has been previously reported by multiple studies.24 , 27 , 28 discussion the allocate study aimed to assess the feasibility and potential clinical utility of real - time molecular proling in the clinical management of advanced or recurrent ovarian cancer . 
we showed that events detected using multimodal targeted molecular proling panels , ( designed to identify point mutations , insertions , deletions , duplications , copynumber alterations , and methylation changes ) reected known common clinically relevant molecular events in different ovarian cancer subtypes.12 , 13 , 21 furthermore , we showed that molecular proling was clinically acceptable and feasible and had the potential to inuence clinical management of more than half of all screened patients , despite no formal linkage to open clinical trials . we showed that molecular proling has clinical utility by matching patients with targetable alterations to the corresponding targeted therapies , identifying clinically unsuspected germline familial cancerassociated mutations , reclassifying intermediate - grade serous tumors , and identifying secondary resistance mutations . we also assessed the acceptability , feasibility , and value of obtaining contemporary fresh biopsies for molecular proling . 
 ( a ) diagnosis - adjusted treatment ( aromatase inhibitor ) of one of two patient cases reclassied from high - grade to low - grade serous on the basis of the mutational ndings . 
 ( b ) recist ( version 1.1 ) measurements of the monitored tumor lesion in the patient treated with braf inhibitor ( combined with epidermal growth factor receptor inhibitor ) on the basis of the allocate ndings ( somatic braf v600e mutation ; treatment currently ongoing )  . 
the additional somatic variant is located 15 bases upstream from exon 8 and is predicted to create a new acceptor splice site ( hsf3 analysis ) , extending the length of exon 8 by 13 bases . 
taking into consideration both mutations , the reading frame of the protein is likely to be restored , with the predicted protein having an 11amino acid substitution and fouramino acid insertion . 
the study had to rely heavily on analysis of archival ffpe samples , which often pose challenges for molecular proling because of dna fragmentation and formalin - induced dna artifacts.29 , 30 although there have been a number of technologic improvements in recent years to allow generation of reliable sequencing results from ffpe samples , analysis of archival tissue may not provide up - to - date information about the current genomic status of the cancer . 
 kondrashova et al invasive way of obtaining an up - to - date snapshot of cancer molecular status.31 however , comprehensive molecular proling of liquid biopsies has technologic challenges resulting from the often low proportion of tumor - derived dna and is considerably more expensive compared with traditional biopsy proling , 32 and its feasibility still needs to be assessed for ovarian cancer . although molecular proling of cancer is becoming more acceptable in routine clinical practice , there is still a need to identify those patients who will derive the most clinical benet . 
optimized patient selection for molecular proling would maintain cost effectiveness , help reduce the potential harm of repeat biopsies , and avoid psychological stress and false hope where such testing is unlikely to alter patients management plans . 
we showed that the number of treatment lines received before study enrollment did not inuence the survival of patients and was deemed an unsuitable standalone indicator for whether the patient should undergo molecular proling of her cancer . 
it is especially important to include rare ovarian cancer subtypes in the molecular proling initiatives because of the limited treatment options available to these patients and the often - aggressive nature of such tumors.33 because molecular proling was often performed at cancer recurrence , the short survival limits the window of opportunity for patient enrollment in targeted therapy trials . 
importantly , patients with platinum - resistant cancers and rare subtypes are in most need of molecular proling as early as possible to help conrm the diagnosis and determine alternative treatment options . we showed that multimodal molecular proling was ethically acceptable , technically feasible , and logistically possible and has a potential place in the clinical management of ovarian cancer ; however , it also needs to match available drug targets to have clinical utility . 
waring provision of study material or patients : gwo - yaw ho , george au - yeung , orla mcnally , deborah neesham , marisa grossi , danny rischin , linda mileshkin collection and assembly of data : olga kondrashova , gwo - yaw ho , george au - yeung , leakhena leas , tiffany boughtwood , kathryn alsop , alexander dobrovic , yi - an ko , clare j . 
wakeeld , orla mcnally , michael quinn , sumitra ananda , deborah neesham , anne hamilton , marisa grossi , yada kanjanapan , danny rischin , nadia tracante , david bowtell , graham r . 
 allocate : molecular proling of ovarian cancer data analysis and interpretation : olga kondrashova , gwo - yaw ho , george au - yeung , giada zapparoli , arthur l . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . george au - yeung research funding : roche / genentech ( inst ) kathryn alsop research funding : astrazeneca ( inst ) alexander dobrovic honoraria : astrazeneca , amgen consulting or advisory role : astrazeneca , amgen patents , royalties , other intellectual property : provisional patent travel , accommodations , expenses : bio - rad matthew j . 
wakeeld travel , accommodations , expenses : merck sharp & dohme ( i ) michael quinn employment : tesaro anne hamilton research funding : glaxosmithkline ( inst ) , janssen ( inst ) , amgen ( inst ) , eli lilly ( inst ) , abbvie ( inst ) , clovis oncology ( inst ) alison freimund patents , royalties , other intellectual property : certied principal investigator of the clinical trial precise , which is receiving study drug and partial study funding from beigene pharmaceuticals travel , accommodations , expenses : roche yada kanjanapan travel , accommodations , expenses : merck sharp & dohme , astrazeneca / medimmune danny rischin research funding : genentech / roche , merck , amgen , regeneron , bristolmyers squibb , glaxosmithkline travel , accommodations , expenses : merck nadia tracante research funding : astrazeneca ( inst ) david bowtell honoraria : astrazeneca consulting or advisory role : astrazeneca research funding : roche / genentech , astrazeneca , beigene patents , royalties , other intellectual property : astrazeneca , genentech , roche clare l . 
scott research funding : roche / genentech , clovis oncology , sierra oncology , eisai patents , royalties , other intellectual property : royalty agreement for venetoclax ( inst ) expert testimony : astrazeneca travel , accommodations , expenses : astrazeneca other relationship : clovis oncology linda mileshkin travel , accommodations , expenses : beigene paul m . 
waring employment : dorevitch pathology , australian clinical laboratories , roche honoraria : illumina , roche , novartis , pzer , astrazeneca , merck consulting or advisory role : pillar biosciences , xing technologies travel , accommodations , expenses : pillar biosciences , dorevitch pathology no other potential conicts of interest were reported . acknowledgment we thank all of the women who participated in these research programs . the australian ovarian cancer study group ( aocs ) also acknowledges the cooperation of the participating institutions in australia and acknowledges the contribution of the study nurses , research assistants , and all clinical and scientic collaborators to the study . 
nat genet 50 : 1262 - 1270 , 2018 tothill rw , tinker av , george j , et al : novel molecular subtypes of serous and endometrioid ovarian cancer linked to clinical outcome . 
clin cancer res 14 : 5198 - 5208 , 2008 alexandrov lb , nik - zainal s , wedge dc , et al : signatures of mutational processes in human cancer . 
nature 500 : 415 - 421 , 2013 [ erratum : nature 502 : 258 , 2013 ] romero i , bast rc jr : minireview : human ovarian cancerbiology , current management , and paths to personalizing therapy . 
lancet 384 : 1376 - 1388 , 2014 goff b : measuring ovarian cancer care : why are we still failing ? gynecol oncol 136 : 1 - 2 , 2015 syn nl - x , yong w - p , goh b - c , et al : evolving landscape of tumor molecular proling for personalized cancer therapy : a comprehensive review . 
expert opin drug metab toxicol 12 : 911 - 922 , 2016 sholl lm , do k , shivdasani p , et al : institutional implementation of clinical tumor proling on an unselected cancer population . 
jci insight 1 : e87062 , 2016 barlesi f , mazieres j , merlio j - p , et al : routine molecular proling of patients with advanced non - small - cell lung cancer : results of a 1 - year nationwide programme of the french cooperative thoracic intergroup ( ifct )  . 
pfaff e , kessler t , balasubramanian gp , et al : feasibility of real - time molecular proling for patients with newly diagnosed glioblastoma without mgmt promoter hypermethylationthe nct neuro master match ( n2m2 ) pilot study . 
ross js , ali sm , wang k , et al : comprehensive genomic proling of epithelial ovarian cancer by next generation sequencing - based diagnostic assay reveals new routes to targeted therapies . 
richards s , aziz n , bale s , et al : standards and guidelines for the interpretation of sequence variants : a joint consensus recommendation of the american college of medical genetics and genomics and the association for molecular pathology . 
kondrashova o , love cj , lunke s , et al : high - throughput amplicon - based copy number detection of 11 genes in formalin - xed parafn - embedded ovarian tumour samples by mlpa - seq . 
swisher em , lin kk , oza am , et al : rucaparib in relapsed , platinum - sensitive high - grade ovarian carcinoma ( ariel2 part 1 ) : an international , multicentre , open - label , phase 2 trial . 
aziz d , etemadmoghadam d , caldon ce , et al : 19q12 amplied and non - amplied subsets of high grade serous ovarian cancer with overexpression of cyclin e1 differ in their molecular drivers and clinical outcomes . 
 allocate : molecular proling of ovarian cancer appendix patients recruited ( n = 113 ) ( n = 59 ) pmcc ( n = 54 ) excluded insufficient neoplastic ( n = 8 ) cellularity or dna quantity poor - quality dna ( n = 3 ) no sample available ( n = 2 ) died before sample collection ( n = 1 ) patient samples analyzed ( n = 99 ) ( n = 51 ) pmcc ( n = 48 ) mutation panel version 1 , 29 genes ( n = 56 ) version 1.5 , 38 genes ( n = 38 ) panel , 11 genes no . 
patients were recruited from two tertiary hospitals in melbourne : royal womens hospital ( rwh ) and peter maccallum cancer centre ( pmcc )  . biopsy or archival tumor samples were screened by mutation and copy - number variation ( cnv ) panels where possible . 
dna fragmentation levels were assessed by a qc multiplex pcr assay targeting the gapdh gene , which should generate amplied products of 100 , 200 , 300 , and 400 bp in an unfragmented dna sample . 
each sample was scored on the basis of the number of visible amplied products : 100 - bp band corresponds to dna score of 1 ; 100 - bp and weak 200 - bp bands correspond to dna score of 1.5 ; 100 - bp and 200 - bp bands correspond to dna score of 2 ; 100 - bp , 200 - bp , and weak 300 - bp bands correspond to dna score of 2.5 ; 100 - bp , 200 - bp , and 300 - bp bands correspond to dna score of 3 ; 100 - bp , 200 - bp , 300 - bp , and weak 400 - bp bands correspond to dna score of 3.5 ; and 100 - bp , 200 - bp , 300 - bp , and 400 - bp bands correspond to dna score of 4 . the mutation panel required dna with little to no fragmentation ; therefore , very poor - quality dna samples had to be excluded from the analysis , and poor - quality dna samples had to be repeated in duplicate to reduce the number of dropout target regions . kondrashova et al very poor poor moderate good primary pfi < 12 months ( n = 37 ) 12 months ( n = 47 ) time ( years ) no . 
 ( a ) kaplan - meier overall survival analysis of the patients from the time of diagnosis stratied by the duration of the primary platinumfree interval ( pfi ; n = 84 ) where pfi could be determined . 
neoplastic cellularity on the basis of pathologist review of a representative tumor section stained with hematoxylin and eosin . pathogenicity classication : score of 3 represents variant of uncertain signicance ; score of 5 , pathogenic . 
 response of a metastatic breast carcinoma with a previously uncharacterized erbb2 g776v mutation to human epidermal growth factor receptor 2targeted therapy introduction we present a case of a patient with advanced estrogen receptor / progesterone receptorpositive , her2 - negative ( by fluorescent in situ hybridization ) breast cancer , refractory to estrogen receptortargeted therapy . 
in vitro experiments showed that erbb2 g776v is an oncogenic driver , and further largescale analysis of genomic profiles of breast carcinomas suggested the existence of a distinct subtype of her2 - negative breast cancer driven by a combination of activating erbb2 kinase domain mutations and inactivating map3k1 alterations . 
these observations suggest that patients with breast cancer who have relapsed / refractory disease can benefit from cancer genomic profiling to identify unanticipated opportunities for targeted therapy , including the use of combinatorial therapies with anti - her2 agents for those cases with erbb2 mutations . management of estrogen receptor ( er ) / progesterone receptor ( pr ) - positive breast cancer refractory to endocrine therapy presents a clinical challenge , although recent studies demonstrating the acquisition of esr1 mutations1 - 5 or alterations in the pi3k / mtor pathway6 - 8 have identified mechanisms of such resistance . 
in addition , unlike the breast cancer described in this case report , where the tumor was her2 negative , a small subset of er - positive breast cancers are also her2 positive and have been dubbed triple - positive cases ; in the absence of her2 - targeted therapy , these have a poor prognosis and worse response to endocrine therapy relative to er - positive breast cancers in general , 9 - 11 but they have been reported to respond to anti - her2 agents.11 , 12 recently , several lines of investigation have demonstrated that mutations in the her2 gene ( erbb2 ) are oncogenic drivers in breast carcinoma , as evidenced by patient responses to her2 - targeted therapy . 
erbb2 mutations such as s310f , l755s , v777l , and l869q have been shown to be strong drivers associated with clinical sensitivity to her2 - targeted agents.13 - 16 in addition , erbb2 mutations have been reported to be prevalent in invasive lobular breast carcinoma , which is typically er / pr positive , her2 negative , and cdh1 mutant.17 - 19 we report on a patient with advanced breast cancer harboring a previously uncharacterized erbb2 g776v variant , who derived clinical benefit from treatment with trastuzumab plus pertuzumab ( tp ) regimens . 
furthermore , breast carcinomas with erbb2 kinase domain ( kd ) mutations are marked by cosegregation with map3k1 alterations , and the majority of breast cancer cases with the g776v mutation are er positive , which are not general features of her2 - positive or erbb2 - mutant breast cancer and , thus , may denote a distinct class of breast carcinoma driven by erbb2 kd alterations . methods comprehensive genomic profiling dna was extracted from 40 microns of formalinfixed paraffin - embedded sections , and comprehensive yakov chudnovsky runjun d . 
 genomic profiling was performed in a clinical laboratory improvement amendments certified , college of american pathologistsaccredited reference laboratory ( foundation medicine ) on hybridization - captured , adaptor ligationbased libraries to a mean coverage depth of  . 
the construct was then shuttled into the pcfg5 retroviral vector ( which includes a zeocyn resistance marker and ires - gfp sequence ) using the in - fusion hd cloning system kit ( clonetech laboratories , mountain view , ca ) , and verified using sanger sequencing . retroviral particles were produced using fnx amphotrophic packaging cells . 
cells were selected under 10 mg / ml zeocin for 3 weeks . agar colony - formation assays , wells were seeded with 7 , 000 cells and grown for 2 weeks before imaging . 
codons 23652 were defined as the extracellular domain ( ecd ) , and codons 720987 were defined as the kd.22 the p value was calculated using logistic regression , and p values were corrected for multiple testing using the falsediscovery rate23 method to generate q values . the odds ratio ( or ) for each variant type is calculated from the logistic regression coefficient ; an or  . 
1.0 indicates more frequent co - occurrence than expected by chance , whereas an pr , 1.0 indicates less frequent co - occurrence than expected by chance . results case description for western blots , cells were serum starved for 6 hours before lysate harvesting . 
lysates were probed using the following antibodies : her2 ( monoclonal , ab - 17 ) from thermo fisher scientific ( waltham , ma ) , phospho - her2 ( py1248 ) from emd millipore ( billerica , ma ) , p44 / 42 mapk and phospho p44 / 42 mapk from cell signaling technologies ( danvers , ma )  . 
in july 2003 , the patient presented with a t2 n0 m0 , er - positive , pr - positive , her2negative ( nonamplified by fluorescent in situ hybridization , 2 + by immunohistochemistry ) invasive ductal carcinoma of the left breast . 
in december 2005 , she developed metastasis to the sternum and lung , and was initially treated with ovarian suppression and zoledronate . she received radiation therapy to the sternal lesions in december 2008 and again in may 2012 . 
additional antiestrogen therapies used included letrozole ( january 2009 to january 2011 and again from february 2012 to may 2013 ) and fulvestrant ( february 2011 to january 2012 )  . in early 2013 , positron emission tomographycomputed tomography ( pet - ct ) scans showed increasing activity in the lung lesions , and the patient underwent a video - assisted thoracoscopic surgery procedure in may 2013 . 
the ca15 - 3 tumor marker level decreased with capecitabine ( down from 391 to 85 u / ml , but then rising to 213 u / ml ) and also with estradiol ( decreasing further to 74 u / ml , but then rising to 132 u / ml ; fig 1 )  . 
trastuzumab , pertuzumab , and exemestane were started in october to november 2014 , and the patient responded well to this , with marked improvement on pet - ct scan and decrease in ca15 - 3 level to 43 u / ml . 
however , by february 2015 , the ca15 - 3 level rose to 58 u / ml and the patients treatment was changed to nabpaclitaxel , trastuzumab , and pertuzumab . 
the ca15 - 3 level decreased to a nadir of 31 u / ml ( normal range for ca15 - 3 is 0 to 31 u / ml ) , the pet - ct scan showed no areas of increased uptake , and the patient remained on this regimen for a total of seven cycles . 
in december 2015 , pet - ct showed new uptake in her lung nodules , and the patient enrolled in an unrelated clinical trial . preclinical characterization of her2 ( erbb2 ) g776v the her2 g776v mutant was stably overexpressed in nih 3t3 cells by retroviral transduction . capecitabine estradiol trastuzumab pertuzumab exemestane nabpaclitaxel trastuzumab pertuzumab maintanence trastuzumab date ascopubs.org / journal / po jco precision oncology 3 fig 1 . 
immunoblotting showed that these cell lines expressed elevated levels of active phosphorylated mapk ( similar to cells expressing her2 v777l ) , but nonelevated levels of phosphorylated her2 , which may be an artifact of the overexpression system ( fig 2a )  . 
we also assayed these cell lines for colony formation in soft agar . we found that cells expressing her2 g776v formed colonies at a rate similar to that of the her2 v777l mutant ( figs 2b and 2c )  . 
together , these results suggest that g776v is an activating mutation , causing increased signaling through the her2 / mapk pathway and allowing for anchorage - independent growth of nih 3t3 cells . genomic co - occurrence of map3k1 alterations with erbb2 alterations among the 10 , 790 breast carcinoma cases that have undergone cgp in our laboratory , 1 , 329 ( 12.3% ) have been found to harbor alterations in erbb2 , including 1 , 041 cases ( 9.6% ) with erbb2 amplification , 229 cases ( 2.1% ) with erbb2 short variants ( substitutions or inframe insertions or deletions ) , and 59 ( 0.5% ) with both ( table 1 )  . 
to identify additional genomic variants that may cooperate with erbb2 mutations in the pathogenesis of her2 - negative breast cancer , we calculated the co - occurrence of alterations in each of 345 genes profiled at foundation medicine with various alterations in erbb2 ( data supplement )  . 
as discussed , cdh1 alterations have been reported to co - occur with erbb2 mutations in the context of invasive lobular breast carcinoma.17 - 19 tbx3 has also been reported to be enriched for mutations in lobular breast carcinoma , 25 as well in neuroendocrine breast cancer , 26 but its role in breast cancer is not entirely clear : it has been suggested to be a tumor suppressor27 , 28 and an oncogene29 , 30 in different studies . 
we chose to further examine the tumor suppressor gene map3k1 , which was mutated in the patient described in this case report . alterations in map3k1 co - occur with erbb2 short variants significantly more frequently than expected by chance in breast cancer cases profiled in our laboratory , but erbb2 alterations , in general , are not significantly enriched for cooccurrence with map3k1 variants ( table 1 )  . furthermore , although activating mutations in erbb2 are found in both the ecd and the kd , 21 only kd mutations , and not ecd mutations , are significantly enriched for co - occurrence with map3k1 alterations ( table 1 )  . 
map3k1 alterations have been identified in 513 ( 4.8% ) of the 10 , 790 breast carcinoma cases profiled at foundation medicine and at a similar frequency range of 0% to 8% of breast cancers in several large - scale sequencing studies.27 , 31 - 33 map3k1 inactivation via mutation or copy number loss has been reported to be particularly prevalent in the luminal a subtype of breast cancer , which is distinct from the subtype that is characterized by erbb2 amplification.33 , 34 consistent with this , among the breast carcinoma cases profiled using our hybrid capture based assay , erbb2 copy number alterations co - occur with map3k1 variants significantly less frequently than expected by chance ( table 1 )  . 
notably , although subtype data were not available for the breast cancer cases profiled in our laboratory , logistic regression g776va v777l her2 wt parental ascopubs.org / journal / po jco precision oncology fig 2 . 
 ( a ) western blot showing expression of active phosphorylated and total her2 and mapk in untransduced ( parental ) nih 3t3 cells and those transduced with wt human her2 or the indicated mutants . 
g776va and g776vb are duplicate cell lines that were transduced independently . ( b ) representative images and ( c ) quantification of soft - agar colony formation ( anchorage - independent growth ) by untransduced ( parental ) nih 3t3 cells and those transduced with wt human her2 or the indicated mutants . 
 analysis to control for alteration status of the genes reported to be most frequently mutated in luminal a breast cancer ( ie , tp53 , pik3ca , gata3 , and cdh1 ) 33 retained significant enrichment of cooccurrence of map3k1 alterations with all erbb2 short variants and with erbb2 kd short variants ( table 2 )  . 
this indicates that the co - occurrence of erbb2 and map3k1 variants in a subset of breast carcinoma cases is independent of the status of luminal aassociated genes and cannot be attributed solely to these cases belonging to the luminal a subtype . 
these findings suggest that there may be a particular subtype of her2 - negative , predominantly er - positive breast cancer driven by a combination of activating erbb2 kinase domain mutations and inactivating map3k1 alterations . discussion this is the first demonstration of clinical response to tp regimens ( tp plus exemestane followed by tp plus nab - paclitaxel ) in a patient with a her2 kinase domain mutation ( erbb2 g776v ) and expands our knowledge of treatment options for patients with metastatic breast cancer containing erbb2 mutations . 
although it cannot be excluded that the clinical benefit was due to the exemestane or nab - paclitaxel , these findings are consistent with four previous studies that have reported responses of patients with erbb2 - mutant ( s310f , l755s , v777l , l869q ) breast cancer to antiher2 agents including antibodies and tyrosine kinase inhibitors , with a cytotoxic chemotherapy backbone in three of the four cases.13 - 16 in addition , studies in cultured cells and animal xenograft models have shown that multiple erbb2 mutations associated with erbb2 amplification - negative breast cancer are activating , oncogenic , and sensitive to the irreversible pan - her inhibitor neratinib and , in some cases , to the reversible pan - her inhibitor lapatinib and the anti - her2 antibody trastuzumab.21 the effects of the g776v mutation on her2 functions had not previously been characterized in published studies , although one study reported that this alteration is untargetable.35 however , including the substitution similar alterations , g776s36 and the compound substitution and insertion g776vinsc , 37 - 39 have been shown to be activating . 
 her2 - targeted agents have shown high rates of clinical benefit in her2 - positive breast cancers and are approved for both er - negative and erpositive patients.11 , 12 the clinical data for her2negative breast carcinoma cases driven by erbb2 mutations are considerably more limited . 
a recent large - scale study of nonamplification genomic alterations in erbb2 in breast cancer18 reported three patients who responded to anti - her2 therapy , two with er - positive tumors and one with triple - negative cancer.13 - 15 , 18 consistent with this , the patient we report here had er - positive cancer , and additional analysis showed that 80% ( four of five ) of breast cancers profiled at foundation medicine and found to carry the erbb2 g776v mutation were er positive . 
the previous study reported that several genes are frequently coaltered with erbb2 in erbb2 - nonamplified breast cancers , particularly the tumor suppressor tp53 and the oncogene pik3ca.18 here , we show that erbb2 - nonamplified breast carcinomas driven by erbb2 kinase domain mutations specifically are significantly enriched for co - alteration with the tumor suppressor map3k1 . 
although frequent alteration of map3k1 in the luminal / erpositive breast cancer subtype has been reported , 33 the current study provides evidence of association between erbb2 and map3k1 mutations independent of subtype and suggests that activating mutations in the erbb2 kinase domain may cooperate with inactivation of map3k1 to promote cancer progression . 
additional work will also be needed to elucidate the effects of er status on the clinical efficacy of her2 - targeted agents in erbb2 - mutated breast cancer . in this patients case , the clinical decision to use tp - based regimens was based on prior reports of similar erbb2 mutations in breast cancer or nsclc.36 - 42 , 46 , 48 the preclinical experiments reported here confirmed that erbb2 g776v is an activating mutation , and the patient had a good clinical outcome on tp - based therapy . 
this study adds to a body of evidence supporting the use of her2 - targeted therapy in patients with metastatic breast cancer with erbb2 mutations , although given that the tp - based regimens in this case included exemestane or nab - paclitaxel that may have significantly contributed to the clinical benefit , caution must be exercised in applying these findings to the treatment of other patients . 
for more information about ascos conflict of interest policy , please refer to or po.ascopubs.org / site / ifc . yakov chudnovsky employment : foundation medicine stock and other ownership interests : foundation medicine travel , accommodations , expenses : foundation medicine runjun d . 
schrock employment : foundation medicine stock and other ownership interests : foundation medicine caitlin connelly employment : foundation medicine kyle gowen employment : foundation medicine stock and other ownership interests : foundation medicine travel , accommodations , expenses : foundation medicine garrett m . 
miller employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine patents , royalties , other intellectual property : receive periodic royalties related to t790m patent awarded to memorial sloan - kettering cancer center jeffrey s . 
ross employment : foundation medicine leadership : foundation medicine stock and other ownership interests : foundation medicine honoraria : pfizer , emd merck serono research funding : foundation medicine siraj m . 
ali employment : foundation medicine stock and other ownership interests : exelixis , blueprint medicines , agios patents , royalties , other intellectual property : patents via foundation medicine , patents via seres health related to microbiome in non - neoplastic disease ( inst ) ron bose honoraria : genentech , novartis consulting or advisory role : genentech affiliations yakov chudnovsky , alexa b . 
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tokunaga e , kimura y , oki e , et al : akt is frequently activated in her2 / neu - positive breast cancers and associated with poor prognosis among hormone - treated patients . 
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schwab rb , koehler m , ali sm , et al : genomic profiling and treatment of her2 + , er + , pgr + triple positive breast cancer : a case report and literature review . 
ross js , slodkowska ea , symmans wf , et al : the her - 2 receptor and breast cancer : ten years of targeted antiher - 2 therapy and personalized medicine . 
ali sm , alpaugh rk , downing sr , et al : response of an erbb2 - mutated inflammatory breast carcinoma to human epidermal growth factor receptor 2 - targeted therapy . 
ben - baruch ne , bose r , kavuri sm , et al : her2 - mutated breast cancer responds to treatment with single - agent neratinib , a second - generation her2 / egfr tyrosine kinase inhibitor . 
chumsri s , weidler j , ali s , et al : prolonged response to trastuzumab in a patient with her2 - nonamplified breast cancer with elevated her2 dimerization harboring an erbb2 s310f mutation . 
grellety t , soubeyran i , robert j , et al : a clinical case of invasive lobular breast carcinoma with erbb2 and cdh1 mutations presenting a dramatic response to anti - her2 - directed therapy . 
ross js , wang k , sheehan ce , et al : relapsed classic e - cadherin ( cdh1 ) - mutated invasive lobular breast cancer shows a high frequency of her2 ( erbb2 ) gene mutations . 
ross js , gay lm , wang k , et al : nonamplification erbb2 genomic alterations in 5605 cases of recurrent and metastatic breast cancer : an emerging opportunity for anti - her2 targeted therapies . 
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shimamura t , ji h , minami y , et al : non - small - cell lung cancer and ba / f3 transformed cells harboring the erbb2 g776insv_g / c mutation are sensitive to the dual - specific epidermal growth factor receptor and erbb2 inhibitor hki - 272 . 
suzuki t , fujii a , ohya j , et al : antitumor activity of a dual epidermal growth factor receptor and erbb2 kinase inhibitor mp - 412 ( av - 412 ) in mouse xenograft models . 
wang se , narasanna a , perez - torres m , et al : her2 kinase domain mutation results in constitutive phosphorylation and activation of her2 and egfr and resistance to egfr tyrosine kinase inhibitors . 
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kris mg , camidge dr , giaccone g , et al : targeting her2 aberrations as actionable drivers in lung cancers : phase ii trial of the pan - her tyrosine kinase inhibitor dacomitinib in patients with her2 - mutant or amplified tumors . 
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sohal , md , mph1 a 53 - year - old woman with no signicant medical history presented to her primary care physician with fatigue and anorexia in may 2016 . 
she subsequently underwent a liver biopsy in september 2016 , and the pathology was consistent with adenocarcinoma ( strongly and diffusely positive for ck7 , with weak , patchy expression for ck20 ; programmed death ligand 1 , 2% )  . 
she was diagnosed with cancer of unknown primary , despite extensive workup revealing caudal - type homeobox 2 , thyroid transcription factor 1 , napsin a , gata - 3 , arginase , receptor 2 , and human epidermal growth factor mammaglobin negativity on immunohistochemical staining and no lesions on esophagogastroduodenoscopy or repeat colonoscopy ; however , the pathology was thought to be suggestive of a biliary origin . she received three doses of uorouracil and oxaliplathowever , she deteriorated clinically . 
genomic sequencing performed on her initial biopsied tissue ( foundationone ; foundation medicine , cambridge , ma ) was notable for mutations in braf v600e , apc , and cdkn2a ( table 1 )  . 
her case was reviewed at our genomics tumor board in december 2016 , and the recommendation was made to trial ( nci - match [ national pursue either a clinical cancer institute molecular analysis for therapy choice ; clinicaltrials.gov identier : nct02465060 ] or mypathway [ clinicaltrials.gov identier : nct02091141 ] ; each trial , the vemurafenib arm was open and available at the time ) or off - label treatment with dabrafenib and trametinib based on the asco 2016 update.1 at our institution , if two outside experts agree with the scientic data presented , off - label therapy can be approved on a case - by - case basis . given that she was not a clinical trial candidate because of the high bilirubin , off - label treatment with dabrafenib and trametinib was started in december 2016 . 
it is important to note that hepatic dysfunction , although closely monitored , is not a contraindication to initiating treatment with dabrafenib and trametinib . although serum alt elevations can occur in approximately 35% to 42% of patients receiving combination therapy , elevations greater than ve times the upper limit of normal occur in only 4% of such patients . 
in addition , there have been no instances of clinically apparent acute liver injury or hepatic failure in prelicensure studies , and there have been no published reports of clinically apparent hepatotoxicity with either drug.2 our patient was noted to experience clear clinical benet , with her total bilirubin and ast normalizing within just 2.5 months of treatment initiation and the remainder of her liver function enzymes continuing to downtrend . 
she had remarkable disease response , with radiographic ( fig 1 ) and clinical improvement until may 2018 ( a duration of almost 18 months ) , at which point there was concern about radiographic progression . 
cisplatin and gemcitabine were considered but not agreed to by the patient and family because of prior potential failure of oxaliplatin . her other option was to pursue a phase i clinical trial at an outside institution . 
her case was again discussed at the genomics tumor board in july 2018 , at which time there was deemed to be no targetable therapeutic option beyond the braf alteration , for which she had already been treated . 
interestingly , her second biopsy did identify some additional , albeit nontherapeutic , alterations not seen on the rst : rictor amplication and mtap loss of exons 6 to 8 . 
in a study analyzing these alterations in melanoma cell lines , it was found that v600e - mutant braf inhibits mammalian target of rapamycin complex 2induced phosphorylation of akt ser473 in the presence of pten . 
therapeutic implications of genomic sequencing , november 2016 sadaps and sohal fda - approved therapies genomic alterations detected * patients tumor type another tumor type potential clinical trials braf v600e none cobimetinib dabrafenib regorafenib nct01827384 nct01531361 ( phase i , targeting braf ) nct02034110 ( phase ii , targeting braf , mek ) trametinib nct02465060 ( phase ii , nci - match ) vemurafenib nct02693535 ( phase ii , tapur study ) apc r856c cdkn2a / b : cdkn2a loss exon 1 and cdkn2b loss none none none none none none abbreviations : fda , us food and drug administration ; nci - match , national cancer institute molecular analysis for therapy choice ; tapur , targeted agent and proling utilization registry . * variants of unknown signicance , 10 ; microsatellite stable ; low tumor mutational burden , 4 . discovered rictor amplication contributed to the development of braf inhibitor resistance . cleveland clinic to allow publication of this case have been obtained . per the request of the patient and her family and preliminary data extrapolated from the keynote 022 phase ii trial ( clinicaltrials.gov identier : nct02130466 ) , pembrolizumab ( via compassionate use ) was added to her regimen of dabrafenib plus trametinib starting in august 2018 . 
although high tumor mutational burden ( tmb ) has been demonstrated to be a useful biomarker in predicting immunotherapy responsiveness , 4 , 5 most studies ( eg , mypathway ) have used much higher tmb cutoffs , generally of at least 16 or more mutations per megabase , which far exceeds the tmb score obtained for our patient in either of her next - generation sequencing reports . 
she died in january 2019 , secondary to septic shock with multiorgan failure . because the patient died , consent could not be obtained ; however , no identifying personal health information has been disclosed . 
patients who receive standard - of - care gemcitabine and cisplatin chemotherapy have an overall survival ( os ) benet of 3.6 months when compared with gemcitabine monotherapy.6 even then , most patients develop treatment resistance within a few months , and median os remains less than 1 year . 
outcomes for second - line therapies have not been promising , with median progression - free survival of only a few months.7 - 13 recent advances in precision medicine have allowed for the identication of potentially targetable mutations in the effort to improve therapeutic outcomes in this population . promising targets identied in cholangiocarcinoma thus far include idh 1 / 2 , fgfr , her2 , and , the focus of our patient case , braf mutations.14 braf encodes protein kinases that function downstream of ras as part of the mitogenactivated protein kinase signaling cascade , which promotes cell proliferation , survival , and transformation . 
therapeutic implications of repeat genomic sequencing , june 2018 fda - approved therapies genomic alterations detected * patients tumor type another tumor type potential clinical trials braf v600e none cobimetinib dabrafenib regorafenib trametinib vemurafenib nct02091141 ( phase ii , mypathway ) nct02070549 ( phase i , targeting mek ) nct01989585 ( phase i / ii ) nct02428712 ( phase i / ii , targeting braf / craf ) nct02693535 ( phase ii , tapur study ) nct02034110 ( phase ii , targeting braf , mek ) apc r856c cdkn2a / b : cdkn2a loss exon 1 and cdkn2b loss riktor amplication none none none none none none none none nct02795156 ( phase ii ) nct02466802 ( phase i ) nct02097225 ( phase i ) nct01531361 ( phase i ) nct02576444 ( phase ii ) nct02142803 ( phase i ) nct03065062 ( phase i ) nct02159989 ( phase i ) nct02719691 ( phase i ) nct02583542 ( phase i / ii ) mtap loss of exons 6 to 8 none none none abbreviations : fda , us food and drug administration ; tapur , targeted agent and proling utilization registry . * variants of unknown signicance , 10 ; microsatellite stable ; low tumor mutational burden , 1 . and hyperactivate its downstream signaling.15 braf mutations are reported in up to 22% of biliary tract cancers , among which it is most commonly seen in intrahepatic cholangiocarcinoma . 
braf mutations have typically been associated with poor prognosis in patients with cholangiocarcinoma , including worse os , higher tumor grade , and chemotherapy resistance.16 there have been a few case reports on the use of dabrafenib and trametinib in cholangiocarcinoma , describing remarkable clinical and radiographic responses in patients who experienced progression during standard - of - care chemotherapy and who continued to do well 5 to 9 months out.17 , 18 most recently , a phase ii international clinical trial of dabrafenib plus trametinib in braf - mutated rare gi cancers was reported as a late - breaking presentation at the 30th european organisation for research and treatment of cancernational cancer instituteamerican association for cancer research symposium on molecular targets and cancer therapeutics . 
sohal honoraria : foundation medicine consulting or advisory role : perthera research funding : novartis ( inst ) , celgene ( inst ) , oncomed ( inst ) , bayer healthcare pharmaceuticals ( inst ) , genentech ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) , loxo ( inst ) travel , accommodations , expenses : foundation medicine no other potential conicts of interest were reported . references flaherty k , davies ma , grob jj , et al : genomic analysis and 3 - y efcacy and safety update of combi - d : a phase iii study of dabrafenib ( d ) + trametinib ( t ) vs d monotherapy in patients with unresectable or metastatic braf v600e / k - mutant cutaneous melanoma . 
plos one 7 : e42598 , 2012 chan ta , yarchoan m , jaffee e , et al : development of tumor mutation burden as an immunotherapy biomarker : utility for the oncology clinic . 
ann oncol 30 : 44 - 56 , 2019 legrand f , gandara d , mariathasan s , et al : association of high tissue tmb and atezolizumab efcacy across multiple tumor types . 
j clin oncol 36 , 2018 ( suppl ; abstr 12000 ) valle j , wasan h , palmer dh , et al : cisplatin plus gemcitabine versus gemcitabine for biliary tract cancer . 
croitoru a , gramaticu i , dinu i , et al : fluoropyrimidines plus cisplatin versus gemcitabine / gemcitabine plus cisplatin in locally advanced and metastatic biliary tract carcinomaa retrospective study . 
fornaro l , vivaldi c , cereda s , et al : second - line chemotherapy in advanced biliary cancer progressed to rst - line platinum - gemcitabine combination : a multicenter survey and pooled analysis with published data . 
brugnara s , sicher m , bonandini em , et al : treatment with combined dabrafenib and trametinib in brafv600e - mutated metastatic malignant melanoma : a case of long - term complete response after treatment cessation . 
loaiza - bonilla a , clayton e , furth e , et al : dramatic response to dabrafenib and trametinib combination in a braf v600e - mutated cholangiocarcinoma : implementation of a molecular tumour board and next - generation sequencing for personalized medicine . 
presented at the 30th eortc - nci - aacr symposium on molecular targets and cancer therapeutics , dublin , ireland , november 13 - 16 , 2018 ( abstr 2 ) 20 . 
george , md1 ; and susan halabi , phd8 purpose androgen receptor splice variant 7 ( ar - v7 ) detection in circulating tumor cells ( ctcs ) is associated with a low probability of response and short progression - free ( pfs ) and overall survival ( os ) in men with metastatic castration - resistant prostate cancer ( mcrpc ) treated with enzalutamide or abiraterone . 
os , conrmed prostate - specic antigen ( psa ) , and objective radiologic responses were secondary end points . results we enrolled 118 men with mcrpc treated with abiraterone or enzalutamide , 51 of whom received subsequent docetaxel or cabazitaxel . 
all patients provided written informed consent under stitutional review board approval at all participating centers within the department of defensefunded prostate cancer clinical trial consortium.16 study design and assessments prophecy is a prospective multicenter study evaluating the ability of baseline ( pretreatment ) ar - v7 status in ctcs to predict treatment outcomes with abiraterone or enzalutamide as well as subsequent taxane chemotherapy upon disease progression . 
cellsearch ( menarini silicon biosystems , huntington valley , pa ) ctc enumeration was performed at these time points for all patients and processed in a college of american physicians / clinical laboratory improvement amendmentsapproved central laboratory at memorial sloan kettering cancer center.17 , 18 treatment selection was at the discretion of the treating physician without knowledge of ar - v7 status . 
all data sets were separately sent to the study statistician ( s.h. ) , who unblinded the data after database lock . analysis of ctcs ctcs were analyzed in two central laboratories , each blinded to the results of the other . 
baseline pretaxane characteristics of patients enrolled according to epic sciences ar - v7 status based on ar - v7 detection after abiraterone or enzalutamide and before taxane epic sciences ar - v7 status ( % ) positive ( n = 8 ) negative ( n = 42 ) 62 - 79 45 - 87 6 - 881 96.5 1 - 850 0 - 325 characteristic age , years median range race white black other gleason sum 8 - 10 kps 90 poor - risk feature psa , ng / ml median range taxane used docetaxel cabazitaxel months median range hemoglobin , 12 g / dl elevated alp elevated baseline serum ldh presence of liver metastasis presence of clinically signicant pain requiring cellsearch ctcs , cells per 7.5 ml opiates range median , % ( n = 32 ) psadt , 3 months prior docetaxel for mhspc  . 
20 bone metastases time from ar - v7 sample to chemotherapy start , 0 - 17 0 - 33 abbreviations : alp , alkaline phosphatase ; ar - v7 , androgen receptor splice variant 7 ; ctc , circulating tumor cell ; kps , karnofsky performance score ; ldh , lactate dehydrogenase ; mhspc , metastatic hormone - sensitive prostate cancer ; psa , prostate - specic antigen ; psadt , prostate - specic antigen doubling time . registration to clinical or radiographic progression or death , whichever occurred rst . 
radiographic progression was assessed at each center using pcwg3 - modied recist ( version 1.1 ) soft tissue and bone scan criteria.22 clinical progression was dened as a composite end point including death , escalating pain or other symptomatic progression , initiation of new systemic therapy , or a skeletal - related event . secondary clinical end points included conrmed 50% prostate - specic antigen ( psa ) decline , radiographic response per recist ( verson 1.1 ) , 23 and os , and these same outcomes for subsequent taxane chemotherapy . data analysis the primary objective of prophecy was to validate that patients with pretreatment ar - v7negative ctcs have prolonged pfs with abiraterone or enzalutamide compared with ar - v7positive patients . 
with longer follow - up , analyses of the time - toevent end points ( pfs and os ) were also updated , and patients who received taxane chemotherapy were observed for response , radiographic progression , and death . 
details regarding study design have been published elsewhere.9 patients with no evaluable ctcs were considered ar - v7 negative , and all patients with sufcient blood collection were analyzed regardless of their evaluable ctcs . 
in secondary analyses , the proportional hazards model was used for assessing the prognostic value of ar - v7 status for pfs and os after adjusting for validated prognostic factors ( risk score ) .14 , 15 , 24 for taxane outcomes , pfs was dened from the date of starting chemotherapy to clinical or radiographic progression or death , whichever occurred rst . 
no power or sample size analysis is provided for this secondary descriptive analysis , because prophecy was powered around the primary objective and previously reported . between may 2015 and january 2017 , we prospectively enrolled 118 men with high - risk mcrpc who were initiating treatment with abiraterone , enzalutamide , or both at one of ve academic medical centers . 
baseline characteristics of the cohort were previously published and included 36 men who had received prior enzalutamide or abiraterone therapy.9 of these 118 men treated with subsequent ar inhibitor therapy , 51 experienced progression and were treated with taxane chemotherapy , including docetaxel ( n = 42 ) or cabazitaxel ( n = 9 ; consort diagram provided in appendix fig a1 )  . 
baseline characteristics of these patients at the time of taxane chemotherapy are listed in table 1 based on epic sciences ar - v7 status and appendix table a1 based on johns hopkins ar - v7 status . 
as of the nal database lock on october 15 , 2019 , median follow - up times from study registration ( before abiraterone or enzalutamide treatment ) and taxane initiation were 35 and 23 months , respectively . 
table 2 and figure 1 summarize the results of pfs and os by baseline ar - v7 status for each ctc assay . conrmed 50% psa declines were observed in 11% and 30% of patients with ar - v7positive and ar - v7negative disease by johns hopkins assay , respectively , and radiographic responses ( complete or partial responses by recist [ version 1.1 ] criteria ) were seen in 7% and 9% of patients , respectively . 
results were unchanged when two patients with psa - only progression were considered censored ( appendix table a3 )  . os did not differ from the start of taxane chemotherapy by ar - v7 status . 
table 3 and figure 2 summarize the results of pfs and os by baseline ar - v7 status for each ctc assay . conrmed 50% psa responses with taxane therapy were observed in 36% and 32% of patients with ar - v7positive versus ar - v7negative disease by johns hopkins assay , respectively , and radiographic responses ( complete or partial responses by recist [ version 1.1 ] ) were observed in 10% and 20% of patients , respectively . 
conrmed 50% psa responses were observed in 40% and 33% of those with ar - v7positive versus ar - v7negative disease by epic sciences nuclear assay , respectively , and radiographic responses ( complete or partial responses by recist [ version 1.1 ] ) were observed in 13% and 17% of patients , respectively ( appendix fig a2 )  . 
 a pre - abi / enza at progression on abi / enza at progression on taxane nuclear localized ar - v7 ctc total ctc nuclear localized ar - v7 ctc nuclear localized ar - v7 ctc total ctc total ctc 123456789 2345789 * * * * * * * * patient id patient id patient id armstrong et al 123456789 2345789 patient id patient id patient id 123456789 2345789 patient id patient id patient id * * * * * * * fig 3 . 
bar plot demonstrating heterogeneity of androgen receptor splice variant 7 ( ar - v7 ) expression in circulating tumor cells ( ctcs ) by either the johns hopkins ( jhu ) messenger rna assay or the epic sciences nuclear protein assay collected from men in the prophecy study at one of three time points : ( a ) before abiraterone ( abi ) or enzalutamide ( enza ) therapy , ( b ) at progression during abiraterone or enzalutamide treatment , and ( c ) at progression during subsequent taxane chemotherapy . 
for the epic sciences nuclear protein assay , approximately 1 ml of blood is analyzed , and total and nuclear - localized ar - v7positive ctcs are expressed per 1 ml of blood . 
 ( * ) no data . disease pretreatment who received abiraterone or enzalutamide and pretaxane therapy . finally , we examined how ar - v7 changes during the treatment course from before abiraterone or enzalutamide to progression and then after progression during taxane chemotherapy . 
at baseline , ar - v7 positivity was 10% versus 24% by epic sciences and johns hopkins assays , respectively , with a majority of men with ar - v7positive disease by epic sciences ( nine of 11 ; 82% positive agreement ) also testing positive by johns hopkins assay . johns hopkinspositive , epic sciencesnegative results were observed , particularly in those men with low epic sciences ctcs or nonnuclear ar - v7 protein expression . although a majority of ctcs in men with mcrpc were ar - v7 negative , even in those with ar - v7positive disease , the proportion of ar - v7positive cells ranged from 1% to 100% ( median , 20% ; fig 3 )  . 
at progression during taxane chemotherapy , 33% ( four of 12 ) and 48% ( 12 of 25 ) of evaluable men had ar - v7 detected by epic sciences and johns hopkins criteria , respectively ( appendix table a4 )  . 
these results conrm previously published data showing ar - v7positive disease remains sensitive to taxane chemotherapy.11 - 13 in the secondor third - line mcrpc setting , cabazitaxel improves os and should be considered a reasonable third - line treatment option , 5 and docetaxel or cabazitaxel are effective treatments after progression with abiraterone or enzalutamide , with pfs estimates of 4 to 6 months in these poor - risk men.14 , 24 , 26 , 27 the results are particularly important with regard to current practice , given the recent proven benet and use of these same ar inhibitors in the metastatic hormone - sensitive pc and nonmetastatic crpc settings , where ar therapy cross - resistance concerns remain when a patient experiences progression to mcrpc during therapy.28 - 32 a majority of men with ar - v7positive disease by epic sciences assay ( nine [ 82% ] of 11 ) were also positive by johns hopkins assay ; however , 17 ( 60% ) of 28 patients with positive disease by johns hopkins assay were negative by epic sciences assay at baseline . 
these differences largely reect the differential sensitivities of the assays for ar - v7 detection in ctc - based rna expression versus protein and the distinction between nuclear versus cytoplasmic localization . 
some patients developed ar - v7positive disease at progression during abiraterone or enzalutamide treatment , despite being ar - v7 negative at baseline , whereas some men with ar - v7positive disease converted to arv7negative status at progression , illustrating the need to assess ctc biomarker status at each management decision point ( fig 3 )  . 
a limitation of our study includes the lack of random assignment to taxane or ar therapy based on arv7 test results , and as such , our results show a prognostic rather than predictive utility . 
 armstrong et al support supported by a grant from the prostate cancer foundation and movember ; by the department of defense prostate cancer clinical trials consortium , which provided infrastructural support ; by the national institutes of health and grant 1r01ca233585 - 01 , duke cancer institute ( dci ) grant no . 
p30 ca014236 , and dci shared resources for biostatistics , ow cytometry , and sequencing and genomic technologies ( a.j.a. ) ; in part by department of defense grants no . 
george , susan halabi manuscript writing : all authors final approval of manuscript : all authors accountable for all aspects of the work : all authors consulting or advisory role : bayer , sano , dendreon , medivation , janssen biotech , pzer , astellas scientic and medical affairs , clovis oncology , astrazeneca speakers bureau : dendreon , bayer research funding : dendreon ( inst ) , sano ( inst ) , bayer ( inst ) , pzer ( inst ) , novartis ( inst ) , janssen oncology ( inst ) , medivation ( inst ) , astellas pharma ( inst ) , gilead sciences ( inst ) , roche / genentech ( inst ) , active biotech ( inst ) , bristol myers squibb ( inst ) , constellation pharmaceuticals ( inst ) , merck ( inst ) patents , royalties , other intellectual property : circulating tumor cell novel capture technology ( inst ) travel , accommodations , expenses : dendreon , janssen biotech , bayer , astellas scientic and medical affairs jun luo consulting or advisory role : sun pharma , janssen oncology , tolero pharmaceuticals research funding : sano ( inst ) , orion pharma ( inst ) , mirati therapeutics ( inst ) , gilead sciences ( inst ) , astellas pharma ( inst ) , constellation pharmaceuticals ( inst ) , calibr ( inst ) , cardiff oncology ( inst ) patents , royalties , other intellectual property : coinventor of a technology assigned to johns hopkins university , which licensed to tokai pharmaceuticals ( inst ) ; coinventor of a technology licensed to qiagen ( inst ) ; coinventor of a technology licensed to a&g pharmaceuticals ( inst ) david m . 
nanus consulting or advisory role : roche / genentech research funding : novartis ( inst ) , boehringer ingelheim ( inst ) , zenith epigenetics ( inst ) , astrazeneca ( inst ) , immumedics ( inst ) , janssen ( inst ) , clovis oncology ( inst ) , pzer ( inst ) paraskevi giannakakou employment : novartis ( i ) stock and other ownership interests : novartis ( i ) patents , royalties , other intellectual property : coinventor on international patent application docket no . 
danila honoraria : angle , bayer , screencell , janssen oncology , pzer , aximmune , pzer , clovis oncology , astellas pharma consulting or advisory role : angle , bayer , sanador , aximmune , pzer , clovis oncology , astellas pharma , janssen scientic affairs research funding : prostate cancer foundation , genentech , janssen research & development ( inst ) patents , royalties , other intellectual property : gene expression prole associated with prostate cancer travel , accommodations , expenses : cambridge healthtech institute , prostate cancer foundation , screencell , stopcancer , american austrian open medical institute , janssen biotech , genzyme , pzer , janssen scientic affairs , astellas pharma andrew j . 
berry honoraria : pzer , merck , genomic health , janssen oncology consulting or advisory role : merck , pzer , genomic health , janssen oncology research funding : merck ( inst ) travel , accommodations , expenses : merck , pzer , genomic health , janssen oncology tian zhang leadership : capio biosciences ( i ) , archimmune therapeutics ( i ) stock and other ownership interests : capio biosciences ( i ) , archimmune therapeutics ( i ) , nanorobotics ( i ) honoraria : exelixis , genentech / roche , mjh life sciences , pacic genuity consulting or advisory role : janssen , genentech / roche , sano , exelixis , astrazeneca , pzer , bristol myers squibb , foundation medicine , pharmacyclics , amgen , merck , seattle genetics speakers bureau : exelixis , genentech / roche , genomic health , sano research funding : janssen ( inst ) , acerta pharma ( inst ) , pzer ( inst ) , merrimack ( inst ) , stem centrx ( inst ) , novartis ( inst ) , omniseq ( inst ) , personal genome diagnostics ( inst ) , regeneron ( inst ) , merck ( inst ) , mirati therapeutics ( inst ) , astellas pharma patents , royalties , other intellectual property : circulating tumor cell novel capture by c - met technology ( inst ) ; prochelators as targeted prodrugs for prostate cancer ( inst ) travel , accommodations , expenses : acerta pharma , genomic health , astrazeneca michael r . 
harrison consulting or advisory role : bayer , sano , exelixis , genentech , argos therapeutics , fujilm , janssen oncology , astrazeneca , pzer , bristol myers squibb speakers bureau : genentech , exelixis research funding : argos therapeutics ( inst ) , bristol myers squibb ( inst ) , genentech ( inst ) , pzer ( inst ) , medivation / astellas pharma ( inst ) , merck ( inst ) , clovis oncology ( inst ) , acerta pharma ( inst ) , astrazeneca ( inst ) changxue lu patents , royalties , other intellectual property : inventor of the patent that was licensed to qiagen and received royalty joseph d . 
scher leadership : asterias biotherapeutics stock and other ownership interests : asterias biotherapeutics honoraria : research to practice consulting or advisory role : janssen biotech , amgen , janssen research & development , menarini silicon biosystems , wirb - copernicus group , essa , sano , ambry genetics , konica minolta , pzer , bayer research funding : janssen ( inst ) , illumina ( inst ) , epic sciences ( inst ) , menarini silicon biosystems ( inst ) , thermosher scientic biomarkers ( inst ) travel , accommodations , expenses : asterias biotherapeutics , menarini silicon biosystems , amgen , wirb - copernicus group , konica minolta , essa , prostate cancer foundation , sano , bayer , phosplatin therapeutics richard wenstrup employment : epic sciences leadership : epic sciences stock and other ownership interests : epic sciences consulting or advisory role : blueprint genetics , resolys patents , royalties , other intellectual property : patent royalties from assurexhealth travel , accommodations , expenses : epic systems scott t . 
tagawa consulting or advisory role : medivation , astellas pharma , dendreon , janssen , bayer , genentech , endocyte , immunomedics , karyopharm therapeutics , abbvie , tolmar , qed , amgen , sano , pzer , clovis oncology , novartis , genomic health , point biopharma research funding : lilly ( inst ) , sano ( inst ) , janssen ( inst ) , astellas pharma ( inst ) , progenics ( inst ) , millennium pharmaceuticals ( inst ) , amgen ( inst ) , bristol myers squibb ( inst ) , dendreon ( inst ) , rexahn pharmaceuticals ( inst ) , bayer ( inst ) , genentech ( inst ) , newlink genetics ( inst ) , inovio pharmaceuticals ( inst ) , astrazeneca ( inst ) , immunomedics ( inst ) , novartis ( inst ) , aveo ( inst ) , boehringer ingelheim ( inst ) , merck ( inst ) , stem centrx ( inst ) , karyopharm therapeutics ( inst ) , abbvie ( inst ) , medivation ( inst ) , endocyte ( inst ) , exelixis ( inst ) , clovis oncology ( inst ) travel , accommodations , expenses : sano , immunomedics , amgen uncompensated relationships : telix pharmaceuticals , atlab pharma , phosplatin therapeutics emmanuel s . 
antonarakis honoraria : sano , dendreon , medivation , janssen biotech , essa , astellas pharma , merck , astrazeneca , clovis oncology consulting or advisory role : sano , dendreon , janssen biotech , essa , merck , astrazeneca , clovis oncology , lilly , bayer research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sano ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) , merck ( inst ) , astrazeneca ( inst ) , clovis oncology ( inst ) , constellation pharmaceuticals ( inst ) patents , royalties , other intellectual property : coinventor of a biomarker technology that has been licensed to qiagen travel , accommodations , expenses : sano , dendreon , medivation daniel j . 
george leadership : capio biosciences honoraria : sano , bayer , exelixis , emd serono , onclive , pzer , urotoday , acceleron pharma , american association for cancer research , axess oncology , janssen oncology , millennium medical publishing consulting or advisory role : bayer , exelixis , pzer , sano , astellas pharma , innocrin pharma , bristol myers squibb , genentech , janssen , merck sharp & dohme , myovant sciences , astrazeneca , michael j . 
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armstrong aj , szmulewitz rz , petrylak dp , et al : arches : a randomized , phase iii study of androgen deprivation therapy with enzalutamide or placebo in men with metastatic hormone - sensitive prostate cancer . 
aggarwal r , huang j , alumkal jj , et al : clinical and genomic characterization of treatment - emergent small - cell neuroendocrine prostate cancer : a multiinstitutional prospective study . 
de laere b , van dam pj , whitington t , et al : comprehensive proling of the androgen receptor in liquid biopsies from castration - resistant prostate cancer reveals novel intra - ar structural variation and splice variant expression patterns . 
kohli m , ho y , hillman dw , et al : androgen receptor variant ar - v9 is coexpressed with ar - v7 in prostate cancer metastases and predicts abiraterone commun 7 : 13668 , 2016 resistance . 
de laere b , oeyen s , mayrhofer m , et al : tp53 outperforms other androgen receptor biomarkers to predict abiraterone or enzalutamide outcome in metastatic castration - resistant prostate cancer . 
 armstrong et al appendix assessed for eligibility ( n = 131 ) did not meet inclusion criteria ( n = 13 ) received hormone therapy abiraterone enzalutamide both ( n = 118 ) ( n = 55 ) ( n = 58 ) ( n = 5 ) progression during treatment death during treatment ( n = 105 ) ( n = 4 ) received subsequent taxane therapy docetaxel cabazitaxel ( n = 51 ) ( n = 42 ) ( n = 9 ) progression during treatment death during treatment ( n = 46 ) ( n = 3 ) fig a1 . 
waterfall plots of best overall prostate - specic antigen ( psa ) decline from pretaxane baseline during therapy with docetaxel or cabazitaxel according to ( a ) epic sciences and ( b ) johns hopkins androgen receptor splice variant 7 ( ar - v7 ) status . 
baseline pretaxane characteristics of patients enrolled according to johns hopkins ar - v7 status johns hopkins ar - v7 status ( % ) positive ( n = 20 ) 48 - 82 negative ( n = 31 ) 45 - 87 elevated baseline serum ldh presence of liver metastasis presence of clinically signicant pain requiring opiates cellsearch ctcs , cells per 7.5 ml baseline pretaxane characteristic age , years median range race white black other gleason sum 8 - 10 poor - risk feature hemoglobin , 12 g / dl elevated alp range median , % ( n = 37 ) psadt , 3 months prior docetaxel for mhspc  . 
 successful targeting of an atg7 - raf1 gene fusion in anaplastic pleomorphic xanthoastrocytoma with leptomeningeal dissemination mehdi touat , md1 ; nadia younan , md1 ; philipp euskirchen , md1 , 2 , 3 , 4 , 5 ; maxime fontanilles , md1 ; karima mokhtari , md1 ; caroline dehais , md1 ; patrick tilleul , pharmd6 ; amithys rahimian - aghda , msc1 ; adam resnick , phd7 ; anne - paule gimenez - roqueplo , md , phd8 , 9 , 10 ; h el `ene blons , pharmd , phd8 , 9 , 11 ; kh e hoang - xuan , md , phd1 ; jean - yves delattre , md , phd1 ; ahmed idbaih , md , phd1 ; pierre laurent - puig , md , phd8 , 9 , 11 ; and marc sanson , md , phd1 introduction pleomorphic xanthoastrocytoma ( pxa ) is an uncommon primary brain tumor occurring primarily in children and young adults.1 although pxa is typically considered a relatively indolent entity , some tumors are accompanied by anaplastic features associated with high rates of recurrence after local treatment and unfavorable outcome.2 accordingly , anaplastic pxa ( who grade 3 ) has been added to the 2016 who classication of cns tumors as a distinct entity.1 there is no standard management for patients with anaplastic pxa that recurs after surgery ; neither chemotherapy nor radiotherapy have demonstrated clinical benet in this disease.2 , 3 the identication of activating in recent years , brafv600e mutations in 50% of patients with pxa has rened our understanding of these disorders as malignancies driven by aberrant activation of the mitogenactivated protein kinase ( mapk ) signaling pathway.1 , 3 - 5 this was further supported by the observation of both preclinical and clinical activity of vemurafenib , a selective brafv600e inhibitor , in brafv600e - mutant gliomas.6 , 7 however , patients with braf wild - type pxa are not candidates for treatment with selective brafv600e inhibitors , and little is known about the spectrum of molecular alterations occurring in this population . 
recent studies showed that a subset of braf wild - type pxa might harbor rare braf or raf1 fusions , 8 , 9 which have been associated with exquisite sensitivity to mapk signaling inhibition in preclinical models.10 it remains unknown whether patients who have glioma with braf or raf1 gene fusions might respond to therapies targeting mapk signaling . 
histopathologic analysis showed a tumor composed of pleomorphic glial cells with the presence of mitoses , necrosis , and microvascular proliferation , consistent with who grade 3 anaplastic pxa ( fig 2 )  . 
although rhabdoid morphology was observed in some sectors , both epithelial membrane antigen and p53 immunostainings were negative , and we did not observe loss of ini1 , features that were previously associated with rhabdoid glioblastomas and cns atypical teratoid / rhabdoid tumors , respectively . 
furthermore , targeted sequencing of the tumor did not nd mutations in braf ( exons 11 and 15 ) , idh1 , idh2 , h3f3a , hist1h3b , or smarcb1 . 
array comparative genomic hybridization revealed a 9p deletion involving cdkn2a and cdkn2b , which have been previously associated with poor outcome in brafv600e - mutant gliomas.3 , 11 , 12 given the unfavorable prognosis , she was rst treated with adjuvant chemoradiotherapy ( 60 gy in 30 fractions over 6 weeks along with once - per - day temozolomide 75 mg / m2 ) followed by temozolomide ( 200 mg / m2 ) for 6 cycles until november 2015 ( fig 1a )  . in february 2016 , routine surveillance mri scans showed increased contrast enhancement in the right occipital lobe . 
 touat et al context key objective to report the successful treatment of a patient with refractory braf - wild - type anaplastic pxas harboring an in - frame atg7raf1 fusion with the mek inhibitor cobimetinib . knowledge generated we report for the rst time , to our knowledge , that raf1 gene fusions are actionable molecular events in high - grade gliomas . this report highlights the oncogenic role of mapk - activating alterations including raf1 rearrangements and brafv600e mutations in a subset of pediatric and adult gliomas . relevance cobimetinib can achieve therapeutic exposure within the cns , including the cerebrospinal uid in patients with raf1translocated high - grade gliomas . showed leptomeningeal enhancement in the posterior cerebral fossa ( fig 1b )  . 
neoplastic meningitis was conrmed by lumbar puncture showing 42 white blood cells per l ( 84% lymphocytes ) , hyperproteinorachia ( 0.55 g / l ) , and the presence of tumor cells in the cerebrospinal uid ( csf ; fig 1b )  . 
intravenous thiotepa ( 45 mg / m2 ) was begun , the treatment was discontinued after one infusion because of grade 4 thrombopenia and febrile neutropenia with infectious pneumonia , which required intravenous antibiotics . the patient was enrolled in the precision medicine program exorare for tumor molecular characterization using rna sequencing and matched tumor or normal whole - exome sequencing . 
reverse transcriptase - polymerase chain reaction and sanger sequencing conrmed the expression of an in - frame atg7raf1 fusion transcript in the recurrent tumor ( second surgery , 2016 ; fig 3b )  . 
interestingly , no additional molecular alteration was found by whole - exome among 475 genes previously associated with cancer , which suggested that the atg7 - raf1 fusion was the main oncogenic driver . moreover , previous reports showed that fusions involving exon 8 of raf1 are recurrent events in cancer including pxa8 , 9 , 13 and can result in constitutive activation of the tyrosine kinase domain and downstream mapk signaling through the loss of the n - terminal autoinhibitory domain of raf1.14 treatment with sorafenib ( 200 mg twice per day ) was then started in october 2016 through off - label use after informed consent . 
unfortunately , her clinical condition rapidly deteriorated with partial seizures , confusion , cerebellar ataxia , diplopia , hypoacousia , headaches , and diffuse pain in the lower limbs , for which treatment with intravenous morphine , steroids , and midazolam was begun . on the basis of preclinical data suggesting that mek inhibition in astrocytomas harboring raf1 fusions has superior efcacy , 10 sorafenib was discontinued and treatment with off - label cobimetinib ( 60 mg per day , 3 weeks on and 1 week off ) was started in november 2016 , after family members provided informed consent ( fig 1a )  . 
the patient dramatically improved after a few days of treatment , with complete regression of the confusion and headaches and partial regression of the cerebellar ataxia and pain in the lower limbs . 
subsequent lumbar puncture showed complete cytologic response in the csf ( fig 1b ) with regression of both pleocytosis ( 1 white blood cell per l ) and hyperproteinorachia ( 0.15 g / l ; fig 1b )  . 
 ( b ) top : serial contrast - enhanced t1 - weighted images of brain magnetic resonance imaging ( mri ) and cerebrospinal uid ( csf ; may - gr unwald - giemsa stain ) cytology at ( left ) initial presentation , ( middle ) pretreatment , and ( right ) during treatment with cobimetinib showing the right occipital lesion , the leptomeningeal enhancement on the brain mri ( white arrows ) , and the presence of neoplastic cells in the csf ( black arrowheads ) before treatment with cobimetinib was started . 
the observation of clinical activity with both braf and mek inhibitors suggest that brafand raf1 - driven gliomas , even in patients who have been heavily pretreated , display a high level of mapk pathway dependency and possibly less molecular heterogeneity than the majority of gliomas driven by other alterations such as egfr variants.20 - 22 despite previous reports indicating activity of sorafenib in treating patients with cancer who harbor mutations of braf or araf ( both paralogs of raf1 ) , 23 , 24 our patient did not respond to treatment with sorafenib . 
 ( a ) hematoxylin - eosin and ( b ) reticulin colorations showing a pleomorphic tumor proliferation , with the presence of xanthomatous cells with nuclear atypia , reticulin bers , microvascular proliferation , and necrosis . 
 ( c - f ) immunohistochemical stains showing tumor cell immunoreactivity for ( c ) glial brillary acidic protein , ( d ) cd34 , and ( e ) oligodendrocyte transcription factor 2 . 
 ( f ) high mitotic activity was noted on mib - 1 staining . alterations is currently ongoing ( nct02639546 ; safety and pharmacokinetics of cobimetinib in pediatric and young adult participants with previously treated solid tumors [ imatrixcobi ] ) , although adult patients are not yet eligible for this study . 
furthermore , novel mek inhibitors optimized for achieving higher brain exposure might have a role in these diseases.28 in conclusion , our report provides evidence for the oncoincluding raf1 reargenic role of mapk alterations , in pediatric and adult brain tumors and rangements , suggests that raf1 fusions may represent potential therapeutic targets in a subset of patients with braf wild - type high - grade gliomas . 
a recent report of a patient with melanoma with an ano10raf1 fusion reported long - lasting clinical improvement after treatment with the mek inhibitor trametinib , 29 suggesting that patients with raf1 fusiondriven tumors might respond to mek inhibition regardless of histology . 
for more information about asco 's conict of interest policy , please refer to or ascopubs.org / po / authorcenter . mehdi touat consulting or advisory role : agios pharmaceutical , taiho oncology travel , accommodations , expenses : merck sharp & dohme maxime fontanilles travel , accommodations , expenses : roche patrick tilleul honoraria : takeda , astellas pharma , roche , biogen , evidera , baxter , gr unenthal group , chiesi , bristol - myers squibb , msd , sandoz - novartis , pzer , astrazeneca h el `ene blons honoraria : astrazeneca , bristol - myers squibb , msd oncology kh e hoang - xhuan travel , accommodations , expenses : abbvie ahmed idbaih travel , accommodations , expenses : carthera pierre laurent - puig honoraria : amgen , astrazeneca , boehringer ingelheim , merck serono , merck , roche , sano consulting or advisory role : merck , bristol - myers squibb , boehringer ingelheim patents , royalties , other intellectual property : inventor of mir31 - 3p ( license to integragen ) travel , accommodations , expenses : roche , merck marc sanson consulting or advisory role : abbvie , genenta travel , accommodations , expenses : abbvie no other potential conicts of interest were reported . acknowledgment the authors thank ines detrait and delphine le corre for tissue preparation and acid nucleic extractions , and dr yvan bieche and integragen for the genomic analyses performed in this patient . references louis dn , ohgaki h , wiestler od , et al : world health organization histological classication of tumours of the central nervous system , 4th edition revised . lyon , france , international agency for research on cancer , 2016 ida cm , rodriguez fj , burger pc , et al : pleomorphic xanthoastrocytoma : natural history and long - term follow - up . 
brain pathol 25 : 575 - 586 , 2015 lassaletta a , zapotocky m , mistry m , et al : therapeutic and prognostic implications of braf v600e in pediatric low - grade gliomas . 
j clin oncol 35 : 2934 - 2941 , 2017 dias - santagata d , lam q , vernovsky k , et al : braf v600e mutations are common in pleomorphic xanthoastrocytoma : diagnostic and therapeutic implications . plos one 6 : e17948 , 2011 schindler g , capper d , meyer j , et al : analysis of braf v600e mutation in 1 , 320 nervous system tumors reveals high mutation frequencies in pleomorphic xanthoastrocytoma , ganglioglioma and extra - cerebellar pilocytic astrocytoma . 
clin cancer res 17 : 7595 - 7604 , 2011 kaley t , touat m , subbiah v , et al : braf inhibition in brafv600 - mutant gliomas : results from the ve - basket study . 
brain pathol 29 : 85 - 96 , 2018 jain p , fierst tm , han hj , et al : craf gene fusions in pediatric low - grade gliomas dene a distinct drug response based on dimerization proles . 
huillard e , hashizume r , phillips jj , et al : cooperative interactions of brafv600e kinase and cdkn2a locus deciency in pediatric malignant astrocytoma as a basis for rational therapy . 
 cobimetinib in anaplastic pleomorphic xanthoastrocytoma with raf1 fusion jones dt , hutter b , j ager n , et al : recurrent somatic alterations of fgfr1 and ntrk2 in pilocytic astrocytoma . 
nat genet 45 : 927 - 932 , 2013 johnson a , severson e , gay l , et al : comprehensive genomic proling of 282 pediatric lowand high - grade gliomas reveals genomic drivers , tumor mutational burden , and hypermutation signatures . 
reinhardt a , stichel d , schrimpf d , et al : anaplastic astrocytoma with piloid features , a novel molecular class of idh wildtype glioma with recurrent mapk pathway , cdkn2a / b and atrx alterations . 
szerlip nj , pedraza a , chakravarty d , et al : intratumoral heterogeneity of receptor tyrosine kinases egfr and pdgfra amplication in glioblastoma denes subpopulations with distinct growth factor response . 
cancer discov 4 : 956 - 971 , 2014 imielinski m , greulich h , kaplan b , et al : oncogenic and sorafenib - sensitive araf mutations in lung adenocarcinoma . 
casadei gardini a , chiadini e , faloppi l , et al : efcacy of sorafenib in braf - mutated non - small - cell lung cancer ( nsclc ) and no response in synchronous braf wild type - hepatocellular carcinoma : a case report . 
choo ef , ly j , chan j , et al : role of p - glycoprotein on the brain penetration and brain pharmacodynamic activity of the mek inhibitor cobimetinib . 
gampa g , kim m , cook - rostie n , et al : brain distribution of a novel mek inhibitor e6201 : implications in the treatment of melanoma brain metastases . 
blumenthal , md1 ; and reena philip , phd1 purpose next - generation sequencing ( ngs ) oncology panels are becoming integral in hospital and academic settings to guide patient treatment and enrollment in clinical trials . 
although ngs technologies have revolutionized decision - making for cancer therapeutics , physicians may face many challenges in parsing and prioritizing ngs - based test results to determine the best course of treatment for individual patients . 
here , we discuss the presentations and discussion highlights across the four sessions of the workshop . methods the goal of the public workshop was to engage stakeholders and solicit input from experts in precision oncology to discuss the integration of complex ngs data into patient management and regulatory innovation within the precision oncology community . 
the us food and drug administration gathered representatives from academia , industry , patient advocacy , government , and professional organizations for a series of presentations followed by panel discussions . 
after the workshop , the transcript and speaker presentation slides were reviewed and summarized for manuscript preparation . results speakers and panelists provided diverse perspectives on the integration of ngs technology into patient care for oncology and on the complexities that surround data interpretation and sharing . 
2019 by american society of clinical oncology introduction the goal of precision oncology is to use the genetic informationgermline or somaticfrom a patient with cancer to help determine which drug ( s ) might be most effective in treating his or her disease . 
next - generation sequencing ( ngs ) is increasingly used in precision oncology because of its ability to identify many mutations simultaneously , thereby maximizing the amount of information obtained from a single test.1 the global endeavor to identify somatic mutations within a patients tumor genome has led to an unprecedented amount of genomic information , with varying degrees of associated clinical evidence . 
ngs can report a vast number of mutations which may lead to clinician uncertainty in the interpretation and prioritization of mutations with respect to the clinical signicance and optimal course of treatment.2 in january 2017 , the association for molecular pathology ( amp ) , asco , and the college of american pathologists ( cap ) published a joint consensus recommendation for standards and guidelines for the interpretation and reporting of sequence variants in cancer3 ; however , stakeholders have not consistently implemented these recommendations . 
 horne et al context key objective to provide an overview of a public workshop hosted by the us food and drug administration that discussed key concepts and considerations for the classication and interpretation of genetic variants in precision oncology . knowledge generated key highlights and ndings from the discussion include the conclusion that as the use of next - generation sequencing oncopanels in the clinical setting increases , it is critical to develop a framework that ensures accurate and consistent interpretation of genetic variants . 
in addition , transparency in data sourcing and reporting methodologies , as well as frequent updating of variant interpretations , are necessary to advance science and appropriately care for patients . relevance as precision medicine advances , clear communication among stakeholders in oncology will be key to creating an environment that facilitates generating and sharing data that have value to patients . treatement options , in addition to providing tumor proling data.6 , 7 with fda approval and authorization of these two ngs - based pan - tumor oncology panels ( oncopanels ) , the agency was in a unique position to foster a dialogue among key stakeholders about this innovative technology . input on january 29 , 2018 , the fda held a public workshop to engage stakeholders and solicit from experts in precision oncology and patient representatives to discuss how genetic sequencing data could be best implemented in patient management . 
to set the stage for the workshop discussion , dr philip outlined the fdas new regulatory pathway for ngs tumor - proling tests , as summarized in the fdas center for devices and radiologic health fact sheet published online on november 15 , 2017.8 as described by dr philip , the agencys three - tiered approach for reporting biomarkers in tumor - proling ngs tests includes the following : level 1 , companion diagnostic claims ; level 2 , cancer mutations with evidence of clinical signicance ; and level 3 , cancer mutations with potential clinical signicance . 
tumor - proling ngs tests may include companion diagnostic claims ( level 1 ) that are prescriptive for a specic therapy and are supported by the clinical validity of the test for each biomarker reported . 
bowles , phd , myriad genetic laboratories best practices for the use of clinical databases for variant classication and facmg interpretation in clinical oncology session 4 : future directions for data sharing , standardization , and establishing consistency in precision oncology dane dickson , md cureone us food and drug administration public workshop : variant classication dennis dean , phd seven bridges genomics creating a community view : standards , analyses , and data to advance robert grossman , phd university of chicago the important role of data commons for sharing variant classication and consistency in precision oncology interpretation data in precision oncology len lichtenfeld , md american cancer society cancer action panelist network * afliations noted in the table are based on speaker afliations at the time of the public workshop and may not reect the current afliation . validity has not been demonstrated either in professional guidelines or with the test , but is suggestive on the basis of clinical / biologic evidence . session 1 : overview of the state of science for sequence variant classication in oncology and its practical use in treating patients use of an individuals mutation prole for clinical decision making is driving the ever - expanding number of biomarkerbased clinical trials and clinical regimens in precision oncology . 
 horne et al vincent miller , md , indicated that fmi lters out germline mutations but further noted that when reporting germline mutations , laboratories need to have an operation in place , or at least have an understanding with the clinicians , so that the information can be followed up with genetic counseling . comprehensive variant annotation is necessary to inform treatment selection and match patients to clinical trials . 
the number of patients who are matched to either clinical trials or personalized treatments on the basis of their genomic data were reported by panelists to be between 10% and 37% . 
to compile and interpret the evidence , scientists and pathologists continually gather new information from guidelines , published literature , public databases , clinical trials , fdaapproved therapeutic labeling , and other sources . 
this comprehensive information is then used to sort biomarkers , either manually or in combination with bioinformatics software algorithms , on the basis of levels of evidence . panelists concluded that a key to the success of somatic genotyping will be developing statistical tools and bioinformatics infrastructure to identify clinically meaningful mutations . 
dr berger noted that as more sequencing data accumulates , integrated analyses of big data will allow for the identication of novel hotspot mutations occurring at frequencies greater than would be expected by chance . this approach would allow for these novel mutations to be directly tested in targeted clinical trials to assess drug sensitivity . 
panelists noted that the eld will continue to evolve and become more challenging with the increase in tissue - agnostic trials in which patients are enrolled on the basis of biomarker status , irrespective of the tumor type , which could , in turn , lead to an increase in tissue - agnostic drug indications . 
john deeken , md , also highlighted some of the unique challenges faced when running an in - house 50 - gene oncopanel at a community - based hospital system . these challenges included the cost of developing and supporting an oncopanel test and the lack of reimbursement for the majority of ngs testing performed . 
donna roscoe , phd , noted that the fda is striving to ensure that there are validated tests on the market that will allow for dynamic use within clinical settings to enable clinicians to optimize patient decisions in oncology and other therapeutic areas . session 2 : levels of evidence required for reporting variants and guiding patient treatment widespread implementation of ngs data in clinical settings has been accompanied by challenges in standardization , interpretation , and reporting of genetic tests . 
shashikant kulkarni , phd , provided an overview of the proposed guidelines published by a multidisciplinary working group convened by amp , asco , and cap for variant interpretation and reporting.3 the four - tiered system to categorize somatic sequence variations on the basis of their levels of evidence are as follows : tier i , variants with strong clinical signicance ; tier ii , variants with potential clinical signicance ; tier iii , variants of unknown clinical signicance ; and tier iv , variants deemed benign or likely benign.3 guidelines were developed to provide a general framework , on the basis of an evidence - based variant classication approach , for the standardized interpretation and reporting of somatic variants in cancer . 
for example , variants with strong clinical evidence include those with level a evidence ( fda - approved therapies or included in professional guidelines ) or level b evidence ( well - powered studies with consensus from experts in the eld )  . 
variants with potential clinical evidence are those with level c evidence ( fda - approved therapies for different tumor types or investigational therapies of multiple small published studies with some consensus ) or level d evidence ( preclinical trials or found in a few case reports without consensus )  . in general , it is widely accepted that tests should be optimized to ensure coverage across targets and high sensitivity for detecting low - frequency mutations ; however , as noted in the consensus manuscript , 3 the eld is split on the use of variant allele frequency ( vaf ) in reporting and clinical practice . 
one perspective , provided from a workshop attendee , was that if frequencies are too low , the detected mutations could represent subclonal events and may not necessarily be appropriate therapeutic targets . 
on the contrary , apostolia - maria tsimberidou , md , phd , noted that , as a clinical investigator , there is utility in having allele fraction present in the patient report as the data could be used to interpret clinical outcomes , particularly because patients have multiple molecular alterations . 
a consensus was not reached by workshop panelists or attendees regarding the clinical use or validity of reporting vaf in precision oncology . standardizing the annotation and reporting of somatic mutations from ngs data remains a challenge . 
john pfeifer , md , phd , pointed out that there is a gray zone between where the technical portion of the ngs test ends and the practice of medicine begins . 
although many of the speakers and panelists used the amp / asco / cap guidelines , several groups used a slightly modied tiering system . panelists generally agreed that treatment options for tier ii and below , as noted in the amp / asco / cap guidelines , should be considered only once tier i treatment options have been exhausted . 
moreover , panelists expressed the need to create a databasethat is , a knowledge basethat can assist in resolving discordances in variant interpretation and allow for the generation of community standards . session 3 : best practices for use of public / private databases for variant classication and interpretation in oncology to positively affect patient care , mutations detected using ngs technology must be appropriately interpreted and classied . 
the panel unanimously agreed that a known drawback to using publicly available databases for variant classication is that interpretation is not always consistent . heidi rehm , phd , noted that the quality of the data rests in the hands of those who deposit the information into the database and that amassing sufcient information to provide high - quality classication data requires global sharing . kenna shaw , phd , afrmed that standards and rules are needed to not only interpret but reinterpret variant classication , and she summarized the efforts being conducted at her institution to amass a personalized cancer therapy knowledge base . 
dr shaw provided an overview of aacr project genie ( genomics evidence neoplasia information exchange ) , which presently includes 17 institutions across the world that are working together to develop a regulatorygrade registry that aggregates and links cancer genomic data with clinical outcomes from tens of thousands of cancer patients . 
project genie will allow for sharing of the accumulated data with the global research community through cbioportal and the synapse platform with the noted caveat that the underlying functional evidence int the knowledge base will continue to change over time . panelists agreed that databases should be transparent about data sources , methods , and rules used for reporting mutation - associated clinical claims . 
karla bowles , phd , noted that subjective tools , such as literature reviews , population data , and structural analysis , should be used with caution , as interpretations from these data are often sources of discrepancies . 
the number of session 4 : future directions for data sharing , standardization , and establishing consistency in precision oncology many mutations identied by genomic tests for oncology are novel , rare , or otherwise lack conclusive evidence to support a clinical these mutations will only increase as additional genes are added to oncopanels and the costs of sequencing decrease . understanding the clinical utility of these mutations requires addressing barriers that prevent accurate classication . 
dane dickson , md , cited improved data sharing as a critical need and described the utility of high - quality databases that include both diagnostic results and clinical outcomes . dennis dean , phd , described the need for interoperability of complex systems and tools to enable analysis of large data sets . interoperability requires standards and languages to support reproducibility . 
dean discussed rabix , a suite of open - source development tools for creating and running computation workows , as a development environment that uses common workow language to promote the analysis of combined large data sets . 
robert grossman , phd , emphasized the need for data commonsthat is , a unied data system that promotes sharingsuch as the national cancer institute that use data models and genomic data commons , metadata services to harmonize and share cancer genomic datasets . 
grossman discussed the concept of leveraging funders , journal editors , and payers to incentivize the data sharing required to build a data commons . as a patient advocate , len lichtenfeld , md , discussed the challenges of translating the information generated by large - scale projects to communities that lack the resources and infrastructure to access the latest information necessary to improve care . 
 horne et al in conclusion , precision oncology is a rapidly evolving eld . with more oncopanels being developed , and as more genomic and patient outcome data accumulate , physicians are faced with new challenges in interpreting ngs - based test results to determine the best treatment course for each patient . 
in addition , there are multiple public and private databases available that aid in variant classication and interpretation ; however , methods used to classify variants and how these databases align remain unclear . 
to that end , the fda recently nalized a guidance document entitled , use of public human genetic variant databases to support clinical validity for genetic and genomic - based in vitro diagnostics . 
david litwack employment : prevail therapeutics travel , accommodations , expenses : prevail therapeutics no other potential conicts of interest were reported . acknowledgment the authors thank all event staff at the us food and drug administration for helping to execute a seamless public workshop that was benecial to both in - person and online attendees . 
the authors thank the workshop presenters who graciously provided their permission to publish details about their titles and summaries in the manuscript table and text . references strom sp : current practices and guidelines for clinical next - generation sequencing oncology testing . 
n engl j med 375 : 711 - 713 , 2016 li mm , datto m , duncavage ej , et al : standards and guidelines for the interpretation and reporting of sequence variants in cancer : a joint consensus recommendation of the association for molecular pathology , american society of clinical oncology , and college of american pathologists . 
us food and drug administration : use of public human genetic variant databases to support clinical validity for genetic and genomic - based in vitro diagnostics : guidance for stakholders and food and drug administration staff . 
us food and drug administration : public workshop - - weighing the evidence : variant classication and interpretation in precision oncology , january 29 , 2018 , workshops and conferences ( medical devices )  . 
 c long - term complete response of an androgen receptorpositive triple - negative metastatic breast cancer to abiraterone acetate introduction several gene expression array studies have identified a new breast cancer subtype characterized by the expression of the androgen receptor ( ar ) , absence of the estrogen receptor ( er ) , and paradoxical expression of many genes that are typically expressed in er - positive luminal tumors.1 - 3 two thirds of this tumor subtype are human epidermal growth factor receptor 2 ( her2 ) positive . 
these ar - positive and triple - negative tumors have been identified as a stable subtype in two series of tnbcs.4 , 5 of note , ar is also expressed in approximately 75% of er - positive / her2 - negative breast cancers.6 however , clinical and preclinical data suggest that ars act as a tumor suppressor gene in er - positive tumors and as an oncogene in er - negative tumors.7 in both retrospective series8 and prospective clinical trials , 9 - 11 the following immunohistochemistry ( ihc ) definition is classically used to identify this breast cancer subtype : ar positive and er , progesterone receptor ( pr ) negative , and her2 negative . 
there is no universal consensus on defining ar positivity to date , although the accepted definition of ar positivity is 10% . preclinical in vitro2 , 12 - 14 and in vivo14 , 15 data suggest that androgens are involved in the development and growth of the mda - mb - 453 cell line , which is used as an in vitro model for the ar - positive tnbc subtype.2 consequently , in three prospective clinical trials , either competitive antagonists of the ar ( bicalutamide or enzalutamide ) or androgen synthesis suppressor , cyp17 inhibitor ( abiraterone acetate , aa ) , were evaluated in ar - positive tnbcs . 
 she received neoadjuvant chemotherapy ( three cycles of fluorouracil , epirubicin , and cyclophosphamide followed by three cycles of docetaxel ) followed by mastectomy and axillary lymph node dissection ( level 1 and 2 )  . 
 the arrows show the index masses with changes with therapies . multiple sclerosis and administered interferon at a dose of 30 g per week . in november 2007 , the patient was diagnosed with an ipsilateral axillary lymph node relapse without distant metastasis . 
no further treatment was proposed . in july 2013 , she presented with a 4 - cm left axillary mass with skin involvement ( fig 1a ) and two supraclavicular 1 - cm lymph nodes ; a core biopsy of the axillary mass confirmed tnbc , with a proliferation index ( ki - 67 ) of 15% . 
on the computed tomography scan ( figs 1b and 1c ) , in addition to the axillary mass , several chest soft tissue masses were observed ; no visceral or bone metastasis was observed . 
the patient was included in the ucbg 2012 - 1 trial and received experimental treatment with 1 , 000 mg of aa and 10 mg of prednisone administered orally , daily . 
ten months after the treatment initiation , clinical and computed tomography scan evaluations showed that the patient achieved a cr ( on the basis of the response evaluation criteria in solid tumors criteria )  . 
after 4 years , the patient is still receiving the treatment with aa and low - dose prednisone , with a prolonged cr ( figs 1d - 1f )  . 
concomitantly , she has been receiving interferon treatment for multiple sclerosis . further ihc analyses later performed on the 2006 mastectomy and the 2007 axillary relapse showed that 100% of cells were ar positive . 
 furthermore , ihc analyses on additional markers in the 2013 axillary relapse confirmed a pronounced apocrine feature with marked forkhead box a1 and gross cystic disease fluid protein 15 expression . 
ongoing clinical trials on ar - positive triple negative breast cancer in metastatic setting single agent combination antiandrogen ar antagonist enzalutamide ( phase iii , clinicaltrials.gov identifier : nct02929576 , withdrawn ) bicalutamide v chemotherapy ( phase iii / first line , clinicaltrials . gov identifier : nct03055312 , recruiting ) darolutamide v chemotherapy ( randomized phase ii , first and second line , clinicaltrials.gov identifier : nct03383679 , recruiting ) bicalutamide plus cdk4 / 6 inhibitor ribociclib ( phase i / ii , clinicaltrials.gov identifier : nct03090165 , recruiting ) bicalutamide plus cdk4 / 6 inhibitor palbociclib ( phase i / ii , clinicaltrials.gov identifier : nct02605486 , recruiting ) enzalutamide plus pi3k inhibitor alpelisib ( phase i , clinicaltrials.gov identifier : nct03207529 , not yet recruiting ) or plus pi3k inhibitor taselisib ( phase i / ii , clinicaltrials.gov identifier : nct02457910 , recruiting ) cyp17a1 inhibitors orteronel ( tak - 700 ; phase ii , clinicaltrials.gov identifier : nct01990209 , recruiting ) seviteronel ( phase i / ii , clinicaltrials.gov identifier : nct02580448 , recruiting ) selective ar modulator cr1447 ( phase ii , clinicaltrials.gov identifier : nct02067741 , recruiting ) enobosarm plus pembrolizumab ( phase ii , clinicaltrials.gov identifier : nct02971761 , recruiting ) enobosarm ( phase ii , clinicaltrials.gov identifier : nct02368691 , terminated ) abbreviations : ar , androgen receptor ; cdk , cyclin - dependent kinase ; her2 , human epidermal growth factor receptor 2 ; pi3k , phosphatidylinositol 3 - kinase . from a clinicians perspective , the cbrs at 6 months ( 19% to 29% ) observed in this breast cancer subtype in the three prospective trials testing ar antagonist or androgen synthesis inhibitor are modest but clinically relevant . 
patients with ar - positive tnbcs seem to be older compared with the whole tnbc population.9 - 11 , 17 they also tend to relapse after a long interval after the primary tumor treatment . 
in our opinion , in ar - positive tnbcs , treatment choice between antiandrogens and chemotherapy could take into account different factors , including disease - free interval , tumor burden , and the need for rapid disease / symptom control , similar to luminal erand / or pr - positive tumors . 
of note , it is important to remember that progression - free survival for first - line chemotherapy is merely 4 to 6 months.18 , 19 from a researchers perspective , cbrs at 6 months with antiandrogens in this tumor subtype are much lower than those observed with anti - aromatase inhibitors used as single agents in luminal erand / or pr - positive cancers . 
in the latter group , the historical cbrs range from 49% to 59% for first - line and from 24% to 37% for second - line treatments , respectively.20 hence , there is a need to improve these results in ar - positive tnbcs , and we briefly outline four key areas that could be improved . first , ihc is probably not ideal to identify this breast cancer subtype . 
of note , in the enzalutamide trial , 10 patients with low ar ( 1% to 9% ) were included in an exploratory cohort , and some of these patients responded . 
in two large series of tnbcs analyzed by gene expression array , 11% and 17% of tumors were ar positive.4 , 5 in a tnbc series analyzed by ihc , 22% to 35% of patients were ar positive.8 it is difficult to explain this difference . 
hence , there is a need to better identify this subtype in clinical practice , for example , by using rna signatures with a selected number of transcripts.5 second , predictors of antiandrogen treatment sensitivity in this breast cancer subtype should be developed . 
new preclinical models are needed ; the reliability of the mda - mb - 453 cell line has been in question because of genomic alterations , such as ar mutation.22 , 23 this ar q865h mutation in its ligand - binding domain is reported to decrease sensitivity to dihydrotestosterone , limiting its use to test antiandrogen therapy.22 a new patient - derived xenograft model of molecular apocrine tumors , directly derived from patients , could be a solution.24 finally , we need better drugs and combinations . 
 however , both enzalutamide and abiraterone have shown to improve the sensitivity of tnbc cell lines toward immune - mediated lysis , providing potential rationale for combination of immunotherapy with antiandrogen therapy.25 in conclusion , we believe that this patients case is important for clinicians . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center  . thomas grellety consulting or advisory role : novartis herv bonnefoi consulting or advisory role : abbvie , astellas pharma , bayer healthcare pharmaceuticals , innocrin pharmaceuticals , puma biotechnology research funding : bayer ( inst ) travel , accommodations , expenses : roche , pfizer acknowledgment we thank ravi nookala , phd , of institut bergoni for the medical writing service . affiliations thomas grellety and herv bonnefoi , institut bergoni unicancer , universit bordeaux , institut national de la sant et de la recherche mdicale u1218 , institut national de la sant et de la recherche mdicale cic1401 ; and thomas grellety , gaetan macgrogan , camille chakiba , michele kind , and herv bonnefoi , institut bergoni , bordeaux , france . support supported by the fondation pour la lutte contre le cancer pour les recherches medico - biologiques , site de recherche intgre sur le cancer - bordeaux recherche intgre oncologie , and groupement interrgional de recherche clinique et dinnovation sud - ouest outre - mer grant no . 
vera - badillo fe , templeton aj , de gouveia p , et al : androgen receptor expression and outcomes in early breast cancer : a systematic review and meta - analysis . 
hickey te , robinson jl , carroll js , et al : minireview : the androgen receptor in breast tissues : growth inhibitor , tumor suppressor , oncogene ? mol endocrinol 26 : 1252 - 1267 , 2012 8 . 
gucalp a , tolaney s , isakoff sj , et al : phase ii trial of bicalutamide in patients with androgen receptor - positive , estrogen receptor - negative metastatic breast cancer . 
traina ta , miller k , yardley da , et al : results from a phase 2 study of enzalutamide ( enza ) , an androgen receptor ( ar ) inhibitor , in advanced ar + triple - negative breast cancer . 
bonnefoi h , grellety t , tredan o , et al : a phase ii trial of abiraterone acetate plus prednisone in patients with triple - negative androgen receptor positive locally advanced or metastatic breast cancer ( ucbg 12 - 1 )  . 
lehmann bd , bauer ja , schafer jm , et al : pik3ca mutations in androgen receptor - positive triple negative breast cancer confer sensitivity to the combination of pi3k and androgen receptor inhibitors . 
arce - salinas c , riesco - martinez mc , hanna w , et al : complete response of metastatic androgen receptor - positive breast cancer to bicalutamide : case report and review of the literature . 
oshaughnessy j , schwartzberg l , danso ma , et al : phase iii study of iniparib plus gemcitabine and carboplatin versus gemcitabine and carboplatin in patients with metastatic triple - negative breast cancer . 
miles dw , diras v , corts j , et al : first - line bevacizumab in combination with chemotherapy for her2 - negative metastatic breast cancer : pooled and subgroup analyses of data from 2447 patients . 
moore nl , buchanan g , harris jm , et al : an androgen receptor mutation in the mda - mb - 453 cell line model of molecular apocrine breast cancer compromises receptor activity . 
vranic s , gatalica z , wang zy : update on the molecular profile of the mda - mb - 453 cell line as a model for apocrine breast carcinoma studies . 
 response of nf1 - mutated melanoma to an mek inhibitor introduction molecular classification of melanoma has established three subtypes of braf wild - type tumors , 1 nf1 mutant ( 10% to 15% ) , ras mutant ( 28% ) , and triple - negative ( 10% ) , for which treatment options are limited . 
his sister had been diagnosed with acute leukemia but family history was otherwise noncontributory . after wide local excision , histopathologic examination revealed an ulcerated nodular melanoma , breslow 4.8 mm , clark v , and 2 mitoses / mm2 ( stage pt4b , american joint committee on cancer , 7th edition )  . 
the sentinel lymph node biopsy was positive , motivating a parotidectomy and left cervical lymphadenectomy , which removed 33 lymph nodes ( seven positive , one with extracapsular extension )  . 
sequencing of the sentinel biopsy with 52 - gene hotspot panel ( appendix ) revealed no mutations in braf , nras , or kit . in accordance with recommendations , 2 adjuvant radiotherapy ( 48 gy ) was administered . 
the patient participated in a clinical trial of adjuvant pembrolizumab versus placebo ( nct02362594 ) and was randomly assigned to the pembrolizumab ar treatment was interrupted after four doses because of the appearance of liver , bone , cutaneous , and subcutaneous metastases . excision of a subcutaneous lesion confirmed metastatic relapse with no programmed death ligand 1 ( pd - l1 ) expression , and the patient received ipilimumab plus nivolumab for 2 months , followed by nivolumab for 3 months.3 the disease progressed with new metastases in the skin , liver , pancreas , spleen , lungs , adrenal glands , and lymph nodes . 
chemotherapy with cisplatin , vinblastine , dacarbazine , and interferon alpha was administered for two cycles , until additional disease progression.4 additional sequencing was performed using a panel covering 409 cancer - related genes ( appendix ) , and 43 somatic mutations ( appendix table a1 ) , corresponding to 29.5 nonsynonymous mutations / mb , were identified . 
the mutational profile ( fig 1a ) was typical of cutaneous melanoma , 5 with the wide spectrum of allelic frequencies ( af ) being consistent with the progressive accumulation of mutations over time ( fig 1b )  . 
ptpn11 contained two mutations ( fig 1d ) : one resulting in an early stop codon ( trp423 * , af = 26% ) and another , a single amino acid change ( thr468pro , af = 31% ) , both in the protein - phosphatase domain , which autoinhibit ras activation of shp26 and are likely to induce gain - of - function . on the basis of these findings , from july 2017 , we administered trametinib , a mek inhibitor , and , 6 weeks later , clinically evaluable cutaneous and subcutaneous lesions had visibly regressed . 
this was confirmed by positron emission tomography / computed tomography ( fig 2 ) , in which no new metastases were observed , no measurable lesions had increased , and most lesions had cline py yann christinat mario kreutzfeldt thomas a . 
whole - brain radiotherapy was initiated , followed by pembrolizumab , but the patient died 11 weeks after the end of trametinib therapy . two biopsy specimens were obtained during and after trametinib treatment and were analyzed with the 409 - gene panel . 
the three samples sequenced shared 39 mutations ( appendix table a1 ) , and the pretrametinib and post - trametinib samples had four additional nonshared mutations each ( table 1 )  . the pretrametinib sample showed diffuse nuclear expression of phosphorylated extracellular regulated kinase ( erk ) , consistent with mitogen - activated protein kinase ( mapk ) activation , in contrast to the other samples ( fig 3a )  . 
samples obtained before and after trametinib did not express pd - l1 and had negligible infiltration by cd8 lymphocytes , but during treatment , both pd - l1 expression and cd8 + density increased significantly ( fig 3b )  . discussion herein , we document , to our knowledge , the first response to trametinib in nf1 - mutated melanoma . 
radiologic evaluation with [ 18f ] fluorodeoxyglucose ( [ 18f ] fdg ) positron emission tomography ( pet ) / computed tomography ( ct ) before and during treatment with trametinib . 
 ( a ) baseline image showed multiple supra and infra - diaphragmatic lesions in the skin , liver , pancreas , spleen , lungs , bone , adrenal glands , and lymph nodes . 
 ( c ) ct scan and fdgpet / ct showed a morpho - metabolic decrease of the cervical lesion . in a phase i trial of trametinib , four of 39 patients with braf wild - type tumor had a partial response , 22 but none carried an nf1 mutation . 
with the exception of the nf1 splice mutation in the initial sample , none of the remaining unique mutations is predicted to be pathogenic or known to be a cancer hotspot mutation . 
a patient with nf1 - associated optic glioma treated with trametinib had rapid improvement that persisted for 4 months , 24 and trametinib treatment of one patient with a refractory ependymoma harboring mutations in both nf1 and ptpn11 resulted in disease stabilization for 10 weeks.25 nf1 - mutated tumors , as in this case , have a higher mutation burden than do other melanoma subtypes10 , and the accumulation of protein - coding mutations favors response to immune checkpoint inhibitors by generating mutated peptides that are recognized as neoantigens.30 nevertheless , this tumor did not have significant cd8 + infiltration , did not express pd - l1 before treatment with trametinib , and did not respond to pembrolizumab or the association of ipilimumab and nivolumab . in our patient , disease progression occurred after 5 months of trametinib , and none of the mutations found exclusively in the midor post - treatment biopsy specimens are known to induce resistance to mek inhibitors . 
although crebbp loss may activate the ras pathway , it does not modify sensitivity to mek inhibition in vitro26 and would not be expected to induce resistance to trametinib in our patient . 
genomic screens suggest that resistance to trametinib may be acquired through changes in the atxn1lcic - ets transcription factor axis , downstream of mek.29 our analyses would not capture atxn1l or etv upregulation , but would detect cic mutations , which were not present . 
 these events could recapitulate the effects of erk activation without nuclear phosphorylated erk localization , which we saw before , but not during and after trametinib . the increase in cd8 + infiltration and pd - l1 expression during trametinib treatment ( fig 3 ) is in accordance with the findings of previous studies . 
a mouse model treated with an raf inhibitor resulted in a notable increase in cd8 + infiltration that might have contributed to response , 31 and the same pattern has been observed in melanomas treated with braf or braf plus mek inhibitrs.32 the increase in cd8 + infiltrate may be explained by the effect of mek inhibition , which can protect t cells from t - cell receptordriven apoptosis.33 alternatively , major histocompatibility complex class i internalization driven by mapk activation34 could also be reversed by mek inhibition ( not observed in this case )  . 
 ( b ) cd8 t - cell infiltrate , programmed deathligand 1 ( pd - l1 ) , and hla class i expression before , during , and after treatment with trametinib . 
pd - l1 expression in the treatment sample is estimated at approximately 2% . might be required to achieve a robust immune response.35 - 37 changes that occurred under treatment might be enhanced by combined immunotherapy . this report supports the exploration of mek inhibitors for nf1 - mutated melanoma in clinical trials , with attention to the presence of concomitant ptpn11 mutations . 
mckee speakers ' bureau : novartis travel , accommodations , expenses : roche pierre - yves dietrich research funding : novartis ( inst ) petros tsantoulis honoraria : roche , pfizer travel , accommodations , expenses : amgen financial support : thomas a . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . affiliations all authors : university hospital of geneva , geneva , switzerland . references 161 : 1681 - 1696 , 2015 1 . 
atkins mb , hsu j , lee s , et al : phase iii trial comparing concurrent biochemotherapy with cisplatin , vinblastine , dacarbazine , interleukin - 2 , and interferon alfa - 2b with cisplatin , vinblastine , and dacarbazine alone in patients with metastatic malignant melanoma ( e3695 ) : a trial coordinated by the eastern cooperative oncology group . 
martinelli s , torreri p , tinti m , et al : diverse driving forces underlie the invariant occurrence of the t42a , e139d , i282v and t468m shp2 amino acid substitutions causing noonan and leopard syndromes . 
falchook gs , lewis kd , infante jr , et al : activity of the oral mek inhibitor trametinib in patients with advanced melanoma : a phase 1 dose - escalation trial . 
tafe lj , gorlov ip , de abreu fb , et al : implementation of a molecular tumor board : the impact on treatment decisions for 35 patients evaluated at dartmouth - hitchcock medical center . 
dixon za , nicholson l , zeppetzauer m , et al : crebbp knockdown enhances ras / raf / mek / erk signaling in ras pathway mutated acute lymphoblastic leukemia but does not modulate chemotherapeutic response . 
frederick dt , piris a , cogdill ap , et al : braf inhibition is associated with enhanced melanoma antigen expression and a more favorable tumor microenvironment in patients with metastatic melanoma . 
ebert pjr , cheung j , yang y , et al : map kinase inhibition promotes t cell and anti - tumor activity in combination with pd - l1 checkpoint blockade . 
bradley sd , chen z , melendez b , et al : brafv600e co - opts a conserved mhc class i internalization pathway to diminish antigen presentation and cd8 + t - cell recognition of melanoma . 
bendell jc , kim tw , boon cg , et al : clinical activity and safety of cobimetinib ( cobi ) and atezolizumab in colorectal cancer ( crc )  . 
desai j , hong ys , kim je , et al : efficacy and safety of cobimetinib ( cobi ) and atezolizumab ( atezo ) in an expanded phase 1b study of microsatellite - stable ( mss ) metastatic colorectal cancer ( mcrc )  . 
sullivan r , gonzalez r , lewis kd , et al : atezolizumab ( a ) + cobimetinib ( c ) + vemurafenib ( v ) in brafv600 - mutant metastatic melanoma ( mel ) : updated safety and clinical activity . 
 clinical utility of clia - grade ar - v7 testing in patients with metastatic castration - resistant prostate cancer purpose a splice variant of the androgen receptor , ar - v7 , confers resistance to ar - targeted therapies ( atts ) but not taxane chemotherapies in patients with metastatic castrationresistant prostate cancer . 
since august 2015 , a clinical - grade assay to detect ar - v7 messenger rna expression in circulating tumors cells ( ctcs ) has been available to providers through a clinical laboratory improvement amendmentscertified laboratory at johns hopkins university . methods we contacted ordering providers of the first 150 consecutive tests by using a questionnaire - based survey to determine how the results of ar - v7 testing were used to influence clinical practice . results in all , 142 ( 95% ) of 150 questionnaires were completed by 38 providers from 29 sites across the united states and canada . 
prevalence of ar - v7 detection increased with prior exposure to atts ( abiraterone and enzalutamide nave , 22% ; after abiraterone or enzalutamide , 35% ; after abiraterone and enzalutamide , 43% )  . 
2017 by american society of clinical oncology introduction metastatic castration - resistant prostate cancer ( mcrpc ) remains dependent on androgen receptor ( ar ) signaling for survival in the presence low testosterone levels.1 two novel artargeted therapies ( atts ) , abiraterone and enzalutamide , induced high objective response rates and improved overall survival in patients with mcrpc.2 , 3 treatment with abiraterone or enzalutamide in the prechemotherapy setting led to a 50% decline in prostate - specific antigen ( psa50 ) response in 62% and 78% of these patients , respectively.2 , 3 however , sequential use of abiraterone and enzalutamide has resulted in much lower psa response rates with the use of the second att agent ( ie , abiraterone after enzalutamide , 10% to 15% ; enzalutamide after abiraterone , 20% to 30% ) .4 - 6 these data underscore the importance of identifying a predictive biomarker of resistance to att to prevent the use of subsequent futile therapy . potential mechanisms of resistance to att include ar amplification and mutation , as well as the expression of arsplicevariants.7a well - characterized mark c . 
eisenberger jun luo emmanuel s . antonarakis author affiliations and support information ( if applicable ) appear at the end of this article . the content is solely the responsibility of the authors and does not necessarily represent the official views of the national cancer institute or the national institutes of health . corresponding author : emmanuel s . 
 splice variant , ar - v7 , is a truncated form of fulllength ar ( ar - fl ) that lacks the ligand - binding domain but retains both the transactivation and dna - binding domains , allowing for constitutive ar signaling in the absence of androgen.8 - 10 in patients with mcrpc , detection of ar - v7 in circulating tumors cells ( ctcs ) was shown to predict resistance to novel atts.11 - 13 moreover , ar - v7 + patients had a significantly shorter overall survival , suggesting a prognostic value of ar - v7 in addition to its use as a predictive biomarker.11 , 13 chemotherapy is an alternative to att for arv7 + patients with mcrpc . 
detection of ar - v7 has been shown not to preclude response to taxanebased chemotherapy.14 , 15 further prospective investigation found a significant survival benefit with the use of taxanes versus atts in patients with ar - v7 + disease.16 interestingly , the presence of this splice variant is a dynamic feature with possible conversion from ar - v7 + to ar - v7 status after chemotherapy with taxanes.14 , 17 these data suggest that serial arv7 testing may guide the clinical treatment of patients with mcrpc . 
those patients with ar - v7 prostate cancer may continue to benefit from att , whereas chemotherapy may be more effective in patients with detectable ar - v7 transcript.18 if the clinical utility of ar - v7 testing can be confirmed , it may also have an economic benefit . in a recent study , we modeled the cost of treating all patients with mcrpc with abiraterone or enzalutamide versus using ar - v7 testing to direct treatment.19 by using a clinical scenario in which ar - v7 + patients were changed from treatment with abiraterone and / or enzalutamide to chemotherapy thus avoiding the cost of futile att therapy , ar - v7 testing resulted in a theoretical cost savings to the health care system of $150 million per year . 
to this end , since august 2015 , clinicalgrade ar - v7 testing performed in a clinical laboratory improvement amendments ( clia ) certified laboratory at johns hopkins university has been available to health care providers for clinical use.20 however , despite the commercial availability of this ar - v7 test , its clinical utility is unknown . 
here , we have retrospectively compiled questionnaire - based data on how ordering providers are applying the results of ar - v7 testing in their clinical practice to influence decision making . methods the analytical validation and test characteristics of our clia - grade ar - v7 assay have been described previously.20 our molecular pathology database was queried for all ar - v7 tests ordered by internal and external providers for clinical purposes . 
clinical results of this test were reported as ctc , ctc + / ar - v7 , or ctc + / ar - v7 + , because each of these categories is associated with different outcomes.12 a clinical utility questionnaire ( data supplement ) was generated for each ar - v7 test ordered and was mailed or e - mailed to each ordering provider . we defined a biomarker - based change in treatment as a confirmation of treatment choice or a change from one therapy to another after ar - v7 testing . 
the institutional review board at johns hopkins university approved this study and granted a waiver of consent to contact the provider of each ar - v7 test ordered because that was considered a clinical audit . 
the ordering provider was then contacted for participation and asked to complete a questionnaire pertaining to treatment decisions that were made on the basis of results of that specific ar - v7 test . 
if a provider did not wish to participate or the questionnaire was not returned after two attempts to contact the provider , data for that patient were not included in the analysis . one hundred fifty consecutive ar - v7 clinical test results were obtained between august 31 , 2015 , and august 31 , 2016 , representing the first 150 tests ordered . 
from these , 142 questionnaires ( 95% ) were completed and returned by 38 providers across 29 sites ( 28 in the united states [ in 22 states ] and one in canada )  . 
the significance level was set at p , .05 , and corrections were not performed for multiple comparisons . results information from 142 of 150 questionnaires sent ( 95% participant response rate ) were included in this analysis . 
the number of lines of additional systemic therapies for mcrpc among these patients was reported as follows : 24% ( n = 33 ) had received no other lines , 27% ( n = 39 ) had received one line , 27% ( n = 39 ) had received two lines , 13% ( n = 18 ) had received three lines , and 9% ( n = 13 ) had received four or more lines of systemic therapy before testing . 
of tests abiraterone enzalutamide abiraterone or enzalutamide abiraterone enzalutamide nave test result ctc 40 / 142 28.17 ctc + / ar - v7 42 / 142 29.58 8 / 40 20.0 11 / 40 27.5 21 / 40 52.5 8 / 42 19.0 20 / 42 47.62 14 / 42 33.33 ctc + / ar - v7 + 60 / 142 42.25 26 / 60 43.33 21 / 60 35.0 13 / 60 21.66 abbreviations : ar - v7 , androgen receptor splice variant 7 ; att , ar - targeted therapy ; ctc , circulating tumor cell ; n / n , number of patients in that category divided by total number of patients . overall , the prevalence of a ctc result was 28% , the prevalence of a ctc + / ar - v7 result was 30% , and the prevalence of a ctc + / ar - v7 + result was 42% . 
patients who were treated with abiraterone and / or enzalutamide resulted in a higher prevalence of ar - v7 detection compared with patients who were not treated with an att : 22% of treatment - nave patients were ar - v7 + ; after treatment with abiraterone or enzalutamide , 35% of patients were ar - v7 + ; and after treatment with abiraterone and enzalutamide , 43% of patients were ar - v7 +  . to assess the clinical utility of ar - v7 testing , providers were asked whether the ar - v7 status influenced their decision making . 
the majority of ar - v7 tests ( ctc or ctc + / ar - v7 ) did not change the clinical practice of the providers ( table 2 )  . 
however , almost two thirds ( 62% ) of ar - v7 + tests resulted in a change in management . in patients for whom treatment was changed , providers were then asked to specify the type of therapy selected on the basis of the test result . 
patients with an ar - v7 result ( ctc or ctc + / ar - v7 ) were preferentially treated with an att agent ( confirmed ar treatment , or changed from taxane to ar therapy )  . 
conversely , after an ar - v7 + result , most patients were changed from an att agent to taxane chemotherapy ( 43% ) or were enrolled in a clinical trial ( 43% )  . 
psa50 rr data were missing from 16% ( n = 12 ) and 22% ( n = 15 ) of questionnaires in which management was changed or not changed , respectively . we also investigated which systemic therapy was used in patients with mcrpc after progression on both abiraterone and enzalutamide , according to ar - v7 status ( table 5 )  . 
by contrast , ar - v7 + patients who had already received abiraterone and enzalutamide were more often treated on a clinical trial ( 54% ) compared with treatment using chemotherapy ( 19% )  . 
in the patients who were treated with docetaxel , those who were ar - v7 were commonly treated with standard chemotherapy ( ie , cabazitaxel ; 67% [ six of nine ] ) whereas ar - v7 + patients were more frequently placed on a clinical trial ( 58% [ 11 of 19 ] )  . finally , we examined provider treatment preferences for ar - v7 + patients irrespective of the prior therapies received ( table 6 )  . 
a minority of patients ( 7% ) received either enzalutamide or abiraterone despite an ar - v7 + result , whereas all ar - v7 + patients managed with observation ( 10% ) enrolled in hospice shortly thereafter . to summarize the data compiled from providers real - world experience with ar - v7 testing , we propose a hypothetical treatment algorithm for making decisions regarding patients with mcrpc using ar - v7 as a potential treatment - selection biomarker ( fig 1 )  . 
after first - line systemic therapy with abiraterone or enzalutamide , ar - v7 + patients would preferentially cross over to taxane - based therapy , whereas those who are ar - v7 may continue on a second att . 
because of occasional conversions from ar - v7 + to ar - v7 status , men progressing on taxane treatment can be retested and could potentially consider treatment with an att if the ar - v7 status reverts to negative . 
finally , even patients progressing after treatment with abiraterone and enzalutamide may be considered for ar - v7 testing if an ar - v7directed clinical trial is available . discussion the optimal sequencing of therapeutic agents in patients with mcrpc is unknown and remains a major challenge . 
to this end , the national comprehensive cancer network prostate cancer guidelines now suggest that ar - v7 testing can be considered and may play a role in guiding therapy selection in mcrpc , but at this time , these guidelines have not gone as far as recommending testing to determine treatment choice . 
in another recent consensus report , the majority of prostate cancer specialists polled ( 59% ) stated that ar - v7 testing would be useful for some ( majority or minority of ) patients with mcrpc.21 although further prospective validation of the predictive ability of ar - v7 is currently ongoing , here we investigated the clinical utility of ar - v7 testing in a real - world setting . we asked providers whether the result of the arv7 test influenced their clinical practice for that specific patient . 
although our findings are retrospective , they suggest that ar - v7 testing may possibly lead to improved clinical responses to treatment , at least in terms of psa50 rr . 
we did not assess for radiographic progression - free or overall survival , which may not have correlated with psa50 rr . the statistically significant psa50 rr difference between the change and no - change groups is largely driven by the ar - v7 + subgroup ( described in appendix table a3 )  . 
ar - v7 + patients for whom management did not change had a psa50 rr of 5% ( v 39% in ar - v71 patients for whom treatment was changed )  . 
we hypothesize that ar - v7 + patients in the change group were more commonly treated with chemotherapy compared with the no - change group , resulting in improved outcomes . 
we also acknowledge a high psa50 rr in ar - v7 + patients treated with chemotherapy and ar - v7 patients treated with att ( both in the change group )  . 
nonetheless , these data suggest that further prospective investigation is warranted to study biomarker - driven clinical outcomes . by using the treatment history captured by our questionnaires , we were able to observe an increasing prevalence of ar - v7 detection with prior exposure to atts , as expected . 
this finding is corroborated by the recent biomarker data from the armor3 - sv ( a study of galeterone compared with enzalutamide in men expressing androgen receptor splice variant - 7 mrna [ ar - v7 ] metastatic crpc ) trial , in which first - line patients with mcrpc who had previously received docetaxel for metastatic hormone - sensitive disease had a higher prevalence of ar - v7 detection compared with chemotherapy - nave patients.22 moreover , 79% of men with newly developed mcrpc had prior exposure to bicalutamide . 
the higher trend of ar - v7 + tests after treatment with docetaxel or bicalutamide , in the absence of a novel att , may suggest that total number of therapies ( ie , more advanced disease ) contributes to ar - v7 expression in addition to the known relationship with prior att exposure . 
another provocative hypothesis might be that docetaxel works as an ar - modulating therapy in prostate cancer , inhibiting microtubule - dependent nuclear transport of wild - type ar but not ar - v7 , thereby selecting for the emergence of ar - v7expressing clones during or after chemotherapy treatment . this study had some additional limitations . 
first , the prevalence of ar - v7 was probably overestimated compared with earlier reports because providers were more likely to order a test if the clinical scenario suggested that the test might be positive . other significant weaknesses of this analysis were its retrospective nature and reliance on selfreporting by providers . 
an audit of 14 randomly selected questionnaires determined that providers gave accurate responses to the questionnaire in most instances ( see appendix ) , suggesting that our data represent the true clinical course for each patient . 
finally , we concede that many patients will receive all atts approved by the us food and drug administration , regardless of ar - v7 status , because clinical responses to atts are sometimes observed in arv7 + patients.13 however , the clinical utility of arv7 testing may potentially be clearest in ar - v7 + patients who have additional atts still available for treatment . 
by identifying high - risk patients ( ie , arv7 + ) who have adequate performance status earlier in their mcrpc treatment , this would allow them to be treated with taxane therapy before the chemotherapy window closes . 
potential decision algorithm based on serial androgen receptor splice variant 7 ( ar - v7 ) testing across the castration - resistant prostate cancer landscape . after each line of therapy , we propose an algorithm for consideration of ar - v7 testing . 
after abiraterone and enzalutamide treatment , patients should be subject to ar - v7 testing only if an ar - v7directed clinical trial is available . ( * ) indicates limited clinical data supporting the use of atts in ar - v7 + patients that subsequently convert to ar - v7 . 
 ( ) denotes a clinical trial that does not require a positive ar - v7 test for ar - v7 patients , whereas ar - v7 + patients should consider an arv7directed trial , if available . first - line therapy clinical ar - v7 testing ? second - line therapy clinical ar - v7 testing ? third - line therapy abiraterone enzalutamide consider ar - v7directed clinical trial / taxane docetaxel taxane / trial enzalutamide abiraterone consider ar - v7directed clinical trial / taxane receive either chemotherapy or atts at their physicians discretion . we propose a decision algorithm using serial arv7 testing across the mcrpc landscape . 
this algorithm is based largely on published data suggesting that the presence of ar - v7 confers resistance to atts but does not influence response to taxane chemotherapy.11 , 13 , 14 , 16 we note that at this time , there is no clinical trial evidence to support the use of atts in ar - v7 + patients who convert to ar - v7 status after chemotherapy . 
in our study , 17 of 22 ar - v7 + patients were enrolled on a clinical trial that mandated ar - v7 detection as an entry criterion , suggesting that many of the tests in this study were ordered for the purpose of screening for a clinical trial . 
finally , there is ongoing debate in the prostate cancer community about whether ar - v7 detection is merely a proxy for ar amplification or overexpression and not an independent predictor of response to therapy or clinical outcomes.21 although several studies have shown that ar - v7 detection is indeed correlated with ar - fl expression , ar - v7 still remains independently prognostic in multivariable analysis after controlling for ar - fl levels.11 , 13 , 23 in conclusion , to our knowledge , this is the first study to examine the preliminary real - world clinical utility of clia - grade ar - v7 testing in patients with mcrpc . 
we show that ar - v7 testing influenced clinical decision making overall ( regardless of test results ) but that its utility was greatest in the setting of ar - v7 + results . 
 jun luo honoraria : gilead sciences , sanofi consulting or advisory role : tokai pharmaceuticals , sun pharmaceutical industries , janssen oncology research funding : sanofi ( inst ) , orion pharma ( inst ) , mirati therapeutics ( inst ) , gilead sciences ( inst ) , astellas pharma ( inst ) patents , royalties , other intellectual property : co - inventor of an ar - v7 biomarker technology assigned to johns hopkins university who licensed to tokai pharmaceuticals ; co - inventor of a technology licensed to qiagen emmanuel s . 
antonarakis honoraria : sanofi , dendreon , medivation , janssen biotech , essa , astellas pharma consulting or advisory role : sanofi , dendreon , medivation , janssen biotech , essa , astellas pharma research funding : janssen biotech ( inst ) , johnson & johnson ( inst ) , sanofi ( inst ) , dendreon ( inst ) , aragon pharmaceuticals ( inst ) , exelixis ( inst ) , millennium pharmaceuticals ( inst ) , genentech ( inst ) , novartis ( inst ) , astellas pharma ( inst ) , tokai pharmaceuticals ( inst ) travel , accommodations , expenses : sanofi , dendreon , medivation mark c . 
w81xwh - 15 - 2 - 0050 and w81xwh - 12 - 1 - 0605 ( j.l. ) , johns hopkins prostate specialized programs of research excellence grant p50 ca058236 ( j.l. ) , the patrick c . 
beer tm , armstrong aj , rathkopf de , et al : enzalutamide in metastatic prostate cancer before chemotherapy . n engl j med 368 : 138 - 148 , 2013 n engl j med 371 : 424 - 433 , 2014 4 . 
maughan bl , luber b , nadal r , et al : comparing sequencing of abiraterone and enzalutamide in men with metastatic castration - resistant prostate cancer : a retrospective study . 
dehm sm , schmidt lj , heemers hv , et al : splicing of a novel androgen receptor exon generates a constitutively active androgen receptor that mediates prostate cancer therapy resistance . 
hu r , dunn ta , wei s , et al : ligand - independent androgen receptor variants derived from splicing of cryptic exons signify hormone - refractory prostate cancer . 
antonarakis es , lu c , wang h , et al : ar - v7 and resistance to enzalutamide and abiraterone in prostate cancer . n engl j med 371 : 1028 - 1038 , 2014 12 . 
antonarakis es , lu c , luber b , et al : clinical significance of androgen receptor splice variant - 7 mrna detection in circulating tumor cells of men with metastatic castration - resistant prostate cancer treated with firstand second - line abiraterone and enzalutamide . 
antonarakis es , lu c , luber b , et al : androgen receptor splice variant 7 and efficacy of taxane chemotherapy in patients with metastatic castration - resistant prostate cancer . 
onstenk w , sieuwerts am , kraan j , et al : efficacy of cabazitaxel in castration - resistant prostate cancer is independent of the presence of ar - v7 in circulating tumor cells . 
scher hi , lu d , schreiber na , et al : association of ar - v7 on circulating tumor cells as a treatment - specific biomarker with outcomes and survival in castration - resistant prostate cancer . 
sprenger c , uo t , plymate s : androgen receptor splice variant v7 ( ar - v7 ) in circulating tumor cells : a coming of age for ar splice variants ? ann oncol 26 : 1805 - 1807 , 2015 19 . 
markowski mc , frick kd , eshleman jr , et al : cost - savings analysis of ar - v7 testing in patients with metastatic castration - resistant prostate cancer eligible for treatment with abiraterone or enzalutamide . 
lokhandwala pm , riel sl , haley l , et al : analytical validation of androgen receptor splice variant 7 detection in a clinical laboratory improvement amendments ( clia ) laboratory setting . 
gillessen s , attard g , beer tm , et al : management of patients with advanced prostate cancer : the report of the advanced prostate cancer consensus conference apccc 2017 . 
taplin me , antonarakis es , ferrante kj , et al : clinical factors associated with ar - v7 detection in armor3 - sv , a randomized trial of galeterone ( gal ) vs enzalutamide ( enz ) in men with ar - v7 + metastatic castration - resistant prostate cancer ( mcrpc )  . 
silberstein j , luber b , wang h , et al : clinical significance of ar mrna quantification from circulating tumor cells ( ctcs ) in men with metastatic castration - resistant prostate cancer ( mcrpc ) treated with abiraterone ( abi ) or enzalutamide ( enza )  . 
j clin oncol 35 , 2017 ( suppl ; abstr 132 ) we further queried our database to investigate the difference in the 50% decline in prostate - specific antigen ( psa50 ) response rate ( rr ) between the change and no - change groups on the basis of androgen receptor splice variant 7 ( ar - v7 ) status . 
for patients with ar - v7 + disease , the psa50 rr in those who did not change therapy was 5.3% ( one of 19 ) compared with 38.7% ( 12 of 31 ) in the change group ( table a3 )  . 
in the ar - v72 patients , the psa50 rr was 45.45% ( 15 of 33 ) in the no - change group versus 68.88% ( 22 of 32 ) in the change group . 
within both the ar - v7 + and ar - v7 groups , there was no discernible difference in number of lines of therapy between the change and no - change group . 
we also examined psa50 rr by treatment choice in those patients who had a change in treatment ( these data were not solicited for patients who did not have a treatment change in the questionnaire )  . 
in the 14 questionnaires audited , we found two minor discrepancies : ( 1 ) bicalutamide was listed in error as a prior therapy ( one time ) , and ( 2 ) the correct clinical trial was misidentified for a patient ( one time )  . subjective responses ( ie , clinical helpfulness and change in management ) were not assessed . 
dinardo , md1 introduction germline predispositions to hematologic malignancies in adult patients presenting with a diagnosis of myelodysplastic syndrome ( mds ) or acute myeloid leukemia ( aml ) are commonly underestimated . 
through next - generation sequencing ( ngs ) , many genes involved in hereditary mds or aml are now evaluated , including runx1 , cebpa , gata2 , tp53 , etv6 , and ddx41.1 , 2 germline gata2 mutations are a common cause for predisposition to mds or aml.3 patients with gata2 deciency can have manifestations ranging from mild cytopenias to life - threatening infections and myeloid neoplasia . 
the incidence of gata2 deciency is still unknown ; however , gata2 mutations may account for approximately 75% of adolescent patients with monosomy 7 mds.4 approximately 20% to 30% of gata2 mutations are inherited in an autosomal dominant fashion , whereas others are sporadic or de novo mutations.5 because molecular testing for mds and aml has become more commonplace , we recognize that some clinicians may incorrectly equate a negative ngs panel as ruling out any potential inherited malignancy predisposition . 
in addition , promoter mutations ( ie , ankrd26 ) and intronic mutations ( ie gata2 ) may often be missed if the ngs panel is restricted to exonic sequences . 
specic testing for fanconi anemia and dyskeratosis congenita when clinically indicated should be performed , for example , diepoxybutane or mitomycin cinduced chromosomal breakage assay and telomere length owuorescence in situ hybridization analysis , respectively . 
publically available registries and genomic data sets such as clinvar and gnomad are increasingly useful to provide insight into clinical signicance of identied variants . here , we report on two patients with a history of immunodeciency and myeloid neoplasia . 
1 is a 24 - year - old hispanic man who presented for evaluation of pancytopenia , mainly leukopenia associated with recurrent extensive warts on bilateral hands and recurrent panniculitis . 
his blood counts were as follows : white blood cell count , 3.2 109 / l ; hemoglobin , 14.1 g / dl ; and platelet count , 186 109 / l . 
concurrent ow cytometry analysis demonstrated a small population of aberrant myeloblasts , lack of hematogones , virtual absence of monocytes , and markedly reduced natural killer ( nk ) cells . 
a peripheral blood sample was obtained for ow cytometry study that showed no monocytes , nk cell lymphopenia ( 0.4% of lymphocyte gate ; fig 1b ) , and decreased b cells ( 3.8% of lymphocyte gate )  . 
a targeted exome sequence analysis of the following genes was performed on cultured skin broblasts : ankrd26 , cebpa , ddx41 , etv6 , gata2 , runx1 , srp72 , terc , tert , and tp53 . 
her blood counts showed a white blood cell count of 2.9 109 / l , with 75% neutrophils , 21% lymphocytes , 1% monocytes , hemoglobin of 10.1 g / dl , and platelet count of 164 109 / l . 
her past medical history was unremarkable , and her family history was negative for any immunologic or hematologic diseases . because of persistent ebv viremia , she received autologous ebv - specic cytotoxic t - lymphocyte cells . 
she received intensive cytarabine - based chemotherapy , and her induction course was complicated by an infection with mycobacterium fortuituflow cytometry analysis showed that she achieved complete remission with negative minimal residual disease . 
before proceeding with allogeneic hematopoietic stem - cell transplantation ( hsct ) from her sibling , the patient was referred to our hereditary hematologic malignancy clinic.6 a skin biopsy was performed for cultured skin broblasts , and genetic testing demonstrated a heterozygous deletion that included at least exon 2 of the gata2 gene . 
top : prehsct , the bone marrow shows a near absence of monocytes on ( left ) cd45 / ssc and ( middle ) cd14 ( thick arrows ) ; ( right ) no stage i or stage ii hematogones or mature b cells ( thin arrows )  . 
this variant has been previously reported in at least 29 other patients.4 , 10 - 14 the gata2 mutation detected in patient no . 2 was a large deletion involving at least exon 2 . 
to our knowledge , this is the rst time this specic deletion has been reported , although other in - frame or full gene gata2 deletions have been described.4 , 15 gata2 deciency can have various clinical presentations.11 , 16 patient no.1 presented initially with dermatologic problems , including extragenital warts and recurrent severe panniculitis ; mild cytopenias and hypocellular mds occurred later in his disease course . 
laboratory ndings include monocytopenia , dendritic cell cytopenias , b and nk lymphocytopenia , relative increase in t cells with an inverted cd4 : cd8 ratio , lack of hematogones , and various degrees of dysplasia.13 bm cellularity may vary from hypocellular marrow with severe cytopenias to normoor hypercellular marrow . 
 abou dalle et al stem cell exhaustion.3 the median age at diagnosis of 380 younger patients was approximately 20 years ( range , 12 to 35 years ) , with a high risk of progression to aml in 75% of carriers . 
complex cytogenetics and del ( 5q ) were not usually observed.5 patients with immunodeciency and recurrent infections along with a new diagnosis of mds at a younger age should be screened for an underlying germline mutation . 
genetic testing for germline mutations should sequence the most common genes responsible for familial predisposition to mds or aml , including ankrd26 , cebpa , ddx41 , etv6 , gata2 , runx1 , srp72 , samd9 , samd9l , terc , tert , and tp53 using nonhematopoietic tissue , usually cultured skin broblasts . gata2 sequencing should involve deletion and duplication analysis and intron 5 of the gata2 gene to detect all possible pathogenic variants . 
dinardo , md , department of leukemia , the university of texas md anderson cancer center , 1515 holcombe blvd , unit 0428 , houston , tx 77030 ; e - mail : cdinardo@mdanderson.org. support supported in part by specialized programs of research excellence grant no . 
cortes consulting or advisory role : bristol - myers squibb , biolinerx , novartis , pzer , amphivena therapeutics , daiichi sankyo , bio - path holdings , astellas pharma , takeda pharmaceuticals research funding : bristol - myers squibb ( inst ) , novartis ( inst ) , pzer ( inst ) , celgene ( inst ) , arog pharmaceuticals ( inst ) , astellas pharma ( inst ) , ambit biosciences ( inst ) , celator pharmaceuticals ( inst ) , immunogen ( inst ) , sun pharmaceutical industries ( inst ) , takeda pharmaceuticals ( inst ) alessandra ferrajoli research funding : celgene , genentech , acerta pharma dimitrios p . 
kontoyiannis employment : md anderson cancer center honoraria : gilead sciences , astellas pharma , t2 biosystems , mylan consulting or advisory role : merck , astellas pharma , fast track to growth , pzer , astellas pharma sa a . 
blood 129 : 424 - 447 , 2017 arber da , orazi a , hasserjian r , et al : the 2016 revision to the world health organization classication of myeloid neoplasms and acute leukemia . 
semin hematol 54 : 81 - 86 , 2017 dinardo cd , bannon sa , routbort m , et al : evaluation of patients and families with concern for predispositions to hematologic malignancies within the hereditary hematologic malignancy clinic ( hhmc )  . 
blood 80 : 575 - 581 , 1992 vicente c , conchillo a , garca - s anchez ma , et al : the role of the gata2 transcription factor in normal and malignant hematopoiesis . 
crit rev oncol hematol 82 : 1 - 17 , 2012 tsai fy , orkin sh : transcription factor gata - 2 is required for proliferation / survival of early hematopoietic cells and mast cell formation , but not for erythroid and myeloid terminal differentiation . 
hsu ap , johnson kd , falcone el , et al : gata2 haploinsufciency caused by mutations in a conserved intronic element leads to monomac syndrome . blood21 : 3830 - 3837 , 2013 11 . 
kazenwadel j , secker ga , liu yj , et al : loss - of - function germline gata2 mutations in patients with mds / aml or monomac syndrome and primary lymphedema reveal a key role for gata2 in the lymphatic vasculature . 
 c mechanistic learning for combinatorial strategies with immuno - oncology drugs : can model - informed designs help investigators ? joseph ciccolini , pharmd , phd1 ; dominique barbolosi , phd1 ; nicolas andr e , md , phd1 , 2 ; fabrice barlesi , md , phd3 ; and s ebastien benzekry , phd4 the past couple of years have seen an unprecedented number of failures of clinical trials investigating combinatorial strategies with immuno - oncology drugs ( iods )  . beyond the highly publicized crashes of the mystic study1 ( antipd - l1 plus anti - ctla4 in nonsmall - cell lung cancer [ nsclc ] ) or the echo - 301 trial2 ( antipd - 1 and anti - ido in melanoma ) , many other attempts to combine immunotherapy with radiation therapy ( rt ) , 3 chemotherapy , 4 metronomic chemotherapy , 5 or antiangiogenics6 have similarly led to disappointing results . 
because successful immunotherapy is restricted today to a limited number of patients in a limited number of cancers ( melanoma , lung cancer , head and neck cancer , and kidney cancer , with 5 - year survival rates , 40% ) , developing appropriate strategies to stretch efcacy remains critical ( eg , by turning cold tumors [ noninammatory with lack of inltrating t cells ] into hot ones [ inltrated by t cells ] )  . 
several studies successfully associated conventional treatments with iods in comparative phase iii trials.7 , 8 however , these trials should not hide the high attrition rate of too many other studies . 
one of the common characteristics of the trials is the lack of computational pharmacology support , plus the lack of prior knowledge regarding the pharmacokinetics ( pk ) / pharmacodynamics ( pd ) relationships of the combined treatments . 
actually , comes from the fact that , sometimes , some combinatorial clinical trials manage to be successful . author affiliations and support information ( if applicable ) appear at the end of this article . accepted on march 20 , 2020 and published at ascopubs.org / journal / po on may 8 , 2020 : doi 1200 / po.19.00381 to improve the design of such combinatorial trials beyond trial - and - error methods , we propose an innovative strategy termed mechanistic learning ( fig 1 )  . we dene it as the combination of mechanistic modelingsimulation of the kinetics of pathophysiologic processesand statistical ( machine ) learning . using data generated from previous clinical trials and preclinical experiments , it consists in building computational models able to simulate and predict the toxicity and efcacy outcomes of candidate regimens . the optimal scheduling is then selected for clinical trial testing . 
limited options when performing combinatorial trials are therefore a major caveat , possibly explaining many failures , or at least limiting the conclusions regarding the real intrinsic potential of a given combination . 
for instance , in the checkmate032 study , the antipd - 1 nivolumab and the antictla4 ipilimumab were administered to patients with nsclc using only 2 dosing modes ( ie , 1 and 3 mg / kg and vice versa )  . 
these doses were chosen because they were already combined in a previous phase i study.9 in dose - nding trials , up to 5 dose levels ranging from 0.1 to 20 mg / kg have been tested for nivolumab and ipilimumab used as single agents without reaching dose - limiting toxicities.10 , 11 consequently , at least 25 different combinations in dosing could have been explored in checkmate - 032 , not to mention the countless variations in sequencing and scheduling . 
in the subsequent checkmate - 143 study , the same strategy failed to improve survival in patients with glioblastoma.12 another example of a poorly designed study is the modul umbrella trial , which tested a triple combination of uoropyrimidines , the antiangiogenic bevacizumab , and the antipd - l1 atezolizumab in patients with metastatic colorectal cancer ( mcrc )  . 
baseline data can be composed of demographic , clinical , pathologic ( eg , histologic type ) , molecular ( eg , genetic mutations ) , or biologic ( eg , blood counts ) variables . 
survival data ( eg , progression - free or overall survival ) can also be modeled with a mechanistic basis ( instead of biologically agnostic survival analysis based on , eg , cox regression ) , using adapted , survival learning statistical methods . 
ct1 , rst chemotherapy ; ct2 , second chemotherapy ; mtki , maintenance tyrosine kinase inhibitor ; ps , performance status ; tgi , tumor growth inhibition ; tki , tyrosine kinase inhibitor . surprisingly , in this study , all drugs were administered concomitantly at xed dosing . 
this combination failed to exhibit signicant efcacy in terms of progression - free survival , and thus , the conclusion was that adding atezolizumab to standard of care for maintenance in mcrc showed no benet.13 actually , this conclusion may sound peremptory because it is not possible to know whether or not different dosing or scheduling with exactly the same drugs would have performed better . 
for instance , trial of nivolumab , 23 the impact of dosing ( ie , 0.1 - 10 mg / kg ) on pd - 1 receptor occupancy was investigated . 
similar target engagement ( ie , 64% - 70% ) was achieved regardless of the dosing , thus prompting several observers to conclude that pk / pd relationships were at with iods and , therefore , that interpatient variability was not an issue . 
however , in this seminal study , pd - 1 inhibition was measured only on circulating t lymphocytes extracted from peripheral blood and not on inltrated t lymphocytes in the tumor microenvironment . 
importantly , the pharmacokinetics of most therapeutic monoclonal antibodies is characterized by large interindividual variability and reduced ability to diffuse the vascular space and reach solid tumors.24 out of therefore , to what extent differences in nivolumab dosing could affect or not target engagement at the tumor levels , and not only in circulating t cells , remains to be fully investigated . 
critically , it would also be highly informative to analyze the data generated using the initial model to close the mechanistic learning loop . using similar principles for tumor heterogeneity , others have proposed the concept of adaptive therapy , suggesting individuals be treated only upon disease progression.38 this was further successfully translated at bedside in patients with metastatic castration - resistant prostate cancer.39 such a strategy could help to personalize combinations of iods and aromatase inhibitors in the neoadjuvant treatment of breast cancer.40 despite their scarcity , these studies highlight how application of mathematical modeling in clinical trials in oncology is now feasible and can rationalize study design . these innovative methods are yet to be extended to iod combinations . 
modeling immunotherapy has recently been applied to gain insights on optimal modes for combinations with rt.41 - 43 for instance , kosinsky et al42 were able to simulate multiple sequences of antipd - 1 treatment in combination with rt and validated their results using preclinical data . 
 commentary the general modeling methodology that could be undertakenmechanistic learningis a combination of mechanistic modeling and statistical learning , either from machine learning , mixed - effects learning , 45 or survival learning , 46 for integration of the multimodal data arising from clinical trials or routine management ( fig 1 )  . 
as output , it would provide informative simulations of the effect of various doses and schedules to aid decisions in early clinical studies . these would consist of predicted probabilities of graded toxicities , tumor growth kinetics in response to treatment , and survival outcomes . 
of note , there is a major trend by health regulatory agencies such as the us food and drug administration to call for incorporating extensive modeling and simulation into clinical research.47 in this respect , and regarding the current challenges with iods , 48 we believe that mechanistic learning could be a valuable tool for decision making when setting up combinatorial strategies . conclusion after a rst phase of enthusiasm , success stories with immunotherapy seem to have reached a glass ceiling because many studies now fail to further stretch either response rates or survival.49 consequently , combining immune checkpoint inhibitors with other treatments likely to boost tumor immunity is a rising strategy in clinical oncology . 
for more information about ascos conict of interest policy , please refer to or ascopubs . org / po / author - center . open payments is a public database containing information reported by companies about payments made to us - licensed physicians ( open payments )  . joseph ciccolini honoraria : pierre fabre , pzer , roche , novartis research funding : roche , merck serono travel , accommodations , expenses : astrazeneca nicolas andr e research funding : bristol - myers squibb ( inst ) travel , accommodations , expenses : bristol - myers squibb fabrice barlesi honoraria : genentech , pzer , pierre fabre , astrazeneca , bristol - myers squibb , boehringer ingelheim , eli lilly , novartis , merck serono , msd oncology , takeda , bayer consulting or advisory role : genentech , pzer , novartis , pierre fabre , bristol - myers squibb , astrazeneca / medimmune , boehringer ingelheim , eli lilly , merck serono , msd oncology , takeda , bayer research funding : genentech ( inst ) , astrazeneca / medimmune ( inst ) , bristol - myers squibb ( inst ) , pierre fabre ( inst ) , abbvie ( inst ) , amgen ( inst ) , bayer ( inst ) , boehringer ingelheim ( inst ) , eisai ( inst ) , eli lilly ( inst ) , ipsen ( inst ) , innate pharma ( inst ) , novartis ( inst ) , merck serono ( inst ) , msd oncology ( inst ) , pzer ( inst ) , sano - aventis ( inst ) , takeda ( inst ) travel , accommodations , expenses : genentech , bristol - myers squibb , astrazeneca / medimmune , msd oncology no other potential conicts of interest were reported . acknowledgment we thank elena ivanchenko for graphic assistance . 
in memory of marie - christine masini . references 41 : 41 - 48 , 2019 rizvi na , chul cho b , reinmuth n , et al : durvalumab with or without tremelimumab vs platinum - based chemotherapy as rst - line treatment for metastatic nonsmall cell lung cancer : mystic . 
mcbride sm , sherman ej , tsai cj , et al : a phase ii randomized trial of nivolumab with stereotactic body radiotherapy ( sbrt ) versus nivolumab alone in metastatic ( m1 ) head and neck squamous cell carcinoma . 
 ciccolini et al rothschild s , zippelius a , savic s , et al : sakk 16 / 14 : anti - pd - l1 antibody durvalumab ( medi4736 ) in addition to neoadjuvant chemotherapy in patients with stage iiia ( n2 ) non - small cell lung cancer ( nsclc ) a multicenter single - arm phase ii trial . 
j clin oncol 36 , 2018 ( suppl 15 ; abstr tps8584 ) 1200 / jco.2018.36.15_suppl.tps8584 toulmonde m , penel n , adam j , et al : use of pd - 1 targeting , macrophage inltration , and ido pathway activation in sarcomas : a phase 2 clinical trial . 
jama oncol 4 : 93 - 97 , 2018 gao j , karam ja , tannir nm , et al : a pilot randomized study evaluating nivolumab ( nivo ) or nivo + bevacizumab ( bev ) or nivo + ipilimumab ( ipi ) in patients with metastatic renal cell carcinoma ( mrcc ) eligible for cytoreductive nephrectomy ( cn ) , metastasectomy ( ms ) or post - treatment biopsy ( bx )  . 
j clin oncol 36 , 2018 ( suppl 15 ; abstr 4520 ) socinski ma , jotte rm , cappuzzo f , et al : atezolizumab for rst - line treatment of metastatic nonsquamous nsclc . 
hellmann md , rizvi na , goldman jw , et al : nivolumab plus ipilimumab as rst - line treatment for advanced non - small - cell lung cancer ( checkmate 012 ) : results of an open - label , phase 1 , multicohort study . 
ribas a , camacho lh , lopez - berestein g , et al : antitumor activity in melanoma and anti - self responses in a phase i trial with the anti - cytotoxic t lymphocyteassociated antigen 4 monoclonal antibody cp - 675 , 206 . 
grothey a , tabernero j , arnold d , et al : fluoropyrimidine and bevacizumab plus or minus atezolizumab as rst - line treatment for braf wild type metastatic colorectal cancer : findings from the modul trial of biomarker - driven maintenance . 
schaer da , beckmann rp , dempsey ja , et al : the cdk4 / 6 inhibitor abemaciclib induces a t cell inamed tumor microenvironment and enhances the efcacy of pd - l1 checkpoint blockade . 
heery cr , osullivan - coyne g , madan ra , et al : avelumab for metastatic or locally advanced previously treated solid tumours ( javelin solid tumor ) : a phase 1a , multicohort , dose - escalation trial . 
lindauer a , valiathan cr , mehta k , et al : translational pharmacokinetic / pharmacodynamic modeling of tumor growth inhibition supports dose - range selection of the antipd - 1 antibody pembrolizumab . 
long gv , tykodi ss , schneider jg , et al : assessment of nivolumab exposure and clinical safety of 480 mg every 4 weeks at - dosing schedule in patients with cancer . 
h enin e , meille c , barbolosi d , et al : revisiting dosing regimen using pk / pd modeling : the model1 phase i / ii trial of docetaxel plus epirubicin in metastatic breast cancer patients . 
barlesi f , imbs d - c , tomasini p , et al : mathematical modeling for phase i cancer trials : a study of metronomic vinorelbine for advanced non - small cell lung cancer ( nsclc ) and mesothelioma patients . 
yu ha , sima c , feldman d , et al : phase 1 study of twice weekly pulse dose and daily low - dose erlotinib as initial treatment for patients with egfr - mutant lung cancers . 
poleszczuk jt , luddy ka , prokopiou s , et al : abscopal benets of localized radiotherapy depend on activated t cell trafcking and distribution between j immunother cancer 6 : 17 , 2018 metastatic lesions . 
claret l , girard p , hoff pm , et al : model - based prediction of phase iii overall survival in colorectal cancer on the basis of phase ii tumor dynamics . 
coosemans a , vankerckhoven a , baert t , et al : combining conventional therapy with immunotherapy : a risky business ? eur j cancer 113 : 41 - 44 , 2019 49 . 
murray leslie samuel paolo nuciforo jose jimenez guillem argiles rodrigo dienstmann josef tabernero lucia picariello luca messerini stefania nobili enrico mini kieran sheahan elizabeth ryan ( continued ) purpose transcriptomic profiling of colorectal cancer ( crc ) has led to the identification of four consensus molecular subtypes ( cms1 to 4 ) that have prognostic value in stage ii and iii disease . 
2018 by american society of clinical oncology introduction colorectal cancer ( crc ) has the third highest worldwide incidence.1 although 75% of patients present with operable diseasemainly stages ii and iiiapproximately 40% experience disease recurrence.2 compared with surgery alone , adjuvant chemotherapy improves survival in only approximately 3% of patients with stage ii disease , rising to 15% to 20% for those with stage iii disease . 
 contributed equally to this work . corresponding author : daniel longley , phd , centre for cancer research and cell biology , queens university belfast , 97 lisburn rd , belfast , bt9 7bl united kingdom ; e - mail : d.longley@qub.ac.uk. licensed under the creative commons attribution 4.0 license significant advances have been made in the molecular stratification of crc , leading to the identification of four consensus molecular subtypes ( cms1 to 4 ) .3 cms1 is enriched for microsatellite instability , is immune rich , and correlates with good prognosis , and cms4 is stromal rich , with high levels of cancer - associated fibroblasts , and has a relatively poor prognosis . 
 cms3 is defined by the activation of multiple metabolic pathways , potentially as a result of its enrichment for kras mutations.4 the epithelial - rich cms2 is the largest group , accounting for approximately 40% of all tumors . 
of these , 188 samples with > 50% tumor content passed quality control and were subjected to rna and dna analysis ( appendix )  . transcriptomics high - quality transcriptomics data were obtained for 156 of the 188 samples ( almac xcel array ; almac diagnostics , craigavon , united kingdom )  . 
residual technical batch effects were corrected using the combat method ( sva package ) , and data were deposited in the national center for biotechnology information gene expression omnibus repository ( gse103479 )  . 
the clinical pathologic details of this cohort are provided in table 1 . data analysis gse3958210 and gse1433311 crc data sets were downloaded from the national center for biotechnology information gene expression omnibus repository and their respective cel files uploaded into r . 
similar results were obtained in the larger gse39582 cohort for stage ii disease ( log - rank test p = .071 ) , whereas in stage iii disease , this correlation reached significance ( p = .001 ; data supplement )  . 
when we combined the taxonomy and gse39582 cohorts to increase statistical power , the benefit from adjuvant chemotherapy for cms2 was significant in both stage ii disease ( log - rank test p = .02 ; hazard ratio [ hr ] , 0.21 [ wald test p = 3.52 102 ] ; fig 1a ) and stage iii disease ( log - rank test p < .001 ; hr , 0.22 [ wald test p = 1.48 104 ] ; fig 1b )  . 
of note , no significant benefit from adjuvant chemotherapy was observed in cms1 or cms4 , although a nonsignificant trend was observed in cms4 stage iii disease ( log - rank test p = .089 ; data supplement )  . these results suggest that the more epithelial cms2 and cms3 subgroups benefit from adjuvant chemotherapy . 
in support of this , in a combined analysis of cms2 and cms3 , benefit from adjuvant chemotherapy was significant in both stage ii disease ( log - rank test p = .0042 ; hr , 0.16 [ wald test p = .012 ] ; fig 1c ) and stage iii disease ( log - rank test p < .001 ; hr , 0.20 [ wald test p = 1.14 106 ] ; fig 1d )  . 
in contrast , in a combined analysis of the cms1 and cms4 subgroups , no benefit from adjuvant chemotherapy was observed ( data supplement )  . when cms2 subgroup results for stage ii disease were adjusted for t stage ( t4 v t3 ) , age , and sex using cox proportional hazards regression analysis , the significance of the benefit from chemotherapy was lost ( hr , 0.31 ; wald test p = .121 ; log likelihood ratio , 7.0 105 ; fig 1e ) ; however , in stage iii disease , adjusting for t stage ( t4 or n2 v t1 to t3 / n1 ) , age , and sex , the significance of benefit from chemotherapy in cms2 was maintained ( hr , 0.27 ; wald test p = .007 ; log likelihood p = 3.25 105 ; fig 1f )  . 
in cox proportional hazards regression analyses of the combined cms2 and cms3 subgroups , the significance of benefit from chemotherapy was maintained in stage ii disease ( hr , 0.23 ; wald test p = .049 ; log likelihood ratio , 2.72 105 ; fig 1g ) and stage iii disease ( hr , 0.21 ; wald test p < .001 ; log likelihood p = 3.19 107 ; fig 1h )  . clinical implications of tumor - intrinsic stratification in cms2 as previously reported , 6 there are limited associations between cms and cris classifications for example , cms4 is distributed relatively evenly between the five cris subtypes ( data supplement ) ; however , some clear patterns were observed , with cms2 almost exclusively distributed between cris - c , - d , and - e ( fig 2a )  . 
 subsequently , we investigated whether substratification of cms2 into cris - c , - d , or - e could identify a more specific subset of patients with stage ii and iii disease who derive benefit from adjuvant chemotherapy . 
these results were confirmed in an additional independent cohort , gse14333 ( logrank test p = .02 ; hr , 0.12 [ wald test p = .05 ] ; data supplement )  . 
in the other 2 cris subgroups ( cris - a and - b ) , no significant benefit from adjuvant chemotherapy was observed in either stage ii or iii disease , although a nonsignificant trend was observed in cris - a for stage iii disease ( p = .057 ; data supplement ) , which is consistent with this subgroup being enriched for cms3 , where a significant benefit was observed ( data supplement )  . 
when cris - c results were adjusted for t stage , age , and sex using cox proportional hazards regression analyses , the benefit from chemotherapy maintained significance in stage ii disease ( hr , 0.12 ; wald test p = .045 ; log likelihood p = .0054 ; fig 2d ) and stage iii disease ( hr , 0.27 ; wald test p = .02 ; log likelihood p = 1.11 103 ; fig 2e ) ; furthermore , for combined stage ii and iii disease , adjusted hr was 0.20 ( wald test p < .001 ; log likelihood p = 7.5 106 ; data supplement )  . 
 ( a and b ) kaplan - meier plots of 5 - year overall survival ( os ) for consensus molecular subtype 2 ( cms2 ) patients who received adjuvant fluorouracil ( fu ) - based treatment ( gold ) and those who did not receive treatment ( surgery alone , blue ) , in the ( a ) stage ii combined ( taxonomy and gse39582 ) cohort and the ( b ) stage iii combined ( taxonomy and gse39582 ) cohort . 
 ( c and d ) kaplan - meier plots for 5 - year os for combined cms2 and cms3 patients in the ( c ) stage ii combined ( taxonomy and gse39582 ) cohort and the ( d ) stage iii combined ( taxonomy and gse39582 ) cohort . 
to account for potential intratumoral heterogeneity of putative biomarkers in specific tumor regions , tmas were generated from the taxonomy cohort to incorporate three cores each from ct , if , and tumor - adjacent sr regions . 
cd8 and cd3 levels were defined using immunohistochemistry , and patients were stratified into high and low groups using the median as cutoff ( representative cd8 and cd3 images ; figs 3a and 3b )  . 
we further assessed cd8 + lymphocytes in histologically normal tissue adjacent to the tumor and found no difference in survival between high and low cd8 levels ( log - rank test p = .72 ; data supplement )  . 
of note , no correlations were found between cd3 + lymphocyte levels and prognosis ( if log - rank test p = .55 ; sr log - rank test p = .75 ; ct log - rank test p = .8 ; normal log - rank test p = .82 ; data supplement )  . for each patient , cd8 scores in each tumor subregion correlated closely with one another ( p < .001 ; data supplement )  . 
 as expected on the basis of correlations for individual regions ( data supplement ) , applying this tumor average score to the combined stage ii and iii taxonomy cohort revealed that high levels of cd8 + lymphocytes identified cris - c patients with good prognosis ( log - rank p = .0031 ; hr , 12.18 [ wald test p = .0191 ] ; fig 4a )  . 
in contrast , average cd3 scores , which again did not correlate closely with average cd8 scores ( fig 3c ) , were not prognostic ( fig 4b )  . 
of note , cd8 mrna expression was unable to distinguish good and poor prognosis patients ( log - rank p = .83 ; data supplement ) , which indicates the need for immunohistochemistry in combination with transcriptomic profiling for effective prognostication . 
 ( e - h ) forest plots show the results from the adjusted cox proportional hazards regression analysis for the ( e ) stage ii cms2 combined cohort , the ( f ) stage iii cms2 combined cohort , the ( g ) stage ii cms2 and cms3 combined cohort , and the ( h ) stage iii cms2 and cms3 combined cohort . 
for adjusted analyses , data are stratified by treatment and adjusted for t stage , sex , and age in stage ii , and for age and sex in stage iii . 
 ( a ) caleydo plots display mapping of patient samples from the consensus molecular subtype 2 to the colorectal cancer intrinsic subtypes ( cris ) in the combined ( taxonomy and gse39582 ) data sets . 
 ( a and b ) representative images of samples display high and low ( a ) cd8 and ( b ) cd3 expression in each of the three tumor regions sampled : invasive front ( if ) , stromal rich ( sr ) , and central tumor ( ct )  . 
 ( a - c ) kaplan meier plots of patients with ( a ) cd8 - high versus cd8 - low stage ii and iii disease in the colorectal cancer intrinsic subtype ( cris ) - c surgery - only , taxonomy cohort ; ( b ) cd3 - high versus cd3 - low stage ii and iii disease in the cris - c surgery - only , taxonomy cohort ; and ( c ) cd8 - high versus cd8low stage ii disease in the cris - c surgery - only , taxonomy cohort . 
therapeutic benefit from adjuvant chemotherapy is modest for this group as a whole , with an absolute improvement in survival of approximately 3%.18 - 22 currently , additional pathologic characteristics , such as obstruction , perforation , extramural venous invasion , and t stage ( t4 ) , are used to identify poor prognostic stage ii disease and guide the decision of whether to start chemotherapy treatment.23 additional methods of assessing the risk of recurrence in the adjuvant disease setting have been the focus of many studies in recent years , 24 - 29 which has led to the development of the 12 - gene oncotype dx assay.30 this algorithm has been extensively clinically tested31 - 33 and demonstrated to identify patients with stage ii disease who are at higher risk of recurrence and patients with stage iii disease who are at lower risk of recurrence.34 , 35 additional signatures have been proposed , including the 18 - gene prognostic classifier , known as coloprint , 36 and the 634 - gene prognostic classifier , known as coldx.27 the current study indicates that the transcriptionally definable cms2 / cris - c patient subgroup may be the cohort of patients within stage ii disease that benefits from standard adjuvant fu - based chemotherapy . 
these data correlate well with our previous study on the prognostic significance of immune - derived programmed death ligand 1 mrna expression in crc , in which we postulated that patients with low immune infiltrates would significantly benefit from adjuvant fu - based chemotherapy after surgery.9 , 37 meta - analysis of the idea ( international duration evaluation of adjuvant chemotherapy ) collaboration examined whether a 3 - month duration of oxaliplatin containing adjuvant chemotherapyfolfox4 , modified folfox6 , or xeloxis as effective as a 6 - month schedule in patients with stage iii crc . 
this study found that the 3 - month treatment was almost as effective as the 6 - month treatment and reduced the risk of treatment associated toxicity , thus concluding that a 3 - month treatment would be more beneficial for patients with low - risk ( t1 to 3 / n1 tumors ) stage iii disease.38 our study suggests that levels of cd8 + lymphocytes could also be used to identify such low - risk patients , at least in the cris - c subgroup . 
of note , cris - c is enriched for mutant tp53 and wild - type kras tumors , 6 but neither of these established molecular markers provided additional information with regard to disease outcome within the cris - c subgroup . collectively , these results provide the first evidence of the predictive value of the now well established cms and more recently described cris transcription - based classification systems . 
 our results also emphasize the utility of combining cms and cris subtyping in a substratification strategy to maximize clinical benefit from adjuvant fu - based chemotherapy in patients with stage ii and iii crc . 
murray , leslie samuel , jose jimenez , guillem argiles , lucia picariello , luca messerini , stefania nobili , enrico mini , elizabeth ryan , sandra van schaeybroeck , daniel b . 
longley tumor - infiltrating lymphocytes , would potentially enable the prospective identification of the cris - c / cd8 - low stage ii patients who significantly benefit from adjuvant fu - based chemotherapy . 
however , we recognize that there are a number of limitations in the current study , which was conducted on a relatively small number of retrospective samples that were collected outside of clinical trials , and we realize that this hypothesis - generating study now requires validation in either larger patient cohorts or stratified trial cohorts enriched for the cris - c patient subtype . 
nonetheless , this study suggests that transcription - based classification systems , such as cms and cris , have the potential to be developed into patient stratification tools and , when used alone or alongside other molecular pathology approaches , such as immunohistochemistry , could enable the selection of patients with crc who are most likely to benefit from adjuvant chemotherapy , while at the same time sparing nonresponders the potentially harmful treatment related adverse events and sequelae of chemotherapy . 
of importance , the cris subtyping method uses gene expression from tumor epithelial cells only and is independent of stromal - derived signals ; therefore , the cris subgroups can be detected irrespective of the profiling technology used or the tissue source.15 such robustness and reproducibility are critical for clinical translation . 
murray , leslie samuel , paolo nuciforo , jose jimenez , guillem argiles , josef tabernero , lucia picariello , luca messerini , stefania nobili , enrico mini , kieran sheahan , elizabeth ryan , sandra van schaeybroeck , mark lawler , daniel b . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . richard wilson consulting or advisory role : merck serono , sirtex medical , amgen , servier , clovis oncology , halozyme , bristol - myers squibb research funding : almac group ( inst ) travel , accommodations , expenses : merck serono , amgen vicky m . 
murray research funding : vertebrate antibodies ( inst ) leslie samuel consulting or advisory role : mundipharma research funding : mologen ( inst ) , roche ( inst ) , merck ( inst ) , eli lilly ( inst ) , taiho pharmaceutical ( inst ) travel , accommodations , expenses : mologen wendy l . 
longley stock and other ownership interests : fusion antibodies consulting or advisory role : astex pharmaceuticals sandra van schaeybroeck no relationship to disclose mark lawler honoraria : pfizer research funding : astex pharmaceuticals patents , royalties , other intellectual property : inhibitors of the antiapoptotic protein flip travel , accommodations , expenses : astex pharmaceuticals affiliations wendy l . 
murray and leslie samuel , national health service grampian , aberdeen , united kingdom ; najeeb ashraf syed and puthen veettil jithesh , sidra medical and research center , qatar ; paolo nuciforo , jose jimenez , guillem argiles , rodrigo dienstmann , and josef tabernero , university hospital vall dhebron , barcelona , spain ; lucia picariello , luca messerini , stefania nobili , and enrico mini , university of florence , florence , italy ; and kieran sheahan and elizabeth ryan , university college dublin , dublin , ireland . funded by cancer research uk grants no . 
lenz h - j , ou f - s , venook ap , et al : impact of consensus molecular subtyping ( cms ) on overall survival ( os ) and progression free survival ( pfs ) in patients ( pts ) with metastatic colorectal cancer ( mcrc ) : analysis of calgb / swog 80405 ( alliance )  . 
dunne pd , mcart dg , bradley ca , et al : challenging the cancer molecular stratification dogma : intratumoral heterogeneity undermines consensus molecular subtypes and potential diagnostic value in colorectal cancer . 
marisa l , de reynis a , duval a , et al : gene expression classification of colon cancer into molecular subtypes : characterization , validation , and prognostic value . 
jorissen rn , gibbs p , christie m , et al : metastasis - associated gene expression changes predict poor outcomes in patients with dukes stage b and c colorectal cancer . 
galon j , costes a , sanchez - cabo f , et al : type , density , and location of immune cells within human colorectal tumors predict clinical outcome . 
hutchins gga , treanor d , wright a , et al : intratumoral stromal morphometry predicts disease recurrence but not response to 5 - fluorouracil : results from the quasar trial of colorectal cancer . 
roepman p , schlicker a , tabernero j , et al : colorectal cancer intrinsic subtypes predict chemotherapy benefit , deficient mismatch repair and epithelial - to - mesenchymal transition . 
figueredo a , charette ml , maroun j , et al : adjuvant therapy for stage ii colon cancer : a systematic review from the cancer care ontario program in evidence - based cares gastrointestinal cancer disease site group . 
kelley rk , venook ap : prognostic and predictive markers in stage ii colon cancer : is there a role for gene expression profiling ? clin colorectal cancer 10 : 73 - 80 , 2011 26 . 
kennedy rd , bylesjo m , kerr p , et al : development and independent validation of a prognostic assay for stage ii colon cancer using formalin - fixed paraffin - embedded tissue . 
tabernero j , salazar r , roepman r , et al : additional validation of a genomic signature ( coloprint ) for the risk stratification of stage ii colon cancer patients . 
oconnell mj , lavery i , yothers g , et al : relationship between tumor gene expression and recurrence in four independent studies of patients with stage ii / iii colon cancer treated with surgery alone or surgery plus adjuvant fluorouracil plus leucovorj clin oncol 28 : 3937 - 3944 , 2010 31 . 
gray rg , quirke p , handley k , et al : validation study of a quantitative multigene reverse transcriptase - polymerase chain reaction assay for assessment of recurrence risk in patients with stage ii colon cancer . 
venook ap , niedzwiecki d , lopatin m , et al : biologic determinants of tumor recurrence in stage ii colon cancer : validation study of the 12 - gene recurrence score in cancer and leukemia group b ( calgb ) 9581 . 
cartwright t , chao c , lee m , et al : effect of the 12 - gene colon cancer assay results on adjuvant treatment recommendations in patients with stage ii colon cancer . 
srivastava g , renfro la , behrens rj , et al : prospective multicenter study of the impact of oncotype dx colon cancer assay results on treatment recommendations in stage ii colon cancer patients . 
dunne pd , mcart dg , oreilly pg , et al : immune - derived pd - l1 gene expression defines a subgroup of stage ii / iii colorectal cancer patients with favorable prognosis who may be harmed by sdjuvant chemotherapy . 
shi q , sobrero af , shields af , et al : prospective pooled analysis of six phase iii trials investigating duration of adjuvant ( adjuv ) oxaliplatin - based therapy ( 3 vs 6 months ) for patients ( pts ) with stage iii colon cancer ( cc ) : the idea ( international duration evaluation of adjuvant chemotherapy ) collaboration . 
 appendix development of a multiomics patient cohort the taxonomy cohort was assembled from an initial cohort of 363 patients with stage ii and iii disease from four european centers ( vall dhebron institute of oncology , barcelona , spain ; st vincents university hospital , dublin , ireland ; university of florence , florence , italy ; and university of aberdeen , aberdeen , united kingdom )  . 
this work was approved by the medicine , dentistry , and biomedical sciences school ethics committee ( ref : 12 / 12v4 )  . samples from 194 patients with 50% or more tumor content as assessed by hematoxylin and eosin staining were subjected to rna extraction . 
 data for samples were preprocessed and aligned according to best practices ( broad institute : tute.org / gatk / discussion / 3060 / how - should - i - pre - process - data - from - multiplexed - sequencing - and - multi - library - designs ) using burrows - wheeler aligner for alignment and gatk 3.4 for realignment and recalibration . 
cd8 was detected using the anti - cd8 antibody c8 / 144b ( dako , carpinteria , ca ) using the leica bond max staining platform ( leica microsystems , wetzlar , germany )  . 
for each tumor core , cd3 + and cd8 + t - cell populations were scored using the open access image analysis software qupath ( bankhead p , et al : sci rep 7 : 16878 , 2017 )  . 
measurements of tissue area and positive cell counts for each core provided cell density measurements , which are expressed as the number of positive cells per square millimeter of tissue . 
high and low cd3 / cd8 levels were calculated using the median level as cutoff . statistical analyses for kaplan - meier survival analysis and cox proportional hazards regression analysis , significance was assessed using log - rank and wald tests , respectively . 
cox proportional hazards regression analysis was used to assess overall survival at 5 years for adjuvant chemotherapy before and after adjustment for age , t stage , and sex ( stage ii and iii ) and age , sex , and stage ( stage ii and iii combined )  . 
 palbociclib in patients with pancreatic and biliary cancer with cdkn2a alterations : results from the targeted agent and proling utilization registry study tareq al baghdadi , md1 ; susan halabi , phd2 ; elizabeth garrett - mayer , phd3 ; pam k . 
schilsky , md3 purpose the targeted agent and proling utilization registry ( tapur ) study identies signals of antitumor activity of commercially available targeted agents in patients with advanced cancers that harbor genomic alterations known as drug targets . 
in this article , data from two cohorts of patients with pancreatic and biliary cancers with cdkn2a loss or mutation treated with palbociclib are reported . methods eligible patients age 12 years and older with advanced measurable or evaluable solid tumors are provided treatment according to protocol - specied genomic matching rules . 
secondary end points include safety , progression - free survival ( pfs ) , and overall survival ( os )  . results between july 2016 and november 2017 , 12 and 10 patients with pancreatic and biliary cancer , respectively , with cdkn2a loss or mutation were treated with palbociclib . 
despite recent advances , outcomes remain poor with a median overall survival ( os ) of less than 12 months in stage iv biliary and pancreatic cancers , 1 - 4 and new therapies are urgently needed . cyclin - dependent kinase ( cdk ) inhibitor 2a ( cdkn2a ) encodes p16ink4a , which plays an important role in cell - cycle regulation through inhibition of cdk4 / 6 . cdkn2a loss or mutation is found in a wide array of malignancies and may lead to increased cdk activity.5 in a report of the mutational landscape of advanced pancreatic cancer , 46.5% of tumors harbored alterations in cdkn2a.6 palbociclib is an orally available selective cdk inhibitor approved for the treatment of hormone receptorpositive , human epidermal growth factor receptor 2 ( her2 ) negative breast cancer in combination with endocrine therapy . the targeted agent and proling utilization registry ( tapur ) study is a prospective , phase ii , pragmatic basket trial designed to identify signals of antitumor activity of commercially available targeted agents in patients with advanced cancers that harbor genomic alterations known to be drug targets . 
this study examined whether patients with advanced biliary and pancreatic cancer with cdkn2a loss or mutation would be responsive to palbociclib , an oral cyclin - dependent kinase inhibitor . knowledge generated the results demonstrated that palbociclib monotherapy has no meaningful clinical activity in patients with cdkn2a mutated or deleted advanced pancreatic or biliary adenocarcinoma . relevance off - label prescribing of palbociclib for the treatment of patients with pancreatic and biliary tract cancers with cdkn2a loss or mutation is not recommended . 
these patients should be offered participation in clinical trials of new treatment approaches . methods trial design the rationale and study design have been reported previously in detail.7 patients with advanced cancer and no standard treatment options are eligible if they have a tumor that harbors a genomic alteration known to be a target of or to predict sensitivity to one of the available study drugs . the primary study end point is antitumor activity , dened as objective response ( or ) at 8 weeks or later or stable disease ( sd ) at 16 weeks or later from the time of enrollment . secondary end points include progression - free survival ( pfs ) , os , and toxicity . 
patients are matched to one of according to prespecied protocol matching rules on the basis of genomic testing performed by laboratories selected by clinical sites that have certication under the clinical laboratory improvement amendments and accreditation from the college of american pathologists . 
treating physicians may choose to consult with the tapur molecular tumor board for appropriate targeted treatment options where none or multiple treatment matches surface within the tapur matching rules or if the treating physician would like to propose a treatment match outside the matching rules . 
radiographic assessment and clinical evaluation for response evaluation are performed at 8 and 16 weeks after initiation of treatment ; then every 12 weeks while the patient remains in the study ; and then at the end of study treatment , where possible . 
patients are placed in multiple parallel cohorts dened by study drug , genomic alteration , and tumor type . each cohort has the same optimal simon two - stage design , with a total possible cohort size of 28 patients . 
the design requires 10 patients to be enrolled in a cohort in stage i and if fewer than two patients have or or sd of at least 16 weeks duration , the cohort is permanently closed . 
if at least seven patients in the total cohort have a response of at least 16 weeks duration , the null hypothesis is rejected , and it is concluded that a signal of activity has been identied . patients eligible patients are required to meet both protocoland drugspecic inclusion and exclusion criteria . 
protocol - specic eligibility criteria include advanced measurable or evaluable solid tumors per recist version 1.1 ; eastern cooperative oncology group ( ecog ) performance status ( ps ) of 0 , 1 , or 2 ; and a protocol - specied genomic target identied by a test performed in a laboratory that has clinical laboratory improvement amendments certication and college of american pathologists accreditation . 
 palbociclib in pancreatic / biliary cancer with cdkn2a alterations addition , to match to palbociclib , patients must have a cancer type other than breast and not have received food or drugs within 7 days before the start of study treatment that are known to be cyp3a4 inhibitors or inducers . 
detailed inclusion and exclusion criteria for tapur have been previously reported.7 patients treated with palbociclib received standard doses ( 125 mg orally daily for 21 days followed by 7 days off treatment to complete a 28 - day cycle ) until disease progression . 
all patients were tested for alterations using next - generation sequencing ( ngs ) platforms , with more than half the patients determined to have cdkn2a loss ( table 1 )  . patients in both cohorts continued treatment with palbociclib until disease progression , and no patients withdrew from the study . trial oversight the tapur study protocol was reviewed and approved by a central institutional review board and , in some cases , by the local institutional review board at participating sites . patients provide written consent before any screening activities or data collection . 
the tapur study was designed by asco staff with input from asco volunteer members and the participating pharmaceutical companies . the tapur data and safety monitoring board ( dsmb ) is an independent board appointed by asco and meets biannually to monitor the study and review the safety and efcacy ndings . 
in the case of the cohorts reported herein , the dsmb reviewed the safety and efcacy data and determined that both cohorts should permanently close at the end of stage i enrollment and that the ndings be released . study end points the primary end point is or , dened as complete or partial response at or before 16 weeks , or sd at 16 weeks or later as reported per recist version 1.1. 
 al baghdadi et al results patients with pancreatic cancer twelve patients with pancreatic cancer and cdkn2a loss or mutation treated with palbociclib were enrolled in the study across seven sites from july 25 , 2016 , to april 28 , 2017 . 
the median age was 62 years ( range , 52 to 70 years ) ; 67% of patients were male ; and 10 patients were white , one black , and one other . 
other common genomic alterations noted in this cohort were mutations in braf , fgfr1 , frs2 , kras , and tp53 , with kras mutations being the most commonly reported in 10 of 12 patients . two patients who were enrolled and received treatment were subsequently found to be ineligible because they had not met the eligibility requirement for a hemoglobin level of 9.0 g / dl or greater at the time of enrollment . 
of the 10 eligible patients , nine experienced progression at or before 8 weeks ; the remaining patient had tumor progression at 16 weeks . all patients were included in the analysis for safety , pfs , and os . 
no other grade 3 or higher adverse event or serious adverse event was observed as at least possibly related to palbociclib . patients with biliary cancer ten patients with biliary cancer with cdkn2a loss or mutation treated with palbociclib were enrolled in the study across six sites from august 9 , 2016 , to november 11 , 2017 . 
other genomic alterations noted in this cohort included arid1a , atm , braf , fgfr2 , fh , kras , nras , pik3ca , and vhl . all 10 patients experienced progression at or before 10 weeks . 
four patients experienced grade 3 or 4 adverse events of thrombocytopenia at least possibly related to palbociclib . discussion this phase ii study in patients with advanced pancreatic or biliary cancers with cdkn2a loss or mutation treated with single - agent palbociclib demonstrated no clinical activity . the toxicity is similar to previous reports of monotherapy with palbociclib . cdkn2a is a tumor suppressor gene frequently altered by mutations , deletions , and epigenetic silencing . 
of patients loss mutation loss cdkn2a / 2b homozygous loss p16ink4a a4_p11del , p16ink4a l16fs * 9 , loss exons 2 - 3 splice site 151 - 2a.g p16ink4a r58 * and p14arf p72l p16ink4a a36fs * 17 , p16ink4a n71fs * 49 and p14arf q85fs * 50 + splice site 151 - 1g.c truncation exon 2 foundationone mi - oncoseq foundationone foundationone foundationone foundationone foundationone foundationone abbreviations : mi - oncoseq , michigan oncology sequencing project ; ngs , next - generation sequencing . cdkn2a mutations / deletions occur frequently in pancreatic adenocarcinoma.11 moreover , alterations that abrogate the rb / p16 tumor suppressor pathway are seen in virtually all pancreatic carcinomas.12 cdkn2a mutations occur in a minority of cholangiocarcinomas and are associated with a poor prognosis.13 , 14 prior studies of multiple rb - positive tumors have shown that most are sensitive to some degree to cdk4 / 6 inhibition.15 - 18 preclinical studies assessing the impact of cdk4 / 6 inhibition on pancreatic cancer cell lines and xenograft models showed conicting data . 
for example , one study showed that palbociclib inhibited the growth of pancreatic cancer cell lines but resulted in upregulation of the expression of genes that promote invasion and metastasis.19 another showed that established pancreatic cell lines displayed a relatively weak response to palbociclib , but palbociclib had potent activity in patient - derived xenografts.20 palbociclib is approved for the treatment of patients with advanced hormone receptorpositive , her2 - negative breast cancer in combination with an aromatase inhibitor or fulvestrant.21 , 22 palbociclib showed promising activity in patients with liposarcoma23 and cdkn2a - mutated nonsmallcell lung cancer.24 however , palbociclib was not effective in lung cancer25 or unselected patients with squamous cell urothelial cancer.26 prior studies have suggested several mechanisms of resistance to cdk4 / 6 inhibitors in human cancer cell lines and xenograft models , including cdk4 amplication , rb loss , and cyclin e1 amplication.27 - 31 the potential for prior exposure to systemic chemotherapy to induce resistance to palbociclib through these or other mechanisms has not been explored but might have contributed to the lack of efcacy of palbociclib in this trial . 
it is conceivable , therefore , that the use of palbociclib alone or in combination earlier in the treatment course could be benecial . the association of cdkn2a mutations / deletions with clinical activity of cdk4 / 6 inhibitors is undetermined . 
in patients with hormone receptorpositive , her2 - negative breast cancer , cdkn2a mutations do not predict activity of either palbociclib or ribociclib.32 , 33 a report revealed that cdkn2a mutant cancers show only intermediate sensitivity to cdk4 / 6 inhibition with abemaciclib , whereas genetic events that activate d - type cyclins were associated with high sensitivity.30 the effects of combining other targeted agents with palbociclib in pancreatic adenocarcinoma cell lines have been explored . 
the addition of a mek inhibitor31 and a mammalian target of rapamycin inhibitor30 , 34 was synergistic . the latter may relate to metabolic reprogramming of pancreatic cancer cells by cdk4 / 6 inhibition , which results in increased oxidative phosphorylation , increased consumption of glucose and glutamine , and activation of mammalian target of rapamycin pathway.34 these and other novel combinations hopefully will allow successful treatment of pancreatic adenocarcinoma and other malignancies on the basis of a sound understanding of mechanisms that underlie cancer cell resistance . 
for more information about ascos conict of interest policy , please refer to or ascopubs.org / po / authorcenter . tareq al baghdadi stock and other ownership interests : array biopharma , astrazeneca , biogin , bristol - myers squibb , merck , portola pharmaceuticals , spectrum pharmaceuticals , tracon pharma , celgene , seattle genetics , sunesis pharmaceuticals honoraria : cardinal health , medscape consulting or advisory role : celgene , bristol - myers squibb , heron therapeutics travel , accommodations , expenses : cardinal health , celgene , bristolmyers squibb , heron therapeutics susan halabi consulting or advisory role : eisai , ferring pharmaceuticals vaibhav sahai consulting or advisory role : celgene , halozyme , newlink genetics , ipsen , incyte research funding : celgene ( inst ) , bristol - myers squibb ( inst ) , agios ( inst ) , incyte ( inst ) , clovis oncology ( inst ) , debiopharm group ( inst ) , fibrogen ( inst ) , halozyme ( inst ) , medimmune ( inst ) , rafael pharmaceuticals ( inst ) , ipsen ( inst ) ricardo h . 
alvarez employment : cancer treatment centers of america leadership : cancer treatment centers of america consulting or advisory role : eisai , puma biotechnology , r - pharma , pzer speakers bureau : eisai , pzer other relationship : eisai , puma biotechnology , pzer edward s . 
kim honoraria : astrazeneca , boehringer ingelheim , pzer , merck , takeda pharmaceuticals , roche , genentech consulting or advisory role : astrazeneca , boehringer ingelheim , pzer , merck , takeda pharmaceuticals , roche , genentech research funding : boehringer ingelheim , merck , ignyta , genentech , roche travel , accommodations , expenses : astrazeneca , boehringer ingelheim , takeda pharmaceuticals , genentech , roche , pzer , merck kathleen j . 
schilsky research funding : astrazeneca ( inst ) , bayer ag ( inst ) , bristol - myers squibb ( inst ) , genentech ( inst ) , roche ( inst ) , eli lilly ( inst ) , merck ( inst ) , pzer ( inst ) , boehringer ingelheim ( inst ) , varian ( inst ) no other potential conicts of interest were reported . references conroy t , desseigne f , ychou m , et al : folfirinox versus gemcitabine for metastatic pancreatic cancer . 
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n engl j med 362 : 1273 - 1281 , 2010 sahai v , catalano pj , zalupski mm , et al : nab - paclitaxel and gemcitabine as rst - line treatment of advanced or metastatic cholangiocarcinoma : a phase 2 clinical trial . 
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finn rs , dering j , conklin d , et al : pd 0332991 , a selective cyclin d kinase 4 / 6 inhibitor , preferentially inhibits proliferation of luminal estrogen receptor - positive human breast cancer cell lines in vitro . 
baughn lb , di liberto m , wu k , et al : a novel orally active small molecule potently induces g1 arrest in primary myeloma cells and prevents tumor growth by specic inhibition of cyclin - dependent kinase 4 / 6 . 
young rj , waldeck k , martin c , et al : loss of cdkn2a expression is a frequent event in primary invasive melanoma and correlates with sensitivity to the cdk4 / 6 inhibitor pd0332991 in melanoma cell lines . 
cristofanilli m , turner nc , bondarenko i , et al : fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment of hormone - receptor - positive , her2negative metastatic breast cancer that progressed on previous endocrine therapy ( paloma - 3 ) : final analysis of the multicentre , double - blind , phase 3 randomised controlled trial . 
dickson ma , schwartz gk , keohan ml , et al : progression - free survival among patients with well - differentiated or dedifferentiated liposarcoma treated with cdk4 inhibitor palbociclib : a phase 2 clinical trial . 
gopalan pk , pinder mc , chiappori a , et al : a phase ii clinical trial of the cdk 4 / 6 inhibitor palbociclib ( pd 0332991 ) in previously treated , advanced non - small cell lung cancer ( nsclc ) patients with inactivated cdkn2a . 
edelman mj , redman mw , albain ks , et al : a phase ii study of palbociclib ( p ) for previously treated cell cycle gene alteration positive patients ( pts ) with stage iv squamous cell lung cancer ( scc ) : lung - map sub - study swog s1400c . 
rose tl , chism dd , alva as , et al : phase ii trial of palbociclib in patients with metastatic urothelial cancer after failure of rst - line chemotherapy . 
herrera abreu mt , asghar u , elliot r , et al : pi3 kinase / mtor inhibition increases sensitivity of er positive breast cancers to cdk4 / 6 inhibition by blocking cell cycle re - entry driven by cyclind1 and inducing apoptosis . 
gong x , litcheld lm , webster y , et al : genomic aberrations that activate d - type cyclins are associated with enhanced sensitivity to the cdk4 and cdk6 31 . 
finn rs , crown jp , lang i , et al : the cyclin - dependent kinase 4 / 6 inhibitor palbociclib in combination with letrozole versus letrozole alone as rst - line treatment of oestrogen receptor - positive , her2 - negative , advanced breast cancer ( paloma - 1 / trio - 18 ) : a randomised phase 2 study . 
andre f , stemmer sm , campone m , et al : ribociclib + letrozole for rst - line treatment of hormone receptor - positive ( hr + ) , human epidermal growth factor receptor 2 - negative ( her2 - ) advanced breast cancer ( abc ) : efcacy by baseline tumor markers . 
 entrectinib in two pediatric patients with inflammatory myofibroblastic tumors harboring ros1 or alk gene fusions introduction inflammatory myofibroblastic tumor ( imt ) is a rare , indolent spindle cell tumor that typically affects children and young adults.1 , 2 imts occur predominantly in visceral soft tissue and are categorized as an intermediate malignancy because they have a potential for local recurrence but rarely progress to distant metastases.2 , 3 approximately 50% of imts harbor alk rearrangements , although gene fusions involving ros1 , ntrk3 , and pdgfr have also been identified.2 , 4 - 6 previously , the presence of alk gene fusions was typically identified using immunohistochemistry7 ; however , newer techniques such as hybridization capture - based next - generation sequencing ( ngs ) and ngs - based anchored multiplex polymerase chain reaction ( pcr ) testing can now be used to detect gene fusions.8 - 10 identifying patients with actionable gene fusions is important , given the availability of promising therapeutic strategies.2 , 4 surgical resection is the standard of care for patients with a solitary imt , 11 but patients with unresectable or advanced disease have limited treatment options . 
the current national comprehensive cancer network guidelines for soft tissue sarcoma recommend the use of alk inhibitors for patients with alk gene fusions12 ; however , there are no targeted agents approved specifically for use in fusion - positive imts . 
 entrectinib is an investigational , cns - active , potent , and selective inhibitor of trk , ros1 , and alk.8 , 13 , 14 in phase i trials , entrectinib demonstrated clinical efficacy in patients with different tumor types harboring ntrk , ros1 , or alk fusions , regardless of the fusion partner gene.8 a majority of the responses to entrectinib occurred in a rapid and durable manner , and some patients remained on study because they received clinical benefit , even after experiencing disease progression.8 here , we present two patients with fusion positive imts ( dctn1 - alk and tfg - ros1 ) who were enrolled in the ongoing startrk - ng phase i / ib trial ( nct02650401 : study of rxdx 101 in children with recurrent or refractory solid tumors and primary cns tumors , with or without trk , ros1 , or alk fusions ) and treated with entrectinib . 
further molecular testing using a hybrid capture - based targeted exome sequencing assay15 revealed a dctn1 - alk fusion ( fig 1a ) , which determined eligibility to enroll in the startrk - ng trial . 
 ( a ) the dctn1alk rearrangement identified in patient 1 is a deletion that results in the fusion of dctn1 exons 1 - 26 with alk exons 20 - 29 . 
 ( d ) axial t1 postcontrast image shows complete response of the tumor to entrectinib treatment ( no measurable tumor present , red arrow )  . the patient provided informed consent , and entrectinib was started in may 2017 at a dose of 550 mg / m2 taken orally once per day ( 1 cycle was 28 days )  . 
 at the time of this report , she continues daily entrectinib and has no limitations in academic or athletic activities . patient 2 is a 10 - year - old girl who presented with daily high - grade fevers , cough , weight loss , and changes in physical activity over a 2 - month period . 
hybrid capture - based targeted exome sequencing and anchored multiplex pcr as described above15 , 16 identified a tfg - ros1 gene fusion ( fig 2a ) , and she was subsequently enrolled in the startrk - ng trial . the patient provided informed consent and entrectinib was started in may 2017 at a dose of 550 mg / m2 orally once per day . 
in addition , by month 4 of treatment , the residual mass was primarily nonenhancing on contrast - enhancing magnetic resonance imaging , suggesting relative lack of activity ( fig 2b - 2c )  . 
while on treatment , she experienced constipation , mild bloating , nausea , and weight gashe also experienced nighttime urinary incontinence that was potentially related to treatment and improved with simple changes in her nighttime routine . 
both patients exhibited clinically significant responses to the investigational agent entrectinib , which was well tolerated , and the observed adverse effects were consistent with the reported safety profile of entrectinib.8 these cases are in agreement with previous reports demonstrating the clinical efficacy and tolerability of entrectinib in patients with solid tumors harboring ntrk , ros1 , or alk gene fusions , regardless of fusion partner.8 , 17 - 20 entrectinib seems to be well tolerated , as demonstrated in 203 patients treated at the recommended phase ii dose of 600 mg once per day.21 the most common treatment - related adverse events ( traes ) of any grade were dysgeusia ( 38% ) , fatigue ( 29% ) , constipation ( 23% ) , and dizziness ( 23% )  . 
in preclinical studies , entrectinib was a potent inhibitor of trk - driven neuroblastoma , 22 and it has demonstrated clinical activity in a 20 - month - old patient with infantile fibrosarcoma harboring an ntrk fusion.23 the benefit observed in the two patients reported here along with published data on the benefit of entrectinib in trk fusion - positive infantile fibrosarcoma highlight the potential of entrectinib in pediatric tumors harboring trk , ros1 , or alk fusions . 
the startrk - ng trial is currently enrolling pediatric patients with cancer , including primary cns tumors , neuroblastoma , and other non - neuroblastoma extracranial solid tumors harboring gene fusions in ntrk , ros1 , or alk , or harboring alk molecular alterations.23 these cases add to the growing body of evidence that demonstrates the diversity of gene fusion drivers in the formation of imt and underscore the importance of screening patients with imts for ntrk , ros1 , and alk gene fusions by using the best available diagnostic techniques . 
 the gene fusions present in these patients were identified by using a workflow that sequentially uses two different diagnostic platforms : a hybrid capture - based targeted exome sequencing assay ( msk - impact ) and anchored multiplex pcr ( archer fusionplex )  . 
 these cases also highlight the importance of treating patients with imts who harbor trk , ros1 , or alk fusions with drugs , such as entrectinib , that bind and inhibit the kinase domains of these fusion proteins . 
imt is often characterized by the presence of alk rearrangements ; however , additional gene fusions have also been identified in this rare cancer , including ros1 , ntrk3 , and pdgfr , 2 , 4 , 5 including a patient with etv6 - ntrk3 fusion - positive imt who is being considered for treatment with entrectinib.27 in patients with alk fusion positive imt , there have been varying efficacy results reported when patients are treated with alk inhibitors , including crizotinib , ceritinib , and alectinib.28 - 32 in addition , a recent report noted that a patient with imt harboring a tfg - ros1 fusion exhibited a poor response to crizotinib.6 there remains an unmet need in this patient population for safe and effective therapies that can treat patients across a wide range of gene fusion drivers . 
for more information about asco 's conflict of interest policy , please refer to or ascopubs.org / po / author - center . the potential benefit of entrectinib in that it inhibits select targeted kinases with high potency , allowing for the treatment of multiple distinct patient populations with one therapy . we have demonstrated clinically significant improvement in two patients with imts who harbor actionable gene fusions treated with entrectinib in the startrk - ng trial . 
basu no relationship to disclose acknowledgments the authors thank the patients who granted us consent to present their cases for the benefit of the scientific , medical , and patient communities worldwide and nick cianciola , of the lockwood group , for providing medical writing support funded by ignyta . accountable for all aspects of the work : all authors stock and other ownership interests : ignyta affiliations srikanth r . 
basu , memorial sloan kettering cancer center , new york , ny ; and edna chow - maneval , ignyta , san diego , ca . support supported by ignyta ; funded by national institutes of health national cancer institute grant no . 
antonescu cr , suurmeijer aj , zhang l , et al : molecular characterization of inflammatory myofibroblastic tumors with frequent alk and ros1 gene fusions and rare novel ret rearrangement . 
drilon a , siena s , ou si , et al : safety and antitumor activity of the multitargeted pan - trk , ros1 , and alk inhibitor entrectinib : combined results from two phase i trials ( alka - 372 - 001 and startrk - 1 )  . 
loke bn , lee vkm , sudhanshi j , et al : novel exon - exon breakpoint in cic - dux4 fusion sarcoma identified by anchored multiplex pcr ( archer fusionplex sarcoma panel )  . 
menichincheri m , ardini e , magnaghi p , et al : discovery of entrectinib : a new 3 - aminoindazole as a potent anaplastic lymphoma kinase ( alk ) , c - ros oncogene 1 kinase ( ros1 ) , and pantropomyosin receptor kinases ( pan - trks ) inhibitor . 
ardini e , menichincheri m , banfi p , et al : entrectinib , a pan - trk , ros1 , and alk inhibitor with activity in multiple molecularly defined cancer indications . 
cheng dt , mitchell tn , zehir a , et al : memorial sloan kettering - integrated mutation profiling of actionable cancer targets ( msk - impact ) : a hybridization capture - based next - generation sequencing clinical assay for solid tumor molecular oncology . 
green dc , deharvengt sj , de abreu fb , et al : use of anchored multiplex pcr enrichment for detection of gene fusions in solid tumors by next generation sequencing . 
drilon a , li g , dogan s , et al : what hides behind the masc : clinical response and acquired resistance to entrectinib after etv6 - ntrk3 identification in a mammary analogue secretory carcinoma ( masc )  . 
sartore - bianchi a , ardini e , bosotti r , et al : sensitivity to entrectinib associated with a novel lmna - ntrk1 gene fusion in metastatic colorectal cancer . 
ahn mj , cho bc , siena s , et al : entrectinib in patients with locally advanced or metastatic ros1 fusion - positive non - small cell lung cancer ( nsclc )  . 
rangaraju s , li g , christiansen j , et al : pediatric phase 1 / 1b study of entrectinib in patients with primary brain tumors , neuroblastoma , and ntrk , ros1 , or alk fusions . 
vendrell ja , taviaux s , bganton b , et al : detection of known and novel alk fusion transcripts in lung cancer patients using next - generation sequencing approaches . 
subbiah v , mcmahon c , patel s , et al : stump unstumped : anti - tumor response to anaplastic lymphoma kinase ( alk ) inhibitor based targeted therapy in uterine inflammatory myofibroblastic tumor with myxoid features harboring dctn1 - alk fusion . 
ono a , murakami h , serizawa m , et al : drastic initial response and subsequent response to two alk inhibitors in a patient with a highly aggressive alk - rearranged inflammatory myofibroblastic tumor arising in the pleural cavity . 
mansfield as , murphy sj , harris fr , et al : chromoplectic tpm3 - alk rearrangement in a patient with inflammatory myofibroblastic tumor who responded to ceritinib after progression on crizotinib . 
 la radiologia medica ( 2019 ) 124 : 408413 neuroradiology singlecenter experience using the3max or4max reperfusion catheter forthetreatment ofacute ischemic stroke withdistal arterial occlusions inpatients noteligible forintravenous fibrinolysis danielegiusepperomano1 ignaziomariavallone1 paolagennari1 maurizioacampa2 giuseppemartini2 sandrabracco1 tommasocasseri1 saraleonini1 rossanatassi2 samuelecioni1 received : 10 september 2018 / accepted : 4 december 2018 / published online : 13 december 2018 italian society of medical radiology 2018 abstract background in acute stroke , distal cerebrovascular occlusions can be linked to severe clinical symptoms , and treatment by mechanical thrombectomy may have an important clinical impact . 
when intravenous fibrinolytic therapy is firmly contraindicated , it remains the only treatment option . methods a total of 42 patients with isolated distal arterial occlusions and absolute contraindication for intravenous fibrinolytic therapy were retrospectively included . 
in a cohort of patients with absolute contraindication for intravenous fibrinolytic therapy , a significant percentage achieved good revascularization . keywords acute stroke distal occlusions mechanical thrombectomy introduction in 2015 , five randomized trials investigated the efficacy of modern endovascular therapies for stroke [ 15 ]  . 
they provided strong evidence to support the use of mechanical thrombectomy when initiated within 6h from stroke onset , prompting worldwide changes in the guidelines for management of acute stroke due to large - vessel occlusion . * daniele giuseppe romano dromano80@gmail.com 1 unit ofneuroimaging andneurointervention ( nint ) , department ofneurological andsensorineural sciences , azienda ospedaliera universitaria senese , policlinico santa maria alle scotte , viale m . 
bracci 2 , siena , italy 2 stroke unit , department ofneurological andsensorineural sciences , azienda ospedaliera universitaria senese , policlinico santa maria alle scotte , siena , italy these trials used a variety of treatment approaches , including the mandatory use of intravenous thrombolysis before the initiation of endovascular therapy . consequently , american heart association ( aha ) / american stroke association ( asa ) published its scientific rationale for the inclusion and exclusion criteria for intravenous alteplase in acute ischemic stroke [ 6 ]  . 
even if some of the original exclusion criteria have proven to be unnecessarily restrictive in clinical practice , absolute contraindications remain . the occlusion of smaller arteries , such as the m2 or m3 segments of the middle cerebral artery ( mca ) , a2 segments of the anterior cerebral artery ( aca ) or the posterior cerebral artery ( pca ) , sometimes causes ischemic strokes with pronounced clinical impact on the patient [ 7 ]  . the updated aha 2018 stroke guidelines [ 8 ] specifically talk about distal occlusions . 
 the number of attempts was guided by tici score after aspiration . before treatment , informed consent was obtained from technical success was defined as recanalization of the the patient if conscious or a legal representative . target vessel according to tici score 2b . for each patient , we considered age , sex , risk factors , baseline mrs , nihss and aspect score ( or early signs of ischemia in vascular territory of a2 or p1p2 ) , time from symptoms onset to groin puncture , time from groin puncture to revascularization , type of endovascular procedure ( adapt alone vs stent retriever ) and device used , tici score at the end of the procedure , kind of anesthesia , aspect score at 24h or signs of ischemia in vascular territory of a2 or p1 , complications , nihss at 24h and 30days , rankin score ( mrs ) at 90 - days follow - up . all patients underwent unenhanced ct to exclude hemorrhage and ct angiography to detect cerebrovascular occlusions . 
in case of uncertain onset of the symptoms ( i.e. , wake - up stroke ) , patients were considered eligible for treatment when salvageable brain parenchyma was depicted by perfusion ct mismatch . 
all patients were evaluated by a stroke - dedicated neurologist . two blinded neuroradiologists with 8 and 23years of experience in interventional neurovascular procedures ( dgr and sb ) reviewed all imaging data and assessed aspect score from the baseline ct scan and the tici scores after intervention . 
they also reviewed the imaging data for complications of emboli to new territory , vessel dissection , vasospasm , vessel perforation and ich . statistical analysis continuous parameters were compared using the students t test for normally distributed data or the mannwhitney u test for not normally or ordinally distributed data . 
a p value of 0.05% or lower was considered to be statistically significant . results we retrospectively included 42 consecutive patients with acute ischemic stroke from distal arterial occlusions and absolute contraindication to fibrinolytic therapy for the following reasons : current use of anticoagulant with inr > 1.7 or pt > 15s ( n = 13 ) , platelet count < 100 000 / mm3 [ 1 ] , after 4.5h time window ( n = 28 )  . patients with wake - up stroke were 11 / 42 . all patients were treated in our hospital with thromboaspiration as first intention using the penumbra reperfusion catheter . target vessel occlusions were : m2 ( n = 46 ) , p1 ( n = 4 ) , a2 ( n = 2 )  . 1 3 la radiologia medica ( 2019 ) 124 : 408413 410 fig . 
1 male patient , 72 y.o with right m2 parietal branch occlusion ( a , b ) , ace 64 reperfusion catheter was advanced over a 3max aspiration catheter into the right mca to the site of occlusion and left at the face of the thrombus ( c , d ) , aspiration was applied resulting in successful revascularization 4h after symptom onset ( e , f ) 57.1% were female ( n = 24 )  . 
 [ 18 ] achieved substantially the same clinical outcome in the treatment of m2 occlusions using stent retriever versus thromboaspiration , with slightly less complications in the last . notably aspiration catheters offer an alternative strategy for achieving thrombus removal by applying suction at the proximal portion of the occlusion and drawing it into the catheter lumen . 
the smaller percentage of successful outcome was explained by the inclusion criteria ( patients with absolute contraindication for intravenous fibrinolytic therapy ) and clinical characteristics of our population ( moderate to severe stroke with a mean nihss score of 18 )  . the duration of the endovascular treatment ( time from groin puncture to reperfusion ) was significantly lower in patients who underwent adapt alone because a stent retriever was used in case of failure of adapt . 
nonetheless , switching to other techniques might provide better angiographic outcomes in cases with unsuccessful reperfusion after a few attempts with the adapt technique . general anesthesia ( used in 71.4% of cases ) , keeping the patient motionless , allows a safer procedure when dealing with a small intracranial vessel occlusion and permits the operator to concentrate on the procedure . procedural or anesthetic complications did not occur in the present study . the risk profile for symptomatic bleeding was similar to that in recently reported controlled clinical trials [ 15 ]  . main limitations of this paper are the lack of randomization and the fact that it is a single - center , retrospective and observational study over a long period . conclusions in a cohort of patients with absolute contraindication for intravenous fibrinolytic therapy , a significant percentage achieved good revascularization . direct thromboaspiration appears a safe technique in acute isolated distal arterial occlusions . 
fifty - two patients ( study group ) underwent 256 - mdct low - dose ccta ( 80kv ; automated - mas ; 60ml of cm , 350 mgl / ml ) with prospective ecg - triggering acquisition and imr . 
a control group of 46 patients underwent 256 - mdct standard prospective ecg - gated protocol ( 100kv ; automated - mas ; 70ml of cm , 400 mgl / ml ; idose4 )  . 
radiation dose exposure was quantified as dlp , ctdivol and ed . results mean values of mas were significantly lower for imr - ccta ( 167 62 mas ) compared to idose - ccta ( 278 55 mas ) , p < 0.001. 
therefore , according to alara principle , low - dose coronary ct angiography has recently been performed in several studies [ 11 , 12 ] , thanks to the use of wide detector panels [ 13 , 14 ] and due to a reduction of tube - current and / or tube - voltage setting . 
for this reason , hybrid - iterative reconstruction ( hir ) algorithm for ct , such as asir ( ge healthcare ) , aidr 3d ( toshiba medical ) and idose ( philips healthcare ) , was introduced vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 350359 in clinical practice in the last years , in order to reduce the image noise due to the use of low - dose protocol with filtered back projection ( fbp ) reconstruction technique . 
unfortunately , some artifacts and a certain amount of image noise was still present in hir images , so the new model - based iterative reconstruction algorithm ( i.e. , imr , philips healthcare ; veo , ge healthcare ; admire , siemens ; first , toshiba medical , canon ) was introduced in clinical practice , trying to solve these problems . 
this new reconstruction technique can effectively control the image noise while maximizing the spatial resolution with a significant radiation dose sparing than those obtained with fbp and hybrid - iterative reconstruction algorithm [ 17 ]  . one of the concerns of the model - based iterative reconstruction algorithm is the time spend to generate the final images ; but , thanks to new faster computing hardware and algorithmic optimization , nowadays the reconstruction time for imr is of about 2min for cardiac ct ( about 200 images / minute ) [ 17 ] , making imr applicable also in clinical practice . moreover , this reconstruction technique combined to low - dose protocol leads to lower contrast medium volume use thanks to higher attenuation levels of iodinated contrast medium at low kv - setting due to greater photoelectric effect and decreased compton scattering [ 12 , 1820 ]  . 
in order to obtain an optimal intra - luminal contrast enhancement , the start of scanning was individually obtained for each patient by using bolustracking technique ( bt ) , with a trigger level of 120 hu and a delay time between 5 and 8s . 
the trigger area was manually placed at the proximal ascending aorta , in order to reduce the time needed for the ct bed to reach the starting level of acquisition . 
in all 52 patients of this group , low volume ( 60ml ) of intermediate iodine concentration contrast agent ( xenetix 350 , 350 mgl / ml , guerbet aulnay , france ) was administered , with a flow rate of 4.5ml / s followed by saline flushing ( volume 35ml ; flow rate 4.5ml / s ) , for a total iodine amount of 21g . all the raw data were reconstructed with the new modelbased iterative reconstruction algorithm ( imr level 1 ) and standard filter cardiac routine , as suggested from the vendor . control group protocol control group patients were evaluated on a different 256mdct scanner ( brilliance ict , philips medical systems , best , the netherlands ) , with a standard 100kv protocol and automated tube - current modulation ( range of 200800 mas )  . 
the other scan parameters were : collimation 128 0.625 ; rotation time 0.33s ; thickness 1mm ; increment 1mm ; fov 350mm ; matrix 512 512 ( table1 )  . in all patients of the control group , we used a total of 70ml of a high iodine concentration cm ( iomeron 400 , 400 mgl / ml , bracco imaging , italy ) at a flow rate of 4.5ml / s , followed by saline flushing ( 50ml ; flow rate 4.5ml / s ) , for a total iodine amount of 28g . the dual - scout image was used to optimize the acquisition volume and the same prospective ecg - gating protocol of the study group ( step & shoot ) was used to acquire the cardiac examination . the raw data were reconstructed with hybrid - iterative reconstruction algorithm ( idose4 , level 4 ) and standard filter cardiac routine was applied . radiation dose quantification to analyze the radiation dose exposure , the ct dose - length product ( dlp , mgy cm ) and the ct dose index ( ctdivol , mgy ) were recorded for all scans . 
we also calculated the effective radiation dose ( ed ) of coronary cta , using the known formula ed = k dlp , where dlp ( mgy m ) is the dose - length product and k is the region - specific normalized effective dose ( msv / mgy1cm1 ) , derived from the paper by deak etal . 
 [ 28 ] ; the region - specific conversion coefficients of k = 0.0146msv / mgy1cm1 were used for both the 80 - kv and 100 - kv protocols [ 28 ]  . quantitative image evaluation images were anonymized and then processed on a dedicated workstation ( intellispace portal , philips ) in order to produce multiplanar reconstructions , maximum intensity projections ( mip ) and volume rendering ( vr ) images . 
final images were analyzed by two radiologists in consensus for the quantitative evaluation . vessel contrast enhancement ( mean attenuation value , hu ) was measured in the axial native images , by manually placing a circular region of interest ( roi ) in the center of vascular lumen in the left ventricle , ascending aorta , in the proximal and distal segment of left anterior descendant ( lad ) , left circumflex ( lcx ) and right coronary artery ( rca )  . 
the rois size was as large as possible depending on artery size , avoiding wall calcifications and atherosclerotic plaque , and in order not to be affected by pixel variability . we also compared the image noise of two groups , determined as the standard deviation ( sd ) of the attenuation value in each proximal coronary segment . 
moreover , we evaluated the contrast resolution by calculating the contrastto - noise ratio ( cnr ) using the formula : cnr = huahub where hua is the mean attenuation of the proximal tract of rca , hub and sdb are the mean attenuation and standard deviation of the adjacent adipose tissue , as reported in the paper by park etal . 
for subjective evaluation , the overall diagnostic quality of the images of ascending aorta and the previously described coronary arteries ( lad , lcx and rca ) were evaluated using a 4 - points subjective scale [ 30 ] : 4 as excellent ( minimal image noise and artifacts with excellent visualization of boundary of each coronary segment ) ; 3 as good ( some image noise , good visualization of the boundary , minor artifacts especially in small middle and distal coronary segments and good visualization of proximal tract ) ; 2 as acceptable ( delineation of the boundary equivocal but within an acceptable range , minor artifacts and sufficient visualization of proximal and middle tract ) ; 1 as low ( major artifacts , unsatisfactory delineation of the boundary or poor visualization of coronary arteries at any levels )  . moreover , subjective image noise , image texture and image sharpness were evaluated by the two radiologists using a similar 4 - point scale . 
for the evaluation of the image texture and noise : 4 was excellent ( noise and unnatural texture not present , with high diagnostic images ) ; 3 was good ( image noise and unnatural texture present but do not interfere with depiction of adjacent structures ) ; 2 was acceptable ( image noise and unnatural image texture that interfere with depiction of adjacent structures ) ; 1 was low ( image noise and unnatural texture unacceptable ; low diagnostic images )  . 
image sharpness was graded by evaluating ascending aortic wall : 4 excellent , the best sharp image ; 3 good , better than average ; 2 as acceptable but poorer than average ; 1 as low because of a blurry image [ 7 ]  . statistical analysis all continuous variables were expressed as mean standard deviation ( sd ) and compared with t - student test and mannwhitney u test , as appropriate . 
categorical variables are expressed as number and percentage and compared with 2 test , using bonferroni correction . the agreement between the two observers in the subjective image evaluation was measured with the kappa statistic , where a value of 0 = no agreement ; > 0 and 0.20 = poor ; 0.210.40 = fair ; 0.410.60 = moderate ; 0.610.80 = substantial ; and 0.810.99 = almost perfect agreement . all statistical analyses were performed with commercially available software ( med calc , med calc software 14.8.1 , mariakerke , belgium )  . 
a value of p < 0.05 was considered to be a statistically significant difference . table 2 comparison of patients characteristics of the study and control groups data / protocol study group control group p value no . 
in the last 10years , the patients radiation burden concerns led to the optimization of ccta protocol with the introduction of new techniques , such as the step and shoot acquisition , and by modifying acquisition parameters settings , as lower tubecurrent and mas modulation . 
c , d curved and straight reconstruction of right coronary artery with a good visualization of artery wall due to high snr and cnr leading to high spatial resolution 1 3 356 la radiologia medica ( 2019 ) 124 : 350359 fig . 
a , b shows the overall image quality between the idose4 image ( a ) and imr ( b ) , with lower image noise and higher spatial resolution in the image on the right . 
on the contrary , the attenuation value of the three coronary arteries was better in the imr studies compared to idose4 ( p < 0.05 ) , obtaining a mean attenuation value in coronary lumen measured in all patients above to the minimum value of 300 hu , as suggested in literature [ 32 , 33 ]  . 
the overall subjective image quality was better for imr - group compared to idose one for both the readers , without any statistical differences ( p = 0.23 and p = 0.47 for reader 1 and reader 2 , respectively )  . 
also for the other qualitative evaluations , the scores were better for study group compared to control one , without any difference ( p > 0.05 ) except for the texture evaluation of reader 1 , who assigned higher rate to imr - images , as shown in table5 . these results demonstrated that low - dose ccta with imr reconstruction provides comparable diagnostic images compared to standard dose examination . 
moreover , the use of reduced kv - setting , increasing the image noise in the raw data , avoids the plastic appearance of mbir into the final images , previously described in literature by barras etal . 
moreover , we used only the first level ( imr1 ) of the model - based iterative reconstruction ( imr 13 ) , suggested from the vendor and selected as standard by our institution . 
thirdly , the patients in our series had a bmi 30kg / m2 , and therefore , further studies are needed to test the lowkv protocol combined to imr in patients with higher bmi . 
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park ch , lee j , oh c , han kh , kim th ( 2015 ) the feasibility of sub - millisievert coronary ct angiography with low tube voltage , prospective ecg gating , and a knowledge - based iterative model reconstruction algorithint j cardiovasc imaging 31 ( 2 ) : 197203 . 
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therefore , dce - mri parameters can predict tumor aggressiveness and crt efficacy , playing a role as imaging biomarkers in patients with larc . keywords locally advanced rectal cancer magnetic resonance imaging imaging biomarkers neoadjuvant therapy patient outcome * andrea laghi andrea.laghi@uniroma1.it introduction 1 department ofsurgical andmedical sciences andtranslational medicine , sapienza university ofrome , radiology unit santandrea university hospital , via di grottarossa , 1035 - 1039 , 00189rome , italy 2 department ofradiological sciences , oncology andpathology , uoc radiologia , policlinico umberto i hospital , sapienza university ofrome , viale regina elena , 324 , 00161rome , italy 3 department ofradiological sciences , oncology andpathology , uoc radioterapia , policlinico umberto i hospital , sapienza university ofrome , viale regina elena , 324 , 00161rome , italy 4 department ofradiological sciences , oncology andpathology , uoc anatomia - patologica , policlinico umberto i hospital , sapienza university ofrome , viale regina elena , 324 , 00161rome , italy neoadjuvant chemoradiotherapy ( crt ) is the treatment of choice in patients with locally advanced rectal cancer ( larc ) [ 13 ]  . 
thus , a reliable diagnostic method able to stratify larc patients could be beneficial to reduce crt - related toxicity and select the proper treatment strategy for each patient . magnetic resonance imaging ( mri ) represents the noninvasive reference standard in the diagnosis of larc due to its excellent contrast resolution [ 5 , 6 ]  . 
however , conventional mri only relies on morphological parameters such as changes in tumor size , volume , and signal intensity [ 7 ] , resulting inadequate in predicting response to crt [ 8 ]  . 
due to their correlation with tumor aggressiveness [ 11 ] , dce - mri parameters quantification could represent an appealing strategy in management of patients with larc , helping in the selection of the most appropriate treatment for each patient and eventually resulting in a better prognosis [ 12 ]  . in the last decades , dce - mri parameters for larc have been widely investigated , with particular interest in the assessment of tumor response after crt and patient prognosis prediction [ 1318 ]  . 
however , inconsistent results have been returned among different investigations , reporting either good efficacy [ 15 , 19 ] of dce - mri in predicting response to crt or opposite results [ 14 , 17 ]  . hence , the aim of our study was to correlate dce - mri parameters to tumor grading and to assess their reliability in predicting pathological complete response ( pcr ) before neoadjuvant crt in patients with larc . materials andmethods patients characteristics this retrospective study was approved by the institutional review board of ( blinded ) with a waiver for informed consent . 
the study included data from consecutive patients with histologically proven larc at stage ii ( ct34 , n0 , m0 ) or stage iii ( ct1 - 4 , n + , m0 ) who had undergone clinical assessment by dce - mri before and after crt between august 2015 and february 2016 . 
a routine clinical imaging protocol wasacquired , which included high - resolution t2 - weighted fast recovery fast - spin echo ( 2d frfse ) sequencewith the following parameters : tr : 20864172ms ; te : 11.4122.3ms ; acceleration factor ( nex ) : 2 ; slice thickness : 4mm ; matrix : 512 512 . 
dedicated axial oblique and coronal oblique planes wereobtained , respectively , orthogonal and parallel to the long axis of the rectuaxial dwi images were obtained using a single - shot echo - planar imaging sequence with spectral adiabatic inversion recovery fat saturation technique ( tr : 4400ms ; te : 81.4ms ; nex , 2 ; slice thickness : 4mm ; matrix : 256 256 ; b values : 0 , 200 , 800s / mm2 )  . for the specific purpose of our study , dce - mri was added to the standard rectal cancer mri clinical protocol . 
 dce images wereobtained with a 3d gradient recalled echo ( gre ; tr : 14.05 ms ; te : 3.66 ms ; nex , 1 ; slice thickness : 3 mm ; matrix : 320 320 ) sequence which started simultaneous to the intravenous administration of gadolinium chelate ( gadobenate dimeglumine , multihance ; bracco imaging ; 0.1mmol / kg ) at 2ml / s followed by 15ml of saline flush at the same flow rate . 
the entire volume was acquired in 1s , and the acquisition was repeated over a scan time of 60s using a thin collimation ( 2mm ) in order to obtain an accurate evaluation of the contrast media kinetics in the tumor tissue during all vascular phases . neoadjuvant therapy chemoradiotherapy was administered following the standard of care in our institution [ 20 ]  . 
an additional dose of 5.49gy was administered to the tumor volume in 35days ( 615 mv energy photons )  . chemotherapy was administered through a central venous access as follows : 5 or 6 cycles of oxaliplatin ( 2 - h infusion 50mg / m2 ) on the first day of each week of radiotherapy followed by five daily continuous infusions of 5 - fu 200mg / m2 / die . 
toxicity was evaluated according to nci - ctc version 3.0dsds. table 1 dce - mri exclusion criteria incomplete dce - mri acquisition or histopathological analysis contraindication to the use of neoadjuvant therapy or surgical treatment suspension of neoadjuvant combination chemotherapy and radiation treatment prior to surgery treatment with concurrent and experimental drugs , or participation in another clinical trial technical problems in post - processing of dce - mri images diagnosis of mucinous rectal adenocarcinoma 1 3 la radiologia medica ( 2019 ) 124 : 331338 surgical technique during a time frame of 6 to 8weeks after the completion of crt , all patients underwent total mesorectal excision [ 21 ] performed by experienced colorectal surgeons , each of them with at least 10years of experience in this technique . histopathological assessment a single gastrointestinal pathologist with 10years of experience in rectal cancer performed all of the histopathology analyses , which were carried out as assessments of the basic histopathology of the primary tumor ( type and grade of the tumor ) samples obtained as a biopsy specimen taken before the crt treatment . 
all analyses comprised evaluation of surgical margins and other histological features , including t stage and n stage according to the 7th edition of the american joint committee on cancer [ 22 ]  . for the specific purpose of our study , patients were divided into two groups : complete responders ( cr ) and noncomplete responder ( ncr )  . 
cr group includedpatients who showed downstaging after crt and whose surgical intervention was classified as pathological complete response ( ypt0n0 ) , hereafter indicated as pcr . perfusion imaging mri_1 and mri_2 images were processed with a dedicated software ( olea sphere , v2.3 ; olea medical , la ciotat , france ) and were analyzed using the extended tofts model [ 23 ] to evaluate quantitative perfusion parameters . 
two board certified radiologists with 8 and 5years of experience in rectal mridrew in consensus the region - of - interests ( roi ) on perfusion maps around the central tumor ( carefully avoiding necrosis or cystic areas ) and the external iliac artery . 
other additional rois were placed in the gluteus maximus and in the healthy intestinal wall to normalize signal intensities as reported in other studies to overcome the issue of high range of absolute perfusion values [ 2426 ]  . 
for each roi , the software provided values for ktrans ( plasma - toextravascular volume transfer ) , kep ( extravascular - to - plasma volume transfer constant ) , ve ( extravascular extracellular volume fraction per unit of tissue volume ) , vp ( plasma volume ) , wash - in ( velocity of enhancement ) , wash - out ( velocity of enhancement loss ) , curve - washout ( wash - out slope ) , peak enhancement , peak ( maximal concentration of contrast agent ) , and tme ( time - to - maximal enhancement )  . statistical analysis test was used to assess normality of data distribution . 
tumor roi values were normalized to the healthy intestinal wall and maximum gluteus muscle . spearmans test was used to assess correlation between dce - mri parameters and tumor grading , and tumor pathological status related to crt . 
comparison between mri_1 values and mri_2 values , cr patients and ncr patients , and g3 , g2 , and g1 tumors was carried out using either mannwhitney u test ( if data presented a nonparametric distribution ) or unpaired t test ( if data presented a parametric distribution )  . 
discriminatory power of each parameter to predict tumor grading or cr was assessed by receiver operating characteristic ( roc ) curve analysis and the calculated area under the curve and the corresponding p value . 
p value of < 0.05 was considered statistically significant . results patient characteristics from an initial cohort of 51 patients , 11 were excluded due to incomplete mri examination ( n = 1 ) , suspension of crt prior to surgery ( n = 5 ) , and participation in other clinical trials ( n = 5 )  . 
 wash - out returned the largest area under the roc curve ( = 0.801 ; [ 95% ic 0.7630.851 ] ) ; a wash - out value of 0.79 provided a sensitivity of 80% and a specificity of 70% in differentiating g3g2 from g1 larc . 
in particular , 17 patients ( 68% ) showed partial response , 5 patients ( 20% ) showed stable disease , and 3 patients ( 15% ) were classified as non - responders . 
these perfusion parameters showed a moderate discriminatory power ( area under the curve : 0.709 [ 95% ic 0.6720.737 ] for ktrans ; 0.71 [ 95% ic 0.6850.749 ] for tme ; and 0.68 [ 95% ic 0.6500.716 ] for auc , respectively )  . 
we documented the correlation of some dce - mri parameters with tumor grading , their changes during crt and their potential to distinguish , at baseline examination , patients with larc that will achieve pcr from those non - responsive to crt . it has been reported that the degree of angiogenesis in a tumor correlates with tumor grading and aggressiveness , which in turn are related to prognosis and response to treatment [ 27 , 28 ]  . 
more mature vessels can permit a higher exchange between the blood bed and the interstitial space , with more effective passage and permeability of different substances , including mri contrast media . 
on the contrary , poorly differentiated tumors consist of disorganized and leaky vessels , with ineffective exchange and inefficient delivery of substances , such as oxygen which may contribute to tumor hypoxia [ 29 ]  . we demonstrated that wash - out and kep are two perfusion parameters significantly correlated with tumor grading . 
in detail , our results indicate that wash - out values are positively correlated with tumor grade resulting higher in g3 - tumors , while kep values show a negative correlation with cancer grading resulting higher in g1 - tumors . 
kep , defined as the ratio between ktrans and ve , is the rate constant of contrast agent escaped from the extracellular extravascular space into plasma compartment [ 30 ]  . 
higher kep in well - differentiated tumors means that there is an increased return flow from the tumor interstitial space to neo - vessels and this reflects a more permeable neo - vasculature allowing better exchange between interstitial space and vessels . 
on the contrary , poorly differentiated tumors presented a lower kep , reflecting a lower vessel permeability and a lower capability of the tumor to exchange substances with the vascular network . an inverse correlation between kep and tumor grade has also been found by yeo etal . 
 [ 11 ] , which investigated quantitative perfusion parameters in 46 patients with rectal cancer , reporting higher kep values in well - differentiated tumors . the analysis of perfusion parameters changes between baseline and post - crt examination showed a significant ve increase . 
 [ 32 ] documented higher ve associated with tumor regression in patients with cervical cancer during crt , and with liver metastases shrinkage from rectal cancer during chemotherapy , respectively . 
6 receiver operating characteristic ( roc ) curves of tme , auc , and ktrans patient management by the implementation of wait - andwatchstrategy [ 35 ] , ultimately reducing the number ofsurgical interventions and their related risks . 
our results indicate ktrans as a reliable indicator of complete response to crt : at the baseline mri examination , we demonstrated higher ktrans in those patients lately identified as pcr . 
ktrans has been widely investigated as a new tumor biomarker , and our finding of a higher ktrans in cr group is in accordance with other investigations [ 4 , 19 , 34 ]  . 
 first , our sample size was relatively small and further investigations with larger sample sizes are advisable to confirm our results and toobtain robust data on overall survival and disease - free survival . 
third , despite a consensus session with two expert readers , the manual roi placement is less reproducible than an automated placement , which would be more appropriate to guarantee standardization of measurements . conclusion mri - derived ktrans , tme , and auc measured before crt are reliable in discriminating cr and ncr patients with larc , while kep and wash - out significantly correlate with tumor grading . 
we evaluated the relationship between maximum and mean standardized uptake values ( suvmax and suvmean , respectively ) , metabolic tumor volume and total lesion glycolysis ( tlg ) of primary tumor and cervical lymph nodes with disease - free survival ( dfs ) and overall survival ( os )  . 
the corresponding planning target volume consisting of gtvs plus asymmetric margins of 0.51.5 cm to account for microscopic diseases and setup uncertainties was planned to receive a total dose of 70gy with conventional or moderately accelerated fractionation ( 22.12gy per fraction , 5 fractions per week )  . 
radiotherapy ( rt ) was delivered by relying on a conventional static fields technique ( conventional imrt ) or volumetric modulated arc therapy ( vmat ) with sequential or simultaneous integrated boost approaches . chemotherapy patients staged i and iia received exclusive rt , whereas patients with stage iibiiiiv received concomitant platinum - based cht . 
a boundary box to autocontour and 1 3 416 la radiologia medica ( 2019 ) 124 : 414421 segment the region of interest was placed over the image , reviewed and adjusted to ensure that the entire lesion was included in all three sectional pet images ( axial , coronal , sagittal )  . 
these vois were segmented automatically using an iterative adaptive algorithm to detect the threshold level that separated the target volume from the background tissue by weighting the maximum and mean standardized uptake value ( suvmax and suvmean ) within the target volume with a weighting factor . 
this weighting factor was automatically set at 0.5 [ 16 , 17 ]  . using the generated voi , suvmax , suvmean and metabolic tumor volume ( mtv ) were automatically recorded . 
 total lesions glycolysis ( tlg ) was calculated multiplying suvmean by mtv . in patients with multiple hypermetabolic lymph nodes , the metabolic parameters of each node were summed . followup after rt completion , patients received follow - up examinations including clinical exams and mri at predefined intervals , typically every 36months for the first 3years and annually thereafter . 
pearson correlation coefficients ( ) were determined to test the correlation between pet and clinical and biomarker features . overall survival ( os ) and disease - free survival ( dfs ) were evaluated starting from the first day of treatment ( cht or rt , whichever came first ) to the day of death or recurrence . 
maximal chi - square method was used to determine the optimal cutoff values for pet parameters and for the following factors : age , t stage , n stage , overall stage and gtvs . 
additionally , tlg - t had the highest hr for os . 1 3 la radiologia medica ( 2019 ) 124 : 414421 table 1 general characteristics of population ( n = 49pts ) table 2 distributions for pet and clinical parameters characteristics no . 
although limited to a small retrospective cohort of patients , the present study is the most comprehensive to date performed in a low - incidence area . at baseline , no correlation was discovered between pet and clinical , biological and therapeutic parameters . 
specifically , the correlation between pet indicators and clinical stage is a controversial issue in literature [ 1820 ]  . although some differences can be found in methods of t and n staging among ours and other series , we can bolster the idea that tnm staging and pet could detect different information . 
moreover , the fact we did not find any correlation between pet parameters and gtv strengthens the 1 3 418 la radiologia medica ( 2019 ) 124 : 414421 fig . 
ned no evidence of disease , dod dead of disease supposition that tumor volume cannot be related to its metabolic activity in npc . metabolic information provided by pet / ct imaging was investigated into target volume delineation by many authors . 
we 1 3 420 la radiologia medica ( 2019 ) 124 : 414421 think that additional ad hoc studies are necessary to clarify the use of pet / ct in this setting . the identification of prognostic factors plays an important role for cancer treatment stratification and improvement of clinical outcome in npc patients . two recent meta - analyses on the prognostic role of 18ffdg pet / ct in npc patients found that suvmax , tlg and mtv of primary tumor predict the risk of failure or death , notwithstanding the differences in method adopted in the literature taken into consideration [ 26 , 27 ]  . in our study , we showed that suvmax , suvmean and tlg of primary tumor were significant predictors of os in non - endemic ebv - related npc patients treated with imrt with or without systemic treatments ; tlg was demonstrated to have the highest hr for os . 
in particular , in the largest series including 371 patients , those showing a suvmax lower than 9 , 3 significantly had better 5 - year os compared to patients with higher values [ 9 ]  . 
 [ 19 ] in a study on 179 patients concluded that suvmax > 10.22 predicted worse moreover , in our analysis , a prognostic role of primary tumor suvmean was identified . 
similarly , patients having a tlg > 65 showed lower os and dfs compared to patients who with tlg < 65cc [ 11 ]  . on the other side , we did not find any association between pet parameters and dfs . although a crucial reason may be a low number of patients for the study , it is also true that a factor that can predict the outcome of loco - regional / distant metastasis survival and dfs may not always yield the same results for os . 
 xiao suggested that high fdg accumulation may primarily reflect the proliferative activity of npc and thus tumor aggressiveness [ 19 ]  . we can state that suv - t and tlg - t may refer to very aggressive tumors unsuited to salvage treatment . 
standard lumbar mri protocol of sagittal , and axial t1 weighted images ( wi ) and t2 wi and coronal short tau inversion recovery ( stir ) t2 wi were obtained . 
the level and above the level of lstv were evaluated for the lumbar disc space and facet degeneration based on grading methods which compares subtype groups with each other . results prevalence of lstv was 32% ( 600 of 1875 )  . 
but the groups with higher grade of disc degeneration were type iv and iii . conclusion in young male patients with lbp , lstv was found to be high in frequency and mostly occurred to be subtype i . 
coronal t2 stir images are useful in showing lumbosacral region anomalies and variants , and should be included in the routine lumbar mri protocol . keywords lowback pain lstv ( lumbocral transitional vertebra ) magnetic resonance imaging male maging in the lumbosacral transitional vertebra , the extreme elongation in the transverse process of the last lumbar vertebra fuses with the first sacral segment in different shapes in different subtypes called sacralization [ 1 ]  . 
in previous studies , lstv was studied in both sexes in different age groups and very variable results were obtained [ 4 ]  . the subgroups and types of lstv in regarding to disc and facet degenerations in young male patients with low vol . : ( 0123456789 ) 1 3 376 la radiologia medica ( 2019 ) 124 : 375381 back pain were investigated retrospectively by using castellvis lstv classification [ 8 ]  . materials andmethods the research was approved by the institutional review board at the local hospital . 
between march 2012 and january 2017 , 1875 consecutive lumbar spine mri studies on adult male patients younger than 40years of age with lower back pain , lumbar radiculopathy , or both at least four weeks were reviewed . 
both t1 - weighted spin - echo images ( tr / te , 637 / 12 ; repetition time msec / echo time msec ) and t2 - weighted fast spin - echo images ( 3073 / 85 ) were obtained through the lumbosacral spine in the sagittal plane and t2 - weighted fast spin - echo images in the axial plane ( 4.400 / 85 ) of the lumbar spine with slice thickness of 4mm were performed . 
also coronal t2 short tau inversion recovery ( stir ) images were added ( 2580 / 35 ) for exact evaluation of lumbosacral area and measurements of transverse process according to the literature with slice thickness of 4.5mm , sectioned parallel to the cauda equina at l3 to l5 vertebral body levels , was obtained [ 9 , 10 ]  . 
the field of view was 200 200mm for axial scans and 280 280mm for sagittal scans , with a matrix of 256 256 , slice thickness of 4.3mm , and a 1mm gap for both axial and sagittal imaging . lstvs were classified into incomplete or complete as well as uni or bilateral origin according to the castellvis classification [ 8 ]  . 
the disc degeneration and facet degeneration of the lstv level and above were recorded and correlated among the lstv subtypes i - iv . statistical analyses were performed using spss statistical software . 
1 coronal stir t2wi demonstrate the castellvi classification of lstv : a type ia : dysplastic unilaterally enlarged transverse process ( thick arrow ) , bone changes in iliac bone ( thin arrow ) ; b type ib : dysplastic bilaterally enlarged transvers process ( thick arrow ) , bone changes in sacrum ( thin arrow ) ; c type iia unilaterally pseudoarticulation of the transverse process with the sacrum with increased sclerosis ( arrow ) ; d type iib bilateral pseudoarticulation of the transverse process with the sacrum with increased sclerosis ( arrows ) 1 3 la radiologia medica ( 2019 ) 124 : 375381 fig . 
2 coronal stir t2 wi demonstrate the castellvi classification of lstv : a type iiia : unilaterally fusion with the sacrum ( arrows ) ; b type iiib : bilaterally fusion with the sacrum ( arrows ) ; c type iv : lstv type ii ( long arrow ) with type iii on the contralateral side ( short arrow ) using bonferroni - corrected mannwhitney u test to compare disc degeneraton , facet arthrosis and the t test for continuous variables , and chi square test . 
for comparisons , continuous variables were compared by using analysis of variance or ranked analyzes of variance as required , and categorical variables were compared by using chi square test . 
these variations can be detected easily with coronal mr images especially in type 1 lstv , otherwise axial and sagittal images are not enough to detect type i ( fig.3 a , b ) [ 13 ]  . 
these results correlated well with the previous reports [ 4 ]  . facet arthrosis , disc degeneration at the lstv level and above level were evaluated and compared among the lstv subtypes . 
the bonferroni - corrected mannwhitney u test analysis was done and facet degeneration has been found to be most affected in type i to the type ii and type iii on both sides ( p < 0.0083 ) on above level of the transition . 
 short tau inversion recovery ( stir ) coronal mri sequences which produces fat supression and yields high tissue contrast especially for the diagnosis of bone and soft tissue lesions were obtained for detailed anatomy ( fig.2 ) [ 12 ]  . more lstvs detected than most of the studies in the study ( 32% )  . 
the high prevalence of lstv may be explained by the superiority of the mr protocol used to diagnose lstv and the selection of young male patients with lbp for the study . patients with lstv can show age - related lumbar degeneration over time , which may mask early degenerative disease associated with lstv [ 4 , 8 , 18 ]  . 
for these reasons , this study was conducted in young male population to prevent age or sex - related outcomes for degeneration . the reason of pain in lstv is also a debate . 
 the articulation anomaly , contralateral facet ( in one sided anomaly ) degeneration , early degeneration and instability of the above level of lstv and nerve compression from bone hypertrophy are the main causes of low back pain in lstv [ 14 ]  . 
transitional level degeneration among subgroups of the lstv is most common in patients with lstv type ii in their study [ 14 ]  . the anatomy and variations is always complicated in nature . 
so , the pain is found to be much resistant to the therapy in lstv [ 21 ]  . the lstv prevalence was reported 4.635.9% in patients with low back pain and has been suggested to be investigated in the differential diagnosis especially in young population [ 15 , 17 , 21 , 22 ]  . 
all of the sagittal , axial and coronal mri images should be obtained for the correct identification of the transitional lumbosacral component [ 11 , 14 , 15 ]  . 
secondly , due to the large number of cases , we have not been able to assess the professions and physical activities of our patients , their body mass index as well . despite these limitations , to the best of our knowledge , this study was the first that was performed with mri in a young male group . 
in order to distinguish this variant from age - related degenerative changes and different age - related anatomic findings , it has been planned and studied in young male patients for the standardization of the study . conclusion lstv were found in 32% of selected young male population . 
it was known to be disc and facet degeneration were seen widely by the age which can mask lstv related degenerative findings alone [ 4 , 8 , 18 ]  . 
for this type of study formal consent is not required . la radiologia medica ( 2019 ) 124 : 422431 radiotherapy highdose intensitymodulated radiation therapy asprimary treatment ofprostate cancer : genitourinary / gastrointestinal toxicity andoutcomes , asingleinstitution experience beatricedetti1 muhammedbaki1 carlottabecherini1 calogerosaieva2 danielescartoni1 irenegiacomelli1 lauratrombetta1 cinziaciabatti1 giuliocarta1 lindapoggesi1 camilladellipaoli1 francescaterziani1 robertagrassi1 lorenzolivi1 cristinamuntoni1 emanuelaolmetto1 giuliofrancolini1 anaturkaj1 julianatopulli1 received : 7 july 2017 / accepted : 5 december 2018 / published online : 3 january 2019 italian society of medical radiology 2019 abstract purpose prostatectomy , radiotherapy and watchful waiting are the main therapeutic options available for local stage of prostate cancer ( pca )  . 
we report our experience on 394 patients affected by prostate cancer primarily treated with high - dose , image - guided , imrt , focusing on gastrointestinal , genitourinary toxicities and biochemical control . methods from july 2003 to august 2014 , 394 patients were treated with radical high - dose radiotherapy ( hdrt ) for prostate cancer ; the mean total radiation dose was 79gy in standard fractions . 
hormonal therapy ( ht ) was administered to 7.6% of low - risk patients , to 20.3% of intermediate - risk patients and to 72% of high - risk patients . 
patients were evaluated for biochemical failure , local recurrence ( lr ) and metastases . results ninety - seven patients ( 26.65% ) developed acute gu toxicity at the medium dose of 25.4gy , grade 1 ( g1 ) or grade 2 ( g2 ) in 94 cases . 
moreover , continued technologic advancements , as image - guided radiotherapy , could lead to further reduction in toxicity , thus increasing the therapeutic index . keywords prostate cancer intensity - modulated radiation therapy ( imrt ) genitourinary toxicity gastrointestinal toxicity introduction prostate cancer is the second most common cancer and the sixth leading cause of death among men [ 1 ]  . 
 radical prostatectomy ( rp ) , radiotherapy ( rt ) and watchful waiting / active surveillance in selected cases are the main available therapeutic options for early - stage disease . 
biochemical control and survival rates obtained with either treatment are comparable , at least in localized prostate cancer [ 3 ]  . randomized trials supported the indication of higher doses of rt in the treatment of prostate cancer [ 4 , 5 ] , associated with better results and higher biochemical disease control [ 69 ]  . 
in fact , the proximity of the rectum and bladder has been a limiting factor in safe dose escalation both in 2d and in 3d treatment planning era [ 6 , 11 ]  . 
 nevertheless , the technological evolution and improvements led to spare organs at risk ( oars ) and to limit their exposure : intensity - modulated radiotherapy ( imrt ) in association with image - guided radiation therapy ( igrt ) allowed to lower rates of severe toxicity , as well as a better quality of life [ 12 ] , often respecting normal tissue - sparing goals since igrt allows to correct target and oars movement immediately . 
in particular , imrt is associated with a significant reduction in acute g2 + gastrointestinal ( gi ) toxicity with a trend for a decrease in late g2 + gi toxicity [ 13 ]  . 
we , herein , report our institutional experience in 394 patients with localized prostate cancer treated with definitive high - dose , image - guided - intensity - modulated radiotherapy ( ig - imrt )  . 
we have also reported disease outcomes , in terms of loco - regional recurrence ( lr ) and distant metastasis occurrence ( dm )  . materials andmethods from our institutional database , we retrospectively reviewed the clinical data of 394 patients , treated between july 2003 and august 2014 with radical high - dose rt for localized prostate cancer . 
the main eligibility criteria were added which include : untreated histologically confirmed adenocarcinoma of the prostate and stage ct1c - t4 n0 m0 according to the sixth edition american joint committee on cancer staging systeprognostic risk groups stratification was made based on damico criteria . 
 data that were extracted from our medical records included age and tumor characteristics like gleason score and pretreatment psa . staging magnetic resonance imaging ( mri ) to evaluate for extraprostatic extension of disease . 
the planning ct scan was performed with 3 - mm slices in the supine position with leg immobilization system ( combifix - sinmed , civco , kalona , ia , usa )  . 
the clinical target volume ( ctv ) was limited to the prostate in low - risk patients , while in high - risk patients the entire seminal vesicles were included in the ctv . the planning treatment volume ( ptv ) was generated by adding an 8 - mm isotropic expansion to the ctv excepting 6mm posteriorly . 
for treatment planning , the dosevolume constraints for the bladder were v65 < 50% and a maximum dose < 65 gy ; for the small bowel v15 < 120 ccs and v45 195 ccs ; for the rectum : v50 gy 50% , v60gy 35% , and v70gy 20% . 
dose constraints for the organs at risk ( oar ) were selected based upon quantitative analyses of normal tissue effects in the clinic ( quantec ) data [ 17 ]  . 
ht was administered to 7.6% of low - risk patients ( subgroup treated in the earlier period ) , 20.3% of intermediate - risk patients and 72% of high - risk patients . 
 two hundred and forty - three patients received neoadjuvant , concurrent and adjuvant ht for a total of 6 - month duration in intermediate risk and for a total of 2years in high - risk disease . 
during rt , patients were visited at least once weekly by a physician . followup andtoxicity evaluation staging of pelvic lymph node and bone metastases was performed by computed tomography ( ct ) scan and bone scan , as indicated , and these were negative for all examined patients . 
radiological assessments were performed only as indicated by symptomatology or in case of biochemical failure according to astro criteria [ 21 ]  . statistical analysis loco - regional recurrence disease - free survival ( lr - dfs ) was defined as the time from the end of radiation therapy to the date of the first event , between loco - regional recurrence and biochemical failure . 
loco - regional recurrence was defined as the appearance of a new lesion in the prostate bed or in the pelvis lymph nodes detected by ct scan or by choline - pet . 
distant metastasis disease - free survival ( dm - dfs ) was defined as the time from the end of radiation therapy to the date of the first event of appearance of distant lesions , detected by ct scan , choline - pet or bone scintigraphy . 
in 38 cases ( 9.6% of the entire cohort , 54.3% of all deaths ) , death was deemed to be cancer related . the treatment was overall well tolerated , and all patients completed the prescribed course . 
 moreover , at mannwhitney statistical test no significant correlations were recorded between the dvh parameters and the toxicities developed by the patients ( see table3 )  . furthermore , we evaluated the comparison between available individual parameters of patients and toxicity by applying an appropriate statistical test according to the variables under consideration ( mannwhitney or chisquare test ) ( see table4 )  . 
4 dm - dfs according to administration of hormonal therapy ( ht ) before radiotherapy ( rt ) discussion comparison between radiotherapy and radical prostatectomy ( rp ) for localized prostate cancer is still a controversial issue . 
randomized clinical studies are necessary to better understand the benefits and risks of each therapeutic approach . we know that higher doses administered are associated with more probability of local control in prostate cancer . 
however , despite the better local control rates and outcomes that can be achieved with higher doses , we know that it can be translated into a big cost in terms of toxicities , especially to the rectum and bladder . 
the rates of acute and late toxicities after definitive rt vary according to the published studies ; generally grade 2 / 3 side effects can reach 40% of cases [ 3133 ]  . 
literature helps us to estimate them ; in fact , urinary incontinence and chronic proctitis are common and well - described side effects of radiotherapy , and sometimes they can develop into complications that can compromise the quality of life , some of which may even necessitate hospital admission or surgical intervention , namely posttreatment urinary or rectal bleeding , infections in the urinary tract or lower gastrointestinal tract and recto - urethral fistulae [ 30 ]  . 
the availability of three - dimensional conformal radiation therapy ( 3d - crt ) in addition to intensity - modulated radiation therapy ( imrt ) has prompted several investigators in the last 20years to explore the use of these technologies to escalate the radiation dose in prostate cancer avoiding worsening of the possible side effects . 
3d - crt , not long ago , had allowed a better sparing of the adjacent oars and a resultant decrease in rectal and bladder toxicity when compared to earlier techniques [ 25 , 28 , 29 ]  . 
in recent years , this advantage has even become greater with the development of imrt that allows a sharper dose falloff gradient , concave dose distributions and narrower margins with a more conformal delivery of isodose lines to ptv . 
most of the trials involving imrt use for prostate cancer therapy have demonstrated both safety and efficacy of dose escalation supported by the results shown in the literature [ 34 , 35 ]  . 
based on the growing body of literature in this regard , imrt has become the standard of care and most commonly employed technique . in our study , despite the use of higher radiation doses , the use of ig - imrt resulted in a low incidence of severe toxicities . 
 [ 13 ] published their results from the radiation therapy oncology group 0126 prostate cancer trial and demonstrated a significant reduction in acute gi / gu toxicity > g2 and a trend for a clinically meaningful reduction in late gi toxicity > g2 in patients treated with imrt compared as 3d - crt , while vora etal . 
with regard to disease outcomes , our results are in line with other published experiences in demonstrating that definitive ig - imrt in combination with adt ( as indicated ) can achieve long - lasting disease control in low - / intermediaterisk patients . we also showed favorable outcomes for patients with high - risk prostate cancer . 
however , the high precision of this technique requires precise delivery methods in order to reduce to the maximum the possibility of geographical miss that may result in increased dosevolume effects on the oars and in increased side effects , such as proctitis or cystitis [ 42 ]  . 
such image guidance for dose - escalated imrt should be the standard of care . several studies have analyzed both interand intrafractional displacements of the prostate , which ranged from 0.2 to 21mm depending primarily on rectal and bladder filling . 
 the magnitude and effect of organ motion of the prostate can be reduced significantly by standardized rectal and bladder filling and an accurate imaging [ 19 ] so their measures were used in our treatment . in our study , ht pre - rt was associated with a worse survival and a higher risk of distant metastasis . 
 [ 43 ] demonstrated that the use of long - course ht , from 3months before high - dose rt to 2years after , is associated with a better survival and a lower percentage of biochemical failure , without increasing radiotherapy toxicity . 
they showed that neoadjuvant ht , before radical prostatectomy , has no effect on survival , while neoadjuvant and adjuvant ht in combination with radiotherapy result in an increasing disease - specific and overall survival , although the duration of ht remains under debate . 
there appears to be an increased risk of cardiovascular morbidity and mortality associated with luteinizing hormone - releasing hormone agonists , particularly in men with preexisting cardiovascular disease , but the relevance of this in the adjuvant / neoadjuvant setting is currently unclear . 
a potential explanation for our results could be the heterogeneity of our population on the correlation of ht use with higher - risk disease based on damico classification and consequently with a worse prognosis . 
a particular strength of this analysis is that all of the patients included were treated at the same institution with the same positioning technique , identical delivery and immobilization devices , and a similar protocol for drinking and evacuation before treatment . 
this led to more standardization accounting for less interand intrafractional organ motion than in the previous reports . conclusions our data confirm the efficacy and limited toxicity of doseescalated ig - imrt for prostate cancer . 
further improvements in treatment delivery and image guidance should be the focus of future investigation to further improve the therapeutic ratio . compliance with ethical standards conflict of interest we declare that the absence of conflict of interest and financial relationships relevant to the content of this article have been disclosed by all authors . 
we had full access to all data in this study , and we take complete responsibility for the integrity of the data and the accuracy of the data analysis . research involving human participants all procedures performed in this study involving human participants were in accordance with the ethical standards of the institutional and its later amendments or comparable ethical standards . 
for our retrospective study , formal consent is not required . informed consent all authors declare that informed consent was obtained from all individual participants included in the study and to have used adequate strategies for protecting anonymity . 
our objective is to compare outcomes of conventional laparoscopic ligation ( ll ) and occluding balloon embolization ( obe ) a percutaneous interventional procedure . materials and methods we treated retrospectively a total of 98 patients , divided in two cohorts ; arm a with 48 and arm b with 50 patients . 
we performed a comparative analysis ( fishers test ) of intra - operative time , hospitalization and patients postoperative recovery time . results and limitations outcomes have been in line with the recent literature ones , allowing the occluding balloon embolization a small advantage for quicker operative average time , hospitalization needed and full recovery to normal activities for the patient . 
86 , campusul universitar vasile goldis , arad , romania 4 department ofradiology andradiotherapy , policlinico universitario gaspare rodolico , azienda ospedaliera universitaria policlinico vittorio emanuele , via santa sofia n.29 , 95100catania , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 438443 background varicocele is a relatively complex pathology that affects the pampiniform plexus of veins in the spermatic cord . 
 according to the modern literature [ 1 , 2 ] , this condition affects 2025% of the normal adult male population and is well known as the most common treatable cause of male infertility ; percentages are higher in studies applied to infertile population ( up to 40% )  . 
a gross , first sight of well - developed va is the enlargement of the testicle , and at this level veins can be easily seen through patients skin , aspect named in the past and modern literature as a bag of worms . objective this paper aims to compare the conventional laparoscopic ligation ( ll ) with a specific approach among other methods used to treat this condition in interventional radiology ( ir ) , which is not yet known as standard one , named occluding balloon embolization ( obe )  . 
 a great concern from patients perspective is the potential benefit of treating an established va in order to enhance chances of natural conception ; for its characteristics , management of this pathology has indeed a sensitive nature . 
this original research will be focused on patients advantages and outcomes of these techniques . methodology the study plan is a retrospective comparative analysis , and the design is a parallel one with a total of 98 adult patients divided in two cohorts ; arm a with 48 and arm b with 50 patients ( with observational purposes ) , from two european institutions . 
hence , all patients have been asked to respect 3 and 6months follow - up ; clinical examination and ultrasonography were performed . we treated group - a patients with ll , two operators for the entire cohort with more than 200 cases experience . 
the cohort is made of 48 patients , 22 with symptomatology and 24 with spermiographic abnormalities ; age range varies from 16 to 45years old , with average of 29years . 
for surgical methodology , our team has followed tu and glassberg [ 5 ] surgical steps . patients from group b underwent obe with the technique explained in the literature [ 6 ] by a single operator with more than 200 cases . 
1 shows a lsv phlebography , the white arrow specifies position of the catheter tip ( mid - portion of the vein ) , contrast reflux ensure the presence of va 1 3 440 la radiologia medica ( 2019 ) 124 : 438443 4 . 
2 a shows the balloon in position and inflated before testicles wrapping and sclerosant agent injection ( white arrow ) , b post - embolization check - up shows lsv occlusion ( black arrow ) fig . 
 a correct position of the ob catheter ( proximal barrage ) , b rubber band / tourniquet ( distal barrage ) , c : valved introducer , d pampiniform plexus within the scrotum considering complications , three patients encountered minor allergic reactions ( no medical therapy required ) , just one case with major allergic reaction and subsequent injection of betamethasone . 
the retrospective study did not require ethical approval by local commission . patients involved in this study have been selected from june 2014 up to april 2016 ; in cases of partial occlusion of the lsv , embolization has been finalized with coils . inclusion andexclusion criteria main criterion of acceptance is va grade iii according to the sarteschis classification [ 7 ] , thus diagnosed by cdus ; hence clinically recognized as grade iii , left sided only . 
both persistent pain and spermiogram anomalies have been recognized as criteria of inclusion . exclusions criteria , instead , are : previous therapeutic attempts , coagulopathies and age below 14years old and above 42years of age . 
no other comorbidities have been accepted such as diabetes , hypertension and other existing diseases ; particular attention has been devoted to further possible scrotal conditions . results andlimitations both techniques showed a good amenability in terms of results ; moreover , outcomes of this research have been in line with the recent literature ones [ 811 ] , allowing the obe a small advantage for quicker operative average time , hospitalization needed and full recovery to normal activities for the patient ( fig4 )  . 
medical therapy suggested after treatment is ibuprofen ( brufen 600mgabbot ) if required by symptomatology . for laparoscopic procedure , the operative time average is of 45min ( door to door ) , and is practiced in day - hospital regime ( 24h ) due to patients preparation and post - anesthesiology care . 
analgesic prescribed post - operatory outcome measurements andstatistical analysis our method concerning outcome measurements has been focused on patients benefits , such as : operative time , hospital stay and full recovery . 
fisher test has been used for statistical analysis , creating a 2 2 contingency table and applying a two - tailed p value ; table1 shows rate of complications and technical success / recurrence . operative time ( minutes ) hospital stay ( hours ) full recovery ( days ) fig . 
the single intra - operative dose of antibiotic therapy is considered sufficient . we have decided not to run a cost - effectiveness analysis due to lack of time and possible biases driven by price differences of materials used among different countries . 
nevertheless , some publications [ 8 ] assess similar costs between percutaneous embolization and ll , while others [ 12 ] claim microsurgery repair to be cheaper than these two approaches analyzed in this paper . 
being this work a retrospective one with a limited number of cases evaluated , the common decision has been to avoid semen analysis ; results would eventually be not statistically relevant in this particular effort . discussion treating varicocele improves semen parameters and testicle dimension , providing support to further therapies of reproductive medicine / biology such as icsi ( intra - cytoplasmic sperm injection ) and tese ( testicular sperm extraction ) , hence is the only strategy at our disposition in the case of painful symptomatology of the scrotum related to va . 
the technique proposed in this research is already known as a useful maneuver in some situation of spermatic embolization [ 13 ] , but it has been suggested as standard technique for va only in one paper [ 6 ] ; up - to - date reviews such as the one proposed by halpern etal . 
laparoscopic varicocelectomy has been previously compared to percutaneous embolization [ 8 ] ; nonetheless , more in detail , for a certain period and probably even nowadays coils usage is preferred by many operators . 
underline the effectiveness of percutaneous sclerotherapy as first line of treatment , this group has used mainly the aethoxysclerol as agent of choice , similarly to our experience ; hence , they do mention the use of the occluding balloon in cases of severe renal vein reflux [ 10 ]  . 
this original research , despite a limited casuistry , has provided more glances of viable approaches and techniques ; the obe has not been compared to surgical procedures up until now . 
the advantage of injecting sclerosant agent through an occluding balloon is mainly the enhanced control of the injection , accompanied by maximum concentration of aethoxysclerol at static flow and without dilution ( occurring with free flow technique )  . 
additionally , in the hands of an experienced operator , obe technique could be performed even in the cases of right - sided va , adapting opportunely to eventual anatomical variants [ 15 ]  . 
our results prove , in line with the modern literature [ 14 ] , comparable outcomes of these interventions ; conceding obe a slight advantage in terms of hospital stay and full recovery to normal activity of patients , minding the use of radiologic equipment and irradiation at acceptable levels . 
further studies among differences of these and other approaches such as microsurgery could uncover the best option suitable in terms of cost - effectiveness , patients safety and satisfaction of the procedure and resulting complication rates . 
last but not least , we believe this topic needs further efforts in order to improve quality of data available , besides randomized controlled trials including live birth and pregnancy rates as suggested by the latest cochrane review [ 14 ]  . conclusion in consonance with the modern literature , these two techniques have not showed a significant statistical difference . 
in ll , a longer recovery period is needed as well , though this time may vary slightly from patient to patient . one of the disadvantages produced by radiological procedures are the effects of radiation to patients body and gonad , and these have been statistically analyzed and discussed before attempting such intervention . 
color and pw - doppler analysis showed a reduction in renal blood flow in kidneys during the hypoperfusion with a progressive and significant change from baseline values of resistive index ( ri )  . 
at the histological evaluation , 60min of hypoperfusion resulted in ischemic changes in the kidneys . conclusions the results of this experimental study encourage the use of the described model to study acute renal ischemia trough severe hypoperfusion . 
cardarelli hospital , via cardarelli 9 , 80131naples , italy 3 division ofpathology , department ofpublic , clinic andpreventive medicine , second university ofnaples , piazza miraglia 2 , 80138naples , italy 4 department ofradiology , university ofmolise , via francesco de sanctis , 1 , 86100campobasso , italy introduction acute ischemia is the most common cause of acute renal failure [ 1 ]  . 
the acute kidney injury following the hemorrhagic shock remains a crucial problem : it occurs in approximately 30% of patients admitted in intensive care units and is commonly associated with multiple organ dysfunction syndrome ( mods ) [ 2 ]  . 
ultrasound ( us ) is the first choice for its non - invasiveness , thus permitting repeated measurements invivo [ 4 ] , as already demonstrated in previous studies [ 5 , 6 ] , and renal blood flow can be evaluated using us color and pulsed - wave ( pw ) doppler [ 4 ]  . 
in the literature , many studies use animal models reproducing ischemia blocking locally renal vessels , with a clamp or with a surgical ligation [ 79 ]  . none of them evaluate acute kidney injury caused by systemic hypoperfusion , assessable recreating hemorrhagic shock , and explored by micro - us . 
 other models are not severe enough [ 11 , 14 ] or the ischemic injury is followed by reperfusion , or the histological damage caused by ischemia is not analyzed [ 15 , 16 ]  . 
furthermore , it is not clear whether they are suitable for a radiological evaluation , thus permitting to systematically study the imaging findings . the aim of this work is to create an animal model of acute renal ischemia induced by systemic hypoperfusion , which may result controllable and reproducible , to study , in real time , hemorrhagic shock in rats with micro - us . 
this model allows not only to define the morphological changes that occur in renal parenchyma and in other organs after hemorrhagic shock , but also to test diagnostic markers and drugs , which is becoming crucial in the success and timeliness of research and is allowing a more efficient approach in investigating small living animal models longitudinally studied by noninvasive imaging tools [ 17 , 18 ]  . 
the progression of renal damage was monitored by a high resolution micro - us system , dedicated for small animals . materials andmethods animal preparation all procedures performed on animals were in accordance with the ethical standards of the institution and were approved by the institutional animal care and use committee . 
mean arterial blood pressure ( map ) was continuously measured using a catheter placed in the right femoral artery and connected to a pressure transducer , displaying on a monitor the map values . appendages were secured to electrocardiogram pads to allow constant monitoring of the heart and the respiratory rate . surgical procedures andcatheter placement after a bilateral inguinal incision , polyethylene catheters pe50 ( inner diameter , 0.58 ; outer diameter , 0.96mm ; clay adams , becton dickinson & co , parsippany , nj , usa ) were placed in the femoral arteries and fixed by polyglycolic acid suture ( vicryl 3 / 0 , ethicon inc , summerville , nj )  . 
the catheter inserted in the right femoral artery was connected to a pressure transducer ( apt300 , harvard apparatus , holliston , massachusetts , usa ) calibrated to the atmospheric pressure . 
it was achieved in 2530mfor the next 60min , the map was maintained at a constant pressure value , between 25 and 30mmhg , by automatic pump infusion and withdrawal . us imaging rats were placed in a supine position on the imaging platform ( vevo rat platform , visualsonics , toronto , canada )  . 
 depilatory cream was used to remove fur from the abdominal skin , and medical ultrasound acoustic gel ( aquasonic 100 ; parker laboratories , inc , fairfield , nj ) was used as a coupling fluid between the real - time micro - visualization scanhead and the skus imaging was performed using 1 3 la radiologia medica ( 2019 ) 124 : 323330 fig . 
1 a vevo 2100 us system ; b inguinal incision with isolated femoral artery ( yellow clip ) and positioning of the catheter ; c view of the bilateral inguinal incisions with catheters placed in the femoral arteries ; d syringe pump ; e pressure transducer the vevo 2100 system with 30 micron resolution ( visualsonics , toronto , canada ) using the ms250 transducer ( 1324 mhz ) , positioned and fixed by a dedicated arm ( visualsonics vevo integrated rail system ii )  . 
renal size , morphology and echogenicity were evaluated in b - mode ; it was used to acquire two dimensional images of the kidneys . the probe was positioned on the abdominal skin with a thin layer of ultrasound acoustic gel . 
the main renal arteries arise laterally from the aorta and were visualized using a transverse midline approach . renal blood flow was evaluated using color - doppler us , in a transversal scan of each kidney , and the area of interest was positioned including the kidney vessels to examine the arterial and venous flow . 
the sample volume was placed within the renal artery at the hilum , and the system generates a pw - doppler spectrum which provides the velocity information with the software . 
the same pw - doppler analysis was done for intrarenal arteries , the arcuate arteries ( at the cortico - medullary junction ) or interlobar arteries ( adjacent to the medullary pyramids )  . 
the arcuate arteries are relatively small and tortuous , and determination of the angle of doppler insonation relative to the vessel , required for blood flow velocity calculation , cannot be accurately achieved . 
therefore , analysis of arcuate artery flow spectra is mainlybased on ri evaluation , where doppler insonation angle is irrelevant [ 20 , 21 ]  . interobserver variability assessment the evaluation of renal echogenicity , before and after the hypoperfusion , was assessed independently by two observers ( fi and ts ) , who have graded the kidney echogenicity in comparison with the image acquired at t0 . the kidney echogenicity was graded and recorded using the following scale : grade 1 hypoechoic ; grade 0 : equally echoic ; grade 1 : slight hyperechoic ; grade 2 : moderately hyperechoic ; grade 3 : markedly hyperechoic . interobserver agreement among the two readers was assessed using cohen statistic . 
reliability of categorical data is commonly quantified by the kappa coefficient , which indicates the beyond chance agreement and ranges 1 3 326 la radiologia medica ( 2019 ) 124 : 323330 from 0 ( indicating no agreement beyond chance ) to 1 ( when agreement is perfect )  . to calculate the interobserver agreement by cohen statistic , the grade 2 of kidney echogenicity was considered as positive ( + ) and the grade 1 as negative ( ) ( table1 ) , and p < 0.05 was considered to indicate statistical significance . 
a colordoppler us scan in axial plane showing the physiological blood flow in the renal artery ( red arrow ) and in the renal vein ( white arrow ) ; b color - doppler us scan in axial plane showing a marked reduction in renal blood flow after 60min of renal hypoperfusion ; c pulsed - wave doppler us image showing the renal blood velocity at the renal artery before the induction of hypoperfusion ; d pulsed - wave doppler us image showing reduced blood flow velocity in the left renal artery after 60min of hypoperfusion fig . 
4 renal blood flow at both the renal and intrarenal arteries showing the increase in vascular resistance at different time : a pwdoppler analysis at the renal artery after 60 min of hypoperfusion , showing a high peak systolic frequency shift with a ri > 0.70 ; b renal blood flow at intrarenal arteries after 30min of ischemia . 
histology revealed anatomopathological alterations in both cortex and medulla , such as dilatation and congestion of glomerular arterioles , edema of the connective tissue with some polymorphonuclear cells ( pmn ) , intraparenchymal hemorrhage , red blood cell extravasation , cellular debris , flaked cells and amorphous material in tubular lumens . 
in models with a map of 3035mmhg [ 22 , 23 ] , regulatory mechanism are still effective , making it difficult to maintain a severe shock requiring repeated withdrawal of blood , negatively affecting reproducibility . 
models of severe shock protracted for 60min have been realized , but none of them evaluates the suitability to study organs with imaging techniques in comparison with histological findings [ 15 , 16 ]  . 
5 results of the two observers evaluation of the kidney echogenicity , graded and recorded using the following scale : grade 1 hypoechoic ; 0 , equally echoic ; grade 1 : slight hyperechoic ; grade 2 : moderately hyperechoic ; grade 3 : definitely hyperechoic fig . 
 a cortex of the left kidney 40 : dilatation of bowmans space with red blood cell extravasation ( black arrow ) , glomerular congestion ( blue arrow ) and edema of the connective tissue with rare pmn ( red arrow )  . 
b cortico - medullary junction of left kidney 40 : cellular debris , flaked cells ( blue arrow ) and amorphous material in tubular lumens ( black arrow ) 1 3 la radiologia medica ( 2019 ) 124 : 323330 ischemia , but most of them are focused on chronic injury , studied on models of localized ischemia obtained by surgical ligation or clamping of the renal artery [ 9 , 24 ]  . 
the model we here describe is a systemic model that allows to study with micro - us the physiopathology of acute ischemia in the kidneys , by a pure model of hypoperfusion , which is the most common cause of renal failure . 
for its realization , several issues have been evaluated . in rats with a weight equal to or less than 320g , the reduced caliber of the vessel caused a difficult catheterization of the femoral arteries . 
on the other side , in animals with a weight exceeding 420g , the acquisition of ultrasound images is hampered by the interposition of the intestinal loops , considering the forced decubitus . 
consequently , the choice of the weight has to range from 400 to 410 g , preferably with the aid of a few drops of papaverine that locally dilate the artery , facilitating the access of the catheter . the supine position is obliged by the presence of the catheters , but is also ideal for the acquisition of ultrasound images of the kidney and other abdominal and thoracic organs during the state of hypoperfusion . another issue to be considered in the model planning was the choice of the blood pressure value to achieve during the shock period : from data literature , a value equal to or less than 20mmhg results in the death of rats in about 20min [ 15 ]  . 
achieving a map between 21 and 24mmhg , there is a high variability in terms of survival [ 15 ] , while achieving a value of map higher than 30mmhg the compensation mechanisms are still too effective [ 15 ]  . 
this means that the most severe model of hypoperfusion reproducible must maintain a map between 25 and 30mmhg . the length established for the shock period is 60min as it is the optimal ischemic duration for depiction of renal ischemia on us [ 9 ]  . 
the state of suffering is evident as altered respiratory rate and sudden drop in blood pressure , immediately after the 60th min , which cannot be compensated by the syringe pump . micro - us with pw and color - doppler allows to examine and to monitor in real - time vessels blood flow and organs during hypoperfusion in the animal model , being a useful and versatile tool in the study of physiopathological mechanisms and in the evaluation of the efficacy of new experimental therapy . 
in intrarenal ( segmental and arcuate ) arteries , ri slightly increased during the first 30mafter 30min of hypoperfusion ri decreased remaining , however , below the threshold of 0.70 , this is probably due to the intervention of compensatory mechanisms . the rat model used in this study has several limitations : blood withdrawal was slow , thus not causing a significant increase in the heart rate , while in clinical practice bleeding can be more rapid leading to a compensatory tachycardia . 
 severe hemorrhagic shock cannot be prolonged for more than 60min , as evidenced by the decrease in the respiratory rate and by the sudden fall of the map value at the end of the first hour of hypoperfusion . 
our study has no correlation with laboratoristic data ; however , the kidney injury was histologically confirmed . conclusions this study protocol reproduces a severe hemorrhagic shock in a rat model , with a reasonable survival rate of the animals for the experimental period . 
the analytic data set included the interpreting radiologists years of experience , patient age , patient gender , radiologist gender , ordering service and clinical question to be answered as collected from the radiology request forms . results of the 1996 us and ct examinations performed between october and december 2016 in the inpatient setting , 34% ( 683 examinations ) had a radiologists rai . 
indeed , the growth rate of imaging reflects expanded applications that have occurred over the years in high - tech imaging services such as computed tomography ( ct ) , magnetic resonance ( mr ) imaging and ctpositron emission tomography ( pet - ct )  . 
some publications have suggested that as many as 2050% of high - tech imaging procedures may fail to provide information that improves patient welfare and therefore may represent , at least in part , unnecessary imaging services [ 3 ]  . 
aside from referring physicians , it has been reported that radiologists too make recommendations for further imaging tests in their vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 432437 interpretative reports [ 4 ]  . 
the aim of our study was to measure the proportion of radiologists additional recommended imaging examinations ( rai ) at a hospitalbased inpatient setting and to estimate the influence on rai of radiologist gender and radiologistsyears of experience , of patient gender , patient age , ordering service and clinical question to be answered as collected from the radiology request forms . methods inpatient ct and us examinations interpreted by fifteen radiologists between october and december 2016 at the fondazione ptv policlinico tor vergata were evaluated by two radiologists . 
reports that recommended correlate with clinical information or other suggestions to glean missing clinical information were excluded . the influence on rai of radiologist gender and radiologistsyears of experience and of patient gender , patient age and ordering service were evaluated . 
also the clinical question to be answered was collected from the radiology request forfor each of the clinical question to be answered collected , the number and percentage of examinations with at least one rai were enumerated . 
then the effect size ( odds ratios ) and significance ( confidence intervals ) of each clinical question to be answered on the likelihood of rai was calculated . this retrospective study was approved and waived for patients consents by the institutional review board ( irb )  . statistical analysis data were analyzed with the nonparametric mannwhitney u test . 
 odds ratio with the respective confidence intervals was calculated using medcalc software . results analysis ofct andus imaging reports of the 1996 us and ct examinations performed between october and december 2016 in the inpatient setting at the fondazione ptv policlinico tor vergata , 34% ( 683 examinations ) had a radiologists recommendation for additional ct , pet - ct or mri . 
the largest proportion of imaging examinations prompted by a radiologists recommendation was for chest ct ( n = 260 , 38% ) , followed by pet - ct ( n = 198 , 29% ) , abdominal ct ( n = 164 , 24% ) and abdominal mri ( n = 61 , 9% )  . 
chest ct was most often prompted by a recommendation in chest ct ( 58% ) and whole body ct reports ( 42% ) ; pet - ct , in chest ct ( 52% ) and in whole body ct ( 48% ) ; abdominal ct , in abdominal us ( 93% ) and in whole body ct ( 7% ) reports ; abdominal mri , in abdominal ct ( 56% ) and in abdominal us ( 44% ) reports . 
 also , inconclusive radiology examinations were another relatively common reason for additional imaging recommendation ( 11% )  . pulmonary solid or subsolid nodules < 6mm were the most common findings that prompted a rai ( 31% ) , followed by adenopathy ( 23% )  . 
the other findings leading to additional imaging were renal lesions ( 14% ) , liver lesions ( 12% ) and pulmonary parenchyma abnormalities other than nodules ( 9% )  . correlation withclinical variables in our cohort , there were 438 patients ( 172 males and 266 females , mean age 52 14years ) , 203 were hospitalized in the clinical medicine department , 132 in the surgery department and 103 in the neuroscience department . 
the authors found that the individual radiologist influenced the frequency of recommendations for additional imaging , the percentages of recommendations for additional imaging ranged from 12% to 45% . in our study , chest ct was the most represented rai . 
we hypothesize that the higher proportion of recommendations for follow - up chest ct of small nodules < mm 6 resulted from our radiologists not adherence to these recognized guidelines [ 8 ]  . pet - ct was the second most frequently rai . 
most of the published studies have shown high pet - ct sensitivity and specificity when maximum standardized uptake value of 2.5 was used as the cutoff to differentiate benign from malignant conditions [ 9 ]  . 
 however , no clear guidelines have been established for the employment of pet - ct in the evaluation of enlarged lymph nodes [ 9 ]  . liver and renal lesions were the other findings that often generated radiologist - recommended mri or ct evaluation in our cohort . 
6 scatterplot shows distribution of rai percentages by use of the two discriminant functions obtained for linear discriminant analysis : y - axis , radiologists years of experience ; x - axis , radiologist gender . 
blaivas and lyon [ 5 ] and baumgarten and nelson [ 6 ] found that in abdominal computed tomographic scans the rate of radiologists recommendations for additional imaging in the outpatients setting was , respectively , 31% and 19% , which is comparable to what we found in our inpatient setting ( 34% )  . 
 table 1 rai stratified according to clinical question to be answered as collected from the radiology request forms 1 3 436 la radiologia medica ( 2019 ) 124 : 432437 evaluation by which they can be characterized as benign versus malignant . 
although it is known that most incidental findings often have little or no clinical significance , the drive to evaluate them is often prompt by radiologist and patient unwillingness to accept uncertainty , even given the rare possibility of an important diagnosis . 
by the inappropriate or suboptimal selection of the initial imaging modality . indeed , the excessive ordering of diagnostic tests is one of the most frequently encountered forms of defensive medicine ( a ) , which is defined as a deviation from sound medical practice induced mainly by the fear of liability [ 13 ]  . 
radiologists aware that malpractice liability can make clinical errors more costly , resort to diagnostic tests that , they hope , will reduce the probability of diagnostic error . however , defensive medicine typically operates together with several other variables to motivate clinical practice decisions [ 14 ]  . 
some of these variables may be clinical such as patient symptoms , seriousness of the suspected disease , degree of certainty about diagnosis and accuracy of the available diagnostic tests . 
others are nonclinical , such as availability of technology , years of training and communication skills . with respect to the radiologist gender , we found that male radiologists were more prone to recommend a supplement examination . 
thus , it maybe not surprising that in our cohort female radiologists recommend for less supplement imaging than male radiologists . on the other side , a communication gap between the radiologist and the referring clinician could result in ( b . ) inappropriate or suboptimal selection of the initial imaging modality [ 16 ]  . 
a radiologistclinician consultation would be advisable for a better and more complete understanding of the clinical scenario , especially for complicated patients with multi - morbidities such as those hospitalized in the clinical medicine department . 
however , whether or not these systems will lead to changes in radiologists recommended clinical imaging also remains to be seen . notably , in our cohort of radiologists there was a negative correlation between the radiologists years of experience and rai meaning that there is a tendency in younger participants to recommend supplement imaging . 
we hypothesize that radiologists improve their accuracy and confidence as they build their experience base and gain more knowledge through continuing education . when rai was stratified according to the clinical question to be answered , pneumonia showed the highest rate of rai due to follow - up of lung nodules . 
 it is possible that recommendations for further imaging are not acted upon by the referring physician [ 18 ]  . in conclusion , a high percentage of rai resulted from ct and us radiologists reports in our inpatient setting . 
chest ct follow - up was the most frequently rai driven by the presence of pulmonary nodule in prior ct imaging , followed by pet - ct driven by adenopathy documented in prior ct . 
also , follow - up studies are warranted to assess the number of rai that are actually acted upon by the referring physicians . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this study was approved and waived for patients consents by the institutional review board ( irb )  . 
these methods seem to have similar efficacies for the evaluation of vessel stenosis , legitimizing the use of the developed phantom as a versatile and reproducible instrument that could be used during quality controls programs . keywords carotid atherosclerosis diagnosis ultrasound magnetic resonance imaging quality controls introduction atherosclerosis is a chronic disease that affects medium and large arteries . 
the resultant plaque can obstruct lumen or disseminate material into blood stream and could be a cause of myocardial infarction , stroke and peripheral vascular disease [ 1 ]  . in particular , carotid atherosclerosis is very important in the pathogenesis of cerebral ischemia [ 2 ]  . 
although advances in the understanding and treatment of these lesions * giuseppe acri gacri@unime.it italy 1 department ofbiomorf , university ofmessina , messina , irccs centro neurolesi bonino - pulejo , messina , italy 3 biomedical department ofinternal andspecialistic medicine , university ofpalermo , palermo , italy 4 casa di cura cristo re , messina , italy 5 high school campo calabro ( rc ) , campocalabro , italy have been performed , thrombotic complications of atherosclerosis remain one of the most important causes of morbidity and mortality in western society [ 3 ]  . it should be important to have a noninvasive imaging technique capable to identify , not only the presence , but also the stage of intra - plaque hemorrhage . 
currently , the predominant noninvasive imaging modalities investigated for this purpose are ( a ) ultrasonography ( us ) and ( b ) magnetic resonance imaging ( mri ) techniques [ 4 ]  . in particular , us and mri are highly sophisticated imaging modalities for an accurate and timely diagnosis [ 2 , 5 , 6 ]  . 
mri utilizes powerful static magnetic fields to align the magnetic spins of the protons in water molecules and to drive the larmor precession which provides the signal used to construct the image [ 7 ] , whereas the principle of ecography is similar to that of sonar or radar ; in essence , following an us pulse transmission , echoes from the medium being interrogated are detected and used to form an image [ 8 ]  . these us waves are transmitted from probe to body , and the signal is reflected wherever there is an interface between two tissues with different acoustic impedances . 
it should be possible to differentiate soft and unstable plaques with liquid constituents from solid , hard , and stable plaques . these diagnostic modalities are based on acquisition and correct evaluation of images . 
underhill [ 13 ] , crowe [ 14 ] and mani [ 15 ] were the first who investigated the relation between carotid mri and us . in any case , it is important to guarantee the maintenance of the consistent image quality of the radiological equipments . 
in this context , quality controls ( qc ) have an important role because qc enables a complete evaluation of system status and image quality [ 1618 ] and permit the identification of image quality degradation and source of possible equipment malfunction [ 5 , 19 ]  . 
in fact , the purpose of qc testing is to detect changes that may result in a clinically significant degradation in image quality [ 20 ] which reduces the ability to detect and correctly interpret abnormal findings . for this reason , the optimization of image reproducibility motivates the calibration of acquisition protocols that use phantoms with defined dimensions , inserts etc . phantoms are usually used in order to guarantee the maintenance of consistent image quality over lifetime of the diagnostic equipment . in this context , to geometrically characterize carotid atherosclerotic lesions , diameter stenosis percentage and area stenosis percentage have to be determined . 
therefore , accuracy of stenosis size represents a significant parameter that should be estimated during qc , to correctly evaluate area stenosis percentage . however , most us and mri scanners adopt specific automated procedures that require the use of dedicated phantoms . 
1 upper and lateral view of the phantom modalities and require specific protocols depending also on specific diagnostic device [ 2123 ]  . recently , we realized a single polymethyl methacrylate ( pmma ) phantom that was suitable to perform quality inspection both on ct and on mri that may be used to provide a complete quality inspection of a ct and mri equipment [ 24 ]  . 
in this work , we performed a us and mri examination , by using the novel phantom , for a qualitative and quantitative stenosis evaluation . the reliability of this study was evaluated by a detailed statistical analysis . 
the parameters that characterize the blood vessel are : diameter 5mm and thickness 1min order to mimic the us and mri characteristics of a stenosis , we inserted a thin semirigid plastic wall . 
the choice of pmma and semirigid plastic tubing was related to the necessity of using no ferromagnetic elements in order to perform geometric stenosis measurements both on an mri scanner and on an us device . 
in previous works , stenosis models with different diameter and / or area reductions have been manufactured in order to study the effect of the degree of stenosis and flow rate in large vessels in ct , mri and us [ 2123 ] , but no comparison among different 1 3 370 la radiologia medica ( 2019 ) 124 : 368374 table 1 physical and acoustic properties of blood mimicking fluid compared with the human blood properties human blood ( 37c ) blood mimicking characteristics ( e.g. , viscosity , acoustic properties ) of human blood , as indicated in table1 . 
in particular , models which mimicked area stenosis in large vessels ranging from 18% up to 90% were made . the pmma box was filled with distillate water , while the hollow cylinder was filled with a liquid solution , mimicking human blood , and containing : water , glycerol , orgasol , detergens , citric acid and acnibio ocs ( dansk fantom service )  . 
 orgasol , characterized by nylon particles 5m in diameter , has been used in blood mimicking fluids when natural buoyancy of the particles has been achieved , whereas glycerol avoids refraction [ 2527 ]  . 
2 us images of the novel dedicated phantoa longitudinal cross section ; b longitudinal cross section and measurements performed us andmri data acquisition the common carotid artery ( cca ) us data were obtained as longitudinal cross sections using two different us devices : a philips iu22 us and a philips ie33 systein both us systems , a broadband linear l9 - 3 probe , operating in 39mhz frequency range , was used . 
in both cases , the sequences we considered were a t1 - weighted turbo spin echo ( t1w tse ) sequence and a t2 - weighted turbo spin echo ( t2w tse ) one . 
in addition , a t2 spectral presaturation with inversion recovery ( t2 spir ) sequence was also considered in order to suppress fat and reconstruct carotid artery wall [ 2830 ]  . 
 the concordance correlation coefficient combines measures of precision and accuracy , to determine how the observed data deviate from the line of perfect concordance ( line at 45 on a square scatter plot )  . 
intra - rater analysis was used to determine test rest - reliability , comparing the different scores marked by the same rater on the same phantom with different methods . finally , inter - rater agreement was assessed between the various measurements obtained with the different techniques in order to test the performance stability with different raters . 
statistical significance was set at p < 0.05. results accuracy measurements in tables4 and 5 , the results of the measurements , respectively , conducted on us and mri devices are reported . 
in this study , we assess the diagnostic ability of us and mri techniques to identify and measure carotid stenosis . in order to choose a method for investigation , different parameters should be considered : availability of modality , level of optimization and the capability of patient and operator . 
on the other hand , by using mri it is possible to acquire tridimensional images with the high contrast resolution . other authors have conducted studies about the use of dedicated phantoms to evaluate stenosis parameter [ 2123 ] , but no comparison between diagnostic devices was performed . 
this is a first study that reports a comparison among two different us modalities and two different mri strength fields ( 1.5 and 3 t ) with a novel phantom approach . in this context , we developed a novel phantom , simulating a vessel stenosis that can be used both on mri and on us devices . 
its preparation requires only the filling of the hollow cylinder and the pmma box , using , respectively , a solution , simulating human blood and distillate water . the accuracy obtained using the 3 t device is significantly higher than that obtained using the other diagnostic scanners . however , statistical analysis showed that no significant difference exist between us and mri techniques . 
in fact , us and mri have shown similar diagnostic efficacies for the evaluation of vessel stenosis , using the novel phanto the obtained results showed that there was concordance between the two different diagnostic techniques ; however , we found significant results in inter - rater agreement . 
this could be due to the fact that the 3.0 t magnet has the capability to provide a better image quality as the base for improved diagnostic performance , because doubling the field strength ( almost ) doubles signal - to - noise ratio , that is , the quantity of signal made available from the patient in order to build mri images . the proposed method employs a new universal phantom , which can be used on any us and mri device , in a quick manner , to evaluate stenosis vessel . 
mean adc values ( b50 + b400 + b800 / 3 ) of parathyroid lesions were compared with that of normal appearing thyroid parenchyma ( tp ) , sternocleidomastoid muscle ( scm ) and jugulodigastric lymph nodes ( jdln )  . results of lesions , 4 were parathyroid hyperplasia , 13 parathyroid adenoma and 3 parathyroid adenocarcinoma . 
by increasing strength ( b value ) of diffusion tensor on dwi , solid parathyroid lesions still kept their brightness comparing other soft tissue structures of head and neck region because of their high t2 properties . conclusion solid parathyroid lesions had higher diffusion properties comparing other soft tissues structures of head and neck region . 
 preoperative evaluation of parathyroid pathology includes studies such as usg , scintigraphy , ct , spect - ct fusion scan ( 4d ct ) and mri [ 2 ]  . 
 accurate localization of parathyroid adenoma is valuable to * seyma yildiz drseymayildiz@gmail.com 1 department ofradiology , bezmialem vakif university , istanbul , turkey limit the extent of surgery with the goal of a unilateral small incision with minimal distortion of the normal anatomy , and fewer structures placed at risk . mri has been widely used in the evaluation of parathyroid disease . 
recently , diffusion - weighted mri has gained a widespread usage for diagnostic purposes due to its ability to provide a new contrast in evaluation of head and neck masses . 
the apparent diffusion vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 360367 coefficient ( adc ) , a measure of diffusion , is valuable quantitative metric , and helpful in distinguishing malignancy from benign lesions [ 5 ]  . 
the aim of this study was to evaluate the mri findings of solid parathyroid lesions and to elaborate on a possible improvement of mri detection of parathyroid lesions by the use of additional dwi . materials andmethods patients the surgeons in our institution prefer at least two imaging techniques to localize the parathyroid lesions before surgery to minimize the extent of surgery . 
twenty patients ( 4 men , 16 women , mean age 56 , 7years , range 3487years ) with hpt who underwent conventional mri for parathyroid pathology between august 2011 and january 2014 were enrolled . 
our institutional review board approved the study . mri examination all mri examinations were performed using a 1.5 t wholebody superconducting mri machine ( siemens , avanto , erlangen , germany ) with a head and neck coil . 
mean adc values ( b50 + b400 + b800 / 3 ) of the lesions were calculated automatically on images with b factors of 50 , 400 and 800s / mm2 , and adc values were expressed in square millimeters per second . image analysis one neuroradiologist ( aa ) reviewed the routine mri images only visually . 
at the same time , mean adc measurements were taken from normal appearing thyroid parenchyma ( tp ) , sternocleidomastoid muscle ( scm ) , jugulodigastric lymph nodes ( jdln ) and thyroid gland lesions ( tl ) for comparison with that of parathyroid lesions . 
the size of the rois was big enough to cover the interested area excluding outer borders of regions under evaluation . results of total 20 solid parathyroid lesion , 4 were parathyroid hyperplasia , 13 parathyroid adenoma and 3 parathyroid adenocarcinoma . 
however , similar to parathyroid adenoma and hyperplasia , parathyroid carcinomas had high diffusion properties compared to other soft tissue structures of head and neck region ( table2 )  . 
by increasing strength of diffusion tensor on dwi , all three types of parathyroid lesions still kept their brightness comparing other soft tissue structures of head and neck region because of their high t2 properties . 
however , scintigraphy has also imaging pitfalls since coexistent thyroid lesions , including hyperplastic thyroid nodules , chronic thyroiditis , hurthle cell lesions and adenomas , can retain radiotracer [ 13 ]  . recently , contrast - enhanced thin - collimation ct has been used for preoperative evaluation of patients with hpt . 
 [ 16 ] suggested multiphase ct as an ideal imaging method for preoperative evaluation hyperfunctioning parathyroid tissue because of its higher sensitivity than usg and scintigraphy ( 88% for ct , 21% for us , 54% for scintigraphy )  . 
1 af coronal fat - saturated t2 ( a ) , axial t2 ( b ) , fat - saturated t2 ( c ) , t1 ( d ) and postcontrast t1w ( e ) images demonstrate small , well - defined , homogenous , t2 bright and avidly enhancing nodular lesion within the posterior aspect of the thyroid gland on the right , suggesting parathyroid adenoma or hyperplasia . 
on dwi views , comparing to the nearby structures , parathyroid lesion keeps its brightness as the strength of tensor increases on dwi images due to its high t2 content . 
spectct is more informative by giving the exact anatomical localization of the lesion in major ectopic lesions and distorted neck anatomy [ 17 ]  . although less commonly used for preoperative evaluation of patients with hpt than other modalities , the 1 3 364 la radiologia medica ( 2019 ) 124 : 360367 fig . 
2 af coronal fat - saturated t2 ( a ) , axial t2 ( b ) , fat - saturated t2 ( c ) , t1 ( d ) and postcontrast t1w ( e ) images demonstrate large , illdefined , heterogeneous , infiltrative , t2 bright and enhancing lesion in the posterior and inferior aspect of the thyroid gland on the left , suggesting parathyroid adenocarcinoma . 
on dwi views , comparing to the nearby structures , parathyroid lesion keeps its brightness as the strength of tensor increases on dwi images due to its high t2 content . 
surgical result was reported as parathyroid adenocarcinoma reported sensitivity of mri , including both patients who have undergone surgery and patients who have not , is 4288% [ 6 , 9 , 11 , 18 , 19 ]  . 
also multiparametric mr perfusion can distinguish ptas from adjacent thyroid tissue or lymph nodes with a highly diagnostic accuracy . images of the neck are generally obtained from the skull base to the sternal notch . 
the imaging characteristics of parathyroid adenomas are most commonly hypo - to - isointense on t1w and high intensity on t2w conventional imaging [ 3 , 4 , 21 ]  . 
another potential pitfall in the detection of the parathyroid adenomas is the presence of associated thyroid disease which may be present approximately in % 30 of patients with hpt [ 23 ]  . 
however , false - negative results are most commonly associated with adenoma that is isointense on t1 and t2w sequences ; the addition of contrast - enhanced images can increase the sensitivity in these cases [ 18 ]  . parathyroid carcinoma is a rare malignancy developed from the parenchymal cells of the parathyroid glands . 
the mri characteristics of parathyroid adenocarcinoma have not been described well in the literature . in our study group , small sized , well - defined borders , t2 brightness , increased diffusion and homogenous appearance on t1 , dwi , t2 and postcontrast t1w images were properties of parathyroid hyperplasia and parathyroid adenoma . 
large sized , ill - defined borders , t2 brightness and heterogeneity on all sequences including t1 , t2 , dwi and postcontrast t1w images were properties of parathyroid adenocarcinoma . 
when evaluating dwi with increasing diffusion strength ( b50 , 400 , 800 ) , parathyroid lesion keeps their brightness longer on images when comparing with other soft tissues structures ( tp , jdln , tl ) of head and neck region . 
our results were in concordance with the literature . routine conventional mri is useful examination for parathyroid pathologies and helpful in differentiation of benign lesions from malignant ones , but it has disadvantages of high cost and longer examination . 
diffusion properties of parathyroid hyperplasia , parathyroid adenoma and parathyroid adenocarcinoma are higher than that of nearby structures ; this feature makes them easily differentiate from adjacent structures but the overlap of measured adc values of all three parathyroid lesions is too wide to enable differentiation from each other . in conclusion , mri is very successful in demonstration of parathyroid lesions . 
 solid parathyroid lesions , whether being parathyroid hyperplasia , parathyroid adenoma or parathyroid adenocarcinoma , have higher diffusion properties comparing the other soft tissues structures of head and neck region . 
this feature enables us to easily differentiate solid parathyroid lesions from nearby structures on fat - saturated t2w and dwi . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . informed consent our studies is retrospective . 
the results of imaging evaluation were compared with surgical findings , considered as reference standard . results during the study period , 124 patients operated on for anal fistulas underwent complete preoperative imaging assessment . 
the fistulas were classified as simple in 68 / 126 ( 53.9% ) and complex in 58 / 126 ( 46.03% ) cases , according to fistulas parks classification and the most recent american guidelines . 
in both simple and complex anal fistulas , 3d - eaus did not show a significantly higher accuracy in the evaluation of internal openings , if compared with mr ( p = 0.47 ; mcnemars chi - square test )  . 
in the complex anal fistulas , mr showed a significantly higher accuracy in the evaluation of secondary extensions if compared with 3d - eaus ( p = 0.041 ; mcnemars chi - square test ) , whereas in the simple anal fistulas , no significant difference was found . conclusion in the preoperative work - up of patients with anorectal fistulas , 3d - eaus may represent the first - line diagnostic tool . 
vanvitelli , piazza miraglia 2 , 80138naples , italy 3 department ofsurgery , villa esther hospital , via due principati 169 , 83100avellino , italy 4 department ofsurgery , pellegrini hospital , asl na1 centro , via portamedina alla pignasecca 41 , 80134naples , italy 5 department ofsurgery , university ofcampania l . 
exclusion criteria included age less than 18 , refusal to participate in the study , absolute contraindication to surgery or to mr and anal stenosis precluding the execution of 3d - eaus . all patients who met these criteria were preoperatively assessed by anamnestic evaluation , clinical examination , 3d - eaus and mr . clinical examination and 3d - eaus were performed , respectively , by a colorectal surgeon and a radiologist together with the same surgeon . mr examinations were evaluated in consensus by two radiologists ( fi and ar ) with 4 and 11years of experience in the pelvic imaging . surgery was performed by another colorectal surgeon blinded to 3d - eaus and mr results . the local ethical committee approved the study protocol . 
all patients gave written informed consent . clinical examination clinical examination included anamnesis , combined inspection and palpation of perineal area and anorectal digital examination , to evaluate the swellings and tenderness of perineal area and the suspected external and internal openings . 
the injection of the h2o2 through the external orifice allows a better depiction of the fistula tract that appears hyperechoic ( arrows ) : a axial plane , b sagittal plane fig . 
after an initial localizer in the three different planes , the study protocol starts with the following sequences including the small pelvis , the perineum and the gluteal regions ( table1 ) : axial tse t1 - w ; axial tse t2 - w ; and sagittal tse t2 - w . 
the use of fat saturation avoids the use of intravenous contrast medium as active fistula tracts appear spontaneously hyperintense , thus allowing a detailed evaluation of the fistula anatomy [ 9 , 25 ]  . 
 examination underanesthesia ( eua ) surgery was performed under subarachnoid anesthesia with patients in the lithotomy position . in the presence of suspected external orifices , lockhartmummery fistula probes and h2o2 were used to search for the fistula tracks and identify the internal openings . 
all the abscesses were incised and evacuated . the site and number of external openings , the site of internal openings and the anatomic relationship between fistulas or abscesses and anorectal musculature were examined and recorded . based on the parks classification [ 24 ] , and on the ascrs ( american society of colorectal surgeons ) guidelines [ 3 ] , the anal fistulas with intersphincteric and low transsphincteric primary tracks ( crossing < 30% of the external sphincter ) were classified as simple , whereas the anorectal fistulas with high transsphincteric ( crossing < 30% of the external sphincter ) , suprasphincteric and extrasphincteric primary tracks were considered complex . the anterior fistulas in women , the horseshoe fistulas and those associated with malignancy , ibd and radiation were also classified as complex disease . statistical analysis values are expressed , according to distribution , as mean standard deviation ( sd ) or medians and range . 
 prevalence data were compared between groups using the fishers exact test , whereas continuous data were compared between each group using the student t test or the mannwhitney u test , when indicated . the concordance between 3d - eaus and eua in defining the anorectal fistulas severity was evaluated through the simple kappa coefficient ( k )  . 
the diagnostic value in the identification of primary tracks did not show any difference . in table3 the 3d - eaus and mr sensitivity and specificity in the detection of simple fistulas internal openings , primary tracks and secondary tracks are compared . 
 although 3d - eaus showed higher sensitivity in the detection of internal openings and mr exhibited higher sensitivity in the detection of secondary extensions , no significant differences were found . table4 shows the 3d - eaus and mr sensitivity and specificity in the detection of complex fistulas internal openings , primary tracks and secondary extensions . 
 discussion although 3d - eaus and mr are generally considered useful tools in the preoperative evaluation of anorectal fistulas , the specific role of each imaging technique is still not well clarified and their weight in the different anorectal sepsis severity grades is still a matter of debate . in this study we evaluated the role of both diagnostic imaging techniques in the simple and complex perianal sepsis . first of all , our results suggest an excellent agreement between 3d - eaus and surgery in defining the anorectal sepsis severity . 
according to previous studies [ 1923 ] , this finding seems to encourage the routine use of 3d - eaus in the preoperative evaluation of patients with anorectal fistulas , with the aim to support the surgeon in planning the more appropriate therapeutic strategy . overall , our data show high and comparable sensitivity and specificity of 3d - eaus and mr in the evaluation of fistulas primary tracks , internal openings and secondary extensions . 
however , the diagnostic value of the two imaging techniques showed some differences depending on the sepsis severity grade . particularly , in the cases of fistulas classified as simple on the basis of assessment with 3d - eaus , the accuracy of mr in the detection of internal openings , primary tracks 1 3 la radiologia medica ( 2019 ) 124 : 339349 fig . 
therefore , in the simple fistulas , the additional mr evaluation did not provide substantial advantages , over ultrasound study , in the definition of fistulas anatomy . however , in the cases of fistulas graded as complex by 3d - eaus , mr showed a significantly higher accuracy in the evaluation of secondary extensions if compared with ultrasound , proving a definite advantage , over 3d - eaus alone , in the study of fistulas complete morphology ( figs.4 , 5 , 6 )  . although the reasons for this different accuracy cannot be inferred from the reported data , it is plausible that the secondary extensions of complex fistulas tend to be more numerous and distant from the anus and rectum 1 3 346 la radiologia medica ( 2019 ) 124 : 339349 fig . 
williams jg , farrands pa , williams ab , taylor ba , lunniss pj , sagar pm , varma js , george bd ( 2007 ) the treatment of anal fistula : acpgbi position statement . 
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reginelli a , mandato y , cavaliere c , pizza nl , russo a , cappabianca s , brunese l , rotondo a , grassi r ( 2012 ) threedimensional anal endosonography in depicting anal - canal anatomy . 
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siddiqui mr , ashrafian h , tozer p , daulatzai n , burling d , hart a etal ( 2012 ) a diagnostic accuracy meta - analysis of endoanal ultrasound and mri for perianal fistula assessment . 
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ognibene nm , basile m , di maurizio m , petrillo g , de filippi c ( 2016 ) features and perspectives of mr enterography for pediatric crohn disease assessment . 
foti pv , farina r , coronella m , palmucci s , ognibene n , milone p , conti bellocchi c , samperi l , inserra g , laghi a , ettorre gc ( 2015 ) crohns disease of the small bowel : evaluation of ileal inflammation by diffusion - weighted mr imaging and correlation with the harveybradshaw index . 
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buchanan gn , halligan s , bartram ci , williams ab , tarroni d , cohen cr ( 2004 ) clinical examination , endosonography , and mr imaging in preoperative assessment of fistula in ano : comparison with outcome - based reference standard . 
these patients underwent planning ct ( pct ) for radiation therapy ( rt ) and contrast - enhanced three - dimensional fast - spoiled gradientecho image ( 3d fspgr ) to assist tumor delineation . 
hypofractionated stereotactic radiotherapy ( hsrt ) with 3 or 5 fractions is the preferred mode of radiotherapy treatments for non - removable vs , where the gross tumor volume is bigger and / or of irregular shape [ 1 , 2 ]  . 
in mr - only planning , the image registration between ct and mr scans is eliminated , and at the same time , one can get rid of the radiation exposure as a result of a ct scan . radiation therapy planning ( rtp ) depends on threedimensional ( 3d ) computed tomography ( ct ) for dose calculation . 
significant development in treatment planning systems for past two decades has led to the generation of 3d dose color wash overlapped on the patient ct images at all three planes . 
many countries still depend on ct - based planning , and mri primarily assists in delineation of targets and critical structures , where appropriate mr sequence is registered to the planning ct ( pct ) images . 
ct scans are assumed to be geometrically accurate , but in case of mri , there might be geometric imperfections due to main and gradient magnetic fields and / or due to distribution of magnetic susceptibility values with biological tissues [ 11 ]  . there are quite a few studies that have employed mr images for radiation planning . 
 autosegmentation of structures from one or more mr sequence ( s ) was developed where 3d - pseudo - ct is generated and used for subsequent radiation planning [ 1315 ]  . 
 this study is one of a kind where bulk densities are assigned mainly to three structures ( bone , air , and soft tissue ) , derived directly from mr images . 
our aim is to compare the dose calculation accuracy of plans done on planning ct image and ct - value - assigned mr image . materials andmethods patient selection the scientific and ethics board has approved this work . 
ultra - fast - spoiled gradient - echo image sequences use a small flip angle and very short repetition time and optimized k - space filling to reduce the overall acquisition time . 
fspgr image is registered with the ct image using rigid registration algorithm version 11.0 ( varian medical systems , palo alto , usa )  . automatic registration is done using 3d coordinate system and it is followed by manual correction and verification by the oncologists for valid image fusion . 
treatment planning was performed for 6 mv beams on clinac - ix linear accelerator equipped with 120 leaves millennium multi - leaf collimator and with eclipse treatment planning software ( varian medical systems , palo alto , usa ) by senior clinical physicists . 
the dose calculation grid size greater than 2mm gives a dose difference of 2.3% of the prescribed dose for imrt treatments as compared with 1.5mm especially in high - dose gradient areas [ 16 ]  . 
as the image registration is already performed , the structures , the treatment plan along with optimization parameters , and priorities are copied from pct and pasted on fspgr image set . 
in this study , the fspgr image set is assigned hounsfield units ( hu ) values for three structures created viz : bone = + 1000 , air = 1000 , and body ( soft tissue ) = 25 . 
the corresponding mass densities recommended by icru 46 [ 17 ] are 1.61g / cm3 for bone , 0.001g / cm3 for air cavities and 1.025g / cm3 for average soft tissue . 
figure1 shows the comparison of 50% isodose coverage of plans generated on ( a ) planning ct ( b ) mrct without optimization and ( c ) mrct with optimization . evaluation parameters parameters such as conformity indices ( ci ) , max dose ( dmax ) to brainstem ( bs ) , and dose received by 0.5cc of brainstem ( d0.5cc ) were chosen for evaluation of the quality of plans generated . 
gamma agreement index ( gai ) and correlation coefficient ( r ) are used to predict the agreement of plans generated on mrct versus pct using omnipro imrt quality assurance ( qa ) software ( iba dosimetry , gmbh , germany )  . 
the extent of correlation coefficient varies between minus one and plus one , i.e. , 1 0 1 where r = 1 indicates perfect inverse correlation , while r = + 1 indicates perfect direct linear correlation between two variables [ 19 ]  . 
detailed descriptions of characteristics of parameters selected for evaluation are found in table2 with respect to hsrt treatments . single - factor analysis of variance ( anova ) test is carried out to find the statistically significant difference between the plans generated on ctplan , ddc and opt_dc . 
if p value < 0.05 , we reject the null hypothesis and conclude that there is a significant difference between the parameters generated from plans . results the metrics mentioned in table2 are applied to the extracted data and the results of deviation of ddc and opt_dc of mrct from original plan done on pct are obtained . 
the range and mean deviation values of dmax and d0.5cc of bs for ddc versus ctplan and 1 3 la radiologia medica ( 2019 ) 124 : 400407 table 2 evaluation parameters parameter conformity of prescribed dosea dose to the brainstem ( bs ) ( 5fx hsrt ) ( endpointcranial neuropathy ) b gamma agreement index ( gai ) correlation coefficient ( r ) a rtog 0915 b aapm task group 101 description / dose constraint 1 . 
 ci1 - ratio of the prescription isodose volume to the planning target volume ; ctplanplans done on planning ct ; ddcplans dose on mrct without optimization ; opt_dcplans done on mrct with optimization opt_dc versus ctplan are given in table4 . 
the dosimetric verification of mr versus ct - based planning for prostate patients using intensity modulated radiation therapy has been validated by chen etal [ 8 ]  . in this study , the delivered fluences of ddc and opt_ dc were not acquired / analyzed and compared only with approved plans ( calculated fluences ) done using ctplan . 
this criterion is sufficient since the treated plans done using pct passes the routine qa procedures of hsrt treatments.1 the mean values of ci2 are not relevant and not discussed here since the passing criterion of ci2 value falls under a range of value and are different for different ptv volumes2 . 
it is inferred from fig.1 that the plans done on mrct with and without optimization are qualitatively similar to those plans done on pct and statistically proved with anova test . 
the differences in dose volume patients considered under this study , bs lies in close proximity to the ptv and in addition hsrt involves delivering unusually high dose per fraction of 5gy ( steep dose fall off )  . 
4 dose color washes in coronal plane in omnipro imrt software for a original ct b ddc and c opt_dc deviation may also because of mild / negligible peripheral distortions from mr image set as the soft tissue structure ( body ) is created using mr image set . 
this is also evident from the anova tests where p value is > 0.05. the location of tumors in this study is in the region of hetero - density area ( cp angle )  . 
also generation 1 3 406 la radiologia medica ( 2019 ) 124 : 400407 compliance with ethical standards conflict of interest all authors contributed to this study declare that they have no conflict of interest with respect to the manuscript . ethical standards institutional scientific and ethics board has approved this study . 
comparing with hydrocephalus , the width of prepontine cistern ( ppc ) / the width of aqueductus sylvii ( as ) was significantly higher and other csf metrics with standardized systolic and sum of systolic and diastolic flow durations were significantly lower . 
compared with normal group , ppc / as and reverse / forward flow duration were significantly lower and other csf metrics were significantly higher . conclusion in hydrocephalus , significant increase in asv and peak velocities were noted . 
communicating hydrocephalus could be with obstruction to csf absorption secondary to subarachnoid bleeding , leptomeningeal carcinomatosis or infective meningitis or could be without obstruction to csf absorption such as in normal pressure hydrocephalus , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 382391 hydrocephalus ex - vacuo or colpocephaly secondary to parenchymal volume loss or in choroid plexus papillomas due to overproduction of csf . 
most common imaging findings of hydrocephalus are : ventriculomegaly ( evans index > 0.3 ) , enlargement of the third ventricular recesses and lateral ventricular horns , decreased mamillopontine distance and frontal horn angle , thinning and elevation of the corpus callosum , normal or narrowed cortical sulci , periventricular white matter hyperintensities due to interstitial edema and aqueductal flow void phenomenon in t2w images . 
in csf flow studies , dilated aqueductus sylvii and increased asv may be seen [ 1 , pseudotumor cerebri or iih is a disorder of unknown etiology that is characterized by elevated intracranial pressure , usually occurs in obese women in the childbearing years [ 35 ]  . 
there is no evidence of deformity or obstruction of the ventricular system , and neurodiagnostic studies are otherwise normal except for increased cerebrospinal fluid pressure ( greater than 200mm of water in the non - obese and probably greater than 250mm of water in the obese patient )  . 
mri findings of iih are widening of perioptic subarachnoid space , optic nerve tortuosity , posterior scleral flattening , preliminary enhancement of optic nerves , empty sella , tonsillar herniation , perimesencephalic cistern obliteration , shrinkage of ventricles , enlargement of meckels cave and bilateral transverse sinus compression [ 6 ]  . 
in the literature , only one study was present detailing csf flow metric in iih suggesting statistically decreased peak flow velocity in untreated iih patients [ 4 ]  . with recent advances on mri , mri is not only beneficial in the diagnosis of csf - related diseases , but also helps clinicians in planning the treatment and follow - up of patients . 
new mri sequences including phase - contrast magnetic resonance imaging ( pc - mri ) , 3d - heavily t2w ( 3d constructive interference in steady state ) ( 3d - ciss ) and 3d sampling perfection with application - optimized contrasts using different flip angle evolutions ( 3d - space ) enable evaluation of csf - related pathologies with higher sensitivity and specificity . 
this study is retrospective casecontrol observational study , and our purpose is to evaluate csf dynamics of iih and communicating hydrocephalus and search for any correlation between mri findings , csf metrics and csf opening pressure in iih . materials andmethods subjects twenty - nine patients ( average age 37.28 , m / f 2 / 27 ) ( age range 1857years ) with a diagnosis of iih and 43 patients ( average age 29.12 , m / f 23 / 20 ) ( age range 1178years ) with a diagnosis of high - pressure communicating hydrocephalus based on standard clinical and laboratory criteria , referred from our neurology department , were included . 
 cases with normal pressure hydrocephalus , hydrocephalus ex - vacuo or colpocephaly secondary to parenchymal volume loss or hydrocephalus due to overproduction such as in choroid plexus papilloma were all excluded . 
control group included 30 healthy volunteers ( average age 36.57 , m / f 25 / 5 ) ( age range 2065years ) , with normal neurological examination , clinical and laboratory findings . 
for all patients in this study , a detailed history , neurological examination and laboratory findings were retrospectively evaluated in our hospital via computer - based archive systehealthy volunteers also underwent csf flow study . 
all subjects were fully informed and gave their written informed consent . imaging technique mri was performed on a 1.5 tesla system ( avanto ; siemens medical solution , erlangen , germany ) using head coil . 
mean modulus , magnitude of complex difference and directional phase difference images perpendicular to the cerebral aqueduct in the sagittal plane were then obtained at the semi - axial plane . 
1 axial images acquired perpendicular to ampulla la radiologia medica ( 2019 ) 124 : 382391 1430 cardiac phase sections according to heart rate were : tr : 31.25ms , te : 8.06ms , slice thickness : 3mm , nsa : 1 , fov : 16 10cm , matrix 128 256 and flip angle , 10 . 
flow in the caudocranial direction ( diastolic or reverse flow ) was identified as negative , and flow in the craniocaudal direction ( systolic or forward flow ) was identified as positive . 
 parameters used for 3d - t2 ciss were : slice thickness : 1mm , fov : 200mm , matrix 290 320 , tr : 6.06ms , tr : 2.61ms and flip angle 70 . 
parameters used for 3d - t2 space were : slice thickness : 1 mm , fov : 240 mm , matrix 231 256 , tr : 2500 and tr : 501 . mri analysis the images obtained from all subjects ( subjects with iih , subjects with hydrocephalus and healthy subjects ) were evaluated by two separate radiologists ( aa and tfy ) using the siemens user console ( argus software , siemens , erlangen , germany )  . 
on midline sagittal t2 ciss images , at the midpontine level , width of prepontine cistern ( ppc ) and width of cerebral aqueductus sylvii ( as ) were measured and ppc / as ratio was calculated . 
velocity versus time , peak flow velocity versus time ( fig.3 ) , flow versus time and net flow versus time curves of the flow passing through the as during one cardiac cycle were obtained . 
systolic ( arrow on a ) and diastolic durations ( arrow on b ) are shown volume ( l ) , net forward flow volume ( l ) , asv ( aqueductal stroke volume ) ( l ) , as area ( mm2 ) , ppc / as ratio , the average flow volume in one cardiac cycle ( ml / min ) , systolic and diastolic flow times ( ms ) , standardized ( by heart rate - 60 beats / min ) systolic and diastolic flow times ( ms ) , the ratio of diastolic and systolic time , the sum and difference of systolic and diastolic flow times ( ms ) and the sum and difference of standardized systolic and diastolic flow times ( ms ) were calculated . 
the average volume flow in one cardiac cycle was calculated by the formula : forward volume + reverse volume / range ( 0680ms ) 60ml / mthe asv was calculated by the formula : forward volume + reverse volume / 2 . 
 positive values of peak flow velocity were recorded . in iih patients , accompanying conventional mri and mr venography findings including empty sella , optic nerve sheath edema , posterior scleral flattening , perimesencephalic cistern obliteration , shrinkage of ventricles , enlargement of meckels cave , tonsillar herniation and transverse sinus compression were also noted . statistical analysis all statistical analyses were performed using spss for windows version 23.0 software package ( ibm corp . , new york , ny ; formerly spss inc . , chicago , il )  . 
subjects were evaluated in three separate groups : group with communicating hydrocephalus ( n = 43 ) , group with iih ( n = 29 ) and group with healthy volunteers ( n = 30 )  . 
for each three groups , mean standard deviation of frequently used csf flow metrics ( asv , average volume flow in one cardiac cycle , and peak flow velocities ) was calculated . first , distribution of variables from three groups was evaluated by using shapirowilk normality test . 
when sum of standardized systolic and diastolic flow time was evaluated , a significant difference between healthy subjects and hydrocephalus was not present ( p = 0.382 ) , [ median values in healthy group , 636ms ( minimum 374ms , maximum 821ms ) / hydrocephalus , 618ms ( minimum 324ms , maximum 807ms ) ]  . 
a statistically significant difference was not determined in other csf flow metrics between two groups ( table2 )  . in patients with iih , there was no correlation of empty sella , optic nerve sheath edema , posterior scleral flattening , perimesencephalic cistern obliteration , shrinkage of ventricles , enlargement of meckels cave , tonsillar herniation , transverse sinus compression and ppc / as ratio with asv values . 
among conventional mr and mr venography findings including ppc / as ratio and asv , there was only statistically significant difference in csf opening pressure between iih patients with transverse sinus compression and iih patients without transverse sinus compression . 
aqueductal stroke volume ( asv ) , a flow metric , is the average of forward flow volume during systole and reverse flow volume during diastole in each cardiac cycle . 
however , location of axial views of pc - mri in our study was through ampulla of as , which is widest and middle - third area of as . normal csf flow at the level of as and foramen magnum is biphasic due to pump mechanissystolic expansion of intracranial vessels and brain parenchyma results in csf movement from ventricular system toward the spinal canal ( craniocaudal flow , systolic csf flow , forward flow ) , while diastolic contraction of intracranial vessels and brain parenchyma results in reduction in intracranial pressure and secondary csf movement from spinal region to subarachnoid space and ventricular system within the brain ( caudocranial flow , diastolic flow , reverse flow )  . in this study , we measured diastolic flow time in iih and healthy subjects . 
in iih comparing with healthy subjects , standardized diastolic flow time ( median value in iih , 395ms / healthy subjects , 484ms ) and difference between standardized diastolic and systolic flow time ( median value in iih , 206ms / healthy subjects , 289ms ) and sum of standardized systolic and diastolic flow times ( median value in iih 542ms / healthy subjects 636ms ) were found statistically significantly short . 
comparing the sum of standardized systolic and diastolic flow times among three groups , it was statistically shortest in iih ( median value in healthy subjects 636ms , hydrocephalus 618ms , iih 542ms ) , but not statistically significant difference noted between hydrocephalus and healthy subjects . 
in iih , we also observed abnormal csf flow pulsatile resulting from attempt to flow against the increased pressure . ct and mri findings in patients with iih are dilated optic nerve sheath , empty sella , posterior scleral flattening , prelaminar optic nerve enhancement , vertical tortuous appearance of orbital optic nerves , enlargement of meckel cave and rarely tonsillar herniation . 
 in a study of diyvata etal . , mri findings were found similar in both iih and secondary intracranial hypertension [ 15 ]  . they reported that optic nerve head protrusion and posterior scleral flattening were significantly associated with iih with no statistically significant difference found in the occurrence of rest of the findings . 
they suggested that clinical features , not the degree of stenosis , should be used to determine management in iih . in our study , we compared csf opening pressure and csf flow metrics with cranial mri and mr venography findings . 
in our study , in comparison with as area and ppc / as ratio , there was no significant difference between patients with iih and healthy subjects but a statistically significant difference was found between hydrocephalus and other two groups . 
this led to a statistically significant decrease in ppc / as ratio in hydrocephalus 1 3 390 la radiologia medica ( 2019 ) 124 : 382391 compared to two other groups . 
in the present study , we found statistically significant increase in asv , peak flow velocity , forward flow volume , reverse flow volume , net forward flow volume , forward flow velocity , reverse flow velocity and average flow volume in one cardiac cycle in hydrocephalus , compared to healthy subjects . high asv values in hydrocephalus are due to increased csf volume and increased as area . 
however , only statistically significant difference was found between patients with hydrocephalus and iih . in comparison with asv values of all three groups , a significant increase in asv was detected in hydrocephalus , whereas no significant difference between iih and healthy subjects ( median asv 180l in hydrocephalus , 15l in iih and 21.2l in healthy subjects )  . 
the average flow volume in one cardiac cycle showed similar ranking ( median value 31.76ml / min in hydrocephalus , 2.6ml / min in iih , and 3.7ml / min in healthy subjects )  . 
asv shows the volume of csf passing through as , and it has a positive correlation with area of as and volume of csf within the lateral and third ventricles . 
we thought that these findings were expected effects of decreased intraventricular csf volume as well as increased intracranial pressure . conclusion csf flow dynamic is so complex , and pathways of csf production and absorption are still speculative . 
this mainly comes from shortening in diastolic flow duration that is probably effects of increased impedance of csf flow against increased intracranial pressure and unchanged or even decreased intraventricular csf volume . 
in conclusion , csf flow dynamic is not fully understood ; further , more detailed , larger - scale studies should be performed to reveal the role and variability of csf flow in diseases . authors contribution tfy and ht contributed to data collection , data archiving , manuscript writing ; aa was involved in project development , data collection , data archiving , manuscript writing ; em contributed to data collection , data archiving ; gk , neurologist , took care of the patients ; sk and aa were involved in project development ; mok contributed to biostatistical analysis . compliance with ethical standards conflict of interest the authors have declared no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
restoring the normal alignment and articular congruity after a distal radius fracture is important in order to obtain good functional results [ 2 , 3 ] , in addition to preventing the development of osteoarthritis [ 4 ]  . 
open * alessandro stecco a.stecco@libero.it 1 radiology institute , services diagnosis andtherapies department , maggiore della carit hospital , university ofeastern piedmont upo university , corso mazzini 18 , 28100novara , italy 2 orthopaedics andtraumatology department , maggiore della carit hospital , university ofeastern piedmont , novara , italy 3 medical physics department , maggiore della carit hospital , university ofeastern piedmont , novara , italy reduction and internal fixation ( orif ) with plates and screws has been demonstrated to be effective in the treatment of unstable distal radius and ulnar fractures [ 5 ]  . magnetic resonance imaging ( mri ) is a useful tool to study the most common complications associated with plating . 
however , metallic implants can cause significant image distortion in mri and are known to interfere with the accurate identification of fractures , infections and recurrent tumours surrounding an implant , or even loosening of the implant [ 5 ]  . two mri techniques have been implemented in order to reduce metal - induced artefacts : the view angle tilting ( vat ) technique and the higher readout bandwidth ( hibw ) technique [ 611 ]  . 
in our department , we have a dedicated low - field mri scanner with metal artefact reduction ( mar ) sequences , which was applied in the study of distal radius and ulna fractures treated with volar plating . the purpose of this study was to compare these two optimised mar sequences in their efficiency in reducing vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 392399 metallic artefacts , using a low - field mri scanner . 
to our knowledge , this is the first study to evaluate the role of mar sequences in wrists after plating using a dedicated low - field mri scanner . materials andmethods patients we evaluated 21 patients who underwent mri from november 2014 to march 2016 at our institution . 
ten patients underwent an mri due to pain , one due to a dorsal wrist tumefaction ( suspicion of a ganglion cyst on ultrasound ) and five due to a slight decrease in range of motion . one patient had extensor digitorum communis tendon rupture , four had a partial scapholunate ligament tear , one had a luno - triquetral ligament tear , one had an extensor digitorum communis tenosynovitis , one patient had an extensor carpi ulnaris tendon ganglion cyst , one had a trapeziometacarpal osteoarthritis , one had carpometacarpal osteoarthritis , and two patients had a triangular fibrocartilage complex ( tfcc ) lesion ( one patient with a 1a and one with a 1d lesion , according to the palmer classification [ 13 ] )  . 
the patients had been treated with a 2.4mm variable angle locking compression plate ( lcp ) two - column volar distal radius plate ( depuy synthes , johnson & johnson , west chester , pa , usa )  . 
patients gave their consent prior to mri , and as the study was retrospective in nature , approval from the local ethics committee was not sought . magnetic resonance imaging sequences all patients were examined using a dedicated 0.3t scanner ( o - scan , esaote , italy )  . 
coronal fse t2 vat sequence ( 4460 / 96 ; 3mm section thickness , 0.3 gap , 512 512 field of view , 12ms echo spacing , 9 echo train length , 15 sections , 5min 21s acquisition time )  . our protocol usually also contains standard axial fse t2w , axial se ( spin echo ) t1w , coronal stir ( short - tau inversion recovery ) and coronal gradient - echo ( gre ) t1 sequences ; however , these were not analysed in this study . 
the artefacts volumes were then , after rois manual tracing , automatically calculated using the measure stack plugin ( available at av.com / measu resta ck.htm ) , which performed measurements on a series of distinct regions of interest ( roi ) in the slices of a stack . 
after entering the slice spacing ( section thickness , thus 3mm ) , the results were summed to determine the total volume of the artefact . the two components of teams reader 1 and reader 2 collaborated in consensus to perform and validate , in a doublereading fashion , the measurements of cumulative areas of the signal voids and artefacts on standard and mar images . this type of work does not require approval by ethics committee , because of the retrospective nature of the study , 1 3 394 la radiologia medica ( 2019 ) 124 : 392399 but before all diagnostic exams patients received and signed informed consent . statistical analyses cohens k value . 
quantitative statistics were used to compare the signal void ( black artefact ) and artefact distortion ( bright artefact )  . a preliminary testretest statistical evaluation has been carried out by the two equipes of raters ( reader 1 and reader 2 ) , who performed independently multiple measurements ( 10 ) on the same predefined area of artefact , in the same randomly selected data set among the case series . 
1 standard coronal fast spin echo ( fse ) t2 , b coronal fse t2 optimised with high bandwidth ( fse - hibw ) and c coronal fse t2 view angle tilting ( vat ) sequences . 
single manually drawn regions of interest ( roi ) were then summed , and the total volume was calculated 1 3 la radiologia medica ( 2019 ) 124 : 392399 fig . 
2 standard coronal fast spin echo ( fse ) t2 , b coronal fse t2 optimised with high bandwidth ( fse - hibw ) and c coronal fse t2 view angle tilting ( vat ) sequences . 
3 standard coronal fast spin echo ( fse ) t2 , b coronal fse t2 optimised with high bandwidth ( fse - hibw ) and c coronal fse t2 view angle tilting ( vat ) sequences . 
 open reduction and internal fixation ( orif ) with plates and screws is considered to be the most effective treatment for displaced and unstable fractures.. the most common complications associated with volar or dorsal plating are a loss of reduction after plate fixation , irritation of the median nerve [ 5 ] and lesions or irritation of the extensor or flexor tendons . 
many of these complications are related to the features of the device ( thickness , shape , screws or material ) or the surgical approach and technique . rupture or irritation of the extensor tendons is the most frequent problem associated with the dorsal approach . 
carpal tunnel syndrome has also been associated with volar plating [ 18 , 22 , 23 ] ; however , this may occur in distal radius fractures regardless of the treatment method used . 
the inhomogeneity correction arises from the additional tilting gradient in the slice - select direction , so that the slice is effectively viewed at a tan1 ( gz / gx ) angle . 
 when viewed at this angle , shifts in the slice - selection plane compensate for shifts during readout , such that plane shifts are re - registered in the images . 
however , vat images are prone to blurring in the frequency - encoding direction , which has hindered the widespread use of this technique [ 7 ]  . the hibw technique increases the resolution in the frequency - encoding direction [ 8 , 9 ]  . 
as the bandwidth ( pixels ) increases , the effects from the geometric distortion and intravoxel phase dispersion form a smaller proportion of the total signal , thereby reducing image distortion . 
 alternatively , the field of view ( fov ) could be decreased for the same image matrix , but this is not routinely performed because the anatomical region of interest would not be completely visible . 
the disadvantage of using stronger gradients for these measurements is a decrease in the signal - to - noise ratio ( snr ) [ 10 , 11 ]  . dedicated mri scanners are increasingly used to study extremities as they have many advantages over whole - body scanners . 
the main advantages of extremity scanners over whole - body high - field scannersare : decreased purchase and maintenance costs , lower weight , easier installation in a small space and faster patient diagnosis ( in the office setting )  . 
the installation of low - field mr scanners is also beneficial for interventional and intraoperative use . in our study , we observed a significant decrease in both the black and bright artefacts for the hibw and vat sequences . 
 [ 21 ] described seven patients who had lost fixation of a volar lunate facet fragment , with subsequent carpal displacement 1 3 398 la radiologia medica ( 2019 ) 124 : 392399 blurred which reduced the overall quality of the images . 
the poorer quality of images obtained by the vat sequence may make the evaluation of subtle alterations in small anatomical structures ( ligaments or tendons ) more difficult when compared to standard fse t2 and hibw sequences . on the other hand , bone is easily evaluated ; therefore , vat sequences could be used to obtain a more detailed evaluation of the bone surrounding the screws or metallic implants . 
in our opinion , hibw sequences represent a good compromise , both quantitatively and qualitatively , as it provides images of acceptable quality in addition to significant reduction in artefacts . this study has several limitations . 
another limitation of this retrospective study was that the patients were randomly chosen , and because of this , there was a wide range in the time between surgery and mri among the patients . 
 we were also unable to qualitatively assess the artefacts , even though our primary goal was to perform a quantitative analysis . more studies are required to verify the clinical impacts of these different sequences . 
due to the use of the drape , radiation exposure of primary operators abdominal area , genitals , thyroid and eye lenses was reduced by an average of 59% , 60% , 65% and 59% , respectively . 
however , dose area product ( dap ) and peak skin dose ( psd ) were increased by 20% when part of the drape was placed into the x - ray field . conclusion during evar and pta procedures , primary operators organs are exposed to considerable radiation doses . 
box2208 , 71003heraklion , crete , greece interventional radiology unit , department ofradiology , university hospital ofheraklion , medical school , university ofcrete , crete , greece 3 vascular surgery unit , department ofcardiothoracic andvascular surgery , university hospital ofheraklion , medical school , university ofcrete , crete , greece 4 department ofmedical physics , university hospital ofheraklion , medical school , faculty ofmedicine , university ofcrete , p.o. 
box2208 , 71003iraklion , crete , greece introduction atherosclerosis of aortoiliac arteries , abdominal aorta and below the knee arteries can cause intermittent claudication , gangrene , limb ischemia and loss of a limb [ 13 ]  . 
pta is the most common fluoroscopically guided intervention for the treatment of peripheral artery disease [ 4 ]  . the most frequent form of aortic aneurysm is the abdominal aortic aneurysm ( aaa ) [ 5 ]  . 
the procedures were performed by three experienced interventionalists . the following data were recorded for all patients : total fluoroscopy time , dap , psd and the number of digital subtraction angiography ( dsa ) series . 
positioning of the c - arm in left / right ( lao / rao ) direction was between 0 and 45 for both procedures . occupational doses in both procedures were determined using thermoluminescence dosimetry ( tld ) chips ( tld200 , hashaw , solon , oh )  . 
at the beginning of each procedure , tld chips were placed on the left side of the head , on the protective eyewear , over and underneath the thyroid collar , on chest level over and underneath the apron and on the middle finger of both hands of the primary operator . 
estimation of the effective dose with this algorithm is independent of aprons thickness . to evaluate the efficacy of a radioprotective drape , experiments were performed using two physical anthropomorphic phantoms ( rando - alderson research labs , ca , usa ) and a 0.25mm pb equivalent drape ( ecolab , saint paul , minnesota , usa )  . 
total fluoroscopy time and the number of dsa runs were the same for all simulations . statistical analysis statistical analysis was performed using prism software ( graphpad , ca , usa ) , and office excel ( microsoft , wa , usa )  . 
2 positioning of the drape in the first experiment ( left ) , second experiment ( middle ) , third experiment ( right ) results there was a statistically significant difference in fluoroscopy time ( p = 0.0008 ) and dap ( p < 0.0001 ) , between pta and evar procedures ( table1 )  . table 2 presents occupational doses of the primary operator , for evar and pta procedures , respectively . 
figures3 and 4 show the correlations between chest dose over the apron , right - hand dose , thyroid dose over the collar , eye lens dose and fluoroscopy time for the primary operator in pta and evar procedures . table3 presents the maximum number of evar or pta procedures an interventionalist can perform annually . 
the calculated maximum workloads were based on the annual effective dose limit and equivalent dose to the lens of the eye limit recommended by icrp as well as on median ed and eye lens doses presented in table2 . the results of this study show that the drapes significantly contribute to the operators radioprotection . 
specifically , radiation exposure of the abdominal area , genitals and thyroid , was reduced by an average of 59% , 60% , 65% , respectively , due to the use of the drape . 
on the contrary , differences up to 20% were noted when half of the drape was placed into the field ( table5 )  . discussion dap and fluoroscopy time are directly related with the radiation exposure of the interventionalists . 
4 correlations between different body parts doses and fluoroscopy time in evar procedures table 3 maximum permissible annual workload based on ed and eye lens doses procedure number of procedures ( based on ed ) number of procedures ( based on eye lens dose ) evar 4255 4545 1626 tabulated data ( table2 ) show that radiation exposure of the primary operator was higher in evar procedures than in pta procedures . 
based on the literature , hand doses of the interventionalists during pta procedures range from 21 to 190 sv [ 1315 , 23 , 24 ]  . eye lens doses during pta procedures have been evaluated by a number of studies [ 1315 , 2325 ]  . 
the wide range of these values indicates that several parameters including complexity of the procedures as well as the experience of the operator affect the radiation exposure of the interventionalists . 
further , a mean reduction up to 29% , 60% , and 60% , of the radiation exposure , was recorded for the right side of the head , the forehead and the left side of the head , respectively . 
these results are in agreement with the corresponding results presented in the literature [ 1517 ]  . the efficacy of the drape has been evaluated by a number of studies . 
specifically , dap and psd were 1 3 la radiologia medica ( 2019 ) 124 : 539545 increased by 20% when part of the drape was placed into the x - ray field . 
radiation dose increases when a drape is in the x - ray field because aec increases the exposure in an attempt to maintain image quality . our study has some limitations that should be considered . 
a patient study is needed to confirm the effect of the drapes positioning on aec . conclusion during evar and pta procedures , primary operators organs are exposed to considerable radiation doses . 
the non - contrast - enhanced scan sequences were performed with noise indexes ( nis ) of 11 , 14 , and 16 for the 0 to < 1 , 1 to < 3 , and 3 to < 6 year age groups , respectively . 
enhanced scan sequence : the ni default was 9 , and the data were subjected to the filtered back projection reconstruction algorithall other scanning parameters were the same as those used in the non - contrast - enhanced scan sequence . results in the 0 to < 1year group , the image qualities were scored as 3 or above with asir weights of 50% for the lung window and 40% for the mediastinal window ; in the 1 to < 3year group , the image qualities were scored as 3 or above with asir weights of 60% for the lung window and 50% for the mediastinal window ; in the 3 to < 6year group , the image qualities were scored as 3 or above with asir weights of 70% for the lung window and 60% for the mediastinal window . conclusion for low - dose chest ct scans of preschool - age children , application of the asir technique significantly improved image quality and reduced image noise . 
however , the reduction in tube potential increases image noise , decreases the signal - to - noise ratio ( snr ) , and influences the detection of subtle lesions . 
 as reported [ 8 ] , under the conditions of assured quality of ct reconstruction images and not influencing the diagnosis by the radiologist , asir allows 3265% reductions in x - ray radiation dosage compared with the traditional fbp . 
however , the use of an asir reconstruction technique with over - reduction in ct scan conditions may cause over - smoothing of images and mask some image information , which can affect the clinical diagnosis . 
to optimize the ct scan dose , it is required to explore the best asir ratios for different groups of people and in different scanning areas while practicing ct scans . currently , there are several reports on the study of applying asir on adult chest ct examinations , but there are fewer reports on the application of asir in childrens chest ct scans . 
this study aims to evaluate the combined application of asir and ni on the chest ct scans of preschool - age children . information andmethod this is a prospective study , this study was approved by the independent medical ethics committee of our hospital , and the family members of all children provided informed consent before the study . general information clinical pretest children who underwent ct non - contrast - enhanced and enhanced scans at our department due to clinical needs from june 2015 to june 2016 were included . 
slice thickness was 5mm with 5 - mm intervals , the field of view ( fov ) was small body , the pitch was 1.375 : 1 , the rotation time was 0.6s , and the matrix was 512 512 . 
for enhanced scans , the ni was set at 9 for all examinations , and all other scanning parameters were the same as in normal scan . interest ( roi ) was circular in shape . 
image snrs were calculated as follows : left ventricle snr = left ventricle ct value / erector spinae sd value , whereas the erector spinae snr = erector spinae ct value / erector spinae sd value . 
 all other scan parameters were the same as those used in the clinical pretest . data measurement data measurements were performed on the non - contrastenhanced chest ct images of the children . 
the ct and sd values of the left ventricle and erector spinae were measured from the slice with the maximum left ventricle area and the two slices above and below . 
the region of the ct dose index volume ( ctdivol ) and dose length product ( dlp ) of non - contrast - enhanced and enhanced ct scans for each group were recorded . 
 the k values were as follows : 0.0039msvmgy1cm1 for the 0 to < 1year age group , 0.0026msvmgy1cm1 for the 1 to < 3year age group , and 0.0018msvmgy1cm1 for the 3 to < 6year age group [ 9 ]  . 
the average of each group was calculated . subjective evaluation ofimage quality the 4 - point scale used in the chest ct image evaluation by the quality control team of the laboratory of the researchers was adapted . 
this scale was developed by the members of the quality control team through referencing high - impact studies in the literature and evaluation standards implemented in other pediatric hospitals with consideration of the conditions of our equipment [ 1015 ]  . 
the evaluation team was composed of an associate chief physician in the department of radiology and two radiology physicians with more than 5years of work experience . the images of the mediastinal window ( w280 , l70 ) and lung window ( w1300 , l - 500 ) taken from children in each group were evaluated by the two senior physicians using a 4 - point image quality evaluation scale with scan parameters concealed . 
b measurement of the anteroposterior and horizontal diameters on the slice with maximum area in the left ventricle 1 3 470 la radiologia medica ( 2019 ) 124 : 467477 points indicated good image quality with clear lesion and anatomical details ; 3 points indicated good image quality with clear illustration of most of the lesion and anatomical details except for a few images , which did not affect the diagnosis ; 2 points indicated poor image quality that could not satisfy the diagnostic requirements ; and 1 point indicated poor image quality that did not allow diagnosis . 
 the quantified parameters are expressed as x s . clinical pretest comparisons of the baseline data ( age , anteroposterior thoracic diameter , and axial thoracic diameter ) , subjective evaluation of image quality , scan radiation doses , image snr , and image noise of each patient group under different ni conditions were conducted with one - way analysis of variance ( anova )  . 
if the results were statistically significant , multiple comparisons were performed using the bonferroni method ; a value of p < 0.05 was considered statistically significant . clinical test : the subjective evaluation results of image quality , image snr , and image noise of the children using asir with different weights were examined using anova for repeated measurements . 
such a phenomenon was more apparent at the edges of the images ( table9 )  . for images of the group aged 0 to < 1year , the image qualities were scored as 3 and above with asir weights of 50% for the lung window and 40% for the mediastinal window . 
2 a six - month - old boy , lung window , asir weights of 40% , b six - month - old boy , mediastinal window , asir weights of 30% , c six - monthold boy , lung window , asir weights of 50% , d six - monthold boy , mediastinal window , asir weights of 40% , e six - month - old boy , lung window , asir weights of 60% , f six - month - old boy , mediastinal window , asir weights of 50% 1 3 la radiologia medica ( 2019 ) 124 : 467477 474 fig . 
3 a two - year - old girl , lung window , asir weights of 50% , b two - year - old girl , mediastinal window , asir weights of 40% , c two - year - old girl , lung window , asir weights of 60% , d two - year - old girl , mediastinal window , asir weights of 50% , e two - year - old girl , lung window , asir weights of 70% , f two - year - old girl , mediastinal window , asir weights of 60% for images of the group aged 1 to < 3years , the image qualities were scored as 3 and above with asir weights of 60% for the lung window and 50% for the mediastinal window . 
to reduce the effects of these differences , we divided preschool - age children into groups of 0 to < 1 , 1 to < 3 , and 3 to < 6years . 
stringent requirements were set for inclusion and exclusion of patients to assure the universality of the research results . in non - contrast - enhanced scan sequences , it is unknown whether the ct images obtained after adjusting the scan parameter ni could satisfy the diagnostic requirements . 
4 a four - year - old boy , lung window , asir weights of 60% , b four - year - old boy , mediastinal window , asir weights of 50% , c four - year - old boy , lung window , asir weights of 70% , d four - year - old boy , mediastinal window , asir weights of 60% , e four - year - old boy , lung window , asir weights of 80% , f four - year - old boy , mediastinal window , asir weights of 70% scan images were from children who also needed enhanced scans . 
in other words , if the quality levels of the non - contrast - enhanced ct images were reduced due to the increase in ni and the diagnosis was affected , the use of regular parameters in their enhanced scan sequence ensured a satisfactory image quality for diagnosis . 
with this method , the disadvantage of poor image quality obtained in a nonenhanced scan was overcome , and repetitive scans on children , which increase the radiation dose , could be avoided . in our study , dlp , ctdivol , and ed were considered as the indexes to evaluate the radiation dose in the ct examinations of children . 
the image reconstruction method implemented in our study was asir , which has been reported and demonstrated various advantages , such as effectively reducing image noise and increasing image quality [ 2228 ]  . the clinical pretest results showed that the choice of ni is crucial and directly affects the radiation dose and ct image quality of the children subjected to ct scans . 
the optimal ni value increased with the age of the child and thus varied for different age groups as follows : 11 for the 0 to < 1year group , 14 for the 1 to < 3year group , and 16 for the 3 to < 6year group . 
so , for the clinical tests in our research , the nis were set at 11 , 14 , and 16 for the 0 to < 1 , 1 to < 3 , and 3 to < 6year age groups , respectively . the clinical pretest results can be used to guide clinical practice and provide the optimal ni values for ct scans for preschool children of all ages , which can be directly applied to the ct equipment models used in this study while providing references for ct equipment of other models . 
we also 1 3 476 la radiologia medica ( 2019 ) 124 : 467477 found that the weight of asir directly affects the image quality , and its impact on children and adults is different . 
 in the case of adults , except for some body types , the asir weight is essentially the same ; however , the asir weights for children of different ages differ significantly , and different age groups have their respective optimal weights . the clinical test results showed that the asir technique can significantly reduce the effective radiation dose by 42% for children aged 0 to < 1year , by 63% for children aged 1 to < 3years , and by 72% for children aged 3 to < 6years , without reducing image quality . 
when the children in each age group were subjected to a scan with the optimal ni value , the image quality was closely correlated with the weight of asir , and the optimal asir weights of different age groups were as follows : 50% for the lung window and 40% for the mediastinal window for the 0 to < 1year group , 60% for the lung window and 50% for the mediastinal window for the 1 to < 3year group , and 70% for the lung window and 60% for the mediastinal window for the 3 to < 6year group . 
this result provides guidance for the application of the asir technique in children , and this method can also be extended to other age groups so that their optimal asir weights can be determined . 
this result can also guide the choice of parameters for other similar iterative reconstruction techniques , in which the optimal iterative reconstruction parameters of children of different age groups can be explored . a limitation of our study is the small sample size . 
further studies are needed to refine the application of asir in pediatric chest ct scans . in summary , for low - dose chest ct scans of preschoolage children , application of the asir technique significantly improved image quality and reduced image noise . 
contrast - enhanced magnetic resonance angiography ( ce - mra ) and digital subtraction angiography ( dsa ) were performed at 3months post - procedure and correlated . results primary cp was used in 13 patients , while sac was used in three patients . 
no sac reperfusion was seen in aneurysms with packing densities 29% , irrespective of either embolization method . conclusion favorable midterm results for coil packing of saas seem to depend on the coil packing density with a coil volume approximately a quarter of the aneurysm volume being most effective . 
follow - up should involve the use of ce - mra as this modality has been shown to be superior over dsa in detecting aneurysm reperfusion and coil compaction . level of evidence level iv , therapeutic study . keywords splenic artery aneurysm visceral aneurysm aneurysm embolization selective coiling stent - assisted coiling packing density mra follow - up protocol * mikoaj wojtaszek nwojtaszek@gmail.com 2nd department ofclinical radiology , medical university ofwarsaw , banacha 1a street , 02 - 097warsaw , poland 2 vascular unit , kent & canterbury hospital , east kent hospital university nhs trust , canterbury , kentct13ng , 3 department ofgeneral andendocrine surgery , medical university ofwarsaw , banacha 1a street , 02 - 097warsaw , poland introduction true splenic artery aneurysms ( saas ) are the most common visceral artery aneurysms . the acc / aha guidelines recommend treating saa when symptomatic or larger than 2cm and in women of childbearing age and patients undergoing liver transplantation , regardless of size [ 1 ]  . based on autopsy studies , the prevalence of visceral artery aneurysms has been estimated to be up to 10% , with up to 25% complicated by rupture and a mortality rate of up to 70% [ 24 ]  . 
1 a final angiogram of a treated 17 mm cp splenic aneurysm , b cta shows an infarct of the posterior aspect of the spleen and a coil packed splenic aneurysm , c selective angiogram performed just after the cta shows translocation of the coils from the aneurysm sac , occlusion of a major dorsal branch of the middle segment of the splenic artery and class ii reperfusion of the aneurysm sac , d a self - expandable xpert stent ( abbott medical ) is implanted across the aneurysm neck to secure the translocated coils , e a follow - up 3month dsa shows patency of the splenic artery without aneurysm sac reperfusion , f no sac reperfusion and splenic artery patency is further confirmed by ce - mra coils and preserving the parent artery has been reported with diligent follow - up imaging necessary to detect aneurysmal re - growth and plan intervention , but the optimal method and timing of follow - up has not yet been established . 
aneurysms with a wide neck received stent - assisted coil exclusion ( sac ) of the aneurysm sac with the parent artery supported with a self - expandable stent ( xpert self - expandable stent , abbott vascular , abbott park , il , usa )  . 
all patients received single - agent antiplatelet therapy ( acetylsalicylic acid , 75mg ) post - procedure for the following 3months . patient population followup methods , techniques andparameters all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
this retrospective review evaluated 16 consecutive patients ( 4 men ; mean age 46.7 , range 2879 ) , who underwent selective true saa embolization between june 2012 and march 2016 using detachable fibered embolization coils ( concerto , medtronic , minneapolis , mn , usa )  . 
next , coronal breath - hold fatsaturated spoiled gradient - recalled echo sequences ( fast lowangle shotflash 3d ) were performed before and after iv bolus administration of paramagnetic contrast material . 
after contrast administration , four measurements were performed with pauses at 0s , 5s , 5s and a total acquisition time of 1 3 la radiologia medica ( 2019 ) 124 : 450459 1 3 454 la radiologia medica ( 2019 ) 124 : 450459 fig . 
2 a initial selective angiogram of a 26mm splenic artery aneurysm in the mid - distal segment of the splenic artery , b final angiogram after cp of the splenic aneurysm , c initial , 3 month ce - mra of the cp splenic aneurysm ( coils and thrombus depicted by white arrowheads ) together with class iii reperfusion ( depicted by black arrows ) of the aneurysm sac , d selective angiogram before reembolization ( also 3 months ) showing coil compaction and class iii reperfusion of the aneurysm sac , e completion angiogram after reembolization showing complete occlusion of the aneurysm , f a 3month control ce - mra showing persistent reperfusion ( class ii ) of the aneurysm sac ( depicted by black arrows ) 46s . 
as mra is not a validated diagnostic method for the assessment of recanalization in coil embolized visceral aneurysms , these results were correlated with a dsa study performed on the same day . 
the follow - up period was defined as the time from treatment to the last ce - mra study . image analysis andpacking density ce - mr angiography image analysis was performed on a 3d workstation ( syngovia , siemens , erlangen , germany ) using subtracted source images to obtain multiplanar reformatted , maximum - intensity projection . 
aneurysm occlusion was classified as follows : class 1 , complete occlusion ; class 2 , residual neck ; class 3 , residual aneurysm using a neuroradiology assessment scheme as proposed by roy etal . 
results were compared using the fisher and student t tests . results sixteen patients with saa treated with fibered detachable coils had complete datasets available ( ce - mra and dsa )  . 
one patient presented with acute left flank pain 23days after the initial procedure , and cta showed an infarction of approximately 20% of the spleen and an occluded dorsal splenic branch . 
there was a significant difference in the incidence of aneurysm sac reperfusion on cemra study in between coil packing and stent - assisted coiling 1 3 la radiologia medica ( 2019 ) 124 : 450459 1 3 456 la radiologia medica ( 2019 ) 124 : 450459 fig . 
3 a initial selective angiogram of a 23 - mm splenic artery aneurysm in the mid - distal segment of the splenic artery , b a self - expandable xpert stent ( abbott medical ) is placed and expanded across the splenic artery aneurysm neck , c final angiogram after sac of the mid - segment of the splenic artery with complete aneurysm occlusion , d a 3 - month control dsa shows occlusion of the aneurysm and supporting stent with a large network of collaterals between the major and dorsal pancreatic arteries supplying the distal segment of the splenic artery , e ce - mra also showing complete occlusion of the aneurysm and underlying segment of the splenic artery . 
in the sac group , no statistical differences could be determined between the different aneurysm size groups in relation to aneurysm coil packing ( table2 )  . no sac reperfusion or coil compaction was seen in aneurysms in which a packing density of 29% was achieved , irrespective of either embolization method . 
 the thick line denotes a cutoff value of 29% discussion endovascular techniques , including embolization and stent graft placement , are now considered alternatives to conventional surgery in the treatment of splenic aneurysms [ 8 , 9 ]  . 
several authors have reported follow - up intervals at 1 and 6months after coil embolization using cta imaging , but it is now believed that this modality is hampered with excessive beam hardening artifacts making assessment of aneurysm reperfusion unreliable [ 10 , 11 ]  . 
as dsa missed 1 / 3 of the sac reperfusions in this study , and considering the low rate of rupture for visceral aneurysms , we suggest a simplified follow - up protocol which comprises a cemra performed at 3months . 
if reperfusion or compaction is present , a follow - up dsa should be performed with the intent to repack the residual aneurysa satisfactory scan at 3months should be followed up by ce - mra at 1year . 
if residual neck ( class ii ) is observed , a consensus decision should be reached , in which the risk of rupture is assessed in relation to the potential technical challenge of reembolization . 
a detailed follow - up flowchart is presented in fig.6. the relationship between packing density , coil compaction and sac reperfusion in visceral aneurysms has been previously studied by yasumoto etal . 
in this paper , a packing density of above 24% has been shown to be sufficient in preventing reperfusion in long - term follow - up while in our study a packing density of 29% was enough to prevent aneurysm reperfusion . 
 this technique is much more demanding and often impossible and will worsen splenic artery patency , as we have shown . one of the limitations of the present study is that it was conducted retrospectively in a single center and had a small series size . 
the small population group hampers adequate statistical analysis of the influence of the size of the aneurysm , but also the location on the packing density threshold , making comparison of cp and sac groups difficult statistically . 
we were unable to study the effects of anticoagulation therapy and blood pressure control in this study for similar reasons . conclusions in conclusion , favorable midterm results for coil packing of saas seem to depend on the coil packing density with a coil volume approximately a quarter of the aneurysm volume being most effective . 
 ( * technical and clinical risk for reembolization should be stratified before undertaking the procedure , especially in class ii reperfusions ) a single stage procedure , accurate follow - up of these patients is essential , as some will require further interventions . 
follow - up should involve the use of ce - mra at regular intervals as this modality has been shown to be superior over dsa in detecting aneurysm reperfusion and coil compaction . declaration and its later amendments or comparable ethical standards . 
to find the superior plan , h - vmat with three different arc designs including , two partial arcs ( 2a ) , four partial arcs ( 4a ) and four tangential arcs ( ta ) were created for each study case by combining 3dcrt and vmat with 75% 3dcrt / 25% vmat dose proportion of prescription dose . results all h - vmat plans achieved the expected target coverage . 
further , 2a h - vmat delivers less mu and beam - on time compared to 4a h - vmat . keywords breast cancer whole breast vmat hybrid - vmat introduction breast cancer is among the most common cancers in women worldwide [ 1 ]  . 
as an adjunct to surgery and chemotherapy , rt in early - stage breast cancer patients halves the rate of disease recurrence and reduces the breast cancer mortality by sixth [ 2 ]  . 
with advancement in rt techniques , the 5 - year , 10 - year and 15 - year overall survival of the breast cancer patients has improved to 89% , 83% and 78% , respectively [ 3 ]  . 
to avoid long - term complications , sparing organs at risk ( oar ) such as ipsilateral lung ( il ) , contralateral lung ( cl ) , heart and contralateral breast ( cb ) at different dose volume levels has been suggested in numerous clinical studies [ 514 ]  . 
further , reducing the dose inhomogeneity and skin dose helps in minimizing the rt - induced toxicities such as fibrosis , erythema and moist desquamation [ 15 , 16 ]  . 
the most common rt techniques available for whole breast irradiation in a linear accelerator setup are bi - tangential 3 - dimensional conformal radiotherapy ( 3dcrt ) , field - in - field ( finf ) , intensity modulated radiotherapy ( imrt ) and volumetric modulated arc therapy ( vmat )  . 
in contrast , imrt and vmat techniques provide improved dose conformity , homogeneity and sparing of high dose irradiation , however , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 546554 at the expense of increased low dose spread to normal tissue ( nt )  . though these advanced treatment techniques generate clinically acceptable plans , innovative methods are needed to get a well - adjusted result between ptv and oar dose parameters . 
 several researchers have reported on the benefit of hybrid techniques compared to other techniques in various disease sites ( whole breast [ 1722 ] , bilateral breast [ 23 ] , chest wall [ 24 ] , oral cavity [ 25 ] , lung and esophagus [ 26 ] , prostate [ 27 ] )  . 
in previous hybrid studies on breast rt , commonly 3dcrt had been kept as a base dose plan and imrt or vmat as a hybrid component [ 1721 ]  . 
 [ 22 ] kept imrt as a base dose plan and vmat as a hybrid plan . most of the published data have discussed the benefit of h - imrt for whole breast rt , whereas studies using hybridvmat ( h - vmat ) are sparse [ 1724 ]  . 
 further , in non - hybrid dosimetric studies , the vmat - only plans with different arc designs have shown to be superior compared to other plans for whole breast rt [ 2830 ]  . 
the objective of the present study is to evaluate different vmat designs in hybrid setting combined with 3dcrt as a base dose plan for left - sided whole breast rt . methods andmaterials patient selection andcontouring this study included twenty - six patients , median age of 50years ( range 2370years ) , with left - sided early breast cancer without nodal involvement . 
all scans were exported to eclipse ( version 13.6 , varian medical systems , usa ) treatment planning system ( tps ) for target and oar delineation and treatment planning . 
also , normal tissue ( nt : external body volume minus ptv ) and skin defined as a 4mm of tissue between the ptv and the body surface in the region encompassing 2cm around the ptv were contoured . 
for high dose control in nt , a virtual ring structure of 1cm thickness around the ptv was contoured . treatment planning to find the optimal plan , h - vmat plans were generated by summation of the 3dcrt plus vmat plans with three different arc arrangements comprising : two partial arcs ( 2a ) , four partial arcs ( 4a ) and four tangential arcs ( ta ) in the eclipse tps as described below . 
a single isocenter was placed at the center of ptv in the cranio - caudal direction and in the axial slice it was kept at lungptv interface to avoid beam divergence to il and heart . 
dose calculations were done using analytical anisotropic algorithm ( aaa ) with 2.5 - mm dose grid matrix and normalized to ptv mean dose equal to the prescribed dose [ 31 ]  . 
the dose objectives used for ptv and oar are described in table1 . the 3dcrt plan consisted of two coplanar open tangential fields with gantry angles based on the ptv contour . 
in order to accommodate the ptv shape changes as well as breathing effect during treatment , 2cm air gap was given from the body surface . the 2a vmat plan consisted of two coplanar partial arcs : arc1 rotated clockwise from 300 to 50 ( arc length 110 ) with collimator angle 15 , and arc2 rotated clockwise from 50 to 160 ( arc length 110 ) with collimator angle 345 . 
 for each patient , dose to oar was minimized as low as possibly achievable without compromising the ptv coverage ; however , same objective functions were used for all three vmat plans for a particular patient . 
 similarly , arc3 rotated clockwise from 110 to 160 and arc4 dosimetric evaluation to evaluate the plan quality , quantitative analysis was performed by using dose volume histograms ( dvh )  . 
the paddick [ 32 ] ci was calculated , as ci = v_ptvref v_ptvref v_ref v_ptv where v_ptvref is the volume of reference isodose ( 95% ) inside the ptv ; and v_ptv , v_ref are the volume of ptv and reference isodose ( 95% ) , respectively . 
the hi was calculated , as hi = d2% d98% where d2% and d98% are the doses received by 2% , 98% of the ptv and dp is the prescription dose [ 31 ]  . 
the gi was calculated , as gi = v50% v_ptv 1 3 la radiologia medica ( 2019 ) 124 : 546554 where v50% is the volume of 50% isodose and v_ptv is the volume of ptv . 
treatment delivery parameters such as mu and beam - on time ( bot : time taken to deliver first mu to last mu ) were also recorded . additionally , the chest wall separation ( cws ) , maximum heart distance ( mhd ) and central lung distance ( cld ) were measured as illustrated in fig.2 and defined by das etal . 
the correlation coefficients ( r ) were calculated between ptv coverage , ci , hi versus cws ; heart dose parameters versus mhd ; il dose parameters versus cld . statistical analysis the dosimetric results of three h - vmat plans were statistically analyzed using the mannwhitney u test for nonparametric paired group comparison . 
the beam - on time was 46s less in the 2a h - vmat plan ( p < 0.00001 ) compared to other plans . the cws , mhd , cld and average volumes of the ptv , heart , il are summarized in table3 . 
table4 summarizes the correlation coefficients ( r ) between ptv coverage , ci , hi versus cws and ptv volume ; heart dose parameters versus mhd ; il dose parameters versus cld for all plans . 
similarly , intermediate correlations ( r ~ 0.8 ) were noticed between cld and il mean , v20gy , v40gy for all plans . cws = chest wall separation ; mhd = maximum heart distance ; cld = central lung distance fig . 
the second cancer risk was lower in 3dcrt [ 34 ] than vmat , and the cosmetic outcomes were improved in imrt / vmat compared to 3dcrt [ 16 ]  . 
 h - vmat technique efficiently limits the setup and breathing effect by delivering most of the dose using open 3dcrt beams with widened skin flash margin . in several non - hybrid dosimetric studies , different vmat designs were used for whole breast rt . 
 the present study utilized two split arcs and tangential arcs design in h - vmat plans . to get optimal beam geometry , several plans with different arc lengths were generated prior to this study . 
these plans included a 190 arc length between the two tangential fields used in 3dcrt ( 300130 ) , a 220 arc length between 300 and 160 and a 240 arc length between 300 and 180 . 
therefore , in this study , average dose proportion ( 75% dose weighting for 3dcrt and 25% dose weighting for vmat plans ) was chosen by considering the balance between the risks of low and high dose levels . the main aim of hybrid plan is to improve the ptv coverage , ci , hi and reduce low and high dose volumes to heart , il , cl and cb , thereby reducing the risk of longterm complications such as heart disease , pneumonitis and radiation induced secondary cancers . 
robust clinical studies with strong dosimetric correlation have made a set of doseconstraint recommendations to limit the dose of radiation received by specific volumes of oar in order to prevent long - term adverse outcomes [ 514 ]  . 
moreover , planning technique , beam geometry , optimization , dose calculation algorithms used and planners skill play a significant role in generating optimal plans . the main uncertainties in whole breast rt are setup and breathing effect . 
deep inspiration breath - hold ( dibh ) and gated techniques have been 1 3 la radiologia medica ( 2019 ) 124 : 546554 shown to reduce high dose to heart and il . 
to decrease setup uncertainties , appropriate ptv margin and daily image guidance should be considered . the key factor to get an optimal h - vmat plan would be its ability to reduce high dose as well as low dose radiation to oar without compromising the ptv parameters . 
2a h - vmat provided statistically similar results compared to 4a h - vmat , in addition reduced mu ( ~ 23 mu ) as well as beam - on time ( ~ 46s )  . 
however , in whole breast rt with simultaneous integrated boost or nodal volumes or hypo fractionated dose settings , 4a h - vmat might provide favorable results by increased beam modulation . conclusion in the present dosimetric study , 2a and 4a h - vmat techniques were effective in reducing oar doses as well as improving ptv dosimetric parameters . 
prospective clinical trials with long - term follow - up in patients would provide insight into actual benefits of such innovative techniques . compliance with ethical standards conflict of interest all authors who contributed to this study declare that they have no conflict of interest with respect to the manuscript . ethical approval institutional scientific and ethics board has approved this study . 
this article does not contain any studies with human participants performed by any of the authors . informed consent the informed consent has been waived off by the ethics board of the institute considering this as a retrospective study with no human involved . 
we measured the correlations using the spearman correlation coefficients ( rs ) for all combinations of the bivariate pair , performed pairwise comparisons of the rs values , and calculated the coefficients of determination . 
all analyses were conducted with the jmp pro software . results the stronger bivariate correlations were represented by the estotal cites rs = 0.968 , p < 0.001 , r2 = 0.937 ; and the citescoresjr rs = 0.911 , p < 0.001 , r2 = 0.829. 
from 105 possible combinations of pairwise comparisons , 38 depicted a p value > 0.050 which would suggest interchangeability among bivariate correlations . conclusions our findings support our hypothesis that the if does not show the best correlation between other metrics . 
cuauhtemoc , 06726mexicocity , mexico 2 escuela de medicina , universidad de sonora , hermosillo , mexico 3 departamento de metodologia de la investigacion , instituto nacional de pediatria , mexicocity , mexico 4 department ofradiology , i.m. 
2 , 119992moscow , russia introduction with the emergence of new databases offering competitive algorithms to participate in the bibliometric boosting game , new metrics are around , each with their strengths and weaknesses ; the bibliometric analysis of these metrics attempts to measure the impact of a journals published material that can reinforce their prestige [ 1 ]  . 
some questions remain unanswered in this field : which index metric should i use to select the journal to submit for publication ? in which journal will my research have the most extensive circulation ? several alternative metrics are available for the journals editor in the last years , and many editors have decided to publish them parallel to the impact factor ( if ) : the scimago journal rank ( sjr ) , the source normalized impact per paper ( snip ) , the eigenfactor score ( es ) , and vol . : ( 0123456789 ) 1 3 496 la radiologia medica ( 2019 ) 124 : 495504 the citescore ( citescore )  . 
of articles [ published ] , cited half - life , es , and article influence score ] , the es was the best predictors of 2 - years - ahead citations . 
this evidence was proved for the journals in the gastroenterology and hepatology [ 3 ] ; neurosciences [ 4 ] ; and radiology , nuclear medicine & medical imaging [ 5 ] categories . several journals have published comparisons of the if with sjr , snip , and es in some specialties such as otolaryngology [ 6 ] , nuclear medicine [ 7 ] , pediatric neurology [ 8 ] , occupational therapy [ 9 ] , psychiatry and psychology [ 10 ] , nephrology [ 11 ] , obstetrics and gynecology [ 12 ] , clinical medicine and infectology [ 13 ]  . 
furthermore , the use of citescore has been reported for journals in behavioral neuroscience [ 14 ] , dermatology [ 15 ] , pharmaceuticals science and molecular medicine [ 16 ] , trade journals [ 17 ] , structural chemistry [ 18 ] , and nursing [ 19 ]  . 
studies about bibliometrics continue being a trending topic , as many editors and authors in this category comment on several aspects of the if and its association with concurrent bibliometrics [ 2024 ]  . we aimed to obtain correlation values between the if and the metrics mentioned above and to assess significant differences between bivariate correlations of if with sjr , snip , es , and citescore in the radiology , nuclear medicine & medical imaging category . 
our findings might help authors in this category to understand which indices offer the best association with total cites or if ; then , authors could use this information to decide which bibliometric they use to rank their target journals before submission . table 1 basic bibliometric concepts [ 26 ] bibliometric index concept total cites snip the total number of times that a journal has been cited by all journals included in the database in the jcr year . 
citations to journals listed in jcr have compiled annually from the jcr years combined database , regardless of which jcr edition lists the journal and regardless of what kind of article was cited or when the cited article was published . 
each unique article - to - article link is counted as a citation all citations to the journal in the current jcr year to items published in the previous 2years , divided by the total number of scholarly items ( these comprise articles , reviews , and proceedings papers ) published in the journal over the last 2years . 
though not a strict mathematical average , the journal impact factor provides a functional approximation of the mean citation rate per citable item it is a measurement factor that establishes the quality of scientific publications based on the count of citations obtained by each publication . 
it is performed on the calculation of citations received by journals in 3years , giving higher weight to citations from prestigious journals ( those with high citation rates and low self - citations ) using the algorithm of google pagerank it measures contextual citation impact by weighting citations based on the total number of citations in a subject field . 
unlike the well - known journal impact factor , snip corrects for differences in citation practices between scientific fields , thereby allowing for more accurate between - field comparisons of citation impact . 
cwts journal indicators also provide stability intervals that indicate the reliability of the snip value of a journal it measures the number of times the articles from the journal published in the past 5years have been cited in the journal citation reports ( jcr ) year . 
every reference from one article in a journal to another article from the same journal is discounted , and weights each reference according to a stochastic measure of the number of time researchers spend reading the journal citescore citescore is a metric that measures the list of citations per article published . 
it provides added value to compare and evaluate scientific citescore calculates the citations of all the documents of a specific year in all the papers published in the previous 3years . 
that number is divided by the number of papers indexed in scopus published in those same years 1 3 la radiologia medica ( 2019 ) 124 : 495504 materials andmethods study design retrospective study . 
if , total cites , and es of journals in the radiology , nuclear medicine & medical imaging category from the web of knowledge [ 2 ] were recorded from the journal citation reports ( jcr ) [ 25 ] available for 2017 . 
the impact factor ( if ) is a measure of the frequency with which the average article in a journal has been cited in a particular year which can be consulted in the platform web of knowledge every year . 
the context within which the snip is evaluated is determined by the reference practices of the journals within the thematic field in question , as well as the extent to which the database covers this field . 
the citescore is the youngest metric , was proposed in december 2016 [ 29 ] , and is one of the three major indices included in scopus by elsevier to rank publication sources [ 17 ] ; the definition can be explained by its formula [ 17 ]  . 
citescore for year n ( citescore n ) sums the citations received in year n to documents published in years n 1 , n 2 , and n 3 and divides this by the number of documents published in the three consecutive years n 1 , n 2 , and n 3 . citescore n = citation count in n documents documents ( n 3 ) ( n 1 ) for instance , citescore n = citation count in 2019 documents 2016 2018 according to scopus , the 3 - year citescore time window was chosen as the best fit for all subject areas [ 17 ]  . we only chose journals in the radiology , nuclear medicine & medical imaging that coincidentally depicted values for if , es , sjr , snip , and citescore reported for the year 2017 . 
we additionally recorded the number of total cites as it is the standard variable considered for these metrics , and we also wanted to know the correlation values for this variable . 
a total of 122 journals were selected ; see table a in the supplementary online - only file . sample size calculation we used a sample size formula based on correlation coefficients in a cross - sectional study [ 30 ]  . 
the pairs of bivariate correlations were calculated using the formula for combinations c ( n , r ) = p ( n , r ) / r ! ; then , we use n = 6 for the number of bibliometrics and r = 2 for the number of pairs , which gave us 15 possible pairs . 
the previous three examples revealed that the average difference in r values of 0.146 is enough to warrant significant differences when you compare correlation values ; this difference represents a coefficient of determination of 0.021 ; it means a 2.1% of the variance in r values would suggest not interchangeability between bivariate correlations . 
table4 shows the pairwise comparisons with a p value < 0.050 , indicating not interchangeability among bivariate correlations of bibliometric indices ( table5 )  . comparison ofcorrelation coefficients withearlier studies we found only three previous studies in the literature that included some of the bivariate correlations evaluated in this studyour findings showed very strong correlation values for the citescoreif and sjrif were very similar to the values reported in the category of occupational therapy [ 9 ]  . 
figure2 shows the correlation matrix for all selected variables . pairwise comparison ofcorrelation coefficients from 105 possible combinations of pairwise comparisons , 38 depicted a p value > 0.050 which would indicate interchangeability among bivariate correlations . 
among those pairs with p values > 0.700 , sjr and citescore were not significant when each one was compared with the total cites ; similar observations were found for citescorees and esif . 
table4 shows the the measure of academic performance using bibliometrics usually applies to the impact of the scientific work of a journal or an author ; or the eligibility of a researcher to compete for a national scientific qualification , to receive funds or to become professor [ 18 ]  . 
the assessment of the scientific impact of journals evaluated by bibliometrics is a complex , multi - dimensional construct , and therefore the use of a single bibliometric index is considered inappropriate to rank , evaluate , and value journals [ 33 ]  . 
then , the use of multiple newer metrics provides a more comprehensive view of journals and their relative placements in their fields [ 34 ] ; this approach let referees go beyond the if limits . in this study , we were able to calculate correlations coefficients and pairwise comparisons between six selected bibliometrics : total cites , if , sjr , snip , es , and citescore in the radiology , nuclear medicine & medical imaging 1 3 500 la radiologia medica ( 2019 ) 124 : 495504 fig . 
it is evident the non - normal distribution of the majority of selected indices category in his study , we performed comprehensive pairwise comparisons among bibliometrics from the leader databases ( web of science , scopus , and scimago )  . the citescore was proposed in december 2016 by elsevier ; we only found one study that compared ranking positions of nuclear medicine journals using the sjr , if , and es from 2010 , but the authors did not present correlation coefficients [ 7 ]  . 
independently of the limitations based in the years that each index considered in their calculations , we were surprised to discover that the index that reached the highest correlation with the total cites in our chosen category was total citeses . 
this pair had an rs = 0.967 , other rs correlations were represented by total citesif rs = 0.729 , total cites snip and total citessjr rs = 0.686 , and the lower correlation was observed for total citescitescore with rs = 0.665 ; we had believed that citescore would depict the highest relationship as it is the more contemporary algorithour findings agree with a previous study in the neurology category that showed a moderate association between the citescore ; however , this study did not include pairwise comparisons of the r coefficients [ 8 ]  . 
one of the reasons for this finding could be related to the fact that citescore covers twice as many journals22 , 000 to the ifs 11 , 000and that its formula counts the total number of documents in the previous 3years [ 17 ]  . although if became the leader metric for consideration of tenure and promotion , and budget and resource planning in most of the universities , research institutions , and colleges [ 35 ] , contradictory opinions have stated that the if is not a perfect metric and has severe limitations [ 24 , 3638 ]  . a previous study [ 5 ] revealed the es was bibliometric that captured the best prediction of citations of a journal . 
our findings reveal that correlation values show the same behavior as the if : each medical speciality depicts different r threshold for significance [ 35 ]  . because es is a per - journal measure that represents each journal size , based on its total citations [ 39 ] , we considered the total cites as an additional variable in our analyses and graphs . 
however , we considered this interpretation misleading because each medical speciality should be analyzed independently and with a clear understanding of the correlation values among metrics for that selected category . 
the same study reported for the sjrif a negative r = 0.35 ; we found for the same variables an r = 0.884 , but the studies were performed in different categories of medical journals [ 6 ]  . 
 we did not include altmetrics in our comparisons , because they were out of the scope of this article . additional factors , such as longer time frames , the number of articles published in each issue , circulation of each journal , host of factors impacting citation ( self - citation , semi - mandatory , and mandatory citation ) might all influence citation calculations . 
we did not include these possible confounding factors , as the web of knowledge , scj , and scopus do not consider thealso , some factors that may affect author where to submit their work were outside the scope of this study : topic , affiliation with society , geography , rejection by earlier submission , familiarity with the submission and revision process , turnaround time , and invitation by editors . 
readers should be aware that the jcr contains approximately 171 categories in the sciences and 54 in the social sciences ; then , publication of future studies validating our model in other specialities would be desirable . in conclusion , bivariate correlations of bibliometric indices report a wide range of values from very strong to weak and even negative associations ; but these results vary depending on the selected categories . 
there is a growing trend to report on bibliometric analyses in particular disciplines looking for a better assessment of the significance and importance of scientific radiologists and other medical specialities ( nuclear medicine , interventional radiologists , and related fields ) should have the reference values of correlations among the essential bibliometric indices in their area ; these values may become a new standard of the quality of research . acknowledgements moises villaseor - almaraz , m.d. , was a research fellow at directorate of research , hospital general de mexico eduardo liceaga , during 2018 . 
univariate radiomic analysis was performed to find highly correlated radiomic features with imrt response , and a paired t test was used to find significant features between responders and non - responders . 
to find high predictive radiomic models , tenfold cross - validation as the criterion for feature selection and classification was applied on the pre - , postand delta imrt radiomic features , and area under the curve ( auc ) of receiver operating characteristics was calculated as model performance value . results of 33 patients , 15 patients ( 45% ) were found as responders . 
studies have indicated that intensity - modulated radiation therapy ( imrt ) has several benefits for prostate cancer patients in terms of both tumor control and normal tissue toxicity [ 1 ]  . 
 for example , the common marker , prostate - specific antigen ( psa ) , has some limitations including substantial differences in its accuracy , sensitivity , specificity and positive predictive value [ 3 ]  . 
on the other hand , prostate cancer diagnosis , staging and grading using some current methods suffer from several limitations such as invasiveness , low sensitivity and chance of patient infections [ 4 ] , and also , treatment effectiveness assessment using imaging is mostly based on morphological parameters and contrast media kinetics which are not best predictors of short - term response [ 5 ]  . as an advanced image quantification issue , radiomics may potentially serve as a new promising approach to reach precise personalized therapy in prostate cancer [ 6 , 7 ]  . 
 some previous studies have indicated that radiomic features extracted from different prostate mri scans including t2weighted ( t2w ) , dw , dynamic contrast - enhanced ( dce ) and adc could be the feasible biomarkers for prostate cancer detection / diagnosis [ 8 , 9 ] , aggressiveness [ 10 ] , staging and therapy response prediction [ 11 ]  . 
previous prostate radiomic studies also have revealed that there are good correlations among mr image features and gleason scores ( gs ) of prostate cancer zones , biochemical recurrence [ 12 ] and gene expression [ 13 ]  . regarding prostate cancer , on the other hand , a wealth of data has been published on the radiation therapy ( rt ) response evaluation using diffusion - weighted imaging ( dwi ) and identified that apparent diffusing coefficient ( adc ) obtained from dw images is a feasible noninvasive approach to assess rt response in different cancers [ 1417 ]  . 
 for prostate cancer , studies have found that adc is a favorable indicator to predict and evaluate response to different rt approaches including intensity - modulated radiation therapy ( imrt ) [ 18 ] , three - dimensional conformal rt ( 3dcrt ) [ 19 ] and ion therapy [ 20 ]  . in recent years , researchers have investigated a variety of machine learning ( ml ) approaches to build high accuracy , reliability and efficiency predictive and prognostic radiomic models in different cancers [ 2123 ]  . 
hence , some studies have suggested that it is essential to compare different ml models for radiomics - based clinical decision making [ 21 , 24 ]  . to the best of our knowledge , there is no report on prostate cancer imrt response prediction using radiomic approaches . 
also , we tested several ml methods for gleason scores and prostate cancer stage prediction . materials andmethods the general framework of this study is depicted in fig.1. this wok was conducted as a prospective research study , and all ethical issues relating to the patients are approved by the ethical committee . 
all procedures performed in studies involving human participants were in accordance with the 1964 helsinki declaration and its later amendments . patients andtherapy a total of 33 prostate cancer patients who were diagnosed and treated from april 2015 to june 2017 were included in this study . 
all imrt plans were generated using varian eclipse system . imaging all patients underwent two mri scans before and after treatment called pre - imrt and post - imrt scans , respectively . 
transverse t1 - weighted images were acquired as follows : repetition time / echo time ( msec ) , 563 / 14 ; section thickness , 3mm ; intersection gap , 2mm ; field of view , 2240cm ; and matrix , 256 224 . 
transverse , coronal and sagittal t2 - weighted were acquired as follows : repetition time / echo time ( msec ) 3000 / 101 ; section thickness , 3mm ; intersection gap , 2mm ; field of view , 1424cm ; and matrix , 265 205 . 
transverse dw sequences were acquired with a single - shot spin - echo echo - planar imaging sequence with single b value ( 1200s / mm2 ) ; section thickness , 3.5mm ; intersection gap , 2mm ; field of view , 1424cm ; matrix , 150 150 ; and with the same orientation and location used to acquire transverse 1 3 la radiologia medica ( 2019 ) 124 : 555567 data acquisition t2 weighted adc map image preprocessing 3 , 64 gray level image segmentation & response evaluation feature extraction classification model evaluation fig . 
1 flowchart of the present study intensity shape texture ( glrlm , glcm , glszm , ngldm , gldm ) feature selection select from model ( sm ) select k best ( sb ) select percentile ( sp ) variance threshold ( vt ) adaptive boost ( ab ) decision tree ( dt ) linear support vector machine ( lsvm ) gaussian nave bayesian ( gnb ) k - nearest neighborhood ( knn ) gaussian nave bayesian ( gnb ) k - nearest neighborhood ( knn ) logistic regression ( lreg ) bernoulli nave bayesian ( bnb ) t2 - weighted images . 
preand post - imrt scan protocols including t1w , t2w and dw images for all patients were same . response evaluation in the present study , prostate cancer response was assessed based on the changes of adc values before and after imrt . 
in this situation , roi was drawn in the same area as that initially used in the pre - therapy , based on the anatomical markers and was also described by previous studies [ 25 , 26 ]  . 
the percentage changes ( pc ) of adc values 1 3 558 la radiologia medica ( 2019 ) 124 : 555567 pre - post - imrt were considered as imrt response ( ( adcpost - imrtadcpre - imrt / adcpre - imrt ) 100 )  . 
this therapy response evaluation was obtained from previous studies [ 27 , 28 ]  . preprocessing before feature extraction and in order to normalize the intensities across all the patients , to reduce noise and to increase sensitivity , image intensities were normalized between 3 , where is the mean value of gray levels inside the region of interest ( roi ) and is the standard deviation . 
in this issue , 3 limits image intensities in the range [ 3 , + 3 ] and removes the dependency on the shift of the mean value and on multiplicative change in the image intensity and also minimizes intraand interscanner effects in mri texture analysis . 
also , all images were quantized to 64 gray - level intensities for noise reduction and image uniformity . tumor segmentation in this study , t2w and adc images were used for radiomic analysis . 
we also obtained delta imrt features by relative changes of pre - / post - imrt features : ( features post - imrtfeatures pre - imrt / features pre - imrt )  . feature selection because many of features extracted from images are simply noise or highly correlated with each other , they could enhance the chance of overfitting , decreasing prediction accuracy , maximizing the computational cost . 
in this regard , feature selection is a critical issue in radiomic analysis . in this study , we used four feature selection methods : selectkbest_chi2 ( sk ) , variance threshold ( vt ) , select from model ( sm ) and select percentile ( sp )  . 
in sp method , an anova test is used with percentile of 20 , 40 , 60 and 80% . univariate analysis in this study , our main focus was on the imrt response prediction . 
our univariate analysis has two main steps : ( 1 ) highly correlated radiomic features with imrt response were selected among four groups of feature selection and ( 2 ) a paired t - test was performed to find significant features among responder and non - responders . 
 box plots were made to compare selected features among responder and non - responder groups . classification the objective of this study was to stratify patients into two labeled classes using different ml classifiers . 
this issue also was repeated to classify patients with stages t2 and t3 ( t2 patients were labeled as 1 , and t3 patients were labeled as 0 ) and patients with gs 7 and gs > 7 ( t 2 patients with gs 7 were labeled as 1 , and patients with gs > 7 were labeled as 0 )  . a total of nine classification methods based on ml approaches were used in the analysis : linear support vector machine ( lsvm ) , logistic regression ( lreg ) , bernoulli naive bayes ( benb ) , stochastic gradient descent ( sgd ) , k - nearest neighbors ( knn ) , decision tree ( dt ) , random forest ( rf ) , adaptive boosting ( adbo ) and gaussian naive bayes ( ganb )  . 
in balance method , we have equal data from each class ( binary classification ) , whereas in unbalance , there are no equal data and data are selected randomly . all information regarding all ml algorithms for feature selection and classification is summarized in supplementary table2 . statistical analysis all analyses regarding the feature selection and classification were performed using in house - developed python codes . 
 1 3 la radiologia medica ( 2019 ) 124 : 555567 in order to find best predictive models for these classifications , we tested different combinations of feature selection and classification methods . 
classifiers were trained using the tenfold cross - validation method , and their predictive performance was then evaluated using the area under the receiver operator characteristic ( roc ) curve ( auc )  . 
the predictive performance of all models was compared based on the mean aucs . results patients andimrt response thirty - three prostate cancer patients with median age of 73years ( 5182 ) were studied . 
the box plots comparing selected radiomic features are shown in fig.2 ( a for t2w and b for adc )  . imrt response prediction models for imrt response prediction , several radiomic models based on the image features , classification and feature selection methods were obtained . 
the models performance ( auc ) as cross - combination of feature selection and classification approaches for pre - imrt t2 w and adc image features is depicted in fig.3 ( a for t2w and b for adc )  . 
in comparison with other methods , e.g. , psa , quantified radiomic features may be more feasible , noninvasive and easy to use . in our predictive modeling , in addition to pre - treatment radiomic features , we also analyzed features extracted from post - treatment mr images for response predicting in prostate cancer patients . 
because the main aim of the radiomic analysis is to assess intra - tumor heterogeneity , post - treatment radiomic analysis will show the impact of therapy on this heterogeneity . 
on the other hand , after the treatment , the tumor status underwent several structural changes and therefore radiomic feature changes , which will be interesting to understand how a therapy modality acts . 
because response monitoring in prostate cancer patients is based on the several months to years follow - up , our radiomic models may be useful for tailor the therapy and individualized radiotherapy . 
several studies have applied radiomic analysis on post - treatment images and indicated that these issues have the potentials for several clinical decision makings such as adaptive radiotherapy , new therapy prescription and late response prediction [ 3032 ]  . 
they found that most of the post - rt features were significant with the pet response , whereas clinical stage was not associated with the response . for delta radiomics , to our knowledge , no published reports have investigated the possibility of using delta radiomic features extracted from mr images for predicting response in prostate cancer patients . 
 several investigations have mentioned the utility of delta radiomics for prognosis predicting in cancers including liver metastases in colorectal cancer [ 34 ] , metastatic renal cell cancer [ 35 ] , esophageal cancer which would develop radiation pneumonitis [ 36 ] and non - small cell lung cancer [ 37 ]  . 
in some previous studies , delta radiomic model had found more performance which differs from our results . in this study , we observed that several pre - treatment radiomic features are highly correlated with imrt response . 
2 ( continued ) cluster shade are good measures of tumor homogeneity , heterogeneity , smoothness , randomness and symmetry which finally determine how a specific tumor respond to a specific therapy . 
our results are in concordance with some previous studies [ 3840 ]  . as was discussed by some previous studies , for the successful realization of predictive or prognostic radiomic modeling , different feature selection and classification methods have to be evaluated and compared . 
there are few studies which compared different machine learning approaches as feature selection and classification methods for developing radiomic models in non - small cell lung cancer ( survival prediction ) [ 41 ] , lung cancer ( survival prediction ) [ 21 ] and head and neck squamous cell carcinoma ( survival prediction ) [ 42 ]  . 
3 a heatmap depicting the predictive performance ( auc ) of feature selection ( in rows ) and classification ( in columns ) methods of pre - imrt t2w models . 
4 box plot comparing of the predictive performance ( mean auc ) of all the radiomic models 1 3 la radiologia medica ( 2019 ) 124 : 555567 564 fig . 
5 a heatmap depicting the predictive performance ( auc ) of classification ( in rows ) and all the image sets ( in columns ) methods of pre - imrt t2w models . 
in regard to correlation between gleason scores and radiomic features , although it is not new and have been reported by some previous studies , we performed this investigation by using new machine learning approaches , and for classification of gs 7 and gs > 7 , fehr etal . 
they used generalized linear regression and generalized estimating equations methods to differentiate between gleason scores of 3 + 3 = 6 versus ( 3 + 4 = 7 or 4 + 3 = 7 ) , 3 + 3 = 6 ver sus > 7 and 3 + 4 versus > 3 + 4 using mri - derived texture parameters [ 44 ]  . 
it could be a new noninvasive , simple and easy method for cancer staging without any patient discomforts . although our results are significant , this study has several limitations : first , small number of patients . 
whole liver dose , tumor dose and healthy injected liver dose , lung dose and if applicable the gallbladder dose were all calculated by using the medical internal radiation dose ( mird ) formula from spectct images . 
there were no detected grade 2 or 3 adverse events . conclusion tare is safely performed without cystic artery embolization when its origin is close to the treatment area . keywords cystic artery embolization transarterial radioembolization y90 introduction transarterial radioembolization ( tare ) with yttrium - 90 ( y90 ) , also known as selective internal radiotherapy ( sirt ) , has been increasingly used as a locoregional therapy option for primary and secondary malignant hepatic tumors [ 14 ]  . 
the most feared complication is nontarget delivery of y90 - labeled microspheres into the surrounding tissues through the hepatico - enteric arteries ( cystic artery , right gastric artery , gastroduodenal artery and hepatic falciform artery ) resulting in gastrointestinal ulceration or radiation cholecystitis [ 68 ]  . 
radiation cholecystitis resulting from the nontarget delivery of microspheres through the cystic artery is generally a subclinical , self - limiting process and rarely requires surgery [ 9 , 10 ]  . 
however , gallbladder involvement after the pretreatment angiography , with technetium - 99m - labeled macroaggregated albumin ( 99mtc - maa ) , is not rare and could be detected in 812% of the patients [ 1113 ]  . 
however , pre - treatment coil embolization does not always preclude nontarget embolization due vol . : ( 0123456789 ) 1 3 576 la radiologia medica ( 2019 ) 124 : 575580 to recanalization of the occluded artery and / or development of collaterals [ 1417 ]  . 
in addition , coil embolization of the cystic artery itself , although occasionally observed , can cause ischemic cholecystitis which results in even more serious complications [ 10 ]  . 
some other groups do not routinely perform coil embolization [ 17 ] and position the microcatheter distal to the hepatico - enteric artery origin when possible or alternatively they may induce vasospasm or temporary embolization during the y90 treatment when distal positioning is not possible [ 18 ]  . 
the debates about how to manage the cystic artery during tare are continuing and have not yet arrived at a definitive conclusion [ 5 , 18 ]  . in the present study , we aimed to assess radiation - induced cholecystitis in cases of cystic artery origin nearby the treatment zone for tare treatment . materials andmethods patient population local institutional review board approved this retrospective single - center study . 
all of the hepatic angiograms of the patients with primary or secondary malignant liver tumors treated with tare were extracted from the radiology database between january 2014 and january 2018 , and patients in whom cystic artery origin was located in the surrounding area of the treatment zone on 99mtc - maa angiograms were included in this study . ct angiography of the liver and blood tests including liver functions were obtained from all patients before the procedure . 
all of the patients in this cohort were deemed suitable for tare by the multidisciplinary tumor board of the hospital . pre - treatment evaluation hepatic angiography obtained with delivery of 99mtc - maa into the target hepatic arteries was performed in all patients , and single - photon emission computed tomography ( spectct ) or fusion of spect and ct images was obtained . patients with cholecystectomy , non - enhanced or embolized cystic arteries or microcatheter position distal to the cystic artery on pre - treatment evaluation angiograms with 99mtc - maa were excluded . assessment ofgallbladder withspectct the gallbladder was assessed for 99mtc - maa involvement both qualitatively by visual evaluation and quantitatively by calculating the radiation doses from the spectct images . 
whole liver dose , tumor dose and healthy injected liver dose , lung dose and if applicable the gallbladder dose were all calculated by using the medical internal radiation dose ( mird ) formula ( 20 )  . 
only the wall of the gallbladder was used for dose calculation , and the gallbladder lumen was excluded . procedure all procedures were performed via standard right femoral approach with a 4f or 5f short vascular sheath under local anesthesia . 
microcatheters with a distal luminal size of 2.8f ( progreat , terumo , somerset , new jersey , usa , or embocath , biosphere medical , rockland , ma ) were used for right hepatic artery selective catheterization . 
in all patients , the cystic artery was visualized , and when feasible , the cystic artery origin was bypassed and the microcatheter was placed distal to the cystic artery origifbypass was not technically possible , 99mtc - maa infusion was performed from the placed microcatheter and a decision to proceed with y90 treatment was made based on spectct findings . 
if it was decided to proceed with y90 treatment , on the day of the tare ( 715days after the pre - treatment session ) , all of the angiographic devices were selected same as with the pretreatment 99mtc - maa angiography in order to imitate the same conditions . 
temporary or permanent coil embolization of the cystic artery was not felt necessary in this cohort , neither was preferred an anti - reflux infusion system , nor provocation of vasospasm within the cystic artery . 
all procedures were performed by two interventional radiologists with > 10years and 5years of individual experience in embolization procedures . followup clinical assessment with laboratory workup ( including liver function tests ) was repeated on the first day and at 1month after the treatment . 
spectct images show radioactivity in whole gallbladder wall ( arrows ) which was scored as moderatesevere involvement failure ( increasing ascites , icterus and elevated laboratory test results ) , liver abscess , intrahepatic bilomas and liver infarction were also noted . with ultrasound ( us ) , dynamic computed tomography ( ct ) and / or position emission tomography ( pet ) and / or dynamic liver magnetic resonance imaging ( mri ) at 13months following treatment and at 36 - month intervals thereafter . 
the observed adverse events regarding both gallbladder problems ( cholecystitis , right upper quadrant pain , etc . ) and others were classified according to the national cancer institutes common terminology criteria for adverse events ( ctcae v5.0 ) [ 20 ]  . 
a total of 34 tare procedures from 29 patients ( 18 men and 11 women ) , with a mean age of 65 13.3years meeting the inclusion criteria , were involved in the current study . 
increasing ascites , icterus , elevated laboratory test results , liver abscess , intrahepatic bilomas or liver infarction was not encountered during follow - up visits . discussion the current study demonstrated that without taking a precaution for the cystic artery , y90 - labeled microspheres might be safely delivered into the target hepatic artery when cystic artery origin was located in the close proximity ( less than 8 - 10mm ) of the tare treatment zone . 
however , administration of y90 microspheres into the cystic artery has always been avoided whenever possible in our unit , and the cystic artery origin was always bypassed with the microcatheter which was placed distal to the cystic artery orighowever , it became complicated when the bypass or la radiologia medica ( 2019 ) 124 : 575580 coil embolization was technically impossible , and the cystic artery was retained in the treatment zone . 
in those group of patients , if there is no moderatesevere maa uptake ( none or mild ) on spectct , we proceed with tare , whereas if there is moderatesevere maa uptake on spectct , tare is postponed until cholecystectomy . 
nevertheless , as a result of not very uncommon anatomical variations and technical infeasibility of super - selective catheterization of the cystic artery , in some cases it might be impossible to refrain from the delivery of some radioactive - labeled spheres into the cystic artery [ 21 , 22 ]  . 
we know from previous studies that the proximal microcatheter position might not always cause radiation - induced cholecystitis ( ric ) , and pathological evaluation of some hepatectomy cases showed multiple microspheres within the gallbladder wall in totally asymptomatic patients [ 23 ]  . 
 [ 18 ] that the microcatheter could be repositioned to change the flow and diminish the gallbladder perfusion , and therefore , cystic artery might be safely included [ 18 ]  . 
 [ 18 ] also reported different options to cope with cystic artery to prevent ric , despite the fact that they noted proximal microcatheter position did not always cause ric . 
moreover , although the cystic artery was located within the treatment zone , we observed even no radioactivity in the gallbladder wall on spectct images in 23 procedures in this series . 
 [ 24 ] reported three patients with detected radioactivity in the gallbladder wall without any signs or symptoms of ric during the follow - up and they did not use any precaution for the cystic artery before the procedure . 
within the quality improvement guidelines , it was also noted that radioactivity detected in the gallbladder wall on spectct is not uncommon and not always resulted in ric clinically or radiologically , and if any ric is diagnosed , it does not always need surgical treatment [ 25 ]  . in a comparison study of cystic artery embolization , powerski etal . 
 at our institution , we prefer distal microcatheter position whenever possible or feasible , or to leave the cystic artery within the tare treatment zone because both embolization and delivery of y90 - labeled microspheres may result in cholecystitis [ 10 , 19 ]  . 
pre - treatment coil embolization does not always preclude nontarget embolization due to 1 3 la radiologia medica ( 2019 ) 124 : 575580 recanalization of the occluded artery and / or development of collaterals [ 1417 , 27 ]  . 
if there is a significant gallbladder radioactivity on spectct images , we perform a proximal coil embolization of the cystic artery before tare . spectct is useful for gallbladder assessment before tare , and a risk of cholecystitis could be assigned by measuring the radioactivity in the wall of the gallbladder [ 25 ]  . 
however , the detected radioactivity in the gallbladder wall may not always mean an increased risk of ric because it was not the radioactivity itself , but the concentration or amount of it in the gallbladder wall on spectct , which enabled us to make a reliable sirt without a complication of ric . 
and , nine out of 11 patients were totally symptoms free or negative for any changes in laboratory tests . several alternatives were described to eliminate the risk of ric during hepatic tare procedure : ( 1 ) permanent or temporary embolization of the cystic artery with coils or gelfoam [ 26 , 27 ] , ( 2 ) positioning the microcatheter distal to the cystic artery [ 6 , 11 ] , ( 3 ) causing vasospasm with a guidewire [ 18 ] or ( 4 ) utilization of an anti - reflux infusion system [ 30 ] , ( 5 ) antibiotic usage [ 24 ] and repositioning of the microcatheter to change the flow direction [ 18 , 28 ] or ( 6 ) delivery of separate doses for right anterior and right posterior hepatic arteries [ 19 ] were all previously reported . our findings might only hold true for tare with glass particles . 
it is well known that because of the mildly larger size and larger number of particles , resin microspheres have more embolic effect over glass microspheres and this critical point may create a tendency to cholecystitis [ 31 ]  . 
in one case , there was a left kidney in left iliac fossa . conclusion although rare and probably overlooked , a plras can be encountered in patients with situs viscerum inversus or presenting a left - sided ivc with hemiazygos continuation . 
these vessels can cause technical problems during surgery at the left renal hilum and should be specifically searched for in patients with vascular anomalies . keywords renal vessels anomalies ivc hemiazygos continuation of ivc left - sided precaval renal artery * lorenzo e . 
gemelli , rome , italy 4 diagnostica perimmagini ospedaliera , ospedale evangelico internazionale , presidio ospedaliero di voltri , genoa , italy 5 department ofradiology , univ med pharm iuliu hatieganu , cluj - napoca , romania 6 department ofradiology , faculty ofmedicine , dokuz eylul university , izmir , turkey 7 department ofhealth sciences ( dissal ) , radiology section , university ofgenoa , radiologia durgenza , ospedale policlinico san martino ist , largo r . 
benzi , 10 , 16132genoa , italy introduction knowledge of the number , course and relationships of the renal arteries is of great importance for correct planning of surgical procedures to kidney , aorta and retroperitoneal region . 
 both anatomical and radiologic studies report the presence of vascular anomalies in about 30% of examined subjects [ 1 ]  . the right renal artery takes origin from the aorta and crosses the midline passing posteriorly to the inferior vena cava ( ivc )  . 
anomalous right renal arteries with precaval course ( prras ) can be encountered , and their presence has been associated with renal rotational anomalies and pelvic dilatation [ 2 , 3 ]  . to the best of our knowledge , there are no reports of left renal arteries with a precaval course ( plras )  . 
only one case with a complex vascular anomaly ( common renal arterial trunk originating from the aorta with a recurrent precaval and preaortic left renal artery ) has been described in vol . : ( 0123456789 ) 1 3 la radiologia medica ( 2019 ) 124 : 445449 446 fig . 
there is a left ivc ( open arrow ) with hemiazygos continuation which passes behind the left diaphragmatic crus ( c , d ) , gives a retroaortic branch to the azygos vein ( e ) and continues cranially as a small accessory hemiazygos ( curved arrow in f )  . 
b oblique reconstruction along the course of the left and lower right renal arteries shows the left ( open arrow ) and right ( arrowhead ) ivcs , as well as the two ( right and left ) renal arteries , both with a precaval course . 
we describe herein the imaging findings observed in eight patients in whom a plra was observed . materials andmethods we reviewed the teaching files of six radiologic departments for patients with lpras . 
 this study was approved , and the need for informed consent was waived by the ethics committee of the institution of the corresponding author . results all patients have been examined for problems not related to the vascular anomalies that are the object of the present study . 
 two patients had undergone evaluation of the chest ( one with unenhanced ct and one with mr ) , and the left - sided ivc and the plra were visible in the most caudal parts of the studies ; only selected images were available for review in these as well as in three other patients . 
 ( the patient had undergone unenhanced ct of the chest only . ) the remaining patient had situs viscerum inversus ; he had absent infrarenal right ivc , and the renal vein from the right kidney continued cranially into a vein interpreted as a right - sided hemiazygos . 
the hemiazygos passed between the left diaphragmatic crus and the vertebral bodies , gave a branch to the azygos vein , passing posteriorly to the aorta and then 1 3 case # ivc right renal artery left renal artery renal veins right kidney left kidney table 1 summary of imaging findings hemiazygos continuation of left ivc la radiologia medica ( 2019 ) 124 : 445449 non - visible normal normal plra plra plra non - visible normal normal normal normal normal retroaortic right normal normal renal vein main from iliac normal normal main artery normal ; accessory prra to lower pole artery ; accessory plra ectopic , left lower quadrant , with anterior malrotation normal normal normal plra plra plra normal normal normal normal normal normal normal left normal right to azygos left normal right to rightsided hemiazygos 448 non - visible double , right smaller left only double , right interrupted , continuing into hepatic collaterals . 
however , most left - sided inferior ivcs , at the level of the renal hilum , do not continue cranially , but flow into the left renal vein , which crosses the midline and then ascends as a right - sided ivc with a normal course to the right of the aorta . 
the same happens also in most patients with double ivc : the left one , again , flows into the left renal vein to join into a single ivc on the right side [ 5 ]  . 
embryologically , this is considered as due to persistence of the left supracardinal vein these cases , in fact , the left ivc turns backwards , passes between the left diaphragmatic crus and the lateral aspect of the vertebral bodies and ascends into the thorax . 
then , the left renal artery seems to run in a normal way , and it is the ivc that takes a course posterior to the artery . the findings observed in the patient with an ectopic left kidney and in the one with situs viscerum inversus are somewhat different and , possibly , the developmental anomalies causing the plra are also different . as regards the first case , it is known that ectopic kidneys have a higher number of associated vascular anomalies and that it is the final position of the kidney to determine the position and number of renal arteries . 
 we did not encounter a patient with combined presence of a left ivc without hemiazygos continuation and an ectopic kidney in the left lower inferior abdominal quadrant ; however , we believe that a plra could be possible also in this case . as regards the second one , it must be remembered that prras are considered the result of a persistent caudal vessel arising ventrally from the aorta after formation of the normal ivc [ 3 ]  . 
the same mechanism , but in the presence of a left - sided ivc due to situs viscerum inversus , could possibly explain the anomalous relationship between the two vessels . to the best of our knowledge , no attention has been paid to the relationship of the left renal artery with the ivc in the reported patients with a left - sided ivc and hemiazygos continuation [ 610 ]  . 
however , in one of the illustrations in a paper on multidetector ct of the ivc by sheith and fishman [ 11 ] , this anomaly seems present , but has not been described either in the caption or in the text . 
 [ 12 ] reported on a patient with left - sided ivc with hemiazygos continuation who underwent surgery for a nutcracker phenomenon affecting the right renal vethe paper shows a drawing illustrating the relationships among the vessels at the renal hilum in which the left renal artery is shown posteriorly to the ivc , but in the description of the surgical intervention , no special mention to this relationship was given . there are some limitations to our study . 
although a plra was recognized in all of our cases , we cannot exclude other relationships between the renal vessels and the left - sided ivc with hemiazygos continuation or other associated anomalies in a larger series of patients . to conclude , although rare and probably overlooked until now , a plra can be encountered in patients with situs viscerum inversus or presenting a left - sided ivc with hemiazygos continuation . 
it can be an additional cause of technical problems during retroperitoneal surgery at the left renal hilum and should be specifically searched for in patients with these vascular anomalies . funding this study has received no funding . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . informed consent this study was approved , and the need for informed consent was waived by the ethics committee of the institution of the corresponding author ( 335reg2014 )  . la radiologia medica ( 2019 ) 124 : 568574 ultrasonography clinical value ofhighresolution ( 517mhz ) echocolor doppler ( ecd ) foridentifying filling materials andassessment ofdamage orcomplications inaesthetic medicine / surgery mariascottodisantolo1 candidamassimo1 giovannitortora2 valeriaromeo1 micheleamitrano1 arturobrunetti1 massimoimbriaco1 received : 4 august 2017 / accepted : 5 december 2018 / published online : 5 january 2019 italian society of medical radiology 2019 abstract purpose the purpose of this retrospective study is to evaluate the role of echo - color - doppler ( ecd ) imaging in identifying a series of characteristics pursuant to aesthetic filling material such as their degree of absorbability and their potential complications which include their propensity to stimulate the formation of encapsulated foreign - body granulomas . 
in the latter case , ecd can be of aid by giving indication for surgical therapy . materials and methods over a 4 - year period , we studied 180 patients ( 60 ) who underwent an aesthetic medical / surgical treatment . 
we used ecd to evaluate the implant material , its thickness , the injection site , the integrity of dermal layers and the presence of any associated complications . results in 97% ( 174 / 180 ) of our patients , we were able to identify the type of material used ; furthermore , 57% of patients had a hyaluronic acid implant , 14% a lipofilling and 29% a non - absorbable filler ( with 10% of silicone )  . 
in 6 / 180 ( 3% ) , we could not recognize the material used ; 89% ( 161 / 180 ) of our patients presented post - injection complications ; moreover , 67% showed peri - implant dermalhypodermal thickening areas with adjacent lymphostasis , 6% displayed an abnormal implant site , and 17% showed inflammation with encapsulated foreign - body granulomas that required subsequent surgical excision . 
 biopsy samples were obtained from 37 / 180 patients ( 21% ) ; among these , 31 patients had an ecd evidence of granuloma and on 6 patients we were not able to define the injected material . 
bianchi , naples , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 568574 introduction high - resolution ( 517mhz ) color - doppler ultrasound ( ecd ) is widely used in the evaluation of normal and pathological skin [ 19 ] ( figs.1a , b , 2 ) ; it plays an important role in aesthetic medicine / surgery , in the filling technique , in identifying filling materials and in the assessment of subsequent damage or complications [ 1020 ] ( table1 )  . 
 in the study of superficial organs and in particular in the dermatological field , the depth of the region to be investigated is 12cm and pathological skin lesions are often less then 1mm thick ; as a result , the use of high - frequency / high - resolution / reduced scan depth probes is crucial [ 1 , 2 ]  . 
the lesion is hyper vascular with regular margins there are several types of fillers : absorbable , non - absorbable , synthetic and autologous adipose tissue in the lipofilling technique . among the absorbable fillers , the most used is hyaluronic acid ( pure or mixed with lidocaine ) which is a glycosaminoglycan component of the dermis consisting of long , unbranched chains of disaccharide units . 
the mixed formulation ( hyaluronic acid and lidocaine ) appears as a circumscribed hypoechoic areolae with regular margins localized in the dermis or subcutaneous adipose tissue or as pseudocysts with inner echoes ( debris ) and septa [ 11 , 13 , 1517 ] ( table1 )  . 
polymethylmethacrylate appears as hyperechoic dots with a small comet tail artifact , and calcium hydroxyapatite appears as hyperechoic bands with a posterior acoustic shadowing artifact ; the latter artifact is the one classically described in calcified structures [ 1113 , 1517 ] ( table1 )  . polyacrylamide gel , another synthetic filler , appears as mostly oval anechoic pseudocysts with increased echogenicity of the surrounding subcutaneous tissue [ 1113 , 1517 ] ( table 1 ) ; its deposits have been reported to not change in size at least for 1year [ 1117 ] ( table1 )  . the most well - known non - absorbable filler is silicone ( pure or in oily formulations ) whose medical aesthetic use was forbidden in the usa in 1991 and in italy in 1992 because of the high incidence of complications [ 11 , 13 , 15 , 16 ] ( table1 )  . 
silicone echo - genicity depends on the formulation type ; pure silicone is anechoic , similar to intact breast implants , while silicone oil is hyperechoic , with posterior reverberation / scattering artifact ( snow - storm appearance ) , similar to ruptured silicone implants when pure silicone is fig . 
1 a longitudinal scan of healthy skin on the dorsal region of the arm in a 36 - year - old male with mild photo aging ; sonographic representation of all the layers of the dermis , epidermis and subcutaneous adipose tissue . 
b longitudinal scan of the healthy nail bed in a 30 - year - old woman patient 1 3 570 la radiologia medica ( 2019 ) 124 : 568574 table 1 filler materials characteristics observed on ecd hyaluronic acid glycosaminoglycan component of the dermis consisting anechoic pseudocysts that decrease in size over 3 to of long , unbranched chains of disaccharide units 6months in pure formulation pseudocysts with inner echoes ( debris ) and septa in mixed formulation hyaluronic acid and lidocaine collagen bovine glycosaminoglycan component of the dermis consisting anechoic pseudocysts that decrease in size over 3 to of long , unbranched chains of disaccharide units 6months poly - l - lactic acid synthetic , biodegradable , biocompatible , immunologianechoic pseudocysts that decrease in size over 3 to cally inert peptide polymer 6months silicone highly purified long - chain polydimethylsiloxane pure silicone implant appeared anechoic , similar to echotrimethylsiloxy - terminated silicone oil genicity described in intact breast implants calcium hydroxyapatite synthetic filler , semi - permanent inorganic material hyperechoic bands with a posterior acoustic shadowing polymethylmethacrylate synthetic filler , semi - permanent inorganic material lipofilling grafting autologous adipose tissue silicone oil was hyperechoic , showing a posterior reverberation or scattering artifact , similar to the one seen in ruptured silicone implants when the pure silicone is mixed with the fatty tissue of the breast artifact hyperechoic dots with a mini comet tail artifact area of hyper echo - genicity with regular margins corresponding to the implanted adipose tissue mixed with the fatty breast tissue [ 1113 ] ( table1 )  . 
finally , the lipofilling technique consists in grafting autologous adipose tissue to correct soft tissue volumetric defects secondary to trauma , cancer excisions , congenital defects and aging [ 2 , 12 ] ( table1 )  . 
among the most frequent complications is the foreign - body reaction ( initial inflammation and subsequent granuloma formation ) , whose recognition is crucial to direct the patient to surgery . 
less common adverse reactions include fistulous tracts of fluid collections , skin necrosis due to intravascular filler injection and secondary capillary or larger - vessel thrombosis [ 1820 ]  . 
the aim of this study is to evaluate the role of ecd in identifying different types of filling material , their possible complications and the accuracy of ecd in diagnosing and indicating treatment for possible subsequent foreign - body granulomas . materials andmethods our retrospective study was performed on material and data available in our department in accordance to the 1964 declaration of helsinki ethical standards ( and its subsequent amendments )  . 
exclusion criteria were : pregnancy or breast - feeding , general contraindication to surgical or aesthetical procedures and psychological problems . over a 4 - year period ( january 2012september 2015 ) , 180 patients ( 60 ) aged between 20 and 76years were evaluated with ecd after the aesthetic treatment to identify filler materials , to evaluate the possible resulting damage and post - op complications , especially the onset of persistent ecchymosis and nodules . 
ecd was performed by a 16 - year experienced operator ( msds ) on the affected skin region using a high - frequency transducer ( 517mhz ) and a philips iu22 ultrasound device ( best , the netherlands )  . 
the echostructure and echo - genicity of the dysmorphic region was studied in order to evaluate the implant type ( table1 ) , its thickness , the site of implantation , dermal layer integrity , the presence of a newly formed granuloma ( capsulated or not ) , vascularization and inflammation ( using slow - flows ecd settings )  . 107 / 180 patients showed the presence of filler within the nasolabial folds , 21 / 180 patients showed filler lips , 50 / 180 cheekbones filler , 1 patient showed filler at the level of a sternal scar and 1 patient into the arms ( table2 )  . 
ecd foreign - body granuloma diagnosis was based on the visualization of an inhomogeneous hypoechoic collection with some internal echoes with or without a hyperechoic peripheral rim ( capsule ) exhibiting a rich vascular supply on color - doppler 1 3 la radiologia medica ( 2019 ) 124 : 568574 table 2 filler materials characteristics observed on ecd , in 180 patients studied after filler treatment , injection sites number of patients filling material identified sonographically injection sites hyaluronic acid lipofilling calcium hydroxyapatite polymethylmethacrylate silicone material unidentified clearly nasolabial folds ( 75 ) lips ( 14 ) cheekbones ( 10 ) nose ( 1 ) nasolabial folds ( 19 ) cheekbones ( 3 ) lips ( 1 ) sternum ( 1 ) cheekbones ( 25 ) nasolabial folds ( 6 ) nasolabial folds ( 2 ) cheekbones ( 12 ) lips ( 5 ) nasolabial folds ( 5 ) lips ( 1 ) fig . 
4 ultrasound examination obtained in the transverse view at the level of skin region affected by dimorphism ( sternum ) and at the adjacent region , showing measurement of the autologous fat implant fig . 
3 longitudinal scan of nasolabial groove in a 40 - year - old woman shows hyaluronic acid implant 10 days after treatment , well located and without ultrasonographic evidence of complications examinations . 
 the vascular signal was evaluated at the injection site using colorand power - doppler functions set to slow speed blood flow ( color doppler : prf 500hz , wall filter 27hz , gain 75% , persistent media ; power doppler : prf 350hz , wall filter 45hz , gain 85% , low optimization ) [ 1 , 2 ] , therefore providing a flow qualitative analysis as well as the peak systolic velocity [ 1 , 2 ]  . results ecd was able to identify the type of filler material used in medical treatments and cosmetic surgery according to data already present in the literature ( table1 )  . 
5 longitudinal scan of biceps in a 43 - year - old man shows ultrasonographic evidence of diffuse and large area of ultrasound beam attenuation as traditional silicone implant patients ( 97% ) , we identified the type of material used ( table2 )  . 
 50 / 174 ( 29% ) patients had a non - absorbable filler implant ( tables1 and 2 ) primarily calcium hydroxyapatite ( 36 / 50 , 72% ) which appeared as hyperechoic bands with a posterior acoustic shadowing artifact ( table1 and 2 )  . 
14 / 50 ( 28% ) patients had another type of non - absorbable filler , polymethylmethacrylate , which appeared as hyperechoic dots with a mini comet tail artifact ( table1 and 2 )  . 
in 20 / 180 ( 11% ) patients , ecd showed previous undeclared implants , 5 ( 3% ) 1 3 572 table 3 complications observed on ecd in 161 / 180 patients studied after filler treatment la radiologia medica ( 2019 ) 124 : 568574 number of complications type of complications locations lymphostasis abnormal implant site hyaluronic acid granuloma polymethylmethacrylate granuloma hydroxyapatite granuloma nasolabial folds ( 108 ) lips ( 5 ) cheekbones ( 7 ) suprafascial cheekbones ( 10 ) nasolabial folds ( 11 ) lips ( 2 ) nasolabial folds ( 6 ) nasolabial folds ( 5 ) cheekbones ( 2 ) previous undeclared silicone implant granuloma lips ( 5 ) fig . 
transverse view showing the inflammatory reaction after filler treatment of these were silicone implants with a foreign - body granuloma allowing to avoid a second aesthetic treatment and preventing possible medical legal issues ( fig.5 ; tables2 and 3 )  . 
in 6 / 180 patients ( 3 , 3% ) , we could not recognize the material used because of the intense adjacent inflammation and because of the evidence of repeated different absorbable filler treatments ( table3 )  . 
6 a longitudinal scan of zygomatic region in a 42 - year - old woman who complained of pain and swelling , 1month after the aesthetic treatment ; abnormal implant site ( suprafascial cheekbones )  . 
biopsy samples were obtained from 37 patients , 31 ( 17% ) with us evidence of encapsulated foreign - body granulomas and 6 in which ecd was not able to successfully define the injected material . 
 among these , 5 specimens that were identified sonographically as silicone granulomas showed empty vacuoles surrounded by fibrous tissue , giant cells with cytoplasmic phagocytosed silicone particles and inflammatory cells . 
as for the 6 patients in which ecd could not define filler material , histology determined the presence of intense chronic inflammation with macrophages , giant cells ( fig.7 ) ; 3 / 6 ( 50% ) also showed cystic granulomas including hyaluronic acid . 
 a comparison between histological results and ultrasound diagnosis is shown in table4 . discussion the results of this study show that ecd can identify different filling materials and possible post - surgical complications ; in addition , when performed by an expert sonographer and with the state of the art technique , ecd shows a 78% diagnostic accuracy in identifying the presence of foreign - body encapsulated granulomas , directing the patient to the most appropriate surgical procedure . 
the use of us in the dermatological field is strongly tied to a series of innovations : the availability of high - frequency transducers ( > 15mhz ) , the introduction of techniques that reduce artifacts while optimizing resolution power and the possibility of studying both the vascularization of expansive skin lesions and angiogenesis with the color - doppler function [ 1 , 2 , 4 , 5 , 9 , 11 , 1317 ]  . 
the massive recourse to medicine and cosmetic surgery in a perpetual pursuit of beauty has increased the number of legal medical practices and , as a consequence , also the number of medical errors and complications related to the type of equipment used . 
a skin ultrasound , performed by doctors with sonography and cosmetic medicine experience , allows for the recognition the type of material used , the exclusion of the presence of silicone , of great importance for subsequent medical legal issues and the evaluation of possible complications in time . 
this will provide both qualitative and quantitative data ( volumetric follow up of implant material dimension through repeated us ) regarding the successful resolution of a potential problem [ 11 , 13 , 1520 ]  . 
sonographically , the granuloma is not easy recognized ; it can either have a thick hypoechoic rim or , if fibrotic phenomena prevail , a hyperechoic rim that shows vascular signal at color and power doppler especially if there is associated inflammation . 
in our study , us was also helpful in patients with foreign - body granulomas caused by post multidistrict infiltration of acidlidocaine ; in this case us targeted the infiltration of hyaluronidase which allowed for resolution . 
our study shows the importance of us in recognizing different types of filling materials used in medicine and cosmetic surgery procedures as well as their complications ; it can also help to identify previous implants that were not declared by the patient . 
this noninvasive , precise and detailed diagnostic methodology is of great value especially to those patients who usually have a high cosmetic expectancy and try to avoid invasive procedures such as biopsies [ 1120 ]  . conclusion ecd is a low - cost widespread noninvasive diagnostic tool that allows the identification of filling materials used as well as the evaluation of damage and complications from aesthetic medicine / surgical treatments [ 47 , 917 ]  . 
diagnostic accuracy of the dect maps ( qualitative assessment ) and of the ct numbers ( quantitative assessment ) , interobserver and intraobserver agreements were calculated . results mri revealed 61 edematous vertebrae and 52 collapsed non - edematous vertebrae . 
 dect numbers were significantly different between positive ( mean 23 hu , range 189 , 29 hu ) and negative cases ( mean 126 hu , range 321 , 66 hu ) with p < 0.001. 
sempreboni 10 , 37024negrar , vr , italy 2 department oforthopaedic surgery , irccs sacro cuore don calabria hospital , negrar , italy 3 department ofanesthesia andanalgesic therapy , irccs sacro cuore don calabria hospital , negrar , italy introduction vertebral compression fractures represent a common clinical problem , especially in the elderly population , and are associated with a decreased quality of life and increased mortality [ 1 , 2 ]  . 
common causes of vertebral compression fractures include postmenopausal osteoporosis , where skeletal mass and bone strength diminish with the aging process , trauma , malignancies and secondary osteoporosis [ 3 ]  . 
for example , percutaneous vertebroplasty stabilizes the fracture and strengthens the vertebrae immediately after the procedure [ 5 , 6 ]  . imaging procedures such as magnetic resonance ( mr ) imaging , bone scintigraphy and computed tomography ( ct ) help to determine the treatment choice and relative location [ 7 ]  . 
however , mri cannot be routinely vol . : ( 0123456789 ) 1 3 488 la radiologia medica ( 2019 ) 124 : 487494 used in all patients in the acute settings owing to reduced availability , contraindications and / or metal artefacts . 
also , ct is commonly used in trauma to rule out thoracic and abdominal traumatic lesions [ 14 ]  . with the advancements in dual - energy ct ( dect ) technology , material decomposition and the elimination of misregistration artefacts are possible [ 15 ]  . 
 also dect have been successfully used to evaluate abdominal and pelvic trauma [ 20 ]  . the possibility to demonstrate acute vertebral fractures by using dect have been shown in previous studies using second generation scanners [ 4 , 8 ]  . 
 [ 22 ] focused on the performance of 5 readers and used both a second and a third - generation dual - source scanner , although the number of patients studied with the newer dual - source ct was relatively limited . the purpose of our study was to investigate the reproducibility of dect in the evaluation of vertebral fractures and bone marrow edema with a 384 - slice third - generation systethe diagnostic accuracy values of dect were calculated by using mri as the standard of reference . materials andmethods patient population this prospective study was approved by the institutional review board , and all patients provided informed consent . 
five patients were excluded because of non - mri - compatible pacemaker ( n = 3 ) , incomplete mri protocol ( n = 1 ) and claustrophobia ( n = 1 )  . 
one pathologic fracture due to tumor infiltration and three vertebral bodies with subtotal vertebral collapse were excluded from this study . dect protocol the dect examinations were performed with a third - generation 384 - slice dual - source ct scanner ( somatom definition force , siemens healthcare , forchheim , germany )  . 
the predefined tube currenttime product was set at a ratio of 1.6 : 1 ( tube a , 220 quality reference mas ; tube b , 138 quality reference mas )  . 
 soft - tissue kernel ( qr32 ) 80 - kvp and 150 - kvp set images were transferred to an offline workstation ( syngovia vb20 ; siemens , erlangen , germany )  . the software uses a three - material decomposition resulting in a virtual non - calcium image . 
the information was color - coded with a color lookup table which codes bone marrow and edema in shades of green - yellow to orange - red ( parallely to the progressive increase of density ) ; 3d volume rendering maps coding bone marrow edema in shades of green and normal bone in blue were also available . 
the de - specific information was fused with the conventional grayscale morphologic images ( thickness , 1mm ; increment , 1mm )  . mri protocol mr imaging was performed with a commercially available 1.5 - t unit ( magnetom avanto fit ; siemens healthcare , erlangen , germany )  . 
standard t1 - weighted spin echo , t2 - weighted turbo spin echo , and turbo inversion - recovery magnitude ( tirm ) sequences were performed in the sagittal orientation . 
mr imaging parameters are summarized in table1 . image analysis on all images datasets available , each vertebral body was evaluated for the presence of bone marrow edema using a binary classification system ( 1 = presence of fracture / bone marrow edema and 0 = absence of acute findings )  . as the standard of reference , all mr images were evaluated in random order , by an experienced radiologist ( 20years of experience ) blinded to ct findings . 
the vertebral bodies were graded as normal ( grade 0 ) , minimal fracture ( grade 1 with 2025% decrease in anterior , middle , and / or posterior height ) , moderate fracture ( grade 2 with 2540% decrease in height ) , and severe fracture ( grade 3 with > 40% decrease in height )  . standard axial , coronal and sagittal reconstructed ct and dect images ( 3d and 2d color - coded maps ) were analyzed by two independent radiologists ( 35 and 15years of experience in radiology , respectively ) in a random order , blinded to clinical and mri findings on a dedicated syngovia workstation . 
to determine the intraobserver agreement , the dect images were re - evaluated randomly after 30days . quantitative analysis of dect numbers was performed by achieving two circular regions of interest ( roi ) for each vertebral body , placed on the suspected area , and using mean value for further analysis [ 8 ]  . 1 3 490 statistical analysis the statistical analyses were performed with statacorp . 
mri images served as the standard of reference . table 2 clinical data of patients enrolled la radiologia medica ( 2019 ) 124 : 487494 the receiver operating characteristic ( roc ) curve analysis and calculations of the area under the roc curve ( auc ) were used to evaluate the attenuation values from dect scans . 
the sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy of dect for the diagnosis of vertebral fracture were calculated on a per - vertebra basis both as regards qualitative and quantitative assessment . 
2 sixty - two - year old man with traumatic acute dorso - lumbar pathe mri study ( 3a ) shows a grade 1 acute fracture of l1 vertebral body , with mild hyperintensity on the sagittal tirm image ( yellow arrow )  . 
 on the sagittal reconstructed dect color - coded image ( 3b ) the bone marrow edema is confirmed by the presence of shades of green ( yellow arrow )  . 
 on the parasagittal 3d dect map ( 3c ) , the acute fracture can be easily recognized appearing green ( yellow arrow ) , while the normal vertebral bodies are coded in blue 1 3 la radiologia medica ( 2019 ) 124 : 487494 fig . 
3 sixty - four - year old woman with atraumatic acute lumbar pathe mri study ( 4a ) shows a grade 1 acute fracture of l4 vertebral body , with mild hyperintensity on the sagittal tirm image ( yellow arrow )  . 
 on the sagittal reconstructed dect color - coded image ( 4b ) and on the parasagittal 3d dect map ( 4c ) , the bone marrow edema is confirmed by the presence of shades of green ( yellow arrow )  . 
in line with previous studies [ 8 , 15 , 21 , 22 ] , our results demonstrated that dect represents a reliable imaging technique for the identification of fresh fracture and to rule out the presence of bone marrow edema in the case of non - edematous collapsed vertebral bodies . 
used a cutoff value of - 80 hu for the ct numbers , obtaining a sensitivity of 96.3% , a specificity of 98.2% , and an overall accuracy of 97.6% in the subgroup of vertebral bodies with less than 50% sclerosis and / or air . 
although we did not perform a sub - analysis of sclerotic vertebral bodies , we obtained a relatively high value of overall accuracy that could be explained by the advancement in vnc post processing technique . 
 by using a cutoff of 47 hu ( similar to our 50 hu threshold ) , the authors obtained a sensitivity of 92.0% , specificity of 82.6% , accuracy of 84.0% , positive predictive value of 48.9% , and negative predictive value of 98.3% for the differentiation of edematous vertebral bodies . in the study of kaup etal . 
the multiplanar reformatted 2d color - coded maps , created and superimposed to the bone window grayscale dataset , were the most adequate for the evaluation of bone marrow edema . 
 the level of superimposed map can be modified from a level showing only the colors of the map to a level showing only the standard grayscale ct images : this allowed us to evaluate traditional ct images and color - coded maps together , reducing reading time . 
 in this case , the sclerosis caused an abnormal subtraction process , covering the bone marrow edema on color - coded maps with subsequent misdiagnosis . our study population was relatively younger compared with the populations in the studies by wang etal . 
 however , as previously stated , our findings confirmed that the diagnostic accuracy of dect in depicting bone marrow edema tends to increase in patients with osteoporotic bone structure because of the prevalence of fatty instead 1 3 la radiologia medica ( 2019 ) 124 : 487494 of red bone marrow and reduced trabecular bone structures [ 8 , 21 ]  . 
however , as previously described , the mean age of patients enrolled in our study was inferior when compared to the populations of similar studies [ 8 , 22 ]  . 
moreover , a comparative analysis of qualitative versus quantitative analysis was not performed ; as previously discussed , we believe that the dect numbers and dect maps are strictly correlated , so that the quantitative analysis could represent an additional tool that helps radiologists to discriminate subtle imaging findings . 
any abnormal middle ear attenuation on high - resolution ct images ( hrct ) or dect color - coded maps , and any abnormal signal on mri images was evaluated by four experienced radiologists . 
ct numbers were significantly different between positive ( mean 57.6hu , range 65 , 112hu ) and negative cases ( mean 5.4hu , range 100 , 66hu ) with p < 0.001. 
the disease is treated surgically often followed by a second - look approach to check for residual tissue or recurrence [ 4 ]  . high - resolution computed tomography ( hrct ) of the temporal bone is widely accepted to detect cholesteatoma and to assess the extension and possible complications of the disease [ 5 ]  . 
however , ct opacity is nonspecific for vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 478486 cholesteatoma , and the diagnosis is based on the high specificity of lesion location and patterns of bone erosion [ 6 ]  . 
 also , ct is not reliable in case of atypical locations , especially to distinguish recurrence from postoperative changes [ 68 ]  . because of its high keratin content , cholesteatoma has specific signal - intensity characteristics on magnetic resonance imaging with very high signal intensity on diffusionweighted imaging ( dwi ) at high b value ( 8001000s / mm2 ) [ 911 ]  . 
however , mri cannot be routinely used in all patients with suspected cholesteatoma owing to reduced availability , contraindications and / or metal artifacts . with the advancements in dual - energy ct technology ( dect ) , material decomposition and the elimination of misregistration artifacts are possible [ 15 ]  . 
materials , particularly those with high atomic weight numbers ( e.g. , iodine and calcium ) , display different attenuation measurements at different kilovoltage peak levels [ 16 , 17 ]  . 
dect has been proposed to demonstrate the presence of bone marrow edema in vertebral compression fractures , to evaluate brain hemorrhage and iodine extravasation in the brain [ 1823 ]  . 
 however , dect has not yet been proposed for the evaluation of cholesteatoma . in the setting of a filled hypodense post - surgical cavity with suspect of local recurrence or residual disease , dect materials decomposition capabilities could be potentially used to differentiate cholesteatoma from other non - cholesteatomatous tissues ( i.e. , trapped fluids , granulation tissue )  . thus , the purpose of our study was to prospectively evaluate the diagnostic accuracy of dect and mri to identify residualrecurrent cholesteatoma using the second - look surgery as the reference standard . materials andmethods patient population this prospective study was approved by the institutional review board , and all patients provided informed consent . 
six patients were excluded because of non - mri - compatible pacemaker ( n = 2 ) , incomplete mri protocol ( n = 1 ) , claustrophobia ( n = 1 ) , and absence of surgical correlation ( n = 2 )  . 
1 flowchart with inclusion and exclusion criteria of patients enrolled in previously surgically treated ears ( fetid discharge , pain , hear deterioration ) or presence of soft tissue density mass in the surgical cavity at standard ct . dect protocol the dect examinations were performed with a third - generation 384 - slice dual - source ct scanner ( somatom definition force , siemens healthcare , forchheim , germany ) [ 15 ]  . 
 soft tissue kernel ( qr32 ) 80 - kvp and 150 - kvp set images were transferred to an offline workstation ( syngovia vb20 ; siemens , erlangen , germany )  . 
a customized postprocessing based on the de liver virtual non - contrast application [ 1619 ] was used in order to enhance subtle differences between tissues with similar , intermediate density . 
the images were evaluated by two independent radiologists ( xx and xx with 35 and 15years of experience in radiology , respectively ) in a random order , blinded to clinical and mri findings . 
the maps were available on three planes ; each reader was free to modify window settings and imaging parameters including slice thickness , magnification , and level of superimposition between hrct images and color - coded maps . 
moreover , standard hrct images were always available for review on a dedicated window in order to correlate the maps with the presence of subtle erosions and for anatomical reference . 
in particular , by using the default settings of the fat map , a tissue appearing in blueviolet on the look - up table was coded cholesteatoma , whereas the tissues coded in gray / yellow were characterized as scar and trapped inflammatory fluid , respectively . for any disagreement on presence of cholesteatoma , a consensus reading was appended , and the consensual results were used for further analysis . 
quantitative analysis of dect numbers was performed on the blended images on syngovia software by achieving two circular regions of interest ( roi ) for each ear , covering half to 2 / 3 of the suspected soft tissue mass ( identified on the dect maps or on standard reconstruction according to the reader choice ) , and using mean value for further analysis . the mr examinations were analyzed in a separate session , in random order , by two blinded radiologists ( xx and xx , 25 and 5years of experience in radiology , respectively )  . 
surgery served as the standard of reference . the sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy of the dect color - coded maps ( qualitative analysis ) and of the ct numbers ( quantitative analysis ) , and of the mri images for the diagnosis of residual or recurrent cholesteatoma were calculated on a per - ear basis . 
interobserver and intraobserver agreement for the qualitative analysis were calculated with weighted k statistics . for the quantitative analysis , the receiver operating characteristic ( roc ) curve analysis and calculations of the area under the roc curve ( auc ) were used to evaluate the attenuation values from dect scans . 
the ear - based results and relative diagnostic performance values of the imaging methods employed are shown in tables2 and 3 , respectively . surgical andpathological results at surgery , the diagnosis of cholesteatoma was obtained in 16 / 24 ears ( 66.6% recurrence rate ) because of the presence 1 3 la radiologia medica ( 2019 ) 124 : 478486 table 1 clinical data in 19 patents / 24 ears with 16 residual / recurrent cholesteatoma parameter value aage ( years ) aage of male ( years ) aage of female ( years ) no of male no of female treated on one side only treated on both sides canal wall up technique canal wall down technique total cholesteatomas single cholesteatomas bilateral cholesteatomas right lesions left lesions 62 . 
on the coronal reconstructed highresolution ct image of the left ear ( a ) , intermediate density tissue can be depicted within the surgical cavity , without significant erosions ( thin arrow )  . 
by using an algorithm intended for the evaluation of liver fat content to create color - coded maps , an overall accuracy of 87.5% in determining the presence versus the absence of residual or recurrent cholesteatoma was achieved , without any significant difference with respect to dwi images . 
an additional explanation is that the structural properties of cholesteatoma , rich of keratin proteins , could have led to its appearance on dect . in line with the results of previous studies [ 26 , 27 ] , conventional imaging signs on hrct images alone allowed us to depict cholesteatoma in 4 of 16 ears following mastoid 1 3 la radiologia medica ( 2019 ) 124 : 478486 fig . 
on the coronal reconstructed high - resolution ct image of the right ear ( a ) , a thickened hypodense fold ( thin arrow ) can be depicted without erosive changes of the adjacent neo - cavity wall and without signal changes on coronal dwi image ( b )  . 
the high overall accuracy of mri could be also explained by the absence of cholesterinic granulomas or other confounding lesions in our series . sensitivity , specificity , ppv , npv and accuracy of dect maps were 87.5%. 
an additional peripherally located lesion , missed at mri as well , was misdiagnosed as a fn at dect maps both from reader 1 and reader 2 . one false positive shared by mri , and dect ( for both readers ) was represented by a squamous cell carcinoma : the lesion was misdiagnosed at mri because of its dwi hyperintensity but lack of significant contrast enhancement . 
at dect , an intermediate density lesions were depicted , coded in blueviolet on the maps , which was consistent with the incorrect diagnosis of cholesteatoma . at dect , an additional fp for reader 2 was due to the presence of an earwax plug left from previous surgery . 
in particular , cholesteatomas represented high density tissue on the maps and were coded as blueviolet , whereas fluid and scars represented medium and low density areas and were coded as yellow and gray , respectively . 
conversely , inflammatory fluid and cholesteatoma were relatively spared from this subtraction process , showing medium and high density values ( with dect numbers similar to those expected on conventional ct images )  . 
moreover , when considering the intended use of the color - coded maps employed , we may argue that inflammatory fluid and cholesteatoma were coded as yellow and blueviolet areas on the color - coded maps , respectively , as expected for fatty and non - fatty areas of the liver . this study had some limitations . 
first , few patients were enrolled and larger series are need to confirm our preliminary results ; also , a possible selection bias may depend on the enrollment of patients with high clinical suspicion of residual / recurrent cholesteatoma . 
although the methods described in this paper represent a reproducible approach , new dedicated decomposition algorithms would be desiderable and could lead to more reliable results in the future . in conclusion , by using surgical and pathological data as the standard of reference , both mri and dect provided an accurate demonstration of residual / recurrent cholesteatoma . 
 1 3 la radiologia medica ( 2019 ) 124 : 478486 while mri can be considered the most accurate imaging method , dect may represent a promising imaging tool in patients with contraindications for mri . 
sarmento kma jr , sampaio all , santos tgt etal ( 2017 ) highfrequency conductive hearing loss as diagnostic test for incomplete ossicular discontinuity in non - cholesteatomatous chronic suppurative otitis media . 
ms - estells f , mateos - fernndez m , carrascosa - bisquert b etal ( 2012 ) contemporary non - echo - planar diffusion - weighted imaging of middle ear cholesteatomas . 
alvo a , garrido c , salas etal ( 2014 ) use of non - echo - planar diffusion - weighted mr imaging for the detection of cholesteatomas in high - risk tympanic retraction pockets . 
dremmen mh , hofman pa , hof jr etal ( 2012 ) the diagnostic accuracy of non - echo - planar diffusion - weighted imaging in the detection of residual and / or recurrent cholesteatoma of the temporal bone . 
chen s , ikawa f , kurisu k etal ( 2001 ) quantitative mr evaluation of intracranial epidermoid tumors by fast fluid - attenuated inversion recovery imaging and echo - planar diffusion - weighted imaging . 
aikele p , kittner t , offergeld c etal ( 2003 ) diffusion - weighted mr imaging of cholesteatoma in pediatric and adult patients who have undergone middle ear surgery . 
palmer we , simeone fj ( 2018 ) can dual - energy ct challenge mr imaging in the diagnosis of focal infiltrative bone marrow lesions ? radiology 286 ( 1 ) : 214216 . 
petritsch b , kosmala a , weng am etal ( 2017 ) vertebral compression fractures : third - generation dual - energy ct for detection of bone marrow edema at visual and quantitative analyses . 
mallinson pi , coupal tm , mclaughlin pd et al ( 2016 ) dual - energy ct for the musculoskeletal syste radiology 281 ( 3 ) : 690707 ( review ) 22 . 
bodanapally uk , shanmuganathan k , issa g etal ( 2018 ) dualenergy ct in hemorrhagic progression of cerebral contusion : overestimation of hematoma volumes on standard 120 - kv images and rectification with virtual high - energy monochromatic images after contrast - enhanced whole - body imaging . 
bonatti m , lombardo f , zamboni ga etal ( 2018 ) iodine extravasation quantification on dual - energy ct of the brain performed after mechanical thrombectomy for acute ischemic stroke can predict hemorrhagic complications . 
magarelli n , de santis v , marziali g etal ( 2018 ) application and advantages of monoenergetic reconstruction images for the reduction of metallic artifacts using dual - energy ct in knee and hip prostheses . 
hu r , daftari besheli l , young j etal ( 2016 ) dual - energy head ct enables accurate distinction of intraparenchymal hemorrhage from calcification in emergency department patients . 
osman nm , rahman aa , ali mt ( 2017 ) the accuracy and sensitivity of diffusion - weighted magnetic resonance imaging with apparent diffusion coefficients in diagnosis of recurrent cholesteatoma . 
when biliary communication is clearly shown on t2w haste sequences , it should be reported as cysto - biliary communication even if there is no leakage of gadoxetic acid into the cyst on ce - mrcp . keywords biliary system gadoxetic acid hydatid cyst magnetic resonance cholangiopancreatography introduction hydatid disease is a widespread zoonosis and more commonly seen in the mediterranean area [ 1 , 2 ]  . 
no : 1 , umraniye , 34764istanbul , turkey 2 general surgery department , university ofhealth sciences umraniye training andresearch hospital , istanbul , turkey there are some major complications of hydatid cyst . 
 the rupture of the cyst into peritoneal cavity which leads to peritonitis , transdiaphragmatic rupture into thorax , or rupture into biliary system and abscess formation are lifethreatening complications [ 2 , 4 ]  . 
if there is any suspicion of biliary communication in hydatid cyst , surgical procedures such as cystectomy and unroofing with primary closure of biliary communication can be preferred [ 3 , 5 ]  . 
therefore , preoperative diagnosis of cysto - biliary communication is vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 460466 necessary for selecting the most appropriate treatment option , guiding surgical planning , and decreasing the risk of mortality of the patient . magnetic resonance imaging ( mri ) is usually performed for the detection of complications . 
there are two kinds of hepatobiliary - specific contrast agent : gadobenate dimeglumine ( gd - bopta , multihance ; bracco imaging , milan , italy ) and gadoxetic acid ( gd - eob - dtpa , primovist ; bayer pharma ag , berlin , germany )  . 
contrast - enhanced magnetic resonance cholangiopancreatography ( cemrcp ) is performed by administration of gadoxetic acid because of its hepatobiliary specificity and high biliary excretion ( 50% ) [ 8 ]  . the aim of our study was to evaluate the effectiveness of ce - mrcp and t2 - weighted half - fourier acquisition singleshot turbo spin - echo ( t2w haste ) sequences for diagnosis of cysto - biliary communication in hydatid cysts compared to surgical results . 
we aimed to present the results and our experiences about ce - mrcps of hepatic hydatid cysts with biliary communication . materials andmethods patients the institutional review board approved this retrospective study , and informed consent was waived . 
between october 2014 and october 2016 , at a single institution , 52 consecutive patients who underwent surgery because of hepatic hydatid cysts were reviewed from our hospitals picture archiving and communications systewe excluded a total of seven patients : six without preoperative mri examinations and one patient with suboptimal image due to patient motion and susceptibility artifacts . 
a final cohort of 45 patients [ 21 ( 46.70% ) men and 24 ( 53.30% ) women with a mean age of 45 15 ( sd ) years ( range 2067years ) ] were included in our study and preoperative abdominal contrastenhanced mri examinations were reviewed . 
there were no patients with > 3mg / dl serum bilirubin level which causes insufficient visualization of the biliary system in ce - mrcp due to diminished biliary excretion . magnetic resonance imaging andimage evaluation all mris were performed on a 1.5 tesla system ( magnetom avanto , siemens healthineers , erlangen , germany )  . 
the parameters of routine abdominal mri sequences were as follows : coronal t2w haste [ tr / te : 2000 / 130 , field of view ( fov ) : 420mm , slice thickness 7mm ] , axial t2 - weighted haste ( tr / te : 2000 / 162 , fov : 440mm , flip angle 90 , slice thickness 6mm ) with and without fat saturation , spoiled dual - gradient echo t1 - weighted inand opposed - phase mr imaging ( tr / te : 209209 / 2.34.8 , slice thickness 7mm ) , axial precontrast and postcontrast dynamic t1 3d vibe ( tr / te : 800 / 22 , fov : 440mm , slice thickness 5mm ) sequences . 
 in 27 patients , 0.1ml / kg ( 0.25mmol / kg ) gadoxetic acid was intravenously administered as a contrast agent at a rate of 2ml / s , followed by a bolus of 20ml saline . 
on t2w haste sequences , extension or contact of an intrahepatic bile duct with the contour of the cyst and also focal dilatation of a bile duct near the contour defect of the cyst were accepted as positive findings for cysto - biliary communication . 
 these roi measurements inside the cyst were performed on non - contrast t1 - weighted sequence , hepatobiliaryspecific delayed phase , at 1 - h , 2 - h , and 24 - h delayed t1 - weighted sequences after contrast injection . 
the degree of observer agreement , as indicated by kappa coefficients ( k ) , was interpreted as follows : 00.20 , slight agreement ; 0.210.40 , fair agreement ; 0.410.60 , moderate agreement ; 0.610.80 , substantial agreement ; and 0.811.00 , almost perfect agreement [ 10 ]  . results a total of 45 patients with 45 hepatic hydatid cysts were enrolled in our study . 
the excretion of contrast agent into the intrahepatic biliary system and the common bile duct was observed in all patients with ce - mrcps ( n = 27 )  . 
the duration between preoperative mri and surgery ranged 130days with the mean duration of 12days . the radiological findings were divided into two groups as t2w haste sequences ( n = 45 ) and ce - mrcps ( n = 27 ) findings . 
of 45 hydatid cysts , 23 cysts were 10cm and 22 were < 10cwhen we compared the findings of < 10cm cysts with 10cm cysts , we also found that larger cysts ( 10 cm ) increased the specificity , ppv , and accuracy of findings on t2w haste sequences . 
1 ce - mrcp at hepatobiliary phase shows contrast agent inside the gall bladder ( * ) , the common bile duct ( white arrow ) and intrahepatic bile duct ( black arrow ) ( a , b )  . 
the contour defect ( small black arrow ) of hydatid cyst with extension of a dilated biliary duct ( white arrow ) through defect was demonstrated on t2w - haste sequence ( c )  . 
 among interpretations of ce - mrcps , there was also perfect interobserver agreement ( k = 1 )  . discussion the complications of hydatid cysts can increase morbidity and mortality . 
2 ce - mrcp shows contrast inside the intrahepatic bile ducts ( white arrows ) : gall bladder ( black arrow ) ( a ) and the common bile duct ( white arrow ) ( b )  . 
there was no difference between roi measurements inside the surgically proven cyst with biliary communication at non - contrast ( c ) and at hepatobiliary phase ( d ) axial t1 - weighted images . 
 the contour defect of cyst with extension of a bile duct ( white arrow ) through defect ( small black arrow ) was illustrated on axial t2w haste sequence ( e , f ) the surgery is required and the type of the surgery [ 1114 ]  . 
the visualization of the biliary system and the bile leakage can be shown by excretion of contrast agent within the biliary systethus , the presence of contrast agent inside the hydatid cyst indicates cysto - biliary communication . in a previous study , kantarci etal . 
among hydatid cysts with biliary communication , there was one false - negative result in < 5cm cysts ( n = 6 ) , one in cysts between 5 and 10cm ( n = 15 ) , and two false - negative results in > 10cm cysts ( n = 14 ) on ce - mrcps [ 8 ]  . 
although 51% of patients had 10cm cysts ( n = 23 ) in our study , no leakage of contrast agent inside the cyst with biliary communication was observed . a few previous studies were published on the role of cemrcp for diagnosis of the postoperative biliary leakage [ 1821 ]  . 
 [ 18 ] detected five false - negative results in traumatic group ( n = 20 ) , six false - negative results in postoperative group ( n = 49 ) , and four false - negative results in hydatid cyst group ( n = 30 ) after combined analysis with mrcps and ce - mrcps [ 18 ]  . 
 [ 19 ] found the sensitivity of 96.4% , specificity of 100% , and accuracy of 97.1% for detection of an active bile leakage in ce - mrcps ( n = 34 ) at 2025min , 6090min , and 150180min delayed images . 
in contrast to some previous studies [ 18 , 20 ] , the sensitivity ratio in ce - mrcp at 2025min images ( 42.9% ) was lower , and there was one false - negative result [ 19 ]  . 
they concluded that although the visualization of the biliary system was sufficient at hepatobiliary phase and liver function tests are normal , the bile leakage may not be demonstrated on ce - mrcp and prolonged delayed phase images are required [ 21 ]  . 
moreover , in two patients with documented cysto - biliary communication after interventional procedures , no leakage of gadoxetic acid into the cyst was noted at prolonged delayed phase images [ 21 ]  . 
 on the contrary to previous studies [ 8 , 1821 ] , no contrast agent inside the cyst was detected in our study , although all cysto - biliary communications were clearly shown on t2w haste sequences . 
in our study , we investigated the relationship between hydatid cyst and the biliary system by comparing signs on routine axial and coronal t2w haste sequences , instead of mrcps , with findings of ce - mrcps . 
to decrease the bias of reader , two radiologists evaluated mris without knowledge of surgical findings . the reasons for non - visualization of gadoxetic acid in the cysts with biliary communications may be related to the size of biliary communication between the cyst and the biliary system , small volume leakage and high pressure inside the cyst [ 12 , 21 , 22 ]  . 
 we hypothesized that the increased pressure inside the cyst and the compression of bile ducts could be the reasons for no leakage of contrast agent inside the cyst . several studies were conducted to investigate the effect of the size of the hydatid cysts on biliary communication and the size of the cyst was found as an important predictor . 
all cysts 10cm had biliary communication in our study . we noticed a mismatch of findings in diagnosis of biliary communication in the cyst on routine abdominal t2whaste sequences and ce - mrcps . 
we recommend that if biliary communication of a cyst is seen on t2w haste sequences but no leakage of gadoxetic acid inside the cyst is shown on delayed phase of ce - mrcp , it should still be reported as cysto - biliary communication . 
the contour defect of a hydatid cyst with extension of a dilated bile duct through the defect is an important clue for cysto - biliary communication on t2w haste sequences . 
 so , on t2w haste sequences , the existence of marginal defect of cyst is an essential finding . the limitations of our study were as follows : retrospectively collected data were analyzed and the sample size was small . 
in a prospective study , subtracted images could be more valuable to demonstrate the leakage of contrast agent . in conclusion , ce - mrcp is an important noninvasive modality for depicting detailed anatomy and the visualization of the biliary system preoperatively . 
on the basis of our experience , we believe that when the contour defect of hydatid cyst with extension of a dilated bile duct through the defect is clearly shown on axial or coronal t2w haste sequences , it should be reported as a cyst with biliary communication . 
di diagnostica perimmagini ed ecografia interventistica , ospedale evangelico internazionale , genova , italy 7 dipartimento di diagnostica perimmagini , pineta grande hospital , castelvolturno ( ce ) , italy 8 unit di diagnostica perimmagini , casa di cure fornaca , torino , italy 9 universit degli studi di varese , bustoarsizio , italy 10 radiologia pediatrica e specialistica , azienda ospedaliera universitaria ospedali riuniti , universit politecnica delle marche , ancona , italy 3 department ofapplied clinical science andbiotechnology , 11 dipartimento di scienze biomediche perla salute , universit university oflaquila , laquila , italy degli studi di milano , milan , italy 4 unit operativa di radiologia diagnostica ed interventistica , irccs istituto ortopedico galeazzi , via riccardo galeazzi 4 , 20161milano , italy 12 u.o. 
they are sequences with long time of repetition ( tr ) and intermediate time of echo ( te ) halfway between pd - weighted sequences ( te = 1020ms ) and t2 - weighted sequences ( te = 80100ms )  . 
the advantage of these sequences is that te is short enough to maintain optimal anatomic detail ( as pd - weighted sequences ) and high sensitivity to fluid ( as t2 - weighted sequences )  . 
in this setting , strict adherence to standardized protocol is crucial to increase diagnostic performance and minimize variability among different diagnostic centres and readers [ 2 ]  . the aim of this paper is to provide standardized technical recommendations for musculoskeletal mri scans proposed by the italian college of musculoskeletal radiology . 
these recommendations are designed to give a uniform application of mri protocols over the national territory , to increase reproducibility and improve diagnostic performance . these technical recommendations can be applied to mri equipment of any manufacturer with different technical features . 
orientation of scan planes for shoulder examination : a axial plane ; b coronal oblique plane ; c sagittal oblique plane ; d aber 1 3 524 la radiologia medica ( 2019 ) 124 : 522538 in case of musculoskeletal tumours , the mri protocol often depends on tumour location . 
orientation of scan planes for elbow examination : a axial plane ; b coronal plane ; c sagittal plane macro - instability and micro - instability pathologies axial fat - saturated pd - weighted in extrarotation of the axial fat - saturated pd - weighted in intra - rotation of the humerus humerus elbow patients position patient does not tolerate the prone position , alternatively he can be positioned supine with elbow extended along the body in wide gantry scanners . elbow flexion at 6090 ( for the bicipital tendon , coracobrachialis tendon and tricipital tendon pathologies ) , consider the humerus as a reference for the planes positioning . flexed , abducted and supinated ( fabs ) elbow position for distal insertion of the biceps brachii tendon pathologies ( optional )  . scan planes extended elbow , patient in prone position with extended elbow and abducted limb ( superman position )  . 
orientation of scan planes for wrist examination : a axial plane ; b coronal plane ; c sagittal plane 1 3 la radiologia medica ( 2019 ) 124 : 522538 sagittal fat - saturated pd - / int - weighted mra examination saline solutionbased contrast agent indications sequences axial fat - saturated pd - / int - weighted coronal t2 - weighted or stir coronal fat - saturated pd - / int - weighted sagittal fat - saturated pd - / int - weighted wrist patients position pronated wrist in superman position . if the patient is not able to maintain the prone position for his clinical conditions , it is possible to consider the supine position with limb along the body in wide gantry scanners . scan planes axial parallel to the radiocarpal articular plane . 
orientation of scan planes for thumb examination : a axial plane ; b coronal plane ; c sagittal plane la radiologia medica ( 2019 ) 124 : 522538 fov maximum 120mm ; maximum thickness 3mm . fingers standard mri examination sequences axial fat - saturated pd - weighted axial t1 - weighted coronal fat - saturated pd - weighted sagittal fat - saturated pd - / int - weighted sagittal t2 - weighted this examination should be preferably performed on highfield scanners ( 1.5 or 3 t )  . patients position the superman position 1 3 la radiologia medica ( 2019 ) 124 : 522538 fig . 
alberto bellelli , roberto caudana , carlo faletti , eugenio genovese , carlo masciocchi and vincenzo spina are past chairs of the italian college of musculoskeletal radiology . compliance with ethical standards conflicts of interests the authors declare that they have no conflict of interest . ethical approval this article does not contain any studies with human participants or animals performed by any of the authors . 
itt can present as a thyroid nodule , and be confused with malignancy with its hyperechoic pattern ; this might cause unnecessary fine - needle aspiration biopsies and / or surgical interventions . 
we also aim to describe the most sensitive and most specific diagnostic parameters of itt . methods we have evaluated us examination reports of 56 children for whom differential diagnosis included itt between february 2015 and august 2018 . 
we have recorded sonographic characteristics of the lesions , cdus data , and thyroid hormone levels . results study population consists of 56 patients ( 22 itt , 34 other diagnoses )  . 
the most valuable criteria to predict itt presence were the fusiform shape and the longest diameter of the lesion . conclusions fusiform shape and a maximum diameter of 9mm are the most selective criteria to predict itt diagnosis . keywords intrathyroidal ectopic thymus tissue ultrasound diagnosis introduction the prevalence of thyroid nodules in pediatric population is 0.22% , which is lower than adults [ 1 ]  . 
when located in cervical region , it is generally seen between the * sonay aydin sonaydin89@hotmail.com 1 department ofradiology , sami ulus training andresearch hospital , 06340altnda , ankara , turkey 2 department ofradiology , erzincan university , erzincan , turkey 3 department ofradiology , ankara training andresearch hospital , ankara , turkey angle of the mandible and the manubrium [ 3 ]  . 
the most ectopic thymic pathways are located laterally according to thyroid gland [ 4 ] ; however , occasionally , ectopic thymus tissue can be found intrathyroidically , too . ultrasonography ( us ) is the modality of choice for evaluating thyroid gland pathologies in children as being noninvasive and not containing ionizing radiation . 
itt can present as a thyroid nodule , and be confused with malignancy with its hyperechoic pattern [ 5 ] ; this might cause unnecessary fine - needle aspiration biopsies and / or surgical interventions . sonographic detection of itt can be easier for the ones involved in pediatric radiology , but it is still a relatively unknown and difficult diagnosis . 
us examinations were performed by a 7 - mhz linear transducer ( toshiba , xario )  . we have recorded sonographic characteristics of the lesions , cdus data , and thyroid hormone levels . 
youdens index was used to define predictive values about lesion diameters . a two - tailed value of p < 0.05 was considered statistically significant . results study population consists of 56 patients ( 22 itt , 34 other diagnoses )  . 
it is also fusiform in shape ; however , its maximum diameter is measured 15mm , and typical punctate and thin linear internal echoes are not present table 1 pathological diagnosis other than itt diagnosis n ( % ) thyroiditis papillary cancer benign cytology atypia 13 ( 38.2% ) 2 ( 5.9% ) 15 ( 44.1% ) 4 ( 11.8% ) table 2 distribution of parameters according to pathological diagnovariables other diagnoses n = 34 itt n = 22 9.5 ( 516 ) 10 ( 417 ) 0.680 between itt and other diagnosis groups . 
also , a 1mm decrease in the longest diameter of the lesion increases the possibility of itt diagnosis 1.32 times ( or = 0.76 ; p = 0.006 ) ( table3 )  . discussion the development of thymus begins in the sixth week of gestation from ventral sacculation of the third pharyngeal pouch and minor portions of the fourth pharyngeal pouch . 
the bilateral primordial thymus fuses at midline in the eighth week to form the bilobed thymus , which will later descend into the superior mediastinuthe routes of descent of the thymus and of the thyroid are alike because of the proximity of the thyroid diverticulum to the third branchial pouch . 
in the current study , we mainly aim to define the most sensitive and most specific diagnostic parameters to predict itt diagnosis in order to prevent unnecessary invasive procedures and follow - up examinations . typical us appearance of itt is defined as a hypoechoic ( more hypoechoic than the surrounding strap muscles ) lesion with punctate and thin linear internal echoes [ 9 ]  . 
it is stated in the literature that the echogenicities in itt can correspond to hassalls corpuscles rather than microcalcifications [ 10 ]  . in the literature , itt can generally be presented as a fusiform lesion [ 3 , 5 , 9 ]  . 
our results are consistent with the literature ; fusiform shape is the most common itt shape , as well as the rate of being fusiform shape is higher in itt group than the other diagnoses . 
the information contributes to the literature , as far as we know this is the first study to evaluate the diagnostic power of the sonographic parameters . itt was defined to be hypovascular or isovascular compared to the adjacent thyroid parenchyma [ 5 , 11 ]  . 
in other studies [ 5 , 12 ] , it is emphasized that itt lesions are generally subcentimeter , but they did not define any cutoff values , or do not use the diameter of the lesion as a diagnostic criterion like fusiform shape , and typical us appearance . 
different from the literature , we showed that the diameter of the lesion is one of the most powerful criteria to predict itt diagnosis . most of the itt cases were euthyroid in our study . 
we believe that abnormal thyroid hormone levels seen in itt cases are caused by concurrent , independent pathologies , such as thyroiditis . 1 3 la radiologia medica ( 2019 ) 124 : 505509 36 ( 4 ) : 299308 . 
hernandez - cassis c , poniecka a , vogel ck , mckenzie jm ( 2008 ) a six - year - old boy with a suspicious thyroid nodule : intrathyroidal thymic tissue . 
vlachopapadopoulou ea , vakaki m , karachaliou fe , kaloumenou i , kalogerakou k , gali c , michalacos s ( 2016 ) ectopic intrathyroidal thymus in childhood : a sonographic finding leading to misdiagnosis . 
avula s , daneman a , navarro om , moineddin r , urbach s , daneman d ( 2010 ) incidental thyroid abnormalities identified on neck us for non - thyroid disorders . 
yildiz ae , ceyhan k , siklar z , bilir p , yagmurlu ea , berberoglu m , fitoz s ( 2015 ) intrathyroidal ectopic thymus in children : retrospective analysis of grayscale and doppler sonographic features . 
first , unfortunately , some of the patients did not have follow - up us examinations ; hence , the study can offer limited information about followup change of itts . 
lastly , we did not examine the prevalence of itt according to age subgroups , because we did not have enough itt cases for such an evaluation . in the literature , the articles about itt are generally case reports or case series . 
there are not so many original articles , and the present articles are not inclusive of our study ; such as some of them concentrate on only gray - scale us findings , while some of them contain localization data mainly . 
also , our study contributes to the growing literature by defining the diagnostic power of examined parameters . to conclude , itt must be kept in mind in the differential diagnosis of thyroid lesions in pediatric population in order to prevent unnecessary interventional procedures and follow - up examinations . 
simple clinic data and imaging findings were considered : ( a ) location ( craniocaudal and axial ) , ( b ) size , ( c ) morphology , ( d ) dural contact , ( e ) signal characteristics , ( f ) enhancement degree and patterns . 
the surgical treatment of schwannomas requires incision of both the dura mater and arachnoid membrane , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 510521 because the tumors reside in the subarachnoid space . 
the attachment site of the meningioma to the dura mater must be resected with the tumor to remove any residual tumor cells ; thus , preservation of the arachnoid membrane helps prevent postoperative csf leakage . 
to solve this issue , we conducted this retrospective study to develop the usefulness of mr imaging for the differential diagnosis of these two entities . materials andmethods population data this retrospective study was approved by our institutional review board , and the requirement for informed consent was waived . 
the following inclusion criteria were : ( a ) pathology - proven meningiomas or schwannomas , ( b ) patients with multiparametric mr imaging including t1wi , t2wi , and enhanced t1wi sequences , and ( c ) patients with surgical resection . of these , 27 patients were excluded for the following reasons : ( a ) patient with operation before ( n = 4 ) , ( b ) neurofibromatosis ( n = 5 ) , ( c ) unsatisfactory imaging quality for review ( n = 6 ) , ( d ) main part of lesion - located paravertebral region ( n = 4 ) , or ( e ) without enhancement mr images ( n = 8 )  . 
therefore , a final cohort of 157 patients was included . we reviewed each case with respect to age , gender , the nature of preoperative symptoms , duration of the symptoms , location of the tumor and mri findings . imaging data all mr examinations in all 157 patients were performed on 1.5 - tesla mr scanner ( 65 cases , magnetom aera ; siemens healthcare , erlangen , germany ) or 3.0 - tesla mr scanner ( 92 cases , siemens magnetom trio tim , erlangen , germany ) , and surface coils were used for all patients . including t1wi spin - echo ( se ) sagittal ( for 1.5t , tr / te = 550 / 11ms , nex = 4 , for 3.0t tr / te = 500 / 9.5ms , nex = 4 ) , and fast spin - echo ( fse ) t2 - weighted sequences ( tr / te = 3000 / 500ms for 1.5t ; tr / te = 2500 / 100ms for 3.0t ) sequences t2wi axial ( for 1.5t , tr / te = 500 / 12ms , nex = 4 ; for 3.0t , tr / te = 470 / 11ms , nex = 4 ) , and followed by enhanced fat - suppressed t1wi in the axial plane , the sagittal and the coronal plane . 
both of them were blinded to age , gender , clinical history , symptoms and histopathologic results at the time of interpretation . following items were evaluated onmr images its location ( a ) craniocaudal : cervical region , cervicothoracic region , thoracic region , thoracolumbar region , lumbar region , lumbosacral region or sacral region ; and ( b ) axial location : anterolateral , posterolateral or lateral , and ventral ( midline anterior ) or dorsal ( midline posterior )  . size as the average of long and short axes more accurately reflects three - dimensional tumor volume [ 7 ]  . 
the greatest diameter of each tumor was obtained on the contrast - enhanced images . morphologic characteristics ( 1 ) oval or round shape ( mainly depending on sagittal / coronal images ) , ( 2 ) dumbbell type , ( 3 ) intervertebral foramen widening , ( 4 ) the ginkgo leaf sign . the ginkgo leaf sign : the shape of the deformed cord and the streak resembled a ginkgo leaf on contrast - enhanced axial mr images [ 8 ]  . dural contact the dural tail sign was considered according to the following criteria [ 9 ] : ( 1 ) the tail should be identified at least on two successive sections through the tumor , ( 2 ) the tail should taper smoothly away from the tumor , and ( 3 ) the tail has an 1 3 512 la radiologia medica ( 2019 ) 124 : 510521 enhancement greater than that of the tumor itself , with bone signal abnormalities occasionally . signal characteristics on t1wi ( precontrast ) and t2wi the signal intensity of the lesions was compared with that of the spinal cord . 
 ( 1 ) hypointense was lower than spinal cord , not equal to csf , ( 2 ) isointense was equal to spinal cord , ( 3 ) hyperintense was higher than spinal cord and ( 4 ) miscellaneous signal was formed by of different signs but not classified as any of the aforementioned , and ( 5 ) cystic degeneration ( for t2wi ) as indicated by signal intensity equal to that of the cerebrospinal fluid , exhibiting low intensity on t1wi and high intensity on t2wi . enhancement degree andpatterns on t1wi 1 . 
and a multivariate logistic regression analysis was performed to assess which factors affected the diagnosis results between schwannomas and meningiomas based on the performance of mr image findings and simple clinic data . 
diagnostic parameterssensitivity ( se ) , specificity ( sp ) , positive predictive value ( ppv ) and negative predictive value ( npv ) were calculated on a lesion and a patient basis for mr imaging . interobserver agreement analysis with k statistic was performed to determine consistency between the two radiologists for detection of tumor for the different mr imaging findings . 
the k values were interpreted as follows : 0.000.20 , slight agreement ; 0.210.40 , fair agreement ; 0.410.60 , moderate agreement ; 0.610.80 , substantial agreement ; and 0.811.00 , almost perfect agreement ( 28 )  . 
most of the patients had progressive transverse spinal cord lesions , such as progressive paraparesis , nerve palsy , shoulder and back pain , sciatica , impotence , and bowel dysfunctions . 
among the meningioma group , there was a predominance in the female group ( 40 cases , 75.5% ) , and there were 43 ( 81.1% ) patients with the age of 6187years . 
concerning schwannomas , 9 cases ( 8.6% ) were ventral or anterolateral ( one case , 0.96% ; 8 cases , 7.6% , right - anterolateral / left - anterolateral , 3 : 1 ) , 42 cases ( 40.4% , right - posterolateral / left - posterolateral , 4 : 3 ) were posterolateral , while there was no case identified in the dorsal region , and 43 ( 41.4% ) schwannomas were lateral ( right / left , 22 : 21 )  . 
for the schwannomas , there were 13 ( 12.5% ) cases in the vertebral junction regions ( cervical - thoracic , thoracic - lumbar and lumbosacral : 3 , 6 and 4 cases , respectively ) , and multiple schwannomas ( 10 cases , 9.6% ) occurred in anywhere of intraspinal canal ( cervical , thoracic , thoracic - lumbar and lumbosacral : 5 , 3 , 1 and 1 cases , respectively ) , of which features were not manifested in the meningiomas group . statistical analysis demonstrated difference between the two groups : meningiomas seldom occurred in the vertebral junction regions . 
oval or round shape was observed in 63 cases of schwannomas , and a dumbbell shape with intervertebral foramen widening was manifested in 31 cases ( multiple lesions not involved )  . 
thirty - two ( 60.4% ) meningiomas demonstrated the dural tail sign , and only 6 ( 6.8% ) schwannomas did the dural tail sign on contrast - enhanced t1wi . 
 the dural tail sign was highly significant difference between the two groups ( 2 = 51.55 , p < 0.001 ) 1 3 la radiologia medica ( 2019 ) 124 : 510521 fig . 
there was no the dural tail sign in multiple schwannomas in our work . signal intensity on t1wi ( precontrast ) and t2wi on precontrast t1wis , 3 ( 5.7% ) meningiomas were hypointense , and 50 ( 94.3% ) cases were isointense ( hetero - / homogenous , 15 / 35 )  . 
in contrast to meningiomas , 23 ( 22.1% ) schwannomas demonstrated isointense signal on t2wis ( hetero - / homogenous , 1 3 516 la radiologia medica ( 2019 ) 124 : 510521 12 / 11 ) , 31 ( 29.8% ) schwannomas demonstrated hyperintense signal ( hetero - / homogenous , 18 / 13 ) , and 31 schwannomas ( 29.8% ) demonstrated fluid signal intensity ( cyst degeneration )  . 
thirty - four ( 32.7% ) schwannomas demonstrated rim enhancement , and 5 ( 4.8% ) schwannomas did focal enhancement , of which moderate and marked enhancement were as follows : diffuse : 0 / 65 , rim : 1 / 33 , focal : 1 / 4 , respectively . 
 ( table2 ) multivariate logistic regression forty - six ( 86.8% ) meningiomas demonstrated diffuse enhancement and 7 ( 13.2% ) meningiomas demonstrated rim enhancement , of which moderate and marked enhancement were manifested on contrast - enhanced mr images ( moderate / marked 2 / 44 , 1 / 6 , respectively )  . 
meningiomas were almost hypointense ( 50 , 94.3% ) , while schwannomas ( multiple lesions involved , the maximum lesion was analyzed ) , 56 ( 53.8% ) cases were hypointense , 40 ( 38.5% ) cases homogenous isointense , 2 cases hyperintense and 6 cases miscellaneous signal . 
schwannomas usually demonstrated rim enhancement , while meningiomas did diffuse enhancement ( 2 = 10.58 , p = 0.005 ) 1 3 la radiologia medica ( 2019 ) 124 : 510521 fig . 
a miscellaneous signal oval lesion with marked heterogeneity ( rim with focal enhancement ) was manifested in the left - posterolateral area ( white arrow ) , and it extended over several vertebra along the spinal canal ( white arrow ) , there was a fluidfluid level inside it ( b and e , black arrowhead )  . 
the four most common intradural spinal tumors are the following : schwannoma ( 30% ) , which is the most common intradural extramedullary spinal tumor , occurring at a rate of approximately 0.30.4 per 100 , 000 persons per year . 
intradural intramedullary of which concerning 90% is glial tumors ; ependymoma ( 60% ) is the most common spinal cord tumor in adults , and astrocytoma ( 30% ) is the second most common spinal cord tumor in adults [ 1 , 10 ]  . mri is considered the best preoperative imaging technique to diagnose spinal tumors . 
studying the statistical weight of these modalities on basis of multivariate logistic regression , six statistically significant findings ( age , size , dural tail sign , morphology , sign of t2wi and axial location ) were screened to facilitate the differential diagnosis . 
the capability of logistic equation analysis is 87.1% , indicating that these imaging findings may be useful for differential diagnosis of the two lesions . based on a certain finding only , such as sex , craniocaudal distribution , gave excellent results when evaluated with our series , but they were not included in the multivariate logistic equation . 
an oval lesion manifested hypointense on t1wi ( white arrow ) , marked rim enhancement in the right lateral area ( white arrowhead ) , and the adjacent spinal cord was compressed to the dorsal area . 
an isointense round lesion ( white arrow ) with marked homogeneity enhancement was demonstrated in the right lateral area ( white arrowhead ) , the adjacent spinal cord was compressed to the lea 41 - year - old man with two intraspinal schwannomas in the lumbar . 
the big lesion manifested fluid signal intensity on t2wi ( white arrow ) with marked rim enhancement and septal enhancement ( black arrowhead ) and the round small lesion manifested isointense signal with marked homogenous enhancement ( white arrowhead )  . 
an oval lesion manifested hypointense on t1wi ( white arrow ) , marked rim enhancement with focal mural nodule enhancement in the right - anterolateral area ( white arrowhead ) it gets the most appropriate regression model ; moreover , the multicollinearity does not exist anymore . more than 95% of meningiomas were benign tumors and occurred most frequently in older women [ 4 ]  . 
the female preponderance in the adult population was even stronger than that associated with intracranial meningiomas , and it was thought to be due to the effect of estrogen [ 11 , 12 ]  . 
most spinal meningiomas ( 80% ) arise in the thoracic region , with less common 1 3 la radiologia medica ( 2019 ) 124 : 510521 involvement of the cervical ( 15% ) or lumbar ( 5% ) regions [ 10 ]  . 
intramedullary schwannomas are overwhelmingly rare [ 13 ]  . the typical spinal meningioma is a small , single , discrete , round or oval intradural tumor , but occasionally it may present multiple lesion ( 2% )  . 
in general , schwannomas are solitary , well - circumscribed and encapsulated tumors , commonly arising from the dorsal sensory roots of the cervical and lumbar spine with less frequent involvement of the thoracic region and rarely occur in the lumbosacral region [ 12 , 14 ]  . 
consequently , we suggest that coronal images ( for lateral tumors ) and sagittal images ( for ventral or dorsal tumors ) can be used to study the relation between the tumor and the dura , and to search for the dural tail sign . 
but our results do not conform to these findings , 50 ( 94.3% ) meningiomas manifested isointensity , while 56 ( 53.8% ) schwannomas cases did hypointensity , 6 cases hyperintense and 2 cases miscellaneous signal on t1wi . 
 we speculate that focal areas of even greater hyperintensity on t2wi often corresponds to cystic portions , whereas hypointensity may represent hemorrhage , dense cellularity or collagen deposition [ 12 , 25 ]  . 
schwannomas tendency to cyst formation and hemorrhage were greater in the spine than the intracranial examples and other extramedullary spinal tumors , such as meningiomas [ 26 ]  . 1 3 520 la radiologia medica ( 2019 ) 124 : 510521 in our series , all schwannomas and meningiomas were easily detected on contrast - enhanced mri , and none of schwannomas or meningiomas were not enhanced . 
 the first and foremost , the study was retrospective , and the reviewers were all specialized in differentiating schwannomas from meningiomas , not include any cases of other intradural extramedullary tumors such as cysts , capillary hemangiomas , or ependymoma , which might possess the influenced sensitivity of mr imaging for differentiating the two lesion types . 
finally , because the cases were retrospectively collected over 8years from two different types of mr machines , protocols were inevitably not standardized . conclusions to sum up , simple clinical data associated with mri findings can be used to an accurate diagnosis in the vast majority spinal meningiomas and schwannomas , if various imaging features are analyzed carefully and discreetly . a thoracic vertebra canal tumor with diffuse homogenous enhancement and the dural tail sign in females proved statistically significant as predictors of meningioma , while a tumor with widening of neural foramen , fluid signal intensity on t2wi , rim enhancement proved statistically significant as predictors of schwannoma , especially occurred in vertebral junction regions or lumbar locations . 
in the future , diffusion - weighted imaging and susceptibility weighted imaging may increase the accuracy of imaging findings in the differentiation of spinal schwannomas and meningiomas . compliance with ethical standards conflict of interest no conflict of interest exists in the submission of this manuscript , and manuscript is approved by all authors for publication . 
i would like to declare on behalf of my co - authors that the work described was original research that has not been published previously , and not under consideration for publication elsewhere , in whole or in part . 
all the authors listed have approved the manuscript that is enclosed . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent this retrospective study was approved by our institutional review board , and the requirement for informed consent was waived . la radiologia medica ( 2019 ) 124 : 662670 radiotherapy concomitant radiotherapy andtki inmetastatic egfr oralkmutated nonsmall cell lung cancer : amulticentric analysis onbehalf ofairo lung cancer study group paoloborghetti1 marcolorenzobon1 rachelegiubbolini2 niccologiajlevra3 rosariomazzola3 marcoperna4 lucavisani4 fiammettameacci4 mariataraborrelli5 lucatriggiani1 davidefranceschini6 carlogreco7 alessiobruni2 stefanomariamagrini1 vieriscotti4 received : 25 july 2018 / accepted : 29 january 2019 / published online : 15 february 2019 italian society of medical radiology 2019 abstract purpose to investigate the role of radiotherapy ( rt ) in the management of egfror alk - mutated metastatic non - small cell lung cancer ( nsclc ) treated with tki . materials and methods clinical data of 106 patients ( pts ) from five institutions treated with rt concomitant to tki were retrospectively revised . 
patients with four or less metastasis were defined as oligometastatic / oligoprogressive ( om / op ) ; sites of rt were brain , bone , lung or others in 46% , 27% , 14% and 13% , respectively . 
multivariate analysis confirmed srt ( hr 0.355 , ci 95% 0.2120.595 ; p < 0.001 ) and median duration of tki > 14months ( hr 0.17 , 95% ci 0.100.30 ; p < 0.001 ) as independent factors related to better os . 
therefore , platinum - based chemotherapy has been replaced by anti - egfr ( gefitinib , erlotinib , afatinib , osimertinib ) or anti - alk ( crizotinib , ceritinib , alectinib ) tkis in the first - line treatment of this subset of patients [ 13 ]  . median progression - free survival ( pfs ) and overall survival ( os ) of patients treated with tkis range between 813 * marco lorenzo bon marcolorenzo89.mlb@gmail.com extended author information available on the last page of the article and 1825months , respectively . 
however , it is becoming clearer that patients with stage iv egfror alk - mutated nsclc represent a heterogeneous group in terms of disease characteristics and , therefore , survival outcomes . 
clinical presentation can occur with low or high burden of metastatic disease , and it can be affected by the number , dimension and / or location of the metastatic lesions [ 46 ]  . oligometastatic status represents a condition with a low disease burden at presentation ( commonly 46 metastatic lesions )  . 
according to these inclusion criteria , patients were divided in three groups : those who underwent rt no more than 30days before the beginning of the drug ( group a ) , those who underwent rt no more than 30days after the definitive suspension of the tki ( group b ) and those who underwent rt during the administration of the drug ( group c )  . in terms of disease burden at rt presentation , the patients were classified in oligometastatic or oligoprogressive ( om / op ) state , defined as four or less metastatic lesions , and polymetastatic or polyprogressive ( pm / pp ) state , defined as more than four lesions , according to the institutional policy and supported by the literature [ 12 ]  . all the dose fractionation schedules were considered ; the term hypofractionated rt ( hrt ) includes treatments with a palliative aim , as 30gy in 10 fractions , 20gy in 5 fractions or 8gy in 1 fraction . 
the term stereotactic rt ( srt ) means an ablative treatment able to deliver bed over 60gy in a few fractions ( mean 80gy , range 60178gy , considering an alpha / beta for the tumor equal to 10 )  . mutation analysis was conducted by extracting dna and identifying egfr exon 19 deletion and exon 21 l858r mutations by standard sequencing and fragment analysis , while to detect alk gene translocations fluorescence insitu testing ( fish ) has been used . 
in order to analyze the efficacy of the combined treatment , overall survival ( os ) , defined as time from the beginning of drug treatment to death ( any cause ) or until the last follow - up , was estimated with kaplanmeier curves . 
the same variables reported above and potentially affecting os were investigated at univariate analysis with the logrank test ; multivariate analysis was performed with the cox regression model , including all variables resulted statistically significant at univariate analysis . 
acute toxicities , according to rt schedule , were defined as adverse events occurring at the site of irradiation within 90days , whereas late toxicities are those becoming evident after 90days . 
the majority of the patients ( 65 , 61% ) were nave to previous chemotherapy ; 33 ( 31% ) were treated with a first chemotherapy line , while eight patients ( 8% ) received two or more chemotherapy lines before tki . 
fifty - nine patients were treated with gefitinib , 19 with erlotinib , 18 with crizotinib and 10 with other tkis ; four patients were on a secondline tki ( osimertinib and ceritinib )  . 
only two cases of g2 toxicity have been recorded in the srt group , while 5 , 7 and 2 cases with grade 1 , 2 and 3 toxicities , respectively , were registered in the hypofractionated group . 
srt stereotactic radiotherapy , hrt hypofractionated radiotherapy , om / op oligometastatic / oligoprogressive disease , pm / pp polymetastatic / polyprogressive disease discussion preclinical studies demonstrate the possible synergistic effect of tkis given concurrently with radiation at several levels , including effects on cell cycle kinetics , apoptosis induction and the targeting of accelerated cellular repopulation . 
a potential relationship between egfr signaling and dna damage repair has been recently supported by data regarding the inhibition of rad51 expression , a protein involved in the cell double - strand break repair systewhen combined with radiation , erlotinib enhances the induction of apoptosis , inhibits egfr autophosphorylation and rad51 expression following radiation exposure , promoting an increase in radiosensitivity [ 16 , 17 ]  . available data suggest that the om / op condition in nsclc is characterized by better outcomes , also in the absence of ablative treatments [ 7 ]  . 
furthermore , some authors suggest that oligometastatic patients more frequently progress with a further oligoprogressive pattern in comparison with polymetastatic patients [ 18 ]  . recent retrospective and randomized prospective studies show that rt given at progression or on residual disease after partial response on oligometastatic foci fairly improves pfs and may allow longer disease - free intervals [ 9 ]  . 
it is still unclear if ablative treatment of om / op disease may change the natural history of the disease and contribute to a real survival benefit [ 1215 ]  . accordingly , recent retrospective and some prospective studies tried to identify which patients subgroup can achieve a clinical advantage from local treatments . 
nevertheless , some authors remark that the site of metastasis , a longer disease - free interval and the presence of driver mutations characterize patients who can benefit more from locally ablative treatment . 
probably , these parameters indirectly reflect a more favorable tumor biology , in which srt can sterilize metastatic foci , ablate lesion in sanctuary locations , overcome drug resistance and promote drug holidays [ 19 , 20 ]  . our study corroborates these hypotheses , finding that srt schedule is a factor independently associated with better os at multivariate analysis . 
the authors find out that the ablation of all the metastatic foci in op patients treated with crizotinib allowed an extended duration of drug exposure and was associated with longer overall survival [ 21 ]  . these retrospective findings have been recently confirmed by the preliminary results of a prospective randomized trial [ 22 ]  . in our series , the majority of patients treated with concomitant tkis did not interrupt the drug administration . 
our data are consistent with the available evidence identifying patients with a good performance status , om / op disease and the presence of a driver mutation as the best candidates for srt . 
srt can be safely administered also concurrently with tkis . increasing evidences suggest that the ablative treatment of all sites of disease in patients with a limited number of metastases improves clinical outcomes . 
a multi - disciplinary discussion each time this condition occurs is strongly encouraged . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards the study was performed in accordance with the declaration of helsinki . 
the questionnaire was developed by the board of the italian college of chest radiology of the italian society of medical and interventional radiology ( sirm ) and by an experienced group of italian academic chest radiologists . 
the link to the online electronic survey was submitted by email to all the sirm members . results a total of 767 radiologists , corresponding to 7.5% of all the sirm members , participated in the online survey . 
the majority of participants ( 92% ) routinely describe the attenuation of pulmonary nodules in the report , and 84.1% recommend the further follow - up , with 92.7% of respondents taking ct nodule morphological features into consideration . 
the majority of sirm members express a need for an update on this topic . keywords pulmonary nodule computed tomography management italian survey chest radiology introduction the continuous technical development and widespread use of computed tomography ( ct ) have led to an increasing number of pulmonary nodules detected , which represents a considerable diagnostic and management challenge [ 1 ]  . the proper management of lung nodules needs an appropriate evaluation , in terms of adequate ct technique chosen , correct identification and interpretation of imaging findings , and optimal follow - up recommendation according to the nodules characteristics . to date , several guidelines from the major medical societies are available for the management of pulmonary nodule * cristiano rampinelli cristiano.rampinelli@ieo.it extended author information available on the last page of the article incidentally identified on ct [ 24 ] , with distinct algorithms for solid and subsolid nodules ( namely , part - solid and ground - glass nodules )  . 
however , in the current clinical practice it is unclear whether radiologists agree with such guidelines , since a variety of strategies can be adopted for nodule detection and management . 
the final version of the survey , which consisted in 23 multiple - choice questions , was created as an online electronic survey using the surveymonkey webbased tool [ 5 ]  . 
the first four questions of the survey were aimed to collect generic information on survey participants , namely the years of experience in radiology , the italian area of belonging , the site of work ( university / research hospital , public hospital , private hospital ) and the daily time committed to thoracic imaging . the following five questions were related to technical aspects and reading tools that are routinely used in chest ct analysis , while ten questions were aimed to collect information on nodule characteristics , management and diagnostic algorithms . the final section included four questions on the role of trans - thoracic ct - guided biopsy , on the multidisciplinary approach to lung nodule and the need of congresses and refresher courses focused on pulmonary nodule . multiple answers were allowed only for two questions . 
the mean time to complete the questionnaire was 620 . the experience in radiology of respondents was quite homogeneously distributed with a faintly higher prevalence of experienced radiologists ( 20.1% with less than 5 - year experience , 16.7% with 5to 9 - year experience , 28.3% with 10to 19 - year experience and 34.9% with more than 20 - year experience ) ( q1 )  . 
slightly more than half of participants ( 53.7% ) were employed in a public hospital while one - fourth ( 25.6% ) in a university / research hospital ( q3 )  . 
significant differences in the distribution of the answers among the two groups ( p < 0.05 ) have been observed for some questions , and results are summarized in table2 . 
particularly , radiologists working at university / research hospitals use two - reconstruction ct protocol for evaluating pulmonary nodules and dedicated software for volumetric analysis when nodule diameter assessment is inconclusive , more frequently than the other respondents ( q5 , q9 )  . 
lung nodule density is always reported by the majority of radiologists in both groups , even though with a higher rate among university / research radiologists ( q10 ) , who also prefer to measure part - solid nodule by reporting the maximum diameter of both the solid component and the entire nodule ( q11 )  . 
with regard to nodule management , university / research radiologists rely more on the fleischner society guidelines and consider pet - ct not indicated for the characterization of a solid nodule < 8mm compared to the rest of respondents ( q15 , q18 )  . 
ct - guided lung biopsies are performed in the majority of university / research hospitals , with a higher rate than the other institutions , mostly carried out by radiologists ( q21 )  . 
finally , university / research radiologists attend a weekly lung nodule multidisciplinary meeting in the 45.9% of cases as compared to the 21.6% of the rest of participants ( q22 )  . discussion the present study evaluated the approach of the sirm members to the complex topic of pulmonary nodule in ct . 
the questionnaire was aimed to identify potential critical issues in regard to ct technique , image reading and interpretation as well as management of incidental pulmonary nodules . as expected , we observed a strong consensus among respondents on some questions . 
particularly , the vast majority of participants ( 92% ) routinely described the attenuation appearance ( solid , part - solid , ground - glass ) of pulmonary nodules identified on ct scan in the radiological report , and 84% recommended the further work - up . 
1 the graph shows results of the sub - analysis conducted for q15 on the basis of the years of experience in radiology ( < 5years ; 59years ; 1019years ; 20years ) ( q1 )  . 
2 the graph shows results of the sub - analysis conducted for q20 on the basis of the years of experience in radiology ( < 5years ; 59years ; 1019years ; 20years ) ( q1 )  . 
 radiologists with experience 20years tend to suggest a biopsy for the characterization of a ground - glass nodule with a diameter > 10mm more often than the other groups 1 3 la radiologia medica ( 2019 ) 124 : 602612 606 fig . 
3 the graph shows results of the sub - analysis conducted for q18 on the basis of the years of experience in radiology ( < 5years ; 59years ; 1019years ; 20years ) ( q1 )  . 
 a significantly higher number of radiologists with experience < 5years does not indicate a pet - ct for characterizing a solid pulmonary nodule with a diameter < 8mm than the other groups features of pulmonary nodules to indicate the subsequent management , demonstrating that morphology is still considered a significant determinant by radiologists , regardless of the nodule size and density . 
these results denoted the awareness of the different strategies for managing pulmonary nodules , indicating an active role of radiologists in suggesting the optimal work - up strategy . on the other hand , we noted a variety of practices regarding the ct technique and reading tools routinely used in the chest examinations . 
for example , while 91.5% of the respondents use thin section thickness for lung nodules evaluation , as suggested by the fleischner society [ 6 ] , only half of themslightly more if we consider the setting of university / research radiologistsregularly perform two reconstructions , respectively , with sharp and standard kernel ( q5 )  . 
 the former reconstruction is suitable for the evaluation of nodule borders , attenuation and measurements , while the latter is suggested for the assessment of the nodules internal content ( calcifications , fat tissue )  . we also found a variability on the use of contrast medium for pulmonary nodule characterization . 
 actually , the dynamic assessment of lung nodule enhancement has not been widely used in the clinical practice over the years , probably because of the relatively high radiation dose and its variability in diagnostic performance in characterizing nodules according to the technique used , mainly in terms of specificity ( 5893% ) [ 7 ]  . concerning radiation exposure , only 44.1% of participants always use low - radiation dose ct protocol for the follow - up of pulmonary nodules ( q7 )  . 
several dose reduction strategies are available in the current generation of ct scanners , including lowering ma and kvp , and using high - pitch technique , automatic tube current modulation and iterative reconstructions [ 811 ]  . 
particularly for follow - up ct scans , further efforts are therefore required to expand the adoption of optimized ct protocols to minimize patient radiation exposure . among italian radiologists , mpr and mip were the tools of choice for pulmonary nodule evaluation ( q8 , q9 )  . 
this could be explained by the convenience and user - friendliness of these widely integrated reporting tools , compared to the limited availability of cad systems and software for volumetric analysis , which are rarely incorporated into the pacs system and often time - consuming . 
volumetric analysis software is more frequently used , even if not extensively , by radiologists working at university / research hospitals , due to a greater availability / integration of these systems in these institutions , as demonstrated by the results of the specific sub - analysis ( q9 )  . from the questions focused on pulmonary nodule management , we observed again a variety of approaches , which reflect the challenge of this topic . 
in particular , we found that the 57.7% of participants preferred the fleischner society guidelines for the management of pulmonary nodules detected incidentally , specifically in the subgroups of radiologists less experienced and employed in university / research hospitals ( q15 )  . 
however , in our survey the adherence to the fleischner society guidelines is not comprehensive , as can be observed from the response concerning the follow - up of solid nodules < 6mm in adult patients without 1 3 la radiologia medica ( 2019 ) 124 : 602612 1 3 608 la radiologia medica ( 2019 ) 124 : 602612 risk factors . 
although no follow - up is suggested for such nodules in the fleischner guidelines [ 2 ] , only 32.3% of participants follow this indication , while about 57% ask for 3 to 6months follow - up and 11% send the subject to the referring physician or specialist ( q15 )  . 
similarly , in the case of a ground - glass nodule stable at annual follow - up , only 11.2% of the participants followed the fleischner societys recommendation of a further 2 - year follow - up , while favoring instead a shorter follow - up ( 75% ) ( q16 )  . 
therefore , even if the fleischner society guidelines are the primary choice , the respondents tend to adopt a more cautious approach with a shorter follow - up for both solid and ground - glass nodules . 
 in fact , the pulmonary nodule guidelines , that also take into account several aspects , including the patients will , provide recommendations and not mandatory rules . with regard to interventional lung procedures ( q21 ) , even though in a substantial rate of institutions ct - guided biopsies are not performed at all ( 35.8% ) , our analysis demonstrated that where biopsies are carried out , radiologists are mostly involved . since the management of pulmonary nodules is challenging , the multidisciplinary team plays an important role [ 13 ]  . 
 unfortunately , more than half of respondents reported that there are no multidisciplinary meetings in their workplace ( q22 ) , especially among those who do not work in university / research hospitals . 
this observation underlines the need for congresses or refresher courses to continue education in the field of nodule work - up ( q23 )  . pet - ct plays an important role in the characterization of pulmonary nodule due to its capacity of assessing nodule metabolism by evaluating the 18f - fluorodeoxyglucose ( 18f - fdg ) uptake . 
these data underline that radiologists need a more in - depth knowledge of the advantages and limitations of the application of nuclear medicine in this field . the present study has some limitations . 
with almost 800 respondents , this is one of the largest surveys among italian radiologists ever reported , but it corresponds to a rather low survey response rate of 7.5%. 
when compared to other surveys , our response rate is , however , in the range of two recent surveys among sirm members , conducted on teleradiology and musculoskeletal interventional procedures , which achieved a response rate of 17% and 5.4% , respectively [ 15 , 16 ]  . 
the reason of the low response rate was possibly related to the specialist topic of the survey ( pulmonary nodule ) proposed to a general radiology audience ( all sirm members )  . 
moreover , physicians are a professional group with low survey response rates in general [ 17 , 18 ]  . another limitation was that the questionnaire was sent to the sirm members 4days prior to the online publication of the recommendations on pulmonary nodule measurement from the fleischner society ( 26 june 2017 ) [ 6 ]  . 
moreover , also in presence of specific guidelines the adherence of radiologists may be not complete . in conclusion , the results of this national survey allowed us to obtain a comprehensive view of the attitudes of the italian radiologists toward the complex and debated topic of pulmonary nodule management . 
this retrospective study investigated safety and efficacy of embolization agents with small - particle embolization treating patients with massive hemoptysis due to ipvs . methods patients with massive hemoptysis ( n = 207 ) underwent computed tomography angiography of bronchial artery . 
only four patients experienced mild hemoptysis during the 24 - month follow - up with the efficiency of 75.0%. conclusions intercostal artery embolization with 300500m alone or combined with microcoils is a safe and effective procedure in patients with ipvs - induced bronchial hemoptysis . keywords catheter intercostal pulmonary venous shunt massive hemoptysis interventional therapy introduction massive hemoptysis , defined as the coughing up of blood or bloodstained mucus , is a common life - threatening sign of respiratory disease [ 1 ]  . 
systemic arterial ( bronchial or nonbronchial ) pulmonary circulation shunt , known as systemic - to - pulmonary venous shunt , is anatomically abnormal that induces recurrent and life - threatening * xiaolin zhang sxdxfzg@sina.com 1 first college ofclinical medical science , china three gorges university , yichang443003 , china 2 department ofradiology , yichang central peoples hospital , 183 yiling road , yichang443003 , china hemoptysis [ 25 ]  . 
 ipvs is characterized by earlier development of thickened interatrial ( ia ) shunts , hyperplastic blood vessels , and pulmonary veins observed in digital subtraction angiography ( dsa )  . 
however , ipvs has not been reported as an independent disease . current therapeutic methods for bronchial massive hemoptysis include hemostatics , surgery , and bronchial artery embolization [ 16 ]  . 
treatments using small - particle embolization agents ( i.e. , smallparticle embolization ) , such as 300500m gel foam or polyvinyl alcohol ( pva ) particles , have been recently investigated . 
these agents greatly reduce the extent of embolism and improve hemostatic efficacy . nonbronchial artery pulmonary circulation shunt , especially intercostal arterypulmonary artery shunt , is usually accompanied by massive hemoptysis when pulmonary lesions spread to the pleura [ 12 , 13 ]  . 
this may be due to the low number of clinical reports about ipvs , which is usually ignored during treatment because the incidence rate is low [ 14 ]  . this retrospective study used dsa to investigate the safety and efficacy of small - particle embolization in patients with massive hemoptysis and ipvs . methods patients from february 2009 through september 2015 , 207 patients underwent bae , for the management of massive hemoptysis [ 111 ]  . 
twenty - four of these patients received a diagnosis of ipvs determined by dsa and were included for the final analysis . of the 24 ipvs patients in the study population ( 7 women , 17 men ; aged 3272years ) , 15 and 9 , respectively , had first - time and recurrent hemoptysis . 
these patients did not achieve effective hemostasis by the traditional hemostatic medications and were subjected to examination with dsa , computed tomography angiography ( cta ) of the bronchial artery , and then interventional embolization . 
in addition , based on the location of lung lesions and associated pleura determined by ct , the following were explored : bronchial artery dominated by the vagus nerve ; ias ; branches of the subclavian artery ; esophageal inherent artery ; and phrenic arteries . vagus nervedominated bronchial artery intravascular embolization based on the angiographic findings for the bronchial artery and nonbronchial systemic arteries , embolization was performed with a 3f superselective microcatheter ( terumo , tokyo , japan )  . 
embolization agents included pva particles ( 300500m ) and microcoils ( mwce - 35 - 3 - 3 , mwce35 - 3 - 4 , mwce - 35 - 3 - 5 ) , both supplied by cook medical ( bloomington , usa )  . for ia embolization , pva was used when the volume of ipvs was 4ml . 
when the vascular angiography was performed , a dose of contrast agent ( adequately displayed the shunting phenomenon and did not flow back ) greater than 4ml was larger flow volume , and less than 4ml was small flow volume . clinically successful embolization was determined by disappearance of the ipvs and abnormal ia network , or retention of contrast agents in the ia . 
the bronchial artery was embolized in the same way as described above . postoperative treatment dsa was performed using the standard angiography suites innova 3100iq ( ge , fairfield , usa ) and fd20 ( philips amsterdam , netherlands ) , with odixanol isotonic non - ionic contrast agent ( visipaque , 320mgi / ml ; ge , carrigtohill , ireland )  . 
the flow rate of contrast agent was manually adjusted to guarantee clear visualization all patients were required to lie and relax in bed , without extensive right leg movement , for 24h . 
 percussion on the back was performed if it was difficult for the patient to discharge sputum or hemoptysis . 1 3 590 la radiologia medica ( 2019 ) 124 : 588594 patients were followed for 148months , with an average of 30months . 
the ct results of all patients suggested involvement of the pleura ( figs.1a and 2a ) , with clearly thickened pleura in some cases ( table1 )  . dsa images ofculprit arteries a total of 51 culprit bronchial arteries ( diameter 2mm ) , two left internal thoracic arteries , and two left phrenic arteries were identified by dsa . 
contrast agents entered the branches of the pulmonary vein through the ia in a spray pattern , and flowed back to the left atriuthe main pulmonary vein was straight and clear in dsa images . 
c the right ia embolism and pulmonary vein shunt disappeared after embolization with microcoils combined with 300500m pva particles 1 3 la radiologia medica ( 2019 ) 124 : 588594 fig . 
a ct scan showed a shadow on the right upper lobe of the lung and involved pleura , in which thickened blood vessels could be observed ( arrow )  . 
however , the main pulmonary vein was light , due to the small shunt volume . in this study , we identified nine large volume ipvss and 30 small - volume ipvss . 
the dsa results of all patients corresponded well with the results of the cta of the bronchial artery , except for one culprit left phrenic artery that was identified during the operation . interventional embolization the superselective microcatheter was inserted into the ia , without disturbing the individual spinal artery . 
for embolization , pva particles ( 300500m ) were used in 7 smallvolume ipvss , and pva particles combined with microcoils ( pva + mc ) in 30 small - volume ipvss . embolization was not performed for one ia , since the mouth of this ia was too narrow to form an acute angle with the main artery and the cobra catheter could not be applied . 
 embolization could not be accomplished for another ia , because the wall of the artery was damaged by the catheter during operation . artery dissection was found after 2min when the microwire began to smoke during repeat micro - wire operation . 
the complications improved within 1week after proper treatment . 1 3 592 la radiologia medica ( 2019 ) 124 : 588594 the short - term follow - up found that hemoptysis recurred in two patients , with blood volume < 300ml ( the hemoptysis volume before embolization ) ( table3 )  . 
massive hemoptysis was cured after treatment with bae . during the mid - term follow - up , hemoptysis reoccurred in one patient 6months after the embolization ( table3 )  . 
the long - term effective rate was 75.0%. discussion hemoptysis with intercostal artery involvement is often accompanied by body - pulmonary circulation shunt , with thickened pleura and the involved lung tissue close to pleura . 
 the pathogenesis of ipvs indicates an increased intercostal artery flow due to the pleural or subpleural inflammatory disease , following by the formation of a shunt with the adjacent pulmonary venous system . in this study , we found that 11.6% ( 24 / 207 ) of patients with massive hemoptysis had ipvs , which is a lower occurrence rate than intercostal arterypulmonary artery shunt . 
since patients in this study mainly had bronchiectasis , thus the overall incidence of body - pulmonary circulation shunt is relatively low . patients with intercostal arterial - pulmonary vein shunt showed thickened intercostal artery , with early development during intercostal arteriography . 
the larger area or the thicker pleura indicated greater abnormal proliferation of the vascular network and a bigger shunt volume . in our study , dsa with hand - push was carried out to avoid blood vessel damage caused by the high - pressure syringe , and the proper flow rate according to the shunt volume was selected to guarantee clear development of the pulmonary vein without reflux . 
the direction of blood flow in the pulmonary artery was away from heart . for patients with diabetes or hyperlipidemia , the placement of the catheter should be gentle enough to avoid the artery wall , spinal artery damage , artery dissection , or vagal reflex . 
for example , in our study , one phrenic artery was not found by bronchial artery cta , but was identified by further examination during the operation . in our study , all microcatheters were inserted into the main intercostal artery with care to avoid the spinal artery during the operation . 
the small pva particles could more closely approach the shunt to reduce the possibility of re - communication between blood vessels and the opening of collateral circulation , achieving better hemostasis . 
the lesson we learned from these cases was that the catheter insertion 1 3 la radiologia medica ( 2019 ) 124 : 588594 must be as gentle as possible to avoid damage to the artery wall and angiorrhexis . 
for example , rlg or yashiro catheter could be used to replace the cobra catheter if the cobra catheter insertion failed . the intercostal artery has an important role in blood supply to the thoracic cage , including the spinal cord , thoracodorsal muscle , and thoracodorsal skit usually does not supply the lung . 
this indicated that main artery embolization alone cannot successfully stop hemoptysis . embolization particles > 350 m or nbca ( n - butyl cyanoacrylate ) agents are safe for bps and do not induce serious complications [ 16 ]  . 
thus , we suggest that coils can be applied first to slow the blood flow before performing the embolization . it has been reported that simultaneous embolization of the bronchial , intercostal , thoracic , and phrenic arteries can cause respiratory muscle ischemia , or even dyspnea . 
we should be cautious to avoid embolization of the intercostal artery , especially embolizing multiple intercostal arteries , for patients with poor respiratory function . taken together , we think that blocking the main intercostal artery and shunt can correct abnormal blood flow , reduce the pressure in branches of the pulmonary vein to stop bleeding , and decrease the possibility of bacterial spread and ectopic embolization formed by a microthrombus . in summary , 300500m pva particles alone or combined with microcoils was safe for intercostal artery embolization . 
together with excellent postoperative prevention and management of lung infection [ 19 ] , our embolization achieved good efficacy . the limitation of this manuscript is that this is a retrospective study and monocentric review , and prospective studies include multiple centers with more patients should be conducted in the future to verify our findings . intercostal artery embolization with 300500m alone or combined with microcoils is a safe and effective procedure in patients with ipvs - induced bronchial hemoptysis . compliance with ethical standards conflict of interest yonghui liang declares that he has no conflict of interest . 
written informed consent was obtained from each included patient . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 671681 radiotherapy trends incombined radiochemotherapy forlocally advanced rectal cancer : asurvey amongradiation oncology centers ofsicily region onbehalf ofairo giuseppeprivitera1 robertomilazzotto1 , 2 alessandratocco1 , 2 graziaacquaviva3 corradospatola1 francescomarletta3 lorenzamarino4 alfiodigrazia4 rosalbasalvo5 giovannicartia5 angeloplatania6 lauramolino2 , 7 annasantacaterina6 marilenamattaceraso8 pasqualefrosina8 robertoianni9 michelebono9 lucaliardo10 salvatorebonanno10 leonardalapaglia11 manuelafederico11 ivanfazio11 gianlucamortellaro12 giuseppeferrera12 antonellatripoli12 giovannaevangelista12 antoninodaidone13 giampaolobiti13 marcobadalamenti13 luciaognibene13 albertocacciola2 , 7 silvanaparisi2 , 7 stefanopergolizzi2 , 7 received : 20 november 2018 / accepted : 11 february 2019 / published online : 26 february 2019 italian society of medical radiology 2019 abstract aim to conduct a survey among sicilian centers of radiation oncology belonging to associazione italiana di radioterapia ed oncologia clinica ( airo ) , to record the different methods of integration of radio - chemotherapy both in neoadjuvant and adjuvant settings , to evaluate surgical procedures in relation to the sphincter preservation and to report the different toxicity profiles of the treatment strategies . methods a questionnaire was sent at the end of 2017 to all the radiation oncology centers of sicily region in order to collect the data from individual centers and the treatment characteristics retrospectively over the previous 5years , from 2012 to 2016 . 
the requested data concerned the type of integrated treatment ( neoadjuvant vs adjuvant vs radical ) , combination with chemotherapy ( induction , concomitant , adjuvant ) , type of surgical intervention ( sphincter - saving vs abdomino - perineal resection ) , disease stage , schedule and radiotherapy technique adopted , as well as toxicity detected over the treatment period . results a total of 784 pts ( m / f : 509 / 275 ) were treated between 2012 and 2016 , with a median age of 67years ( range 2592 )  . 
 the majority of patients was treated in the neoadjuvant phase ( 62% of the total ) compared to the adjuvant phase ( 31% ) and to those treated radically ( 7% )  . 
the use of chemotherapy alone before concomitant treatment is more common for patients treated in the adjuvant phase ( 64% of this subgroup ) , while 14% of patients treated in the neoadjuvant phase received induction chemotherapy before the concomitant phase ; in both cases of chemotherapy alone , the majority of patients ( 91% ) received oxaliplatin - based protocols ( folfox / xelox / capox )  . 
the overall rate of sphincter - saving surgery ( anterior resection ) was 72% , but the contribution of neoadjuvant treatment allowed to reach a rate of 83% in this subgroup ( against 65% found in the subgroup of patients treated in adjuvant phase )  . 
traditional radiotherapy schedule ( 4550gy in 2528 fractions ) was used in 90% of patients , of which an intensified treatment in neoadjuvant phase ( 45gy + boost of 910gy ) was used in 11% of patients . 
interestingly , the toxicity rates were significantly higher in the adjuvant group compared to the neoadjuvant ( gi : 58% vs 31% , gu : 21% vs 10% )  . extended author information available on the last page of the article vol . : ( 0123456789 ) 1 3 672 la radiologia medica ( 2019 ) 124 : 671681 conclusion the present survey shows that in the sicily region integrated therapies for rectal cancer have allowed a neoadjuvant approach in the majority of patients , thus resulting in a greater use of sphincter conservative surgery . 
the toxicity has also been reported to be significantly less in this treatment setting . keywords rectal cancer survey airo neoadjuvant treatment radio - chemotherapy introduction from an epidemiological point of view , cancer of the rectum is usually associated with colon cancer , as the majority of studies does not consider the two pathologies separately ; generally , in clinical trials we often refer to colorectal cancer . 
in italy , about 53.000 new cases are diagnosed per year [ 2 ] , representing the second most incident cancer in men ( after prostate cancer ) and in women ( after breast cancer )  . 
of these , around 30% arises from the rectucolorectal cancer prognosis is considered favorable , with survival rates for rectal cancer at 5 and 10years of 62% and 58% , respectively . 
the overall mortality in the world for colorectal cancer is about half of the incidence : in particular , mortality is decreasing in both males and females due to early diagnosis and admission to better surgical treatments and adjuvant therapies . 
in italy , compared to northern regions , the southern regions register lower survival rates of about 68% in males and 56% in females , with a trend toward improvement in recent years . 
in sicily , the incidence and prevalence of colorectal cancer is lower than other italian regions ; on average , based on the regional cancer registries report of years 20032011 , 1623 , 4 new cases are estimated per year in male and 1410 , 8 new cases in female . 
the 5 - year survival rate is 60% for both sexes [ 2 , 3 ]  . management of rectal cancer is a matter of debate , in particular regarding the timing of single therapeutic approaches . 
 surgery still represents the main treatment for rectal cancer , and the implementation of total mesorectal excision has dramatically reduced the local recurrence rates for locally advanced tumors [ 4 ]  . 
radiotherapy maintains a relevant role in increasing local control rates , both in preoperative and postoperative setting compared to surgery alone [ 5 ]  . in locally advanced rectal carcinoma ( larc ) of the middle - lower rectum ( localized to < 12cm from the anal verge ) , preoperative long - course radiotherapy in combination with chemotherapy with 5 - fluorouracil or capecitabine is the standard treatment , statistically reducing the incidence of local recurrences and prolonging overall survival [ 69 ]  . 
adjuvant radio - chemotherapy should be considered the standard care for patients with pt1 - 3 n1 - 2 m0 cancers , while management of pt3 n0 m0 patients is still a matter of debate . herein , we report the results of a survey conducted among sicilian centers of radiation oncology in order to assess the trend in the management of locally advanced rectal cancer , in light of the changes emerging over time from clinical trials and from the new technological developments . 
the current survey would represent the starting point to improve the integration between different therapeutic modalities and to optimize and standardize the therapeutic strategy . materials andmethods the survey was organized in radiation oncology centers of sicily region belonging to associazione italiana di radioterapia ed oncologia clinica ( airo ) by sending a questionnaire at the end of 2017 to collect the data from individual centers regarding clinical and technical aspects of radiotherapy treatments for patients affected by locally advanced rectal cancer . it was decided to collect data over a period of 5years , from january 2012 to december 2016 , in order to have a sufficient follow - up time for reporting the results and toxicity of the treatments . 
the data collected refer , in relation to the single catchment areas , to about 85% of the sicilian population that was , according to the last surveys of istituto nazionale di statistica ( istat ) , of 5 , 026 , 989 people . 
three other centers did not return the questionnaire within 6months from the date of submission and have been therefore excluded . patient data a total of 784 pts ( male / female : 509 / 275 ) were treated with radiation therapy for larc between 2012 and 2016 , so they were included in the survey and all clinical and technical data were collected . 
the distribution of patients by gender and age reflects what was shown at national level by the aforementioned aiom - airtum report , with the exception of a significant higher incidence in the male sex compared to the female , that did not correspond to the epidemiological data from the sicilian regional cancer registries [ 2 , 3 ]  . 
the incidence of the disease in the sicilian regional population appears to be smaller than the national average , and it is worth to note that about one - third of the incident cases have been treated with radiotherapy at sicilian centers . 
this would probably be related , at least in part , to interregional health migration , to a missed indication to radiotherapy or to the patients difficulties to reach radiotherapy departments . staging procedures atdiagnosis andtemporal distribution ofpatients all patients received an endoscopic procedure in order to perform a biopsy for histological confirmation of the disease before to be treated . 
an eus staging was performed in a minority of patients ( 28% ) , while a higher percentage ( 52% , 497 pts ) received a pelvic mr for local staging . 
a small amount ( 14% ) of pts received a pet or pet / ct as a part of initial staging of disease . histology was adenocarcinoma in almost all cases , with only 2% of other histologies ( i.e. , squamous cell cancer ) and 6% of carcinoma nos . 
tumor regression grade ( trg , according to dworak ) was evaluated in patients undergoing neoadjuvant radiotherapy in almost all cases . the temporal distribution of patients recruitment at radiotherapy centers is specified below : year 2012 : 137 pts year 2013 : 166 pts year 2014 : 159 pts year 2015 : 140 pts year 2016 : 182 pts treatment strategy the differences reported across the years do not reach the statistical significance . radiation therapy was prescribed with curative intent in 729 patients ( 93% ) , before or after surgery . 
the treatment had instead a radical purpose in 55 patients ( 7% ) , for whom 1 3 674 la radiologia medica ( 2019 ) 124 : 671681 no surgical indication was given . 
patients with local recurrence of carcinoma of the rectum were excluded from the survey . the spread of the neoadjuvant preoperative strategy has been significant , and indeed this therapeutic approach has been implemented in 486 patients ( 62% ) , while the adjuvant postoperative strategy has been applied in 243 patients ( 31% )  . 
oral capecitabine was preferred in 429 patients ( 73% ) , and continuous infusion of 5 - fluorouracil was used in 159 patients ( 27% )  . treatment strategy also included a systemic chemotherapy before concomitant radio - chemotherapy phase in 224 patients : this strategy has been more frequently used in patients treated in the adjuvant phase ( 64% of the subgroup ) , compared to those treated in the neoadjuvant phase ( 14% of the subgroup )  . 
the induction chemotherapy strategy , before concomitant rt - ct , was in the majority of cases oxaliplatin - based , with folfox , xelox or capox protocols . twenty - five percent of patients ( n = 196 ) did not receive combined chemotherapy , mainly for cardiovascular diseases . the therapeutic strategy is obviously dependent on tumor staging at the time of recruitment ( table2 )  . 
consequently , considering that the diagnosis of larc is conducted differently in the different centers , we classified the patients recruited as follows : ct2 - 3nx 186 pts , ct2 - 3n + 253 pts , ct4nx / + 47 pts . 
the patients treated in the postoperative adjuvant phase had the following distribution by stage : pt2n1 - 2 18 pts , pt3n0 74 pts , pt3n1 - 2 123 pts , pt4n0 12 pts , pt4n1 - 2 16 pts . 
patients treated without surgery had the following distribution by stage : ct3nx / + 19 pts , ct4nx / + 36 pts . table 2 patients distribution for treatment strategy , systemic therapy and stage at recruitment treatment strategy curative ( with surgery ) neoadjuvant treatment adjuvant treatment radical or palliative systemic chemotherapy concomitant capecitabine concomitant 5fu induction oxa - based chemotherapy before rt - ct adjuvant chemotherapy after rt - ct no chemotherapy stage distribution in neoadjuvant setting ct2 - 3nx ct2 - 3n + ct4nx / + stage distribution in adjuvant setting pt2n1 - 2 pt3n0 pt3n1 - 2 pt4n0 pt4n1 - 2 stage distribution in radical / palliative setting ct3nx / + ct4nx / + number ( percentage ) 729 ( 93 ) 486 ( 62 ) 243 ( 31 ) 55 ( 7 ) 588 ( 75 ) 429 ( 73 ) 159 ( 27 ) adjuvant strategy : 156 ( 64 ) neoadjuvant strategy ( intensification regimens ) : 68 ( 14 ) 18 ( 3 ) 196 ( 25 ) 486 ( 62 ) 186 ( 38 ) 253 ( 52 ) 47 ( 10 ) 243 ( 31 ) 18 ( 7 ) 74 ( 30 ) 123 ( 51 ) 12 ( 5 ) 16 ( 7 ) 55 ( 7 ) 19 ( 35 ) 36 ( 65 ) 5fu 5 - fluorouracil , oxa oxaliplatin , rt - ct radio - chemotherapy , rt radiotherapy 1 3 la radiologia medica ( 2019 ) 124 : 671681 radiotherapy schedule anddata fromsurgery radiotherapy was performed in most cases with a longcourse schedule ( 706 pts , 90% ) , with a total dose ranging from 45 to 60gy , both in neoadjuvant and adjuvant settings . 
 in neoadjuvant setting , a portion of the sample of patients ( 88 pts , 11% of total , but 18% of neoadjuvant group ) was treated with an intensified schedule . 
a small sample of patients ( 35 pts , 4.5% ) was treated with long - course regimen to a radical dose of 60gy , because they were judged inoperable , because of medical reasons or technically unresectable tumor . 
figure1a , b shows the details of the regimens used in the radiotherapy treatments . conven ( cid : 31 ) onal frac ( cid : 31 ) onated rt : 706 pts ( 90% ) hypofrac ( cid : 31 ) onated rt : 78 pts ( 10% ) toxicity 45 gy wp ( neoadjuvant / adjuvant ) 50 gy wp ( neoadjuvant / adjuvant ) 45 gy wp + 9 gy boost ( intensied neoadjuvant ) 50 gy wp + 10 gy boost ( radical rt ) 25 gy in 5 frac ( cid : 31 ) ons ( neoadjuvant short - course ) 30 - 39 gy in 10 - 13 frac ( cid : 31 ) ons ( pallia ( cid : 31 ) ve ) legend : wp : whole - pelvis radiotherapy fig . 
1 radiotherapy schedule used in conventional fractionated rt ( a ) and in hypofractionated rt ( b ) three - dimensional conformal technique , performed using a 3 - field technique with the patient in the prone position or with a box technique with the patient in the supine position , was preferred in the majority of centers and it was employed in 572 patients ( 73% )  . 
an intensity - modulated technique , with static step - and - shoot technique or volumetric arc - therapy , was employed in 212 patients ( 27% ) , in order to reduce dose to small bowel and bladder and increase treatment tolerability , especially for patients treated in the postoperative adjuvant phase . the survey questionnaire did not explicitly require the target volumes to be specified , which will probably be the subject of evaluation of a subsequent multicentric survey . 
 nevertheless , most of the centers participating in the survey ( 10 / 13 ) reported to have followed the airo guidelines on gastrointestinal tumors during the treatment planning procedures . surgery was performed in 729 patients ( 93% ) , and information on surgical treatment received is available for 690 patients ( 88% )  . 
data from surgery are available and complete for patients treated in adjuvant phase , while those for patients treated preoperatively are partially complete , as sometimes the follow - up is carried out by other specialists . 
the rate of sphincter - saving surgery reaches 83% in the subgroup treated with neoadjuvant combined radio - chemotherapy , versus the rate of 65% of pts treated in adjuvant phase . adjuvant radiotherapy was performed after a median time interval from surgery of 7 weeks , with a range of 512weeks . 
in the subgroup of neoadjuvant radiotherapy , the conventional interval time to surgery of 1week , in case of short - course rt , and 69weeks , in case of long - course rt , was respected in the majority of patients ( 85% )  . data on toxicity were complete for what concerns acute and subacute toxicity , since the visits during radiotherapy and in the immediate post - treatment are conventionally carried out every week in all the centers . 
as specified before , the common terminology criteria for adverse events ( ctcae v5.0 ) criteria were utilized commonly . overall , most patients reported grade i and ii toxicities , both gastrointestinal ( gi , 39% ) , cutaneous ( 23% ) and genitourinary ( gu , 14% ) , without any need to stop treatment . 
 grade iii diarrhea was developed by 31 patients ( 4% ) , of whom 20 were treated in the adjuvant phase , nine in the neoadjuvant phase and two treated radically ; a treatment interruption of 613days was then necessary in these cases , with a definitive suspension of chemotherapy . 
2 acute / subacute toxicity report in patients treated with neoadjuvant , adjuvant or radical strategy la radiologia medica ( 2019 ) 124 : 671681 toxicity report neoadjuvant treatment adjuvant treatment radical / pallia ( cid : 15 ) ve treatment gi grade i - ii tox gu grade iii tox gi grade iii tox gu grade i - ii tox skin grade i - ii tox skin grade iii tox hematologic grade i - ii tox hematologic grade iii tox legend : gi : gastro - intes ( cid : 15 ) nal . 
overall , 56% of patients performed follow - up at the radiotherapy centers , so late toxicity data are only partially available , with 83 patients ( 10% ) reporting symptoms of anal sphincter discomfort , rectal tenesmus , fecal incontinence or , on the contrary , evacuative difficulties . 
 cases of chronic post - actinic enteritis with subocclusive crises were not common ( 2% )  . discussion the management of locally advanced rectal cancer has undergone remarkable changes in recent years . 
the development of total mesorectal excision surgery and the evidences from randomized clinical trials about the use of radiotherapy and , especially , the addition of fluorouracil to radiotherapy have definitively confirmed their role in the management of this pathology in order to reduce local recurrences and to improve survival . 
randomized clinical trials have also shown that radiotherapybefore surgery further improves local control [ 8 , 1416 ]  . nevertheless , there are still many inconsistencies in the management of these patients , both during the diagnostic and staging phase , both for the treatment and the timing of the various interventions . 
the development of multidisciplinary teams can aid in increasing the use of preoperative radiotherapy and the rates of sphincter - saving procedures , as reported in the literature [ 17 ]  . the present survey was conducted in order to assess the trend in the management of larc in sicily , to record the different methods of staging and treat such disease , through the integration of radio - chemotherapy both in neoadjuvant and adjuvant settings , with the aim to improve , optimize and standardize its management . the epidemiological data from sicilian cancer registries , updated to 2016 but related to the period 20032011 , show a regional median incidence of 5509 new cases per year of rectal cancer in male and 4062 new cases per year in female . 
 according to the regional cancer registries , the male / female ratio is 58% / 42% ; our report , on the other hand , shows a higher prevalence of male sex , with a ratio of 65% / 35% . 
the overall number of new patients in the regional population is , moreover , quite higher than the number of patients treated with radiotherapy at the regional centers . the difference is probably due to a series of motivations . 
moreover , the latter are related to all tumors of the rectum , including initial stages and local recurrences , while the survey refers only to cases of locally advanced cancer . 
in this regard , the difficulty of patients to reach radiotherapy centers and the lack of treatment indication , especially for > 75yearold patients , may play a significant role . 
finally , it must be remembered that the survey was completed by 13 out of 17 sicilian radiotherapy centers , which overall treat a catchment area of about 85% of the regional population . 
the relatively low absolute number of rectal cancer patients treated at sicilian radiotherapy centers can be explained by all these motivations , as well as by the controversies related to the 1 3 la radiologia medica ( 2019 ) 124 : 671681 indication to the radiation treatment for patients suffering from pt3n0 disease . the survey highlighted significant differences between the various centers in relation to the pre - treatment staging procedures , especially for patients undergoing neoadjuvant therapy . 
regarding local staging for patients undergoing neoadjuvant radiotherapy , airo guidelines [ 18 ] , while not giving clear indications , confirm the role of transrectal echoendoscopy and pelvic mri in assessing the depth of parietal invasion and lymph nodes involvement . 
 the literature data [ 1113 , 19 , 20 ] show that mri has a greater accuracy than echoendoscopy on the definition of t ( 94% vs 90% ) and above all of n ( 85% vs 7383% )  . 
our survey showed a considerable diffusion of the use of mri in local staging , used in 52% of patients , while the use of eus appears to be reduced ( 28% of patients )  . 
regarding systemic staging , the use of chest and abdomen ct was superior than that of pet / ct scan ( 55% vs 14% )  . the main purpose of the survey was to effectively evaluate the diffusion of the organ preservation strategies at the sicilian regional radiotherapy centers , and in particular of the radio - chemotherapy neoadjuvant treatment , as within the regional airo sicilia group there was feeling of reduced use in clinical practice of this therapeutic strategy . 
surprisingly , however , we could point out that around two - thirds of the treatments carried out followed a neoadjuvant treatment strategy ( 62% ) , whose main objective is to reduce the percentage of local recurrences and to increase the resectability . 
 patients treated with radical intent to a dose of 60gy ( 4.5% ) should be added to the sample of patients treated in neoadjuvant : they were not candidates for surgery for various reasons , but nevertheless they maintained an organ preservation . 
unfortunately , the proportion of patients treated postoperatively is quite high ( 31% ) , and it deserves a further reduction , but this is due to the persistent resistance of some surgeons and the slow diffusion of multidisciplinary groups , especially in peripheral hospital centers . trials published over the last decades have indisputably demonstrated the superiority of neoadjuvant compared to adjuvant approach [ 14 , 16 ]  . 
from a careful analysis of the collected data , it can be pointed out that this practice remains more widespread in radiotherapy centers that do not have a direct collaboration with the surgeons , generally due to logistic problems . 
this involves often a unilateral therapeutic management by the surgeons at the time of recruitment , with consequent less indications to the neoadjuvant strategy . adjuvant treatment has the advantage to allow a better selection of patients , according to the pathological stage , but at the expenses of an increased acute and late toxicity , mainly gi . 
there is no difference between adjuvant and neoadjuvant approaches in terms of distant metastases [ 6 ]  . concurrent 5 - fluorouracil chemotherapy in combination with radiotherapy is considered the standard of care for larc [ 7 , 8 ]  . 
oral capecitabine has demonstrated the non - inferiority to 5 - fu [ 9 ] , so today the two drugs are considered equivalent , and capecitabine is often preferred for a better clinical compliance , with reduced issues related to the central venous access . 
the survey has demonstrated a broad adherence in the regional territory to this therapeutic standard : concomitant capecitabine was preferred in 73% of the sample , while continuous infusion of 5 - fu was administered in 27% of patients . 
regarding the use of other compounds , mainly oxaliplatin , 224 patients ( 64% of the adjuvant group and 14% of the neoadjuvant group ) were treated with folfox or capox or xelox protocol , for a median of 36 cycles , before concomitant radio - chemotherapy . 
the combination of 5fu and oxaliplatin is widely employed in adjuvant setting , both in colon and in rectal cancer , due to the evidence of a significant improvement in disease - free and overall survival [ 21 ] , but there is yet no clear evidence for the efficacy of adding oxaliplatin to the neoadjuvant multimodal treatment of patients with locally advanced rectal cancer . 
therefore , the data of currently available randomized trials using oxaliplatin - based chemotherapy in neoadjuvant setting did not allow a diffusion in clinical practice , so their use remains experimental [ 15 , 22 , 23 ]  . 
chemotherapy was not administered in 25% of the sample , mainly due to cardiovascular diseases . long - course radiotherapy is considered the standard of care both in adjuvant and neoadjuvant settings , and our data are in accordance with this clinical practice : 706 patients ( 90% of the total ) were treated with conventional fractionation to 4550 , 4gy , 125 of which treated up to 5460gy . 
 this regimen is widely considered the most appropriate when the treatment goal is to maximize tumor downsizing , increase resectability rate of initially bulky tumors and to ameliorate the rate of sphincter - saving surgery in patients initially candidate to abdomino - perineal resection . as previously reported , a fair number of patients in the survey ( 88 pts , 11% of the sample ) were treated with an intensified preoperative regimen with a concomitant boost to a total dose of 54gy . 
according to the standard of care of 4550gy , a median of 15% of pathological complete response ( pcr ) is reported in randomized trials [ 8 , 1416 ]  . 
 it is believed that an increased dose to the site of primitive tumor may allow to improve the rate of tumor regression and 1 3 678 la radiologia medica ( 2019 ) 124 : 671681 of pathologic complete response [ 24 ] ; recent trials reported a pcr rate up to 30% when an intensification regimen was adopted , generally using a boost to the macroscopic disease attempting to increase the rate of organ preservation [ 25 ]  . 
it is worth to note that , to date , there is no consensus about prescription dose , target volume definition and combination chemotherapy , so further confirmations from randomized trials are needed to allow the intensified treatment to be disseminated in clinical practice . short - course neoadjuvant protocol , 25gy in 5 fractions in a week , has been used in a few patients ( 58 pts , 7% )  . 
however , the lack of combination chemotherapy and of tumor downsizing make it not useful when patients are not candidate initially to a sphincter preservation and when mesorectal fascia is infiltrated or close to the tumor . it has been demonstrated that the rate of local control is similar between long - course and short - course radiotherapy [ 26 ]  . 
other hypofractionated regimens were adopted for 20 patients ( 2.5% ) , mainly with palliative intent for inoperable patients with low performance status , in order to reduce local symptoms ( pain or bleeding ) or the risk of occlusion . the survey reports information on the main technical aspects of radiotherapy treatment : a three - dimensional conformal technique was largely preferred toward intensity - modulated ones ( 73% vs 27% )  . 
the rationale for using imrt or vmat is to reduce dose to the small bowel and bladder and to reduce the incidence of gastrointestinal and genitourinary toxicity , especially for patients treated in postoperative adjuvant phase or when clinically or technically required . 
almost all centers participating in the survey followed the above - mentioned airo guidelines to define setup procedures , volumes of interest definition , planning , dose reporting and delivery , according to icru 62 and quality assurance procedures [ 18 , 2729 ]  . organ preservation is considered an additional goal of larc treatment . 
in recent years , it has been playing an increasing role and this has fostered novel targeted trials of intensification of treatment , both for chemotherapy and for radiotherapy [ 15 , 25 , 30 , 31 ]  . 
however , it should be noted that often the information related to the surgical treatment received by patients treated with neoadjuvant strategy is incomplete , as patients are lost to follow - up , which is often conducted by other specialists . 
in our case series , about 15% of patients have no data on the surgical treatment received after neoadjuvant radio - chemotherapy , while the surgical data of patients treated in the adjuvant phase are comprehensive . 
 taken together this data suggest that greater diffusion and integration of multidisciplinary groups is desirable in order to better understand and integrate the surgical information and the follow - up data . the increased rate of sphincter - saving surgery reported in our case series in the group treated with neoadjuvant approach does not allow definitive conclusions to be drawn , as the survey was not aimed at evaluating this parameter . 
 however , the data is in line with previously reported studies , according to which the use of the neoadjuvant approach should be considered in all patients with low rectal cancer that are not candidates for organ preservation at diagnosis . as regard toxicity , the literature clearly shows that combined radio - chemotherapy increased the rate of gastrointestinal toxicity [ 69 ] compared with the use of radiation only . 
 protocols of chemotherapy and / or radiotherapy intensification [ 15 , 21 , 22 , 25 , 31 ] have reported a further increased toxicity compared with conventional radio - chemotherapy . 
as previously pointed out , most patients reported grade iii side effects ( ctcae v5.0 ) , while grade iii gastrointestinal toxicity was reported in only 4% of sample , most of which were treated in the adjuvant phase [ 32 , 33 ]  . the tolerance of combined radio - chemotherapy is greater with the neoadjuvant approach compared to the adjuvant one . 
in the postoperative phase , in fact , as a consequence of the surgical amputation and the poor use of the surgical devices supporting the intestinal loops , the latter have greater exposure to irradiation , especially with the use of 3d - conformal radiotherapy technique . 
reports and images were evaluated by neurologists who assessed : disease - specific muscular involvement pattern ; presence of sufficient information to order the appropriate genetic / diagnostic tests ; presence of sufficient information to make therapeutic decision / perform biopsy and necessity to review mri images . 
mannwhitney and fishers exact tests were used to compare the number of key features for nsr and sr and neurologists answers for reports produced by neuroradiologists with different experience . results thirty - one srs and 101 nsrs were reviewed . 
when reports produced by expert neuroradiologists were evaluated , no significant difference in neurologists answers was observed . conclusion sr of ind - mri contained more often clinically relevant information considered important for disease management than nsr . 
radiologists expertise affects completeness of nsr reports . keywords magnetic resonance imaging neuromuscular diseases limb - girdle muscular dystrophies sarcoglycanopathies structured reporting * francesco alessandrino falessandrino@bwh.harvard.edu 1 neuroradiology department , irccs c . 
gemelli , rome , italy 3 radiology unit , istituto dermopatico dellimmacolata - irccs - flmm , rome , italy 4 neuroradiology unit , fondazione irccs ca granda ospedale maggiore policlinico , milan , italy 5 unit ofneuroradiology , irccs san raffaele scientific institute , milan , italy 6 neuroradiology unit , department ofimaging , irccs bambino ges childrens hospital , rome , italy 7 neuromuscular andrare diseases unit , department ofneuroscience , fondazione irccs ca granda ospedale maggiore policlinico , milan , italy 8 pediatric neurology andnemo clinical centre , universit cattolica del sacro cuore , fondazione policlinico universitario a . 
mondino foundation , pavia , italy 10 department ofbrain andbehavioural neuroscience , university ofpavia , pavia , italy 11 department ofradiology , harvard medical school , brigham andwomens hospital , 75 francis street , boston , ma02115 , usa vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 628635 introduction over the last few years , substantial progress has been made in the genetic diagnosis of inherited neuromuscular disorders ( ind ) with the identification of over 400 genetically distinct forms . 
this complex genetic heterogeneity makes the diagnosis extremely challenging since the most commonly used diagnostic tests , including muscle enzymes , electrophysiological studies , and muscle biopsy , are not always specific [ 1 ]  . 
it is well known that mutations in the same gene can originate different phenotypes and that the same phenotype and even the same muscle alteration detected by electron microscope can be the consequence of different genetic defects [ 2 , 3 ]  . there has been increasing evidence that muscle mri can be an important additional tool in diagnosis and follow - up of patients with ind , providing valuable information on muscle bulk , shape , volume , dystrophic , and inflammatory changes [ 48 ]  . 
mri often allows recognition of specific patterns of muscle involvement and has proved to be helpful in narrowing the differential diagnosis , aiding in the selection of the appropriate genetic and biochemical diagnostic investigations , as well as identifying which muscle to target for pathological studies [ 48 ]  . the advent of new next - generation sequencing and other molecular tools has significantly facilitated the diagnostic pathway in ind ; nonetheless , muscle mri still plays a relevant role in solving diagnostic dilemmas and in the interpretation of the results obtained from molecular panels . 
despite the bulk of evidence published in the last two decades , the use of muscle mri is still relatively limited to research settings or to a limited number of tertiary care centers . 
in the past decades , to overcome variability and increase completeness , consistency and readability of radiologic reports , structured report ( sr ) templates have been adopted in many fields of radiology , from oncologic imaging to neuroradiology [ 912 ]  . various studies analyzed the impact of clinician experience in evaluating sr in different fields of radiology , showing that sr more often contains adequate information for patient care with decreased variability compared to non - structured report ( nsr ) , in most cases [ 916 ]  . 
thus far , since muscle mri of ind has been mainly limited to tertiary care centers in which clinicians are often involved in the interpretation of the mri , and consequently , little has been reported about the possible use of sr in neuromuscular disorders and how srs are perceived by the referring clinician . 
the difficulties in this field are related to the accuracy of the reports but also to the fact that their interpretation should be based on the knowledge of the patterns of muscle involvement reported in the literature . the aim of this study was to establish whether sr of mri in patients with ind provides more clinically relevant information for disease management compared with nsr and whether the completeness of mri reports is affected by neuroradiologists level of expertise . materials andmethods study population institutional review board approval at all the institutions was obtained for this hipaa compliant study . 
from each institution , the radiology information system ( ris ) at the radiology departments of the various institution was queried for reports of mri of the lower limbs with indication of suspected / known ind generated 3years before ( from november 1 , 2013 , to october 31 , 2016 ) and 1year after implementation of a sr template ( from november 1 , 2016 , to october 1 , 2017 )  . 
only reports produced by a randomly selected neuroradiologist for each institution were included . in order to establish whether the level of expertise might have affected the accuracy of the sr and nsr , it was noted whether the mri reports were produced by neuroradiologists with more than 15years of expertise ( experienced neuroradiologists in reading mri for suspected / known ind ) or by less experienced neuroradiologists ( less than 15years of expertise ) in the corresponding referral clinical center for ind . 
all neuroradiologists reported a minimum of 50 mri reports for suspected / known ind per year . mri protocol given the retrospective nature and multi - institutional nature of the study , technical mri parameters varied among the different institutions . 
at a minimum , sequential , non - contrastenhanced , axial turbo spin echo ( tse ) t1 - weighted ( t1w ) and short - time inversion recovery ( stir ) sequences were used to study the lower limb muscles including the pelvic girdle , the thighs , and lower legs bilaterally . subjects lay in the scanner in the feet - first supine position , with the lower limbs lying in a comfortable position on the scanner bed . 
a fabricated thermoplastic splint and sandbags were used to stabilize the limbs and to minimize motion , 1 3 630 la radiologia medica ( 2019 ) 124 : 628635 when necessary . 
the patients did not receive any sedation and the total examination time was approximately 30min . mentioned in the report , regardless if the finding was positive or negative , and absent if not mentioned . turbo spin echo , t1w , and stir sequences were acquired on axial plane selected with respect to the long axis of the femoral shaft for the thighs and with respect to the long axis of the tibia and fibula for the lower legs . 
each muscle was evaluated throughout its length . scan parameters were as follows : tse t1 > tr 600ms , te 20ms , fov 1638cm ( selected according to patients size ) , pixel 1 1 , slice thickness 5 mm , flip angle 90 , interslice gap 0.5mstir > tr 4500ms , te 100ms , ti 150ms , fov 1638cm ( selected according to patient size ) , pixel 1 1 , slice thickness 5mm , interslice gap 0.5mm. descriptive analysis was used to identify the muscles that were more frequently affected in the different segments . 
each feature was considered present if the key features , in part based on a previous paper describing the pattern of muscular involvement in ind , were : ( 1 ) type of sequences acquired ( mention of type of sequence and part of body imaged ) ; ( 2 ) entity of the subcutaneous tissue relative to underlying muscular bulk ( increased , similar , or reduced ) ; ( 3 ) fat replacement of single muscle bundles ( mention of specific muscle ) ; ( 4 ) selective muscular involvement pattern , defined according to literature data ; ( 5 ) specific muscular involvement at the pelvic girdle ( mention of specific muscles ) ; ( 6 ) specific muscular involvement at the thigh ( mention of specific muscles ) ; ( 7 ) specific muscular involvement at the lower leg ( mention of specific muscles ) ; ( 8 ) specific muscle bundles hyperintense on t2 - stir sequences ; ( 9 ) overall impression [ 19 ]  . 
figure1 shows three examples of the key features evaluated on lower limb mri . evaluation ofreports andmri byclinicians after sr and nsr were selected for neuroradiologists evaluation of key features , a sample of de - identified randomly selected sample of sr and nsr was provided to clinicians for their evaluation . 
one neurologist for each institute with more than 15years of experience in ind management evaluated independently the reports and mri images . firstly , clinicians evaluated the reports : for each evaluation , clinicians were asked the following questions : 1 . 
case 1 : 16 - year - old male patient with suspected facioscapulohumeral muscular dystrophy ( fshd ) presenting with lagophthalmos , horizontal smile , winging scapulae , horizontal clavicula , limited upper limbs abduction and mild steppage gait . 
a t1 - weighted image acquired at the level of the thigh shows mild hyperintensity of the right long head of the biceps femoris muscle ( arrows ) and of both semimembranosus muscles , consistent with fat infiltration . 
b t2 / stir image acquired at the same level of the thigh showing hyperintensity of the left long head of the biceps femoris muscle and mildly of the semimembranosus of the same side , as a radiological sign of intramuscular edema ( arrows )  . 
c t1 - weighted image acquired at the level of the pelvic girdle shows fat infiltration of the bilateral gluteus maximus and gluteus medius muscles ( black arrowheads )  . 
case 3 : 11 - year - old male child with suspected limb - girdle muscular dystrophy presenting with positive gowers sign , waddling gait , prominent calf , winging scapulae and hyperlordosis . 
reports were initially screened for the presence of artifacts , 1 3 632 la radiologia medica ( 2019 ) 124 : 628635 completeness , and the presence of positive findings . 
mri reports mentioning the presence of artifacts ( n = 2 ) , interruption of the mri examination ( n = 1 ) , and mri reports with the absence of any positive findings ( n = 14 ) were excluded . 
 a total of 132 reports of lower limbs mri with indication of suspected / known ind created by a total of 6 neuroradiologists were included ; of these 101 were nsrs , 31 were srs . 
 sixty - eight mri reports were produced by neuroradiologists with more than 15years of experience in ind diagnosis ( 48 nsr and 20 sr ) , and 64 mri reports by less experienced neuroradiologists ( 53 nsrs and 11 srs )  . 
 regarding single key features , entity of the subcutaneous tissue relative to underlying muscular bulk ( p value : < 0.0001 ) , fat replacement of single muscle bundles ( p value : < 0.0001 ) , the specific muscular involvement at the thigh ( p value : < 0.0001 ) , at the lower leg ( p value : 0.0003 ) , and the presence of specific muscle bundles hyperintense on stir sequences ( p < 0.0001 ) were significantly more often reported in sr than nsr . 
the application of sr in various fields of radiology , from mammography to neuroradiology to have shown that this system has been useful to improve completeness and clarity of reports , facilitate data mining , and improve communications of results to the referring physician [ 11 , 21 , 22 ]  . our study showed that sr of mri in patients with ind contained more clinically relevant and important information for disease management compared with nsr . 
specifically , the entity of the subcutaneous tissue relative to underlying muscular bulk , the fat replacement of single muscle bundles , the specific muscular involvement at the thigh and lower leg and the t2 - stir hyperintensity of specific muscle bundles , were significantly more often reported in sr than in nsr . 
even though these findings are considered crucial for mri diagnosis of ind , our multi - institutional study shows these are not always mentioned in the mri reports , and the clinical practice varies widely according to neuroradiologists experience . 
a potential bias of this study is that the clinicians were often involved in the multidisciplinary discussion of the mri findings and that the reports may not always reflect the multidisciplinary discussion . 
nevertheless , since radiologic reports are formal documents that should be made available for patients , clinicians and other radiologists , our findings suggest that more attention should be paid to make sure that clinically relevant information is consistently present in the report . 1 3 634 la radiologia medica ( 2019 ) 124 : 628635 neurologists understood disease - specific pattern of muscular involvement and had enough information for making adequate clinical decision or to perform a biopsy more often when reading sr rather than nsr . 
furthermore , neurologists needed to evaluate images significantly less often to make decisions in patient care , when reading sr rather than nsr . these findings are in agreement with previous studies reporting that sr conveys adequate clinical information on imaging studies more often than nsr in other areas of neuroradiology and musculoskeletal radiology [ 11 , 12 , 2325 ]  . 
our study confirmed that also for mri reports of suspected / known ind , sr more often contains more often a significantly higher number of key features affecting management of this condition . similarly , regarding neurologist evaluation of reports , a previous study of our group showed that when evaluating brain mri reports of patients with known / suspected multiple sclerosis , experienced neurologists found that sr had more often sufficient information for clinical decision - making than nsr and needed to evaluate images to make clinical decision significantly more often with nsr [ 12 ]  . this study has some limitations , including its retrospective nature . 
we divided radiologists in only two categories based on their experience , more than 15years or less than 15 years of experience , clustering together novices and radiologists with moderate experience in reading mri for ind . 
more recent nsr might have been more informative than nsr performed years before , both for increased radiologist experience , and for the potential improvement related to peerreview of the cases . 
in this study , we did not evaluate this aspect , as we focused in comparing nsr with sr , although it is reasonable to predict that more recent nsr , might have been more complete than the nsr performed years before . our results clearly showed that the mri reports produced by neuroradiologists with more than 15years of experience in ind diagnosis , gave neurologists adequate information for patient care both when sr as when nsr , whereas when the report was produced by a radiologist with less than 15years of experience , only the sr gave the clinician sufficient information to understand the pattern of muscular involvement to make clinical decisions / to perform a biopsy . 
this does not suggest that muscle mri should be performed or interpreted only by very experienced neuroradiologists but rather that less experienced neuroradiologists should use sr as it will provide a structured approach to fill the mri report with all the relevant information . 
further studies are needed to establish the compliance to the use of sr within the same institution or across different institutions . in conclusion , our study suggests that sr can facilitate communication of findings and support neurologists in medical or therapeutic decisions and provide more complete information in patients with ind especially when reported by neuroradiologists with lower level of expertise . funding this research did not receive any specific grant from funding agencies in the public , commercial , or not - for - profit sectors . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent for this type of study formal consent is not required . la radiologia medica ( 2019 ) 124 : 682692 radiotherapy interobserver variability ofclinical target volume delineation indefinitive radiotherapy ofneck lymph node metastases fromunknown primary . 
acooperative study oftheitalian association ofradiotherapy andclinical oncology ( airo ) head andneck group mariannatrignani1 esterorlandi6 domenicogenovesi1 almalinabacigalupo7 angelaargenone2 saidedibiase1 danielamusio3 annamerlotti4 stefanoursino5 received : 31 october 2018 / accepted : 11 february 2019 / published online : 9 march 2019 italian society of medical radiology 2019 abstract background this study , promoted by italian association of radiotherapy and clinical oncology ( airo ) head and neck group , aimed to assess the current national practice of target volume delineation on a case of neck lymph node metastases from unknown primary evaluating inter - observer variability , in a setting of primary radiotherapy . materials and methods a case of metastatic neck lymph node from occult primary was proposed to 17 radiation oncologists . 
a comparison between following parameters of the ctvs was performed : centroids distances , dice similarity index ( dsi ) , jaccard index and mean distance to agreement ( mda )  . 
accurate target volume definition is thus an important goal and standard of quality to attain radiation oncology , in order to avoid geographic miss , reduced local control and poor survival , excessive irradiation of surrounding normal tissues and increased radiotherapy toxicity [ 16 ]  . 
highly conformal radiotherapy * marianna trignani marianna.trignani@unich.it extended author information available on the last page of the article techniques such as intensity - modulated radiotherapy ( imrt ) can increase the effects of contouring variability and inaccuracy , particularly in head and neck ( h&n ) cancer treatment where target definition is challenging and requires a detailed knowledge of h&n anatomy and pathways of tumor spread . 
several guidelines and contouring atlases have been proposed in an effort to standardize the h&n target delineation process defining both neck nodal levels for radiation oncologist practice and site - specific treatment recommendations regarding nodal station coverage [ 79 ]  . for h&n district , several authors studied the impact of inter - observer variation in organs at risk delineation , such as parotid glands , but few studies studied inter - observer vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 682692 variability in relation to h&n target volumes [ 10 , 11 ] and particularly in the setting of occult primary tumors . uptake value ( suv ) of 3.6. 
no other areas of abnormal accumulation were found . neck lymph node metastases from unknown primary represent a rare and heterogeneous malignant disease , accounting for 28% of the overall malignancies and 35% of all solid tumors [ 1216 ]  . 
prospective randomized studies are not available ; thus , treatment strategies differ widely and are based on retrospective studies , clinical experience and institutional policy [ 12 ]  . the present study , promoted by italian association of radiotherapy and clinical oncology ( airo ) head and neck group , was carried out with the aim of assessing the current national practice of h&n contouring with regard to a case of neck lymph node metastases from unknown primary and to evaluate inter - observer variability of target volume definition in a setting of primary radiotherapy . material andmethod this was a multi - institutional contouring dummy run in the context of a contouring course promoted by the airo head and neck cooperative group for a case of a patient affected by metastatic neck lymph nodes squamous cell carcinoma with an unknown primary site . case description in 2014 , a non - smoking 53 - year - old man found , by a selfexamination , a solid nodule formation located on the left site of the neck . 
at the neck and thyroid ultrasound procedure , two hypo - echoic thyroid nodules , measuring 4mm ( right lobe ) and 6mm ( left lobe ) , not vascularized and without suspect elastosonography characteristics , were identified ; a solid formation of oval shape , with inhomogeneous echogenicity ( maximum diameter of 25mm ) , adjacent to the left submandibular glands was also found . 
furthermore , it was required to define the anatomical node levels and mucosal site encompassed in the clinical target volume ( ctv ) ; considering three different dose levels corresponding to the risk of microscopic disease , ctvs were distinguished as follows : ctv high dose , ctv intermediate dose and ctv low dose [ 1719 ]  . 
finally , it was requested to indicate whether any ctv changes would be felt necessary in case of hpv positivity . contouring section a national reference rt center was identified on the basis of per - year head and neck cancer ( hnc ) - treated patients ( more than 30 ) and of hnc expertise according to scientific publications . 
contouring data from the latter were considered as the benchmark in the comparison analysis . methodology participant centers to the contouring dummy run promoted by the airo h&n group were requested to delineate target volumes by their clinical experience without specific instructions in terms of guidelines or recommendations and tools of contouring ( i.e. , atlas of reference )  . 1 3 684 la radiologia medica ( 2019 ) 124 : 682692 the planning ct scan was obtained with a standard acquisition protocol ( supine position , thermoplastic mask immobilizing both head and shoulders ; slice thickness of 2mm and reconstruction interval of 2mm )  . 
 a comparison between these parameters of the ctvs was performed [ 2022 ]  . descriptive statistics ( minimum , maximum , mean , standard deviation , median , 25th and 75th percentile and coefficient of variation [ cv ] ) was calculated for each parameter . statistical analysis was performed using spss advanced statistica 11.0 software ( spss inc , chicago , illinois , usa ) and r open source software . dice similarity index ( dsi ) , jaccard index , mean distance toagreement andhausdorff distance dice similarity index ( dsi ) , jaccard index , mean distance to agreement and hausdorff distance were computed to compare target volume of participating centers in respect of reference center . dsi is expression of contours overlap . 
it was used as a statistical validation metric to evaluate the spatial overlap accuracy of the different delineations of ctvs [ 2325 ] and compared with the contouring of the reference contour considered as the benchmark . given two observers contouring the volumes a and b , dsi is defined as : dsi = 2|a b| |a| + |b| the value of a dsi is a scalar coefficient ranging from 0 to 1 , with 0 indicating no spatial overlap between two sets of binary segmentation results and 1 complete overlap . in addition to dsi , a closely related similarity metric called jaccard index was also calculated [ 26 , 27 ]  . the jaccard index measures similarity between finite sample sets and is defined as the size of the intersection divided by the size of the union of the sample sets : j ( a , b ) = |a b| |a b| |a b| ( |a| + |b| |a b| ) 2d and d = 2j ( if a and b are both empty , we define j ( a , b ) = 1 ) .0 j ( a , b ) 1 . 
mda is a geometrical parameter that measures the per voxel shortest distance from the surface of one structure to another , ideally when two structures overlap the mda results in 0mm [ 28 , 29 ]  . the hausdorff distance is a shape comparison method based on a distance measure of the edge maps of two objects . 
diagnostic and therapeutic approach for this disease is well codified , even if some controversies exist [ 35 , 36 ]  . in the context of treatment management , surgery represents the first therapeutic step , while radiotherapy is reserved in case of macroscopic tumor residual , pn > 1 , extra - capsular extension ( ece ) , neck violation or in patient not amenable to surgery . 
the center of reference is represented in white in the intermediate dose volume ; node stations at low risk of microscopic disease should be included in the low dose volume [ 17 , 3741 ]  . 
it seems easy , but discrepancies can affect the putative primary tumor site definition , the inclusion or not of the oral cavity , the extension of the pharynx to be irradiated [ 38 ] , such as neck irradiation extension ( i.e. , bilateral vs unilateral neck , extensive irradiation )  . in this scenario , inter - observer variability must be further considered . 
target variability delineation is a well - known source of errors in radiotherapy that has been well investigated in several tumors sites but in hn district , particularly in the setting of neck nodes metastases of occult primary . the present airo head and neck group study aim was to assess current national practice of h&n contouring with regard to a case of neck lymph node metastases from unknown primary , evaluating inter - observer variability of target volume definition in a setting of primary radiotherapy . 1 3 688 la radiologia medica ( 2019 ) 124 : 682692 fig . 
considering the uncertainty regarding the occult primary management as well as the anatomical complexity of head and neck district , a dsi > 0.60 could be considered acceptable , and in this study , a dsi near 0.60 was obtained in five ctvs hd and three ctvs ld [ 24 , 46 ]  . to the best of our knowledge , this is the first experience evaluating dsi values for the inter - observer variability in delineation of h&n district in relation to nodes metastases from occult primary rt . although dsi value is often applied in studies of interobserver variability , it could not be fully representative of the variability between two volumes . 
 these parameters contributed to define spatial differences of ctvs and confirmed variability shown by dsi . in the hpv era , the viral infection represents an additional factor to consider prescribing radiotherapy volumes in nodes metastases from occult primary and it could contribute to increase inter - observer variability . 
this translates into the qualitative analyses of our study ; in fact , when it was requested to indicate any ctvs 1 3 690 la radiologia medica ( 2019 ) 124 : 682692 changes taking into account hpv status , 59% of participating ros suggested a de - intensification of the prescription . conclusion in this study , a notable heterogeneity of global radiotherapy management in nodes metastases from occult primary was detected . 
four patients presented a peak systolic velocity ( psv ) between 130 and 150cm / s , six a psv between 150 and 180cm / s , and three a psv > 180cm / s . 
further studies with longer - term outcome are necessary to confirm our results . keywords carotid artery stent in - stent restenosis dual - layer stent introduction carotid endarterectomy ( cea ) is the gold standard for treating symptomatic carotid stenosis [ 1 ]  . 
although cas is no more effective than cea in preventing subsequent stroke , [ 2 ] , its less invasiveness , decreased patient discomfort and * gianpaolo carrafiello gcarraf@gmail.com 1 diagnostic andinterventional radiology department , asst santi paolo e carlo , san paolo hospital , university ofmilan , via a di rudin 8 , 20142milan , italy 2 vascular surgery unit , surgical sciences department , asst santi paolo e carlo , san paolo hospital , university ofmilan , milan , italy 3 department ofradiology , cto hospital , azienda dei colli , naples , italy shorter hospitalization make it a good alternative in selected patients . in the last years , cases with cas have been increasing , while those with cea have been decreasing [ 3 ]  . two concerns are related to cas : the intraand periprocedural risk of vascular events and the risk of in - stent restenosis ( isr ) during follow - up [ 3 ]  . 
the use of embolic protection devices limited the risk of periprocedural stroke to 6% , which is comparable to that in patients with cea [ 4 ]  . new dual - layer stents were designed with the aim of increasing the plaque coverage and decreasing the risk of dislodging through the stent strut [ 5 , 6 ]  . 
 [ 6 ] showed good safety and efficacy of duallayer stent in the treatment of carotid stenosis , with a low vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 704709 table 1 characteristics of patients and devices used during carotid stenting with roadsaver stents incidence of delayed embolic events and new ipsilateral ischemic brain lesions . the prevalence of plaque prolapse after cas , as assessed by oct ( optical coherence tomography ) , has been estimated between 29% for closed - cell design and 69% for open - cell design [ 7 ]  . in patients with lipid - rich plaques , a higher incidence of in - stent restenosis is registered . 
plaque prolapse , as assessed by oct , is relatively low with this novel device , as revealed in a multicenter italian study [ 5 ]  . the present study is a retrospective single - center study . 
 our aim was to evaluate the incidence of in - stent restenosis at 12 - month follow - up , in patients treated with new duallayer roadsaver stent . materials andmethods we selected all patients who underwent cas and received a roadsaver ( terumo corp . , tokyo , japan ) stent between february 2017 and july 2018 ; in a total of 21 patients , 13 ( 8 men and 5 women , mean age 75.8years old ; range 6584years old ) presented a follow - up of 12months ( table1 )  . principal inclusion criteria were age > 18years and documented carotid artery stenosis . 
symptomatic patients had to have a stenosis 50% evaluated by duplex ultrasound ( dus ) according to the nascet criteria [ 8 ] ; for asymptomatic patients , the stenosis had to be 70% and suitable for treatment according to the vascular and neurological specialists . principal exclusion criteria were carotid obstruction , previous stenting at the same site , acute stroke within the last 30days , myocardial infarction within 72h and intracranial hemorrhage in the previous 12months . the clinical evaluation included a neurological examination performed by an independent neurologist using the national institute of health stroke scale ( nihss ) [ 9 ]  . plaque morphological characteristics were determined by dus and defined as echolucent ( lipidic plaque ) , echogenic ( fibrotic plaque ) and heterogeneous texture ( heterogeneous plaque )  . carotid stenosis was revealed by dus and multidetector ct ( mdct ) scan . 
the degree of stenosis determined at grayscale and dus , considering internal carotid artery ( ica ) peak systolic velocity ( psv ) , should be stratified into the categories of normal ( no stenosis ) , < 50% stenosis ( psv < 130 cm / s ) , 5069% stenosis ( 130 < psv < 150 cm / s ) , 7079% severe stenosis ( 150 < psv < 180cm / s ) , 80% near occlusion to total occlusion ( psv > 180cm / s ) [ 10 ]  . 
 angiography revealed the extension and the morphology of the plaque . 1 3 706 la radiologia medica ( 2019 ) 124 : 704709 all patients have been evaluated by a team including an expert on stroke as suggested by the iccs - spread joint committee [ 11 ] ; in particular on the basis of their risk factors and / or comorbidities , asymptomatic patients were considered susceptible to cas . all patients had at least one coexisting condition on specific anatomic and comorbid clinical criteria that potentially increased the risk posed by cea , according to sapphire criteria [ 12 ]  . 
neurological complications were quantified by the national institutes of health stroke scale ( nihss ) , and recovery was evaluated by median rankin scale ( mrs )  . characteristics of patients and their lesions are summarized in table1 . the study was conformed to the declaration of helsinki , and patients gave written informed consent for the procedure . procedure each patient was on dual antiplatelet therapy ( aspirin 100mg and clopidogrel 75mg daily for at least 3days before the procedure or loading doses of 300mg of aspirin and clopidogrel the day before the procedure )  . 
moreover , in those patients a mdct was performed to confirm findings of dus . results technical success was achieved in all cases with a residual stenosis < 30% at postprocedural angiographic examination . 
in both patients ceus and mdct denied the presence of significant stenosis ( fig.2ah ) ( table1 )  . discussion restenosis has been one of the most important remote complications of both cas and cea , although more frequently associated with the cas [ 14 ]  . 
 based on dus criterions , crest reported a cumulative isr incidence of 6.0% in 2years after cas [ 16 ]  . three forms of isr were described [ 15 ]  . 
the commonest is in - stent restenosis , which probably is due to neointimal hyperplasia , caused by a symmetrical or asymmetrical 1 3 la radiologia medica ( 2019 ) 124 : 704709 fig . 
1 ct image reveals ica stenosis and its morphology ( a ) ; angiogram performed before stenting ( b ) ; angiogram performed at the end of the procedure with a minimal residual stenosis of ica ( c ) narrowing of the lumen within the stent after an initial good result . 
the end - of - stent restenosis is similar to the recurrent stenosis after carotid patch thromboendarterectomy , which has been ascribed to local factors or technical errors . the less frequent type is tandem restenosis that may represent the most benign type regarding treatment durability [ 15 ]  . several factors seem to be implicated with the risk of isr : female gender and advanced age and concomitant conditions like diabetes mellitus , hypertension and dislipidemia may be more frequently associated with isr ; moreover , patients who received cas for stenosis related to radiotherapy or post - cea and the use of multiple stents , the use of open - cell stents and patients with post - cas residual stenosis are more prone to isr [ 3 , 6 , 1720 ]  . technological advances in endoluminal equipment made more frequent the indication for cas even in patients not strictly at risk of cea [ 21 ]  . the increase in indications for cas will require not only demonstration of feasibility and immediate clinical success but also durability in long - term studies . in a published single - center experience with 1000 carotid wallstent implantations , restenosis occurred in 3.2% ( 32 ) stented lesions ; among the retreated lesions , 1% [ 9 ] were those who had > 30% residual stenosis on the control angiogram ; all had calcified plaque [ 17 ]  . other authors analyzed the clinical impact and predictors of carotid artery isr [ 19 ] ; during the long - term followup period , the combined rate of ipsilateral stroke and death was 33.3% in the group with an isr > 70% ( 2 strokes and 2 deaths )  . 
they did not indicate the stent used , but the clinical impact of isr is important and they invited to a closer surveillance in the high - risk subgroup . double - layer stents are one of the recently introduced new stent designs to treat carotid stenoses as well . 
to date , we have literature data about feasibility , clinical success and safety about the use of roadsaver double - layer stent [ 6 , 2224 ]  . no data are published about the incidence of isr using this new generation of stent ; unfortunately , the too small population represents the biggest weakness of our study . 
no meaningful statistical analysis was possible to obtafirst of all , our preliminary results need confirmation with more patients . in one patient with suspected residual intra - stent stenosis at the final angiogram , a minimal intimal hyperplasia was revealed at 6 - month follow - up , not increased at 12 - month examinations . 
the only first large series published [ 24 ] revealed a restenosis rate which does not seem different 1 3 708 la radiologia medica ( 2019 ) 124 : 704709 fig . 
2 ct image reveals ica stenosis and its morphology ( a ) ; angiogram performed before stenting ( b ) ; angiogram performed at the end of the procedure with a minimal residual stenosis of ica ( c ) ; b - mode us image ( d ) and dus image ( e ) at 12 - month follow - up : the latter shows a minimal intra - stent intimal hyperplasia ( white arrow ) ; psv of about 80cm / s reveals a nonsignificant intra - stent stenosis ( f ) ; ct scan confirms minimal nonsignificant intra - stent intimal hyperplasia ( g , h ) from other stents , although randomized studies are still lacking . 
the same authors hypothesized a novel pattern of restenosis , with plaque growth between the two layers , probably associated with a lower embolic risk . our data should be considered as supportive to those just published . 
a second objective was to assess whether there were other histopathologic features that could affect mean adc value . methods in this 4 - year retrospective study were included 125 patients who underwent radical or modified mastectomy for monofocal bc . 
adc value was shown to be significantly related to tils level ( p < 0.0001 ) and cancer histotype ( p = 0.0006 ) , with a lower mean adc value correlated to absentlow til level and ductal histotype . conclusion bcs with absentlow til showed a statistically significant lower mean adc value than those with mediumhigh til . 
the latter is the treatment of choice for patients with locally advanced breast cancer , and those who show pathologic complete response ( pcr ) to nac may experience prolonged disease - free survival . 
 [ 16 ] have shown that higher til level is associated with her2 + dcis . in this study , we hypothesized that adc value could predict til level , which could help to identify bcs with a better response to nac and patients with prolonged disease - free survival . 
a second objective was to assess whether there were other histopathologic features that could affect mean adc value . materials andmethods study population the ethics committee of our institution approved this retrospective study . 
exclusion criteria were : preoperative breast mri in another institution ( n = 5 ) ; mri performed without dwi sequence ( n = 3 ) ; and history of neoadjuvant treatment for bc ( n = 28 )  . 
according to these criteria , the final cohort consisted of 125 patients . mri technique all mri examinations were performed with 1.5 - t machine ( achieva , philips healthcare , andover , ma ) and a 7 - channel dedicated breast coil ( sense breast 7 ch ) with patients in prone position . 
in order to assess adc value , a region of interest ( roi ) was manually drawn in each slice in which the lesion was detectable on the b = 800smm 2 dw images . 
only mean adc value , which corresponds to the area - weighted average of the adc values found within each lesion slice , was used in the analysis . pathologic analysis all patients underwent radical or modified unilateral mastectomy for monofocal bc . 
the surgical piece was fixed in formalin and included in paraffthin sections were evaluated by the same pathologist with more than 10 - year experience in breast pathology , and the presence of til was assessed . 
 [ 15 ] , based on til level , we divided bcs into two groups : tumors with til level 10% were classified as absentlow til and those with til level > 10% were classified as mediumhigh til . 
 tumor size , histotype , estrogen and progesterone hormone receptor expression ( er , pr ) , human epidermal growth factor receptor 2 ( her2 ) expression , proliferation defined by the ki - 67 labeling index , histologic subtype , grade and tumor cellularity were also recorded . 
her2 positivity was defined as 3 + score by ihc in > 30% of invasive 1 3 la radiologia medica ( 2019 ) 124 : 581587 tumor cells using the hercept test ( dako , glostrup , denmark )  . 
equivocal cases at ihc ( 2 + score or 3 + in 30% of invasive tumor cells ) were subjected to fluorescence insitu hybridization ( fish ) analysis [ 17 ]  . 
tumor cellularity was defined as percentages in 10% increments and was calculated from five arbitrarily selected high - power fields in each specimen using a computer prograaccording to tumor cellularity , we divided bcs into two groups : tumors with low cellularity ( < 60% ) and tumors with high cellularity ( 60% )  . 
adc threshold was chosen by the area under roc curve ( auc ) and youden index . in order to assess histotype , grade and ki - 67 expression differences between absentlow til group and mediumhigh til group , mannwhitney u test was used . 
moreover , tils were shown to be the most important factor on which mean adc value depends . within the tumor , there are different cellular and stromal components , on which the average adc value of the neoplastic lesion may depend . 
moreover , adc is also dependent on histotype , and this finding is probably attributable to the lower cellular density of invasive lobular cancer compared to ductal ones . dwi is an mri technique that does not require contrast medium , with a short acquisition time and high specificity in bc detection [ 2022 ]  . 
1 a 34 - year - old woman with a 15 - mm invasive ductal cancer in her left breast with absentlow til that appears hyperintense on dwis obtained at b = 0 ( a ) and b = 800 ( b ) and hypointense on adc map ( 0.891 * 103mm2s1 ) ( c ) including histotype and proliferative index [ 8 , 9 , 23 ]  . 
 [ 24 ] demonstrated that adc value was significantly higher in er - negative than in er - positive cancer , but we did not find this . to our knowledge , there are no previously published works in scientific literature comparable to this one . 
 [ 25 ] obtained a non - statistically significant difference in mean adc value between bc with low and high til levels , but they only considered triple - negative bcs and used a til threshold value of 50% to distinguish the two groups . 
 [ 26 ] reported that only tumor cellularity and ki - 67 were independently associated with mean adc value , and not tils . in the present study , the choice to stratify bcs into two til groups , as reported by asamo etal . 
 [ 15 ] , was performed because most of the previous studies that evaluated til as a predictor of nac response used 10% as a cutoff value [ 11 ]  . 
however , til level assessment , to date , presents a poor intra - observer reproducibility , and it is a subject of debate in the current scientific literature [ 2729 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 581587 fig . 
2 a 46 - year - old woman with a 12 - mm invasive ductal cancer in her right breast with mediumhigh til that appears hyperintense on dwis obtained at b = 0 ( a ) and b = 800 ( b ) and hypointense on adc map ( 1.023 * 103mm2s1 ) ( c ) fig . 
3 a 39 - year - old woman with a 18 - mm invasive lobular cancer in her right breast with absentlow til that appears faintly hyperintense on dwis obtained at b = 0 ( a ) and b = 800 ( b ) and hypointense on adc map ( 1.208 * 103mm2s1 ) ( c ) fig . 
4 a 45 - year - old woman with a 20 - mm invasive lobular cancer in her left breast with mediumhigh til that appears faintly hyperintense on dwis obtained at b = 0 ( a ) and b = 800 ( b ) and hypointense on adc map ( 1.354 * 103mm2s1 ) ( c ) til level in bc has recently taken an important oncological role [ 30 , 31 ]  . 
 in some studies , it showed a positive predictive value for response to nac , and patients that show a pcr to nac may experience prolonged disease - free survival . 
we review the various surgical techniques used in pe , discuss optimal ct protocols for postsurgical evaluation and describe cross - sectional imaging appearances of normal postoperative anatomic changes as well as early and late complications . 
gemelli 8 , 00168rome , italy introduction pelvic exenteration ( pe ) is a radical en bloc resection of multiple endoand exopelvic organs affected by cancer , followed by reconstructive surgical procedures to restore compromised urinary , intestinal and sexual functions [ 1 ]  . 
early and late postoperative complications after pe in patients treated for advanced , persistent or recurrent gynecologic cancers are vol . : ( 0123456789 ) 1 3 694 la radiologia medica ( 2019 ) 124 : 693703 the focus of this review . 
we describe the types of pe and the expected ct imaging findings after surgery , showing the ct appearances of most common complications including bleeding , wound infection , urinary injury ( anastomotic leak , stricture , fistula ) and gastrointestinal injury ( anastomotic leak , bowel occlusion , fistula )  . 
lastly , the imaging pattern of local tumor recurrence after pe is discussed . surgical techniques different types of pe can be performed depending on the tumor location and extent to other pelvic structures . 
supralevatoric pe is a resection above levator ani muscle , with spare of anal sphincter and urogenital diaphragtranslevatoric pe is an excision below pelvic floor muscles , with partial or complete removal of levator ani muscle , anal sphincter and urogenital diaphragmore extended exenteration is required when tumor affects the pelvic sidewall [ 8 ]  . 
the laterally extended endopelvic resection ( leer ) includes resection of all pelvic viscera with any of the endopelvic parietal structures , such as paravisceral fat pad , internal iliac vessels , obturator internus and levator ani muscles [ 9 ]  . 
extended pelvic resection ( epr ) is characterized by an extensive pelvic excision including pelvic sidewall muscles , bones and major neural and / or vascular structures as common and / or external iliac vessels [ 10 ]  . 
b sagittal ct scan , acquired 7days after total pe , shows the absence of bladder and the presence of bilateral ureteral stent ( curved arrow ) due to urinary diversion . 
 b sagittal ct scan illustrates the pelvic cavity after anterior pe with the absence of lower urinary tract organs ( urinary bladder and urethra ) 1 3 la radiologia medica ( 2019 ) 124 : 693703 fig . 
 the imaging protocol usually includes abdomen and pelvis ct scan ( with or without chest ) before and after intravenous ( iv ) administration of contrast material [ 13 ]  . 
enhanced arterial and portal phases ( 3040s and 7080s delayed acquisition after injection of contrast media ) are mandatory to detect active bleeding , in case of suspected hemorrhage [ 14 ]  . 
after scanning , the radiologist can use post - processing techniques as multiplanar reformatting ( mpr ) , maximum intensity projection ( mip ) and volume rendering ( vr )  . 
therefore , the familiarity with the type of pe performed helps the radiologists to interpret imaging and differentiate between normal findings and postsurgical complications . after anterior pe , ct allows recognition of the absence of bladder / urethra and the presence of a urinary reconstruction , also known as urinary diversion . 
mpr and mip postprocessed images may be useful to accurately detect ureters and the integrity of ureteroenteric anastomosis [ 17 ]  . when vaginectomy is performed during anterior pe , the reconstruction of functioning vagina is indicated . 
coronal reformatted mip image , from a ct scan acquired at excretory phase ( 15 min delayed after contrast media injection ) , shows the ileal conduit ( white arrow ) located in the right lower abdomen and the ureters anastomosed at its proximal end . 
 the black arrow indicates the ureteroenteric anastomosis such as the absence of rectus abdominis muscle in its normal site and the evidence of vram flap vascular pedicle represented by the deep inferior epigastric artery [ 22 ]  . postoperative pelvic imaging afterposterior pe posterior pe consists of two main surgery procedures : translevatoric pe with creation of end colostomy and supralevatoric pe with colorectal / coloanal anastomosis . during translevatoric pe , rectum and anus are resected , and a permanent colostomy is usually created in the left lower abdominal quadrant . 
combined positron emission tomography ( pet ) / ct might be considered a complementary method if tumor 1 3 la radiologia medica ( 2019 ) 124 : 693703 recurrence is suspected , because of its higher sensitivity and specificity compared to ct [ 25 ]  . the linea alba and the sacrum [ 23 ]  . 
ct images show the bowel anastomosis line evidenced by surgical clips and the enlargement of the presacral space with anterior displacement of the rectua marked ( 35cm ) dislocation of rectum from the sacrum associated with persistent ( > 6months ) fluid or air in the presacral space is suspicious for anastomotic leak , fistula or tumor recurrence [ 24 , 26 ]  . pelvic soft tissue reconstruction after posterior pe is based on the use of autologous vascularized pedicle flaps . 
due to its angiogenetic property , omental flap helps the wound healing and reduces postsurgical complications , like abscesses and adhesions between pelvic floor and organs [ 22 ]  . 
axial enhanced ct image shows the omental pedicle flap with fat density ( star ) in the presacral space and the small bowel dislocated in the anterior compartment of the pelvic cavity postoperative pelvic imaging aftertotal pe total pe is a complete exenteration of pelvic organs that consists of both anterior and posterior pe . 
pelvic reconstruction is also required to restore sexual functioning and to provide an acceptable body image . postsurgical complications postoperative complications after pe can be classified as early ( < 30days ) and late ( > 30days ) according to the time interval from surgery [ 27 ]  . 
common postoperative complications include hemorrhage , pelvic abscess , wound infection , urinary injury ( leakage , obstruction , fistula ) and gastrointestinal injury ( anastomotic leak , bowel occlusion , fistula )  . 
ct with the use of multiplanar reformatted images offers an accurate identification of complications by providing a support for the surgeon to decide the best treatment approach for each patient . general complications hemorrhage andhematoma hemorrhage is an intra - operative and early postoperative major complication with an incidence rate of 39.4% and a potential fatal prognosis if not diagnosed on time [ 29 ]  . 
bleeding commonly originates in the presacral plexus or in the internal table 2 type of pe and their most common related complications anterior pe posterior pe total pe hemorrhage infection / abscess wound dehiscence urinary tract injury gastrointestinal tract injury + pe pelvic exenteration + , low risk ; + + , high risk 1 3 698 la radiologia medica ( 2019 ) 124 : 693703 fig . 
bilateral deep thrombosis of external iliac veins ( arrowheads , c ) is also present iliac vein , or it can be locally confined to wound site [ 29 ]  . 
bleeding may also develop as pelvic hematoma , which typically shows higher density ( 7090 hu ) at unenhanced ct scan [ 13 ]  . infection andpelvic abscess infection remains one of the most common complications of surgical procedure in gynecology [ 30 ]  . 
the management is various , and if no surgical revision is required , ct - guided drainage in combination with antibiotics is the preferred treatment approach [ 30 ]  . wound infection anddehiscence about 214% of patients who underwent pe develop wound infection , most commonly involving the laparotomy site [ 27 ]  . 
sagittal enhanced ct scan shows a fluid collection containing a large amount of gas in the presacral space ( line arrow ) associated with a widening of the presacral space ( > 35 cm )  . 
urography ct is useful to study enterourinary fistula ( fig.9 ) , while ct with rectal administration of water - soluble iodinate contrast is indicated in case of low enterogenital fistula [ 16 , 17 ]  . 
as recurrent tumor may cause fistulas , accurate evaluation of any soft tissue mass or other signs of malignancy should always be done . complications afteranterior pe urinary leak urinary leak from a newly formed conduit is a major , early postoperative complication after anterior pe . 
the urine leak rate in the pe surgery is reported in excess of 15% , while the urine leak rate after conduit formation for a primary urological malignancy is < 5% [ 3537 ]  . 
the diagnosis is related to the presence of creatinine - rich fluid from abdominal drains or wound sites , or evidence of sites of iodinated urine extravasation on imaging [ 35 ]  . 
depending on the site , there are two types of leak : ( a ) anastomotic leak , when urine extravasation originates from ureteroenteric anastomosis , and ( b ) conduit leak , when urine extravasation originates anywhere else along the conduit . 
urography ct may show iodinated urine outside the injured ureteral / conduit segment and the shedding into the retroperitoneum or less commonly into 1 3 700 la radiologia medica ( 2019 ) 124 : 693703 fig . 
9 malignant enterourinary fistula between the ileal conduit and the cecum in a 52 - year - old woman who underwent total pe for recurrence of cervical cancer ( 10 months earlier )  . 
a coronal and b axial images , from a ct scan acquired after administration of water - soluble iodinated contrast through the ileal stoma , show the opacification of the cecum and the presence of a fistulous tract ( line arrows ) that connects the ileal conduit ( dashed line arrows ) to the cecu the presence of solid enhancing masses ( arrowhead , b ) in the right side of the pelvis , adjacent to the ileal conduit , represents recurrence of tumor the peritoneal cavity . 
the management is conservative if the urine leak is small and asymptomatic ; otherwise , it needs surgical revision or radiological intervention ( percutaneous nephrostomies or percutaneous drain insertion ) [ 37 ]  . urinoma urinoma is a urine collection located commonly in perirenal space or in the retroperitoneum along psoas muscle . 
ct scan , during excretory phase , shows the progressive increase of attenuation inside the urinoma due to iodinated urine entering into the collection [ 15 ]  . urinary stricture urinary stricture generally involves the ureteroenteric anastomosis and occurs lately within 12 years after surgery . 
ureteral strictures are classified as benign , in case of ureteral fibrosis secondary to ischemic lesion or improperly fashioned anastomosis , and malignant when tumor recurrence grows close to ureteroenteric anastomosis . 
b axial excretory phase ct image , acquired 10min later , shows an influx of contrast material into the collection ( arrow ) 1 3 la radiologia medica ( 2019 ) 124 : 693703 fig . 
c coronal excretory phase ct scan confirms the soft tissue lesion ( arrow ) located close to the right ureteroenteric anastomosis associated with dilation of the urinary tract above on the right side ( black star ) complications afterposterior pe bowel anastomotic leak bowel anastomotic leak is a major , early complication after posterior pe associated with a high morbidity . 
the extravasation of rectal contrast medium is the most predictable sign for an anastomotic leak [ 39 , 40 ]  . bowel occlusion bowel occlusion is a late complication that occurs in 4.415.4% of cases after posterior pe and involves more frequently the small bowel [ 27 ]  . 
closed - loop obstruction is a type of small bowel occlusion where a bowel segment is obstructed at two adjacent points along its course ( fig.12 ) ; when the closed - loop rotates on its vascular axis , it forms small intestinal volvulus . 
radiologist should exclude bowel strangulation , perforation and peritonitis that are potential fatal sequelae of bowel occlusion . adynamic ileus is a common early cause of functional bowel occlusion due to the paralysis of intestinal motility in the immediate postsurgical timing . 
generally , this condition does not last more than 48h after surgery and can be conservatively managed . complications aftertotal pe total pe is a more radical exenteration surgery than partial pe with higher rate of postoperative complications . 
urinary and gastrointestinal tract complications are both documented after this surgical operation ( table2 )  . 1 3 702 la radiologia medica ( 2019 ) 124 : 693703 conclusion pe remains the most challenging surgical operation in patients with advanced , persistent or recurrent gynecological cancers . 
12 small bowel obstruction due to adhesions in a 48 - year - old woman who underwent posterior pe for recurrence of cervical cancer ( 4 months earlier )  . 
an inter - observer reliability analysis was performed . results the prevalence of emissary veins in mri was found in the right mastoid emissary vein ( mev ) 82.7% and left mev 81.4%. 
there was a statistically significant difference between the left mev and oev and transverse sinus anatomic variations . conclusion mr imaging is a noninvasive and irradiating imaging method for detecting posterior fossa major emissary veins , and we recommend using mr imaging for preoperative evaluation of posterior fossa major emissary veins and related dural venous sinuses . keywords magnetic resonance cranial fossa cerebral veins mastoid introduction emissary veins are venous structures without valves and are located between the venous sinuses and the extracranial venous circulation . 
the blood flow in the emissary veins is usually from external * pinar gulmez cakmak pinarcakmak20@gmail.com 1 department ofradiology , faculty ofmedicine , pamukkale university , kinikli kampusu , 20100denizli , turkey to internal . 
in some conditions , such as intracranial vascular malformations or internal jugular venous hypoplasia of craniosynostosis , venous drainage of the brain is provided by emissary veins [ 5 ]  . 
anatomic variations of the major venous sinuses appear as hypoplasia or aplasia in cross - sectional imaging [ 69 ]  . preoperative detection of emissary veins , particularly in temporal bone surgery , within mastoid bone or in close proximity , may prevent complications such as bleeding or venous thrombosis . 
digital subtraction angiography , computerized tomography angiography and magnetic resonance venography ( mrv ) are used in the radiological evaluation of the brain venous systemrv can be achieved by using either non - enhanced ( two - dimensional time of flight mrv , phase contrast mrv ) or contrast - enhanced vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 620627 ( gadolinium enhanced 3 - dimensional mrv , auto - triggered 3d gd - enhanced mrv ) methods . 
contrast - enhanced mrv has the advantage of showing the detail of intracranial venous anatomy and has relatively faster acquisition time compared to non - enhanced mrv [ 1113 ]  . 
there are studies about transverse sinus and sigmoid sinus anatomic variations in the literature [ 79 ]  . we found no other radiological study investigating the relationship between the presence of emissary veins and the anatomic variations of venous sinuses . 
the aim of this study was to find the prevalence of emissary veins in the posterior cranial fossa and to compare the presence of these emissary veins with the anatomic variations of the dural venous sinuses detected in mr venography . materials andmethods study population the study protocol was approved by the local ethics committee of our university . 
posterior fossa emissary veins and dural venous sinus anatomic variations in 247 patients who underwent mr venography ( mrv ) examinations were evaluated retrospectively between january 2015 and september 2017 . 
1 axial mr images show that mastoid emissary vein ( mev ) diameter measurements ( close to the medial wall of the cranial bone ) mri was performed using two 1.5t superconducting magnets ( ge signa excite hd ; ge medical systems , usa , ingenia ; philips medical systems , best , the netherlands ) with an 8 - channel neurovascular coil . 
subsequently , the statistical analysis presence of the emissary veins was compared with the dural venous sinus anatomic variations . data analysis was performed on a personal computer using statistical software ( spss 16 for windows , chicago , il )  . 
the absence of left mev ( p = 0.007 for r1 , p = 0.011 for r2 ) and the presence of oev ( p = 0.005 for r1 , p = 0.004 for r2 ) and right pcev ( p = 0.038 for r1 , p = 0.024 for r2 ) were found to be statistically significant in women for both radiologists . 
no correlation was found between the other variations of transverse and sigmoid sinus with gender . there was not any statistically significant difference between transverse and sigmoid venous sinus anatomic variations and the presence of posterior condylar emissary veins . 
however , a statistically significant difference was found between the anatomic variations of the left mev and oev and transverse sinus ( table4 )  . discussion various sizes of emissary vein have been described in previous studies [ 1420 ]  . 
 other studies investigating pcev prevalence have been performed with smaller numbers of patients or cadavers according to our study , and different prevalence values have been reported [ 24 , 14 , 18 ]  . 
in our study , the largest mastoid emissary vein diameter was 4.9mm and posterior condylar emissary vein diameter was 6.0mm. the comparison of the frequency of mev , pcev and oev in the present study and the previous studies is presented in table5 . there are some differences in the prevalence of mev among the studies performed in the literature using cadaver and imaging modalities . 
 [ 19 ] reported that the prevalence of occipital foramen ( of ) in over 200 specimens was 7% on the right and 4% on the lein the literature , there is no imaging study about the prevalence of oev . 
 [ 23 ] reported that emissary veins serve to cool the venous blood table 5 the comparison of the frequency of the emissary veins study type mev prevalence ( % ) pcev prevalence ( % ) oev prevalence ( % ) ruiz etal . 
 bleeding is common , and tactics for achieving hemostasis of the mev include bipolar coagulation , vessel ligation , and packing the vein with hemostatic material [ 10 ]  . 
a case of dural arteriovenous malformation embolized via enlarged mev has been reported [ 29 ]  . in the literature , there are ct and cadaver studies in which the emissary canal is evaluated [ 3 , 1416 , 30 ]  . 
in addition , the ultrashort tr and te enable has extremely short acquisition times ( shorter than fse ) , and the images can be post - processed using mip , volume rendering or 3d techniques . 
mr venography is frequently used in dural venous sinus imaging , except for patients with contraindications to mr ( e.g. , pacemakers , cochlear implants , non - mr compatible cerebral aneurysm clips )  . 
magnetic resonance venography have made it possible to visualize the dural sinuses and cerebral veins without the use of invasive procedures or ionizing radiation [ 1113 ]  . dural venous sinuses are the major blood drainage system in the craniuthe sinuses in the superior group are superior sagittal ( sss ) , inferior sagittal ( iss ) , straight ( ss ) , occipital ( os ) , transverse ( ts ) and sigmoid sinuses . 
reported that 21 ( 20% ) patients had aplasia of the left transverse sinus , 41 ( 39% ) patients hypoplasia of the left transverse sinus , 33 ( 31% ) patients symmetric sinuses , 6 ( 6% ) patients hypoplasia of the right transverse sinus , and 4 ( 4% ) patients aplasia of the right transverse sinus [ 8 ]  . 
in our study , 119 ( 54.1% ) of the symmetric transverse sinus and 67 ( 30.4% ) of the left hypoplastic / aplastic transverse sinus , 165 ( 75% ) of the symmetric sigmoid sinuses and 35 ( 15.9% ) of the left hypoplastic sigmoid sinus were found . 
we did not find any significant difference between the rest of anatomic variations of the venous sinus and the gender . embryologically , emissary veins were identified from the third month of gestation and the development of the emissary veins has been reported to develop after transverse sinus ballooning [ 21 ]  . 
these findings in our study demonstrate a strong association between the presence of the emissary veins and 1 3 626 la radiologia medica ( 2019 ) 124 : 620627 the dural venous sinus variations starting with ballooning of the sinuses in embryological development . our study has several limitations such as being retrospective . 
in our study , brain mr and mrv were noninvasive and irradiating imaging methods and no comparison was made with other imaging modalities ( ct angiography , digital subtraction angiography )  . 
finally , the number of patients is limited and to increase the statistical significance of the relationship between dural venous sinus variations and the presence of emissary veins could be done with increasing the number of patients . conclusion mr imaging with a balanced gre sequence is a successful method for detecting posterior fossa major emissary veins . 
 the prevalence of emissary veins in mri was found at right mev to be 82.7% , left mev 81.4% , right pcev 77.3% , left pcev 75% and oev 28.6%. 
from a radiological perspective , this correlation proves that the posterior fossa emissary veins were formed by a ballooning from the transverse sinus . authors contributions pgc was involved in protocol development ; data collection and management ; data analysis ; and manuscript writing and editing . 
fracture lines and comminution zones were identified by reduced three - dimensional computed tomography reconstructions and then graphically superimposed onto a standard template to create two - dimensional fracture maps , followed by the conversion into heating maps . 
based on qualitative descriptive fracture mapping analyses , the patterns of intra - articular distal radius fractures were determined . results it was observed that the highest fracture line intensity was located as an inverted t shape zone in the dorsal aspect of the joint with high incidence of fractures and the prominently intense color in heat mapping . 
in this study , a new surgical approach was attempted , but due to the lack of evidence - based evidence , long - term postoperative complications and hand function should be further evaluated . conclusion this study redefines a new method for the classification of intra - articular fractures of the distal radius , which allows doctors to have a clearer understanding of the characteristics of distal radius fractures . 
 although the surgical management for drfs is variable , the principle is to restore the bone anatomic structures and to recover the function of the wrist joint after rigid internal fixation as soon as possible . 
recently , with the development of volar locking palmar plates , which have been demonstrated to have a low - profile design , a capacity of neutralizing the load across the fracture sites and the non - requirement of vol . : ( 0123456789 ) 1 3 614 la radiologia medica ( 2019 ) 124 : 613619 good bone quality , volar locking plate fixation has been widely used in the treatment of distal radius intra - articular fractures . 
in particular , due to the unexposed joint capsule through the volar locking approach , the location and dependence of internal fixation for fractures of the distal radius articular surface is principally relied on x - ray examinations and surgeons experience , requiring precise and effective methods . 
therefore , it has become a strong interest for surgeons to know how to achieve the articular surface fracture fixation after restoring the articular surface and whether to add other screws when volar locking plate distal screws are used to fix important fracture fragments , especially for the elderly patients with osteoporosis [ 2 ]  . 
 recently wrist arthroscopy may be an effective method to observe the fracture line of distal fractures but not popular because of technique and expense [ 3 ]  . the current study aimed to explore the distribution characteristics of the fracture lines in drfs by building fracture maps reconstructed using axial computed tomography ( ct ) scan images of patients with intra - articular fractures of distal radius . 
as fracture mapping can contribute to the better understanding and accurate evaluation on the fracture patterns of drfs ( e.g. , location and frequency of the injury of the articular surface ) , through fracture mapping , surgeons hence could further anticipate the fracture patterns through superimposing fracture lines , zones of comminution and articular involvement , which provide novel mechanistic insights and develop therapeutic strategies of drfs [ 4 ]  . materials andmethods patients consecutive image sampling was conducted for the patients with distal radial fractures at department of orthopedics of tongji hospital ( tongji university , shanghai , china ) between july 2014 and january 2016 by using the international classification of diseases , ninth revision , clinical modification ( icd - 9 - cm ) codes . 
in total , 40 of 265 patients with distal radial fractures were screened for entry into the current study . fracture mapping three - dimensional computed tomography ( q3dct ) analyses were performed to visualize the distributions and locations of fracture lines . 
 the selected ct images were then reloaded into software mimics 17.0 ( mimics , boston , ma ) , and bone structures were marked manually in axial , sagittal and coronal planes to create 3d polygon mesh reconstructions . 
all the articular images were subsequently superimposed by software photoshop cc ( version 2015.5 ; adobe systems incorporated , san jose , ca ) to build a frequency diagram as determined by the density of fracture lines . heat mapping anddata analysis as a mean to obtain a more intuitive understanding of the 2d fracture mapping , the initial diagrams were also converted into fracture heat maps by using photoshop cc ( adobe systems incorporated )  . 
the heat maps were created based on the fracture lines and represented the relative frequency of fracture lines that have been graphically displayed as colors . the analysis of the fracture maps was descriptive . 
in the heat mapping , the distribution frequency of the fracture on the articular surface is distinguished by the change in appearance of the intensity . results there were 23 ( 57.5% ) female and 17 ( 42.5% ) male cases for intra - articular fractures of the distal radius eligible in the current study . 
according to the association for osteosynthesis / association for the study of internal fixation ( ao / asif ) fracture classification system , there were 3 cases ( 7.5% ) of type b1 , 2 cases ( 5% ) of 1 3 la radiologia medica ( 2019 ) 124 : 613619 fig . 
a free bone fragments marked with different colors ; b a 3d reconstructed model ; c a 3d image manually reset ; d a 3d image with the fracture lines drawn fig . 
a in the process of 3d reconstruction , the backbone of radius was in translucent mode and the position of the backbone was then adjusted to form the ellipse through overlapping the margin of the bony cortex . 
by adjusting the parameters in the diagram ( width and depth ) , the center of the ellipse was adjusted at the centroid of the articular surface ( i.e. , the intersection of dashed red lines ) to form a standard articular surface . 
b illustration of the articular view and some important anatomy landmarks such as flexor pollicis longus ( fpl ) , the dangerous zone ( fpl would be threatened in this zone during the volar plate implanting ) and the safe zone . 
on the volar aspect of the joint , the fracture lines were shown to be less distributed and dispersed , which are accompanied with the lower color intensity in heat mapping . 
as the functions of the wrist joint mostly depend on the integrity and axial direction of the distal radius , precise reconstruction of the articular surface and rigid fixation of main fracture fragments are the key to reduce the risk of traumatic osteoarthritis and achieve satisfactory function recovery . 
in this fixation technique , to be able to insert the distal locking screws into the proper locations and to the accurate depth is well known 1 3 616 la radiologia medica ( 2019 ) 124 : 613619 fig . 
b the intensity of the color represents the frequency of the fracture occurrence , and fracture line intensity is illustrated by heat mapping analyto be the foundation to achieve adequate fixed capacity and the compression of debris . 
however , the proper treatment of intra - articular fracture of distal radius requires great understanding of the fracture pattern and optimal preoperative planning for surgeons ; and thus , there is an urgent requirement of the surgeons in predictably defining the fracture patterns in the articular surface of distal radius before operation . 
although fracture mapping techniques have obtained the substantial advancements and have been widely used in clinical practice to further understand the injury patterns [ 5 ]  . in the current study , intra - articular distal radius fractures were mapped by 3d reconstruction of articular surface with the data transferred from preoperative ct examination , which is currently widely used in assessing the distal radius fractures [ 6 , 7 ]  . 
thus , articular surface details such as the ankle , fossa and protrusion of the articular surface were clearly displayed . in addition , by analyzing fracture line distribution , the location of the fragments could be inferred , and the area of the metaphyseal collapse ( effective bone loss ) companied with potential instability also could be estimated . 
two of the fracture lines traverse the articular surface and intersect . as the most common type , type is observed to be with more bone loss and less lunate and scaphoid fossa surface . 
a lunate fossa and scaphoid fossa : two independent stress distribution areas in the radial articular surface , which could form the radiocarpal joint with the lunar and scaphoid ; sigmoid notch : an important anatomical structure of the radius , which forms the distal radioulnar joint with ulnar head and serves as the pivot of forearm pronation and postpronation . 
b the keystone area : the intermediate column ( ic ) in the three - column biomechanical construction and the main conduction area of the energy load which is often used as a key point for screw placement 1 3 la radiologia medica ( 2019 ) 124 : 613619 fig . 
dorsal approach is thus recommended in surgery . in addition , there was also acceptable bone loss found in type , which could be treated by volar approach surgery , so that bone grafting may not be performed intraoperatively . 
 the fracture lines at the lunate fossa or scaphoid fossa were characterized to be intensively distributed at the edge of the fossa and directly through the center of the fossa sparsely . 
 previous studies have shown that the reconstruction of the articular surface of the lunate fossa and scaphoid fossa is critical to facilitate the recovery of the wrist function and to reduce postoperative complications [ 9 ]  . since type fractures involved sigmoid notch , aside from reconstruction of the distal radioulnar joint surface and exploring the damage of surrounding soft tissue ( tfcc ) , the volar approach cold also be achieved . 
as the triangular fibrocartilage complex ( tfcc ) was considered as the major ligamentous stabilizer of the distal radioulnar joint [ 10 ] , more attention should be paid for restoring the stability of tfcc , which is dependent on the distribution of the fracture lines at the sigmoid notch , during the fracture reduction and fixation . for type fractures , the focus of reduction is on the styloid process of the radius . 
these findings indicated that the keystone area is not an isolated articular surface of the distal radius but an important area with dense trabecular bone structure in the dorsal aspect of the distal radius , strongly supporting the rationality and safety of the keystone area screwing . 
apart from the keystone area , the radial styloid process was shown to be the area with the lowest fracture rate , which suggests it could be served as another screw inserting point . 
however , due to the lack of a precise intraoperative instrument to assess the positions ( orientation and depth ) of the screws , it still relies on the surgeons experience and skill level to reach the proper position and decrease iatrogenic complications ( e.g. , the extensor tendon problems ) in the clinic [ 11 , 12 ]  . by retrospectively analyzing the typical x - rays of each type before surgery , it was found that for the and type fractures , the preoperative anteroposterior x - ray has 1 3 618 la radiologia medica ( 2019 ) 124 : 613619 observation . 
both the anteroposterior x - ray and the lateral x - ray can achieve effective in conclusion , mapping analyses of the number and distribution of the fracture lines could reveal the classification of distal radial intra - articular fractures . 
the results from the current study will be useful for the further understanding of the fracture patterns , providing the basis for the preoperative use of diagnostic imaging methods as well as for further developments in surgical approaches and fixation techniques for specific fracture types . 
a , c , e , g , i the anteroposterior x - ray film ; b , d , f , h , j represents the lateral x - ray fil although fracture lines can be seen in ( a , c ) , it is difficult to distinguish the distribution of fracture lines on the dorsal and dorsal sides . 
separation and displacement of the volar and dorsal fractures of the distal radius can be observed in ( j ) 1 3 la radiologia medica ( 2019 ) 124 : 613619 size and the assignment of all fracture fragments to one of the quadrants . 
the study group used 100kvp and reduced cm concentration of 270mgi / ml , and the images in this group were reconstructed with 50% adaptive statistical iterative reconstruction ( asir ) and mbir . 
the subjective quality included overall image noise , enhancement degree , lesion ( including mediastinum mass , pulmonary space - occupying lesions , and parenchymal infiltrative lesions ) conspicuity , and beam - hardening artifacts . 
56 , nanlishi road , xicheng district , beijing100045 , china 2 department ofradiology , tokyo womens medical university & medical center east , tokyo116 - 8567 , japan 3 respiratory department , beijing childrens hospital , capital medical university , no . 
56 , nanlishi road , xicheng district , beijing100045 , china vol . : ( 0123456789 ) 1 3 596 introduction low - dose computed tomography ( ct ) is being rapidly adopted in clinical practice [ 1 ] , especially in pediatric population . 
a large number of studies have been focused on using low - dose ct in children [ 2 , 3 ] , and on using iterative reconstruction ( ir ) algorithms to maintain image quality under low - dose conditions in imaging various body parts such as chest , abdomen , and blood vessels [ 48 ]  . 
related researches have shown that full model - based iterative reconstruction ( mbir ) is more effective than adaptive statistical iterative reconstruction ( asir ) , resulting in more significant reduction in image noise [ 912 ]  . 
studies have shown that the use of low tube voltage in ct scanning can improve contrast - enhancing effects [ 13 ] , which can be utilized to reduce the amount of iodine in contrast mediuin our study , we performed low - radiation - dose contrast - enhanced chest ct in a group of children using reduced contrast medium concentration ( 270mgi / ml ) to lower the total contrast dose and used the low voltage of 100kvp to offset the contrast dose reduction . 
our objective was to determine the effects of the full model - based iterative reconstruction ( mbir ) algorithm in improving the image quality under low - dose conditions , using the state - of - the - art adaptive statistical iterative reconstruction ( asir ) as the reference of standard . materials andmethods general information this study was approved by the ethics committee of our hospital . 
a total of 56 children who underwent chest ct examination from august 1 to october 31 , 2015 , were enrolled in the study group , and the projections of the contrast - enhanced phase in this group were reconstructed with both asir ( default reconstruction ) and mbir . 
clinically , all patients la radiologia medica ( 2019 ) 124 : 595601 underwent the contrast - enhanced ct scans to evaluate the parenchymal lesions and their correlation with surrounding tissues . instruments imaging data were collected using a ct scanner with a gemstone detector ( discovery hdct 750 , ge , usa )  . 
both patient groups shared the following same scan and contrast injection protocol : helical pitch value of 1.375 and rotation speed of 0.4s ; automatic tube current modulation ( atcm ) in the range of 10700ma during the scan to obtain agebased image noise index ( ni ) settings : ni = 11 hu for children with age of 012months , ni = 13 hu for 12years old , and ni = 15 hu for 314years old ; total contrast agent volume based on body weight at ratios of 1.21.8ml / kg ( 1.8ml / kg for child with weight of 35kg , 1.6ml / kg for 510kg , 1.4ml / kg for 1015kg , and 1.2ml / kg for 1535kg )  . 
the contrast agent was administrated through intravenous injection using a single - tube high - pressure syringe at the rate of 0.43.0ml / s and total injection time of 15s . 
for the study group , the tube voltage was set at 100kv , and the 270 mgi / ml concentration contrast medium ( iodixanol , ge healthcare , america ) was used . 
the original data obtained were reconstructed with mbir ( study group 1 ) and 50% asir ( study group 2 ) at image slice thickness of 0.625m for the control group , tube voltage was set at 120kv and the 320 mgi / ml concentration contrast medium ( iodixanol ) was injected . 
images in the control group were reconstructed with 50% asir only at slice thickness of 0.625mduring the ct scans , the children were lying on their back with arms raised overhead without holding breath . 
oral sedative medicine ( 10% chloral hydrate , 0.5ml / kg ) was given to children who could not cooperate , and scan was performed after subjects falling to sleep . 
additionally , the normal 5 - mm slice thickness images were reconstructed for the routine clinical diagnostic purpose . subjective image quality evaluation the three sets of images were transmitted to a ge aw4.6 ct workstation for analysis and measurement . 
two physicians , one with 12years of experiences ( 3years in adult imaging and 8years in pediatric imaging ) and the other with 17years of experiences in pediatric imaging , examined the images arranged in random order . 
during the evaluation process , the doctors were allowed to adjust the width of display window 1 3 la radiologia medica ( 2019 ) 124 : 595601 according to personal habits and use the multi - plane recombination tool equipped on the workstation to observe the images at multiple perspectives . quantitative evaluation of image quality was performed in refer to relevant studies [ 4 , 14 ]  . 
for overall image noise : 4 indicated that the image was exquisite with very little noise ; 3 meant that the image was fine with acceptable noise ; 2 referred to an image with some noise , but the overall quality still met the diagnostic requirement ; while 1 was defined as that the image quality was difficult to accept . 
for evaluation of the degree of enhancement , 4 referred to that images of the soft tissue and the mediastinum structure were obviously enhanced with the boundary between the edge and the surrounding clearly defined ; 3 indicated that the degree of enhancement was obvious , with the slightly blurred edge with clear resolution ; 2 meant that image was somewhat enhanced with the surrounding tissue distinguishable , but the edge was not clear , still meeting the diagnostic requirement ; and 1 was defined as poor structural enhancement with marginal boundary unclear and could not meet the diagnostic requirement . 
lesion display ability was in concern with the display of the ranges and details of lesions , including mediastinum mass , pulmonary spaceoccupying lesions , and parenchymal infiltrative lesions , as well as the display of small blood vessels in or around the lesion : 4 stood for a clear lesion structure display with good contrast and good detail ; 3 indicated decent display of the lesion and detailed structure with clear boundary ; 2 meant low clarity of the lesion and detailed structure and poor contrast , but still met the basic diagnostic requirement ; while 1 referred to image with lesion and surrounding tissue difficult to be distinguished . 
for evaluation of beam - hardening artifacts : 4 indicated that the image was even and delicate with no obvious beam - hardening artifact ; 3 stood for a small amount of observable beam - hardening artifacts but without impact on the diagnosis ; 2 referred to images with more apparent beam - hardening artifacts but the diagnosis was not affected ; while 1 meant that image was with more beamhardening artifacts that affected the diagnosis . 
a unified score was given after discussion according to the scoring standard , and the original scores from the two reviewers were tested for consistency . objective image quality measurement after the subjective image quality evaluation was completed , the two doctors performed the objective quality evaluation of the image together by measuring the image noise . 
 the sizes of rois for ct value and sd measurement in the back muscle were set to be half of the cross - sectional area of the descending aorta at the same plane . 
the signal - to - noise ratio ( snr ) was calculated as the ratio between ct value and the noise value in each tissue , and the contrast - to - noise ratio ( cnr ) of the left ventricle was calculated using the following formula : cnr = ( ct value ( left ventricular ) ct value measurement ofradiation dose andcontrast dose ( muscle ) ) sd ( muscle ) the radiation dose , volumetric ct dose index ( ctdivol ) , dose length product ( dlp ) , and the total volume of contrast agent used were recorded in both groups . 
the amount of iodine used was then calculated according to the concentration of the contrast agent . statistical analysis measurement data including subjective score and objective noise measurement were represented as x s . 
the analysis of variance ( anova ) was used to compare the differences in the subjective score and objective measurement among the three image groups , and kappa test was used to evaluate the consistency of the subjective scores by the two radiologists . 
all statistical analysis was performed using spss version 17.0 ( ibm , usa ) with p < 0.05 considered as statistically significant . results a total of 56 children ( 36 males and 20 females , with a median age of 4 years , ranging 4 months14 years ) were enrolled in the observation group . 
the noise of mbir image was reduced by 42.80% ( in left ventricle ) and 59.36% ( in muscle ) compared to those of the asir image in the control group . 
however , the snr and cnr of mbir images were significantly increased , with cnr of mbir image in the study group increased by 165.70% compared to the asir image of the control group . 
evaluation of asir images from the study group and the control group showed that there was no statistical difference in the overall image noise scores , both lower than the diagnostic requirements . 
although the thickness of layer in a was 0.625mm , the noise was significantly lower than that of c and e , close to that of b and d , indicating that mbir could significantly reduce image noise . 
the edge of the low - density component ( white arrow ) in the lesion of c was unclear , while it could be observed relatively more clearly in mbir images with both the thick and thin layers . 
similar changes could be observed in control group images of d and e ; horizontal beam - hardening artifact ( black arrow ) could be observed in c , resulted from reduced electron penetration in the low - voltage scanning , which was not obvious in e with the conventional voltage , and in a in which mbir eliminated the artifact ; the mediastinal small blood vessel ( white arrow ) in c was blurred and not continuous , although it could not be clearly displayed in b due to the layer thickness ; mbir images could clearly show small lesions due to low noise of solid tissues or organs , it is still recommended to use a 100kv setting [ 18 ]  . 
 according to our previous experience , children before the age of 14 who did not enter puberty are usually with a relatively constant body size significantly smaller than adults , therefore suitable for low - voltage ct scans . 
in our study , we have limited the use of 100 kvp for patients with age less than 14years of age . scanning at low voltage can significantly improve the contrast of the image , especially the ct value of the contrast agent [ 20 , 21 ] , which facilitates observation of the lesion . 
on the other side , low - voltage scanning increases the beam - hardening artifact of the image , which is not conducive to image observation [ 19 ] , especially the observation of detailed structures . 
while the increased beam - hardening artifacts at 100kv scanning had a certain impact on the image quality , especially at a layer thickness of 0.625mm which usually with high noise level , the detail display capability was reduced . 
compared to the asir images of the control group , cnr of the mbir images was increased by 165.70% , which was similar to the previous research results [ 14 ]  . 
in these settings , when only asir images from the study group and the control group were evaluated , it was found that both the subjective quality and objective quality of the images from the two groups were with no significant difference . 
therefore , the 100kv low - voltage scan can reduce the amount of contrast agent by about 20% compared with the conventional 120kv scan under the premise of ensuring image quality , similar to the previous findings in the heart scanning [ 23 ]  . there are several end goals when designing the research projects with iterative reconstruction algorithms . 
the most common one is to reduce dose ( either radiation and / or contrast medium dose ) while maintaining similar image quality in terms of enhancement and image noise by using more advanced iterative reconstruction algorithms . 
in our research , the main object was to demonstrate the ability of mbir algorithm to significantly improve image quality compared with the stateof - the - art asir algorithm at similar radiation dose . 
we assigned same noise index for both the study and control groups in our study , and the ct system adjusted tube current to achieve the target noise setting , which resulted in similar radiation dosage for the two groups . according to previous research , mbir could significantly reduce the noise of images , with the quality of 0.625 - mm mbir image similar to that of the 5 - mm fbp images [ 10 ]  . 
considering that chest - enhanced ct is mainly to observe the mediastinal occupancy or vascular condition , the 0.625 - mm image allows observation of more details in the chest lesion . 
the results of the current study have demonstrated the potential of the full model - based iterative reconstruction in imaging solid tissues or organs with the 0.625 - mm thin slice thickness rather than the standard 5 - mm images : mbir could reduce image noise more effectively than asir algorithm , improve image quality , and facilitate the observation of fine structures of lesions under thinner images . 
however , due to the limited noise reduction in asir , the microstructure observation was not satisfactory for small enhanced lesions and small blood vessels , and the fine structures of lesions could not be clearly observed . 
the mbir significantly reduced the noise and eliminated excessive beam - hardening artifacts , which not only highlighted the high degree of enhancement brought about by 100kv , but also further improved the observation of fine structures . 1 3 la radiologia medica ( 2019 ) 124 : 595601 there are still some limitations in the current study : first , skewed distributed prevented age stratification or weight stratification . 
osteochondral defects were most commonly detected at the medial talar dome : in 29 of 37 patients ( 78.3% ) in the ocd without loose bodies group and in 16 of 29 ( 55.2% ) patients in the ocd with loose bodies group . 
 ocds of the distal tibial plafond are not rare in the ankle joint and are often associated with loose bodies . keywords ankle joint mr arthrography anterolateral impingement osteochondritis dissecans loose body introduction traditionally , the majority of osteochondral lesions of the tibiotalar joint have been described as occurring in the posteromedial and anterolateral talar dome [ 13 ]  . 
our * hayri ogul drhogul@gmail.com 1 department ofradiology , medical faculty , ataturk university , erzurum , turkey 2 department ofradiology , erzincan university mengcek gazi training andresearch hospital , erzincan , turkey 3 department oforthopedic , medical faculty , ataturk university , erzurum , turkey 4 niversite mah . , niversite lojmanlar kme evleri lojman sitesi 45 blok no : 50 kap no : 3 , yakutiye / erzurum , turkey experience with ankle magnetic resonance ( mr ) arthrography suggests that an osteochondral lesion of the tibial and fibular plafond is not rare in patients with osteochondritis dissecans ( ocd )  . 
for an optimal treatment approach , it is also crucial to determine the stage of the osteochondral lesion . computed tomography ( ct ) and mr arthrography examinations are very sensitive imaging methods for the evaluation of loose bodies and ocds . 
in patients with loose bodies , intra - articular - injected contrast media might leak into adjacent anatomic compartments , and this situation shows the possible migration pathways of loose bodies . 
the purpose of our study was to use mr arthrography to determine the relationship between joint capsule thickness and the stage of osteochondral lesions of the tibiotalar joint and to evaluate their clinical results . 
additionally , this arthrographic study demonstrates the unusual locations of osteochondral lesions of the tibiotalar joint . materials andmethods patients this retrospective study included 82 consecutive patients referred to ataturk university hospital for ankle mr arthrography between march 2015 and february 2017 . 
 diluted contrast medium ( 0.5mmol / l gadopentetate dimeglumine , magnevist , bayer schering pharma , germany ) at a concentration of 1 : 200 was injected ( 0.1ml contrast medium diluted in 20 ml normal saline )  . 
our mr arthrography protocol includes turbo spin - echo ( se ) t1 - weighted ( tr / te , 650 / 15ms echo train length , 8 section thickness , 3mm spacing , 0.3mm field of view , 130200mm matrix , 256 256 three signals acquired ) and fat - suppressed turbo se t1 - weighted images . 
two staff radiologists with 11 and 4years of experience in musculoskeletal imaging , respectively , who were blinded to the diagnosis of the patients independently analyzed the mr arthrography images . 
all mr arthrography images were evaluated in a randomized fashion followed by evaluation of the same mr arthrography images4weeks later in a different randomized order for assessment of intraand interobserver agreement . 
volumetric measurements of extra - articular contrast material leakage ( into adjacent synovial compartments ) and tibiotalar joint capacity were taken with a 3d volume measurement workstation ( myriad pro , intrasense , france )  . osteochondral lesions of the tibiotalar joint on the basis of ct and mr arthrography were divided into four subtypes . 
a p value was calculated for each comparison , and values 0.05 were considered to indicate statistical significance . we evaluated other features of anterolateral impingement ( e.g. , scar tissue of the synovium , meniscoid lesions , and synovial plicae / bands )  . results arthroscopy andct arthrography the time interval between ct or mr arthrography and arthroscopy was between 2weeks and 2months . 
all ct arthrography examinations were performed using a second - generation somatom definition flash 256 - slice dual - source multidetector ct scanner ( siemens healthcare , forchheim , germany )  . 
the mannwhitney u test was used to compare the relationship between anteromedial , anterolateral , and posterior joint capsule thickness for both the ocd without loose bodies and ocd with loose bodies groups . 
four of the remaining six patients ( 23.5% ) had grade ii anterolateral impingement syndrome ( fig.3 ) , and two of the remaining six patients ( 11.8% ) had grade iii anterolateral impingement syndrome . 
locations of the ocd , loose bodies , and extravasation are summarized in table3 . we detected a moderate interobserver agreement in the detection of the osteochondral defects and loose body localizations in the ocd with loose bodies group . 
anterolateral capsular thickening in the ocd patients with loose bodies clinically was associated with anterolateral impingement syndrome . intra - articular loose bodies might associate with impingement syndrome in the ankle joint [ 10 , 11 ]  . 
c axial t1 - weighted fat - suppressed conventional spin - echo mr image shows thickening of the inferior portion of the anterior tibiofibular ligament ( grade ii thickening of the inferior anterior tibiofibular ligament )  . 
f axial t1 - weighted fat - suppressed conventional spin - echo mr image shows a smooth contour of the anterolateral joint capsule 1 3 658 la radiologia medica ( 2019 ) 124 : 653661 it has been alleged that traumatic occasions account for a substantial percentage of ocd etiologies , although this has not been definitively established [ 12 , 13 ]  . 
it is known that inversion injury of the ankle joint is an important precursor for the development of osteochondral damage at the medial anterior tibial plafond and the medial talar dome [ 14 ]  . 
current study results advance the trauma theory for the development of anterolateral impingement syndrome , as lesions originating from medial talar dome and medial tibial plafond corresponded with 86.3% of the ocd patients with loose bodies . prior to the last two decades , when osteochondral lesion of the ankle joint was diagnosed it exclusively referred to ocd of the talar dome . 
furthermore , it has also been reported that these lesions were frequently encountered , contrary to popular belief , when examinations were re - checked , and the low prevalence was most likely due to overlooking of the anatomical location [ 5 , 8 , 14 ]  . 
 for the last 2 years , we have detected nine lesions in our database , for which the annual encounter rate was similar to those authors . in a biomechanical study , athanasiou etal . 
 in contrast to our findings , most of these tibial and fibular lesions were kissing lesions , and furthermore , none of these lesions at the distal tibia and fibula was reported as stage 4 ocd . 
the sensitivity of conventional mr imaging is somewhat lower compared to mr arthrography in the staging of ocd due to the insufficient delineation of loose bodies [ 17 ]  . 
d axial t1 - weighted non - suppressed conventional spin - echo mr image shows diffuse irregular thickening of the anterolateral capsular tissues and obliterating of the anterolateral ankle recess ( grade iv irregular nodular soft tissue thickening ) radiological evidence representing varying degrees of anterolateral impingement that we found in all patients with loose bodies supports the above idea . 
in our study , all of the detected ocds of the tibial plafond were grade 4 , and all those lesions were associated with the clinical and arthrographic findings of high - grade ( grade 34 ) anterolateral soft tissue impingement syndrome . 
one of the reasons for the absence of the above - mentioned lesions might be healing of stage 1 or 2 ocds of the talar dome . in ankle joint ocds , free fragments of cartilage or bone might stay within the joint space or migrate to adjacent synovial compartments [ 17 ]  . 
ct and mr examinations performed after the injection of contrast material in the joint space are the most sensitive imaging methods for the evaluation of loose bodies and ocds [ 13 , 17 ]  . 
for instance , a loose body located adjacent to the tendon of the flexor hallucis longus can be a cause of chronic irritation of this tendon and is thus one of the reasons underlying constant and recurrent pain of the heel and posterior foot . 
in our series , eleven cases ( 38% of all loose bodies ) had loose bodies located in adjacent anatomic compartments ( posterior talocalcaneal joint and synovium of the tendon of the flexor hallucis longus )  . 
we think that these rates were considerable amounts and that intra - articular - injected contrast material that leaked into adjacent compartments eased our work for the detection of loose bodies . no age restrictions in patient populations should be recognized as a limitation in this study . 
in these patients , especially in those with loose bodies , fractures of osteophytic fragments might complicate the situation . concerning ocds of the ankle joint , this mr arthrography study showed that clinic and mr arthrographic findings of anterolateral impingement syndrome often accompany grade 4 ocds . 
routine head mri and three - dimensional pseudo - continuous arterial spin labeling were performed using a 3.0 - t system within 7days prior to operations , and at 4 consecutive time - points ( 24 , 48 , 72 , and 96h ) after operations . 
comparisons within groups were made using paired t test , and comparisons between groups were made using independent - sample t test . results the cbf values markedly increased at 24h after cas and cea ( p < 0.05 ) compared with baseline . 
most patients showed peak cbf values on the ipsilateral side at 72h ( 13 / 19 , 68% ) after cas and at 48h ( 10 / 13 , 77% ) after cea , which then declined . 
previous studies have only revealed an improvement in cbf in the ipsilateral side by monitoring 1day after cas [ 912 ] and cea [ 13 , 14 ]  . a number of methodologies , including quantitative magnetic resonance angiography ( qmra ) [ 9 ] , dynamic susceptibility contrast perfusion mr ( dsc ) [ 10 ] , xenon - 133 single - photon emission computed tomography ( spect ) [ 11 ] , continuous arterial spin labeling ( casl ) [ 13 ] , and perfusion computed tomography ( pct ) [ 14 ] , have been applied to investigate hemodynamic changes after cas and cea . 
 recently , three - dimensional ( 3d ) pseudo - casl ( pcasl ) was shown to be a promising technology with high signalto - noise ratio ( snr ) and spatial resolution and was able to vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 636642 quantify absolute cbf invivo [ 15 , 16 ]  . 
the highly precise 3d - pcasl , which does not need a gadolinium - based tracer , can be used repeatedly to evaluate cbf changes over time and has favorable intraand inter - scanner reliability and reproducibility [ 17 ]  . 
all study protocols were approved by the institutional review board of our hospital , and written informed consents were obtained from all patients . all the patients were diagnosed using conventional angiography . 
to ensure patient safety , blood pressure was monitored in accordance with the patients specific condition by two experienced clinicians , and a systolic blood pressure value of < 120mm hg / diastolic blood pressure value of < 80mm hg was maintained during the 2496 - h period after cas and cea to reduce the influence on postoperative cbf changes . 
patients who satisfied the following criteria were enrolled : ( 1 ) symptomatic severe unilateral intracranial ica stenosis ( 7099% stenosis ) ; ( 2 ) no obvious abnormality in the rest of the cerebral artery ; and ( 3 ) ica stenosis caused by atherosclerosis . 
first , fast - spoiled gradient - recalled echo was normalized to montreal neurological institute template space using spm8 ( statistical parametric mapping , university college of london , available at softw are / spm8 ) on the matlab platform ( r2013b ; math works , natick , ma , usa )  . 
subsequently , cbf map was coregistered to the normalized t1 - weighted template and spatially smoothed with a 6 - mm full - width - at - half - maximum gaussian kernel . 
according to the time of data acquisition , cbf values of ipsilateral ica territory of cas ( g1 ) , contralateral ica territory of cas ( g2 ) , ipsilateral ica territory of cea ( g3 ) , and contralateral ica territory of cea ( g4 ) were divided into five groups : within 7days before operation 1 3 638 la radiologia medica ( 2019 ) 124 : 636642 fig . 
mean cbf value of ipsilateral and contralateral sides was measured by using voi ( t0 ) , and at 4 consecutive time - points post - treatment : 24h ( t1 ) , 48h ( t2 ) , 72h ( t3 ) , and 96h ( t4 )  . 
comparisons between t0 and t1t4 post - treatment cbf values for the treated side and those for the contralateral side were made separately for cea and cas groups using a paired t test . 
meanwhile , demographics including blood pressure , age , degree of stenosis , sex , hypertension , hyperlipidemia , diabetes mellitus , obesity , and cigarette smoking were compared between patients who underwent cea and cas . 
data are presented as mean sem . results the baseline characteristics of patients treated with cea and cas , including age , sex , blood pressure , degree of stenosis , and vascular risk factors , are summarized in table1 . 
in the later time - points , most patients showed peak cbf values on the ipsilateral side 72h ( 13 / 19 , 68% ) after cas , which then declined at 96h ; most patients showed peak cbf values on the ipsilateral side 48h ( 10 / 13 , 77% ) after cea , which descended 72 h and remained relatively stable at 96h . 
however , the major challenge of the revascularization of ica stenosis following cea or cas is the postoperative management including blood pressure control and cerebral hyperperfusion syndrome ( chs ) [ 7 , 8 ] , which are all associated with cerebral hemodynamic changes due to a state of maximal vasodilation of the cerebral arterioles and poor cerebrovascular pressure autoregulation as a result of prolonged perfusion reduction caused by the stenosis [ 46 ]  . 
 in the present study , we had found that the cbf values markedly increased at 24h after cas and cea compared with baseline , but the peak cbf values on the ipsilateral side were presented at 72h ( 13 / 19 , 68% ) after cas and at 48h ( 10 / 13 , 77% ) after cea , which then declined . 
what is more , the cbf values for the ipsilateral ica territory of cea group were significantly higher than those of cas group whether at 24 , 48 , 72 , or 96h . 
to the best of our knowledge , this is the first study to investigate the pattern of cbf changes after cea or cas and compare the differences of postoperative effect between cea and cas by using 3d - pcasl . as revealed by the linear graph , we postulated that postoperative 72 h after cas and 48 h after cea might be focused to prevent subsequent severe complications such as chs which is associated with the fluctuation of cbf changes , and an early discharge within the time frame should also be avoided . 
 from these data , it can be inferred that the cbf values between the ipsilateral and contralateral sides are close after the treatments , which is consistent with our results . 
the conclusion may suggest the importance of first achieving collateral circulation to relieve the hypoperfusion effects of the ipsilateral side and providing metabolic compensation before treatment ; these actions additionally moderate the high perfusion pressure after cea and cas . the prevalence of chs between cas and cea for patients with severe ica stenosis has long remained a contentious medical issue . 
we found that cea resulted in higher cbf values of ipsilateral ica territory than cas at the 24 - h , 48 - h , 72 - h , and 96 - h time - points . 
however , we believe that the results might imply both types of explanation for the individual differences : for patients with risk factors for chs , such as bilateral carotid artery stenosis , previous stroke , and peri - procedural hypertension [ 5 ] , a higher cbf might be harmful after cea , and for patients without risk factors for chs , a higher cbf might be beneficial or neutral fig . 
2 absolute cbf quantification in ica territory of ipsilateral and contralateral sides on 7 days before cas and cea and consecutive scan once per 24 h after cas and cea . 
t0 , before operation ; t1 , 24 h after operation ; t2 , 48 h after operation ; t3 , 72 h after operation ; t4 , 96h after operation . 
data are mean sem we also found that the cbf values of the contralateral and ipsilateral ica territories showed similar variations , but the increase in cbf on the contralateral side was smaller than that on the ipsilateral side . 
moreover , previous studies have shown that cbf values increased not only in the ipsilateral side , but also in the contralateral side after cea and cas ; for example , yun etal . 
secondly , only a single pld of 2.0s as recommended in asl white paper was used in this study [ 33 ] , which might induce error since the flow arrival time might be shifted for the sake of blood velocity changes after cea and cas . 
considering the multiple parametric evaluation including arterial arrival time map and delay - corrected cbf map and considering the superiority to visualize slow flow , the multi - delay asl protocol might be useful to solve the problehowever , the multi - delay asl required long scanning time . 
this distends the spinoglenoid notch and can be enlarged in cases of suprascapular neuropathy which is evident on mri . keywords suprascapular neuropathy magnetic resonance imaging arthroscopic suprascapular nerve decompression suprascapular vein spinoglenoid notch introduction suprascapular neuropathy ( ssn ) is caused by entrapment of the suprascapular nerve under the transverse scapular ligament and can result in chronic shoulder pain [ 1 , 2 ]  . 
multiple etiologies for ssn exist including cysts originating from the glenoid labrum , tumor , ossification of the transverse scapular ligament , and traction from either overhead activity or retraction of the supraspinatus in a rotator cuff tear [ 1 , 36 ]  . 
 the diagnosis of ssn is difficult and is typically made on * yoshihiro katsuura yoshikatsuura@gmail.com 1 department oforthopaedic surgery , university oftennessee college ofmedicine , chattanooga , 975 east third st . , hospital box260 , chattanooga , tn37403 , usa 2 department ofradiology , erlanger university hospital , chattanooga , usa 3 royal colleges ofsurgeons inireland , dublin , ireland the basis of clinical examinationnotably pain and rotator cuff weakness [ 1 , 7 , 8 ]  . 
magnetic resonance imaging ( mri ) may be used to detect signs of denervation in the supraspinatus and infraspinatus , identify mass lesions , and rule out other causes of shoulder pain such as rotator cuff tears [ 7 , 12 , 13 ]  . 
currently , there are no simple and definedradiographic markers of suprascapular neuropathy . the suprascapular vein passes under the transverse scapular ligament along with the surpascapular nerve as it courses toward the jugular system where it empties [ 14 ]  . 
the healthy controls had a varicosity size on average of 2.3mm , whereas the ssn patients vol . : ( 0123456789 ) 1 3 644 la radiologia medica ( 2019 ) 124 : 643652 had an average of 8.4mthe second was by van meir etal . 
we suggest that examining the spinoglenoid notch for distension ( an indirect marker of venous engorgement ) on magnetic resonance imaging ( mri ) can aid in the diagnosis of ssn . 
the goal of this study was to compare spinoglenoid notch distension size on mri between patients with electrodiagnostic confirmed ssn treated with arthroscopic release to normal shoulder controls . institutional review board approval was granted for this study in february 2018 , which was compliant with the health insurance portability and accountability act ( hipaa )  . 
a waiver for informed consent was obtained . methods patients a retrospective review of prospectively collected data was performed of patients who had failed conservative therapy and undergone arthroscopic suprascapular nerve release by the senior author between november 2013 and november 2014 . 
patients were included if they had the following : a clinical diagnosis of ssn based on examination by the senior author , an electrodiagnostic confirmation of ssn , and an available shoulder mri . 
data collected included age , sex , body mass index ( bmi ) , diabetic status , smoking status , and workers compensation status . sixtyssn patients were compared to 47 normal shoulders of patients ages 1830years who were randomly selected based on our population of shoulder mris on the pacs systepatients in this cohort were included if they had no significant derangement of the shoulder per the radiology report . 
patients of this age - group were selected because of the highest likelihood of having a normal shoulder free of degenerative change . image protocol andanalysis due to the retrospective nature of this study , performed over several years across two institutions , mr imaging protocol and parameters varied . 
all non - arthrogram examinations included an axial t2 fast spin echo ( fse ) sequence with fat saturation or proton density ( pd ) sequence with fat saturation ( tr = 20003920 , te = 3048 ) and all arthrogram examinations included either an axial t2 fse with fat saturation or axial t1 fat saturated ( fs ) sequence ( tr = 339.0900.0 , te = 1123 ) from which measurements were obtained . the spinoglenoid notch distension was evaluated by two independent observers who did not refer to each others findings . 
to ensure reproducibility of the measurements and calculate the intra - rater reliability , a second set of blinded measurements were made by each observer 6weeks after the first set . 
moreover , muscle quality was rated according to the goutallier classification where grade 0 was no fatty infiltration , grade 1 was some fatty streaking , grade 2 was fat < muscle , grade 3 was muscle = fat and grade 4 was fat > muscle [ 18 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 643652 fig . 
the coronal section ( red line ) is scrolled progressively posterior until at the base of the spinoglenoid notch is reached ( green line ) while still within the bone of the glenoid . 
sensitivity and specificity were tabulated using cross - tabs function . statistics were performed using the statistical package for the social sciences software ( ibm , version 24.0 , chicago , usa )  . 
a dependent t - test was used to compare means within the same group ( i.e. , vas improvement ) , and an independent t test was used to compare the means of the varicosity size and glenoid neck width as well results patients the average age of the ssn group ( n = 60 , female = 29 ) was 52years ( range 2172 )  . 
with the image set on the correct coronal section ( fig.1 ) , the axial section ( red line ) is scrolled progressively inferior until at the base of the suprascapular notch within the bone of the glenoid ( green line ) current or former smokers , and 16 were workers - comp patients . 
the average age of the control group ( n = 47 , female = 21 ) was 24years ( range 1830years )  . reliability andreproducibility analysis the interclass correlation coefficient for the intra - rater reliability for was 0.89 ( p < 0.001 ) for spinoglenoid notch distension and 0.87 ( p < 0.0001 ) for the glenoid neck 1 3 la radiologia medica ( 2019 ) 124 : 643652 fig . 
the interclass correlation coefficient for the intra - rater reliability for was 0.95 ( p < 0.0001 ) for spinoglenoid notch distension and 0.98 ( p < 0.0001 ) for the glenoid neck measurement again indicating excellent agreement . 
 the mean diameter of the transverse scapular ligament was 7.54mm ( sd = 2.03 ) in the ssn group and 4.49 mm 1 3 648 la radiologia medica ( 2019 ) 124 : 643652 fig . 
e axial proton density view of the same patient shows distension of the spinoglenoid notch measuring 7mm sensitivity andspecificity discussion using a spinoglenoid notch distension value of 7mm as a cutoff for a screening test , the sensitivity for suprascapular neuropathy was 74% and the specificity was 78% . 
the nerve then courses with the suprascapular vein under the spinoglenoid ligament in the spinoglenoid notch on its way to innervate the infraspinatus [ 14 , 19 , 20 ]  . 
despite being a relatively small caliber 1 3 la radiologia medica ( 2019 ) 124 : 643652 1 3 650 la radiologia medica ( 2019 ) 124 : 643652 fig . 
7 bar chart comparing glenoid width averages between suprascapular neuropathy ( ssn ) patients and controls nerve , it supplies the significant amount of sensory and motor innervation to the shoulder [ 14 , 2022 ]  . 
as the nerve is tethered to the scapula at this location , it is sensitive to compression from mass effect caused by cysts , varicosities , or hypertrophy of the transverse scapular ligament [ 46 , 23 ]  . the diagnosis of suprascapular neuropathy is often elusive . 
part of the reason for this is that it is often difficult to make the diagnosis asthere are no quantitative imaging methods to aid in the clinical work up [ 1 ]  . 
 additional tools to aid in the diagnosis of ssn should be developed . on examining the images of normal shoulder mris from the control group , we noted that the infraspinatus invests into the spinoglenoid notch . 
we found that the distance between the glenoid and the infraspinatus at the spinoglenoid notch ( spinoglenoid notch distension ) to be increased in patients with suprascapular neruropathy ( m = 8.36 mm ) , which was almost identical to the vein caliber measured by carroll etal . 
as the suprascapular vein runs underneath the transverse scapular ligament with the suprascapular nerve [ 14 ] , we postulate that the anatomical basis for the distension of the spinoglenoid notch is obstruction of the suprascapular veins caused by hypertrophy of the transverse scapular ligament . 
additionally , in cases of overhead use of the arm , the veins may suffer intimal damage via 1 3 la radiologia medica ( 2019 ) 124 : 643652 compression by the transverse scapular ligament accelerating formation of varicosities . 
while previous studies have implicated varicose veins as a cause of ssn , we suggest instead that varicose veins are the result of impeded flow back toward the jugular systespinoglenoid notch distension may be used as an adjunct diagnostic sign to aid the clinician in patients with refractory shoulder pawe suggest that a varicosity notch size of > 7mm is a good cutoff to support the diagnosis of ssnin conjunction with clinical and electrophysiologic findings as this value had the best combined sensitivity and specificity of a range of values we tested . 
however , a simpler test is examining the spinoglenoid notch on an axial view to see whether the infraspinatus is pushed away from the groove . the treatment of suprascapular neuropathy is a trial of conservative therapy followed by open or arthroscopic release which has been shown to be effective in a number of studies [ 2629 ]  . there were several weaknesses with this study . 
we also performed a sub - analysis examining the difference in notch size between non - contrast and arthrogram studies in the control group and were unable to find a significant difference . 
to account for the age difference between the two groups , we specifically examined the agematched subset of patients in the ssn group and the difference in varicosity size remained significant from controls . 
 we hope this study will help lead to future prospective studies comparing well - shoulder to ill - shoulder with bilateral mri scans as well as comparing mris in patients with negative emg / ncs studies to patient with confirmed ssn . in conclusion , the varicosity size is a simple measurement which can aid in the diagnosis of ssn and should be examined in suspected cases . compliance with ethical standards conflict of interest disclosure of potential conflicts of interest : no financial support was utilized for this study . 
all authors declare that they have no conflicts of interests . research involving human participants and / or animals all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . informed consent institutional review board approval was obtained from ut - college of medicine institutional review board , study number 18 - 021 . 
prospective studies are needed to further assess its role among locoregional treatment options for liver metastases from crc . keywords liver metastases stereotactic body radiotherapy colorectal cancer oligometastases introduction colorectal cancer ( crc ) is estimated to be the second most frequently diagnosed cancer in europe , accounting for 447 , 000 new cases in 2012 , and one of the most relevant causes of cancer mortality worldwide with 694 , 000 deaths in the same year [ 1 , 2 ]  . over the last two decades , the clinical outcome of patients with metastatic crc ( mcrc ) has improved due to many factors , such as local ablative treatments ( lats ) [ 3 ]  . 
potentially , lats can have a curative intent for oligometastatic patients [ 4 ] and could play a role in the management of an oligoprogressive disease , in which only a solitary or few ( 5 ) metastatic localizations progress , while all other sites of disease are stable or responding to the current regimen [ 5 ]  . 
over the past two decades , extensive clinical experience demonstrated sbrt to be a safe and high - precision technology method to deliver ablative treatments for different metastatic sites [ 8 ] , including liver metastases [ 9 ]  . since 2012 , robotic sbrt has been offered in our institution as a possible alternative to surgery or other lats for liver oligometastases in colorectal cancer patients unsuitable for surgery . the aim of our retrospective study was to report the clinical outcome of robotic sbrt in this setting . 
during treatment planning , the following organs at risk ( oars ) were delineated : left and right lung , esophagus , heart , thoracic wall or ribs , left and right kidneys , small and large bowel , duodenum , stomach , spinal canal , whole liver , great vessels . 
for most patients , the intended prescription dose was 37.5gy in three fractions , prescribed to the 70% isodose line to cover 95% of the ptv [ 10 ]  . 
 patients were prescribed proton pump inhibitors , serotonin 5 - hydroxytryptamine antagonists , benzodiazepines and antacids as clinically indicated . followup andtoxicity evaluation after the last application , a clinical examination was performed and treatment toxicity was scored , if present , according to the common terminology criteria for adverse events ( ctc - ae ) scale , v 4.0.3. 
treatment response was 1 3 872 la radiologia medica ( 2019 ) 124 : 870876 evaluated by serial contrast - enhanced spiral ct or mri scan 2months after end of sbrt . 
complete response ( cr ) was defined as disappearance of all target lesions ; partial response ( pr ) as at least a 30% decrease in the sum of diameters of target lesions ; progression disease ( pd ) as at least a 20% increase in the sum of diameters of target lesions . 
local control ( lc ) was defined as the time of absence of progression disease at the site of sbrt from the end of the treatment . statistical analysis local control , local and distant progression - free survival ( pfs ) and overall survival ( os ) curves were evaluated by the kaplanmeier method . 
for cb , additional investigation included treatment planning related parameters such as number of fractions , physical and biological effective dose ( bed10 , considering / = 10 ) coverages . 
in order to comply with dose constraints to organs at risk , a risk - adapted approach was followed for the treatment of nine lesions , which were irradiated in five fractions instead of three . 
 then , we compared the bed10 mean dose covering the ptvs between lf and lc , and we found that its median value was smaller in the lf group ( 89.26gy ) than in lc fig . 
actuarial 1 3 874 la radiologia medica ( 2019 ) 124 : 870876 although surgical resection is presently accepted as the first choice among strategies for ablation , for many reasons only a small percentage of patients qualify for surgical procedures [ 14 ]  . up to now , ct - guided percutaneous radiofrequency ablation ( rfa ) is the most common local treatment option to be offered to such patients [ 15 ]  . 
in recent years , sbrt has become the current standard in medically inoperable early lung cancer patient [ 16 ] and , potentially , it could be the same for unresectable liver metastases treatment [ 17 ]  . our analysis counted one of the most numerous series addressing the use of high doses of radiation by means of robotic sbrt in the treatment of liver metastases exclusively from crc . 
moreover , our study has other limitations : its retrospective nature , the heterogeneity of the prescription doses , the differences in the timing of sbrt with respect to other treatments . our results demonstrated that it is possible to have good outcomes on response rate and survival analysis , keeping an excellent safety profile . 
 [ 18 ] in their subgroup analysis on liver metastasis from adenocarcinoma , confirming that colorectal adenocarcinoma has a statistically significant worst lc than other histologies [ 19 , 20 ] , which is perhaps related to the fact that these patients are generally heavily pretreated and surgically unresectable [ 21 ]  . moreover , as chang etal . 
 [ 22 ] had already concluded in their meta - analysis , a dose of 4652gy in three fractions or higher is required to achieve 90% lc at 1year for the treatment of hepatic cr metastases . although a good performance in terms of lc , in our analysis , pfs ( both hepatic and distant ) was poor , if compared with the results obtained by berkovic etal . 
swaminath and dawson [ 23 ] had already noticed in their analysis that , although excellent local control rates were achieved , many patients developed out - of - field progression probably because of the relatively high number of patients with extrahepatic disease and / or more than three metastatic lesions , suggesting that a closer attention should be reserved to patients who really belong to a relatively good prognostic group with longer survival expectancy and offering a strong rationale for combining sbrt with systemic treatments , as hypothesized by scorsetti etal . 
in fact , comparing survival curves of patients with or without extrahepatic disease before sbrt , there is a clear advantage for the second ones , both in os and in pfs ( supplementary materials , figures1 and 2 )  . 
previous extrahepatic disease and number of metastatic lesions > 3 showed a statistically significant correlation at univariate analysis ; this result was confirmed at multivariate analysis only for the presence of previous extrahepatic disease , as in the pfs analysis . toxicity no complications were observed during or after fiducials placement . 
as referred by hellman and weichselbaum , the theory of oligometastases considers that there could be a subgroup of patients with metastatic disease that is intermediate between completely absent and widely metastatic [ 12 ]  . 
on the other hand , their cohort was less homogeneous than ours , since also patients treated for extrahepatic localizations ( lung , lymph nodes , suprarenal gland ) were included in the analysis . 
 [ 29 ] performed a phase 1 / 2 study enrolling about 70% of patients with liver metastases from non - colorectal origin ( lung , breast , ovary , esophagus and others )  . 
likewise , in scorsettis study [ 9 ] , more than 50% of patients had metastases from non - colorectal primary tumor , and more than 80% of patients received a prescription dose of 75gy in three fractions ( mean dose to ptv )  . 
as expected , very limited treatment - related toxicity was observed in our cohort ; however , it has to be acknowledged that our local control rate is at the lower range of published data . in particular , the rate of actuarial lc at 2years in these experiences ranges between 64 and 92% ( supplementary table2 )  . 
as a matter of fact , the net effect of sbrt on the irradiated lesion is critically dependent on the delivered physical total dose and fractionation , the applied bed , the size of the gtv , the prescription modality and the intrinsic biological radiosensitivity . 
overall , patients selection refinement and prospective trials based on strict inclusion criteria in the setting of oligometastatic crc should be warranted . conclusions survival and toxicity results of our retrospective analysis support the hypothesis that sbrt for liver metastases from crc is a feasible treatment , combining an excellent safety profile with acceptable efficacy results . 
in addition , only controlled studies could allow us to define how to best select oligometastatic patients potentially profiting from a locoregional treatment with the aim to defer further systemic therapies . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards informed consent was obtained from all individual participants included in the study . 
to detect urine leakage , we initially performed conventional cystography after retrograde distention of the bladder with dilute iodinated contrast material , followed by ultra - low - dose ct cystography . 
the diagnostic accuracy of these two modalities was compared , and the technical characteristics of ultra - low - dose ct cystography were examined . results all 31 referred patients were included in this study . 
of the 31 patients , 27 ( 87.1% ) underwent bladder repair after radical prostatectomy , 3 ( 9.7% ) after radical cystectomy , and 1 ( 3.2% ) after bladder diverticulectomy . 
based on these findings , we were able to establish a proper treatment plan . conclusions ultra - low - dose ct cystography is an accurate method for evaluating urine leakage after bladder repair , and this technique may help determine the most appropriate treatment strategy for patients with urine leakage after bladder repair . keywords anastomotic leakage radiation dosage computed tomography fluoroscopy introduction recently , awareness and concern about radiation exposure have increased . 
in the republic of korea , the number of radiation - generating devices has rapidly increased * seong hoon choi 0733280@uuh.ulsan.kr 1 department ofurology , ulsan university hospital , university ofulsan college ofmedicine , ulsan , korea 2 department ofradiology , ulsan university hospital , university ofulsan college ofmedicine , 877 bangeojinsunwando - ro , dong - gu , ulsan44033 , korea from 59 , 739 in 2008 to 72 , 626 in 2012 [ 2 ]  . 
in a study involving conventional non - contrast ct , the reported exposure dose ( ed ) for the abdomen and pelvis was between 10 and 20msv [ 6 ]  . 
therefore , if dose - reduced ct can be shown to accurately diagnose bladder injury , low - dose and ultra - lowdose ct could be applied to a wide variety of cases . one of the advantages of ct compared with conventional cystography is the ability to detect anatomical relationships . 
 a major concern associated with dose - reduced ct is higher noise , which results in lower image quality that may reduce the accuracy of this technique for detecting anatomical relationships and facilitating differential diagnoses . 
moreover , while low - dose and ultra - low - dose ct are effective for detecting urolithiasis [ 7 , 11 ] , it remains uncertain whether low - dose ct cystography can detect bladder injury or urine leakage . 
therefore , we performed a prospective cohort study to compare the accuracy and technical characteristics of ultra - low - dose ct cystography with those of conventional retrograde cystography . materials andmethods study participants from november 2015 to october 2017 , we prospectively examined 31 consecutive patients referred for cystography after bladder repair . 
 to diagnose urine leakage , we initially performed conventional cystography after retrograde distention of the bladder with dilute iodinated contrast material , followed by ultralow - dose ct cystography ( table1 )  . imaging technique andinterpretation conventional cystography was performed in the following manner : with the patient supine on the examination table , the urine bag was disconnected from the foley catheter and the foley catheter was suctioned using a 50 - ml syringe until the bladder was completely emptied . 
additional pelvic ap radiographs were obtained after the initial infusion of approximately 100ml of contrast material and after either infusion of another 150ml of contrast material or occurrence of one of the following endpoints : ( 1 ) 300ml of contrast material was completely infused into the bladder , ( 2 ) urinary leakage occurred due to continuous bladder detrusor activity with infusion less than 300ml , or ( 3 ) the patient complained of pain in the abdomen and pelvis . 
oblique radiographs were also obtained , followed by an ap radiograph after bladder emptying . ct cystography was performed in the following manner : with the patient supine on the examination table , the foley catheter was suctioned using a 50 - ml syringe , as described above . 
ultra - low - dose ct images were reconstructed using idose level 5 , which is one of the iterative reconstruction ( ir ) algorithms [ 12 , 13 ]  . 
the ct parameters were as follows : a pitch of 0.915 , collimation of 0.625mm , matrix size of 512 512 pixels , sectional thickness / reconstruction interval of 2mm , collimation of 2 64 0.6mm , pitch of 1.2 , and gantry rotation time of 0.5s. 
the reductions in radiation dose were compared between the two modalities and also with regard to the patients bmi [ 14 ]  . image findings were interpreted by an expert radiologist in the genitourinary division of the radiology department of our institution . 
the following conventional cystography and ct cystography findings were recorded : ( 1 ) presence or absence of leakage , ( 2 ) location of leakage , and ( 3 ) amount of leakage . 
the amount of leakage analyzed by conventional cystography was scored according to a previous report as follows : grade i , extraperitoneal leakage within 6cm of the vesicourethral anastomosis ( vua ) ; grade 2 , extraperitoneal leakage extending beyond 6cm from the vua ; and grade 3 , intraperitoneal leakage [ 15 ]  . 
informed consent was obtained from all subjects when they were enrolled . results the mean conventional cystography dose area product , ct cystography dose length product values , and the effective radiation dose are summarized in table2 . 
the estimated dose reduction using ultra - low - dose ct compared with the dose in conventional cystography was 60.7%. four of the 31 patients were diagnosed with urine leakage by conventional cystography . 
in all of the patients who were diagnosed with urine leakage by conventional cystography , leakage was observed at the posterior aspect of the vua ; moreover , all had grade 1 leakage ( leakage within 6cm of the vua )  . 
the amount of leakage in these patients was not large ( average , 1.31cm2 ; range , 0.581.74cm2 ) ( table3 )  . by performing ct cystography , we were able to track the precise locations and amounts of urine leakage . 
all nine patients who had urinary leakage , including the two with longer retention of the foley catheter , experienced no further complications and were discharged . discussion conventional cystography has been accepted as the standard for the assessment of bladder trauma [ 8 ]  . 
our study also showed that conventional cystography detected leakage at the posterior aspect of the vua in all patients who were diagnosed with urine leakage ; however , it is thought that the contrast collects in the dependent position by gravity . 
in particular , according to ultra - low - dose ct cystography , patient i had urine leakage at the 3 oclock position of vua , whereas 1 3 la radiologia medica ( 2019 ) 124 : 812818 fig . 
ct cystography identified the location of leakage at the 4 oclock position of vua , and the amount of leakage was estimated to be 7.08cm2 ( black arrow )  . 
c ct cystography showed patient i to have urine leakage at the 3 oclock position of the vua ( black arrow ) , but conventional cystography ( white arrow ) detected leakage at the posterior aspect of the vua according to conventional cystography , there was leakage at the posterior aspect of vua . lately , iterative reconstruction ( ir ) algorithms have received attention as good new methods for reducing radiation dose during ct examination [ 17 ]  . 
this 4th generation iterative reconstruction technique in preventing photon starvation artifacts ( streaks , bias ) prior to image creation and in maintaining image texture to overcome the artificial or plastic look of images that have been frequently reported when using previous iterative reconstruction techniques . 
evidence from rigorous clinical evaluations demonstrates the potential of idose to improve image quality and / or lower radiation dose levels beyond those previously achievable with conventional , routine - dose acquisitions , fbp reconstructions [ 12 , 13 ]  . 
for the ultra - lowdose protocols , the assumed effective dose was 0.44msv , which was very low and comparable to the dose used for conventional single plain radiography of the kidneys , ureter , and bladder [ 19 ]  . 
thus , low - dose or ultra - low - dose protocols could potentially contribute toward reducing the lifetime cumulative radiation dose as well as cancer risk [ 2 , 20 ]  . urinary leakage is a challenging , short - term complication that can occur regardless of the surgical approach used and may reduce patients quality of life [ 21 ]  . 
however , although most urine leakages are self - limited , urine leakage - induced complications include infection , metabolic abnormality as a result of intraperitoneal urine reabsorption , and urinoma formation [ 23 , 24 ]  . 
although there have been no previous reports providing definitive criteria for persistent or massive vua urine leakage , some studies have defined anastomotic urine leakage as a persistent daily amount of urine ( over 1500ml ) in the suction drain for more than 6days and for which an invasive interventional procedure had to be performed [ 27 , 28 ]  . 
our findings suggest that the use of ultra - low - dose ct may help to guide treatment and avoid unnecessary procedures in addition to reducing the risks associated with radiation exposure . our study has several limitations . 
moreover , although ultra - low - dose ct cystography was the more accurate modality for determining urine leakage compared to conventional cystography , we cannot rule out the possibility that extravasations outside the urethra or bladder lumen detected by ultra - low - dose ct cystography were not urine leakages . 
nonetheless , to our knowledge , this study is the first to evaluate the accuracy and technical characteristics of ultra - low - dose ct cystography as an optimal modality to track the precise location and amount of urine leakage and limit the radiation dose . 
 these results establish a foundation for future studies and treatments . conclusions ultra - low - dose ct cystography enables accurate evaluation of urine leakage after bladder repair despite the small radiation dose . 
the survey consisted of 11 multiple - choice questions about participants demographics , current local modalities of pic acquisition and storage , perceived advantages and disadvantages of pic dematerialisation over conventional paper - based pic , and overall opinion about pic dematerialisation . results a total of 1791 radiologists ( amounting to 17.4% of active sirm members for the year 2016 ) joined the survey . 
conversely , the need to create dedicated areas for pic acquisition inside each radiological unit ( 64.0% ) and to gain preliminary approval for the use of advanced digital signature tools from patients ( 51.8% ) were seen as potential disadvantages . 
however , concerns were raised that its practical implementation might face hurdles due to its complexity in current real life working conditions . keywords informed consent dematerialisation online survey paperless * lorenzo faggioni lfaggioni@sirm.org 1 department ofexperimental , diagnostic andspecialty medicine , s . 
orsola malpighi university hospital , bologna , italy 2 diagnostic andinterventional radiology , university hospital ofpisa , via paradisa 2 , 56100pisa , italy 3 department ofradiology , university ofcampania l . 
vanvitelli , naples , italy 4 snr foundation , rome , italy 5 uoc radiodiagnostica , aou policlinico vittorio emanuele , catania , italy 6 department ofimaging , asl 3 genovese villa scassi hospital , genoa , italy 7 department ofradiology , usl n . 
bosco hospital , turin , italy 9 department ofinterventional anddiagnostic radiology , arcispedale santanna , ferrara , italy 10 radiology department , universit politecnica delle marche , ancona , italy 11 department ofradiology , candiolo cancer institute , fpo - irccs , candiolo , turin , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 846853 introduction dematerialisation is a complex process involving the development of a digital document flow with full legal value aimed to support and , in perspective , replace conventional document production and archiving for public or private activities [ 112 ]  . 
the advantages of digitisation over paperand film - based workflow in radiology have been widely demonstrated [ 1317 ] , and attempts have since been made to extend the process to administrative key areas of healthcare data management , including , on a national level , the introduction of the digital medical recipe in most italian regions [ 312 ]  . 
however , to our knowledge , no systematic initiatives have been taken so far towards dematerialisation of patients informed consent ( pic ) for diagnostic and interventional radiology procedures , despite incentives from international [ 1 , 2 ] and national government agencies and healthcare institutions to promote digitisation in the public administration as well as in the healthcare system [ 312 ]  . 
such delay is due to the need for dematerialised pic to be formally equivalent to its conventional , paper - based version , implying for it to fully conform to current laws and privacy regulations , ensure proper patients understanding of medical procedures for which written informed consent is required , and provide seamless integration with existing ris / pacs infrastructure at radiological centres [ 18 , 19 ]  . 
while the development of a fully functional programme for pic dematerialisation may pose significant legal and technical challenges , evidence exists in the literature that pic dematerialisation with the aid of portable devices is feasible and as effective or superior to conventional methods in several aspects [ 2024 ]  . the italian society of medical radiology ( sirm ) has promoted the development of guidelines for pic dematerialisation and has put the imaging informatics chapter and informed consent commission of sirm in charge for its implementation . 
in this context , we sought to gain insight about the current modalities of pic acquisition for radiological procedures in italy and the opinion of italian radiologists about pic dematerialisation via an online survey . materials andmethods the online survey was launched as part of an initiative by the imaging informatics chapter of sirm aimed to promote dematerialisation of pic for radiological procedures ( both diagnostic and interventional ) , in cooperation with a number of it firms . 
the survey was devised following suggestions from a multidisciplinary expert panel of sirm and consisted of 11 questions , of which 9 were single choice and 2 multiple choice ( appendix )  . 
a free text field was left at the bottom of each question for additional comments . based upon a similar approach to two previous sirm surveys on teleradiology and radiological structured reporting [ 25 , 26 ] , every single sirm member received a personal email invitation to join the survey via a direct web link from the president of the sirm imaging informatics working group . 
b multiple answers allowed medical directors [ 23.7% ( 423 / 1780 ) ] or consultants [ 16.9% ( 301 / 1780 ) ] , respectively ( question #4 )  . the majority of responders deemed their it skills good [ 67.9% ( 1207 / 1778 ) ] or excellent [ 12.6% ( 224 / 1778 ) ] , whereas a minority declared to have barely sufficient [ 18.7% ( 332 / 1778 ) ] or poor [ 0.8% ( 15 / 1778 ) ] it skills , respectively ( question #5 )  . pic forms were mostly developed locally at each survey participants institution [ 77.0% ( 1311 / 1702 ) ] or , less frequently , by sirm [ 38.5% ( 655 / 1702 ) ] or the health department of each region [ 10.5% ( 180 / 1702 ) ] ( question #6 )  . pic could be revoked by the patient anytime before the examination according to 62.4% ( 1105 / 1772 ) of survey respondents ( question #7 ) , and pic forms were mainly stored in the hospital archive [ 82.7% ( 1428 / 1726 ) ] or , much less frequently , outside of the hospital [ 6.9% ( 119 / 1726 ) ] or were digitally archived into the ris [ 6.8% ( 117 / 1726 ) ] ( question #8 )  . the main advantages of dematerialised pic over conventional , paper - based pic as perceived by the survey respondents ( question #9 ) were its easier and faster recovery [ 96.5% ( 1669 / 1729 ) ] , safer storage and conservation [ 94.5% ( 1643 / 1738 ) ] , reduced cost due to the workflow going paperless [ 90.7% ( 1573 / 1735 ) ] , higher degree of protection in case of medico - legal litigation [ 83.8% ( 1439 / 1717 ) ] , and simplified patient identification and registration [ 74.3% 1 3 la radiologia medica ( 2019 ) 124 : 846853 ( 1274 / 1714 ) ] ( table2 )  . 
this latter circumstance may be due to different factors , including the current lack or inadequacy of technical infrastructures for digital pic collection ( including tablet devices running ad hoc software and connected to dedicated hospital wireless networks ) and / or of integration with existing ris / pacs environments , in spite of substantial investments into dematerialisation by government agencies . 
besides , some features of conventional , paper - based pic acquisition have emerged from the survey that should be incorporated in a dematerialised , digital pic version , including the possibility for patients to revoke their consent anytime before radiological procedures ( question #7 )  . 
in other terms , such basic aspects of conventional pic should be taken into account and preserved in the design and practical implementation of dematerialised pic solutions in order to maintain their legal validity , so that the transition from conventional to dematerialised pic should not substantially alter workflow . 
 furthermore , the current , more frequent usage of pic forms developed locally ( 77.0% of respondents to question #6 ) rather than by regional health departments ( 10.5% ) or , better , national scientific societies such as sirm ( 38.5% ) could be 1 3 la radiologia medica ( 2019 ) 124 : 846853 a potential , yet surmountable hurdle to standardisation and large - scale setup of dematerialised pic tools . 
these latter would actually benefit from the adoption of a single , predefined validated pic model for each radiological procedure , which could also be advantageous for data mining purposes and eventually in case of medico - legal issues [ 2731 ]  . overall , the majority of survey respondents were favourable to pic dematerialisation and acknowledged several advantages of digital over conventional pic , the main ones being easier and faster data retrieval , safer data storage , and reduced running costs . 
in this perspective , tablet - based methods for pic collection have shown to be preferred over conventional pic by both patients and medical staff and has proven more effective at ensuring adequate patients understanding of medical procedures and research trials [ 2024 , 32 , 33 ]  . 
interestingly , our finding of a rate of pic dematerialisation supporters consistently higher than 90% across all age classes of survey participants ( independent of and greater than their self - assessed it skills ) may suggest that radiologists are confident about the usability of digital pic and / or believe that its advantages would outweigh any potential difficulties related to its use as a routine working tool . on the other hand , the main potential drawbacks of pic dematerialisation as pointed out in the survey were related to technical difficulties in carrying out the process in real working environments . 
actually , tablet - based pic acquisition resulted to be more time consuming than paper - based pic collection [ 21 , 24 ] , and earlier work by haller etal . 
 [ 34 ] cautioned against the use of palmtops for electronic data collection in clinical research due to a significant increase in data entry time and risk of typing errors and missing data in comparison with paper - based questionnaires . 
 [ 21 ] found a positive correlation between the duration ofelectronic ipad - based briefings and patient age , paralleled by a negative correlation between patient age and computer skills , but nonetheless the majority of patients would prefer ipad briefings to conventional written informed consent forms in the future . 
even more specifically , it has been suggested that the higher degree of understanding and overall satisfaction provided by tabletbased pic may improve adhesion to clinical trials [ 23 ]  . a limitation of our study is the relatively small number of sirm members joining the survey ( 1791 / 10304 , corresponding to 17.4% of all active sirm members in full standing for the year 2016 ) , which could restrict the validity of our findings to a minority of all members . 
however , the participation rate to our survey was slightly higher than two recent online surveys involving sirm members on teleradiology [ 16.5% ( 1599 / 9662 ) ] [ 25 ] and radiological structured reporting [ 12.1% ( 1159 / 9560 ) ] [ 26 ] , and much higher than a similar european online survey on teleradiology ( 368 radiology professionals from 35 european countries ) [ 35 ] , confirming that pic dematerialisation has gained significant interest within the radiological community . conclusions our findings show that the majority of radiologist members of sirm involved in the survey were favourable to pic dematerialisation . 
though most of them were aware of the potential long - term advantages of pic dematerialisation over conventional , paper - based pic ( mainly related to greater ease , speed , and safety of data collection , storage and retrieval ) , concerns emerged about potential technical and organisational hurdles that its practical implementation may pose , including the need for extra space and time for digital pic collection ( which would add to regular radiologists workload ) , authorisation to use patients advanced digital signature , and to cater for patients who wish to remain anonymous . 
cchf is a life - threatening disease observed endemically over a wide geographical regions in the world , and there is limited information about pulmonary findings in cchf patients . purpose we aimed to investigate the pulmonary findings belonging to a large cchf patient cohort and to determine if there is any relationship between laboratory findings and disease severity . materials and methods a total of 165 patients who were diagnosed with cchf and examined through chest x - ray ( cxr ) due to respiratory symptoms at their first examination and / or during their hospitalization were included in this study . 
the general non - specific symptoms of cchf are fever , malaise , * fatma akta fatmakokcu79@hotmail.com 1 department ofradiology , faculty ofmedicine , gaziosmanpaa university school ofmedicine , 60100tokat , turkey 2 pulmonary diseases department , versa hospital , nevehir , turkey anorexia , nausea / vomiting , and myalgia , which are observed after the contact . 
in addition , intracranial bleeding , gastrointestinal bleeding , and alveolar hemorrhage that are life - threatening and often responsible for mortality can be observed as well [ 14 ]  . 
however , the number of studies related to pulmonary imaging in cchf is very rare and limited despite the increasing number of cases in the world and in our country [ 14 ]  . 
 we may propose simple pulmonary imaging such as cxr to be used within the following 5days after the first examination as an effective tool to evaluate clinical course and severity of the disease . the aim of this study was to investigate the chest x - ray findings of cchf patients with respiratory findings and to determine if there is any relationship between the laboratory findings and severity of the disease . materials andmethods a total of 464 patients with confirmed cchf were admitted to emergency department and department of infectious diseases and clinical microbiology between january 2011 and december 2016 . 
 patients using medicines that may cause pulmonary toxicity and having acute or chronic lung diseases , malignancies , heart diseases , and blood diseases , and a history of thoracic radiotherapy or surgery in addition to cchf were excluded from the study . 
additionally , patients who were clinically diagnosed with pulmonary infection ( such as cough sputum ) and who were diagnosed with other microorganisms in their cultures were not included in the study as well . ethical approval was obtained from ethics committee of the university . 
in addition to demographical findings of the patients such as age , gender , occupation , place of residence , tick exposure , clinical findings , and medical history , laboratory findings and radiological images of lungs were evaluated . 
the cchf diagnosis was made based on the detection of virus genome by using enzyme - linked immunosorbent assay ( elisa ) or polymerase chain reaction ( pcr )  . statistical analysis data are expressed as mean standard deviation . 
 out of 40 patients with comorbidity , 23 were found to have hypertension , three of them had diabetes mellitus , 13 were diagnosed with both hypertension and diabetes mellitus , and one of them had hypothyroids . 
the frequency of general symptoms of the patients observed during the first examination is presented in table2 . based on the laboratory findings , the mean values of liver - specific enzymes such as alkaline phosphatase ( alp ) , alanine aminotransferase ( alt ) , aspartate aminotransferase ( ast ) , gamma - glutamyltransferase ( ggt ) , creatine kinase ( ck ) , and lactate dehydrogenase ( ldh ) were seen to be high . single and / or multiple abnormal imaging findings were detected in 93 patients ( 56.4% ) as a result of cxr examination during the first examination . 
in a similar vein , four patients , claimed to have ground glass densities on cxr , and one patient , claimed to have pleural effusion , were not found to have these findings according to the results of the thorax ct . 
the comparison of survival and cxr findings of patients is shown in table5 . discussion cchf is a life - threatening zoonotic viral disease that can be seen endemically in many regions in the world . 
the most frequent clinical symptoms are fatigue ( 92.3% ) , fever ( 89.4% ) , myalgia ( 69.7% ) , headache ( 68.1% ) , and nausea ( 64.7% ) ; 23% of patients had bleeding ( petechiae , epistaxis , gingival bleeding , vaginal bleeding , and bleeding in internal organs ) [ 10 ]  . 
this situation might be related to the possibility that males work in occupations with high risk of being in contact with ticks . as in many other viral diseases , cchf may cause symptoms of pulmonary involvement and may lead to death . 
the results of the thorax ct revealed that 20 of these patients ( 86% ) had pleural effusion , 12 of them ( 52% ) had consolidation , nine ( 39% ) had atelectasis , and 14 ( 60% ) had 1 3 la radiologia medica ( 2019 ) 124 : 826832 fig . 
however , hemoptysis was detected in a total of nine out of 27 patients with hemorrhage ( six of those patients died )  . there have been a very limited number of studies on pulmonary radiological findings in cchf in the literature . 
however , it has been stated that it can share similarities with mechanism of pulmonary pathologies such as pleural effusion , pneumonitis , hemoptysis , and alveolar hemorrhage in other febrile viral hemorrhagic diseases [ 15 , 16 ]  . 
in a study performed on dengue hemorrhagic fever , a total of 468 cxr taken from 363 patients were examined and parenchymal infiltration and pleural effusion were observed in more than half of the patients on the third day of follow - up . 
 moreover , these radiological findings were found to be closely related to laboratory findings of leukocyte count , platelet count , aptt , alt , and albumin levels in the same study [ 18 ]  . 
 in conclusion , pleural effusion and other findings related to pulmonary involvement can be seen in cchf due to endothelial damage caused by viral load in the circulation , increased capillary permeability , and hemorrhages due to low platelet . in the study by akta etal . 
the results of the study revealed that there was no statistically significant difference between the two examination techniques in terms of detecting parenchymal infiltration , alveolar infiltration , and pleural effusion . 
when these patients were compared , it was found that there was consolidation in cxr of the four patients and pleural effusion in one patient while they were not observed in thorax ct . 
on the other hand , based on thorax ct results , ground glass density was detected in four patients and atelectasis in two patients , and these were not observed in cxr . 
therefore , there was a possibility of response to the treatment and spontaneous regression or progression in the findings . the mortality rate of cchf generally ranges from 2 to 80% . 
this result can be associated with the fact that cchf is endemic in this region ; therefore , medical staff and people are informed about the disease , and thus , they are alert . 
in addition , the experience in the clinical follow - up might also contribute to the decrease in mortality rate besides improvements in medical care conditions in cchf and increase in awareness of the seriousness of the disease . it is known that mortality and some laboratory parameters prolonged a ptt , increased inr , high alt , ast and ldh , low platelet , and increased leukocyte are related to each other [ 23 , 24 ]  . 
for this reason , all of the cchf patients who were found to have pathologic cxr result should be considered at high risk . our choice to conduct a retrospective study is the first limitation ; on the other hand , medical information of the patients and their radiological images has been recorded in a proper way . 
the other limitation was the inability to confirm the cxr findings of the patients as not all of these patients had thorax ct . in conclusion , cchf is a serious public health problem that can be fatal . 
according to the results of our study , we suggest that 1 3 832 la radiologia medica ( 2019 ) 124 : 826832 radiological imaging of pulmonary system should be performed primarily with cxr . 
pulmonary involvement ( pleural effusion , consolidation , and ground glass opacity ) affects the survival in cchf negatively , and further examination should be performed with thorax ct in case of necessity . 
the association between findings was assessed using fishers exact test , while correlation at ct scan was evaluated with the spearman analysis . results bronchiectasis / bronchioloectasis ( 89.8% ) , nodule ( s ) ( 81.6% ) , tree - in - bud ( tib ) , and consolidation ( 79.6% each ) figured among the most common parenchymal findings . 
2 , university offlorence , azienda ospedaliero - universitaria careggi , largo brambilla 3 , 50134florence , italy 2 rheumatology unit , department ofexperimental andclinical medicine , university offlorence , azienda ospedaliero - universitaria careggi , 50134florence , italy infectious diseases unit , department ofexperimental andclinical medicine , university offlorence , 50134florence , italy infectious andtropical diseases unit , azienda ospedaliero - universitaria careggi , 50134florence , italy 5 department ofhealth science , university offlorence , viale g.b. 
morgagni 48 , 50134florence , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 838845 introduction tuberculosis ( tb ) continues to be a public health concern in many european countries , despite the remarkable progress made in the last decade with respect to diagnosis and treatment availability . 
in many non - european countries , the prevalence of tb is still high , even in the multi - drug - resistant foreuropean countries , such as italy , have a high number of cases , especially among groups of vulnerable populations , such as immigrants and people co - infected with hiv [ 1 , 2 ]  . 
 the presence of immigrants from high - endemic areas is considered by many authors as one of the main reasons for the recent spurt in the number of tb patients in italy . 
to avoid misunderstanding the description of the epidemiological picture , it needs to be specified that a foreign - born population does not contribute significantly to the transmission of infection to the native population [ 6 ]  . tuberculosis is often diagnosed late , many times after the onset of the symptoms , and can involve any organ , with variable manifestations . 
although laboratory tests are essential , a radiological analysis can aid clinicians in the diagnosis , allowing the early start of infection control measures ( airborne precautions ) , that can be discontinued only when ( 1 ) another diagnosis explains the clinical signs and / or tb disease is considered unlikely ; ( 2 ) patient has three negative afb sputum smear results [ 7 ]  . while symptoms and physical findings can be nonspecific , specific signs of tb can be identified using radiological techniques . 
a computed tomography ( ct ) of the chest increases the specificity of the diagnosis , better showing distinct findings such as ground glass opacity ( ggo ) and tree - in - bud ( tib ) , and may be helpful , particularly when the x - ray does not show typical findings associated with tb ( cavities , consolidations , calcifications , etc . ) [ 8 , 9 ]  . against this backdrop , after observing a series of pulmonary tb patients until their healing , we propose this retrospective study to identify the most frequent radiological findings , to determine those with the highest degree of association , and to identify the most suggestive radiological findings for acid - fast bacilli ( afb ) positive disease . materials andmethods patients andstudy design we retrospectively reviewed the medical records of patients admitted to the infectious and tropical diseases unit at azienda ospedaliero - universitaria ( aou ) careggi ( florence , italy ) between 2014 and 2016 . 
on 28 may 2018 , the study obtained the approval of the local ethics committee ( protocol #12819 )  . all patients had provided their written informed consent for submission of their chest ct and , if necessary , of an iodinated contrast agent , according to the principles of the declaration of helsinki . 
tuberculosis ; hospitalization at other hospitals ; diagnosis of disease with primary or secondary pulmonary involvement due to other comorbidities ( cystic fibrosis , primary ciliary dyskinesia , autoimmune diseases ) ; diagnosis of respiratory tb in the absence of pulmonary involvement ; chest ct performed at a radiological service other than aou careggi . from january 2014 to december 2016 , 191 patients were admitted with a generic diagnosis of mycobacterial infection to the infectious and tropical diseases unit of aou careggi , and 127 of these patients were infected with m . 
only 109 showed pulmonary involvement , 102 of them didnt show comorbidities ( 5 had previously received a diagnosis of autoimmune disease and 2 had previously received a diagnosis of cystic fibrosis ) , 54 of whom executed a chest ct during diagnosis at one of the aou careggi radiological services . 
five patients were excluded from the study because of incomplete clinical data ( 2 ) , ct imaging of low quality ( 2 ) , and absence of dicom files of ct scans ( 1 )  . 
medical records provided the following data : ( 1 ) demographic data ( age , sex , nationality , time of permanence in italy ) ; ( 2 ) signs and symptoms before hospitalization ( asthenia , chest pain , cough , dyspnea , fever , haemoptysis , hyporexia , night sweating , weight loss ) ; ( 3 ) laboratory data ( leucocyte count , neutrophils percentage , c - reactive protein ) ; ( 4 ) microbiological data ( afb stain , culture methods , gene amplification test performed on sputum and , if present , on bronchoalveolar lavage )  . 1 3 840 la radiologia medica ( 2019 ) 124 : 838845 all ct scans in dicom were evaluated in consensus by two expert radiologists , vs and lm ( 5 and 7years of experience , respectively )  . 
a third evaluation was performed by sc ( 30years of experience ) , when the opinions differed . the observers checked for the presence or the absence of 10 parenchymal ct findings , as reported in the third paragraph : ( 1 ) bronchiectasis and bronchioloectasis ; ( 2 ) bulla ; ( 3 ) calcification ( s ) ; ( 4 ) cavity ; ( 5 ) consolidation ; ( 6 ) ggo ; ( 7 ) micronodule ( s ) ; ( 8 ) nodule ( s ) ; ( 9 ) serous reaction ; and ( 10 ) tib . 
they also looked for the presence or the absence of four mediastinal lymph node findings , as reported later : ( 1 ) calcification ( s ) ; ( 2 ) cavity ; ( 3 ) colliquation ; and ( 4 ) lymphadenopathy . hence , we defined the association between various findings as a pattern and calculated the degree of correlation among parenchymal findings . we then studied the prevalence of each finding in the entire sample and in the afb stain - positive subgroup , looking for findings that strongly correlated with positivity , to identify patterns that could predict afb positivity , and vice versa . it should be underlined that in the last years , the radiological difference between primary and post - primary tb has been questioned . 
many evidences show that the radiographic appearance of pulmonary tb does not depend on the time since infection , and other factors , like the immunocompetence of the host , can condition it [ 10 ]  . 
so , we avoided to differentiate patients in the two categories primary and post - primary tb . imaging studies helical multiphasic ct was performed on 49 patients using somatom plus volume zoom 4 ( siemens medical solutions ) unit with 37 - mm contiguous sections . 
the routine ct protocol comprised volumetric end - inspiratory and end - expiratory low - dose scans in a 16or 64 - row scanner ( somatom sensation , siemens , erlangen , germany ) , using the following parameters : 120kv for patients 35kg , 100kv for patients < 35kg , mas 1540 , 0 , 6mm collimation , slice thickness 2mm , reconstruction increment 0.8mm , pitch 1 , kernel b30 . 
ct scans were evaluated for the presence of the following 10 signs , as defined by the fleischner society [ 11 ] : bronchiectasis this refers to irreversible localized or diffuse bronchial dilatation . 
morphological criteria on thinsection ct scans include bronchial dilatation with regard to the accompanying pulmonary artery , lack of tapering of bronchi , and the identification of bronchi within 1cm of the pleural surface . bronchioloectasis it is the dilatation of bronchioles . 
 when dilated bronchioles are filled with exudate and are thick - walled , they are visible as a tib or as centrilobular nodules . bulla an airspace measuring more than 1cm in diameter sharply demarcated by a thin wall no greater than 1mm in thickness . 
it appears as a rounded focal lucency or an area of decreased attenuation , 1cm or more in diameter , bounded by a thin wall . calcification this refers to a zone of lung parenchyma with a very high attenuation value . cavity it is a gas - filled space , seen as a lucency or lowattenuation area , within pulmonary consolidation , a mass , or a nodule . consolidation it refers to an exudate or other product of a disease that replaces alveolar air , rendering the lung solid . 
it appears as a homogeneous increase in pulmonary parenchymal attenuation , which obscures the margins of vessels and airway walls . ggo it appears as hazy increased opacity , with preservation of bronchial and vascular margins . lymphadenopathy it is a lymph node with a short axis greater than 1cm . micronodule it refers to a discrete , small , round , focal opacity , with a diameter less than 3mm . nodule it is a rounded or irregular opacity , well or poorly defined , measuring up to 3cm in diameter . serous reaction the term serous reaction refers to all the findings that prove an involvement of serous membranes : pachypleuritis , pericardial effusion , pleural effusion , pleural empyema , and pleural thickening . tib it refers to multiple areas of centri - lobular nodules with a linear branching pattern that resembles a budding tree . 
it reflects a spectrum of endoand peribronchiolar disorders , including mucoid impaction , inflammation , and / or fibrosis . statistics in our study , data were presented in percentage terms . 
the association between suggestive findings for a transmissible disease ( scored positive or negative at afb stain ) and each ct scan finding ( yes or no ) was assessed using fishers exact test . 
the variables with significant association with afb positivity were entered into a multivariate logistic regression model , considering , as dependent variable , the afb positivity ( 1 for positive results , 0 for negative results )  . 
 among the 39 foreign patients ( 7 , 8 , 10 , and 14 , from africa , asia , south america , and eastern europe , in that order ) , only five ( 12.8% ) had been in italy for less than 1year , eight ( 20.5% ) from 1 to 5years , and 26 ( 66.7% ) for more than 5years . 
tuberculosis ( n = 64 ) excluded : absence of pulmonary involvement ( n = 18 ) excluded : presence of comorbidities ( n = 7 ) excluded : ct scan not performed ( n = 48 ) excluded : lack of data ( n = 5 ) patients infected by mycobacterium tuberculosis ( n = 127 ) patients with pulmonary involvement ( n = 109 ) patients without comorbitidies ( n = 102 ) patients that have performed a ct scan at diagnosis ( n = 54 ) enrolled patients ( n = 49 ) 1 3 842 la radiologia medica ( 2019 ) 124 : 838845 bulla serous reaction calcification ground glass opacity micronodule cavity tree - in - bud consolidation nodule bronchi ( olo ) ectasis cavity colliquation calcification limphadenopathy fig . 
2 frequency of parenchymal and nodal finding ( s ) nodule ( s ) and ggo ( r = 0.488 ; p < 0.05 ) bronchi ( olo ) ectasis and cavity ( r = 0.465 ; p < 0.05 ) tib and micronodule ( s ) ( r = 0.464 ; p < 0.05 ) tib and ggo ( r = 0.428 ; p < 0.05 ) nodule ( s ) and micronodule ( s ) ( r = 0.400 ; p < 0.05 ) high correlation involved only the seven most frequent parenchymal findings ( see fig.2 ) ; no nodal finding showed high correlation . 
no patient showed all the 10 parenchymal findings . radiological findings inafbpositive patients we found that only three findings ( consolidation , tib , cavity , p < 0.05 ) have a positive predictive value for afb stain , as shown in table1 . 
consolidation , tib , and cavity can be seen as a pattern , the only one with a positive predictive value of 100% if all three were detected together ( 25 , 60 and 77.8% if zero , one or two of them were present , respectively )  . consolidation , tib , cavity and serous reaction were included in the first multivariate logistic regression model as independent variables . 
serous reactions might indicate afb stain negativity bold values represent a significantvalue discussion as far as we know , our series is the only recent one that examined the radiological features of pulmonary tb in a low - incidence area . 
however , there are some findings which are more frequent , such as bronchi ( olo ) ectasis , nodule ( s ) , tib , and consolidation ( fig.3 ) , found in 44 , 40 , 39 , and 39 patients , respectively . 
other associations showed a contradictory positive predictive value , as that one among the four findings bronchi ( olo ) ectasis , nodule , micronodule and ggo , which demonstrated a positive predictive value of 95.7% if all four findings were present , but also conflicting values of 75% versus 71.4% if one or two of them were present , respectively . 
however , we believe this is a statistical result with no clinical meaning , since 65% of the subjects that do not have a serous reaction are afb positive as well . 
ct scans show scattered bronchiectasis ( arrows ) and tib in both lungs ( a ) and in the rear portion of both lungs ( b ) 1 3 844 la radiologia medica ( 2019 ) 124 : 838845 which is reported in 61% of our patients . 
in the literature , however , this frequency ranges from high values ( 7695% ) [ 1416 , 18 ] to low values ( 312% ) [ 2024 ]  . 
 for other frequent findingsnodule , consolidation , and tibour percentages do not significantly differ from the majority of data present in the literature , which shows , for example , the frequency of consolidation ranging from 54.7 to 96% [ 1519 , 2127 ]  . from an epidemiological point of view , our study population is mainly represented by foreign patients ( 39 of 49 ) , most of whom lived in italy for more than 5years . 
this confirmed that , despite the reduction in italian native population , the presence of migrants from high - endemic areas is one of the main causes of a stable incidence rate of tb cases ( approximately six per 100 , 000 inhabitants ) [ 4 ] , even if it does not contribute to infect the native population [ 6 ]  . the present study is not without limitations . 
nevertheless , the aim of the present study was to identify the most frequent findings with a view to examining them in a future prospective study . third , our report lacks inter - observer correlation index , because we adopted consensus evaluation . 
the application of an inter - observer correlation index in only 49 patients should have been not so confident between the two readers . finally , information about chronic obstructive pulmonary disease and smoking habit is not reported because the data is discontinuously acquired . 
however , since the average age is 40years , the induced risk is not so high . in conclusion , our data confirm ( 1 ) extreme heterogeneity of pulmonary tb while also revealing that no finding or pattern is clearly prevalent over others or unique to the disease . 
 ( 2 ) there are couples of findings ( tib and cavity ; tib and bronchi ( olo ) ectasis ; tib and consolidation ; nodule ( s ) and ggo ; bronchi ( olo ) ectasis and cavity ) with high correlation , which can help us to make the right diagnosis . 
 ( 3 ) although we identify a triad ( tib , cavity , and consolidation ) that strongly predicts afb positivity , we have not found any predictive sign of afb negativity . 
 ct scan shows in the left lower lobe a cavity of cm 4.20 ( asterisk ) surrounded by tib , and in the left upper lobe a consolidation ( arrowhead )  . 
moreover , in the right lung ct shows scattered bronchiectasis ( arrow ) for afb , but also 82% of patients without calcification ( s ) were positive for afb . 
this confirms that microbiological examination continues to be crucial for tb diagnosis . in our series , bronchi ( olo ) ectasis was the most represented finding , which is clearly not of the case with pulmonary tb . 
however , after having excluded the presence of other primary causes of bronchiectasis ( cystic fibrosis , primary ciliary dyskinesia , and autoimmune diseases ) , the correlation we found between bronchi ( olo ) ectasis and cavity ( r = 0.465 ; p < 0.05 ) could have a new meaning . 
in fact , these strong correlations and those between tib - cavity ( r = 0.577 ; p < 0.05 ) , tib - bronchi ( olo ) ectasis ( r = 0.498 ; p < 0.05 ) , and tib - consolidation ( r = 0.497 ; p < 0.05 ) suggest a unique pathogenetic path that was previously reported in the literature [ 12 ]  . 
accordingly , tib indicates mainly an endobronchial diffusion of the disease , but is recognized in a large number of conditions as diffuse panbronchiolitis and cystic fibrosis ; bronchiectasis is an expression of both bronchial wall malacia and chronic disease [ 11 , 13 ]  . 
the latter leads to parenchymal inflammation , consolidation , and ultimately , to cavity . some of the frequency values detected by us ( see the results section ) lack a precise confirmation in the literature . 
in the literature , the frequency values of bronchiectasis sensu stricto in tb patients range from 64% [ 18 ] and 89.3% [ 19 ] ( high frequency ) to 5% 14.3% [ 20 ] , 21% [ 21 ] , and 29% [ 22 ] ( low frequency )  . 
we can notice a similar trend with ggo , 1 3 la radiologia medica ( 2019 ) 124 : 838845 compliance with ethical standards conflict of interest all authors declare that they do not have conflict of interest . ethical standards this article does not contain any studies with animals performed by any of the authors . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
on 28 may 2018 , the study obtained the approval of the local ethics committee ( protocol #12819 )  . informed consent informed consent was obtained from all individual participants included in the study . 
all patients had provided their written informed consent for submission of their chest ct and , if necessary , of an iodinated contrast agent , according to the principles of the declaration of helsinki . 
cisplatin concomitant chemotherapy was administered during imrt . results fourteen patients with cervical cancer were prospectively recruited between august 2014 and june 2017 , 13 ( 93% ) had a lacc , one ( 7% ) patient was not evaluable because 18fdg - pet / ct evidenced metastases to the liver undetected by previous ct / mri . 
imrt median dose to the pelvis was 48.6gy in 27 fractions , sib median dose 54gy in 27 fractions , hdr - bt boost median dose 21gy in 3 fractions . 
there were no grade 4 acute and / or late toxicities . conclusions the 18fdg - pet / ct influenced stage assessment and rt treatment planning due to its high specificity in distant metastases and nodal involvement detection . 
maria hospital , terni , italy vol . : ( 0123456789 ) 1 3 820 introduction cervical cancer remains the third most common malignancy worldwide and up to half of patients present with locally advance disease even if screening and prevention are improved [ 1 ]  . 
since 1999 exclusive concomitant radiotherapy ( rt ) plus chemotherapy is the standard treatment for locally advance cervical cancer ( lacc ) , and 5 - year overall survival ( os ) rate is near 70% [ 2 ]  . 
literature data show that 18fdg - pet / ct has a higher sensitivity than ct and magnetic resonance imaging ( mri ) , not only in detecting occult metastasis but also nodal involvement , while mri remains the best imaging technique to evaluate local tumor extension [ 4 , 5 ]  . 
therefore , 18fdg - pet / ct can influence the staging of cervical cancer and resulting therapeutic decision , particularly for rt field extension and dose to administer to involved lymph nodes [ 5 ]  . 
few experiences in literature evaluated outcome of 18fdgpet / ct based treatment plan and the use of simultaneous integrated boost ( sib ) for treatment of lacc [ 3 , 69 ]  . in clinical practice , a sib associated to conventional fractionation rt , is used with the aim to increase rt total dose to the tumor without increasing total treatment time . 
 moreover , overall treatment time of rt is crucial for the results because it has been shown that lc and os decrease by about 1% per day when time to rt exceeds 8weeks [ 1012 ]  . 
the influence of 18fdg - pet / ct for diagnosis and treatment decision were also discussed . materials andmethods patients with lacc diagnosed with 18fdg - pet / ct and enrolled between august 2014 and june 2017 were prospectively evaluated after definitive chemo - radiotherapy . 
 a concomitant weekly cisplatin ( 40mg / sq ) and subsequent three - dimensional - high - dose - rate brachytherapy la radiologia medica ( 2019 ) 124 : 819825 ( hdr - bt ) boost to the primary tumor were administered . 
the imrt was delivered with a ct - based planning system of the 18fdg - pet / ct , and it was done in supine position with empty rectum and filled bladder . 
 low dose ct was used for attenuation correction . the clinical target volume ( ctv ) included the entire uterus , vagina based on disease extension , lower common iliac , external and internal iliac , obturator and presacral nodes . 
for imrt , ctv was defined by a 7mm expansion of nodal regions with subtraction of the pelvic bones , femoral heads and vertebral bodies , then a margin of generally 5mm in all directions was added to ctv to obtain planning treatment volume ( ptv )  . 
based on the institutional set - up verification protocols , for the first 3days of treatment , patients position was verify by kv cone beam ct system integrated in the machine . 
then any variation of set - up was checked once a week . for hdr - bt , a ct - based planning was performed using a single uterine fletchers applicator and two vaginal ovoids , then a ct was done each fraction to verify appropriateness of placement . 
the brachytherapy ctv included disease volume based on clinical and mri evaluation done at the end of imrt and on viswanathan guidelines [ 14 ] ; prescription and optimization were performed on ctv based on uterine size , configuration and disease location . 
treatment plans were 1 3 la radiologia medica ( 2019 ) 124 : 819825 generated on the plato brachytherapy planning system , version 14.2.6 ( nucletron ) or oncentra brachytherapy planning system , version 4.1.2. the hdr - bt was administered 3 times a week , fractionation schemes were selected taking into account equivalent dose , quantec organs at risk ( oar ) constrains , patient compliance and previous imrt dose [ 15 , 16 ]  . 
treatment planning parameters adopted for hdr - bt were those of the american brachytherapy society [ 15 ]  . for combined treatment , cumulative dose ( i.e. , imrt plus hdr - bt ) was calculated with an / ratio of 10 for ctv ; for tolerance dose concerning late effects , an / ratio of 3 was used in the calculation of the equivalent dose in 2 - gy fraction to oar [ 17 ]  . for each patient , an informed consent was obtained both for imrt and hdr - bt according to the rules of our institution . response was assessed 12 months after the end of treatment with physical and mri exams . 
further follow - up was done using clinical and mri exams every 34months for first 2years , then every 6months ; ct was performed every 6months and 18fdg - pet / ct only when there was a suspicious of progression or relapse . in accord with the response evaluation criteria in solid tumors [ 18 ] , complete response ( cr ) was defined as complete resolution of enhancing lesion , partial response ( pr ) , 30% decrease in size of the lesion , progression of disease ( pd ) , > 20% increase in size of the lesion , and stable disease ( sd ) , no change in dimension of the lesion or does not meet criteria for cr , pr or pd . 
local relapse was defined as failure inside the rt fields in patients with local control and distant relapse as a failure outside rt fields . common terminology criteria for adverse events version 4.03 was used to grade toxicity . 
statistical analysis was performed using a software package ( medcalc 11.1 broekstraat 52 , b - 9030 mariakerke belgium ) and the kaplanmeier product - limit method [ 19 ]  . 
a value of p < 0.05 ( two tailed ) was considered statistically significant . results fourteen patients with cervical cancer treated at two italian centres ( terni and ancona , 8 and 6 cases , respectively ) were prospectively assessed . 
there were 13 of 14 patients evaluable for all study endpoints ; one ( 7% ) patient was not evaluable because 18fdg - pet / ct evidenced metastases to the liver undetected by previous ct / mri . 
apart from this case , 18fdg - pet / ct changed the stage derived from ct / mri findings , in other 7 ( 50% ) patients in which a more extensive disease due to nodal involvement was evidenced . 
 so , after 18fdg - pet / ct we modified treatment volume in these 7 patients . with respect to ct / mri findings , 18fdg - pet / ct changed local tumor extension in no case . 
clinical stage was as follows : apart from patient with liver metastasis , the other 13 patients were in figo stage iia , iib , iiib , iva and ivb in 1 , 6 , 2 , 1 and 3 cases , respectively . 
it is worth of note that 11 patients had nodal involvement , pelvic and / or lumbo - aortic in 8 and 3 cases , respectively . all patients underwent imrt to the primary tumor and pelvic draining lymph nodes , 3 of 13 ( 23% ) patients were treated also on para - aortic region . 
median total treatment time was 7weeks ( range , 616weeks ) , 2 patients temporary interrupted imrt for haematological grade ( g ) 3 and gastrointestinal g2 toxicity , respectively . after a median follow - up of 30months ( range , 641 ) , all patients were alive , 9 ( 69% ) without disease , 3 ( 23% ) with metastatic disease but no local relapse , and 1 ( 8% ) patient maintained her pr . 
at first control after treatment , 12 ( 92% ) of 13 patients obtained clinical and radiological cr , and one 1 3 822 la radiologia medica ( 2019 ) 124 : 819825 ( 8% ) a pr . 
2 distant control probability 1 3 la radiologia medica ( 2019 ) 124 : 819825 such as age , histology , stage and dose were assessed and had no prognostic impact . regarding acute toxicity , g1 - 2 nausea was registered in 3 ( 23% ) cases , g2 dysuria in 2 ( 16% ) , g2 proctitis in 3 ( 23% ) , g1 - 2 diarrhea in 3 ( 23% ) , g3 neutropenia in 3 ( 231% ) and g3 thrombocytopenia in 1 ( 8% ) patient ( table1 )  . generally , chemo - radiotherapy resulted feasible : 10 of 13 ( 77% ) patients completed treatment as planned , 3 ( 23% ) had iatrogenic toxicity . 
in 1 patient with acute grade 3 neutropenia and g2 diarrhea , chemotherapy was stopped after the fourth cycle and rt temporary interrupted ; in another case , chemo - radiotherapy was temporary interrupted for g3 neutropenia and thrombocytopenia ; 1 patient with grade 2 diarrhea interrupted treatment for 5days ( table1 )  . 
regarding late toxicity , g1 vaginal stenosis was found in 1 ( 8% ) case , g1 hematuria and dyspareunia in 1 ( 8% ) , and g3 rectal bleeding in 1 ( 8% ) patient . 
no g4 toxicity was registered ( table1 )  . discussion recently 18fdg - pet / ct has become an interesting modality for staging , re - staging and assessing response to therapy in lacc management . 
this exam , resulting from a combination of metabolic pet information and anatomic ct images , can be more accurate than ct or mri in detecting regional lymph node involvement and extra - pelvic disease [ 5 ]  . 
lymph node status , though not included in the figo system , is an important prognostic factor which should be considered in the therapeutic strategy [ 3 , 5 , 6 ]  . 
although mri remains the best imaging technique to evaluate local tumor extension , several data have shown that 18fdg - pet / ct has a higher sensitivity with respect to ct and mri , not only in detecting occult metastases ( 95% ) but also nodal involvement ( 100% ) [ 4 , 5 , 9 ]  . 
in clinical practice , 18fdg - pet / ct staging altered lacc management in a population variable from 18% to 44% by changing treatment strategy from surgery to chemo - radiotherapy or palliation . 
moreover , rt planning can be influenced by 18fdg - pet / ct imaging both in defining field extension and in prescribing higher doses to involved lymph nodes [ 5 , 9 , 20 ]  . our series confirmed these indications . 
in fact , 18fdgpet / ct changed the stage derived from ct / mri findings , in 8 of 14 ( 57% ) patients in which a more extensive disease due to nodal involvement ( 7 cases ) or metastatic disease ( 1 case ) was evidenced , and did not change local tumor extension assessed by mri . 
so , in the 7 patients with an evidence of nodal disease unidentified at ct / mri , ctv was enlarged to encompass nodal metastases which received also a higher dose using the sib technique . in our experience this discrepancy between 18fdg - pet / ct and ct / mri is higher with respect to literature data [ 5 , 9 , 20 ]  . 
a possible explication of this discrepancy is the prevalence of advanced figo stage in our patients and the consequent higher probability of nodal and / or metastatic involvement . in clinical practice the planning with 18fdg - pet / ct is uncommon . 
however , patients have a long follow - up ( median 30months ) and pet / ct did change figo stage and treatment approach in 57% ( 8 of 14 ) of cases . 
so , our study , although suboptimal for the paucity and inhomogeneity of patients recruited , can result of some interest considering the role of 18fdg - pet / ct in changing not only the stage and therapeutic strategy , but also in better defining imrt targets in lacc . our patients underwent 18fdg - pet / ct in rt treatment position to have a more precise sib - ctv contour and to reduce set - up error probability . 
as in other published similar series of 18fdg - pet / ct simulation , for sib - ctv a margin of only 5mm was done to obtain sib - ptv [ 21 ]  . 
 when 18fdg - pet / ct was available only for staging and not for rt simulation , margins between ctv and ptv were generally > 5mm [ 3 , 8 , 9 ]  . 
this difference in size of expansion is very important because can condition the table 1 acute and late toxicities registered with common terminology criteria for adverse events version 4.03 scale entity upper gastro - enteric ( nausea / diarrhea ) lower gastro - enteric ( proctitis / rectal bleeding ) genito - urinary ( dysuria / vaginal stenosis / dyspareunia ) hematologic ( neutropenia / thrombocytopenia ) acute ( % ) late ( % ) acute ( % ) late ( % ) acute ( % ) late ( % ) acute ( % ) late ( % ) grade 1 grade 2 grade 3 grade 4 1 3 824 la radiologia medica ( 2019 ) 124 : 819825 appearance of iatrogenic toxicity . 
in fact , the tighter is tumor margin the lesser is expected toxicity to surrounding healthy tissues . the administration of a boost dose to positive lymph nodes by sib is a modern technique which allows to increase total dose without increasing total treatment time and toxicity [ 13 , 22 , 23 ]  . 
with 30months of median follow - up , our 86% of lc rate at 3years was similar to vargos experience in which lc and regional control rates at 3years were 76% and 94% , respectively [ 3 ]  . 
in another paper , local and pelvic control rates were > 90% but number of patients was limited and median follow - up of only 9months [ 13 ]  . the 67% of dc probability at 3years was quite inferior to literature data where it results between 77 and 90% [ 3 , 6 ]  . 
 nevertheless , only 3 ( 23% ) patients had local or distant progression , compliance to the treatment was very high , and toxicity acceptable considering that all patients completed scheduled treatment . although our prospective study had recruited a relatively small number of patients , follow up is quite long and standardized 18fdg - pet / ct was used for rt simulation and imrt / sib administration according to the best modern concept of diagnosis and treatment of lacc . 
the aim of this study is to calculate the accuracy of chest computed tomography to detect surgically resectable blebs or bullae in patients with primary spontaneous pneumothorax . methods this is a retrospective study includes all patients with primary spontaneous pneumothorax who underwent chest computed tomography evaluation for their disease over the period from january 2005 to december 2015 . 
patients who underwent surgical exploration were sub - grouped to calculate the sensitivity and the specificity of the chest computed tomography to detect surgically resectable pulmonary blebs or bullae . results a total of 143 patients were included in the study . 
therefore , the routine use of chest computed tomography scan before the surgical exploration in patients with primary spontaneous pneumothorax should depend on the clinical judgment . keywords blebs bullae computed tomography primary spontaneous pneumothorax introduction spontaneous pneumothorax is usually classified into primary and secondary types . 
while the primary type occurs without the presence of underlying lung disorder , the secondary one occurs when the lung has a disorder leading to the formation of cystic cavities [ 1 ]  . although the patients with primary spontaneous pneumothorax ( psp ) have no obvious lung disease , abnormalities in the visceral pleura such as blebs or bullae are usually present . 
the intuitional review board approves this study on february 9 , 2017 , with the number irb - 2017 - 01 - 017 . the study includes all patients with psp who underwent chest ct evaluation during their admission . 
the chest ct in this study was a highresolution non - contrast - enhanced ct of the chest with 64 - row mdct ( somatom definition , siemens healthcare sector ; forchheim , germany ) using a standardized chest ct protocol with the following parameters : collimation : 32 2 0.6mm ; weight - adapted selection of the tube voltage for both tubes ( ranging between 100 and 120kv ) with adapted tube current setting ( ranging between 90 and 100 effective mas ) ; 4d dose modulation ( care dose 4d ) ; pitch : 3 ; rotation time : 0.28s. 
all patients underwent ct scan examinations in the supine position and were required to hold their breath at full inspiration . ct images of 1 - mm slice thickness for 2 - mm intervals in the lung parenchyma in axial and coronal [ window level : 600 hu ; window width : 1500 hu ] were used for analysis . all images were displayed using a picture archiving and communication system ( pacs ) workstation ( syngo.plaza. siemens healthcare sector , erlangen , germany )  . the diagnosis of psp was confirmed by reviewing the patients initial chest x - ray and charts . 
all chest ct la radiologia medica ( 2019 ) 124 : 833837 examinations of the patients were reviewed by one expert radiologist looking for the presence of ipsilateral and contralateral blebs or bullae and the presence of other abnormalities in the lung or pleura . 
 the surgical management includes intercostal chest tube drainage of the pneumothorax that may be followed by surgical exploration of the pleural cavity depending on the patient response to the drainage procedure . 
the recurrence rate of psp is lower in the operated patients whether they were operated after the first or the second episode of psp as the surgical intervention reduces the risk of recurrence [ 5 ]  . 
moreover , the surgical intervention reduces the length of hospital stay as the operated patients usually require three hospitalstay days , while it requires about five to seven days for the conservative management patients . 
1 high - resolution computed tomography of the chest , coronal ( a ) and axial cuts ( b , c ) : left pneumothorax , red arrows ( b , c )  . 
2 an algorithm of the study sample 174 patients 143 patients 31 patients excluded as they dont have chest ct evaluation 23 patients underwent only drainage procedure 120 patients underwent surgical exploration taken as a subgroup to determine the sensitivity if chest ct scan in detecting surgically resectable blebs or bullae table 1 chest computed tomography finding of 143 patients with primary spontaneous pneumothorax number of patients ( % ) table 2 2 2 table correlates the chest computed tomography finding to the surgical exploration finding of 120 patients with primary spontaneous pneumothorax chest computed tomography findings of pulmonary blebs or bullae surgical findings of resectable pulmonary blebs or bullae total finding pneumothorax side right left pulmonary blebs ipsilateral contralateral pulmonary bullae ipsilateral contralateral 70 ( 49.0% ) 73 ( 51.0% ) 119 ( 83.2% ) 103 ( 72.0% ) 32 ( 22.4% ) 21 ( 14.7% ) total surgery looking for pulmonary blebs or bullae for resection with or without the use of pleurodesis . 
the patient who underwent surgical exploration was taken as a sample to determine the sensitivity and the specificity of chest ct scan in detecting surgically resectable blebs or bullae . statistical analysis of the sample was carried using statistical package for the social sciences version 21 ( ibm corp . , armonk , ny , usa )  . 
out of the 94 patients who found to surgically resectable pulmonary blebs or bullae , the chest ct scan could detect the pulmonary blebs or bullae in 90 patients of them with a calculated sensitivity of 95.7%. 
on the other hand , 11 patients have a negative chest ct scan among the 26 patients who did not found to have surgically resectable pulmonary blebs or bullae with a calculated specificity of 42.3%. 
most of the samples are males ( n = 141 , 98.6% ) with a mean age of 24 6.2years. through evaluation of the chest ct scan of the patients , 119 patients ( 83.2% ) have ipsilateral blebs and 32 patients ( 22.3% ) have ipsilateral bullae . 
contralateral blebs were present in 103 patients ( 72.0% ) and contralateral bullae were present in 21 patients ( 14.7% ) ( table1 )  . psp occurs usually in males who are smokers , tall , and thin [ 4 ]  . 
chest x - ray can also detect abnormalities in the pleura that may have an effect on the recurrence rate [ 7 ]  . chest ct scan is an evolving method that is commonly used for psp to detect the presence of abnormalities in the lung or pleural cavity , mainly the presence of pulmonary 1 3 836 la radiologia medica ( 2019 ) 124 : 833837 blebs or bullae [ 8 ]  . 
the sensitivity of the chest ct scan to detect those changes is increased when the ct scan that is used is high resolution with thin slice and reviewing both the axial and coronal view [ 9 , 10 ]  . 
 moreover , chest ct scan can show abnormalities in the pattern of the thorax that is commonly found in patients with psp as they tend to be taller , wider transversely , and flatter anteroposteriorly [ 1214 ]  . 
unexpected lesions can also be detected by the use of chest ct scan in patients with psp especially in children and females [ 15 , 16 ]  . the ipsilateral recurrence rate of psp is increased with the presence of ipsilateral blebs and bullae in the chest ct scan if no surgical exploration offered [ 17 ]  . 
this is a very crucial element in the discussion with the patients in our culture as the recurrence on the contralateral side can occur even with doing a surgery on the ipsilateral side . 
on the other hand , an absence of pulmonary blebs or bullae on the chest ct scan fails to predict the recurrence rate psp [ 16 , 21 , 22 ]  . even though chest ct scan has those benefits , the current guidelines limit the use of chest ct scan to the complicated cases of psp [ 23 , 24 ]  . 
in fact , some studies advocate the use of surgical exploration even in the absence of abnormalities in the chest ct scan [ 21 , 25 ]  . the study was limited as it was a retrospective study involving only one center with specific geographic distribution . 
a more prospective study is needed to study the recurrence rate of psp in relation to chest ct scan findings with consideration of the histopathological evaluation of the resected specimen . conclusion the sensitivity of the chest ct scan is high in detecting surgically resectable pulmonary blebs or bullae . 
the aim of our work was to evaluate the potentialities of carotid computed tomography angiography ( ccta ) in assessing composition of atherosclerotic plaque . materials and methods we retrospectively evaluated 29 patients ( 7 women and 22 men , age range 5481 ; mean age 69 ) who underwent carotid endarterectomy . 
mcnemars test was used for comparison of dichotomous variables . results a significant correlation between histology and ccta was found with respect to the areas corresponding to adipose , fibrotic and calcified plaques . 
carotid atherosclerotic disease is a common condition preferably affecting the elderly population , considering that a carotid artery stenosis has been reported in up to 75% of men and 62% of women aged 65years [ 13 ]  . 
these components associated with endothelial erosion may lead to plaque instability and contribute to severe disease and clinical risk [ 810 ]  . on the basis of their degree , carotid stenoses have been classified as moderate ( 5069% of vessel lumen ) or severe ( 70% of lumen )  . 
since cerebrovascular events causing acute occlusion of a cerebral vessel are the consequence of embolisms typically arising from a carotid bifurcation plaque , several recent studies suggest investigating other processes , besides the degree of stenosis , as possible causes of the atherosclerotic plaque . 
vulnerable plaques are associated with crucial morphologic findings : rupture of the fibrous cap , signs of intra - plaque hemorrhage , the presence of adipose large core and irregularities ( ulcerations ) on the plaque surface [ 1214 ]  . 
among the different diagnostic imaging techniques currently available , multidetector ct angiography ( mdct ) is considered the most effective thanks to its availability , velocity of execution , high spatial resolution and multi - planar reconstructions . 
as suggested by many authors [ 15 , 16 ] , mdct plays an important role in predicting vulnerability of atherosclerotic plaque as the inner density of the plaque is inversely proportional to the risk of rupture and consequent cerebral embolisbased on these considerations , we retrospectively analyzed atherosclerotic carotid plaque composition using mdct with the aim to assess quantitatively adipose , fibrous and calcified intra - plaque tissue and compare the imaging data with the histological features obtained from carotid endarterectomy ( cea ) samples . 
the institutional review board of our university approved this retrospective study protocol . materials andmethods from january 2016 to february 2017 , we selected 29 patients ( 7 women and 22 men , age range 5481 ; mean age 69 ) who underwent carotid endarterectomy ( cea ) due to the presence of hemodynamic internal carotid artery stenosis 70% with or without neurological symptoms . 
all patients received 60ml of contrast medium 400mg / ml ( iomeprolo , iomeron ; bracco imaging italia ) followed by 40ml saline bolus chaser , both with an injection rate of 4ml / s . 
poor - quality ct images were excluded from our study . image analysis ct images were sent to a stand - alone workstation ( vitrea workstation , toshiba medical systems europe ) operating with dedicated post - processing 3d analysis software sureplaquetm . 
in our experience , range 100 to 49 ( hu ) was displayed in red ( adipose plaque component ) , range 50149 ( hu ) in blue ( fibrotic component ) , and range 1501300 ( hu ) in yellow ( calcific component )  . 
to assess the atherosclerotic plaque composition , the vessel was studied at the level of maximum stenosis and 3mm above and below the slice selected as the one showing the largest plaque area . 
 the percentage of the three different components of the 1 3 la radiologia medica ( 2019 ) 124 : 795803 atherosclerotic plaque ( adipose , fibrous and calcified tissue ) was assessed using pre - specified hounsfield unit ( hu ) densitometric values . 
according to our pre - defined protocol , the plaque component presenting a hu value between 100 and 49 was classified as adipose tissue , between 50 and 150 fibrous tissue , and higher than 150 calcified tissue . 
to avoid rupture or fragmentation of the plaque the specimen wasobtainedbyerodingthe outer media and adventitia . of the different areas occupied by each of the components , by calculating it on the total surface of the plaque . statistical analysis continuous variables were summarized as means with standard deviation , and categorical variables were reported as absolute or relative frequencies . 
vessel and plaque parameters were compared between ccta and histology using the pearson correlation coefficient ( r ) with two - sided p values and with 95% confidence intervals ( ci ) for r . 
 similarly to ccta image acquisition and analysis , the arteries were sectioned serially 5mm above and below the level of major stenosis , dehydrated in graded ethanol and embedded in low - temperature - fusion paraffin for histological studies . 
serial 3 - m - thick sections were cut in order to reach the maximum plaque thickness ; the sections located above and below the maximum plaque extension were discarded as they did not show a complete view of the lesion . 
the whole image was therefore employed to select the corresponding calcified , fibrotic and adipose areas within the plaque . these evaluations were independently performed by two pathologists ( av and rs ) in a double - blinded fashion . finally , through an image analysis system ( ias , delta system , rome , italy ) it was possible to obtain the percentage considering the differences in thickness between ccta slices ( 0.5mm ) and histological sections ( 3m ) , the matching between ccta and histology was considered with great care to avoid , as much as possible , misregistration . 
the table on the top shows percentages of the different components of the plaque showing very good correlation with histological values obtained from the specimen using massons trichrome staining protocol . 
2 maximum intensity projection ( mip ) ct ( left ) and volume rendering ( right ) reconstructions of a mainly fibrotic carotid bifurcation atherosclerotic plaque , presenting a relatively high adipose component . 
3 maximum intensity projection ( mip ) ct ( left ) and volume rendering ( right ) reconstructions of a carotid bifurcation atherosclerotic plaque presenting a prevalence of calcified tissue . 
in the center of the figure , residual vessel lumen is shown in green 1 3 la radiologia medica ( 2019 ) 124 : 795803 discussion the results of our study confirm that mdct can be a reliable diagnostic imaging tool to assess different components of the atherosclerotic carotid plaque , useful to identify vulnerability criteria . 
on the other hand , a relatively moderate correlation with histology regarding adipose and fibrotic tissue was reported in exvivo studies [ 16 ] , where the authors found a wide range of overlapping values for differentiation of non - calcified from mixed plaques . 
they explained the obtained data with the frequent coexistence of calcium and the consequent blooming effect ; in fact , the correlation for adipose tissue was particularly inaccurate in severely calcified plaques . 
the blooming effect , caused by calcifications , leads to overestimation , on ct images , of the calcified component and often does not allow adequate evaluation of the non - calcified parts . 
 [ 20 ] who reported sensitivity and specificity values of 93% , however , excluding from the analysis all the slices presenting a cluster of calciusaremi and achenbach [ 21 ] reported that differentiation of soft and lipid - rich plaque from more stable fibrous ones is still difficult and significant overlap in attenuation values exists . on current clinical computed tomography scanner , thin fibrous cap detection is not possible , and the vulnerable plaques may be misdiagnosed or overlooked [ 22 ]  . 
nevertheless , a low attenuation core surrounded by a rim - like area of higher attenuation also known as napkin sign may be suggestive of plaque at high risk of cerebrovascular events . when performing mdct , it is important to consider that hyperdense areas projecting outside vessel lumen could be referable to plaque ulcerations but also to focal calcifications ; it is thus recommended to acquire unenhanced scans in order to assess the correct diagnosis , since a true ulceration will appear hypodense on unenhanced scans . the vulnerable plaque is reportedly 60 hu in density [ 23 , 24 ]  . 
on the coronary plane , a low - density plaque is considered as vulnerable , and the boundary hu between lipid - rich and non - lipid - rich plaque is established at 5070 [ 25 , 26 ]  . our data aided by these considerations suggest that limitations still persist in the characterization of plaques even using a wide - detector apparatus with thin 0.5 - mm detectors [ 27 ] and considering lipid - rich plaque with 50 hu in density . 
we also observed a moderate correlation between histology and ccta in adipose tissue ( r = 0.55 ; p < 0.012 ) with respect to fibrotic ( r = 0.90 ; p < 0.0001 ) and calcified ( r = 0.79 ; p < 0.0001 ) tissue within the plaques . 
overestimation of the calcified component may be the consequence of blooming artefacts also present in our experience . according to our experience , in heavily calcified plaques , a slight modification of the aforementioned thresholds when analyzing different components of the plaque might be appropriate in order to overcome limitations depending on blooming effects ; this concept , however , has still to be demonstrated in larger case series . the moderate correlation of the adipose component with histology may be more reliably related to the coexistence of the calcified component hindering an adequate estimation of the adipose one . this affirmation may be supported by the evidence that the adipose area is underestimated at ccta if compared to histology considering that it was excluded that discrepancies could be related to the manipulations of the plaque . 
for all these reasons , our experience confirms the good potentialities of ccta in plaque characterization that , combined with an accurate stenosis assessment , may suggest an interesting role in the one - shot evaluation . currently , other diagnostic imaging techniques provide several fundamental information regarding plaque morphology and clinical relevance . 
ultrasonography with doppler examination is considered a fast and first - line imaging technique able to estimate the degree of stenosis and useful to identify echo - lucent plaques more prone to rupture due to their high content in fat tissue ; nevertheless , its reproducibility is not always adequate [ 2830 ]  . some studies , however , showed the superiority of contrast - enhanced ultrasound ( ceus ) to conventional us , particularly regarding the possibility to identify ulcerated plaques in terms of sensitivity and inter - observer agreement [ 31 ]  . mri is considered the best imaging technique for plaque characterization based on the evidence and status of the fibrous cap ( thick , thin or fissured ) usually appearing as a juxta - luminal low - signal band on time - of - flight ( tof ) 1 3 802 la radiologia medica ( 2019 ) 124 : 795803 sequences ; lack of the hypointense zone in tof sequences between vessel lumen and plaque represents a sign of ulceration . 
thanks to the different imaging patterns of blood products on t1 - weighted , t2 - weighted and tof sequences , it is also possible to age the areas of hemorrhage . moreover , mri , performed with contrast enhancement in dynamic technique , is a valuable tool to identify possible intra - plaque enhancing areas , referrable to signs of inflammation or hemorrhage and to assess the possible presence of neovascularization , which is considered a sign of vulnerability since these vessels are highly prone to rupture . these patients would be better candidates for carotid endarterectomy than for carotid stenting , considering that the latter has been demonstrated to present a higher risk of intra - procedural complications [ 15 ] due to possible thromboembolic complications . however , mri has some limitations including poor spatial resolution , scarce ability to demonstrate the calcified components and quite long acquisition times [ 3234 ]  . 
on the other hand , mri may prove useful in selected patients showing unfavorable morphologic features of the plaque on ct imaging and its use may prove of support during plaque analysis in the attempt of evaluating the individual risk of developing cerebral stroke [ 35 , 36 ]  . limitations our study presents some limitations . 
first , histology is considered as the reference standard in quantitative assessment of carotid plaque composition using mdct ; nevertheless , carotid plaque specimens may be damaged during transportation between operating rooms and histological examinations ; these phenomena are likely to affect mostly the softest component of the plaque , represented by fat . 
this was necessary to have a correlation technique represented by histological analysis , but on the other hand , this could limit the clinical application of our data , since many cerebral strokes occur in patients presenting a lower degree of stenosis [ 37 ] and correlation between ct imaging and histopathological findings should be investigated . 
finally , our data were obtained from a relatively small cohort , while a larger sample size may have provided more reproducible results . conclusions our data suggest that ccta has adequate characteristics to identify correctly the different components of carotid atherosclerotic plaques , with some limitations in plaques with a relevant adipose component . 
postnatal imaging , postoperative report , histology , autopsy , and clinical outcomes were the reference standard to calculate sensitivity , specificity , accuracy , positive predictive value ( ppv ) , and negative predictive value ( npv ) of prenatal mri in detecting airway patency . 
we also assessed mri performance in the diagnosis of the mass nature . results we obtained data about postnatal airway status in 19 of 23 patients ; prenatal mri demonstrated a sensitivity of 9 / 9 [ 100% , 95% confidence interval ( ci ) 66100% ] , specificity 8 / 10 ( 80% , 4498% ) , accuracy 17 / 19 ( 89% , 6799% ) , ppv 9 / 11 ( 82% , 4898% ) , and npv 8 / 8 ( 100% , 63100% ) ; the interobserver agreement was perfect . 
buzzi childrens hospital asst fatebenefratelli - sacco , via castelvetro 32 , 20154milan , italy 4 radiology unit , irccs policlinico san donato , via morandi 30 , 20097sandonatomilanese , milan , italy 5 department ofbiomedical sciences forhealth , universit degli studi di milano , via morandi 30 , 20097sandonatomilanese , milan , italy introduction congenital neck masses are rare and usually benign [ 1 ] ; however , they may compress and distort foetal airway resulting in hypoxic injury and neonatal death [ 25 ]  . 
the antenatal detection of a neck mass and its effect with the foetal airway is of paramount importance as it may change the therapeutic strategy and management of the delivery [ 2 , 3 ]  . in order to prevent respiratory distress , at birth is available the ex utero intrapartum therapy ( exit ) procedure . 
in fact , the progress of imaging techniques allows antenatal selection of those foetuses with congenital abnormalities , who need special care at birth in highly specialized hospital [ 5 , 6 ]  . 
in clinical practice , ultrasound ( us ) is the first line imaging modality to evaluate pregnancies , thanks to its wide availability , low cost , and absence of radiation exposure [ 10 , 11 ]  . 
despite its limitations , in most cases us is sufficient to characterize foetal malformations , but sometime , it does not provide complete information for a proper treatment planning , as in case of neck mass , where it can only identify indirect signs of airway obstruction , such as polyhydramnios , tongue protrusion , and absence of swallowing [ 2 , 5 , 10 , 12 , 13 ]  . 
magnetic resonance imaging ( mri ) is now a complementary tool for evaluating foetuses with foetal airway and neck mass anomalies at prenatal us [ 3 , 11 , 13 ]  . 
as previously published in case reports and small case series , mri is actually considered the best imaging modality to directly visualize the foetal airway , thanks to its intrinsic high softtissue contrast , high spatial resolution , and application of new ultrafast sequences [ 11 , 1316 ]  . the aim of our study was to investigate the diagnostic performance of prenatal mri in neck mass characterization , with special focus on the foetal airway status . materials andmethods patient selection we retrospectively reviewed all prenatal mri examinations performed in our institution from may 2001 to february 2016 , performed after a second - level ultrasound suspicious for neck mass carried out at most 7days before . 
all mothers signed a written informed consent prior to prenatal mri and a disclaimer regarding data collection about clinical and imaging follow - up . prenatal mri protocol prenatal mri examinations were performed on a 1.5 - t system ( philips achieva , the netherlands )  . 
they were blinded to the patients name , indication to mr , and final diagnosis ; instead , they were aware of the gestational age at the time of the examination . foetal airway the readers evaluated the involvement of foetal airway on t2 - weighted images , where the airway was better identifiable because of the brightness of its fluid content . 
foetal airway was considered involved if the lumen was : obstructed : not visible at all at the level of the mass narrowed : any narrowing of the airway diameter at the level of the mass respect to the airway diameter above or under the mass . displacement of the airway alone was not sufficient for considering airway threatened . mass characteristics we divided neck in anterior , posterior , and laterocervical regions . anterior region : limited posteriorly by the transverse processes of the cervical vertebrae , including infrahyoid and suprahyoid regions and the median visceral space of the neck posterior region : located behind the transverse processes of the cervical vertebrae , including cervical spine and 1 3 la radiologia medica ( 2019 ) 124 : 917925 the posteriorly surrounding soft tissues together with the nuchal region laterocervical region : including the neurovascular bundle region , the sternocleidomastoid muscle , and the supraclavicular region . we also assessed the development of the mass into the mediastinum . the structure of the masses was assessed considering the characteristics of the signal on t1 and t2 weighted sequences ; hence , we classified each mass as cystic ( high signal on t2w and low signal on t1w ) , solid ( low signal on t2w and low signal on t1w ) , or mixed ( cystic - solid signal )  . to estimate the size of the mass , we considered the maximum diameter in any plane . for each mass , a hypothesis of diagnosis of nature was given by the two readers , distinguishing among lymphatic vascular malformation , teratoma , or other lesion . 
the prenatal us diagnosis is also reported in table2 . reference standard the need for respiratory care in neonatal period , determined by clinical outcomes , postnatal imaging , surgery , histology , or autopsy , was considered the reference standard for determination of airways involvement . 
respiratory care included exit procedure and intubation . the final diagnosis was confirmed by histopathology in case of resection or biopsy of the mass or by autopsy in case of non - delivered foetuses or neonatal death . 
unequivocal clinical course was used for final diagnosis of some lymphatic vascular malformations thatwere followed up with us , mri , and surgical visitand which showed regression , spontaneously or after sclerotherapy . statistical analysis for each foetus , the following variables were recorded : the gestational age and diagnosis at the time of us , the gestational and maternal age at the time of prenatal mri . 
distributions were given as counts and percentages for categorical variables and as median and interquartile range ( iqr ) for continuous variables . we calculated the diagnostic performance of prenatal mri as sensitivity , specificity , overall accuracy , positive predictive value ( ppv ) , and negative predictive value ( npv ) with their 95% confidence intervals for the involvement of the airway by the neck mass . 
the interobserver agreement in evaluating airway status , as well as in the diagnosis of mass nature , was estimated by using the cohen statistics . differences between lymphatic vascular malformations and teratomas were assessed in terms of location , structure , maximum diameter , gestational , and maternal age at the time of the prenatal mri . 
 significance level was set at 0.05. results postnatal follow - up was available in 23 of the 26 foetuses , 14 females and 9 males ; three patients were lost to postnatal follow - up . 
of these 23 , 19 women carried the pregnancy to term , three voluntarily terminated the pregnancy , and a woman experienced intrauterine foetal demise . at the time of the us , the median gestational age was 25weeks ( iqr 1934 )  . 
at the time of the prenatal mri , the median gestational age was 28weeks ( iqr 2037 ) and the median maternal age was 32years ( iqr 2149 ) ; see table1 for more detail . among the 19 delivered neonates , 17 ( 90% ) survived through neonatal period and were alive after a follow - up of at least 1year ( range 113years )  . airway involvement postnatal confirmation about airway involvement was available only for the 19 delivered foetuses . eight of 19 babies did not need any neonatal respiratory assistance at birth ; nine of 19 babies needed neonatal respiratory care : six exit procedures and three endotracheal intubations were performed . 
exit procedure was performed in three babies affected by a lymphatic malformation , two by a teratoma and one by a venous vascular malformation ; all newborns had long - term survival but one with a huge teratoma extending into the mediastinum , died on the third day due to respiratory insufficiency . 
among babies undergone intubation : one had a thyroid goitre , one a lymphatic malformation , and one a branchial cyst ; the newborn with the goitre died shortly after the intubation for multi - organ failure . 
in 4 exit procedures , airway was secured by intubation ; in 2 exit procedures , tracheotomy was necessary . in diagnosing the foetal airway involvement by the neck mass , prenatal mri demonstrated a sensitivity of 9 / 9 ( 100% , 66100% ) , a specificity of 8 / 10 ( 80% , 4498% ) , an accuracy of 17 / 19 ( 89% , 6799% ) , a ppv of 9 / 11 ( 82% , 4898% ) , and a npv of 8 / 8 ( 100% , 63100% )  . 
 only one lymphatic vascular malformation and one teratoma developed into the mediastinum ; in both cases , exit procedure was successfully performed . prenatal mri correctly identified 21 / 23 ( 91% ) cervical masses , while prenatal us correctly identified 17 / 23 ( 74% )  . there were two wrong mri diagnoses : a branchial cyst ( fig.3 ) misdiagnosed as lymphatic vascular malformation and a lymphatic vascular malformation misdiagnosed as teratoma . 
the two cases of disagreement were the venous vascular malformation and the neurocristic cutaneous hamartoma , both correctly diagnosed only by the more experienced reader . at the time of prenatal mri , teratomas had a median maximum diameter ( 68mm , iqr 6178 ) greater ( p = 0.032 ) than that of lymphatic vascular malformations ( 52 mm , iqr 3762 )  . 
instead , there was no significant difference between lymphatic vascular malformations and teratomas in terms of median gestational age ( 28 weeks for both , p = 0.750 , mannwhitney u test ) , median maternal age ( 32 vs 31years , respectively ; p = 0.385 , mannwhitney u test ) , 1 3 la radiologia medica ( 2019 ) 124 : 917925 fig . 
ss - tse t2 - weighted axial mr image ( a ) shows a high signal multiseptated left neck mass ( * ) , deviating and compressing the oropharynx ( arrow ) ; ss - tse t2 - weighted sagittal image ( b ) demonstrates the mass ( * ) compressing the oropharynx ( arrow ) , while larynx and trachea are patent ( arrowheads ) ; sense btfe coronal image ( c ) shows the mass ( * ) compressing the airway at the level of oropharynx ( arrow ) ; trachea is patent ( arrowhead ) fig . 
sstse t2 - weighted sagittal ( a ) , coronal ( b ) , and axial ( c ) images show an exophytic mass ( * ) with mixed solid and cystic structure , obstructing oropharynx , hypopharynx , and larynx ( arrow ) with hyperextension of the foetal neck ; nasopharynx and trachea are patent ( arrowheads ) and gestational age at the discovery of the disease ( 23 vs 26weeks , respectively ; p = 0.892 , mannwhitney u test )  . among foetuses affected with teratomas , three had hyperextension of the neck and two had polyhydramnios . details are reported in table3 . discussion foetal neck masses , although uncommon and usually benign , may become life - threatening and have clinical relevance if they compromise the airway , leading to the risk of severe respiratory distress at birth . 
if a foetal neck mass is detected , parents and clinicians are forced to take critical decisions about time and mode of delivery and management of the newborn . lymphatic vascular malformations and teratomas are the most common foetal cervical masses [ 2 , 3 , 17 , 20 ] ; about 30% of childhood and 25% of all neonatal teratomas occur in the neck [ 21 , 22 ]  . 
congenital lymphatic malformations are slow - flow vascular malformations due to an abnormal development of the lymphatic system , presenting in microand / or macrocystic form [ 3 , 23 , 24 ]  . 
 ss - tse t2 - weighted sagittal ( a ) , axial ( b ) , and coronal ( c ) mr images show a hypersignal cystic mass ( * ) slightly compressing the oropharynx ( arrow ) ; coronal image ( c ) shows patent trachea ( arrowhead )  . 
the misdiagnosis of lymphatic malformation was made in this foetus table 2 prenatal ultrasound diagnoses , prenatal magnetic resonance imaging diagnoses , and postnatal confirmation case us diagnosis r1 mr diagnosis r2 mr diagnosis postnatal diagnosis other other teratoma other teratoma teratoma teratoma teratoma teratoma teratoma teratoma teratoma other other other other teratoma teratoma teratoma teratoma teratoma teratoma teratoma other teratoma other teratoma teratoma teratoma teratoma teratoma teratoma teratoma goitre neurocristic cutaneous hamartoma venous malformation rich branchial cyst teratoma teratoma teratoma teratoma teratoma teratoma us ultrasound , mr magnetic resonance , r1 12years experience reader , r2 2years experience reader , lm lymphatic malformation , rich rapidly involuting congenital hemangioma teratomas are germ cell tumour originating from the midline of the body , composed of all embryonal layers : endoderm , ectoderm , mesoderm [ 3 , 17 ]  . our data , about location and structure of lymphatic vascular malformations and teratomas , confirmed data of the literature . 
in fact , lymphatic vascular malformations 1 3 la radiologia medica ( 2019 ) 124 : 917925 table 3 mass features observed at prenatal magnetic resonance imagcase site structure postnatal diagnosis max diameter ( mm ) solid mixed solid solid cystic mixed cystic mixed cystic cystic cystic cystic cystic cystic cystic cystic cystic mixed mixed mixed mixed mixed mixed goitre neurocristic cutaneous hamartoma venous malformation rich branchial cyst teratoma teratoma teratoma teratoma teratoma teratoma a anterior , p posterior , lc laterocervical , lm lymphatic malformation , rich rapidly involuting congenital hemangioma are more often located posteriorly or posterolaterally in the neck , with cystic texture ( in our series 83% , 10 / 12 ) , and teratomas are more commonly anteriorly located , with mixed cystic - solid structure ( in our series 100% , 6 / 6 ) [ 3 , 11 , 19 , 25 , 26 ] ; two cases of lymphatic vascular malformations with mixed appearance were probably due to the coexistence of microcystic and macrocystic pattern . we agree with hedrick [ 7 ] , when he affirms that the involvement of the airway depends on the location rather than the mass size . 
in fact , in our experience , 5 of 6 anteriorly located masses required respiratory care at birth , while none of the posteriorly located needed it , and less than half of the lesions ( 4 / 9 ) located in the laterocervical space underwent neonatal respiratory assistance . 
this could be explicated by the proximity of the anteriorly located mass to the airway . the extension of the masses into the mediastinum is an additional risk factor for compromising the airway , as in one of our cases , where a huge teratoma completely obstructed the foetal trachea , requiring exit procedure at birth . we also found that teratomas had median maximum diameter greater than lymphatic vascular malformations at the time of the prenatal mri . 
teratomas are often huge when diagnosed , determining sometimes hyperextension of the foetal neck , as we saw in three foetuses , polyhydramnios , as we saw in two foetuses , and dystocia [ 19 ]  . the fact that no significant difference was found between lymphatic vascular malformations and teratoma , in term of median gestational age at the time of the prenatal mri ( 28weeks ) , could be explained based on our obstetric surveillance system , which establishes a period to perform us to detect morphological anomalies . in the presence of a foetal neck mass , in addition to lymphatic vascular malformation and teratoma , must be considered other rare expansive lesions , such as thyroid goitre , hemangioma , neuroblastoma , branchial cyst , laryngocele , and soft - tissue tumours [ 17 , 26 ]  . 
in most cases , us is sufficient to identify foetal body anomalies and choose the proper therapy , but in some cases , sonographic features are unclear and the abnormality is not completely characterized [ 10 ]  . mri begun to be used in pregnant women in 1983 [ 12 , 27 ]  . 
currently , thanks to its absence of radiation exposure , large field of view , intrinsic high soft - tissue contrast , high spatial resolution , multiplanar capability , and application of new ultrafast sequences , it allows to obtain high detail about extent , location , and structure of the mass , making clinicians more confident in the diagnosis [ 6 , 10 , 13 ]  . in our experience , mri demonstrated substantial accuracy in prenatal diagnosing of mass nature , having correctly identified 21 of 23 masses . 
the different level in interpreting prenatal mri could explain this difference , allowing the more expert reader to understand when a mass was other than teratoma or lymphatic vascular malformation , which have specific features . 
we did not calculate the agreement between prenatal us and postnatal diagnosis about mass nature , because the us examinations were all performed in second - level centres but by different operators , so without any standardization . correct diagnosis of mass nature and details about mass characteristics are certainly necessary for paediatric surgeons , anaesthesiologists , gynaecologists , and other members of the multidisciplinary team to plan the best treatment ; however , the most important issue to consider 1 3 924 la radiologia medica ( 2019 ) 124 : 917925 is the status of the foetal airway [ 7 ] , because airway obstruction could bring newborn to death . despite us has the advantage to be a real time examination , which allows to evaluate the presence of foetal movements , it can only identify indirect signs of airway obstruction , such as polyhydramnios , tongue protrusion , or absence of swallowing [ 2 , 5 ]  . 
conversely , visualization of the foetal anatomy is possible with high - resolution mr images , beingwhite foetal airway easily identifiable on t2 - weighted images thanks to the high signal of the amniotic fluid content , which enables accurate diagnosis [ 2 , 11 , 15 , 19 , 25 ]  . from our study emerges that prenatal mri has a sensitivity of 100% and a positive predictive value of 82% in evaluating the involvement of foetal airway in case of neck mass , with an acceptable rate of wrong positive ( 18% )  . in fact , only two babies with mri examination positive for airway impairment were misdiagnosed ; one was intubated at birth and extubated some hours later , after a postnatal mri study revealing spontaneous regression of the malformation , by now , far from the airway ; the other baby was delivered by planned caesarean section and could breathe spontaneously . 
we think that to obtain updated information , it might have been better to repeat mri closer to the date set for the childbirth . moreover , there was another case of overtreatment : prenatal mri at 21weeks of gestation correctly showed patent airway , very close to a large lymphatic malformation . 
thus , we can state that a negative mri examination , in consideration of its very high sensitivity and npv , is a reliable tool to exclude significant airway impairment and avoid invasive maternal foetal procedures . regarding the status of the airway , the two readers agreed in all cases . 
indeed , the bright foetal airway is relatively simple to identify on t2 - weighted images , so if it is not visible or thinned at the level of the mass , its involvement can be reasonably supposed . 
hence , the performance of prenatal mr in the assessment of foetal airway seems not influenced by the readers experience . conclusion prenatal us remains the first line tool in the evaluation of foetal neck anatomy . 
in case of potential airway obstruction , we believe in the need for serial foetal mri , repeating it as close as possible to the planned delivery date . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . 
the authors did not receive any funding for the present study . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent for this type of study , formal consent is not required . 
strohmenger. diagnostic imaging in dental anomalies diagnostic imaging in dental traumatology table of recommendations glossary introduction technological improvement in diagnostic imaging techniques and equipment has recently led to a great qualitative and quantitative improvement . dental imaging has dramatically changed over the last fifteen years , in particular in the field of oral surgery and paediatric dentistry . 
in both these specialties , scientific evidence has increased , highlighting the need for guidelines concerning radiation dose justification and optimisation in dental imaging . as a matter of fact , several scientific articles and communications on dose issues in dental imaging increased , with particular focus on applied physics in medicine . 
in ministry of health secretariat general office 2 national guidelines for dental diagnostic imaging in the developmental age november 2017 introduction work group bibliographical research current regulations considerations on radiological risks and containment strategies in x - ray examinations diagnostic imaging for caries and periodontal disease diagnostic imaging in orthodontics and gnathology diagnostic imaging in cranio - maxillofacial malformations this sense , interest also arose in the international scientific community , leading to publication of guidelines by several institutions and societies ( 1 , 2 , 3 , 4 , 5 , 6 )  . among the campaigns for oral health promotion , in 2016 the national department of health decided to prepare guidelines on dental diagnostic imaging procedures in children and adolescents . therefore , a dedicated workgroup was created under the coordination of laura strohmenger , member of the w.h.o. 
collaborating centre for epidemiology and community dentistry . 1 3 la radiologia medica ( 2019 ) 124 : 887916 this document aims to support the dental professional in choosing the adequate diagnostic technique , minimising the radiation dose in observance of the as low as reasonably achievable ( alara ) principle ( 7 )  . 
medical subject headings used for bibliographical research radiological field patient field dental radiology dental radiography dental cone beam dental cbct intraoral panoramic cephalometer * child * adolescent paediatric from the identified publications , 185 articles and 7 web pages were selected , whose references are reported in this document . for evaluation of the gathered documents , we used prisma ( preferred reporting items for systematic reviews and meta - analyses ) , one of the tools suggested by the methodological manual of the 2011 national guidelines system how to produce , disseminate and update public health guidelines . bibliography guidelines for the safe use of dental and maxillofacial cbct : a review with recommendations for south africa . 
4 principle of optimisation introduces the diagnostic reference levels ( drl ) with the aim of providing a working tool to guarantee an optimisation process standardisation for the most common radiological practices . 
these are easily measureable dose - level thresholds that should never be exceeded in normal examination of average build patient groups , and for well - defined appliances and techniques . 
in the field of dental radiological imaging , there are currently no defined drls in italy , whereas some drl values defined in other countries will be illustrated in a dedicated section of this document . specific aspects regarding apparatuses are featured in art . 
8 , including the obligation to define quality assurance programmes , to make acceptance and performance tests , and for the head of radiological equipment to state their clinical adequacy . 
so , within the context of these guidelines purpose , it is highlighted that all dental radiological practices involving exposure of paediatric patients must be considered as special practices , in accordance with the above - mentioned art . 
all provisions of the latter article must therefore be adhered to , including periodic dosimetric assessments by a medical physics expert , based on which the head of radiological equipment shall judge the technical service quality and the diagnostic procedure . generally , in the current regulatory framework and in particular with regard to the implementation modes , the european guidelines on radiation protection must be taken into consideration . 
among these , we point out : european guidelines on radiation protection in dental radiologyno 136 [ 1 ] 1 3 la radiologia medica ( 2019 ) 124 : 887916 criteria for acceptability of medical radiological equipment used in diagnostic radiology , nuclear medicine and radiotherapyno 162 [ 2 ] cone beam ct for dental and maxillofacial radiology no 172 [ 3 ] moreover , the reference technical regulations defined by the italian electrotechnical committee are of fundamental importance in verifying the equipment technical features . 
all these methods use x - rays and thus ionising radiation that may interact at a cellular level . when ionising radiation passes through a cell , there may be ionisations of atoms in the molecules that constitute the cell itself . 
damage to the dna may be entirely repaired by means of complex mechanisms ; it may be irreparable , with consequent cellular death ; or it may be partially repairable with the consequent appearance of a genetic mutation . 
 this mutation could be the primum movens of a complex series of events potentially resulting in carcinogenesis or , in the case of the involvement of germ cells , causing hereditary diseases in the radiated persons progeny . the biological effects of ionising radiation may be grouped in deterministic effects and stochastic effects . deterministic effects are caused by exposure to ionising radiation doses that are far higher than those used in radiological diagnostics , occurring only if specific threshold values are exceeded and with a gravity that increases with an increase in the absorbed dose . 
they are caused by cellular death and may manifest themselves in pancytopenia , alopecia , sterility , burns , pneumonia and serious gastrointestinal disturbances , with possible death of the radiated person . stochastic effects are caused by radiation doses lower than those required for the manifestation of deterministic effects and are due to non - lethal and unrepaired cells damage that may become manifest with a variable latency , even of several years . for the purposes of radiation protection , the accepted assumption is that there is a linear relationship between risk and radiation dose , and that there is no threshold value below which risk is zero . 
in the absence of certainty in this regard , a prudential approach is preferred to ensure that the dose of radiation employed for radiological diagnostics is the minimum indispensable for producing an image of adequate diagnostic quality . the absorbed dose for ionising radiation may be defined as the quantity of energy deposited in the exposed tissues or organs . 
 the gray is a very large unit of measurement in diagnostic imaging so it is therefore more practical to use the milligray as unit of measurement , corresponding to one thousandth of a gray . 1 3 892 la radiologia medica ( 2019 ) 124 : 887916 the risks due to exposure to different types of ionising radiation may be compared in terms of equivalent dose . 
moreover , the effective dose allows comparison of doses resulting from different techniques employed for the same medical examination and / or comparison of doses resulting from similar procedures carried out in several institutions . 
it follows that the risk must always be kept in mind , especially in the case of using radiological procedures that expose patients to high doses of radiation , this being justifiable only when there is a clear benefit to the patient deriving from execution of the procedure itself . 
for radiological procedures in the dental field , the scientific reference literature consistently reports the values of effective dose and equivalent dose to be at levels of microsieverts ( sv ) , where one sv is equal to one thousandth of an msv . 
in the context of cbct procedures in dentistry during the developmental years , ludlows recent review [ 1 ] provides a metanalysis of assessments of effective doses with paediatric protocols and phantoms , derived from the use of 10 different apparatuses . 
the assessments are subdivided into those deriving involving the use of a medium or large field of view ( height greater than 10cm ) or small field of view ( height less than 10cm ) for maxillary bone and for mandible . 
ludlow underscores that the effective dose assessed using paediatric simulation phantoms with cbct apparatuses is around 36% greater than that found with adult phantoms , an increase to be correlated mainly with the greater proximity of the thyroid to the inferior margin of the jaw in children , with the consequence of a greater irradiation , both direct and as scatter from the maxillary structures . 
median values of effective dose , thyroid and salivary glands doses for a range of cbct equipments and protocols employed on paediatric simulation phantoms [ 1 ] effective dose dose to thyroid dose to salivary small maxillary bone small jaw medium or large ( 16177 ) ( 24331 ) ( 39430 ) ( 53575 ) ( 3273382 ) 1003 ( 3844265 ) glands 1930 ( 4384974 ) 1654 ( 4045937 ) 2045 ( 5316622 ) the values in brackets are the minimummaximum range . 1 3 la radiologia medica ( 2019 ) 124 : 887916 examination carried out , dose indicators for the patient have been defined , specific to the different radiological methodologies . 
the availability of such dosimetric indicators makes it feasible to carry out multicentric data gathering that , with appropriate statistical analyses , can be used to define diagnostic reference levels . the obligation to have this dose indication available is prescribed by the italian regulations 187 / 00 in article 8 , subparagraph 8 : in the case of utilisation of a newly installed radiodiagnostic equipment , this must be equipped , if feasible , with a device that informs the specialist about the quantity of ionised radiation produced by the device during the radiological procedure . 
the latest european directive on the subject of protection from ionising radiation ( 2013 / 59 / euratom ) , currently being integrated into the national regulations , confirms this obligation and , moreover , prescribes the recording of the pertinent parameters for assessment of the dose to the patient for each examination . 
indicators of doses used in the various apparatuses for dental radiology magnitude apparatus on which used definition unit of measurement normally used air kerma ( kair ) entrance skin air kerma ( esak ) entrance skin dose ( esd ) mgy cm dose area product ( dap ) kerma area product ( kap ) computed tomography dose index ( ctdi ) intraoral air kerma value measured in correspondence to the entrance of the beam into patient cephalometry unit intraoral , orthopantomograph , cephalometry unit , cbct dose value resulting from product of air kerma and backscatter factor measured in correspondence to entrance of beam into patient product of the area of a radiological beam section and the average air kerma on that section multislice ct computed tomography dose index . 
see [ 2 ] for a more complete definition 1 3 894 la radiologia medica ( 2019 ) 124 : 887916 kerma ( kinetic energy released per unit mass ) means the kinetic energy transferred by the x photons to the charged particles of the irradiated material : for the x - ray energies used in radiodiagnostics , its air value coincides with the value of the dose , and therefore , the two terms may be used in an equivalent manner . 
the esak ( entrance skin air kerma ) for an intraoral apparatus therefore corresponds to the air dose assessed on the axis of the beam at the exit of the cylinder and is a quantity directly proportional to the duration of exposure and to the intensity of the anodic current . 
the dap ( dose area product ) takes into account of both the intensity of the beam and its dimensions , and its assessment does not depend on the distance from the source for which it is evaluated . 
where these data are not available on already installed devices , the medical physics expert in charge of dosimetry must measure and tabulate them in such a way that the clinician can take account of these indicators in the choice of the protocols to use . 
in the case of availability of these data , the medical physics expert must check their accuracy , with a maximum acceptable tolerance of 50% . what are thetypical dose indicator values givenintheliterature forthevarious examinations ? in the absence of diagnostic reference levels defined at european or national level , the dosimetric indicators presented in the previous paragraph and available with newly installed radiological equipment may be compared with the values published in the literature . 
values of dose indicators in the literature for cephalometry units used with paediatric patients reference data typology of datum magnitude utilised kim 2014 [ 10 ] 121.3mgycm2 diagnostic reference holroyd 2011 [ 13 ] dap 25mgycm2 diagnostic reference reference level resulting from data analysis of 50 centres in germany ence level resulting from data analysis of 62 centres in greece level resulting from data analysis of 20 centres in korea level resulting from data analysis of 27 centres in great britain for cbct equipment , to date there are no published studies with multicentric data collection of dosimetric indicators . 
values of dose indicators in the literature for cbct with protocols for paediatric patients reference magnitude utilised data ludlow 2015 typology of datum average values deriving from the setting of paediatric protocols on 10 different apparatuses fov large and medium 529mgycm2 fov small maxillary 121mgycm2 fov small jaw 153mgycm2 what characteristics must theacquisition protocols andparameters have forradiodiagnostic dental examinations inthedevelopmental years ? in general , studies published in recent years underline the need to define acquisition protocols with parameters adapted to the reduced dimensions and the diagnostic requirements specific for the paediatric patient , with the published multicentric assessments often highlighting the use of inadequate parameters . an anglo - saxon study of 2013 [ 15 ] of intraoral examinations showed the national diagnostic reference level to be exceeded in 35% of the operational modes used for adult patients and in no less than 61% of those used for paediatric patients . 
the same study highlights how , notwithstanding the fact that the technological evolution of digital detectors and collimation systems offers the possibility of significant dose reductions , in many cases the technical parameters used lead to patient exposures greater than those required to obtain the correct diagnostic information . a finnish work of 2015 [ 16 ] presents an investigation carried out on 241 orthopantomographs and 118 cephalometric units used on paediatric patients : the panoramic images turned out to be wider than necessary in 70% of the cases and of greater length in 96% . 
thyroid protection was used in roughly 71% of cases . image gently is an awareness - raising and educational campaign concerning proper radiological risk management for paediatric patients , promoted by american scientific associations in the paediatric and radiology field . 
they have summarised in the following six steps the key points for minimising dose in dental radiology practices in the developmental years [ 17 ] : selection of radiological images in conformity with the patients specific needs ; the use of detectors with maximum sensitivity ( high speed in the case of film or equivalent digital systems ) ; collimation of the beam on the area of interest ; use of thyroid collar for all intraoral examinations , and for extraoral examinations when it does not interfere with the area under examination ; suitable reduction in exposure parameters ( time , intensity of anodic currents , etc . ) in comparison with parameters employed for adult patients ; use of cbct only when necessary . 1 3 896 la radiologia medica ( 2019 ) 124 : 887916 among the most common technical errors that might cause artifacts in the images , one must consider : carrying out examinations in the presence of hairclips , metal jewellery , food in the mouth ( sweets , chewing gum ) , removable dental prostheses ; incorrect positioning of the patient ; incorrect positioning of the tongue ; errors in limiting patient movement during image acquisition . increase the exposure times which , coupled with the method of positioning the apparatus , augments the risk of movement artefacts . 
so special attention must be paid to justification of the use of these devices and , while awaiting further evidence from the literature , it is expected that their use will remain limited to very particular cases where it is not effectively possible to employ a fixed intraoral unit . in drawing up these guidelines , comparative evaluation of the recent reference bibliography has allowed the formulation of the following recommendations . the main actions to be adopted in order to reduce the frequency of these errors are : recommendation 1 programme suitable child - friendly time schedules for preparing and carrying out the examination , longer than those necessary for adults ; train staff in suitable communications skills with kids and their families ; calm the patient : in the case of excessive anxiety and restlessness , do not insist ; if necessary , postpone the session ; check also with the parents that jewellery , hairclips and dental prostheses have been removed , as well as sweets or gum from the childs mouth ; pay great attention to correct positioning of the patient ( neck , back , shoulders ) ; without rush or fuss , show the patient the correct positioning of the tongue ( in contact with the palate ) ; for teleradiography of the cranium : in the case of roll , pitch or rotation , always consider carefully the real need to repeat the examination ; most errors influence assessment of the main angles [ 18 ]  . the 2012 document radiation protection 162 [ 9 ] defines new acceptability criteria for technical and functional parameters of all radiological apparatuses , including those used in the dental sector . 
in the same document , it is underlined that this kind of equipment generally works with lower voltage and ma at conventional intraoral examinations , involving the need to strength of recommendation : a degree of evidence : iv recent dosimetric studies [ 22 , 23 ] show that the use of an adult protocol on a paediatric patient may involve unjustified exposure doses . 
limiting the fov in line with the other parameters and compatibly with diagnostic requirements is in general a rule to follow in order to minimise the dose to the paediatric patient . 
there are , however , studies 1 3 la radiologia medica ( 2019 ) 124 : 887916 showing that with some equipment a reduction in fov may be associated with an increase in other exposure parameters , as the beam intensity , such that the dose may even be greater [ 24 ]  . 
it is , therefore , necessary to pay attention to all the parameters associated with the different equipment settings , and in order to compare them from a dose viewpoint , it is appropriate to refer to the dap indication supplied . a recent study by pauwels [ 25 ] evaluated image quality indices on variation in the anatomical dimension concerned . 
the results show the possibility of reducing the dose in the paediatric field by maintaining the kv value relatively high ( 90kv on the apparatus examined ) and reducing the value of the mas prescribed for an adult by 40% for paediatric patients of around 3years old and by 20% for those around 10years old . recommendation 4 the lead thyroid collar contributes significantly toreducing thedose tothethyroid forall radiodiagnostic dental examinations inthedevelopmental years . 
in thecontext ofcbct , it isparticularly recommended forextended fields , exceptincases where , atthetime ofpositioning thepatient , thetechnician , theradiologist orthespecialist ascertains there tobe arisk ofartifacts orpossible superimpositions withregard totheanatomical structures ofinterest . 
as forcephalometry , theuse isrecommended wherethere isnoneed tovisualise bony structures belowthesecond cervical vertebra strength ofrecommendation : adegree ofevidence : iv the assessments made by hidalgo [ 26 ] on a cbct apparatus with fov diameter 17cm and height 12cm , and with various types of thyroid collar , show dose reductions to the thyroid of between approximately 20 and 40% . numerous recent studies [ 27 , 28 , 29 ] highlight the compatibility of thyroid protection in carrying out cephalometry on paediatric patients , which involves a significant reduction in the dose at the thyroid , with the limitation that the bone structures represented start from the second cervical vertebra . bibliography ludlow jb , timothy r , walker c , hunter r , benavides e , samuelson db , scheske mj . 
 2013 ; 64 ( 6 ) : 7559 . european commission radiation protection no 162 criteria for acceptability of medical radiological equipment used in diagnostic radiology , nuclear medicine and radiotherapy directorate - general for energy directorate dnuclear energy unit d4 radiation protection 2012 . berkhout we , suomalainen a , brullmann d , jacobs r , horner k , stamatakis hc justification and good practice in using handheld portable dental x - ray equipment : a position paper prepared by the european academy of dentomaxillofacial radiology ( eadmfr )  . 
2011 ; 40 : 471475 . diagnostic imaging forcaries andperiodontal disease numerous studies ( 110 ) agree that visual examination , especially in primary dentition , is a key factor in assessing the presence or absence of dental caries . 
in fact , for the former type , it seems that radiographic analysis is not necessary to confirm diagnosis . regarding non - invasive diagnostic systems ( 13 ) , the aid of fibre - optic transillumination ( foti ) may significantly favour the diagnostic process ( 14 , 15 )  . ex ante caries risk assessment of a patient ( 1620 , b ) appears to be another discriminating factor in the diagnostic process of carious lesions in primary dentition . 
further radiographic examinations are notjustified strength of recommendation : a degree of evidence : i assessment of carious processes in permanent teeth appears to be sufficiently supported by inspective clinical examinations , to be performed according to well - established criteria ( 1720 ) and backedparticularly for high caries risk patientsin case there is clinical suspicion by a bitewing x - ray and , if necessary , by periapical images to be taken using image receptor holders and beam aiming appliances . 1 3 la radiologia medica ( 2019 ) 124 : 887916 taking an x - ray , using the paralleling technique , of teeth with suspected caries lesions that may have jeopardised pulpal health is particularly indicated for high caries risk patients ( 21 )  . 
it should be stressed that , in certain areas of the mouth , especially the upper and lower posterior areas , the superimposition of other bony structures might make it difficult to examine and outline the periapical image . 
 examinations such ascbct are notindicated inthis diagnostic phase strength ofrecommendation : adegree ofevidence : iii if a fistula is present in the vestibular mucosa , close to the apex of either primary or permanent teeth , it should always raise suspicion of a septic lesion of the dental pulp also affecting the periapical tissues . intraoral x - ray , with the aid of a beam aiming device , is diagnostic investigation of choice . 
5 xray examination ofapermanent tooth showing infection signs onthemarginal gingiva seems tobe indicated , especially forpatients withconfirmed high risk ofperiodontal disease strength ofrecommendation : b degree ofevidence : iii procedures such as direct pulp capping , apexogenesis , apecification and also complete root canal treatment require taking a preoperative x - ray with a paralleling syste this may give sufficient clues regarding the degree of maturity of the root apex and the estimated working length ( 35 )  . clinicians are advised to be in possession of this image already in the diagnostic phase . 
it is worth remembering that , where cleaning and shaping of the endodontium are necessary in immature teeth , electronic apex locators are not reliable ( 36 , 37 )  . 
the followup images should be taken three months , six months , one year , sincetheend oftherapy andthen annually forthenextthree years strength ofrecommendation : adegree ofevidence : ii based on findings from the literature , radiographic treatment longterm follow - up of primary teeth is deemed justifiable ( 38 )  . in case of septic or traumatic pathological processes leading to eradication or conservative ( partial or complete ) treatment of the pulp , a careful observation phase allows accurate assessment of positive or negative signs of the health conditions of the periapical tissues ( 38 , a , b , c , d , e , f )  . 
 on this subject , there are no studies indicating exact timing to mandatorily comply with for following checkups ( 34 ) ; there are , however , longitudinal studies about the assessment of healing processes of edodontically originated periapical lesions , in which patients were checked over time spans varying between six and twelve months , for the initial phases of treatment , and then once a year for a period from three to five years ( 35 )  . 
radiographic followup isrecommended afterthree andsix months andthen annually forthenextthree years , depending ontheclinical situation strength ofrecommendation : adegree ofevidence : ii on the other hand , indications do emerge in checkup schedule to comply with , for assessing radiographic appearance of the pulp chamber and root canalas well as of the apex of permanent teeth which , having undergone conservative pulp treatment ( direct or indirect pulp capping / pulpotomy ) , must be regularly checked to avoid complications , such as obliteration of the root canal , or the onset of endodontically originated periapical lesions , in case partial or complete necrosis of the pulp occurs ( 3436 , a )  . clinicians should also keep track of problems that may arise in case the pulp disease justifies an endodontic treatment , although the tooth has not completed formation of the root apex , by performing an apexogenesis or apecification procedure which , based on scientific evidence , should be then supervised for a six months to three years time span ( 33 )  . bibliography pitts nb , ekstrand kr , foundation i . 
international caries detection and assessment system ( icdas ) and its international caries classification and management system ( iccms ) methods for staging of the caries process and enabling dentists to manage caries . 
community dentistry and oral epidemiology 2013 ; 41 ( 1 ) : e4152 . gimenez t , piovesan c , braga mm , raggio dp , deery c , ricketts dn , etal . 
journal of dental research 2015 ; 94 ( 7 ) : 895904 . gimenez t , piovesan c , braga mm , raggio dp , deery c , ricketts dn , etal . 
 caries research 2015 ; 49 ( 5 ) : 523530 . lino jr , ramos - jorge j , coelho vs , ramos - jorge ml , moyses mr , ribeiro jc . 
international dental journal 2015 ; 65 ( 4 ) : 178181 . ferraz eg , silva lr , sarmento va , de jesus campos e , de oliveira tf , magalhaes jc , etal . 
can we trust visual methods alone for detecting caries in teeth ? evidence - based dentistry 2016 ; 17 ( 2 ) : 4142 . melo m , pascual a , camps i , del campo a , ata - ali j . 
jbr - btr : organe de la societe royale belge de radiologie 2011 ; 94 ( 5 ) : 254265 . castilho ls , cotta fv , bueno ac , moreira an , ferreira ef , magalhaes cs . 
european archives of paediatric dentistry : official journal of the european academy of paediatric dentistry 2016 ; 17 ( 1 ) : 1325 . bussaneli dg , restrepo m , boldieri t , pretel h , mancini mw , santos - pinto l , etal . 
lasers in medical science 2015 ; 30 ( 7 ) : 18731879 . kuhnisch j , sochtig f , pitchika v , laubender r , neuhaus kw , lussi a , etal . 
evidence on existing caries risk assessment systems : are they predictive of future caries ? community dentistry and oral epidemiology 2013 ; 41 ( 1 ) : 6778 . gauba k , goyal a , mittal n . 
the journal of clinical pediatric dentistry 2016 ; 40 ( 1 ) : 3643 . goolsby sp , young da , chiang hk , carrico ck , jackson lv , rechmann p . 
 european archives of paediatric dentistry : official journal of the european academy of paediatric dentistry 2010 ; 11 ( 4 ) : 166174 . mejare ia , axelsson s , davidson t , frisk f , hakeberg m , kvist t , etal . 
international endodontic journal 2012 ; 45 ( 7 ) : 597613 . american academy on pediatric dentistry ad hoc committee on pedodontic r , american academy on pediatric dentistry council on clinical a . 
diagnostic accuracy of periapical radiography and 1 3 902 la radiologia medica ( 2019 ) 124 : 887916 cone beam computed tomography in detecting apical periodontitis using histopathological findings as a reference standard . 
international endodontic journal 2013 ; 46 ( 6 ) : 483491 . kuhnisch j , ekstrand kr , pretty i , twetman s , van loveren c , gizani s , etal . 
since every patient is unique , the need for dental x - rays can only be determined upon the analysis of his medical and dental history , and of his clinical condition and after assessing exposure to environmental risk factors that could jeopardise oral health . x - ray should only be used as a diagnostic examination when considered useful for the patients health , and when it may provide additional information helpful for treatment , complying with the principle of justification . 
given the importance and the current relevance of this issue , numerous guidelines have been published.17 these studies unanimously agree that prescribing x - ray examinations is solely advisable as necessary . 
in compliance with all the international guidelines , 17 this section will describe indications and levels of evidence for each type of radiographic examination suitable for identifying disease , also concerning the costbenefit ratio . for the orthodontic patient , radiographic examination generally consists of panoramic radiography , i.e. 
orthopantomography ( opt ) , and latero - lateral teleradiography of the head , which may be supplemented , in the most complex cases , by more specific examinations . opt allows assessing the presence or agenesis of permanent teeth , the position of teeth yet to erupt , and any supernumerary teeth.8 it is not , however , advisable for evaluating caries in patients suffering from dental decay about to undergo orthodontic treatment . 
in such cases , in fact , a bitewing image is to be preferred.9 teleradiography of the head and cephalometric analysis are indicated for orthodontic diagnosis , treatment planning and the monitoring of results following therapy on the maxillo - mandibular bony structure . 
a useful aid in choosing the appropriate age to prescribe this radiographic examination is the index of orthodontic treatment need ( iotn ) .10 this index allows objective distinction between severe cases requiring early treatment ( iotn 4 and iotn 5 ) and cases which treatment may begin by the age of 1011.11 the use of teleradiography for pa projection for facial asymmetries must be carried out with great care , considering the difficulty in locating the cephalometric points in this projection.12 , 13 moreover , it should be kept in mind that even slight rotations of the head in the cephalostat might mask the presence of facial asymmetry.12 , 14 cone beam computed tomography ( cbct ) guarantees the volumetric graphic 3d representation of all anatomical bony structures , as well as overcoming the limitations of ordinary 2d radiographic imagesi.e. 
geometric distortion and superimposition of bony and dental structures , and improper positioning of the patients head in the cephalostat15since usual practice continues to favour 2d , even though 3d16 cephalometric analyses do exist . 1 3 la radiologia medica ( 2019 ) 124 : 887916 routine prescription of this examination for young patients is considerably limited , by both the literature and all the existing guidelines , 15 , 17 upon radiation dose , to individual clinical cases . 
it should be highlighted , though , that it is current common practice among orthodontists to convert 3d images into 2d , for cephalometric analysis.15 , 17 in all cases , choosing the fov is crucial when prescribing this examination , in order not to expose the patient to a non - optimised radiation dose with an acquisition field too extensive for the target zone . 
in orthodontics , small and medium fovs are indicated for the assessment of impacted teeth , root resorption caused by impacted teeth , and the designated area for mini - screw insertion in patients with malocclusion.14 , 1820 moreover , successful application of mini - implants is influenced by cbct14 evaluation of bone density , as it reduces the risk of screw detachment . 
in all these cases , with one single exposure , despite the higher radiation dose being used , the orthodontist and the oral and maxillofacial surgeons get access all the required information . the use of large fovs for a 3d cephalometric examination in simple clinical cases is not validated by the literature , nor by existing guidelines.17 temporomandibular disorders ( tmd ) affect the temporomandibular joint ( tmj ) , the masticatory muscles and associated structures . 
in a recent update , the american academy of orofacial pain divided tmds into two large categories : tmj disorders and masticatory muscle disorders.24 the prevalence of tmd in newborns , children and teenagers is highly variable in the literature , inasmuch as data between 6 and 68% are reported . 
 radiological examination is only indicated when insufficient information is obtained from the anamnesticclinical examinations.24 , 34 different radiological techniques are employed in study of the tmj , with different sensitivities , specificity and appropriateness in relation to the diagnostic question . 
 magnetic resonance ( mr ) and computed tomography ( ct ) and / or cbct scanning should be preferred over conventional radiography . ct is held to be the gold standard imaging technique for bone lesion assessment , while mri is considered the gold standard for ligament and articular capsule structure analysis.24 , 34 recommendation no . 
1 for acorrect orthodontic diagnosis andtreatment planning , apanoramic radiography andateleradiography are necessary strength ofrecommendation : adegree ofevidence : i teleradiography of the skull in norma lateralis , panoramic radiography and radiography of the non - dominant hand and wrist should be prescribed based on the degree of malocclusion ( iotn ) 10 and the patients age.17 frequent radiographic checkups to monitor progress of therapy are advised against and inappropriate , unless there is a precise clinical indication . in case of serious craniofacial dysmorphoses or of skeletal iii class , orthodontic treatment will begin early , getting radiographic records of the patient is advisable at an early stage . 
2 limit prescription ofcbct and , preferably , use small andmedium fovs strength ofrecommendation : adegree ofevidence : i in the past decade , a considerable increase in the use of cbct in dentistry , especially in orthodontics , was witnessed . 
nonetheless , numerous recent guidelines and studies have drastically limited prescription of cbct to selected clinical cases . cbct is therefore indicated for diagnosis and treatment planning for severe dysmorphosescraniofacial syndromes , impacted teeth , bone anomalies , serious facial asymmetries and condylar aplasia or hypoplasia.17 1 3 904 recommendation no . 
4 posterioranterior teleradiography , withrelated cephalometric analysis , requires ahighly experienced clinician strength of recommendation : a degree of evidence : i cephalometric analysis of the posterioranterior teleradiograph , compared to the latero - lateral analysis , requires the clinician to have extensive experience , as localisation of the cephalometric points is far more complex due to bone superimpositions . 
they are insufficient for assessment of la radiologia medica ( 2019 ) 124 : 887916 the bony structures ( condyle and glenoid cavity ) and may reproduce the condyleglenoid cavity relationships unreliably , due to projection errors bound to the imaging technique.24 , 34 bibliography k . 
diagnostic criteria for temporomandibular disorders ( dc / tmd ) for clinical and research applications : recommendations of the international rdc / tmd consortium network * and orofacial pain special interest groupdagger . 
clinical classification of 1416 - year - old danish children according to functional status of the masticatory systecommunity dent oral epidemiol 1988 ; 16 : 4751 . pahkala r , laine t , narhi m , ettala - ylitalo um . 
pediatric dentistry sept - oct 2015 ; 37 ( 5 ) : 7884 . guarnieri r , cavallini c , vernucci r , vichi m , leonardi r , barbato e . 
med oral patol oral cir bucal 2016 ; 21 : e743 - e750 . 1 3 906 la radiologia medica ( 2019 ) 124 : 887916 diagnostic imaging incraniomaxillofacial malformations recommendation no . 
craniosynostoses and craniofacial stenoses , as well as orofacial clefts and branchial arch syndromes , are an example . since we are dealing with deformations that are often present at birth , radiographic investigations should be proportionate to the diagnostic and therapeutic objectives of the single case.6 , 13 the golden rule is that radiographic investigations should be carried out only when they are essential to diagnosis and treatment planning.6 , 13 , 14 by way of example , the diagnosis of skull malformations and of cranial suture anomalies is purely clinical.3 , 13 , 14 , 15 direct x - ray imaging is not indicated as a routine examination , since the same information may be obtained by ultrasound imaging.2 , 5 , 15 , 24 multislice computer tomography ( msct ) or cbct is indicated in selected cases , when necessary for treatment planning.15 , 22 msct and cbct are not indicated as a routine examination for cleft lip and palate , since their diagnosis is clinical . 
2 diagnosis ofcraniostenosis isstrictly clinical , 4 , 14 , 15 , 18 , 21 butct may be of assistance23 strength ofrecommendation : adegree ofevidence : ii for treatment planning , a ct examination is indicated.5 , 14 , 23 for suspected anomalies of the cranial sutures and the anterior fontanelle , an ultrasound examination is often sufficient.2 , 5 , 15 , 24 msct orcbct may be indicated foranalysis ofi andii branchial arch syndromes craniofacial defects andwiththepurpose oftreatment planning.1 , 7 , 8 , 14 , 15 , 17 , 18 , 20 strength of recommendation : a degree of evidence : ii in cranio - maxillofacial defects , cbct may be indicated as an investigation alternative to msct , 2 , 24 since the radiation dose , based on scientific evidence , is lower where evaluation of the soft tissues is not required.3 , 6 , 9 , 19 , 23 bibliography adam m . 
australian dental journal 2014 ; 59 ( 174185 )  . boeddinghaus r , whyte a / european journal of radiology 66 ( 2008 ) 396418 . cabrera - martos i etal . 
2011 jan ; 22 ( 1 ) : 47 kuijpers mar , chiu yt , nada rm , carels cel , fudalej ps ( 2014 ) three - dimensional imaging methods for quantitative analysis of facial soft tissues and skeletal morphology in patients with orofacial clefts : a systematic review . 
2015 oct ; 37 ( 8 ) : 989 diagnostic imaging indental anomalies tooth impaction . an impacted tooth is one that , somehow , fails to erupt in the oral cavity within the expected developmental window.1 an impacted tooth may also be defined as a tooth , which is partially or not erupted , showing clinical , anatomical and radiological signs that suggest its correct eruption is unlikely.2 dental impaction is a common problem ( 2550% of the world population ) , which prevalence is strongly related to age , gender , ethnicity and anatomical localisation ( quadrants ) , 3 , 4 while its incidence appears to be increasing.5 the teeth of normal permanent dentition that are most often impacted are , in order of frequency , third molars , upper canines , premolars , and upper central incisors.6 in europe , impaction of third molars is observed in more than 70% of young adults , 7 and extraction of third molars is the most frequent procedure in oral surgery . possible causes of dental impaction are lack of space , position anomalies , supernumerary teeth , persistence of primary teeth , odontogenic cysts / tumours , trauma and systemic diseases . 
1 on suspicion ofdental impaction , level i radiological examination must notbe carried outbeforetheage of6 strength of recommendation a degree of evidence i at 6years of age , permanent tooth buds , except those of the iii molars , are visible in the panoramic image , a level i radiographic investigation . 
2 la radiologia medica ( 2019 ) 124 : 887916 impacted tooth and its relationship with adjacent anatomical structures , especially with the maxillary sinus floor.19 , 21 on suspicion ofdental impaction , orthopantomography should be thefirst diagnostic examination recommendation no . 
this image provides information on the position of the impacted tooth , its relationship with the alveolar ridge , its projective relationships with the adjacent teeth and structures and the presence of any associated lesions ( radiotransparent and / or radio - opaque periradicular lesions ) .12 however , 2d imaging techniques turn out to be less accurate in assessing dental impaction than 3d cbct . 
3 level i radiographic investigations are anefficient tool indefining therisk ofinjuring thealveolar nerve and , innoncritical cases , may be considered sufficient intreatment planning fortheextraction ofaiii lower molar strength ofrecommendation adegree ofevidence iv with reference to impaction of the third lower molars , orthopantomography , and , in some cases , intraoral radiography , is an efficient imaging technique for estimating the risk of injuring the lower alveolar nerve.14 , 15 so , if level i radiographic investigations exclude any chance contact between the iii lower molar and the mandibular canals , 2d imaging may be held to be sufficient and 3d cbct imaging unnecessary.16 , 18 recommendation no . 
in particular , identifying and evaluating the extent of an external root resorption processsometimes observed in dental impaction , especially in the upper caninesrequire a 3d evaluation.22 , 24 so , on suspicion of external root resorption associated with dental impaction , a 3d cbct imaging technique is indicated.22 , 25 recommendation no . 
6 periapical intraoral imaging may be used fordental impaction oftheupper incisorcanine region strength ofrecommendation : b degree ofevidence : iv periapical radiography is an imaging technique generally used in dentistry to evaluate periapical lesions , root morphology ( when planning extraction / endodontic treatment ) and post - implant surgery checkup . 
this anomaly , only found in permanent dentition , causes an alteration of the normal sequence in the dental arch.28 , 29 tooth transposition may be found in two forms , complete ( true / complete transposition ) and incomplete ( pseudo / incomplete transposition ) .30 in its complete form , transposition involves the whole permanent tooth ( crown and root ) , while , in the incomplete form , only the crown is involved . transposition is a relatively rare , usually unilateral , anomaly , which prevalence in the population is around 0.3%.28 it is more frequently found in female patients ( female / male ratio 3 : 1 ) and in the upper arch , 29 and it is often associated with other dental anomalies.31 in most cases , tooth transposition occurs between the canine and the neighbouring teeth , in particular between the upper canine and first premolar , followed by transposition between the upper canine and lateral incisor ( 28 , 29 )  . the aetiology of tooth transposition remains unknown to date . 
1 on suspicion oftooth transposition , level i radiological investigation should notbe carried outearlier thantheage ofsix strength of recommendation : a degree of evidence : i at age 6 , permanent tooth buds , third molars excepted , are visible on the panoramic image . 
2 on suspicion oftooth transposition , theindicated level i radiological investigation isorthopantomography , which may be sufficient fortreatment planning strength ofrecommendation : adegree ofevidence : i level i radiographic investigations are the first step in the diagnostic approach to tooth transposition , and the panoramic image is indicated in order to confirm diagnostic suspicion . 
the main advantages , compared to those of intraoral images , are it shows both jaws in one single two - dimensional image , and it allows reducing exposure to radiation ( 10 times less than radiographic status ) .11 there is no clinical evidence supporting the use of cbct as an initial diagnostic examination for tooth transposition . 
4 intraoral periapical imaging may be used intooth transpositions strength ofrecommendation : b degree ofevidence : v periapical radiography is an imaging technique generally used in dentistry to evaluate periapical lesions , root morphology ( when planning extraction / endodontic treatment ) and post - implant surgery checkup . 
this radiographic image provides information on the number and position of supernumerary teeth , their relationship with the alveolar ridge , the projective relationships with teeth and adjacent structures and the presence of any associated lesions ( radio - transparent lesions and / or periradicular radio - opaque lesions ) .12 however , in the assessment of a supernumerary tooth that has caused dental impaction , 2d imaging techniques turn out to be less accurate than 3d cbct . 
in particular , it should be considered that 2d imaging is significantly less effective than 3d imaging in establishing correct positioning of the supernumerary teeth with regard to adjacent structures ( teeth and critical structures such as the mandibular canal , the nasal fossa and the maxillary sinus ) 13 and also in supplying necessary information for correct surgical planning . 
it may occur in a sporadic form or associated with hypodontia , within the picture of genetic syndromes . the term dilaceration describes the presence of a sharp curvature of the root with regard to the crown . 
according to some authors , for a tooth to be defined as dilacerated , the angle formed by the axis along the root must be 90 , while others say 20.33 the aetiology of dilaceration is not fully known yet . 
the most supported explanation is that this shape anomaly results from a traumatic event , occurring to the corresponding deciduous tooth in early childhood , even though idiopathic forms are described , probably consequent upon ectopic development of the tooth germ.33 dens invaginatus ( dens in dente ) is an anomaly mainly involving the upper lateral incisors and originates from infolding and consequent development of part of a tooth within another tooth . the fusion and germination of two neighbouring permanent germs determine the formation of teeth with separate pulp chambers and completely fused , either at the level of 1 3 la radiologia medica ( 2019 ) 124 : 887916 the crown in the former case or with a single pulp chamber in the latter . 
 2012 ; 54 ( 2 ) : 197203 . celikoglu m , miloglu o , oztek o ( 2010 ) investigation of tooth transposition in a non - syndromic turkish anatolian population : characteristic features and associated dental anomalies . 
2015 aug 15 ; 8 ( 8 ) : 118905 . diagnostic imaging indental traumatology for dento - alveolar traumatology , please refer to guidelines for prevention and clinical management of dental trauma in children and adolescents ( 2012 ) ( 1 , 11 , a )  . diagnostic imaging in dental trauma is used to evaluate the degree of root formation of the tooth affected by trauma and to assess tooth displacement or possible root fracture . 
2 periapical intraoral xray isnecessary inthediagnostic investigation ofdentoalveolar trauma inpaediatric patients strength ofrecommendation : adegree ofevidence : iv periapical intraoral x - ray performed with an adequate paralleling system is the imaging technique of choice , which finds indication in identifying dento - alveolar modifications subsequent to localised trauma . 
dental radiographic examinations : recommendations for patient selection and limiting radiation exposure ; 2012 . govindarajan m , reddy vn , ramalingam k , durai ks , rao pa , prabhu a . 
dental trauma guide : a source 1 3 914 la radiologia medica ( 2019 ) 124 : 887916 a e.gov.it / imgs / c_17_pubbl icazi diagnostic imaging for caries and periodontal disease . strength of recommendation : a degree of evidence : i of evidence - based treatment guidelines for dental trauma . 
in all patients , when carious lesions are suspected in permanent teeth , the favoured radiographic image of choice is the bitewing . this film size is large enough to evaluate the whole crown of a permanent tooth . 
intraoral x - ray is indicated for assessment , over time , of the periapical and pulp health conditions of permanent teeth that have undergone conservative treatment of the dental pulp . 
intraoral x - ray is indicated for periapical health condition periodical assessment of mature or immature teeth that have undergone provisional endodontic treatment ( apecification ) , pulp regeneration or definitive rct . 
msct or cbct may be indicated for analysis of i and ii branchial arch syndrome craniofacial defects with the purpose of treatment planning . strength of recommendation : a degree of evidence : i strength of recommendation : a degree of evidence : ii strength of recommendation : a degree of evidence : ii strength of recommendation : a degree of evidence : i strength of recommendation : a degree of evidence : iv strength of recommendation : a degree of evidence : iv strength of recommendation : b degree of evidence : iv strength of recommendation : a degree of evidence : iv strength of recommendation : b degree of evidence : iv strength of recommendation : a degree of evidence : iv strength of recommendation : a degree of evidence : i strength of recommendation : a degree of evidence : i strength of recommendation : a degree of evidence : v strength of recommendation : b degree of evidence : v strength of recommendation : a degree of evidence : iv 1 . 
cbct is the level ii examination indicated for selected cases in which level i investigations ( periapical intraoral radiography ) do not supply sufficient diagnostic information for suitable therapeutic planning . glossary strength of recommendation : a degree of evidence : iv strength of recommendation : a degree of evidence : iv strength of recommendation : a degree of evidence : iv strength of recommendation : a degree of evidence : iv diagnostic imaging in dental traumatology . alara as low as reasonably achievable : each exposure to radiation must be kept as low as it is reasonably achievable base on both economic and social considerations . 
under these circumstances , it is reasonable to minimise a risk that may be presumed to exist also at levels lower than the recommended limits , considering that what fovfield of view : the field of investigation prescribed in order to avoid subjecting the patient to useless radiation with areas of acquisition that are over - extensive with regard to the district under examination . 
availability of different fovs ( small , medium , large ) depends on the device used . iotnindex of orthodontic treatment need : devised to rate the need for an orthodontic treatment based on dental position alterations that may be associated with selected functional alterations . 
besides being used for epidemiological research , it is also used as a tool by the national health service to assess childrens orthodontic treatment priority and eligibility for free care . 
the iotn index has 5 classes for orthodontic condition grading . drlsdiagnostic reference levels : radiation dose levels for each diagnostic imaging system or , in nuclear medicine diagnostics , levels of activity , for each type of examination , performed with standard appliances , for groups of patients of standard body size or for standard dummies . 
for six selected radiologists , the number and types of reported examinations as well as the related radiology report turnaround times ( rtats ) were analyzed in detail and compared between the two 1 - year periods . results overall , there was a significant increase of 10.3% in the total number of examinations performed in the whole department in 2016 compared with 2014 . 
subspecialized reporting allows the individual radiologist to focus on a special field of professional competence but can result in longer overall rtat . keywords subspecialization reporting time professional competence radiologists * martin h . 
15 , 81377munich , germany vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 860869 introduction a high degree of subspecialization among referring physicians from different clinical specialties has implications for radiologists in that it requires increasingly specialized diagnostic skills tailored to the specific needs of referrers [ 1 , 2 ]  . 
referring physicians expect radiologic examinations to adhere to high technical standards and expect high - quality radiology reports to be available within a short time [ 3 ]  . in this era of lower health care spending and reimbursement models mostly based on the payment of fixed amounts per service , efficient organization of examination and reporting workflow becomes essential for both hospital - based and officebased radiologists [ 46 ]  . 
in europe , radiology departments and practices organize reporting workflow by imaging modality such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) , mammography , and conventional radiography . an alternative to general reporting is subspecialized reporting . 
with this option , reporting is organized by organ system such as abdomen , chest , musculoskeletal , and vascular system , and radiologists form teams focusing on the examination of one organ system with any imaging modality [ 7 , 8 ]  . 
using subspecialized reporting , radiologists can develop in - depth skills and experience in a specific area , allowing them to better meet the needs of subspecialized referring physicians and ensuring consistently high reporting quality [ 9 , 10 ]  . 
in addition to improving quality , subspecialized reporting has the potential to also enhance reporting efficiency . based on these considerations , the radiologic department of a swiss university hospital introduced an internal subspecialized examination and reporting system in mid - 2015 . 
the subspecialties defined were thoracic and cardiovascular imaging , abdominal and urogenital imaging ( including mammography ) , musculoskeletal imaging , and emergency imaging . in this study , we analyzed the effects of switching from general to subspecialized reporting on reporting workflow in a representative group of radiologists from our department who worked under both systems during the study period . 
specifically , we investigated how the implementation of subspecialized reporting altered the range of types of examinations reported by individual radiologists and reporting efficiency in terms of reporting volumes and radiology report turnaround time ( rtat )  . materials andmethods we conducted an internal analysis in the radiology department of a swiss university hospital to compare workflow before and after implementation of subspecialized reporting . 
subspecialized reporting was introduced on may 1 , 2015 . before the introduction of subspecialized reporting in 2015 , the radiologists selected for this analysis worked by imaging modality , i.e. , ct , mri , conventional radiography , and mammography . 
rtat was defined as the interval from the end of the examination to finalization of the report . for detailed analysis , six radiologists who worked in the department throughout the two 1 - year periods under investigation were selected . 
the preliminary report is then discussed with the staff or senior radiologist responsible for the respective modality and then finalized by the latter after any necessary editing was done to minimize effects of outliers or of imaging material only stored in the picture archiving and communication system ( pacs ) for documentation purposes on the calculation of average rtats . all data for the analysis were extracted from the radiology information system ( ris ; centricity ris - i 4.2 plus , ge medical systems , milwaukee , wi , usa )  . 
the following data were recorded : type of examination , date of examination , end of examination , beginning and end of reporting time , and finalizer . for each report , rtat was calculated in minutes . 
for comparison of rtats before and after introduction of subspecialized reporting , the following classification was used : more than 2h shorter with subspecialized reporting [ ] , 12h shorter with subspecialized reporting [ ] , no more than 1h longer or shorter with subspecialized reporting [ 0 ] , 15h longer with subspecialized reporting [ + ] , more than 5h longer with subspecialized reporting [ + + ]  . statistical analysis the cochranmantelhaenszel test was used to test for significant differences in the number of different types of examinations following the introduction of subspecialized reporting for all six radiologists taken together . 
the chisquare test was applied to analyze possible differences in the comparison of individual radiologists . changes in the range of examinations reported by each radiologist in terms of a shift toward a higher share of subspecialized imaging studies were assessed using a one - sided cochranmantelhaenszel test . 
the impact of subspecialized reporting on the range of types of imaging studies reported by each radiologist was assessed by the chi - square test . whether subspecialized reporting had a significant effect on rtat was tested for each radiologist using a two - tailed mannwhitneywilcoxon test and was based on an analysis of the subset of the 10 most common types of imaging studies reported by that radiologist in 2016 . 1 3 la radiologia medica ( 2019 ) 124 : 860869 fig . 
with the introduction of the subspecialized reporting system , teams for different organ systems or body regions were formed , who worked independently of the imaging modality used for the examination . 
the subspecialties defined were thoracic and cardiovascular imaging , abdominal and urogenital imaging ( including ent imaging and breast imaging ) , musculoskeletal imaging , emergency imaging , and pediatric imaging . 
statistical calculations were done using the r software ( r foundation for statistical computing , vienna , austria )  . results we included a total of 67 , 585 reports from 2014 and 72 , 224 reports from 2016 . 
 the proportion of reports finalized within the evaluated 72 - h period was 97.8% in the full year before and 95.2% in the full year after implementation of a subspecialized reporting . for each of the six radiologists , introduction of the subspecialized system led to an approximately 25% reduction in the range of examination types reported . 
the reduction was statistically significant for five of the six radiologists ( p < 0.05 , see table2 )  . this reduction was associated with an increase in the share of reports pertaining to the respective subspecialty for four of the six radiologists . 
following introduction of subspecialized reporting , this radiologists 10 most commonly reported types of examinations accounted for 78.1% of his / her overall reporting volume in his / her specialized area . 
on the contrary , rtats were in part even markedly longer after switching to subspecialized reporting . these findings must be interpreted in light of an overall increase of approximately 7% in the departments total reporting volume , and this increase in workload also included the six radiologists selected for this study . 
the increase in imaging studies performed by our department is in agreement with general national and international data indicating a steady increase in radiologic examinations [ 11 , 12 ]  . as expected , the introduction of subspecialized reporting in 2016 led to a concentration on examinations of the respective subspecialties among the six radiologists included in our analysis in that the range of different examination types reported became smaller for all of them compared with 2014 ( see table2 )  . 
reporting of a narrower range of examinations was especially conspicuous for radiologist a ( who became head of the abdominal imaging team with the introduction of subspecialized reporting , 30% decrease ) and radiologist c ( head of the thoracic and vascular imaging team , 34% decrease )  . as expected after switching to the new system , subspecialized reports accounted for a higher proportion of the total reporting volume ( for examinations performed during standard weekday working hours ) in 2016 compared with 2014 . 
this high increase is attributable to the fact that , with his / her extensive expertise and experience , radiologist a covered nearly the complete range of imaging studies in his / her reporting activities under the earlier general reporting system ; hence , the impact of subspecialization was especially marked . 
in contrast , the range of examination types reported by radiologist e ( head of pediatric imaging before and after introduction of the new system ) was nearly unchanged after the switch of systems . 
this is not surprising since pediatric radiology with its focus on examinations tailored to the specific needs of young patients already was a largely autonomous unit before the introduction of subspecialized reporting . while a concentration on the defined subspecialties was expected , it was surprising that subspecialized reporting , rather than making reporting workflow more efficient , even resulted in longer rtats for many types of examinations . 
a possible explanation is that a large proportion of residents , as in our department , which is one of the largest teaching institutions for radiology residents in switzerland , results in a more complex and time - consuming reporting workflow . 
 [ 13 ] show that , median rtats can be dramatically shortened , from approximately 17h to approximately 3h and 30min , when fully trained radiologists directly report imaging studies under a subspecialized system . another , specific factor contributing to longer rtats for radiologist a in our analysis may be that , as head of the abdominal imaging team , he / she was also responsible for all complex reports and imaging examinations revealing rare findings . 
an effect of this policy is that radiologist a tends to get a large share of difficult abdominal imaging cases for a second opinion . conversely , for radiologist b ( head of emergency imaging ) , focusing on a specialized range of examinations to be reported ( 28% decrease , from 87 to 63 types of examinations , in 2016 , see table 2 ) resulted in consistently shorter or nearly unchanged rtats compared to 2014 ( see table3 radiologist b )  . 
moreover , the spatial arrangement , with the supervising radiologist being based directly next to the emergency ct scanner during standard weekday working hours , facilitates workflow and finalization of preliminary reports generated by the residents of the team . overall , our results show that subspecialized reporting has not only benefits but also disadvantages and risks . 
greater in - depth skills in a well - defined area of their field allow radiologists to solve more complex problems , which is likely to have a positive mental effect . 
 in addition , the growing complexity of a specialty like radiology makes it more and more difficult for an individual radiologist to master all its many facets with the required depth of expertise [ 17 , 18 ]  . subspecialization can also have a positive impact on residents who rotate through different fields of radiology during their training . 
clearly defined rotations allow radiologists to focus on a specialized area for a predefined time [ 19 ] rather than having to constantly switch between many different types of examinations . 
various studies have so far shown that subspecialization in radiology can lead to a higher quality and precision in radiologic reports in the individual sub - disciplines [ 20 , 21 ]  . 
we could also recognize this effect in our clinic after the implementation of a subspecialized reporting systealthough it was not the aim to quantify changes in the quality of reports after introducing a subspecialized system , we nevertheless achieved an apparently significantly higher perceived quality among our referrals with multiple positive feedbacks . on the other hand , subspecialization can have negative effects [ 22 ] , because repetition can be boring and less motivating . 
monotony can lead to greater fluctuation , making staff to leave and seek employment where they work on a broader , more generalized range of imaging studies if they prefer such an approach to focus on a narrow subspecialized area . 
from our perspective , there are different possible reasons for this : ( 1 ) the number of reports that are being sent between different senior radiologists to get a second opinion had significantly increased after the implementation of the subspecialized systein a radiology information system ( ris ) database research , we found that there were only about 2% of the reports signed by two senior radiologists in 2014 , while this percentage increased to over 10% in the year 2016 . 
a possible reason for this especially in the group of abdominal imaging was that reporting on liver imaging was dedicated to three specific radiologists with the best experience in this field . 
obviously , this not only leads to a higher quality of the reports , but also causes longer reporting time ; ( 2 ) difficult findings and reports are intentionally withheld by individual specialized radiologists in order to first discuss these with the referring colleagues in a weekly tumor board . 
the reports then become more focused and there are fewer misunderstandings in difficult situations , but the reporting time increases ; ( 3 ) nonurgent reports were not finally completed before weekends or public holidays . according to the directive of the european union as of february 2018 , it is mandatory for the member states to make sure that for radiologic examinations which are based on ionizing radiation , the dose is being documented afterward in the radiologic report ( article 58 , b ) [ 23 ]  . 
this is due to the fact that we wished to include radiologists from each of the four subspecialized areas introduced with the new systemoreover , all radiologists selected had to be present throughout the two study periods , i.e. , throughout 2014 and 2016 , without longer leaves of absence . 
 the involvement of residents in reporting workflow in all areas including complex and highly specialized imaging studies further contributed to a much greater complexity and hence longer rtats in our study . 
from our perspective , ultrasound is different from all the other diagnostic methods like ct , mri or conventional radiography as the reporting time as a part of the overall procedure time is less important than for all the other procedures . 
cchf is a life - threatening disease observed endemically over a wide geographical regions in the world , and there is limited information about pulmonary findings in cchf patients . purpose we aimed to investigate the pulmonary findings belonging to a large cchf patient cohort and to determine if there is any relationship between laboratory findings and disease severity . materials and methods a total of 165 patients who were diagnosed with cchf and examined through chest x - ray ( cxr ) due to respiratory symptoms at their first examination and / or during their hospitalization were included in this study . 
the general non - specific symptoms of cchf are fever , malaise , * fatma akta fatmakokcu79@hotmail.com 1 department ofradiology , faculty ofmedicine , gaziosmanpaa university school ofmedicine , 60100tokat , turkey 2 pulmonary diseases department , versa hospital , nevehir , turkey anorexia , nausea / vomiting , and myalgia , which are observed after the contact . 
in addition , intracranial bleeding , gastrointestinal bleeding , and alveolar hemorrhage that are life - threatening and often responsible for mortality can be observed as well [ 14 ]  . 
however , the number of studies related to pulmonary imaging in cchf is very rare and limited despite the increasing number of cases in the world and in our country [ 14 ]  . 
 we may propose simple pulmonary imaging such as cxr to be used within the following 5days after the first examination as an effective tool to evaluate clinical course and severity of the disease . the aim of this study was to investigate the chest x - ray findings of cchf patients with respiratory findings and to determine if there is any relationship between the laboratory findings and severity of the disease . materials andmethods a total of 464 patients with confirmed cchf were admitted to emergency department and department of infectious diseases and clinical microbiology between january 2011 and december 2016 . 
 patients using medicines that may cause pulmonary toxicity and having acute or chronic lung diseases , malignancies , heart diseases , and blood diseases , and a history of thoracic radiotherapy or surgery in addition to cchf were excluded from the study . 
additionally , patients who were clinically diagnosed with pulmonary infection ( such as cough sputum ) and who were diagnosed with other microorganisms in their cultures were not included in the study as well . ethical approval was obtained from ethics committee of the university . 
in addition to demographical findings of the patients such as age , gender , occupation , place of residence , tick exposure , clinical findings , and medical history , laboratory findings and radiological images of lungs were evaluated . 
the cchf diagnosis was made based on the detection of virus genome by using enzyme - linked immunosorbent assay ( elisa ) or polymerase chain reaction ( pcr )  . statistical analysis data are expressed as mean standard deviation . 
 out of 40 patients with comorbidity , 23 were found to have hypertension , three of them had diabetes mellitus , 13 were diagnosed with both hypertension and diabetes mellitus , and one of them had hypothyroids . 
the frequency of general symptoms of the patients observed during the first examination is presented in table2 . based on the laboratory findings , the mean values of liver - specific enzymes such as alkaline phosphatase ( alp ) , alanine aminotransferase ( alt ) , aspartate aminotransferase ( ast ) , gamma - glutamyltransferase ( ggt ) , creatine kinase ( ck ) , and lactate dehydrogenase ( ldh ) were seen to be high . single and / or multiple abnormal imaging findings were detected in 93 patients ( 56.4% ) as a result of cxr examination during the first examination . 
in a similar vein , four patients , claimed to have ground glass densities on cxr , and one patient , claimed to have pleural effusion , were not found to have these findings according to the results of the thorax ct . 
the comparison of survival and cxr findings of patients is shown in table5 . discussion cchf is a life - threatening zoonotic viral disease that can be seen endemically in many regions in the world . 
the most frequent clinical symptoms are fatigue ( 92.3% ) , fever ( 89.4% ) , myalgia ( 69.7% ) , headache ( 68.1% ) , and nausea ( 64.7% ) ; 23% of patients had bleeding ( petechiae , epistaxis , gingival bleeding , vaginal bleeding , and bleeding in internal organs ) [ 10 ]  . 
this situation might be related to the possibility that males work in occupations with high risk of being in contact with ticks . as in many other viral diseases , cchf may cause symptoms of pulmonary involvement and may lead to death . 
the results of the thorax ct revealed that 20 of these patients ( 86% ) had pleural effusion , 12 of them ( 52% ) had consolidation , nine ( 39% ) had atelectasis , and 14 ( 60% ) had 1 3 la radiologia medica ( 2019 ) 124 : 826832 fig . 
however , hemoptysis was detected in a total of nine out of 27 patients with hemorrhage ( six of those patients died )  . there have been a very limited number of studies on pulmonary radiological findings in cchf in the literature . 
however , it has been stated that it can share similarities with mechanism of pulmonary pathologies such as pleural effusion , pneumonitis , hemoptysis , and alveolar hemorrhage in other febrile viral hemorrhagic diseases [ 15 , 16 ]  . 
in a study performed on dengue hemorrhagic fever , a total of 468 cxr taken from 363 patients were examined and parenchymal infiltration and pleural effusion were observed in more than half of the patients on the third day of follow - up . 
 moreover , these radiological findings were found to be closely related to laboratory findings of leukocyte count , platelet count , aptt , alt , and albumin levels in the same study [ 18 ]  . 
 in conclusion , pleural effusion and other findings related to pulmonary involvement can be seen in cchf due to endothelial damage caused by viral load in the circulation , increased capillary permeability , and hemorrhages due to low platelet . in the study by akta etal . 
the results of the study revealed that there was no statistically significant difference between the two examination techniques in terms of detecting parenchymal infiltration , alveolar infiltration , and pleural effusion . 
when these patients were compared , it was found that there was consolidation in cxr of the four patients and pleural effusion in one patient while they were not observed in thorax ct . 
on the other hand , based on thorax ct results , ground glass density was detected in four patients and atelectasis in two patients , and these were not observed in cxr . 
therefore , there was a possibility of response to the treatment and spontaneous regression or progression in the findings . the mortality rate of cchf generally ranges from 2 to 80% . 
this result can be associated with the fact that cchf is endemic in this region ; therefore , medical staff and people are informed about the disease , and thus , they are alert . 
in addition , the experience in the clinical follow - up might also contribute to the decrease in mortality rate besides improvements in medical care conditions in cchf and increase in awareness of the seriousness of the disease . it is known that mortality and some laboratory parameters prolonged a ptt , increased inr , high alt , ast and ldh , low platelet , and increased leukocyte are related to each other [ 23 , 24 ]  . 
for this reason , all of the cchf patients who were found to have pathologic cxr result should be considered at high risk . our choice to conduct a retrospective study is the first limitation ; on the other hand , medical information of the patients and their radiological images has been recorded in a proper way . 
the other limitation was the inability to confirm the cxr findings of the patients as not all of these patients had thorax ct . in conclusion , cchf is a serious public health problem that can be fatal . 
according to the results of our study , we suggest that 1 3 832 la radiologia medica ( 2019 ) 124 : 826832 radiological imaging of pulmonary system should be performed primarily with cxr . 
pulmonary involvement ( pleural effusion , consolidation , and ground glass opacity ) affects the survival in cchf negatively , and further examination should be performed with thorax ct in case of necessity . 
to detect urine leakage , we initially performed conventional cystography after retrograde distention of the bladder with dilute iodinated contrast material , followed by ultra - low - dose ct cystography . 
the diagnostic accuracy of these two modalities was compared , and the technical characteristics of ultra - low - dose ct cystography were examined . results all 31 referred patients were included in this study . 
of the 31 patients , 27 ( 87.1% ) underwent bladder repair after radical prostatectomy , 3 ( 9.7% ) after radical cystectomy , and 1 ( 3.2% ) after bladder diverticulectomy . 
based on these findings , we were able to establish a proper treatment plan . conclusions ultra - low - dose ct cystography is an accurate method for evaluating urine leakage after bladder repair , and this technique may help determine the most appropriate treatment strategy for patients with urine leakage after bladder repair . keywords anastomotic leakage radiation dosage computed tomography fluoroscopy introduction recently , awareness and concern about radiation exposure have increased . 
in the republic of korea , the number of radiation - generating devices has rapidly increased * seong hoon choi 0733280@uuh.ulsan.kr 1 department ofurology , ulsan university hospital , university ofulsan college ofmedicine , ulsan , korea 2 department ofradiology , ulsan university hospital , university ofulsan college ofmedicine , 877 bangeojinsunwando - ro , dong - gu , ulsan44033 , korea from 59 , 739 in 2008 to 72 , 626 in 2012 [ 2 ]  . 
in a study involving conventional non - contrast ct , the reported exposure dose ( ed ) for the abdomen and pelvis was between 10 and 20msv [ 6 ]  . 
therefore , if dose - reduced ct can be shown to accurately diagnose bladder injury , low - dose and ultra - lowdose ct could be applied to a wide variety of cases . one of the advantages of ct compared with conventional cystography is the ability to detect anatomical relationships . 
 a major concern associated with dose - reduced ct is higher noise , which results in lower image quality that may reduce the accuracy of this technique for detecting anatomical relationships and facilitating differential diagnoses . 
moreover , while low - dose and ultra - low - dose ct are effective for detecting urolithiasis [ 7 , 11 ] , it remains uncertain whether low - dose ct cystography can detect bladder injury or urine leakage . 
therefore , we performed a prospective cohort study to compare the accuracy and technical characteristics of ultra - low - dose ct cystography with those of conventional retrograde cystography . materials andmethods study participants from november 2015 to october 2017 , we prospectively examined 31 consecutive patients referred for cystography after bladder repair . 
 to diagnose urine leakage , we initially performed conventional cystography after retrograde distention of the bladder with dilute iodinated contrast material , followed by ultralow - dose ct cystography ( table1 )  . imaging technique andinterpretation conventional cystography was performed in the following manner : with the patient supine on the examination table , the urine bag was disconnected from the foley catheter and the foley catheter was suctioned using a 50 - ml syringe until the bladder was completely emptied . 
additional pelvic ap radiographs were obtained after the initial infusion of approximately 100ml of contrast material and after either infusion of another 150ml of contrast material or occurrence of one of the following endpoints : ( 1 ) 300ml of contrast material was completely infused into the bladder , ( 2 ) urinary leakage occurred due to continuous bladder detrusor activity with infusion less than 300ml , or ( 3 ) the patient complained of pain in the abdomen and pelvis . 
oblique radiographs were also obtained , followed by an ap radiograph after bladder emptying . ct cystography was performed in the following manner : with the patient supine on the examination table , the foley catheter was suctioned using a 50 - ml syringe , as described above . 
ultra - low - dose ct images were reconstructed using idose level 5 , which is one of the iterative reconstruction ( ir ) algorithms [ 12 , 13 ]  . 
the ct parameters were as follows : a pitch of 0.915 , collimation of 0.625mm , matrix size of 512 512 pixels , sectional thickness / reconstruction interval of 2mm , collimation of 2 64 0.6mm , pitch of 1.2 , and gantry rotation time of 0.5s. 
the reductions in radiation dose were compared between the two modalities and also with regard to the patients bmi [ 14 ]  . image findings were interpreted by an expert radiologist in the genitourinary division of the radiology department of our institution . 
the following conventional cystography and ct cystography findings were recorded : ( 1 ) presence or absence of leakage , ( 2 ) location of leakage , and ( 3 ) amount of leakage . 
the amount of leakage analyzed by conventional cystography was scored according to a previous report as follows : grade i , extraperitoneal leakage within 6cm of the vesicourethral anastomosis ( vua ) ; grade 2 , extraperitoneal leakage extending beyond 6cm from the vua ; and grade 3 , intraperitoneal leakage [ 15 ]  . 
informed consent was obtained from all subjects when they were enrolled . results the mean conventional cystography dose area product , ct cystography dose length product values , and the effective radiation dose are summarized in table2 . 
the estimated dose reduction using ultra - low - dose ct compared with the dose in conventional cystography was 60.7%. four of the 31 patients were diagnosed with urine leakage by conventional cystography . 
in all of the patients who were diagnosed with urine leakage by conventional cystography , leakage was observed at the posterior aspect of the vua ; moreover , all had grade 1 leakage ( leakage within 6cm of the vua )  . 
the amount of leakage in these patients was not large ( average , 1.31cm2 ; range , 0.581.74cm2 ) ( table3 )  . by performing ct cystography , we were able to track the precise locations and amounts of urine leakage . 
all nine patients who had urinary leakage , including the two with longer retention of the foley catheter , experienced no further complications and were discharged . discussion conventional cystography has been accepted as the standard for the assessment of bladder trauma [ 8 ]  . 
our study also showed that conventional cystography detected leakage at the posterior aspect of the vua in all patients who were diagnosed with urine leakage ; however , it is thought that the contrast collects in the dependent position by gravity . 
in particular , according to ultra - low - dose ct cystography , patient i had urine leakage at the 3 oclock position of vua , whereas 1 3 la radiologia medica ( 2019 ) 124 : 812818 fig . 
ct cystography identified the location of leakage at the 4 oclock position of vua , and the amount of leakage was estimated to be 7.08cm2 ( black arrow )  . 
c ct cystography showed patient i to have urine leakage at the 3 oclock position of the vua ( black arrow ) , but conventional cystography ( white arrow ) detected leakage at the posterior aspect of the vua according to conventional cystography , there was leakage at the posterior aspect of vua . lately , iterative reconstruction ( ir ) algorithms have received attention as good new methods for reducing radiation dose during ct examination [ 17 ]  . 
this 4th generation iterative reconstruction technique in preventing photon starvation artifacts ( streaks , bias ) prior to image creation and in maintaining image texture to overcome the artificial or plastic look of images that have been frequently reported when using previous iterative reconstruction techniques . 
evidence from rigorous clinical evaluations demonstrates the potential of idose to improve image quality and / or lower radiation dose levels beyond those previously achievable with conventional , routine - dose acquisitions , fbp reconstructions [ 12 , 13 ]  . 
for the ultra - lowdose protocols , the assumed effective dose was 0.44msv , which was very low and comparable to the dose used for conventional single plain radiography of the kidneys , ureter , and bladder [ 19 ]  . 
thus , low - dose or ultra - low - dose protocols could potentially contribute toward reducing the lifetime cumulative radiation dose as well as cancer risk [ 2 , 20 ]  . urinary leakage is a challenging , short - term complication that can occur regardless of the surgical approach used and may reduce patients quality of life [ 21 ]  . 
however , although most urine leakages are self - limited , urine leakage - induced complications include infection , metabolic abnormality as a result of intraperitoneal urine reabsorption , and urinoma formation [ 23 , 24 ]  . 
although there have been no previous reports providing definitive criteria for persistent or massive vua urine leakage , some studies have defined anastomotic urine leakage as a persistent daily amount of urine ( over 1500ml ) in the suction drain for more than 6days and for which an invasive interventional procedure had to be performed [ 27 , 28 ]  . 
our findings suggest that the use of ultra - low - dose ct may help to guide treatment and avoid unnecessary procedures in addition to reducing the risks associated with radiation exposure . our study has several limitations . 
moreover , although ultra - low - dose ct cystography was the more accurate modality for determining urine leakage compared to conventional cystography , we cannot rule out the possibility that extravasations outside the urethra or bladder lumen detected by ultra - low - dose ct cystography were not urine leakages . 
nonetheless , to our knowledge , this study is the first to evaluate the accuracy and technical characteristics of ultra - low - dose ct cystography as an optimal modality to track the precise location and amount of urine leakage and limit the radiation dose . 
 these results establish a foundation for future studies and treatments . conclusions ultra - low - dose ct cystography enables accurate evaluation of urine leakage after bladder repair despite the small radiation dose . 
prospective studies are needed to further assess its role among locoregional treatment options for liver metastases from crc . keywords liver metastases stereotactic body radiotherapy colorectal cancer oligometastases introduction colorectal cancer ( crc ) is estimated to be the second most frequently diagnosed cancer in europe , accounting for 447 , 000 new cases in 2012 , and one of the most relevant causes of cancer mortality worldwide with 694 , 000 deaths in the same year [ 1 , 2 ]  . over the last two decades , the clinical outcome of patients with metastatic crc ( mcrc ) has improved due to many factors , such as local ablative treatments ( lats ) [ 3 ]  . 
potentially , lats can have a curative intent for oligometastatic patients [ 4 ] and could play a role in the management of an oligoprogressive disease , in which only a solitary or few ( 5 ) metastatic localizations progress , while all other sites of disease are stable or responding to the current regimen [ 5 ]  . 
over the past two decades , extensive clinical experience demonstrated sbrt to be a safe and high - precision technology method to deliver ablative treatments for different metastatic sites [ 8 ] , including liver metastases [ 9 ]  . since 2012 , robotic sbrt has been offered in our institution as a possible alternative to surgery or other lats for liver oligometastases in colorectal cancer patients unsuitable for surgery . the aim of our retrospective study was to report the clinical outcome of robotic sbrt in this setting . 
during treatment planning , the following organs at risk ( oars ) were delineated : left and right lung , esophagus , heart , thoracic wall or ribs , left and right kidneys , small and large bowel , duodenum , stomach , spinal canal , whole liver , great vessels . 
for most patients , the intended prescription dose was 37.5gy in three fractions , prescribed to the 70% isodose line to cover 95% of the ptv [ 10 ]  . 
 patients were prescribed proton pump inhibitors , serotonin 5 - hydroxytryptamine antagonists , benzodiazepines and antacids as clinically indicated . followup andtoxicity evaluation after the last application , a clinical examination was performed and treatment toxicity was scored , if present , according to the common terminology criteria for adverse events ( ctc - ae ) scale , v 4.0.3. 
treatment response was 1 3 872 la radiologia medica ( 2019 ) 124 : 870876 evaluated by serial contrast - enhanced spiral ct or mri scan 2months after end of sbrt . 
complete response ( cr ) was defined as disappearance of all target lesions ; partial response ( pr ) as at least a 30% decrease in the sum of diameters of target lesions ; progression disease ( pd ) as at least a 20% increase in the sum of diameters of target lesions . 
local control ( lc ) was defined as the time of absence of progression disease at the site of sbrt from the end of the treatment . statistical analysis local control , local and distant progression - free survival ( pfs ) and overall survival ( os ) curves were evaluated by the kaplanmeier method . 
for cb , additional investigation included treatment planning related parameters such as number of fractions , physical and biological effective dose ( bed10 , considering / = 10 ) coverages . 
in order to comply with dose constraints to organs at risk , a risk - adapted approach was followed for the treatment of nine lesions , which were irradiated in five fractions instead of three . 
 then , we compared the bed10 mean dose covering the ptvs between lf and lc , and we found that its median value was smaller in the lf group ( 89.26gy ) than in lc fig . 
actuarial 1 3 874 la radiologia medica ( 2019 ) 124 : 870876 although surgical resection is presently accepted as the first choice among strategies for ablation , for many reasons only a small percentage of patients qualify for surgical procedures [ 14 ]  . up to now , ct - guided percutaneous radiofrequency ablation ( rfa ) is the most common local treatment option to be offered to such patients [ 15 ]  . 
in recent years , sbrt has become the current standard in medically inoperable early lung cancer patient [ 16 ] and , potentially , it could be the same for unresectable liver metastases treatment [ 17 ]  . our analysis counted one of the most numerous series addressing the use of high doses of radiation by means of robotic sbrt in the treatment of liver metastases exclusively from crc . 
moreover , our study has other limitations : its retrospective nature , the heterogeneity of the prescription doses , the differences in the timing of sbrt with respect to other treatments . our results demonstrated that it is possible to have good outcomes on response rate and survival analysis , keeping an excellent safety profile . 
 [ 18 ] in their subgroup analysis on liver metastasis from adenocarcinoma , confirming that colorectal adenocarcinoma has a statistically significant worst lc than other histologies [ 19 , 20 ] , which is perhaps related to the fact that these patients are generally heavily pretreated and surgically unresectable [ 21 ]  . moreover , as chang etal . 
 [ 22 ] had already concluded in their meta - analysis , a dose of 4652gy in three fractions or higher is required to achieve 90% lc at 1year for the treatment of hepatic cr metastases . although a good performance in terms of lc , in our analysis , pfs ( both hepatic and distant ) was poor , if compared with the results obtained by berkovic etal . 
swaminath and dawson [ 23 ] had already noticed in their analysis that , although excellent local control rates were achieved , many patients developed out - of - field progression probably because of the relatively high number of patients with extrahepatic disease and / or more than three metastatic lesions , suggesting that a closer attention should be reserved to patients who really belong to a relatively good prognostic group with longer survival expectancy and offering a strong rationale for combining sbrt with systemic treatments , as hypothesized by scorsetti etal . 
in fact , comparing survival curves of patients with or without extrahepatic disease before sbrt , there is a clear advantage for the second ones , both in os and in pfs ( supplementary materials , figures1 and 2 )  . 
previous extrahepatic disease and number of metastatic lesions > 3 showed a statistically significant correlation at univariate analysis ; this result was confirmed at multivariate analysis only for the presence of previous extrahepatic disease , as in the pfs analysis . toxicity no complications were observed during or after fiducials placement . 
as referred by hellman and weichselbaum , the theory of oligometastases considers that there could be a subgroup of patients with metastatic disease that is intermediate between completely absent and widely metastatic [ 12 ]  . 
on the other hand , their cohort was less homogeneous than ours , since also patients treated for extrahepatic localizations ( lung , lymph nodes , suprarenal gland ) were included in the analysis . 
 [ 29 ] performed a phase 1 / 2 study enrolling about 70% of patients with liver metastases from non - colorectal origin ( lung , breast , ovary , esophagus and others )  . 
likewise , in scorsettis study [ 9 ] , more than 50% of patients had metastases from non - colorectal primary tumor , and more than 80% of patients received a prescription dose of 75gy in three fractions ( mean dose to ptv )  . 
as expected , very limited treatment - related toxicity was observed in our cohort ; however , it has to be acknowledged that our local control rate is at the lower range of published data . in particular , the rate of actuarial lc at 2years in these experiences ranges between 64 and 92% ( supplementary table2 )  . 
as a matter of fact , the net effect of sbrt on the irradiated lesion is critically dependent on the delivered physical total dose and fractionation , the applied bed , the size of the gtv , the prescription modality and the intrinsic biological radiosensitivity . 
overall , patients selection refinement and prospective trials based on strict inclusion criteria in the setting of oligometastatic crc should be warranted . conclusions survival and toxicity results of our retrospective analysis support the hypothesis that sbrt for liver metastases from crc is a feasible treatment , combining an excellent safety profile with acceptable efficacy results . 
in addition , only controlled studies could allow us to define how to best select oligometastatic patients potentially profiting from a locoregional treatment with the aim to defer further systemic therapies . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards informed consent was obtained from all individual participants included in the study . 
the survey consisted of 11 multiple - choice questions about participants demographics , current local modalities of pic acquisition and storage , perceived advantages and disadvantages of pic dematerialisation over conventional paper - based pic , and overall opinion about pic dematerialisation . results a total of 1791 radiologists ( amounting to 17.4% of active sirm members for the year 2016 ) joined the survey . 
conversely , the need to create dedicated areas for pic acquisition inside each radiological unit ( 64.0% ) and to gain preliminary approval for the use of advanced digital signature tools from patients ( 51.8% ) were seen as potential disadvantages . 
however , concerns were raised that its practical implementation might face hurdles due to its complexity in current real life working conditions . keywords informed consent dematerialisation online survey paperless * lorenzo faggioni lfaggioni@sirm.org 1 department ofexperimental , diagnostic andspecialty medicine , s . 
orsola malpighi university hospital , bologna , italy 2 diagnostic andinterventional radiology , university hospital ofpisa , via paradisa 2 , 56100pisa , italy 3 department ofradiology , university ofcampania l . 
vanvitelli , naples , italy 4 snr foundation , rome , italy 5 uoc radiodiagnostica , aou policlinico vittorio emanuele , catania , italy 6 department ofimaging , asl 3 genovese villa scassi hospital , genoa , italy 7 department ofradiology , usl n . 
bosco hospital , turin , italy 9 department ofinterventional anddiagnostic radiology , arcispedale santanna , ferrara , italy 10 radiology department , universit politecnica delle marche , ancona , italy 11 department ofradiology , candiolo cancer institute , fpo - irccs , candiolo , turin , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 846853 introduction dematerialisation is a complex process involving the development of a digital document flow with full legal value aimed to support and , in perspective , replace conventional document production and archiving for public or private activities [ 112 ]  . 
the advantages of digitisation over paperand film - based workflow in radiology have been widely demonstrated [ 1317 ] , and attempts have since been made to extend the process to administrative key areas of healthcare data management , including , on a national level , the introduction of the digital medical recipe in most italian regions [ 312 ]  . 
however , to our knowledge , no systematic initiatives have been taken so far towards dematerialisation of patients informed consent ( pic ) for diagnostic and interventional radiology procedures , despite incentives from international [ 1 , 2 ] and national government agencies and healthcare institutions to promote digitisation in the public administration as well as in the healthcare system [ 312 ]  . 
such delay is due to the need for dematerialised pic to be formally equivalent to its conventional , paper - based version , implying for it to fully conform to current laws and privacy regulations , ensure proper patients understanding of medical procedures for which written informed consent is required , and provide seamless integration with existing ris / pacs infrastructure at radiological centres [ 18 , 19 ]  . 
while the development of a fully functional programme for pic dematerialisation may pose significant legal and technical challenges , evidence exists in the literature that pic dematerialisation with the aid of portable devices is feasible and as effective or superior to conventional methods in several aspects [ 2024 ]  . the italian society of medical radiology ( sirm ) has promoted the development of guidelines for pic dematerialisation and has put the imaging informatics chapter and informed consent commission of sirm in charge for its implementation . 
in this context , we sought to gain insight about the current modalities of pic acquisition for radiological procedures in italy and the opinion of italian radiologists about pic dematerialisation via an online survey . materials andmethods the online survey was launched as part of an initiative by the imaging informatics chapter of sirm aimed to promote dematerialisation of pic for radiological procedures ( both diagnostic and interventional ) , in cooperation with a number of it firms . 
the survey was devised following suggestions from a multidisciplinary expert panel of sirm and consisted of 11 questions , of which 9 were single choice and 2 multiple choice ( appendix )  . 
a free text field was left at the bottom of each question for additional comments . based upon a similar approach to two previous sirm surveys on teleradiology and radiological structured reporting [ 25 , 26 ] , every single sirm member received a personal email invitation to join the survey via a direct web link from the president of the sirm imaging informatics working group . 
b multiple answers allowed medical directors [ 23.7% ( 423 / 1780 ) ] or consultants [ 16.9% ( 301 / 1780 ) ] , respectively ( question #4 )  . the majority of responders deemed their it skills good [ 67.9% ( 1207 / 1778 ) ] or excellent [ 12.6% ( 224 / 1778 ) ] , whereas a minority declared to have barely sufficient [ 18.7% ( 332 / 1778 ) ] or poor [ 0.8% ( 15 / 1778 ) ] it skills , respectively ( question #5 )  . pic forms were mostly developed locally at each survey participants institution [ 77.0% ( 1311 / 1702 ) ] or , less frequently , by sirm [ 38.5% ( 655 / 1702 ) ] or the health department of each region [ 10.5% ( 180 / 1702 ) ] ( question #6 )  . pic could be revoked by the patient anytime before the examination according to 62.4% ( 1105 / 1772 ) of survey respondents ( question #7 ) , and pic forms were mainly stored in the hospital archive [ 82.7% ( 1428 / 1726 ) ] or , much less frequently , outside of the hospital [ 6.9% ( 119 / 1726 ) ] or were digitally archived into the ris [ 6.8% ( 117 / 1726 ) ] ( question #8 )  . the main advantages of dematerialised pic over conventional , paper - based pic as perceived by the survey respondents ( question #9 ) were its easier and faster recovery [ 96.5% ( 1669 / 1729 ) ] , safer storage and conservation [ 94.5% ( 1643 / 1738 ) ] , reduced cost due to the workflow going paperless [ 90.7% ( 1573 / 1735 ) ] , higher degree of protection in case of medico - legal litigation [ 83.8% ( 1439 / 1717 ) ] , and simplified patient identification and registration [ 74.3% 1 3 la radiologia medica ( 2019 ) 124 : 846853 ( 1274 / 1714 ) ] ( table2 )  . 
this latter circumstance may be due to different factors , including the current lack or inadequacy of technical infrastructures for digital pic collection ( including tablet devices running ad hoc software and connected to dedicated hospital wireless networks ) and / or of integration with existing ris / pacs environments , in spite of substantial investments into dematerialisation by government agencies . 
besides , some features of conventional , paper - based pic acquisition have emerged from the survey that should be incorporated in a dematerialised , digital pic version , including the possibility for patients to revoke their consent anytime before radiological procedures ( question #7 )  . 
in other terms , such basic aspects of conventional pic should be taken into account and preserved in the design and practical implementation of dematerialised pic solutions in order to maintain their legal validity , so that the transition from conventional to dematerialised pic should not substantially alter workflow . 
 furthermore , the current , more frequent usage of pic forms developed locally ( 77.0% of respondents to question #6 ) rather than by regional health departments ( 10.5% ) or , better , national scientific societies such as sirm ( 38.5% ) could be 1 3 la radiologia medica ( 2019 ) 124 : 846853 a potential , yet surmountable hurdle to standardisation and large - scale setup of dematerialised pic tools . 
these latter would actually benefit from the adoption of a single , predefined validated pic model for each radiological procedure , which could also be advantageous for data mining purposes and eventually in case of medico - legal issues [ 2731 ]  . overall , the majority of survey respondents were favourable to pic dematerialisation and acknowledged several advantages of digital over conventional pic , the main ones being easier and faster data retrieval , safer data storage , and reduced running costs . 
in this perspective , tablet - based methods for pic collection have shown to be preferred over conventional pic by both patients and medical staff and has proven more effective at ensuring adequate patients understanding of medical procedures and research trials [ 2024 , 32 , 33 ]  . 
interestingly , our finding of a rate of pic dematerialisation supporters consistently higher than 90% across all age classes of survey participants ( independent of and greater than their self - assessed it skills ) may suggest that radiologists are confident about the usability of digital pic and / or believe that its advantages would outweigh any potential difficulties related to its use as a routine working tool . on the other hand , the main potential drawbacks of pic dematerialisation as pointed out in the survey were related to technical difficulties in carrying out the process in real working environments . 
actually , tablet - based pic acquisition resulted to be more time consuming than paper - based pic collection [ 21 , 24 ] , and earlier work by haller etal . 
 [ 34 ] cautioned against the use of palmtops for electronic data collection in clinical research due to a significant increase in data entry time and risk of typing errors and missing data in comparison with paper - based questionnaires . 
 [ 21 ] found a positive correlation between the duration ofelectronic ipad - based briefings and patient age , paralleled by a negative correlation between patient age and computer skills , but nonetheless the majority of patients would prefer ipad briefings to conventional written informed consent forms in the future . 
even more specifically , it has been suggested that the higher degree of understanding and overall satisfaction provided by tabletbased pic may improve adhesion to clinical trials [ 23 ]  . a limitation of our study is the relatively small number of sirm members joining the survey ( 1791 / 10304 , corresponding to 17.4% of all active sirm members in full standing for the year 2016 ) , which could restrict the validity of our findings to a minority of all members . 
however , the participation rate to our survey was slightly higher than two recent online surveys involving sirm members on teleradiology [ 16.5% ( 1599 / 9662 ) ] [ 25 ] and radiological structured reporting [ 12.1% ( 1159 / 9560 ) ] [ 26 ] , and much higher than a similar european online survey on teleradiology ( 368 radiology professionals from 35 european countries ) [ 35 ] , confirming that pic dematerialisation has gained significant interest within the radiological community . conclusions our findings show that the majority of radiologist members of sirm involved in the survey were favourable to pic dematerialisation . 
though most of them were aware of the potential long - term advantages of pic dematerialisation over conventional , paper - based pic ( mainly related to greater ease , speed , and safety of data collection , storage and retrieval ) , concerns emerged about potential technical and organisational hurdles that its practical implementation may pose , including the need for extra space and time for digital pic collection ( which would add to regular radiologists workload ) , authorisation to use patients advanced digital signature , and to cater for patients who wish to remain anonymous . 
considering the overall issues involving your professional activity , do you believe this process would be needed ? la radiologia medica ( 2019 ) 124 : 854859 radiotherapy extrapleural pneumonectomy intheera ofimageguided intensitymodulated radiotherapy marcotrovo1 davidefranceschini2 carlofurlan3 francescapietrobon3 stefanovagge4 eleonorafarina5 albertorevelant5 lucavisani6 virginiamaragna6 giuseppeparisi1 vieriscotti6 received : 18 july 2018 / accepted : 14 march 2019 / published online : 8 april 2019 italian society of medical radiology 2019 abstract purpose to assess the outcome of malignant pleural mesothelioma patients treated with extra - pleural pneumonectomy ( epp ) and adjuvant radiotherapy ( rt ) , using the most advanced radiotherapeutic techniques , namely image - guided intensitymodulated rt ( ig - imrt )  . methods and materials fifty - four patients were analyzed . 
the study endpoints included loco - regional control ( lrc ) , distant metastases free survival ( dmfs ) , and overall survival ( os ) , as well as radiation - related toxicity . results major patients and treatment characteristics were the following : median age 62years , epithelioid histology in 51 ( 94% ) cases , locally advanced disease in 41 ( 90% ) cases , and metastatic mediastinal lymph nodes in 27 patients ( 50% )  . 
the predominant pattern of failure was distant : 34 patients ( 62.9% ) developed some component of distant failure , and only 5 patients ( 9.2% ) developed an isolated loco - regional recurrence . 
other major toxicities included : grade 2 and 3 pneumonitis in 1 and 2 cases , respectively , 1 case of bronchial fistula , pleural empyema , and grade 3 esophagitis , respectively . conclusions although executed in the era of high - technology radiotherapy ( ig - imrt ) , epp should not be routinely performed . keywords malignant pleural mesothelioma image - guided imrt extra - pleural pneumonectomy introduction malignant pleural mesothelioma ( mpm ) is a rare cancer , strictly correlated with asbestos exposure . 
its prognosis is usually poor , with a median survival of 68months in untreated patients [ 1 ]  . extra - pleural pneumonectomy ( epp ) represents an aggressive surgical approach that has been shown to increase survival as part of a trimodal therapeutic strategy including * giuseppe parisi giuseppe.parisi@asuiud.sanita.fvg.it extended author information available on the last page of the article adjuvant chemotherapy and radiotherapy . 
 reported a 5 - year survival of 46% in selected patients , including who had an epithelial histology , with negative resection margins and without metastatic extra - pleural nodes [ 2 ]  . 
due to these results , in recent years such surgical approach fell out of favor among the scientific community , mainly due to the severe perioperative stress , the noticeable complication rate , and the long - term detrimental anatomical and functional effects [ 3 ]  . 
a less invasive approach , as lungsparing surgery , found place particularly after the publication of the mars trial , a feasibility study in which patients were randomized to receive epp or not [ 4 ]  . 
in a meta - analysis comparing epp with lung - sparing surgery , it was documented that pleurectomy / decortication might be performed vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 854859 with lower morbidity and mortality than epp while resulting in comparable long - term survival [ 5 ]  . 
however , the comparison of both procedures has several limitations and the choice for a specific therapy is still highly individual based on the extension of the disease , the patient comorbidities , and the center experience . also , the role of adjuvant radiotherapy ( rt ) was questioned after the recent publication of the sakk trial , a randomized trial that failed to show a clinical advantage of adjuvant rt following epp [ 6 ]  . 
it must be underlined that in this study different fractionation schemes and rt techniques , including 3d conformal rt , were adopted . considering the uncertainties of the published literature , we conducted the present study to assess the outcome of mpm patients treated with epp and adjuvant rt , using the most advanced radiotherapeutic techniques , namely imageguided intensity - modulated radiation therapy ( ig - imrt ) , in major academic centers in our country . loco - regional ( lrr ) and distant relapses were assessed using chestabdomen ct , which was performed every 46months ; fdg - pet / ct was added at the workflow in case of concerns of disease progression . 
lrr was defined as any clinical or radiographic recurrence in the chest wall ( local ) or in the regional lymph nodes ( hilar , mediastinal , or internal mammary lymph nodes )  . the study endpoints , including loco - regional control ( lrc ) , distant metastases free survival ( dmfs ) , and overall survival ( os ) , were estimated using the kaplanmeier method , starting from the date of completion of rt until death or the last available follow . 
the hazard ratios for potential risk factors included age , sex , performance materials andmethods table 1 patient , tumor , and treatment characteristics this is a retrospective studies including patients data collected in prospective databases in four academic centers in italy . 
each patient signed an informed consent form that was approved by each institutional review board before entry into the registry . in the study period , 66 patients were treated with epp and adjuvant ig - imrt for mpm . 
ten patients were excluded from the study : 7 were lost at follow - up immediately after the completion of rt ( were followed in other facilities ) , and 5 were treated with palliative radiation doses . 
planning target volume ( ptv ) was generated adding an isotropic margin of 0.5cm to the clinical target volume ( ctv ) , which encompassed the entire hemithorax , including the ipsilateral mediastinum if interested by disease , the pericardium and diaphragm , as well as the thoracotomy scars and any drain sites , according to the technique proposed by the researchers from the md anderson cancer center [ 7 ]  . 
imrt was delivered with tomotherapy in 17 patients [ 8 ] , using a volumetric imrt technique in 27 patients [ 9 ] , and static 7 - field sliding window imrt in 10 patients [ 10 ]  . 
cone beam ct or megavoltage ct scans were performed daily for each patient , in order to properly guide the radiation treatment . patients were followed at regular intervals to determine tumor status and presence of symptoms . 
1 kaplan - mayer estimates of overall survival of patients treated with extrapleural pneumonectomy and imageguided intensity modulated radiation therapy table 2 pattern of failure failure pattern local local only local and nodal local and distant local , nodal , and distant nodal nodal only nodal and distant distant distant only month n ( % ) 13 ( 24.0% ) 4 ( 7.4% ) 1 ( 1.8% ) 5 ( 9.2% ) 3 ( 5.5% ) 9 ( 16.6% ) 5 ( 9.2% ) 34 ( 62.9% ) 21 ( 38.8% ) chemotherapy , 4 patients ( 7% ) received adjuvant chemotherapy , and 3 patients ( 5% ) received both neoadjuvant and adjuvant chemotherapy . 
the median number of chemotherapy cycles , consisting of cisplatin / carboplatin and pemetrexed , was 4 ( range 37 cycles )  . all patients underwent postoperative imrt , with a total radiation dose ranging between 50 and 60gy in 2530 fractions . 
the predominant pattern of failure was distant : 34 patients ( 62.9% ) developed some component of distant failure , and only 5 patients ( 9.2% ) developed an isolated loco - regional recurrence . 
we did not find any risk factor correlating with overall survival at the univariate analysis . three fatal ( grade 5 ) pneumonitis were documented within 6months from the completion of radiotherapy . 
other major status , histologic subtype , stage of disease , gross residual disease after surgery , and chemotherapy administration . results patients , tumor , and treatment characteristics are shown in table1 . 
2 kaplan - mayer estimates of loco - regional control ( a ) and distant metastasis - free survival ( b ) of patients treated with extrapleural pneumonectomy and imageguided intensity modulated radiation therapy months months toxicities included : grade 2 and 3 pneumonitis in 1 and 2 cases , respectively , 1 case of bronchial fistula , pleural empyema , and grade 3 esophagitis , respectively . 
nine patients reported severe fatigue . discussion in the present paper , we wished to report the clinical outcome of mpm patients treated with epp , followed by the 1 3 858 la radiologia medica ( 2019 ) 124 : 854859 table 3 trimodality with extra - pleural pneumonectomy and intensity - modulated radiation therapy for malignant pleural mesothelioma author year no . 
of patients who completed trimodality therapy key results : median overall survival ( months ) key results : 2 - year overall survival ( % ) krug [ 13 ] patel [ 14 ] gomez [ 15 ] thieke [ 16 ] present study 2009 2011 2013 2015 2018 predominant pattern of failure distant ( 65% ) distant ( 60% ) distant ( 75% ) not reported distant ( 63% ) most advanced radiotherapeutic treatment , namely imageguided imrt , with the hypothesis that the adoption of such technology could lead to better clinical results . 
these results are particularly unsatisfying if considering that the patient population was selected positively : only patients that successfully underwent epp were included in the analysis . it has been reported that almost 50% of patients who are suitable candidates for trimodality therapy actually complete the proposed treatment . 
authors from the european institute of oncology reported that of the 83 patients candidate to chemotherapy , epp , and rt , only 37 ( 45% ) completed the planned trimodality treatment [ 11 ]  . 
reported that only 30 out of 60 patients completed high - dose hemithoracic rt after epp ; the median os for all patients intended to undergo trimodality therapy was 14months [ 12 ]  . 
similarly , a multicentric study conducted in usa on neoadjuvant chemotherapy followed by epp and radiation reported that only 57% of the enrolled patients started radiation therapy [ 13 ]  . 
the author documented a median os of 17months and 29months in the intention to treat population and in the population that completed hemithoracic radiotherapy , respectively . our results are comparable with those published in the literature by the researchers from major academic centers in north america . 
the principal findings of these studies are summarized in table3 . in our study , only 5 ( 9.2% ) patients experienced an isolated loco - regional failure , and predominant pattern of failure was distant : 62.9% of patients failed distantly . 
 these data suggest that the high control rate obtained with extensive surgery and high - dose ig - imrt did not translate into a survival advantage . according to this , it has been showed that less aggressive therapeutic approaches , such as lung - sparing surgery followed by hemithoracic rt , might be suitable to manage a systemic disease such as mpm while guaranteeing an adequate rate of loco - regional control [ 17 , 18 ]  . the main limit of our study is a possible patient selection bias , as previously discussed . 
it is implicit that surgery - related toxicities and deaths were not considered in the present analysis , and patients who progressed immediately after surgery or chemotherapy were not enrolled in the study . 
on the other hand , these features highlight the poor results obtained in our study . taken together , our findings , including survival and pattern of failure , imply that epp , although executed in the era of high - technology radiotherapy ( ig - imrt ) , should not be routinely performed . 
probably , lung - sparing surgery represents a valid therapeutic option for mpm patients . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
 intravascular attenuation ( iva ) , signal - to - noise ratio ( snr ) , contrast - to - noise ratio ( cnr ) and image noise were compared . 
computed tomography angiography ( cta ) is less invasive , safe and with diagnostic performance comparable to dsa and is often used as * marco fogante marco.fogante89@gmail.com 1 department ofradiology , azienda ospedalierouniversitaria , ospedali riuniti di ancona , via conca 71 , 60126torrette , ancona , italy 2 department ofradiology - school ofradiology , universit politecnica delle marche , ancona , italy preoperative examination in pad [ 7 , 8 ]  . 
but , with this technique there is the risk to overrun contrast bolus , especially with vascular pathologies , such as stenosis and aneurysmal dilatations , which delay the arrival of contrast vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 184190 medium at the peripheral arteries with inadequate filling of small distal arteries at acquisition time [ 1518 ]  . modulation , care dose 4d ( siemens , medical solution ) ; and matrix , 350 350mm . dual - source ct ( dsct ) , with two x - ray tubes placed at 95 to each other , has allowed , compared to single - source ct ( ssct ) , greater spatial and temporal resolution , by the use of flash imaging characterized by high pitch and halving rotation time [ 1921 ]  . our hypothesis is to experiment a new protocol , with dsct flash caudo - cranial acquisition , rather than craniocaudal , to reduce radiation dose and obtain a better contrastographic peripheral arteries attenuation . 
the aim of this study is to compare radiation dose and image quality of lower extremity cta between ssct cranio - caudal acquisition and dsct flash caudo - cranial acquisition . materials andmethods patients selection this prospective study received institutional review board approval . 
exclusion criteria were : allergy to iodinated contrast medium , renal insufficiency ( estimated glomerular filtration rate < 60ml / min / 1.73m2 , according to european society of urogenital radiology ) and history of stents or bypass in lower limbs arteries . 
based on a random - number table , all patients were assigned into a control group , group a ( n = 30 ) , submitted to protocol 1 ( p1 ) , with ssct cranio - caudal acquisition and an experimental group , group b ( n = 30 ) , subjected to protocol ( p2 ) , with dsct flash caudo - cranial acquisition . ct scan protocol all cta examinations were performed using 192 2 - sections dsct scanner ( somatom force , siemens medical solutions , forchheim , germany ) with patients in supine position and feet toward the gantry . 
a 20 - gauge cannula was inserted into superficial vein of the right antecubital fossa connected to a two - way injector with 1.0ml / kg infusion of contrast medium ( iopamidol , 370mgi / ml ) at flow rate of 4.0ml / s , followed by 60ml of saline at the same flow rate . in both protocols , was obtained anteriorposterior scout from the xyphoid process to the feet . 
the acquisition parameters were : tube voltage , 80kvp ; automatic tube current control group a underwent p1 with ssct cranio - caudal acquisition , bolus tracking technique and monitoring region positioned at the abdominal aorta bifurcation level . 
the different acquisition parameters used in two protocols are summarized in table1 . image analysis the ct images were reconstructed with slice thickness of 1mm and interval thickness of 0.7mm with advanced modeled iterative reconstruction ( admire , siemens healthcare ) , strength 3 and body vascular 36 ( bv36 ) algorith all datasets were transferred to a dedicated workstation ( syngo.via , siemens medical solution , forchheim , germany )  . 
maximum intensity projection ( mip ) , curved planar reformation ( cpr ) and volume rendering ( vr ) images were obtained for each patient . images quality evaluation to evaluate objective image quality , all measurements were taken by a radiologist with 10years of cta experience . 
 intravascular attenuation ( iva ) was measured , by positioning a region of interest ( roi ) in axial images in five locations : aortic artery bifurcation , common iliac arteries , common femoral arteries , middle third of superficial femoral artery and middle third of popliteal artery . 
before image evaluation , the observers were instructed to divide the vascular structures into three segments ( aortoiliac , femoropopliteal and the below the knee ) and then score the image quality in these segments using a 4 - point scale according to the degree of noise artefacts , the presence of streak artefacts and graininess of the images . 
 the scoring criteria were as follows [ 22 ] : poor ( grade 1 ) , graininess or streak artefacts were significant and did not provide sufficient information for the diagnosis ; adequate ( grade 2 ) , the examination provided acceptable information but unsatisfactory image quality ; good ( grade 3 ) , image quality was satisfactory enough to provide the information necessary to make an adequate radiological diagnosis ; excellent ( grade 4 ) , image quality provided optimal information for a radiological diagnosis . 
in the event of observer disagreement , another reading session was convoked to reach an agreement . radiation dose estimation ctdivol and dlp were used to estimate radiation dose of each patient and were recorded in the dose report . statistical analysis statistical analysis was performed using version 19 of the spss software . 
 the analysis of variance was used to compare mean value of iva , snr , cnr and in . kappa analysis was used to assess the inter - observer agreement of the subjective image quality rating . 
a k value less than 0.20 indicates poor agreement ; 0.210.40 , fair agreement ; 0.410.60 , moderate agreement ; 0.610.80 , good agreement ; and 0.811.00 , very good agreement . 
there were no statistically significant differences in age , gender , weight and height between the two groups ( table2 )  . image quality table3 summarizes mean values of iva , snr , cnr and in of two protocols . 
the use of low - voltage , automated modulation systems of mas and iterative reconstruction techniques achieves , with the same radiation dose , better iva , snr and cnr [ 1114 ]  . 
 to obtain an appropriate acquisition time of angiographic phase , bolus tracking is the technique that guarantees , in most cases , better results [ 1518 , 28 , 29 ]  . 
dsct with flash protocol has allowed to improve spatial and temporal resolution , compared to ssct , using high pitch and half rotation time [ 19 , 20 ]  . 
our hypothesis is to experiment , with dsct a flash caudo - cranial acquisition , rather than craniocaudal , to reduce radiation dose and obtain a better contrastographic peripheral arteries attenuation . 
possible explanation is that the use of high pitch and high rapid scan provides less radiant exposure . mean values of iva , snr and cnr were higher in p2 than in p1 with better image quality for small arteries below the knee . 
possible explanation of these results is that the caudo - cranial acquisitions were started when the radiologist saw contrast medium in the popliteal fossa , avoiding the risk of overrunning contrast bolus , especially with vascular pathologies , such as stenosis and aneurysmal dilatations , which delay the arrival of contrast medium with little filling of the small distal arteries at the time of scanning . 
moreover , the rapid acquisition with high pitch assured , even if starting from the ankles , an excellent opacification up to cranial portions of the abdominal aorta . to date , this is the first study in scientific literature to experiment a flash acquisition protocol with caudocranial scan . 
in this work , group a was submitted to p1 with 70kvp , cranio - caudal acquisition in ssct and were obtained mean iva , snr , cnr and in values comparable to those of qi etal . 
for an accurate evaluation of the effective radiation dose , direct organ measurements should be taken . in conclusion , with dsct and flash caudo - cranial acquisition we obtained a dose reduction administered to the 1 3 la radiologia medica ( 2019 ) 124 : 184190 patient of 40.9% in ctdivol and of 42.8% in dlp with better mean values of iva , snr and cnr compared to a ssct with 70 kvp and cranio - caudal acquisition protocol . 
this new protocol may contribute to reduce radiation dose and to obtain better image quality with correct acquisition time of angiographic phase in the lower extremity cta examination . compliance with ethical standards conflict of interest the authors declared no potential conflicts of interests associated with this study . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
ceus might be used instead of contrast - enhanced computed tomography ( cect ) during spleen injury follow - up in order to reduce radiation exposure . objective assess diagnostic comparability between ceus and cect in the evaluation of dsvi and dae during spleen injury follow - up . subjects and methods a total of 139 trauma patients ( 101 males , 38 females ; mean age 48.6years ) with cect diagnosed spleen injury were prospectively evaluated . 
twelve patients performed digital subtraction angiography ( dsa ) during follow - up , and the diagnostic performance comparability between ceus and dsa was evaluated . results ceus showed 17 delayed spleen injury complications , and in 122 patients no complication was suspected . 
compared to dsa , ceus showed a sensitivity of 100% and a positive predictive value of 91.7%. conclusions ceus can be used during spleen injury follow - up instead of cect . 
positive ceus examinations could perform cect and , when necessary , dsa in order to confirm and treat spleen injury complications . keywords contrast - enhanced ultrasound ( ceus ) delayed splenic vascular injury delayed active extravasation blunt splenic trauma non - operative management introduction the spleen is the second most frequent organ involved in blunt abdominal trauma ( 13% ) after the liver ( 16% ) [ 1 ]  . 
 delayed splenic vascular injury ( dsvi ) and delayed active extravasation ( dae ) are reported to occur , respectively , in * corrado tagliati corrado.tagliati@gmail.com 1 school ofradiology , universit politecnica delle marche , ancona , italy 2 sod clinica di radiologia , durgenza e dellarea oncologica , azienda ospedaliero universitaria ospedali riuniti , ancona , italy 3 department ofradiological sciences , azienda ospedaliero universitaria ospedali riuniti , universit politecnica delle marche , ancona , italy 323% and 1.5% of blunt splenic injuries ( bsi ) [ 25 ]  . 
nonoperative management ( nom ) of blunt splenic trauma is the treatment of choice for hemodynamically stable patients in an optimal setting in which monitoring and frequent clinical evaluations are possible , and an operating room is available for urgent laparotomy . 
nom allows the preservation of spleen role in immune system , reducing the risk of future infections , the most serious of which are part of the overwhelming post - splenectomy infection ( opsi ) syndrome . 
 delayed splenic rupture is a life - threatening injury complication , and it is thought that it could be related to the rupture of a pseudoaneurysm ( psa ) , clot disruption or expansion of vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 170175 a subcapsular hematoma [ 4 , 8 , 9 ]  . 
there are different classifications of spleen trauma injury grade ; the american association for the surgery of trauma ( aast ) spleen injury scale ( sis ) is the most used [ 10 ] ( table1 )  . 
according to the western trauma association ( wta ) algorithm , in all patients with aast - sis grade ii or higher - grade injuries a repeat imaging may be considered before hospital discharge to rule out psa formation [ 11 ]  . conventional ultrasound ( us ) , contrast - enhanced ultrasound ( ceus ) and ct are used to assess patients with blunt abdominal trauma . 
conventional us is generally used in the early assessment of polytrauma patients in order to assess intra - abdominal free fluid , a technique known as focused assessment with sonography for trauma ( fast )  . 
in adult patients , ct is the most used imaging modality in spleen injury follow - up , but ceus is a promising alternative imaging modality in this field [ 13 ]  . 
according to efsumb guidelines , ceus can be used in the follow - up of conservatively managed abdominal trauma to reduce the number of ct examinations , particularly in children [ 14 ]  . 
according to the world society of emergency surgery ( wses ) guidelines , ct scan repetition during the admission should be considered in adult patients with an initial diagnosis of moderate lesions ( hemodynamically stable aast - sis grade iii - v lesions ) as well as when there is lowering hematocrit levels , vascular anomalies , underlying splenic pathology or coagulopathy , and in neurologically impaired patients . 
according to the same guidelines , ceus follow - up seems reasonable to minimize the risk of life - threatening hemorrhage and associated complications in children [ 15 ]  . 
dsvi are splenic - contained table 1 aast spleen injury scale ( 1994 revision ) [ 10 ] grade injury type description of injury vascular injuries , and consist of pseudoaneurysm ( psa ) and post - traumatic arteriovenous fistula ( avf ) : these two entities are usually indistinguishable by means of ceus or ct [ 1921 ]  . 
another study demonstrated a high sensitivity ( 83% ) and specificity ( 92% ) of ceus at detection of post - traumatic liver and splenic psa in the pediatric population [ 23 ]  . to our knowledge , no previous study evaluated ceus diagnostic performance in diagnosing dsvi and dae in adult patients with serial ceus examinations during follow - up . the study aim was to assess diagnostic comparability between ceus and cect in the evaluation of dsvi and dae during spleen injury follow - up . subjects andmethods patient population during the 2years period 20162017 , 824 hemodynamically stable trauma patients without diffuse peritonitis underwent contrast - enhanced ct ( cect ) in our emergency department . 
the study population consisted , therefore , of 139 adult patients ( 101 males ; 38 females ; m : f 2.7 : 1 ; mean age 48.6years , range 1886 ) who underwent ceus and cect follow - up between january 2016 and december 2017 . hematoma laceration hematoma laceration hematoma laceration laceration laceration vascular subcapsular , < 10% surface area capsular tear , < 1cm parenchymal depth subcapsular , 1050% surface area intraparenchymal , < 5cm in diameter capsular tear , 13cm parenchymal depth that does not involve a trabecular vessel subcapsular , > 50% surface area or expanding ; ruptured subcapsular or parenchymal hematoma ; intraparenchymal hematoma > 5cm or expanding > 3cm parenchymal depth involving trabecular vessels laceration involving segmental or hilar vessels producing major devascularization ( > 25% of spleen ) completely shattered spleen hilar vascular injury with devascularized spleen 1 3 172 la radiologia medica ( 2019 ) 124 : 170175 the study was approved by the institutional review board and ethics committee of our institution . 
informed consent was obtained from all individual participants included in the study . statistical analysis ceus technique ceus follow - up consisted of one - to - eight ( mean 4.7 ) serial examinations at 13715306090180days ( 1day ) after trauma until spleen injury became no more visible . 
ceus were performed with continuous image acquisition , starting immediately after contrast injection and lasting 5min . ct technique all the 139 patients underwent a cect examination between 3 and 7days after trauma . 
cect examination was performed using a 16 - slice ct ( philips brilliance ) , with arterious , venous and delayed post - contrast images after intravenous injection of 90120ml iopamidol 370mg i / ml ( iopamiro 370 , bracco , milan , italy ) with an electronic power injector ( stellant ; medrad ) at a flow rate of 3ml / s . image assessment two radiologists , with more than 10years experience in ceus and cect abdominal imaging , evaluated in consensus ceus and cect images in order to detect a dsvi or a dae . 
 dsvi was diagnosed by ct when a hyperdense round or oval area of contrast enhancement with distinct margins in arterial phase did not increase in size in portal venous phase . 
 in the thirteen patients eligible for interventional procedures , dsa images , considered as the standard of reference , were reviewed by an experienced interventional radiologist ( with 10years of experience in interventional radiology ) , who was unaware of the ceus and cect findings . 
dsa diagnosis was compared with that made using ceus to assess the two modalities comparability . in the 139 patients included in the study , ceus diagnosis was compared with cect one , and diagnostic performance comparability was assessed . 
cect diagnosed 16 delayed spleen injury complications in these 17 patients ( 12 dsvi and 4 dae ) ; cect diagnosed a small dsvi ( 2mm of maximum diameter ) in another patient . 
previous studies showed that ceus can detect active bleeding [ 16 , 22 ] or demonstrated the usefulness of performing one or two ceus during follow - up [ 24 , 25 ]  . 
some other studies reported the usefulness of performing a follow - up ct scan 48 or 72h after admission in patients with grade ii in order to diagnose a possible psa development [ 4 , 25 , 26 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 170175 fig . 
3 63 - year - old man with active bleeding diagnosed by ceus ( a ) 3days after blunt abdominal trauma and confirmed by subsequent ct scan ( b ) in the present study , all delayed splenic injury complications were diagnosed in the first 7days after trauma , and none occurred in aast - sis grade i spleen injuries . 
this study demonstrate that ceus is a valuable imaging modality that could be performed during splenic injury followup ; in fact , splenic injury complications could be promptly diagnosed and embolized before a splenectomy would be necessary . 
this is particularly useful during the first 7days after trauma in patients with aast - sis grade ii , when complications are more probably to occur [ 9 ]  . 
4 50 - year - old man with a delayed splenic vascular injury showed by ceus ( a ) and ct scan ( b ) , and confirmed by subsequent dsa ( c ) la radiologia medica ( 2019 ) 124 : 170175 lower grade blunt splenic injuries in order to avoid a lot of unuseful ct scans [ 13 ]  . 
ceus allows to perform serial spleen injury evaluation at short time intervals , and our study results strongly support the use of ceus as a follow - up imaging modality of splenic injury . 
in fact ceus is safe , relatively cheap , and can be performed at the patients bedside in critical - ill patients , such as in intensive care unit ( icu ) ones . 
therefore , we could affirm that ceus could fill a gap in diagnostic imaging , and that it could represent the reference imaging modality in splenic injury follow - up . 
we do not have the haughtiness to think that the study cohort could be the representative of all the patient cohorts in other hospitals , but we think that the use of an imaging modality like ceus could be used at least in the first seven days after trauma in patients with aast - sis grade ii at pre - established intervals ( e.g. , 137days after trauma ) in order to diagnose dsvi and dae , and to reduce ct scans . this study has some limitations : it is a single - institute analysis , and the study population is small . 
however , to our knowledge , this is the first study which evaluated ceus efficacy in diagnosing dsvi and dae with respect to ct and dsa performing many serial ceus examinations . compliance with ethical standards conflict of interest the authors declared no potential conflicts of interests associated with this study . ethical standard all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
the morphometry of the pituitary stalk with 1.5t mr images was useful in diagnosing the infundibular lesion and to assess the efficacy of treatment given by chemotherapy for many pathological conditions . 
there are no data regarding the morphometry of the pituitary stalk in the adult population . methods one hundred and fifty normal brain mr images ( 75 males and 75 females ) were analyzed for the evaluation of stalk and other parameters . 
these normative data shall be of help in the evaluation of stalk in various neurosurgical and endocrinological pathologies and lead the radiologist and endocrinologist in the early diagnosis and management of hypothalamo - pituitary axis diseases . keywords fendersons funnel infundibulum morphometry mri pituitary stalk introduction pituitary stalk or infundibular stalk is an axonal tract of magnocellular neurons of supraoptic and paraventricular nuclei which connects the hypothalamic nuclei with * amirthalingam umamageswari dr_amirthauma@yahoo.co.in 1 department ofanatomy , jawaharlal institute ofpostgraduate medical education andresearch [ jipmer ] , dhanvantri nagar , pondicherry605006 , india 2 department ofradiodiagnosis , jawaharlal institute ofpostgraduate medical education andresearch [ jipmer ] , dhanvantri nagar , pondicherry605006 , india 3 department ofradiodiagnosis , sri manakulavinayagar medical college andhospital , kalitheerthalkuppam , puducherry605107 , india neurohypophysis . 
the normal morphometry of pituitary stalk and infundibular recess , in relation to adjacent floor of the third ventricle , helps to diagnose the pituitary infundibular lesion in an early stage which can help to avoid delay in diagnosis of pathological conditions like inflammation , infections , neoplasm , lymphocytic infundibuloneurohypophysitis , and neurosarcoidosis [ 37 ]  . 
high - resolution heavily t2 - weighted 3d sequence space ( sampling perfection with application optimized contrasts using different flip - angle evolution ) was used to acquire thin 1 - mm sections . 
true sagittal sections were confirmed by the presence of stalk , infundibular recess , cerebral aqueduct , and anteriorposterior commissural line in the same visualized midsagittal plane image . one hundred and fifty mr images ( 75 males and 75 females ) that were reported as normal by a neuroradiologist were included in the study . 
the ratio shows a gradual increase in the age - groups below 50years , and then , it starts decreasing in the elderly populations . 1 3 208 la radiologia medica ( 2019 ) 124 : 206210 fig . 
being a midline structure , the position and displacement of stalk give vital clues in the evaluation and differentiation of pituitary and hypothalamic lesions . in many diseases , stalk itself may be involved in the form of either stalk interruption as in congenital pituitary insufficiency , or enlargement in various inflammatory and neoplastic causes , or elongation in empty sella syndrome which has varied clinical presentations [ 8 ]  . 
there is a need for normative data in the evaluation of stalk to compare its normal morphologysize ( length ) , thickness ( diameter ) , and enhancementand position including stretch into the sellar compartment . mri is considered as the investigation of choice to diagnose the pituitary and infundibular lesions [ 9 ]  . 
there was a gradual increase in the length of the pituitary stalk from 18 to 60years ( table2 )  . the length and the position of the pituitary stalk can be influenced by the surrounding structure like tuberculum sellae , dorsum sellae , and diaphragm sellae . 
 the relation between the type of chiasm and the pituitary stalk was more often ( p < 0.05 ) 90 or greater for prefixed chiasmata and acute angles for normal or postfixed chiasmata . 
a prefixed chiasm will displace the pituitary stalk more anteriorly , which is prone to injury during anterior approaches to the midline skull base structures [ 12 ]  . the thickness of the stalk was considered larger in girls than boys in the adolescent age - groups in both mri and ct study [ 10 , 13 ]  . 
this correlates well with the present study . the thickness is important in diagnosing the hypothalamic lesions including glioma and neuroepithelial tumors like dermoid , teratoma , dysgerminoma , and hamartoma [ 13 ]  . 
isolated thickness can be seen in diabetes insipidus , but the presence of both diabetes insipidus and stalk thickening may be seen in germinomas [ 14 ]  . the stalk thickness is an important factor in follow - up of chemotherapy in case of diabetes and gh deficiency [ 15 ]  . 
the present study shows 5.24m there is a gradual increase in the depth from younger to elder individuals ( table2 )  . the recess may be elongated or enlarged with the apparent lengthening of the stalk in cases of empty sellathe extension of suprasellar csf space into the bony sellar compartment . 
in extreme cases , the suprasellar structure of optic chiasma itself may be dragged into the sella causing serious table 3 comparison of measurements of pituitary stalk with the previous study study study number of subjects diameter of the stalk ( mm ) length of the stalk ( mm ) depth of infundibular recess ( mm ) ratio of length of the stalk to the depth of the recess satogami etal . 
in the literature , the ratio between the pituitary stalk and the basilar artery was considered as a screening tool to evaluate the tumor involving the pituitary stalk [ 10 , 13 ]  . 
since the basilar artery localization is difficult in routine mri , this ratio can be considered as an alternative tool for the pituitary stalk - to - basilar artery ratio . 
an extensive study is needed to evaluate the sensitivity of the ratio in the clinical settings and its implications . conclusion the morphometry of the pituitary stalk is equally important as the pituitary gland . 
it can also be used in planning the appropriate management for the infundibular lesions based on the thickness and the modularity including metastatic disease in the follow - up neuroimaging . 
ceus spleen injury diagnostic sensitivity was 96.9% and , according to the american association for the surgery of trauma ( aast ) spleen injury scale ( sis ) , ceus - ct concordance was 95.8%. conclusions spleen injury healing time in blunt abdominal trauma nonoperatively managed is significantly related to aastsis grade , sch presence and grade , and spleen infarct development , and ceus can be used in order to evaluate spleen injury grade . keywords contrast - enhanced ultrasound ( ceus ) abdominal imaging spleen nonoperative management introduction the spleen is one of the most frequent splanchnic organs involved in blunt abdominal trauma , frequently reported as the second one after liver [ 1 , 2 ]  . 
nonoperative management ( nom ) is currently considered the best management option in stable patients in an optimal setting in which monitoring and frequent clinical evaluations are possible , and an * corrado tagliati corrado.tagliati@gmail.com 1 school ofradiology , universit politecnica delle marche , ancona , italy 2 sod clinica di radiologia , durgenza e dellarea oncologica , azienda ospedaliero universitaria ospedali riuniti , universit politecnica delle marche , ancona , italy 3 sod radiologia pediatrica e specialistica , azienda ospedaliero universitaria ospedali riuniti , universit politecnica delle marche , ancona , italy operating room is available for urgent laparotomy . 
nom allows the preservation of the important immunological spleen role , reducing the risk of future infections , the most serious of which are part of the overwhelming post - splenectomy infection ( opsi ) syndrome . 
moreover , avoidance of surgery - related complications , a shorter hospitalization period and a concomitant reduction in costs have been reported [ 3 ]  . some recent articles and guidelines define the timing of contact restriction and the conditions that require to repeat imaging after a splenic injury managed nonoperatively [ 46 ] , and a few previous studies assessed spleen injury healing time in adult patients nonoperatively managed [ 79 ]  . ct is considered the reference standard in order to detect and assess spleen injury grade , but a high ceus performance in these fields was reported in some previous studies and guidelines [ 1015 ]  . 
clinical follow - up lasted at least 6months ( range 612months )  . as serial ceus examinations were performed at preestablished intervals , spleen injury healing time was evaluated considering the number of ceus performed during follow - up . all patients underwent an abdomen - pelvis ct examination ( 16 slices ct philips brilliance ; philips medical systems , best , netherlands ) with iv administration of 90120 of iopamidol ( 370mg i / ml of iopamiro 370 ) using an electronic power injector ( ct injector ; medrad ) at a flow rate of 3ml / s . 
all patients with a ct - diagnosed spleen injury underwent at least one ceus study and no more than 8 ones during 6months period at pre - established intervals ( 1 , 3 , 8 , 15 , 30 , 60 , 90 and 180days after trauma ) , until spleen injury became no more identifiable . 
all scans were reported by a group of six radiologists with more than 10 - years experience in abdominal imaging ( ct , us and ceus ) and reviewed by two of theeach ct and ceus report stated the injury presence and its location and size . 
ct performed in the ed and the first ceus were evaluated in order to classify spleen injury grade using american association for the surgery of trauma ( aast ) spleen injury scale ( sis ) [ 17 ] ( table1 )  . 
the patients ( 5 out of 101 ) that developed a spleen infarct after splenic artery embolization ( ae ) were excluded from ceus sensitivity analysis and from the comparison of ct and ceus spleen injury grade evaluation , as the first ceus was done after ae and spleen infarct prevented a correct evaluation of injury grade . the study was approved by the institutional review board and the ethics committee of our institution . 
15.8 ( ostend , bel )  . table 1 association for the surgery of trauma ( aast ) spleen injury scale ( sis ) ( 1994 revision ) [ 10 ] grade injury type description of injury hematoma laceration hematoma laceration hematoma laceration laceration laceration vascular subcapsular , < 10% surface area capsular tear , < 1cm parenchymal depth subcapsular , 1050% surface area intraparenchymal , < 5cm in diameter capsular tear , 13cm parenchymal depth that does not involve a trabecular vessel subcapsular , > 50% surface area or expanding ; ruptured subcapsular or parenchymal hematoma ; intraparenchymal hematoma > 5cm or expanding > 3cm parenchymal depth involving trabecular vessels laceration involving segmental or hilar vessels producing major devascularization ( > 25% of spleen ) completely shattered spleen hilar vascular injury with devascularized spleen 1 3 la radiologia medica ( 2019 ) 124 : 163169 results table 3 mean ceus follow - up examinations and spleen injury healing time patients characteristics are summarized in table2 . mean ceus follow - up examinations and spleen injury healing time are reported in table 3 . 
the first follow - up ceus examination identified no - one spleen injury in 3 patients ( 3.1% ) , and all these patients were diagnosed as grade i by ct . 
 spleen injury healing time could be evaluated by ceus , and it is significantly related to aast - sis grade , sch presence and grade , and spleen infarct development . 
moreover , ceus is able to detect and correctly grade spleen injury severity . blunt abdominal trauma could cause hematoma or laceration that are showed by ct and ceus as hypodense or hypoechoic areas after contrast media injection . 
aast - sis , association for the surgery of traumaspleen injury scale ; sch , subcapsular hematoma ; ae , spleen artery angioembolization 1 3 166 la radiologia medica ( 2019 ) 124 : 163169 fig . 
1 78 - year - old man with aast - sis grade i showed by ct performed at the emergency department ( a ) and by ceus examination one day later ( b )  . 
two months later the lesion was no more detectable by ceus follow - up examination ( c ) spleen injuries progressively heal and , at least , become no more visible . western trauma association algorithm recommends contact restrictions for at least 4weeks for patients with aast - sis grade i injuries , 8weeks for patients with grade ii and grade iii injuries , and 12weeks for grade iv and grade v splenic injuries managed nonoperatively [ 4 ]  . 
the same algorithm reports that a routine post - discharge imaging study to confirm complete healing in asymptomatic patients has typically not been recommended except in patients with professions involving a high risk for contact [ 4 ]  . 
according to the world society of emergency surgery ( wses ) guidelines , activity restriction may be suggested for 46weeks in minor injuries ( aast - sis grade iii ) and up to 24months in moderate and severe injuries ( grade iiiv ) [ 5 ]  . 
in the outpatient setting , repeat imaging may also be helpful when a patient desires to return to a vigorous activity , such as contact sports [ 6 ]  . some previous studies assessed spleen injury healing time using us or ceus in pediatric population , and using us , ceus or ct in adult one [ 79 , 1820 ]  . 
in adult patients , ct is the most used imaging modality in spleen injury follow - up , but ceus is a promising alternative imaging modality in this field [ 21 ]  . 
to the best of our knowledge , only a previous study used ceus in order to evaluate spleen and liver injury healing time in adult patients [ 9 ]  . 
in particular , ceus was performed in the emergency room and repeated at 12 , 24 , 48h after the trauma ; later , ceus follow - up was performed at 30days and , in the event of persistent structural parenchymal alterations related to the trauma , again at 90days [ 9 ]  . 
therefore , our study is the first one that evaluated spleen injury healing time using ceus even in adult patients with aast - sis 1 3 la radiologia medica ( 2019 ) 124 : 163169 fig . 
no - one injury was showed by ceus examination in 3 patients ; therefore , they were considered false negative cases pts number of patients , aast - sis association for the surgery of traumaspleen injury scale grade iv and in which ceus examination was repeated up to 180days when necessary . 
our data confirmed previously reported direct correlation between aast - sis spleen trauma grade detected in the first ct carried out in the emergency department ( ed ) and the time required for radiographic healing [ 7 , 8 ]  . 
in the present study was found shorter healing time period than those previously reported by two studies in which spleen injury follow - up was performed in adult patients , respectively , with conventional us and ct [ 7 , 8 ]  . 
 previous studies assessed ceus performance and proved 1 3 168 la radiologia medica ( 2019 ) 124 : 163169 its accuracy in spleen injury detection and grade evaluation , even after angioembolization , and the present study is in line with them [ 10 , 16 , 22 ]  . although in recent years some publications have shown that there are some advantages in the use of the new grading system of splenic injury proposed by marmery etal . 
 [ 2326 ] particularly for predicting which patients with blunt splenic trauma need arteriography or splenic interventionaast - sis still continues to be the most widely used splenic injury grading system [ 3 , 2729 ] , and therefore , we have decided to use the latter . 
furthermore , using aast - sis in our study it was possible to compare spleen injury grade between ct examinations performed in the ed and ceus ones carried out the following day . 
this would not have been possible using the new classification system , as the patients who would have been classified as grades iva or ivb for ctdiagnosed active bleeding would have been classified as grades iiii by ceus examination , because the latter has always been performed after ae in these patients . this study could be useful in clinical practice as it allows to know spleen injury healing time evaluated by ceus in adult patients ; it also recognized some factors that are significantly related to healing time , such as aast - sis grade , sch presence and grade , and spleen infarct development . 
therefore , many factors related to spleen injury , and not only spleen injury grade , need to be taken into account in order to recommend activity limitations and contact restriction , particularly if follow - up us , ceus , or ct is not performed to demonstrate spleen injury healing . 
since ceus and ct scans were interpreted by two examiners consensually , inter - observer variability was not considered . compliance with ethical standards conflict of interest the authors declared no potential conflicts of interests associated with this study . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
we assessed qualitative ( presence and extent of wall thickening , degree of contrast enhancement of the thickened wall on cect images , and signal intensity of the thickened wall on t2 - weighted images ) and quantitative ( maximum thickness of the thickened wall ) imaging findings . results eccentric and smooth wall thickening was observed in 11 / 11 ( 100% ) patients . 
the signal intensity of the thickened wall on t2 - weighted images was isointense relative to that of normal lymph nodes in 7 / 8 ( 88% ) and mildly hyperintense in 1 / 8 ( 12% ) patient . 
they demonstrate * hiroki kato hkato@gifu - u.ac.jp 1 department ofradiology , gifu university school ofmedicine , 1 - 1 yanagido , gifu501 - 1194 , japan 2 department ofotolaryngology , gifu university school ofmedicine , gifu , japan 3 department oftumor pathology , gifu university school ofmedicine , gifu , japan bimodal patient age peaks at < 5years ( accounting for 20% of all branchial cleft anomalies ) and 2040years ( accounting for 75% of all branchial cleft anomalies ) without sex predilection . sbccs usually present as solitary , painless , fluctuant , and slow - growing masses in the lateral neck . 
sbccs are usually located at the anteromedial border of the sternocleidomastoid muscle , lateral to the carotid space , behind the angle of the mandible , and generally posterior to the submandibular gland . 
although atypical imaging features may be observed when the lesions are accompanied with infection , hemorrhage , or carcinomatous transformation [ 6 ] , to the best of our knowledge , no previous study has reported on imaging findings focused on wall thickening of infection - free and benign sbccs . 
hence , this study was performed with the aim of assessing the ct and mr imaging findings of infection - free and benign sbccs with an emphasis on qualitative and quantitative characteristics of wall thickening . materials andmethods patients the study was approved by the human research committee of the institutional review board , and complied with the guidelines of the health insurance portability and accountability act . 
we searched electronic medical records of gifu university hospital for patients histopathologically diagnosed with benign sbccs treated by complete excision between april 2004 and may 2018 and identified consecutive 18 patients with benign sbccs . 
among them , 5 patients with infected sbccs and 2 patients who underwent only unenhanced ct as preoperative radiological examination were excluded . in total , 11 patients ( 6 males and 5 females ; age range 1459years ; mean age 40years ) met the inclusion criteria ; these patients underwent preoperative contrast - enhanced ct ( cect ) and / or mr imaging . 
ten patients presented with painless neck swelling , and the remaining one patient presented with neck swelling with mild papatients characteristics are summarized in table1 . ct imaging all 11 patients were examined using multidetector - row ct . 
ct imaging was performed using a 8 - slice ct scanner ( lightspeed ultra ; ge healthcare , milwaukee , wi , usa ) , a 16 - slice ct scanner ( lightspeed 16 ; ge healthcare , milwaukee , wi , usa ) , or a 64 - slice ct scanner ( brilliance table 1 patient characteristics number of patients age ( year ) mean range gender male female location right left clinical symptom painless neck swelling neck swelling with mild pain examination ct ( contrast - enhanced ct ) mri ( contrast - enhanced mri ) 1459 11 ( 7 ) 8 ( 5 ) ct 64 ; philips medical systems , best , the netherlands )  . 
 unenhanced ct images were obtained in all patients , and contrast - enhanced ct images were obtained in 7 patients 45s after initiating intravenous bolus injection of 100ml of nonionic iodine contrast material containing 240 or 300 - mg iodine per ml . 
all mr images were obtained using the parallel imaging technique at 4 - mm section thickness with 1 - mm intersection gap with axial field of view ( fov ) of 20cm or coronal fov of 26caxial non - fat - suppressed t2 - weighted fast spin - echo ( tr / te , 41024269 / 90 ) , axial non - fat - suppressed t1 - weighted spin - echo ( tr / te , 679827 / 915 ) , coronal fat - suppressed t2 - weighted fast spin - echo ( tr / te , 39835283 / 8090 ) , and coronal non - fatsuppressed t1 - weighted spin - echo ( tr / te , 400713 / 1014 ) images were obtained in all patients . 
axial and coronal gadolinium - enhanced fat - suppressed t1 - weighted spin - echo ( tr / te , 623841 / 912 ) images were obtained in 5 patients after the intravenous injection of 0.1mmol / kg of gadopentetate dimeglumine ( magnevist , bayer healthcare , leverkusen , germany ) or gadobutrol ( gadavist , bayer healthcare , leverkusen , germany )  . 1 3 la radiologia medica ( 2019 ) 124 : 199205 image assessment two radiologists with 19 and 5years of post - training experience of head and neck imaging , respectively , reviewed the ct and mr images , and any disagreements among the radiologists were resolved by consensus . first , sbccs were classified into the following four subtypes on the basis of the bailey classification : i , the most superficial subtype , which reaches as deep as the platysma surface and lies along the anterior surface of the sternomastoid muscle ; ii , the most common subtype , identified along the surface of the sternomastoid muscle and posterior to the submandibular gland ; iii , extends medially at the bifurcation of the internal and external carotid arteries to the lateral pharyngeal wall ; and iv , arises in the pharyngeal mucosal space [ 7 ]  . second , we assessed qualitative imaging findings ( presence and extent of wall thickening , degree of contrast enhancement of the thickened wall on cect images , signal intensity of the thickened wall on t2 - weighted images , and signal intensity of intracavitary fluid on t2and t1 - weighted images )  . 
the extent of wall thickening ( percentage of the thickened wall to the circumference of the wall ) was qualitatively graded using the following fourpoint scale : 1 , small ( 1%25% ) ; 2 , moderate ( 26%50% ) ; 3 , extensive ( 51%75% ) ; and 4 diffuse ( 76%100% )  . 
the signal intensity of the thickened wall on t2 - weighted images was compared with that of normal lymph nodes , and the signal intensity of the intracavitary fluid on t2and t1 - weighted images was compared with that of the spinal cord . third , we assessed quantitative imaging findings ( maximum and minimum diameter of sbcc , maximum thickness of the thickened wall , and ct value of the intracavitary fluid )  . 
the maximum thickness of the thickened wall was measured on cect or mr images , whereas ct value of the intracavitary fluid was measured on unenhanced ct images . results table2 summarizes the imaging findings of sbccs . 
the maximum diameter was always consistent with the superior - to - inferior axis . with regard to the cyst wall , eccentric and smooth wall thickening was observed in 11 / 11 ( 100% ) patients , with the absence of mural irregularity and mural nodules ( figs.1 , 2 , 3 )  . 
the signal intensity of the thickened wall on t2 - weighted mr images was isointense relative to that of normal lymph nodes in 7 / 8 ( 88% ) and mildly hyperintense in 1 / 8 ( 12% ) patients . 
the signal intensity of the intracavitary fluid on t2 - weighted images was homogeneously table 2 ct and mr imaging findings of infection - free and benign sbcc patient no . / age / sex bailey classification maximum diameter ( mm ) eccentric and smooth wall thickening extent ( percentage ) of thickened wall maximum thickness of thickened wall ( mm ) ce of thickened wall on si of thickened wall on t2wi 1 / 44 / m 2 / 48 / f 3 / 49 / m 4 / 40 / m 5 / 20 / f 6 / 32 / m 7 / 50 / f 8 / 39 / f 9 / 14 / f 10 / 48 / m 11 / 59 / m extensive ( 51%75% ) small ( 1%25% ) moderate ( 26%50% ) small ( 1%25% ) moderate ( 26%50% ) moderate ( 26%50% ) moderate ( 26%50% ) moderate ( 26%50% ) small ( 1%25% ) moderate ( 26%50% ) small ( 1%25% ) mild , homo mild , homo mild , homo mild , homo mild hyper mild , homo mild , homo mild , homo sbcc = second branchial cleft cyst , ce = contrast enhancement , homo = homogeneous , na = not available , si = signal t2wi = t2 - weighted image , iso = isointensity , hyper = hyperintensity intensity , si of thickened wall on t2wi is compared with normal lymph nodes 1 3 202 la radiologia medica ( 2019 ) 124 : 199205 fig . 
coronal gadoliniumenhanced fat - suppressed t1 - weighted image ( tr / te , 650 / 12 ms ) shows a unilocular cystic lesion ( arrow ) with mildly enhanced eccentric and smooth wall thickening ( arrow head ) fig . 
 b axial t2 - weighted image ( tr / te , 4102 / 90ms ) shows a unilocular cystic lesion ( arrow ) with isointense wall thickening relative to normal lymph nodes ( arrow head )  . 
axial gadolinium - enhanced fatsuppressed t1 - weighted image ( tr / te , 841 / 9ms ) shows a unilocular cystic lesion ( arrow ) with mildly enhanced eccentric and smooth wall thickening ( arrow head ) 1 3 la radiologia medica ( 2019 ) 124 : 199205 fig . 
 b axial t2 - weighted image ( tr / te , 4415 / 100ms ) shows a unilocular cystic lesion ( arrow ) with slightly hyperintense wall thickening relative to normal lymph nodes ( arrow heads )  . 
 axial gadolinium - enhanced fatsuppressed t1 - weighted image ( tr / te , 607 / 10ms ) shows a unilocular cystic lesion ( arrow ) with mildly enhanced eccentric and smooth wall thickening ( arrow heads )  . 
hematoxylin and eosin ( h&e ) stain shows focal proliferation of lymphoid tissue ( arrows ) adjacent to the epithelium within thin cyst wall low , isointense , and hyperintense relative to those of the spinal cord in 1 / 8 ( 13% ) , 1 / 8 ( 13% ) , and 6 / 8 ( 75% ) patients , respectively . 
the signal intensity of intracavitary fluid on t1 - weighted images was homogeneously low , isointense , and hyperintense relative to those of the spinal cord in 1 / 8 ( 13% ) , 3 / 8 ( 38% ) , and 4 / 8 ( 50% ) patients , respectively . discussion sbccs are unilocular and usually between 2 and 6cm in diameter . 
histopathologically , sbccs are most commonly lined by stratified squamous epithelium ( 90% ) and less commonly by columnar respiratory epithelium ( 8% ) , with occasional goblet cells and transitional areas of both epithelia . 
because one of the characteristics of pathologic findings of sbccs is a lymphoid tissue with reactive germinal centers and without true lymph node architecture beneath the epithelium within the cyst wall , sbccs are also referred to as lymphoepithelial cysts . 
 although branchiogenic carcinoma , a squamous cell carcinoma ( scc ) arising in a branchial cyst , has been reported previously , it is currently considered to be an exceptional diagnosis , with < 40 patients fulfilling the strict diagnostic criteria [ 8 ]  . typical ct findings of sbccs include well - circumscribed and homogeneously hypodense cystic masses surrounded by a uniformly thin , smooth wall [ 2 , 5 ]  . 
the mural thickness is attributed to the response of the lymphoid tissue , and the degree of mural thickness varies depending on the presence and severity of any associated inflammatory processes [ 2 , 5 ]  . in the present study , infection - free and benign sbccs were always accompanied by eccentric and smooth wall thickening , which did not exceed 4mm in total thickness . 
conversely , infection of sbccs leads to necrosis of the epithelial lining , with variable degrees of acute and chronic inflammation and 1 3 204 la radiologia medica ( 2019 ) 124 : 199205 granulation of the tissue . 
because circumferential wall thickening is expected in infected sbccs , eccentric wall thickening may be a characteristic imaging feature of infection - free and benign sbccs . although the intracavitary fluid of sbccs typically showed low - to - intermediate signal intensity on t1 - weighted images , the proteinaceous content of sbcc or its chronic infection can also cause hyperintensity on t1 - weighted images [ 2 , 4 ]  . 
 although hyperintensity has been observed on t2 - weighted images because of the presence of intracystic fluid [ 4 ] , hypointensity on t2 - weighted images has been observed , albeit rarely , because of solidification of the cystic fluid [ 6 ]  . differential diagnoses of sbccs include benign and malignant conditions with cystic lesions in the lateral neck . 
 among patients with clinically diagnosed lateral cervical cysts , postoperative histopathological examination revealed malignancies in 9.2%14.4% of the patients ; the most common malignancy was cystic nodal metastasis from scc , followed by that from papillary thyroid carcinoma ( ptc ) [ 911 ]  . 
conversely , differential diagnoses of benign cystic lesion in the lateral neck include lymphangioma , venous malformation , diving ranula , abscess , and tuberculous / suppurative lymphadenitis [ 4 ]  . 
cystic schwannoma should also be included as a differential diagnosis of sbccs [ 12 ]  . the differential diagnosis between sbccs and cystic nodal metastases from scc can be challenging . 
this phenomenon is thought to be caused by the eccentric and smooth wall thickening in sbccs . cystic changes within nodal metastases occur in 26%70% of patients with nodal metastases from ptcs [ 16 , 17 ]  . 
however , because characteristic findings of nodal metastases from ptcs include a location in the mid or lower jugular chain , internal nodules , internal septum [ 18 ] , and a relatively small size ( mean 12mm ) [ 16 ] , these imaging findings could be the key for differentiating ptcs from sbccs . 
as for the signal intensity of cystic components on t1 - weighted images , although hyperintensity compared with fat was observed in 27% of nodal metastases from ptcs [ 16 ] , hyperintensity related to sbccs was observed inconsistently . this study had several limitations . 
however , because patients who underwent cect and / or mr imaging were included , we believe that assessment of cyst wall thickening could be performed accurately . conclusions in conclusion , eccentric and smooth wall thickening was common on cect and mr imaging findings in infectionfree and benign sbccs . 
histopathologically , the thickened walls of sbccs were mainly composed of lymphoid tissue adjacent to the epitheliuthese characteristic imaging findings of the walls of sbccs may be useful for differentiating them from other cystic lesions in the lateral neck . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . ethical standards this article does not contain any studies with human participants performed by any of the authors . informed consent for this type of study , formal consent is not required . 
a three - month retention time is reasonable for airway stents . keywords post - tracheotomy tracheal stenosis post - intubation tracheal stenosis airway stent fluoroscopy complications introduction tracheal intubation and tracheotomy with mechanical ventilation may bring a variety of potentially life - threatening complications , such as post - tracheotomy tracheal stenosis ( ptts ) and post - intubation tracheal stenosis ( pits ) , with an incidence ranges from 0.3 to 80% [ 1 ]  . 
surgical resection and end - to - end anastomosis are the classic techniques for dreamweaver08@126.com * xinwei han * gang wu wuganghenan2004@126.com 1 department ofinterventional radiology , the first affiliated hospital ofzhengzhou university , no.1 , east jian she road , zhengzhou450052 , china the treatment of tracheal stenosis [ 2 ]  . 
unfortunately , surgery is not suitable for patients with long segmental stenosis or complicated underlying diseases , and those patients may not be willing to undergo open surgery under general anesthesia [ 3 ]  . 
nowadays , a variety of minimally invasive interventional treatments , such as balloon dilation and tracheal stent implantation , is suggested as an alternative to surgery for patients with medical contraindications or recurrence restenosis [ 4 , 5 ]  . since first adoption of metallic airway stents to treat tracheal stenosis in 1989 [ 6 ] , airway stents have been widely used in clinic [ 710 ]  . 
although airway stents are well tolerated , safe and effective [ 1114 ] , this treatment is still debatable and even abandoned in clinical practice for benign tracheal stenosis due to high rate of symptomatic vol . : ( 0123456789 ) 1 3 192 la radiologia medica ( 2019 ) 124 : 191198 recurrence and complications [ 1517 ]  . 
covered stents should be removed within a certain time to reduce longterm complications for benign stenosis [ 18 , 19 ] , which was usually performed by flexible bronchoscopy under general anesthesia or local anesthesia [ 11 , 12 , 16 , 17 , 2032 ]  . 
we reported our clinical results in stent removal for ptts and pits under fluoroscopic guidance and local anesthesia . materials andmethods patients this study was approved by the ethics committee and medical records management section of our university ( permit number : keyan - 2017 - 023 )  . 
all patients were indicated surgical resection ; however , they were unable to tolerate anesthesia due to severe dyspnea and had to implant stents first to alleviate the symptoms , to avoid unexpected accidents or even death . 
a 5f vertebral artery catheter ( cook corporation , bloomington , ind , usa ) was advanced along a 0.035 inch stiff hydrophilic guide wire ( cook corporation )  . 
routine removal defines as stent removal in patients with no obvious symptom or sign , although complications such as excessive granulation tissue or stent migration may able to be found during stent removal or by endoscopy . 
a severe pits was shown by ct before stenting ( a ) , which was dilated after stenting and 2months after stent removal ( b ) 1 3 la radiologia medica ( 2019 ) 124 : 191198 fig . 
one piece of strut residue was successfully removed endoscopically ( c ) patency defines as patent airway condition after stent removal without restenosis , tracheal intubation , tracheotomy , surgical resection or death . 
statistical significance was considered when p < 0.05. results the patients characteristics thirty - eight airway stents were successfully inserted in 32 consecutive patients over a five - year period . 
two patients showed dyspnea immediately after removal and required mechanical ventilation in ptts ( table3 )  . second stenting afterremoval intolerance of stenting , stent migration and replacement of bare stent . 
following doctors advice , more than half of patients were admitted to hospital for stents removal to avoid long - term complications , although they complained no obvious symptom or sign . 
 restenosis caused by tissue hyperplasia was the most common indication for later stent removal . complications ofstent insertion andremoval insufficient expansion of stents was most common complication immediately after stent insertion ; balloon tracheoplasty was performed for those with severe tracheal stenosis . 
besides , three patients showed stent migration and one patient complained of intolerance of stenting in ptts . except strut residue in three stent removal , 35 of 38 airway stents were successfully removed fluoroscopically , with a technical success rate of 92.1%. 
there were six complications of second stenting was performed in six cases ; included four stents were inserted again after removal due to restenosis in pits , and two stents were inserted after removal due to stent migration in ptts . 
coronal ct showed that the stent was in good position immediately after stent placement ( a ) , and the stent was obviously migrated downwards more than 2months later ( b )  . 
airway stents have been widely used in clinic [ 710 ] , which are reported as well tolerated , safe and effective for management of benign tracheal stenosis [ 1114 ]  . 
for benign stenosis , airway stents should be removed within a certain time to reduce complications caused by long - term stent retention , because a limited retention is capable of relieving dyspnea and minimizing recurrence of stenosis by routine stent removal [ 18 , 19 ]  . stent insertion and extraction was usually performed by flexible bronchoscopy under general anesthesia or conscious sedation [ 11 , 12 , 16 , 2024 ]  . 
our data indicated that fluoroscopic insertion and removal of airway stent is safe and effective for pits and ptts . the application of airway stent is becoming more and more widespread in benign tracheal stenosis . 
the incidence of complications was similar as that previously reported in rigid bronchoscopy [ 27 , 28 , 32 , 35 ]  . major complications ( such as stent migration and stent rupture ) are generally considered indications of stent removal [ 14 ]  . 
in our opinion , the shorter the stent retention time ( 3months ) the better once achieves the purpose of treatment to avoid long - term complications . in conclusion , fluoroscopic insertion and removal of airway stent is safe and effective for pits and ptts . 
indications for treatment were the risk of rupture / hemorrhage due to size greater than 4cm and symptomatology ; in one case , a previous hemorrhage was the indication for treatment . 
technical and clinical success , safety , and quality of life ( qol ) were evaluated in a mean follow - up of 9months ( range 312 )  . results technical success was obtained in all cases . 
clinical success was obtained in all cases ; the volume of the ablated amls was not related with symptoms relief ; all patients referred a significant improvement in their qol , with a regularization of daily activities . 
post - ablation syndrome was registered in 5 cases and was self - limited in all cases . conclusions symptoms relief , lower risk of hemorrhage and a normalized qol were obtained in all patients with a safe and mini - invasive procedure . keywords angiomyolipoma tuberous sclerosis quality of life microwaves introduction tuberous sclerosis complex ( tsc ) is a genetic disorder characterized by the growth of hamartomas in multiple organs . 
 up to 80% of patients with tsc have at least 1 angiomyolipoma ( aml ) in their lifetime [ 1 ]  . their growth can be rapid and unpredictable and may cause problems including hemorrhage , renal dysfunction , and rarely venous thrombosis [ 2 ]  . 
it has been shown that renal amls > 4cm are at increased risk of further growth and eventual hemorrhage [ 3 ]  . nephron preservation is a key treatment consideration , especially in patients with multiple , bilateral , and often very large amls , like those suffering from tsc [ 4 ]  . 
for many years , first - line treatment of these lesions was surgical excision ; nephron sparing surgery permits to preserve renal function , but in particular in patients with tsc , the * gianpaolo carrafiello gcarraf@gmail.com 1 diagnostic andinterventional radiology department , asst santi paolo e carlo , san paolo hospital , university ofmilan , via a di rudin 8 , 20142milan , italy 2 radiology department , uninsubria , varese , italy 3 nephrology department , san paolo hospital , university ofmilan , via a di rudin 8 , 20142milan , italy 4 nuclear medicine department , irccs istituto nazionale dei tumori , milan , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 176183 propensity for recurrences is high so these patients have to be undergone several surgical treatments for multiple amls [ 5 ]  . advances in minimally invasive techniques allow for most of these tumors to be successfully treated [ 6 ]  . 
transarterial embolization has an established role in the modern management of renal lesions amenable to nephron sparing options , especially in larger aml and in acutely bleeding lesions [ 5 ]  . a number of investigators have explored the use of percutaneous ablative techniques such as radiofrequency ( rf ) ablation , cryoablation , and microwave ( mw ) ablation for the treatment of amls [ 5 ]  . compared to rf , mw energy produces larger and hotter ablation zones in less time [ 7 ] and more effectively penetrates macroscopic fat [ 8 ] , which is the major component of most amls . thanks to its known less intra - procedural pain , safety , and repeatabilities , percutaneous mwa is generally well tolerated by all patients treated [ 9 ]  . the aim of the present study was to evaluate safety , efficacy , and quality of the life of the patients with tsc treated with percutaneous mwa . materials andmethods patients this retrospective study was compliant with the health insurance portability and accountability act ( hipaa )  . 
 clinical and radiological data were retrospectively reviewed for all patients who had tcs associated with amls . our series includes nine patients ( 7 females and 2 males ; mean age 27.6years , range 2334 ) , with 10 renal amls ( all tcs associated ) with a mean size 42.8cm ( range 2470 ) ( table1 ) treated with image - guided percutaneous mw ablation . 
the primary indication for treatment was risk of rupture / hemorrhage due to size greater than 4cm ; moreover , in all patients a persistent growth was observed and all patients were symptomatic , flank pain and pressure except that one ; in the latter case , a previous hemorrhage was the indication for treatment ( table1 )  . the procedures were performed between july 2016 and december 2017 . 
patients were referred to our interventional radiology department by nephrologists of our hospital where patients with tcs refer . each patients case was discussed in the contest of a multidisciplinary meeting , during which the indication for thermal ablation was given . 
indications , benefits , and risks of the procedure were explained and discussed with every patient , and informed consent was obtained before treatment . three of the patients treated presented neurological involvement , well controlled with medications ; all patients presented cutaneous angiofibromas . coagulation blood tests resulted within the reference values in all patients [ 10 ]  . a first - generation cephalosporin ( cefazolin 2 gr b.i.d. ; pfizer srl , milan , italy ) was administered at the beginning of every procedure as antibiotic prophylaxis . procedure a 10 ml solution of lidocaine was injected to obtain local anesthesia in correspondence with the entrance site of the antenna . 
vital parameters ( heart rate , respiratory rate , and blood pressure ) , together with oxygen saturation and electrocardiographic tracing , were continuously monitored during the procedure . the antenna was positioned under us guidance ( arietta v70 ( hitachi aloka medical , tokyo , japan ) ) in 2 cases . 
after the guided placement of the antenna into the target tumor , the ablative procedure itself consisted in the delivery of thermal energy to the tissue , produced by maintenance of a power of 100w for a total time between 5 and 9min , as specified by the manufacturer , obtaining the desired necrosis volume . outcomes technical success consisted in a correct position of the antenna into the target lesion , as planned before treatment . 
 time of ablation was registered in all patients . clinical success was defined as the improvement or disappearance of the symptomatology and the normal performance for daily activities . as mentioned above , all patients had a pre - procedural mri . 
1 ct scan performed during the procedure to assess the correct position of the antenna ( a , b ) ; dynamic mri acquisition after iv administration of contrast medium performed 4weeks after the procedure confirmed the ablated area within the aml ( c , d ) fig . 
moreover , they were asked about the tolerance of the procedure ( post - ablation syndrome ( fever , malaise , pain , myalgia , nausea and vomiting ) usually resolving within 4days post - procedure ) [ 12 ] and post - procedural paa single trained interviewer registered prospectively the data about the qol before treatment , and then , the information obtained by a phone interview about symptomatology and daily activities after 4 weeks , 3 , 6 , and 12months after the procedure . 
sf - 36 includes one multiitem scale that assesses eight health concepts : ( 1 ) limitations in physical activities because of health problems ; ( 2 ) limitations in social activities because of physical or emotional problems ; ( 3 ) limitations in usual role activities because of physical health problems ; ( 4 ) bodily pain ; ( 5 ) general mental health ( psychological distress and wellbeing ) ; ( 6 ) limitations in usual role activities because of emotional problems ; ( 7 ) vitality ( energy and fatigue ) ; and ( 8 ) general health perceptions . in table3 , we indicated the tolerance of the procedure , post - procedural pain , and the scored qol of our patients before the procedure , and then 4weeks , 3 , 6 and 12months after the procedure . complications were classified according to common terminology criteria for adverse events [ 13 , 14 ]  . safety was evaluated on the basis of the complications recorded immediately after the procedure and during the follow - up . 
a complication was defined as immediate when table 3 quality - of - life questionnaire included : procedure tolerance ; health concepts ( physical or emotional problems concerning health ) procedure tolerance ( pa sdr ) ; post - procedural pain pre - procedure sf - 36 health status 4w post - procedure sf - 36 health status 3m post - procedure sf - 36 health status 6m post - procedure sf - 36 health status 12m post - procedure sf - 36 health status m , 28 yo 3 d mild fever ; f , 25 yo no pain 2 d fever , myalgia ; no pain no ; no f , 34 yo no ; no f , 25 yo 3 d fever , myalgia , nausea ; 2 d myalgia ; f , 23 yo f , 31 yo no ; no f , 26 yo no ; no m , 30 yo no ; no f , 27 yo 3 d myalgia , nausea ; no ( dancer ) ( runner ) m male , f female , yo years old , pa sdr post - ablation syndrome , w weeks , mmonths , d days 1 3 la radiologia medica ( 2019 ) 124 : 176183 it occurred up to 24h following the procedure , as periprocedural if occurred within 30days , and as delayed if occurred more than 30days after the procedure [ 14 ]  . 
major complications were defined as events that , if untreated , could leave to life - threatening , or events that led to substantial morbidity and disability , or could be cause of hospital readmission or substantially lengthened the patients hospital stay [ 14 ]  . 
minor complications included characteristic symptoms of the post - ablation syndrome ( fever , pain , nausea , and vomiting ) if lasting more than 4days after the ablation procedure . was not significantly related with the improvement in the symptoms . no patients have experienced renal hemorrhage , and all patients are asymptomatic at 12 - month follow - up . 
 one patient developed a small post - procedural subcapsular hematoma which was self - limited and clinically occult . post - ablation syndrome was registered in 5 cases and was statistic analysis spss v25.0 ( chicago , il ) was used for all statistical analyses . 
mean ablation time was 5min and 3s ( range 39min )  . technical success was obtained in all cases : antenna was correctly positioned within the lesion . post - ablation imaging demonstrated the area of ablation , compared with pre - procedural mri . 
the volume of ablation renal manifestations are the second most common findings associated with tsc , with amls occurring in 80% and renal cystic disease in 50% of patients , but only 3% of these patients present polycystic kidney disease ( pkd ) [ 15 ]  . typically children with tsc are born with normal kidneys , but develop cystic disease and angiomyolipomas as they age . 
3 scatter plot of distribution of health status ( assessed by sf - 36 questionnaire ) per time 1 3 182 la radiologia medica ( 2019 ) 124 : 176183 ( ckd ) , affecting approximately one million patients with tsc worldwide [ 15 ]  . ckd represents the most common causes of death in adult patients , with increasing morbidity and mortality [ 16 ]  . a cross - sectional study of tsc patients revealed an increase in amls during childhood and adolescence that then stabilized throughout adulthood [ 17 ]  . 
angiomyolipomas significantly affect the lives of patients because these lesions are at high risk of hemorrhage when a diameter is larger than 4cm and can invade adjacent normal renal parenchyma leading to ckd with development , sometimes , of uremia . given the frequent association of tsc and amls , the most logical intervention is to treat amls with diameter greater than 4cm to reduce risk of hemorrhage , and not to actually remove the aml . 
due to the bilateral nature of the renal lesions in tsc , and in order to preserve functional renal mass , nephrectomy should not be undertaken without a very careful risk - benefit analysis . the indications for the treatment of amls are different : to avoid hemorrhage , that is one of the most important aims , to destroy the mesenchymal tumor elements ; these results must be obtained by thermal coagulation . like in other districts ( uterus , liver , etc . ) , if technically possible , we preferred thermo - ablation over embolization , because in most cases post - procedural course is uneventful and post - ablation syndrome , when present , is milder than post - embolization symptomatology . the results of preliminary studies suggest that mw ablation of renal amls is technically feasible and appears to be safe and effective at early follow - up [ 8 ]  . thermal ablation is widely accepted as second - line therapy for medically or surgically inoperable patients with small renal cell carcinomas ( rcc ) [ 18 , 19 ]  . in the literature , the use of other percutaneous ablative techniques such as radiofrequency ( rf ) ablation and cryoablation was described . 
as for radiofrequency , recently published series include small amls ( 1.52.5cm ) [ 6 ]  . although rfa and cryoablation appear to be safe in smalland medium - sized renal amls , long - term efficacy data are lacking [ 6 ]  . the indications for the treatment of aml are different ; avoiding hemorrhage is one of the most important aims whereby immediate vascular thrombosis and destroying the mesenchymal tumor elements by thermal coagulation must be obtained . 
tissues with low electrical conductivity ( such as fat ) force current to higher conductivity pathways in the electrical circuit , thereby reducing the amount of heat generated in the low - conductivity fat , resulting in less effective tissue heating [ 20 ]  . 
in 2 cases , patients started to play sports again and in all cases an improvement in symptoms was registered ; moreover , a lower risk of hemorrhage was immediately obtained , because mri images performed during follow - up revealed the volume of ablation and in particular the necrosis of the most vascularized areas of the aml ( compared to pre - procedural images )  . 
our patients with amls are all affected by tcs ; clinicians consider quality of life an important parameter in this class of patients , because tcs may lead to neurological symptoms , pulmonary involvement as well as renal disease discussed [ 15 ]  . 
moreover the vogts triad ( facial angiofibromas , mental retardation and intractable epilepsy ) may characterize these patients , even if less than 40% of them have all three features [ 23 ]  . 
in our series , all well - controlled patients presented extra - renal disease ; thermal ablation of amls gave them a restitutio to normal daily activities with an estimated increase in health status of 0.683 per week ( data from standardized regression coefficient )  . 
symptoms relief , lower risk of hemorrhage and a normalized quality of life were obtained in all patients . pearson analysis could not demonstrate a statistically significant correlation between preand post - procedural health status and aml volume or treated area volume . in conclusion , a longer follow - up and most numerous samples are necessary to confirm our preliminary results . 
 moreover , a randomized study to compare mwa and embolization should be planned to evaluate safety , effectiveness , and compliance of the patient . 1 3 la radiologia medica ( 2019 ) 124 : 176183 compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 234240 radiotherapy evaluation ofitalian radiotherapy research from1985 to2005 : preliminary analysis albafiorentino1 rosariomazzola2 valentinalancellotta3 simonettasaldi3 sarachierchini3 annaritaalitto4 paoloborghetti5 fabianagregucci1 michelefiore6 isaccodesideri7 lorenzamarino8 danielagreto7 giovannidomenicotebala9 airo giovani italian association of radiation oncology - young members working group received : 13 september 2018 / accepted : 2 november 2018 / published online : 14 november 2018 italian society of medical radiology 2018 abstract aim the difficulty in conducting meaningful clinical research is a multifactorial issue , involving political , financial and cultural problems , which can lead to unexpected negative long - term consequences , in terms of knowledge advancement and impact on patient care . 
the aims of the present review were to evaluate the publications of italian radiotherapy ( rt ) groups during a 20 - year period and to verify whether research is still appealing to young radiation oncologists ( ros ) in italy . methods pubmed database was searched for english - language articles published by italian groups from january 1985 to december 2005 . 
analyzed variables were : publication / year , kind of study , geographical area and age of the first author . results the systematic review identified 3291 articles : 1207 papers fulfilled the inclusion criteria . 
the age of the first / second author was evaluated on 716 papers : in more than 50% of cases , the first author was younger than 40 . conclusion despite a general gradual improvement , rt clinical research suffers in italy ( as elsewhere ) from insufficient funding , with a negative impact on evidence production . 
it is worth noting that clinical research is still appealing and accessible to junior italian ro . keywords radiotherapy italian research * alba fiorentino albafiorentino@hotmail.it 1 radiotherapy oncology department , general regional hospital f . 
127km 4 , 70021acquavivadellefonti , bari , italy 2 radiotherapy oncology department , sacro cuore don calabria hospital , negrar , verona , italy 3 radiation oncology section , university ofperugia , perugia , italy 4 radiotherapy oncology department , fondazione policlinico universitario a . 
gemelli irccs , uoc radioterapia , rome , italy 5 radiation oncology department university andspedali civili , brescia , italy 6 radiation oncology , campus bio - medico university , rome , italy 7 department ofbiomedical , experimental andclinical sciences mario serio , section ofradiation oncology , university offlorence , florence , italy 8 radiotherapy oncology department , rem , viagrande , catania , italy 9 surgical department , east kent hospitals university nhs foundation trust , ashford , uk vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 234240 introduction for the oncological community , as well as for the whole medical community , clinical research is crucial to determine the safety and effectiveness of medications , devices , diagnostic procedures and treatment regimens for cancer patients . 
the so - called pyramid of levels of evidence provides a way to evaluate the quality of the available evidence ( level of evidence , loe ) and the reliability of consequent recommendations ( grade of recommendation , gor )  . 
it is therefore important to understand , both from a public policy perspective and from clinicians , including universities and national association of radiation oncology , point of view , the evolution of radiation therapy research , to identify strengths , weaknesses and opportunities . the aim of the present research was to perform a critical appraisal of the italian scientific amount in the field of radiation oncology in a 30 - year period ( 19852015 ) , to define its trend and to emphasize its strength and weaknesses . 
moreover , we aimed at evaluating the impact of junior radiation oncologists ( ros ) on the whole scientific production and to speculate whether research is still accessible and appealing to young specialists . this preliminary analysis reports an evaluation of the first 20years ( from 1985 to 2005 ) , just to get an early idea of the big picture , in order to be able to plan the subsequent analysis on the correct indicators . materials andmethods literature search andselection ofstudies pubmed database was searched by two independent ros , for articles published in english from january 1985 to december 2015 using as keywords radiotherapy combined with italy [ ( radiotherapy ) and ( italy ) ]  . 
studies eligible for inclusion in this analysis were : case reports , radiobiological studies , clinical and dosimetric retrospective or prospective studies ( phase iiiiii ) in which rt was used , systematic or not reviews and meta - analyses . 
 exclusion criteria were : study not conducted in italy , study in which rt was not used or was not investigated , study in which no italian ro was in the authors list . statistical analysis the abstracts of the selected papers were analyzed , and the following variables were considered : ( 1 ) year of publication ; ( 2 ) type of trial ( retrospective , prospective , including phase iiiiii trials , reviews , metanalysis , case reports , dosimetric study , translational and radiobiological research ) ; ( 3 ) geographical area of rt institution ( northern , central and southern italy ) ; ( 4 ) age of the first / second author ( only in the papers whose authors were a ro )  . 
to summarize the most relevant findings of the analyzed variables , descriptive statistics and linear regression analysis were performed on medcalc ver 18.2. results the systematic pubmed search ( 19852015 ) identified 9729 records . 
the present study is not a systematic review aimed at the statistical analysis of pooled data , but just a gross evaluation of the scientific production in a single country and in a specific time frame . 
the peak of number of papers in 1994 could be explained due to the improvements of tc simulation in the early 1990s ; in fact , most of papers are retrospective analysis analyzing tc simulation . based on the type of study , retrospective analysis , prospective phase iii trials and literature reviews were 44 , 20 and 14.5% of all published data , respectively . 
since 2000s , the regression analysis showed that randomized trials quantitatively increased with a linear trend ( r2 = 0.78 ) , although their absolute number remains low ( 48 / 1207 , 4% of all the publications )  . as regards the geographical area where the research was conducted , despite a general increase in the research production in all the areas ( fig.4 ) , northern italy provided the bulk of italian research in rt ( 58.7% ) , whereas southern italy published only 7.2% of all the studies here analyzed . after further review , the articles whose first / second author was not a ro were excluded , and in the remaining papers ( 716 / 1207 , 59.3% ) , the age of the first / second author was recorded . 
5 rate of young ( < 40yo ) first authors per year authored by junior ro increased , the percentage of studies where the first / second author was under 40 showed a progressive reduction . [ 4 , 5 ] , but we must not forget that the continuous widening of the spectrum of indications to rt takes the steps from the findings of clinical research . discussion during the natural history of oncologic diseases , approximately 60% of patients receive rt as part of their therapeutic course . 
in the last few years , the scientific community saw a worldwide improved access to rt , to deliver a comprehensive cancer treatment in 2012 , the european society for radiotherapy and oncology ( estro ) published a document on the future development and growth of rt and clinical oncology both within europe and at a global level in the forthcoming decades , where the society confirmed the importance of optimal individualized patient care that could be reached by integrating new clinical and preclinical evidence from biology , molecular / functional and anatomic imaging and the use of new systemic agents together with the delivery of high precision radiation therapy [ 7 ]  . 
although the investments in rt are often heterogeneous , the implementation of 1 3 238 la radiologia medica ( 2019 ) 124 : 234240 high - quality rt needed technical advances , such as imageguided rt , intensity - modulated rt , stereotactic body rt and radiosurgery , and heavy particles therapy . 
in fact , the increasing amount of robust evidence about new rt approaches allowed an expansion of the population for whom rt will be part of evidence - based cancer [ 8 , 9 ]  . 
what is the part played by italian scholars in rt within the big worldwide picture ? in other terms , what is the impact of italian scientific production , specific to rt , on the worldwide knowledge ? as junior members of the italian association of radiation oncologist ( airo ) , we aimed to perform a critical appraisal of the scientific production in rt coming from italian centers in quite a longtime span ( 30years )  . 
 therefore , we decided to carry on a preliminary analysis on the first two decades ( 19852005 ) to have a rough idea of the trend during the years , in terms of number of publications , geographical area of production of the study and age of the first / second author . 
in consideration that new techniques and technologies ( e.g. , intensity - modulated rt or igrt ) have been implemented in the first years of 2000 , the idea that from 2005 to nowadays the italian research was more complex than the past was the background for splitting the analysis of entire period . 
the subsequent evaluation ( 19852015 ) will be based on the findings of the present preliminary results . to our knowledge , this is the first study aimed at performing critical analysis of the amount and type of research on rt in italy with the intent to identify straight and weakness for the future planning of rt research , investments for rt centers and universities . 
about the type of publications , retrospective studies represented more than 40% of the whole scientific production , because collection and analysis of data are easier , the absence of implications such as randomization , informed consent and ethical and legal issues and the much lower costs . 
however , these studies provide evidence of a lower level ( loe - 2b ) so they usually cannot be used to draw sensible recommendations ( gor - 2 )  . 
moreover , in terms of phase iii trial , usa , japan , italy , republic of korea and spain had a relatively low ratio of phase iii / phase ii trials ; conversely , uk , netherlands , sweden and poland published more phase iii studies [ 10 ]  . 
this discrepancy is not clear but , probably , could be related to economic and cultural factors [ 10 ]  . at the same time , the number of reviews and meta - analyses is increasing , meaning that probably a growing number of authors decided to devote themselves to cheaper , timeefficient and office - based studies , which can be published on high - rank journals and attract funding and career improvements , instead of embarking in difficult , time - consuming and expensive rcts [ 2 ]  . 
several authors pointed out how , at least in the last decade , there has been a worldwide linear increase in rcts and an exponential increase in systematic reviews and meta - analyses [ 2 , 1214 ]  . 
the authors showed that only 5.3% of the oncological studies were rt trials and that sponsorship or funding for rt trials was significantly less than that for other oncological studies [ 15 ]  . 
these data support the hypothesis that , to date in oncology , research funding seems to be mainly focused to improve the armamentarium of new drugs , and unfortunately , private and governmental support for research in radiation oncology is significantly lower than for medical oncology [ 14 ]  . 
we wonder if there is a direct causative relation between the paucity of funding and the absence of well - structured changing practice rcts in rt . about the geographical area of research , northern italy produced the very most of italian scientific papers . 
probably , the northsouth gap can be explained by several aspects : ( 1 ) the number of rt centers , ( 2 ) the number of research centers , including universities , ( 3 ) the unequal distribution of funds and ( 4 ) the differences in terms of technologies . 
in fact , the numbers of rt centers increased during the analyzed period ( 77 in the 1989 , 96 in 1995 and 138 in 2002 ) , but about 50% of the centers were in the northern italy , despite similar population density . 
on the other hand , in the next years , the italian universities will be called to improve the young specialists formation in terms of methodological scientific education and we are sure that this will represent a great boost for research in italy , in particular in the analyzed field . 
this too entails the need for adequate financing . finally , the present analysis was the first report about the role of the contribution of young ro to rt research publication . 
thus , an increasing number of young specialists result as first / second author of papers in the 1990s , probably due to the relatively young age of radiation oncology as a single specialty in medicine . 
however , the trend of the rate of junior authors on the total number of papers published per year showed that in the same period , the percentage of papers whose first author is under 40 is gradually reducing . 
 the growing clinical commitment of junior ro and trainees , and the modifications of their timetables after the introduction of the european working time directive represent two factors which might have diverted time from research . 
scientific societies , including airo , and universities should support trainees and junior ro in getting a good training in research methodology , either during or after the specialist training , and to have access to research grants and facilities . 
 italian ministries for health and for education , university and research recently promoted research programs explicitly reserved for younger researchers , and more than 1300 university research positions for younger people have been financed for the current year . 
however , considering the costs of clinical research and randomized trials , especially if no profit , this financial effort should be increased to obtain a significant impact on the research systeit should be also noted that trials in radiation oncology are often less costly than trials in other clinical disciplines . 
other assets that can be exploited to facilitate an increased involvement of young specialists in radiation oncology research are the estro school of radiotherapy and oncology that aims to improve , professionalize and standardize knowledge and practice in radiation oncology and the young associations , including estro and airo young [ 1620 ]  . 
these associations can establish a solid network of connections and promote educational and research projects , contributing to an increasing role of young specialists in clinical research in radiation oncology . conclusion in conclusion , despite the limitation of the present data ( analysis of published papers in which major pitfall is to balance methodological and scientific issues with political ones ) showed that italian research in rt in the period 19852005 has been generally good , in terms of numbers of publications , and its quality , in terms of number of changing practice studies , is slowly but steadily improving . 
the simple parameters we have evaluated represent sufficiently reliable indicators to get a gross picture of rt research in italy , in the period considered , allowing to study its evolution in the subsequent periods analyzing bibliometrics parameters to evaluate also the quality of research . compliance with ethical standards conflict of interest alba fiorentino declares that she has no conflict of interest . 
it was requested that only one physician per facility completed the survey , and that he / she was dedicated to pc management in his / her daily clinical practice . 
more than 80% of respondents would perform radiotherapy ( rt ) to both the prostate and all metastases sites , but mostly up to 23 metastases ; furthermore , > 80% of physicians would perform rt on both nodal and bone secondary lesions . 
most respondents deem a cholineor prostate - specific membrane antigen ( psma ) - positron emission tomography ( pet ) mandatory before considering a patient affected by ompc for non - palliative rt . 
more than 90% of respondents confirmed to be interested in participating in a multicentre study regarding this subject . conclusions this survey investigated the current opinion of italian radiation oncologists and confirmed their interest in ompc management . keywords prostate cancer oligometastatic radiotherapy survey introduction local control of primary tumour in the presence of metastatic disease has been associated with improved outcome in several malignancies . 
nevertheless , the recent development of imaging techniques , such as cholineand prostate - specific membrane antigen ( psma ) - positron emission tomography ( pet ) / computed tomography ( ct ) , allows an earlier detection of metastatic disease in an intermediate state of tumour spread with better prognosis . 
in this subset of patients , a more aggressive approach could improve tumour control , postpone biochemical and clinical disease progression and delay the start of more toxic systemic treatments [ 4 ]  . 
limited retrospective studies suggested that interventions , including local and / or metastasis - directed therapy using surgery and rt , can improve survival outcomes with minimal risk of adverse effects [ 5 ]  . 
 since there are no guidelines to address this kind of treatment approach and studies providing rt + adt in this cohort are ongoing , the aim of this survey was to evaluate the current management of abinitio oligometastatic prostate cancer ( ompc ) patients in the italian radiotherapy facilities and to investigate the interest in participating in a multicentre study . table 1 list of questions included in the survey methods the study was conducted on behalf of the uro - oncologic study group of associazione italiana di radioterapia e oncologia clinica ( airo )  . 
it was requested that only one physician per facility completed the survey and that he / she was dedicated to pc management in his / her daily clinical practice . the questionnaire consisted of 15 questions concerning the management of abinitio ompc . 
the rate of completion after beginning the questionnaire was 100% , and the standard completion time was 4min . at question 1 , 27% of respondents answered they have been working as radiation oncologists for less than 5years , 15% for 510years , 30% for 1020years and 28% for more for how long have you been working as a radiation oncologist ? are you specifically involved in the treatment of pc ? in what kind of facility are you currently working ? where is your department geographically located ? is a regular prostate multidisciplinary team meeting performed in your facility ? how many patients affected with abinitio ompc are annually referred to your department for non - palliative rt ? which criteria do you adopt to evaluate if a patient affected with abinitio ompc is a candidate to non - palliative rt ? in a fit non - symptomatic patient affected with abinitio ompc what treatment would you recommend ? what imaging technique do you consider mandatory to evaluate this subset of patients ? which secondary lesions would you irradiate with non - palliative intent ? what volumes would you treat ? what technique and fractionation would you adopt ? how would you associate adt ? how would you perform the follow - up of these patients after treatment ? would you be interested in participating in a multicentre study of rt associated with adt in patients affected with abinitio ompc ? 1 3 la radiologia medica ( 2019 ) 124 : 211217 than 20 years . 
the majority of respondents work in a public non - academic facility ( 50% ) , while 31% work in a public academic or research institute and 19% in a private centre . 
 regarding geographic location of the departments , in northern , central and southern ( and isles ) italy work 41% , 34% and 23% of respondents , respectively , while 2% of italian radiation oncologist who completed the survey work abroad . 
seven percentage of respondents do not evaluate this subset of patients because they are not referred for rt evaluation . management andtreatment regarding selection criteria for treatment of prostate and / or metastatic sites , 26% of respondents would consider age and performance status , 19% biological features of the disease ( psa , gleason score , etc . ) , 28% the extent of the disease ( number and volume of the lesions ) , 13% technical feasibility and 76% all previous alternatives . 
physicians could choose more than one answer . in a fit asymptomatic patient affected with ompc , 9% of responders would offer rt to all secondary lesions , 1% to the prostate alone and 81% to both the prostate and all metastases , while 9% would not perform any rt , only adt . clinicians were asked which imaging technique they would consider mandatory before treating these patients : results are listed in table2 ( multiple answers were allowed )  . the sites the responders would most likely irradiate with non - palliative intent were : lymph nodes only , only bone metastases , both lymph nodal and bone lesions and none in 13% , 1% , 81% and 5% , respectively . 
regarding the number and site of lesions the responders would treat , results are summarized in table3 . a stereotactic body radiotherapy ( sbrt ) would be performed to both the prostate and metastases by 18% of clinicians ; 48% would offer sbrt to metastatic sites and standard or moderately hypofractionated schedule to the prostate ; 33% would choose a standard or moderately hypofractionated schedule for both ; no radiation treatment would be performed by 1% . the association of rt with adt was the topic of 13th question : 46 months of adt were chosen by 8% of respondents , 1236months of adt by 53% , continuous adt until biochemical progression by 24% ; 11% would not add any systemic treatment to rt ; 4% declared they do not deal with adt in their daily practice . the proposed follow - up scheme after treatment is shown in table4 ( multiple answers were allowed )  . 
numerous recent studies clearly show that metastatic pc is an extremely heterogeneous condition ranging from abinitio castration - naive low - volume disease to metachronous castration - resistant high - volume cancer . 
one hundred and eleven radiation oncologists filled in the questionnaire ; since we recommended to complete only one questionnaire per each centre , and 195 centres are active in italy , the response rate is higher than usually achieved when online surveys are conducted in our country . 
 we think actually that younger specialists may be probably more interested in this area of developing treatments . more than half of the respondents work , as expected , in a non - academic public facility ; over 30% work in an academic one , instead . 
it is possible that physicians working in an academic context are more likely to consider and perform innovative treatments , which also may require adequate technological equipment . not surprisingly , the percentage of the respondents according to geographic areas roughly follows the distribution of the radiation oncology centers in the country : 42% of the respondents come from the northern italy ( where 44% of the centres are located ) , 34% from the central italy ( 24% of the centres ) and 24% from southern italy ( 32% of the centres )  . almost two - thirds of the respondents work in a centre where regular mdt meetings are performed . 
it has been recently pointed out that the mdt meetings had an impact upon patient assessment and management practices in 445% of cases ; moreover , patients discussed at mdt meetings are more likely to receive more accurate and complete pre - operative staging and neo - adjuvant / adjuvant la radiologia medica ( 2019 ) 124 : 211217 treatments [ 8 ]  . 
another study showed that an uro - oncology mdt modifies management plans in about one quarter of cases , especially in metastatic patients , also improving cross - referral and consideration for clinical trials [ 9 ]  . 
the percentage of physicians who evaluate these patients for a non - palliative treatment appeared higher than expected : 27% see more than 20 of these patients in a year . 
the actual rate of abinitio oligometastatic patients is not clear , but with the development of new diagnostic tools , as whole - body mri and psma - pet / ct , the number is expected to increase . selection criteria for treatment were quite homogeneous , with 76% of respondents considering all listed criteria ( age and performance status , biological features of the disease , extent of the disease and technical feasibility ) useful in assessing the indication for a more aggressive treatment . 
 according to nccn guidelines , there are no specific criteria regarding age or comorbidities with regard to the indication to radical pc treatment ; however , life expectancy of at least 5years for high or regional risk patients is recommended . 
in elderly patients with a poor performance status , a palliative - only rt should be offered . the diagnostic topic is an interesting one , both in the initial / staging and in follow - up phase , as in case of progression ( re - staging )  . 
the standard work - up of staging for high - risk and locally advanced or metastatic pc includes abdominal ct or mri and bone scan , to assess distant disease . 
in recent years , since the widespread use of new systemic agents for upfront ( oligo ) metastatic patients and metastases - directed local treatments , the interest in a precise diagnosis of number and site of secondary lesions is growing . 
comparative reviews of whole - body ( wb ) mri and pet / ct have already demonstrated superior accuracy in metastasis detection in advanced - stage prostate cancer than ct and bone scans . 
 a recent study investigated the role of wb - mri to assess oligometastatic disease ( defined as 3 synchronous lesions ) , 1 3 la radiologia medica ( 2019 ) 124 : 211217 finding out that only about one fourth of the patients with hormone - naive prostate cancer had disease that could be classified as truly oligometastatic [ 13 ]  . 
the high sensitivity and specificity ( 80% and 97% , respectively ) of psma - pet / ct also may allow discriminating the true oligometastatic patients from those who have actually a widespread disease that has not been detected by ct or bone scan [ 14 ]  . 
over 90% of respondents would indeed perform a cholineor psma - pet / ct before evaluating a patient for aggressive treatment ; a local staging with mpmri would be recommended by 38% of respondents : this would be useful in locally advanced pc , as ct3 tumours , to avoid target missing in prostate rt . 
another relevant aspect is the appropriateness of employing such an expensive and time - consuming examination in a metastatic scenario , whereas other patients waiting for a radical treatment would probably benefit the most of it . it has been suggested that oligometastatic disease may represent an intermediate state of tumour spread with limited metastatic capacity , with a better prognosis compared to a more extensive metastatic disease [ 15 ]  . 
it would be crucial to identify patients whose disease is really less aggressive , so that the treatment of both primary and all metastatic would actually impact on local control , time to progression , castration resistance and even survival . 
it might be reasonable to consider as prognostic factors psa value , psa - doubling time , number of sites and pattern of metastatic spread , in order to select patients more suitable for an aggressive treatment , which can actually impact on patients outcome [ 16 ]  . 
the site , number and volume of secondary lesions also have to be considered carefully , since it would be complicated ( other than pointless ) to irradiate several or very large metastasis at a high , biologically effective dose , even with modern techniques [ 17 ]  . technical feasibility is a crucial issue . 
it does not mean that being able to do something implies that we should , but the irradiation of small isolated lymph nodes , for example , would be more complicated without advanced diagnostic tools ( as cholineor psma - pet / ct ) and high precision up to date rt equipment . 
if an extreme hypofractionated / stereotactic approach is considered for the treatment of the primary tumour , it should be performed in centres with adequate clinical experience and with the technological tools needed for both delivery and image guidance [ 18 ]  . over 80% of responders would irradiate both the prostate and all metastatic sites , if technically feasible and clinically indicated . 
the rationale of treating this subset of patients is indeed to achieve long - term local control , and therefore longer time to progression , so the irradiation of only a quote of disease would be probably insufficient . 
if there is growing evidence in treating metastatic sites in castration - sensitive pc , studies evaluating the role of prostate irradiation in this subset of patients are ongoing , and few retrospective experiences have been published [ 17 , 1922 ]  . 
nevertheless , 9% of the respondents would not perform any radiation treatment , but only adt as suggested by nccn guidelines [ 11 ]  . defining the oligometastatic state in prostate cancer is controversial and has varied across published and ongoing trials : most studies consider the limit up to 35 metastases [ 19 ]  . 
over twothirds of respondents would irradiate both the prostate and up to 23 secondary lesions : the treatment of the prostate and 45 metastases would be probably considered a technical challenge and clinically less indicated for most of the regarding the type of metastases to be irradiated , more than 80% of respondents would treat both nodal and bone lesions , if technically feasible . 
most studies have been performed delivering extreme hypofractionated treatments ( 1850gy in 110 fractions ) on secondary lesions , due to their excellent local control results as well as convenience [ 17 , 23 ]  . 
although the majority of respondents would offer a sbrt approach to metastatic sites , and only 18% also to the prostate , if technically feasible , about one third would perform a conventional or moderately hypofractionated treatment on both primary and secondary lesions [ 24 ]  . 
this can be understood in the case of nodal metastasis , or with bone lesions within the pelvic area , so that a single comprehensive treatment plan can be performed . 
it might be more difficult to justify a large number of fractions in a patient affected with more than one extra - pelvic lesion . the use of high doses delivered in a limited number of fractions , as we do with sbrt , is not only a convenient approach for the patient and the facility : due to its peculiar radiobiological features , characterized by a low / value , pc should be the ideal candidate for extreme hypofractionation [ 24 ]  . regarding systemic treatment , more than half of respondents would prescribe adt for 1236months , as current 1 3 216 la radiologia medica ( 2019 ) 124 : 211217 guidelines recommend for high - risk or locally advanced pc . 
even though metastases - directed sbrt in hormone sensitive ompc already treated with rt or surgery may be performed to delay the onset of adt ( and therefore its side effects ) , in this subset of abinitio oligometastatic patients the primary tumour is not controlled , and it is in fact a potential source for further metastatic spread . 
moreover , since long - term adt associated with rt is considered a standard approach in high - risk and locally advanced / node - positive pc , it should be mandatory in metastatic patients , who have been so far treated with continuous or intermittent adt alone [ 11 ]  . 
indeed , 24% of respondents suggested the use of adt until progression , which usually occurs within 2years from adt onset in this subset of patients . a small number of respondents ( 4% ) asserted that they do not deal with adt in their daily practice : radiation oncologists in italy are authorized to prescribe hormonal therapies , so the decision not to do it might be either a personal or a facility policy . cholineand psma - pet / ct also represent high sensitivity and specificity techniques for the detection of locoregional and distant metastases in pc patients with recurrence of disease [ 25 ] and have been proposed for re - staging for disease progression by 59% of respondents . 
although a standard follow - up scheme in this subset of patients has not been defined yet , it has been proposed to perform clinical examination , psa value and testosterone levels ( systematically or in case of psa rise ) every 36months by 92% of respondents . a number of prospective studies regarding the treatment of abinitio ompc are being developed , and the interest in this topic is growing ; 91% of respondents confirmed to be interested in participating in a multicentre study of non - palliative rt in this subset of patients . 
one of the aims of the uro - oncologic study group of airo is to elaborate shared guidelines and to promote multicentric trials regarding cutting - edge topics of our clinical practice . 
the development of a study protocol regarding the combination of adt and rt to the prostate and secondary lesions in abinitio ompc is indeed under investigation . strength points of our survey are represented by the relatively high response rate and by good heterogeneity for experience , geographic origin and centre type . 
many interesting sparks about assessment , management and treatment of abinitio ompc emerged , as outlined above . the major limitation of the survey is that , despite our request , about 20% of respondents declared not to be pc specialists : maybe a quote of them work in a facility where radiation oncologists are not divided into pathology - directed groups , so these colleagues are dealing also but not mainly with pc in their daily practice . 
in oncology , the role of wb - mri has expanded to the point of being recommended in international guidelines for the assessment of several cancer histotypes ( multiple myeloma , melanoma , prostate cancer ) and cancer - prone syndromes ( lifraumeni and hereditary paragangliomapheochromocytoma syndromes )  . 
the literature shows growing use of wb - mri for the staging and follow - up of other cancer histotypes and cancer - related syndromes ( including breast cancer , lymphoma , neurofibromatosis , and von hippellindau syndromes )  . 
the main aim of this review is to examine the current scientific evidence for the use of wb - mri in oncology . keywords magnetic resonance imaging diffusion - weighted imaging oncology whole - body mri cancer screening cancer - related syndromes * paul e . 
2 , university offlorence azienda ospedaliero - universitaria careggi , florence , italy 8 department ofradiology , ospedali riuniti , universit politecnica delle marche , ancona , italy introduction in 1905 , albert einstein published an article in annalen der physik describing the random motions of small particles suspended in a fluid that provided the first quantitative theory for the natural phenomenon widely known as the brownian motion . 
essentially , einsteins theory allows one to relate the diffusion constant to physical quantities , such as the mean squared displacement of a particle in a given interval of time [ 1 ]  . 
denis le bihan published the first article displaying diffusion - weighted magnetic resonance images of the central nervous system in 1985 [ 2 ] , some 80years after einsteins theory on water diffusion . 
since then , diffusion - weighted imaging ( dwi ) has evolved as a clinical magnetic resonance imaging ( mri ) technique ; it first entered practice in neuroradiology for the assessment of cerebral ischemia [ 3 ] and subsequently has extended into oncological applications [ 4 , 5 ]  . in 2004 , taro takahara started applying dwi in a single , whole - body ( wb ) examination , thus giving birth to the wbmri examination as we know it today : used mostly in oncological applications to provide a combination of morphologic vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 218233 and diffusion - weighted images from head to mid - thigh . 
taking steps to ensure good background body suppression of the signal , this first whole - body mri ( wb - mri ) with dwi examinations took almost an hour to acquire and required off - line image concatenation to produce an unified stack of slices for visualization [ 6 ]  . 
as highlighted in recent meta - analyses [ 7 , 8 ] , the growing evidence regarding the use of wb - mri in oncology has come to support recommendations of whole - body mri in international guidelines [ 911 ] and widening clinical adoption for different cancer histotypes [ 12 , 13 ]  . our aim is to review the current scientific evidence for the use of wb - mri in oncology . imaging acquisition protocol where f and w are , respectively , the fat and water images produced by the dixon technique . t2 - weighted images are acquired in the axial plane without fat suppression using turbo spin - echo ( tse ) sequences , with half - fourier acquisition single - shot turbo spin - echo ( haste ) being preferred . 
notably , some centers do not include t2 - weighted images in the wb - mri protocol in order to limit the acquisition time as similar information is provided by low b - value dwi images , but at a lower spatial resolution . t1 - weighted images and t2 - weighted images with fat suppression via short tau inversion recovery ( stir ) , acquired the spine in the sagittal plane , are usually warranted for investigation of suspected skeletal metastasis . the uptake of wb - mri as a radiological technique is closely tied to technical developments that have contributed to achieving a good spatial resolution with good signal - to - noise ratio throughout the body , including continuous moving - table acquisitions , multi - channel surface receiver coils , and parallel imaging acquisition . 
these developments have dramatically reduced the scanning time for wb - mri , such that dwi can now be performed along with supporting morphologic t1and t2 - weighted images of the whole body in a reasonably short acquisition time ( 3045min )  . the anatomical coverage of a wb - mri examination is usually from the skull base to mid - thigh analogous to positron emission tomography ( pet ) and computed tomography ( ct ) scans , though in specific clinical contexts it may be extended from vertex to feet . 
imaging is usually performed with a large field of view ( 4045cm ) [ 14 ]  . morphologic images due to their short acquisition times , t1 - weighted images of the chest and abdomen are usually performed within breath - holds as this prevents misinterpretation due to motion artifacts . 
gradient echo ( ge ) and dixon techniques are increasingly used for the t1 - weighted images due to their capability to derive multiple images ( including in - phase , opposite phase , water , and fat images ) in a single acquisition . 
intravenous contrast agent administration with subsequent post - contrast t1 image acquisition is performed only for specific clinical requests , such as the detection of brain metastases or characterization of liver masses . post - processing of the dixon images and specifically derivation of a fat fraction ( f% ) map that describes fat distribution are recommended [ 15 ]  . 
a fat fraction map can be computed on most of the mri post - processing consoles as : 100 f ( f + w ) diffusionweighted images dwi is usually performed using relatively thick sections ( from 5 to 7mm ) in an axial orientation during free breathing using a single - shot spin - echo planar imaging ( ssh - epi ) acquisition , to reduce both acquisition time and image distortion . 
fat suppression with the stir is strongly recommended in order to provide homogeneous fat signal suppression at larger fields of view . in the interest of limiting examination duration , two b - values are usually sufficient but three or more b - values are likely to more precisely quantify the apparent diffusion coefficient ( adc ) value , as requested for the tumor response assessment . 
the lowest b - value is usually in the range from 50 to 100s / mm2 to minimize perfusionrelated signal , while the highest is typically between 800 and 1000s / mm2 to allow good detection of hyper - cellular lesions with a good signal - to - noise ratio . 
depending on the mr scanner homogeneity and patient size , between four and six stacks of contiguous slices ( corresponding to different bed positions ) are usually necessary to perform wb - mri from skull base to mid - thigh . post - processing of the dwi data is mandatory and should consist of : unification of the high b - value images into a single series ( consecutive from superior to inferior ) , generation of maximum intensity projections ( mips ) of the unified high b - value series at small angular increments ( typically 3 ) rotating around the cranialcaudal axis , generation of coronal multi - planar reconstructions ( mprs ) of the unified high b - value series , if dedicated t2 - weighted images were not acquired , unify the low b - value images into a single series , unification of the adc maps into a single series ( consecutive from superior to inferior )  . 1 3 220 la radiologia medica ( 2019 ) 124 : 218233 mip reconstructions are usually displayed with an inverted gray scale , to provide a panoramic view similar to pet examinations . 
a complete image acquisition protocol is summarized in table1 , and a typical example of wb - mri imaging , including dwi , is displayed in fig.1. other possible wbmri protocols other wb - mri protocols for oncology have been used in the studies published over the last 15years . 
their differences can be described in terms of the following four concepts : anatomical coverage , imaging planes , mr sequences and reconstructions , and contrast administration . the anatomical coverage can be extended from the vertex to the feet ( including upper limbs ) when evaluating bone involvement in diseases that frequently involve the long bones , such as multiple myeloma ( mm ) [ 16 , 17 ] , when evaluating soft tissues in melanoma patients [ 18 , 19 ] , as well as for cancer screening in patients with lifraumeni syndrome [ 20 ]  . 
extending the anatomical coverage implies longer acquisition times . as regards imaging planes , many studies have made use of the coronal plane for morphologic whole - body images , alone or in combination with axial imaging [ 16 , 2129 ]  . 
in some cases , this choice may allow a better trade - off between scan time and image coverage , but is also a matter of scanner performance , radiologist preference , local practices , and considerations of readability , for example , the axial skeleton [ 30 ]  . 
the addition of dedicated single body part imaging is worth considering for specific assessment of brain , liver [ 31 , 32 ] , and chest [ 32 ]  . 
sagittal acquisition of the whole spine is included in the majority of wb - mri published protocols [ 2125 , 27 , 3134 ] , as it allows rapid acquisition and efficient evaluation of vertebral lesions , spinal cord compression , and vertebral fractures [ 26 ]  . the choice of the mr sequences and reconstructions used in wb - mri protocols has seen considerable evolution , and while not all include dwi [ 2125 , 32 ] , the majority of studies without dwi were published between 2002 and 2013 , when dwi of the whole body was quite time - consuming and quality inconsistent . 
mr technology developments in the last few years have significantly improved the quality and time efficiency of dwi in large volumes , allowing its wider and easier application in wb - mri protocols . 
similarly , the use of f% maps that we suggest in this review for bone assessment is a recent introduction to wb - mri and is only described in two studies published in 2017 , using wbmri for multiple myeloma [ 17 ] and breast cancer [ 34 , 35 ] patients . 
that earlier studies did not make use of f% maps is probably due to progressive acceleration of the dixon acquisition and prior lack of experience with this application in wb - mri . contrast administration is reported primarily in studies where wb - mri was used for patients with tumors requiring brain assessment , such as melanoma [ 18 , 31 ] and lung adenocarcinoma [ 27 ]  . 
 however , dwi has largely replaced the administration of contrast agents in many studies performed in patients with osteotropic tumor histotypes [ 26 , 3436 ] and lymphoma [ 29 , 37 ]  . clinical applications inoncology multiple myeloma multiple myeloma ( mm ) is a hematological disorder characterized by the accumulation of neoplastic plasma cells in the bone marrow . 
axial scans include multiple t1 - weighted images from a single dixon acquisition ( namely in - phase , out of phase , water , and fat images ) and t2weighted images performed without fat suppression . 
two different diffusion weightings ( with b - values of 50s / mm2 and 900s / mm2 , respectively , in this example ) are used to calculate the adc map ( third column )  . 
for this reason , the international myeloma working group ( imwg ) has affirmed that even the presence of asymptomatic bone disease on conventional radiography should be considered a criterion of symptomatic mm , requiring treatment [ 38 ]  . 
involving 611 mm patients , wb - mri detected more focal lesions than conventional whole - body x - rays in three of the most common metastatic sites for mm , including spine ( 78% versus 16% ; p value 0.001 ) , pelvis ( 64% versus 28% ; p value 0.001 ) , and sternum ( 24% versus 3% ; p value 0.001 ) [ 39 ]  . 
similar results were observed in a prospective cohort study conducted by baurmelnyk on 41 newly diagnosed mm patients , in which wb - mri showed diagnostic performance superior to conventional wholebody computed tomography ( ct ) in the detection of skeletal lesions ( ct understaged 11 / 41 patients compared to mri , p < 0.001 ) [ 40 ]  . 
finally , wb - mri is also recommended for the staging of solitary bone plasmacytoma ( sbp ) , an early - stage malignancy with a clinical course between monoclonal gammopathy of undetermined significance ( mgus ) and mm [ 38 ]  . melanoma although newly discovered immunological treatments for advanced melanoma have significantly increased overall survival , most patients with stage iiiiv melanoma will still die of the disease [ 42 ]  . 
in a later study involving 71 scans , wb - mri with dwi but without contrast - enhanced scans and wb - dwi without dwi but with contrast agent were seen to have an equivalent diagnostic performance in the detection of extracranial metastases from advanced melanoma [ 31 ]  . 
moreover , wb - mri is recommended for the follow - up of melanoma patients staged from iic to iv [ 9 , 44 ]  . prostate cancer mortality rates for prostate cancer are low , despite it being the most common cancer among males in europe [ 45 ]  . 
furthermore , prostate - specific membrane antigen ( psma ) pet / ct scans may fail to provide information on tumor viability during androgen receptor inhibition [ 48 ]  . 
2 contrast - enhanced ( gadolinium - ethoxybenzyl - diethylenetriamine pentaacetic acid , gd - eob - dtpa ) wb - mri with dwi performed on a patient with a stage iii melanoma . 
the same lesion is clearly detectable in the high b - value ( 900s / mm2 ) diffusion - weighted image performed in the same session ( b ) cancer ( eortc ) considers wb - mri as a one - size - fitall solution for evaluating treatment efficacy in advanced prostate cancer patients [ 50 ]  . the advanced prostate cancer consensus conference ( apccc ) has confirmed that psa alone is not reliable for monitoring disease activity in mcrpc , suggesting the use of a robust imaging technique before deciding to start a new line of treatment . 
in this respect , their guidelines recognize the superior diagnostic performance of wb - mri relative to ct and bs in the detection and assessment of skeletal metastasis [ 51 ] , though they note limited availability of the wb - mri technique . lymphoma fluorodeoxyglucose ( fdg ) - pet / ct is the imaging technique recommended for the most common lymphomas , fig . 
consistent with this , the national comprehensive cancer network ( nccn ) recommends serial ct or pet / ct examinations for both the staging and follow - up of lymphoma patients [ 53 ]  . 
the sensitivity of wb - mri with dwi to hyper - cellular lesions , independent of glucose metabolism , allows a reliable radiological evaluation of these lymphoma subtypes [ 54 ]  . in a prospective study conducted by mayerhoefer etal . 
 [ 13 ] on 140 patients , wb - mri with dwi demonstrated better sensitivity ( 94.4% ) than fdg - pet / ct ( 60.9% ) and contrast - enhanced ct ( 70.7% ) in staging patients with lymphoma subtypes of variable fdg avidity . 
 ( the majority were malt lymphomas . ) further , the same group found wbmri with dwi to have a diagnostic performance similar to fdg - pet / ct and ct in fdg - avid lymphomas [ 55 ]  . a growing application of wb - mri in lymphoma involves young patients irrespective of histotype . 
in a 1 3 224 la radiologia medica ( 2019 ) 124 : 218233 breast cancer in the last two decades , conservative treatments and early detection have substantially improved the prognosis for patients with low - stage breast cancer ( bc ) [ 66 ]  . 
nevertheless , according to the american cancer society , 5 - year overall survival for patients with advanced ( stage iv ) bc remains unfavorably low at just 22% [ 67 ]  . 
notably , bone metastases were present at the first staging procedure in 49.7% of invasive ductal cancer ( idc ) and in 61.7% of invasive lobular cancer ( ilc ) subtypes , respectively [ 68 ]  . 
 the widely accepted response evaluation criteria in solid tumors ( recist ) are not suited to a proper assessment of bone metastases and in fact consider them to not be measurable . 
according to the new criteria , bone metastases are considered measurable only once they have spread to the surrounding soft tissue with an extent larger than 10mm in diameter , which rarely occurs in clinical practice [ 69 ]  . 
this situation points to a significant unmet clinical need for means to evaluate bony metastases , with implications beyond breast cancer . in a 2011 meta - analysis by yang etal . 
 [ 70 ] covering 145 studies with 15 , 221 metastatic cancer patients , wb - mri showed diagnostic performance comparable to pet and superior to ct and bs in the detection of skeletal metastases ( table3 )  . 
 observed that out of the 46 treatment changes made due to progressive disease ( pd ) detected at imaging , in 34.7% of the cases ( 16 paired examinations ) , pd was visible only on wb - mri and not on the ct - cap examinations [ 12 ]  . 
similarly among 40 cases of progressive disease findings in a group of 58 patients who had both wb - mri and ct - cap or an 18f - fdg - pet / ct within 8weeks , zugni etal . 
 [ 71 ] found that all 40 ( 100% ) have been identified on wb - mri but only 23 ( 58% ) were also identified by ct - cap or 18f - fdg - pet / wb - mri has also shown promising diagnostic performance and established itself as a safe and accurate diagnostic imaging method for the systemic staging of pregnant bc patients ; some 40% of whom receive a diagnosis when bc is already at an advanced stage [ 72 ]  . 
4 a patient admitted with an initial diagnosis of prostate adenocarcinoma ( gs 5 + 4 , biopsy positive in 8 / 8 cores ) , psa = 29 ng / ml , positive digital rectal examination ( ct2c )  . 
the systemic staging , previously assessed with contrast - enhanced ct examinations of chest , abdomen , and pelvis ( ct - cap ) and bs , was negative for metastatic disease . 
subsequent systemic staging with wb - mri with dwi showed two metastases , one in the anterior arch of a left rib ( arrow ) and the other at level of retroperitoneal lymph node ( arrowhead )  . 
a multiparametric mri examination performed in the same session showed a pi - rads five lesion ( dashed line ) , visible on t2 - weighted axial images , high b - value diffusion - weighted images , and adc map recent study by brenner etal . , the overall 10 - year survival for lymphoma patients younger than 35years of age was seen to be above 90% ( 94.7% for patients < 24years and 89.4% for patients comprised between 25 and 35years , respectively ) [ 56 ]  . 
despite this long survival , the nccn guidelines still recommend pet / ct or ct for the staging and follow - up of lymphoma patients [ 57 ] , with 69 examinations to be performed in the first two years after diagnosis . 
after multiple lines of systemic treatments fdg - pet / ct and wb - mri were performed before and 6 months after initiating chemotherapy under the eshap scheme and peripheral blood stem cell transplantation . 
it has been reported that patients who have symptoms at onset have a poorer prognosis , and this is mainly related to the fact that vision reestablishment starts earlier compared with patients with mild symptoms , but restoration of visual function is still possible [ 6 , 7 ]  . 
corticosteroid treatment hastens recovery following on , but this does not improve final visual function . magnetic resonance imaging ( mri ) may help on diagnosis as it allows detecting optic nerve inflammation , to rule out differential diagnoses , and to predict the risk for developing ms [ 1 , 4 ]  . the application of mri in the assessment of optic nerve damage in a single episode of acute on has been rarely performed [ 4 ] , and its role in predicting the prognosis of visual impairment and visual outcome after on is not clear [ 4 , 610 ]  . optical coherence tomography ( oct ) is a noninvasive imaging technique used in ophthalmology to visualize the layers of the retina . 
it allows the depiction of unmyelinated central nervous system axons within the retina , the so - called retinal nerve fiber layer ( rnfl ) , and provides a measurement of its thickness ( micron - scale )  . 
the rnfl thickness is used as a noninvasive biomarker of neurodegeneration and axonal loss in ms [ 11 , 12 ]  . our aim was to assess brain and orbital mri findings of patients with a first attack of acute on , and their correlation with visual acuity at presentation , visual recovery , ms development and a possible correlation between orbits mri pattern and rnfl on oct . patients we retrospectively revised the ophthalmological , neurological and imaging data of patients who were admitted to our emergency department ( ed ) with the first episode of acute on from january 2015 to january 2017 ( n = 85 )  . the exclusion criteria were : patients aged < 18years ; previous episodes of on ; history of ms or optic neuromyelitis ( nmo ) ; patients affected by known ophthalmological diseases ; patients affected by immunological / infective disorders ; patients with previous neurological events ; patients with family history of leber hereditary optic neuropathy ; lack of complete ophthalmological , neurological , imaging data ; time between symptoms onset and presentation > 14days ; time between ed arrival and mri execution > 14days ; mri executed in other institutions ; lack of follow - up data ; clinical follow - up < 1year . we therefore included in our study 37 patients ( age range 2157years ; mean age 33years ) , 26 females and 11 males . 
twenty had right on , 13 had on in the left eye , and 4 had bilateral on , for a total of 41 affected eyes . after the arrival , each patient underwent a complete ophthalmological examination , including fundoscopic examination , visual acuity assessment , visual field and oct , brain and orbits unenhanced computed tomography , according to the protocol of our emergency department , to exclude intracranial and orbital abnormalities , blood tests to exclude infective / autoimmune causes of on and to test aqp4 antibodies myelin oligodendrocyte glycoprotein ( mog ) igg and cerebrospinal fluid ( csf ) collection for detection of the oligoclonal bands , as previously described [ 13 ]  . following the neuro - ophthalmological confirmation of the diagnosis of on , steroid therapy was administered intravenously within 24h from the patient access ( methylprednisolone 1g / day for 5days , followed by a low - dose steroid oral regimen for 15days )  . methods andmaterials this retrospective study has been approved by our institutional review board ( institutional review board area 1 milan ; reference number : 2018 / st / 116 )  . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments . 
the number of brain and spinal cord lesions was recorded . optic nerves mris were reported as ( 1 ) normal , ( 2 ) stiralteration without contrast enhancement ( ce ) , ( 3 ) stir signal abnormalities + ce . 
optic nerves pathologic findings were localized into three sites [ intra - orbital ( io ) , canalicular ( ca ) and chiasmal ( ch ) ] , and the length of altered signal or ce was measured in cm . visual acuity visual acuity was measured at patients arrival , according to snellen chart ( decimal )  . 
light perception and motus manus ( mm ) were assigned a decimal visual acuity of 0 . the degree of visual acuity was further divided into three groups : severe deficit ( mm4 / 10 ) , intermediate deficit ( 57 / 10 ) , slight deficit ( 8 / 10 , 9 / 10 )  . 
each patient was followed - up for at least 12months ( mean follow time : 16 4months )  . oct test was acquired using the same machine ( spectralis version 6.3.2 , eye explorer software 1.6.1.0 , heidelberg engineering , heidelberg , germany ) , after mydriasis induced with 1% tropicamide . oct produces a cross - sectional image of the peripapillary retina which is color - coded and shows the temporal , superior , nasal , inferior and temporal sections on the same image . the software automatically recognizes the retinal nerve fiber layer ( rnfl ) layer , measures the rnfl thickness along the scan and reports the results on a graphic display showing the rnfl thickness ( in m )  . 
pearson chi - square test for categorical variables was used to assess the correlation between brain mri patterns and visual acuity , visual outcome and diagnosis , and between orbits mri patterns and visual acuity , visual outcome and diagnosis . 
logistic regression model was applied to variables with p < 0.05. we then performed mannwhitney u test to assess the correlation between the lesions number and the diagnosis , applied the logistic regression model and finally performed roc curve analysis , and to evaluate the correlation between orbital mri pattern and extension of the altered signal of the optic nerve . kruskalwallis test was performed to assess possible correlation between orbits mri pattern and rnfl thickness at oct . results brain mris were classified as follows : ( 1 ) normal in 9 patients out of 37 patients ; ( 2 ) millimetric hyperintensities in t2 and flair with location and morphology not typical for demyelinating lesions in 9 out of 37 patients ; ( 3 ) lesions with ms - like shape , localized in typical ms sites with dissemination in space without contrast enhancement in 13 out of 37 patients and ( 4 ) lesions with ms - like shape , localized in typical ms sites with dissemination in space and coexistence of gadolinium - enhancing and non - enhancing lesions in 6 out of 37 patients . ms - like shape lesions number range was : 025 , with a mean number of 8 2 . ophthalmological evaluation including visual acuity assessment was executed at 6months to establish the visual outcome . 
optic nerves pathologic findings were localized into the io segment in 9 out of 27 eyes with signal abnormalities ( 33.3% ) ; into the ca segment in 16 out of 27 eyes ( 59.2% ) ; io + ca in 2 out of 27 eyes ( 7.4% ) , whereas no localization was observed in the ch segment . 
mean visual acuity at follow - up was 7 1 / 10 . twenty - five patients ( 67.5% ) received a diagnosis of ms ; 12 patients ( 32.4% ) received a diagnosis of cis ; in our group no patients received a diagnosis of nmo . 
3 roc curve shows the correlation between the lesions number and the diagnosis of ms 1 3 la radiologia medica ( 2019 ) 124 : 12961303 1301 discussion different disorders determine the inflammation of the optic nerve , but the form caused by ms related demyelination is the most common [ 2 ]  . 
demyelinating on represents the first manifestation of ms in about 20% of patients [ 19 ] and a diagnosis that brings great concerns to patients who are often young and previously healthy . the execution of mri , soon after the onset of symptoms , has important implications : first , mri helps clinicians to confirm the diagnosis of on , but it can also provide with useful information for patient management and treatment planning . in our case series , most optic nerve lesions were in the intra - orbital segment , and this is in line with the evidence of another study by soelberg etal . 
in a study on 37 adult patients with a recent or past attack of on who executed obits mri with stir sequence [ 20 ] , highsignal abnormalities of the optic nerves were found in 84% of symptomatic subjects and poor visual outcome was observed in patients with more extensive lesions , or with lesions located in the optic canal . 
our study shows that visual evoked potentials were more sensitive than mri in detecting lesions and in diagnosing demyelinating disease of the optic nerve ; however , we must consider that this study was conducted in 1998 and the mr equipment was certainly less efficient than the currently available scanners . stir sequence showed abnormalities in 88% of acute on in another retrospective study [ 21 ]  . we observed a lower rate of optic nerves altered signal ; however , differences in rates of mri abnormalities detected at optic nerves can be explained by different timings of mri execution after symptoms onset and by the beginning of the steroid treatment in our patients : berg etal . , for example , performed the mri within 24h form the patients arrival , before the corticosteroid therapy . in accordance with the literature , in our group of patients , all optic nerve abnormalities were in the io or ca segment without any involvement of the ch portion , which is instead considered typical for neuromyelitis optica spectrum disorder [ 22 , 23 ]  . in our study , we did not demonstrate a significant correlation between orbits mri pattern and visual outcome at follow - up . in a prospective study by hickman et al . 
 [ 6 ] in 33 patients , 15 of whom performed serial gadoliniumenhanced orbits mri until enhancement ceased , short acute lesion on triple - dose gadolinium - enhanced imaging are associated with initial improvement in vision ( p < 0.01 ) , but recovery was not related to the duration of enhancement . 
 [ 24 ] analyzed a group of 107 patients and observed that optic nerves with gadolinium enhancement in the optic canal had poorer color vision , compared with optic nerves with abnormalities in other segments . 
 they also report that that when there was complete involvement of all segments of the nerves the threshold perimetry and color vision were mostly impaired , and that optic nerves with enhancing segments longer than 17mm had poorer baseline visual acuity , threshold perimetry and color vision . 
 however , visual recovery was similar regardless of location or length of abnormal enhancement at baseline , and this fact is in line with our results . the extension of optic nerve abnormalities has been proposed as predictor of visual outcome in a study on 22 patients [ 25 ] , where complete visual recovery was observed in patients with lesions extension less than 17.5 mm , whereas lesions greater than 17.5mm and / or lesions with intracanalicular location were associated with incomplete or partial recovery . the intracanalicular location was identified as a risk factor for poor outcome also in a retrospective study of 50 patients acute on , who executed mri including stir sequence of the optic nerve [ 21 ] , together with initial low visual acuity ( less than 2 / 10 ) and the absence of orbital pain . in the attempt to predict visual recovery after on , zhang etal . 
 [ 26 ] proposed the use of texture analysis in a study on 25 patients with acute optic neuritis : open source software imagej was applied for the assessment of texture heterogeneity calculated on the coronal stir image showing the largest cross - sectional area of the lesion in the optic nerve . 
they observed that only baseline lesion texture independently correlated with visual recovery at 6 and 12months , whereas no other mri variables at baseline , as altered signal length and gadolinium enhancement length , nor ophthalmic variables , as rnfl , correlated with visual outcome . 
the absence of a correlation between signal abnormalities in stir and gadolinium enhancement of the optic nerves and visual recovery is in line with our results . we confirmed that mri brain lesions at presentation with optic neuritis ( on ) increase the risk of developing clinically definite multiple sclerosis . 
the evidence that the presence of brain lesions at the onset of on is related to the diagnosis of ms is in accordance with the literature : previous studies have reported that patients with no brain lesions at the onset of on have a 1522% risk of ms compared to a 5688% risk 1 3 1302 la radiologia medica ( 2019 ) 124 : 12961303 in patients with one or more brain lesions [ 14 , 27 , 28 ]  . 
this evidence has important clinical implications , since these patients may be later at a greater risk of disability [ 4 ]  . all patients with spinal lesions received a diagnosis of ms , and this agrees with other studies [ 4 , 29 ]  . another option for the assessment of patients affected by on is represented by oct . 
data in the literature demonstrated the relationships between rnfl thickness and visual acuity , visual field and color vision , and previous results affirmed that oct can be used as a noninvasive biomarker of neurodegeneration and axonal loss in ms [ 30 ] and of optic nerve atrophy [ 31 , 32 ]  . 
moreover , a strong correlation between rnfl thickness and visual outcome has been observed in ms patients [ 3335 ] , suggesting that a lower rnfl thinning in early ms is related to a better visual outcome [ 33 ] .we use this ophthalmological technique in combination with mri examination . limitations our study has some limitations , first of all the 1 - year clinical follow - up : it is indeed possible for the patient to develop ms at a greater distance of time ; however , the same followup period was also considered in other studies in patients with on [ 4 , 8 , 20 , 24 ]  . 
this is a retrospective study ; however , we considered only the patients with complete clinical , ophthalmological and imaging documentation , eliminating from our case series all patients with partial or incomplete data ; the patient population is not huge , but comparable to that proposed in other similar studies . 
another limitation is the execution of mri after the beginning of the steroid treatment , since the administration of steroids reduces active lesions contrast enhancement of the optic nerves , brain and spinal cord . conclusions in conclusion , the correlation between orbits mri pattern at baseline and visual recovery remains unclear , whereas the observation of brain lesions and their number at the first episode of on can help predict the development of ms . 
the identification of those patients who may convert to ms is important , as they may later be at greater risk of disability [ 30 ]  . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards as stated in materials and methods , this retrospective study has been approved by our institutional review board ( institutional review board area 1 milan ; reference number : 2018 / st / 116 )  . 
therefore , we want to evaluate the diagnostic performance of preoperative mri with a dedicated axillary sequence for axillary lymph node ( aln ) metastasis in patients with early ductal breast cancer and determine potential predictors of axillary nodal positivity . materials and methods we retrospectively reviewed the mri findings for 74 consecutive patients diagnosed with invasive breast cancer . 
peritumoral high signal intensity on t2 - weighted images ( p = 0.015 ) of the primary tumor was significantly associated with aln metastasis . conclusion our findings suggest that preoperative axial + reconstructed coronal mr images exhibit good diagnostic performance for aln metastasis in patients with early ductal breast cancer . 
in addition , peritumoral high signal intensity on t2 - weighted images of the primary tumor can be used as a predictor of aln metastasis in these patients . keywords axilla breast cancer lymph node magnetic resonance imaging metastasis introduction axillary staging of primary breast cancer is important to determine the treatment and prognosis [ 1 ]  . 
axillary lymph node ( aln ) dissection ( alnd ) used to be a conventional * mijung jang mjjang74@gmail.com 1 department ofradiology , chung - ang university hospital , chung - ang university college ofmedicine , 102 heukseok - ro , dongjak - gu , seoul06973 , republicofkorea 2 department ofradiology , seoul national university bundang hospital , gumi - ro , bundang - gu , seongnam - si , gyeonggi - do13620 , republicofkorea 3 department ofradiology , chungbuk national university hospital , 776 1sunhwan - ro , seowon - gu , cheongju , cungcheongbuk28644 , republicofkorea staging method ; however , the performance of this invasive procedure may result in overtreatment for patients without lymph node metastasis . 
therefore , alnd has largely been replaced by sentinel lymph node biopsy ( slnb ) for surgical axillary staging , and alnd is performed for patients with positive slnb findings in recent use [ 2 , 3 ]  . ultrasound ( us ) is considered the best imaging tool for breast cancer diagnosis , which can have high sensitivity and high specificity for axillary nodal staging [ 4 ]  . 
in addition , us - guided fine needle aspiration biopsy ( fnab ) exhibited high specificity and a high positive predictive value ( ppv ) for axillary staging in previous studies [ 46 ]  . 
however , following the reporting of the acosog z0011 trial findings [ 7 ] , the usefulness of us - guided fnab for aln staging in patients with breast cancer is needed to be revisited [ 8 , 9 ]  . 
the results of the acosog z0011 trial suggested that only patients with extensive nodal involvement ( more than vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 12201228 1221 three axillary nodes ) should undergo alnd in the setting of early breast cancer . 
considering that the identification of metastases on us images commits patients to alnd , the use of us and us - guided fnab , particularly for patients with early breast cancer and relatively few axillary nodal metastases , was challenged after publication of the acosog z0011 trial findings [ 11 ]  . 
these changes have spurred a reappraisal of the role of many other noninvasive imaging modalities for aln staging . magnetic resonance imaging ( mri ) is widely used for the preoperative evaluation of breast cancer . 
staging of aln metastasis using mri is generally based on the size and additional morphological characteristics such as irregular margins , an inhomogeneous cortex , perifocal edema , and asymmetry [ 12 ]  . 
many advanced techniques such as ultrasound particles of iron oxide ( uspio ) - enhanced t2 * imaging , diffusion - weighted imaging ( dwi ) , and dedicated high - spatial resolution axillary mri have been attempted to improve the accuracy of aln metastasis detection [ 13 , 14 ]  . 
 however , these techniques are very difficult to use in clinical practice , considering they are time - consuming because of the addition of experimental sequences or a dedicated axillary coil . 
 [ 14 ] demonstrated that the sensitivity and specificity of any advanced mri techniques were not better than those of snlb for the detection of aln metastasis in patients with early breast cancer . 
therefore , the aims of the present study were to evaluate the diagnostic performance of preoperative mri using a dedicated axillary sequence on a 3 - tesla magnet with the addition of coronal multiplanar reconstruction images for aln metastasis in patients with early ductal breast cancer . 
in addition , we also determined the clinicopathological and imaging factors predicting axillary nodal positivity in early ductal breast cancer patients . materials andmethods study population this study was a retrospective review of the medical records of patients with early breast cancer diagnosed and treated at our institution between october 2015 and december 2015 . 
 the protocol of this observational study was approved by the institutional review board of our hospital , a tertiary referral center , which waived the requirements for informed written consent for use of these data ( irb no . : b - 1907 - 550 - 109 )  . 
of these , 103 were excluded for the following reasons : no invasive component on final pathology [ ductal carcinoma insitu only ( n = 36 ) ] , advanced disease requiring preoperative systemic therapy ( n = 27 ) , bilateral cancer ( n = 14 ) , other breast cancers such as invasive lobular carcinoma ( n = 11 ) , unavailable mri data or mri performed elsewhere ( n = 8 ) , unknown primary tumor with axillary metastasis ( n = 3 ) , performance of excisional biopsy instead of breast conserving surgery ( n = 3 ) , and recurrent breast cancer ( n = 1 )  . 
finally , a total of 74 consecutive patients were included in this study . mri protocol mri was performed using a 3.0 - tesla ( t ) mri device ( achieva , philips healthcare , best , the netherlands ) with a 16 - channel dedicated breast surface coil . 
coronal reconstruction was performed on the basis of the axial images using a commercial computeraided diagnosis ( cad ) workstation ( cadstream version 4.1.3 ; confirma , inc , kirkland , wa )  . 
the cad system was configured to compare the pixel intensity values of the precontrast and immediate post - contrast image series using a 50% enhancement threshold . axillary mr image analysis two radiologists with experience in breast mr image interpretation retrospectively reviewed the mri images , respectively . 
the reviewers were informed 1 3 1222 la radiologia medica ( 2019 ) 124 : 12201228 about the primary cancer site only for the purpose of comparisons with the contralateral axilla as a control . 
clinical aln positivity was recorded when one or more positive findings were noted by both reviewers on axial or axial + coronal mr images . positive mri findings indicating lymph node metastasis included the following : a short - axis diameter of > 0.5cm , a maximal cortical thickness of > 0.3cm , eccentric cortical thickening , and loss or compression of the fatty hilu both axillae were evaluated at the same time , and the aln ipsilateral to the breast cancer was compared with the contralateral node . 
if there were no differences in number , size , or shape between the ipsilateral and contralateral alns , we recorded nodal negativity in accordance with the concept of asymmetry described by baltzer etal . 
we additionally included a cn0 stage , which represented negative mri findings , in the present study . breast mr image analysis breast mr images were evaluated for the primary tumor morphology and size and the presence of peritumoral edema by one of three radiologists with experience in breast mr image interpretation . 
the lesion morphology was evaluated as mass or non - mass enhancement ( nme ) , and peritumoral edema was evaluated on t2 - weighted image as absent or present . 
the maximal diameter of the tumor was recorded as the radiological tumor size . reference standard ( pathological nodal stages ) andstatistical analysis the final histopathological findings in either alnd or slnb specimens were used as the reference standard . 
in cases of n0 ( i + ) , i.e. , when very small deposits of isolated tumor cells were found in a lymph node ( less than 0.2mm or 200 cells ) , the nodal stage was still designated as n0 . 
in other words , the n0 ( i + ) stage represented negative findings in the present study . the clinical nodal status was correlated with the corresponding pathological nodal status , and the diagnostic performance of mri for aln metastasis was assessed on the basis of these correlations . 
in addition , these values , along with the area under the receiver operating characteristic curve ( auc ) value , were calculated for axial and axial + coronal images and compared . 
the patient and primary tumor characteristics , including age ; family history ; clinical symptoms ; the primary tumor size ( pathological ) , multiplicity , and molecular subtype ; and the mri findings for the primary tumor ( morphology , size , and presence of peritumoral edema ) , were correlated with the pathologic nodal stage . 
the primary malignancies included invasive ductal carcinoma in 71 patients , microinvasive ductal carcinoma in two patients , and mixed invasive ductal and lobular carcinoma in one patient . diagnostic performance ofmri according to axial scan analysis , there were 50 patients with negative findings and 24 patients with positive findings . 
final pathological analysis revealed positive findings for eight ( 33.3% ) of the 24 patients with positive mri findings ; the remaining 16 ( 66.7% ) patients showed negative pathological findings . 
with regard to the 50 patients showing negative mri findings , final pathological analysis confirmed negative findings for 41 ( 82% ) and positive findings for nine ( 18% ; table1 )  . 
six ( 40% ) of the 15 patients with positive mri findings showed positive findings in the final pathological analysis ; the remaining nine ( 60% ) showed negative findings . 
1 receiver operating characteristic curve ( roc ) to assess the diagnostic performance of axial alone and axial + reconstructed coronal magnetic resonance images for axillary lymph node metastasis in patients with early ductal breast cancer correlation ofclinicopathological andmri findings fortheprimary tumor withthepresence ofaln metastasis table3 shows the clinicopathological and mri findings for the primary breast lesions in the aln positive and negative groups . 
the tumor stage was significantly higher ( p < 0.001 ) , and the pathological tumor size was significantly greater ( p = 0.008 ) in the positive group than in the negative group . 
the dedicated axillary sequence used in this study can eliminate pulsation artifact due to use of phase encoding direction and can be easily added the routine dce - mri protocol because it uses the same breast coil for the primary breast cancer instead of a separate coil for the axilla . 
3 preoperative breast magnetic resonance images of a 43 - yearold woman who underwent total mastectomy for left breast cancer a contrast - enhanced axial t1 - weighted image shows a proven malignant mass in the outer quadrant of the left breast . 
these findings suggest that postprocessing using cad software can improve the diagnostic performance of axillary mri for aln metastasis without the need for supplemental advanced sequences such as uspio - enhanced t2 * sequences , dwi , and dedicated high - spatial resolution axillary sequences . 
we also compared various clinicopathological and mri features of the primary tumor between the node - positive and node - negative groups and found that venous / lymphatic invasion , the pathological stage , and the pathological size , which are widely known prognostic factors for breast cancer , showed significant differences between the two groups . 
the presence of peritumoral 1 3 1226 la radiologia medica ( 2019 ) 124 : 12201228 edema on t2 - weighted images was also associated with aln metastasis . in a recent article evaluating the practical approach to breast mr image interpretation and reporting , the authors described that the use of image postprocessing , such as subtraction , maximum intensity projections ( mips ) , threedimensional reconstruction , region of interest analysis , and automatic color mapping using cad software , should also be included in the breast mri report [ 16 ]  . 
although image postprocessing is widely used in practice , to the best of our knowledge , this is the first study comparing axial images with axial + reconstructed coronal images for axillary staging . 
the authors obtained two additional sequences , including a t2 - weighted haste and a t1 - weighted , contrast - enhanced , fat - saturated sequence with coronal orientation and demonstrated a clinically feasible fast protocol for local and locoregional staging of breast cancer . 
 [ 14 ] demonstrated that uspioenhanced t2 * sequences showed superior sensitivity ( 98% ) and inferior specificity ( 96% ) for aln metastasis in patients with early breast cancer . 
therefore , this technique could be a useful addition to current diagnostic techniques , although it cannot compete with slnb , which exhibits high sensitivity ( 9395% ) and specificity ( 100% ) [ 17 , 18 ]  . 
 while the difference in the diagnostic performance between our study and previous studies is not remarkable , our result is significant with regard to clinical practice , because reconstructed coronal images were obtained by postprocessing after routine mri . 
that is , the diagnostic performance for axillary staging in early breast cancer was significantly improved without additional experimental mri sequences or a dedicated axillary coil . the aln disease status is the most significant prognostic factor for patients with early - stage breast cancer . 
in the present study , venous / lymphatic invasion by the primary tumor cells and the pathological stage and size of the primary tumor were found to be potential predictors of aln metastasis . 
on the basis of these findings , we can assume that venous / lymphatic invasion by the primary tumor and the pathological stage and size of the primary tumor is associated with peritumoral edema on t2 - weighted images . 
in particular , peritumoral edema on t2 - weighted images or rim enhancement of the primary breast lesion on dynamic contrast - enhanced images was significantly correlated with the disease prognosis . 
 [ 28 ] reported that preoperative breast mri findings of rim enhancement and peritumoral edema may be used as prognostic biomarkers for predicting distant metastasis in patients with breast cancer . 
although multivariate analysis for the association between peritumoral edema and other possible correlated factors such as molecular subtypes ( luminal a / b , human epidermal growth factor - positive , and triple - negative ) was not performed because of the small total sample size , peritumoral edema by itself was confirmed to be a significant predictor of aln metastasis in our study . our study was limited by the small sample size and selection bias due to the retrospective design . 
to minimize discordant results , the sizes of the 1 3 la radiologia medica ( 2019 ) 124 : 12201228 1227 most suspicious alns on mri were correlated with those of pathologically proven metastatic lymph nodes ; however , we could not confidently confirm any correlation . 
third , we used reconstructed coronal images created by postprocessing techniques , but this protocol may be unsuitable for screening postoperative patients because of the possibility of metal artifacts . in conclusion , preoperative breast mri showed a relatively high specificity value and npv for the detection of aln metastasis in patients with early ductal breast cancer . 
ishmael pastore roberta perri marco pesapane filippo petralia giuseppe petrillo antonella petrillo mario piacentino filippo pintari robert pinto antonio pinto fabio pinzi valentina pirtoli luigi pofi enrico pozzi mucelli fabio pradella silvia quaia emilio la radiologia medica ( 2019 ) 124 : 13331335 quattrocchi carlo cosimo rampado osvaldo regge daniele renzulli padiglione 2 radiologia golfieri righini andrea romanini laura romano andrea rosi giovanni rossi andrea rossi michele saba luca sabatini umberto ahin ertan salerno sergio salvolini ugo samarakoon rushani sartori paolo scevola germano sconfienza luca maria secinaro aurelio seitun sara sessa barbara shikhare sumer sibilla luisella somma francesco spampinato sofia sperandeo marco splendiani alessandra stabile ianora amato antonio stasolla alessandro stecco alessandro stramare roberto sverzellati nicola tagliafico alberto tartaglione tommaso tedeschi enrico teke memik tofani alessandro toma paolo tonerini michele tonolini massimo torricelli pietro tortora fabio triulzi fabio trovato guglielmo turgut bekir ugga lorenzo ukmar maja 1 3 la radiologia medica ( 2019 ) 124 : 13331335 1335 valeri gianluca valeriani maurizio vanzulli angelo varrassi marco verrone giovanni volterrani luca woniak krzysztof xiaoyun su zappia marcello zeng jing zuiani chiara zampa virna zanirato rambaldi giuseppe a . 
the role of whole - body computed tomography ( wb - ct ) in self - referred and asymptomatic patients has been debated . aim to determine frequency and spectrum of wb - ct findings in average - risk subjects derived from a medical - check - upunit , to evaluate recommendations reported and distribution according to sex and age - groups . materials and methods we retrospectively reviewed 6516 subjects who underwent wb - ct ( june 2004 / february 2015 )  . 
de tarazona , k3 , 31500tudela , navarra , spain 4 present address : complejo hospitalario de navarra , calle de irunlarrea 3 , 31008pamplona , navarra , spain vol . : ( 0123456789 ) 1 3 1200 introduction since the development of the first x - ray scanner in 1971 , computed tomography ( ct ) has emerged as a potential tool for diagnosis in symptomatic patients [ 1 ]  . 
in the recent years , the role of this technique has also been advocated to allow early detection of certain diseases in specific asymptomatic individuals , such as screening for lung cancer [ 25 ] or coronary calcium screening as a robust predictor of cardiovascular outcomes [ 68 ]  . 
furthermore , institutions as the american college of radiology ( acr ) have developed the acr appropriateness criteria for performing screening for colorectal cancer with ct colonography in specific clinical conditions [ 911 ]  . in the current health care environment , there is a growing awareness that prevention and early diagnosis may reduce the high mortality associated with cancer , cardiovascular and other severe diseases . 
this fact , together with the high accuracy , wide availability and fast image acquisition of ct [ 2 ] , may allow the use of this technology as an effective whole - body diagnostic strategy in patients derived from a check - up - unit . 
whole - body ct ( wb - ct ) can be defined as the integration of calcium scoring and cross - sectional chest and abdominopelvic imaging for the recognition of any abnormality . 
the role of wb - ct in self - referred and asymptomatic patients has been continuously debated since the publication of first article in 2002 , as a way to provide early diagnosis of cancer as well as cardiac and other diseases [ 1215 ]  . 
however , there are no more recent publications available that assess the usefulness of wb - ct and its findings . the aims of our study were to determine the frequency and spectrum of wb - ct findings in average - risk subjects derived from a medical - check - up - unit , to establish the recommendations reported by radiologists in these examinations and to evaluate the distribution of wb - ct findings according to sex and age - groups . materials andmethods patient population we retrospectively reviewed 6516 consecutive subjects who underwent wb - ct from june 2004 to february 2015 . 
a physician specialized in internal medicine from a specific la radiologia medica ( 2019 ) 124 : 11991211 medical - check - up - unit composed of three physicians ( with 2532years of experience ) who evaluated every patient . 
they determined the indication of performing a ct based on a table of risk factors previously defined by a committee of experts in radiology , internal medicine , cardiology and vascular pathology . 
all subjects were older than 40years ( mean age 58.4years ) , non - symptomatic , with no history of malignancy , and with one or more risk factors , including arterial hypertension , diabetes , history of cigarette smoking , obesity or hypercholesterolemia . written informed consent for study protocol was obtained from all patients before ct examinations . wholebody ct protocol all examinations were performed using a sixty - four - row multidetector ct ( 64 - mdct ) ( somatom definition and somatom sensation - 64 , siemens healthcare , forchheim , germany ) , with tube voltage and reference tube current time product variable depending on region included . 
all images were stored in pacs . the protocol of wb - ct included : low - dose chest ct ( 120kv and 40ma / s ) without contrast material . coronary artery calcium measurement ( 120 kv and 138ma / s ) in cases where coronary calcification was identified in low - dose chest ct . abdominopelvic ct ( 120kv and 180ma / s ) performed after intravenous injection of 120 - ml iodinated contrast medium ( omnipaquetm 300 ( iohexol ) , 300mgi / ml , ge healthcare bio - sciences , madrid , spain ) , at 2ml / s . 
sometimes , a delayed phase was necessary to confirm a diagnosis . additionally , osteo - ct ( 80kv and 250ma / s ) was performed in women to quantify bone density . 
for the analysis , bone density values of three consecutive vertebrae were compared with a reference phantototal trabecular , cortical and final bone mineral density according to age were obtained . findings anddatabase all ct images were reviewed at a computer workstation by eight expert radiologists with 1317years of experience . 
radiologists completed a specific questionnaire with three modules : chest ct , abdominopelvic ct and bone ct 1 3 la radiologia medica ( 2019 ) 124 : 11991211 1201 findings ( including calcium score and bone mass measurement )  . 
radiological findings : it is categorized according to location and classified as normal / abnormal for ( i ) every organ , ( ii ) every module , and ( iii ) every examination . 
we multiplied the recorded dose - length product ( dlp ) by a weighting factor of 0.014 msv / mgy ( for chest and calcium score ) and 0.017msv / mgy ( for abdomen and spine ) [ 19 ]  . statistical analysis descriptive statistics to analyze the number of imaging findings and recommendations were used . 
a chi - square test and a linear - by - linear association test were used to evaluate the distribution of the most important radiological findings detected in the chest , abdomen , pelvis and bones , in relation to gender and age - group , respectively . all p values < 0.05 were considered statistically significant . 
the data analysis was performed using spss 20.0 software ( armonk , ny : ibm corp )  . results subjects data a total of 6516 subjects ( 4499 men ( 69% , mean age of 58.1years ) and 2017 women ( 31% , mean age of 59.1years ) , overall mean age of 58.4years and mean body - mass - index of 27.69 ) underwent wb - ct . according to age , we classified them into four groups : group 1 ( 4049years , 324 women and 826 men ) , group 2 ( 5059 years , 776 women and 1806 men ) , group 3 ( 6069 years , 589 women and 1294 men ) and group 4 ( > 69years , 328 women and 573 men )  . radiological findings global ct results only 1.60% ( 104 / 6516 ) of individuals had a completely normal wb - ct . 
a physician from a specific medical check - up - unit evaluated every patient and determined the indication of performing a ct based on a table of risk factors previously defined by a multidisciplinary committee of experts . 
all these findings are important since they would encourage for risk factor modification , specific treatments and appropriate follow - up . the abdominal findings we observed were more numerous than those described with other non - ionizing examinations , such as ultrasound , performed in asymptomatic patients . 
therefore , wb - ct allows detecting a greater number and type of significant positive abdominal findings compared to ultrasound . 1 3 la radiologia medica ( 2019 ) 124 : 11991211 1209 as described by furtado etal . , in our cohort , we observed male predominance and we did not observe statistically significant differences in the main radiological findings between both sex groups , except for emphysema , bronchiectasis , bronchial disease and coronary calcium . in line with previous studies , the proportion of patients with significant radiological findings increased with age , except for emphysema and fatty liver , in which the distribution between the four age - groups was similar . in our cohort , a total of 1179 recommendations were performed . 
 [ 20 ] described abdominal recommendations more frequently ( 289 of 1192 patients )  . since ct is a technique available but expensive and uses ionizing radiation , it is controversial to be considered at the moment in a screening context [ 12 ]  . 
we do not intend to defend this exploration as a screening method , but we believe it can be considered as a useful tool in specific patients to identify important abdominal pathologies , when they are still asymptomatic , especially in a context of medical check - up - unit , where a physician evaluates each patient and determines the need to indicate or not a ct . one of the main discussible problems of wb - ct is the radiation dose . 
although some articles support that no dose of radiation is safe , the number of predicted radiation - induced cancers is tiny compared to the very large cancer incidence rate in humans , making statistical limitations for evaluating the impact of radiation on cancer rate [ 1 , 2429 ]  . 
that is the reason why we consider a physician should provide the indication for a wb - ct . some authors have debated the ethical problem of overimaging using x - ray such as salerno etal . 
this equipment employs an automated dose management that adapts scanning parameters to any patient , allowing to use high - quality ultra - low - dose imaging with a tin filter , providing significantly optimized dose efficiency . 
 however , radiologists adherence to these guidelines is not universal [ 3336 ]  . it is important to note that wb - ct in all patients of this study was indicated by a physician specialized in internal medicine . 
this had been already defended in recent articles , such as mazzei and volterrani [ 37 ] who defended that both clinicians and radiologists should be involved in choosing the most appropriate diagnostic imaging for each patient and each pathology . besides , the majority of patients who come to a check - up unit are people intrinsically concerned about their health status . 
in general , they feel more anxious about not to know how they are at that moment , than for the possible nonsignificant findings that may be detected in the wb - ct . incidental findings in radiologic explorations are becoming more frequent due to the improvement of the different radiological techniques , which implies greater sensitivity in the detection of pathological and non - pathological findings . 
 hence , the importance of radiologists , who should transmit in their reports the need to perform determined follow - up or other complementary techniques , depending on the incidental finding . 
this information will be also very helpful for the physician , who has requested the ct , to understand the relevance of a particular findings and , consequently , to adequately explain 1 3 1210 la radiologia medica ( 2019 ) 124 : 11991211 to the patient the importance of thethis fact highlights the importance of a fluent radiologistphysician and physicianpatient communication [ 38 ]  . thing is that many of these findings were detected at an early stage , allowing less aggressive and sometimes curative treatment . the last controversy of this technique is the cost - effectiveness [ 31 , 39 ]  . 
some previous works have found low prevalence of cancer in the evaluated populations and high rate of falsepositive findings that contribute to increased cost , individuals anxiety and over diagnosis , leading to unnecessary follow - ups and treatments . we think there is not enough information to use this exploration as a screening strategy . 
but on the basis of our results , although further research is needed to optimize wb - ct programs , we think this technique may be useful in a multidisciplinary well - planned check - up unit where radiologists and internal physicians maintain a close relationship in order to obtain the maximum benefit of diagnostic tests requested and to improve the patients health . 
with a standardized reporting system , a medical control about recommendations and a wellmanaged follow - up system , wb - ct may have an important role in providing real benefits to patients from early diagnosis of disease and changes in lifestyle to improve global health . the main limitation of this study is that our findings were based on a retrospective review of radiologist reports . 
also , the explorations were interpreted by different expert radiologists , and in most of relevant findings , the radiologists used the same consensus guidelines , such as the elcap protocol for lung nodules or the agatston classification for coronary calciu however , other non - tumoral findings were classified as mild , moderate or severe , according to a qualitative method , being more suggestive of undergoing inter - observer variations . 
 however , these variations were probably not very significant , taking into account that they were analyzed by expert radiologists in a specific area ( thorax or abdomen )  . a second limitation is that although the majority of findings ( mainly tumors ) were confirmed , few patients did not come back to our hospital and we could not achieve the final diagnosis . 
in these years , various changes , mainly in relation to radiation dose optimization and recommendations , were improved . finally , we did not evaluate the development of other diseases in short - term or long - term follow - up . 
therefore , we only have a complete assessment of the health of a specific individual at a particular time point , and we cannot predict the development of a future pathology . conclusion this examination allows identifying a number of non - depreciable findings that significantly increasing with age , highlighting different types of tumors . 
and the most important however , it should not be forgotten that most of findings are benign , so individuals should be aware of the high number of benign positive results that are diagnosed with this test and the unknown value of a negative test . the development of new radiological equipment in the recent years has increased the quality of the image with a significant decrease in the dose . 
given the lack of available literature in this line of research and our recent publication [ 2 ] discussed by ghaffari , we would like the opportunity to comment and provide our respective opinion . 
we have been utilizing rectal spacer implants in our practice over the last 7years [ 36 ] and have not had any major adverse events to report and , therefore , have recommended it as a safe and effective adjunct treatment for post - prostatectomy radiotherapy . 
ghaffari commented on multiple aspects of our work that we would like to address . first , conducting a randomized two - arm study is of potential value ; however , given ours is a large community cancer clinic ( and not an academic institution ) , we had interest in providing this treatment to all patients electing to receive hydrogel spacer implantation . 
additionally , given our radiation therapy protocols had changed prior to the use of our hydrogel rectal spacer implant practice in post - prostatectomy patients , we did not find value in comparing the outcomes against our own historical controls . 
this is a valid methodology in clinical practice medicine . second , we agree that rectal dosimetry planning preand post - implant would be of value to the field and plan to complete this study in the near future as an adjunct to the original presentation of our work . 
however , hydrogel rectal spacer implants are now covered by the majority of insurance companies in the usa as an authorized procedure with little to no cost to the patient . 
we would be keener to suggest that the use of a rectal retractor may be more uncomfortable to the patient , especially with a fractionated regimen for post - prostatectomy radiotherapy [ 7 ]  . third , in regard to ctv volume reporting , we did not find it necessary to report this given we had reported the ptv volume and mean dose in our original manuscript . 
additionally , in the manuscript we had defined for the first 25 fractions , the ctv as the residual prostatic bed , plus internal / external iliac nodes , and for the subsequent 15 fractions the ctv was defined as the residual prostatic bed plus margin [ 2 ]  . lastly , we welcome ghaffaris suggestion for the consideration of alternative technologies for rectal displacement from radiotherapy targets , namely his rectal retractor . 
the field of rectal spacer implants for prostate radiotherapy has evolved over the years , and many technologies have been utilized , including hyaluronic acid [ 3 , 4 ] , collagen [ 8 ] , and blood patch [ 9 ]  . 
the hydrogel spacer implant has withstood robustclinical investigations over the last decade and continues to be used as a valid technique for prostate spacing [ 5 , 10 ]  . 
1 , east jian she road , zhengzhou450052 , china 2 department ofhistology andembryology , college ofbasic medicine , zhengzhou university , zhengzhou , china although rare , pus in the mediastinum or pleural cavity may corrode vessels and result in an even higher mortality [ 7 ]  . 
over the past two decades , various conservative management protocols have been reported , such as endoscopic transluminal drainage or clipping , metallic stent placement and the application of biodegradable fistulae plugs or fibrin glue [ 4 , 810 ]  . 
despite these therapeutic modalities , treating an esophagogastric anastomotic leakage remains challenging and the optimal treatment has not yet been determined [ 2 , 4 , 11 ]  . considering the patients pathophysiologic changes and anatomic characteristics , we designed a protocol consisting of three - tube method ( abscess drainage tube , gastrointestinal decompression tube and jejunal feeding tube ) with or without temporary covered esophageal stent placement . 
this study enrolled all patients with esophagomediastinal and esophagobronchial fistulas after esophagogastro - anastomosis , who received three - tube method ( jejunal feeding tube , and thoracic drainage tube , gastrointestinal decompression tube and jejunal feeding tube placement ) with or without temporary esophageal stent placement in our department between january 2013 and february 2018 . 
a esophagography showing the site of fistula in the upper esophagus and irregular abscess in the mediastinub esophagography shows that the abscess cavity disappeared 1.7months after transnasal drainage tube placement . 
c , d at 1.7months after three - tube treatment , a chest ct scan in the mediastinal window shows disappearance of mediastinal abscess , re - expansion of the lungs with no pleural effusion 1 3 la radiologia medica ( 2019 ) 124 : 12531261 1255 fig . 
c , d at 1.6months after three - tube treatment and stent placement , a chest ct scan in the mediastinal window shows disappearance of esophagopleural fistula and reexpansion of the left lungs chest ( figs.2a , b ; 3a , b )  . 
esophageal covered stent placement is used for patients with enough length ( > 100mm ) of esophagus to effectively fix stents to avoid stent migration or failure of stent placement . 
the catheter tip was delivered into the distal end of the abscess cavity and then exchanged with a 5 - f pigtail catheter ( cook medical , inc . , bloomington , in , usa ) or a 5 - f straight catheter ( cook medical , inc . , bloomington , in , usa )  . 
a jejunal feeding tube was inserted into the proximal jejunusimilarly , gastrointestinal decompression tube was introduced into the gastral cavity . esophageal stent placement eight patients were treated with fluoroscopic placement of retrievable covered esophageal stent ( nanjing micro - tech medical company , nanjing , china )  . 
the diameter of the stents ranges from 18 to 20mthe length of the stents ranges from 7 to 14cthe stent was chosen based on the leakage location , and adequate stent coverage is allowed on either side of the leakage to ensure complete occlusion , with 3 to 5cm longer than the leakage . 
d after removal of stent and drainage tube , esophagography shows that the contrast agent flows though the esophagus without any leakage saline was injected and irrigated through the drainage tube twice a day . 
the covered stent and drainage tube was removed when chest ct showed complete disappearance of abscess cavity , full re - expansion of the lungs , with no pleural effusion ( figs.2c , d ; 3c , d )  . results general information this study involved a total of 23 patients with esophagogastric anastomotic leakage , including 19 men and 4 women ( table1 )  . 
 there were 17 cases of esophagopleural fistula , and six patients showed esophagomediastinal fistula . intervention andcomplications three - tube method was used for all patients , of which , eight patients received covered stent placement . 
a total of 10 covered esophageal stents were placed , with a median diameter of 20mm , median length of 120mall patients underwent abscess drainage tube placement or exchange of chest tube . 
no massive hemorrhage , esophageal 1 3 la radiologia medica ( 2019 ) 124 : 12531261 1257 1 3 1258 la radiologia medica ( 2019 ) 124 : 12531261 1 3 la radiologia medica ( 2019 ) 124 : 12531261 1259 rupture or other complications occurred during procedures . 
no grade 4 , grade 5 or grade 6 complications were observed . postoperative management all patients showed a reducing amount of pus daily , and the drainage fluid gradually became clear . 
chest ct , esophagography and radiographic examination showed that the abscess cavity had markedly decreased in seven patients or disappeared in 16 cases , indicating that continuous negative pressure suction via the drainage tube was effective . 
thirteen patients were able to return to their normal living conditions without any symptoone patient showed slight reflux with no need of medicine , and two patients showed mild choking feeling due to anastomotic restenosis . 
various 1 3 1260 la radiologia medica ( 2019 ) 124 : 12531261 conservative management protocols have been reported , such as endoscopic transluminal drainage or clipping , metallic stent placement and the application of biodegradable fistulae plugs or fibrin glue [ 4 , 810 ]  . 
esophageal stent placement is an alternative approach , which was initially used as palliative treatment for dysphagia in patients with esophageal cancer . recently , applications of esophageal stent have expanded to treat benign disease [ 14 , 15 ]  . 
owning to the ability to be removed easier with less damage , plastic stents are commonly used for the treatment for leaks and strictures of benign disease [ 1618 ]  . 
however , metallic stents also have been used for temporary treatment for benign diseases in recent years ; the appropriate type of stent for anastomotic leakage remains controversial [ 14 ]  . successful management of an esophagogastric anastomotic leakage requires prompt elimination of ongoing contamination by insertion of the covered stent and by adequate therapy of the associated mediastinal and thoracic infection . 
there was no perioperative death in this study , which is substantially lower than reported in other series [ 16 , 17 , 21 ] or conventional surgical therapy [ 6 ]  . 
in our series , all patients received continue chest drain , with a median duration of 2.5months. the duration between surgery and diagnosis is essential for the clinical outcomes [ 13 ]  . 
only eight patients received stent placement , which prohibit drawing a clear conclusion on the use of the covered stent . in conclusion , interventional treatment for esophagogastric anastomotic leakage can be considered a safe and effective alternative to operative treatment . 
examination protocol includes coronal and axial fisp , t2 - w half - fourier rare and dwi sequences , a baseline coronal t1 - w fat - saturated ultrafast ( gre ) sequence followed by contrast 3d t1 - w gre . 
all images were assessed by two radiologists who graded each of bowel segments for the presence of inflammation on a four - point confidence scale on the basis of wall thickening and wall signal on dwi and adc maps and comparing their results with post - contrast images . 
one false positive case corresponded to the absence of inflammatory histopathology changes at the level of the terminal ileum in a 15 - year - old male , and one false negative case was in a 10 - year - old female with only jejunal lesion . 
 these results emphasize the utility to include the dwi / adc in standard mr enterography protocols and suggest that dwi could replace t1 - weighted post - contrast sequences . keywords crohn disease pediatric mr enterography diffusion small bowel * gabriele masselli gabriele.masselli@uniroma1.it 1 radiology department , umberto i hospital , sapienza university , viale del policlinico 155 , 00161rome , italy 2 pediatric department , umberto i hospital , sapienza university , viale del policlinico 155 , 00161rome , italy 3 radiology department , careggi university hospital , university offlorence , largo g.a. 
vanvitelli , piazza miraglia 2 , 80138naples , italy introduction crohns disease ( cd ) is a chronic inflammatory and remitting disorder of the gastrointestinal tract ; in 25% of cases , it is diagnosed in childhood with an increasing incidence in children . 
one recent study showed that the incidence of pediatric cd has doubled in the usa over the last 12years [ 1 ]  . magnetic resonance enterography ( mre ) is an increasingly important pediatric imaging modality that is most often used to evaluate inflammatory bowel disease ( ibd ) , sparing children and adolescents from potential risks of ionizing radiation exposure [ 26 ]  . 
conventional mre requires vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 13061314 1307 intravenous administration of gadolinium - based contrast agents ( ca ) ; the most current concern about ca in children has been the accumulation of gd in the basal ganglia , which is of uncertain clinical significance but should be considered in patients with ibd , who undergo multiple imaging examinations over time to evaluate symptom recurrence [ 7 , 8 ]  . a non - contrast mre does not need glucagon injection and would improve patient comfort and compliance , reducing scanning time and in some cases avoiding the need for pediatric sedation ; moreover , it would reduce sanitary costs ( in the usa , contrast adds up to $1000 to the mri price for out - of - pocket paying patients ) [ 9 ]  . in this regard , diffusion - weighted imaging ( dwi ) has been increasingly used for abdominal and pelvic examinations due to its ability to measure molecular water diffusion into the extracellular space and to detect microscopic changes of inflammatory processes . 
its values decrease with increased tissue cellularity or cell density and may help in the quantitative analysis of disease activity [ 1012 ]  . dwi appears well adapted for children thanks to rapid acquisition time , a free breathing mode that reduced motion artifacts , high tissue contrast and finally because it obviates the need for contrast enhancement . 
currently , dwi is considered an additional sequence in the mre and only a few studies have been done in order to evaluate its potential and diagnostic accuracy alone and in comparison with standard mri sequences [ 13 , 14 ]  . the aim of this study was to determine whether mre performed with dwi sequences , without administration of intravenous gd - ca , is comparable to contrast - enhanced mre ( ce - mre ) in the detection of small - bowel inflammation in pediatric patients with cd . materials andmethods patients andmethods this prospective study was approved by the institutional review board of our university . 
parent or guardian informed consent and subject assent were obtained at the time of study enrollment . sixty - eight consecutive patients ( 38 females and 30 males ; mean age 10.3years ; range , 616years ) treated at the ibd pediatric unit of our university hospital were consecutively and prospectively included between april 2015 and june 2018 . inclusion criterion was the diagnosis of cd according to lennardjones criteria [ 6 ]  . 
coronal and axial fisp images were obtained first , and if distension was adequate , t2 - w images were obtained in the coronal and axial planes with a singleshot half - fourier rare sequences ( i.e. , haste half - fourier acquisition single - shot turbo spin echo )  . coronal dwi and axial dwi were obtained by using a single - shot spin - echo - type echo - planar imaging ( epi ) sequence with fat suppression and parallel technique ( reduction factor 2 )  . 
imaging parameters for dwi were as follows : tr / te 2500 ms / 80 ms ; matrix 128 128 ; field of view 280 400mm ; slice thickness / gap 6mm / 1mm ; 6 averages ; bandwidth 1930hz / pixel . 
the time required to acquire the dwi set was 3mb values of 50 , 400 and 800s / mm2 , as used in other abdominal applications [ 13 ] , were employed ( table1 )  . 
isotropic adc maps were generated with a commercially available software workstation system ( leonardo ; siemens , erlangen , germany ) using all b values and taking an average value of the three directions of diffusion sensitization . 
the bowel wall was considered to be thickened when it was > 3mon dwi , grading scores of 0 and 1 were regarded as indicating normal bowel wall and scores of 2 and 3 bowel wall inflammation . on t2 - w images , we analyzed the following signs : wall thickness ( setting a grading score of 1 : 3mm , 2 : 46mm and 3 : > 6 mm ) , submucosal edema , aphthous ulcers , lymphadenopathy . on t1 - w post - contrast images , we analyzed the following signs : comb sign ( defined as mural stratification with engorged vasa recta that penetrate the bowel wall perpendicular to the bowel lumen ) , mesenteric hyperemia and stratified contrast enhancement of the mucosa . to minimize recall bias , two reading sessions were performed 4weeks apart from each other and mr images ( t2 , contrast t1 and diffusion - weighted images ) were randomly analyzed during the different sessions . patient information was removed from all images . 
during each imaging analysis , the readers were asked to determine the presence and location of small - bowel inflammation . moreover , after 3weeks , during a third interpretation , the two readers ( 1 ) resolved discrepancies in consensus and determined the diagnoses that were compared with the reference standard diagnoses ; and ( 2 ) evaluated image quality of t1 - weighted images post - contrast and dwi images by using a point scale : a score of 0 indicated non - diagnostic images ; 1 , diagnostic images with numerous artifacts ; 2 , diagnostic images with a few artifacts ; and 3 , diagnostic images without artifacts ; ( 3 ) objective measurements of adcs signal intensity were calculated using the standard tools of the workstation . 
regions of interest ( rois ) on the adc maps were drawn by an mr imaging physicist ( s.s. , 10years of experience in abdominal mr imaging ) and the two radiologists in consensus by using visual correlation of the adc maps with the anatomic information derived from the corresponding t2 - weighted images . 
three values for each zone were recorded , and the final adc value was the average . 1 3 la radiologia medica ( 2019 ) 124 : 13061314 1309 the largest possible polygonal - shaped regions of interest ( rois ) , ranging from 8 to 18mm2 , were placed at the level of the small - bowel wall . inflammation ( eais = 0 ) and those with histopathological inflammation ( ais score > 1 ) using the mannwhitney u test . reference standards the standard of reference for the presence of active lesion of ibd was histopathological findings ( obtained by biopsy during endoscopic examination in 63 cases and by surgical specimens in 5 cases : 1 lesion of the jejunum and 4 lesions of the ileum )  . the mr findings were correlated with the corresponding histological references for each segment by a coordinator not involved in the studies . histopathology activity score the intestinal biopsies were stained with hematoxylineosin and retrospectively reviewed by an experienced pathologist > 10years of experience , who was unaware of clinical information or mri findings . 
the histopathologist applied an endoscopic biopsy acute inflammatory score ( eais : table2 ) based on the typical morphological features of crohns disease described in guidelines published by the european crohns and colitis organization . at least three samples of biopsy were collected for each patient , and the highest score for each was used for that patient , in accordance with the standard procedure in our institution . statistical analysis quantitative variables are given as means and standard deviation ( s.d. ) or as medians in the case of an abnormal distribution . 
proportions are expressed as percentages and 95% confident intervals ( cis )  . differences in quantitative measures were tested by students test or kruskalwallis test if the conditions of students test were not met . 
qualitative variables were compared by exact fishers test or chi - squared test . using the histopathological standard of reference , adc values were compared between patients with no histological table 2 histopathology grading for acute inflammation score ( ais ) histological variable erosion or ulceration polymorphs in the lamina propria cryptitis crypt abscess formation inflammatory exudates granulomas grade 0 = no , 1 = yes 0 = no , 1 = yes 0 = no , 1 = yes 0 = no , 1 = yes 0 = no , 1 = yes 0 = no , 1 = yes eais scores were then compared across qualitative dwi grades using kruskalwallis test with post hoc correction . the sensitivity and specificity of dwi grades 2 and 3 for active disease ( ais > 1 ) were calculated . 
a threshold was determined by calculating receiver operating characteristic ( roc ) curves . all correlations were studied using spearmans nonparametric correlation coefficients ( r and p value , respectively )  . 
calculations were done with stata v10 ( stata corp . , college station , tx , usa )  . the strength of agreement was considered poor for values less than 0.20 , fair for values of 0.210.40 , moderate for values of 0.410.60 , good for values of 0.610.80 and very good for values of 0.811.00. results the mean time between mre and endoscopy with biopsy was 5.5days ( range 121days )  . based on the histopathology , findings were classified 48 / 68 ( 70% ) patients in acute inflammatory phase and 20 / 68 ( 30% ) patients in no - acute inflammatory phase , respectively . baseline patient characteristics are shown in table3 . 
particularly , this last characteristic could avoid the venous access , the risk of adverse reactions to the contrast medium and minimize patient discomfort particularly important in the pediatric population that can preclude their cooperation at this examination . there are several advantages in using dwi instead of ce t1 - w images : a shorter examination duration ( if postgadolinium mr imaging is not performed ) and no need for catheter placement and for glucagon injection . in our study , images obtained by dwi displayed better image quality than ce t1 - w images . 
a coronal steady - state true fisp image showed thickening of the wall of the terminal ileum ( arrows ) with evidence of increased layered enhancement on b coronal post - contrast t1 - weighted image . 
e axial t2 - weighted single - shot fast spin - echo image with fat saturation shows thickness of the wall of the terminal ileum ( short arrow ) with a hyperintense fluid collection ( arrow )  . 
in the future , further studies investigating dwi findings using different b values may determine their role in the detection of bowel inflammation . finally , comparison of imaging results with histological activity as gold standard is debatable since inflammation in crohns disease is discontinuous , leading to sampling error for histological assessment . 
transmural inflammation in crohns disease may also mean that histological mucosal healing does not represent quiescent disease , since deeper inflammation , although invariably in the form of lymphoid hyperplasia , and therefore reflecting chronic inflammation rather than acute inflammation , may persist [ 34 , 35 ]  . in conclusion , our study has shown that dwi sequences with the corresponding adc maps have a high accuracy in detecting the bowel segment affected by cd and that , associated with the standard t2 - weighted images , allows to increase the diagnostic accuracy . 1 3 la radiologia medica ( 2019 ) 124 : 13061314 1313 fig . 
a coronal t2 - weighted haste image showed mild thickening of jejunal small - bowel loop ( arrows ) with no evidence of increased enhancement on b coronal post - contrast t1 - weighted image . 
based on the restriction of the diffusion cd in the active phase was diagnosed that was confirmed by endoscopy this evidence suggests the utility to include the dwi / adc in the standard protocols of mr enterography . 
dwi could replace t1 - weighted post - contrast sequences for detecting small - bowel acute inflammation in patients with cd , avoiding injection of contrast medium and reducing the examination time making the examination better tolerated by pediatric patients . compliance with ethical standards conflict of interest the authors declare that there is no conflict of interest regarding the publication of this paper . ethical standards the present study was conducted in accordance with the institutional ethical committee of sapienza university of rome . 1 3 1314 la radiologia medica ( 2019 ) 124 : 13061314 informed consent parent or guardian informed consent was obtained at the time of study enrollment . la radiologia medica ( 2019 ) 124 : 13241332 radiotherapy locally advanced inoperable primary orrecurrent nonsmall cell lung cancer treated with4week hypofractionated radiation therapy ( 3gy / fraction ) mauriziovaleriani1 mattiafalchettoosti1 lucamarinelli1 lucanicosia1 chiarareverberi1 vitalianadesanctis1 davidemollo1 received : 7 february 2019 / accepted : 7 july 2019 / published online : 17 july 2019 italian society of medical radiology 2019 abstract background the prognosis of locally advanced non - small cell lung cancer ( nsclc ) treated with conventional radiotherapy remains poor . 
hypofractionation reduces overall treatment time increasing biological effect in patients not suitable for concurrent chemo - radiotherapy . method from january 2009 to october 2016 , 76 inoperable locally advanced primary or recurrent nsclc patients were treated with 60gy in 20 fractions of 3gy / each for 4weeks as exclusive or post - chemotherapy treatment . 
univariate and multivariate analyses demonstrated that patients with complete response presented better outcomes , whereas no statistically relevant difference was evidenced in terms of previous chemotherapy , recurrent vs primary disease , volume and stage . 
complete local response was a predictor of better outcomes , and any efforts will be made to perform prospective clinical trials to further evaluate hypofractionated regimens with increased lesional bed . keywords locally advanced nsclc radiation therapy 3d - rt hypofractionation introduction lung cancer is the leading cause of death related to cancer [ 1 ]  . 
nevertheless , the prognosis remains poor , with a 5 - year * maurizio valeriani mauval1@libero.it 1 department ofradiation oncology , sant andrea hospital , sapienza university , via di grottarossa 1035 - 1039 , 00189rome , italy overall survival ( os ) rate ranging from 5 to 10% [ 5 ] and a median survival time approximately of 16 to 17months after concurrent treatment ; intensification of regional heed has been attempted to improve local control and survival rates [ 6 ]  . 
treatment intensification may be obtained also by shortening the overall treatment time with the purpose to reduce accelerated repopulation of tumor cells that could start 46weeks after the beginning of treatment [ 8 ]  . 
these studies demonstrated good local control with acceptable acute and late toxicity rates after hyport based on three - dimensional conformal radiation therapy ( 3d - crt ) modern planning system [ 10 , 11 ]  . based on these postulations on 2009 , we started to treat patients affected by inoperable advanced - stage nsclc not suitable to concurrent chemo - radiotherapy for comorbidities . 
 response , local control , toxicity rates and survivals were evaluated . methods andmaterials patients we retrospectively collected data regarding 76 histologically confirmed inoperable locally advanced primary or recurrent nsclc patients treated with curative hypofractionated radiotherapy in our department between january 2009 and october 2016 . 
all patients had performance status ( eastern cooperative oncology group criteria ) 2 . pre - treatment evaluation consisted of contrast - enhanced total body computed tomography ( ct - tb ) scan , bronchoscopy with histological examination , respiratory functional tests , 18 - fluorodeoxyglucose positron - emission tomography ( fdg - pet / ct ) scan . 
all patients signed written informed consent . treatment all patients underwent pre - treatment ct planning in the supine position , merged with diagnostic ct and pet - ct for the target volume delineations ( gross tumor volumegtv , clinical target volumectv )  . 
the gtv1 and the gtv2 included the primary tumor and the clinically positive lymph nodes with a short - axis diameter 1cm and / or positive at pet - ct scan . 
during treatment , all patients underwent medical examination and blood test examinations . followup andstatistics the first follow - up was planned 2months after rt completion with contrast - enhanced ct - tb and blood test examinations ; then , follow - up period was about 3months for the first 2years after rt completion and every 6months afterward . 
 fdg / pet - ct was performed until 6months after rt or for suspected radiological progression . toxicities were evaluated using the common terminology criteria for adverse events ( ctcae ) version 4.0 and were classified as acute ( within 3months from rt ) or late ( after 3months from rt )  . the response evaluation criteria in solid tumors ( recist 1.1 ) measurement was used to determine response rates and progression of disease [ 13 ]  . 
patients , who underwent local or distant progression , were treated with rt or local therapy when possible and / or systemic therapy . kaplanmeier method was used for univariate analysis and cox regression model for multivariate analysis . 
progression - free survival ( pfs ) and the loco - regional pfs ( lr - pfs ) were defined as the time to loco - regional / systemic progression or death and the time to loco - regional progression , respectively . 
subgroup analysis was performed by stage ( iiia vs iiibiiic vs iva ) , chemotherapy ( cht ) prior to rt ( yes vs no ) , type of disease ( primary vs recurrent disease ) , responses ( cr vs pr vs nc - pd ) and volume ( < 250cc vs 250cc ) ( table1 )  . statistical analysis was performed using the spss statistical software package version 24.0 ( spss , inc . , chicago , il , usa )  . 
previous cht ( p = 0.518 ) and volume ( p = 0.173 ) were not statistically relevant . fifty - eight patients ( 76.4% ) progressed : 12 ( 15.8% ) only loco - regionally , 23 ( 30.3% ) only at distance and 23 ( 30.3% ) both loco - regionally and at distance . 
previous cht ( p = 0.303 ) , type of disease ( p = 0.342 ) , volume ( p = 0.620 ) and stage ( p = 0.148 ) were not statistically relevant . forty - six patients ( 60.5% ) developed distant metastasis in one or multiple sites ; contralateral lung was involved in 17 cases , brain in 14 , bone in 16 and liver in 7 . 
 no correlation between dosimetric parameters and grade 2 or 3 lung toxicity was found , whereas grade 2 or 3 acute esophageal toxicity was correlated with mean dose ( > 13.5 gy ) and v42 ( > 20% )  . 
data are summarized in table5 . discussion up to date , there is an increasingly interest to hypofractionation for the treatment of locally advanced nsclc with the aim to intensify the treatment and to shortening the total treatment time . 
in the past , the use of hypofractionation was limited by concerns about high rate of late toxicities until improvement of planning and delivery techniques was empowered . therefore , a significant percentage of patients develop an advanced - stage nsclc presenting comorbidities , advanced age , poor performance status and potentially poor tolerance of standard concurrent chemo - radiotherapy ( crt )  . 
then , many different hypofractionated schedules were used with doses ranging from 45gy in 15 fractions to 84gy in 35 fractions [ 1519 ]  . minding all the above points , we analyzed in our study a cohort of inoperable locally advanced primary or recurrent nsclc patients , not suitable to concurrent chemoradiotherapy for comorbidities , with exclusive or postchemotherapy hypofractionated radiotherapy . 
a randomized eortc study [ 25 ] reported a median survival similar to our ( 17months ) in patients treated with 2 cycles of induction 1 3 la radiologia medica ( 2019 ) 124 : 13241332 1331 cisplatin and gemcitabine or concurrent low dose daily cisplatin and 66gy in 24 fractions . 
six out of 75 patients ( 8% ) presented grade 45 toxicities ( for damage of proximal bronchial tree and surrounding vasculature ) , and most of them received a total dose of at least 75gy . hypofractionation was generally well tolerated with three studies reporting any significant differences in terms of toxicities with respect to conventional fractionation . 
our study presented some limitations : retrospective evaluation , limited number of patients and wide - range interval in recruiting study population . conclusion outcomes in locally advanced nsclc remain non - satisfactory , and concurrent chemo - radiotherapy represents , actually , the standard treatment . 
cdi should be suspected in case of unexplained diarrhea and abdominal pain in patients with a recent history of antibiotic use and healthcare exposures ; diagnosis is based on a combination of clinical and laboratory findings with demonstration of c . 
considerable overlap exists between the cect findings of cdi and those of colitis of other origins , such as typhlitis , ischemic colitis , graft - versus - host disease , radiation colitis and inflammatory bowel diseases ; however , some features may help distinguish between these conditions . 
this paper provides a comprehensive overview of the imaging features of clostridium difficile colitis and its mimics , with a view to assist the radiologist in reaching the correct diagnosis . keywords clostridium infections pseudomembranous enterocolitis differential diagnosis contrast - enhanced computed tomography abbreviations c . 
difficile can colonize and proliferate in the gut of individuals with altered microbiota , producing two major exotoxins ( toxin a and toxin b ) able to damage the human colonic epithelium and to stimulate the inflammatory response ; histologically , the consequence of mucosal necrosis is the formation of pseudomembranes , an inflammatory exudate overlaying the denuded mucosa [ 1 , 2 ]  . 
the incidence of clostridium difficile infection ( cdi ) has dramatically increased in the last decades , and estimates predict a continuing increase in the coming years [ 3 ] ; today cdi is a leading cause of hospital - associated infections in europe ( about seven cases for every 10 , 000 hospitalized patients ) ; incidence is similar in the usa , where cdi causes 14 , 000 deaths each year [ 1 ]  . 
a considerable rise in mortality was observed since the worldwide emergence of new vol . : ( 0123456789 ) 1 3 1186 la radiologia medica ( 2019 ) 124 : 11851198 hypervirulent strains , such as c . 
clinicians should consider the possibility of cdi in patients with unexplained diarrhea associated or not with abdominal pain , in patients with a recent history of antibiotic use and healthcare exposures [ 6 , 7 ]  . 
however , severe cases of cdi have been reported in otherwise healthy patients , without traditional risk factors [ 8 ]  . the diagnosis of cdi is based on the combination of clinical and laboratory findings and requires the demonstration of c . 
although it is not routinely part of the evaluation of cdi , colonoscopy with biopsies may help to confirm the diagnosis of cdi ruling out other colonic etiologies , particularly when results from stool testing are negative or still pending [ 9 , 10 ] ; however , colonoscopy is an invasive procedure with an associated risk of bleeding and perforation . contrast - enhanced computed tomography ( cect ) plays an important role in the management of patients with suspected colonic disease thanks to its ability to evaluate both the colonic wall and the adjacent soft tissues ; cect also helps in determining the extent and severity of the disease and in detecting potential complications , such as toxic megacolon and perforation [ 11 , 12 ]  . 
however , a significant number of patients shows no abnormalities on abdominal cect scan and often cect findings do not allow a reliable distinction to be made between cdi and other colonic diseases ; the list of possible differential diagnoses is long and includes , among others , typhlitis , ischemic colitis , graft - versus - host disease ( gvhd ) , radiation colitis and inflammatory bowel disease ( ibd ) [ 13 , 14 ]  . 
the aim of this paper is to review the cect findings that can help to identify and differentiate cdi from other inflammatory conditions of the colon . imaging features ofclostridium difficile colitis since clinical presentation can be unclear or misleading and due to the in - depthness of the differential diagnosis , computed tomography plays a crucial role in evaluating the patient , especially in case of severe abdominal paeven if the examination protocol is not fixed and should be adapted to each situation , in patients with abdominal pain with suspicion of a colonic origin , a triple - phase ct protocol ( unenhanced , late arterial and portal venous phase ) of the abdomen and pelvis is indicated . 
the standard intravenous contrast material is a nonionic , low - osmolar iodinated one with a concentration between 350 and 400mgi / ml , administered using a power injector at a rate of 34ml / s with a bolus tracking technique . 
a delayed arterial phase ( 15s after peak aortic enhancement ) is optimal to depict the enhancement pattern of colonic wall and is required for the assessment of mesenteric arterial supply ; portal phase ( 7080s ) allows to exclude other causes of acute abdominal pain and to outline the venous drainage . at our institution , oral contrast material is not routinely administered because it is time - consuming ( at least 6090min for adequate opacification of the entire colon )  . 
 however , oral contrast agents can be used to improve image quality ; in this case , low - density oral contrast agents are preferable because they do not obscure mural enhancement . intestinal ct findings intestinal cect findings suggestive of cdi include colonic wall thickening and colon wall nodularity . colonic wall thickening represents the most common finding in cdi ; it can be circumferential or eccentric and it is generally more prominent in comparison with other inflammatory colonic diseases with the exception of crohns disease [ 14 ]  . 
in the majority of the cases , cdi presents as a pancolitis with a marked thickening that can be seen throughout the whole colon ( fig.1 ) ; in up to 3040% of the cases , there is a limited involvement of the right colon , and in other cases , the disease starts in the rectum and extends proximally to the left colon [ 14 , 18 ]  . 
some cases of small bowel involvement have been reported in the literature , mainly as isolated case reports , particularly in patients with surgically altered small bowel anatomy [ 1922 ]  . the administration of intravenous contrast material provides several important advantages in assessing wall abnormalities . 
wall thickening is typically irregular and often asymmetric with a shaggy internal outline , probably due to mucosal edema , and cect can better depict the presence of nodular swelling projections ( wall nodularity ) protruding into the lumen ( the ct equivalent to thumbprinting classically seen in barium enema ) [ 15 ]  . 
 ( 64 patients who underwent abdominal ct scan within 3days of stool sample for cytotoxin assay ) , the presence of wall nodularity was statistically associated with a more severe clinical disease , regardless of the degree of colonic involvement [ 23 ]  . in association with thickened colonic wall and wall nodularity , other cect findings can be a clue for diagnosis . 
 mucosal hyperemia and submucosal inflammation can give rise to an abnormal pattern of wall enhancement , with a 1 3 la radiologia medica ( 2019 ) 124 : 11851198 1187 fig . 
1 clostridium difficile colitis : axial ( a , b ) and coronal ( c ) cect images show marked and irregular wall thickening ( maximum thickness of 23 mm ) , with intense enhancement of the mucosa ( white arrows )  . 
mild inflammatory changes are present in the pericolic fatty tissue ( dashed arrow ) stratified multilayered appearance of colonic wall ( target sign ) [ 14 ]  . even if it is not always possible in urgent cases , oral contrast material can be helpful in order to distend the colon and to better define its luminal surface . 
2 clostridium difficile colitis : axial cect scan demonstrates low - attenuation wall thickening involving the entire length of the colon with intense mucosal enhancement ( white arrow , a ) ; the enhancing mucosa is stretched over the edematous haustral folds , resembling an accordion even in the absence of intra - luminal contrast ( black arrow , b )  . 
a large amount of ascites is also present ( dashed arrow , c ) 1 3 1188 la radiologia medica ( 2019 ) 124 : 11851198 extraintestinal ct findings pericolic stranding and ascites are the most common extraintestinal findings . 
in some series , ascites has been reported in a high number of patients with cdi and can serve as a useful adjunct in the differential diagnosis with crohns disease [ 13 , 14 , 16 , 25 ]  . 
however , ascites is not specific since it can be seen in a large variety of other inflammatory and infectious diseases and also in case of coexisting medical conditions ( e.g. , portal hypertension , congestive heart failure and metastatic cancer ) [ 26 ]  . as mentioned above , a considerable rise in mortality was observed following the spread of hypervirulent strains of cd . 
to the best of our knowledge , only one study analyzed the ct features of cdi after the outbreak of epidemic hypervirulent strains , trying to outline the existence of differences in ct presentation with the classic form of cdi . 
retrospectively reviewed the abdominal ct of 165 patients with confirmed cdi ( ct performed within 72h from positive stool sample examination ) ; patients were stratified in two groups depending on the year of diagnosis ( 19982002 , 43 patients ; 20032006 , 122 patients ) , which corresponds , respectively , toa low or high likelihood of 027 hypervirulent strain infection . 
the following ct features were reviewed : increased colonic wall thickness , diffuse colon involvement ( pancolitis ) , target sign and the presence of pleural effusion , ascites and subcutaneous edema . 
difficile , and the radiological presentation of patients with severe cdi was similar either before or during the epidemic period ( 20032006 ) [ 27 ]  . differential diagnosis due to the poor specificity and the overlap of imaging findings between different colonic diseases , the radiologist should be aware of the extensive differential diagnosis and analyze the diagnostic clues and their distribution carefully in order to reach a correct diagnosis of cdi . typhlitis typhlitis , also known as neutropenic colitis , is a life - threatening disease that primarily affects immunocompromised patients [ 28 , 29 ]  . 
in its classic form , typhlitis affects the cecum , which maybe due to its limited blood supply ; the ascending colon and the terminal ileum can also be involved . 
 clinical and laboratory findings are often non - specific : patients typically present with fever , diarrhea abdominal tenderness and abdominal pain predominantly in the right lower quadrant ; intestinal bleeding is usually less common [ 28 , 30 ]  . on cect , findings suggestive of typhilitis include cecal distension and circumferential wall thickening ; the affected colonic wall may show an intramural pattern of low attenuation due to submucosal edema [ 31 ]  . 
 while typhlitis is usually limited to the cecum ( even if any segment of the small and large bowel can be involved ) , cdi is more likely to cause a pancolitis ; however , some of these cases of limited involvement of cecum and right - side colon have been described , making it more difficult to distinguish among the two conditions [ 13 ]  . ischemic colitis ischemic colitis ( ic ) is the most common form of intestinal ischemia , representing about the 70% of the cases [ 33 ]  . 
 ic results from a reduced vascular flow to the colon either for arterial and venous occlusion ( i.e. , occlusive forms ) and low flow states due to hypotension , congestive heart failure , cardiac arrhythmias and hemorrhagic or septic shock ( nonocclusive mesenteric ischemia : nomi ) ; ischemia is usually limited to the mucosa or submucosa , but in severe and advanced cases transmural necrosis may develop [ 34 ]  . 
early colonoscopy performed within 48h of presentation is the gold standard for the diagnosis of ic , but this is an invasive procedure with an associated risk of complications such as perforation ; according to the american college of gastroenterology ( acg ) , the diagnosis of ic can be suggested relying on cect findings ; in case of high clinical suspicions , ct should be the first - line imaging to assess the distribution and the phase of ic [ 36 ]  . cect findings vary in relation to the stage and the extent of the disease , depending on the underlying pathogenesis . 
in vascular occlusive forms , the ischemic injury is followed by reperfusion from riolans arcades collateral vessels : in the acute phase , the colonic wall is thickened and has a stratified appearance due to edema and / or hemorrhage with a subsequent narrowing of the lumen [ 37 ]  . 
the involved tract can show a low - attenuation pattern due to edema ( with a possible target sign on cect ) or , in case of intramural hemorrhage , a hyperdense colonic wall on non - contrast - enhanced ct . 
3 typhlitis : axial ( a , b ) cect images show moderate wall thickening of the cecum and terminal ileum ( white arrows ) in a man with hodgkin lymphoma who has recently completed chemotherapy . 
 coronal cect image ( c ) demonstrates an ill - defined , infiltrating soft tissue mass ( dashed arrow ) in the mesentery that displaces the small intestine and abdominal vessels be present [ 14 ]  . 
if riolans arcade provides an adequate blood supply , the colonic wall returns to normal thickness and pericolic and free fluids gradually decrease , if not the loss of muscular tone and the absence of blood supply lead to the thinning of the bowel wall with a paper - thin appearance [ 37 ]  . 
pneumatosis with or without air in the mesenteric vessels or portal vein is detected in severe cases of ic when transmural necrosis occurs and indicates a poor prognosis [ 37 ]  . 
in chronic stages , weeks or months later or with long - standing arthrosclerosis , fibrotic changes lead to a mild and irregular circumferential thickening of the colonic wall ; gaping lumen and disappearance of the haustral folds are common associated findings [ 38 ]  . since the above - mentioned cect findings are not pathognomonic , emphasis should be placed on geographic distribution of the abnormalities and on the presence of extra - intestinal findings to reach the correct diagnosis . in the occlusive form of ic , the pattern of bowel involvement in ic is related to vascular anatomy , showing a clear demarcation with the non - ischemic tract [ 38 ]  . 
ic is more likely to occur in certain weak points , known as watershed areas , at borders of territories supplied by different vascular systems ; these include the splenic flexure ( griffiths point ) , the retto - sigmoid junction ( sudecks point ) and also the ilealcecal region because of the scarcity of marginal vessels [ 39 ]  . 
the presence of arterial filling defects , aortic dissection with the involvement of mesenteric arteries , small arterial aneurism and occlusion ( in the setting of vasculitides ) and venous thrombosis often with engorged mesenteric veins due to outflow obstruction is typically observed ; the presence of signs of ischemic damage involving other visceral organs ( i.e. , the liver , kidneys , spleen and pancreas ) may help the radiologist , suggesting the diagnosis ( fig.4 ) [ 40 ]  . nomi , which accounts ~ 2030% of all cases of acute mesenteric ischemia , represents a real diagnostic challenge for the radiologist [ 41 ]  . 
as a result of this , the affected colon usually appears dilated with a classic paper - thin wall due to the marked decrease in muscular tone and vascular volume loss ; the geographic distribution simulates an obstruction of both the superior and inferior mesenteric arteries . 
 this presentation may mimic the appearance of normal distended colon and the presence of pericolic fluid often 1 3 1190 la radiologia medica ( 2019 ) 124 : 11851198 fig . 
4 ischemic colitis : axial ( a , b ) and coronal ( c ) cect images show circumferential , symmetric wall thickening and abnormal enhancement of the left colon with a stratified appearance due to edema ( white arrows )  . 
the left kidney is reduced in size due to vascular - based suffering ( e ; open arrow ) and multiple ischemic lesions of the spleen are present ( f ; open arrow ) representing the only other associated finding [ 37 , 38 ]  . 
the reduction in contrast enhancement of other visceral organs , along with the patients clinical history , is an important diagnostic clue [ 38 ]  . graftversushost disease the gastrointestinal tract is one of the principal target organs in acute gvhd ( beyond the first month after allogeneic bone marrow transplantation ) ; the colon can be affected in isolation or as a part of a pan - intestinal involvement [ 42 ]  . 
the development of intestinal gvhd is due to mucosal cell and intestinal stem cells disruption as a consequence of immune dysregulation ; alteration of gut microbiota also plays an important role [ 43 ]  . 
presenting symptoms include diarrhea , with or without hematochezia , and crampy abdominal pain ; these symptoms should raise the suspicion for gvhd or infection . the gastrointestinal tract is one of the principal target organs in acute gvhd . 
the pattern of bowel involvement shows a discontinuous distribution with normal portions of bowels separating the involved tract , and frequently , the small bowel is also affected ; the length of bowel involvement in gvhd is generally less extensive in comparison with radiation - induced colitis [ 24 ]  . 
wall thickening is less marked than in typhlitis and cdi , and although a certain overlap of wall thickness ranges can be seen , a measurement > 7mm should lead to exclude gvhd as a possible diagnosis ( fig.5 ) [ 16 ]  . radiation colitis radiation therapy to the pelvis is often used as adjuvant or neoadjuvant therapy in many gynecologic , urologic and rectal cancers . 
one of the major adverse effects is the development of radiation - induced injuries to the surrounding healthy tissues , such as small bowel and colon [ 46 ]  . 
5 graft - versus - host disease : circumferential wall thickening , with intense enhancement of the mucosa involving the entire length of the colon ( a , b ; white arrows )  . 
this appearance and the extent of colon involvement can mimic that of clostridium difficile colitis , but the thickness of colonic wall is inferior ( maximum thickness of 7mm ) and the small bowel is also affected ( c ; open arrow )  . 
note also the marked engorgement of the vasa recta and fat stranding ( dashed arrows ) acute radiation colitis usually occurs within 24weeks after the treatment ; the clinical presentation is non - specific with diarrhea , abdominal pain and tenesmus , which are usually self - limited [ 46 ]  . 
clinical history is fundamental to suggest the diagnosis , and cect is generally not necessary ; if performed , cect in the acute phase demonstrates wall thickening of the affected tract with adjacent inflammatory stranding ( fig.6 ) [ 14 ]  . 
difficile , a large variety of bacterial , viral and parasitic pathogens are responsible for infectious colitis ; in developed countries , bacteria are the most common cause of infectious colitis and include escherichia coli , shigella , salmonella , yersinia , campylobacter , staphylococcus and chlamydia trachomatis [ 14 ] ; cytomegalovirus is a common cause of colitis in immunosuppressed patients [ 24 ]  . generally , the diagnosis of infectious colitis is based on clinical symptoms and confirmed on the basis of stool analysis and / or colonoscopy [ 48 ]  . cect is generally not required for the diagnosis of infectious colitis , but may be performed incidentally or in cases with equivocal clinical presentation . 
in the acute phase , all these types of infectious colitis manifest with wall thickening ( which usually enhances homogeneously ) , inflammation of the pericolic fat and various degrees of ascites ( fig.7 ) [ 49 ]  . 
colonic distension and multiple air - fluid levels may be seen due to increased fluid production [ 14 ]  . inflammatory colitis ibd include crohns disease ( cd ) and ulcerative colitis ( uc ) , two long - term , relapsingremitting disorders characterized by inflammation of the gastrointestinal tract [ 50 ]  . 
uc typically begins in the rectum and extends proximally ; the inflammation is confined to the mucosa and uniform in distribution with a preponderance of left - sided colon [ 51 ]  . 
cd can affect any segment of the gastrointestinal tract and shows a discontinuous pattern of inflammation with uninvolved areas separated by areas of transmural inflammation ( skip lesions ) ; over 60% of patients show colonic involvement [ 52 ]  . 
6 radiation colitis : axial ( a , b ) and sagittal ( c ) cect images demonstrate smooth wall thickening in the rectum and sigmoid colon ( white arrows )  . 
7 infectious colitis : moderate wall thickening of the transverse colon with homogeneous enhancement ( a ; white arrow ) in a young man with severe diarrhea or abdominal pathe small bowel is also affected ( b ; dashed arrow )  . 
stool cultures were positive for e.coli 1 3 la radiologia medica ( 2019 ) 124 : 11851198 1193 wall thickening is associated with mural stratification ; in the acute phase , the water halo sign is frequently encountered on cect , even if non - specific [ 24 ]  . 
submucosal edema and pericolonic soft tissue changes with dilatation and engorgement of the vasa recta ( comb sign ) are other important additional findings ( fig.8 ) [ 53 ]  . 
fatty proliferation of the mesentery and the presence of pericolic lymphadenopathy are very suggestive of cd [ 24 , 54 ] ; on the other side , proliferation of perirectal fat with enlargement of pre - sacral space is more often seen in uc , even if non - specific [ 14 , 53 ]  . 
radiographs show a total or segmental distension of the colon ( > 6cm in the transverse colon ) with a loss of haustral folds [ 56 , 58 ]  . clinical presentation in association with family history can suggest the diagnosis . 
even in acute onset , the presence of antecedent rectal bleeding is an important clue for the diagnosis [ 11 , 54 ]  . evolution ofclostridium difficile infection with successful therapy , symptomatic improvement is generally observed after 12days , while diarrhea takes more time to resolve ( usually 36days ) [ 59 ]  . 
in case of complicated cdi , ct scan of the abdomen and the pelvis should be performed to determine whether perforation or toxic megacolon is present [ 60 ]  . 
progression to toxic megacolon should be suspected in case of rapid abdominal distension and lessening of diarrhea due to paralytic ileus ; the diagnosis requires radiological proof of colonic dilatation ( diameter of transverse colon > 6cm ) in the presence of signs of severe systemic inflammatory response [ 62 , 63 ]  . today cdi is essentially a medical disease , and surgical intervention is generally not required [ 60 , 63 ]  . 
8 inflammatory colitis : circumferential wall thickening in a patient with cd in the acute phase ( coronal image a , sagittal image b and coronal with zoom image c ; white arrows ) ; associate findings such as engorgement of the vasa recta ( i.e. , comb sign ) ( b , c ; dashed arrows ) and the presence of mesenteric lymphadenopathy ( coronal with zoom image d ; black arrow ) are often important clues for the diagnosis 1 3 1194 la radiologia medica ( 2019 ) 124 : 11851198 fig . 
9 evolution of clostridium difficile infection : colonic wall thickness ( white arrows ) and pericolic free fluid ( dashed arrows ) at the time of diagnosis of cdi ( a , b ) and 7days after the start of medical therapy ( c , d ) ; the decrease in wall thickness and pericolic and free fluids is evident intervention . 
the following parameters were recorded : wall thickness , extent of colon abnormalities , caliber of the largest portion of the colon , presence / absence of the accordion sign and target sign , the degree of pericolonic stranding and ascites , presence / absence of pleural effusion and subcutaneous edema . 
 none of the parameters evaluated significantly differs in comparison with nonsurgical control group , and cect findings are not necessarily correlated with the severity of the disease [ 64 ]  . 
no statistical correlation was found between cect findings and clinical parameters and none of the cect parameters evaluated was useful to predict the need for surgical intervention [ 65 ]  . 
 in the series by boland etal . , nodular haustral thickening ( including the accordion pattern ) was the only imaging finding that correlated with the severity of the disease , being significantly more frequent in patients with elevated wbc ( > 11.000 / mm3 ) regardless of the extent of colonic involvement [ 23 ]  . 
 reported that increased colonic wall thickness ( 11mm ) and the presence of pleural effusion were independently associated with an increased likelihood of developing complicated cdi [ 27 ]  . conclusion although the confirmation of the diagnosis is based on the demonstration of toxigenic c . 
difficile toxins by stool test , cect is a useful examination to raise the suspicion of 1 3 la radiologia medica ( 2019 ) 124 : 11851198 1195 1 3 1196 la radiologia medica ( 2019 ) 124 : 11851198 clostridium difficile colitis and to evaluate the extension of the disease as well as of possible complications . 
although colitis of other origins can occasionally mimic the cect appearance of cdi , the degree of wall thickening , the extension and location of colonic involvement and the presence of associated extracolonic findings , especially in patients with a recent history of antibiotic use and healthcare exposures , are important points of differential diagnosis . 
inclusion criteria were : preoperative mr including diffusion - weighted imaging ( dwi ) and perfusion dynamic contrast - enhanced ( dce ) sequence ; cytoreductive surgery performed within a month from mr ; and minimum follow - up of 12months . 
dwi parameters included apparent diffusion coefficient ( adc ) of the largest ovarian mass ( o - adc ) and normalized ovarian adc as a ratio between ovarian adc and muscle adc ( m - adc )  . 
none of the other functional parameters showed either difference between r0 and r1 patients or association with pfs in the first 12months . conclusions this preliminary study demonstrated a slightly significant association between normalized ovarian adc and the presence of residual tumor at surgery . 
 in the usa , oc ranks as the second most common female * stefania rizzo stefania.rizzo@eoc.ch 1 postgraduate school ofradiodiagnostics , universit degli studi di milano , via festa del perdono 7 , 20122milan , italy 2 department ofradiology , aslvc , corso mario abbiate 21 , 13100vercelli , italy 3 division ofepidemiology andbiostatistics , ieo european institute ofoncology irccs , milan , italy 4 department ofgynecology , ieo european institute ofoncology irccs , via ripamonti 435 , 20141milan , italy genital cancer , and the first cause of death from gynecological malignancies , with estimated new cases and deaths for 2019 of 22530 and 13980 , respectively [ 2 ]  . 
standard treatment for oc patients consists of primary cytoreductive surgery followed by six cycles of platinum - based chemotherapy 5 department ofoncology andhemato - oncology , universit degli studi di milano , milan , italy 6 department ofradiotherapy , ieo european institute ofoncology irccs , via ripamonti 435 , 20141milan , italy 7 department ofradiology , ieo european institute ofoncology irccs , via ripamonti 435 , 20141milan , italy 8 clinica di radiologia eocistituto imaging della svizzera italiana , via tesserete 47 , 6900lugano , switzerland vol . : ( 0123456789 ) 1 3 1316 la radiologia medica ( 2019 ) 124 : 13151323 [ 3 ]  . 
no residual tumor at surgery is still the most important prognostic factor because of a demonstrated inverse relationship between the extent of residual disease and patient survival [ 4 ]  . in some cases , tumor spread may not allow the complete resection of disease , or it may require a very aggressive approach that might trigger important postoperative complications . 
these cases are usually sent to three or more cycles of neoadjuvant chemotherapy and subsequent interval debulking surgery followed by adjuvant chemotherapy [ 4 ]  . according to the european society of urogenital radiology guidelines , preoperative staging of oc is based on computed tomography ( ct ) [ 5 ] , whereas magnetic resonance ( mr ) is reserved to patients that may not undergo a contrast - enhanced ct . 
nevertheless , recent studies have demonstrated that mr including diffusion - weighted imaging ( dwi ) may predict the extent of disease better than ct in oc patients , thus offering a better prediction of the outcome of cytoreductive surgery [ 6 ]  . 
moreover , several recent studies have focused on functional quantitative parameters derived from mri , such as dwi and dynamic contrastenhanced ( dce ) perfusion [ 710 ] , suggesting that a combination of functional and morphologic information may represent a powerful tool for improving preoperative staging as well as for response assessment [ 1113 ]  . dwi depicts molecular diffusion , mainly measuring the cellularity within a tissue based on the movements of water protons in the extracellular space . 
dce perfusion parameters assess the microvascular environment within a lesion , taking into account the permeability of vessels and giving the opportunity to quantify the extravascular space , the intravascular space and the movements of blood between each of thesome authors have investigated the use of mri perfusion in gynecological malignancies , such as for the detection of uterine cervical cancer , for staging of endometrial cancer and for characterization of adnexal masses [ 9 ]  . to the best of our knowledge , no previous study has investigated the role of mr functional imaging techniques for prediction of outcome of oc patients . therefore , the first purpose of this study was to evaluate whether the dwi and dce quantitative parameters derived from staging mr in oc patient may be associated with the presence of residual tumor at surgery ; secondary purpose was to assess whether the above - mentioned functional sequences may predict progression free survival ( pfs ) in the first 12months after surgery . materials andmethods patients selection this prospective study includes patients affected by oc who underwent cytoreductive surgery after a whole - body mr for preoperative staging at our institution between april 2016 and july 2017 . 
 inclusion criteria consisted of surgery performed at our institution within 1month from mri , high - grade serous oc histological type , preoperative mr including dwi and dce quantitative perfusion sequences and minimum follow - up of 12months . 
exclusion criteria were : lack of a proper follow - up ; mr performed after neoadjuvant chemotherapy ; and mr examination performed on a different mr machine . the following patients characteristics were retrieved : age at surgery ; body mass index ; surgical staging according to the international federation of gynecology and obstetrics ( figo ) ; presence of residual tumor ( rt ) at surgery , indicated as r0 = no rt or rt smaller than 10mm ; r1 = rt higher than 10mm ; date of last visit ; and status ( relapse or not )  . 
afterward , dce imaging sequence was acquired before , during and after injection of a gadolinium chelate ( gadoteric acid ) , at a dose of 0.2ml / kg and rate of 3ml / s . 
images were obtained sequentially at 15 - s intervals for 315s . dwi measurements the adc measurement was taken on a four - view display , by uploading the t2 images of the pelvis as morphologic images , the b = 0 dw images that most closely reflect the t2 images , thus allowing an evaluation of the entire tumor diffusion , and the adc maps . 
a radiologist with 15years of experience in gynecological radiology traced freehand twodimensional ( 2d ) regions of interest ( rois ) on the largest ovarian mass including the most large solid component ( excluding cystic components , if present ) on the b = 0 diffusion - weighted images , and then applied to the corresponding image in the adc map . 
subsequent adc of ovarian masses ( o - adc ) and adc of ovarian mass normalized to the muscle ( m - adc ) were calculated . dce measurements a radiologist ( sr ) with 15years of experience in gynecological radiology placed a volume of interest ( voi ) on the solid part of the largest ovarian mass ; each voi was elaborated by a specific tool ( geniq , ge healthcare ) , which is a software application running on aw ( advantage workstation tm ) on the volumeshare platform , where quantitative functional data about the tissue flow , permeability and contrast leakage from the vascular space into the extravascular extracellular space ( ees ) were collected . 
specifically , the following parameters , whose definitions are shown in table1 , were table 1 definitions and units of geniq map parameters geniq map definition included for analysis : bolus arrival time ( bat ) area ; contrastenhancement ratio ( cer ) area ; initial area under the gadolinium concentration time curve ( iaugc ) ; rate transfer constant of gadolinium from the extravascular to the vascular space ( kep ) ; volume transfer constant from vascular space to extravascular and extracellular space ( ktrans ) ; maximum slope of increase area ( msl ) ; volume of extracellular and extravascular space ( ve ) ; and intracellular space ( int )  . statistical analysis distribution of o - adc and normalized m - adc was described using mean and standard deviation . 
difference in o - adc and normalized m - adc between groups of patients with different characteristics was assessed with the student t test and also using the nonparametric median test . 
all p values were two - sided , and those < 0.05 were considered statistically significant . results this study included 49 patients with high - grade serous oc ( mean age at diagnosis 58years , range 4178 )  . 
rt after surgery was present in 8 / 49 patients ( 16% ) ( table2 )  . an example of the extraction of dce quantitative parameters by the geniq tool used in this study is shown in fig.1. the analysis evaluating o - adc and normalized m - adc according to patients characteristics did not demonstrate significant association , as shown in table2 . pfs curve for 40 patients with r0 disease and available follow - up is shown in fig.2. 
1 an example of the extraction of dce quantitative parameters by the geniq tool used in this study 1 3 1320 la radiologia medica ( 2019 ) 124 : 13151323 our results show that the value of normalized ovarian adc imaging at preoperative mri may be associated with the risk of residual tumor at surgery . 
the association of adc values with clinical outcome is concordant with previous studies , demonstrating that adc values increased the precision of diagnosis and helped to predict the prognosis as a therapeutic response [ 22 ]  . 
a recent study has also shown that the adc value was associated with histological severity of oc and predicted the clinical outcome : namely , low adc values were associated with traditional histopathological prognostic markers , such as poorly differentiated tumors , high ki - 67 expression and vegf receptor expression [ 23 ]  . many studies are in support of the use of perfusion dce sequences , especially in the field of oncology . 
indeed , dcemri enables noninvasive characterization of tissue vasculature , blood volume and permeability , thereby providing information about tumor angiogenesis , which is essential in the development and metastatic dissemination of malignant tumors [ 24 ]  . 
dce analysis may include qualitative semiquantitative and quantitative measures [ 24 , 25 ]  . in gynecological malignancies , semiquantitative analysis , referring to an analysis of kinetics of the curve of contrast enhancement , has been suggested in cervical cancer as an useful tool to predict percentage tumor regression after nonsurgical therapy [ 7 ] ; in endometrial cancer for the detection of small tumors , and in combination with t2w images and dwi to better evaluate deep myometrial invasion [ 13 , 26 ] ; and in the evaluation of complex adnexal masses undetermined at ultrasound as an adjunctive sequence to dwi for characterization [ 27 ]  . on the other hand , quantitative measures are complex but most generalizable and standardized [ 25 , 28 ]  . 
these measures refer to a two - compartment model where the extracellularextravascular space ( ees , tissue ) and the capillary vascular plasma can be considered two compartments that are individually well mixed . 
dce - mri can generate quantitative parameters such as the volume transfer coefficient , ktrans between blood plasma and ees , the volume of the ees , ve , and the rate constant between ees and blood plasma , kep . 
therefore , many previous papers have hypothesized scoring systems or other methods to predict the outcome of cytoreductive surgery [ 1519 ]  . for the evaluation of ovarian masses , mr is considered helpful in evaluating the location , size and nature of the ovarian lesion , as well as in determining the response to treatment [ 20 ]  . 
besides the usual morphologic sequences , functional sequences such as dwi and dce , which are able to offer semiquantitative or quantitative information , have been introduced for use in different clinical settings and / or research settings [ 8 , 11 ]  . dwi displays information about water mobility , tissue cellularity and the integrity of the cellular membranes . 
the quantitative parameter adc is derived from the exponential attenuation of signal intensity between at least two b values and represents the gradient of the signal intensity logarithm line produced between two b values . 
the adc value describes microscopic water diffusibility and is decreased in the presence of factors that restrict water diffusion , such as the cell membrane and the viscosity of the fluid [ 10 , 12 ]  . 
despite its recognized value in diagnosing and monitoring of disease , there is some controversy in the literature regarding the limited reproducibility of adc estimates across different imaging platforms and imaging sites . 
the lack of significance of the dce quantitative parameters may be related to the small group of patients evaluated as well as to the inclusion of a single histological type ( high grade serous oc ) that may show similar behavior in terms of angiogenesis and vasculature . this study has several limitations . 
however , the patients included in this study are part of an undergoing prospective clinical trial , aiming to assess whether wholebody mr may perform preoperative evaluation of oc patients better than ct . 
we have decided to perform this ad interim analysis to assess the overall performance of quantitative dce imaging on the ovarian mass , in order to decide whether this sequence was worthy of an adjunctive time , especially for those patients uncomfortable with the duration of the mr examination . 
 however , we included only patients undergoing surgery at our institution , which is a third referral center for oc treatment ; therefore , we can assume that surgeons with comparable technical skills and experience operated all patients . 
 moreover , the percentage of patients with rt at surgery may appear low to evaluate data trend ; however , since the percentage of rt in this study ( 16% ) is comparable to the one reported in the literature , an increase in the patients number would have not changed this proportion . 
 however , the relapse within the first 12months is an important clinical endpoint for oc patients because it is the basis to define the platinum resistance of patients . in conclusion , in this study we demonstrated a slightly significant association between m - adc and the presence of residual tumor at surgery , whereas dwi - related parameters and dce perfusion quantitative parameters did not show association with residual tumor at surgery and pfs in the first 12months . 
these results may suggest that dce perfusion parameters in oc patients undergoing mr for staging are not needed for the prediction of outcome . acknowledgements we hereby thank antonello vidiri for sharing his knowledge about the use of the software tool for quantitative dce analysis . 
the recent developments in ct technology with the introduction of the third - generation dual - source ( ds ) dual - energy ( de ) ct scanners well suited to respond to these challenges . 
 the aim of this article is to describe the state - of - the - art in dsct protocol with de technology in pediatric chd patients , providing some case examples of our experience over an 18 - month period . keywords dual - source ct dual - energy ct congenital heart disease pediatric patients state - of - the - art introduction congenital heart disease ( chd ) is the most common inborn pathology with an incidence of 1% and a prevalence of 810 per 1000 live births . 
 table1 shows the main chds . imaging assessment of pediatric chd patients is challenging for the wide spectrum of disease and complex congenital defects , high heart rates , motion artifacts from cardiac and respiration movements and limited patient cooperation . 
imaging modalities for evaluating chd in pediatric patients include echocardiography , conventional invasive angiography , magnetic resonance imaging ( mri ) and computed tomography ( ct ) [ 2 , 3 ]  . 
despite these advantages , the high heart rate , the use of ionizing radiation and the limited patient cooperation are limiting factors and ct is not the modality of choice for imaging in pediatric patients [ 5 ]  . 
however , the development in ct technology with the introduction of the third - generation dual - source ( ds ) dualenergy ( de ) ct scanners well suited to respond to these challenges [ 6 ]  . the aim of this article is to describe the state - of - the - art in dsct protocol with de technology in pediatric chd patients to obtain high - quality images with low radiation dose , providing some case examples of our experience over an 18 - month period . technical parameters * marco fogante marco.fogante89@gmail.com 1 radiology department , azienda ospedaliero universitaria ospedali riuniti , 60126ancona , italy third - generation dsct scanner uses two x - ray tubes working at the same energy ( single - energy ) or at different energy ( de )  . 
two x - ray tubes are placed approximately at 95 to each other and can work at high ( from 120 to vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 12381252 1239 table 1 clinical classification of congenital heart diseases table 2 technical parameters of third - generation dual - source dualenergy ct scanner acyanotic heart disease increased pulmonary venous flow ( pulmonary edema ) hypoplastic left heart aortic coarctation interrupted aortic arch congestive heart failure neonatal sepsis increased pulmonary arterial flow ( shunt vascularity ) atrial septal defect ventricular septal defect patent ductus arteriosus atrio - ventricular canal defect cyanotic heart disease decreased pulmonary vascularity with cardiomegaly ebstein anomaly decreased pulmonary vascularity without cardiomegaly tetralogy of fallot usually increased pulmonary vascularity without cardiomegaly transposition of great arteries truncus arteriosus tricuspid atresia partial / total anomalous pulmonary venous return single ventricle 150kv ) and at low ( from 70 to 100kv ) energies [ 79 ]  . 
 third - generation ds systems have a tin filter in front of the high - energy tube , that attenuates lower energy photons , thereby increasing the difference of spectral energy . 
the fov of the low - energy tube is 50cm , whereas the fov of the highenergy tube is 35cthe potential disadvantage of the fov of the smaller tube is the evaluation of the structures located peripherally in larger patient . 
third - generation ds - dect allows a submillimeter spatial resolution of the heart and coronary arteries in one or a few heartbeats , a high temporal resolution , a radiation dose reduction with high - pitch values and low tube voltage , new algorithms of iterative reconstruction , and provides additional clinical information with de technology . 
thirdgeneration dsct makes possible to scan non - cooperative pediatric patients with minimal sedation , free breathing and without - blockage of heart rate , even to heart rate around 140beats / mthe highest temporal resolution should be used to minimize motion artifacts . 
nevertheless , beta - blockers are safe in pediatric patients without contraindications and should be considered if high - definition imaging is required because image quality remains heart - pulse - dependent [ 21 ]  . contrast injection third - generation dsct allows contrast volume saving , because using a low tube voltage ( 70kv ) x - rays generated have an average energy close to the k - edge of iodine ( 33.2kev ) , improving contrast enhancement . 
moreover , the fast scan protocol provides precise shaping and timing 1 3 1240 la radiologia medica ( 2019 ) 124 : 12381252 of the contrast peak enhancement for optimal intravascular attenuation and allows reducing contrast volume [ 22 ]  . 
for these reasons , keeping the iodine delivery rate constant , contrast medium ( cm ) with low iodine concentration ( 300mgi / ml ) showed a higher vascular enhancement than cm with high iodine concentration ( 400mgi / ml ) , allowing iodine load reduction . 
intravenous line size ranging from 24 - gauge in neonates to 18 - gauce in older children , with flow rates between 0.5 and 5ml / s and pressure settings of 50300lb per square inch ( psi )  . 
central venous catheter might be used in critically pediatric patient , but it allows for adequate injection in children with age less than 1 - year because maximum flow rate is 0.41.2ml / s and maximum pressure value is 2550 psi . 
the triphasic approach consists of a two - phase contrast administration ( about half at the regular rate plus the remainder either at a slower rate ) followed by saline with slower flow rate . 
 this method should be used for the assessment of complex cardiovascular disease to obtain simultaneous evaluation of right and left - side structures [ 24 , 25 ]  . scan timing scan time can be decided with three different techniques : fixed - time , bolus - test and bolus - tracking . 
the site of cannulation and scan protocol must be considered ; an extra delay of 24s should be added when injecting from the leg and when using shorter scan methods . 
nevertheless , this technique is prone to inaccuracy and it is challenging because it is limited reproducibility from the different time of contrast transit for anatomical , functional and technical reasons [ 26 ]  . bolus - test technique consists of calculating vascular peak enhancement time of a small contrast volume by monitoring cm transit on a selected slice . 
this method involves additional cm and radiation and it is not routinely applicate in children [ 27 ]  . bolus - tracking technique is the most useful in pediatric patients . 
when is necessary the visualization of the cardiac chambers and the descending aorta in the same plane , the region of interest could be placed within the left ventricle and the trigger threshold should be set 100 hu . 
 visual start should be used with restless patients because with automatic approach , the movements of the patient during the bolus measurement can cause to start too early or too late . 
to reduce radiation exposure , monitoring should start at the end of contrast injection and should be reduced in frequency ( one each second ) , and tube voltage should be reduced ( 70kv ) [ 28 ]  . scan protocol the scan range should include the heart , the thoracic aorta and the pulmonary arteries . the scan acquisition can be non - electrocardiogram ( ecg ) - synchronized or ecg - synchronized . nonecgsynchronized acquisition non - ecg - synchronized acquisition should be used when the diagnostic purpose concerns extra - cardiac anatomy . 
 the high temporal resolution allows for good quality imaging of extra - cardiac structures because they are less sensitive to heart motion than the heart itself [ 29 ]  . 
 moreover , respiratory artifacts are responsible for imaging degradation and non - synchronized acquisition is obtained more quickly than synchronized acquisition , and thus is responsible for fewer respiratory artifacts [ 30 ]  . 
finally , synchronized acquisition requires a much higher radiation dose than non - synchronized acquisition because the exposure time is longer due to low pitch acquisitions [ 31 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 12381252 1241 fig . 
the main acquisition modes include : prospective ecg - triggered high - pitch spiral , prospective ecg - gated sequential , and retrospective ecg - gated spiral [ 33 ]  . prospective ecg - triggered high - pitch spiral mode should be used in uncooperative patients because it reduces respiratory and cardiac motion artifacts , as well as the need for sedation and general anesthesia . 
this mode uses two x - ray tubes to achieve both maximum temporal resolution and z - axis scan speed , resulting in rapid and large gapless non - overlapping imaging in a single heartbeat . 
the length of the rr interval in pediatric patients is around 500ms at a heart rate of around 120 beats / man ecg - triggered high - pitch scan with a 12cm scan length takes up to 130ms . 
mostly , only information on the anatomy is required and not the rule out of coronary artery disease as in adults , providing sufficient diagnostic image quality [ 34 ]  . prospective ecg - gated sequential mode should be used in cooperative patients with irregular heart rate . 
this mode allows to increase the percentage of the cardiac cycle phase acquired ( from 30 to 60% of the diastolic phase ) , to select the ecg phase without motion artifacts , and avoid nondiagnostic scans [ 35 ]  . 
an issue of prospective ecg - gated sequential mode is the possibility of a stack artifact when scanning a larger length in the z - axis than the collimation width . 
in children , because the length of the z - axis is not elevated and the focus is mainly on anatomy assessment , the stack artifacts can be less problematic [ 36 ]  . retrospective ecg - gated spiral mode should be use with very irregular heart rate where the need for ecg editing is expected , or when the functional cardiac information could be necessary . 
this technique loses efficiency at higher heart rate because of less efficient slope - up time and slope - down time of the ecg - based tube current modulation [ 37 ]  . de clinical applications de clinical applications in pediatric chd patients include better evaluation of vascular structures and shunts , assessment of the myocardial and lung perfusion and reduction in metal artifact . 
the post - processing techniques that best exploit the advantages of de in chds are material decomposition and virtual mono - energetic [ 38 ]  . material decomposition allows discriminating structures based on attenuation characteristics at different energy levels . 
the system uses three - material decomposition algorithm in the image - space domathe three materials used for material differentiation in pediatric chd are soft tissue , calcium , and iodine . 
type a interrupted aortic arch , after the left subclavian artery origin , with a gap between the ascending and descending thoracic aorta , in sagittal ( a ) and coronal ( b ) views ( yellow arrows )  . 
iodine overlay images allow quantitative evaluation of iodine content , a reference region is placed in an area of maximum contrast enhancement and another region of interest in placed in the target area of a contrast materialenhanced image . 
because absolute threshold values for increased or decreased iodine content have not been defined and iodine measurements may vary among vendors , the quantitative analysis is best performed by assessing relative contrast enhancement values [ 40 ]  . 
another application is the evaluation of myocardial perfusion , which provides the myocardial iodine distribution during the first pass arterial enhancement and can detect myocardial blood supply [ 41 ]  . 
medium smooth convolution kernel should be used with a low - intermediate strength [ 49 ]  . dsct , electrocardiogram ; bv , body vascular ; ctdivol , volume computed tomography dose index ; dlp , dose length product ; ssde , sizespecific dose estimates postprocessing application allows assessing qualitative and quantitative lung perfusion . 
dect may be an efficient method to assess perfused lung blood volume in chds , such as pulmonary atresia , arteriovenous malformations and tetralogy of fallot [ 42 ]  . 
 these perfusion defects correlate with increased right - toleft shunt and combined with the morphologic analysis can improve detectability of the cyanotic chd [ 43 ]  . virtual mono - energetic allows reconstruction of virtual images that simulate the attenuation values of an image acquired by using a single - energy value . 
these values reduce metal and beam - hardening artifacts from injected cm in the subclavian vein , axillary vein , or superior vena cava [ 45 , 46 ]  . for extra - cardiac structures evaluation are necessary multi planar reformations in sagittal and coronal planes . 
volume rendering reconstructions are necessary for a tridimensional overview of cardiac and great vessel anatomy [ 50 , 51 ]  . radiation dose radiation dose reduction in pediatric patient is important because organ sensitivity to radiation is much higher than in adults , and a risk of developing cancer in the future cannot be totally ruled out . 
using this protocol , radiation exposure is estimated to be less than 1msv , which is equivalent to the dose delivered by natural radiation over a 6 - month period [ 54 ]  . 
retrospective ecg - gated scan mode provides from 2 to 4msv [ 55 , 56 ]  . concerning dect in the pediatric population , in the few prior publications , the radiation exposure level from dect is equivalent to or even less than that of a comparable single - energy examination [ 57 ]  . 
moreover , dect scanners can generate virtual non - enhanced images , which have the potential to reduce radiation exposure by eliminating the need for a true nonenhanced acquisition [ 58 , 59 ]  . case examples clinical indications for cardiac ct in the pediatric population with chds cover a wide spectrusome case examples are provided , all acquired on a dsct scanner with la radiologia medica ( 2019 ) 124 : 12381252 de technology ( somatom force , siemens heathineers , forchleim , germany )  . hypoplastic left heart syndrome hypoplastic left heart syndrome ( hlhs ) comprises a wide spectrum of cardiac malformations , including hypoplasia or atresia of the aortic and mitral valves and hypoplasia of the left ventricle and ascending aorta . 
hlhs is the fourth most common cardiac malformation to manifest in the first year of life behind ventricular septal defect , transposition of the great arteries , and tetralogy of fallot . 
however , the recent evolution of palliative surgical procedures has increased the survival rate in children with these malformations [ 60 ]  . ct has become a valuable modality in evaluating the complex anatomic findings associated with hlhs . 
ct provides information for surgical planning , include location and size of the hypoplastic ascending aorta , and post - surgical assessment , such as the modified fontan procedure , a lateral tunnel created within or near the right atrium to direct blood from the inferior vena cava to the right pulmonary artery to reduce patient cyanosis [ 61 ]  . 
ct protocol and radiation dose are summarized in table3 . interrupted aortic arch withpatent ductus arteriosus interrupted aortic arch ( iaa ) accounts for approximately 1.5% of all chds and 15% of iaa patients have digeorge syndrome . 
 according to the site of interruption , three different types are described : type a ( 30% ) , the interruption is distal to the origin of left subclavian artery ; type b ( 43% ) , the interruption is between the left carotid and left subclavian arteries and digeorge syndrome is reported in about 50% of patients ; type c ( 17% ) , the interruption is between the innominate and left carotid arteries . 
bicuspid aortic valve occurs in 60% of all cases , sub - aortic stenosis occurs in about 20% , and truncus arteriosus in about 10% [ 62 ]  . ct has become a valuable modality in evaluating the complex anatomic findings associated with iaa . 
ct can be used to evaluate the type and the level of iaa , the pda , the aortic valve and potential post - surgical complications [ 63 ]  . 
large ventricular septum defect ( a ) , anterior shift of the aorta over the ventricular septum defect ( b ) , right ventricular outflow tract obstruction with pulmonary artery atresia and dextro - position of the aortic arch ( c )  . 
ct protocol and radiation dose are summarized in table4 . ebstein anomaly ebstein anomaly ( ea ) accounts for < 1% of all chds with an equal distribution between male and female . 
as a consequence of this apical and anterior displacement of the tv functional orifice , functionally rv is variably hypoplastic ; the myocardium above the orifice becomes atrialized and , thus , thin and dysfunctional ; the myocardium below the orifice typically possesses a more normal ventricular wall thickness but is still dysfunctional . 
the rv impairment and the tv regurgitation decrease forward flow across the pulmonary valve reducing systemic cardiac output and increase right atrial dimensions and pressure thus favoring a right - to - left shunt through the interatrial communication ; cyanosis depends upon the rightto - left shunting [ 64 ]  . ct has become a valuable modality in evaluating the complex anatomic findings associated with ea . 
ct protocol and radiation dose are summarized in table5 . tetralogy offallot tetralogy of fallot ( tof ) occurs in 10% of all chds and is the most common cyanotic defect seen in children beyond infancy . 
it involves the following four anatomic abnormalities of the heart : large ventricle septal defect ( vsd ) , anterior shift of the aorta over the vsd ( overriding aorta ) , rv outflow tract ( ot ) obstruction , and rv hypertrophy . 
tof and pulmonary atresia with vsd occurs in approximately 1520% of all tetralogy cases and the pulmonary supply is most commonly mediated through a pda ( 70% ) and less commonly through major aorto - pulmonary collateral arteries ( mapcas ) ( 30% ) [ 66 ]  . ct has become a valuable modality in evaluating the complex anatomic findings associated with both unrepaired and repaired tof patients . 
ct can be used to evaluate the rvot obstruction , the aortic root anatomy and the overriding aorta , the vsd , the pda , the mapcas , the patency of surgical palliative shunt placement and for long - term sequelae and complications . 
ct protocol and radiation dose are summarized in table6 . transposition ofthegreat arteries transposition of great arteries ( tga ) accounts for 25% of all chds with a prevalence of about 0.20.3 of 1000 births ; it is more common in males than in females with a ratio of 23 : 1 . 
it derives from truncal ridge and infundibulum normal spiraling rotation failure during fetal life which results in discordant ventriculo - arterial connection : aorta arises from the morphologically right ventricle ( rv ) and is located anteriorly and to the right of pulmonary artery ( pa ) ( d - transposition ) , whereas the pa arises from morphologically left ventricle ( lv )  . 
during neonatal period , patent ductus arteriosus ( pda ) and mainly patent foramen ovale ( pfo ) usually maintain an adequate mixing because they ensure the effective systemic / pulmonary blood flow going , respectively , into the aorta and the pa ; as the pda starts to close and pfo by itself is restrictive in size , infant develops severe cyanosis [ 69 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 12381252 1249 fig . 
 volume rendering reconstructions in superior view with ( e ) and without aorta ( f ) ct has become a valuable modality in evaluating the complex anatomic findings associated tga . 
ct can be used to evaluate the origin and course of the great arteries , the presence and size of the pda and / or pfo , and any associated anomalies such as lvot obstruction and aortic coarctation [ 70 ]  . 
ct protocol and radiation dose are summarized in table7 . conclusion dsct with de technology is an important low - invasive diagnostic tool for the evaluation of chd in pediatric patients , providing relevant information for optimal surgical management . 
then , we selected retrospectively , among the 1500 patients underwent to cedm at the breast diagnostics department of the careggi university hospital of florence and the national cancer institute of milan from september 2016 to november 2018 , 31 women ( mean age 57.1 aa ; range 4178 aa ) with a definitive histological diagnosis of ilc . 
specificity in the characterization of additional lesions was 66.7% , and the diagnosis of the extension of disease was correct in 77.4% of cases : nme also led to a decrease in diagnostic accuracy in the evaluation of disease extension up to 40% versus 85% for masses and 80% for masses associated with nme ( m / nme )  . 
moreover , in 12 / 31 ( 38.7% ) , cedm allowed to correctly identify lesions not shown by mammography + ultrasonography + tomosynthesis : in the half of these ( 6 / 12 ) , there was a multicentricity , thus allowing an adequate surgical planning change . 
cedm was also very accurate in analyzing the maximum diameter of the masses , while it was much less reliable in the case of the m / nme and pure nme . 
 in conclusion , cedm is a new promising imaging technique in the loco - regional preoperative staging and in the evaluation of disease extension for ilc , especially in case of mass enhancement lesions . keywords breast contrast - enhanced digital mammography contrast - enhanced spectral mammography invasive lobular breast cancer breast cancer staging * giulia bicchierai giulia.bicchierai@gmail.com 1 department ofradiology , university ofpalermo , palermo , italy 2 diagnostic senology unit , azienda ospedaliero - universitaria careggi , largo g . 
brambilla 3 , 50134florence , italy 3 general management staff , azienda ospedaliero - universitaria careggi , florence , italy 4 breast imaging unit , fondazione irccs istituto nazionale 5 department ofradiology , azienda ospedaliero - universitaria dei tumori , milan , italy careggi , florence , italy introduction invasive lobular carcinoma ( ilc ) is the second most frequent invasive breast cancer ( 515% ) after ductal histotype ( idc ) ( 7090% ) , compared to which is more difficult to diagnose by mammography and ultrasonography and has a greater tendency to multifocality , multicentricity or bilaterality [ 14 ]  . 
then , magnetic resonance imaging ( mri ) is recommended from international guidelines in the preoperative work - up for all ilc patients , thanks to its high sensitivity ( 9598% ) , also in detecting of adjunctive lesions in the ipsilateral or contralateral breast , not previously identified with mammography or us , not even with the most recent advances in these diagnostic techniques [ 514 ]  . 
recently , contrast - enhanced digital mammography ( cedm ) has shown a similar sensitivity and an even greater specificity vol . : ( 0123456789 ) 1 3 1230 la radiologia medica ( 2019 ) 124 : 12291237 compared to mri , in the detection of breast lesions , both for index lesions and for possible additional lesions , with lower costs , greater rapidity , greater patient compliance , especially in the claustrophobic , greater availability , and with the possibility to verify if microcalcifications have contrast enhancement , thanks to the perfect correspondence between full - field digital mammography ( ffdm ) and cedm images [ 1521 ]  . 
the aim of our study was to assess the performance of cedm in the preoperative loco - regional staging of ilc patients , about the valuation of the extension of disease and in measurement of lesions . 
we also calculated the distribution of frequencies of various histological parameters ( i.e. , positivity to the receptor for estrogens , positivity to the receptor for the progesterone , ki67 , her - 2 positivity ) in our sample . 
 cedm technique cedm was performed using a selenia dimensions mammography system ( hologic , marlborough , ma ) capable of performing full - field 2d digital mammography , 3d tomosynthesis and cedm ( high and low energy )  . 
an intravenous injection of 1.5ml / kg body weight of an iodinebased contrast agent ( ultravist 370 , bayer healthcare llc , whippany , nj ) was administered with an automated bolus injection with a flow of 3ml / s , followed by 20ml of saline solution . 
1 flow chart of patient enrollment cedm image , 2 acquisitions were performed at 2631kvp with rhodium and silver filters ( rh and ag ) for low - energy acquisition , and at 4549kvp with a copper filter for high acquisition power . 
a recombination algorithm was used to subtract the non - enhanced breast tissue , and then to provide a subtracted image in which only the areas of post - contrastographic enhancement were highlighted : this will allow to evaluate the neoangiogenesis of the tumor , as in mri . 
 acquisitions in both standard projections ( cc and mlo ) , carried out also 8min after the administration of the contrast medium , also make it possible to carry out a qualitative assessment of the enhancements kinetics . 
 [ 22 , 23 ] imaging interpretation andhistological parameters two different radiologists , with more than 30years of experience in breast imaging in the two different hospitals , performed ultrasonography and analyzed mammograms and tomosynthesis of the 31 patients of our study ( of which they knew the medical history ) , according to bi - rads criteria established by the american college of radiology ( acr )  . 
as in mri , cedm classifies all 31 index lesions detected in the subtracted images into three main groups : focus , mass and non - mass enhancement ( nme ) ; we also included a further category , called m / nme , when the index lesion is composed by a mass closely associated with a nme component . 
according to the bi - rads , they analyzed morphological and kinetics findings of the enhancement of lesions and valuated the number of lesions and then the extension of the disease . 
the two radiologists measured the maximum diameter of index lesions at cedm : in case of m / nme , they measure the maximum diameter of the sum of the two components . 
 statistical analysis we calculated cedm sensitivity and specificity in detecting of adjunctive lesions and the accuracy in assessing the local extent of disease first in the total of the sample and then for the various subgroups , divided for type of contrast enhancement ( masses , nme and m / nme )  . 
then , we have analyzed if and how cedm sensitivity , specificity and accuracy in assessing of the local extent of disease were influenced by the different types of contrast enhancement . 
regarding the dimensional analysis of index lesions , mean , median , standard deviation and the ranges of their measurements on the entire sample and in the subgroups were calculated . 
 the blandaltman plot was used to explore the agreement between cedm index lesion measurements and histology ( gold standard ) , and the intraclass correlation coefficient ( icc ) was calculated [ 31 , 32 ]  . 
freemanhalton extension of fishers exact probability test was used to verify any significant differences between the masses , nme , m / nme , in the distribution of lesion histological parameters . 
the index lesion occurred in 20 / 31 ( 64.5% ) of the cases like a mass , in 6 / 31 ( 19.3% ) like nme , in 5 / 31 ( 16.1% ) t 1 3 la radiologia medica ( 2019 ) 124 : 12291237 1233 like a m / nme , in 0 / 31 ( 0% ) like focus , and the distribution of their enhancement features is described in tab.1. cedm , additional lesions , extension ofdisease andhistological parameters in 12 / 31 ( 38.7% ) , cedm allowed to correctly identify lesions not shown by mammography + ultrasonography + tomosynthesis : in the half of these ( 6 / 12 ) , there was a multicentricity , thus allowing an adequate surgical planning change [ 3338 ]  . 
other histological features are shown in tab.3 : they were correlated with the three main categories ( masses , nme , m / nme ) , and no significant variations were found between the various groups [ 39 ]  . 
nme is associated , although without statistical significance ( p : 0.20 ) , with a higher risk of a progesterone receptor negativity ( 3 / 6 , 50.0% ) , and with statistical significance ( p : 0.03 ) to a moderate ( 2 + ) or high ( 3 + ) her2 positivity : this significance is further greater ( p : 0.021 ) if we consider the sum of nme and m / nme rather than masses only . 
fish analysis in moderate ( 2 + ) her2 positivity cases showed no gene amplification for all , and then the real and relevant positivity to her2 was detected in only 1 / 31 ( mass - like lesion )  . 
then , we have calculated the intraclass correlation coefficient ( icc ) for the entire sample and its result ( 0.858 ; 95% ic 0.7060.932 ) suggests a good performance of the cedm in the valuation of the maximum diameter of the lesion . 
then , a correct loco - regional staging with an evaluation of the extent of the disease is fundamental , even more than in other histological variants , to allow the most appropriate treatment and avoid any complications [ 4548 ]  . 
3 blandaltman plots 1 3 la radiologia medica ( 2019 ) 124 : 12291237 1235 cedm , which is more recent than mri [ 11 , 35 , 39 ]  . 
furthermore , in our study , unlike what was done in previous ones , we analyzed the differences in the various categories of enhancements such as m , nme and m / nme : the presence of a nme led to a lowering of cedm sensitivity in detecting any additional lesions up to 25% , versus 100% demonstrated in presence of a mass - like enhancement or a m / nme . 
nme led to a decrease in diagnostic accuracy in the evaluation of disease extension up to 40% , unlike what happens for masses ( 85% ) and for m / nme ( 80% ) : for the latter categories , data are absolutely similar to the performance of the mri reported in the literature [ 35 ]  . 
etal , cedm proves to be accurate in assessing the maximum diameter of the index lesion , being in agreement with its dimensions at the definitive histology [ 41 ]  . 
even if the sample size is very small , and therefore requires a multicenter study with a significantly larger sample , the performance seems to be better in case of masses or nme , and worse in case of masses closely associated with a non - mass enhancement . 
as well as in patels study and in other studies , the literature about ilc is described that almost all of lesions present expression of the estrogen receptor , in the ours the 100% of lesions shows a positivity to er . 
nme is associated , although not significantly , with a higher risk of a progesterone receptor negativity , while is correlated significantly with an increased expression of her2 ( 2 + or 3 + ) , compared to the presence of a mass enhancement : the necessary additional study with fish technique on moderate positivity to her2 , however , showed that all were not amplified , and then the real positivity was present only in 1 / 31 ( mass - like lesion )  . 
because this is a bi - centric study , the evaluation of the images was performed by different radiologists , as were different the surgeons who managed the patients , planning and performing surgical interventions and the pathologists . 
being a relatively recent diagnostic technique , the lack of experience of radiologists may have been a limitation for the study , especially in the early stages of it , even if as in case of introduction of each new diagnostic technique , it is to be considered a learning curve of the operators ; we believe that the experience of over 30years in breast imaging of our two radiologists of the study has reduced , although only partially , the influence of this limitation . 
the assessment of the intensity of the enhancement of lesions moreover was qualitative , in the absence , to date , of a validated quantitative system for its measurement in cedm , and thus also the evaluation of its kinetics . 
furthermore , the sample size is small , making definitive results more difficult ; therefore , a larger prospective study is needed to confirm our conclusions . conclusions cedm has proved to be a new promising imaging technique in case of loco - regional preoperative staging for ilc , especially in case of mass enhancement lesions . 
imaging assessment included : pre - procedural mdct , intra - procedural dp - cbct performed before first and second dsm - taces and 1 - month follow - up mdct . 
in particular , degradable starch microsphere trans - arterial chemo - embolization ( dsm - tace ) combines the advantages of loco - regional approach ( maximization of local drug delivering whilst reducing the systemic toxicity ) with the ones of a resorbable carrier that significantly increases the safety profile of the procedure by reducing the ischaemia time and vessel occlusion rate [ 2 ]  . 
in fact , a patient with bilobar spread will complete treatment within 2months ( four cycles ) and will be reassessed for lesion response with mdct only after 1month from the last dsm - tace . during the last few years , attention has been focused on the optimum modality for guidance of these treatments . 
the introduction of cone - beam computer tomography ( cbct ) to the field of liver catheter - based procedures has contributed to significant improvement in clinical outcomes , versus the use of standard digital subtraction angiography ( dsa ) guidance alone [ 3 ]  . 
in particular , cbct has been able to depict a significant rate of occult lesions missed at pre - procedural mdct [ 4 ] and the presence of extra - hepatic feeders [ 3 , 5 , 6 ] and provide a roadmap of the tumour vascular supply to facilitate successful and complete embolization [ 79 ]  . 
 recently , dual - phase cbct , consisting in introducing an additional delayed acquisition , has shown to facilitate hypovascular lesion visualization [ 10 ]  . despite these advantages in aiding the embolization procedure , only a few studies have focused on this technique ability to intra - procedurally predict the treatment outcome , with controversial results [ 11 , 12 ]  . 
for these reasons the aim of this study is to evaluate the potential prognostic value of sequential dual - phase cbct imaging performed during dsm - tace session in predicting the nodules response to treatment . materials andmethods this study was approved by the ethical institutional review board . 
all enrolled hccs were of typical vascular behaviour ( exhibiting washin in the arterial phase and washout on the delayed venous phase ) diagnosed on the basis of mdct only being greater than 2cm in diameter . 
the scan delay before the initiation of late arterial phase imaging was determined by means of bolus tracking with automated scan triggering ( care bolus ct ; siemens medical system )  . 
digital subtraction angiography ( dsa ) and cbct were acquired after having positioned the 4 - fr catheter in the common hepatic artery coupled with a power injector ( mark v provis ; medrad , beek , the netherlands )  . 
power injector parameters were 3.5ml / s , 900 psi , intra - arterial injection lasted 15s and first cbct acquisition started with 8 - s delay from the injection start . 
c - arm rotates 200 around the patient in 8 - s acquiring images every 0.5 at 60 frame / second for a total of 419 images with a 512x512x387 matrix and isotropic resolution of 0.49mm resulting in a 25 25 19cm fov . 
the data sets were automatically transferred to a workstation ( x - workplace , siemens healthineers , erlangen , germany ) for reconstruction and analysis . dsmtace protocol the protocol stipulated two sessions of dsm - tace on each involved lobe with 28 days between the two procedures . 
second row ( yellow box ) , management of monolobar disease 1 3 la radiologia medica ( 2019 ) 124 : 12121219 1215 imaging timing imaging assessment included a pre - procedural mdct performed less than a month before treatment , a first dual - phase cbct performed before the beginning of the first dsmtace session , a second dual - phase cbct performed before the beginning of the second dsm - tace session and a follow - up mdct performed after 1month after completion of treatment . 
attenuation values are expressed in hounsfield unit ( hu ) for mdct acquisitions , and pseudo - attenuation values are expressed in arbitrary unit in all intra - procedural cbct acquisition . to assess the predictive value of dp - cbct regarding the dsm - tace protocol per lesion , the modification over time of the lesions attenuation was correlated with the post - procedural modify response evaluation criteria in solid tumours ( mrecist )  . 
in detail , the modification of pseudoattenuation and attenuation were calculated as the difference of : first cbct and second cbct values ( arterial and venous acquisitions ) and pre - procedural mdct and post - procedural mdct values ( arterial and venous acquisitions )  . followup evaluation follow - up mdct was performed to assess treatment outcome , according to mrecist criteria [ 13 ] for hcc lesions . 
response to treatment was categorized as : complete response ( cr ) , partial response ( pr ) , stable disease ( sd ) and progressive disease ( pd )  . statistical analysis the normality of each continuous variable group was tested using the kolmogorovsmirnov z test . 
digital subtracted angiography ( a ) performed from the common hepatic artery showing multiple hypervascular hcc distributed in the both lobes ; the arrow shows the hcc of the vi segment detailed in the following images . 
in particular , it is possible to demonstrate the reduction in attenuation arterial ( b , e ) and venous ( f , i ) phases and pseudo - attenuation arterial ( c , d ) and venous ( g , h ) phases in a complete response nodule 1 3 1216 la radiologia medica ( 2019 ) 124 : 12121219 positive and negative cases = 0.33 for cr / pr + sd + pr , 1 for or / sd + pd and 3 for dc / pd . 
roc curve analysis was also performed and the auc were calculated for the difference of attenuation between first and second cbcts and preand post - mdct ( both arterial and venous phases )  . 
roc curve analysis ( fig.3 ) showed that the higher the attenuation ( hu and hu * ) difference between preand postprocedural mdct and first and second dp - cbcts was , the better the clinical outcome will be . 
the complete analysis is shown in table3 and in fig.4. discussion a strong association was found between the change in lesion attenuation assessed intra - procedurally over a set of multiple dsm - tace sessions and the prediction of treatment outcome evaluated at post - procedural mdct . 
they focused their studies on dp - cbct imaging before single - session tace procedures , failing to identify a statistically significant association ( univariate and multivariate analysis ) between lesions attenuation and post - procedural mrecist criteria . 
in fact , no standard treatment scheme was defined in the literature regarding the eventual readministration of tace ( conventional tace , deb - tace or dsm - tace ) protocol and several factors should be taken 1 3 1218 la radiologia medica ( 2019 ) 124 : 12121219 fig . 
the first column shows , for arterial ct phase ( first row ) and arterial cbct phase ( second row ) the sensitivity / specificity trend in relation to cut - off change , respectively , for complete response ( a ) , objective response ( b ) and disease control ( c )  . 
the second column highlighted the optimal cut - off with the corresponding sensitivity and specificity for complete response ( a ) , objective response ( b ) and disease control ( c ) into account , including : procedure timeline and embolization drug choice [ 17 , 18 ]  . 
on - demand scheme , over the scheduled one , is usually considered safer being re - treatment proposed only in case of progression of disease [ 19 , 20 ]  . 
 [ 22 ] demonstrated that switching from epirubicin to cisplatin in patients with refractory response to epirubicin - loaded deb - tace is a safe , well - tolerated and efficacious treatment strategy . 
however , unlike liver function , the effect of the dsm - tace could be assessed only at the end of the pre - defined administrative protocol ( 2 sessions per lobe ) by ct or mri . 
therefore , the possibility to predict intra - procedurally , with a predetermined cut - off , the effectiveness of the ongoing dsm - tace treatment introduces another parameter that impacts the management of the patient , avoiding unnecessary drug administration that could potentially impair the limited liver functional reserve . 
 for instance , the execution of dp - cbct by demonstrating lesion attenuation modification by early prediction of treatment failure could permit either drug switch , drug combination or dosage adjustment . our study presents several potential limitations . 
firstly , sample size is small ( 24 patients ) , although the usage of a per - nodule analysis ( 96 nodules ) in a subset of advanced disease patients supplies this limitation according to our sample size analysis . 
despite these limitations that can be 1 3 la radiologia medica ( 2019 ) 124 : 12121219 1219 addressed by increasing the sample size , we strongly believe that the lesion attenuation modification measurement is a simple tool that could lead to a significant clinical benefit . conclusion dp - cbct can predict intra - procedurally , by assessing lesion pseudo - attenuation modification , the dsm - tace 1 - month treatment outcome . 
 specific attention will be focused on the interaction of x - rays with matter , on the principles of attenuation of x - rays in ct toward the intrinsic limits of conventional ct , on the material decomposition algorithms ( twoand three - basis - material decomposition algorithms ) and on effective rho - z methods . 
the progresses in material decomposition algorithms , in computational power of computers and in ct hardware , lead to the development of different technological solutions for dect in clinical practice . 
this was the first empirical observation of material decomposition in computed tomography ( ct ) opening a new research field : material decomposition in dual - energy computed tomography ( dect ) [ 2 , 3 ]  . 
in the following years , several technologies have been developed and the applications of dect are more widely spread in the clinical routine . this review will provide a brief overview on theoretical principles behind dect ( better understood after reviewing the interactions of x - rays with matter ) , the available technologies and the main clinical applications . xrays : interaction withmatter the polychromatic spectrum ( photons with different wavelengths and energies ) of x - rays produced by the tube interacts and exchange energy with the biological matter with a combination of several phenomena : rayleigh scattering , photoelectric absorption , compton scattering , and pair production . 
the probability of each of them , expressed as cross section ( ) , is related to the energy of the incident photon and properties of the material [ 5 ]  . 
the rayleigh scattering ( r ) and the pair production give minor contribution to x - ray attenuation and are considered of minor relevance at energies used in ct [ 5 ]  . the photoelectric absorption ( ) involves the electrons of the inner shells ( k or l )  . 
the energy is completely transferred from the photon to the electron which is ejected ; the vacancy is filled by an electron from outer shells with emission of characteristic radiation or an auger electron . 
the probability of photoelectric interaction as linear attenuation coefficient ( , see the next section ) follows the rule : = k a ( h ) 3 z4e3 la radiologia medica ( 2019 ) 124 : 12811295 where k is a constant depending on the electron shell , is the density , z is the atomic number of the target , a the atomic weight , h is the plancks constant , is the speed of photon , and e is the energy of the incident photon . 
when the photon energy reaches the binding energy of the electron , there is a peak in the probability of photoelectric absorption ( absorption edge , k - edge if an electron in the k - shell is involved )  . 
for energies above the absorption edge , the probability of interactions rapidly decreases ( 1 / e3 ) [ 5 , 6 ]  . the compton scattering ( c ) involves the electrons in the outer shell . 
the incident photon exchanges part of the kinetic energy with the electron ; the electron is ejected , and the scattered photon continues the travel with a lower energy and a scatter angle . 
the probability of compton scattering is proportional to the electron density ( number of electrons per gram , ne ) , which is quite constant for most materials except for hydrogen . 
the probability of compton scattering , described as linear attenuation coefficient ( c ) , can be approximated as proportional to the electron density and inversely proportional to the x - ray photon energy [ 7 ] : c nee1 limits ofcomputed tomography ( ct ) andphysical principles ofdualenergy ct ( dect ) experimentally , when a monochromatic ( one specific energy ) x - ray beam with an energy e and intensity i0 is attenuated by a homogeneous material , the residual intensity after at a thickness x ( ix ) follows the lambertbeers law : ix = i0ex = i0e ( , z , e ) x where e is th eulers or napiers constant and the linear attenuation coefficient ( the fractional attenuation of the x - ray beam per unit thickness of the attenuating material ) is a function of the energy of the x - ray beam ( e ) , the atomic number ( z ) and the physical density ( ) of the material [ 8 ]  . 
 in ct , the linear attenuation coefficient of each scanned voxel ( r , the considered unit volume ) can be derived from the ct number ( ct# ) in the hounsfields equation [ 1 , 9 ] : ct# = ( r ) water water 1000 the linear attenuation coefficient is related to the physical density , and its application in the attenuation of 1 3 la radiologia medica ( 2019 ) 124 : 12811295 1283 biological tissues can be less convenient . 
the physical density of the attenuating material is influenced by the physical state of the matter ; however , the energies involved in photonelectron interactions are much greater than the energies involved in molecular bindings ; thus , the linear attenuation coefficient can be considered approximately proportional the physical density and eq.3 can be written as : ix = i0e ( z , e ) where / can is the mass attenuation coefficient [ 8 ]  . 
in the case of a mixture of materials , such as biological tissues , the mass attenuation coefficient can be approximated as the sum of the mass attenuation coefficients of each compound : where wi is the weight fraction of each compound of the mixture [ 8 ]  . 
this is the mathematical expression of the intrinsic limits of ct : considering the attenuation of a mixture with two known materials at unknown proportions , eq.6 has no solution because it is an equation in two unknowns ( w1 and w2 ) and one solution ( , or ct# ) [ 8 , 9 ]  . 
the plot shows the linear attenuation coefficient ( total ) of iodine at different densities ( = 0.1 g / cm3 , light blue ; = 0.01 g / cm3 , dark blue ) and calcium ( = 0.1 g / cm3 , red ) as function of energy of the incident x - ray photon . 
approximating the x - ray beam in ct to monochromatic , the colored curves are a representation of the ct numbers ( total ) of a given material at a given density when irradiated with a given energy . 
the attenuation curve is characteristic of the material and models the compton and photoelectric interactions : the blue curves of iodine at two different densities are equal with the same absorption edges ; the value of linear attenuation coefficient ( total ) is function of energy ( the shape of the curve ) and of density ( light and dark blue curves of iodine )  . 
if the same materials at the same densities are scanned at a different energy levels ( e.g. , 10kev , black dashed line ) , the linear attenuation coefficients and the ct numbers are clearly different ( black arrowheads )  . 
by knowing the attenuation curves , a couple of materials can be characterized and quantified if scanned at two energy levels ( i.e. , material decomposition in dualenergy ct )  . 
national institute of standards and technology ( : / / www.nist.gov / ; accessed on october 8 , 2019 ) 1 3 1284 la radiologia medica ( 2019 ) 124 : 12811295 fig . 
in the mixed images , the ct numbers in each pixel pixels are a weighted sum of the correspondent ct numbers in the lowand highenergy reconstructed images and can be considered as similar to conventional ct . 
the material decomposition evaluates the different attenuation curves of the basis materials , allowing for material labeling ( iodine : blue map and arrowheads ; calcium : red map and arrowheads ) ( e ) = ( e ) + ( e ) + ( e ) ( e ) + two - basis - material decomposition in the projection domain ( raw data ) ( fig.3 ) [ 2 , 3 ]  . this principle is at the basis of the first two - basis - material decomposition algorithm developed by alvarez and macovski . 
this demonstrates that when using a conventional x - ray beam , the effective attenuation coefficient can be calculated from the contribution of compton and photoelectric interactions modeled on the effective eff ( density ) and zeff ( atomic number ) of the material : ( e ) e ( e ) e e = e + fkn ( e ) ( e ) ( e ) + ( e ) + where and are constants , d 3 4 , g 3 3.5 and fkn ( e ) is the kleinnishina function . 
the right term of the third part of eq.8 is the linear combination , respectively , of the ] and compton [ fkn ( e ) ] interphotoelectric [ actions . 
 the work of alvarez and macovski is at the basis of the rho - z ( z ) algorithms for material decomposition and the eeg starting from the work of alvarez and macovski , kalender etal . 
defined the mass attenuation coefficient of a given mixture , as function of energy [ ( / ) ( e ) ] , with a linear combination of the mass attenuation coefficients of two hypothetical known basis materials ( 1 and 2 ) present at different mass densities ( 1 and 2 , see also the weight fractions wi in eq.6 ) at the spatial location r : ( r , e ) = 1 ( r ) ( e ) + 2 ( r ) the linear attenuation coefficient at a given spatial location ( r , e ) ( i.e. , the measured attenuation in ct ) is the sum of two known materials with known mass attenuation coefficients [ ( / ) 1 , 2 ] present at unknown mass densities within the voxel ( unknown 1 , 2 ) ; the equation has no solution when a single x - ray spectrum is used [ 13 ]  . if we measure the attenuation coefficients after irradiation with two x - ray energies ( high and low , h and l , ih and il ) , eq.9 can be solved as a system of two equations with two solutions ( ( r , e ) h , l ) and two unknowns ( 1 , 2 )  . 
vmi at low kev are useful for highlighting focal lesions in condition of low contrast ( e.g. , in liver or pancreas ) ( fig.4 ) or for improvement ofthe contrast - to - noise ratio and reduction of the administeredcontrastmaterial [ 14 ]  . 
conversely , vmi at high kev are useful for reduction of proton - starving and beam - hardening artifacts in the presence of metallic objects at the expense of contrast ( fig.5 ) [ 15 ]  . 
a drawback of some vmi algorithms is the increasing noise at lower energies ; this problem has been addressed with the introduction of noise - corrected vmi ( monoplus , monoenergetic plus , siemens healthineers ) [ 16 ]  . 
the theoretical advantage of the approach in the projection domain is the avoidance of beam - hardening artifacts : the linear attenuation coefficient is obtained from the attenuation coefficient of the basis materials at the calculated mass densities [ 13 ]  . 
 a critical issue of the projection domain approach is the large amount of data processed and the high computational power required : the post - processing of dual - energy data could be easier on reconstructed images ( fig.3 ) [ 13 ]  . 
equation8 can be defined as the linear combination of the mass attenuation coefficients of two basis materials present in the mixture with fractional masses of m1 + m2 = 1 ( being m2 = 1m1 )  . 
also , the effective linear attenuation coefficient ( eff ) can be calculated from the ct numbers ( ct# ) as in eq.4 : e = water = e + fkn ( e ) 1000 = e 1 m1 ( 12 ) 1 3 1286 la radiologia medica ( 2019 ) 124 : 12811295 fig . 
despite the strong weighting of the low voltage on image a , the monochromatic plus reconstruction allows for better visualization of a higher number of liver metastases ( empty arrowheads ) fig . 
 a , b dual - energy acquisitions 100 / 150kvp , mixed 0.8 , venous phase , soft - tissue window ( a ) and bone window ( b )  . 
marked beam - hardening and photonstarving artifacts are present close to the prosthesis ( arrowheads ) limiting the evaluation of the soft tissues ( a ) and the cortical bone ( b )  . 
the artifacts are reduced , the visualization of pelvic soft tissues ( c ) and the cortical bone ( d ) are improved ( empty arrowheads ) at the expense of contrast ( * ) the effective linear attenuation coefficient is calculated from the ct number ( ct# ) , it is a function of photoelectric and compton interaction of a mixture with an atomic number zeff but can also be defined as a function of two unknowns : the effective mass density ( eff ) and the fractional mass of one basis material ( m1 )  . 
the ct acquisition with two different x - ray energy spectra ( h and l ) provides two datasets of reconstructed images that can be processed to obtain the two unknowns : ct#h 1000 + 1 ct#l 1000 + 1 water = e water = e 1 m1 1 m1 ( 13 ) this is the concept behind the material decomposition on image domain this case , since the reconstructed images are used , the beam - hardening artifacts are not automatically removed andneed to be corrected [ 17 ]  . 
proposed a hybrid algorithm with a pre - processing in the projection domain to reduce beam - hardening artifacts [ 18 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 12811295 1287 an interesting point is that any material with different atomic number than the chosen basis material variably contributes ( and is characterized as ) to the attenuation of each of the basis material in all of these algorithms [ 13 ]  . 
a classical case was the calcium quantification in osteoporosis with dual - energy acquisitions of vertebral bones , with a mixture of calcium , fat ( yellow marrow ) and water or soft tissue ( red marrow )  . 
the authors started from the hypothesis that the effective linear attenuation coefficient in function of x - ray energy eff ( e ) comes from the sum of the mass attenuation coefficients of each basis material ( i ) multiplied by their concentrations ( the concentration ci is defined as the product between the fractional volume vi and mass density i ) , similarly to what expressed in eqs.6 , 9 , 10 , 12 , and 13 : ( 15 ) ct ( h ) = v1ct#1 ( h ) + v2ct#2 ( h ) + v3ct#3 ( h ) ct ( l ) = v1ct#1 ( l ) + v2ct#2 ( l ) + v3ct#3 ( l ) v1 + v2 + v3 = 1 where ct#i ( e ) are the ct numbers of pure basis materials at the given x - ray energy , previously obtained ( e.g. , calcium hydroxyapatite as a model for bone )  . 
this model allows for calculation , in the image domain , of relative quantities ( fractional volumes ) of three basis materials , by two measurements ( acquisitions at two different energies ) with a third condition ( the conservation of volume )  . 
the model cannot be generalized because the conservation of volume is not always respected ( e.g. , salt in water or iron in fat or soft tissue )  . a more generalized model was proposed by liu etal . 
in b , the blue dot over the separation line is the pixel labeled as iodine , while the red dot is the pixel labeled as calcium ( see also fig.2 ) 1 3 1288 la radiologia medica ( 2019 ) 124 : 12811295 fig . 
a dual source : two tubes working at different voltages and two asymmetrical detectors are mounted with an offset of nearly 90 , increased in the latest generation to improve the fov of system b up to 35.5cthe tin filtration for better spectral separation is possible with these scanners . 
the main purpose of this architecture was of achieving a temporal resolution acceptable for cardiac studies ( < 100ms : 6585ms ) with both tubes working ( flash or turboflash acquisition , siemens healthineers ) ; the dual - energy mode with the two tubes at different kvp is a natural corollary in these scanners [ 4 , 23 ]  . due to engineering issues ( balance and space in the gantry ) , the two detectors are asymmetrical with the smaller detector b limited to a field of view ( fov ) of 266mm in the first generation ( thus limiting the fov for material decomposition )  . 
the straton tube in the first generation was capable of 20kv steps between 80 and 140kv in the first generation , allowing for the combination of 80 / 140kv in dual - energy acquisitions . 
in the second generation , a tin filter ( 0.4mm ) was added to improve the spectral separation ( the robustness of material decomposition algorithms is proportional to separation of the two x - ray spectra ) allowing for two combinations in dual - energy acquisitions ( 80 / 140kv ; 100 / 140sn kv ) [ 24 ]  . 
in the third generation , the vectron tube was introduced : it is capable of 10kv steps between 70kv and 1 3 la radiologia medica ( 2019 ) 124 : 12811295 1289 150kv with a maximum current of 1300ma at 70kv . 
this technology allows for ( 1 ) a more frequent use of low voltages ( contrast and dose reduction ) and ( 2 ) better spectral separation ( 70100 kv / 140150 sn kv )  . 
moreover , the higher power allows for a more aggressive filtration at high voltages ( 0.6mm tin ) with further improvement of spectral separation ( fig.7 ) [ 25 ]  . with the newer generations , the rotation speed was improved ( up to 0.25s ) with no limitations for dual energy , together with the z - axis coverage and the introduction of integrated stellar detectors ( the lower noise in the stellar detectors improved the material decomposition )  . 
iterative reconstructions can be used with both tubes [ 25 ]  . this technical solution requires the material decomposition to be performed on image domain ( due to ~ 90 offset of the projections ) , and adequate algorithms are implemented to reduce the cross - scattered radiation between the two systems . 
besides the material decomposition , virtual monochromatic and rho - z methods , the scanner provides the blended ( mixed ) images for reading and reporting , in which the pixels are a weighted sum of the ct numbers from the highand low - energy datasets , without any material decomposition performed ( fig.3 ) [ 23 ]  . fast kvp switching in the fast kvp switching scanners ( discovery ct 750 hd and revolution , ge healthcare , milwaukee , wi ) , the x - ray tube switches between 80 and 140 kvp in less than 0.2ms , thus acquiring highand low - energy projections within the same rotation with almost no - temporal mismatch and at a full fov of 50cm . regarding the x - ray tube , the spectral separation ( and the material decomposition ) is affected by the ramp - up and ramp - down of the tube voltages while switching . 
at low voltage , the photon output is lower and the noise increases : higher current and longer exposure time are necessary at low kv ( typical exposure ratio : 80 / 140 kvp = 60% / 40% ) ; the automatic current modulation is not feasible in this configuration , and the dose reduction is implemented only with the iterative reconstructions . 
other challenges in detector design are the position of the photodiodes and the necessary presence of an antiscatter grid reducing the optical sensitivity when comparedto conventional detectors with photodiodes below the scintillator . 
conventional ct images are reconstructed by weighted summation of the highand low - energy datasets ; iterative reconstructions can be used for dose reduction [ 22 ]  . the split filter the split filter in the somatom edge twinbeam ( siemens healthineers , forchheim , germany ) is composed of two different metals : tin and gold , which , respectively , filter the low and high components to split a polychromatic x - ray beathe dual - energy datasets are acquired with each half of the detector receiving the split beathis allows for dualenergy information at full fov of 50cm with no limitations in rotation speed . 
potential drawbacks are the short pitch values ( 0.30.5 ) , the necessary high power of the tube because of filtration , with potential limitations in larger patients , and the limited spectral separation ( fig.7 ) [ 27 ]  . consecutive acquisitions this method does not require a dedicated hardware . 
dose reduction techniques , such as automatic current modulation , can be used ( fig.7 ) [ 28 ]  . 1 3 1290 la radiologia medica ( 2019 ) 124 : 12811295 1 3 la radiologia medica ( 2019 ) 124 : 12811295 1291 fig . 
 b iodine map ( red ) showing a perfusion defect ( * ) in the right lower lobe close to the pulmonary embolus ( arrowhead ) ; dual - energy acquisition 90 / 150sn , iodine overlayct dualenergy ct : postprocessing andclinical applications the applications of dual - energy can be divided in materialselective and energy - selective . 
the former includes material decomposition with material labeling , quantification ( distribution maps ) and subtraction ( vnc ) ; the latter includes the monoenergetic imaging , effective atomic number and effective electron density ( rho - z maps )  . 
table1 provides an overview of the algorithms and main clinical application dual - energy techniques . materialselective images : material subtraction , quantification andlabeling with material - selective images , a given basis material is detected , labeled and subtracted : iodine , calcium or other known materials ( e.g. , monosodium urate ) are frequently used as basis material . in neuroradiology , the main application of material decomposition is the material labeling and quantification of iodine in the presence of hemorrhagic material . 
the evaluation of contrast enhancement of a hemorrhagic brain lesion may be challenging in both ct and in magnetic resonance ( mri ) , while dect is able to distinguish the different spectral characteristics of iodine and iron . 
 [ 29 ] demonstrated a significantly higher sensitivity of iodine maps fused with virtual unenhanced images for detection of enhancing hemorrhagic brain lesions . in thoracic imaging , iodine maps allow for the evaluation of perfusion defects in pulmonary embolism , beyond the ct angiography , in acute and chronic setting ( fig.8 ) [ 30 , 31 ]  . 
 in cardiovascular imaging , the iodine maps are useful for the evaluation of myocardial perfusion while the selective subtraction of iodine in virtual non - contrast ( vnc ) images provided good results for the calcium score [ 3436 ]  . 
calcium labeling and subtraction with dual energy is useful for bone removal and plaque removal , improving the evaluation of vascular studies and the evaluation of vascular lumen [ 35 , 36 ]  . 
recorded an improved diagnostic accuracy with dect in characterization lipidic , necrotic , fibrous components and calcium in atherosclerotic plaques [ 37 ]  . an application of material decomposition in abdominal and oncological studies is the vnc reconstructions with avoidance of basal acquisitions and dose reduction , particularly relevant in selected populations ( e.g. , pediatric population ) [ 3842 ]  . 
it has to be pointed that small , often unimportant , differences in attenuation values need to be accounted when using virtual non - contrast images in abdomen ( fig.9 ) [ 43 , 44 ]  . 
the evaluation of iodine maps allows for accurate discrimination between enhancing and unenhancing lesions : this may be relevant in complicated cystic lesions of the kidney [ 45 ]  . 
regarding treatment response , the iodine quantification showed promising results : changes in iodine uptake are a more accurate indicator of treatment response to target or antiangiogenic agents than morphological criteria [ 4749 ]  . 
the evaluation of iodine maps has demonstrated their utility in the evaluation of the gastrointestinal tract , improving the detection of inflammatory , vascular ( ischemic ) and neoplastic lesions [ 50 ]  . 
b dual - energy acquisition , venous phase ( 90150sn kvp ) , 3 - basis - material decomposition ( liver vnc , siemens healthineers ) , virtual non - contrast . 
virtual non - contrast acquisitions are of good quality , may be useful for avoiding basal acquisitions , but sometimes present variable differences in attenuation when compared to basal acquisitions fig . 
material decomposition allows for labeling of monosodium urate crystals in green on coronal ( b ) and volume rendering ( vr ) reconstructions ( c ) ( arrowheads ) with volumetric estimation in liver imaging , the iron quantification with dect is an important tool when mri is contraindicated [ 53 ]  . in musculoskeletal radiology , material labeling is useful for the quantification of monosodium urate crystals in gout and differentiation with other crystal arthropathies ( fig.10 ) [ 54 , 55 ]  . 
the evaluation of bone marrow disorders , typically evaluated with mri , is an expanding application of material decomposition : dect is useful for depiction of bone marrow edema and bone lesions ( three - material decomposition and virtual non - calcium ) [ 57 , 58 ]  . 
vnc and iodine subtraction are also useful in the case of intravenous contrast injection or in ct arthrography [ 59 , 60 ]  . energyselective applications : virtual monoenergetic images andrhoz methods vmi are produced with the linear attenuation coefficients of basis materials obtained from the material decomposition , with the possibility of reconstruction of simulated images in a wide range of energy levels , within or out of the ranges effectively used . 
the vmi reconstructions have demonstrated promising results for the evaluation of pancreatic adenocarcinomas , focal liver lesions ( fig.4 ) or for the extension of endometrial adenocarcinomas [ 6163 ]  . 
another field of applications is the optimization of contrast , similarly to acquisitions at low voltages ( not always possible ) , with potential reduction of the dose of contrast material , in particular in cardiovascular imaging , and in the evaluation of pulmonary embolism [ 14 , 6466 ]  . 
vmi at high kev simulate the use of high - energy x - ray beams and are useful for attenuation of beam - hardening artifacts at the expense of contrast ( fig.5 ) [ 15 ]  . a material or a mixture with unknown attenuation coefficients can be semiquantitatively assessed on the spectral curve and highlighted ; this is the case of biliary noncalcific stones or foreign bodies , such as in drug mules [ 6769 ]  . finally , the rho - z methods still have more limited implementation : interesting applications in tissue characterization , mainly in cartilages and tendons [ 59 ]  . conclusion in this review , we have provided a brief overview on physical and theoretical principles , and clinical applications of dual - energy ct , which is a growing technique with expanding applications . funding no funding was received for this paper . compliance with ethical standards conflict of interest aa is a speaker for siemens healthineers . 
all the staging ct scans were evaluated by three experienced radiologists dedicated to thoracic disease in order to radiologically define the predominant pattern of presentation . results the following parenchymal patterns were observed : 11 patients with single / multiple nodules , five with masses / mass - like consolidations , 14 with consolidations with air bronchogram , 16 with ground - glass opacity , ten with angiogram sign , 22 with perilymphatic and / or peribronchovascular spread , 15 with associated lymphadenopathies , and 13 with pleural / chest wall involvement . 
the main characteristics of ppls were the presence of consolidations and ground - glass opacities , with perilymphatic and / or bronchovascular spread . conclusion all the characteristics of the work should alert the radiologist to consider lymphoma among the possible differential diagnoses , always correlating the results of the ct examination with appropriate clinical laboratory evaluations . keywords lung neoplasm lymphoma malt high - resolution computed tomography diagnosis differential diagnosis introduction lymphoproliferative disorders of the lung can be divided into primary pulmonary lymphomas ( ppls ) and secondary pulmonary involvement by lymphomas arising from adjacent nodal sites ( such as mediastinal or hilar lymph nodes and thymus ) or by haematogenous dissemination from an extrapulmonary site of involvement . 
ppl is defined as a malignant monoclonal lymphoid proliferation within the lung parenchyma , in a patient without any detectable extrapulmonary involvement at least 3months after initial * vittorio miele vmiele@sirm.org 1 department ofemergency radiology , university hospital careggi , largo brambilla 3 , 50123florence , italy 2 haematology unit department ofoncology , university hospital careggi , florence , italy 3 haematology unit andbone marrow transplant unit , san camillo forlanini hospital , rome , italy diagnosis [ 1 ]  . 
it is a rare disease , representing approximately 34% of extranodal lymphomas ( less than 1% of all nhl cases ) and 0.51% of all primary malignancies involving the lung [ 26 ]  . 
ppls can be malt lymphoma ( maltomalow - grade marginal zone b - cell lymphoma of mucosa - associated lymphoid tissue ) , other non - hodgkin lymphomas or hodgkin lymphoma . 
 malt lymphoma is the most common type , representing 5890% of all the ppls ; it is more common in females , often associated with autoimmune disease [ 7 ]  . 
others rare types of ppls include mantle - cell lymphoma ( mcl ) , follicular lymphoma ( fl ) or lymphoplasmacytic lymphoma ( ll ) [ 3 , 4 , 8 ]  . 
in such case , parenchymal involvement usually occurs by direct extension vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 12621269 1263 of mediastinal pathology or it is associated with disseminating disease [ 5 , 810 ]  . 
clinical findings are often unspecific or absent ; pulmonary symptoms such as cough , dyspnoea , haemoptysis , or chest pain may occur , as well as systemic symptoms like fever , weight loss , and fatigue . 
this study aimed to describe the predominant ct patterns of plls evidenced in our population of patients , focusing on the differential diagnosis to address the problematic role of the radiologist in making a correct diagnosis and to help the clinicians to set the right therapy . materials andmethods inclusion criteria our institutional board review approved this retrospective study . 
inclusion criteria were patients age between 18 and 90years , acquisition of informed consent , histological diagnosis of ppl , pre - treatment chest ct with contrast medium utilization . reference standard the diagnosis was histologically confirmed by lung biopsy in all cases . 
clinical staging was referred to as ann - arbor staging , also assessing the presence of systemic symptoms ( fever , night sweats , weight loss of > 10% of body weight over 6months ) [ 11 ]  . imaging protocol because of the length of the considered period ( 16years ) , images were acquired by the use of different ct scanners and technique protocols ( scanners : lightspeed vct 64 , ge ; sensation 16 , siemens ; sensation 64 , siemens ; optima 64 , ge ; ict 128 , philips ; somatom definition flash , siemens )  . 
the acquisitions were all in inspiration phases , and high - resolution images were contiguously reconstructed at 11.5mm using a smooth kernel for mediastinal structures and a sharp one for parenchymal evaluation . imaging review anddata analysis all images were stored in a picture archiving and communication system ( pacs )  . 
an independent and retrospective review of chest imaging for each patient was performed by two radiologists to define the predominant pattern of ppl presentation ; in case of discordance , a consensual agreement was reached . 
ct scans were assessed for the presence of single or multiple pulmonary nodules ( diameter < 2.5cm ) , monolateral or bilateral , masses ( diameter > 2.5cm ) or mass - like consolidations , with or without the coexistence of a positive angiogram sign , ground - glass opacities , parenchymal distribution ( bronchovascular or perilymphatic ) , the presence of hilarmediastinal lymph nodes ( long axis > 1.5cm ) and pleura / chest wall involvement . 
all thoracic images were also assessed for evidence of other associated pulmonary pathology ( such as bronchiectasis / bronchiolectasis , emphysema , and fibrosis )  . results patients were 14 males and 16 females , aged 5686years at diagnosis ( mean age 72years )  . 
angiogram sign and pleural involvement were similar in both malt and dlbcl . discussion the lung is frequently involved in metastatic localization of hodgkin and non - hodgkin lymphomas ( up to 38% in hl and up to 24% un nhl ) [ 7 , 9 , 12 ]  . 
b one - year follow - up ct after chemotherapy shows multiple bronchiectasis in the medium lobe that remains stable for many years 1 3 1266 la radiologia medica ( 2019 ) 124 : 12621269 fig . 
b 8 - month follow - up ct after treatment lymphoid tumours are rare ; as discussed before , malt lymphoma is more common than dlbcl ( 5890% and 1020% respectively )  . 
although dlbcl can occur as a primary proliferation , it can also arise from the transformation of a malt lymphoma into a more aggressive dlbcl [ 6 , 13 ]  . 
imaging manifestations of ppls may overlap with other ct features of completely different diseases and usually make a radiological diagnosis is difficult . in our case series , the most prevalent ct findings in both malt and dlbcl are the presence of masses and consolidations , together with diffuse / focal ground - glass opacities and with perilymphatic and peribronchovascular spread of these lesions . 
on imaging , the ct features of malt and dlbcl can overlap ; in both cases , patients can present nodules or consolidations , although cavitation and necrosis of the lesion are more frequent in dlbcl than in malt lymphoma itself [ 2 , 9 ]  . 
in a majority of patients , a followup ct scan shows any growth of the lesion , which can be stable for many years [ 20 , 21 ]  . 
however , a similar pattern can be seen in other entities and the differential diagnosis , in this case , includes organizing pneumonia , eosinophilic or lipoid pneumonia , lymphoid interstitial pneumonia ( lip ) or lung adenocarcinoma with lepidic growth [ 13 , 22 ]  . 
chest radiograph in a shows a mass - like consolidation in the lower right lobe , confirmed at ct study in b crazy paving appearance was associated with the lesion in the medium lobe . 
b one - year follow - up ct after therapy patient , but it is unlikely that there is a transformation of lip into a malignant process [ 9 ]  . ( transplant , autoimmune disease , clinical indolent behaviour , hiv infection , smoke ) [ 19 , 23 , 26 ]  . usually , air bronchogram is common in ppls because the bronchi and bronchioles tend to be unaffected from the proliferation of the tumour . 
angiogram sign , that is an enhancing pulmonary vessel within a homogeneous area of consolidation , is a feature of ppl ; it is a usual sign but non - specific . 
it could be present in other conditions such as mucinous adenocarcinoma , post - obstructive consolidation , and also in all the lymphoproliferative diseases [ 19 , 2325 ]  . 
 in general , a consolidation with homogeneous attenuation , air bronchograms , and angiogram signs are typical features of ppls but non - specific ; radiologist should keep high suspicion in patients with these ct features and high - risk factors the typical perilymphatic spread of ppls lesions could simulate other diseases , in particular , sarcoidosis and lymphangitic carcinomatosis . 
all these three entities are characterized by abnormalities of the bronchovascular bundles , subpleural interstitium , and interlobular septa ; the thickened interlobular septa and alterations of the subpleural interstitia are significantly greater in lymphangitic carcinomatosis than in the other two diseases [ 27 , 28 ]  . 
 lymphangitic carcinomatous often involves the peripheral interstitium at first , and then progresses towards the central area ( retrograde spread ) ; instead , lung lymphoma and sarcoidosis tend to progress from the lymph nodes 1 3 1268 la radiologia medica ( 2019 ) 124 : 12621269 to the peripheral lymphatics ( anterograde spread )  . 
mediastinal hilar lymphadenopathies and pleural involvement are not frequent in our case series as well as in the other most recent clinical studies [ 23 , 30 , 31 ]  . 
pleural involvement can be shown as a focal thickening , a secondary effusion or a pyothorax , especially in patients with epsteinbarr viruspositive dlbcl [ 32 , 33 ]  . differential diagnosis of ppls includes also two other clinical situations : lymphomatoid granulomatosis ( lg ) and post - transplant lymphoproliferative disorders ( ptld )  . 
radiologically lg can be indistinguishable with ppls but , when both cavitations and ground - glass halos are present , the disease appears similar to granulomatosis with polyangiitis ( wegener granulomatosis , especially in 30% cases here are necrotic coalescing and cavitated nodules ) [ 35 ]  . 
ptld collects a group of lymphoproliferative disorders occurring in the post - solid organ or post - stem cell transplant , varying from benign polyclonal conditions to malignant monoclonal diseases [ 3 , 5 , 9 ]  . 
imaging manifestations are similar to dlbcl , including solid masses - nodules , consolidations , ground - glass opacities ; solid masses in ptld tend not to cavitate [ 19 ]  . 
 both lg and ptld lesions are avidly hypermetabolic at fdg - pet [ 3638 ]  . despite everything , nowadays lung biopsy is still necessary to achieve a definitive diagnosis , essentially in all cases of ppls . 
percutaneous ct - guided or bronchoscopic biopsy may be sufficient for solid lesions ; in the case of groundglass opacity , consolidation , and interstitial involvement , an open surgical biopsy may be required [ 3 , 15 , 30 ]  . this study has some limitations . 
second , the statistical analysis did not reveal any significant correlation between our data , may be because of the various heterogeneity of ppls at ct imaging and the small number of patients . 
however , to the best of our knowledge in the most recent literature , this work contains one of the numerically most significant case series of ppl [ 23 , 30 , 31 , 39 , 40 ]  . in conclusion , we have described the imaging findings in a series of 30 ppls , confirmed by lung biopsy . 
radiologists have to be aware of the various radiological patterns of penile traumatic lesions , in order to establish a prompt and correct diagnosis . keywords penile trauma fracture priapism ultrasonography magnetic resonance retrograde urethrography introduction acute penile traumas are uncommon , with an incidence of 1 / 175.000 in emergency department [ 1 ]  . 
the primary and clinical distinction is between penetrating and non - penetrating traumas : furthermore , it should also be evaluated if the trauma occurred when the penis was flaccid or erect , because the resulting injury is different [ 2 ]  . 
radiological approach is the first choice in cases of blunt trauma , while clinical evaluation , before surgical exploration , is usually sufficient in patients with penetrating traumas [ 3 ]  . 
ultrasonography ( us ) is the first - choice imaging modality in evaluating patients with penile trauma : in particular in expert hands , using high - resolution and high - frequency probes , with color and spectral doppler investigation , us can be really useful and can guide the management of the patient [ 46 ]  . 
magnetic resonance imaging ( mri ) is the best diagnostic tool in evaluating the integrity of tunica albuginea , even in patient with severe injury , because of its panoramic and multiplanar capabilities and excellent tissue contrast [ 79 ]  . 
in emergency department , us is the first ( and often unique ) imaging technique and mri is used only in particular situations in the clinical practice , for example when it is necessary to identify a small tear of ta in a suspect penile fracture . 
the cc are composed of sinusoidal spaces with smooth muscles and endothelium ( erectile tissue ) : the inter - cavernosal septum divides these two structures , and it is porous , allowing the passage of blood from one side to the other . 
in mri , the cc and cs have variable signal intensity depending on the rate of blood flow within the cavernous spaces : usually , they have an intermediate t1w and t2w signal . 
 the thin dartos fascia lies superficial to bucks fascia ; it is not always seen in mri and separates the connective subcutaneous tissue from relatively t2 - hyperintense skin epidermis . 
the vascular anatomy of penis is very variable [ 10 ] , but there are three main paired sources of arterial inflow in the penis : the dorsal artery , which is lateral to the deep dorsal vein and supplies the glans , penis and skin ; the cavernosal artery , a terminal branch of the internal pudendal artery located in the center of each cc , which provides arterial inflow to the cc during erection ; the bulbourethral artery which supplies the urethral bulb and posterior cs . 
 the venous drainage is through the dorsal veins : the superficial dorsal vein , which is superficial to the bucks fascia , and the deep dorsal vein , which is deep to the bucks fascia . 
normal t2 sequence mri ( b ) and sonographic ( c ) anatomy of the penis 1 3 1272 la radiologia medica ( 2019 ) 124 : 12701280 superficial one drains the external envelopes of the penis . 
 the two systems , although separated from the bucks fascia , communicate widely with each other and can , therefore , mutually substitute each other . because of its superficial location , the penis is ideally suited for us imaging . 
sonographic evaluation of the penis is performed with patient in a supine position , and the penis should be in the anatomic position , lying superiorly against the anterior abdominal wall . 
mr imaging of the penis is facilitated by appropriate positioning of the patient : in supine position , the penis is dorsiflexed against the lower abdominal wall in the midline . 
imaging protocols are customized to each patient , but , in general , an axial t1w spin - echo and axial , sagittal , coronal fast spinecho t2w images are obtained . 
both in us and mr imaging , if there is the necessity to have imaging of erect penis , prostaglandin e1 is injected into one corpus cavernosum . penetrating trauma the severity of penetrating traumas to the penis is variable , depending on the involvement of the skin , urethra and erectile tissue , and most of these are caused by selfinflicted mutilation in psychiatric patients or inflicted by a second part [ 2 ]  . 
one of the main reasons of penetrating injury is self - insertion of foreign bodies into urethra on purpose of sexual eroticism : in these cases , retrograde urethrography can be used to assess any possible urethral lesions [ 15 , 16 ]  . 
us and color doppler investigations have a role in identifying hematomas and any possible foreign bodies retained within the penis : in particular , color doppler interrogation of cavernosal arteries allows evaluation of associated vascular injuries . 
 us imaging of penile hematoma from penetrating injuries , as well as hematomas from other causes , depends on the moment of onset : hyperechoic lesion in acute phase , with time it appears as hypoechoic area also with cystic alterations and septated wall . 
cavernosal hematomas can evolve with complete restoration or with a fibrotic scar [ 17 ]  . table 1 basic protocol for post - trauma penile mri basic protocol for post - trauma penile mri baseline standard sequences axial , coronal , sagittal t2w tse ( slice thickness 35mm ) axial t1w tse ( slice thickness 3mm ) additional sequences for trauma axial t1w gre ( slice thickness 35mm ) sagittal , axial t2w stir ( slice thickness 35mm ) anatomic evaluation of cc and cs integrity of ta characterizing fluid collections anatomic evaluation of cc and cs integrity of ta characterizing fluid collections characterizing blood collections characterizing fluid collections and edema after gadolinium administration standard sequences axial , sagittal post - contrast t1w fat suppressed gre ( slice thickness 35mm ) tissues evaluating the enhancement of penile soft tse turbo spin - echo , gre gradient - echo , stir short - inversion time - inversion recovery , cc corpus cavernosum , cs corpus spongiosum , ta tunica albuginea 1 3 la radiologia medica ( 2019 ) 124 : 12701280 nonpenetrating trauma erect penis most of traumas to the erect penis happen during sexual activities and often result in penile fracture , urethral lesions and extratunical hematomas . 
 generally , a tear occurs only in one of the cc ; however , cs fracture can occur and urethral lesions are associated in 1020% of cases [ 9 , 18 , 19 ]  . 
erect penis has an increased risk of fracture because the ta stretches and gets thinner during erection : it has to be remembered that ta is one of the strongest human fasciae and its thickness decreases from 2 to 0.50.25mm during erection [ 11 , 21 ]  . 
penile fractures are rare urologic emergencies : patients hear a popping or cracking sound associated with pain and rapid detumescence , swelling and penile deformity [ 19 , 22 ]  . 
most authors are for an immediate surgical repair of the fracture and making an imaging diagnosis before surgery is recommended : in fact , preoperative imaging is helpful in confirming the correct clinical diagnosis and can also differentiate true penile fracture from false / pseudofracture ( a false fracture is , for example , a hematoma without any ta defect ) [ 3 , 6 , 23 ]  . 
early surgical intervention can prevent late complications such as fibrosis , scarring and angulation of the organ ; surgery is generally recommended in case of suspected urethral injury and ta tear . 
the us detection rate in identifying ta tear is between 88 and 100% [ 6 , 25 ] , but us was unable to detect any ta tear in 12% of patients in the study of mehrjardi etal . 
however , sometimes us evaluation may be nondiagnostic , especially in the detection of small tears or in the presence of a thrombus that closes the ta defect . mri can be used in diagnosing penile fracture because of its panoramic view and multiplanar reconstructions ; however , it is often not performed in acute setting [ 3 , 8 ]  . 
the mri detection rate in identifying tear of ta was between 98 and 100% [ 6 , 28 ]  . in the literature , some authors have found that an accurate delineation of the site of rupture can enable surgeon to use a small focal incision , rather than a more invasive approach used in the past [ 3133 ]  . 
evaluation of the urethra with us is limited : us may be able to show edema or hematoma of corpus spongiosum , but a small isolated injury can be misdiagnosed [ 35 ]  . 
in the proximal third of the penile shaft of the right cc , there is an inhomogeneous oval hypoechoic area , referable to hematoma with a maximum axial diameter of 11.4mm ( arrow , figure a ) ; the tunica albuginea appears intact ( arrowhead )  . 
b , c sagittal t1w pre - contrast and post - contrast sagittal reconstructions that help in recognizing the focal interruption of the tunica albuginea ( arrows ) presence of air in the cavernosa corpora is suggestive of urethral injury , and it should be evaluated . 
a better visualization of the urethra is possible through sonourethrography : this is a retrograde technique in which a saline solution or a lubricant anesthetic jelly is inserted into the urethra via either a foley catheter or a syringe placed directly in the meatus [ 11 ]  . 
torn veins usually collapse and are not visible with us imaging , but sometimes they may undergo a post - traumatic thrombosis ( enlarged vessels with echogenic content )  . 
usually , aspiration of the hematoma is recommended to prevent septal fibrosis and its symptoms ( rigidity and penile shortening )  . 1 3 la radiologia medica ( 2019 ) 124 : 12701280 1275 fig . 
in this patient , the penis crushed against the pelvic bone ( asterisks ) after a blunt trauma : there is neither evidence of hematoma nor a ta laceration fig . 
catheter is placed in the urethra in the corpus spongiosum ( asterisk ) flaccid penis non - penetrating traumas to flaccid penis are usually caused by blunt perineal injuries , where the basis of the penile shaft is crushed against the pelvic bone [ 2 ]  . 
injury to the deep venous plexus or to the smooth muscle trabeculae can lead to intracavernosal hematoma : ta is usually intact in these patients [ 2 , 11 ]  . 
intracavernosal hematoma is usually bilateral , and its us appearance varies depending on the moment of bleeding : hematomas appear as a hyperechoic mass in the acute phase and then become cystic , often with septations . 
priapism is defined as a prolonged ( > 3h ) and sometimes painful penile erection without sexual desire , and it is classified as high - flow and low - flow priapism [ 3 , 5 , 41 ]  . 
patients usually come to the emergency department because of a painless persistent erection : the disease is occasionally recognized several days or month 1 3 la radiologia medica ( 2019 ) 124 : 12701280 1276 fig . 
9 isolated disruption of penile septuaxial ( a ) and sagittal ( b ) t2w images show a round well - circumscribed hematoma near the septum , with a hypointense wall ( arrow ) in subacute phase fig . 
a we can see a tear of the right cc with a large hypoechoic area ( with diameter equal to the diameter of the cc ) ( arrow )  . 
the tear shows a connection with the cavernous artery and has an arterial color doppler signal ( b ) : this sign indicates the presence of a fistula in high - flow priapis tunica albuginea and left cc are intact after the trauma , because of its symptoms that are not dramatic in low - flow priapism [ 43 , 44 ]  . 
nowadays , color doppler us is the imaging modality of choice because of its sensitivity and non - invasiveness and wide availability in radiology emergency department [ 42 , 44 ]  . 
11 artero - cavernosum fistula and high - flow priapisa a large hypoechoic area within the right corpus cavernosum , which shows a connection with the cavernous artery and has an arterial color doppler signal ( b )  . 
below the laceration , both corpora cavernosa are erected ( c ) and the doppler signal is suggestive of the presence of high - flow priapism ( d )  . 
any post - traumatic morphostructural alterations of the left corpus cavernosus are appreciated hypoechoic area , with well - circumscribed margins in the cc : in this area , color doppler interrogation demonstrates a characteristic arterial color blush ( extravasation of blood from the torn artery ) with high velocity and turbulent flow in the site of fistulization . 
12 arteriography pre ( a ) and post ( b ) insertion of spirals , as therapy for high - flow priapisin figure a , it is appreciable the flushing of contrast media from the cavernosal right artery ( arrow ) 1 3 1278 la radiologia medica ( 2019 ) 124 : 12701280 penis is rigid and painful . 
low - flow priapism is usually not caused by a direct penile trauma , but it can follow a central nervous system trauma or it can be secondary to medications , thrombophilic state , malignancy and neurological disorders [ 47 ]  . 
in low - flow priapism , there is a malfunction in penile vascular outflow : obstruction to the physiological venous outflow leads to a high intracavernosal pressure , irreversible ischemic alterations and permanent erectile disease . 
usually , priapism is well evaluated clinically : sometimes the analysis of cavernosal blood gas level may help , with a low oxygen tension in case of low - flow priapis the main aim of the therapy is to have a rapid reduction of the ischemic state , and in emergency , there is a limited role for imaging . 
the area ( arrows ) is hypointense both in t1w ( a ) and t2w ( b , c ) sequences , thus indicating a fibrotic area that could be mistaken for a ta tear , especially in sagittal reconstruction ( c ) 1 3 la radiologia medica ( 2019 ) 124 : 12701280 1279 fig . 
 axial t1w ( a ) and t2w ( b ) , sagittal t2w ( c ) images show diffuse hypointense fibrotic areas in both cc and the crura with thickening of the ta ( asterisks )  . 
it is possible to appreciate widespread fibrotic alterations of both cc in the entire length of the penis , except only for the peripheral portion of the cc themselves ( arrow )  . 
 after gadolinium administration ( d , e ) , the fibrotic areas do not enhance post - traumatic scarring and fibrosis may involve the ta , the corpora cavernosa and the surrounding tissues [ 35 ]  . 
usually , a diffuse penile fibrosis is a consequence of permanent low - flow priapism ; rarely , it can follow highflow priapism as well , as it has been described by savoca etal . 
radiologists must be aware that they have the key role to optimize clinical management of patients with penile trauma , escaping from errors and vain therapies , in order to avoid the potential irreversible sequelae . author contributions cozzi d , verrone gb and pradella s contributed to manuscript writing / editing ; damico g and agostini s contributed to manuscript writing / editing , data collection and management ; bartolini m and miele v contributed to protocol / project development . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . ethical standard this article does not contain any studies with human participants or animals performed by any of the authors . la radiologia medica ( 2019 ) 124 : 10371042 ultrasonography receiver operating characteristic analysis ofultrasound joint inflammation inrelation tostructural damage anddisease activity inrheumatoid arthritis huihuali1 johncarsonallenjr.2 julianthumboo3 , 4 , 5 yorkkiattan3 , 4 , 5 received : 23 april 2019 / accepted : 24 june 2019 / published online : 3 july 2019 italian society of medical radiology 2019 abstract objective to investigate whether ultrasound greyscale ( gs ) and power doppler ( pd ) joint inflammation may be useful in identifying rheumatoid arthritis ( ra ) patients in different states of structural damage and disease activity . methods in this cross - sectional study utilizing 36 - joint ultrasonography , bone erosion was scored dichotomously ( 1 = yes / 0 = no ) while gs and pd joint inflammations were graded semi - quantitatively ( 03 ) at each joint recess . 
ultrasound power doppler ( pd ) imaging provides valuable real - time information on synovial vascularity , while ultrasound greyscale ( gs ) imaging provides essential structural information at the joints such as extent of synovium thickening and erosive changes in bone [ 2 ]  . 
because pd and gs imaging are both core components of ra ultrasound joint assessment , the increased focus on standardization and clinical validation work over the past decade is not surprising [ 3 ]  . 
 both the european league against rheumatism ( eular ) and the american college of rheumatology ( acr ) have vol . : ( 0123456789 ) 1 3 1038 la radiologia medica ( 2019 ) 124 : 10371042 published recommendations on ultrasonography use in the clinical management of patients with ra [ 4 ] and rheumatology clinical practice [ 5 ]  . 
despite efforts to define the role of musculoskeletal ultrasound in ra clinical management , important practical issues remain to be addressed , one being a determination of the accuracy of ultrasound - diagnosed joint inflammation as a clinical marker for identifying ra patients in different states of disease activity and structural damage . 
in the recent literature , only a single recent study was found that utilized roc analysis to determine optimal cut - off values of ultrasound pd and gs joint inflammation metrics to identify ra patients in remission based the 28 - joint disease activity score ( das28 ) [ 8 ] , and none investigating optimal cut - off values for identifying patients with high bone erosion burden detected on ultrasonography . 
by applying roc curve analysis , our study aims to fill a current knowledge gap by investigating whether ultrasound gs and pd joint inflammation scores may be useful for identifying ra patients in different states of structural damage and disease activity . methods ra patients with at least one swollen and / or tender joint were recruited into this cross - sectional study from march 2016 till january 2017 . 
 [ 10 ] as follows : a semi - quantitative score of grade 0 refers to no colour signal ; a score of grade 1 refers to up to either ( a ) 2 single and 1 confluent signal or ( b ) up to three colour signals ; a score of grade 2 refers to greater than grade 1 to less than 50% filled with colour signals ; a score of grade 3 refers to greater or more than 50% filled with colour signals . 
ultrasound gs scoring relied on a previously published ultrasonographic atlas [ 11 ] which utilized representative ultrasound images for b - mode ( combined score for synovitis and joint fluid ) semi - quantitative ( 03 ) severity scoring . 
score of 0 = absence ; score of 1 3 la radiologia medica ( 2019 ) 124 : 10371042 1039 1 = mild ( describing the presence of a small hypoechoeic / anechoic line which is beneath the joint capsule ) ; score of 2 = moderate ( describing the joint capsule being elevated parallel to the joint area ) ; score of 3 = severe ( where there is a strong distension of the joint capsule )  . 
dichotomously scoring of ultrasound - detected bone erosion was utilized , as there has been no general consensus on which other more sophisticated methods of scoring bone erosion to use ( such as using a semi - quantitative scoring scale )  . 
das28 is a widely accepted composite disease activity marker for ra in the routine clinical practice and the threshold criteria of ( a ) 2.6 , ( b ) 3.2 and ( c ) 5.1 were used in our study as these are the generally accepted threshold score levels for das28 to distinguish patients in ( a ) remission versus low disease activity , ( b ) low versus moderate disease activity and ( c ) moderate versus high disease activity in ra respectively . 
 [ 8 ] previously looked at optimal cut - off values for ultrasound inflammatory scores to identify ra patients in disease remission , although a similar analysis using ultrasound joint inflammation scores was not performed for ultrasound - detected bone erosion . 
from the auc results of both our study and that by leng etal . , it appears that ultrasound pd inflammation is more useful than ultrasound gs inflammation in identifying ra patients in different states of disease activity . 
this may be explained in part by the inability of ultrasound pd vascularity to reflect the overall cumulative inflammatory burden at the joints over time when performed as a single time - point measurement . 
there is evidence to suggest that measuring joint inflammation over time ( time - integration ) can provide better prognostic information on disease outcomes compared to single time - point measurements as demonstrated by the two studies [ 13 , 14 ]  . 
although mri synovitis and bone marrow oedema at the dominant wrist were independent predictors of 3 - year radiographic progression , in this study , the 1 - year cumulative inflammatory measures of mri synovitis and bone marrow oedema were shown to be more informative in explaining variation in radiographic changes compared to baseline mri values . ultrasound gs joint inflammation has been shown to be associated with ra structural joint damage by various imaging modalities , including ultrasound - detected bone erosion [ 15 ] , radiographic [ 16 ] and mri structural damage progression [ 17 ] , thereby showing evidence of construct validity . 
to the best of our knowledge , the present study is the first to use extended 36 - joint ultrasonography ( with 60 joint recesses scanned per patient ) in an ra cohort with overall longstanding and moderate disease activity in conjunction with roc analysis to determine an optimal gs ultrasound joint inflammation score cut - off to identify patients with high ( ultrasound - detected ) bone erosion burden . 
we arbitrarily utilized the median score in the definition of high ultrasound - detected bone erosion burden as there is presently no general consensus on what constitutes a high or low erosive burden on ultrasonography at the patient level . 
 [ 18 ] has previously shown that improvement in ultrasound gs synovial hypertrophy can occur as early as 2weeks in a cohort of 89 ra patients treated with abatacept followed up longitudinally for 24weeks . 
future well - designed longitudinal studies on ultrasound gs joint inflammation in large ra cohorts will be required to shed light on this aspect of dmards therapy . one limitation of our study is the relatively small sample size , although we have gone to great lengths to study ultrasound joint inflammation and structural damage by using extended 36 - joint ultrasonography on each patient . 
 we believe that including a greater number of joints in the assessment will give a more comprehensive evaluation of 1 3 1042 la radiologia medica ( 2019 ) 124 : 10371042 how gs and pd joint inflammation relate to ultrasounddetected bone erosion . 
notwithstanding the claims of greater feasibility , better representation and use of logistic regression methods in joint selection by some ra ultrasound researchers advocating for using fewer numbers of joints in ultrasonography [ 19 ] , there is presently no formal consensus on a minimum joint set to scan . 
because our study cohort also has an overall longstanding disease duration and moderate disease activity , with the majority of the patients on conventional dmardsand none on biologics , our derived cut - off values for ultrasound gs and pd joint inflammation scores for identifying patients with high bone erosion burden and high disease activity state will require further validation in other independent ra cohorts with different clinical and treatment profiles . in summary , via the application of an extended 36 joints ultrasonography , we performed roc analysis to obtain sensitivity , specificity and other diagnostic parameters to determine whether ultrasound gs and pd joint inflammation scores may be helpful in identifying ra patients in different states of structural damage and disease activity . 
early diagnosis and treatment of lvv are paramount to reduce the risk of ischemic complications such as visual loss and strokes , vascular stenosis and occlusion , and aortic aneurysm formation . 
use of imaging modalities [ ultrasound ( us ) , magnetic resonance imaging ( mri ) , computed tomography ( ct ) and [ 18f ] - fluorodeoxyglucose positron emission tomography ( pet ) ] has steadily increased to enable assessment of cranial and extracranial arteries , as well as the aorta . 
however , these various imaging tools are not yet uniformly used in routine clinical practice and controversy exists as to which imaging modality best provides meaningful assessments of disease activity and damage in lvv . 
early diagnosis and treatment of lvv are paramount to reduce the risk of ischemic complications such as visual loss and strokes , vascular stenosis and occlusion , and aortic aneurysm formation [ 3 , 4 ]  . the first temporal artery biopsy ( tab ) was performed at the mayo clinic in 1932 and was held as the gold standard test to confirm the diagnosis of gca until recently [ 5 ]  . 
thus , use of imaging modalities [ ultrasound ( us ) , magnetic resonance imaging ( mri ) , computed tomography ( ct ) and [ 18f ] - fluorodeoxyglucose positron emission tomography ( pet ) ] has steadily increased to enable assessment of cranial and extracranial arteries , as well as the aorta [ 10 , 11 ]  . 
further , extracranial arteries are not accessible for histological assessment , and in lv - gca , temporal arteries are spared in 40% of patients [ 12 , 13 ]  . 
ultrasound - guided fast track approach in assessing gca patients has led to a reduction in irreversible vision loss and has introduced the concept of gca with and without cranial involvement , or gca with or without large vessel involvement ( lv - gca ) [ 1416 ]  . in tak , temporal arteries are frequently spared , and biopsies of the large vessels are generally not feasible . 
due to strong evidence and high taskforce agreement , emphasis is placed on early confirmation or exclusion of gca to prevent disease complications of luminal changes caused by vasculitis ( such as stenosis , aneurysm or occlusion ) but cannot identify vessel wall pathology . 
these advances have created controversy regarding which imaging modality best provides meaningful assessments of disease activity and damage [ 4 ]  . aortitis is a common finding in gca and tak and can occur secondary to infections , other forms of vasculitis , but rarely occurs as an isolated idiopathic disease found incidentally on radiologically or histological assessments from resected aortic aneurysms [ 18 , 19 ]  . several studies have evaluated the use of us , mri , ct and pet in lvv over the last two decades . 
the aim of this review is to summarize the current evidence of imaging in patients with or suspected of having lvv , and to highlight the clinical implications of the eular recommendations . eular recommendations the eular recommendations were informed by a systematic literature review ( slr ) by duftner etal . 
 [ 21 ] that assessed 43 prospective studies , published until march 2017 , with sample sizes of at least 20 patients with suspected and / or established primary lvv . 
of note , some of the articles assessed overlap in domains and imaging modalities . when reviewing the guidelines , ct and mri also refer to ct angiography ( cta ) and mr angiography ( mra ) , fig . 
the halo sign typically resolves within 24 weeks of glucocorticoid therapy [ 23 , 24 , 2835 ] and has not been prospectively studied as a marker to assess disease activity . majority of the us studies in the slr ( n = 16 / 17 studies ) in gca tested for the halo sign . 
analysis of 8 studies ( 605 patients ) comparing the halo sign to a clinical diagnosis of gca revealed a positive likelihood ratio ( lr + ) of 19 , negative likelihood ratio ( lr ) of 0.2 with a pooled sensitivity ( sn ) of 77% and specificity ( sp ) of 96% . 
when the halo sign was compared with tab as the reference standard , a comparably good diagnostic performance was obtained ( n = 7 studies , 289 patients )  . 
the inclusion of vessel stenosis or occlusion on us did not provide further diagnostic accuracy versus halo alone [ 21 ] , since vascular stenosis or occlusion occurs due to inflammatory wall swelling , which is a correlate of the halo sign [ 9 , 23 , 32 , 36 , 37 ]  . 
imaging should ideally occur within 1week of glucocorticoid therapy initiation , as treatment rapidly reduces the sensitivity of imaging beyond this time frame [ 9 , 2325 ]  . the working group highly agreed based on expert opinion that imaging examinations must be done by trained specialist using appropriate equipment , operational procedures and settings . 
 development of training programmes , as well as national and international courses for imaging in lvv ( particularly for us ) is needed to facilitate implementation of these recommendations . cranial giant cell arteritis role ofultrasound incranial giant cell arteritis ultrasound should be the primary imaging test in patients with cranial symptoms due to a high level of evidence , good test performance , rapid access , lack of radiation or need of contrast material , safety , with relative low costs compared with other modalities . 1 3 968 la radiologia medica ( 2019 ) 124 : 965972 role ofmagnetic resonance imaging incranial giant cell arteritis high - resolution mri refers to the use of 1.5 to preferably 3 tesla mri to visualize vessel wall thickening and contrast enhancement as signs of vasculitis in the superficial temporal and occipital arteries . 
 thus , based on quality evidence and high agreement , mri of the cranial arteries can be used as an alternative to diagnose gca if us is not available or inconclusive . when mri was compared to tab , mri yielded a sn of 93% and a sp of 81% ( n = 6 studies , 443 patients )  . 
it is tempting to compare these results to that of us , and to consider better diagnostic accuracy in mri ; however , these data must be interpreted with caution . 
for example , in most mri studies , tab was only performed in cases with high a suspicion of gca , while in us studies , most patients underwent a tab [ 21 ]  . 
mri allows for the detection of concurrent structural lesions such as vessel wall thickening , luminal stenosis , occlusion , as well as arterial wall enhancement [ 21 ]  . 
specific sequences ( laid out in the eular guidelines ) are required to image both the arterial wall and lumen . advantages of mri include standardization of data acquisition , assessment of multiple cranial and extracranial arteries , including the aorta . 
this remains an area that requires further study [ 48 ]  . challenges with full mra include specific technical settings , multiple coils and long acquisition time in the scanner . 
since patients with suspected gca are treated with high dose glucocorticoids prior to completing investigations , mri must be performed urgently within 4days of treatment initiation to avoid false negatives . role ofpositron emission tomography andct scan incranial giant cell arteritis utilization of pet . 
practically , most centers do not have rapid access to pet which limits its use in routine practice . large vessel giant cell arteritis lv - gca can present with the absence of typical cranial symptoms and non - specific complaints . 
if gca cannot be confirmed or excluded based on clinical , laboratory and imaging results , use of tab and / or additional imaging is warranted , as it may be a case of lv - gca . 
based on expert consensus , the working group agreed that mural inflammation and / or luminal changes in extracranial arteries present on either us , mri , ct and / or pet support the diagnosis of lv - gca . 
notably , tab has a lower sensitivity in patients with predominant lv - gca as compared with cranial gca [ 12 , 13 , 50 ]  . role ofultrasound inlarge vessel giant cell arteritis in patients with a high clinical suspicion of gca with negative or inconclusive temporal artery scans , assessment of axillary and other cranial and / or extracranial arteries is valuable . 
despite this , based on expert consensus , the working group endorses assessment of axillary arteries . currently , no study has answered whether us is useful to assess relapse or monitoring of disease activity [ 29 ]  . 
also , new large vessel vasculitis lesions have been reported in up to 10% of gca patients followed by serial us despite treatment [ 34 ]  . role ofmagnetic resonance imaging inlarge vessel giant cell arteritis no study was identified in the slr addressing the role of mri for evaluating extracranial lv - gca . 
mri can be used to monitor inflammation and / or aortic dilatation . role ofpositron emission tomography andct scan inlarge vessel giant cell arteritis the working group agreed that ct and pet could not be recommended in diagnosing cranial gca . 
this is pertinent 1 3 la radiologia medica ( 2019 ) 124 : 965972 in elderly patients with constitutional symptoms without specific clinical features of gca and / or polymyalgia rheumatica ( pmr )  . 
this example highlights how the performance of a diagnostic test is influenced by the reference standard , and that a reliable standard is needed in extracranial lvv to facilitate future studies . in the same study by blockmans etal . 
two - thirds of patients in full clinical remission still had a positive pet at both follow - up visits , and pet scores did not significantly differ between remission and relapse . 
whether ongoing tracer uptake in patients in full clinical remission is caused by low - grade inflammation or remodeling , and whether targeting treatment to modify these changes has any impact on future outcomes requires further studies [ 21 ]  . disadvantages of pet include high costs , lower availability , radiation exposure , rapid reduction of sn to 36% after 10days of glucocorticoid treatment and misinterpretation of atherosclerosis as lvv with inexperienced readers [ 53 , 54 ]  . ct may be useful to detect structural lesions and vessel wall inflammation while enabling a higher resolution with shorter procedural time compared to mri . 
 there is only one small study ( 24 patients ) that reported a sn of 73% and sp of 78% using cta compared to a clinical diagnosis of gca [ 48 ]  . takayasus arteritis the taskforce agreed based on expert consensus , that us , pet and / or ct may be used as alternative imaging modalities in patients with suspected of tak . 
note , us is of limited value for assessment of the thoracic aorta . role ofultrasound intakayasus arteritis no studies have evaluated us in the diagnosis of tak , but it is of value in the assessment of patients with upper and lower limb claudication . 
us can be used to screen for structural damage in patients with signs or symptoms of stenosis , occlusion , aneurysm and / or in those with recurrent / persistent large vessel inflammation . 
however , us has not been able to demonstrate the capability to differentiate active disease from remission in tak [ 55 ]  . role ofmagnetic resonance imaging intakayasus arteritis based on expert consensus and a high level of agreement , patients with suspected tak should be investigated with mri assuming prompt availability and expertise . 
the most significant limitation of mri is availability . role ofpositron emission tomography andct scan intakayasus arteritis no studies have evaluated pet in tak ; it may be useful in patients suspected to have infection or malignancy . 
one small study ( 25 patients ) using cta compared to conventional angiography for diagnosing tak revealed a sn and sp of 100% [ 58 ]  . role ofimaging infollowup ofgiant cell arteritis andtakayasus arteritis in patients with lvv in full clinical and biochemical remission , the utility of additional imaging to determine disease activity is unknown . 
involved extracranial arteries may have residual inflammatory changes that remain for months , 1 3 970 la radiologia medica ( 2019 ) 124 : 965972 making them valuable targets to assess for disease remission [ 28 , 30 , 31 , 34 , 35 ]  . cranial and lv - gca . 
studies to clarify the role of imaging in disease monitoring are also required . mra , cta and / or us may be used for long - term monitoring of structural damage to detect stenosis , occlusion , dilatation and / or aneurysm formation . 
risk factors for aortic dilatation include baseline aortic inflammation , male sex , hypertension and smoking history [ 52 , 60 ]  . angiography conventional angiography was not evaluated in the slr though it was the gold standard in diagnosing lvv . 
based on expert opinion , the task force was in agreement that due to the invasiveness , high resource utilization , procedural risk and lack of vessel wall morphology evaluation , angiography should be superseded by modern imaging modalities . 
the main indication for conventional angiography in lvv is for interventions such as angioplasty or stenting [ 61 ]  . conclusions prompt recognition of lvv is vital to prevent complications and harms of unnecessary treatment . 
as these imaging modalities have reshaped our understanding of lvv , they have led to new unexplored questions . mri and pet / ct will have an expanding role in the diagnosis and monitoring of lvv as us is operator dependent and lacks the ability to assess the thoracic aorta . 
us in comparison has good test performance , rapid access , lack of radiation or need for contrast material , along with a relative low cost . going forward , there is a need for prospective studies comparing the diagnostic value of us to mri and pet / ct . 
studies to clarify whether a standardized hierarchical approach to assess different vascular territories ( e.g. , temporal , carotid , subclavian and axillary arteries ) with us , or other imaging modalities improve the diagnostic certainty of as novel treatments are explored in lvv , the need for better classification criteria with a greater emphasis on imaging is required . 
by means of t2 - wi , ece was evaluated in a qualitative manner , according to pi - rads v.2 ( two groups with low and high risk of ece ) ; sensitivity and specificity were calculated for both groups . 
we performed a quantitative analysis on two tractographic parameters , fractional anisotropy ( fa ) and apparent diffusion coefficient ( adc ) and computed the ratio between the lesion quadrant and its contralateral ( l / h ratio )  . 
these cut - off values were used in association with t2 - wi to reassess patients and to evaluate whether specificity and sensitivity of ece detection change . results t2 - wi showed a sensitivity of 80% and a specificity of 71% in detection of ece . 
the simultaneous use of t2 - wi and tractography revealed high sensitivity ( 100% ) on patients with low suspect of ece ( on t2 - wi ) and high specificity ( 83% ) on patients with high suspect of ece ( on t2 - wi )  . conclusion the morphologic component of t2 - weighted imaging and functional aspect of dti should be interpreted together to more successfully assess the presence of ece . keywords prostate cancer extra - capsular extension dti tractography staging introduction radical prostatectomy is a commonly used treatment modality for localized prostate cancer that has been shown to present higher cancer - specific survival than conservative management in high - risk patients [ 1 , 2 ]  . radical retropubic prostatectomy ( rrp ) is one of the most commonly used surgical techniques and provides excellent long - term cancer control in patients with clinically localized prostate cancer ( pca )  . 
erectile dysfunction ( ed ) is one of the complications after rrp , and the recovery of * matteo catania id634iff@studenti.univr.it 1 ospedale policlinico gb rossi , verona , italy erectile function is quantitatively related to the preservation of the neurovascular bundles ( nvbs ) [ 3 ]  . 
however , extra - capsular extension ( ece ) is found in a significant number of patients with clinically localized prostate cancer treated with radical prostatectomy [ 5 ]  . 
therefore , it would be valuable to assess the risk of ece before surgery for correct therapeutic planning [ 1 ]  . several studies have investigated the role of preoperative mri in patients with prostate cancer to evaluate ece [ 1 ]  . 
the method is based on the sensitivity to anisotropic diffusion of the water protons in the biological tissues with a strictly orientated texture , such as nervous central and peripheral fibres . 
in this type of tissues , the spread of water protons is not accidental or brownian , but oriented along a specific axis , thus being referred to as anisotropic [ 10 ]  . 
 through the measurement of fractional anisotropy ( fa ) for each single voxel in at least six non - collinear and noncoplanar directions , dti can quantify the phenomenon of anisotropic diffusion . 
by integrating the fa values of all voxels , it becomes possible to represent the direction of the nerve fibres in all three dimensions of the space , guaranteeing both quantitative and qualitative information [ 11 ] .this technology has also recently been used also to map peri - prostatic nerve fibres ( pnf ) because it offers optimal representation of the peri - prostatic plexus , and could be used as a potential biomarker in predicting ece in patients with pca [ 3 , 12 ]  . 
however , the assessment of ece using t2 - wi is based on a strictly morphologic viewpoint , whereas the dti is a functional marker and cannot be directly compared with t2 - weighted imaging findings due to the low spatial resolution of the dti sequence . 
we believe that instead of comparing the accuracies of t2 - wi and dti with tractography in determining ece , these two sequences should be used together . purpose the aim of this study was to evaluate the role of dti ( with fibretracking ) and t2 - wi used together for predicting extra - capsular extension in patients with localized prostate cancer , using radical prostatectomy as the reference standard . method andmaterials patient selection this prospective study was approved by our institutional review board and included male patients with biopsy - proven clinically significant prostate cancer ( gleason > 6 ) in the peripheral zone , candidate to radical prostatectomy , who gave their written informed consent to mri examination before surgery . 
after standard anatomical tse and dwi sequences , the diffusion tensor imaging was acquired in 32 directions ( tr / te 1449 / 88ms , thickness 3mm , b - value = 0.800s / mm 2 ) , with a scan duration for dti sequence of 3min and 14s . 
at last , the dynamic imaging was performed during gadolinium chelate injection ( 0.1mmol per kilogram of body weight gadolinium chelates , gadovist , schering , berlin , germany ) with a power injector ( medrad spectris solaris ; medrad , pittsburgh , pa , usa ) at a rate of 2ml / s . 
the dynamic imaging consisted of the repetition of 14 t1 dixon acquisitions after contrast injection . image analysis two types of analysis had been conducted in this study : a qualitative analysis and a quantitative one . qualitative analysis : morphologic assessment ont2weighted imaging two radiologists with 20 and 7years of experience in prostate imaging ( readers 1 and 2 , respectively ) independently reviewed the images at a pacs system ; just in case there was no consensus between the two radiologists , then it was tried to reach a consensus together . 
in this way , we tried to overcome the bias that could arise from the difference experience of the two radiologists . ece was evaluated according to pi - rads second version on t2 - w images . 
we wanted to keep reader 1 in both analyses as he has more experience ( 20years ) , while we replaced reader 2 with reader 3 in the quantitative analysis so that it was blind to the qualitative analysis . 
the reader 1 instead performed the qualitative and quantitative analyses in two different periods at time , so as not to correlate the two analyses . the reconstruction was performed by using the fiber tracking software provided by philips ( version 4.1 ) , which consisted of a deterministic tracking algorithm based on the criterion of linear propagation using the following parameters : angle threshold of 45 , fa threshold of 0.15 and minimum length threshold of 5mm , analogously to other published studies [ 11 ]  . in the dti post - processing phase , the dti images were synchronized with the axial t2 - weighted images to correct eventual movement artefacts of the patients ; subsequently , the axial t2 - w images were fused with the synchronized dti images , obtaining a t2 - w / dti hybrid images . 
b voluminous lesion of the left posterior quadrant with extracapsular invasion ( arrows ) and involvement of the seminal vesicle and peri - prostatic adipose tissue 1 3 la radiologia medica ( 2019 ) 124 : 946954 fig . 
2 a positioning of the rois in a patient with lesion involving the capsule in the posterior right quadrant : on an axial plane passing through the lesion , two orthogonal planes are tracked passing through the centre of the gland , dividing it into four quadrants and placing a roi on the side of the lesion ( red ) and in the opposite side ( green ) , obtaining the tractographic reconstructions shown in b after software elaboration the number , the fa and adc values and the length in millimetres were calculated for each reconstructed tractography at the tumour level , both on the lesion quadrant and on the opposite healthy side . pathologic data collection surgical specimens were assessed by the dedicated genitourinary pathologist ( 19years of experience ) and processed according to the stanford protocol [ 13 ]  . 
reader 3 reviewed the records in the pathology database to evaluate the status of extra - prostatic extension , which is the preferred term for the presence of tumour beyond the confines of the prostate gland ( note h in the stanford protocol ) , and descriptors of extra - prostatic extension ( focal versus non - focal ) were used [ 13 ]  . the patient population was clustered into two groups according to the extra - prostatic extension status : the first group with intra - prostatic tumour ( controls group ) and the second group with histological extra - prostatic extension , both focal and non - focal ( cases group )  . statistical analysis in the qualitative analysis , in both groups ( a and b ) based on t2 - wi , sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) were calculated for assessment of ece . in the quantitative analysis , only in the group of patients with extra - capsular infiltration ( cases group ) , the ratio was calculated for each of the five output parameters of the tractographic reconstruction between the lesion quadrant and the contralateral one ( t3 / health ratio )  . 
these analyses were applied to the fa and adc values . results pathological assessment ofece based on radical prostatectomy , ece was found in 15 of 36 ( 42.7% ) patients ; in this group ( cases group , with histological evidence of ece ) , the lesion infiltrating the capsule was localized : in the right anterior quadrant in 2 / 15 ( 13% ) , in the right posterior quadrant in 6 / 15 ( 40% ) , in the left posterior in 4 / 15 ( 27% ) and finally in the left anterior quadrant in 3 / 15 ( 20% ) ; thus , the cases group was formed by 15 patients , while the controls group was composed by 21 patients . qualitative analysis on the t2 - wi , the morphologic evaluation of ece was found in 18 patients ( group a ) , while in the other 18 patients there was no evidence of ece ( group b ) ( table2 )  . 
thus , the ece assessment on t2 - wi showed values of sensibility , specificity , ppv and ppn , respectively , of 80% , 71% , 66% and 83% ( table2 )  . table 2 a representation of the two groups ( low and high risk of ece ) based on the presence or absence of ece on the t2 - w images , b calculation of the sensitivity , specificity , npv , ppv , fn and fp of t2 - w images t2 - wi histological ece ( cases ) histological no ece ( controls ) total t2 - w risk ece t2 - w risk ece sensitivity specificity n = 3 n = 6 quantitative analysis the t3 / health ratio of the five tractographic parameters showed a univocal trend only for the fa and adc parameters ; for fa , all the ratios were < 1 ; for adc , they were all > 1 ( table3 )  . 
 these cut - off values are potentially applicable as an aid in the reporting of multiparametric mri of the prostate in preoperative local staging to improve surgical planning and treatment decisions . given the low spatial resolution of dti , trying to identify direct evidence of ece on dti maps will be limited and nobody can think to use only dti in the ece evaluation . 
there is suspect of ece on t2 - w images : this is confirmed with dti and tractographic reconstructions ( fa = 0.68 [ cut - off < 0.87 ] and adc = 1.41 [ cut - off > 1.23 ] ) 1 3 la radiologia medica ( 2019 ) 124 : 946954 fig . 
6 blandaltman analysis related to interobserver concordance of the adc and fa parameters fundamentally morphologic , dti is known to provide functional information . of the values on different scanners , and we are already applying in this sense . therefore , the key of our analytic approach was to comprehensively incorporate both sequences in determining ece of prostate cancer rather than to directly compare the accuracies of the two sequences . a further important result of our study was represented by the high interobserver agreement values , demonstrating that dti of the nvbs is reliable technique . 
moreover , neither the bias nor limits of agreement between dti output metrics across repeated assessments were not clinically important for either observer , suggesting the potential repeatability of the technique [ 11 ]  . 
however , repeated dti acquisitions under the same conditions were not performed . with regard to the feasibility in clinical practice , we are convinced that it is absolutely feasible as the sequence does not last long ( 3min and 14s ) and the post - processing analysis lasts about 2 min ( launch the application , draw two rois and calculate the ratio between two numbers )  . 
regarding reproducibility on different machines , we have no data regarding the reproducibility of the same sequence on different scanners in prostate imaging as we have used only one scanner . 
having said that , we know from the literature that the quantitative analysis of adc and fa values obtained in the dti sequence provides different values depending on the scanner used in neuroimaging . 
in fact , we have tried to limit this variability by normalizing the values of fa and adc with the healthy contralateral side so as to obtain an absolute value and not a measurement . 
this is in fact a preliminary study , and surely other studies will be needed in this area , both to implement the number of patients studied , and to assess the reproducibility in the study we did not use the endorectal coil ; even if panebianco etal . 
we aligned ourselves with the di paola method [ 11 ]  . the main limitations of the present study were the potential miscount of nerve fibres because of the presence of linear non - nerve structures ( fibromuscular tissue , arteries and veins ) and the relatively small number of patients included in the study . 
analyzed variables included patients sex , age , cirrhosis etiology , childpugh status , size of the lesion , liver segment , subcapsular or central liver site , type of imaging used for fusion ( mr / ct ) , and the presence of surrounding anatomical landmarks ( sal ) < 3cm from the index lesion . results the primary efficacy was 59.4% ( 22 / 37 nodules ) ; nine lesions ( 24.3% ) were partially ablated ( pa ) , six lesions ( 16.7% ) were mistargeted ( ma )  . 
the outcome of the procedure is heavily affected by the presence of sal . keywords hepatocellular carcinoma fusion imaging thermal ablation * marco calandri marco.calandri@unito.it 1 radiology unit , department ofoncology , san luigi gonzaga hospital , orbassano ( torino ) , university oftorino , turin , italy 2 department ofsurgical sciences , radiology institute , citt della salute e della scienza , torino , university oftorino , turin , italy 3 gastro - hepatology unit , department ofmedical sciences , aou citt della salute e della scienza , turin , italy 4 liver transplant center , a.o.u. 
citt della salute e della scienza di torino , university ofturin , turin , italy introduction image - guided percutaneous thermal ablation is a well - established curative treatment for the very early and early stage of hepatocellular carcinoma ( hcc ) [ 1 , 2 ] that remains the sixth most common cancer worldwide and the third leading cause of cancer - related deaths in the world [ 3 ]  . nowadays , ultrasound ( us ) guidance , especially in europe and eastern countries , remains the most used guiding modality because of its several advantages , such as real - time control , accessibility , relatively low cost without ionizing radiation exposure [ 1 , 4 ]  . nevertheless , due to the great recent developments in the ct and mri fields , interventional radiologists are asked to reach and treat percutaneously smaller nodules , not clearly detectable on conventional ultrasound imaging [ 5 , vol . : ( 0123456789 ) 1 3 1044 la radiologia medica ( 2019 ) 124 : 10431048 6 ]  . 
indeed , according to the literature data , approximately 14.633.1% of the hcc nodules are inconspicuous on conventional b - mode evaluation and ablation could not be performed under the sole us guidance [ 4 , 79 ]  . contrast - enhanced us ( ceus ) has been reported as a valuable aid in these cases to target properly the nodules . 
 however , because of poor conspicuity , location or low arterial phase wash - in , there are some cases ( up to 45% in the literature series ) in which even ceus fails to clearly detect the nodule [ 10 ]  . in recent years , fusion imaging ( fi ) has been proposed as a solution to overcome these limitations of us guidance , enabling a real - time display of mr or ct images on the same screen during ablation [ 1115 ]  . despite the presence in the literature of several reports on this topic , factors affecting fi guidance during ablation of us inconspicuous hcc nodules have never been fully investigated , especially if performed under conscious sedation , when patients can breathe spontaneously , potentially affecting the synchronization process of fi . the aim of our study is to evaluate , in this specific setting , the most relevant factors affecting the outcome of thermal ablation of completely inconspicuous hcc nodules with fi guidance . undetectable with conventional b - mode ultrasound only . 
 among these , 21 nodules were visible with good conspicuity at ceus examination by injecting 2.4ml of sonovue ( bracco , milan , italy ) ; 37 nodules in 26 patients were completely undetectable at b - mode or ceus examination and fi guidance was performed . 
variables extracted from the database or updated by review of electronic medical records for each patient and procedure included sex , age , cirrhosis etiology , childpugh status , size of the lesion , liver segment , subcapsular or central liver site , type of imaging used for fusion ( mri sequences or ct phases ) , and the presence of surrounding anatomical landmarks ( sal ) ; sal were defined as any anatomical structure ( such as vessels larger than 3mm , cysts or ligaments ) no more distant than 3cm on axial ct or mr images from the index lesion . ablations were done under conscious sedation by interventional radiologists using a 17 - gauge rfa electrode multi - tined needle ( med - italia , medolla , italy ) with a radiofrequency generator ( rf3000 , 200w capacity , radiofrequency ablation system , boston scientific )  . 
before the needle insertion , 10ml of 2% lidocaine hydrochloride was injected at the puncture site . materials andmethods study design this study was approved by the institutional ethics review board . 
the prospectively compiled interventional radiology liver ablation registry of our institution was retrospectively evaluated and updated by review of the electronic medical records to identify consecutive patients who underwent percutaneous liver ablation for the treatment of hcc nodules from january 2016 through may 2018 . patient selection , ablation eligibility criteria andtechnique patients were considered for percutaneous ablation in case of no more than three hcc nodules , measuring 3cm each . 
 hcc diagnosis was performed with cross - sectional imaging ( ct or mri ) according to easl criteria . indication for ablation was discussed at the institutions multidisciplinary hcc tumor board . 
with the plane registration , the physician found the same plane on real - time us and uploaded ct or mr images ( any plane can be used but , for simplicity , the umbilicus axial plane was considered the first choice ) [ 16 ]  . 
other available functions , such as rotate or drag , were useful to optimize the real - time us - cect / cemri matching [ 17 ]  . assessment oftumor ablation results standardized terminology and reporting criteria for tumor ablation were utilized to determine ablation endpoints [ 18 ]  . 
residual unablated tumor ( partial ablation pa ) was defined as the presence of peripheral or nodular enhancement within 1cm of the ablated area at the first imaging follow - up ( triple - phase contrast - enhanced computed tomography [ ct ] or magnetic resonance [ mr ] )  . 
we defined missed ablation ( ma ) as the condition of complete 1 3 la radiologia medica ( 2019 ) 124 : 10431048 1045 table 1 patients and nodules characteristics mistargeting of the nodule at the first ablation attempt , when the distance between ablated volume center and ideal target point preoperatively established was greater than 5mm [ 19 ]  . 
local tumor progression ( ltp ) was defined as the appearance of tumor foci at the edge of the ablation zone or within 1cm after at least one cross - sectional imaging had demonstrated complete ablation . statistical analysis the normality of distribution for continuous numeric data was assessed with saphirowilk test . 
thus , according to the defined groups , data were reported as mean , standard deviation ( sd ) , and ranges for normally distributed variables , while median , ranges , and interquartile ranges were used for not normally distributed variables . 
 statistical analysis was performed using graphpad stats software ( 2018 )  . results from january 2016 to may 2018 , a total of 37 hcc nodules in 26 patients ( see table1 for nodule and patient characteristics ) underwent image - guided ablation relying only on fi guidance in consideration of their undetectability at conventional b - mode or ceus imaging . 
 ( see table1 for patients characteristics . ) according to claviendindo classification , only two minor complications requiring standard medical therapy ( grade i ) were observed after two ablation sessions . 
according to cirse classification of complications , only two nonsevere complications occurred ( grade ii )  . complete ablation ( primary efficacy ) was obtained in 22 / 37 nodules ( 59.4% ) ; nine lesions ( 24.3% ) were partially ablated ( pa ) , whereas six lesions ( 16.7% ) were mistargeted ( ma )  . 
among the seven remaining nodules , in four cases ( two patients ) , intrahepatic progression was observed and tace was performed ; in two cases , patients underwent liver transplantation , and in one case , patient was lost to followup . 
 discussion our study investigated the role of fusion imaging guidance in treating hcc nodules completely undetectable at conventional b - mode us or ceus evaluation . the main findings of our study were : the primary efficacy of fi - guided treatments is 59.4% ; the secondary efficacy reaches the 81.1% with a ltp rates at 1year f.u. 
 [ 19 ] analyzed a series of fi - guided ablation of completely inconspicuous liver metastases and they demonstrated a similar primary success rate ( 56.7% 17 / 30 patients , in the pet - ct group )  . 
in our series , however , even in case of missed ablation at the first ablation , the ablation scar was used as reliable internal anatomical landmark to repeat the fi targeting and to perform ablation . 
indeed , we reached a 100% ca as a second attempt with an overall ltp rate ( 6.7% ) in line with the other literature reports about poorly visible or visible nodules [ 13 , 22 , 26 ]  . as for the anatomical landmarks , they are well known among fi operators for their role in the second part of the plane and point registration [ 17 ]  . 
our study suggests for them a role of paramount importance in case of ablation of completely inconspicuous nodules in procedures performed in critical technical conditions , such as under conscious sedation , spontaneous breathing and with a pre - acquired ct . 
 in fact , with endotracheal general anesthesia , the breath of the patient can be well controlled using a breathing machine for as long as 2min , greatly facilitating co - registration and subsequent ablation . furthermore , our series was characterized by the usage of pre - acquired cross - sectional imaging ( ct or mr )  . 
in other series , the availability of ct in the operatory room allowed for acquisition of real - time ct images with the patient already under general anesthesia and in the desired decubitus , so the correspondence between ct and us images is increased [ 27 ]  . however , these facilities are rarely available in most of the ir services worldwide and physicians are usually asked to merge with real - time us a pre - acquired ct or mri in supine position . 
therefore , we believe our study gives pertinent information on the relevance of anatomical landmarks in a specific but widespread clinical setting of fusion imaging . as for other possible predicting factors that may affect the outcome of the ablation , our study did not find any significant statistical correlation . 
the ct scans were reviewed by three different radiologists , who evaluated the findings potentially associated with acute rejection such as air trapping , tree - in - bud , consolidations , crazy paving , ground - glass opacity , bronchiectasis , thickening of intralobular or interlobular septa and presence of pleural effusion . 
the association between a tissue diagnosis of acute rejection and the above - mentioned ct findings was assessed using a multivariate model of logistic regression . results based on our results , none of the ct findings included in the study , alone or in combination , showed significant statistical association with the diagnosis of acute rejection . conclusion ct is a very useful technique for the assessment of lung transplant recipients although it has limited accuracy for the assessment of acute rejection . 
 oneand five - year survival rates are approximately 75% and 50% [ 1 , 2 ]  . postoperative graft surveillance includes laboratory data , pulmonary function tests , bronchoscopy with broncho - alveolar lavage ( bal ) and biopsies , and imaging . 
many studies have examined the role of hrct in the diagnosis of chronic rejection , but only a few attempted to assess the accuracy of hrct for the diagnosis of acute rejection [ 3 ]  . 
the aim of this study is to evaluate the sensitivity , specificity and predictive values of hrct for the detection of acute rejection ( ar ) and to determine which computed tomography findings are associated with histopathologically proven acute rejection . materials andmethods study population one hundred sixty lung transplants have been performed at our institute between 2005 and 2018 . 
our final population included 78 patients ; 37 patients with no histopathologic evidence of pulmonary abnormalities ( control group ) ; and 41 patients with a diagnosis of acute rejection . 
 our study was approved by the ethical committee of our hospital . histopathology sampling in our institution , symptomatic and asymptomatic lung transplant recipients are followed up with a regular schedule of blood work , respiratory function tests and clinical assessment . 
a bronchoscopy and ct scan are performed at 1month , 6months and then yearly or when required clinically . bronchoscopy includes a broncho - alveolar lavage and multiple trans - bronchial biopsies ( tbb ) ; a minimum of 6 samples is usually procured from all lobes of one lung . 
the degree of acute rejection is evaluated according to the conventional criteria established for pulmonary rejection : degree a0 , no rejection ; degree a1 , minimal rejection ; degree a2 , mild rejection ; degree a3 , moderate rejection ; degree a4 , serious rejection [ 4 ]  . 
bal samples are also assessed for standard and opportunistic infections , including bacteria , fungal , and viral species . ct scan evaluation ct scans were acquired by lightspeed 16 slice scanner ( ge healthcare , usa ) or lightspeed vct 64 slice scanner ( ge healthcare , usa ) systems . 
when used , the contrast medium was administered by a mechanical injector ( medrad double head ct injector stellant siemens , indianola , pa , usa ) ; 30ml of normal saline solution was administered at the end of the intravenous contrast medium infusion . 
the arterial phase , conventionally acquired in the caudocranial direction , started 6s after reaching the peak of the contrast medium concentration by smart prep technique , with a region of interest on the common trunk of the pulmonary artery . 
the late phase was acquired 50s after the contrast medium administration . images were later reconstructed in the post - processing phase , by dedicated consoles ( advantage windows 4.6 , ge ) , to obtain reconstructions by multi - planar images ( mpr , multi - planar reconstruction ) , images that enhance the contrast density ( mip , maximum - intensity projection ) or highlight hypodensity on a hyperdense background ( minip , minimum intensity projection ) , and volumetric images ( vr , volume rendering ) , to evaluate both vascular and bronchial structures . 
images were then retrospectively analyzed by image archiving and communication systems ( pacs , ge medical systems ) , with two high - definition screens barco ( 5 megapixel ) as visualization support . 
ct scans were assessed by visualization of a window for both soft tissues ( level , 40 uh ; width , 440 uh ) and lung ( level , 700 uh , 1 3 1002 la radiologia medica ( 2019 ) 124 : 10001005 width , 10001500 uh )  . 
a single thoracic radiologist ( ad ) selected the ct scans included in the study . three independent thoracic radiologists ( ad , sc and gm ) reviewed all the ct scans ; they revised and evaluated the single ct tests in a consensus . 
the following ct parameters were evaluated in a non - quantitative fashion ( absent or present ) in order to express a judgment on the presence of acute rejection : air trapping , tree - in - bud , consolidations , crazy paving , ground - glass opacity , bronchiectasis , thickening of intralobular or interlobular septa and pleural effusion . statistical analysis descriptive statistics of the population are presented using absolute and relative frequencies , as appropriate . 
multivariate analysis was performed with the logistic regression model . results among the 41 patients with ar , the degree of acute rejection was a1 and a2 except for 7 patients ( 17% ) with a3 rejection . 
three years after lung transplantation she has a recurrence of acute rejection characterized by peribronchial wall thickening ( yellow arrows ) and tree - in - bud opacities ( red circle )  . 
according to fishers exact test , none of the ct findings included in the study , alone or in combination , showed any significant statistical association with the diagnosis of acute rejection , as showed by p values > 0.05.figures1 , 2 , 3 , 4 , 5 show some cases with the above mentioned ct findings . 
it may occur early ( days or weeks ) or late ( months or years ) after transplantation and require treatment adjustments in case of recurrence [ 6 ]  . 
 recurrent episodes of acute rejection may increase the chance of developing chronic rejection , which is the main cause of late morbidity and mortality in lung transplant recipients [ 7 ]  . 
tbb is the gold standard for the diagnosis 1 3 1004 la radiologia medica ( 2019 ) 124 : 10001005 with the diagnosis of acute rejection [ 3 ]  . 
their population with acute rejection consisted of 34 patients . our results are consistent with the findings of gotway and colleagues , although there are some methodological differences between the two studies . 
as showed in other studies , the casual tbb procurement is a significant bias for the assessment of acute rejection , especially in its mild - moderate phases [ 8 , 9 ]  . 
a limitation of both studies is the small number of cases of severe rejection ( 7 patients with a3 and no patient with a4 in our study ) included in the analysis , a finding that could possibly increase the sensitivity of single ct results , as demonstrated by other authors [ 11 ]  . in 6 cases , despite evidence of acute rejection on histopathology , the ct was considered normal , without any ct abnormality , probably because of the early stage of ar . 
 similarly , in the study by gotway , 5 patients with negative ct scans showed histopathologic diagnosis of acute rejection . on the other hand , in 29 of 37 patients ( 78% ) with no histopathologic evidence of acute rejection ( control group ) , ct scans identified at least one of the radiological abnormalities suggested as possible indicators of acute rejection . 
however , their population consisted of only 8 patients diagnosed with acute rejection by pathology , of which only 5 had significant ct findings , mostly bilateral . unlike the studies by loubeyre etal . 
 [ 12 ] , in our research we did not take into account repeated findings in the same patient , but only those corresponding to the first biopsy - proven episode of acute rejection . 
two - thirds of the centers reporting to the international society for heart and lung transplantation ( ishl ) registry include a tbb in their surveillance protocol within the first year post - transplantation ; nevertheless , the role of tbb in completely asymptomatic patients is still controversial . 
surveillance with tbb showed the presence of acute rejection in up to 73% of clinically and physically stable patients , highlighting that a timely treatment of these silent episodes could reduce the development of chronic rejection [ 8 ]  . it is a matter of debate whether episodes of grade a1 ar without recurrence or progression to higher grades may be a significant independent predictor of obliterative bronchiolitis . 
none of the ct findings included in the study , alone or in combination , showed any significant statistical association 1 3 la radiologia medica ( 2019 ) 124 : 10001005 1005 of acute rejection may influence the likelihood and course of subsequent episodes . as demonstrated in our study , hrct has limited accuracy for the assessment of acute rejection , and none of the findings considered in our study is significantly associated with acute rejection . 
it has proven value for the characterization of other postoperative complications [ 13 ] such as bronchial stricture and dehiscence , infections , vascular complications , malignancies and chronic rejection . 
 moreover , ct scan may facilitate trans - bronchial biopsies by guiding the sampling of the most affected areas of the lung . in conclusion , hrct is a very useful technique and may support clinicians in the follow - up of lung transplant recipients . 
in adult populations , 9398% of all scalp lesions are benign , with the most common diagnosis being trichilemmal cysts ( 41% of all scalp lesions ) , followed by epidermal cysts , lipoma , nevi , and sebaceous cysts [ 24 ]  . 
in pediatric populations , 9799% of all scalp lesions are benign , with the most common diagnosis being nevus sebaceous ( 60% of all scalp lesions ) , followed by infantile hemangioma , melanocytic nevi , and juvenile xanthogranuloma [ 5 , 6 ]  . 
a clear understanding of the scalps anatomy is essential for the topographic characterization of the lesion as the first step in the differential * hiroki kato hkato@gifu - u.ac.jp 1 department ofradiology , gifu university school ofmedicine , 1 - 1 yanagido , gifu501 - 1194 , japan diagnosis ( table1 ) , as the majority ( 82% ) of scalp lesions in adults originate from the skin layer [ 2 ]  . the rate of correct preoperative diagnosis for scalp lesions ranged from 13 to 27% among neurosurgery , plastic surgery , or general surgery departments [ 2 ]  . 
although radiological investigations of some scalp lesions have been reported [ 810 ] , to the best of our knowledge , there have been no review articles with emphasis on ct and mri features of scalp lesions . 
therefore , the aim of this review article is to describe a variety of cutaneous and subcutaneous lesions of the scalp in terms of the anatomic origin with emphasis on ct and mri features . anatomy the soft - tissue envelope of the cranial vault is named the scalp , extending from the external occipital protuberance and superior nuchal lines to the supraorbital margins and vol . : ( 0123456789 ) 1 3 la radiologia medica ( 2019 ) 124 : 10491061 1050 origin table 1 classification of scalp lesions melanocytic origin appendageal origin follicular differentiation benign malignant keratinocytic origin epidermoid cyst / dermoid cyst / teratoid cyst , keratoasquamous cell carcinoma , basal cell carcicanthoma , seborrheic keratosis melanocytic nevus , blue nevi noma , bowen disease malignant melanoma pilomatricoma , trichilemmal cyst / proliferating pilomatrical carcinoma , malignant prolifertricholemmal tumor ating tricholemmal tumor sebaceous differentiation apocrine and eccrine differentiation sebaceoma / sebaceous adenoma eccrine poroma , hidrocystoma , syringoma sebaceous carcinoma adenocarcinoma , porocarcinoma , apocrine carcinoma hematolymphoid origin langerhans cell histiocytosis , rosaidorfman disease , malignant lymphoma juvenile xanthogranuloma soft tissue origin adipocytic vascular neural origin others lipoma , lipoma variant infantile hemangioma , venous malformation / cavernatypical lipomatous tumor , liposarcoma angiosarcoma ous hemangioma lymphangioma lymphatic smooth and skeletal muscle leiomyoma fibrous , fibrohistiocytic and histiocytic dermatofibroma , keloid / hypertrophic scar , infantile myofibromatosis neurofibroma , schwannoma leiomyosarcoma dermatofibroma protuberance , fibrosarcoma merkel cell carcinoma , malignant peripheral nerve sheath tumor dermoid / teratoid cyst metastasis anchored laterally by each ear . 
the scalp consists of five histologic layers : skin , subcutaneous tissue ( superficial fascia ) , galea aponeurotica ( deep fascia ) , loose areolar connective tissue , and pericranium ( fig.1 ) [ 1 , 3 , 7 ]  . 
this single unit can move along the loose areolar tissue over the pericranium adherent to the calvaria . the skin is the outermost region of the scalp , which is composed of thin external epidermis and thick inner dermis , which both decrease in thickness with age . 
the epidermis is composed of stratified squamous epithelium , with a thickness of 0.040.4mthe dermis is usually thinnest over the forehead and thickest over the occipital region [ 1 , 3 ] with a thickness of 0.52.5mthe skin also contains closely arranged adnexa ( consisting of sebaceous glands , hair follicles , and eccrine and apocrine glands ) surrounded by dense networks of blood vessels and lymphatics [ 3 ]  . the subcutaneous tissue , also known as the subcutis or superficial fascia , is a fibrofatty layer that connects the skin to the underlying galea aponeurotica of the occipitofrontalis muscle and provides a passageway for blood vessels , nerves , and lymphatic tissue . 
at the vertex , the subcutaneous tissue has a thickness of 47mm . the galea aponeurotica , also called the deep fascia , is a strong , thin , tendinous sheath that descends laterally into the temporal fossa as the superficial temporal fascia . 
the galea aponeurotica has a thickness of 12mm . the loose connective tissue , which is also referred to as the areolar tissue , comprises the subgaleal layer between the galea aponeurotica and the pericraniuthis layer contains the most widely distributed connective tissues and is composed of a central dense collagenous layer surrounded by vascularized areolar tissue . 
this layer has several functions , including support and binding , fluid retention , defense , and nutrient storage . the periosteum covering the outer surface of the skull is known as the pericraniuthe pericranium is a fibrous membrane that is tightly attached to the outer table of the skull . 
laterally , it terminates at the origin of the temporalis muscle along the superior temporal line . imaging the skin layer presents on ct as a soft - tissue density and on mri as isointense to muscle . 
upon encountering cutaneous lesions arising from the skin layer , the depth of the lesion 1 3 la radiologia medica ( 2019 ) 124 : 10491061 1051 and the invasion of nearby subcutaneous tissue should be assessed by radiologists on the basis of ct and mri . the subcutaneous tissue layer appears as a hypodense area on ct and as an area with hyperintensity on t1and t2 - weighted mr images because of its fat content . 
on fat - suppressed contrast - enhanced t1 - weighted images , the enhancement of subcutaneous tissue can be observed because of its rich vascular network . the galea aponeurotica layer is shown on mri as an area that is isointense to muscles . 
in contrast , the loose connective tissue and the pericranium cannot normally be visualized by either ct or mri and can only be detected pathologically [ 7 ]  . the depth of tumor invasion is an important prognostic factor for local recurrence and distant metastasis after surgery . 
if cutaneous lesions invade the subcutaneous tissue , the subcutaneous tissue appears as an area of hyperintensity on fat - suppressed t2 - weighted images and as an area of hypointensity on t1 - weighted images . 
the tumor extends down to the cranial bone ; full - depth resection is required , including the dura if necessary . benign lesions trichilemmal cysts , proliferating trichilemmal tumors trichilemmal cysts , otherwise known as pilar cysts or isthmus - catagen cysts , are the most common form of intradermal or subcutaneous cysts of the scalp , accounting for 510% of the population . 
histologically , these cysts are lined by squamous epithelium , containing a granular layer ( trichilemmal keratinization ) that is filled with homogenous keratcalcifications are common features in trichilemmal cysts . 
the presence of calcification causes inhomogeneity on t2 - weighted images ; the lack of intralesional enhancement can be observed on contrast - enhanced images ( fig.2 ) [ 12 ]  . 
as the underlying skull vault and skin surface are not affected by trichilemmal cysts , enhanced soft - tissue components with irregular margins , invasion into surrounding structures , and erosion of adjacent bony tissue are indicative signs of malignant transformation . sebaceoma sebaceous neoplasms are uncommon cutaneous tumors arising in the sebaceous glands , which are responsible for secreting lipids and other substances into the hair follicle infundibulum [ 14 ]  . 
the scalp consists of five histologic layers : skin , subcutaneous tissue ( superficial fascia ) , galea aponeurotica ( deep fascia ) , loose connective tissue , and periosteum ( pericranium ) 1 3 1052 la radiologia medica ( 2019 ) 124 : 10491061 fig . 
the cystic wall is lined by stratified squamous epithelium , with sebaceous lobules present in , or adjacent to , the cystic wall . sebaceomas are located in the dermis and frequently expand downward to the subcutaneous tissue layer [ 16 ]  . 
in contrast , if the cystic cavities are filled with large amounts of keratin and hair , they appear as areas with hypoto isointensity on t1 - weighted images and hyperintensity on t2 - weighed images . epidermoid / dermoid / teratoid cysts epidermoid , dermoid , and teratoid cysts are common , related , cutaneous cysts lined by squamous epithelium , classified according to whether they are lined by simple squamous epithelium ( epidermoid cysts ) , the presence of skin adnexa in the cystic wall ( dermoid cysts ) , or the presence of other tissues , such as muscle , cartilage , or bone ( teratoid cysts )  . 
these types 1 3 la radiologia medica ( 2019 ) 124 : 10491061 1053 of cysts occur in the head and neck region , generally occurring in young to middle - aged adults with a male - to - female ratio of 3 : 1 . 
dermoid and teratoid cysts are usually found as congenital masses in pediatric patients [ 17 ]  . on ct and mri , these types of cysts appear as welldemarcated , oval - shaped , subcutaneous cystic masses adjacent to the overlying skepidermoid cysts appear as areas with isoto hyperintensity on t1 - weighted images and hyperintensity with variable hypointense foci , including internal linear dark debris , on t2 - weighted images ( fig.5 ) [ 10 ]  . 
although peripheral , thin - rim enhancement without central enhancement is usually observed , the rupture of epidermoid cysts results in the enhancement of internal septa and a thickened , irregular rim , with fuzzy enhancement in surrounding subcutaneous tissues [ 18 ]  . 
dermoid cysts typically appear as areas with hyperintensity due to their fat content on t1 - weighted images and variable intensities on t2 - weighted images [ 19 ]  . 
teratoid cysts show as the presence of calcification on ct , reflecting the formation of cartilage or bone . keratoacanthoma keratoacanthoma is a self - limiting , epidermal tumor that is cryptic because of its nosological position at the border between benignity and malignancy [ 20 ]  . 
 lesions show an intermediate intensity on t1 - weighted images and a mixture of intermediate and high signal intensities on t2 - weighted images with peripheral thin - rim enhancement [ 22 ]  . pilomatricoma pilomatricoma , which is also known as calcifying epithelioma , is a rare , benign tumor of the dermis or subcutaneous tissue , which originates from pluripotent cells that normally differentiate into hair matrix cells [ 8 ]  . 
a t1 - weighted image shows a exophytic , cup - shaped , well - demarcated cutaneous lesion ( arrow ) with central recesses of keratotic horn ( arrow head )  . 
approximately , half of the tumors occur in the head and neck region , followed by the upper extremities , trunk , and lower extremities ; the sites that are most commonly affected by pilomatricoma are the cheek , neck , eyebrows , and scalp [ 23 ]  . 
reticular and ring - like hyperintensities on fat - suppressed t2 - weighted and fat - suppressed contrast - enhanced t1 - weighted images are frequently observed , corresponding to intratumoral stroma and tumor capsule with various degrees of inflammatory cell infiltration and vascular proliferation , respectively ( fig.7 ) [ 8 ]  . 
 melanocytic nevi melanocytic nevi , which is also called moles , are common skin lesions that are characterized by benign clonal proliferation of cells expressing a melanocytic phenotype , with heterogeneous clinical and molecular characteristics [ 24 ]  . 
 melanocytic nevi are formed by nests of melanocytes in epidermal junctions ( junctional nevi ) , dermis ( intradermal nevi ) , or both compartments ( compound nevi )  . 
as the risk of malignant transformation of melanocytic nevi strongly depends on size , giant congenital melanocytic nevi are associated with an increased risk of malignant melanoma . melanocytic nevi present as flat patch lesions on the sk hyperdensity relative to soft tissue has been observed on ct owing to the melanin content of melanocytic nevi . 
although melanocytic nevi rarely invade the underlying fascia , muscle , or deeper structures , giant congenital melanocytic nevi may invade the subcutaneous tissue or beyond with ill - defined margins . neurofibroma neurofibroma is a benign nerve sheath tumor with a neuroectodermal origin , accounting for 5% of all benign soft - tissue tumors [ 25 ]  . 
at least 10% of diffuse neurofibromas are associated with neurofibromatosis type 1 . diffuse neurofibroma involves both the skin and the subcutaneous tissue , also frequently extending to the fascia over muscle , commonly with plaque - like or infiltrative growth patterns . 
despite being mildly or markedly hyperintense to muscle in t2 - weighted images and isointense or mildly hyperintense to muscle in t1 - weighted images , mr signal intensities of neurofibroma are typically nonspecific [ 25 ]  . vascular anomalies / infantile hemangioma vascular anomalies can be divided into two main categories : vascular tumors and malformations . 
infantile hemangiomas are the most common childhood tumors , with an incidence of 1223% among low - birth - weight , preterm infants and with a female - to - male ratio of 3 : 1 [ 26 ]  . 
c fat - suppressed contrast - enhanced t1 - weighted image shows reticular and ring - like enhancement ( arrow ) with perilesional fat stranding ( arrow heads ) 1 3 1056 la radiologia medica ( 2019 ) 124 : 10491061 fig . 
t2 - weighted image shows a heterogeneously hyperintense lesion with plaque - like growth ( arrow ) lipoma lipoma is the most common type of benign mesenchymal tumor , which is composed of mature fat cells . 
surgical approaches and planning differ between superficial and deep lipomas ; therefore , accurate assessment of localization is necessary for radiologists . on ct , lipomas appear as round or ovoid , well - delineated homogeneous masses associated with fat attenuation . 
the findings of a large tumor size , thick septa with moderate or marked enhancement , and nodular or patchy nonadipose components are indicative of well - differentiated liposarcomas [ 31 ]  . malignant tumors basal cell carcinoma ( bcc ) andsquamous cell carcinoma ( scc ) bcc and scc are the most common histologic subtypes of malignant cutaneous tumors of the scalp , accounting for 41% and 17% of all cases , respectively [ 32 ]  . 
b t1 - weighted image shows heterogeneous isoto hyperintensity ( arrow ) frequently occur in the head and neck region ( 60% of the cases ) , typically presenting two to 6weeks after birth as small lesions and rapidly growing in the first 1218months ( proliferating phase )  . 
subsequently , half of all the cases are completely resolved by 5years of age ( involuting phase )  . infantile hemangiomas typically appear as well - defined , lobulated , noninfiltrating masses , with hypointensity on t1 - weighted images and hyperintensity on t2 - weighted images ( fig.10 ) [ 27 , 28 ]  . 
as bccs and sccs both show nonspecific hypointensity on t1 - weighted images and isoto hyperintensity on t2 - weighted images ( fig.11 ) [ 33 ] , bccs and sccs are indistinguishable from one another with mri . 
sccs are more likely to be invasive than bccs ; however , peritumoral or deeper soft - tissue enhancement may be seen more often in cases of sccs than in those of bccs on contrast - enhanced t1 - weighted images . malignant melanoma malignant melanoma is a malignancy of pigment - producing cells ( melanocytes ) , which are located predominantly in the skhead and neck melanomas comprise 18% of all melanomas , and 7% of all melanomas arise on the scalp [ 34 ]  . 
 melanomas of the scalp frequently occur in the sixth decade , with a male predilection ( male - to - female ratio = 4 : 1 ) , which is significantly greater than for other sites [ 34 ]  . 
the tumor thickness of melanomas is greater in the scalp ( 2.6mm ) than in other sites ( 1.71.9mm ) , correlating positively with the risk of lymph node and distant metastasis . 
the location of melanoma on the scalp is , therefore , an independent adverse prognostic factor [ 34 ]  . stable - free radicals within melanin pigments are paramagnetic and induce shortening of t1 and t2 relaxation times ; therefore , the expected signal pattern for melanotic melanoma is hyperintensity on t1 - weighted images and hypointensity on t2 - weighted images ( fig.12 ) [ 33 ]  . 
the signal intensity varies depending on several factors , and intralesional hemorrhage also has a significant effect on mri . merkel cell carcinoma ( mcc ) mcc is a rare , aggressive , primary cutaneous neuroendocrine carcinoma . 
as sun exposure is considered a significant risk factor for mcc ( 81% ) , cases frequently occur in the head and neck region , accounting for 2948% of all primary mccs [ 35 ]  . 
b fat - suppressed contrast - enhanced t1 - weighted image shows homogeneously intense enhancement ( arrow ) of bccs and 38% of sccs are located on the scalp [ 3 ]  . 
 bccs and sccs of the scalp usually occur in patients in the sixth to seventh decades , with a female - to - male ratio of 1.1 : 1 and 1.3 : 1 for bccs and sccs , respectively [ 32 ]  . 
bccs and sccs of the scalp have a greater tendency to ulcerate , compared with other locations on the skas sccs of the scalp are often diagnosed at an advanced stage , this location may be considered an independent risk factor for poor prognosis [ 3 ]  . 
for sccs and bccs of the scalp , the maximum diameter greater than 10mm , the poorly defined borders , the recurrent tumor , and the history of immunosuppression and prior radiation therapy are clinical manifestations indicative of high - risk tumors . 1 3 1058 la radiologia medica ( 2019 ) 124 : 10491061 fig . 
 t2 - weighted image shows an ill - demarcated , heterogeneously isointense , cutaneous lesion ( arrow ) lymph node enlargement is often observed , alongside fine , compressed , retained fatty tissue [ 9 ]  . angiosarcoma angiosarcoma is a malignant tumor of vascular endothelial cells , often associated with local recurrence and metastasis , resulting in a poor prognosis . 
the characteristic findings for angiosarcoma include the presence of high - flow serpentine vessels , whereas low - flow vessels may show hyperintensity on t2 - weighted images [ 37 ]  . 
on contrast - enhanced images , solid components are intensely enhanced , whereas tumor necrosis is depicted as nonenhancing areas [ 37 ]  . metastasis cutaneous metastasis from primary visceral malignancy is clinically relatively uncommon , with a reported incidence fig . 
b t1 - weighted image shows heterogeneous hyperintensity ( arrow ) ranging from 0.22 to 10% , whereas 40% of the cases with cutaneous metastases also present with internal metastases [ 38 ]  . 
on ct and mri , cutaneous and subcutaneous metastases commonly manifest as multiple , variable - sized , poorly defined nodules , or as infiltrative softtissue masses with homogeneous or heterogeneous contrast enhancement . 1 3 la radiologia medica ( 2019 ) 124 : 10491061 1059 common subtype , which occurs on the scalp [ 3 ]  . 
if lymphomas present with subcutaneous bulky masses of the scalp with extensive cranial vault involvement , both bone lymphoma with scalp invasion and cutaneous lymphoma with bone invasion should be considered as differential diagnoses . 
 although ct and mri play important roles in tissue characterization and evaluating the depth of invasion of scalp lesions , it is challenging for radiologists to differentiate between scalp tumors because the imaging findings are typically similar and nonspecific . 
unenhanced ct image shows a homogeneous soft - tissue lesion ( arrow ) conclusions malignant lymphoma malignant lymphoma accounts for 0.64.8% of all malignant scalp tumors [ 2 , 32 ]  . 
the most common b - cell lymphomas of the scalp are primary cutaneous follicle center lymphoma and primary cutaneous marginal zone lymphoma , both of which have excellent prognoses [ 3 ]  . 
t1 - weighted image shows a hypointense subcutaneous nodule ( arrow ) 1 3 1060 la radiologia medica ( 2019 ) 124 : 10491061 utility of fine - needle aspiration in the diagnosis of primary scalp lesions . 
yang cc , chen ya , tsai yl , shih ih , chen w ( 2014 ) neoplastic skin lesions of the scalp in children : a retrospective study of 265 cases in taiwan . 
kato h , kanematsu m , watanabe h , nagano a , shu e , seishima m , miyazaki t ( 2016 ) mr imaging findings of pilomatricomas : a radiological - pathological correlation . 
anderson se , beer kt , banic a , steinbach ls , martin m , friedrich ee , stauffer e , vock p , greiner rh ( 2005 ) mri of merkel cell carcinoma : histologic correlation and review of the literature . 
kim hk , kim sm , lee sh , racadio jm , shin mj ( 2011 ) subcutaneous epidermal inclusion cysts : ultrasound ( us ) and mr imaging findings . 
prior a , anania p , pacetti m , secci f , ravegnani m , pavanello m , piatelli g , cama a , consales a ( 2018 ) dermoid and epidermoid cysts of scalp : case series of 234 consecutive patients . 
hong sh , chung hw , choi jy , koh yh , choi ja , kang hs ( 2006 ) mri findings of subcutaneous epidermal cysts : emphasis on the presence of rupture . 
sorenson ep , powel je , rozzelle cj , tubbs rs , loukas m ( 2013 ) scalp dermoids : a review of their anatomy , diagnosis , and treatment . 
t2 - weighted image shows a homogeneously isointense subcutaneous lesions ( arrows ) compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
 for this type of study , formal consent is not required . human and animal rights this article does not contain any studies with human participants performed by any of the authors . informed consent for this type of study , formal consent is not required . 
angulated , sharply defined borders occurred in 82.7% of itts in our series and accompanied both fusiform - shaped and bizarre - shaped itts ( fig.1 ) [ 2 ]  . 
this distinction is important since nodules in children , even when < 1cm , should undergo fine - needle aspiration ( fna ) when ultrasonography indicates malignancy [ 3 ]  . 
consequently , geometric / geographic instead of irregular better describes itts various shapes [ 2 ]  . itts reportedly exhibit a typical hypoechoic pattern with echogenic linear and punctate foci [ 15 ]  . 
in our study , itts internal echogenic dots either evenly or unevenly distributed showed a variable thin or thick configuration and were routinely compared with and found identical to those of the same patients thymic speckles ( fig.2 ) [ 2 ]  . 
however , itts tend to occur at the posterior aspect of the middle and lower thirds of the thyroid lobes , reflecting the embryological relationship between thymus and thyroid gland [ 2 , 4 , 5 ]  . 
thymic tongues should be differentiated from extrathyroid extension of an aggressive lesion . sparse or no vascularity in itts has been repeatedly reported [ 2 , 4 , 5 ]  . 
consequently , a strong aspect of this original article is the radiologic - pathologic correlation which provides solid proof for the diagnosis . conclusively , small - sized fusiform thyroid lesions could suggest the diagnosis of itt provided that attention is paid to additional details . 
further studies that will compare the occurrence of features like identical pattern of speckles with mediastinal thymus , low - lying and posterior location of lesion , well demarcated , angulated borders and sparse or no internal vascularity with / without extrathyroidal extension in both itts and non - itt thyroidal lesions , are necessary vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 10641065 1065 fig . 
the lesion is small , sharply demarcated , is located at the posterior aspect of the thyroid lobe , exhibits four angulations ( arrows ) and contains thin speckles which are identical to the speckles of the neighbouring cervical thymus ( * ) fig . 
we underline how important it is to determine whether a vascular anomaly has a regional vascular origin , or if there are other entities , ranging from benign to malignant lesions , which have flow - signal or blood degradation products . 
even though clinical examination and patients history are the first and indispensable steps in the initial diagnosis , the role of imaging is crucial , not only to determine whether a mass represents a true tumour / pseudo - tumour , but also to achieve a more correct diagnosis and determine the extension of the tumour / pseudo - tumour and its relation with the nearby anatomic structures . keywords soft tissue tumour pseudo - tumour vascular malformation vascular tumour children paediatric introduction the purpose of this article is to provide an up - to - date overview on imaging of paediatric vascular soft tissue masses , including neoplastic and non - neoplastic lesions , also considering non - vascular differential diagnosis . advanced clinical evaluation should be the first step in framing the diagnosis ( age , site , texture , colour , etc . ) , but soft tissue tumours and pseudo - tumours are more and * paolo tom paolo.toma@opbg.net 1 department ofimaging , bambino ges childrens hospital irccs , piazza santonofrio , 4 , 00165rome , italy 2 radiology department , santobono - pausilipon children 3 department ofradiology , g . 
gaslini institute , irccs , hospital , naples , italy genova , italy interventional radiology unit , department ofimaging , bambino ges childrens hospital irccs , rome , italy 5 department ofbiopathology andmedical biotechnologies ( di.bi.med ) , policlinico university ofpalermo , palermo , italy 6 department ofadvanced biomedical sciences , university federico ii , naples , italy more frequently referred to primary care sonography ( us ) as a contemporary first - line approach . 
 the first approach to vascular soft tissue masses in children is often challenging , due to their heterogeneous origin , which leads to a different treatment and prognosis [ 14 ]  . malignant lesions are very rare in paediatric age group : benign soft tissue tumours outstrip their malignant equivalents by about 100 to 1 , but most cutaneous and subcutaneous masses are very small and are often excised without imaging studies [ 5 ]  . 
however , 4% of solid malignancies in children are in the soft tissues , and this is why clinical and radiological approach is crucial for patient management [ 68 ]  . the diagnostic approach to paediatric soft tissue masses should follow an organic process , which consists in clinical evaluation , imaging examination , and eventual biopsy . age as systematically reported by brisse et al . 
for example , vascular tumours , infantile myofibromatosis , infantile fibrosarcoma , and subcutaneous metastases from neuroblastoma are more commonly reported in neonates and in early infancy , whilst others , such as rms , lipoblastomas or infantile aggressive fibromatosis , arise before the 5th year of age . 
indeed , lesions bigger than 5cm associated with pain and deeper involvement are more commonly associated with malignancy than to a benign lesion [ 711 ]  . imaging examination after clinical examination , the second crucial step is imaging evaluation of the tumour , not only to determine whether a mass represents a true tumour / pseudo - tumour , but also to achieve a more correct diagnosis and determine its extension and relation with the nearby anatomic structures [ 14 ]  . biopsy or fine - needle aspiration when both imaging and clinical examination have not achieved definitive proofs of 1 3 la radiologia medica ( 2019 ) 124 : 935945 table 1 sonographic pattern of soft tissue masses . 
in all the other cases , when the benign origin of the mass has been determined , patient management will only include simple observation , medical treatment or surgery [ 7 ]  . the aim of this review is to propose a rational diagnostic approach for soft tissue masses in children , which may mimic vascular anomalies . imaging evaluation the first choice examination is ultrasonography . ultrasound ( us ) with grey scale and colour doppler , with its wide availability , low costs , lack of ionizing radiation and no need for children sedation , are considered as the technique of choice for soft tissue lesion assessment , especially when dealing with small and superficial lesions [ 14 ]  . during examination , the practitioner should assess the following elements : anatomic location , depth of the lesion ( dermis , subcutaneous tissues , fascia , muscle , bone ) , its shape and margins , its echo texture and internal features , and , last but not least , its vascularity . moreover , when performing soft tissue ultrasound , a crucial and diriment tip is always to look at the symmetry of the lesions . 
 its appearance is hypoechoic with vascular density patternboth arterial and venous flow , in the proliferative stage , becoming smaller , more echogenic and less vascular , infantile haemangioma venous malformations lipoblastoma plexiform schwannoma / neurofibroma fibrous hamartoma of infancy clear cell sarcoma rhabdomyosarcoma spiradenoma cellulitis venous malformations plexiform schwannoma / neurofibroma infantile myofibromatosis infantile haemangioma congenital haemangiomas kaposiform haemangioendothetufted angioma arteriovenous malformation lioma ( avm ) infantile myofibromatosis pilomatrixoma lymph nodes ( metastases ) nasal glioma rhabdomyosarcoma phleboliths congenital haemangiomas kaposiform haemangioendothelioma pilomatrixoma myositis ossificans infantile myofibromatosis bone tumours sarcomas lympho - adenomegalies lymphatic malformations benign cysts popliteal , dermoid dacriocistocele necrotic areas of malignant tumours pilomatrixoma target pattern hyper - vascular pattern calcifications cystic lesions hyperechoic pattern infantile haemangioma lipoma / lipoblastoma fibrous hamartoma of infancy cellulitis subcutaneous fat necrosis bone fracture ( muscles ) echoic inhomogeneous pattern venous malformations cellulitis nodular fasciitis subcutaneous granuloma annular calme ( childhood asymmetrical labium majus enlargement ) axillary breast tissue in bold the proper vascular anomalies , in standard mimickers of vascular anomalies 1 3 938 fig . 
 hypoechoic lobular pattern of the intra - parotid mass ( white arrows ) , showing , on doppler us , high vessel density , high flow velocity , low resistance index , broadening of the spectrum ( a , b ) la radiologia medica ( 2019 ) 124 : 935945 fig . 
2 infantile haemangioma in the forearm of a 40 - day - old female : colour doppler examination shows afferent vessels due to fibro - fatty proliferation in involution stage ( fig.1 , 2 ) [ 1 , 4 , 14 , 15 ]  . 
differently from infantile haemangioma , vm presents with phleboliths , which , although not common , are very helpful in differential diagnosis ( dd ) , because they are rare in other paediatric soft tissue masses ( fig.3 ) [ 1 , 4 , 15 ]  . 
moreover , under the clinical point of view , they may expand with valsalva manoeuvre , after compression , and with gravity ( in the dependent limb ) [ 4 , 15 ]  . mr shows , in both cases , hypo / iso - density on t1 ( signal increases during involution phase due to fat deposition of theih ) compared with the surrounding muscles , hyper - density on t2 , and homogeneous enhancement after contrast media administrationwhich instead appears less prominent in case of involutions [ 1 , 4 ]  . vm differs from ih for the absence of flow in gradientecho ( ge ) imaging and shows spare signal void foci in all sequences , due to phleboliths and foci without enhancement in case of thrombi or a target sign ( described in the dedicated section ) [ 1 , 4 ]  . 
c t2w fat sat sequence shows multiple venous lakes with coagula inside ( target pattern ) mimickers of vascular anomalies : lipoblastoma may enter in dd due to its myxocollagenous stroma . 
however , the reported flow voids are normally less prominent in schwannomas and neurofibromas than in haemangioma due to the lower vascularity , as well as the entity of contrast enhancement ( and the entity of colour signal on colour doppler us ) , which is greater in haemangioma than in neurogenic tumours [ 2 , 17 , 18 ]  . target signs ( included in the dedicated section ) can be presented as well , both on us , due to the visualization of 1 3 la radiologia medica ( 2019 ) 124 : 935945 the entering and exiting nerve , and on mr , as a central zone of tightly packed fibbers , consisting of collagen or a highly cellular component , and a peripheral zone of non - fibrillary stromal or myxoid material , exhibiting various enhancements ( fig.4 ) [ 2 , 14 , 15 ]  . 
they differ from ce to ih since they show rapid infiltrative growth pattern , endothelium spindling , micro - thrombi , hemosiderin deposits ( depicted on mr ) , and often lymphatic aberrations [ 1 , 4 , 27 , 28 ]  . 
7 rapidly involuting congenital haemangioma ( rich ) of the neck in a newborn , colour doppler shows hyper - vascularization , but venous flow is arterialized ( a )  . 
blood supply and drainage anomalies can lead to asymmetric overgrowth or the involved body part , trophic changes may be present due to ischemia from arterial steal , haemorrhage , and highoutput heart failure , when capillaries are massive in size [ 1 , 4 , 2932 ]  . precautions should be taken when scanning these lesions , because they can be extremely fragile and a large amount of blood can be quickly lost . 
 suggest preparing emergency plans , including a haemostasis kit [ 4 ]  . on sonography , they appear as hypoechoic conglomerates of tortuous vessels , with or without a discrete soft tissue mass , associated with hyper - echogenic fibro - fatty proliferation in the surrounding tissues [ 1 , 4 ]  . on colour doppler interrogation , avm show high flows and high vascular density with a multidirectional flow [ 4 , 27 , 28 ]  . 
although it can show vascular patterns and calcifications , these features are never present at the same time , since the first tends to appear in the early stages due to inflammation , whilst the second only appears in the late phase . 
in dd , mr plays a pivotal role , since it demonstrates an intramuscular soft tissue mass deep into the fascia , with iso - hyper - signal intensity on t1 - weighted imagescompared to the surrounding musclesand a very high signal intensity on t2 - weighted images [ 2 , 38 ]  . also synovial sarcomas show , in 30% of cases , calcifications with a non - specific us appearance ( that can vary widely on the basis of the malignant potential of the tumour : from hypoechoic mass with lobulated margins to inhomogeneous hypo - echogenity with irregular margins , with potential vascularization in the areas of viable malignancy ) ( fig.11 ) [ 2 , 39 ]  . 
it appears as a firm , red to bluish skin - covered mass , which , nevertheless , does not exhibit any pulsations or increasing in size with the valsalva manoeuvres or compression of the ipsilateral jugular vein . us and doppler flow differentiate these entities , depicting the different cystic or solid nature of the masses and the characteristic low arterial flow velocity during the enddiastolic phase , unlike haemangioma , which shows a high arterial doppler flow velocity [ 12 , 35 , 36 ]  . 
nevertheless , mr is the imaging modality of choice , and can display nasal gliomas being often isointense compared to normal brain at mr imaging [ 12 ]  . calcifications proper vascular anomalies and some of the mimickers of vascular anomalies have been discussed in the previous paragraphs . 1 3 la radiologia medica ( 2019 ) 124 : 935945 fig . 
lymphatic vesicles can be detected on the skin or the mucosae , and they represent the most useful sign for clinical diagnosis [ 1 , 4 , 2932 , 40 , 41 ]  . imaging on us macro - cystic lymphatic malformations do not collapse after compression ( unlike venous malformations ) and appear as soft tissues composed of multiple cystic spaces ( anechoic or having varying degrees of echogenicity , or presenting with fluidfluid levels , especially when haemorrhage occurs ) and thin septa . 
the multiple cystic spaces show no inner flow on doppler investigation , however , it can be detected in the septa ( fig.12 ) [ 1 , 4 , 14 ]  . in case of micro cystic lymphatic malformations , us appearance is different as they show an increased echogenicity , which is attributed to the multiple interfaces caused by tiny cysts that are beyond the resolution of the us equipment [ 1 , 4 , 14 , 40 , 41 ]  . on mri they appear as multi septate cystic masses that can infiltrate surrounding tissues , which are typically hypointense on t1 - weighted images and hyperintense on t2 - weighted images , and do not show enhancementwhich is an important feature in differential diagnosis from venous malformations . 
nevertheless , inner septa may show various degrees of post - contrast media administration enhancement , since they are vascularized [ 1 , 4 , 14 , 40 , 41 ]  . cysts with protein content or prior haemorrhage can show a heterogeneous intensity [ 1 , 4 , 14 ]  . mimickers of vascular anomalies : dacriocystocele may enter in dd with vascular anomalies and nasal gliomas since , under the clinical point of view , it appears as a grey - blue cystic swelling below the medial canthus . 
laffan ee , ngan by , navarro om ( 2009 ) pediatric soft - tissue tumors and pseudotumors : mr imaging features with pathologic correlation : part 2 tumors of fibroblastic / myofibroblastic , socalled fibrohistiocytic , muscular , lymphomatous , neurogenic , hair matrix , and uncertain origradiographics 29 ( 4 ) : e36 3 . 
morn fe , morriss mc , jones jj , hunter jv ( 2004 ) lumps and bumps on the head in children : use of ct and mr imaging in solving the clinical diagnostic dilemma . 
arioni c , bellini c , oddone m , risso fm , scopesi f , nozza p , serra g , tom p ( 2006 ) congenital fibrous hamartoma of the knee . 
de beuckeleer lh , de schepper am , vandevenne je , bloem jl , davies am , oudkerk m , hauben e , van marck e , somville j , vanel d , steinbach ls ( 2000 ) mr imaging of clear cell sarcoma ( malignant melanoma of the soft parts ) : a multicenter correlative mri - pathology study of 21 cases and literature review . 
jin w , kim gy , lew bl , yang dm , kim hc , ryu jk , park js , ryu kn ( 2008 ) sonographic findings of an eccrine spiradenoma : case report and literature review . 
wortsman x , wortsman j , arellano j , oroz j , giugliano c , benavides mi , bordon c ( 2010 ) pilomatrixomas presenting as vascular tumors on color doppler ultrasound . 
abate m , salini v , rimondi e , errani c , alberghini m , mercuri m , pelotti p ( 2011 ) post traumatic myositis ossificans : sonographic findings . 
pang lm , roebuck dj , griffith jf , kumta sm , metreweli c ( 2001 ) alveolar soft part sarcoma : a rare soft - tissue malignancy with distinctive clinical and radiological features . 
murphey md , gibson ms , jennings bt , crespo - rodrguez am , fanburg - smith j , gajewski da ( 2006 ) imaging of synovial sarcoma with radiologic - pathologic correlation . 
khuu a , yablon cm , jacobson ja , inyang a , lucas dr , biermann js ( 2014 ) nodular fasciitis : characteristic imaging features on sonography and magnetic resonance imaging . 
pham h , fessell dp , femino je , sharp s , jacobson ja , hayes cw ( 2003 ) sonography and mr imaging of selected benign masses in the ankle and foot . 
gokli a , neuman j , lukse r , koshy j , kong f , laor t ( 2016 ) childhood asymmetrical labium majus enlargement sonographic and mr imaging appearances . 
a pivotal prospective randomized controlled trial has shown that hydrogel spacer has a great role in reducing the rectal wall doses and improving rectal toxicities during definitive prostate radiotherapy [ 1 ]  . 
 [ 3 ] have reported gastrointestinal ( gi ) and genitourinary ( gu ) toxicities in salvage and / or adjuvant post - prostatectomy radiotherapy with hydrogel spacer implant , and i would like to thank the authors for sharing wonderful work . 
their study did not have control group to compare observed results , and even they did not perform a comparative planning study between the preand post - implantation of hydrogel to elucidate the effect of a hydrogel spacer implant on rectal wall doses . 
 initially , it is important to know the impact of a hydrogel * hamed ghaffari hamedghaffari@yahoo.com 1 department ofmedical physics , school ofmedicine , iran university ofmedical sciences , tehran , iran spacer on rectal dosimetry during post - prostatectomy radiotherapy because hydrogel injection has an expensive and invasive procedure . 
 [ 2 ] have previously expressed the prerequisites for hydrogel spacer application in the post - prostatectomy setting , including single and macroscopically visible tumor recurrence located in the proximity of the rectal wall and a very high level of safety that the lesion is the only site of recurrence . 
it should be noted that the entire prostatic fossa ( from the pubic bone to the rectal wall in the anteriorposterior axis , as well as potential microscopic tumor spread ) is defined as the ctv in the standard treatment [ 4 ]  . 
a strategy that can be applied to reduce the potential risk of the remaining tumor cells at the anterior rectal wall is to include the prostatic fossa and hydrogel spacer within the ctv ; however , the improvement in rectal dosimetry will be reduced . 
 [ 3 ] have confidently expressed that the application of a hydrogel spacer does not compromise biochemical control rates and maintains and / or reduces grades of gu and gi toxicities in comparison with previously published reports without the use of a hydrogel spacer injection . 
as stated above , reliability of these results is difficult . in summary , i think that a two - arm study with large sample size and well - defined inclusion and exclusion criteria is required to elucidate the role of a hydrogel spacer in reducing rectal wall doses and rectal toxicities during post - prostatectomy radiotherapy . 
as stated above , reducing gi and gu toxicities in salvage and / or adjuvant post - prostatectomy radiotherapy with hydrogel spacer implant in a single - arm study is not reliable . 
meanwhile , based on my experience on the application of a rectal retractor in definitive prostate radiotherapy [ 5 , 6 ] , the rectal retractor can be used in the postprostatectomy radiotherapy setting with promising results as an alternative method to a hydrogel spacer . 
where are we now ? marwingutierrez1 , 2 antoniogarca4 chiarabertolazzi1 marikatardella3 luisrodriguez1 jaimemendoza1 deniseclavijocornejo1 received : 4 april 2019 / accepted : 18 june 2019 / published online : 2 july 2019 italian society of medical radiology 2019 abstract lung ultrasound ( lus ) achieved an intriguing role in the management of pulmonary involvement in patients affected by connective tissues diseases ( ctds )  . 
few studies have been performed to support its usefulness in the evaluation of the presence and the severity of interstitial lung disease ( ild ) , relating it to the information obtained with chest high - resolution computed tomography ( hrct )  . 
nevertheless , ild is the second cause of death in systemic sclerosis ( ssc ) and rheumatoid arthritis ( ra ) [ 3 ]  . in daily clinical practice , conventional chest radiography is the first imaging tool used to evaluate the presence of ild , but it is of limited use due to its low sensitivity , particularly in early stage of disease . 
chest high - resolution computed tomography ( hrct ) is considered the gold standard in the diagnosis of ild and in the ability to identify lung pattern of different interstitial pneumonia [ 4 ]  . in the last 20years , many authors demonstrated the utility of ultrasound ( us ) assessment in the evaluation of lung and pleural diseases , offering new tools for the management of acute and chronic pulmonary conditions [ 512 ]  . 
the elementary findings detectable are vol . : ( 0123456789 ) 1 3 990 la radiologia medica ( 2019 ) 124 : 989999 artifacts generated from the thickened interlobular septa at lung surface level . 
in the evaluation of methodological quality of the included studies , we applied the newcastle - ottawa scale ( nos ) , which is a tool developed to assess quality of nonrandomized observational studies [ 20 ]  . methods we reviewed all relevant scientific articles regarding ild in ctds published in the last 18years , according to the preferred reporting items for systematic review and meta - analysis ( prisma ) guidelines [ 19 ]  . 
we performed a systemic research on the electronic databases ( pubmed and embase ) using the following search terms in all possible combinations : ultrasound , ultrasonography , sonography , interstitial lung disease , pulmonary fibrosis , interstitial pulmonary fibrosis , interstitial fibrosis , systemic sclerosis , rheumatoid arthritis , sjgrens syndrome and systemic lupus erythematosus . 
two independent rheumatologists ( mg , mt ) screened all the titles , abstracts and full reports of articles identified , and in case of disagreement , a third investigator ( cb ) was consulted , obtaining a consensus . 
in table1 are summarized demographic data , number of patients enrolled and type of diseases included . the largest number of articles concerns the ssc , since the incidence of ild in this disease is higher than in other ctds . 
the first study was conducted by an italian group in 2009 [ 13 ] ; they subjected 33 consecutive ssc patients to a lus assessment , using a 2.53.5mhz cardiac transducer , in the anterior , middle and posterior chest . 
sixty - two pulmonary intercostal spaces ( lis ) were included with an average lus examination time of 10mlus data were correlated with hrct data , using the score proposed by warrick etal . 
they obtained a linear correlation between the lus and hrct data and a significant correlation between the number of b lines and the diffusion capacity values of carbon monoxide ( dlco )  . the same group of authors [ 22 ] conducted a study on 25 patients to compare the evaluation of lus performed with two different probes : a 2.53.53.5mhz heart probe and a 612mhz linear probe used at 6mhz , and with hrct chest data , using the warrick score . 
lus evaluations were performed on 50 lis in anterior , middle and posterior chest , with a 27mhz convex broadband multifrequency transducer , using an average time of 23min for each patient . 
they found a positive correlation between the lus data and the dlco values and , in addition , a significant linear correlation between the semiquantitative lus score and the warrick score . 
among the ssc patients , eight were classified as limited ssc , five as diffuse ssc and three as ssc without scleroderma dssc ( 24 ) / lssc ( 15 ) lssc ( 33 ) , dssc ( 15 ) , sjgrens syndrome lssc ( 42 ) , dssc ( 21 ) , sine scleroderma ( 4 ) sd standard deviation ; n / a not applicable ; ssc systemic sclerosis ; ctd connective tissue disease ; ra rheumatoid arthritis ; ss sjgren syndrome ; dssc diffuse systemic sclerosis ; lssc limited systemic sclerosis ; sle systemic lupus erythematosus ; ild interstitial lung disease were observed in the lis at the level of the lower posterior regions of the chest , which were proposed by the authors as the first lis to be evaluated in the initial phase of the ild . the same group of researchers [ 17 ] proposed a simplified evaluation of the lus , performing a post hoc analysis . 
they included 36 ctd patients ( 28 ssc , 2 sjgrens syndrome , one undifferentiated ctd , two antisynthetase syndrome , two dermatomyositis , one mixed ctd ) , performing the evaluation of lus with a 27mhz broadband multifrequency convex transducer . 
they found a significant correlation between the complete and simplified lus score ( p = 0.0001 ) and a positive correlation between the simplified lus score and the hrct score ( p = 0.0006 ) , both in the quantification and extension of the ild . 
they correlated the lus data with chest hrct and proposed the definition of pleural irregularities when the thickening of the pleural line was greater than 2.8mm and a pleural score : 0 = without areas of irregularity , 1 = 15 areas of pleural irregularity and 2 = > 5 areas of pleural irregularity . 
 they performed lus evaluation in 62 lis of cw , using a 2.53.5mhz cardiac transducer with a length of 2.5cm , and correlated ultrasound data with hrct and pulmonary function tests . 
they found 100% sensitivity and 59% specificity when the total number of b lines was > 5 , and an agreement of 83% between hrct and lus for ild detection . 
the evaluation of lus included the evaluation of ten lis : for the anterior chest : the fourth lis along the midclavicular line ; for the lateral chest : the fourth lis along the anterior and middle - axillary axillary lines ; and for the posterior chest : the eighth lis along the subscapular and posterior axillary lines . 
the purpose of the study was to evaluate the ability of the lus to detect pleural line thickness ( usually < 3.0mm ) for the study of subclinical ild in patients with ssc to plan hrct evaluation . 
pleural line thickening ( 3.05.0mm ) was found in 97 patients , subpleural nodules in 32 patients and major pleural line thickening ( > 5.0mm ) in 35 patients , while normal pleural line thickening was found in 26 patients without ild . 
all lus data showed good agreement with the hrct score , classified as extended pulmonary fibrosis ( pf ) ( definitely involving the mediumhigh lung ) , limited or baseline pf ( only involving the posterior lower - base lung ) or absent pf ( no apparent sign )  . in accordance with the previous study , buda etal . 
 [ 26 ] proposed a new method to describe the results of the lus for the ild criteria : pleural line irregularity , pleural line narrowing , the fragmentary nature of the pleural line , pleural line blurring , pleural line thickening , b - line artifacts 3 and subpleural consolidations < 5mthey performed a study at a single center to correlate lus results with hrct results , using warricks score , in a cohort of 52 ild patients compared to 50 healthy subjects . 
the most frequent result was a thickening of the pleural line ( thickness 2mm ) , mainly in the lower lung fields in patients with ssc , while in severe cases of ild a blurred pleural line was detected , which is detected in patients with honeycombing in the hrtc scan . 
 [ 27 ] conducted a transversal study with the aim of correlating the results of lus , hrct thoracic and pfts in 39 patients with ssc , including the modified rodnan skin score ( mrss ) as a clinical variable . 
 [ 29 ] in 2018 designed a cross - sectional study to determine a cutoff point of the number of b lines to detect the presence of significant ild in 40 consecutive ssc patients in relation to the warrick hrct score . 
the authors adopted the previous lus score of 14 lis [ 17 ] for the evaluation of each patient and showed that a value of 10 b lines is highly predictive for the significant presence of ssc - ild in hcrt , using as external criterion a warrick score of 7 . 
 they also found a strong correlation between the total lus 1 3 la radiologia medica ( 2019 ) 124 : 989999 score and the dlco and a moderate correlation between the total lus score and quality of life measures . also in 2018 , hassan etal . 
in 29 patients with abnormal hrct ( warrick score > 7 ) and lus , two had a low score ( 615 b lines ) and 27 had moderate or severe scores ( 16 b lines )  . 
a total of 29 patients were studied with a ps - usd , whose sensitivity and specificity with respect to chest hrct were 89% and 50% , respectively . an interesting element was introduced by hasan etal . 
 [ 33 ] who studied the accuracy of lus in ild diagnosis by comparing it with hrct chest data ( including ground glass , reticular , nodular or honey combing ) and with pft . 
they divided the chest into four areas and considered a positive region when they found three or more b lines in a longitudinal plane between two ribs and defined an examination as positive when there were two or more positive regions bilaterally . 
 [ 34 ] proposed a transverse study to estimate the value of lus as a diagnostic screening tool in patients with ra who did not show clinical signs or symptoms of ild . 
on the other hand , lus showed sporadic abnormalities in 7% of healthy controls . recently , the same authors [ 14 ] conducted a new study with the aim of determining the diagnostic value of lus in the diagnosis of ild in patients with ctds [ ra , ssc and systemic lupus erythematosus ( sle ) ] and , as a second aim , to determine the possible correlation between the frequency of pathological results of lus and the underlying disease . 
lus was correlated with chest hrct showing a sensitivity of 1 ( 95% ci 0.3981.0 ) , a specificity of 0.89 ( 95% ci 0.5180.997 ) and a positive probability of 9.00 ( 95% ci 7.111.3 ) to detect ild . 
 lus achieved an excellent correlation with hrct data in sjgrens syndrome with ild . table2 shows the feasibility , reliability , sensitivity and specificity of lus , while the technical characteristics of lus and the type of score used in all studies involved in the review are represented in table3 . discussion identification and quantification of early manifestations of ild in ctds are an important objective to improve the quality of life of patients affected by ctds and for prognosis [ 1 , 3741 ]  . 
in this regard , lus has recently demonstrated a high sensitivity in the detection of signs indicative of ild , even in the early stages of the disease and , especially , a high negative predictive value . 
hrct remains the gold standard in ild identification ; however , lus , due to the absence of ionizing radiation and its simplicity of execution , even in the patients bed , can be considered as an excellent screening tool . 
lus has demonstrated encouraging validity , reliability and feasibility , and currently , it could be considered as an excellent methodology to establish the correct timing of hrct in ild assessment . how to behave in the preclinical stages of disease , however , remains a topic of debate [ 30 ]  . 
interesting the cutoff point of ten b lines to detect the presence of sscild proposed as a reference on the basis of which to send patients to perform a hrct [ 29 ]  . despite the progress of studies in the literature , there is still much to be done , and some crucial points need to be discussed . 
currently , the number of lis used in the studies is very variable , from 10 to 72 on the other hand , new possibilities of interpretation of pathological findings are emerging , in particular with regard to pleural abnormalities . 
pleural abnormalities appear to be adequately related to specific hrct findings such as ground - glass opacity and extensive fibrosis and could therefore be considered an ild imaging biomarker [ 15 ]  . 
 moreover , in the future , there will be an increasing interest in pocket - sized ultrasound machines , which can be used to evaluate lung diseases without the need for top of the range machines to acquire reliable information . in conclusion , this review showed how lus can become an important technique for assessing lung disease in rheumatic diseases with suspected lung involvement . 
applications of this imaging method are still growing , and further opportunities are likely to arise in the light of the vibrant field of research . funding the authors have not declared a specific grant for this research from any funding agency in the public , commercial or not - for - profit sectors . compliance with ethical standards conflict of interest the authors would like to make the following statements with regard to their conflicts of interest / financial disclosures : mg has attended advisory board meetings and scientific consultancies and has obtained speaking fees for : abbvie , novartis , ucb , esaote spa , janssen , bristol - myers squibb , merck sharp & dohme , pfizer , sanofi aventis . 
in this scenario , the radiologist plays a key role in both diagnostic and therapeutic workups of pavms : chest x - ray , computed tomography and magnetic resonance are effective tools for pavms identification and confirmation of the suspected diagnosis . 
furthermore , imaging modalities provide most of the elements for pavms classification according to their angioarchitecture ( simple and complex ) and help the clinicians in establishing which lesion requires prompt treatment and which one will benefit of imaging follow - up alone . 
endovascular management of pavms has grown up as the first - line treatment in respect of surgery during last decades , showing lower risk of intraand post - procedural complications and offering a wide number of treatment options and materials , ensuring effective management in virtually any clinical situation ; interventional treatment aims to exclude pavms from pulmonary circulation , and specific technique and embolic agents should be selected according to pre - treatment imaging , in order to obtain the best procedural outcome . 
this paper proposes a review of the clinical and radiological features that a radiologist needs to know for pavms diagnosis and proper management , also showing an overview of the most common endovascular treatment strategies and embolization materials . keywords pulmonary arteriovenous malformation pulmonary arteriovenous fistula hereditary hemorrhagic telangiectasia oslerweberrendu disease ct imaging endovascular treatment introduction pulmonary arteriovenous malformations ( pavms ) or fistulas are a rare condition , firstly described by churton etal . 
 in this scenario , the radiologist plays a key role in both the diagnostic and therapeutic workup of pavms : chest x - ray ( cxr ) , computed tomography ( ct ) and magnetic resonance ( mr ) are essential tools for diagnosis , treatment planning and follow - up of pavms , providing the majority of the elements required for a proper management ; on the other hand , endovascular management of pavms is vol . : ( 0123456789 ) 1 3 974 la radiologia medica ( 2019 ) 124 : 973988 carving out a role as first - line treatment option for these lesions , showing high safety and effectiveness . the article focuses on the clinical and radiological features of pulmonary arteriovenous malformations according to what the radiologist needs to know for a correct patient management ; etiology and classification are also described , and an overview of the current endovascular treatment techniques and materials available is proposed . etiology congenital pavms most of pavms are congenital ( 80% ) , and a tight association with hereditary hemorrhagic telangiectasia ( hht ) is described in the literature ( 4790% ) [ 38 ]  . 
hht is an autosomal dominant disorder associated with the mutation of one of the following proteins : endoglin ( eng gene , hht1 subtype ) or activin a receptor type ii - like 1 ( akl1 gene , hht2 subtype ) [ 9 , 10 ] ; among hht subtypes , hht1 has the strongest association with pavms [ 11 ] , probably because endoglin is part of the cellular membrane receptor for tgfthat is a key factor in the regulation of the angiogenetic process [ 12 ]  . 
in a small percentage of cases ( ~ 2% ) , a mutation in smad4 [ 13 ] is observed , coexisting in these patients the juvenile polyposis [ 14 ]  . on the other hand , only 1050% of patients with hht will develop pavms during their lives [ 4 , 15 ] , and there is lack of evidence about possible genetic locus , other than eng , akl1 and smad4 , associated with pavms development [ 16 , 17 ] , suggesting that congenital pavms conceal genetic basis that are still widely unclear . pavms inpregnancy pregnancy is associated with the growth of preexisting pavms [ 21 ] , especially in hht patients : probably , the underlying cause is the increased blood flow / volume and cardiac outputtypical hemodynamic effects observed in pregnancyassociated with the complex changes promoted by progesterone on the pulmonary venous bed . 
the consequence is an increased risk of major clinical events associated with pavms rupture / embolization , such as hemoptysis , hemothorax and cerebrovascular disorders [ 21 , 22 ]  . classification the classification of pavms currently used was proposed by white [ 23 ] : pavms are classified as simple and complex , on the basis of their angioarchitecture . 
two particular subtypes of complex pavms are diffuse and telangiectatic ones : diffuse subtype is characterized by the involvement of a large part of parenchyma , sometimes even an entire lung , by a tangle of malformed vessels ; telangiectatic pavms involve only part of pulmonary lobe , and their vascular network is usually microscopic , beyond the spatial resolution power of ct [ 24 ]  . pavms are also classified on the basis of the feeding arteries size : if a feeding artery has a diameter of 3mm or greater , pavm is classified as macroscopic , otherwise as microscopic ( fig.1 ) [ 25 ]  . acquired pavms clinical features pavms are acquired in 20% of cases and associated with pathological conditions such as hepatic cirrhosis , infectious diseases , traumas , mitral valve stenotic disease , fanconis syndrome and metastatic cancer [ 2 ]  . 
among these , chest traumas , cardiothoracic surgery , hepatic cirrhosis , metastatic cancer , mitral stenosis , infections and amyloidosis are described most frequently [ 3 ] ; sporadic cases of pavms in constrictive pericarditis [ 18 ] , lung parenchymal cyst [ 19 ] and chronic thromboembolic disease [ 20 ] have also been reported . in our opinion , this great variability of conditions associated with acquired pavms subtends a common underlying developmental mechanism , probably triggered by a chronic angiogenetic impulse to the lung vasculature . clinical presentation of pavms is extremely heterogeneous : some patients are completely asymptomatic , and some others present from vague to even life - threatening respiratory symptoms such as dyspnea and hypoxemia at rest or during exertion . 
platypnea ( orthostatic dyspnea ) and orthodeoxia ( orthostatic hypoxemia ) are typical features and usually affect patients with pavms located in the lower lobes , probably as the consequence of a blood flow redistribution to the site of pavms in the upright position [ 26 ] ; less frequently , pavms manifest as a clinical emergency with hemoptysis [ 27 ] and / or hemothorax ( table1 ) [ 7 ]  . hht patients have a major risk of complications , severe symptomatology , multi - organ disease and rapid progression of pavms [ 3 ]  . 
simple pavms are characterized by the presence of a single segmental feeding artery ; their angioarchitecture may consist of a direct communication between the segmental artery and a usually aneurysmatic draining vein ( a ) or of multiple sub - segmental arteries merging in a tangle of malformed vessels draining in one ( b ) or multiple ( c ) veins . 
complex pavms receive blood supply from two or more segmental arteries ( d ) ; diffuse subtype shows a wide parenchymal involvement with a mess of malformed vessels of similar size ( e ) that in the telangiectatic subtype are too small to be discerned with imaging ( f ) or assessed with certainty , hht should be promptly confirmed by the presence of curacao criteria ( table2 ) [ 28 ] : the presence of three or four criteria confirms the diagnosis of hht , and the presence of two criteria makes the diagnosis possible or suspected , whereas one or less criteria make the diagnosis unlikely . imaging diagnostic workup the radiologist is like a metronome in the pavms decision - making process ; cxr , ct and mr provide essential elements for both treatment and careful observation of 1 3 976 la radiologia medica ( 2019 ) 124 : 973988 table 1 clinical features of pavms symptoms signs complications absence of sympanemia brain abscess toms chest pain cough dizziness dyspnea dyspnea on exertion clubbing cyanosis hypoxemia polycythemia pulmonary hypertencerebrovascular stroke endocarditis epistaxis hemoptysis hemothorax sion pulmonary rumors telangiectasia heart failure splanchnic abscess splanchnic embolization attack transient ischemic fatigue migraine orthodeoxia palpitation platypnea seizures syncope pavms pulmonary arteriovenous malformation table 2 curacao criteria recurrent and spontaneous epistaxis ( > 1 episode ) first - degree relative with hht specific anatomical locations of telangiectasia ( face , fingers , mouth , oral and nasal mucosa ) arteriovenous malformations at visceral sites ( lung , liver and brain ) hht hereditary hemorrhagic telangiectasia diagnosed pavms . chest xray respiratory symptoms are usually the first clinical event among patients with pavms [ 29 , 30 ]  . 
in this scenario , cxr is the ideal first imaging tool , due to the mini - invasiveness and diffuse availability , providing good sensitivity ( 70% ) and excellent specificity ( 98% ) for diagnosis of pavms , when nodular opacities are evident [ 31 ]  . 
these characteristics allowed cxr to be proposed in screening programs for pavms in patients with hht , in association with transthoracic contrast echocardiography ( ttce ) [ 31 , 32 ]  . according to the european guidelines on quality criteria for diagnostic radiographic images [ 33 ] , the best diagnostic results are obtained when cxr is performed in the upright position and both postero - anterior ( pa ) and lateral projections are performed . 
a correct acquisition of cxr is essential , in order to avoid misdiagnosis of small pavms or fistulas located behind normal structures such as heart or diaphragm [ 34 ]  . 
cxr appearance of pavms is chameleonic : some patients show no evidence of parenchymal involvement , due to microvascular telangiectasia ; some others may have a heavy impairment of pulmonary parenchyma with multiple and diffuse pavms in both lungs [ 2 , 34 ] , but usually are less than 5cm in the largest diameter [ 2 , 10 , 24 ]  . 
frontal chest x - ray radiogram shows two well - defined homogeneous mass - like opacities with lobulated shapes ( circle ) in the sub - pleural parenchyma of the left lung ( a ) confirmed in the lateral radiogram ( b ) that better shows also serpiginous opacities directed from the lesions to the hilum , referable to feeding vessels ( arrowheads ) 1 3 la radiologia medica ( 2019 ) 124 : 973988 from the pulmonary hilum and reach the fistula , whereas draining veins arise from pavm to reach the left atrium [ 2 , 24 ]  . 
when visible , feeding vessels appear as tubular opacities that connect the suspected fistula to the mediastinum and veins are usually larger than arteries ; the diameter of vessels is usually > 4mm but < 7mm , even if vessels with diameter > 20mm have been previously reported [ 36 ]  . 
 in some cases , parenchymal hemorrhage , resulting from the rupture of the lesion , or atelectasis , as a consequence of ab estrinseco bronchial compression , is observed [ 2 ]  . computed tomography ct is the gold standard among noninvasive diagnostic tools for pavms [ 24 , 36 ]  . 
there is lack of evidence about ct acquisition protocols for dose reduction , and a wide inter - study and intra - study variability is observed in the literature , probably as the consequence of different patients populations ( screening , follow - up , etc . ) and ct scanners ( singleto multi - slice )  . 
some authors suggest a low - dose unenhanced ct acquisition of the thorax [ 41 , 42 ] , in order to identify pavms and exclude other pathologies such as calcified granulomas [ 35 ]  . 
maximum intensity projection images confirm the presence of a macroscopic pavm characterized by the presence of a nidus ( circle ) receiving an arterial feeder ( arrow ) from the apical segmental pulmonary artery and draining in a large venous collector ( arrowhead ) ( b )  . 
complex pavms are also recognized on ct scans with simplicity and are distinguished from simple type for the presence of more than one feeding artery , originating from multiple segmental arterial branches ( fig.3 ) [ 24 ]  . 
the recognition of diffuse and telangiectatic subtypes may be more laborious : in the diffuse subtype , a tangle of pathological feeding arteries and veins in association with a homogeneous involvement of a whole segment , lobe or fig . 
c the presence of multiple simple pavms ( arrows ) in the lower lobes strengthened the suspected diagnosis 1 3 la radiologia medica ( 2019 ) 124 : 973988 lung is evident . 
telangiectatic pavms appear as a groundglass area , with possible solid nodular component inside , and both feeding artery and vein are frequently absent ; this type of lesions is usually diagnosed in children , and their diagnosis may be challenging , but multiple pavms with typical appearance usually coexist in both lungs , suggesting the nature of the lesions ( fig.4 ) [ 24 ]  . whatever the nature of pavm , the identification of at least a feeding artery and vein is mandatory for establishing the diagnosis on ct images [ 35 ]  . 
the identification of arterial feeders is also necessary to assess the vessel diameter ; this measurement should be performed as near as possible to the nidus of the pavm , however , beyond non - afferent parenchymal vessels , because an arterial diameter of 3mm or larger is the current cutoff to indicate endovascular treatment [ 25 ] , in the face of an increased risk of complications [ 23 ]  . 
their study reported that the dynamic contrast - enhanced mra with the improved temporal and spatial resolution can be used in children and infants for the assessment of congenital vascular disease . in the study of schneider etal . , the contrast - enhanced mra was reported to be an effective screening tool for the detection of pavms in patients with hereditary hemorrhagic telangiectasia . 
contrast - enhanced mra is also a superior technique to global or selective pulmonary angiography , permitting the detection of significantly more pavms both over all ( p = 0.0003 ) and when compared solely with the initial global or selective pulmonary angiography ( p < 0.0001 ) [ 46 ]  . time - resolved mr angiography was recently reported to be a more useful option than ct for assessing the reperfusion of pavms after coil embolization because of its high sensitivity in detecting blood flow and the absence of ionizing radiation , and it offers a noninvasive examination with high resolution [ 47 , 48 ]  . unfortunately , most of the series enrolled few patients and the level of evidence remains basically low . in general , 3d contrast - enhanced mr angiography has shown good identification rate for pavms > 5cm , with an acceptable demonstration of number and size of feeding vessels ; however , the diagnostic accuracy seems to be significantly lower for lesions < 5cm , limiting the use of this technique in setting indication to treatment [ 49 ]  . interventional management endovascular treatment of pavms has carved out a significant role over the years , proving to be superior to surgery in terms of complications rate and hospitalization length [ 50 ]  . 
5 pavms treatment complications : ct axial image of a 54 - year - old man presenting with left thoracic pain , 7 days after endovascular occlusion of an inferior left lobe pavm with coiling ( arrow )  . 
a well - demarcated triangular sub - pleural consolidation area is evident , distally to the treated lesion ( circle ) ; the ct appearance and the clinical onset suggest the nature of the lesion as a post - procedural pulmonary infarction 1 3 980 la radiologia medica ( 2019 ) 124 : 973988 this goal is achieved by closing the feeder vessels of the pavm as near as possible to the nidus , in order to preserve normal vessels , lung parenchyma and preventing collateral reperfusion . 
coil selection is a delicate step : the diameter should not be smaller than that of the feeder vessel , because the risk of paradoxical embolization may increase [ 52 ] ; on the other hand , coils with a too large diameter may unfit the vessel , causing local complications , such as vessel rupture or migration in nontarget adjacent vessels ; a 2030% coil oversizing , with respect to vessel diameter , has been described as a good compromise to prevent complications [ 52 ]  . 
also , coil length may affect deployment : a short length can lead to the use of many coils , with a rising in procedural costs and increasing the risk of paradoxical embolization or retrograde migration ; moreover , an excessive length makes difficult the coil folding process in the target vessel . 
a 30 - year - old woman presenting with dyspnea : chest radiogram ( a ) shows the presence of a round bilobated opacity in the right middle lobe ( arrow ) , with two tubular opacities converging to the pulmonary hilum ( arrowheads ) , suspected for pavm . 
contrast - enhanced ct ( b ) confirms the presence and the nature of the lesion , revealing a well - defined nidus ( arrow ) , a feeding artery ( white dot ) and an efferent vein ( white star ) ; a little collateral feeding artery originating from the same segmental artery is also evident , defining the lesion as simple pavm . 
the occlusion of the main ( c ) and collateral ( d ) arterial feeders to the pavm by means of metallic coils , allowed pavm complete vascular exclusion ( e ) 1 3 982 la radiologia medica ( 2019 ) 124 : 973988 fig . 
7 anchor technique : ( a ) selective angiography of an artery suppling an inferior right lobe malformation ( star ) showing the presence of multiple collateral vessels near the lesion ( arrow )  . 
a catheter is placed into one of the collaterals by mean of coaxial technique ( b ) and a long metallic coil is deployed starting from the collateral vessel ( c ) into the lumen of feeding artery of the vascular malformation ( d )  . 
b the small size of the feeders and their collaterals suggested the operator to choice a scaffold technique placing an oversized , rigid coil in each feeding vessel ( arrowheads ) , in order to create a supportive system for the deployment c of multiple filling coils . 
d final control showing the complete vascular exclusion of the fistulas 1 3 la radiologia medica ( 2019 ) 124 : 973988 whatever the embolization technique , advantages of using coils consist of a relative ease of use , the possibility of deployment control and excellent adaptability to the vascular lumen . 
on the other hand , the major limit lies in the necessity to reach the target vessel and the need for sufficient lumen space for the deployment . there is no evidence in the literature about changes in procedural outcome for different coils type [ 56 ] , and vascular recanalization is observed in up to 19% of cases [ 26 ]  . onyx vascular plugs amplatzer vascular plugs are dense nitinol mesh devices that reduce blood flow in the target vessel and promote thrombosis once deployed . 
each device has a relatively rigid delivery system which carries the plug , through the catheter , till the site of embolization ; the plug is anchored to the delivery system by a screw mechanism which , once the target vessel is reached , is manually turned counterclockwise , with subsequent plug deployment [ 57 ]  . 
a new generation of plugs composed by microvascular plugs ( medtronic , dublin , ireland ) and endoluminal occlusion system ( artventive , carlsbad , california ) has been recently described for pavms treatment [ 5860 ] ; they differ from classical vascular plug for the presence of a polytetrafluoroethylene membrane that induces vessels occlusion and allows the reduction in both profile and size of the device in respect of amplatzer vascular plugs . 
once in contact with blood , dmso rapidly dissolves and ethylene vinyl alcohol begins the polymerization process [ 52 ]  . the great advantage of onyx resides in the injection technique : the non - adhesive nature of the mixture , and the relatively long time of polymerization , ensures in - vessel navigation by onyx , favoring the embolization of distant lesions ; in addition , onyx progressive polymerization helps to prevent nontarget embolization and reflux , making the embolization process safer with respect to other liquid embolic agents . 
onyx disadvantages consist of the necessity of dmso - compatible catheters , higher procedural costs and a good experience in onyx injection / manipulation , in order to prevent nontarget or distal embolization . venous sac embolization ( vse ) vse has been also proposed as an alternative technique to feeding artery embolization for pavms endovascular management . 
maximum intensity projection coronal reconstructions show vascular plugs ( arrowheads ) in the lumen of the feeding arteries of two pavms ( arrows ) in the right lower lobe ( a ) ; to notice that the site of deployment is distant from the nidus for both vascular plugs , increasing the risk of vascular collateralization to the lesions . 
on the other hand , coils produce more metallic artifacts in respect of vascular plugs ( b ) that can make posttreatment assessment more difficult 1 3 984 la radiologia medica ( 2019 ) 124 : 973988 fig . 
10 digital angiography ( a ) in a 28 - year - old woman with a pulmonary fistula of the left lung characterized by unique feeding artery ( dot ) and a large aneurysmatic vein ( star )  . 
the deployment of a plug ( thin arrow ) proximal to the shunt was preferred over the coil due to the high risk of systemic migration ; marked flow reduction in the aneurysmatic vein was obtained ( c )  . 
embolization is completed by the deployment of two coils ( thick arrow ) behind the plug ( d ) , with no evidence of fistula reperfusion at the final angiographic control ( e ) embolization is the complete savings of the arterial pulmonary circulation , with a reduced risk of nontarget embolization and complications , such as pulmonary infarction . 
in this sense , the procedure may be useful when feeder arteries are too short to allow safe treatment or when the target of embolization is a high - flow pavm , with an increased risk of paradoxical embolization [ 62 , 63 ]  . 
given the increased risk of coil migration on the venous side of the pavm , due to the presence of larger vessels , some authors suggest the use of a detachable coil as first , in order to obtain a safe coil deployment and reduce complication during the filling phase of the procedure [ 62 , 63 ]  . there is poor literature evidence and no consensus about which is the best way among venous and arterial approach for venous sac embolization ; in essence , both techniques seem to be effective [ 64 , 65 ]  . followup andposttreatment evaluation follow - up of patients with pavms is also important : according to the international guidelines for diagnosis and management of hht [ 25 ] , patients with small pavms not requiring embolotherapy , or patients with suspected pavms , should undergo ct examination after case - by - case analysis , every 15years ; for those undergoing embolotherapy , first ct examination should be performed at 612months and then every 3years ; this reduced follow - up time interval is recommended because up to 20% of patients with treated pavms will experience lesion recanalization as the consequence of pavm reperfusion at the site of embolization , new vessels recruitment , preexisting feeding vessels hypertrophy or as the consequence of an incomplete exclusion during the first 1 3 la radiologia medica ( 2019 ) 124 : 973988 fig . 
contrast - enhanced ct is considered the standard technique for follow - up of these patients ; good treatment outcome is confirmed by the reduction in size of the nidus and the absence of enhancement in the treated feeding arteries ; draining veins may preserve contrast enhancement , but this sign is not specific because a retrograde perfusion of the lesion is possible [ 26 ]  . 
 [ 68 ] , authors suggest that an absolute diameter of 2.5mm or more of the draining 1 3 986 la radiologia medica ( 2019 ) 124 : 973988 vein at follow - up unenhanced ct was strongly associated with pavm patency after endovascular treatment . time - resolved mr may offer advantages in the follow - up of treated pavms , especially for those treated with coils , because the induced metallic artefacts , that limit ct diagnostic performance , have less impact on mr images evaluation [ 69 ]  . 
a diagnostic and therapeutic flowchart for patients with suspected pavm is shown in fig.11. conclusion pavms persist to be a medical challenge in the face of their complex anatomy , their vague and variable clinical appearance and the particular population ( hht ) involved by this disease . 
the radiologist plays a key role in the diagnostic workup of pavms , but there is still much to be done to improve both ct and mr protocols , in order to modulate dose and personalize the examination . endovascular treatment is now identified as the treatment of choice for pavms , offering lower complication rates and less hospitalization time , compared to surgery . 
however , chemotherapy and radiation therapy comprehend a complex scenario due to the wide choice of strategies including neoadjuvant vol . : ( 0123456789 ) 1 3 956 la radiologia medica ( 2019 ) 124 : 955964 chemotherapy ( nact ) , followed by surgery [ 4 ]  . 
the choice of the most adequate treatment usually depends on certain prognostic factors , such as tumor volume , parametrial and lymphovascular space invasion revealed through biopsy and locoregional lymph node status [ 5 , 6 ]  . 
mr imaging is the gold standard for accurate preoperative assessment of tumor volume and parametrial invasion as well as detection of lymphadenopathy [ 4 ] ; indeed , great importance has been given to nodal disease in the last figo staging guidelines of 2018 , being considered one major prognostic factor . on the other hand , histopathological analysis is the gold standard for establishing tumor heterogeneity , but in many cases it is difficult to assess structural , phenotypic or genetic intratumoral features on the basis of random sampling or biopsy [ 7 ]  . 
however , identification of some phenotypic or genetic features can be useful to predict response to neoadjuvant therapy in order to make therapeutic decisions and to avoid over - toxicity in connection with ineffective treatment . differentiation of histological features using conventional mr imaging is still challenging because tumors may be very similar in appearance on conventional t2 - weighted images despite histological diversity [ 8 , 9 ]  . 
in this contest , texture analysis ( ta ) applied to imaging has proved to be an imaging prognostic marker for poor survival in several tumor types ( colorectal primary tumor and liver metastases , lymphoma , lung , head and neck , esophageal renal and prostatic cancer ) correlating with glucose metabolism , stage and unfavorable genetic mutation [ 9 , 1221 ]  . in particular , magnetic resonance ta has proved to be an imaging biomarker of tumor response to neoadjuvant therapy in breast cancer ( using t2 and t1 contrast - subtracted sequences ) [ 22 ] and to neoadjuvant chemoradiotherapy in rectal cancer ( using t2 sequences ) [ 23 ]  . 
another recent study has demonstrated that texture analysis applied to mrdynamic contrast - enhanced images is useful for outcome prediction [ 24 ]  . regarding cervical cancer , few preliminary studies evaluated the efficacy of texture to identify node involvement or to predict local recurrence after chemiotherapy , with promising results . 
the aim of this study was to investigate any correlation between tumor features ( grading and histology ) and ta parameters or conventional parameters ( maximum diameter and adc value ) to evaluate which of the conventional parameters and ta parameters better predict the response to nact , and if there was any possible correlation between each other . materials andmethods study population from november 2015 to april 2016 , 28 patients ( age range 3565years ) with lacc were retrospectively evaluated applying texture analysis to mr images obtained prior to nact . 
diagnosis of cervical cancer was previously confirmed in all patients through diagnostic hysteroscopy and biopsy , and histopathological examination had established histological type and tumor grading . all patients were staged according to the figo criteria and all underwent vaginal and rectal examination under anesthesia as well as a standard chest radiograph . 
patients were excluded from the study if : ( a ) mr imaging acquisition was incomplete ; and ( b ) nact was discontinued before surgery . mr examination mr imaging was carried out using a 3t scanner ( discovery mr750 ; general electrics , milwaukee , wi ) equipped with high - performance gradients using an 8 - channel - phased array coil with the patient in the supine position . 
mr protocol included high - resolution morphological imaging of the pelvis using turbo - spin echo ( tse , repetition time , 20864172ms ; echo time , 11.4122.3ms ; nex , 2 ; slice thickness , 4mm ; matrix , 512 512 ) oriented in the sagittal plane , axial oblique plane ( perpendicular to the major axis of the cervix ) and coronal oblique plane ( parallel to the major axis of the cervix )  . neoadjuvant therapy andsurgical technique patients affected by lacc were scheduled to receive three 21 - day cycles of platinum - based nact followed by radical surgery as already described in the literature [ 25 ]  . 
in patients whose lesions remained unresectable also after nact , tumor response was assessed through clinical 1 3 la radiologia medica ( 2019 ) 124 : 955964 evaluation and assessment of tumor volume / disease extension revealed at the most recent mr examination after nact . texture analysis heterogeneity of the cervical tumor was assessed with texrad , a proprietary software algorithm ( texrad ltd , somerset , england , uk )  . 
a region of interest ( roi ) was delineated around the cervical lesion area on a single - slice t2 - weighted mr image by a radiologist with 6years experience in abdominal mr imaging . 
texture analysis of image within the roi was obtained using the filtration - histogram method that comprises an initial filtration step that highlights image features of a specified size , followed by histogram analysis of the filtered image [ 9 ]  . the filter basically extracts and enhances intensity - variation features of different sizes corresponding to the spatial scale of the filter itself ( ssf in radius ) : fine ( ssf = 1mm ) , medium ( ssf = 1.51.8mm ) and coarse ( ssf = 2mm )  . 
quantification of histograms ( with and without filtration ) was based on the calculation of the following parameters : mean : average value of pixel intensity ; mean positive pixels ( mpp ) : average value of positive standard deviation ( sd ) : variation or dispersion from the ( hyperintense ) pixels ; mean value ; skewness : a measure of the asymmetry of the histograhyperintense features within the image increase the mean value and result in positive skewness , whereas hypointense features within the image decrease the mean value and result in negative skewness [ 8 , 9 ] ; entropy : the disorder and randomness of gray - level distribution in terms of pixel orientation within the image ; kurtosis : a measure of the peakedness of the histograa positive kurtosis indicates a histogram that is more peaked and consequently that the collected data are distributed mainly around their mean . 
this indicates that there is more variability and heterogeneity in the dataset [ 8 , 9 ]  . conventional evaluation radiologists collected for every case the maximum diameter expressed in millimiters and evaluated on t2 oblique plane . to calculate adc parameters , radiologists draw a region of interest ( roi ) on the peripheral portion of the lesion on the adc map ( mean size 3 mm2 ; range 25 mm2 ) , with careful exclusion of the necrotic or cystic portions inside the tumor . statistical analysis descriptive statistics are provided as mean standard deviation for continuous variables . 
unpaired t test was used to evaluate whether the obtained data were statistically different comparing squamous cell carcinoma to adenocarcinoma , g3 to g1g2 tumors , and responders to non - responders . 
ta showed that adenocarcinoma exhibited more bright pixels on mr images than squamous cell carcinoma , thereby presenting high values , both mean pixel values ( mean ) and mean of positive ( hyperintense ) pixels ( mpp )  . 
 the mean area under the curve ( auc ) used to discriminate between adenocarcinoma and squamous cell carcinoma was 0.91 using coarse filtration ( ssf 2 ) with a significant discriminatory power ( p = 0.002 ) : the optimal cutoff for identifying adenocarcinoma was 29 . 
 kurtosis showed a tendency to be lower in patients with adenocarcinoma , but there was no statistically significant difference between the two histological groups . ta andtumor grading dividing the lesions into three categories : well - differentiated ( g1 ) , moderately differentiated ( g2 ) and poorly differentiated ( g3 ) , histopathological examination classified one patient in g1 , 15 in g2 and 12 in g3 . 
 a total of 15 patients responded to nact : 3 presented complete response ( cr ) and 12 presented partial response ( pr ) ; 13 patients were non - responders : 6 had disease progression ( pd ) and 7 had stable disease ( sd )  . ta andtumor response tonact ta parameters related to response to nact are listed in table 3 . 
this filtration seemed to yield the lowest p values ( p = 0.002 ) when unpaired t test was applied to compare the difference between responders and non - responders . 
the optimal cutoff found for kurtosis to identify non - responders was 3.7 yielding a sensitivity of 92% and a specificity of 75% conventional parameters did not show any significative correlation to the tumor response to nact . 
few studies reported that lower value of adc correlated with poorer prognosis [ 26 , 27 ] even in our sample we had a lower mean value , however , not statistically relevant . 
in contrast , adenocarcinoma presents an alternation of solid and fluid components ( glandular elements and contents of the glandular duct , respectively ) which may explain a more heterogeneous distribution of pixels in the histogram with both alternating positive pixels ( the vast majority ) and negative fig . 
 the greater structural homogeneity seems to reflect also the better response rates and complete response to nact which are usually obtained in cases of squamous cell carcinoma as reported in the literature [ 2932 ]  . 
the structural heterogeneity of adenocarcinoma expressed the tendency of this tumor type to be more aggressive and less sensitive to nact . texture analysis andhistological grading well - differentiated tumors have a better prognosis than poorly differentiated tumors [ 32 ] , but in this study none of the texture parameters yielded a statistically significant correlation with histological grading . 
however , it may be interesting to mention that , even if not statistically significant , kurtosis was slightly lower in patients with high - grade lesions ( g3 ) than in patients with intermediate - grade lesions ( g1g2 ) , thus reflecting a greater dispersion of pixel distribution in g3 tumors linked to the higher heterogeneity of tumor structure . texture analysis andtumor response tonact at ta , responders presented a higher degree of kurtosis expressing a more homogeneous distribution of pixels within the lesions , whereas non - responders presented greater heterogeneity with lower kurtosis . 
this variability may reflect a more disorganized histological structure with great alteration of tumor cell morphology , nuclear enlargement and an ineffective vascular net causing a reduced efficacy of chemotherapeutics . 
in line with the more heterogeneous histological structure and to the more aggressive biological behavior , adenocarcinoma showed a lower peak of the histogram ( arrow ) than squamous cell carcinoma and a lower kurtosis 1 3 962 la radiologia medica ( 2019 ) 124 : 955964 fig . 
responders showed a more homogenous pixels intensity , with a less dispersion of pixel distribution and a higher peak of the histogram ( red arrow ) and a consequent higher kurtosis compared to non - responders . 
from a clinical point of view , being able to early detect responders patients would allow to avoid ineffective treatments , the collateral effects directly associated , and at last start alternative therapies . 
even if the use of a 3t mr system can reduce the impact of image noise on biological heterogeneity , which can affect texture analysis , especially using fine texture scale [ 16 ] , we should consider that mri can introduce a higher variability in data acquisition than ct can , related mainly to the complexity of the technique and the higher number of parameters that can be modified . 
this variability could , in theory , affect reproducibility of the results . certainly it would have been better to normalize the whole image before applying texture analysis , but we decided to use the original non - normalized images to demonstrate the feasibility of texture analysis using t2w mr images . 
moreover , other authors in literature have successfully used mrta in non - normalized t2 - weighted images in rectal and breast cancer [ 23 , 33 ]  . finally , our considerations are based solely on ta values correlated to histological tumor type , grading and response to treatment but there is no correlation with markers of tumor angiogenesis , glucose metabolism and hypoxia which may influence tumor aggressiveness according to previous studies . 
it would be interesting to compare pre - treatment texture data with post - nact texture analysis and with patient survival . conclusion in conclusion , ta applied to t2 - weighted mr sequences of lacc seems to be a promising tool for describing tumor heterogeneity having demonstrated a strong potential for differentiating adenocarcinoma from squamous cell carcinoma and predicting response to nact . 
 therefore , ta may add information to patient prognosis , 1 3 la radiologia medica ( 2019 ) 124 : 955964 especially when data from histological specimens are limited and insufficient . 
diagnostic accuracy values for diagnosing bme were calculated for dect maps ( qualitative assessment ) and for ct numbers ( quantitative assessment ) by using receiver operator curves and area under the curve ( auc ) , using mri as the gold standard . 
sempreboni 10 , 37024negrar , vr , italy 2 department oforthopedic surgery , irccs sacro cuore hospital , negrar , italy introduction bone marrow edema ( bme ) of the ankle represents a common clinical problem in adult population [ 13 ]  . 
it may be diagnosed following acute traumas , or in a chronic clinical scenario without recent traumas , as , for example , in the bone marrow edema syndrome or in post - traumatic arthritis [ 46 ]  . 
early preventive measures , including restriction or cessation of activity after the diagnosis , may be crucial in preventing further deterioration of articular lesions [ 8 , 9 ]  . 
a recently published meta - analysis confirmed that the diagnostic performance of dect for the evaluation of the spine ( sensitivity , 0.84 ; specificity , 0.98 ) and of the appendicular skeleton ( sensitivity , 0.84 ; specificity , 0.93 ) was excellent [ 20 ]  . 
nevertheless , the majority of these studies focused on patients in the acute settings , and there no papers available describing the role of dect in diagnosing bme of the ankle in patients without recent trauma . 
moreover , dect has been used for the evaluation of urate deposition in patients with gouty arthritis and for the assessment of achilles tendinopathy [ 2427 ]  . the purpose of our study was to investigate the diagnostic accuracy values of a third - generation dect scanner in detecting bme in the ankle , by using mri as the standard of reference . materials andmethod patient population this prospective study was approved by the institutional review board , and all patients provided informed consent . 
eligibility criteria were represented by acute pain following sprained ankle ( n = 13 ) , or chronic pain ( n = 27 ) in patients with negative conventional radiographs . 
the ct examinations were used for the evaluation of ankle anatomy and to rule out subtle meshed fracture , while mri was used to assess the presence of bme and to evaluate ankle ligaments and tendons . four patients were excluded because of non - mri - compatible pacemaker ( n = 1 ) , incomplete mri protocol ( n = 1 ) , metal artifacts from previous surgery ( n = 1 ) , and claustrophobia ( n = 1 )  . 
1 diagram showing flowchart of patients enrolled 1 3 1030 la radiologia medica ( 2019 ) 124 : 10281036 product was set at a ratio of 1.6 : 1 ( tube a , 220 quality reference mas ; tube b , 138 quality reference mas )  . 
soft tissue kernel ( qr32 ) 80 - kvp and 150kvp set images were transferred to an offline workstation ( syngovia vb20 ; siemens , erlangen , germany )  . the software uses a three - material decomposition resulting in a virtual non - calcium image ( vnca )  . 
the information was color - coded with a color lookup table which codes bone marrow and edema in shades of green - yellow to orange - red ( parallelly to the progressive increase in density ) ; 3d volume rendering maps coding bone marrow edema in shades of green and normal bone in blue were also available . 
the de - specific information was fused with the conventional grayscale morphologic images ( thickness , 1mm ; increment , 1mm )  . mri protocol mr imaging was performed with a commercially available 1.5 - t unit ( magnetom avanto fit ; siemens healthcare , erlangen , germany )  . 
standard t1 - weighted spin - echo , t2 - weighted turbo spin - echo , and turbo inversion - recovery magnitude ( tirm ) sequences were performed in the axial and sagittal orientation . 
 image analysis on all images datasets available , each ankle was evaluated for the presence of bone marrow edema using a binary classification system ( 1 = presence of bme and 0 = absence of bme )  . 
at mri , the diagnosis of bme was based on signal intensity increase at tirm imaging with a signal decay at t1 - weighted imaging . in the second reading session , dect images were analyzed by two independent radiologists ( reader 1 and reader 2 , with 15 and 35years of experience in radiology , respectively )  . 
standard axial , coronal , and sagittal reconstructed ct and dect images ( 3d and 2d color - coded maps ) were analyzed in a random order , blinded to clinical and mri findings on a dedicated syngovia workstation , in order to calculate diagnostic accuracy values . 
the diagnosis of bme was based on the presence of shades of green - yellow to orange - red on 2d maps and on the presence of shades of green on 3d maps . 
for any disagreement on the presence of bme , a consensus reading was appended , and the consensual results were used for further analysis . in the third reading session , the dect images were reevaluated randomly after 30days by reader 2 and reader 3 in order to determine the intraobserver agreement . finally , the quantitative analysis of dect numbers was performed by the same two readers on dect maps or standard ct images according to radiologist choice by achieving two circular regions of interest ( roi ) for each involved area , and using mean value for further analysis [ 13 ]  . 
in positive cases , normal adjacent bone in the spared segment was used for comparison . the site of bme ( involved bones ) and presence of associated imaging findings including ocl of the talus , meshed fractures , or stress fractures were recorded by the readers 1 3 la radiologia medica ( 2019 ) 124 : 10281036 1031 on mri and dect images with mri images available , we placed the rois at the location with highest density changes on dect maps according to the radiologist choice . table 2 clinical data of patients enrolled parameter value statistical analysis the statistical analyses were performed with statacorp . 
the receiver operating characteristic ( roc ) curve analysis and calculations of the area under the roc curve ( auc ) were used to evaluate the attenuation values from dect scans . 
the optimal cutoff value in hu showing the highest accuracy for distinguishing presence versus absence of bone marrow edema was determined by using youdens index and roc curves and used for calculation of diagnostic accuracy values . 
the sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) , and accuracy of dect for the diagnosis of bme were calculated on a per - patient basis as regards both qualitative and quantitative assessment . 
interobserver and intraobserver agreements for the qualitative analysis were calculated with weighted k - statistics as follows : poor agreement = less than 0.20 ; fair agreement = 0.200.40 ; moderate agreement = 0.400.60 ; good agreement = 0.600.80 ; very good agreement = 0.801.00. results clinical data of patients enrolled are summarized in table2 . 
bme was depicted in patients with recent trauma in 9 / 13 cases ( 69.2% ) and in 16 / 27 patients ( 59.2% ) suffering from chronic pain . the diagnostic accuracy values of dect on a perpatient analysis are summarized in table3 . 
on the sagittal reconstructed 1 - mm 2d dect color - coded image ( b ) , the bme areas are characterized by shades of green to yellow ( white arrows )  . 
on the coronal t1 - weighted image ( b ) , the ocl ( white arrow ) is hyperintense , whereas the bme appears slightly hypointense ( arrowheads )  . 
on the coronal 1 - mm reconstructed 2d dect color - coded map ( c ) , the ocl is imaged as a red area ( white arrow ) with surrounding bme appearing as shades of green ( arrowheads )  . 
on the coronal 3d dect image ( d ) , the bme is coded in green ( arrowheads ) , whereas the ocl , not directly recognized , is characterized by a subtle transparence ( white arrow ) fig . 
on the sagittal 1 - mm reconstructed 2d dect map ( c ) , the stress fractures ( white arrows ) can be recognized on the posterior aspect of the heel , associated with diffuse bme . 
 while our results confirmed similar values as regards the sensitivity ( 90% and 87.5% , respectively ) , we obtained higher values of specificity ( 86.6% for both readers )  . 
moreover , the qualitative assessment of 2d and 3d maps was superior to the attenuation measurements in the detection of bone bruises around the ankle joint ( 90% accuracy for reader 1 versus 87.5% accuracy of quantitative analysis )  . 
achieved different cutoff values , namely 80hu , 70hu , and 39hu , for ankle mortise , talar dome , and talar body / head , respectively [ 21 ]  . 
 the difference of ct numbers and of the relative cutoff with respect to previous studies [ 16 , 21 ] could be partly due to the use of different parameters ( 80kv150kv with a tin filter versus 80140kv ) and software employed . 
conversely , ct numbers may become less accurate going distally in the foot , because of the relative small size of mid - foot bones , with relative prevalence of cortical bone . 
however , in our experience , the analysis of ct numbers may help in selected cases to characterize subtle or equivocal imaging findings at the visual assessment . bone sclerosis represents a pitfall for vnca imaging in the ankle . 
bone sclerosis could cover a mild area of bme , especially in the subchondral regions ; an abnormal subtraction process in these cases would lead to the presence of normal ct numbers at the quantitative assessment . 
conversely , a mild sclerotic area can generate a local increase in ct numbers in a bme spared area , leading to a fp result in both the dect maps and on the quantitative assessment of ct numbers . 
the patient was experiencing pain relief at the time of the 3 - month imaging follow - up , showing the reduction in the bme of the talus and of the conspicuity of the ocl . in our study , we had a prevalence of patients suffering from chronic pain of the ankle with respect to patients with acute traumatic paalso , all the two cases of meshed fractures not diagnosed on x - ray examinations and the three stress fractures were correctly pointed out at dect . 
in these cases , the standard high - resolution ct images represent an additional tool for the assessment of cortical bone involvement [ 29 , 30 ]  . the ocls of the talus were correctly diagnosed in 4 of 5 cases , with good correlation with mri images . 
in this case , the possibility to evaluate the high - resolution ct images on multiple planes allowed us to rule out the presence of migrated fragments and to confirm the integrity of cortical bone . 
first , a relatively limited number of patients were included and larger studies are 1 3 la radiologia medica ( 2019 ) 124 : 10281036 1035 needed to corroborate our results . 
second , a comparative analysis of qualitative versus quantitative analysis was not performed ; as previously discussed , we believe that the quantitative analysis could represent an additional tool that helps radiologists to discriminate subtle imaging findings . 
diagnostic performance parameters and receiver operating characteristic ( roc ) curves of cesm were calculated and compared to those of ffdm or ffdm + bus ( mcnemars test )  . 
good agreement between tumor diameters measured using cesm and histopathology was observed ( spearmans rank correlation , r = 0.891 , p < 0.0001 ) , although this technique tended to produce an overestimation of the size ( + 7mm )  . conclusions cesm has high diagnostic accuracy and can be considered as a useful technique for the assessment of breast lesions . keywords contrast - enhanced dual - energy spectral mammography ( cesm ) digital mammography breast cancer iodinated contrast medium breast ultrasound * octavio prez - luzardo octavio.perez@ulpgc.es 1 breast imaging section , department ofradiology , grupo hospitalario san roque , c / dolores de la rocha , 35001laspalmasdegrancanaria , spain 2 breast surgery service , insular andmaternal andchild hospitals , plaza pasteur s / n , 35016laspalmasdegrancanaria , spain 3 research institute ofbiomedical andhealth sciences ( iuibs ) , university oflas palmas de gran canaria , paseo blas cabrera felipe s / n , 35016laspalmasdegrancanaria , spain 4 spanish biomedical research centre , physiopathology ofobesity andnutrition ( ciberobn ) , madrid , spain introduction an estimated 1.7 million new breast cancer cases are diagnosed each year , and it is also the cause of the highest number of cancer deaths among women ( around 570 , 000 deaths per year ) [ 1 ]  . 
the implementation of screening programs based on the performance of mammograms on the general population , together with the development of neoadjuvant chemotherapy and anti - estrogenic therapy , has contributed to decreasing mortality due to this disease [ 2 ]  . 
this allows ffdm to use a dual - energy subtraction algorithm to depict contrast - enhanced cancers that would otherwise be occult on standard unenhanced mammography [ 59 ]  . 
this makes cesm a very promising technique , since it combines the relative simplicity , low cost , and practicality of the mammography with the high sensitivity of the mri [ 912 ]  . cesm was launched in 2010 ( senobright cesm , general electric healthcare , usa ) , but it is still available only in a relatively small number of breast imaging centers , and it is estimated that only around 200 , 000 cesm examinations have been performed to date in both research and clinical settings [ 13 ]  . 
in fact , the available studies in which the diagnostic performance of this technique is evaluated include about 3000 patients in total ( average 160 patients / study ) [ 1420 ] , and a recent review has indicated that further studies with larger series of patients are needed to validate the initial literature [ 4 ]  . since cesm implementation in our hospital in 2013 , it has been employed routinely and a retrospective analysis of our imaging bank has been made . 
we have included 644 breast lesions studied by cesm ( 465 patients ) , and we have compared its performance to that of ffdm , alone or combined with breast ultrasound ( bus )  . patients andmethods patients andstudy design in our hospital , women without contraindications for the intravenous administration of an iodine - based contrast agent are eligible for cesm if : ( a ) a clarification of already identified abnormalities by mammography and / or bus is needed , namely mass lesions , areas of parenchyma distortion , focal asymmetries , or suspicious microcalcifications , or ( b ) they need further evaluation of heterogeneous dense breast parenchyma . 
since cesm implementation in our hospital , all patients have been informed that this is a novel technique and that their radiological data could be used in future scientific studies . 
only those patients from whom written informed consent was obtained , according to a model previously approved by the ethics committee of our institution , were included in this study . 
exclusion criteria included pregnancy , breast feeding , age less than 18 , known brca1 / brca2 carriers ( in whom mri is the only cost - effective technique for supplemental screening [ 21 ] ) , history of renal disease , and allergy to iodine . we collected and recorded the following information from each patient : age , personal and familial history of breast cancer , clinical symptoms ( nipple discharge , palpable mass , skin retraction , inflammatory breast ) , indication of cesm , and the presence of additional malignant lesions . 
all the imaging techniques were performed within a time window of maximum 8days . the senobright application allows the production of low and high energy image for each mammography view which in turn gives a recombined image that shows the enhanced structures . 
two minutes after injecting the iv contrast media , low and high energy images are acquired following this order : a cranialcaudal view of non - suspicious breast ; b mediallateral oblique view of non - suspicious breast ; c mediallateral oblique view of suspicious breast ; and d cranialcaudal view of suspicious breast . 
they did not even have the information about which breast was suspicious of malignancy / pathology , since the workstation always presents the images in the same way , independently of the order in which they were obtained . 
the radiologists were provided with a template in which they could categorize the information related to each lesion observed by cesm according to the qualitative morphological descriptors previously described for this technique , based on the bi - radsmri [ 23 , 24 ]  . 
subsequently , they assigned the lesion a 15 classification as proposed previously for cesm ( 1negative ; 2benign findings ; 3probably benign ; 4suspicious abnormality ; and 5highly suspicious of malignancy ) [ 23 , 24 ]  . 
breast density was categorized according to the recommendations of the american college of radiology [ 25 ] as class a : fatty ; class b : scattered fibroglandular density ; class c : heterogeneously dense ; or class d : extremely dense . in the second stage , two other radiologists with more than 10years of experience ( > 12 , 000 mammograms / year ) reviewed all the discrepant cases ( 9.8% of cases ) that is , when a given descriptor was scored differently by the three radiologists [ 23 , 24 ] and provided a consensus opinion . 
 finally , the principal investigator correlated all data between both techniques and was also responsible for relating the imaging results to the gold standard employed as reference . reference standard procedures used toaddress true disease status to assess the current disease status of each patient disease status of each patient , different strategies were followed , depending on the type of lesion [ 3 , 26 , 27 ]  . when available , histopathological result , from surgery or biopsy , was used as the reference standard . 
in the case of cysts , an additional ultrasound was performed in which an aspiration of the contents of the cyst was done , in order to prove its non - solid nature . 
when the result of the histopathological analysis of this aspirate revealed the presence of atypical cells , the lesion was similarly biopsied , and the histopathological result was considered the gold standard . 
 in the cases in which superimposed fibroglandular tissue gave rise to a suspicious lesion , an additional localized mammography projection of the area and also a supplementary bus study oriented to that area were performed . 
in these recalls , if the images remained unchanged , the patient was discharged and in the other eventuality a biopsy of the suspicious area was performed , and the histopathological result obtained was considered as the gold standard . 1 3 la radiologia medica ( 2019 ) 124 : 10061017 1009 the biopsy was usually performed immediately after cesm examination . 
however , when the patients were referred for the cesm imaging for cancer staging ( 84 patients , 118 lesions ) , they had previously undergone the biopsy before cesm examination . 
however , as described above , the radiologists participating in this study did not have this information when they retrospectively reviewed the images . for evaluation of the diagnostic performance of ffdm , ffdm + bus , and cesm , lesion images classified 13 were considered as benign and 45 as malignant . all histopathological diagnostics were performed by the same certified pathologist with 20years of experience in breast cancer . 
immunohistochemical determination of estrogen receptor ( er ) and progesterone receptor ( pr ) was carried out , and her - 2 / neu status , tumor grade , and nodal involvement in malignant cases were also assessed . statistical analysis all the statistical analyses were done using graphpad prism v6.0 ( graphpad software , ca , usa )  . 
using the benignmalignant cutoff value , sensitivity , specificity , positive predictive value ( ppv ) , and negative predictive value ( npv ) were calculated for the three imaging modalities . 
the mean difference between the image and the histological results was calculated and related to the interval in which 95% of the calculated differences ( limits of agreement , loa ) were found . 
the differences between the imaging techniques and histological measurements did not follow a normal distribution ( kolmogorovsmirnov test ) , and therefore , nonparametric statistical tests were used in the subsequent analyses involving this variable ( mannwhitney u test or the kruskalwallis test [ for comparisons of more than two groups ] ) [ 9 ]  . 
 a total of 283 patients ( 367 lesions ) had a previous ffdm study , and 182 patients ( 277 lesions ) had a previous complementary ffdm + bus study . 
therefore , 367 lesions were seen by ffdm and cesm , and 277 lesions were seen by ffdm + bus and cesm . we employed the histopathological diagnosis of the surgical piece as the gold standard for the 426 malignant lesions obtained from the patients who underwent surgery . 
of these non - enhancing malignant lesions , three belonged to patients bearing breast prostheses ( 1 infiltrating ductal carcinoma , 1 ductal carcinoma insitu , and 1 invasive lobular carcinoma ) , and the remaining lesions were : infiltrative intraductal carcinoma ( 6 lesions ) ; intraductal carcinoma insitu ( 3 lesions ) ; angiosarcoma ( 2 lesions )  . 
seven of the 14 non - enhancing lesions were located in breasts that were classified as heterogeneously dense ( n = 3 , category c ) or extremely dense ( n = 4 , category d )  . 
for the 10 remaining benign lesions that were enhanced by the contrast medium , there did not seem to be any particular characteristic that explained the reason for said uptake . 
however , cesm did not improve the negative predictive value with respect to any of the other two diagnostic imaging methods . a similar trend was observed for the roc curves . 
the comparison among the auc values was statistically significant in all the cases : p < 0.001 for the comparison between ffdm and ffdm + bus ; p < 0.001 for the comparison between ffdm and cesm ; and p < 0.05 for the comparison between ffdm + bus and cesm . table3 shows only 63 lesions were misclassified by cesm ( 9.7% of the total series )  . 
compared to previous studies with fewer numbers of cases [ 3 , 1518 , 20 , 23 , 2830 ] , it practically quadruples the average number of lesions reported to date ( a range of 49261 lesions , an average of 158 lesions per study )  . several authors have demonstrated the similarity of the performance of cesm and contrast - enhanced breast mri [ 5 , 15 , 29 , 31 , 32 ]  . 
due to the similarities between the two techniques , it has been proposed that the bi - rads - mri could be used to characterize the cesm image of the breast lesions [ 23 , 24 ]  . 
the underlying causes of this misdiagnosis were related , in most cases , either to characteristics of the patients or to lesions , or to diagnostic limitations of digital mammography in general and of cesm in particular ( such as bearing breast prostheses )  . 
in our series , 87% of the misdiagnosed cases were included in one of the following groups : ( a ) lesions in high density breasts , which are more difficult to diagnose either by ffdm or cesm [ 17 ] ; ( b ) lesions in small breasts of thin , middle - aged women [ 9 , 35 , 36 ] ; ( c ) lesions in patients bearing breast prostheses [ 6 , 8 ] ; ( d ) belonged to special benign pathological conditions that have been reported to simulate malignant pathology , such as in the case of diabetic mastopathy [ 37 ] ; or ( e ) corresponded to microcalcifications without associated mass [ 28 , 38 ]  . 
4 prediction of tumor size by mammography ( left column ) , mammography plus breast ultrasound ( center column ) and cesm ( right column ) : ( upper panels ) box plots illustrating the median size difference between the imaging technique ( s ) and histopathology , with the corresponding interquartile range and whiskers from the 5th to the 95th percentile ; ( middle panels ) scatterplots and spearmans correlation coefficient of maximum tumor diameter measurements between the imaging technique ( s ) and histopathology ( lower panels ) ; bland altman plots illustrating the size difference between the imaging technique ( s ) and histology compared to the histological size . 
the recombined image shows the contrast enhancement of the two mass lesions without an enhancement of the microcalcification area ( which was finally part of a moderately differentiated infiltrative ductal carcinoma ) fig . 
the recombined image of cesm ( b ) does not clarify anything regarding the low energy image ( a ) , since the mammary parenchyma diffusely uptakes contrast media bilaterally , without highlighting the lesion in a specific way , and without a clear cause that may explain this behavior . 
it allowed detection of even some very difficult lesions , such as a carcinoma hidden behind a fibroadenoma , which has already been published by our group as an interesting case report [ 39 ]  . 
 this means that our results support the previous studies , indicating that cesm has high diagnostic accuracy , even higher than the combination of two complementary imaging techniques such as ffdm + bus . 
in any case , our results indicate that this technique can be considered as a useful imaging technique for the initial assessment of breast lesions , at least in the clinical setting . 
in our experience , cesm would have allowed us to rule out malignancy directly in up to 13.8% of cases ( 89 benign lesions out of a total series of 644 lesions were correctly classified as benign by cesm ) , avoiding delays in diagnosis ( and the associated stress ) , as well as additional costs . additionally , our results also indicate that tumor measurement with cesm has good correlation rates with the histopathologically determined size . 
 both the correlation indexes and the concordance percentages were similar or even higher than those described for the mri [ 4246 ] and , despite the overestimation of the size , definitely superior to that of the ffdm and ffdm + bus , as we have previously reported [ 9 ]  . 
preoperative accurate estimation of tumor size is very necessary for adequate surgical planning , and several authors have proposed that the most accurate measurement is obtained by mri [ 42 , 43 , 47 ]  . 
 according to the results of this study , cesm presented the best prediction rates of the actual size of the tumor piece , so it can also be considered a suitable imaging technique for this purpose . this study has several limitations . 
in addition , when analyzing the results , we found that there was a low representation of clusters of microcalcifications , as well as very few cases of carcinomas insitu . 
additionally , it should be also taken into account that certain patients , particularly those with benign lesions , were asked to participate voluntarily in the study in order to also observe the behavior of the lesions with low suspicion of malignancy , which might introduce a new case selection bias . 
it is also noteworthy that in a retrospective study , like the one presented here , it is not possible to directly compare the diagnostic performance of cesm with traditional imaging tools , such as magnified views , digital tomosynthesis of the breast , or targeted ultrasound . 
this may lead to bias in the results , although there are still no data to indicate the extent to which the menstrual cycle influences the uptake of contrast in cesm . conclusions our data allow the conclusion that the diagnostic performance of cesm is higher than that of ffdm or ffdm + bus . 
all the bodies were pmct - scanned prior to autopsy , and internal putrefactive state was determined using the radiological alteration index ( rai ) by a radiologist with expertise in forensic radiology and a forensic pathologist trained in forensic imaging . 
after pmct scans , grade of external putrefaction ( gep ) was assigned during the external examination and the complete autopsy was performed by forensic pathologists . results the pmct images evaluation revealed that the rai index was > 61 in all bodies , corresponding to a moderatemassive presence of putrefactive gas . 
the gas grade was > ii in correspondence of the major vessels , heart cavities , liver parenchyma , vertebra l3 and subcutaneous pectoral tissues , and varied from i to iii in correspondence of the kidney . 
cadaveric external examination revealed the presence of advanced transformative phenomena , with a gep3 and gep4 in most of the cases , with body swelling , eyes and tongue protrusion , body fluids expulsion and fat liquefaction . conclusion radiological imaging by pmct as an adjunct to autopsy in advanced decomposed bodies represents a useful tool in detecting post - mortem gas , even in very small amounts . 
following the most recent advances , ct technology is today frequently requested as a complement before conventional autopsy , or in some cases as a supplement , for non - invasive post - mortem diagnosis [ 24 ]  . 
 pmct offers a detailed visualization of anatomical structures , injury patterns or localization of foreign bodies prior to dissection [ 5 ] , allowing the study of body parts or areas that are not routinely dissected during a standard autopsy , such as the viscerocranium , craniocervical junction , larynx , shoulder girdle , pelvis , extremities and soft tissue of the back [ 69 ]  . 
furthermore , while the traditional autopsy determines a destruction of the residual findings , pmct allows preserving images for re - evaluation and reinterpretation over vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 10181027 1019 time , also with the aid of post - processing 3d reconstructions . 
pmct represents a useful procedure in many forensic scenarios that are often very difficult to interpret only with conventional autopsy [ 1014 ] , as in the case of decomposed bodies , because putrefaction processes can impressively alter the appearance of corps and consequently add more difficulty in determining the cause of death . 
in fact , body decomposition is determined by a combination of fermentation processes by gastrointestinal flora , aggression of external bacteria and other micro - organisms , and autolytic digestion of body tissues by endogenous enzymes . 
the rate and extent of post - mortem changes and decomposition processes are quite variable and are dependent on the cause of death and the external environment [ 15 ]  . 
as a consequence , examination of a putrefied body represents a remarkable challenge for the forensic pathologists [ 16 , 17 ]  . gas formation is a hallmark feature of putrefaction , since gaseous bloating in advanced decomposed bodies is determined by vascular and intra - parenchymatous gases . 
pmct allows to detect exact localization of post - mortem gas in the whole body , even in very small amounts , and to distinguish between normal decomposition processes and pathologic gas collections that may have contributed to causing the death , such as air embolism , pneumothorax or pneumoperitoneum [ 1829 ]  . the aim of the present study is to report radiological findings and features in advanced decomposed bodies obtained by pmct , even if possible with autopsy correlation . 
an overview of the radiological cadaveric modifications in different anatomical sites , due to natural decomposition processes that can be mistaken for pathologic processes , is also offered . materials andmethods subjects this retrospective descriptive multicentric study was conducted between may 2013 and november 2016 , including forensic cases selected among those admitted to the medicolegal centres of rome , foggia and ferrara ( italy ) by the local enquiring authorities to ascertain the cause of death . 
eleven bodies ( cases 111 ) were exhumed on the order of a judge , while 30 bodies ( cases 1241 ) were found at the crime scenes ( table1 )  . 
cases 111 consisted of subjects deceased in a hospital with an ascertained pmi as obtained from clinical records , while cases 1241 were found dead after a presumptive pmi ( sd ) , reconstructed on the base of testimonies and forensic considerations . 
 pmct scans were performed on a 64 - section ct system ( somatom sensation cardiac 64 - slice scanner ; siemens , forchheim , germany ) according to standardized scanning protocol : tube voltage 120kv ; tube current 250mas ; section thickness 0.6 mm ; reconstruction interval 0.5 mm ; gantry rotation time 0.5 s ; and pitch 0.9. 
pmct data were transferred to a workstation for post - processing images reconstruction , performed with a slice thickness of 1.25mm in increments of 0.7mm , using soft tissue deconvolution algorithm ( b20 kernel ) and bone - weighted deconvolution filter ( b46 kernel )  . 
images were finally analysed using a viewing software ( osirix v.5.8.2 32 - bit ; pixmeo , geneva , switzerland ) , calculating two - dimensional sagittal and coronal reformations and volume rendering ( vr ) reconstructions . the present study was conducted in accordance with the helsinki declaration . 
as all the examinations were parts of a complete forensic examination ordered by the local enquiring authorities , no specific consensus by the relatives was necessary prior to the realization of all pmct ; after the examination , all results were analysed anonymously . image analysis images viewing and assessment was performed by 2 radiologists with expertise in forensic radiology ( 2 and 30years of experience , respectively ) and 2 forensic pathologists trained in forensic imaging ( 3 and 35years of experience , respectively )  . 
to promote consistent assessments , a concordance was preliminarily tested between the investigators . the internal putrefactive state was determined by the aforementioned observers using the radiological alteration index ( rai )  . 
rai was determined by pmct in 7 selected sites , including the major vessels ( left innominate vena and abdominal aorta ) , selected bones ( vertebra l3 ) , selected organs ( heart cavities , liver parenchyma and vessels , and kidney parenchyma ) and subcutaneous tissues and muscles ( subcutaneous pectoral tissues ) , according to the standardized protocol by egger etal . 
in particular , the grade of gas presence ( 0 , i , ii or iii ) was determined for the major vessels and selected bones ( one gas bubble to completely filled with gas ) , and for the selected organs , subcutaneous 1 3 1020 table 1 description of the main characteristics of 41 advanced decomposed bodies including sex , age , cause of death and post - mortem interval ( pmi ) cases age ( years ) cause of death pmi ( days ) la radiologia medica ( 2019 ) 124 : 10181027 haemorrhagic shock after femur fracture cardiogenic syncope heart failure by bleeding and anaemia acute bleeding in chronic subdural haematoma heart failure by anaemia haemorrhagic shock after femur fracture bleeding in non - hodgkins lymphoma haemorrhagic shock cardiogenic pulmonary oedema multi - organ failure septic shock ischaemic cardiomyopathy heart failure in alcohol intoxication traumatic brain injury fatal firearm injury fatal firearm injury asphyxia heart failure fatal firearm injury heart failure in chronic alcohol abuse heart failure arrhythmia in cocaine abuse dismemberment after fatal strangling accidental train falling injury drowning fatal firearm injury traumatic brain injury cardiogenic pulmonary oedema cardiogenic pulmonary oedema asphyxia drowning drowning drowning drowning drowning asphyxia slaughtering cardiogenic pulmonary oedema hanging frostbite cardiogenic pulmonary oedema 634 89 7 1 5 1 90 5 4 1 14 5 33 1 120 10 30 5 5 1 4 1 4 1 4 1 180 90 30 5 4 1 12 2 6 1 12 2 25 5 25 5 150 30 15 5 13 2 13 2 35 5 7 1 6 1 25 5 4 1 pmi post - mortem interval . 
cases 111 : ascertained pmi as obtained from clinical records ; cases 1241 : presumptive pmi ( sd ) reconstructed on the base of testimonies and forensic considerations tissues and muscles ( one gas bubble to extensive emphysema )  . 
once a grade was assigned for each site , according to the corresponding scores , the rai was calculated . conventional autopsy after pmct scans , the complete conventional autopsy of each body ( examination of the cranial , thoracic and abdominal cavities ) was performed by forensic pathologists . 1 3 la radiologia medica ( 2019 ) 124 : 10181027 1021 the grade of external putrefaction ( gep ) was assigned by the forensic pathologist during the external examination of the bodies , according to the standardized classification of maujean etal . 
 [ 31 ] , based on the putrefaction signs described in the forensic literature : sites heart cavities table 2 gas grade and score determined for 7 selected sites gas grades scores number of cases gep1 ( beginning ) : green skin discoloration was preliver parenchyma and vessent in the abdomen area ; gep2 ( moderate ) : detachment of the skin and / or blisters containing reddish purplish serous liquid occurred at the extremities and in the sloping regions ; gep3 ( advanced ) : putrefactive gases produced body swelling , eyes and tongue protrusion and body fluids expulsion ; gep4 ( major ) : fat liquefaction and / or darkening colouring of the integument and drying of the body extremities were observed ; gep5 ( mummified ) : drying of the whole body with sels left innominate vena abdominal aorta kidney parenchyma leather - like skin was evident . vertebra l3 a complete autopsy report was provided in all the cases , and causes of death were subsequently investigated by histological and toxicological examinations . 
in particular , the correlation between gep and pmi , and rai and pmi has been studied ; the correlation between gep and rai has also been investigated . results the pmct images evaluation and the analysis of putrefactive internal state revealed that , in all the examined cases , gas grade was > ii in correspondence of the major vessels ( left innominate vena and abdominal aorta ) , heart cavities , liver parenchyma , vertebra l3 and subcutaneous pectoral tissues ; in correspondence of the kidney , the gas grade varied from i to iii ( table2 )  . in the selected 7 sites , the rai index was > 61 in all bodies ( interval 61100 , median 85 ) ( table3 )  . 
in particular , intracranial gas accumulation was observed in all cases , distributed on the top of the calvarium and in the vascular structures of the posterior cranial fossa ; in 22 / 41 ( 54% ) cases , gas accumulation filled more than 50% of the whole intracranial space . 
small gaseous collections were ubiquitously distributed within the brain parenchyma , with a swiss - cheese aspect ; brain volume was reduced in all cases , placed in the sloping region of the calvariuin all cases , loss of definition of the greywhite matter junction and effacement of the sulci and ventricles were detectable . 
 as a consequence of the degenerative processes , adipose degeneration and fat liquefaction associated with multiple gaseous collections were observed in all examined bodies , with a marked fluid collection in the pleural and peritoneal space . 
soft and connective tissues were collapsed and showed gaseous degeneration , notably in correspondence of periskeletal muscular structures or in elective areas , i.e. , gaseous ballooning of the scrotuparenchymatous organs were not completely recognizable in shape and appearance , liquefied and characterized by the collapse of the residual parenchymas . 
grade of external putrefaction ( gep ) assigned in all the examined bodies resulted gep3 ( 11 / 41 , 27% ) and gep4 ( 18 / 41 , 42% ) in most fig . 
five out of 41 ( 12% ) bodies presented widespread phenomena of aggression by the fungal 1 3 1024 la radiologia medica ( 2019 ) 124 : 10181027 greyish pink colour , colliquated , homogenized and with pultaceous consistency . 
in the thoracic cavity , the pleural space showed accumulation of serosanguinous putrefactive fluid or resulted covered with a mixture of brownish - blackish putrefactive liquid and fine yellowish granular residue ; the lungs appeared collapsed towards the mediastinum , with pleura raised in bubbles , soft and pasty at palpation . 
8 autopsy findings : dura mater detached from the endocranium ( a ) ; brain colliquated , homogenized and with pultaceous consistency ( b ) ; heart flattened and empty , strongly reduced in form and consistency ( c ) ; intra - abdominal putrefactive phenomena ( d )  . 
furthermore , in advanced putrefaction , the texture can be completely dissolved , leading to liquefaction of entire organs , as shown in the images analysis carried out in the present study [ 9 , 16 , 19 ]  . 
these alterations often lead to misinterpretation of the radiological findings and to difficulties in determining the cause and manner of death . the knowledge of the standard pmct findings following the post - mortem changes and the decomposition status is important when interpreting pmct images , because decomposition has a great impact on the imaging features . 
the aetiology of post - mortem gas detected on pmct , in fact , can be multifactorial and not necessarily related to putrefaction [ 6 , 9 , 13 , 1621 ]  . decomposition gas normally occurs within 2448 - h postmortem and is typically produced by intestinal flora [ 20 ]  . 
 gas can be also detected in many other conditions such as sepsis , ischaemia and tissue damage , which is associated with rapid decomposition and putrefaction [ 32 ]  . 
intravascular gas could also be produced during cardiopulmonary resuscitation ( cpr ) : chest compression causes the vaporization of dissolved gas in blood and the rupture of pulmonary vessels , allowing the air to enter the pulmonary vein and reach the systemic circulation . 
furthermore , in hospitalized subjects , the bronchovenous fistulas caused by endotracheal intubation and the alveolar rupture caused by positive - pressure ventilation barotrauma may lead to intravascular gas entry [ 3335 ]  . on the other hand , putrefactive gas should not be mistaken for pathologic gas collections that may have contributed or caused the death , such as air embolism , pneumothorax or pneumoperitoneum [ 2226 ]  . in all the above - mentioned cases , asymmetric or focal gas collections should be considered suspicious and related to pathological or traumatic causes . 
in our study , an asymmetric soft tissue gas distribution was detected in perforating gunshot wounds through the chest in 2 cases , but these findings were clearly related to the underlying traumatic injury . 
in fact , gas presence was reported in many cases of penetrating trauma with associated lacero - contusive foci and air bubble at the entry site [ 19 , 36 ]  . radiological imaging by pmct , as an adjunct to conventional autopsy in advanced decomposed bodies , has been proven to be a useful tool in detecting post - mortem gas localization , even in very small amounts . 
in all the examined cases , a symmetrical ubiquitous gas accumulation has been detected within the heart cavities , vascular system , body cavities , parenchymatous organs , soft tissues and bones , as shown in results . our results have demonstrated in all cases ubiquitously moderate - diffuse presence of gas ( grade ii to iii ) , particularly in correspondence of soft subcutaneous tissues , vertebral body l3 and cardiovascular structures such as heart cavities , abdominal aorta and left innominate veinterestingly , parenchymatous organs have shown a different distribution pattern , as in correspondence of liver ( grade ii to iii ) and kidney ( grade i to iii ) a different gaseous amount has been found . 
this partial exception could be explained by the fact that the perirenal capsule protects more the renal structure from the putrefactive phenomena , coinciding with the autoptic data confirming that kidney moderately resists putrefaction . furthermore , according to pmct standardized imaging assessment and the subsequent statistical analysis conducted on gep and rai values , a strong positive correlation between the external and internal grade of putrefaction has been established . 
therefore , from the present study , the combined use of gep and rai resulted useful in the assessment of the putrefactive state in advanced decomposed bodies , providing reliable data prior to autoptic investigation and supporting the forensic pathologist in the evaluation of cadaveric post - mortem changes [ 37 ]  . conclusion according to this standardized approach , an objective description of the post - mortem transformative phenomena was offered . 
assessment of external ( gep ) and internal ( rai ) grade of putrefaction is even more important , considering its decisive role as an aid in discriminating the various causes of death , particularly confused by the overlap of putrefactive phenomena . 
scientific organizations supporting clinical radiologists and medical physicists have published guidelines reporting parameters useful to quantify the radiation output and to assess patient dose . conclusions our research revealed that there is not a shared interpretation of patient exposure information to be included in radiological report . 
in this respect , this directive should emphasize the need for justification of medical exposure , including the exposure of asymptomatic individuals , and should strengthen the requirements concerning information to be provided to patients , the recording and reporting of doses from medical procedures , the use of diagnostic reference levels and the availability of dose - indicating devices . 
after all , iaea basic safety standards also stressed the issue that patients have to be informed about benefits and radiation risks associated with radiological procedures [ 2 ]  . secondly , because of the increasing number of radiological examinations , such as interventional radiology ( ir ) procedures , or ct scansas reported , for example , by the organization for economic co - operation and development ( oecd ) [ 3 ] ( fig.1 ) , the knowledge about patient doses in medical procedures has become an important topic for population dose assessment [ 46 ]  . information included in radiological report should make aware the patient about radiological risk index associated with an increased probability of cancer over the remaining lifespan , arising from a medical exposure . 
the doses involved in diagnostic radiology , indeed , are below the minimum threshold dose for deterministic effects ( 100msv ) , but a potential dose for stochastic effects , i.e. , cancer induction and genetic changes . 
this radiation risk index is critically dependent on the age and sex distribution of the exposed population . without any other specification relative to art.58 point b , its implementation in european member states could lead to choice among four types of information : patient exposure , understood as a pure physical quantity related to x - ray tube output and thus a machine parameter ; absorbed dose , a physical quantity more complex than exposure , requiring a professional evaluation from a medical physics expert ( mpe ) starting from machine parameters ; effective dose , a radiological protection quantity providing a single number proportional to the radiobiological fig . 
 ( source : : / / data.oecd.org / healt heqt / compu tedtomog raphy - ct - scann ers.htm ) 1 3 la radiologia medica ( 2019 ) 124 : 783793 detriment from a particular type of radiation exposure [ 7 ]  . relative radiological risk index expressed as an average effective dose range , but identified using symbols or comparative scales [ 810 ]  . especially regarding the most known dosimetric quantity effective dose , scientific community knows that it results inappropriate for the estimation of individual risk , as it does not consider health status , age and sex [ 11 ] , and it is calculated using uniformly irradiated phantoms ( a different setting respect to routine radiological examinations )  . 
moreover , icrp 103 stated that the effective dose is calculated for a reference person and not for an individual ; for individual retrospective dose and risk assessment , individual parameters and uncertainties have to be taken into account , with the direct involvement of an mpe [ 7 ]  . the aim of this study was to properly define the information regarding patient exposure to ionizing radiations in the radiological report , according to the european directive 2013 / 59 / euratom ( eu 2013 / 59 art.58 ( b ) )  . 
to better understand the meaning of quantities analyzed later in the paper , a brief description is given in the following paragraphs . radiation dose metrics it is clear to scientific community that patient exposure does not mean patient dose , but it suggests some useful information to evaluate dose released to patient . using laymans term , exposure can be thought as how much is it raining ? , absorbed dose as how much did you get wet ? and estimated dose as what are the chances of getting a cold due to getting wet in the rain ? [ 12 ]  . patient exposure the information on exposure is a machine - related parameter representing the device output measured using specific tube settings ( tube voltage , tube current , exposure time , field of view , sourcesurface distance and so on )  . 
x - ray tube output is used to calculate incident air kerma ( ki ) , i.e. , the energy absorbed in air per mass unit on beam axis ( definition valid in diagnostic radiology energy range )  . 
a dose index representing incident air kerma can be easily defined for each radiological modality , using technical devices added to the equipment . this index is not the patient absorbed dose , but it could be correlated with patients features ( the thickness ) when , for example , an automatic exposure control system is activated ; anyway , it is related to patient dose . 
moreover , the dose index has to be previously validated by the mpe involved in radiological procedures optimization process and in quality assurance program . patient absorbed dose energy transported by radiation and then released to patient is the absorbed dose , i.e. , the energy imparted to matter ( the patient ) per mass unit . 
the biological effect of radiation is enclosed in the quantity equivalent dose , defined in a tissue t , given a physical absorbed dose dt released from different types of radiation . patient effective dose in order to take into account the contribution to the overall detriment derived from different organs radiosensitivity , icrp [ 13 ] introduces the effective dose ( expressed in millisievert , msv ) as the sum of products of tissue weighting factors and absorbed dose inside tissues and organs of the body . 
tissue weighting coefficients wt are derived from epidemiologic studies on population exposed to high dose of radiation and represent reference values for humans averaged over both sexes and all ages , thus not relating to characteristics of each individual [ 7 ]  . 
 the european report rp 154 [ 11 ] also confirms that effective dose should be used for comparison purpose only in order to assess , for example , doses from different diagnostic procedures performed in different hospitals and countries . 
 furthermore , rp 154 affirms that effective dose is not recommended for epidemiological evaluations . different softwares are available allowing to calculate effective or equivalent patient dose in medical exposure using different human phantoms and calculation models ( pcxmc [ 14 ] , ct - expo [ 15 ] , virtualdose [ 16 ] )  . 1 3 786 la radiologia medica ( 2019 ) 124 : 783793 relative radiological risk index in order to make aware patients about differences between radiological procedures and their associated risk , a relative radiation risk index could be included in clinical report . 
effective dose ranges are based on reviews of the current literature , us and european diagnostic reference level publications , and experience of medical physicists and radiologists . two examples of relative radiological risk index employed by radiologists as appropriateness criteria are described : relative radiation level ( rrl ) comparative scale [ 8 ] developed by the american college of radiology ( acr ) appropriateness criteria and dose classes system as reported by italian reference guidelines on diagnostic imaging [ 9 ]  . 
recently the european society of radiology provided an iguide reporting the rrls scale for common diagnostic procedures [ 10 ]  . acr suggested a comparative scale assigning a symbol for each radiation level associated with an effective dose range ( see table1 )  . 
a similar scale is given for pediatric patients [ 8 ]  . the italian association of medical radiology ( sirm ) [ 9 ] together with national health institutions also published a dose classification system for radiological procedures ( see table2 )  . a good approach for communicating medical exposure risk to patients in a radiological examinations , using effective dose or related levels , could be to quantify risk as the time needed to receive the same effective dose from natural background . 
table3 summarizes this comparison , assuming a background exposure of 3msv / year as reported by peck and samei [ 17 ]  . another way to convey the risk is to consider a chest radiography as a reference and then comparing a radiological procedure with the equivalent number of chest radiographies [ 9 ]  . international legislative background currently not all european member states have transposed the eu directive 2013 / 59 yet . in may 2016 , the european community approved a tender project to monitor the transposition of the basic safety standards ( bss ) directive ( eu 2013 / 59 ) into member states national legislation and to support its implementation in the medical area . 
 ( adapted from [ 8 ] ) relative radiation level adult effective dose estimate range ( msv ) example examination ultrasound ; mri limbs and chest radiography pelvis radiography and mammography abdomen ct and nuclear medicine bone scan abdomen ct with or without contrast and whole - body pet total body ct with contrast ; stent or shunt placement ; and interventionl radiology procedures table 2 risk classification of radiological procedures as provided by italian guidelines . 
one of the projects objectives was to prepare and perform a survey collecting information on member states strategies and plans for bss transposition ( medical area )  . regarding the effort of countries to transpose the art . 
 no more specification about which country and dose metrics definition was reported . in october 2014 , the board of heads of european radiological protection competent authorities ( herca ) approved an action plan [ 19 ] in relation to the transposition and implementation of eu 2013 / 59 . 
at the time of writing , the action 4 is still going on . since before the entering into force of new directive , some european countries provided in their legislation the inclusion of dosimetric information in radiological report , also specifying which dose unit should be indicated . the french legislation [ 20 ] , for example , established in 2006 that useful information for assessing dose received by patient ( [ ] les informations utiles lestimation de la dose recue par le patient [ ] ) has to be included in the radiological report ( more details in table4 )  . 
 french nuclear safety authority ( asn ) [ 22 ] is working with government on production of ministerial orders and on implementation texts of eu 2013 / 59 . in england , the department of health and social care has published in june 2018 the guidance to the ionising radiation ( medical exposure ) regulations 2017 [ 23 ]  . 
the sociedad espanola de fisica medica ( sefm ) during the vii national meeting on radiation protection in medical field ( april 2018 ) debated about eu 2013 / 59 transposition outcomes . 
in particular , sefm highlighted that the patient dose management , strongly hoped by the new directive , has stoked the business on dose recording systems [ 26 ]  . in italy , national law on radiation protection ( medical exposures ) [ 27 ] orders that the responsible practitioner and the employer , according to their own authority , provide for registration of every single radiological procedure although in a synthetic way ( article 12 )  . 
in particular , aifm contributed to insert in a regional health plan the population dose monitoring from medical exposures through radiological information system ( ris ) , as well as the faculty to inform patients about dose received by radiological examination . furthermore , because of the increasing spread of dose monitoring systems , aifm instituted in 2014 a working group with the aim of establishing reference guidelines on acceptance test of dose monitoring systems , claiming the need for a coherent , complete and uncorrupted migration of information from radiology modality to the software . 
the group published at the end of 2016 a complete report on general aspects of dose monitoring systems and on essential dose parameters to be collected for each modality [ 29 ]  . 
 the french decree [ 21 ] indicates that information relating to patient exposure , executed procedures and all information useful to assess dose received by patient , shall be included in radiological report . 
french legislation system was so sensitive to this issue maybe because of the great ct number per 1000 inhabitants in 2016 ( the greatest among the five countries considered ) [ 3 ]  . english regulations [ 23 ] in addition to what provided by france specify that such information might enable the estimation of the effective dose to the individual to be made at a later date , if necessary . german x - ray ordinance [ 24 ] only refers to dosimetric information recoding for each radiological procedure , without specifying dose metrics . 
article 58 ( b ) is not yet embodied in national law as well as in spain and italy . our perception is that the transposition process is recently started in europe . 
it is important that manufacturers specify the maximum uncertainty of dosimetric index . step 3 the third step is to transfer dosimetric parameter related to each radiological procedure to physicians report . 
 any diagnostic modality can provide exposure data in a different way : dose screen image ( fig.3 ) : a report produced by the device , containing exposure parameters ( kv , mas , etc . ) and a dosimetric index ( ctdi , dlp , dap , etc . ) if available ; image header dicom ( fig.4 ) : the file associated with image , containing metadata related to exposition ( for example , in a ct series it collects a cumulative dose information )  . 
data are stored in image header as attributes of standardized dicom tags . modality performed procedure step ( mpps ) ( fig.5 ) : a notification message sent from the modality to a dicom server in order to trace the procedures status . radiation dose structured report ( rdsr ) ( fig.6 ) : the document - like report able to collect both dosimetric and non - dosimetric ( geometry , patient name , patient id , etc . ) data for each exposure event . 
efomp also recommends that medical equipment used for interventional radiology equipment used for computed tomography not mandatory for equipment installed before february , 6 , 2018 new medical radiodiagnostic equipment producing ionizing radiation mandatory for all machines mandatory for all machines mandatory capability to transfer relevant not mandatory for equipment not mandatory for equipment mandatory installed before february 6 , 2018 installed before february 6 , 2018 table 5 extract summary of art.60 [ 1 ] feature requested a device or a feature informing of quantity of radiation produced by the equipment during the procedure a device or a feature informing at the end of the procedure , of relevant parameters for assessing the patient dose parameters for assessing patient dose to the record of the examination 1 3 la radiologia medica ( 2019 ) 124 : 783793 790 table 6 efomp recommended parameters for eu directive transposition of art.60 ( adapted from [ 32 ] ) modality metrics computed tomography dose index ctdivol [ mgy ] or ctdiw [ mgy ] indicating phantom size size - specific dose estimatesssde [ mgy ] dose length productdlp [ mgycm ] interventional radiology air kermaarea product kap [ gycm2 ] general fluoroscopy planar x - ray mammography cbct * dental radiography ( panoramic projection ) * * reference air kerma [ mgy ] air kermaarea product kap [ gycm2 ] air kermaarea product kap [ gycm2 ] entrance surface air kermaesak [ mgy ] incident air kermaiak [ mgy ] mean glandular dosemgd [ mgy ] air kermaarea product kap [ gycm2 ] * incident air kermaiak air kerma length product * metrics recommended by aifmsirm etal . 
3 an example of dose screen image , from ct modality conclusion the literal transposition of art.58 ( b ) indicates that patient exposure information and not patient dose information shall be added in radiological report . 
on the other hand , the mpe can estimate individual patient dose finalized to provide the radiological risk starting from machine parameters . anyway , in this review we considered four possible scenarios of art.58 ( b ) implementation : patient exposure data on the report . different organizations suggested the recommended machine parameters / exposure data for each radiological modality ; this information will provide a record for retrospective calculation of patient doses when needed . 
if requested by patient , mpe can assess the patient absorbed dose . patient absorbed dose on the report . in this scenario , the mpe should always be involved and , as responsible of patient dose estimation , he has to sign the radiological report . 
absorbed dose calculation is based on complex process that needs deep knowledge of software , phantoms and calculation models . effective dose and relative radiological risk index on the also allow : report . these values , expressed in units of millisievert ( msv ) , are based on effective doses and give a very approximate ment : assessment of radiological risk without taking into account patient specificity and then individual risk . 
in spite of this , we have to acknowledge that the use of relative radiological risk index is advantageous because it makes easy patient communication and understanding of risk : patients prefer symbols and scales to indicate risk [ 37 ]  . as stated and analyzed so far , the authors wish that italian implementation of art.58 ( b ) will provide exposure information on clinical report . the machine parameters are the most simple solution to implement art.58 ( b ) in radiological practice . 
they indeed , derived directly from equipment , are objective quantities that do not require further evaluation and may be easily transfer to physicians report , as described before in this paper . 
in order to assure accuracy and quality of these steps and to previously validate these data , a mpe has to be always involved . the use of appropriate optimized exam protocols for every type of medical radiological procedure is relevant to give meaningful patient exposure information . 
moreover , a team working among radiographers , physicians and medical physicists is desirable . dosimetric data entry on the radiological report will radiological individual risk estimates in terms of detri1 3 792 la radiologia medica ( 2019 ) 124 : 783793 a better implementation of art.64 eu 2013 / 59 regarding dose estimates of population from medical exposure , in terms of collective effective dose ; the dose management should be used as an optimization mean to decrease overall base dose ( from medical exposures ) ; an easier and more effective checking and review of diagnostic reference levels ( drl ) , in order to optimize radiological practice and then to support international audits as , for example , the eurosafe initiative promoted by european society of radiology [ 38 ]  . it is also important to highlight that dosimetric information included in patient radiological report will assume a legal value . 
the patient , indeed , could have one more tool for taking legal actions against the facility where he has been exposed ; in a future bad scenario , it would be possible that a patient undergoing to radiological examination uses his dosimetric information to compare doses from similar examinations executed in different facilities . 
that is why dosimetric information must be certified and it cannot disregard from a good optimization policy inside the radiology department . the national institution involved to drl collection should provide to a more frequently drl monitoring in order to make dosimetric data from medical exposures as uniform as possible in the majority of facilities . 
the european directive 2013 / 59 / euratom takes into account the new recommendations on reduction in the dose limit for the lens of the eye for planned occupational exposures released in 2012 by the international commission on radiological protection ( icrp 118 )  . materials and methods different dose - monitoring procedures and devices were considered . 
 the current status of eye lens radiation protection and the main methods for dose reduction were investigated . results the analysis showed that the workers , potentially exceeding the new limit , are clinical staff performing interventional procedures with a relatively high x - ray dose . 
regarding radiological protection issues , the considered literature reports that the proper use of personal protective equipment may reduce the eye lens absorbed dose . conclusion the evaluation of the occupational eye lens dose is essential to establish which method of personal dose monitoring should be preferred . 
furthermore , education and training about the right use of personal protective equipment are important for medical staff working with ionizing radiation . keywords eye lens dose radiation protection occupational dose dose limit dose reduction european directive 2013 / 59 introduction the new european directive 2013 / 59 / euratom ( eu 2013 / 59 ) introduces several changes to the protection of workers against the dangers arising from exposure to ionizing radiation [ 1 ]  . 
during these procedures , indeed , the upper body is not usually protected as trunk , which is systematically shielded by lead aprons . as a direct consequence of article 9 , eu 2013 / 59 article 40 updates the criterion for classification of workers by specifying that workers who are liable to receive an equivalent loe dose greater of 15msv / year shall be classified as category a . 
this more restrictive criterion , which equals the equivalent dose for public , is likely to result in an increase in workers classified in category a . a second aspect to be considered is the detection dose modality for individual monitoring of workers most at risk , likely to exceed the dose limit of 20msv / year for the eye lens . the aim of this article is to understand whether and how the new loe dose limit will affect the daily routine of clinical staff working with ionization radiation . 
we considered only x - ray exposures in interventional cardiology and radiology or surgery procedures using x - ray imaging such as ct - guided interventions [ 4 ] , fluoroscopically guided procedures , electrophysiology procedures , etc . 
the role of the radiation protection equipment in reducing the dose absorbed by the lens of the eye is also discussed . 2017 approved code of practice introduced a flexibility for 5 - year averaging for dose limit to lens of the eye , subject to conditions specified by hse [ 6 ]  . 
belgium , the netherlands , slovenia , and france actual legislation [ 7 ] provide the effective dose limit of 20msv each year rather than 20msv / year on average over 5years and mandatory personal dosimetry for category b workers . the new french decree on workers radiation protection [ 8 , 9 ] provides that the classification in category a is for exposed workers likely to receive an annual effective dose greater than 6msv or an equivalent dose greater than 150msv for skin and extremities ; the classification in category b is addressed to workers likely to exceed an effective dose of 1msv and an equivalent loe dose exceeding 15msv or 50msv for skin and extremities . 
in italy , current legislation has not transposed the new directive yet : italian exposed workers are included in category a if they are likely to overcome 6msv of effective dose for whole body , or equivalent dose of 45msv for eye lens or 150msv for extremities [ 10 ]  . 
with the new loe dose limit ( 20msv ) , an increase in classified a workers and the contextual decrease in classified b workers are expected . in other european union member states , the expressions category a and category b workers are often used . 
 the category a worker is equivalent to a classified worker , category b to a non - classified worker [ 11 ]  . materials andmethods lens dosemonitoring devices exposed workers classification we have already mentioned that lowering the loe dose limit will increase the number of workers classified in category a . 
it should be kept in mind that a non - negligible contribution to individual doses derives from radiation scattered from the patient . looking at international state of the art , the england transposition of eu 2013 / 59 , for example , reports that classified workers are those likely to receive an effective dose greater than 6msv / year or an equivalent loe dose greater than 15msv / year or an equivalent dose of 150msv for skin and extremities [ 5 ]  . 
regarding the risk of exceeding the loe dose limit of 20msv , the english radiation regulations for individual monitoring of occupational exposures to external radiation , the operational quantity recommended by icrp is the personal dose equivalent ( hp ( d ) ) whose unit of measure is the sievert ( sv ) [ 12 ]  . 
icrp proposed a depth of 3mm ( d = 3mm ) for the assessment of the loe dose because it corresponds to the depth at which the part of the eye sensitive to ionizing radiation is located . in the case of homogeneous irradiation conditions , it is also possible to obtain the hp ( 3 ) value from hp ( 0.07 ) and hp ( 10 ) quantities using appropriate correction factors [ 13 ]  . 
hp ( 3 ) values come from dosimeters positioned close to the eyes . among different technologies , thermoluminescent dosimeters ( tlds ) are the most used for medical workers monitoring . 
there are different types on market such as the eyed dosimeter ( fig.1a ) which can be worn on a narrow headband adjacent to the eye [ 14 ] , the dosiris dosimeter 1 3 730 la radiologia medica ( 2019 ) 124 : 728735 fig . 
in these devices , the stimulated light emission during the reading procedure is produced by a laser pulse rather than heat [ 17 ]  . tlds and oslds can only provide retrospective information ( passive dosimeters )  . 
 another example of active dosimeter is the doseaware system ( fig.2b ) [ 19 ]  . a more general approach to choose the appropriate dosimeter for workers is provided by the international atomic energy agency ( iaea ) and the international radiation protection association ( irpa ) [ 20 , 21 ]  . 
they divided exposed workers into three categories : those exposed to a relatively uniform whole - body radiation field for which the whole - body dosimeter will provide a good estimate of the loe dose ; those exposed to highly non - uniform radiation field in which the loe may be preferentially exposed . 
in this case , estimation of potential eye lens dose is this case is required ; those exposed to weakly penetrating radiation , such as beta particles or photons of low energies , significantly contributing to the loe dose but not to the effective dose . 
2 different active dosimeters : a the unfors edd 30 dosimeter [ 18 ] , b the doseaware system [ 19 ] dosemonitoring procedure the physical surveillance of people working with ionizing radiations , one of the issues ascribed on radiation protection experts ( rpe ) includes the pivotal theme of dose - monitoring procedures . before starting with individual regulatory monitoring , it is necessary to identify the workers most at risk of exceeding the eye lens dose limit for the population ( 15msv )  . according to the new directive art . 
besides , an adequate system for dose monitoring when [ ] category a workers are liable to receive significant internal exposure or significant exposure of the lens of the eye or extremities it is required . for an adequate system , it is intended a system able to measure a dose value as closer as possible to the one really absorbed by the tissue considered . it is therefore essential to establish what level of exposure should be considered significant and consequently to decide whether and which dosimeter to provide to the worker . irpa guidance on implementation of eye dose monitoring of workers [ 21 ] suggests dose - monitoring procedures based on potential absorbed doses . 
it considers hp ( 3 ) value and identifies two cases : ( 1 ) annual dose range from 1msv to 6msv and ( 2 ) annual dose exceeding 6msv . 
table 1 summarizes all the abovedescribed approaches . reduction inoccupational eye lens dose the new dose limit introduced in eu 2013 / 59 also requires a more careful evaluation of all possible solutions to reduce the loe dose . 
the main exposure source for an operator is the scattered radiation leaving the patient , so reducing the patient exposure will directly yield a lower exposure of the medical staff [ 24 ]  . factors contributing to eye lens dose include : the distance between operator and patient , the incident angle of radiation source , the position of the display unit , which determines the operators head orientation with regard to the scattered field , the type and position of the protection equipment . 
 ( university of glasgow ) 16 610 > 10 initial monitoring with collar or head dosimeter to establish dose levels regular monitoring is recommended regular monitoring with collar or head dosimeter is mandatory routine monitoring routine monitoring regular monitoring with collar dosimeter is recommended regular monitoring with head dosimeter is recommended regular monitoring with head dosimeter is required in interventional radiology , in order to optimize patients and workers radiation protection . regarding the occupational dose reduction in interventional cardiology procedures , a practical guide by european heart rhythm association ( ehra ) [ 24 ] described how each technical parameter can affect the dose for patients and staff ; this guide proposed practical ways to reduce radiation exposure . secondly , radiation protection devices ( shielding ) and personal protective equipment must be evaluated , based on exposure source parameters ( energy and position )  . eye lens exposure can be reduced by wearing protective eyewear with leadglass lens , adapted to face geometry . 
 it should be positioned as close as possible to patient and closer to image detector to decrease scattered radiation ; a dose reduction factor ( drf ) of 5 is typically applied for ceiling - suspended shields [ 26 ]  . 
in some situations , a lead protective cabinet protecting the operator can be recommended , thought it could physically obstruct the simultaneous presence of other protective devices . irpa proposes guidance on the use of protection device for the eye [ 21 ]  . 
it suggests the use of ceiling - suspended screens or protective eyewear when the annual unprotected dose is in the range from 3 to 6msv ; the use of both of them when annual unprotected dose exceeds 6msv . 
usually , the use of collective protection devices ( i.e. , ceilingsuspended shields ) is preferred to the use of personal protective equipment [ 27 ]  . a new device recently available on the market is a disposable radiation absorbing pad that results in a mean primary operator reduction dose of about 40% in interventional radiology [ 28 ]  . 
3 different ceiling - suspended eye shields 1 3 la radiologia medica ( 2019 ) 124 : 728735 protection topics to guarantee the effective employment of protective devices described above . table 3 equivalent eye lens doses per procedure ( sv ) for different categories of clinical staff adapted from [ 32 ] overview oftheestimated occupational equivalent dose the transposition of eu 2013 / 59 and consequently the possible adoption of the new loe dose limit put the attention on the current values absorbed by workers exposed to ionizing radiations . 
table2 shows a literature summary of occupational equivalent loe doses in interventional procedure [ 4 , 2933 ]  . the wide range of doses reported in table2 is mainly due to the presence of protective devices ( not always specified in the study ) as well as the different x - ray tube setting during procedures . 
the study of karolinska university hospital [ 34 ] highlighted the importance of the position of workers during interventional procedures in order to distinguish staff categories ( primary physician , scrub nurse and / or circulating nurse ) more at risk of exceeding the dose limit of 20msv / year . 
as predictable , primary physicians resulted the most exposed workers [ more details in table3 ] ; radiologists and cardiologist have the highest occupational equivalent eye dose . interventional procedures radiology ( sv ) cardiology ( sv ) neuroradiology ( sv ) primary physician scrub nurse circulating nurse results anddiscussion the analyzed studies demonstrate that exposed workers involved in interventional procedures using x - rays could potentially exceed the eye lens equivalent dose of 20msv / year if a radiation protection environment is not properly structured . 
the reported loe occupational doses are not homogeneous because they are not always normalized per time exposure and the work pattern is not indicated , so these studies cannot be considered as representative of state of the art . the retrospective assessment of occupational eye lens dose could be conducted throughout chest or neck dose measurements from personal dosimeter [ 29 , 31 , 34 ]  . as far as occupational eye lens dose reduction is concerned , the three well - known factors time , distance and shielding must be kept in mind . 
besides , optimizing the patient exposure , directly related to the worker exposure , is essential . among protection devices mentioned , ceiling - suspended systems provide the highest drf , and their use is more functional than glasses . 
 ( 2017 ) not specified ceiling - suspended screen osl on glasses hp ( 3 ) no eyewear edd30 near the left eye active dosimeter clipped onto eyewear sciahbasi a . 
 ( 2017 ) a ct - guided interventions mobile leaded glass suspended from the ceiling hp ( 3 ) uncorrected use of shields tld hp ( 3 ) category average dose / procedure ( sv ) interventional radiologya interventional cardiology neuroangiography interventional radiology and cardiology interventional cardiology interventional cardiology ~ 169 ~ 34 ~ 114 1 3 734 study table 4 the maximum procedures number ( mpn ) calculated for each study average dose / procedure ( sv ) vano e . 
 ( 2017 ) ~ 169 ~ 34 ~ 114 ~ 118 ~ 589 ~ 175 radio - induced cataract is not a stochastic effect with a probability of occurring related to absorbed dose , but it is a tissue reaction related to a threshold value . 
thus , the optimization process has to be balanced on potential exceeding of eye lens dose limit of 20msv . in order to prevent the exposed workers to exceed the dose limit , we suggest to previously estimate the maximum number of procedures ( mpn ) that each worker should perform and to consider the type and the duration of these procedures . 
the estimates of mpn should be performed in each interventional radiology facility , based on averaged equivalent eye lens dose values per procedure obtained from individual monitoring and for each category ( primary physician , scrub nurse , and circulating nurse )  . 
similarly , each procedure should be performed according to a pre - established written protocol . regarding workers classification and dose limits , all countries that have already transposed the new directive , confirmed the loe dose limit of 20msv / year . 
some member states does not distinguish exposed workers in two categories : england is an example of this , and it defines an equivalent loe dose greater than 15msv / year as exposed workers classification criterion . conclusion the new loe dose limit ( 20msv / year ) and the new threshold value for the equivalent loe dose for exposed workers a ( 15msv / year ) suggested by the european directive 2013 / 59 / euratom are significantly lower than the previous ones ( 150msv / year and 45msv / year )  . 
strategies for la radiologia medica ( 2019 ) 124 : 728735 effective reduction , protection , monitoring , and dosimetry must be implemented . the first topic to address is classification of workers : many workers , currently classified as category b , could be classified as category a because possibly exceeding the new limit value of 15msv / year , the same of population limit . 
consequently , the number of workers belonging to category a and then management costs could increase . in this regard , a monitoring loe dose campaign could be necessary for each exposed worker ; a first retrospective assessment could be done from whole body dosimeters placed above lead apron . 
whole - body personal dosimeter for workers belonging to category b is recommended for a transition period . for regulatory monitoring , a personal eye - dedicated dosimeter is recommended and the best solution is an active dosimeter providing real - time information about radiation exposures as well as alarms at for particular dose levels . optimization of procedures ( e.g. , source and operator position , beam collimation , exposure time , etc . ) and of workloads ( in terms of number of procedures performed by each operator ) is a relevant aspect for the reduction in the absorbed loe dose . 
an adequate distribution of workloads , using the mpn calculation , could prevent the removal of that exposed workers who are most at risk of exceeding the loe dose limit . education and training on the effective and appropriate use of collective and personal protection equipment are essential elements to achieve good protection and acceptableeyelens doses . the results reported in this paper show that loe doses can be significantly reduced if lead glasses and ceiling mounted shields are properly used . 
a close cooperation and collaboration across all the physicians responsible for patient care in requiring imaging examination is also important , balancing possible ionizing radiation disadvantages and patient benefits in terms of care . keywords overimaging overdiagnosis ethics radiation protection * sergio salerno sergio.salerno@unipa.it 1 department ofdiagnostic radiology , university ofpalermo , policlinico via del vespro 127 , 90127palermo , italy 2 department ofsurgical andmedical sciences andtranslational medicine , santandrea university hospital , sapienza - university ofrome , via di grottarossa 1035 , 00189rome , italy 3 department ofbiomedical , surgical anddental sciences , university ofmilan , via pascal 36 , 20133milan , italy 4 department ofradiology , ss giovanni e paolo hospital , castello 6777 , 30122venice , italy 5 department ofradiology , cto hospital , azienda ospedaliera dei colli , naples , italy 6 department ofdiagnostic radiology , hopital europen georges pompidou paris aphp , universit paris - descartes , paris , france introduction the field of biomedical imaging , in particular the area of radiology , has expanded intensely over the last decade . 
the contemporary role of the radiologist is being challenged as the use of images by clinicians is continuously increasing . the development of medical imaging over the past two decades has produced undisputable benefits to patients in terms of life expectancy and quality of life [ 1 ]  . 
this evolution reflects the utilization of complex ionizing and nonionizing radiation technologies such as multidetector computed tomography ( mdct ) , positron emission tomography ( pet ) , and magnetic resonance imaging ( mri )  . 
part of such growth , however , can be attributed to the overuse of imaging services . overuse can be defined as the application of imaging procedures where conditions clearly show that they are unlikely to increase the patient outcome . key factors influencing imaging overuse include : the practice behaviour of referring physicians , self - referral ( including referral for additional radiological examinations ) , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 714720 duplicate imaging studies , defensive medicine , missed educational opportunities when inappropriate procedures are requested , patient demand , payment mechanisms , and financial incentives ( as in the us healthcare system ) [ 2 ]  . self - referral was known since 1920s , well before the advent of high technology in radiology , but observers generally agree its volume has increased in the last 2030years [ 3 ]  . 
self - referral can be manifested in two main ways forms : a physician who is not an imaging specialist ( or a non - physician provider ) referring patients to his or her own on - site imaging services represents the first form of self - referral ; the second form of self - referral consists of physicians referring their patients to outside facilities in which they has personal a financial interest . 
self - referral denotes a conflict of interest for the referring physician when the financial profit from conducting the procedure may prevail , the medical necessity of the procedure . defensive medicine has been defined as diagnostic or therapeutic actions applied mainly to safeguard against potential claims of malpractice rather than to benefit the patient . 
too often these studies are expensive and provide doubtful benefits to individuals undergoing the moreover , physicians should encourage patients to report imaging examinations they have undergone previously in order to avoid duplicate studies . 
 duplicate studies contribute to overuse of medical imaging [ 6 ]  . recent research shows that approximately one - third of healthcare spending is duplicative , is unhelpful , or makes patients worse [ 7 ]  . 
unnecessary imaging studies rarely reveal the cause of patients complaint , yet may disclose incidental findings , which necessitate further imaging or interventional procedures to be clarified [ 8 ]  . 
therefore , imaging information must not be considered absolute , but rather must be understood inside a specific clinical context including the patient history , previous radiological examinations , and other clinical data to form a combined picture that reasonably either confirms or excludes a given diagnosis [ 9 ]  . because of the possible selfinterest by policy makers , payers , physicians , imaging industry , and patients , it clearly emerges the ethical imperatives of trust and right conduct . 
it is clear that a serious part of the increasing healthcare costs and fragmentation of medical care resides in cooperation and collaboration across many sectors , including radiologists , industry , referring clinicians , healthcare service payers , and public interest groups . the bioethical principle of distributive justice holds that healthcare resources should be distributed as equitably as possible . 
given finite resources for health services , it is unethical to provide expensive non - essential health services to one sector of the society when another sector lacks of essential services [ 11 ]  . 
despite persistent inequity in the distribution of healthcare resources in the usa , we should ask about new medical interventions , does this test or treatment undermine the fair distribution of health resources ? given the importance of this subject and the magnitude of its potential economic impact , it is important to restore objectivity . speaking more in deep about radiological protection , we daily deal not only with useless or inappropriate examinations , but with imaging modalities which may themselves lead to detrimental effects on patients , especially when using contrast media administration and radiation exposure . 
with respect to other planned exposure situations , the justification lies more often with the profession , rather than with government or regulatory authorities , and the final responsibility for the justification , in the use of a particular procedure , lies with the relevant physician , who should be aware of risks and benefits of the involved procedures [ 12 , 13 ]  . 
in case of radiological examinations exceeding the needs of good medical practice , the only result may be an 1 3 716 la radiologia medica ( 2019 ) 124 : 714720 unjustifiable possible risk for patients , not providing any real benefit , with the result of inconvenience application of the main principles of radiological protection and medical ethics [ 14 ]  . 
the potential risks and the uncertainties regarding the risk associated with radiation exposures have a significant role in the decision to undertake a procedure , and also the complexity , in communicating the risk , has to be taken into consideration . 
in fact , informed consent is more than simply getting a patient to sign a written consent form , it is a communication process , which requires additional time for a real and comprehensive informed consent , and this is also related to the critical question of having the proper time to dedicate to the individual patients . 
value judgements on appropriateness of a procedure require knowledge on the implications of the act and about the ethical and societal values on which to base the decisions for that act . 
the system of radiological protection developed by the international commission on radiological protection ( icrp ) has evolved and continues to evolve on the basis of three recognized pillars : science of radiological protection , a set of ethical values , and experience accumulated from the daily practice of radiological protection by professionals [ 15 , 16 ]  . 
it is evident that quantifying benefits and harms is often problematic and the threshold between an appropriate and an inappropriate act can vary among patients and patient groups [ 17 ]  . 
it is also evident that ethics alone cannot offer a definitive solution to questions and dilemmas , but it can certainly provide useful insights into the principles and philosophy of radiological protection . 
in such way , it can be of help in the dialogue among experts , and among experts , patients , and people , to highlight values and preferences in view of a positive balance between potential benefits and harms . regarding the ethical dimension of radiological protection , it is worthwhile to mention the contribution by giovanni silini , who reviewed the ethical foundation of the radiological protection system in his sievert lecture , in 1992 [ 18 ] , by emphasizing that the system has been rationally developed and , at the same time , with the desire to act reasonably . 
in radiological protection , the core ethical values , as addressed in the recent icrp publication on ethical foundations of the system of radiological protection [ 15 ] , support the aims of the radiological protection system and its three fundamental principles : justification , optimization , and individual dose limitation . 
 as well known , the origin of medical ethics lies with hippocratic oath and more recent with the approach by beauchamp and childress [ 19 , 20 ] given through the four principles of biomedical ethics : autonomy , the right of patients to make their own choice ; beneficence , to act taking in mind the best interest for the patient ; non - maleficence , to consider not to harm ; justice , to be fair . 
the core ethical values recognized in the system of radiological protection are clearly consistent with the principles of biomedical ethics , when considering beneficence and non - maleficence in one single concept ; the autonomy replaced by dignity ; and the addition of prudence . overimaging as applications of imaging procedures where circumstances indicate that they are unlikely to provide additional positive outcomes for the patient may increase the average dose to the population resulting from medical exposures . 
given the moral obligation of healthcare providers , first , do not harm , the ethical indication is to lower the risk , with benefit outweighing the risk , by considering procedures appropriately prescribed and appropriately performed ( justification and optimization ) [ 21 ]  . 
at the same time , there is an ethical relevance related to benefit to the society , which is not achieved and quite disregarded , if an unbalance between health outcome and corresponding costs is created [ 2224 ]  . supply and demand are considered the main mechanisms at the base of overimaging . 
expanded availability of technological medical procedures and increased demand from patients / individuals , together with referring clinicians for assurance , can create the feeling and perception of imaging as a mean to comfort patients and clinicians , where the benefits may easily be overestimated , while risks and costs are somewhat neglected [ 25 ]  . 
individual health assessment which is addressed in the last european directive on radiation protection ( bss ) could also play a role in increasing unnecessary examinations . the obligation to benefit the patient must be balanced against the obligation not to cause harm , with the purpose of ensuring that benefits will outweigh , harms ( beneficence , non - maleficence ) [ 26 ] and the attention to these ethical values may become a difficult task if the risks are uncertain , as for the low doses . 
overestimation of risks might result in not performing an imaging procedure that could be of benefit and underestimation of risk might result in an increase in risk for patient and society without any advantage for the patient [ 27 , 28 ]  . 
prudence should not be taken as synonymous of conservatism or never taking risk , but it defines and sustains the way in which decisions are made , and it does not refer only to the outcome of those decisions . 
we can say that prudence represents the ability to take an informed and well - considered decision under uncertainty , without having a full knowledge of the consequences of the undertaken action . 
a proper imaging examination , at the right time , with attention to justification and optimization , 1 3 la radiologia medica ( 2019 ) 124 : 714720 can have significant value for the patient and the society , while overutilization of imaging brings inappropriate use of resources that could be used for other medical purposes , thus violating the justice in the distribution of advantages and disadvantages . 
justice relates our sense of fairness , and we can say that considering radiation risk a particular attention has to be given to avoid overimaging children in view of their higher risk of adverse effects of radiation , compared with adult [ 28 ]  . this is particularly true when considering the exponential increase in radiological examinations during the last decades , and the consequent increased number of imaging findings which are not related to the original diagnostic dilemma . 
indeed , market research studies have shown that in the usa the number of computed tomography ( ct ) examinations increased from 3 million / year in 1980 to 6 million / year in 2006 ; the actual estimated increased rate is between 8 and 10% / year [ 2931 ]  . it also results from the medicare program ( reimbursing diagnostic imaging services in the usa ) that during this period ct scans of the abdomen tripled and those of the thorax quintupled . 
furthermore , the number of magnetic resonance imaging ( mri ) studies is constantly increasing , with brain examinations rising by fourfold , spinal examinations by sixfold , and knee examinations by tenfold [ 32 ]  . 
a recent study reported that in these tests , in 68% of the cases , abnormalities causing no symptoms , called incidentalomas , were detected [ 32 , 33 ]  . 
of course , a finding in a non - symptomatic patient causes negative psychological effects on the patient . in this regard , for example , it is reported that the risk of death for a liver biopsy performed for the purpose of investigating an incidentaloma ( from about 12 per 1000 to 4 ) is of the same order of magnitude as the probability that incidentaloma is a deadly tumour [ 35 ]  . also , in the field of ct , an important aspect concerns the detection of anomalies affecting venous circulation and their possible consequences at the pulmonary level . 
in fact , the prevalence of pulmonary embolism is significantly influenced by the diagnostic tests performed , while from a clinical point of view , few patients with venous thrombosis of the lower limbs have respiratory disorders [ 36 ]  . currently in most cases , nuclear medicine was replaced by the spiral ct . 
this investigation , in patients with thrombosis of the peripheral veins of the lower limbs , identifies 34% more patients with micro pulmonary embolisms compared to the nuclear medicine test [ 37 ]  . 
therefore , although ct increases the micropulmonary embolisms detection rate [ 38 ] , it also entails the risk of contrast media injection , radiation exposure , and increased costs [ 39 ]  . ultrasound investigations can also be a source of overdiagnosis . 
occasional finding of thyroid nodules almost always leads to the request of at least one subsequent follow - up test , if not directly to the direct execution of a fine needle aspiration . 
the diffusion of transrectal ultrasound ( trus ) and trus - guided biopsy has led to a clear increase in the diagnosis , without , however , significant effects on reduction in mortality rate . 
one study showed that performing six samples in symptomatic patients , no neoplasm was found , but referring the same patients to saturation biopsy with 3238 samples , prostate cancer was detected in 14% [ 42 ]  . the american cancer society has recently stated that prostate cancer has a slow growth and no tests should be done in men who have a life expectancy of less than 10years . 
a recent us study even states that screening programs would increase prostate cancer mortality by 13% , as a result of post - surgical and therapeutic complications in patients who would otherwise have not undergone any treatment [ 43 ]  . professor albin , the discoverer of the psa , recently published in the new york times an article entitled the great error of the prostate stating that unfortunately psa test fails to distinguish between two types of prostate cancer : the one that can develop up to be mortal and the other one which remains silent [ 44 ]  . 
ulterior source of overdiagnosis is mr examinations , especially of the musculoskeletal syste approximately 40% of people undergoing mri of the knee , despite being substantially asymptomatic , may have meniscal injuries [ 45 , 46 ]  . 
approximately 50% of people undergoing mri of the lumbar spine , although without significant symptoms in the back , may have disc protrusions [ 47 ]  . the matter of the costs of overdiagnosis is then strongly correlated with that of inappropriateness . 
in italy , a sector study has shown a rate of inappropriateness in outpatient radiology requests of 44% [ 48 ]  . the chairman of the italian society of medical and interventional radiology ( sirm ) , in a recent article , confirmed that in the country one - third of the radiological investigations performed is inappropriate [ 49 ]  . 
calculating that in italy about 100 million radiological examinations per year 1 3 718 la radiologia medica ( 2019 ) 124 : 714720 are performed and that the average cost of radiological services , taking into account the various types , is about 80 , it is likely to estimate the economic value of the inappropriate tests in about 3 billion eur / year . but now , we must consider the most human and important factor of overdiagnosis and overusing of medical radiological examinations : the inappropriate and potentially useless radiation exposure of the population , without any improvement of cost / benefit ratio . the overuse of medical imaging , when involves methods delivering ionizing radiation , increases the radiation exposure and thus the associated risks such as cancer induction [ 50 , 51 ]  . 
in particular , overdiagnosis is associated with ductal carcinoma insitu , a rare tumour ( less than 5% of the annual incidence of breast cancers ) which progresses to invasive disease in a wide time frame ranging between 5 and 15years according to the grade . 
it has been evaluated that the mean glandular dose for screening mammography ranges between 3 and 10mgy and it is mainly influenced by the number of views acquired , the technology used and by patient - related factors [ 57 , 58 ]  . 
 in this setting , the number of false positive is also crucial since it has been demonstrated that 9.251% of positive controls at the first round turns to be a false positive which become 21% at the second round and 33% at the third round determining 2.3% of minor and 2.73% of major invasive procedures [ 63 , 64 ]  . 
since the effect of screening on lung cancer mortality has been estimated to be about 5% , the risk of radiation - induced cancer can be considered acceptable [ 60 , 62 , 66 ]  . the last major setting where overdiagnosis increases overuse and thus radiation exposure is the field of emergency . 
in particular , the use of computed tomography has increased fourfold in the last 10years for any clinical condition such as trauma , pulmonary infections , abdominal pain , and pulmonary embolism [ 53 , 68 ]  . 
the indiscriminate use of computed tomography determines an increase in incidental findings leading to a costly and potentially harmful diagnostic , therapeutic , or interventional cascade [ 68 ]  . 
in a recent survey , over 85% of emergency physicians interviewed felt that 22% of advanced imaging studies ordered were not clinically justified . conclusion while the radiation exposure risks related to screening imaging seem justified by the benefit of a greater mortality reduction , despite the negative influence of not negligible overdiagnosis , in the setting of emergency imaging this phenomenon as well as overuse negatively influences the radiation exposure of patients without the compensation of clinical benefits . in practice , searching for reasonableness and tolerability is a permanent effort directed to act wisely , based on accumulated knowledge , ethical values , and experiences . 
a single - source 64 - mdct ( lightspeed vct , ge ) scan was performed in 705 patients from january to august 2017 ( 207 coronary examinations and 498 vascular examinations ) and 753 patients underwent thirdgeneration 192 2 - dsct ( somatom force , siemens ) scan from january to august 2018 ( 302 coronary examinations and 451 vascular examinations )  . 
volume ct dose index ( ctdivol ) , dose length product ( dlp ) , effective dose ( ed ) , tube voltage ( tv ) and exposure time ( et ) , pitch factor ( pf ) were registered for each patient . 
 cta has been widely used in the diagnostic evaluation of many vascular diseases , and serves as first - line modality in the early diagnosis of abdominal aortic aneurysm or aortic dissection and to follow - up patients treated with endovascular stents and stent grafts , with the aim of determining their patency or potential complications [ 310 ]  . 
 indeed , an effective dose of 5msv adds only a small , negligible additional risk to lifetime cancer risk , but the diagnostic information and the clinical consequences resulting from a coronary cta may outweigh this very small theoretical additional cancer risk [ 24 ]  . related to this , the introduction of dual - source ct ( dsct ) scanners provided a series of improvements , such as fast gantry rotation speed ( from 280 to 250ms ) , increased longitudinal detector coverage ( from 38mm for 128 - slice dsct to 58mm for 192 - slice dsct ) and more powerful roentgen tube . 
this causes reduced gantry rotation time and high - pitch values , which combined with the possibility to reach higher mas and consequently to reduce kv , should improve image quality and reduce radiation dose , compared with the other ct scanner . 
moreover , the dcst scanners equipped of two x - ray sources at 95 to each other [ 25 ] provided a new scan protocol , defined turboflash ( tfp ) , suitable for patient with regular heart rate lower than 65 beats per minute ( bpm ) that allows minimal radiation exposure and concurrent reduction in any motion artifacts from moving structures , such as heart , valves or pulsating aortic root [ 2631 ]  . 
exclusion criteria were : groups of cv type examinations with size smaller than 30 patients in 64 - mdct or in dsct ( superior limbs artery examination , n = 2 with ssct and n = 15 with dsct ; coronary examinations performed with pp in 64 - mdct n = 7 )  . 
we chose to collect patients from the same period of two different years to obtain two cohorts as homogenous as possible . the final population was made up of 1458 patients . 
a 20 - gauge cannula was inserted into superficial vein of the right antecubital fossa , connected to a two - way injector : one with contrast medium ( cm ) ( iopamidol , 370mg i / ml , bracco ) and the other with saline solution . 64mdct ( lightspeed vct , ge ) coronary protocol retrospective ecg trigger was used . 
cm volume was weight - based ( 1.5 ml / kg ) with flow rate of 5 ml / s followed by 50ml of saline solution at the same flow rate . 
scan started , automatically , 10 s after that a region of interest ( roi ) enhancement reached 150 hounsfield unit ( hu )  . table2 summarized scan parameters for cv protocols with 64 - mdct . 192 2dsct ( somatom force , siemens ) coronary protocol ecg - triggered scan was performed with tfp in patients with rhythmic heart rate lesser than 65bpm , with pp in patients with rhythmic heart rate between 66 and 80bpm and with rp in patients with heart rate greater than 80bpm or in case of arrhythmia . bolus test technique was used : 4ml of cm at flow rate of 5ml / s followed by 35ml of saline solution at the same flow rate was used to evaluate peak time ( pt ) in ascending aorta . 
scan started , automatically , 6s after that roi enhancement reached 250 hounsfield unit ( hu )  . table3 summarized scan parameters for cv protocols with 192 2 - dsct . radiation dose volume ct dose index ( ctdivol ) and dose length product ( dlp ) were registered for each patient . 
effective dose ( ed ) , an useful parameter to optimize rd , was calculated by multiplying dlp value by k factor ( k = 0.014 for thoracic examinations and k = 0.015 for abdominal or thoracicabdominal examinations ) , according to guidelines from the american association of physicists in medicine [ 35 ]  . 
for all comparisons , p value less than 0.05 was considered statistically significant . results coronary study : radiation dose andscanning parameters in table4 are summarized and compared ctdivol , dlp , ed , tv , et and pf between dsct and mdct with rp . 
figure1 compares ed between mdct and dsct in each coronary protocol . vascular study : radiation dose andscanning parameters in table5 are summarized and compared ctdivol , dlp , ed , kvp , et and pf between tfp , pp and rp in dsct . 
in all three protocols , mean tv was between 80 and 90kv , but it was significantly lower with pp compared to tfp and rp , which instead showed the greater tv ( 87.8kv ) ; this can partly justify the higher dose delivered compared with the other protocols . 
in fact , the most relevant difference between the three protocols is related with et , significantly lower in rp compared , respectively , with pp ( 60.0% ) and rp ( 74.8% ) , which conceivably has to be considered the largest cause of radiation dose reduction . concerning vascular examinations , the greater radiation dose reduction , with dsct , was found in inferior limb artery study , with 73.1% dlp and ed decrease . 
in particular , the greatest et reduction occurred in thoracic aorta examinations where at the same time , there was the greater pf increase , compared with the other vascular examinations . 
on the contrary , due to the need of leaving time to contrast media to arrive at limb extremities , the lowest et reduction was found in the examinations of lower limb arteries associated with the smaller pf increase , compared to the other vascular exam types . 
another remarkable aspect to underline is that in thoracic aorta and thoracicabdominal aorta , et and kv were significantly lower with dsct than with 64 - mdct , because the prospective ecg triggering sometimes used in the latter one was very burdensome in terms of radiation exposure , due to smaller tube coverage and lower pf , which results in higher et . to the best of our knowledge , no work has compared radiation dose and scanning parameters between 192dstc and 64 - ssct . 
however , they used 70kv for all examinations and disabled ecg - controlled tube current modulation , as a standard protocol , instead of our experience in which we prefer to use an automatic modulation of tube voltage ( care kv , siemens , medical solution ) and tube current ( care dose 4d , siemens )  . 
first , the study is based on a historical comparison , with no guarantee that the populations are entirely comparable , even if patients were selected from the database of the same hospital . 
intra - individual comparisons with repeated examinations using different protocols would strengthen our claims , but this is not possible for obvious ethical reasons . in conclusion , in cv examinations , ctdi , dlp and ed considerably decrease with 192 - dsct in comparison with conventional 64 - mdct , and we can hypothesize that the reduction is mainly associated with higher pf and tv used . funding this research did not receive any specific grant from funding agencies in the public , commercial or not - for - profit sectors . 1 3 760 la radiologia medica ( 2019 ) 124 : 753761 compliance with ethical standards conflict of interest the authors declared no potential conflict of interest associated with this study . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 711713 editorial editorial fromguest editors current euratom legislation ( de 59 / 2013 ) : new patient management inradiation protection giuseppeguglielmi1 antoniopinto2 sergiosalerno3 received : 29 may 2019 / accepted : 6 august 2019 / published online : 29 august 2019 italian society of medical radiology 2019 keywords euratom legislation radiation protection radiation dose it is our great pleasure to introduce this issue of la radiologia medica focussed in the current euratom legislation on radiation protection . 
 furthermore , the new european directive replacing and integrating in some cases the previous directives 89 / 618 / euratom , 90 / 641 / euratom , 96 / 29 / euratom , 97 / 43 / euratom and 2003 / 122 / euratom , is expected to have a significant and constructive impact on european radiodiagnostic and radiotherapeutic procedures . 
one of the main goals of the directive , born based on the continuous increase of radiation exposure of general population for medical reason , is the information and communication to the patients . 
new scientific data on tissue reactions call for the optimization principle to be applied to equivalent doses as well , where appropriate , in order to keep doses as low as reasonably achievable , alara principle . 
this new directive should also follow new international commission on radiation protection ( icrp ) guidance on the limit for equivalent dose for the lens of the eye in occupational exposure . 
it should be noted also that according to the world health organization the concept of health is understood to cover the physical , mental and social well - being of an individual and not merely the absence of disease or infirmity . in the opening article , salerno etal . 
 [ 2 ] analysed the key factors that influence imaging overuse with x - ray such as self - referral , defensive medicine ( diagnostic or therapeutic actions applied mainly to safeguard against potential claims of malpractice rather than to benefit the patient ) and duplicate imaging studies . 
 [ 3 ] described the wide spectrum of changes introduced by council directive 2013 / 59 / euratorelevant changes include new definitions , a new dose limit for the eye lens , non - medical imaging exposures , procedures in asymptomatic individuals , the use and regular review of diagnostic reference levels ( including interventional procedures ) , dosimetric information in imaging systems and its transfer to the examination report , new requirements on responsibilities , the registry and analysis of accidental or unintended exposure and population dose evaluation . 
 [ 7 ] compared radiation exposure associated with daily practice cardiovascular examinations performed on two different multidetector computed tomography ( mdct ) scanners : a conventional 64 - mdct and a third - generation dual - source ( ds ) mdct . 
 [ 8 ] analysed the main human factors that may increase patient dose as inaccurate scan over - length and patients positioning in ct colonography ( ctc ) and their effect in radiation exposure : radiographers and radiologists need to be aware of dose variation and noise effects on vertical positioning and over - scanning . 
 [ 10 ] described several contemporary and emerging concerns related to radioprotection in radiation therapy , including quality and safety in external beam radiotherapy and brachytherapy , foetal dose , secondary malignancies and the safety issues related to the new techniques and treatment strategies . in the last closing article , cornacchia etal . 
 [ 11 ] reported the information regarding patient exposure to ionizing radiations in the radiological report , according to the european directive 2013 / 59 / euratom ( eu 2013 / 59 art.58 ( b ) ) : for such purpose , results from other member states eu 2013 / 59 transpositions and from guidelines recommendation published by international organizations involved in diagnostic radiology have been evaluated . 
each of these two groups were further divided in two age groups ( or > 10years old ) including patients scanned in the same period of two consecutive years , in 2017 with a 16 - row lightspeed ct ( ge healthcare ) or in 2018 with a somatom force dsct ( siemens healthineers )  . 
in low - dose chest ct , the frequent use of tin filter required higher tube current ; a total dlp 3 times lower was achieved with dsct in patients 10years old . 
the growing number of pediatric ct examinations and radiation exposure raised the concern of a hypothetical increased risk of radiation - induced cancer in adult age [ 24 ]  . 
even though these evidences still need to be fully understood and validated , they had a major impact on global media and a positive influence on scientific research [ 5 ]  . recent technological advances in mdct for pediatric applications focused on dose reduction and faster acquisition for reduction in artifacts in children [ 6 , 7 ]  . 
in particular , the dual - source ct technology ( dsct ) , conceived for cardiovascular imaging , is equipped with two independent x - ray tubedetector systems ( somatom definition , flash and force , siemens healthineers , forchheim , germany ) [ 8 ]  . 
when the tubes work at the same voltage ( kvp ) , an extremely fast acquisition with low rotation times and high pitch is feasible ; vol . : ( 0123456789 ) 1 3 746 la radiologia medica ( 2019 ) 124 : 745752 this is worthy in pediatric population reducing the need of sedation [ 9 ]  . 
the obtained virtual non - contrast images may represent an acceptable solution for avoiding the pre - contrast acquisition with considerable dose reduction [ 12 ]  . going beyond the dect and ultrafast acquisitions already mentioned , several technological solutions contribute to significant dose reduction . 
on the opposite side , the implementation of efficient detector technologies and iterative reconstructions also cooperates to noise and then dose reduction resulting in better image quality [ 1719 ]  . the new - generation ct scanners , with dual - energy technology , efficient dose reduction and ultrafast acquisitions , will realistically expand pediatric ct applications with diagnostic advantages and good image quality . in the present study , we will provide an overview in terms of dose reduction and image quality in a pediatric population after installation of a third - generation dsct in our department . 
examination protocols from two different scanners ( a single - source ct , ssct and dsct ) will be compared in the same period of two consecutive years . materials andmethods inclusion criteria andpatient population we included pediatric patients ( < 20years old ) who underwent to ct examinations at division of special and pediatric radiology of university hospital ospedali riuniti umberto i - gm lancisi - g salesi . 
we included patients scanned in the first 7months of 2017 ( for ssct ) or in the first 7months of 2018 ( for dsct )  . the exam protocols included were studies of neck , thorax and abdomen in oncological patients , dividing the patient population in two groups group a ( 010years old ) and group b ( 1120years old )  . 
pediatric patients undergoing low - dose chest ct for lung diseases ( lung malformations , pneumonia and cystic fibrosis ) were also divided in group c ( 010years old ) and group d ( 1120years old )  . 
emergency ct , neuroradiological and musculoskeletal ct examinations were excluded . image acquisition in the first 7months of 2017 , all pediatric patients were scanned with a ssct , a 16 - row lightspeed scanner ( ge healthcare , milwaukee , wi )  . 
patients less than 6years old required sedation . after installation of a third - generation dsct in january 2018 , oncological and thoracic examinations in pediatric patients were performed with a somatom force ( siemens healthineers , forchheim , germany ) when possible . 
the somatom force scanner is equipped with two tubes delivering high power at voltages between 70kv and 150kv in steps of 10kv with automatic modulation of kv and ma , tin filters for spectral shaping and with high - efficiency stellar detectors ( siemens healthineers , forchheim , germany )  . 
the low - dose chest protocols included highpitch ultrafast acquisitions ( turboflash , siemens healthineers , forchheim , germany ) , dual - energy acquisitions and spectral shaping with tin filter , tailored on patients age and body weight . 
 protocols with dsct did not require sedation . data retrieval data were acquired by a radiation dose index monitoring ( rdim ) system ( dosewatch , ge healthcare , buc , france ) , collecting all the information present on the dicom header and on the dicom radiation dose structured report ( rdsr ) , in order to get information on the whole exam and on the singles scans . patients age , body mass index ( bmi ) , kvp , x - ray tube current per rotation ( mas ) , total exposure time ( ms ) , slice thickness ( st ) and spacing ( sp ) , number of series ( excluding localizers , bolus tracking or bolus test ) and the number of images per series were retrieved . 
when dect was performed , the low kvp was reported ; the high kvp was always 150 sn kv . regarding the dose parameters , we extracted the mean ctdivol ( mgy ) , the total dlp ( mgy * cm ) and the calculated ssde ( mgy ; dosewatch , ge healthcare , buc , france )  . 1 3 la radiologia medica ( 2019 ) 124 : 745752 image quality , data analysis andstatistics image quality , technical parameters anddoses the image quality was evaluated in consensus by two radiologists ( cl , aa ) in consensus on a semiquantitative fivepoint scale as follows : 1 . 
statistical analysis was performed with medcalc v12.5 ( ostend , belgium )  . results patient population table1 summarizes the patient demographics of each group of the population included in the study . 
dect dual - energy ct , hp ultrafast acquisition at high pitch ( siemens healthineers ) , ssh spectral shaping with tin filter 1 3 748 la radiologia medica ( 2019 ) 124 : 745752 1 3 la radiologia medica ( 2019 ) 124 : 745752 1 3 750 la radiologia medica ( 2019 ) 124 : 745752 fig . 
80 kvp ; pitch 0.9375 ; slice thickness 2.5 mm ; kernel standard ; asir 50% ; ctdivol 6.147.56 mgy ; total dlp : 320.29 mgy * c dg follow - up with dsct ( somatom force , siemens healthineers ) and dual - energy acquisition . 
the image quality was significantly higher with the dsct . discussion the therapeutic successes in the managements of clinical conditions such as infantile cancers or lung diseases lead to a significant improvement of the survival of these patients with long follow - up periods of pathologies and their complications [ 1 , 20 ]  . 
the longer survival has led to an increase in ct examinations in pediatric patients with concerns about potential risks in terms of induced cancers after radiation exposure [ 24 ]  . 
the debate on benefits and potential harms of ct in pediatric patients pushed the scientific progress ; fast acquisitions matched with dose reduction strategies are of great value in this setting [ 5 ]  . in our study , we provided an overview in terms of image quality and dose reduction in pediatric patients in two different settings : oncological staging and low - dose chest ct . 
however , considering the same period of the year , a lower number of patients have been evaluated on dsct within groups a , b ( the oncological patients ) and c ( patients with lung diseases , less than 10 years old )  . 
it has to be explicated that the pediatric department , the pediatric oncology and the ssct scanner 1 3 la radiologia medica ( 2019 ) 124 : 745752 ( lightspeed 16 , ge healthcare ) on one side , and the dsct on the other side is in two separated facilities . 
this may have had influence in patients transportation and logistics in particular for younger patients with worse clinical conditions . in our oncological population ( tables2 , 3 ) , we achieved significantly lower delivered dose in both patients groups . 
a better image quality , beyond the implementation of iterative reconstructions present on both scanners , has in part to be related to reduction in motion artifacts in faster acquisitions with dsct . the significant reduction in motion artifacts plays a main role in chest examinations where lower rotation times and acquisitions at ultra - high pitch possible with dsct significantly increased image quality ( tables4 , 5 ) [ 9 , 25 ]  . 
in younger and uncooperative patients , the acquisitions at ultrahigh pitch mode no longer required sedation on dsct , while with the ssct sedation was necessary for patients younger than 6years . as expected , with low - dose chest ct examinations ( tables4 , 5 ) , we achieved lower ctdi values in all patients groups . 
the higher median tube current with dsct in these groups of patients has to be related to the frequent use of spectral shaping with tin filter , which is compensated by the tube current . 
even though the evidences in terms of dose reduction with the spectral shaping are less robust for the pediatric population , in particular when considering smaller children , in our pediatric population , we recorded a lower dose also in terms of total dlp in smaller patients ( table4 ) , while in older patients was comparable ( table5 ) [ 14 , 15 ]  . 
 moreover , in chest ct with dsct , sequential acquisitions planned on ssct were avoided with only volumetric acquisitions with more images but also more information and better anatomical coverage . this study has some limitations . 
even if there are no strictly defined limits for patient radiation exposure , it is recommended to try to keep doses as low as reasonably achievable ( the alara principle )  . 
finally , the risk - benefit analysis of each examination , and careful communication of this risk to the patient , is emphasized . keywords pediatric radiology radiation protection computed tomography radiation - induced cancer child pregnancy introduction the use of medical imaging in children has increased during the past few decades , raising concerns about risks associated with radiation . 
new techniques are now employed in medical fields where justification , optimization , quality assurance and training may need careful evaluation , such as * paolo tom paolo.toma@opbg.net 1 dipartimento diagnostica perimmagini , ospedale pediatrico bambino ges , irccs , rome , italy 2 dipartimento di diagnostica perimmagini , policlinico universit degli studi di palermo , via del vespro 127 , cap90127palermo , italy 3 uoc radiologia ospedale pediatrico giannina gaslini , genoa , italy 4 servizio prevenzione e protezione / fisica sanitaria , ospedale pediatrico bambino ges , irccs , rome , italy 5 department ofclinical radiology , great ormond street hospital forchildren , nhs foundation trust , london , uk use of cone - beam ct in dentistry . 
10% or more of ct examinations worldwide are performed for patients under the age of 18 . managing exposure to radiation from medical imaging is a complex challenge ; efforts that aim to reduce exposure in childhood include improvements in pediatric protocols , technological advances in equipment and implementation of diagnostic reference levels ( drls )  . european directive framework the new european directive 2013 / 59 / euratom sets out basic safety standards for protection against the dangers arising from exposure to ionizing radiation and highlights the need for justification of medical exposure , requirements concerning patient information , quality assurance programs ( recording and reporting doses from radiological procedures ) , the use of drls , the availability of dose - indicating devices and vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 736744 the improved role and support of the medical physics experts in imaging . damage ( greater in middle age ) , which may vary according to cancer type [ 7 ]  . article 61 of the european directive 2013 / 59 / euratom [ 1 ] is focused on children , emphasizing that special attention will be paid to quality assurance programs and to the evaluation of the dose or verification of the activity administered for the practices involving medical exposure of children and to high doses procedures , which may be the case in interventional radiology , nuclear medicine , computed tomography or radiotherapy . article 62 of the european directive 2013 / 59 / euratom states that if pregnancy cannot be excluded , depending on the medical radiological procedure , special attention shall be given to the justification and optimization , taking into account both the pregnant mother and the unborn child . factors thatinfluence therisks ofradiation the biochemical and physiologic damage produced by radiation generally occurs within hours or days , but the impact of these changes , such as the induction of cancer , can take decades to manifest . 
the third step is tumorigenicity [ 2 ]  . radiation exposures , like the medical ones , induce a cellular genomic instability that is transmitted to progeny , which was little described as a persistent enhancement in the rate of which genetic changes arise in the descendants of the irradiated cells after many generations of replication has been termed a non - targeted effect of radiation , as genomic damage occurs in the cells that receive no direct radiation exposure [ 3 ]  . 
most childhood tumors occur sporadically , but in 1015% of the cases , a strong family association and genetic basis for radiation sensitivity are present , such as li - fraumeni syndrome or neurofibromatosis type 1 , although the exact mechanism for this is unclear . the effects of radiation are the greatest on rapidly developing tissues and organsin fetuses , infants and young children [ 4 ]  . 
in pregnancy , the major biological effects of fetal demise , growth restriction , organ malformations and cognitive deficits are seen only with doses in excess of routine diagnostic imaging [ 5 ]  . 
recently noted that cancer induction risk ( greater at younger ages ) must be balanced with the radiation - induced promotion of premalignant evolution ofknowledge estimates of the carcinogenic risk of radiation are derived from epidemiological studies of large populations , such as the atomic bomb survivor cohort and nuclear industry workers and also from dose - response models , such as the linear no threshold ( lnt ) [ 8 ]  . 
diagnostic imaging uses lowlevel radiation that is defined , for the purposes of radiation risk , as < 100150msv ( i.e. , < 20msv for a single - phase pediatric ct examinations )  . 
 [ 11 ] , the lnt model is commonly adopted because it ensures a conservative approach ( i.e. , the model may overestimate the risk of cancer induction at low doses )  . the radiation - induced clustering of dna double - strand breaks into repair centers shows a nonlinear doseresponse in human cells and is much higher at smaller doses , implying that lnt extrapolation could lead to overestimation of cancer risk in the low dose range [ 12 ]  . 
the life span study ( lss ) cohort of about 120 000 subjects included atomic bomb survivors and residents of hiroshima and nagasaki who were not in either city at the time of the bombing . 
the fukushima health management survey will then contribute to future epidemiological research on nodular thyroid diseases in children and adolescents [ 15 ]  . the risk associated with low doses is estimated to be small , such that it cannot be quantified accurately , as even very large studies would lack adequate statistical power to demonstrate small differences . 
published the preliminary results of the epi - ct study ( epidemiological study to quantify risks for pediatric computerized tomography and to optimize doses ) that recruited a total of about 950 000 patients who had undergone ct at least once before the age of 22years [ 16 ]  . 
when considering time since the exposure greater than 5years , the cancer standardized mortality ratios ( smrs , i.e. , the ratio between observed and expected number of deaths based on national reference rates ) decreased to the level of the general population while the non - cancer smrs remained significantly increased . 
these authors conclude that the study population was less healthy than the general population , and reverse causation bias should be considered for cancer risk analyses . the american association of physicists in medicine ( aapm ) supports the position that when such exposures are medically appropriate , the anticipated benefits to the patient are highly likely to outweigh any small potential risks . 
in the position statement pp 25 - c , aapm declares that at the present time , epidemiological evidence supporting increased cancer incidence or mortality from radiation doses below 100msv is inconclusive.and that any predictions of hypothetical cancer incidence and mortality from the use of diagnostic imaging are highly speculative this may lead some patients to fear or refuse safe and appropriate medical imaging , to the detriment of the patient [ 17 ]  . 
it may be hypothesized that low - dose radiation could enhance the immune system response and thus reduce cancer incidence overall . imaging dose optimization there are no absolute defined limits for patient radiation exposure . 
two international campaigns aim to reduce exposure of children : ( a ) image gently [ 24 ] sponsored by the alliance for radiation safety in pediatric imaging in the us and in 70 other countries around the world ; ( b ) eurosafe imaging [ 25 ] sponsored by the european society of radiology ( esr )  . gonadal shielding the use of gonadal shielding is debated . 
 [ 27 ] determined the incidence of missing or misplaced gonadal shields in pediatric orthopedic practice and determined the frequency with which visualization of bony landmarks is compromised by pelvic shielding . 
further , they reported that , because of the identified errors in misplacement of pelvic shielding and potential repeated imaging , pelvic shielding does not reduce the risk of radiation exposure for boys and potentially increases the risk of radiation exposure for girls . furthermore , slovis and strauss [ 29 ] highlighted how a significant fraction of the gonadal dose in both genders is from internal scatter , which is not attenuated by a properly placed gonadal shield . 
assuming that with proper collimation , added filtration and technique selection , the gonadal 1 3 la radiologia medica ( 2019 ) 124 : 736744 dose without lead shielding from the examination should be 2550gy for boys and 1325gy for girls , the estimated increased risk from omitting gonad shielding is relatively small . 
these authors conclude that in order to lower the radiation dose , reducing the number of radiographs and teaching the proper collimation of images can have a greater effect than placing gonadal shields . radiation protection influoroscopy radiation reduction is not always appropriate because some examinations require multiple and additional projections , greater fluoroscopy time or magnification , or lower image noise to answer specific clinical questions . 
planning includes clarifying with requesting physicians what the clinical question is , i.e. , whether the radiation imaging test is justified , and also preoperative planning for efficiency can minimize dose during fluoroscopic and angiographic examinations . a number of dose management strategies exist for fluoroscopy and interventional radiology , including those by the international atomic energy agency and alliance for radiation safety in pediatric imaging [ 30 ]  . 
radiation exposure in fluoroscopy is widely variable across and even within different institutions , [ 31 ] hindered by lack of technical standardization . the only fluoroscopic examination included in the pidrl report was the micturating cystourethrography , and no national pediatric drls have been set for interventional radiology procedures in any eu country to date [ 22 ]  . 
drls for non - standard or newer life - saving interventional radiology procedures may be neither possible nor useful for more complex procedures . icrp 121 reports some key concepts to reduce dose during fluoroscopic examinations [ 32 ]  . 
still images acquired using last - image hold should be used to review findings instead of live fluoroscopy ( repeated exposure )  . the radiation field adjustments should be done with the light beam and not with the fluoroscopy function ( x - ray beam )  . 
collimation of the x - ray beam is essential to reduce the exposed area and to keep radiosensitive areas ( breast , eyes , thyroid and gonads ) away from the x - ray beam , when possible . 
finally , patient dose needs to be recorded and reviewed . interventional radiology procedures account for only 1% of x - ray procedures , but they are responsible of 10 - 15% of cumulative x - ray exposure . 
suggested values for the trigger level for a deterministic effect are a skin dose of 3gy , a kerma - area product of 500gycm2 , or an air kerma at the patient entrance reference point of 5gy [ 34 ]  . when the patients radiation dose from the procedure exceeds the institutions trigger level , clinical follow - up should be performed for early detection and management of skin injuries . optimization ofpediatric ct protocols relative to other imaging modalities , ct can provide a comparatively large dose of ionizing radiation . 
technical innovations allowing faster examinations and better quality imaging have spread the use of ct in children in the last two decades [ 37 ]  . clearly , imaging modalities that do not depend on ionizing radiation , such as ultrasound or mri , are realistic alternatives . 
several authors emphasize that attention shall be given not to reduce the ct dose too much : the real risk to the patient of an inadequate examination , either not yielding the correct diagnosis or needing to be repeated because it was non - diagnostic , is far greater than a small risk of latent malignancy [ 39 ]  . 
mdct scanners are now installed with default settings providing 1 3 740 la radiologia medica ( 2019 ) 124 : 736744 a perfect standard image and deliver the corresponding standard dose . optimization is a process by which a substantial portion of the standard dose is eliminated with a consequent increase in noise , but without loss in diagnostic performance and / or confidence . 
a number of factors are involved in the optimization of ct protocols . tube current : a reduction in tube current ( ma ) is directly related to an increase in image noise and the opposite . 
however , very small children generally have less adipose tissue between organs and tissue planes and this can result in an excessive image noise related to tube current reduction and may need a proportional increase of the product of tube current and tube rotation time ( s )  . 
weight - based or girthbased protocols should be used when imaging pediatric patients , rather than age - based protocols . optimization includes consideration of the following factors : peak kilovoltage : increasing the kilovoltage ( kvp ) increases the energy of spectrums photons , which results in a more penetrating x - ray beakvp has an exponential relationship with dose , and a decrease of 20kvp will decrease the dose by about 3540% . 
a lower kvp generally improves bone detail and substantially increases contrast for ct angiography , while soft tissue studies without the use of a contrast agent are typically improved by increases in the kvp with appropriate reductions in the ma to result in reasonable patient doses [ 34 ]  . pitch : a pitch of approximately 1.31.4 and a short rotation time ( ~ 0.5s ) to minimize total scanning time are generally recommended for pediatric body ct examinations . 
cardiac studies require a faster rotation time and a lower pitch , thus resulting in increased patient dose . automatic exposure control ( aec ) : this system is available in most modern scanners . 
the improper use of aec can result in increased patient dose or non - diagnostic examination [ 42 ]  . patient positioning : centering the patients body in the isocenter of the ct gantry reduces the radiation dose to the patient . 
if the patient is not correctly positioned , the bowtie filters produce an inappropriate compensation of the x - ray beam resulting in more x - rays penetrating thinner peripheral portions of the patients body and less x - rays penetrating in the central , thicker portion of the patient [ 43 ]  . iterative reconstructions : this method processes several passes over the raw data ( obtained using low - dose techniques ) to produce more accurate model of images and to reduce the amount of noise [ 44 ]  . 
implementation requires time , careful adjustment of many acquisition parameters and diagnostic image acceptance . clinical indication - based ct : acceptable levels of image noise are not the same for all ct examinations . 
this changes according to the body site ( i.e. , imaging of the chest or skeletal system , can tolerate relatively increased noise , thus requiring a smaller dose , compared to brain , liver and other solid abdominal organs ) , and the clinical indications , including cumulative patient exposure . 
for example , a low - dose ct technique may be used to detect renal stones in children without compromising detection [ 46 ]  . single - phase scan : a single - phase scan is generally all that is needed in pediatric imaging [ 41 ]  . 
in order to reduce the dose , the length of the scout and the scan length should be limited to the clinical area of interest [ 47 ]  . radiation protection inpregnancy thousands of pregnant women are exposed to diagnostic radiation examinations each year . 
a misinformation on the radiological risks related to diagnostic examinations in pregnant or potentially pregnant women always causes anxiety in radiologists and patients and can lead to voluntary interruption of pregnancy . several well - recognized published documents provide guidance regarding imaging of pregnant women . 
the ircp 84 [ 48 ] states that prenatal doses from most properly done diagnostic procedures present no measurably increased risk of prenatal death , malformation , or impairment of mental development over the background incidence of these entities . 
this evidence is based on atomic bombs survivors and survivors of childhood cancers treated with radiotherapy . 1 3 la radiologia medica ( 2019 ) 124 : 736744 the american college of radiology established that fetal doses below 100mgy should not be considered a reason for terminating a pregnancy [ 49 ]  . 
the american college of obstetricians and gynecologists [ 50 ] published the following policy statement : women should be counseled that x - ray exposure from a single diagnostic procedure does not result in harmful fetal effects . 
specifically , exposure to < 5rad ( 50mgy ) has not been associated with an increase in fetal anomalies or pregnancy loss . according to these documents , the risk to the unborn baby from radiation doses of < 50mgy is negligible . 
doubling that dose ( i.e. , 100mgy ) , the increase over background incidence for organ malformation and the development of childhood cancer combined results in about 1% . according to the international commission on radiological protection , prenatal doses from most correctly performed diagnostic procedures present no measurably increased risk of prenatal or postnatal death , developmental damage including malformation , or impairment of mental development over the background incidence of these entities ; lifetime cancer risk following in utero exposure is assumed to be similar to that following irradiation in early childhood [ 51 ]  . 
however , there is no safe level : the alara principle requires that we use diagnostic methods without ionizing radiation whenever they are equivalent in reaching the diagnosis to those with radiation . 
the risks to the mother require justification , such as the proliferating breast gland that is more sensitive to radiation , or the metabolic adaptations to as well as anatomical changes of the pregnancy that may predispose to certain diseases , modifying indirectly the risks or benefits of a diagnostic imaging procedure . 
effects may be either stochastic or deterministic , with a rather high threshold [ 52 ]  . while the natural risk for malformations at birth is 4% , 100mgy of conceptus dose will only slightly reduce the proportion of children without a malformation from 96 to 95.8% [ 5 ] , and similarly , the natural rate of 99.3% of children without a cancer during childhood will just marginally decrease to 99.07%. in summary , after implantation of the conceptus in utero exposure by less than 100mgy has no proven deterministic effects , but the stochastic effects of cancer induction , although small , are estimated to exist and to increase in proportion to the dose [ 53 ]  . 
deterministic effects exhibit a threshold of around 100mgy even during the most sensitive phase of organogenesis . the alara principle means that ultrasonography and magnetic resonance imaging and any non - imaging diagnostic examinations should be considered before x - ray imaging or nuclear medicine techniques are used . 
when ionizing radiation is appropriate , lower exposure is preferred to higher exposure as long as imaging quality is adequate to answer the clinical question . the anatomical area exposed to direct radiation is the most important factor predicting the uterine dose . in general , when performing a radiological examination in a pregnant woman , the clinical risk of not performing the examination must be evaluated . 
if the fetus is in the direct beam , the procedure should be tailored to reduce the fetus dose ( i.e. , for radiographic examinations : collimate the beam , increase kvp , remove the anti - scatter grid ; for ct : collimate the beam and reduce the scan to the very specific area of interest )  . 
fluoroscopic time must always be limited to the minimum [ 52 ]  . any department offering imaging services , beyond complying with general quality standards , has a number of duties regarding radiation exposure of pregnant patients . duties ofadepartment ofradiology , communication anddecision duties of a department of imaging include information , screening for pregnancy , counseling , documentation and the decision for the best justified examination . 
the stronger the arguments for a critical situation of one of them are , the easier is the justification ; in contrast , a vague suspicion would not justify an important exposure . 
while policies in different departments may differ slightly , it is important that each department formally states its rules in written form and follows them consistently . imaging thenonpregnant woman every adolescent girl and woman of childbearing age has to be considered as potentially pregnant and should be asked whether she is pregnant or thinks she could be [ 52 , 54 ]  . 
as the hormone level does not increase before implantation ( with individual variation ) , it is suggested not to perform the test earlier than 10days after ovulation ; blood tests are more sensitive and , thus , become positive around 2days earlier [ 56 ]  . 
patients below the age of 16 / 18years pose an additional management challenge : they are both children under the responsibility of their parents and individuals with their own rights of privacy and discretion . 
depending on the national legislation , the medical staff has a critical role of giving information to and accepting decisions and consent from the right person . 1 3 742 la radiologia medica ( 2019 ) 124 : 736744 imaging thepregnant woman if pregnancy has been confirmed , justification will differ in the following three scenarios : - imaging without ionizing radiation and imaging of the extremities or the head and neck are justified as in non - pregnant women . 
as radiation exposure is absent or irrelevant , the examinations can be performed anytime . - imaging of the trunk of the body without direct radiation to the conceptus will cause some scatter radiation and a dose of well below 1mgy to the conceptus . 
examinations of this category will usually be performed when well - justified , but optimization becomes more important : the field of view should be minimized to the clinical question . 
a medical physicist should calculate the conceptus dose for intermediate or high - dose examinations of the trunk with the potential of more than 1mgy to the uterus , but not for examinations of the extremities or head . 
 termination of pregnancy should only really be considered for conceptus doses above 100mgy , depending on the phase of pregnancy [ 50 , 51 ]  . occupational exposure the first duty of a department is to inform female workers of the existence and the risks of occupational exposure , the legal duties and rights , and to train them to behave correctly to minimize exposure [ 51 ]  . 
international guidance and national laws clearly prescribe the exposure level allowed for a pregnant worker : as soon as she informs the employer of the pregnancy , the employer shall ensure employment conditions for the pregnant worker such that the equivalent dose to the unborn child is as low as reasonably achievable and unlikely to exceed 1msv during at least the remainder of the pregnancy [ 57 ]  . comparison of the radiation exposure from a diagnostic examination with other radiation exposures ( such as chest x - rays or natural background radiation ) has been proposed as a tool to communicate with parents , but this system may be misleading ; in fact , the dose of a chest x - ray is so low that comparing it with the level of dose of any other radiological procedure may be unnecessarily alarming . 
moreover , background radiation involves whole - body exposure , whereas diagnostic radiation exposures more often have regional ( more localized ) exposures . a key concept that may help in the communication of the potential risk from radiological examination is that of the lifetime baseline risk ( lbr ) and the lifetime attributable risk ( lar )  . the lbr is the general chance that everyone has of having a cancer and / or dying from cancer over the course of her / his lifetime . 
the benefit of early diagnosis and treatment must be balanced with the current understanding of latent cancer risk , compared to the age of the patient and other comorbidities . a recent who document helps support the discussion about benefits and risks of radiological examinations [ 58 ]  . taking active steps to reduce the risk of ionizing radiation during pregnancy and childhood is imperative . 
relevant changes include new definitions , a new dose limit for the eye lens , non - medical imaging exposures , procedures in asymptomatic individuals , the use and regular review of diagnostic reference levels ( including interventional procedures ) , dosimetric information in imaging systems and its transfer to the examination report , new requirements on responsibilities , the registry and analysis of accidental or unintended exposure and population dose evaluation ( based on age and gender distribution )  . 
furthermore , the directive emphasises the need for justification of medical exposure ( including asymptomatic individuals ) , introduces requirements concerning patient information and strengthens those for recording and reporting doses from radiological procedures , the use of diagnostic reference levels , the availability of dose - indicating devices and the improved role and support of the medical physics experts in imaging . keywords bss european directive euratom medical exposures radiation protection radiodiagnostic and radiotherapeutic procedures introduction the new european directive 2013 / 59 / euratom [ 1 ] , laying down basic safety standards ( bss ) for protection against the dangers arising from exposure to ionising radiation and repealing directives 89 / 618 / euratom , 90 / 641 / euratom , 96 / 29 / euratom , 97 / 43 / euratom and 2003 / 122 / euratom , is expected to have a relevant and positive impact on european radiodiagnostic and radiotherapeutic procedures . the basic safety standards take into account the new recommendations of the international commission on radiological protection ( icrp ) [ 2 , 3 ] and are revised in the light of new scientific evidence and operational experience . 
the directive was unanimously adopted by the council of the european union ( eu ) on 5 december 2013 after 4years of work by different european scientific and technical committees . 
dose limits shall not apply to medical exposures . according to the new directive , a high level of competence and a clear definition of responsibilities and tasks among all professionals involved in medical exposures are fundamental to ensure adequate protection of patients undergoing medical radiodiagnostic and radiotherapeutic procedures . 
this applies to medical doctors , dentists and other health professionals entitled to take clinical responsibility for individual medical exposures , to medical physics experts and to other professionals carrying out practical aspects of medical radiological procedures , such as radiographers and technicians in radiodiagnostic medicine , nuclear medicine and radiotherapy . furthermore , the directive requires radiation protection education , training and provision of information . the directive distinguishes between existing , planned and emergency exposure situations . 
considering this new framework , the directive covers all exposure situations and all categories of exposure , namely occupational , public and medical . the most relevant changes in the new directive in comparison with the existing ones96 / 29 / euratom [ 4 ] on the protection of workers and the general public and 97 / 43 / euratom [ 57 ] on medical exposuresare : 1 . 
new non - medical imaging exposures ( article 22 ) replacing the old medico - legal exposures other requirements of directive 2013 / 59 / euratom with high relevance to medical imaging are : 1 . 
member states shall ensure that the operational protection of exposed workers is based on optimisation of radiation protection in all working conditions , including occupational exposures as a consequence of practices involving medical exposures . regulation forradiological procedures inasymptomatic individuals a new article ( 55.2.h ) on justification has been added , concerning medical radiological procedures on asymptomatic individuals , to be performed for early disease detection . 
 such procedures should either be part of a health screening programme or require specific documented justification for that individual by the practitioner , in consultation with the referrer , following guidelines from relevant medical scientific societies and the competent authority . 
underlines the need for appropriate local reviews whenever diagnostic reference levels are consistently exceeded and requires that appropriate corrective action is taken without undue delay . article 18 of the new directive deals with education , information and training in the field of medical exposure . 
the selection of equipment required to perform radiation protection measurements ; equipment for interventional radiology installed after 6 february 2018 must have a device to inform the practitioner and those carrying out practical aspects of the medical procedures of the quantity of radiation produced during the procedure . equipment for interventional radiology and computer radiography must have a device to inform the practitioner and those carrying out practical aspects of the medical procedures of the quantity of radiation produced at the end of the procedure . 
such equipment installed after 6 february 2018 must be able to transfer the information required above to the record of the examination . all new medical radiodiagnostic equipment must provide the practitioner with the relevant parameters for assessing patient dose and where appropriate to transfer this information to the record of the examination and , if available , to the rdim systems to ensure data recording as required by the directive for the purpose of dose assessment to the population . equipment used for external beam radiotherapy , installed after 6 february 2018 , with energies greater than 1 mv , must have a device that verifies the key treatment parameters . it is the responsibility of each department of radiology , nuclear medicine and radiotherapy to ensure the correct management , verification and safe storage of exposure data for the different procedures according to international standards using the reference metrics indicated in table1 . these parameters provide information on the individual procedure , but must take into account the level of uncertainty of the data supplied or estimated . 
the uncertainty should be estimated by the appropriate medical physics expert for each modality . it should be noted that the registration of the exposure data must be provided for all procedures , such as interventional radiology procedures performed with portable or remote equipment . the exposure data , supplied by the medical radiological equipment outside radiology departments , must be managed as an integral part of the radiology information systems with 1 3 726 la radiologia medica ( 2019 ) 124 : 721727 the metrics indicated by the international standards and by the present document . for radiotherapy treatments , the dose to the tumour target and to the critical organs is an integral part of the end - oftreatment clinical report . 
exposure data deriving from the imaging used for the preparation of the treatment plan and verification must be recorded and archived according to the same procedures envisaged for diagnostic imaging . for radiometabolic therapy treatments in nuclear medicine , reference should be made to the specific document / guidelines that defines the specific fields of application for the different therapies / isotopes , provided by the manufacturer and as developed jointly by the nuclear medicine and medical physics societies . for nuclear medicine activities , that use unsealed sources , the activity administered , the radiopharmaceutical used and correction factors that allow these data to be correlated with the patients exposure must be documented . for hybrid equipment , e.g. 
pet / ct , exposure data for both diagnostic techniques must be reported . in order to guarantee the efficacy of the registration of the activity and the type of radioisotope used for nuclear medicine investigations , it is necessary , in compliance with the regulations for the good preparation of radiopharmaceuticals , that the flow of information throughout the process is also traceable and certified . the exposure data will have to be managed by carrying out appropriate tests as indicated by current standards . 
this must be implemented correctly and exhaustively by the equipment manufacturers and be updated throughout the life of the equipment used . accidental andunintended exposures : article 63 member states shall ensure that : a . 
for all medical exposures , the undertaking implements an appropriate system for the record keeping and analysis of events involving or potentially involving accidental or unintended medical exposures , commensurate with the radiological risk posed by the practice ; d . 
arrangements are made to inform the referrer and the practitioner , and the patient , or their representative , about clinically significant unintended or accidental exposures and the results of the analysis ; ( ii ) ( i ) the undertaking declares as soon as possible to the competent authority the occurrence of significant events as defined by the competent authority ; the results of the investigation and the corrective measures to avoid such events are reported to the competent authority within the time period specified by the member state ; f . 
mechanisms are in place for the timely dissemination of information , relevant to radiation protection in medical exposure , regarding lessons learned from significant events . article 63 introduces a new set of requirements for registration and analysis of accidental and unintended medical exposures . in the registration of accidental exposures , tools of incident reporting must be present to record and manage the incidents . estimates ofpopulation doses : article 64 the age and gender must now be taken into account in the distribution of individual dose estimates from medical exposures . 
the competent authorities of each member state will have responsibility for the registration and monitoring of population exposures ; for this purpose , exposure data storage systems ( rispacs ) become indispensable . 
rdim systems are useful for transferring correct and certified data to central depositories responsible for collecting and analysing the data . for such transfers , it is essential to use recognised international standards and precisely the ihe profiles for radiation exposure monitoring ( rem )  . the data to be sent to the central depositories must be certified by the practitioner responsible for the radiological system and by the medical physics expert in order to ensure the correct management of exposure data . the above - mentioned professionals must be provided with the appropriate instruments and technological resources to carry out their functions . general recommendation it is inappropriate to use the estimated effective dose parameter for an individual patient . 
this quantity refers to a standard patient ( usually reference phantom ) and should therefore not be used to derive individual radiological risk values ( icrp 103 )  . the evaluation of the radiation dose to the patient , if required or necessary , requires complex evaluation of the 1 3 la radiologia medica ( 2019 ) 124 : 721727 experimental data , and it is the exclusive competence of the medical physics expert . if the referrer wants to know the risk associated with the estimate of the radiation dose absorbed by a patient , it should be obtained from the practitioner . 
the estimate of the absorbed dose is the responsibility of the medical physics expert who will carry out a personalised dosimetric evaluation . finally , it is considered essential that authoritative sources of information are used on the complex issue of medical exposures . 
for all these activities , radiation oncologist should coordinate and collaborate with a team including different professionals : nurses , radiographers ( rtt ) , clinical engineers , information system experts , taking advantage in particular of the dosimetry expertise of the medical physicist . 
this paper describes several contemporary and emerging concerns related to radioprotection in radiation therapy including quality and safety in external beam radiotherapy and brachytherapy , foetal dose , secondary malignancies , and the safety issues related to the new techniques and treatment strategies . keywords radioprotection radiotherapy radiation exposure radiation risk management introduction in radiation therapy , unlike most other applications involving ionizing radiation , the intent is to deliver high doses of radiation to cancer , limited by the adverse effects of radiation to healthy tissues . 
radiation safety , for patients and staff , is a crucial responsibility for all members of the radiation oncology department . a high level of competence and a clear definition of responsibilities and tasks among all professionals involved in medical exposure are fundamental to ensure adequate protection of patients undergoing radiotherapy . 
this applies to medical doctors , medical physicists and other professionals carrying out practical aspects of radiotherapy procedures , such as radiographers . clinical responsibility means responsibility of a practitioner ( health professional who is entitled to take clinical responsibility for an individual medical exposure in accordance with national requirements ) for individual medical exposures , in particular : justification , optimization , clinical evaluation of the outcome , cooperation with other specialists , giving information on the risk of ionizing radiation to patients , etc . the regulatory bodies require that health professionals with responsibilities for medical exposure are specialized in the appropriate area and that they fulfil the requirements for education , training and competence in the relevant specialty . radiation oncologists ( ro ) have the full and final responsibility for treatment , follow - up and supportive care of the patient . 
they should : ensure that the exposure of normal tissue is kept as low as reasonably achievable while the required dose is delivered to the planning target volume ( the alara principle )  . establish optimized protocols and quality assurance programmes for therapeutic procedures . ensure that radiotherapeutic procedures for women who are pregnant or likely to be pregnant be avoided unless there are strong clinical indications ( otherwise life - threatening diseases ) ; assume the responsibility for the consent procedure regarding prosecution / interruption of the pregnancy , and when needed define the most efficient radiation protection strategy for the women and embryo / foetus . evaluate any radiation accident or incident from a medical point of view . for all these activities , ro should coordinate and collaborate with a team including different professionals : nurses , radiographers ( rtt ) , clinical engineers , information system experts , taking advantage in particular of the dosimetry expertise of the medical physicist . safety andquality inexternal radiotherapy andbrachytherapy the actual work up of the radiotherapy process is needed to guarantee appropriateness , quality and safety . 
over the last decade , the rapid development of new technology has significantly changed the way in which radiotherapy is planned and delivered , with the surge of a variety of new technologies and approaches . external beam radiotherapy three - dimensional computed tomography - based planning is today a standard , but more recent imaging modalities such as magnetic resonance imaging ( mri ) and positron emission tomography ( pet ) may be used . 
flattening filter - free machines , improved immobilization techniques and more sophisticated planning and data management software are the basis for the exponential increase in the use of stereotactic techniques , delivering very high fractional doses . 
 more than half of the italian linear accelerators ( linacs ) are in fact equipped [ 2 ] with cone beam or megavoltage ct on board , to verify target position before delivering the appropriate radiation dose to the target . 
the radiation exposure deriving from the ct used for the treatment plan preparation and the verification of the correct patient daily treatment position may be globally considered irrelevant for the calculation of the dose delivered to patient [ 3 ]  . 
in fact , igrt permits a large dose reduction to critical structures thanks to clinical target volume ( ctv ) planning target volume ( ptv ) margin reduction [ 4 ]  . 
therefore , even if the frequency and number of cts obtained may change according to specific disease and to different igrt strategies , such extra dose may be considered almost negligible . 
the recent clinical introduction of hybrid machines combining a linac and an on - board mri allows the ro to avoid the use of ionizing radiations to perform igrt treatments ; the same holds true for the new mri simulators . 1 3 la radiologia medica ( 2019 ) 124 : 777782 at the same time , new techniques may raise new concerns . 
for example , the use of techniques such as intensity - modulated radiotherapy ( imrt ) or volumetric modulated arc therapy ( vmat ) may expose larger volumes of normal tissue to low doses , in comparison with conventional 3dcrt . 
some authors , for example , are reluctant to use imrt for female with hodgkin lymphoma because of concerns over excessive low - dose exposure of large volumes of normal tissues such as the breast [ 6 ]  . 
however , although the risk of breast cancer is clearly dose - dependent , the relationship between lowdose radiation and carcinogenesis is more speculative [ 7 ] , as further specified in the section on radioprotection of children and during pregnancy . therefore , training of the radiation oncologists should provide sufficiently detailed knowledges and adequate skills to cope with these technical advances in external beam radiotherapy . 
however , every step of the radiotherapy work - up requires the knowledge of the natural history and biology of cancer that profoundly impact also on the dose reduction to critical organs . 
a typical example of that is the very large reduction in the treated volumes in the management of hodgkins lymphomas ( from extended fields to involved fields ) as well as for paediatric patients , avoiding unnecessary exposure of a very large amount of healthy tissues , independently from the technique used . 
for example , dose escalation aiming at better tumour control should be considered cautiously when applied to concomitant chemoradiotherapy for lung cancer [ 8 ]  . brachytherapy another effective therapeutic use of radiation is brachytherapy , in which radioactive sources are placed permanently or temporarily in or very near the target volume . 
in some cases , the ro works together with the surgeon to position brachytherapy devices , such as needles , during open surgery , but in general the surgical competence and the expertise necessary for the ro involved in this technique must be very high . 
the use of afterand / or remote - loading devices allows reducing the risks of exposure of the involved professionals ; brachytherapy is , however , more demanding from the radioprotection point of view than external beam radiotherapy . the main concept of brachytherapy is to exploit the rapid fall - off of the dose with the increasing distance from the sources . 
among the more widely used procedures , permanent implantation of encapsulated 125i and 103pd sources , colloquially called seeds , has been a common method for low dose rate ( ldr ) prostate cancer treatment since the 1990s [ 10 ]  . 
more recently , breast brachytherapy with balloon - catheters , and particularly high dose rate ( hdr ) brachytherapy , has increased significantly and , in general , adherence to recommended radiation protection standards based on the usual principles ( distance , time , shielding ) is important in the process of patient care . trained personnel must be appropriately informed and work together to ensure adequate radiation protection during the work up of this highly individualized treatment . 
for a detailed analysis of radiation protection measures in brachytherapy , the interested reader is referred to guidelines and recommendations produced by several organizations , including the american brachytherapy society ( abs ) , astro , the groupe european de curiethrapie - european society for therapeutic radiology and oncology ( gec - estro ) , the acr and the aapm [ 1113 ]  . radioprotection ofchildren andduringpregnancy ionizing radiation is a known carcinogen to which children are particularly vulnerable [ 14 ]  . 
although the mechanism of greater susceptibility is not well understood , it is likely to be linked to faster cell division in growing and developing tissues [ 15 ]  . 
 age dependence for these cancers , which are among the 1 3 780 la radiologia medica ( 2019 ) 124 : 777782 diseases for which radiation has been more often involved as a possible causative agent , is complex , and generally , the risk due to radiation is added to the overall increase in cancer risk due to aging . these considerations may have an impact on treatment planning . 
some concerns include a possibly increased risk of secondary cancers ( sc ) from imrt but accumulating evidence suggests that sc risk after imrt is likely not higher than with more traditional techniques such as 3d - crt . 
 [ 17 ] , there was no difference in the risk of leukaemia or myelodysplasia after imrt versus 3d - crt , and also the risks of other solid cancers and lymphomas did not significantly differ between imrt and 3d - crt . 
 [ 18 ] : nevertheless , this initial report remains unclear whether in addition to the other advantages of particle therapy for some tumour types it might measurably reduce clinical sc risk . 
despite the potential increased risk of sc , rt for paediatric cancer is a life - saving procedure that should not be withheld when clinically indicated . managing cancer during pregnancy is another very critical clinical situation . 
pregnant women with malignant diseases are advised to delay radiotherapy until after delivery but when this is not possible due to life - threatening tumours , it is estimated that the possible radiation effects , such as mental retardation and organ malformations probably only begin to manifest above a threshold dose of at least 500mgy [ 19 ]  . 
in effect , the dose to the embryo and foetus depend on several factors [ 21 ] : ( a ) the treatment machine used and its leakage radiation ; ( b ) the target dose : the risk of detrimental effects on the embryo / foetus is less likely when treating diseases such as lymphomas ( prescribed doses 3040gy ) compared to lung neoplasms ( prescription doses of about 60gy ) ; ( c ) the size of the radiation fields ; ( d ) the distance from the edges of the fields to the embryofoetus ; and ( e ) the use of wedges , lead blocks , compensators and other scattering objects . 
lesser leakage , lower target dose , smaller radiation fields , greater distance of the edges of the radiation fields from the embryofoetus , and avoidance of wedges and other scattering objects decrease the radiation dose to the embryofoetus . 
 radiation treatment for neoplasms of the head , neck and thoracic region with adequate uterine shielding should be only performed in centres with experience in managing patients diagnosed with cancer during pregnancy . prevention ofaccidental exposure in italy , about 230 , 000 patients per year are submitted to radiotherapy out of 366 , 000 people / year with malignant tumour ( airtum 2014 )  . 
in europe , the 2013 / 59 / euratom directive that sets the basic safety standards concerning protection against dangers arising from exposure to ionizing radiation makes a legal obligation to report and makes corrective measures for accidental and involuntary exposures [ 24 ]  . 
all reasonable measures are to be taken to minimize the probability and magnitude of accidental or unintended exposures of individuals subject to medical exposure ; 1 3 la radiologia medica ( 2019 ) 124 : 777782 2 . 
for radiotherapeutic practices , the quality assurance programme includes : a study of the risks to be prevented , an appropriate system for the record keeping and analysis of events ( follow - up ) ; 3 . 
for all medical exposures , the person responsible for the treatment machine should implement an appropriate system for the record keeping and analysis of events involving or potentially involving accidental or unintended medical exposures , commensurate with the radiological risk posed by the practice ; 4 . 
the hospital and the ro should inform the patient ( or his representative ) and the general practitioner caring for him about any clinically significant unintended or accidental exposures and about the results of analysis ; 5 . 
the undertaking ( the hospital manager ) declares as soon as possible to the competent authority the occurrence of significant events ; also , the results of the investigation and the corrective measures to avoid such events are reported to the competent authority within the time period specified by the member state ; 6 . 
mechanisms are in place for the timely dissemination of information relevant to radiation protection in medical exposure regarding lessons learned from significant events . recently , an italian intersociety consensus underlined these points and recommend to use the available incident reporting tools along with exposure data [ 26 ]  . major cases of accidental exposure in radiotherapy have only been reported a few times over many decades of modern radiotherapy practice throughout the world . 
these rare severe accidental exposures in radiotherapy were due to different causes ( accelerator software problems , incorrect decay data , miscalibration of beams , erroneous use of treatment planning system ( tps ) , computer file not updated and errors in tps data entry )  . 
in italy , the risk of potentially severe errors has been tentatively estimated at about 0.2%. reporting an incident is of little value if what happens is not investigated and analysed . 
different types of ils exist based mainly on the generic hospital incident reporting system or on radiation oncology - specific syste the first one has the advantage to address specific quality and safety concerns , but it might be not targeted for radiotherapy because of the complexity of the processes involved ; from another perspective , develop a specific rt system might be challenging . 
a possible practical option could be to integrate generic incident reporting system with specific radiation oncology report with the aim to identify the so - called sentinel event and get conclusions about patient and treatment - specific factors , to avoid further events [ 28 ]  . 
 furthermore , ilss are recommended by authoritative radiation oncology societies as the american society for therapeutic radiology and oncology ( astro )  . conclusions radiation oncology is a technologically demanding field , which is dependent on well - trained and highly skilled members of the radiation oncology teait is crucial that all members of the team maintain the proper credentials , skills and training levels , satisfying clinical competencies . for radiotherapy treatments , the delivery of radiation dose to the tumour target , minimizing the exposure to critical organs , is an integral part of the end - of - treatment clinical report . 
this software provides estimates of effective dose and doses to the other various organs . results average value of the patients position is found to be below the isocentre for 48 25mm and 29 27mm in the prone and supine position . 
it was observed that the increase in ctdi and dlp values for patients in group 1 , due to the inaccurate positioning , was estimated at about 30% and 20% for prone and supine position , respectively , while in group 2 , a decrease in ctdi and dlp values was estimated at about 16% and 18% for prone and supine position , respectively , due to an average position above isocentre . 
a dose increase ranging from 4 up to 13% was calculated with increasing the overscanned region below anal orifice . conclusion radiographers and radiologists need to be aware of dose variation and noise effects on vertical positioning and over - scanning . 
17 , 90128palermo , italy 5 department ofsurgical andmedical sciences andtranslational medicine , sapienza - university ofrome , santandrea university hospital , via di grottarossa 1035 , 00189rome , italy introduction the constantly increasing number of computed tomography ( ct ) examinations and consequent progressive increase of dose exposition of population lead clinicians and patients themselves to a growing concern about radiation dose [ 14 ]  . 
 dose exposition needs to be as low as possible without reducing the quality of ct examinations especially when x - rays are used for screening purpose [ 59 ]  . ct colonography ( ctc ) performed with multi - detector ct scanner ( mdct ) is well known as valuable alternative technique to optical colonoscopy ( oc ) in the evaluation of colon , replacing barium enema for all clinical queries [ 10 , 11 ]  . 
american college of radiologist ( acr ) and the american cancer society ( acs ) colorectal cancer advisory group suggest ctc for colorectal cancer screening vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 762767 on individual basis , also in high - risk patients if unwilling to undergo colonoscopy [ 6 ]  . msct 64 slice ( ge lightspeed vct - ser ) equipped with volara digital das and asir . european society for gastrointestinal radiology ( esgar ) and acr guidelines suggest a standardized low - dose acquisition protocol aimed to maintain dose exposure as low as reasonable achievable [ 5 , 6 ]  . 
the guidelines for screening ctc recommend a tube voltage of 120kv , tube current of 5080ma and total exposure dose for two positions ( prone and supine ) within a ct dose index volume ( ctdivol ) of 12.5mgy. 
in ctc position , operator mistake may have in higher impact compared to routine abdominal scan due to double acquisition performed with patient supine and prone . ctc acquisition protocol parameters and reconstruction techniques are routinely implemented for reducing radiation dose according to patients size ; however , some pure operator - dependent factors can significantly affect radiation exposure [ 12 ]  . different studies underlined how patient positioning with respect to gantry isocentre could increase absorbed and effective dose in thoracic and abdominal ct [ 7 ]  . 
moreover , scan length affect organ dose , if we consider that exceeding below anal orifice , in the case of ctc acquisitions , leads to irradiation of male gonads [ 1315 ]  . for all of these reasons , we focused our investigation on these two , most relevant , operator - dependent parameters ( exact patients position and precise scan length ) that can be easily corrected during examination . 
in ctc position , operators mistake may have higher impact compared to routine abdominal scan due to the double acquisition performed with patient supine and prone . materials andmethods we performed a retrospective analysis of mdct acquisition data of two separated groups of patients that underwent ctc in 2years in two different secondary referral hospitals , policlinico universitario of palermo ( group 1 ) and ospedale universitario i.c.o.t. 
of latina ( group 2 )  . both electronic medical record databases were retrospectively searched for consecutive patients who underwent ctc of the abdomen between march 2015 and may 2017 . 
patients were eligible for inclusion in the study if they underwent clinically indicated ctc and both prone and supine scans were available . our final study population consisted of 199 patients . 
both centres have similar examination protocol consisting in 2 scout scans and other 2 abdomen scans , respectively , in prone and supine position , according to esgar guidelines [ 5 ]  . care dose4d performs automatic tube current modulation in the angular and longitudinal directions and also adapts to different anatomical regions and patient sizes . 
volara digital data acquisition system ( das ) delivers high processing power for high - quality images and low - dose performance based on attenuation and mas revelation from initial scan ( ge healthcare source )  . all images were imported into commercially available software , which supports dual - energy post - processing capabilities in group 1 ( syngo dual energy , version vb 10b ; siemens healthcare ) and in osiris in group 2 . 
the last distal images to include the inferior pubic rami were considered within the protocol , while any additional images below were instead considered not necessary and potentially avoidable . ct dose reports were derived from pacs in ctdivol ( ct dose index volume ) and dlp ( doselength product )  . the ct scanner software provided ctdivol values , and according to their specifications , these values were measured according to guidelines eur16262 / 1998 [ 16 ] ( and to verify that the measured value was within 10% of the console displayed ctdivol [ 16 ] )  . in order to evaluate the estimated effective total dose and the dose to various organs , we used the ct - expo software version 2.2. 
for 1 3 764 la radiologia medica ( 2019 ) 124 : 762767 each patient , an estimate of the effective dose was achieved by using the dlp value stored inside the pacs system and the scanner obtained through the ct - expo software . 
since real patients do not match exactly the features ( in terms of weight and height ) of the standard patients , the dose values obtained through this analysis are only estimates of the real doses absorbed by patients [ 17 ]  . regarding the calculation of dose increase due to inaccurate patient positioning , we used the values of ctdi as function of the position reported in the literature [ 1821 ]  . 
in particular , we fitted those experimental values with a quadratic function ( of the type f ( x ) = a * 2 + b * x + c ) and we used the best - fit function to rescale the dose values obtained from the images . 
patient bmi data were not available as not routinely collected , and due to the retrospective nature of the study , but patient thickness of the abdomen was available from the images data [ 17 ]  . results mean estimated dose in first cohort was slightly below 5.0msv for the university hospital of palermo , while in second cohort was about 3.1msv. 
this involves a significant increase of the effective dose of about 23% as shown in fig.3. in the case of the university hospital of latina , since the patients are on average scanned above the isocentre and according to literature the positioning above the isocentre involves a dose reduction , the decrease in ctdi and dlp values , due to this positioning , was estimated at about 16% and 18% for prone and supine position , respectively [ 1820 ]  . 
if the data from both hospitals are analysed together , on average an increase in ctdi and dlp values , due to the positioning , was estimated at about 15% and 4% for prone and supine position , respectively . 
error bars correspond to 1 s.d maximum patient thicknesses were calculated from ct images in both prone and supine positions . the values related to the patients scanned in group 1 are 234 33mm and 262 38mm in the prone and supine position , respectively , whereas , these values are 270 36mm and 291 38mm in the prone and supine positions , for group 2 . 
as expected , the thickness values in prone position are smaller than those in supine position because at prone position the body weight squeezes the abdomen . furthermore , we noticed that often the acquisition of ctc exceeded the area required for the diagnostic question 1 3 la radiologia medica ( 2019 ) 124 : 762767 fig . 
error bars correspond to 1 s.d of the examination ; indeed , the acquisitions were performed by scanning also regions below the anal orifice , therefore exposing sensitive anatomical organs to ionizing radiation , especially in male patients . 
through our ct - expo software version 2.2 , we estimated effective dose to testicles and prostate in our 31 male patients , that is values ranging between 212msv ( mean 3msv ) for testicles and 428msv ( mean 9msv ) for prostate . 
in one patient , over - scanning below anal orifice was not significant ( 0mm in prone position ; 12mm in supine position ) with estimated dose of below 2msv to testicles and prostate . mean estimated dose in group 1 was slightly below 5msv , while in group 2 was about 3msv ( table1 )  . as can also be seen from fig.4 , the process of overscanning regions up to 8cm below anal orifice involves a percentage increment of effective dose of atmost 2% for female patients . discussion berrington de gonzalez [ 22 ] reported estimated mean effective dose per ctc screening study between 7 and 8msv in patients from 50 to 80years old . 
mean estimated effective dose for our patients was ~ 5msv and ~ 3msv , respectively , for two cohorts . as confirmed in recent literature , moderate - level iterative reconstruction and high - level iterative reconstruction methods have crucial role in saving dose protocols [ 18 ] , thus reducing radiation - related risks [ 2 , 22 ] , an even more essential matter concerning a screening examination as ctc . 
 however , we need to remember that even if our ct scanner is equipped with iterative reconstruction , wrong positioning leads to an unnecessary dose increase [ 19 , 20 ]  . our results show that imprecise acquisition techniques , occurring when optimized protocols for implementing the fig . 
nowadays , the acquisition technique is an important topic to take into account in the daily practice of acquisition of examinations , giving larger importance to the amount of ionizing radiation dose that is provided to the patient in routine tests [ 11 ]  . in literature , consequences of wrong positioning are well documented . 
 [ 19 ] reported significant changes in organ doses resulting from vertical positioning in paediatric chest ct ( breast dose increased up to 16% and thyroid dose up to 24% in lower positions )  . 
 [ 20 ] performed a study reviewing a group of 480 patients , showing mis - centring of 2.2cm in average below the isocentre with an increase of 23% for patient dose . 
reviewing and comparing these data to phantom testing , eurosafe imaging group observed a 22% difference in dose from 6 - cm table height difference , resulting also in contrast change and noise increase [ 21 ]  . 
two different scout views are required in ctc examination because the abdomen in obese patients may vary in supine and prone position ; in fact in prone one the abdomen may be squeezed resulting in a diverse ap and ll value from supine position . our data suggest that there is a trend for radiographers to get worst centring on prone position ( 48 25mm ) than on supine position ( 29 27mm ) , probably because a supine abdomen ct scan is far more common that prone and anyway each scanning is susceptible of errors . during our retrospective analysis , we found that scan often exceeded the area required for the ctc examination , including also regions below the anal orifice , therefore exposing sensitive anatomical organs to ionizing radiation , especially in male patients . on the basis of fig.4 which reports estimates of the effective dose increment with increasing the over - scanning below anal orifice ( calculated through the ct - expo software ) , we can conclude that an over - scanning of 2cm would cause an effective dose increment of about 6% , whereas this dose increase is of about 12% for over - scanning of 5c five centimeters is the mean value of over - scanning for the first cohort , while two centimeters is the mean value for the second cohort . furthermore , we can evaluate differences between two centres where this study was conducted . 
both table height and extension of scanning below anal orifice parameters varied significantly between the two patient groups . naturally , the best examination possible is the one that maintains an acceptable diagnostic quality with lowest dose possible , as alara principle states [ 9 ]  . 
radiologists and radiographers need to be specifically trained to perform such peculiar examination in order to reduce patient dose exposure [ 3 ]  . our study is characterized by intrinsic limitation : firstly , only two centres were involved and a retrospective analysis that can be improved with further data derived from direct modification in acquisition technique and phantom measurements . 
our patients data may be considered incomplete due to the lack of body mass index ( bmi ) , but in the patient area of interest , the abdomen , we have the data of patient thickness according to the ssde of the aapm [ 17 ]  . 
then , distance between table and centre of patient and from anal orifice to last slice was not automatized . this study was aimed to evaluate operator - related errors on positioning and centring of patients regardless of availability of iterative reconstruction methods and patient characteristics . 
it is our believe that only if you acquire and measure dosimetric data , you can understand real impact of centring errors on daily practice , especially for screening examination as ctc . dose surveillance programs as doses from computed tomography ( ct ) examinations in the uk are useful to understand and monitor ionizing radiation impact on general population . 
even if dose saving technology and continuous update of ct apparatus are essential , a significant dose reduction can be obtained from operator - dependent factors surveillance . in conclusion , radiographers and radiologists need to be aware of dose variation and noise effects on vertical positioning and over - scanning . 
more accurate training need to be achieved even so when examination protocol varies from general practice . compliance with ethical standards conflict of interest the authors declare they have no conflict of interest . ethical approval this article is a retrospective study not implying any modification in patients treatment or images protocol and is an analysis of dose data of the ct examinations performed . 
effective doses due to the radiopharmaceuticals can be estimated by multiplying the administered activities by the effective dose coefficients , while for the ct component the dose - length product can be multiplied by a conversion coefficient k . 
although the effective dose can be used to estimate and compare the risk of radiation exposure across multiple imaging techniques , clinicians should be aware that it represents a generic evaluation of the risk derived from a given procedure to a generic model of the human body . 
it cannot be applied to a single individual and should not be used for epidemiologic studies or the estimation of population risks due to the inherent uncertainties and oversimplifications involved . 
this has led to an increase in per capita annual radiation dose to the us population due to nuclear medicine procedures from 0.14msv in 1982 to 0.8 msv in 2006 [ 1 ]  . most of this rapid growth is due to the diffusion of molecular hybrid imaging procedures such as single - photon emission computed tomography / computed tomography ( spect / ct ) and positron emission tomography / computed tomography ( pet / ct ) that provide relevant functional and anatomical information [ 2 ]  . 
these hybrid systems show high sensitivity , specificity , and accuracy and also increase reader confidence and decrease inter - observer variability through more accurate localization and definition of scintigraphic findings [ 3 ]  . the spect and pet have been used for some years to obtain functional and metabolic information in a variety of pathologic conditions . 
the following introduction of ct determined a significant change , commuting spect and pet in hybrid imaging systems ( spect / ct and pet / ct ) , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 768776 which are able to provide functional and anatomic images and to overcome the limitations of the separate modalities . 
 within a few years , hybrid imaging became one of the most powerful diagnostic tools available in a number of nuclear medicine departments across the world , and nowadays it plays a vital role in the clinicians daily workflow [ 4 ]  . hybrid imaging is used in several clinical applications , especially in oncology , since it allows a better localization of disease , its characterization before and after therapy , an accurate delineation for biopsy and therapy planning , as well as the detection of the most clinically relevant lesions [ 5 ]  . 
pet / mri hybrid scanners have been introduced into clinical practice both as separate units with a common bed and as a fully integrated unit that allows for simultaneous acquisition of pet and mri . 
although these devices are considerably more expensive than commercial pet / ct units and the clinical indications are still being developed , they have received growing attention ( fig.2 ) in regard to the reduction in radiation dose to the patient due to the elimination of the ct component [ 6 ]  . however , the hybrid systems ( figs.3 , 4 ) inevitably lead to an increase in medical radiation exposure because the radiation dose to patients is the sum of the dose due to the administered radiopharmaceutical and the dose from the ct component of the study [ 7 ]  . 
1 trend of scientific papers published in medical literature ( pubmed ) between 1989 and 2018 about spect / ct and pet / ct 1 3 770 la radiologia medica ( 2019 ) 124 : 768776 fig . 
4 example of pet / ct system radiation doses inhybrid imaging in hybrid imaging , the total radiation dose to patients is the sum of the dose due to the radiopharmaceutical used for spect / pet imaging and the dose derived from the ct component of the study . 
the combined acquisition of functional and anatomical images can substantially increase radiation exposure to patients , particularly in case of a hybrid system with diagnostic ct capabilities . in nuclear medicine , the effective dose due to the administration of radiopharmaceuticals can be calculated by multiplying the administered activity by the effective dose coefficients per unit of administered activity . 
 [ 9 ] , adapted from the icrp publication 80 [ 10 ] , and the administered activities in terms of diagnostic reference levels ( drls ) recommended by dlvo 187 / 00 [ 11 ] for spect and pet . the ct component is responsible for a considerable percentage of the patient dose of a hybrid imaging examination [ 1214 ]  . 
the dlp can also be used to obtain an approximate estimate of the effective dose to the patient , by multiplying the dlp by a conversion coefficient k specific for the anatomical region under examination ( e = k dlp )  . 
in these data , each clinical purpose was associated with a wide range of doses and there was a significant overlap in doses for different clinical purposes , thus highlighting the need for optimization in hybrid imaging . 
for most studies , the ct effective doses were less than 30% of the ones due to radiopharmaceuticals and they only exceeded the 50% mark in case of the radiopharmaceuticals administered for half - body pet / ct and meta - iodobenzylguanidine ( mibg ) spect / ct examinations . in hybrid imaging , the effective dose due to the ct component depends on the different clinical purposes such as attenuation correction ( ac ) , anatomical localization , and sometimes even diagnosis . 
 [ 17 ] , with reference to diagnostic spect / ct , reported an additional 614msv to the radiation dose of the radiopharmaceutical , depending on the field of view in z - axis . 
miller [ 20 ] showed an even lower radiation exposure for the ct component of the spect / ct examination , such as 0.47msv for an abdominal non - diagnostic localization and attenuation - correction scan . 
however , the estimated value of effective dose is subject to a high degree of uncertainty , related to the tissue - weighting coefficients that are used and their estimation of relative biologic risk [ 22 ]  . 
thus , effective dose must be interpreted as a broad , generic estimate of biologic risk , and differences of several msv do not imply a true discrepancy in biologic risk [ 23 , 24 ]  . martin [ 23 ] evaluated the inherent uncertainties in estimating effective dose to be about 40% . 
as a consequence , biologic risk should be described using broad categories : negligible , < 0.1 msv ; minimal , 0.11 msv ; very low , 110msv ; and low , 10100msv [ 23 ]  . 
he also suggested that because effective dose was defined by the icrp [ icrp 103 ] to represent an overall risk averaged over all ages and both sexes for a reference patient , neither the monte carlobased organ - dose coefficients nor the dlp - based k values [ 15 ] should be used to calculate effective dose estimates for individual patients or to predict population risks . moreover , the k coefficient is based on data averaged over many scanner makes and models and therefore cannot accurately represent a specific scanner . 
finally , since the dose coefficients are calculated using a simplified anthropomorphic patient model , all estimates of effective dose are applicable only to scans of a standard adult patient . 
considering the recent increase in the number of overweight and obese patients , the calculated values of effective dose should therefore be used with caution . in conclusion , although the effective dose can be used to estimate and compare the risk of radiation exposure across multiple imaging techniques , clinicians should be aware that table 4 radiation dose reduction methods in hybrid imaging it represents a generic evaluation of the risk derived from a given procedure to a generic model of the human body . 
it cannot be applied to a single individual and should not be used for epidemiologic studies or the estimation of population risks due to the inherent uncertainties and oversimplifications involved . dose reduction andoptimization inhybrid imaging practical ways to reduce radiation dose to patients eligible for hybrid imaging include adjustments to both the planning phase and throughout the execution of the study ( table4 )  . planning phase prior to the execution , spect / ct and pet / ct must be subject to the principle of individual justification of radiation exposure , which is stated as a sufficient net benefit when balanced against possible detriment that the examination might cause . 
both the prescriber and the nuclear medicine physician must take into account the specific objectives of the examination and the clinical data of the patient involved , in order to avoid unnecessary radiation exposure [ 11 ]  . in addition to the radiation exposure justification , the choice of the radiopharmaceutical which has shorter physical and biological half - life also permits to reduce the patient radiation dose . 
usually , 99mtc - labeled radiopharmaceuticals should be preferred due to the favorable physical properties of the radionuclide . drls are a useful tool to optimize the radiation dose to patients undergoing spect / ct or pet / ct examinations . 
the drls related to the radiopharmaceutical component of a hybrid imaging procedure are established in terms of administered activity , while the ctdivol and the dlp are used for the ct component . 
currently in italy , the drls for planar and spect radiopharmaceuticals are set at a national level in dl 187 / 00 , while for the pet radiopharmaceuticals they are defined only at a local level . 
as to the ct component , the adoption of the standard planning phase execution phase general and individual justification of the examination choice of the radiopharmaceuticals , promoting the ones with shorter physical and biological half - lives adherence to national and / or institutional dlrs patient hydration and bladder voiding detectors with higher energy resolution ( cdznte in spect / ct ) special collimators , which allow a higher sensitivity ( variable focus collimators ) iterative algorithms able to reconstruct the image with less counts without affecting spatial resolution 1 3 774 la radiologia medica ( 2019 ) 124 : 768776 diagnostic drls is not appropriate because of differences in the clinical purpose , scan range , and image quality requirements of hybrid imaging ct scan . 
two surveys have been recently conducted in switzerland and uk in order to evaluate ct doses for a wide range of pet / ct and spect / ct procedures aiming to propose national drls [ 16 , 25 ]  . hydration and bladder voiding are also important ways for dose reduction in hybrid imaging since they limit the radiation dose to the bladder , which is the critical organ subject to the higher exposure . 
these devices , mainly used in nuclear cardiology , provide a fourfold to sevenfold improvement in sensitivity thanks to higher resolution and contrast - to - noise ratio , if compared with a conventional dual - detector spect . 
a variable focus collimator was developed by siemens retaining the magnifying properties of a cone - beam collimator near the center of the field of view and eliminating the truncation artifacts at the edges of the field that are common to pinhole and focusing collimators . 
several studies conducted in different fields proved that it is possible to achieve the same image quality with a smaller number of collected counts [ 3134 ]  . similarly , also in ct imaging the introduction of iterative methods allowed significant radiation dose reduction without sacrificing image quality . 
it is now recognized iterative methods , compared with fbp method , increases detectability at a given radiation dose and allows radiation dose reduction while maintaining low - contrast detectability . in hybrid imaging , the structural information provided by ct serves different purposes such as ac , anatomical localization , and sometimes even diagnosis . 
the radiation dose due to ct can be reduced by an accurate choice of ct protocols ( i.e. , lowor high - dose ct ) and scan parameters , such as tube potential , tube load , rotation time , beam width , pitch , and reconstructed image thickness . 
as a general rule , low - dose acquisition is suggested when a recent diagnostic ct is available , in case of evaluation of treatment response , and to better study lesions showed in planar or spect images . a large number of studies covering the previously mentioned parameters have been published [ 35 ]  . 
the introduction of simulation tools allows to optimize the ct scanning parameter by adding an artificial level of noise to the ct raw data in order to simulate a lower - dose examination , without affecting the image quality . 
a useful method to reduce the dose to radiosensitive organs close to the body surface ( i.e. , mammary glands , thyroid glands , and eye lenses ) in spect / ct is the organ - based tube current modulation . 
to compensate for this reduction , the tube current in the x - ray projection from the opposite side is increased thus leaving mean image noise constant [ 27 ]  . 
in musculoskeletal imaging , uric acid material decomposition images can help identify articular deposition of uric acid crystals ( in addition to the detection of uric acid renal stones )  . 
material separation can also help detect bone marrow edema on ct in the case of trauma , algoneurodystrophy , inflammation ( osteitis ) or malignant bone marrow infiltrates , such as metastases . 
dual - source scanners are equipped with two x - ray tubes , which work at different voltages ( 70kv and 150kvp ) allowing simultaneous acquisition of images at these two different energy levels . 
the use of two x - ray tubes with different energy levels makes it possible to extract information and characterizes the chemical composition of material , based on the different degrees of x - ray beam , absorption and attenuation , according to the atomic weight electron density of the compounds [ 7 ]  . 
comparing attenuation values at high vol . : ( 0123456789 ) 1 3 1176 la radiologia medica ( 2019 ) 124 : 11751183 and low energy levels permits dect post - processing algorithms and provides the basis for material decomposition [ 8 ]  . 
the principal applications in musculoskeletal imaging include : ( 1 ) detection of urate crystals in gout or other crystal - induced arthropathies , e.g. , calcium pyrophosphate dehydrate ( cppd ) crystal arthropathy ; ( 2 ) bone marrow edema ( bme ) detection , e.g. , in the case of trauma , algoneurodystrophy or inflammation ( osteitis ) ; ( 3 ) characterization of collagenous structures , such as tendons , ligaments and intervertebral disks ; ( 4 ) minimization of metal prosthesis beam - attenuating artifacts . 
in this context , one of the most outstanding possibilities in musculoskeletal radiology is the so - called virtual non - calcium technique ( vnca technique ) , which makes it possible for edemas to be visualized , as it is necessary to detect fragility fractures [ 9 ]  . 
several technical approaches such as , sequential acquisition , rapid voltage switching , dual - source ct ( dsct ) , layer detecting , quantum countingoffer different spectral contrasts and dose efficiencies . 
three main types of algorithms are currently used to post - process dect data sets : ( 1 ) image optimization algorithms usually provide three sets of images : two sets of mono - energetic images ( typically at 80 or 100kev and 140kev ) , as well as an optimum contrast image from nonlinear blending of the low - energy images ( providing high contrast ) and high - energy images ( providing low noise ) ; ( 2 ) differentiation algorithms allow a certain material to be subtracted from the data set , or the differentiation between two materials , through color - coding , for example ; ( 3 ) quantification algorithms are based on three - material decompositions and can provide color - coded images of iodine content in post - contrast examinations [ 10 ]  . applications ofdualenergy ct tomusculoskeletal imaging dualenergy ct forevaluation oftophaceous gout gout is one of the most common forms of inflammatory arthritis , with prevalence rates above 1% across much of the world . 
dect may be a promising and noninvasive imaging method to assess and diagnose early - stage or acute gout and can help to prevent complication of the chronic late stage of the disease . 
it can directly depict monosodium urate ( msu ) deposits and may easily confirm a diagnosis of gout in patients with normal serum urate levels or exclude it in patients with hyperuricemia [ 11 ]  . 
dect is able to separate different materials , such as calcium , a high molecular weight compound , from uric acid , a low molecular weight compound , as well as cortical bone from trabecular bone . 
 the materials are then color - coded and superimposed on to standard dect images at a multimodality workstation , where multiplanar and three - dimensional volume rendering reformations may be produced and viewed 360 around any axis to best depict the msu deposits . 
this function is particularly useful in quantifying monosodium urate crystals and can be used to monitor the response to treatment and as an outcome measure in patients with gout [ 13 ]  . 
in recent years , a number of studies have shown the ability of dect to detect deposits of monosodium urate crystals with high sensitivity ( 78100% ) and specificity ( 89100% ) [ 1417 ]  . 
therefore , the use of dedicated software dect can measure tophus volumes in the extremities and may be able to demonstrate reduction in tophus volume after successful therapy [ 13 , 18 ]  . 
knee joint view displaying ( b ) urate deposits ( depicted in green ) in the popliteal groove region ( arrow head ) and synovial suprapatellar , lateral and medial recesses of both knees . 
hand / wrist view ( c ) displaying numerous urate deposits ( depicted in green ) along the metacarpophalangeal and proximal and distal interphalangeal joints and in the right wrist . 
automated quantification of urate volume is displayed at the top of each image many reports , including meta - analysis or systemic reviews , have compared us with dect for the diagnosis of confirmed or suspected gout [ 19 ]  . 
dect is a highly accurate tool for detecting the presence of monosodium urate crystals and for confirming gout or distinguishing it from other inflammatory arthritis , although the overall sensitivity of us is higher than that of dect . 
in some studies , dect has proved to be superior in synovial fluid analysis and that a number of patients could be tested false negative by synovial fluid examination alone [ 12 , 23 ]  . dualenergy ct forthedetection ofbone marrow lesions mri has been used as a method of choice for detection of bme . 
conventional ct does not permit the visualization of bone marrow , despite the implementation of numerous protocols , because it is incapable of removing the bone trabeculation and therefore provides inadequate visualization of the bone marrow cavity [ 2426 ]  . 
dect acquires two ct data sets at different energy levels simultaneously and it can characterize and differentiate various chemical elements , through the use of material decomposition protocols [ 8 , 27 ]  . 
 post - processing software is then used to remove calcium in trabecular bone by using a vnca subtraction process , thus creating vnca images [ 24 , 2830 ] , so that the bone marrow can be assessed without superposition . 
in recent years , siemens healthcare has released innovative software containing an enhanced , color - coded , dual - energy ct vnca application , so edema detected can be depicted as color imaging grayscale overlay or even 3d . 
these areas of increased bone marrow attenuation may be due to trauma ( fig.2 ) , algoneurodystrophy ( fig.3 ) , inflammation ( osteitis ) or malignant bone marrow infiltrates , such as metastases . these conditions differ only slightly in density , and there is a considerable overlap , so the differentiation cannot be realized yet , but it appears theoretically possible . 
numerous pitfalls , which can cause false - positive results , have to be recognized ; in particular , it appears difficult to evaluate areas of bone marrow immediately adjacent to cortical bone , sclerotic bone or gas due to potential artifacts [ 28 , 29 ]  . 
2 short tau inversion recovery mr images in the coronal ( a ) and sagittal ( b ) plane demonstrating diffuse bone marrow edema involving the distal right radio , within the side of fracture ( hypointense line , arrow head )  . 
coronal ( d ) multiplanar reformatted color - coded dual - energy virtual non - calcium image showed extensive bone marrow edema ( coded green ) and fracture involving the distal radio ( arrow head ) fig . 
3 short tau inversion recovery mr image in the coronal plane ( a ) demonstrating diffuse bone marrow edema involving head and neck of left femur in patient with algoneurodystrophy ( arrow head ) ; coronal multiplanar reformatted color - coded dual - energy virtual non - calcium image ( b ) reveals bone marrow signal ( depicted in green ) involving the head and neck of left femur , which corresponds to bone marrow edema on the mr image . 
the dedicated software also allows the precise calculation of the attenuation values to be referred to edema in the region of interest ( roi ) 1 3 la radiologia medica ( 2019 ) 124 : 11751183 1179 protocols to detect trauma - associated bme in the spine and extremities , malignant bone marrow infiltration [ 3134 ] and marrow edema associated with inflammatory rheumatic diseases , such as rheumatoid arthritis ( ra ) ( fig.4 ) [ 35 , 36 ] and axial spondyloarthritis [ 31 ]  . 
dect vnca reconstruction has been demonstrated as able to detect bme in traumatic fractured vertebrae and in the detection of incidental thoracolumbar vertebral compression fractures in oncological patients without previous trauma , with high diagnostic accuracy [ 4042 ]  . 
a recent study showed that the dect vnca technique is feasible in the assessment of bme in the sacroiliac joints in patients with axial spondyloarthritis ( axspa ) [ 31 ]  . 
the authors used dect with visual analysis of color - coded images and quantitative roi - based density measurements to detect sacroiliac joint bme , and mr images served as the reference standard . 
dect with the addition of color - coded vnca images to standard ct is also able to simultaneously visualize bme and minor structural lesions in the sacroiliac joints of patients with axspa [ 35 ]  . collagen analysis : ligaments , tendons andintervertebral disks dect is offering a new imaging method to visualize tendons and ligaments . 
with the use of a tissue decomposition algorithm and thanks to their relatively high density , due to the presence of hydroxylysine and hydroxyproline side chains , dect is be able to visualize soft tissue collagenous structures , such as ligaments and tendons , and recognize pathological conditions . using a dedicated software these structures can then be color - coded and fused to standard grayscale ct images . 
 recent studies [ 8 , 43 ] have demonstrated that with dect it is possible to visualize some ligament structures of the knee , such as the anterior cruciate ligament , posterior cruciate ligament , patellar ligament and fibular collateral ligament , without intraarticular contrast media injection , while others , such as the tibial collateral ligament , transversal ligament and oblique popliteal ligament , were not satisfactorily displayed for diagnostic assessment [ 43 ]  . 
althoughthe sensitivity in the detection of ligament damage is lower than for mri , dect may be considered a new imaging method in patients with mri contraindications such as in the case of pacemakers , claustrophobia and in the case of obesity . 
 dect may also play a role in the characterization of tendons , and the volume rendering technique allows anatomic localization , the relationship of the tendons to the bony structures and a better delineation of the soft tissue to be visualized . 
dect makes it possible to visualize the continuity , profile and insertion of many tendons such as the flexor pollicis longus tendon , flexor digitorum superficialis / profundus tendon , achilles tendon , extensor hallucis longus tendon and extensor digitorum longus tendon . 
4 short tau inversion recovery mr image in the sagittal plane of right foot / ankle demonstrating diffuse bone marrow edema involving the tarsal bones and the and the bases of the metatarsal bones in a patient with rheumatoid arthritis ( arrow head ) ( a ) ; sagittal multiplanar reformatted color - coded dual - energy virtual non - calcium image reveals bone marrow signal ( depicted in green ) involving the tarsal bones and the bases of metatarsal bones ( b )  . 
the dedicated software also allows the precise calculation of the attenuation values to be referred to edema in the roi 1 3 1180 la radiologia medica ( 2019 ) 124 : 11751183 dualenergy ct using iodine overlay techniques iodine mapping is an image processing technique used with dect to improve iodine contrast resolution . 
iodine mapping with dect has been clinically used for visualization of regional lung perfusion and in the diagnosis of pulmonary embolism [ 1 , 44 ] and other disorders such as metastatic renal cell carcinoma and squamous carcinoma of the head and neck [ 4547 ]  . 
recently , this innovative imaging method had been used in musculoskeletal issues and in particular to detect inflammation lesions , such as synovitis and tenosynovitis , in the peripheral joints of patients with rheumatic diseases . 
the acquired data are processed with a dedicated software , using a three - material decomposition technique that can identify iodine - containing voxels from dual - energy data and create a virtual unenhanced image . 
the authors concluded that dect iodine mapping is an image processing technique that can delineate inflammatory lesions , preserving the features of ct , such as the reliable evaluation of structural changes and may be particularly useful , not only in early diagnosis of inflammatory arthritis , but also in therapeutic assessment . 
the same authors , in another prospective study [ 49 ] , determined the feasibility of dect with an iodine overlay image ( ioi ) for evaluation of psa in the hand . 
dect is superior to mr arthrography and ct arthrography in the detection of meniscal tears , in the demonstration of suspected intraarticular hip pathology and in the assessment of glenohumeral joint cartilage [ 6 , 58 , 59 ]  . 
however , other studies and large patient trials are required to confirm the potential role of dect arthrography and its clinical efficacy . bone mineral density analysis anddetection ofmetastases promising early results have been seen for the detection of vertebral body density by dect , when compared with dual x - ray absorptiometry ( dxa ) [ 50 , 51 ]  . 
with dedicated software , using quantitative and qualitative tissue decomposition and virtual non - contrast - enhanced imaging and iodine mapping , dect may define and color - code cortical and trabecular bone and makes it possible to identify metastases as abnormal tissue composition or defects in trabecular bone [ 52 ]  . 
however , these techniques will require further investigation to validate their application in a clinical setting . metal artifact reduction techniques many studies support the use of dect in metal artifact reduction through the implementation of energy - specific post - processing , which allows a virtual monochromatic energy spectrum to be created [ 5356 ]  . 
when compared with conventional polychromatic ct imaging , dect demonstrates a lower susceptibility to beam hardening artifacts , provides superior quality and improves the visualization of the peri - prosthetic cortex , medullary bone trabeculation and adjacent soft tissue [ 53 ] , without an increase in the total radiation dose [ 8 , 57 ]  . conclusion in summary , dect represents an emerging field in clinical ct imaging . 
the ability of dect to differentiate materials of different effective atomic numbers makes several new and clinically relevant ct applications possible in the musculoskeletal field , such as detecting bme in the case of trauma , algoneurodystrophy , inflammation ( osteitis ) or malignant bone marrow infiltrates , such as metastases , and to visualize 1 3 la radiologia medica ( 2019 ) 124 : 11751183 1181 tendons and ligaments . 
recently , ultrasonography ( us ) is widely used in musculoskeletal field and us performs better or at least equally well for identification of osteophytes and morphologic degeneration of cartilage in oa patients . 
this review article explains relevant pathologic findings in oa and clinical usefulness in daily practice with us images . keywords ultrasound osteoarthritis synovitis osteophyte cartilage introduction osteoarthritis ( oa ) is the most common disorder of human joints . 
oa of the knee and hip is diagnosed in 40% of people aged > 65years in the uk , and pain is the major symptom of oa causing disability ( e.g. , difficulty in walking and climbing stairs ) [ 1 ]  . 
severity of knee oa is assessed commonly using the kellgrenlawrence system , which is a composite score combining osteophyte presence and jsn for the whole knee [ 3 ]  . 
jsn evaluation is the gold standard in daily practice and has been recommended as the best available method for assessment of jointdamage progression due to oa [ 4 ]  . 
however , conventional radiography is not sensitive to early degenerative changes of cartilage ( which are already occurring before radiographic reduction of the joint space ) and structural alterations visible on conventional radiography ( osteophytes and jsn ) appear only at the relatively late stages of oa [ 5 , 6 ]  . 
in contrast to grading using the kellgrenlawrence system , featureoriented atlas - based compartmental radiographic grading according to standards set by the osteoarthritis research society international is becoming deployed more frequently in clinical research [ 7 ]  . 
 however , radiographic jsn reflects cartilage thinning and meniscal extrusion and does not demonstrate morphologic damage to cartilage and menisci directly [ 8 , 9 ]  . currently , magnetic resonance imaging ( mri ) is being used increasingly to visualize cartilage and intra - articular vol . : ( 0123456789 ) 1 3 1102 la radiologia medica ( 2019 ) 124 : 11011111 of inflamed tissues using noninvasive imaging in daily clinical practice is important . 
although conventional radiography shows lesions affecting bone structure , detection of synovial inflammation using radiography is difficult . us and mri have been recognized as valuable imaging tools to evaluate inflammation severity in synovial tissues [ 19 , 20 ]  . 
the outcome measures in rheumatology ( omeract ) us working group defined synovial hypertrophy as abnormal hypoechoic ( relative to subdermal fat , but sometimes may be isoechoic or hyperechoic ) intra - articular tissue ( fig.1a ) that is nondisplaceable and poorly compressible and which may exhibit a doppler signal [ 21 ]  . 
for example , in ra , a high pdus is associated with pathologic findings of active synovitis , including neovascularization and intensive infiltration of inflammatory cells such as macrophage - like synoviocytes and t - helper - 17 cells [ 22 ]  . 
fluid aspiration is very important for resolving pitfalls in differential diagnoses . us assessment of cartilage has limitations since the acoustic window has only a small area of cartilage available for structures directly . 
mri is the gold standard for assessing the knee joint and is considered to be the most accurate imaging modality for assessment of knee oa [ 2 , 10 ]  . 
despite its high sensitivity , however , mri is not usually employed as an initial imaging method for knee oa and is not readily available for serial evaluation of cartilage status due to practical reasons and expense [ 11 ]  . 
ultrasound ( us ) has been less well studied , but recent high - resolution us , which can be dynamic and offer multiplane visualization , has become of great interest in oa research and daily clinical practice . 
morphologic changes in the bone surface , menisci and femoral cartilage can be depicted reliably and assessed semiquantitatively and / or quantitatively as single features upon us examination [ 1214 ]  . 
additionally , us examination is relatively inexpensive , does not involve ionizing radiation and , overall , there are no contraindications to its use [ 15 , 16 ]  . 
in this review , we describe the specific findings and utility of us for oa assessment . us findings inoa synovitis oa is regarded widely as being primarily a degenerative disorder of articular cartilage , but which is associated with synovial inflammation . 
accurate assessment of synovial inflammation is important for the early diagnosis and evaluation of disease activity not only in inflammatory arthropathies , such as rheumatoid arthritis ( ra ) , but also in oa . 
3 a normal hyaline cartilage is visualized as a homogeneously anechoic layer ( aplio i800 with 24 - mhz probe ultrahigh - frequency transducer , canon medical systems )  . 
usually , on us , an osteophyte has a posterior acoustic shadow , and the size of the osteophyte correlates with the severity of joint damage and duration of oa . 
5 an ultrasound - detected bone erosion ( asterisk ) is discontinuity of the bone surface that is visible in two perpendicular planes at metacarpal head , longitudinal dorsal scan ( a ) and transverse dorsal scan ( b ) la radiologia medica ( 2019 ) 124 : 11011111 in oa . 
however , erosive oa ( sometimes called inflammatory oa ) with more inflammatory signs , such as synovial hypertrophy , pdus and effusion , is recognized an important subtype of hand oa . 
prevalence of knee oa in older populations is increasing and leads to a lower quality of life and working disability , which has major implications for health care and the overall economy [ 29 , 30 ]  . 
highresolution us can be employed to assess the superficial structures in a knee joint , such as synovial tissue , cartilage , menisci , osteophytes and popliteal cysts ( bakers cyst )  . synovitis inknee oa synovial proliferation in knee oa is usually low grade , which can be visualized with / without synovial fluid and / or pdus , though some patients have severe synovitis as the same as in ra . 
a prospective study provided evidence that oa synovitis also generates joint - damage progression , and that usdetected effusion is a predictor of the requirement of total knee arthroplasty [ 31 ]  . 
thus , us - detected synovitis of knee oa can be a target of treatment , as well as demonstrating that us may be a useful outcome measure for studies involving inflammation treatment . cartilage inknee oa establishing clinical measurements of cartilage health and identifying changes in cartilage status are very important for evaluating the effectiveness of protocols to reduce the risk of the development and progression of knee oa [ 32 ]  . 
 although evaluation of knee cartilage by us can be limited due to the depth and lack of adequate visualization , some diseases can be detected clearly by high - resolution us . 
cartilage thickness is an important measure to detect the onset and progression of oa because structural changes in the development and progression of clinical oa are characterized by thinning and loss of cartilage . 
it has been suggested that the center of the medial femoral cartilage should be assessed to evaluate changes in cartilage morphology at the early stage of knee oa [ 36 ]  . 
therefore , accurate and effective tools to measure medial femoral cartilage thickness could be clinically useful and necessary to detect cartilage defects and monitor the treatment effects for thein diagnostic assessment of cartilage thickness , us can be an alternative measure as a clinically available and cost - effective imaging method for articular cartilage of the knee [ 37 ]  . 
we reported that us - assessed damage to the medial femoral cartilage correlated strongly with radiographic narrowing of the medial tibiofemoral joint , and that us was a sensitive imaging method for detecting cartilage damage even in the early radiographic stages of knee oa [ 26 ]  . 
although the peripheral aspects of menisci are visualized clearly , the inner regions are often poorly identified and , in particular , overall visualization of the lateral meniscus tends to be limited [ 39 ]  . 
however , some studies have reported that us assessment is a more accurate imaging method for the detection of medial meniscal extrusion ( fig.6b ) ( which is caused by knee oa and related to knee pain and radiographic medial jsn ) than radiographic assessment [ 18 ]  . 
cyst aspiration with usguided corticosteroid injection from the posterior side of the knee yielded clinical improvement and cyst - volume reduction in patients with a bakers cyst secondary to knee oa [ 45 ]  . 
thus , us examination of the popliteal fossa should be undertaken to detect a bakers cyst to prevent advancement of knee oa . differential diagnoses inknee oa other diseases that should be differentiated from knee oa are crystal - induced arthropathies such as gout and calcium pyrophosphate deposition disease ( cppd )  . 
in one study , dcs identification indicated gout with 83% sensitivity and 76% specificity and disappeared when the serum level of uric acid was < 6ml / dl [ 48 ]  . 
the dcs is differentiated from the normal cartilage interface in that of the latter as a smooth , less bright continuous interface identified only if the cartilage surface is perpendicular to the transducer sound beathe dcs of gout should be differentiated from chondrocalcinosis ( which is seen in cppd and other conditions ) , which appears as hyperechoic calcific foci within the hyaline cartilage [ 47 , 49 ]  . 
they reported that us was an accurate and reliable imaging method for detection of calcification of articular cartilage in the knee joint in patients with cppd [ 52 ]  . 
this four - point scale was : 0 = normal cartilage ( anechoic structure , normal margins of cartilage ) ; 1 = loss of anechoic structure and / or focal thinning of the cartilage layer or irregularities and / or loss of sharpness of at least one cartilage margin ; 2 = loss of anechoic structure and / or focal thinning of the cartilage layer and irregularities and / or loss of sharpness of at least one cartilage margin ; 3 = focal absence or complete loss of the cartilage layer . 
however , the prevalence of hand oa using radiography is not known because of the considerable variation between studies , which may be due to differences in types of populations , disease definitions and / or risk factors ( e.g. , genetic background or environmental exposures ) across study cohorts [ 56 ]  . 
hand oa is found frequently in the first carpometacarpal joint and 25 distal interphalangeal ( dip ) joints , but is also found in 15 proximal interphalangeal joints and 15 metacarpophalangeal joints . 
a , b longitudinal scans 1 3 1108 la radiologia medica ( 2019 ) 124 : 11011111 hyaluronic acid in patients with hand oa , and a decrease in joint thickening and pdus was found . differential diagnoses inhand oa psoriatic arthritis ( psa ) is an inflammatory arthritis that develops in 540% patients with psoriasis [ 62 ]  . 
psa affects the dip joint frequently , and arthritis in the dip joint can be confused with oa , and periosteal proliferation at the level of the dip joints goes into differential diagnosis with oa osteophytes . 
these agents are indicated for treatment of the pain associated with knee oa in patients who do not respond adequately to conservative therapies . traditionally , intra - articular injections have been carried out using anatomic landmarks to identify the correct trajectory for needle placement . 
this has been due , in large part , to the fact that the treating physician cannot visualize the area of interest directly , and variations in anatomy are common . 
furthermore , inaccurate corticosteroid injections in the knee , for example , can result in post - injection pain , crystal synovitis , hemarthrosis , joint sepsis , atrophy of articular cartilage , as well as systemic effects ( e.g. , fluid retention or exacerbation of hypertension or diabetes mellitus ) [ 66 ]  . 
therefore , identification of methods and appropriate training to aid correct placement of the needle during these procedures are warranted . fluoroscopy , ct and mri can be used to improve the accuracy of intra - articular injections . 
however , musculoskeletal us is very practical because it is rapid , safe , relatively inexpensive , emits no ionizing radiation and can be undertaken in the outpatient clinical setting [ 67 ]  . 
radiographic features of psa are characteristic and differ from those observed in ra , especially in the distribution of affected joints and in the presence of destructive changes and bone proliferation at the same time . 
the presence of radiographic bone erosions is fundamental for ra classification , according also to the more recent classification criteria ( american college of rheumatology ( acr ) / european league against rheumatism ( eular ) 2010 classification criteria ) [ 6 ] , while for psa , in the classification criteria for psoriatic arthritis ( caspar ) , radiography still remains one of the main criteria for classifying psa [ 7 ]  . assessing radiographic abnormalities is one of the most powerful means available to the clinical investigator for determining the effects of ra and has been used as a relatively objective marker in clinical trials for evaluating treatment response [ 8 ]  . 
therefore , the current gold standard for radiological evaluation of disease progression in ra is the assessment of disease progression with plain radiographs . many researches have shown that in ra , joint damage occurs within the first 2years after symptom appearance [ 1114 ]  . 
it has been demonstrated that within 4months of vol . : ( 0123456789 ) 1 3 1072 la radiologia medica ( 2019 ) 124 : 10711086 disease onset , 34.9% of patients have erosions evident on x - ray , and 54.9% were erosive at the 12th - month follow - up [ 15 ]  . with the increasing use of dmards and biological dmards ( bdmards ) , early diagnosis is now of paramount importance , and disease progression has to be assessed regularly to monitor efficacy of the treatment [ 1618 ]  . 
in these patients , effective therapy can reduce the odds of progression [ 20 , 21 ] , and both early and intensive treatment can alter the course of the disease by slowing the rate of radiographic progression [ 22 , 23 ]  . regarding psa , at the current state of the art , there is evidence supporting the concept of psa being a distinct disease from ra clinically [ 24 ] , radiologically , and pathologically [ 25 ]  . 
in psa , the presence of radiological damage has been enhanced in 47% of patients within the first 2years , and as in ra , the use of bdmards has been capable of inhibiting progression of structural damage in several randomized controlled trials [ 28 ]  . rheumatoid arthritis andpsoriatic arthritis radiographic comparison as mentioned above , despite certain similarities , the two inflammatory joint diseases show considerably different features . 
in ra , usually , the metacarpophalangeal ( mcp ) joints , the proximal interphalangeal ( pip ) joints , all wrist compartments , and the metatarsophalangeal ( mtp ) joints are the most commonly involved sites . 
in addition , joints in the midfoot and hindfoot , knees , glenohumeral joint at the shoulder , the elbow , and cervical spine can also be affected [ 29 , 30 ]  . in psa , the distribution of affected joints is more often asymmetric and oligoarticular than in ra . 
the distal interphalangeal ( dip ) joints are frequently and early involved , while in ra involvement of the dip joints , in general , is rare and more often a feature of the late disease . 
in psa , dip joints , large joints of the lower extremities , the axial spine , and sacroiliac joints are commonly affected ; the mcp and mtp joints and wrist can be involved as well . the first radiographic changes observed in ra are soft tissue swelling and juxta - articular osteopenia as bone density is reduced adjacent to the joint as a result of local synovial inflammation [ 31 ]  . 
the lack of osteoporosis , even in patients with severe destructive arthritis , is a reliable sign in the differentiation of psa from ra , although the presence of osteoporosis does not exclude psa . the erosions in ra tend to be periarticular and are often described as marginal erosions as they are close to the joint and reflect the direct mechanical action of the hypertrophied synovium and granulation tissue . 
the inflamed synovium slowly invades adjacent structures , causing damage and destruction to the cartilage and bone , leading to joint space narrowing ( jsn ) and bone erosion that can be seen on radiographs . 
the jsn in ra tends to be uniform and concentric , reflecting the generalized nature of the synovial inflammation within the joint . in psa , the early erosive changes predominate in the marginal articular areas , resembling mouse ears . 
 later , the bone appears as if it is being gnawed away , the bone surface becomes frequently irregular or jagged but still sharply delineated , whereas peripherally new bone formation may create an unclear ill - defined outline . 
the uniform reduction of joint space is the radiographic expression of cartilage loss and could be seen at any involved joint , more typically at the dip and pip joints , and more infrequently at the mcp joints . the proliferation of erosions may form irregular excrescences with a spiculated appearance . 
condensation of bone on the periosteal and endosteal surfaces accompanied by thickening of the trabeculae can cause radiodensity of an entire phalanx ( ivory phalanx ) , another manifestation of bone proliferation . 
table1 summarizes the main radiological differences between ra and psa . 1 3 la radiologia medica ( 2019 ) 124 : 10711086 table 1 radiological features that distinguish between rheumatoid arthritis and psoriatic arthritis radiographic features rheumatoid arthritis preponderance for radial sites number of erosions severity of erosions ( size ) erosion distribution dip erosions number of osteophytes severity of osteophytes ( size ) bone proliferation inflammatory changes synovitis tenosynovitis enthesitis dactylitis mutilans ( erosions on both sides of joints ) dips distal interphalangeal joints 1073 psoriatic arthritis evenly distributed radiographic scoring methods inrheumatoid arthritis as discussed above , in ra all the synovial joints can be affected but only some joints in a scoring method can be included . 
these studies indicate the importance to include feet in a scoring method assessing ra radiographic damage . the scoring systems that have been designed to evaluate radiographic changes in ra can be divided into two main groups : global and detailed . 
global scoring systems assign one score to the entire joint , taking into account all the abnormalities seen , whereas detailed systems assign scores on at least two separate variables for each joint evaluated [ 37 , 38 ]  . 
radiographic scores , such as the larsen and sharp scores [ 39 ] and their modifications [ 40 , 41 ] , are the standard methods for determining joint damage and its progression [ 42 , 43 ]  . 
table2 summarizes the main ra features included in the different radiographic scoring methods described below . sharp scoring method ( 1971 ) in 1971 , sharp and colleagues proposed a detailed scoring method for the hands and wrists that is divided into two scores , one for erosions and the other for jsn [ 44 ]  . 
the table 2 features of rheumatoid arthritis included in the sharp and in the larsen scoring systems and further modifications scoring method erosion jsn osteoporosis soft ankylosis cyst sharp ( 1971 ) larsen ( 1977 ) modified sharp ( 1985 ) kaye ( 1987 ) van der heijde / sharp ( 1989 ) + modified larsen ( 1995 ) genant ( 1998 ) ratingen score ( 1998 ) sens ( 1999 ) jsn joint space narrowing , sens simplified erosion narrowing score + = included in the scoring system ; = not included in the scoring system tissue swelling alignment / ( sub ) luxation 1 3 1074 la radiologia medica ( 2019 ) 124 : 10711086 fig . 
a joints selected in each hand for erosions : 4 pip , 5 mcp , ip , scaphoid , lunate , distal ulna , distal radius , the two components of the cmc joints of the thumb are evaluated separately ( pmc and trapeziumtrapezoid )  . 
b joints selected in each foot for erosions : the proximal and distal articular components of the mtp and ip are evaluated separately resulting in a 010 score for each joint . 
c joints selected in the hand : the cmc 3 , cmc 4 , cmc 5 are scored separately , the ip is not included , only the radio - scaphoid part of the radiocarpal joint is evaluated . 
cmc carpometacarpal , cs capitatescaphoid , ip interphalangeal joint , lun lunate , mcp metacarpophalangeal joint , mtp metatarsophalangeal joint , pip proximal interphalangeal joint , pmc proximal metacarpal , rad radius , rc radio - scaphoid , sc scaphoid , st scaphoid - trapezium , tt trapezium trapezoid , ul ulna number and selection of joints in the sharp score evolved in the years , and a modification proposed in 1985 of the sharp method [ 45 ] is now considered the standard for the method . and wrists and also for the feet . 
larsen produced a set of standard reference films to compare the grading of the joints . modified sharp method ( 1985 ) larsen scoring method ( 1977 ) the larsen method was developed by larsen etal . 
however , grade 1 can be based on soft tissue joint swelling only , which is not a real sign of structural damage and is also difficult to assess reliably . 
erosions are counted when discrete , and surface erosions are scored according to the surface area involved [ 45 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 10711086 1075 fig . 
inevaluable joints were not scored and were therefore excluded from analysis . van der heijdemodified sharp scoring method ( 1989 ) the most noticeable difference in the van der heijde modification is the addition of the joints of the forefoot . 
some sites ( triquetrum for erosions and lunate triquetrum , first ip joint and radioulnar joint for jsn ) were difficult to assess in a reliable fashion , mainly due to superimposition , and often were difficult to score leading to interobserver disagreement . 
these modifications also enhance sensitivity and increase reliability . simplified erosion andnarrowing score ( sens ) ( 1999 ) the sens was developed by van der heijde [ 54 ] and is a simplified method by summing the number of eroded and narrowed joints on selected joints on hand and foot radiographs . 
it exploits the same joints of hands and feet , but as opposed to applying a semiquantitative scale of 04 for jsn and 05 for erosions , the sens simply dichotomizes ( bimodal answer modality ) whether an erosion is absent ( score 0 ) or present ( score 1 ) and whether jsn is absent ( score 0 ) or present ( score 1 )  . 
a joints selected in each hand for erosions : 4 pip , 5 mcp , the ip , the cmc of the thumb , scaphoid , distal ulna , distal radius . 
cmc carpometacarpal , csl capitatescaphoidlunate , ip interphalangeal joint , lun lunate , mcp metacarpophalangeal joint , mtp metatarsophalangeal joint , pip proximal interphalangeal joint , pmc proximal metacarpal , rad radius , rc radiocarpal , sc scaphoid st scaphoidtrapezium , ul ulna . 
the + sign represents a 0.5 increment feasibility ofthescoring methods inclinical practice an important disadvantage of the scoring methods for clinical trials is the fact that they require significant training and that scoring according to these methods is time - consuming , making these techniques unfeasible for routine clinical practice . 
the time to score seven radiographs of hands and feet was found to be 3.9min for larsen , 19min for sharp , 25min for the sharp / van der heijde method , and 9min for the ratingen method [ 58 ]  . 
the time needed is one drawback of both the sharp method and the sharp / van der heijde method ; it is related to their higher degree of detail as compared with the larsen and sens methods . radiographic scoring methods inpsoriatic arthritis the measurement of radiographic joint damage in psa is a core outcome measure in both randomized control trials for novel therapies [ 60 ] and longitudinal observational 1 3 1078 la radiologia medica ( 2019 ) 124 : 10711086 fig . 
a joints selected in each hand for erosions : 4 pip , 5 mcp , ip , scaphoid , lunate , distal ulna , distal radius , the two components of the cmc joints of the thumb are evaluated separately ( pmc and trapeziumtrapezoid )  . 
c joints selected in the hand : the cmc 3 , cmc 4 , cmc 5 are scored separately , the ip is not included , only the radioscaphoid part of the radiocarpal joint is evaluated . 
cmc carpometacarpal , cs capitatescaphoid , ip interphalangeal joint , lun lunate , mcp metacarpophalangeal joint , mtp metatarsophalangeal joint , pip proximal interphalangeal joint , pmc proximal metacarpal , rad radius , rc radio - scaphoid , sc scaphoid , st scaphoidtrapezium , tt trapezium trapezoid , ul ulna 1 3 la radiologia medica ( 2019 ) 124 : 10711086 1079 studies [ 61 ] and is included in the research agenda as a domain of interest by the outcome measures in rheumatology ( omeract ) [ 62 ]  . 
these instruments include the modified steinbrocker global scoring method , the modified sharp score ( mss ) , and the modified sharp / van der heijde score ( msvdhs ) for psa [ 36 , 63 ]  . 
as for scoring systems adopted in ra , their lowest common denominator is the large time to performoreover , their scoring requires trained observers . modified steinbrocker global scoring method this method was developed at the psa clinic at the university of toronto . 
the same joints were scored as in the original method , with the addition of the dip from 2 to 5 joints of hands [ 36 , 63 ]  . 
other radiographically detectable changes in psa , such as periostitis and tuft resorption are recorded and scored separately , but not included in the score value . sharpvan der heijdemodified scoring method forpsoriatic arthritis ( msvdhs ) the modification based on the sharpvan der heijde method for ra scores the same joints and definitions as seen in ra [ 41 ] , with the addition of the eight dip joints for erosions and the eight dip and two ip joints of the thumb for jsn . 
spars assess the same joints of the pars in a simpler manner : the grade of the combination of erosion and bony proliferation of the pars is replaced by the sum of joints with erosion and the number of joints with bony proliferation . 
there was consensus that mss and msvdhs were the optimal tool to use in randomized controlled trials ( where sensitivity to change is often the most important attribute of the outcome measure ) , but the most appropriate tool for use in longitudinal observational studies has yet to be established [ 62 ]  . 
the spars has properties which are close to the ones of the msvdhs and pars allowing a quicker calculation [ 67 ]  . 1 3 1080 table 4 features of psoriatic arthritis included in the five radiographic scoring systems for psoriatic arthritis scoring method la radiologia medica ( 2019 ) 124 : 10711086 erosion joint space narrowing bony proliferation modified steinbrocker global scoring method modified sharp score ( mss ) modified sharpvan der heijde method for psoriatic arthritis ( msvdhs ) psoriatic arthritis ratingen score ( pars ) simplified psoriatic arthritis radiographic score ( spars ) fig . 
dip distal interphalangeal joint , ip interphalangeal joint , mcp metacarpophalangeal joint , mtp metatarsophalangeal joint , pip proximal interphalangeal joint conclusion plain radiography remains the gold standard for the assessment of structural joint damage in ra and psa . 
 plain radiography can be helpful in the differentiation of ra from psa and other joint conditions , including osteoarthritis , calcium pyrophosphate deposition disease , gout , and neoplasms [ 71 ]  . 
early bone erosions are correlated with poor long - term radiographic and functional outcome , and early progression in radiographic erosions is related to future impairment in physical function [ 72 ]  . 
the presence of gross osteolysis and pencil in cup is scored separately ; if one of these abnormalities is present , the joint gets the maximum score assigned for erosion ( 5 points ) and for jsn ( 4 points )  . 
a joints selected in each hand for erosions : 4 pip , 5 mcp , ip , scaphoid , lunate , distal ulna , distal radius , the two components of the cmc joints of the thumb are evaluated separately ( pmc and trapeziumtrapezoid )  . 
b joints selected in each foot for erosions : the proximal and distal articular components of the mtp joints and ip are evaluated separately resulting in a 010 score for each joint . 
c joints selected in the hand in the msvdhs : the cmc 3 , cmc 4 , cmc 5 are scored separately , the ip is not included , only the radio - scaphoid part of the radiocarpal joint is evaluated . 
cmc carpometacarpal , cs capitatescaphoid , dip distal interphalangeal , ip interphalangeal joint , lun lunate , mcp metacarpophalangeal joint , mtp metatarsophalangeal joint , pip proximal interphalangeal joint , pmc proximal metacarpal , rad radius , rs radio - scaphoid , sc scaphoid , st scaphoidtrapezium , tt trapezium trapezoid , ul ulna of concepts concerning the severity of ra and psa and the need for tight control to prevent anatomic damage . 
it will have , also , a crucial role in many aspects of treatment in the rheumatic diseases , including identifying patients who are suitable for use of disease - modifying antirheumatic drugs ( dmards ) and biological agents ( bdmards ) , predicting patient response and relapse , and identifying true disease remission [ 17 , 19 , 71 , 73 , 74 ]  . 
a deeper insight into the mechanism of structural changes triggered by these chronic joint diseases is essential for developing therapies that can arrest , prevent , and even reverse bone and cartilage changes . even though magnetic resonance imaging ( mri ) and ultrasound ( us ) demonstrated to be more sensitive than radiographs in detecting early structural changes in joints and surrounding structures [ 75 , 76 ] , availability and costs may limit the use of these techniques in daily clinical practice . further research in the use of mri and us will lead to their proper integration with conventional radiography . 
a joints evaluated in each hand for destruction and proliferation : 4 dip , 4 pip , 5 mcp , the ip of the thumb and the wrist ( evaluated as one joint )  . 
dip distal interphalangeal joint , ip interphalangeal joint , mcp metacarpophalangeal joint , mtp metatarsophalangeal joint , pip proximal interphalangeal joint 1 3 la radiologia medica ( 2019 ) 124 : 10711086 1083 fig . 
 a joints evaluated in each hand for erosion , joint space narrowing and bone proliferation : 4 dip , 4 pip , 5 mcp , the ip of the thumb , and wrist is evaluated as one joint . 
ct is the standard reference imaging modality for visualizing bone damage , including bone erosions in ra , but lacks sensitivity for soft - tissue changes , including synovitis and tenosynovitis . 
ct has a minimal role in ra clinical trials and practice , except in selected patients where mri is contraindicated or not available or if crystal arthritis such as gout or pseudo - gout is suspected . 
mri has documented utility in diagnosis , monitoring and prognostication of patients with ra and is increasingly used for these purposes in clinical practice and particularly clinical trials . keywords magnetic resonance imaging computed tomography rheumatoid arthritis synovitis bone erosion tenosynovitis bone marrow edema diagnosis monitoring prognostication introduction early diagnosis combined with early initiation of appropriate therapy and tight control of inflammation has been recognized as essential for optimal clinical outcomes in rheumatoid arthritis ( ra ) [ 1 ]  . 
this has increased the need for powerful , sensitive techniques that at an early stage can diagnose and indicate the prognosis of patients with ra and accurately monitor the efficacy of treatment . conventional radiography is able to detect structural joint damage in patients with established disease , but is not * mikkel stergaard mo@dadlnet.dk 1 copenhagen center forarthritis research ( copecare ) , center forrheumatology andspine diseases , rigshospitalet , valdemar hansens vej 17 , 2600glostrup , denmark 2 department ofclinical medicine , university ofcopenhagen , copenhagen , denmark 3 department ofradiology , bispebjerg andfrederiksberg hospital , university ofcopenhagen , copenhagen , denmark sensitive for detecting early disease manifestations such as soft - tissue changes and bone damage at its earliest stages [ 2 ]  . computed tomography ( ct ) is a three - dimensional radiographic technique favored by the lack of projectional superimposition and by an exquisite inherent contrast between bone and soft tissue , which makes it a gold standard reference for the detection of bone damage , including bone erosion , new bone formation , calcifications and sclerosis . 
however , ct is hampered by very limited ability to visualize soft - tissue changes using conventional monochromatic ct units , but the introduction of newer ct technologies such as dual - energy or multispectral ct that allows better chemical composition quantification and tissue separation may change this in the near future . magnetic resonance imaging ( mri ) is a non - ionizing imaging technique that has excellent soft - tissue visualization and allows multiplanar tomographic imaging of the body in any plane without projectional superimposition and geometric distortions associated with projectional techniques , such as radiography . 
thus , early bone involvement and inflammatory soft - tissue changes of synovitis vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 11281141 1129 fig . 
axial pre ( a , c ) and post ( b , d ) contrast t1 - weighted images obtained before treatment ( a , b ) and at 1 - year follow - up during treatment with intraarticular glucocortocoids and methotrexate . 
 at baseline , marked post - contrast enhancement , indicating synovitis ( arrows ) , is seen , while only minimal synovitis ( arrows ) is seen at follow - up ( fig.1 ) and tenosynovitis ( fig.2 ) , which are not detectable by conventional clinical , biochemical and radiographic methods , can be directly visualized and evaluated in detail by mri [ 3 ]  . 
disadvantages of mri include relatively higher costs , longer examination times and lower availability than both radiography and ct , and except for whole - body mri ( wbmri ) , mri has restricted anatomical coverage per imaging session . 
mri , as compared to ultrasonography ( us ) , offers greater anatomical coverage than ultrasonography ( us ) does , because us cannot penetrate bone , and thus cannot visualize structures hidden in acoustic shadows . 
coronal short tau inversion recovery ( stir ) images before and 1 year after initiation of tumor necrosis factor inhibitor therapy show bone marrow edema ( osteitis , arrows ) in several carpal joints at baseline , which has disappeared at follow - up 1 3 1130 la radiologia medica ( 2019 ) 124 : 11281141 in clinical trials , the advantage of mri compared to us highly predominates , due to the possibility of standardized image acquisition , centralized reading with full blinding of both image acquisition and reading . 
in clinical practice , us is favored by providing results immediately and thus allows more rapid therapeutic decision making as well as potential for imaging - guided punctures , aspirations , biopsies and injections , but this requires a skilled ultrasonographer and in most instances high - end us equipment in the outpatient clinic [ 3 ]  . this review article will focus on the potential uses of mri and ct in the clinical management of patients with suspected or definite ra . 
after sections on technical aspects , it will describe the current knowledge on mri and ct , respectively , for early detection of ra manifestations , diagnosis of ra , monitoring of disease activity and joint damage progression and its role in determining prognosis . 
 the usefulness in both clinical trials and routine practice will be discussed . magnetic resonance imaging ( mri ) technical considerations high - resolution , t1 - weighted ( t1w ) often three - dimensional ( 3d ) imaging sequences , obtained before and after intravenous contrast injection with or without fat saturation ( fig.1 ) , and a water sensitive technique , such as t2 - weighted ( t2w ) spin echo with fs or short tau inversion recovery ( stir ) ( fig.3 ) , constitute the standard sequences obtained in ra [ 4 ]  . for evaluating structural changes , such as bone erosion , t1 - weighted images are preferred ( fig.4 ) [ 2 , 46 ]  . 
3 coronal t1w 3d gradient echo images post - contrast with axial reconstructions in the level of the wrist ( lower right ) and mcp1 ( upper right ) in a 57 - year - old male with ra for 8years show moderate flexor tendon tenosynovitis of the common flexor retinaculum of the wrist ( arrows ) that can be followed on the axial images involving the flexor pollicis longus and fifth flexor tendons . 
axial ( a ) and coronal ( b ) pre - contrast t1 - weighted images and a coronal short tau inversion recovery ( stir ) image ( c ) show a bone erosion ( long arrows ) in the metacarpal head surrounded by bone marrow edema ( osteitis , short arrows ) also be applied , e.g. , dual echo steady state ( dess ) 3d gradient echo sequences . 
new mri techniques continue to be developed , and a variety of sequences are now available for detecting free water in otherwise fatty bone marrow , indicative of inflammationso called bone marrow edema ( bme ) or osteitis . 
these include t2w spin echo with fat saturation ( t2 fs ) , proton density - weighted with fat saturation ( pdw fs ) or water - excitation ( t2we ) and short tau inversion recovery ( stir ) sequences , but also hybrid sequences , and techniques applying chemical shift - based fatwater separation , such as the dixon technique [ 8 ]  . 
the dixon technique is increasingly being employed , though t2 fs and stir sequences are still most frequent , because of their high general reliability , consistency across different manufacturers and , for stir , applicability at lower magnetic field strengths ( < 1t )  . whole - body mri is promising technique that allows imaging of the entire body in one examination , i.e. , simultaneous assessment of peripheral and axial joints and entheses in both ra [ 9 ] , spondyloarthritis and psoriatic arthritis [ 1012 ] , where it may provide an mri - based total joint inflammation count . 
improved image resolution and more validation are still needed for wbmri imaging of the small joints of the hands and feet , before the method is ready for routine use . dynamic contrast - enhanced mri ( dce - mri ) is based on the perfusion dynamics of synovial enhancement curves after contrast injection and has been found to correlate with synovial histopathological inflammation ( fig.5 ) [ 13 , 14 ]  . 
it involves no ionizing radiation or risk of malignancy , with the major contraindications being claustrophobia or the presence of any metal devices including pacemakers or clips ( though many of these are now made mri safe )  . 
the european society of urogenital radiology ( esur ) guidelines recommend no patients should be denied a well - indicated gd - enhanced mri , and those agents with highest stability ( lowest risk of nephrogenic systemic fibrosis ) ( e.g. , macrocyclic gd chelates , such as gadoterate meglumine and gadoteridol ) should be used , at the lowest diagnostic dose [ 20 ]  . mri detection ofpathology inra the clinical value of mri in ra relates primarily to its ability to evaluate the wrists , hands and feet in high detail , which is also the main focus of this section . 
mri is also useful for evaluating other anatomical sites involved by ra , such as the knees , hips , elbows and shoulders , and the axial skeleton , particularly the cervical spine . 
comparisons with miniarthroscopy and histopathological findings have documented that mri synovitis , as determined by gd - enhanced t1 - weighted mri , reflects true synovial 1 3 1132 la radiologia medica ( 2019 ) 124 : 11281141 fig . 
from left to right : coronal t1w non - fat - saturated spin echo , coronal stir , coronal 3d gradient echo fat - saturated post - contrast vibe sequence and coronal dce - mri analyzed with dynamika , image analysis group , london , uk . 
 note the severe bme on the initial stir and the moderate - to - severe synovitis ( bright enhancing tissue ) on the 3d vibe sequence as well as the high perfusion / inflammation in the dce - image ( seen as bright and white colors )  . 
this is associated with a significant reduction in the bme on the stir , a slight reduction in contrast enhancing synovitis on the vibe sequence , and a significant reduction in the perfusion in the enhancing synovium , seen as more dark red colors on the dce - mri inflammation [ 13 , 14 , 18 , 22 ]  . 
diagnostic tests are never 100% sensitive or specific , and thus , the inherent trade - off between false - negative and false - positive rates as one increases the positivity criterion for that test must be considered carefully in light of the particular role that imaging is being asked to play . 
the tendon itself may appear normal , or it may be thickened , irregular and / or have increased signal intensity within the tendon on t2w / pdw and stir images ( tendonitis ) , or with complete or incomplete tears [ 28 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 11281141 1133 table 1 definitions of important ra joint pathologies [ 4 ] synovitis : an area in the synovial compartment that shows above - normal post - gadolinium enhancement ( signal intensity increase ) of a thickness greater than the width of the normal synovium mri bone erosion : a sharply marginated bone lesion , with correct juxtaarticular localization and typical signal characteristics * , which is visible in two planes with a cortical break seen in at least one plane * * * on t1 - weighted images : discontinuity of the signal void of cortical bone and loss of normal high signal intensity of bone marrow fat . 
rapid post - gadolinium enhancement suggests presence of active , hypervascularized pannus tissue in the erosion * * other focal bone lesions and variations of normal anatomy must obviously be considered , but are generally distinguishable with associated mri osteitis / bone marrow edema : a lesion * within the trabecular bone , with ill - defined margins and signal characteristics consistent with imaging and clinical findings increased water content * * * may occur alone or surrounding an erosion * * high signal intensity on t2 - weighted fat saturation or stir images and low signal intensity on t1 - weighted images mri joint space narrowing : reduced joint space width compared to normal , as assessed in a slice perpendicular to the joint surface mri tenosynovitis : peritendinous effusion * and / or tenosynovial post - contrast enhancement * * , seen on axial sequences over 3 consecutive * high signal intensity on t2 - weighted fat - saturated / stir images * * enhancement ( signal intensity increase ) is judged by comparison with t1 - weighted images obtained before and after i.v. 
gadolinium - contrast slices bone marrow edema bone marrow edema ( figs.3 , 4 ) , i.e. , the presence of mrisigns of increased water in the bone marrow compartment , is frequently detected in ra . 
whereas erosions reflect bone damage that has already occurred , bme appears to represent the link ( forerunner ) from joint inflammation to bone destruction where persistent osteitis leads to trabecular bone loss and an erosion [ 3234 ]  . enthesitis agreement for detection of bone erosions in ra wrists and mcp - joints between mri and ct , the gold standard reference for detection of bone damage , provides evidence that mri erosions represent true bone damage [ 43 , 44 ]  . erosions are also frequently seen in other inflammatory arthritidies and erosive oa and are thus not specific for ra . 
 small erosion - like lesions can also be visualized in healthy controls and oa [ 25 , 26 ] , so to avoid overestimation , using strict definitions of bone erosion and other pathologies is essential . 
as an example , bone erosions should be visible in two planes , with a cortical break visible in at least one plane to be registered ( fig.4 ) , and the normal anatomy and pitfalls should be kept in mind [ 21 , 45 , 46 ]  . 
cartilage assessment in small joints requires high image quality and resolution , but reliable semi - quantitative assessment systems have been developed [ 3739 ]  . bone erosion bone erosion ( fig.4 ) is detected with higher sensitivity with mri than radiography [ 4042 ] , and the very high level of all joints , tendons and ligaments of the cervical spine can be involved in ra , leading to spine instability or subluxations . 
the primary imaging modality is cr , but mri can provide detailed information on bone and soft - tissue abnormalities , e.g. , the pannus tissue around the odontoid process , and this can be a valuable supplement to radiographic evaluation ( fig.7 ) [ 2 , 48 , 49 ]  . 
mri erosions of the atlas and reduced subarachnoid space are associated with subsequent clinical neurological dysfunction [ 50 ] , and cord compression on mri better predicts subsequent clinical deterioration than initial clinical and radiographic features [ 51 ]  . 
a mid - sagittal 3d ct reformat of the cervical spine shows degenerative spine changes on multiple cervical levels as well as block vertebrae between c4 and c5 with approximately 5mm anterolistesis between c3 and the block vertebrae . 
bd corresponding mri of the same mid - sagittal slice , b t1 weighted image without fat saturation , c t2 - weighted image without fat saturation and d stir image showing capsular hypertrophy , small erosions in the c1 / c2 articulation and slight bone marrow edema of dens axis on the stir sequence ( arrow heads )  . 
e a lateral right - sided 3d ct sagittal reformat at the level of the articulation between massa lateraris and axis c2 showing severe erosive changes in the articulation between massa lateralis of c1 and c2 ( arrowheads ) along with degenerative changes of the upper cervical facet joints ( arrows )  . 
fh corresponding mri of the same right - sided sagittal slice , f t1 - weighted image without fat saturation , g t2 - weighted image without fat saturation and h stir showing destruction of the right - sided articulation between massa lateralis c1 and axis c2 ( arrowheads ) as well as severe bone marrow edema of the adjacent bone of the articulation on the stir sequence h ( arrows )  . 
facet joint degeneration is also noted ( open arrows ) for the use of imaging in ra clinical management state that monitoring of functional instability of the cervical spine by lateral radiograph obtained in flexion and neutral should be performed in patients with clinical suspicion of cervical involvement . 
furthermore , eular recommends that mri should be performed when the radiography is positive or specific neurological symptoms and signs are present [ 2 ]  . diagnosis longitudinal studies of undifferentiated arthritis have documented an independent predictive value of mri in the subsequent diagnosis of ra [ 52 , 53 ]  . 
in patients with undifferentiated arthritis , a prediction model , including clinical hand arthritis , morning stiffness , positive rheumatoid factor and mri bone edema score in metatarsophalangeal and wrist joints , correctly identified the development of ra or non - ra in 82% of patients [ 53 ]  . 
in another study of undifferentiated arthritis , assessment of mri tenosynovitis was helpful in predicting future ra diagnosis or disease - modifying antirheumatic drugs therapy initiation [ 54 ]  . in the acr / eular 2010 criteria for ra [ 55 ] , classification as definite ra is based on the presence of definite clinical synovitis ( swelling at clinical examination ) in 1 joint , absence of an alternative diagnosis that better explains the synovitis and achievement of a total score 6 ( of a possible 10 ) from the individual scores in four domains . 
t1 - weighted mid - sagittal mri of cervical spine ( c ) and corresponding t2 - weighted mid - sagittal image ( d ) in the same patient as ( b ) show capsular hypertrophy and erosions in the top of dens axis ( c2 , arrows ) specific for ra , and the acr / eular criteria are classification not diagnostic criteria . 
in the diagnostic process of the individual patient in routine clinical practice , it is important always to consider the clinical context ( as with any other diagnostic test ) to avoid over - diagnosis , since mri findings are not pathognomonic . 
the eular recommendations also state that when there is diagnostic doubt , cr , ultrasound or mri can be used to improve the certainty of a diagnosis of ra above clinical criteria alone . 
the recommendations also state the presence of inflammation seen with ultrasound or mri can be used to predict the progression to clinical ra from undifferentiated inflammatory arthritis [ 2 ]  . monitoring disease activity andstructural damage clinical trials andobservational cohorts to be valuable for monitoring joint inflammation and destruction , a method must be truthful , reproducible and sensitive to change . 
several randomized controlled trials have documented the superior ability of mri to discriminate the effects of different therapies in inhibiting progressive structural bone and cartilage damage [ 38 , 6163 ]  . 
the omeract erosion score is closely correlated with erosion volumes estimated by mri and ct [ 64 ]  . due to the high responsiveness and discriminatory ability , and because mri has demonstrated criterion validity for osteitis and synovitis with histology and construct validity for erosions when compared with ct , there has been a rapid increase in the use of mri in ra randomized clinical trials over the past decade . 
a report by the imaging subcommittee of the american college of rheumatology ( acr ) clinical trials task force [ 65 ] concluded that mri met the omeract validation filter for truth , discrimination and feasibility [ 66 ] and that mri best serves the purpose of achieving sensitive ascertainment of structural damage in rcts while also providing objective measures 1 3 1136 la radiologia medica ( 2019 ) 124 : 11281141 fig . 
a , b two sagittal 3d ct reformats show degenerative spine changes on multiple cervical levels as well as a block vertebra between c4 and c5 with approximately 5mm anterolistesis between c3 and the block vertebrae . 
c coronal reformat shows erosions in the left part of the dens axis ( black arrowhead ) , and there are severe erosive changes in the articulation between massa lateralis of c1 and c2 on the right side . 
e axial slice at the level of the articulation of the neck of dens axis ( * ) , in the plane corresponding to the black dotted line in c . 
white arrowheads point at severe erosive changes in the articulation between massa lateralis of c1 and c2 on the right side also seen in c of inflammatory predictors of damage [ 65 ]  . 
quantitative methods , like dynamic mri ( fig.5 ) and quantitative volume determination of synovitis , bme and erosion based on supervised machine learning techniques may also prove useful for early treatment - induced changes in joint inflammation [ 15 , 19 ]  . 
all these methods are used in clinical trials but require further validation before clinical use can be recommended . routine clinical practice the eular recommendations state that us and mri are superior to clinical examination in the detection of joint inflammation ; these techniques should be considered for more accurate assessment of inflammation [ 2 ]  . 
however , important questions remain about when such imaging is needed and when it is cost - effective to do ? there is a lack of studies to document exactly how mri should be used for this purpose , e.g. , imaging is not needed to assess disease activity if the patient has obvious clinical signs of active ra . 
for assessment of inflammation in the bone ( osteitis ) , mri is currently , however , the only available modality , and it is also the best method , except for computed tomography ( ct ) , for monitoring of progression of erosions [ 30 , 31 , 4244 , 67 , 68 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 11281141 predicting disease outcome the predictive value of mri - detected pathology in wrist and / or mcp joints for subsequent radiographic progression in bilateral hands , wrists and feet is well established . 
regression analyses in 3and 5 - year follow - up in two cohorts and in clinical trials have documented that mribone edema is a strong predictor of short - term and long - term ( 3 , 5 and 11year ) radiographic progression [ 7174 ]  . thus , mri in early ra is a useful method to predict patients with potentially worse outcomes , which may assist the clinician in the choice of treatment strategy . 
in agreement with this , the eular recommendations for the use of imaging in the clinical management of ra state mri bone edema is a strong independent predictor of subsequent radiographic progression in early ra and should be considered for use as a prognostic indicator [ 2 ]  . 
this indicates that the presence of bme could be used as an inclusion criterion in clinical trials to enrich the study population for patients with high risk of structural progression . utility inclinical remission another issue of high clinical importance is whether mri is useful to predict the disease course in patients in clinical remission . 
mri synovitis and bme are found frequently in patients in clinical remission [ 75 , 76 ] , and these findings are significantly related to subsequent progressive structural damage [ 7779 ]  . 
these encouraging results are acknowledged in the eular recommendation , which states that mri and us can detect inflammation that predicts subsequent joint damage , even when clinical remission is present [ 2 ]  . mri may assist in predicting the success of tapering of biologics . 
in a cohort of routine care ra patients in sustained remission on biological disease - modifying antirheumatic drugs ( bdmards ) , the bdmard therapy was tapered according to a predefined treatment guideline . 
successful tapering was independently predicted by 1 previous bdmard , male gender , low baseline mri combined inflammation score ( synovitis , tenosynovitis and bone marrow edema ) and / or combined damage score ( erosion and joint space narrowing ) [ 80 ]  . 
the available data encourage further exploration of mri for predicting the disease course and for evaluating disease status , including defining remission . computed tomography although still limited in soft - tissue contrast , conventional ct offers fast and reliable acquisition , high resolution 1137 and multiplanar capabilities that have promoted its use in recent years . technical aspects ct image acquisition is no longer restricted to the axial plane , and its multiplanar capability is now so pronounced that many ct scans of the body are now interpreted primarily from thin - slice coronal or sagittal reconstructions in the same way as mri . 
while this is not a problem with the more distal extremities as the exposure doses are smaller and the tissue more radiation resistant , it remains an issue for spine , hip and shoulder ct . 
consequently , in most routine clinical situations , radiography provides sufficient information of a similar nature to ct for clinical decision making and x - ray is cheaper than ct and readily available ; ultrasonography is a better and cheaper way to visualize and quantify superficial softtissue pathology ; and mri offers superior soft - tissue contrast and bone marrow imaging . 
however , the technology continues to evolve and low - dose ct ( ldct ) is becoming more common with iterative reconstruction techniques which reduce the radiation exposure by about 80% [ 81 ]  . 
 exposure dose from ldct of the sacroiliac joints is similar to radiography and should probably replace radiography as a first - line test in many cases [ 82 ]  . ldct can quantify bone formation in the spine which is undetectable with radiography [ 83 ] , and cone - beam ct is a new technology that can detect bone erosion in extremities at extremely low dose [ 84 ]  . dual - energy ct ( dect ) allows the separation of calcium containing bone from the soft - tissue components , thereby allowing detection of soft - tissue changes that were previously invisible with ct . 
for example , it has recently been reported that dect can detect bone marrow edema ( bme ) with good reliability even in the small bones of the wrist in patients with ra [ 85 , 86 ]  . dect can also be used for analysis of composition of some specific tissues , most particularly urate crystals which can be detected in bone and soft tissues ( see below )  . 1 3 1138 ct inra the excellent contrast between bone and soft tissue makes ct a gold standard reference for the detection of bone damage , including erosion in ra . 
modern ct with isotropic voxel acquisition and three - dimensional visualization allows accurate detection and quantification of bone erosion with good intra - observer agreement , whereas radiography is limited by its two - dimensional projection and superimposition of structures . 
however , ct is very limited in ability to visualize soft - tissue changes and even with contrast enhancement and complex subtraction techniques ; ct is still inferior to mri and ultrasound for assessment of synovial changes such as thickening and hyperemia . 
detection of erosion on ct and mri shows very good agreement although ct is slightly more sensitive [ 43 , 67 ]  . diagnosis , monitoring andprognostication ct is not currently used in routine clinical practice for the diagnosis of ra . 
ct is used for problem solving in specific cases such as examination of the cervical spine if mri is unavailable or contraindicated . ct may potentially be useful for longitudinal assessment of damage progression [ 67 , 87 ] , and ct can detect and quantify repair of erosion [ 88 ]  . 
no ct data are available for prognostication in ra , and current use of ct in ra is very limited but since it has been shown to detect erosion reliably [ 89 ] , scoring systems are in development [ 90 ]  . conclusion mri is a sensitive imaging modality which has documented utility in diagnosis , monitoring and prognostication of patients with ra , and important new knowledge and technical improvements are continuously being acquired . 
several questions regarding the optimal use of these imaging modalities in routine practice and in clinical trials still need to be scientifically explored . compliance with ethical standards conflict of interest m has received speaker / consultant fees from abbvie , bms , boehringer - ingelheim , celgene , eli lilly , hospira , janssen , merck , novartis , novo , orion , pfizer , regeneron , roche and la radiologia medica ( 2019 ) 124 : 11281141 ucb , and research grants from abbvie , celgene , centocor , merck , and novartis . 
mb is a shareholder of image analysis group and serves as a consultant to image analysis group , eli lilly , esaote , celgene , pfizer , abbvie , carestream / canon , siemens and astrazeneca . ethical standards the manuscript does not contain clinical studies or patient data . 
this article does not contain any studies with human participants or animals performed by any of the authors . la radiologia medica ( 2019 ) 124 : 10671070 editorial musculoskeletal imaging oftheinflammatory anddegenerative joints : current status andperspectives faustosalaffi1 marinacarotti2 antoniobarile3 received : 22 january 2019 / accepted : 11 february 2019 / published online : 27 february 2019 italian society of medical radiology 2019 this special issue of la radiologia medica focuses on the broad spectrum of musculoskeletal imaging , ranging from essential concepts for inflammatory ( rheumatoid arthritis , spondyloarthritis , gout , and other crystal - induced arthropathies ) , noninflammatory ( osteoarthritis , algoneurodystrophy ) to multisystem and general pathologic conditions ( such as large - vessel vasculitis ) [ 1 ]  . 
musculoskeletal radiology continues to evolve rapidly , benefiting from advances as continually improving magnets , sequences in magnetic resonance imaging ( mri ) as well as the broader application of plain radiographs , ultrasonography ( us ) , and computed tomography ( ct ) , or dual - energy ct ( dect ) to the musculoskeletal system [ 2 ]  . 
the articles included in this focused issue have been compiled with a goal to provide a valuable resource for residents , fellows , and practicing radiologists and rheumatologists in the scope of a shared interpretation of musculoskeletal imaging examinations . 
both specialties have a duty to use imaging cost - effectively , to provide the requisite clinical information on diagnosis , prognosis , and serial assessment with the least risk and inconvenience to the patient . 
radiographic progression is one of the most important outcome measures in ra and psa clinical trials , because it reflects historical disease activity , is associated with loss of function over time , and can be reliably assessed [ 3 ]  . 
the various scoring systems for the two diseases are detailed in this issue . the potential applications of us in rheumatology have been further increased with the dawn of the third generation us machines , equipped with very high - frequency probes ( > 10mhz )  . 
these can reach a spatial resolution of less than a tenth of a millimeter and make it possible to study the finest details of the smaller joints and hand tendons which are involved early on in ra [ 58 ]  . 
in their article , ultrasound imaging in rheumatoid arthritis , emilio filippucci , md , and colleagues at the rheumatological clinic , universit politecnica delle marche , ancona ( italy ) , provide an overview of the main studies focusing on the value of us in the assessment of the patients with ra , and discussing the elementary lesions detectable by us ( synovitis , bone erosion , cartilage damage , tenosynovitis , and tendon damage ) , the scoring systems currently available , and the scanning protocols in definite clinical settings ( undifferentiated arthritis , early and long - standing ra )  . several sonographic abnormalities may be also observed in patients with osteoarthritis ( oa ) [ 9 ]  . 
federico bruno , md , and colleagues at the department of biotechnology and applied clinical sciences , university of laquila , laquila ( italy ) , in the article new advances in mri diagnosis of degenerative osteoarthropathy of the peripheral joints , provide an overview of the recent applications of advanced mri techniques for the evaluation of degenerative joint changes ( notably affecting the articular cartilage ) that could have a great potential in the early diagnosis and treatment monitoring . while conventional radiography and us remain a mainstay in rheumatology , mri and ct have become increasingly common in patient care . 
efficient methods for diagnosis , monitoring , and prognostication are essential in early ra [ 13 , 14 ]  . mikkel stergaard , md , ph.d. , and colleagues at the center for rheumatology and spine diseases , rigshospitalet , glostrup , and the department of clinical medicine , university of copenhagen , copenhagen ( denmark ) , focused on the potential uses of mri and ct in the clinical management of patients with suspected or definite ra in the article imaging in rheumatoid arthritis : the role of magnetic resonance imaging and computed tomography . 
 after sections on technical aspects , it described the current knowledge on mri and ct for early detection of ra manifestations , diagnosis of ra , monitoring of disease activity and joint damage progression , and its role in determining prognosis . sacroiliac ( si ) joints involvement is a crucial feature of inflammatory spondyloarthropathies , and mri is the gold standard imaging modality to detect si pathology [ 1518 ]  . 
maria antonietta mazzei , md , and colleagues at the department of medical , surgical and neuro sciences , diagnostic imaging , university of siena ( italy ) , in their article magnetic resonance imaging of the sacroiliac joints in spa : with or without intravenous contrast media ? , discuss the different mr imaging modalities and strategies available for the assessment of inflammatory involvement of the si joints , with a particular focus on the advantages and limits in the use of intravenous contrast media . despite the recognized fundamental role of mri in inflammatory joint pathologies , as previously discussed , mr imaging findings in clinical diagnostic criteria often lack specificity , giving potential diagnostic issues especially in the differential diagnosis with degenerative alterations [ 1820 ]  . 
to further explore this topic , in the contribution mri of the axial skeleton : differentiating non - inflammatory disease and axial spondyloarthritis a review of current concept and applications , ernesto la paglia , md , and colleagues at the department of radiology , ospedale ss . 
antonio e biagio e cesare arrigo , alessandria ( italy ) , discuss the main mri signs and the possible differential diagnoses , to improve the diagnostic performance in inflammatory spondyloarthropathies . although the role of imaging in the diagnosis , staging , and disease monitoring has been well established [ 21 ] , several anatomical variants and imaging artifacts can show unusual appearance , leading to possible diagnostic pitfalls [ 22 , 23 ]  . 
marcello zappia , md , and colleagues at the dipartimento di medicina e di scienze della salute vincenzo tiberio , universit del molise , campobasso ( italy ) , with their contribution diagnostic imaging pitfalls in rheumatology , illustrate the possible imaging pitfalls encountered in the imaging of inflammatory joint pathologies , and the available tips and tricks to recognize them . with the assistance of innovations in scanner engineering and software design , dual - energy ct ( dect ) is a recently developed advanced imaging method in the last decade . 
the principal advantages of dect over conventional ct in the musculoskeletal setting relate to the additional information provided regarding tissue composition , artifact reduction , and image optimization [ 2426 ]  . 
marina carotti , md , and colleagues at the radiology department , universit politecnica delle marche , ancona ( italy ) , focus on applications of dect to musculoskeletal imaging including gout and other crystal - induced arthropathies , virtual non - calcium images , and the study of bone marrow lesions in the application of dual - energy computed tomography in the diagnosis of musculoskeletal disordersa review of current concepts and applications . the next portion of this monograph is dedicated to multimodality musculoskeletal imaging . 
where are we now ? , marwin gutierrez , md , and colleagues at the instituto nacional de rehabilitacin , mexico city , and rheumatology section , center of excellence of rheumatology , mexico city ( mexico ) , provide an overview of the role of us in the assessment of ild in rheumatic disorders and discuss the current evidence supporting its clinical application in daily clinical practice . lvv is the most common form of primary vasculitis comprising giant cell arteritis ( gca ) , takayasu arteritis ( tak ) , and idiopathic aortitis ( ia ) [ 31 , 32 ]  . 
early diagnosis and treatment of lvv are paramount to reduce the risk of ischemic complications such as visual loss and strokes , vascular stenosis and occlusion , and aortic aneurysm formation . 
use of imaging modalities ( us , mri , ct , and [ 18f ] - fluorodeoxyglucose positron emission tomography ( pet ) ) has steadily increased to enable assessment of cranial and extracranial arteries , as well as the aorta . 
key concepts underlying lvv are covered in the article eular recommendations for the use of imaging in large vessel vasculitis in clinical practice by mohammad bardi , md , and colleagues at the department of rheumatology , university of british columbia ( canada ) , that summarizes the current evidence of imaging in patients with or suspected of having lvv and highlights the clinical implications of the eular recommendations . as guest editors , we hope that this monograph issue provides residents , fellows , and practicing radiologists and rheumatologists with a strong foundation for interpreting multimodality musculoskeletal imaging studies . 
these include quantitative analysis and several compositional techniques ( t1 and t2 relaxometry measurements and mapping , sodium imaging , delayed gadolinium - enhanced mri of cartilage dgemric , glycosaminoglycan - specific chemical exchange saturation transfer gagcest , diffusion - weighted imaging dwi and diffusion tensor imaging dti )  . 
these compositional mri techniques may have the potential to serve as quantitative , reproducible , noninvasive and objective endpoints for oa assessment , particularly in diagnosis of early and pre - radiographic stages of the disease and in monitoring disease progression and treatment effects over time . keywords mri cartilage advanced imaging t2 mapping dwi introduction degenerative osteoarthritis ( oa ) of the peripheral joints is a leading cause of musculoskeletal - related morbidity and disability in the western world [ 15 ]  . 
the pathological process of oa influences different articular structures , but the degeneration of articular cartilage represents the * antonio barile antonio.barile@cc.univaq.it 1 department ofbiotechnological andapplied clinical sciences , university oflaquila , via vetoio 1 , 67100laquila , italy 2 department ofprecision medicine , university ofcampania luigi vanvitelli , naples , italy 3 department life andhealth v . 
tiberio , university ofmolise , campobasso , italy 4 department ofradiology , scientific institute casa sollievo della sofferenza hospital , university offoggia , foggia , italy 5 department ofradiology , ospedali riuniti , universit politecnica delle marche , ancona , italy primum movens in the pathogenic phases of the disease . 
magnetic resonance imaging ( mri ) , due to its excellent soft tissue contrast resolution , is the preferred imaging tool for the evaluation of different diseases affecting the musculoskeletal system , both for diagnostic and interventional purposes [ 1126 ]  . 
in the last years , several advanced mr imaging sequences and techniques were developed to provide a global , sensitive and specific assessment of the joint degenerative processes with semiquantitative , quantitative and compositional analysis methods [ 30 , vol . : ( 0123456789 ) 1 3 1122 la radiologia medica ( 2019 ) 124 : 11211127 31 ]  . 
in this article , we review the recent advances in mri techniques and analysis to assess degenerative articular changes in the peripheral joints . applications andresults semiquantitative analysis semiquantitative mr scoring systems are based on the global morphological evaluation of pathological changes ( e.g. , alterations of articular cartilage , subchondral bone , fibrocartilages ) that affect the functional and structural joint integrity and determine the severity of the disease [ 32 ]  . 
four scoring systems were established for the knee : the whole organ magnetic resonance score ( worms ) , the knee osteoarthritis scoring system ( koss ) , the boston - leeds osteoarthritis knee scoring ( bloks ) and the moaks ( mri osteoarthritis knee score )  . 
concerning the method , in brief , the joint is divided into several articular compartments / subregions ( e.g. , medial and lateral tibia , medial and lateral femoral condyle ) , and several joint features ( e.g. , cartilage signal and morphology , synovitis , subchondral bone ) are analyzed and scored according to the severity of the involvement ( fig.1 ) [ 34 ]  . numerous studies validated the reproducibility of these scoring systems ; the moaks is currently the most used one for the knee , bringing together the advantages of all scoring systems [ 35 ]  . 
the clinical value of semiquantitative analysis was demonstrated by the presence of some specific alterations ( such as hoffa synovitis , joint effusion , medial meniscus lesions ) being associated with an increased risk of oa radiographic progression . 
other studies , using these methods for transversal and longitudinal comparisons of the disease evolution , highlighted how the presence of cartilage damage and the presence of subchondral edema correlate with an increased risk of prosthetic surgery [ 10 , 32 , 33 , 3540 ]  . quantitative evaluation quantitative assessment with mri provides a more sensitive and specific assessment of the degree of cartilage degeneration and is superior to semiquantitative techniques to evaluate structural changes [ 38 , 39 , 41 ]  . technique three - dimensional ( 3d ) , high - resolution sequences are required to image the bonecartilage interface and the cartilage surface with adequate contrast . 
this allows extracting data sets and image reconstructions to evaluate several quantitative features ( e.g. , cartilage thickness , area , volume ) as continuous variables [ 31 , 33 , 42 ]  . applications andresults studies on quantitative cartilage evaluation showed good inter - operator reproducibility at different degrees of cartilage degeneration and excellent correlation with the surgical and histological findings . 
quantitative methods have a good correlation with semiquantitative results , even if more sensitive and specific in predicting cartilage loss ( especially in small widespread defects using regional analysis ) ; for these reasons , some authors suggest a combined use of the techniques [ 31 , 3335 , 38 , 39 , 4144 ]  . 
changes in cartilage volume and thickness were used as an outcome in observational studies and trials of pharmacological treatments ( e.g. , chondroitin sulfate ) , physical therapy and rehabilitation , and surgical treatments . 
the need for dedicated software and the timeconsuming analysis is still considered a major disadvantage to the routine clinical application [ 5 , 30 , 40 , 4548 ]  . compositional analysis articular cartilage is made of chondrocytes , spersed within a matrix composed of water and a highly organized network of collagen proteoglycans ( pgs ) and glicosaminoglycans ( gags )  . 
notably , these matrix changes , however , are not apparent on standard morphological mri sequences in the early stages of oa development [ 9 , 31 , 45 , 48 , 49 ]  . 
based on the knowledge of the pathogenesis of joint degenerative processes , we know that at the histological level the biochemical changes in cartilage ultrastructure , including the reduction of proteoglycans ( pgs ) and glycosaminoglycans ( gags ) and the increase in water content , precede morphological changes . 
in particular , mr imaging techniques are based on the modification of one or more cartilaginous ultrastructural components ( e.g. , gag , pg ) [ 40 , 50 ]  . 
these techniques include the measurement of relaxation times ( t2 and t1rho mapping ) , the sodium imaging , the delayed gadolinium enhancement mri of cartilage ( dgemric ) imaging , the chemical exchange saturation transfer imaging of gag ( gagcest ) imaging and the diffusion imaging ( dwi and dti ) [ 30 , 40 , 42 , 45 , 48 , 49 , 51 ]  . techniques t2 andt1 mapping these sequences measure the t1 and t2 relaxation times ( expressed in ms ) of the molecules present at the tissue level . 
the relaxation time of t2 is measured as a function of the signal measured in multi - echo se and fse t2 - weighted images with mono or multi - exponential decay curve at the different echo times ( te ) [ 42 , 5255 ]  . t1 mapping is a compositional technique sensitive to regional changes in cartilage matrix proteoglycans fig . 
on the right , quantitative analysis through the positioning of regions of interests ( roi ) shows t2 relaxation times in the normal value range 1 3 1124 la radiologia medica ( 2019 ) 124 : 11211127 fig . 
t2 mapping color map b clearly depicts the same area in red , and quantitative analysis c confirms higher t2 relaxation time values , consistent with collagen degradation and thus chondropathy characterized by continuous resonance rf pulse . 
the main disadvantages are represented by issues related to high sar ( due to the application of long - lasting rf pulses ) and long acquisition times [ 42 , 45 ]  . a fundamental advantage of relaxation mapping sequences is that contrast medium administration is not necessary . 
in addition to dwi , diffusion tendon imaging ( dti ) can also be applied to cartilage imaging , evaluating the fractional anisotropy as a parameter of water diffusion in various spatial orientations . 
similar to other compositional sequences , diffusion and tensor parameters correlate with the collagen and proteoglycan content within the cartilage matrix and can be used as quantitative markers of cartilage degeneration . 
the loss of collagen and proteoglycan can lead to significant increases in mean diffusion ( fig.4 ) [ 40 , 42 , 43 , 49 , 51 , 55 ]  . sodium imaging ( 23na ) this compositional imaging technique is based on the detection of sodium , the positive cation linked to the negatively charged glycosaminoglycan ( gag ) of the cartilage matrix . 
axial dwi sequence b with adc map c confirms altered cartilage matrix with increased diffusion values 1 3 la radiologia medica ( 2019 ) 124 : 11211127 1125 more specifically , the concentration of sodium within the cartilage matrix is directly correlated with the concentration of gag and therefore proteoglycan . 
however , one of the limits of invivo sodium imaging of cartilage is the low intrinsic snr , caused by the low 23na mri signal compared to the one from protons [ 30 , 40 , 42 , 43 , 45 , 49 ]  . delayed gadolinium enhancement mri ofcartilage ( dgemric ) increasingly important in studies of cartilage degeneration and in testing new therapies for prevention or delaying the progression of oa , due to the recent widespread development of disease - modifying drugs and regenerative therapies ( e.g. , platelet - rich plasma , hyaluronic acid , chondrocyte implantation ) [ 5661 ]  . 
as the efficacy is closely connected with the early establishment of treatment , their use requires suitable biomarkers to provide an early diagnosis and detect signs of progression during treatment [ 62 ]  . 
advanced mri findings can represent , in this scenario , a powerful tool to understand how to best treat and manage oa and possibly will allow making a target - based therapy for every single component of the cartilage matrix [ 6366 ]  . for this imaging method , the administration of contrast medium ( gadolinium ) , injected intravenously , is necessary . 
 gadolinium is negatively charged and is rejected by positively charged gags in cartilage , while in the case of cartilage matrix degradation , the amount of contrast in cartilage tissue will be increased in an inversely related manner . 
the dgemric technique showed high sensitivity and specificity ; the routine clinical use is limited by the need for high doses of gadolinium [ 40 , 42 , 45 , 46 , 49 , 51 ]  . chemical exchange saturation transfer imaging ofgag ( gagcest ) this sequence is based on the constant transfer of labile protons between solutes ( in the case of cartilage , gags ) and water . 
the proton transfer between water molecules and the one between water and gag are different , and the difference between waterwater transfer and watergag transfer is measured as the magnetic transfer ratio . 
unfortunately , strong magnetic fields ( 7t scanners ) are required to obtain sufficient signal , thus widespread use , even in the research field , is currently limited [ 42 , 45 , 49 ]  . conclusion advanced imaging mri techniques for the study of joint degenerative pathology represent a particularly promising field of research , which has seen significant developments in recent years . 
in particular , we revise the general aspects common to most procedures and the different imagingguided interventions which can be performed around joints , soft tissues , and spine . keywords interventional radiology ultrasound musculoskeletal system tendinopathy osteoarthritis introduction imaging - guided interventional procedures have become increasingly popular in the treatment of several pathologic conditions in the musculoskeletal systebesides oncological treatments , musculoskeletal procedures can be performed to treat differentdegenerative or inflammatory conditions . according to the anatomical location to reach , interventional procedures can be guided using ultrasound , fluoroscopy , computed tomography ( ct ) , or occasionally magnetic resonance ( mr ) [ 1 ]  . 
ultrasound has certainly the great advantage of being cheap , quick , available , real time , and radiation - free and is excellent to perform interventional procedures in the soft tissues [ 24 ]  . 
however , ultrasound may be occasionally limited by deep anatomical location of the * luca maria sconfienza io@lucasconfienza.it irccs istituto ortopedico galeazzi , via riccardo galeazzi 4 , 20161milano , italy 2 s.c. 
diagnostica perimmagini ed ecografia interventistica , ospedale evangelico internazionale , 16121genova , italy 3 dipartimento di scienze biomediche perla salute , universit degli studi di milano , 20100milano , italy 4 department ofinterventional radiology , university hospital ofstrasbourg , 67000strasbourg , france 5 dipartimento di radiologia interventistica , istituto europeo di oncologia irccs , 20100milano , italy area to treat or by the interposition of bony cortex , which does not allow ultrasound beam penetration . 
fluoroscopy and ct are more useful for procedures involving the bone , with the former more useful when longitudinal precision and real - time visualization are needed and the latter preferred when axial precision is required . 
 last , mr is theoretically ideal to guide procedures in the musculoskeletal system , as it combines most of the advantages of all other modalities ; however , the limited diffusion of dedicated magnets and high costs have remarkably limited its application in clinical practice . in the setting of degenerative and inflammatory conditions , interventional procedures can be used to perform joint injections or aspirations and procedures in or around tendons and bones . 
this paper is aimed to review clinical indications and technical aspects of these kinds of procedures . general aspects some aspects should be considered when performing interventional procedures in the musculoskeletal system : disinfection : all procedures should be performed under strict sterile conditions . 
sterile material ( gloves , draping , probe covers for ultrasound procedures ) should be used to ensure the best sterility possible in the operatvol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 11121120 1113 ing environment . 
accurate skin disinfection should also be achieved using specific antiseptic solutions ( e.g. , iodineor chlorhexidine - based solutions ) ; substances to inject : according to the disease to treat , different substances can be injected . 
theycan be particulate ( e.g. , triamcinolone acetonide , with lower solubility and longer duration of action ) or non - particulate ( e.g. , dexamethasone , with shorter duration of action )  . 
steroids are not contraindicated in diabetic patients , who should expect only a transient , non - clinically significant increase in glycemia ; however , an increased risk of infections should be considered in these patients . 
 blood products ( such as platelet - rich plasma [ prp ] or autologous blood ) have the purpose of delivering in the selected site growth factors contained in platelets . 
it is commonly used for bone procedures , such as vertebroplasty and kyphoplasty . patients positioning : the patient should be positioned according to the area to treat , so standardization cannot be done . 
however , for procedures other than simple injections , we recommend having the patient laying down on the examination bed to avoid the occurrence of vasovagal reactions ; ultrasound guidance : when performing ultrasoundguided procedures , the needle can be inserted with two different approaches with respect to the ultrasound bea more commonly , the in - plane modality is used , which implies that the needle is inserted perpendicularly and on the same plane of the ultrasound beam ( i.e. , needle is inserted oblique from the short side of the probe )  . 
in some cases , however , the out - of - plane approach might be preferred , which implies that the needle is inserted almost parallel to the ultrasound beam ( i.e. , needle inserted almost vertical on the long side of the probe )  . 
this approach requires greater experience , as only the needle tip is visualized , but is helpful in those cases where joint or peri - tendinous space is limited or when lateral access is precluded . post - procedure care : in case of simple procedures performed on an outpatient basis , we generally ask the patient to remain in our department for about 30min of observation after treatment . 
other , more complex procedures require a longer hospital stay . joint procedures for all joint procedures , ultrasound should be the guidance modality of choice , as it has comparable accuracy to fluoroscopy , but it does not use ionizing radiations [ 1 ]  . 
according to each specific anatomical site , the joint should be positioned to maximize effusion visibility in the desired recess ( e.g. , humerus maximally externally rotated to squeeze anterior joint recess and inflate posterior recess )  . 
in degenerative conditions , aspiration of synovial fluid is usually performed prior to injection , with the purpose of eliminating the highest amount of synovial fluid in the joint , which may potentially interfere with the effect of the injectable . 
with the same technique , synovial biopsies can be performed to obtain tissue specimens to confirm or clarify a clinical diagnosis of inflammatory arthritis . needles should be chosen according to the specific joint . 
 for fluid aspiration , generally large - bore needles ( e.g. , 1618 gauge ) should be preferred , as they do not get obstructed by synovial tissue or intra - articular debris . 
longer spinal needles ( 9cm ) are preferred for deeper joints such as the hip , 1 3 1114 la radiologia medica ( 2019 ) 124 : 11121120 while standard length needles ( 45cm ) can be used in all other joints . 
we prefer to use 14 gauge semiautomatic tru - cut needles . for simple joint aspiration , local anesthesia is not generally required , as the stingy sensation induced by anesthesia injection is very similar to the little discomfort induced by the aspiration needle . 
of note , we do not recommend injecting anesthesia inside the joint to avoid interference with the potential bacterial load . injections intra - articular injections are generally performed to treat degenerative or inflammatory or conditions not responding to oral anti - inflammatory drugs . 
for longer term pain relief , ha and prp may be considered in patients with degenerative joint disease . soft tissue procedures drainage offluid collections superficial or deep fluid collections include abscesses , hematomas , or seromas and can be treated with imageguided percutaneous aspiration or drainage . 
abscesses may develop from surgical procedures , trauma , foreign bodies , or the spreading of contiguous or distant infections , while hematomas and seromas are usually caused by traumatic events or after surgical procedures [ 5 ]  . ultrasound is the modality of choice to guide aspiration or drainage of fluid collections . 
the direct puncture technique is generally preferred , although in some cases , the tube can be also inserted over a previously placed guide wire ( seldinger technique )  . 
 tube caliber ranges from 6 to 24 fr and is selected according to the thickness of the collected fluid ; accordingly , highly corpuscolated collections ( e.g. , hematoma ) need large caliber tubes ( 1624fr )  . prior to aspiration of hematomas , the degree of internal coagulation should be evaluated ; in particular , operators should rule out an active bleeding supplying the hematoma before puncturing it . 
in the end , if no signs of infection are noted , it is preferred not to drain the hematoma . ganglion aspiration soft tissue ganglia can occur around multiple joints throughout the musculoskeletal systethey are more frequent between 2040years of age [ 7 ] and are commonly encountered around the wrist , where they represent the most common benign soft tissue lesion [ 8 ]  . 
however , aspiration has been reported to be effective in up to 89% of cases [ 29 ] , although recurrence is frequent . due to the superficial location of ganglion cysts , the procedure is generally performed under us guidance with inplane or out - of - plane approach using a large - bore needle ( 1618 gauge )  . 
when the ganglion is completely drained , a small amount of steroid is generally injected into the cavity and a compression dressing is applied for a week to minimize the risk of recurrence . an example of ganglion aspiration is shown in fig.1. bursitis bursitis is a common reactive process characterized by thickening of the bursal walls in response to an external stimulus , which may be associated or not with increased fluid content [ 9 ]  . 
septic bursitis may also occur , being transcutaneous route the most common way of contamination [ 10 , 11 ]  . intra - bursal steroid or ha injection of aseptic bursitis is generally performed for therapeutic purposes when patients do not benefit from conservative treatment to reduce local inflammation and pain case of septic bursitis , bursal drainage is mainly indicated for diagnostic purposes and steroids should not be used , as they reduce local immunity [ 12 ]  . bursal injection is performed under us guidance , inserting a 2123 gauge needle in the bursa with an in - plane 1 3 la radiologia medica ( 2019 ) 124 : 11121120 1115 is the so - called calcific enthesopathy , and it should not be confused with calcific tendinopathy , which is a totally different entity [ 1525 ]  . histopathological evaluation reveals disordered proliferation of tenocytes , a small amount of physiologic collagen fibers , an increase of fibrous matrix , and often neovascularization [ 26 ]  . 
in the chronic phases ( at least 6months ) , inflammation may be absent , suggesting that the inflammation process is probably a trigger in the pathologic process [ 26 ]  . 
us findings include tendon thickening with fibrillary disorganization , ill - defined hypoechogenicity , and increased vascularity on power doppler examination [ 27 , 28 ]  . several therapeutic procedures can be performed under us guidance to treat tendinopathy ; they range from the widely used peri - tendinous injection of corticosteroid or low molecular weight ha , dry needling , sclerotherapy , prolotherapy , high - volume injections ( hydrodissection ) , autologous blood injection , and newest regenerative therapeutic alternatives , including prp [ 29 ] and adipose - derived mesenchymal stem cells ( ascs ) [ 30 ]  . for all procedures , the probe is placed on the affected tendon with a longitudinal approach . 
in such cases , the purpose of the infiltrative therapy will be to bring the drug ( steroid or low molecular weight ha ) exactly in the space between the sliding sheath and the tendon to achieve the maximum therapeutic effect without damaging the tendon [ 3134 ]  . 
in case of stenosing tenosynovitis ( such as de quervains disease and trigger finger ) , steroid injection can be combined with a second treatment consisting in a injection of low molecular weight ha ( about 1ml ) between the tendon and the retinaculum or tendon sheath [ 35 ]  . 
this has the twofold purpose of favoring tendon gliding and stretching the peritendinous tissues , allowing to obtain satisfactory results up to 12months [ 36 ]  . an example of tendinopathy treatment is shown in fig.3. spine procedures interventional radiology can be of great value in the treatment of several spine conditions , which may cause back pain and disability . 
us guidance should help to pierce only one side of the bursa to avoid drug leakage in the underlying structures . an example of bursal injection is shown in fig.2. tendinopathies degenerative tendinopathy is characterized by structural degenerative changes of the collagen fibers with accompanying fibrosis , associated with minimal or no inflammation signs [ 13 ]  . 
following fj injection , pain relief is generally temporary ( weeksmonths ) and usually patients come back for recurring pain such cases , if patients have reported some pain relief following fj injections , they can be treated with thermocoagulation of the fj nerves ( i.e. , rhizolysis ) which is performed under local anesthesia and imaging guidance . selective nerve root block ( snrb ) nerve root compression is another very common cause of back pain , generally associated with neuropathic manifestations with electric sensation irradiating to the lower limbs with a typical dermatomeric distribution . 
us guidance can also be used . injections can be performed in the posterior epidural space or around the nerve roots . technically , the patient lies prone or supine ( e.g. , cervical peri - radicular injection ) or prone ( dorso - lumbar epidural or peri - radicular injections ) on the bed and a 20g spinal needle is used . when injection is performed in the posterior epidural space , a co2 - test is performed to confirm the epidural location of the needle before injecting the drug . 
if co2 dissection of the posterior epidural space is not achieved ( e.g. , post - surgical fibrosis ) , few ml of contrast medium can be injected to confirm the right location of the needle . 
despite the type of agent used ( co2 or contrast medium ) , the typical epidural location is confirmed when the injected lies around the dural sac with a reversed crescent shape morphology ( i.e. , concavity of the crescent facing the dural sac )  . on the other hand , when peri - radicular injections are performed , mainly at the cervical or lumbar level , the needle tip is advanced at the posterior distal aspect of the neuroforamen and few ml of contrast medium is injected to confirm that the needle is not inside a vessel , which contraindicated the steroidal injections . 
if the needle is correctly deployed , injected contrast medium spreads around the nerve root ( rootgram ) and sometimes also in the epidural space . once checked the correct needle position , a 1 : 1 solution of non - particulated steroid ( e.g. , dexamethasone ) and local anesthetic can be injected . 
of note , the use of non - particulated steroids in this anatomical area is very important especially in the cervical spine , as inadvertent intra - arterial injection may lead to thrombosis of distal branches with fig . 
p patellar tendon , h hoffas fat pad , arrow needle tip , asterisks dry needling procedure and prp injection and increased accuracy of spine procedures and is mainly based on fluoroscopy and computed tomography ( ct )  . 
more recently , the use of us + ct / mr fusion imaging has been reported [ 37 ]  . facet joint ( fj ) injections fj osteoarthritis is a very common and frequently overlooked painful condition , which can be considered responsible for 1540% cases of low back pain ( lbp )  . 
in the end , pain is evoked by palpation of the target fj and is increased with hyperextension of the spine . in such cases , fj injections with local anesthetics or and steroids can be performed . currently , fj injections are commonly performed under fluoroscopy or ct guidance , allowing excellent visualization of typical bony landmarks to guide the procedure . 
 the patient is positioned prone on the bed , and the joint is approached directly either with posterolateral or straight posterior vertical approaches to the joint using a 20 gauge spinal needle . 
correct needle placement may be confirmed by injecting a small amount of contrast agent ( 0.2ml ) , and 1 3 la radiologia medica ( 2019 ) 124 : 11121120 1117 potentially life - threatening sequelae . 
transient anesthesia in the innervated territories of the injected root is a minor side effect of this treatment . disc procedures intervertebral discs can be affected by both degenerative and inflammatory conditions [ 39 ]  . 
regarding inflammatory conditions , the disc may be affected by infections ( i.e. , spondylodiscitis ) and discal biopsy can be performed with similar technique . the procedure can be performed either under ct or fluoroscopic guidance . 
 however , in general , most of these symptoms disappear after two weeks . an example of disc biopsy is shown in fig.4. kyphoplasty andvertebroplasty vertebral compression fractures ( vcf ) represent a cause of thoracic and lumbar spine paalthough some vcf can be due to high - energy trauma , many of them occur after lowenergy or no trauma in patients with altered bone structure , such as metastases or osteoporosis [ 4448 ]  . 
 the main issue of osteoporosis is of being a silent disease , so if patients do not undergo routine screening , a fracture may be the only sign of this condition . 
conservative treatment for osteoporotic vcf includes pain management with bracing , rest , analgesic and anti - inflammatory drugs , calcium , vitamin d , and bisphosphonates supplements [ 50 ]  . 
4 76 - year - old male patient presenting with a systemic inflammatory syndrome and lumbar pa a contrast - enhanced sagittal t1 - weighted and b stir sequences raised the suspicion of l3 - l4 spondylodiscitis ( arrows )  . 
5 90 - year - old osteoporotic female patient presenting with spontaneous sudden dorsal paa sagittal t1 - weighted and b stir sequences showed t8 and t9 vertebral compression fractures ( arrows )  . 
the patient underwent double - level vertebroplasty under conscious sedation and local anesthesia ; fluoroscopic guidance was used to c deploy a 10g bone bevelled bone trocar in each vertebral body and to d inject the polymethyl methacrylate ( pmma ) , asterisk . 
final e fluoroscopic and f cbct images confirmed the good distribution of the pmma ( from endplate to endplate in the anterior two - thirds of the vertebral body ) in each treated level approach [ 53 , 54 ]  . 
extra - osseous approaches should be avoided due to the risk of iatrogenic injuries to the thoracic / lumbar artery supplying the anterior spinal artery ( adamkiewiczs artery )  . 
kyphoplasty is a modification of vertebroplasty , characterized by the percutaneous insertion of an inflatable high - pressure compliant balloons into the fractured vertebral body with the aim of restoring the vertebral height and create a cavity inside the vertebra where the cement can be injected for vf stabilization [ 56 ]  . 
both vertebroplasty and kyphoplasty can be performed under general anesthesia , although conscious sedation is also possible [ 5759 ]  . pmma is the most frequently used cement in both procedures , although new biological materials , such as calcium phosphate and hydroxyapatite , have been introduced [ 60 ] even though there is no general agreement on their use ; for this reason , pmma is still the most commonly used agent . vertebroplasty and kyphoplasty are equivalent in terms of early and long - term pain relief ; the only advantages of kyphoplasty over vertebroplasty are ( 1 ) higher chance to restore the kyphotic deformation , thus ideally having a better long - term impact on the respiratory function ; ( 2 ) a reduced risk of extra - osseous pmma leakage . 
in most of the cases , pmma leakages remain clinically nonsignificant unless large amount of pmma leak in the antero / lateral venous plexus with subsequent massive pulmonary embolism ; or in the posterior venous plexus with subsequent compression of the spinal cord . 
however , epidural injections can be performed with chilled saline and steroids to prevent neurologic complications related to the transient exothermic pmma polymerization . 1 3 la radiologia medica ( 2019 ) 124 : 11121120 1119 an example of vertebroplasty is shown in fig.5. conclusion interventional procedures in the musculoskeletal system can be used to treat a wide variety of inflammatory and degenerative conditions . 
the ra - induced morpho - structural changes can be effectively detected and measured by us , and us findings represent an additional advantage over clinical and laboratory evaluation , showing the face of the disease ( i.e. , proliferative synovitis ) and revealing its aggressive behavior ( i.e. , presence of bone erosions not detectable by conventional radiography )  . 
the present review provides an overview of the main studies focusing on the value of us in the assessment of the patients with ra , and discussing the elementary lesions detectable by us ( synovitis , bone erosion , cartilage damage , tenosynovitis and tendon damage ) , the scoring systems currently available and the scanning protocols in definite clinical settings ( undifferentiated arthritis , early and long standing ra )  . keywords ultrasonography rheumatoid arthritis synovitis bone erosion scoring systems introduction rheumatoid arthritis ( ra ) is a chronic inflammatory autoimmune disease , mainly involving the small joints of the hands and feet . 
in fact , further evidence is still required to increase specificity , reduce false positivity and provide knowledge 1 clinica reumatologica , universit politecnica delle marche , ospedale carlo urbani , via aldo moro , 25 , 60035jesi , ancona , italy 2 dipartimento diagnostica perimmagini , ulss 6 euganea , ospedale di cittadella , casa di ricovero , 40 , 35013 , cittadella , padova , italy 3 radiology department , universit politecnica delle marche , ospedali riuniti di ancona , via conca , 71 , 60126ancona , italy vol . : ( 0123456789 ) 1 3 1088 la radiologia medica ( 2019 ) 124 : 10871100 regarding the long - term impact of ultrasonography ( us ) findings . 
thus , us is still not included in the standard procedures recommended by eular for the management of early arthritis [ 57 ]  . over the last two decades , a growing number of studies have been published aiming at investigating the role of us in the diagnosis and follow - up of patients with ra . the analysis of the obtained results indicates that a systematic use of us may provide the following additional values [ 812 ] : in ra . 
b severe joint dislocation due to volar subluxation of the proximal phalanx together with extensive synovial proliferation ( * ) and massive erosive change in the metacarpal head ( arrow )  . 
in this scenario where many publications emphasize the importance of identifying synovitis and erosions at an early stage , it is essential to know the possible pitfalls which can determine both false positives and false negatives . 
the high variability of the musculoskeletal system anatomy makes it necessary to have a correct knowledge of all anatomical complexes , in order not to confuse them with the pathology . 
moreover , the correct and standardized method of the execution and interpretation of the exams , such as ultrasound , is crucial to identifying and correctly monitoring the pathological hallmarks of the arthritis . 
this paper aims to provide an instrument to radiologists , highlighting the main imaging pitfalls in ultrasound and magnetic resonance which may be encountered in daily practice . keywords mri arthritis ultrasound enthesitis pitfalls introduction joint effusion andsynovitis arthritis and spondyloarthritis represent a heterogeneous group of inflammatory disorders characterized by the chronic inflammation of joints and enthesis . although the diagnosis is still based on clinical criteria , imaging is of fundamental help in the management of these diseases [ 1 , 2 ]  . 
salvatore hospital , university oflaquila , laquila , italy 5 department ofradiology , pineta grande hospital , castelvolturno , ce , italy synovial effusion and synovitis are the hallmarks of chronic inflammatory arthritis and both ultrasound ( us ) and magnetic resonance ( mr ) are widely used for their detection , grading and monitoring [ 3 ]  . the us synovial effusion is defined as abnormal hypoechoic or anechoic ( relatively to the subdermal fat , but sometimes it may be isoechoic or hyperechoic ) intraarticular material that is displaceable and compressible ; the us synovial hypertrophy is defined as abnormal hypoechoic ( relatively to the subdermal fat , but sometimes may be isoechoic or hyperechoic ) intraarticular tissue that is non - displaceable and poorly compressible and which may exhibit a doppler signal [ 4 ]  . 
in fact colour doppler ( cd ) and power doppler ( pd ) us are able to detect pathological synovial blood flow in the synovial tissue , which reflects the inflammatory activity in the joint [ 5 ]  . one potential us pitfall is the failure to detect intraarticular fluid collection and synovial hyperaemia in the presence of synovial hypertrophy . in the small joint the excessive pressure of the us probe might dislocate the fluid on the other side with the result of hiding it ; moreover , the transducer pressure might compress the small synovial vessels with the disappearance of vol . : ( 0123456789 ) 1 3 1168 la radiologia medica ( 2019 ) 124 : 11671174 the doppler signal . 
in addition , if the us scan is performed with the hip in internal rotation , the anterior joint capsule becomes convex anteriorly measuring more than 7mm [ 9 ]  . normal fat structures can also simulate synovial hypertrophy at us scan , such as the prefemoral fat pad . 
3 a , d normal prefemoral fat pad ( arrows ) in a lateral transverse us scan of the superolateral recess of the knee simulates synovial hyperplasia but on b axial pd fatsat sequence mr image shows normal fat low signal . 
c , d true synovial hyperplasia appears hyperechoic on c transverse us scan and shows high signal on d axial pd fatsat sequence mr ( not distinguishable from synovial fluid ) 1 3 la radiologia medica ( 2019 ) 124 : 11671174 1169 fig . 
4 short axis pdus scan of the long head biceps tendon in its bicipital groove shows : a ascending branch of the anterior humeral circumflex artery ( black arrow ) that runs laterally to the tendon ; b synovial hyperplasia ( white arrows ) with several spots of doppler ( black arrows ) and sheath fluid distension ( star )  . 
5 long axis us scan of the fourth compartment extensor tendon at the level of radiocarpal joint showing the normal extensor retinaculum of the wrist ( white arrows ) that runs perpendicular to the tendons . 
6 long axis us scan of the achilles tendon enthesis shows a several doppler spots when the ankle is positioned in plantar flexion and b no doppler signal is visible in dorsiflexion . 
even the presence of a low grade of an inflammation severity should be considered with caution when it is used for a diagnostic purpose [ 15 ]  . tenosynovitis tenosynovitis is defined on b - mode us as an abnormal anechoic and / or hypoechoic ( relatively to tendon fibres ) tendon sheath widening , related both to the presence of tenosynovial abnormal fluid and / or hypertrophy [ 16 ]  . structures that may simulate an ultrasonographic tenosynovitis are the retinacula of the extensor tendons of wrist and ankle . 
8 pdw fatsat axial mr image of the shoulder showing two tendons ( arrows ) of the long head biceps in the bicipital groove 1 3 la radiologia medica ( 2019 ) 124 : 11671174 1171 fig . 
9 longitudinal dorsal us scan of the second metacarpophalangeal joint showing : a normal pseudoerosion ( arrow ) of metacarpal bone and b true erosion of the metacarpal head with cortical discontinuities ( arrow )  . 
mc metacarpal head , p2 second proximal phalanx ankle at the level of the radiocarpal and tibiotalar joints , running over the extensor tendons more or less parallel to thein healthy subjects the extensor retinacula measure 0.61.7mm in thickness over the wrist and 0.61.4mm over the ankle [ 17 , 18 ]  . 
the normal extensor retinaculum shows a subtle fibrillar echotexture when imaged perpendicular to the sound beam and it is slightly hypoechoic compared with adjacent tendons and with the subcutaneous fat . 
10 t1w coronal mr image of the wrist showing normal cortical irregularity of the radial aspect of the capitate bone ( arrow ) at the insertion of the scaphocapitate ligament 1 3 1172 fig . 
11 stir oblique coronal mr image of the sacroiliac joint showing accessory sacroiliac joint on the right side ( white arrow ) and the iliosacral complex on the left side ( arrowheads ) with intrarticular high signal due to the presence of several vessels la radiologia medica ( 2019 ) 124 : 11671174 enthesitis the us enthesitis is defined as an hypoechoic and / or thickened insertion of the tendon close to the bone ( within 2mm from the bony cortex ) which exhibits a doppler signal if it is active and which may show erosions and enthesophytes / calcifications as a sign of structural damage [ 20 , 21 ]  . probably the most insidious pitfall during the us scan of the enthesis is the failure to detect the doppler signal due to the position of the joint . 
on the contrary of the b - mode scan , during the pd - scan of the enthesis the tendon must not have tension , in order to avoid the collapse of the vessels and the hiding of the doppler signal . 
therefore , during the pdus scan of the achilles tendon , the ankle should be positioned in plantar flexion or in neutral position ( fig.6 ) ; during the pdus scan of the quadriceps and patellar tendons , the knee should be extended [ 2224 ]  . in mr a potential mistake is related to the identification of small enthesophytes and syndesmophytes when no active inflammation is present . 
the accessory tendon frequently has an extraarticular origin from the superior capsule , rather than the intraarticular one and some authors consider this structure as an aponeurotic expansion [ 29 , 30 ]  . 
the pseudoerosion is a cortical homogeneous depression ( mean depth , 0.3mm ) in 1 3 la radiologia medica ( 2019 ) 124 : 11671174 1173 the dorsal metacarpal head , located adjacent to the hyaline articular cartilage at the site of the dorsal joint recess [ 33 ]  . 
contrast material when evaluating the response to tumor necrosis factor ( tnf ) antagonists therapy , on the extension of bone marrow oedema ( bmo ) and pathological enhancement ( osteitis / synovitis ) in the sacroiliac joints ( sijs ) on mri . materials and methods forty - three patients ( 25 females and 18 males , mean age of 54 16.60years , range 2275years ) with a clinical diagnosis of spa and active sacroiliitis at mri with i.v. 
scores difference ( improvement ) after treatment was calculated in the mri sequences both with and without contrast agent ( respectively , mean value and range 3.18 , 012 with contrast and 1.63 , 07 without contrast )  . 
inflammation at either ligament , tendon or capsular insertions , or enthesitis , is the hallmark of these diseases which consist of ankylosing spondylitis , psoriatic arthritis , arthritis / spondylitis associated with inflammatory bowel disease and reactive arthritis [ 1 ]  . 
in fact , sacroiliac joints ( sijs ) involvement is one of the key criteria for diagnosing axial spa , which usually occurs in the first stages of the vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 11421150 1143 sacroiliitis at mri with i.v. 
inclusion criteria included meeting the asas classification criteria for spa and not being treated with glucocorticoids , nonsteroidal anti - inflammatory drugs ( nsaids ) or disease modifying antirheumatic drugs for a period of at least 2months prior to the trial . 
thanks to the recent introduction of new and promising treatment options , such as tumour necrosis factor ( tnf ) antagonists therapy , which could modify the natural history of the disease , not only an early diagnosis is fundamental , but also an objective mean to evaluate response to therapy is often demanded by clinicians . 
in this respect , imaging , together with clinical and laboratory evaluation , are not only important tools to achieve an accurate diagnosis but also in the grading of disease modification , influencing both clinical management and therapy [ 2 ]  . 
conventional radiography is the most accepted imaging method for diagnosing sacroiliitis because it is relatively inexpensive , readily available , and , when it yields positive findings , very effective ; however , conventional radiography can only detect advanced structural damage , which usually requires several years to become evident and above all active inflammation cannot be assessed [ 3 ] , making this technique unsuitable to evaluate response to therapy . 
instead , magnetic resonance imaging ( mri ) can provide an early diagnosis and is able to quantify inflammatory activity showing bone marrow oedema ( bmo ) or osteitis , synovitis , which makes it ideal for monitoring disease activity too . 
thus , in 2009 , mri was included in the new assessment of spondyloarthritis international society ( asas ) criteria for the diagnosis of axial spa , in order to facilitate the identification of early features of spa before radiographic findings and in the assessment of treatment response . 
despite this , a clear definition of mri active sacroiliitis still does not exist , even if the presence of subchondral bone oedema is believed mandatory and examination without an i.v. 
 contrast material in evaluating the response to tnf antagonists therapy in the sijs , comparing the reduction grade of bmo and osteitis / synovitis , respectively , on mri without and with i.v. 
contrast agent , with bath ankylosing spondylitis disease activity index ( basdai ) before and after treatment . materials andmethods this study was approved by the institutional review board of ouruniversity hospital . 
written informed consent was obtained from all participants . patient information from december 2014 to march 2016 , 43 patients ( 25 females and 18 males , mean age of 54 16.60years , range 2275years ) with a clinical diagnosis of spa and active fig . 
2 ad unilateral sacroiliitis in a 64 - year - old woman with right upper sacrum bmo on t2 w fat - saturated images and osteitis on 3d gradient - echo t1 w images after i.v. 
of the contrast agent ( a , b ) ; after 6 months of tnf antagonists therapy the oedema was unchanged , whereas osteitis disappeared ( c , d ) subtracted from the later scans . 
the first two sequences ( t1 - weighted fse and t2 - weighted frfse ) allow the detection of structural changes like erosions and sclerosis ; t2 - weighted fat - saturated images depict inflammatory bmo as increased signal intensity and the latter sequence allows the detection of osteitis , synovitis and capsulitis . image analysis two experienced observers , a radiologist and a resident radiologist , with more than 15 and 3years experience , respectively , in musculoskeletal imaging , were blinded to the patients clinical characteristics and evaluated mri images , scoring bmo in t2 - weighted fat - saturated sequences and areas of pathological enhancement in gradient - echo t1 sequences after i.v. 
the score was semiquantitative and based on the extension and intensity of the lesions ; grade 0 = no inflammatory changes ; grade 1 = inflammation involving up to 20% of the joint area ( signal intensity changes confined to the joint space , joint capsule and erosions ) ; grade 2 - 3 = inflammation of paraarticular bone marrow involving up to 50% or over 50% of the region . 
any disagreement was discussed until a consensus was reached . 1 3 la radiologia medica ( 2019 ) 124 : 11421150 1145 statistical analysis descriptive statistics were used to describe the overall distribution of the scores ; students t test was used to compare the difference ( improvement ) between basdai scores at baseline and after treatment ; students t test and blandaltman plot were used to compare the differences between mr scores ( improvement ) at baseline and after treatment in sequences with and without contrast media . 
in contingency tables , the values are expressed as percentage of the total number of patients . results among all the 43 patients , 3 were excluded since they refused mr follow - up and 2 since therapy was prematurely interrupted for adverse dermatological reactions . 
3 ad a 41 - year - old woman with chronic bilateral sacroiliitis , represented by diffuse subchondral sclerosis involving the iliac portion of sij , developed a clinical exacerbation . 
a , b there was no bmo on t2 - weighted fat - saturated images , but a little area of synovitis in the upper left sacrum on 3d gradient - echo t1w images after i.v. 
injection of the contrast agent ; c , d after therapy an area of sclerosis was clear on both sequences 1 3 1146 table 1 summary of the scoring results of mri findings ( bmo and osteitis / synovitis ) and basdai for each patient before and after therapy la radiologia medica ( 2019 ) 124 : 11421150 patient ( n ) bone marrow oedema osteitis / synovitis basdai before after before after before after with the sacral aspect of sijs being the most commonly affected area ( more than 70% of the patients )  . 
thirtysix out of 38 patients showed an improvement on clinical assessment after therapy , assessed by the basdai : 20 out of 36 ( 55.5% ) showed reduction / disappearance of both enhancement and bmo , but the reduced grade of the first parameter was higher ; 11 out of 36 ( 30.5% ) showed reduction / disappearance of pathological enhancement , whereas bmo was unchanged ( fig.2 ) ; 2 out of 36 ( 5.5% ) showed reduction of enhancement in the absence of bmo before or after therapy ( fig.3 ) ; 3 out of 36 ( 8.3% ) and the remaining 2 out of 38 did not show modification of mri findings . 
moreover , a significant 1 3 la radiologia medica ( 2019 ) 124 : 11421150 1147 discussion inflammatory sacroiliitis is a chronic , disabling disease because of the patients pain and motions restriction due to progressive structural damages of sijs . 
in the past , several therapies have been used to treat these pathologies , for example , nonsteroidal anti - inflammatory drugs ( nsaids ) , corticosteroids and immunosuppressant drugs . 
tnf antagonists have been investigated in randomized controlled trials in patients with spa , and benefits were obtained particularly in patients with recent - onset disease ; in fact , most of response rates were higher than in controlled trials of the same drugs used to treat advanced disease , suggesting the existence of a window opportunity [ 7 ]  . 
however , the management of these therapies requires great attention in diagnosis and follow - up ; such therapy is not only expensive but may also raise the risk of developing serious infections and malignancies [ 8 , 9 ]  . 
recently , it has been shown that dose tapering of tnf antagonists is a feasible therapeutic option in patients with spa and low disease activity , without relevant changes in the clinical outcome , resulting in remarkable cost savings [ 10 ]  . 
although disease activity is usually assessed by clinical and biochemical parameters , mri may help to objectify response to therapy and therefore to optimize treatment plan for each patient [ 11 , 12 ]  . 
mri is the best imaging modality able to detect and quantify active inflammatory changes of the sijs , even if dual - energy ct ( dect ) , at present , seems to be promising in this regard , despite limited to bmo detection and quantification [ 1315 ]  . 
although several studies in the literature compared mri contrast - enhanced fat - saturated t1 weighted sequences with t2 - weighted fat - saturated sequences to diagnose active inflammatory sacroiliitis , reporting bmo sufficient for this task [ 16 , 17 ] , other studies declared that the administration of contrast medium may be beneficial by providing a different view of the lesions with another sequence , which can be helpful when mri is interpreted by inexperienced readers or when minimal changes occur [ 18 ]  . 
in particular , thanks to its higher spatial resolution , post - contrastt1 - weighted imaging is more sensitive in detecting small subchondral lesions and other imaging findings that are sometimes difficult to see without contrast material administration , such as synovitis and capsulitis [ 3 , 19 ]  . furthermore , the pathogenetic mechanism of spa has not yet been fully clarified and there are many hypotheses about the mechanism of inflammation development and damage production . 
4 box plot of scores difference ( improvement ) in the mr sequences with and without contrast agent administration difference ( p < 0.05 ) was found between the improvement calculated in the sequences with and without contrast media administration . 
 descriptive statistics show differences in score between the mri sequences with and without contrast agent , demonstrating a higher improvement in post - therapy using the former ( figs4 , 5 , 6 , table2 )  . 
5 function of empirical distribution for the improvement ; black ( mr with contrast ) , red ( mr without contrast ) 1 3 1148 la radiologia medica ( 2019 ) 124 : 11421150 and after therapy . 
moreover , in patients with chronic sacroiliitis , findings such as long - standing erosions sometimes showed nuanced bmo in absence of active inflammation signs in post - contrast sequences ; in such cases , post - contrast sequences are extremely useful to establish a proper therapeutic management . 
on the other hand , the presence of inflammation alone may not be the primary factor associated with structural damage progression , which seems to be also related to the development of fat metaplasia . 
in this regards , further studies are necessary to understand the physiopathological connections between inflammation , fat metaplasia and structural damage in spa . some limitations of our study should be noted . 
in addition , mri scores before and after treatment were correlated with basdai since ankylosing spondylitis disease activity score ( asdas ) was not available for all the patients ; in this regard asdas seems to be more closely associated with inflammatory biomarkers and may better reflect the inflammatory disease process in patients with axial spa treated with tnf inhibitors [ 3336 ]  . 
6 blandaltman plot showing the dispersion of the values from the mean suggests a difference between the mr improvement calculated on the sequences with and without contrast agent most involved area [ 20 , 21 ] , whereas others argued that the pathologic mechanism of spa is different from that of ra , since the most affected region is the enthesis [ 2226 ]  . 
 however , studies that investigated sacroiliitis through fine needle aspiration biopsy found that in the early stage of the disease , pannus formation , which is constituted by highly vascular granulation tissue formed by the inflamed synovium and / or subchondral bone marrow , in the area where bone and cartilage oppose one another , may be the pathological hallmark ; subsequently , inflammation may trigger the formation of angiogenesis with an increased microvessel density that provides a channel for inflammatory cell invasion and mediator expression , which in turn worsen the local damage to the cartilage [ 2732 ]  . this increase in angiogenesis has been shown to decrease significantly after tnf antagonist treatment , revealing the pivotal role of angiogenesis in spa . 
this statement seems to be supported by the thesis that subchondral inflammation may trigger the formation of angiogenesis with an increased microvessel density that provides a channel for inflammatory cell invasion and inflammatory mediator expression , which in turn worsen the local damage to the cartilage . 
antonio e biagio e cesare arrigo , via venezia 16 , 15121alessandria , italy 2 department ofhealth sciences ( dissal ) , university ofgenoa , c.so montegrappa 26 , genoa , italy 3 department ofmedical , surgical andneuro sciences , diagnostic imaging , azienda ospedaliera universitaria senese , university ofsiena , viale bracci 10 , 53100siena , italy introduction axial skeleton , including both the spine and the sacroiliac joints ( sijs ) , represents a diagnostic challenge both for the clinician and for the radiologist . 
in the literature , vertebral column has been the main target of study in degenerative diseases , while sijs have been the leading subject of study , especially in magnetic resonance imaging ( mri ) , in relation to spondyloarthritis ( spa )  . 
in fact , mri plays an important role in the diagnosis of axial spa by detecting sacroiliitis ( using the assessment in spondyloarthritis international society ( asas ) imaging arm ) , more sensitively and also with a better reproducibility compared with conventional radiography . 
however , more recent studies , which have included both patients with spa diagnosis and patients with non - specific low back pain ( lbp ) , showed that mri findings related to sijs , once considered specific for diagnosis of spa , are also prevalent in patients with non - specific lbp [ 16 ]  . at the same time , vertebral features specific for spa diagnosis may be underdiagnosed in the context of a large prevalence of degenerative findings ( modic , etc . ) , which indeed could mislead the assessment of spa diagnosis [ 7 ]  . 
thus , the best knowledge in the use of instrumental and diagnostic techniques , such as mri , able to identify the objective signs of inflammation , such as bone edema , that is a non - specific but very early vol . : ( 0123456789 ) 1 3 1152 la radiologia medica ( 2019 ) 124 : 11511166 finding should be desirable . 
in particular , regarding the use of mri , the main risk is overdiagnosing spa ( just as damaging as a diagnostic delay ) , scotomizing the most common degenerative diseases recognized in acute phase : pousses during discoarthrosis or fibromyalgic syndromes in which a lumbar pain with inflammatory characteristics could be present in up to 40% of cases [ 8 , 9 ]  . 
in fact , literature data report that only 36% of patients with inflammatory lumbar pain had a diagnosis of sacroiliitis based on mri findings according to asas criteria : in this sense , anamnesis and clinical history are important in differential diagnosis . 
furthermore , the diagnostic delay in diagnosing spa exposes the patient to very important consequences in terms of activity and evolution of the disease , with impaired quality of life , functional limitations and increased risk of cardiovascular events , professional economy , especially when dealing with young people with loss of workability and medical nomadism , which requires specialist advice and therapies that are inappropriate . the aim of this manuscript is to review the differences in degenerative and spa - related mri findings in spine and sijs in order to give a complete scenario in differential diagnosis of low back pain using imaging . mri andaxial skeleton : technique andassessment in order to better identify the mri findings of both degenerative and inflammatory diseases , it is important to give the definition of prescriptive and executive appropriateness and fairness in mri of axial skeleton and , moreover , the definition of spine and pelvis mri study protocols . mr examination of specific anatomical regions should be performed using dedicated spinal or body phased - array coils . in the early diagnosis of axial spa , a sijs mri is recommended . 
in clinical practice , and especially in case of doubt , spinal mri may be useful for the positive diagnosis of other diseases ( e.g. , modic type 1 , scheuermanns disease , diffuse idiopathic skeletal hyperostosis )  . 
in spa patients , the mri scan range on sagittal slices should be laterally extended to include the paravertebral structures such as facet , costotransversal and costovertebral joints that are commonly involved in spa . 
 sagittal sequences should be positioned to comprehend the entire spine including facet joints , the costovertebral and costotransverse joints ( a ) , and coronal sequences should be positioned to comprehend the entire spine too , including anterior longitudinal ligament and the posterior part of the spine to the spinous process , including the zygoapophyseal joint , the costovertebral and costotransverse joints ( b , c , d ) 1 3 la radiologia medica ( 2019 ) 124 : 11511166 1153 inflammatory findings , such as erosions , sclerosis , fat deposition and bone marrow edema ( bme ) , which is considered an objective sign of inflammation , identifying the concept of non - radiographic spondyloarthritis ( nr - spa ) in new asas criteria ( figs.3 , 4 ) [ 1 ]  . 
the use of intravenous ( i.v. ) injection of paramagnetic contrast media has proven valuable in showing the extension of inflammatory changes , and in particular in demonstrating osteitis , as well as abscesses in septic sacroiliitis or spondylodiscitis or in the assessment of neoplastic disease . 
injection of contrast media in spondyloarthropathies may be useful , although this is debatable . mri findings inthesacroiliac joints : sacroiliitis andnoninflammatory disease the special configuration and anatomy of sijs determine that they undergo morphological transformations throughout life and produce a degeneration in which extrinsic factors , such as trauma or stress ( scoliosis , dysmetria , previous surgery of the column , pregnancy , childbirth , etc . ) , or intrinsic diseases , both inflammatory or infectious ( spondyloarthropathies and , less frequently , septic arthritis ) , and , less frequently , tumor lesions , could act on their changes . normal mri anatomy the sij is one of the largest axial joints and is composed in its upper and dorsal region by a syndesmosis , which is a fibrous joint in which the bony surfaces are joined by interosseous ligaments , and a cartilaginous area , classically defined as synovium , which extends into the lower two - thirds of the ventral area , but actually has a structure of symphysis with hyaline cartilage firmly attached to the adjacent bone by fibrous tissue . 
these anatomical features could explain why the changes begin and are more relevant in the iliac aspect of the joint , while rheumatoid arthritis has a poor expression in the sijs and inflammatory changes in spondyloarthropathies show similar changes to those that occur in a symphysis . 
articular stability is provided by the intrinsic sacroiliac ligaments in the ventral region and interosseous ligaments in the dorsal area and extrinsic ligaments , which are fibrous extensions of closer muscles and contribute to capsular reinforcement [ 1013 ]  . 
axial sequences should be positioned from 1 to 2cm above the iliac crests to the femoral lesser trochanter with fov sized enough to cover the entire soft tissue in the anteroposterior direction for the study of the enthesis ( a )  . 
oblique coronal and oblique axial sequences ( b ) should be , respectively , oriented along the long axis of the sacral bone and oriented perpendicularly to the semi - coronal or along the short axis of the sacral bone , to comprehend the entire sacroiliac joint t1 - weighted sequences ( tse t1w ) and high intrinsic contrast sequences , turbo spin - echo t2 - weighted sequences ( tse t2w ) with fat suppression or short - tau inversion recovery ( stir ) sequences should be performed in order to obtain a clear detection , respectively , of both structural and 1 3 1154 la radiologia medica ( 2019 ) 124 : 11511166 fig . 
if there is only one lesion , it should be present at least on two consecutive slices ; if there is more than one lesion on a single slice , one slice may be enough ; b corresponding hypointensity for bme in coronal oblique tse t1w and structural lesions such as erosions fig . 
4 oblique axial tse t1w ( a ) and tse t2w ( b ) and spir t1w with gadolinium ( c ) and oblique coronal stir ( d ) : outcomes of inflammatory process with evolution in adipose substitution of bone marrow opposed to the sacroiliac articulations , on both sides , with fine structural irregularity of the articular line and enhancement of the anteroinferior portion degenerative changes in all joints from the age of 50 on , some type of degeneration is observed , and these changes are more profuse in women than in men of the same age and progress more rapidly in female multiparae than in nulliparous women . 
also , anatomical variants are observed and the knowledge of these variants is essential to avoid diagnostic errors ( accessory sacroiliac joint 1719% , iliosacral complex 5.89.5% , bipartite iliac bone 4.17.8% , defect semicircular articular surfaces 3.74.8% , crescent articular surface 3.5% and ossification centers of the sacral rings 1% )  . 
most of them share the fact that they are often observed in people older than 60years and some are more frequent in women ( the first of the variants in women with more than three children ) and in obese patients [ 1416 ]  . fatty bone marrow deposition , sclerosis and erosions were strongly associated with female gender , and this could be explained by a correlation between sij findings and a different load distribution in women and / or pregnancy - related physiological changes of the pelvic girdle and birth - related strain [ 17 ]  . 
in the literature , associations between bme and degenerative / load - related changes at different locations such as spine ( modic type i changes ) [ 18 , 19 ] and knee [ 20 , 21 ] are known . 
 [ 8 ] , supported by bme being more prevalent in the oldest patients in their study , assumed that bme in sijs also may be correlated with degenerative changes due to impaired chronic loading . both osteoarthritis and arthritis can present common structural changes such as subchondral sclerosis , joint clamping ( which will favor arthritis when the joint measures less than 2mm in patients under 40years of age ) and ankylosis . 
osteophytes , pneumocystis and intra - articular vacuum are typical of osteoarthritis , although arthritis without active inflammation may present intra - articular void that could be a sign of inactivity . table 1 active and structural changes of the sijs according to asas active inflammatory lesions inflammatory changes erosions are typical of chronic morphological changes of arthritis . 
on the other hand , when there are acute inflammatory signs in a spondyloarthropathy or infectious arthritis , the only test to detect inflammation with good sensitivity and specificity is mri . 
spinal spa - related mri findings are rare , and bme is the most common ( 21% ) in sijs ; furthermore , spinal inflammatory lesions suggestive of axial spa are rarely found in the absence of sacroiliitis on mri ( or radiography ) [ 3 ]  . in the literature , from 10% [ 8 ] to 36% [ 22 ] of the patients fulfill the asas criteria for spa via the imaging arm ( mri findings fulfilling the asas definition of a positive mri for sacroiliitis , with a final clinical diagnosis of axial spa ; table1 )  . 
however , whether this is an appraisal of the prevalence of patients with true spa , it remains unknown in the general population , due to the uncertainties regarding the diagnostic performance of the criteria which resemble more a classification system than proper diagnostic criteria ; therefore , their specificity might be low due to a high prevalence of a positive mri among non - specific lbp patients . 
 historically , the aim in research of mri findings in sijs focused on patients with inflammatory back pain or spa and few studies have reported on mri findings in sijs in patients with non - inflammatory back pain [ 23 ]  . 
a few casecontrol studies have reported the prevalence of bme , fatty marrow deposition , erosions and ankylosis at the sijs in patients with non - specific lbp to be 2227% [ 8 , 23 ] , 1527% [ 8 , 9 ] , 413% [ 8 , 9 ] and 0% [ 8 , 9 ] , respectively , suggesting a high specificity of ankylosis for stadium iv of spa . among patients with bme in sij , it is reported in the literature a significantly higher prevalence of erosions in patients fulfilling the asas criteria for spa ( 41% ) compared to those who did not achieve these criteria ( 20% )  . 
bone marrow edema area of high signal on t2 fs or stir images ; typically located subchondrally in the cartilaginous parts of the sijs thickening of the sijs capsule and adjacent ligaments ; it appears as hyperintense signal on t2 fs or stir images and / or hyperintense on contrast - enhanced t1 fs sequences it presents as a hyperintense signal on contrast - enhanced t1 fs images , in the synovial part of the sacroiliac joint it is seen as hyperintense signal at sacroiliac ligaments or entheses on stir or t1 fs contrast - enhanced sequences ; it could be accompanied by bme of the bony part of the entheses ( bme ) 2 . 
bone erosions subchondral area of low - intensity signal at the sijs on all sequences joint facet / subchondral bone abnormalities appearing as few , multiple , localized or contiguous low signal intensities on t1 - weighted mr images with varying signal intensity on t1 fs or t2 fs sequences 3 . 
bony bridges , ankyloses subchondral hyperintense signal on t1and t2 - weighted images , which is suppressed on fs or stir sequences bony appositions , end stage of disease with union across the joint 1 3 1156 la radiologia medica ( 2019 ) 124 : 11511166 these results support the inclusion of erosions in the definition of a positive mri finding for the classification of spa [ 6 , 2426 ]  . 
furthermore , sijs erosions were most prevalent in patients aged 1829years and bme in patients aged 3040years , whereas sijs sclerosis and fatty marrow deposition were most common in women . mri of the sijs commonly shows non - inflammatory disease in patients clinically suspected of si : 41% of patients with lbp had normal mri findings ; 36% of patients showed mri features compatible , according to asas criteria , with sacroiliitis in axial spa ( bme and erosions ) ; 21% of the patients showed bme ; and only 44% of these showed a diagnosis compatible with si according to the asas criteria ( bme and erosions )  . 
in order to detect such finding is suggested to obtain axial stir images from l5 to the lesser trochanter when performing mri of the si joint , much helpful than obtaining only semi - coronal sequences of the sijs , which may cause undetection of unexpected findings [ 22 ]  . 
5 axial tse t2w ( a ) and t1w ( b ) sequences and axial tse t2 ( c ) and corresponding sagittal stir sequences of the spine ( d ) show degenerative pathology of the articular facets . 
 articular hypertrophy with alteration of the loads on the facet with osteophytes , thinning of the joint space , bone marrow edema , soft tissue signal changes around the apophyseal joint 1 3 la radiologia medica ( 2019 ) 124 : 11511166 1157 fig . 
lumbar findings are in general more frequent than thoracic findings , and thoracic findings are reported to be more frequent than cervical findings or vice versa [ 27 ]  . 
7 sagittal stir ( a ) , coronal oblique spair t2w ( b ) , axial tse t2w ( c ) and spair t2w ( d ) demonstrate a normal aspect of sacroiliac synchondrosis in a 44 - year - old male patient with suspected sacroiliitis , compared to evidence of a left posterolateral hernia migrated posteriorly along the wall of s1 la radiologia medica ( 2019 ) 124 : 11511166 fig . 
8 transient osteoporosis of the hips in a 33 - year - old patient in the seventh month of pregnancy demonstrates a characteristic bone marrow edema of the cervico - cephalic region of both femurs , respectively , clockwise , in the axial stir sequences ( a ) , sagittal tse t1w ( b ) , coronal stir ( c ) and tse t1w ( d ) 1 3 la radiologia medica ( 2019 ) 124 : 11511166 1159 fig . 
9 coronal oblique spair t2w ( a ) and axial tse t2w ( b ) : left hemisacralized lumbosacral transition vertebra with reactive bone marrow edema and marginal sclerosis patients with degenerative changes . 
 the pathogenetic process begins with discal thinning and consequent cranial subluxation of the upper articular process onto the underlying vertebra versus inferior articular process of the overlying vertebra with alteration of the loads on the facet . 
mri findings are osteophytes , subchondral sclerosis , cysts ( fig.6 ) , thinning of the joint space , bme , fatty marrow deposition , soft tissue signal changes around the apophyseal joint . 
 inflammatory changes only 10% of patients who underwent mri for lbp show inflammatory changes in the column ( instead of 28% of patients who present inflammatory changes in sijs ) : bme / adipose replacement of somatic edges ( romanus vertebra ) , erosive changes within intervertebral space ( andersson lesions ) , chondroid metaplasia and enchondral ossification leading to syndesmophytes formation and vertebral fusion . 
 also , bme of costovertebral joints and apophyseal joint and edema in the insertion of thorny ligaments may be depicted . in particular , early spinal changes encompass erosion of vertebral corners ( romanus lesions ) causing vertebral squaring and eliciting reactive sclerosis ; these changes are caused by fig . 
10 ct axial scan in a 32 - year - old woman who had given birth to her second child 6months before affected by pain in the lower back and buttocks shows osteitis condensans ilii presenting as a bilateral sclerotic lesion , mainly in iliac bone adjacent to both sacroiliac joint with relative normal joint space ( no joint irregularity , erosions or loss of joint space is observed ) for vertebral endplate signal changes , it was noticed that the anterior location was the most common in the thoracic spine , while in the lumbar spine , widespread vertebral endplate signal changes were the most frequent . 
in the thoracic spine , the load is mainly on the anterior part of the motion segment due to the kyphosis and vice versa in the lumbar region due to the lordosis . 
 moreover , the lumbar segments have more degrees of freedom of movement , including sagittal angulation and axial rotation , making loading on the entire endplate possible in opposition to the thoracic spine , which has a limited range of motion due to the rib cage . 
the regional differences in the location of vertebral endplate signal changes found in the literature support the hypothesis that the occurrence of vertebral endplate signal changes is related to mechanical loading [ 28 ]  . 
fulfillment of the imaging arm of the asas criteria takes into account the presence of mri - documented inflammation only in the sijs , but not in the spine [ 29 ]  . 
in daily clinical practice , mri findings can be useful in confirming a clinical diagnosis of non - radiographic axial spa and detecting objective evidence of active inflammation in patients with an established diagnosis of non - radiographic axial spa . 
the literature agrees on the distribution of the dvu involvement along the spine with findings of thoracic and lumbar region of the spine being the areas most frequently affected by inflammation in axial spa [ 2934 ]  . 
according to the most recent literature , a positive mri spine ( the presence of 5 / 3 inflammatory lesion that is corner bme lesions ) was rare in patients without sacroiliitis on mri - si and x - ray - si . 
 addition of mri spine as imaging criterion to the asas axial spa criteria had a low yield of newly classified patients and is therefore not recommended [ 35 ]  . current concepts andapplication inaxial spa represents a diagnostic challenge being known that the diagnostic delay between the first symptoms and the certain diagnosis of the disease is around 8years . 
the reasons for this delay are essentially based on the difficulties of early 1 3 la radiologia medica ( 2019 ) 124 : 11511166 1161 ( defined as sacroileitis , term not properly correct because it implies a process of inflammatory nature that cannot be unveiled in traditional radiography , able to highlight structural lesions such as joint erosions and subchondral bone sclerosis )  . the new asas criteria [ 1 ] allow a more early classification and identification of the concept of nr - spa . 
it is therefore extremely important to have clinical diagnostic tools capable of addressing the diagnostic question of spa , especially of axial forms , also with a view to exploiting the therapeutic window of opportunity , which allows to obtain the best efficacy before the appearance of irreversible alterations . the recent recommendations for the use of imaging techniques in the diagnosis and management of spa in clinical practice [ 37 ] have produced ten evidence - based recommendations in monitoring of inflammation and structural damage , in outcome prediction , in response to treatment and in the detection of spinal fractures and osteoporosis . diagnostic criteria inaxial spa in general , conventional radiography of the sijs is recommended as the first imaging technique for the diagnosis of si in axial spa [ 38 ]  . 
a sagittal tse t1w image , hypointense bone marrow edema , b sagittal spair t2w image , hyperintense bone marrow edema diagnosis if the modified new york conventional criteria [ 36 ] are used , which require the obligatory presence of structural lesions of the sijs to the radiography of the pelvis fig . 
 a sagittal tse t1w image , hypointense bone marrow with sclerosis , b sagittal spair t2w image , hypointense bone marrow with sclerosis la radiologia medica ( 2019 ) 124 : 11511166 fig . 
15 a , b sagittal tse t1and t2 - weighted mr image shows typical characteristic of schmorls node located at the inferior endplate of l3 and l4 vertebrae on mr imaging . 
c sagittal stir sequence shows schmorls nodes located at the inferior endplate of l2 and superior endplate of l3 vertebrae : bone marrow edema and hemorrhagic infarction surround the herniation of the intervertebral disk nuclear material through the cartilaginous and body endplate into the body of the vertebra if the diagnosis of axial spa cannot be established by clinical characteristics and conventional radiography and there is still suspicion of axial spa , the mri of the sijs is recommended . 
injection of contrast media sequences of the spine demonstrate discitis of the l1l2 disk space with rime enhancement and osteomyelitis of the adjacent l1 and l2 vertebral bodies in patient affected by spondylodiscitis fig . 
injection of contrast media sequences of the intervertebral space demonstrate destruction of the disk space with rime enhancement and osteomyelitis of the adjacent vertebral bodies in patient affected by spondylodiscitis on mri might be observed in half the patients with nonradiographic axial spa without sijs inflammation . 
however , fulfillment of the imaging arm of the asas criteria takes into account the presence of mri - documented inflammation only in the sijs , but not in the spine . 
rheumatologists in clinical practice rightly dispute a diagnosis of axial spa even when there is a high number of spa features ( ibp , a positive family history of spa , a good response to nonsteroidal anti - inflammatory drugs , elevated c - reactive protein or erythrocyte sedimentation rate and enthesitis ) , especially when imaging is normal and patients are negative for hlab27 . 
the best knowledge in the use of instrumental methods associated with greater awareness of the clinics , supported by the irreplaceable comparison with radiologists , must be the objectives to be pursued in reducing the diagnostic delay and optimizing the care of patients with spondyloarthritis . 
18 sagittal tse t2w ( a ) and t1w ( b ) spine sequences in axial spa show a total bony bridge at the level of d10d11 ( c ) such as chondroid metaplasia phenomenon and enchondral ossification leading to syndesmophytes formation ( d ) la radiologia medica ( 2019 ) 124 : 11511166 sensitivity toward the spa , through a shared path on clinical findings and instrumental methods [ 40 ]  . response to therapy in sijs involvement in spa using the evaluation of enhancement [ 4244 ]  . the concomitant presence of pelvic enthesitis phenomena in more than one site on the mri examination of the axial skeleton during spa increases the specificity and the positive predictive value ( ppv ) in the diagnosis of spa , especially when the findings of sacroileitis are equivocal or absent . 
enthesitic sites with high ppv in the diagnosis of spa are the wings and the iliac crest and the posterior interosseous ligaments , while the great trochanter and the posterior spinal ligaments of the sacroiliac joints constitute enthesitic sites with less ppv ( fig.19 ) [ 41 ]  . other imaging techniques , in addition to conventional radiography and mri , are not usually recommended for axial spa diagnosis . 
bone scintigraphy and ultrasounds ( us ) are not recommended for the diagnosis of si in axial spa . monitoring oftheactivity intheaxial spa mri of the sijs and / or spine joints can be used to determine and monitoring disease activity in the axial spa , providing additional information to clinical and biochemical evaluations . 
in general , stir sequences are sufficient to detect inflammation and the use of contrast medium is not necessary , even though some recent articles have reported an improvement in the mri assessment of monitoring ofstructural changes intheaxial spa conventional radiography of si and / or spinal column joints can be used for the long - term monitoring of structural damage , particularly the formation of new bone , in axial spa . 
mri can provide further information . forecasting oftheoutcome / gravity intheaxial spa in patients with ankylosing spondylitis ( not with non - radiographic axial spa ) , a preliminary conventional radiograph of the lumbar and cervical spine is recommended to detect syndesmophytes , which are predictive of the development of new syndesmophytes . 
mri findings ( vertebral inflammatory lesions or adipose substitution ) could also be used to predict the development of new radiographic syndesmophytes . forecast ofthetreatment effect intheaxial spa the high inflammatory activity in mri ( bme ) , particularly in the column of patients with ankylosing spondylitis , could be predictive of a good clinical response to treatment with anti - tnf drugs in axial spa . 
thus , mri can help in the decision to initiate therapy with an anti - tnf , in addition to clinical examination and pcr . 1 3 la radiologia medica ( 2019 ) 124 : 11511166 1165 fig . 
 ( circles ) mri of the pelvis carried out with axial scan planes and stir sequences at the level of the main enthesis showingthe presence of bone edema as a sign of osteitis in patients affected by axial spondyloarthritis a possible comment on these indications , which represent an undoubted value in terms of actual practice , concerns that mri scan of the spine is not recommended for the diagnosis of axial spa . 
therefore , a global discussion on the subject through a systematic review of the literature and a meta - analysis is necessary . methods a systematic search of pubmed was performed up to april 23 , 2018 . 
studies exploring the role of pmcta in cases of sudden cardiac death and the accuracy of this method in diagnosing the cause of death compared to traditional autopsy were included . results the overall sensitivity and specificity of the seven included studies , using conventional autopsy as a reference standard , were 92% and 95% , respectively . 
however , pmcta can improve the performance of the autopsy , serving as an aid and guide in the sampling phase for histopathological investigations . keywords postmortem computed tomography angiography traditional autopsy sudden cardiac death coronary artery disease * vittorio fineschi vfinesc@tin.it 1 department ofanatomical , histological , forensic andorthopaedic sciences , sapienza university ofrome , viale regina elena 336 , 00161rome , italy irccs neuromed , via atinense 18 , pozzilli86077 , italy 3 department ofradiological sciences , oncology andpathology , sapienza university , viale regina elena 324 , 00161rome , italy introduction sudden cardiac death ( scd ) has been defined as a natural , unexpected fatal event occurring within 1h from the onset of symptoms in an apparently healthy subject or in one whose disease was not so severe as to predict an abrupt outcome . 
the incidence of scd increases with age , in line with the increase in the incidence of the coronary artery disease which , according to numerous studies , represents the pathology most frequently involved in the determinism of sudden death ( sudden coronary death ) [ 1 , 2 ]  . postmortem examination and autopsy represent reliable methods for determining the causes of scd [ 3 , 4 ]  . 
 however , due to ethical , religious , cultural , economic and organizational reasons , the number of autopsies performed vol . : ( 0123456789 ) 1 3 110 la radiologia medica ( 2019 ) 124 : 109117 is decreasing worldwide and the use of minimally invasive ancillary methods is considered preferable in some circumstances . in view of these circumstances , postmortem cardiac imaging is assuming increasing importance in the study of myocardium and coronary arteries as an aid and guide in the execution of conventional autopsy and , sometimes , as an alternative [ 5 , 6 ]  . currently , postmortem computed tomography ( pmct ) , postmortem computed tomography angiography ( pmcta ) , postmortem magnetic resonance ( pmmr ) and postmortem magnetic resonance angiography ( pmmra ) have become established methods due to numerous studies that have documented the undeniable advantages in terms of acquisition times , costs and possibility to review the data acquired at any time [ 713 ]  . a series of studies have been performed over the years to assess the efficacy of pmcta in solving cases of sudden cardiac death , even in comparison with the traditional autopsy . 
the pubmed section similar articles and the references of the selected articles were used to expand the research . inclusion andexclusion criteria studies were included if they met the following criteria : ( 1 ) population consisting of persons who died of suspected sudden cardiac death ; ( 2 ) evaluation of the accuracy of pmcta in diagnosing the cause of death and in detecting major or minor diagnostic findings ; ( 3 ) comparison of the efficacy of pmcta with the gold standard , the conventional autopsy ; ( 4 ) availability of the entire panel of true positives ( tp ) , false positives ( fp ) , false negatives ( fn ) and true negatives ( tn ) , or sufficient data to calculate themeanwhile , studies were excluded if they were : ( 1 ) case reports ; ( 2 ) not original research , such as review articles ; ( 3 ) studies conducted on fetuses . data extraction andassessment data from each included study were extracted using microsoft excel spreadsheets , including information on authors , journal , publishing years , nation , population selection criteria , sample size , gender , age , diagnostic technique under examination , reference standards , as well as results in terms of tp , fp , fn and tn . the quality of the individual studies was determined through the quadas - 2 ( quality assessment of diagnostic accuracy study ) tool , structured in four key domains : ( 1 ) patient selection ; ( 2 ) index test ; ( 3 ) reference standard ; and ( 4 ) flow and timing . 
the studies were considered at low risk of bias if the population selection criterion was clear , if the radiologist and forensic pathologist operated in double - blind , if they both had access to the same information about the case and if the interval between performing the imaging exam and the autopsy was less than 72h . 
the studies were considered at moderate risk of bias in the presence of at least one of the following conditions : ( 1 ) unclear selection , ( 2 ) knowledge by the radiologist or the forensic pathologist of the other test results , ( 3 ) latency time between the two investigations exceeding 72h . 
the studies were considered at high risk of bias in the presence of two or more of the previously indicated conditions . statistical analysis the meta - analysis was conducted using stata 13.0 ( stata corporation , college station , texas , usa ) [ 1619 ]  . 
the 1 3 la radiologia medica ( 2019 ) 124 : 109117 results in terms of tp , fp , fn and tn were used to calculate the sensitivity and specificity in each of the primary studies . 
the sensitivity and specificity values of the individual studies were graphically represented in a forest plot using the meta - disc software ( unit of clinical biostatistics , ramn y cajal hospital , madrid , spain )  . 
for the synthesis of the results on the pmcta performances , two random effect models were used : the bivariate model and the hsroc ( hierarchical summary receiver operating characteristic ) model . results included studies by applying the search strategy mentioned above , we found a total of 793 studies in pubmed . 
 the process of study inclusion is illustrated in fig.1. the sample size ranged between 5 and 38 with a total of 127 subjects ; the publication time was from 2010 to 2014 . 
the risk of bias was globally low or unclear in the four domains except for the reference standard ; the latter was at high risk in two studies because the autopsy was performed by a pathologist aware of the results of radiological investigations . 
therefore , four studies were considered at low risk of bias , one at low / undefined risk and two at moderate / undefined risk ( table2 )  . qualitative analysis ( systematic review ) bolliger etal . 
 [ 20 ] evaluated the diagnostic accuracy of a minimally invasive approach ( pmct , pmcta , ct - guided biopsy ) in 20 cases of apparently natural death of which 11 of sudden coronary death . 
 [ 23 ] radiology ( 2012 ) international journal of selective coronary pmcta 77 ( range 4292 ) 56 ( range 1580 ) whole body pmcta 16 : 4 52.3 ( range 3789 ) 21 : 2 whole body pmcta morgan etal . 
in 8 cases , there was complete agreement between the data obtained from the two tests , while in one case radiological investigations had overestimated the severity of a stenosis that was considered nonsignificant to autopsy . 
 [ 22 ] have shown a concordance between conventional autopsy and pmcta associated with ct - guided biopsy in 20 cases of sudden death after chest pain 8 of the 9 cases of sudden coronary death , the pmcta had been able to highlight the alterations responsible for the death , while in one case , early myocardial infarction of the papillary muscles had been missed . pmcta allowed an excellent visualization of the coronary arteries and a better evaluation of stenosis and occlusions . 
regarding the detection of coronary disease , pmcta and autopsy showed complete concordance in identifying at least one area of critical stenosis in each case ; however , 18 discrepancies were recorded , including 5 major and 13 minor . 
in 18 cases , 1 3 la radiologia medica ( 2019 ) 124 : 109117 both the autopsy and the pmcta showed coronary lesions that only in 11 cases were causally related to death . 
3 forest plot of specificity 1 3 114 la radiologia medica ( 2019 ) 124 : 109117 in conventional postmortem investigations , the diagnosis of coronary artery disease or ischemic heart disease is obtained after a complete autopsy followed by a gross examination of the heart and a microscopic examination with histological and immunohistochemical staining . 
nevertheless , such investigations require the experience of the pathologist and the application of a rigorous methodological approach to the complex task represented by sudden cardiac death . postmortem imaging provides a decisive contribution to forensic pathology , its importance is widely recognized , and its use is increasingly common in forensic practice [ 27 ]  . 
this consideration assumes remarkable significance in light of the importance of imaging methods in the approach to cases of sudden cardiac death [ 28 , 29 ]  . computed tomography ( ct ) is the most widely used method in modern forensic radiology . 
despite the extensive use of this type of investigation , the method presents two major limitations consisting of the low density of soft tissues and the poor visualization of vascular structures . 
in fact , in the included primary studies that required the execution of a scan without contrast medium before pmcta , pmct did not prove useful in the diagnosis of coronary heart disease , being able only to highlight findings such as cardiac tamponade or calcifications of coronary arteries . post - mortem ct angiography ( pmcta ) , on the other hand , is a minimally invasive procedure , able to show direct ( coronary stenosis or occlusions ) and indirect ( contrastographic enhancement of the myocardium as a sign of ischemic necrosis ) evidence of coronary artery disease with a much higher diagnostic accuracy than unenhanced pmct [ 30 , 31 ]  . the main advantage of pmcta is the possibility of visualizing myocardial bridging and alterations of luminal patency without altering the examined vascular structure , as it inevitably occurs during the conventional investigation . 
in fact , pmcta studies the vessels throughout their course allowing to identify even small areas of critical stenosis that could be missed by the sections carried out during the autopsy . 
in addition , pmcta has shown to be superior to autopsy in investigating the patency of coronary vessels as it is able to demonstrate through perfusion pressure the patency of calcific vessels that had been described as occluded at the autopsy . post mortem ct angiography also allows the study and three - dimensional evaluation of coronary artery bypass grafts and coronary stents , [ 32 , 33 ] facilitating the forensic pathologist in the identification of findings difficult to highlight during autopsy due to the adhesion phenomena attributable to the surgical manipulation of the pericardium and heart . 
5 bivariat model of sensitivity and specificity 1 3 la radiologia medica ( 2019 ) 124 : 109117 the main limitation of pmcta is the impossibility of providing data on the functional relevance of a stenosis , being an exclusively morphological imaging technique . 
 the included primary studies have also shown that only a relatively low percentage of ischemic myocardial necrosis was detectable by pmcta as a contrast enhancement area , documenting a sensitivity limit of this method compared to the histopathological evaluation or other imaging techniques such as pmmr . 
on the other hand , the tomographic scans are limited by the impossibility of visualizing the vessels downstream of the stenosis and by the difficulty in ascertaining the acute or chronic nature of the stenosis . 
a further doubt about the diagnostic efficacy of pmcta could derive from the possibility of a thrombus displacement following coronary artery reperfusion , with consequent failure to visualize coronary occlusion ; although the hypothesis cannot be refuted with certainty , several studies have reported as unlikely the possibility that a perfusion pressure lower than the invivo one can determine the displacement of a thrombus . the present systematic review and meta - analysis demonstrated the high accuracy of pmcta in the diagnosis of sudden coronary death . 
post mortem ct angiography represents a valid tool for the assessment of coronary arteries anatomy , for the detection of stenosis and occlusions , [ 34 ] as well as for the guide of sampling for histological examination . 
at the same time , however , this method has proved less effective in the visualization of myocardial ischemia and necrosis . there are two major limitations concerning the present study . 
first , the meta - analysis was performed on a small number of primary studies , many of which had a small population and did not provide enough information to clearly determine the quality of the study . 
therefore , even if an hsroc model was used for data analysis , the results should be interpreted carefully . for these reasons , to date , autopsy followed by histological examination remains the gold standard for the diagnosis of sudden coronary death . 
in fact , pmcta is extremely useful in cases where a minimally invasive approach is required for several reasons or in cases where a guide to myocardial and coronary sampling is required during the autopsy . in conclusion , in the field of cardiac pathology , postmortem coronary imaging is still insufficient to establish with certainty the cause of death and autopsy remains the gold standard . 
currently , in fact , no radiological technique can replace the histological examination . the value of this study is in the combination of data from several studies resulting in the evaluation of a larger cohort of subjects as well as in obtaining data more applicable to forensic practice . 
nevertheless , further studies are still required to offer better evidence on the use of pmcta as a routine investigation or as an aid to conventional autopsy . the role of pmcta in cases of sudden cardiac death is that of guidance and aid to traditional autopsy . 
in particular , this investigation can determine an increase in diagnostic performance and ensure a better evaluation of the coronary arteries as well as a more accurate coronary and myocardial sampling [ 3640 ]  . for these reasons , postmortem computed tomography angiography must be considered an ancillary method in determining the cause of sudden cardiac death , rather than an alternative to conventional investigations [ 41 , 42 ]  . authors contribution all authors contributed to manuscript drafting and critical discussion and approved the definitive version . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . 
we also attempted to identify a relationship between mdct imaging and the 2010 world health organization ( who ) classification system . materials and methods we selected all patients with pathologically proven gi - nets diagnosed between january 2010 and august 2017 . 
we also analysed the relationship between mdct imaging and the 2010 who classification . results a total of 20 patients ( 13 males , 7 females , age range 3789years , mean age 69.9years ) were included in our study . 
 the majority of gi - nets ( 85% ) occurred in the small bowel and mainly in the terminal ileuforty - five percentage of our gi - nets were diagnosed after an access to emergency medical service for obstruction symptoms or gastrointestinal bleeding . 
desmoplastic reaction and lymph nodes metastases were significantly correlated with higher grade of gi - nets . conclusions the majority of gi - nets appears as intraluminal mass often associated with extra - intestinal signs . 
contrast - enhanced mdct has allowed an optimization of scan protocols , with many advantages , including ( 1 ) very rapid scan times reducing movement artefacts ; ( 2 ) contrast - enhanced images with arterial and portal phase and ( 3 ) the ability to reformat the images in thinner slices , in order to improving resolution and allowing the images to be viewed optimally in different anatomical planes . 
for these reasons , contrast - enhanced mdct is the main imaging modality for diagnosis , staging , preoperative evaluation and post - treatment follow - up of net [ 24 ]  . 
mdct images of gi - nets usually appear as a hyper - enhancing nodular mass arising from the bowel wall or as a regional uniform bowel wall thickening [ 4 , 5 ]  . 
the world health organization ( who ) classification system of 2010 attempted to grade gi - nets on the basis of their ki - 67 index and mitotic count , dividing these tumours into well - differentiated neuroendocrine tumours ( grades 1 and 2 , ki - 67 index < 2% and 320% , respectively ) , also termed carcinoid tumours , and poorly differentiated neuroendocrine carcinomas ( grade 3 , ki - 67 > 20% ) [ 610 ]  . 
we also attempted to identify a relationship between mdct imaging and the 2010 who classification system . materials andmethods patients with a query ( gastrointestinal and neuroendocrine tumours ) of the patients medical records database at the careggi hospital of florence , a radiologist resident selected all patients with pathologically proven gi - nets diagnosed between january 2010 and august 2017 . 
 all patients signed a written consent form . all ct investigations were carried out on a 64 - detector helical ct ( somatom sensation 64 , siemens healthcare , germany )  . a standard protocol was used : the patients were scanned in supine with craniocaudal breath - hold scans ; all cases underwent non - contrast and contrast - enhanced mdct scanning with a thickness of the scanning slices of 3 or 5m iodinated contrast medium ( ultravist 300 , bayer schering , berlin , germany ) was injected in the antecubital vein at a flow rate of 34ml / s using an automatic injector , immediately followed by a saline flush ( 4050ml ) with a rate of injection of 34ml / s . 
dual - phasic contrast - enhanced images were obtained during the arterial phase ( 3035s after the start of the injection ) and portal venous phase ( 7075s after initiation of the injection )  . the parameters for both non - contrast and contrastenhanced ct examination were : tube voltage , 120kv ; tube current , 200250 mas , depending on the patients size ; beam collimation , 64 0.5mm ; and rotation time , 0.4s. imaging analysis all gi - nets were retrospectively assessed for the mdct intestinal and extra - intestinal signs . 
the readers were blinded to the clinical and pathological data of all of the patients . among intestinal signs , we evaluated morphological features , classifying the lesions as the following , in accordance with the existing literature [ 4 , 5 , 11 ] : intraluminal nodular mass arising from the bowel wall and regional uniform bowel wall thickening . the extra - intestinal signs included mesenteric metastasis surrounded by a desmoplastic reaction , ascites , lymph nodes and liver metastases . 
in accordance with the existing literature [ 5 , 12 ] , we classified as mesenteric metastasis a mass - like process generally located in the mesenteric fat near to the primary tumour , which may or may not be calcified . 
these signs were classified as the classic desmoplastic reaction that could lead to kinking of the bowel , resulting in bowel obstruction , or in venous ischaemia [ 5 , 12 , 13 ]  . 1 3 96 pathological classification histopathological classification of gi - nets was made according to who 2010 guidelines [ 610 ] as : grade 1 ( g1 ) , mitotic count < 2 per 10 high - power fields ( hpf ) and / or ki - 67 2% ; grade 2 ( g2 ) , mitotic count 220 per 10 hpf and / or ki - 67 320% ; and grade 3 ( g3 ) , mitotic count > 20 per 10 hpf and / or ki - 67 > 20% . statistical methods graphpad prism v7.0 software ( graphpad software inc . , la jolla , ca , usa ) was used to perform all statistical analyses . 
 among these , eight patients did not undergo contrastenhanced mdct in the immediate preoperative period and three patients were excluded for poor mdct image quality . a total of 20 patients ( 13 males , 7 females , age range 3789years , mean age 69.9years ) were included in our study . of the 20 cases , 3 ( 15% ) were duodenal neuroendocrine tumours and 17 ( 85% ) were small - bowel neuroendocrine tumours , defined as tumours of the jejunum and of the ileum [ 14 ]  . 
three patients complained weight loss and abdominal pain as their first symptovomiting was present in two cases , and only one patient showed jaundice due to the presence of a periampullary duodenal tumour . 
finally , in two cases , gi - nets were discovered incidentally by mdct imaging studies performed during follow - up of a lung cancer and of a breast cancer , respectively , ( table1 )  . mdct andhistopathological findings mdct findings of each patient are shown in table 2 . 
axial ( a ) and coronal ( b ) contrast - enhanced mdct images in the arterial phase demonstrate a wellcircumscribed enhancing mass ( white arrows ) in the ileocecal valve 1 3 la radiologia medica ( 2019 ) 124 : 94102 fig . 
axial ( a , b ) , sagittal ( c ) and coronal ( d ) contrastenhanced mdct images in the arterial phase demonstrate multiple intraluminal masses ( white arrows ) fig . 
arterial phase ( c ) and portal venous phase ( d ) contrast - enhanced mdct show multiple hyper - vascular liver metastases that become almost isodense on the portal venous phase except for central regions of necrosis . 
5 gastrointestinal neuroendocrine carcinoma ( g3 ) in the terminal ileuaxial contrastenhanced mdct image in the portal venous phase ( a ) demonstrates a bowel wall thickening of the terminal ileum and a stellate soft - tissue nodule ( white star ) in the mesentery , typical of a desmoplastic reaction . 
there were no statistically significant differences in intestinal signs , liver metastases and ascites ( table3 )  . discussion in the last 20years , the incidence of gi - net has increased probably due to recent improvements in diagnostic techniques such as the diffusion of thin - section multi - detector ct . 
although nets can occur in any organ , approximately 6070% of these tumours arise in the gastrointestinal tract because it has the largest reservoir of neuroendocrine cells in the body [ 15 ]  . 
studies analysing data from 1973 to 1997 found that the most common site of gi - nets is the small bowel , defined as jejunum and ileum [ 16 ]  . 
our study confirmed that the majority of gi - nets ( 85% ) occurs in the small bowel and mainly in the terminal ileum . at the time of initial diagnosis , half of the patients with gi - nets have advanced disease [ 17 ] , with metastases to the regional lymph nodes , liver and , finally , bone [ 18 , 19 ]  . 
in addition , the carcinoid syndrome occurs in the presence of liver metastases because only with hepatic metastatic disease the biologically active metabolite ( 5 - hydroxy - tryptamine ) , which is otherwise inactivated in 1 3 la radiologia medica ( 2019 ) 124 : 94102 100 fig . 
6 neuroendocrine tumour ( g2 ) in the terminal ileu axial ( a ) and coronal ( c ) contrast - enhanced mdct images demonstrate a bowel wall thickening of the terminal ileum ( white arrows ) : the thickened wall is homogeneously enhanced . 
the presence of the characteristic carcinoid syndrome can facilitate nets detection , otherwise patients present non - specific symptoms , such as weight loss , bleeding or abdominal pain or are asymptomatic [ 20 , 21 ]  . 
 this result demonstrates how the radiologists should suspect gi - nets also in the emergency setting . in mdct , after administration of contrast medium , the primary tumour usually presents as a hyper - enhancing , nodular mass arising from the bowel wall or as a regional uniform bowel wall thickening [ 4 , 5 ]  . 
similar to their results , we observed intraluminal nodular mass in 75% of our patients and wall thickening in 25% . a very typical extra - intestinal finding in gi - nets is the mesenteric metastasis , which generally appears as a masslike process in the mesenteric fat near the primary tumour . 
 we observed desmoplastic reaction in 40% of cases , lymph nodes metastases in 60% , liver metastases in 45% and ascites in 35% . the who 2010 classification system is currently wellaccepted by clinicians as a simple , reproducible , and prognostic effective grading of gi - nets , since the who classification from 2017 is only for pancreatic net ( p - nets ) [ 6 ]  . 
the who classified gi - nets into well - differentiated tumours with benign or uncertain behaviour ( g1 ) ; welldifferentiated tumours with low - grade malignant behaviour ( g2 ) ; and poorly differentiated carcinomas with high - grade malignant behaviour ( g3 ) [ 610 ]  . 
in recent literature , concerning 1 3 la radiologia medica ( 2019 ) 124 : 94102 gi - nets , no correlation between imaging features and grading of pathologic classification is reported . 
our results indicated that mdct imaging features may be predictive of gi - nets classifications . in our series , all g1 tumours appeared as intraluminal mass while 50% of g3 tumours showed a bowel wall thickening as intestinal sign . 
nevertheless , no statistically significant differences were found in intestinal signs . comparing mdct and histopathological findings , we found statistically significant difference among g1 , g2 and g3 tumours in desmoplastic reaction and lymph nodes metastases . 
this is likely due to the fact that the pathological grading criteria were established based on the mitotic count and ki - 67 index , both of which reflect the proliferation and invasiveness of tumour cells [ 23 , 24 ]  . several criticisms may be raised with respect to our study . 
second , although we examined gi - nets between january 2010 and august 2017 , our sample size is rather small consisting of 20 patients because patients did not undergo contrast - enhanced mdct in the immediate preoperative period or with poor mdct image quality were excluded . 
thus , it may be possible that the distribution of grading correlation we found is different in a more general population . in conclusion , as confirmed in the literature , our study showed that the majority of gi - nets appears as intraluminal nodular mass often associated with extra - intestinal signs on mdct imaging . on the other hand , we found a statistically significant correlation between higher grade of gi - nets and extra - intestinal signs , not previously demonstrated . 
therefore , mdct imaging is a technique that may be useful in predicting the pathological classification of gi - nets . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . 
no funding was received for this study . ethical approval all procedures performed in the studies involvement human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 132135 radiotherapy fiducial markers implantation forprostate imageguided radiotherapy : areport onthetransperineal approach luigidecicco1 stefanobracelli1 received : 21 may 2018 / accepted : 15 october 2018 / published online : 25 october 2018 italian society of medical radiology 2018 abstract introduction in the external beam prostate cancer radiation therapy , daily gland displacement could lead to a target missing . 
the use of intra - prostatic gold fiducial markers for daily prostate position verification and correction before and during treatment delivery ( image - guided radiotherapy , igrt ) is widely used in the radiation therapy centers to accurately target the prostate . 
we report our experience in prostate fiducial markers implantation through a transperineal approach . patients and methods between september 2011 and january 2018 at our center , 101 patients underwent gold seed fiducial marker transperineal ultrasound - guided implantation for prostate igrt . 
no markers lost or migration occurred . discussion and conclusion according to our experience , prostate fiducial markers implantation through a transperineal approach is safe and should be recommended to limit the use of antibiotic therapy and patients morbidity . 
a previous turp was not related to a higher risk of loss of seeds . keywords prostate cancer radiotherapy fiducial markers image - guided radiotherapy prostate radiotherapy introduction in the external beam prostate cancer radiation therapy , daily gland displacement could lead to a target missing . 
prostate pelvic motion up to 2cm are reported , so that the use of intra - prostatic gold fiducial markers for daily prostate position verification and correction before and during treatment delivery ( image - guided radiotherapy , igrt ) is widely used in the radiation therapy centers because accurately targeting of the prostate allows margin reduction , sparing normal tissue treated and thereby reducing complications , [ 1 , 2 ] without affecting tumor control and allowing dose escalation . 
 gold fiducial markers are considered an accurate , reliable and tolerable method of daily prostate localization [ 3 ]  . the most commonly used implantation procedure involves transrectal ultrasound - guided insertion of fiducial markers , with no negligible complications such as infections , pain and rectal bleeding . we report our experience in prostate fiducial markers implantation through a transperineal approach ; it is very similar to radioactive seed implantation for low - dose - rate brachytherapy . patients andmethods * luigi de cicco luigi.decicco@yahoo.it 1 department ofradiation oncology , asst della valle olona , via a . 
da brescia , 1 , 21052bustoarsizio , va , italy between september 2011 and january 2018 at our center , after a written consent acquisition , 101 patients underwent gold seed fiducial markers transperineal ultrasound - guided implantation for prostate igrt , performed by a referring vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 132135 radiation oncologist with proper skills in prostate brachytherapy ( dcl )  . 
one marker was placed in the prostate base , one at the apex and one in the middle ; two seeds were released in a prostatic lobe and one in the other one . of each fiducial , were acquired and printed two orthogonal ultrasound images to record the correct intra - prostatic position . in one patient , one seed was detected through the prostatic capsule with a higher risk of lost , so a fourth seed was implanted into the gland . after the procedure , patients remained under observation for about 2h and were encouraged to drink water and to urinate into a container to detect a possible hematuria . 
after 2h and at least two voids , the patients were re - evaluated in relation to any dysuria , or pabefore discharge , they were instructed to contact the referring radiation oncologist if there were any complications or variation in the urinary framework or pain . the planning tc was performed at least 7days later . 
during radiation treatment , daily cone - beam ct or orthogonal kv / mv was used to verify the correct position of the target and monitor the number of the markers and distance between them . in 3 ( 7% ) patients the antiplatelet oral therapy was not interrupted ( table1 )  . all the 101 procedures of fiducial markers implantation through the perineum under transrectal ultrasound guidance were uncomplicated . 
no procedure was interrupted because of unsustainable patient pain . in one patient , that have stopped antiplatelet oral therapy 7 days before the procedure , a singleepisode of self - limiting urinary bleeding occurred just after implantation . 
all the patients , at the evaluation before discharge , reported no pain or dysuria . no rectal bleeding , no urinary obstruction or infection and no episode of hematospermia were reported in the next days . all patients started radiation therapy as planned , without any delay . during the subsequent phases of the radiation treatment , all the implanted markers were detected within the prostate gland ; no markers lost or migration grater than 2mm occurred . discussion andconclusion the insertion of intra - prostatic markers for igrt is commonly used to track the prostate gland before and during radiation treatment delivery to reduce margin around prostate , sparing surrounding organs and escalating dose to the tumor . 
the transrectal implantation way is the widely used one because this procedure is commonly carried out by urologists and this approach requires the same equipment used for the prostatic biopsies , so that , likewise to transrectal prostate biopsy , no negligible complications such as infections , pain and rectal bleeding are expected . an increasing incidence of multidrug resistant infections is reported in the transrectal prostate biopsy that is similar to the transrectal seed implantation procedure , with febrile infection rates commonly ranging from 1 to 4% despite the prophylactic antibiotic therapy [ 4 ]  . results median age of the 101 patients was 75years ( range 5384 )  . twenty - two ( 21.8% ) patients had previously been subjected to a transurethral prostate resection ( turp ) for obstructive urinary symptoms because of benign prostatic hypertrophy . forty - three ( 42.6% ) patients were in anticoagulant or antiplatelet oral therapy . 
according to their cardiovascular risk , in 13 patients of this group ( 30% ) these medications were stopped , in 27 ( 63% ) patients were replaced with low molecular weight heparin 710days before the implant , and table 1 characteristics of patients median ( age ) 75years ( range 5384 ) no of patients ( % ) previous turp in anticoagulant or antiplatelet therapy 1 . 
3 ( 7% ) turp transurethral prostate resection , ebpm low molecular weight heparin 1 3 134 la radiologia medica ( 2019 ) 124 : 132135 there are increasing concerns about the incidence of serious infection associated with this procedure , in tandem with a rise in the prevalence of rectal ciprofloxacin - resistant organisms ( cro )  . 
reported a relatively high rate of seeds loss , implanting four markers in two strands with two fiducial each one , 1cm apart ; the two strands of the two markers were located on the same plane in the middle of the prostate , at least 2cm apart from the midline . 
 all intra - prostatic fiducials were usefully used to track the prostate gland before and during treatment [ 10 ]  . the first report on the transperineal markers implantation technique was on a little group of 12 patients ; no infective episodes occurred , but a mild rectal bleeding associated with significant pain resulted from the procedure in the initial half of the series , maybe related to the lower experience of the operator in this part of the learning curve [ 12 ]  . a seed loss in igrt could compromise the correct continuation of the treatment . 
it could be related to the implantation technique or operator experience ; seed misplacing had been reported more frequently in the first group of implanted patients [ 12 ]  . 
several authors had already highlighted the importance of avoiding the urethra and releasing the seeds only when the tip of needle has sure penetrated the capsule , considering the tending of the prostate by the needle , to avoid their loss [ 2 ]  . transperineal ultrasound - guided prostate fiducial markers implantation is very similar to radioactive seed implantation for low - dose - rate brachytherapy ; seed loss through the urinary tract is a common event after prostate brachytherapy ; and it is significantly more frequent in patients with prior turp [ 13 ]  . 
no previous report regarding the implant of seeds for igrt shows the presence or absence of previous turp among the characteristics of the patients ; it could be related to rate of loss of seeds reported in these series . no gold implanted seed was lost in our experience . 
 according to our knowledge , no previous report exists on the prostate fiducial markers implantation in patients with a previous turp ; it should not be considered a contraindication to the procedure , because in our series sparing the cavity linked to the previous turp avoided the risk of seeds loss . according to the literature data , in our series the fiducial markers implantation into the prostate gland through a transperineal approach resulted in a very low rate of complications . 
avoiding to cross the rectum , the risk of rectal bleeding or infections is very limited , the use of antibiotic prophylaxis can be omitted , and the start of radiation treatment is not delayed . 1 3 la radiologia medica ( 2019 ) 124 : 132135 no antibiotic prophylaxis was adopted in our series resulting in no infective event in 101 procedures . despite the high number of patients in anticoagulant or antiplatelet therapy ( 42.6% ) , due to the high median age ( 75years ) and the consequent frequent comorbidities , a low incidence ( 1% ) of self - limiting hematuria ( a single episode ) and no case of hematospermia were recorded . our detected low risk of bleeding agrees with other bibliographic experiences previously reported ; moman etal . 
 [ 9 ] do not advise discontinuation of anticoagulant therapy to their patients because the risk of bleeding is considered inferior to the impact of possible blood clot formation , and no severe bleeding has occurred in the past years . no worsening of baseline urinary obstruction symptoms was reported by the patients . 
all the patients after the procedure referred no persistent pain our series , no systemic analgesic drug was administered before the procedure , but only local anesthesia with mepivacaine injection was enough to tolerate it ; no drug was necessary after it . according to our experience , prostate fiducial markers implantation through a transperineal approach is safe even in patients with a previous turp , in anticoagulant or antiplatelet therapy , and advanced age ; it should be also recommended to limit the use of antibiotic therapy and patients morbidity . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this is a retrospective study . 
future studies are needed to confirm our findings . keywords prostate lesion magnetic resonance imaging ivim perfusion prostate cancer is the most common cancer in men ( after skin cancer )  . 
during progression switch , prostate cancer induces angiogenesis and vasculogenesis , and as a result , it shows rapid contrast enhancement and washout in dynamic contrast - enhanced mri sequences [ 5 ]  . 
it has clearly shown that diffusionweighted images with high b value ( 2000s / mm2 ) improve detection of prostate cancer , but there is an ongoing controversy in the literature related to the value of intravoxel incoherent motion ( ivim ) imaging [ 7 , 8 ]  . 
since the rate of signal attenuation resulting from perfusion is typically an order of magnitude greater than from molecular diffusion in tissues because of larger vol . : ( 0123456789 ) 1 3 88 la radiologia medica ( 2019 ) 124 : 8793 distances of proton displacement during the application of the pulses , its relative contribution to the diffusion - weighted mri signal becomes significant only at very low b values [ 9 , 10 ]  . dce - mri uses compartmental pharmacokinetic models of tracer kinetics to describe the microscopic processes leading to the distribution of molecules of contrast agent between the vascular and extravascular spaces . 
time dependence of contrast agent concentration was applied to calculate contrast agent transfer rate between blood and tissue ( ktrans ) , contrast agent back - flux rate constant ( kep ) , extravascular extracellular fractional volume ( ve ) , initial area under curve ( iauc ) and 2 values ( tofts model )  . 
due to sensitivity to contrast media , dynamic contrast - enhanced imaging table 1 acquisition parameters of the multiparametric mri protocol was not performed in 3 patients , and due to image distortion , 2 patients were excluded from the study . 
dcemri was performed with a 3d volumetric t1 - weighted gradient echo sequence using the view - sharing undersampling technique twist ( time - resolved angiography with stochastic trajectories )  . 
using an automated injector ( spectris solaris , medrad , indianola , pa ) , 0.1mmol / kg bolus of gadolinium - based contrast agent was injected intravenously , followed by 20ml saline flush , both at a rate of 2ml / s . 
mri parameters are shown in table1 . dwi data in a dicom format were transferred to a standard personal computer running an in - house - developed software package ( firevoxel , .nyu.edu / hr18 / publi c ) ( 12 )  . 
 [ 9 ] : sbs0 = ( 1 f ) exp ( bd ) + f exp [ b ( d + d ) ] where sb is the signal intensity in the pixel with diffusion gradient b , s0 is the signal intensity in the pixel without diffusion gradient , d is the true diffusion as reflected by pure molecular diffusion , f is the perfusion fraction related to microcirculation , and d * is the pseudodiffusion coefficient representing perfusion - related diffusion or incoherent microcirculation [ 12 ]  . the methods , formulas and parameters we used in our study are as follows : and prostate intraepithelial neoplasia were accepted as malignant . statistical analysis data were analyzed using the statistical package for the social sciences version 20.0 for windows ( spss inc . , chicago , il , usa )  . 
all patients underwent histopathological analysis , and cases with prostate cancer the normal peripheral zone ( pz ) was considered to show a homogeneously high - intensity signal on the t2 - weighted images . 
the voi placed ( b ) on lesion and the ktrans fusion map ( c ) and concentration curve and values ( d ) showed high ktrans , kep , ve , iauc and 2 values . 
two patients ( gleason 7 and gleason 9 ) had extraprostatic extension . discussion in our study , we found that the ivim diffusion and dynamic contrast - enhanced parameters of malignant tumors in peripheral zone and transitional zone differ . 
there was a significant difference between malignant transitional zone lesions and benignnormal transitional zone tissue for all parameters except kep , whereas there was no significant difference between malignant peripheral zone lesions and benignnormal peripheral zone tissue for ve , f and dp values . 
 the f ( perfusion fraction ) in the prostate cancer was significantly lower than that in the normal transitional and 1 3 92 la radiologia medica ( 2019 ) 124 : 8793 fig . 
the voi placed ( b ) on lesion and the ktrans fusion map ( c ) and concentration curve and values ( d ) showed low ktrans , kep , ve , iauc and 2 values . 
there were no significant differences in the normal transitional and peripheral zones , benign tissue and prostate cancer for the dp ( perfusion - related diffusion coefficient ) [ 7 ]  . 
our study showed that dp , dt and f values were significantly lower for transitional zone tumors , but dp and f values were not significantly lower for peripheral zone tumors . 
we also showed that lower dt values are important to diagnose prostate cancer in both transitional zone and peripheral zone . we also found that perfusion parameters ktrans , kep and iauc were significantly higher for peripheral zone malignant tumors , and ktrans , ve and iauc were significantly higher for transitional zone tumors . 
also found higher ktrans , kep , ve and iauc values in malignant lesions and stated that higher iauc is strongly correlated with prostate malignant lesions [ 13 ]  . this study has several limitations . 
third , we accepted premalignant lesions ( hgsil , high - grade squamous intraepithelial lesions , and asap , atypical small acinar proliferation ) as malignant that might influence our results . 
finally , we did not use endorectal coil in our study since in prostate imaging guidelines , it is only recommended but not a must . 1 3 la radiologia medica ( 2019 ) 124 : 8793 conclusion in conclusion , both restricted diffusionpseudodiffusion and increased perfusion parameters ( especially ktrans and iauc ) are important to differentiate prostate cancer from benign pathologies . 
the aim of this study was to evaluate the tissue stiffness values of pgs of hiv - infected children via swe and compare the results with the counterparts of healthy subjects . materials and methods this single - center , prospective study included the pg examinations of 23 pediatric hiv patients and 40 healthy children via grayscale ultrasound and swe . 
in addition , when the patients were separated into two groups according to the appearance of pg on grayscale ultrasound as homogeneous and heterogeneous , stiffness values were increased in the patients with homogeneous parenchymal appearance . 
swe can be used as an ultrasound - assisted noninvasive technique in this manner . keywords human immunodeficiency virus infection parotid gland shear wave elastography children introduction the association of parotid gland involvement with human immunodeficiency virus ( hiv ) infection has been reported soon after the first description of hiv infection [ 1 ]  . 
parotid gland involvement is usually presented as soft , painless , sometimes cystic , slowgrowing masses which ismostly accompanied by persistent cervical or generalized lymphadenopathy which may also be the initial manifestation of hiv infection [ 5 ]  . parotid gland ( pg ) imaging via either ultrasonography , computerized tomography ( ct ) or magnetic resonance imaging ( mri ) has long been used for the pg enlargement detection and follow - up [ 68 ]  . 
as far as we could research from english literature , no study has yet been performed regarding pg examination in hiv - infected children . in our study , we evaluated the pgs of hiv - infected children and compared the tissue stiffness values with the counterparts of healthy subjects . 
all cases in the study had sufficient image quality obtained and appropriate technique achieved , so no case was excluded from the study . grayscale ultrasound and swe measurements were completed by experienced pediatric radiologists with more than 10years of ultrasound and 5years of elastography experiences . 
the quality mode , which is identified as the propagation mode ( arrival time contour ) , is a mode in which reliable data are obtained when the lines are parallel and smooth , and the increase in distance between lines is parallel to the increase in stiffness . 
the speed of ultrasound waves was either measured in meters / second ( m / s ) or kilopascals ( kpa ) ; within seconds the result was displayed on the ultrasound screen . 
three valid measurements were recorded in kpa and m / s modes la radiologia medica ( 2019 ) 124 : 126131 values were automatically calculated by averaging 9 values for each pg . 
mannwhitney u test table 1 charactertistics of hiv - infected children parameter twenty - three children with the median age of 11 ( 117 ) years were included in the study . 
the median of cd4 counts and hiv viral load on the last patient were 267 ( 62820 ) cells / l and < 45 ( < 45896.398 ) copies / ml , respectively . 
others demonstrated lymphocytic aggregations , lymphoepithelial cysts , fatty infiltration and isolated lymphadenopathy . most of the reports point out the presence of cystic lesions in pgs of hiv - infected patients . 
increased tissue stiffness shown by swe even in the absence of those gross changes is particularly noteworthy . in our study , the patients with homogeneous pg appearance also had higher stiffness values than healthy controls . 
in the patients with heterogeneous pg appearance , swe can be used as an assistant for ultrasound . parotid gland enlargement in hiv can be due to inflammatory disorders , infections , neoplasms and benign lymphoepithelial cysts , so - called blecs . 
histologically , benign lymphoepithelial lesions with ductal metaplasia , reactive hyperplasia of an intraparotid lymph node and benign lymphoepithelial cysts are observed in pgs of patients with hiv infection [ 16 ]  . 
the second category named shear wave speed ( sws ) measurement includes transient elastography ( te ) and arfi quantification , as a point shear wave elastography ( p - swe ) , which can quantitatively calculate sws for assessing tissue stiffness . 
both p - swe and 2d - swe are based on capturing the propagation of sws induced by displacement of local tissues under the excitation of acoustic impulses from probes . 
 [ 14 ] mentioned that arfi provides a quick , easy and reliable diagnostic tool for the assessment of disease severity and progression in patients with chronic recurrent parotitis that can be seamlessly implemented into preexisting ultrasound protocols . our study is privileged since it is the first study evaluating pgs of hiv - infected children via swe . 
during routine cervical examination , pg evaluation via swe together with grayscale ultrasound can be very helpful . among the limitations of our study are the low numbers of patients , no deep lobe of pg measurements and lack of histological evaluation . 
another limitation is that elastography measurements were taken by single operator , and there was no comparison between users . conclusions pg examination of hiv - infected children via swe reveals increased tissue stiffness when compared with healthy subjects . 
swe can be used in the detection of early parenchymal 1 3 la radiologia medica ( 2019 ) 124 : 126131 changes even in the patients with homogeneous pg appearance . 
the diagnostic performance and agreement of us features between the cad system and the radiologist were compared . results sixty - two patients ( 50 f ; age 60 12years ) were enrolled : 77.4% ( 48 / 62 ) of thyroid nodules were benign , 22.6% ( 14 / 62 ) were undetermined to malignant and required follow - up or surgery . 
although it is an innovative tool with good potential , additional efforts are needed to improve its diagnostic performance . keywords computer - aided diagnosis nodule thyroid ultrasound * salvatore gitto sal.gitto@gmail.com 1 scuola di specializzazione inradiodiagnostica , universit degli studi di milano , via festa del perdono 7 , 20122milan , italy 2 scuola di specializzazione inendocrinologia e malattie del metabolismo , universit degli studi di milano , milan , italy 3 fondazione irccs istituto nazionale dei tumori , milan , italy 4 servizio di radiologia , irccs policlinico san donato , sandonatomilanese , italy 5 dipartimento di scienze biomediche perla salute , universit degli studi di milano , milan , italy 6 unit operativa di radiologia diagnostica ed interventistica , irccs istituto ortopedico galeazzi , milan , italy 7 divisione di radiologia interventistica , ieo , istituto europeo di oncologia irccs , milano , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 118125 introduction thyroid nodules are detected in up to 68% of general population and malignancies are observed in 310% of cases [ 1 , 2 ]  . 
 the critical role of the radiologist is to detect and characterize thyroid nodules with ultrasound ( us ) and us - guided fine - needle aspiration biopsy ( fnab ) serving as diagnostic cornerstones [ 3 ]  . 
us and fnab ensure the identification of thyroid nodules that need to be removed , such as malignancies and indeterminate follicular lesions , also reducing the number of unnecessary surgical procedures in favor of both conservative and minimally invasive treatment of benign thyroid nodules [ 48 ]  . computer - aided diagnosis ( cad ) systems have been developed to aid the radiologist in the image interpretation , speed up the diagnostic process and reduce interobserver variability . 
it aims to help users to increase diagnostic confidence with accurate and consistent recommendations , and improve patient throughput by adopting automatic report feature [ 9 ]  . the aim of our study is to compare the diagnostic performance of this new , commercially available cad system with that of a non - computer - aided radiologist in the characterization of low - to - high suspicion thyroid nodules . materials andmethods study design andpopulation the institutional review board of our hospital approved this retrospective study and waived the need for informed consent . 
thy 1 according to the bethesda system for reporting thyroid cytopathology [ 15 ] ; and ( 2 ) oblique rather than axial thyroid nodule us image available for post - processing . us examination andfnab all us examinations and procedures were performed with the patient lying supine on the examination table and the neck in hyperextension ; right or left - deviation were used according to the nodule location . 
the right and left lobes of the thyroid gland were evaluated in axial and longitudinal planes by a radiologist with 5years of experience in diagnostic and interventional thyroid imaging using a high - end us system ( rs80a with prestige us systemsamsung medical imaging , seoul , korea ) equipped with a broadband linear - array transducer ( l312a ) that worked at a fixed frequency of 10mhz . 
cytological analysis results were available in 47days after the procedure and classified according to the bethesda system for reporting thyroid cytopathology [ 15 ]  . postprocessing andimage analysis post - processing was performed in consensus by a radiology resident and an endocrinology resident with 18 and 6months of supervised experience in thyroid imaging , respectively , both blinded to cytological results . 
for each patient , an axial b - mode image of the thyroid nodule selected for fnab was combined with s - detect for thyroid ( samsung medical imaging , seoul , korea )  . 
based on this box , it performs thyroid nodule segmentation and then allows the user to select among a series of candidates or manually modify the contours of the lesion . 
 1 3 120 la radiologia medica ( 2019 ) 124 : 118125 information regarding the presence of calcifications is available only upon user selection , and thus the operators selected it after they retrieved this information from medical imaging reports that were provided by the experienced radiologist at the time of examination and were available for review . 
k - tirads [ 17 ] , russ [ 18 ] , and american thyroid association guidelines [ 11 ] , are embedded in the us systek - tirads was chosen for rating the nodule risk of malignancy in this study . the same radiologist performing the fnab with 5years of experience in diagnostic and interventional thyroid imaging , blinded to cytological results and post - processing analysis , randomly reviewed the thyroid nodule us images previously used for post - processing . 
a recommendation on the nodule risk of malignancy was formulated and based on k - tirads . statistical analysis for statistical analysis , anonymous data were entered into a database ( microsoft excel 2010 ) and then analyzed with spss 22.0 windows version ( spss inc . , armonk , ny , table 1 lexicons for thyroid nodule us assessment provided by the cad system [ 9 ] lexicon composition echogenicity orientation margins spongiform shape calcificationsa elasticitya vascularitya a only user selection is available indication solid partially cystic cystic hyper / isoechoic hypoechoic parallel non - parallel well - defined smooth microlobulate / spiculated ill - defined appearance non - appearance ovoid to round irregular micro / macrocalcifications no calcifications stiff soft appearance non - appearance usa )  . 
interobserver agreement between the cad system and the radiologist for assessment of thyroid nodule composition , echogenicity , orientation , margins , shape , and k - tirads was measured with the kappa statistic and interpreted using landis and kochs scale [ 19 ]  . 
for both the cad system and the radiologist , the sensitivity , specificity , positive predictive value , negative predictive value and accuracy in the identification of thyroid nodule requiring follow - up or surgery were calculated . 
categorical variables were reported as absolute value and percentage ; continuous variables were reported as mean value standard deviation , as detailed in the text . results a series of 79 patients ( 20 men , 59 women ; age 61 12years ) were referred for us - guided fnab of a thyroid nodule . 
among them , 17 patients were excluded due to non - diagnostic specimen after cytological analysis ( 8 cases ) or oblique rather than axial thyroid nodule us image available for post - processing ( 9 cases )  . 
 thyroid nodule maximum diameter measured 18 7m according to the bethesda system for reporting thyroid cytopathology [ 15 ] , 77.4% ( 48 out of 62 ) of thyroid nodules were cystic or benign , 22.6% ( 14 out of 68 ) were undetermined to malignant and required follow - up or surgery ( table2 )  . post - processing was performed in all included thyroid nodules and took 4 to 5min per nodule . 
thyroid nodules were classified into the k - tirads categories 3 , 4 and 5 in 50 , 8 and 4 cases by the cad system and 35 , 18 and 9 cases by the radiologist , respectively . 
 table4 details the sensitivity , specificity , positive predictive value , negative predictive value and accuracy for both the 1 3 la radiologia medica ( 2019 ) 124 : 118125 table 2 diagnostic categories of the thyroid nodules in our population according to the bethesda system for reporting thyroid cytopathology [ 15 ] diagnostic categories table 3 us features and k - tirads assigned to each thyroid nodule by the cad system and the experienced radiologist thy 1cconsistent with cyst thy 2benign thy 3aatypia of undetermined significance or follicular lesion of undetermined signifi4 ( 6.5% ) 44 ( 70.9% ) 8 ( 12.9% ) cance thy 3ffollicular neoplasm or suspicious for a follicular neoplasm thy 4suspicious for malignancy thy 5malignant lexicon indication cad system radiologist composition echogenicity orientation margins shape k - tirads solid partially cystic cystic hyper / isoechoic hypoechoic parallel non - parallel well - defined smooth microlobulate / spiculated ill - defined ovoid to round irregular category 3 ( low suspicion ) category 4 ( intermediate suspicion ) category 5 ( high suspicion ) no . 
this thyroid nodule was undetermined ( thy 3a ) according to the bethesda system for reporting thyroid cytopathology discussion thyroid nodules are a common clinical problem with a reported prevalence up to 68% of general population . 
the vast majority consists of benign lesions not requiring intervention or follow - up , as malignancies are observed only in 310% of cases [ 1 , 2 ]  . 
specifically , the radiologist classified the orientation and margin as non - parallel and well - defined , whereas the cad system classified them as parallel and ill - defined , respectively . 
such interobserver variability reflects that described between radiologists themselves , although higher concordance was found in margin evaluation [ 22 ]  . in the literature , there are a limited number of studies using cad systems and us to characterize thyroid nodules . 
some preliminary studies based on images obtained from ceus - 3d ( contrast - enhanced three - dimensional ultrasound ) , 2d - us ( two - dimensional ultrasound ) and hrus ( high - resolution ultrasound ) reported an excellent accuracy for thyroid malignancy detection [ 2326 ]  . 
however , such studies were conducted by independent research groups on a small number of patients not enrolled in a clinical setting , using non - commercial systems impractical for real time use because of complex and long - lasting post - processing analyses [ 2326 ]  . 
patients with a decisive diagnosis of either a benign or malignant thyroid lesion obtained by fnab , core - needle biopsy , surgical specimen histopathology or very low suspicion us finding of spongiform or cystic aspect were included . 
compared the diagnostic performance of an us image - based automatic thyroid recognition system built upon a multiple - scale convolution neural network model with that of an experienced 1 3 124 la radiologia medica ( 2019 ) 124 : 118125 radiologist using the current guidelines for thyroid nodule management [ 28 ]  . 
similarly , the cad system had comparable sensitivity but lower specificity than the experienced radiologist [ 28 ]  . the difference between our results and those obtained by the aforementioned studies may be due to several reasons , firstly including the use of different reference standards . 
indeed , according to the current international guidelines , fnab should guide thyroid nodule management along with clinical data and us evaluation , and it is regarded as the best triage test for preoperative assessment of thyroid nodules [ 10 ]  . 
further , the aforementioned studies hypothesized that the cad system may help to reduce unnecessary invasive procedures requested by inexperienced users although a radiologist performed post - processing in both cases [ 27 , 28 ]  . 
this was mainly related to the selection of the segmented nodule among a series of candidates provided by the cad system or , alternatively , to the need of manually modifying the contours of the lesion . 
indeed , we required that the segmented part and the thyroid nodule matched completely in order to increase the specificity of the cad systethis differs from the study by choi etal . 
where nodule segmentation was regarded as successful if , although not perfect , the segmented part was still representative of the nodule and the maximum contour mismatch did not exceed 30% [ 27 ]  . 
further , we did not assess thyroid nodules with spongiform or cystic appearance as our study population included patients referred for fnab and such us patterns require invasive procedures only if relevant in size or for therapeutic purposes [ 10 ]  . in conclusion , at present , the cad system is less sensitive than an experienced radiologist and showed slight - to - substantial agreement with the radiologist for the characterization of thyroid nodules . 
the classic presentation is abdominal pain , diarrhoea and / or rectal bleeding , but it is not specific and highly variable and so the diagnosis usually depends on clinical suspicion and is supported by serologic and colonoscopic findings . 
while plain radiography and ultrasound can orient the diagnosis , ct allows to define the morphofunctional alterations discriminating the non - occlusive forms from the occlusive forms and in most cases to estimate the timing of ischaemic damage . 
purpose of the review is to define the role of ct in the early identification of pathological findings and in the definition of evolution of colonic ischaemic lesions , in order to plan the correct therapeutic approach , suggesting the decision of medical or surgical treatment . keywords ischaemic colitis bowel infarction abdominal pain introduction ischaemic colitis ( ic ) is the most common manifestation of vascular disorder in the gastrointestinal tract . the pathogenesis of ic depends on two different forms of vascular colonic insult : non - occlusive injury and occlusive injury [ 1 ]  . the classic presentation of ic is abdominal pain , diarrhoea and / or rectal bleeding , but it is not specific and highly variable , so the diagnosis usually depends on clinical suspicion and has to be supported by serologic , radiological and colonoscopic findings . 
the anatomic damage results in ischaemic necrosis of variable severity : the ischaemic injury may involve only the colonic mucosal and submucosal layer or result in transmural ischaemic injury [ 2 , 3 ]  . 
even if colonoscopy within 48h represents the gold standard for final * graziella di grezia graziella.digrezia@gmail.com 1 radiology department , criscuoli hospital , santangelodeilombardi , avellino , italy 2 radiology department , university ofcampania luigi vanvitelli , naples , italy 3 radiology department , casa di cura villa dei fiori , acerra , napoli , italy diagnosis and different imaging methods have been used to diagnose ic , american college of gastroenterology clinical guideline considers computed tomography ( ct ) the main technique for the non - invasive diagnosis of ic . purpose of this report is to define the role of ct in the early identification of pathological findings and in the definition of ischaemic lesions evolution in order to plan the correct therapeutic approach , suggesting the decision of medical or surgical treatment [ 4 ]  . materials andmethods we retrospectively analyzed 95 cases of surgically confirmed ischaemic colitis in patients that underwent ct scan in radiology departments of our hospitals in the period between 1 january 2007 and 31 december 2016 . 
in case of occlusive cause , arterial from venous thrombosis has been diagnosed . the following findings were assessed : the location and length of the colonic segment involved ; the appearance and degree of wall thickening ; the presence of a double - halo or target configuration ( two or three concentric rings ) ; pericolic vol . : ( 0123456789 ) 1 3 104 la radiologia medica ( 2019 ) 124 : 103108 streakiness , peritoneal fluid or blood , the presence of intramural , mesenteric or portal venous gas , and free intraperitoneal air or other relevant abdominal findings were also recorded . 
the bowel wall was considered thickened if it measured more than 3mm in diameter . results all images have been analyzed and post - processed with multiplanar and three - dimensional reconstructions . of the 95 cases of ischaemic colitis , 72 were occlusive infarction , ( 35 cases of arterial thrombosis and 37 of venous thrombosis ) and 23 were non - occlusive cases . of the 58 cases of arterial thrombosis and non - occlusive ischaemia , reperfusion damage occurred in 13 . discussion the incidence of ic reported in the literature is of 6.144 cases / 100 , 000 person years with confirmatory histopathology , but it is a underestimated value because it could be a misdiagnosed cause of acute abdomen for its wide spectrum of clinical symptoms , the non - specificity of clinical and laboratory tests and the transient course of the disease . ic is caused by an acute interruption or chronic decrease in the colonic blood supply as in general hypotension , arterial stenosis and occlusion , bowel obstruction and venous outflow obstruction . 
although ic is usually observed in the elderly , the disease is now being increasingly diagnosed in persons younger than 50years of age , with definite predisposing causes , including vasculitis , medications , cocaine use , haemodialysis and long aeroplane flight [ 57 ]  . the superior mesenteric artery ( sma ) , which perfuses the ascending and transverse colon , and the inferior mesenteric artery ( ima ) , which distributes to the descending and sigmoid colon , are the two major arteries supplying most of the colon . 
the internal iliac arteries supply the rectu the splenic flexure ( griffiths point ) and sigmoid colon ( sudecks point ) are so - called watershed areas because these regions are located between two different vascular systems and so are particularly vulnerable to ischaemic insults . 
a third potential watershed area is the right colon , where the marginal vessel is poorly developed in up to 50% of people . the pathogenesis of acute ic depends on two different forms of vascular colonic insult : occlusive injury ( fig.1 ) and non - occlusive injury ( fig.2 ) [ 8 ]  . 
these remarks are useful in considering differential diagnosis with pathology having similar imaging features , but different distribution , as crohn . the classic presentation of acute ic is abdominal pain , diarrhoea and / or rectal bleeding , but it is not specific and highly variable and so the diagnosis usually depends on clinical suspicion and is supported with serologic and colonoscopic findings [ 9 , 10 ]  . the second one consists of non - occlusive ischaemia of the bowel caused by a sudden drop in blood flow in the small vessels of the colon , generally secondary to a lowflow state . 
 thinning of the bowel wall or paper - thin wall is caused by volume loss of tissue and vessels in the bowel wall and by loss of intestinal muscular tone due to the lack of blood flow . 
the latter could be misdiagnosed because of the similarity to the physiological colonic meteorism . the unthickened or paper - thin colonic wall is found in all conditions where ischaemia is not followed by effective reperfusion ; in acute phase , this condition could be observed in all cases of nomi until reperfusion occurs and in vasculopathic patients with ima occlusion in which the riolano arcade is unable to provide for an adequate blood supply . 
 a low - flow state causes a broad reduction in blood flow , simulating a simultaneous obstruction of sma and ima ; this explains the finding of wall thickness from normal to paper - thin wall in the acute phase of non - occlusive colitis with gaping lumen . the administration of iv contrast medium allows to evaluate the bowel wall enhancement as bowel wall hypodensity on enhanced ct in case of the absence of effective reperfusion due to the bowel wall ischaemic injury . 1 3 la radiologia medica ( 2019 ) 124 : 103108 fig . 
three kinds of infarction : abdominal ct showing an arterial occlusion ( a ) , a venous thrombosis ( b ) and narrowing of the sma with poor demonstration of the branches of the arteries in a non - occlusive mesenteric ischaemia ( c , d ) in case of nomi , beyond intestinal damage , there was also a parenchymal involvement ( liver , kidney , spleen ) in ischaemic injury . 
when reperfusion occurs , findings are not discernable from the first ones . clinically , ic may be classified as two major forms : non - gangrenous ( mild ) and gangrenous ( acute fulminant )  . 
the gangrenous form is associated with transmural necrosis and requires urgent surgery . colonoscopy within 48h represents until today the gold standard for final diagnosis , but it can be non - diagnostic in emergency setting without previous preparation and it should not underestimate the risk of perforation . imaging methods too have been used to diagnose ic . 
 plain radiography may show suggestive signs of chronic disease such as thumbprinting , which appears as rounded densities along the sides of a gas - filled distended colon , dilation of the colonic loops and loss of haustration . ultrasound is able to detect abnormalities in the bowel wall and identify segmental involvement of the colon . 
it allows to evaluate bowel wall thickening , colon wall stratification , pericolic fat , free fluid and pneumatosis . today , ct scan with iv contrast media allows defining the injured colonic segment and detecting the presence of complications.ct allows determining the morphofunctional alterations discriminating the non - occlusive forms from the occlusive forms , and it allows estimating the timing of ischaemic damage . the anatomic damage results in ischaemic necrosis of variable severity ; the ischaemic injury may involve only the colonic mucosal and submucosal layer or result in transmural ischaemic injury . 
also , imaging features can vary depending on the time course and aetiology , and the radiological findings can be summarized in four main categories ( table1 )  . the pericolic fluid is a crucial finding for ic diagnosis since its evidence suggests the presence of ongoing damage , thus focusing the attention on other pathological aspects which could be misdiagnosed : in fact , in case of acute ischaemic non - occlusive ic , the dilated thinned colonic wall could be misinterpreted as a physiological colonic distension caused by the presence of intestinal gas . 
in case of reperfusion , the amount of pericolic fluid may increase or decrease , depending on the evolution of 1 3 la radiologia medica ( 2019 ) 124 : 103108 106 fig . 
ct in axial plane ( a ) and coronal reconstruction ( b ) show a non - occlusive mesenteric ischaemia with mesenteric imbibition , wall , mesenteric vessels pneumatosis and portal pneumatosis . 
ct in axial plane ( c ) and coronal reconstruction ( d ) show a non - occlusive mesenteric ischaemia with wall thickening and stratification due to reperfusion damage fig . 
in addition , perivisceral imbibition has been reported , especially in subacute phase ( a , b ) , ( f , g ) left colonic features at doublecontrast barium x - ray 1 3 la radiologia medica ( 2019 ) 124 : 103108 fig . 
 b free fluid in peritoneal cavity ( white arrows ) table 1 radiological findings of ischaemic colitis vessel findings retroperitoneal cavity findings bowel wall findings parenchymal findings vascular occlusion or stenosisfindings of defects or occlusion of the sma e ima vascular pneumatosisthe presence of gas within the mesenteric venules and portal venous system free fluid pneumoretroperitoneum wall thickness ( normal thickness < 3 mm ) wall enhancement is considered pathological in the presence of a double - halo or target configuration ( two or three concentric rings ) or when absent wall pneumatosis signs of ischaemic damage involving the liver , kidneys , spleen and pancreas the ischaemic damage and thickened walls suggesting the decision of medical or surgical treatment ( table2 ) [ 11 ]  . pathological findings and in the definition of evolution of ischaemic lesions and [ 12 ]  . however , it requires the use of ionizing radiation and an iodinate contrast agent , limiting the possibility to use this technique in a short - term follow - up . acg clinical guideline ct considers ct the main technique for the non - invasive diagnosis of acute ic and recognizes the role in follow - up of mri in the identification of the treatment depends on the severity and cause of the ischaemia , and the detection of ic signs is crucial to plan the correct therapeutic approach and reduce the reported mortality rate ( 412% )  . 
multiple embolizing agents have been described , and among them , onyx seems to be promising ; this is a liquid embolic agent , originally applied in neurointerventional radiology and recently adopted also in peripheral embolizations . 
the aim of this study is to report on a 10 - year experience of transarterial embolization of peripheral high - flow avm with onyx in terms of technical and clinical outcomes . materials and methods retrospective analysis was conducted on patients affected by high - flow avm and treated electively by transarterial embolization with onyx . 
technical and clinical success was evaluated ; follow - up was conducted 30days after the last treatment session and yearly in case of success . results sixteen patients have been included , totally 38 embolizing procedures . 
technical success was obtained in 11 patients ; at 30 - day follow - up , 15 patients showed improvements in symptoms , even those with incomplete embolization ; however , after almost 1year from treatment accomplishment , 7 patients showed relapse of symptoms and presented radiological signs of avm recurrence . 
no clinically relevant complications occurred . conclusions in this series , in accordance with previous but limited published data , onyx appeared safe and technically effective to embolize high - flow peripheral avm with transarterial approach . 
cardarelli 9 , 80131naples , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 154162 introduction vascular malformations presenting with an arterial component are defined as high - flow arteriovenous malformations ( avms ) ; these vascular lesions are constituted by arteriovenous microfistulae through a vascular nidus [ 1 ]  . 
 according to the localization into or outside the central nervous system , they are divided into central and peripheral , respectively [ 2 ]  . different classification systems [ 35 ] have been proposed in the literature focusing on morphology [ 3 , 6 ] and clinical impact [ 4 ] ; however , confidence of operators in each unique angiographic avm architecture is essential in planning the proper endovascular strategy , considering also that the angioarchitecture can evolve while staging sessions of embolization . clinical presentation of high - flow avms ranges from asymptomatic to intermittent pain , tissue swelling , bleeding and even right heart failure [ 7 , 8 ]  . the surgical resection is avoided because historically it carried high rate of recurrence due to incomplete vascular eradication , so the first - choice treatment is the catheterdirected embolization [ 1 , 9 ] ; these are technically challenging procedures because of the risk of nontarget embolization and / or incomplete treatment . multiple embolizing agents can be adopted ; thanks to the technological developments promoted by industries , today interventional radiologists handle several agents , allowing a customized embolization procedure based on the vascular pattern they are facing with . 
onyx ( ev3 , irvine , california , usa ) is a nonadhesive liquid embolizing agent ; originally adopted in interventional neuroradiology , its use has been reported also in peripheral embolization for the treatment of avm , type ii aortic endoleak , portal vein embolization , aneurysms and bleedings [ 1013 ] ; it consists of a plastic polymer ( ethylene vinyl alcohol , evoh ) dissolved in a organic solvent agent ( dimethyl sulfoxide , dmso ) ; fluoroscopic visibility is obtained thanks to the tantalum powder component suspension after shaking of the evoh vial for almost 20min before usage . the aim of this study is to report on a single - center 10 - year experience transarterial high - flow avm embolization with onyx in terms of technical and clinical outcomes . materials andmethods sample this is a tertiary care - level single - center , retrospective analysis of the last 10years , from january 2007 to april 2018 , focusing on patients affected by high - flow avm and managed by transarterial embolization . 
 written informed consent was obtained the day before the procedure . based on the local picture archive and communication system ( pacs ) and electronic records , retrospective data collection included : preinterventional clinical radiological evaluations , procedural data and post - procedural clinical radiological assessment . 
in case of unavailable data on the electronic records , patients were interviewed by phone calls . preprocedural radiological evaluation included always first - level examinations ( echo color doppler ultrasound , ecd - us ) and a consequent second - level imaging ( contrastenhanced computed tomography , ct and / or magnetic resonance , mr )  . 
in all cases , diagnosis of avm was acquired before angiography . embolization technique for a comfortable intervention , procedures were conducted under local anesthesia in correspondence with the vascular access and sedatives for pain reduction ; no general anesthesia was given . standard vascular access consisted of us - guided or fluoroscopy - guided retrograde femoral puncture with 5 french sheath ( radifocus introducer ii , terumo , japan ) positioning . with a diagnostic 5 french catheter , different tip curves related to the lesion anatomy , preprocedural angiography was performed with different obliquities projections . 
 according to the best projection to visualize the avm feeder ( s ) and nidus , the 5 french catheter was then positioned as distal as possible , and then , a microcatheter was navigated into each feeding artery as close as possible to the nidus . 
to completely suck the liquids , 14 - gauge and 16 - gauge cannulas were , respectively , inserted into evoh and dmso vials ; then , the syringes were filled with air and injected into the vials to increase the pressure on the liquid content ; finally , 1 3 156 la radiologia medica ( 2019 ) 124 : 154162 fig . 
1 patient 4 , procedural angiography of a 24 - year - old woman affected by a high - flow avm of the right leg presenting with swelling and padiagnostic angiography demonstrated two arterial feeders originating from the posterior tibial artery . 
f angiographic control after onyx 34 injection showing onyx cast in the posterior portion of the avm ( white arrow , same in figure g ) and a small amount of accidental onyx reflux into the posterior tibial artery ( black arrow , same in figure g )  . 
h final angiographic control after embolization completion with onyx 34 demonstrating complete technical success with a small amount of onyx occluding the posterior tibial artery in correspondence with the middle tract ( black arrow )  . 
when evoh starts outflowing from the microcatheter , the first injection has to voluntary reflux around the microcatheter tip and should be waited for 23min ; this is intended to create a cast that avoids further evoh reflux and possible nontarget embolization . 
then , evoh injection is continued until the desired embolization is obtained ; at the end of the procedure , the dead space of 1 3 la radiologia medica ( 2019 ) 124 : 154162 fig . 
2 patient 13 , procedural angiography of a 29 - year - old woman affected by a high - flow avm of the uterus presenting with pain , bleeding and dysmenorrhea . 
ab contrast - enhanced ct ( a ) and mr ( b ) in arterial phase in axial planes showing highflow avm of the uterus fed by both uterine arteries appearing ectasic and tortuosous ( white arrows )  . 
c angiography acquired after contrast injection from pigtail catheter positioned in aorta ; uterine avm was confirmed with dominant venous drainage in the left common iliac vein ( white asterisk )  . 
at 30 - day clinical follow - up , patient showed partial improvement in symptoms ; therefore , another treatment session was planned with additional embolizing agents from both arterial ( coils and particles ) and venous districts ( sodium tetradecyl sulfate )  . 
at 1 - year clinical follow - up , the patient was clinically asymptomatic with regular period the microcatheter is cleaned with dmso , and finally , the microcatheter is retrieved in aspiration . final angiograms are acquired from the 5 french catheter . eventually , additional embolizing agents ( coils , particles , glue , sodium tetradecyl sulfate ) were needed to seal the vessels lumen or to occlude small collaterals unsuitable for onyx embolization . the arterial puncture site was closed by manual compression or mechanical hemostasis ( femoseal , terumo , japan )  . no anticoagulants were used during any of the procedures . antiinflammatories and antibiotics were prescribed for 5days after the intervention to prevent / reduce the occurence of the post - embolization syndrome . procedural outcome evaluation technical success was defined as disappearance of nidus and drainage vein ( s ) opacification at final angiograms ; in some cases , multiple treatment sessions would be performed to obtain the devascularization . clinical success was intended as improvement in symptoms without the need for additional therapies . intraand post - procedural complications were registered and evaluated according to the cirse classification system for complication [ 14 ]  . 1 3 158 la radiologia medica ( 2019 ) 124 : 154162 fig . 
3 patient 14 , procedural angiography of a 39 - year - old man affected by a wide high - flow avm of the right emi - thorax presenting with hemoptysis . 
ad diagnostic angiography showing avm refurnishment from intercostal ( a ) , bronchial ( bc ) and mammary ( d ) arteries , with multiple anastomosis ; other right thoracic intercostal arteries were involved ( not shown )  . 
 at 30 - day clinical follow - up , patient showed improvement in symptoms ; however , after two months he suffered from new hemoptysis episodes ; therefore , another two treatment sessions were performed . 
in two patients ( patients 10 and 13 ) , an additional transvenous approach was required for retrograde embolization session ; both were complex pelvic avms . microcatheters used were dmso compatible ( rebar 18 and rebar 27 , medtronic , usa ) ; however , in accordance with empirical experience as well as previous published papers [ 1517 ] , also not technically dmso - compatible microcatheters ( progreat 2.7 , terumo , japan ) were employed without problems . additional embolizing agents were required in five patients ( patients 10 , 11 , 13 , 14 and 16 )  . technical success was obtained in 68.7% ( 11 out of 16 patients ) ; in five patients ( patients 10 , 11 , 12 , 14 and 16 ) , cirse classification system for complications [ 14 ] was adopted : one episode of nontarget embolization due to evoh reflux occurred ( patient 4 ) , with consequent peroneal artery definitive embolization ; however , no long - term ischemic clinical sequelae were seen ( grade 3 )  . 
in three patients , groin swelling and hematoma , self - limiting without additional therapies , were registered ( grade 1 ) ; 4 patients who showed post - embolization syndrome up to 5days after the procedure were managed with antiinflammatory and antibiotics ( grade 1 )  . after all the procedures , a normal finding was garlic smelling present for 4872h because of dmso elimination via respiration and sweat . all patients were symptomatic before treatment ; at the follow - up visit 30days after the last embolization session , all but one patient ( patient 16 ) showed improvements in symptoms , even those with incomplete embolization ( 30day clinical success 93.7% ) ; however , after almost 1year from treatment accomplishment , 43.7% of the patients 1 3 table 1 patient data in terms of sex , age , body district involved and clinical findings patient sex age district clinics 1st and 2nd hand fingers swelling 160 m 23 tongue m 73 thigh m 68 bronchus 46 humerus m 23 humerus m 28 buttock 38 uterus pelvis eyelid pelvis 29 uterus m 39 bronchus / ribs pelvis m 29 functional impairment swelling pain bleeding functional impairment swelling swelling pain hemoptysis swelling pain swelling pain swelling pain pain bleeding functional impairment pain bleeding pain bleeding functional impairment pain bleeding functional impairment pain bleeding functional impairment hemoptysis pain bleeding functional impairment swelling pain bleeding showed relapse of symptoms and presented signs of avm recurrence at contrast - enhanced ct and / or mr . discussion onyx is a liquid embolizing agent introduced in the routine clinical practice at the beginning of 2000s by neurointerventionalists for the treatment of central avm . 
its successful usage for the treatment of peripheral avms has also been reported , by both transvascular and direct puncture techniques , in adults and children [ 1 , 5 , 9 , 10 , 1620 ] ; however , literature data about peripheral applications are still scarce and studies have been conducted in small samples . la radiologia medica ( 2019 ) 124 : 154162 it is considered mainly as an alternative to cyanoacrylate . 
 compared to glue , it presents the advantage of nonadhesive property ; its injection is therefore voluntary slow , permitting to visualize the fulfilling of the lesion without the risk of microcatheter glueing . 
recently , industry competitors have developed other new liquid nonadhesive embolizing agents in ready - to - use format and those agents have already been adopted in neurointervention [ 21 ] ; however , because of the very last development , clinical efficacy has to be still evaluated in the literature in peripheral avm treatment . specifical evoh - related complications are rare : microcatheter entrapments have been reported [ 2224 ] and these are consequences of ab estrinseco compression of onyx cast on the microcatheter in narrow and tortuous vessels after long - lasting procedures with extended segments entrapped . 
another risk to consider is skin darkening in case of subcutaneous lesions , due to tantalum deposition ; this is mainly related to direct injection technique [ 1 , 25 ]  . 
on the other hand , dmso should be handled with special care because compared to evoh it induces pain and vasospasms if injected fast , reducing evoh distalization ; patients should always be informed of the postprocedural 4872 - h garlic smelling occurring because of dmso elimination . overall , in this sample complications were scarce and of low grade according to cirse classification system , all without clinical sequelae . dmso - compatible microcatheters should be preferably adopted ; however , off - label usage of not technically compatible microcatheters has been reported without problems [ 1517 ] , as in this series . 
in some particularly challenging cases , tip - detachable microcatheters have been successfully employed , also from a transvenous approach [ 19 , 26 , 27 ]  . high - flow avm is extremely complex vascular lesions which should be treated with a customized approach based on the diagnostic angiographic findings . 
multiple embolizing agents have been adopted , and onyx is one of the most successful in the literature [ 1 , 9 , 18 , 19 ] because of its ability to form a cast penetrating the nidus , even if this is not directly reachable with microcatheter . in the peripheral body , the most frequently reported use of onyx is represented by the treatment of the type ii endoleaks of abdominal aortic aneurysms [ 11 , 12 ] ; literature data concerning peripheral avm embolization with onyx are still scarce . 1 3 la radiologia medica ( 2019 ) 124 : 154162 table 2 embolization data , technical and clinical success , follow - up patient treatment sessions additional transvenous access procedural technical success 30 - day clinical success 1 - year follow - up additional embolizing agents sts sodium tetradecyl sulfate glue coils glue coils coils particles coils particles glue coils in an initial case series published in 2004 , numan etal . 
the reason of this low success rate may be explained by the uncomplete knowledge of onyx properties at that time and since handling of this material has improved thanks to the experience acquired in neurovascular interventions . more recently in 2016 , de beule etal . 
 [ 1 ] reported their experience on peripheral avm embolizations with onyx on 28 sessions of 19 patients : compared to the data reported in this sample , they described similar post - embolization avm total occlusion rate ( 63% )  . additional agents should be considered to occlude vessels not suitable for onyx , as occurred in 31.2% of cases in this series ; comparable additional agents usage rates were reported by both de beule etal . 
 [ 19 ] reported a novel technique of retrograde transvenous onyx embolization of peripheral avm , after preliminary transarterial and transvenous flow reduction , with encouraging results . even if complete technical success is obtained , at follow - up recurrences have to be expected because of frequent recruitment of new arterial feeders . 
on the other hand , it should be underlined that even if technical success is not completely obtained at first attempt , temporary symptom relief may occur because of reduced blood flow to the nidus , as reported also by numan etal . 
 [ 18 ] ; therefore , multiple treatment sessions are usually required , and in this sample , only eight of sixteen patients have been treated once . main limitation of this study is the small number of patients although this is the reported sample with the highest number of procedures concerning peripheral avm onyx embolization ; however , it should be considered that the global incidence of the pathology is low . 
another issue is that only trained operators performed the embolizations ; indeed , considering the specific injection technique and the material cost , onyx should not be handled by short - experienced interventionalists . 1 3 162 la radiologia medica ( 2019 ) 124 : 154162 in conclusion , in this series , in accordance with previous but limited published data , onyx appeared as a safe and technically effective agent to embolize high - flow avm with transarterial approach . 
however , clinical imaging follow - up is mandatory in these patients because new feeder recruitment has to be expected ; patients should be informed of the concrete possibility of multiple treatment sessions . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . research involving human participants all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual patients included in the study . la radiologia medica ( 2019 ) 124 : 136144 radiotherapy hypofractionated radiation therapy inthemanagement oflocally advanced nsclc : anarrative review oftheliterature onbehalf oftheitalian association ofradiation oncology ( airo ) lung working group giuseppeparisi1 rosariomazzola2 patriziaciammella3 giorgiatimon3 alessandrafozza4 davidefranceschini5 federiconavarria6 alessiobruni7 marcoperna8 niccolgiajlevra2 filippoalongi2 vieriscotti8 marcotrovo1 received : 28 may 2018 / accepted : 15 october 2018 / published online : 27 october 2018 italian society of medical radiology 2018 abstract a systematic literature was performed to assess the benefit in terms of effectiveness and feasibility of hypofractionated radiotherapy ( hyport ) , with or without chemotherapy ( ct ) , in the treatment of locally advanced non - small cell lung cancer ( nsclc )  . 
we have identified all studies , published from 2007 onwards , on patients with locally advanced nsclc treated with hyport with radical intent , with a minimal dose per fraction of 2.4gy , with or without concurrent chemotherapy . 
actuarial 2 - year pfs ranged from 13 to 57.8% , and 1 , 2and 3 - year overall survival ( os ) ranged from 51.3 to 95% , from 22 to 68.7% , and from 7 to 32% , respectively . 
non - small cell lung cancer ( nsclc ) represents the majority of lung cancer diagnosis , and most of these are in locally advanced stage , half of which unresectable [ 2 , 3 ]  . 
the standard radiation scheme is 6066gy delivered in 3033 fractions [ 5 ]  . nevertheless , after standard radiation doses of crt , the risk of local recurrence remains high and 5 - year survival is poor . 
radiation therapy oncology group ( rtog ) 0617 randomized phase 3 study failed to show a beneficial effect in survival when delivering higher dose of rt at 2gy per fraction [ 8 ]  . 
a strategy to increase the biological effective dose ( bed ) of rt could be obtained using hypofractionated regimens characterized by a reduction in the overall treatment time with dose per fraction higher than 2gy [ 1113 ]  . considering the technological worldwide implementation in rt facilities and the issue of maintaining limited waiting list for the patients , hypofractionated was adopted in many centers and in several clinical settings , including lung cancer [ 14 ]  . aim of the current narrative review is to assess the benefit of hypofractionated rt , with or without concurrent chemotherapy ( ct ) , in terms of effectiveness and feasibility in the treatment of locally advanced nsclc . materials andmethods all studies included in the present review satisfied the following criteria : ( 1 ) patients with locally advanced nsclc , ( 2 ) patients treated with hypofractionated rt with radical intent , ( 3 ) with a minimal dose per fraction of 2.4gy , ( 4 ) patients treated with hypofractionated rt with or without concomitant ct , ( 5 ) studies published from 2007 onwards , ( 6 ) english manuscripts . 
disagreement was resolved by consensus ; if consensus could not be achieved , the study coordinator provided an assessment of eligibility . for data extraction , all the papers were scrutinized for the following information : study design ( retrospective , prospective ) ; number of patients ; number of patients comprise in study with concomitant ct ; oncological treatment strategy ( rt alone and / or sequential crt , versus concurrent crt ) ; total dose ; dose per fraction ; definition of acute and late toxicity profile clinical outcomes . results twenty - nine studies [ 1543 ] of hypofractionated rt in locally advanced nsclc with or without concurrent ct that met the inclusion criteria were identified , for a total of 2614 patients . 
of these , eight were phase i trials , and ten were phase ii trials . clinical outcomes innonconcurrent chemotherapy group seventeen studies [ 1531 ] , for a total of 1730 patients , without concurrent ct that met the inclusion criteria were identified . 
the most common ct agents employed were cisplatin ( 70.5% ) , predominantly in doublet with , gemcitabine or vinorelbine . 1 3 138 la radiologia medica ( 2019 ) 124 : 136144 1 3 la radiologia medica ( 2019 ) 124 : 136144 the most common rt technique was 3d - conformal radiation therapy ( 3d - crt ) ( 64.7% ) , whereas intensity - modulated rt ( imrt ) was employed in only three studies ( 23.5% ) ; in one study patients were treated with protons . 
actuarial 2 - year progression free survival ( pfs ) , which was reported in 12 studies , ranged from 13 to 57.8% , and 1 - , 2and 3 - year overall survival ( os ) ranged from 51.3 to 95% , from 22 to 68.7% , and from 7 to 32% , respectively . in only three studies ( 17.6% ) , elective lymph nodes were irradiated . 
regarding pulmonary toxicity , acute pneumonitis occured in 044% , whereas late pneumonitis occured in 047% , most commonly grade 3 . clinical outcomes inconcurrent chemotherapy group sixteen studies of hypofractionated rt [ 15 , 16 , 26 , 30 , 31 ] delivered concomitantly with ct were identified , for a total of 884 treated patients ( table2 )  . 
the most common ct agents employed were cisplatin 50% , carboplatin 25% and vinorelbine 37.5% ; other agents employed less frequently were , liposomal doxorubicin , docetaxel , gemcitabine , cetuximab and alk - inhibitors . 
acute esophagitis occurred in 041.7% , while late esophageal toxicity occurred in 08.3%. the overall incidence of acute pneumonitis ranged from 0 to 23% , whereas late pneumonitis occured in 047% , similarly to the non - concomitant ct group . discussion most of nsclc patients with locally advanced disease have poor prognosis [ 45 ]  . 
in fact , the treatment 1 3 140 la radiologia medica ( 2019 ) 124 : 136144 failure of the primary nsclc has a detrimental impact in terms of pfs , metastasis - free survival and os [ 46 ]  . to date , the standard of care is represented by rt using conventional fractionation , with concurrent or sequential platinum - based ct [ 47 ]  . 
at a median follow - up of 22.9months , 74gy given in 2gy per fractions with concurrent ct showed to be not better than 60gy for patients affected by stage iii nsclc . 
the authors concluded that high - dose conformal rt might be potentially harmful [ 8 ]  . on the other hand , it has been demonstrated that a long duration of rt in nsclc seems to be detrimental in terms of tumor control and survival , due to accelerated repopulation of tumor cells , with a loss of local control of 1.66% per day of lengthening over 6weeks [ 9 , 10 ]  . 
in the present review , we analyzed the available literature data concerning the role of hypofractionated rt in the management of locally advanced nsclc distinguishing two main groups : ( 1 ) non - concurrent ct patients and ( 2 ) concomitant ct patients . looking at the first patients category , 1 - , 2and 3 - year os ranged between 51 and 95% , 22 and 68% , and 7 and 32% , respectively ; 2 - year pfs varied from 13 to 58% . 
there was no significant difference regarding pulmonary toxicity . analyzing the clinical outcomes of hypofractionated rt administered concomitantly with ct , 3 - year os ranged from 31 to 44% , whereas 2 - year pfs varied between 19 and 58% . 
 speculatively , potential higher rates of oncological outcomes compared to conventional crt could be expected using a hypofractionation regimen in non - concurrent than in concomitant hypofractionated rt for nsclc . 
 obviously , these last assumptions need to be confirmed and a direct comparison between different fractionation schedules requires well - designed randomized studies before to draw any kind of definitive conclusion . radiobiological modelings suggest that shortened treatment schedules might increase the risk of late toxicity . 
in the available data here reported , acute esophagitis occurred in 015% in the nonconcurrent group comparing to 041.7% in the concomitant arregarding pulmonary toxicity , acute pneumonitis occurred in 044% , whereas late pneumonitis was recorded until to 47% of cases , most commonly grade 3 . 
a similar pulmonary toxicity profile was noted in the non - concomitant hypofractionated group . conclusions in summary , in the current review of the literature an extreme heterogeneity was noted in terms of the rt - treatment schedules , in terms of the adopted techniques as well as the administered drugs in combination with irradiation . 
these conditions associated with the rapid evolution of technologies and the hypothesis of association with new target agents and immunotherapy could constitute , in the future , a potential new frontier in the treatment of locally advanced nsclc . author contribution statements in our review are listed 13 authors . 
all authors approved the final manuscript . compliance with ethical standards conflict of interest all authors declare no conflict of interest . research involving human participants and / or animals this article does not contain any studies with human participants or animals performed by any of the authors . 1 3 la radiologia medica ( 2019 ) 124 : 136144 1 3 142 la radiologia medica ( 2019 ) 124 : 136144 la radiologia medica ( 2019 ) 124 : 145153 radiotherapy delta radiomics forrectal cancer response prediction withhybrid 0.35t magnetic resonanceguided radiotherapy ( mrgrt ) : ahypothesisgenerating study foraninnovative personalized medicine approach lucaboldrini1 davidecusumano1 giudittachiloiro1 calogerocas1 carlottamasciocchi1 jacopolenkowicz1 francescocellini2 nicoladinapoli2 luigiazario3 stefaniateodoli2 mariaantoniettagambacorta1 marcodespirito3 vincenzovalentini1 received : 7 june 2018 / accepted : 15 october 2018 / published online : 29 october 2018 the author ( s ) 2018 abstract the aim of this study was to evaluate the variation of radiomics features , defined as delta radiomics , in patients undergoing neoadjuvant radiochemotherapy ( rct ) for rectal cancer treated with hybrid magnetic resonance ( mr ) - guided radiotherapy ( mrgrt )  . 
an imaging acquisition protocol of 6 mr scans per patient was performed : the first mr was acquired at first simulation ( t0 ) and the remaining ones at fractions 5 , 10 , 15 , 20 and 25 . 
the variations of each feature during treatment were quantified , and the ratio between the values calculated at different dose levels and the one extracted at t0 was calculated too . 
the most predictive feature ratios in ccr prediction were the l_least and glnu ones , calculated at the second week of treatment ( 22gy ) with a p value = 0.001. 
delta radiomics approach showed promising results and the quantitative analysis of images throughout mrgrt treatment can successfully predict ccr offering an innovative personalized medicine approach to rectal cancer treatment . keywords rectal cancer radiomics delta radiomics personalized medicine innovative biotechnology mridian viewray * davide cusumano davide.cusumano@policlinicogemelli.it 1 dipartimento di diagnostica perimmagini , radioterapia oncologica ed ematologia , istituto di radiologia , fondazione policlinico a . 
gemelli irccs universit cattolica sacro cuore , rome , italy introduction significant improvements in locally advanced rectal cancer ( larc ) treatment have been met in the past two decades , and to date the typical therapeutic workflow is represented by neoadjuvant long - course radiochemotherapy ( rct ) , followed by total mesorectal excision ( tme ) [ 14 ]  . regardless of the initial disease stage , approximately 1142% of these patients achieve a pathological complete response ( pcr ) after long - course rct . 
in a very recent systematic review and pooled analysis , however , patients undergoing w&w approach showed a 3 - year overall survival of 93.5% ( against a 90.1% rate for patients with pcr ) and a non - regrowth free survival rate was of 89.2% at 3years , supporting the favourable prognostic value of ccr already supposed by the first conservative experiences of habrgama etal . 
no detection of residual lesions or the presence of a flat scar at endoscopic examination . image analysis an imaging protocol consisting in 6 mr acquisitions was applied to all patients . the first mr scan was acquired during the treatment simulation procedures ( t0gy ) , and the others were performed one every five fractions ( t11gy , t22gy , t33gy , t44gy and t55gy )  . figure1 shows the imaging protocol applied in a case where a clinical complete response was achieved . 
the red contour indicates the gtv delineation . all images were acquired on mridian using a true fast imaging ( trufi ) with steady - state precession sequence , sixteen consecutive patients ( 13 males and 3 females ) affected by larc ( stages iiaiiic ) , with a median age of 64years ( range 4986 ) were retrospectively enrolled for this study . five patients ( 31% ) showed ccr at restaging examinations ( dre and mri )  . patients characteristics are described in table1 . median time interval between end of neoadjuvant rct and restaging examinations was 62days . a total of 53 radiomics features belonging to four families ( morphological , statistical , fractal and textural based on runlength matrix ) were extracted from each raw image , without applying any image filter . a total of 318 radiomics features were therefore obtained ( 53 features extracted from the simulation image and 265 calculated as delta features )  . of these , a total of 6 simulation features and 57 delta radiomics features showed a p value < 0.05 ( wmw test ) in discriminating ccr patients from the non - responding ones . 
 table2 reports the features that are significant with the corresponding time of acquisition and p values . as reported in the tables , most of the delta radiomics features show a higher statistical significance in discriminating between ccr and not - ccr patients when compared to those extracted from the analysis of the simulation images . more specifically , three delta features ( energy , grey level non - uniformity and least axis length ) showed a statistically 1 3 148 la radiologia medica ( 2019 ) 124 : 145153 fig . 
the introduction of the described radiomics workflow can enrich the observations already available in the literature that took into account the predictive power of different tumour - related parameters during treatment : as an example , palmisano etal . 
patients undergoing ccr are indicated in light grey this significant limit has been recently overcome by the availability of mrgrt daily setup images that allow the development of imaging - based response predictors during rct treatments course with no additional burden in terms of dose to the patient , costs and procedures . indeed , the aim of this hypothesis - generating study was to explore the potentialities of the delta radiomics approach , more than to train a multiparametric prediction model , as the limited number of patients could not gather reliable conclusions . the choice of using the wilcoxonmannwhitney test to investigate the predictive value of the delta radiomics parameters was adopted considering a recent study carried out by parmar etal . , who compared 14 different feature selection methods . 
the other authors do not have conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . all the definitions refer to the image biomarker standardisation initiative by zwanenburg etal . 
all patients underwent mr imaging with a 1.5 t scanner system , including diffusionweighted imaging ( dwi ) with three different b values ( b = 0 , 500 and 800s / mm2 )  . 
the entire tumor volume was manually delineated on the adc maps , using the t2 - weighted images and dwis with b = 800s / mm2 as a guide to the lesion location . 
the optimal cutoff values for adcmean and adcmedian as predictors for lymphoma were 0.83 103 mm2 / s and 0.73 103 mm2 / s , respectively . conclusions the whole - lesion adc histogram analysis of cervical lymphadenopathy may help to discriminate lymphomas from non - nasopharyngeal scc in patients with unknown clinical primary tumor . keywords diffusion - weighted imaging head and neck cancer neck nodes quantitative imaging * antonello vidiri antonello.vidiri@ifo.gov.it 1 radiology anddiagnostic imaging department , irccs regina elena national cancer institute , via elio chianesi 53 , 00144rome , italy 2 medical physics laboratory , irccs regina elena national cancer institute , via elio chianesi 53 , 00144rome , italy 3 department ofradiology , f . 
policlinico gemelli irccs , largo agostino gemelli 8 , 00168rome , italy 4 department ofotolaryngology andhead andneck surgery , irccs regina elena national cancer institute , via elio chianesi 53 , 00144rome , italy 5 department ofhematology , irccs regina elena national cancer institute , via elio chianesi 53 , 00144rome , italy 6 department ofpathology , irccs regina elena national cancer institute , via elio chianesi 53 , 00144rome , italy 7 via pieve di cadore 30 , 00135rome , italy vol . : ( 0123456789 ) 1 3 20 introduction in an era of advanced diagnostics , metastasis to cervical lymph nodes from an occult primary tumor is a rare clinical entity and ranges approximately from 1.5% to 9% of all head and neck malignancies [ 14 ]  . 
in the neck , two - thirds of cervical lymph nodes are histologically confirmed as squamous cell carcinomas ( sccs ) , followed by undifferentiated carcinoma and adenocarcinoma [ 5 ]  . 
a formal fine needle aspiration ( fnac ) is the preferred method of biopsy in a patient affected by a scc lymphadenopathy , who presents to a physician for diagnostic examination . 
in fact fnac does not allow to differentiate histological subtypes and to perform the differential diagnosis between hyperplasia and low - grade non - hodgkin lymphoma [ 7 ]  . on the basis of conventional mri alone , it is very difficult to differentiate scc from lymphoma but advances in mri acquisition techniques , as diffusion and perfusion mri , demonstrated to be useful noninvasive imaging tools for a better tumor characterization [ 8 , 9 ]  . 
several dwi studies reported that the apparent diffusion coefficient ( adc ) is helpful in the differential diagnosis of these two head and neck malignancies , because dwi typically shows different rates of microscopic water diffusion in tissues , according to different features of tumor cellularity [ 1014 ]  . 
most of these studies documented an overlap of adc values between scc and lymphoma in head and neck lesions , based on a simplistic adc analysis of mean values within manually selected regions of interest ( rois ) inside the lesion . 
however , this approach to the image analysis is not recommended by the international consensus [ 15 ] , as the roi placement is subjective , does not allow a straightforward comparison between results from different centers , besides the fact that it does not enable to address the tumor heterogeneity [ 16 , 17 ]  . the calculation of the whole - volume adc histogram , based on the distribution of the voxel - level values within the entire lesion , can improve the reproducibility of quantitative dwi , promoting a standardization of adc [ 15 , 18 ]  . 
a few studies , based on the adc histogram analysis , documented a better differentiation of head and neck lesions , as well as an improvement in grading tumors and in predicting the outcome of chemo - radiotherapy [ 8 , 1922 ]  . la radiologia medica ( 2019 ) 124 : 1926 the aim of this study was to retrospectively evaluate the potential of whole - volume adc histogram of cervical lymph node to discriminate between lymphomas and metastatic non - nasopharyngeal sccs , in patients without any evidence of a primary tumor on clinical examination . materials andmethods patient population the present retrospective study was authorized by the hospital ethics committee . 
the patients were eligible for the study if they had : ( 1 ) solitary or multiple cervical lymph node metastases , without evidence of primary tumor after initial clinical examination ; ( 2 ) a histological confirmation with fnac or biopsy ; ( 3 ) pre - treatment mri studies according to the imaging protocol described in the following section . 
 the exclusion criteria for the patients were : ( 1 ) histological confirmation of nasopharyngeal carcinoma ( npc ) or nasopharyngeal lymphoma , ( 2 ) image distortion because of strong susceptibility and / or motion artifacts on dwi , and ( 3 ) largely necrotic node . mr imaging protocol mr imaging was performed with a 1.5 t scanner system ( optima mr 450w , ge healthcare , milwaukee , wi , usa ) , using a 16 - channel receive - only rf coils : a head coil , a surface neck , and a spine coil . 
fast spin - echo t2 - weighted imaging ( fse t2wi ) on the coronal plane ( acquisition matrix 288 256 , field of view 27cm , repetition time / echo time ( tr / te ) 5901ms / 102ms , slice thickness 4mm ) was first obtained , followed by axial spin - echo t1 - weighted imaging ( se t1wi ) ( acquisition matrix 288 256 , field of view 20cm , tr / te 617ms / 8.1ms , slice thickness 3mm ) and axial fse t2wi ( acquisition matrix 288 256 , field of view 20cm , tr / te 6844ms / 105ms , slice thickness 3mm )  . 
dwis were obtained by single - shot spin - echo echo planar imaging with the following parameters : acquisition matrix , 128 128 ; field of view , 2628cm ; tr / te , 2393ms / 66.4ms ; slice thickness , 4 . 
three different b values ( b = 0 , 500 and 800s / mm2 ) were used , with all diffusionsensitizing gradients applied in three orthogonal directions to obtain trace - weighted images . 
to take the reduced signal - to - noise ratio with the largest b values into account , six signal averages were chosen for b value of 0s / mm2 , 8 for b values of 500s / mm2 and 10 for a b value of 800s / mm2 . 
the asset ( array spatial sensitivity encoding technique ) imaging option with a scan time reduction factor of 2 was used , with a resulting scan duration of 2min and 30s . 
 after gadolinium infusion ( 0.1mmol / kg ) , lava ( liver 1 3 la radiologia medica ( 2019 ) 124 : 1926 acquisition with volume acceleration ) sequences ( tr 9.8 te mfov 26 , matrix 288 288 and slice 1mm ) were performed . adc analyses the adc analyses were articulated in three main phases : 1 . 
the entire tumor volume was delineated on the adc maps , using the t2 - weighted images and dwis with b = 800s / mm2 as a guide to the lesion location . 
the adc maps and the delineated contours were loaded in the matlab workspace ( release 2013a , the math works , inc . , natick , ma , usa ) , where dedicated scripts were developed for the quantitative image analyses . 
 from the volumetric distribution of adc values , the following parameters were derived : mean ( adcmean ) , standard deviation ( adcstd ) , median ( adcmedian ) , skewness and kurtosis . the skewness is a measure of degree of asymmetry of the distribution ( skewness is negative if the distribution is skewed to the left , while positive if it is skewed to the right )  . 
medcalc software ( version 9 , mariakerke , belgium ) was used for the statistical analyses . results from february 2011 until september 2017 , a total of 47 patients were initially selected for this study . 
among them , three patients were excluded because of strong susceptibility and / or motion artifacts on dwi , two patients were excluded because of largely necrotic nodes and three patients because they had histological confirmation of nasopharyngeal scc . 
 tumor characteristics are reported in more detail in table1 . mri was able to identify a small primary tumor in the hypopharynx in three patients , while mri findings were negative for detection of primary tumor in 16 patients . 
among these 16 patients , pet - ct was able to identify a primary tumor in the palatine tonsil for three patients and in base of the tongue for one patient ; the panendoscopy and tonsillectomy were useful in three patients ( they had small foci in palatine tonsil ) , while the site of primary tumor remained unknown in 9 patients . summary statistics of adc values for the two patient groups ( lymphoma and scc ) are reported in table2 and illustrated in fig.1. 
the edges of the box are the 25th and 75th percentiles , and the horizontal lines extend from the minimum to the maximum value , outliers being plotted with cross - markers . 
areas under the roc curves ( aucs ) for the most significant adc histogram parameters are reported in table3 , with the optimal cutoff values and the corresponding sensitivity and specificity . 
the adcmean and adcmedian had the best discriminative powers for differentiating lymphoma and scc , with optimal cutoff values as predictors for lymphoma of 0.83 103 mm2 / s and 0.73 103 mm2 / s , respectively . 
to eliminate the dependence of the histogram from the between - subject differences in the volume size , voxel counts were calculated as percentages , dividing them by the total number of voxels in the whole lymph node . some illustrative cases are reported in figs.3 , 4 and 5 . discussion the differential diagnosis between scc and lymphoma represents an important issue , particularly in patients affected by a painless neck mass with unknown clinical primary tumor , who already underwent a non - diagnostic fnac [ 7 ]  . 
 in this set of patients , mri and advanced mr techniques may have a central role in the differential diagnosis of malignant lymphadenopathies , as mri techniques provide an accurate tissue characterization , both anatomical and physiological [ 17 ]  . 
however , conventional sequences are limited because of some overlapping appearance of scc metastases and lymphoma , even if lymphomas typically shows lower t2 - weighted signal intensity and more homogeneous enhancement after contrast medium infusion [ 24 ]  . 
 previous studies demonstrated the ability of dwi to differentiate scc nodes and lymphomas , the last having lower adc values , compared to sccs , with an optimal cutoff of about 0.7 103 mm2 / s [ 1014 ]  . 
this is because npc is typically characterized by high concentration of macromolecular content , high cellularity , high nuclear to cytoplasmic ratio and low content of keratin [ 26 ] , which lead to decreased diffusion coefficients compared to other anatomic sites [ 27 ]  . 
for these reasons , it has been suggested in the literature not to consider sccs as a single group but to take into account the location of the primary tumor to assess the diagnostic power of dwi and determine the optimal adc cutoff values [ 25 ]  . in the present retrospective study , we evaluated the ability of whole - volume adc histogram of cervical lymph node to discriminate lymphomas from metastatic fig . 
3 axial t2 - weighted image ( a ) in a 59 - year - old man shows a right neck mass with homogeneous and moderately high signal intensity ; the parametric maps of the apparent diffusion coefficient adc in the same anatomical location ( b ) ; adc histogram within the entire tumor volume ( c )  . 
4 axial t2 - weighted image ( a ) in a 55 - year - old man shows a right neck mass in the levels iia and iib with disomogeneous and moderate hyperintensity signal ; the parametric maps of the apparent diffusion coefficient adc in the same anatomical location ( b ) , adc histogram within the entire tumor volume ( c )  . 
5 axial t2 - weighted image ( a ) in a 67 - year - old man shows a left neck node in the level iv with homogenous and moderate high signal intensity , without extranodal extension ; the parametric maps of the apparent diffusion coefficient adc in the same anatomical location ( b ) ; adc histogram within the entire tumor volume ( c )  . 
the histogram analysis does not allow a differential diagnosis between scc and lymphoma : the adcmedian was 0.80 103 mm2 / s , suggesting a scc , while adcmean was 0.83 103 mm2 / s , which was identical to the cutoff value . 
first - order statistics , including mean , median , standard deviation , skewness and kurtosis , was calculated on the basis of the distribution of the adc values to extract some texture features of the tumor heterogeneity [ 16 ]  . 
we hypothesized that considering the entire lesion instead of a single representative roi could improve the reproducibility and promote a standardization of dwi analysis [ 15 , 18 ]  . we found that both adcmean and adcmedian of lymphomas were significantly lower than those of the sccs , consistently with previous studies [ 8 , 12 ]  . 
correspondingly , adcmean and adcmedian had good auc values with remarkably high specificity and ppv scores : the cutoff value of 0.83 103 mm2 / s for adcmean allowed us a correct diagnosis in all the scc lesions . 
lymphomas had higher skewness as well , i.e. , exhibited a shift to the left in the distribution of adc values , which is indicative of 1 3 la radiologia medica ( 2019 ) 124 : 1926 remarkably decreased water mobility , as a consequence of the high cellularity and high nucleus - to - cytoplasm ratio of lymphomas [ 12 , 20 , 28 ]  . 
these features of the adc values distribution are better exemplified in fig.2 , by a visual comparison of the averaged adc histograms among the two patients groups . nevertheless , both kurtosis and skweness did not allow a differential diagnosis between lymphomas and non - nasopharyngeal sccs : they did not significantly differ between the two patient groups , though kurtosis showed a trend toward significance . 
 [ 8 ] , who reported that the 90th percentile of adc ( adc90 ) had the best diagnostic performance , followed by adcmean and adcmedian ; however , it was not indicated whether the differences between aucs of adcmean / adcmedian and adc90 were statistically significant or not . 
the optimal adc cutoff values in this study may not be straightforwardly applicable in other centers due to differences in dwi acquisition protocols , no consensus existing about the most appropriate number and range of b values . 
moreover , the lymphoma population had a prevalence of diffuse large b cell histology and this represents a risk of bias that could have affected our results . in future investigations , we plan to study the potential of combined analyses of t2 - weighted signal intensity and contrast enhancement together with adc , as we believe that this might further improve the diagnostic ability of mri findings to clarify the nature of cervical lymph node metastases . conclusions the whole - lesion adc histogram analysis of cervical lymphadenopathy may help to discriminate lymphomas from non - nasopharyngeal scc in patients with unknown clinical primary tumor . 
the adcmean and adcmedian values had the highest diagnostic powers , showing good diagnostic accuracy with remarkably high specificity . acknowledgements we thank michele farella , elisa tommasini , pierfrancesco rinaldi for their continued technical assistance . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the 145 cases of ggns were divided into pre - invasive ( pi ) group ( n = 46 ) , micro - invasive adenocarcinoma ( mia ) group ( n = 48 ) , and invasive adenocarcinoma ( iac ) group ( n = 51 )  . 
the presence of a tumourlung interface in the mia and iac groups was significantly higher than that in the pi group ( p < 0.05 ) , but no significant difference was found between the mia and iac groups . 
the presence of a pleural indentation sign in the iac group was significantly higher than that in the other two groups ( p < 0.05 ) , but no significant difference was noted between the latter two groups . 
no significant difference was found in the ggn density , vacuole sign , air bronchus sign and notch sign among the three groups . conclusions the hrct signs of ggns could be used to differentiate among pre - invasive lesions , micro - invasive lesions and invasive lung adenocarcinoma . keywords high - resolution computed tomography ground glass nodule pathologic classification lung adenocarcinoma introduction ground glass nodules ( ggns ) can be classified as pure ggns and mixed ggns , depending on whether they contain solid components [ 1 , 2 ]  . 
ordinary ct cannot display ggns or display them clearly , while * shuang - qing chen sznaonao@163.com 1 department ofoncology , the affiliated suzhou hospital ofnanjing medical university , suzhou215001 , china 2 department ofradiology , the affiliated suzhou hospital ofnanjing medical university , no . 
16 , bai - ta - xi road , suzhou215001 , jiangsuprovince , china high - resolution computed tomography ( hrct ) can improve the image quality and display ggns more clearly [ 3 , 4 ]  . in 2011 , the international association for the study of lung cancer ( iaslc ) , the american thoracic society ( ats ) and the european respiratory society ( ers ) jointly issued a new international multidisciplinary classification of lung adenocarcinoma and first proposed the term microinvasive adenocarcinoma ( mia ) [ 5 ]  . 
given the increased number of lung ggns detected and advocacy of the clinical strategy of the partial resection of pre - invasive and micro - invasive carcinoma , it is primarily important to differentiate among pre - invasive , micro - invasive and invasive adenocarcinoma lesions in the new classification [ 6 , 7 ]  . 
 the aim of the present study was to observe the relationship between hrct signs and the new pathologic classification vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 813 in ggn - like lung adenocarcinoma to explore the clinical value of hrct in the diagnosis of lung adenocarcinoma . materials andmethods patients the hrct data of 145 patients with single - onset ggns 2cm in diameter and surgically treated between january 2014 and december 2016 were retrospectively reviewed . 
 according to the 2011 edition of the international multidisciplinary classification of lung adenocarcinoma , they were classified into three groups : pre - invasive ( pi ) group ( n = 46 ) , including 21 cases of atypical adenomatous hyperplasia ( aah ) and 14 cases of adenocarcinoma insitu ( ais ) ; microinvasive adenocarcinoma ( mia ) group ( n = 48 ) ; and invasive adenocarcinoma ( iac ) group ( n = 51 )  . 
in the retrospective analysis , all patients provided informed consent requirement before enrolment , and the study was approved by the ethics committee of nanjing medical university . examination methods a philips brilliance 128 - slice spiral ct scanner was used for examination , with the patient holding their breath during the stable respirations . 
routine ct was first performed from the lung apex to the base ; after location of the nodule , high - resolution thin - section target scanning was performed under the conditions of 120kv , 299ma , 1 - mm thickness and a 1 - mm interval . 
depending on the size and density of the lesions , the window width and position were adjusted from time zero during the processing procedure to obtain the optimal images . image analysis the images were interpreted by two senior radiologists independently in a blind manner . 
density : the maximal ggn cross section was selected from the standard reconstruction images of the ggn by avoiding the blood vessel and bronchus ; three regions of interest ( rois ) were selected , the ct value was measured , and the mean value of three measurements was used for analysis . 
inside and around the ggn : tumourlung interface , pleural indentation , notch sign , air bronchus sign , vacuole sign , lobulated sign and spicule sign of the ggn . 
tumour microvascular ct imaging sign : the tumour microvascular ct imaging sign was defined when one or more vessels entered the lesion and the course of the vascular segment of the lesion was twisted and rigid . 
no significant difference was noted in the ggn density , notch sign , air bronchus sign and vacuole sign among the three groups . discussion with wider applications of hrct in recent years , the detection rate of ggn has increased obviously [ 8 , 9 ]  . 
a transverse thin - section target scanning imaging ; b coronary mpr imaging ; c pathology confirmed for iac 1 3 la radiologia medica ( 2019 ) 124 : 813 fig . 
a transverse thin - section target scanning imaging ; b sagittal mpr imaging ; c pathology confirmed for iac 1 3 12 la radiologia medica ( 2019 ) 124 : 813 first proposes the method of classification appropriate for surgical resection and biopsy , increasing the 5 - year survival rate of the complete surgical resection of pre - invasive and micro - invasive carcinoma to 100% [ 5 , 7 , 11 ]  . 
 [ 16 ] found that the size of pre - invasive ggns was significantly smaller than that of micro - invasive and invasive gnns , and the ggn size could help differentiate between pre - invasive and invasive lesions . 
the results of the present study showed that the ggn size was increased positively with the increasing degree of malignancy , and significant differences were noted in the ggn size among the three groups , findings that were consistent with those of eguchi etal . 
however , there was no significant difference in the ggn density among the three groups , suggesting that the ggn density is not an effective sign for the judgment of invasion . 
the cause may be that it is difficult to select rois when the lesion is not sufficiently large or the density is uneven . studies have shown that with the increasing degree of ggn invasiveness , the presence of lobulated , spicule and notch signs were also increased , reflecting the morphologic changes in ggn progression from a pre - invasive state to a micro - invasive / invasive state [ 17 , 18 ]  . 
it was found that , in the present study , the presence of lobulated and spiculated signs in micro - invasive and invasive adenocarcinoma was not only significantly higher than that in pre - invasive lesions but also showed a significant difference between micro - invasive and invasive lesions , indicating that these two signs have a relatively high value to assess the invasiveness and degree of invasion of gnn . 
 [ 20 ] pointed out that the presence of a rough tumourlung interface on ggns tended to indicate malignancy , likely because with the increase in the degree of invasion , the tumour cell arrangement on alveolar walls became dense and thickened , thus presenting a clearer tumourlung interface on ct imaging . 
we also found that the clarity of the tumourlung interface can be used as an indicator of pre - invasive and invasive lesions but did not seem to work effectively for the differentiation between micro - invasive and invasive adenocarcinomas . 
comparison of the tumour microvascular ct imaging signs showed that they occurred more frequently in the mia and iac groups than that in the pi group , implying that the entry of one or more vessels into the lesion and a twisted and rigid vascular running course within the lesion may suggest a greater possibility of malignancy of ggn [ 17 ]  . 
 the mechanism underlying microvascular formation remains unclear at present , possibly because of traction of the fibrous components within the lesion on the surrounding normal vessels , resulting in vascular course change . 
others have proposed that the infiltrative growth of the tumour tissue into small vessels of the lesion or interlobular infiltrative growth stimulated the growth of fibrous components , causing blood vessels to become twisted and rigid [ 21 , 22 ]  . 
in the present study , we found no significant difference between the micro - invasive and invasive groups , and further analysis is awaited concerning the details of tumour microvascular ct imaging signs . in summary , the size , lobulated sign , spicule sign , notch sign , tumourlung interface , and tumour microvascular ct imaging sign can help better understand the new classification of small ggn - like lung adenocarcinoma . 
the aim of the study is to isolate which features of magnetic resonance imaging ( mri ) - based radiomic analysis have to be considered the most significant predictors of metastasis in oncological patients with spinal bone marrow metastatic disease . materials and methods eight oncological patients ( 3 lung cancer ; 1 prostatic cancer ; 1 esophageal cancer ; 1 nasopharyngeal cancer ; 1 hepatocarcinoma ; 1 breast cancer ) with pre - radiotherapy mr imaging for a total of 58 dorsal vertebral bodies , 29 metastatic and 29 non - metastatic were included . 
a wilcoxon test was applied to the 89 features and the most statistically significant of them underwent to a stepwise feature selection , to find the best performing predictors of metastasis in a logistic regression model . 
 an internal cross - validation via bootstrap was conducted for estimating the model performance in terms of the area under the curve ( auc ) of the receiver operating characteristic . results of the 89 textural features tested , 16 were found to differ with statistical significance in the metastatic vs nonmetastatic group . 
the internal cross - validation showed an auc of 0.8141 ( 95% ci 0.68540.9427 ) in t1 images and 0.9116 ( 95% ci 0.82940.9937 ) in t2 images . conclusions the results suggest that mri - based radiomic analysis on oncological patients with bone marrow metastatic disease is able to differentiate between metastatic and non - metastatic vertebral bodies . 
the most significant predictors of metastasis were found to be based on t2 sequence and were one morphological and one textural feature . keywords vertebral metastases radiomics magnetic resonance quantitative imaging oncology radiotherapy * laura filograna laura.filograna@gmail.com 1 department ofradiation oncology gemelli - art , catholic university ofrome , school ofmedicine , foundation university hospital a . 
gemelli 8 , 00168rome , italy 4 department ofdiagnostic andinterventional radiology , molecular imaging andradiotherapy , ptv foundation , tor vergata university ofrome , viale oxford 81 , 00133rome , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 5057 introduction metastatic bone disease is , unfortunately , a common event in the evolution of cancer . 
the development of metastases represents a challenge for the clinician who manage with oncological patients , because , once bone metastases occurred , cancer becomes a systemic pathology and palliative therapy is the only viable approach . the spine is the commonest site of metastases . 
in radiomics a large amount of advanced quantitative imaging features are extracted from medical images obtained with computed tomography ( ct ) , positron emission tomography ( pet ) or magnetic resonance imaging ( mri ) , with the aim to build diagnostic , prognostic and predictive models . since its origin , this image analysis method has been largely employed in the management of oncological patients . 
many other studies with radiomics - based analysis have been performed in the management of different tumors types [ 712 ]  . magnetic resonance ( mr ) imaging plays a crucial role in the characterization of spinal bone marrow disorders and in monitoring response to therapy [ 13 ]  . 
for these reasons mr is considered an imaging method of vital importance for the management of oncological patients with bone marrow metastatic disease . to our knowledge , there is only one paper using both morphological and textural features analysis on mr imaging for the study of vertebral bone marrow metastases [ 14 ]  . 
in particular , the authors analyze preand post - radiotherapy mr imaging for evaluating early response to therapy in patients with metastatic cancer , with promising results [ 14 ]  . in this paper , from pre - treatment mr images of oncological patients with diagnosed vertebral bone marrow metastases quantitative imaging features of pathological vs non - pathological vertebral bodies are extracted by t1 and t2 images and analyzed with the aim to isolate which features of mr imaging - based radiomic analysis have to be considered the most significant predictors of spinal bone marrow metastatic disease in oncological patients . materials andmethods eight patients ( 5 male , 3 female , age range 4180 aa , mean age 60years old ) with cancer ( 3 lung cancer ; 1 prostatic cancer ; 1 esophageal cancer ; 1 nasopharyngeal cancer ; 1 hepatocarcinoma ; 1 breast ) with vertebral bone marrow metastases with pre - radiotherapy mr imaging were examined . 
a vertebral body was considered metastatic on mri , if on t1 - weighted sequences the lesion appeared hypointense compared to fatty tissue , and if on t2 - weighted images it showed a variable hyperintensity [ 15 ] , with or without a hyperintense halo , due to perilesional edema [ 16 , 17 ]  . none of the vertebral bodies examined had pathological or non - pathological fracture . 
the obtained data were transferred to an automated data extraction system for morphological , statistical and textural analysis . three groups of features were used for the analysis : statistical / histogram , morphological and textural features . 
in statistical / histogram features , the three - dimensional data from contoured volume are translated to an histogram that illustrates the fractional volume in the examined structure for the range of voxel values , in this study , intensity values . 
to the histogram , statistic tests can be applied for calculating , for example , skewness , kurtosis , median , mean . 1 3 la radiologia medica ( 2019 ) 124 : 5057 fig . 
1 60 - year - old woman with breast carcinoma : the images are referred to sagittal t1 image ( a ) and the same sagittal t1 image ( b ) with the roi traced on a non - metastatic vertebral body , visualized with a particular ( non - diagnostic ) viewer built for moddicom - based radiomic analysis . 
also other more complex features such as the surface to volume ratio or descriptors of tumor compactness can be determined . finally , textural features are based on second - order statistics or co - occurrence matrix . 
by the co - occurrence matrix many advanced features can be extracted , for example , contrast , autocorrelation , correlation , cluster prominence , maximum probability , dissimilarity , sum entropy , sum variance . 
grey - level run length matrix features can describe grey - level non - uniformity , short and long run emphasis , run length non uniformity , high grey - level run emphasis , low grey - level run emphasis . with the aim to find among this large amount of features the most representative in differentiating metastatic vs nonmetastatic vertebral bodies in the study population selected , initially a total of 89 features deriving from the three groups ( statistical / histogram , morphological and textural features ) have been extracted without any kind of image filtering for 1 3 la radiologia medica ( 2019 ) 124 : 5057 fig . 
2 72 - year - old man with lung cancer : the images are referred to sagittal t1 image ( a ) and t2 fs image ( c ) and the same sagittal t1 image ( b ) and t2 image ( d ) with the roi traced on a metastatic vertebral body , visualized with a particular ( non - diagnostic ) viewer built for moddicom - based radiomic analysis . 
note presence of an ocular metastasis hypointense in t1 ( a ) and hyperintense in t2 fs image ( c ) , and the dishomogeneity of the pixel colors distribution for the presence of a focal concentration of color pixel corresponding to the metastasis t1 and t2 mri scans . 
the image processing and feature extraction was performed with the r library moddicom for radiomics analysis , a library whose aim is to support medical image analysis , feature extraction , radiobiological and clinical modeling . 
 the statistical software r version 3.4.2 was used for statistical analysis [ 18 ]  . given the set of features , their number was furtherly restricted by using a wilcoxon test , performed to investigate their statistical significance with respect to the outcome ( differentiating metastatic vs non - metastatic bodies )  . 
these two features were found the best ones for discriminating among metastatic and non - metastatic vertebral bodies in t2 weighted images , in our study population . 1 3 la radiologia medica ( 2019 ) 124 : 5057 discussion in this paper , mri - based radiomic analysis on untreated with radiotherapy oncological patients with bone marrow metastatic disease has been demonstrated as being able to differentiate between metastatic and non - metastatic vertebral bodies . 
furthermore , two features for t1 ( one morphological , and one histogram feature ) , and two for t2 images ( one morphological and one textural feature ) were identified as the best differentiating healthy and metastatic vertebral bodies in a radiomic analysis , respectively , in the two imaging data sets . the process of radiomics consists on the extraction and analysis of advanced quantitative imaging features with the aim of creating mineable databases for conducting predictive and prognostic correlations between images and patients outcome [ 17 ]  . the classical approach in imaging analysis of cancer is based on qualitative inferences ; a quantitative approach consists generally on the measurement of tumor dimensions or on a region of interest ( roi ) - based analysis . 
 unfortunately , these measurements , particularly tumor dimensions , do not reflect the tumor tissue complexity and do not generally correlate with prognosis . in opposition to the classical approach , radiomics analysis of tumor , by analyzing quantitative features related to tumors texture and morphology , offers the possibility to generating predictive models . according to kumar [ 17 ] , the radiomics process includes five steps , i.e. , ( 1 ) image acquisition and reconstruction , ( 2 ) image segmentation and rendering ( 3 ) feature extraction and feature qualification ( 4 ) databases and data sharing and ( 5 ) ad hoc informatic analyses . 
each of these steps poses some specific challenges . in the present study this process was applied on metastatic vertebral bodies , by using moddicom , an userfriendly and freely available library , able to be the platform for conducting radiomics analysis as proposed by dinapoli etal . 
the tumoral mass can be characterized by a very large amount of quantitative features that describe its complexity , belonging to the three large groups of radiomics features reported in the section materials and methods . this huge amount of features includes also some features that may not be straightly representative of the fig . 
3 in this figure , the area under the curve ( auc ) of the receiver operating characteristic ( roc ) deriving from the cross - validation via bootstrapping technique on the model constructed on t1 images ( features : center of mass shift and minimum grey level ) is illustrated fig . 
as kumar underlines [ 11 ] , often the number of radiomics features potentially included in the analysis is higher than the number of the subjects examined , particularly if it is considered that the study population included in this kind of studies , rarely is large . 
thus , the risk is to reduce the power of the study , and to augment the possibility of over fitting data . in this context , the selection of specific features best fitting the specific task in the management of the oncological patient under examination is crucial for optimizing the study . in this contribute , oncological patients with diagnosed vertebral bone marrow metastatic disease were analyzed with a radiomics approach based on mr images , according to the protocol proposed by dinapoli etal . 
in 2013 [ 14 ] tried to apply radiomics principles on preand post - radiation therapy mr examination of the spine for evaluating early therapy - induced bone marrow changes . 
in this work the authors conduct a roibased analysis on mr images related to 35 patients with spine and hip using 36 radiomics features with the aim to create a neural network - based classification system for the recognition and characterization of post - radiation bone marrow lesions detected with conventional mr imaging . 
among the 36 features , five textural ones were isolated as the optimal : the standard deviation , the difference entropy , the sum average , the entropy and the long run emphasis . in the present study 89 features for the 58 vertebral soma ( 29 metastatic and 29 non - metastatic ) examined in both t1 and t2 images were computed . 
of these features , 6 for t1 and 10 for t2 were found to differ with statistical significance in the metastatic vs non - metastatic group , and two of these , respectively , for t1 and two for t2 images have been demonstrated as predictors best performing for the characterization of vertebral bodies affected by metastases . 
moreover , one histogram feature , minimum grey level , and one textural feature , grey - level co - occurrence matrix joint variance , were found as being the best fitting features , respectively , in t1 images and t2 images . center of mass shift is the distance between the roi volume centroid and the intensity - weighted roi volume centroid , and measures the placement of high and low intensity regions within the volume . 
grey - level cooccurrence matrix joint variance is the grey - level weighted variance of joint probabilities . going beyond the specific meaning of each feature , it is important to note that the more robust results according to the p value , auc calculation to 95% ci were the two features isolated on t2 sequence ( tables1 , 2 )  . 
particularly , they were one morphological feature center of mass shift and one textural feature grey - level co - occurrence matrix joint variance . both the selected features straightly depend on the heterogeneity of signal intensity of the vertebral body examined . 
moreover , the evidence that t2 fat saturated images best describe the differences between non - metastatic and metastatic vertebral bodies can be explained by the fact that the presence of the metastatic tissue causes more important variation in the distribution of the signal intensity in t2 fat saturated images than it does occur in t1 images . 
on t2 fat saturated images , in fact , the signal hyperintensity differences are more evident with respect to the surrounding not affected bone marrow than in t1 images , as they better reflect not only the presence of the tumoral tissue , but also the perilesional edema . this study has some limitation . 
many factors , in fact , influence the signal intensity of the nonmetastatic vertebral bodies , in relation to the different percentages of adipocytes and red marrow depending on the age , eventual medicament assumption of the subjects , etc . 
a larger study population is needed to clarify the influence of these factors on the final results . in conclusion , in this study the radiomics features most representative of metastatic versus non - metastatic vertebral bodies are identified in our model . 
with the advantage to foster radiomics analysis for the study of vertebral bone marrow metastatic disease , we propose the privileged use of one morphological feature , center of mass shift , and one textural feature , grey - level co - occurrence matrix joint variance , in t2 fat saturated images . 
at 1 - month follow - up enhanced mri , complete remission was achieved in 82.6% of patients ( 38 / 46 ) , and partial remission in 17.4% ( 8 / 46 )  . 
tace combined with simultaneous rfa provides a new treatment option for solitary large hccs in which dynact has important clinical value . keywords hepatocellular carcinoma therapeutic embolization interventional radiology dynact introduction compared with other countries , large hccs ( maximal diameter > 5cm ) have a higher incidence in asia , especially in china . 
newer technologies such as the flat - panel detector digital subtraction angiography ( dsa ) system with cbct have become popular in clinical practice , and perspective , photography , dsa , and 3d reconstruction / imaging can be performed simultaneously on the same working bed using dynact [ such as the artis zee dsa system with cbct ( siemens , germany ) ] [ 9 ]  . 
 after tace under dsa , dynact can be used for scanning vol . : ( 0123456789 ) 1 3 2 la radiologia medica ( 2019 ) 124 : 17 and imaging and the puncture site and the route can then be determined . 
the use of dynact not only realizes simultaneous combination of tace and rfa , but also maximizes the synergistic effect of tace and rfa , increasing therapeutic efficacy [ 11 ]  . 
ultrasound also could be simultaneously used to guide ablation after tace [ 12 ] , and that contrast - enhanced ultrasound and fusion imaging were another advanced technique for difficult cases [ 13 ]  . 
 this study was undertaken to investigate the clinical value and safety of dynact in the treatment of solitary large hccs . materials andmethods general patient characteristics all patients were diagnosed with hcc by imaging or pathological examination and received tace with simultaneous dynact - guided rfa . 
a radio frequency of 460khz was chosen , and a rita multipolar radiofrequency ablation electrode needle ( outer tube diameter : 14g ) with nine hook - shaped bundle electrodes ( umbrella - like opening with the diameter of 5cm ) was used . treatment methods tace treatment after routine skin sterilization , local anesthesia with lidocaine was administered . 
rfa was performed immediately in the region where iodine oil deposition is poor under the guidance of dynact . dynactguided syngo iguide needle puncture dynact image acquisition lateral x - rays . 
the following parameters were used : rotation angle of c - arm : 200 ; rate of image capture : 50 frames / s ; increment in each frame : 0.5 ; x - ray dose : 0.36gy / frame ; total time : 8s ; and total number of frames : 396 . 
the inner puncture target spot was selected , and the surface puncture was marked , according to the puncture routine automatically selected by the iguide software ( fig.1b ) ; the depth of puncture was also displayed ; ( 2 ) the bulls eye position was selected , the operating lever was pushed , the c - arm was automatically fixed at the bulls eye position , and then the inner puncture site was assured to overlap the surface puncture site . 
rfa was performed using a power of 150200w and temperature of 105c for 1520mfor the large tumor size , the needle location was adjusted after ablation at a site for further ablation until the ablated area covered the edge of the tumor and its three - dimensional space . 
we studied the time to progression ( ttp ) and 1 - , 2 - , and 3 - year survival rates . response assessment technical success was defined as completion of both tace and rfa in one treatment session . 
initial tumor response was assessed by contrast - enhanced mri 1 month after treatment according to the modified response evaluation criteria in solid tumor ( m - recist ) developed by the american association for the study of liver diseases ( aasld ) [ 14 ] : complete remission ( cr ) , partial remission ( pr ) , stable disease ( sd ) , progressive disease ( pd )  . 
for a lesion close to the important organs ( peripheral lesion , subdiaphragmatic lesion , and lesion close to the intestine ) , lidocaine in normal saline was injected to separate the lesion from surrounding tissues , followed by puncture . 
after initial treatment , ten patients received a second tace or rfa during follow - up , of whom cr was achieved in seven patients ( as the remaining patients did not receive further tace or rfa due to tumor progression or personal rejection )  . 
the occurrence rate of grade 3 was 6.5% , included subcapsular hematoma of liver ( n = 2 ) , sand diaphragmatic damage with pleural effusion ( n = 1 )  . discussion in recent years , rfa has become a common nonsurgical treatment besides tace and its effectiveness has been confirmed in small hccs , comparable to that of radical treatments ( such as surgical intervention and liver transplantation )  . 
with the development of rfa instrumentation and imaging guidance equipment and the accumulation of clinical experience , rfa has been increasingly used in the treatment of large hccs [ 17 ]  . 
local tumor progression - free survival after dynact - guided tace with simultaneous rfa ( b ) 1 3 6 la radiologia medica ( 2019 ) 124 : 17 combination of tace with simultaneous rfa , providing a new , convenient , and effective treatment for large hccs . 
 [ 14 , 19 ] employed tace with simultaneous cbct - guided rfa in the treatment of large hccs in 21 patients , with a technical success rate of 100% . dynact employs ctcb using the artis zee dsa system ( simens , germany ) and can realize synchronized acquisition with flat - panel detector during c - arm rotation . 
after image reconstruction using the workstation , three - dimensional images of the target lesion and ct images of soft tissues can be obtained , which overcomes the limitations of traditional instruments . 
at 1 , 2 , and 3years after surgery , the survival rate was 89.1% ( 41 / 46 ) , 71.7% ( 33 / 46 ) , and 56.5% ( 26 / 46 ) , respectively , which is consistent with the survival rates reported by takaki etal . 
in 46 patients , no intraoperative and postoperative severe complications were observed , suggesting favorable safety of this technique . based on our findings , dynact - guided tace with simultaneous rfa appears safe and reliable for treatment of solitary large hccs . 
the advantages of this technique include simultaneous combination of tace and rfa which reduces the time interval between two treatments , thus avoiding the clearance of lipiodol and chemotherapeutics and the formation of new collateral vessels and vascular recanalization after embolization in this time interval [ 21 ]  . 
in addition , dynact - guided tace with simultaneous rfa may exert a synergistic effect , i.e. , rfa after complete lipiodol deposition may maximize the heat conduction effect of the lipiodol , and , therefore , the heat produced by the rf needle can focus on the site of lipiodol deposition , exerting maximum anti - tumor effect ; this is important for irregular large hccs because peripheral tumor is difficult to completely ablate by rfa , but rfa after complete lipiodol deposition improves transduction of heat to peripheral tissues , which reduces the risk for recurrence and metastasis [ 19 , 22 ]  . 
with rotation of the c - arm , the patients can receive rfa on the same treatment bed without movement after tace , which avoids the transfer of patients which normally occurs during traditional interventional therapy . 
finally , the instrument can provide information in a real - time manner , which is helpful for the adjustment of treatment protocol ; dynact scanning after tace can accurately display and identify lipiodol deposition in normal liver tissues , which is helpful for decision making in surgery ( i.e. , whether or not additional lipiodol injection is needed ) [ 23 ]  . of note , dynact has several limitations including : ( 1 ) the puncture should be continuously monitored by dynact , which increases the radiation exposure to clinicians ; ( 2 ) the images obtained from dynact should be subjected to mpr reconstruction in the workstation , and the reconstructed images have poor resolution and poor intensity differences between tissues as compared with those from routine ct [ 24 ]  . 
the inclusion and exclusion criteria were strict , i.e. , patients should receive complete preoperative examinations , the functional reserve of the liver should be carefully evaluated , liver - protective treatment should be administered after surgery to avoid liver failure , especially for those with poor liver reserve function , chemotherapeutics acting on cell division or proliferation were preferred , and two or more chemotherapeutics were recommended for chemotherapy [ 25 ]  . 
in addition , local analgesic treatment with lidocaine was administered during surgery because patients receiving combined treatment experience longer operative times . conclusions our results indicated that dynact - guided tace with simultaneous rfa is a safe and efficacious treatment for solitary large hccs . 
the aim of the present paper is to increase awareness , acceptance and adoption of interventional radiology procedures for the treatment of bm ; and to present the joint position of the italian college of musculoskeletal radiology and the italian college of interventional radiology . keywords bone metastasis skeletal - related events interventional radiology epidemiology andclinical manifestations ofbone metastases bone metastases ( bm ) are the most common malignant lesions of the bone , commonly involving the axial skeleton , pelvic ring and proximal extremities [ 1 ]  . 
in the usa , it is estimated that approximately 100 , 000 individuals develop bm every year [ 2 ] ; and the incidence is expected to increase in the future due to the improved survival of cancer patients . 
 the incidence of bm is particularly high in patients suffering from breast , prostate or lung cancer ; intermediate in those presenting with melanoma , renal or thyroid cancer ; and relatively low in patients presenting with gastrointestinal tumors . * roberto luigi cazzato gigicazzato@hotmail.it extended author information available on the last page of the article bm significantly impact patients clinical status due to pain , fractures , compression of nearby structures such as nerves , hypercalcemia , and often require radiation therapy ( rt ) and / or surgery , especially when spinal cord compression is noted . 
usually three types of fractures occur in cancer patients , namely pathologic fractures ( pf ) , impending fractures ( imf ) , and fractures related to bone insufficiency ( bif )  . 
lastly , bif result from bone reabsorption due to vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 3449 medical therapies ( e.g. , hormonal therapies , steroids ) and / or cytokines produced by the tumor [ 57 ]  . current treatment modalities to treat pain and prevent fractures are medical therapy ( including analgesics , bisphosphonates and denosumab ) and rt ; both allow good but far from excellent results . 
although rt is considered the best evidencebased non - interventional treatment for bm - related pain , several limitations have been observed : ( a ) ineffectiveness in case of radio - resistant tumors such as renal cancer or melanoma ; ( b ) 12 - week latency between the end of treatment and the onset of pain relief ; ( c ) overall ( complete and partial ) pain relief observed in less than 60% of patients and recurrent pain in up to 50% of those who respond by 2024weeks after the end of treatment ; ( d ) retreatment is not always possible if the maximal radiation dose has already been delivered ; ( e ) no immediate bone consolidation is provided [ 35 ]  . 
 although the recently introduced tumoricidal stereotactic body rt yields higher rates of local tumor control and pain management compared with standard external beam rt [ 9 , 10 ] , the risk of secondary fracture is significantly increased when the former technique is used [ 9 ]  . 
on the other hand , bone - targeting agents interfering with tumor - mediated osteolysis , can reduce but not completely remove the risk of sres [ 3 ]  . in this setting , interventional radiology procedures may play an important primary or complementary role to manage bm [ 1113 ] , especially in the palliative setting where pain and fracture management is necessary . the aim of the present paper is to increase awareness , acceptance and adoption of interventional radiology procedures for the treatment of bm ; and to present the joint position of the italian college of musculoskeletal radiology and the italian college of interventional radiology . interventional procedures osteoplasty indications percutaneous osteoplasty refers to polymethylmethacrylate ( pmma ) injection into weakened or fractured bone . 
on the other hand , in case of tumor compression of the spinal cord or in case of vertebral instability due to tumor involvement of the posterior elements of the vertebra , surgical decompression / stabilization should be considered as early as possible . 
this is due to the fact that pmma has limited resistance to torsion and bending ; therefore , surgical endomedullary nailing is the preferred option to achieve effective biomechanical stabilization . 
 absolute contraindications to osteoplasty are local / systemic infection , known allergy to the pmma and irreversible coagulopathy . technique the procedure can be performed under fluoroscopic and / or ct - guidance often under local anesthesia / mild sedation . 
the consolidation time of pmma is variable ( 820min ) , and its polymerization results in an exothermic reaction with temperature > 70c , which is , however , inadequate to achieve effective local tumor control . results osteoplasty has been proved to be effective for the symptomatic treatment of osteolytic tumors including multiple myeloma . 
1 a , b painful lytic metastasis of t12 in a 70 - year * old patient suffering from hepatocellular carcinoma ; the metastasis disrupted the posterior wall of the vertebral body ( white arrows )  . 
c , d percutaneous vertebroplasty was safely performed with immediate pain relief and no cement leakage ( vertebroplasty was also performed in t11 and l1 during the same interventional session due to painful pathological fractures ) fig . 
b the fracture was fixed percutaneously by means of a compressive screw ; the screw tip was fixed in distal normal bone through the injection of few ml of cement ( white arrow ) osteosynthesis indications percutaneous osteosynthesis is consistent with screw fixation to consolidate minimally / non - displaced fractures of the pelvic ring [ 21 ]  . 
the technique can also be performed in the proximal femur to consolidate imf ( i.e. , mirels score 8 ) without significant trochanteric and cortical involvement [ 22 , 23 ]  . 
accordingly , osteosynthesis should be strictly reserved for non - surgical cancer patients with limited life expectancy to provide rapid analgesia and mobilization 1 3 la radiologia medica ( 2019 ) 124 : 3449 without the need for suspension of systemic therapies , which is often necessary with surgical treatments . 
moreover , compared to surgery , risk of bleeding and infection is also significantly reduced . thermal ablation indications technique percutaneous osteosynthesis is performed under fluoroscopic and / or ct - guidance . 
due to the long procedural time ( around 2h due to challenging bone access ) , general anesthesia is usually preferred over local anesthesia / mild sedation . threaded screws are used in case of mildly displaced fractures in order to achieve maximal inter - fragment compression . 
finally , pmma - injectable screws providing distal holes are preferred in cases of advanced osteoporotic bone to enhance screw anchoring . the most challenging phase of the procedure is often the perpendicular bridging of the fracture line by means of a 1.82mmk - wire ; after which , the screw is manually advanced over the wire by means of a screwdriver until its distal tip is safely anchored within distal healthy bone , and its head abuts the cortical bone . results osteosynthesis has been shown to be effective for the symptomatic treatment of pelvic fractures or those of the proximal femur . 
in a study of 64 patients undergoing pelvic osteosynthesis alone or in combination with osteoplasty , a median pain reduction of 6 / 10 points was noted , with only two secondary fractures observed in the proximal femur [ 25 ]  . 
another similar series of 33 patients reported an effective analgesic / functional amelioration in 87.1% cases at 1 - month follow - up [ 21 ] ; nevertheless , three major and one minor complications were reported . 
moreover , although no secondary fractures were reported , unfavorable local evolution of the treated site ( i.e. , poor consolidation and / or screw loosening ) was noted in 12.5% cases on imaging follow - up ( mean 8.7month ) thus , suggesting the need for strict clinical follow - up . 
the final necrotic volume depends on the amount of energy delivered and the local tissue characteristics such as vascularization , which may be responsible for energy dissipation ( i.e. , heat / cold - sink effect ) [ 26 , 31 ]  . compared to rt , the effects of ablation are immediate and there is no limit to the number of ablative treatments that can be performed on the same tumor , which is not the case for rt as it cannot be repeated once the maximum dose of the target organ is reached . 
in the majority of cases , bone consolidation can be combined with ablation in the same session . anesthesia ( deep sedation , general anesthesia , nerve block or spinal anesthesia ) is usually required [ 32 ]  . 
antibiotic prophylaxis remains controversial although it is generally applied [ 32 ]  . techniques laser lasers deliver electromagnetic energy in the infrared wavelength through small optic fibers deployed coaxially into 18g needles . 
however , only small ablation zones can be obtained since , even when multiple fibers are activated simultaneously , ablations zones rarely exceed 23cm [ 3133 ] ; for this reason , lasers can be applied to treat only small benign bone tumors such as osteoid osteoma [ 34 ]  . radiofrequency ablation ( rfa ) rfa is probably the most commonly applied technique in bone ablation [ 31 , 33 , 35 ]  . 
for this reason , rfa cannot be used if pacemakers or other implantable electric devices are present , or in case of osteoblastic bm impeding effective conduction of the electrical current , which can flow between the electrode and the grounding pads attached on the skin of the patient ( unipolar system ) , or between two electrodes or two dipoles localized at the distal tip of the same electrode 1 3 38 la radiologia medica ( 2019 ) 124 : 3449 fig . 
f bilateral bipolar rfa was performed with thermal monitoring at the level of the posterior wall ( white arrow ) and hydro - dissection of the epidural space ( black arrow ) ; g , h in the end , vertebroplasty was performed to prevent a secondary vertebral body collapse . 
nevertheless , rfa cannot achieve ablation zones that exceed 34cm . microwave ablation ( mwa ) mwa uses electromagnetic energy , which is delivered through an antenna [ 31 , 35 , 38 ]  . 
the main drawbacks of mwa are : ( a ) oval - shaped ablations , especially with first generation antennas ; ( b ) limited experience available with bm due to the fact that the technique is relatively new [ 39 , 40 ]  . cryoablation ( ca ) ca destroys tumors using cold temperatures ( up to - 40 c ) dissipated into tissues through dedicated cryoprobes [ 3033 , 35 ]  . 
 cellular death occurs through a complex mechanism that is not completely understood , including mechanical damage to cellular membranes induced by ice crystals , osmotic changes into the tissue , endothelial injury , ischemia , and cryo - immunological effects . 
compared to the other techniques of ablation , the main advantages of ca are : ( a ) precise control of the ablation area due to adequate visualization by common imaging modalities ( especially ct or mri ) , thus allowing for precise intra - operative evaluation of tumor coverage ; ( b ) multiple probes ( up to 40 with the most recent systems , each with different sizes and shapes of ablation ) can be simultaneously activated with a final synergistic effect ; therefore , the iceball can be shaped according to tumor morphology , and large - volume bm can be treated ; ( c ) possibility of treating osteoblastic bm since the iceball can easily go through cortical and blastic bone ; ( d ) since the iceball has intrinsic anesthetic properties , the procedure is less painful compared to heat - based techniques ; accordingly , ca is preferred for the treatment of bm with soft tissue extension . 
apart from its totally non - invasive profile , mrgfus has the benefit of allowing optimal mri resolution to target bm , and allows monitoring of the temperature reached within the tumor , surrounding it as well as in interposed tissues ( except bone )  . 
on the other hand , since bone can absorb the ultrasound beam , it is possible to induce high periosteal temperatures to achieve effective pain management in case of painful bm . 
drawbacks include limited availability of the technique , long procedural time ( 23h ) , and contraindication in patients contraindicated to mri . protective measures to adopt during bone ablation thermal ablation is generally considered safe ; nevertheless , the most common complications include the unintentional ablation of nearby non - target organs , particularly nerves . 
in bone ablation , all these measures can be applied ( table1 ) alone or in combination to avoid iatrogenic injuries , in particular for nerves and sk co2 or fluids are often injected to achieve physical displacement . 
the great advantage of fluid dissection over table 1 protective measures that can be adopted during ablation advantages disadvantages fluid dissection angioplasty balloon low thermal conductivity highly soluble no renal or hepatic toxicity non - allergic low cost sterile suitable with all imaging modalities ( us , ct , and mri ) : spontaneous visualization under mri - guidance ; increased visualization under ct - guidance with 510% contrast medium dilution low cost sterile allow for temperature adjustment non gravity - dependent distribution no need for volume readjustment no cooling or warming properties distribution in anti - declivous areas unsuitable for us - guidance distribution to dependent area potential fluid overload temperature monitoring somatosensory - evoked potentials precise knowledge of the temperature in critical areas needs precise thermocouple deployment precise monitoring of electrical conduction of the tested nerve relatively expensive technically challenging unsuitable for the protection of neurological structures difficult to be performed requires dedicated trained physicians no neuromuscular blocking neither muscle relaxant agents should be administered during the procedure cannot be used continuously in order to prevent muscle fatigue no neuromuscular blocking neither muscle relaxant agents should be administered electrostimulation simple to be performed no specific training required 1 3 40 la radiologia medica ( 2019 ) 124 : 3449 co2 is that fluid temperature may allow for warming - up or cooling - down of the non - target structure during ablation . angioplasty balloon ( 510mm 2040mm ) interposition is rarely used due to the high risk of nerve damage during balloon manipulation . temperature monitoring is usually achieved directly through percutaneous deployment of thermocouples or fiber - optic sensors that can be easily combined with fluid dissection , especially when the latter alone is not deemed sufficient . 
in case of mrgfus ablation , non - invasive mrimediated temperature monitoring can be obtained . electrostimulation and somatosensory - evoked potentials allow for the functional monitoring of nerves during the ablation and are particularly useful since nerve roots are very sensitive outside the physiologic range ( 1045c ) [ 4650 ]  . 
usually , fluids ( including local anesthetic agents ) are injected within the sub - cutaneous tissue to increase its width ; additionally , sterile gloves filled with hot or cold saline can be transiently applied on the target area to mitigate skin temperature change during the ablation . results reported in patients affected by tumors that are commonly considered aggressive , such as lung cancer [ 51 ]  . 
accordingly , it is important to take into account each patients tumor biology when selecting candidates for curative ablation . a considerable number of papers provide evidence of ablation in achieving fast and effective pain relief in patients presenting with painful bm ( table3 )  . 
given the non - invasive profile of hifu , it is likely that it will obtain a prominent position in the future for the palliative management of bm . embolization indications the aim of trans - arterial embolization ( tae ) is to devascularize hyper - vascular bm and to preserve all non - target vessels . 
accordingly , tae should be as selective as possible . tae can be applied in case of hyper - vascular bm in order despite the relative few patients that can benefit from curative treatments , growing evidence is demonstrating the effectiveness of such therapeutic treatments in selected patients ( table2 )  . 
minimize the blood loss during subsequent surgery ; in this scenario , tae should be performed within 3days from surgery to reduce the risk of tumor revascularization [ 5255 ] ; table 2 results of curative ablation study histology sitea ablation modality mean tumor size ( cm ) no . 
 nsclc bone ca , rfa , 45 ( 76 ) 68% 1years 2.6% nr not reported , ca cryoablation , rfa radiofrequency ablation , mwa microwave ablation , mskmusculoskeletal , nsclcnon - small - cell lung carcinoma a study includes metastatic sites beyond bone and soft tissue ; only data related to bone and soft tissue metastases are reported [ 82 ] [ 83 ] [ 85 ] [ 51 ] mean 1 3 la radiologia medica ( 2019 ) 124 : 3449 table 3 results of palliative ablation study ablation modality no . 
permanent agents are most commonly used for preoperative tae and for palliative cases ; however , temporary agents such as gelatin sponge have also shown their efficacy before surgery [ 56 ]  . 
4 a large ( 13 cm ) painful right iliac metastasis from hepatocellular carcinoma in a 55 - year - old patient undergoing combined single - session embolization and cryoablation ; due to the metastasis , the patient was bedridden . 
 d , e cryoablation was accomplished by means of 10 cryoprobes producing a large iceball ( * ) , and with concomitant hydro - dissection to protect the femoral nerve ( white arrow )  . 
f 1 - month mri follow - up showed complete devascularization of the tumor ( * ) ; at the same time interval the patient was able to walk again 1 3 42 results arterio - venous shunts . 
lastly , particles are most commonly used for bone devascularization and the choice of particles diameter ( 401200 micron ) is dependent on vessel size and desired distal embolization . in a large series of 93 patients undergoing pre - surgical embolization of spinal tumors , the benefits of embolization have been demonstrated in terms of reduction of intra - operative blood loss , especially when hyper - vascular bm from renal cell carcinomas were treated , and extensive surgery ( corpectomy / vertebrectomy ) was performed [ 57 ]  . another series of 243 patients undergoing bm embolization reported > 50% and 97% reduction in pain and analgesic consumption , respectively . 
nevertheless , post - embolization syndrome , ischemic pain at the embolization site , paresthesia , skin breakdown , and sub - cutaneous necrosis were observed in 35% patients [ 58 ]  . preprocedure workup , clinical andtechnical requirements normal coagulation parameters , renal function and the absence of infection should be checked . 
a series of prognostic factors favouring curative treatments have been identified : oligometastatic / metachronous status ; the absence or limited cortical bone disruption ; limited bm size ( < 2cm ) ; long life expectancy ; and good patient performance status [ 59 ]  . 
patients should be offered such treatment in case of focal pain ( 4 / 10 on a 010 visual analogic scale over the 24h ) corresponding to a focal bm on cross - sectional imaging . 
 ideally , ablation should target the interface between the normal bone and the bm ; nevertheless , whenever possible , complete bm destruction should be achieved . tumor debulking can be achieved with ablation such as in the case of bm extending to surrounding soft tissues or spinal tumors growing quickly into the spinal canal . 
 nevertheless , it should be noted that local tumor control cannot be achieved if the bm has already invaded the anterior epidural space . despite the curative or palliative intent , when ablation and / or embolization are performed ( or following rt ) , bone strength is impaired ; and a substantial risk of secondary bif exists . 
accordingly , based on simple biomechanical consideration , interventional or surgical consolidation is mandatory to avoid a secondary bif , which usually occurs within the first few weeks even though cases of delayed bif have been reported [ 61 ]  . 
consolidation should ideally be performed during the same interventional session , or at the latest during the same hospital stay . followup afterinterventional treatments in the majority of cases , the main goal of percutaneous treatment is pain management [ 8 , 62 ]  . 
for this reason , many authors evaluate procedural success on the basis of clinical data by applying pain scales ( e.g. , vas scale , brief pain inventory ) or quality of life scores ( e.g. , mcgill quality of life questionnaire ) [ 39 , 40 , 6365 ]  . 
additionally , some authors also evaluate the consumption of analgesics including opioids [ 40 , 66 ] that are nevertheless limited by side effects such as constipation , sedation , and nausea . 
 clinical data are collected at least 1week after treatment ( to reduce the placebo effects or other confounding factors , such as the effects of analgesics administered during the procedure or pain related to the procedure itself ) , and thereafter , follow - up is scheduled at 1 , 3 and 6months according to the patients status and disease evolution . unless new symptoms occur , imaging follow - up is unnecessary in patients with diffuse metastatic disease who underwent palliative treatments [ 39 , 67 ]  . 
on other hand , oligometastatic patients treated with a curative intent should undergo periodic imaging follow - up to assess local tumor control ( i.e. , identification of residual viable or recurring tumor in the treated area )  . 
to avoid confounding variables , such as inflammation , the first followup study should be carried out 4 or even 812weeks after the treatment [ 40 , 59 , 70 ]  . 
finally , it is important to notice that recist criteria cannot be used in the setting of bm as recist has only been used for soft tissue metastases ; moreover , bm is often considered non - measurable [ 68 ]  . possible interactions withother treatments the application of interventional radiology for the management of bm is relatively recent . 
this may explain why no comparative studies are available between interventional treatments and rt , which still remains the widely accepted gold standard for the treatment of sres , particularly pain [ 71 ]  . 
in the few studies describing the combined use of rt and percutaneous treatments [ 63 , 66 , 72 ] , authors emphasized the achievement of better results in terms of pain relief when the combined approach was applied as compared to a single treatment modality , without significant increase in morbidity . 
the exact mechanisms through which the combined treatment relieves pain remain largely unknown , although it has been advocated that tumor microenvironment perturbation resulting from ablation may enhance the effect of rt [ 73 ]  . the development of immunotherapy has resulted in new and revolutionary advances . 
it has been postulated that this phenomenon is immune mediated and is mainly observed in patients undergoing rt 1 3 la radiologia medica ( 2019 ) 124 : 3449 fig . 
indeed , focal treatments such as rt may trigger and potentiate the effects of immunotherapeutic agents ; and it has been postulated that similar to rt , thermal ablation can also stimulate a systemic immune - mediated antitumor response [ 7578 ]  . medical therapy for bm disease relies on agents ( bisphosphonates or denosumab ) avoiding bone loss [ 3 , 7 ]  . 
to our knowledge , no side effects have been described in patients receiving such agents and interventional treatments . surgery can be the definitive solution in oligometastatic patients with slowly evolving disease and long life expectancy . 
however , there are different limitations to its use since surgical interventions carry a significant risk of infection and bleeding coupled to a long recovery time [ 67 , 71 ] ; as a result of which , a long delay to systemic therapies is expected . 
due to the complex clinical scenario regarding bm , we suggest that the most adapted therapeutic strategy should be chosen in consensus by a dedicated multidisciplinary tumor board including medical oncologists , radiation oncologists , surgeons and interventional radiologists . 
interventional treatments have several different advantages including the synergic effect with all the other non - interventional treatments , no need for significant interruption of systemic therapies , reduced morbidity and in - hospital stay , and patients fast recovery . 
due to technical and anatomic specifications , interventional treatments should be performed by trained interventional radiologists ( or by young interventional radiologists under the supervision of a senior )  . 
interventional procedures on bm are usually painful , and the interventional radiologist performing the procedure may not be able to provide alone the best intraoperative anesthesia and postoperative analgesia ; as a consequence , dedicated anesthesiology teams should be involved . 
 evaluated parameters were gender and age of the patients , size , side , homogeneity , morphology , radiodensity , mineralization , borders , relation to roots , affected tooth or teeth and location of the analyzed lesions . results of the 6340 assessed patients , 354 ( 5.6% ) harbored 362 lesions . 
radiopaque image , radicular location , round shape , homogeneous core and well - defined boundaries were the more frequent io features . conclusions our method allows to analyze io lesions with precise parameters . 
analysis of the results does not support the previously suggested theories to explain their origin , and these figures suggest that the so - called ios are developmental alterations of the bone . keywords idiopathic osteosclerosis bone lesions radiopaque osseous lesions developmental bone alterations introduction intrabony radiopaque lesions are common manifestations of neoplasia , sequelae of carious lesions , traumatic event , malignant tumors , metastasis , neoplastic and non - neoplastic entities or developmental alterations . 
many different names have been proposed for them : osteosclerosis , condensing osteitis , bone eburnation , bone scar , osteopetrotic scar , osteopetrosis , enostosis , sclerotic bone , socket sclerosis , bone whorl and dense bone island [ 124 ]  . 
other names were : focal sclerosing osteomyelitis , focal periapical osteopetrosis , focal osteosclerosis and idiopathic osteosclerosis * constantino ledesma - montes cledezma@unam.mx 1 clinical oral pathology laboratory , divisin de estudios de posgrado e investigacin , facultad de odontologa , universidad nacional autnoma de mxico , 04510mexico , d.f. , mexico 2 laboratory ofimmunology , divisin de estudios de posgrado e investigacin , facultad de odontologa , universidad nacional autnoma de mxico , 04510mexico , d.f. , mexico ( io )  . 
these synonyms were used for many years by researchers in different studies , and differences in interpretation , terminology , methodology , image features , analyzed populations and frequencies produced confusion in the literature [ 119 , 2124 ]  . in recent years , several studies on radiopaque lesions of the maxillofacial regions separated two distinct entities of different origin [ 1 , 2 , 59 , 13 , 15 , 18 , 21 , 22 ]  . 
the first is condensing osteitis , and it arises from an inflammatory process as sequelae of caries , pulpal necrosis , deep or large restorations or associated with teeth serving as abutments for fixed bridges or partial dentures . 
 a panoramic radiograph was made to all of them , and all radiographs were reviewed and discussed by two panelists ( cl - m and jchg ) , solving discrepancies by consensus and agreement . 
for stringent selection , we added parameters to those previously proposed [ 7 , 9 , 15 , 19 , 23 , 24 ] and excluded lesions presented with the following features : 1 . 
lesions associated with periodontal disease zones . in this study , we included those painless , radiopaque or mixed ( radiolucentradiopaque ) lesions , located in the tooth - bearing areas associated with vital , non - carious teeth or tooth . 
sometimes , teeth contained small restorations , and frequently , the lesions were seen separated from the root and they were not associated with inflammatory , infectious or traumatic episodes . la radiologia medica ( 2019 ) 124 : 2733 fig . 
the maxillary portion was superiorly limited by the floor of the maxillary sinus and floor of the nasal cavity ; the mandibular area was limited by the upper portion of the mandibular canal and a straight line connecting both mental foramina . 
these zones were limited by the left and right distal portions of the third molars . relation to roots and bone : for classification purposes , a modification of the geist and katz study ( 9 ) was used . 
the observed io decrease in frequency in older age groups was noticed in this study and other studies [ 1 , 2 , 4 , 5 , 8 , 9 , 11 , 24 ] , suggesting that this phenomenon may be related to the loss of bone in mature and old people . 
 as it was in other studies [ 1 , 2 , 4 , 5 , 8 , 9 , 11 , 24 ] , these findings strongly suggest that io lesions are developmental alterations or anatomic variants of the bone . in this study and previously reported studies , io lesions were more commonly found in the mandible than in the maxilla [ 113 , 1519 , 2124 ]  . 
relation to bone and roots varied widely from lesions entirely surrounded by bone , lesions in contact with the lamina dura or periodontal ligament and others entirely obscuring or covering part of the root . to date , origin of io lesions is a matter of debate . 
analyzing this theory , the resulting lesions are associated with dental trauma or more commonly to a long standing carious process and they fall in the condensing osteitis group of lesions . 
interestingly , there are reports on the microscopic features of histologically processed cases showing the presence of bone tissue and no traces of roots [ 9 , 10 ]  . 
additionally , data on the more common occurrence of io cases in the molar areas and the higher frequency of lesions without inflammatory , traumatic or other stimulatory effects do not support this proposal . 
our findings on location of the analyzed lesions suggest that ios surrounded by bone could arise from cells of osteoblastic lineage and those in contact with periodontal ligament could derive from both osteoblastic cells and noncommissioned periodontal cells . several authors suggested that ios are developmental alterations of the bone [ 1 , 4 , 5 , 8 , 9 , 11 , 12 , 24 ]  . 
the clinical care classification system [ 20 ] defines a developmental alteration as the change in or modification of age - specific normal growth standards and or developmental skills , and commonly , frequency of developmental alterations is different between the studied populations . 
in this study , we found that ios was detected in 5.6% of our patients , and in other reports [ 119 , 2124 ] io frequency varied widely in each of the studied communities . 
also , in this study , ios were common during the 2nd to 4th decades declining in older patients , their frequency also rose from 1st to 3rd decades and then decreased , and additionally , size increased in patients aged between 7 and 30years and then decreased . 
the higher io frequency in the young group compared with frequency in the old patient group , the increasing size of the radiopacities in patients up to 30years and its decrease in older patients support the possibility that io 1 3 32 la radiologia medica ( 2019 ) 124 : 2733 lesions develop and grow at early ages mainly . 
additionally , the sudden increase in io frequency from 0.8% in children to 24.3% in the 3rd decade supports this assertion , suggesting that io is more frequent during development and maturation ages . our study analyzed many io imagenologic features are poorly studied in the past . 
previous reports considered that round or oval shape is the form for io , and this study showed that a high percentage ( 20.2% ) of the studied lesions were of irregular , squared , elongated or triangular shapes . 
we found that most of them were well - defined lesions , but 21% showed ill - defined boundaries . technically , there are three entities characterized by osteosclerosis in the maxillofacial area . 
we consider that io lesions could be defined as asymptomatic , non - expansile , osteosclerotic , radiopaque sometimes mixed ( radiolucentradiopaque ) lesions , developing in the tooth - bearing area , that appear at any age , in both women and men , lacking any relationship with inflammatory , infectious or traumatic phenomena . 
io lesions should not be diagnosed when these radiopaque lesions are located in places with previous tooth extraction or surgical procedures , and they are lesions that cannot be diagnosed as any other known osteosclerotic entity . 
the second entity comprises a set of osteosclerotic lesions radiographically similar to those analyzed here , but they are observed outside the area considered in the study and they never were located in the tooth - bearing area . 
the third entity is known as condensing osteitis . in the past , it was proposed that cases resembling this lesion were related to traumatic occlusion [ 6 , 9 , 16 , 18 ]  . 
 during the study , we found few cases of radiopaque areas close to the tip of the root , associated with radicular resorption , and they were diagnosed as condensing osteitis and excluded from the study . 
these osteosclerotic lesions associated with excessive occlusal forces and root resorption do not fulfill the parameters mentioned here and should be considered examples of condensing osteitis . conclusions ios are not associated with inflammatory , traumatic or infectious stimulus . 
 the aim of this study is to investigate the causes and incidence of violence against radiographers in radiology departments of educational centers and hospitals . materials and methods in this descriptive - analytic study , violence incidence was investigated in all 121 radiographers working in radiology departments of educational centers of kermanshah in 2016 . 
data analysis was also performed using descriptive statistics and t test and chi - square tests by stata 11 software . results the results showed that 72.7% of radiographers had experienced violence in their work environment . 
the verbal violence against radiographers younger than 40 was significantly higher ( p = 0.04 ) than the age group above 40years . conclusion the incidence of verbal violence against radiographers in radiology departments is high which can be reduced by providing adequate human resource and equipment in radiology departments , re - training courses on the prevention and management of violent behavior and the suing the violent events against radiologists . keywords physical violence verbal violence radiologists of radiology department introduction any violent act whether physical or verbal against people at their workplace can be defined as violence in workplace [ 1 ]  . 
however , these acts can be also from other * sogand abbasi azizi kahkeshan1994@gmail.com 1 department ofradiology andnuclear medicine , school ofparamedicine , kermanshah university ofmedical sciences , kermanshah , iran 2 student research committee , kermanshah university ofmedical sciences , kermanshah , iran personnel in the medical staff [ 2 ]  . 
recent reports on violence in treatment departments showed that about 25% of violent incidences have occurred in this area and more than half of care centers staffs have the experience of at least one time of physical or verbal violence throughout their professional life . 
as a group of high - risk jobs , the probability of violent experience is 16 times higher for a care - health employee as compared with other services [ 5 ]  . 
occurrence of workplace violence can lead to anger , fear , frustration , humiliation , anxiety , stress , sense of disability , isolation or sometimes vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 1418 feeling of guilt or tendency to retaliate , change behavior or change of workplace [ 2 ]  . 
on a large group of italian radiologists to investigate the incidence of violent behavior , they found that despite the fact that violence against radiologists is relatively unknown , the phenomenon is significant ; and 20% of radiologists are victims of physical and verbal violence [ 2 ]  . 
a study in hong kong showed that 61% of radiographers experienced violence during past 3years , and 34% had more than 5 violent incidents , with verbal violence ( 97% ) mostly by the patients as the most common type . 
in the healthcare area , lack of policy on organizational reporting of perceived violence , lack of employees belief in the usefulness of reporting and their concern that violence and insults may be considered as evidence of their poor performance or ignorance are the most important barriers in reporting violence at work [ 11 ]  . 
considering the increasing prevalence of occupational violence in developing countries and the high rates of violence against the medical staff and its serious complications , it is necessary to carry out further studies in this field to find the ways to reduce the frequency of these incidents and their consequences . 
this information helps international organizations to propose specific legal systems for addressing and resolving violence at the workplace [ 1517 ]  . radiographers are often exposed to various forms of violence due to their direct communication with patients and their relatives and faced with many professional tensions , especially during radiography of emergency patients . 
since there has not been a study on the experiences of radiographers about occupational violence in iran , the purpose of this study is to investigate the incidence of verbal and physical violence from the patients and their relatives to the radiographers of educational centers of kermanshah university of medical science . materials andmethods the target community of this descriptive - analytical study includes all 121 radiographers of the radiology department of kermanshah university of medical sciences , kermanshah , iran , in 2017 , who had more than 1year of experience and were volunteers to participate in the study . 
the first part included the demographic data of radiographers such as age , sex , work experience , employment status and work shithe second part of the questionnaire included questions that assessed violence in terms of type , and cause of violence , as well as the response of radiographers to violence . 
the research staff referred to the radiology centers in different work shifts and explained the objectives of the study ; they distributed the anonymous questionnaire among the volunteer radiographers and then collected the completed ones . 
at the end , the collected data were analyzed by stata 11 software using descriptive statistics and inferential tests including chi - square with a significant level of p < 0.05. results in this study , all the 121 radiographers working in educational hospitals affiliated to kermanshah university of medical sciences completed the questionnaires . 
seventy - seven ( 63.6% ) of the radiographers were women and 52 of them ( 42.9% ) had below 5 - year work experience record ; and 49 radiographers ( 49.5% ) were officially registered ( table 1 )  . 
also , the findings indicated that the highest rate of violence was from accompaniments ( 73 , 64.4% ) with middle - aged age group ( 45 , 40.9% ) ( table2 )  . 
the distribution of violators in terms of age group showed that most of the violence actors were in the middle - age group . considering that each radiographers was allowed to choose several causes for physical and verbal violence , the results showed that overcrowding of patients in radiology department with the highest frequency ( 21.0% ) was the most important cause of violence against radiographers . 
the lack of available security facilities ( 12.6% ) and inadequate number of radiology personnel ( 11.7% ) are the other reasons for the emergence of violence ( table3 )  . 
similarly , considering that every radiographers was allowed to choose several options to respond to the violence , the most important table 1 frequency if violence against radiology department radiographers based on their demographic data variable group frequency number ( % ) verbal violence number ( % ) physical violence number ( % ) total number ( % ) test results experience employment status age group women > 40 510 1120 > 20 contractual contract resident official young middle - aged adults 77 ( 63.6 ) 22 ( 36.4 ) 89 ( 73.5 ) 32 ( 26.5 ) 52 ( 42.9 ) 15 ( 12.4 ) 34 ( 28.1 ) 20 ( 16.6 ) 7 ( 5.8 ) 18 ( 14.9 ) 47 ( 38.8 ) 49 ( 40.5 ) 17 ( 14 ) 48 . 
jiao and colleagues also reported that according to their study on occupational violence against nurses , 7.8% of nurses experienced physical violence and 24% had faced with verbal violence [ 17 ]  . 
it seems that educating radiographers to improve their communication skills and anger management the principles can reduce the prevalence of violence . the results of the present study showed that the verbal violence was higher toward radiographers younger than 40 . 
it seems that due to the lack of communication skills and the management of occupational violence during university studies , only the professional experience and social interactions of radiographers in the age group over 40years can lead to a significant reduction in the incidence of occupational violence against them . the results of present study showed that the most number of violence against radiographs was from the patient accompaniment . 
also , magnavita study found that patients were mostly committing violent events against radiographers ( 37.1% ) and their accompaniments and relatives ( 34.3% ) were in the next rank [ 2 ]  . 
the difference in the results seems to be due to cultural differences . the results of this study indicated that overcrowding of patients in radiology departments ( 33% ) , lack of available security facilities and shortage of personnel are the most important causes of violence against radiographers . 
showed that the long waiting for radiotherapy services , communication problems and dissatisfaction with the provided services by radiographers are the most important causes of violence [ 9 ]  . 
regarding the increasing number of patients in radiology centers , it seems that providing adequate equipment and human resources can reduce patients congestion and improve the level of patients satisfaction with the quality of radiology services . in the present study , the reaction of radiologists to the violence against them was first inviting the invader to calm down ( 21% ) ; then they asked for help from their colleagues ( 15% )  . 
since the degree of violence , the level of personnel experience , staff working hours and other influential factors can be effective in this response , the reaction of the photographers and other medical staff can be different . given the high rate of violence , more diagnostic errors are likely to occur . 
studies conducted in hong kong [ 9 ] , uk [ 19 ] , and egypt [ 20 , 21 ] show that increased violence reduces work performance and increases the number of diagnostic errors by radiologists and radiographers . 
it seems that annual education is effective in this regard and it is suggested that educational content should include evaluation and reduction of the underlying conditions of violence , violent behavior management , identification of security risks , reporting of violence and its documentation , methods of acquisition assistance insituations of violence , behavioral control , use of security equipment , etc . 
it is also necessary to address these trainings at universities and at radiologist and radiographer training units [ 1923 ]  . conclusion results of this study showed high prevalence of workplace violence against radiology department personnel in centers affiliated by kermanshah university of medical science . 
 1 3 18 la radiologia medica ( 2019 ) 124 : 1418 therefore , equipping the hospitals with adequate radiography facilities and human resources , implementing educational programs for the security staffs to enable them , holding educational courses about preventing and management of violence against radiographers as well as definite legal systems to sue the violence cases , paying serious attention to violence against the personnel and establishment of responsible centers to track the case reports of violence are necessary . compliance with ethical standards conflict of interest mohammad - rasoul tohidnia declares that he has no conflicts of interest . 
no limb amputation was witnessed . conclusions according to our experience , endovascular approach appeared as an effective treatment for popliteal artery aneurysms , as it appeared affected by a low rate of periand post - procedural complications . 
it could be proposed as treatment of choice in patients with high surgical risk . keywords popliteal artery aneurysm endovascular treatment stent graft introduction popliteal artery aneurysms ( paa ) are the most frequent peripheral aneurysms ; they could be associated with other large vessel aneurysms ; and they could be unilateral or bilateral [ 1 ]  . 
most of the time , these types of aneurysm are asymptomatic and are diagnosed by screening examinations because they present as a pulsatile mass of the popliteal fossa [ 2 ]  . 
if symptoms are present , they could vary between different degrees of ischemic symptoms of lower extremities [ 3 ] , such as claudication , distal ischemia due to embolization , or * giuseppe guzzardi guz@libero.it 1 scdu radiologia diagnostica ed interventistica , azienda ospedaliero - universitaria maggiore della carit , novara , italy 2 sc radiologia diagnostica ed interventistica , ospedale regionale u . 
di radiologia , azienda ospedaliera mater domini , catanzaro , italy 4 sc chirurgia vascolare , azienda ospedaliero - universitaria maggiore della carit , novara , italy acute limb ischemia due to aneurysm thrombosis [ 4 ] ; less frequently , they could lead to neurovascular compression [ 5 ] or they could rupture and lead to hemorrhage , usually confined in the popliteal fossa [ 6 ]  . to assess whether these aneurysms should be treated , if asymptomatic , diameter of the lesion is the most important characteristic that should be taken into consideration ; aneurysms 2cm are considered candidates for treatment [ 7 ]  . 
 symptomatic aneurysms should be treated regardless of their dimensions . until recently , surgery was considered as treatment of choice of this pathology , especially for large and symptomatic lesions , and it is performed with aneurysmectomy followed by surgical bypass . 
in the last 7years , we retrospectively analyzed 48 patients treated for paa , who were affected by severe systemic comorbidities and were therefore excluded from surgical repair . we divided patients in groups based on the length ( cut off : 70mm ) and diameter of the lesion ( cutoff : 25mm ) , on the number of runoff vessels ( 1 , 2 , or 3 ) , and on the patient symptoms ( symptomatic or asymptomatic ) to obtain homogeneous groups and to compare outcomes with anatomical and clinical feature of the aneurysm . symptomatic patients were defined as those with peripheral embolism , complete acute thrombosis , venous compression , or claudication due to the paa . 
inclusion criteria were technical feasibility ( proximal and distal landing zone of at least 2cm , no limits in length lesion ) and patency of at least one tibial vessel . exclusion criteria were age < 60 years old ; severe comorbidities ( asa > 3 ) ; contraindication to antiplatelet , anticoagulant , or thrombolytic therapy [ 10 , 11 ]  . 
patients younger than 60years old and in good clinical conditions were considered for open repair . pre - procedural planning was performed with angio - ct study in all patients ( lightspeedplus , ge , milwaukee , usa , and aquilion 64 , toshiba , tokyo , japan ) , and ct acquisition parameters were section thickness 0.625mm ; pitch 1 : 0.984 ; rotation time 0.7s ; kv 100 ; ma in between 250 and 600 depending on patient constitution . 
we injected 100ml of iodinated contrast medium ( iomeron , bracco , milano , it , 400mg / ml ) at a rate of 45ml / s , followed by a 30 - ml chaser bolus of saline solution at the same speed . post - processing mpr ( multiplanar reconstruction ) and mip ( maximum intensity projection ) were performed to assess morphological characteristics of the vessel and to choose the correct device to implant evaluating best vascular access . all procedures were performed in angiographic room , using a monoplane angiograph ( integris allura xper fd20 philips , eindhoven , the netherlands , and innova , ge , milwaukee , usa ) with local anesthesia . endovascular procedures were performed by three different operators , all having 15years of experience in angiographic procedures . la radiologia medica ( 2019 ) 124 : 7985 vascular access was performed by percutaneous anterograde common femoral artery puncture to avoid crossing the aortic carrefour ( often tortuous and calcific ) with wide and stiff devices ( from 8 to 11 french ) ; after the diagnostical angiography the aneurysm was crossed with a guidewire ( hydrophilic guidewire 0.035 , radiofocus , glidewire , terumo , tokyo , japan ) and a catheter ( 5f , cordis , miami , usa )  . 
all patients , in our case series , were treated with the same kind of endoprosthesis gore viabahn ( gore , flagstaff , az , usa ) which is characterized by a good elasticity and flexibility , allowing the positioning of these devices even in the intraarticular segment of the vessel . after graft positioning , we performed angioplasty with semi - compliant balloon at the proximal and distal end of the endoprosthesis to allow a better sealing of the aneurysmatic lesion . angiographic controls were performed after deployment and angioplasty of the stent graft both in leg extension and in knee flection to assess whether knee movements were causing graft compression , displacement , or rupture . during the procedure , we administered intravenously a weight - adjusted bolus of heparafter the procedure , all patients were treated with antiplatelet therapy with acetylsalicylic acid 100mg and clopidogrel 75mg for 1month and single antiplatelet therapy afterward . follow - up was performed with the clinical examination followed by duplex scan and / or cta at 1 , 3 , 6months after treatment and then yearly . we evaluated technical success defined as correct deployment of the graft with complete exclusion of the aneurys primary outcome of our study was the evidence of primary or secondary patency of the stent graft at follow - up ( secondary patency was defined as restored patency through the originally treated segment )  . 
we evaluated as secondary outcomes the incidence of infections of the graft and development of type i endoleak due to extension of the disease and / or migration of the stent graft that required a second intervention . evaluation of procedural costs was not performed , considering that main endpoints were clinical and the most literature regarding this subject takes into consideration mainly peripheral obstructive disease rather than peripheral aneurysmatic disease [ 12 ]  . statistical analysis data were collected and analyzed using spss 15.0 software ( spss inc , chicago , ill )  . 
patency was evaluated 1 3 la radiologia medica ( 2019 ) 124 : 7985 using kaplanmeier curves and log - rank tests with the related standard error ( se )  . table 2 procedural details results we treated 48 aneurysms , deploying a total of 79 endoprosthesis . 
mean aneurysm length was 76.3mm ( range 22200mm ) , and 24 / 48 ( 50% ) patients had an aneurysm whose length was > 70mm ; mean diameter of the lesion was 34.4mm ( range 2160mm ) , and in 27 / 48 ( 56% ) of cases the aneurysm was > 25mm of diameter . thirty - one patients ( 64.6% ) were asymptomatic , and the diagnosis was incidental during duplex scan or ct imaging performed for other reasons , while 17 ( 35.4% ) had symptoms at diagnosis ; in eight cases patients presented with mild claudication , seven had distal limb ischemia with rest pain , due to peripheral embolism from the aneurysm , and two presented symptoms due to neurovascular compression from the aneurysm . patients selected had at least one runoff vessel . 
more specifically , most of the enrolled patients had two runoff vessels ( 21 / 48 , 44% ) , seventeen ( 35% ) had three runoff vessels , while ten ( 21% ) had only one runoff vessel . all patients selected in our study were treated electively with percutaneous access and local anesthesia ( table2 )  . 
at 30 - day follow - up , we registered a total of five endograft thromboses that were treated with intra - arterial thrombolysis with complete recanalization of the prosthesis in three patients ; two patients also required angioplasty after locoregional fibrinolysis , to achieve a good stent graft patency . out of these patients , three had no other relapses and the endoprosthesis was still patent at long - term follow - up , while in two cases occurred a second graft thrombosis that required to perform a surgical bypass ( table3 )  . 
three patients presented a progression of the disease and required a reintervention to extend the coverage of the graft ; only one patient presented infection of the endoprosthesis 5months after the procedure and was treated by removing the stent and with surgical bypass . 
in our case series , we did not witness any case of type ii endoleak at shortand at long - term follow - up . in our study group , primary stent graft patency was 34 / 48 ( 70.8% ) while secondary patency was 43 / 48 ( 89.6% ) ; no limb amputation was reported . we did not find any statistically significant difference in long - term patency rate between patients with long and short lesions ( 70mm or > 70mm ) , with small or large 1 3 82 la radiologia medica ( 2019 ) 124 : 7985 fig . 
3 primary and secondary patency related to lesion length ( blue : 25mm , green : > 25mm ) [ 2 ] , it is associated with a high rate of limb amputation due to a decreased distal perfusion [ 3 ]  . studies have shown how surgical bypass patency is highly influenced by the clinical conditions of the patients . 
patients treated in elective settings showed a long - term patency of 80% while patients treated due to severe symptoms in emergency settings showed a long - term patency of only 60% [ 13 ]  . endovascular techniques for the treatment of aneurysms have developed significantly in the recent years , granting a good outcome in a high percentage of patients for both aortic and distal arteries aneurysms [ 14 , 15 ] ; therefore , endovascular treatment has been chosen in a higher percentage of patients showing suitable anatomical conditions . our exclusion criteria according to patient age were inspired by the literature [ 10 , 11 ] ; both antonello etal . 
we stretched that limit to 60years old , for selected patients , to allow surgical repair in a wider 1 3 84 la radiologia medica ( 2019 ) 124 : 7985 fig . 
4 primary and secondary patency related to number of runoff vessels ( blue : one vessel , green : two vessels , gray : three vessels ) range of patients , reserving endovascular repair to older and high - risk ones ( asa > 3 )  . main challenge of endovascular treatment of aneurysms of the popliteal artery is represented by the fact that this anatomical district is highly mobile and flexible ; therefore , devices implanted must be able to sustain a high compressive force during limb flexion , to grant a valid distal perfusion and avoid stent thrombosis [ 17 , 18 ]  . endovascular treatment of popliteal aneurysms has been performed with different techniques such as multilayer and covered stents . 
few cases of multilayer stents treatment of aneurysms have been reported in the literature [ 16 ] , which showed a variable rate of aneurysms occlusion in association with a moderate percentage of stent thrombosis ; therefore , their use has decreased over the last years . 
 [ 21 ] reported a large case series confronting open surgical repair with endovascular repair in patients with popliteal aneurysms comparing a total of 178 patients treated with surgical technique and 134 with endovascular approach ; patients of the surgical group were more frequently symptomatic , with distal limb ischemia and a decreased runoff score . 
further studies will be needed to correctly evaluate whether patients and aneurysms characteristics could predict the efficacy of the treatment , and this will require a larger number of treated cases and longer follow - up and would allow a better patient selection . compliance with ethical standards conflict of interest on behalf of all authors , the corresponding author states that there is no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 5864 radiotherapy inoperable earlystage primary andearly recurrent nonsmall cell lung cancer : outcomes ofamonoinstitutional experience using amoderate hypofractionated schedule mauriziovaleriani1 mattiafalchettoosti1 lucamarinelli1 chiarareverberi1 vitalianadesanctis1 davidemollo1 lucanicosia1 received : 26 june 2018 / accepted : 20 august 2018 / published online : 3 september 2018 italian society of medical radiology 2018 abstract background patients with medically inoperable early - stage non - small cell lung cancer ( nsclc ) may beneficiate of a hypofractionated radiation therapy in order to intensificate the treatment and to reduce the number of hospital access . methods from 2007 to 2015 , 27 patients with early - stage primary or limited loco - regional recurrent ( t2a > 4cm , t2b n0 or t12 n1m0 ) nsclc were treated . 
survival outcomes were statistically favourable in patients with partial or complete response with respect to patients with stable or progressive disease , whereas stage ( n0 vs n1 ) and primary or relapse / recurrent disease not . 
standard treatment for early - stage non - small cell lung cancer ( nsclc ) is surgical resection [ 3 ] with a 5 - year overall survival ( os ) ranging between 55 and 72% in stage i disease and between 29 and 51% [ 4 ] in stage ii disease . 
t1t2a n0 patients can be treated with stereotactic radiotherapy [ 57 ] , but in t2b n0 or t12 n1 patients , stereotactic radiotherapy may be infeasible for the volume and / or for the site of the disease . 
several studies have evaluated the vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 5864 role of moderate hypofractionation [ 12 , 13 ] in order to intensify the treatment and limiting tumour repopulation [ 14 , 15 ] by reducing the total treatment time . 
based on these factors in 2007 , we started to treat early - stage primary or limited recurrent nsclc patients with a moderate hypofractionated schedule . methods andmaterials patients twenty - seven patients with early - stage primary or limited loco - regional recurrent ( t2a > 4cm , t2b n0 or t12 n1m0 ) nsclc were treated in our institution from 2007 to 2015 . 
free breathing basal ct images were matched with the maximum intensity projection ( mip ) series , with diagnostic ct and with pet - tc using automatic matching systethe gross tumour volume 1 ( gtv1 ) included the pulmonary lesion ; gtv2 included lymph nodes with a short axis diameter 1 cm and / or positive nodes at pet - tc . 
all patients were treated with 3d - crt using multiple coplanar and non - coplanar fields and received 60gy in 20 fractions of 3gy , 5 times per week delivered by a linear accelerator ( 6 - mv photon beams )  . 
time - adjusted biological effective dose ( bed ) was calculated using the following formula : bed = nd ( 1 + d / [ a / b ] ) ln2 ( t tk ) [ 16 ] , where nd is the total dose , d the dose per fraction , t the overall treatment time expressed in days , and tk the proliferation start time ( 28days )  . 
a total body contrast - enhanced ct was performed at 1month after rt completion and every 6months afterwards , a pet - tc was performed at 3months after rt and in case of suspected 1 3 60 la radiologia medica ( 2019 ) 124 : 5864 fig . 
response rates were determined using response evaluation criteria in solid tumours ( recist version 1.1 ) [ 19 ]  . statistical analysis was performed using spss , version 24.0 , software ( spss , inc , chicago , il )  . 
progression - free survival ( pfs ) was defined as the time to local / systemic progression or death and loco - regional pfs ( lr - pfs ) as the time to infield or outfield local and regional recurrence / progression . 
twelve patients achieved a complete response ( cr ) ( 44.4% ) and 8 a partial response ( pr ) ( 29.6% ) with a tumour response rate of 74% . 
also pfs and mfs were statistically better in patients with partial or complete response ( median pfs 47months , median mfs 62months ) with respect to patients with stable or progressive disease ( median pfs 3months , median mfs 10months ) with 1 3 la radiologia medica ( 2019 ) 124 : 5864 css , lr - pfs , pfs and mfs . 
thus , 13 patients ( 48.1% ) presented metastasis : 4 in controlateral lung , 2 distant nodes , 3 bone , 2 brain , 1 brain plus bone and 1 adreanal . stage ( n0 vs n1 ) and primary or relapse / recurrent diseases were not statistically significant in terms of os , patients with primary or recurrent early - stage nsclc may be managed with surgery , but for medically inoperable cases or patients who refused surgery , radiotherapy may be a valid option . stereotactic radiotherapy represents the standard treatment for low - volume n0 lesions . 
in patients not suitable to stereotactic approach for high - volume n0 or n1 disease , an intensified treatment may be evaluated in order to ameliorate results of standard dose and fractionation radiation therapy . 
in our case 60gy in 4weeks presented a bed10 [ 16 ] of 79.4gy , whereas , for example , 70gy in 35 fractions over 7weeks has a bed10 normalized with time factor of 70.9gy. therefore , frequently early - stage nsclc patients were referred for radiotherapy in presence of comorbidity , which may affect survival [ 20 , 21 ] , or for old age . 
in our cohort median age was 76years and there were some cases ( 5 / 27 patients ) that died of causes not related to the disease , but after a median of 42months . 
patients with complete or partial response presented a statistically significant better os , css , lr - pfs , pfs and mfs with respect to patients with stable or progressive disease . 
table3 summarizes the most important studies on moderate hypofractionation in nsclc . these results showed that moderate hypofractionation is well tolerated with a very low rate of high - grade toxicity . 
moreover , the results , in terms of survival , obtained in our study are promising and compared favourably with the results of the other studies despite that in some of these were enrolled patients with t1 or t2a n0 disease that currently were treated with stereotactic radiotherapy [ 57 ]  . 
a greater number of patients and a longer follow - up are necessary to confirm the results obtained with our treatment . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 6578 radiotherapy late toxicity ofimageguided hypofractionated radiotherapy forprostate : nonrandomized comparison withconventional fractionation barbaraalicjajereczekfossa1 , 2 alessiasurgo2 mariannaalessandragerardi2 dariozerini2 giuliamarvaso2 deliaciardo2 stefaniavolpe1 , 2 damarispatriciarojas1 , 2 giuliariva1 , 2 ombrettaalessandro1 , 2 samanthadicuonzo2 giuseppefanetti1 , 2 paolaromanelli2 annastarzyska4 federicacattani5 raffaellacambria5 cristianafodor2 cristinagaribaldi5 chiararoman5 , 6 ottaviodecobelli1 , 7 robertoorecchia8 patrickmaisonneuve3 andreamaucieri2 received : 6 march 2018 / accepted : 28 august 2018 / published online : 15 september 2018 italian society of medical radiology 2018 abstract purpose to evaluate the incidence and predictors for late toxicity and tumor outcome after hypofractionated radiotherapy using three different image - guided radiotherapy ( igrt ) systems ( hypo - igrt ) compared with conventional fractionation without image guidance ( non - igrt )  . methods and materials we compared the late rectal and urinary toxicity and outcome in 179 prostate cancer patients treated with hypo - igrt ( 70.2gy / 26 fractions ) and 174 non - igrt patients ( 80gy / 40 fractions )  . 
5and 8 - year recurrence - free survival ( rfs ) and overall survival ( os ) were analyzed . results mean follow - up was 81months for hypo - igrt and 90months for non - igrt group . 
mainly mild late toxicity was observed : hypo - igrt group experienced 65 rectal ( 30.9% g1 / g2 ; 6.3% g3 / g4 ) and 105 urinary events ( 56% g1 / g2 ; 4% g3 / g4 )  . 
multivariate analysis showed that hypo - igrt is a predictor for late genitourinary toxicity , whereas hypo - igrt , acute urinary toxicity and androgen deprivation therapy are predictors for late rectal toxicity . 
advanced t stage and higher gleason score ( gs ) were correlated with worse rfs . conclusions a small increase in mild late toxicity , but not statistically significant increase in severe late toxicity in the hypoigrt group when compared with conventional non - igrt group was observed . 
prostate cancer radiobiological behavior ( slow proliferation rate with high sensitivity to high dose per fraction ) [ 6 , 7 ] , technological advantages in treatment planning and high precision in dose delivery and accuracy of target definition ( image - guided vol . : ( 0123456789 ) 1 3 66 la radiologia medica ( 2019 ) 124 : 6578 radiotherapy , igrt ) allowed introduction of hypofractionated radiotherapy schedules [ 1 ]  . italy ( eio no 79 )  . 
the inclusion criteria and techniques were described in our previous paper [ 11 ]  . since 2003 , we used in our department 3 - dimensional conformal ( 3d - crt ) 2 - dynamic arc radiotherapy to the dose of 80gy / 40 fractions for prostate cancer treatment [ 5 , 8 ]  . 
 in 2006 , three igrt modalities were installed : ultrasoundbased b - mode acquisition and targeting system ( bat ) , stereo x - ray imaging system ( exactrac ) and cone beam computed tomography ( ct ) ( on board imager ct )  . 
the higher incidence of the acute rectal reaction was not significant in multivariate analysis . in the present report , we analyzed the late toxicity registered in the same two - patient cohorts : this is a follow - up study of the previous publication in the urologic oncology [ 11 ]  . the aim of this report is to evaluate the incidence and predictors for late toxicity of the hypo - igrt and secondarily to analyze tumor outcome data . despite methodological limitations ( non - randomized comparison ) , such analysis might help clinicians in discussing with a patient the treatment choice and possible treatment - related toxicity . 
moreover , it creates a hypothesis for further prospective investigation . assessment ofthetoxicity andtumor outcome data after treatment , a radiation oncologist or urologist clinically evaluated patients every 6months for the first year and once a year for 10years . 
late rectal and urinary toxicities were evaluated in patients with follow - up > 3months according to the radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc ) criteria [ 12 ]  . biochemical failure was defined according to american society for radiation oncology ( astro ) phoenix 2005 ( nadir plus 2ng / ml at call ) [ 13 ]  . 
prostate - specific antigen ( psa ) test was performed every 3months for the first 2years after radiotherapy , every 6months for 5years and annually thereafter . clinical failure included local recurrence , regional recurrence and distant metastases : magnetic resonance imaging ( mri ) , ct , choline c - 11 positron emission tomography / ct scan ( choline pet - ct ) or prostate biopsy was used to study patients with psa increase or clinical suspect . statistical analysis in the same way as our previous study , we evaluated the occurrence of two separate radiotherapy - related toxicities ( rectal and urinary ) within the whole population ( hypoigrt and non - igrt groups ) and in hypo - igrt cohort alone . 
univariate and multivariate cox proportional hazards regression models were used to assess the impact of various patient - , tumorand treatment - related factors on late rectal and urinary toxicity . 
the actuarial cumulative incidence rates of rectal and urinary toxicities and the actuarial rfs and overall survival ( os ) rates were estimated for both groups at 5 and 8years and were calculated using kaplanmeier method . 
shortly , patients treated with hypo - igrt were significantly older , had less advanced disease and received less androgen deprivation therapy ( adt ) or previous transuretheral prostate resection ( turp )  . 
therefore , univariate and multivariate analysis ( tables3 , 4 and 5 ) was built on 349 patients including 175 patients treated with hypo - igrt . a predominance of limited g1 events was observed in both groups ( table2 )  . 
there were few g3 and g4 events in both groups ( no g5 event )  . considering high - grade rectal toxicity , all g3 events ( 11 in hypo - igrt group and 5 in non - igrt group ) were proctopathy or persistent rectal bleeding ( requiring transfusion only in two cases ) resolved with coagulation laser therapy . 
as far as high - grade urinary toxicity is concerned , in hypo - igrt group , six g3 urinary events occurred , namely severe dysuria , nicturia and frequent macroscopic hematuria requiring interruption of anticoagulants and / or cystostopic revision in three cases . 
at the last follow - up , 137 hypo - igrt patients had no evidence of disease ( ned ) and 11 were alive with disease ( awd ) and five patients died for prostate cancer ( dod )  . 
in multivariate analysis , risk of recurrence was higher in patients with t3 disease ( hr = 3.00 ; 95% ci 1.426.38 ; p = 0.004 ) and gs > 6mg / ml ( hr = 2.74 ; 95% ci 1.514.96 ; p = 0.0009 ) , while risk of death was significantly higher among patients who received neoadjuvant plus concomitant adt ( hr = 3.18 ; 95% ci 1.546.59 ; p = 0.002 ) ( table6 )  . discussion our study , including 353 patients ( divided into two cohorts of 179 and 174 patients ) , showed a small increase in the mild late urinary and rectal toxicity among prostate cancer patients treated with hypo - igrt schedule when compared to patients treated with conventionally fractionated radiotherapy without image guidance . 
 the tumor outcome univariate analysis showed a gain in 8 - year rfs in hypo - igrt group ( p = 0.0005 ) , although the os was comparable between the two groups . 
 the challenges for numerous non - igrt patients include the follow - up by the urologists ( radiotherapy toxicity might have been underestimated ) and pre - treatment staging based in many cases on the clinical evaluation only . 
the most recently treated hypo - igrt patients were followed mainly by radiation oncologists , and most probably any late event was registered . several recent clinical studies investigated hypofractionation in prostate cancer [ 1825 ] comparing toxicity and efficacy of the short schedules with the conventional fractionation radiotherapy . 
 in both cases , high precision treatment planning and dose delivery are essential for sparing adjacent normal tissue and to decrease toxicity . in this scenario , our analysis , as well as the current evidence , showed that late urinary and rectal toxicity might be increased in the moderate hypo - igrt group [ 2124 ]  . 
 [ 22 ] in a recent multicentric randomized study similarly observed an increased rectal and urinary toxicity comparing two radiotherapy fractionation schedules : 73.8gy / 41 fractions versus 70gy / 28 fractions . 
albeit the power of the randomized character of the study , they compare 3d / intensity modulated radiotherapy ( imrt ) hypofractionated and 3d / imrt conventional treatment without specification in imaging guidance . 
perhaps the selection of a unique 3d - technique and the advantage of igrt might have influenced the recurrence rate , even though the multivariate analysis connected igrt group with an increased urinary toxicity . 
 [ 20 ] randomized trial revealed no difference in late adverse reactions between hypofractionation and conventional fractionation 3d - treatment , but the authors underlined that the incidence of complications increased with time . 
in our series , the incidence of rectal and urinary events increased 2436months after treatment : the rectal toxicity remained almost constant with no great difference between the two groups , but urinary toxicity , especially in the hypo - igrt group , continues to rise . 
 indeed , the lack of significant correlation between acute and late urinary toxicities observed in our study reflects complex mechanisms involved in urinary tract functioning after radiotherapy . interestingly , use of exactrac igrt system was weakly correlated with higher rectal toxicity in the multivariate analysis . 
 [ 21 ] in a mixed risk prostate cancer population showed that late rectal and urinary toxicity was not considerably different , but they analyzed the important correlation with the urinary toxicity > g2 and compromised baseline dysfunction . 
a sub - analysis of the main severe rectal toxicity demonstrated an increase in g3 or g4 toxicity when patients underwent previous turp or used anticoagulants for cardiac dysfunctions . no difference in os in both groups was found in line with all recent evidences [ 1825 ]  . at the same time as well as imrt , stereotactic body radiotherapy ( sbrt ) for organ - confined or locally advanced prostate cancer is becoming almost standard in our clinical practice . 
the advances in technologies and the improvements in detection and characterization of prostate cancer lesions ( as the multiparametric prostate mri ) have led to increase the use of extreme hypofractionated schedules . 
furthermore , future studies on the dosimetric , clinical and biological aspects ( improvement in planning and dose distribution with use of mri - based planning , prevention of late radiotherapyinduced injury or identification of patients at risk of toxicity ) are warranted in order to improve the therapeutic index of hypofractionation . conclusions a small increase in mild late urinary and rectal toxicity in the hypo - igrt group when compared with conventional non - igrt treatment was observed with no statistically significant difference in the severe late toxicity between the two cohorts . 
no major predictor for late toxicity has been found apart from previous acute rectal toxicity and of borderline significance with the use of exactrac systethe study confirms the hypothesis that igrt allows for safe moderate hypofractionation , offering a shorter overall treatment time , an impact in term of prostate cancer rfs and providing potentially more economic health care . 
although in the last decade anthracycline - based chemotherapy single agent or in combinations has been able to improve clinical benefits , prognosis is still poor and stss represent an important unmet medical need . 
the following attempts to provide a review of literature focusing on the available data concerning novel treatments and future prospective for the management of metastatic stss . keywords soft tissue sarcomas immune - checkpoint inhibitors pembrolizumab eribulin olaratumab targeted therapy introduction soft tissue sarcomas ( stss ) represent a rare and heterogeneous group of solid tumours derived from mesenchymal progenitors and account for 1% of all adult malignancies [ 1 ]  . 
an observational study of the american college of surgeons showed that among a cohort of 4550 patients suffering from sarcomas , 46% originate from thigh , buttock and groin , 13% by * giuseppe badalamenti giuseppe.badalamenti@unipa.it 1 section ofmedical oncology , department ofsurgical , oncological , andoral sciences , university ofpalermo , palermo , italy 2 academic unit ofmedical oncology , institute forcancer treatment andresearch , policlinico hospital san martino , genoa , italy 3 department ofinternal medicine , school ofmedicine , university ofgenoa , genoa , italy upper extremities , 18% torso , 13% retroperitoneum and 9% head and neck [ 2 ]  . as classified by the world health organization ( who ) , the group of stss comprise more than 100 different histologies according to the presumptive tissue in origin [ 3 ]  . 
after the development of distant metastasis the median overall survival ( os ) is 1219months , and almost 20% of patients are still alive at 3years [ 4 ]  . 
for patients with a good performance status and sts histology that is known to have sensitivity to anthracyclines ( liposarcoma , leiomyosarcoma , synovial sarcoma , pleomorphic or undifferentiated sarcoma , malignant nerve sheath tumour , angiosarcoma ) , anthracyclinebased chemotherapy represents the standard of care for first - line setting [ 5 ]  . 
for patients ineligible to anthracycline vol . : ( 0123456789 ) 1 3 260 la radiologia medica ( 2019 ) 124 : 259265 combination due to a poor performance status or extensive comorbidity , pegylated liposomal doxorubicin , gemcitabine alone or in combination and dacarbazine are reasonable options [ 68 ]  . 
 weekly paclitaxel seems to be useful for advanced angiosarcomas [ 9 ] ; synovial sarcomas are sensitive to alkylating agents as ifosfamide [ 10 ] ; sunitinib appears to be active in patients with solitary fibrous tumour and alveolar sarcoma , clear cell sarcoma and extra - skeletal myxoid chondrosarcoma [ 1113 ] ; gemcitabine plus docetaxel regimen is active on uterine leiomyosarcomas [ 14 ]  . 
 pazopanib might be considered for stss other than liposarcomas for patients progressing on first - line chemotherapy ( including anthracyclines ) [ 16 ]  . although these treatments or chemotherapy combinations have been able to improve clinical benefits , prognosis is still poor and stss represent an important unmet medical need . continuous advances in cancer genetics and genomics have contributed to change management paradigms of stss as it occurred for other solid tumours . 
several treatments have been recently developed with the specific aim of targeting different cell pathways and immune - checkpoints that have been recognized to drive tumour progression ( table1 )  . 
 the following attempts to provide a review of literature focusing on the available data concerning novel treatments and future prospective for the management of metastatic stss . methods a literature search using pubmed was carried out with no date restriction up to november 2017 . 
a computerized search of the abstracts reported at asco and esmo library , and the clinical trial database on the website caltr ial.gov was performed to identify relevant unpublished studies and ongoing trials . 
 finally , a crosscheck references from review articles and relevant studies on the same topic were performed to confirm retrieval of all pertinent trials . eligible studies had to fulfil the following criteria : randomized prospective phase iiiii trial assessing new or recently approved treatments for patients with metastatic stss . table 1 main characteristics of clinical trials carried out on metastatic sts patients clinical trial drug histological type study design primary endpoint n . 
no language restriction was applied . olaratumab platelet - derived growth factor ( pdgf ) and pdgf receptor ( pdgfr ) are key regulators of oncogenesis process in many solid tumours , including mesenchymal stem cell differentiation , angiogenesis and tumour growth [ 17 ]  . 
olaratumab alone or in combination with doxorubicin showed antitumor activities in human sarcoma xenograft models [ 20 ]  . basing on these data and rationale , an open - label phase ib / ii trial randomized 133 patients with histologically confirmed stss diagnosis to receive olaratumab 15mg / kg on day 1 and 8 plus doxorubicin 75mg / m2 day 1 three - weekly or doxorubicin alone [ 21 ]  . 
this achievement was consistent across the subgroup analysis including pdgfr status , histological subtypes ( leiomyosarcoma versus nonleiomyosarcoma ) and number of previous treatments ( 0 versus 1 )  . 
infusion - related reaction ( 3% ) was the main cause leading to olaratumab discontinuation , whereas 5% of ejection - fraction decrease was the most common reason of discontinuation in doxorubicin group . 
the most common adverse events in the combination arm include neutropenia , nausea , fatigue , vomiting and mucositis [ 21 ]  . despite clinical trial limitation due to the small sample size and heterogeneity of stss histology , this finding is particularly notable given the little progress in improvement of median os achieved for patients suffering from metastatic stss . 
however , this small benefit was achieved at expense of higher toxicities without any improvement in median os ( hr 0.83 , p = 0.76 ) [ 22 ]  . 
os in whole population and in patients with leiomyosarcoma are the two primary objectives of the study . a phase ib trial ( nct02783599 ) is recruiting potentially 40 patients to receive olaratumab 20mg / m2 alone for day 1 and 8 of the first cycle , then olaratumab 20mg / m2 in combination with doxorubicin 75mg / m2 for the second cycle and then olaratumab 15mg / m2 on the same schedule alongside doxorubicin for the third cycle . 
the primary endpoint was to molecularly characterize the circulating tumour cell preand post - olaratumab , and to analyze pdgfr , pdgfr , and pdgf ligand changes . a phase ib / ii ( nct02659020 ) trial is enrolling patients with metastatic stss to assess safety , activity and efficacy of olaratumab in combination with gemcitabine and docetaxel . 
os is the primary endpoint . an open - label phase i trial ( nct03126591 ) is recruiting patients with metastatic stss who has progressed to standard treatment to receive olaratumab plus pembrolizumab . 
this finding may be partially explained by the occurrence of activating mutation in the gene encoding the pdgfr [ 24 ]  . most gists harbouring pdgfr are primarily resistant to standard therapy due to d842v mutation that leads tumours not to be inhibited by approved treatments [ 25 ]  . 
 given the benefits achieved by olaratumab targeting pdgfr in preclinical models [ 20 ] , a phase ii trial evaluated tumour response to olaratumab in 30 previously treated 1 3 262 la radiologia medica ( 2019 ) 124 : 259265 metastatic gists into two cohorts with or without pdgfr mutations , respectively [ 26 ]  . 
despite the limitation of this trial due to small sample size and inter - study heterogeneity to draw a definitive conclusion , these data provide the rationale for further study of pdgfr - mutant gist in larger study [ 26 ]  . eribulin eribulin , originally isolated from the marine sponge halichondria okadai , is a structurally modified analogue of halichondrin b . 
moreover , eribulin seems also to inhibit wnt / - catenin signalling , alter tumour vascularization resulting in higher perfusion and drug delivery , and reverse the epithelial to mesenchymal transition [ 28 , 29 ]  . 
given eribulins antitumor activity in preclinical xenograft models of leiomyosarcomas and fibrosarcomas , a non - randomized phase ii ( study 17 ) trial assessed the activity and safety of eribulin 1.4mg / m2 administered intravenously on days 1 and 8 every 3weeks in four independent strata of 128 patients with mesenchymal tumours ( leiomyosarcoma , liposarcoma , synovial sarcoma and other defined sts ) [ 31 ]  . 
activity was demonstrated in patients with liposarcoma ( 46.9% pfs at 12weeks , 95% ci 29.165.3% ) and leiomyosarcoma ( 31.6% pfs at 12weeks , 95% ci 17.648.7% ) [ 31 ]  . an open - label phase iii trial ( study 309 ) randomly assigned 458 patients with metastatic intermediate or high - grade liposarcoma and leiomyosarcoma previously progressed on anthracycline - based chemotherapy to receive eribulin 1.4mg / m2 day 1 and 8 or dacarbazine 8501200mg / m2 every 21days until disease progression or unacceptable toxicities [ 32 ]  . 
most common adverse events with eribulin included neutropenia ( 43 versus 24% ) , pyrexia ( 28 versus 14% ) , alopecia ( 35 versus 3% ) and peripheral sensory neuropathy [ 32 ]  . basing on these results , eribulin has been approved in the usa and europe for treatment of metastatic liposarcoma for patients who received prior anthracycline - based chemotherapy . an ongoing single - arm ( nct03331250 ) phase ii trial aims to assess the activity and effectiveness of eribulin 1.4mg / m2 on day 1 and 8 administered intravenously threeweekly in patients with unresectable or metastatic angiosarcoma and hemangioendothelioma treated with at least one prior systemic treatment . 
 primary completion date is estimated for may 31 , 2021 . immunecheckpoint inhibitors although the approval in the last decade of several drugs for the treatment of metastatic stss [ 15 , 16 ] , these therapies did not achieve a substantial cure rate , leading to the development of new agents . response to conventional radiotherapy or chemotherapy is dependent on histology because some subtypes are chemo - resistant . cancer immunotherapy is gradually taking on a key role in the management of metastatic solid tumours , preventing the development of resistant clones to traditional chemotherapy and fostering tumour recognition by the immune system [ 34 ]  . 
historically , studies using cytokines or immune adjuvants provided small benefits for patients with metastatic stss [ 35 , 36 ]  . in a randomized phase iii trial , immunotherapy with adjuvant mifamurtide , a nonspecific immune stimulator , improves os in patients with osteosarcoma [ 37 ]  . 
recently , the appeal for the improved clinical benefits in several solid tumours due to immune - checkpoint inhibitors leads to assess the safety and activity of these agents in stss . a two - cohort , single - arm , open - label phase ii trial ( sarc028 ) enrolled 84 patients with metastatic or unresectable stss ( leiomyosarcoma , poorly differentiated or dedifferentiated liposarcoma , ewings sarcoma , synovial sarcoma , undifferentiated pleomorphic osteosarcoma , dedifferentiated or mesenchymal chondrosarcoma ) previously progressed up to three lines of chemotherapy to receive pembrolizumab 200mg intravenously every 3weeks until 1 3 la radiologia medica ( 2019 ) 124 : 259265 progression or unacceptable toxicities [ 38 ]  . 
almost 18% of patients with stss had a clinically meaningful objective response , including 40% with undifferentiated pleomorphic sarcoma , 20% with liposarcoma , 10% with synovial sarcoma , and 5% with osteosarcoma . 
no patients with leiomyosarcoma had an objective response . this result is consistent with data from a phase ii trial on nivolumab in leiomyosarcomas that was stopped early because of futility , suggesting a detrimental effect of antipd1 single agent in this subset of patients [ 39 ]  . 
although the mechanism of immune resistance related to leiomyosarcoma histology is still unclear , pten loss and pi3k pathway may play a key role in this process [ 40 ]  . 
 most common adverse events were anaemia , decreased lymphocyte count and platelet count in the bone sarcoma group , whereas anaemia decreased lymphocyte count and prolonged activated partial thromboplastin time in the stss group . in an open - label multicentre phase ii trial , 85 patients with metastatic stss or osteosarcoma previously treated with standard chemotherapies were randomized to receive the anti - pd1 monoclonal antibody nivolumab with or without the anti - ctla4 ipilimumab [ 41 ]  . 
many ongoing trials are still recruiting patients with metastatic stss to assess the activity and efficacy of immune - checkpoint inhibitors in metastatic settings in combination with chemotherapy or neoadjuvant setting with radiotherapy ( nct03092323 , nct03092323 , nct03307616 )  . 
briefly , several ongoing phase i / ii clinical trials are exploring the activity of pembrolizumab in combination with doxorubicin ( nct02888665 , nct03056001 ) , axitinib ( nct02636725 ) , olaratumab ( nct03126591 )  . 
similarly , several ongoing phase i / ii trials are assessing safety and tolerability of nivolumab single agent ( nct03316274 ) or in combination with pazopanib ( nct03149120 ) , ipilimumab ( nct03219671 , nct02982486 , nct02500797 , nct02304458 , nct02428192 )  . conclusion histology - driven approach still remains the mainstay for the treatment of advanced unresectable or metastatic stss . 
although the utmost efforts in the development and quick approval of novel active and practice changing drugs [ 15 , 16 , 21 , 32 ] , prognosis is still poor [ 4 ]  . 
however , standard morphological sequences are often not sufficient to characterize the exact nature of the lesion , addressing the patient to an invasive bioptic examination for the definitive diagnosis . 
the recent technological advances with the development of functional mri modalities such as diffusion - weighted imaging , dynamic contrast - enhanced perfusion imaging , magnetic resonance spectroscopy , and diffusion tensor imaging with tractography have implemented the multiparametricity of mr to evaluate in a noninvasive manner the biochemical , structural , and metabolic features of tumor tissues . 
the purpose of this article is to review the state of the art of these advanced mri techniques , with focus on their technique and clinical application . keywords mri soft tissue tumors dwi spectroscopy dti introduction soft tissue tumors ( stt ) that include a large variety of benign and malignant lesions are of a diverse histological nature . 
incidence increases with age and is higher in males : benign lesions have an incidence of approximately 300 / 100 , 000 , while malignant ones ( that account for 1% of all malignant tumors ) about 5 / 10 , 000 per year . 
the prognosis of these diseases depends on a correct and early diagnosis , the efficacy of treatment , and accurate follow - up for monitoring of recurrence [ 1 ]  . 
beyond the clinical evaluation , imaging plays a fundamental role in the initial assessment of soft tissue tumors for a cost - effective patient management , and mr imaging is considered the modality of choice due to its intrinsic high tissue contrast and multiplanarity , as in the study of other pathologies in the musculoskeletal field [ 110 ]  . 
with the use of standard pulse sequences , it is possible to evaluate the signal intensity , growth pattern , degree of enhancement , and relationship with neighboring * antonio barile antonio.barile@cc.univaq.it 1 department ofbiotechnology andapplied clinical sciences , s . 
standard protocols should include t1and t2 - weighted sequences , with and without fat saturation , gradient echo sequences ( detection of hemorrhage ) , and post - contrast acquisitions , in at least two orthogonal planes [ 12 , 13 ]  . 
however , using standard morphological sequences alone , few soft tissue lesions have specific and pathognomonic mr characteristics ( e.g. , simple lipoma / cyst , hemangioma ) , and the differential diagnosis remains very wide for most cases ; another problem is to differentiate a benign histotype from a malignant , also often not immediate with standard imaging as some overlap exists [ 1417 ]  . 
many limitations of the standard mr sequences are also encountered in the follow - up , both in assessing the response to radiochemotherapy treatment and in identifying possible residual and recurrent tumor after surgery [ 13 ]  . 
in recent years , there has been an increased technical advancement in functional mr sequences , such as proton ( 1h ) magnetic resonance spectroscopy ( mrs ) , diffusion - weighted mri ( dwi ) , and dynamic contrast - enhanced ( dce ) mri . 
these sequences provide detailed structural and metabolic information about vol . : ( 0123456789 ) 1 3 244 la radiologia medica ( 2019 ) 124 : 243252 tumor tissue , allowing to formulate a diagnostic hypothesis as close as possible to histological diagnosis in a noninvasive way [ 13 , 2023 ]  . the purpose of this article is to review technical aspects of each of these advanced mr imaging techniques , with a particular focus on their clinical application in the characterization , differentiation of benign from malignant lesions and the assessment of response to treatment in soft tissue tumors . diffusionweighted imaging ( dwi ) dwi is a functional mri technique that provides information about tissue cellularity and cell membrane integrity , evaluating the diffusivity of water molecules ( brownian motion ) [ 2427 ]  . technique the dwi signal is given by the degree of movement of water molecules in cellular spaces ( extracellular , intracellular , transcellular , and intravascular ) , in an inversely proportional manner [ 28 ]  . 
it is important to take into account the contribution to the dwi signal of the intravascular movement of water molecules since in very vascularized lesions it can be significant [ 1 , 11 , 19 ]  . there are several dwi sequences , including spin - echo dwi , echo - planar imaging ( epi ) , and steady - state free precession sequences [ 11 ]  . 
some authors suggest that the evaluation of the minimum adc may be more accurate as it would represent the area of the greatest cellularity of the lesion [ 11 , 29 ]  . 
as mentioned earlier , it is important to take into account tissue perfusion and intravascular water component , as adc values increase in vascularized tumors , leading to overlapping in adc values between benign and malignant tumors . 
the main limits of dwi are represented by the inherent low signal - to - noise ratio and by the low spatial resolution , the artifacts from susceptibility ( artifacts in correspondence of tissues with blood products or air )  . 
for these reasons , dwi must always be interpreted in conjunction with anatomical sequences [ 15 , 19 , 29 , 30 ]  . applications the dwi signal and the adc values reflect the cellularity of the tissues , so even if there are no normal cutoff values , dwi can characterize the biological activity of the tissues . 
in the study of musculoskeletal soft tissue tumors , this means that , as a general rule , benign tumors with a low degree of biological activity will have a loss of adc signal as the b values increase , while malignant tumors ( in which the water has greater restriction in movement ) will show high intensity at high b values . 
the authors found the highest values in benign cystic tumors and the lowest values in giant cell tumors of tendon sheaths ( maybe due to their spindle - shaped stromal cells and multinucleated giant cells histological composition )  . 
 [ 30 ] , using conventional mri and dwi sequences together , obtained values of sensitivity , specificity , and accuracy of 96% , 85.7% , and 90% , respectively . 
the authors confirmed the persistence of high signal intensity with increasing b values in all malignant lesions ( muscular metastases , myxoid liposarcoma , etc . ) on the qualitative evaluation , with low adc values on quantitative analysis with increasing b values , although with differences among the various histological types . 
they also found that higher b values ( more than 800s / mm2 ) are useful to increase the contrast between benign and malignant lesions and thus reduce the number of equivocal cases . 
 [ 32 ] reported the role of dwi in the distinction between benign and malignant peripheral nerve sheath tumors ; in particular , their results showed that the minimum adc value is a better indicator of malignancy than the average adc value , due to the heterogeneity in cellularity of both benign and malignant pnsts . 
dwi sequences show values of 2.75 103 mm2 / s ( b value = 1000 ) on adc map , confirming the benign cystic nature of the lesion 1 3 246 la radiologia medica ( 2019 ) 124 : 243252 in another study [ 28 ] , mean adc of desmoid tumors was found to be significantly higher than that of malignant soft tissue tumors without overlap in the minimum adc values . dwi has proved very useful also in the assessment of treatment response to chemotherapy in soft tissue tumors . 
similarly , the evaluation of enhancement patterns can be challenging , as both granulation and scar tissues ( aspecific tissue changes after chemo / radiotherapy ) are enhancing after contrast administration , and the differentiation from the viable tumor is not always direct [ 15 ]  . 
dwi demonstrated to improve this discrimination earlier than conventional imaging , as solid tumors are characterized by high cellularity with intact cell membranes , while tissues after cytotoxic treatment show lower cellularity and membrane damage [ 15 , 22 ]  . 
dwi implements standard morphological sequences also in the evaluation of postsurgical follow - up [ 6 , 35 , 36 ] , aiding to detect residual / recurrent tumor tissue . dynamic perfusion mri dynamic perfusion mri is a functional imaging technique often used to evaluate musculoskeletal tumors , mainly to depict early intravascular and interstitial distribution of gadolinium [ 22 , 29 , 37 ]  . technique dce - mri is typically performed with multiple repeated rapid , volumetric , and gradient echo sequences acquired immediately after intravenous administration of gadoliniuat our institution , routine dynamic contrast enhancement is performed using t1 3 double fast spin - echo ( dfse ) sequences with fat saturation [ 29 ]  . 
we then perform eight 19 - s scans in fast succession , with a scan delay variable on the region to be studied but that never exceeding 20s , to ensure proper arterial - phase perfusion . 
semiquantitative methods of postprocessing involve the postprocessing of timeintensity curves using three identical rois positioned at a site of marked early tumor enhancement , in an artery , and in a healthy muscle , respectively [ 22 , 37 , 38 ]  . 
the resulting timeintensity curves provide a graphic representation of contrast perfusion , from which quantitative information ( time to enhancement , wash in , peak enhancement , and washout ) can be obtained [ 37 ]  . the curves can be classified into five types [ 22 ] : type 1 , no enhancement ( e.g. , lipoma ) ; type 2 , weak and gradual enhancement ( e.g. , benign tumors or schwannoma ) ; type 3 , rapid early enhancement followed by a plateau ( e.g. , benign vascular tumors , desmoid tumors , abscesses , and some malignant tumors , but with limited specificity ) ; type 4 , rapid early enhancement followed washout ( highly vascular tumors with small interstitial compartment such as malignant histiocytofibroma , synovial sarcoma , and leiomyosarcoma and several benign tumors such as giant cell tumor ) ; type 5 , rapid early enhancement followed by slow , gradual enhancement ( tumors with large interstitial compartments such as myxoid tumors )  . however , even if malignant lesions typically demonstrate rapid early arterial enhancement and higher slopes of enhancement compared with benign lesions , the patterns may show some degree of overlap secondary to highly vascularized benign lesions and poorly vascularized or necrotic malignant lesions [ 29 ]  . applications the main applications in the imaging of soft tissue tumors of dynamic perfusion mri are in the characterization of the lesions , identification of viable tumor areas to target biopsy , monitoring of chemotherapy treatment outcome , and differentiation of residual tumor from scarring [ 11 , 22 , 39 ]  . 
regarding soft tissue lesions , whereas perfusion mri enabled differentiation between lesions with low and high biological aggressiveness , we could never obtain typical timeintensity curves for the various histological tumor types [ 37 ]  . 
pictures a14 : lipoma of the elbow showing homogeneous hyperintense signal intensity on a t1 - weighted sequence ( a1 ) and no enhancement on qualitative evaluation after gadolinium administration ( a2 )  . 
the second subcutaneous lesion ( b14 ) shows inhomogeneous internal structure with areas of adipose signal intensity , intralesional septa , and prevalent peripheral enhancement after gadolinium injection ( b3 ) , with evidence of a type 2 signal intensity curve . 
cases c14 show a subcutaneous polilobulated lesion of the leg strictly adherent to the superficial fascia , with inhomogeneous internal structure and intense contrast enhancement after gadolinium injection ( c4 ) , with evidence of timeintensity curves types 3 and 4 ( arrow )  . 
the mri features of the lesion are consistent with a myxoid liposarcoma on dynamic contrast - enhanced mr imaging , malignant peripheral nerve sheath tumors ( mpnsts ) usually show early arterial enhancement that is much rarer in their benign counterpart ( bpnsts ) [ 23 ]  . the application of dynamic perfusion mri in guiding bioptic procedures is particularly useful in soft tissue tumors that have a significant cystic or hemorrhagic component [ 1 , 41 ] , as purely fluid areas without contrast enhancement should be avoided during biopsy , to prefer the more solid , enhanced portions . 
dynamic contrast - enhanced mri is also helpful in delineating tumor margins ; in fact , tumor enhancement is precocious and faster than that of peritumoral edema and the initial slopes of tumor and nontumor tissues differ significantly [ 11 ]  . perfusion mri is also useful for distinguishing cysts from myxoid tumors and to characterize the benign or malignant nature of myxoid lesions : cysts show no enhancement , while the myxoid component of sarcomas exhibits early and avid enhancement [ 11 ]  . 
the authors postulated that whether differentiation of low - flow from high - flow vascular malformations can be made with nearly 100% sensitivity and specificity setting a 30 - s threshold for the contrast rise time [ 43 ]  . dynamic enhancement is also showing utility in monitoring chemotherapy response , evaluating the degree of tumor necrosis and distinguishing postoperative tissue changes ( e.g. , fibrosis ) from recurrent tumor [ 1 ]  . 
direct visual ( qualitative ) inspection of mri images allows simple recognition of perfused viable tumor tissue with less intense ( slower enhancing ) areas of peritumoral edema , normal tissue , and tumor necrosis [ 11 ]  . 
 quantitatively , an at least 60% decrease in the timeintensity curve slope value indicates more than 90% of tumor necrosis and good treatment outcome [ 11 , 22 ]  . 
optimal follow - up requires three dynamic perfusion mri studies : preoperatively ( before the biopsy and before surgery ) and postoperatively ( during chemotherapy ) [ 11 ]  . 
follow - up examinations ( after 36months ) are necessary when evaluating the treatment response after radiotherapy , as radiotherapy may lead to granulation tissue with increased perfusion that cannot be distinguished by residual tumor early [ 22 ]  . magnetic resonance spectroscopy ( mrs ) mrs is a functional noninvasive imaging technique that requires no intravenous contrast administration and characterizes lesions based on their metabolic constituents [ 1 , 11 , 13 , 29 , 44 ]  . 
 higher field strengths provide a greater signal - to - noise ratio ( snr ) , with improved spectral resolution ; the main drawbacks are the increased field inhomogeneity and the consequently increased metabolite line widths [ 44 ]  . 
using the multi - voxel technique , it is possible to obtain information over a wider field of view , analyzing entire large lesions and surrounding tissue or multiple lesions with a single acquisition . 
the positioning of rois is critical to avoid areas containing bony structures , necrotic or hemorrhagic foci ( underestimation of the choline peak ) , calcifications ( increased field inhomogeneity ) , fat ( can obscure the choline peaks ) , or muscle ( overestimation of the choline peak )  . 
the enhancing portion of the tumor is targeted in roi positioning ; for tumors exhibiting weak / slow enhancement or no enhancement after 5min , the voxel is positioned at sites of delayed enhancement [ 44 ]  . applications already widely used in neuroradiology , magnetic resonance spectroscopy ( mrs ) has recently gained also a role in the musculoskeletal field . 
one of the main applications is the assessment of malignancy in musculoskeletal tumors since specific metabolites ( trimethylamine / choline - containing compounds including phosphocholine , glycerophosphocholine , and free choline ) are distinctively increased in malignant lesions , and they are considered as a marker of malignancy [ 45 ]  . 
to date , the literature results in musculoskeletal mrs investigated the qualitative analysis of the choline or trimethylamine peak as a marker for malignancy [ 21 , 44 ]  . 
in a series of russo etal . , all tumors with a mitotic index greater than 2 / 10 hpf had a positive choline peak and were malignant and correlation between 1h - mrs findings and mitotic index was high [ 16 ]  . 
3 mri axial images of a solid lesion at the level of the flexor tendons of the wrist showing a low signal intensity on t1and t2 - weighted sequences ( a , b ) and intense contrast enhancement after gadolinium injection ( c )  . 
the imaging features are consistent with a giant cell tumor of the tendon sheaths ( gctts ) positive choline peak , and also a large number of inflammatory lesions may produce a high choline peak [ 16 ]  . for example , benign peripheral nerve sheath tumors typically have detectable choline content by mrs . 
in a recent study that used mr spectroscopy to evaluate bpnsts and mpnsts , trimethylamine concentrations and the trimethylamine fraction were found to be relatively lower in the benign neoplasms , and a trimethylamine fraction threshold of 50% resulted in 100% sensitivity and 72.2% specificity [ 45 ]  . the presence of a lipid peak can be detected in the wall of abscesses , in the solid part of highly malignant lesions , and in tumors during treatment response , probably related to cell membrane turnover . 
lipid peak , however , has to be analyzed carefully , due to the possibility of lipid contamination caused by surrounding tissue [ 11 , 16 ]  . mrs evaluation of choline may be used not only for tumor characterization but also to assess treatment response , showing a choline peak reduction after chemotherapy in malignant musculoskeletal lesions [ 11 ]  . the limitation of the literature choline mrs studies up to date is that they are mostly qualitative rather than quantitative , making the distinction of metabolically active benign soft tissue tumors from malignant masses difficult . 
 so , currently , the utility of mrs is limited to its high negative predictive value [ 29 ]  . diffusion tensor imaging andtractography diffusion tensor imaging ( dti ) and tractography are feasible techniques to visualize the spatial anatomy of peripheral nerves in the presence of stt , especially in cases where the course and the involvement of major peripheral nerves are difficult to assess with standard morphological mr sequences [ 20 , 23 , 42 , 46 ]  . technique dti evaluates the three - dimensional ( 3d ) motion of protons in tissues providing quantitative data on the amount and directionality of random movement of water molecules [ 46 ]  . 
4 axial ( a ) an coronal ( b ) mr images of a rounded fusiform lesion at the level of the posterior compartment of the leg ( within the soleus muscle ) showing intense , homogeneous contrast enhancement . 
 axial dti sequence ( c ) with fiber track reconstruction ( d ) demonstrates the growth of the lesion within the nerve fibers and its relationship to thethe imaging features are consistent with the diagnosis of schwannoma limiting it in another , the so - called anisotropy . 
images are evaluated for image quality , adc of the lesion , tractography , and fractional anisotropy of nerves . applications in musculoskeletal imaging clinical practice , dti and tractography are mainly used to evaluate peripheral nerve tumors and soft tissue tumors arising around nerve structures [ 20 ]  . 
this approach is of paramount importance not only for the diagnosis when there is often great difficulty in correctly delineating the tumor from healthy nerve structures , but also for the preoperative planning , as the preservation of unaffected nerve fascicles is important to maintain neuromuscular function after surgery [ 20 ]  . 
 moreover , correlation of d sectional images with surgical findings , particularly in anatomically complex regions , can 1 3 la radiologia medica ( 2019 ) 124 : 243252 be challenging [ 46 ]  . 
in schwannomas , in which the tumor originates from the sheath of a single fascicle , leaving the main trunk of the peripheral nerve attached to the mass , dti and tractography imaging are helpful in the differential diagnosis with neurofibromas , clearly depicting the eccentric and separate tumor growth relative to the involved nerve . 
the added information obtained from these sequences , either alone or integrated , may improve multiparametric evaluations of soft tissue tumors that result in more accurate diagnosis , appropriate treatment planning , and monitoring of treatment efficacy . 
it is important to further implement these techniques to be able to use them on a routine clinical basis and to standardize furtherly acquisition protocols . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical approval this article does not contain any studies with human participants performed by any of the authors . la radiologia medica ( 2019 ) 124 : 290300 radiotherapy influence ofage andsubtype inoutcome ofoperable liposarcoma danielagreto1 calogerosaieva2 mauroloi1 francescaterziani1 lucavisani1 pietrogarlatti1 monicalorusso1 cristinamuntoni1 carlottabecherini1 julianatopulli1 domenicocampanacci3 giovannibeltrami3 guidoscoccianti3 francescomuratori3 pierluigibonomo1 isaccodesideri1 giuliofrancolini1 lorenzolivi1 received : 13 february 2018 / accepted : 2 november 2018 / published online : 12 november 2018 italian society of medical radiology 2018 abstract aim liposarcoma ( lps ) is rare tumor deriving from adipocytes . 
the aim of this study is to evaluate whether clinical characteristics , tumor and treatment - related features affect clinical outcome in patients treated with curative intent for non - metastatic liposarcoma . methods data of patients with locally advanced , non - metastatic liposarcoma treated between 1990 and 2015 were retrospectively reviewed . 
statistical analysis was performed to assess correlation between the above - cited variables and local recurrence - free survival ( dfs - lr ) , distant metastasis - free survival , overall survival ( os ) and disease - specific survival ( dss ) ; moreover , differences in clinical outcome between the two age groups were identified . results data of 186 patients were collected . 
further studies are needed to stratify patients subgroup and develop tailored treatment strategies ( i.e. , altered fractionations and different chemotherapy regimens in aggressive subtypes ) , in particular more prospective trials are needed to develop treatment guidelines in elderly sts , taking into account the frailty and the peculiarity of this subgroup . keywords liposarcoma radiotherapy soft tissue sarcoma age extended author information available on the last page of the article vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 290300 background soft tissue sarcomas ( stss ) are rare tumors accounting for about 1% of all tumors [ 1 ]  . 
liposarcoma is a heterogeneous disease characterized by different clinical behavior according to histological subtypes : ddlps showed the most aggressive clinical course in terms of disease recurrence and worse os . 
further studies are needed to stratify patients subgroup and develop tailored treatment strategies ( i.e. , altered fractionations and different chemotherapy regimens in aggressive subtypes ) , in particular more prospective trials are needed to develop treatment guidelines in elderly sts , taking into account the frailty and the peculiarity of this subgroup . 
well - differentiated liposarcomas ( wdlps ) are considered locally aggressive , with low potential for metastatic spread [ 4 ] ; however , more aggressive features of disease can be acquired in the event of local recurrence . 
 dedifferentiated liposarcoma ( ddlps ) , both de novo and secondary to progression from a well - differentiated disease , [ 4 ] , has a worse prognosis with a 41% and a 1730% rate of local recurrence and metastatic spread , respectively . 
myxoid liposarcoma ( mlps ) , the most common subtypes in pediatric population , is characterized by a particular metastatic pattern , with high predisposition to spread into fat - bearing areas , such as mediastinum , bone marrow or retroperitoneum [ 8 , 9 ]  . 
pleomorphic liposarcoma ( plps ) is the subtype with the lowest grade of differentiation characterized by poor outcomes , with an estimated risk of 3445% of local recurrence and 3257% of metastatic disease [ 10 ]  . 
approximately 40% of sts patients are diagnosed over the age of 65 [ 14 ] , and in particular , with the exception of mlps , most liposarcoma subtypes are diagnosed in adults [ 15 ]  . 
it is unclear whether differences in outcome can be explained by a more aggressive biological behavior or because in most cases elder patients do not receive full standard treatment and are not included in clinical trials [ 16 ]  . a tailored approach taking into account the specificity of disease subtype and age at presentation could be helpful in delineating therapeutic management of liposarcoma . 
the aim of this study is to evaluate whether clinical characteristics , tumorand treatment - related features affect clinical outcome in patients treated with curative intent for nonmetastatic liposarcoma . materials andmethods data of patients with locally advanced , non - metastatic liposarcoma treated between 1990 and 2015 were retrospectively reviewed . 
a baseline chest ct scan or x - ray was performed in all patients , to exclude metastatic lung disease ; contrast - enhanced magnetic resonance ( mri ) and / or ct of the primary tumor location was performed , to complete locoregional staging and define tumors relationship with surrounding anatomical structures . 
all patients were selected to undergo radical surgery ; in case of unresectable , locally advanced disease , preoperative rt for a total dose of 50gy ( 2gy per fraction for 5days a week ) was delivered , to reduce the tumor size . 
postoperative rt ( port ) was delivered in case of high - grade disease , tumor diameter > 5cm and / or deep location , for a total dose of 60gy ( 2gy per fraction for 5days a week )  . 
anthracycline - based chemotherapy was administered in case of high - risk disease ( at least two of the following prognostic factors : high grade , deep - seated tumor , large dimensions , positive surgical margins ) in association to rt . 
 treatment schedule consisted of epirubicin ( 60mg / m2 on days 12 ) and ifosfamide ( 3g / m2 on days 13 ) , repeated every 21days ( table1 )  . 
 data about age at diagnosis , sex , age , tumor location ( trunk , upper and lower limb ) and tumor depth were collected , as well as histopathological characteristics such as tumor size , 1 3 292 la radiologia medica ( 2019 ) 124 : 290300 table 1 treatment procedures chemotherapy postoperative radiotherapy preoperative radiotherapy brachytherapy epirubicin : 60mg / m2 day : 1 , 2 ifosfamide : 3g / m2 / dayday : 1 , 2 , 3 every 21days 60gy : 2gy per fraction ; 5days a week 50gy : 2gy per fraction ; 5days a week 3035gy ( brachy needles implantation ) grade ( according to fnclcc grading system [ 18 ] ) , surgical margins status . 
the pathological specimens of patients treated before 2013 were reviewed and classified according to 2013 world health organization ( who ) classification of tumors of soft tissue and bone [ 19 ]  . clinical outcome endpoints analyzed were local relapse - free survival ( lrfs ) , distant relapse - free survival ( drfs ) , overall survival ( os ) and disease - specific survival ( dss )  . 
overall survival ( os ) and dss were calculated from the date of surgery to the time of the last follow - up or death for any causes and death from cancer , respectively ; local relapse - free survival ( lrfs ) and distant relapse - free survival ( drfs ) were calculated from the surgery to the time of the local recurrence and the time of the distant metastasis development , respectively . 
wide excision , marginal surgery and intralesional excision were performed in 151 ( 81.2% ) , 25 ( 13.4% ) and 7 ( 3.8% ) patients , 1 3 la radiologia medica ( 2019 ) 124 : 290300 respectively ; three ( 1.6% ) patients , all of whom younger than 65years , underwent amputation . 
port was administered in 112 ( 60.2% ) cases : brachytherapy ( bt ) was delivered in addition to external beam ( ebrt ) in 39 patients and as an exclusive treatment in six patients . 
5 kaplanmeier curves analysis of os in all patients surgical resection remains the cornerstone of curative management of liposarcoma , as well as for other subtypes of soft tissue sarcoma . 
depending on patients and tumor characteristics , surgery is often associated with rt and / or chemotherapy . however , liposarcoma is a heterogeneous disease , with distinct subtypes and variable clinical behavior [ 15 ]  . 
in particular , the role of port in wdlps is debated , since the low risk of distant metastases could be related to a decreased clinical benefit in this subset [ 20 ]  . 
conversely , local control rates of about 97% are reported for mlps treated with surgery and rt [ 21 , 22 ] ; moreover , preoperative rt might yield excellent responses , due to the high radiosensitivity of mlps , and should always be considered when patients are not amenable to upfront surgery [ 23 , 24 ]  . due to the high heterogeneity of liposarcomas , literature data about clinical outcomes are extremely different . 
in our cohort , at a mean follow - up of 10years , about one patient out of four experienced local recurrence or metastatic relapse ; half of the patients were alive at the time of our analysis . 
authors reported rates of relapse of 1857% , 728% and 1645% in dlps , mlps and plps , respectively , and survival rates ranging between 7693% , 5464% , 4075% and 063% in wdlps , dlps , mlps and plps . 
 [ 25 ] proposed a 1 3 298 la radiologia medica ( 2019 ) 124 : 290300 liposarcoma - specific postoperative nomogram for diseasespecific survival ( dss ) , aimed to provide an individualized estimate of cancer specific mortality . 
identification of risk classes could allow to intensify treatment in certain disease subtypes with poor clinical outcomes ( i.e. , chemotherapy to reduce metastatic spread in plps ) , while overtreatment could be avoided in more favorable subgroups . 
in soft tissue sarcoma , baseline features such as age , tumor grade and surgical margins are well - known predictive factors of clinical outcome . in our series , age older than 65 was an independent prognostic factor affecting local and distant recurrence and os . 
specific genomic alterations are more likely to occur in older patients , influencing prognosis [ 30 ]  . in our report , disease characteristics and treatment modalities distribution between patients younger than 65years and the elderly were different . 
plps and ddlps that were more common in our elderly patients are well - known histopathological subtypes correlated to a worst prognosis in terms of local and distant recurrence than mlps , and the response to perioperative treatments such as radiotherapy and chemotherapy are expected inferior compared to mlps [ 15 ]  . 
preoperative radiotherapy was delivered in 12.1% of patients older than 65years compared to 30% of younger patients ( p = 0.004 ) ; multidisciplinary team in case of elderly patients usually reserve radiotherapy indication only in very high risk of disease recurrence such as positive margins , high - grade and deepsited tumors . 
 [ 32 ] analyzed 1240 localized soft tissue sarcoma patients from the french soft tissue sarcoma database , reporting that tumor grade was an independent predictor of metastasis in all the histologies ( 15.2% of patients had a diagnosis of liposarcoma ) with the exception of malignant schwannomas and rhabdomyosarcomas . 
according to a large cohort - based analysis of 1513 soft tissue sarcoma cases [ 33 ] , anthracycline - based adjuvant chemotherapy improved dmfs and os only in g3 patients . 
it could be possible that the worse outcome of patients treated with preoperative radiotherapy was due to unfavorable disease with large tumor size and deep - sited location . in our cohort , wide excision was significantly related to improved survival . 
due to the high risk of microscopic residual disease in the peritumoral tissue , the adequacy of surgical margins has been investigated by several authors as a major predictor of outcome ; its value has been confirmed in a recent study [ 37 ]  . 
liposarcoma often infiltrates surrounding soft tissue ; thus , it is possible that maximizing tumor control in the primary site might result in improved long - term disease control [ 38 ]  . finally , the safety of concomitant rt and chemotherapy administration was analyzed . 
our data are similar to those described in literature [ 39 ]  . conclusions liposarcoma is a heterogeneous disease characterized by different clinical behavior according to histological subtype : ddlps showed the most aggressive clinical course in terms of disease recurrence and worse os . 
further studies are needed to stratify patients subgroup and develop tailored treatment strategies ( i.e. , altered fractionations and different chemotherapy regimens in aggressive subtypes ) , in particular more prospective trials are needed to develop treatment guidelines in elderly sts , taking into account the frailty and the peculiarity of this subgroup . compliance with ethical standards conflict of interest none . ethical approval this article does not contain any studies with animals performed by any of the authors . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 241242 editorial artificial intelligence : achallenge forthird millennium radiologist robertograssi1 vittoriomiele2 andreagiovagnoni3 received : 4 january 2019 / accepted : 14 january 2019 / published online : 1 february 2019 italian society of medical radiology 2019 diagnostic imaging techniques , i.e. 
they produce a large number of images , on which the radiologist writes , after a subjective and personal evaluation , essentially qualitative , the diagnosis , the so - called report . these diagnostic technologies acquire an enormous amount of numerical data in dicom format , of which only a part is visually evaluated in greyscale . 
hundreds to thousands can be derived from a statistical mathematical analysis of raw data [ 1 ]  . for some years now , throughout the world , there has been an attempt not to disperse this great mass of information in the raw data . 
the ambitious objective is to identify , thanks to complex mathematical and statistical algorithms , which information , inaccessible to simple visual analysis , can predict the evolution of the disease and the effectiveness of the therapy , but in a quantitative and objective way . artificial intelligence , machine learning , big data , radiomics are just some of the many terms that are used by researchers in the field , especially computer scientists , clinical engineers , physicists , to define their activities . 
brambilla , 3 , 50134florence , italy 3 department ofradiological sciences , azienda ospedaliero universitaria ospedali riuniti , universit politecnica delle marche , ancona , italy what is missing then and what will be the keystone to achieve these goals ? the answer may seem trivial , but it is not : the radiologists collaboration . in fact , it will never be sufficient to collect only the data , raw or in dicom format , also re - elaborated to constitute the so - called big data , but it will be necessary to correlate them with the radiological reports , so that the computer can process them and find the correlation between them and the phenotype in question . but , to do this , the computer must have a standardized report , which , in part , is also referred to as a structured report . 
it , thanks to the recognized authoritativeness , has the possibility to convey its use in a large number of structures . oncology is the first area in which to apply . 
combining the huge amount of data tagged with the radiological reports will be like inserting the plug into the socket : our radiological world will glow with a new light . 
our report will contain over time not only a subjective and qualitative interpretation of the images , our diagnosis , but also a series of numerical values , objective and quantitative features , our contribution to the prognosis , because some of them will have proved useful to predict the efficacy of the therapeutic response . 
parp inhibitors exert antitumor activity by both catalytic parp inhibition and parpdna trapping , moreover parp inhibition represents a potential synthetic lethal approach against cancers with specific dna - repair defects . 
soft tissue sarcoma ( stss ) are a heterogeneous group of mesenchymal tumors with locally destructive growth , high risk of recurrence and distant metastasis . objectives the purpuse of this review is to provide an overview of the main preclinical and clinical data on use of parpi in stss and of effect and safety of combination of parpi with irradiation . results due to numerous genomic alterations in stss , the dna damage response pathway can offer an interesting target for biologic therapy . 
although mechanisms of synergisms are not completely known , combination of radiation therapy and parp inhibitors exerts antitumor effect by accumulation of unrepaired dna damage , arrest in g2 / m , activity both on oxic and hypoxic cells , reoxygenation by effect on vessels and promotion of senescence . 
early trials have shown a good tolerance profile . conclusions the use of parp inhibitors in advanced stage stss , alone or combined in multimodal treatments , is of great interest and warrants further investigations . keywords poly ( adp - ribose ) polymerases ( parp ) soft tissue sarcoma ( stss ) dna damage response pathway radiation therapy * monica mangoni monica.mangoni@unifi.it 1 department ofbiomedical , experimental andclinical sciences mario serio , section ofradiation oncology , university offlorence , largo brambilla 3 , 50134florence , italy 2 department oforthopaedic oncology , azienda ospedaliera universitaria careggi , largo brambilla 3 , 50134florence , italy itt , istituto toscano tumori , via taddeo alderotti 26 / n , 50139florence , italy introduction poly ( adp - ribose ) polymerases ( parp ) are a large family of enzymes involved in several cellular processes , including dna single - strand break repair ( ssb ) via the baseexcision repair ( ber ) pathway [ 1 , 2 ]  . 
subsequently , parp1 leaves damaged dna , owing to the dense negative charge of padpr , and allows vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 282289 fig . 
the resulting negatively charged poly ( adp - ribose ) polymers decrease the affinity of parp1 for dna , while recruit additional dna repair proteins , leading to dna repair . 
loss of function of brca proteins ( hr deficiency ) leads to unrepaired damage ( i.e. , due to replication fork collapse ) and subsequent cell death , or to the use of alternative repair pathways , such as non - homologous end joining ( nhej )  . 
 moreover , parp - 1 , due to the inhibition that blocks autoparylation , can remain trapped onto dna damaged site , in particular during ber , and determine an obstruction to replication forks . 
in this case , if parp1 cannot cope with ssbs during this semi - conservative repair process , the accumulated unrepaired ssbs that are converted to dsbs could became highly toxic to cells . 
parp - 1 is implicated in the cellular response to dsbs by promoting hr at damaged replication forks , and repressing the nonhomologous end - joining ( nhej ) repair , 1 3 284 la radiologia medica ( 2019 ) 124 : 282289 the alternative dsb repair pathway in response of a defective hr . 
hr represents a strong determinant of response of the hr - competent cells to parp inhibition . the combination between hr deficiency and a parp inhibition can be described as a synthetic lethality , that is the cell death as result of a combination of deficiency in the expression of genes , due to mutations , epigenetic alterations , and inhibition . 
many cancers seem to be particularly sensitive to parp inhibition , such as ovarian cancers and other solid tumor with germline mutations in brca1 or brca2 , crucial proteins for hr . 
indeed , in brca1 / 2 defective cells , parpi induce an increase in ssbs , which in turn are transformed during replication in irreparable toxic dna double - strand breaks ( dsbs ) , due to the hr process defect [ 2 , 6 ]  . 
additional genetic modulators of parpi sensitivity have been identified , such as mutations in the genes encoding atm , atr or pten , and elevated parp1 expression is emerging as a measure of parpi sensitivity [ 7 , 8 ]  . parp inhibition may represent a new potential synthetic lethal approach against cancers with specific dna - repair defects . 
moreover , the parp - trapping mechanism may have a pivotal role in the synergy between a parpi and dna damaging agents [ 3 ]  . there are currently three parpi that have been fdaapproved for use : olaparib ( astra zeneca , london , uk ) , rucaparib ( clovis oncology , boulder , co , usa ) , and niraparib ( tesaro inc . , waltham , ma , usa )  . 
other parpi in active development include veliparib ( abbvie pharmaceuticals , north chicago , il , usa ) , and talazoparib ( pfizer pharmaceuticals , new york city , ny , usa ) [ 9 ]  . soft tissue sarcoma ( stss ) are a heterogeneous group of mesenchymal tumors with locally destructive growth , high risk of recurrence and distant metastasis [ 10 , 11 ]  . 
both preand post - operative radiotherapy ( rt ) are recommended for intermediate or high - grade stss and for patients with large or marginally excised , low - grade tumors . 
although exist some controlled evidences about of the benefit of chemotherapy , often are conflicting , due to the different chemosensitivity depending on the histological subtype , and insufficient to support chemotherapy as a standard administration . 
for that reason , at present , it does not exist a shared strategy and many efforts are necessary to ameliorate knowledge on subtypes genetic profile , tumorigenesis and drug activity to allow specific and individualized treatments [ 1113 ]  . 
 cytogenetic molecular analyses have allowed two different types of sarcoma to be distinguished : stss with simple genomics , associated with a simple genomic alteration , and stss with complex genomics , characterized by very complex karyotypes and a high genomic instability . 
from well - differentiated to de - differentiated histotypes , the secondary genetic mutations determine an increased genomic complexity , chromosome aberrations and loss of specific targets [ 14 , 15 ]  . 
notably , ewsfli1 gene fusion acts in a positive feedback loop to maintain the expression of parp1 , which is required for ewsfli - mediated transcription , thereby enforcing oncogene - dependent sensitivity to parp - 1 inhibition [ 16 ]  . 
thus , it is speculated that ewsfli1 transcriptional program primes ewing sarcoma cells for hypersensitivity to parpi by inducing high parp1 expression , increasing the availability of parp1 for trapping , and elevating basal dna damage [ 7 ]  . 
the ability of parpi to trap parp differs among parpi , and is not linked to their ability to inhibit parp ; veliparib is a potent inhibitor of parp enzymatic activity but a poor trapper and results less toxic than olaparib in ewing sarcoma cells [ 17 ]  . 
 the comparison of four parp inhibitors in ewing sarcoma cells showed marked differences in the single agent cytotoxicity with decreasing potency in the order of talazoparib ( ic50 10 nm ) > niraparib ( ic50 300 nm ) > olaparib ( ic50 1000 nm ) > veliparib ( ic50 10 , 000 nm ) [ 18 ]  . 
after the discovery of the ability of parpi to trap parp , that is even more toxic to cells than the accumulating dna damage , the combination of parpi and cytotoxic drugs was tested [ 20 ]  . 
the combination with a chemotherapy agent can drive accumulation of dna damage in ewing sarcoma cells , heightening the recruitment of parp1 to dna for ssb repair , and thereby driving enhanced parp1 trapping [ 7 ]  . 
the differential ability of chemotherapeutic drugs to synergize with parpi has been attributed to the type of dna lesions generated by the anticancer agents that differentially require parp1 for dna repair or affect binding of parp1 to the dna [ 18 ]  . 
consequently , the antiapoptotic protein mcl - 1 is downregulated , the proapoptotic proteins bax and bak are activated , mitochondrial outer membrane is permeabilizated and caspases and caspasedependent cell death are activated [ 18 ]  . 
mechanistically , talazoparib and temozolomide cooperated to induce apoptotic cell death , loss of mitochondrial membrane potential , caspase activation , dna fragmentation and caspase - dependent cell death [ 18 ]  . parpi have been reported to act also in concert with doxorubicin , melphalan , carboplatin , etoposide and irinotecan or its active metabolite sn38 in ewing sarcoma cells and other stss cell lines [ 18 , 2123 ]  . 
in u2os osteosarcoma cell line , knockdown of parp - 1 resulted in decreased cell proliferation , increased cell apoptosis , and g0 / g1 phase arrest and correlated with elevated chemosensitivity to cisplatin through inactivation of the erk1 / 2 signaling pathway [ 24 ]  . 
in ewing sarcoma cells , the combination of olaparib and trabectedin was found to be highly synergistic , inhibiting cell proliferation , inducing apoptosis , and the accumulation of g2 / m [ 25 , 26 ]  . 
thus , ewing sarcoma cells were the most sensitive to the combination parpi / trabectedin , preclinical data show additive or synergic activity also in large panels of stss [ 27 ] , where different degree of synergism was observed among different cells line [ 26 ]  . 
for example , in leiomyosarcoma models the combination was significantly more active than single agents , while in osteosarcoma models no further advantage was obtained if compared to trabectedin alone . 
parp1 expression or different parylation was showed to dictate the degree of the synergism [ 26 ] , i.e. , single nucleotide polymorphism in the parp1 gene ( val762ala ) is known to result in a less efficient parp1 variant [ 28 ]  . 
moreover , gene sets involved in the combination synergism suggest a specific dna - damage response / repair and cell cycle control gene signatures that might become predictive biomarkers of response [ 26 ]  . 
despite the fact that parpi as single agents exerted promising cytotoxicity against stss cells invitro [ 29 ] , they exerted limited efficacy in xenograft models [ 18 ] without improvement of survival [ 21 ]  . 
synergistic effect was observed with combining treatment of parpi with cyclophosphamide , topotecan , temozolomide , irinotecan and trabectedin [ 16 , 20 , 25 , 27 , 30 , 31 ]  . clinical data withparpi instss the first phase ii clinical trial testing single - agent parpi in ewing sarcoma patients with recurrent disease failed to show improvement in outcome [ 7 , 16 , 32 , 33 ]  . 
clinical 1 3 286 la radiologia medica ( 2019 ) 124 : 282289 data were consistent with the minimal activity observed in xenograft model , due to poor parp1 trapping invivo [ 16 ]  . 
in the recent phase i nct01286987 study , talazoparib showed single - agent antitumor activity and a tolerable safety profile in brca mutation - associated breast and ovarian cancers , and in patients with pancreatic and small cell lung cancer , however , for patients with ewings sarcoma no objective response was observed [ 34 ]  . 
a possible explanation for the discrepancy between invitro and invivo / clinical effect is that some cell lines may have been derived from patient tumor samples that were not yet chemoresistant , while all participant of clinical trials had relapse or progression after standard chemotherapy [ 32 ]  . 
actually there are two phase ii trials ( pediatric match nct03233204 and nct03155620 ) evaluating single agent olaparib in advanced tumors with defects in dna damage repair genes , including stss . 
early results showed good tolerance of the combination and in 22 patients evaluable for response 18% partial responses ( synovial sarcoma , leiomyosarcoma ) and 23% stable diseases ( liposarcoma , ewing sarcoma , solitary - fibrous - tumor , malignant peripheral nerve sheath tumor ) [ 35 ]  . parpi andirradiation ionizing radiation causes damage mainly through interaction with dna , leading to strand breaks and nucleotides damage . 
thus , there is a strong rationale in multimodal treatments combining parpi and radiation therapy ( rt ) , with described median enhancement ratio from 1 , 3 to 1 , 5 [ 4 ]  . 
the effect is greater in highly proliferating tumor cells and could be enhanced in cancers harboring defects in hr and by synthetic lethality mechanis combined treatment is of great interest in stss due to presence of genetic alteration amplifying parpi effect , moreover rt is part of standard treatment in intermediate / high - grade stss and locally advanced disease [ 12 ]  . 
the radiosensitizing effects can be observed at much lower olaparib doses than the single agent effect , suggesting a crucial role to the increased requirement of parp activity after radiation . 
in lung and pancreatic cancer cell lines combined treatment increases expression of h2ax and 53bp1 foci and upregulates expression of phosphorylated atm , atr and their respective kinases [ 39 ]  . 
either in cell culture studies or in tumor - bearing animal experiments , the primary effect of the combination treatment almost uniformly reflected growth arrest rather than cell death with little or no contribution from apoptosis , as confirmed by demonstrating that radiosensitization is not altered by caspase inhibition . 
however , the possible recovery of senescent cells and re - entry into cell 1 3 la radiologia medica ( 2019 ) 124 : 282289 cycle after prolonged arrest could lead to tumor recurrence [ 45 ]  . parpi andirradiation instss combined treatment of rt and parpi has showed radiosensitization with olaparib in ewing sarcoma , leading to synergistic increases in apoptosis and cell death in a ewsfli1 dependent manner , as shown using the comet assay . 
in addition , in a xenograft model olaparib in combination with a single dose of ionizing radiation ( 4gy ) showed delayed tumor growth ; examination of treated tumors demonstrated profound effects on dna damage , apoptosis , and proliferation [ 46 ]  . 
moderate radiosensitization in ewing sarcoma was observed also with rucaparib [ 47 ]  . our group is working on combination of radiation with olaparib , iniparib and veliparib in four human cell lines of stss ( fibrosarcoma , liposarcoma , leiomyosarcoma and rhabdomyosarcoma )  . 
in brain , veliparib ( 200mg bid ) in combination with whole brain rt ( wbrt ) in patients with metastases demonstrated an adverse event profile similar to that of wbrt alone [ 49 ]  . 
however , data are not univocal and in a phase i study on glioblastoma , association of veliparib with radiotherapy and temozolomide was found unsafe because of hematologic complications [ 50 ]  . 
in thorax , a phase i study with veliparib and rt on loco regional radiotherapy for local recurrence of triple negative breast cancer , showed comforting safety data [ 52 ]  . 
a phase i study of veliparib in combination with low - dose fractionated whole abdominal radiation therapy ( ldfwar ) in patients with peritoneal carcinomatosis demonstrated that combined treatment is a tolerable regimen with primary toxicities of myelosuppression , fatigue and gastrointestinal symptoms . 
 these studies suggest that olaparib might be a carcinogen and warrant further investigations [ 55 ]  . conclusions in conclusion , parpi are promising agents that can give advantages in stss treatment , alone or in multimodal therapies . 
notably , radiosensitizing activity of parpi is of great interest due to the large use of rt in standard protocols of stss and to the presence of genetic alteration amplifying parpi effect . 
the morphologic diagnosis of sarcoma relies on the evaluation as well as the integration of four main features : the shape of the neoplastic cells ; the pattern of growth ; the quality of the background ; the architecture of the vascular network . 
molecular genetics is increasingly used for diagnostic purposes to distinguish specific subtypes of sarcomas , to support diagnosis in non - canonical clinical presentations and also to distinguish true sarcomas from benign mimickers . 
with many exceptions , histologic typing does not provide sufficient information for predicting the clinical course of the disease and , therefore , grading systems based on histological parameters were introduced to provide a more accurate estimation of the degree of malignancy of tumors . 
 the three - tiered system devised by the french federation of cancer centers sarcoma group ( fnclcc ) systems is widely adopted ; however , several limitations exist that have led to the development of prognostic nomograms that incorporate the specific histotype as one of the relevant parameters . keywords soft tissue sarcoma immunohistochemistry molecular genetics introduction soft tissue sarcomas represent a heterogeneous group of rare malignancies with an overall incidence of around 5 / 100 , 000 / year . 
half of the cases occur in the limbs ( wherein the thigh is by far the commonest site ) , 30% occur intra - abdominally ( including the retroperitoneum ) , and 15% arise in the trunk and in the head and neck region . 
to avoid major mistakes , careful evaluation of clinical presentation and integration of immunohistochemistry and molecular genetics whenever relevant are mandatory . soft tissue sarcomas are currently classified on the basis of the 2013 who classification of soft tissue tumors [ 2 ]  . 
who classifies the different entities on the basis of vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2019 ) 124 : 266281 histomorphology and includes all available immunophenotypic and genetic data since the 2002 edition [ 3 ]  . 
the major advances introduced since 2002 can be summarized as follows : adipocytic tumors one of the major changes introduced since 2002 is represented by the use of a stricter terminological definition of well - differentiated liposarcoma , which represents the commonest of liposarcoma subtypes . 
it has been clarified that the terms atypical lipomatous tumor and well - differentiated liposarcoma are synonyms and that the latter term should only be used for lesions that occur in the retroperitoneum / mediastinum or in other anatomic sites where complete resectability is unachievable . 
the use of the term atypical lipomatous tumors for resectable lesions is justified by the fact they never recur and are most often cured by complete ( even marginal ) surgical excision . 
in 2002 , it was recognized that in dedifferentiated liposarcoma ( defined as morphological progression from well - differentiated liposarcoma to high - grade non - lipogenic sarcoma ) , also a low - grade dedifferentiation can be observed . 
to reflect the fact that both lesions actually represent the ends of a morphological spectrum of a genetically distinct histology , in 2002 myxoid and round cell liposarcoma merged in one single entity . 
in 2013 , the term round cell liposarcoma was eliminated and replaced by the label high - grade myxoid liposarcoma to underline the fact that clinical outcome depends on the amount of hypercellularity and not on the shape on neoplastic cells that can be either rounded or spindled . fibroblastic / myofibroblastic tumors a key conceptual change was represented by the inclusion of hemangiopericytoma ( hpc ) since 2002 within the chapter on solitary fibrous tumor . 
at that time , it was already clear that hpc merely represented a collection of unrelated , benign as well as malignant , sharing an hpc - like vascular network ( i.e. , the presence of dilated , thin - walled , branched blood vessels ) fig.1. 
as a logical consequence of this conceptual evolution in 2013 , the label hemangiopericytoma table 1 intermediate ( locally aggressive and / or rarely metastasizing ) and malign soft tissue tumors recognized by 2013 who classification of soft tissue tumors intermediate adipocytic tumors atypical lipomatous tumor / well - differentiated liposarcoma malignant adipocytic tumors dedifferentiated liposarcoma myxoid liposarcoma pleomorphic liposarcoma intermediate fibroblastic / myofibroblastic tumors superficial fibromatosis desmoid - type fibromatosis lipofibromatosis giant cell fibroblastoma dermatofibrosarcoma protuberans and variants solitary fibrous tumor inflammatory myofibroblastic tumor low - grade myofibroblastic sarcoma myxoinflammatory myofibroblastic tumor infantile fibrosarcoma malignant fibroblastic / myofibroblastic tumors adult fibrosarcoma myxofibrosarcoma low - grade fibromyxoid sarcoma sclerosing epithelioid fibrosarcoma intermediate so - called fibrohistiocytic tumors plexiform fibrohistiocytic tumor gant cell tumor of soft tissues malignant smooth muscle tumors leiomyosarcoma malignant skeletal muscle tumors embryonal rhabdomyosarcoma alveolar rhabdomyosarcoma pleomorphic rhabdomyosarcoma spindle cell / sclerosing rhabdomyosarcoma intermediate vascular tumors kaposiform hemangioendothelioma retiform hemangioendothelioma papillary intralymphatic angioendothelioma composite hemangioendothelioma pseudomyogenic ( epithelioid sarcoma - like ) hemangioendothelioma kaposi sarcoma malignant vascular tumors epithelioid hemangioendothelioma angiosarcoma of soft tissue malignant chondro - osseous tumors extraskeletal mesenchymal chondrosarcoma gastrointestinal stromal tumors malignant nerve sheath tumors malignant peripheral nerve sheath tumor 1 3 268 table 1 ( continued ) epithelioid malignant peripheral nerve sheath tumor malignant triton tumor malignant granular cell tumor ectomesenchymoma intermediate tumors of uncertain differentiation hemosiderotic fibrolipomatous tumor atypical fibroxanthoma angiomatoid fibrous histiocytoma ossifying fibromyxoid tumor mixed tumor myoepithelioma myoepithelial carcinoma phosphaturic mesenchymal tumor malignant tumors of uncertain differentiation synovial sarcoma epithelioid sarcoma alveolar soft parts sarcoma clear cell sarcoma of soft tissues extraskeletal myxoid chondrosarcoma ewing sarcoma desmoplastic small round cell tumor extra renal rhabdoid tumor pecoma intimal sarcoma undifferentiated / unclassified sarcoma undifferentiated spindle cell sarcoma undifferentiated pleomorphic sarcoma undifferentiated round cell sarcoma undifferentiated epithelioid sarcoma la radiologia medica ( 2019 ) 124 : 266281 organized in a perivascular pattern of growth survives within the label myopericytoma . fibrosarcoma also experienced a significant remodeling . 
whereas it is currently recognized that most superficially located fibrosarcomas actually represent examples of fibrosarcomatous dermatofibrosarcoma protuberans ( fs - dfsp ) , infantile fibrosarcoma is confirmed as a clinically , pathologically and , genetically distinct entity . 
these are low - grade fibromyxoid sarcoma , myxoinflammatory fibroblastic sarcoma , sclerosing epithelioid fibrosarcoma , and low - grade myofibroblastic sarcoma . socalled fibrohistiocytic tumors the same destiny of hpc occurred to malignant fibrous histiocytoma ( mfh ) who also totally disappeared in 2013 . 
as of today pleomorphic mfh , once the most commonly diagnosed sarcoma , is now synonymous with high - grade undifferentiated pleomorphic sarcoma and it should not exceed approximately 5% of newly diagnosed sarcomas . 
the so - called giant cell variant of mfh appears to be an heterogeneous collection of clinically as well as morphologically distinctive lesions that includes giant cell tumor of soft tissue , extraskeletal osteosarcoma , and spindle cell sarcoma ( most often leiomyosarcoma ) featuring osteoclast - like giant cells . 
as its line of differentiation remains unknown , it has also been moved to the category of mesenchymal tumors of uncertain differentiation . the existence of a broader category of undifferentiated sarcomas ( pleomorphic , epithelioid , round cell , and spindle cell ) is now fully acknowledged . 
currently , the original ( still valid ) idea generated by arthur purdy stout of the existence of lesions mainly composed of contractile cells in the last two decades , several new entities have been characterized , particularly in the intermediate malignancy category , including the kaposiform , retiform , and composite hemangioendothelioma . 
since the 2002 who classification epithelioid hemangioendothelioma ( ehe ) 1 3 la radiologia medica ( 2019 ) 124 : 266281 has been reclassified as malignant due to its considerable metastatic rate ranging between 15 and 30% . 
a novel , genetically distinct entity named pseudomyogenic hemangioendothelioma , characterized by multifocality as well as relatively indolent clinical behavior , has also been added to the group of vascular neoplasm of intermediate malignancy . tumors ofuncertain differentiation this category contains tumors without a clear line of differentiation or without a normal cellular counterpart . 
since we now know more about divergent differentiation in various sarcomas subtypes , the category of malignant mesenchymoma is also losing ground as it is currently acknowledged that heterologous differentiation may occur in context of specific entities such as malignant peripheral nerve sheath tumor ( mpnst ) and dedifferentiated liposarcoma . 
the morphologically rather elusive category of intimal sarcoma was introduced as a new entity in this group . principles ofsarcomagenesis the pathogenesis of the vast majority of soft tissue sarcomas is still unknown and most of them arise de novo without an apparent causative factor . 
in rare cases , genetic and environmental factors such as radiation , lymphedema ( secondary angiosarcoma of the breast ) , viral infections ( hhv8 infection is associated with kaposi sarcoma ) , exposure to chemicals ( vinyl chloride is linked to hepatic angiosarcoma ) , and immunodeficiency ( ebv infection in immunodeficient subjects is associated with the development of smooth muscle tumors ) have been identified as risk factors . 
it is broadly accepted that trauma does not represent a predisposing factor and that , at best , it can simply draw attention to the presence of pre - existing mass . genetic susceptibility plays a role in a minority of soft tissue sarcomas . 
the autosomal dominant lifraumeni syndrome ( wherein germline mutations of the tp53 gene occur ) has been shown to predispose to the development of malignant tumors , one - third of which are represented by bone and soft tissue sarcomas . 
recent data have shown that approximately half of patients with sarcoma have putatively pathogenic monogenic and polygenic variation in known and novel cancer genes among which are tp53 , atm , atr , brca2 , and ercc2 [ 4 ]  . in the last two decades , molecular genetics have greatly contributed to elucidate some of the molecular mechanisms associated with the development of soft tissue sarcomas [ 57 ]  . 
good examples are represented by desmoid fibromatosis ( the vast majority of which are associated with mutations of either the ctnnb1 or apc genes ) and gastrointestinal stromal tumors ( most often associated with mutation of the kit and pdgfra genes and far less often of the braf , sdh and nf1 genes )  . 
in this context , particularly relevant is the occurrence of gene copy number alterations as observed in well - differentiated / dedifferentiated liposarcoma , wherein the amplification of the mdm2 , cdk4 and hmga2 genes represents the key driver genetic event . pathologic diagnosis sarcomas are currently classified on the basis of their morphology , their immunophenotype , and their molecular status . 
for practical reasons , the classification scheme follows a histogenetic approach , even though currently it is no longer believed that a given mesenchymal neoplasm actually originates from a mature normal counterpart . 
interestingly , the list of lesions of unknown histogenesis ( i.e. , unknown line of differentiation ) has increased in size , reflecting the uncertainties surrounding the mechanisms of sarcomagenesis . microscopic observation of hematoxylinand eosinstained slides still represents the mainstay of sarcoma classification . 
any other ancillary technique ( immunohistochemistry and / or molecular pathology / genetics ) , even the most sophisticated , certainly represents an important complement to , but under no circumstances a replacement for , classic morphological observation . 
it should be also noted that macroscopic observation too plays a fundamental role , firstly in providing accurate reporting of the status of surgical margins , and secondly in guiding proper sampling and , therefore , posing the milestone for correct classification . 
the diagnosis of sarcoma relies upon the evaluation as well as the integration of four main features : despite the intrinsic challenge of sarcoma diagnosis , is possible to achieve a correct classification in most instances , provided that cases are approached following a rigorous 1 . 
the architecture of the vascular network . this approach possesses the great merit of reducing dramatically the number of diagnostic options , also allowing a rational choice of ancillary immunohistochemical and molecular tests . 
spindle cells are defined by the presence of an elongated cytoplasm , harboring oval nuclei that can be blunt - ended ( as typically seen in smooth muscle tumors ) ( fig.2a ) , tapering ( as seen in myofibroblastic tumors ) or pointed ( as seen most often in neural neoplasm )  . 
neoplastic cells exhibit extreme nuclear pleomorphismultiple prominent nucleoli are seen 1 3 la radiologia medica ( 2019 ) 124 : 266281 table 3 intermediate and malignant soft tissue neoplasm featuring spindle cell morphology table 5 malignant soft tissue neoplasm featuring round cell morphology dermatofibrosarcoma protuberans ( dfsp ) fibrosarcomatous dermatofibrosarcoma protuberans giant cell fibroblastoma angiomatoid malignant fibrous histiocytoma low - grade myofibroblastic sarcoma desmoid fibromatosis phosphaturic mesenchymal tumor gastrointestinal stromal tumor ( gist ) leiomyosarcoma solitary fibrous tumor synovial sarcoma infantile fibrosarcoma malignant peripheral nerve sheath tumor ( mpnst ) spindle cell liposarcoma spindle cell and sclerosing rhabdomyosarcoma intimal sarcoma undifferentiated spindle cell sarcoma table 4 intermediate and malignant soft tissue neoplasm featuring epithelioid cell morphology epithelioid sarcoma classic type epithelioid sarcoma proximal type malignant rhabdoid tumor malignant myoepithelioma ( myoepithelial carcinoma ) pseudomyogenic hemangioendothelioma ( can be spindled ) epithelioid hemangioendothelioma epithelioid angiosarcoma epithelioid malignant peripheral nerve sheath tumor clear cell sarcoma of soft parts clear cell sarcoma of gastrointestinal tract ( malignant gastrointestinal neuroectodermal tumor ) sclerosing epithelioid fibrosarcoma alveolar soft part sarcoma pecoma epithelioid pleomorphic liposarcoma epithelioid gist epithelioid myxofibrosarcoma epithelioid leiomyosarcoma epithelioid rhabdomyosarcoma epithelioid inflammatory myofibroblastic sarcoma undifferentiated epithelioid sarcoma 4 . 
soft tissue malignancies featuring a predominantly pleomorphic morphology are listed in table6 . ewing sarcoma cic - dux4 associated round cell sarcoma bcor - ccbn3 associated round cell sarcoma extraskeletal mesenchymal chondrosarcoma desmoplastic small round cell tumor alveolar rhabdomyosarcoma poorly differentiated round cell synovial sarcoma high - grade myxoid ( formerly round cell ) liposarcoma table 6 malignant soft tissue neoplasm featuring pleomorphic morphology pleomorphic rhabdomyosarcoma pleomorphic liposarcoma dedifferentiated liposarcoma extraskeletal osteosarcoma pleomorphic high - grade myxofibrosarcoma pleomorphic leiomyosarcoma pleomorphic malignant peripheral nerve sheath tumor undifferentiated pleomorphic sarcoma the patterns ofgrowth the pattern of growth of the neoplastic cell population is extremely important as helps to further refine the possible diagnostic options . 
the presence of osteogenic matrix represents prerequisite to the diagnosis of extraskeletal osteosarcoma . the architecture ofthevascular network blood vessels can variably organize to form a plexiform , archiform , and hpc - like architecture . 
 myxofibrosarcoma myxoinflammatory fibroblastic sarcoma low - grade fibromyxoid sarcoma myxoid liposarcoma extraskeletal myxoid chondrosarcoma ossifying fibromyxoid tumor embryonal rhabdomyosarcoma this patter has been variably labeled as chicken wire of crows feet depending on the imagination of the pathologist . 
the lesions associated with an hpc - like vascular network are listed in table8 . as already mentioned , the integration of the abovementioned morphologic features which is enable to reduce significantly the number of diagnostic options to the extent that in some instances ancillary technique may play a rather limited role . 
however , in many situations an accurate diagnosis may require a second step represented by application of a variable ( ideally relatively limited ) number of immunohistochemical stains . immunohistochemical characterization ofsoft tissue tumors immunohistochemical characterization plays a key role in the diagnostic workup of soft tissue sarcomas [ 8 , 9 ]  . 
the number of potential diagnostic markers has grown exponentially through the years ; however in consideration of the natural evolution of the field , some markers have lost their role while others have gained diagnostic relevance . 
it has to be underlined that , with some exceptions that will be discussed , the majority of classic differentiation markers tend to show good sensitivity , however , associated with rather limited specificity . 
to identify myogenic differentiation in dedifferentiated liposarcoma . myogenic differentiation markers classic myogenic markers are basically represented by smooth muscle actin , muscle specific actin , desmin , and h - caldesmon . demonstration of myogenic ( both smooth muscle and striated ) differentiation is clinically relevant in the following situations : 1 . 
to differentiate between rhabdomyosarcoma and nonrhabdomyosarcoma pediatric soft tissue tumors ( those two broad groups definitely undergo distinct systemic treatments )  . table 8 soft tissue neoplasm featuring an hpc - like vascular network benign soft tissue neoplasm featuring an hpc - like vascular network myofibroma / myofibromatosis myopericytoma deep - seated benign fibrous histiocytoma malignant soft tissue neoplasm featuring an hpc - like vascular network solitary fibrous tumor phosphaturic mesenchymal tumor synovial sarcoma extraskeletal mesenchymal chondrosarcoma malignant peripheral nerve sheath tumor infantile fibrosarcoma smooth muscle actin immunopositivity is observed in most smooth muscle tumors but also , in myofibroblastic , myoepithelial and pericytic neoplasmuscle specific actin ( hhf - 35 ) also stains smooth muscle lesions and , however , also represents a very sensitive markers of striated muscle differentiation , staining up to 90% of rhabdomyosarcomas of all subtypes ( embryonal , alveolar , and pleomorphic )  . 
h - caldesmon immunoreactivity is observed in most smooth muscle neoplasin contrast with other smooth muscle markers , it tends to be negative in myofibroblastic lesions as well as in rhabdomyoblastic neoplasm . the most specific and sensitive markers to demonstrate rhabdomyoblastic differentiation remain myogenin ( myf4 ) , a lineage restricted nuclear transcription factor involved in striated muscle differentiation . 
recently , it has been shown that myod1 ( myf3 ) , an alternative nuclear transcription factor involved with the development of striated muscle , represents the most sensitive marker for the spindle cell variant of rhabdomyosarcoma , wherein myod1 gene homozygous mutations have shown to occur . neural differentiation markers paradoxically , the best use of the prototypic schwannian differentiation markers , namely s100 protein , is achieved out of context of recognition of mpnst . 
in fact , approximately 1 3 276 la radiologia medica ( 2019 ) 124 : 266281 only 30% of malignant peripheral nerve sheath tumors ( mpnst ) exhibit s - 100 positivity , which is usually limited to less than 30% of neoplastic cells . 
it has to be stressed that s100 exhibits a distinctive multispecificity to the extent that its evaluation needs to be strictly performed in context with morphology . the best use of s100 immunostains is as follows : 1 . 
recognition of cartilaginous differentiation ( particularly useful to identify focal heterologous component in mpnst and dedifferentiated liposarcoma )  . another member of the group of the intermediate filaments , glial fibrillary acidic protein ( gfap ) is also detectable in schwann cells . 
gfap immunopositivity can also be observed in myoepithelial neoplas sox10 and h3k27me3 ( histone 3k27 trimethylation ) represent more recently introduced markers that can be used in the diagnosis of neural soft tissue neoplassox10 is involved in melanogenesis and schwannian differentiation , and has been proposed as a valid immunohistochemical marker for both melanocytic and neural neoplassox10 tends to immunostain the vast majority of benign neural mesenchymal lesion whereas when dealing with mpnst its sensitivity is much lower , with approximately 20% of cases showing positivity in a minority of neoplastic cells . 
 h3k27me expression tends to be lost in approximately half of mpnst as a consequence of homozygous inactivation of the polycomb repressive complex 2 ( prc2 )  . epithelial differentiation markers any soft tissue neoplasm featuring true epithelial differentiation or epithelioid morphology is characterized by variable expression of epithelial differentiation markers , namely cytokeratin and epithelial membrane antigen ( ema )  . 
epithelial membrane antigen also stains most epithelioid sarcomas , and 90% of synovial sarcoma ( including poorly differentiated ones ) , therefore , representing the most sensitive marker of epithelial differentiation in this context . endothelial differentiation markers demonstration of endothelial differentiation appears crucial when dealing with poorly differentiated vascular neoplasms , in particular epithelioid angiosarcoma that may often lacks overt vasoformative morphology . 
when dealing with vascular neoplasm cd34 is very sensitive , but it has to be stressed that is also expressed in half of epithelioid sarcomas in addition to an endless list of non - vascular spindle cell neoplasms . 
in the recent years , as a byproduct of new insights in the molecular pathogenesis of vascular neoplasm , a number of new diagnostic immunohistochemical markers have been made available . 
fosb expression is consistently observed in pseudomyogenic hemangioendothelioma ( associated with an fosb - serpin1 gene fusion ) as well as in subset of epithelioid hemangioma . melanocytic differentiation markers despite total lack of specificity s100 remains the most sensitive marker of melanocytic differentiation . 
hmb - 45 , melana ( mart1 ) and mitf1 all represent sensitive melanocytic differentiation ; however , their sensitivity drops significantly when dealing with sarcomatoid variants of malignant melanoma , wherein s100 is most often the only expressed diagnostic marker . 
they not only play an obvious role in the differential diagnosis of malignant melanoma , but they have also proved extremely helpful in recognizing the members of the clinically as well as morphologically heterogeneous 1 3 la radiologia medica ( 2019 ) 124 : 266281 family of pecomas , as well in the proper classification of clear cell sarcoma . other useful immunohistochemical markers there exist an increasing number of immunohistochemical markers that despite variable specificity play a major role in the differential diagnosis of soft tissue sarcomas . alk ( anaplastic lymphoma kinase ) cytoplasmic expression of the tyrosine kinase alk plays a key role in supporting the diagnosis of inflammatory myofibroblastic tumor ( imt ) , including the aggressive epithelioid subtypes . 
 unfortunately , approximately half of cases of imt lack alk expression . betacatenin nuclear expression of beta - catenin represents an extremely valuable confirmatory finding in the diagnosis of desmoid fibromatosis . 
nuclear accumulation is due to mutation of the ctnnb1 gene ( found in up to 90% of sporadic desmoid fibromatosis ) or alternatively , of the apc gene ( in the context of gardners syndrome )  . brachyury ( t ) nuclear expression of brachyury represents a key diagnostic feature in the recognition of chordoma and is very helpful in the differential diagnosis with chondrosarcoma , metastatic carcinoma and myoepithelial neoplasms . cd99 when dealing with the differential diagnosis of small round cell sarcomas , cd99 ( a cell surface glycoprotein normally expressed on thymic t cells ) represents a powerful diagnostic marker . 
importantly , immunopositivity in non - ewing tumors tends to be more diffuse , rarely matching the thick membrane staining typically observed in ewing sarcoma . cyclinb3 expression of the cell cycle regulator cyclin - b3 seems to be useful in the recognition of a small subset or poorly differentiated round cell sarcomas associated with a bbcor - cnnb3 gene fusion . sion is consistently observed in malignant rhabdoid tumors ( including atypical teratoid rhabdoid tumors of cns ) as a consequence of ini1 biallelic inactivation . 
loss of ini1 is also observed in up to 95% of both classic and proximal variants of epithelioid sarcoma wherein it tends to be associated with homozygous deletion of the ini1 locus . 
ini1 negativity has been described also in up to 70% of epithelioid mpnst , in 1035% of myoepithelial carcinoma , and in almost all renal medullary carcinoma . kit ( cd117 ) kit represents a tyrosine kinase receptor that is involved on the development of mast cells , melanocytes and interstitial cells of cajal . 
kit expression does not predict response to tyrosine kinase inhibitors and can be observed in unrelated neoplasm such as seminoma , thymic carcinoma , melanocytic neoplasm , and mast cell disorders . mdm2 ( murine double minutes ) mdm2 is the product of the mdm2 proto - oncogene , the main function of which is to promote cell proliferation via inhibition of tp53 . 
 mdm2 overexpression related to gene amplification is also observed in intimal sarcoma and in bone by low - grade osteosarcoma . muc4 ( mucin 4 ) muc4 is a high molecular weight transmembrane glycoprotein normally expressed in epithelial cells . 
the major diagnostic role of muc4 is represented by diagnostic confirmation of both low - grade fibromyxoid sarcoma and sclerosing epithelioid fibrosarcoma , wherein gene expression profiling has identified its upregulation . rb ( retinoblastoma gene product ) rb is the product of the rb tumor suppressor gene that acts as a potent negative regulator of cell cycle . 
the same phenomenon is observed also in atypical spindle cell lipomatous tumor . dog1 ( discovered ongist 1 ) dog1 represents a useful and sensitive marker for diagnosis of gist and is extremely helpful in rescuing at least half of kit - negative gist cases . ini1 ( smarcb1 ) ini1 also known as smarcb1 is a member of the baf molecular complex that contributes to the process of chromatin remodeling and plays a key role in regulating transcription of dna . 
satb2 is best used whenever h&e does not 1 3 278 la radiologia medica ( 2019 ) 124 : 266281 molecular characterization ofsoft tissue tumors tions . discriminate unequivocally between osteoid and sclerotic collagen , or when osteoid is minimally or not represented in the sample . stat6 nuclear expression of stat6 is consistently expressed in all variant of solitary fibrous tumors as a consequence of the nab2 - stat6 gene fusion . tfe3 tfe3 decorates the neoplastic cell population of alveolar soft part sarcoma ( as a consequence , the presence of the aspscr1 - tfe3 gene fusion leads to the overexpression of the tfe3 protein ) , but as other markers it is not entirely specific . 
in fact , it is expressed also in xp11 translocated renal cell carcinomas , in a small subset ( approximately 5% ) of perivascular epithelioid cell tumors ( pecoma ) , and in a small subset of epithelioid hemangioendothelioma . tle1 tle1 is a transcriptional co - repressor that inhibits wnt signaling . 
gene profiling studies have demonstrated high levels of tle1 in synovial sarcoma that can be detected immunohistochemically . wt1 nuclear expression of the c - terminus wt1 ( wilms tumor 1 ) can be used as a confirmatory tool in the diagnosis of desmoplastic small round cell tumor . the marriage of molecular genetics and soft tissue tumor pathology certainly represents one of the most fruitful events of the last decade . 
the close relationship between morphology ( including immunohistochemistry ) and molecular genetics was certified by the 2002 who classifications of bone and soft tissue tumors and further expended in the 2013 update [ 1 , 2 ]  . this integration has impacted on several aspects of pathology [ 1012 ] : 1 . 
as an example , the identification of the fosb - serpine1 gene fusion in pseudomyogenic hemangioendothelioma has greatly contributed to the credibility of this newly identified entity [ 13 ]  . 
the merging of myxoid liposarcoma and round cell liposarcoma into a single entity has been certainly supported by the detection in both lesions of the same rearrangement involving the chop gene . improvement ofdiagnostic accuracy from the diagnostic standpoint in the last two decades , it has become clear that molecular testing may add diagnostic accuracy in important subsets of challenging soft tissue tumors . 
their occurrence can be routinely assessed for diagnostic purposes via fish and / or pcr - based techniques . the diagnostic utility of molecular genetics can be best exemplified in the following situations : 1 . 
distinguishing sarcomas from benign mimickers . distinguishing specific subtypes of sarcomas the distinction of specific sarcoma subtypes is becoming increasingly important as more specific local as well as systemic treatments are being developed . 
round cell sarcomas include ewing sarcoma , desmoplastic small round cell tumor ( dsrct ) , alveolar rhabdomyosarcoma , poorly differentiated round cell synovial sarcoma ( pdss ) , cic - rearranged and bcor - rearranged undifferentiated round cell sarcomas and a minority of cases or high - grade liposarcoma featuring a round cell morphology . 
 1 3 la radiologia medica ( 2019 ) 124 : 266281 the demonstration by fish of ewsr1 , ss18 and foxo1 rearrangements in ewing sarcoma , rms and pdss , respectively , or , alternatively , of specific chimerical transcripts by pcr - based techniques or via an ngs - based approach , is of great help for achieving a correct diagnosis . 
as far as fish analysis of the ewsr1 gene is concerned a major caveat is represented by the fact that its rearrangement can occur in a variety of unrelated lesions . 
as a consequence , any result needs to be mandatorily interpreted in context with morphology and immunohistochemical findings . the identification of gene copy number variations has also proved extremely helpful . 
the perfect example is represented by dedifferentiated liposarcoma , a pleomorphic mostly ( but not exclusively ) retroperitoneal adipocytic malignancy that , in contrast with other sarcoma such as leiomyosarcoma , exhibits the tendency to recur locally with a comparatively lower rate of metastatic spread . 
in this context , the detection of mdm2 amplification by fish or quantitative rtpcr certainly represents a useful diagnostic adjunct [ 15 ]  . supporting diagnosis in noncanonical clinical presenta tions as a result of the widespread use of molecular pathology as a confirmatory diagnostic tool , the range of clinical presentations of many entities has broadened . 
molecular genetics has undoubtedly greatly contributed for instance to the identification of primary ewing sarcoma of the skin , kidney , and meninges , as well of synovial sarcomas occurring at visceral sites such as the lungs and the gastrointestinal tract . distinguishing true sarcomas from benign mimics as already mentioned , the morphological appearance of mesenchymal lesions not always reflects the clinical behavior . 
this is particularly true when dealing with lowgrade fibromyxoid sarcoma ( lgfms ) , a deceptively bland looking spindle cell mesenchymal malignancy characterized by an aggressive clinical behavior on long - term basis . 
the differential diagnosis of lgfms includes benign lesions such as perineurioma , neurofibroma , cellular myxoma , and nodular fasciitis , as well locally aggressive neoplasms such as desmoid fibromatosis . 
even if muc4 expression is currently regarded as a key diagnostic feature , the identification of fus rearrangement via interphase fish or the identification of either fus - creb3l2 or fus - creb3l2 transcripts represents an extremely useful diagnostic tool [ 16 ]  . 
 as mentioned , desmoid fibromatosis enters the differential diagnosis and it should be , therefore , noted that in addition to immunohistochemical detection of nuclear accumulation of - catenin , mutational analysis of the ctnnb1 gene may also represent a valuable diagnostic tool [ 17 ]  . identification ofmolecular predictive andprognostic markers during the last decade , several attempts have been made to determine the prognostic value of molecular genetic findings . 
both factors may unfortunately hamper a large - scale clinical application of cinsarc . an extremely important , clinically relevant exception is represented by gastrointestinal stromal tumors ( gist ) , wherein the type of mutations involving both the kit and pdgfra genes are associated with distinctive outcomes [ 19 ]  . 
 as examples , it is now well known that deletions occurring at the exon 11 of the kit gene are associated with more aggressive disease , whereas mutations of exon 18 of the pdgfra gene generally identify a more indolent clinical course . 
distinct mutation types reflect different objective response rates ( greater for kit exon 11 mutation and much lower for the so - called wild - type gist ) as well as different progression - free survival and overall survival . 
mutational analysis in gist impacts also over dose selection : in fact the progression - free survival of gist patients with kit exon 9 mutations is known 1 3 280 la radiologia medica ( 2019 ) 124 : 266281 to be significantly better in patients treated with 800mg of imatinib as compared to 400mg per day . it has also to be stressed how molecular pathology / genetics represents the most valuable tool in order to identify and validate new therapeutic targets . 
good examples are represented by alk in inflammatory myofibroblastic tumor [ 20 ] , mdm2 and cdk4 in dedifferentiated liposarcoma , the mtor pathway in malignant pecoma and lymphangioleiomyomatosis , pdgfb in dermatofibrosarcoma protuberans [ 21 ] , kdr in angiosarcoma , ntrk3 in gist [ 22 ] , and csf1 in giant cell tumor of tendon sheath [ 23 ]  . the grading ofsoft tissue sarcomas soft tissue sarcomas tend to behave aggressively and metastasize in a large percentage of cases . 
tumor size , location , depth , and histological type are all prognostic factors in terms of metastatic risk and overall survival . with many exceptions , histologic typing does not provide sufficient information for predicting the clinical course of the disease and , therefore , grading systems based on histological parameters were introduced to provide a more accurate estimation of the degree of malignancy of tumors . several different grading systems have been developed . 
 the most successful have been the three - tiered systems of the national cancer institute ( nci ) and the french federation of cancer centers sarcoma group ( fnclcc ) scheme . 
as summarized in table9 , each parameter generates a score the sum of which determines a final score that assigns the tumor to one of the three groups . prognostic nomograms that recently have incorporated the revised who classification of soft tissue tumors represent an additional valuable clinical tool [ 26 ]  . 
from one of these monograms , a freely downloadable application for portable devices termed sarculator has been also generated . in conclusion , soft tissue sarcomas represent a heterogeneous group of clinicopathologic distinct tumor entities . 
both immunohistochemistry and genetics have proved extremely valuable not only in increasing diagnostic accuracy , but also in refining classification and validating newly described tumor entity . table 9 fnlcc grading system tumor differentiation score 1 sarcoma closely resembling normal adult mesenchymal tissue sarcoma for which histologic typing is certain in myxoid variants expression may be weaker score 2 score 3 mitotic count score 1 score 2 score 3 tumor necrosis score 0 score 1 score 2 histologic grade grade 1 grade 2 grade 3 09 mitoses / 10hpf 1019 mitoses / 10hpf 20 mitoses / 10hpf no necrosis < 50% tumor necrosis > 50% tumor necrosis total score : 2 to 3 total score : 4 to 5 total score : 6 to 8 funding this study was not funded . compliance with ethical standards conflict of interest ap dei tos has received speaker honoraria from pfizer , lilly oncology ; pharmamar . 
first , because the imaging alone usually is not able to ensure a definitive diagnosis , ir has a basic role in the staging : the percutaneous biopsy is infact an irreplaceable step . 
furthermore , the proved safety and effectiveness of ir in a multiple oncologial applications prompt a wider use also in this field . keywords soft - tissue lesions sarcomas desmoid lesions interventional radiology biopsy introduction biopsy soft - tissue lesions are rarely encountered and belong to a large and heterogeneous group of different pathologies . 
the imaging features are of complex interpretation and since it is often difficult to accomplish a final diagnosis based on imaging alone [ 2 , 8 , 9 ] , biopsy becomes mandatory to obtain a histological diagnosis [ 24 , 10 ]  . in the last years , the field of pathological anatomy has tremendously developed . 
histological examinations as well as biochemical and molecular studies ( biomarkers ) play a capital role in the diagnosis and management of the great variety of lesions , in particular in the oncological field . 
once the diagnosis has been accomplished , the oncologist needs to know the biological features of the neoplastic tissue to step forward in the complex process of therapeutic decision - making . 
in fact , a successful biopsy mainly depends on the quality of its execution [ 11 ] ; also the surgical strategy depends on the technical success of a biopsy . 
 the extraction of the tissue represents a crucial process : if necrotic or healthy tissues are taken instead of vital and vol . : ( 0123456789 ) 1 3 254 la radiologia medica ( 2019 ) 124 : 253258 pathological ones , the procedure is useless or even harmful for the patient [ 12 ]  . 
nevertheless , only the radiologist has the possibility to choose among other techniques ( mri in particular ) and has familiarity with all the diagnostic imaging tools available . an interesting discussion is going on about the opportunity of performing an incisional biopsy ( ib ) and / or a core needle biopsy ( cnb ) [ 1315 ]  . 
 on other hand , cnb is a percutaneous procedure through which it is usually possible to obtain the right quantity of tissue to perform both histological examinations and molecular studies . 
cnb is performed in the radiological department under us , ct , fluoro or mr guidance thanks to specific needles that allow reaching of the lesions deeply located in the tissues with a minimum impairment of the structure . 
 complications are the same as encountered during ib , but with lower frequency ( from 0.1 to 10% , usually inferior to 5% ) [ 14 , 16 ]  . 
the same authors suggest a flowchart for the biopsy of soft tissue : ib is reserved only in limited cases ( lesions of the limbs ) in which the ( already performed ) cnb has resulted not diagnostic . 
they in fact , suggest the use of imaging - guided cnb as first choice for biopsy in the bone and soft - tissue lesions both in the spine and in the limbs . 
unlike lesions in the limbs , for the lesions located in the spine , if the first biopsy is not diagnostic , a second extraction must be performed under ct guidance , but with intraoperative frozen sections . 
in conclusion , ib should be performed only when a second extraction is required to obtain the final diagnosis , after a first , scarcely diagnostic cnb but only when we are studying soft - tissue lesions of the limbs . 
in another study [ 11 ] , the authors suggest that the diagnostic accuracy of cnb is better in case of metastatic lesions than in case of primitive ones . in conclusion , the stage of a soft - tissue lesion is defined with biopsy . 
with the exception of particular cases , the best cost - effectiveness ratio is obtained using imaging - guided cnb performed by an interventional radiologist . treatments the management of soft - tissue lesions is mainly surgical [ 24 ]  . 
nevertheless , ir can nowadays rely on a great variety of effective and safe treatments of ablation , such as radiofrequency , microwaves , cryoablation , focused ultrasounds , etc . , that are employed to treat lesions with homogeneous necrosis and extremely defined margins [ 1723 ]  . 
the safety profile of these treatments is very high because , apart from the optimal control in releasing energy , multiple systems to control the sensitive structures are available [ 28 ] : there are thermocouples to monitoring the temperature reached near sensitive structures or it is possible to move these sensitive structures , far from the region of ablation thanks to injection of air , carbon dioxide , saline or glucosate solutions . 
finally different complications , like bleeding , that can occur during the treatment could be managed immediately in the ir department [ 29 ]  . in addition , the endovascular treatments can be employed in the management of soft - tissue lesions . 
the second advantage is represented by the injection of a chemotherapeutic drug during the embolization ( chemoembolization ) that can increase the effectiveness of the drugs ( when administered systematically through a peripheral vein ) and leads to a better quality of life and longer relapse intervals [ 31 ]  . among the soft - tissue lesions , those well vascularized are particularly suitable for treatment with chemoor simple embolization : this technique consists in the puncture of a peripheral artery ( usually femoral or radial artery ) and the navigation of the arterial system until the vessels that feed the lesion : there it is possible ( thanks to specific material such as microcoils , glue or microparticles ) to occlude the vessels to obtain an ischemic necrosis of the lesion . some experiences were described for both the aims stated above : in particular a preoperative embolization 1 3 la radiologia medica ( 2019 ) 124 : 253258 of highly vascularized lesions reduces the perioperative risks and the size of the lesion , thus making the surgical intervention more complete and effective [ 32 ]  . 
the use of embolization as therapy for unresectable lesions [ 31 ] , in particular soft tissue sarcomas also was described and proved as effective : in particular , the selective transarterial chemoembolization , when performed as therapy for unresectable lesions seems to be very effective in terms of decreasing cancer pain and increasing tumor relapse intervals ; even if the authors of this study stated some limitations like a small cohort of patients and short followup , no complications were recorded and so this treatment can be considered also safe . among the ablative treatments instead [ 32 ] , one possible application of ir is represented by the treatment of desmoid tumors , where it has proven to be safe and effective [ 7 , 17 , 32 , 33 ]  . 
first , it gives the possibility to treat even large and multiple lesions in one session , creating a large area of ablation , with low risks of spreading the pathological cells . 
in case they are symptomatic and / or enlarged on serial exams , ablation can be considered as non - surgical treatment to control the disease [ 7 ]  . another field of application of ir is represented by the treatment of venous malformations or low - flow vascular malformations . 
these different types of soft - tissue lesions can be treated by ir as alternative to the injection of sclerosing agents currently widely accepted as first - line treatment [ 34 ]  . 
t1w fat sat follow - up 1 year after treatment with the disappearance of the lesions ( mrgfus ) [ 37 ] have proven to be safe and effective tools to control venous malformations or low - flow vascular malformations . 
the main advantage of ir over the injection of sclerosing agents is the possibility of visualizing the lesion during the treatment . finally , the keloid represents a further field of application of ir [ 7 ] , even if its use , however , is still under investigation and further research studies are needed . ir appears to be useful also in the treatment of soft tissue sarcoma ( sts ) [ 3 , 4 , 6 ] , a group of extremely heterogeneous neoplasms ( more than 100 sarcoma subtypes have been identified ) of mesenchymal origin that occur mainly in the soft tissue ( 80% ) and in the bone ( 20% )  . 
due to their rarity ( as said above , less than 1% of all cancers in the adult ) , specific groups of specialists have been created to develop an appropriate service for management ( sarcoma groups )  . 
radiotherapy and chemotherapy play a role also as neo - adjuvant treatments to reduce the size of the lesion and to allow a more effective and complete surgical treatment [ 3 , 6 ]  . 
to date , the role of ir is limited to the management of local recurrence or metastases : in selected cases , as for example in the oligometastatic disease , radiofrequency or cryoablation may be performed to prolong remission or reduce symptoms [ 3 , 4 , 17 , 38 ]  . finally , ir can represent a very useful and effective tool in cases of relapse of soft - tissue malignant lesions after surgery . 
in fact , should this event occur , because the malignant nature of the nodules can only be suspected on the imaging of follow - up , will be certainly not easy for the surgeon to propose to the patient an additional invasive treatment to remove lesions suspected for relapse . 
in these cases , ir may represent a valid solution : by means of ablation , in fact , it is possible to destroy the suspected nodules with a minimally invasive and repeatable procedure . 
 we employed cryoablation with excellent results in terms of complications ( none ) and control of disease in a long - term follow - up study ( 2years )  . conclusions the ir is growing up and consolidating its role in the management of the soft - tissue lesions . 
first , in fact , during the pathway towards the diagnosis , the imaging - guided biopsy is an irreplaceable step ( in particular an imaging - guided 1 3 la radiologia medica ( 2019 ) 124 : 253258 core needle biopsy , as the scientific evidence underlines )  . 
 moreover , in the therapeutical pathway , even if the surgery is considered the gold standard therapy , there are two types of procedures that are demonstrated safe and effective : the embolization , to reduce the risk of bleeding during surgery and to make the surgical procedure safer and easier and the ablation of the metastasis and of the relapses of lesions during the follow - up , to reduce the invasiveness of re - intervention procedures . compliance with ethical standards funding this study was not funded . conflict of interest all authors declare that they have no conflict of interest . ethical approval this article does not contain any studies with human participants performed by any of the authors . la radiologia medica ( 2019 ) 124 : 315322 radiotherapy radiotherapy foroligometastatic cancer : asurvey amongradiation oncologists oflombardy ( airolombardy ) , italy barbaraalicjajereczekfossa1 , 2 barbarabortolato3 mariannaalessandragerardi1 virginiamariaarienti3 stefaniaberlinghieri4 stefanobracelli5 michelabuglione6 mariangelacaputo7 gianpierocatalano8 luigifrancocazzaniga9 luigidecicco5 nadiadimuzio10 francescoromeofilippone9 andreifodor10 davidefranceschini11 paolofrata4 stefaniagottardo2 , 15 giovannibattistaivaldi12 antoniolaudati13 stefanomariamagrini6 elisamantero7 ilariameaglia12 saramorlino7 mauropalazzi3 fabiopiccoli9 paolaromanelli1 martascorsetti11 , 14 flaviaserafini13 lucianoscandolaro13 riccardovaldagni2 , 7 , 16 robertoorecchia2 , 17 paoloantognoni15 the lombardy section of the italian society of oncological radiotherapy ( associazione italiana di radioterapia oncologicalombardia , airol ) samanthadicuonzo1 received : 9 october 2017 / accepted : 5 december 2018 / published online : 15 december 2018 italian society of medical radiology 2018 abstract aims to evaluate the use of radiotherapy ( rt ) for oligometastatic cancer ( omc ) among radiation oncologists in lombardy , italy . methods and study design a survey with 12 items regarding data of 2016 was sent to all 34 lombardy rt centers . 
patient data items a total of 15.681 patients were treated in 2016 with external beam rt in 12 responding centers , and 1.087 patients were treated for omc ( 7% )  . 
brain , lymph node , lung , bone , liver and others were the most common treated sites ( 24% , 24% , 22% , 17% , 8% and 5% , respectively )  . 
the vast majority of patients ( 95% ) were treated with image - guided intensity - modulated rt or stereotactic rt . conclusions seven percent of all rt patients in lombardy are treated for omc . 
the initiative of multicenter and multidisciplinary collaboration has been undertaken in order to prepare the platform for prospective and / or observational studies in omc . keywords oligometastatic cancer lombardy radiotherapy survey stereotactic body radiotherapy introduction the concept of the oligometastatic cancer was introduced in 1995 by hellman and weichselbaum for defining a disease stage with a limited number of clinically detectable metastases [ 1 ]  . 
historically , metastasectomy * marianna alessandra gerardi marianna.gerardi@ieo.it extended author information available on the last page of the article has been performed in selected cases of low - burden metastatic cancer showing promising results in numerous series [ 46 ]  . 
new terms like metastasis - directed therapy ( mdt ) and local or lesion ablative treatment ( lat ) have been coined in order to distinguish the radical local strategies aiming to eradicate metastatic cancer cell deposits ( mdt , lat ) from palliative local therapies delivered with aim to alleviate symptoms ( palliative treatment ) [ 37 ]  . 
radiotherapy planning , delivery and verification development have allowed for the irradiation vol . : ( 0123456789 ) 1 3 316 la radiologia medica ( 2019 ) 124 : 315322 of small volumes with extreme precision so the delivery of high ablative doses with limited normal tissues exposure has become feasible . 
indeed , stereotactic radiotherapy is now frequently proposed in oligometastatic cancer patient and provides high local control and , in some cases , long - lasting progression - free and treatment - free intervals [ 79 ]  . 
moreover , the general information on their approach to oligometastatic cancer and the patient - , diseaseand treatment - related variables of the cases treated in lombardy in 2016 were also collected and analyzed . methods andstudy design a survey with 12 items regarding data of 2016 was sent to all 34 lombardy rt centers using emailing list of the lombardy section of the italian society of oncological radiotherapy ( associazione italiana di radioterapia oncologicalombardia , airo - l )  . 
all 13 centers responded to the general items , and 12 centers submitted basic patient / disease / treatment characteristics . specific items results general items five centers ( 5 / 13 , 38% ) consider oligometastatic cancer if number of metastases is less or equal to three metastases , and eight centers ( 8 / 13 , 62% ) define oligometastatic state if the number of metastases is less or equal to 5 . none of the responding centers defines as oligometastatic case a patient with more than five sites of disease . 
one of these three centers is a university - based comprehensive cancer center and two are large university - based general hospitals ( one with a dedicated cancer center )  . primary tumor included lung , prostate , breast , colorectal , kidney and other malignancies in 33% , 21% , 12% , 9% , 6% and 19% of all oligometastatic cancer cases treated with radiotherapy in lombardy in 2016 , respectively . 
although in the whole series , the lung was the most common primary tumor treated in a oligometastatic setting , followed by table 2 general items of the survey with the results from the 13 responding centers general items centers tot ( 13 ) 1 . 
in one high - volume center with particular expertise for gastrointestinal malignancy , colorectal tumor was the most common primary ( 28% of all cases )  . brain , lymph node , lung , bone , liver and others were the most common treated sites ( 24% , 24% , 22% , 17% , 8% and 5% of all sites , respectively )  . 
 liver oligometastases were treated in 3 out of 12 centers ( 25% of all facilities )  . the majority of patients ( 75% ) were treated for one metastasis , while 14% , 4% and 7% patients received radiotherapy to two , three and more than three lesions , respectively . 
in one of these high - volume centers , 33% of all patients treated for oligometastatic cancer received their therapy to more than three lesions . the vast majority of patients ( 95% ) were treated with image - guided intensity - modulated radiotherapy ( imrt ) or stereotactic radiotherapy , and 5% were treated with threedimensional conformal radiotherapy ( 3dcrt ) technique . discussion our survey showed that oligometastatic cancer is frequently treated with radiotherapy in lombardy . 
lombardy , a region of northern italy accounting for approximately 15% 1 3 la radiologia medica ( 2019 ) 124 : 315322 of the total country population ( 10 out of 61 millions of residents ) , hosts 34 radiotherapy facilities with 87 megavoltage units [ 21 ]  . 
oncology network ( rete oncologica lombarda , rol ) is well defined by the local health authorities [ 22 ] , and regular multidisciplinary meetings are held in the majority of hospitals [ 23 ]  . 
however , we think that our report is an important base to create the multi - institutional collaboration able to fully evaluate the role of ablative irradiation in this particular patient population . although radiotherapy is frequently employed in lombardy in the treatment of oligometastatic cancer , our survey shows that the definition of oligometastasis has not been established yet . 
the recent san gallen conference on the management of patients with advanced prostate cancer ( apccc 2017 ) reported that the panel of 60 experts - in - field did not reach consensus on the definition of oligometastatic disease [ 25 ] , although recent studies show the prognostic role of the number of metastasis [ 26 , 27 ]  . 
 sixty - one percent of the panelists voted for a limited number of bone and / or lymph nodes as a clinically meaningful definition of oligometastatic prostate cancer that helps in decision making ( local ablative treatment of all lesions vs systemic therapy ) , whereas the remaining panelists voted for more strict criteria for oligometastatic disease definition ; interestingly 10% of the panelists did not believe that oligometastatic prostate cancer does exist as a clinically meaningful entity at all . 
fourteen percent of panelists voted for two metastases , 66% for three metastases , and 20% of these panelists voted for five metastases as a cutoff for oligometastatic cancer [ 25 ]  . similarly , numerous fractionation schedules are employed for radiotherapy of oligometastatic cancer both in our survey and in the literature series [ 710 , 1219 , 28 , 29 ]  . 
this reflects the lack of consensus , lack of prospectively validated regimens and heterogeneity of clinical scenarios with regards to the treated volume of oligometastases ( ranging from small lymph node to large metastases ) and proximity to critical visceral organs . 
importantly , a significant percentage of oligometastatic patients receive ablative radiotherapy in previously treated areas ; this will require more cautious schedules with lower dose / fraction and lower total dose [ 30 ]  . the vast majority of lombardy centers used advanced technology ( imrt , igrt , stereotactic radiotherapy ) for treatment of oligometastatic patients . 
indeed , low - volume metastatic disease traditionally treated with conventionally fractionated palliative radiotherapy is now being managed by high - precision extreme hypofractionation with ablative / radical intent [ 31 ]  . 
 stereotactic radiotherapy is actually considered a synonym of image - guided extreme hypofractionation ( fraction doses 5gy given in 5 or 8 fractions ) [ 31 , 32 ] , even if originally this term was reserved for stereotactic target localization [ 33 ]  . 
in fact , only one center in our series routinely uses dose / fraction < 5gy to treat oligometastatic cancer , while four centers routinely use dose / fraction > 10gy . 
 only two centers routinely use regimens with more than five fractions . stereotactic radiotherapy differs from conventionally fractionated radiotherapy in terms of physical , technological and radiobiological aspects [ 3134 ]  . 
high doses of radiotherapy have different mechanisms of vascular and endothelial damage , increase in dna lethal harm and decrease in sublethal damage repair leading to major tumor cell death and high anti - tumor effect [ 31 , 35 ]  . 
high local control after stereotactic radiotherapy is constantly reported in all series , with rates exceeding 80% , quite higher than conventionally fractionated radiotherapy results , at low toxicity including mainly mild acute events and isolated g3g4 late events [ 720 , 29 , 3638 ]  . 
in recent series , stereotactic / hypofractionated radiotherapy with vmat has reached similar local control and a low toxicity rate as other techniques [ 39 , 40 ]  . numerous investigators observed favorable long - term outcome after radical local treatment of a selected group of non - small cell lung cancer patients with good performance 1 3 320 la radiologia medica ( 2019 ) 124 : 315322 status presenting with synchronous oligometastatic disease [ 41 ]  . 
such findings prompted the identification of oligometastatic stage in a new tnm staging system [ 42 ]  . apart from surprisingly high local control after stereotactic irradiation , new interaction between radiotherapy and immune system has been described [ 43 ]  . 
irradiation stimulates the release of signals and cytokines recruiting inflammatory cells into the tumor microenvironment like antigen - presenting cells that activate cytotoxic t cell function [ 43 ]  . 
in some rare cases , the anti - tumor effect of radiotherapy has been observed out of the radiation field and this phenomenon has been called abscopal effect [ 43 ]  . 
 these unknown mechanisms have opened a new field of radiotherapy investigation , including combination with new agents , in particular immunotherapy drugs [ 35 , 43 ]  . other new potential roles of stereotactic radiotherapy have been reported . 
for example , recent multicenter , randomized phase 2 study showed that local consolidative local therapy in non - small cell lung cancer patients with three or fewer metastases that did not progress after initial systemic therapy improved progression - free survival compared with maintenance therapy alone [ 44 ]  . 
for prostate cancer lymph node oligometastases , a propensity - scored matched analysis showed improvement in cancer - specific and overall survival with mdt over standard of care [ 46 ]  . 
these results suggest that aggressive local ablative therapy in oligometastatic cancer should be further explored in phase 3 trials . the level of evidence for use of stereotactic radiotherapy in oligometastatic cancer remains low , and the majority of the available studies are retrospective monoor multi - institutional series . 
numerous prospective and controlled trials have been undertaken in the recent years and will help to establish the role of stereotactic irradiation in the scenario of oligometastatic cancer and explore its full potential . 
our initiative showing that oligometastatic cancer is a significant proportion of all radiotherapy - treated patients in lombardy should help to create a platform for retrospective and prospective investigation . conclusions our survey showed that oligometastatic cancer is frequently treated with irradiation in lombardy . 
the initiative of multicenter and multidisciplinary collaboration has been undertaken in order to prepare the platform for prospective and / or observational studies in oligometastatic cancer . acknowledgements we thank the airo - lombardia , for the excellent coordination of the activities through the lombardy centers , and fondazione ieo - ccm . compliance with ethical standards conflict of interest the authors have no disclosure of potential conflicts of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . informed consent this is a survey among radiation oncologists . 
therefore , a matched cohort analysis was performed in high risk soft tissue patients to analyse differences in terms of clinical outcome and toxicity between patients treated with concomitant radio - chemotherapy ( rtct ) and radiotherapy ( rt ) alone . materials and methods for each patient in rt group was selected a patient in the rtct group matching for age , t stage and grading . 
acute and late toxicity were recorded , overall survival , recurrence free survival and distant metastases free survival were analysed and compared between the two groups . results ninety patients were selected , half of patients underwent radio - chemotherapy and half received radiotherapy alone . 
 during the treatment grade 3 dermatitis was recorded in 15 ( 16.7% ) patients , 6 ( 6.7% ) patients associated chemotherapy and during follow up 12 ( 13.3% ) patients developed grade 2 late fibrosis , 3 ( 3.3% ) joint stiffness and 1 ( 1.1% ) patient experienced a bone fracture . 
at the time of analysis 15 ( 16.7% ) patients were dead , 6 ( 6.7% ) patients in the rtct group and 9 ( 10% ) patients in the rt group . 
tailored treatment has to be considered in elderly soft tissue patients to guarantee a better outcome in this high risk and fragile population . keywords soft tissue sarcoma radio - chemotherapy radiotherapy chemotherapy toxicity * daniela greto daniela.greto@unifi.it 1 department ofradiation oncology , azienda ospedaliero universitaria careggi , university offlorence , largo brambilla 3 , 50141florence , italy 2 department oforthopaedic oncology andreconstructive surgery , azienda ospedaliero universitaria careggi , university offlorence , florence , italy introduction soft tissue sarcomas ( stss ) are a rare disease accounting less than 1% of all adult neoplasms [ 1 ]  . 
however , the reported high rate of skin toxicity correlated with the association of radiotherapy and anthracycline - based chemotherapy [ 7 ] , and very few retrospective studies reporting the safety of concomitant treatment in soft tissue sarcoma result in an uncommon use of concurrent radio - chemotherapy in sts patients . 
for these reasons , the use of concurrent adjuvant radio - chemotherapy is infrequent in sts patients . the aim of our study is to compare clinical outcome and toxicity of two cohorts of patients matched for clinical and pathological characteristics treated with the association of radiotherapy and chemotherapy or radiotherapy alone for localised soft tissue sarcoma following upfront surgery . materials andmethods we retrospectively reviewed data from patients treated at our institution for soft tissue sarcoma between 1994 and 2014 . 
patients were eligible for this study in the presence of the following inclusion criteria : ( 1 ) histologically confirmed soft tissue sarcoma treated with upfront surgery ( 2 ) curative resection with negative margins ( 3 ) no evidence of distant metastases at the time of surgery ( 4 ) receiving post - operatively at least 60gy in 2gy fractions as adjuvant treatment with or without concurrent chemotherapy ( 5 ) in patients treated with chemotherapy , administration of at least three cycles of an anthracycline - based regimen , of whom at least one during the radiotherapy course . 
a matched - pair analysis was performed to compare rates of local control ( lc ) , distant metastases - free survival rates ( dmfs ) , overall survival ( os ) and treatment - related toxicities between patients receiving adjuvant radiotherapy ( rt ) and chemoradiotherapy ( crt ) following surgical excision of the primary tumour . for each patient in the crt group , a corresponding pair in rt group was identified by matching for age ( superior or inferior / equal to 65years ) , grading according to fnclcc [ 8 ] and t stage according to tnm classification system for sarcoma [ 9 ]  . 
late toxicity was recorded during followup that was performed every 3months for the first 2years , every 6months for 3years and annually thereafter . chemotherapy chemotherapy was considered associated to radiotherapy if patients received at least one cycle of chemotherapy concurrently to radiotherapy course . 
 five cycles of adjuvant chemotherapy were the therapeutic standard before 2012 , thereafter three cycles were administered when the italian sarcoma group and the spanish sarcoma group published a randomised clinical study demonstrating that three cycles of preoperative chemotherapy were not inferior to three preoperative cycles followed by two post - operative cycles of chemotherapy [ 10 ]  . granulocyte colony - stimulating factor was administered day 4 . 
statistical analysis was performed using the sem software ( silex development , mirefleurs , france )  . results patients andtreatmentrelated characteristics one hundred and fifty - eight patients met the inclusion criteria . 
 no significant differences in terms of gender , margin status and radiotherapy dose were found between the two groups . among patients who received chemotherapy , 24 ( 53.3% ) received 5 cycles , while in 21 ( 46.7% ) patients , three cycles were administered . 
none of the variables analysed was found as independent prognostic factor of local relapse at multivariate analysis . a total of 29 patients developed distant metastases , in particular 14 ( 15.6% ) patients in the rtct group and 15 ( 16.7% ) patients in the rt group . 
in the rtct group , among tumourrelated deaths , there were 3 ( 6.7% ) metastatic patients and 2 ( 4.4% ) patients with both local and distant relapse ; in the rt group 2 ( 4.4% ) patients had metastatic disease and 7 ( 15.6% ) patients suffered from both local and distant recurrence . 
 toxicity acute radiotherapy toxicity was recorded during radiotherapy course , and 15 ( 16.7% ) patients developed grade 1 3 la radiologia medica ( 2019 ) 124 : 301308 radioand chemotherapy compared to patients treated with radiotherapy alone for localised soft tissue sarcoma . 
 although our study has some limits such as the retrospective nature , the limited number of patients and the impossibility to analyse the differences between the histological subgroups due to the small population size , it provides a balanced evaluation of the impact of the chemotherapy in adjunction to radiotherapy on the outcome of localised soft tissue sarcoma patients . 
this study is one of the latest that reported the outcome of adjuvant chemoradiotherapy in stss , but before other studies investigated the role of post - operative chemotherapy in the same setting . 
a recent pooled analysis of two eortc phase iii trials [ 14 ] comparing adjuvant anthracycline - based chemotherapy to a control in localised soft tissue patients enrolled a total of 819 patients with a median follow - up of 8.2years. 
 in a large database , analysis included 3422 patients diagnosed with localised high - grade and large tumour ( > 8cm ) [ 15 ] ; the clinical choice to prescribe chemotherapy and / or radiotherapy in the perioperative setting and the clinical benefit of these treatments were investigated . 
at a median follow - up of 49months ( 2872months ) , the 5 - year overall survival was 62.1% in patients treated with radio - chemotherapy compared to 35.7% with surgery alone and 49.4% with radiotherapy or chemotherapy in the perioperative setting ( p < 0.001 ) ; mortality hr was reduced by 37% with radiotherapy and by 24% with chemotherapy . 
grade 3 dermatitis was recorded in 15 ( 16.7% ) patients ; of these , 6 ( 6.7% ) patients received chemotherapy ; local toxicity was developed at a median dose of 56.6gy ( range : 3866 )  . 
in locally advanced soft tissue sarcoma , surgery is the cornerstone of treatment and radiotherapy in preoperative or post - operative setting is complementary to conservative surgery to guarantee a local control comparable to radical surgery [ 12 ]  . the role of adjuvant chemotherapy in localised soft tissue sarcoma is still controversial [ 13 ]  . 
in most cases , randomised studies and retrospective series such as the present study that did not find a significant impact of chemotherapy in perioperative treatment of soft tissue sarcoma analysed a limited number of patients , and it could result in a not sufficient population size to be powered to observe survival difference . 
moreover , soft tissue sarcoma is a heterogeneous disease including more than 50 different histological subtypes with different prognosis and sensibility to chemotherapy ; the absence of subgroup analysis for histological subtypes could not individualise patients with unfavourable histology that could benefit from chemotherapy . 
 future studies with larger population stratified according to histology are necessary to identify high - risk patients who could benefit from chemotherapy . moreover , the caution to administered chemotherapy concurrent to radiotherapy is due to the well - known increased risk of toxicity ; historically , in breast cancer patients , the concurrent administration of anthracyclines with radiotherapy was correlated to high risk of radiation dermatitis and cardiac toxicity ; for this reason , a sequential treatment is preferred [ 16 ]  . 
if on the one hand , the early skin toxicity was well managed with supportive care , the authors correlated the higher late toxicity possibly to the 3d conformal radiotherapy technique that could not spare the dose to the organs at risk . 
the only bone fracture developed at 1year of follow - up occurred in a patient treated with radiotherapy alone ; in this case , a large volume of the femur was included in the treatment volume due to the bone involvement . 
no difference in toxicity was found between the two treatment groups . the acceptable toxicity profile of concurrent radiochemotherapy in this study could be explained first of all because in the 15.6% of patients , radiotherapy was delivered with helical tomotherapy , a high conformal technique that reduced the dose to the organs at risk [ 17 ]  . 
furthermore , with respect to other study that considers tumour size 8cm , in our study , the 22.2% of patients had a tumour smaller or equal to 5cm resulting in smaller treatment volume that correlates with a lower risk of local toxicity [ 18 ]  . 
 finally , to reduce the risk of radiation dermatitis , during the radiotherapy , contouring the treatment volume usually had a 3mm gap from patient surface to decrease the dose to the sk [ 19 ]  . if on the one hand chemotherapy did not affect clinical outcome , age was an important prognostic factor in the population studied . 
it is accepted that the incidence of cancer increases with age due to the summation of genetic and epigenetic mutations during the life that favours the carcinogenesis [ 20 ]  . 
moreover , elderly patients often had larger tumours due to late diagnosis and highergrade tumours probably associated to the higher incidence of genetic aberrations in elderly patients [ 21 ]  . 
surgery is the most important approach in stss , but in elderly population , the decreased performance status and comorbidities that could be associated with postoperative complications sometimes excluded this treatment . 
the authors concluded that elderly patients must be treated with a surgical approach such as the younger patients but that it is necessary to select elderly patients according to specific geriatric scale to guarantee the better approach to this vulnerable population . 
in particular , anthracycline - based chemotherapy increases the incidence of chemotherapy - related toxicity in 1 3 la radiologia medica ( 2019 ) 124 : 301308 elderly patients [ 23 ] , and the investigational use of novel agents with a better toxicity profile could be difficult considering the low presence of elderly patients in clinical targets . 
 the uncommon use of radiotherapy in this population is often correlated to logistical difficulties and patient refusal . in conclusion , this study did not demonstrate an increase in clinical outcome correlated with the administration of adjuvant chemotherapy in high - risk soft tissue sarcoma patients . 
older age is a poor prognostic factor in sts patients , and a tailored approach for elderly patients is necessary to guarantee an increase in clinical outcome in this unfavourable population . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval this article does not contain any studies with animals performed by any of the authors . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2019 ) 124 : 309314 radiotherapy intensitymodulated radiotherapy andhypofractionated volumetric modulated arc therapy forelderly patients withbreast cancer : comparison ofacute andlate toxicities albafiorentino1 fabianagregucci1 gianluisasicignano1 niccologiajlevra1 ruggeroruggieri1 sergiofersino1 stefanianaccarato1 albertomassocco2 stefaniecorradini3 filippoalongi1 , 4 rosariomazzola1 vanessafiglia1 francescoricchetti1 received : 26 january 2018 / accepted : 5 december 2018 / published online : 13 december 2018 italian society of medical radiology 2018 abstract purpose to evaluate the differences between conventional fractionated intensity - modulated radiotherapy ( imrt ) and hypofractionated ( hyport ) volumetric modulated arc therapy ( vmat ) in elderly women affected by early - stage breast cancer ( bc ) in terms of rt - related acute / late side effect . materials and methods between october 2011 and july 2015 , 80 consecutive elderly bc patients were treated with imrt for 5weeks ( 40 patients ) or hyport - vmat for 3weeks ( 40 patients )  . 
for patients receiving imrt or hyport - vmat , a total dose of 50gy ( 25 fractions ) or 40.5gy ( 15 fractions ) was prescribed to the whole ipsilateral breast , respectively . 
regarding late adverse events , only grade 1 skin toxicity was recorded . conclusion the present study showed that whole breast imrt and hyport - vmat are feasible and well tolerated in earlystage bc elderly patients and that hyport - vmat is affected by lower risk of acute and late rt - related side effects . keywords breast cancer elderly intensity - modulated radiotherapy volumetric modulated arc therapy * fabiana gregucci fabianagregucci@gmail.com 1 radiation oncology , cancer care center , ospedale sacro cuore don calabria , via don sempreboni 5 , 37034negrar , verona , italy 2 breast unit , cancer care center , ospedale sacro cuore don calabria , negrar , verona , italy 3 radiation oncology , ludwig - maximilians university ofmunich , munich , germany 4 university ofbrescia , brescia , italy introduction the standard of care for patients with early - stage breast cancer ( bc ) consists of lumpectomy followed by adjuvant whole breast radiotherapy ( rt ) , which results in a significant reduction in ipsilateral breast recurrences and bc - specific mortality [ 1 ]  . 
a recent randomized trial showed that boost delivery reduces the risk of local recurrence at 20years even in elderly patients over 60years of age : the gain is small but statistically significant and is linked to the compromise of an increased local risk of fibrosis [ 2 ]  . 
in recent decades , several randomized trials evaluated the role of hypofractionated vol . : ( 0123456789 ) 1 3 310 la radiologia medica ( 2019 ) 124 : 309314 rt ( hyport ) delivered over a period of 3weeks compared to the standard approach and showed equivalence in local control and survival without increased toxicity [ 35 ]  . 
the cancer and leukemia group b ( calgb ) 9343 trial randomized patients over 70years with er - positive bc to tamoxifen alone or tamoxifen plus adjuvant rt and showed a small but statistically significant reduction in ipsilateral breast tumor recurrence without impact on overall survival ( os ) in patients who received rt [ 8 ]  . 
moreover , elderly patients are more frequently affected by bc with favorable tumor biology and at the same time have a shorter overall life expectancy compared to younger patientstherefore , the potential benefit of adjuvant rt may be obfuscated [ 6 ]  . 
lately , technological and technical improvements in modern radiotherapy , such as intensity - modulated rt ( imrt ) or volumetric modulated arc therapy ( vmat ) , have become widespread available in clinical practice . 
the hypothetical advantages of imrt / vmat over three - dimensional conformal rt are : a better dose distribution within the target volume ( in terms of homogeneity ) and a reduction in high doses to healthy tissues and organs at risk [ 10 ]  . 
 although the new techniques significantly reduce the risk of acute toxicities and allow to deliver the boost simultaneously and integrated ( sib ) , modulated rt techniques are still not considered a standard of care as they have no impact on local control or patients quality of life [ 1113 ]  . 
based on this background , we hypothesized that elderly people , who often suffer from additional comorbidities that can influence rt - related toxicity [ 14 ] , could benefit from modulated rt techniques to reduce rt - related side effects . 
the objective of the present retrospective analysis was to investigate the differences regarding rt - related acute / late side effects between conventional fractionated imrt ( over 5weeks ) and hyport - vmat ( over 3weeks ) in elderly patients . materials andmethods between october 2011 and july 2015 , 80 consecutive elderly patients affected by bc were treated with breast irradiation after breast - conserving surgery : 40 patients received imrt over 5weeks , and 40 patients received hyport - vmat over 3weeks . 
rt began no later than 4weeks after surgery and / or by the end of adjuvant chemotherapy . radiation therapy all patients were immobilized in a supine position ( posiboard frame , civco inc . , orange city , ia , usa ) and underwent a planning computed tomography ( 3mm slide thickness ) without intravenous contrast . 
 a clinical target volume ( ctvbreast ) was obtained encompassing the glandular tissue of the breast , while the planning target volume ( ptvbreast ) was defined by adding a 5mm expansion in the transverse plane and 8mm in cranialcaudal direction to the ctvbreast . 
for patients who received imrt , a total dose of 50gy ( 25 fractions ) was prescribed to ptvbreast , while for patients receiving hyport - vmat 40.5gy ( 15 fractions ) was prescribed to ptvbreast . 
a total dose of 60gy in 25 fractions was prescribed to ptvboost for imrt , and a total dose of 48gy ( 15 fractions ) was prescribed for hyport - vmat . 
all vmat and imrt plans were created using 6 - mv photon beams commissioned for a varian trilogy linac ( varian medical system , palo alto , california , usa )  . 
for planning , approval was required : ptvbreast d95% 47.5gy for imrt and > 38.5gy for hyport - vmat , ptvboost d95% 57gy for imrt and > 45.6gy for hyport - vmat , respectively , a maximum dose ( d2% ) 107% to the ptvboost and a minimum dose to 95% of both ptvs not lower than 95% of their , respectively , prescribed doses . side effects evaluation acute and late side effects were evaluated using the radiation therapy oncology group ( rtog ) / eortc radiation morbidity scoring syste all patients were evaluated weekly during the treatment and every 34months for the first 2years of follow - up and then every 6months . 
 cosmetic results were scored by a four - grade scale ( excellent / good / fair / poor ) according to harris and colleagues 1 3 la radiologia medica ( 2019 ) 124 : 309314 ( harvard cosmetic scale ) , based on breast retraction and fibrosis , skin changes and match line effect [ 15 ]  . factors table 1 patients and tumor characteristics ( n = 80 ) statistical analysis to summarize the most relevant features of the clinical variables , descriptive statistic was performed . 
contingence tables with fishers exact test and chi - squared pearson test were utilized to evaluate on univariate analysis , association between the onset of skin toxicity and the following parameters : age ( < 75 vs 75years ) , breast volume ( < 700 vs 700cc ) and chemotherapy administration . results median follow - up time was 45 months ( range 3470 )  . 
regarding late adverse events , skin toxicity was overall mild without any grade 2 or higher toxicity , but resulted in significantly better outcome for patients treated with hyport - vmat . 
as observed in previous studies [ 17 ] , under - treatment and non - guideline - adherent treatment of elderly patients were recorded following breastconserving surgery , even if adjuvant whole breast rt is considered the standard of care . 
there are a variety of barriers why clinicians may not follow evidence - based recommendations in elderly patients , including the complaints of patients to undergo a time - consuming treatment lasting over a period of 56weeks , the associated comorbidities or the belief that bc may be more indolent in elderly patients [ 6 , 1820 ]  . 
indeed , adjuvant rt showed to decrease significantly the incidence of any recurrence without improving os in women older than 70years , as highlighted by the meta - analysis by the early breast cancer trialists collaborative group ( ebctcg ) [ 21 ]  . 
while two randomized trials demonstrated a modest reduction in local recurrence with no difference in breast cancer - specific survival in elderly women with early - stage estrogen receptor ( er ) - positive tumors receiving tamoxifen , the magnitude of benefit for er - negative tumors remains poorly understood [ 8 , 22 ]  . 
for this reason , the omission of rt as a standard - of - care option for elderly patients has to be evaluated with caution and tumor biology ; comorbidities , performance status and patient - related preferences have to be taken into account . 
over the last decades , several randomized trials showed equivalence of hyport delivered over 3weeks as compared to the standard approach in terms of local control and survival [ 35 ]  . 
nowadays , imrt / vmat is not considered the standard approach , even if they are superior to standard 3d conformal rt in terms of reduction in normal tissues irradiation and optimal target dose distribution [ 1013 , 2328 ]  . 
with this background , the hypothesis of our la radiologia medica ( 2019 ) 124 : 309314 study was that elderly patients , who often suffer from other comorbidities , could benefit from imrt / vmat in terms of reduction in acute and late toxicities . 
although there are some limitations in evaluating different fractionation schedules in terms of toxicity and the modality of the boost ( simultaneous concomitant ) , the 2 schedules represent the oldest ( 50gy in 5weeks ) and the newest ( 40gy in 3weeks ) standard fractionation for breast cancer . 
the present analysis showed the feasibility and tolerability of both techniques for bc patients aged over 70years : ( a ) all patients completed the imrt or hyport - vmat without discontinuation , and ( b ) no acute g3 or higher side effects and no late toxicity of > g1 was registered . 
however , a significant difference in terms of acute and late skin side effects was shown in favor of hyport - vmat , probably due its better dose homogeneity compared to imrt . 
 in fact , in a phase iii study published by morganti and colleagues , 332 patients were treated in three different schedules : historical control group ( standard 3d conformal rt , 50.4gy plus sequential 10gy electron boost , over 6weeks ) ; mara - 1 study ( imrt , 44gy plus concomitant 4gy boost , over 3weeks ) ; and mara - 2 study ( imrt , 50gy plus concomitant 10gy boost , over 5weeks ) [ 29 ]  . 
moreover , in a recent retrospective study , which analyzed the role of hyport in bc patients over 60years , g2 and g3 late skin toxicities were about 20 and 5% [ 30 ]  . 
in the present analysis , acute skin toxicity was very low with 25% and 0% of g2 and g3 for imrt patients and 2.5% and 0% for vmat patients , respectively . 
in fact , dose inhomogeneity was significantly associated with toxicity : in the study of morganti , simplified imrt was used for breast irradiation and 3d conformal rt for the boost , while in the study of lazzari etal . 
regarding the analysis of irradiated volume , larger ptv was associated with a greater risk of acute toxicity , as showed in several published studies [ 14 , 29 , 30 ]  . 
regarding the relationship of age and rt - related side effects , considering the low incidence of toxicity , this study confirmed that age over 75 was not considered a risk factor correlated to toxicity , as showed by several other studies [ 3133 ]  . 1 3 la radiologia medica ( 2019 ) 124 : 309314 conclusion whole breast imrt and hyport - vmat are feasible and well tolerated in elderly bc patients . 
despite its limitations ( small sample size , retrospective nature of the analysis and short follow - up ) , one hypothesis that emerges from this analysis is that in elderly bc patients , regardless of comorbidities and breast volume , hyport - vmat is associated with a lower risk of acute and late rt - related side effects . 
further studies are needed in this context . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . 
cova1 1uco di radiologia , 2uco di anatomia patologica , universit di trieste , ospedale di cattinara , strada di fiume 449 , i - 34149 , trieste , italy correspondence to : f . 
between january 2004 and june 2005 , 516 thyroid nodules in 420 patients ( 181 solitary thyroid nodules and 239 multiple nodules ) were prospectively evaluated with us , colour - doppler us and us - guided fna . 
the sensitivity , specificity , ppv , npv and overall accuracy values of grey - scale us were 46% , 73% , 34% , 82% and 67% , respectively , for solitary thyroid nodules and 35% , 72% , 14% , 90% and 68% , respectively , for multiple nodules . 
thyroid nodules cannot be accurately characterised using grey - scale us or colour - doppler us . key words thyroid nodule ultrasound colour - doppler us fine - needle aspiration biopsy riassunto obiettivo . 
nel periodo tra gennaio 2004 e giugno 2005 sono stati valutati prospetticamente con ecografia , eco - color doppler e agoaspirazione sotto guida ecografica 516 noduli tiroidei in 420 pazienti ( 181 pazienti portatori di un nodulo solitario e 239 pazienti con noduli multipli )  . 
nei pazienti con nodulo tiroideo solitario i valori di sensibilit , specificit , vpp , vpn e accuratezza diagnostica dellecografia in scala dei grigi sono risultati rispettivamente del 46% , 73% , 34% , 82% e 67% . 
thyroid cytology , as well , poses interpretation problems and requires knowledge of the functional status of the thyroid and the hormone status of the patient in order to be correctly interpreted . 
in fact , the approach to a patient with a thyroid nodule is complicated by the fact that no single diagnostic test is sufficiently specific and sensitive enough to allow correct characterisation . 
characterisation of a thyroid nodule requires a multidisciplinary approach based on clinical and laboratory assessment , us , scintigraphy and cytology [ 4 ] , all of which contribute to guiding the diagnosis and treatment decisions . 
 the purpose of this study was to evaluate , in a large , consecutive series of 516 thyroid nodules assessed by colourdoppler us and cytology , the correlation between the diagnosis of benign or malignant nodule at grey - scale and colourdoppler us and the cytological findings . 
la caratterizzazione del nodulo tiroideo richiede infatti un approccio multidisciplinare basato sulla valutazione clinica e laboratoristica , sullecografia , sulla scintigrafia e sulla citologia [ 4 ] che insieme concorrono allorientamento diagnostico , ed alla scelta terapeutica . scopo di questo lavoro stato valutare , su unampia casistica consecutiva di 516 noduli tiroidei studiati con eco - color doppler e con citologia , la correlazione tra la diagnosi ecografica ed eco - color doppler di benignit o di malignit del nodulo e i risultati della citologia . materials and methods between january 2004 and june 2005 , 516 thyroid nodules in 468 patients were prospectively studied with colourdoppler us and fine - needle aspiration ( fna ) cytology . 
the thyroid nodules were solitary in 181 patients ( 29 men , 152 women , age range 2683 years , mean age 56 ) and multiple ( n = 335 ) in 237 patients ( 30 men , 207 women , age range 2985 years , mean age 62 )  . 
 the us studies were carried out with digital us scanners ( technos mp , esaote biomedica , genoa , italy and hdi5000 , atl , washington , usa ) using broadband lineararray transducers ( 510mhz )  . 
as regards grey - scale us , the nodules were evaluated for echogenicity and echostructure , margins , the presence and characteristics of the peripheral halo , the presence of calcifications and their morphology and relationships with surrounding organs . 
per quanto riguarda lecografia in scala dei grigi sono stati considerati lecogenicit e lecostruttura del nodulo , le caratteristiche dei margini , la presenza e le caratteristiche dellalone periferico , la presenza di calcificazioni e la loro morfologia , i rapporti con gli organi contigui . 
in base alle loro caratteristiche i noduli tiroidei sono stati classificati come benigni , sospetti e maligni , secondo i criteri stabiliti in letteratura [ 2 , 59 ]  . 
all nodules show regular margins and a thin regular halo ( ac ) , have an almost entirely cystic ( a ) or predominantly solid hyperechoic echostructure ( b ) , with no calcifications ( a , b ) or with eggshell calcifications ( c )  . 
i noduli presentano margini regolari , alone periferico sottile e regolare ( a - c ) , ecostruttura prevalentemente cistica ( a ) , o prevalentemente solida con iperecogenicit ( b ) , assenza di calcificazioni ( a , b ) o calcificazioni a guscio ( c )  . 
il riscontro di un pattern di tipo i , ii , iv stato considerato segno di benignit , mentre il pattern di tipo iii stato considerato sospetto [ 1012 ]  . tutti i 516 noduli considerati sono stati sottoposti ad agoaspirazione ecoguidata con ago da 2527 g ed aspirazione forzata . 
la valutazione estemporanea stata soggettiva , senza effettuare la colorazione rapida e la visione dei vetrini al microscopio . tutti i noduli solitari della tiroide sottoposti ad agoaspirazione avevano dimensioni maggiori di 6 mi noduli cistici sono stati sottoposti ad evacuazione e ad analisi citologica del liquido aspirato . 
nei pazienti con gozzo multinodulare sono stati sottoposti ad agoaspirato il nodulo dominante e eventuali noduli con caratteristiche sospette allecografia in scala dei grigi e / o alleco color doppler . 
patterns i , ii and iv were considered to indicate benign disease , whereas pattern iii was regarded as suspicious [ 1012 ]  . all 516 nodules underwent fna biopsy with a 25to 27gauge needle and forced aspiration . 
the procedure was carried out by the radiologist in the presence of the cytologist in charge of processing the sample and evaluating its adequacy . immediate evaluation was subjective , without quick staining or viewing of the slides under the microscope . 
thyroid nodule with suspicious us features ( a ) due to the presence of irregular margins and focal absence of peripheral halo ( curved arrow ) ; cytologic findings , benign nodule . 
cytology findings were classified as inadequate , benign , indeterminate , suspicious or malignant , in accordance with published criteria [ 13 ]  . analisi statistica benigni , indeterminati , sospetti , maligni secondo i criteri riportati in letteratura [ 13 ]  . statistical analysis differences in age , gender and cytological diagnosis between the group of patients with solitary nodules and those with multinodular goitre were evaluated by using the mannwhitney test , fishers exact test and the chi - square test ( 2 )  . the reliability of grey - scale us and colour - doppler us in characterising thyroid nodules was assessed by calculating sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy using cytology as the reference study . 
to calculate these values with regard to imaging , all nodules with benign features were considered to be negative ; all nodules with indeterminate or suspicious features were considered to be positive . with regard to cytology , cytologically benign nodules were considered negative , and indeterminate / suspicious or malignant nodules were considered positive . 
this subdivision is in fact arbitrary in that most indeterminate / suspicious lesions feature cells without atypia ; nonetheless , it reflects the need , in clinical practice , to monitor these patients both by using us to detect changes in the size or appearance of nodules and by using serial fna biopsy . 
 le differenze di et , sesso , diagnosi citologica riscontrate nel gruppo di pazienti con nodulo solitario e con gozzo multinodulare sono state valutate utilizzando il test di mannwhitney , il test esatto di fisher , e il test del chi quadrato ( 2 )  . 
lattendibilit dellecografia in scala dei grigi e delleco - color doppler nella caratterizzazione dei noduli tiroidei , utilizzando come indagine di riferimento la citologia , stata valutata calcolando i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) ed accuratezza diagnostica ( ad )  . 
per calcolare questi valori , per quanto riguarda limaging , sono stati considerati come negativi i noduli con caratteristiche benigne ; positivi tutti i noduli con caratteristiche indeterminate o sospetti per malignit . 
diagnosi citologica : nodulo maligno . risultati citologia abbiamo osservato che let media dei pazienti con noduli multipli era significativamente maggiore rispetto allet media dei pazienti con nodulo solitario ( test di mann - whitney , p < 0 , 001 )  . 
sia nei pazienti con noduli multipli che in quelli con nodulo solitario si osservata una netta prevalenza femminile ; tra i due gruppi di pazienti , peraltro , non sono state riscontrate differenze significative nella distribuzione tra maschi e femmine ( test esatto di fisher , p = 0 , 396 )  . sono risultati inadeguati 48 / 516 prelievi per valutazione citologica ( 9 , 3% ) , in particolare , 21 / 181 ( 11 , 6% ) prelievi in pazienti con nodulo solitario e 27 / 335 ( 8 , 1% ) prelievi in pazienti con noduli multipli . 
di questi noduli , 397 sono stati considerati benigni ( 85% ) , 63 sono stati considerati indeterminati ( 13% ) e 8 sospetti per malignit ( 2% )  . 
percentages are given in parentheses cytology solitary nodule multiple nodules inadequate benign indeterminate suspicious for malignancy total inadeguato benigno indeterminato sospetto per malignit totale 21 ( 11.6% ) 123 ( 67.9% ) 32 ( 17.7% ) 5 ( 2.8% ) 21 ( 11 , 6% ) 123 ( 67 , 9% ) 32 ( 17 , 7% ) 5 ( 2 , 8% ) 27 ( 8.1% ) 274 ( 81.8% ) 31 ( 9.2% ) 3 ( 0.9% ) 27 ( 8 , 1% ) 274 ( 81 , 8% ) 31 ( 9 , 2% ) 3 ( 0 , 9% ) tabella 1 agoaspirazione dei noduli tiroidei . 
i valori percentuali sono riportati tra parentesi citologia nodulo solitario noduli multipli cytology ecografia b - mode e eco - color doppler a total of 48 / 516 cytological samples ( 9.3% ) were considered inadequate ; in particular , 21 / 181 ( 11.6% ) samples from solitary nodules and 27 / 335 ( 8.1% ) samples from multiple nodules . 
differences in the distribution of cytological diagnoses among patients with solitary nodules and those with multiple nodules were statistically significant ( 2 = 13.98 , p < 0.003 ) , indicating a prevalence of benign nodules among patients with multiple nodules compared with those with solitary nodules ( table 1 )  . b - mode us and colour - doppler us of the nodules that subsequently underwent aspiration , 330 were considered benign on us ( 110 in patients with a solitary nodule and 220 in patients with multiple nodules ) , whereas 131 were considered suspicious ( 44 and 87 , respectively ) and seven malignant ( six and one , respectively )  . 
of the nodules with benign us appearance , 82% ( 90 / 110 ) of solitary nodules and 90% ( 198 / 220 ) of multiple nodules were found to be benign at cytology . 
of the nodules with suspicious us appearance , 29% ( 13 / 44 ) of solitary nodules and 13% ( 11 / 87 ) of multiple nodules were found to be indeterminate or suspicious at cytology . 
 considering nodules displaying benign features both on us and colour - doppler us , on the one hand , and those displaying suspicious features on either of the two techniques , on the other hand , 83% ( 83 / 99 ) of benign solitary allecografia sono stati considerati benigni 330 dei noduli successivamente aspirati ( 110 in pazienti con noduli solitari e 220 in pazienti con noduli multipli ) , mentre 131 sono stati considerati sospetti ( 44 e 87 rispettivamente ) e 7 maligni ( 6 e 1 rispettivamente )  . 
l82% ( 90 / 110 ) dei noduli solitari e il 90% ( 198 / 220 ) dei noduli multipli con caratteristiche di benignit allecografia in scala dei grigi sono risultati benigni alla citologia . 
il 29% ( 13 / 44 ) dei noduli solitari e il 13% ( 11 / 87 ) dei noduli multipli sospetti allecografia sono risultati indeterminati o sospetti per malignit alla citologia . 
il 71% ( 5 / 7 ) dei noduli maligni allecografia risultato indeterminato o sospetto per malignit alla citologia ( tabelle 2 e 3 )  . se si considerano da una parte i noduli che presentano caratteristiche di benignit sia allecografia che al color doppler , dallaltra tutti i noduli che presentano caratteristiche sospette in almeno una delle due tecniche , l83% ( 83 / 99 ) dei noduli solitari e l89% ( 157 / 176 ) dei noduli multipli benigni allecografia ed al color doppler risultato benigno alla citologia ( tabella 4 )  . 
tuttavia , solo il 34% ( 21 / 61 ) dei noduli solitari e il 11% ( 15 / 132 ) dei noduli multipli indeterminati o sospetti per malignit allecografia associata alla valutazione color doppler risultato indeterminato o sospetto per malignit alla citologia ( tabella 4 )  . attendibilit diagnostica dellecografia b - mode e delleco - color doppler la tabella 5 riporta i valori di sensibilit , specificit , vpp , vpn e accuratezza diagnostica dellecografia in scala dei grigi e dellecografia associata alleco - color doppler dei noduli solitari e dei noduli multipli utilizzando come indagine di riferimento la valutazione citologica . 
comparison of ultrasound ( us ) , colour - doppler us and cytology cytologya ( n = 160 ) ultrasound colour - doppler usb benign suspicious malignant pattern ii pattern iii pattern iv tabella 2 noduli tiroidei solitari : 181 pazienti , 21 dei quali ( 11 , 6% ) con prelievo citologico inadeguato . 
confronto tra laspetto ecografico dei noduli , il quadro eco - color doppler e i risultati della citologia citologiaa ( n = 160 ) ecografia eco - color dopplerb benigno sospetto maligno pattern ii pattern iii pattern iv benign indeterminate suspicious total a21 nodules with inadequate fine - needle aspiration ( c1 ) bno nodule showed a type i colour - doppler us pattern benigno indeterminato sospetto per malignit totale a21 noduli con agoaspirato inadeguato ( c1 ) b nessun nodulo presentava un pattern eco - color doppler di tipo i benign indeterminate suspicious total 22 0 a27 nodules with inadequate fine - needle aspiration ( c1 ) bno nodule showed a type i colour - doppler us pattern benigno indeterminato sospetto per malignit totale a27 noduli con agoaspirato inadeguato ( c1 ) bnessun nodulo presentava un pattern eco - color doppler di tipo i table 3 patients with multiple thyroid nodules : 239 patients , 335 nodules undergoing fine - needle aspiration biopsy , 27 ( 8.1% ) of which had inadequate cytology . 
comparison of ultrasound ( us ) , colour - doppler us , and cytology cytologya ( n = 308 ) ultrasound colour - doppler usb benign suspicious malignant pattern ii pattern iii pattern iv tabella 3 pazienti con multipli noduli tiroidei : 239 pazienti , 335 noduli aspirati , 27 dei quali ( 8 , 1% ) con prelievo citologico inadeguato . 
confronto tra laspetto ecografico dei noduli , il quadro eco - color doppler e i risultati della citologia citologiaa ( n = 308 ) ecografia eco - color dopplerb benigno sospetto maligno pattern ii pattern iii pattern iv 20 1 2 f . 
percentages are given in parentheses imaging cytology solitary nodulea ( n = 160 ) multiple nodulesb ( n = 308 ) benign indeterminate suspicious benign indeterminate suspicious benign suspicious features 83 ( 51.9% ) 40 ( 25.0% ) 15 ( 9.4% ) 17 ( 10.6% ) 1 ( 0.6% ) 4 ( 2.5% ) 157 ( 51.0% ) 117 ( 37.9% ) 19 ( 6.2% ) 12 ( 3.9% ) 0 ( 0.0% ) 3 ( 1.0% ) a21 nodules with inadequate fine - needle aspiration ( c1 ) b27 nodules with inadequate fine - needle aspiration ( c1 ) tabella 4 confronto tra le caratteristiche allimaging dei noduli tiroidei ( ecografia associata ad eco - color doppler ) e i risultati della citologia . 
i valori percentuali sono riportati tra parentesi imaging citologia nodulo solitarioa ( n = 160 ) noduli multiplib ( n = 308 ) benigno indeterminato benigno indeterminato sospetto per malignit sospetto per malignit benigno caratteri sospetti 83 ( 51 , 9% ) 40 ( 25 , 0% ) 15 ( 9 , 4% ) 17 ( 10 , 6% ) 1 ( 0 , 6% ) 4 ( 2 , 5% ) 157 ( 51 , 0% ) 117 ( 37 , 9% ) 19 ( 6 , 2% ) 12 ( 3 , 9% ) 0 ( 0 , 0% ) 3 ( 1 , 0% ) a 21 noduli con agoaspirato inadeguato ( c1 ) b 27 noduli con agoaspirato inadeguato ( c1 ) nodules and 89% ( 157 / 176 ) of benign multiple nodules on us and on colour - doppler us were found to be benign at cytology ( table 4 )  . 
nonetheless , only 34% ( 21 / 61 ) of solitary nodules and 11% ( 15 / 132 ) of multiple nodules that were indeterminate or suspicious on us and colour - doppler us were found to be indeterminate or suspicious at cytology ( table 4 )  . di una specificit compresa tra il 72% e il 73% , sensibilit e vpp sono compresi rispettivamente tra 35%46% e 14%34% . 
la valutazione della vascolarizzazione dei noduli al color doppler comporta un modesto aumento della sensibilit al prezzo di una riduzione della specificit . diagnostic reliability of b - mode us and colour - doppler us discussione table 5 shows the sensitivity , specificity , ppv , npv and diagnostic accuracy of grey - scale us and colour - doppler us for solitary and multiple nodules , using cytological assessment as the reference study . 
colour - doppler us assessment of nodule vascularity moderately increases sensitivity at the expense of specificity . the discovery of one or more thyroid nodules is a frequent occurrence in the general population . 
compresa tra 0 , 3% e 1 , 7% dei noduli nelle casistiche europee [ 3 ] , risulta pi elevata nelle casistiche americane , tra il 9% e il 13% dei noduli sottoposti a valutazione citologica [ 17 , 18 ]  . 
as regards cytology , only nodules classified as benign were considered negative ; all remaining nodules were considered positive solitary nodulea ( n = 160 ) multiple nodulesb ( n = 308 ) ultrasound ultrasound + colour - doppler us ultrasound ultrasound + colour - doppler us sensitivity specificity accuracy a21 nodules with inadequate fine - needle aspiration ( c1 ) b27 nodules with inadequate fine - needle aspiration ( c1 ) sensibilit specificit accuratezza a 21 noduli con agoaspirato inadeguato ( c1 ) b 27 noduli con agoaspirato inadeguato ( c1 ) tabella 5 valori di sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) e accuratezza diagnostica dellimaging ( ecografia ed ecografia associata ad eco - color doppler ) nei pazienti con nodulo solitario e in quelli con noduli multipli , utilizzando come indagine di riferimento la citologia . 
tutti gli altri noduli sono stati considerati positivi nodulo solitarioa ( n = 160 ) noduli multiplib ( n = 308 ) ecografia ecografia + doppler ecografia ecografia + doppler varies in different populations is estimated at 10%41% [ 14 , 15 ]  . 
the incidence of malignancy is similar among patients with solitary nodules and multiple nodules [ 2 , 17 , 18 ]  . the mean age of patients with multiple nodules in our series was significantly higher than that of patients with a solitary nodule , in keeping with the epidemiological data that show that the incidence of thyroid nodules increases with age . the high incidence of nodular thyroid disease and the low prevalence of malignancy call for a diagnostic workup capable of screening the limited number of nodules that require surgery . 
the approach is currently multidisciplinary , based on clinical and laboratory data , ultrasonography , scintigraphy and fna cytology . in patients with a solitary nodule , us permits detection of the nodule and offers guidance for the biopsy . 
its role is more complex in patients with multiple nodules , as only a lalta incidenza dei noduli tiroidei e la bassa prevalenza di malignit rendono necessario un iter diagnostico finalizzato a selezionare un numero limitato di noduli che necessitano di trattamento chirurgico . 
tale iter attualmente multidisciplinare , basato sulla clinica , i dati di laboratorio , lecografia , la scintigrafia e lagoaspirazione con esame citologico . nei pazienti con nodulo solitario lecografia consente lindividuazione del nodulo e la guida al prelievo per lesame citologico . 
il criterio di selezione comunemente utilizzato quello di sottoporre a prelievo per valutazione citologica il nodulo di maggiori dimensioni ; si tratta tuttavia di un criterio arbitrario in quanto diversi studi hanno dimostrato che non esiste correlazione tra le dimensioni del nodulo e la prevalenza di malignit [ 9 , 17 , 18 ]  . 
bench esista infatti una semeiotica ecografica ed eco - color doppler che stabilisce i criteri di benignit e di sospetto del nodulo tiroideo [ 3 , 511 ] , la sua reale attendibilit controversa , e la possibilit dellecografia di diffef . 
the current approach is to sample the largest nodule for cytology ; however , this is arbitrary in that several studies have shown that there is no correlation between nodule size and the prevalence of malignancy [ 9 , 17 , 18 ]  . 
this approach is also controversial . even though us and colour - doppler us imaging criteria exist for distinguishing benign and suspicious thyroid nodules [ 3 , 511 ] , their actual reliability has been questioned , and the ability of us to effectively differentiate benign from malignant thyroid nodules is currently being reconsidered [ 2 , 7 , 8 , 19 , 20 ]  . 
in agreement with previous reports [ 21 ] , it proved to be limited in identifying malignant nodules and was poorly predictive of disease in the case of positive findings . 
as a result , no us or colour - doppler us criteria exist that enable recognition of suspicious thyroid nodules and selection for cytology . our series revealed that grey - scale us had reasonable specificity for the characterisation of thyroid nodules and a reasonable npv both in solitary and in multiple nodules . this result does not , however , allow us to conclude that us is effective in correctly classifying a thyroid nodule as benign , because the high prevalence of benign nodules alone accounts for this , regardless of the real diagnostic effectiveness of the study . 
 in our series , the prevalence of cytologically suspicious or malignant lesions was significantly higher in patients with solitary nodules compared with those with multiple nodules . this finding conflicts with the recent literature , which reports a similar prevalence in the two groups [ 18 ]  . 
a possible explanation for this discrepancy is related to the different criteria used for selecting nodules for biopsy : in patients in our study with solitary nodules , all nodules larger than 6 mm were sampled , independent of their us and colour - doppler us features . 
owing to the poor sensitivity of us and colour - doppler us in characterising thyroid nodules , it is likely that some suspicious or malignant nodules were not sampled in patients with goitre because of their benign appearance on us and colour - doppler us . 
a similar issue has also been addressed by other authors who emphasised that , against the similar overall likelihood of patients with solitary or multiple nodules developing thyroid cancer , needle biopsy of the largest nodule will fail to identify approximately 1 / 3 malignant lesions in patients with multiple nodules [ 2 ]  . 
fna cytology is an accurate technique in characterising thyroid nodules [ 2 , 13 ] , but it suffers from a renziare efficacemente i noduli benigni della tiroide da quelli maligni attualmente ridimensionata [ 2 , 7 , 8 , 19 , 20 ]  . i risultati del nostro studio confermano la tendenza della letteratura . 
nella nostra casistica lecografia in scala dei grigi ha presentato bassa sensibilit e basso vpp nel riconoscere i noduli tiroidei maligni , ovvero , in accordo con la letteratura [ 21 ] , ha dimostrato scarsa capacit nellindividuare i noduli maligni associata ad una scarsa probabilit di malattia in caso di ecografia positiva . 
non esistono pertanto criteri ecografici ed eco - color doppler che consentono di riconoscere i noduli sospetti della tiroide e di focalizzare su di essi la valutazione citologica . la nostra casistica ha rilevato una discreta specificit dellecografia in scala dei grigi nella caratterizzazione del nodulo tiroideo ed un discreto vpn sia nei noduli solitari che nei pazienti con noduli multipli . 
questo risultato non consente tuttavia di concludere che lecografia efficace nel diagnosticare correttamente un nodulo tiroideo come benigno in quanto lalta prevalenza di noduli benigni spiega da sola questo risultato indipendentemente dalla reale efficacia diagnostica dellindagine . 
la valutazione doppler ha nella nostra esperienza comportato una ulteriore riduzione della specificit senza sostanziali variazioni del vpn . nella nostra casistica la prevalenza di lesioni sospette o maligne alla citologia stata significativamente maggiore nei pazienti con nodulo solitario rispetto ai pazienti con noduli multipli . 
una possibile spiegazione di questa discrepanza deriva dalle differenze nei criteri di selezione dei noduli biopsiati ; nei pazienti con nodulo solitario , infatti , sono stati biopsiati tutti i noduli di dimensioni > 6 mm , indipendentemente dalle caratteristiche ecografiche ed eco - color doppler ; nei pazienti con noduli multipli stato sottoposto a biopsia il nodulo pi voluminoso e eventuali noduli con caratteristiche sospette allecografia e / o alleco - color doppler . in conseguenza della scarsa sensibilit dellecografia e delleco - color doppler nella caratterizzazione dei noduli tiroidei verosimile che nei pazienti con gozzo alcuni noduli sospetti o maligni non siano stati sottoposti ad agoaspirazione , a causa delle loro caratteristiche ecografiche e color doppler di benignit . 
una simile problematica stata affrontata anche in altri lavori che sottolineano come , a fronte di una probabilit globale , analoga , per paziente con nodulo singolo e con noduli multipli , di sviluppare una neoplasia tiroidea , lagobiopsia nei pazienti con noduli multipli del solo nodulo di maggiori dimensioni comporta la mancata identificazione di circa 1 / 3 delle lesioni maligne [ 2 ]  . un limite di questo studio che come test di riferimento stata considerata la valutazione citologica . 
lagoaspirato tiroideo una tecnica accurata per la caratterizzazione dei noduli tiroidei [ 2 , 13 ] , ma gravato da una quota di prelievi inadeguati , da una piccola quota di falsi positivi e di falsi negativi , da una quota di prelievi con caratteristiche sospette che non possono essere caratterizzati come benigni o maligni e , soprattutto , da una quota rilevante di esami indeterminati [ 2 , 13 ]  . 
the reported rate of false - positive and false - negative results is less than 1% [ 2 ]  . the rate of inadequate samples depends on the manner in which cytological evaluation is carried out . 
a significant limitation to our study is that the cytologist did not perform quick staining or examine the material under the microscope immediately , as this procedure would make examination times longer , which would be incompatible with the departments workload . 
despite this limitation , the presence of the cytologist in the us room is useful and justified , as it reduces examination times , ensures correct slide preparation and allows a rough visual inspection of sample adequacy . 
in our series , the rate of inadequate samples was 9.3% , that is , lower than the rates of 15%20% usually reported in the literature [ 2 ]  . 
in our study , the sensitivity , specificity , ppv , npv and diagnostic accuracy of imaging were calculated by considering those nodules to be positive , that is , not benign . 
the decision to consider all suspicious and indeterminate nodules to be positive results in a lower sensitivity and ppv compared with the values that would be obtained if histology were taken as the reference method . 
on the other hand , only some of the thyroid nodules with indeterminate or suspicious cytology are removed by surgery , so that histological correlation is not available for those nodules . 
 the results of this study , in agreement with the most recent literature , confirm that us and colour - doppler us with the commonly accepted semiotic criteria are unable to provide the sufficiently accurate characterisation of thyroid nodules needed to select nodules for biopsy . 
whereas for single nodules the prevailing tendency is to cytologically sample all nodules larger than 6 mm , the problem is particularly serious in patients with goitre , as not all nodules can be aspirated , and the choice is necessarily based on us imaging . 
the sonologist and the clinician need to be aware of the limitations vi riportata in letteratura inferiore a 1% [ 2 ]  . la quota di prelievi inadeguati dipende dalle modalit con le quali viene eseguito lesame . 
un limite importante del nostro studio dato dal fatto che il citologo presente in sala ecografica non esegue una colorazione rapida e la visione estemporanea al microscopio del materiale ; questa procedura , infatti , comporterebbe un aumento inaccettabile dei tempi di esame , non compatibile con i carichi di lavoro del nostro servizio . 
nonostante questo limite , a nostro parere , la presenza del citologo in sala ecografica utile e giustificata in quanto riduce il tempo necessario per lesame , garantisce la corretta preparazione del vetrino e una valutazione , sia pure grossolana e ispettiva , della sua adeguatezza . 
nella nostra casistica i prelievi inadeguati sono risultati infatti del 9.3% , una quota inferiore a quella comunemente riportata in letteratura del 15%20% [ 2 ]  . la quota di noduli sospetti alla citologia che risulta istologicamente maligno varia secondo le diverse casistiche tra il 30% e il 65% [ 4 ]  . 
nel nostro lavoro , tuttavia , la sensibilit , specificit , vpp , vpn e accuratezza diagnostica dellimaging sono stati calcolati considerando questi noduli come positivi , e pertanto non benigni . 
la scelta di considerare come positivi i noduli sospetti e indeterminati comporta pertanto una riduzione dei valori di sensibilit e vpp , rispetto a quelli che si otterrebbero considerando come indagine di riferimento la valutazione istologica . 
daltra parte , solo una parte dei noduli tiroidei con citologia indeterminata o sospetta viene rimossa chirurgicamente e lesame istologico non pertanto disponibile per questo tipo di valutazione . conclusioni lapproccio alla diagnosi della patologia nodulare tiroidea necessariamente multidisciplinare . 
il ruolo nella caratterizzazione dei noduli invece stato progressivamente ridimensionato . i risultati di questo studio , in accordo con la letteratura pi recente , confermano come , utilizzando i criteri semeiologici comunemente accettati , lecografia e leco - color doppler non consentono una caratterizzazione accurata del nodulo tiroideo utile per orientare la scelta del nodulo da sottoporre a biopsia . 
mentre per quanto riguarda il nodulo singolo la tendenza prevalente quella di eseguire il prelievo citologico su tutti i noduli di dimensioni > 6 mm , il problema particolarmente importante nei pazienti con gozzo nei quali impossibile aspirare tutti i noduli e la scelta necessariamente basata sullimaging ecografico . 
in these patients , us follow - up and accurate nodule measurement is fundamental for identifying the fastest growing nodules , which require cytologic sampling regardless of size and morphological features . duazione di una quota di lesioni maligne . 
this paper describes the most appropriate mri techniques and sequences for the study of cardiovascular heart diseases on the basis of an analysis of mri studies carried out between january 2003 and june 2006 on 274 patients affected by all of the main congenital cardiovascular malformations , as well as a review of the literature . 
the advantages of mri with respect to other imaging techniques , the problems encountered and the main clinical applications and indications of mri , with special reference to the most common disease entities , are then discussed to define the role , the utility and the future perspectives of this imaging technique in the study of congenital heart diseases . key words congenital heart diseases cardiovascular magnetic resonance tetralogy of fallot riassunto negli ultimi decenni , importanti progressi nel trattamento medico e chirurgico delle cardiopatie congenite hanno reso pi elevate le aspettative di vita di questi pazienti , ma hanno anche aumentato il numero di coloro che necessitano di un monitoraggio continuo per identificare complicanze e difetti residui . 
la risonanza magnetica ( rm ) , in virt della sua non invasivit , riproducibilit ed accuratezza nel dettaglio morfologico e funzionale una metodica ideale per il follow - up di questi giovani pazienti . attraverso la valutazione della nostra esperienza di studio con rm nel periodo compreso dal gennaio 2003 al giugno 2006 , durante il quale sono stati valutati 274 pazienti affetti da tutte le principali malformazioni congenite del cuore e dei grossi vasi , e attraverso lanalisi della letteratura , sono descritte le modalit da adottare e le sequenze da impiegare per un corretto studio con rm di questa patologia . 
sono successivamente discussi i vantaggi rispetto alle altre metodiche dimaging , le problematiche da affrontare e le indicazioni ed applicazioni cliniche pi frequenti , con particolare approfondimento dei pi comuni quadri patologici studiati , definendo in conclusione lutilit e il ruolo di questa metodica nello studio delle cardiopatie congenite e le prospettive future . parole chiave cardiopatie congenite risonanza magnetica cardiovascolare tetralogia di fallot introduction introduzione congenital heart disease is undoubtedly the most common malformation , with an incidence of 0.5%1.2% of live births [ 1 ]  . 
these rates become even higher if minor cardiovascular defects are included that do not require treatment or are unle cardiopatie congenite rappresentano in assoluto la patologia malformativa pi frequente , con unincidenza variabile dallo 0 , 5% all1 , 2% dei nati vivi [ 1 ]  . 
advances in palliative and corrective surgical treatment and interventional procedures have dramatically improved patients life expectancy , leading to increasing numbers of patients who survive into adulthood [ 2 , 3 ]  . 
in addition , the continuous improvement of cardiovascular imaging techniques has contributed to the early detection of mild diseases that would otherwise go undetected and that , although not warranting immediate treatment , need to be followed up . 
at the same time , increasing numbers of patients need clinical and imaging follow - up over extended periods of time to identify possible postsurgical complications , or recurrences such as recoarctation , and to monitor a residual defect [ 6 ]  . 
whereas in the past , the role of imaging mainly involved detecting cardiac malformations and therefore providing morphological data , today , the importance of prognostic evaluation and follow - up , especially among adult patients [ 79 ] , requires larger amounts of both morphological and functional information , and the most accurate , reproducible and above all noninvasive imaging technique possible . magnetic resonance imaging ( mri ) , in particular , has made remarkable progress during the last few years regarding both acquisition speed and software design [ 10 ]  . 
mri offers important advantages over other imaging modalities in the study of congenital heart diseases : its high spatial and temporal resolution allow extremely accurate rendering of morphological and functional details , whereas its multiplanar capabilities and large field of view afford a panoramic view with unlimited access to thoracic and extrathoracic structures [ 11 ]  . 
i progressi nel trattamento chirurgico palliativo e correttivo e nelle procedure interventistiche delle cardiopatie congenite hanno determinato un netto miglioramento delle aspettative di vita dei pazienti , che nella maggior parte dei casi raggiungono let adulta [ 2 , 3 ]  . 
contemporaneamente , il continuo miglioramento delle metodiche dimaging cardiaco ha reso pi facile il riconoscimento delle forme lievi , che diversamente sarebbero passate inosservate e che , pur non necessitando un trattamento immediato , pongono il problema di una valutazione evolutiva . 
contemporaneamente aumentato il numero dei pazienti che necessita di una continua sorveglianza clinica e strumentale nel corso del tempo , sia per riconoscere precocemente eventuali complicanze post - chirurgiche sia per identificare la possibile ricorrenza di un aspetto malformativo , come nel caso della ricoartazione aortica , o infine per monitorare un difetto residuo [ 6 ]  . 
se in passato il ruolo dellimaging era prevalentemente basato sullidentificazione delle malformazioni cardiache e conseguentemente sul dato morfologico , oggi la valutazione prognostica e il follow - up sono divenuti elementi fondamentali , in particolare negli adulti [ 79 ] , richiedendo una maggiore ricchezza di informazioni , anche funzionali e una metodica dindagine il pi possibile accurata , riproducibile e soprattutto non invasiva . la rm in particolare stata protagonista negli ultimi anni di un notevole avanzamento tecnologico in termini sia di velocit delle sequenze che di software applicativi [ 10 ]  . 
la rm possiede alcuni significativi vantaggi rispetto alle altre metodiche dimaging nella valutazione delle anomalie congenite cardiovascolari : fornisce il dettaglio morfologico e funzionale con estrema accuratezza , in virt dellelevata risoluzione spaziale e temporale delle sue sequenze , mentre la multiplanarit e lampio campo di vista le consentono una visione panoramica senza limiti di accesso alle strutture toraciche ed extratoraciche [ 11 ]  . 
queste caratteristiche , e in particolare la non invasivit e lelevata riproducibilit dei parametri , la rendono una metodica ideale per lo studio delle cardiopatie congenite , considerando la progressiva evoluzione delle caratteristiche della popolazione di studio [ 2 , 12 ]  . alla luce della nostra esperienza nello studio morfologico e funzionale delle cardiopatie congenite con rm e attraverso lanalisi della letteratura , in questa review sono discusse lutilit e il ruolo della rm nella diagnosi , valutazione preoperatoria e follow - up di queste patologie malformative , del . 
cardiovascular mri is generally well tolerated by patients , despite an average scan duration of 4060 min . nonetheless , psychological reactions such as panic attacks or feelings of fear do occur , although more frequently among adults and adolescents than among children , who , on the other hand , are less cooperative ( age < 10 years )  . 
therefore , to avoid the risk of incomplete and poor - quality examinations , patients and / or their relatives need to be informed about the mri examination ( duration , intravenous line placement , need for breath - holding and immobility during image acquisition )  . 
for children aged 6 years or younger who are unable to follow breath - holding and immobility instructions , sedation or general anaesthesia are indicated . segmental analysis methodology the study of congenital heart disease calls for a systematic approach [ 7 , 13 ] , especially for the evaluation of complex congenital malformations and the definition of ambiguous situs , owing to the alteration of the relationships among the atria , ventricles and great vessels . 
an axial and , if necessary , a coronal stack of black - blood fast spin - echo ( bbfse ) images covering the entire thorax is sufficient . segmental analysis was performed in all patients , even those with a known diagnosis , because it defines the anatomical relationships between cardiac and extracardiac structures and helps identification of associated anomalies , which may have been missed on echocardiography ( limited field of view ) or cardiac catheterisation . mri examination : sequences all patients were studied with a 1.5 - tesla ( t ) mri scanner [ signa horizon , general electric medical systems ( gems ) , milwaukee , wi , usa ] equipped with a dedicated cardiac and thoracic coil ( cardiac and torsopa phased array ) , the latter used for the study of congenital aortic anomalies . 
the morphological study of congenital heart diseases was performed with a breath - hold electrocardiographic - triggered bbfse sequence [ double inversion recovery pulse , matrix 256224 , field of view ( fov ) 40 cm , echo time ( te ) 40 ms , repetition time ( tr ) 1 r - r interval ] acquired at end - inspiration and covering the entire thorax in the axial plane ( section thickness , 57 mm without gap ) and , if required , in the coronal and oblique sagittal plane ( tables 2 and 3 ) ( section thickness 45 mm , without gap )  . when cardiac anatomy was complex , the study was completed with a gradient - echo ( gre ) sequence with fast imaging employing steady - state acquisition ( fiesta ) ( gems ) , with repetition of the same axial and coronal images and , if diovascolare dellospedale s . 
tutti i pazienti sono stati precedentemente valutati mediante ecocardiografia transtoracica e / o transesofagea . tecnica di esecuzione dellindagine rm preparazione del paziente e criteri di inclusione le cause di esclusione dallindagine di rm sono state la presenza di un pace - maker ventricolare e / o un defibrillatore intra - cardiaco , clips metalliche endocraniche e forme severe di claustrofobia . 
lesame , pur avendo una durata media di 4060 minuti , normalmente ben tollerato , ma possono manifestarsi reazioni psicologiche quali attacchi di panico o sensazioni di paura , pi frequenti negli adulti e adolescenti rispetto ai bambini [ 9 ] , i quali daltra parte hanno una ridotta capacit collaborativa ( et < 10 anni )  . 
pertanto , per evitare il rischio di indagini incomplete e di ridotta qualit , occorre informare i pazienti e / o i loro familiari sulle caratteristiche dellesame ( durata , reperimento della via venosa , necessit di apnea e immobilit durante lacquisizione delle immagini )  . 
per quelli di et uguale o inferiore ai 6 anni , incapaci di seguire le istruzioni relative al respiro e allimmobilit , vi indicazione generale ad eseguire lesame in sedazione o anestesia generale . metodologia dellanalisi segmentaria un approccio sistematico nello studio delle cardiopatie congenite necessario [ 7 , 13 ] , in particolare nella valutazione delle malformazioni congenite complesse e nella definizione dei situus ambigui , data lalterazione delle connessioni tra atri , ventricoli e grandi vasi . 
una serie di immagini black - blood fast spin - echo ( bbfse ) su piano assiale e qualora necessario coronale , a copertura di tutto il torace , sono sufficienti . lanalisi segmentaria stata eseguita in tutti i pazienti , anche quando la diagnosi era nota , anche perch descrive i rapporti con le strutture extracardiache e facilita lidentificazione di eventuali anomalie associate , che possono non essere state mai rilevate dallecocardiogramma ( ridotto campo di vista ) o dal cateterismo cardiaco . esame rm : sequenze tutti i pazienti sono stati studiati con un magnete da 1 , 5 tesla ( signa horizon , general electric medical systems , gems , milwaukee , wisconsin , usa ) , con bobine dedicate cardiaca e toracica ( cardiac e torsopa phased array ) , questultima per lo studio delle anomalie congenite dellaorta . 
axial black - blood fast spinecho ( bbfse ) image shows inverted spatial relationships between the great arteries , the aorta ( ao ) is anterior and to the left of the pulmonary artery ( pa )  . 
note the ventricular trabeculations ( moderator band ) and the septal attachment of the tricuspid valve closer to the left - sided ventricle apex than the mitral valve ( arrows ) , both aspects that identify the right ventricle ( rv )  . 
note the right atrium ( ra ) and the typical finger - like appearance of the left atrial appendage ( asterisk ) identifying the left atrium ( la ) : atrioventricular discordance . 
limmagine assiale black blood fast spin - echo evidenzia uninversione dei rapporti spaziali dei grandi vasi , con laorta ( ao ) disposta a sinistra e anteriormente rispetto allarteria polmonare ( pa )  . 
si noti laccentuata trabecolatura ( banda moderatrice ) e lattacco settale della valvola tricuspide pi vicino allapice del ventricolo posto a snistra rispetto alla valvola mitrale ( frecce ) , entrambi aspetti che identificano il ventricolo destro ( rv )  . 
flow analysis with velocity - encoded cine mri ( vec - mri ) for the assessment of valvular regurgitation and stenosis and the semiquantitative study of vascular and prosthetic stenosis was performed by using a fast phasecontrast sequence ( pc apnea , gems )  . 
quantitative image analysis was performed on a commercially available workstation ( advanced windows 4.0 , gems ) using flow - analysis software ( flow , medis , leiden , the netherlands )  . 
contrast - enhanced mr angiography ( mra ) after intravenous injection ( flow velocity 12 ml / s ) of 0.1 mmol / kg gadobutrol ( gadovist , schering , berlin , germany ) or 0.2 mmol / kg gadopentate dimeglumine ( magnevist , schering ) in patients aged < 18 years was performed in 224 / 274 patients for the evaluation of pulmonary arteries [ tetralogy of fallot ( tof ) , bambini molto piccoli e i neonati sono stati studiati utilizzando la bobina per lo studio dellencefalo ( head , gems )  . lo studio morfologico delle cardiopatie congenite stato condotto con sequenze bbfse cardiosincronizzate ( doppio impulso di inversione , matrice 256224 , fov 40 cm , te 40 ms , tr = 1 intervallo r - r ) , in apnea inspiratoria , a copertura di tutto il torace su piano assiale ( spessore di strato 57 mm , intervallo 0 mm ) e , quando richiesto , coronale e sagittale ( tabella 2 e 3 ) ( spessore di strato 45 mm ed intervallo 0 mm )  . 
finally , the study and analysis of potential structural myocardial alterations ( fibrosis ) by evaluation of interstitial gadolinium accumulation ( late enhancement study ) , as in the case of ischaemic cardiopathy and other cardiomyopathies , was performed with a segmented inversion recovery fast gre sequence ( fgre , gems ) in patients with tof , congenitally corrected tga and tga with atrial switch repair ( table 2 )  . 
parameters included matrix 256160 , magini stata eseguita su una consolle di ricostruzione ( advanced windows , gems ) utilizzando un software di analisi del flusso ( flow , medis , leiden , olanda )  . 
langio - rm dopo iniezione endovenosa ( velocit di flusso 12 ml / s ; 0 , 1 mmoli / kg ) di gadobutrolo ( gadovist , schering , berlin , germania ) o , nei pazienti di et inferiore a 18 anni , di dimeglumina gadopentato ( magnevist , schering ) ( 0 , 2 mmoli / kg ) , stata effettuata in 224 / 274 pazienti per lo studio delle arterie polmonari ( tdf , ap ) , della coartazione aortica o di altre l . 
the natural history of many of these patients , such as those operated on for tof or tga , is greatly influenced by the risk of sequelae such as progressive ventricular dysfunction [ 14 , 15 ] , so that quantification of ventricular volumes and mass has become essential . 
its limitations ( operator dependence , acoustic window , use of geometric assumptions ) , however , lead to an underestimation of left ventricular volumes , with the risk of assigning patients to a different functional class in up to 44% of cases [ 16 ]  . 
 [ 17 ] in a meta - analysis of data on the quantification of cardiac volumes in a population of 164 patients derived from nine studies comparing mri and scintigraphy . mri has the advantage of calculating ventricular volumes , ejection fraction and mass without the use of geometric assumptions [ 18 ] and , with its high spatial and contrast resolution and reproducibility , it is now considered the gold standard for the evaluation of biventricular function [ 1923 ]  . 
another important component of functional analysis in the follow - up of surgically repaired congenital cardiovascular malformations is flow analysis for evaluation of pulmonary valve function and identification of residual intracardiac shunts in patients with surgical correction of tof , the measurement of pressure gradients in vascular and prosthetic conduit stenoses ( senning , mustard and fontan operations ) and the study of collateral circulation in patients with suspected recoarctation [ 24 ]  . 
since the 1990s , several authors [ 25 , 26 ] have validated this technique , demonstrating the optimal correlation with echocardiography ( colour - doppler ) in the measurement of transpulmonary , transaortic and transmitral valve flow and velocity , both in normal subjects and in patients with valvular disease , and even highlighting the superiority of mri over doppler ultrasonography when the acoustic window is limited . 
infine la ricerca e lanalisi delle possibili alterazioni strutturali ( fibrosi ) del miocardio valutando laccumulo interstiziale miocardico del gadolinio ( studio di late enhancement ) , analogamente a quanto avviene nella cardiopatia ischemica o in altre cardiomiopatie , stata effettuata con una sequenza segmented inversion recovery fast gre ( fgre , gems ) nei pazienti con tdf , tgv congenitamente corretta o tgv operata con switch atriale ( tabella 2 )  . 
i parametri includevano : matrice 256160 , fov 32 cm , tr / te 5 , 3 / 1 , 7 ms , flip angle 45 , spessore di strato 7 mm , intervallo 0 mm , nex 2 , tempo di inversione per lannullamento del segnale del miocardio normale , calcolato per ogni paziente , 230400 ms . ruolo e indicazioni cliniche della rm nella valutazione morfo - funzionale delle cardiopatie congenite il follow - up dei pazienti operati attualmente lindicazione prevalente allimpiego della rm nello studio delle cardiopatie congenite . 
per molti di questi pazienti , infatti , come quelli operati di tdf o tgv , la storia naturale grandemente influenzata dal rischio di sequele quali ad esempio una progressiva disfunzione ventricolare [ 14 , 15 ] ed elementi come il calcolo dei volumi e della massa ventricolari sono divenuti fondamentali . 
la metodica maggiormente utilizzata nella pratica clinica per il calcolo dei parametri di funzione ventricolare lecocardiografia transtoracica bidimensionale . tuttavia i suoi limiti ( operatore - dipendenza , finestra acustica , utilizzo di assunzioni geometriche ) portano ad una sottostima dei volumi ventricolari sinistri , con il rischio di attribuire i pazienti ad una classe funzionale diversa sino al 44% dei casi [ 16 ]  . 
 [ 17 ] attraverso la metanalisi dei dati relativi alla quantificazione dei volumi cardiaci di una popolazione di 164 pazienti , ricavata da 9 studi comparativi tra la rm e la scintigrafia . la rm ha il vantaggio di calcolare volumi , frazione deiezione e massa ventricolari senza assunzioni geometriche [ 18 ] e per la sua elevata risoluzione spaziale e di contrasto e riproducibilit , considerata oggi il gold - standard per la valutazione della funzione biventricolare [ 1923 ]  . unaltra importante componente dellanalisi funzionale nel follow - up delle cardiopatie congenite operate riguarda gli studi flussimetrici per la valutazione della funzione valvolare polmonare e il riconoscimento di shunts intracardiaci residui nei pazienti operati di tdf , il calcolo dei gradienti pressori nelle stenosi vascolari e dei condotti protesici ( interventi di senning , mustard e fontan ) e la valutazione dei circoli collaterali nel sospetto di ricoartazione [ 24 ]  . 
to the left : axial - orientated gradient - echo ( balanced fast field echo technique ) image ( four - chamber long - axis view ) shows severe dilation of the right cardiac sections . 
to the right : sagittal orientated gradient - echo ( balanced fast field echo technique ) image acquired on a plane behind the cardiac base identifies a remarkable dilation of the inferior vena cava ( ivc )  . 
ra right atriub velocity - encoded cine mri ( vec - mri ) images of the pulmonary trunk , systolic phase ( left ) and magnitude ( right )  . 
c flow curves of the pulmonary artery ( high ) and ascending aorta ( low ) demonstrate an evident predominance of pulmonary flow with a 3 : 1 ratio between pulmonary and systemic output , indicating a left - to - right shunt . 
to the left : maximum intensity projection reconstructed coronal image ( posterior view ) demonstrates anomalous pulmonary venous return with inferior vena cava drainage of all the right lung pulmonary venous blood through one collector only . 
a destra : limmagine sagittale obliqua gradient - echo con tecnica balanced fast field echo ( a destra ) passante per un piano subito a monte della base cardiaca , identifica unimportante dilatazione della vena cava inferiore ( ivc )  . 
c le curve di flusso dellarteria polmonare ( in alto ) e dellaorta ascendente ( in basso ) dimostrano una netta preponderanza di flusso a livello polmonare con un rapporto tra le gittate polmonare e sistemica 3 : 1 , indicativo di shunt sinistro - destro . 
a sinistra : limmagine di ricostruzione maximum intensity projection ( a sinistra ) su piano coronale ( visione posteriore ) evidenzia un ritorno venoso polmonare anomalo in vena cava inferiore di tutto il sangue venoso polmonare del polmone destro , mediante un unico collettore . 
a destra : limmagine di ricostruzione volume rendering sullo stesso piano ( visione anteriore ) definisce con maggiore chiarezza i rapporti anatomici tra la vena cava inferiore ( ivc ) e la vena polmonare destra ( rpv )  . 
the accurate description of these anatomical relationships is fundamental in surgical planning , as it allows the surgeon to reduce the procedure time [ 34 ]  . tetralogy of fallot despite the favourable outcome of surgery and improved life expectancy , the natural history of patients with tof is si autori [ 25 , 26 ] hanno validato questa tecnica dimostrandone lottima correlazione con lecocardiografia ( color doppler ) nel misurare velocit e flussi transvalvolari mitralici , aortici e polmonari sia in soggetti normali che in pazienti con patologia valvolare , evidenziandone addirittura la superiorit nei casi con limitata finestra acustica allecocardiografia , ma lunicit della rm dovuta soprattutto alla multiplanarit . 
la capacit di orientare il piano della sequenza nei tre assi dello spazio , ponendosi sempre perpendicolarmente al lume vasale , consente un campionamento pi preciso della velocit del sangue [ 27 ]  . 
 [ 28 ] hanno dimostrato una buona correlazione con i valori del cateterismo cardiaco . al pari dellecocardiografia , la completa non invasivit della rm legata al non utilizzo di mezzi di contrasto iodati e di radiazioni ionizzanti , aspetto non trascurabile nello studio dei bambini e / o dei neonati , ha portato al progressivo declino del cateterismo cardiaco diagnostico [ 29 ] e rappresenta un altro vantaggio di questa metodica , anche in considerazione della necessit di eseguire indagini seriate nel corso del follow - up . 
3a sagittal orientated gradient - echo ( balanced fast field echo technique ) image of the pulmonary infundibuludiastolic infundibular flow turbulence ( signal void ) ( arrows ) , indicating pulmonary valve insufficiency . 
b sequenza phase contrast : immagine di fase parallela al piano valvolare polmonare in fase sistolica ( a sinistra ) e diastolica ( a destra ) : il segnale bianco in sistole ( asterisco ) espressione di flusso anterogrado , il segnale nero in diastole ( asterisco ) indice di flusso retrogrado ( rigurgito valvolare )  . 
c curva di flusso valvolare polmonare : il rigurgito polmonare chiaramente visibile e quantificabile nel grafico . characterised by frequent complications and residual defects that require a careful follow - up [ 35 , 36 ]  . 
ventricular septal defects , residual or recurrent pulmonary artery stenoses , right ventricular outflow tract aneurysms , pulmonary regurgitation and consequent right ventricular dysfunction [ 27 , 37 ] represent the main issues in the natural history of patients after correction of tof . 
it has been associated with right ventricular dilation , progressive ventricular dysfunction , reduced exercise tolerance and finally increased risk for atrial and ventricular arrhythmias and sudden cardiac death [ 3941 ]  . 
laccurata descrizione di tali rapporti anatomici estremamente importante per il chirurgo in previsione di un intervento correttivo , in quanto consente di ridurre i tempi delle procedure [ 34 ]  . tetralogia di fallot nonostante la ridotta mortalit chirurgica e la migliorata aspettativa di vita , la storia naturale di questi pazienti contraddistinta da frequenti complicanze e difetti residui che richiedono un attento monitoraggio nel tempo [ 35 , 36 ]  . 
note also the remarkable dilation of the right atriuc sagittal orientated gradient - echo ( balanced fast field echo technique ) images ( short axis view ) at end diastole ( to the left ) and end systole ( to the right ) demonstrate reduced right ventricle contractility and , above all , a severe ventricular infundibulum dyskinesia ( pseudoaneurysm )  . 
d same patient : the graphic synthesises the right ventricle volumes and functional values obtained by outlining endocardial and epicardial borders in end diastole and end systole of all images acquired from the base to the cardiac apex . 
c le immagini sagittali oblique gradient - echo ( tecnica balanced fast field echo ) ( asse corto cardiaco ) in fase telediastolica ( a sinistra ) e telesistolica ( a destra ) dimostrano una ridotta capacit contrattile del ventricolo destro ed in particolare un aspetto severamente discinetico dellinfundibolo ventricolare ( pseudoaneurisma )  . 
d stesso paziente , nel grafico sono sintetizzati i valori dei volumi e dei parametri funzionali del ventricolo destro ottenuti mediante delineazione dei bordi epicardici ed endocardici nelle fasi telediastoliche e telesistoliche di tutte le immagini acquisite dalla base allapice cardiaco . 
designated cutoff values of end - diastolic and end - systolic volumes that , if exceeded , would prevent normalisation of right ventricular volumes , even after homograft placement [ 45 ]  . 
exercise mri , despite the limited availability of systems , is a useful application for the study of both ventricular function and pulmonary regurgitation and is effective in identifying a pulmonary / ventricular dysfunction not detectable at rest . 
 [ 49 ] observed an abnormal response to exercise in 15 patients with corrected tof and normal ejection fraction at rest compared with the control group , characterised by an increase in end - diastolic volume index without a significant change in ejection fraction . 
another recent mri application for the prognostic evaluation of these patients is the late enhancement study of the right ventricular myocardium , in particular the outflow tract , for the analysis of structural alterations ( fibrosis ) as an organic basis of arrhythmias and progressive right ventricular dysfunction [ 50 ]  . 
moreover , vec - mri is almost unique among noninvasive imaging techniques in its capacity to accurately measure flow velocity and pressure gradients through pulmonary stenosis , especially in pulmonary arterial ramifications [ 25 ]  . 
another application of vec - mri in this field is identification of patients with flow disparity in the pulmonary arteries , quantifying the differential contribution of the main - branch pulmonary arteries to pulmonary regurgitation [ 52 ]  . 
finally , mri identifies pulmonary - systemic palliative shunt complications ( stenosis , obstructions , leakages , dilations ) with mra and residual septal defects either directly , by visualising flow turbulence across the defect ( gre sequences ) or indirectly ( vec - mri ) , by calculating aortic and pulmonary artery flow ratio ( pulmonary stroke volume / systemic stroke volume ) [ 27 , 53 , 54 ]  . the completeness and accuracy of information provided by mri in a single examination session make it the modality of choice in the follow - up and prognostic evaluation of tof . transposition of the great arteries tga is a congenital anomaly characterised by an atrioventricular concordance and a ventriculoarterial discordance and is consequently a life - threatening condition that requires surgical correction early in life . 
 [ 45 ] hanno individuato dei valori cut - off per i volumi telediastolici e telesistolici superati i quali non si avrebbe la normalizzazione dei volumi ventricolari destri anche dopo posizionamento dellhomograft [ 45 ]  . 
la rm con test da sforzo , pur limitata dalla disponibilit delle apparecchiature , unutile applicazione dello studio sia della funzione ventricolare che del rigurgito polmonare , efficace nellindividuare una disfunzione ventricolare e / o polmonare non osservabile in condizioni di riposo . 
 [ 49 ] hanno evidenziato in 15 pazienti operati per tdf con frazione deiezione normale a riposo rispetto ai controlli , una risposta alterata allo stress fisico , caratterizzata da un aumento dei volumi telediastolici in assenza di variazioni significative della frazione deiezione . 
unulteriore recente applicazione della rm per la valutazione prognostica di questi pazienti lo studio di late enhancement del miocardio ventricolare destro , in particolare del tratto defflusso , per lanalisi delle alterazioni strutturali ( fibrosi ) come base organica delle aritmie e della progressiva disfunzione ventricolare destra [ 50 ]  . 
the diameter disparity between the two main pulmonary arteries is clearly depicted , without circumscribed stenosis of the left pulmonary artery ( lpa ) ( left pulmonary artery hypoplasia )  . 
d the graphics of the flow curves of right ( high ) and left ( low ) pulmonary arteries quantify the flow disparity between the two arteries ( left pulmonary artery hypoplasia ) and allow evaluation of their different contributions to pulmonary regurgitation . 
si apprezza meglio la disparit di calibro tra le due arterie , senza per significative stenosi circoscritte dellarteria polmonare sinistra ( lpa ) ( ipoplasia dellarteria polmonare sinistra )  . 
d i grafici delle curve di flusso dellarteria polmonare destra ( in alto ) e sinistra ( in basso ) quantificano la netta disparit di flusso tra i due rami polmonari ( ipoplasia dellarteria polmonare sinistra ) e consentono la valutazione del loro diverso contributo allinsufficienza polmonare . choice is the jatene procedure ( arterial switch ) [ 55 ]  . 
infine la rm identifica le complicanze degli shunts palliativi sistemico - polmonari ( stenosi , ostruzioni , leakage , dilatazioni ) con langio - rm e i difetti settali residui sia direttamente , visualizzando una turbolenza di flusso attraverso il l . 
a sinistra : immagine sagittale obliqua black - blood fast spin - echo : si apprezza una evidente ipoplasia dellarco distale e una riduzione di calibro moderata del tratto istmico . 
i grafici dei flussi a livello istmico ( in alto ) e diaframmatico ( in basso ) evidenziano un netto incremento dei flussi in sede aortica distale ( 36% ) indicativo di significativi circoli collaterali ( paziente in valutazione per intervento correttivo )  . monary arteries or right ventricular outflow tract [ 58 , 59 ]  . mri accurately evaluates the morphology of the great arteries after arterial switch , either with bbfse or gre sequences . 
great significance is held by mra for the study of pulmonary artery morphology and the measurement of aortic diameters . the anatomy of the coronary arteries has to be accurately considered as well , because coronary artery reimplantations may become dilated or distorted , with a risk of ostial stenosis , which was also been demonstrated in asymptomatic patients [ 60 ]  . 
le complicanze maggiori nel corso del follow - up sono : la dilatazione della radice aortica , linsufficienza valvolare aortica e le stenosi del tratto defflusso polmonare o delle arterie polmonari [ 58 , 59 ]  . 
grande importanza riveste langio - rm nello studio della morfologia delle arterie polmonari e nelle misurazioni dei diametri aortici . lanatomia delle coronarie va anchessa accuratamente considerata , in quanto i reimpianti coronarici possono dilatarsi o distorcersi con il rischio di stenosi ostiali , dimostrate anche in pazienti asintomatici [ 60 ]  . 
in questi pazienti , pur sopravvivendo sino allet adulta , il ventricolo destro rimane connesso allaorta ed sottoposto a pressioni sistemiche , favorendo la progressiva comparsa di alterazioni della funzione ventricolare sia a riposo che dopo esercizio fisico [ 15 , 62 ]  . 
essi costituiscono una popolazione la cui storia naturale caratterizzata da una percentuale di disfunzione ventricolare destra sino al 10% [ 63 , 64 ] e necessitano di continui controlli per monitorare la funzione ventricolare destra ( ventricolo destro sistemico )  . 
in aggiunta al dato funzionale la rm si avvale anche delle sequenze per lo studio del late enhancement ( tabella 3 ) che identificano eventuali alterazioni strutturali miocardiche ( fibrosi ) del ventricolo sistemico , come recentemente dimostrato da alcuni studi , che hanno inoltre evidenziato una correlazione tra la presenza e / o lestensione delle aree di iperenhancement e il grado di disfunzione ventricolare , let e alcuni parametri elettrofisiologici [ 67 , 68 ]  . 
la rm efficace sia nello studio pre - operatorio , che nel follow - up post - operatorio . lampio campo di vista e la multiplanarit consentono uno studio accurato dellanatomia spesso distorta dellaorta in sede istmica nei pazienti operati , che al contrario rendono ancora pi difficile lapproccio ecocardiografico . 
esame eseguito in anestesia generale . despite survival into adulthood , in these patients , the right ventricle remains connected to the aorta and is subjected to systemic pressures , facilitating the progressive appearance of ventricular function alterations both at rest and after exercise [ 15 , 62 ]  . 
these patients represent a population whose natural history is characterised by a rate of right ventricular dysfunction up to 10% [ 63 , 64 ] and who need periodic follow - up studies to monitor right ventricular contractile function ( systemic right ventricle )  . 
in addition to functional data , mri also makes use of late enhancement sequences ( table 3 ) that identify possible structural myocardial damage ( fibrosis ) of the systemic ventricle , as recently demonstrated by some studies , which also showed a relation between presence and / or extension of areas of hyperenhancement and the extent of ventricular dysfunction , age and some electrophysiological parameters [ 67 , 68 ]  . 
the large fov and multiplanar views permit accurate evaluation of the aortic anatomy of the isthmus , which is frequently distorted in postoperative patients and makes echocardiography even more difficult . 
even after surgical correction , these patients are exposed to the risk of developing complications such as recoarctation , patch pseudoaneurysm and hypertension secondary to residual arch hypoplasia [ 7 , 72 ]  . 
more recently , ther authors showed that mri is effective in the evaluation of the haemodynamic significance of the aortic coarctation [ 76 , 77 ] , and recommend its use above all in uncertain cases and in the presence of mild or moderate coarctation where no collaterals are seen on bbfse or mra images . 
in the latter case , mri might contribute to the identification of those patients at higher risk for medullary ischaemia if submitted to surgical replacement of coarctated aorta [ 76 ]  . 
these data demonstrate that transthoracic echocardiography has remained the dominant diagnostic imaging modality in the study of congenital heart pseudoaneurisma del patch , lipertensione da ipoplasia residua dellarco [ 7 , 72 ]  . 
laccuratezza e la riproducibilit delle misure sono importanti nel valutare gli indici di ricoartazione e nel follow - up degli aneurismi del patch prima dellintervento correttivo chirurgico o endovascolare . la grande potenzialit della rm consiste nel valutare il significato funzionale della stenosi . 
 [ 75 ] hanno dimostrato che la percentuale di incremento di flusso dallaorta discendente prossimale a quella distale correlata alla severit della stenosi e pi recentemente altri autori sottolineano laffidabilit della rm nel valutare il significato emodinamico della coartazione aortica [ 76 , 77 ] , raccomandandone limpiego soprattutto nei casi dubbi o nelle coartazioni lievi - moderate in mancanza di circoli collaterali evidenti nelle immagini bbfse o di angio - rm . 
questi dati dimostrano che lecocardiografia transtoracica ancora la metodica dindagine diagnostica dominante nello studio delle cardiopatie congenite nei bambini , in virt della sua non invasivit , semplicit e pronta disponibilit , senza considerare che la maggioranza di questi pazienti ha unottimale finestra acustica per le strutture cardiache . 
nel corso degli ultimi anni comunque emersa limportanza della rm per lo studio di questi pazienti , capace di superare i limiti dellecocardiografia nel visualizzare le strutture vascolari extracardiache e quelli del cateterismo cardiaco [ 79 , 80 ] , alternativa tradizionale allindagine ecografica , ma non esente dai rischi connessi alla sua natura invasiva . 
routine use of this technique continues to be hampered by several technical challenges ( smaller dimensions of the anatomical structures being imaged , faster heart rate ) requiring strategies to improve spatial and temporal resolution , and by the need for sedation in smaller , and thus noncooperative , children to avoid the deterioration of image quality . 
general anaesthesia with endotracheal intubation overcomes these limitations , achieving adequate sedation and airway protection and allowing acquisition of breath - hold sequences with a reduction of cardiorespiratory motion artefacts . 
several authors have advocated this approach for the study of congenital heart diseases in infants and small children , emphasising its safety and the low risk of complications [ 80 , 82 , 83 ]  . 
nevertheless , close interdisciplinary collaboration among the various specialists involved ( anaesthetist , radiologist , cardiologist ) is required to overcome the logistic and organisational difficulties associated with this approach . future perspectives although cardiac ultrasound is currently the first - line examination for the evaluation of congenital heart diseases , mri has now assumed a fundamental and well - defined role in the diagnosis and prognostic evaluation of these diseases in adults , particularly in the follow - up of postoperative patients and in surgical timing . 
in detail , mri is superior to the other imaging modalities for assessment of right ventricular function , quantification of pulmonary regurgitation in corrected tof , study of systemic ventricle and confirmation of suspected recoarctation . 
these are the main and most common indications for an mri study . it should , however , be remembered that mri is a complementary examination that does not replace echocardiography . 
in newborns and small children , echocardiography remains the primary technique , whereas mri is employed in carefully selected cases and for some specific indications [ 80 ] , even though its role is destined to gain importance in this field . 
la sedazione pu essere ottenuta con varie modalit di medicazione ed sicuramente un approccio adeguato [ 30 , 81 ] , vi sono per alcuni rischi legati alla mancata protezione delle vie aeree , mentre gli accorgimenti tecnici per evitare gli artefatti da respiro allungano notevolmente i tempi dellindagine . 
lanestesia generale con intubazione endotracheale supera questi limiti raggiungendo unadeguata sedazione , proteggendo le vie aeree e permettendo lesecuzione di sequenze in apnea respiratoria riducendo gli artefatti da movimento cardio - respiratorio . 
diversi autori hanno gi auspicato questo tipo di approccio per lo studio delle cardiopatie congenite nei neonati e nei bambini molto piccoli , sottolineandone la sicurezza e il basso rischio di complicanze [ 80 , 82 , 83 ]  . 
comunque necessaria una stretta collaborazione interdisciplinare tra i diversi specialisti coinvolti ( anestesisti , radiologi e cardiologi ) per superare le difficolt logistiche ed organizzative che questo tipo di esame pone . prospettive future nonostante lecocardiografia sia ancora oggi lindagine di prima istanza nello studio delle cardiopatie congenite , la rm ha oramai assunto un ruolo fondamentale e ben preciso nelliter diagnostico e nella valutazione prognostica di queste patologie negli adulti , in particolare nel follow - up dei pazienti operati , fornendo informazioni indispensabili per una corretta valutazione del timing chirurgico . 
nel dettaglio la rm superiore alle altre metodiche nella valutazione della funzione del ventricolo destro , nella quantificazione dellinsufficienza polmonare nei fallot operati , nello studio del ventricolo sistemico e nel confermare un sospetto di ricoartazione . 
nei neonati e nei primi anni di vita lecocardiografia resta ancora oggi la metodica primaria , mentre la rm impiegata in casi accuratamente selezionati e per alcune indicazioni specifiche [ 80 ] , anche se il suo ruolo destinato a divenire sempre pi importante in questo ambito , anche grazie alla sicurezza dellapproccio mediante anestesia generale . 
new perspectives will open , with the routine use of sequences characterised by faster acquisition times and adequate temporal and spatial resolution , such as real - time acquisitions or isotropic imaging [ 84 , 85 ]  . 
exercise mri , in particular , is able to provide additional data to the prognostic evaluation of these patients , even though the real clinical impact of these new applications needs to be evaluated in large follow - up studies . 
it is , however , essential to have an optimal knowledge of the anatomical and pathophysiological features of congenital heart diseases and their surgical treatment to be able to perform adequate mri examinations with shorter scan times and improved patient compliance . nel futuro prossimo la migliorata disponibilit di apparecchi dedicati localizzati in tutta prossimit dei reparti di afferenza e delle sale angiografiche , consentiranno un impiego progressivamente maggiore della rm . 
nuove prospettive si apriranno con limpiego routinario di sequenze con tempi di acquisizione pi rapidi e adeguata risoluzione temporale e spaziale come le acquisizioni in real time o limaging isotropico [ 84 , 85 ]  . 
in particolare la rm con test da sforzo capace di fornire dati aggiuntivi alla valutazione prognostica di questi pazienti , anche se il reale impatto sulla pratica clinica di queste nuove applicazioni dovr essere valutato mediante studi di follow - up su ampie popolazioni di pazienti . 
for each episode , we retrospectively reviewed the baseline chest radiographs obtained before the diagnosis of abpa , those obtained during the course of abpa and those obtained during follow - up . 
radiographic findings that had appeared at the time of abpa diagnosis and disappeared after treatment were considered related to abpa and thus useful for a correct diagnosis of the disease . 
radiographic findings at the time of abpa diagnosis appeared to have deteriorated in 8 / 14 cases when compared with the baseline films ; after treatment , the radiographic findings deteriorated in 6 / 14 cases and improved in 6 / 14 . 
the most significant among the radiographic signs considered ( infiltrates and mucoid impaction ) appeared at the time of abpa diagnosis in 7 / 14 and 4 / 14 cases , respectively , and in some patients , they were also present at baseline and persisted during follow - up . 
the most significant abnormalities are nonspecific and commonly seen on baseline films in cystic fibrosis without abpa and persist after treatment in most cases . key words abpa cystic fibrosis in adult patients chest x - ray riassunto obiettivo . 
sono stati individuati , tra i pazienti seguiti dal centro regionale per la fibrosi cistica , 11 soggetti ( per un totale di 14 episodi di malattia ) con diagnosi di abpa . 
per ciascun episodio stato retrospettivamente analizzato lultimo radiogramma toracico antecedente la diagnosi di abpa , quello eseguito in corso di abpa e quello successivo alla terapia , ricercando la presenza di ispessimento delle pareti bronchiali , bronchiettasie , consolidamenti , atelettasie , impatti mucoidi , linfoadenopatie , versamento pleurico e livelli idro - aerei . 
il quadro radiografico alla diagnosi di abpa era , rispetto ai precedenti , peggiorato in 8 / 14 casi ; dopo terapia i reperti toracici erano peggiorati in 6 / 14 casi e migliorati in 6 / 14 . tra i segni radiografici considerati , i reperti maggiormente significativi ( consolidamenti e impatti mucoidi ) erano comparsi , alla diagnosi di abpa , rispettivamente in 7 / 14 e 4 / 14 casi e in alcuni pazienti erano presenti gi al radiogramma di base e persistevano dopo terapia . 
i risultati evidenziano la scarsa utilit del radiogramma toracico nella diagnosi di abpa nei pazienti con fibrosi cistica : le lesioni pi significative possono essere frequentemente osservate nei pazienti fibrocistici in assenza di abpa , e spesso persistono anche dopo terapia . parole chiave abpa fibrosi cistica nelladulto rx torace v . 
the disease is caused by aspergillus fumigatus ( af ) , a ubiquitous , thermotolerant fungus with a spore size of 35 thanks to these properties , if inhaled , the fungus may cause severe damage to the respiratory systethis is particularly true in subjects affected by diseases in which increased density of secretions and / or altered mucociliary clearance facilitate the trapping of spores within the bronchial lumen , as occurs in asthma and cf . there is no evidence of airway invasion by the microorganism , but persistent colonisation of the tracheobronchial tree produces a hypersensitivity reaction with immune cell activation ( t cd4 + lymphocytes ) , humoral response ( b lymphocytes producing both local and serum immunoglobulin ige , iga and igg ) and eosinophil production [ 1 , 2 , 68 ]  . 
the intense inflammatory response damages the bronchial walls , leading to central bronchiectasis and results in the formation of mucous plugs , atelectasis and eosinophilic infiltrates . clinical presentation of abpa includes the onset or acute exacerbation of dyspnoea , fever , increase in cough and sputum and at times haemoptysis , and respiratory function is deteriorated , in particular , forced expiratory volume in 1 s ( fev1 ) ] [ 16 ]  . 
chest x - ray ( cxr ) and computed tomography ( ct ) patterns of abpa are listed in table 1 [ 16 ]  . in asthma patients , abpa is diagnosed on the basis of well - defined clinical , laboratory and radiographic criteria [ 911 ]  . 
for patients with cf , the cystic fibrosis foundation consensus conference defined the following criteria for the diagnosis of abpa in 2003 [ 1 ] : acute or subacute clinical deterioration increased total serum ige ( > 1 , 000 ng / ml ) immediate cutaneous reactivity to af antigens presence of serum precipitins to af appearance of new radiographic or computed tomography alterations ( infiltrates , mucous plugs ) nonetheless , diagnosis of abpa remains difficult in cf , as some of the criteria suggested are common manifestations of the underlying disease . 
 in fact , the clinical course of cf includes frequent episodes of nonspecific infectious exacerbation with bronchial obstruction , pulmonary infiltrates , and atelectasis , which may mimic abpa [ 12 ]  . 
an immune response to af ( involving the production of ige , iga , igg antibodies and an increase in total serum ige ) may also be noted in the absence of evident abpa [ 13 ]  . 
in addition , cxr and ct alterations seen in patients with cf ( table 2 ) are almost identical to those caused by abpa [ 1416 ]  . patients with clinical suspicion of abpa are assessed with cxr to identify possible changes in the typical radiographic pattern of cf and , above all , to look for areas of consolidation . 
 several authors have used ct , and in particular high - resolution ct ( hrct ) , for the evaluation of patients with abpa . laspergillosi broncopolmonare allergica ( abpa ) una malattia da ipersensibilit , che costituisce una grave complicanza del decorso dellasma severa e della fibrosi cistica ( fc )  . 
responsabile della patologia laspergillus fumigatus ( af ) , un fungo ubiquitario in natura che , grazie alle dimensioni delle spore ( 35 m ) e alla termotolleranza pu provocare , quando inalato , danni anche gravi a carico dellapparato respiratorio , soprattutto in soggetti affetti da patologie in cui laumentata densit delle secrezioni e / o lalterata clearance mucociliare favoriscono lintrappolamento delle spore nel lume bronchiale , come avviene nellasma e nella fc . non vi evidenza di una invasione delle vie aeree da parte del microrganismo , ma la colonizzazione persistente dellalbero respiratorio provoca una reazione da ipersensibilit con attivazione dellimmunit cellulare ( linfociti t cd4 + ) , umorale ( linfociti b produttori di ige , iga e igg sia locali che sieriche ) e degli eosinofili [ 1 , 2 , 68 ]  . 
lintensa risposta infiammatoria danneggia le pareti bronchiali , con sviluppo di bronchiettasie centrali , e determina la formazione di tappi di muco , di atelettasie e di infiltrati eosinofili . clinicamente i pazienti con abpa accusano insorgenza o aggravamento della dispnea , febbre , aumento della tosse e dellescreato , a volte emottisi ; si dimostra deterioramento della funzionalit respiratoria , specie del fev1 [ 16 ]  . 
gli aspetti rx e tc della abpa sono elencati nella tabella 1 [ 16 ]  . nei soggetti asmatici la diagnosi di abpa viene formulata in base a criteri clinici , laboratoristici e radiografici , ben codificati [ 911 ]  . 
la consensus conference della cystic fibrosis foundation ha stabilito , nel 2003 , criteri diversi per la diagnosi di abpa nei pazienti affetti da fc [ 1 ] : deterioramento clinico acuto o subacuto aumento delle ige sieriche totali ( > 1000 ng / ml ) test cutaneo immediato positivo ad antigeni af presenza di precipitine sieriche dirette contro af comparsa di nuove alterazioni rx o tc ( infiltrati , tappi di muco )  . tuttavia in questi pazienti la diagnosi di abpa rimane difficile , in quanto alcuni dei criteri proposti costituiscono comuni manifestazioni della malattia di base . nel decorso della fc sono infatti frequenti episodi di riacutizzazione su base infettiva aspecifica , con ostruzione bronchiale , comparsa di infiltrati polmonari e di atelettasie , che possono simulare il quadro della abpa [ 12 ]  . 
inoltre , possibile riscontrare una risposta immunitaria allaf ( con produzione di anticorpi ige , iga , igg e aumento del titolo sierico di ige totali ) in assenza di abpa conclamata [ 13 ]  . anche le alterazioni rilevabili al radiogramma toracico e alla tc dei pazienti con fc ( tabella 2 ) sono pressoch sovrapponibili a quelle dovute ad abpa [ 1416 ]  . il radiogramma del torace viene eseguito nei pazienti con sospetto clinico di abpa per evidenziare eventuali modificazioni dei reperti tipici della fc e , soprattutto , per ricercare lesioni consolidative . 
nella pratica clinica , per , lhrtc non fa parte dei criteri diagnostici dellabpa e viene utilizzata raramente in corso di riacutizzazione di fc per le alte dosi di radiazioni , lelevato costo e la scarsa specificit ai fini diagnostico - differenziali dei reperti che possono essere riscontrati ; pertanto il paziente viene di solito valutato solo con il radiogramma standard [ 1821 ]  . in letteratura non esistono studi che abbiano valutato sistematicamente il ruolo della diagnostica per immagini nella diagnosi di abpa nei pazienti con fc . 
scopo di questo lavoro valutare la affidabilit del radiogramma standard nella diagnosi di abpa in pazienti affetti da fc e correlare i quadri radiografici con la valutazione funzionale ( fev1 )  . materiali e metodi indeed , it is more sensitive than standard radiographs , particularly in determining the extent and severity of bronchiectasis and mucoid impaction . 
in clinical practice , however , hrct is not regarded as a diagnostic tool for abpa , and it is rarely used da luglio 1994 a maggio 2005 sono stati individuati , tra i pazienti seguiti dal centro regionale per la fibrosi cisticasettore adulti , 11 soggetti ( 9 maschi e 2 femmine con et media di 22 , 1 anni ) con diagnosi di abpa , per un totale di 14 episodi di malattia ( 3 pazienti sono andati incontro a due episodi di abpa )  . table 2 radiographic alterations ( cxr and ct ) in cystic fibrosis tabella 2 alterazioni radiografiche ( rx e ct ) nei pazienti con fc increased lung volume bronchial wall thickening bronchiectasis parenchymal consolidation mucoid impaction cystic lesions interstitial thickening diffuse nodular opacities aumento dei volumi polmonari ispessimento delle pareti bronchiali bronchiettasie addensamenti parenchimali impatti mucoidi lesioni cistiche ispessimento della trama interstiziale opacit nodulari diffuse increased lung volume bronchial wall thickening bronchiectasis ( cylindrical ) parenchymal consolidation ( peribronchial ) mucoid impaction ( isointense ) cystic lesions interstitial thickening diffuse nodular opacities aumento dei volumi polmonari ispessimento delle pareti bronchiali bronchiettasie ( cilindriche ) addensamenti parenchimali ( peribronchiali ) impatti mucoidi ( isodensi ) lesioni cistiche ispessimento della trama interstiziale opacit nodulari diffuse v . 
as a result , the patient is often examined by standard cxr only [ 1821 ]  . no previous study has systematically evaluated the role of imaging in the diagnosis of abpa in patients with cf . 
the aim of this study was to assess the reliability of standard radiography in the diagnosis of abpa in patients with cf and to correlate the radiographic findings with respiratory function ( fev1 )  . materials and methods from july 1994 to may 2005 , among the patients attending the regional cystic fibrosis centre adult section , we identified 11 subjects ( nine men and two women , mean age 22.1 years ) with a diagnosis of abpa and with a total of 14 episodes of abpa ( three patients had had two episodes )  . 
 at the time of the diagnosis , all patients presented with : bronchial obstruction , as assessed by fev1 ige > 1 , 000 ng / ml positive cutaneous reaction ( af skin - prick test ) presence of anti - af ige antibodies eosinophilia ( > 500 cells / ml3 ) peripherally and in the spupositive sputum culture for af all subjects underwent oral antifungal and cortisone treatment and radiographic follow - up . for each patient , we retrospectively assessed the last cxr obtained before the diagnosis of abpa and during a phase of apparent clinical stability ( t0 ) , the cxr obtained at the time of abpa diagnosis ( t1 ) and the follow - up cxr performed after treatment ( t2 )  . 
each cxr was assessed for the presence of bronchial wall thickening , bronchiectasis , areas of consolidation , atelectasis , mucoid impaction , lymphadenopathy , pleural effusion and air - fluid levels . 
findings were evaluated after subdividing the right and left lung fields into three zones for a total of six zones : upper , from the lung apex to the carina , middle , from the carina to the inferior pulmonary veins and lower , below the inferior pulmonary veins . 
 any cxr changes that had appeared at the time of diagnosis and disappeared after treatment were considered to be related to abpa and therefore useful for correct diagnosis of the disease . 
all patients underwent respiratory function testing ( fev1 ) at baseline , at the time of the abpa diagnosis and after treatment ; a 10% change relative to the previous result was considered significant . tutti gli 11 pazienti presentavano al momento della diagnosi : ostruzione bronchiale , valutata mediante la misurazione dei valori di fev1 ; valori di ige > 1000 ng / ml ; positivit al test cutaneo immediato ( prick test per af ) ; comparsa di ige anti - af ; eosinofilia periferica ( > 500 cell / ml3 ) e nellescreato ; positivit per af dellesame colturale dellescreato . tutti i soggetti sono stati sottoposti a terapia mediante cortisonici orali e antifungini , con successivo follow - up radiografico . di ciascun paziente stato retrospettivamente analizzato , per la presenza di ispessimento delle pareti bronchiali , bronchiettasie , consolidamenti , atelettasie , impatti mucoidi , linfoadenopatie , versamento pleurico e livelli idro - aerei , lultimo rx antecedente la diagnosi di abpa eseguito in fase di apparente stabilit clinica ( t0 ) , quello cronologicamente corrispondente al momento della diagnosi ( t1 ) e quello successivo alla terapia , in corso di follow - up ( t2 )  . 
i reperti sono stati valutati suddividendo ciascun campo polmonare in 3 zone : superiore , dallapice alla carena , media dalla carena sino a livello delle vene polmonari inferiori , e inferiore al di sotto delle vene polmonari inferiori , per un totale di 6 zone . 
lintervallo di tempo trascorso tra lesecuzione del radiogramma di base e quello alla diagnosi di abpa ( t0 - t1 ) era compreso tra un minimo di 30 giorni e un massimo di 29 , 5 mesi ( media di 11 , 2 mesi ) ; lintervallo di tempo ( t1 - t2 ) tra il radiogramma alla diagnosi di abpa e radiogramma di controllo era compreso tra un minimo di 4 , 5 mesi e un massimo di 29 mesi ( media 13 , 1 mesi )  . due radiologi hanno soggettivamente valutato per consenso se tra il primo radiogramma e quello alla diagnosi di abpa e tra quello in corso di abpa e il follow - up il quadro radiografico complessivo era stabile , migliorato o peggiorato . le modificazioni del radiogramma comparse in sincronia con la diagnosi e regredite dopo terapia sono state considerate collegate alla abpa e utili per la corretta diagnosi della malattia . 
comparivano a t1 7 nuovi consolidamenti , localizzati 1 / 7 a destra nella zona superiore e 6 / 7 a sinistra ( 2 nella zona superiore , 2 nella media e 2 in quella inferiore )  . dopo terapia i 7 consolidamenti regredivano completamente . 
at t1 , seven new areas of consolidation appeared , one located in the upper right zone and six on the left ( two in the upper zone , two in the middle zone and two in the lower zone )  . 
in one patient in apparently good clinical condition , a new area of consolidation appeared in the lower right zone after treatment . atelectasis atelectasis was present in 2 / 14 cases at t0 ( both in the upper right zone ) and remained unchanged at t1 . 
another area of atelettasie erano presenti in 2 / 14 casi nel radiogramma basale ( entrambe nella zona superiore destra ) , invariate in t1 . alla diagnosi di abpa compariva , sempre nella zona superiore destra di un altro paziente , una ulteriore area di atelettasia . 
le 3 lesioni si risolvevano dopo terapia al radiogramma di follow - up . bronchiettasie bronchiettasie erano evidenti in 9 / 14 casi prima della diagnosi di abpa e , alla diagnosi , venivano considerate invariate in 6 pazienti , aumentate in 2 casi e diminuite in 1 . 
c dopo terapia laddensamento si risolve e il quadro rx sovrapponibile a quello in t0 . atelectasis , again in the upper right zone , appeared in another patient at t1 . 
dopo terapia si evidenziava una ulteriore estensione degli impatti mucoidi in 4 casi , mentre in 3 pazienti le alterazioni regredivano parzialmente . mucoid impaction mucoid impaction was seen in 7 / 14 cases at t0 . 
at t2 , an acute exacerbation of mucoid impaction was observed in four cases , whereas it had partially disappeared in three . hilar adenopathy hilar adenopathy was present in 2 / 14 cases at t0 ( on the left in one patient and bilateral in the other ) and remained unchanged on the following radiographs . 
at t2 , the cxr picture was unchanged relative to t1 in 2 / 14 cases , had adenopatie ilari erano presenti in 2 / 14 casi ( in un paziente a sinistra e nellaltro bilateralmente ) prima della diagnosi e rimanevano invariate nei radiogrammi successivi . 
complessivamente il quadro rx alla diagnosi di abpa risultava invariato in 3 / 14 casi rispetto ai precedenti , peggiorato in 8 / 14 casi ( modicamente in 2 / 8 pazienti , discretamente in 4 / 8 , gravemente in 2 / 8 ) e migliorato in 3 / 14 casi ( modicamente in 1 / 3 e discretamente in 2 / 3 )  . 
dopo terapia i reperti toracici , rispetto alla diagnosi , erano invariati in 2 / 14 casi , modicamente peggiorati in 6 / 14 casi e migliorati in 6 / 14 casi . valutazione funzionale i valori di fev1 ( volume di flusso espiratorio al primo secondo ) riscontrati e le modificazioni a cui questi sono andati incontro al momento della diagnosi di abpa e dopo terapia sono riportati nella tabella 4 . 
c al follow - up laddensamento appare completamente deterso . 9 / 14 casi si osservava una significativa riduzione del fev1 , mentre in 5 casi i valori erano sostanzialmente immodificati . dei 9 casi andati incontro ad un significativo peggioramento alla diagnosi , 7 miglioravano nettamente dopo terapia , e uno migliorava in maniera non significativa . 
nei 5 casi invariati alla diagnosi non si osservava una variazione significativa del fev1 neppure in corso di follow - up . correlazione tra reperti radiografici e valutazione funzionale nei 9 casi che a t1 avevano subito una riduzione significativa del fev1 , il quadro rx era nettamente peggiorato in 5 casi , lievemente peggiorato in 1 caso , invariato in 2 e addirittura lievemente migliorato in un paziente . 
nei 5 casi in cui la funzionalit respiratoria era stabile alla diagnosi , si osservava un peggioramento del quadro radiografico in 2 pazienti , mentre in 2 questo era migliorato . 
dopo terapia i 7 casi in cui i valori di fev1 avevano subito un netto miglioramento e quello con variazione non significativa mostravano reperti toracici migliorati ( nettamente o lievemente ) in 6 casi , lievemente peggiorati in 1 paziente e invariati in 1 ; il paziente con funzionalit respiratoria peggiorata andava incontro ad un lieve peggioramento anche del quadro radiografico . 
nei restanti 5 casi con fev1 stabile , al follow - up le modificazioni rx erano lievemente peggiorate in 3 casi , migliorate in slightly deteriorated in 6 / 14 cases and improved in 6 / 14 casfunctional evaluation the fev1 values observed at t0 , t1 and t2 are reported in table 4 . 
of the nine cases with a significant deterioration at t1 , seven had a marked improvement at t2 and one had slight improvement ; one patient only had a further decrease in fev1 at t2 . 
among the five cases with unchanged fev1 at t1 , no significant change was observed t t2 . correlation between radiographic findings and functional evaluation among the nine cases with a significant decrease in fev1 at t1 , the corresponding radiographic picture had deteriorated markedly in five cases and moderately in one , remained unv . 
among the five cases with unchanged respiratory function at t1 , the corresponding radiographic picture had deteriorated in two and improved in two ; no change was detected in one . 
among the seven cases with markedly improved fev1 and the case with a slight improvement at t2 , the corresponding radiographic picture showed either marked or moderate improvement in six , slight deterioration in one and no change in another ; the patient with decreased fev1 at t2 also had a moderate worsening in the radiographic picture . 
at t2 , fev1 had returned to the t0 levels or increased slightly in ten cases ; the radiographic picture remained unchanged or improved moderately relative to t0 in eight cases but deteriorated in two . 
in four cases , t2 fev1 decreased relative to t0 , and this finding corresponded to an unchanged radiographic picture in three cases and deterioration in one . discussion imaging diagnosis of abpa in patients affected by cf is more complicated than in asthma patients in that radiographic abnormalities caused by the disease are also frequently observed in cf patients not affected by abpa . 
in fact , bronchial wall thickening , mucoid impaction , parenchymal thickening and bronchiectasis may be identified in cf patients both during periods of clinical stability and during phases of acute exacerbation due to bacterial infections . clinical and laboratory criteria suggested by the cystic fibrosis foundation consensus conference are also nonspecific [ 1 ] , as a possible immune response with formation of af antibodies can complicate interpretation of serological para1 e invariate in 1 . 
dopo terapia le percentuali di fev1 erano ritornate ai valori riscontrati a t0 , o addirittura lievemente pi elevati , in 10 casi ; il quadro radiografico era uguale o modicamente migliorato rispetto al radiogramma basale in 8 casi , mentre in 2 era peggiorato . 
in 4 casi i valori di fev1 al follow - up erano peggiorati rispetto a quelli iniziali ; a questi corrispondeva un radiogramma toracico sovrapponibile a t0 in 3 casi e peggiorato in 1 . discussione la diagnosi radiologica di abpa in pazienti affetti da fc risulta assai pi difficile che nei pazienti asmatici in quanto le alterazioni rx indotte dalla malattia si osservano frequentemente in pazienti fc non affetti da abpa . 
infatti , gli ispessimenti delle pareti bronchiali , gli impatti mucoidi , gli addensamenti parenchimali e le bronchiettasie si possono riscontrare nei pazienti fc sia in fase di stabilit clinica , sia in corso di peggioramento dovuto a infezioni batteriche ricorrenti . 
 anche i criteri clinico - laboratoristici proposti dalla consensus conference della cystic fibrosis foundation sono aspecifici [ 1 ] : la possibile comparsa di una risposta immunitaria con la formazione di antigeni diretti contro af pu , infatti , rendere complicata linterpretazione dei vari parametri sierologici utilizzati per la diagnosi di abpa . 
lesecuzione di un radiogramma toracico richiesta routinariamente nei pazienti con fc in cui vi sia una modificazione del quadro clinico - laboratoristico e funzionale che faccia sospettare una abpa , per ricercare dei segni che possano portare ad una conferma del sospetto diagnostico . 
the most significant radiographic findings according to the cystic fibrosis foundation consensus conference , namely , areas of consolidation and mucoid impaction , were inconstantly observed at the time of the diagnosis ( 7 / 14 and 4 / 14 cases , respectively ) and therefore have limited sensitivity . 
durante il follow - up il quadro migliorato nel 42 , 8% dei pazienti , rimasto sostanzialmente invariato nel 14 , 3% dei casi , mentre si osservato addirittura un peggioramento dei reperti radiografici nel 42 , 8% dei casi . 
i reperti maggiormente significativi , in accordo con la consensus conference della cystic fibrosis foundation , e cio i consolidamenti e gli impatti mucoidi , al momento della diagnosi , sono comparsi in maniera incostante ( rispettivamente 7 / 14 e 4 / 14 casi ) , risultando quindi poco sensibili . 
anche altre lesioni che si sono osservate con elevata frequenza in tutti i tre radiogrammi considerati sono risultate poco specifiche : lispessimento delle pareti bronchiali era presente in tutti i 14 soggetti , con peggioramento nel 50% dei casi alla diagnosi e addirittura nel 42 , 8% dei casi dopo terapia ; le bronchiettasie erano presenti nella maggior parte dei casi in tutti i tre radiogrammi eseguiti , senza subire significative variazioni nel corso del tempo . 
pleural effusion and air - fluid levels were absent in all cases , whereas adenopathy remained unchanged in the two cases in which it was seen . respiratory function tests , especially fev1 , proved to be the most reliable tool for monitoring the course of abpa . 
no similar correlation was noted between the clinical course of abpa and chest radiography . conclusions our study was undertaken to assess the reliability of chest radiographs in the diagnosis of abpa in patients affected by cf . 
the results highlight that despite its fundamental role in the diagnosis and follow - up of cf , the technique suffers considerable limitations in the diagnostic and follow - up assessment of cf patients who develop abpa . 
ct and hrct have greater sensitivity but are unable to demonstrate abnormalities that are highly specific for abpa , and they cannot be used routinely to monitor cf because of costs and radiation dose . 
il versamento pleurico e i livelli idroaerei sono risultati assenti in tutti i casi , mentre le adenopatie sono rimaste invariate nei due casi in cui erano presenti . le prove di funzionalit respiratoria , in particolare il fev1 , sono risultate essere il mezzo pi oggettivo per monitorare landamento dellabpa : alla diagnosi di abpa , corrisposto un significativo ( > 10% ) peggioramento del quadro respiratorio nel 64 , 3% dei casi , mentre si osservato un declino della funzionalit non significativo nel 35 , 7% dei casi . 
una analoga correlazione col decorso clinico non si , come gi detto , ottenuta con il radiogramma del torace . conclusioni il nostro studio stato intrapreso con lo scopo di valutare laffidabilit del radiogramma del torace nella diagnosi di abpa nei pazienti affetti da fc . 
i risultati ottenuti hanno dimostrato notevoli limiti di questa metodica , pure indispensabile per la precisazione diagnostica della fc e nel followup , nella valutazione dei pazienti con fc e insorgenza di abpa , sia alla diagnosi che nel follow - up : si infatti evidenziata una scarsa correlazione tra il quadro radiografico e landamento clinico della malattia , dalla sua acuzie alla completa risoluzione . 
bartolozzi1 1divisione di radiologia diagnostica e interventistica , dipartimento di oncologia , trapianti e nuove tecnologie in medicina 2dipartimento ad attivit integrata di endocrinologia e malattie metaboliche , 3dipartimento di chirurgia , universit di pisa , dipartimento immagini , via paradisa 2 , i - 56124 pisa , italy correspondence to : s . 
we included 60 patients with primary hyperparathyroidispreoperative first - line examinations revealed negative and doubtful ultrasound ( us ) findings in 34 and 26 cases , respectively , and negative , doubtful and positive scintigraphic findings in 19 , 20 and 21 cases , respectively . 
in 8 / 10 doubtful cases , surgery confirmed the location of the lesion in five cases , identified the ectopic location of lesions in two cases , and was negative in one case . 
le indagini di primo livello dimostravano : ecografia negativa in 34 casi e dubbia in 26 casi ; scintigrafia con mibi positiva in 21 casi , negativa in 19 casi , dubbia in 20 casi . 
in 8 casi con tc dubbia , la chirurgia ha confermato la lesione nella sede segnalata in 5 casi ed in altra sede in 2 casi , mentre in 1 caso risultata negativa . 
la tcmd rappresenta una metodica accurata nel work - up diagnostico delliperparatiroidismo primario e consente una esplorazione rapida e panoramica dellintera regione cervico - mediastinica . key words parathyroid glands primary hyperparathyroidism multidetector ct parole chiave paratiroidi iperparatiroidismo primitivo tc multidetettore introduction introduzione primary hyperparathyroidism ( phpt ) consists of an alteration in phosphate and calcium metabolism characterised by liperparatiroidismo primario ( phpt ) consiste in unalterazione del metabolismo fosfo - calcico caratterizzata da ecs . 
once considered an extremely rare disease , discovered in cases of severe bone or kidney disorders only , phpt has become the third most commonly diagnosed endocrine disorder after diabetes and thyroid dysfunction . 
the disease accounts for 32% of the causes of hypercalcaemia , and the diagnosis , which is essentially biochemical , is based on the presence of hypercalcaemia associated to high levels of pth . 
however , asymptomatic cases are also frequently encountered that have no or only mild kidney and bone disorders and mild hypercalcaemia ( < 11 mg / dl )  . the estimated prevalence of phpt in the general population is 12 cases / 1 , 000 inhabitants , with a 23 : 1 female - tomale ratio . 
it is currently estimated at approximately 30 : 100 , 000 / year , although it is thought to be rising as a result of the introduction of automated methods for serum calcium determination . 
primary hyperparathyroidism may present in a sporadic ( 90% ) or familial ( 10% ) form : multiple endocrine neoplasia ( men 12 ) , familial hypocalciuric hypercalcaemia , isolated familial hyperparathyroidism associated with jaw tumours ( hpt - jaw tumour syndrome ) or familial isolated hyperparathyroidism . diagnostic imaging of hpt is aimed to identifying the presence of one or more pathological parathyroid glands , a condition that is always associated with gland enlargement and therefore detectable with imaging techniques . 
the search should take into account possible abnormalities in the number of parathyroid glands , which are present in approximately 15% of cases ; and their possible ectopic location , above all of the inferior glands , which are ectopic in 2%8% of cases ( jugulothymic in 10%30% of cases , intrathyroidal in 3%10% and retropharyngeal , retroesophageal or mediastinal in 4%8% )  . 
 ultrasound ( us ) and 99mtc - sestamibi scintigraphy are the first - line diagnostic modalities for detection of a parathyroid lesion , as they are inexpensive , easy to perform and have good detection rates . 
the limitations of us are mainly ectopic locations especially when mediastinal the difficulty in exploring the neck in the presence of a goitre and the fact that it is operator dependent . 
scintigraphy of the parathyroid glands is affected , in terms of diagnostic accuracy , by several factors , including the presence of a goitre and the mitochondrial content of parathyroid lesions [ 2 ]  . 
in the context of hyperparathyroidism , magnetic resonance imaging ( mri ) and computed tomography ( ct ) are considered second - line modalities that are indicated in cases of persistent or recurrent disease in which us and scintigraphy are negative or doubtful . 
 as a multiplanar technique , mri has a high spatial resolution that provides excellent definition of the relationships between the lesion and surrounding structures ; in addition , it permits exploration of poorly accessible areas such as the thoracic inlet and provides good tissue characterisation . 
the reported sensitivity of mri in the detection of hyperfunctioning parathyroid glands varies widely and is heavily influenced by technological advances in this field , with variations between cessiva e parzialmente incontrollata secrezione di paratormone ( pth ) da parte di una o pi ghiandole paratiroidee iperfunzionanti determinante ipercalcemia [ 1 ]  . 
da malattia estremamente rara , diagnosticata solo in caso di grave compromissione ossea o renale , lphpt divenuto il terzo disordine endocrino pi frequentemente diagnosticato dopo il diabete e le tireopatie . 
la malattia rappresenta il 32% delle cause di ipercalcemia e la diagnosi , principalmente biochimica , si basa sulla presenza di ipercalcemia associata ad elevati livelli di pth , ma sono molto frequenti i casi asintomatici con assente o lieve compromissione renale e ossea , con ipercalcemia lieve ( < 11 mg / dl )  . la prevalenza di phtp nella popolazione generale stimata di 12 casi / 1000 abitanti , con rapporto f / m 23 : 1 ; lincidenza generalmente cresce allaumentare dellet e nella sottopopolazione delle donne in et menopausale ( al di sopra dei 50 anni ) valutata in circa 30 : 100000 / anno , ma considerata in aumento dopo lintroduzione del dosaggio della calcemia con metodiche automatiche . 
lphtp pu presentarsi in forma sporadica ( 90% ) o familiare ( 10% ) : neoplasia endocrina multipla ( men 12 ) , ipercalcemia familiare ipocalciurica , iperparatiroidismo familiare isolato associato a tumori della mandibola ( hpt - jaw tumor syndrome ) , iperparatiroidismo familiare isolato . la diagnostica per immagini delliperparatirodismo finalizzata alla individuazione di una o pi ghiandole paratiroidee patologiche , condizione che si associa sempre ad un loro aumento di volume che le rende pertanto riconoscibili alle tecniche di imaging . 
tale ricerca deve tener conto di possibili anomalie di numero delle ghiandole paratiroidee , presenti complessivamente nel 15% dei casi e di eventuali localizzazioni ectopiche , specie delle ghiandole inferiori , presenti nel 2%8% dei casi ( giugulo - timica 10%30% dei casi , intratiroidea 3%10% , retrofaringea , retroesofagea o mediastinica 4%8% dei casi complessivamente )  . 
 lecografia e la scintigrafia 99mtc - sestamibi rappresentano il primo livello diagnostico nella individuazione di una lesione paratiroidea , in quanto a basso costo , di facile esecuzione ed affidabili in termini di detection rate . 
i limiti dellecografia sono rappresentati principalmente dalle localizzazioni ectopiche , mediastinica in particolare , dalle difficolt di esplorazione del collo in presenza di gozzo e dal fatto di essere una metodica operatore dipendente . 
la scintigrafia paratiroidea risulta daltronde condizionata , in termini di accuratezza diagnostica , da alcuni fattori , essenzialmente rappresentati dal gozzo e dal contenuto mitocondriale delle lesioni paratiroidee stesse [ 2 ]  . 
nellambito dellimaging delliperparatiroidismo la rm e la tc sono considerate metodiche di secondo livello e lindicazione principale rappresentata dai casi con malattia persistente o recidiva , in cui lecografia e la scintigrafia risultano negative o dubbie . la risonanza magnetica ( rm ) in quanto tecnica multiplanare , presenta una elevata risoluzione spaziale con ottima definizione dei rapporti della lesione con le strutture circostanti , permette inoltre di esplorare aree meno agevoli quali lo stretto toracico superiore e consente una buona caratterizzazione tissutale . 
the pitfalls of mri include long examination times , the need to use different coils for the study of the neck and mediastinum , the frequent presence of movement artefacts that affect image quality and poor patient compliance . 
the use of fast sequences and intravenous contrast material ( gadolinium ) enables analysis of the enhancement pattern of a nodular lesion , with the limitation that the same analysis cannot be simultaneously performed on other lesions detected in the same cervicomediastinal field . indications for the use of ct in head and neck pathology , as in other body regions , have been greatly extended as a result of technological progress , the advent of spiral scanners and the introduction of multidetector acquisition systems . the main advantages of multislice scanners are the possibility of studying large body volumes with thin slices and improved spatial resolution during relatively short examination times and the possibility to perform multiplanar reconstructions . 
 the aim of this prospective study was to evaluate the diagnostic accuracy of mdct in the detection of a primary parathyroid lesion and define its possible role in the diagnostic workup of hyperparathyroidism . materials and methods between january 2003 and june 2006 , we studied 375 patients ( 158 men , 217 women , mean age 57 years ) with clinical , biochemical and hormonal evidence suggestive of hyperparathyroidismost patients had been referred to us by the endocrinology department for a us study of the neck to search for a parathyroid lesion . 
integration of the data provided by the two first - line imaging modalities was done by the endocrinologist , who had to decide whether to refer the patient directly for surgery or in cases in which the two techniques had provided negative , doubtful or discordant results to continue the diagnostic workup . 
when both modalities were negative or doubtful , the patients underwent a second biochemical and hormonal assessment to exclude other causes of hyperparathyroidisin the event primary hyperparathyroidism was confirmed , they proceeded to a ct study to complete the diagnostic workup . 
ct studies were also done in patients with negative us but positive scintigraphic findings , especially when these raised a suspicion of ectopic location . mdct was performed in 60 patients ( 16% ) ( 15 men , 45 women , mean age 57 years ) with clinical and laboratory confirmation of hyperparathyroidism and no history of allergic reaction to iodinated contrast material . 
forty - seven patients had phpt at first surgery , seven had phpt in a context of multiple endocrine neoplasia , five had a recurrence of phpt vi sono stati in questo campo , con variazioni comprese tra il 13% e l88% [ 3 , 4 ]  . 
tra gli svantaggi della rm vanno considerati i tempi piuttosto lunghi di esecuzione dellindagine , la necessit di utilizzare bobine diverse per lo studio del collo e del mediastino , a cui si aggiunge il frequente rilievo di artefatti da movimento che alterano la qualit dellesame e la scarsa compliance allesecuzione di tale indagine da parte di molti pazienti . 
utilizzando sequenze veloci e la somministrazione di mdc ev ( gadolinio ) possibile inoltre analizzare il comportamento contrastografico di una lesione nodulare , con il limite tuttavia di non poter effettuare contemporaneamente la stessa valutazione su altre tumefazioni eventualmente incluse nello stesso campo dindagine cervico - mediastinico . le indicazioni allo studio con tomografia computerizzata ( tc ) della patologia del capo e del collo ha subito , come del resto anche in altri distretti corporei , un importante impulso grazie allavanzamento tecnologico ed allavvento di apparecchiature di tipo spirale ed allintroduzione di sistemi di acquisizione multidetettore . 
il principale vantaggio di tali apparecchiature infatti rappresentato dalla possibilit di poter studiare ampi volumi corporei con tempi di acquisizione relativamente brevi , utilizzando uno spessore di strato sottile , a vantaggio della risoluzione spaziale e della possibilit di poter eseguire elaborazioni multiplanari . 
 scopo del nostro studio , a carattere prospettico , stato quello di valutare laccuratezza diagnostica della tc multidetettore nellidentificazione di una tumefazione primitivamente paratiroidea e di definirne il possibile ruolo nel workup diagnostico delliperparatiroidismo . materiali e metodi in un periodo compreso tra gennaio 2003 e giugno 2006 sono giunti alla nostra osservazione 375 pazienti ( 158 m , 217 f , et media di 57 anni ) nei quali i parametri clinici , bio - umorali ed ormonali deponevano per un quadro di iperparatiroidismo . 
la maggior parte dei pazienti erano stati inviati c / o la nostra struttura dalluo di endocrinologia per eseguire uno studio ecografico del collo mirato alla ricerca di una tumefazione paratiroidea . 
in tutti i casi lo studio ecografico stato eseguito in cieco , ovvero senza conoscere il risultato della scintigrafia , qualora questultima fosse stata eseguita in epoca antecedente alla nostra osservazione . lintegrazione dei dati forniti dalle due metodiche di primo livello era affidata allo specialistica endocrinologo , il quale decideva se inviare il paziente direttamente allintervento chirurgico o , nei casi in cui entrambe le tecniche risultassero negative o fornissero reperti dubbi o discordanti , di proseguire liter diagnostico - strumentale . 
il work - up diagnostico utilizzato stato il seguente : in caso di positivit dellecografia e della scintigrafia il paziente veniva inviato direttamente allintervento chirurgico ; simile atteggiamento anche in caso di scintigrafia negativa , ma di chiara positivit ecos . 
thirty patients ( 50% ) had an associated thyroid disorder : chronic thyroiditis in 12 ( 20% ) , multinodular goitre ( mng ) in 18 ( 30% ) ( volume between 26 and 85 ml , average 47 ml ) and two had already undergone total thyroidectomy for goitre . 
us findings were negative in 34 cases ( 57% ) and doubtful in 26 ( 33% ) , whereas scintigraphy was positive in 21 ( 35% ) , negative in 19 ( 15% ) and doubtful in 20 ( 33% )  . 
 us and colour - doppler us studies were carried out with new - generation scanners ( technos , esaote biomedica , genoa , italy ) equipped with 7.5to 10 - mhz electronic lineararray probes . 
additional scans were obtained with the neck in the right or left lateral position to better visualise the deep tracheooesophageal cervical region where parathyroid lesions may at times be located . 
the study was judged to be positive for a primary parathyroid lesion in the presence of a nodule displaying the following features : oval or elongated shape , extraglandular perithyroid location , low echogenicity ( expression of hypercellular tissue with few interfaces ) , deformation during lateral neck movements , colour / power doppler vascular signals that were neither peripheral ( typical of thyroid nodules ) or linear intraglandular ( typical of lymph nodes ) and possible demonstration of an arterial vascular pole [ 6 ]  . scintigraphy was performed after the intravenous infusion of 555 mbq of 99mtc - sestamibi ( 2 - methoxyisobutyl isonitrile ) , a molecule that has a high affinity for glands and cells with high metabolic turnover . 
 [ 7 ] : a positive judgement for parathyroid lesion was expressed in the presence of persistent uptake of the tracer at the cervicomediastinal level at 15 min and at 3 h after clearance from the thyroid . all ct studies were performed using multidetector equipment ( lightspeed plus , general electric medical system , milwaukee , wi , usa ) , with scans at baseline and after intravenous administration of 110130 ml nonionic iodinated contrast material ( iomeron 400 , bracco , milan , italy ) at a flow rate of 3 ml / s . 
the study protocol involved a baseline scan with 5 - mm slice thickness , 5 - mm reconstruction interval , pitch 3 ( hq mode ) , 120 kv , 200 ma and single field of view ( fov ) for exploration of the neck and mediastinum ( 2025 mm )  . 
postcontrast scans were obtained 30 s and 80 s after administration of contrast material with , in both cases , a slice thickness of 2.5 mm , a reconstruction interval 1.25 mm , pitch 3 ( hq mode ) , 120 kv , 250300 ma and the same fov as used for the baseline scans . 
the field of exploration of ct study was between the mandibular angles and the plane passing just below the tracheal bifurcation . all native axial images were transferred to a dedicated workstation ( advantage windows 4.0 , general electric medical systems ) where multiplanar reconstruction studies were performed . 
quando entrambe le metodiche risultavano negative o dubbie , il paziente subiva una seconda rivalutazione bioumorale ed ormonale , mirate ad escludere altre cause di iperparatiroidismo e , in caso di conferma del quadro , era sottoposto a completamento diagnostico con tc . 
questultima era richiesta anche in presenza di negativit ecografica , ma con reperti scintigrafici positivi , specie nei casi in cui questultimi ponevano il sospetto di localizzazione ectopica . il completamento diagnostico con tc multidetettore stato eseguito in 60 pazienti ( 16% ) ( 15 m , 45 f , et media di 57 anni ) nei quali vi era riconferma clinico - laboratoristica di iperparatiroidismo ed assenza allanamnesi di diatesi allergica al mdc iodato . 
in 47 casi si trattava di phpt al primo intervento , 7 casi di phpt in neoplasia endocrina multipla ; 5 pazienti presentavano una recidiva del quadro iperparatiroideo a distanza di un periodo di remissione dal primo intervento ; un caso infine era affetto da una persistenza della malattia dopo lintervento stesso . 
in 30 pazienti ( 50% ) era associata una tireopatia : tiroidite cronica in 12 casi ( 20% ) , gozzo multinodulare ( gmn ) in 18 casi ( 30% ) ( volume compreso tra 2685 ml , media 47 ml ) ; due pazienti erano gi stati sottoposti a tiroidectomia totale per gozzo . 
in tali pazienti il controllo ecografico risultava negativo in 34 casi ( 57% ) e dubbio in 26 ( 33% ) , mentre la scintigrafia dimostrava reperti positivi in 21 casi ( 35% ) , negativi in 19 casi ( 15% ) e dubbi in 20 casi ( 33% )  . gli studi ecografici ed eco - color doppler sono stati eseguiti con apparecchi di ultima generazione ( technos , esaote biomedica , genova , italia ) provvisti di sonde lineari elettroniche da 7 , 510 mhz . 
scansioni ecografiche aggiuntive sono state effettuate con il collo in posizione laterale destra o sinistra , al fine di visualizzare meglio la regione cervicale profonda tracheo - esofagea dove le lesioni paratiroidee possono essere a volte localizzate . 
veniva espresso un giudizio positivo per lesione primitivamente paratiroidea in presenza di un nodulo con morfologia ovoidale o allungata situato in sede peritiroidea extraghiandolare , a bassa ecogenicit ( espressione di tessuto ipercellulato e con scarse interfacce ) , eventualmente deformabile nei movimenti di lateralit del collo , provvisto di segnali vascolari intralesionali alla valutazione eco - color / power doppler , privi di distribuzione periferica ( tipico dei noduli tiroidei ) o lineare intraghiandolare ( tipico dei linfonodi ) , con la possibilit di dimostrare un polo vascolare arterioso [ 6 ]  . la scintigrafia stata eseguita mediante linfusione ev di 555 mbq di 99mtc - sestamibi ( 6 - metossi - butil - isonitrile ) , molecola che mostra spiccato tropismo per le ghiandole e le cellule ad elevato turn - over metabolico . 
1 multidetector computed tomography in primary hyperparathyroidisthe axial image ( left ) and the coronal reconstruction ( right ) performed after contrast medium administration allow identification of a small , hyperdense , nodular lesion ( arrow ) , attributable to a parathyroid lesion , located close to the right thyroid lobe and the oesophagus . 
limmagine assiale ( sinistra ) e la ricostruzione sul piano coronale ( destra ) evidenziano , dopo somministrazione di mdc , la presenza di una piccola formazione nodulare iperdensa ( freccia ) riferibile a lesione primitivamente paratiroidea , contigua alla tiroide ed alla parete postero - laterale destra dellesofago . 
le acquisizioni post - contrastografiche erano effettuate dopo 30 s e 80 s dalla somministrazione di mdc utilizzando , in entrambi i casi , uno spessore di strato di 2 , 5 mm , un intervallo di ricostruzione di 1 , 25 mm , pitch 3 ( modalit hq ) , 120 kv , 250300 ma e fov uguale alle scansioni basali . 
il campo di esplorazione dellesame tc era compreso tra gli angoli mandibolari ed il piano passante subito inferiormente la biforcazione tracheale . tutte le immagini assiali native acquisite erano inviate ad una stazione di lavoro dedicata ( advantage windows 4.0 ; ge / medical systems , milwaukee , wi ) dove venivano eseguiti studi di ricostruzione multiplanare . 
il tempo dedicato agli studi di elaborazione risultava in ogni caso inferiore a 20 minuti . la tc ha espresso un giudizio di sospetta tumefazione paratiroidea in base alla sede ( extratiroidea ) della lesione , alla sua morfologia ( ovoidale o allungata ) , alleventuale dimostrazione dei vasi afferenti alla lesione ed al grado di captazione contrastografica , confrontato questultimo con fig . 
dopo somministrazione di mdc iodato la tumefazione paratiroidea era sospettata alla tc , in entrambe le fasi di acquisizione ( arteriosa e venosa ) , in presenza di un marcato enhancement contrastografico , questultimo legato alla loro caratteristica ipervascolarizzazione , con un wash - in e wash - out pressoch sovrapponibile o solo lievemente inferiore rispetto al parenchima tiroideo . 
sulla base di tali caratteri la tc ha espresso un giudizio positivo per lesione paratiroidea in 35 ( 58% ) casi , negativo in 15 ( 25% ) casi e dubbio in 10 ( 17% )  . 
i reperti tc sono stati confrontati con i reperti dellesplorazione chirurgica . risultati lintervento chirurgico stato eseguito in 40 / 60 ( 67% ) pazienti e condotto con approccio mini - invasivo in 18 casi ( 45 ) , mentre in 22 casi ( 55% ) stata effettuata una tecnica tradizionale open . 
il peso delle ghiandole paratiroidee asportato era compreso tra 15 mg e 2400 mg , con una media di 620 mg ; il diametro massimo delle lesioni risultava compreso tra 6 mm e 38 mm ( media 17 , 5 mm )  . 
dopo lescissione della tumefazione paratiroidea stato effettuato , in tutti i casi , il dosaggio intraoperatorio del pth circolante per verificare lassenza di eventuali altre lesioni o focolai di abnorme secrezione di pth . 
in tali casi la concomitante presenza di patologia tiroidea era osservata in 5 casi ( 22% ) ( 4 gmn , 1 tiroidite cronica di hashimoto ) , mentre 1 paziente ( 4% ) era stato in precedenza sottoposto ad intervento di tiroidectomia totale ; 4 pazienti ( 17% ) erano stati sottoposti a pregressa paratiroidectomia parziale . 
in 22 pazienti si trattava di una lesione singola , mentre 1 paziente risultava affetto da 2 lesioni ; in 20 casi si trattava di lesioni originate dalle ghiandole inferiori , in 4 casi da quelle superiori . in 8 casi ( 20% ) con tc dubbia lintervento chirurgico ha identificato la lesione nella sede segnalata in 5 casi ( 62 , 5% ) ( veri positivi ) , mentre in 2 casi ( 25% ) stata identificata in altra sede ( falsi positivi )  . 
on contrast - enhanced ct , a parathyroid lesion was suspected in both arterial and venous ct acquisition phases in the presence of a marked enhancement , indicating hypervascularity , with identical or only slightly slower washin and washout compared with the thyroid parenchyma . 
on the basis of the outlined criteria , ct was positive for parathyroid lesions in 35 ( 58% ) cases , negative in 15 ( 25% ) and doubtful in 10 ( 17% )  . 
la valutazione densitometrica della lesione ( p ) contigua allarco aortico , confrontata con quella di un linfonodo ( l ) a sede cervicale , in condizioni basali ( sinistra ) e dopo 30 secondi dalla somministrazione di mdc ( destra ) , permette di dimostrare la natura paratiroidea della lesione mediastinica in base al suo diverso comportamento post - contrastografico rispetto al linfonodo cervicale . results forty out of 60 ( 67% ) patients underwent surgery , with a minimally invasive approach in 18 cases ( 45% ) and an open technique in 22 ( 55% )  . 
in 2 casi le lesioni erano localizzate nelle ghiandole inferiori , in 5 casi in quelle superiori . in 9 pazienti ( 22 , 5% ) con tc negativa il chirurgo ha identificato la lesione paratiroidea in 8 casi ( 89% ) ( falsi negativi ) , mentre in 1 caso ( 11% ) lesplorazione chirurgica risultata negativa ( vero negativo )  . 
in tali pazienti lassociazione con un quadro tireopatico era osservato in 7 casi ( 5 gmn , 2 tiroidite cronica ) ; un paziente aveva subito un pregresso intervento di tiroidectomia totale . 
in 2 casi si trattava di lesioni ad origine dalle ghiandole inferiori , in 6 casi da quelle superiori . nel complesso la tc ha riportato 28 veri positivi , 8 falsi s . 
le ricostruzioni multiplanari nel piano coronale ( sinistra ) e sagittale ( destra ) permettono di evidenziare la presenza di un nodulo paratiroideo ipervascolarizzato ( freccia ) a localizzazione retrosternale situato in contiguit con un linfonodo mediastinico ( punta di freccia )  . 
five of these cases ( 22% ) had concomitant thyroid disease [ four multinodal goitre ( mng ) , one chronic hashimoto thyroiditis ] , whereas one patient ( 4% ) had already undergone total thyroidectomy and four ( 17% ) had undergone partial parathyroidectomy . 
in 20 cases , the lesions originated from the inferior glands and in four cases from the superior glands . of eight cases ( 20% ) with doubtful ct findings , surgical exploration identified the lesion in the location suggested by ct in five cases ( 62.5% ) ( true positives ) , whereas in two cases ( 25% ) , the lesion was identified in another site ( false positives )  . 
in two cases , the lesions were located in the inferior glands and in five cases in the superior glands . of nine patients ( 22.5% ) with negative ct , surgery identified the parathyroid lesion in eight cases ( 89% ) ( false negatives ) , whereas it was negative in one case ( 11% ) ( true negative )  . 
in two cases , the lesions originated from the inferior glands and in six cases from the superior glands . overall , ct yielded 28 true positives , eight false negatives , three false positives and one true negative . 
at contrast - enhanced ct , all lesions were hyperattenuating in both acquisition phases , with similar attenuation patterns to the thyroid parenchyma in all cases of lesions smaller than 2 c larger nodules showed greater hyperdensity and greater structural heterogeneity . 
dopo somministrazione di mdc iodato si osservava in tutti i casi un aspetto iperdenso delle lesioni in entrambe le fasi di acquisizione , con un comportamento densitometrico sovrapponibile a quello del parenchima tiroideo in tutti i casi di lesioni di dimensioni inferiori ai 2 cnei casi di noduli pi grandi era possibile osservare un livello di iperdensit minore ed una maggiore disomogeneit strutturale . 
gli autori a sfavore basano la loro posizione sul fatto che un chirurgo esperto comunque in grado di localizzare la paratiroide abnorme al primo intervento nel 95% dei casi , mentre le tecniche radiologiche sono , in tal senso , meno affidabili e , solo qualora adeguatamente integrate , possono raggiungere valori di detection rate maggiori del 90% ; esse inoltre risultano gravate da una percentuale di falsi positivi valutabile in circa il 25% [ 9 , 10 ]  . 
pi concordi appaiono invece le posizioni nei casi di iperparatiroidismo recidivante o persistente nei quali il successo chirurgico nettamente inferiore , valutato in circa il 60% e dove si rende pi evidente il contributo della diagnostica per immagini [ 11 , 12 ]  . 
a tale riguardo , le cause pi frequenti di insuccesso sono rappresentate dallinesperienza degli operatori , dalla soprannumerariet ghiandolare e dalle localizzazioni ectopiche , questultime con frequenza stimata intorno al 5%20% al primo intervento e 32% nei casi di phpt recidivante [ 13 ]  . gli autori a favore della localizzazione pre - operatoria basano la loro posizione sul fatto che limaging facilita in ogni caso lintervento , ne riduce i tempi e le complicanze , permette lidentificazione delle ghiandole ectopiche , le eventuali patologie associate ( tireopatie ) e quindi aiuta il chirurgo nella pianificazione dellintervento [ 14 , 15 ]  . 
il dosaggio del pth intra - operatorio , effettuato dopo lescissione della lesione , rappresenta inoltre un valido indicatore di effettiva remissione della malattia , in quanto permette di escludere la presenza di altre ghiandole abnormi e quindi di effettuare , in s . 
opponents base their views on the fact that an experienced surgeon is able to localise abnormal parathyroid glands at initial surgery in 95% of cases , whereas imaging techniques are less reliable , reaching detection rates higher than 90% only if they are adequately integrated . in addition , imaging is burdened by a false positive rate of about 25% [ 9 , 10 ]  . 
less controversy surrounds the use of preoperative imaging in recurrent or persistent parathyroidism , in which surgical success rates are definitely lower ( approximately 60% ) and where the contribution of diagnostic imaging is more evident [ 11 , 12 ]  . 
the most frequent causes of failure are operator inexperience , presence of supernumerary glands and ectopic locations , which have an estimated incidence of 5%20% at initial surgery and of 32% in cases of recurrent phpt [ 13 ]  . 
 proponents of preoperative localisation base their view on the fact that imaging in any case facilitates the operation , reduces surgical time and complications , allows identification of ectopic glands and possible associated conditions ( thyroid disease ) and therefore helps in surgical planning [ 14 , 15 ]  . 
in addition , intraoperative pth assays , done after the lesion has been excised , provide a valuable indication of effective remission , as they allow one to exclude other abnormal glands and therefore to perform , in the absence of contralateral thyroid disease , a unilateral neck exploration only [ 16 ]  . 
on the other hand , precise preoperative localisation is a prerequisite for planning minimally invasive surgery , a technique proposed by various groups , especially in the absence of goitre [ 17 , 18 ]  . the search for a parathyroid lesion generally involves the use of noninvasive imaging techniques such as us , colourdoppler us , sestamibi scintigraphy , ct and mri . 
the diagnostic accuracy of each method mainly depends on lesion location and size , the presence of concomitant thyroid disease and operator experience [ 2 , 6 , 20 ]  . in the diagnostic workup of hyperparathyroidism , us and 99mtc - sestamibi scintigraphy are considered first - line modalities capable of differentiating cervical and extracervical lesions . 
both techniques are reliable in demonstrating a parathyroid lesion with sensitivity values , in the absence of concurrent thyroid disease of approximately 90% for each technique separately and higher when the two techniques are appropriately combined . 
the presence of associated thyroid disease and / or enlarged perithyroid cervical nodes , such as those seen in chronic thyroiditis , reduce the diagnostic capabilities of both us and scintigraphy and introduce a high rate of false positive results . 
in these cases , colour - doppler us is useful for differentiating parathyroid lesions from other nodular lesions of the neck such as thyroid nodules , abnormal lymph nodes or vessels . the proposal of some authors to use us - guided interventional techniques ( such as needle aspiration for cytology or pth assays on the aspirate ) to confirm or exclude the parathyroid origin of a cervical mass in patients with hyperparathyroidism has not been unanimously accepted . 
daltronde lesatta identificazione pre - operatoria della lesione rappresenta un requisito indispensabile per una programmazione dellintervento chirurgico con approccio mini - invasivo , tecnica questultima proposta da vari gruppi , specie in assenza di concomitante gozzo [ 17 , 18 ]  . nella ricerca di una lesione paratiroidea sono in genere utilizzate tecniche di imaging non invasive quali lecografia , leco - color doppler , la scintigrafia con sestamibi , la tc e la rm . 
laccuratezza diagnostica di ogni metodica dipende essenzialmente dalla sede e dalle dimensioni della lesione , dalla presenza o meno di concomitante patologia tiroidea e dallesperienza delloperatore [ 2 , 6 , 20 ]  . nel work - up diagnostico - strumentale delliperparatiroidismo lecografia e la scintigrafia con 99mtecnezio - sestamibi ( tc - mibi ) , sono considerate le metodiche di primo livello , capaci di selezionare le lesioni situate a livello cervicale da quelle a sede extracervicale . 
entrambe si dimostrano affidabili nel dimostrare una lesione paratiroidea , con valori di sensibilit per ciascuna di esse , in assenza di concomitante patologia tiroidea , valutata in circa il 90% , con un apporto diagnostico superiore quando le due tecniche vengono opportunamente integrate . 
la presenza di tireopatia associata e / o di linfoadenomegalie cervicali a sede peritiroidea , quali ad esempio quelle che usualmente accompagnano la tiroidite cronica , riducono la capacit diagnostica sia dellecografia che della scintigrafia ed introducono elevati falsi positivi . 
in questi casi leco - color doppler si dimostrato un utile completamento diagnostico nel differenziare le lesioni paratiroidee da altre lesioni nodulari del collo quali i noduli tiroidei , i linfonodi , i vasi . la proposta di alcuni autori di utilizzare tecniche interventistiche ecoguidate ( quali lago - aspirato per lanalisi citologica o il dosaggio del pth sullago - aspirato ) al fine di confermare o escludere la natura paratiroidea di una tumefazione cervicale in pazienti affetti da iperparatiroidismo , non da tutti condivisa , per la limpossibilit spesso da parte del citologo di distinguere le cellule paratiroidee da quelle tiroidee e per il rischio di contaminazione emorragica della loggia paratiroidea stessa ( evento questultimo possibile in considerazione del carattere ipervascolare di tali lesioni ) che pu aumentare le difficolt chirurgiche e le complicanze post - chirurgiche e , specie nei casi di approccio mini - invasivo , indurre a procrastinare lintervento stesso [ 21 , 22 ]  . dopo lesecuzione delle due indagini di primo livello si possono configurare quattro situazioni : la positivit delle due metodiche , la positivit ecografica e la negativit scintigrafica , risultati negativi per entrambe le tecniche ed infine reperti ecografici negativi , ma scintigrafici positivi . 
the same approach is adopted in the case that scintigraphy is negative but us reveals the presence of a primary parathyroid mass having typical location , morphostructural characteristics and colour - doppler pattern . in our study , multidetector ct was used as a second - line modality in cases of negative us and scintigraphy or negative us but positive scintigraphy , situations that are often accompanied by multinodular goitre or are suspicious for ectopic location . 
our series did not include patients who underwent mri as a second - line investigation , a technique we use in patients with a history of iodine allergy or those who refuse iodinated contrast material . 
of the 375 patients studied , only 16% required ct to complete the diagnostic workup , confirming that first - line modalities are able to adequately screen patients in most cases . 
in the presence of thyroid disease , ct proved to be more reliable in recognising the inferior glands ( 92% of cases ) than the superior glands ( 47% of cases )  . 
of the cases with doubtful or negative ct , 73% had lesions in the superior glands and 27% in the inferior glands . this is related to the fact that lesions arising from the inferior glands are more readily distinguished on postcontrast images , as they are hyperdense relative to extranodal tissues ( cellular fat , muscle , oesophagus or trachea )  . 
in addition , lesions originating from the superior parathyroid glands may frequently display a thin , elongated appearance , as they develop in a confined space delimited by rigid structures such as the vertebral spine or trachea posteriorly and the thyroid parenchyma anteriorly , especially if the thyroid is nodular . 
in such cases , the parathyroid lesion may easily be confused with a lobulation of the thyroid parenchyma from which it is difficult to differentiate , even on multiplanar reconstructions . 
a completely different scenario is when the parathyroid lesion needs to be differentiated from the lymph nodes , which occurs almost constantly in the presence of concomitant chronic hashimoto thyroiditis . 
in our study , this association was detected in five patients , and in all of them , ct enabled differentiation of the two lesions by revealing different enhancement patterns , a renel nostro studio abbiamo utilizzato la tc multidetettore , quale metodica di secondo livello , in caso di negativit sia dellecografia che della scintigrafia o in presenza di positivit solo scintigrafica , situazioni spesso accompagnate da un concomitante gozzo multinodulare o che facevano sospettare una localizzazione ectopica . 
in questa casistica non sono stati inclusi quei pazienti che , nellambito di un accertamento di secondo livello , sono stati studiati con rm , metodica in diversi casi da noi comunque utilizzata , come ad esempio in quei pazienti che presentavano una storia di allergia allo iodio o che rifiutavano la somministrazione di mdc iodato . 
nellambito dellampia popolazione di pazienti da noi osservata ( n = 375 ) solo nel 16% dei casi si reso necessario il completamento con tc , a conferma che nella maggior parte dei casi le metodiche di primo livello sono in grado di poter effettuare una valida selezione . 
in presenza di tireopatia la tc si dimostrata pi affidabile nel riconoscere le ghiandole della loggia inferiore ( 92% dei casi ) rispetto a quelle della loggia superiore ( 47% dei casi ) e nei casi con tc dubbia o negativa le lesioni erano localizzate alle ghiandole superiori nel 73% dei casi ed alle ghiandole inferiori nel 27% . 
questo dato in relazione al fatto che le tumefazioni ad origine dalle ghiandole inferiori possono essere pi facilmente distinte in fase post - contrastografica , in base al loro aspetto iperdenso , rispetto ai tessuti extranodulari , questi ultimi rappresentati da cellulare adiposo , muscoli , esofago o trachea . 
non infrequentemente inoltre le lesioni a partenza dalle ghiandole paratiroidee superiori possono assumere un aspetto allungato ed esile in quanto vengono a svilupparsi in uno spazio anatomico ristretto , delimitato posteriormente da strutture rigide quale la colonna vertebrale o la trachea ed il parenchima tiroideo anteriormente , specie se questultimo sede di noduli ; in tali casi la paratiroide patologica pu pertanto essere facilmente confusa con una lobatura del parenchima tiroideo dal quale risulta mal differenziale anche ricorrendo a ricostruzioni multiplanari . ben diverso il caso in cui la lesione paratiroidea deve essere differenziata dai linfonodi , situazione che si verifica pressoch costantemente in presenza di una concomitante tiroidite cronica di hashimoto . 
i linfonodi di accompagnamento della tiroidite si localizzano spesso nella stessa sede dove normalmente vengono ricercate le ghiandole paratiroidee abnormi ed il loro carattere morfo - strutturale spesso simile ; in queste situazioni sia lecografia che leco - color doppler forniscono dati incerti . 
nel nostro studio questa associazione stata rilevata in 5 pazienti ed in tutti i casi la tc ha permesso di differenziare le due lesioni sulla base di un diverso comportamento contrastografico , espressione di una diversa cellularit e vascolarizzazione . 
un valido aiuto ci stato offerto , in tal senso , soprattutto nei casi in cui le lesioni originavano dalle ghiandole inferiori , dalla individuazione angio - tc dellarteria tiroidea inferiore e dei piccoli vasi arteriosi afferenti alla lesione stessa . 
in this respect , especially in cases of lesions arising from the inferior glands , we were greatly aided by the ct - angiography identification of the inferior thyroid artery and small arteries supplying the lesion . 
even in patients with previous neck surgery ( two with total thyroidectomy and four with partial parathyroidectomy ) , ct allowed reliable identification of the lesions in 5 / 6 cases ( 83% )  . 
one limitation emerged in patients with previous total thyroidectomy , where , especially in the case of small lesions , the technique did not allow differentiation of parathyroid nodules from residual thyroid tissue on the basis of enhancement alone . 
even in this case , analysis of the vessels supplying the lesion helped our interpretation . all the ectopic lesions in our series were successfully recognised at ct , which proved to be more reliable than the older ct scanners in this respect , although very similar to them in the case of mediastinal locations . 
finally , in patients undergoing first surgery and in the four cases of recurrent phpt , ct had a sensitivity of 86% and 100% , respectively . these data are considerably higher than those reported in the literature , which range from 50% to 70% in phpt and 46% to 60% in recurrences . conclusions in conclusion , mdct proved to be an accurate second - line investigation that enabled fast exploration of the entire cervical and upper mediastinal region and was able to defining the relationships between parathyroid lesions and vascular structures and to differentiate parathyroid lesions from other cervical structures such as lymph nodes . 
 pregressa chirurgia sul collo ( 2 con tiroidectomia totale e 4 con paratiroidectomia parziale ) la tc si dimostrata affidabile ed ha permesso il riconoscimento delle lesioni in 5 / 6 casi ( 83% )  . 
nei pazienti sottoposti a pregressa tiroidectomia totale un limite della metodica si dimostrata , soprattutto nei casi di lesioni piccole , per la difficolt di poter differenziare , sulla base del solo comportamento contrastografico , i noduli paratiroidei dai residui ghiandolari tiroidei ; anche in questultimo caso tuttavia ci siamo aiutati con lanalisi dei vasi afferenti alle lesione . le lesioni ectopiche da noi osservate sono state in tutti i casi riconosciute dallesame tc , confermandosi in tal senso pi affidabile rispetto ad apparecchiature tc meno recenti , ma pressoch sovrapponibile a questultime limitatamente alle localizzazioni mediastiniche . 
martingano2 1uo di radiologia , universit magna graecia di catanzaro , campus di germaneto , viale europa , i - 88100 catanzaro , italy 2uco di radiologia , universit di trieste , ospedale di cattinara , strada di fiume 447 , i - 34149 trieste , italy correspondence to : o . 
other advantages of mri are high - contrast resolution and multiplanar view , as well as extensive coverage of the skeleton with whole - body mri ( wbmri )  . 
according to some authors much work remains to be done to improve sensitivity and specificity of mri in order to define the real clinical value of this imaging modality in the multidisciplinary management of patients with a haematological malignancy . 
this article presents recent developments and perspectives in the use of mri in oncohaematological diseases . key words haematology bone marrow magnetic resonance imaging tissue characterisation contrast enhancement whole body bone marrow diseases riassunto la risonanza magnetica ( rm ) ha aperto nuove possibilit alla radiologia diagnostica per la valutazione del midollo osseo . 
altri vantaggi della rm sono rappresentati dallelevata risoluzione di contrasto e dalla visione multiplanare , assieme ad unampia copertura dello scheletro , fino alla rm whole body ( wbmri )  . 
tuttavia la specificit delle alterazioni di segnale bassa , perci i reperti di rm devono essere integrati con la clinica e i risultati di laboratorio assieme alla valutazione ematologica ed oncologica . la rm fornisce informazioni che aiutano la diagnosi , lo staging ed il follow - up di diverse malattie del midollo osseo . 
secondo alcuni autori molto lavoro deve ancora essere fatto per migliorare la sensibilit e la specificit della rm e per definire il reale valore clinico di questa modalit di imaging nella gestione multidisciplinare del paziente con una neoplasia ematologica . questo articolo presenta i recenti sviluppi e le prospettive nelluso della rm nelle patologie oncoematologiche . parole chiave ematologia midollo osseo risonanza magnetica caratterizzazione tissutale contrast enhancement whole body malattie midollo osseo introduction introduzione in oncohaematology and haematology , diagnosis and determination of disease stage , prognostic factors and response to treatment are of remarkable value in adjusting the initial treatment to the spread and aggressiveness of the disease to avoid overor undertreatment during the course of the disease and to enable different therapies to be compared [ 13 ]  . microscopic evaluation of bone marrow specimens from blind aspirations and biopsies remains fundamental for determining diagnosis , treatment and prognosis . 
biopsy or asin ematologia ed in oncoematologia estremamente importante stabilire la diagnosi , lo stadio di malattia , i fattori prognostici e la risposta al trattamento , in modo da poter bilanciare il trattamento iniziale alla diffusione e allaggressivit della patologia , evitare sovra o sottodosaggi e comparare differenti trattamenti [ 13 ]  . 
la valutazione microscopica dei campioni di midollo osseo da aspirati eseguiti alla cieca o da biopsie mantiene il suo ruolo fondamentale nel determinare la diagnosi , la prognosi e il trattamento da intraprendere . 
furthermore , whereas many haematological disorders are known to diffusely infiltrate the axial bone marrow , the overall distribution of disease can be heterogeneous on a length scale , precluding an accurate and definitive assessment via an aspirate or a biopsy from a single site [ 46 ]  . magnetic resonance imaging ( mri ) is the only imaging technique that allows direct visualisation of bone marrow , and it is the most sensitive . 
it is a noninvasive technique that complements bone marrow aspirations and biopsies by sampling a large volume of bone marrow and providing information that aids in diagnosis , staging and follow - up of bone marrow disease [ 46 ]  . 
therefore mri findings need to be integrated with clinical and laboratory findings as well as with haematological and oncological evaluation [ 2 , 4 ]  . imaging techniques many pulse sequences are available for bone marrow mri . mr appearance of bone marrow is highly dependent on the pulse sequence used and the relative amounts of fat and water within the marrow . 
conventional spin echo ( se ) t1weighted sequence is effective for imaging bone marrow due to its capability in showing the different signal intensity of red and yellow marrow , to the relatively high sensitivity in detecting bone marrow pathology and to good image quality and relatively short imaging time [ 411 ]  . 
limitations of se t1 - weighted sequence include low specificity , as most bone marrow disorders exhibit low signal intensity , and relatively low sensitivity in detecting pathology in children due to the similarity of signal intensity characteristics of normal red marrow with the predominant low signal of bone marrow disorders with this sequence [ 1214 ]  . se t2 - weighted sequence shows good sensitivity in detecting bone marrow pathology and allows good definition of the fluid component of the lesion . 
fse t2 - weighted sequences can be combined with frequency - selective fat suppression to improve the conspicuity of marrow lesions [ 15 ]  . biopsie e gli aspirati campionano solitamente un volume non superiore a 0 , 1 cm3 rispetto ad un volume totale di midollo potenzialmente attivo superiore ai 1000 cm3 . 
inoltre , sebbene molte patologie ematologiche infiltrino diffusamente il midollo osseo assiale , la generale distribuzione della malattia pu essere eterogenea in estensione , impedendo una valutazione accurata e definitiva qualora si utilizzi un aspirato o una biopsia provenienti da una singola sede [ 46 ]  . la risonanza magnetica lunica tecnica in grado di visualizzare direttamente il midollo osseo ed la pi sensibile . una tecnica non invasiva complementare allaspirato o alla biopsia midollare che consente di studiare un ampio volume di midollo e fornisce informazioni utili per la diagnosi , lo staging ed il follow - up delle malattie del midollo osseo [ 46 ]  . 
recentemente la disponibilit di gradienti pi veloci e di lettini a rapido movimento hanno aperto la strada alla rm whole body nellindividuazione delle malattie del midollo osseo [ 710 ]  . 
dal momento che le caratteristiche di segnale delle lesioni focali e multifocali non sono specifiche per la diagnosi , la rm del midollo osseo deve essere interpretata nel contesto clinico ; pertanto i reperti di risonanza devono essere integrati con quelli clinici e laboratoristici , assieme alla valutazione ematologica ed oncologica [ 2 , 4 ]  . tecniche di imaging per limaging rm del midollo osseo sono oggi disponibili numerose sequenze . 
la sequenza spin echo ( se ) convenzionale t1 - pesata una sequenza efficace per lo studio del midollo osseo , grazie alla capacit di evidenziare la differente intensit di segnale del midollo rosso e giallo , alla capacit sufficientemente elevata di individuare la patologia del midollo osseo , alla buona qualit di immagine e al tempo di acquisizione relativamente breve [ 411 ]  . 
gli svantaggi della sequenza se t1 - pesata comprendono la bassa specificit , dal momento che la maggior parte delle malattie del midollo osseo ha bassa intensit di segnale , e la sensibilit relativamente bassa in et pediatrica , a causa della somiglianza di intensit di segnale fra il midollo rosso normale e il basso segnale delle patologie midollari in questa sequenza [ 1214 ]  . la sequenza se t2 - pesata dotata di una buona sensibilit nellindividuazione della patologia midollare e permette una buona definizione della componente fluida delle lesioni , tuttavia la qualit di immagine spesso scarsa e il tempo di acquisizione lungo . le sequenze fast se t2 pesate ( fse ) hanno ampiamente rimpiazzato le convenzionali se t2 - pesate grazie alla notevole riduzione del tempo di esame . 
tuttavia , nonostante questo vantaggio e la buona qualit di immagine , la sequenza fse t2 - pesata presenta uno svantaggio importante che ne limita limpiego , rappresentato dallelevato segnale provereduction of fat signal intensity can be obtained with many sequences , which use different mechanisms to cancel the fat signal and enhance lesion visibility . 
the most widely used fat - suppressed sequence for bone marrow imaging is the stir sequence [ 15 ]  . diffusion - weighted imaging has been recently used for vertebral bone marrow evaluation based on the assumption that interstitial water increase in bone marrow oedema due to benign compression fractures can be differentiated from restricted motion of water molecules in tumour cell infiltration [ 16 , 17 ]  . 
data published in the literature suggest that diffusion - weighted sequences are an additional tool for differentiating vertebral fractures due to osteoporotic collapse with bone marrow oedema and metastatic collapse , and this might be helpful for monitoring response to therapy in metastatic disease [ 18 ]  . selective water and fat imaging methods or imaging with and without fat suppression have been used for quantitative evaluation of signal strengths and relaxation times to obtain more specific information on the response of haematological diseases to therapy . 
in addition to imaging , 1h - mr spectroscopy of red vertebral bone marrow has been proposed for diagnosis and follow - up in patients with bone marrow malignancies such as leukaemia , lymphoma and myeloma [ 1923 ]  . after gadolinium injection , normal bone marrow shows no signal intensity changes on t1 - weighted images , and measurements show no or only little increase . 
contrast - enhanced mr imaging with opposedphase gradient - echo sequences showing haematopoietic bone marrow with low signal intensity as opposed to intermediate intensity of fat marrow has proved to be suitable for demonstrating bone marrow involvement . 
la sequenza fse t2 - pesata deve comunque essere combinata con la tecnica a soppressione selettiva del grasso , per migliorare la visibilit delle lesioni midollari [ 15 ]  . 
la riduzione di intensit del segnale del grasso pu essere ottenuta con diverse sequenze che utilizzano differenti meccanismi per cancellare il segnale del grasso e migliorare la visibilit delle lesioni . 
vi sono quattro tipi principali di sequenze a soppressione del grasso : la short ti inversion recovery ( stir ) , la saturazione selettiva , le sequenze a chemical shift e ad opposizione di fase . 
la sequenza a soppressione del grasso pi usata nellimaging del midollo osseo la sequenza stir [ 15 ]  . limaging di diffusione stato recentemente usato per la valutazione del midollo osseo vertebrale , in base al principio che laumento di liquido interstiziale nelledema del midollo osseo dovuto ad una frattura da compressione benigna differenziabile dalla ridotta mobilit delle molecole dacqua che si ha nellinfiltrazione di cellule tumorali [ 16 , 17 ]  . 
i lavori pubblicati in letteratura riportano che le sequenze di diffusione sono uno strumento addizionale per differenziare le fratture vertebrali dovute ad un crollo osteoporotico con edema midollare dal crollo metastatico e questo pu essere utile per monitorare la risposta alla terapia nella malattia metastatica [ 18 ]  . i metodi di imaging selettivo per lacqua e per il grasso , con o senza la soppressione del grasso , sono stati usati per la valutazione quantitativa dellintensit di segnale e dei tempi di rilassamento cos da ottenere informazioni pi specifiche sulla risposta alle terapie delle patologie ematologiche . 
accanto allimaging , la spettroscopia 1h - rm del midollo rosso vertebrale stata proposta per la diagnosi ed il follow - up terapeutico nei pazienti con neoplasie del midollo osseo come la leucemia , il linfoma ed il mieloma [ 1923 ]  . dopo liniezione di gadolinio il midollo osseo normale non mostra alterazioni dellintensit di segnale nelle sequenze t1 - pesate e le misurazioni dimostrano solo un lieve aumento di segnale o nessun aumento . 
limaging rm dopo contrasto con le sequenze gradient - echo ad opposizione di fase , in cui il midollo ematopoietico ha una bassa intensit di segnale , diversamente dallintensit intermedia del midollo adiposo , si dimostrato adatto ad evidenziare il coinvolgimento del midollo osseo . 
luso dellimaging dopo contrasto in risonanza magnetica , particolarmente con le sequenze dinamiche , per lo studio dei pazienti con coinvolgimento midollare nelle malattie onco - ematologiche sta aumentando . dal punto di vista del contenimento dei costi , luso del mezzo o . 
mri criteria for normal bone marrow are based not only on t1 - weighted signal intensity analysis but also on enhancement time curve ( etc ) analysis , both of which warrant further evaluation in patients with bone marrow diseases [ 2426 ]  . recently , ultrasmall , superparamagnetic iron oxide particles have been developed for evaluation of phagocytic activity of bone marrow . 
ultrasmall particles are taken up by the reticuloendothelial system of bone marrow to reduce the t1 and t2 signal of normal marrow , thus improving contrast between infiltrated and normal marrow [ 28 ]  . new developments in mri equipment allow coronal images ( se t1 - weighted and stir images ) of the entire skeleton [ whole - body mri ( wbmri ) ] to be obtained by a tablemoving technique in a matter of minutes . 
the maximal longitudinal field of view ( fov ) is 180210 c the larger fov enables head - to - toe scanning of most adult patients without repositioning of the patient [ 30 ]  . 
it is necessary to acquire t1 - weighted and stir images for different stations , from head to feet , by using the combination of moving tabletop , table extender and image - melding software [ 31 ]  . in the evaluation of bone metastatic disease , lymphoma and myeloma , sagittal images of the spine are acquired employing tse t1 , t2 and stir sequences . 
interpretation may generally take place in as little as 1015 min [ 9 ]  . mri of normal bone marrow normal bone marrow is dynamic , and this produces a wide spectrum of appearances of bone in mri . 
normal haematopoietically inactive , hypocellular , fatty or yellow marrow consists of apdi contrasto in rm deve , come minimo , avere la potenzialit di modificare la diagnosi e la prognosi . 
la decisione di impiegare il mezzo di contrasto deve essere diretta ad ottenere risposta ad uno specifico quesito diagnostico che non possa essere risolto con metodi pi semplici [ 26 , 27 ]  . lenhancement dinamico del midollo osseo normale fortemente influenzato dallet e dal contenuto di grasso . lenhancement midollare diminuisce marcatamente allaumentare dellet e con la conversione adiposa , nonostante una variabilit interindividuale . 
alcuni autori ritengono che lenhancement midollare non sia adeguatamente valutabile con le sequenze spin - echo t1 - pesate , ma possa essere analizzato utilizzando sequenze dinamiche ultraveloci , che comportano unelevata risoluzione temporale ed una forte pesatura in t1 . 
i criteri di imaging di rm per definire il midollo osseo normale non sono basati sulla sola analisi dellintensit di segnale in t1 , ma anche sui dati di analisi della curva temporale di enhancement ( etc ) , che forniscono , entrambi , informazioni aggiuntive per la valutazione del paziente con malattia del midollo osseo [ 2426 ]  . recentemente sono state sviluppate particelle superparamagnetiche di ossido di ferro di piccole dimensioni per valutare lattivit fagocitaria anche nel midollo osseo . 
le piccole particelle sono captate dal sistema reticolo - endoteliale del midollo osseo e riducono il segnale t1 e t2 del midollo normale , migliorando cos il contrasto fra midollo normale ed infiltrato [ 28 ]  . i nuovi sviluppi nellapparecchiatura di rm permettono di ottenere immagini coronali ( se t1 - pesate e stir ) dellintero scheletro ( rm whole body ) nel tempo di minuti , utilizzando una tecnica con movimento del tavolo . 
il massimo campo di vista ( fov ) longitudinale di 180210 cil fov pi grande permette una scansione dalla testa ai piedi della maggior parte dei pazienti adulti senza necessit di riposizionare il paziente [ 30 ]  . 
necessario acquisire immagini t1 - pesate e stir per le differenti stazioni , dalla testa ai piedi , usando una combinazione di lettino portapazienti movibile , estensione del lettino e software di integrazione dellimmagine [ 31 ]  . nella valutazione della malattia metastatica dellosso , del linfoma e del mieloma , vengono acquisite anche immagini sagittali della colonna vertebrale utilizzando sequenze spin - echo t1 , t2 e stir . 
le immagini vengono quindi riallineate velocemente utilizzando software dedicati per facilitare la visione panoramica immediata , migliorata dallo scorrimento individuale delle immagini in cine - loop alla workstation . proximately 15% water , 5% protein and 80% fat . 
with aging , the fat content of cellular marrow increases so that by the age 70 , cellular marrow is approximately 30% water , 60% fat and 10% protein . at birth , most of marrow contains haematopoietic cells because of the high demands for blood by the neonate . 
this is true also for the appendicular skeleton [ 1 , 2 , 4 , 1113 , 32 ]  . haematopoietic marrow hyperplasia represents a deviation from the accepted adult red - yellow pattern distribution . this variation in red marrow distribution is generally discovered as an incidental finding on routine knee mri examination . 
its prevalence varies from 0.7% to 35% of the healthy population . large residual red marrow islands represent a physiological variation of the normal adult pattern in women , obese subjects and cigarette smokers , and in marathon runners with sports anaemia [ 1 ]  . normal age - related distribution of haematopoietic and fatty marrow has to be taken into account in the interpretation of images [ 32 ]  . 
understanding the possible variability is also a prerequisite to the interpretation of mr images of bone marrow pathology . mri of abnormal bone marrow signal intensity of bone marrow reflects its major components . 
there are three mri patterns of abnormal marrow that reflect different types of histological infiltration of bone marrow : focal pattern diffuse homogeneous pattern diffuse heterogeneous ( variegated or salt - and - pepper ) pattern the patterns of bone marrow involvement are not specific [ 16 ]  . 
the focal pattern of marrow involvement is characterised by the presence of an area of normal marrow replacement , generally but not always with low signal intensity on t1 - weighted images and variable signal intensity on t2 - weighted images . 
appearance of bone marrow on mri sometimes remains normal in patients with biopsy - proven marrow disease . classification of bone marrow changes according to their pathophysiological mechanisms has gained general acceptance [ 16 ]  . 
con linvecchiamento , il contenuto adiposo del midollo cellulare aumenta cos che a 70 anni il midollo cellulare composto da 60% grasso , 30% acqua e 10% proteine . alla nascita , a causa dellelevata richiesta di sangue del neonato , la maggior parte del midollo contiene cellule ematopoietiche . 
levoluzione graduale del midollo osseo da rosso a giallo durante laccrescimento pu presentare una variabilit interindividuale , particolarmente a livello vertebrale , ma anche a livello dello scheletro appendicolare [ 1 , 2 , 4 , 1113 , 32 ]  . liperplasia del midollo ematopoietico rappresenta una deviazione dal pattern normale di distribuzione rosso - giallo delladulto . 
ampie isole residue di midollo rosso rappresentano una variazione fisiologica del pattern normale adulto nelle donne , negli obesi , nei fumatori di sigarette e nei maratoneti con anemia dello sportivo [ 1 ]  . la normale distribuzione et - correlata del midollo ematopoietico ed adiposo deve essere presa in considerazione , quando si interpretano le immagini [ 32 ] , poich la conoscenza della possibile variabilit degli aspetti in funzione dellet rappresenta un prerequisito indispensabile allinterpretazione delle immagini di rm nella patologia del midollo osseo . rm del midollo osseo patologico lintensit di segnale riflette i componenti principali del midollo osseo . 
bone marrow ischaemia is the death of bone and red cells . myeloma mm is the most common primary tumour arising in bone , accounting for 10% of haematological malignancies and 1% of all malignant diseases . 
the staging system devised by durie and salmon was based on serum haematological , urinary bence - jones protein and skeletal survey findings [ 33 ]  . more marrow lesions are detected with mri than with plan radiograph or bone scan . 
vi sono tre pattern di rm del midollo patologico , che riflettono i tipi istologici di infiltrazione del midollo osseo : pattern focale ; pattern diffuso omogeneo ; pattern diffuso eterogeneo ( aspetto variegato a sale e pepe )  . i pattern di coinvolgimento del midollo osseo non sono specifici [ 16 ]  . 
il pattern focale di coinvolgimento midollare caratterizzato dalla presenza di unarea di sostituzione del midollo normale generalmente , ma non sempre , con bassa intensit di segnale nelle sequenze t1 - pesate ed intensit di segnale variabile nelle sequenze t2 - pesate . 
laspetto del midollo osseo in rm talvolta rimane normale anche nei pazienti in cui la malattia midollare dimostrata alla biopsia . la classificazione delle variazioni del midollo osseo in base al loro meccanismo fisio - patologico generalmente aco . 
spinecho ( se ) t1 - weighted image of the hip shows the typical salt - and - pepper pattern of bone marrow ( b ) , which is better seen on the turbo short t1 inversion recovery ( t - stir ) image ( c )  . 
limmagine se t1 - pesata mostra il tipico pattern pepe e sale del midollo osseo ( b ) , che si dimostra meglio nellimmagine t - stir ( c )  . 
alla t - stir della colonna toraco - lombare si vede il pattern pepe e sale diffuso del midollo osseo e una lesione focale di l1 ( e )  . have a solitary bone plasmocytoma . 
progression to systemic disease in patients with solitary bone plasmocytoma has been attributed to growth of previously occult disease [ 5 , 35 ]  . mri should be part of the staging procedures in patients with solitary bone plasmocytoma to better assess the local extent of the tumour , define radiation portals and search for other unanticipated foci of disease . 
some authors emphasise the role of mdct in combination with mri for staging these tumours . mdct is markedly superior to conventional radiography and allows more precise assessment of bony destruction [ 36 ]  . 
other authors emphasise the role of nuclear medicine in solitary myeloma to exclude other involved sites [ 37 ]  . a well - recognised contribution of mri in the management of patients with mm is the evaluation of patients with neurological symptoms . 
in possible acute spinal cord compression , mri is the first , and often the only , examination to perform [ 3 ]  . the staging system of durie and salmon [ 33 ] developed in cettata [ 16 ]  . 
lischemia del midollo osseo la morte dellosso e delle cellule ematopoietiche . mieloma il mieloma multiplo ( mm ) il tumore primitivo dellosso pi comune , rappresentando il 10% delle neoplasie ematologiche e l1% di tutte le neoplasie . 
il sistema di stadiazione proposto da durie e salmon era basato sui reperti laboratoristici del sangue , sulle proteine di bence - jones urinarie e sulle radiografie dello scheletro [ 33 ]  . 
proposed implementation of mri in the staging system of durie and salmon [ 35 ]  . the combination of mri in the staging system of durie and salmon provided the best results with respect to survival . 
because the spine covers a large portion of the red marrow and it is the major site of involvement in patients with mm , the spine is ideally suited for staging the extent of bone marrow involvement [ 35 ]  . wbmri allows direct visualisation of actual tumour burden within the bone marrow [ 9 ] : in the stage with slight interstitial plasma cell infiltration ( < 20% in bone marrow biopsy ) , a normal - looking bone marrow signal is found in all sequences . 
 because the importance of mri for sensitive detection and prognostic significance of bone marrow infiltrates has been well demonstrated , durie and coworkers recently created the durie and salmon plus staging systems [ 39 ]  . 
concerning diagnostic imaging , mri and fluorodeoxyglucose positron emission tomography ( fdg - pet ) were included for staging patients with mm : a three - grade scale for spinal mri has been recently implemented in the clinical staging systems of durie and salmon . selection of therapy is based upon this classification [ 39 ]  . however , traditional mri protocols often do not include the skull , sternum or ribs , which are areas with large amounts of red marrow and represent frequent sites of infiltration . 
in future studies , a large series of patients and different staging systems inclusive of mri should be evaluated and compared with staging without the inclusion of mri . mri bone marrow surveys in patients with mm demonstrate the broad spectrum of involvement , treatment results , areas of potential complications and sites of focal disease for safe bone biopsy . 
recently , some authors have suggested the use of dynamic contrast - enhanced mri for diagnosing and grading bone marrow involvement in patients with lymphoproliferative disease and diffuse bone marrow infiltration as well as for evaluating treatment response [ 42 , 43 ]  . precedentemente occulta [ 5 , 35 ]  . 
la rm dovrebbe essere parte delle procedure di stadiazione nei pazienti con plasmocitoma osseo solitario per meglio determinare lestensione locale del tumore , per definire il campo dirradiazione e per ricercare altri foci di malattia non precedentemente conosciuti . 
la soppressione del grasso fornisce un elevato contrasto fra i foci tumorali ed il midollo normale . la rm pu riconoscere foci occulti dinteressamento mielomatoso e pu prevedere un decorso di malattia pi sfavorevole . 
altri autori enfatizzano il ruolo della medicina nucleare nel mieloma solitario per escludere altri siti di coinvolgimento [ 37 ]  . un contributo ben conosciuto della rm , nella gestione dei pazienti affetti da mieloma multiplo , la valutazione dei pazienti che presentano sintomi neurologici . 
daltra parte la tc permette una valutazione ottimale della distruzione ossea . nellipotesi di compressione midollare acuta la rm il primo , e spesso lunico , esame da eseguire [ 3 ]  . il sistema di stadiazione di durie e salmon [ 33 ] , sviluppato nel 1975 , ancora largamente in uso . 
dal momento che la colonna vertebrale rappresenta unampia porzione del midollo rosso e che uno dei principali siti di coinvolgimento nei pazienti con mieloma multiplo , il rachide il sito ideale per la stadiazione dellestensione del coinvolgimento midollare [ 35 ]  . la rm whole body permette la visualizzazione diretta del reale coinvolgimento tumorale allinterno del midollo osseo [ 9 ] : nello stadio di infiltrazione plasmacellulare interstiziale lieve ( < 20% alla biopsia del midollo osseo ) , in tutte le sequenze il midollo osseo presenta segnale normale . 
coronal whole - body magnetic resonance imaging ( a ) and sagittal t1 - weighted ( b ) and short t1 inversion recovery ( c ) images show normal bone marrow signals . 
istologicamente questo corrisponde ad uninfiltrazione moderata di plasmacellule ( < 20% vol alla biopsia del midollo osseo )  . lymphoma although secondary osseous involvement is relatively common in both hodgkins disease and nhl and occurs in up to 16% of cases , primary bone lymphoma is uncommon . 
lymphomatous involvement of bone marrow is seen as diffuse , primarily heterogeneous , replacement of collaboratori hanno sviluppato il sistema di stadiazione durie e salmon plus [ 39 ]  . 
per quanto riguarda limaging diagnostico , sono state incluse nella stadiazione dei pazienti con mieloma multiplo la rm e la fdg - pet : una scala a tre gradi per la rm del rachide stata aggiunta nel sistema di stadiazione clinico di salmon e durie . 
la scelta della terapia si basa su questa classificazione [ 39 ]  . tuttavia , i tradizionali protocolli di rm spesso non includono il cranio , lo sterno e le coste , che sono aree ad elevato contenuto di midollo rosso e spesso rappresentano sede di infiltrazione . 
coronal t1 - weighted ( a , b ) and short t1 inversion recovery ( stir ) ( c , d ) wholebody magnetic resonance imaging show a homogeneous decrease of signal in t1 - weighted spin - echo images and increased signal intensity on fat - suppressed images . 
la rm whole body coronale t1 - pesata ( a , b ) e stir ( c , d ) mostrano unomogenea diminuzione di segnale nelle t1 - se e un aumento di intensit nelle immagini a soppressione del grasso . 
patients with lymphoma and femoral marrow involvement seen on mri appear to have an overall lower survival rate than patients with normal femoral marrow on mri , whatever the results of blind biopsy . recently some authors have emphasised the role of wbmri as a noninvasive and nonradiation imaging method , which is used to assess stage and prognosis , select biopsy sites and monitor treatment response in patients who cannot undergo pretreatment ct - pet [ 46 , 47 ]  . leukaemias are a group of different neoplasms derived from arrested , or aberrant , development of a clone of normal haematopoietic cells . 
these immature cells proliferate progressively within bone marrow , replacing normal hematopoietic tissue and circulating within the peripheral blood being leukaemia no dimostrato che un sistema di staging esteso , che includa la rm , ha una significativa influenza sulla prognosi del paziente e sul tasso di sopravvivenza : usando il sistema di stadiazione classico di durie e salmon senza la rm , 25 di 77 pazienti sarebbero stati sottostadiati . 
sarebbe necessario valutare , in futuri studi , un grande numero di pazienti e diversi sistemi di staging che comprendano la rm e , quindi , compararli con le stadiazioni che non includono la rm . unanalisi con rm del midollo osseo nei pazienti con mieloma multiplo dimostra lampio spettro di coinvolgimento , i risultati del trattamento , le aree di potenziali complicanze ed i siti di malattia focale per una biopsia ossea sicura . 
nel iii stadio di mieloma multiplo , il coinvolgimento del midollo osseo vertebrale in rm si correla con la prognosi [ 40 , 41 ]  . vi sono prove crescenti che langiogenesi incrementa nelle neoplasie ematologiche . 
focal bone lesions are more common in acute lymphoblastic leukaemia than in acute myelogenous leukaemia [ 14 ]  . there are no definite findings to suggest that mri has a clinical role to play in patients with acute leukaemia . 
however , it is useful in patients suspected of relapse , for example , in patients believed to be in remission who re - present with bone pain or in patients at high risk of relapse in whom serial bone marrow biopsies are negative [ 1 , 2 , 5 ]  . 
accurate assessment of residti con malattia linfoproliferativa ed infiltrazione midollare diffusa ed anche per la valutazione della risposta al trattamento [ 42 , 43 ]  . linfoma sebbene il coinvolgimento osseo secondario sia relativamente comune sia nella malattia di hodgkin sia nel linfoma non hodgkin ( nhl ) , ed avvenga fino al 16% dei casi , il linfoma osseo primario non comune . 
the d - 6 lesion is slightly hyperintense on turbo short t1 inversion recovery ( t - stir ) image ( c ) , whereas the haemangioma shows low signal intensity . 
nellimmagine tse - t2 pesata gli emangiomi sono iperintensi , mentre la lesione linfomatosa appare lievemente ipointensa ( b )  . la lesione di d6 appare lievemente iperintensa nellimmagine t - stir ( c ) , mentre lemangioma ha bassa intensit di segnale . 
il tessuto solido mostra omogeneo enhancement nellimmagine spir t1 - pesata dopo iniezione intravenosa di mezzo di contrasto ( d )  . ual disease may be important for predicting outcome in patients with acute leukaemia in complete remission . 
some authors have emphasised the role of mri of femoral marrow in predicting outcome in adult patients with aml in complete remission [ 48 ]  . post - therapy changes special diagnostic problems occur in patients with cancer of the haematopoietic system during therapy . 
before evaluating posttherapy changes seen on mri of bone marrow , it is necessary to be familiar with changes that occur in each mr pattern of abnormal marrow after treatment . 
i pazienti con linfoma e coinvolgimento del midollo femorale diagnosticato in rm sembrano avere un tasso di sopravvivenza generale inferiore rispetto ai pazienti con midollo femorale normale alla rm , qualunque sia il risultato della biopsia eseguita alla cieca . recentemente alcuni autori hanno sottolineato il ruolo della rm whole body come tecnica di imaging non invasiva e priva di radiazioni per la formulazione dello stadio e della prognosi , per selezionare i siti da bioptizzare e per monitorare la risposta terapeutica nei pazienti che non possono sottoporsi ad una tc - pet prima del trattamento [ 46 , 47 ]  . leucemia le leucemie sono un gruppo di differenti neoplasie che derivano dallarresto o da un aberrante sviluppo di un clone di cellule ematopoietiche normali . 
le lesioni ossee focali sono pi comuni nella leucemia linfoblastica acuta piuttosto che nella leucemia mieloide acuta [ 14 ]  . non vi sono risultati definitivi che dimostrino che la rm abbia un ruolo nei pazienti con leucemia acuta . 
donna di 36 anni con pancitopenia ( gr 1 , 2 ; emoglobina 6 , 6 , piastrine 67000 ) da chemioterapia con temozolomide usato per trattare una neoplasia cerebrale ( oligoastrocitoma anaplastico )  . 
dopo il trattamento con g - csf ( gb 8 , 6 , emoglobina 9 , 6 g / dl , piastrine 409000 ) le immagini pesate in t1 ( b ) e stir ( c ) dimostrano una diffusa basa intensit di segnale nelle t1 e lieve aumento omogeneo dellintensit di segnale nella stir dovuto alla riconversione midollare . images predominantly inside the rt field . 
the characteristic fatty marrow appearance is not reversible for doses equal to or higher than 30 to 40 gy , because destruction of vascular sinusoids is nonreversible . changes that occur in bone marrow after chemotherapy are known from histological studies [ 4951 ]  . administration of haematopoietic growth factors may delay the fatty transformation of bone marrow or may cause reconversion of fatty to haematopoietic marrow and simulate persistent or relapsing disease [ 5254 ]  . 
colony - stimulating factor ( csf ) , in the form of granulocyte macrophage csf ( gmcsf ) and g - csf is becoming a widely used adjuvant to chemotherapy for treating many malignancies , because it dealterazioni post - terapia particolari problemi diagnostici si presentano nei pazienti con neoplasie del sistema ematopoietico durante la terapia . prima di valutare le alterazioni post - terapia che si verificano nelle immagini rm del midollo osseo , necessario avere dimestichezza con le alterazioni che avvengono nel midollo patologico dopo terapia . 
dopo uniniziale diminuzione dellintensit di segnale nelle immagini t1 - pesate ed un aumento in quelle stir , dovuto alledema ed alla necrosi midollare , si verifica la deplezione midollare . 
tuttavia , una diminuzione di enhancement dopo contrasto si osservata nel midollo osseo , non solo allinterno , ma anche fuori dal campo di radioterapia nel primo mese dopo la terapia . 
 i cambiamenti che avvengono nel midollo osseo dopo chemioterapia sono noti dagli studi isologici [ 4951 ]  . la somministrazione di fattori di crescita ematopoietici ritarda la trasformazione adiposa del midollo ematopoietico e simula una malattia persistente o recidiva [ 5254 ]  . 
i fattori di crescita , nella forma di gmcsf e di gcsf , stanno divenendo un adiuvante alla chemioterapia largamente utilizzato nel trattamento di diverse neoplasie , perch provocano una diminuzione dellincidenza di eventi neutropenici e di infezioni e riducono il numero e la durata delle ospedalizzazioni e delle terapie antibiotiche . 
si ritiene che tutti i radiologi che interpretino uno studio di rm di un paziente con neoplasia maligna debbano avere familiarit con questi aspetti del midollo osseo . nel 2002 , dalrup - link et al . 
proposero luso degli ossidi di ferro superparamagnetici per differenziare linfiltrazione tumorale dal midollo osseo ipercellulare nei pazienti con linfoma non hodgkdopo la somministrazione di particelle di ossido di ferro superparamagnetico ( spio ) si osserva unalterazione del segnale del midollo osseo vertebrale simile a quella che si verifica nel fegato e nella milza . 
immagini t1 - pesate ( a ) e stir ( b ) dopo trattamento con gsf : nel midollo osseo vi sono un basso segnale nellimmagine t1 e un incremento disomogeneo nellimmagine stir , dovuti allaumento di midollo ematopoietico . crease the incidence of neutropenic events and infections and reduces the number and length of hospitalisations and duration of antibiotic therapy . 
we believe that all radiologists interpreting mri studies of patients with primary malignant tumours should be familiar with these aspects of bone marrow . recurrent in 2002 , daldrup - link et al . 
after administration of superparamagnetic iron oxide particles ( spio ) , a signal intensity change similar to that seen in the liver and spleen is observed in vertebral bone marrow . 
it is important to note that in patients with a minor amount of diffuse tumour cell infiltration , iron oxide uptake approximated that of normal haematopoietic bone marrow [ 28 ]  . some authors recently proposed dynamic gadoterate meglumine - enhanced turbo fast low - angle shot ( flash ) mr images to evaluate the increased spinal bone marrow enhancement in patients with lymphoproliferative diseases and diffuse bone marrow infiltration and to monitor bone perfusion in the follow - up of patients receiving antiangiogenesis therapy . 
thus , dynamic contrast - enhanced mri may be helpful in diagnosing and grading bone marrow involvement in such patients and for evaluating treatment response to angiogenesis - inhibiting drugs such as thalidomide . 
initial results of a clinical histological study involving patients with mm revealed that after chemotherapy , mean microvessel density was significantly lower in responders compared with nonresponders [ 26 ]  . it is important to point out that wbmri of therapeutic response in human bone marrow was achieved without the use of contrast agents by using diffusion - weighted echo - planar mri of physiological water . 
the results encourage further investigation . conclusions although it is unlikely that mri will actually replace bone marrow biopsy for detecting bone marrow disease , mri and particularly wbmri is useful in evaluating the entire bone marrow and the number , type and location of bone marrow lesions [ 9 , 10 ]  . 
iliac crest biopsy may be negative when bone marrow infiltration is focal rather than diffuse . understanding the normal age - related changes in bone marrow signal is required for interpretation . 
although the morphological aspects are useful , pathological changes can be nonspecific , and correlation should always be made with clinical , laboratory and radiological findings . what is todays clinical role of bone marrow mri in oncohaematological disease ? infiltrazione tumorale di tipo diffuso , luptake di ossidi di ferro simile a quello del midollo osseo ematopoietico normale [ 28 ]  . alcuni autori hanno recentemente proposto le immagini dinamiche di tipo turbo flash con gadoterato meglumina come mezzo di contrasto per valutare laumentato enhancement del midollo osseo del rachide nei pazienti con malattie linfoproliferative ed infiltrazione midollare diffusa e per monitorare il follow - up dei pazienti che ricevono una terapia angiogenetica . 
perci le sequenze dinamiche dopo contrasto potrebbero essere utili nella diagnosi e nel grading del coinvolgimento midollare in questi pazienti e per valutare la risposta al trattamento con farmaci che inibiscono langiogenesi , come la talidomide . 
i risultati iniziali di uno studio clinico istologico che coinvolge i pazienti con mieloma multiplo rivelano che dopo la chemioterapia la densit media di vasi di piccolo calibro significativamente inferiore nei pazienti che rispondono alla terapia rispetto ai non responders [ 26 ]  . importante sottolineare che limaging whole body per valutare la risposta terapeutica nel midollo osseo umano era stato ottenuto senza utilizzare mezzo di contrasto , ma servendosi di imaging echo - planare di diffusione del liquido fisiologico . 
i risultati incoraggiano a continuare le ricerche . conclusioni sebbene non sia probabile che la rm possa rimpiazzare la biopsia del midollo osseo per lindividuazione della patologia midollare , la rm , e particolarmente la rm whole body , utile per valutare il midollo osseo nella sua interezza ed il numero , il tipo e la sede delle lesioni midollari [ 9 , 10 ]  . 
la biopsia della cresta iliaca pu essere negativa , quando linfiltrazione midollare non diffusa ma focale . la comprensione dei normali cambiamenti che avvengono nel segnale del midollo osseo con let necessaria per linterpretazione . 
sebbene alcuni aspetti morfologici possano essere utili , le variazioni patologiche non sono specifiche , perci sempre necessaria la correlazione fra la clinica ed i reperti radiologici e laboratoristici . quale ruolo clinico riveste oggi la rm del midollo osseo nelle malattie onco - ematlogiche ? 1 . 
la rm pu essere utilizzata per selezionare i siti di biopsia , dato che la biopsia della cresta iliaca pu risultare negativa in presenza di uninfiltrazione midollare focale e non diffusa . 
optimal marrow evaluation should include both biopsy and mri , and it is important to note that biopsy induces important changes in the mri signal and creates hot spots on bone scintigraphy . 
mri is a useful adjunct to bone marrow biopsy for patients who are candidates for bone marrow transplant and in particular for patients with lymphoma , a disease with a well - known patchy mode of infiltration of the bone marrow [ 5 ]  . mri requires someone with a great deal of experience in making choices regarding imaging conditions and evaluating findings . 
technical - methodological guidelines need to be devised , and research is under way and not only for sequences but also for a contrast medium [ 6063 ]  . wbmri has oncological applications in evaluation of skeletal metastases , myeloma and lymphoma . 
nevertheless , it is reasonable to propose that wbmri should be used as a single modality as a first step in bone marrow imaging in oncohaematological diseases [ 9 , 10 ]  . a balanced and positive relationship within the team composed of different specialists is necessary , because today in medicine , multidisciplinary patient management is mandatory . 
as in other malignancies , close liaison between clinician and radiologist is essential to determine the most appropriate use of imaging for individual patient care . te notare che la biopsia induce importanti cambiamenti del segnale di rm del midollo osseo e crea degli spot ipercaptanti alla scintigrafia ossea . 
la rm un utile complemento alla biopsia midollare per i pazienti candidati a trapianto del midollo osseo e , in particolare , per i pazienti con linfoma , una malattia di cui nota linfiltrazione midollare a chiazze [ 5 ]  . la rm richiede un operatore con molta esperienza per la scelta dei piani di studio e delle sequenze da utilizzare e per linterpretazione dei reperti . 
necessario formulare delle linee guida tecnico - metodologiche , e la ricerca ancora in corso , non solo sulle sequenze , ma anche sui mezzi di contrasto [ 6063 ]  . in ambito onco - ematologico la rm whole body trova oggi applicazione nella valutazione delle metastasi scheletriche , del mieloma , del linfoma . 
tuttavia ipotizzabile che la rm whole body debba essere usata come unica modalit di imaging di primo livello del midollo osseo nelle patologie onco - ematologiche [ 9 , 10 ]  . necessario istaurare un rapporto valido e bilanciato allinterno di un team composto da differenti specialisti , perch nella medicina odierna necessaria una gestione multidisciplinare del paziente . 
isbn 978 - 88 - 470 - 0666 - 9 . published online : 23 july 2007 this book has come a long way from the in - depth knowledge and experience acquired daily on the field by a group of radiologists who have always had a keen interest in the pathophysiology and morphodynamism of the small bowel in acute abdominal disease . through the correct interpretation of these findings , radiologists enable clinicians both to establish a diagnosis and to evaluate the time course of the event , thereby guiding them towards the most appropriate treatment strategy . the decision to use an atlas - textbook to illustrate one of the most common causes of acute abdomen , namely , small - bowel obstruction and its natural course , emerged during the itinerant courses of the urgency and emergency section of the societ italiana di radiologia medical , as this topic invariably met with great interest among course participants , who repeatedly asked for an easy and straightforward text that could serve as a quick reference . the topic lends itself particularly well to this purpose , as it presents the entire spectrum of findings that a young radiologist should be familiar with . 
a large part of the text focuses on computed tomography ( ct ) imaging , the main tool for understanding the ileum - mesentery complex . the authors fill a gap in the scientific literature on this difficult topic , which , for a correct approach to imaging , requires in - depth knowledge of the clinical pathophysiology of the disease . questo libro nasce da una profonda conoscenza ed esperienza acquisite quotidianamente sul campo da un gruppo di radiologi attenti , da sempre , agli aspetti fisiopatologici e al morfodinamismo del tenue nella patologia addominale acuta . grazie alla corretta interpretazione di questi rilievi , il radiologo offre al clinico la possibilit sia di fare diagnosi , sia di valutare la cronologia dellevento , indirizzandolo verso la decisione terapeutica idonea . la scelta di illustrare con un testo - atlante una delle cause pi frequenti di addome acuto locclusione del piccolo intestino e il suo evolversi maturata nei corsi itineranti della sezione di urgenza ed emergenza della societ italiana di radiologia medica . 
tale argomento , infatti , ha sempre suscitato interesse nei discenti , i quali hanno ripetutamente chiesto un testo facile , comprensibile e di rapida consultazione . largomento ben si presta a questo scopo , poich mostra lintero paradigma dei reperti che un giovane radiologo deve conoscere . 
in the past , when patients required a contrast - enhanced imaging study , the tendency was to select magnetic resonance ( mr ) imaging with a gadolinium ( gd ) - based contrast agent over computed tomography ( ct ) with iodinated contrast media ( cm ) due to the known nephrotoxic nature of iodinated cm , which is associated in some patients with the development of contrast - induced nephropathy ( cin )  . 
however , recently , the administration of gd - based contrast agents has been associated with a severe , potentially fatal , adverse reaction , termed nephrogenic systemic fibrosis ( nsf ) , in patients with moderate - tosevere renal insufficiency [ 1 ]  . 
in order to optimise patient outcomes , imaging of patients with ckd requires an understanding of the risk factors for both cin and nsf . key words contrast media nephrogenic systemic fibrosis renal disease contrast - induced nephropathy gadolinium riassunto sovente nei pazienti con insufficienza renale cronica si presenta la necessit di effettuare una procedura di imaging diagnostico con mezzo di contrasto ( mdc ) e il radiologo si trova a dover decidere qual la modalit di imaging pi idonea per ciascun paziente in base al grado di compromissione della funzionalit renale . 
in passato la tendenza era quella di indirizzare il paziente alla risonanza magnetica ( rm ) con chelati del gadolinio ( gd ) piuttosto che sottoporlo alla tomografia computerizzata ( tc ) con mdc iodato , data la potenziale nefrotossicit di questi agenti che in alcuni pazienti pu dar luogo a nefropatia da contrasto ( cin )  . recentemente tuttavia , la somministrazione di mezzi di contrasto per rm a base di gd in pazienti con insufficienza renale da moderata a grave stata associata alla comparsa di una malattia grave e con esito potenzialmente fatale conosciuta come fibrosi sistemica nefrogenica ( nsf ) [ 1 ]  . 
per ottimizzare la gestione del paziente con funzionalit renale compromessa da sottoporre a procedure di imaging necessaria pertanto la comprensione dei fattori di rischio per entrambe queste patologie . parole chiave mezzi di contrasto fibrosi sistemica nefrogenica insufficienza renale nefropatia da contrasto gadolinio introduction introduzione for over 10 years , when patients with renal impairment required a contrast - enhanced imaging procedure , radiologists were inclined to select magnetic resonance ( mr ) over computed tomography ( ct ) in order to preserve kidney function , as iodinated contrast media ( cm ) used in ct have been shown to increase the risk of contrast - induced nephropathy ( cin ) in that group of patients . 
cin is defined as an acute decline in renal function following administration of iodinated cm with no other known cause , is responsible for over 10% of cases of hospital - acquired renal insufficiency and is associated with significant morbidity and mortality . 
 da oltre 10 anni , quando un paziente con ridotta funzionalit renale doveva essere sottoposto ad una procedura di imaging con mezzo di contrasto ( mdc ) , il radiologo era incline a selezionare la risonanza magnetica ( rm ) invece della tomografia computerizzata ( tc ) per preservare la funzionalit renale , dal momento che noto che in quel gruppo di pazienti i mezzi di contrasto iodati usati nella tc possono aumentare il rischio di insorgenza di nefropatia da contrasto ( cin )  . 
1 a 49 - year - old man with terminal renal failure [ glomerular filtration rate ( gfr ) 10 ml / min / 1.73 m2 ] was first exposed to gadodiamide ( 0.3 mmol / kg ) during a magnetic resonance angiography study in april 2003 . 
1 paziente di sesso maschile di 49 anni con insufficienza renale terminale ( gfr 10 ml / min / 1 , 73 m2 ) stato dapprima esposto a somministrazione di gadodiamide ( 0 , 3 mmol / kg ) durante unindagine in mra nellaprile 2003 in seguito alla quale ha sviluppato unnsf progressiva con gravi variazioni cutanee e cachessia . 
il paziente deceduto 30 mesi dopo la prima somministrazione ( per gentile concessione del peter marckmann , dipartimento di of nefrologia dellospedale universitario di copenhagen , herlev , danimarca )  . recently , a severe , systemic adverse reaction nephrogenic systemic fibrosis ( nsf ) has been observed days to months following administration of some of the extracellular gadolinium ( gd ) - based mr contrast agents in patients with baseline renal insufficiency [ 1 , 2 ]  . 
thus , selection of an imaging modality in the patient with reduced renal function [ chronic kidney disease ( ckd ) stage 45 : glomerular filtration rate ( gfr ) < 30 ml / min / 1.73 m2 ] is no longer a simple decision : this same patient group has an increased risk for both cin after administration of iodinated cm and nsf after administration of gd - based mr contrast agents . 
 determination of patients at risk for cin and nsf baseline renal insufficiency is the greatest risk factor for both cin and nsf : the poorer the kidney function ( based on gfr ) , the higher the risk . 
pertanto la scelta della modalit di imaging nel paziente con funzionalit renale ridotta ( insufficienza di stadio 4 - 5 : gfr < 30 ml / min / 1 , 73 m2 ) pi complessa di un tempo , in quanto questo stesso gruppo di pazienti presenta un aumentato rischio sia per la cin dopo somministrazione di mdc iodato che per lnsf dopo somministrazione di mdc a base di gd . in questo articolo passer in rassegna le attuali conoscenze riguardo ai fattori di rischio per cin e nsf e alla loro prevenzione . individuazione dei pazienti a rischio di cin e nsf il principale fattore di rischio sia per la cin che per lnsf la presenza di insufficienza renale : maggiore il grado di compromissione della funzionalit ( in base al gfr ) e maggiore il rischio . 
tuttavia , lidentificazione e la stratificazione dei pazienti con insufficienza renale non semplice e diversi studi hanno dimostrato che lestendere a tutti i pazienti la misurazione della creatinina serica e del gfr non conveniente dal punto di vista del costo - beneficio [ 3 ]  . 
inoltre le formule usate per calcolare la funzionalit renale ( quella di cockroft - gault e quella nota come modification of diet in renal disease [ mdrd ] ) si dimostrano utili solo in pazienti con un gfr < 60 ml / min / 1 , 73 m2 e i risultati ottenuti con lapplicazione di queste due formule possono differire tra loro . il comitato per la sicurezza dimpiego dei mezzi di contrasto della societ europea di radiologia urogenitale ( esur ) raccomanda che venga effettuatata di routine la determinazione dei livelli di creatinina serica e la stima del grf in determinati gruppi di pazienti : quelli con pregressa creatininemia elevata , i diabetici trattati con metformina , i pazienti da sottoporre a somministrazione endoarteriosa del mdc e quelli con unanamnesi compatibile con livelli elevati di creatinina ( per esempio , nefropatia , storia di chirurgia renale , proteinuria , diabete mellito , ipertensione , gotta o recente assunzione di farmaci nefrotossici ) [ 4 ]  . 
una volta confermata la presenza e lentit della insufficienza renale , allora il radiologo pu essere in grado di raccomandare la modalit di imaging pi opportuna per il paziente . not cost effective [ 3 ]  . 
cockcroft - gault and modification of diet in renal disease ( mdrd ) ] are useful only in patients with a gfr < 60 ml / min / 1.73 m2 , and the results obtained with these two formulae may differ . 
once the existence and level of renal dysfunction are confirmed , radiologists can then recommend the best imaging modality for each patient . prevention of cin for many years , it has been recognised that cin develops in significantly more patients after administration of high - osmolar cm ( osmolality > 1 , 500 mosm / kg ) compared with low - osmolar cm ( osmolality < 915 mosm / kg ) [ 5 ]  . 
however , it remains controversial whether differences in the incidence of cin exist between available cm , either low - osmolar cm or isoosmolar cm ( iocm , osmolality 290 mosm / kg ) [ 6 ]  . 
a total of eight nonionic monomers ( iohexol , iomeprol , iopamidol , iopentol , ioxilan , iopromide , ioversol and iobitridol ) , one ionic dimer ( ioxaglate ) and one nonionic dimer ( iodixanol ) are currently approved for intravascular use in europe , with their level of use varying from country to country . eleven studies have compared a low - osmolar cm with an iocm . 
in seven of these head - to - head comparisons , the cm was given intra - arterially : two were favourable for the nonionic dimer , whereas the remaining five showed no statistically significant difference between the two ca systematic analysis of published papers and us food and drug administration ( fda ) reports of adverse events demonstrated that the risk of cin after intra - arterial injection was higher in patients following the nonionic monomer iohexol than following another nonionic monomer iopamidol [ 7 ]  . 
one study demonstrated a significantly lower rate of cin after administration of the nonionic monomer than the dimer , and when one pools the two almost identical studies active and impact , and looks at the patients with reduced renal function ( < 40 ml / min / 1.73 m2 ) , no patient in the monomer group developed cin ( serum creatinine increase > 44 mol / l , 4872 h ) , whereas six did so in the group who received the dimer ( p < 0.0059 ) ( [ 10 ] ; hst personal communication )  . 
thomsen : imaging patients with chronic kidney disease : cin or nsf ? prevenzione della cin per molti anni stato riconosciuto che la cin si verifica con maggiore frequenza in pazienti a cui veniva somministrato un mdc ad alta osmolarit ( osmolalit > 1 , 500 mosm / kg ) che non dopo somministrazione di un mdc a bassa osmolarit ( osmolalit < 915 mosm / kg ) [ 5 ]  . 
rimane invece controverso se esista una differenza nellincidenza di cin tra i mezzi di contrasto a bassa osmolarit e iso - osmolari ( osmolalit 290 mosm / kg ) [ 6 ]  . 
attualmente in europa sono approvati per luso intravascolare otto mezzi di contrasto monomerici nonionici ( iohexolo , iomeprolo , iopamidolo , iopentolo , ioxilan , iopromide , ioversolo , e iobitridolo ) , un dimero ionico ( ioxaglato ) , and e un dimero nonionico ( iodixanolo ) con livelli di utilizzo variabili da paese a paese . sono stati riportati 11 studi di confronto diretto tra un mdc a bassa osmolarit e uno iso - osmolare . 
in 7 di questi il mdc stato somministrato per via intrarteriosa : 2 erano favorevoli al dimero non ionico mentre i rimanenti 5 non dimostravano una differenza significativa tra i due prodotti . unanalisi sistematica della letteratura e delle segnalazioni di reazioni avverse alla food and drug administration ( fda ) ha dimostrato che il rischio di cin dopo somministrazione intrarteriosa era pi alto nei pazienti che avevano ricevuto il monomero nonionico iohexolo rispetto a un altro monomero nonionico , lo iopamidolo [ 7 ]  . per quanto riguarda la via endovenosa , nessuno studio ha riportato dei dati a favore del dimero nonionico [ 8 , 9 ] ( tabella 1 )  . 
vi invece uno studio che ha dimostrato unincidenza significativamente pi bassa di cin dopo la somministrazione del monomero nonionico rispetto al dimero , e quando si combinano i dati di due studi quasi identici , lactive e limpact , e si considerano i pazienti con funzionalit renale ridotta ( < 40 ml / min / 1 , 73 m2 ) , si riscontra che nessun paziente nel gruppo a cui era stato somministrato il monomero ha sviluppato la cin ( aumento della creatinina > 44 mol / l , dopo 4872 ore ) mentre nel gruppo che aveva ricevuto il dimero 6 pazienti la avevano sviluppata ( p < 0 , 0059 ) ( [ 10 ] , hst , comunicazione personale )  . in conclusione , controverso se esistano delle differenze di nefrotossicit tra i mezzi di contrasto a bassa osmolarit dopo somministrazione intrarteriosa , mentre sta diventando chiaro che non vi alcun vantaggio associato alluso del dimero nonionico per procedure endovenose . prevenzione dellnsf diverse osservazioni recenti suggeriscono che la somministrazione di alcuni , ma non di tutti , i mezzi di contrasto a distribuzione extracellulare a base di gd possa essere causa dello sviluppo di nsf in pazienti con insufficienza renale grave ( < 30 ml / min / 1 , 73 m2 ) o in dialisi . 
thomsen : imaging patients with chronic kidney disease : cin or nsf ? table 1 prospective , randomised trials of various low - osmolar nonionic monomeric contrast media and the isoosmolar nonionic dimer with regard to contrastinduced nephropathy in relation to intravenous injection for computed tomography . 
no other randomised , prospective trials where the contrast medium is given intravenously have been published study locm ( monomers ) iodixanol ( dimer ) definition of cin carraro et al . 
 [ 10 ] total 0 / 32 ( iopromide ) 4 / 25 ( iobiditrol ) 0 / 76 ( iomeprol ) 0 / 77 ( iopamidol ) 4 / 210 ( 2% ) 1 / 32 4 / 25 5 / 72 2 / 76 12 / 209 ( 6% ) locm , low - osmolar contrast media ; cin , contrast - induced nephropathy ; scr , serum creatinine tabella 1 studi prospettici , randomizzati , di confronto tra diversi mezzi di contrasto monomerici nonionici a bassa osmolarit e il dimero nonionico iso - osmolare in termini di incidenza di cin dopo somministrazione per procedura di tc . 
 [ 10 ] totale 0 / 32 ( iopromide ) 4 / 25 ( iobiditrol ) 0 / 76 ( iomeprol ) 0 / 77 ( iopamidol ) 4 / 210 ( 2% ) 1 / 32 4 / 25 5 / 72 2 / 76 12 / 209 ( 6% ) locm , mezzi di contrasto a bassa osmolarit ; cin , nefropatia da contrasto ; scr , creatinina sierica prevention of nsf several recent reports suggest that administration of some , but not all , of the extracellular gd - based contrast agents may be causative for development of nsf in patients with severely reduced renal function ( < 30 ml / min per 1.73 m2 ) or on dialysis . 
the onset varies in general from a few days to 3 months after exposure . the disease is characterised by scleroderma - like skin changes that mainly affect the limbs and trunk . 
strikingly , the overwhelming majority of reported cases ( ~90% ) were observed following administration of the nonionic , linear contrast agent , gadodiamide . the mechanism by which gd - based contrast agents cause nsf is not completely understood . 
these differences in stability become clinically important in patients with reduced renal function , as in va da alcuni giorni ai tre mesi dopo lesposizione al mdc . la nsf caratterizzata da cambiamenti cutanei simili alla sclerodermia che possono interessare gli arti e il tronco . 
lispessimento cutaneo pu anche progredire fino a causare la contrattura con incapacit di estensione delle articolazioni e la fibrosi pu interessare anche altri organi quali muscoli , cuore , fegato e polmoni . 
sorprendentemente , la grande maggioranza dei casi di nsf riportati ( circa il 90% ) sono stati osservati dopo la somministrazione del mdc lineare nonionico gadodiamide . il meccanismo tramite il quale i mezzi di contrasto a base di gd causano lnsf non pienamente chiarito . 
in teoria , durante questa prolungata biodisponibilit , vi una probabilit maggiore che avvenga una transmetallazione con metalli endogeni il che darebbe luogo a un deposito di gd libero a livello cutaneo , cosa che in effetti stata riscontrata nei pazienti affetti da nsf . 
theoretically , during this extended period of bioavailability , transmetallation with endogenous ions has a greater opportunity to occur , resulting in free gd deposition in the skin , which has in fact been observed to occur in nsf patients . 
furthermore , this might explain the overwhelming majority of cases with gadodiamide , as several lines of evidence suggest that gadodiamide , which utilises a linear chelate , is a relatively unstable contrast agent . gadodiamide is now contraindicated in europe for use in patients with a gfr < 30 ml / min / 1.73 m2 , those on dialysis , or those who have had or are awaiting liver transplantation [ 12 ]  . 
thomsen : imaging patients with chronic kidney disease : cin or nsf ? anche spiegare la grande preponderanza di casi osservati dopo la somministrazione di gadodiamide , che essendo costituito da un chelato lineare , un mdc relativamente instabile . attualmente in europa la gadodiamide ha la controindicazione alluso in pazienti con un gfr < 30 ml / min / 1 , 73 m2 , in quelli in dialisi e in quelli che hanno avuto o sono in attesa di trapianto di fegato [ 12 ]  . 
non sono stati riscontrati casi di nsf dopo la somministrazione esclusiva di vari mezzi di contrasto : il gadoterato di dimeglumina , il gadoteridolo , il gadobenato di dimeglumina e il gadobutrolo nonostante luso esteso di questi prodotti in centri di imaging a cui vengono inviati pazienti da dipartimenti di nefrologia . conclusions based on available evidence , baseline renal insufficiency is a significant risk factor for cin in patients undergoing contrast - enhanced ct and for nsf in patients administered a gd - based contrast agent prior to mr imaging . 
for cin , although there have been many studies performed , it is not entirely clear whether there are differences in the incidence of cin among the low - osmolar iodinated cm , whereas for nsf , contrast agent selection clearly impacts the likelihood for the development of this serious adverse event . conclusioni in base alle evidenze disponibili , la preesistenza di una insufficienza renale un fattore di rischio significativo sia per la cin in pazienti che vengono sottoposti a tc con contrasto che per lnsf in pazienti cui viene somministrato un mdc a base di gd per una procedura di rm . 
cova1 1unit clinico operativa di radiologia , 2unit clinico operativa di clinica generale e terapia chirurgica , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , i - 34149 trieste , italy 3unit clinico operativa di anatomia patologica istopatologia e citodiagnostica , universit degli studi di trieste , ospedale maggiore , via della piet 2 , i - 34100 trieste , italy correspondence to : a . 
we retrospectively reviewed the ct scans of 26 patients who underwent surgery for histologically confirmed gist of the stomach ( 20 cases ) , the duodenum ( 1 ) , the caecum ( 1 ) , the small bowel ( 2 ) , the descending colon ( 1 ) and the rectum ( 1 )  . 
sono stati valutati retrospettivamente gli esami tc di 26 pazienti sottoposti ad intervento chirurgico con diagnosi istologica di gist localizzato allo stomaco ( 20 casi ) , al duodeno ( 1 ) , al cieco ( 1 ) , allintestino tenue ( 2 ) , al colon discendente ( 1 ) ed al retto ( 1 )  . 
although they may affect any portion of the gastrointestinal tract , they are seen with different frequencies in the different portions : 60% of gists are located in the stomach and 30% in the small bowel [ 1 ]  . they rarely arise in other locations , such as the large bowel or duodenudiscovery of a gist at the oropharyngeal level is extremely rare [ 2 ]  . 
an uncommon association between crohns disease of the terminal ileum and a high risk of gist development in this anatomical district region has also been reported [ 5 ]  . immunohistochemically , gists are defined as tumours that express a particular cell - surface tyrosine kinase , the cd117 antigen , whose overexpression is directly related to tumour aggressiveness . 
symptoms are nonspecific and essentially depend on tumour size [ 7 ] : small gists are normally asymptomatic and discovered incidentally during diagnostic procedures or surgery performed for other purposes ; these amount to approximately one third of all gist diagnoses . 
the most common clinical presentation of gist is gastrointestinal bleeding related to mucosal ulceration [ 7 ] , which may be chronic with associated anaemia or acute requiring emergency treatment ( approximately 40% of cases of bleeding ) [ 8 ]  . 
occlusion is seen in small - bowel tumours only , and perforation is always rare . the diagnosis is often incidental and , to a small extent only , based on endoscopic procedures , given the predominantly extramucosal growth pattern of gists . 
the aim of this study was to identify the ct patterns of gist and assess the techniques efficacy in identifying those lesions at a higher risk for malignancy , with a view to highlighting those patterns that may prove useful in treatment planning . materials and methods we retrospectively reviewed the ct studies performed between the year 2000 and 2005 in 26 patients ( 12 men , 14 women , mean age 67.6 years ) who underwent surgery for histologically proven gist located in the stomach ( 20 cases ) , the duodenum ( 1 ) , the small bowel ( 2 ) , the caecum ( 1 ) , the descending colon ( 1 ) and the rectum ( 1 )  . 
la loro massima incidenza si osserva fra la quinta e la sesta decade ; pur interessando tutto il tratto gastrointestinale si presentano con differente frequenza nei diversi tratti : nel 60% dei casi sono localizzati a livello dello stomaco , nel 30% al piccolo intestino [ 1 ] , raramente in altri distretti quali colon o duodeno . 
 stata descritta una rara associazione fra il morbo di crohn a carico del tratto terminale dellileo ed un elevato rischio di insorgenza di gist in tale distretto anatomico [ 5 ]  . dal punto di vista immuno - istochimico vengono classificati come gist le forme che esprimono sulla superficie cellulare una particolare tirosin - chinasi : lantigene cd117 , la cui sovra - espressione direttamente correlabile con la malignit della patologia . 
lespressione di un altro marcatore immunologico , il cd34 [ 6 ] appare essere correlato con una maggior propensione della neoplasia alla diffusione secondaria , in quanto codificante per una particolare molecola di adesione . 
la sintomatologia aspecifica e dipende essenzialmente dalla dimensione della neoplasia [ 7 ] : i gist di piccole dimensioni sono solitamente asintomatici e sono diagnosticati generalmente in maniera occasionale durante indagini diagnostiche od interventi chirurgici non correlati con tale patologia ; tali reperti ammontano a circa un terzo del totale . 
la manifestazione clinica pi comune del gist il sanguinamento causato dallerosione della mucosa [ 7 ] , che pu essere cronico con associata anemia oppure acuto e richiedere un trattamento demergenza ( in circa il 40% dei casi di sanguinamento ) [ 8 ]  . 
solamente nel caso di lesioni localizzate al piccolo intestino locclusione frequente ; in tutti i casi rara la perforazione . la diagnosi , spesso occasionale , si basa solo limitatamente su procedure endoscopiche , dato lo sviluppo prevalentemente extramucoso dei gist ; a queste si aggiungono le indagini contrastografiche tradizionali , lecografia e la tomografia computerizzata ( tc ) [ 9 ]  . 
lo scopo di questo lavoro quello di riportare gli aspetti in tc dei gist e di valutare lefficacia dellindagine nellidentificazione delle lesioni a pi elevato rischio di malignit con lobiettivo di evidenziare alcuni aspetti che possano essere utili nella pianificazione della terapia . materiali e metodi sono stati valutati retrospettivamente gli esami tc eseguiti dal 2000 al 2005 in 26 pazienti ( 12 maschi , 14 femmine , et media 67 , 6 anni ) sottoposti ad intervento chirurgico con diaa . 
images were acquired with a 5 - mm slice thickness , 5 - mm reconstruction interval and 7 - mm table feed ( pitch 1.4 ) after oral administration of gastrografin ( nine patients ) or water ( 17 patients ) , in the case of suspected gastric location , with scans obtained at baseline and 70 s and 180 s ( portal and late phase ) after the intravenous injection of 120140 cc of iodinated contrast material ( iomeprolo 300 mgi / ml , iomeron 300 , bracco , milan , italy )  . 
ct images were processed on a dedicated workstation ( easyvision 4.3 , philips medical systems , the netherlands ) where multiplanar ( mpr ) and three - dimensional 3d reconstructions were generated by using the virtual colonoscopy software package . radiographic contrast studies were obtained by using a remote - controlled x - ray system ( omnidiagnost eleva di 1.0 , philips medical systems , the netherlands )  . 
endoscopic us was performed with a hitachi eub 525 fm scanner ( hitachi medica systems europe , wiesbaden , germany ) equipped with a 7.5 - mhz radial probe for endoscopic us . 
administration of contrast medium presence of calcification presence of ulcerations signs of invasion of neighbouring structures ( lack of clear cleavage plane between the mass and the surrounding structures ) distant metastasis lesions were classified in accordance with the literature as benign , borderline or malignant on the basis of their size and mitotic activity : lesions smaller than 5 cm with a mitotic index less than 5 / 50 high - power fields are considered benign . 
 pathological diagnosis of gist was obtained by means of immunohistological staining of tissue sections and detection of antibodies against the cd117 antigen . results ct characteristics of the lesions and their histological correlations are summarised in table 1 . 
overall , histological examination revealed ten benign lesions ( < 5 cm ) , six borderline lesions ( based on size > 5 cm ) and ten malignant lesions that were infiltrating and very large ( > 9 cm )  . 
only one case showed microcalcification gnosi istologica di gist localizzato allo stomaco ( 20 casi ) , al duodeno ( 1 ) , allintestino tenue ( 2 ) , al cieco ( 1 ) , al colon discendente ( 1 ) ed al retto ( 1 )  . 
gli esami tc sono stati eseguiti utilizzando unapparecchiatura tc spirale a singolo strato tomoscan ave 1 ( philips medical systems , olanda )  . le immagini , sono state acquisite con spessore di scansione di a 5 mm , intervallo di ricostruzione di 5 mm ed avanzamento del tavolo di 7 mm ( pitch 1 , 4 ) , dopo somministrazione di gastrografin ( 9 pazienti ) o acqua per os ( 17 pazienti ) , in caso di sospetto clinico di localizzazione gastrica del tumore , con scansioni dirette e durante liniezione endovena di 120140 cc di mdc organoiodato ( iomeprolo 300 mgi / ml , iomeron 300 , bracco , milano , italia ) a 70 s e 180 s ( fase portale e tardiva ) dallinizio della iniezione del mdc . 
le immagini tc sono state rielaborate mediante una workstation dedicata ( easyvision 4.3 , philips medical systems , olanda ) con la quale si sono effettuate ricostruzioni multiplanari ( mpr ) e ricostruzioni 3d mediante il pacchetto software di colonscopia virtuale . le indagini contrastografiche tradizionali sono state eseguite con un apparecchio telecomandato omnidiagnost eleva di 1.0 ( philips medical systems , olanda )  . 
le indagini ecoendoscopiche sono state effettuate mediante un unit ecografica hitachi eub 525 fm ( hitachi medica systems europe , wiesbaden , germania ) equipaggiata con sonda per ecoendoscopia radiale da 7 , 5 mhz . 
per evidenziare gli aspetti tc delle lesioni utili nella pianificazione terapeutica sono stati considerati i seguenti parametri : sede ; dimensioni ; caratteristiche densitometriche prima e dopo la somministrazione di mdc ev ; presenza di calcificazioni ; presenza di ulcerazioni ; segni di infiltrazione delle strutture anatomiche circostanti ( mancanza di un piano di clivaggio evidente in tc fra la massa e le strutture vicine ) ; metastasi a distanza . in accordo con la letteratura le lesioni sono state classificate come benigne , borderline o maligne sulla base delle loro dimensioni e dellindice mitotico : lesioni al di sotto dei 5 cm con un indice mitotico minore di 5 / 50 campi ad alto ingrandimento sono da considerarsi benigne , sono invece da ritenere borderline lesioni con lo stesso indice mitotico ma con dimensioni maggiori di 5 cm , le lesioni con indice mitotico maggiore di 5 / 50 campi ad alto ingrandimento sono da ritenersi maligne qualunque sia la loro dimensione [ 9 ]  . la diagnosi anatomopatologica di gist stata ottenuta mediante tipizzazione immunistologica di preparati della lesione con la dimostrazione di positivit per gli anticorpi rivolti contro lantigene cd117 . risultati le caratteristiche delle lesioni osservate in tc ed i loro correlati istologici sono state riassunte nella tabella 1 . 
4a - d scansioni tc assiali dirette ( a ) e durante iniezione di mdc , fase precoce ( b ) e tardiva ( c ) : processo espansivo solido omogeneo con scarso e tardivo enhancement ( frecce )  . 
d reperto istologico : cellule fusate stipate disposte in fasci variamente orientati . lesioni benigne ( < 5 cm ) , 6 borderline ( in relazione alle dimensioni > 5 cm ) e 10 maligne a carattere infiltrante e comunque , di notevoli dimensioni ( > 9 cm )  . 
laspetto tc pi frequente dei gist dato dalla presenza di una lesione esofitica , spesso di cospicue dimensioni ( oltre i 10 cm ) , a contorni lobulati [ 10 ]  . 
anche nella nostra esperienza ci siamo trovati di fronte a lesioni di dimensioni notevoli ( in 16 casi superiori a 5 cm ed in 10 di questi addirittura superiori ai 9 cm ) ; questo perch queste neoplasie raramente sono stenosanti e tendono ad avere una crescita eccentrica , senza quindi manifestare una sintomatologia di tipo ostruttivo se non tardivamente . per tale motivo a volte vengono diagnosticate in maniera occasionale [ 11 ]  . per quanto riguarda la densit , essa risulta essere spesso disomogenea in relazione alla presenza di aree emorragiche e / o necrotiche , specie nelle lesioni di maggiori dimensioni ( segno di torricelli - bernoulli ) , nonch di spazi cistici [ 12 ]  . nella nostra esperienza in 16 casi su 26 le lesioni presentavano densit disomogenea alle scansioni dirette ed in maniera pi evidente dopo mdc , in relazione alla presenza di componenti necrotiche lenhancement delle aree vascolarizzate risultava globalmente scarso , quantomeno in fase tardiva . 
si trattava peraltro prevalentemente di tumori di dimensioni medio - grandi , mentre nei pochi casi di lesioni piccole ed in una minima percentuale di quelle grandi si evidenziata in tc una struttura omogenea associata ad un enhancement pi intenso . 
in linea di massima si trattava di lesioni successivamente classificate come benigne o borderline allesame istologico , prive di significative aree necroticoemorragiche . la presenza di calcificazioni un reperto incostante ed aspecifico , apprezabile pi di frequente a livello delle metastasi epatiche [ 13 , 14 ]  . 
non sempre la tc in grado di evidenziarle , specie se si utilizza unapparecchiatura monostrato , come nel nostro caso , in cui alcune minute calcificazioni evidenziabili al tavolo operatorio non sono state evidenziate in tc . lulcerazione della lesione rappresenta un indice di malignit ; non sempre per possibile evidenziare tale reperto in tc , specie se molto superficiale , come nella nostra cafig . 
6a - c enhanced computed tomography ( ct ) : expansile mass originating from the right colon and infiltrating the kidney and fat tissue ( a , b )  . 
6a - c scansioni tc assiali dopo somministrazione di mdc : processo espansivo solido a partenza dal colon destro , infiltrazione del rene e del tessuto adiposo ( a , b )  . 
this is because these tumours rarely cause luminal narrowing and tend to have an eccentric growth pattern , so that symptoms secondary to occlusion only arise in the advanced stages of disease . 
 the ct density of gists is often inhomogeneous owing to the presence of haemorrhagic and / or necrotic areas , especially in larger lesions ( torricelli - bernoulli sign ) , and of cystic spaces [ 12 ]  . 
in our study , 16 out of 26 lesions exhibited inhomogeneous density on the unenhanced baseline scans and more marked inhomogeneity on the contrast - enhanced scans as a result of the presence of necrotic components that made enhancement of the vascular areas generally poor , at least in the late phase . 
these were predominantly medium to large size tumours , whereas the few cases of small lesions and a very small proportion of large lesions exhibited homogenous density associated with brighter enhancement . 
most of these lesions were histologically classified as benign or borderline and without significant areas of necrosis or haemorrhage . the presence of calcification is an inconstant and nonspesistica in cui tale reperto stato evidenziato in soli 2 casi su 6 [ 15 , 16 ]  . linfiltrazione della parete del viscere pu dar luogo raramente a focali dilatazioni del lume , causate dalla veloce crescita della neoplasia o anche dallinfiltrazione del plesso mesenterico con conseguente ectasia da atonia causata da denervazione [ 12 ]  . 
a volte per tali segni sono riconoscibili solamente allintervento chirurgico ( nella nostra casistica in 4 casi su 10 di forme infiltranti la tc non ha rilevato segni di infiltrazione locoregionale )  . 
 verosimile che limpiego di apparecchiature multistrato consenta di evidenziare con maggior frequenza e precisione questo segno , molto importante ai fini prognostici e terapeutici . in uno solo dei 26 casi valutati sono state riscontrate metastasi epatiche , ipodense alla scansione diretta e con discreto enhancement dopo liniezione di mdc . 
ct is not always able to demonstrate calcifications , above all if a single - slice scanner is used , as was the case in our study in which some tiny calcifications seen at surgery were missed by ct . 
however , not always is it possible to demonstrate this finding on ct , especially if the ulceration is very superficial , as occurred in our series where ct identified this finding in only two cases out of six [ 15 , 16 ]  . 
 invasion of the bowel wall may occasionally give rise to focal luminal dilatation related to rapid tumour growth or infiltration of the mesenteric plexus , with ectasia caused by loss of tone due to denervation [ 12 ]  . 
in some cases , however , these signs are only recognised at surgery ( in our series , ct failed to detect signs of locoregional invasion in four out of ten cases )  . 
it is likely that the use of multislice ct scanners will allow more frequent and better depiction of this sign , which is very important for prognostic and therapeutic purposes . in only one case out of 26 was liver metastases detected . these were hypodense on the baseline scan and showed moderate enhancement after the injection of contrast material . 
liver metastases are usually small and characterised by low density on baseline scans and intense vascularity and homogeneous enhancement in the portal phase showing complete washout in the late phase , with resultant hypodensity relative to the hepatic parenchyma . 
the presence of ascites is also quite rare and more often related to the outcome of chemotherapy , in particular to the liver failure caused by the treatment [ 17 , 18 ]  . the definition of benign or malignant gist is complex in that these tumours present a wide variability of malignant potential , which is established on the basis of the pathological and immunohistochemical findings . 
tumours larger than 5 cm are generally considered to have the highest malignant potential . other ct findings that point to a diagnosis of malignancy are inhomogeneous enhancement with central low density due to tissue necrosis ( in contrast to benign lesions that tend to enhance homogeneously ) , the presence of ulcerations or signs of locoregional infiltration and / or distant metastasis . 
it should , however , be noted that gists with a mitotic index greater than five mitoses per 50 high - power fields should be classified as malignant regardless of their size at imaging [ 19 ]  . surgery is the treatment of choice , and radical resection of the gist is considered to be the most important prognostic factor for cure in nonmetastatic disease . 
lymphadenectodentensit delle stesse alla scansione diretta , da intensa vascolarizzazione ed omogeneo enhancement in fase portale con completo wash - out in fase tardiva risultando cos nuovamente ipodense rispetto al parenchima . 
esse divengono invece ipovascolarizzate in tutte le fasi dopo trattamento chemioterapico . le metastasi a livello mesenterico sono comuni in corso di recidiva della patologia od in seguito a disseminazione della massa neoplastica escissa ; esse sono di difficile riconoscimento in quanto spesso di piccole dimensioni ed a volte si collocano a distanza dalla lesione primitiva . 
la presenza di metastasi linfonodali non caratteristica comune della lesione , pertanto la dimostrazione di linfoadenopatie satelliti deve far prendere in considerazione la presenza di una lesione di differente natura . 
la presenza di ascite anchessa piuttosto rara ed pi spesso riconducibile agli esiti dei trattamenti chemioterapici in relazione alla insufficienza epatica indotta dal trattamento [ 17 , 18 ]  . la definizione di benignit o malignit dei gist complessa in quanto questi tumori presentano una grande variabilit del grado di malignit , che viene stabilito sulla base dellaspetto anatomopatologico ed immunoistochimico . 
generalmente i tumori di dimensioni superiori ai 5 cm sono quelli a pi alto potenziale di malignit . le altre caratteristiche tc che orientano verso una diagnosi di malignit sono rappresentate dallenhancement disomogeneo con ipodensit centrale data dalla necrosi tissutale ove invece le forme benigne prediligono enhancement omogeneo e dalla presenza di ulcerazioni o di segni di infiltrazione locoregionale e\o metastasi a distanza . 
va in ogni caso osservato come i gist che presentino dal punto di vista istologico un indice mitotico maggiore di 5 mitosi su 50 campi ad alto ingrandimento ( hpf ) siano da classificare come maligni indipendentemente dalle dimensioni della neoplasia allimaging [ 19 ]  . la terapia chirurgica del gist rappresenta il trattamento elettivo e la resezione totale del tumore considerato il fattore prognostico maggiore nella guarigione dei casi non metastatici . 
lobiettivo della terapia chirurgica lasportazione della massa in toto compresa la sua capsula , e con margine di sezione istologicamente libero da neoplasia , mentre la linfoadenectomia non indicata cos come la peritonectomia , data la bassa metastatizzazione a questo livello ; tuttavia la resezione chirurgica viene spesso condizionata dalla localizzazione e dalla grandezza della massa stessa [ 20 , 21 ]  . la tecnica laparoscopica nel trattamento chirurgico dei gist gi stata utilizzata , tuttavia viene riportata in pochi studi , mentre si dimostrata vantaggiosa nel trattamento delle lesioni sanguinanti dello stomaco , consentendo , infatti , una minima manipolazione della massa . mentre per le lesioni di piccole dimensioni o con scarsa aggressivit locale il trattamento di elezione stato ed solo chirurgico , invece fino a poco tempo fa il trattamento adiuvante nel caso di tumori di maggiori dimensioni e di metastasi a distanza era effettuato mediante la chemioterapia e la radioterapia . 
 whereas for small lesions or lesions with limited local aggressiveness the treatment of choice has always been and still is surgery , until recently , patients with larger lesions and those with distant metastases received adjuvant chemotherapy or radiotherapy . 
nowadays , instead , the most innovative approach relies on the use of imatinib , a molecule that acts on a tyrosine - kinase transmembrane receptor to promote apoptosis and inhibit cell proliferation in gist . 
the results achieved to date in the treatment of gist with imatinib have been encouraging in terms of both tumour metastases and shrinkage of the tumour mass [ 22 ]  . no specific indications exist for the use of radiotherapy as either primary or adjuvant treatment . 
in principle , radiotherapy can be used to sterilise possible microscopic disease foci in all those cases at a significant risk for postoperative recurrence and in cases of macroscopic residual tumour or local relapse . 
however , larger studies are needed to assess the real impact of radiotherapy on local disease control and patient survival [ 23 ]  . as for the use of chemotherapy , the oncological literature from the preimatinib days reports cumulative data regarding leiomyosarcomas as a single histological entity without distinguishing by site of occurrence . 
the data on chemotherapy in gist are therefore extrapolated from papers reporting the results of chemotherapy in soft - tissue sarcomas of the adult . the literature shows that antineoplastic chemotherapy does not play a prominent role in the treatment of gastrointestinal stromal tumours . 
clinical response was 10% and 5% in first - line and second - line treatment , respectively , that is , considerably lower than commonly observed in other softtissue sarcomas where response is 40% and approximately 30% in leiomyosarcomas . 
today , following the demonstration of the efficacy of imatinib , chemotherapy plays no more than a marginal role in the treatment of gists . in view of these issues related to treatment options , the role of ct needs to be emphasised . 
our review of 26 cases of gist examined with ct has demonstrated that the large size of these tumours and signs of locoregional infiltration are suggestive of lesions with a high malignancy potential , whereas the presence of distant metastasis is a clear indicator of malignancy , as in other neoplastic lesions . 
i risultati fino ad ora ottenuti nel trattamento di questo tipo di patologia mediante limatinib sono stati promettenti sia nei confronti dei tumori metastatici sia nella riduzione dimensionale delle masse [ 22 ]  . non esistono a tuttoggi indicazioni specifiche circa lutilizzo della radioterapia n come trattamento primario n come terapia adiuvante . 
in linea di principio la radioterapia pu essere utilizzata in tutti quei casi che presentano un rischio significativo di recidiva post - chirurgica allo scopo di sterilizzare eventuali foci microscopici di malattia , e nei casi di residuo macroscopico o di recidiva locale . 
tuttavia , sono necessari studi pi appropriati al fine di valutare il reale impatto della radioterapia sul controllo locale della malattia e sulla sopravvivenza [ 23 ]  . per quanto riguarda limpiego della chemioterapia , la letteratura oncologica nellera pre - imatinib riporta dati cumulativi riguardanti i leiomiosarcomi come entit istologica senza distinguerli per sede dinsorgenza , n esistono pubblicazioni specifiche sui gist , se si esclude un recente studio retrospettivo dellitalian sarcoma group [ 24 ]  . 
i dati sul trattamento chemioterapico dei gist sono pertanto estrapolati da pubblicazioni riportanti i risultati relativi al trattamento chemioterapico dei sarcomi delle parti molli delladulto . dalla letteratura emerge come la chemioterapia antiblastica non abbia avuto un ruolo determinante nel trattamento dei tumori stromali gastrointestinali . 
le risposte cliniche sono state del 10% e del 5% rispettivamente in prima linea e seconda linea di trattamento , percentuali diverse da quelle comunemente osservate negli altri sarcomi dei tessuti molli in cui il tasso di risposte del 40% e nel sottogruppo dei leiomiosarcomi , del 30% circa . 
oggi , in seguito alla dimostrata efficacia dellimatinib nella terapia dei gist , la chemioterapia riveste un ruolo del tutto marginale nel trattamento di questi tumori . sulla base di queste problematiche legate alle possibilit terapeutiche va sottolineato il ruolo della tc . 
la revisione dei 26 casi di gist valutati in tc ha evidenziato come le notevoli dimensioni ed i segni di infiltrazione dei tessuti locoregionali siano indicativi di lesioni con elevato potenziale di malignit , mentre la presenza di metastasi a distanza rappresenta un chiaro indicatore di malignit , come per altro in quasi tutte le forme neoplastiche . 
nei casi in cui vengano evidenziati tumori di grandi dimensioni e / o segni di infiltrazione possibile impostare una opportuna terapia adiuvante prima dellintervento , consentendo cos una maggior radicalit chirurgica al fine di migliorare la prognosi del paziente . 
levidenza alla tc di lesioni secondarie gi al momento della diagnosi consente invece di indirizzare il paziente verso la terapia medica basata sullutilizzo dellimatinib . le altre caratteristiche morfologiche e di enhancement a . 
it is therefore indispensable in clinical staging and treatment planning , as well as being useful in the follow - up of patients treated with either surgery or pharmacological therapy ( imatinib )  . conclusioni in conclusione , la tc in virt della sua elevata panoramicit e risoluzione di contrasto fornisce informazioni determinanti nel riconoscimento e nella caratterizzazione dei reperti radiologici caratteristici dei gist . 
paganelli3 1facolt di medicina e chirurgia , universit degli studi di milano , via festa del perdono 7 , i - 20122 milano , italy 2divisione di radiologia , 3divisione di medicina nucleare , 4divisione di oncologia medica , 5divisione di epidemiologia e biostatistica , istituto europeo di oncologia irccs , via ripamonti , 435 , i - 20141 , milano , italy correspondence to : m . 
tcmd e pet / tc hanno mostrato alta sensibilit e specificit nella diagnosi di recidiva locale di tumore del retto . entrambe le metodiche sono state ugualmente accurate nella diagnosi di metastasi epatiche . 
la tcmd ha mostrato maggiore sensibilit e valore predittivo positivo nella diagnosi di metastasi polmonari . key words pet / ct computed tomography rectal cancer recurrence fluorodeoxyglucose parole chiave pet / tc tomografia computerizzata carcinoma del retto recidiva fluorodesossiglucosio m . 
the percentage of patients who develop local or distant recurrence following curative surgical resection is relatively high , probably due to the presence of neoplastic foci that remain undetected at the time of surgery [ 1 ]  . 
more than one third of patients with colon or rectal cancer develop hepatic metastases [ 2 ] and / or pulmonary metastases [ 3 ] , and this typically occurs within 2 years after surgery [ 4 ]  . 
the early diagnosis of local or distant recurrence is important in that further surgery , radiotherapy and chemotherapy , separately or combined in an integrated multidisciplinary approach , may improve survival and quality of life . 
unfortunately , no standardized follow - up strategy has been yet developed for patients with rectal cancer treated with curative resection [ 5 ]  . to our knowledge no previous study has compared the role of multidetector computed tomography ( mdct ) and that of f18 - fluorodeoxyglucose positron emission tomography - computed tomography ( fdg - pet / ct ) in the follow - up of these patients . 
the aim of this retrospective study was to compare the diagnostic value of mdct and fdg - pet / ct in the diagnosis of local recurrence and distant metastases after radical surgery for rectal cancer . materials and methods patients our institutional guidelines for the follow - up of patients after rectal cancer resection recommend clinical assessment every 46 months [ including serum carcinoembryonic antigen ( cea ) testing ] , abdominal and pelvic mdct every 6 months , chest radiography every year and colonoscopy within 1 year of surgery and every 23 years thereafter . 
this retrospective study included all patients treated with radical surgery for rectal cancer between 2000 and 2004 and who underwent fdg - pet / ct for a suspicion of local or distant recurrence aroused by clinical follow - up or mdct findings in accordance with our guidelines . 
fdg - pet / ct and mdct were performed within 30 days ( mean 22 days ) of one another . the patients had undergone radiotherapy or chemotherapy depending on initial disease stage in accordance with the following indications : patients without sigmoid involvement , with an initial stage greater than t2 , or with n + and any t stage underwent radiotherapy before or after surgery , in combination with various chemotherapy schedules . 
la percentuale di pazienti che sviluppano recidiva locale o a distanza dopo la resezione chirurgica considerata curativa relativamente elevata , probabilmente a causa della presenza di focolai neoplastici non evidenziati al momento dellintervento chirurgico [ 1 ]  . 
pi di un terzo dei pazienti con tumore del colon o del retto sviluppa metastasi epatiche [ 2 ] , e / o metastasi polmonari [ 3 ] , e questo si verifica di solito entro 2 anni dallintervento chirurgico [ 4 ]  . 
la diagnosi precoce di recidiva locale o a distanza importante perch un ulteriore approccio chirurgico , radioterapico e chemioterapico , ciascuno singolarmente o associati in un approccio multidisciplinare integrato , possono migliorare la sopravvivenza e la qualit di vita . 
purtroppo , non esiste ancora una strategia di follow - up standardizzata per i pazienti con tumore del retto sottoposti a intervento chirurgico curativo [ 5 ]  . per quanto a nostra conoscenza dalla letteratura , nessuno studio ha finora confrontato il ruolo della tc multistrato ( tcmd ) e della pet / tc come indagini di follow - up in questi pazienti . 
lo scopo di questo studio retrospettivo stato quindi quello di confrontare la validit diagnostica della tcmd e della pet / tc nella diagnosi di recidiva locale e di metastasi a distanza in pazienti sottoposti a chirurgia radicale di tumore del retto . materiali e metodi pazienti le linee - guida attualmente in uso presso il nostro istituto per il follow - up di pazienti con tumore del retto operato , prevedono una valutazione clinica ogni 46 mesi ( che include dosaggio del cea ematico ) , una tcmd addominopelvica ogni 6 mesi , una radiografia del torace annuale , una colonscopia entro un anno dalla chirurgia e poi ogni 23 anni . 
sono stati inclusi in questo studio retrospettivo tutti i pazienti sottoposti a intervento di chirurgia radicale per tumore del retto tra il 2000 e il 2004 , che sono stati sottoposti ad una pet / tc per il dubbio di recidiva locale o a distanza sollevato da dati clinici o dalla tcmd previsti nel follow - up , secondo quanto indicato dalle nostre linee guida . 
i pazienti inclusi nello studio erano stati sottoposti a radioterapia o chemioterapia in base al loro stadio iniziale secondo le seguenti indicazioni : in assenza di coinvolgimento del sigma , con uno stadio iniziale superiore a t2 o qualunque t con n + , i pazienti sono stam . 
the scans were obtained during a single breath - hold with the following parameters : contiguous acquisition of 2.5 - mm - thick slices , field of view 320280 mm , 120 kv , 240300 ma , 0.8 - s rotation , matrix 512512 and standard reconstruction algorithm . fdg - pet / ct before administration of fdg , all patients fasted for 6 h and underwent blood glucose tests . 
images were acquired with an integrated pet / ct device ( discovery ls , ge medical systems ) composed of an advance nxi pet scanner and an 8 - slice light speed plus ct scanner . 
the axes of the two systems were mechanically aligned to enable transfer of the patient , lying supine , from the ct gantry to the pet scanner with a 60 - cm table shithe pet / ct data were coregistered on a computer . 
ct acquisition parameters were 120 kv , 80 ma , tube rotation time 0.8 s , pitch 1 , 5 and slice thickness 5 mm and were matched with pet image thickness . 
pet data were interactively reconstructed with segmented attenuation correction with the use of ct images [ 6 ]  . the segmented images were displayed as means by the xeleris software ( ge medical systems )  . 
in patients with excessive residual urine , a pelvic acquisition was obtained after positioning a 3 - lumen foley catheter . image interpretation the original reports were considered as the result of the examination . 
any new tissue arising at , or close to , the site of the ti sottoposti a radioterapia prima o dopo la chirurgia , in associazione a chemioterapia secondo vari schemi . 
tutti i pazienti inclusi in questo studio avevano una tc torace - addome - pelvi eseguita per stadiazione prima della chirurgia . nessun paziente affetto da diabete stato incluso in questo studio retrospettivo . diagnostica per immagini tcmd gli esami tc sono stati eseguiti con tc 16 detettori ( lightspeed scanner , general electric medical systems , milwaukee , wi , usa ) , dalle basi polmonari alla sinfisi pubica . 
le scansioni sono state acquisite 70 secondi ( addome superiore ) e 150 secondi ( pelvi ) dopo linizio delliniezione ev di 2 , 0 ml / kg di mdc iodato 350 mg / ml , somministrato con un flusso di 2 ml / s . 
prima dellesame i pazienti hanno bevuto 23 bicchieri dacqua e svuotato la vescica per evitare artefatti causati dalle urine . le immagini sono state acquisite con uno scanner pet / tc integrato ( discovery ls , ge medical systems , milwaukee , wi , usa ) che consiste in un advance nxi pet scanner e un 8 - slice light speed plus ct scanner . 
gli assi dei due sistemi sono stati allineati meccanicamente per muovere il paziente , in posizione supina , dal gantry della tc alla pet , con uno shift del tavolo di 60 clesame pet / tc stato co - registrato su supporto hardware . 
i parametri di acquisizione dellesame tc sono : 120 kv , 80 ma , tempo di rotazione del tubo 0 , 8 s , pitch 1 , 5 , e spessore di strato 5 mm , e sono stati accoppiati allo spessore delle immagini pet . 
subito dopo lacquisizione delle immagini tc , sono state acquisite le immagini pet per coprire lo stesso campo di vista assiale . lacquisizione , in direzione caudo - craniale , stata fatta in 2d ( 4 minuti / posizione del lettino ) , circa 60 minuti dopo liniezione ev di 5 mbq / kg di fdg . 
no quantitative study of standardized uptake value ( suv ) was performed on fdg - pet / ct data because no cut - off value has been established that is definitively indicative of the presence of neoplastic tissue in patients with rectal cancer . 
therefore , a qualitative image analysis was used , which is equivalent to quantitative analysis [ 7 ]  . mdct and fdg - pet / ct results were then independently compared with histology of biopsy or surgical specimens or with the outcome of at least 2 years follow - up . 
sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) for the diagnosis of local or distant recurrence were determined for mdct and fdg - pet / ct . confidence intervals for sensitivity for local recurrence were calculated for each method and then compared . results this study considered 67 patients treated with surgery for rectal carcinoma : 25 had undergone radiotherapy ( 20 before and 5 after surgery ) , 23 had undergone chemotherapy ( 5 before and 18 after surgery ) and 19 had undergone both radiotherapy and chemotherapy after surgery . 
of these , 15 ( 22% ) had local recurrence , 17 ( 25% ) had hepatic metastases ( 7 of whom had local recurrence as well ) and 8 ( 12% ) had pulmonary metastases ( 2 of whom had local recurrence as well )  . local recurrence local recurrence occurred in 15 / 67 patients ( 22% )  . 
initial disease stage of patients with local recurrence was one t2n1 , three t3n0 , five t3n1 , one t3n2 , one t4n0 and one unknown stage because the patient came to our observation after undergoing surgery at another hospital . 
on the basis of initial disease stage , 6 / 15 patients underwent adjuvant chemotherapy , 5 / 15 underwent chemotherapy before and after surgery and 4 / 15 underwent radiotherapy and chemotherapy . the presence of recurrence was suspected on the basis of the clinical data in three patients , increased cea levels in two patients and radiological or endoscopic follow - up in ten patients . 
the first technique to produce a diagnosis of local recurrence was mdct in 6 / 15 patients , fdg - pet / ct in 4 / 15 and colonoscopy in 5 / 15 . both mdct and fdg - pet / ct yielded true negative diagnoses of local recurrence in 51 patients . 
mdct yielded one false positive restata eseguita una acquisizione della regione pelvica dopo posizionamento di catetere di foley a triplo lume . interpretazione delle immagini il referto originale stato considerato come risultato dellesame . 
qualunque nuovo tessuto in corrispondenza della anastomosi chirurgica , o in area ad essa adiacente in ambito pelvico , qualora presentasse caratteristiche di asimmetria , irregolarit , disomogeneo enhancement contrastografico o modificazione rispetto a esami precedenti stato considerato come recidiva locale . 
sui dati della fdg - pet / ct non stato effettuato nessuno studio quantitativo del valore standard di uptake ( standardized uptake value : suv ) perch in letteratura non vi dimostrazione di un valore di cut - off che sia con certezza indicativo della presenza di tessuto neoplastico in pazienti con tumore del retto . pertanto stata usata unanalisi qualitativa delle immagini , che sarebbe paragonabile ad una analisi quantitativa [ 7 ]  . i risultati di tcmd e pet / tc sono stati confrontati in modo indipendente con listologia ( ottenuta con biopsia o con chirurgia ) , o con i risultati di un follow - up minimo di due anni . 
sensibilit , specificit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) nella diagnosi di recidiva locale o a distanza sono stati calcolati per tc e pet / tc . 
gli intervalli di confidenza nella sensibilit diagnostica di recidiva locale sono stati calcolati per entrambe le metodiche e confrontati . risultati in questo studio sono stati inclusi 67 pazienti operati per carcinoma del retto : 25 sono stati sottoposti a radioterapia ( 20 prima e 5 dopo la chirurgia ) , 23 a chemioterapia ( 5 prima e 18 dopo la chirurgia ) , e 19 sia a radioterapia che a chemioterapia dopo la chirurgia . 
di questi : 15 ( 22% ) hanno sviluppato recidiva locale , 17 ( 25% ) hanno sviluppato metastasi epatiche ( 7 dei quali avevano anche recidiva locale ) , 8 ( 12% ) hanno sviluppato metastasi polmonari ( 2 dei quali avevano anche recidiva locale )  . recidiva locale la recidiva locale si verificata in 15 / 67 pazienti ( 22% )  . 
la stadiazione iniziale dei pazienti con recidiva locale era : un t2n1 , tre t3n0 , cinque t3n1 , un t3n2 , un t4n0 , uno non noto perch il paziente giunto alla nostra osservazione dopo lintervento eseguito in un altro ospedale . 
sensitivity , specificity , ppv and npv in the diagnosis of local recurrence were 100% , 98% , 93% and 100% for mdct , and 93% , 98% , 93% and 98% for fdgpet / ct , respectively . 
the difference in sensitivity between the two techniques was not statistically significant , as demonstrated by the overlapping confidence intervals ( 0.781.0 for mdct and 0.681.0 for fdg - pet / ct )  . hepatic metastases during the follow - up period , 17 / 67 patients ( 25% ) developed hepatic metastases . 
initial disease stage in patients with chemioterapia adiuvante , 5 / 15 a chemioterapia prima e dopo chirurgia , 4 / 15 a radio e chemioterapia . la presenza di recidiva stata suggerita in 3 pazienti da dati clinici , in 2 pazienti da incremento del marcatore tumorale ( cea ) , in 10 pazienti da esami di follow - up radiologico o endoscopico . 
la mediana del tempo intercorso tra chirurgia e recidiva locale stata di 22 mesi ( range 1248 mesi )  . la prima modalit che ha posto diagnosi di recidiva locale stata la tcmd in 6 / 15 pazienti , la pet / tc in 4 / 15 e la colonscopia in 5 / 15 . sia tcmd che pet / tc hanno fornito risultati veramente negativi per recidiva locale in 51 pazienti . 
the wall thickening limited to the left portion of the rectal wall , close to the suture line , was reported to be a possible local recurrence ( a )  . 
sensibilit , specificit , vpp e vpn nella diagnosi di recidiva locale sono risultati rispettivamente 100% , 98% , 93% e 100% per la tcmd , e 93% , 98% , 93% e 98% per la pet / tc . 
la differenza di sensibilit tra le due metodiche non stata statisticamente significativa , come mostrato dalla sovrapposizione degli intervalli di confidenza ( 0 , 781 , 0 per la tcmd , e 0 , 681 , 0 per la pet / tc )  . metastasi epatiche durante il periodo di follow - up 17 / 67 pazienti ( 25% ) hanno sviluppato metastasi epatiche . 
la stadiazione iniziale nei pazienti con metastasi epatiche era : t2n0 in 4 pazienti , t2n1 in 3 pazienti , t3n0 in 4 pazienti , t3n1 in 5 pazienti , t3n2 in 1 paziente . 
sensibilit , specificit , vpp e vpn nella diagnosi di metastasi epatiche stata del 100% per entrambe le metodiche . metastasi polmonari metastasi polmonari sono state riscontrate in 8 / 67 pazienti ( 12% )  . 
la tcmd ha posto la prima diagnosi di metastasi polmonari in 6 / 8 casi in cui le lesioni sono state messe in evidenza esaminando con finestra da polmone le scansioni effettuate alle basi polmonari ; la pet / tc in 2 / 8 casi . 
circa il 25% delle recidive da carcinoma del colon - retto sono recidive locoregionali e il 15%20% sono metastasi a distanza potenzialmente resecabili con intento curativo [ 9 ] : una diagnosi precoce che consenta una chirurgia con intento curativo dovrebbe essere lobiettivo del follow - up [ 10 ]  . 
infatti , la riduzione di mortalit legata alla diagnosi precoce di recidiva extra - intestinale dimostrata dai programmi di follow - up intensivi stata equivalente a quella ottenuta dalla terapia adiuvante nei pafig . 
2a , b multidetector computed tomography ( mdct ) performed 18 months after rectal cancer resection and radiotherapy shows irregular and inhomogeneous thickening of the anastomotic wall with dense tissue in the surrounding fat and irregular shape of the suture ( a )  . 
2a , b tcmd , eseguita 18 mesi dopo resezione di carcinoma rettale e radioterapia , che mostra ispessimento irregolare e disomogeneo del tratto anastomotico , con tessuto denso nel grasso perirettale e irregolarit della sutura ( a )  . 
la diagnosi di recidiva locale stata poi confermata anche dalla pet / tc ( b )  . hepatic metastases was t2n0 in four , t2n1 in three , t3n0 in four , t3n1 in five and t3n2 in one . 
the first diagnosis of pulmonary metastasis was provided by mdct in 6 / 8 cases , in which the lesions were visualized by examining the lung base scans with a lung window setting ; fdg - pet / ct provided the first diagnosis in 2 / 8 cases . 
this is comparable to the 30%40% recurrence rate in the first 3 years after surgery reported in the literature [ 8 ]  . approximately 25% of colorectal carcinoma recurrences are locoregional , and 15%20% are potentially resectable distant metastases [ 9 ]  . 
the reduction in mortality resulting from the early diagnosis of extraintestinal recurrence demonstrated by intensive followup programmes was equivalent to that obtained by adjuvant treatment in patients with advanced cancers [ 11 ]  . 
i programmi di follow - up per i pazienti operati per tumore colo - rettale , che includono visita clinica , valutazione del cea ematico , radiografia del polmone , imaging del fegato e colonscopia , migliorano la sopravvivenza , ma non chiaro quale sia la frequenza ottimale degli esami e delle visite [ 12 ]  . 
una metanalisi degli studi prospettici che hanno dimostrato una riduzione del 9%13% della mortalit a 5 anni nei pazienti inclusi in programmi di follow - up intensivo , afferma che i programmi di follow - up intensivo sono economicamente giustificati e andrebbero inclusi nella pratica clinica [ 11 ]  . 
a meta - analysis of prospective studies demonstrating a 9%13% decrease in 5 - year mortality rates in patients included in intensive follow - up programmes [ 11 ] stated that intensive follow - up programmes are economically justified and should become normal clinical practice [ 11 ]  . nevertheless , due to the lack of certainties in this respect , specialised cancer centres adopt different strategies for the management of these patients . 
in the event of increased cea levels , associated with negative results on other follow - up tests , pet / ct should be recommended [ 10 ] given that it plays an important complementary role in the diagnosis of local and distant recurrence [ 4 , 13 , 14 ] and may play a role in subsequent patient management [ 15 , 16 ]  . 
previous studies have shown that the sensitivity and specificity of pet / ct for differentiating between benign and malignant presacral abnormalities reach 100% and 96% , respectively [ 17 ]  . 
in the same study , one third of extrahepatic metastases were missed at ct ( 64% sensitivity ) , whereas pet / ct failed to detect extrahepatic lesions in 11% of cases only ( 89% sensitivity ) [ 18 ]  . 
in a prospective study performed on 102 patients with colorectal carcinoma , pet altered the treatment strategy in 56% of patients as a direct result of unexpected findings [ 15 ]  . 
our retrospective study did not evaluate the mri examinations because mri is not yet part of the standard followup programme . in our study population , fdg - pet / ct and mdct had similar sensitivity , specificity , ppv and npv values for the diagnosis of local recurrence . 
this may be due to the fact that the interpretation of ct images normally relies on dimensional criteria , with large masses usually being interpreted as malignant , even though some are fibrotic or inflammatory tissue [ 17 ]  . 
pet / ct false positive results have been reported to correlate with local inflammatory processes or with the effects of radiotherapy , especially when performed less than 6 months earlier [ 20 ]  . this could explain our only false positive result at fdgpet / ct , which concerned a patient who had never undergone adjuvant therapy after surgery and who had a postoperative reparative process of the bowel wall . in this retrospective study , mdct had greater specificity for the diagnosis of local recurrence than that reported by other studies [ 18 , 19 ]  . 
whereas at the time of reporting the nuclear medicine physicians had just started interpreting pet / ct images , the radiologists had several years experience reading mdct images . cologici specializzati seguono diverse strategie di gestione di questa tipologia di pazienti . 
in caso di aumento del cea , con altri esami di follow - up negativi , la pet / tc dovrebbe essere consigliata [ 10 ] perch svolge un importante ruolo complementare nella diagnosi di recidiva locale e a distanza [ 4 , 13 , 14 ] e pu avere un ruolo nella successiva gestione del paziente [ 15 , 16 ]  . 
studi precedenti hanno mostrato che la sensibilit e specificit della pet / tc nel differenziare le anomalie presacrali benigne da quelle maligne raggiungono rispettivamente valori del 100% e 96% [ 17 ]  . 
nello stesso studio , un terzo delle metastasi extra - epatiche non sono state diagnosticate dalla tc ( sensibilit del 64% ) , mentre la pet / tc ha fallito nella diagnosi di lesioni extraepatiche solo nell11% dei casi ( sensibilit dell89% ) [ 18 ]  . 
 [ 19 ] hanno suggerito che la fdg - pet superiore alla tc e alla rm nel prevedere la risposta a trattamenti multimodali pre - chirurgici in tumori rettali localmente avanzati . 
 nella popolazione di pazienti inclusa in questo studio , la pet / tc e la tcmd hanno mostrato valori paragonabili di sensibilit , specificit , vpp e vpn nella diagnosi di recidiva locale . 
questo pu essere dovuto al fatto che linterpretazione delle immagini tc solitamente legata a criteri dimensionali , cosicch grandi masse sono di solito interpretate come maligne , anche se alcune di esse rappresentano solo tessuto fibrotico o flogistico [ 17 ]  . 
i falsi positivi della tc / pet sono stati descritti come correlati a processi flogistici locali o agli effetti della radioterapia , in particolare se tali trattamenti erano stati effettuati meno di 6 mesi prima [ 20 ]  . 
questo potrebbe spiegare il solo caso falsamente positivo della pet / tc nella diagnosi di recidiva locale , che ha riguardato un paziente che non aveva ricevuto nessuna terapia adiuvante dopo la chirurgia , con esiti post - chirurgici sulla parete intestinale . 
 in questo studio retrospettivo , la tcmd ha mostrato una specificit nella diagnosi di recidiva locale superiore rispetto a quanto riportato da altri studi [ 18 , 19 ]  . 
mentre infatti i medici nucleari , al tempo della refertazione degli esami considerati , avevano appena iniziato lesperienza della interpretazione delle immagini pet / tc , i radiologi avevano diversi anni di esperienza nellinterpretazione delle immagini tcmd . i risultati falsamente negativi della pet / tc sono di solito legati alle dimensioni della lesione ( meno di 5 mm ) e / o alla chemioterapia in corso al momento dellesame . 
in our study , the only fdg - pet / ct false negative result concerned a 5 - mm lesion , which appeared 7 months after the end of the chemotherapy course . 
in this study , mdct and fdg - pet / ct showed the same level of accuracy in diagnosing hepatic metastases , yielding no false positive or false negative results , whereas previous studies have reported different specificity values for ct and pet / ct ( 70% and 90% , respectively ) [ 18 ]  . 
this difference could depend on the better quality of ct images obtained with the multidetector technique , which allows for optimal contrast enhancement and spatial resolution . eight patients ( 12% ) in our study developed pulmonary metastases , and only two of them had local recurrence . 
 [ 21 ] demonstrated that pulmonary metastases also occur in patients with low - stage initial disease ; however , the patients with pulmonary metastases in our study had advanced - stage initial disease ( t2n1 and t4n0 )  . 
in our study , fdg - pet / ct failed to identify two cases of pulmonary metastases ( false negative results ) , one of which was very small ( 5 mm )  . 
in our experience , mdct proved to have a high level of accuracy in the diagnosis of pulmonary metastases , above all due to a multidisciplinary radiological - oncological approach . when reporting ct examinations , particular attention is paid to the patients clinical data , and the scans are always compared to previous ones ( potter kc et al . , european congress of radiology 2005 , vienna )  . 
therefore , positive findings on lung ct , in particular when the images are compared with previous negative scans , may be considered extremely accurate . our study has some limitations . 
no statistical analysis was performed to determine sample suitability , and our series is probably too small to indicate whether fdg - pet / ct or mdct is more accurate in the diagnosis of local or distant recurrence of operated rectal cancer . 
another limit lies in patient selection : as this was a retrospective study , patients did not undergo mdct and fdg - pet / ct at the same time , as would have been the case if these examinations had been part of a standard protocol . 
this could mean that one technique , in this case mdct , may have failed to detect something that was later diagnosed by the other technique , in this case fdg - pet / ct . 
this limitation would have been avoided with a prospective design , but this would have involved greater exposure and costs in the absence of proof of the usefulness of pet / ct . 
for this reason , we decided to compare the diagnostic value of the two techniques retrospectively , regardless of the risk of encountering these limitations . di 5 mm , sviluppatasi 7 mesi dopo il completamento della chemioterapia . 
in questo studio tc e pet / tc hanno mostrato la stessa accuratezza nella diagnosi di metastasi epatiche , in assenza di falsi risultati , mentre studi precedenti avevano mostrato specificit differenti per tc e pet / tc ( 70% e 90% rispettivamente ) [ 18 ]  . 
in questo studio la pet / tc non ha identificato 2 casi di metastasi polmonari ( casi falsi negativi ) , uno dei quali era una lesione molto piccola ( 5 mm )  . 
infatti , durante la refertazione degli esami tc , una elevata attenzione viene prestata alla clinica e gli esami sono sempre confrontati con i precedenti ( potter kc et al . , european congress of radiology 2005 , vienna )  . 
questo risulta particolarmente utile per lesioni polmonari piccole , come quelle che possono essere perse dallesame pet / tc . quindi , i risultati positivi della tc del polmone , in particolare quando i reperti sono confrontati con esami precedentemente negativi , possono essere considerati molto accurati . questo studio ha alcuni limiti . 
non stata eseguita una analisi statistica per determinare lappropriatezza del campione e la nostra casistica probabilmente insufficiente per indicare quale esame diagnostico , tra la pet / tc e la tcmd , sia pi accurato nella diagnosi di recidiva locale o a distanza di tumori del retto operati . 
un altro limite risiede nella selezione dei pazienti : essendo questo uno studio retrospettivo , i pazienti non hanno eseguito tcmd e pet / tc allo stesso tempo , come sarebbe opportuno se tali esami facessero parte di un protocollo standardizzato . 
questo rende possibile che ad una modalit , in questo caso alla tcmd , sia sfuggito qualcosa che stato poi diagnosticato dallaltra modalit , in questo caso la pet / tc . 
questo limite sarebbe stato evitato con una selezione dei pazienti di tipo prospettico , ma ci avrebbe comportato una esposizione ed un costo aggiuntivi , in assenza di una dimostrazione certa dellutilit dellesame pet / tc . 
per tale motivo , abbiamo deciso di confrontare il valore diagnostico delle due modalit in modo retrospettivo , nonostante il rischio di incorrere in tali limiti . conclusions in conclusion , the diagnostic value of fdg - pet / ct and mdct in the follow - up of patients operated on for rectal cancer is comparable , and the advantages of fdg - pet / ct in conclusione , il valore diagnostico attuale di pet / tc e tcmd nel follow - up di pazienti operati di tumore del retto paragonabile , i vantaggi della pet / tc sono la possibilit di valutare con un singolo esame tutto il corpo , la pi bassa conclusioni m . 
in most specialised centres , the follow - up of patients after surgery for rectal carcinoma includes mdct scans every 6 months : we believe the scan should be extended to the chest given the relatively high incidence of pulmonary metastases . 
at present , fdg - pet / ct should only be used to solve any diagnostic doubt resulting from mdct , or in the event of discrepancy between clinical and imaging findings . esposizione alle radiazioni e la possibilit , in futuro , di eseguire un unico esame pet ed una tc con mdc , somministrato per via endovenosa [ 2325 ]  . 
il follow - up dei pazienti operati per carcinoma rettale prevede , nella maggioranza dei centri specialistici , lesecuzione di tcmd ogni 6 mesi : riteniamo che lesame dovrebbe essere esteso al torace , per la relativamente alta incidenza di metastasi polmonari . 
krestin2 1dipartimento di radiologia e dipartimento cuore , imaging cardiovascolare non invasivo , azienda ospedaliera di parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , holland 3dibimel , sezione di scienze radiologiche , universit di palermo , italy 4dipartimento di radiologia , universit degli studi di verona , italy 5dipartimento di radiologia , universit degli studi di trieste , italy correspondence to : f . 
cademartiri , viale rustici , 2 , i - 43100 , parma , italy , tel . : + 39 - 052 - 1961833 , e - mail : filippocademartiri@hotmail.com received : 20 august 2006 / accepted : 2 october 2006 / published online : 23 july 2007 abstract the goal of this article is to illustrate the main invasive and noninvasive diagnostic modalities to image the vulnerable coronary plaque , which is responsible for acute coronary syndrome . 
the main epidemiologic and histological issues are briefly discussed in order to provide an adequate background . comprehensive coronary atherosclerosis imaging should involve visualization of the entire coronary artery tree and plaque characterization , including three - dimensional morphology , relationship with the lumen , composition , vascular remodelling and presence of inflammation . 
in particular , we describe multislice computed tomography , which at present seems to be the most promising noninvasive tool for an exhaustive image - based quantification of coronary atherosclerosis . key words coronary artery disease imaging vulnerable plaque multislice computed tomography ct riassunto con questo articolo si vogliono illustrare le principali metodiche di imaging invasivo e non invasivo , che si prefiggono di identificare la placca vulnerabile coronarica , responsabile delle sindromi coronariche acute . 
un imaging onnicomprensivo della malattia aterosclerotica coronarica dovrebbe essere in grado di visualizzare lintero albero coronarico e caratterizzare la placca nei suoi vari aspetti quali la morfologia tridimensionale , il rapporto con il lume , la composizione tessutale , il rimodellamento vascolare e la presenza di infiammazione . 
nessuna tecnica riesce singolarmente a fornire un quadro talmente completo e nessuna modalit disponibile identifica in modo inequivocabile la placca vulnerabile . particolare attenzione stata rivolta alla tomografia computerizzata multistrato , che sembra , al momento , la tecnica pi promettente nel panorama delle metodiche non invasive per la quantificazione complessiva per immagini della malattia aterosclerotica coronarica . parole chiave coronaropatia aterosclerotica imaging placca vulnerabile tomografia computerizzata multistrato ct introduction introduzione atherosclerosis is a degenerative inflammatory process that affects artery walls . 
this classification reflects the natural history of the disease , which is asymptomatic in the initial stages laterosclerosi un processo degenerativo - infiammatorio che interessa la parete dei vasi arteriosi . 
in the past , vascular stenosis was considered the hallmark of the disease . currently , emphasis is placed on the atherosclerotic plaque , which represents the pathological substrate for vascular stenosis [ 3 , 4 ]  . the introduction over the past 10 years of sophisticated ultrasound ( us ) probes mounted on angiographic catheters has enabled in vivo visualisation of atherosclerotic plaque within the coronaries . 
the aim of this review is to illustrate the results provided by invasive and noninvasive imaging modalities and discuss the advantages and limitations , with special reference to multislice computer tomography ( msct )  . tica , mentre negli stadi pi avanzati progredisce in maniera variabile . 
viene dato attualmente risalto alla placca aterosclerotica , che rappresenta il substrato anatomo - patologico della stenosi vascolare [ 3 , 4 ]  . nellultimo decennio lintroduzione di sofisticate sonde ecografiche applicate a cateteri angiografici ha permesso la visualizzazione in vivo della placca aterosclerotica nelle coronarie . 
lo scopo del lavoro mostrare i risultati ottenuti dalle tecniche di imaging invasivo e non invasivo , illustrandone i vantaggi ed i limiti , con particolare attenzione per la tomografia computerizzata multistrato ( tcms )  . epidemiologia le malattie cardiovascolari sono la prima causa di morte nei paesi industrializzati e prevedibilmente lo diventeranno anche nei paesi in via di sviluppo . 
nei prossimi decenni la mortalit per cardiopatia ischemica destinata ad aumentare dell80% nelle donne e del 100% negli uomini , con un aumento pi marcato nei paesi in via di sviluppo rispetto ai paesi industrializzati [ 5 ]  . 
secondo le pi recenti statistiche dellamerican heart association , laterosclerosi delle coronarie ha una prevalenza del 6 , 9% nella popolazione e un tasso di mortalit per infarto di 177 , 8 per 100000 abitanti [ 6 ]  . 
i dati europei pi recenti riportano un tasso di mortalit di 125 per gli uomini e di 63 per le donne , seppure con unampia variabilit regionale per la presenza di gradienti a direzione nord - sud ed est - ovest . 
litalia ha un tasso di mortalit di 105 per gli uomini e di 51 per le donne [ 710 ]  . i sistemi sanitari si trovano a fronteggiare i costi dovuti allaumento della prevalenza della malattia e delle correlate procedure invasive . 
vi sono , pertanto , delle forti aspettative nei riguardi delle tecniche panoramiche non invasive , che potrebbero sostituire la diagnostica invasiva e fornire una diagnosi precoce di aterosclerosi coronarica , con impatto sul trattamento , la prognosi e il costo complessivo . biologia e fisiopatologia la prima manifestazione di aterosclerosi consiste in un accumulo di materiale lipidico visibile allesame macroscopico che prende il nome di stria lipidica ( fatty streak lesion )  . 
da questo nucleo iniziale , con gli anni , prende forma la placca aterosclerotica matura , la quale consiste in un core lipidico 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 639 epidemiology cardiovascular disease is the leading cause of death in industrialised countries and is emerging as a major cause of death in developing countries . 
over the next few decades , deaths due to ischaemic heart disease are expected to increase by 80% among women and 100% among men , with a more marked rise in developing countries compared with developed countries [ 5 ]  . 
according to the most recent american heart association statistics , coronary atherosclerosis has a prevalence of 6.9% in the general population and a mortality rate due to infarction equal to 177.8 per 100 , 000 inhabitants [ 6 ]  . 
recent data for europe report a mortality rate of 125 among men and 63 among women , but with wide regional variations due to north - south and east - west gradients . 
high expectations are therefore placed on noninvasive panoramic imaging modalities that could replace invasive diagnostic techniques and provide an early diagnosis of coronary atherosclerosis , with impact on treatment , outcomes and overall costs . biology and pathophysiology the first manifestation of atherosclerosis is the accumulation of fatty material , which is grossly visible and is called fatty - streak lesion . 
this means that coronary stenosis is the expression of advanced disease and that the disease needs to be characterised at an earlier stage [ 14 ]  . acute coronary events manifest when atherosclerotic plaque ruptures and blood comes into contact with the plaques lipid content , which is a potent procoagulant . plaque responsible for coronary thrombosis is defined as a culprit plaque at conventional coronary angiography ( cca )  . 
the new frontier is instead to characterise stable plaque that is likely to become complicated , known as vulnerable plaque , before the acute event occurs [ 15 ]  . culprit plaque is characterised on the basis of autopsy studies [ 1618 ] , and the study of vulnerable plaque relied on the experience gained from these studies . 
da ci si evince che la stenosi coronarica espressione di un processo patologico in fase avanzata e sorge quindi la necessit di caratterizzare la malattia in una fase pi precoce [ 14 ]  . levento coronarico acuto si manifesta quando una placca aterosclerotica si fissura e il sangue viene a contatto con il contenuto lipidico , il quale ha un elevatissimo potere procoagulante . 
la nuova ambiziosa frontiera quella di caratterizzare , invece , una placca stabile suscettibile di complicazione , definita placca vulnerabile , prima dellevento acuto [ 15 ]  . la placca culprit stata caratterizzata a partire da studi autoptici [ 1618 ]  . 
 [ 19 ] in seguito hanno identificato la placca vulnerabile come incline alla rottura , caratterizzata da un core lipidico ricoperto da un sottile cappuccio fibroso , e da cellule infiammatorie . 
 [ 20 , 21 ] una capsula fibrosa assottigliata , con spessore inferiore ai 65 m , fa perdere alla placca le caratteristiche di stabilit e la rende incapace di sopportare lo stress circonferenziale con successiva rottura . 
i criteri maggiori sono : linfiammazione ( presenza di monociti , macrofagi , linfoun ampio core lipidico con un sottile cappuccio fibroso lesposizione dellendotelio con liniziale aggregazione citi t ) delle piastrine lulcerazione della placca e una stenosi > 90% . 
 nonostante la placca vulnerabile sia lelemento primariamente responsabile dellulcerazione , anche le caratteristiche del sangue , se inclini alla trombosi ( sangue vulnerabile ) , e le caratteristiche del miocardio , se inclini allaritmia ( miocardio vulnerabile ) , dovrebbero essere tenute in considerazione nella valutazione del rischio coronarico , portando allidentificazione del paziente vulnerabile ad alto rischio di evento cardiaco acuto [ 28 ]  . 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 640 f . 
 [ 20 , 21 ] , plaque with a thin fibrous cap , less than 65 - m thick , loses its stability and becomes unable to withstand circumferential stress , with subsequent rupture . 
la visione planare dellalbero coronarico ( luminografia ) consente lesecuzione di una stima del lume vascolare ( quantitative coronary angiography , qca ) , ma non fornisce indicazioni sullaspetto delle pareti vascolari e leventuale presenza di placche [ 31 ]  . 
secondo una metanalisi il 49% delle lesioni colpevoli , ovvero responsabili di infarto miocardio acuto ( ima ) causato da stenosi non significative inferiori al 50% [ 32 ]  . 
molte di queste metodiche sono invasive ovvero basate sullintroduzione di un catetere , come lecografia intravascolare ( ivus ) , che considerata il gold standard per limaging di placca . ecografia intravascolare livus una tecnica invasiva in grado di fornire immagini assiali del lume e della parete dei vasi , superando la visione 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 641 f . 
2 erosion of a pathological intimal thickening and rupture of a thin fibrous cap atheroma may lead to thrombosis and result in an acute coronary syndrome , or it may heal . 
2 lerosione di un patologico ispessimento intimale e lulcerazione di un ateroma con sottile cappuccio fibroso possono provocare una trombosi ed originare una sindrome coronarica acuta oppure andare incontro a guarigione . 
planar visualisation of the coronary tree ( luminography ) allows estimation of the vascular lumen [ quantitative coronary angiography ( qca ) ] but does not provide information on the appearance of the vessel walls and the possible presence of plaque [ 31 ]  . 
according to a meta - analysis , 49% of culprit lesions responsible , that is , for acute myocardial infarction ( ami ) are related to nonsignificant stenosis less than 50% [ 32 ]  . 
ivus uses a catheter fitted with a miniature rotating transducer in mechanical systems or made up of an annular array of crystals ( up to 64 elements ) in electronic systems . 
frequencies employed are in the range of 20 and 40 mhz , with an axial resolution between 100 and 200 lateral resolution ranges from 200 to 250 m , depending on image depth . 
once inside the vessel , the catheter is withdrawn at a constant speed by means of a motorised mechanism while the study is recorded on a videotape . on ivus , the arterial wall usually displays a trilaminar appearance corresponding to the wall components : the intima , media and adventitia . 
ivus enables an accurate quantitative assessment of the vessel contours , luminal area , atheroma size ( which is relatively hyperechoic to the lumen and media ) , calcification , stent diameter and areas of remodelling [ 37 ]  . ivus may demonstrate the presence of an appreciable atherosclerotic burden in angiographically intact vessels , so this imaging modality may be considered useful for predictplanare dellangiografia . 
lapparecchiatura ivus si avvale di un catetere provvisto di un trasduttore miniaturizzato , rotante nei sistemi meccanici oppure costituito da una matrice anulare di cristalli ( fino a 64 elementi ) nei sistemi elettronici . 
le frequenze impiegate sono comprese tra 20 e 40 mhz , con una risoluzione assiale tra 100 e 200 la risoluzione laterale varia invece tra 200 e 250 m , a seconda della profondit di immagine . 
una volta posizionato allinterno del vaso il catetere viene ritirato con un meccanismo motorizzato a velocit costante e lo studio viene registrato su nastro . la parete arteriosa allindagine ivus mostra solitamente un aspetto trilaminare corrispondente ai componenti della parete : lintima , la media e lavventizia . 
livus consente unaccurata valutazione quantitativa dei contorni dei vasi , dellarea del lume , delle dimensioni dellateroma ( relativamente iperecogeno rispetto al lume e alla media ) , delle calcificazioni , del diametro degli stent e delle aree di rimodellamento [ 37 ]  . livus pu dimostrare la presenza di un apprezzabile carico aterosclerotico in vasi angiograficamente indenni e pertanto questa modalit di imaging potrebbe essere considerata utile nel predire il rischio di un evento acuto [ 38 ]  . sebbene livus consenta una dettagliata visione della parete dei vasi , linterpretazione della composizione di placca verte esclusivamente sulla semplice valutazione qualitativa degli echi . 
in particolare la visualizzazione delle placche inficiata da quelli da riverberazione ( ring - down ad anello , blood speckle ) , a meno che non si provveda a diminuire i guadagni , pur con il rischio di provocare unattenuazione del segnale nei tessuti bersaglio [ 37 ]  . numerosi studi in vivo mostrano risultati promettenti circa le effettive capacit di visualizzazione della placca vulnerabile e la sua correlazione con le sindromi coronariche acute [ 4246 ]  . 
in particolare , uno studio esteso alle tre coronarie ha evidenziato come nei pazienti con sindrome co03 cademartiri 23 - 07 - 2007 11 : 40 pagina 643 ing the risk of an acute event [ 38 ]  . 
hypoechoic plaque is defined as soft plaque , not in relation to its tissue composition but to the characteristics of it acoustic signal relative to the adventitia [ 39 , 40 ]  . 
calcific plaque is , instead , characterised by hypereflective echoes with the posterior shadow cone [ 41 ]  . in fact , mixed - composition plaque with a corresponding mixed sonographic appearance is very common . 
in particular , plaque visualisation is limited by reverberation artefacts ( ring - down , blood speckle ) unless gain is decreased , even though there is a risk of attenuating the signal in the target tissues [ 37 ]  . several in vivo studies have shown promising results as to the techniques effective ability to visualise vulnerable plaque and its correlation with acute coronary syndromes [ 4246 ]  . 
in particular , one study extended to the three coronary arteries showed that ivus can identify multiple ulcerated plaque disseminated along the coronary tree independently of the culprit lesion in patients with acute coronary syndrome [ 47 ]  . 
however , differentiation of the lipid core ( area of reduced echogenicity ) from the fibrous tissue is still difficult , as the thickness of the fibrous cap is below the techniques spatial resolution . 
a new ivus - related technology , called virtual histology , has recently been introduced that generates colour maps of plaque composition on the basis of the amplitude and frequency of the echoes [ 4850 ]  . 
though considered the reference standard for plaque evaluation , ivus cannot be routinely used because of its invasiveness , which implies a 1%3% complication rate [ 51 , 52 ] , the cost of materials and the time required for a single procedure . 
in particular , the excessive length of the examination does not allow for a panoramic assessment of all of the coronary arteries , and therefore , the study of plaque is somewhat segmental . 
currently , ivus is considered supplemental though with independent value to angiography , which is particularly useful in ostial or bifurcation stenosis , in the assessment of diffusely atherosclerotic vessels and in the visualisation of eccentric plaques [ 37 ]  . 
ivus has received the approval of the us food and drug administration ( fda )  . elastography elastography is an ivus - related technique that relies on the different mechanical properties of tissues . 
in particular , by applying a known pressure and recording the strain produced , one can define the heterogeneity of the tissue of an atherosclerotic plaque with high reliability [ 53 ]  . 
tuttavia , ancora ardua una differenziazione del core lipidico ( area a ridotta ecogenicit ) dal tessuto fibroso , dal momento che lo spessore del cappuccio fibroso al di sotto della risoluzione spaziale della metodica . 
recentemente stata introdotta una nuova tecnologia ivus - relata , definita istologia virtuale , che , sulla base dellampiezza e della frequenza degli echi , riesce ad elaborare mappe a colori della composizione di placca [ 4850 ]  . 
livus pur essendo considerata lo standard per la valutazione della placca non pu essere utilizzata routinariamente a causa della sua invasivit , che implica un tasso di complicanze dell1%3% [ 51 , 52 ] , dei costi dei materiali e del tempo necessario per una singola procedura . 
allo stato attuale , pur con un valore indipendente , livus considerata supplementare allangiografia , di particolare utilit nello studio delle stenosi ostiali o di biforcazione , nella valutazione dei vasi diffusamente interessati da aterosclerosi , nella visualizzazione delle placche eccentriche [ 37 ]  . livus ha ricevuto lapprovazione da parte della food and drug admistration ( fda )  . elastografia lelastografia una tecnica ivus - relata che sfrutta le diverse propriet meccaniche dei tessuti . 
studi su pazienti con angina stabile , angina instabile e ima hanno evidenziato caratteristiche di deformabilit delle placche significativamente diverse [ 54 ]  . termografia a differenza delle altre metodiche invasive che forniscono una visualizzazione diretta , la termografia ha come obiettivo quello di caratterizzare la placca dal punto di vista metabolico - funzionale . 
in particolare , condizioni di flogosi localizzata , e quindi di incremento della temperatura , si associano ad instabilit della placca : possibile misurare queste variazioni di temperatura con dei sensori applicati a cateteri ( sensibilit termica 0 , 05c , risoluzione spaziale 500 m ) [ 55 , 56 ]  . 
il riscontro di valori di temperatura significativamente diversi in pazienti con infarto miocardico rispetto a pazienti con angina stabile la dimostrazione di placche in differente stato metabolico [ 57 ]  . 
linformazione aggiuntiva sullo stato flogistico della placca risulta di grande importanza se associata ad una metodica visual - based . 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 644 f . 
in particular , local inflammatory states , and consequent rise in temperature , are associated with plaque instability : these temperature variations can be measured by sensors applied to catheters ( thermal sensitivity 0.05c , spatial resolution 500 m ) [ 55 , 56 ]  . 
the finding of significantly different temperature values between patients with myocardial infarction and patients with stable angina is proof that plaque is in a different metabolic state [ 57 ]  . 
additional information on the inflammatory status of plaque is of great value when associated with a visual - based method . angioscopy vascular angioscopy is the only technique allowing direct visualisation of the endothelium and superficial components of atherosclerotic plaque [ 58 ]  . 
in addition , a temporary occlusion of the vessel needs to be induced in order to view the lesion , as the light signal is heavily affected by the presence of blood . 
angioscopy has been approved for clinical use in japan only . optical coherence tomography optical coherence tomography reconstructs images on the basis of the codification of an image reflected in a similar manner to us , with the difference that infrared rays are used instead of us . 
currently , it is the only technique capable of accurately visualising fibrous caps at risk of rupture ( 65 m ) and identifying a complicated lesion [ 62 ]  . 
its major limitation is the complexity of the procedure : a transient ischaemia of approximately 20 s has to be induced , as electromagnetic waves are heavily attenuated by blood . 
another limitation is its poor penetration depth ( 12 mm ) , which does not allow assessment of the entire thickness of the vessel [ 63 ]  . spectroscopy raman spectroscopy is based on the phenomenon described by the indian physicist raman , whereby the inelastic collilangioscopia vascolare lunica tecnica che permette una visione diretta dellendotelio e delle componenti superficiali della placca aterosclerotica [ 58 ]  . 
lutilizzo in ambito clinico approvato solamente in giappone . optical coherence tomography la tomografia a coerenza ottica ricostruisce le immagini a partire dalla codifica di un segnale riflesso in modo analogo allecografia , con la differenza che al posto degli ultrasuoni si utilizzano i raggi infrarossi . 
unaltra limitazione costituita dalla scarsa penetrazione in profondit ( 12 mm ) che non consente una valutazione a tutto spessore del vaso [ 63 ]  . spettroscopia la spettroscopia raman si fonda sul fenomeno , evidenziato dallomonimo fisico indiano , per il quale dalla collisione anelastica tra un fotone ( con compresa tra 750 e 850 nm ) e una molecola scaturiscono emissioni di luce a differente frequenza [ 64 ]  . 
la spettroscopia raman ha indiscutibili potenzialit per lo studio dellaterosclerosi in termini di composizione chimica , ma non fornisce alcuna informazione sulla morfologia delle arterie . la spettroscopia che utilizza i raggi del vicino infrarosso , con compresa fra 750 e 2500 nm , garantisce una profondit di penetrazione fino a 2 mmoreno et al . 
 [ 68 ] hanno dimostrato in vitro la presenza di uno spettro caratteristico per le placche vulnerabili , riportando sensibilit e specificit molto elevate per i componenti lipidici della placca . 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 645 sion of a photon ( with between 750 and 850 nm ) and a molecule generates light emissions with different frequencies [ 64 ]  . 
a catheter ( ~1 mm ) emits a laser beam focused on the tissue under examination , and the reflected beam contains the spectrum of the chemical structures present in the tissue . 
raman spectroscopy has indisputable potential for the study of atherosclerosis in terms of chemical composition but provides no information on arterial morphology . near - infrared spectroscopy , with between 750 and 2500 nm , has a penetration depth up to 2 m moreno et al . demonstrated the presence of a characteristic spectrum for vulnerable plaque in vitro , reporting very high sensitivity and specificity for the lipid plaque components [ 68 ]  . 
the ex vivo analysis conducted on carotid plaque characterised as stable and vulnerable demonstrated significantly different absorption spectra [ 69 ]  . noninvasive modalities magnetic resonance imaging magnetic resonance imaging ( mri ) was the first noninvasive modality whose potential for tissue characterisation was applied to the study of atherosclerotic plaque [ 70 ]  . 
the use of dedicated coils has made it possible to achieve excellent spatial resolution ( 400400 m ) and to assess the fibrous cap in carotid atheromas [ 71 ]  . 
the sequences employed for luminography are threedimensional ( 3d ) turbo field - echo sequences with prospective echocardiogram ( ecg ) triggering and without contrast administration ; the spatial resolution of these sequences is 1.91.21.2 mstudy of the vessel wall involves the use of double inversion recovery ( ir ) black - blood fast spin echo ( fse ) sequences characterised by short radiofrequency pulses and preliminary inversion pulse , which ensure optimal suppression of the endovascular signal and minimise artefacts due to vessel motion [ 72 ]  . 
contrast - enhanced sequences with gadolinium - diethylenetriaminepentaacetic acid ( gd - dtpa ) or ultrasmall superparamagnetic iron oxide ( uspio ) ( selectively taken up by macrophages in inflamed unstable plaque ) have also been tested and shown to improve the sensitivity of the method [ 73 ]  . 
il calcio si presenta marcatamente ipointenso in t1 , dp e t2 . lutilizzo di bobine dedicate ha permesso di raggiungere unottima risoluzione spaziale ( 400400 m ) e di valutare il cappuccio fibroso a livello delle carotidi [ 71 ]  . 
a livello delle coronarie i risultati non sembrano , per ora , altrettanto convincenti perch le coronarie sono vasi di ridotte dimensioni , a decorso tortuoso ed in continuo movimento . 
attualmente per la luminografia sono utilizzate sequenze 3d turbo field - echo con trigger ecg prospettico senza mezzo di contrasto che presentano una risoluzione spaziale di 1 , 9 1 , 2 1 , 2 mlo studio di parete prevede lutilizzo di sequenze a sangue nero ( dual - ir black - blood fse ) , caratterizzate da brevi impulsi di radiofrequenza e preliminare impulso di inversione , che garantiscono unottima soppressione del segnale endovascolare e minimizzano gli artefatti dovuti al movimento dei vasi [ 72 ]  . 
sono state sperimentate anche sequenze con mezzo di contrasto gadolinio - dtpa o uspio ( selettivamente fagocitato dai macrofagi nelle placche infiammate instabili ) , che hanno migliorato la sensibilit della metodica [ 73 ]  . 
unaltra opportunit offerta dalla rm consiste nella soppressione del segnale proveniente dal tessuto adiposo epicardico che permette una migliore visualizzazione della parete vascolare [ 74 ]  . in letteratura sono presenti , ad oggi , poche esperienze che documentano la caratterizzazione della placca aterosclerotica coronarica umana in vivo [ 75 , 76 ]  . 
in particolare lintroduzione di bobine intravascolari ha permesso il miglioramento della risoluzione spaziale fino a 150 m in un campo magnetico di 4 , 7 t , ampliando le possibilit di caratterizzazione tissutale [ 78 , 79 ]  . 
si prospettano tuttavia tempi piuttosto lunghi per una possibile applicazione clinica . medicina nucleare il punto di forza della medicina nucleare consiste nella capacit di evidenziare lattivit metabolica della placca e di fornire informazioni funzionali complementari a quelle delle metodiche radiologiche . 
in particular , the introduction of intravascular coils has improved spatial resolution up to 150 m in a 4.7 - t magnetic field , extending the potential for tissue characterisation [ 78 , 79 ]  . 
it will , however , take years before possible clinical applications begin . nuclear medicine the strength of nuclear medicine is its ability to visualise the metabolic activity of a plaque and provide complementary functional information to that offered by radiological modalities . 
the leading modality in nuclear medicine is currently positron emission tomography ( pet ) , which acquires images with a spatial resolution up to 45 mm , thereby improving on the performance of single photon emission computed tomography ( spect ) , which has a resolution of 1015 mm [ 81 ]  . 
at the level of the carotids , atherosclerotic plaque has been shown to accumulate the radionuclide 18f - fluorodeoxyglucose , which competes with glucose for uptake by metabolically active cells [ 82 ]  . 
major correlations have also been demonstrated with atherosclerotic plaque vulnerability [ 86 , 87 ]  . multislice computed tomography the first applications of ct to the study of the heart date back to the early 1990s . 
these studies used fourth - generation ct , electron beam computed tomography ( ebct ) , at the time the only technology with a temporal resolution capable of acquiring images synchronised with the cardiac cycle . these experiences were aimed at visualising coronary calcium and allowed a direct assessment of the coronary tree [ 88 ]  . the method had high sensitivity [ 89 ] and allowed definition of a calcium - score parameter that could quantify disease severity [ 90 ]  . 
assessment of the patients biochemical parameters and history ( framingham global risk score ) underestimates risk and results in a wide lit strettamente correlata al grado di attivit metabolica della placca [ 80 ]  . 
la metodica di punta della medicina nucleare attualmente la positron emission tomography ( pet ) che ha la capacit di acquisire immagini con risoluzione spaziale fino a 45 mm , migliorando la performance della single photon emission tomography ( spect ) , che ha una risoluzione di 1015 mm [ 81 ]  . 
nelle carotidi , stata documentata la localizzazione del radionuclide 18f - fluorodesossiglucosio , che compete con il glucosio nei processi di uptake da parte di cellule metabolicamente attive , a livello delle placche aterosclerotiche [ 82 ]  . 
per migliorare la performance della tecnica sono stati , di recente , sviluppati scintillatori intravascolari al fine di garantire una pi elevata sensibilit [ 83 ]  . le applicazioni della medicina nucleare si estendono allimaging molecolare e in particolare allo studio della neoangiogenesi . 
sono state dimostrate importanti correlazioni con la vulnerabilit della placca aterosclerotica [ 86 , 87 ]  . tomografia computerizzata multistrato le prime applicazioni della tomografia computerizzata ( tc ) allo studio del cuore risalgono allinizio degli anni 90 . 
questi studi utilizzavano apparecchi tc di iv generazione , il tomografo a fascio di elettroni ( electron beam computed tomography , ebct ) , allora lunica tecnologia con risoluzione temporale in grado di acquisire immagini sincronizzate con il ciclo cardiaco . 
la metodica era caratterizzata da unelevata sensibilit [ 89 ] tanto da consentire la formulazione di un parametro di calciumscore , in grado di quantificare lo stato di malattia [ 90 ]  . attualmente il calcium score sembra avere valore nellinquadramento del rischio cardiovascolare [ 91 ]  . 
il ruolo del calcium score resta ancora discusso e , comunque , la posizione ufficiale dellultimo consensus document non favorevole allutilizzo dellebct a scopo di screening [ 9295 ]  . lebct non tuttavia in grado di visualizzare le altre componenti della placca aterosclerotica . 
parallelamente , la tcms si rivelata affidabile nel rilevare la presenza del calcio e offre inoltre la possibilit di visualizzare lesioni non calcifiche 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 647 proportion of patients with intermediate risk . 
the role of the calcium score is still debated , and the official position of the latest consensus document does not favour the use of ebct as a screening tool [ 9295 ]  . ebct is not , however , able to visualise the other components of atherosclerotic plaque . 
recent technological developments ( 64 - slice ct ) have provided msct with a spatial resolution of 0.30.30.4 mm3 ( isotropic voxel ) associated with a temporal resolution of 165 ms ( with 180 acquisition protocol )  . 
the contrast material has to provide adequate intravascular opacification and must therefore have a high iodine concentration ( 350400 mgi / ml ) and reach the coronary district with a high flow rate ( 45 ml / s ) [ 101 ]  . 
for the best vascular attenuation to be obtained , the beginning of the scan should be synchronised with the arrival of the contrast material by using the bolus tracking technique [ 102 ]  . 
the reconstruction algorithm exploits the possibility of retrospectively synchronising the data with a specific phase of the cardiac cycle expressed as a percentage of the r - r interval or as a distance in milliseconds from the subsequent r wave . 
this type of study cannot be viewed and evaluated on film , as the complexity and tortuousness of the structures being studied is such that the process would require printing out an excessive number of images . the diagnostic performance of msct is considered excellent in the evaluation of coronary stenosis . 
sixteen - slice scanners have a sensitivity between 82% and 95% , a specificity between 93% and 98% and a negative predictive value ( npv ) of 97%99% [ 103105 ]  . 
i recenti avanzamenti tecnologici ( tc a 64 strati ) hanno conferito alla tcms una risoluzione spaziale di 0 , 30 , 30 , 4 mm3 ( voxel isotropico ) associata ad una risoluzione temporale di 165 ms ( con protocollo di acquisizione a 180 )  . il protocollo usato attualmente per la valutazione delle stenosi coronariche prevede lutilizzo dei seguenti parametri : scansione con 120 kv e 800900 mas , ricostruzione dellimmagine con spessore di strato di 0 , 60 , 75 mm e incremento di ricostruzione di 0 , 30 , 4 mm [ 97100 ]  . 
pertanto la concentrazione iodica deve essere elevata ( 350400 mgi / ml ) e arrivare nel distretto coronarico con alta velocit di flusso ( 45 ml / s ) [ 101 ]  . 
lalgoritmo di ricostruzione sfrutta la possibilit di sincronizzare retrospettivamente i dati con una particolare fase del ciclo cardiaco espressa come percentuale dellintervallo r - r oppure come distanza in ms dalla successiva onda r . 
non pensabile osservare e valutare questo tipo di esame su pellicola perch le strutture in studio hanno unanatomia talmente complessa e tortuosa che richiederebbe la stampa di un numero troppo elevato di immagini . la performance diagnostica della tcms considerata eccellente nella valutazione delle stenosi coronariche . 
gli apparecchi a 16 strati mostrano una sensibilit fra l82% e il 95% , una specificit fra il 93% e il 98% e un valore predittivo negativo fra il 97% e il 99% [ 103105 ]  . 
 [ 111 ] hanno mostrato che le caratteristiche ivus delle lesioni correlano con lattenuazione tcms nel 78% delle sezioni contenenti placche ipoecogene ( placche soft ) , nel 78% delle sezioni contenenti placche iperecogene ( placche fibrose ) , nel 95% delle sezioni contenenti placche calcifi03 cademartiri 23 - 07 - 2007 11 : 40 pagina 648 f . 
le corrispondenti immagini assiali mostrano lesioni di diversa densit ( c , d )  . tures correlated with msct attenuation in 78% of sections containing hypoechoic plaque ( soft plaque ) , in 78% of sections containing hyperechoic plaque ( fibrous plaque ) and in 95% of sections containing calcified plaque . 
in 484 of the 525 sections examined ( 92% ) , atherosclerotic lesions were correctly excluded , whereas the remaining 8% were incorrectly classified as containing prevalently noncalcified plaque ( 36 / 41 sections ) , owing to adjacent calcification , stents or image quality . 
reports a sensitivity of 82% ( 41 / 50 segments with plaque ) and a specificity of 88% ( 29 / 33 intact segments ) relative to ivus , although sensitivity is only 53% for noncalcified plaque . 
visualisation of noncalcified plaque is limited by the size of the plaque and vessel , accuracy improving when the analysis is restricted to the proximal segments ( tables 2 and 3 ) [ 112 ]  . 
in 484 delle 525 sezioni esaminate ( 92% ) , le lesioni aterosclerotiche sono state correttamente escluse , mentre il restante 8% , stato erroneamente classificato come contenente placche prevalentemente non calcifiche ( 36 / 41 sezioni ) a causa delle calcificazioni attigue , degli stents e della qualit di immagine . 
 [ 112 ] riporta rispetto allivus una sensibilit dell82% ( 41 / 50 segmenti con placche ) e una specificit dell88% ( 29 / 33 segmenti indenni ) , sebbene per le placche non calcifiche la sensibilit sia solamente del 53% . la visualizzazione delle placche non calcifiche limitata dalle dimensioni della placca e del vaso , con una migliore accuratezza quando si restringe lanalisi ai segmenti prossimali ( tabelle 2 e 3 ) [ 112 ]  . 
al riguardo i dati presenti in letteratura concordano : le placche dei pazienti con evento acuto hanno densit media minore di quella dei pazienti con angina stabile [ 114116 ]  . 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 649 f . 
le immagini assiali mostrano il lume normale a monte della lesione ( d ) , la placca ( e , f ) a livello della biforcazione e dellada prossimale . table 2 in vivo assessment of coronary atherosclerotic plaque : multislice computed tomography ( msct ) vs . 
intravascular ultrasound ( ivus ) study msct scanner sensitivity ( % ) specificity ( % ) noncalcified soft fibrous calcified total schroeder [ 110 ] leber [ 111 ] achenbach [ 112 ] schoenhagen [ 129 ] moselewski [ 128 ] schroeder [ 110 ] leber [ 111 ] achenbach [ 112 ] schoenhagen [ 129 ] moselewski [ 128 ] a30 / 40 plaques visualised on msct ; bextrapolated data ( 299 / 350 plaques correctly classified ) ; c37 / 46 segments examined tabella 2 valutazione delle placche aterosclerotiche coronariche in vivo : confronto tcms vs ivus studio tcms scanner sensibilit ( % ) specificit ( % ) non calcifiche soffici fibrose calcifiche totale a34 / 40 placche visualizzate dalla tcms ; bdati estrapolati ( 299 / 350 placche correttamente classificate ) ; c37 / 46 segmenti esaminati 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 650 f . 
however , the hu score suggested for noncalcified plaque does not take into account the overlap in density values between fibrous and lipid plaque , as shown by ex vivo and in vivo studies , or the misdiagnosis of thrombi , which have a similar attenuation value [ 120 ] ( tables 4 and 5 )  . 
a phantom study has demonstrated that when used at different concentrations ( 1 : 30 , 1 : 40 , 1 : 50 ) , the iodinated contrast material required to produce adequate density gradients between plaque and blood leads to changes in plaque density [ 121 ]  . 
density ranges defined for soft , fibrous and calcified plaque are therefore unlikely to have an absolute value . nel tentativo di perfezionare la tecnica , sono stati pubblicati vari studi ex vivo con il chiaro vantaggio di un modello non in movimento e del confronto istologico [ 117 ]  . 
 [ 118 ] riportano una significativa differenza in densit ( p < 0 , 01 ) tra placche lipidiche ( 479 hu ) e placche fibro - calcifiche ( 10428 hu )  . 
tuttavia lo score in uh suggerito per la placca non calcifica non tiene conto della sovrapposizione dei valori di densit per le placche fibrose e lipidiche , evidenziato dagli studi ex vivo ed in vivo , e della diagnosi non corretta dei trombi che hanno un analogo valore di attenuazione ( tabella 4 e 5 ) [ 120 ]  . 
da uno studio su fantoccio emerge che il mdc iodato , necessario per creare unadeguata differenza di densit tra placche e sangue , determina , utilizzando diverse concentrazioni ( 1 : 30 , 1 : 40 , 1 : 50 ) , una variazione della densit di placca [ 121 ]  . 
non quindi verosimile che gli intervalli di densit definiti per le placche soffici , fibrose e calcifiche abbiano un valore assoluto . discussion discussione diagnosis of a disease entity in the preclinical phase has become possible in several fields of medicine as a result of imla diagnosi di unentit nosologica in fase pre - clinica oggi possibile in svariati campi della medicina , grazie alla miglio03 cademartiri 23 - 07 - 2007 11 : 40 pagina 651 f . 
atherosclerotic disease is characterised by a different and , in many respects , unclear or unexplored natural course : traditionally regarded as a degenerative disease , it is now believed to be closely related to a generalised inflammatory process [ 123 , 124 ]  . the study of vulnerable plaque is still in its very early stages , and no large - scale prospective studies have been carried out . 
one can nonetheless legitimately consider the current role and future prospects of the techniques that are being applied to the characterisation of coronary atherosclerotic plaque and highlight their potential and limitations . ivus is a well - known , well - tested modality for which a consensus document has been produced [ 37 ]  . 
in addition , development and application will probably be limited to a handful of referral centres due to the high professionalism required for operators and the very high cost of materials . the invasiveness and risks associated with these procedures could also hinder large prospective studies from being conducted . application of noninvasive modalities to the study of the coronaries is more recent [ 75 , 126 ]  . 
there is no agreement on the true potential of msct as to size estimation , with some reports stating that volume is underestimated and others that it is overestimated [ 112 , 128 ]  . 
according to recent publications , msct allows the study of positive vascular remodelling , an event that seems to delay the development of stenosis , on one hand , and to be associated with acute coronary syndromes , on the other [ 129131 ]  . 
the search for a protocol optimised for plaque evaluation and the development of software enabling an accurate and reproducible characterisation could represent valid solutions to these problems . no single imaging modality is currently able to detect and characterise vulnerable coronary plaque unequivocally ( table 6 )  . 
technological issues aside , the success of such a complex goal falls into a broader context of clinical imaging , which requires a careful selection of high - risk patients to be studied with such a specific type of examination . 
la malattia aterosclerotica caratterizzata da una storia naturale diversa e per molti aspetti ancora poco chiara o inesplorata : da sempre considerata una malattia degenerativa , oggi ritenuta fortemente correlata con un processo infiammatorio generalizzato [ 123 , 124 ]  . lo studio della placca vulnerabile in una fase preliminare , mancando studi prospettici su un vasto campione . 
si prefigurano possibilit di sviluppo e applicazione in pochi centri specialistici per la grande professionalit richiesta agli operatori e per lelevatissimo costo dei materiali . linvasivit e i rischi connessi a queste procedure potrebbero inoltre ostacolare lesecuzione di ampi studi prospettici . lapplicazione delle metodiche non invasive allo studio delle coronarie pi recente [ 75 , 126 ]  . 
non vi ancora accordo circa le reali potenzialit della tcms nello stimare le dimensioni : per alcuni ricercatori il volume viene sottostimato , mentre per altri viene sovrastimato [ 112 , 128 ]  . 
la tcms secondo alcune recenti pubblicazioni permette lo studio del rimodellamento vascolare positivo , fenomeno che da un lato sembrerebbe ritardare lo sviluppo delle stenosi e dallaltro essere associato a sindromi coronariche acute [ 129131 ]  . 
la ricerca di un protocollo desame ottimizzato per la valutazione della placca e lo sviluppo di un software , che consenta alloperatore unaffidabile e riproducibile caratterizzazione , potrebbero essere valide soluzioni a queste problematiche . attualmente nessuna metodica di imaging capace di identificare e caratterizzare in modo inequivocabile la placca vulnerabile coronarica ( tabella 6 )  . 
al di l dellaspetto tecnologico , la riuscita di un progetto cos complesso si inserisce in un pi vasto contesto di imaging clinico nel quale appare fondamentale la selezione del paziente ad alto rischio da sottoporre ad un tipo di esame talmente specifico . solo questo tipo di confronto potr validare lefficacia di 03 cademartiri 23 - 07 - 2007 11 : 40 pagina 653 f . 
characterisation of an inflammatory state with assessment of inflammatory markers ( c - reactive protein , fibrinogen , interleukin 6 , tumour necrosis factor - ) could help to identify the vulnerable patient . 
imaging techniques , primarily noninvasive and panoramic techniques such as msct , would come into play at a later stage to evaluna tecnica e la sua superiorit sulle concorrenti . in un ipotetico algoritmo diagnostico , la selezione del paziente ad alto rischio ( sintomatico o asintomatico ) costituirebbe , infatti , il punto di partenza . 
la caratterizzazione dello stato infiammatorio con valutazione dei marcatori della flogosi ( proteina c reattiva , fibrinogeno , interleuchina 6 , tnf - ) potrebbe favorire lidentificazione del paziente vulnerabile . 
le tecniche dimaging , primariamente quelle non invasive e panoramiche come la tcms , entrerebbero in scena in un secondo tempo per valutare lo stato di malattia co03 cademartiri 23 - 07 - 2007 11 : 40 pagina 654 f . 
a rteriosa d ieta e stile di v ita terapia tc m ultistrato ( ? ? ) stenosi p lacca culprit m etodiche invasive placca vulnerabile t rattam ento t rattam ento ( ? ) t erapia m edica ottim izzata fig . 
5 algoritmo diagnostico del paziente vulnerabile e possibile ruolo delle metodiche di imaging non invasive tcms . uate the severity of coronary artery disease by quantifying plaque burden without concentrating on the single vulnerable plaque . 
there is a need to reconsider the concept of vulnerable plaque : rather than simply an entity responsible for the acute event , it is the expression of a disease state that involves the entire coronary tree in the clinical setting of a vulnerable patient . 
image - based msct quantification of coronary atherosclerotic disease seems to be an achievable goal , which will require the close collaboration of radiologists and cardiologists in order to optimise the technique and identify its limitations and advantages . conclusioni la ricerca della placca vulnerabile una grande sfida , che presenta notevoli problematiche , in termini di scelta della tecnica ( risoluzione insoddisfacente ) , selezione del paziente ed eventuale trattamento . 
macchi , via borri 57 , i - 21100 varese , italy 2responsabile medico football club internazionale , milano , italy 3clinica ortopedica e traumatologica delluniversit , irccs policlinico s . 
 + 39 - 0332 - 278967 , fax + 39 - 0332 - 278510 , e - mail : eugegeno@tin.it received : 11 november 2006 / accepted : 26 december 2006 / published ondine : 23 july 2007 abstract purpose . 
in all athletes ( nine first - grade lesions , 11 second - grade lesions ) , by using contrast agent intravenous injection done after 20 days , the appearance of contrast spots affecting part or all the lesioned area were observed . 
us with a second - generation contrast agent , thanks to the neoangiogenesis identification , allows recognition , individuation and monitoring the repair processes in the muscle lesion and allows estimation of when athletes can return to competitive activity . 
in tutti gli atleti ( 9 con lesioni primo grado ; 11 di secondo grado ) , dopo iniezione endovenosa di mdc si osservata a 20 giorni la comparsa di spots di contrasto che interessavano tutta o parte dellarea lesionata ; in 8 lesioni di secondo grado permaneva una zona centrale emorragica . 
lecografia con mdc ecografico di ii generazione , attraverso lidentificazione dei vasi neoformati consente di riconoscere , individuare e monitorare i processi riparativi in sede di lesione muscolare e quindi di stabilire i tempi di ripresa dellattivit agonistica dellatleta con ovvia riduzione delle recidive e delle complicanze . parole chiave ecografia mezzo di contrasto di ii generazione atleti professionisti lesioni muscolari introduction introduzione e.a. 
often , us is utilised only to determine the onset of complications , whereas the evaluation of functional recovery has been mainly limited to clinical examinations [ 2 ]  . 
in professional athletes , the appropriate time to return to competitive activity is scheduled to reduce the risk of lesion complications and relapse . the aim of this study was to evaluate the role of second - generation us contrast media ( cm ) in the follow - up of strain injuries in professional athletes , to check muscle repairing processes and to determine when it is appropriate for athletes to return to competitive performance . materials and methods twenty high - performance athletes affected by indirect strains of the medial gastrocnemius ( 3 cases ) , lateral gastrocnemius ( 2 cases ) , soleus ( 2 cases ) , femoral biceps ( 2 cases ) , semimembranous ( 2 cases ) , semitendinous ( 1 case ) , longus adductor ( 2 cases ) and rectus femoral ( 2 cases ) were examined . 
patients were 18 men and two women aged between 18 and 34 ( mean age : 26 years ) ; 11 were football players , seven were practicing athletes and two were volleyball players . 
each patient was studied during the 48 h following the strain with a basal us examination ( esaote technos mpx , esaote biomedica , genoa , italy ) with a high - frequency linear probe ( 413 mhz )  . our study was based on the analysis of nine first - degree and 11 second - degree strains [ 1 ]  . 
follow - up was carried out in three different temporal phases : phase 1 ( 20 days after trauma ) , phase 2 ( 40 days after trauma ) and phase 3 ( 60 days after trauma )  . 
the process consisted of an iv bolus injection of 5 ml of cm ( 8l / ml of sulfur hexafluoride microbubbles ) obtained through the reconstitution of 25 mg of freeze - dried powder with 5 ml of sodium chloride 0.9% weight / volume , followed by a bolus injection of 5 ml of normal saline . 
in all cases , cm was injected in bolus and only images obtained within 2040 s from the start injection of ly images obtained within 2040 s from the start injection of cm were considered in order to identify the arterial phase . we finally evaluated the distribution , site and intensity of the contrast spots . all examinations were evaluated by two operators ( eag , lc ) separately at the same time . 
at the time of each evaluation , a subjective assessment of pain was performed using the visual analogue scale ( vas ) evaluation lecografia nella diagnostica delle lesioni muscolari traumatiche ormai universalmente riconosciuta come metodica di prima istanza [ 18 ] , mentre considerato secondario il suo ruolo nella valutazione dei processi riparativi [ 2 ] ; dalla maggioranza degli autori lecografia stata utilizzata quasi esclusivamente per individuare linsorgenza di complicanze , mentre la valutazione del recupero funzionale stata principalmente delegata al giudizio clinico [ 2 ]  . 
scopo del lavoro quello di studiare le potenzialit del mezzo di contrasto ( mdc ) ultrasonografico di seconda generazione nel follow - up delle lesioni distrattive in atleti professionisti , al fine di monitorare levoluzione dei processi riparativi del muscolo e quindi di individuare i tempi pi opportuni per la ripresa dellattivit agonistica . materiali e metodi sono stati esaminati 20 atleti ad elevata performance con lesioni muscolari distrattive indirette allarto inferiore dei seguenti muscoli : gastrocnemio mediale ( 3 casi ) , gastrocnemio laterale ( 2 casi ) , soleo ( 2 casi ) , bicipite femorale ( 6 casi ) , semimembranoso ( 2 casi ) , semitendinoso ( 1 caso ) , adduttore lungo ( 2 casi ) , retto - femorale ( 2 casi )  . 
rientravano nello studio 18 maschi e 2 femmine di et compresa tra 18 e 34 anni ( et mediana 26 anni ) ; dei quali 11 giocatori di calcio , 7 praticanti atletica leggera , 2 pallavolisti . 
alla diagnosi tutti i pazienti sono stati studiati con ecografia basale entro 48 ore dallevento traumatico mediante apparecchiatura esaote technos mpx ( esaote biomedica , genova , italia ) con sonda lineare ad alta frequenza ( 413 mhz )  . 
 nella serie del nostro studio il grading delle lesioni stato formulato in tutti i casi con il solo esame ecografico basale ed abbiamo considerato 9 lesioni distrattive di primo grado e 11 di secondo grado [ 1 ]  . 
il follow - up stato condotto in 3 diverse fasi temporali rispetto al trauma : fase 1 a 20 giorni , fase 2 a 40 giorni , fase 3 a 60 giorni . 
il controllo comprendeva lo studio in condizioni basali con sonda lineare ad alta frequenza ( 413 mhz ) e dopo iniezione endovenosa ( ev ) di mdc ultrasonografico di seconda generazione ( sonovue , bracco , milano , italia ) con sonda lineare a basso indice meccanico ( 38 mhz ) , previo consenso informato . 
la procedura prevedeva liniezione ev a bolo di 5 ml di dispersione iniettabile di mdc ( 8 l / ml di microbolle di esafluoruro di zolfo ) ottenuta dalla ricostituzione di 25 mg di polvere liofilizzata con 5 ml di cloruro di sodio 0 , 9% peso / volume , seguita dalliniezione a bolo di almeno 5 ml di soluzione fisiologica . 
also in these patients , the vas evaluation ( vas = 0 ) showed the absence of pain , but these athletes were not allowed to resume their competitive activity . discussion muscle - strain lesions are becoming more frequent in sports [ 4 , 9 ] ; in particular , they are highly frequent in professional athletes due to the major work muscles are required to bear [ 5 , 10 ]  . 
us is the main method used to evaluate muscle strains : it is widely employed for diagnosis [ 2 , 4 , 7 , 8 ] but less so during follow - up [ 11 ]  . 
consequently , they also allow neoformed vessels to be located , which indeed are not visible by power - doppler , which can only locate large - diameter vessels [ 12 ]  . 
to better understand the importance of evaluating the microcirculation in the follow - up of muscle lesions , it is necessary to consider the pathological processes taking place after a traumatic event . 
anche in questi casi con il sistema di valutazione ( vas = 0 ) vi era assenza di dolore , ma si ritenuto di non inviare gli atleti alla ripresa dellattivit agonistica . discussione i traumi muscolari sono evenienze sempre pi frequenti nelle attivit sportive [ 4 , 9 ] ; in particolare negli atleti professionisti le lesioni distrattive mostrano elevata incidenza in relazione alla maggiore richiesta funzionale [ 5 , 10 ]  . 
la diagnosi di lesione muscolare prevalentemente clinico - anamnestica ; il ruolo della diagnostica per immagini quello di confermare la sede della lesione e di stabilirne il grading [ 2 ]  . 
lecografia la metodica di prima istanza nella patologia traumatica muscolare , utilizzata ormai di routine in fase diagnostica [ 2 , 4 , 7 , 8 ] e meno frequentemente durante il follow - up [ 11 ]  . 
b same patient : image obtained using a low - mechanical - index probe with contrast - tuned imaging contrast - specific software ( esaote biomedica , genoa , italy )  . 
c dopo iniezione di mdc , omogenea distribuzione degli spots di contrasto nei capillari neoformati ( frecce )  . microbolle contenenti gas che , introdotte per via endovenosa , esaltano gli echi del torrente circolatorio e consentono quindi di individuare le strutture vascolari compresi i vasi di piccolo calibro , fino al letto capillare e perci anche i vasi neoformati non visibili con metodiche power doppler , anche se particolarmente sensibili e di ultima generazione , in grado di evidenziare unicamente vasi di calibro superiore [ 12 ]  . 
per comprendere quanto sia importante riconoscere il microcircolo nel follow - up delle lesioni muscolari necessario fare un cenno ai processi anatomo - patologici che si succedono dopo levento traumatico . 
immediatamente dopo il danno muscolare viene indotto un processo infiammatorio con vasodilatazione ed edema , da alterazione della permeabilit vascolare , associato a sanguinamento pi o meno abbondante a seconda della sede e del grado della lesione . successivamente si assiste ad organizzazione dellematoma con formazione del coagulo che viene progressivamente colonizzato da parte del tessuto di granulazione ( vasi neoformati e cellule ) , e alla riduzione volumetrica della lesione . 
this process is followed by haematoma organisation and subsequent clot , which is progressively invaded by granulation tissue ( neoformed vessels and cells ) , followed by the release of substances from blood cells and the removal of damaged muscle cells . 
2a - i phase 1 : a second - degree femoral biceps lesion : in b - mode , the lesion appears as an inhomogeneous solid area ( empty white arrows )  . 
b same patient : image obtained using a low - mechanical - index probe with contrasttuned imaging ( cnti ) contrast - specific software ( esaote biomedica , genoa , italy )  . 
c after contrast - medium ( cm ) injection , an intense but inhomogeneous enhancement with peripheral spots ( arrows ) can be observed , which defines the residual organised haematoma ( asterisk )  . 
phase 2 : d second - degree femoral biceps lesion : in b - mode , the lesion appears as a solid , inhomogeneous , small - sized area ( empty white arrows )  . 
f after cm injection , an inhomogeneous enhancement with peripheral spots of minor intensity ( arrows ) and without haemorrhagic residues can be observed . phase 3 : g femoral biceps second - degree lesion : in b - mode , the solid , inhomogeneous area is even more reduced and almost not detectable . 
2a - i fase 1 : a lesione di ii grado del bicipite femorale , esame b - mode , area ipoecogena disomogenea in sede di lesione ( frecce bianche vuote )  . 
fase 2 : d lesione di ii grado bicipite femorale , esame b - mode , area solida disomogenea di dimensioni ridotte in sede di lesione ( frecce bianche vuote ) , e stesso paziente , immagine ottenuta con sonda a basso indice meccanico con modulo contrasto ( cnti ) attivato ( esaote biomedica , genova , italia )  . 
c after contrast - medium ( cm ) injection , the fluid collection is inhomogeneously surrounded by contrast spots , which indicate neoformed capillaries ( arrows ) ; in fact an oval area is present , which is not refillable , and is indicative of an organised haematoma ( asterisks )  . 
e same patient : image obtained using a low - mechanical - index probe with contrast - tuned imaging ( cnti ) contrast - specific software ( esaote biomedica , genoa , italy )  . 
f after cm injection , the fluid collection is inhomogeneously surrounded by contrast spots , which indicate neoformed capillaries ( arrows ) ; a residual oval collection is present , which is not refillable and is indicative of an organised haematoma smaller in size ( asterisks )  . 
phase 3 : g medial gastrocnemius second - degree lesion : in b - mode , the fluid collection is almost reabsorbed ; an echoic solid area at the lesion point is still present ( asterisks )  . 
i after cm injection , a rich and inhomogeneous contrast spot distribution can be observed , indicating the presence of neoformed capillaries and that the scar is still not stable . 
3a - i fase 1 : a lesione di ii grado del gastrocnemio mediale , esame b - mode , residua ampia raccolta fluida ( asterischi )  . , b stesso paziente , immagine ottenuta con sonda a basso indice meccanico con modulo contrasto ( cnti ) attivato ( esaote biomedica , genova , italia )  . 
c dopo iniezione di mdc , la raccolta fluida disomogeneamente circondata da spots di contrasto che indicano la presenza di capillari neoformati ( frecce ) , infatti presente area ovalare che non si riempie riferibile a ematoma organizzato ( asterischi )  . 
f dopo iniezione di mdc , la raccolta fluida disomogeneamente circondata da spots di contrasto che indicano la presenza di capillari neoformati ( frecce ) , residua raccolta ovalare che non si riempie riferibile a ematoma organizzato di dimensioni nettamente ridotte ( asterischi )  . 
fase 3 : g lesione di ii grado del gemello mediale , esame b - mode , riassorbita la raccolta fluida , permane area iso / ipoecogena solida in sede di lesione ( asterischi )  . 
i dopo iniezione di mdc , omogenea e ricca distribuzione degli spots di contrasto ( frecce ) che indicano la persistenza di capillari neoformati , segno di mancata stabilizzazione della cicatrice . fico di ii generazione nel follow - up delle lesioni muscolari ha consentito di correlare i reperti ecografici ai quadri anatomo - patologici , attraverso lidentificazione della neo - angiogenesi tipica del tessuto di granulazione ed ha documentato levoluzione dei processi riparativi , attraverso le modie.a. 
in our study , cm allowed us to correlate us findings with pathological patterns and to document the evolution of the repair processes by demonstrating changes in the haemorrhagic area and its progressive replacement by solid granulation tissue , rich in neoformed microvessels . at the first evaluation after 20 days ( phase 1 ) , unenhanced us showed the presence of solid echoic tissue in all patients . the tissue was inhomogeneous in the area of the lesion , with different degrees of reabsorption of the fluid collection described earlier . 
data from the literature suggest that when solid reparative tissue appears in the area of the lesion and replaces the haemorrhagic content , athletes may resume moderate sports activity [ 14 ]  . 
it is actually not possible to evaluate this phase using us only , because it is not easy to detect the muscle tissues initial organisation around the lesion , and us alone does not have the ability to distinguish a clot from granulation tissue [ 14 ]  . 
therefore , it has been reported that the appropriate time for athletes to resume their sports activity should be determined on the basis of the results of the clinical examination or when symptoms disappear . 
in general , a period of 46 weeks should elapse between the trauma and resumption of activity [ 3 ]  . in our study , after 20 days ( phase 1 ) , the use of cm enabled us to differentiate between the peripheral neoangiogenesis , which is the reparative granulation tissue , and the central solid tissue , which is the organised haematoma without neoangiogenesis . 
in some cases , a thin intermediate band with rare contrast spots was detected between vascularised and nonvascularised tissue ; we considered this band as an initial invasion of reparative tissue from the periphery to the organised haematoma . 
at the first examination after 20 days , cm did not change the therapeutic management , even if it allowed detection of angiogenesis , in the granulation tissue , which is indicative of the repair process . 
in fact , different quantities of cm spots in different areas of the lesion were still present , even though most cases showed a reduction of us signal intensity , and the presence of this pattern was considered a contraindication for the athletes to resume competitive activity . 
at this time , the subjective evaluation was not completely negative , and all \athletes referred to moderate discomfort at the lesion site . muscle - lesion recovery coincides with reabsorption of the neoformed capillary vessels . 
indeed , in 17 / 20 patients examined , we observed the progressive reduction of neoformed vessels until total disappearance of vascular spots 60 days after the trauma ( phase 3 ) ; moreover the 3 / 20 patients with residual vascular spots presented a negative clinical outcome ( vas = 0 )  . 
secondo la letteratura la ripresa di una limitata attivit sportiva non sarebbe controindicata nei pazienti in cui larea di lesione sostituita da tessuto riparativo , quindi nei casi in cui non sia ecograficamente pi rilevabile la componente emorragica in sede di lesione [ 14 ]  . 
in realt determinare questa fase con lecografia tradizionale quasi impossibile , risulta particolarmente complicato evidenziare liniziale organizzazione di tessuto muscolare sano ai bordi della lesione , mentre non esiste semeiotica ecografica che consenta di distinguere un coagulo dal tessuto di granulazione [ 14 ]  . 
pertanto , sulla base di tali considerazioni , attualmente gli autori delegano la scelta della ripresa dellattivit sportiva allesame clinico , considerando come fattore positivo la scomparsa della sintomatologia ; pi in generale viene individuato un periodo non minore di 46 settimane dallevento traumatico [ 3 ]  . seguendo il nostro protocollo , nel follow - up a 20 giorni ( fase 1 ) , liniezione ev di mdc ultrasonografico ha permesso di distinguere una componente , solitamente periferica , dotata di importante microvascolarizzazione ( angiogenesi ) corrispondente al tessuto di granulazione di significato riparativo , dalla componente solida , centrale , riferibile a residuo ematoma organizzato ( assenza di angiogenesi )  . 
in alcuni casi si evidenziato inoltre , tra tessuto vascolarizzato e tessuto non vascolarizzato , una sottile fascia intermedia in cui il segnale del mezzo di contrasto appariva sporadico e che abbiamo interpretato quale segno di iniziale colonizzazione del tessuto riparativo dalla periferia verso lematoma organizzato . 
al primo controllo ecografico a 20 giorni , anche lutilizzo di mdc non modifica in modo significativo il comportamento terapeutico pur consentendo di individuare i fenomeni di angiogenesi che caratterizzano il tessuto di granulazione , sempre presente nei processi riparativi . 
il significato prognostico del mdc si appalesa nei controlli a 40 giorni ( fase 2 ) : infatti in tutti i pazienti residuavano spots diffusi o periferici di mdc , seppur nella maggior parte con riduzione dellintensit del segnale ultrasonografico ; tale comportamento contrastografico ha controindicato il ritorno allattivit agonistica . la guarigione di una lesione muscolare coincide con il riassorbimento dei capillari neoformati ; nella nostra serie di pazienti abbiamo assistito alla progressiva riduzione dei vasi neoformati nel tempo fino alla pressoch completa scomparsa degli spots vascolari in 17 / 20 pazienti a 60 giorni dalla lesione ( fase 3 ) , peraltro nei 3 pazienti nei quali erano presenti residui spots vascolari la clinica era negativa . 
alla luce di quanto osservato possiamo considerare il mdc ecografico un valido indicatore della attivit tissutale con ovvia ricaduta clinica ; infatti in presenza di residua vascolarizzazione dellarea di lesione da parte di capillari neoformati , sconsigliabile la ripresa dellattivit agonistica , poich il processo di guarigione non si pu ritenere completamente concluso . nel follow - up con ecografia senza mdc delle lesioni muscolari il riempimento da parte di tessuto solido , disomogee.a. 
in highdegree lesions or in those not correctly treated , however , the process can turn into scar tissue , whose entity is proportional to the initial seriousness of the lesion [ 1 , 5 ] , to the length of recovery and to the precociousness of the resumption of sports activity . 
in these situations , the us pattern indicates complete repair of muscle injury , and it could indicate that athletes can resume sports activity . nevertheless , in contrast - enhanced examinations carried out in patients who were diagnosed with complete lesion repair by unenhanced us examinations , we still observed the presence of many small neoformed vessels , which clearly indicated the presence of active reparative tissue . 
il processo riparativo ecogeno nelle lesioni meno estese pu completarsi con la restitutio ad integrum del muscolo lesionato o pu , soprattutto nelle lesioni di grado elevato o non adeguatamente trattate , trasformarsi in tessuto fibrocicatriziale la cui entit proporzionale alla gravit della lesione iniziale [ 1 , 5 ] , alla lunghezza del processo di guarigione , e alla precocit del ritorno allattivit sportiva . 
 in entrambe le situazioni tale pattern ecografico espressione della avvenuta riparazione del danno muscolare e indicherebbe la possibilit di ritorno alla attivit sportiva . tuttavia anche nei casi di avvenuta riparazione ecografica della lesione si osservato durante lindagine con mdc tessuto ricco di piccoli vasi neoformati che indicavano inequivocabilmente la presenza di tessuto riparativo in fase di attivit ; noi riteniamo quindi che la presenza di angiogenesi , seppur residua , sia espressione di una lesione riparata , ma non stabile . 
facilmente intuibile perci come , soprattutto negli atleti i cui muscoli sono sottoposti ad un significativo sovraccarico funzionale , tale rilievo rivesta notevole importanza prognostica , in quanto un muscolo ancora sede di fenomeni riparativi , se sottoposto a carichi massimali , presenta un elevato rischio di recidiva di lesione . 
we believe that this method , especially when used for professional athletes , is the only one that can provide the physician with the correct information regarding lesion staging in order to determine with greater accuracy the appropriate time for functional recovery of sports activity to reduce relapses and complications . in conclusione , possiamo affermare che il mdc ecografico di ii generazione consente di riconoscere i processi di angiogenesi tipici di tutti i processi riparativi , tale caratteristica pu e deve essere sfruttata per ottenere informazioni fino ad oggi non cos dettagliate sulla evoluzione dei processi riparativi ed il grado di guarigione del muscolo lesionato . 
forty - one patients ( mean age 30 years ) affected by chondral defects of the knee ( 27 patients ) and ankle joint ( 14 patients ) who underwent arthroscopic autologous osteochondral grafting were studied 6 months and 1 year postoperatively with mri . 
cartilage repair after chondrocyte implantation was studied by assessing the degree of defect filling , graft integration , graft signal intensity , integrity of the subchondral lamina and trabecular oedema underneath the gramr findings were correlated with clinical data . 
postoperative mri evaluation at 6 months demonstrated complete filling of the osteochondral defect in 12 / 41 cases , complete integration in 18 / 41 , mild hyperintensity in 28 / 41 , intact subchondral lamina in 38 / 41 and trabecular oedema in 11 / 41 . postoperative mri evaluation at 1 year demonstrated complete filling of the osteochondral defect in 9 / 41 patients , complete integration in 22 / 41 , mild hyperintensity in 23 / 41 , intact subchondral lamina in 36 / 41 and trabecular oedema in 8 / 41 . 
sono state esaminate con rm a sei mesi ed un anno dallintervento , 41 lesioni cartilaginee del ginocchio ( 27 ) e tibio - tarsiche ( 14 ) , trattate per via artroscopica con impianto di condrociti autologhi su supporto tridimensionale di acido ialuronico . 
levoluzione dellimpianto stata studiata analizzando il grado di colmatura del difetto osteocondrale , il grado di integrazione , lintensit di segnale della cartilagine trapiantata , lintegrit della lamina corticale subcondrale e ledema trabecolare . 
a sei mesi : completo grado di colmatura in 12 / 41 pazienti , integrazione completa dellimpianto in 18 / 41 , modesta iperintensit del segnale in 28 / 41 , lamina subcondrale intatta in 38 / 41 , edema trabecolare in 11 / 41 . 
ad un anno : completo grado di colmatura in 9 / 41 pazienti , integrazione completa dellimpianto in 22 / 41 , modesta iperintensit del segnale in 23 / 41 , lamina subcondrale intatta in 36 / 41 , edema trabecolare in 8 / 41 . 
la valutazione rm presenta elementi prognostici in termini di buon attecchimento dellimpianto . parole chiave risonanza magnetica trapianto di condrociti lesioni cartilaginee introduction introduzione articular cartilage injuries are one of the most common injuries seen in orthopaedic practice [ 1 ]  . 
treatment of such injuries is difficult , as articular cartilage has a limited capacity le lesioni della cartilagine articolare sono le lesioni di pi frequente riscontro in ortopedia [ 1 ]  . 
the most frequently used surgical procedures aim to promote the growth of repair tissue at the level of the chondral defect by means of chondroplasty or chondroabrasion , associated , if necessary , with subchondral perforation or microfracture [ 3 ]  . 
fibrocartilaginous repair tissue has different biochemical and bioelastic properties from that of hyaline cartilage , and the result achieved with these techniques is merely to delay the onset of degenerative osteoarthritis [ 4 ]  . autologous chondrocyte implantation ( aci ) is the first technique that aims to restore the articular surface with hyaline - like cartilage . 
the original technique involved applying to the injury cultures of autologous chondrocytes arthroscopically harvested from non - weight - bearing articular areas ; adhesion to the defect is ensured by a periosteal flap also harvested from the patient [ 5 ]  . 
among the various biomaterials , two are the most commonly used : hyalograft c , which employs hyaluronic - acid scaffolds , and maci ( matrix - induced aci ) , which employs type 1 and type 3 collagen scaffolds [ 8 ]  . 
follow - up after aci can be performed by using several diagnostic procedures , such as clinical assessment , direct visualisation of the graft with arthroscopy with the possibility of obtaining biopsies or indirect visualisation with magnetic resonance imaging ( mri ) [ 9 ]  . 
all subjects were treated with aci with a 3d hyaluronic - acid scaffold ( hyalograft c , fidia advanced biopolymers srl , abano terme , italy ) and underwent clinical assessment by an orthopaedic surgeon and mri evaluation by a musculoskeletal radiologist . the mri studies were performed at 6 and 12 months postoperatively using a 1.5 - tesla ( t ) unit ( symphony , siemens , erlangen , germany ) and the following sequences : sagittal t1 spin echo ( tr : 463 ms ; te : 17 ms ; flip angle : 150 ; fov : 180 ms ; matrix : 240320 ; slice thickness : 4 mm ; number of acquisitions : 2 ) ; sagittal dual fast spin echo ( fse ) ( tr : 600 ms ; te : 18 ms ; flip angle : 20 ; fov : 150 ms ; matrix : 192256 ; slice thickness : 4 mm ; number of acquisitions : 2 ) and coronal and sagittal flash t1 fat - sat ( tr : 500 ms ; te : 8 ms ; flip angle : 65 ; fov : 200 ms ; matrix : 256256 ; slice thickness : 4 mm ; number of acquisitions : 2 )  . each mri study was assessed for : the degree of filling of the osteochondral defect ; the degree of graft integration ; signal intensity ; the integrity of the subchondral lamina ; and trabecular oedema . 
i trattamenti chirurgici pi utilizzati mirano alla crescita di tessuto riparativo a livello del difetto condrale mediante tecniche di condroplastica / condroabrasione , associate o meno a perforazioni subcondrali o microfratture [ 3 ]  . 
il tessuto fibro - cartilagineo di riparazione presenta caratteristiche biochimiche e bioelastiche differenti dalla cartilagine ialina ed il risultato che si riesce ad ottenere con queste metodiche soltanto un ritardo nel progressivo sviluppo del processo artrosico [ 4 ]  . limpianto di condrociti autologhi ( aci ) rappresenta la prima tecnica che si propone di ripristinare la superficie articolare con tessuto cartilagineo di tipo ialino . 
la tecnica originale prevede di applicare sulla lesione colture di condrociti autologhi prelevati per via artroscopica da zone articolari non soggette a carico ; ladesione alla zona innestata viene assicurata da un lembo periostale prelevato dal paziente [ 5 ]  . 
tra i vari biomateriali due sono quelli pi utilizzati : hyalograft c e maci ( matrix - induced autologous chondrocytes implantation ) , nel primo caso i supporti sono costituiti da acido ialuronico ( hyalograft c ) , nel secondo da collagene di tipo i e iii ( maci ) [ 8 ]  . 
il follow - up dei trapianti di condrociti autologhi pu essere effettuato mediante diversi procedimenti diagnostici , quali la valutazione clinica , la visualizzazione diretta dellarea sottoposta a trapianto mediante artroscopia , con possibilit di effettuare biopsie , o la visualizzazione indiretta mediante risonanza magnetica ( rm ) [ 9 ]  . scopo del lavoro quello di valutare , mediante rm , levoluzione dellimpianto di condrociti autologhi su supporto tridimensionale di acido ialuronico e correlare tale evoluzione con landamento clinico . materiali e metodi dal 2002 al 2005 sono stati esaminati , consecutivamente , 41 pazienti ( 30 maschi e 11 femmine ) di et compresa fra i 17 anni ed i 50 anni ( et media 35 , 2 anni , range 1750 ) ; di questi , 27 erano affetti da una lesione a carico della cartilagine dellarticolazione del ginocchio , tutte interessanti il compartimento femoro - tibiale , e 14 da una lesione a carico della cartilagine dellarticolazione tibio - tarsica . 
graft integration was considered complete when the graft showed continuity with the adjacent native cartilage and incomplete when a linear fissure - like lesion or a larger defect could be seen . 
signal intensity of the graft was considered isointense if the graft had the same signal intensity as the adjacent cartilage and hyperintense or hypointense if its signal intensity was higher or lower . 
 each variable was given a score : degree of filling ( score from 0 to 1 : 0 = complete , 1 = incomplete ) , graft integration ( score from 0 to 1 : 0 = complete , 1 = incomplete ) , signal intensity ( score from 0 to 3 : 0 = isointense , 1 = moderately hyperintense , 2 = markedly hyperintense , 3 = hypointense ) , subchondral lamina ( score from 0 to 1 : 0 = intact , 1 = not intact ) and oedema ( score from 0 to 1 : 0 = absent , 1 = present )  . 
the best score , indicative of optimal graft quality according to the literature [ 9 ] is 0 , whereas the worst score is 7 ( 0 = excellent integration , 12 = good integration , 35 = fair integration , 67 = poor integration )  . 
of the 14 patients with injuries of the ankle - joint cartilage , 5 / 14 ( 35.7% ) had excellent results , 7 / 14 ( 50% ) had good results and only 2 / 14 ( 14.3% ) had fair results . 
il grado di colmatura stato valuto in base allo spessore del tessuto trapiantato : stato considerato completo quando la cartilagine trapiantata aveva lo stesso spessore della cartilagine nativa , incompleto quando il tessuto trapiantato era pi sottile rispetto a quello della cartilagine nativa , mentre stato definito ipertrofico quando lo spessore dellimpianto era superiore rispetto a quello della cartilagine nativa . 
lintegrazione stata considerata completa quando limpianto non presentava soluzioni di continuo con la cartilagine adiacente , incompleta quando era visibile o una lesione lineare simile a una fessura oppure un difetto pi ampio . 
per quanto riguarda lintensit del segnale , limpianto stato considerato isointenso se appariva della stessa intensit della cartilagine adiacente , iperintenso o ipointenso se presentava , rispettivamente , unintensit maggiore o minore rispetto alla cartilagine nativa . 
infine stata valutata la presenza o lassenza di edema a livello dellosso subcondrale adiacente alla cartilagine trapiantata . ad ogni parametro esaminato stato assegnato un punteggio predefinito : grado di colmatura ( score da 0 a 1 : 0 = colmatura completa , 1 = colmatura incompleta ) , grado di integrazione ( score da 0 a 1 : 0 = integrazione completa , 1 = integrazione incompleta ) , intensit ( score da 0 a 3 : 0 = isointensit , 1 = moderata iperintensit , 2 = marcata iperintensit , 3 = ipointensit ) , integrit della lamina ( score da 0 a 1 : 0 = lamina intatta , 1 = lamina non intatta ) , edema ( score da 0 a 1 : 0 = assenza di edema , 1 = presenza di edema )  . 
grado di colmatura completo ( a ) : lo spessore dellinnesto uguale allo spessore della cartilagine nativa ; grado di colmatura incompleto ( b ) : lo spessore dellinnesto inferiore allo spessore della cartilagine adiacente . table 1 osteochondral defect filling and graft integration at 6 and 12 months after autologous chondrocyte implantation defect filling complete incomplete hypertrophic graft integration complete incomplete 6 months 12 months 6 mesi 12 mesi tabella 1 grado di colmatura e grado di integrazione a 6 mesi ed a 12 mesi dopo trapianto di condrociti autologhi grado di colmatura completo incompleto ipertrofico grado di integrazione completo incompleto one - year follow - up defect filling was complete in 9 / 41 patients ( 21.9% ) , incomplete in 30 / 41 ( 73.2% ) and hypertrophic in 2 / 41 ( 4.9% ) ( table 1 )  . 
la cartilagine trapiantata risultata essere isointensa in 3 / 41 pazienti ( 7 , 3% ) , moderatamente iperintensa in 28 / 41 pazienti ( 68 , 3% ) , marcatamente iperintensa in 7 / 41 pazienti ( 17 , 1% ) , ipointensa in 3 / 41 pazienti ( 7 , 3% )  . 
una sua lesione espressione di un esito sfavorevole del trapianto . table 2 subchondral lamina at 6 and 12 months after autologous chondrocyte implantation subchondral lamina intact not intact 6 months 12 months 6 mesi 12 mesi tabella 2 caratteristiche della lamina subcondrale a 6 mesi ed a 12 mesi dopo trapianto di condrociti autologhi lamina subcondrale intatta non intatta follow - up a 1 anno tients ( 63% ) with injuries of the knee cartilage had a total score between 95 and 100 on the tegner and lysholm activity scale , 8 / 27 ( 29.6% ) had scores between 84 and 94 and 2 / 27 ( 7.4% ) had scores below 84 . 
of the 14 patients with injuries to ankle - joint cartilage , 10 / 14 ( 71.4% ) had excellent results , 3 / 14 ( 21.4% ) had good results and only 1 / 14 ( 7.2% ) had fair results . 
 the number of patients with poor clinical functional outcome at 1 year was 14 / 41 ( 34.1% ) , eight of whom belonged to the group with knee - cartilage defects and six to the group with ankle cartilage defects . 
graft integration was incomplete in 10 / 14 ( 71.4% ) and complete in tilagine dellarticolazione di ginocchio 8 / 27 pazienti ( 29 , 6% ) hanno ottenuto un punteggio totale tra 95100 ( funzionalit normale ) del protocollo di tegner lysholm , 15 / 27 pazienti ( 55 , 6% ) un punteggio tra 84 e 94 ( sintomatologia solo nelle attivit pesanti ) ed infine 4 / 27 ( 14 , 8% ) un punteggio sotto gli 84 punti ( sintomi nella quotidianit )  . 
dei 14 pazienti con lesioni della cartilagine dellarticolazione tibiotarsica , 5 / 14 ( 35 , 7% ) hanno ottenuto una valutazione eccellente , 7 / 14 ( 50% ) una valutazione buona e solo 2 / 14 ( 14 , 3% ) una valutazione sufficiente . il grado di colmatura risultato completo in 9 / 41 pazienti ( 21 , 9% ) , incompleto in 30 / 41 pazienti ( 73 , 2% ) , ipertrofico in 2 / 41 pazienti ( 4 , 9% ) ( tabella 1 )  . 
il grado di integrazione risultato completo in 22 / 41 pazienti ( 53 , 7% ) , incompleto in 19 / 41 pazienti ( 46 , 3% ) ( tabella 1 )  . 
la lamina subcondrale risultata intatta in 36 / 41 pazienti ( 87 , 8% ) , non intatta in 5 / 41 pazienti ( 12 , 2% ) ( tabella 2 )  . 
la cartilagine trapiantata risultata essere isointensa in 8 / 41 pazienti ( 19 , 5% ) , moderatamente iperintensa in 23 / 41 pazienti ( 56 , 1% ) , marcatamente iperintensa in 7 / 41 pazienti ( 17 , 1% ) , ipointensa in 3 / 41 pazienti ( 7 , 3% )  . 
dei 14 pazienti con lesioni della cartilagine dellarticolazione tibio - tarsica , 10 / 14 ( 71 , 4% ) hanno ottenuto una valutazione eccellente , 3 / 14 ( 21 , 4% ) una valutazione buona e solo 1 / 14 ( 7 , 2% ) una valutazione sufficiente . i casi ad andamento clinico - funzionale peggiore a distanza di 1 anno sono risultati 14 / 41 ( 34 , 1% ) , di cui 8 casi appartenevano al gruppo con lesioni a carico dellarticolazione del ginocchio e 6 al gruppo con lesioni a carico dellarticolazione tibio - tarsica ; in questi il grado di colmatura risultato incompleto in 12 / 14 casi ( 86% ) , completo in 2 / 14 ( 14% ) ; lintegrazione risultata incompleta in 10 / 14 ( 71 , 4% ) , completa in 4 / 14 ( 28 , 6% ) ; limpianto risultato iperintenso in 10 / 14 ( 71 , 4% ) , isointenso in 1 / 14 ( 7 , 2% ) , ipointenso in 3 / 14 ( 21 , 4% ) ; la lamina subcondrale risultata non intatta in 9 / 14 casi ( 64 , 3% ) , intatta in 5 / 14 ( 35 , 7% ) ; ledema subcondrale risultato assente in 10 / 14 ( 71 , 4% ) , presente in 4 / 14 ( 28 , 6% )  . la rm utilizzata di routine nello studio delle lesioni della cartilagine articolare , sia in fase di diagnosi , sia per il successivo monitoraggio delle lesioni dopo il trattamento chirurgico ; in particolare la rm indicata nel valutare se la cartilagine trapiantata presenti caratteristiche del tutto sovrapponibili alla normale cartilagine articolare di tipo ialino [ 1215 ]  . nello studio della cartilagine articolare si utilizzano sequenze specifiche , che determinano un adeguato contrasto tra la cartilagine e le strutture adiacenti . 
le sequenze pi frequentemente utilizzate nel follow - up dei trapianti di condrociti autologhi sono rappresentate da sequenze fast spin echo t2 - dipendenti ( fse ) e sequenze gradient echo ( gre ) con soppressione del grasso e ricostruzioni in tre dimensioni [ 1620 ]  . 
le sequenze t2 - dipendenti , invece , determinano un basso segnale della cartilagine articolare contrapposto ad un alto segnale del liquido sinoviale , e permettono unaccurata valutazione della struttura della cartilagine articolare , sia essa normale o danneggiata [ 16 , 19 , 21 , 22 ]  . 
inoltre le sequenze fse t2 - dipendenti non sono alterate da eventuali artefatti magnetici , che si possono creare in pazienti sottoposti precedentemente ad interventi chirurgici a livello dellarticolazione in esame . con il miglioramento delle tecniche di imaging si sono potuti definire i parametri da analizzare per ogni esame espletato , in modo tale che la valutazione del tessuto di riparazione sia la pi oggettiva possibile . 
6 clinical outcome at 6 and 12 months after autologous chondrocyte implantation in the group with lesions of the ankle joint evaluated by the american orthopaedic food and ankle society scale ( aofas )  . 
6 andamento clinico a 6 mesi e a 12 mesi dei trapianti di condrociti autologhi nel sottogruppo con lesioni a carico dellarticolazione tibio - tarsica valutato secondo il protocollo aofas . articular cartilage is evaluated by using specific sequences that produce adequate contrast between the cartilage and the surrounding structures . 
the most frequently used in the follow - up of aci are t2 - weighted fse and gradient echo ( gre ) sequences with fat suppression and 3d reconstructions [ 1620 ]  . 
gre sequences are characterised by a relatively high signal intensity of cartilage in contrast with a low signal intensity of the surrounding tissues ; 3d gre sequences enable precise determination of cartilage thickness and surface . t2 - weighted sequences , on the other hand , generate a low signal intensity of articular cartilage in contrast to a high signal intensity of synovial fluid and allow accurate evaluation of the structure of both healthy of damaged articular cartilage [ 16 , 19 , 21 , 22 ]  . 
 improvements in imaging techniques have made it possible to establish which parameters should be assessed in each examination so as to make evaluation of repair tissue as obpianto ed infine lo stato della lamina e dellosso subcondrale [ 23 ]  . 
il trapianto si considera infatti riuscito qualora il tessuto appaia dello stesso spessore della cartilagine adiacente e la superficie sia liscia [ 16 ] , i margini non mostrino soluzioni di continuo con la cartilagine nativa , losso subcondrale a livello dellarea sottoposta a trapianto sia anchesso liscio , il midollo osseo abbia la stessa intensit di segnale del normale midollo osseo e il tessuto trapiantato risulti isointenso rispetto alla cartilagine non sottoposta a trapianto [ 16 , 17 ]  . lassegnazione di un punteggio prestabilito ad ogni parametro analizzato rappresenta un ulteriore criterio di oggettivit nella valutazione della riuscita del trapianto di condrociti autologhi . 
scale di valutazione simili sono gi proposte in alcuni lavori presenti in letteratura , come il lavoro di handerson del 2003 o nel lavoro , ancora pi recente di tratting del 2005 [ 9 , 24 ]  . nel nostro studio si sono voluti correlare i parametri rm accettati in letteratura [ 22 , 24 ] come indicativi di attecchif . 
mr images allow an accurate assessment of graft thickness , graft integration with the native cartilage , graft signal intensity and the state of the subchondral lamina and bone [ 23 ]  . 
graft implantation is considered successful when the repair tissue has the same thickness as the adjacent cartilage and has a smooth surface [ 16 ] , the edges of the graft are in continuity with the native cartilage , the subchondral bone beneath the graft is also smooth , bone marrow has the same signal intensity as normal marrow and the graft appears isointense relative to the native cartilage [ 16 , 17 ]  . use of a preestablished scoring system in the analysis of each parameter makes assessing the success of an aci procedure more objective . 
in 2005 [ 9 , 24 ]  . in our study , we attempted to correlate the established mri parameters [ 22 , 24 ] for assessment of successful graft incorporation with the clinical data to evaluate whether there is a true clinical - mri correlation and to identify the most significant parameters for the follow - up . 
defect filling and graft integration are the two parameters that reflect repair tissue growth at the defect site and its good incorporation ; if incomplete , they indicate poor graft outcome , which translates into worse clinical outcomes . 
this is confirmed by three patients in our study ( table 1 ) who had a good clinical outcome at 6 months but a worsening of symptoms at 12 months , at which time mri showed incomplete defect filling or , in one case , graft hypertrophy . 
a similar situation occurred in trattnig et al.s study [ 24 ] : in two out of 20 cases , the degree of osteochrondral defect filling worsened , and this was considered a poor prognostic sign . 
a change was seen in this parameter at 12 months with respect to the previous mri study ( table 2 ) : the subchondral lamina was not intact in five cases as against the three cases seen at 6 months . 
however , moderate signal hyperintensity in the early postoperative period does not preclude the possibility that the signal will return to normal , as was seen in five cases in our series . subchondral bone oedema was absent in 71.4% of cases with poor clinical - functional outcome . 
as has been previmento ben riuscito con i dati clinici , per valutare se esista realmente una correlazione clinico - rm e per identificare i parametri pi significativi nel follow - up . 
il grado di colmatura e il grado di integrazione sono due parametri che riflettono la crescita del tessuto di riparazione nel sito di impianto ed il suo buon attecchimento ; quando risultano essere incompleti , sono indicativi di un esito sfavorevole del trapianto che si traduce in un peggiore andamento clinico . 
a conferma di ci 3 casi del nostro studio ( tabella 1 ) , caratterizzati da buon andamento clinico ai controlli a 6 mesi , hanno invece presentato ai controlli a 12 mesi un peggioramento della sintomatologia e allesame rm si riscontrato un grado di colmatura incompleto o in un caso ipertrofia della cartilagine trapiantata . 
 [ 24 ] presente una situazione analoga : in 2 casi su 20 esaminati si riscontrato un peggioramento nel grado di colmatura del difetto osteocondrale ; tale peggioramento stato considerato un segno prognostico negativo per la riuscita del trapianto . 
nello stesso studio , in 3 pazienti si assistito ad un miglioramento del grado di integrazione da incompleto a completo con conseguente buona riuscita del trapianto effettuato . nel 64 , 3% dei casi ad andamento clinico - funzionale peggiore la lamina subcondrale risultata non intatta . 
la lamina subcondrale di norma non viene intaccata durante gli interventi di impianti di condrociti autologhi e quindi dovrebbe apparire intatta allo studio rm , come risultato nella maggior parte dei casi nel nostro studio . 
si assistito , inoltre , ad una modificazione di tale parametro nei controlli a 12 mesi rispetto ai controlli precedenti ( tabella 2 ) : in 5 casi , infatti , la lamina subcondrale risultata non intatta contro i 3 casi rilevati ai controlli a 6 mesi . 
quindi anche tale parametro pu eventualmente essere espressione di un esito sfavorevole del trapianto . nel 71 , 4% dei casi ad andamento clinico - funzionale peggiore la cartilagine trapiantata risultata essere iperintensa rispetto alla cartilagine nativa . 
a nostro avviso lintensit del segnale manifestazione del grado di maturit del tessuto trapiantato , in particolare se messo in relazione con la cartilagine adiacente , rispetto alla quale dovrebbe risultare isointensa . 
tuttavia una moderata iperintensit di segnale nelle fasi iniziali dopo lintervento non preclude una normalizzazione del segnale , come si potuto constatare in 5 casi della nostra casistica . ledema a livello dellosso subcondrale , infine , risultato assente nel 71 , 4% dei casi di questo studio ad andamento clinico - funzionale peggiore . 
come gi descritto in letteratura [ 12 , 23 ] , la presenza di edema anchessa la manifestazione del normale processo di maturazione della cartilagine sottoposta a trapianto , sinonimo del rimodellamento e f . 
this would appear to be confirmed by the five patients ( table 3 ) who had no oedema and a positive clinical evaluation at 6 months but had subchondral oedema and a clinical evaluation that was either negative ( three cases ) or positive ( two cases ) for vigourous activities only at 12 months . 
il rilievo sembrerebbe dimostrato dai cinque casi ( tabella 3 ) che a 6 mesi erano caratterizzati da assenza di edema e concomitante clinica positiva , mentre ai controlli a 12 mesi si presentavano con edema a livello dellosso subcondrale e clinica negativa in 3 casi o positiva solo per le attivit pi pesanti nei rimanenti 2 casi . 
lassenza di edema quindi indice di una carenza nel processo di maturazione , che determina un peggior andamento clinico . conclusions mri proved to be fundamental in the follow - up of aci procedures , as it enables accurate and noninvasive evaluation of the state of the cartilage grathe parameters degree of defect filling , degree of graft integration and graft signal intensity allow the repair tissue maturation process to be monitored until it displays the typical characteristics of hyalinelike articular cartilage . 
detection of the findings absence of oedema and nonintact subchondral lamina during the early follow - up period has a negative prognostic value . conclusioni la rm si dimostrata fondamentale nel follow - up dei trapianti di condrociti autologhi , in quanto consente unaccurata e non invasiva valutazione dello stato della cartilagine trapiantata . 
i parametri grado di colmatura e di integrazione ed intensit della cartilagine trapiantata permettono di monitorare il processo di maturazione del tessuto trapiantato , fino allacquisizione da parte di questultimo delle caratteristiche definitive tipiche della cartilagine articolare di tipo ialino . 
sorrentino , via san lorenzo 291 / a , i - 90146 palermo , italy , tel . : + 39 - 91 - 6552335 , fax : + 39 - 91 - 6552337 , e - mail : drdiving@yahoo.it received : 19 september 2006 / accepted : 24 november 2006 / published online : 23 july 2007 abstract purpose . 
hrus is a fairly reliable technique in the detection , characterisation and differentiation of the different forms of meniscal cyst . key words meniscal cyst high - resolution ultrasonography knee meniscus riassunto obiettivo . 
lhrus una metodica abbastanza affidabile nellidentificazione , nella valutazione delle caratteristiche semeiologiche e nella distinzione delle differenti forme delle cisti meniscali . parole chiave cisti meniscale ecografia ad elevata risoluzione ginocchio menisco introduction introduzione meniscal cysts are relatively uncommon lesions that are often clinically unrecognised . 
they have a reported incidence ranging from 1%2% to 7%8% in the different arthroscopic and le cisti meniscali sono una patologia abbastanza infrequente , spesso clinicamente misconosciuta , con unincidenza variabile tra l1%2% ed il 7%8% secondo diverse casistiche f . 
in most cases , they are accompanied by mucoid degeneration and horizontal cleavage tear , with infiltration of synovial fluid into the capsular - meniscal complex [ 1 ]  . 
meniscal cysts may manifest either as palpable masses of the knee joint or else be diagnosed at imaging , especially with magnetic resonance imaging ( mri ) performed to assess injuries to meniscal and ligamentous structures . 
within the field of knee - joint imaging , high - resolution ultrasound ( hrus ) is considered the modality of choice for the evaluation of extraarticular disorders on account of its high diagnostic accuracy [ 24 ]  . 
in the study of intra - articular lesions , including meniscal and cruciate ligament alterations , however , the results of us are conflicting because of methodological and anatomotopographic difficulties that make its clinical use controversial and often limited [ 3 , 5 , 6 ]  . 
the aim of this study was to assess the ability of hrus to detect parameniscal cysts and compare the mri and hrus appearance of the various types of meniscal cyst . materials and methods over a 2 - year period , 1 , 857 patients ( 989 men ; mean age 43 years ) underwent mri for either traumatic or degenerative knee disorders . 
mri was performed using a 0.5 - tesla ( t ) superconductive magnet ( vectra , ge medical systems , milwaukee , wi , usa ) with a limb - dedicated transmit / receive coil . 
spin - echo ( se ) t1 ( tr 500 ms , te 20 ms ) and gradientecho ( ge ) t2 * ( tr 320 ms , te 20 ms , flip angle 30 ) sequences were obtained in the sagittal , coronal and axial planes with 3 - mm slice thickness and 1 - mm interval . 
the acquisition matrix was 192256 , reconstruction 256256 and field of view ( fov ) ranging from 15 cm to 20 cmri were jointly evaluated by two radiologists ( fs , an )  . 
all hrus exams were performed by a single radiologist ( ai ) blinded to the mri results , with au5 ( esaote biomedica , genoa , italy ) and hdi 5000 ( atl , bothell , wa , usa ) devices , using high - resolution linear multifrequency transducers ( 712 mhz )  . 
the exam was performed with the patient in the supine position with 3040 knee flexion for identification of the anterior horn of the meniscus and in the prone position with the knee extended knee to examine the posterior horn . 
the scans obtained corresponded to precise anatomical landmarks , taking into account the spatial orientation of the structures to be examined . in order to avoid obliquity artefacts , scans were performed parallel to the femur long axis and absolutely perpendicular to the base of the meniscus . 
nella maggior parte dei casi , si accompagnano a degenerazione mucoide e fissurazione orizzontale del menisco , con infiltrazione di liquido sinoviale sino alla connessione menisco - capsulare [ 1 ]  . 
le cisti meniscali possono manifestarsi o come masse palpabili in relazione con larticolazione del ginocchio o possono venire diagnosticate allimaging , prevalentemente con risonanza magnetica ( rm ) , eseguita nello studio della patologia traumatica delle strutture meniscali e legamentose . 
nellambito della diagnostica per immagini dellarticolazione del ginocchio , lecografia ad elevata risoluzione ( hrus ) viene odiernamente considerata metodica di prima istanza nella valutazione delle affezioni extrarticolari , grazie allelevata accuratezza diagnostica dimostrata [ 24 ]  . 
nello studio della patologia intrarticolare , che include le alterazioni dei menischi e dei legamenti crociati , lecografia , in relazione alle relative difficolt di approccio metodologico e anatomo - topografico , che ne rendono controversa e spesso limitata la sua utilizzazione clinica , mostra spesso risultati molto contrastanti [ 3 , 5 , 6 ]  . 
la rm , di contro , presenta elevata accuratezza diagnostica , con valori del 90%95% nella diagnosi di lesione meniscale e del 95%100% in quella dei legamenti crociati [ 7 , 8 ]  . 
inoltre stata effettuata una comparazione tra laspetto rm di varie tipologie di cisti meniscali con quello hrus . materiali e metodi in un periodo di 2 anni , sono stati sottoposti ad rm del ginocchio per patologia traumatica o degenerativa 1857 pazienti ( 989 uomini ; et media 43 anni )  . 
le indagini rm sono state eseguite utilizzando ununit a magnete superconduttivo da 0 , 5 t ( vectra , ge medical systems , milwaukee , usa ) impiegando una bobina trasmittente / ricevente dedicata per estremit . 
sono state utilizzate sequenze spin - echo ( se ) t1 ( tr = 500 ms ; te = 20 ms ) e gradient - echo ( ge ) t2 * ( tr = 320 ms ; te = 20 ms ; angolo di ribaltamento = 30 ) secondo i piani di scansione sagittale , coronale ed assiale , con spessore di strato di 3 mm ed intervallo di 1 msono state utilizzate una matrice di acquisizione di 192256 e una di ricostruzione di 256256 , con un campo di vista ( fov ) variabile da 15 a 20 cle immagini rm sono state valutate in consenso da due autori ( fs , an )  . 
lo studio hrus stato eseguito in cieco dal medesimo radiologo ( a.i. ) , non a conoscenza della presenza di una cisti parameniscale , con apparecchiature au5 ( esaote biomedica , genova , italia ) e hdi 5000 ( atl , bothell , wa , usa ) utilizzando sonde lineari multifrequenza ( 712 mhz ) ad elevata f . 
in the control group , an equivalent number of patients was recruited , and four patients with cyst - like formations diagnosed as synovial ganglia at mri were purposely included . under normal conditions , hrus allows identification of the meniscal fibrocartilage , which appears as a homogeneously hyperechoic triangle , with the base towards the surface and the apex along the intra - articular direction . 
in two cases , the cyst was wrongly characterised as a synovial ganglion because of its large size ( mean diameter 4.3 cm ) , which did not allow us to appreciate the continuity between the meniscal alteration and the cyst - like formation . 
in none of the cases examined did mri or hrus depict erosions of the surrounding bone structures . surgery and histology confirmed the diagnosis established with mri , which considered to be the gold standard . discussion meniscal cysts are a generally uncommon finding first described by nicase in 1883 and later by ebner in 1904 [ 10 ]  . meniscal cysts are prevalently detected in 20to 40 - year - old men and more frequently in the lateral than medial meniscus , risoluzione . 
lesame stato condotto con paziente in posizione supina , con ginocchio in flessione di circa 3040 , per lidentificazione del corno meniscale anteriore ed in posizione prona con ginocchio esteso , per la valutazione del corno posteriore . 
al fine di evitare artefatti da obliquit sono state effettuate scansioni parallele allasse maggiore del femore e perfettamente perpendicolari alla base del menisco visualizzato . lapplicazione di un leggero stress in valgismo ha facilitato la visualizzazione del corno anteriore della fibrocartilagine meniscale mediale , mentre un leggero stress in varismo ha consentito la visualizzazione del corno anteriore controlaterale . 
i criteri utilizzati per la diagnosi di cisti meniscale sono stati : ( 1 ) identificazione di formazione con caratteristiche semeiologiche ecografiche fluide o miste tipo complex - mass ; ( 2 ) dimostrazione dellesistenza di un rapporto di continuit tra la formazione cistica , larticolazione e la relativa fibrocartilagine meniscale ; ( 3 ) alterazione meniscale lineare in continuit con la formazione cistica . 
tutti i pazienti sono stati sottoposti ad intervento chirurgico e le formazioni resecate sono state sottoposte ad esame istologico . risultati in 52 pazienti lindagine rm ha consentito lidentificazione di una cisti parameniscale . 
in due casi perch erroneamente caratterizzate come ganglio sinoviale a causa delle ampie dimensioni ( diametro medio 4 , 3 cm ) della formazione che non consentivano di apprezzare la continuit tra lalterazione meniscale e la formazione con aspetto cistico , e nellultimo caso , la cisti parameniscale non stata correttamente identificata perch di piccole dimensioni e localizzata in sede profonda posteromediale . 
nel gruppo controllo lhrus ha escluso in tutti i casi la presenza di una cisti meniscale e ha consentito la corretta identificazione e caratterizzazione dei 4 casi con ganglio cistico , le cui dimensioni erano comprese tra 2 cm e 3 clhrus ha manifestato nella detezione delle cisti parameniscali una sensibilit del 94 , 23% , una specificit del f . 
this triangle is separate from the femoral and tibial cortical border represented by a hyperechoic layer and from the hyaline cartilage , which appears as a thin , homogeneous hypoechoic band . 
questo triangolo separato dal profilo corticale osseo femorale e tibiale rappresentato da una stria regolare iper - riflettente , dalla cartilagine ialina di rivestimento articolare , che appare come una sottile banda ipoecogena . 
nella sede anatomica meniscale , si evidenzia una formazione simil - cistica che presenta morfologia a cuori di carta da gioco , a margini netti con tramite fistoloso intra - meniscale . 
ampia formazione simil - cistica ( diametro 4 , 5 cm ) con componente corpuscolata , a margini netti , con tramite fistoloso intra - meniscale sul versante interno distale . 
lintervento chirurgico e listologia hanno confermato la diagnosi rm considerata nel nostro studio come gold standard . discussione le cisti meniscali , in genere , non sono di frequente riscontro e furono descritte per la prima volta da nicase nel 1883 e successivamente da ebner nel 1904 [ 10 ]  . 
le cisti meniscali si evidenziano nella maggior parte dei casi in uomini tra i 20 e i 40 anni , con prevalente coinvolgimento del menisco laterale rispetto al mediale , con rapporto variabile tra 3 : 1 e 7 : 1 [ 1 ] ; esistono , tuttavia , alcuni studi che riportano differenti rapporti di incidenza , con uguale incidenza in entrambi i menischi o con prevalente coinvolgimento del menisco mediale [ 11 ]  . 
la tesi pi accreditata quella microtraumatica iterativa che in associazione alla critica vascolarizzazione del menisco inducono processi degenerativi rappresentati da fenomeni di vacuolizzazione , colliquazione e trasformazione mucoide che partendo dal centro della fibrocartilagine meniscale si portano verso la superficie in direzione capsulare . 
la cisti parameniscale la forma pi frequentemente riscontrata [ 1 , 10 ] ed rappresentata da una raccolta fluido - sinoviale che , tramite la lesione meniscale , si fa strada attraverso i tessuti circostanti [ 1 ]  . 
la sua estrinsecazione pu avvenire : anteriormente , a livello del cuscinetto adiposo sottopatellare , lateralmente , in prossimit del legamento collaterale , posteriormente , tra questo ed il tendine popliteo e medialmente , nel cavo popliteo od in prossimit della zampa doca . 
la diagnosi ecografica di cisti parameniscale si basa sulla identificazione della raccolta fluida contraente stretti rapporti di continuit con la cavit articolare ed , in particolare , con la corrispondente fibrocartilagine meniscale da cui si origina . 
nel presente studio lhrus ha consentito nel 94 , 23% dei casi la corretta identificazione delle cisti parameniscali e le limitazioni sono derivate dalle ampie dimensioni e dalla localizzazione posteriore - profonda . 
come evidenziato nella nostra casistica lecostruttura delle cisti molto variabile e dipende dalla viscosit del fluido sinoviale e dal tempo di comparsa ; leventuale presenza di detriti o di formazioni ecogene nel suo contesto sono in genere messe in relazioni a microframmenti derivanti dal menisco degenerato . 
this leakage may be directed either anteriorly towards the subpatellar fat pad , laterally near the collateral ligament , posteriorly between the collateral ligament and the popliteal tendon or medially within the popliteal fossa or near the anserine bursa . 
meniscal cyst size varies considerably and may also be very large , as seen in our series , with the formation of a pseudocapsule and in some cases internal septation . 
us diagnosis of a parameniscal cyst is based on identification of a fluid collection in close continuity with the articular cavity and , in particular , with the corresponding meniscal fibrocartilage from f . 
as seen in our series , cyst echostructure varies widely and depends on synovial fluid viscosity and the time of appearance ; the possible presence of debris or echogenic masses within the cyst are generally related to microfragments from the degenerated meniscus . 
on the basis of their experience with 13 patients , seymour and lloyd reported that the echostructural variability does not allow adequate diagnostic accuracy and creates problems in the differential diagnosis with other lesions such as cystic ganglia or soft tissue tumours [ 14 ]  . 
in contrast , in our experience , echostructure did not have a negative effect on diagnostic accuracy , and differentiation between parameniscal cysts and cystic ganglia was influenced by the size of the cysts which , when larger than 4 cm , prevented identification of the connection with the meniscus . 
it has been reported that very large cysts are associated with erosion of the cortical bone profile [ 10 , 15 , 16 ] , although this was never detected in our series . 
longitudinal scans were best for visualising the entire meniscal cyst and detecting the connection with the adjacent meniscal fibrocartilage , whereas axial scans proved useful for assessing extension of the lesion . conclusions hrus proved to be a reliable technique in the presumptive diagnosis of meniscal cysts , as it allowed both identification and characterisation of their imaging features . 
hrus does not usually play a role in the diagnostic workup of meniscal lesions , which is carried out by ct and especially mri , two techniques that allow correct identification of the lesion and precise definition of its size . it should nonetheless be emphasised that during an examination to assess superficial tendon and / or ligament structures , hrus can potentially allow the incidental discovery of a meniscal cyst , leading to a presumptive diagnosis useful in the clinical assessment of patients . dellaspetto ecostrutturale non consenta una adeguata accuratezza diagnostica , con problemi di diagnosi differenziale con altre entit patologiche come i gangli cistici o i tumori dei tessuti molli [ 14 ]  . 
nella nostra esperienza , lecostruttura non ha influenzato negativamente laffidabilit diagnostica della metodica e la diagnosi differenziale tra cisti parameniscali e gangli cistici stata inficiata dalle dimensioni , superiori ai 4 cm , che non consentono lidentificazione del tramite con il menisco . 
in presenza di cisti di cospicue dimensioni , stata segnalata la presenza di erosione del profilo corticale osseo [ 10 , 15 , 16 ] , che , tuttavia , nella nostra casistica , non mai stata rilevata . 
le scansioni longitudinali si sono dimostrate le pi idonee ad evidenziare le cisti meniscali in tutto il loro decorso , con dimostrazione del tramite con ladiacente fibrocartilagine meniscale , mentre le scansioni assiali sono servite a verificare lesatta estensione della lesione . conclusioni lhrus si dimostrata una metodica affidabile nella diagnosi presuntiva delle cisti meniscali consentendone sia lidentificazione che la valutazione delle caratteristiche semeiologiche . 
nella nostra esperienza , anche se limitata , la hrus ha mostrato una elevata accuratezza diagnostica possedendo una sensibilit del 94 , 23% , una specificit del 100% , un valore predittivo positivo del 100% e un valore predittivo negativo del 94 , 54% . 
nel corretto iter diagnostico della patologia meniscale del ginocchio la hrus abitualmente non svolge un ruolo , che deve essere assolto dalla tc ed in particolare dalla rm , metodiche che consentono la corretta identificazione della patologia ed un preciso bilancio di estensione . 
all rotational studies were conducted by selective cannulation of the vessel supplying the lesion ( internal carotid artery or vertebral artery ) with a single injection of 20 cc of contrast agent after diagnostic angiography in anterior - posterior ( ap ) and laterolateral ( ll ) views . 
three - dimensional ra enabled accurate definition of site , orientation , morphology and size of the sac and its relationship with the parent arteries and helped us choose the most appropriate angulation of the c - arm for guiding and controlling the embolisation procedure . 
based on our experience before ra equipment became available and in agreement with the literature , we believe that 3dra improves the identification of all lesions and helps refine the choice of the most suitable embolisation material and technique . 
lo studio rotazionale stato sempre eseguito mediante cateterizzazione selettiva del vaso afferente ( carotide interna o arteria vertebrale ) con singola iniezione di 20 cc di mdc dopo angiografia diagnostica nelle due proiezioni ortogonali . 
mediante la 3dra in ogni caso stato possibile definire in maniera accurata la sede , lorientamento , la morfologia e le dimensioni della sacca , il rapporto con i vasi parenti e la scelta dellidonea angolazione dellarco a c ai fini della guida e del controllo dellembolizzazione . 
in base alla nostra esperienza precedente alla disponibilit di un angiografo rotazionale , e in accordo con i dati della letteratura , riteniamo che la 3dra consenta di individuare con maggiore accuratezza tutte le lesioni e di scegliere con maggiore precisione il materiale pi idoneo per la procedura , la tecnica di embolizzazione , nonch di ridurre sensibilmente il numero di proiezioni e quindi la dose di esposizione e di mdc al paziente , con una verosimile riduzione dei tempi di trattamento , dei rischi e delle complicanze . key words cerebral angiography intracranial aneurysm embolization , therapeutic imaging , three - dimensional parole chiave angiografia cerebrale aneurismi intracranici embolizzazione terapeutica imaging tridimensionale a . 
subarachnoid haemorrhage ( sah ) due to aneurysm rupture has an incidence of 1025 / 100 , 000 / year and is a devastating event associated with high morbidity and mortality from rebleeding and vasospasm [ 1 ]  . management of intracranial aneurysms has been facilitated by constant improvements in diagnostic and therapeutic procedures , which have recently led to an increased use of noninvasive imaging [ computed tomography ( ct ) angiography and magnetic resonance ( mr ) angiography ] and percutaneous endovascular treatment rather than conventional surgery [ 2 , 3 ]  . 
the technique and outcome of cerebral embolisation procedures are closely dependent on an accurate preliminary assessment of the morphology and size of the aneurysmal sac and of its relationship with parent vessels . the aim of this study was to assess the systematic use of 3d rotational angiography ( 3dra ) in the diagnosis and preoperative evaluation of cerebral aneurysms with a view to planning endovascular treatment . la prevalenza degli aneurismi cerebrali nella popolazione generale stimata tra 0 , 2% e 6 , 8% . 
lemorragia subaracnoidea ( esa ) da rottura di aneurisma , con unincidenza di 1025 / 100000 / anno , rappresenta un evento devastante con elevata morbilit e mortalit legate soprattutto al risanguinamento e al vasospasmo [ 1 ]  . la gestione dellaneurisma intracranico oggi favorita da un evidente e progressivo miglioramento delle procedure diagnostiche e terapeutiche che nellultimo decennio hanno permesso un crescente orientamento verso limaging non invasivo ( angio - tc e angio - rm ) e il trattamento endovascolare percutaneo rispetto alla chirurgia tradizionale [ 2 , 3 ]  . 
la tecnica di embolizzazione cerebrale e il suo esito sono strettamente dipendenti da una preliminare accurata valutazione morfo - dimensionale della sacca aneurismatica e dei suoi rapporti con i vasi parenti . lobiettivo del presente lavoro quello di valutare lutilit dellimpiego sistematico dellangiografia rotazionale 3d ( 3dra ) nella diagnostica preliminare al trattamento endovascolare degli aneurismi cerebrali , ai fini della pianificazione della procedura . materials and methods thirty - five consecutive aneurysms in 32 patients [ 20 females and 12 males ; age range 3 months ( one case ) to 85 years ; mean age 49.3 years ] were studied and treated using 3dra ( philips allura xper fd 20 single - plane ra system with a flat - panel detector ) between march 2005 and march 2006 . 
fifteen of the aneurysms were treated after sah , whereas 20 had been discovered incidentally at mr performed for different diagnostic indications , or identified as the cause of cranial nerve deficits or embolic ischaemic events . 
the aneurysms were located at the anterior communicating artery or between segments a1 and a2 of the anterior cerebral artery ( seven cases ) , at the origin of the posterior communicating artery ( six cases ) , at the origin of the anterior choroidal artery ( two cases ) , in the ophthalmic segment of the internal carotid artery ( six cases ) , at the internal carotid bifurcation ( three cases ) , at the basilar artery apex ( five cases ) , in the cavernous segment of the internal carotid ( two cases ) and at the bifurcation of the middle cerebral artery ( four cases )  . 
 rotational angiography was performed in all cases via transfemoral access and selective catheterisation of the feeding vessel ( internal carotid or vertebral artery ) with a single injection of 1520 cc nonionic iodinated contrast material at a flow rate of 34 ml / s and 240 rotation of the c - arm with the propeller technique . 
in all cases , the rotational phase was preceded by a preliminary diagnostic 2d acquisition in two orthogonal views [ anterior - posterior ( ap ) and materiali e metodi sono stati studiati e trattati consecutivamente 35 aneurismi con luso di 3dra ( angiografo rotazionale monoplano philips allura xper fd 20 con flat - detector ) in 32 pazienti tra marzo 2005 e marzo 2006 . 
di questi , 15 sono stati trattati dopo esa , mentre 20 aneurismi costituivano reperto occasionale in pazienti sottoposti a rm cerebrale per diversi quesiti diagnostici o rappresentavano la causa di deficit di nervi cranici o eventi ischemici su base embolica . 
la sede degli aneurismi era rispettivamente a livello dellarteria comunicante anteriore o tra i segmenti a1 e a2 dellarteria cerebrale anteriore ( 7 casi ) , allorigine dellarteria comunicante posteriore ( 6 casi ) , allorigine dellarteria corioidea anteriore ( 2 casi ) , nel tratto oftalmico della carotide interna ( 6 casi ) , alla biforcazione di carotide interna ( 3 casi ) , sullapice di basilare ( 5 casi ) , nel tratto cavernoso della carotide interna ( 2 casi ) e alla biforcazione di arteria cerebrale media ( 4 casi )  . lo studio angiografico rotazionale stato sempre eseguito tramite accesso transfemorale e mediante cateterizzazione selettiva del vaso afferente alla lesione ( carotide interna o arteria vertebrale ) con singola iniezione di 1520 cc di mdc iodato non ionico , flusso a 34 ml / s e rotazione dellarco di 240 in modalit propeller . 
all diagnostic examinations were performed with the patient under general anaesthesia , as they formed part of the following interventional procedure and as this ensured total immobility , which is crucial for high diagnostic quality , accuracy and reliability of the examination . 
la fase rotazionale in tutti i casi stata preceduta da una preliminare fase diagnostica 2d nelle due proiezioni ortogonali ( ap e ll ) utilizzata anche per la valutazione panoramica del circolo endocranico . 
in tutti i casi lesame stato eseguito in anestesia generale in quanto parte integrante della successiva fase terapeutica e per le condizioni di assoluta immobilit del paziente , imprescindibili ai fini di una elevata qualit diagnostica e quindi accuratezza e affidabilit dellesame . 
immediatamente al termine dellacquisizione rotazionale , dopo ricezione automatica della serie angiografica non sottratta attraverso una connessione di rete , il software dellapparecchiatura ( workstation integris 3d - ra ) in pochi secondi ha prodotto automaticamente il modello volumetrico in 3d con matrice di 5123 sul quale sono state poi scelte ricostruzioni in volume rendering ( vr ) , gradient rendering ( gr ) , shaded surface ( ss ) o maximum intensity projection ( mip ) a seconda delle informazioni che necessitava il singolo caso . 
1a - d a 3 - month - old child with a giant aneuryson 2d angiograms , it is difficult to determine the precise site of origin of the lesion ( a )  . 
three - dimensional gradient rendering ( b ) and volume rendering ( c ) reconstructions allow accurate localisation of the origin between the right a1 segment and the anterior communicating artery , which appears to be a plexiform variant ( arrow )  . the relationship of the lesion with the adjacent vessels is also clear . 
le ricostruzioni 3d in gr ( b ) e vr ( c ) permettono di localizzare con accuratezza lorigine della lesione situata tra a1 di destra e larteria comunicante anteriore che appare di tipo plessiforme ( freccia )  . 
2a - d two - dimensional angiography ( a ) in a patient with an aneurysm of the anterior communicating artery ( black arrow ) and ophthalmic internal carotid artery ( ica ) ( white arrow ) treated after subarachnoid haemorrhage probably due to the first aneurysthe volume rendering 3d images ( b , c ) clearly show the morphology and orientation of the lesions . 
2a - d angiografia 2d ( a ) in paziente con aneurisma di arteria comunicante anteriore ( freccia nera ) e di ci oftalmica ( freccia bianca ) dopo esa verosimilmente dal primo . 
questultima valutazione stata resa possibile grazie allautomatica rappresentazione dei gradi di angolazione in senso cranio - caudale e laterale del tubo a c riportati nello spazio in alto a sinistra sullimmagine 3d ( visibile nelle figure ) dopo scelta da parte delloperatore delladeguata proiezione di lavoro sul modello stesso . 
a aneurisma di ci oftalmica ; b , c aneurisma allorigine della comunicante posteriore sui quali sono misurati i diametri della sacca e del colletto . la selettiva opacizzazione del vaso arterioso afferente alla lesione senza sovrapposizione di vasi venosi e il celere e non sempre necessario lavoro di post - processing manuale per la sottrazione delle strutture ossee del cranio hanno permesso in ogni caso di ottenere un rapido e accurato imaging volumetrico in tempi stimati mediamente intorno ai 5 minuti . 
sulla console sono state quindi eseguite misurazioni e valutazioni necessarie ai fini della procedura endovascolare in tempi variabili a seconda della complessit dei singoli casi , ma non superiori ai 57 minuti . tra le possibili modalit di ricostruzione 3d sono state utili la vr e la gr per rispondere a tutti i quesiti richiesti dalla successiva fase di embolizzazione . 
non si sono mai verificate complicanze maggiori , mentre per quanto riguarda le complicanze minori ( 1 caso di embolia temporale periferica risolto con fibrinolisi loco - regionale , 2 casi di trombosi precoce della lesione con evidenza di parziale ricanalizzazione nei successivi controlli di follow - up e 1 caso in cui si verificato un lieve bulging di spirali attraverso il colletto aneurismatico ) , tali eventi non erano conseguenti a mancata accuratezza della diagnostica preliminare . among the possible 3d reconstructions , vr and gr were most helpful in providing all the information required for the subsequent embolisation procedure . 
by further modifying the model projection ( c ) , one can clearly distinguish the course and origin of the posterior communicating artery ( arrowhead ) in relation to the aneurysm ( arrow )  . 
vr reconstruction ( d ) shows a wide - necked aneurysm ( arrow ) of the posterior communicating artery ( arrowhead ) ; another projection ( e ) enables identification of a pouch ( arrow ) on the sac and the origin of the communicating artery ( arrowhead ) from the sac itself . 
4a - h alcuni casi in cui le immagini 3d permettono di definire con accuratezza morfologie complesse di sacche aneurismatiche e di stabilire i rapporti della lesione con i vasi parenti . 
modificando ulteriormente la proiezione del modello ( c ) possibile distinguere chiaramente il decorso e lorigine della comunicante posteriore ( punta di freccia ) in rapporto allaneurisma ( freccia )  . 
in d la ricostruzione in vr mostra un aneurisma ( freccia ) di comunicante posteriore ( punta di freccia ) con ampio colletto ; con unaltra proiezione del modello ( e ) possibile individuare una tasca accessoria ( freccia ) sulla sacca e lorigine dellarteria comunicante ( punta di freccia ) dalla sacca stessa . 
i gradi di angolazione del tubo a c forniti nellimmagine in alto a sinistra , dopo aver scelto la proiezione di lavoro per lembolizzazione sul modello volumetrico , permettono di orientare il tubo nella medesima proiezione per guidare la procedura su entrambe le lesioni ( freccia ) ( b ) e controllare il risultato finale che appare ottimale ( freccia ) ( c )  . discussione langiografia a sottrazione digitale rappresenta ancora oggi lesame gold standard per lidentificazione e laccurata valutazione degli aneurismi intracranici . 
limaging non invasivo , e in special modo langio - tc , con il miglioramento delle apparecchiature e dei software di ricostruzione bie tridimensionale , trova sempre maggior applicazione nelliter diagnostico di questa patologia anche ai fini della valutazione per la scelta terapeutica di tipo chirurgico o endovascolare [ 4 ]  . tuttavia , grazie allimpiego selettivo del mezzo di contrasto , alla panoramicit e alla risoluzione spaziale dellesame angiografico , il corretto e affidabile studio dellaneurisma ancora appannaggio di questa metodica , soprattutto nella valutazione preliminare alla procedura di embolizzazione endovascolare e ai fini della sua pianificazione [ 5 ]  . i limiti della metodica angiografica 2d tradizionale nella valutazione pre - interventistica sono rappresentati in molti casi dalla necessit di numerose proiezioni con relative multiple iniezioni di mdc trans - catetere ed esposizioni a serie radiografiche per una corretta definizione morfologica della lesione vascolare , del colletto aneurismatico e dei suoi rapporti con i vasi endocranici . 
non raramente le multiple proiezioni non permettono comunque una esaustiva descrizione di tali dati per sovrapposizioni strutturali non dissociabili a causa dellanatomia vascolare o dei limiti di escursione del tubo a c . 
langiografia tradizionale inoltre non consente misurazioni quantitative dimensionali della sacca , del colletto e dei vasi parenti , estremamente utili soprattutto per la scelta del tipo e delle dimensioni delle spirali metalliche da utilizzare . discussion digital subtraction angiography remains the gold standard examination for the detection and evaluation of intracranial aneurysms . 
noninvasive imaging , in particular ct angiography , with the improvements in hardware and software for 2d and 3d image reconstruction , is progressively gaining ground in the diagnostic workup of cerebral aneurysms and a view to guiding decisions concerning surgical or endovascular management [ 4 ]  . 
however , thanks to the selective use of contrast material , the panoramic view and the spatial resolution afforded by angiography , angiography is still relied upon to provide an accurate and reliable study of the aneurysm , above all for preoperative evaluation before endovascular embolisation and for procedure planning [ 5 ]  . the limitations of conventional 2d angiography in procedure planning are the frequent need to obtain multiple projections with repeated injections of contrast material and increased radiation dose to the patient in order to obtain correct morphological depiction of the aneurysm , aneurysa . 
sulla proiezione laterale ( b ) si osserva unicamente una irregolarit marginale di dubbia interpretazione che si proietta sul profilo superiore del segmento cavernoso della carotide interna ( nel cerchio )  . 
la ricostruzione 3d in vr ( c ) grazie alla sua multiproiettivit identifica un piccolo aneurisma del medesimo segmento della carotide interna e ne mostra chiaramente la morfologia senza necessit di ricorrere a ulteriori iniezioni di mdc e proiezioni angiografiche . mal neck and relationships with intracranial vessels . 
in many cases , these multiple acquisitions fail to provide a comprehensive depiction due to the superimposition of structures that cannot be discerned because of vascular anatomy or limited excursion of the c - armoreover , conventional angiography does not allow quantitative determinations of the size of the sac , neck or parent vessels , which are especially helpful in selecting the type and size of coils to be used for embolisation . in our experience , albeit in a small number of patients , these limitations were always fully overcome by the use of rotational sequences with 3d reconstructions . 
this result was related to the high spatial resolution and selective use of contrast material of angiography compared to the noninvasive modalities , and to the multiple views afforded by the 3d model , which , unlike conventional angiography , allowed complete discrimination of superimposed vascular structures and thus the confident identification and interpretation of aneurysms . similar findings were also reported by other authors [ 610 ] , who confirmed the diagnostics achieved by ra thanks to the major technological developments introduced since its first applications in the 1970s [ 11 , 12 ]  . 
in agreement with these authors , we found that crucial factors in planning the endovascular procedure and ensuring an optimal outcome were the ability to measure the aneurysm quantitatively for selection of the first coil and to determine carm angulation for the appropriate working projection . 
questo dato stato correlato allelevata risoluzione spaziale e allimpiego selettivo del mezzo di contrasto dellesame angiografico rispetto alle metodiche non invasive , e sostanzialmente alla multiproiettivit del modello volumetrico che , rispetto allangiografia tradizionale stessa , ha permesso la completa dissociazione delle strutture vascolari sovrapposte e quindi la sicura interpretazione e lidentificazione degli aneurismi . 
 tali constatazioni sono riportate anche nelle casistiche di altri autori [ 610 ] , i quali confermano la validit diagnostica dellangiografia rotazionale dopo limportante sviluppo consentito dallevoluzione tecnologica dai tempi delle sue prime applicazioni negli anni 70 [ 11 , 12 ]  . 
ai fini della pianificazione del trattamento endovascolare e dellottimale risultato terapeutico , come per gli autori suddetti , risultata fondamentale la possibilit della misurazione quantitativa dellaneurisma per la scelta della prima spirale da rilasciare nella sacca e quella di stabilire langolazione del tubo a c per lidonea proiezione di lavoro . 
7a , b angiographic volume rendering 3d standard reconstruction ( a ) showing an aneurysm of the anterior communicating artery with its neck larger than the sac and the a2 segments of the anterior cerebral arteries originating from the neck itself . 
7a , b ricostruzione angiografica 3d standard in vr ( a ) che mostra un aneurisma di comunicante anteriore con colletto pi ampio della sacca e dal quale emergono i tratti a2 delle cerebrali anteriori . 
 with regard to analysis of results obtained with 3dra , and in partial agreement with recently published analyses [ 1315 ] , there was no case of significant overor undersizing of the aneurysm due to intrinsic limitations of the 3d reconstruction software . 
in our series , this finding was always confirmed when the first coil was positioned , as in all cases its size corresponded with the measurements made on the 3d model by the postprocessing software . 
in some cases ( 5 / 35 ) , the 3d reconstruction software produced artefactual images of the course or emergence of vessels relative to the aneurysm sac , consisting mostly of marginal fusion between single adjacent structures . 
these artefacts have been described for the various digital acquisition and 3d reconstruction modalities and are chiefly related to the spatial resolution of the single machines and degree of geometric distortion intrinsic to the acquisition modality [ 16 , 17 ]  . 
questo dato trova peraltro parziale conferma nei lavori suddetti e la sua verifica , nei nostri casi , stata ottenuta sempre dopo il posizionamento della prima spirale , le cui dimensioni hanno corrisposto in ogni singolo caso alle misure elaborate tramite il software di post - processing sul modello 3d dellaneurisma . 
in alcuni casi ( 5 / 35 ) la ricostruzione 3d ha prodotto immagini artefattuali di decorso o emergenza di vasi in rapporto con la sacca aneurismatica rappresentate prevalentemente da fusione marginale tra singole strutture adiacenti . 
tali artefatti sono descritti nelle varie modalit di acquisizione digitale e ricostruzione 3d e legati principalmente alla risoluzione spaziale delle singole apparecchiature e al grado di distorsione geometrica intrinseca alla modalit di acquisizione [ 16 , 17 ]  . 
in such conditions , an additional 2d angiographic acquisition after selective contrast injection and in the most appropriate projection , as determined on the 3d model , may be useful to provide superimposable images , allowing accurate comparison and diagnostic supplementation . finally , in agreement with other authors [ 18 ] , we believe that the acquisition technique that uses propeller rotation is more useful than the standard technique because it allows less contrast material to be administered for each rotation and a broader rotational arc of the c - arm , with high image quality and shorter acquisition times . va , dopo iniezione selettiva di mdc , secondo la proiezione pi utile determinata sul modello 3d in modo da ottenere immagini di integrazione diagnostica sovrapponibili per un idoneo confronto . in accordo con altri autori [ 18 ] , infine , riteniamo che la tecnica di acquisizione rotazionale in modalit propeller sia vantaggiosa rispetto a quella tradizionale , in quanto permette una ridotta quantit di mdc somministrato per singola rotazione e un pi ampio range di escursione rotazionale del tubo a c con elevata qualit delle immagini in tempi di acquisizione pi rapidi . conclusions in comparison with conventional 2d angiography , 3dra allowed a more confident choice of embolisation technique and materials ( type and angulation of the microcatheter , type and diameter of metal coils ) and a drastic reduction in the number of projections required for evaluating the lesion , leading to lower radiation dose and less contrast material to the patient . the 3d reconstructions enabled the correct identification of some small aneurysms that had doubtful findings on conventional imaging modalities . 
in addition , it allowed accurate evaluation of the lesions , thereby helping us in our choice of embolisation materials and technique and improving our results with regard to aneurysmal sac exclusion and coil deployment , with only one case of slight bulging of the coil through the aneurysm neck . 
finally , 3dra allowed for shorter procedure times and fewer risks and complications related to long procedure times and inaccurate choice of materials . we therefore believe this technique should become an integral part of angiographic diagnostics for planning endovascular treatment of cerebral aneurysms . conclusioni la 3dra , rispetto alla diagnostica 2d tradizionale , ha permesso di scegliere con maggiore precisione il materiale pi idoneo per la procedura ( tipo e curvatura del microcatetere , diametro e tipologia delle spirali metalliche ) , la tecnica di embolizzazione , e di ridurre drammaticamente il numero di proiezioni necessarie alla valutazione della lesione vascolare consentendo pertanto una equivalente riduzione della dose di esposizione e mdc al paziente . grazie alle ricostruzioni 3d sono stati correttamente individuati alcuni piccoli aneurismi , la cui presenza era dubbia con le metodiche di imaging tradizionali . 
inoltre , la possibilit di valutazioni accurate per la scelta del materiale e della tecnica ha consentito di ottenere risultati migliori in termini di esclusione della sacca aneurismatica e di disposizione delle spirali allinterno della sacca stessa , con un solo caso di lieve bulging di spirale attraverso il colletto dellaneurisma . 
la 3dra ha permesso infine la riduzione dei tempi di trattamento , dei rischi e delle complicanze per il paziente , legati sia ai tempi dintervento che alluso e alla scelta dei materiali . 
faccioli , tel : + 39 - 045 - 8124301 , fax : + 39 - 045 - 8277808 , e - mail : nfaccioli@sirm.org received : 01 september 2006 / accepted : 12 february 2007 / published online : 21 september 2007 abstract purpose . 
the aim of this study was to perform a cost analysis of contrast - enhanced ultrasonography ( ceus ) in the study of benign focal liver lesions ( bfll ) with indeterminate appearance on ultrasonography ( us )  . 
this cost analysis shows that ceus is the least expensive second - line modality after baseline us for the diagnosis of bfll . key words cost analysis contrast - enhanced ultrasonography liver benign focal lesions computed tomography riassunto obiettivo . 
i pazienti sono stati 398 , aventi 213 angiomi , 41 iperplasie focali nodulari ( fnh ) , e 154 pseudolesioni ( aree di risparmio di steatosi , aree di steatosi focale )  . 
per la diagnosi di angiomi nel 2002 abbiamo risparmiato 1406 , 97 , nel 2003 5315 , 22 , nel 2004 10317 , 78 , nel 2005 9536 , 13  . 
questo studio sullanalisi dei costi ha dimostrato che la ceus la pi conveniente tecnica di secondo livello dopo lecografia basale per la diagnosi di lesioni focali epatiche benigne . parole chiave analisi dei costi ecografia con mezzo di contrasto fegato lesioni focali benigne tomografia computerizzata n . 
when a focal liver lesion is incidentally discovered on baseline ultrasound ( us ) , the standard second - line examination , where required , is contrast - enhanced ct [ 35 ]  . the use of ceus has been suggested as a valuable diagnostic alternative to ct [ 15 ]  . 
 our analysis considers the costs of radiology services from the point of view of the producer ( the hospital ) whose aim is to provide the patient with the best and most cost - effective clinical approach . 
our study presents a cost - identification analysis as performed in previous studies [ 6 , 7 ] , namely , a partial assessment aimed at determining the impact of ceus and ct on costs . 
the aim of his study is therefore to analyse the impact on costs to the radiology department of the use of ceus rather than ct for the study of benign focal liver lesions ( bfll ) with indeterminate appearance on baseline us over a period of 4 years . materials and methods out of 2 , 140 ceus examinations performed between 2002 and 2005 , we retrospectively reviewed 1 , 187 studies of the liver . 
a decision - making model was constructed for patients with suspicious lesions on baseline us , which turned out to be bfll ( angiomas ; focal nodular hyperplasias ; and pseudolesions , areas of fatty sparing or focal fatty areas ) in 398 patients . 
the criteria by which a focal lesion was classified as indeterminate were the absence of the typical signs of angioma ( a homogeneously hyperechoic lesion with sharp margins ) or the absence of the typical signs of focal fatty area or focal fatty sparing ( a hyperechoic or hypoechoic lesion with sharp or blurred margins located in a typical perihilar or perivascular site )  . 
we analysed the cost effectiveness of ceus based on the need to follow up the studies with a ct scan ; that is , we considered the number of cases in which the information provided by ceus proved conclusive for the diagnosis . 
i progressi tecnologici hanno fatto s che tale indagine possa garantire una specificit elevata , anche se la letteratura riporta un range assai ampio ( tra 85% e 95% ) utilizzando di volta in volta la tomografia computerizzata ( tc ) , la risonanza magnetica ( rm ) o , meglio , listologia come gold standard [ 2 ]  . 
molti lavori hanno infatti preso in considerazione lapporto della ceus nei processi diagnostici e hanno sottolineato i suoi benefici per il trascurabile costo biologico intrinseco della metodica [ 2 , 3 ]  . 
attualmente , dopo il riscontro incidentale di una lesione focale epatica allecografia basale lesame standard di secondo livello , dove richiesto , consiste in una tc con mezzo di contrasto [ 35 ]  . 
in letteratura lutilizzo della metodica ceus segnalata come valida alternativa diagnostica alla tc [ 15 ] ; in caso di persistenza del sospetto si ricorre quindi alla tc , ma solo come eventuale terzo stadio delliter diagnostico . 
 la nostra analisi considera i costi di totale pertinenza dei servizi di radiologia dal punto di vista del produttore ( lazienda ospedaliera ) , il quale ha lobiettivo di fornire al paziente lapproccio clinico migliore e con il miglior rapporto costo - efficacia . 
lanalisi dei costi effettuata del tipo cost - identification cos come in altri lavori [ 6 , 7 ] , ovvero una valutazione parziale con lobiettivo di determinare , analizzando le due indagini considerate ( ceus e tc ) gli effetti sui costi . 
scopo di questo lavoro quindi lanalisi dellimpatto sui costi di pertinenza dei servizi di radiologia dellutilizzo della ceus in luogo della tc nello studio delle lesioni focali epatiche benigne ( lfeb ) ad aspetto non esaustivo dopo ecografia basale ( us ) , in un arco temporale di quattro anni . materiali e metodi su un totale di 2140 esami ceus eseguiti tra il 2002 ed il 2005 sono stati retrospettivamente considerati 1187 esami ceus del fegato , sui quali stato costruito un modello decisionale per pazienti con lesioni sospette allecografia basale rivelatesi poi lfeb ( angiomi , iperplasie focali nodulari , pseudolesioni : aree di risparmio di steatosi o aree di steatosi focale ) , per un totale di 398 pazienti . 
i criteri che hanno fatto classificare una lesione focale come indeterminata sono stati lassenza di aspetto tipico di angioma ( lesione a margini netti , omogeneamente iperecogena ) , o lassenza di aspetto tipico di aree di steatosi focale o di risparmio di steatosi ( lesione a margini netti o sfumati ipero ipoecogene nelle sedi tipiche perilari / perivascolari )  . 
all lesions were followed up for 22 months on average ( range : 836 months ) , and in no case was the initial ceus diagnosis changed during follow - up . as for evaluation of the economic impact from the hospitals point of view , the resources absorbed by the examinations were calculated by defining the unit cost in euros of each type of resource used . 
the resources assessed were equipment costs ( purchase and service contract costs ) , cost of supplies ( contrast agents , saline solution , medical supplies , films ) and staff costs ( radiologist , technician / nurse , administrative staff )  . ceus technique all examinations were carried out by radiologists with more than 5 years experience with a us device equipped with contrast - specific software that uses a harmonic frequency with low acoustic pressure ( 24 mhz coherent contrast imaging or cadence contrast pulse sequencing ; mechanical index 0.2 ; 1213 frames / s )  . 
insonation of the focal lesion was continuous , with dynamic observation of the transition between the unenhanced and the contrast - enhanced phase . the lesion enhancement pattern was compared with that of normal parenchyma and classified according to the literature [ 1 , 5 ]  . ct technique liver ct was performed with a single - detector device using a four - phase technique . 
spiral acquisition was performed with a fixed delay from the start of the injection , after 30 s ( arterial phase ) , after 75 s ( portal phase ) and after 4 min ( equilibrium phase )  . 
scan parameters for all phases were the following : collimation 5 mm , table feed 7.5 mm per rotation , reconstruction interval 5 mall ct studies were performed within 2 weeks from us . economic analysis the differential costs ( defined as the sum of equipment costs , cost of supplies and staff costs ) of ceus and ct were analysed according to the methods in use at our institute . three components of the differential costs were considered : ( 1 ) equipment costs ( depreciation and service contracts ) ; ( 2 ) cost of supplies and related services ; ( 3 ) staff costs . 
the cost of supplies and equipment are inclusive of 20% value added tax . the common costs of productive factors within the radiology department , that is , factors supporting all diagnostic seguire le indagini con un esame tc , ovvero considerando in quanti casi le informazioni ricavate dal mezzo di contrasto ecografico sono risultate esaustive in termini di iter diagnostico . 
nei pazienti con lfeb si sono riscontrati : 213 angiomi , 41 iperplasie focali nodulari ( fnh ) e 154 pseudolesioni ( aree di risparmio di steatosi , aree di steatosi focale ) ; i pazienti con lesioni benigne multiple sono stati considerati unitariamente , in quanto il protocollo dindagine non ha subito variazioni . tutti i pazienti hanno effettuato un esame ceus ( 36 nel 2002 , 113 nel 2003 , 125 nel 2004 , 124 nel 2005 ) e per 98 di questi pazienti si resa necessaria anche lesecuzione di un esame tc ( 9 nel 2002 , 41 nel 2003 , 21 nel 2004 , 27 nel 2005 )  . 
tutte le lesioni sono state seguite in follow - up per un periodo medio di 22 mesi ( range 836 mesi ) , e in nessun caso la diagnosi ceus iniziale mutata nel corso del follow - up . per la valutazione dellimpatto economico dal punto di vista dellazienda ospedaliera sono state calcolate le risorse consumate per svolgere gli esami , definendo per ogni tipologia di risorsa utilizzata il costo unitario in euro ( ) ; le risorse valutate sono state : costo delle apparecchiature ( prezzo di acquisto e manutenzione ) , costo dei materiali ( mezzi di contrasto , soluzione fisiologica , materiale sanitario , pellicole ) , costo del personale ( tempo medico , tecnicoinfermieristico , amministrativo )  . tecnica desame ceus tutte le indagini sono state eseguite da medici radiologi con pi di 5 anni di esperienza su un apparecchio ecografico , dotato di software contrasto specifico che utilizza una frequenza armonica a bassa pressione acustica ( 24 mhz coherent contrast imaging o cadence contrast pulse sequencing ; indice meccanico 0 , 2 ; 1213 frames / s )  . 
un bolo di 2 , 4 ml ( mezza dose ) di mezzo di contrasto di seconda generazione , sonovue ( bracco , milano , italia ) , stato iniettato endovena seguito da un bolo di soluzione salina di 5 ml . linsonazione della lesione focale stata continua con osservazione dinamica del passaggio tra la fase non contrastografica e quella contrastografica . 
il pattern di impregnazione della lesione stato confrontato con quello del normale parenchima e classificato secondo letteratura [ 1 , 5 ]  . tecnica desame tc lo studio tc del fegato stato espletato mediante apparecchio a singolo detettore e tecnica quadrifasica . 
lacquisizione spirale avvenuta con ritardo fisso dallinizio delliniezione a 30 s ( fase arteriosa ) , a 75 s ( fase portale ) e a 4 min ( fase di equilibrio )  . 
 when evaluating differential costs , we confined ourselves to the technical act , disregarding any other costs related to patient management , as done in previous studies [ 6 ]  . 
inclusion of the latter would have required an explicit description of the relations between the radiology department and other departments of our university hospital and , with regards to inpatients , the role played by imaging studies on the therapeutic process . 
therefore , our analysis was limited to the costs incurred by the radiology department , enabling us to make comparisons over time ( with reference to budget targets ) , between volumes ( increasing or decreasing workloads ) and across space ( with reference to other hospitals ) [ 6 ]  . 
 the cost of fixed - asset utilisation ( technology ) was related to the time of use , and the cost of radiological , technical and nursing staff was related to their specific activity measured on the basis of activity time . 
 economic savings were calculated by multiplying the number of lesions not requiring ct scans by the cost of a single ct examination : from this , we subtracted the differential cost of ceus compared with baseline us , i.e. 
the calculation can be represented as follows , where ct , ceus and us indicate their respective costs ( table 1 ) : ctn [ ( ceusus ) n ]  . results costs of ceus equipment costs ( depreciation and service contract ) we considered the cost of our us scanner . 
sono state prese in considerazione 3 componenti del costo differenziale , e precisamente : ( 1 ) costi delle apparecchiature ( ammortamenti e manutenzione ) ; ( 2 ) costi dei materiali e servizi connessi ; ( 3 ) costo del personale . 
i costi di materiali e apparecchiature sono comprensivi di iva al 20% . non sono stati calcolati i costi comuni dei fattori produttivi interni allistituto di radiologia , cio quei fattori che garantiscono unattivit di supporto a tutti gli atti diagnostici svolti nel reparto , poich si tratta di costi che non si modificano al variare del numero totale di esami svolti nel periodo annuo e che , essendo specifici per ogni struttura , rappresentano una variabile indipendente . il costo delle apparecchiature stato calcolato in base al tempo medio di utilizzo per esame delle stesse , valutando il costo dacquisto ed il calcolo dellammortamento . 
il calcolo dellammortamento stato effettuato su base temporale , a valore annuo costante . la durata della vita lavorativa delle apparecchiature radiologiche stata considerata di un tempo tecnologico massimo di otto anni . 
il tempo medico richiesto per lo svolgimento degli esami , considerato conforme al carico di lavoro standard del nostro istituto di radiologia , stato ricavato dal documento sirm per la determinazione dei volumi di attivit e produttivit dei medici radiologi [ 8 ] : tale valore risulta pari a 23 minuti per lo svolgimento di un esame us , 36 minuti per lo svolgimento di un esame ceus e 45 , 6 minuti per un esame nella valutazione del costo differenziale ci siamo limitati a considerare latto tecnico , ignorando tutti gli altri costi legati alla gestione del paziente , cos come in altri lavori [ 6 ] ; ci infatti avrebbe comportato lesplicitazione di tutti i rapporti tra la radiologia e gli altri reparti dellazienda ospedaliero - universitaria e , per i pazienti ricoverati , anche del ruolo che le indagini radiologiche hanno sul processo di cura . 
nella nostra analisi abbiamo quindi introdotto esclusivamente i costi dellistituto di radiologia : cos facendo possibile un confronto nel tempo ( rispetto a obiettivi di budget ) , nel volume ( secondo laumento o la diminuzione dei carichi di lavoro ) e nello spazio ( rispetto ad altre aziende ospedaliere ) [ 6 ]  . 
 il costo di utilizzo dei capitali fissi ( cio la tecnologia impiegata ) legato al tempo di impiego , cos come il costo del personale medico , tecnico e infermieristico legato alle specifiche attivit che li vedono coinvolti mediante misure del tempo di attivit . 
il costo del tempo medico , secondo i dati forniti dalla gestione risorse della nostra direzione sanitaria , risulta pari a 1 , 02 al minuto , mentre per quanto riguarda le figure professionali del tecnico di radiologia e dellinfermiere , di 0 , 37 al minuto . 
 il risparmio economico stato calcolato moltiplicando il numero delle lesioni che non hanno richiesto un esame tc per il costo di un singolo esame tc : da questo prodotto abbiamo sottratto il costo differenziale di un esame ecografico n . 
prendendo in considerazione la singola giornata lavorativa dellecografo pari a 12 ore e valutando in 36 minuti il tempo in cui lapparecchiatura impegnata per un esame delladdome , emerge un ecosto apparecchiature per esame di 8 , 43  . costi dei materiali e servizi connessi lesecuzione di un esame ceus prevede in media lutilizzo di : 2 , 4 ml ( mezza dose ) di mezzo di contrasto ecografico sonovue , per un costo di 30 , 68 a paziente , dato il costo confezione di 61 , 36 ; in media 4 pellicole di 2025 cm dal costo di 2 , 98 luna , per un totale di 11 , 92 ; una ago - cannula da 18 g ( 0 , 44 ) ; 13 ml in media di gel per ultrasuoni ( 0 , 41 per flacone da 260 ml , in media bastevole per 20 esami , quindi con un costo per esame di 0 , 02 ) e 5 ml di soluzione fisiologica ( meno di 0 , 01 , in quanto la confezione da 250 ml ha un costo di 0 , 21 e quella da 500 ml un costo di 0 , 31 ) , entrambi dal costo trascurabile . globalmente quindi risulta un costo variabile per esame di 43 , 04  . costo del personale limpegno temporale del medico dovuto al tempo preliminare allesame legato al raccordo anamnestico e al consenso informato , allesecuzione dellesame , allanalisi delle immagini e alla refertazione . 
we did not consider the actual time worked per year including days off work , as we were only analysing mean staff costs for each examination . for the baseline us scan , we calculated the same equipment costs , lower supplies costs two films instead of four and a radiological and nursing staff time of 23 min [ 8 ]  . 
non stato necessario considerare il tempo lavorativo effettivo annuo , comprese le assenze per congedo ordinario , poich abbiamo considerato solo il costo del tempo medio per esaper lesame ecografico basale stato calcolato il medesimo costo apparecchiature , un costo materiali inferiore , comprendente solo due pellicole , e un tempo medico e infermieristico di 23 min [ 8 ]  . 
da quanto esposto risulta che , sommando tutti i parametri considerati , il costo di un esame ceus del parenchima epatico presso il nostro istituto di 101 , 51 , con un costo differenziale di 55 , 15 rispetto allecografia basale ( tabella 1 )  . costi della tomografia computerizzata costi delle apparecchiature ( ammortamenti e manutenzioni ) il costo di acquisto dellapparecchiatura tc da ammortizzare risultato di 1032913  . 
essa viene utilizzata dallistituto di radiologia con contratto di manutenzione dal costo pari a 15000 , 00 annui , che , sommati alla quota di ammortamento di costo annua e considerando un anno di garanzia risulta di 24375 , 00  . 
prendendo in considerazione la singola giornata lavorativa della tc , pari a 12 ore , e quantificando in 45 , 6 minuti il tempo in cui lapparecchiatura impegnata per un esame delladdome , emerge un costo apparecchiature per esame di 68 , 27  . costi dei materiali e servizi connessi si impiegano in media 110 ml di mezzo di contrasto ; impiegando in ugual misura 4 tipi di mezzo di contrasto uroangiografici non ionici monomeri , il cui costo medio per flacone di 200 ml di 56 , 06 , il costo medio per esame quindi di 30 , 80 ; nella documentazione dellesame tc previsto luso di quattro pellicole 3543 cm dal costo unitario di 7 , 93 , per cui il costo medio delle pellicole per esame quantizzabile in 31 , 72 ; una ago - cannula da 18 g ( 0 , 44 )  . 
inoltre in circa lo 0 , 5% dei pazienti sottoposti a esami tc , essendoci unanamnesi allergica positiva , si esegue anche una preparazione farmacologica ( a base di cortisonici e antiistaminici ) per un costo di 4 , in media 0 , 04 in pi per ogni esame . 
in addition , approximately 0.5% of patients have a history of allergy and require pharmacological preparation ( cortisone and antihistamines ) costing 4 euros , leading to an additional 0.04 euros on average for each examination . 
overall , the variable costs per examination were euros 62.96. staff costs radiologist time covers different activities : review of the patients medical history , obtaining informed consent , planning the examination after patient preparation , acquiring the images and viewing them on the monitor and reporting . 
this description shows that the differential cost of a ct scan at our institute is 211.48 euros ( table 1 )  . technicians assistance radiology the external costs all patients imaged by contrast - enhanced studies with organic iodinated contrast agents , as in ct , undergo a blood test to determine serum creatinine , nitrogen and bilirubin , for an overall cost of approximately 5 euros per examination . this cost does not fall under the examination costs , but ct inevitably has a greater impact than ceus on costs external to the radiology department [ 7 ]  . 
per quanto riguarda il costo unitario legato alla professione infermieristica necessaria allo svolgimento dello stesso di 0 , 37 al min , e quindi di 16 , 87 il costo per esame . 
a differenza dellesame ceus necessaria anche la collaborazione del tecnico sanitario di radiologia medica ( tsrm ) ( 0 , 37 al min ) che comporta un costo aggiuntivo di 16 , 87  . 
da quanto esposto risulta come , sommando tutti i parametri considerati , il costo differenziale di una indagine tc risulti presso il nostro istituto di 211 , 48 ( tabella 1 )  . costi esterni in tutti i pazienti sottoposti a indagini contrastografiche che prevedono limpiego di un mezzo di contrasto organo iodato , quale lesame tc , viene effettuato un prelievo ematico per valutare i livelli sierici di creatinina , azotemia e bilirubinemia per un costo complessivo di circa 5 a esame . 
questo costo non rientra tra i costi dellesame , per inevitabilmente la tc viene a pesare maggiormente sui costi esterni alla struttura radiologica rispetto a un esame ceus [ 7 ]  . risparmio per esami ceus e tc per la diagnosi di angiomi nel 2002 abbiamo compiuto 4 tc / 13 ceus , il risparmio risultato stato di 1406 , 97  . 
in totale nei 4 anni il risparmio per le diagnosi di angioma stato di 26576 , 10  . per diagnosticare iperplasie focali nodulari nellanno 2002 abbiamo effettuato 1 tc / 2 ceus , il risparmio non stato significativo . 
in totale nei 4 anni passati il risparmio per le diagnosi di iperplasia focale nodulare stato di 3126 , 60  . per diagnosticare pseudolesioni nel 2002 abbiamo effettuato 4 tc / 22 ceus , risparmiando 2813 , 94  . 
nel 2003 abbiamo effettuato 17 tc / 50 ceus , risparmiando 5158 , 89  . nel 2004 abbiamo effettuato 5 tc / 38 ceus , risparmiando 5158 , 89  . 
 the introduction of ceus for the diagnosis of bfll with indeterminate appearance on baseline us enabled savings of 4 , 377.24 euros in 2002 , 11 , 255.76 euros in 2003 , 16 , 258.32 euros in 2004 and 15 , 164.01 euros in 2005 ; thus , in the 20022005 period , we saved 47 , 055.33 euros ( table 3 )  . discussion the effectiveness and efficiency of production processes are common concerns in italian health care agencies , particularly now that expenditure responsibilities are being transferred to the regions [ 9 ]  . 
our cost - analysis of ceus , unique in its kind , makes use of techniques commonly used in industry that ensure a methodological rigour that reduces the approximations of conventional cost - calculation methods [ 1016 ]  . the data that emerged from our analysis cannot be easily transferred to other radiology departments , as they reflect the unique situation of our facility at a specific point in time , and the costs incurred by other facilities may be very different as a result of different equipment costs and different organisational choices that may affect the cost of supplies or staff costs . 
the value of this analysis is that it proposes a model that can be applied to other settings and can serve as a stimulus for similar comparisons of the costs of two techniques . 
as previously suggested [ 7 ] , it is clear that cost analysis is merely the first step in a cost - effectiveness analysis that encompasses diagnostic benefits , including effects on treatment and biological costs . 
 the high diagnostic accuracy of ceus in the evaluation of bfll is well established , thanks to the diagnostic power of the dynamic and sinusoidal phases [ 15 ]  . 
the performance of ceus and ct in the characterization of bfll is similar despite the differences between the techniques . ceus nonetheless has a lower cost , and our department achieved savings of 47 , 055.33 euros over 4 years . 
the current diagnostic workup for incidentally detected liver lesions with a suspected benign nature includes baseline us , if necessary followed by ct . ceus can be inserted after baseline us to avoid the subsequent ct examination . 
our study considered cases in which ceus , performed as a complement to baseline us , enabled a definitive diagnosis , thus avoiding the use of ct and the differential cost related to its use . 
this distinction does not apply to malignant lesions , which , once detected , are compulsorily imaged by ct for oncological staging ; this explains why malignant lesions were not considered in our study . furthermore , with regard to biological costs , ceus undiscussione lefficacia e lefficienza dei processi produttivi sono argomenti avvertiti quotidianamente nelle aziende sanitarie , soprattutto in questa fase di regionalizzazione delle responsabilit di spesa [ 9 ]  . 
lanalisi dei costi ceus da noi effettuata in questo campo applicativo fa riferimento a tecniche ampiamente utilizzate in campo industriale che garantiscono un rigore che riduce le approssimazioni dei metodi tradizionali di calcolo dei costi [ 1016 ] , e non risulta comparabile a nessun lavoro in letteratura . 
i dati che emergono dalla nostra analisi non sono facilmente esportabili ad altre unit operative : essi rappresentano una fotografia della situazione nella nostra struttura in un certo momento storico , ma evidente che in altre strutture i costi possono essere estremamente diversi , sia per il costo differente delle apparecchiature utilizzate , sia per differenti scelte organizzative che possono incidere sui costi dei materiali o sui costi del personale . 
come gi suggerito [ 7 ] , chiaro che unanalisi dei costi rappresenta solo un primo tassello per giungere a unanalisi costo - efficacia , che consideri quindi da un lato i benefici diagnostici , includendo le ricadute terapeutiche , e dallaltro i costi biologici . 
 lelevata accuratezza diagnostica della ceus nella valutazione delle lfeb ormai un dato acquisito , in virt del potere diagnostico della fase dinamica e della fase sinusoidale [ 15 ]  . 
ceus e tc hanno performance simili nella caratterizzazione delle lfeb , sebbene le due metodiche abbiano differenti peculiarit : la ceus comunque associata a un costo inferiore , visto il risparmio di 47055 , 33 ottenuto nella nostra struttura nellarco di quattro anni . 
il nostro studio considera i casi in cui la ceus , espletata a completamento dellesame ecografico basale , ha condotto alla diagnosi definitiva risparmiando cos il ricorso a un esame tc e quindi il costo differenziale relativo . 
questa distinzione viene meno per le lesioni maligne per le quali , in seguito alla loro identificazione , si ricorre obbligatoriamente alla tc per esigenze di stadiazione oncologica ; per questo motivo esse non sono state considerate nel nostro studio . 
 non vi dubbio inoltre che , per quanto riguarda i costi biologici , la ceus offra chiari vantaggi rispetto alla tc per lassenza di radiazioni ionizzanti , nonch per lutilizzo di un mezzo di contrasto a microbolle con un profilo di tollerabilit migliore rispetto a un prodotto organo - iodato . 
these factors prompted us to replace ct with ceus as a second - line diagnostic procedure in the study of suspected benign lesions on us , despite the fact that ceus does not offer the same panoramic view as ct and is burdened by a small proportion of technical failures related to meteorism or obesity ( approximately 4% )  . 
 the use of ceus for the diagnosis of bfll over 4 years increased by 217% per year , and in 2005 , ceus was carried out in all patients with suspected benign lesions on us , reserving ct for only 17% ( 7 / 41 ) of thethe ceus examination , performed as a complement to baseline us during the same session , simplifies the diagnostic process , especially in terms of management . 
however , the radiologist needs to be perfectly aware of focal liver lesion semiotics during dynamic imaging , and a remote risk of anaphylactic reactions to us contrast material has been reported . the limitations of this study are related to the inclusion criteria : we arbitrarily decided to exclude malignant or suspicious lesions , which always require a second examination for confirmation or staging . 
the reason for this choice was that if malignant lesions had been included , the ceus study would have necessarily represented an additional cost in the diagnostic workup , and no other study would have been avoided . sostituzione della tc con la ceus come diagnostica di secondo livello nello studio delle lesioni ecograficamente sospette , anche se questultima metodica non garantisce la stessa panoramicit di esame ed gravata da una piccola percentuale di incompetenza tecnica , da meteorismo , o da obesit ( 4% circa )  . 
 lincremento di utilizzo diagnostico della ceus nella diagnosi di lfeb nel nostro istituto nellarco di 4 anni stato infatti del 217% annuo ; inoltre , nel 2005 la ceus stata effettuato in tutti i pazienti con lesioni sospette benigne allus , riservando la tc solo al 17% ( 7 / 41 ) di essi . 
midiri sezione di scienze radiologiche del dipartimento di biotecnologie mediche e medicina legale , via del vespro 127 , i - 90100 palermo , italy correspondence to : lo re , tel . : + 39 - 091 - 6518889 ; + 39 - 328 - 4553761 , fax : + 39 - 091 - 6552305 , e - mail : giuseppe.lore12@tin.it received : 28 august 2006 / accepted : 4 december 2006 / published online : 21 september 2007 abstract objective . 
sono stati esaminati 28 pazienti con diagnosi ileocoloscopica ed istologica di morbo di crohn ( mc ) , 6 pazienti con ileoconoscopia negativa per mc sono stati utilizzati come gruppo di controllo . 
le - tcmd con somministrazione orale di soluzione isotonica consente di valutare con elevata accuratezza le alterazioni dellintestino tenue in pazienti affetti da mc , dimostrandosi valida alternativa agli studi radiologici convenzionali , specie nei pazienti che rifiutano lintubazione naso - digiunale . key words gastrointestinal diseases small bowel multidetector ct parole chiave patologie gastrointestinali intestino tenue tc multidetettore introduction introduzione crohns disease ( cd ) is a chronic inflammatory disease that may affect any portion of the gastrointestinal tract and that requires the use of specific techniques for diagnosis , complication detection and follow - up . 
among the numerous techniques that have been used in the diagnosis and follow - up of patients with cd , the most important are conventional enteroclysis , ultrasound ( us ) , computed tomography ( ct ) and il morbo di crohn ( mc ) una malattia infiammatoria cronica che pu interessare il tratto gastroenterico in tutta la sua estensione , e che necessita di metodiche dedicate per la diagnosi di malattia per la ricerca di complicanze , per il follow - up . 
its main limitations include the high radiation dose [ 2 ] , in part related to the need to use fluoroscopy guidance for placement of the nasojejunal tube [ 3 ] , the invasiveness of the intubation procedure and an inability to provide direct information on possible extraparietal involvement and / or possible complications . 
us is a valuable technique for the diagnosis and follow - up of cd [ 4 , 5 ] , partly due to the possibility of using sonographic contrast media [ 6 ] , as it allows direct evaluation of the diseased bowel loops and the degree of inflammatory activity and detection of complications . 
however , in addition to the limitations inherent to us , that is , the presence of bowel gas and operator dependency , further problems include the length of the examination , quantified by parente et al . 
as 2060 min per exam , and the risk of underestimating low - grade stenoses [ 7 ]  . ct , with or without bowel distension ( ct enteroclysis ) , has been proposed as a modality allowing accurate assessment of bowel involvement and , more recently , its performance has been considerably improved by the use of the newer multidetector ct scanners [ 815 ]  . 
reported that mri could be considered an alternative to ct , as its dynamic capabilities provide additional information in the absence of ionising radiation or iodinated contrast media [ 8 ]  . data from the literature demonstrate that mri does not suffer true limitations in the evaluation of patients with cd ; however , mri is less readily available and more expensive . 
 the aim of our paper is to propose an mdct - enteroclysis technique that does not require nasojejunal intubation and to evaluate the techniques diagnostic capabilities in patients affected by cd . materials and methods between june and december 2005 , we studied 28 patients ( 15 women , 13 men ; mean age 38 years ) by mdct enteroclysis at our department . 
the control group consisted of 15 patients with ileocolonoscopy negative for cd who underwent mdct enteroclysis for other reasons ( eight for intestinal bleeding , five for malabsorption syndrome and two for suspected bowel neoplasm )  . 
all patients were instructed to follow a low - residue diet during the 3 days prior to the examination , and on the third day , they received 4 , 000 ml of water and selg - esse 1000 ( promefarm , milan , italy )  . 
this was necessary to eliminate residual faeces , avoid reflux of faeces into the small fia , la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm )  . lenteroclisi rx costituisce lesame radiologico principale nella diagnosi del mc presentando alta sensibilit e specificit [ 1 ]  . 
le principali limitazioni di questa tecnica sono riconoscibili nellalta dose di esposizione per il paziente [ 2 ] , anche a causa della necessit dellutilizzo della guida fluoroscopica per il posizionamento del sondino naso - digiunale [ 3 ] , nellinvasivit conseguente allintubazione naso - digiunale , e nellincapacit di fornire informazioni dirette sulleventuale interessamento extraparietale e / o eventuali complicanze . 
lecografia rappresenta una valida metodica per la diagnosi e il follow - up del mc [ 4 , 5 ] , anche in relazione al possibile utilizzo dei mezzi di contrasto ( mdd ) ecografici [ 6 ] , consentendo la valutazione diretta delle anse intestinali coinvolte dal processo flogistico , oltre che del suo grado di attivit e delleventuale presenza di complicanze di malattia . 
tuttavia , oltre ai limiti propri della metodica ecografica la presenza di gas nelle anse e la dipendenza dalloperatore altre limitazioni allesecuzione dellesame sono da riconoscere nei lunghi tempi di esecuzione , quantificati da parente in un range di 2060 minuti per esame , e nella possibilit di sottostimare stenosi di basso grado [ 7 ]  . 
la tomografia computerizzata ( tc ) , senza o con distensione della anse intestinali ( enteroclisi tc ) , si proposta come metodica in grado di valutare accuratamente linteressamento intestinale in questi pazienti , e , pi recentemente , numerosi progressi sono stati raggiunti dallutilizzazione dei pi evoluti tomografi multidetettore [ 815 ]  . 
altra tecnica ampiamente utilizzata nei pazienti affetti da mc la risonanza magnetica ( rm ) , dotata di elevata risoluzione di contrasto per i tessuti molli e della possibilit di valutazioni multiplanari [ 1618 ]  . 
hanno evidenziato come la rm possa essere considerata una tecnica alternativa allesame tc , capace di fornire ulteriori informazioni anche grazie alla possibilit di eseguire studi dinamici , in assenza di esposizione a radiazioni ionizzanti e a mdc iodati [ 8 ]  . 
i dati della letteratura dimostrano come lo studio rm non mostri reali limiti nella valutazione dei pazienti affetti da mc rispetto allo studio tc , tuttavia bisogna ricordare la minore disponibilit di tomografi a rm e il maggiore costo dellesame . 
 scopo del nostro lavoro quello di proporre una metodologia di esecuzione dellenteroclisi tc multidetettore ( e - tcmd ) senza intubazione naso - digiunale , oltre che quello di valutarne la capacit diagnostica nei pazienti affetti da morbo di crohn ( mc )  . materiali e metodi dal giugno al dicembre 2005 , 28 pazienti ( 15 femmine , 13 maschi ; et media 38 anni ) sono stati sottoposti a e - tcmd presso il nostro dipartimento . 
mdct was performed after the oral administration of approximately 2 , 000 ml of water and macrogol 4 , 000 ( polyethylene glycol , promefarm , milan , italy ) 6090 min before the examination . 
to reduce bowel peristalsis , patients were administered 20 mg of hyoscine - n - butyl bromide ( buscopan , boehringer ingelheim , italy ) iv 10 min before the ct scan . all patients were studied with a 40 - slice mdct scanner ( brilliance 40 , philips medical system , cleveland , oh , usa )  . 
the examinations were performed before and 70 s after the iv administration of 1.5 ml / kg of iodinated nonionic contrast material ( iomeprol , iomeron 400 , bracco , italy ) at a flow rate of 2.53.5 ml / s , using the following scan parameters : collimation , 400.625 mm ; gantry rotation time , 420 ms ; slice thickness , 1.5 mm ; slice increment , 0.7 mm ; 140 kv ; 250 mas . 
data on the acquired volume were transferred to a dedicated workstation where , besides the axial images , multiplanar ( mpr ) , maximum intensity projection ( mip ) and volume rendering ( vr ) reconstructions were visualised . in each patient , we assessed bowel wall thickness ( reference value < 4 mm ) [ 15 ] , layering , contrast enhancement , ulceration , bowel diameter ( reference value < 3 cm ) [ 15 ] , enhancement of the surrounding fat , enlargement of the afferent vasa recta , nodal involvement ( reference value : maximum transverse diameter > 15 mm ) and presence of complications ( e.g. intraand extraperitoneal fistulae or abscesses )  . 
in 19 patients ( 67.9% ) , the mucosa of the thickened loops enhanced intensely after contrast administration , with engorgement of the mesenteric vasa recta ( comb sign )  . 
none of the patients in the conzione ileale e rifiuto allintubazione naso - digiunale ; criteri di esclusione sono stati : insufficienza renale ( con valore di creatininemia maggiore a 2 mg / dl ) , stato di gravidanza o allergia nota al mdc . 
come gruppo di controllo sono stati valutati 15 pazienti con reperto negativo allileocolonscopia , che hanno eseguito le - tcmd per altra causa ( 8 pazienti con sanguinamento intestinale , 5 pazienti con sindrome da malassorbimento e 2 pazienti con sospetta neoplasia intestinale )  . 
in tutti i casi stata consigliata una dieta priva di scorie nei tre giorni precedenti , e al terzo giorno sono stati somministrati 4000 ml circa di una soluzione di acqua e selg - esse 1000 ( promefarm , milano , italia )  . 
questa preparazione si resa necessaria per eliminare i residui fecali , evitare leventuale reflusso di feci nellintestino tenue , e permettere un pi rapido transito del mezzo di contrasto ( mdc ) negativo endoluminale . 
le - tcmd stato eseguito previa somministrazione orale di circa 2000 ml di una soluzione di acqua e macrogol 4000 ( polietilenglicole , promefarm , milano , italia ) , nei 6090 minuti precedenti . 
per ridurre lattivit peristaltica intestinale , 10 minuti prima dellesecuzione della scansione tc sono stati somministrati per via endovenosa 20 mg di n - butilbromuro di joscina ( buscopan , boehringer ingelheim , italia )  . tutti i pazienti sono stati studiati con un tomografo multidetettore a 40 canali ( brilliance 40 , philips medical system , cleveland , ohio , usa )  . 
in tutti i pazienti lesame stato eseguito prima e dopo 70 secondi dalla somministrazione endovenosa ( e.v. ) di 1 , 5 ml / kg di mdc iodato non ionico ( iomeprolo , iomeron 400 , bracco , italia ) con flusso di 2 , 53 , 5 i seguenti parametri : collimazione ml / s , utilizzando 400 , 625 mm , velocit di rotazione del tubo radiogeno 420 millisecondi , spessore di stato 1 , 5 mm , incremento di strato 0 , 7 mm , 140 kv , 250 mas . 
i dati relativi al volume acquisito sono stati trasferiti su una stazione di lavoro dedicata , e , oltre alle immagini assiali , sono state visualizzate ricostruzioni multiplanari ( mpr ) , mip e volume rendering ( vr )  . 
in ogni paziente sono stati valutati : spessore ( valore di riferimento < 4 mm ) [ 15 ] , stratificazione , enhancement post - contrastografico e presenza di eventuali lesioni ulcerative della parete intestinale , calibro delle anse ( valore di riferimento < 3 cm ) [ 15 ] , imbibizione del tessuto adiposo circostante , aumento di calibro dei vasa recta afferenti , interessamento linfonodale ( valore di riferimento : diametro trasverso massimo > 15 mm ) e presenza di complicanze ( es . : tramiti fistolosi o ascessi intra ed extraperitoneali )  . 
 risultati in nessun caso si sono avuti episodi di nausea e / o vomito e tutti i pazienti hanno giudicato accettabile sia la preparazione catartica che la somministrazione orale di polietilenglicole . 
sensitivity and specificity of mdct enteroclysis were 92.8% and 100% , respectively , with a positive predictive value ( ppv ) of 100% and a negative predictive value ( npv ) of 88.2%. 
the main symptoms are diarrhoea , abdominal pain and subocclusion . the development of fistulae ( enteroenteric , enteroabdominal or enterocutaneous ) or severe complications such as bowel occlusion , perforation or intraand extraintestinal abscesses occurs only late in the disease . 
in 19 pazienti ( 67 , 9% ) la mucosa delle anse patologicamente ispessite appariva dotata di intenso enhancement dopo mdc e.v. , con aumento di calibro dei vasa recta mesenteriali ( segno del pettine )  . 
conventional enteroclysis , with its high sensitivity and specificity , has been the most widely used technique for identifying the sites of disease ( often multifocal ) and assessing possible complications . 
among the major limitations of conventional enteroclysis is an inability to provide direct information on the degree of extramural involvement and the presence of complications . to overcome these limitations , investigators proposed the use of ct enteroclysis . 
the first ct studies of the small bowel , in the 1980s and 1990s , demonstrated that ct had a good diagnostic accuracy for identifying the typical signs of disease on the bowel wall and possible complications [ 812 , 18 , 19 ]  . 
to distend the bowel loops , several types of intraluminal contrast media have been used : positive , such as iodinated contrast agents [ 9 ] , negative , such as 0.5% methylcellulose [ 24 ] or , less commonly , water or lipid contrast media [ 25 ]  . controllo erano presenti segni da riferire a malattia infiammatoria dellintestino tenue . 
dai dati del nostro studio la sensibilit e la specificit delle - tcmd sono state rispettivamente del 92 , 8% e 100% ( vpp = 100% ; vpn = 88 , 2% )  . 
solo tardivamente si manifestano tramiti fistolosi ( entero - enterici , entero - addominali o entero - cutanei ) o complicanze gravi come occlusione intestinale , perforazione o formazione di ascessi intraintestinali ed extraintestinali . 
1a contrast - enhanced axial multidetector computed tomography ( mdct ) enterography image shows a segmental luminal narrowing with mural thickening and layering ( * ) of the distal ileum and engorged mesenteric vessels ( arrow )  . 
1a limmagine sul piano assiale dimostra riduzione di calibro e ispessimento parietale di unansa dellileo distale con stratificazione parietale ( * ) e aumento di calibro dei vasi mesenterici ( freccia )  . 
3a - c axial images ( a , b ) show mesenteric lymphadenopathy ( arrowhead ) , engorged mesenteric vessels ( arrow ) and mural thickening ( * ) of the distal ileuc same patient . 
3a - c le immagini assiali ( a , b ) dimostrano linfoadenomegalie mesenteriche ( testa di freccia ) , aumento di calibro dei vasi mesenterici ( freccia ) e ispessimento parietale ( * ) dellileo distale . 
lileocolonscopia rappresenta il gold standard per la valutazione dellileo nel sospetto di malattia infiammatoria , ma questa tecnica invasiva , non in grado di esplorare la totalit dellintestino tenue e non fornisce informazioni riguardanti leventuale coinvolgimento extraparietale del mc . 
lenteroclisi convenzionale ha rappresentato , per la sua elevata sensibilit e specificit , la tecnica maggiormente utilizzata sia per il riconoscimento delle localizzazioni della malattia , spesso multifocale , sia per la valutazione delle complicanze . 
i primi studi tc dellintestino tenue , eseguiti negli anni 80 e 90 , hanno dimostrato come lesame di tomografia computerizzata sia in grado di identificare con buona accuratezza diagnostica le manifestazioni proprie della malattia a carico della parete intestinale e le eventuali complicanze [ 812 , 18 , 19 ]  . 
si quindi pensato di unire la tecnica dellenteroclisi rx [ 20 ] , con intubazione naso - digiunale e somministrazione di metilcellulosa , a quella della tc [ 2124 ]  . 
per la distensione delle anse intestinali sono stati utilizzati diversi tipi di mdc endoluminali , positivi , come i mdc iodati [ 9 ] , o negativi come la metilcellulosa allo 0 , 5% [ 24 ] o , meno frequentemente , lacqua o mdc lipidici [ 25 ]  . 
 una nuova spinta allo studio tc delle patologie dellintestino stata fornita dalla commercializzazione delle nuove apparecchiature tc multidetettore , caratterizzate da una pi elevata risoluzione temporale , che rende possibile lacquisizione del volume addominale in una singola apnea , e da pi elevata risoluzione spaziale lungo lasse z . 
4 immagine assiale che dimostra una irregolarit con ulcerazioni ( testa di freccia ) del profilo di parete , che appare inoltre ispessita ( * ) , dellileo terminale . the advent of the new multidetector ct scanners added momentum to ct imaging of bowel disease , as these have a higher temporal resolution , allowing the acquisition of the entire abdominal volume in a single breath - hold and a highg . 
6 contrast - enhanced axial multidetector computed tomography enterography shows marked abnormal wall thickening and mucosal enhancement in preterminal ( arrow ) and terminal ileum ( arrowhead ) consistent with crohns disease . 
inoltre possibile dimostrare la presenza di una fistola entero - enterica tra il colon e lileo ( * )  . mpr e vr dotate di maggiore dettaglio anatomico , fornendo una iconografia che si avvicina maggiormente a quella della radiologia convenzionale , pi familiare agli specialistici non radiologi [ 26 ]  . 
per ottenere una buona valutazione dellintestino dunque necessario distendere le anse intestinali con mdc endoluminali , somministrabili sia tramite intubazione naso - digiunale che per via orale [ 27 ]  . lintubazione naso - digiunale per scarsamente tollerata dai pazienti , impedendo in alcuni casi lesecuzione stessa dellesame . 
dimostrano la stratificazione parietale e lenhancement post - contrastografico dellileo distale sede di flogosi attiva ( freccia ) e la presenza di una fistola fra lileo ( testa di freccia bianca ) e il sigma ( testa di freccia gialla )  . 
this results in an isotropic voxel that allows the generation of mpr and vr with finer anatomical detail and the production of images that are closer to those of conventional radiology and therefore more familiar to the referring specialists [ 26 ]  . 
to achieve a good evaluation of the bowel , the bowel needs to be distended with intraluminal contrast media , which may be administered either by nasojejunal intubation or orally [ 27 ]  . nasojejunal intubation is poorly tolerated by patients , precluding execution of the examination in some cases . 
our experience demonstrates that the oral administration of a negative intraluminal contrast agent produces adequate bowel distension , especially of the ileum , and is well tolerated by the patient . 
in the first case , some intestinal segments would be inadequately distended and thus poorly assessable , whereas in the second case , excessive gastric distension could cause vomiting as well as prevent adequate bowel distension . 
to ensure that the proximal small bowel is well distended , it may be useful to administer the last 250500 ml of water and polyethylene glycol solution 1520 min before the examination or before dellileo , con buona tollerabilit da parte del paziente . 
i pazienti sono stati istruiti a bere la soluzione lentamente e in modo continuo , evitando cos sia una discontinuit della colonna idrica dellintestino tenue che la possibile sovradistensione gastrica . 
nel primo caso alcuni tratti di intestino si presenterebbero non adeguatamente distesi , e quindi difficilmente valutabili , nel secondo caso leccessiva distensione gastrica potrebbe stimolare il vomito da parte del paziente oltre che impedire , ancora una volta , una adeguata distensione delle anse intestinali . 
la somministrazione degli ultimi 250500 ml della soluzione di acqua e polietilenglicole 1520 minuti prima dellesecuzione dellesame , e comunque prima della somministrazione del n - butilbromuro di joscina , permetterebbe una adeguata distensione anche delle anse prossimali dellintestino tenue . 
infatti bench la fase arteriosa avrebbe potuto permettere una migliore valutazione dellenhancement mucoso della parete intestinale sede di flogosi , precedenti studi in letteratura hanno sottolineato come lesecuzione di ununica fase post - contrastografica compresa fra 40 e 70 secondi dallinfusione del mdc consenta una adeguata valutazione dellenhancement postg . 
in fact , although the arterial phase might have allowed better evaluation of mucosal enhancement , previous studies have reported that the acquisition of a single postcontrast phase 4070 s after contrast administration enables adequate evaluation of mural enhancement . 
for the assessment of nodal enlargement , we decided to use an arbitrary size threshold , recording only lymph nodes with a transverse diameter greater than 15 mm , given that the visualisation of mesenteric nodes is not necessarily linked to disease . 
also , node size may vary widely , and no reference size criteria have been established [ 31 ]  . use of mpr , mip and vr images proved helpful both in identifying the degree and extent of cd and in detecting complications . 
in particular , mpr and mip images reconstructed in the coronal and coronal oblique plane , with different thicknesses depending on the region and the findings to be analysed , were useful for identifying perivisceral lymphadenopathy and evaluating the extent of disease and complications . 
in evaluating complications , the possibility of having mpr reconstructions in operator - defined planes allows better identification of possible enteroenteric or enterocutaneous fistulae , as well as improved assessment of the extension of fistulae and stenotic segments . 
per quanto concerne il riscontro di linfoadenomegalie abbiamo deciso di utilizzare una soglia dimensionale arbitraria evidenziando solo i linfonodi con diametro trasverso massimo maggiore a 15 minfatti , la presenza di linfonodi mesenterici non sempre si associa alla presenza di malattia e la dimensione dei linfonodi pu essere estremamente variabile , non potendo essere utilizzato alcun criterio dimensionale [ 31 ]  . il ricorso alle immagini mpr , mip e vr stato utile sia nella identificazione del grado e della estensione della malattia infiammatoria intestinale , sia nella identificazione delle complicanze . 
in particolare modo , le immagini mpr e mip ricostruite secondo i piani coronale e coronale obliquo , con spessori diversi in base alla regione e ai reperti analizzati , sono state utili nella identificazione delle linfoadenomegalie periviscerali , nella valutazione dellestensione della malattia e nella identificazione delle complicanze . 
in questo ultimo caso , la possibilit di ottenere ricostruzioni mpr secondo piani definiti dalloperatore , ha consentito una migliore identificazione di eventuali tramiti fistolosi entero - enterici ed enterocutanei , oltre che una migliore valutazione dellestensione sia degli stessi tramiti fistolosi sia di eventuali segmenti stenotici del piccolo intestino . 
per quanto riguarda i due pazienti negativi per mc allindagine e - tcmd , riteniamo che lo stadio di malattia molto precoce , caratterizzato allesame endoscopico dalla presenza di scarse ulcerazioni aftoidi dellultima ansa , non abbia determinato delle alterazioni dellanatomia della parete viscerale tali da renderli evidenziabili allesame e - tcmd . conclusioni conclusions mdct enteroclysis with oral administration of isotonic solution is an easy - to - perform technique that has good diagnostic accuracy for evaluating small - bowel alterations , extraparietal complications and mesenteric involvement in patents with cd . 
 le - tcmd con somministrazione orale di soluzione isotonica si dimostrata una tecnica di facile attuazione che consente di valutare con elevata accuratezza diagnostica le alterazioni del piccolo intestino nei pazienti affetti da mc , nonch la presenza di complicanze extraparietali e il grado di interessamento mesenteriale , dimostrandosi valida alternativa agli studi radiologici convenzionali , specie nei pazienti che rifiutano lintubazione naso - digiunale . 
planning , which was performed with the neuronavigator , was based on analysis of the location of the course of the main white matter tracts adjacent to the lesion ( pyramidal tract , optic radiation and arcuate fasciculus )  . 
overall , 40 / 75 tracts studied had no anatomical relation with the tumour , were not displaced by the tumour or could not be visualised in their entire course . 
analysis of the remaining 35 white matter tracts led to an a priori change in the surgical approach for corticotomy in four patients ( 16% ) , with no disagreement between the two neurosurgeons and an impact on the extent of resection during surgery in 17 ( 68% ) , thus an overall impact on the surgical procedure in 80% of cases . 
mediante un software dedicato , sono state ottenute le relative mappe colorimetriche e ricostruite in tre dimensioni le traiettorie dei fasci di sostanza bianca adiacenti alla neoformazione che sono state elaborate per la pianificazione preoperatoria . 
la pianificazione , effettuata mediante il neuronavigatore , si basata sullanalisi della localizzazione e del decorso dei principali fasci di sostanza bianca adiacenti la lesione ( fascio cortico - spinale , radiazione ottica e fascicolo arcuato )  . 
globalmente , dei 75 fasci considerati , 40 non avevano rapporto anatomico con il tumore , non venivano dislocati dallo stesso o non risultavano visualizzabili in tutto il loro decorso . 
despite the high incidence of cases in which the lesion is responsible for changes that hinder the reconstruction of white matter tracts , the technique can change the surgical approach for corticotomy , defines the extent of resection and leads to some change in the procedure in 80% of cases . 
the improvement of pre - existing symptoms and the absence of new symptoms in the postoperative phase , in our opinion , confirms the value of the technique . key words intra - axial brain tumors mri diffusion tensor imaging tractography preoperative planning intraoperative assessment chirurgico di corticotomia in 4 pazienti ( 16% ) senza casi di discrepanza nel giudizio tra i due neurochirurghi e un impatto sulla definizione dei limiti di resezione durante lintervento in 17 ( 68% ) , risultando complessivamente di impatto sulla procedura chirurgica nell80% dei casi . 
nonostante lelevata incidenza di casi in cui la patologia determina modificazioni che inficiano la possibilit di ricostruire i fasci di sostanza bianca , la tecnica modifica lapproccio chirurgico di corticotomia , consente di definire i limiti di resezione e determina globalmente un cambiamento dellintervento nell80% dei casi . 
il miglioramento della sintomatologia pre - esistente e lassenza di nuovi sintomi in fase post - operatoria conferma , a nostro avviso , la sua validit . parole chiave tumori cerebrali intra - assiali rm tensore di diffusione trattografia pianificazione pre - operatoria valutazione intra - operatoria introduction introduzione magnetic resonance imaging ( mri ) has , for years , been used in assessment , localisation and patterns of intracranial tumours . 
the possibility of combining the two techniques has led to implementing the results in preoperative planning for patients with intracranial tumours , thus enabling greater extension of the resection margins [ 4 ]  . it has also been recently demonstrated that tractography data can be integrated in a standard system of neuronavigation , thus offering surgeons intraoperative visualisation of the main white matter tracts [ 5 ]  . 
knowing the position these tracts during surgery can help prevent significant functional damage linked to overextensive resection [ 6 , 7 ] and help modify the approach to the tumour . the aims of our study were to : assess the possibility of identifying precise white matter tracts situated in proximity to an intracranial tumour define the anatomical and topographical relations between the same white matter tracts and the tumour verify the possibility of integrating tractographic images in the context of a stack of three - dimensional ( 3d ) la risonanza magnetica ( rm ) da anni routinariamente utilizzata per la valutazione , la localizzazione e la caratterizzazione dei tumori cerebrali . 
analogamente , si di recente proposto limpiego del tensore di immagine di diffusione ( dti ) come tecnica per identificare in vivo i tratti di sostanza bianca cerebrale [ 13 ]  . 
la possibilit di combinare le due tecniche ha permesso di implementare i risultati nella pianificazione pre - operatoria di pazienti con tumori cerebrali , consentendo una maggiore estensione dei margini di resezione [ 4 ]  . 
 stato inoltre dimostrato in tempi recenti che i dati della trattografia possono essere integrati in un sistema standard di neuro - navigazione , permettendo una visualizzazione intra - operatoria dei principali fasci di sostanza bianca [ 5 ]  . conoscere la posizione dei principali tratti di sostanza bianca durante lintervento chirurgico pu aiutare a prevenire danni funzionali rilevanti legati a resezioni troppo estese [ 6 , 7 ] e modificare lapproccio alla neoplasia . obiettivi del nostro lavoro sono stati : valutare la possibilit di identificare definiti fasci di sostanza bianca , localizzati in prossimit di un tumore cea . 
tutti i pazienti affetti da tumore cerebrale nel periodo suddetto sono stati infatti studiati anche mediante valutazione della trattografia con rm ; questa stata successivamente valutata in sede pre - operatoria per la pianificazione neurochirurgica , e intra - operatoria , nellambito della neuronavigazione , per la definizione dei margini di resezione . 
undici di questi pazienti erano portatori di glioblastoma multiforme ( gbm ) , 6 metastasi singole , 3 gliomi di iii grado , 4 gliomi di ii grado , un linfoma . 
tutti i pazienti sono stati valutati clinicamente sia in fase preche post - operatoria , a 1 mese dallintervento ( tabella 1 ) per definire la presenza di sintomi riferibili a un coinvolgimento dei fasci mielinici oggetto dello studio e verificare quindi , dal punto di vista clinico , lintegrit degli stessi in seguito allintervento . la valutazione clinica stata eseguita sempre dagli stessi neurochirurghi che hanno classificato i sintomi prima e dopo lintervento come peggiorati ( comparsa di nuovi deficit o aggravamento dei precedenti ) , stazionari o migliorati . protocollo di studio rm pre - operatorio il protocollo di studio pre - operatorio prevedeva lacquisizione , presso la rm del reparto di neuroradiologia del nostro istituto , di sequenze finalizzate a caratterizzare la lesione e a mettere in evidenza i rapporti con le strutture circostanti . 
sono state acquisite sequenze t2 , flair , t1 volumetriche isotropiche ( mprage ) prima e dopo somministrazione endovenosa di mezzo di contrasto ( mdc ) paramagnetico , sequenze di diffusione , perfusione e tensore a 6 direzioni . 
lo studio del tensore di diffusione stato effettuato mediante 6 direzioni non collineari ( valore di b = 0 e 1000 s / mm2 ) con sequenze echomaterials and methods patients the population studied was prospectively selected from all patients scheduled to undergo brain neurosurgery in the mrequipped operating theatre ( brain suite , brain lab ) of our institution between april and october 2006 . 
all patients suffering from brain tumours in this period were also studied with mr tractography , which was then assessed preoperatively for surgical planning and intraoperatively for neuronavigation to define the extent of resection . 
all patients were clinically assessed both in the preand postoperative phase 1 month after surgery ( table 1 ) to establish the presence of symptoms related to involvement of white matter tracts studied and therefore to clinically verify their integrity following surgery . clinical assessment was performed by the same neurosurgeons , who compared symptoms prior to and after surgery and classified them as worsened ( onset of new deficits or worsening of previous symptoms ) , unchanged or improved . preoperative mr protocol the preoperative study protocol involved the acquisition , at the mr suite of the neuroradiology division of our institute , of sequences designed to characterise the lesion and show its relations with the surrounding structures . 
the following sequences were acquired : t2 - weighted sequences , fluid attenuated inversion recovery ( flair ) , isotropic volumetric t1 - weighted magnetisation - prepared rapid acquisition gradient echo ( mprage ) sequences before and after intravenous administration of paramagnetic contrast material , and diffusion , perfusion and tensor sequences in six directions . 
the filter tracking technique involved the 3d reconstruction of the white matter tracts using a fractional anisotropy ( fa ) threshold of 0.2 and an angle between consecutive vector lines greater than 35 . 
the positioning of the roi for fibre tracking varied according to the trajectory of the fibres to be reconstructed ( posterior limb of the internal capsule for the pyramidal tract , lateral geniculate nucleus for the optic radiation and centrum semiovale for the arcuate fasciculus ) [ 1113 ]  . 
once the white matter tracts to be studied had been obtained , the volume of the neoplasm was reconstructed three dimensionally to assess relations with the contiguous structures and possible displacement with adjacent white matter tracts . 
mean data processing time for each tract was 23 m data processing was performed double blind by the same two experienced neuroradiologists ( with the possibility of agreement with a third neuroradiologist in the event of disagreement )  . 
the neuroradiologists also assessed whether the white matter tracts were in relation to the neoplasm ( distance from the margins of altered signal ; in the case of stage ii gliomas , less than 1 cm ) , whether and in which direction they were displaced and whether the bundle could be clearly visualised in its course in proximity to the tumour . tractography results were saved in a file containing the x / y / z coordinates for each fibre . 
after rigid registration of the b = 0 images with the anatomical volumetric package , and after having verified that there were no discrepancies between data ( differences greater than 3 mm ) in the region of the tumour , white matter tracts could be displayed in standard anatomical images . 
overall time for this data processing , which was generally performed the day prior to surgery , had a mean duration of 30 min . preoperative mr study in brain suite during the preoperative mr study in the brain suite , we acquired volumetric isometric t1 - weighted images with the same characteristics as those previously obtained without paramagnetic contrast material administration . 
these sequences were the basis for subsequent fusion with the preoperative images and had the aim of recognising the markers . total acquisition time of preoperative images for surgical planning was therefore considerably limited and on average was less than 10 min , centring included . to simplify mr data registration in the navigation system , we used a multichannel coil containing stereotactic markers that are read by the neuronavigator camera and then registered by the neuronavigator itself . 
la tecnica del fiber tracking prevedeva la ricostruzione tridimensionale delle fibre di sostanza bianca utilizzando una soglia di fa di 0 , 2 , e un angolo di elaborazione superiore a 35 . 
il posizionamento delle roi per il fiber tracking variava a seconda delle traiettorie delle fibre da ricostruire ( braccio posteriore della capsula interna per il fascio piramidale , ganglio genicolato per la radiazione ottica e centro semiovale per il fascicolo arcuato ) [ 1113 ]  . 
una volta ottenuto il fascio di sostanza bianca da valutare , stato ricostruito tridimensionalmente il volume della neoformazione per verificarne i rapporti di contiguit e leventuale dislocazione con le fibre di sostanza bianca adiacenti . 
gli stessi hanno inoltre valutato se il fascio mielinico avesse un rapporto di contiguit con la neoplasia ( distanza dai margini di potenziamento o di alterato segnale , in caso di glioma di ii grado , inferiore a 1 centimetro ) , se e in quale direzione fosse dislocato , e infine se il fascio fosse o meno chiaramente visualizzabile nel suo decorso in prossimit del tumore . 
dopo una registrazione rigida delle immagini b = 0 con il pacchetto volumetrico anatomico e dopo aver verificato che non esistessero discrepanze tra i dati ( differenze superiori a 3 mm ) nella zona del tumore , le ricostruzioni delle fibre possono essere visualizzate nel contesto delle immagini anatomiche . 
il tempo globale di questa elaborazione , generalmente eseguita il giorno antecedente allintervento , ha una durata media di circa 30 minuti . studio rm pre - operatorio in brain suite nel corso dello studio rm pre - operatorio in brain suite sono state acquisite immagini t1 volumetriche isotropiche con le medesime caratteristiche di quelle ottenute in precedenza senza somministrazione di mdc paramagnetico . 
as the tumours were prevalently high grade and neurosurgery aimed at debulking rather than total resection , this only occurred in two cases . assessment of planning on neurosurgical outcome the following methodology was adopted to assess the practical impact that the dti information had on surgical planning and procedure performance . 
in the prospective phase , two neurosurgeons ( lf , gda ) were asked to independently assess , and in the event of discordance assess in agreement , the zione delle immagini pre - operatorie per la preparazione del planning in sala operatoria pertanto notevolmente limitato e non supera mediamente , compresi i centraggi , i 10 minuti . per rendere pi facile la registrazione dei dati rm nel sistema di navigazione , viene utilizzata una bobina multi - canale allinterno della quale sono presenti dei marker stereotassici che vengono letti dalla telecamera del neuronavigatore e quindi registrati dal navigatore stesso . 
results obtained in the two phases of the study were tabled as positive or negative for the two parameters ( corticotomy and resection margins ) ( table 2 )  . 
trattandosi prevalentemente di tumori di alto grado in cui la resezione totale non lobiettivo finale della neurochirurgia ( prevalendo il concetto di citoriduzione ) , questa eventualit si realizzata solo in 2 casi . valutazione del planning sullimpatto neurochirurgico per valutare limpatto pratico che linformazione dellimaging del tensore ha avuto sulla programmazione e a . 
identification and relations of the tracts studied with respect to the tumour patient optic radiation pyramidal tract arcuate fasciculus dem slightly displaced inferiorly superiorly displaced incompletely displayed not in contact but inferiorly displaced medially and superiorly displaced medially and inferiorly displaced , in contact no relation proximal portion as a deep landmark medially displaced , not in contact no relation no relation superiorly and medially displaced , in contact superiorly and anteriorly displaced , in contact no relation superiorly displaced , in contact no relation inferiorly displace , not in contact laterally displaced superiorly displaced medially displaced , in contact medially and superiorly displaced , in contact superiorly displaced medially displaced , in contact medially and superiorly displaced , in contact medially displaced distal portion poorly displayed anteriorly and medially displaced , in contact no relation not in contact , cranial portion poorly displayed no relation no relation no relation no relation medially displaced no relation no relation medially displaced , in contact no relation displaced not displayed in temporal portion no relation not displayed in temporal portion not displayed normal and in contact anteriorly no relation not displayed in the frontal portion no relation poorly displayed in the frontal portion poorly displayed in the temporal portion in contact , not displaced no relation medially displaced , in contact displaced after the temporal portion , in contact with the frontal portion not displayed in the temporal portion medially displaced , in contact posteriorly displaced , not in contact no relation not in contact , poorly displayed cranially no relation no relation no relation displayed only in the frontal portion no relation not displayed anteriorly and medially displaced superiorly displaced and poorly slightly displaced medially , in contact displayed no relation not displayed displayed only in the frontal portion slightly displaced anteriorly slightly displaced anteriorly slightly displaced anteriorly no relation not displayed results integration of tractography data in the volumetric data set for the purposes of neuronavigation was technically possible in all cases . 
in the areas of interest ( where the tumour was in relation to white matter tracts ) there was a correspondence between the b = 0 images and the 3d images , with a deviation that did not exceed 3 mthis deviation tended to increase in the more cranial and caudal portions of the brain , which nonetheless were not assessed , as all tumours were central . table 2 summarises relations between white matter tracts studied and the tumour . 
in una prima fase , prospettica , stato chiesto a 2 neurochirurghi ( lf , gda ) di valutare , in cieco e con consenso in caso di discrepanza , il tipo di approccio chirurgico ( sede della corticotomia ) stabilito sulla base delle immagini rm convenzionali prima e dopo contrasto e sulle stesse immagini integrate con limaging trattografico ( con valutazione del fascio cortico - spinale , della radiazione ottica e del fascicolo arcuato )  . 
in una seconda fase ( retrospettiva ) stato chiesto al neurochirurgo operatore di descrivere se la valutazione delle immagini trattografiche riportate sulla neuronavigazione avesse contribuito a definire i limiti di resezione della lesione . 
i risultati ottenuti nelle due fasi dello studio sono stati tabulati in termini positivo / negativo per i due parametri ( corticotomia e limiti di asportazione ) ( tabella 2 )  . 
nelle zone di interesse ( aree di rapporto anatomico tra il fascio mielinico e il tumore ) esisteva una corrispondenza tra le immagini b = 0 e le 3d con una deviazione che non ha mai superato i 3 m questa deviazione tendeva ad aumentare nelle porzioni pi craniali e caudali del cervello , non oggetto tuttavia della valutazione trattandosi in tutti casi di tumori centrali . 
venti dei 75 fasci considerati ( fascio piramidale , arcuato e radiazione ottica per 25 pazienti ) non avevano rapporti con la neoplasia ; 17 ( 23% del totale e 30% dei fasci aventi rapporto anatomico con il tumore ) non sono stati visualizzati ( anche parzialmente ) in relazione allanisotropia indotta dal tumore lungo il loro decorso . 
al controllo a 1 mese un paziente , precedentemente asintomatico , riferiva un disturbo del linguaggio a tipo disfasia sensoriale , riferibile verosimilmente a un danno del fascicolo arcuato ( da notare come , in questo paziente , non fosse stato possibile documentare in tutto il suo decorso questo fascio mielinico per le modificazioni indotte dalledema peri - lesionale ) ; nei restanti 24 la sintomatologia era invariata , con tendenza al miglioramento in 14 dei 17 pazienti sintomatici per coinvolgimento dei fasci mielinici segnalati ( tabella 1 )  . 
una asportazione estesa del tumore pu ridurre il rischio di eventuale recidiva ( specie nei gliomi di basso grado di malignit ) e consente una maggiore efficacia nelle successive terapie radianti o chemioterapiche . 
at 1 - month follow - up , one patient previously asymptomatic reported a speech disorder ( transcortical sensory dysphasia ) , most likely due to damage to the arcuate fasciculus ( it is worth noting that depiction of the entire course of this white matter tract was not possible in this patient due to changes induced by perilesional oedema )  . in the remaining 24 patients , symptoms remained unchanged , with a tendency to improvement in 14 / 17 patients reporting symptoms related to involvement of white matter tracts studied ( table 1 )  . discussion neurosurgery for a brain tumour is a trade - off between maximum surgical resection on the one hand and maximum sparing of functions on the other . 
these techniques have proved useful in establishing relations between the tumour and the surrounding functional cortical areas ( fmri ) and the state of some white matter tracts ( dti )  . 
knowledge of the structural integrity and location of certain white matter tracts with respect to an intracranial lesion is crucial for neurosurgical planning , both for defining the surgical access point and identifying the extent of tumour resection . dti is a significant advancement in the field of diagnostic imaging . 
it is , in fact , the only method capable of displaying cerebral white matter tracts in vivo , and it has been shown that this knowledge can assist the neurosurgeon in preoperative planning [ 1 ]  . 
although this technique has been available for several years , few studies have systematically analysed the impact dti data has on surgical planning and , more importantly , on surgical success [ 5 , 14 ]  . 
the main aim of the present study was , therefore , to assess how often dti data changes the approach to corticotomy and the extent of tumour resection . our study confirms that dti can be used to identify tumour location and its relations with important white matter linguaggio , migliora decisamente la qualit di vita di questi pazienti . 
questi strumenti si sono dimostrati utili per determinare la relazione tra il tumore e le aree funzionali corticali limitrofe ( fmri ) e lo stato di alcune fibre di sostanza bianca ( dti )  . 
la conoscenza dellintegrit strutturale e la localizzazione di alcuni fasci mielinici rispetto a una patologia cerebrale cruciale ai fini del planning neurochirurgico sia per definire laccesso chirurgico alla lesione che per identificare i limiti di resezione dello stesso . 
infatti il solo metodo che pu visualizzare tratti di sostanza bianca nel cervello in vivo , ed stato dimostrato che questa conoscenza pu aiutare il neurochirurgo nel planning pre - operatorio [ 1 ]  . nonostante questa tecnica abbia ormai qualche anno , pochi studi hanno analizzato in modo sistematico quale impatto abbia effettivamente linformazione fornita dal dti sul planning e , in particolare , sul successo chirurgico [ 5 , 14 ]  . nello specifico , luso pi importante del dti quello di confermare pre - operatoriamente lintegrit e la localizzazione dei tratti dislocati . 
lo scopo principale del presente studio stato appunto quello di valutare in che percentuale le informazioni prodotte dalla trattografia modifichino le modalit di un intervento neurochirugico sia nellapproccio alla corticotomia che nella definizione dei limiti di resezione . 
 il nostro studio ha confermato che il dti pu essere utilizzato per rilevare la localizzazione del tumore in rapporto a fibre importanti di sostanza bianca quali il fascio cortico - spinale , la radiazione ottica e il fascicolo arcuato in pazienti con tumori cerebrali . 
in accordo con i dati riportati da questo autore , anche nel nostro studio gli errori di registrazione non superavano i 3 mm , limite che considerato nel range dellintegrazione tra fmri e dati della neuronavigazione [ 7 , 16 ]  . 
questo margine pu tuttavia variare in aree del cervello non centrali in relazione alla distorsione tipica delle immagini echoplanari in prossimit del basicranio e della volta . una seconda considerazione deve essere fatta sulla possibilit che il tumore determini modificazioni dellanisotropia adiacente in grado di inficiare la possibilit di visualizzazione di un fascio mielinico . 
non oggetto del presente studio la ben nota difficolt di definire il significato anatomico e prognostico di tale interruzione visiva delle fibre ( se da infiltrazione , edema o distruzione delle stesse ) e la nostra attenzione si indirizzata solo alla identificazione dei fasci a . 
nell immagine a sono stati rappresentati in 3d il tumore ( giallo ) , il fascio piramidale ( rosso ) , la radiazione ottica ( viola ) , il fascicolo arcuato ( verde )  . 
images a , b show in 3d the tumour ( yellow ) , the pyramidal tract ( red ) , the optic radiation ( green ) and the t1 - weighted magnetic resonance images following contrast enhancement in the coronal and sagittal planes . 
nelle immagini a , b sono stati rappresentati in 3d il tumore ( giallo ) , il fascio piramidale ( rosso ) , la radiazione ottica ( verde ) e le immagini rm pesate in t1 dopo mdc sui piani coronali e sagittali . 
in agreement with the data reported by these authors , registration errors in our study did not exceed 3 mm , a limit considered to be in the range of integration between fmri and neuronavigation data [ 7 , 16 ]  . to define a safety margin , nimsky proposed a distance of 5 mm as reliable for the pyramidal tract . 
this margin may nonetheless vary in noncentral areas of the brain due to the typical distortion of echoplanar images in proximity to the skull base and vault . secondly , the possibility that the tumour causes adjacent anisotropy changes capable of impeding visualisation of white matter tracts needs to be considered . 
our study did not consider the well - known difficulty in defining the anatomical and prognostic significance of this visual interruption of fibres ( caused by infiltration , oedema or fibre destruction ) , as it focused only on identifying specific tracts . 
more comforting results were obtained for analysis of the pyramidal tract ( not displayed and in only its distal portion in only 16% of cases ) and the optic radiation ( not displayed in only 5% of cases )  . 
as expected , due to limited perifocal oedema , there were no documented cases of anisotropy impeding visualisation of white matter tracts in low - grade tumours . despite these intrinsic limitations , dti associated with 3d tractography for the study of white matter tracts in the brain proved highly useful for preoperative planning . 
in a recent study , they noted that the pyramidal tract shift that occurs after resection of a large part of the tumour can be as high as 8 mm [ 5 ]  . 
this observation was confirmed in our study in the two cases in which tractography was repeated during surgery . this underlines that in some cases , when tumour resection is extensive , dti images need to be repeated . 
il fascicolo arcuato risultato quello maggiormente coinvolto e considerando i casi in cui il tumore avesse un rapporto di contiguit con questo fascio la sua identificazione stata possibile solo nel 12% dei casi . 
risultati decisamente pi confortanti sono stati ottenuti dallanalisi del fascio piramidale ( non visualizzabile e solo nella sua porzione pi distale solo nel 16% dei casi ) e della radiazione ottica ( non visualizzata solo nel 5% dei casi )  . 
come atteso , in relazione allo scarso edema perifocale , non sono mai state documentate alterazioni dellanisotropia in grado di inficiare la visualizzazione dei fasci mielinici nelle forme a basso grado di malignit . nonostante questi limiti intrinseci , la tecnica del tensore di diffusione , associata alla trattografia tridimensionale per lo studio dei fasci di sostanza bianca cerebrale , risultata di grande utilit nella pianificazione pre - operatoria . 
dai risultati dal nostro studio , emerso che nel 16% dei casi analizzati , la tecnica ha modificato a priori lapproccio chirurgico di corticotomia , e nel 68% dei casi la conoscenza della posizione dei fasci mielinici ha posto indicazione sui limiti di resezione , con una modificazione globale della procedura neurochirurgica dell80% . 
di recente lo stesso autore ha sottolineato come lo spostamento del fascio piramidale che si realizza dopo lasportazione di buona parte del tumore possa raggiungere gli 8 mm [ 5 ]  . 
tale incidenza potrebbe inoltre essere pi elevata nei tumori con basso grado di malignit , in cui la resezione completa pi rilevante e che rappresentano una esigua percentuale della nostra casistica cos come di quella di nimsky [ 5 ]  . lattendibilit delle immagini trattografiche nella definizione di un fascio mielinico non una problematica di semplice risoluzione . 
 [ 20 ] , there is insufficient agreement between tractography and intraoperative subcortical electrostimulation , whereas another study [ 21 ] suggests there is good agreement between the two techniques . 
although their case series focused on low - grade glial tumours , gambini et al [ 22 ] showed a correspondence between the sites of intraoperative subcortical neurostimulation and tractography in 84% of motor tracts and 79% of language circuits . 
this means that assessment is possible only when resection is near or in the context of the white matter tract , which according to some authors may lead to postoperative transitory ( 37% ) or permanent ( 7% ) neurological deficit . 
in addition , another study [ 23 ] points out that in 50% of cases , nonsubcortical tracts cannot be identified , thus rendering comparison between intraoperative tractography and electrophysiological mapping even more complex . 
comparison is further complicated by the above - mentioned possible brain shift as a consequence of tumour resection . in our study , whereas the possibility of an intraoperative neurophysiological acquisition was not available , we assessed the effective preservation of white matter tracts on the basis of the clinical assessment performed 1 month after surgery . 
indeed , in this patient , the arcuate fasciculus was not displayed in its entirety due to changes induced by perilesional oedema . all remaining patients displayed no new neurological symptoms , and in more than 80% there was an improvement of the preexisting symptoms of neurological deficit . 
 [ 22 ] , seppure su una casistica di tumori gliali di basso grado , hanno dimostrato una corrispondenza tra i siti di neurostimolazione sottocorticale intraoperatoria e la trattografia dell84% per il fascio motorio e del 79% per i circuiti del liguaggio . 
questo significa che la valutazione possibile solo quando la resezione in prossimit o addirittura nel contesto del fascio mielinico potendo , secondo alcuni autori , determinare linsorgenza di deficit neurologici post - operatori transitori ( 37% ) o permanenti ( 7% )  . 
inoltre , secondo altri autori [ 23 ] non possibile identificare alcuna via sottocorticale nel 50% dei casi , rendendo il paragone tra la trattografia intraoperatoria e il mappaggio elettrofisiologico ancora pi complesso . 
a complicare ulteriormente tale confronto bisogna infine considerare la citata possibile dislocazione delle strutture cerebrali in conseguenza della resezione chirurgica . nel nostro studio , non disponendo della possibilit di una acquisizione neurofisiologica intraoperatoria , abbiamo valutato leffettiva preservazione dei fasci mielinici sulla base della valutazione clinica a distanza di tempo . 
questi dati sono in accordo con quanto riportato recentemente da nimsky [ 24 ] in una casistica di 137 gliomi cerebrali in cui lautore , utilizzando la trattografia intraoperatoria con una metodologia sovrapponibile alla nostra ha documentato la comparsa di nuova sintomatologia neurologica dopo lintervento chirurgico in 4 pazienti ( 2 , 9% della casistica )  . sebbene su una casistica limitata e su prevalente patologia ad alto grado di malignit , evidente , dai nostri risultati , che questo tipo di metodica un elemento di rilievo per una corretta pianificazione pre - operatoria e deve essere considerato un avanzamento importante della moderna diagnostica neuroradiologica per la pianificazione chirurgica di pazienti affetti da neoplasia cerebrale . conclusioni conclusions mr tractography offers the neurosurgeon an anatomical panoramic view and the opportunity for improved planning of surgical resection of intracranial lesions . 
despite the high incidence of cases in which the lesion produces changes that impede reconstruction of white matter tracts ( 30% of cases , with the arcuate fasciculus especially affected ) , the technique la tecnica della trattografia con rm offre al neurochirurgo una nuova panoramica anatomica che permette una migliore pianificazione della procedura chirurgica di resezione di patologia cerebrale . 
nonostante lelevata incidenza di casi in cui la patologia determina modificazioni che inficiano la possibilit di ricostruire i fasci di sostanza bianca ( 30% dei casi e specie nel fascicolo arcuato ) , la tecnica modifica lapa . 
algarotti 8 , i - 00137 roma , italy , tel . : + 39 - 349 - 1946942 , e - mail : stepieri@excite.it received : 25 september 2006 / accepted : 25 january 2007 / published online : 21 september 2007 abstract purpose . 
from 19992005 we treated 164 patients with massive pulmonary emboliswe used the same angiographic catheter for mechanical fragmentation and for administration of the fibrinolytic agent ( 2472 h )  . 
after fragmentation with the angiographic catheter , we observed four types of haemodynamic behaviour : in 61 patients ( 41.4% ) , mean pulmonary artery pressure fell rapidly below 30 mmhg ; in 38 patients ( 23.1% ) , two passes were required to achieve the same result ; in 32 patients ( 19.5% ) three passes were required . 
mechanical fragmentation with the angiographic catheter and administration of fibrinolytic agents effectively brought about a rapid improvement in patients clinical status by moving the embolus towards the periphery . key words pulmonary embolism mechanical fragmentation pharmacological thrombolysis riassunto obiettivo . 
la procedura interventistica stata effettuata direttamente con lo stesso catetere angiografico , sia per la terapia meccanica , che per linfusione del farmaco fibrinolitico nei giorni successivi ( 2472 ore )  . 
la frammentazione meccanica stata effettuata con un solo passaggio del catetere angiografico in 61 ( 41 , 4% ) pazienti e la pressione polmonare media scesa rapidamente al di sotto del valore di 30 mmhg . 
in altri 38 ( 23 , 1% ) casi si reso necessario ricorrere a due passaggi per raggiungere lo stesso risultato ; in 32 pazienti ( 19 , 5% ) si dovuto ricorrere a pi di 3 passaggi . 
la frammentazione meccanica con il semplice catetere angiografico si dimostrata valida e sicura per imprimere un brusco miglioramento delle pressioni polmonari e del generale stato clinico del paziente , mobilizzando lembolo polmonare dalla sua iniziale sede centrale . 
agresti : hybrid treatment with angiographic catheter in massive pulmonary embolism : mechanical fragmentation and fibrinolysis introduction introduzione pulmonary thromboembolism is a relatively common clinical condition [ 1 ]  . 
administration of fibrinolytic agents alone , either systemically or locally via a catheter , may fail to resolve the clinical picture [ 3 ] ; in fact , the severe haemodynamic condition needs to be corrected rapidly by lowering the mean pulmonary artery pressure and improving heart function [ 4 ]  . in 1995 , a technique for pulmonary thrombus fragmentation with the use of a modified pigtail catheter was introduced [ 5 ]  . 
in addition , the few published studies , which are based on small patient populations , show that there is not a great deal of experience with the use of such devices in this highly select field [ 7 , 8 ]  . 
special expertise is also required , and not all interventional radiologists may possess such expertise [ 9 ]  . our approach in cases of massive pulmonary embolism has been to systematically use a simple hybrid treatment involving manual fragmentation of the thrombus / embolus with a conventional angiographic catheter in association with fibrinolytic therapy administered via the same catheter over the following 3 days . 
the aim of the paper is to report the clinical and therapeutic considerations developed with our comparatively large patient population . materials and methods between 1990 and 2005 , 410 patients ( mean age 68 years , range 3578 ) were referred to our division for treatment of severe pulmonary thromboembolis of these , 164 were haemodynamically unstable due to the presence of a massive embolism , and this group was systematically treated by mechanical fragmentation of the thrombus and administration of fibrinolytic agents . the diagnosis of pulmonary embolism was made with computed tomography ( ct ) angiography . 
inclusion criteria for the hybrid combined mechanical and fibrinolytic treatment were severe hypotension ( ap < 90 mmhg ) and shock , angiographic confirmation of massive pulmonary embolism with involvement of the central pulmonary arteries and / or a pulmonary artery with flow diversion towards the contralateral side , and mean pulmonary artery pressure greater than 35 mmhg . hybrid treatment consists of a diagnostic phase and an interventional phase . 
nella variante massiva , lembolia polmonare presenta un grave quadro clinico , che pu mettere a repentaglio la vita del paziente e necessita di una rapida soluzione terapeutica [ 2 ]  . 
la sola somministrazione di farmaci fibrinolitici , per via sistemica o diretta localmente con il catetere , pu non risolvere il quadro clinico [ 3 ] ; c la infatti la necessit di migliorare il grave quadro emodinamico , con labbassamento della pressione polmonare media e il miglioramento del lavoro cardiaco [ 4 ] , in tempi estremamente rapidi . nel 1995 , stata introdotta la tecnica di frammentazione del trombo polmonare con limpiego di un catetere pig - tail modificato [ 5 ]  . 
successivamente , sono stati presentati anche altri presidi meccanici con lo scopo di diminuire i tempi della terapia fibrinolitica e di migliorarne lefficacia [ 6 ] , non solo sul versante arterioso . 
i vari presidi commerciali per , soprattutto per i loro costi , non sempre sono disponibili in una sezione di radiologia interventistica ; inoltre , dai pochi articoli presenti in letteratura , basati su una casistica molto limitata , si evince che c una limitata esperienza di un loro impiego in questo campo molto selezionato [ 7 , 8 ]  . 
richiesta inoltre una particolare perizia , che pu non essere patrimonio di tutti i radiologi interventisti [ 9 ]  . nei gravi quadri clinici abbiamo impiegato sistematicamente un semplice trattamento ibrido : una frammentazione manuale del trombo / embolo , effettuata sempre con un semplice catetere angiografico , associata a una terapia fibrinolitica , praticata dallo stesso catetere per i successivi 3 giorni . 
obiettivo del lavoro stato quello di riportare , sulla base di una ampia casistica , le considerazioni cliniche e terapeutiche maturate durante questa esperienza . materiali e metodi tra il 1990 e il 2005 , sono giunti al nostro servizio 410 pazienti per il trattamento di una tromboembolia polmonare grave : let media stata di 68 anni ( range 3578 ) ; tra di loro , 164 erano in condizioni dinstabilit emodinamica per la presenza di una embolia massiva , per cui stato applicato sistematicamente il trattamento meccanico di frammentazione del trombo seguito da infusione di farmaci fibrinolitici . la diagnosi di embolia polmonare era stata effettuata con angio - tc . 
i fattori di rischio maggiormente evidenziati erano la presenza di un intervento chirurgico nellanamnesi recente ( 48 pazienti ; 29 , 2% ) , una prolungata immobilizzazione ( 33 pazienti ; 20% ) , una sindrome dipercoagulabilit ( deficit di proteina c , antitrombina iii ; 51 pazienti ; 31% ) , combinazione di pi fattori ( 32 pazienti ; 19 , 5% )  . 
agresti : hybrid treatment with angiographic catheter in massive pulmonary embolism : mechanical fragmentation and fibrinolysis tially performed with brachial access using the venous cannula previously inserted at the time of patient admission ; when that was not possible , a femoral access was used . 
after administering local anaesthesia and substituting the needle cannula with a 7 - fr introducer sheath ( 4560 cm , arrow , reading , usa ) , we inserted the hydrophilic guidewire ( jtip , 180 cm , 3 cm floppy tip ; terumo , gadagroup , rome , italy ) , and then over this the angiographic catheter ( 145 pigtail catheter , 120 - cm long , 6 - fr diameter ; cordis , cordis europe , roden , the netherlands )  . 
the catheter enabled us to both measure the mean pulmonary artery pressure and administer the contrast material ( 40 ml at 20 ml / s in the left and right pulmonary arteries and 30 ml at 15 ml / s in the lobar branches ; optiray 300 , tyco healthcare spa , milan , italy ) to assess both the angiographic picture and guide the interventional procedure . the interventional phase of the hybrid treatment involved administration of 300 , 000 iu of urokinase ( urochinasi , ph&t spa , milan , italy ) directly via the pigtail catheter and mechanical fragmentation of the thrombus / embolus . 
the tip of the stiff portion of the guidewire was brought to about 1 cm from the beginning of the distal portion of the pigtail catheter to provide the necessary stiffness to the entire device . 
under direct fluoroscopic control , the angiographic catheter was rotated clockwise inside the pulmonary artery ( 510 rotations ) while at the same time being advanced or withdrawn over the guidewire in a craniocaudal direction . 
when required , mechanical fragmentation was repeated , with further cycles of ten rotations at a time , progressively moving peripherally ( lobar arteries ) or to the contralateral lung if pulmonary artery pressure failed to drop to below 30 mmhg . immediate outcome of the fragmentation procedure was assessed on the basis of the constant measurement of mean pulmonary artery pressure , the findings of pulmonary arteriography and the general haemodynamic status ( restored normotension )  . 
outcome was considered good when mean pulmonary artery pressure fell to 25 mmhg with the first pass of the catheter with clearance of the embolus from the central pulmonary arteries and the re - establishment of systemic arterial pressure above 90 mmhg . 
outcome was moderate if pulmonary artery pressure fell to 30 mmhg and poor when it only fell to 35 mmhg . in the following days , regardless of the pressure level reached after fragmentation with the pigtail catheter , fibrinolytic therapy was instituted in all patients . 
after having replaced the introducer sheath with a shorter one ( 8 fr , 11 cm ) , 50 , 000 iu / h urokinase was administered directly via the angiographic catheter , the tip of which was placed in the branches still affected by the fragments of the pulmonary embolis treatment was continued for 4872 h , with assessment of coagulation parameters every 34 h [ fibrinogen and international normalised ratio ( inr ) ] and angiographic and haemodynamic follow - up ever 24 h . 
in anestesia locale , dopo aver sostituito lago cannula con un introduttore con valvola 7 fr ( lungo 4560 cm , arrow , reading , usa ) , stato prima fatto scorrere il filo guida idrofilico ( punta a j , lungo 180 cm , punta floppy di 3 cm terumo , gadagroup , roma , italia ) e poi , su questo , il catetere angiografico ( pig - tail angolato a 145 , lungo 120 cm , calibro 6 fr cordis , cordis europe , roden , olanda )  . 
con questo stato possibile sia misurare la pressione polmonare media , sia iniettare mezzo di contrasto ( 40 ml a 20 ml / s nelle arterie polmonari destra e sinistra , 30 ml a 15 ml / s nei rami lobari optiray 300 , tycohealthcare spa , milano , italia ) sia per valutare il quadro angiografico , sia per indirizzare la procedura interventistica . la fase interventistica del trattamento ibrido , dopo infusione in bolo di 300000 ui di urochinasi ( urochinasi , ph&t spa , milano , italia ) direttamente dal catetere angiografico , prevedeva la frammentazione meccanica del trombo / embolo . nel catetere angiografico stata inserita la guida idrofilica per la parte caudale , di maggior supporto ; la punta della porzione rigida del filo guida stata portata fino a 1 cm circa dallinizio della porzione distale del catetere pig - tail , per fornire la necessaria consistenza a tutto il presidio . 
sotto diretto controllo fluoroscopico , il catetere angiografico stato girato in senso orario nellarteria polmonare ( 510 rotazioni ) , associandovi contemporanei movimenti di traslazione in senso craniale e caudale . 
ove necessario , la frammentazione meccanica veniva ripetuta , con altri cicli di 10 rotazioni per volta , progredendo sempre pi perifericamente ( arterie lobari ) , o aggredendo il polmone controlaterale se la pressione polmonare non scendeva sotto i 30 mmhg . il controllo degli esiti immediati della procedura di frammentazione veniva effettuato con la costante misurazione della pressione polmonare media , con le risultanze dellarteriografia polmonare e con il quadro emodinamico generale ( ristabilimento della normotensione )  . 
veniva considerato un buon risultato terapeutico il raggiungimento di un valore di pressione polmonare di 25 mmhg gi al primo passaggio , con contemporanea disostruzione delle arterie polmonari pi centrali e il ristabilimento di una pressione arteriosa sistemica oltre i 90 mmhg ; discreta era considerata la discesa della pressione nellarteria polmonare a 30 mmhg ; scarso era considerato il raggiungimento di un livello di 35 mmhg . in tutti i pazienti , indipendentemente dal valore pressorio raggiunto dopo la frammentazione meccanica con il catetere angiografico , dopo aver sostituito lintroduttore con valvola con uno pi corto ( 8 fr , 11 cm ) , la terapia veniva continuata , nei giorni successivi , con la somministrazione di farmaci fibrinolitici ( urochinasi 50000 ui / h ) direttamente dal catetere angiografico , la cui punta era posizionata nei rami ancora maggiormente impegnati dai frammenti dellembolia polmonare . 
agresti : hybrid treatment with angiographic catheter in massive pulmonary embolism : mechanical fragmentation and fibrinolysis results patients were treated within 812 h of onset of symptoms . there were 122 cases ( 74.3% ) of brachial access , 38 ( 23% ) of femoral access and only four cases of jugular access . mean pulmonary artery pressure prior to the diagnostic phase was 46 mmhg ( 5239 mmhg )  . 
injection of fibrinolytic agent alone , before contrast injection , did not substantially decrease the pulmonary artery pressure values ( from 46 to 45.1 mmhg ) , and the difference was not considered to be statistically significant . 
pulmonary artery involvement was right - sided in 62 patients , left - sided in 68 and bilateral in 34 . mechanical fragmentation was performed with a single cycle ( ten rotations of the catheter ) in 68 patients ( 41.4% ) , with mean pulmonary artery pressure dropping rapidly below 30 mmhg , haemodynamic parameters improving substantially and subjective symptoms improving ( less feeling of anxiety and oppression )  . 
labial cyanosis had disappeared , patients were able to lie supine without dyspnoea and no longer needed supplementary oxygen . two fragmentation cycles ( 20 rotations of the catheter ) were required in 38 patients ( 23.1% ) before mean pulmonary artery pressure fell below 30 mmhg . 
however , patients continued to be dependent on oxygen , with the appearance of dyspnoea at the slightest physical exertion . in 26 patients ( 15.8% ) , despite more than six cycles being performed , mean pulmonary artery pressure at no time fell below 35 mmhg . 
in all of these patients , the pulmonary embolism had simultaneously involved both pulmonary arteries la valutazione dei parametri della coagulazione ogni 34 ore ( fibrinogeno e inr ) e il controllo angiografico ed emodinamico ogni 24 ore . 
non sono stati considerati in questo studio i pazienti trattati anche con un trombolizzatore meccanico . risultati i pazienti , giunti nellarco di 812 ore dalla comparsa della sintomatologia , sono stati trattati con accesso brachiale in 122 casi ( 74 , 3% ) , femorale in 38 ( 23% ) e giugulare solo in 4 casi . 
la pressione polmonare media , misurata prima di iniziare la fase diagnostica , era di 46 mmhg ( 5239 mmhg )  . la sola iniezione del farmaco fibrinolitico , prima diniettare il mezzo di contrasto , non ha mai sostanzialmente modificato i valori delle pressioni polmonari : si passati da 46 a 45 , 1 mmhg : tale differenza di pressione non stata giudicata statisticamente significativa . 
il coinvolgimento delle arterie polmonari era preferenzialmente destro in 62 pazienti , sinistro in 68 , bilaterale in 34 . la frammentazione meccanica stata effettuata con un solo passaggio ( 10 rotazioni del catetere ) in 68 pazienti ( 41 , 4% ) ; in questi la pressione polmonare media scesa rapidamente al di sotto del valore di 30 mmhg , con un miglioramento sostanziale dei parametri emodinamici e un miglioramento della sintomatologia soggettiva ( miglioramento del senso dangoscia e di oppressione )  . 
 in altri 38 ( 23 , 1% ) si reso necessario ricorrere a due passaggi di frammentazione ( 20 rotazioni del catetere ) prima di verificare labbassamento della pressione polmonare media sotto i 30 mmhg . 
after mechanical fragmentation with angiographic the catheter , a sudden drop in mean pulmonary artery pressure is recorded , despite peripheral dispersion of the embolus fragments ( b )  . 
la preventiva arteriografia polmonare mostra unembolia polmonare massiva con interessamento di entrambe i polmoni ( a ) : il quadro , subostruttivo a destra e ostruttivo a sinistra , si associa a una pressione polmonare media di 46 mmhg . 
dopo la frammentazione meccanica con il catetere angiografico si registra un brusco abbassamento della pressione polmonare media , nonostante la dispersione periferica di frammenti di emboli ( b )  . 
mechanical fragmentation with the same angiographic catheter leads to a coarse rupture of the embolus with dislocation in peripheral segmental branches but with substantial immediate haemodynamic improvement ( mean pulmonary artery pressure 42 mmhg ) ( b )  . fragmentation is repeated in the upper lobe ( c )  . 
the result after 72 h of therapy is the near complete reperfusion of the right lung , where some peripheral perfusion defects remain in the lower lobe ( d )  . 
in six other patients , administration was suspended due to a further drop in serum fibrinogen . discussion acute massive pulmonary embolism is a severe and potentially fatal clinical condition [ 10 ]  . 
agresti : hybrid treatment with angiographic catheter in massive pulmonary embolism : mechanical fragmentation and fibrinolysis cardiac conditions and the progressive onset of right heart failure [ 11 ]  . 
criteria for distinguishing massive pulmonary embolism are the presence of systemic arterial hypotension ( < 90 mmhg ) and cardiogenic shock ( hypoperfusion , hypoxia , oliguria , altered level of consciousness ) [ 3 ]  . 
survival is therefore dependent on rapid recanalisation of the pulmonary artery and quick reduction of right heart workload . whereas the use of surgery is precluded in acute forms [ 3 , 12 , 13 ] because of the severity of the patients conditions , the invasiveness of the procedure and the rapidity required thrombolytic treatment alone is a valid supplement to heparin therapy for treating pulmonary embolisit has shown fig . 
al termine della terapia fibrinolitica di 72 ore , permangono difetti di perfusione in entrambi i polmoni ( c ) , con una pressione polmonare media rimasta a valori di 30 mmhg . terzo giorno di trattamento , per insufficienza cardiaca . 
in 16 pazienti stato impiantato un filtro cavale per levidenza di una trombosi residua a livello degli arti inferiori . non abbiamo registrato episodi di emorragia nella sede di puntura , mentre in 32 casi ( 19 , 5% ) labbassamento del livello di fibrinogeno al di sotto del livello di sicurezza ( 125 mg / dl ) ha imposto il dimezzamento della dose somministrata ogni ora , quale misura precauzionale ; in altri 6 pazienti la somministrazione stata sospesa per lulteriore abbassamento della fibrinogenemia . discussione lembolia polmonare acuta massiva , o maggiore , un grave quadro clinico , che pu mettere a repentaglio la vita del paziente [ 10 ]  . 
i pazienti sono a serio rischio di decesso nellarco di poche ore , in relazione alle preesistenti condizioni cardiache e per il progressivo instaurarsi di una insufficienza del cuore destro [ 11 ]  . 
i criteri per differenziare lembolia polmonare in forma massiva sono la presenza dipotensione arteriosa sistemica ( < 90 mmhg ) e di shock cardiogeno ( ipoperfusione , ipossia , oliguria , livello di coscienza ) [ 3 ]  . 
mechanical fragmentation with repeated passes only succeeds in breaking the embolus into very large pieces , which occupy the peripheral vessels ( b ) and almost totally exclude them from the circulation . 
larteriografia polmonare mostra la presenza di un grosso embolo nellarteria polmonare sinistra ( a ) ; la frammentazione meccanica con passaggi ripetuti in grado di rompere lembolo in parti molto grandi , che impegnano i vasi periferici ( b ) , escludendoli quasi totalmente dalla circolazione . 
la terapia fibrinolitica in grado di apportare limitati benefici ai frammenti centrali , mentre risolutiva solo per quelli pi periferici ( c )  . quindi , dipende dalla rapidit di ricanalizzazione dellarteria polmonare e dal brusco abbassamento del carico di lavoro a cui sottoposto il cuore destro . se il trattamento chirurgico improponibile nelle forme acute [ 3 , 12 , 13 ] vista la gravit del quadro clinico , la traumaticit dellatto e la rapidit richiesta la sola terapia trombolitica una valida aggiunta alla terapia eparinica per trattare lembolia polmonare . 
si dimostrata valida nel ridurre la mortalit e le recidive [ 14 ] , ma richiede tempo , dosi farmacologiche elevate e assistenza intensiva . viceversa , la frammentazione meccanica ha il vantaggio di conseguire una rapida ricanalizzazione dei vasi polmonari ; il razionale della procedura si basa sul fatto che il volume dellembolo relativamente largo se confrontato con le sole arterie polmonari principali ; viceversa molto pi piccolo se confrontato con il letto polmonare periferico . 
inoltre , la dispersione dellembolo nei rami di suddivisione periferica riduce drasticamente la pressione polmonare , aumenta il flusso disponibile per lo scambio gassoso in rami funzionalmente esclusi in precedenza , diminuisce le resistenze periferiche e il lavoro del cuore destro , migliorando lemodinamica generale . 
non ultimo , la frammentazione dellembolo incrementa la superficie di azione per il farmaco fibrinolitico , accelerando la lisi [ 4 ]  . la procedura di frammentazione stata introdotta nel to be effective in reducing mortality and recurrences [ 14 ] , although it does require time , high doses of fibrinolytic agents and intensive care . in contrast , mechanical fragmentation has the advantage of achieving rapid recanalisation of the pulmonary vessels . the rationale behind the procedure is based on the fact that the embolus is relatively large when compared with the main pulmonary arteries alone , although much smaller when coms . 
in addition , dispersion of the embolus towards the peripheral branches drastically reduces pulmonary artery pressure , increases the flow available for gas exchange in the branches functionally excluded previously , and lowers peripheral resistance and workload of the right heart , thus improving general haemodynamics . 
moreover , fragmentation of the embolus increases the surface area upon which the fibrinolytic agents can act , thus accelerating lysis [ 4 ]  . mechanical fragmentation with a special catheter was introduced in 1995 [ 5 ]  . 
the rotational movement of the tip of the modified pigtail catheter acts directly on the embolus within the pulmonary arteries , causing fragmentation and peripheral dislocation of the smaller fragments . 
in contrast , we employed a conventional pigtail catheter , using the stiff portion of the guidewire to provide greater support to the peripheral or coiled portion of the catheter . 
in this way , we were able to increase the correspondence between the rotational motion of the catheter tip and the motion imparted externally by the hands of the operator . 
in addition , both during and at the end of the rotations , we were able to verify the drop in mean pulmonary artery pressure values , improvement of haemodynamic state and peripheral dislocation of the smaller emboli in real time . 
other studies have reported similar behaviour using conventional angiographic catheters [ 4 , 1519 ] or devices for mechanical thrombolysis [ 6 , 20 , 21 ]  . the different behaviour of the emboli that we encountered with pigtail catheter fragmentation has also been reported in other studies : composition and morphology of emboli varies according to patient age [ 22 ]  . 
the stabilisation period of a thrombus varies from 2 to 33 days ( mean 10 ) , with the process being slower in more compromised patients [ 26 , 27 ]  . 
the different response of the emboli to mechanical fragmentation prompts a number of considerations that may have repercussions for the later management of the patient . on the basis of our experience and several studies published in the literature [ 6 , 16 , 17 , 28 ] , pulmonary emboli and their behaviour following mechanical fragmentation can be divided into four classes : type i : recently formed ( < 5 days ) and unorganised thrombi which have recently embolised . 
further haemodynamic improvement , with the re - establishment of near normal pulmonary artery pressure values , obtained with the administration of fibrinolytic agents over the following days , was further indirect confirmation of the recent formation of the clots and therefore of a greater fragility of the embolic material . 
it is likely that 1995 , con lausilio di un catetere speciale [ 5 ] ; il movimento rotatorio della porzione finale del catetere angiografico modificato agisce direttamente sullembolo , allinterno delle arterie polmonari , causando una frammentazione e una dispersione periferica dei frammenti pi piccoli . 
viceversa , noi abbiamo impiegato un comune catetere angiografico , fornendo un maggior supporto alla porzione pi periferica del catetere , quella arrotolata , con la porzione pi rigida del filo guida ; in questo modo stato possibile anche aumentare la corrispondenza tra movimento rotatorio della punta del catetere e quello impresso esternamente dalle mani delloperatore . dopo alcune torsioni della coda del catetere possibile seguire , sotto diretto controllo fluoroscopico , il movimento rotatorio della punta , in grado di frammentare lembolo . 
inoltre , sia durante che al termine delle rotazioni , stato possibile verificare , in tempo reale , il decremento dei valori di pressione polmonare media , il miglioramento dello stato emodinamico del paziente e la dispersione periferica degli emboli pi piccoli . 
anche altri autori hanno riscontrato lo stesso comportamento utilizzando comuni cateteri angiografici [ 4 , 1519 ] o i presidi per la trombolisi meccanica [ 6 , 20 , 21 ]  . il differente comportamento degli emboli , che abbiamo riscontrato con la semplice frammentazione del catetere angiografico , gi stato segnalato da altri autori : la composizione e la morfologia degli emboli varia con let del paziente [ 22 ]  . inoltre , i trombi tendono a retrarsi poco dopo che si sono formati ; i filamenti di fibrina vengono accollati , il siero viene espulso dal coagulo [ 23 ]  . 
con la retrazione o la compressione meccanica , il coagulo perde oltre il 90% delliniziale contenuto di plasminogeno e diventa sempre pi resistente al trattamento trombolitico [ 24 , 25 ]  . 
sulla base della nostra esperienza , confortata anche dalle esperienze di altri autori [ 6 , 16 , 17 , 28 ] possibile suddividere gli emboli polmonari e il loro comportamento dopo frammentazione meccanica in 4 classi : tipo i : pazienti con trombi di recente formazione ( < 5 giorni ) , non organizzati , che hanno embolizzato di recente . 
abbiamo registrato questa evenienza in 68 pazienti ( 41% ) ; sono quelli che hanno risposto meglio alla frammentazione meccanica con il solo catetere angiografico ; la brusca discesa dei valori pressori durante o al termine della frammentazione ne stata la diretta conseguenza . 
lulteriore miglioramento emodinamico , con ritorno ai valori quasi normali di pressione polmonare , ottenuto dopo linfusione di farmaco fibrinolitico nei giorni successivi , ha fornito lulteriore conferma indiretta della loro recente formazione e quindi di una maggiore friabilit del materiale embolico . 
probabilmente , tali emboli sarebbero andati incontro a risoluzione spontanea nei mesi successivi , ma abbiamo preferito comunque impiegare il farmaco fibrinolitico per aiutare il paziente a risolvere lepisodio acuto e diminuire il rischio dinsorgenza di una ipertensione polmonare . tipo ii : pazienti con trombi relativamente recenti ( < 10 giorni ) , o inizialmente organizzati , che hanno embolizzato s . 
agresti : hybrid treatment with angiographic catheter in massive pulmonary embolism : mechanical fragmentation and fibrinolysis these emboli would have spontaneously resolved over the following months , but we preferred to use the fibrinolytic agent to help the patient overcome the acute episode and reduce the risk of developing pulmonary hypertension . type ii : relatively recent ( < 10 days ) or initially organised thrombi that have recently embolised . 
once the proximal portion of the embolus has been damaged , the fragments that break away are coarser than the previous ones and , importantly , occupy the segmental branches and alter pulmonary perfusion . 
in these cases , continuing therapy in the following days with the administration of fibrinolytic agents is fundamental for attacking the softer portions of the embolus impacted in the segmental branches . 
in our experience , this type of embolism was seen in 38 patients ( 23% )  . type iii : more organised and less recent ( < 15 days ) thrombi , where mechanical fragmentation with the angiographic catheter required a greater number of passes before achieving a significant decrease in mean pulmonary artery pressure . 
the course in these patients , where the severe clinical picture is not completely resolved , will most likely be characterised by the onset of progressive pulmonary hypertension [ 29 ]  . type iv : older ( > 15 days ) and significantly organised thrombi . 
once they have broken away from the deep venous circulation , they present a very hard proximal portion of the embolus ( the part directed towards the guidewire ) , which cannot easily be fragmented with the simple movement of the angiographic catheter or be pierced with the guidewire . 
only 26 patients ( 15.8% ) had this type of embolis these patients required greater clinical care ( the placement of 17 inferior vena cava filters ) and received the least benefits from fibrinolytic treatment ( persistence of high levels of pulmonary artery pressure at the conclusion of the 3 - day therapy )  . continuous infusion of the fibrinolytic agent after mechanical fragmentation is performed because it is able to further improve haemodynamic condition by exploiting the greater surface area exposed to the fibrinolytic agent obtained by fragmentation of the embolus and the pressure difference . 
in questi casi , la prosecuzione della terapia , nei giorni seguenti , con la somministrazione del farmaco fibrinolitico di fondamentale importanza per aggredire le porzioni pi soffici dellembolo , quelle incuneate nei rami segmentali . 
nella nostra esperienza a questo gruppo di pazienti sono riconducibili 38 casi ( 23% )  . tipo iii : pazienti con una storia di trombi maggiormente organizzati , di data pi antica ( < 15 giorni ) , dove la frammentazione meccanica con catetere angiografico richiede un numero superiore di passaggi , prima di ottenere un significativo abbassamento della pressione polmonare media . 
nei giorni successivi , lazione fibrinolitica in grado di apportare solo lievi miglioramenti angiografici ( si sono mantenuti grossolani difetti di perfusione ) , emodinamici ( la pressione polmonare media non scesa sotto i 28 mmhg ) e clinici ( i pazienti seppure senza vistosa dispnea , a riposo continuavano ad avere una dipendenza dallossigeno e compariva dispnea al minimo impegno fisico )  . 
in questi pazienti , con risoluzione incompleta del grave quadro clinico , molto probabilmente levoluzione sar caratterizzata dallinstaurarsi di una progressiva ipertensione polmonare [ 29 ]  . tipo iv : pazienti con trombi di vecchia data ( > 15 giorni ) , notevolmente organizzati , che una volta staccatisi dal circolo venoso profondo presentano la porzione prossimale dellembolo , quella rivolta verso il filo guida , molto dura , consistente , difficili da risolvere con il semplice movimento di frammentazione operato dal catetere angiografico o da attraversare con lo stesso filo guida . 
sono i pazienti che hanno richiesto un maggiore impegno assistenziale ( impianto di 16 filtri cavali ) e che hanno risentito meno dellazione del farmaco fibrinolitico ( persistenza di valori elevati di pressione polmonare al termine dei tre giorni di cura )  . laggiunta del farmaco fibrinolitico in infusione continua , dopo la frammentazione meccanica , trova il suo razionale nel presupposto che possibile migliorare ulteriormente la condizione emodinamica del paziente , sfruttando la maggiore superficie dazione per il farmaco ottenuta dopo la frammentazione dellembolo e la differenza di pressione . 
infatti , in presenza di embolia polmonare massiva , in prossimit dellembolo ostruente si forma un flusso vorticoso ; ogni liquido infuso prossimalmente allembolo occludente ha un contatto temporaneo con i suoi confini e viene deviato e diluito nellarteria polmonare controlaterale non occlusa . 
agresti : hybrid treatment with angiographic catheter in massive pulmonary embolism : mechanical fragmentation and fibrinolysis fluid infused proximally to the obstructive embolus only temporarily comes into contact with its borders and is deviated and diluted in the nonobstructed contralateral artery . 
this enables the agent to be brought into contact with the fragments of the embolus , the surface area of which is now greater , particularly after removal of the external and less fragile portion [ 6 ]  . 
it should be borne in mind that at first , after initial fragmentation with the catheter , the haemodynamic situation can worsen following dislocation of the thrombus / embolus fragments towards the peripheral portions of the pulmonary branches , which may lead to a rise in mean pulmonary artery pressure . 
 our retrospective study identified four classes of haemodynamic behaviour after the hybrid treatment of massive pulmonary embolisit would be interesting to conduct a prospective study aimed at comparing the various therapeutic combinations according to the haemodynamic behaviour encountered in the patient after initial fragmentation with the pigtail catheter ( mechanical fragmentation and systemic heparin therapy alone , fragmentation and locoregional fibrinolytic therapy , fragmentation , emboli aspiration and locoregional fibrinolytic therapy , and fragmentation with aspirating devices and locoregional fibrinolytic therapy ) to confirm the orientations of patient management in order to more correctly define the type of hybrid therapy to systematically apply . monitoring pressure levels and angiographic findings in the acute phase only enabled us to confirm the validity of hybrid treatment in massive pulmonary embolishowever , it did not provide useful indications on the patients progression , onset or otherwise , of pulmonary hypertension or the validity of the approach adopted with respect to systemic pharmacological therapy . 
this also suggests the need for a prospective study to compare results of hybrid therapy with those obtained with systemic or locoregional fibrinolytic therapy . conclusion in conclusion , in patients with massive pulmonary embolism , mechanical fragmentation with a conventional pigtail angiographic catheter and the addition of intrapulmonary fibrinolysis proved capable of rapidly improving severe cardiopulmonary insufficiency . 
the treatment , therefore , is a viable and minimally invasive option capable of producing surprising results : it enables the patient to return to normal or near - normal mean pulmonary artery pressure values extremely rapidly . currently , no single solution is available for the manage [ 24 , 30 ]  . 
questo consente di portare il farmaco verso i frammenti di embolo , la cui superficie esposta allazione del fibrinolitico ora maggiore , soprattutto dopo aver rimosso la porzione pi esterna , meno friabile [ 6 ]  . 
occorre segnalare che , in un primo momento , dopo liniziale frammentazione con il catetere , la situazione emodinamica pu peggiorare in seguito alla dislocazione dei frammenti del trombo / embolo verso le porzioni pi periferiche dei rami polmonari ; tale evento pu comportare un innalzamento della pressione polmonare media . 
sarebbe interessante uno studio prospettico , che mettesse a confronto le varie combinazioni terapeutiche a seconda del comportamento emodinamico riscontrato nel paziente dopo liniziale frammentazione con il catetere angiografico ( solo frammentazione meccanica e terapia eparinica sistemica ; frammentazione e terapia fibrinolitica locoregionale ; frammentazione , aspirazione emboli e terapia fibrinolitica locoregionale ; frammentazione con presidi ad aspirazione e terapia fibrinolitica locoregionale ) per ottenere le conferme sugli indirizzi della gestione successiva del paziente , in modo da definire pi correttamente il tipo di terapia ibrida da applicare poi sistematicamente . il controllo dei valori pressori e delle risultanze dei quadri angiografici solo in fase acuta ci ha consentito di confermare la validit del trattamento ibrido nella embolia polmonare massiva , ma non ci fornisce utili indicazioni sullevoluzione successiva del paziente , sullinstaurarsi o meno dellipertensione polmonare , sulla validit dellopzione terapeutica effettuata rispetto al trattamento farmacologico sistemico . 
anche in questo caso si rende necessario uno studio prospettico per confrontare i risultati di questa impostazione terapeutica ibrida con quelli ottenuti con la sola fibrinolisi , sistemica o locoregionale . conclusione in conclusione , nei pazienti con embolia polmonare massiva la frammentazione meccanica con limpiego di un comune catetere angiografico pigtail , e laggiunta della successiva fibrinolisi intrapolmonare , si dimostrata in grado di migliorare rapidamente il grave quadro dinsufficienza cardiopolmonare che affliggeva il paziente . 
rappresenta quindi una opzione terapeutica reale , minimamente invasiva , con risultati sorprendenti : garantisce al paziente il ritorno a valori di pressione polmonare media normali o compatibili con la vita , in tempi estremamente rapidi . attualmente non disponibile una soluzione unica per la gestione di tutte le sfaccettature con cui si possono presentare i pazienti con embolia polmonare massiva . 
agresti : hybrid treatment with angiographic catheter in massive pulmonary embolism : mechanical fragmentation and fibrinolysis ment of all presentations of massive pulmonary embolism . the most recent guidelines suggest the use of mechanical fragmentation only in the most severe forms [ 31 , 32 ]  . 
our study seems to support this approach : when the embolus fails to immediately respond to mechanical fragmentation with a conventional angiographic catheter , other therapeutic options should be undertaken , including the use of mechanical thrombectomy devices . 
this suggests a greater commitment on the part of the vascular and interventional radiologist , who needs to be well versed in the use of such devices , as well as an economic obligation on the part of the hospital , which needs to consider these devices as lifesaving in such exceptional circumstances . linee guida suggeriscono limpiego della frammentazione meccanica solo nelle forme di embolia pi gravi [ 31 , 32 ] ; la nostra esperienza di trattamento ibrido , meccanico e farmacologico , dellembolia polmonare massiva , sembra avvalorare tale impostazione : quando lembolo non risponde subito alla frammentazione meccanica con il semplice catetere angiografico , dovrebbero essere per impiegate anche altre opzioni terapeutiche , tra cui i presidi meccanici . 
patients had been referred for suspected encephalitis ( n = 2 ) , dural sinus thrombosis ( n = 1 ) and multiple sclerosis ( n = 3 )  . mri examinations were repeated after 4 , 8 and 12 weeks and in two cases also after 6 and 9 months . 
to our knowledge and according to previous reports , the fact that these lesions are detected in a relatively large number of conditions with heterogeneous etiopathogenetic factors leads to the hypothesis that a common underlying pathophysiological mechanism that , considering signal characteristic , reversibility and white matter location , could be represented by vasogenic oedema . key words magnetic resonance imaging corpus callosum splenium focal lesions riassunto obiettivi . 
in 6 pazienti sottoposti a indagini tc e rm sono state riscontrate incidentalmente lesioni focali non emorragiche , isolate , nel contesto dello splenio del corpo calloso . i pazienti giungevano alla nostra osservazione con sospetto clinico di patologia infettiva ( 2 ) , trombotica ( 1 ) , demielinizzante ( 3 ) dellencefalo . 
secondo la nostra esperienza e quella di altri autori , essendo il riscontro di tali lesioni comune a un ampio spettro di condizioni patologiche con fattori eziopatogenetici eterogenei , ipotizzabile che attraverso un comune , complesso meccanismo fisiopatologico tali fattori possano creare squilibri responsabili della comparsa di edema vasogenico che si esprime in unalterazione del segnale rm nello splenio del corpo calloso . parole chiave risonanza magnetica corpo calloso splenio lesioni focali m . 
morphological and signal features of these lesions are usually unambiguous : they appear hyperintense in long tr sequences [ t2 - weighted and fluid attenuated inversion recovery ( flair ) ] and either slightly hypointense or insignificant in t1 . 
lesions are usually divided into two types according to extent and shape : oval , circumscribed , with well - defined borders and located in the middle portion of the splenium ; or wider , with less regular borders and involving the entire spleniu because such findings have been detected in a large number of clinical conditions , there is still controversy regarding their pathogenesis . 
the authors postulated that the lesion aetiopathogenesis and evolution could be related to medications used during treatment , as they were transient in nature and disappeared upon suspension of phenytoin and vigabatrin [ 3 ]  . 
in subsequent studies , several authors reported the detection on mri of transient focal cerebral abnormalities with similar features in patients with no evidence of seizures who were undergoing examination due to suspected viral encephalitis [ 4 ] , rotavirus encephalopathy [ 5 ] , acute cerebellitis [ 6 ] , low - grade glioma [ 7 ] , haemolyticuraemic syndrome [ 8 ] , salmonella - enteritidis - related encephalitis [ 9 ] and high - altitude cerebral oedema [ 10 ]  . although the majority of lesions were described in patients treated for seizures , the same findings were described in a wide spectrum of clinical conditions , suggesting that it is inappropriate to view them as a clearly defined disease pattern . 
rather than ascribing the findings to a distinctive pathology , it is more reasonable to believe that they represent a common specific pathophysiological condition developing in the splenium of the cc during different clinical situations . the aim of this study was to analyse the possible pathogenetic conditions responsible for the appearance of such lesions , attempting to provide an explanation and clinical correlation based upon our experience and on the published data . materials and methods six patients with transient focal lesions in the splenium of the cc were studied in our university department of radiological sciences . 
le caratteristiche morfologiche e di segnale di tali lesioni risultano generalmente univoche : appaiono iperintense nelle sequenze a tr lungo ( t2 pesate e flair ) mentre in quelle pesate in t1 possono manifestare una lieve ipointensit o risultare non apprezzabili ; non stato descritto un definito enhancement dopo iniezione di mezzo di contrasto ( mdc ) paramagnetico . 
per quanto concerne la morfologia e lestensione di tali alterazioni di segnale ne vengono descritte sostanzialmente due tipi : ovoidale , circoscritta , ben definita e mediana , oppure meno definita pi ampia e diffusa , estesa a interessarne lintera superficie . 
 [ 2 ] tali reperti venivano incidentalmente identificati in pazienti epilettici e gli autori formulavano lipotesi di una eziopatogenesi e unevoluzione correlate al relativo trattamento terapeutico , data la caratteristica transitoriet di queste alterazioni e la loro scomparsa alla sospensione di farmaci quali la fenitoina , la vigabatrina etc . 
in seguito , diversi lavori hanno riportato il riscontro di analoghe lesioni con le medesime caratteristiche in corso di condizioni differenti dallepilessia quali encefaliti virali [ 4 ] , encefalopatie da rotavirus [ 5 ] , cerebelliti acute [ 6 ] , glomi di basso grado [ 7 ] , sindrome emolitico - uremica [ 8 ] , encefaliti associate alla salmonella enteritidis [ 9 ] ed edema cerebrale da altitudine [ 10 ]  . in realt , anche se i riscontri pi frequenti sono stati descritti in pazienti trattati per crisi epilettiche di varia tipologia , il fatto che un range cos ampio di condizioni patologiche di base sottenda lo stesso reperto di imaging suggerisce limpossibilit di etichettare questo tipo di lesione quale pattern di una singola condizione clinica . 
pi ragionevole ritenere tali aspetti non tanto lespressione di una patologia piuttosto che di unaltra , ma di determinate condizioni fisiopatologiche che si sviluppano nel contesto dello splenio quale comune denominatore di unampia e variabile gamma di situazioni che ne condizionano la genesi . lo scopo di questo studio pertanto arrivare a formulare delle ipotesi circa le possibili condizioni patogenetiche responsabili della comparsa di tali alterazioni , oltre che identificarne il significato e le eventuali correlazioni cliniche in base alla nostra personale esperienza e ai dati riportati finora in letteratura . materiali e metodi presso listituto di scienze radiologiche delluniversit degli studi di sassari sono state riscontrate in 6 pazienti lesioni transitorie localizzate a livello dello splenio del corpo calloso . 
after the first mri scan , all patients underwent an electroencephalogram ( eeg ) , a complete blood count , and cerebral spinal fluid ( csf ) analysis to investigate the possible presence of pathogenic agents . 
 a 16 - year - old boy with a clinical history of hypopituitarism was referred to our department by the infectious disease ward , with a clinical suspicion of viral encephalitis . 
as this finding was nonspecific and therefore did not allow a definite diagnosis , the patient underwent further clinical investigations . a 22 - year - old woman affected by depressive crises was referred to us because of intense headaches . 
the patient was admitted to the neurology department for further diagnostic tests . a 16 - year - old boy with a clinical history of eczematoid psoriasis and intense frontotemporal headaches developed a faciobrachiocrural hemiparesis . 
in tutti i pazienti , gi sottoposti ad una tc cranio , stata effettuata una rm dellencefalo ( shimadzu 1t philips intera achieva nova s 1 , 5t ) con studio sui piani assiale , coronale e sagittale in tecnica se , tse e ir e sequenze pesate in dp , t2 , flair , diffusione e in t1 prima e dopo iniezione di mdc paramagnetico . in tutti i casi le indagini sono state ripetute dopo 4 , 8 e 12 settimane . 
successivamente al primo esame rm , in tutti i pazienti sono stati inoltre effettuati un esame emocromocitometrico , il prelievo del liquor per la ricerca di eventuali microrganismi patogeni ed un elettroencefalogramma . caso 1 un ragazzo di 16 anni , con storia di ipostatuarismo , giunge alla nostra osservazione , inviato dal reparto di malattie infettive , con sospetto clinico di encefalite virale . 
laspecificit del reperto non consente al momento valide ipotesi diagnostiche , per cui il paziente , sempre in regime di ricovero , viene sottoposto a ulteriori accertamenti clinico - laboratoristici . caso 2 una ragazza di 22 anni , con notizie anamnestiche di crisi depressive , giunge alla nostra osservazione inviata dalla clinica neurologica per cefalea gravativa . 
lesame rm dellencefalo non documenta reperti di significato patologico in ambito parenchimale , mentre evidenzia una dubbia alterazione del normale segnale di flusso nella porzione laterale dei seni traversi , bilateralmente , che rende necessaria una ulteriore valutazione mediante angiografia digitale . 
a circa 3 mesi di distanza , la ricomparsa della sintomatologia rende necessario un secondo esame rm che documenta , nellambito dello splenio del corpo calloso , unarea di alterato segnale priva di enhancement dopo mdc . 
la paziente viene quindi nuovamente ricoverata presso listituto di clinica neurologica per ulteriori accertamenti diagnostici . caso 3 un ragazzo di 16 anni , con precedenti di psoriasi eczematoide e di cefalea gravativa subcontinua a sede fronto - temporale , giunge presso la clinica neurologica per linsorgenza di emiparesi facio - brachio - crurale . 
la tc dellencefalo dimostra la presenza di empiemi multipli sia subdurali che extradurali , associati a marcati fenomeni flogistici delle cavit sinusali paranasali a livello frontale , etmoidale e mascellare . 
la successiva indagine rm dellencefalo mette in evidenza unarea di alterato segnale nel contesto dello splenio del corpo calloso , priva di enhancement , di dubbio significato demielinizzante o neoplastico astrocitario in fase iniziale . 
si decide pertanto di sottoporre la paziente a ulteriori accertamenti diagnostici clinico - laboratoristici . caso 4 caso 5 area of altered signal with no contrast enhancement in the splenium of the cc , which was suspected to be a demyelination - related lesion or an early stage astrocytoma . 
 a 34 - year - old man presenting with a 4 - day history of high fever and chills and vomiting underwent an emergency ct scan , which yielded negative results . 
the mri exam failed to show any sign of infectious disease , the only significant finding being a small area of altered signal in the splenium of the cc similar to the one described in the other cases . 
 un uomo di 34 anni con febbre elevata da 4 giorni associata a brividi e , successivamente , a vomito , viene ricoverato presso la divisione di medicina generale dellospedale civile di olbia , dove una tc dellencefalo fornisce esito negativo . 
presenza di empiemi in regione frontale dopo iniezione di mdc paramagnetico ( c )  . fatta eccezione per unarea di alterato segnale localizzata nello splenio del corpo calloso , priva di impregnazione dopo mdc . 
il paziente prosegue quindi il ricovero per essere sottoposto a tutti gli ulteriori accertamenti diagnostici del caso . caso 6 una ragazza di 17 anni , con storia di appendicite operata , lamenta da un mese deficit visivi , parestesie agli arti superiori , localizzate prevalentemente a destra e associate a cefalea . 
la paziente stata dunque ricoverata per ulteriori accertamenti . in tutti i pazienti le lesioni individuate a livello dello splenio del corpo calloso si sono rivelate focali , prive di enhancement dopo mdc e reversibili . 
i dati clinici sono stati analizzati retrospettivamente con particolare attenzione ai risultati laboratoristici e alla terapia medica effettuata da ogni singolo paziente al fine di cercare di determinare leziologia delle lesioni . 
in 4 pazienti le lesioni sono scomparse congiuntamente alla remissione completa della patologia di base , mentre in due pazienti le lesioni sono perdurate fino a 6 e 9 mesi di distanza dal primo rilievo . 
in 4 pazienti , i valori medi del coefficiente apparente di diffusione ( adc ) misurati a livello della lesione sono risultati di a 17 - year - old girl with a clinical history of surgery for appendicitis presented with a 1 - month history of visual deficiency , upper limb paraesthesia particularly on the right side associated with headache . 
she was then hospitalised for further clinical investigations . risultati in all patients , the lesions detected in the splenium of the cc were transient , focal and with no contrast enhancement . clinical data were analysed retrospectively with special atm . 
3a - e axial fluid attenuated inversion recovery ( a ) , t2 ( b ) and diffusion - weighted ( c ) images show a well - defined focal high signal with low signal in the adc map ( e )  . 
3a - e nel contesto dello splenio del corpo calloso le immagini flair ( a ) , pesate in t2 ( b ) e diffusione ( c ) mostrano una lesione iperintensa , focale e ben definita , con basso segnale nella mappa adc ( e ) e senza un definito enhancement dopo iniezione di mdc paramagnetico ( d )  . tention to the laboratory findings and type of medical treatment received with the aim of identifying the aetiology of such lesions . 
in four patients , mean apparent diffusion coefficient ( adc ) values detected within the splenial lesion were 0.3810 - 3mm2 / s , lower if compared with adc values of frontal grey matter ( 0.9810 - 3mm2 / s ) , frontal white matter adc ( 0.9010 - 3mm2 / s ) and csf ( 3.4410 - 3mm2 / s )  . 
during follow - up , complete resolution of the splenial lesion corresponded to an increase in adc values to those of the frontal white matter ( 0.8610 - 3mm2 / s ) ( table 1 )  . the patient was admitted to the infectious disease ward and case 1 0 , 3810 - 3mm2 / s , inferiori se confrontati ai valori adc della sostanza grigia ( 0 , 9810 - 3mm2 / s ) , della sostanza bianca ( 0 , 9010 - 3mm2 / s ) frontali e del liquor ( 3 , 4410 - 3mm2 / s )  . 
nei controlli effettuati a distanza si evidenziava un recupero dei valori adc comparabili con quelli della sostanza bianca frontale ( 0 , 8610 - 3mm2 / s ) ( tabella 1 )  . caso 1 il paziente , ricoverato presso il reparto di malattie infettive , viene sottoposto a terapia con lovirax per circa una settimana . 
the first mri scan after 4 weeks demonstrated full normalisation of the splenium of the cc , a finding that was also confirmed by subsequent examinations after 8 and 12 weeks . 
a distanza di 4 settimane viene nuovamente eseguita una rm dellencefalo nella quale non appare pi evidente larea descritta a livello dello splenio del corpo calloso , quadro poi confermato anche nei successivi controlli a 8 e 12 settimane . caso 2 caso 3 il giorno successivo allindagine rm il paziente manifesta due episodi convulsivi generalizzati ; viene quindi trasferito nel reparto di rianimazione dove la terapia di base viene integrata con antibiotici aggiuntivi e barbiturici e al paziente praticata assistenza sotto il profilo respiratorio con controllo delle crisi immediato e remissione dello stato febbrile . il paziente quindi sottoposto nuovamente a una tc dellencefalo che si dimostra immodificata rispetto alla precedente . nei giorni seguenti si assiste a un progressivo recupero della forza a carico dellarto inferiore sinistro e alla ripresa della deambulazione . 
a 4 settimane di distanza la persistenza di alterazioni di lato a un esame eeg suggerisce lesecuzione di una indagine rm dellencefalo in cui , accanto a un residuo ascessuale in sede frontale destra , apprezzabile m . 
riesaminato a distanza di qualche mese , si evidenzia la scomparsa completa delle lesioni ascessuali nonch dellarea di iperintensit nel corpo calloso . nel corso di un breve ricovero presso listituto di clinica neurologica la paziente va incontro rapidamente a progressivo miglioramento della sintomatologia , per cui viene dimessa dopo qualche giorno . 
a distanza di 4 , 8 e 12 settimane la ripetizione dellindagine rm mostra un quadro sostanzialmente negativo , fatta eccezione per larea di alterato segnale evidenziata alla prima osservazione , che permane invariata . 
un ulteriore controllo a 3 mesi dallultima osservazione ( 6 mesi dallesordio ) evidenzia la scomparsa della lesione callosa . caso 4 caso 5 durante il ricovero si rileva una leucocitosi neutrofila allesame emocromocitometrico ; lesame del liquor non evidenzia parametri al di fuori della norma . 
gli esami rm dellencefalo ripetuti a 4 , 8 e 12 settimane , in linea con il dato clinico , danno esito negativo , evidenziando peraltro anche la scomparsa dellarea focale di iperintensit localizzata nello splenio del corpo calloso . to regain the ability to walk . 
four weeks later , the persistence of side alterations observed during an eeg prompted the performance of a second mri scan , which showed a residual abscess in the right frontal region associated with a reduction in size and conspicuity of the focal area in the splenium of the cc . 
 ( c ) immagine in t1 dopo iniezione di mdc . caso 6 la paziente mostra un rapido miglioramento clinico e il successivo controllo rm risulta pressoch sovrapponibile al precedente , con lesione dello splenio rimasta invariata . 
a tale proposito risulterebbe opportuna qualche considerazione . secondo quanto riportato da alcuni autori , la completa remissione clinica delle patologie di base conduce a una totale scomparsa delle lesioni [ 4 , 16 ] ; altri correlano tale evenienza a una modificazione del trattamento farmacologico , lesion , which appeared to be unchanged compared to the initial examination . 
after a further 3 months ( 6 months after symptom onset ) , another mri was performed , which demonstrated the complete disappearance of the splenial lesion . case 5 case 6 during hospitalisation , the patients blood tests revealed the presence of a neutrophil leucocytosis , but csf analysis was negative for pathogens . 
mri scans performed 4 , 8 and 12 weeks later were consistent with the clinical findings and presented no abnormalities , confirming normalisation of the focal area located in the splenium of the cc . the patient had a rapid clinical improvement , and the following mri scan was almost superimposable to the previous m . 
6a - e la lesione descritta nel contesto dello splenio del corpo calloso non appare pi apprezzabile nelle immagini pesate in flair ( a ) , t2 ( b ) , diffusione ( c ) e mappa adc ( e ) ; ( d ) t1 dopo iniezione di mdc paramagnetico . one with persistence of the splenial lesion . 
several pathological conditions such as tumours , ischaemia , leukodystrophy , multiple sclerosis , hiv - related encephalopathy and marchiafava - bigspecialmente nei pazienti epilettici , sia che questa si traduca in una interruzione definitiva del farmaco , sia che il farmaco stesso venga sospeso temporaneamente [ 13 , 17 ]  . 
nella nostra esperienza , i pazienti studiati non avevano precedenti di trattamento con farmaci antiepilettici , e , in due casi , le lesioni non sono scomparse congiuntamente alla remissione della sintomatologia . 
rimane dunque aperta la discussione su quanto tale reversibilit possa essere correlata a queste condizioni . altra importante caratteristica rappresentata dallassenza di definite manifestazioni neurologiche correlabili alle lesioni , aspetto questo tuttavia non ancora del tutto chiarito . 
questa ipotesi viene supportata dal fatto che sia nei nostri pazienti , sia in altri studi [ 17 , 18 ] , le lesioni focali perduravano anche a remissione clinica completa , tale che i pazienti sottoposti a controlli nel tempo si dimostravano assolutamente asintomatici . 
however , mri findings associated with these conditions appear to be different from those described in our patients or reported in literature , which present some major common features that make their detection peculiar , the most important of which is their particular transient nature . according to some authors , complete clinical regression of the underlying condition leads to the disappearance of these lesions [ 4 , 16 ] ; others correlate this event with changes in pharmacological treatment ( both temporary and permanent interruption of drug administration ) , especially in epileptic patients [ 13 , 17 ]  . 
in our experience , none of the patients had ever received antiepileptic drugs and , in two cases , the lesions did not disappear when the symptoms regressed , making the correlation between reversibility and symptom relief controversial . another important feature is represented by the lack of specific neurological symptoms related to the lesions , even if this aspect is still not completely clear . 
this hypothesis is supported by the fact that both in our patients and in the cases reported in the literature [ 17 , 18 ] , the focal lesion persisted even after full clinical remission when , during follow - up examinations , patients appeared to be asymptomatic . 
 [ 16 ] postulated that whereas in these patients multiple foci of parenchymal signal alteration on t2 and dw could have indeed been responsible for clinical manifestations , it is possible that such alterations had completely regressed before an mri scan could be performed , making their detection elusive . 
however , it is debatable whether the patient would benefit more from the maintenance of a treatment protocol targeting the underlying pathology or from therapy conversion aimed solely at improving mri findings , which are not connected with any symptowe believe that the disappearance of the lesions is not directly connected to any clinical change , especially considering the remission of symptoms . 
 in addition to reversibility and accompanying lack of symptoms , these lesions share further features : their focal shape and lack of contrast enhancement after injection of paramagnetic contrast mediuthere is stronger agreement on the latter characteristics in the literature . 
to date , there are no reports describing nonenhancing transient and focal lesions in the splenium of the cc unassociated with other abnormalities either in the white or in the grey matter . 
the aetiopathogenesis of these peculiar lesions is the [ 16 ] tuttavia ipotizzano che nei pazienti possano essere presenti foci multipli di alterazione del segnale nel parenchima cerebrale , in t2 e in diffusione , responsabili delle manifestazioni cliniche , ma che questi possano essere andati comunque incontro a remissione completa nel periodo antecedente lesecuzione dellindagine rm non risultando pertanto documentabili . 
tuttavia rimane da stabilire se il beneficio maggiore per il paziente sia quello di mantenere una terapia farmacologica rivolta a curare una patologia di base , interromperla o , ancora , variarla al fine di migliorare un quadro rm che non correlabile ad alcun aspetto sintomatologico . a nostro avviso , infatti , la scomparsa delle lesioni non corrisponde ad alcuna modificazione nella clinica dei pazienti , peraltro gi asintomatici , mentre una variazione nel trattamento farmacologico potrebbe avere ripercussioni sullandamento della patologia di base per la quale i pazienti con tali lesioni sono giunti allo studio rm . oltre alla reversibilit e alla presunta asintomaticit , queste lesioni sono accomunate dallaspetto focale e dallassenza di enhancement dopo somministrazione di mdc . 
su queste due caratteristiche gli autori appaiono pi concordi . non sono infatti riportati lavori in letteratura con descrizione di lesioni focali dello splenio del corpo calloso con carattere di reversibilit , associate ad altre aree di alterato segnale sia nella sostanza bianca che nella sostanza grigia e con assenza di enhancement dopo somministrazione di mdc paramagnetico . 
nella nostra esperienza , in nessuno dei pazienti studiati stato riscontrato un definito enhancement , in linea dunque con i dati riportati attualmente in letteratura . pi vivace , invece , sembra essere la querelle sulle ipotesi eziopatogenetiche e fisiopatologiche di queste particolari alterazioni . 
utile ricordare in primo luogo le varie patologie con le quali tali aspetti possono entrare in diagnosi differenziale : sm , neoplasie , infarto , leucodistrofia ed encefalopatia hiv - correlata possono presentare reperti simili allindagine rm , ma non mostrano quella reversibilit e quellassenza di enhancement caratteristiche invece dei quadri da noi descritti . 
it is useful to recall the diverse conditions that these lesions could mimic : multiple sclerosis , tumours , infarction , leukodystrophy and hiv - related encephalopathy could all yield similar findings on an mri scan but would not show reversibility or lack of contrast enhancement . 
acute disseminated encephalomyelitis is more likely to be multicentric and bilateral , and some foci may show a diffuse or weak uptake of contrast depending on the grade of activity . 
early stage vascular ischaemic lesions may appear similar , but they always leave their mark on the affected brain tissue . as stated , several hypotheses have been put forth to explain the genesis of such abnormalities . 
in addition , dilantin may interfere with the intestinal absorption of dietary folate , causing a deficiency that has been linked to encephalopathy , cerebellar atrophy , myelopathy and peripheral neuropathy [ 21 ]  . 
 [ 4 ] supposed that intramyelinic oedema or macromolecular or phlogistic cell infiltration may cause similar alterations in a particular region of the brain , namely , in the cc . 
in this phenomenon , an increase in central nervous system ( cns ) inflammatory cytokines , such as interleukin - 6 , may play an important role with regard to the pathogenesis leading to mitochondrial dysfunction with lactic acidosis in the cc [ 25 ]  . 
nevertheless , all these theories require further clarification that , according to the authors , could be provided by future studies utilising mr spectroscopy techniques . a different hypothesis has been put forward by mirsattari et al . 
according to their view , such an abrupt withdrawal of pharmaceutical treatment could generate a hydric imbalance linked to alteration of the arginine - vasopressin ( avp ) syste it has been demonstrated that the avp system mediates regional cerebral flow [ 27 ] , affects brain hydric content and possibly plays a role in generating oedema [ 28 , 29 ]  . 
carbamazepine may potentiate avp antidiuretic effects [ 31 , fondamentale nella genesi di tali lesioni , pur riconoscendo che il meccanismo attraverso il quale queste vengono a formarsi ancora poco chiaro . 
inoltre il farmaco potrebbe interferire con lassorbimento intestinale di folati , il cui deficit stato collegato a encefalopatia , atrofia cerebellare , mielopatia e neuropatia periferica [ 21 ]  . 
secondo studi sperimentali , nei trattamenti a lungo termine anche la vigabatrina sarebbe responsabile di un edema intramielinico della sostanza bianca , reversibile in poche settimane dopo la sospensione del farmaco senza effetti residui [ 2224 ]  . 
 [ 4 ] suppongono che un edema intramielinico o un infiltrato flogistico di cellule infiammatorie e macromolecole possano produrre questo tipo di lesione in unarea preferenziale dellencefalo , identificata per lappunto nello splenio del corpo calloso , ipotizzando una specifica affinit dei recettori degli assoni dello splenio per antigeni virali . 
in tale meccanismo sembra possa giocare un ruolo laumento delle citochine infiammatorie del snc ( il - 6 ) che producono una disfunzione mitocondriale con conseguente acidosi lattica a livello dello splenio [ 25 ]  . 
ci verrebbe indotto attraverso un meccanismo di adattamento organico a seguito di una prolungata terapia con farmaci antiepilettici , la cui brusca interruzione provocherebbe degli squilibri nel bilancio idrico dovuti ad alterazioni nel sistema vasopressinaangiotensina ( avp )  . 
 stato dimostrato che il sistema avp regola il flusso cerebrale regionale [ 27 ] , influenza il contenuto di acqua nellencefalo e pu contribuire alla formazione delledema [ 28 , 29 ]  . 
 [ 26 ] , potrebbe indurre un aumento dei livelli serici dellavp con una conseguente alterazione dellequilibrio idrico encefalico che provocherebbe un edema citotossico in una regione vulnerabile come lo splenio del corpo calloso vascolarizzato solamente da rami terminali delle arterie cerebrali posteriori . 
this alteration would in turn induce cytotoxic oedema in a vulnerable region like the splenium of the cc , which is supported only by the terminal branches of posterior cerebral arteries . 
according to the authors , the reversible t2 signal hyperintensity of the white matter without simultaneous grey matter involvement strongly suggests that vasogenic oedema may precipitate such lesions [ 33 ]  . 
in fact , white matter , which has a lower fibre density , offers weaker resistance to oedema compared with grey matter , which is conversely more sensitive to the imbalance between energy demand and relative response and is more likely to be affected by cytotoxic oedema shown on t1 - weighted sequences [ 34 ]  . 
further evidence of this theory is provided by the fact that cytotoxic oedema does not respond to steroid therapy as does vasogenic oedema [ 35 ] , which leaves the brain tissue unaffected after resolution . 
an explanation for this pathogenic mechanism may be a blood - brain barrier alteration due to a cerebral capillary hydrostatic pressure increase , which is commonly observed in conditions such as hypertensive encephalopathy , preeclampsia , seizures , acute intermittent porphyria , toxic effects of cyclosporine , and migraine [ 3638 ]  . 
several factors may interfere with the complex balance of the bloodbrain barrier , such as neurotransmitters and neuromodulators , cyclic nucleotides , nitric oxide , histamine , and cytokines and other factors released by the interaction of white cells and endothelium [ 3941 ]  . 
some of these might be altered as a result of a hypoxemic condition [ 42 ] , and others , such as atrial natriuretic peptide , may be affected by acute mountain sickness [ 43 , 44 ]  . 
 [ 10 ] most closely resemble our own view , namely that transient focal lesions in the splenium of the cc described in our five patients may be related to vasogenic oedema which , albeit through complex and diverse mechanisms , represents the final common denominator among several pathological conditions . 
to validate this theory , in four patients , we detected low mean adc values within the splenial lesion , lower if compared with adc values of frontal grey matter , frontal white matter and csf . mean adc increased to normal values on subsequent examinations ( table 1 )  . conclusions transient signal alterations in the splenium of the cc detectsolo uno su cinque stato trattato con gardenale . 
 [ 10 ] descrivono la presenza di lesioni focali transitorie nello splenio del corpo calloso con le medesime caratteristiche rm da noi descritte in pazienti con edema cerebrale da altitudine . 
secondo gli autori la reversibile iperintensit di segnale in t2 della sostanza bianca senza contemporaneo coinvolgimento della sostanza grigia , suggerisce fortemente che ledema vasogenico sia il fattore alla base di tali lesioni [ 33 ]  . 
la sostanza bianca infatti , avendo una minor densit di fibre , offre una minore resistenza alledema di quanta ne esprima la sostanza grigia , che invece si dimostra pi sensibile allo squilibrio tra richiesta di energia cellulare e relativo apporto , andando quindi incontro pi facilmente alledema citotossico maggiormente apprezzabile su sequenze t1 pesate [ 34 ]  . 
unulteriore evidenza di quanto descritto fornita dal fatto che ledema citotossico non risponde alla terapia steroidea , a differenza di quello vasogenico [ 35 ] che tende inoltre a lasciare integro , senza reliquati , il parenchima encefalico dopo il suo riassorbimento . 
la spiegazione di tale meccanismo patogenetico potrebbe essere ricercata in unalterazione della barriera ematoencefalica per aumento della pressione idrostatica capillare a livello cerebrale , come osservabile in condizioni quali lencefalopatia ipertensiva , la tossiemia in gravidanza , le crisi epilettiche , la porfiria acuta intermittente o gli stati tossici da ciclosporine [ 3638 ]  . 
il complesso equilibrio della bee pu essere influenzato da diversi fattori quali neurotrasmettitori e neuromodulatori , ossido nitrico , istamina , citochine e altri , rilasciati dallinterazione tra globuli bianchi ed endotelio [ 3941 ]  . 
alcuni tra questi risultano alterati nelle condizioni di ipossia [ 42 ] mentre altri , quali lormone natriuretico atriale , possono risultarlo in corso di malessere acuto da altitudine [ 43 , 44 ]  . tra tutte le ipotesi eziopatogenetiche formulate , quelle proposte da hackett et al . 
 [ 10 ] sembrano coincidere maggiormente con la nostra linea di pensiero , secondo la quale le lesioni focali transitorie dello splenio descritte nei 6 pazienti possono essere ricondotte a una condizione di edema vasogenico che , attraverso i pi svariati e complessi meccanismi , potrebbe rappresentare lespressione ultima comune di condizioni patologiche differenti . 
a supporto di tale ipotesi vi il rilievo , in 4 pazienti , a livello della lesione , di bassi valori di adc , inferiori sia a quelli della sostanza grigia che della sostanza bianca frontali e del liquor , e la loro successiva normalizzazione nei controlli a distanza ( tabella 1 )  . conclusioni le alterazioni transitorie del segnale nello splenio del corpo calloso in corso di esami rm dellencefalo sono divenute , nellultimo decennio , un reperto sempre pi frequentemente descritto da numerosi autori . 
ci che nella letteratura stessa appare ancora estremamente variabile la formulazione univoca di unipotesi di natura , date le molteplici condizioni patologiche nel corso delle quali tali alterazioni vengono riscontrate . 
however , none of the patients in our study had undergone antiepileptic treatment , and similar lesions have been detected in patients affected by a wide spectrum of substantially different diseases . 
further research is therefore needed to identify common pathophysiological mechanisms . it seems reasonable to believe that through multiple and complex mechanisms , a number of pathological conditions can create a particular organic situation responsible for the imaging findings , which amount to the final common expression of different pathogenetic factors . 
as described , seizures , antiepileptic drugs , cerebral infections or high - altitude sickness all interfere with the function of the avp system , leading to vasogenic oedema characterised by an mri signal alteration in the splenium of the cc . 
this view explains the lesions transience , as the interruption of the noxa patogena ( seizures , antiepileptic drugs , infection ) leads to the progressive reduction and ultimate disappearance of the abnormal finding . 
in our opinion , this aetiopathogenetic explanation also better accounts for other features , such as the lack of symptoms , the focal shape of the lesions and the absence of contrast enhancement . the area in which such lesions have been typically found may be linked to the anisotropic diffusion in the cc , which , as reported by neeraj et al . 
 [ 45 ] , could be ascribed to a combination of several factors , such as tighter packing of axons , less - permeable myelin sheaths , fewer obliquely oriented axons , altered radius of individual axons and the presence ( or absence ) of collagenous perivascular alae . 
 in conclusion , we believe that the transient focal lesions in the splenium of the cc are an expression of a common aetiopathogenetic denominator , namely , vasogenic oedema induced by multiple pathological conditions through a mechanism involving and affecting the blood - brain barrier . va maggior convergenza dopinione quella che fa riferimento allazione di alcuni farmaci antiepilettici . 
piuttosto arduo ritenere di per s alla base di una stessa lesione differenti fattori eziologici . sembrerebbe quindi opportuno rivolgere particolare attenzione alla ricerca di meccanismi fisiopatogenetici comuni . pi ragionevole ritenere , infatti , che una serie pi o meno ampia di condizioni patologiche contribuisca , attraverso i pi svariati e complessi meccanismi , a creare una particolare situazione organica responsabile della comparsa delle alterazioni descritte quale espressione ultima e comune di differenti fattori eziopatogenetici . 
come descritto in precedenza , le crisi epilettiche , i farmaci antiepilettici , le infezioni cerebrali o laltitudine vanno tutti a interagire con il sistema avp , inducendo un edema vasogenico che si esprime in unalterazione del segnale rm nello splenio del corpo calloso . 
ci spiega la reversibilit nel tempo delle lesioni , visto che al cessare della noxa patogena ( crisi , farmaco , infezione ) la lesione tende progressivamente a ridursi divenendo sempre meno apprezzabile per poi infine scomparire . 
 [ 45 ] , dalla combinazione di diversi fattori quali giunzioni assonali pi strette , guaine mieliniche meno permeabili o pi grosse , minore quantit di assoni orientati obliquamente o presenza nel corpo calloso di strutture diverse dalle guaine mieliniche . 
dagostino5 1department of oncology , surgical unit , universit di palermo , policlinico universitario , via del vespro 129 , i - 90127 palermo , italy 2department of radiology domenico noto , hospital of sciacca , via pompei , i - 92019 sciacca , italy 3department of pathology , 4department of surgery , 5department of radiological sciences , universit di palermo , policlinico universitario , via del vespro 129 , i - 90127 palermo , italy correspondence to : f . 
ph monitoring showed sensitivity of 71% , specificity of 31% , positive predictive value ( ppv ) of 53% and negative predictive value ( npv ) of 50% ; when middle - proximal refluxes only were considered , sensitivity decreased to 45% and specificity increased to 55% . 
furthermore , the association between reflux and oesophagitis demonstrated by the chi - square ( 2 ) test proved to be statistically significant both for wst and ph monitoring , whereas the association between reflux and barretts oesophagus was not significant for either wst or for ph monitoring . 
ph - metria ha presentato sensibilit del 71% , specificit del 31% , valore predittivo positivo ( ppv ) del 53% e valore predittivo negativo ( npv ) del 50% ; la sua specificit aumenta ( 55% ) considerando solamente i reflussi medioprossimali , ma diminuisce la sensibilit ( 45% )  . 
il wst un test semplice e poco costoso , facilmente realizzabile , che pu essere utile nella diagnosi di gerd ; la sua positivit pu essere un indicatore per selezionare i pazienti da avviare allendoscopia con biopsia . parole chiave water siphon test reflusso gastroesofageo ph - metria studio baritato dellesofago e . 
twentyfour - hour ph monitoring is generally considered the gold standard for detection of acid gastroesophageal reflux [ 36 ]  . nevertheless , its use is limited , as it is invasive , expensive , time consuming , not always easily tolerated by the patients and not always readily available [ 7 ]  . 
oesophageal endoscopy is usually performed when severe symptoms are present or when a complication is suspected and systematic biopsies must be taken to confirm oesophagitis , or to detect barretts oesophagus [ 9 ]  . 
radiological reflux evaluation , which was proposed in the early 1950s , is also used to diagnose the morphological aspects of the disease , such as stenosis and the presence of hiatal hernia ( hh ) [ 10 , 11 ]  . however , barium studies have generally been considered insensitive for reflux detection as an event which correlates to the disease , and associated provocative manoeuvres , such as the water siphon test ( wst ) , have been thought to overestimate reflux when compared with ph monitoring [ 1214 ]  . 
several other reports indicate that radiological evaluation can be used as a screening test when gastroesophageal reflux is suspected and its sensitivity and specificity are increased by the use of wst [ 1518 ]  . 
in addition , comparison was made between results of wst and ph monitoring with regards to the possibility of identifying subjects with gerd complicated by oesophagitis , barretts oesophagus or intestinal metaplasia . materials and methods patients we reviewed a series of 160 patients , 77 men and 83 women , with ages ranging from 1974 ( mean 44 ) years referred to the oesophageal surgery unit between january 2002 and december 2005 for evaluation of suspected gerd . 
solitamente , nel sospetto di gerd , vengono utilizzati test diagnostici quali lendoscopia e la ph - metria [ 2 ] , questultima considerata il gold standard per lindividuazione di reflusso gastroesofageo acido [ 36 ]  . 
tuttavia limpiego della ph - metria limitato a causa della sua invasivit , del suo costo , della sua durata , della scarsa tolleranza e della ridotta disponibilit sul territorio [ 7 ] ; inoltre la ph - metria pu misurare lesposizione acida della mucosa esofagea ma non pu rilevare gli episodi di reflusso con ph > 4 ( cio reflusso non acido ) e , per questo , non si pu considerare un test perfetto [ 8 ]  . 
lendoscopia esofagea viene riservata a pazienti con sintomi severi o con sospette complicanze della malattia da reflusso quali lesofagite e / o lesofago di barrett , per la cui diagnosi necessario effettuare biopsie multiple della mucosa [ 9 ]  . 
la valutazione radiologica , che fu proposta sin dallinizio degli anni cinquanta , solitamente usata per diagnosticare le alterazioni morfologiche della malattia , quali stenosi ed esofagiti , e la presenza di ernia iatale [ 10 , 11 ]  . 
lo studio con bario stato generalmente considerato scarsamente sensibile per la rilevazione di reflusso come evento correlato alla malattia ; inoltre si considera che le manovre di provocazione associate , come il water siphon test ( wst ) , sovrastimino il reflusso rispetto alla ph - metria [ 1214 ]  . 
tuttavia , parecchi altri lavori indicano che lo studio radiologico pu essere usato come test di screening nel caso di sospetto di reflusso gastroesofageo e che il wst incrementi i valori di sensibilit e di specificit dellesame [ 1518 ]  . 
 materiali e metodi pazienti abbiamo effettuato una valutazione retrospettiva della nostra serie di 160 pazienti 77 uomini e 83 donne con et compresa tra 19 e 74 anni ( et media : 44 anni ) , avviati allunit di chirurgia esofagea fra gennaio 2002 e dicembre 2005 per sospetta gerd . 
after an overnight fast , patients were given two mouthfuls of barium sulphate suspension ( 60% weight / volume ) in the upright left oblique posterior and in the prone right oblique anterior projections with a bolster placed under the abdomen . 
the patients were then asked to lie on their left side for 30 s , and wst was performed with the patients lying supine while continuously drinking 80 ml of water through a straw and rolling from the supine to the right lateral position . 
grading was as follows : distal ( refluxed column of barium in the lower 5 cm of the oesophagus ) , middle ( reflux up to the tracheal carrefour ) and proximal ( reflux up to pharyngoesophageal junction )  . motility study all motility studies were performed by one of the authors . oesophageal manometry was performed transnasally using an appropriate probe ( marquat c47 ) with an open - ended tip and four radial paths with a bearing point every 5 cperfusion equipment included a nitrogen infusion pump ( model 745 - 0100 , international biomedical inc ) , and data were recorded by an autocalibrating polygraph ( narco bio system mms 200 ) connected to a pc by software for automatic data analysis . 
manometric findings of this condition were two pressure peaks , intrathoracic pressure inversion point , short oesophagus , variable plateau pressure , dystonic high - pressure zone ( hypoor hypertonic ) and double respiratory reversal . twenty - four - hour ph monitoring all ph studies were performed by one of the authors . 
patients underwent 24 - h ambulatory ph monitoring after an overnight fast ; any medication such as prokinetics or proton pump inhibitors ( ppi ) were suspended for at least 7 days before the test . 
after standard calibrations at 37c in ph 7 and ph 1 buffer solutions , the ph catheter was inserted nasally in order to place the proximal electrode 5 cm above the manometrically determined proximal border of the lower oesophageal sphincter and the distal electrode in the proximal stomach . 
during the 24 - h period of ph tro 2 settimane e sono state interpretate indipendentemente e senza alcuna conoscenza dei risultati degli altri test . cineradiografia digitale e water siphon test tutti gli studi dinamici con bario ( cineradiografia ) sono stati eseguiti da due autori impiegando un telecomandato digitale con arco a c ( polifunzionale eurocolumbus tr3d , milano , italia ) con intensificatore di brillanza da 16 pollici e con sequenze di acquisizione di 6 immagini al secondo con matrice 5121024 , secondo una tecnica standardizzata . 
dopo 12 ore di digiuno sono stati somministrati ai pazienti due sorsi di sospensione di solfato di bario 60% peso - volume rispettivamente in posizione ortostatica e proiezione obliqua anteriore destra e in posizione prona e in proiezione obliqua posteriore sinistra dopo posizionamento di un piccolo cuscino radiotrasparente sotto laddome . 
dopo circa 30 secondi di decubito sul fianco sinistro veniva eseguito il wst : il paziente , in posizione supina , assumeva in modo continuato da una cannuccia circa 80 ml di acqua , passando poi dalla posizione supina al decubito laterale destro . 
i reperti manometrici di questa condizione erano il doppio picco pressorio , il punto di inversione della pressione toracica , lesofago corto , il variabile plateau pressorio , la zona di alta pressione distonica ( ipotonica o ipertonica ) , la doppia inversione respiratoria . ph - metria 24 ore tutti i test ph - metrici sono stati eseguiti da uno degli autori . i pazienti sono stati sottoposti a ph - metria 24 ore durante un ricovero in day hospital e dopo un digiuno di almeno 12 ore ; tutti i trattamenti farmacologici , con procinetici e / o inibitori di pompa protonica , sono stati sospesi per almeno 7 giorni prima del test . 
 endoscopy all endoscopic procedures were performed by one of the authors using an olympus videoendoscope ( gif q160 , tokyo , japan ) following the same criteria for all examinations . 
the squamous - columnar junction was identified and the normal z - line or the presence of columnar - lined oesophagus , suspected barretts oesophagus , short ( tongued or < 3 cm ) or long ( 3 cm ) segment , were defined . 
in all patients , four - quadrant biopsies from the distal oesophageal mucosa , at least 1 cm proximal to the gastroesophageal junction , were taken when a normal z - line was identified , and multiple biopsies of the long or short columnar - lined mucosa were performed to detect intestinal metaplasia ( im ) to determine barretts oesophagus . 
four - quadrant biopsies were also taken from the columnar mucosa at least 1 cm distal to the gastroesophageal junction , but the results are beyond the scope of this study . 
all biopsies were immediately fixed in 10% buffered formalin , numbered and sent to the same pathologist , who was unaware of the endoscopic diagnosis . histological analysis all histological analyses were performed by one of the authors . 
all the biopsy samples were fixed in 10% buffered formalin and embedded in paraffin and 5 - m sections were obtained and stained with haematoxylin - eosin and alcian blue periodic acid - schiff to identify goblet cells . 
histological criteria for evidence of reflux oesophagitis included one of the following findings : increase in the basal cell layer thickness > 20% , papillae extending through more than 66% of the epithelial thickness , presence of balloon cells , neutrophils ( > 15 high power field ) or eosinophils , dilatation and congestion of capillary vessels and intraepithelial haemorrhage . 
im was defined as the presence of intestinal - type goblet cells . statistical analysis data were analysed using the sas / stat 8.0 package ( sas institute inc . , cary , nc , usa )  . 
sensitivity , specificity and positive ( ppv ) and negative ( npv ) predictive values of the wst in revealing the possible presence of gastroesophageal reflux were calculated using ph monitoring as the gold stanin antimonio distanziati 15 cm luno dallaltro e un elettrodo di riferimento interno ( zinetics 24 , medtronic , italia )  . 
dopo calibrazione in soluzioni tampone a ph 7 e a ph 1 , il catetere stato inserito per via nasale in modo da posizionare lelettrodo prossimale 5 cm sopra il bordo superiore dello sfintere esofageo inferiore , identificato manometricamente , e lelettrodo distale nello stomaco prossimale . 
durante il periodo di 24 ore di monitoraggio del ph , il paziente veniva mandato a casa e invitato a prendere nota di eventuali sintomi , degli orari dei pasti , di riposo e di risveglio , e comunque incoraggiato a svolgere le proprie attivit giornaliere . 
i dati registrati , scaricati in un pc e analizzati dai programmi specifici multigram gi edition 94 o polygram net , forniti da medtronic italia , sono stati inseriti in una tabella di punteggio ( demeester score ) e un punteggio superiore a 14 , 8 fu considerato anormale [ 3 ]  . 
 endoscopia tutte le procedure endoscopiche sono state eseguite da uno degli autori utilizzando un videoendoscopio olympus ( gif q160 , tokyo , giappone ) e seguendo lo stesso criterio per tutti gli esami . 
per la classificazione delle esofagiti stata utilizzata la classificazione endoscopica di los angeles [ 19 ]  . stata identificata la linea z normale o la presenza di mucosa colonnare estendentesi al di sopra della giunzione gastroesofagea , sospetta per esofago di barrett corto ( a fiamma o < 3 cm ) o lungo ( 3 cm )  . 
in presenza di una linea z normale sono state eseguite 4 biopsie nella mucosa dellesofago distale ( una per quadrante almeno a distanza di un centimetro , prossimali alla giunzione gastroesofagea ) ; in presenza di mucosa colonnare estendentesi prossimalmente alla giunzione gastroesofagea , sono state eseguite biopsie multiple per confermare istologicamente lesofago di barrett . 
tutte le biopsie sono state fissate in formalina tamponata al 10% , numerate e inviate allo stesso patologo , ignaro della diagnosi endoscopica . analisi istologica tutte le analisi istologiche sono state eseguite da uno degli autori . 
tutti i campioni bioptici sono stati fissati in formalina tamponata al 10% , inclusi in paraffina , e le sezioni di 5 micron ottenute sono state colorate con ematossilina - eosina e alcian blue periodic acid - shiff per identificare le cellule goblet . 
i criteri istologici di evidenza di esofagite da reflusso includevano uno dei seguenti parametri : incremento > 20% dello spessore dello strato basale , altezza delle papille > 66% dello spessore epiteliale , presenza di cellule balloon , neutrofili ( > 15 high power field ) o eosinofili , dilatazione e congestione dei capillari , emorragie intraepiteliali . 
sensitivity , specificity and npv and ppv of wst and ph monitoring in revealing the possible presence of oesophagitis ( gold standard : endoscopy ) , barretts oesophagus ( gold standard : endoscopy + biopsy ) and im ( gold standard : histological analysis ) were then calculated . 
ph monitoring wst was positive in 112 patients ( 70% ) , but only 59 / 112 ( 52.67% ) also had positive ph monitoring ; furthermore 24 / 48 patients with a negative wst had a positive ph monitoring ( table 1 )  . 
of the 112 patients with a positive wst , 72 had middle ( 44 / 72 ) and proximal ( 28 / 72 ) reflux , but only 37 of these had positive ph monitoring . 
ph monitoring in the diagnosis of oesophagitis sixty - one out of 160 patients had endoscopic findings of complicated gerd such as oesophagitis also associated to table 1 water siphon test ( wst ) vs . 
ph - metria 24 ore numero di test ph - metria positivi negativi wsta positivi wsta negativi wstb positivi a , considerati globalmente ; wstb , solo reflussi medi e prossimali endoscopico , stata definita dalla presenza di cellule intestinali tipo goblet . 
 analisi statistica i dati sono stati analizzati impiegando il pacchetto software sas / stat 8.0 ( sas institute inc.100 sas campus drive cary , nc27513 - 2414 , usa )  . 
sono stati calcolati i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) del wst , rispetto alla ph - metria ( gold standard ) , ai fini della individuazione del reflusso gastroesofageo . 
inoltre sono stati calcolati i valori di sensibilit , specificit valore predittivo , positivo e negativo di wst e ph - metria nella individuazione di possibile presenza di esofagite ( gold standard : endoscopia ) , di esofago di barrett ( gold standard : endoscopia con biopsia ) e di metaplasia intestinale ( gold standard : esame istologico )  . 
stato infine eseguito il test del chi - quadro per valutare lattendibilit statistica dellassociazione tra presenza di reflusso dimostrato al wst e alla ph - metria con presenza di esofagite , esofago di barrett e metaplasia intestinale ; stato considerato statisticamente significativo un valore di p0 , 05 . risultati in tutti i pazienti sottoposti a cineradiografia digitale era presente unernia iatale . 
ph - metria centododici pazienti presentavano un wst positivo ( 70% ) , ma solamente 59 di questi ( 52 , 67% ) avevano anche una phmetria positiva ; inoltre 24 dei 48 pazienti con wst negativo avevano una ph - metria positiva ( tabella 1 )  . 
settantadue dei 112 pazienti con wst positivo avevano un reflusso medio ( 44 pz ) o prossimale ( 28 pz ) , ma solamente 37 presentavano una ph - metria positiva . 
considerando solamente i pazienti con reflusso medio e prossimale al wst , la sensibilit diminuisce ( 45% ) ma la specificit aumenta ( 55% )  . sessantuno dei 160 pazienti avevano segni endoscopici di malattia da reflusso complicata da esofagite anche associata a esofago di barrett : 48 / 61 di questi pazienti avevano un wst positivo mentre solamente 42 avevano una ph - metria positiva come mostrato in tabella 2 . 
nel confronto tra la capacit di wst e ph - metria di individuare i pazienti con esofagite , avendo come gold standard lendoscopia , si rileva che il wst ( considerati tutti i pazienti positivi ) mostra una sensibilit maggiore ( 79% ) ma valori di specificit ( 35% ) , vpp ( 43% ) e vpn ( 73% ) inferiori rispetto alla ph - metria ; qualora poi si a , considered overall ; wstb , considering only middle and proximal refluxes wst vs . 
vpp , valore predittivo positivo ; vpn , valore predittivo negativo . sensitivity % specificity % ppv % npv % wst overall ph monitoring wst middle / proximal accuracy of wst and ph - monitoring in patients with barretts esophagitis accuratezza del wst e della ph - metria in pazienti con esofago di barret sensitivity % specificity % ppv % npv % wst overall ph monitoring wst middle / proximal fig . 
vpp , valore predittivo positivo ; vpn , valore predittivo negativo . barretts oesophagus : 48 out of 61 patients with complicated gerd had a positive wst , whereas 42 had positive ph monitoring ( table 2 )  . 
if the presence of oesophagitis at endoscopy was considered as evidence of gerd , wst , considered overall , showed a higher sensitivity ( 79% ) but lower specificity ( 35% ) , ppv ( 43% ) and npv ( 73% ) than did ph monitoring . 
in this group of 24 patients with considerino solamente i reflussi medio - prossimali la sensibilit diminuisce ( 61% ) , ma la specificit ( 65% ) il vpp ( 51% ) e il vpn ( 73% ) aumentano , come mostrato in figura 1 . 
in questo gruppo di 24 pazienti , con presenza di mucosa colonnare allendoscopia , esofago di barrett corto o lungo , e presenza di metaplasia intestinale allesame istologico , il wst risultato positivo in 21 pazienti , mentre la ph - metria risultava positiva solamente in 13 pazienti come mostrato in tabella 2 . 
la valutazione statistica del wst fa rilevare valori di sensibilit ( 88% ) , vpp ( 19% ) e vpn ( 94% ) superiori alla ph - metria ma valoe . 
vpp , valore predittivo positivo ; vpn , valore predittivo negativo . endoscopic findings of either long or short columnar - lined mucosa and im findings at histological analysis , wst was positive for reflux in 21 , whereas ph monitoring was positive for reflux in 13 only , as shown in table 2 . 
overall , statistical analysis of wst showed higher sensitivity ( 88% ) , ppv ( 19% ) and npv ( 94% ) and lower specificity ( 33% ) than did ph monitoring . 
considering only middle and proximal reflux at wst , sensitivity decreased ( 54% ) , but specificity increased and was higher ( 57% ) than ph monitoring ( 49% ) , as shown in figure 2 . 
overall in this group of patients , wst showed a higher sensitivity ( 89% ) , ppv ( 36% ) and npv ( 90% ) and lower specificity ( 37% ) than did ph monitoring , but considering only middle and proximal reflux , statistical analysis of wst showed all values higher than ph monitoring , as shown in figure 3 . 
assumendo come popolazione di controllo i pazienti risultati negativi allesame endoscopico e applicando il test del chi - quadro , il wst ( reflusso medio - possimale ) rileva reflussi statisticamente correlati ( p = 0 , 002 ) alla presenza di metaplasia intestinale mentre lo stesso non avviene per la ph - metria ( p = 0 , 3014 ) discussione si ritiene che la diagnosi di gerd possa essere fatta sulla e . 
recently , however , different tests ( 24 - h ph monitoring , endoscopy , radiological study , etc . ) have commonly been used for this frequent disorder , each providing information regarding a different aspect of the disease . 
it is our opinion that in patients with symptoms of gerd , the presence of hh should always be investigated . cineradiography is a noninvasive , useful and reliable test to define the anatomical disorder of the gastroesophageal junction , which , in our own study , was confirmed in 95% by one test only ( motility study or endoscopy ) and in 83% by two tests ( motility study and endoscopy )  . 
 the results of this study demonstrate that wst can be useful for the detection of gastroesophageal reflux , even though it must be borne in mind that it only accounts for a mechanical event and does not provide any information about the chemical changes in the oesophagus . 
taking a positive ph study as evidence of reflux , the sensitivity of wst in predicting gerd is high when considered from an overall point of view , but specificity increases only when middle and proximal refluxes are considered , even though sensitivity decreases . 
nevertheless , the finding of 25% of complicated gerd at endoscopy in patients with a positive wst and negative ph monitoring for reflux clearly shows that ph monitoring is not a perfect standard . 
these data show that rabase della storia clinica del paziente ed generalmente accettato che possa essere indicativa per gerd la risposta positiva alla terapia con farmaci inibitori di pompa protonica . nella diagnosi di gerd , sono stati impiegati test differenti ( ph - metria 24 ore , endoscopia , studio radiologico , ecc . ) ognuno dei quali d informazioni diverse rispetto a differenti aspetti della malattia . 
nostra opinione che , nei pazienti con sintomi di gerd , debba essere sempre ricercata la presenza di ernia iatale , e che lesame radiologico sia un test utile , non invasivo , ma attendibile nel definire lalterazione anatomica della giunzione gastroesofagea ; infatti , nel nostro studio , la diagnosi radiologica di ernia stata confermata nel 95% dei casi da un solo test ( manometria o endoscopia ) e nell83% dei casi da due test ( manometria ed endoscopia )  . i risultati di questo studio dimostrano come il wst possa essere utile nella diagnosi di reflusso gastroesofageo , anche se va tenuto presente che il test , quando positivo , rappresenta solamente levento meccanico del reflusso non fornendo , peraltro , alcuna informazione sulle variazioni chimiche allinterno del lume esofageo . 
assumendo come gold standard per reflusso la positivit alla ph - metria , il wst , globalmente considerato , presenta una elevata sensibilit , ma la specificit aumenta soltanto quando sono considerati come positivi i reflussi medio - prossimali anche se , in questo caso , la sensibilit diminuisce . 
tuttavia , il riscontro di 25% di gerd complicata allendoscopia in pazienti con wst positivo e ph - metria negativa per reflusso indica chiaramente che la ph - metria non un test perfetto . 
one study reported 92% sensitivity 0% specificity [ 20 ] , whereas another reported quite different values , with sensitivity at 70% and specificity at 74% [ 21 ]  . 
this fact would also seem to be confirmed by another recently published study [ 22 ] , which , however , took into consideration only 28 patients with refluxes either at or above the thoracic inlet that were either spontaneous or induced by provocative manoeuvres in the recumbent position . 
in this group of patients , the radiological study showed specificity of 100% and sensitivity of 64% . the difference found in our study , with 45% sensitivity and 55% specificity , is due both to the larger number of patients involved and to the fact that we considered positive those with middle - proximal refluxes . 
 our experience , however , is similar to that reported in the recent literature with regard to the high reliability of a radiologically demonstrated proximal reflux in the diagnosis of gerd and in laryngopharyngeal reflux [ 23 ]  . 
if middle and proximal refluxes are considered , wst accuracy is similar to ph monitoring in predicting oesophagitis , with a significant association between reflux and oesophagitis both for wst and for ph monitoring . 
moreover , in our study , wst seemed more reliable than ph monitoring in predicting barretts oesophagus , even though we did not demonstrate a significant association between reflux demonstrated radiologically or with ph monitoring and this disease . 
fewer than 50% of patients had complicated gerd , showing that objective criteria are necessary to suspect and detect the complication . from this point of view , a highly positive wst might suggest endoscopy with biopsies to detect a complication of gerd , as suggested by the presence of 15% of barretts oesophagus and 13% of im in an endoscopically normal oesophageal mucosa . 
with regard to these conditions , wsts higher accuracy might be explained by the fact that im might be correlated to the presence of bile in the oesophageal refluxate , which might disguise the true acid exposure , resulting in false negative results at ph monitoring [ 8 ]  . 
uno studio ha riportato valori di sensibilit del 92% e di specificit pari a zero [ 20 ] , mentre un altro ha riportato valori totalmente differenti ( sensibilit del 70% , e specificit del 74% ) [ 21 ]  . 
questo dato sembra confermato anche da un recente lavoro [ 22 ] che ha preso in considerazione un campione , seppur piccolo , di 28 pazienti con reflusso fino allimbocco toracico , insorto spontaneamente o dopo test di provocazione . 
la differenza riportata nel nostro studio ( sensibilit del 45% e specificit del 55% ) da attribuire al campione pi ampio di pazienti e al fatto di avere considerato come positivi i pazienti con reflusso medio - prossimale . 
 la nostra esperienza simile a quanto riportato recentemente in letteratura riguardo alla elevata attendibilit di un reflusso prossimale radiologicamente dimostrato nella diagnosi di gerd in pazienti con reflusso laringo - faringeo [ 23 ]  . se si considerano come positivi solamente i reflussi medioprossimali , laccuratezza del wst simile a quella della phmetria nel predire lesofagite , con significativa associazione statistica tra reflusso ed esofagite sia per wst che per phmetria . 
inoltre nel nostro studio il wst sembra pi attendibile della ph - metria nel predire lesofago di barrett , anche se non possibile dimostrare una associazione statisticamente significativa tra reflusso dimostrato radiologicamente o con ph - metria e tale patologia . 
nella nostra casistica , tuttavia , meno del 50% dei pazienti ha avuto una gerd complicata , il che indica che sono necessari criteri oggettivi che facciano sospettare e rilevare la complicanza . 
 da questo punto di vista un wst altamente positivo potrebbe suggerire lindicazione a unendoscopia con biopsie per rilevare una gerd complicata , come dimostrato , nella nostra esperienza , dalla presenza nel 15% dei casi di esofago di barrett e nel 13% di metaplasia intestinale in esofago normale allendoscopia . 
in questi casi la maggiore accuratezza del wst potrebbe essere spiegata dal fatto che la metaplasia intestinale potrebbe essere correlata alla presenza di bile nel materiale refluito in esofago , con effetto tampone dellacido e conseguente risultato falsamente negativo alla ph - metria [ 8 ] ; di contro il wst , mostrando il reflusso del contenuto gastrico in esofago , rappresenta radiologicamente levento meccanico indipendentemente dalla sua componente chimica . conclusions in our opinion , wst is no substitute for 24 - h ph monitoring which , although more expensive , time - consuming and invapossiamo affermare che il wst non sostituisce la ph - metria 24 ore la quale , anche se pi costosa , pi lunga e pi invasiva , deve essere usata per valutazioni quali - quantitative sul conclusioni e . 
on the other hand , wst associated with the barium test could be used as a first choice in patients with suspected gerd , as it is an inexpensive , rapid and noninvasive procedure that is simple to perform , readily available , well tolerated by patients and correlates fairly well with symptoms of gerd . 
in our experience , wst , which shows gerd as a mechanical event , is more reliable than ph monitoring in predicting complicated gerd , especially when barium refluxes extending as far as the tracheal carrefour or the pharyngoesophageal junction are taken into account . 
in patients with symptoms of gerd , wst positive for reflux , especially if a middle or proximal one , might be an indication for endoscopy with multiple biopsies . reflusso ed essenziale in pazienti con presentazione atipica di gerd , in pazienti con insufficiente risposta alla terapia con inibitori di pompa protonica e in pazienti candidati allintervento chirurgico . 
per contro , lesame radiografico con wst pu essere utilizzato in pazienti con sospetta gerd come indagine di prima scelta in quanto procedura economica , veloce e non invasiva , semplice da effettuare , facilmente disponibile , ben tollerata dai pazienti e abbastanza ben correlata con i sintomi di gerd . 
nella nostra esperienza , il wst , che dimostra levento meccanico della malattia da reflusso , pi attendibile della ph - metria nel predire le complicanze della malattia , particolarmente quando il bario refluito si estende fino al carrefour tracheale o alla giunzione faringoesofagea . 
in pazienti con i sintomi di gerd , un wst positivo per reflusso , in particolare se medio - prossimale , potrebbe essere unindicazione per una endoscopia con biopsie multiple . 
fugazzola1 1cattedra di radiologia , 2chirurgia vascolare , 3servizio di anestesia , universit degli studi dellinsubria , azienda ospedalierouniversitaria ospedale di circolo e fondazione macchi , viale borri 57 , i - 21100 varese , italy correspondence to : d . 
between march 1999 and march 2004 , 15 isolated iaas in 13 patients ( mean age : 71.8 years ) were selected for endovascular repair by means of a covered stent or stent - graft : 12 were in the common iliac artery ( 2 with the proximal end 12 mm from the aortic bifurcation and 2 involving the distal hypogastric artery ) , and three were in the external iliac artery . 
follow - up ( mean duration : 25 months , range : 660 months ) in the remaining 11 patients , affected by 13 aneurysms , showed aneurysm exclusion in nine cases and progressive shrinkage of the aneurysmal sac in four cases , whereas in the other five , the size of the aneurysm remained unchanged . 
in a patient with bilateral iaa , bilateral proximal endoleaks were observed after 2 years , and the patient was treated with a bifurcated aortic stent - grain another patient with a large aneurysm , a left aortofemoral bypass became necessary after 2 months because of stent - graft dislodgement . 
however , a longer follow - up and larger patient series are needed to verify the long - term efficacy of this form of treatment . key words iliac aneurysm endovascular therapy arteries stents interventional procedures riassunto obiettivo . 
tra marzo 1999 e marzo 2004 sono stati selezionati per lesclusione endovascolare mediante stent ricoperto o endoprotesi 15 aneurismi isolati dellaai in 13 pazienti ( et media 71 , 8 anni ) : 12 dellarteria iliaca comune ( di cui 2 con estremo prossimale distante 12 mm dalla biforcazione aortica e 2 coinvolgenti distalmente larteria ipogastrica ) e 3 dellarteria iliaca esterna . 
il follow - up ( durata media 25 mesi , range 660 mesi ) , disponibile nei restanti 11 pazienti , portatori di 13 aneurismi , ha dimostrato lesclusione dellaneurisma in 9 casi , con la progressiva riduzione volumetrica della sacca in 4 , mentre negli altri 5 la sacca rimasta immodificata . 
in un paziente portatore di aneurismi isolati dellaai bilaterale si osservato un endoleak prossimale di entrambi gli aneurismi a 2 anni , trattato pertanto con endoprotesi aortica biforcata ; in una paziente con un voluminoso aneurisma si resa necessaria la conversione in by - pass aorto - femorale sinistro a due mesi di distanza per dislocazione di pi endoprotesi embricate ; in un paziente , infine , a due anni si rilevato un endoleak rifornito dallarteria ipogastrica , che non stato trattato . 
tuttavia necessario un follow - up pi protratto e una casistica pi numerosa per verificare lefficacia a lungo termine di questo tipo di trattamento . parole chiave aneurisma iliaco terapia endovascolare arterie stents procedure interventistiche introduction introduzione d . 
specific symptoms resulting from mural thrombosis with distal microembolism , rupture or local compression of venous and nervous structures and the urinary tract are relatively infrequent [ 46 ]  . although data on the natural history of isolated iaas are limited owing to the rare occurrence of these aneurysms , expansile growth and subsequent rupture has been documented by various authors [ 2 , 3 , 5 ]  . 
the treatment of choice for isolated aneurysms of the common or external iliac artery with diameter greater than 3 cm is surgical bypass grafting , even if the patient is asymptomatic [ 2 , 5 ]  . 
as occurs with abdominal aortic aneurysms , surgical repair of isolated iaas is considered major surgery , associated with mortality rates of 7%11% for elective procedures and 30%50% in emergency settings [ 5 ]  . 
 the purpose of this paper is to describe our experience in a series of 15 aneurysms involving the common and / or external iliac arteries in 13 patients treated with stent - grafts and to compare our results with those reported in the literature . materials and methods between march 1999 and march 2004 , 160 abdominal aortic and iliac aneurysms were treated by endovascular repair at our institution . 
in particular , 127 aneurysms were either aortic or aortoiliac ; 4 involved the hypogastric artery , 14 were anastomotic pseudoaneurysms ( 9 distal , 5 proximal ) and 15 were isolated iaas . 
the series considered in this study comprised 13 patients ( 10 men and 3 women ) aged between 55 and 91 years ( mean age 71.8 years ) with either unilateral or bilateral iaas selected for endovascular repair using stentgrafts ( table 1 )  . 
twelve were in the common iliac artery ( 2 in the proximal end 12 mm from the aortic bifurcation and 2 involving the distal hypogastric artery ) and 3 in the external iliac artery . 
hypogastric artery aneurysms ( n = 4 ) treated by coil embolisation upstream or downstream from the aneurysm without stent deployment were not considered in this study . two patients were treated as an emergency : one due to haemorrhagic shock following aneurysm rupture , and the othgli aneurismi isolati dellasse arterioso iliaco ( aai ) sono rari , rappresentando circa il 2%7% di tutti gli aneurismi addominali [ 13 ]  . 
la loro eziologia principalmente ateromasica ; le altre cause ( infettive ; in corso di gravidanza ; malattie del collagene come la sindrome di marfan ) sono assai meno frequenti . 
la maggior parte degli aneurismi isolati dellaai asintomatica e viene pertanto diagnosticata in maniera occasionale mediante ecografia , tomografia computerizzata ( tc ) o angiografia ; i sintomi specifici , conseguenti allo sviluppo di una trombosi murale con microembolia distale , alla rottura e alla compressione locale su strutture venose , nervose e vie urinarie , sono piuttosto infrequenti [ 46 ]  . bench i dati sulla storia naturale degli aneurismi isolati dellaai siano limitati a causa della loro relativa rarit , la crescita espansiva e la conseguente rottura stata documentata in diversi studi [ 2 , 3 , 5 ]  . 
il trattamento di scelta nella dilatazione aneurismatica isolata dellarteria iliaca comune o esterna lintervento chirurgico mediante il confezionamento di un by - pass quando il diametro dellaneurisma supera i 3 cm , anche se il paziente asintomatico [ 2 , 5 ] ; per contro , nella patologia dilatativa dellarteria ipogastrica lintervento chirurgico tecnicamente pi impegnativo , soprattutto in considerazione della posizione profonda nella pelvi di tale vaso . analogamente a quanto avviene per gli aneurismi dellaorta addominale , gli interventi per aneurismi isolati dellaai sono considerati interventi di chirurgia maggiore , associati a un tasso di mortalit del 7%11% in elezione e del 30%50% in condizioni di urgenza [ 5 ]  . 
 scopo del presente lavoro descrivere la nostra esperienza in una serie di 15 aneurismi a carico dellarteria iliaca comune e / o esterna in 13 pazienti trattati con endoprotesi e confrontare i risultati ottenuti con quelli riportati in letteratura . 
 materiali e metodi nel periodo compreso tra marzo 1999 e marzo 2004 presso il nostro istituto sono stati sottoposti a trattamento endovascolare 160 aneurismi dellaorta addominale e degli assi iliaci ; in particolare , 127 erano aortici o aorto - iliaci ; 4 erano di pertinenza dellarteria ipogastrica , 14 erano pseudoaneurismi anastomotici ( 9 distali , 5 prossimali ) e 15 aneurismi isolati dellaai . 
la casistica oggetto di questo lavoro si riferisce a 13 pazienti ( 10 maschi e 3 femmine ) , di et compresa tra 55 e 91 anni ( et media di 71 , 8 anni ) , con aneurismi dellaai monoo bilaterali selezionati per lesclusione endovascolare mediante endoprotesi ( tabella 1 )  . 
complessivamente , si trattava di 15 aneurismi : 12 dellarteria iliaca comune ( di cui 2 con estremo prossimale distante circa 12 mm dalla biforcazione aortica e 2 coinvolgenti distalmente larteria ipogastrica ) e 3 dellarteria iliaca esterna , con diametro medio di 4 cm ( range 2 , 58 ) e lunghezza media di 3 , 2 cm ( range 27 )  . 
all patients had associated cardiorespiratory disease with high surgical and anaesthetic risk . preprocedural planning was performed with spiral ct angiography ( except in 1 case ) to evaluate the morphology , size , and anatomical relationships of the aneurysm and the existence of a portion of healthy artery upstream and downstream from the aneurysm ( proximal and distal necks )  . 
this information is indispensable for deciding whether the procedure is feasible and for determining the diameter and length of the stent - grato better determine the length of the stentgraft , also in consideration of the tortuosity of the iliac axes , during the same session , we performed a preliminary angiographic scan using a marked catheter ( 5f optimed pigtail catheter , ettingen , germany )  . twelve patients were treated in the angiography suite under local anaesthesia ( 2% lidocaine ) with and anaesthetist in attendance and monitoring of vital parameters ( heart rate , arterial pressure , oxygen saturation )  . 
subsequently , we used conical endoprostheses , as in the prosthetic branch and extensions of aortobiiliac stent - grafts ( excluder ) , or metal alloy stentgrafts ( wallgraft ) , which have different calibres at their ends and are therefore best suited to address the 2to 3 - mm discrepancy between the diameter of the proximal and distal fixation points along the iliac axis . 
one case required deployment of two stent - grafts owing to unforeseeable shortening of the wallgraft ; another case required three excluder extensions to exclude a large aneurysm . after deployment , we dilated the wallgraft stent - graft and the passager covered stent with an angioplasty balloon ( powerflex cordis , miami , fl , usa ) and the excluder stent - grafts with a latex balloon ( equalizer boston scientific ) to ensure sealing of the proximal and distal fixation sites and complete exclusion of the aneurysm , which was checked by postprocedural angiography . 
 due pazienti sono stati trattati in urgenza : un paziente per shock emorragico conseguente alla rottura dellaneurisma , unaltra paziente perch aveva sviluppato una fistola artero - venosa tra i vasi iliaci con insufficienza cardiaca da alta portata ; nei rimanenti casi asintomatici la diagnosi stata occasionale nel corso di esami ecografici , tc o angiografici espletati per altri motivi . 
tutti i pazienti erano affetti da patologie associate cardiorespiratorie a elevato rischio chirurgico e anestesiologico . il planning pre - procedura stato effettuato mediante angio - tc spirale ( tranne in 1 caso ) per valutare la morfologia , le dimensioni , i rapporti anatomici e lesistenza di una porzione di arteria sana a monte e a valle dellaneurisma ( colletti prossimale e distale ) , informazioni indispensabili per decidere la fattibilit della procedura e , in secondo luogo , il diametro e la lunghezza della protesi . 
per una pi precisa valutazione della lunghezza della endoprotesi , anche in relazione alla tortuosit degli assi iliaci , stato espletato uno studio angiografico preliminare , nella stessa seduta della procedura interventistica , con catetere centimetrato ( pigtail 5 f optimed , ettingen , germania )  . dodici pazienti sono stati trattati in sala angiografica in anestesia locale ( lidocaina al 2% ) , in assistenza anestesiologica con monitoraggio dei parametri vitali ( frequenza cardiaca , pressione arteriosa , saturazione di ossigeno ) mediante approccio percutaneo transfemorale omolaterale alla lesione con introduttori da 10 - 12 f . 
solo la prima procedura stata effettuata con uno stent ricoperto ( passager ) ; successivamente sono state utilizzate endoprotesi coniche tipo braccio protesico ed estensioni di endoprotesi aorto - bisiliaca ( excluder ) o endoprotesi in lega metallica ( wallgraft ) che abbracciano calibri diversi alle estremit e che quindi si adattano meglio alla discrepanza di 23 mm tra il diametro dellancoraggio prossimale e quello dellancoraggio distale lungo lasse iliaco . 
in the remaining 11 patients with a total of 13 aneurysms the follow - up imaging studies ( mean follow - up : 25 months , range : 660 ) demonstrated stent - graft patency and exclusion of the aneurysm in 8 / 11 patients , for a total of 9 / 13 aneurysms ( cases 18 in table 1 )  . 
nel periodo postoperatorio stata somministrata eparina in infusione endovenosa per 48 ore e quindi eparina a basso peso molecolare per almeno un mese ; successivamente si fatto ricorso alla terapia antiaggregante domiciliare quoad vitam ( 120 mg / die di ticlopidina o di acido acetilsalicilico )  . il follow - up stato espletato mediante esame eco - colordoppler prima della dimissione e con controlli angio - tc seriati a 3612 mesi dal trattamento e , successivamente , una volta allanno , per escludere riperfusioni e per valutare le dimensioni della sacca aneurismatica . 
 risultati in tutti i casi trattati si ottenuta la completa e immediata esclusione della sacca aneurismatica , documentata al controllo angiografico effettuato al termine della procedura ( successo tecnico primario del 100% )  . 
c postprocedural angiogram : complete exclusion of the aneurysmal sac after placement of a stent - graft in the common iliac artery and deployment of platinum coil in the hypogastric artery . 
d ct angiography at 2 years ( volume rendering reconstruction ) : complete exclusion of the aneurysmal sac , the conical shape of the stentgraft and the platinum coil in the hypogastric artery are visible . 
e ct angiography at 2 years ( curved multiplanar reconstruction ) : the aneurysmal sac has almost disappeared and the stent appears patent , without intimal hyperplasia . fig , 1a angio - tc : aneurisma isolato dellarteria iliaca comune di destra di 3 , 4 cm di diametro , con coinvolgimento dellarteria ipogastrica . 
b angiografia pre - procedura : aneurisma isolato dellarteria iliaca comune di destra che coinvolge lemergenza dellarteria ipogastrica e larteria iliaca esterna c angiografia post - procedura : posizionata endoprotesi in arteria iliaca comune e spirale in platino in arteria ipogastrica con completa esclusione della sacca aneurismatica . 
d angio - tc a 2 anni ( ricostruzione vr ) : completa esclusione della sacca aneurismatica , riconoscibile la configurazione conica dellendoprotesi e la presenza di spirale in arteria ipogastrica . 
2a computed tomography ( ct ) angiography : isolated aneurysm of the right common iliac artery with a wide eccentric rim of thrombosis measuring 5.2 cm in its greater axis . 
2a angio - tc : aneurisma isolato dellarteria iliaca comune di destra con vasta banda di trombosi eccentrica a maggior asse di 5 , 2 cb angiografia pre - procedura : dilatazione aneurismatica con colletto prossimale di circa 2 c larteria ipogastrica destra appare steno - occlusa allorigine ( freccia )  . 
d angio - tc a 2 anni ( immagine assiale ) : la sacca aneurismatica appare completamente esclusa e persiste immodificata per dimensioni ( 5 , 2 cm )  . ni embricate di endoprotesi di nitinol della lunghezza di 710 cm , si sono scardinate non avendo un valido sostegno nel contesto della sacca aneurismatica , voluminosa , particolarmente estesa in lunghezza . 
non disponibile un follow - up pi prolungato , essendo il paziente deceduto a 3 anni dal trattamento . in sintesi , 2 / 13 pazienti sono stati esclusi dal follow - up ; nei restanti 11 si riportato un successo clinico in 8 / 11 ( con efficace esclusione di 9 aneurismi )  . discussione gli aneurismi isolati dellaai sono rari [ 7 , 8 ] , e la loro storia naturale caratterizzata da un alto rischio di rottura [ 5 , 9 ]  . 
la crescita dellaneurisma si verifica nel 36% dei pazienti con una velocit di 4 mm allanno ; tuttavia , la dimensione critica di rottura non stata ancora definita [ 10 ]  . 
in 36% of patients , the aneurysm grows at a rate of 4 mm / year , but a critical size for rupture has yet to be been defined [ 10 ]  . 
however , because the signs of impending rupture are difficult to detect and the risk of death from a ruptured aneurysm is particularly high , some authors prefer to operate even aneurysms smaller than 3 cm [ 5 , 9 ]  . 
surgical repair after aneurysm resection and bypass graft deployment is nonetheless a complex procedure , with mortality rates ranging from 7% to 13% [ 5 , 11 ] and a significant rate of complications such as peripheral ischaemia , haemorrhage , bypass infections and ureteral lesions [ 5 ]  . 
endovascular deployment of stent - grafts is a sufficiently safe , alternative approach to surgery that has been shown to be feasible in animals and humans [ 12 , 13 ]  . from the literature , it is clear that experiences of endovascular treatment with covered stents of iaas are limited to case reports and case series with short - term and mid - term follow - up [ 1428 ]  . 
the published results indicate clinical success in 78.9% [ 28 ] to 97% [ 18 , 19 , 25 ] , with 100% success reported for some small series with short - term follow - up [ 15 , 16 ]  . 
in our series , one of the largest published nationally and with the longest mean follow - up period ( 25 months ) [ 22 , 25 , 26 ] , clinical success was achieved in 72% of patients ( 69% of iaas ; in particular , it should be noted that six of the nine successfully treated aneurysms were 3 cm )  . 
this relatively low success rate is justified by several factors : in one patient with a bilateral aneurysm of the common iliac artery with a fairly short proximal neck ( 12 mm ) , the stent - grafts excluded the aneurysms only temporarily ; subsequently , progressive dilatation of the aortic bifurcation caused migration of both stent - grafts , along with appearance of a bilateral type 1 endoleak , requiring deployment of a bifurcated stent - graft after 30 months . 
today , we would consider this case by the same standards as an aortobiiliac aneurysm , that is , deserving treatment with a bifurcated stent - grain one patient with a large , particularly long , aneurysm that communicated with the iliac vein , treatment might have been successful had we used an adequately long stent - graft ( not commercially available at the time ) ; the procedure was , however , carried out as an emergency and allowed elective bypass surgery to be performed after 2 months . 
 no complications , such as stent - graft thrombosis [ 20 , 24 ] , significant intimal hyperplasia [ 19 ] or distal embolisation [ 15 , 21 , 23 , 27 ] were observed . 
in contrast to other series [ 15 , 17 , 23 , 27 ] , there were no cases of intestinal ischaemia or gluteal claudication , probably because the hypogastric trattamento chirurgico elettivo indicato per la maggior parte dei pazienti ed raccomandato per aneurismi asintomatici di diametro > 3 cm , tenuto conto che quelli pi piccoli hanno di solito una buona prognosi [ 2 ] ; tuttavia , data la difficolt di trovare dei segni di imminente rottura e lelevato rischio di morte nel caso questa evenienza si verificasse , alcuni autori preferiscono intervenire anche per dimensioni inferiori [ 5 , 9 ]  . 
la ricostruzione chirurgica dopo resezione dellaneurisma e interposizione di un by - pass per una procedura complessa con tassi di mortalit del 7%13% [ 5 , 11 ] , accompagnati da significative complicanze operatorie quali ischemia periferica , emorragia , infezione del by - pass e lesioni delluretere [ 5 ]  . 
 dalla revisione della letteratura si evince che esperienze relative al trattamento endovascolare con stent ricoperti degli aneurismi dellaai sono limitate a case report e a casistiche con un follow - up a breve e medio termine [ 1428 ] ; i risultati pubblicati riportano un successo clinico variabile dal 78 , 9% [ 28 ] al 97% [ 18 , 19 , 25 ] , con risultati del 100% riferiti da alcuni autori per serie numericamente contenute e con follow - up a breve termine [ 15 , 16 ]  . 
nella casistica personale , che una delle pi numerose tra quelle pubblicate a livello nazionale e con follow - up medio pi lungo ( 25 mesi ) [ 22 , 25 , 26 ] , il successo clinico stato ottenuto nel 72% dei pazienti ( 69% degli aneurismi dellaai : in particolare va segnalato che dei 9 aneurismi trattati con successo , 6 presentavano un diametro 3 cm )  . 
in un paziente , portatore di aneurisma bilaterale dellarteria iliaca comune con colletto prossimale piuttosto corto ( 12 mm ) , le protesi hanno escluso solo temporaneamente gli aneurismi ; peraltro la malattia per la progressiva dilatazione della biforcazione aortica ha provocato la migrazione di entrambe le endoprotesi con comparsa di endoleak bilaterale di tipo i , ci che ha reso necessario il posizionamento a 30 mesi di distanza di una endoprotesi biforcata : tale paziente stato da noi trattato nel 1999 , allinizio della nostra esperienza ; oggi considereremmo questo caso sin dal primo approccio alla stessa stregua di un aneurisma aorto - bis - iliaco , meritevole pertanto di trattamento mediante unendoprotesi biforcata . 
in una paziente , portatrice di aneurisma voluminoso , particolarmente esteso in lunghezza e comunicante con la vena iliaca , il trattamento avrebbe potuto avere successo se si fosse impiegata ununica endoprotesi di lunghezza adeguata ( allora peraltro non disponibile in commercio ) ; la procedura comunque , espletata in urgenza , ha consentito di effettuare , a distanza di 2 mesi , lintervento chirurgico di by - pass in elezione . 
 non si sono verificate complicanze quali trombosi dellendoprotesi [ 20 , 24 ] , iperplasia intimale di significativa entit [ 19 ] , embolizzazione distale [ 15 , 21 , 23 , 27 ] ; non si d . 
abbiamo riscontrato uno pseudoaneurisma della arteria femorale comune , trattato con successo mediante iniezione percutanea di trombina . conclusions conclusioni endovascular repair of iaas has the advantage of being a minimally invasive procedure that can be proposed not only for patients with contraindications for conventional surgery but also for those who are eligible for bypass surgery , as the incidence of complications is lower . 
in small aneurysms , instead , it can be proposed as a definitive procedure , even though longer follow - up periods are needed to establish its efficacy in the long term . il trattamento endovascolare degli aneurismi dellaai possiede i vantaggi delle procedure mini - invasive ed proponibile non solo nei pazienti in cui la chirurgia tradizionale controindicata , ma anche in quelli che possono affrontare lintervento di by - pass per la minore incidenza di complicanze ; inoltre , non preclude lintervento chirurgico , che pu venire effettuato in un secondo tempo . 
fugazzola1 1vascular and interventional radiology , department of radiology , 2department of urology , 3anesthesiology , university of insubria , viale borri 57 , i - 21100 varese , italy correspondence to : g . 
over the last year , we replaced 27 double - j ureteral stents in 20 patients ( 10 men and 10 women ; mean age 67.7 years , range 4383 ) ; 15 / 20 patients had a native kidney , 3 / 20 had a transplanted kidney and 2 / 20 had a ureteroileal conduit . 
all stents were grasped with a gooseneck snare under fluoroscopic control , and the distal end was withdrawn just outside the urethra ; then a wire was advanced through the stent lumen and positioned in the renal pelvis . 
nel corso dellultimo anno abbiamo sostituito 27 stent ureterali in 20 pazienti ( 10 maschi e 10 femmine ; et media 67 , 7 anni , range 4383 ) ; 15 / 20 in reni nativi ; 3 / 20 in pazienti portatori di trapianto renale e 2 / 20 in pazienti con uretero - ileo - cutaneostomia . 
several approaches have been described for retrieval and replacegli stent ureterali sono un dispositivo ampiamente utilizzato nel trattamento delluropatia ostruttiva ; possono essere posizionati per via discendente transnefrostomica o ascendente mediante cistoscopia . 
il management degli stent richiede la sostituzione circa ogni 6 mesi al fine di prevenirne lostruzione e linfezione , che sono evenienze tra loro correlate e relativamente frequenti [ 1 ]  . 
 the purpose of this study was to evaluate the feasibility and results of an interventional radiology technique for transurethral retrieval and replacement of ureteral stents under fluoroscopic control with the aim of proposing the method as an alternative to cystoscopic replacement . te diverse esperienze riguardati la rimozione e la sostituzione di stent ureterali con guida fluoroscopica mediante approccio percutaneo transrenale [ 24 ] o con guida cistoscopica per via transuretrale [ 5 ] ; sono stati riportati solo pochi casi di rimozione e sostituzione per via retrograda senza guida cistoscopica [ 3 , 4 , 68 ]  . 
la sostituzione transrenale una procedura con un rischio di sanguinamento non trascurabile legato al ripetuto passaggio di dispositivi di elevato calibro attraverso il parenchima renale [ 24 ] ; la sostituzione ascendente cistoscopica prevede lutilizzo di stent di calibro non superiore a 6 f , per motivi tecnici legati al diametro del canale operativo del cistoscopio ; tali stent vanno quindi incontro a occlusione pi frequentemente rispetto a quelli posizionati per via discendente [ 5 ]  . 
 scopo del nostro lavoro valutare fattibilit e risultati di una tecnica di radiologia interventistica di rimozione e sostituzione transuretrale degli stent ureterali con guida fluoroscopica , al fine di proporre la metodica come alternativa alla sostituzione cistoscopica . materials and methods materiali e metodi transplants , three kidney over the past year , we replaced 27 double - j ureteral stents in 20 patients ( 10 men and 10 women ; mean age 67.7 years , range 4383 ) ; 13 / 20 patients underwent unilateral stent replacement and 7 / 20 underwent bilateral replacement . 
stents had been implanted antegrade ( 9 cases ) or retrograde ( 18 cases ) to treat malignant ureteral obstructions ( 14 cases : five gynaecological tumours , three bladder carcinomas , three prostate carcinomas and three colorectal carcinomas ) or fibrotic obstructions ( six cases : ureteroileal conduits and one postoperative fibrosis )  . 
all procedures were carried out with the patients under sedation and analgesia ( with propofol , fentanyl and midazolam in appropriate doses for the patients weight , the length of the procedure and the patients pain threshold )  . 
after accurate disinfection , the bladder was catheterised with a vascular introducer sheath ( calibre : 7 f ; length : 15 cm for women and 23 cm for men ) ( cordis , miami , fl , usa )  . 
the bladder was distended with a 3 : 1 solution of iodinated contrast material and saline to reduce pain and facilitate intravesical manoeuvres ; the dilution was chosen to obtain sufficient bladder opacification to provide a landmark for the fluoroscopic manoeuvres without affecting visualisation of the devices . 
the distal end of the ureteral stent was grasped with a 6 - f gooseneck snare catheter with an 18 - mm loop ( hooker , meditalia , biomedica , modena , italy ) under fluoroscopic guidance nellultimo anno abbiamo sostituito 27 stent ureterali con configurazione a doppio j in 20 pazienti ( 10 maschi e 10 femmine ; et media 67 , 7 anni , range 4383 ) ; in 13 / 20 pazienti stata effettuata una sostituzione monolaterale e in 7 / 20 pazienti bilaterale ; in 15 / 20 pazienti la sostituzione stata effettuata in uretere nativo , 3 / 20 pazienti erano portatori di trapianto renale e 2 / 20 di uretero - ileo - cutaneostomia . 
gli stent erano stati posizionati per via anterograda ( in 9 casi ) o retrograda ( in 18 casi ) per trattare ostruzioni ureterali maligne ( 14 casi : 5 tumori ginecologici , 3 carcinomi vescicali , 3 carcinomi prostatici e 3 carcinomi del colon - retto ) o fibrose ( 6 casi : 3 trapianti renali , 2 uretero - ileo - cutaneostomie e 1 post - chirurgica )  . 
tutte le procedure sono state effettuate con sedazione e analgesia ( ottenuta mediante propofol , fentanyl e midazolam in dosi adeguate al peso del paziente , alla durata della procedura e alla tollerabilit del dolore da parte del paziente )  . 
dopo asepsi accurata stato eseguito il cateterismo vescicale utilizzando un introduttore vascolare ( calibro : 7 f ; lunghezza : 15 cm per le femmine e 23 cm per i maschi ) ( cordis , miami , fl , usa )  . 
after stent withdrawal , the hydrophilic guidewire was exchanged with a superstiff device ( amplatz , boston scientific , ratingen , germany ) by using a straight 5 - f catheter ( glidecath , terumo , tokyo , japan )  . 
in one patient with a ureteroileal conduit , the stent could not be withdrawn , as incrustations and adhesions due to recurrent infecstato ottenuto un successo tecnico in 26 / 27 casi . 
in un paziente con uretero - ileo - cutaneostomia non stata possibile la retrazione dello stent , il quale risultava adeso alle pareti ureterali a causa di incrostazioni e aderenze causate da ing . 
durante il follow - up ( 116 mesi , medio 6 , 7 ) , abbiamo osservato 4 ostruzioni di stent trattate con una ulteriore sostituzione retrograda con guida fluoroscopica . discussion ureteral stents are used to maintain ureteral patency in various benign or malignant conditions . 
cystoscopic retrograde replacement has been widely described [ 5 ] ; for cases of failure of this approach , various authors have reported antegrade transrenal replacement [ 24 ]  . a limited number of studies have reported on retrograde replacement under fluoroscopic control , with success rates of 97%100% . 
fluoroscopically guided retrograde removal and replacement with snare catheters may be used when the cystoscopic approach is unfeasible or fails ( patients with frozen pelvis or bladder - neck sclerosis in whom cystoscope manipulation may be difficult ; malignant obstructions involving the ureteral papilla ; patients with ankylosis who are unable to assume the lithotomy position for cystoscope insertion ; patients with bleeding - prone bladder neoplasms because the introduction of cystoscopy instruments that are larger in calibre than those used in fluoroscopic removal carries a higher risk of bleeding ; patients with a urostomy )  . 
in such cases , the advantage of fluoroscopically guided replacement lies in the smaller calibre of the devices ( 68 f ) , which are easier to manipulate inside the bladder and consequently involve a lower risk of bleeding in neoplastic disease . 
in addition , angiographically guided recanalisation of the stent being removed allows maintenance of ureteral - tract patency , which is monitored by fluoroscopy , and the ability to check that the distal extremity of the new stent has reached the renal pelvis . 
because the male urethra is longer and grasping and withdrawing of the stent may be more difficult , special care must be taken when performing these manoeuvres in men [ 6 , 8 ]  . 
in our experience , we used commercial gooseneck snare catheters ; some authors have described the use of homemade snares consisting of a catheter and a hydrophilic guidewire , which , albeit more difficult to manipulate , reduces the cost of the procedure [ 6 ]  . 
forceps - type devices have seldom been used and appear to be poorly suited discussione gli stent ureterali sono utilizzati per mantenere la perviet della via urinaria in diverse patologie benigne e maligne . 
la sostituzione retrograda con guida cistoscopica stata ampiamente descritta [ 5 ] ; in caso di fallimento di tale approccio stata riportata da diversi autori la sostituzione anterograda per via transrenale [ 24 ]  . sono state descritte poche esperienze riguardanti la sostituzione retrograda con guida fluoroscopica con tassi di successo compresi tra 97%100% [ 3 , 4 , 68 ]  . 
la sostituzione retrograda fluoroscopica , mediante catetere a laccio , pu essere utilizzata in caso di non fattibilit o di fallimento dellapproccio cistoscopico ( pazienti con pelvi congelata o con collo vescicale sclerotico nei quali risulta difficoltoso manovrare il cistoscopio ; ostruzioni maligne coinvolgenti la papilla ureterale ; pazienti con anchilosi che non possono essere messi in posizione ginecologica per lintroduzione del cistoscopio ; pazienti con neoplasie facilmente sanguinanti che coinvolgono la vescica , in quanto lintroduzione dei dispositivi cistoscopici , di calibro maggiore rispetto a quelli per la rimozione fluoroscopica , ha un maggior rischio di sanguinamento ; pazienti con urostomie )  . 
il vantaggio della sostituzione con guida fluoroscopica , in questi casi , legata al minor calibro dei dispositivi introdotti ( 68 f ) che risultano pi manovrabili allinterno della vescica e comportano quindi minori rischi di sanguinamento in caso di patologia neoplastica . 
inoltre la ricanalizzazione dello stent da rimuovere mediante guida angiografica consente di mantenere la canalizzazione delluretere , che viene controllata mediante fluoroscopia , e di verificare che lestremo distale del nuovo stent abbia raggiunto la pelvi renale ; tale manovra di fondamentale importanza soprattutto in pazienti con stenosi severe da patologia maligna [ 6 ]  . 
nei pazienti di sesso maschile , a causa della maggiore difficolt nellafferrare e retrarre lo stent in relazione alla lunghezza delluretra , deve essere osservata una particolare attenzione durante lespletamento di queste manovre [ 6 , 8 ]  . 
nella nostra esperienza abbiamo utilizzato cateteri a laccio tipo goose - neck commerciali ; alcuni autori hanno riportato lutilizzo di lacci home made , costituiti da un catetere e una guida idrofilica , che risultano meno maneggevoli ma consentono una riduzione dei costi della procedura [ 6 ]  . 
stent replacement in patients with a kidney transplant does not normally pose special problems , although more accurate asepsis needs to be maintained because of the risk of upper urinary tract contamination in subjects receiving immunosuppressant therapy . 
in this case , we hypothesised that encrustations related to intestinal secretions or recurrent upper urinary tract infections caused the stent to adhere to the ureteral walls , preventing its withdrawal . 
retrograde replacement may also prove unfeasible in the case of proximal stent migration into the renal pelvis with distal end at ureteral level . a further advantage is that pyelographic intraprocedural monitoring with intracavitary injection of contrast material can be performed in addition to fluoroscopic control to ensure more precise and safer positioning of the cranial extremity of the stent and easier negotiation of possible ureteral kinks or bends . raramente utilizzati e paiono poco adatti a questo tipo di procedura in relazione al piccolo calibro dei bracci [ 2 ]  . il rischio di sanguinamento dellapproccio retrogrado minore rispetto alla sostituzione anterograda a causa dellelevato calibro dei dispositivi che in questultimo caso devono attraversare il parenchima renale ; tale approccio deve quindi essere riservato , secondo la nostra opinione , alla eventualit di fallimento della sostituzione retrograda . 
la sostituzione in pazienti con trapianto renale generalmente non pone particolari problemi , ma necessario osservare unasepsi pi accurata in relazione al rischio di contaminazione delle alte vie urinarie in soggetti in terapia immunosoppressiva . 
 lunico caso di insuccesso della rimozione , nella nostra esperienza , si verificato in presenza di derivazione urinaria ( uretero - ileo - cutaneostomia ) ; in questo caso stato ipotizzato che le incrostazioni causate dalle secrezioni intestinali o dalle ricorrenti infezioni delle alte vie urinarie che si erano verificate in questo paziente avessero causato ladesione dello stent alle pareti ureterali impedendone la retrazione . 
la sostituzione retrograda pu risultare non fattibile anche in caso di dislocazione prossimale dello stent in pelvi renale con estremo distale a livello delluretere . inoltre la possibilit di effettuare , oltre al controllo fluoroscopico , anche un controllo intra - procedurale pielografico mediante iniezione intracavitaria di mezzo di contrasto , permette un posizionamento pi preciso e sicuro dellestremo craniale dello stent , superando pi facilmente anche eventuali inginocchiamenti o kinking delluretere . conclusion conclusione in conclusion , transurethral fluoroscopically guided replacement of dysfunctioning ureteral stents may be considered a safe and effective alternative to cystoscopic replacement , as it is just as acceptable to the patient and allows insertion of larger stents with better long - term patency rates . 
in cases where the cystoscopic approach is unfeasible , transurethral fluoroscopically guided replacement should be preferred to transrenal replacement because it is less invasive , avoiding passage through the renal parenchyma and eliminating the risk of bleeding . in conclusione , la procedura pu essere considerata unalternativa sicura ed efficace alla sostituzione per via cistoscopica degli stent ureterali non funzionanti , in quanto almeno altrettanto compliante per il paziente e permette il posizionamento di stent di calibro maggiore , con una migliore perviet a lungo termine . 
in caso di non fattibilit dellapproccio cistoscopico , la sostituzione retrograda preferibile alla sostituzione transrenale per la minore invasivit , poich evita lattraversamento del parenchima renale eliminando il rischio di sanguinamento a esso correlato . 
pupillo , via della mainetta , 88d , i - 67010 coppito , laquila , fax : + 39 - 086 - 4273184 , e - mail : pupillina@libero.it received : 05 september 2006 / accepted : 12 january 2007 / published online : 21 september 2007 abstract purpose . 
magnetic resonance imaging ( mri ) was performed using a 1.5 - t magnet with a phased - array coil and acquisition of t2 - weighted single - shot fast spin echo ( ssfse ) half fourier sequences before intravenous administration of gadolinium , and t1 - weighted fast spoiled gradient ( fspgr ) fat - saturated sequences before and after contrast administration . 
before the examination , patents received oral polyethylene glycol ( peg ) ( 1 , 000 ml for adults ; 10 ml / kg of body weight for children )  . 
abbiamo studiato un campione di 50 pazienti con diagnosi istologica di morbo di crohn ( 37 in fase attiva di malattia ; 13 in remissione clinica ) ; abbiamo utilizzato un magnete da 1 , 5 t , bobina phased array e sequenze t2 dipendenti ssfse half fourier in fase precontrastografica e t1 dipendenti fspgr fat - sat in fase pree post - contrastografica . 
prima di eseguire lesame stato somministrato per os glicole polietilenico ( peg ) ( 1000 ml per adulti ; 10 ml / kg del peso corporeo per bambini )  . abbiamo tracciato roi ( region of interest ) per valutare lintensit del segnale nella parete intestinale normale e patologica e la percentuale dincremento nel tempo . 
in caso di remissione della malattia dopo terapia , per contro , si ha una significativa riduzione dellincremento di segnale , di poco aumentato rispetto a quello delle anse normali . 
lo studio dinamico con risonanza magnetica ( rm ) ci consente di quantificare lattivit infiammatoria locale della parete intestinale . parole chiave morbo di crohn risonanza magnetica cdai introduction introduzione crohns disease is an idiopathic inflammatory disease that may affect any portion of the gastrointestinal tract from the mouth to the anus . 
assessment of disease activity , instead , is based on laboratory parameters and disease activity indexes , among which the gold standard is the crohns disease activity index ( cdai ) , which assigns a score to each sign or symptom ( table 1 ) to enable an overall clinical assessment [ 14 ]  . 
 the diagnosis of crohns disease essentially relies on ileocolonoscopy and radiographic barium studies of the no tenue coinvolto nell80% dei pazienti , con una netta predisposizione della malattia per lileo terminale . 
la patologia interessa anche il colon nel 50% dei pazienti , mentre nel 15%20% dei casi si verifica interessamento isolato del colon e nel 2%3% si osserva una patologia perianale isolata . 
 i pazienti affetti dal morbo di crohn non rappresentano una popolazione omogenea , per cui , per poter meglio orientare le scelte terapeutiche , si reso necessario un sistema di classificazione della patologia basato sulla severit e sullestensione della stessa . 
lattivit di malattia viene invece valutata utilizzando , oltre ai parametri laboratoristici , indici di attivit di malattia tra i quali il gold standard considerato il crohns disease activity index ( cdai ) , che attristool count summed daily for 7 days sum of 7 days of daily ratings as : 0 = none ; 1 = mild ; 2 = moderate ; 3 = severe sum of 7 days of daily ratings as 0 = generally well ; 1 = slightly below par ; 2 = poor ; 3 = very poor ; 4 = terrible any of the following present during the previous 7 days : a . 
fever > 100f 0 = no ; 1 = yes 0 = none ; 2 = questionable ; 5 = definite 47 - hematocrit ( males ) 42 - hematocrit ( females ) 100 [ 1 - ( body weight / standard weight ) ] table 1 crohns disease activity index variable scale liquid or very soft stools abdominal pain general well - being features of extraintestinal disease opiates for diarrhoea abdominal mass hematocrit % body weight below standard tabella 1 indice di attivit del morbo di crohn variabili scala feci liquide o molto morbide dolore addominale benessere generale manifestazione extraintestinali somma di una valutazione quotidiana per 7 giorni somma di una valutazione quotidiana per 7 giorni : 0 = buono ; 1 = lieve ; 2 = moderato ; 3 = severo somma di una valutazione quotidiana per 7 giorni : 0 = buono ; 1 = lievemente sotto la media ; 2 = basso ; 3 = molti basso ; 4 = scarso alcuni dei seguenti aspetti nei precedenti 7 giorni : a . 
febbre > 100f 0 = no ; 1 = si 0 = assente ; 2 = dubbia ; 5 = sicura 47 - ematocrito ( maschi ) 42 - ematocrito ( femmine ) oppiacei per la diarrea masse addominali ematocrito % di peso corporeo sotto la media 100 [ 1 - ( peso corporeo / peso standard ) ] weight 20 each punteggio 20 ognuna v.a. 
sonography is widely used in patients with acute manifestations of disease ; it is able to demonstrate indirect signs of inflammation and , with use of colour power - doppler imaging , it can identify increased wall vascularity . 
spiral computed tomography ( ct ) and ct enteroclysis are valuable tools for detecting stenosis and complications of crohns disease . the diagnostic accuracy of this examination is in part constrained by the difficulty in obtaining adequate lumen distension , a situation that does not allow for correct bowel wall measurement , and by the subjective nature of the assessment of wall enhancement . 
in addition , the use of ionising radiation is not to be underestimated . magnetic resonance imaging ( mri ) is a powerful tool in the diagnosis and follow - up of intestinal diseases [ 822 ]  . 
the technique does not make use of ionising radiation , an important feature if we consider that crohns disease predominantly affects young subjects [ 15 , 2435 ]  . the aim of our study was to assess the possibility of quantifying local inflammatory activity in patients with crohns disease by means of a dynamic study of contrast uptake by the intestinal wall after oral administration of an isosmolar solution to distend the small bowel [ 20 , 36 , 37 ]  . materials and methods fifty patients ( 30 females and 20 males ; age range 871 years , average age 26.3 years ) with crohns disease diagnosed by endoscopic examination and biopsy was studied by mri before and after administration of contrast material . thirty - seven patients were in the active phase of disease ( 25 in the early phase ; 12 in the reactivation phase ) ; 13 were in the remission phase after treatment . 
only five patients had undergone surgery prior to the mri examination ( almost 1 year earlier ) : three had ileocolic resection with terminoterminal anastomosis , and two had ileal resection with sparing of the ileocaecal valve and laterolateral ileoileal anastomosis . 
about 25 min before the examination , patients were administered an oral contrast agent , polyethylene glycol ( peg ) ( 1 , 000 ml for adults ; 10 ml / kg body weight for children ) to distend the small bowel [ 21 , 30 , 38 ]  . 
the mri examination [ 39 , 40 ] was performed with : t2 - weighted single shot fast spin echo ( ssfse ) half fourier sequences [ te : 96.1 ; tr : ( cid : 2 ) ; field of view ( fov ) : 40 40 cm ; matrix : 256 160 ; slice thickness : 5 mm ; acbuisce un punteggio a ogni segno o sintomo ( tabella 1 ) , permettendo cos una valutazione clinica globale [ 14 ]  . 
lecografia viene ampiamente utilizzata soprattutto in pazienti con manifestazioni acute ; in grado di dimostrare segni indiretti di flogosi e , con luso del modulo color power doppler capace di rilevare lincremento della vascolarizzazione parietale . 
la tomografia computerizzata ( tc ) e il clisma - tc mostrano con accuratezza le stenosi e le complicanze del morbo di crohn . laccuratezza diagnostica di tale indagine comunque in parte limitata dalla difficolt a ottenere unadeguata distensione del lume ( tc spirale ) , situazione che non permette la corretta misurazione della parete viscerale , e dalla soggettivit nel valutare il grado di accumulo di contrasto parietale ; inoltre il paziente sottoposto a radiazioni ionizzanti . la risonanza magnetica ( rm ) rappresenta un valido strumento per superare questi limiti nella diagnosi e nel followup delle patologie intestinali [ 822 ]  . 
tale tecnica non espone il paziente a radiazioni ionizzanti , fattore da non sottovalutare dato che la popolazione colpita dalla patologia prevalentemente costituita da persone giovani [ 15 , 2435 ]  . scopo del nostro lavoro stato valutare se possibile determinare il grado di attivit infiammatoria locale in pazienti affetti da morbo di crohn studiando dinamicamente laccumulo di contrasto della parete intestinale dopo somministrazione per via orale di una soluzione isosmotica in grado di produrre distensione intestinale [ 20 , 36 , 37 ]  . materiali e metodi un campione di 50 pazienti ( 30 di sesso femminile e 20 di sesso maschile ; di et compresa tra 8 e 71 anni ; et media 26 , 3 anni ) , con diagnosi di morbo di crohn dimostrata mediante esame endoscopico associato a biopsia , stato sottoposto a esame di rm senza e con mezzo di contrasto paramagnetico . in 37 dei pazienti esaminati la malattia di crohn si presentava in forma attiva ( 25 pazienti erano nella forma primitiva di malattia , 12 pazienti erano in fase di riacutizzazione ) ; 13 pazienti si presentavano in fase di remissione di malattia dopo terapia . 
solo 5 dei pazienti esaminati erano stati precedentemente ( almeno 1 anno prima ) trattati chirurgicamente , 3 mediante resezione ileo - colica con anastomosi termino - terminale e 2 mediante resezione ileale con conservazione della valvola ileo - cecale e anastomosi ileo - ileale latero - laterale . 
peg has the same signal intensity as water , making the distended intestinal lumen appear hyperintense on t2weighted sequences and hypointense on t1 - weighted sequences . image evaluation images were assessed for bowel wall thickness at the terminal ileum , significant and nonsignificant luminal stenosis , and intra - abdominal abscess or fluid collections . 
moreover , after the mri examination , regions of interest ( rois ) of 57 mm2 were placed over the diseased loop and healthy bowel wall to study signal intensity and percentage increase over time and thus quantitatively assess bowel wall vascularity and disease activity [ 41 ]  . 
 spearmans test was used to correlate each patients cdai score with the time required to reach a plateau phase and the percentage of maximum enhancement of the diseased bowel [ 14 , 42 , 43 ]  . 
the software used for statistical analysis was stata ( version 8.2 ; stata corp ; college station ; tx , usa )  . results in 44 ( 88% ) out of 50 patients , we observed significant thickening of the bowel wall at the level of the terminal ileum . more specifically , in 41 out of 44 patients who had not undergone surgery and had a histological diagnosis of crohns disease , the mri study showed significant wall thickening at 1 , 5 t ( slow rate 120 mt / m / s ) , bobina phased array . 
per distendere le anse intestinali abbiamo somministrato per os a ogni paziente , circa 25 minuti prima dellinizio dellesecuzione dellesame , glicole polietilenico ( peg ) ( 1000 ml nei pazienti in et adulta ; 10 ml / kg nei pazienti in et pediatrica ) [ 21 , 30 , 38 ]  . 
inoltre , prima di iniziare lesame abbiamo iniettato per via intramuscolare 1 fiala ( 10 mg / ml ) di butilscopolamina ( buscopan ) per ridurre la peristalsi intestinale [ 31 , 39 ]  . 
lo studio rm [ 39 , 40 ] stato condotto con : sequenze t2 dipendenti di tipo ssfse ( single shot fast spin echo ) half fourier ( te : 96 , 1 ; tr : ( cid : 2 ) ; fov : 40 40 cm ; matrice : 256 160 ; spessore : 5 mm ; tempo di acquisizione : 18 s in apnea ) in fase precontrastografica su piani assiali e coronali o obliqui per consentire lindividuazione dellultima ansa ileale ; una volta individuato il piano ottimale , abbiamo ripetuto la sequenza con matrice pi alta ( 512 256 ) ; sullo stesso piano abbiamo utilizzato sequenze t1 dipendenti di tipo fspgr ( fast spoiled gradient echo ) con saturazione del grasso ( te : 1 , 3 ; tr : 200 ; fov : 40 40 cm ; matrice : 256 160 ; spessore : 5 mm ; tempo di acquisizione : 16 sec in apnea ) in fase precontrastografica e ripetute in serie 6 volte ( le prime 3 luna di seguito allaltra , le altre a distanza di 40 secondi dalla fine della precedente ) dopo somministrazione endovenosa di 0 , 1 mmol / kg di gadolinio . tutti i pazienti , anche quelli in et pediatrica , hanno ben tollerato lesame di rm collaborando adeguatamente con lattivit respiratoria . 
in tutti si avuta unadeguata visualizzazione dellintestino grazie allutilizzo del peg , che ha consentito di ottenere buoni livelli di distensione intestinale ; stato possibile cos ottenere informazioni su tutto lintestino e nel dettaglio sullultima ansa ileale . 
il peg ha presentato un comportamento sovrapponibile a quello dellacqua per quel che riguarda lintensit di segnale , facendo apparire il lume intestinale , disteso da tale soluzione isosmotica , iperintenso nelle sequenze t2 dipendenti e ipointenso nelle sequenze t1 dipendenti . sulle immagini acquisite abbiamo valutato lo spessore della parete intestinale a livello dellultima ansa ileale , la presenza di stenosi significativa o non significativa del lume , la presenza di raccolte ascessuali o di versamento libero endoaddominale , e abbiamo definito come patologiche le anse con uno spessore parietale 4 mm e come significative solo le stenosi associate a dilatazione a monte . 
dopo lesecuzione dellesame rm sono state posizionate delle roi ( region of interest ) delle dimensioni comprese tra 5 e 7 mm2 di area a livello dellansa patologica e a livello della parete intestinale sana al fine di valutare lintensit del segnale e la percentuale dincremento dello stesso nel tempo , ottenendo cos una valutazione quantitativa statistical evaluation analisi delle immagini v.a. 
in 13 out of 44 patients ( 29.5% ) , mri showed bowel wall thickening in other portions of the gasdellincremento di vascolarizzazione della parete intestinale e quindi dellattivit di malattia [ 41 ]  . 
 in 8 pazienti la rm ci ha permesso di esaminare alterazioni a carico del tessuto adiposo mesenteriale , che nelle sequenze t2 dipendenti si presentava con disomogenea iperintensit del segnale . 
 in 41 pazienti ( 82% ) , dopo somministrazione endovenosa di mezzo di contrasto ( 0 , 1 mmol / kg di gadolinio ) si avuta una elevata contrastografia a livello del segmento parietale intestinale ispessito . 
in tutti i 41 pazienti si avuto un incremento contrastografico a tutto spessore pi evidente negli strati pi interni ( mucosa ) , ma solo in 36 pazienti ( 72% ) a tale uptake corrispondeva un cdai > 150 . nel nostro studio abbiamo ottenuto una correlazione positiva , seppur non statisticamente significativa , tra il tempo necessario per raggiungere il plateau e i valori di cdai ottenuti ( r = 0 , 012 , p = 0 , 01 )  . 
successivamente abbiamo statisticamente correlato i valori percentuali di massima impregnazione di mezzo di contrasto a livello della parete intestinale patologica calcolando il coefficiente di correlazione di spearman e ottenendo un valore positivo e statisticamente significativo ( r = 0 , 73 )  . 
in these 41 patients , we observed full - thickness enhancement , more evident at the mucosa level , but in only 36 patients ( 72% ) did this uptake correspond to cdai > 150 . 
therefore , the two methods may be used interchangeably . discussion in patients with active crohns disease , the earliest and most common alteration in the intestinal mucosa is neutrophil - mev.a. 
contrast - enhanced axial t1 - weighted fast spoiled gradient fat - saturated image ( a ) shows marked contrast uptake by the diseased bowel wall , especially at the mucosal level . 
two regions of interest were placed on the image : one over the diseased intestinal wall ( red ) , and one over the healthy intestinal wall ( green )  . 
di gadolinio in cui si evidenzia marcato potenziamento parietale del tratto di intestino ispessito prevalente a livello dello strato mucoso ; in tale immagine sono poste delle roi : una sul segmento patologico ( rossa ) e una su un segmento sano ( verde )  . 
contrast - enhanced axial t1 - weighted fast spoiled gradient fat - saturated image ( a ) shows marked contrast uptake by the diseased bowel wall , especially at the mucosal level . 
regions of interest were placed on a vessel ( light blue ) , on a healthy bowel loop ( green ) and on a diseased loop ( red )  . 
di gadolinio che documenta prevalente impregnazione di mezzo di contrasto degli strati mucosi ; sono posizionate roi a livello di un vaso ( celeste ) , di unansa sana ( verde ) e di unansa patologica ( rossa )  . 
il grafico intensit / tempo ( b ) mostra il diverso uptake contrastografico nel tempo tra strutture vascolari ( linea tratteggiata celeste ) , segmento intestinale sano ( linea tratteggiata verde ) e segmento intestinale patologico ( linea tratteggiata rossa )  . discussione diated injury , whereas the earliest gross alterations due to inflammation are slight hyperperfusion and mucosal oedema . as the disease progresses , the bowel wall becomes thickened , fibrous and stenotic . 
the search for parameters capable la pi precoce e frequente alterazione della mucosa osservabile nellintestino di un paziente con morbo di crohn in fase attiva il danno criptico mediato da neutrofili . 
il razionale nasce da unintrinseca capacit di questa tecnica nellidentificazione dellacqua libera , e quindi dellinfiammazione , e nel fatto che liperemia della parete intestinale si traduce in un aumento dellaccumulo di contrasto a livello del segmento intestinale interessato dalla patologia . 
precedenti lavori hanno dimostrato la possibilit di tali rilievi , ma risultavano limitati da uninadeguata distensione del viscere che limitava le potenzialit diagnostiche di tale indagine ; lutilizzo dei mezzi di contrasto orali ha superato questa limitazione [ 24 , 30 , 31 ]  . 
paragonabile allacqua come intensit di segnale in rm , va considerato come mezzo di contrasto bifasico [ 30 , 31 ] , comportamento utile sia in fase pre - contrastografica , dove nelle sequenze t2 dipendenti fa apparire il lume viscerale che lo contiene disteso e iperintenso , e quindi ben differenziabile dalla parete intestinale che appare ipointensa , sia in fase post - contrastografica nelle sequenze t1 dipendenti con saturazione del grasso , dove il lume viscerale disteso dal peg appare ipointenso e differenziato in maniera ottimale dalla mucosa e dalla sottomucosa , le quali mostrano fisiologicamente una sottile rima di potenziamento contrastografico o , in caso di attivit infiammatoria locale , marcato accumulo di contrasto in relazione alla dilatazione dellinterstizio . 
 nello studio del morbo di crohn informazione clinicamente e prognosticamente di primaria importanza lidentificazione del grado di attivit infiammatoria locale ; questo fattore consentir al clinico di stabilire una terapia specifica e differenziata per ogni singolo paziente [ 14 , 38 , 39 , 42 , 44 ]  . 
per valutare il grado di attivit infiammatoria di parete oltre ai parametri laboratoristici che si controllano regolarmente per monitorare la malattia quali la ves , la conta dei globuli bianchi , hb , albumina , 2 globuline , ferro nel siero , pcr , 1 glicoproteina e 1 antitripsina possono essere utilizzati indici numerici di attivit di malattia , la cui valutazione per potrebbe risultare complessa e richiedere tempo [ 45 ]  . 
quello pi attendibile , da noi utilizzato nel nostro studio per correlarvi i dati quantitativi ottenuti con lo studio mediante rm , il cdai [ 1 , 2 , 15 , 46 ] , che si basa sulla valutazione di 8 variabili ( tabella 1 )  . 
il range degli score da 0 a 600 , con un cut off tra patologia e normalit a 150 , e tra malattia attiva e malattia di grado severo a 450 . 
the rationale lies in the techniques ability to identify free water and consequently inflammation and in the fact that bowel wall hyperperfusion corresponds to increased enhancement of the diseased bowel segment . 
previous studies have demonstrated this ability of mri but were limited by inadequate bowel distension , a limitation now overcome by the use of oral contrast agents [ 24 , 30 , 31 ]  . the oral contrast agent used in our study was peg , an agent consisting of a water solution of polyethylene glycol ( 70 g dissolved in 1 l of water ) , which once ingested prevents the water molecules bonded to it from being absorbed by the intestinal mucosa . 
moreover , because it is not fermentable and cannot be attacked by the bacterial flora , it flows rapidly through the jejunal - ileal loops to the caecumri signal intensity characteristics of peg are similar to those of water , so it can be considered a biphasic oral contrast agent [ 30 , 31 ]  . 
this behaviour proves useful both before contrast injection , when the intestinal lumen appears hyperintense in t2weighted sequences and easily differentiated from the hypointense intestinal wall , and after contrast injection , when the intestinal lumen appears hypointense in t1 - weighted sequences with fat suppression and well differentiated from the mucosal and submucosal layers , which physiologically display a thin rim of enhancement and , pathologically , high contrast enhancement related to interstitial dilatation . 
 in the study of crohns disease , it is clinically and prognostically fundamental to identify the degree of local inflammatory activity , as this information will help the clinician decide on specific treatment for each patient [ 14 , 38 , 39 , 42 , 44 ]  . the aim of our study was to investigate whether it was possible to quantify the degree of disease activity . 
to assess the degree of inflammatory activity , numerical indexes of disease activity can be used [ 45 ] in addition to the laboratory parameters commonly used during follow - up , such as erythrocyte sedimentation rate , white blood cell count , haemoglobin , albumin , 2 globulin , serum iron , c - reactive protein , 1 glycoprotein and 1 antitrypssuch indexes are particv.a. 
the most reliable index and the one used in our study to correlate the quantitative data provided by mri was the cdai [ 1 , 2 , 15 , 46 ]  . 
the limitations of this index are interobserver variability , inclusion of subjective variables such as general well - being and intensity of abdominal pain and the fact that it is based on a diary completed by the patients for 7 days before assessment , a requirement that precludes its use in everyday practice . 
 mri is able to not only easily identify the presence of bowel wall inflammation through assessment of contrast enhancement [ 14 , 29 , 39 , 47 ] but also to quantify this by means of roi evaluation of percentage changes in signal intensity . 
mri has a potentially high diagnostic value in assessment of local inflammatory activity in patients with crohns disease [ 14 , 20 , 36 , 37 , 42 , 47 ]  . 
besides enabling identification of the diseased small bowel segment by accurately visualising luminal stenosis , wall thickening and dilatation of the intestinal loops , mri allowed us to quantify the degree of inflammatory activity in all patients , providing crucial information for treatment planning [ 7 ]  . 
moreover , most of the results obtained with mri had a good correlation with clinical data and cdai scores . conclusions mri is a potentially valuable procedure in assessment of the small bowel in patients with suspected crohns disease or monitoring patients after treatment . 
it is easily reproducible and well tolerated , even by children [ 34 , 38 ] , provides both panoramic and detailed views and allows identification of changes in signal intensity or bowel wall thickness . 
therefore , it can be considered a very useful diagnostic tool that provides data on site , extent , degree of inflammatory activity and complications in patients with histologically proven crohns disease , without the use of ionising radiation [ 11 , 23 , 35 , 49 , 50 ]  . 
its limitations lie in poor depiction of wall alterations such as ulcers or fissures , which are better demonstrated by conventional small - bowel enteroclysis [ 25 , 30 , 48 , 50 ]  . 
finally , dynamic mri enables quantitative analysis la variabilit interosservatore , variabili soggettive del paziente , quali il benessere generale e lintensit del dolore addominale , e anche il fatto che il calcolo si effettua dopo una valutazione per 7 giorni del paziente , il che ne impedisce lutilizzo nella pratica quotidiana . 
inoltre , come gi detto , non accurato in pazienti con fistole e stenosi , e non utilizzabile in pazienti che hanno subito una estesa resezione o stomia ileo - colica . 
nonostante questi limiti , allo stato attuale il cdai da considerarsi ancora il gold standard per la valutazione dellattivit di malattia [ 46 ]  . la rm ci consente di identificare agevolmente la presenza di infiammazione a carico della parete intestinale mediante la valutazione dellaccumulo di mezzo di contrasto [ 14 , 29 , 39 , 47 ] , oltre ad una possibile valutazione quantitativa della stessa mediante la valutazione su volumi campione ( roi ) della variazione percentuale del segnale . 
sono per presenti limiti nella visualizzazione di minime alterazioni superficiali di parete , vista la modesta risoluzione spaziale della tecnica [ 30 , 48 ]  . questa indagine si propone come esame potenzialmente a elevato contributo diagnostico nella valutazione dellattivit infiammatoria locale in pazienti con morbo di crohn [ 14 , 20 , 36 , 37 , 42 , 47 ]  . 
in definitiva , la rm ci ha consentito oltre allidentificazione corretta dei diversi segmenti patologici del piccolo intestino , con una ottima rappresentazione sia del lume stenotico , sia dellispessimento parietale , sia della dilatazione delle anse a monte una valutazione quantitativa del grado di attivit infiammatoria in tutti i casi , utile per la successiva pianificazione terapeutica [ 7 ]  . 
inoltre , in una buona percentuale i risultati ottenuti con lo studio mediante rm si sono dimostrati ben correlabili col dato clinico e numerico ottenuto mediante il calcolo del cdai . 
 conclusioni la rm unindagine di grande interesse nello studio dellintestino nei pazienti con sospetto morbo di crohn , o nel caso di follow - up post - terapia , perch facilmente riproducibile , ben tollerata anche dai pazienti pediatrici [ 34 , 38 ] , panoramica e di dettaglio ; inoltre , consente di identificare alterazioni di segnale o di spessore a carico della parete intestinale . 
pertanto pu senza dubbio rappresentare uno strumento diagnostico estremamente utile nel fornire , senza lutilizzo di radiazioni ionizzanti , informazioni circa la localizzazione , lestensione , il grado di attivit infiammatoria intestinale ed eventuali complicanze in pazienti con diagnosi istologica di morbo di crohn [ 11 , 23 , 35 , 49 , 50 ] , pur nella consapevolezza dei limiti che la metodica presenta nellevidenziare eventuali alterazioni di parete quali ulcerazioni e fissurazioni , meglio identificabili col clisma del tenue [ 25 , 30 , 48 , 50 ]  . 
the aim of this study was to assess the reliability of the sonographic breast imaging reporting and data system ( birads ) classification in differentiating benign from malignant breast masses . 
all lesions were classified according to the sonographic bi - rads lexicon . sensitivity , specificity , accuracy , positive predictive value ( ppv ) and negative predictive value ( npv ) for the sonographic birads lexicon and ppv and npv for each lesion category and each sonographic descriptor were calculated . 
il nostro studio conferma che la classificazione ecografica bi - rads costituisce un accurato sistema per la descrizione e il management delle lesioni mammarie . parole chiave mammella nodulo ecografia diagnosi introduction introduzione in the past 15 years , ultrasound ( us ) has increasingly proved to be indispensable in the study of breast masses , above all as a result of continuing technological advances . 
image quality has been remarkably improved by the introduction of highfrequency probes , harmonic imaging , colourand powerdoppler applications and the use of sonographic contrast menegli ultimi 15 anni lecografia si dimostrata metodica sempre pi indispensabile nello studio delle lesioni mammarie grazie soprattutto agli incessanti avanzamenti tecnologici . 
although breast us was initially used chiefly to distinguish between solid and cystic lesions , its use for characterising solid masses and identifying suspicious findings for biopsy and benign lesions for follow - up has gained increasing interest [ 713 ]  . 
the lexicon introduced by the bi - rads system includes sonographic descriptors referring to lesion shape , orientation , margins , boundary , echo pattern , posterior acoustic features and surrounding tissue . 
on the basis of these descriptors , each lesion is assigned a level of suspicion , which is associated with a recommendation for management ( table 1 ) [ 19 ]  . the purpose of this study was to assess the reliability of the bi - rads system in differentiating between benign and malignant solid breast masses . 
in detail , the aims of the study were to : evaluate the diagnostic accuracy of bi - rads in differentiating benign from malignant breast masses determine sensitivity , specificity , prevalence , and negadellimpiego di mezzi di contrasto ecografici [ 16 ]  . 
bench lecografia mammaria sia stata adoperata inizialmente con lo scopo di distinguere le lesioni solide da quelle liquide , si sviluppato un interesse sempre crescente nellutilizzare gli ultrasuoni per la caratterizzazione delle lesioni solide , per identificare le immagini sospette da sottoporre a biopsia da quelle benigne da inviare al follow - up [ 713 ]  . 
la terminologia introdotta dal sistema bi - rads include descrittori ecografici in riferimento alla forma , allorientamento , ai margini , allinterfaccia , allecogenicit , alle caratteristiche acustiche posteriori e alle alterazioni del parenchima circostante . 
sulla base di questi descrittori ogni lesione viene assegnata ad una classe di sospetto che prevede il successivo comportamento diagnostico - terapeutico ( tabella 1 ) [ 19 ]  . lo scopo di questo studio stato quello di determinare lattendibilit del sistema bi - rads nel differenziare le lesioni solide della mammella in benigne e maligne . 
in particolare le finalit di questo studio sono state : valutare laccuratezza diagnostica del sistema bi - rads nel differenziare le lesioni mammarie benigne da quelle maligne ; definire sensibilit , specificit , prevalenza , valori predittivi negativi e positivi per ogni classe di sospetto ; valutare i valori predittivi positivi e negativi dei vari dematerials and methods studiare il valore diagnostico della diversa associazione us examinations were prospectively performed on all consecutive breast masses undergoing biopsy at our department between november 2004 and march 2006 . 
in some cases fnac was performed at the request of the patient or the referring physician . us imaging was done with a siemens antares device with a linear - array high - frequency transducer ( 1013 mhz )  . the examination involved multiple scans of both breasts and the axillary region and focused on the study of the morphological features of the lesion to be aspirated . 
 all lesions underwent us - guided fnac ( 2125 gauge )  . cytology reports were considered reliable only when they documented a specific diagnosis of malignancy or benignity . cytology was not considered reliable if there was discordance between the sonographic findings and the cytological sample , if the sample was inadequate or if it was found to contain only normal parenchymal cells . 
a specific negative cytological result was defined as no evidence of atypical cells and findings compatible with a diagnosis of complicated cyst , fibroadenoma , galactocele , liponecrosis , granuloma and apocrine metaplasia . 
cases with specific negative cytology were scheduled for short - interval follow - up every 6 months for at least 2 years . all us examinations and fnac were done by two radiologists expert in breast imaging ( mc and pb ) who described and classified the lesions according to the bi - rads system at the time of the examination , without knowing the histopathological results . 
lesions displaying all of the signs suggestive of a benign lesion were assigned to bi - rads category 3 ( oval or round shape , parallel orientation , circumscribed margins , abrupt interface , enhancement or absence of posterior acoustic features , absence of surrounding tissue alterations )  . 
it was decided to include only this type of lesion into category 3 , as inclusion of masses with a single suspicious sign in a previous study [ 20 ] had reduced the npv and increased the ppv by more than 2% . 
in alcuni casi lago - aspirato stato eseguito per volont dei medici curanti o delle pazienti . lo studio ecografico stato eseguito usando un apparecchio siemens antares con trasduttore lineare ad alta frequenza ( 1013 mhz )  . 
lesame ecografico ha incluso lo studio di entrambe le mammelle e della regione ascellare secondo scansioni multiple e si concentrato sullo studio delle caratteristiche morfologiche della lesione da ago - aspirare . tutte le lesioni sono state sottoposte ad ago - aspirato ecoguidato eseguito con ago sottile ( 2125 g )  . 
lesame citologico non stato giudicato attendibile se vi era discordanza tra i risultati dellimmagine ecografica e del prelievo citologico , se il prelievo era insufficiente o se in esso erano state individuate solo cellule parenchimali normali . 
stato considerato un risultato negativo specifico un esame citologico privo di cellule atipiche e compatibile con una diagnosi di cisti complicata , fibroadenoma , galattocele , liponecrosi , granuloma e metaplasia apocrina . 
nei casi di diagnosi citologica negativa specifica la lesione stata inviata ad uno stretto follow - up : ogni 6 mesi per almeno due anni . tutti gli esami ecografici e i successivi ago - aspirati sono stati eseguiti da due radiologi dedicati alla diagnostica senologica ( gli autori mc e pb ) che le hanno descritte e classificate secondo il sistema bi - rads al momento dellesame senza conoscere i risultati istopatologici . 
lesions were assigned to category 4 if they did not meet the requirements for benignity and did not show the combination of at least three suspicious signs , therefore having indeterminate appearance . 
a definitive diagnosis of atypical hyperplasia was classed as a malignant lesion , whereas a definitive diagnosis of typical hyperplasia was classed as a benign lesion . statistical analysis specificity , sensitivity , accuracy , ppv and npv of the birads classification system were calculated by grouping category 3 lesions ( probably benign ) among benign lesions , and category 4 ( probably malignant ) and category 5 ( definitely malignant ) among malignant lesions . 
the ppv and npv of each descriptor was obtained as follows : ppv : number of malignant lesions per sonographic descriptor npv : number of benign lesions per sonographic descripthe 2 and fischer exact tests were used to determine significant differences between the proportions of malignant and benign lesions in the following groups : upper outer quadrant of left breast , including the border areas ( intersection of outer quadrants and upper quadrants ) ( present / absent ) shape ( irregular , oval , round ) diameters less or greater than 1.4 cm orientation ( nonparallel , parallel ) presence or absence of circumscribed margins type of boundary ( abrupt and echogenic halo ) hypoechoic pattern ( presence / absence ) posterior acoustic features ( enhancement , shadowing , none ) alterations of the surrounding tissue ( presence / absence ) category ( 3 , 4 , 5 ) ratio between horizontal and vertical diameter greater or less than 1 cm . to assess the predictive factors for malignant lesions we constructed a logistic regression model . 
the variables included were : shape ( oval ) noncircumscribed margins echogenic halo hypoechoic pattern posterior acoustic features ( enhancement ) surrounding tissue alterations category ( category 3 ) orientation and age ( age group < 53 years )  . regression analysis was conducted using the stepwise procedure with backward elimination ; the hosmer and lemeshow test was used to evaluate the goodness of the model . 
stato deciso di comprendere nelle classe iii solo questo tipo di lesioni dato che in un precedente studio [ 20 ] la presenza di formazioni con un unico segno sospetto in classe iii ne aveva abbassato il valore predittivo negativo e innalzato il valore predittivo positivo oltre il 2% . 
alla iv classe sono state assegnate tutte le lesioni che non soddisfacevano i criteri per le lesioni benigne e che non presentavano la combinazione di almeno tre segni suggestivi di malignit , e che perci apparivano indeterminate . 
una diagnosi definitiva di iperplasia atipica stata considerata come lesione maligna ; per contro una diagnosi definitiva di iperplasia tipica stata considerata come lesione benigna . analisi statistica stata calcolata la specificit , la sensibilit , laccuratezza , il valore predittivo positivo e negativo ( vpp e vpn ) del sistema di classificazione bi - rads , includendo le lesioni di iii classe ( lesioni giudicate probabilmente benigne ) nel gruppo delle lesioni benigne , quelle di iv ( lesioni giudicate probabilmente maligne ) e di v classe ( lesioni giudicate francamente maligne ) nel gruppo delle lesioni maligne . 
patients with bi - rads category 3 and 4 lesions , for which fnac documented a specific benign lesion , were advised to repeat the sonographic examination every 6 months for at least 2 years . mean patient age was 53.2 ( range : 1990 ) years . 
mean lesion dimensions were : horizontal diameter 13.9 mm ( range 390 mm ) and vertical diameter 10.3 mm ( range 380 mm )  . on the basis of the bi - rads classification system , our cases were classed as follows : 63 in category 3 , 94 in category 4 and 135 in category 5 . 
no cases were assigned to categories 0 , 1 , 2 or 6 , in keeping with the inclusion criteria . cytology and histology revealed 168 malignant lesions and 124 benign lesions . 
of the irregular - shaped lesions , 28 were assigned to category 4 ( percentage of category 4 lesions with irregular shape : 29.7% ) and 130 to category 5 ( percentage of category 5 lesions with irregular shape : 96.2% ) ( table 3 )  . costruito un modello di regressione logistica . 
le variabili inserite nel modello sono state : forma ( con riferimento alla caratteristica ovalare ) margini non circoscritti alone iperecogeno ipoecogenecit caratteristiche posteriori ( con riferimento alla caratteristica enhancement ) alterazioni del parenchima circostante classe ( con riferimento la classe iii ) orientamento ed et ( con riferimento al gruppo det < 53 anni )  . lanalisi di regressione stata condotta utilizzando la procedura stepwise con eliminazione a ritroso ( backward elimination ) ; la bont del modello stata valutata utilizzando il test di hosmer e lemeshow . 
le dimensioni medie delle lesioni sono state : diametro orizzontale medio 13 , 9 mm ( range 390 mm ) , diametro verticale medio 10 , 3 mm ( range 380 mm )  . basandoci sulle definizioni proposte dal sistema bi - rads , i nostri casi sono stati classificati nel modo che segue : 63 in classe iii , 94 in classe iv , e 135 in classe v . 
il sistema ecografico bi - rads ha mostrato il 77 , 0% di accuratezza , il 98 , 2% di sensibilit , il 48 , 4% di specificit , con un vpp e un vpn rispettivamente del 72 , 0% e del 95 , 2% ( tabella 2 )  . centocinquantotto casi presentavano morfologia irregolare , 100 ovalare e 34 rotondeggiante . 
delle 158 lesioni con morfologia irregolare , 134 erano maligne e 24 benigne per un vpp e un vpn rispettivamente dell84 , 8% e del 15 , 2% . delle lesioni con morfologia irregolare 28 sono state assegnate alla classe iv ( percentuale di lesioni della iv classe che presentavano morfologia irregolare : 29 , 7% ) e 130 alla classe v ( percentuale di lesioni della classe v con morfologia irregolare : 96 , 2% ) ( tabella 3 )  . i margini erano circoscritti in 80 casi , indistinti in 106 , angolari in 63 , microlobulati in 7 , spiculati in 36 . 
lesame istologico ha confermato una lesione benigna ( fibroadenoma )  . angular in 63 , microlobulated in seven and spiculated in 36 . only eight of 80 lesions ( 10.0% ) with circumscribed margins were found to be malignant , with npv of 90.0%. 
only seven cases had microlobulated margins , and all of table 3 shape descriptor in relation to the breast imaging reporting and data system classification tabella 3 distribuzione della morfologia in relazione alla classificazione bi - rads total totale category diagnosis round oval irregular totals b . 
2 small , round , hypoechoic mass with indistinct margins , abrupt interface , and absence of posterior acoustic features ( breast imaging reporting and data system category 4 )  . 
si trattava di un carcinoma duttale invasivo . ipoecogene , 134 appartenevano alla v classe ( oltre il 99% di tutte le lesioni di classe v ) , 71 alla classe iv ( il 75 , 5% di tutte le lesioni di classe iv ) e 57 alla classe iii ( il 90% di tutte le lesioni di classe iii )  . 
tale parametro si dimostrato essere inversamente proporzionale alla classe di sospetto ( da 1 , 82 a 1 , 12 )  . dei 292 casi 200 presentavano uninterfaccia netta e 92 un alone iperecogeno . 
di 292 casi , 167 ( il 42 , 8% ) hanno mostrato assenza di segni acustici posteriori e la gran parte di queste lesioni stata assegnata alla iv classe . 
su 22 lesioni che presentavano rinforzo acustico posteriore , 16 si sono rivelate benigne ( vpn del 72 , 7% ) e 6 maligne ( 3 poste in iv classe , 1 in iii e 2 in v )  . 
of the 262 hypoechoic lesions , 134 were category 5 ( more than 99% of all category 5 lesions ) , 71 were category 4 ( 75.5% of all category 4 lesion ) and 57 were category 3 ( 90% of all category 3 lesions )  . 
solo 18 lesioni ( 17 maligne e 1 benigna ) hanno mostrato distorsione del parenchima circostante ( tabella 9 )  . la maggior parte dei casi assegnati alla iv classe presentavano ecostruttura ipoecogena e margini indistinti . 
come si osserva nella tabella 10 , lunica variabile che non ha riportato differenze significative tra i due gruppi di lesioni lassociazione della lesione maligna con il quadrante supero - esterno della mammella sinistra , che presenta un livello di p = 0 , 669 . relativamente ai risultati dellanalisi multivariata , la regressione logistica ha permesso di valutare la stima del rischio di avere una lesione maligna , sotto forma di odds ratio ( or ) ed i relativi intervalli di confidenza al 95% ( ic 95% )  . utilizzando questa metodica , per valori di or superiori ad 1 si considera che il fattore di esposizione sia un fattore di rischio , mentre per valori inferiori a 1 si considera che il fattore di esposizione sia un fattore protettivo . 
fra le covariate inserite nel modello quelle che sono risultate avere un rischio significativamente maggiore di avere lesioni maligne ( or significativamente maggiore di 1 ) sono : la morfologia rotondeggiante rispetto alla ovalare , al limite della significativit con p = 0 , 52 la morfologia irregolare rispetto alla ovalare con p = 0 , 008 lassenza di caratteristiche acustiche posteriori rispetto allenhancement con p = 0 , 025 infine le classi 4 e 5 rispetto alla 3 , con rispettivamente p = 0 , 001 e p < 0 , 001 . il test di hosmer e lemeshow , con un p = 0 , 37 , indica che il modello utilizzato nella regressione buono per predire la fig . 
relativamente alla forma , il rischio di avere una lesione maligna particolarmente elevato nelle donne che presentano una forma irregolare ( rischio pi di 3 , 5 volte maggiore rispetto a coloro che hanno una lesione con forma ovalare ) , mentre coloro che presentano una lesione rotondeggiante hanno un rischio che tale lesione sia maligna poco pi di 2 , 5 volte rispetto a coloro che hanno una lesione con forma ovalare . 
of the 22 lesions with posterior enhancement , 16 proved to be benign ( npv 72.7% ) and six malignant ( three in category 4 , one in category 3 and two in category 5 )  . 
only 18 lesions ( 17 malignant and one benign ) showed parenchymal distortion ( table 9 )  . the majority of cases assigned to category 4 had hypoechoic echo pattern and indistinct margins . 
as can be seen in table 10 , the only variable that did not differ significantly between the two groups was location of the malignant lesion in the upper outer quadrant of the left breast , for which the p value was 0.669. with regard to multivariate analysis , logistic regression was used to estimate the risk of having a malignant lesion , in the form of odds ratio ( or ) and corresponding 95% confifig . 
si trattato di un caso falso positivo . table 9 surrounding tissue alterations in relation to the breast imaging reporting and data system classification tabella 9 alterazioni del parenchima circostante secondo la classificazione bi - rads category diagnosis no alterationssurrounding tissue alterations totals b , benign ; m , malignant classe diagnosi nessuna alterazione alterazioni del parenchima circostante totale b , benigno ; m , maligno total totale m . 
of the covariates included in the model , those associated with a significantly higher risk of having a malignant lesion ( or significantly > 1 ) are : round rather than oval shape , almost significant with p = 0.52 irregular rather than oval shape ( p = 0.008 ) absence of posterior acoustic features rather than enhancement ( p = 0.025 ) categories 4 and 5 rather than category 3 , with p = 0.001 and p < 0.001 , respectively the hosmer and lemeshow test , with a p = 0.37 , indicates that the model used in regression was good for predicting the outcome variable of having a malignant lesion . multivariate analysis clearly showed that the risk of having a malignant lesion is particularly high in women with senza caratteristiche acustiche posteriori rispetto al quelle che presentano enhancement ( tabelle 10 , 11 )  . discussione per la frequente sovrapposizione di segni benigni e maligni , i noduli mammari studiati ecograficamente vengono spesso sottoposti a biopsia per determinarne la natura [ 912 ]  . 
il gran numero di biopsie eseguite su lesioni benigne o per desiderio delle pazienti o per lincertezza del medico o per lindicazione di alcuni protocolli , rappresenta un ulteriore problema [ 21 ]  . 
infatti , un eccessivo numero di biopsie non necessarie ha un effetto svantaggioso determinando laumento dei costi dei programmi di screening e di tutela della salute pubblica [ 10 , 21 , 22 ]  . lecografia mammaria non sfruttata al massimo delle sue potenzialit se il suo utilizzo viene limitato alla sola capacit di differenziare le lesioni liquide da quelle solide o alm . 
the p values for the variable category show higher statistical significance . with regard to shape , the risk of having a malignant lesion is particularly high in women with irregularly shaped lesions ( 3.5 times higher risk compared with those with an oval lesion ) , whereas women with a round lesion are a little more than 2.5 times more likely to have a malignant lesion than those with an oval lesion . 
al fine di diminuire il numero di biopsie non necessarie , lecografia dovrebbe tendere ad una sempre pi precisa caratterizzazione delle lesioni [ 6 , 7 , 12 ]  . 
tale sistema aiuta il radiologo nella descrizione delle caratteristiche ecografiche e nellassegnazione ad una classe definitiva di appartenenza alla quale associato il trattamento clinico pi appropriato per la paziente [ 19 ]  . 
se questi criteri fossero strettamente applicati a partire dalliniziale referto radiologico , il numero delle biopsie per le lesioni benigne potrebbe essere ridotto . questo studio conferma lalta sensibilit ( e cio lidentificazione di lesioni maligne in pazienti con tumore al seno , 95 , 3% ) e lalto valore predittivo negativo ( e cio lidentificazione dei veri negativi in donne senza malattia , 92 , 3% ) del sistema ecografico bi - rads . 
performance of too many unnecessary biopsies has detrimental effects that increase the cost of screening and public health protection programmes [ 10 , 21 , 22 ]  . breast us is not used to its full potential if it is limited to the differentiation of cystic and solid lesions or the study of particularly dense breasts . 
 [ 7 ] nella loro ampia casistica hanno riportato un 98 , 4% di sensibilit , un 67 , 8% di specificit , un 38% di vpp , un 99 , 5% di vpn e un 72 , 9% di accuratezza . 
nello studio di stavros , il vpp era significativamente pi basso rispetto al nostro ( 38% vs 72% ) , probabilmente in relazione alla diversa prevalenza di tumori mammari ( 17% vs 57% ) e ai diversi criteri di selezione delle pazienti . 
nel nostro studio laccuratezza diagnostica dellecografia ( 77 , 0% ) nella differenziazione delle lesioni mammarie benigne e maligne attraverso luso del sistema classificativo bi - rads stata simile ai risultati ottenuti nello studio di stravos . nel nostro studio il vpn per la iii classe stato pari al 95 , 3% . 
in our study , the diagnostic accuracy of us ( 77.0% ) in differentiating benign from malignant breast lesions through the use of the bi - rads classification system was similar to that obtained by stavros et al . 
because only lesions studied by cytology and / or histology were included in this study , only a small number of women with probably benign lesions and with a known diagnosis were included , and in these cases , the decision to perform cytology was made by the patient or the referring physician . the risk of malignancy for category 3 lesions should be lower than 2% . 
if the apparently benign mass increases in size during follow - up , lesion classification is changed to category 4 and a biopsy becomes appropriate [ 19 , 22 ]  . 
solo le lesioni che sono state sottoposte allesame citologico e / o istologico sono state inserite in questo studio , perci solo un piccolo numero di donne con delle lesioni probabilmente benigne e con diagnosi nota sono state incluse . 
in questi casi lesame citologico stato eseguito per scelta della paziente o del medico curante . il rischio di malignit per le lesioni assegnate alla classe iii dovrebbe essere inferiore al 2% . 
se la massa apparentemente benigna aumenta di dimensioni durante il follow - up , si modifica trasformandosi in una lesione di classe iv , perci lesame bioptico a questo punto appare appropriato [ 19 , 22 ]  . 
nessuna delle lesioni della nostra casistica attribuite alla iii classe ha mostrato modificazioni morfologiche o dimensionali durante il follow - up ( anche se non abbiamo il follow - up completo di tutte le pazienti )  . nel nostro studio , i vpp per le classi iv e v sono stati rispettivamente del 48 , 9% e 88 , 1% . 
in questa categoria lorientamento e le caratteristiche morfologiche costituiscono i segni pi validi per differenziare le lesioni benigne da quelle maligne . solo un piccolo numero di casi posti in iv classe ha mostrato alone iperecogeno o segni acustici posteriori e in nessun caso si sono documentate alterazioni del parenchima circostante . comunque questi criteri non sono stati sufficienti per discriminare le lesioni maligne da quelle benigne ed stato sempre necessario ricorrere alla biopsia . 
delle lesioni assegnate alla v classe ( 135 ) , 119 si sono rivelate maligne e 16 benigne . queste lesioni hanno presentato almeno tre segni sospetti per la malignit : morfologia irregolare , margini non circoscritti , orientamento anti - parallelo , alone iperecogeno e presenza di sbarramento acustico posteriore o di alterazioni del tessuto circostante . 
these lesions displayed at least three suspicious signs : irregular shape , noncircumscribed margins , nonparallel orientation , echogenic halo and presence of posterior shadowing or alterations of the surrounding tissue . lesion morphology is one of the most reliable criteria for differentiating benign and malignant breast masses . 
round shape proved to be a nonspecific sign . margin evaluation revealed that only 36 lesions had spiculated margins , and these were classified as category 4 or 5 . the relatively small number of masses with spiculated margins is probably due to the small size of the lesions studied ( mean diameter among category 5 lesions was less than 13 mm ) , the introduction of new margin descriptors ( angular and microlobulated ) and the fact that an echogenic halo often reflects the presence of spiculations that are too small to be detected on us . 
hypoechoic pattern had a lower ppv compared with irregular shape or noncircumscribed margins , but this variable increases in reliability if it is associated with other suspicious signs . in agreement with other authors [ 5 , 2427 ] , lesion shape , margins and echo pattern were the most significant factors in the differential diagnosis between benign and malignant lesions . 
the variable orientation was closely related to lesion shape ; generally , all oval lesions tended to have parallel orientation . irregular morphology was often found to be associated with nonparallel orientation . 
in our study , parallel orire risultata associata con il pi alto vpp ( 84 , 8% ) , mentre la morfologia ovalare con il pi alto vpn ( 80 , 0% )  . 
il relativo basso numero di masse a margini spiculati probabilmente dovuto alle piccole dimensioni delle lesioni studiate ( il diametro medio delle lesioni poste in classe v stato inferiore a 13 mm ) , allintroduzione di nuovi descrittori dei margini ( angolari e microlobulati ) e al fatto che lalone iperecogeno in molti casi espressione della presenza di spicule troppo piccole per essere visualizzate ecograficamente . 
leco - pattern ipoecogeno ha mostrato un vpp pi basso rispetto alla morfologia irregolare o ai margini non circoscritti , ma lattendibilit di questo parametro aumenta se si associa ad altri segni di sospetto . in accordo con altri autori [ 5 , 2427 ] la morfologia , i margini e leco - pattern rappresentano i fattori pi significativi per la diagnosi differenziale benigno / maligno in ecografia . 
il vpp del segno antiparallelo stato del 71 , 5% ( 85 , 9% per le lesioni poste in classe v e 66 , 6% per quelle poste in classe iv )  . 
 [ 25 ] nel valutare gli aspetti caratteristici dei noduli maligni hanno incluso come parametro un rapporto tra diametro trasversale e antero - posteriore pari o inferiore a 1 , 4 . 
i nostri risultati confermano questo valore come soglia significativa per assegnare la lesione alla classe iii ( 1 , 82 ) o alle classi iv e v ( 1 , 46 e 1 , 12 )  . 
linterfaccia netta di contro ha mostrato un vpn pari al 73 , 5% . la presenza di sbarramento acustico posteriore il risultato dellattenuazione degli ultrasuoni da parte della reazione desmoplastica tipica del cancro mammario [ 6 ]  . 
despite the fact that posterior attenuation is more commonly associated with malignant breast lesions , this sign may also be seen in benign lesions [ 6 , 28 ]  . 
in agreement with other authors [ 7 , 24 ] , both types of transmission were considered nonspecific signs . most of our cases showed no alteration of the surrounding tissue , probably as a result of the small size of lesions . 
only 17 tumours had distortion of the surrounding tissue or skin thickening . conclusions our study confirmed that the bi - rads classification system proposed by the acr is an accurate system for the description and management of breast masses . 
in the analysis of our results , we noted that some sonographic signs , such as hypoechoic pattern and indistinct margins , are often less predictive of malignancy if compared with irregular shape ; spiculated , angular or microlobulated margins ; echogenic halo ; and posterior acoustic shadowing . 
on the other hand , some sonographic signs normally associated with benign lesions , such as round shape , abrupt interface and the absence of posterior acoustic signs , are often seen in malignant lesions . oval shape , parallel orientation and circumscribed margins are the signs that best characterise benign lesions . however , regardless of ppv or npv of each sign , the heterogeneous nature of tumours calls for a global assessment based on the combination of multiple signs . 
this is the only method that achieves a more reliable discrimination between benign lesions or lesions with a low likelihood of malignancy ( displaying a combination of signs predictive of benignity ) and malignant lesions or lesions with some likelihood of malignancy ( displaying a combination of signs predictive of malignancy )  . if judgement is based on a meticulous description of lesions and the correct combination of signs , minimally or highly suspicious lesions requiring biopsy may be distinlesioni hanno rivelato la presenza di sbarramento acustico posteriore : il vpp per questo segno stato del 73 , 8% ( 82 , 35% per la classe v e 66 , 66% per la classe iv )  . 
malgrado lattenuazione posteriore sia un segno ecografico pi comunemente associato a lesioni mammarie maligne , questo stesso reperto ecografico pu essere rilevato anche in lesioni benigne [ 6 , 28 ]  . 
bench la presenza di sbarramento sia preoccupante come segno ecografico per la possibile malignit della lesione , noi riteniamo che n una normale trasmissione degli ultrasuoni n una trasmissione con enhancement possa essere usata come elemento di rassicurazione circa la benignit della lesione . 
in accordo con altri autori [ 7 , 24 ] , entrambe le modalit di trasmissione vengono considerate segni aspecifici . la maggior parte dei nostri casi non ha mostrato alterazioni del parenchima circostante probabilmente in relazione alle piccole dimensioni delle lesioni . 
solo 17 tumori hanno presentato distorsione del parenchima circostante o ispessimento cutaneo . conclusioni il nostro studio ha confermato che il sistema di descrittori bi - rads proposto dallacr costituisce un accurato sistema per la descrizione e il management delle lesioni mammarie . nellanalisi dei nostri risultati abbiamo notato che alcuni segni ecografici come lipoecogenicit e i margini indistinti sono spesso meno predittivi di malignit se confrontati con la forma irregolare , i margini spiculati , angolari o microlobulati , lalone iperecogeno e lo sbarramento acustico posteriore . 
daltra parte alcuni segni ecografici abbinati generalmente alle lesioni benigne hanno spesso dimostrato di essere associati anche a lesioni maligne come , nello specifico , la morfologia rotondeggiante , linterfaccia netta e lassenza di segni acustici posteriori . 
la morfologia ovalare , lorientamento parallelo , i margini circoscritti sono i segni che caratterizzano meglio le lesioni benigne . a prescindere dal valore predittivo positivo o negativo di ogni segno , a causa delletereogeneit delle forme tumorali , necessaria una valutazione complessiva della lesione basata sullassociazione di molteplici segni . 
questo lunico modo per distinguere con maggior attendibilit le lesioni benigne o quelle con bassa probabilit di essere maligne ( per le quali esiste unassociazione di segni predittivi di benignit ) da quelle maligne o con pi o meno alta probabilit di malignit ( per le quali esiste unassociazione di pi segni predittivi di malignit )  . basandoci su una scrupolosa descrizione delle lesioni e su una corretta associazione di diversi segni , le lesioni minimamente o altamente sospette che richiedono lesecuzione di una biopsia possono essere distinte dalle lesioni probabilm . 
it is , in fact , very unlikely that an apparently benign lesion will be found to be malignant , and the reason for this is the high npv of us . 
we believe that only through experience and a careful periodic review of cases is it possible to achieve an accurate interpretation of sonographic descriptors . mente benigne che possono essere sottoposte ad un stretto follow - up . 
da una casistica di 468 pazienti con diagnosi istologica di neoplasia mammaria maligna sottoposte a rmm , abbiamo estrapolato 27 casi ( 5 , 7% ) di neoplasie rare , confermate alla diagnosi istologica definitiva : 4 ( 0 , 9% ) carcinomi papillari intracistici , 4 ( 0 , 9% ) carcinomi papillari intraduttali , 5 ( 1 , 0 % ) carcinomi papillari invasivi , 2 ( 0 , 4% ) carcinomi midollari , 7 ( 1 , 5% ) carcinomi mucinosi , 3 ( 0 , 6% ) carcinomi tubulari , 1 ( 0 , 2% ) carcinoma tubulo - lobulare e 1 ( 0 , 2% ) tumore desmoide . 
di frequente le neoplasie maligne rare della mammella , verosimilmente a causa dellelevato grado di differenziazione e delle peculiarit istologiche , presentano alla rmm caratteristiche morfologiche e di enhancement poco sospette e vengono classificate come lesioni dubbie / indeterminate . key words breast magnetic resonance mammography breast rare neoplasms parole chiave mammella risonanza magnetica mammaria tumori mammari rari introduction introduzione breast cancer is a major public health issue worldwide . 
according to estimates , in 2002 , there were more than one million new breast cancer diagnoses , more than 400 , 000 deaths il tumore della mammella attualmente uno dei principali problemi di salute pubblica su scala mondiale . 
breast cancer is an extremely heterogeneous disease , with a wide variety of clinical presentations and stages at presentation , biological behaviour , histological features , imaging findings , responses to treatment and prognostic features . 
the two most common histological types of breast cancer are ductal and lobular carcinomas , constituting approximately 75% and 15% of all breast neoplasms , respectively [ 2 ]  . 
this may explain why almost all of the literature about breast neoplasms is focused on the epidemiological , pathological , imaging and clinical features of these histological types , whereas much less is known about the rarer types of breast cancer , which together account for about 10% of all cases [ 3 ]  . over the last few years , magnetic resonance mammography ( mrm ) has gained increasing importance in the field of breast imaging . 
scientific evidence from many large - scale trials has confirmed the high efficacy of mrm for the diagnosis of primary and recurrent breast cancer , with reported sensitivity approaching 100% [ 46 ]  . 
the most important indications for mrm are cancer detection in young women with a genetic - hereditary risk of breast carcinoma [ 7 , 8 ] , in patients with carcinoma of unknown primary ( cup ) syndrome [ 9 , 10 ] and in women with breast implants [ 11 ] ; characterisation of equivocal mammographic and / or sonographic findings [ 12 ] ; local staging before surgical intervention [ 1315 ] or as preand post - neoadjuvant chemotherapy examination [ 16 , 17 ] and follow - up after breast - conservative surgery / radiotherapy [ 1820 ]  . 
to make the most of this diagnostic tool , now that its use is becoming increasingly widespread , it is imperative to be familiar with the mrm appearance of breast cancer of cases showing both usual and unusual semiological features . whereas much is known about the mrm appearance of the most frequently encountered histological breast cancer subtypes , ductal and lobular invasive carcinomas [ 21 ] , much less is known about mrm appearance of rare histological types [ 2226 ]  . 
on the other hand , rare tumours constitute a remarkable proportion of breast neoplasms and can be found rather frequently in some groups of women who might take particular advantage of mrm , namely , carriers of brca 1 germline mutations ( medullary carcinoma ) [ 27 ] , patients with nipple discharge ( papillary carcinoma ) [ 28 , 29 ] and women with gardners disease ( desmoid tumour ) [ 30 ]  . the purpose of this study is to describe mrm features of rare malignant neoplasms of the breast , utilising data from the literature and from our experience . materials and methods patients out of 468 patients with a breast malignancy who between september 2003 and june 2006 underwent preoperative ne di nuovi casi , oltre 400000 sono state le morti causate dalla neoplasia mammaria e pi di 4 milioni di donne ne sono attualmente affette [ 1 ]  . 
la patologia neoplastica mammaria estremamente eterogenea , abbracciando una vastissima gamma di modalit e stadi di presentazione , comportamento biologico , caratteristiche istologiche , aspetto radiologico , risposta ai vari tipi di trattamento e caratteristiche prognostiche . 
ci spiega perch la quasi totalit della produzione medica scientifica in ambito senologico sia incentrata sulla valutazione degli aspetti epidemiologici , patologici , radiologici e clinici dei suddetti istotipi e molto minore sia stata lattenzione per istotipi pi rari che , nel complesso , costituiscono il 10% delle neoplasie mammarie [ 3 ]  . negli ultimi anni , la risonanza magnetica mammaria ( rmm ) ha guadagnato un ruolo sempre pi importante nella diagnostica senologica . 
numerosi studi su larga scala hanno infatti messo in evidenza lelevata efficacia della rmm nellidentificazione di carcinomi mammari , sia primitivi che esito di recidive , con valori di sensibilit che possono raggiungere il 100% [ 46 ]  . 
in particolare le sue applicazioni principali sono lidentificazione di neoplasie mammarie in giovani donne ad alto rischio genetico [ 7 , 8 ] , in pazienti con cup syndrome [ 9 , 10 ] e con protesi mammarie [ 11 ] , la caratterizzazione di reperti mammografici ed ecografici di incerto significato diagnostico [ 12 ] , il bilancio di estensione di neoplasie gi istologicamente diagnosticate [ 1315 ] o nella valutazione pree post - chemioterapia neoadiuvante in caso di tumori localmente avanzati [ 16 , 17 ] e il follow - up post chirurgia conservativa / radioterapia [ 1820 ]  . 
per poterne sfruttare a pieno le potenzialit , oggi che questa metodica si sta diffondendo su larga scala , fondamentale che i radiologi entrino sempre pi in confidenza con la semeiotica della rmm , imparando a riconoscere sia gli aspetti tipici che atipici orientativi verso neoplasie mammarie . sebbene al momento attuale siano gi noti molti aspetti relativi alla semeiotica rmm delle neoplasie mammarie pi frequenti carcinoma duttale e lobulare infiltrante [ 21 ] sono molto meno conosciute le caratteristiche delle neoplasie maligne rare della mammella [ 2226 ]  . 
all 5 invasive papillary carcinomas were histological grade 2 ( according to elston - ellis ) , both medullary carcinomas were grade 3 , 3 / 7 mucinous carcinomas were grade 1 and 4 / 7 were grade 2 , all three tubular carcinomas were grade 1 and the tubulo - lobular carcinoma was grade 2 . with respect to hormone receptor status , 20 ( 74% ) patients had estrogen - receptor - positive / progesterone - receptor - positive ( er + / pr + ) tumours , 3 ( 11% ) had er - / prtumours , 1 ( 4% ) had an er + / prtumour and in 3 ( 11% ) cases hormone receptor profile was assessed . 
patients age ranged from 33 and 77 ( mean age 60 ) years . biopsies were performed under sonographic guidance in 25 cases , by using a 14 - gauge automated or semiautomated device ; and under stereotactic guidance in two cases , by an 11 - gauge directional vacuum - assisted biopsy probe . 
histological diagnoses were confirmed by pathological analysis of the surgical specimens ( 24 lumpectomies and 3 mastectomies )  . mrm technique in 20 cases , mrm was performed with a 1.5 - t system ( magnetom , avanto , siemens medical system , erlangen , germany ) with a dedicated bilateral breast surface coil and the patient in prone position . 
t1 - weighted images were acquired using a 3d fast low - angle shot ( flash ) pulse sequence with the following imaging parameters : tr / te 15 / 4.7 ms ; flip angle 25 ; matrix 197448 ; field of view 350175 mm ; section thickness 1.8 mm ; scanning time 88s . 
in the remaining seven cases , mrm scans were obtained using a 1 - t system ( magnetom impact , siemens , erlangen , germany ) with a dedicated bilateral breast surface coil and the patient in prone position . 
t1 - weighted 3d flash images were obtained with imaging parameters of tr / te 14 / 7 ms ; flip angle 25 ; matrix 192256 ; field of view 320160 mm ; section thickness 2.5 mm ; acquistition time 84s . gadopentetate dimeglumine ( magnevist , schering berlin , germany ) was administered iv as a bolus injection at a dose of 0.1 mmol / kg body weight at a flow rate of 2 ml / s followed by a 20 - ml saline flush . 
the images obtained underwent postprocessing : subtraction of the precontrast images from the postcontrast ones , and multiplanar reconstrucmateriali e metodi pazienti da 468 pazienti con neoplasia mammaria che , tra settembre 2003 e giugno 2006 , sono state sottoposte a rmm preoperatoria per bilancio di estensione , sono stati estrapolati 27 ( 5 , 7% ) casi di neoplasia mammaria maligna di istotipo raro ( secondo la classificazione who )  . 
in particolare : 13 ( 2 , 8% ) carcinomi papillari di cui 4 ( 0 , 9% ) carcinomi papillari intracistici , 4 ( 0 , 9% ) carcinomi papillari intraduttali , 5 ( 1 , 0 % ) carcinomi papillari invasivi ; 12 ( 2 , 5% ) varianti di carcinoma duttale infiltrante ( cdi ) di cui 2 ( 0 , 4% ) carcinomi midollari , 7 ( 1 , 5% ) carcinomi mucinosi e 3 ( 0 , 6% ) carcinomi tubulari ; 1 ( 0 , 2% ) carcinoma tubulo - lobulare e 1 ( 0 , 2% ) tumore desmoide ( fibromatosi extra - addominale )  . 
i 5 carcinomi papillari invasivi presentavano tutti grado istologico 2 secondo elston ellis , i 2 carcinomi midollari grado 3 , 3 / 7 carcinomi mucinosi grado 1 e 4 / 7 grado 2 , tutti i carcinomi tubulari grado 1 ed il carcinoma tubulo - lobulare grado 2 . lo stato recettoriale in 20 ( 74% ) pazienti era positivo sia per estrogeni che per progesterone , in 3 ( 11% ) era negativo , in 1 ( 4% ) caso positivo per estrogeni e negativo per progesterone e in 3 ( 11% ) casi non stato valutato . 
lesame istologico dei linfonodi ascellari ha evidenziato metastasi linfonodali in 2 casi ( 7% ) , entrambi carcinomi midollari . let delle pazienti risultava compresa tra 33 e 77 anni , con media di 60 anni . 
 la diagnosi di neoplasia mammaria stata posta mediante biopsia percutanea con prelievo microistologico sotto guida ecografica in 25 casi ( ago da 14 g , dispositivi di prelievo automatici o semi - automatici ) e sotto guida stereotassica in 2 casi ( mammotome 11 g ) e confermata sul campione operatorio ( 24 quadrantectomie e 3 mastectomie )  . esame rmm in 20 pazienti lesame stato effettuato con un magnete da 1 , 5 t ( magnetom , avanto , siemens medical system , erlagen , germania )  . 
stata eseguita una sequenza flash 3d utilizzando i seguenti parametri : tr / te = 15 / 4 , 7 ms ; flip angle 25 ; matrice 197448 pixel ; fov 350175 ; spessore 1 , 8 mm ; tempo di acquisizione 88 secondi . 
nelle rimanenti 7 pazienti la rmm stata eseguita con un sistema a 1 t ( magnetom impact , siemens , erlangen , germania ) , anche in questo caso in posizione prona e con bobina di superficie bilaterale dedicata . 
sono state eseguite sequenze flash 3d con i seguenti parametri : tr / te = 14 / 7 ms ; flip angle 25 ; matrice 192256 pixel ; fov 320160 ; spessore di 2 , 5 mm ; tempo di acquisizione 84s . in tutti i casi le immagini sono state acquisite sul piano coronale in una acquisizione precedente e in cinque successive alliniezione endovenosa di 0 , 1 mmol di gd - dtpa / kg di peso corporeo alla velocit di 2 ml al secondo , seguita a . 
in particular , morphological criteria included shape ( round , oval , dendritic , irregular ) ; borders ( well - defined , ill - defined ) ; pattern of contrast enhancement [ homogeneous , inhomogeneous and rim - like ( stronger enhancement of the peripheral portion of the lesion and delayed , slight enhancement of tumour core )  . 
kinetic criteria were enhancement rate that is the relative signal intensity increase that occurs in the first postcontrast minute ( less than 50% , between 50% and 100% , more than 100% ) and morphology of time - intensity curves ( continuous increase , type i ; plateau , type ii ; washout , type iii )  . 
the readers indicated a level of diagnostic suspicion and classified each lesion in one of five classes according to the breast imaging reporting and data system ( bi - rads ) [ 32 ]  . results one intracystic papillary carcinoma and one invasive papillary carcinoma were not detected at mrm . 
the former had been identified at mammography as a cluster of pleomorphic microcalcifications ( 10 mm ) , whereas the latter was a tiny ( 5 mm ) , hypoechoic , nonvascular mass unidentifiable at mammography . 
pathological examination of surgical specimens revealed the presence of neoplasms in both cases . the morphological and kinetic features of papillary neoplasms proved to be quite variable ( table 1 )  . 
enhancement rates were variable ( less than 50% , 33% ; between 50% and 100% , 33% ; and more than 100% , 33% ) , and time - intensity curves were type i in 1 case ( 33% ) and type ii in 2 cases ( 66% )  . intraductal papillary carcinomas presented as spiculated or irregular masses in 3 cases ( 75% ) and as an oval - shaped mass in 1 case ( 25% ) , with well - defined margins in 75% of cases and homogeneous enhancement pattern in 50% and inhomogeneous in the remaining cases . 
in all cases , the enhancement rate was less than 100% ( in 3 cases less than 50% ) , with type i ( 50% ) and ii kinetic curves ( 50% )  . the 4 ( 80% ) invasive papillary carcinomas detectable at mrm , demonstrated a wide range of shapes ( oval 50% , spiculated 25% and irregular 25% ) , with mainly ill - defined margins ( 75% ) and inhomogeneous ( 75% ) or rim - like ( 25% ) enhancement patterns . 
posizionando una regione dinteresse ( roi ) sulle focalit evidenti sono state costruite curve delle variazioni di intensit di segnale / tempo . valutazione delle immagini le immagini sono state valutate in consenso da due radiologi esperti in diagnostica senologica . 
in particolare i parametri morfologici descritti includevano : forma della lesione ( rotondeggiante ; ovalare ; spiculata ; irregolare ) , margini ( ben definiti ; mal definiti ) e pattern di enhancement ( omogeneo ; disomogeneo ; rim - like enhancement accumulo di mezzo di contrasto ( mdc ) prevalentemente nella porzione periferica della lesione , con aspetto ad anello , ed eventuale riempimento tardivo della porzione pi centrale ) ; mentre quelli cinetici comprendevano lenhancement rate , cio lincremento relativo dellintensit di segnale nel primo minuto dopo la somministrazione di mdc ( inferiore al 50% , compreso tra 50% e 100% , superiore al 100% ) e laspetto della curva cinetica intensit - tempo ( incremento progressivo e graduale , tipo i ; rapido wash in e successivo plateau , tipo ii ; rapido wash in e wash out , tipo iii )  . 
i lettori hanno inoltre classificato le lesioni in base al grado di sospetto radiologico , secondo una scala da 1 a 5 in relazione al breast imaging reporting and data system ( bi - rads - mri ) [ 32 ]  . risultati uno dei carcinomi papillari intracistici e uno dei carcinomi papillari invasivi non sono risultati identificabili alla rmm . nel primo caso la lesione si presentava mammograficamente come un focolaio di microcalcificazioni a morfologia plemorfa con estensione di 10 mm , mentre nel secondo caso si trattava di una minuta ( diametro di 5 mm ) formazione solida ipoecogena , non vascolarizzata , non evidente alla mammografia . 
lenhancement rate risultato variabile ( inferiore al 50% , 33% ; compreso tra 50% e 100% , 33% ; superiore a 100% , 33% ) e la curva cinetica risultata di tipo i in 1 ( 33% ) caso e di tipo ii in 2 ( 66% ) casi . i carcinomi papillari intraduttali si sono presentati con forma spiculata o irregolare in 3 ( 75% ) casi e ovalare in 1 ( 25% ) caso , margini ben definiti nel 75% dei casi e un pata . 
in the upper quadrants of the left breast , an oval , enhancing mass with well - defined borders ( enhancement rate 108% , time - signal intensitive curve type ii ) is shown . 
al passaggio tra i quadranti superiori della mammella sinistra si apprezza unarea focale ovalare a margini ben definiti di intenso enhancement ( enhancement rate : 108% , curva intensit / tempo di tipo ii )  . 
as a result of these features , this lesion was classified as bi - rads 4 . the desmoid tumour appeared on mrm as an irregular focal area with well - defined borders , mildly and inhomogeneously hyperintense after contrast administration ( enhancement rate less than 50% and type i kinetic curve ) , with nonsuspicious appearance ( bi - rads 2 ) ( table 3 )  . tern denhancement omogeneo nella met dei casi e disomogeneo nella rimanente met . 
lenhancement rate risultato in tutti i casi inferiore al 100% ( in 3 casi inferiore al 50% ) , con curve di tipo i ( 50% ) e ii ( 50% )  . i 4 ( 80% ) carcinomi papillari invasivi identificabili alla rmm hanno dimostrato morfologia variabile ( ovalare , 50% ; spiculata , 25% ; irregolare , 25% ) e , nella gran parte dei casi ( 75% ) , margini mal definiti e pattern denhancement disomogeneo ( 75% ) o tipo rim ( 25% )  . 
in 3 / 4 neoplasie papillari invasive lenhancement rate era superiore al 100% con curva cinetica di iii tipo , mentre nel quarto caso ( 25% ) lincremento iniziale di enhancement era compreso tra 50% e 100% e la curva era di tipo ii . le neoplasie papillari sono state classificate secondo il bi - rads come segue : 1 / 4 ( 25% ) carcinoma papillare intracistico e 1 / 5 ( 20% ) carcinoma papillare invasivo come birads 1 ; 1 / 4 ( 25% ) carcinoma papillare intraduttale come bi - rads 2 ; 2 / 4 ( 50% ) carcinomi papillari intracistici e 3 / 4 ( 75% ) intraduttali come bi - rads 3 ; 1 / 4 ( 25% ) carcinoma papillare intracistico e 2 / 5 ( 40% ) invasivi come bi - rads 4 e , infine , 2 / 5 ( 40% ) carcinomi invasivi come bi - rads 5 . le caratteristiche morfologiche e cinetiche delle varianti di carcinoma duttale infiltrante sono risultate piuttosto eterogenee , con differenze consistenti tra i diversi sottotipi ( tabella 2 )  . 
nessuna delle neoplasie di questo gruppo ha presentato una curva dinamica di tipo iii . i lettori che hanno esaminato i casi hanno espresso un grado di sospetto bi - rads 3 per 3 ( 43% ) dei carcinomi mucinosi e per tutti ( 100% ) i carcinomi tubulari , bi - rads 4 per 4 ( 57% ) neoplasie mucinose e bi - rads 5 per entrambe a . 
in the outer quadrants of the left breast ( arrow ) an irregular , inhomogeneously enhancing mass with ill - defined margins ( enhancement rate 112% , time - signal intensity curve type ii ) can be appreciated . 
al passaggio tra i quadranti esterni della mammella sinistra ( freccia ) evidente unarea focale a morfologia irregolare e margini mal definiti di disomogeneo e intenso enhancement ( enhancement rate : 112% , curva intensit / tempo di tipo ii )  . 
in the upper - outer quadrant of the right breast ( arrow ) , an irregular , mildly enhancing mass ( enhancement rate 70% , time - signal intensity curve type i ) is shown . 
a focal round area with well - defined margins and hypointense central core and peripheral , mild enhancement ( rim - like enhancement ) ( enhancement rate 45% , time - signal intensity curve type i ) is shown in the upper - outer quadrant of the left breast ( arrow )  . 
al quadrante superoesterno della mammella sinistra ( freccia ) , si evidenzia unarea focale a morfologia rotondeggiante e margini ben definiti , con porzione centrale ipointensa e orletto periferico lievemente iperintenso ( rim - like enhancement ) ( enhancement rate : 45% , curva intensit / tempo tipo i )  . 
in the upper quadrants of the left breast , an irregular , ill - defined , inhomogeneously hyperintense mass ( enhancement rate 74% , dynamic curve type ii ) is demonstrated . 
5 carcinoma tubulo - lobulare di grado 2 . nei quadranti superiori della mammella sinistra apprezzabile unarea irregolare a margini poco definiti , disomogeneamente iperintensa ( enhancement rate : 74% , curva cinetica tipo ii )  . 
lesions are identified because they enhance after iv injection of contrast agent , and mrm identifies the angiogenic focus rather than the tumour focus itself [ 21 , 33 , 34 ]  . 
these pathophysiological features seem to account for kinetic signs considered highly suggestive for invasive carcinoma , such as strong enhancement after contrast material injection and decrease of signal intensity in the early postcontrast period ( washout phenomenon )  . 
for example , 48% of lesions identified at mrm had an oval or round shape and 60% smooth margins , both of which are features typically associated with solid benign lesions , such as fibroadenomas [ 43 ] or papillomas , or small foci of fibrocystic change . 
moreover , only 28% and 12% of lesions , repregnazione , con protratta persistenza delliperintensit di segnale ( enhancement rate compreso tra 50% e 100% , curva cinetica di tipo ii ) ( tabella 3 )  . 
in considerazione di tali aspetti i due lettori hanno espresso un grado di sospetto diagnostico bi - rads 4 . laspetto del tumore desmoide risultato quello di unarea focale a morfologia irregolare e a margini netti , lievemente e disomogeneamente iperintensa dopo la somministrazione del mdc ( enhancement rate < 50% e curva cinetica di tipo i ) , presentando un aspetto poco sospetto ( bi - rads 2 ) ( tabella 3 )  . la valutazione globale degli aspetti morfologici e cinetici delle 27 neoplasie di istotipo raro riassunta in tabella 4 . nel complesso , il grado di sospetto espresso dai due lettori per le neoplasie esaminate risultato il seguente : 7 , 5% birads 1 , 7 , 5% bi - rads 2 , 40% bi - rads 3 , 30% bi - rads 4 e 15% bi - rads 5 ( tabella 5 )  . discussione le basi fisiopatologiche della rmm sono lincremento della vascolarizzazione ( densit vascolare ) nella sede della neoplasia , che conduce a un accumulo del mdc , e una aumentata permeabilit capillare , che determina una rapida fuoriuscita di mdc nellinterstizio tumorale . 
per tali motivi la lesione mammaria viene identificata in seguito al netto incremento di intensit rispetto ai tessuti circostanti dopo somministrazione di mdc , con dimostrazione , da parte della rmm , del focolaio angiogenetico piuttosto che della focalit tumorale di per s [ 21 , 33 , 34 ]  . 
questi aspetti fisiopatologici sono in parte in grado di spiegare le caratteristiche cinetiche considerate suggestive di neoplasia mammaria , in particolare lelevato incremento di intensit di segnale dopo mdc e la rapida dismissione dello stesso ( fenomeno descritto dalla curva cinetica tipo wash out )  . 
as a consequence , less than 50% of tumours were properly classified as bi - rads 4 and 5 , whereas 7.5% were interpreted as benign ( bi - rads 2 ) and 40% as probably benign ( bi - rads 3 )  . 
 il valore diagnostico di tali aspetti stato valutato da numerosi autori [ 31 , 3538 ] che , pur sottolineandone lelevato valore predittivo positivo , hanno riscontrato la possibilit che alcune neoplasie mammarie , in particolare le neoplasie intraduttali , i carcinomi lobulari e alcuni istotipi rari , in relazione alle loro specifiche caratteristiche istologiche e pattern di crescita , possano presentarsi in rmm con aspetti suggestivi per formazioni benigne piuttosto che maligne [ 36 , 39 ] o , in alcuni casi , non essere addirittura identificabili [ 4042 ] , originando dei falsi negativi . i risultati della nostra esperienza si pongono in linea con tali osservazioni , dimostrando che le neoplasie mammarie di istotipo raro tendono frequentemente a presentare caratteristiche suggestive di benignit ( 47 , 5% ) o addirittura a non essere riconoscibili alla rmm ( 7 , 5% )  . 
infatti ben il 48% delle neoplasie identificabili alla rmm presentava forma ovalare o rotondeggiante e il 60% margini netti , entrambi aspetti morfologici tipicamente associati a formazioni solide benigne come fibroadenomi [ 43 ] o papillomi , o a piccoli foci di mastopatia fibroso - cistica . 
inoltre solo il 28% e il 12% delle lesioni esaminate , alla valutazione dinamica , hanno dimostrato , rispettivamente , un enhancement rate superiore al 100% e una curva cinetica di tipo iii , altamente suggestivi per neoplasie mammarie maligne . 
come conseguenza di tali modalit di presentazione , meno della met delle lesioni stata classificata correttamente come bi - rads 4 e 5 , mentre il 7 , 5% e il 40% delle neoplasie sono state interpretate rispettivamente come benigne ( bi - rads 2 ) e probabilmente benigne ( bi - rads 3 )  . in particolare , si sono presentati con aspetti poco suggestivi per malignit i tumori papillari intracistici e intraduttali verosimilmente in relazione alla scarsa vascolarizzazione e alle caratteristiche di non invasivit , i carcinomi mucinosi , tubulari e il tumore desmoide . 
a spiegazione dellaspetto presentato dai carcinomi mucinosi , pu essere invocata , come gi commentato in letteratura [ 22 ] , la presenza di abbondante quantit di mucina che rende difficoltosa e lenta la diffusione del mdc allinterno della massa neoplastica . 
labbondante componente fibrosa [ 44 ] potrebbe invece essere responsabile degli aspetti rmm poco sospetti presentati dai carcinomi tubulari [ 45 ] e dei tumori desmoidi [ 46 ]  . 
alcune delle varianti rare di cdi , in particolare i carcinomi mucinosi e i tubulari , e i carcinomi papillari sono estremamente ben differenziati e sono associati a minimo potenziale metastatico e a buona prognosi [ 2 , 48 ]  . 
finally , a relevant role might be played , as hypothesised by mussurakis et al . [ 47 ] , by the high degree of differentiation of these tumours . some special types of idc , such as mucinous and tubular carcinomas and papillary carcinomas , are highly differentiated and are associated with low metastatic potential and a good prognosis [ 2 , 48 ]  . 
most of the tumours we evaluated were grade 1 or 2 , with a positive hormone receptor profile . the only exception was the appearance of medullary carcinomas , which exhibited mrm characteristics highly suggestive of malignancy ( both were classified as bi - rads 5 ) and had , in agreement with the literature [ 2 ] , more aggressive biological features histological grade 3 and negative hormone receptor status than other rare tumours . bi - rads 1 bi - rads 2 bi - rads 3 bi - rads 4 bi - rads 5 bi - rads 1 bi - rads 2 bi - rads 3 bi - rads 4 bi - rads 5 conclusioni 2 ( 7.5% ) 2 ( 7.5% ) 11 ( 40% ) 8 ( 30% ) 4 ( 15% ) 2 ( 7 , 5% ) 2 ( 7 , 5% ) 11 ( 40% ) 8 ( 30% ) 4 ( 15% ) tabella 5 tabella riassuntiva relativa alle classi breast imaging reporting and data system ( bi - rads ) totale ( percentuale ) conclusions analysis of mrm appearance of rare tumours did not reveal any distinctive feature . 
these findings strengthen the concept that mrm must be interpreted in conjunction with the other breast imaging diagnostic examinations and that it cannot replace breast biopsy . dallanalisi delle caratteristiche rmm di tumori di istotipo raro non sono emersi aspetti peculiari , e il dato pi rilevante risultato essere la tendenza di questi a presentarsi come lesioni benigne o poco sospette , o a non essere identificabili allesame rmm . 
bazzocchi1 1istituto di radiologia , azienda ospedaliero - universitaria di udine , via colugna 50 , i - 33100 udine , italy 2diagnostica senologica , aou careggi , viale pieraccini 17 , i - 50139 firenze , italy correspondence to : v . 
all patients underwent mammography , high - frequency broadband us and percutaneous breast biopsy with a 14 - gauge needle and a mean number of five samples ( range 47 passes )  . 
twenty - seven out of 65 dcis at core biopsy were found to have an invasive or microinvasive component at surgical excision , leading to rate of histological underestimation of core biopsy of 41.5%. 
although some histological features ( such as stromal fibrosis , periductal inflammatory infiltrate , high nuclear grade ) can suggest the presence of an invasive component , the sonographic appearance of dcis cannot be used to predict the cases that are underestimated on us - guided core biopsy . nevertheless , a sonographically detectable solid component , either inside dilatated ducts or associated with microcalcifications , and a size greater than 20 mm are frequently associated with the presence of an invasive component . key words ductal carcinoma in situ breast neoplasms diagnosis us breast biopsy riassunto obiettivi . 
tutte le pazienti hanno eseguito lesame mammografico e successivamente ecografico con sonda ad alta frequenza a larga banda , e la biopsia percutanea con aghi da 14 g con un numero medio di 5 frustoli ( range 47 )  . 
ventisette / 65 lesioni con diagnosi bioptica percutanea di cdis sono risultate associate a una componente infiltrante o microinfiltrante allesame istologico definitivo , ottenendo pertanto una sottostima istologica della core - biopsy pari al 41 , 5% . 
lelevata incidenza di sottostime istologiche alla core - biopsy impone un atteggiamento oltremodo prudente di fronte a una diagnosi di cdis effettuata con la core - biopsy stessa . sebbene alcune caratteristiche istologiche presenti nei frustoli bioptici prelevati ( quali la fibrosi stromale , linfiltrato infiammatorio periduttale , lalto grado nucleare ) possano suggerire la presenza di una componente invasiva , le caratteristiche ecografiche dei cdis non possono essere utilizzate per predire i casi che vengono sottostimati alla biopsia percutanea eco - guidata . 
esso viene considerato un potenziale precursore del carcinoma invasivo , a differenza del carcinoma lobulare in situ ( clis ) considerato piuttosto un indicatore di alto rischio per lo sviluppo di tumore alla mammella omolaterale o controlaterale [ 1 , 2 ]  . 
il carcinoma duttale in situ ( cdis ) istologicamente rappresentato da un gruppo eterogeneo di lesioni che presentano differenti caratteristiche istologiche , pattern di crescita , presentazione clinica e comportamento biologico [ 1 ]  . 
lintroduzione dello screening mammografico ha determinato il sempre pi frequente riconoscimento di lesioni subcliniche : il cdis rappresenta il 15%20% di tutti i tumori mammari , e il 25%56% di tutti i tumori clinicamente occulti [ 3 , 4 ]  . 
 la mammografia rappresenta lindagine pi sensibile e pi accurata per la diagnosi dei cdis , con una riduzione della sua accuratezza diagnostica solo nei casi di cdis non associati a microcalcificazioni [ 5 , 6 ]  . 
alla mammografia , dal 62% al 98% dei cdis vengono diagnosticati grazie alla presenza delle microcalcificazioni , mentre solo il 2%23% si manifesta come masse focali o asimmetrie di densit , o come distorsioni architetturali [ 58 ]  . 
in particolare , lecografia potrebbe svolgere potenzialmente alcuni ruoli nella valutazione dei cdis , includendo anche i casi che non si manifestano sotto forma di microcalcificazioni [ 11 ] : lecografia pu essere utilizzata per visualizzare ampi ( > 10 mm ) focolai di microcalcificazioni con forte sospetto di malignit e pu essere utilizzata come guida nelle procedure di biopsia percutanea ; lecografia pu giocare un ruolo importante nella valutazione dei cdis non calcifici , non solo nella identificazione di queste lesioni ma anche nella valutazione della loro estensione ; lecografia pu essere usata per rilevare cdis mammograficamente occulti nelle pazienti con elevata densit mammaria [ 11 , 1517 ]  . tra le varie tecniche di prelievo percutaneo per la caratterizzazione delle lesioni mammarie , ha avuto particolare introduction introduzione ductal carcinoma in situ ( dcis ) is defined as a proliferation of malignant epithelial cells within the ducts and lobules of the breast parenchyma yet without microscopic evidence of invasion through the basement membrane into the periductal stromal tissue . 
it is considered a potential precursor of invasive carcinoma , unlike lobular carcinoma in situ ( lcis ) , which is instead regarded as a high - risk lesion for the development of cancer in the same or contralateral breast [ 1 , 2 ]  . histologically , dcis is not a single entity but a heterogeneous group of lesions that differ in their histopathologic features , growth pattern , clinical presentation and biological behaviour [ 1 ]  . before the widespread diffusion of mammographic screening , dcis was rarely detected , and accounted for only 0.8%5% of all breast cancers [ 3 ]  . 
the introduction of mammographic screening has significantly increased the frequency with which clinically occult breast neoplasms are diagnosed , and dcis now accounts for 15%20% of all detected breast cancers and for 25%56% of all clinically occult cancers [ 3 , 4 ]  . 
 mammography is the primary and most sensitive tool for the detection of dcis , demonstrating a poor performance only in the absence of microcalcifications [ 5 , 6 ]  . 
although mammography identifies most cases of dcis , 6%23% of dcis lesions are not mammographically detectable [ 59 ]  . some recent studies have examined the role of us in the evaluation of mammographically detected microcalcifications [ 1014 ]  . 
in particular , us could have several potential roles in the evaluation of dcis , including those without calcifications [ 11 ] : it can be a useful diagnostic tool in the case of large ( > 10 mm ) clusters of microcalcifications that are highly suspicious for malignancy and can be used as a guide for interventional procedures . it may play an important role in the evaluation of noncalcified dcis , not only in detecting the lesion but also in evaluating its extent . it can be used to reveal mammographically occult dcis in patients with dense breasts [ 11 , 1517 ]  . percutaneous breast biopsy with automatic devices is widely considered one of the most effective techniques for breast lesion characterisation . 
core needle biopsy ( cnb ) is a simple , fast ( with real - time visualisation of needle position during the procedure ) and comfortable technique ( the patient is supine and breast compression is not required ) , and it is v . 
however , in some situations , cnb may underestimate the lesion , as in cases of atypical ductal hyperplasia ( adh ) on cnb that turn out to be dcis on surgical biopsy or dcis on cnb that are found to be invasive ductal carcinomas at final histology on the surgical specimen [ 12 , 13 , 1820 ]  . the purposes of our study were to retrospectively review our series of lesions with a cnb diagnosis of dcis and compare the results with those obtained after surgery and to describe the sonographic appearances of both pure dcis and dcis with an invasive component with a view to identifying possible sonographic features that might be useful in the case of cnb underestimation . materials and methods between 2000 and 2005 , 2 , 423 patients underwent mammography , us and breast cnb under us guidance at our institution . 
all 65 patients with dcis diagnosed at us - guided cnb presented spontaneously to our institution . among these , 44 were asymptomatic and were undergoing routine mammography and sonography , whereas 21 had a palpable nodule ( three with bloody nipple discharge and one with pagets disease )  . 
us examinations were performed with a broadband 5to 12 - mhz linear - array transducer ( hdi 5000 philips - advanced technology laboratories , bothell , wa , usa ) and a broadband 10to 13 - mhz linear - array transducer ( technos esaote )  . 
 sonograms were reviewed for : masses : us features ( hypoechoic , inhomogeneous ) , shape ( round , oval ) , size and margins ( regular or irregular or microlobulated ) architectural distortion ductal changes ( dilatation , extension , duct filled with hyperechoic spots , etc . ) microcalcifications on the basis of mammographic and sonographic features , lesions were classified according to the breast imaging reporting and data system ( bi - rads ) of the american college of radiology [ 21 ] ; in cases of disagreement between the two modalities , we considered the higher bi - rads category . all dcis were sonographically detectable , so the biopsy procedures were performed under us guidance . 
cnb was performed by using an automated gun system ( bard , magnum biopsy instrument , covington , ga , usa ) with 17 - mm sample window and 23 - mm throw or by using a semiautomatic biopsy gun ( precisa , hospital service ) with a 14 - gauge needle . 
la core - biopsy una metodica semplice , rapida ( con la visualizzazione della posizione dellago in tempo reale ) , confortevole per la paziente ( che viene posizionata supina senza necessit di comprimere la mammella ) , meno invasiva e meno costosa della biopsia chirurgica . 
esistono tuttavia delle situazioni nelle quali la diagnosi ottenuta con la biopsia percutanea rappresenta una sottostima istologica , in quanto lesioni diagnosticate come iperplasia duttale atipica ( ida ) possono poi risultare dei cdis o , ancora , lesioni diagnosticate come cdis possono parimenti risultare dei carcinomi duttali infiltranti alla verifica istologica definitiva dopo escissione chirurgica [ 12 , 13 , 1820 ]  . scopo del nostro lavoro stato rivalutare retrospettivamente la nostra casistica riguardante le lesioni mammarie con diagnosi istologica percutanea di cdis , mettendo a confronto i risultati della biopsia percutanea con quelli ottenuti dalla escissione chirurgica , e descrivere le caratteristiche ecografiche del cdis puro e del cdis con componente invasiva , valutando se alcuni aspetti ecografici possono aiutare nella identificazione dei casi sottostimati alla biopsia percutanea . materiali e metodi dal 2000 al 2005 , 2423 pazienti sono state sottoposte a mammografia , ecografia mammaria ( us ) e biopsia mammaria ecoguidata . 
nel contesto di tali diagnosi bioptiche , 65 casi ( 6 , 7% ) erano cdis e 903 ( 93 , 3% ) carcinomi invasivi . le lesioni diagnosticate come cdis alla biopsia percutanea eco - guidata sono state riscontrate in donne che si sono presentate spontaneamente presso il nostro istituto . 
in particolare , 44 pazienti asintomatiche eseguivano i periodici controlli mammografici ed ecografici , mentre 21 pazienti presentavano una massa clinicamente palpabile ( in tre di esse si associava anche una secrezione ematica dal capezzolo , in una paziente una malattia di paget del capezzolo )  . 
abbiamo valutato retrospettivamente soltanto le 65 lesioni diagnosticate come carcinoma duttale in situ , al fine di analizzare le caratteristiche ecografiche e valutare lapporto della core - biopsy con guida ecografica . 
lecografia mammaria stata eseguita mediante sonda lineare broadband da 512 mhz ( hdi 5000 philips - advanced technology laboratories , bothell , wa , usa ) e sonda lineare broadband da 1013 mhz ( technos esaote )  . le ecografie mammarie sono state riviste per la valutazione di : masse : sono state riportate lecogenicit ( ipoecogene , disomogenee ) , la morfologia ( rotonda , ovale ) le dimensioni e le caratteristiche dei margini ( regolari o irregolari o microlobulati ) ; distorsioni architetturali ; v . 
all biopsies were performed with the patient in a supine or supine - oblique position . the mean number of core samples obtained for each lesion was five ( range 47 passes )  . 
le core - biopsies sono state eseguite con dispositivi di prelievo automatico ( bard , magnum biopsy instrument , covington , ga , usa ) o semi - automatico ( precisa , hospital service ) , entrambi con finestra di prelievo di 17 mm e corsa del mandrino di 23 mm , con aghi trancianti da 14 gauge . 
la tecnica utilizzata per eseguire le biopsie ecoguidate con sistema automatico gi stata descritta in precedenza [ 18 , 22 , 23 ]  . tutte le biopsie sono state eseguite con paziente supina o in posizione supina - obliqua , con approccio laterale per le lesioni localizzate ai quadranti esterni , e con approccio mediale per le lesioni localizzate ai quadranti interni . il numero medio dei frustoli bioptici ottenuti per ogni lesione stato di 5 ( intervallo da 4 a 7 passaggi )  . 
tutte le biopsie sono state precedute da uniniezione locale di 5 cc di anestetico ( 2% di mepivacaina , astra zeneca ) attraverso ago da 26 g ( terumo europe nv , leuven , belgio )  . il consenso informato e lanamnesi sulla coagulazione sono stati ottenuti prima della biopsia mammaria , e le eventuali terapie anticoagulanti sono state sospese 3648 ore prima del prelievo . 
i risultati istopatologici della nodulectomia o della mastectomia sono stati confrontable 1 correlation between percutaneous core - biopsy and histologic diagnosis at surgical excision final diagnosis : pure dcis final diagnosis : dcis with invasive component final diagnosis : benign 35 ( 53.9% ) 3 ( 4.6% ) 27 ( 41.5% ) 7 microinvasive 20 invasive tabella 1 confronto tra diagnosi bioptica core - biopsy e diagnosi istologica definitiva ( pezzo operatorio ) diagnosi bioptica core - biopsy diagnosi definitiva ca invasivi diagnosi definitiva benigna cdis 65 35 ( 53 , 9% ) 3 ( 4 , 6% ) 27 ( 41 , 5% ) 7 mic 20 infiltranti percutaneous corebiopsy dcis 65 dcis , ductal carcinoma in situ diagnosi bioptica core - biopsy cdis , carcinoma duttale in situ v . 
1a , b pure ductal carcinoma in situ ( dcis ) ( percutaneous biopsy / surgical excision concordance ) , occult at mammography , in a 48 - year - old asymptomatic patient . 
ventinove su 38 cdis puri ( 76 , 3% ) erano visibili alla mammografia , e il loro aspetto predominante era rappresentato da microcalcificazioni isolate in 22 casi ( 75 , 9% ) , opacit associate o non a microcalcificazioni in 7 casi ( 24 , 1% )  . 
la maggior parte delle lesioni ( 23 / 38 , 60 , 5% ) sono state classificate come sospette allecografia ( 15 / 38 , 39.5% con bi - rads 4 ) o altamente suggestive di malignit ( 8 / 38 , 21% con bi - rads 5 )  . 
2a , b pure ductal carcinoma in situ ( dcis ) ( percutaneous biopsy / surgical excision concordance ) in a 56 - year - old patient , with a palpable mass in the left breast . 
a lecografia dimostra la presenza di una formazione ovalare ipoecogena , a margini in gran parte regolari , al cui interno si apprezzano alcuni spot iperecogeni , corrispondenti alle microcalcificazioni . 
most of these lesions ( 23 / 38 , 60.5% ) were classified as suspicious ( 15 / 38 , 39.5% , birads 4 ) or highly suspicious ( 8 / 38 , 21% , birads 5 ) for malignancy . 
the us features of dcis with invasive component were : solid round masses , hypoechoic , microlobulated , not calcified , highly vascular in 17 cases ( 63% ) solid oval masses , hypoechoic , microlobulated , with internal hyperechoic spots corresponding to microcalcifications in six cases ( 22% ) fig . 
3a , b pure ductal carcinoma in situ ( dcis ) ( percutaneous biopsy / surgical excision concordance ) , occult at mammography , in a 46 - year - old patient with bloody nipple discharge . 
3a , b cdis puro ( concordanza core - biopsy / chirurgia ) occulto alla mammografia , in donna di 46 anni con secrezione spontanea siero - ematica . a lecografia dimostra la presenza di strutture duttali dilatate , con pareti lievemente ispessite e contenenti materiale ecogeno di tipo necrotico . 
tutte le lesioni sono state classificate come sospette per malignit ( bi - rads 4 in 20 / 27 casi , 74% ) o altamente suggestive per malignit ( bi - rads 5 in 7 / 27 casi , 26% ) ( tabella 5 )  . 
 considerando come casi di sottostima istologica solo quelli con infiltrazione ( escludendo cio i cdis microinvasivi , dal momento che le lesioni microinvasive , confrontate con i cdis puri , non differiscono per tasso di recidiva locoregionale , per tasso di sopravvivenza libera da malattia e sopravvivenza totale ) la percentuale di sottostima si ridurrebbe dal 41 , 5% al 31% ( 20 su 65 lesioni )  . la mammografia rappresenta lindagine pi importante e pi sensibile per lidentificazione dei cdis associati a mifig . 
lecografia ( us ) ha avuto finora un ruolo marginale nella diagnosi dei cdis a causa della scarsa visibilit ecografica delle microcalcificazioni , specialmente nel caso di microcalcificazioni isolate o di microcalcificazioni che si sviluppano nel contesto di un parenchima fibro - ghiandolare diffusamente iperecogeno . negli ultimi anni , lintroduzione delle nuove sonde broadband , lineari ad alta frequenza , con maggior risoluzione spaziale e maggior risoluzione di contrasto ( la cos detta ecografia ad alta risoluzione ) ha permesso di incrementare la sensibilit e specificit dellus , e la confidenza diagnostica delloperatore [ 2426 ]  . 
daltra parte ben noto in letteratura che dal 6% al 23% dei cdis risultano mammograficamente occulti [ 4 , 5 , 7 , 9 , 27 ] , percentuale corrispondente al 21 , 5% ( 14 / 65 ) nella nostra casistica . 
essa risulta inoltre meglio tollerata dalle pazienti , rispetto alla guida stereotassica , poich la posizione supina risulta pi confortevole , senza necessit di comprimere la mammella , e la visualizzazione in tempo reale dellago bioptico permette di prelevare in ogni sede della mammella , incluse le regioni periferiche lungo il prolungamento ascellare o la parete toracica in caso di esiti di mastectomia . 
i suoi risultati sono estremamente validi , e se applicata con una metodologia adeguata ( utilizzando aghi da 14 g , con lunga escursione del mandrino , con un minimo di 5 prelievi ) in grado di fornire risultati paragonabili a quelli della biopsia chirurgica , considerata finora il gold standard di riferimento . nella letteratura , considerando le procedure eseguite sia con guida ecografica che mammografica , la concordanza con la biopsia chirurgica compresa tra l80% e il 96% . nella nostra serie consecutiva di 2423 core - biopsy ecoguidate con ago da 14 g , in 65 casi stato diagnosticato un cdis , mentre allesame istologico post - chirurgico stata riscontrata la presenza di una componente infiltrante in 27 casi ( 41 , 5% )  . 
 nonostante lelevata concordanza tra i risultati istologici ottenuti con la scnb ( stereotactic core needle biopsy ) e la successiva escissione chirurgica , molti autori hanno riportato percentuali variabili ( dal 15% al 36% ) di cdis senza fig . 
allecografia si evidenzia piccolo nodulo ( 5 mm ) , tenuemente ipoecogeno , microlobulato , con buona trasmissione del segnale acustico posteriore ; si riconosce tenue alone iperecogeno perilesionale come da reazione desmoplastica . 
chirurgia : cdis con focolai di infiltrazione stromale . ductal changes ( focal dilatation with intraductal hypoechoic necrotic - like material , associated with microcalcifications ) in four cases ( 15% ) at us , most lesions ranged in size from 10 to 20 mm ( 13 / 27 , 48% ) , 11 were > 20 mm ( 41% ) and three < 10 mm ( 11% ) ( table 4 )  . 
all lesions were classified as suspicious ( birads 4 in 20 / 27 cases , 74% ) or as highly suspicious ( bi - rads 5 in 7 / 27 cases , 26% ) for malignancy ( table 5 )  . considering only dcis with invasive component demonstrated at surgical excision ( thus excluding microinvasive dcis , as they have a similar locoregional recurrence rate , disease - free survival and overall survival rate to pure dcis ) , the underestimation rate is reduced to 31% ( 20 / 65 lesions )  . discussion mammography is the most important and sensitive technique for the detection of dcis associated with microcalcifications . 
moreover , it shows the number and extent of microcalcification clusters and can be used as a guide for biopsy . until now , us had only a marginal role in the diagnosis of v . 
over the last few years , the introduction of new broadband highfrequency linear - array transducers with higher spatial and contrast resolution ( so called highresolution sonography ) has improved the techniques sensitivity and specificity and the operators diagnostic confidence [ 2426 ]  . 
in our series , 21.5% ( 14 / 65 ) of dcis was mammographically occult , in line with the percentage of 623% reported in the literature [ 4 , 5 , 7 , 9 , 27 ]  . 
us , performed by expert physicians with high - resolution linear - array broadband transducers with 10to 13 - mhz frequency , may be considered complementary to mammography for the detection of dcis , especially for those not associated with microcalcifications , and for the evaluation of the ductal extent of dcis in dense breasts [ 11 ]  . 
us - guided cnb offers many advantages over surgical biopsy , as it is fast , less costly and less invasive ( no surgical scars responsible for mammographic and sonographic distortion )  . 
moreover , it is more comfortable than stereotactic biopsy ( no breast compression is required ) and , thanks to the real - time visualisation of the needle probe , allows tissue retrieval from all breast regions , including peripheral regions such as the axillary tail and chest wall in the case of a previous mastectomy . 
if correctly performed ( using 14 - gauge needles , long throw and at least five tissue samples ) , its results are as satisfying as those of excisional biopsy , which is still considered the gold standard procedure . in literature , the concordance between cnb ( performed both under sonographic and mammographic guidance ) and surgical excision ranges from 80% to 96% . 
our study revealed an underestimation rate of 41.5% , with surgical excision demonstrating microinfiltration ( invasive foci 1 mm ) or infiltration in 27 lesions ( seven dcis were microinvasive and 20 dcis showed invasive components at definitive histology )  . most investigations of the accuracy of cnb in the diagnosis of dcis focus on stereotactically rather than sonographically guided procedures . 
despite the high concordance between stereotactic core needle biopsy ( scnb ) and surgical excision , many authors have reported variable ranges ( 15%36% ) of pure dcis diagnosed on scnb later upgraded to invasive carcinomas after lumpectomy [ 2834 ]  . in a paper comparing the outcome of us - guided cnb and vacuum - assisted biopsies ( vab ) for the diagnosis of dcis , philpotts et al . 
 [ 19 ] found no significant differences in the outcomes of us - guided core biopsies performed with the 14gauge automated gun compared with those performed with the 11 - gauge vacuum - assisted device . 
in particular , no differences were reported regarding the number of false - negative cancers , underestimation , complications or recommendations aspetti di infiltrazione stromale alla scnb , risultati poi delle lesioni infiltranti alla successiva nodulectomia [ 2834 ]  . 
 [ 19 ] effettuano un confronto anche con i risultati della vacuumassisted biopsy ( vab ) , senza riportare significative differenze di accuratezza tra le diagnosi ottenute con il sistema automatico ( ago 14 g ) e quelle ottenute con il sistema vab ( ago 11 g )  . 
in particolare , gli autori riportano risultati della cb comparabili con quelli della vab per quanto concerne il numero di carcinomi falsi - negativi e di sottostime istologiche , a parit di complicanze . 
essi ritengono inoltre che non vi siano differenze sostanziali nel rinvio a re - biopsia ( o biopsia chirurgica ) fra cb e vab , in relazione alle problematiche concernenti la discordanza tra quadro radiologico e istologico , in caso di diagnosi di lesione proliferativa ad alto rischio ( radial - scar , iperplasia duttale atipica , clis , papilloma ) o in caso di biopsia inadeguata ( evento questultimo abbastanza raro per entrambe le metodiche )  . inoltre , il numero di frustoli considerato sufficiente per la diagnosi di un nodulo ecografico solitamente inferiore con lutilizzo della biopsia ecoguidata ( 4 - 5 frustoli ) , dal momento che il prelievo avviene in tempo reale con la visualizzazione dellago , rispetto alla biopsia sotto guida stereotassica che necessita di pi di 10 frustoli ( soprattutto in presenza di microcalcificazioni ) [ 19 ]  . 
il sistema di biopsia vab a guida ecografica , caratterizzato dallinserimento manuale dellago allinterno della lesione senza il sistema di avanzamento automatico , potrebbe invece essere utilizzato nei casi di noduli ecografici profondi o nelle lesioni di difficile visualizzazione , al fine di ridurre il rischio di perforazione della gabbia toracica [ 19 ]  . per quanto concerne la biopsia sotto guida stereotassica ( scnb ) , lee et al . 
 [ 35 ] , nella loro casistica di 59 cdis diagnosticati alla scnb , hanno presentato un tasso di sottostima pari al 18% ( 6 / 34 ) tra i cdis biopsiati con sistema vab con ago da 11 g e pari al 44% ( 11 / 25 ) tra i cdis biopsiati con sistema di prelievo automatico con ago da 14 g . 
 [ 36 ] , nella loro casistica di 40 lesioni consecutive diagnosticate come cdis utilizzando la guida stereotassica , hanno ottenuto valori di sottostima sostanzialmente pi bassi con il vacuum - assisted device da 11 g ( 15% , 3 / 20 ) rispetto al sistema automatico da 14 g ( 35% , 7 / 20 )  . 
la maggiore accuratezza nella diagnosi istologica percutanea dimostrata dai sistemi vab con ago da 11 g si pu spiegare con il ricorso ad aghi di maggior calibro , che consentono il prelievo di una maggiore quantit di tessuto , e con il maggior numero di prelievi bioptici ottenuti . 
in letteratura , molti autori per ritengono che i sistemi di vacuum - assisted biopsy ( vab ) possano ridurre , ma non eliminare completamente , il numero delle sottostime istologiche percutanee nelle diagnosi di cdis [ 2834 ]  . i motivi delle sottostime istologiche percutanee riscontrate anche con i sistemi vab da 11 g sarebbero legati al fatto che le calcificazioni , ossia il target di prelievo delle procedure stereotassiche , non corrispondono effettivamente alle aree di tumore invasivo che , cos , potrebbero non essere adeguatamente incluse allinterno dei frustoli calcifici prelevati . 
in fact , a second biopsy , or better surgical biopsy , is warranted in all cases of radiologicalpathological discordance , core biopsy diagnosis of high - risk proliferative lesions ( radial scar , atypical ductal hyperplasia , lcis , papillary lesion ) or inadequate sampling ( occurring quite infrequently with both modalities )  . the minimum number of specimens needed for a histological diagnosis is usually lower for us - guided biopsy ( 45 specimens ) than for stereotactic biopsy ( more than 10 specimens ) , particularly in the presence of microcalcifications [ 19 ]  . 
us - guided vab , with the transducer manually introduced into the lesion without shooting through automated systems , might be used in cases of deep nodules or low visibility in order to reduce the risk of chest wall perforation [ 19 ]  . with regard to scnb , a study by lee et al . 
 [ 35 ] on 59 dcis diagnosed by scnb reported an 18% ( 6 / 34 ) underestimation rate for vab with 11 - gauge needles and a 44% ( 11 / 25 ) underestimation rate for an automated system with 14 - gauge needles [ 35 ]  . 
similar results were reported by won et al . , with underestimation rates for stereotactic vab of 15% and of 35% with 11 - gauge and 14 - gauge needles , respectively [ 36 ]  . 
in the literature , vab is regarded as a useful diagnostic tool , able to reduce but not completely avoid underestimation in the diagnosis of dcis [ 2834 ]  . 
 however , the reasons for the underestimations produced even by the 11 - gauge vab systems are related to microcalcifications , which the biopsy aims to target , not being contained within the invasive tumoral component . 
the most frequent appearances were : mass without microcalcifications mass with microcalcifications isolated microcalcifications it is also important to consider : ductal changes dimensions mass without microcalcifications this was the most frequent appearance of dcis and was mainly a solid nodule with microlobulated boundaries and guardanti laccuratezza della diagnosi istologica percutanea su focolai di microcalcificazioni , quando vengano utilizzati dispositivi di prelievo automatico , in relazione alla esiguit del materiale bioptico fornito dagli aghi 14 g ( materiale che talvolta risulta anche frammentato ) e pertanto non sempre rappresentativo dellintera lesione che si desidera sottoporre a biopsia . 
gli aspetti principali da considerare sono rappresentati dal riscontro di : massa senza microcalcificazioni massa con microcalcificazioni microcalcificazioni isolate . va inoltre considerato leventuale pattern di presentazioaspetti duttali dimensioni . massa senza microcalcificazioni si tratta dellaspetto ecografico di cdis riscontrato nella nostra casistica pi frequentemente , caratterizzato da una massa solida , microlobulata , non calcifica ( riconosciuta nel 47 , 4% dei cdis puri e nel 63% dei cdis invasivi )  . 
tale aspetto quello comunemente riscontrato nei cdis non associati a microcalcificazioni , che istologicamente corrispondono al pattern cribriforme , micropapillare , papillare o solido , e che si accrescono senza formare n necrosi n calcificazioni , senza reazione desmoplastica ( corrispondente a fenomeni di fibrosi , sclerosi o fenomeni cicatriziali ) ; questultima caratterizza invece lassorbimento acustico posteriore tipico dei carcinomi invasivi aggressivi . 
molti autori hanno sottolineato la possibilit di dimostrare le microcalcificazioni grazie allecografia ad alta risoluzione , dove appaiono come piccoli spot iperecogeni , in genere non associati allassorbimento acustico posteriore in relazione alle loro ridotte dimensioni [ 13 , 24 , 26 ]  . 
alcuni autori hanno sottolineato inoltre che le calcificazioni associate a lesioni maligne sono pi facilmente visibili allus poich si sviluppano allinterno di un nodulo solido , mentre la maggior parte delle calcificazioni benigne si forma nel parenchima mammario fibro - ghianv . 
dcis not associated with microcalcifications correspond histologically to cribriform , micropapillary , papillary or solid patterns that grow without forming necrosis , calcifications or desmoplastic reaction ( fibrosis , sclerosis , scarring ) ; a desmoplastic reaction may explain the presence of posterior acoustic shadowing in aggressive invasive cancers . 
 mass with microcalcifications microcalcifications , set within solid masses , represent the second most frequent us pattern ( found in 23.7% of pure dcis and in 22% of dcis with invasive component )  . 
many authors have recently emphasised the possibility of identifying microcalcifications through high - resolution sonography , where they appear as small , hyperechoic spots without posterior acoustic shadowing due to their small size [ 13 , 24 , 26 ]  . 
calcifications associated with malignant lesions are easily detected on us , as they develop within a solid nodule , whereas most benign calcifications develop in hyperechoic fibroglandular breast parenchyma and are more difficult to identify [ 11 ]  . isolated microcalcifications isolated microcalcifications within normal breast parenchyma were found in only four cases ( 10.5% ) of pure dcis but in no case of invasive dcis . 
usually , it is very difficult to depict small clusters of microcalcifications at us , especially if they are < 5 mm in size , as these small hyperechoic spots are not associated with posterior acoustic shadowing and can be confused with hyperechoic us tissue interfaces or with speckle artefacts [ 24 , 26 ]  . 
the microcalcifications more easily depicted by us are large ( > 10 mm ) clusters of packed , highly suspicious ( bi - rads 5 ) calcifications with segmental distribution [ 13 ]  . 
 [ 38 ] , who defined the extension of tumoral cells towards the nipple as ductal diffusion and the extension of tumoral cells in the opposite direction as a branching pattern . 
they interpreted this branching pattern as the expression of the diffusion of a proliferative process through the ductal system and correlated it to a high probability of malignancy [ 38 ]  . 
in fact , intraductal vascularisation dolare iperecogeno e pertanto pi difficile da identificare [ 11 ]  . microcalcificazioni isolate la presenza di microcalcificazioni isolate nel contesto del parenchima mammario normale stata evidenziata solo in 4 casi ( 10 , 5% ) di cdis puri , ma in nessun caso di cdis invasivo . 
di solito molto difficile individuare piccoli focolai di microcalcificazioni allus , soprattutto quelli con dimensioni < 5 mm , dal momento che questi piccoli spot iperecogeni non associati ad assorbimento acustico posteriore possono essere confusi con le interfacce acustiche iperecogene del tessuto o con i cosiddetti speckle artifacts [ 24 , 26 ]  . 
le microcalcificazioni che hanno maggior probabilit di essere viste allus sono rappresentate da focolai di microcalcificazioni con dimensioni > 10 mm , con numerosi spot calcifici allinterno del focolaio , caratterizzati da una distribuzione segmentale e da un elevato sospetto di malignit ( bi - rads 5 ) [ 13 ]  . 
 [ 38 ] hanno descritto gi questi tipici aspetti duttali , definendo come diffusione duttale lestensione delle cellule tumorali verso la regione del capezzolo , e come pattern ramificato lestensione delle cellule tumorali in direzione opposta rispetto al capezzolo . 
gli autori hanno interpretato questo pattern ramificato come lespressione della diffusione del processo proliferativo lungo il sistema duttale , correlandolo ad una maggior probabilit di malignit [ 38 ]  . va sottolineato inoltre lapporto del color - doppler nel definire la natura del contenuto dei dotti dilatati . 
nevertheless , this underestimation rate appears to be irrelevant in relation to the total number of breast neoplasms diagnosed on cnb ( 27 / 968 , 2.8% ) and seems not to affect patient outcome , although this statement should be further confirmed . 
we found no sonographic pattern specific for invasive component , although features such as a solid component , either inside dilatated ducts or together with microcalcifications , and a size > 20 mm are more frequently associated with infiltration . criterio dimensionale per quanto riguarda invece il criterio dimensionale , la maggior parte delle lesioni riscontrate presentava dimensioni comprese tra 10 e 20 mm ( 58% dei cdis puri , 48% dei cdis sottostimati ) ; tuttavia va sottolineato che il 40% dei cdis puri presentava dimensioni inferiori ai 10 mm , mentre il 41% dei cdis invasivi presentava dimensioni pi grossolane , superiori ai 20 mpertanto possiamo affermare che il riscontro ecografico di lesioni con dimensioni > 20 mm pu far sospettare pi frequentemente la presenza di una componente invasiva . conclusioni la diagnosi di cdis alla cb sotto guida ecografia gravata da un numero elevato di sottostime istologiche ( 41 , 5% )  . 
daltro canto , questa percentuale di sottostima sembra essere irrilevante sul totale dei cancri diagnosticati alla cb ( 27 / 968 , 2 , 8% ) e inoltre il tasso di sottostima istologica sembra non influenzare loutcome delle pazienti , nonostante tale affermazione necessiti di ulteriori studi per essere confermata . 
non esistono pattern ecografici specifici per la diagnosi della componente infiltrante , anche se la presenza della componente solida visibile ecograficamente , sia allinterno di immagini duttali che nei casi associati a calcificazioni , e le dimensioni superiori a 20 mm delle lesioni , si associno pi frequentemente a infiltrazione . 
carriero scdu radiologia , sezione di risonanza magnetica , ao maggiore della carit , universit del piemonte orientale , c.so mazzini 18 , i - 28100 novara , italy correspondence to : a . 
contrast - enhanced mra , even with a low - field ( 0.5 - t ) unit , is a feasible , sensitive and accurate technique for the study of the renal arteries of the transplanted kidney . key word renal transplant renal artery stenosis angio - mri riassunto obiettivo . 
langio - rm con contrasto iniettato con tecnica a bolo di contrasto , per lo studio delle arterie renali dei reni trapiantati , una metodica fattibile dal punto di vista pratico , sensibile e con unottima accuratezza diagnostica , anche con apparecchiatura rm a basso campo ( 0 , 5 t )  . parole chiave trapianto renale stenosi dellarteria renale angio - rm introduction introduzione in 2005 alone 213 kidney transplants from cadaver donors were performed in the italian region of piedmont , 80 of solo nel 2005 in piemonte sono stati effettuati 213 trapianti di reni da donatore cadavere , e nella nostra struttura ospe1026 09 stecco 19 - 10 - 2007 13 : 41 pagina 1027 a . 
in either case , well - defined images are required to evaluate the presence , site , degree and extent of stenosis , information that facilitates the choice between endovascular or surgical treatment and allows more invasive radiological techniques to be avoided . colour - doppler ultrasound ( us ) is the easiest and fastest imaging tool for diagnosing possible vascular complications of the kidney graft [ 9 , 10 ]  . 
the current gold standard is digital subtraction angiography ( dsa ) [ 11 , 12 ] , which has proved to provide the best characterization of arterial stenosis and atheromas , especially since the introduction of the three - dimensional rotational technique . 
other reasons include potential nephrotoxicity of the contrast material , need for percutaneous access , the use of ionising radiation and possible complications that may occur during the procedure that carry a low but definite risk of mortality ( 0.02% ) [ 13 , 14 ]  . some authors [ 1517 ] have evaluated the role of magnetic resonance angiography ( mra ) in the detection and characterisation of arterial stenosis , describing it as a noninvasive method that relies on intravenous injection of gadolinium and does not require ionising radiation or percutaneous access . 
the aim of our study was to assess interobserver variability , sensitivity , specificity and diagnostic accuracy of contrast - enhanced low - field mri in the evaluation of arterial stenosis of the transplanted kidney by analysing both source images and digitally reconstructed images . materials and methods patients we studied 49 patients ( 31 men , 18 women ; age 2473 years ; all cadaver - donor kidney recipients ) who underwent a total of 64 mra examinations for clinical suspicion of renal artery stenosis based on : the presence of non - rejection - related renal failure , alterations identified on colour - doppler us and hypertension of unknown origsome of these patients were undergoing a series of follow - up studies owing to difficult clinical situations . 
in entrambi i casi si necessita di immagini ben definite per valutare la presenza , il sito , il grado e lestensione della stenosi e questo rende pi facile anche la scelta del trattamento endovascolare o chirurgico , e ancora permette di evitare indagini radiologiche pi invasive . leco - color doppler lo strumento pi facile e veloce da utilizzare per diagnosticare eventuali complicazioni vascolari nei reni trapiantati [ 9 , 10 ] , ma allo stesso tempo una metodica operatore dipendente , caratterizzata da una variabilit durante lesecuzione e quindi dallimpossibilit , in alcuni casi , di evidenziare totalmente o parzialmente larteria renale . 
attualmente il gold standard radiologico langiografia a sottrazione digitale ( dsa ) [ 11 , 12 ] , che sin dallintroduzione dellangiografia volumetrica rotazionale , si dimostrata capace di caratterizzare al meglio le stenosi arteriose e le placche ateromatose . 
questa tecnica angiografica necessita per di iniezione intra - arteriosa di mezzo di contrasto iodato , e per questo e non solo considerata invasiva ; inoltre bene ricordare la potenziale nefrotossicit del mdc , la necessit di un accesso percutaneo , lutilizzo di raggi x , e le possibili complicanze durante la procedura che presentano un seppur basso ( 0 , 02% ) rischio di mortalit [ 13 , 14 ]  . alcuni autori [ 1517 ] hanno valutato il ruolo dellangiografia con risonanza magnetica ( arm ) nella visualizzazione e caratterizzazione delle stenosi arteriose considerandola una metodica non invasiva per lutilizzo intravenoso di gadolinio , lassenza di raggi x e di accesso percutaneo ; tutti hanno per utilizzato un tomografo rm a medio - alto campo magnetico ( 1 - 1 , 5 tesla ) , senza menzionare le possibilit di utilizzo di un tomografo rm a basso campo ( 0 , 5 t )  . 
per questo il nostro studio mira a valutare la variabilit tra gli esaminatori , la sensibilit , la specificit e laccuratezza diagnostica della tomografia rm a basso campo con mdc , nella valutazione delle stenosi arteriose del rene trapiantato , con losservazione sia delle immagini originali , sia delle ricostruzioni digitali . materiali e metodi pazienti sono stati esaminati 49 pazienti ( 31 maschi e 18 femmine , di et compresa tra i 24 e i 73 anni , tutti sottoposti a trapianto renale da donazione da cadavere ) , sottoposti ad un totale di 64 arm per sospetto clinico di stenosi dellarteria renale , dovuto a : presenza di insufficienza renale non da rigetto ; alterazioni evidenziate mediante eco - color doppler ; ipertensione di origine sconosciuta . 
a bolus of 1 ml of gadolinium - benzyloxypropionictetraacetate ( gdbopta ) ( multihance , bracco , italy ) was infused via an automatic injector ( spectris , medrad , pittsburgh , pa , usa ) at a rate of 2.0 ml / s , followed by 20 ml of saline solution . 
during the bolus test , a single sagittal section was acquired with the multiphase technique using a fast - gradient t1 sequence with high temporal resolution ( tr / te min / 2.6 ; flip angle 60 ; ta 30s ; slice 10 - mm ; fov 40 cm ; matrix 224128 ; nex 1 ) , positioned along the course of the aorta , after a preliminary localization sequence in the coronal plane . 
then we proceeded with a scan using fast gradient echo sequences ( fgre - 3d ; tr / te / inversion time min / 1.9 / 41 ; flip angle 50 ; ta 27s ; thickness 5 mm ; fov 42 cm ; matrix 320160 , nex 1 ) with fat suppression . 
this pulse sequence is characterised by optimal signal - to - noise ratio ( snr ) and rotation time ( tr ) , with centric k - space encoding that improves contrast between vascular structures and especially snr . 
fat suppression ( inversion time = 41 ms ) does not require additional digital subtraction of contrast images from the mask image but nevertheless provides suppression and deletion of nonvascular structures . post - processing with 3d algorithms was performed on a workstation ( advantage windows 4.0 , ge , milwaukee , il , usa ) by a third operator to create maximum intensity projection ( mip ) and multiplanar reconstructions ( mpr )  . 
mip images were obtained with 20 rotations at 18 on the longitudinal axis to cover 360 of the volume acquired ; mpr images were generated to visualise simultaneously three windows displaying sagittal , coronal and axial views . 
 to evaluate possible stenoses of the iliac arteries , patients also underwent dsa with a digital subtraction philips integris v5000 unit ( philips , eindhoven , the netherlands ) , during which multiple boluses ( 20 ml ) of noniodinated contrast medium ( iomeron 300 , bracco ) were injected into the abdominal aorta at a rate of 10 ml / s . 
patients with suspected stenosis of the anastomosis or external iliac artery were administered a bolus of 810 ml of contrast material in the iliac artery at a rate of 3 ml / s . 
images were acquired in the anteroposterior and oblique positions ( 30 )  . image analysis two radiologists ( po and as ) evaluated the three mra images sets ( mip , mpr and raw data ) , which had been processed by a fourth - year radiology resident blinded to patients clinical conditions and dsa results . 
images were evaluated using a preprinted form on which readers had to indicate whether stenosis was present and the arterial branch involved , divided into three segments ( preanastomotic , anastomotic and postanastomotic )  . 
where a stenosis was identi1028 ( 22 , 4% ) sono stati inoltre sottoposti a dsa , anche pi volte per il lungo follow - up o per delle ristenosi dopo angioplastica : tutti i pazienti hanno firmato il consenso informato prima dellesame . tecnica dellimmagine le scansioni rm sono state acquisite grazie ad una bobina phased - array ( body - flex ii ) e ad uno scanner a 0 , 5 t ( signa contour , ge , milwaukee , il , usa ) , con gradienti aggiornati . 
stato eseguito un test ( bolus track ) di infusione per il calcolo del tempo di circolo , con 1 ml di gadolinium - benzyloxypropionictetraacetato ( gd - bopta ) ( multihance , bracco , italia ) , con velocit di infusione di 2 , 0 ml / s , seguito dallinfusione di 20 ml di soluzione salina ; tutto tramite iniettore automatico ( spectris , medrad , pittsburg , pa , usa )  . durante liniezione del bolus test stata acquisita con tecnica multifasica una singola sezione nel piano sagittale con sequenza fast - gradient t1 ad elevata risoluzione temporale ( tr / te min / 2 , 6 ; flip angle 60 ; ta 30 s ; slice 10 mm ; fov 40 cm ; matrice 224128 ; nex 1 ) , posizionata lungo il decorso dellaorta , dopo una preliminare sequenza di localizzazione sul piano coronale . 
dopo aver calcolato il tempo di circolo e pianificato le sequenze angio - rm con mdc , sono state iniettati 30 ml di gd - bopta , seguiti da 20 ml di soluzione salina alla velocit di 2 , 0 ml / s . 
questa sequenza ad impulsi caratterizzata da valori di snr e tr ottimizzati , con una fase di codifica centrica del - spazio , al fine di ottimizzare il contrasto tra le strutture vascolari e soprattutto il rapporto segnale - rumore . 
la tecnica di soppressione del grasso ( tempo di inversione = 41 ms ) non richiede altre sottrazioni digitali delle immagini con contrasto dalla maschera , ottenendo comunque la soppressione e la cancellazione delle strutture non vascolari . la rielaborazione con algoritmi 3d stata effettuata da un terzo operatore con una workstation ( advantage windows 4.0 , ge , milwaukee , il , usa ) , al fine di creare delle ricostruzioni mip e multiplanari ( mpr )  . 
le immagini mip sono state ottenute con venti rotazioni di 18 attorno allasse longitudinale in modo da coprire i 360 del volume acquisito ; le ricostruzioni mpr sono state effettuate in modo da ottenere nella stessa schermata contemporaneamente tre finestre con visione sagittale , coronale ed assiale . al fine di confermare eventuali stenosi delle arterie iliache , i pazienti sono stati inoltre sottoposti a dsa con angiografo digitale tipo integris v5000 ( philips , eindhoven , olanda ) , durante la quale stato iniettato un bolo ( 20 ml ) di mdc non iodato ( iomeron 300 bracco ) attraverso un catatere posizionato in aorta addominale sottorenale e con una velocit di infusione di 10 ml / s . 
ai pazienti con sospetta stenosi a livello dellanastomosi o della arteria iliaca esterna , durante la asd sono stati somministrati 810 ml di mdc in bolo nellarteria iliaca esterna ad una velocit di 3 ml / s . 
dsa results were regarded as the gold standard against which mra results were compared . statistical analysis statistical analyses were performed with excel ( microsoft , redmond , wa , usa )  . 
le valutazioni delle immagini sono state eseguite utilizzando un modulo cartaceo a risposte obbligate , ovvero determinando la presenza o meno della stenosi e considerando il ramo arterioso diviso in tre sezioni : pre - anastomotica , anastomotica e post - anastomotica . 
quando stata identificata una stenosi stata eseguita una misurazione della stessa ( a ) ed stato calcolato il rapporto tra il restringimento e il diametro dellarteria ( b ) nel tratto a valle pi vicino non coinvolto dalla stenosi : 100x ( 1a / b ) [ 18 , 19 ]  . 
i pazienti sono stati classificati come portatori di stenosi lieve ( 0%39% ) , moderata ( 40%69% ) o severa ( > 70% ) [ 20 ] , ma solo il riscontro di una stenosi grave stato considerato emodinamicamente significativo e quindi in tal caso lesame stato considerato positivo . 
le immagini dsa sono state valutate invece da un esperto radiologo interventista ( r.f. ) sempre mantenendo la soglia del 70% , per considerare lesame angiografico positivo . abbiamo considerato i risultati dellangiografia come gold standard e confrontato gli stessi con i risultati della angio - rm . analisi statistiche of the 49 patients enrolled , 36 underwent a single mra examination , 11 underwent two examinations and two underwent three , for a total of 64 mra examinations . 
la dsa conferma la presenza di entrambe le stenosi , quella craniale > 70% , laltra emodinamicamente non significativa . 1029 09 stecco 19 - 10 - 2007 13 : 41 pagina 1030 a . 
lanalisi finale si basata su 70 scansioni per 210 tratti vascolari e per un totale di 630 immagini ( mip , mpr , dati sorgente )  . undici pazienti ( 4 dei quali hanno ripetuto due volte lesame ) , sono stati sottoposti a 15 angiografie digitali , al fine di confermare e possibilmente trattare la stenosi . 
un esame arm stato scartato per insufficiente acquisizione dei dati che non hanno permesso la ricostruzione completa del peduncolo vascolare ; mentre un altro paziente , sottoposto a due angiografie , stato scartato dallo studio per motivi statistici in quanto la stenosi era dovuta a fistola post - bioptica . per due pazienti abbiamo considerato quattro esami ( per la presenza di due diverse stenosi e per la presenza di due arterie renali ) ; quindi un totale di 14 angiogrammi digitali renali hanno mostrato 42 sezioni vascolari ( sempre divise in pre - anastomotiche , anastomotiche , post - anastomotiche )  . 
la sensibilit , la specificit e laccuratezza diagnostica delle immagini mip , mpr e partizionali , nella determinazione della presenza e dellentit della stenosi , sono riportare nella tabella 3 : laccordo tra i due radiologi risultato elevato ( = 0 , 7976 )  . 
the latter patient was subsequently followed up by colour - doppler us and computed tomography ( ct ) , which showed that the anastomosis had not suffered damage from exposure to the magnetic field . 
the final analysis was based on 70 scans for 210 vascular segments for a total of 630 images ( mip , mpr , raw data )  . eleven patients ( four with two mra scans ) underwent 15 dsa examinations to confirm and possibly treat the stenosis . one angiogram was discarded due to inadequate data acquisition preventing complete reconstruction of the vascular pedicle ; another patient , who underwent two angiographic studies , was excluded for statistical reasons , as the stenosis was due to a postbiopsy fistula . 
sensitivity , specificity and diagnostic accuracy of the mip , mpr and raw data image sets for evaluation of the presence and severity of stenosis are shown in table 3 . 
the role of mra in the evaluation of vascular complications of the kidney graft is pazienti con complicanze post - trapianto rena , fondamentale in un momento diagnostico dove lo strumento di diagnosi deve arrecare minor danno possibile ad un parenchima renale gi sofferente ; pertanto langiografia dovrebbe essere limitata ai casi con elevato sospetto clinico e radiologico . tra le varie complicanze , vascolari e non , precoci e tardive , che possano interessare un rene trapiantato , la stenosi dellarteria renale la pi frequente [ 25 ]  . 
il ruolo dellarm nella valutazione delle complicanze vascolari del rene trapiantato noto , come anche lutilit dellabbinare una valutazione arm con tecnica a contrasto di fase , a quella a bolo di contrasto [ 22 ]  . 
tutti gli studi precedenti hanno preso in esame casistiche studiate con magneti da 1 t o 1 , 5 t ; non invece chiaro allo stato se sia utile e che impatto abbiano le immagini ottenute con magneti a basso campo ( 0 , 5 t )  . 
all previous studies have been conducted on patients imaged with 1 - t or 1.5 - t equipment , so the usefulness and impact of images obtained with low - field ( 0.5 - t ) magnets has not been clarified . 
clearly with this type of magnet , the possibility of conducting studies with phase - contrast sequences is limited by the length of the scan , which increases the time during which the patient must lie still , with motion artefacts consequently reducing overall examination quality . 
phase - contrast mra and bolus - contrast mra can both be performed on low - field mri scanners with fast - gradient sequences . bolus - contrast mra , even with a 0.5 - t unit , may be diagnostic in the evaluation of renal arteries . 
sia larm con tecnica pc che larm con tecnica a bolo di contrasto sono entrambe eseguibili con un tomografo rm a basso campo con sequenze di tipo fast - gradient . larm a bolo di contrasto pu essere diagnostica nella valutazione delle arterie renali , anche usando un magnete a 0 , 5 t . 
solo il 2 , 7% degli esami arm non sono risultati diagnostici nel nostro studio ; al contrario nel 97 , 3% dei casi siamo riusciti ad ottenere una valutazione diagnostica sullo stato delle arterie del rene trapiantato . 
in our experience , although bolus - contrast mra was not particularly specific in detecting the stenosis , it proved to have higher specificity in quantifying the lesion . as reported in the literature , raw data image sets play a fundamental role given that they are both sensitive and specific and are routinely evaluated to complete the analysis of mip images in cases of arterial dissection , nonocclusive thrombus , in the presence of metal clips and venous contamination [ 2326 ] biamo rilevato delle differenze tra le ricostruzioni mip , mpr e le immagini partizionali ( sorgente , grezze ) , in termini di identificazione della stenosi ; le immagini partizionali si sono rivelate pi sensibili ( 75% vs 62 , 5% ) , egualmente specifiche e con una maggior accuratezza diagnostica ( 75% vs 71 , 43% ) nello stabilire il grado di severit della stenosi . 
secondo la nostra esperienza , larm a bolo di contrasto non si dimostrato un esame molto specifico nellidentificare le stenosi , al contrario invece presentando una maggiore specificit nella sua quantificazione . come gi riscontrato in letteratura le immagini partizionali hanno un ruolo fondamentale , essendo sia sensibili che specifiche , e vengono routinariamente analizzate perch completano lanalisi delle mip nei casi di dissezione arteriosa , di trombo non occlusivo , in presenza di clips metalliche e in overlap venoso [ 2326 ] in conclusione , i nostri risultati dimostrano che larm 1033 09 stecco 19 - 10 - 2007 13 : 41 pagina 1034 a . 
historically , cacs was introduced with electron beam computed tomography ( ebct ) , but in the last 30 years , many changes have occurred in ct , where the development of multidetector spiral technology has made reliable the noninvasive study of the heart and coronary arteries . 
correlation studies with intravascular ultrasound ( ivus ) and histology have demonstrated the capability of multidetector ct ( mdct ) to provide information useful for characterising atherosclerotic plaque in a noninvasive manner . 
this has shifted the interest from heavily calcified deposits to plaque with a low - density core and small , superficial calcified nodules , features more frequently present in atherosclerotic plaque prone to rupture and responsible for acute coronary events ( culprit lesions )  . 
the purpose of this review article is to summarise the recent evolution and revolution in the field of ct , strengthen the importance of a coronary ct study not limited to cacs evaluation and cad grading but also used to obtain information about plaque composition , and to improve stratification of the patient at risk for acute coronary events . key words coronary artery calcium score coronary calcium screening multidetector computed tomography intravascular ultrasound riassunto la deposizione di calcio lungo le pareti delle arterie coronarie un indicatore biologico della malattia aterosclerotica e la sua quantit potrebbe riflettere la severit della malattia coronarica ( cad )  . 
in molti lavori della letteratura stato riconosciuto al coronary artery calcium score ( cacs ) un ruolo di strumento di screening della malattia coronarica ; storicamente esso stato introdotto con la electron beam - ct ( ebct ) , ma negli ultimi anni la tumultuosa evoluzione / rivoluzione tecnologica in ambito della tomografia computerizzata ( tc ) , con lo sviluppo di scanner spirali multidetettore , ha reso possibile lo studio non invasivo del cuore e delle coronarie anche con questa metodica . 
studi di correlazione con lecografia endovascolare ( ivus ) e listologia hanno recentemente documentato la possibilit di ottenere mediante tcmd ed in maniera non invasiva informazioni utili ai fini della caratterizzazione della placca aterosclerotica , spostando lattenzione dai marcati depositi di calcio alle placche coronariche con core a bassa densit e piccoli noduli calcifici superficiali , reperti pi frequentemente presenti nelle lesioni ateromasiche a rischio di rottura e responsabili , pertanto , di eventi coronarici acuti ( culprit lesion )  . 
lo scopo di questa review di riassumere levoluzione verificatasi recentemente nel campo della tomografia computerizzata , sottolineando limportanza di uno studio angiografico non invasivo delle coronarie con tcmd non limitato solamente alla semplice valutazione del cacs ed al grading delle lesioni , ma utile anche al fine di ottenere informazioni relative alla composizione della placca e migliorare , quindi , la stratificazione del paziente a rischio di evento coronarico acuto . parole chiave coronary artery calcium score screening del calcio coronarico tomografia computerizzata multidetettore ecografia intravascolare r . 
bonomo : coronary artery calcium score : has anything changed ? introduction introduzione in the last 30 years , diagnostic imaging , and in particular computed tomography ( ct ) , has been characterised by dramatic progress , regarded both as evolution and revolution . from its introduction in 1971 until 1989 , the hardware component of ct scanners evolved from the first generation of mechanical scanners , developed by g.n. 
furthermore , in the last 10 years , we have witnessed a rapid and tumultuous evolution of spiral ct scanners with the introduction and development of the multidetector spiral technology , from the first dual - slice ct scanner ( 1992 ) , through the four ( 1998 ) , eight - , 12 - , 16 ( 2003 ) , 40and currently 322 ( flying focal spot technology ) or 64 - detector - row ct scanner ( 64 - dct ) ( 20042005 )  . at the same time , this evolution has been accompanied by a revolution in the field of ct imaging , both in acquisition or reconstruction time and in image quality . 
cormack , alla tc spirale a singolo strato ( tcss ) , che ha rappresentato la vera pietra miliare sia per la tc in senso lato che per la tecnica di angio - tc . 
inoltre , nellultimo decennio siamo stati tutti testimoni della rapida e forse sin troppo tumultuosa evoluzione degli scanner tc spirale con lintroduzione e sviluppo della tecnologia multi - detettore , dai primi scanner a due strati ( 1992 ) , poi quelli a quattro ( 1998 ) , otto , dodici , sedici ( 2003 ) , quaranta , e recentemente ( 20042005 ) a 322 ( flying focal spot technology ) o 64 file di detettori ( 64tcmd )  . 
contemporaneamente , tale evoluzione stata accompagnata da una reale rivoluzione nel campo dellimaging tc , sia per quanto riguarda il tempo di acquisizione o ricostruzione delle immagini che per la qualit diagnostica di queste ultime . 
for these reasons , mandatory requisites for dedicated diagnostic hardware are high temporal and spatial resolution , an acquisition time well - matched with the apnoea compliance of the patient and dedicated and accurate ecg synchronisation . historically , cardiac ct imaging started with electron beam ct ( ebct ) [ 1117 ] , characterised by the highest temporal resolution ( 100 ms ) but with a limited spread , mostly in european countries , fundamentally due to the high cost and to a restricted application in examination of different anatomic regions ( thorax ; abdomen )  . 
one of the main results achieved by ebct in cardiac imaging has been noninvasive assessment of calcium deposits along the coronary artery walls , making noninvasive assessment of coronary atherosclerotic plaque burden reliable through measurement of a calcium score index , the agatston score ( as ) [ 18 ]  . 
given that calcium deposition is a surrogate biomarker of atherosclerotic disease , and given the strict correlation between the amount of calcium in the artery wall , disease severity , the likelihood of high - grade stenoses and the high negative predictive value ( npv ) of the score , supporters of cacs as a screening tool for coronary artery disease ( cad ) consider that cacs could be useful for evaluating subjects with more than one conventional risk factor for atherosclerotic disease [ 19 ] , for patients with atypical chest pain , for clinical decision making jointly to the conventional risk factors and treatment monitoring . 
furthermore , it has been demonstrated that a high cacs could increase the risk in patients classified as at intermediate - risk from the framingham risk score [ 20 ]  . 
some authors [ 21 ] suggest using the cacs to substitute the age factor among the conventional risk factors ; in fact , although the cacs increases with the age , age alone is not a real risk factor for coronary calcium but is a cumulative measure of exposure to conventional risk factors . prospective studies conducted on large cohorts of subjects [ 22 , 23 ] could probably explain in the coming years the real meaning and the possible utility of cacs . 
the significance of the cacs has been summarised by the expert consensus document on ebct for the diagnosis and prognosis of cad [ 36 , 37 ] , as briefly reported in table 1 . 
per tali motivi , requisiti imprescindibili di un hardware diagnostico dedicato allo studio delle coronarie sono essenzialmente una elevata risoluzione sia spaziale che temporale , una durata della scansione compatibile con la compliance respiratoria del paziente ed un dedicato e quanto pi preciso software di cardiosincronizzazione . storicamente , la cardio - tc nasce con la electron beamct ( ebct ) [ 1117 ] , caratterizzata dalla maggior risoluzione temporale ( 100 ms ) , ma con limitata diffusione territoriale , soprattutto in ambito europeo , essenzialmente per i suoi elevati costi e per la ristretta applicabilit nello studio di differenti regioni anatomiche ( torace , addome )  . 
uno dei principali risultati ottenuti con la ebct nellimaging cardiaco stata la visualizzazione dei depositi di calcio lungo le pareti delle arterie coronarie , rendendo cos possibile la valutazione non invasiva del carico aterosclerotico complessivo mediante la determinazione di uno score quantitativo del calcio presente , lo score di agatston ( as ) [ 18 ]  . 
il principale scopo del calcium score coronarico ( cacs ) la visualizzazione e quantificazione del calcio coronarico ai fini dellidentificazione dei soggetti asintomatici ad alto rischio di evento coronarico acuto . 
essendo il calcio un marcatore biologico della malattia aterosclerotica e data la stretta correlazione tra il quantitativo di calcio presente nella parete arteriosa , la severit della malattia e la probabilit di stenosi severe ed , infine , dato lelevato valore predittitivo negativo ( vpn ) dello score , i sostenitori del cacs come strumento di screening della malattia coronarica ( cad ) considerano che il cacs possa essere quindi utile nella valutazione dei soggetti con pi di un fattore di rischio ( fr ) convenzionale per malattia aterosclerotica [ 19 ] , nei pazienti con dolore toracico atipico o nellassumere particolari decisioni cliniche unitamente alla valutazione dei fr convenzionali o nel monitoraggio del trattamento ( statine )  . 
inoltre , stato dimostrato che un elevato valore di cacs possa effettivamente aumentare il rischio in quei pazienti classificati a rischio intermedio secondo lo score di framingham [ 20 ]  . 
qualcuno ipotizza [ 21 ] di impiegare il cacs come alternativa al fattore et tra i fr convenzionali della malattia aterosclerotica ; infatti , sebbene il cacs aumenti con let , la sola et non costituisce un reale fattore di rischio per laccumulo di calcio coronarico , rappresentando una misura cumulativa dellesposizione ai fr convenzionali . studi prospettici attualmente condotti su ampie coorti di soggetti [ 22 , 23 ] potranno probabilmente spiegare nei prossimi anni il reale significato e leventuale utilit clinica dello screening del calcio coronarico . 
in effect , these nonsignificant lesions are often the real culprit plaque and are responsible for the acute onset of coronary events because of the greater weakness of their components and structure . 
these details , together with the small but always present risks [ 43 , 44 ] and the high percentage ( up to 30% ) of ca examinations performed with simple diagnostic purposes and not followed by interventional procedures ( ptca / stenting ) , should prompt the search alternative , noninvasive diagnostic tools for assessing coronary arteries in well - selected patients . as the reliability of mdct in detecting and grading coronary artery stenoses has been established [ 110 ] , the challenge now is to define the ability of this diagnostic tool to distinguish coronary artery plaque prone to rupture or with findings suspected for instability and potentially responsible of acute coronary events [ 4446 ]  . 
studies using intravascular ultrasound ( ivus ) have illustrated the association between the pattern of distribution of coronary artery calcifications ( step and shot technique ) o quella spirale ( volumetric ) ; la seconda caratterizzata da una maggiore riproducibilit , essenzialmente dovuta alla minore incidenza di effetti di volume parziale , ma limitata dalla maggiore dose di esposizione del paziente [ 34 , 35 ]  . 
inoltre , in entrambe le modalit di esecuzione , la tcmd caratterizzata da maggiore riproducibilit sia inter - scan che inter - osservatore del ms versus vs e as [ 28 , 34 ] con differenze significative anche in pazienti con frequenza cardiaca 70 battiti per minuto ( bpm ) [ 29 ]  . 
modified from [ 42 ] major criteria inflammation thin fibrous cap large lipid corea superficial plaque erosion superficial platelet aggregation severe stenosis ( > 90% ) a minor criteria small superficial calcified nodulea haemorrhagic foci inside plaque endothelial dysfunction positive remodellinga shimmering yellow aassessable with multidetector computed tomography shimmer tabella 2 placca vulnerabile : criteri maggiori e minori . 
modificata da [ 42 ] criteri maggiori infiammazione sottile cappuccio fibroso criteri minori piccolo noduli calcifici superficialia foci emorragici nel contesto della placca disfunzione endoteliale rimodellamento positivoa ampio core lipidicoa erosione superficiale della placca aggregazione superficiale piastrinica riflesso giallastro stenosi severa ( > 90% ) a a valutabile con la tcmd and different clinical settings , such as acute myocardial infarction ( ami ) , unstable angina pectoris ( uap ) and stable angina pectoris ( sap ) [ 47 ]  . 
this mechanism is often responsible for the lack of symptoms , because the diameter enlargement initially prevents any significant lumen reduction and consequently preserves the distal blood flow [ 49 ] but with greater weakness of these plaques and a risk of rupture . 
otherwise , in sap the remodelling process is more frequently negative because of a fibrosing process , and it is often accompanied by significant lumen reduction , presence of symptoms and plaque stability . nowadays , state - of - the - art mdct scanners are able to acquire data with isotropic submillimetre spatial resolution [ 50 ]  . 
correlation studies with ivus and histology [ 5153 ] have demonstrated the capacity of mdct to noninvasively provide information useful for characterising atherosclerotic plaque , shifting the interest from heavy coronary calcium deposits for identification of patients at risk , to plaque with low - density core and small superficial calcified nodules , features more frequently present in atherosclerotic plaque prone to rupture and therefore responsible for acute coronary events . affette da stenosi non significative , in particolare con stenosi 70% . 
in effetti , tali lesioni non emodinamicamente significative sono nella maggioranza dei casi le reali culprit lesion ( lesioni colpevoli ) , responsabili dellinsorgenza acuta dellevento coronarico a causa della maggiore debolezza / friabilit delle loro componenti e struttura . 
le caratteristiche delle placche a rischio di rottura sono state precedentemente ed estesamente descritte [ 42 ] con la distinzione di criteri maggiori e minori ( tabella 2 )  . 
questi particolari in associazione ai rischi , rari ma pur sempre presenti [ 43 , 44 ] e alla significativa percentuale ( sino al 30% ) di esami coronarografici eseguiti per semplice finalit diagnostica e non seguiti pertanto da procedure interventistiche ( ptca / stenting ) dovrebbero obbligare , in pazienti adeguatamente selezionati , a cercare alternative diagnostiche non invasive per la valutazione del circolo coronarico . essendo stata gi definita la possibilit di visualizzare e definire lentit delle stenosi coronariche mediante tcmd [ 110 ] , la sfida pi ambiziosa si sposta attualmente alla definizione della capacit di tale metodica diagnostica di distinguere tra le placche coronariche quelle a rischio di rottura / complicanza o con reperti sospetti per instabilit e , quindi , potenzialmente responsabili di eventi coronarici acuti [ 4446 ]  . 
in studi condotti con ecografia endovascolare ( ivus ) , stata dimostrata lassociazione tra pattern di distribuzione delle calcificazioni coronariche e differenti quadri clinici , quali linfarto miocardico acuto ( ami ) , langina pectoris instabile ( uap ) e quella stabile ( sap ) [ 47 ]  . 
inoltre , il processo aterosclerotico negli eventi coronarici acuti frequentemente accompagnato da fenomeni di rimodellamento positivo del vaso [ 48 ] ; tale meccanismo spesso responsabile della mancanza di sintomatologia in quanto laumento del diametro vasale complessivo limita inizialmente leffetto della placca ateroslcerotica sullemodinamica locale , preservando cos distalmente il flusso ematico [ 49 ] , ma la debolezza delle componenti della placca stessa sono alla base del rischio di rottura e complicanza . 
4 intravascular ultrasound studies [ 47 ] have described the association between the distribution pattern of coronary artery calcifications and different clinical settings , such as acute myocardial infarction ( ami ) , unstable angina pectoris ( uap ) and stable angina pectoris ( sap )  . 
4 stato riportata [ 47 ] , da studi condotti mediante ecografia intravascolare ( ivus ) , lassociazione tra diversi pattern di distribuzione del calcio coronarico e differenti quadri clinici quali linfarto miocardico acuto ( ami ) , langina pectoris instabile ( uap ) e langina pectoris stabile ( sap )  . 
the multidetector computed tomography ( mdct ) curved multiplanar reconstruction ( mpr ) ( b ) of the cx shows lesion length , whereas axial reconstructions ( 13 ) of the vessel demonstrate the eccentric noncalcified plaque and severe lumen reduction ( arrowheads )  . 
la ricostruzione mpr curvata ( b ) della cx ben documenta la lunghezza della lesione , mentre le immagini ricostruite perpendicolarmente allasse del vaso ( 13 ) documentano la placca eccentrica non calcifica e la marcata riduzione del lume residuo ( teste di freccia )  . 
6a - e curved multiplanar reconstruction ( mpr ) image ( a ) of a concentric , noncalcified plaque in the proximal segment of the anterior descending artery ( ada ) ( arrowheads ) distally treated 1 year earlier with percutaneous transluminal coronary angioplasty ( ptca ) and stenting . 
the mpr image axial to the vessel ( b ) shows lumen reduction and the presence of a concentric , noncalcified tissue ( arrowheads ) around the residual vessel lumen . 
mpr reconstruction ( c ) of the circumflex coronary artery ( cx ) with a segmental mixed atherosclerotic lesion , as demonstrated by the axial image ( d ) with eccentric calcified nodule and small amount of noncalcified tissue ( arrowhead ) between calcium and residual lumen . 
limmagine ricostruita perpendicolarmente allasse del vaso ( b ) ben documenta la riduzione del lume e la presenza di tessuto concentrico ipodenso non calcifico ( teste di freccia ) attorno al lume residuo opacizzato . 
ricostruzione mpr - curvata della ada ( e ) con tre lesioni eccentriche non significative composte da noduli calcifici superficiali ( frecce )  . table 3 computed tomography ( ct ) density value of different components of atherosclerotic plaque feature ct density value ( hu ) recent thrombus lipid plaque fibrous plaque calcium plaque ~100 > 130 tabella 3 placca calcifica > 130 spostato linteresse , ai fini dellidentificazione del paziente a rischio , dai marcati depositi di calcio lungo le pareti delle coronarie alle placche con core ipodenso ( core lipidico ) e piccoli noduli calcifici superficiali , reperti maggiormente presenti nelle placche a rischio di rottura / complicanza e , quindi , responsabili dellinsorgenza di eventi coronarici acuti . 
 conclusione in conclusione , diversamente da quanto si pensasse in precedenza quando per la visualizzazione delle coronarie era a disposizione solamente la ebct ed essa era utilizzata essenzialmente per la valutazione del quantitativo di calcio , r . 
bonomo : coronary artery calcium score : has anything changed ? conclusion in conclusion , unlike in the past when the only available means to visualise coronary arteries was ebct which was used to assess and screen for coronary calcium , the use of mdct should probably induce us to change some of our opinions on the basis of new features . 
in fact , mdct with retrospective ecg gating has made the noninvasive study of coronary arteries reliable , with a real role in clinical practice mostly thanks to its high npv for the detection of significant cad . 
in the near future , it could probably play an important clinical role for a more accurate stratification of atherosclerotic risk , no longer simply based on visualisation and quantification of calcium deposits but prevalently based on direct , noninvasive visualisation of coronary plaque and characterisation of their components . limpiego dei nuovi scanner tcmd dovrebbe probabilmente indurci a modificare alcuni concetti sulla base dei nuovi reperti che siamo attualmente in grado di ricercare nel corso dello studio angio - tc del circolo coronarico . 
sardanelli universit degli studi di milano , dipartimento di scienze medico - chirurgiche , servizio di radiologia , irccs policlinico san donato , via morandi 30 , i - 20097 san donato milanese , milano , italy correspondence to : a . 
at the department of radiology of the policlinico san donato ( university of milan ) , breast mr is routinely performed at 1.5 t as follows : 36 - slice axial 2d shorttime inversion - recovery ( stir ) sequence ; 128 - partition 3d gradient - echo coronal sequence ( 1 - mm3 isotropic voxel ) before and after rapid automatic intravenous injection of 0.1 mmol / kg of gd - dota ( one precontrast and four postcontrast phases )  . postprocessing includes temporal subtraction ( postcontrast minus precontrast ) , maximum intensity projections ( mips ) , percent enhancement - to - time curves for small regions of interest , and axial and / or sagittal multiplanar reconstructions . 
we select only four mips of an early subtracted dynamic phase : one axial similar to craniocaudal x - ray mammographic views , one coronal , and two lateral similar to lateral 90 x - ray mammographic views . 
for each lesion described in the report , we select five items , including three images , one graph , and one table : stir image , precontrast and subtracted postcontrast images ( morphology ) , percent enhancement - to - time curves and a table of raw data generating the curves ( dynamics )  . 
the selected items range usually from four ( no detected lesion ) to 14 ( one lesion , studied also with 1h - mrs ) , to 34 ( five lesions , one of them studied also with 1h - mrs )  . 
presso il nostro dipartimento di radiologia le indagini di rm mammaria sono routinariamente effettuate a 1 , 5 t secondo il seguente protocollo : sequenza assiale 2d short - time inversion - recovery ( stir ) , 36 strati ; sequenza coronale 3d gradient - echo ( 128 partizioni ; voxel isotropico , 1 mm3 ) prima e dopo somministrazione automatica rapida di 0 , 1 mmol / kg di gd - dota ( una fase precontrasto e quattro postcontrasto )  . 
 il postprocessing include : sottrazione temporale ( postcontrasto meno precontrasto ) , ricostruzioni con algoritmo di massima intensit ( mip ) , curve di enhancement percentuale in funzione del tempo per piccole regioni di interesse e ricostruzioni multiplanari assiali e / o sagittali . 
tale protocollo genera oltre 1200 immagini per indagine . tra queste operiamo una ridotta selezione che include quattro mip di una fase dinamica precoce con sottrazione : una assiale simile alle proiezioni mammografiche cranio - caudali , due laterali simili alle proiezioni mammografiche laterali 90 e una coronale . per ciascuna lesione descritta nel referto selezioniamo cinque oggetti che includono tre immagini , un grafico e una tabella : immagine stir , immagini precontrasto e postcontrasto sottratte ( valutazione morfologica ) , curve di enhancement percentuale in funzione del tempo e tabella dei dati grezzi che generano le curve ( valutazione dinamica )  . 
se stata effettuata spettroscopia protonica , si aggiungono altri 5 oggetti : due spettri elaborati ( valutazione metabolica ) e le tre immagini di localizzazione del volume di interesse spettroscopico . 
il numero degli oggetti selezionati oscilla usualmente da quattro ( nessuna lesione evidenziata ) a 14 ( una lesione , studiata anche con spettroscopia protonica ) , a 34 ( cinque lesioni , una delle quali studiata anche con spettroscopia protonica )  . 
la rm mammaria pu essere sintetizzata presentando solo una minima frazione di tutte le immagini generate . parole chiave mammella risonanza magnetica ( rm ) spettroscopia a risonanza magnetica introduction introduzione magnetic resonance ( mr ) imaging of the breast has gained an important role in breast cancer diagnosis thanks to a very high sensitivity for at least five important indications : presurgical local staging and treatment planning , suspected recurrence in the operated breast , evaluation of the effect of neoadjuvant therapy , search for occult primary breast cancer with known metastases , and surveillance of women at high genetic - familial risk of breast cancer [ 1 ]  . 
however , some authors propose proton mr spectroscopy ( 1h - mrs ) to further increase the ability to characterise the lesion , with a gain in specificity [ 36 ]  . in breast mr , we daily face a general problem for crosssectional imaging . 
the development of hardware , software , and more and more sophisticated postprocessing techniques enable us to get native , postprocessed , and reconstructed images , including three - dimensional ( 3d ) representations . these are of great interest not only for radiologists but also for surgeons , radiation therapists , and oncologists , as it has been shown for fields other than mr or breast diseases [ 79 ]  . 
in our opinion , the key point is the ability of radiologists to manage a great deal of information ( i.e. , a huge number of images ) produced during a state - of - the - art examination , in order to provide other physicians selected information as an efficient clinical synthesis . 
 we present here a proposal to summarise a complete breast mr examination presenting contrast - enhanced breast 3d maximum intensity projections ( mips ) and a reduced number of images containing morphologic , dynamic , and metabolic information of lesions described in the report . la rm mammaria ha ormai acquisito un ruolo rilevante nella diagnosi dei tumori mammari in virt della sua elevata sensibilit . 
almeno cinque importanti indicazioni sono definite : stadiazione prechirurgica e pianificazione del trattamento ; sospetta recidiva nella mammella operata ; valutazione delleffetto della terapia neoadiuvante ; ricerca di tumore mammario primitivo occulto in paziente con note metastasi ; sorveglianza delle donne ad alto rischio genetico - familiare di tumore mammario [ 1 ]  . 
sebbene lintegrazione di parametri morfologici e dinamici consenta di ottenere livelli relativamente elevati di specificit [ 2 ] , alcuni autori propongono lutilizzo della spettroscopia protonica per elevare le capacit di caratterizzazione lesionale con un guadagno in specificit [ 36 ]  . in rm mammaria ci troviamo ad affrontare quotidianamente un problema generale per le attuali tecniche tomografiche . 
lo sviluppo di hardware , software e tecniche di postprocessing sempre pi sofisticate ci consente di ottenere immagini native , elaborate e ricostruite comprese le rappresentazioni tridimensionali ( 3d ) di grande interesse non solo per i radiologi ma anche per i chirurghi , i radioterapisti e gli oncologi , come stato dimostrato anche in ambiti differenti da quello rm e delle applicazioni senologiche [ 79 ]  . 
1h - mrs is performed with one ( rarely two or three ) single - voxel point - resolved spin - echo sequence with spectral lipid and water suppression ( tr / te 1 , 500 / 136 ms ; bandwidth 1 khz ; 512 excitations ; acquisition time 13 min )  . 
1h - mrs postprocessing is performed using relatively standardised protocols , including fourier transform , filters ( exponential , gaussian , hennings , rectangular ) , phase and baseline correction , and curve fitting aimed at calculating the area under the investigated compound peaks . 
identification of the different compound peaks is obtained considering the position of their central frequency on the parts per million ( ppm ) axis . thus , at the end of the examination , we have generated 36 predynamic images , 640 native and 512 subtracted images of the dynamic study , and a variable number of multiplanar reconstructions , for a total of more than 1 , 200 images . 
spettroscopia protonica : una ( raramente due o tre ) acquisizioni con sequenza a voxel singolo point resolved spin - echo con soppressione spettrale dei lipidi e dellacqua ( tr / te , 1500 / 136 ms ; banda passante , 1 khz ; 512 eccitazioni ; tempo di acquisizione , circa 13 minuti )  . 
il postprocessing del segnale spettroscopico avviene mediante luso di protocolli relativamente standardizzati che includono la trasformata di fourier , lutilizzo di filtri ( esponenziale , gaussiano , di henning , rettangolare ) ; la correzione della fase e della linea di base ; la costruzione di una curva finalizzata al calcolo dellarea sottesa dal picco dei composti indagati . 
il riconoscimento dei picchi avviene in funzione della frequenza centrale sullasse delle parti per milione ( ppm )  . alla fine dellindagine , abbiamo cos generato 36 immagini predinamiche , 640 immagini native e 512 sottratte dello studio dinamico e un numero variabile di ricostruzioni multiplanari per un totale di oltre 1200 immagini . 
breast magnetic resonance imaging is presented using only maximum intensity projections of the first subtracted images ( a axial ; b coronal ; c right lateral ; d left lateral )  . 
conclusioni del referto : nessun focolaio sospetto di contrast enhancement in entrambe le mammelle . we select a small series of images that can be printed or stored on a digital support , e.g. 
3d mips of the optimal ( considering the best visualisation of the possible lesions ) dynamic subtracted sequence ( 4in - 1 format , if they are printed ) : a . 
selected images for each detected lesion specifically described in the report ( from 20 - in - 1 to 30 - in - 1 film format , if they are printed ) : a . 
immagini selezionate per ciascuna lesione individuata e specificatamente descritta nel referto ( formato da 20 - in - 1 a 30 - in - 1 , se sono stampate ) : a . 
2a - d a 65 - year - old asymptomatic woman with positive x - ray mammography and ultrasound in the lower inner quadrant of the right breast ( not shown )  . 
breast magnetic resonance imaging maximum intensity projections are presented ( a axial ; b coronal ; c right lateral ; d left lateral ) , with multiple foci of contrast enhancement in the lower inner quadrant of the right breast and a small focus of contrast enhancement in the lower inner quadrant of the left breast . 
le mip della rm dinamica ( prima fase contrastografica sottratta ; a , assiale ; b , coronale ; c , laterale destra ; d , laterale sinistra ) evidenziano multipli focolai di contrast enhancement al quadrante infero - interno della mammella destra e un piccolo focolaio di contrast enhancement al quadrante infero - interno di sinistra . 
postprocessed proton spectrum without ( f1 ) and with ( f2 ) calculation of the integral under the choline - containing compounds peak , obtained for the volume of interest including the largest malignant focus located on sagittal ( f3 ) , coronal ( f4 ) and axial ( f5 ) reference images . 
comment : by integrating morphologic and dynamic criteria , the five foci in the right breast were classified as malignant lesions , whereas the focus in the left breast was classified as a probably benign lesion . 
sar tuttavia opportuno che il clinico sia guidato alla valutazione di un limitato numero di immagini selezionate dal radiologo . results risultati the selected items usually range from four ( no detected lesion ) , to 14 ( one lesion , studied with 1h - mrs also ) , to 34 ( five lesions , one studied with 1h - mrs also )  . 
the percentage of items presented with the report compared with the total number of generated images is equal to 0.33% ( 4 / 1 , 200 ) , 1.17% ( 14 / 1 , 200 ) , and 2.83% ( 34 / 1 , 200 ) , respectively . 
thus , breast mr imaging and 1h - mrs can be effectively summarised by presenting a minimal fraction of all generated images . il numero degli oggetti selezionati oscilla usualmente da quattro ( nessuna lesione evidenziata ) a 14 ( una lesione , studiata anche con spettroscopia ) , a 34 ( cinque lesioni , una delle quali studiata anche con spettroscopia )  . 
la percentuale di oggetti presentati rispetto al totale delle immagini pari allo 0 , 33% ( 4 / 1200 ) , 1 , 17% ( 14 / 1200 ) e 2 , 83% ( 34 / 1200 ) , rispettivamente . la rm mammaria ( imaging dinamico e spettroscopia ) pu quindi essere efficacemente sintetizzata presentando solo una minima frazione di tutte le immagini generate . discussion using cross - sectional high - resolution imaging techniques , an heavy bulk of images is increasingly obtained . 
the challenge is to convey the diagnostic message to other physicians selecting a small number of images . subtracted contrast - enhanced 3d mips of the breasts can easily and quickly give a general evaluation of breast vasculature and show possible parenchymal foci of contrast enhancement . 
in our opinion , this approach manages to link the new cross - sectional imaging modality , mr , to a known background ( xray mammography is the standard imaging modality of reference for all physicians dealing with breast diseases ) , adding the coronal view to complete the 3d information . moreover , using an isotropic ( 1 - mm3 voxel ) imaging protocol , the same high spatial resolution is obtained in lateral and axial mips . 
finally , we should take into account that an asymmetrical increased breast mip map was demonstrated to be frequently associated with ipsilateral invasive cancers [ 11 , 12 ]  . when one ore more enhancing foci is specifically evaluated and reported , we present a small selected series of images demonstrating its morphology , dynamics , and metabolismorphology ( shape , borders , signal intensity , and contrast material internal uptake distribution ) is displayed 1066 discussione lutilizzo di tecniche tomografiche ad alta risoluzione genera sempre pi frequentemente un enorme numero di immagini . 
la sfida che occorre raccogliere riuscire a trasmettere il messaggio diagnostico operando la selezione di un numero di immagini molto pi ridotto . le proiezioni mammarie mip 3d delle scansioni contrastografiche sottratte forniscono una rappresentazione rapida e semplificata che rende possibile una valutazione generale della vascolarizzazione mammaria e il riconoscimento di eventuali focolai parenchimali di contrast enhancement . 
a nostro avviso , questo approccio riesce a collegare la nuova modalit senologica tomografica , la rm , a un riferimento ben noto ( la mammografia rimane la tecnica standard per tutti gli specialisti dellambito senologico ) , aggiungendo altres la proiezione coronale a completamento dellinformazione 3d . peraltro , utilizzando un protocollo di studio dinamico isotropico con voxel di 1 - mm3 , si ottiene la medesima elevata risoluzione spaziale anche nelle mip laterali e assiale . 
le immagini mip possono essere concepite come mappe che si aggiungono alla mammografia , soprattutto in caso di discordanza dimensionale del parametro t ( es . : in presenza di un tumore invasivo associato a estensiva componente intraduttale ) o come strumento esclusivo , quando la lesione mammograficamente occulta e visibile solo alla rm . 
metabolism is displayed through the 1h - mrs spectrum associated with three - plane orthogonal images localising the voi . due to the main commitment to cancer detection in breast imaging , it is not surprising that when no suspicious or clinically relevant abnormality is found , only four images can summarise 1 , 192 precontrast and dynamic images : four localizer , 36 predynamic , 640 native , and 512 subtracted of the dynamic study ( note that if multiplanar reconstructions are obtained , a total of 1 , 200 images is reached and probably outnumbered )  . 
 at our hospital , surgeons and oncologists have showed a progressive interest in breast mr after looking at this small series of images we select and present to thepreviously , they were discouraged with the large number of films they received for a breast mr examination . 
none of the colleagues , with the exception of radiologists dedicated to breast mr , can extract clinically useful information from this bulk of data in a small time interval , even if a highquality mr study is done ( the higher examination quality , probably the larger number of images )  . 
printed on films , stored on cd - rom , or also sent through pacs , only a reduced number of selected images can be useful to surgeons , oncologists , radiotherapists , or other physician dealing with breast diseases . the radiologists ability to recognise and characterise breast lesions with mr on the basis of morphology , dynamics , and metabolism must be made available to other physicians while offering a high level of synthesis . 
daltra parte cinque - dieci immagini sono ampiamente sufficienti per mostrare le caratteristiche utili alla caratterizzazione di ciascuna eventuale lesione . chirurghi e oncologi del nostro ospedale hanno mostrato un progressivo interesse verso la rm mammaria osservando soltanto la ridotta serie di immagini che non presentiamo loro . in precedenza , essi si trovavano in difficolt di fronte al grande numero di immagini ( e di pellicole ) che ricevevano per una indagine rm mammaria . 
linvio al clinico di tutta la serie completa delle immagini troppo e troppo poco al tempo stesso : nessuno dei colleghi , con la sola eccezione dei radiologi con esperienza in rm mammaria , sarebbe in grado di estrarre informazione clinicamente utile in tempi ragionevoli da questo ammasso di dati , anche se lindagine rm fosse di elevata qualit ( anzi , pi elevata la qualit dellindagine , tendenzialmente maggiore sar il numero delle immagini )  . 
stampate su pellicola , archiviate su cd - rom o anche inviate mediante pacs , solo un ridotto numero dimmagini sono utili a chirurghi , oncologi , radioterapisti o agli altri colleghi dellambito senologico . labilit del radiologo nel riconoscere e caratterizzare le lesioni mammarie con rm in base a criteri morfologici , dinamici e metabolici deve essere messa a disposizione dei colleghi offrendo un elevato livello di sintesi . 
between march 2001 and june 2003 , cmi was performed on 40 patients ( 27 men and 13 women , age 2358 years , median 41 years ) affected by irreparable medial meniscal lesions . 
all patients underwent mri follow - up at 6 months and 1 year and 16 patients 2 years after the operation ; 12 patients underwent second - look arthroscopy with implant biopsy . all mri examinations were performed with a 1.5 - t unit using ge t2 * , spin - echo ( se ) t1 , and fatsat fast spin - echo ( fse ) dp and t2 - weighted sequences , with different orientations . 
mri follow - up at 6 months showed cmi shape and size to be normal ( type 3 ) in 35 / 40 patients and type 2 in 5 / 40 patients . cmi signal intensity was type 1 in 32 / 40 patients and type 2 in 8 / 40 . 
at 24 months , cmi size was type 3 in 9 / 16 patients , type 2 in 6 / 16 , and type 1 in one patient in whom the implant could not be identified , as it had been totally resorbed . 
quaranta pazienti , 27 maschi e 13 femmine ( di et compresa tra 23 e 58 anni , et mediana : 41 anni ) , sottoposti a impianto di menisco protesico mediale per via artroscopica , hanno eseguito follow - up con rm a 6 mesi e a 1 anno e solo 16 pazienti a 2 anni dallintervento ; in 12 casi stato eseguito second look artroscopico con prelievo bioptico dellimpianto . 
in 2 / 40 pazienti vi era versamento reattivo sinoviale . nel controllo a 12 mesi la morfologia e le dimensioni dellimpianto erano normali ( tipo 3 ) in 33 / 40 pazienti , mentre erano di tipo 2 in 7 / 40 . 
nel controllo a 24 mesi in 9 / 16 pazienti le dimensioni del cmi erano di tipo 3 , in 6 / 16 di tipo 2 ; in 1 pazienti limpianto non risultava identificabile , totalmente patients . 
la rm consente di monitorare nel tempo le variazioni morfologiche e strutturali del cmi , riteniamo che il follow - up possa essere prolungato altre i 2 anni , fino alla stabilizzazione del cmi e alla completa risoluzione delle aree di edema della spongiosa ossea subcondrale . 
nellunico caso di evoluzione sfavorevole del cmi non si sono individuati segni diretti o indiretti correlabili . parole chiave ginocchio impianto di menisco collagenico risonanza magnetica artro - rm menisco operato introduction introduzione meniscal fibrocartilage is a cushioning tissue essential for joint stability in that it controls the transmission of forces and distributes loads across the joint [ 1 , 2 ]  . 
the best treatment for meniscal injury is to preserve the meniscus by suturing the lesion . however , in many cases , meniscal injuries are irreparable and require partial or total meniscectomy [ 4 ]  . 
a tissue engineering technique , however , has provided a prosthetic material with ideal properties : a biocompatible absorbable collagen meniscus derived from bovine achilles tendons , which promotes new meniscal tissue formation [ 813 ]  . the benefits of magnetic resonance imaging ( mri ) in the diagnosis and follow - up of meniscal injuries have already been described in the literature [ 1418 ]  . 
the purpose of our study was to identify mri patterns that could be used to define the evolution of collagen meniscal implants ( cmi ) and correlate them with the clinical and histological data ( from patients undergoing second - look arthroscopy )  . la fibrocartilagine meniscale un interpositore indispensabile alla stabilit articolare , controlla la trasmissione delle forze e distribuisce il carico dellarticolazione [ 1 , 2 ] , ma noto da molto tempo che la perdita di materiale meniscale porta a progressiva degenerazione condrale ed osteocondrale con grave alterazione della funzionalit articolare [ 1 , 35 ]  . 
tuttavia in molti casi le lesioni meniscali non sono riparabili pertanto si esegue una meniscectomia parziale o totale [ 4 ] : per questo motivo la sostituzione del tessuto meniscale asportato con un menisco protesico potrebbe essere una soluzione per prevenire i fenomeni degenerativi [ 6 , 7 ]  . 
con una tecnica di ingegneria tissutale stato ottenuto un materiale protesico con caratteristiche ottimali : un menisco collagenico , derivato da tendine dachille bovino , biocompatibile e riassorbibile che induce la formazione di nuovo tessuto meniscale [ 813 ]  . sono state gi descritte in letteratura i vantaggi della risonanza magnetica ( rm ) nella diagnosi e nel follow - up delle lesioni meniscali [ 1418 ]  . 
scopo del nostro lavoro individuare patterns rm idonei a definire levoluzione dellimpianto collagenico ( cmi ) , comparati con i dati clinici ed istologici ( ottenuti nei pazienti sottoposti a second - look artroscopico )  . materials and methods materiali e metodi mri follow - up was performed on 40 patients ( 27 men and 13 women ; age range 2358 years ; median age 41 years ) treated with bovine collagen meniscus implants positioned via arthroscopy . 
in all cases , a medial prosthetic meniscus was implanted , in the right knee in 24 pail follow - up con risonanza magnetica ( rm ) stato eseguito in 40 pazienti di et compresa tra 23 e 58 anni ( et mediana 41 anni ) , 27 maschi e 13 femmine , sottoposti a impianto di menisco collagenico bovino ( cmi ) per via artroscopica . 
twenty - one patients underwent combined surgical procedures [ 16 anterior cruciate ligament repairs ; two microfractures to treat chondral lesions of the patella and internal femoral condyle , respectively ; two autologous chondrocyte implantations in the medial femoral condyle ( mfc ) ; one valgus tibial osteotomy ]  . all patients underwent clinical and mri follow - up at 6 months and 1 year ; only 16 patients were followed up for 2 years . 
patient selection for second - look arthroscopy was based on clinical findings ( persisting pain ; joint trauma with possible damage to the implant ) and the need for an arthroscopic procedure for associated disorders ( harvesting and implantation of autologous chondrocytes ; removal of tibial plateau from valgus osteotomy )  . 
on the basis of these characteristics , we identified three patterns that were classified from 1 to 3 , with higher scores reflecting patterns more closely resembling those of the normal meniscus ( table 1 )  . 
in 21 casi stata eseguita chirurgia associata ( 16 ricostruzioni del legamento crociato anteriore ; 2 microfratture per trattamento di patologia condrale rispettivamente rotulea e del condilo femorale interno ; 2 impianti di condrociti autologhi a livello del condilo femorale mediale ; 1 osteotomia tibiale devarizzante )  . tutti i pazienti sono stati sottoposti a follow - up clinico e radiologico , mediante esame rm a 6 mesi e a 1 anno , solo 16 pazienti sono rientrati nel follow - up a 2 anni dallintervento . 
la selezione dei pazienti da sottoporre al second look stata effettuata in base a dati clinici ( persistenza della sintomatologia dolorosa ; trauma dellarticolazione con possibile lesione dellimpianto ) e in base alla necessit di sottoporre i pazienti ad un intervento artroscopico per patologia associata a quella del menisco ( prelievo e impianto di condrociti autologhi ; rimozione di placche tibiali da osteotomia devarizzante )  . 
in base a queste caratteristiche abbiamo individuato tre tipi di patterns che abbiamo classificato da 1 a 3 , con valore tanto pi alto quanto pi queste si avvicinano alle caratteristiche del menisco normale ( tabella 1 )  . 
per quanto riguarda i criteri indiretti abbiamo preso in considerazione lo stato del rivestimento condrale nella sede dellimpianto ( condilo femorale e piatto tibiale rispettivamente interno ed esterno ) stimando il grado di erosione cartilaginea considerando una percentuale superiore o inferiore al 50% e leventuale presenza di segni di sofferenza a carico della spongiosa ossea subcondrale corrispondente allimpianto . 
tutte le valutazioni sono state elaborate , indipendentemente , da due operatori ( eg , mga )  . analisi statistica nel confronto di proporzioni , visto il numero ridotto di casi , per la valutazione della morfologia del cmi si utilizzato il test esatto di fisher . 
nel confronto di proporzioni di tabelle superiori a 22 si fatto ricorso al test 2 per la valutazione dellintensit di segnale del cmi in tutti i controlli . risultati follow - up a 6 mesi nel controllo rm a 6 mesi stato evidenziato il cmi in tutti i casi esaminati . 
sono stati identificati 3 casi ( 7 , 5% ) di patologia condrale a livello del condilo femorale mediale , in 1 caso associata a lesione condrale a carico del piatto tibiale corrispondente . 
in 1 / 40 si osservato esteso edema della spongiosa del condilo femorale esterno , non in relazione allimpianto di pertinenza del menisco interno ; lalterazione di segnale stata considerata come algodistrofia , totalmente regredita gi al controllo a 12 mesi . 
collagen meniscus implant ( cmi ) size is identical to that of the normal meniscus : type 3 ( arrow ) ; the sagittal images obtained with fat - suppressed t2 / dp show an inhomogeneous and marked increase in signal intensity : type 1 ( arrow )  . 
b same patient : follow - up at 12 months . on the t2 / dp - weighted sagittal images with fat suppression , scaffold size is type 3 ( arrow ) , but signal intensity is reduced compared with the previous examination ; signal characteristics are type 2 ( arrow )  . 
scaffold size is still type 3 ( arrow ) , but signal intensity is reduced with respect to the examination at 12 months : signal characteristics are type 3 ( arrow )  . 
il cmi presenta dimensioni sovrapponibili a quelle del menisco normale : tipo 3 ( freccia ) , nelle immagini sagittali ottenute in t2 / dp con soppressione del grasso si osserva disomogeneo e marcato aumento dellintensit di segnale : tipo 1 ( freccia )  . 
nelle immagini sagittali ottenute in t2 / dp con soppressione del grasso il complesso mostra dimensioni di tipo 3 ( freccia ) , ma si osserva riduzione dellintensit di segnale rispetto al controllo precedente : le caratteristiche di segnale sono di tipo 2 ( freccia )  . 
il complesso mantiene dimensioni di tipo 3 ( freccia ) , ma si osserva riduzione dellintensit di segnale rispetto al controllo a 12 mesi : le caratteristiche di segnale sono di tipo 3 ( freccia )  . 
nelle immagini sagittali se t1 ottenute dopo iniezione intra - articolare di mdc il cmi mostra dimensioni di tipo 3 ( freccia ) , limpianto integrato , non vi infiltrazione di mdc . showed subchondral bone marrow oedema , which had completely regressed in 5 / 8 patients . 
in the t2 / dp sagittal images with fat suppression , collagen meniscus implant ( cmi ) size is type 3 , and the signal intensity has inhomogeneously increased , reaching type 1 ( white arrow )  . 
nelle immagini sagittali ottenute in t2 / dp con soppressione del grasso le dimensioni del cmi sono di tipo 3 e lintensit di segnale disomogeneamente aumentata , di tipo 1 ( freccia bianca )  . 
il complesso mostra riduzione delle dimensioni del cmi e diviene di tipo 2 ( freccia bianca ) , ma si osserva riduzione delle dimensioni del cmi che diviene di tipo 2 ( freccia bianca )  . 
3a , b on the t2 / dp - weighted and fat - suppressed coronal images , the interface between the prosthetic meniscus and the native meniscus is indicated by a sharp hyperintense line both at 6 ( white arrows in a ) and 12 ( white arrows in b ) months . 
a 12 mesi in nessun caso abbiamo riscontrato reazione sinoviale ( tabella 3 )  . follow - up a 24 mesi nel controllo a 24 mesi la valutazione relativa alla morfologia e allintensit di segnale dellimpianto stata effettuata in base alla valutazione combinata dellesame rm convezionale e dellartro - rm . 
in 11 / 15 pazienti il complesso presentava caratteristiche di segnale di tipo 2 , mentre in 4 / 15 lintensit del complesso era sovrapponibile a quella del menisco normale , di tipo 3 ( fig . 6a ) , confermando la progressiva riduzione dellintensit di segnale osservata al controllo precedente . 
attraverso liniezione di mdc intra - articolare abbiamo potuto stimare il grado di erosione in 1 / 5 > 50% , sottostimato allindagine basale ( fig . 7a , b ) e in 4 / 5 < 50% . 
in 11 / 15 patients , the complex showed type 2 signal characteristics , whereas in 4 / 15 , signal intensity was identical to that 1042 table 3 indirect signs : results at 6 , 12 , and 24 months follow - up chondral pathology subchondral bone marrow oedema synovial reaction e . 
in no case was synovial reaction observed ( table 3 )  . in the 12 patients who underwent second - look arthroscopy and biopsy , a progressive reduction in implant size ( from 25% to 90% ) was identified in the posterior horn region . 
in nessun caso si osservata reazione sinoviale ( tabella 3 )  . nei 12 pazienti sottoposti a second look artroscopico con prelievo bioptico si rilevata una progressiva riduzione delle dimensioni ( da un minimo del 25% ad un massimo del 90% ) dellimpianto a livello del corno posteriore . 
solo in 1 paziente limpianto risultava totalmente riassorbito ( a conferma del rilievo rm ) , con frammenti liberi della protesi . per quanto riguarda lanalisi statistica dei nostri risultati , nella valutazione della morfologia del cmi il test esatto di fisher non ha evidenziato differenze statisticamente significative tra 6 e 12 mesi , mentre la differenza stata significativa tra 6 e 24 mesi ( p = 0 , 033 )  . 
nellanalisi della differenza della sofferenza sottocondrale i dati a 6 mesi confrontati con quelli a 12 mesi , valutati con il test esatto di fisher , mostrano un trend di significativit ( p = 0 , 09 )  . discussione le lesioni meniscali sono di frequente riscontro , rappresentano circa i 2 / 3 di tutte le lesioni del ginocchio , spesso associate a patologie capsulo - legamentose e cartilaginee [ 3 , 18 ]  . in passato la meniscectomia mirava a risolvere la sintomatologia dolorosa , ma nel tempo larticolazione era sottoposta ad anomali carichi sulle superfici articolari e conseguente degenerazione cartilaginea che culminava osteoartrosi [ 4 ]  . 
nel 1992 stato proposto per la sperimentazione sulluomo il cmi che ha dimostrato , dai primi studi a medio termine , risultati incoraggianti [ 3 , 611 , 20 , 21 ]  . 
t2 / dp - weighted sagittal scan with fat suppression : both size and signal intensity are unchanged ( white arrow ) , and a sharp interface can be seen between the prosthetic and native meniscus ( small arrows )  . 
scansione sagittale t2 / dp con soppressione del grasso : le dimensioni del cmi sono di tipo 2 e lintensit di segnale di tipo 2 ( freccia bianca )  . 
scansione sagittale t2 / dp con soppressione del grasso : sia le dimensioni che lintensit di segnale sono invariati ( freccia bianca ) , si evidenzia netta interfaccia tra il menisco protesico e il menisco nativo ( frecce piccole )  . 
in the past , meniscectomy was used to treat pain , but with time , the discussion 1044 cmi ha lo scopo di ripristinare la perdita di sostanza meniscale e favorire i processi di rigenerazione meniscale in caso di meniscectomia parziale [ 711 , 13 , 20 , 21 ]  . 
a t2 / dp - weighted sagittal image with fat suppression : collagen meniscus implant ( cmi ) signal intensity is identical to that of the normal meniscus ( type 3 ) ( white arrow ) , and an interface is visible between the implant and the native meniscus ( small white arrow )  . 
a scansione sagittale t2 / dp con soppressione del grasso : lintensit di segnale del cmi sovrapponibile a quella del menisco normale , di tipo 3 ( freccia bianca ) e si osserva interfaccia tra limpianto e il menisco nativo ( freccia bianca piccola )  . 
a spin - echo t1 - weighted sagittal scan obtained after intra - articular injection of contrast agent : chondral erosion of the internal femoral condyle involving more than 50% of the cartilage thickness ( empty black arrow )  . 
scansione sagittale se t1 , ottenuta dopo iniezione intra - articolare di mdc : erosione cartilaginea del condilo femorale interno che interessa pi del 50% dellintero spessore della cartilagine ( freccia nera vuota )  . 
the purpose of cmi is to compensate for the loss of meniscal tissue and promote meniscal regeneration after partial meniscectomy [ 711 , 13 , 20 , 21 ]  . 
the data provided by morphological and ultrastructural studies have shown that cells are able to migrate within the prosthetic implant , grow , and produce new extracellular matrix [ 8 , 9 , 11 , 20 , 21 ]  . 
a vast body of literature exists on the role of mri with and without contrast material in patients after meniscectomy [ 16 , 17 , 18 , 2226 ] , whereas no studies have investigated the role of mri in patients who have undergone implantation of bovine collagen menisci . in our study , the evaluation of the direct criteria revealed that morphology and size were substantially preserved and similar to those of the normal meniscus in most patients ( 87.5% at 6 months ; 82.5% at 12 months ; 56.25% at 24 months )  . 
in particular , implant height reduction is to be attributed to compressive forces acting on the knee during walking [ 3 ] and does not seem to jeopardise integration of the cmi and native meniscus . the few cases of synovial reaction ( only two cases at 6 months ) and its complete resolution during follow - up reflect the arthroscopic finding that no inflammatory processes affected the implant site , confirming the safety and biocompatibility of the prosthetic material . in our experience , data implant / meniscus complex integration are more controversial : contrary to our expectations , data from the first examination at 6 months may be considered either insufficient or nonsignificant . 
identification of an interface between the residual meniscus and the implant is the only sign that can help distinguish the two components and might be considered an evolutionary step in the integration between the cmi and the native meniscus . unfortunately , however , our data show that the lack of an interface has no significance with regard to an unfavourable implant outcome , as confirmed by the case of complete resorption of the implant at 2 years despite the interface having being identified at 12 months . 
 mri follow - up showed a progressive reduction in implant signal intensity : at 6 months , it was strongly hyperintense in 80% , with a drastic reduction at 12 months ( 35% ) , but no implant had a signal intensity of normal meniscus at either 6 or 12 months . 
the ultrastructural explanation for this lies in the progressive maturation of the newly formed tissue that experiences a reduction in the number of vessels and increased arrangement of collagen cells and fibrils into perpendicular planes [ 3 , 13 ]  . 
in our view , the interpretation of signal patterns of implant / meniscus complexes is still controversial , as only 26.6% of patients showed a signal intensity similar to that of the native meniscus at 24 months . 
ampia la letteratura sul ruolo della rm con e senza mezzo di contrasto nel paziente meniscectomizzato [ 16 , 17 , 18 , 2226 ] , mentre non sono presenti contributi sul ruolo della rm nei soggetti sottoposti ad impianto di menisco collogenico bovino . nella nostra serie la valutazione dei criteri diretti ha permesso di rilevare la sostanziale conservazione di morfologia e dimensioni simili a quelle del menisco normale nella maggior parte dei pazienti ( 87 , 5% dei pazienti a 6 mesi ; 82 , 5% dei pazienti a 12 mesi ; 56 , 25% dei pazienti a 24 mesi )  . 
la riduzione progressiva delle dimensioni documentata con rm ( 37 , 5% dei pazienti a 24 mesi ) confermata dai dati forniti nel corso del second look artroscopico effettuato sugli stessi pazienti . 
in particolare la riduzione in altezza dellimpianto da attribuire alle forze meccaniche in compressione sviluppate sul ginocchio durante la marcia [ 3 ] , e non sembra compromettere lintegrazione cmi - menisco nativo . lo scarso riscontro di reazione sinoviale ( solo 2 casi a 6 mesi ) e la completa risoluzione nel follow - up corrisponde al dato artroscopico di assenza di fenomeni infiammatori a livello dellimpianto , confermando la sicurezza e biocompatibilit del materiale protesico utilizzato . nella nostra esperienza riteniamo pi controverse le informazioni sullintegrazione del complesso impianto / menisco : queste possono essere ritenute scarse o non significative , al contrario di quanto si prevedeva nel primo controllo a 6 mesi . 
lidentificazione di una interfaccia tra il menisco residuo e limpianto lunico segno che pu aiutare a distinguere le due componenti e potrebbe essere considerato evolutivo dei processi di integrazione tra il cmi ed il menisco nativo , ma , sfortunatamente , alla luce dei nostri dati , lassenza di interfaccia non significativa per una evoluzione sfavorevole del complesso . 
questa affermazione sembra avvalorata dal fatto che in un caso , seppur in presenza di interfaccia dimostrata al controllo a 12 mesi , si potuto evidenziare il completo riassorbimento del complesso nel controllo a 2 anni dallintervento ; il dato stato confermato dallartroscopia , infatti in sede di impianto non si riscontrato tessuto simil - meniscale . il follow - up con rm ha rilevato progressiva riduzione dellintensit di segnale dellimpianto : a 6 mesi nell80% dei casi limpianto risultava marcatamente iperintenso con drastica riduzione a 12 mesi ( 35% ) , ma sia a 6 che a 12 mesi nessun impianto mostrava intensit di segnale sovrapponibile a quella del menisco normale . 
il dato si spiega dal punto di vista ultrastrutturale con la progressiva maturazione del tessuto neoformato che va incontro alla riduzione del numero dei vasi e a maggiore organizzazione in piani ortogonali delle cellule e delle fibrille collageniche [ 3 , 13 ]  . 
alla luce della nostra esperienza rimane controversa linterpretazione dellevoluzione del segnale del complesso impianto / menisco , in quanto solo il 26 , 6% dei pazienti a 24 mesi mostra intensit di segnale sovrapponibile a quella del menisco nativo , tale valutazione ci induce a sospettare che a 2 anni , in una buona percentuale , il complesso non abbia completato il processo di maturazione o rigenerazione tissutale e quindi non possiamo ritenere concluso il follow - up . us to suspect that in most cases , the complex has not yet completed the process of tissue maturation or regeneration after 2 years and that consequently , we cannot consider the follow - up to be concluded . 
 the purpose of the bovine collagen meniscus implant is to restore the physiological thickness of the fibrocartilage cushion in order to re - establish correct distribution of articular loads and prevent possible cartilage damage from the wear caused by altered biomechanical loads . 
the aim of mri is therefore not only to assess the meniscus / implant complex but to identify possible early signs of chondral and subchondral disorders that may herald possible failure . chondral lesions have been shown to remain substantially unchanged at imaging 5 years after implantation [ 27 ]  . 
in our series , the chondral alterations observed at 6 months remained unchanged at 12 months , in agreement with the literature [ 27 ] , but two new cases of chondral lesions were identified at follow - up after 24 months . 
in our series , follow - up at 24 months included the use of intra - articular contrast material , which significantly increases the rate of detection of small chondral lesions [ 26 ]  . 
it may therefore be advisable to use intra - articular contrast material as early as the first follow - up examination at 6 months , as it is very likely that the chondral lesions that appeared after 2 years were in fact present earlier but could not be identified with conventional mri . 
 we can reasonably state that the first follow - up at 6 months does not enable us to establish any certain correlation between associated chondral lesions and subchondral bone marrow oedema . 
in most cases , the signal alteration of the spongy bone decreases or disappears at later follow - up examinations , and no direct correlation can be identified between subchondral bone marrow oedema , chondral lesions and possible implant failure . 
in fact , in the only case with implant resorption , which occurred between 12 and 24 months , the previous examinations showed neither subchondral bone marrow oedema nor chondral lesions . 
 finally , we can conclude that mri is a valuable modality for the follow - up of patients who have undergone collagen meniscus implants and that , in light of our results , intra - articular contrast material should preferably be injected at the first follow - up examination to identify any chondral lesions as early as possible . 
we believe that only the follow - up can allow one to express certain judgements on implant integration , a process that can be considered concluded only when complete stabilisation of the complex has been demonstrated . 
this corresponds to the finding of markedly low signal intensity typical of the meniscus and complete resolution of bone marrow oedema , a process that could take more than 2 years in some patients . 
la rm non ha quindi il solo compito di valutare il complesso menisco / impianto , ma ha lo scopo di individuare la presenza di segni precoci di sofferenza condrale e sotto - condrale che possano prevedere leventuale fallimento terapeutico . 
stata descritta sostanziale stabilit nel tempo delle lesioni condrali nei controlli strumentali a 5 anni dallimpianto [ 27 ] , nella nostra serie le alterazioni condrali osservate al controllo a 6 mesi si sono mantenute immodificate a 12 mesi , in accordo con quanto riportato in letteratura [ 27 ] , ma si sono osservati 2 nuovi casi di lesioni condrali al controllo a 24 mesi . 
questa discrepanza tra gli studi potrebbe essere spiegata con la differente tecnica utilizzata , infatti nella nostra casistica i controlli a 24 mesi prevedevano lutilizzo di mdc intra - articolare che incrementa sensibilmente il riconoscimento delle piccole lesioni condrali [ 26 ]  . 
tali considerazioni sono sufficienti a concludere che forse preferibile associare il mdc intra - articolare gi al primo controllo a 6 mesi , poich , molto verosimilmente , le nuove lesioni condrali comparse a 2 anni si sarebbero potute riconoscere pi precocemente , infatti tali alterazioni non erano identificabili allesame basale ed in un paziente con lartro - rm stato possibile modificare il grading della lesione condrale . con buona approssimazione si pu affermare che al primo controllo a 6 mesi non possibile stabilire una sicura correlazione tra le lesioni condrali associate e la sofferenza della spongiosa sotto - condrale . 
lalterazione di segnale della spongiosa decresce o scompare nella maggior parte dei casi con lavanzare del follow - up ed inoltre non possibile stabilire una diretta correlazione tra la sofferenza della spongiosa , le lesioni condrali e leventuale fallimento dellimpianto ; infatti nellunico caso di riassorbimento dellimpianto , avvenuto tra i 12 e 24 mesi , nei controlli precedenti non vi erano aree di sofferenza della spongiosa sottocondrale e lesioni condrali , quindi tali alterazioni possono essere considerate segni indiretti correlati alla sintomatologia dolorosa e alla stabilit dellarticolazione , ma non segni predisponesti al fallimento dellimpianto . in conclusione si pu affermare la validit del follow - up strumentale con rm nei pazienti sottoposti ad impianto con menisco collagenico e che alla luce di quanto emerso sia preferibile iniettare il mdc intra - articolare gi al primo controllo , al fine di individuare pi precocemente eventuali sofferenze condrali . 
noi riteniamo che solo il follow - up pu esprimere giudizi sicuri sullintegrazione dellimpianto e questo pu ritenersi concluso solo quando si sia dimostrata la completa stabilizzazione del complesso che corrisponde al raggiungimento delliposegnale caratteristico del menisco e la completa risoluzione delledema della spongiosa , quindi in taluni pazienti potrebbe essere giustificato il prolungarsi dei controlli oltre i 2 anni . 
albrizio , the queen elizabeth hospital , kings lynn , norfolk , pe30 4et , uk , tel . : + 44 - 0155 - 3766649 , fax : + 44 - 0135 - 5584473 , e - mail : contact@drmauroalbrizio.it received : 23 november 2006 / accepted : 26 january 2007 / published online : 19 october 2007 abstract ppurpose . 
lintroduzione del wells score non ha prodotto una variazione statisticamente significativa del tasso di ctpa positive . parole chiave ctpa wells embolia polmonare metodi predittivi introduction introduzione there is ample evidence in the literature to support computed tomography pulmonary angiography ( ctpa ) as the first - line imaging investigation for suspected pulmonary embolism ( pe ) [ 16 ]  . 
with the widespread availability of multislice ct scanners , ctpa has effectively rendered conventional pulmonary angiography obsolete , despite limited sensitivity in the visualisation of subsegmental clots [ 7 ]  . 
ctpa offers the significant advantage of identifying a wide range of chest diseases , thereby facilitating differential diagnosis [ 8 , 9 ]  . the advent of multislice and multiplane technology has la validit della ctpa quale strumento di scelta per la diagnosi di embolia polmonare ( pe ) riportata in diversi studi scientifici [ 16 ]  . 
nel regno unito , la disponibilit di ctpa su tutto il territorio nazionale ha reso obsoleto luso dellangiografia polmonare nonostante lefficacia limitata della ctpa nel rilevare la presenza di emboli di piccola taglia [ 7 ]  . 
studies have even shown that patients with clinically suspected acute pe , no symptoms or signs of deep venous thrombosis ( dvt ) and negative ctpa generally have a good clinical outcome at 3 months and that it is probably safe to withdraw anticoagulation treatment in such cases [ 1 , 13 ]  . according to a meta - analysis by moores et al . 
for this reason , ctpa is often applied as part of a screening algorithm that includes predictive rules [ 14 , 15 ] and other diagnostic tests such as d - dimers , lower - extremity ultrasonography and lung scintigraphy [ 1619 ]  . 
it is an important step in contemporary diagnostic strategies aiming to limit the number of unnecessary imaging investigations . the two most widely used prediction models for pe described in the literature are the canadian prediction rule ( the wells score ) and the geneva prediction rule . 
we present an audit that aims to evaluate the effect of the protocol on the rate of positive ctpas . materials and methods at our hospital all ctpas are requested on a standard x - ray form , usually filled in by an accident and emergency ( a&e ) or ward doctor and signed by a consultant . 
the local protocol uses a slice thickness of 3.2 mm , a pitch of 1.25 and a reconstruction interval of 1.6 mm ; 100 ml of 300 mg i / ml iohexol are administered at a rate of 3 ml / s through an 18 - gauge antecubital venous cannula . 
ctpa is performed in arrested inspiration starting at the lung bases and covering the entire thorax . a list of all patients who underwent ctpa from august 2004 to january 2005 and from march 2005 to august 2005 was obtained from the computerised radiology information syste using a sequential method , we selected 100 cases from the preimplementation period ( that is , prior to february 2005 ) and 100 from the postimplementation period ( that is , after february 2005 )  . 
mean age was 65 years ( 63 in the preimplementation period and 67 in the postimplementation period ) ranging from 18 to 91 years . lavvento delle ctpa multislice e multiplane ha poi ulteriormente affinato laccuratezza dellimmagine permettendo una diagnosi pi precisa [ 10 ]  . 
al momento la letteratura conferma che la ctpa offre una sensibilit complessiva del 77% ( 95% per embolie segmentali e 89% per embolie pi voluminose ) e una specificit dell89% [ 12 ]  . 
sulla base di questi risultati alcuni studiosi hanno addirittura affermato che i pazienti con sospetta embolia polmonare , ma senza sintomi di trombosi delle vene profonde degli arti inferiori ( dvt ) e con una ctpa negativa hanno generalmente un risultato clinico soddisfacente a 3 mesi e che quindi plausibile , in tali casi , la sospensione del trattamento anticoagulante [ 1 , 13 ]  . dunque esistono numerose evidenze scientifiche che confermano laccuratezza della ctpa nella diagnosi di embolia polmonare . 
secondo la meta - analisi di moores [ 1 ] , ogni volta che viene sospettata unembolia polmonare , il paziente ha una probabilit di conferma radiologica che varia tra il 15 , 4% e il 37 , 4% . 
per questo motivo la ctpa spesso parte di algoritmi diagnostici che includono metodi predittivi [ 14 , 15 ] e altri strumenti come i d - dimeri , lecografia delle vene degli arti inferiori e la scintigrafia polmonare [ 1619 ]  . 
questa suddivisione pu risultare estremamente utile se ci si pone lobiettivo di limitare il numero di pazienti esposti inutilmente a radiazioni . i due modelli predittivi pi usati per lembolia polmonare sono il canadian prediction rule ( o wells score ) e il geneva prediction rule . 
lo scopo di questo studio dunque quello di valutare gli effetti di tale protocollo sul tasso di ctpa positive per embolia polmonare . materiali e metodi nella nostra struttura ospedaliera , le ctpa sono richieste a mezzo di un modulo compilato da personale medico di qualunque livello , tuttavia sempre necessaria la firma di un primario . 
la scansione viene effettuata a 3 , 2 mil mezzo di contrasto ( iohexol ) somministrato ad una velocit di 3 ml / secondo utilizzando un ago cannula di 18 g generalmente in una vena antecubitale . 
mizzi : rate of computed tomography pulmonary angiographies ( ctpa ) positive for pulmonary embolism and predictive scores results table 1 shows the demographic distribution of patients before and after protocol implementation . 
tables 2 and 3 summarise the sources of referral for ctpa : the majority of referrals to the radiology department ( 58% of the total 200 patients ) came from an acute medical ward both in the pre - implementation and post - implementation periods , but it is not possible to define whether these patients had arrived on ward following a first assessment at the a&e or by their general practitioner . 
positive findings other than pe were seen in up to 62% of ctpas . discussion since february 2004 , patients presenting to our institution with a high clinical probability for pe ( as demonstrated by the wells score ) have been treated with low molecular weight heparin and only subsequently assessed by ctpa . 
in patients with an intermediate or low clinical probability of pe , ddimers are assayed : if d - dimers are elevated , the patient proceeds to ctpa , whereas if they are negative , pulmonary embolism is reliably excluded and ctpa is not performed . 
however , there was no significant difference in the rate of positive ctpas before and after protocol implementactpa poi effettuata in ispirazione partendo dalla base del torace . utilizzando il database del dipartimento di radiologia abbiamo ottenuto la lista dei pazienti sottoposti a ctpa tra agosto 2004 e gennaio 2005 ( periodo precedente allintroduzione del nuovo protocollo ) e tra marzo 2005 e agosto 2005 ( periodo successivo allintroduzione del protocollo )  . usando un metodo sequenziale , abbiamo selezionato 100 casi nel periodo precedente lintroduzione del protocollo e 100 casi nel periodo successivo , per un totale di 200 pazienti . 
let di tali pazienti variava da 18 a 91 anni con una mediana di 65 ( 63 nel periodo precedente allintroduzione del protocollo e 67 nel periodo successivo )  . risultati la tabella 1 rappresenta la distribuzione demografica dei pazienti prima e dopo lintroduzione del protocollo . 
la provenienza della richiesta di consulenza radiologica rappresentata nelle tabelle 2 e 3 : la maggior parte delle richieste di ctpa ( 58% del totale ) proveniva da un reparto di medicina sia prima che dopo lintroduzione del protocollo . 
lortopedia risultava essere la specialit chirurgia con pi alta percentuale di richieste di consulenza radiologica , ma anche quella con pi alto tasso di ctpa negative . sul totale di 200 pazienti con sospetta embolia polmonare , la conferma radiologica stata ottenuta in 50 casi ( 25% del totale ; 23% nel periodo antecedente lintroduzione del wells score e 27% nel periodo successivo )  . 
nel 62% dei table 1 demographic distribution of patients before and after protocol implementation pre - implenentation period patients with confirmed pte post - implementation period patients with confirmed pte n . 
patients males / females age ( mean ) number of d - dimer requests 4555 tabella 1 distribuzione demografica dei pazienti prima e dopo lintroduzione del protocollo periodo antecedente pazienti con conferma periodo successivo alllintroduzione diagnostica di pe del protocollo allintroduzione del protocollo pazienti con conferma diagnostica di pe 1211 1211 2664 2664 1215 1215 n . 
mizzi : rate of computed tomography pulmonary angiographies ( ctpa ) positive for pulmonary embolism and predictive scores table 2 source of referral for ctpa source of referral pre - implementation post - implementation casi la ctpa ha consentito di pervenire ad una diagnosi diversa da quella di embolia polmonare . discussione a partire da febbraio 2004 , nella nostra clinica i pazienti con alta probabilit di essere affetti da embolia polmonare sono trattati con eparina a basso peso molecolare e solo successivamente allinizio della terapia sono sottoposti a ctpa . 
per i pazienti con probabilit medio - bassa il valore dei d - dimeri a guidare il management successivo : se i ddimeri sono elevati , il paziente viene sottoposto a ctpa , se i d - dimeri sono negativi la diagnosi di pe si pu considerare esclusa e la ctpa non viene considerata come strumento diagnostico . nel nostro studio la percentuale di pazienti con confermata embolia polmonare variata dal 23% al 27% con lintroduzione del wells score . 
se consideriamo il range della meta - analisi di moores [ 1 ] possiamo confermare che i risultati ottenuti sia nel periodo antecedente lintroduzione del wells score sia in quello successivo non si discostino affatto dallintervallo di valori rilevato . ciononostante , a livello puramente statistico , lintroduzione del wells score non ha portato ad un cambiamento significativo nel numero di pazienti con diagnosi di pe confermata . 
tale risultato pu avere una duplice spiegazione : ( i ) il protocollo ( e quindi il wells score ) non offre nessun vantaggio predittivo - diagnostico rispetto al semplice esame tabella 2 provenienza della richiesta di ctpa provenienza della richiesta di ctpa ( reparti ) periodo antecedente periodo successivo allintroduzione del protocollo ( % ) allintroduzione del protocollo ( % ) medical ward geriatrics general surgery orthopaedics thoracic surgery medical out - patient 3 unit itu and ccu oncology gynaecology medicina ( reparto ) pronto soccorso geriatria chirurgia generale 2 ortopedia chirurgia toracica 2 medicina ( clinica ) terapia intensiva oncologia ginecologia table 3 post - operative patients general surgery thoracic gynaecology orthaopaedic total tabella 3 pazienti post - operatori source chirurgia generale chirurgia toracica ginecologia ortopedia totale source pre - implementation ( % ) pre - implementation ( % ) post - implementation ( % ) post - implementation ( % ) total ctpas positive for pe total ctpas positive for pe periodo antecedente alllintroduzione del protocollo ( % ) periodo antecedente alllintroduzione del protocollo ( % ) periodo successivo allintroduzione del protocollo ( % ) periodo successivo allintroduzione del protocollo ( % ) numero totale di ctpa positive per pe numero totale di ctpa positive per pe m . 
this suggests one of two possibilities : ( 1 ) the protocol ( the wells score ) offers no significant predictive - diagnostic advantage over plain clinical judgement , or ( 2 ) the protocol exists in theory but is not being adhered to in clinical practice . it is clear that the number of patients recruited in this study is not sufficiently large to refute the validity of the wells score , which has been widely validated by the literature and whose predictive value can be therefore assumed . the most likely reason for the results of this audit remains the second possibility : the protocol may not have been adequately applied in clinical practice . 
if this is true , we believe there might be a potential for increasing further the rate of positive ctpas and thus reducing the number of patients undergoing unnecessary scans . an example of how this could be achieved is the introduction of a specific mandatory pro - forma to be submitted whenever a request for ctpa is made . 
the pro - forma would include details of clinical probability ( wells score ) , d - dimer levels ( when appropriate ) and make reference to the hospital protocol ; it would also represent a legal document attesting to the need to expose the patient to ionising radiation as well as being an excellent tool for further research . clinico , ( ii ) il protocollo esiste in teoria , ma non stato applicato sufficientemente nella pratica clinica . 
va sottolineato che il numero di pazienti utilizzato per questo studio non abbastanza grande da consentire di confutare la validit del wells score confermata invece da una larga porzione di letteratura scientifica . 
se tale interpretazione corretta si pu considerare potenzialmente possibile un ulteriore incremento del numero di ctpa positive con lobiettivo di ridurre il numero di pazienti esposti inutilmente a radiazioni . un esempio di come tale risultato possa essere ottenuto lintroduzione di un pro - forma obbligatorio da compilare ogni qualvolta una richiesta di ctpa viene avanzata . 
tale pro - forma conterrebbe riferimenti al wells score , ai d - dimeri ( se necessari ) e al protocollo ospedaliero in s e sarebbe anche un documento legale comprovante la necessit di esporre il paziente a radiazioni nonch un ottimo strumento per lo svolgimento di ulteriori indagini scientifiche . conclusions the results of this audit show that the rate of positive ctpas at our hospital lies well within the accepted range . 
simplification of the scoring criteria and the introduction pro formas are recommended . conclusioni i risultati di questo studio dimostrano che il tasso di ctpa positive rientra nel range indicato in letteratura come accettabile . 
zobel1 1centro interdisciplinare per la ricerca bio - medica , department of radiology , 2department of oncology , universit campus bio - medico di roma , via longoni 47 , i - 00155 roma , italy correspondence to : c.c. 
analysis of the cases observed for the first time during the 19962000 period showed osteolytic lesions in 53.6% ( 15 / 28 ) , osteosclerotic lesions in 32.1% ( 9 / 28 ) and mixed lesions in 14.3% ( 4 / 28 )  . 
tra il 1996 e il 2005 , 468 pazienti con carcinoma della mammella sono stati sottoposti presso il nostro dipartimento ad una tc di stadiazione o per follow - up . 
in pazienti con metastasi ossee , la tc ha rilevato 18 pazienti con lesioni osteolitiche ( 30% ) , 32 con lesioni osteoaddensanti ( 53 , 3% ) e 10 ( 16 , 7% ) con lesioni miste . 
lanalisi dei casi osservati per la prima volta nel periodo compreso tra il 1996 e 2000 , ha mostrato lesioni osteolitiche nel 53 , 6% dei casi ( 15 / 28 ) , lesioni osteoaddensanti nel 32 , 1% dei casi ( 9 / 28 ) e miste nel 14 , 3% dei casi ( 4 / 28 ) mentre i risultati erano rispettivamente del 9 , 4% ( 3 / 32 ) , 71 , 9% ( 23 / 32 ) e 18 , 7% ( 6 / 32 ) per gli stessi gruppi nel periodo compreso tra il 2001 e 2005 . 
lanalisi istologica di tutti i casi evidenziava la presenza di carcinoma duttale infiltrante nel 81 , 9% dei casi , di carcinoma lobulare infiltrante nel 11 , 2% dei casi , di carcinoma duttale lobulare misto nel 3 , 7% dei casi e nel 3% dei casi di carcinoma midollare . 
imaging of bone metastases in breast cancer is an essential step to stage the disease , plan a therapeutic intervention and monitor response to treatment , whether chemotherapy , radiotherapy or endocrine therapy . 
numerous imaging modalities are now used , such as conventional x - rays , bone scintigraphy , computed tomography ( ct ) , magnetic resonance imaging ( mri ) , positron emission tomography ( pet ) and single photon emission ct ( spect )  . 
however , a standard diagnostic and follow - up protocol has not been established in clinical practice , and meta - analyses have not been possible because of the heterogeneity of imaging data . moreover , the response evaluation criteria to solid tumours ( recist ) system always considered bone disease as an unmeasurable entity until hamaoka et al . 
revised those criteria by including ct and mri findings , highlighting the contribution of these techniques above all in the assessment of bone response to therapy [ 4 ]  . compared with conventional x - rays where at least 30% variation of mineral content is necessary to reach the detection threshold [ 5 ] , ct shows areas of decreased or absent density ( osteolytic , due to the destruction of bone matrix ) or hyperdense areas as in sclerotic bone lesions ( osteosclerotic ) , confirming the positive finding of bone scan hypermetabolic areas , with a relatively low cost in the context of whole - body follow - up study and a higher sensitivity ranging from 71% to 100% [ 6 ]  . 
ct provides the most accurate morphological images of the bone , allowing visualisation of compact and trabecular bone and tumour margins and dimensions [ 4 ] ; on follow - up studies , it depicts the presence of sclerosis in the context of lytic lesions , thus allowing a better evaluation of response to treatment [ 4 ]  . 
 even though single - slice ct has had limited value in the evaluation of multiple bone sites , the advent of multislice and spiral ct has allowed whole - body scans in a very short time . 
lavvento dei bifosfonati di terza generazione pu aver cambiato laspetto tc delle metastasi ossee da carcinoma della mammella . parole chiave tomografia computerizzata carcinoma della mammella metastasi ossee acido zoledronico il carcinoma della mammella caratterizzato da una alta prevalenza di metastasi ossee : dal 30% al 85% dei pazienti con metastasi da cancro della mammella presenta un coinvolgimento secondario osseo durante il corso della patologia [ 1 , 2 ] e losso rappresenta il primo sito di metastasi dal 26% al 50% dei casi [ 2 , 3 ]  . 
limaging delle metastasi ossee nel carcinoma della mammella rappresenta una tappa essenziale nella stadiazione della patologia , nella pianificazione di un adeguato intervento terapeutico e nel controllo della risposta al trattamento , sia esso chemioterapico , radioterapico o endocrino . 
numerose tecniche di imaging sono oggi utilizzate e comprendono la radiologia tradizionale , la scintigrafia ossea , la tomografia computerizzata ( tc ) , la risonanza magnetica ( rm ) , la tomografia ad emissione di positroni ( pet ) e la tomografia computerizzata a singola emissione di positroni ( spect )  . 
tuttavia , non stato ancora stabilito un protocollo standard per la diagnosi ed il follow - up nella pratica clinica e studi di metanalisi non sono stati possibili soprattutto per la grande eterogeneit dei dati radiologici . 
 [ 4 ] hanno modificato questi criteri includendo le informazioni derivanti dalle immagini tc e rm , evidenziando il miglioramento che queste tecniche apportano , specialmente nella valutazione della risposta dellosso alla terapia . rispetto alla radiologia tradizionale , dove per evidenziare una lesione necessaria una perdita di almeno il 30% del contenuto minerale dellosso [ 5 ] , la tc mostra aree di densit assente o diminuita ( osteolitiche ) , dovuta alla distruzione della matrice ossea , o aree iperdense come da lesioni ossee sclerotiche ( osteoaddensanti ) , che confermano la presenza di aree di ipercaptazione alla scintigrafia , con un costo relativamente basso nel contesto di un follow - up total body e con una sensibilit che varia dal 71% al 100% [ 6 ]  . 
la tc fornisce le immagini pi accurate della morfologia ossea , permettendo la visualizzazione dellosso compatto e trabecolare , del margine e delle dimensioni del tumore [ 4 ]  . 
lytic lesions , reducing the bone resistance to load or tangential forces , are strongly linked to skeletal - related events , including pathological fractures , radiation therapy , bone surgery or spinal cord compression [ 9 ]  . 
 the advent of new ct equipment and the routine use of ct scans in the follow - up of breast cancer patients may have modified the real incidence of bone metastases and their radiological appearance in comparison with the past . 
here we present a retrospective analysis of the radiological appearance of bone metastases in patients with advanced breast cancer referred to our department through 19962005 in which we observed a predominant osteosclerotic pattern on ct scans . 
images were obtained with a single - row ct ( high speed general electric , 19962003 ) and with 16 - row spiral ct scanner ( somatom sensation 16 , siemens , 20032005 )  . 
ct studies were performed before and during bolus administration of nonionic iodinated contrast agent at a concentration of 350 mgi / ml ( iobitridol xenetix , guerbet , france )  . 
the malignant nature of the lesions was determined by considering progression , the presence of nel contesto di lesioni litiche , consentendo cos una migliore valutazione della risposta al trattamento [ 4 ]  . sebbene la tc a singolo strato ha avuto un valore limitato nella valutazione di siti multipli di metastasi , lavvento della tc multistrato e spirale permette di effettuare oggi uno studio di tutto lo scheletro osseo in poco tempo . 
la tc totalbody fa parte oggi degli esami di routine nel protocollo di follow - up dei pazienti oncologici e la possibilit di valutare lintero volume corporeo , usando la finestra per losso , ha dato alla tc un ruolo molto importante nel diagnosticare lesioni ossee e nel valutare la risposta alla terapia [ 7 , 8 ]  . 
le lesioni litiche , riducendo la resistenza dellosso alle forze tangenziali e di carico , sono fortemente correlate ad eventi scheletrici definiti sre ( skeletal related events ) , e che includono linsorgenza di fratture patologiche , terapia radiante dellosso , e terapia chirurgica ortopedica [ 9 ]  . 
le lesioni miste rappresentano daltra parte uno stadio intermedio tra le lesioni litiche e le blastiche . lavvento di nuove tecniche tc e luso di routine della tecnica tc nei protocolli di follow - up del carcinoma della mammella potrebbero aver modificato la reale incidenza delle metastasi ossee e il loro quadro radiologico rispetto al passato . 
in questo lavoro presentiamo una analisi retrospettiva del quadro radiologico delle metastasi ossee nelle pazienti affette da carcinoma della mammella in stadio avanzato osservati nel nostro dipartimento nel periodo compreso tra il 1996 e 2005 , nei quali abbiamo osservato un aspetto di tipo prevalentemente osteoaddensante allesame tc . 
tra il 1996 e il 2005 , 468 donne con una diagnosi di carcinoma della mammella sono state sottoposte ad un esame tc nel nostro dipartimento , sia per effettuare una prima stadiazione , sia per follow - up . 
dal 2000 sono giunte allosservazione nel nostro dipartimento donne affette da carcinoma della mammella che provenivano dal programma di screening effettuato seguendo le linee guida dellautorit regionale di sanit del lazio . 
le immagini sono state ottenute con tc a singolo strato ( high speed general electric 19962003 ) e con tc spirale a 16 strati ( somatom sensation 16 , siemens , 20032005 )  . 
le immagini sono state acquisite prima e durante somministrazione di mezzo di contrasto , alla concentrazione di 350 mgi / ml ( iobitridol , xenetix , guerbet , francia )  . 
negli studi di follow - up , le pazienti venivano sottoposte di routine ad un esame tc ogni sei mesi nel primo anno e ogni dodici mesi nei successive cinque anni . lesame tc ha evidenziato metastasi sistemiche in 142 / 468 pazienti , 60 delle quali con coinvolgimento osseo , confermato dalla scintigrafia ossea . 
due esperti radiologi hanno osservato indipendentemente gli esami tc delle pazienti con carcinoma della mammella , riportando su un file di microsoft excel laspetto delle metastasi ossee ( litiche , miste o addensanti ) e la loro localizzazione . 
also , grading of breast cancer at histology failed to correlate with radiological appearance of bone metastases at initial diagnosis . since 2001 , 20 out of 47 patients received zoledronic acid i.v. 
 ( zometa , novartis pharma stein ag , switzerland ) ( 4 mg every 28 days )  . higher prevalence of osteosclerotic lesions we performed a temporal distribution curve of lytic , mixed and sclerotic metastases and observed an increased prevalence of sclerotic changes since 2000 . 
women undergoing mastectomy , with a histological grade defined according to the nottingham method and a stage according to the tnm classification , were 68.3% ( 41 / 60 )  . 
the prevalence of osteosclerotic lesions at higher ptn did not change significantly , whereas osteolytic lesions became significantly more abundant . evaluation and interpretation of mixed lesions ( meaning a mixture of lytic and blastic lesions in the same patient or a mixture of lytic and sclerotic component in the same lesion ) was difficult due to the limits of a retrospective observation . association between bone metastasis and zoledronic acid treatment zoledronic acid was introduced in the chemotherapy protocols in 2001 . 
in pazienti con metastasi ossee , la tc ha rilevato 18 pazienti con lesioni osteolitiche ( 30% ) , 32 con lesioni osteoaddensanti ( 53 , 3% ) e 10 con lesioni miste ( 16 , 7% )  . 
lesame istologico di tutti i casi ha evidenziato l81 , 9% di carcinoma duttale infiltrante ; l11 , 2% di carcinoma lobulare infiltrante : il 3 , 7% di carcinoma misto duttale - lobulare ed il 3% di carcinoma midollare . 
non stata trovata correlazione tra il grading istologico del carcinoma della mammella alla prima diagnosi e laspetto radiologico delle metastasi alla prima diagnosi . a partire dal 2001 , 20 dei 47 pazienti sono stati trattati con somministrazione endovenosa di acido zoledronico ( zometa , novartis pharma stein ag , svizzera ) 4 mg ogni 28 giorni . incremento della prevalenza delle lesioni osteoaddensanti abbiamo analizzato le curve di distribuzione nel tempo delle lesioni metastatiche litiche , miste e osteoaddensanti ed abbiamo osservato un aumento della prevalenza delle modificazioni sclerotiche a partire dal 2001 . 
paragonando la distribuzione delle metastasi ossee tra i due gruppi , abbiamo trovato un valore chi quadro molto alto con una differenza statisticamente significativa ( p < 0 , 001 ) nella direzione di una pi alta prevalenza di lesioni ostreoaddensanti . correlazione tra metastasi ossee e stadio del carcinoma della mammella alla prima diagnosi non abbiamo trovato una correlazione statisticamente significativa tra laspetto radiologico delle metastasi ossee ed il tipo istologico del tumore primitivo . 
le donne sottoposte ad un intervento chirurgico di mastectomia , con un grado istologico definito secondo il metodo di nottingham e la stadiazione definita secondo la classificazione tnm , erano il 1053 c.c. 
we found no correlation with sclerosis of bone metastases when standard chemotherapy agents , antiestrogens and chemotherapy plus monoclonal antibodies ( trastuzumab , herceptin ; roche , basel , switzerland ) were considered . 68 , 3% ( 41 / 60 )  . 
le pazienti con una stadiazione pt1n0 e pt1n1 - 3 alla prima diagnosi presentavano rispettivamente il 75% e il 50% di lesioni osteoaddensanti , mentre non erano evidenti lesioni litiche . 
test 2 mostra una differenza statisticamente significativa ( p < 0 , 05 ) acido zoledronico no acido zoledronico totale discussion bone metastases are osteostructural dysmorphisms due to secondary localisation of tumour cells following systemic dissemination through the blood and / or lymphatic vessels . in the case of breast cancer , they have been described to be mainly osteolytic ( up to 50% ) , as areas of bone resorption , and , more rarely , as osteosclerotic , as areas of bone deposition , or mixed [ 1 , 12 ]  . 
this phenomenon has been explained by the activation of osteoclastic activity in the bone tissue stimulated by a paracrine effect of substances produced by the tumour cells , such as the parathyroid - hormone - related protein ( pthrp ) [ 13 ] , interleukin - 8 ( il - 8 ) [ 14 ] , il - 11 and vascular endothelial growth factor ( vegf ) , as well as bonederived mediators such as tumour growth factor ( tgf ) - beta [ 15 ] and insulin - like growth factor - 1 ( igf - 1 ) [ 16 ]  . 
lanalisi degli effetti sullaspetto delle metastasi ossee dovuti alla somministrazione di acido zoledronico stata effettuata dividendo le pazienti del gruppo 20012005 in due gruppi : quelle trattate con acido zoledronico ( n = 20 ) e quelle non trattate ( n = 27 )  . 
un aumento statisticamente significativo delle lesioni osteoaddensanti stato osservato nel gruppo trattato con acido zoledronico ( p < 0 , 05 ) ( tabella 1 )  . durante la ristadiazione effettuata mediante tc condotta sulle stesse pazienti , una variazione sclerotica progressiva stata inoltre osservata durante i trattamenti chemioterapici che comprendevano la somministrazione ev di acido zoledronico . 
non abbiamo trovato una correlazione statisticamente significativa tra sclerosi delle metastasi ossee ed altri trattamenti farmacologici : agenti chemioterapici standard , antiestrogeni e chemioterapia standard con associazione di anticorpi monoclonali ( trastuzumab , herceptin , roche , basilea , svizzera )  . discussione le metastasi ossee si possono definire come dismorfismi osteostrutturali determinati dalla localizzazione secondaria delle cellule tumorali in seguito a disseminazione sistemica per via ematica o linfatica : nel caso del carcinoma della mammella sono state descritte come lesioni prevalentemente litiche ( in pi del 50% dei casi ) e , soltanto raramente , come lesioni osteoaddensanti in quanto aree di deposizione ossea o come lesioni miste [ 1 , 12 ]  . 
questo fenomeno stato spiegato dallattivazione osteoclastica del tessuto osseo , stimolata dalleffetto indotto da sostanze paracrine prodotte da cellule tumorali come le proteine producenti ormone analogo del pth ( pthrp ) [ 13 ] , interleuchina 8 ( il - 8 ) [ 14 ] , interleuchina 11 e fattore di crescita vascolare endoteliale ( vegf ) e mediatori derivati dallosso come il tgfbeta [ 15 ] e il fattore di crescita analogo dellinsulina di tipo i ( igf - 1 ) [ 16 ]  . 
lattivazione degli osteoclasti come fattore principale determinante losteolisi , stato confermato dallevidenza che gli osteoclasti sono stati trovati in prossimit dei depositi di tumore osseo alla microscopia elettronica e dal fatto che le lesioni ossee di tipo osteolitico presentano delle lacune di riassorbimento osteoclastico ben riconoscibili . 
inoltre , i farmaci in grado di inibire lattivit osteoclastica ( ad esempio bifosfonati , plicamicina , e nitrato di gallio ) sono attivi contro tutti i tipi di metastasi ossea [ 12 ] e riducono inoltre la ipercalce1055 c.c. 
una donna di 51 anni con carcinoma della mammella ( carcinoma duttale infiltrante , pt2n1 ) sottoposta a mastectomia e chemioterapia adiuvante , ricevette diagnosi di metastasi osteolitiche nel 1999 . durante trattamento con acido zoledronico , le lesioni litiche vertebrali mostrano progressiva sclerosi , fino a coinvolgere completamente la lesione . 
a e d immagini tc ottenute nel marzo 2004 ; b ed e stesso livello delle immagini a e d rispettivamente , ottenute sei mesi dopo ; c ed f stesso livello delle immagini a e d rispettivamente , ottenute dodici mesi dopo . well - recognisable osteoclast resorption lacunae . 
on the other hand , it has been shown that breast cancer cells may directly promote bone resorption in vitro , producing both mineral release and bone matrix degradation , when added to devitalised bone [ 17 ] , leading to the hypothesis of a possible convergence of the two mechanisms in the origin of osteolysis . the most common sites of bone involvement include axial bones such as vertebrae and pelvis , possibly because of the high vascularity and abundant presence of red bone marrow , even though ribs , skull and femur may also be involved [ 7 , 8 , 18 ]  . ct is very useful in detecting bone metastases and assessing their response to treatment [ 7 , 8 ]  . 
daltra parte , tuttavia , stato dimostrato che le cellule neoplastiche del carcinoma della mammella possono promuovere direttamente il riassorbimento osseo in vitro , determinando il rilascio di prodotti di degradazione della matrice ossea , quando aggiunti ad osso devitalizzato [ 17 ] , permettendo cos di ipotizzare una possibile convergenza dei due meccanismi allorigine dellosteolisi . le sedi pi comuni di coinvolgimento dellosso comprendono lo scheletro assiale , tra cui le vertebre e la pelvi , verosimilmente a causa dellabbondante vascolarizzazione e della presenza di midollo ematopoietico , anche se possibile il coinvolgimento di coste , cranio e femore [ 7 , 8 , 18 ]  . la tc molto utile nellindividuare metastasi ossee e nel valutare la risposta al trattamento [ 7 , 8 ]  . 
tuttavia il progredire della lisi ossea o la comparsa di nuove aree di osteolisi , che possono presentarsi o allinterno di aree di sclerosi o in regioni miste o come au1056 c.c. 
a 68 - year - old woman received a diagnosis of breast cancer ( pt1n0 ) in 1993 and follow - up studies were negative until osteolytic lesions were diagnosed in 2004 ( a , c )  . 
the significance of these distribution changes is not clear , but some hypotheses can be suggested . in the last year bone metastases have been diagnosed earlier than in the past , also thanks to the advent of breast cancer screening programmes that have led to earlier therapeutic approaches . 
even though a correlation study , in respect to the stage of disease at the time of diagnosis , was not possible due to the small size of groups , the trend observed is worth of further analysis on larger populations . response to chemotherapy treatments has been correlated with sclerosis of bone metastases , even though a clear association between cytotoxic drugs and osteosclerotic lesions has never been demonstrated . 
adding bisphosphonates to chemotherapy protocols has become a standard strategy in mento delle dimensioni originarie di una lesione blastica , potrebbero rappresentare un indice di progressione di malattia . nel nostro studio retrospettivo abbiamo rilevato una alta prevalenza di lesioni ossee metastatiche osteoaddensanti in pazienti affette da carcinoma della mammella nel periodo compreso tra il 20012005 rispetto a quelle del periodo compreso tra il 19962000 ( 71 , 9% versus 32 , 1% )  . 
il significato del cambiamento di questa distribuzione non ancora chiaro ma possono comunque essere avanzate alcune ipotesi . nellultimo periodo le metastasi ossee sono state diagnosticate pi precocemente grazie ai programmi di screening , consentendo trattamenti pi precoci . 
sebbene non sia possibile uno studio di correlazione rispetto alla precocit della diagnosi , a causa del campione troppo piccolo , landamento osservato appare meritevole di ulteriori analisi su un campione di maggiori dimensioni . la risposta al trattamento chemioterapico stata correlata con la sclerosi delle metastasi ossee anche se una chiara associazione tra i farmaci citotossici e le lesioni di tipo osteoaddensante non stata trovata . 
bisphosphonates are accumulated in the site of metabolically active bone and play a complex role on bone metastasis , modifying the osteoblastosteoclast equilibrium [ 20 ]  . different functions have been ascribed to biphosphonates and especially to zoledronic acid , such as a direct antitumoural effect and antiosteoclastic and antiangiogenetic activity . 
the first is explained by the proapoptotic effect played against the tumour cells , inhibiting their growth and possibly their invasion through the endothelium [ 2124 ]  . the antiosteoclastic activity is realised through inhibition of formation , migration and activity of osteoclasts [ 25 , 26 ] and by inducing osteoclastic apoptosis [ 27 ]  . 
administration of 4 mg of zoledronic acid [ 28 ]  . a macroscopic effect of zoledronic acid through change ct appearance of bone metastases could be related to all three of these effects on bone metabolism , with sclerosis of osteolytic lesions explained by a reduction of osteoclastic activity and a decrease in microvascular perfusion of bone lesions . the correlation between zoledronic acid and osteosclerotic lesions due to metastatic breast cancer brings new insights into the mechanisms of response to therapy of bone metastases . 
a prospective analysis conducted on follow - up studies , comparing ct appearance of bone metastases before and after zoledronic acid treatment , will clarify some of the questions raised by these preliminary data . minato una riduzione definitiva dellincidenza di eventi scheletrici ( sre ) [ 19 ]  . 
lacido zoledronico un bifosfonato di terza generazione , con una attivit clinica stimata 100 volte maggiore dei bifosfonati di prima generazione ( ad esempio etidronato , clodronato ) , inibendo il riassorbimento osseo anche a concentrazioni micromolari . 
i bifosfonati si accumulano nelle sedi ossee metabolicamente attive e giocano un ruolo complesso sulle metastasi ossee , modificando lequilibrio tra osteoblasti e osteoclasti [ 20 ]  . funzioni diverse sono state attribuite ai bifosfonati ed in modo particolare allacido zoledronico , tra questi un effetto antitumorale diretto , una attivit anti - osteoclastica ed una attivit anti - angiogenica . 
leffetto anti - angiogenico supportato dallevidenza di una riduzione significativa dei livelli sierici di vegf dopo la somministrazione ev di 4 mg di acido zoledronico [ 28 ]  . un effetto macroscopico dellacido zoledronico evidenziabile attraverso la modificazione dellaspetto tc delle metastasi ossee potrebbe essere correlato a tutti e tre questi effetti sul metabolismo osseo con conseguente sclerosi delle lesioni osteolitiche dovute ad una riduzione dellattivit osteoclastica , ed ad una riduzione della perfusione vascolare nelle lesioni ossee . la correlazione tra acido zoledronico e le lesioni osteoaddensanti da metastasi della mammella apre nuove prospettive nellanalisi del meccanismo di risposta alla terapia delle metastasi ossee . 
radiologia , roma , italy 2istituto di medicina del lavoro delluniversit cattolica del sacro cuore , largo gemelli 8 , i - 00168 roma , italy 3medico del lavoro , roma , italy 4u.o. 
regardless of the outcome of legal proceedings , physicians who are sued usually perceive the claim as an assault on their integrity and may suffer psychological or physical effects known as malpractice stress syndrome . 
radiological errors were purportedly related to occupational discomfort , and the latter variable was significantly associated with work dissatisfaction and a low level of psychological and physical well - being . 
i radiologi hanno una buona conoscenza del fenomeno della cosiddetta malpractice medica e della cause che contribuiscono ad enfatizzarlo , cos come delle condizioni lavorative che causano stress da lavoro , insoddisfazione e aumento degli errori ; mostrano per una insufficiente padronanza delle tecniche di clinical risk management e della dottrina del consenso informato . 
analysis of reports presented by radiologists to the professions insurance agency between 1993 and 2005 to safeguard themselves from legal proceedings of civil liability shows that about one half of insured radiologists have received or will shortly receive a claim for compensation or will be called to face criminal proceedings related to their professional activity performed in the last decade . 
in one third of these cases , claims refer to events involving the death of the patient , which produces requests for very high compensation payments and possible severe criminal repercussions [ 1 ]  . apart from the legal consequences , however , litigation can become a stress factor for the physician known as malpractice stress . 
we therefore felt the need to perform a study in italy regarding the consequences that compensation claims for civil liability and criminal proceedings have on the well - being and professional conduct of radiologists . le denunce contro i medici per presunta malpractice sono un fenomeno di rilievo anche in italia . 
lanalisi delle segnalazioni presentate dai radiologi allistituto assicuratore tra il 1993 ed il 2005 per tutelarsi da azioni di responsabilit civile indica che circa la met dei radiologi assicurati ha ricevuto o sta per ricevere una richiesta di risarcimento o una citazione penale relativa allattivit professionale svolta nellultimo decennio . 
in un terzo dei casi le denunce si riferiscono ad eventi nei quali si verificato il decesso del paziente ; ci determina richieste di risarcimento di importo molto elevato e possibili pesanti ripercussioni penali [ 1 ]  . al di l delle conseguenze legali , lazione di responsabilit pu rappresentare per il sanitario un fattore di stress , il cosiddetto stress da malpractice . 
che la denuncia per responsabilit civile rappresenti per il medico un vero e proprio fattore di stress stato intuito sin dalla fine degli anni 80 , dai ricercatori americani [ 2 ] ; studi recenti dimostrano come il timore di denunce sia in grado di influenzare i comportamenti dei medici e le loro scelte professionali [ 35 ]  . 
ci parso necessario , pertanto , avviare anche nel nostro paese unindagine sulle conseguenze che le richieste di risarcimento per responsabilit civile e le denunce penali esplicano sul benessere e sui comportamenti professionali dei medici radiologi . materials and methods radiologists attending two radiology and oncology radiotherapy congresses were invited to anonymously respond to a questionnaire that explored their knowledge and opinions regarding malpractice , their personal experience of litigation for alleged malpractice and how they coped with the event . the questionnaire comprised two parts : one devised ad hoc for the study and one derived from previously published experiences . 
the first part of the questionnaire asked respondents to provide some personal data ( gender , age range , years of professional experience , professional role or qualification , type of public or private professional activity ) and included a series of questions relating to malpractice and the causes of clinical error . 
opinions regarding malpractice were investigated through a series of 24 statements : physicians were invited to express their level of agreement to each statement . replies were graded from ( 1 ) strongly disagree to ( 5 ) strongly agree , according to a 5 - point likert scale . 
in this case , the scale ranged from ( 1 ) totally irrelevant to ( 5 ) highly relevant . the second part of the questionnaire contained the italian version of several standardised questionnaires modified to render them appropriate to the sample being studied . 
with these tools we aimed to assess ( 1 ) consequences of litigation , ( 2 ) level of job satisfaction and ( 3 ) level of individual 1070 materiali e metodi i radiologi partecipanti a due congressi di radiologia e di radioterapia oncologica sono stati invitati a compilare un questionario anonimo , che indagava le conoscenze ed opinioni riguardanti il fenomeno della malpractice , la personale esperienza di denunce per presunta malpractice e il vissuto relativo a tale evento . 
la prima parte del questionario richiedeva lindicazione di alcuni dati anagrafici ( sesso , classe di et , anni di esperienza professionale , ruolo o qualifica professionale , tipo di attivit professionale pubblica o privata ) e conteneva una serie di domande relative alla malpractice ed alle cause di errore medico . 
le opinioni relative al fenomeno della malpractice sono state indagate proponendo ai medici radiologi una serie di 24 affermazioni ed invitandoli ad esprimere il grado di consenso con ciascuna affermazione . 
la risposta era graduata da ( 1 ) non sono affatto daccordo a ( 5 ) sono del tutto daccordo , secondo una scala analogico verbale - numerica di likert . 
this questionnaire was developed to describe the consequences of an assault , a threat or another form of harassment and was used in the italian version to assess the consequences of violent actions on health care workers [ 7 , 8 ]  . 
in this case , only the section regarding harassment was considered , which involves ten possible responses ( fear , distress , anger , anxiety , humiliation , guilt , disappointment , helplessness , physical harm or no harm )  . 
the overall score , which is obtained by adding up the scores to all of questions and therefore ranges from 7 to 70 points , expresses the degree of job satisfaction . 
psychological and physical well - being at the time of the study was assessed using the goldberg general health questionnaire [ 11 ] in the 12 - item version ( ghq - 12 ) , which is recommended as a valid screening test for psychological distress [ 12 ]  . 
each of the ghq - 12 questions offers the choice of four responses , which can either be interpreted in a bimodal fashion or with an increasing score in the manner of a likert scale . 
adoption of the former or the latter method influences only the frequency of subjects classified as possible cases but not the validity of the results at the group level [ 12 ]  . bearing this in mind , we chose to use a 4 - point likert scale , because this method produces results better approaching normal distribution . 
the final score ranges from 12 to 48 points ; low values correspond to complete well - being , whereas higher values are indicative of a state of psychological tension . we distributed 350 questionnaires at the two congresses : 321 were returned , of which seven were discarded as being incomplete . 
a total of 314 physicians therefore responded to the questionnaires , equivalent to a response rate of 89.7%. data were analysed with the spss software package ( statistical package for social sciences )  . 
analysis of the frequency of the individual variables was conducted using descriptive statistics , whereas comparison between groups was performed using the mann - whitney u test for nonparametric data . 
this technique derives principal components , giving rise to correlation matrices that indicate strength of association among the variables . la seconda parte del questionario conteneva la versione italiana di alcuni questionari standardizzati , con opportune modificazioni che li rendevano adeguati alla casistica in oggetto . 
mediante tali strumenti ci si proposti di valutare ( a ) le conseguenze della denuncia ; ( b ) il grado di soddisfazione ricavata dallattivit professionale ; ( c ) il livello individuale di benessere psico - fisico al momento dellindagine . 
tale questionario stato messo a punto allo scopo di descrivere le conseguenze di una aggressione , di una minaccia o di unaltra forma di molestia ed stato usato , nella versione italiana , per valutare le conseguenze di azioni violente sul personale sanitario [ 7 , 8 ]  . in questo caso stata impiegata ovviamente solo la sezione relativa alle conseguenze delle azioni moleste , che consta di dieci possibili risposte ( paura , angoscia , rabbia , ansia , umiliazione , senso di colpa , delusione , senso di essere indifeso , danni fisici , o nessun danno )  . 
il livello di soddisfazione ricavata dal lavoro stato indagato mediante il questionario messo a punto da warr [ 9 ] , nella versione specificamente impiegata per indagini su popolazioni mediche [ 10 ]  . 
lo stato di benessere psicofisico al momento dellindagine stato valutato tramite il general health questionnaire di goldberg [ 11 ] , nella versione in 12 domande che stata raccomandata come valido test di screening per il distress psicologico [ 12 ]  . 
ciascuna delle domande del ghq - 12 prevede quattro risposte , che possono essere interpretate con un punteggio dicotomo , o con un punteggio crescente come una comune scala likert . ladozione di uno o dellaltro metodo influenza solo la frequenza di soggetti classificabili come possibili casi , ma non la validit dei risultati a livello di gruppo [ 12 ] ; in considerazione di ci , abbiamo impiegato in questo lavoro la scala likert in 4 punti , perch in tal modo i risultati approssimano meglio la distribuzione normale . 
il punteggio finale varia da 12 a 48 punti ; valori bassi corrispondono al pieno benessere , mentre valori elevati esprimono uno stato di tensione psicologica . nelle diverse sedi congressuali sono stati distribuiti 350 questionari ; i medici ne hanno restituiti 321 e di questi 7 sono stati scartati perch incompleti . 
complessivamente , quindi , hanno risposto 314 medici , pari all89 , 7% degli intervistati . i dati sono stati analizzati mediante il software statistico spss ( statistical package for social science )  . 
per lanalisi delle frequenze delle singole variabili sono state utilizzate le statistiche descrittive ; i confronti tra gruppi sono stati effettuati con il test u di mann whitney per dati non parametrici . stata impiegata lanalisi della regressione logistica ( forward stepwise conditional logistic regression ) per la selezione dei fattori predittivi nel caso di variabili dipendenti binarie , come ad esempio lavvenuta denuncia per malpractice . 
a large majority were men ( 251 men , 79.9% ; 63 women ) , and nearly all were practising in the public sector ( 289 physicians , > 92% )  . 
physicians practising within the national health system fell into three categories : 20% were department heads ( 59 ) , 19% were division heads ( 56 ) and the remaining 61% were staff physicians ( 174 )  . 
demographics of the sample are summarised in table 1 . one third of physicians ( 105 , 33.4% ) responded that they had been sued for civil or criminal liability with a request for compensation at some time . 
there were no significant differences between radiotherapists and radiologists with regard to demographic variables ( gender , age ) , or work - related variables ( experience , role , public or private sector )  . 
the mean number of consequences of litigation indicated by radiologists was 2.8 , whereas only 11.3% of respondents reported not having suffered any harm . with regard to the consequences malpractice litigation had on their professional practice , 39.0% of respondents admitted having altered their professional conduct . 
indeed , the mean number of consequences and the frequency of each consequence of malpractice litigation was the same in the two groups when compared using the mann - whitney u test . opinions on malpractice respondents were asked to express their opinions on the subject of malpractice , and their responses demonstrated that they were aware of the risk of civil and criminal proceedings . in fact , 246 ( 78.3% ) stated they strongly agreed with the statement : the radiologist is exposed to civil and criminal 1072 riabile dipendente . 
la seconda variabile selezionata tramite il coefficiente di correlazione parziale pi elevato , e candidata per linserimento ; se ne valuta per anche luscita dal modello , con un valore di significativit predefinito ( p = 0 , 10 )  . 
mediante tale statistica si procede allestrazione di componenti principali , dando luogo a matrici di correlazione che indicano la forza di associazione delle variabili tra di loro . risultati hanno partecipato 314 medici , di cui 108 specialisti in radioterapia e 206 specialisti in radiologia in attivit lavorativa . 
i soggetti esaminati risultavano prevalentemente di sesso maschile ( 251 maschi , pari al 79 , 9% , 63 femmine ) , e quasi tutti operanti nel settore pubblico ( 289 medici , oltre il 92% )  . i medici dipendenti del ssn erano per il 20% direttori di unit operativa ( 59 unit ) , per oltre il 19% responsabili di struttura semplice ( 56 unit ) , per il rimanente dirigenti medici ( 174 unit , 61% )  . 
la classe di et pi frequente risultata quella compresa tra 46 e 50 anni ( 27 , 7% ) , la categoria di esperienza lavorativa pi frequente quella superiore a 26 anni ( 22 , 6% )  . 
 un terzo dei medici ( 105 soggetti , pari al 33 , 4% ) ha risposto nel questionario di avere subito in passato una denuncia civile o penale con richiesta di risarcimento . 
il gruppo dei radioterapisti non presentava differenze significative con quello dei radiologi per nessuna delle variabili anagrafiche ( genere , et ) n per quelle legate al lavoro ( esperienza , ruolo , attivit nel settore pubblico o privato )  . 
anche la prevalenza delle denunce risultata uguale nei due gruppi , se confrontata con il test u di mann whitney ( p > 0 , 19 ) ( tabella 1 )  . lanalisi di regressione logistica ha dimostrato che il solo fattore anagrafico significativamente associato con loccorrenza di denunce let ( p < 0 , 0001 ) , mentre gli altri fattori ( genere , anni di esperienza , tipo di struttura pubblica o privata , posizione gerarchica ) non sono correlati ( tabella 2 )  . conseguenze della denuncia i radiologi e radioterapisti che avevano subito una denuncia per presunta malpractice sono stati invitati a riferire le sensazioni provate in relazione allaccaduto . 
apprendere di essere stati denunciati ha indotto in molti radiologi : sensazione di essere indifeso ( 39 , 0% ) , delusione ( 32 , 4% ) , angoscia ( 32 , 4% ) , umiliazione ( 19 , 0% )  . 
significance calculated with the two - tailed mann - whitney u test for nonparametric data entire group number ( % ) radiologists number ( % ) radiotherapists number ( % ) significance p value 251 ( 79.9 ) 167 ( 81.1 ) role department head division head staff physician other tabella 1 caratteristiche anagrafiche del campione esaminato e confronto tra i due sottogruppi ( radiologi e radioterapisti )  . 
al contrario , solo l11 , 3% dichiara di non avere riportato alcun danno . per quanto riguarda le conseguenze che la denuncia ha avuto sulla condotta professionale , il 39 , 0% degli intervistati ha ammesso di avere cambiato la propria condotta . 
the first was statistically associated with seven of the eight causes ( excessive workloads , insufficient time , obsolete equipment , lack of opportunity to consult with colleagues , inadequate continuing education , poor work organisation , tense and uncooperative work climate ) , whereas the second component was correlated only with imprecise requests from referring physicians . the two components have a clear logical construct in that the first expresses distress related to the workplace and the second expresses distress related to the external environment . by adding the responses to the seven questions making up the first component , an indicator of workplace distress can la maggior parte dei professionisti intervistati ritiene che il rischio di denuncia non riguardi solo i meno preparati ( 74 , 2% di pareri contrari ad una affermazione in tal senso , contro il 15 , 6% di favorevoli ) , e che le denunce siano imprevedibili e indipendenti dalla perizia personale ( 73 , 2% di approvazione a questa proposizione ) e possano colpire chiunque ( il 92 , 7% si pronuncia in tal senso )  . 
la prima di tali domande registra una differenza molto significativa ( p < 0 , 005 ) tra coloro che hanno subito una denuncia e gli altri , con i primi pi decisi a negare che il rischio di denuncia riguardi solo i meno preparati . in larga prevalenza , gli intervistati ritengono che gli anziani siano pi esperti dei giovani ( 65 , 4% favorevoli , 14 , 6% incerti , 20% contrari a questa affermazione )  . 
sono incerti sullaffermazione che i giovani possano essere pi aggiornati ( 8 , 9% del tutto daccordo , 43 , 9% parzialmente daccordo , 23 , 6% incerto , 23 , 5% contrario ) , ma tendono a pensare che i giovani facciano pi errori degli anziani ( 49 , 7% daccordo , 28% incerto , 22 , 3% contrario )  . nel complesso , la larga maggioranza del campione ( 73% ) si dichiara preoccupata di poter essere denunciata ; tale preoccupazione significativamente maggiore nel gruppo di chi ha gi subito una denuncia ( p < 0 , 018 )  . 
i radiologi / radioterapisti ritengono che il rischio di denunce spinga a modificare in senso difensivo la pratica medica ( 86 , 6% daccordo o del tutto daccordo )  . le cause delle denunce il fenomeno della malpractice medica sarebbe sostenuto da una serie di fattori ( tabella 3 ) , tra i quali i radiologi annoverano , in ordine di frequenza , lorientamento dei massmedia in senso non favorevole ai medici ( 65 , 3% del tutto daccordo , 23 , 2% daccordo , solo 5 , 7% contrario ) , la possibilit di ottenere cospicui risarcimenti ( 49% del tutto daccordo , 35% daccordo , 6% contrario ) e le dichiarazioni di altri medici ( 81% daccordo , 9% contrario )  . 
tra i fattori favorenti il rischio di denunce vengono indicati anche i cattivi rapporti con i pazienti ( concorda oltre il 71% ) e le pretese eccessive dei pazienti ( concorda il 60% )  . 
meno della met ( 40 , 5% ) attribuisce laumento delle denunce genericamente allo sfascio della sanit , mentre una percentuale analoga di specialisti ( 37 , 9% ) contrario a tale affermazione , ed il rimanente 21 , 7% incerto . alcune di queste risposte risentono significativamente delle esperienze personali . 
i medici che hanno subito una denuncia indicano con frequenza significativamente maggiore rispetto agli altri le responsabilit di altri medici ( p < 0 , 0001 ) , il ruolo dei mass media ( p < 0 , 002 ) , la ricerca di risarcimenti ( p < 0 , 019 )  . lerrore diagnostico tra i fattori che concorrono a determinare lerrore in radiologia e radioterapia ( tabella 4 ) vengono annoverati , in ordine di consenso , i ritmi di lavoro eccessivi ( vengono definiti molto importanti dal 67% degli intervistati e concorda sullimportanza un ulteriore 30% ) , i tempi insufficienti per la refertazione per i radiologi , o per i radioterapisti lelabo1075 a . 
it should be borne in mind that in identifying the causes of error , there were no significant differences between those who had been involved in civil or criminal proceedings and those who had not . possible solutions despite the fact that according to respondents the risk of malpractice litigation would lead radiologists to adopt defensive practices , only 34.7% believe that suggesting further examinations is an appropriate method for avoiding litigation , whereas 51.6% were not in favour of this type of behaviour . most respondents felt that constant adherence to guidelines , even when not convinced of their usefulness , would help to avoid malpractice litigation ( 51% ) , even though 18% were uncertain and 31% did not agree . 
in contrast to these last findings , with regard to the need or otherwise of informing the patient of the results of the radiological examination , 34% of radiologists believe it is better not to inform the patient in the event of an unfavourable diagnosis , because the patient may not be prepared to face such a diagnosis . 
a further 15% were uncertain how to respond , so the percentage of those who would always inform the patient even in the event of an unfavourable diagnosis fell to about 50% . opinions regarding the usefulness of clinical risk management techniques were divided . 
in this context , there was also a certain difference between those who have and those who have not been sued for alleged malpractice , with the former expressing greater faith in clinical risk management . 
tale disagio risulta inversamente correlato con la soddisfazione dal lavoro e con il livello di benessere psicofisico : al crescere del disagio per lambiente di lavoro si associano bassi livelli di soddisfazione ( correlazione inversa , coefficiente di segno negativo ) ed elevati livelli di malessere psicologico , misurati dal ghq - 12 ( correlazione diretta , coefficiente di segno positivo ) ( tabella 6 )  . 
importante sottolineare che nellidentificazione delle cause di errore non emergono differenze significative tra coloro che avevano subito una denuncia civile o penale rispetto a quelle degli altri colleghi non denunciati . le possibili soluzioni nonostante il fatto che secondo gli intervistati il rischio di denunce avrebbe spinto molti radiologi a modificare in senso difensivo la propria pratica , solo il 34 , 7% ritiene che per evitare denunce sia bene suggerire lesecuzione di ulteriori accertamenti , mentre il 51 , 6% contrario a tale atteggiamento . seguire sempre le linee guida , anche se non si convinti della loro reale utilit , consentirebbe di evitare il contenzioso secondo la maggior parte degli intervistati ( 51% ) , anche se , a questo riguardo , si rileva il 18% di incerti ed il 31% di contrari . 
questa domanda registra una differenza significativa tra coloro che hanno subito una denuncia e gli altri ( p < 0 , 038 ) , con una maggiore propensione a seguire acriticamente le linee guida da parte dei primi . con riferimento al consenso informato , l84 , 7% ritiene necessario raccoglierlo nei casi in cui la tecnica radiologica potrebbe comportare problemi per il paziente ( si noti che circa il 13% dei radiologi decisamente contrario a chiedere il consenso ) , mentre il 97 , 5% ritiene necessario informare in modo completo i pazienti . 
in us hospitals , the radiology department is among those that receive the highest number of claims for compensation due to diagnostic error [ 15 ] , and payments for incorrect radiological diagnosis are amongst the highest [ 16 ]  . 
the most recent data regarding the italian situation show that the risk of litigation for civil liability has become as significant for italian radiologists as it is in the united states , albeit with a lower incidence [ 1 ]  . considerations regarding the relevance of the problem led us to investigate the phenomenon among italian radiologists to determine their opinions on the topic and to assess the effects that civil and criminal proceedings have on physician health . 
as far as we know , this is the first attempt to shed light on the topic . this study has the limitation of not having been performed on a randomised population . 
nonetheless , the high representation of one category ( radiotherapists ) with respect to the national total , and the fact that there were no significant differences between responses provided by radiotherapists and those provided by radiologists , suggests that the study faithfully reflects the real situation . our study takes into consideration two different albeit closely related features : diagnostic errors and malpractice litigation , with the aim of assessing the consequences of these features on the health and professional behaviour of the study population . 
due to reasons linked to how errors are detected , data regarding medical error is highly uncertain italy there have been a number of estimates based on patient reporting , which place radiologists in a comparatively better situation than other specialists ( table 7 )  . 
the technical committee on clinical risk of the ministry of health , however , has dedicated special attention to the problem of error in radiology [ 18 ] , which is a clear sign of the significance of the problem . in our study , physicians who responded to the questionnaire clearly demonstrated their awareness of strategies for reducing radiological errors , particularly those which reason [ 19 ] classifies as latent errors errors that are inherent to the workplace . 
adequate time and workload and the availability of human resources and appropriate equipment are undoubtedly conditions that can enhance a policy of limiting the risk of clinical error in radiology as in other medical fields . our study appears to demonstrate a widespread and alarming situation of discomfort caused by the excessive workloads and insufficient time for reporting results or formulating treatment plans , poor work organisation and a noncooperative and tense working climate . 
added to this are staff shortages , which in many cases render consulting with colleagues for a second opinion practically impossible ; obsolete radiological equipment ; and the inability to be sufficiently up to date at the professional level . 
even though these factors were examined with reference to an abstract situano di comunicare al paziente lesito della indagine radiologica , il 34% dei radiologi ritiene che sia meglio non informare il paziente in caso di diagnosi infausta , perch questi potrebbe non essere pronto a riceverla , ed un ulteriore 15% palesa incertezze a questo quesito , per cui la percentuale di quanti informerebbero in ogni caso il paziente dei risultati dellindagine radiologica infausta scende al 50% circa . i pareri sullutilit delle tecniche di clinical risk management sono divisi . 
centodieci radiologi ( il 35% ) manifestano incertezza e i rimanenti sono equamente divisi tra quanti ritengono utili le tecniche di gestione del rischio clinico ( 33 , 1% ) e quanti invece temono che la segnalazione sistematica spontanea di errori e quasi errori ( near miss events ) possa aumentare il rischio di denunce contro i medici ( 31 , 9% )  . 
a questo proposito si manifesta anche una certa divaricazione tra chi ha subito una denuncia e chi no , con una dichiarata maggiore fiducia dei primi nella gestione del rischio clinico ; la differenza , tuttavia , non raggiunge significativit statistica ( p > 0 , 07 )  . oltre la met degli intervistati ritiene necessario un intervento del legislatore per limitare le denunce contro i medici ( concorda il 64 , 6% ) ; tale ipotesi vede maggiormente favorevoli coloro che hanno gi subito una denuncia ( p < 0 , 024 )  . discussione la diagnostica per immagini in usa la specialit a pi alto rischio di denunce per malpractice , dopo le discipline chirurgiche [ 14 ]  . 
sempre in usa in ospedale , il dipartimento di radiologia tra quelli che ricevono il maggior numero di denunce per errore diagnostico [ 15 ] e gli indennizzi per errata diagnosi radiologica sono tra i pi elevati in assoluto [ 16 ]  . 
i pi recenti dati riferiti al nostro paese consentono di affermare che il rischio di denuncia per responsabilit civile ha assunto per i radiologi italiani rilievo paragonabile a quello che si osserva negli stati uniti , anche se con incidenza inferiore [ 1 ]  . le considerazioni sulla rilevanza del problema ci hanno spinto ad indagare tra i medici radiologi italiani , al fine di conoscere le loro opinioni sullargomento , e di valutare gli effetti che le denunce civili e penali hanno sulla salute del medico . 
a nostra conoscenza , questo il primo tentativo di fare luce sullargomento . questo studio ha la limitazione di non essere stato svolto su una popolazione randomizzata ; tuttavia , lelevata rappresentazione di una categoria ( quella dei radioterapisti ) rispetto al totale nazionale , e il fatto che non emergano significative differenze nelle risposte fornite dai radioterapisti rispetto a quelle dei radiologi , inducono a ritenere che lo studio fornisca una buona rappresentazione della realt . la nostra ricerca ha preso in considerazione due aspetti diversi , anche se tra loro strettamente correlati : quella dellerrore diagnostico , e quello delle denunce per malpractice , al fine di valutare le conseguenze sullo stato di salute e sui comportamenti professionali . 
this is confirmed by the fact that the discomfort measured in this way is significantly and inversely correlated with job satisfaction ( measured by the warr questionnaire ) and directly correlated with the ghq - 12 score , which measures the level of psychological and physical well - being at the time of the study . 
it is recognised that caution is required when dealing with cross - sectional studies , which by definition are unable to provide information regarding causation . however , it appears likely that the experience of difficult evitato in assoluto , ma la sua frequenza pu e deve essere controllata e ridotta [ 17 ]  . 
i dati relativi agli errori medici sono , per considerazioni legate alle modalit di rilevazione degli errori stessi , estremamente aleatori ; nel nostro paese esistono alcune stime , basate sulle segnalazioni dei pazienti , che pongono la radiologia in una situazione comparativamente migliore di altre specialit ( tabella 7 )  . 
la commissione tecnica sul rischio clinico del ministero della salute ha tuttavia dedicato una specifica attenzione al problema dellerrore in radiologia [ 18 ] a testimonianza del rilievo del problema.nella nostra ricerca , i medici intervistati hanno dimostrato di sapere con chiarezza quali possano essere le strategie per la riduzione degli errori radiologici , soprattutto di quelli che reason [ 19 ] classifica come errori latenti , 1078 a . 
while taking great care in interpreting the data , the association of litigation with radiologist age alone and not with other associated variables , such as years of professional experience or hierarchical role in the healthcare system , suggests that ageing and the degenerative conditions associated with it may affect the radiologists ability to interpret radiological findinsiti nellorganizzazione del lavoro : la congruit dei tempi e dei ritmi di lavoro e la disponibilit di risorse umane e strumentali adeguate , sono sicuramente le condizioni che possono favorire una politica di controllo del rischio di errori clinici in radiologia come nelle altre discipline mediche . dal nostro lavoro pare emergere una condivisa e allarmante situazione di disagio per i ritmi di lavoro i tempi insufficienti per la refertazione o per lelaborazione dei piani di cura , la cattiva organizzazione del lavoro , il clima lavorativo non collaborativo o carico di tensioni . 
a ci si aggiunge la carenza di organico , che determina in molti casi limpossibilit di consultare i colleghi per ottenere una seconda opinione , lobsolescenza delle macchine radiologiche , limpossibilit di un sufficiente aggiornamento profes1079 a . 
this is , of course , merely a hypothesis at this stage and would need to be verified on the basis of larger and possibly longitudinal studies . clinical error is often at the origin of malpractice claims , even though there is no biunique correspondence between the two phenomena , such that there may be both serious errors that do not give rise to litigation and litigation not substantiated by errors . it is often claimed that the term malpractice is often inappropriately used , as most legal proceedings against physicians are groundless and are resolved with acquittal . 
in any event , the blame associated with negligence , or alleged negligence , can significantly affect the physician involved . physicians sued for alleged malpractice perceive the proceedings as a threat to their integrity and can react in a dysfunctional fashion [ 20 ]  . 
these ailments can include a sense of isolation , low self - esteem , tension , depression , insomnia and other emotional problems , including anxiety attacks , irritability , frustration , asthenia , a reduction in sexual desire , loss of appetite and apathy . our study confirms that radiologists involved in proceedings for civil or criminal liability present a series of psychological and physical symptoms related to the traumatic event , symptoms that are very similar to those experienced after physical assault and that in some cases can give rise to posttraumatic stress disorder [ f43.1 according to the diagnostic 1080 sionale . 
anche se tali fattori sono indagati con riferimento ad una situazione astratta , intuibile che ciascuno dei radiologi nel rispondere alle domande abbia fatto riferimento soprattutto alla sua propria esperienza professionale . 
a conferma di ci , si osserva che il disagio cos misurato si correla significativamente , e in modo inverso , con la soddisfazione dal lavoro ( misurata dal questionario di warr ) e direttamente con il punteggio del ghq - 12 che misura il livello di malessere psicofisico al momento dellindagine . 
pur con la cautela che si deve osservare in tutte le indagini trasversali , che per definizione non consentono di inferire sulla causalit , suggestiva lipotesi che lesperienza di condizioni lavorative difficili e conflittuali ed il disagio lavorativo che ne consegue , oltre a determinare un aumento degli errori , siano allorigine di una minore soddisfazione dei radiologi e di un eccessivo stress professionale che si traduce in una alterazione dei livelli di benessere psicofisico . tra le possibili cause di errore clinico occorre ricordarne una che , seppure non direttamente indagata nel nostro questionario , ha dimostrato una significativa associazione con loccorrenza di denunce : let anagrafica . 
pur con ogni cautela interpretativa , lassociazione delle denunce solo con let del radiologo e non con grandezze ad essa correlate , come gli anni di esperienza professionale o il ruolo gerarchico nellorganizzazione sanitaria , inducono a formulare lipotesi che linvecchiamento e le condizioni morbose degenerative ad esso associate possano determinare alterazioni a . 
only a minority of respondents indicated the absence of symptoms , and it is difficult to say whether they were subjects particularly resistant to this type of stress or whether they were subjects in whom the process of denial was particularly strong . regardless , our study shows that being sued for alleged malpractice leads to a number of significant changes in ones opinion of the problem and of the measures enacted to protect oneself . 
many physicians who had been sued for alleged malpractice reported a change in their work behaviour , with the adoption of defensive practices that may even lead to refusal of seriously ill patients or patients perceived as dangerous , or to less empathy and at times aversion towards such patients . 
some radiologists in the united states have abandoned certain procetable 6 correlation between work distress ( principal component 1 of causes of error ) , job satisfaction ( warr scale ) and psychological and physical well - being [ general health questionnaire ( ghq ) - 12 ]  . 
correlations with a positive sign ( + ) indicate that one variable increases as another increases , whereas a negative ( ) sign indicates an inverse correlation where high values of one variable are associated with low values of the other disagio ghq - 12 warr pearson correlatino sig . 
in grassetto le correlazioni significative . le correlazioni di segno positivo indicano che una variabile cresce al crescere dellaltra , quelle di segno negativo indicano una correlazione inversa , valori alti di una variabile si associano con valori bassi dellaltra ghq - 12 pearson + 0 , 161 ( * ) disagio coefficiente di correlazione sig . 
si tratta , al momento , solo di unipotesi che dovr essere verificata sulla base di studi di maggiori dimensioni , possibilmente a carattere longitudinale . lerrore clinico spesso allorigine delle denunce per malpractice , anche se tra i due fenomeni non vi corrispondenza biunivoca , potendo esistere sia errori gravi che non danno luogo a denunce , che denunce non sostanziate da errori . da pi parti si sostiene che il termine malpractice usato spesso in modo improprio , giacch la gran parte delle azioni di contenzioso contro i medici sono infondate , e i processi si risolvono con assoluzioni . 
generally speaking , however , in numerous cases , the attention required to follow the proceedings , the lengthy times required to prepare the defence and the constant rumination over the event place the physician in social isolation , which can even disrupt family relations . the cross - sectional nature of our study , which was based on the reporting of consequences to events at times quite remote , did not enable assessment of the effects malpractice stress can have on current health . 
it is nonetheless clear that this specific stress factor is added to the numerous causes of professional strain , many of which are specific to the medical profession , such as coping with the suffering and death of patients and the difficulty in providing a service of constant quality in a system of reduced resources [ 22 ]  . 1082 pria integrit e possono reagire in modo disfunzionale [ 20 ]  . indipendentemente dallesito del confronto giudiziario , il medico pu sperimentare una serie di segni e sintomi , che vanno sotto il nome di sindrome dello stress da malpractice o malpractice stress sindrome ( mss )  . 
tali disturbi comprendono : senso di isolamento , riduzione dellautostima , tensione , depressione , insonnia ed altri disturbi emozionali , a volte attacchi di angoscia , irritabilit , frustrazione , talora astenia , riduzione della libido , inappetenza ed apatia . nella nostra indagine si conferma che i radiologi sottoposti a denunce di responsabilit civile o penale hanno presentano una serie di sintomi psicologici e fisici in relazione con tale evento traumatico , del tutto analoghi e sovrapponibili a quelli che si verificano dopo unaggressione fisica e che possono dare luogo , in alcuni casi , ad un disturbo posttraumatico da stress ( condizione morbosa classificata f43.1 nel dsm - iv - tr ) [ 21 ]  . 
solo una minoranza non riferisce sintomi ma , allo stato , non si pu dire se si tratti di soggetti particolarmente resistenti a tale tipo di stress o di casi in cui il sistema di negazione particolarmente strutturato . comunque si osserva nella nostra ricerca che lessere stati denunciati induce alcuni significativi cambiamenti delle proprie opinioni sul problema della malpractice e sulle misure messe in atto per difendersi da essa . 
molti tra i medici denunciati riferiscono un cambiamento delle proprie abitudini di lavoro , con ladozione di pratiche difensive che talora giungono al rifiuto di pazienti particolarmente gravi o percepiti come pericolosi o una ridotta empatia e talora avversione verso taluni pazienti . 
negli stati uniti stato osservato che alcuni tendono ad abbandonare determinate procedure , sulle quali hanno minore controllo o che ritengono possano esporli maggiormente a contenzioso : il caso , ad esempio , della mammografia [ 3 , 5 ]  . 
fortunatamente , nella maggior parte dei casi la controversia che ha dato luogo alla denuncia pu essere risolta in sede extragiudiziale , o non passa il vaglio delle indagini preliminari . 
ma in generale , in non pochi casi lattenzione posta al processo , i lunghi tempi necessari per organizzare la difesa e la ruminazione sullaccaduto pongono il medico in una situazione di isolamento sociale che pu talora giungere a turbare anche le relazioni familiari . il carattere trasversale del nostro studio , basato sul recupero anamnestico delle conseguenze di eventi talora remoti , non consente di valutare il rilievo che lo stress da malpractice esplica sullo stato di salute attuale . 
tuttavia evidente che questo specifico fattore di stress si aggiunge alle molteplici cause di tensione o strain professionale , molte delle quali specifiche della professione medica , come il confronto con le sofferenze e la morte dei pazienti e le difficolt nel fornire un servizio di qualit costante in un contesto di riduzione delle risorse [ 22 ]  . poich la possibilit di confrontarsi efficacemente con tale tipo di stress discende direttamente dal grado di consapea . 
however , it does appear that radiologists hold little faith in the techniques of clinical risk management and are not fully aware of the need for informed consent and the relative legal implications . 
such training would need to begin at university and be followed up in specialty courses , where ideally each physician would be made aware of the problems related to clinical error and the procedures aimed at minimising and managing it . 
similarly desirable would be a commitment to continuing education , possibly to be organised and carried out with the assistance of scientific and professional associations , to enable radiologists and radiotherapists to compare their experiences and , through such comparison , improve their own abilities for limiting error and its consequences . note : data regarding the opinions of radiotherapists were partially communicated at the xvi national congress a.i.r.o. , associazione italiana radioterapia oncologica . 
malpractice in radiation oncology : the physicians experience volezza del problema e dal possesso delle corrette tecniche di controllo , occorre domandarsi se i radiologi italiani siano culturalmente attrezzati per controllare le problematiche dellerrore diagnostico e lo stress da malpractice . in base ai dati forniti da questa indagine possibile dire che i radiologi italiani hanno una sufficiente conoscenza del tema delle controversie legali e dei fattori che possono determinare un aumento della frequenza degli errori medici . non sembra per che essi credano alla efficacia delle tecniche del clinical risk management , n che siano pienamente consapevoli della necessit del consenso informato e della relativa giurisprudenza . 
tale formazione dovrebbe essere iniziata nelluniversit e segnatamente nei corsi di specializzazione , nei quali sarebbe auspicabile che ciascun medico fosse messo a conoscenza delle problematiche legate allerrore clinico e delle procedure tendenti a minimizzarlo e gestirlo . sarebbe poi opportuno un impegno di aggiornamento permanente , da operarsi eventualmente con il concorso delle societ scientifiche e degli ordini professionali , per consentire agli specialisti radiologi e radioterapisti di confrontare le proprie esperienze e migliorare in questo confronto la propria capacit di controllo sullerrore e sulle sue conseguenze . i dati relativi alle opinioni dei radioterapisti sono stati parzialmente comunicati al xvi congresso nazionale a.i.r.o. , associazione italiana radioterapia oncologica , lecce , 21 - 24 ottobre 2006 . 
particularly interesting in view of the expected future developments is the section on contrast - enhanced sonography for the study of tumour neoangiogenesis . the second chapter is devoted to the examination technique and basic sonographic semiotics . 
of great value to radiologists in training , the chapter is intended as a necessary step to allow readers to fully understand the clinical issues discussed in chapter three . the third chapter is the heart of the book . 
as a result , this chapter truly meets the needs of ultrasound radiologists who are faced with a whole range of oncological issues in their daily clinical practice . the fourth chapter deals with ultrasound - guided interventional procedures in oncology . 
one section is given over to the description , complete with technical details , of diagnostic procedures such as fine - needle aspiration or biopsy of superficial and deep lesions , and the positioning of drains . 
the final section focuses on the use of ultrasound to assess and monitor lesions after treatment . in conclusion , this book is a complete , exhaustive and easy - toread textbook on ultrasound in oncology . lopera in volume singolo si propone come un aggiornato , completo ed esauriente testo - atlante di ecografia focalizzato sulle applicazioni cliniche della metodica in campo oncologico . la capacit di sintesi degli autori permette di ritrovare nelle 395 pagine di questo libro la trattazione di tutte quelle problematiche che , nella pratica clinica , il medico ecografista si trova ad affrontare in campo oncologico sia con intenti diagnostici che terapeutici . il libro articolato in quattro capitoli . il primo capitolo presenta le possibilit della moderna ecografia in oncologia . 
particolarmente interessante per gli attesi sviluppi futuri il paragrafo dedicato in questo capitolo allo studio della neoangiogenesi tumorale con impiego di mezzi di contrasto in ecografia . il secondo capitolo dedicato alla metodologia dindagine e alla semeiotica ecografica elementare . 
questo capitolo rappresenta un passaggio obbligato , voluto dagli autori , per poter comprendere appieno le problematiche cliniche successivamente trattate nel capitolo tre . il terzo capitolo dunque il cuore del libro . 
il capitolo quindi realmente capace di soddisfare le richieste del medico ecografista per fronteggiare le svariate problematiche cliniche oncologiche della pratica clinica quotidiana . il quarto capitolo tratta le procedure interventistiche ecoguidate in campo oncologico . 
viene dedicato spazio , con particolari di tecnica , alle procedure diagnostiche quali lagoaspirazione o la biopsia di lesioni superficiali e profonde nonch al posizionamento di drenaggi . vengono quindi descritte le possibilit di guida ecografica di procedure di trattamento delle lesioni epatiche quali la alcolizzazione e la termoablazione . 
mollet1 1dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , holland 2dipartimento di radiologia e di cardiologia , azienda ospedaliero - universitaria di parma , viale rustici , 2 , i - 43100 parma , italy 3dipartimento di radiologia , universit degli studi di verona , italy 4unit di riabilitazione cardiovascolare , fondazione don gnocchi onlus , parma , italy 5dibimel , sezione di scienze radiologiche , universit di palermo , palmermo , italy 6dipartimento di cardiologia , ospedale versilia , lido di camaiore viareggio , viareggio , italy correspondence to : f . 
we studied 72 patients ( 38 men , 34 women , mean age 53.98.0 years ) with atypical or typical chest pain and stratified in the lowto intermediate risk category . msct - ca ( sensation 64 cardiac , siemens , germany ) was performed after iv administration of 100 ml of iodinated contrast material ( iomeprol 400 mgi / ml , bracco , italy )  . 
msct - ca scored 15 false positives on a per - segment base , which affected only marginally the per - patient performance ( only one false positive )  . 
we concluded that 64 - slice ct - ca is a diagnostic modality with high sensitivity and negative predictive value in patients at low to intermediate risk . key words multislice computed tomography ct coronary angiography conventional coronary angiography coronary artery disease 64 - slice ct low cardiovascular risk riassunto obiettivo . 
sono stati studiati 72 pazienti ( 38 maschi , 34 donne , et media 53 , 98 , 0 anni ) che presentavano dolore toracico atipico o angina pectoris stabile e che venivano stratificati nella categoria del rischio basso - intermedio . 
sensibilit , specificit , valore predittivo positivo e negativo dellac - tc nella determinazione delle stenosi significative utilizzando unanalisi per segmenti sono risultate , rispettivamente , del 100% , 98 , 6% , 71 , 2% e 100% . 
this is related to the fact that validation studies have been performed on candidates for conventional coronary angiography ( cag ) and therefore on patients with typical symptoms , a high risk level and a positive exercise tests . 
the recent guidelines on stable angina of the european society of cardiology have added ct to the diagnostic algorithm and , with a low level of evidence ( iib ) , suggest that the technique be used in patients with low to intermediate risk and with doubtful stress test results or inability to undergo stress testing [ 18 ]  . very few studies have investigated the diagnostic performance of msct - ca in patients at low to intermediate risk [ 19 ]  . 
the aim of this study was to evaluate the diagnostic accuracy of 64 - slice msct - ca for detecting significant stenoses in a population of patients at low to intermediate risk . materials and methods patient population between march 2005 and march 2006 , we recruited 72 patients ( 38 men , 34 women , mean age 53.98.0 years ) with a low or intermediate cardiovascular risk atypical chest pain ( 26 / 72 ; 36.1% ) or exertional angina ( 46 / 72 ; 63.9% ) , and positive , doubtful or inconclusive stress electrocardiogram ( ecg ) who were scheduled for cag to determine the presence and extent of coronary disease . 
only patients with sinus rhythm , those who had never undergone percutaneous angioplasty or surgical by - pass grafting and those who were able to hold their breath for at least 12 s were included in the study . 
our institutions ethics committee approved the study protocol , and all patients provided their informed consent . patients with a heart rate ( hr ) above 65 bpm were administered , if no contraindications were present , a single oral dose patient preparation langiografia coronarica ( ac ) con tomografia computerizzata ( tc ) spirale multistrato ( ac - tc ) una nuova modalit diagnostica per la rilevazione delle stenosi coronariche significative ( riduzione del calibro del lume > 50% ) [ 17 ]  . lelevata sensibilit e valore predittivo negativo costituiscono uno dei dati pi coerenti nella recente letteratura di questa metodica [ 317 ]  . 
le recenti linee guida della societ europea di cardiologia sullangina stabile introducono la tc nellalgoritmo diagnostico e con un livello basso di evidenza ( iib ) suggeriscono che la tc possa essere utilizzata nei pazienti a rischio basso - intermedio nei quali i test provocativi siano dubbi o non eseguibili [ 18 ]  . 
scopo dello studio di valutare laccuratezza diagnostica della ac - tc a 64 strati nella a rilevazione di stenosi significative in una popolazione di pazienti a rischio basso - intermedio . materiali e metodi popolazione studiata dal marzo 2005 al marzo 2006 , sono stati arruolati 72 pazienti ( 38 maschi , 34 femmine , et media 53 , 98 , 0 anni ) con rischio cardiovascolare basso o intermedio , con dolore toracico atipico ( 26 / 72 ; 36 , 1% ) o angina da sforzo ( 46 / 72 ; 63 , 9% ) , e ecg da stress positivo / dubbio / inconclusivo , programmati per lesecuzione di unangiografia coronarica convenzionale allo scopo di determinare la presenza e lestensione della malattia coronarica . 
solo i pazienti con ritmo sinusale , mai sottoposti ad angioplastica percutanea o ad intervento chirurgico per il posizionamento di by - pass e capaci di trattenere il respiro per almeno 12 secondi , sono stati inclusi nello studio . 
i pazienti nei quali esistevano delle controindicazione assolute alla somministrazione endovenosa di mezzo di contrasto iodato ( ad esempio , allergia nota , insufficienza renale o disordini tiroidei ) sono stati esclusi dallo studio . 
a few minutes before the scan , patients received sublingual isosorbide dinitrate ( carvasin 5 mg , wyeth lederle )  . scan protocol and image reconstruction the ct study was performed with a 64 - slice scanner ( sensation 64 , siemens , forchheim , germany )  . 
images were reconstructed with the following parameters : effective slice thickness 3 mm , reconstruction increment 1.5 mm , field of view ( fov ) 150180 mm , dedicated convolution filter for the calcium score . 
 dedicated software ( windose , medical physics institute , erlangen , germany ) was used to calculate the radiation dose delivered during the angiographic scan ( mean value 15.2 msv for women and 21.4 msv for men )  . 
patients were administered 100 ml of iodinated contrast material ( iomeprol , iomeron 400 , bracco , milan ) at a rate of 5 ml / s via an automatic injector ( stellant , medrad , pittsburgh , pa , usa ) connected to a 20 - gauge needle cannula previously positioned in an antecubital vein [ 5 ]  . to optimise opacification of the coronary arteries , the bolus - tracking technique ( care bolus , siemens , forchheim , germany ) was used to synchronise the arrival of the contrast agent in the coronaries with the beginning of the scan [ 5 , 20 ]  . 
the temporal windows used were midand end diastolic ( from 300 to 450 ms before the following r wave and / or from 60% to 70% of the r - r interval )  . 
ai pazienti con una frequenza cardiaca superiore a 75 bpm stata somministrata per via orale una dose addizionale di 1 mg di lorazepam ( temesta , wyeth - ayerst )  . 
pochi minuti prima della scansione stato somministrato isosorbide dinitrato sublinguale ( carvasin 5 mg , wyeth lederle )  . protocollo di scansione e ricostruzione delle immagini per lo studio mediante tc stato utilizzato uno scanner a 64 strati ( sensation 64 , siemens , forchheim , germania )  . 
le immagini sono state ricostruite con i seguenti parametri : spessore di strato effettivo 3 mm , incremento di ricostruzione 1 , 5 mm , campo di vista ( fov ) 150180 mm , filtro di convoluzione dedicato per il calcium score . 
non stata utilizzata la modulazione prospettica dellamperaggio al fine di non compromettere leventuale necessit di eseguire ricostruzioni con finestra temporale posizionata in fase tele - sistolica . utilizzando un software dedicato ( windose , istituto di fisica medica , erlangen , germania ) stata calcolata la dose di radiazioni ionizzanti alla quale i pazienti sono stati esposti durante la scansione angiografica ( valore medio 15 , 2 msv per le donne e 21 , 4 msv per gli uomini )  . 
la tecnologia con doppia macchia focale oscillante sullasse z ( flying focal spot ) permette di sovra - campionare due volte per ogni posizione angolare del tubo radiogeno le 32 file di detettori dello spessore minimo di 0 , 6 mquesta geometria di scansione consente di ottenere unimmagine con voxel isotropico di 0 , 4 mm3 . 
the reconstruction algorithm applied acquires the data during a single heartbeat obtained during half a rotation of the x - ray tube . quantitative coronary angiography ( cag ) cag was performed within 2 weeks of the msct - ca study . 
a single observer , unaware of the msct - ca results , identified the coronary segments by using a 17 - segment classification modified from that provided by the american heart association ( aha ) [ 21 ]  . 
all segments , regardless of diameter , were included in the comparison with msct - ca . segments were classed as nonsignificantly stenotic ( normal or with wall irregularities or with < 50% lumen reduction ) or significantly stenotic ( 50% lumen reduction )  . 
cases of disagreement between the two observers were resolved by consensus . image quality was assessed on each segment and classified as good ( no motion artefacts or severe calcification ) , adequate ( presence of artefacts degrading the image but not preventing evaluation with an acceptable level of diagnostic confidence ) or poor ( artefacts allowing image evaluation with low diagnostic confidence )  . statistical analysis the diagnostic performance of msct - ca for detecting significant atherosclerotic coronary lesions , using cag as the reference standard , is reported below in terms of sensitivity , specificity and positive and negative predictive value , with 95% confidence intervals ( cis ) calculated using binomial expansion . 
i dati della scansione angiografica sono stati ottenuti durante una singola acquisizione della durata di 12 , 20 , 9 s . sono state effettuate delle ricostruzioni retrospettive basate sul segnale ecg per ottenere una qualit dellimmagine priva di artefatti da movimento . 
le finestre temporali utilizzate sono state la fase mesoe tele - diastolica ( da 300 a 450 ms prima della successiva onda r e / o dal 60% al 70% dellintervallo r - r )  . 
quando ritenuto necessario ( ad esempio , in caso di persistente movimento cardiaco residuo che riduce la qualit diagnostica dellimmagine ) sono state analizzate altre ricostruzioni in differenti finestre temporali di ricostruzioni del ciclo cardiaco , generalmente dal 25% al 35% dellintervallo r - r ( oppure + 225 ms , + 275 ms , e + 325 ms dopo la precedente onda r )  . 
lalgoritmo di ricostruzione utilizzato preleva i dati derivanti da un singolo battito cardiaco ottenuto durante met rotazione del tubo radiogeno . angiografia coronarica quantitativa ( cag ) la cag stata eseguita entro 2 settimane dallac - tc . 
un singolo osservatore , non a conoscenza dei risultati dellactc , ha identificato i segmenti coronarici utilizzando una classificazione in 17 segmenti modificata da quella fornita dallamerican heart association [ 21 ]  . 
i segmenti sono stati classificati come non significativamente stenotici ( normali o con irregolarit della parete o con riduzione del diametro luminale < 50% ) o significativamente stenotici ( riduzione del lume coronarico 50% )  . le stenosi coronariche sono state quantificate in due proiezioni ortogonali utilizzando un algoritmo di misurazione validato per langiografia coronarica ( caas , pie medical , maastricht , olanda )  . valutazione dellimmagine di ac - tc tutte le scansioni sono state analizzate indipendentemente da due osservatori , che non erano a conoscenza dei risultati dellangiografia coronarica convenzionale . 
most patients with at least one stenosis > 50% ( 13 / 71 , 18% ) had single - vessel disease . table 2 shows the additional data provided by msct . coronary calcium scores according to agatston were very low ( 47.790.4 ) , reflecting the low disease prevalence in the study population and the low coronary disease burden . 
oral - blockers ( used in over 90% patients ) before the examination were effective in reducing mean hr by approximately 10 bpm ( from approximately 70 bpm to 60 bpm during the angiographic scan )  . interobserver variability , expressed as a k - value , for detecting significant lesions was 0.98 ( corresponding to excellent on a semiquantitative scale )  . 
image quality on a per - segment basis was classified as good in 98.5% of cases , moderate in 1.2% and poor in 0.4%. a total of 1 , 098 segments were included in the comparison with cag . 
la maggior parte dei pazienti con almeno una stenosi > 50% ( 13 / 71 ; 18% ) erano mono - vasali . in tabella 2 vengono riportate multiple informazioni ulteriori ricavate dalla tc . 
il calcium score coronarico secondo agatston risultato molto basso ( 47 , 790 , 4 ) , rispecchiando la bassa prevalenza di malattia nella popolazione ed il basso carico di malattia coronarica . 
leffetto della terapia beta - bloccante orale ( utilizzata in oltre il 90% dei pazienti ) prima dellesame si dimostrato efficace nel ridurre in media di circa 10 bpm la frequenza cardiaca media ( da circa 70 bpm a circa 60 bpm durante la scansione angiografica )  . le variabilit inter - osservatore , espressa come valori di k , per lindividuazione delle lesioni significative risultata 0 , 98 ( corrispondente a ottima su una scala semi - quantitativa )  . 
la qualit delle immagini su base segmentale stata classificata come buona nel 98 , 5% , moderata nel 1 , 2% e bassa nel 0 , 4% . sono stati inclusi per il confronto con langiografia coronarica convenzionale 1098 segmenti . 
il numero di falsi positivi ha un impatto particolarmente evidente nella valutazione per segmento ( n = 15 ) e per vaso ( n da 2 a 5 eccetto che per il tronco comune ) , mentre nella valutazione per paziente ( n = 1 ) non si evidenzia particolarmente . se la ac - tc fosse stata utilizzata come gate - keeper per langiografia coronarica , sarebbe stata indotta una cag in un paziente che non avrebbe poi dimostrato stenosi significative , mentre tutti i pazienti con stenosi sarebbero correttamente stati inviati alla cag ( tabella 4 )  . 
nessun paziente con malattia coronarica significativa sarebbe erroneamente stato classificato come senza stenosi coronariche significative . discussione lac - tc con apparecchiature di ultima generazione ( 64 strati ) permette una valutazione dellintero albero coronarico ( vasi principali e loro rami collaterali e marginali ) [ 317 ]  . 
gli studi di validazione condotti fino a questo momento si sono focalizzati su popolazioni di pazienti ad elevata probabilit pre - test di malattia coronarica ( range 50%80% circa )  . 
no patient with significant coronary disease would have been misclassified as not having significant coronary stenoses . discussion msct - ca with the latest - generation scanners ( 64 slice ) allows evaluation of the entire coronary tree ( main vessels and their collateral and marginal branches ) [ 317 ]  . 
infatti , sia nelle recenti linee guida della societ europea di cardiologia [ 18 ] , sia in un recente documento di consenso sullappropriatezza delle indicazioni della cardio - tc e cardio - rm [ 22 ] , viene suggerito che un utilizzo congruo della metodica sarebbe nei casi in cui il paziente sia a rischio basso - intermedio ed i test provocativi siano dubbi , non fattibili o inconclusivi . questa popolazione non stata ancora studiata approfonditamente nella letteratura nota se non in una esperienza di nikolaou et al . 
the sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) are expressed as percentages , followed by 95% confidence intervals ( cis ) calculated with binomal expansion in parentheses . tp , true positive ; tn , true negative ; fp , false positive ; fn , false negative ; rca , right coronary artery ; lmt , left main trunk ; lad , left anterior descending artery ; lcx , left circumflex artery tabella 3 valori di accuratezza diagnostica della tc a 64 strati 1045 sensibilit specificit il criterio di valutazione la stenosi coronarica significativa che corrisponde ad una riduzione del lume 50% . 
i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) , sono espressi in percentuale seguiti da parentesi con gli intervalli di confidenza del 95% calcolati con espansione binomiale . vp , veri positivi ; vn , veri negativi ; fp , falsi positivi ; fn , falsi negativi ; acd , arteria coronaria destra ; tcs , tronco comune sinistro ; ada , arteria coronaria discendente anteriore ; acx , arteria coronaria circonflessa f . 
il diagramma mostra come i pazienti si sono distribuiti sulla base delle informazioni diagnostiche della coronarografia tc ( ac - tc )  . i pazienti con ac - tc negativa sono poi risultati tutti negativi alla coronarografia convenzionale . 
both the recent guidelines of the european society of cardiology [ 18 ] and a recent consensus statement on the appropriateness criteria for cardiac ct and cardiac magnetic resonance imaging ( mri ) [ 22 ] suggest that appropriate use of msct - ca would be in cases of patients at low to intermediate risk and doubtful , unfeasible or inconclusive stress tests . 
rimane comunque preservato anche in questo lavoro lelevato valore predittivo negativo [ 19 ]  . nel nostro studio esistono diversi elementi di innovazione . il primo riguarda la tecnologia a 64 strati non precedentemente decritta in questo campo di applicazione clinica . 
however , this study focusing on a low - risk population had the problem that , although a reasonable number of patients were enrolled ( n = 72 ) , the 6.9% disease prevalence ( number of positive cases = 5 ) did not make it possible to transfer the results into clinical practice ( very wide cis ) [ 19 ]  . 
lalbero coronarico risultato esplorabile in toto in tutti i pazienti ed i falsi positivi sono stati tutti generati in pazienti con maggiore carico di malattia dove altre lesioni significative ( > 50% ) erano gi presenti . 
sections obtained orthogonally to the vessel axis in the planes shown in c ( 1 , 2 and 3 ) show the portion above the stenosis , the stenosis , and the portion below the stenosis . 
le sezioni ortogonali allasse del vaso effettuate sui piani indicati in c ( 1 , 2 e 3 ) indicano in tratto a monte , la stenosi , ed il tratto a valle della lesione . 
the entire coronary tree was assessable in all patients , and false positive results all occurred in patients with a greater disease burden , where other significant lesions ( > 50% ) were already present . false positive results had a particularly evident impact in the evaluation per segment and per vessel but not in the evaluation per patient . 
this is explained by the fact that most false positive results occurred in patients with a greater disease burden who already had other significant stenoses located in other coronary segments ( that is , in the seven patients with multivessel disease , equal to 10% of the total population )  . calcifications did not produce excessive artefacts in the population studied , whose calcium score was generally low ( lower mean age and more female patients compared with other studies )  . 
this , together with the relatively low prevalence of disease , is likely to account for the optimal results achieved in the per - segment , per - vessel and per - patient evaluation . 
in fact , in our population , only five significant lesions were present in the distal segments ( according to the coronary segmental classification aha : 4 - 8 - 9 - 10 - 14 - 15 )  . 
this explanation is also suple calcificazioni non sono state motivo di eccessivi artefatti nella popolazione studiata che era caratterizzata da un basso calcium score globale ( et media pi bassa i altri studi e popolazione femminile molto pi rappresentata )  . 
la malattia nei vasi distali molto pi probabile nei pazienti ad alto rischio ed in particolare nei diabetici ( che sono stati esclusi dalla nostra popolazione )  . infatti , nella nostra popolazione solo 5 lesioni significative erano presenti nei segmenti distali ( secondo la classificazione dei segmenti coronarici aha : 4 - 8 - 9 - 10 - 14 - 15 )  . 
questa spiegazione sostenuta anche dalla elevatissima concordanza tra gli osservatori , sostenuta dalla bassa prevalenza di malattia ( vedi anche valore medio di calcium score )  . come valore aggiunto della ac - tc abbiamo voluto includere la valutazione dei parametri volumetrici del ventricolo sinistro estrapolati contestualmente allesame angiografico . 
however , this reduces the systems flexibility in the image reconstruction phase , as it is no longer possible to use end - systolic reconstructions , which in many cases are diagnostically decisive ( in our population , the operators found it necessary to also use the systolic phase in 54% of cases , which in 7% of cases was recognised as the principal reconstruction phase )  . the use of - blockers may be considered a limitation , even though it is still not clear how many patients have to be excluded from msct - ca in clinical practice because of contraindications to the administration of - blockers combined with impossibility of administering other negative chronotropic agents . 
patients with an initial heart rate above 70 bpm received a dose of - blockers before the scan , which allowed mean hr to be lowered to 60.6 bp future improvements in temporal resolution will progressively reduce the need for b - blockers . 
reports have already been published on the use of dual - source ct systems , characterised by a temporal resolution of 83 ms [ 3436 ]  . ottenere una ragionevole prevalenza di malattia ed una realistica rappresentazione della pratica clinica abbiamo dovuto includere pazienti a rischio basso - intermedio con ecg stress dubbio - inconclusivo , ma anche quelli con test provocativo positivo . 
in aggiunta , questa costituisce la popolazione nella quale , essendo la probabilit di malattia bassa , i test provocativi hanno una performance ridotta [ 30 , 31 ]  . 
inoltre , la presenza di sintomi tipici o atipici non un fattore condizionante la mortalit dei pazienti sottoposti a stress ecg [ 32 ]  . la dose di radiazioni stimata durante lac - tc ( 15 , 221 , 4 msv ) superiore a quella di una cag . 
lesposizione a radiazioni ionizzanti pu essere ridotta utilizzando la modulazione prospettica della corrente del tubo radiogeno [ 33 ]  . tuttavia , in questo modo , si riduce la flessibilit del sistema in fase di ricostruzione delle immagini . 
non pi possibile infatti utilizzare a fase tele - sistolica di ricostruzione che in molti casi pu risultare dirimente dal punto di vista diagnostico ( nella nostra popolazione stato necessario secondo gli operatori utilizzare anche la fase sistolica nel 54% dei casi e nel 7% dei casi la fase sistolica era riconosciuta come la fase principale di ricostruzione )  . lutilizzo di - bloccanti pu essere considerato una limitazione anche se ad oggi non stato chiarito quanti siano nella pratica clinica i pazienti che devono essere esclusi dalla scansione mediante ac - tc sulla base del criterio della contro - indicazione alla somministrazione dei - bloccanti concomitante alla impossibilit di somministrare altri farmaci cronotropi negativi . 
i pazienti con una frequenza cardiaca iniziale al di sopra di 60 bpm hanno ricevuto una dose di - bloccanti prima della scansione che ha permesso di ridurre la frequenza cardiaca media a 60 , 6 bpi miglioramenti futuri in termini di risoluzione temporale renderanno progressivamente meno necessario lutilizzo di betabloccanti . 
in questo campo siamo gi a conoscenza di esperienze mediante apparecchiature a doppia sorgente caratterizzate da risoluzione temporale in hardware di 83 ms [ 3436 ]  . conclusioni conclusions noninvasive 64 - slice msct - ca is a technique with a high diagnostic accuracy in the detection of significant coronary stenoses in patients with atypical pain or stable angina and low to intermediate risk . 
given the low disease prevalence in this population , msct - ca may become an ideal screening tool to exclude the presence of critical coronary disease and avoid the use of cag in a subset of patients . lac - tc non invasiva a 64 strati una tecnica ad elevata accuratezza diagnostica nellidentificazione delle stenosi coronariche significative in pazienti con dolore atipico o angina stabile con rischio basso - intermedio . 
am j cardiol 98 : 145148 16 garcia mj , lessick j , hoffmann mh ( 2006 ) accuracy of 16 - row multidetector computed tomography for the assessment of coronary artery stenosis . 
ropers d , rixe j , anders k et al ( 2006 ) usefulness of multidetector row spiral computed tomography with 64x 0.6mm collimation and 330 - ms rotation for the noninvasive detection of significant coronary artery stenoses . 
fox k , garcia ma , ardissino d et al ( 2006 ) guidelines on the management of stable angina pectoris : executive summary : the task force on the management of stable angina pectoris of the european society of cardiology . eur heart j 27 : 13411381 19 . 
nikolaou k , rist c , wintersperger bj et al ( 2006 ) clinical value of mdct in the diagnosis of coronary artery disease in patients with a low pretest likelihood of significant disease . 
cademartiri f , nieman k , van der lugt a et al ( 2004 ) intravenous contrast material administration at 16 - detector row helical ct coronary angiography : test bolus versus bolus - tracking technique . 
austen wg , edwards je , frye rl et al ( 1975 ) a reporting system on patients evaluated for coronary artery disease . report of the ad hoc committee for grading of coronary artery disease , council on cardiovascular surgery , american heart association . 
hendel rc , patel mr , kramer cm et al ( 2006 ) accf / acr / scct / scmr / asnc / nasci / scai / sir 2006 appropriateness criteria for cardiac computed tomography and cardiac magnetic resonance imaging : a report of the american college of cardiology foundation quality strategic directions committee appropriateness criteria working group , american college of radiology , society of cardiovascular computed tomography , society for cardiovascular magnetic resonance , american society of nuclear cardiology , north american society for cardiac imaging , society for cardiovascular angiography and interventions , and society of interventional radiology . 
juergens ku , grude m , fallenberg em et al ( 2002 ) using ecg - gated multidetector ct to evaluate global left ventricular myocardial function in patients with coronary artery disease . ajr am j roentgenol 179 : 15451550 24 . 
juergens ku , grude m , maintz d et al ( 2004 ) multi - detector row ct of left ventricular function with dedicated analysis software versus mr imaging : initial experience . 
schuijf jd , bax jj , jukema jw et al ( 2004 ) noninvasive angiography and assessment of left ventricular function using multislice computed tomography in patients with type 2 diabetes . diabetes care 27 : 29052910 26 . 
heuschmid m , rothfuss jk , schroeder s et al ( 2005 ) assessment of left ventricular myocardial function using 16 - slice multidetector - row computed tomography : comparison with magnetic resonance imaging and echocardiography . 
salm lp , schuijf jd , de roos a et al ( 2006 ) global and regional left ventricular function assessment with 16detector row ct : comparison with echocardiography and cardiovascular magnetic resonance . 
torricelli1 1cattedra e servizio di radiologia i , dipartimento integrato dei servizi diagnostici e per immagini , 2cattedra e servizio di cardiologia , dipartimento integrato emergenza urgenza , universit degli studi di modena e reggio emilia , azienda ospedaliero - universitaria policlinico di modena , via del pozzo 71 , i - 41100 modena , italy correspondence to : g . 
the gadolinium - enhanced images were evaluated using a segmental model with two different methods : a visual score on a 5 - point scale ( 0 no hyperenhancement , 4 hyperenhancement > 76% of myocardial wall ) and a quantitative analysis based on the manual tracing of infarct contours with automatic threshold analysis . 
le immagini post - gadolinio sono state valutate utilizzando un modello segmentale con 2 metodi : uno score visuale con scala a 5 punti ( 0 = assenza di enhancement , 4 = enhancement > 76% della parete ) ed unanalisi quantitativa disegnando manualmente larea dellinfarto con correzione automatica dei contorni . 
dei 1280 segmenti , 322 ( 25 , 1% ) presentavano contrattilit alterata con enhancement in 327 ( 25 , 5% ) valutati visivamente e in 414 ( 32 , 3% ) quantitativamente . 
tra i segmenti con normale o lieve ipocinesia l89 , 2% aveva uno score di enhancement 1 , mentre l80 , 2% dei segmenti discinetici o acinetici aveva uno score 3 . 
lanalisi visuale del delayed enhancement un approccio pi rapido e sufficiente per definire lestensione transmurale dellinfarto ; inoltre ha unalta correlazione con la disfunzione contrattile . parole chiave imaging risonanza magnetica infarto miocardio mezzi di contrasto disfunzione ventricolare g . 
in acute infarction , contrast washin and wash - out kinetics as well as altered integrity of myocyte and sarcolemmal membranes may play an important role [ 4 ]  . 
in the setting of chronic infarction , the areas of scarring and fibrosis alter the kinetic behaviour and distribution of gadolinium as the extracellular space increases [ 5 ]  . 
estimating viability and scar tissue is important for guiding treatment in patients with ischaemic heart disease , and the correlation between myocardial injury and hyperenhancement on cemri is very close [ 6 ]  . 
furthermore , ce - mri is also useful in assessing the transmural extent of infarction , information often needed by the cardiologist to decide whether or not the patient will benefit from revascularisation . 
as the first method may be less accurate and the latter may be time consuming , the aim of our study was to demonstrate the feasibility of visual analysis compared with quantitative evaluation . 
exclusion criteria were recent ( < 1 month ) myocardial infarction , arrhythmias and general contraindications to mri ( e.g. , pacemakers , intracranial clips , claustrophobia )  . all patients gave written informed consent to participate in the study , and the local ethics committee approved the study protocol . 
 study protocol the study protocol included a cine - mri study at rest in three planes ( two chambers , four chambers and multiple short axes ) to analyse regional and global left ventricular function , followed by ce - mri to evaluate the presence of infarction . all images were acquired using a five - element synergy coil during breath - holds and were gated to the electrocardiogra noto che la risonanza magnetica con contrasto ( cemri ) permette una precisa delineazione dellestensione e della transmuralit dellinfarto miocardico con una elevata risoluzione spaziale . 
il meccanismo dellenhancement miocardico nella sede dellinfarto duplice , sia legato alla rottura delle membrane dei miociti che permette la diffusione del contrasto paramagnetico a base di gadolinio nello spazio intracellulare , sia per espansione dello spazio interstiziale per deposizione di collagene [ 13 ]  . 
nellinfarto acuto le cinetiche di wash - in e wash - out del mezzo di contrasto come anche lalterata integrit delle membrane dei miociti e del sarcolemma , giocano un ruolo importante [ 4 ]  . in sede di infarto cronico le aree di cicatrice e fibrosi portano ad una modificazione del comportamento di cinesi e di distribuzione del gadolinio allaumentare dello spazio intracellulare [ 5 ]  . 
stimare la presenza di tessuto vitale e necrotico importante e necessario per guidare il follow - up dei pazienti con cardiopatia ischemica ; la correlazione tra danno miocardico e iper - enhancement tissutale alta [ 6 ]  . 
inoltre , la cemri utile nel valutare la transmuralit dellinfarto , che rappresenta una informazione necessaria al cardiologo per impostare la terapia e selezionare i pazienti che trarrebbero beneficio da eventuale rivascolarizzazione . lanalisi delle immagini ottenute con sequenze di cemri pu essere effettuata visivamente o quantitativamente [ 79 ] e , dato che il primo metodo potrebbe risultare meno accurato ed il secondo pi laborioso , lo scopo del nostro studio di dimostrare la fattibilit della valutazione visuale rispetto a quella quantitativa . 
oltre a ci , abbiamo correlato il grado di iper - enhancement con le alterazioni contrattili a riposo . materiali e metodi popolazione abbiamo valutato 80 pazienti ( et media di 63 , 18 anni , 76 , 4% maschi ) , con nota cardiopatia ischemica cronica e precedente infarto ( almeno 1 mese prima dello studio )  . 
i criteri di esclusione erano : infarto miocardico recente ( < 1 mese ) , aritmie e controindicazioni generali allesecuzione di risonanza magnetica ( come presenza di pace - maker , clips intracraniche , claustrofobia )  . il consenso informato stato ottenuto da tutti i pazienti arruolati nello studio . 
i pazienti sono stati sottoposti a risonanza magnetica cardiaca 1 , 5 tesla ( philips intera , best , olanda )  . protocollo di studio il protocollo di studio include lo studio funzionale di risog . 
depending on the size of the heart , 1012 cine short - axis views were obtained from apex to base with a bffe sequence during breath - holds of approximately 15 s . 
delayed - enhancement images were acquired approximately 15 min after administration of intravenous contrast material [ 0.1 mmol / kg , gadoliniumtetraazacyclododecane tetraacetic acid ( dota ) , dotarem ] with a t1 - weighted turbo fast low - angle shot sensitivity - encoded sequence with a segmented 180 inversion recovery preparatory pulse . 
the inversion time ( ti ) that permits complete suppression of normal myocardium signal was individually adapted and typically ranged from 260 ms to 320 ms . the optimum ti to null healthy myocardium and highlight the evidence of infarcted tissue , where gadolinium accumulates , was found by using a series of real - time images obtained in the same plane with variable inversion time ( look - locker sequences )  . 
each segment was assigned a wall - motion score : 0 = normokinesia ; 1 = mild hypokinesia ; 2 = severe hypokinesia ; 3 = akinesia ; 4 = dyskinesia . global function was evaluated by outlining endocardial and epicardial borders manually on the short - axis images with cardiac software ( cardiac analysis , viewforum 4.1 , philips , nl )  . 
left ventricle ( lv ) end - systolic and end - diastolic volumes and ejection fraction were calculated . to visually quantify infarct size on the delayed - enhancement mr images , each segment was assigned a visual score on a 5 - point scale ( 0 = no hyperenhancement , 1 = hyperenhancement 1%25% of lv wall thickness , 2 = hyperenhancement 26%50% of lv wall thickness , 3 = hyperenhancement 51%75% of lv wall thickness , 4 = hyperenhancement > 76% of lv wall thickness )  . quantitative analysis involved manually tracing the lv endocardial and epicardial borders and placing two regions of interest ( rois ) : one at the centre of the infarction area , and the other at the centre of normokinetic healthy myocardiuscar tissue is then automatically delineated based on a threshold signal intensity ( si ) derived from the mean intensity of infarcted and normal myocardiu the threshold was considered to be ( si of infarction + si of normal myocardium ) / 2 . 
therefore , myocardium exhibiting a higher signanza magnetica a riposo su tre i piani cardiaci ( due camere , quattro camere e multipli assi corti ) per analizzare la funzione ventricolare regionale e globale ( cine - mri ) , seguito da lo studio con contrasto ( cemri ) per valutare la presenza di infarto . 
tutte le immagini sono state acquisite con il mantenimento dellapnea e sincronizzazione cardiaca utilizzando una bobina synergy a 5 canali . la cinesi ventricolare sinistra stata valutata utilizzando sequenze bilanciate fast field echo ( b - ffe ) sui tre piani : due camere , quattro camere e asse corto del cuore . 
le immagini tardive di delayed enhancement sono state acquisite circa 15 minuti dopo somministrazione di contrasto endovenoso ( 0 , 1 mmol / kg , gadolinium - dota , dotarem ) utilizzando una sequenza t1 pesata turbo gradient echo con un impulso di inversione preparatorio di 180 . 
lottimale ti per annullare il segnale del miocardio normale ed evidenziare il segnale del tessuto infartuato , dove il gadolinio si accumula , stato selezionato utilizzando una serie di immagini ottenute in tempo reale su uno stesso piano con tempi di inversione variabili ( sequenza look - locker )  . 
i parametri applicati per la sequenza ir - ge sono stati i seguenti : tr / te 4 , 4 / 1 , 32 ms , fa 15 , ti 260320 ms , sense 2 , fattore tfe 14 , spir soppressione del grasso , matrice 256 , spessore di fetta 8 analisi dei dati la funzione regionale e globale del ventricolo sinistro stata valutata sulle immagini di cine - mri secondo il modello segmentale a 16 segmenti derivato da quello a 17 segmenti di cerqueira [ 10 ] , ottenendo 1280 segmenti ( 16 segmenti per 80 pazienti )  . 
ad ogni segmento stato attribuito uno score di cinesi definito come wall motion score ( wms ) variabile da 0 = normocinesi , 1 = ipocinesia lieve , 2 = severa ipocinesia , 3 = acinesia , 4 = discinesia . la funzione globale stata ottenuta delineando i bordi endocardici ed epicardici sulle immagini in asse corto utilizzando un software dedicato cardiaco ( cardiac analysis , viewforum 4.1 , philips , olanda )  . 
per quantificare visivamente lentit dellinfarto sulle immagini di cemri stato assegnato ad ogni segmento un punteggio visuale in base a una scala da 5 punti variabile da : 0 = asg . 
in both the qualitative and quantitative approaches , areas of persistent microvascular obstruction were considered part of the infarction and were included manually in the enhanced region in the quantitative approach . delayed - enhancement images were scored visually by two radiologists with different experience ( one board - certified radiologist and one resident radiologist )  . 
cardiac medical therapy was continued during the study and consisted of angiotensin - converting enzyme ( ace ) inhibitors in 62 patients and beta - blockers in 68 . cardiac mri analysis mean lv ejection fraction was 49.314.9%. 
among segments with normal or mild hypokinesia , 89.2% had a delayed enhancement score 1 , whereas 80.2% of akinetic or dyskinetic segments had a score 3 , confirming the relationship between transmurality of infarction and contractile impairment ( table 1 )  . there was almost perfect agreement between the visual senza di iper - enhancement , 1 = iper - enhancement 1%25% dello spessore ventricolare sinistro , 2 = iper - enhancement 26%50% dello spessore ventricolare sinistro , 3 = iperenhancement 51%75% dello spessore ventricolare sinistro , 4 = iper - enhancement > 76% dello spessore ventricolare sinistro . lanalisi quantitativa stata basata sulla delineazione manuale dei contorni endocardici ed epicardici del ventricolo sinistro e successivamente sono state posizionate due regioni di interesse ( roi ) : una nel centro del miocardio infartuato e una nel centro di miocardio sano normocinetico . 
da ci , segue la delineazione automatica del tessuto infartuato sulla base di un valore di intensit di segnale ( si ) soglia derivante dalla media delle intensit del tessuto infartuato e normale . 
ci consegue che il miocardio che presenta un valore di intensit seriore al valore soglia considerato infartuato . il software permette di ottenere anche grafici ad occhio di bue , di facile lettura nel valutare la transmuralit dellinfarto . 
le aree di ostruzione microvascolare persistente sono state considerate in entrambi gli approcci come parte della zona infartuata ed incluse manualmente nella zona di enhancement durante la valutazione quantitativa . le immagini di delayed enhancement sono state esaminate due radiologi con differente esperienza ( un medico radiologo esperto e un medico radiologo in formazione ) ; per calcolare la variabilit inter - osservatore dellapproccio visuale sono stati considerati 20 pazienti . 
la variabilit intraosservatore stata calcolata sui medesimi 20 pazienti che sono stati rivalutati dal medico radiologo esperto dopo un mese . valutazione statistica la valutazione statistica stata effettuata ( software stata ) considerando la valutazione quantitativa come gold standard : le concordanze tra lanalisi visuale e quantitativa dellinfarto e tra lo score di cinesi segmentale e lanalisi visuale dellinfarto sono state calcolate usando il valore  . 
un valore di p < 0 , 05 stato considerato statisticamente significativo . risultati popolazione dei pazienti la popolazione in studio era composta da 80 pazienti consecutivi , la maggior parte dei quali maschi ( 76 , 4% ) , con unet media di 63 , 18 anni . 
there was a moderate but statistically significant correlation between the visual scar score and the segmental wall - motion score , the value being 0.58 , with se 0.025 and p < 0.01. among normal or mild hypokinetic segments ( score : 01 ) , 89.2% had a visual score 1 , and among dyskinetic or akinetic segments ( score : 34 ) , 80.2% had a visual score 3 ( tables 3 and 4 )  . 
interand intraobserver agreement of the visual score were both excellent : 89% and 94% , respectively . discussion cardiac ce - mri is now considered the gold standard in zima convertitore dellangiotensina in 62 pazienti e betabloccanti in 68 pazienti ; essa non stata interrotta durante lo studio . analisi di risonanza magnetica cardiaca la frazione di eiezione media era di 49 , 314 , 9% . 
tra i segmenti con cinesi normale o lieve ipocinesi , l89 , 2% presentava uno score 1 , mentre 80 , 2% dei segmenti acinetici o discinetici presentava uno score3 , confermando la relazione tra la transmuralit dellinfarto e la disfunzione contrattile ( tabella 1 )  . si riscontrata una pressoch perfetta concordanza tra il metodo visuale e quantitativo con un valore di 0 , 92 con errore standard ( se ) di 0 , 023 e p < 0 , 01 ( tabella 2 ) ; lanalisi visuale ha sottostimato 104 ( 8 , 1% ) e sovrastimato 19 ( 1 , 5% ) segmenti . 
inoltre stata trovata una correlazione moderata ma statisticamente significativa , tra lo score visuale e lo score di motilit segmentale con valori di 0 , 58 con se di 0 , 025 e p < 0 , 01 . 
tra i segmenti con cinesi normale o lievemente depressa ( score : 01 ) , l89 , 2% ha score visuale 1 e tra i segmenti discinetici o acinetici ( score : 34 ) , l80 , 2% ha score visuale 3 ( tabelle 3 , 4 )  . 
le concordanze interad intra - osservatore dello score visuale erano entrambe eccellenti : 89% e 94% rispettivamente . discussione la risonanza magnetica cardiaca con contrasto attualmente considerata il gold standard per la definizione della presenza di infarto miocardico e ci dovuto alla sua alta capacit di visualizzare il tessuto necrotico dopo somministrazione di gadolinio . 
numerosi studi hanno confermato alta concordanza tra la distribuzione di gadolinio e lestensione dellinfarto valutato mediante analisi istologica , suggerendo che larea di miocardio che presenta enhancement costituita da tessuto cicatriziale [ 4 ]  . lestensione dellinfarto , come evidenziato da cerm , cosiderata uno dei fattori prognostici principali da valutare nei pazienti con cardiopatia ischemica , in quanto si correla direttamente al rimodellamento ventricolare sinistro . 
per definire precisamente quanto del tessuto cardiaco danneggiato , i metodi quantitativi proposti in letteratura sono molteplici e variano a seconda del software di post - processing impiegato . lestensione del tessuto cicatriziale e la sua distribuzione transmurale sono fattori prognostici importanti , dato che un g . 
many different studies have confirmed the close correlation between gadolinium distribution and extent of infarction as assessed by histological examination , suggesting that what hyperenhances in delayed - enhancement imaging is scar tissue [ 4 ]  . 
infarction extent , as depicted by ce - mri , is now considered one of the main prognostic factors in patients with ischaemic heart disease , as it correlates directly with left ventricular remodelling . 
many quantitative methods , depending on the scanners and postprocessing software used , have been proposed in the literature to define precisely how much heart tissue is infarcted . the extent of scar tissue and its transmural distribution are important prognostic factors , given that a large infarct but with circumferential distribution can cause less contractile dysfunction than one that is small but transmural . 
moreover , it is well known that in dysfunctional segments , the likelihood of improvement in regional contractility after revascularisation decreases progressively as the transmural infarto esteso ma con una distribuzione circonferenziale pu causare una disfunzione contrattile minore di un infarto di minore estensione longitudinale , ma transmurale . 
inoltre riconosciuto che nei segmenti con alterazione della cinesi , la probabilit di miglioramento contrattile post - rivascolarizzazione diminuisce progressivamente con laumentare dellestensione transmurale della zona di iper - enhancement [ 11 ]  . i nostri risultati mostrano che la valutazione visuale del tessuto cicatriziale correla molto bene con quella quantitativa , considerando sia i segmenti interessati sia la loro corrispondente transmuralit . 
oltre a ci , lanalisi visuale ha alta concordanza sia interche intra - osservatore , quindi pu essere considerata un approccio altamente riproducibile per definire in modo semplice e rapido lestensione e la transmuralit dellinfarto . tuttavia , bisogna riconoscere che il metodo quantitativo permette di ottenere lesatta quantificazione dellinfarto esprimendo tale dato come percentuale o come grammi di tessuto danneggiato rispetto al miocardio sano , in modo tag . 
the visual score may therefore be considered a timesaving and reproducible approach to easily define infarct extent and transmurality . however , it must be noted that the quantitative method provides exact quantification of infarction in terms of percentage or grams of damaged tissue with respect to normal myocardium , allowing one to infer the amount of healthy myocardium , which is another important parameter in defining prognosis . 
our software permits us to define a threshold intensity of scar tissue based on the different intensities of normal and hyperenhanced myocardium , so that damaged tissue can be automatically defined and quantified . 
it does not , however , have the recently reported postprocessing correction algorithms , such as the feature analysis and comle da poter dedurre lentit di tessuto normale , che risulta essere un altro importante parametro per definire la prognosi di tali pazienti . 
il software impiegato nel presente studio consente di fissare un valore soglia basandosi sulla differenza di intensit di segnale tra tessuto infartuato e miocardio remoto ; tale approccio consente di definire e quantificare automaticamente il tessuto danneggiato . 
nonostante ci , questo software non possiede gli algoritmi di correzione recentemente riportati in letteratura , come lalgoritmo di feature analysis and combined thresholding ( fact ) [ 8 , 9 ] , che , proposto su animali e in una piccola coorte di pazienti , permette di escludere gli errori di volume parziale , di segmentazione imperfetta e gli errori di calcolo automatico dovuti per esempio alla presenza di aree di ostruzione microvascolare nel contesto dellarea infartuata . tutto ci sottolinea la necessit di nuovi algoritmi che siano facilmente utilizzabili e che quantifichino accuratamente la presenza di infarto nelle immagini ottenute per lo studio del delayed enhancement , dato che questa tecnica la metodica non invasiva con pi alta risoluzione total totale g . 
this highlights a need for new , easy - touse algorithms that can accurately quantify the extent of infarction on delayed - enhancement imaging , a noninvasive technique providing the highest spatial resolution currently available for the assessment of viability . the software algorithm employed in our study allowed us to identify , in a few cases , subendocardial infarction that had been visually underestimated . 
moreover , it better defined the limits between score 3 and 4 transmural extent that , although not affecting prognosis if taken alone , can in fact change the final evaluation and patient management when integrated with the other clinical and functional parameters . 
 not surprisingly , there was good agreement between the visual scar score and wall - motion score , as segments with little or no infarction had no contractile impairment , whereas segments with infarct transmurality > 50% had variable contractile dysfunction . 
the less - than - excellent concordance ( index 0.57 ) may be due to a direct or reverse tethering effect of the adjacent healthy myocardium . we can conclude that visual analysis of delayed enhancement is a timesaving approach that is adequate for assessing infarct extent and transmurality and that has a close correlation with wall - motion abnormalities . 
quantification of scar tissue may also be important in patients with intermediate transmurality , who should be referred for coronary angioplasty to improve the viable but stunned or hibernated myocardiua work in progress is to determine the amount of scar tissue before and after coronary revascularisation to assess possible shrinkage of infarction with respect to healthy myocardium . our study demonstrated that the qualitative approach is sufficient in routine clinical practice . 
however , another application could be to use both methods to evaluate infarct size before and after drug therapy in order to further validate the visual analysis approach in an experimental setting . 
further studies are needed above all to compare the amount of scar tissue before and after revascularisation to evaluate whether there is effective improvement due to infarct shrinkage or whether the exact quantity of damaged tissue is predictive of future response to revascularisation . spaziale attualmente disponibile per valutare la vitalit tissutale . lalgoritmo utilizzato dal nostro software ha permesso di identificare in alcuni casi la presenza di infarto sub - endocardico , che visivamente era stato sottostimato ; inoltre ha definito meglio i limiti tra estensione transmurale con score 3 e 4 che da sola non influenza la prognosi del paziente ma che integrata con gli altri parametri clinici e funzionali , pu modificare la valutazione finale ed il trattamento del paziente . naturalmente , abbiamo riscontrato una buona concordanza tra lo score visuale e lo score di cinesi , dato che segmenti senza infarto o con una piccola quantit di danno miocardico non presentavano disfunzione contrattile , mentre segmenti con una transmuralit infartuale maggiore del 50% mostravano gradi variabili di alterazione della cinesi . la concordanza non eccellente ( indice di 0 , 57 ) potrebbe essere dovuta alleffetto di trascinamento diretto e / o inverso del miocardio sano adiacente . possiamo concludere che lanalisi visuale del delayed enhancement un approccio meno laborioso e sufficiente per valutare la transmuralit e lestensione spaziale dellinfarto ; inoltre ha una notevole correlazione con le alterazioni contrattili . 
la quantificazione del tessuto cicatriziale potrebbe essere importante in pazienti con una transmuralit intermedia che dovrebbero essere indirizzati verso una procedura invasiva mediante coronarografia tradizionale per migliorare il miocardio vitale , ma stordito od ibernato . 
una studio in corso di calcolare la quantit di tessuto danneggiato prima e dopo rivascolarizzazione coronarica in modo tale da valutare una eventuale diminuzione dellinfarto rispetto al corrispondente tessuto miocardico sano . il significato di questo studio che lapproccio qualitativo risulta essere sufficiente nella routine clinica , ma certo in campo di ricerca unaltra applicazione potrebbe essere di valutare le dimensioni infartuati prima e dopo terapia farmacologia con entrambi i metodi , per validare anche in campo sperimentale lanalisi visuale . 
midiri2 , 5 1dipartimento di radiologia e dipartimento cuore , imaging cardiovascolare non invasivo , azienda ospedaliera di parma , via gramsci 14 , i - 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , holland 3istituto di radiologia , universit degli studi di verona , verona , italy 4istituto di radiologia , ospedale universitario cattinara , trieste , italy 5dibimel , sezione di scienze radiologiche , universit di palermo , palermo , italy correspondence to : f . 
six hundred and seventy patients undergoing msct - ca with 16 - slice and 64 - slice ct scanners for suspected atherosclerotic disease of the coronary arteries were retrospectively reviewed . 
a significant number of noncardiac findings might have been missed in msct - ca scans ; the appropriate approach should be as a team trained in cardiology and radiology . key words multislice ct coronary angiography collateral findings incidental findings riassunto obiettivo . 
sono stati riscontrati 1234 rilievi accessori , divisi in 332 ( 26 , 9% ) non significativi , 821 ( 66 , 53% ) significativi e 81 ( 6 , 56% ) in obbligo di ulteriori accertamenti . 
lapproccio appropriato dovrebbe prevedere la lettura degli esami da parte di un team esperto in cardiologia e radiologia . parole chiave angiografia coronarica mediante tc multistrato reperti collaterali reperti incidentali f . 
noninvasive vascular imaging represents an important clinical application , as multislice ct coronary angiography ( msct - ca ) has proven to be a reliable alternative to conventional digital subtraction angiography [ 25 ]  . 
these technical advances permit a reliable study of coronary arteries to quantify calcium deposits among coronary plaques [ 6 ] and to detect significant stenosis [ 7 , 8 ] , anatomical variants of the anatomy of the coronaries [ 9 ] and functional evaluation of the heart [ 10 ]  . 
consequently , msct - ca has shown to be the technique of choice in patients with lowto intermediate risk of acute chest pain [ 11 ]  . msct - ca appears to be an excellent tool for improving diagnostic accuracy in patients with chest pain and moderate pretest probability of coronary artery disease ( cad ) and negative or equivocal findings on exercise stress testing . 
on the other hand , the wide availability of these scanners has led to a constant increase of these studies , with the emerging problem of extracardiac collateral findings revealed during msct - ca . 
sometimes these findings are of primary importance for the patients health and reaching a correct diagnosis . the aim of this study was to further investigate this aspect of msct - ca through the analysis of collateral findings . materials and methods patient population six hundred and seventy consecutive patients ( 380 men and 290 women , mean age 59.710.2 years ) undergoing msctca due to suspected cad between january 2004 and january 2005 were retrospectively studied in a single - centre study . 
four hundred and forty - six examinations were performed using a 16 - slice ct scanner ( sensation 16 , siemens , forchheim , germany ) and 224 with a 64 - slice scanner ( sensation 64 , siemens , forchheim , germany )  . inclusion and exclusion criteria inclusion criteria for the msct - ca examination were regular heart rate < 65 beats per minute ( bpm ) and ability of the patient to hold the breath for 20 s ( 16 - slice scanner only )  . exclusion criteria were refusal to provide informed consent , prior adverse reactions to iodinated contrast material , kidney failure ( serum creatinine > 120 mmol / l ) , possible pregnancy , impaired respiratory function , unstable clinical condition or marked heart failure , prior coronary angioplasty or coronary surgery and nondiagnostic examination quality . 
the local ethics committee approved the study , and all patients provided informed consent . la tecnologia multistrato tc ha permesso lapplicazione della tomografia computerizzata per lo studio del cuore e delle arterie coronarie [ 1 ]  . 
lo sviluppo di apparecchiature a 16 e 64 strati permette attualmente lo studio del cuore in tempo ridotto e con un aumento sostanziale in termini di risoluzione temporale e spaziale . 
queste evoluzioni tecnologiche permettono uno studio affidabile dellalbero coronarico per la quantificazione dei depositi di calcio a livello delle placche coronariche [ 6 ] , per la ricerca di stenosi significative [ 7 , 8 ] , varianti anatomiche [ 9 ] e addirittura per lo studio funzionale del cuore [ 10 ]  . 
conseguentemente , la ac - tcms ha dimostrato di essere la tecnica di prima scelta nei pazienti con dolore toracio acuto e profilo a basso - intermedio rischio [ 11 ]  . 
la ac - tcms sembra essere uneccellente metodica per migliorare laccuratezza diagnostica nei pazienti con dolore toracico , moderata probabilit pretest di coronaropatia e rilievi negativi o dubbi nei vari stress test . 
daltra parte la larga disponibilit odierna di queste apparecchiature ha portato ad un aumento costante degli esami effettuati , facendo emergere il problema di reperti collaterali dimostrati durante questi esami . 
alle volte tali rilievi possono essere di importanza primaria per la salute del paziente e permettono un corretto inquadramento diagnostico . quindi lo scopo del nostro studio consiste nellapprofondire questo aspetto della tc delle coronarie attraverso lanalisi dei reperti collaterali osservati . materiali e metodi popolazione di studio sono stati valutati retrospettivamente mediante uno studio monocentrico 670 pazienti consecutivi ( 380 maschi e 290 femmine , et media 59 , 710 , 2 anni ) sottoposti a ac - tcms per sospetta patologia delle coronarie nel periodo compreso tra gennaio 2004 e gennaio 2005 . 
quattrocentoquarantasei di tali indagini sono state eseguite mediante apparecchiatura tc a 16 strati ( sensation 16 , siemens , forchheim , germania ) , e 224 con tc a 64 strati ( sensation 64 , siemens , forchheim , germania )  . criteri di inclusione ed esclusione i criteri di inclusione per gli esami ac - tcms erano costituiti da un ritmo cardiaco < 65 battiti / minuto ( bpm ) e la capacit di trattenere lapnea inspiratoria per 20 s ( solamente per apparecchiatura 16 - strati )  . 
i criteri di esclusione erano rappresentati da : rifiuto al consenso informato per lo studio , precedenti reazioni avverse al mezzo di contrasto iodato , insufficienza cardiaca , ( creatininemia > 120 mmol / l ) , gravidanza , insufficiente funzionalit respiratoria , condizioni clif . 
patients were scanned in the supine position during breath hold from the level of the pulmonary arteries through the very cranial part of the abdomen in order to visualise the base of the heart . 
in patients with a known coronary artery bypass graft , the scan was extended cranially from the level of the aortic arch through the base of the heart . scan protocol we intravenously administered 80100 ml of nonionic iodinated contrast material ( iomeprol 400 mg / ml , iomeron , bracco , milan , italy ) at a flow rate of 45 ml / s , followed by 40 ml of saline solution at the same rate . 
the contrast material was administered with a dual - syringe automatic injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an 18 - gauge cannula placed in an antecubital vescan synchronisation with contrast material passage was performed with the bolus tracking technique ( care bolus , siemens , forchheim , germany ) [ 2 ]  . 
scan and reconstruction parameters for the 16and 64 - slice scanners are summarised in table 1 . data processing a retrospective electrocardiogram ( ecg ) - gated technique was used for image reconstruction . 
data sets were reconstructed during the mid - to - end diastolic phase , with reconstruction windows set at 300 ms to 450 ms before the next r wave or 60%70% of the rr interval . 
if mildly irregular heart rates were encountered , such as bundle branch blocks or premature beats , the temporal variability in the reconstruction phase was compensated for manually with ecg editing . 
inaccurate detection of the r waves was corrected , and temporal windows applied to premature beats were deleted , filling the next diastolic interval with one or more temporal windows to avoid data gaps . the reconstructed slice thickness was 0.75 mm , with a reconstruction increment of 0.4 mall ct data sets were filtered with a medium - soft convolution kernel . in addition , images were reconstructed with 1 - mm thickness and reconstruction increment of 0.6 mm , with an axial field of view ( fov ) collimated to the patients chest using standard mediastinal window ( 350 w / 50 c ) and lung window ( 1 , 400 w / 600 c ) levels to evaluate soft tissue and lung parenchyma . image evaluation all scans were reviewed by two radiologists ; data sets obtained with a large fov were reviewed in mediastinal and lung windows . 
il comitato etico locale ha approvato lo studio e tutti i pazienti esaminati hanno fornito il consenso informato . preparazione del paziente per i pazienti studiati con apparecchio a 16 e 64 strati in caso di frequenze cardiache uguali o superiori a 65 bpm , sono stati somministrati 100 mg di metoprololo unora prima dellesecuzione dellesame . 
i pazienti sono stati studiati in posizione supina in apnea inspiratoria dal livello delle arterie polmonari fino alla porzione prossimale delladdome in modo tale da comprendere anche la base del cuore . 
in pazienti con bypass il limite della scansione stato innalzato cranialmente alla porzione iniziale dellarco aortico fino alla base del cuore . protocollo di scansione abbiamo somministrato per via endovenosa 80100 ml di mezzo di contrasto non ionico iodato ( iomeprol 400 mgl / ml , iomeron , bracco , milano , italia ) con un flusso di 45 ml / s , seguito da 40 ml di soluzione salina allo stesso flusso . 
il mezzo di contrasto stato introdotto tramite un iniettore automatico a doppia pompa ( stellant , medrad , pittsburgh , pa , usa ) connesso ad una vena antecubitale connessa con un agocannula da 18 g . 
la sincronizzazione della scansione con il passaggio del mezzo di contrasto stata eseguita mediante la tecnica del bolus tracking ( care bolus , siemens , forchheim , germania ) [ 2 ]  . 
i parametri di acquisizione e di ricostruzione per gli apparecchi a 16 e 64 - strati sono riassunti in tabella 1 . elaborazione dei dati per la ricostruzione delle immagini stata utilizzata una tecnica retrospettica ecg - gated . 
i pacchetti di dati sono stati ricostruiti durante la fase meso / tele - diastolica , con finestre di ricostruzione da 300 ms fino a 450 ms dalla successiva onda r o 60% fino a 70% dellintervallo r - r . 
in caso di qualit delle immagini non sufficiente sono state eseguite ricostruzioni aggiuntive durante la fase tele - sistolica ( 25% fino a 35% dellintervallo r - r )  . 
la ricerca non accurata delle onde r stata corretta e le finestre temporali applicate ai battiti ectopici sono state eliminate , compensando il successivo intervallo diastolico con uno o pi finestre . 
the clinical importance of noncardiac findings was divided into three categories : minor ( no clinical meaning ; not necessary to report ) , mild ( uncertain clinical meaning ; preferably mentioned in the report ) , major ( compulsory to be further investigated ; mandatory to report )  . 
among significant - disease patients , medical records were reviewed to check the clinical followup , subsequent examinations or surgical procedures of noncardiac abnormalities in the 6 months after msct - ca . 
the clinical statistics results in aggiunta , le immagini sono state ricostruite con uno spessore di fetta di 1 mm e un incremento di ricostruzione di 0 , 6 mm con un campo di vista assiale collimato al torace del paziente utilizzando le finestre mediastiniche ( 350 w / 50 c ) e polmonari ( 1400 w / 600 c ) per valutare i tessuti molli ed il parenchima . valutazione delle immagini tutte le scansioni sono state analizzate da 2 radiologi . 
limportanza clinica dei reperti collaterali non cardiaci stata distinta in 3 categorie : minori ( senza significato clinico ; senza necessit di essere segnalato ) , intermedio ( significato clinico incerto ; preferibilmente menzionato nel referto ) , maggiore ( necessari ulteriori accertamenti , indispensabile la segnalazione sul referto )  . 
i pazienti con malattie importanti sono stati tenuti in follow - up alla ricerca di ulteriori accertamenti , o procedure chirurgiche nei 6 mesi successivi alla angiografia coronarica mediante tcms . tabella 1 parametri di scansione nella angiografia coronarica tc : 16 strati e 64 strati f . 
among a total of 1 , 234 findings , 417 ( 33.79% ) were detected in the lungs , 665 ( 53.88% ) and in the mediastinum , 74.13% of which were mediastinal lymph nodes ( table 3 )  . findings were then subdivided into three main categories : minor , mild and major . 
among the 1 , 234 additional findings recorded , 81 patients ( 12.08% ) revealed major findings , 439 ( 65.5% ) had mild findings and 12 ( 1.8% ) had only minor findings . 
in the other case , msct - ca permitted incidental diagnosis of multiple lytic lesions located at the body and peduncles of two thoracic vertebrae in a 66 - year - old man with suspected atherosclerotic disease who underwent a 16slice msct - ca . 
le frequenza dei sintomi , fattori di rischio , e qualsiasi reperto collaterale osservato sono state espresse in valori assoluti e percentuali . risultati tra i 670 esami effettuati , l85% ha dimostrato malattie delle arterie coronarie . 
given that the msct scans were done to detect atherosclerotic disease as part of various research protocols , it is remarkable that accidental pathological changes in organs and structures , which were not the target organs of the examination , were found almost in every patient . 
tra 1234 reperti addizionali riscontrati , 81 pazienti ( 12 , 08% ) hanno dimostrato reperti maggiori , 439 ( 65 , 5% ) avevano reperti intermedi e 12 ( 1 , 8% ) avevano solo reperti minori . 
the three categories identified were : minor ( no clinical meaning ; not necessary to report ) , mild ( uncertain clinical meaning ; preferably mentioned in the report ) , major ( compulsory to be further investigated ; mandatory to report ) svc , superior vena cava ; r , right ; l , left dental extracoronary findings in msct - ca , the detection of malignant disease in one case and the possibility of justifying dyspnoea and properly treat the patient in the other case , emphasise the importance of accurate and complete reading of the investigation [ 12 ]  . there is very little in the literature about the prevalence of noncardiac abnormalities in cardiac ct studies [ 1315 ]  . 
the higher prevalence of lesion in our study is mainly due to a very systematic and accurate analysis of all kind of possible abnormalities within the scan range ; for this reason , only 138 ( 20.6% ) patients were completely without any additional finding . 
se consideriamo solamente i reperti maggiori riportiamo una prevalenza del 45 , 6% . gli esami tc del cuore vengono eseguiti con una frequenza in costante aumento nei vari paesi come metodi di f . 
le tre categorie identificate sono : minori ( senza significato clinico , senza necessit di essere segnalato ) , intermedio ( significato clinico incerto ; preferibilmente menzionato nel referto ) , maggiore ( necessari ulteriori accertamenti , indispensabile la segnalazione sul referto ) vcs , vena cava superiore ; d , destra ; s , sinistra malignant disease were revealed . 
the authors reviewed the scans done with a fov of 350 mm , never imaging the entire chest , and thus the most lateral parts of the lungs could not have been investigated in some patients . 
dato che gli esami tc sono stati eseguiti per ricercare malattie aterosclerotiche come parte di vari protocolli di ricerca , un fatto considerevole che sono stai riscontrati reperti accessori in quasi tutti i pazienti . 
tale percentuale cos elevata di rilievi addizionali , il riconoscimento di patologia maligna in un caso e la possibilit di giustificare la dispnea e quindi trattare appropriatamente il paziente nellaltro caso , enfatizza limportanza di una lettura accurata e completa dellindagine [ 12 ]  . in letteratura corrente vi sono pochissimi lavori circa la prevalenza di anomalie non cardiache in studi cardiaci f . 
of 1 , 812 consecutive patients undergoing ebct cardiac studies , the authors reviewed only the mediastinal windows but also encountered cardiac findings such as mitral valve or pericardiac pathologies . 
moreover , abnormalities found in that study were a large number of minor , relatively insignificant , abnormalities , such as scars , granulomas , atelectasis , degenerative arthritis and rib fractures . 
la prevalenza maggiore di lesioni nel nostro studio soprattutto dovuta ad unanalisi molto accurata e sistematica di tutte le possibili anomalie allinterno del range di scansione ; per tale ragione solo 138 ( 20 , 6% ) pazienti si sono dimostrati completamente senza malattia . 
nel suo studio , onuma ha descritto che il 22 , 7% dei pazienti aveva un reperto non significativo che necessitava un lavoro addizionale e sono stati riscontrati solo 4 casi ( 0 , 8% ) di patologia neoplastica maligna . 
gli autori hanno revisionato le scansioni effettuate con un campo di vista di 350 mm , mai comprendente lintero torace , e quindi le porzioni pi laterali dei polmoni in alcuni pazienti non sono state studiate , asserendo che non necessario ricoprire lintero torace in quanto rappresenta un lavoro in pi . 
noi abbiamo analizzato lintera sezione toracica acquisita e ricostruita in modo specifico processato a partire dai dati grezzi , fatto che rappresenta effettivamente un lavoro aggiuntivo per loperatore , ma pu rivelare una grande quantit di reperti aggiuntivi medi e maggiori che altrimenti non sarebbero scoperti . un altro lavoro significativo stato pubblicato da hunold et al . 
in 1812 pazienti consecutivi sottoposti a ebct studi del cuore , gli autori hanno revisionato solamente le finestre mediastiniche , ma hanno annoverato nella casistica anche reperti cardiaci come la presenza di valvole mitraliche o patologie pericardiche . 
inoltre le anomalie incluse nel loro studio comprendevano un elevato numero di reperti minori relativamente privi di significato pratico come cicatrici , granulomi , atelettasie , artriti degenerative o esiti di fratture costali . 
nel nostro studio abbiamo descritto anche lesioni minori che rappresentano 332 su 2198 , 15 , 1% di tutte le lesioni descritte . come gi notato da onuma , hunold nel suo lavoro non ha revisionato le finestre polmonari e perci il numero effettivo di noduli polmonari presenti nei pazienti esaminati sconosciuto . 
2a , b vertebral metastases : incidental finding of multiple lytic lesions located at the body and peduncles of two thoracic vertebrae ( arrows in a and b ) in a 66 - year - old man with suspected atherosclerotic disease who underwent a 16 - slice computed tomography coronary angiography . 
diagnosi accidentale di multiple lesioni litiche localizzate al corpo e peduncoli di due vertebre toraciche ( frecce in a e b ) in un maschio di 66 anni con sospetta coronaropatia sottoposto a ac - tcms . 
in our study , we discovered seven patients with pulmonary nodules > 1 cm , two with lung cancer and two with lung metastasis , but these pathologies were already known and in follow - up . although in clinical practice , it has been proposed that msct - ca may be interpreted by cardiologists who evaluate only the heart and the coronaries [ 18 ]  . 
this practice should be discouraged on the basis of our large series of cases , as the prevalence of extracardiac findings is extremely high so that they will need further investigation . in some cases , the operator may keep the fov as small as possible to include the heart only . 
for this reason , if the operator looks at the coronaries only , some part of the radiation dose given to the patient is wasted , eliminating the opportunity , as our results confirm , to find what might be important additional findings . how ethical it is to ignore or overlook these anatomical regions is a controversy based on a turf battle . 
in addition , the patients interest should always be preserved , and any finding regarding his / her health should be reported . con noduli polmonari superiori ad 1 cm di cui 2 con neoplasia al polmone e 2 pazienti con metastasi polmonari ( questa patologie erano gi note e in follow - up )  . sebbene nella pratica clinica sia stato proposto che la tc cuore potrebbe essere interpretata solamente da cardiologi per la valutazione dellalbero coronario [ 18 ] , questo approccio dovrebbe essere scoraggiato sulla base della nostra casistica dal momento che la prevalenza di reperti extra cardiaci risulta estremamente elevata e parecchie volte necessita di ulteriori indagini . in alcuni casi loperatore potrebbe tenere il campo di vista il pi stretto possibile in modo da includere solamente il cuore . 
tale approccio corretto nellintento della visualizzazione del solo albero coronarico , comunque le informazioni disponibili per lo studio delle aree periferiche al cuore esistono e sono contenute nei dati grezzi . 
per tale ragione se loperatore si concentra solo sulle coronarie , una parte della dose somministrata al paziente viene sprecata , annullando lopportunit , come i nostri risultati confermano , di scoprire eventuali reperti aggiuntivi . 
riteniamo che allapice dellinteresse vi sia la salute del paziente e qualsiasi reperto che riguardi la sua salute sia da riportare nel referto . conclusions conclusioni in conclusion , a significant number of noncardiac findings can be detected in msct - ca scans . 
we studied 120 patients with suspected small - bowel disease by 16 - slice mdct after oral administration of a polyethylene glycol solution ( n = 56 ) or methylcellulose via a nasojejunal tube ( n = 64 )  . 
fifteen patients were found to be affected by small - bowel neoplasm ( six had non - hodgkins lymphoma , three had carcinoid tumour , two had peutz - jeghers syndrome , two had adenocarcinoma , two had melanoma metastases , one had lipoma )  . in the remaining patients , 58 cases of crohns disease and seven miscellaneous diseases were detected . 
mdct performed after bowel - loop distension with low - density contrast material and iv administration of iodinated contrast agent is a reliable method for diagnosing and staging small - bowel neoplasms . key words neoplasms small bowel enteroclysis multidetector - ct riassunto obiettivo . 
sono stati studiati 120 pazienti con sospetta patologia tenuale mediante tc multidetettore ( 16 strati ) previa somministrazione di polietilenglicole per via orale ( n = 56 ) o di metilcellulosa attraverso sondino naso - digiunale ( n = 64 )  . 
lesame tc stato eseguito prima e durante infusione di 130 ml di mdc iodato con flusso di 3 ml / s ed inizio delle scansioni dopo 40 secondi dallinizio della somministrazione . 
quindici pazienti sono risultati affetti da neoplasia dellintestino tenue ( 6 pazienti con linfoma non hodgking , 3 con carcinoide , 2 con sindrome di peutz jeghers , 2 con adenocarcinoma , 1 con metastasi da melanoma e 1 con lipoma )  . in 58 pazienti la diagnosi era di morbo di crohn , in 7 pazienti erano presenti patologie varie . 
la tc multidetettore effettuata previa distensione delle anse con mdc ipodenso ed infusione ev di mdc iodato una metodica utile nella diagnosi e stadiazione delle neoplasie tenuali . parole chiave neoplasie intestino tenue enteroclisi tc multidetettore introduction introduzione primary tumours of the small bowel account for only 5% of all gastrointestinal tumours , and this is quite surprising considering the length , extensive surface and structural diversity of the small intestine . 
 le neoplasie primitive dellintestino tenue rappresentano solo il 5% di tutti i tumori gastrointestinali e questa unevenienza sorprendente se consideriamo la notevole lunghezza del tenue , la sua vasta superficie e la diversit degli elementi strutturali . 
an interesting , though not very recent , study analysed data of all patients with a diagnosis of malignancy of the small bowel over 21 years [ 1 ] , evaluating time from symptom onset to the first medical contact and the time from medical contact to diagnosis . 
the authors demonstrated that the average delay in diagnosis attributable to the patient was less than 2 months , the delay attributable to the physician not ordering the appropriate diagnostic test was 8.2 months , and that attributable to the radiologist failing to make the diagnosis was 12 months . 
as a consequence , the greatest delay in diagnosis occurred after the patient had sought medical help and was the result of incorrect radiological interpretations or false - negative results . three quarters of the patients observed in that study had advanced disease at the time of diagnosis . small - bowel barium studies ( barium follow - through ) and small - bowel enema ( or enteroclysis ) are standard examinations when either neoplastic or inflammatory disease of the small bowel is suspected . 
these examinations visualise the gastrointestinal tract from the inside and therefore allow accurate evaluation of the normal features and possible alterations of the mucosa and lumen , but they provide only indirect information on the intestinal wall and adjacent extraintestinal structures [ 2 ]  . 
tomographic techniques , such as ultrasound and computed tomography ( ct ) , directly depict both the wall ( allowing evaluation of thickness and structural characteristics ) and adjacent structures ( mesentery , adjacent fibrofatty tissue , lymph nodes , peritoneal spaces )  . 
additionally , as this modality is noninvasive and involves no exposure to ionising radiation , it is ideal in patients requiring prolonged follow - up ( chronic inflammatory diseases ) or in children , or to confirm or rule out clinical suspicion , reserving the other diagnostic methods for strongly suspicious cases or cases with positive ultrasound [ 3 ]  . 
introduction of the multidetector technique is also modifying the diagnostic workup of patients with suspected small - bowel disease [ 48 ] , but only few reports have described the use of this method in patients with small - bowel neoplasms [ 912 ]  . the purpose of our study was to evaluate the diagnostic potential of multidetector ct ( mdct ) in the study of smallbowel tumours after distension of the small bowel with a low - density contrast agent . materials and methods study population we examined 120 consecutive patients with a definite , strongly suspected or suspected diagnosis of small - bowel 1014 locclusione intestinale il sintomo di esordio nel 36% dei pazienti [ 1 ]  . nonostante si sia verificato negli ultimi 40 anni un notevole miglioramento sia della chirurgia che dellimaging diagnostico , la sopravvivenza dei pazienti con malignit primitiva dellintestino tenue non ha mostrato un parallelo miglioramento , principalmente in rapporto allo stadio avanzato del tumore al momento dellintervento chirurgico . 
anche se non recente , un interessante studio ha analizzato i dati di tutti i pazienti con diagnosi di malignit dellintestino tenue in un periodo di 21 anni [ 1 ] , valutando lintervallo di tempo che intercorreva tra linizio dei sintomi ed il primo contatto medico e tra il contatto medico e la diagnosi , e ha dimostrato che il ritardo diagnostico medio attribuibile al paziente era inferiore a 2 mesi ; quello attribuibile al medico per mancata richiesta di un test diagnostico appropriato era di 8 , 2 mesi ; quello attribuibile al radiologo per mancata diagnosi era 12 mesi . 
tra i pazienti osservati in questo studio , tre quarti di essi aveva una malattia avanzata al momento della diagnosi . il tenue baritato per os ( o transito intestinale ) e il clisma del tenue ( o enteroclisi ) sono gli esami che solitamente vengono effettuati nel sospetto di patologia dellintestino tenue , sia neoplastica che infiammatoria . 
essi visualizzano il tratto gastroenterico dallinterno e quindi possono valutare con accuratezza i caratteri normali e le eventuali alterazioni della mucosa e del lume del viscere , ma forniscono informazioni solo indirette sulla parete intestinale e sulle strutture extraintestinali adiacenti [ 2 ]  . 
le tecniche tomografiche , quali ecografia e tomografia computerizzata ( tc ) , consentono invece la visualizzazione diretta sia della parete ( valutandone spessore e caratteri strutturali ) sia delle strutture extraviscerali adiacenti ( mesentere , cellulare fibroadiposo periviscerale , linfonodi , spazi peritoneali )  . 
lesame ecografico ha anche la prerogativa di visualizzare tono e attivit contrattile dei segmenti tenuali , esaminati in condizioni assolutamente fisiologiche , ed essendo tecnica non invasiva e priva di esposizione a radiazioni ionizzanti , si propone come mezzo ideale qualora sia necessario un follow - up prolungato nel tempo ( pazienti con patologia infiammatoria cronica ) oppure in et pediatrica , oppure per avvalorare o al contrario escludere un sospetto clinico riservando altre metodiche diagnostiche solo ai casi risultati effettivamente sospetti o positivi allecografia [ 3 ]  . 
definite diagnoses were based on histological examination of the biopsy specimen ; strongly suspected diagnoses were based on a recent contrast - enhanced study of the small bowel ( small - bowel enema or barium study ) that was positive for small - bowel disease ; suspected diagnoses were based on the presence of clinical signs and symptoms ( diarrhoea , abdominal pain , bleeding ) indicative of small - bowel disease . 
after methylcellulose infusion , the ct scan was performed before and during iv administration of iodinated contrast material , with image acquisition from the diaphragm to the perineum during a single inspiration . 
the contrast - enhanced ct study was acquired 40 s after iv administration of 130150 ml of contrast material ( ultravist 370 , schering ag , berlin , germany ) injected at a rate of 3 ml / s . 
il consenso informato stato ottenuto da tutti i pazienti . tecnica prima dellesame tutti i pazienti venivano sottoposti a preparazione intestinale secondo il seguente schema : due giorni prima dellesame , dieta povera di frutta e verdura ; il giorno prima , 150 mg di una miscela di sennosidi a e b con una tazza di t zuccherato alle ore 8 : 00 ; alle 13 : 00 , dieta semiliquida ; alle 17 : 00 , 15 mg di solfato di magnesio in 3 / 3 4 / / di un bicchiere di acqua tiepida seguita dallassunzione di 3 litri di acqua nelle 45 ore successive ; alle 21 : 00 , una tazza di brodo caldo ; dalle 21 : 00 in poi , digiuno . cinquantasei pazienti ottenevano una distensione dellintestino mediante somministrazione orale di 1 , 52 , 0 l di una soluzione iso - osmolare di polietilen - glicole somministrata in dosi uguali di 100 ml a partire da 45 minuti prima dellesame tc ( enterografia - tc con peg o peg - tc )  . 
sessantaquattro pazienti sono stati sottoposti al posizionamento sotto guida fluoroscopica di un sondino naso - digiunale 1216 f cui seguita liniezione manuale di 1 , 52 , 5 l di metilcellulosa prima dellesame tc ( enteroclisi tc o e - tc )  . al fine di evitare spasmi , ottenere una omogenea distensione dellintestino tenue , ridurre il disagio e la tensione addominale , veniva somministrato endovena ai pazienti un farmaco anticolinergico ( n - butilscopolamina ) ; somministravamo 10 mg di farmaco quando il paziente cominciava ad avvertire dolore addominale ( generalmente dopo la somministrazione di 11 , 5 l di metilcellulosa o di peg ) , 10 mg subito prima dellacquisizione delle immagini tc . tutti i pazienti venivano studiati con tc multidetettore a 16 strati ( lightspeed pro16 , ge medical system , milwakee , usa ) , con i seguenti parametri di scansione : collimazione 1 , 25 mm , velocit di scorrimento del tavolo 13 , 75 mm / rot , 120 kw , mas 500 , pitch 1 , 375 , tempo di rotazione 0 , 6 s . 
al termine dellinfusione di metilcellulosa , lesame tc veniva eseguito prima e durante la somministrazione di mdc iodato ev , con acquisizione delle immagini dal diaframma al perineo , durante una singola inspirazione . 
lacquisizione delle immagini avveniva in decubito supino tranne che nei pazienti sottoposti ad enteroclisi tc nei quali si verificava vomito al termine o durante linfusione di metilcellulosa ; in tali pazienti lassunzione del decubito prono 1015 l.m. 
a welldistended loop was defined as pathological if thinner than 3 m pathological loops were assessed for wall - thickening characteristics ( symmetrical / asymmetrical , circumferential / eccentric ) , degree and pattern of parietal enhancement after contrast administration ( homogeneously hyperdense or hypodense , stratified , inhomogeneous , target sign with alternating layers of hyperdensity and hypodensity )  . 
we also considered the presence of associated signs : perienteric stranding ( loss of the normal interface between the loop wall and the mesentery ) ; comb sign ( mesenteric hypervascularity with vascular dilatation , tortuosity , hypertrophy and increased spacing , dilatation of the vasa recta ) ; fibrofatty proliferation ( increased attenuation of mesenteric fat ) ; complications such as abscesses ( round or oval masses with fluid density , delimited by a hyperdense wall and possibly containing air ) , fistulae ( communication between two contiguous organs or with the skin ) or phlegmons ( poorly defined mesenteric densities ) ; enlarged lymph nodes ; reduced lumen size with possible upstream dilatation ; extravisceral masses ; and others . the 2 statistical test was used to confirm the statistical significance of the difference between bowel - loop distension in patients studied with peg - ct and those studied with ct enteroclysis . 
a significance level of 95% was considered adequate [ 13 ]  . results examinations were successfully completed in all patients . vomiting occurred in 7 / 64 ( 11% ) patients studied with ct enteroclysis . with reference to the degree of loop distension in patients studied with peg - ct , complete distension of the proximal jejunum was found in 35 / 56 ( 62% ) , of the distal jejunum in 42 / 56 ( 76% ) , of the proximal ileum in 47 / 56 ( 84% ) , of the distal ileum in 47 / 56 ( 84% ) and of the terminal ileum in 43 / 56 ( 78% ) patients . 
in patients studied with ct enteroclysis , complete distension of the proximal jejunum was found in 50 / 64 ( 79% ) cases , of the distal jejunum in 53 / 64 1016 serviva ad ostacolare il reflusso di metilcellulosa nello stomaco e a ridurre il rischio di inalazione del vomito , favorendo pertanto leffettuazione dellesame stesso . 
lo studio tc con il contrasto veniva acquisito 40 secondi dopo la somministrazione ev di 130150 ml di mezzo di contrasto ( ultravist 370 , schering ag , berlino , germania ) , iniettato alla velocit di 3m / s ; se ritenuto opportuno , lesame veniva completato con studio del parenchima epatico in fase portale e tardiva . con una computer workstation ( advantage windows , ge medical system ) le immagini assiali venivano rielaborate con ricostruzioni in 2d , coronali ed eventualmente sagittali . analisi delle immagini tc due radiologi esperti in radiologia gastro - intestinale , non coinvolti nelleffettuazione dellesame , hanno rivisto le immagini in consenso senza essere a conoscenza dei dati clinici e chirurgici , e hanno valutato grado di distensione delle anse tenuali , numero e sede delle anse patologiche . il grado di distensione delle anse stato classificato con una scala soggettiva a 4 punti ( 0 : distensione assente ; 1 : incompleta ; 2 : parziale ; 3 : completa )  . 
unansa ben distesa stata definita patologica se di spessore superiore a 3 mdi essa abbiamo valutato le caratteristiche dellispessimento parietale ( simmetrico / asimmetrico , circonferenziale / eccentrico ) , il grado e le caratteristiche dellenhancement parietale dopo mdc iodato : omogeneamente iperdenso o ipodenso , stratificato , disomogeneo , segno del bersaglio ( o target sign : strati alternati di ipered ipodensit )  . 
abbiamo inoltre considerato la presenza di segni associati : stranding perienterico ( perdita della normale interfaccia tra la parete dellansa e il mesentere ) ; segno del pettine ( o comb sign , cio ipervascolarizzazione del mesentere coinvolto da flogosi che si manifesta come dilatazione delle arterie mesenteriche , tortuosit , ipertrofia e maggiore ampiezza , dilatazione dei vasi retti ) ; proliferazione fibroadiposa ( o fibrofatty proliferation : aumento dei valori di attenuazione del grasso mesenterico ) ; complicanze , come ascessi ( masse a densit fluida rotondeggianti o ovoidali , delimitate da parete iperdensa ; eventuale presenza di aria allinterno della massa ) , fistole ( comunicazioni tra due organi attigui o comunicazioni con la cute ) e flemmoni ( densit mesenteriali scarsamente definite ) ; linfoadenomegalie ; riduzione di calibro del lume con eventuale dilatazione a monte ; masse extraviscerali ; altro . per la verifica della significativit statistica della differenza tra la distensione delle anse intestinali nei pazienti studiati con peg - tc e in quelli studiati con enteroclisi - tc , si adottato il test statistico del 2 . 
si considerato adeguato un livello di significativit pari al 95% [ 13 ]  . ( 83% ) , of the proximal ileum in 58 / 64 ( 90% ) , of the distal ileum in 59 / 64 ( 92% ) and of the terminal ileum in 58 / 64 ( 90% ) patients . 
an additional dose of 250300 ml of methylcellulose or peg was administered at the end of the unenhanced scans in 5 / 64 ( 8% ) patients and in 8 / 56 ( 14% ) patients , respectively . distension of the proximal jejunum and terminal ileum was found to differ significantly , as confirmed by the 2 test ( with 4.10 degrees of freedom ) in patients studied with ct enteroclysis and those studied with peg - ct . 
in other words , distension of the proximal jejunum and the terminal ileum was significantly better in patients studied with ct enteroclysis compared with those studied with peg - ct . 
the first iv dose of 10 mg was usually administered after 11.5 l of methylcellulose or peg . fifteen out of 120 patients ( 12.5% ) had small - bowel neoplasms ( table 1 )  . 
vomito si verificato in 7 / 64 ( 11% ) pazienti studiati con enteroclisi tc . in riferimento al grado di distensione delle anse , nei pazienti studiati con peg - tc si riscontrata una distensione completa del digiuno prossimale in 35 / 56 ( 62% ) pazienti , del digiuno distale in 42 / 56 ( 76% ) pazienti , dellileo prossimale in 47 / 56 ( 84% ) pazienti , dellileo distale in 47 / 56 ( 84% ) pazienti e dellultima ansa in 43 / 56 ( 78% ) pazienti . nei pazienti studiati con enteroclisi tc si riscontrata una distensione completa del digiuno prossimale in 50 / 64 ( 79% ) pazienti , del digiuno distale in 53 / 64 ( 83% ) pazienti , dellileo prossimale in 58 / 64 ( 90% ) pazienti , dellileo distale in 59 / 64 ( 92% ) pazienti e dellultima ansa in 58 / 64 ( 90% ) pazienti . 
2 computed tomography enteroclysis shows minimal hypodense wall thickening of a few jejunal loops ( inside of octagon ) ; several lymphadenopathies ( inside the triangle ) are also evident . 
2 lenteroclisi tc documenta minimo ispessimento parietale ipodenso di alcune anse digiunali ( allinterno dellottagono ) ; limitrofe ad esse sono evidenti diverse linfoadenomegalie ( allinterno del triangolo )  . 
in altre parole la distensione del digiuno prossimale e dellultima ansa ileale sono risultate migliori in modo statisticamente significativo nei pazienti studiati con enteroclisi tc rispetto a quelli studiati con peg - tc . 
la prima dose di 10 mg ev stata solitamente somministrata dopo la somministrazione di 11 , 5 l di metilcellulosa o di peg . quindici / 120 ( 12 , 5% ) pazienti sono risultati affetti da neoplasia dellintestino tenue ( tabella 1 ) ; in particolare abbiamo riscontrato un tumore primitivo benigno in 4 / 15 ( 27% ) pazienti , un tumore primitivo maligno in 10 / 15 ( 67% ) , una localizzazione metastatica da melanoma in 1 / 15 ( 6% )  . 
4 tc con peg : formazione polipoide dellultima ansa ileale ( freccia grande ) in paziente affetta da sindrome di peutz - jeghers ; altri polipi pi piccoli ( frecce piccole ) sono evidenti vicino ad essa . discussione discussion small - bowel neoplasms are uncommon tumours that are often small and difficult to identify and therefore constitute a major diagnostic challenge for radiologists . 
il clisma del tenue ( effettuato previa somministrazione di bario e metilcellulosa tramite sondino naso - digiunale ) e il tenue baritato per os ( solo bario somministrato per via orale ) sono gli esami che vengono solitamente effettuati nel sospetto di patologia neoplastica dellintestino tenue . 
these findings are similar to those of a previous study that attributed a sensitivity of 44% to barium follow - through studies in detecting actual neoplasms in the small bowel [ 15 ]  . 
the results of these studies indicate that small - bowel enema is far more sensitive than barium follow - through in identifying small - bowel tumours , because it can diagnose tumours at an early stage and consequently influence their prognosis . over the last few years , however , the introduction of ct associated with iodinated contrast material and small - bowel distension has modified the diagnostic approach to patients with suspected small - bowel disease [ 9 , 1620 ]  . 
reperto operatorio : metastasi da melanoma . ricano ha comparato il valore del clisma del tenue con quello del tenue baritato per os nella dimostrazione di tumori maligni primitivi del tenue [ 14 ]  . 
i risultati ottenuti da questi studi indicano che il clisma del tenue molto pi sensibile del tenue maritato per os nellindividuare i tumori dellintestino tenue , in quanto pu diagnosticare tumori in stadio precoce e di conseguenza influenzare la prognosi . negli ultimi anni , tuttavia , lintroduzione della tc associata alla somministrazione di mezzo di contrasto iodato e alla distensione delle anse tenuali , ha modificato lapproccio diagnostico al paziente con sospetta patologia tenuale [ 9 , 1620 ]  . 
segni tc caratteristici di una neoformazione maligna sono lispessimento della parete eccentrico o asimmetrico , un contorno ( sia interno che esterno ) lobulato e / o la presenza di una massa della densit dei tessuti molli superiore ai due cm , estesa dal lume alla superficie sierosa [ 18 , l.m. 
la recente introduzione della tc multidetettore ha migliorato la sensibilit della metodica nel rilievo di piccole lesioni neoplastiche [ 5 , 9 , 11 , 12 ] , nonch la qualit delle ricostruzioni 2d e 3d , permettendo di ottenere immagini gradite al clinico e al chirurgo perch utili alla pianificazione chirurgica [ 5 , 19 ]  . un problema dello studio tc dellintestino tenue la mancanza di una standardizzazione della tecnica in letteratura ove non esiste un accordo su quale sia il tipo di contrasto da impiegare per la distensione delle anse , ipodenso [ 2527 ] o iperdenso [ 28 ] , e sulla modalit di somministrazione , per via orale a dose unica , multipla o frazionata [ 23 , 29 ] oppure tramite sondino naso - digiunale con pompa di infusione [ 20 , 30 , 31 ] o senza pompa di infusione [ 19 , 27 ]  . 
i mdc iperdensi sono pi noti e sperimentati , consentono di delimitare le anse intestinali e stabilire se un processo espansivo intrao extraluminale , ma non consentono , per lelevata densit , una accurata valutazione delle caratteristiche di parete ed interferiscono con eventuali ricostruzioni 3d simil - angiografiche . 
i mezzi di contrasto ipodensi sono preferibili a quelli iperdensi perch permettono una migliore rappresentazione dellenhancement della parete compresa tra lipodensit del fluido endoluminale e lipodensit del tessuto adiposo extraluminale [ 26 ] e non interferiscono con le ricostruzioni similangiografiche . 
come mezzi di contrasto ipodensi sono stati proposti per via orale acqua , aria , emulsioni di olio , volumen o peg , oppure metilcellulosa o acqua tramite sondino naso - digiunale [ 12 , 19 , 20 , 2527 , 3032 ]  . le emulsioni di olio forniscono valori di densit pi negativi rispetto allacqua , ma a causa del sapore non sono apprezzate dai pazienti e lelevato costo limita il loro routinario impiego clinico . 
lacqua ha il vantaggio della economicit , della buona accettabilit da parte del paziente , di consentire laccurata valutazione della parete intestinale e del suo enhancement , di non interferire con eventuali ricostruzioni 3d simil - angiografiche , ma viene rapidamente assorbita e tende a stimolare la peristalsi , non garantendo una adeguata distensione del digiuno distale e dellileo . 
laria , somministrata o mediante assunzione orale di sostanze effervescenti a rilascio ritardato o , per lo studio delle ultime anse ileali , per via rettale , ha ottenuto risultati soddisfacenti sulla dimostrazione di patologie intraluminali ed intramurali , anche se leccessiva differenza tra la sua densit ( 800 hu ) e quella della parete intestinale dopo mdc ( da + 100 a - 135 hu ) determina spesso comparsa di artefatti che ne hanno limitato limpiego . 
7a , b polyethylene glycol computed tomography shows ( a ) an intraluminal mass ( black arrow ) with fat density associated with loop invagination ( white arrow )  . 
no agreement exists in the literature on the type of contrast material to be used for bowel distension low density [ 2527 ] or highdensity [ 28 ] or regarding administration protocol oral in a single dose or in multiple or split doses [ 23 , 29 ] , or via a nasojejunal tube with [ 20 , 30 , 31 ] or without [ 19 , 27 ] an infusion pump . 
they allow intestinal loops to be delimited and help verify whether an expansive process is intraor extraluminal , but they do not allow , given their high density , accurate evaluation of wall characteristics , and they interfere with possible angiographylike 3d reconstructions . 
low - density agents are to be preferred because they allow better depiction of wall enhancement between the hypodensity of the intraluminal fluid and the hypodensity of the extraluminal fat tissue [ 26 ] and do not interfere with angiography - like reconstructions . 
proposed low - density contrast agents are water , air , oil emulsions , volumen or peg for oral use , and methylcellulose or water administered through a nasojejunal tube [ 12 , 19 , 20 , 2537 , 3032 ]  . 
oil emulsions provide lower density values than do water , but because of their taste , patients do not appreciate them , and their high cost limits their routine clinical use . 
water is cheap , well - tolerated by patients , allows accurate evaluation of the intestinal wall and its enhancement , and does not interfere with any 3d angiography - like reconstructions ; however , it is absorbed rapidly and tends to stimulate peristalsis , failing to ensure adequate distension of the distal jejunum and the ileuair , administered either orally through delayed - release effervescent substances or rectally , for the study of the terminal ileum , has produced satisfactory results in the demonstration of intraluminal and intramural diseases . however , the excessive difference between its density ( 800 hu ) and that of the enhanced intestinal wall ( + 100135 hu ) often gives rise to artefacts , which have limited its use . 
 a common drawback of oral contrast agents is that they fail to ensure a suitable and uniform distension of all smallbowel loops , giving rise to significant problems in differenti1022 fig . 
8 enteroclisi tc ( scansione ottenuta in posizione prona ) : ultima ansa ileale ed ileo distale a pareti ispessite ; in particolare evidente laspetto target sign dellultima ansa ileale ( freccia grande ) associato a comb sign ( frecce piccole )  . li tra ispessimenti parietali reali o insufficiente distensione / spasmo viscerale . 
il problema viene superato , a prezzo di maggiori invasivit , tempo e costo , dallenteroclisi - tc , metodica sviluppata nei primi anni 90 , in cui , prima dellesecuzione dellesame tc senza e con mdc ev , quantit variabili ( 20002750 cc ) di mdc ipodenso ( metilcellulosa o acqua ) o iperdenso ( diatrizoato di sodio al 4%15% , solfato di bario all1% ) vengono infuse manualmente o con pompa peristaltica attraverso sondino naso - digiunale [ 12 , 19 , 20 , 27 , 30 , 31 ]  . nel nostro lavoro abbiamo usato entrambe le tecniche ed abbiamo preferito usare due mezzi di contrasto ipodensi in modo da ottenere un ottimale studio della parete compresa tra lipodensit del lume opacizzato dal contrasto e lipoating between real wall thickenings and inadequate distension or spas the problem can be overcome although with greater invasiveness , time and costs by using ct enteroclysis , a method developed in the early 1990s in which variable amounts ( 2 , 0002 , 750 cc ) of low - density ( methylcellulose or water ) or high - density ( 4%15% sodium diatrizoate , 1% barium sulphate ) contrast material are infused by hand or with a peristaltic pump through a nasojejunal tube before the ct scan with and without iv contrast material [ 12 , 19 , 20 , 27 , 30 , 31 ]  . in our study , we employed both techniques , and we preferred to use two low - density contrast agents in order to obtain an optimal study of the wall between the hypodensity of the enhanced lumen and the hypodensity of the extravisceral fat . 
we chose methylcellulose for ct enteroclysis and peg for ct enterography , the former already widely employed both in small - bowel enema and in ct [ 19 , 20 , 30 , 31 ] , the latter mainly used in magnetic resonance imaging [ 33 , 34 ] and more rarely in ct [ 26 ]  . 
in contrast to other authors [ 21 , 31 ] , we preferred to administer the hypotonic agent in two doses of 10 mg , the first when the patient felt abdominal pain ( generally after receiving 11.5 l of methylcellulose or peg ) , the second immediately before the ct scan . 
 if we compared the degree of loop distension obtained using ct enteroclysis and peg enterography in our study , we found that the degree of distension was better with enteroclysis compared with the simple oral administration of contrast material , particularly with regard to the jejunu this finding might , theoretically , lower the sensitivity of ct in detecting jejunal neoplasms if the loop is not well distended . 
in our study , we identified ten jejunal neoplasms ( table 1 ) , five studied with ct enteroclysis and five with peg - ct , and all were well depicted . 
regardless of the technique used , in all neoplastic patients , we obtained excellent characterisation of wall masses with exophytic and intraluminal growth patterns . as for the iodinated contrast material , there is no agreement in the literature over the timing of administration : some prefer a 25 - s arterial phase [ 31 ] , others a late arterial phase [ 20 , 28 ] , yet others a single phase of 60 / 70 s [ 35 ]  . 
in our study , the ct investigation was performed 40 s after the start of infusion to obtain a study of the loops in the arterial phase , possibly followed by a study of the liver parenchyma in the portal and late phases . 
iodinated contrast material administration helped us to better define the wall thickness and enhancement pattern , to optimise lesion characterisation , to differentiate between lymphadenopathy and wall masses and to stage the neoplasms . 
abbiamo scelto la metilcellulosa per lenteroclisi tc e il peg per lenterografia tc , la prima gi ampiamente impiegata sia nel clisma del tenue che nellesame tc [ 19 , 20 , 30 , 31 ] , il secondo usato principalmente in rm [ 33 , 34 ] , pi raramente in tc [ 26 ]  . poich non abbiamo una pompa per linfusione , abbiamo somministrato manualmente la metilcellulosa , cercando di ottenere uniniezione costante e continua . 
la tc veniva eseguita al termine dellinfusione ; se le scansioni di base senza contrasto dimostravano una non ottimale distensione delle anse , somministravamo unulteriore dose di metilcellulosa . inoltre , abbiamo usato un ipotonizzante , somministrato ev in modo da avere una maggiore rapidit dazione , con la finalit di ottenere unomogenea distensione delle anse e ridurre il grado di disagio del paziente . 
a differenza di altri autori [ 21 , 31 ] , abbiamo preferito somministrare lipotonizzante in due dosi di 10 mg , la prima quando il paziente lamentava dolore addominale ( generalmente dopo la somministrazione di 11 , 5 l di metilcellulosa o di peg ) , la seconda subito prima dellesame tc . 
seguendo questi accorgimenti , in uno studio precedente abbiamo dimostrato di potere ottenere anche senza pompa di infusione una buona distensione delle anse tenuali [ 19 ]  . se nel nostro lavoro confrontiamo il grado di distensione delle anse ottenuto con le due metodiche , enteroclisi tc ed enterografia con peg , riscontriamo che il grado di distensione migliore con tecnica enteroclisi rispetto alla semplice somministrazione del mezzo di contrasto per via orale , in particolare nel digiuno . 
nel nostro studio abbiamo dimostrato 10 localizzazioni neoplastiche digiunali ( tabella 1 ) , 5 studiate con enteroclisi tc , 5 studiate con peg - tc , e in tali pazienti abbiamo ottenuto una buona rappresentazione della patologia neoplastica . 
indipendentemente dalla tecnica impiegata , in tutti i pazienti neoplastici abbiamo ottenuto uneccellente caratterizzazione delle masse parietali sia a sviluppo esofitico che endoluminali . per quanto riguarda il mezzo di contrasto iodato , non esiste un accordo in letteratura sul tempo di somministrazione : alcuni preferiscono una fase arteriosa a 25 secondi [ 31 ] , altri una fase arteriosa tardiva [ 20 , 28 ] , altri una singola fase a 6070 secondi [ 35 ]  . 
nel nostro studio lesame tc stato effettuato dopo 40 secondi dallinizio dellinfusione iodata , in modo da ottenere uno studio delle anse in fase arteriosa con eventuale completamento di studio del parenchima epatico in fase portale e tardiva . 
la somministrazione del contrasto iodato ci ha permesso di definire meglio lo spessore della parete e le caratteristiche del contrast enhancement parietale , di ottimizzare la caratterizzazione delle lesioni , di differenziare tra linfoadenopatie e masse parietali , e di stadiare la patologia neoplastica . 
rispetto ad esse la tc ha il vantaggio di definire lestensione reale delle lesioni parietali , leventuale estensione transmurale , il grado di coinvolgimento del mesentere e le localizzazioni a distanza . 
in our study , for example , we identified extramural extension in five patients and nodal enlargement in the six cases of lymphoma and the case of adenocarcinoma ; hepatic metastases were present in one case of carcinoid tumour associated with calcified lymph nodes and hypervascular lymphadenopathy . 
however , ct was unable to depict the fine details of the mucosal surface and intramural structures that only barium studies can demonstrate [ 8 , 19 , 30 ]  . 
this factor represents a significant limitation , particularly in diseases where the mucosal layer integrity needs to be demonstrated . in conclusion , multidetector ct , performed after distension of the small bowel with low - density contrast material and after infusion of iodinated contrast material , is a useful method in the diagnosis and staging of small - bowel neoplasms . 
it requires a scrupulous technique and , in selected cases , should be integrated with conventional radiological methods . stro studio , ad esempio , abbiamo riscontrato unestensione extramurale in 5 pazienti , linfoadenomegalie nei 6 casi di linfoma e nel caso di adenocarcinoma ; metastasi epatiche erano presenti in un caso di carcinoide ove si associavano anche linfonodi calcifici e linfoadenomegalie ipervascolarizzate . 
tuttavia , la tc non pu fornire quei fini dettagli della superficie mucosa e delle strutture intramurali che solo gli esami con contrasto baritato possono dimostrare [ 8 , 19 , 30 ]  . 
tale dato costituisce una limitazione importante della metodica , in particolare nelle patologie in cui sia necessario dimostrare leventuale integrit dello strato mucoso . in conclusione possiamo affermare che la tc multidetettore , effettuata previa distensione delle anse tenuali con mezzo di contrasto ipodenso e dopo infusione di mezzo di contrasto iodato , una metodica utile nella diagnosi e stadiazione della patologia neoplastica tenuale . 
sixty patients were evaluated with 64row cta ( vct , general electric healthcare , milwaukee , wi , usa ) with a collimation of 0.625 mm after the injection of iodinated nonionic contrast material ( 4 ml / s )  . 
the common hepatic artery was normal in 60% of patients . the inferior pancreaticoduodenal arteries were either absent or not assessable in 8.3% of cases and there was a double trunk in 5% , a common trunk in 83.3% and a single vessel in 3.3%. 
the techniques high sensitivity allowed us to observe that the prevalence of vascular abnormalities is higher than that reported in the literature . key words mdct angiography hepatic arteries anomalies abdominal vessels riassunto obiettivo . 
sono stati valutati 60 pazienti sottoposti a studio con angio - tc a 64 strati , utilizzando una collimazione submillimetrica ( 0 , 625 ) e previa somministrazione di mezzo di contrasto iodato non ionico ad alto flusso ( 4 ml / s )  . 
le arterie pancreatico - duodenali inferiori risultavano assenti o non valutabili nel 8 , 3% , era presente un doppio tronco nel 5% , un tronco comune nel 83 , 3% , ed un unico vaso nel 3 , 3% . 
questa elevata sensibilit ha permesso di rilevare come il numero di anomalie vascolari risulti pi elevato di quello riportato in letteratura . parole chiave angiografia mdct anomalie delle arterie epatiche vasi addominali introduction introduzione technological advances in multidetector computed tomography ( mdct ) and hardware and software systems have made gli sviluppi tecnologici della tomografia computerizzata multidetettore , dei sistemi hardware e dei software applicar . 
this makes the technique indispensable for surgeons , for example , in planning liver transplantation surgery or , more commonly , in fashioning intestinal anastomoses , the success of which is dependent on adequate vascularity . 
in addition , several regions , such as the splenic fissure of the transverse colon , show major variations in both the distribution and calibre of vessels , which often affect the outcome of surgery . our study aimed to assess the accuracy of 64 - row cta in studying vascular anatomy and evaluating the prevalence of anatomical variations in the origin and collateral branches of the coeliac trunk and superior and inferior mesenteric arteries . 
our findings were compared with those of previous studies based on other methods ( conventional angiography and anatomical dissection )  . materials and methods patient population between march and june 2006 , 350 patients were studied by multidetector spiral ct at our department . 
from among these 150 patients , a radiologist ( cndc ) not involved in subsequent image analysis prospectively and consecutively selected 60 patients meeting the following inclusion criteria : performance of a ct scan in the arterial and venous phase for a variety of clinical indications , from inflammatory ( crohns disease , prostatitis ) to oncological diseases ( breast cancer , lung cancer , prostate cancer , colon cancer )  . 
exclusion criteria were the presence of any condition likely to affect normal vascular anatomy , such as gastric resection surgery ; extended jejunoileal resections ; colonic resections ; anterior rectal resection ; partial pancreaticoduodenectomy ; bariatric surgery ; liver , pancreas , bowel or multiorgan transplants ; and major hepatic resections . 
patients were also excluded if they had conditions that could modify normal arterial diameter and blood flow , as this would affect the study of collateral circulation between the coeliac trunk and the superior mesenteric artery and between the superior and inferior mesenteric artery . 
in detail , patients were excluded if they had stenotic or aneurysmal disease of the arteries to be studied , severe aortic atherosclerosis , arteritis with possible involvement of the vessels being studied ( kawasakis disease , polyarteritis nodosa , takayasus arteritis , churg - strauss syndrome ) present for at least 5 years , severe untreated abdominal aorta aneurysms or aortic dissection . 
patients who had undergone splenectomy , minor hepatic resections , partial jejunoileal resections or had ascending or thoracic aorta disorders were included because the vascular changes associated with these conditions were irrelevant for the purposes of the study . tivi , hanno reso langiografia con tc spirale multidetettore il test diagnostico di scelta per lo studio non invasivo dei vasi splancnici [ 1 ]  . 
le tc di ultima generazione a 64 strati permettono lesecuzione di esami ad altissima risoluzione spaziale ( fino a 0 , 4 mm ) con risoluzione temporale di pochi secondi . 
si pensi ai vantaggi che ci determina in fase di programmazione di interventi di trapianto del fegato o , pi frequentemente , nellesecuzione di anastomosi intestinali , per la cui corretta tenuta fondamentale una adeguata vascolarizzazione . 
inoltre , alcuni distretti , come la flessura splenica del colon trasverso , presentano unimportante variabilit sia nella distribuzione che nel calibro vasale , che spesso inficiano la buona riuscita dellintervento . il nostro studio si prefisso lo scopo di valutare quanto langio - tc a 64 strati sia adeguata nello studio dellanatomia vascolare e nella valutazione dellincidenza delle varianti anatomiche del tripode celiaco , delle arterie mesenteriche superiori ed inferiori , sia per quanto riguarda la loro origine dallaorta sia per quanto riguarda i loro rami collaterali ; tali risultati sono stati confrontati con quelli presenti in letteratura ottenuti con altre metodiche ( angiografia e dissezione anatomica )  . materiali e metodi popolazione di pazienti nel periodo compreso tra marzo e giugno del 2006 , presso il nostro istituto sono stati sottoposti a tc spirale multidetettore 350 pazienti , dei quali 150 per tc total body o addomepelvi . 
tra questi ultimi 150 casi , un radiologo ( c.n.d.c ) non coinvolto nella successiva fase di lettura ha selezionato prospetticamente e consecutivamente 60 pazienti che rientravano nei seguenti criteri di inclusione : esecuzione di uno studio in fase arteriosa e venosa per indicazioni cliniche di varia natura da quelle di origine infiammatoria ( morbo di crohn , prostatiti ) ad indicazioni di tipo oncologico ( tumore della mammella , tumore del polmone , tumore della prostata , tumore del colon )  . 
i criteri di esclusione riguardavano tutte quelle condizioni che potevano modificare la normale anatomia vascolare come : interventi chirurgici di resezione gastrica ; resezioni digiuno - ileali estese ; resezioni coliche ; resezione anteriore del retto ; duodeno - cefalopancreasectomia ; chirurgia bariatrica ; trapianti di fegato , pancreas , intestino o trapianti multiviscerali ; resezioni epatiche maggiori . 
sono stati esclusi anche i pazienti affetti da condizioni patologiche che potevano modificare il normale calibro e flusso arterioso alterando lo studio dei circoli collaterali tra tripode celiaco ed arteria mesenterica superiore e tra arteria mesenterica superiore ed inferiore . 
thus , a patient weighing 80 kg will require the injection of 40 gi ( approximately 115 ml of contrast medium followed by 40 ml of saline solution ) ( xenetix 350 , guerbet , france )  . 
the injection rate , identical for contrast bolus and saline solution , should be high , as arterial enhancement is directly dependent on flow rate ; in our study , a flow rate of 4.0 ml / s was used routinely . 
we used multiplanar reconstructions ( mprs ) in the three spatial planes and three - dimensional reconstructions using maximum intensity projection ( mip ) and volume rendering ( vr )  . 
images were reconstructed and analysed interactively by two radiologists working in consensus , who wrote up the reports on a specific computerised forfor the study of variation of the hepatic arteries , we adopted the michels classification ( table 1 )  . 
sono stati inclusi nello studio i pazienti sottoposti a splenectomia , resezioni epatiche minori , resezioni digiunoileali segmentarie e patologie dellaorta ascendente o toracica dato che le modificazioni vascolari associate a tali quadri patologici risultano ininfluenti ai fini dello studio . tecnica di studio le immagini tc sono state ottenute mediante unapparecchiatura tc multidetettore a 64 strati ( vct , general electric healthcare , milwaukee , usa ) con matrice simmetrica composta da 64 file di detettori , ciascuno dello spessore minimo di 0 , 625 mm utilizando una collimazione di 0 , 625 . 
la somministrazione di mdc risulta un elemento fondamentale per la buona riuscita dellesame : per liniezione del mezzo di contrasto stato utilizzato un iniettore a doppia testa ( ezem , empower cta , ny , usa ) che consente di iniettare un bolo compatto di mezzo di contrasto iodato seguito da una spinta di un bolo di soluzione fisiologica ( nacl 0 , 9% )  . 
la quantit di iodio necessaria per una buona opacizzazione dei vasi mesenterici , espressa in grammi di iodio , si pu ottenere dividendo per due il peso del paziente ( gi = bw / 2 dove g = grammi ; i = iodio ; bw = body weight = peso del paziente )  . 
pertanto per un paziente di 80 kg si devono iniettare circa 40 g di iodio ( circa 115 ml di mdc seguito da 40 ml di soluzione fisiologica ) ( xenetix 350 ; guerbet , francia )  . 
la velocit di iniezione , identica per il bolo di mezzo di contrasto e per quello di soluzione fisiologica , deve essere elevata in quanto lenhancement vascolare arterioso direttamente dipendente dalla velocit del flusso ; nella nostra esperienza abbiamo utilizzato routinariamente una velocit di flusso di 4 , 0 ml / s . 
il tempo di ritardo dallinizio della scansione stato stabilito mediante una tecnica di identificazione automatica del bolo ( bolus tracking ) posizionando la regione di interesse per il calcolo della densit a livello dellaorta al passaggio toraco - addominale ; linizio della scansione avviene ad una densit di 150 uh . lanalisi delle immagini stato eseguito su console dedicata ge equipaggiata con software di ricostruzione advantage windows 4.2 utilizzando ricostruzioni multiplanari sui tre piani dello spazio e ricostruzioni tridimensionali utilizzando algoritmi di ricostruzione di massima intensit ( mip ) e di resa di volume ( volume rendering )  . 
le analisi statistiche sono state effettuate mediante il software statistical package for the social sciences version 14.0 ( spss , chicago , illinois , usa )  . risultati dei pazienti studiati 29 / 60 ( 48 , 3% ) erano di sesso femminir . 
left hepatic artery from left gastric artery and right hepatic artery from superior mesenteric artery common hepatic artery from superior mesenteric artery common hepatic artery from left gastric artery viii anatomia normale epatica sinistra da gastrica sinistra epatica destra da arteria mesenterica superiore epatica sinistra da gastrica sinistra + epatica destra da arteria mesenterica superiore epatica sinistra acc . 
in 5% of cases , there was no common hepatic artery , and the left hepatic artery originated from the left gastric artery and the right hepatic artery from the superior mesenteric artery ( michels iv )  . 
a arteria gastrica sinistra ; b tronco spleno - epato - mesenterico ; c tronco spleno - epatico ; d arteria splenica ; e arteria epatica comune ; f arteria epatica propria ; g arteria epatica sinistra ; h arteria epatica destra ; i arteria epatica destra accessoria che origina dallarteria pancreatico - duodenale inferiore , primo ramo dellarteria mesenterica superiore . j arteria gastroduodenale ; k arteria mesenterica superiore . le e 31 / 60 ( 51 , 7% ) di sesso maschile . 
let era compresa tra i 26 e gli 80 anni ( et media 60 , 314 , 6 )  . superior mesenteric artery tronco celiaco the superior mesenteric artery arose from the aorta at l1 in il tronco celiaco nel 96 , 7% dei casi originava dallaorta r . 
nel 56 , 7% dei pazienti il tripode presentava una normale triforcazione ; nel 10% era presente unarteria epatica sinistra che originava dallarteria gastrica di sinistra ; nel 16 , 7% vi era solo larteria epatica sinistra mentre larteria epatica destra nasceva dalla mesenterica superiore ; nel 5% dei casi vi era lassenza dellepatica comune con lepatica sinistra che originava dalla gastrica sinistra e lepatica destra dallams ; nell1 , 7% stata riscontrata unarteria gastrica sinistra originare direttamente dallaorta ; nell1 , 7% si osservava la gastrica sinistra originare dallaorta e la epatica destra dalla ams ; nell1 , 7% vi era lassenza dellarteria epatica comune con lepatica sinistra che nasceva dalla colica media e lepatica destra dallarteria mesenterica superiore ; nell1 , 7% si osservava una gastrica sinistra originare dallarteria splenica ; sempre in un 1 , 7% vi era una origine separata dei vasi del tripode celiaco ; nell1 , 7% dei casi era presente unepatica sinistra accessoria che originava dalla gastrica sinistra ; infine sempre in un 1 , 7% si registrava lassenza dellarteria epatica comune con lepatica sinistra che originava dalla gastrica sinistra e lepatica destra dallarteria mesenterica superiore . arterie epatiche per quanto riguarda la variabilit delle arterie epatiche abbiamo seguito la classificazione di michels ( tabella 1 )  . larteria epatica comune risultata normale nel 60% dei casi ( michels i )  . 
le arterie pancreatico - duodenali inferiori risultavano assenti o non valutabili nel 8 , 3% , era presente un doppio tronco nel 5% , un tronco comune nel 83 , 3% , ed un unico vaso nel 3 , 3% . 
le arterie sigmoidee variavano in numero da un minimo di 1 ad un massimo di 3 con una media di 1 , 90 , 39 , nel 13 , 3% dei casi era presente una sola arteria sigmoidea , nell83 , 3% erano due , e nel 3 , 3% risultavano essere tre . 
larcata di riolano risultata valutabile nel 31 , 7% dei casi , e di questi era sviluppata nel 68 , 4% . discussione lo studio effettuato risulta uno dei primi in letteratura condotti in fase preliminare con angio - tc a 64 strati per lo studio delle variabilit anatomica del tripode celiaco , dellarteria mesenterica superiore ed inferiore , e dei loro vasi collaterali . 
il confronto tra i nostri dati e quelli presenti in letteratura presenta alcune convergenze ed alcune divergenze che necessitano di unanalisi dettagliata ( tabella 2 )  . la frequenza del tripode che origina in maniera classica dallaorta risultata leggermente pi alta rispetto alla letteratura [ 2 ] , tale risultato dovuto probabilmente al numero di pazienti non elevato ; mentre la frequenza delle anomalie riscontrate ( tronco celiaco mesenterico ed assenza del tripode ) fedele alla letteratura . 
4a - g three - dimensional volume - rendered computed tomography angiography image showing the absence of a common hepatic artery , with the right hepatic artery arising from the superior mesenteric artery and the left hepatic artery from the inferior pancreaticoduodenal artery . 
these arteries originated from the superior mesenteric arteries in 86.7% of cases , from the middle colic artery in 8.3% , from the right colic artery in 3.3% and from the arc of buhler in 1.7%. 
there were no further superior mesenteric artery collaterals . inferior mesenteric artery the inferior mesenteric artery originated from the aorta at the level of the lower third of l3 in 100% of cases . 
the sigmoid arteries ranged in number from one to three ( mean 1.90.39 ) ; there was a single sigmoid artery in 13.3% of cases , two in 83.3% , and three in 3.3%. 
the riolan arcade was assessable in 31.7% of cases and developed in 68.4%. discussion this study is one of the first preliminary studies conducted with 64 - row cta to investigate anatomical variations of the coeliac trunk and superior and inferior mesenteric arteries and their collateral vessels . 
 the incidence of coeliac trunks with a normal origin from the aorta was found to be slightly higher than reported in the literature [ 2 ] , probably as a result of the small size of our study sample . 
our findings with regard to the origin of the superior and inferior mesenteric arteries confirmed the very low incidence of abnormalities . the literature reports a higher frequency of coeliac trunks with normal anatomy and collaterals than observed in our study [ 3 ]  . 
this result may be explained by the small number of patients , as previously noted , but also by the greater sensitivity of 64 - row ct in detecting minor abnormalities , such as accessory hepatic arteries , that are more difficult to visualise on conventional angiography . 
the reported incidence of left gastric arteries originating from the aorta is 10% [ 4 ] , whereas the incidence in our study was substantially lower . the splenic artery with its collaterals was the most constant vessel to arise from the coeliac trunk . 
compared to the anatomy of the hepatic arteries reported by other angiographic or anatomical studies [ 511 ] based on the michels classification , the common hepatic artery originated normally from the coeliac trunk , with an incidence similar to that reported in the literature . 
abnormalities of the origin of the left hepatic artery ( michels ii ) had a higher prevalence than previously reported ; the prevalence of right hepatic arteries arising from the superior mesenteric artery was also higher than reported in the literature . 
the absence of the common hepatic artery , with the left hepatic artery originating from the left gastric artery and the right hepatic artery from the superior mesenteric artery ( michels iv ) , was also more common in our study than reported in the literature . 
conventional angiography is unable to depict small arteries such as accessory or aberrant hepatic arteries ( michels ii , iii and iv ) , which means that the method may underestimate the true prevalence of these vessels [ 5 ]  . 
the reason for this is that in conventional angiography , correct vessel cannulation is operator dependent , and it is technically difficult to opacify colportata in letteratura pi alta rispetto a quella del nostro studio [ 3 ] , tale risultato pu essere la conseguenza di un bias dovuto al basso numero di pazienti studiati come gi riportato ; tuttavia pu essere anche ricondotto alla maggiore sensibilit della tc a 64 strati nel rilevare le piccole anomalie , come le arterie epatiche accessorie che pi difficilmente si rilevano negli studi agiografici classici . 
dalla comparazione dellanatomia delle arterie epatiche rilevate con altri studi angiografici o anatomici [ 511 ] basati sulla classificazione di michels abbiamo rilevato che larteria epatica comune nel nostro studio origina regolarmente dal tripode celiaco , con una frequenza che concorda con la letteratura . 
le anomalie di origine dellarteria epatica sinistra ( michels ii ) , presenta una prevalenza maggiore rispetto alla media della letteratura ; anche per lepatica destra che nasce dallarteria mesenterica superiore stata riscontrata una maggiore prevalenza rispetto alla media della letteratura . 
anche lassenza dellepatica comune con lepatica sinistra che originava dalla gastrica sinistra e lepatica destra dallarteria mesenterica superiore ( michels iv ) , presentava una prevalenza maggiore nei nostri risultati rispetto alla letteratura . questa maggiore frequenza delle anomalie nel nostro studio riteniamo possa essere dovuta allalta sensibilit della metodica che permette la visualizzazione anche di vasi di piccolo calibro . 
infatti langiografia tradizionale mostra una certa difficolt nel riconoscimento di arterie di piccolo calibro come le arterie epatiche accessorie o aberranti ( michels ii , iii e iv ) e quindi tale metodica pu sottostimare la reale prevalenza di questi vasi [ 5 ]  . 
questo da ricondursi al fatto che nellangiografia tradizionale il corretto incannulamento dei vasi risulta operatore dipendente , con una certa difficolt tecnica nellopacizzazione dei rami collaterali a bassa portata ematica . 
viceversa la nostra serie si dimostrata pi efficace nel riconoscimento di tali tronchi grazie alla risoluzione spaziale submillimetrica della tc a 64 strati ed alla tecnica del bolus tracking , che rende possibile un perfetto timing nellopacizzazione dei vasi . 
non sono state rilevate anomalie dei tipi vi , vii , ix e x mentre in letteratura riportata una prevalenza media rispettivamente di 3 , 1%2 , 2% , 0 , 4%0 , 4% , 2 , 7%1 , 2% e 0 , 07%0 , 2% . 
come il nostro studio , anche altri lavori mostrano una elevata prevalenza di casi non classificati ; riteniamo che questo sia sempre da ricondurre allalta sensibilit della metodica da noi utilizzata . 
inoltre da sottolineare come in tutti gli studi analizzati nessuno riporti la presenza dellanomalia tipo x di michels ( epatica comune da gastrica sinistra ) , questo ci porta a concludere che a fronte dei notevoli sviluppi r . 
in contrast , recognition of these vessels was more effective in our series as a result of the submillimetre spatial resolution of 64 - row ct and the bolus tracking technique , which allows perfect timing for vessel opacification . 
this leads us to think that , given the developments in vascular imaging that enable dellimaging vascolare che permette oramai la visualizzazione pressoch di tutti i vasi addominali , sarebbe forse il momento di aggiornare la classificazione di michels inserendo anche quei casi non riportati da lui , ma che presentano una discreta frequenza , come per esempio lepatica comune che nasce direttamente dallaorta o lepatica sinistra dalla colica media . 
tali anomalie non classificate risultano , daltra parte di fondamentale importanza per una corretta programmazione chirurgica . per quanto riguarda larteria mesenterica inferiore , non stata riscontrata nessuna arteria di testut , riteniamo a causa del ridotto numero di pazienti visto che la sua presenza in letteratura riportata solo aneddotticamente senza una precisa percentuale [ 12 ]  . le arterie pancreatico - duodenali inferiori sono risultati i tronchi pi difficili da valutare . 
these unclassified anomalies are fundamental for correct surgical planning . as regards the inferior mesenteric artery , we found no case of testut artery , possibly because of the small study sample , given that its presence has only been reported anecdotally without precise percentages [ 12 ]  . the inferior pancreaticoduodenal arteries proved to be the most difficult to evaluate . 
our findings were in agreement with previous series as regards the manner of origin of these arteries ( single trunk , double trunk [ 13 , 14 ] , single anterior branch [ 15 ] , not assessable or absent )  . 
our data on the origin of the inferior pancreaticoduodenal arteries indicate a higher frequency of abnormalities compared with previous studies , in which the frequency of their origin from the superior mesenteric arteries ranges from 1.8% to 50% depending on the method used , with higher rates with imaging than with autopsy studies [ 16 ]  . 
the frequency of the presence of the arc of buhler , which courses between the superior mesenteric artery and the coeliac trunk and between the superior mesenteric artery and the splenic artery , was similar to that reported in the literature [ 17 ]  . the number of jejunal and ileal arteries was lower than that reported in the literature [ 18 , 19 ]  . 
on ct , it is impossible to distinguish clearly the upper and lower group , as one cannot infer when the superior mesenteric artery enters the root of the mesentery . this subdivision was made arbitrarily by assuming that the presence of a greater distance than observed between the first arteries marked the transition from the upper to the lower group . 
the origin of the right colic artery from the superior mesenteric artery was substantially more frequent compared with that reported in the literature ( 10.7% of cases ) [ 20 ]  . 
the middle colic artery was visualised with a high frequency in our study compared with other studies , where it was reported to be extremely variable ( from 36% to 98% ) [ 21 , 22 ] , with evidence of the middle colic artery arising from the right colic artery in 53% of cases [ 23 ]  . even this highly discordant finding may be due to the small number of patients studied . we found no collaterals to the superior mesenteric artery . among the collaterals to the inferior mesenteric artery , the left colic artery was always present . 
i dati riscontrati riferiti alle anomalie di origine delle arterie pancreatico - duodenali inferiori mostrano una frequenza superiore rispetto alla letteratura in cui la nascita dallarteria mesenterica superiore varia dall1 , 8% al 50% a seconda delle metodiche usate , con valori pi elevati per quelle radiologiche rispetto alle dissezioni [ 16 ]  . 
lorigine delle arterie pancreatico - duodenali inferiori dalla colica media e dalla colica destra in letteratura viene considerata aneddottica mentre nel nostro caso si riscontrata con una frequenza relativamente alta ( 3 , 3%8 , 3% )  . 
la frequenza della presenza dellarco di buhler , il cui decorso stato identificato tra larteria mesenterica superiore ed il tripode celiaco e tra lams e larteria splenica , risultata paragonabile a quella presente in letteratura [ 17 ]  . il numero delle arterie digiuno - ileali risultato inferiore a quello riportato in letteratura [ 18 , 19 ] : riteniamo che ci sia dovuto al fatto che i piccoli rami terminali che irrorano la parte finale dellileo possano essere misconosciuti a causa della sovrapposizione della arcate ileali . 
allesame tc non possibile dividere in maniera esatta il gruppo superiore dallinferiore visto che non si pu dedurre quando larteria mesenterica superiore entra nella radice del mesentere . tale suddivisione stata effettuata in maniera arbitraria assumendo che la presenza di una distanza maggiore di quella osservata tra le prime arterie segnasse il passaggio dal gruppo superiore a quello inferiore . 
langio - tc ha dimostrato di poter rilevare anche i piccoli rami delle arterie digiunoileali arrivando a visualizzare anche la seconda serie di arcate intestinali . larteria ileocolica e la colica destra si sono mostrate estremamente costanti ( 100% dei casi )  . 
lorigine della colica destra dalla mesenterica superiore risulta con una frequenza sensibilmente superiore rispetto alla letteratura ove si riscontra solo nel 10 , 7% dei casi [ 20 ]  . 
larteria colica media stata rilevata con unalta frequenza nel nostro studio rispetto alla letteratura ove la sua presenza risulta estremamente variabile a seconda degli studi eseguiti ( tra il 36% al 98% ) [ 21 , 22 ] con evidenza nel 53% dei casi della nascita dellarteria colica media dalla colica destra [ 23 ]  . 
il numero delle arterie sigmoidee ( da minimo di 1 ad un massimo di 3 nella nostra esperienza ) , come gi riportato in letteratura , correlato alla lunghezza e mobilit del sigma . il dato sulla presenza e sviluppo dellarcata di riolano risulta compatibile con i dati in letteratura , ove riportata unampia variabilit di questo collaterale ( dal 9 , 6% al 99 , 97% ) [ 24 , 25 ] .una precisa conoscenza della sua prevalenza fondamentale , soprattutto in ambito chirurgico . come gi riportato durante la discussione , bisogna sottolineare come i dati rilevati vadano interpretati tenendo anche presente i limiti del nostro studio : in primo luogo il relar . 
 as stated , our data should be interpreted within the limitations of the study : first , the relatively small number of patients studied , which might affect the statistical frequency of given abnormalities ; and second , the lack of a direct correlation with a diagnostic reference standard such as conventional angiography . conclusions sixty - four - row cta is superior to conventional angiography in terms of diagnostic accuracy , safety , patient compliance and examination time . 
our study demonstrates that the new 64 - row ct scanners have reached a high definition in the study of mesenteric vessels , in part thanks to bolus tracking techniques , allowing the visualisation of small vessels and accessory arteries that are difficult to identify with other methods . our findings indicate a larger number of vascular abnormalities than reported in the literature with other modalities . if confirmed , this result would call for a review of the old classifications , such as the michels classification for the hepatic arteries , which although still in use , underestimate the real prevalence of aberrant vessels . 
similarly , we found abnormalities not contained in the michels classification , such as the right hepatic artery originating from the right or middle colic artery . besides replacing conventional angiography in vascular imaging , 64 - row cta also represents an innovation in surgical planning . 
the possibility of performing three - dimensional reconstructions that provide the surgeon with a detailed map of the abdominal vasculature reduces the risk of iatrogenic injuries or ischaemia caused by the ligation of aberrant vascular trunks . our study demonstrated that 64 - row cta can assess the calibre of anastomotic circulations , such as the riolan arcade and the arc of buhler , and therefore be used to evaluate the possibility of using these vessels for intestinal anastomoses . 
 in conclusion , 64 - row cta not only offers substantial advantages in the field of vascular imaging but also promises important developments in anatomical knowledge and surgical planning , becoming the first - line noninvasive modality for the study of abdominal vessels . tivamente basso numero di pazienti studiati , che potrebbe influenzare la frequenza statistica di determinate anomalie riportate ed in secondo luogo , la mancanza di confronto diretto con tecniche diagnostiche standard di riferimento come langiografia tradizionale . conclusioni langio - tc a 64 strati risulta essere una metodica che per adeguatezza diagnostica , sicurezza , compliance per il paziente e velocit di esecuzione risulta superiore allangiografia convenzionale . 
il nostro lavoro dimostra lalta definizione raggiunta dalle nuove tc a 64 strati nello studio dei vasi mesenterici , grazie anche alle metodiche di bolus tracking , permettendo di visualizzare piccoli vasi ed arterie accessorie , difficilmente identificabili con altre metodiche . nel nostro studio stato rilevato un numero di anomalie vascolari pi alto di quello riportato in letteratura con altre metodiche ; tale risultato se confermato renderebbe addirittura necessario aggiornare le vecchie classificazioni , come quella di michels sulle arterie epatiche , utilizzate fino ad ora , in cui presente una sottostima della reale frequenza dei vasi aberranti . 
del maschio1 1department of radiology , 2department of surgery , 3department of gastroenterology , 4department of pathology , vita - salute university , san raffaele hospital , via olgettina 60 , i - 20132 , milan , italy correspondence to : s . 
twenty - nine endocrine pancreatic lesions with definitive morphological and immunohistochemical characterisation after surgical treatment ( n = 24 ) or fine - needleaspiration cytology under endoscopic ultrasonography guidance ( n = 5 ) were retrospectively evaluated . 
endocrine tumour and normal pancreas attenuation and the mean absolute tumour - to - gland attenuation difference were measured in each phase , and data were analysed with students t test . 
in our experience , the pancreatic phase can replace the arterial phase in the evaluation of pancreatic endocrine tumours . key words pancreas spiral computed tomography endocrine system neoplasms riassunto obiettivo . 
sono state valutate retrospettivamente 29 lesioni endocrine pancreatiche , con diagnosi definitiva alla valutazione morfologica e immuno - istochimica , dopo trattamento chirurgico ( n = 24 ) o prelievo citologico sotto guida ecoendoscopica ( n = 5 )  . 
le immagini ottenute in ciascuna fase sono state interpretate da due radiologi , esperti in patologia pancreatica , alloscuro delle diagnosi definitive , valutando le densit di ghiandola pancreatica e tumore e la differenza di attenuazione tumore - ghiandola in valore assoluto , in ogni fase ; i dati ottenuti sono stati analizzati con il test t di student . 
per entrambi i radiologi il valore assoluto della differenza di attenuazione tumore - ghiandola in fase pancreatica ( 4053 hu e 3456 hu ) risultata significativamente maggiore ( p < 0 , 05 ) di quella ottenuta in fase arteriosa ( 3138 hu e 2643 hu )  . 
sct has variable sensitivity ( 47%72% ) [ 13 ] in the detection of endocrine pancreatic tumours , and this sensitivity significantly decreases in the evaluation of small ( < 2 cm ) lesions ( 12% ) [ 2 ]  . 
most of them [ 46 ] have used 4or 8 - row ct scanners and analysed a limited number of lesions and mostly a specific subtype of endocrine tumours ( insulinomas ) , or they have evaluated endocrine lesions together with pancreatic or periampullary tumours [ 7 , 8 ]  . 
 the dual - phase technique , with a pancreatic and portal phase , has been reported [ 1013 ] to be the best choice for detection and staging of pancreatic ductal adenocarcinoma with both sct and mdct . 
in the assessment of pancreatic endocrine tumours , especially insulinomas , the dual - phase ct technique has mostly been reported [ 1 , 4 , 5 , 1416 ]  . 
with mdct , the reported biphasic technique consists of either an early or late arterial phase [ 4 , 14 ] followed by a portal phase [ 4 ]  . 
it has been reported that the pancreatic phase may replace the arterial phase in insulinoma protocols , but further studies have been advocated to asses this issue [ 4 ]  . 
a recent paper has reported on the use of a dual - phase technique with an arterial phase ( at 25 s ) and an early portal phase ( at 5560 s ) , stating that pancreatic endocrine tumours , especially small ones , are better detected during the arterial phase of enhancement [ 9 ] , but the number of patients included in the study was not indicated . the aim of our study was to assess whether the pancreatic phase may replace the arterial phase in the evaluation of endocrine pancreatic tumours , as suggested in the literature [ 4 ] and already accepted for pancreatic adenocarcinomas [ 1013 ] using a 16 - row ct scanner with triple - phase technique . materials and methods patients we retrospectively analysed the ct examinations of 23 patients with a definitive diagnosis of pancreatic endocrine tumour . 
the patients underwent surgical resection ( n = 20 ) or fine - needle - aspiration cytology ( fnac ) with endoscopic ultrasonography ( eus ) guidance ( n = 3 ) , which led to a definitive diagnosis of pancreatic endocrine tumour . 
 a total of 29 lesions were identified ; six patients had multifocal disease ( two lesions per patient ) and two were affect1000 il valore della tomografia spirale computerizzata ( sct ) nella valutazione dei tumori endocrini pancreatici gi stato riportato in vari studi [ 18 ] ; la sensibilit di questa metodica nella ricerca delle lesioni endocrine pancreatiche variabile ( range 47%72% ) [ 13 ] , con una significativa riduzione ( 12% ) nella valutazione di lesioni di piccolo diametro ( < 2 cm ) [ 2 ]  . 
la maggior parte di questi studi [ 46 ] utilizza una tecnologia a 4 o 8 detettori e si occupano di un numero limitato di lesioni , soprattutto di insulinomi , ossia solo di una specifica categoria di tumori endocrini , o analizzano le lesioni endocrine con altri tumori pancreatici o periampollari [ 7 , 8 ]  . 
la pubblicazione pi recente , che tratta specificamente i tumori endocrini pancreatici , un education exhibit in cui viene utilizzato uno scanner a 64 detettori [ 9 ]  . la tecnica bifasica , con acquisizione delle immagini in fase pancreatica e portale , considerata [ 1013 ] la scelta migliore per lidentificazione e la stadiazione delladenocarcinoma duttale , sia in sct che in mdtc . 
considerando la mdct la tecnica bifasica descritta consiste in una fase arteriosa , alternativamente precoce o tardiva [ 4 , 14 ] , seguita da una fase portale [ 4 ]  . 
la tecnica trifasica di acquisizione ( con fase arteriosa , pancreatica e portale ) stata utilizzata solo in pochi pazienti [ 4 , 6 ] ; in letteratura stato riportato come la fase pancreatica possa sostituire la fase arteriosa nei protocolli di studio degli insulinomi , ma questa ipotesi necessita di essere confermata in ulteriori studi [ 4 ]  . 
un recente lavoro afferma che , utilizzando la tecnica bifasica con fase arteriosa ( a 1520 secondi ) e portale precoce ( 5560 secondi ) , le lesioni endocrine pancreatiche siano meglio identificabili in fase arteriosa , specie quelle di piccole dimensioni , ma non viene specificato il numero di pazienti reclutati nello studio [ 9 ]  . scopo di questo studio determinare se la fase pancreatica possa sostituire la fase arteriosa nella valutazione delle lesioni endocrine pancreatiche , come suggerito in letteratura [ 4 ] e gi accettato per ladenocarcinoma pancreatico [ 1013 ] , utilizzando uno scanner a 16 detettori e la tecnica di studio trifasica . materiali e metodi pazienti sono state retrospettivamente analizzate indagini tc di 23 pazienti con diagnosi definitiva di tumore endocrino pancreatico ; tutti gli esami tc sono stati effettuati dal dicembre 2004 allagosto 2006 presso la nostra unit operativa di radiologia . 
ten of 23 patients ( 44% ) had functioning pancreatic endocrine tumours with the typical symptoms of a hormone - secreting lesion : hypoglycaemia ( n = 7 ) , skin rash ( n = 1 ) , cushings syndrome ( n = 1 ) and diarrhoea and dehydration ( n = 1 )  . 
six had nonspecific symptoms ( 26% ) : mesogastric pain ( n = 4 ) and left upper abdominal pain ( n = 2 )  . the remaining seven patients ( 30% ) were asymptomatic , and the pancreatic mass was detected during sonographic evaluation performed for annual follow - up of gallbladder ( n = 3 ) and kidney stones ( n = 4 )  . 
 histological evaluation our series was composed of 24 histological specimens obtained at surgery and five cytological specimens obtained by eus - guided fnac ; the 24 histological specimens were analysed according to the world health organization ( who ) criteria [ 17 ]  . 
the results of morphological and immunohistochemical evaluation and correlation with symptoms are shown in table 1 . mdct technique all examinations were conducted with a 16 - row ct scanner ( aquilion 16 , toshiba , tokyo , japan )  . 
for the unenhanced acquisition , a scan from the top of the liver to the aortic bifurcation was performed with the following parameters : kv 120 ; ma 250 ; gantry rotation time 0.5 s ; hp 15.0 ; beam pitch 0.9 ; couch speed 30 mm / rotation ; acquisition thickness 2 mm ; reconstruction index 2 m the triple - phase technique consists of an acquisition during the arterial , pancreatic and portal phases . 
for contrast administration , a 20 - gauge plastic intravenous catheter was placed in an antecubital vein , and the line was connected to a power injector ( stellant d , medrad inc . , indianola , ia < usa )  . 
a total of 2 ml / kg of body weight of low osmolarity iopamidol ( ultravist 370 , schering ag , berlin , germany ) , ordinarily used for thorax and abdominal ct at our institution , was administered at a rate of 3.64.0 ml / s , followed by 30 ml of normal saline solution at the same rate ( stellant d , medrad inc . , indianola , usa )  . the parameters of the triple - phase acquisition were : kv 120 ; ma 250 ; gantry rotation time 0.5 s ; hp 15.0 ; beam pitch 0.9 ; couch speed 30 mm / rotation ; acquisition thickness 1 mm ; reconstruction index 0.8 mscan extension was the same as for unenhanced scans . 
if a study of the thorax and abdomen was required , the portal scan started from the apex of the lungs and extended to the pelvis . to define the correct timing of the arterial phase , a bolusgendo ad una diagnosi definitiva di tumore endocrino del pancreas . sono state quindi identificate 29 lesioni ; in 6 pazienti stata osservata una malattia multifocale ( 2 lesioni per paziente ) e 2 di essi erano affetti da neoplasie endocrine multiple tipo i ( men - 1 )  . 
dieci / 23 ( 44% ) pazienti erano affetti da tumori endocrini pancreatici funzionanti e presentavano sintomi tipici correlati allipersecrezione ormonale : ipoglicemia ( n = 7 ) ; rush cutaneo ( n = 1 ) ; sindrome di cushing ( n = 1 ) ; diarrea e disidratazione ( n = 1 )  . 
tredici / 23 ( 56% ) pazienti erano affetti da tumori endocrini pancreatici non funzionanti ; 6 pazienti ( 26% ) presentavano sintomi aspecifici : dolore in mesogastrio ( n = 4 ) , dolore in epigastrio ( n = 2 )  . 
gli altri 7 pazienti ( 30% ) erano asintomatici e la masse pancreatiche erano state rilevate durante una valutazione ecografica effettuata per un controllo annuale di colelitiasi ( n = 3 ) e per valutazione di calcoli renali ( n = 4 )  . 
il consenso informato stato ottenuto in tutti i 23 pazienti prima di sottoporsi a indagine tc multidetettore con tecnica trifasica , secondo un protocollo approvato dal comitato etico del nostro istituto . valutazione istologica i nostri reperti erano composti da 24 campioni istologici , ottenuti da trattamento chirurgico e da 5 campioni citologici ottenuti mediante agoaspirato sotto guida ecoendoscopica ; i reperti istologici sono stati analizzati secondo i criteri who del 2000 [ 17 ]  . 
i risultati della valutazione morfologica ed immuno - istochimica e la correlazione con i sintomi sono presentati nella tabella 1 . tecnica di acquisizione mdct tutte le 29 lesioni sono state studiate con mdct a 16 detettori ( aquilion 16 , toshiba , tokyo , giappone )  . 
nei 30 minuti prima dellesame sono stati somministrati per via orale 7501000 ml di acqua ; stata quindi effettuata una scansione senza mezzo di contrasto , seguita da una acquisizione trifasica . 
nellacquisizione senza mezzo di contrasto si effettuata una scansione dallapice del fegato sino alla biforcazione aortica con i seguenti parametri : 120 kv , 250 ma , gantry rotation time : 0 , 5 s , spessore di acquisizione 2 mm16 file di detettori , helical pitch ( hp ) : 15 , 0 , beam pitch : 0 , 9 , velocit del tavolo 30 mm / rotazione , spessore di ricostruzione : 2 mm , con intervallo di ricostruzione di 2 mm . la tecnica trifasica consiste in acquisizioni in fase arteriosa , fase pancreatica e portale . 
per linfusione ev di mdc stato utilizzato un accesso venoso periferico del calibro di 20 gauge , posizionato a livello della superficie volare dellavambraccio o del gomito ; stato somministrato un totale di 2 ml / kg di peso corporeo di iopamidolo ( ultravist 370 , schering ag , berlin , germania ) , routinariamente utilizzato per indagini tc torace e addome nel nostro istituto , seguito da 30 ml di soluzione fisiologica ; entrambe le infusioni sono state eseguite con un flusso di 3 , 64 , 0 ml / s grazie a un iniettore automatico a doppia siringa ( stellant d , medrad inc . , indianola , usa )  . i parametri dellacquisizione trifasica erano : 120 kv , 250 ma , rotation time : 0 , 5 s , spessore di acquisizione : 1 mm16 1001 s . 
nei casi in cui era richiesto uno studio di torace e addome , la scansione portale iniziava dellapice del polmone e si estendeva sino alla pelvi . per stabilire il timing corretto della fase arteriosa , stata utilizzata la tecnica del bolus tracking . 
la regione di interesse ( roi ) stata posizionata a livello dellaorta addominale , allaltezza di piani passanti per lorigine del tronco celiaco ; stato definito il valore di densit da raggiungere per la partenza automatica dellacquisizione in fase arteriosa aggiungendo 70 hu alla densit basale in aorta . 
le fasi pancreatiche e portali sono state iniziate , rispettivamente , 45 e 70 secondi dopo liniezione del mezzo di contrasto , circa 25 e 50 secondi dopo la fase arteriosa , secondo quanto riportato in letteratura [ 13 ]  . interpretazione delle immagini le immagini ottenute durante ciascuna fase sono state internonfunctioning tumours well - differentiated endocrine tumour with benign behaviour well - differentiated endocrine carcinoma well - differentiated endocrine tumour well - differentiated endocrine tumour with benign behaviour well - differentiated endocrine tumour well - differentiated endocrine tumour well - differentiated endocrine tumour with benign behaviour well - differentiated endocrine tumour with benign behaviour well - differentiated endocrine tumour with uncertain behaviour well - differentiated endocrine tumour with uncertain behaviour well - differentiated endocrine carcinoma well - differentiated endocrine carcinoma poorly differentiated endocrine carcinomapan - in2 poorly differentiated endocrine carcinomapan - in2 poorly differentiated endocrine carcinoma poorly differentiated endocrine carcinoma well - differentiated endocrine carcinoma well - differentiated endocrine tumour with uncertain behaviour pan - in2 , pancreatic intraephitelial heoplasia type 2 tracking technique was used : a region of interest ( roi ) was positioned on the abdominal aorta , near the origin of the coeliac trunk , and the scan was triggered at the threshold aortic attenuation ( 70 hu above baseline )  . 
the pancreatic and portal phases started 45 and 70 s , respectively , after the start of the injection of contrast medium , about 25 and 50 s , respectively , after the arterial phase , as suggested in the literature [ 13 ]  . image interpretation images obtained during each phase were interpreted separately by two senior radiologists experienced in pancreatic pathology and who were blinded to the histopathological results . 
in addition , the arterial and pancreatic phase images were assessed for the presence of arterial variation and hypervascular liver metastases . postprocessing was performed using 2d ( multiplanar reconstructions ) and 3d ( maximum intensity projection ) reconstructions to demonstrate the pancreatic pertinence of possible exophytic lesions and evaluate the presence or ab1002 s . 
surgical treatment was considered the gold standard in the evaluation of vascular involvement and arterial variations . the endocrine pancreatic tumours included in our study were divided into three groups on the basis of their size : group a ( diameter 2 cm ) , group b ( diameter from 2 to 4 cm ) , group c ( diameter 4 cm )  . 
attenuation of the normal pancreatic parenchyma and the tumour , expressed in hounsfield units , in all phases ( unenhanced , arterial , pancreatic and portal ) was measured using a circular roi . 
essi hanno analizzato le immagini ottenute in tutte le fasi su work station dedicata ( vitrea2 , vital images inc . , minnetonka , minnesota , usa ) , rilevando la presenza di lesioni pancreatiche focali e definendo le loro dimensioni e il tipo di pattern contrastografico tumorale ( ipervascolare , ipovascolare o eterogeneo )  . 
inoltre hanno valutato la presenza di anomalie vascolari arteriose e di metastasi epatiche nella fasi arteriosa e pancreatica . il post - processing stato effettuato attraverso luso di ricostruzioni 2d ( ricostruzioni multiplanari : mpr ) e 3d ( maximum intensity projection : mip ) , per dimostrare la pertinenza pancreatica di eventuali lesioni esofitiche e per valutare la presenza eventuale di coinvolgimento vascolare , secondo i criteri espressi in letteratura [ 18 , 19 ] e di eventuali anomalie vascolari arteriose . 
comparison of attenuation differences between the tumour and normal pancreas in different phases of contrast enhancement and of the mean absolute tumour - to - gland attenuation difference in the arterial , pancreatic and portal phases were performed with the paired students t test . 
finally , a statistical analysis of the mean absolute tumour - to - gland attenuation difference in the arterial and pancreatic phases was performed in hypervascular lesions only and in group a lesions ( diameter 2 cm ) only . results all mdct examinations were of diagnostic quality , and all pancreatic lesions were detected on both the arterial and pancreatic phases . 
stata misurata lattenuazione del tumore e del pancreas normale , espressa in hu , in tutte le fasi effettuate ( basale , arteriosa , pancreatica e portale ) , utilizzando una roi circolare . 
le regioni di interesse sono state accuratamente posizionate allinterno dei margini dellintera lesione ; nel caso in cui la lesione fosse disomogenea , le regioni di interesse sono state collocate in modo da includere lintera lesione , senza escludere le componenti tumorali dotate di diversi valori di attenuazione tc . 
quindi stata misurata la differenza media di attenuazione tumore - ghiandola , espressa in valore assoluto , nelle fasi arteriosa , pancreatica e portale . stato analizzato il contributo delle fasi arteriosa e pancreatica alla confidenza diagnostica di ciascun radiologo nel riconoscere le lesioni pancreatiche ipero ipovascolari , le lesioni eterogenee , le anomalie vascolari arteriose e le metastasi ipervascolari epatiche ; stato utilizzato uno schema valutativo basato su una scala di 4 punti che riflettono lapporto soggettivo di ogni fase alla confidenza diagnostica ( 3 = contributo elevato , 2 = contributo medio , 1 = contributo basso , 0 = nessun contributo )  . analisi statistica i dati , distribuiti secondo una normale continua , sono stati presentati come media deviazione standard ( sd )  . 
i confronti tra le differenze di attenuazione tra il tumore e il pancreas normale nelle diverse fasi e tra le differenze medie assolute di attenuazione tumore - ghiandola nelle fasi arteriose , pancreatiche e portali sono stati effettuati con il test t di student . 
i dati registrati da ciascun radiologo sono stati analizzati separatamente e quindi i dati raccolti da entrambi i radiologi sono stati infine confrontati per valutare la concordanza diagnostica , in particolare per valutare leventuale presenza di una differenza significativa tra i 2 osservatori . 
infine lanalisi statistica stata effettuata considerando il valore assoluto della differenza di attenuazione media tra tumore e ghiandola pancreatica , in fase arteriosa e pancreatica , nelle sole lesioni ipervascolari e nelle sole lesioni di gruppo a ( diametro 2 cm )  . risultati tutte le indagini tc erano di qualit diagnostica e tutte le lesioni pancreatiche sono state rilevate in entrambe le fasi , arteriosa e pancreatica . 
il diametro medio delle lesioni pancreatiche era 36 , 8 mm ( range : 898 mm ) ; esse erano localizzate a livello del processo uncinato ( n = 5 ) , a livello della testa ( n = 8 ) , a livello del corpo ( n = 8 ) e a livello della coda ( n = 8 ) pancreatici . 
1a - d transverse computed tomography images in a 63 - year - old woman with hypervascular , insulin - secreting , well - differentiated endocrine tumour with benign behaviour in pancreatic tail ( arrow )  . 
a image of the tumour obtained in the unenhanced phase , with tumour - to - gland attenuation difference of 5 hu for the first observer and 1 hu for the second . 
b image of tumour obtained in the arterial phase , with tumour - to - gland attenuation difference of 52 hu for the first observer and 46 hu for the second . 
c image of tumour obtained in the pancreatic phase , with tumour - to - gland attenuation difference of 89 hu for the first observer and 85 hu for the second . 
1a - d immagini tc assiali in una donna di 63 anni affetta da un tumore endocrino ipervascolare ben differenziato secernente insulina con comportamento benigno nella coda pancreatica ( freccia )  . 
a immagine del tumore ottenuta nellacquisizione senza mezzo di contrasto , con una differenza di attenuazione tumore vs ghiandola di 5 hu per il primo osservatore e 1 hu per il secondo . 
b immagine del tumore ottenuta nella fase arteriosa , con una differenza di attenuazione tumore vs ghiandola di 52 hu per il primo osservatore e 46 hu per il secondo . 
c immagine del tumore ottenuta nella fase pancreatica , con una differenza di attenuazione tumore vs ghiandola di 89 hu per il primo osservatore e 85 hu per il secondo . 
d immagine del tumore ottenuta nella fase portale , con una differenza di attenuazione tumore vs ghiandola di 43 hu per il primo osservatore e 34 hu per il secondo . diameter was 21 ( range 762 ) m no hypovascular liver metastases were identified . 
a image of the tumour obtained in the unenhanced phase , with tumour - to - gland attenuation difference of 0 hu for the first observer and 12 hu for the second . 
b image of tumour obtained in the arterial phase , with tumour - to - gland attenuation difference of 41 hu for the first observer and 53 hu for the second . 
c image of the tumour obtained in the pancreatic phase , with tumour - to - gland attenuation difference of 46 hu for the first observer and 50 hu for the second . 
d image of the tumour obtained in the pancreatic phase , with tumour - to - gland attenuation difference of 8 hu for the first observer and 10 hu for the second . 
2a - e immagini assiali e ricostruzione coronale in una donna di 32 anni affetta da un tumore endocrino ipovascolare ben differenziato secernente insulina con comportamento incerto a livello del passaggio corpo - coda pancreatico ( freccia )  . 
a immagine del tumore ottenuta nellacquisizione senza mezzo di contrasto , con una differenza di attenuazione tumore vs ghiandola di 0 hu per il primo osservatore e 12 hu per il secondo . 
b immagine del tumore ottenuta nella fase arteriosa , con una differenza di attenuazione tumore vs ghiandola di 41 hu per il primo osservatore e 53 hu per il secondo . 
c immagine del tumore ottenuta nella fase pancreatica , con una differenza di attenuazione tumore vs ghiandola di 46 hu per il primo osservatore e 50 hu per il secondo . 
d immagine del tumore ottenuta nella fase portale , con una differenza di attenuazione tumore vs ghiandola di 8 hu per il primo osservatore e 10 hu per il secondo . 
e la ricostruzione coronale mostra lorigine di questo tumore dal passaggio corpo - coda pancreatico . mente un coinvolgimento vascolare , confermato dallesplorazione chirurgica , in 5 pazienti : infiltrazione dellarteria e della vena splenica ( n = 1 ) , della vena splenica ( n = 1 ) , della vena mesenterica superiore ( n = 1 ) , della vena porta ( n = 1 ) ; ( 20% ) hypervascular , none hypovascular , four ( 80% ) heterogeneous . data obtained on the attenuation of normal pancreas and endocrine tumour by both radiologists are shown in table 2 . for the first observer , mean absolute tumour - to - gland attenuation was greatest on images obtained in the pancreatic ( 4053 hu ; p < 0.001 ) and arterial ( 3138 hu ; p = 0.02 ) phase when each of these values was compared with that in the portal phase ( 26 hu29 )  . 
3a - d transverse computed tomography images in a 40 - year - old woman with heterogeneous vasoactive - intestinal - peptide - secreting , well - differentiated endocrine tumour with uncertain behaviour in the pancreatic uncinate process ( arrow )  . 
a image of the tumour obtained in the unenhanced phase , with tumourto - gland attenuation difference of 3 hu for the first observer and 29 hu for the second . 
b image of the tumour obtained in the arterial phase , with tumour - togland attenuation difference of 67 hu for the first observer and 89 hu for the second . 
c image of the tumour obtained in the pancreatic phase , with tumourto - gland attenuation difference of 100 hu for the first observer and 115 hu for the second . 
3a - d immagini assiali in una donna di 40 anni affetta da un tumore endocrino disomogeneo ben differenziato secernente vip con comportamento incerto nel processo uncinato ( freccia )  . 
a immagine del tumore ottenuta nellacquizione senza mezzo di contrasto , con una differenza di attenuazione tumore vs ghiandola di 3 hu per il primo osservatore e 29 hu per il secondo . 
b immagine del tumore ottenuta nella fase arteriosa , con una differenza di attenuazione tumore vs ghiandola di 67 hu per il primo osservatore e 89 hu per il secondo . 
c immagine del tumore ottenuta nella fase pancreatica , con una differenza di attenuazione tumore vs ghiandola di 100 hu per il primo osservatore e 115 hu per il secondo . 
d immagine del tumore ottenuta nella fase portale , con una differenza di attenuazione tumore vs ghiandola di 74 hu per il primo osservatore e 74 hu per il secondo . gland attenuation was greatest on images obtained in the pancreatic phase ( 3456 hu ; p < 0.001 ) when compared with that in the portal phase ( 2640 hu )  . 
il numero medio di metastasi ipervascolari era 11 ( range 221 ) , localizzate sia nel lobo destro sia nel lobo sinistro ; il loro diametro medio era 21 mm ( range 762 mm )  . 
le anomalie vascolari arteriose e le metastasi epatiche ipervascolari sono stati rilevati da entrambi i radiologi , sia in fase arteriosa che in fase pancreatica , senza differenze . sono state rilevate anomalie vascolari arteriose in 6 pazienti ( 26% ) : in 1 caso larteria epatica originava dallarte1007 s . 
4a - d transverse computed tomography images in a 51 - year - old man with heterogeneous , glucagons - secreting , well - differentiated endocrine carcinoma in the pancreatic body ( arrow ) with hypervascular liver metastases . 
a image of the tumour obtained in the unenhanced phase , with tumour - to - gland attenuation difference of 16 hu for the first observer and 18 hu for the second . b image of the tumour obtained in the arterial phase , with tumour - to - gland attenuation difference of 42 hu for the first observer and 35 hu for the second . 
4a - d immagini assiali in un uomo di 51 anni affetto da un carcinoma endocrino disomogeneo ben differenziato secernente glucagone nel corpo del pancreas ( freccia ) con metastasi epatiche ipervascolari . 
a immagine del tumore ottenuta nellacquisizione senza mezzo di contrasto , con una differenza di attenuazione tumore vs ghiandola di 16 hu per il primo osservatore e 18 hu per il secondo . 
b immagine del tumore ottenuta nella fase arteriosa , con una differenza di attenuazione tumore vs ghiandola di 42 hu per il primo osservatore e 35 hu per il secondo . 
c immagine del tumore ottenuta nella fase pancreatica , con una differenza di attenuazione tumore vs ghiandola di 77 hu per il primo osservatore e 85 hu per il secondo . 
questi reperti sono stati confermati allesplorazione chirurgica . tredici lesioni erano incluse nel gruppo a : 11 ( 85% ) erano ipervascolari , 2 ( 15% ) ipovascolari , nessuna era disomogenea . 
cinque lesioni erano incluse nel gruppo c : 1 ( 20% ) era ipervascolare , nessuna era ipovascolare , 4 ( 80% ) erano disomogenee . i dati ottenuti da entrambi i radiologi , analizzando latte1008 s . 
analizzando i dati del primo osservatore , il valore assoluto medio della differenza di attenuazione tra la lesione e il pancreas sano era maggiore nelle immagini ottenute nella fase pancreatica ( 4053 hu ; p < 0 , 001 ) e nella fase arteriosa ( 3138 hu ; p < 0 , 02 ) , quando ciascuno di questi valori era confrontato con quello della fase portale ( 26 hu29 )  . 
era presente una differenza statisticamente significativa ( p = 0 , 02 ) tra i valori assoluti medi di differenza di attenuazione tra la lesione e il pancreas sano nella fase arteriosa e pancreatica . 
per il secondo osservatore , il valore assoluto medio della differenza di attenuazione tra la lesione e il pancreas era maggiore nelle immagini ottenute nella fase pancreatica ( 3456 hu ; p < 0 , 001 ) , quando confrontato con quello in fase portale ( 2640 hu )  . 
non cera una differenza statisticamente significativa ( p = 0 , 086 ) tra il valore assoluto medio della differenza di attenuazione tra la lesione e il pancreas sano in fase arteriosa ( 2643 hu ) e quello in fase portale . 
anche in questo caso , stata trovata una differenza statisticamente significativa ( p = 0 , 001 ) tra i valori assoluti medi di differenza di attenuazione tra la lesione e il pancreas sano in fase arteriosa e pancreatica . 
non cera una differenza statisticamente significativa nei dati espressi da ciascun radiologo ( media p = 0 , 4 , range : 0 , 1670 , 991 )  . per il primo radiologo il valore assoluto medio della differenza di attenuazione tra la lesione e il pancreas sano era maggiore in fase pancreatica rispetto al valore in fase arteriosa , sia nelle lesioni ipervascolari ( 5833 hu vs 4822 hu , p = 0 , 21 ) , sia nelle lesioni di gruppo a ( 5923 hu vs 4524 hu , p = 0 , 11 )  . 
anche per il secondo radiologo il valore assoluto medio della differenza di attenuazione tra la lesione e il pancreas sano era maggiore in fase pancreatica rispetto al valore in fase arteriosa , sia nelle lesioni ipervascolari ( 5940 hu vs 4338 hu , p = 0 , 01 ) , sia nelle lesioni di gruppo a ( 6141 hu vs 4030 hu , p < 0 , 01 )  . i risultati espressi riguardo al contributo soggettivo delle fasi arteriosa e pancreatica alla confidenza diagnostica sono riportati nella tabella 3 . 
il contributo medio alla confidenza diagnostica delle fasi arteriosa e pancreatica stato rispettivamente di 2 , 11 , 2 e 3 , 00 . discussione per valutare se la fase pancreatica possa sostituire la fase arteriosa nella valutazione di tumori endocrini pancreatici , come suggerito in letteratura [ 4 ] , sono state analizzate da 2 radiologi , separatamente , le differenti attenuazioni della ghiandola pancreatica sana e del tumore , specialmente il valore assoluto della differenza media di attenuazione tra tumore e pancreas sano , in ciascuna delle fasi della tecnica trifasica di acquisizione con mdct . 
5a , b two - dimensional reconstructions in a 57 - year - old woman with hypovascular adrenocorticotropin - hormone - secreting , functioning , well - differentiated endocrine carcinoma in the pancreatic head ( ring )  . 
similar determinations have already been reported for pancreatic adenocarcinoma for both spiral and multidetector ct [ 1215 ] , indicating that routine acquisition of images in the arterial phase is not necessary for the detection of the pancreatic adenocarcinoma [ 13 ]  . 
the latest paper reported that pancreatic endocrine tumours , especially small ones , were better detected during the arterial phase of enhancement [ 9 ] , but the study did not consider the pancreatic phase . no statistical determinations have been done to asses whether the pancreatic phase is better than the arterial phase in the evaluation of endocrine pancreatic tumours . 
the novelty of our study was to compare and analyse statistically the data obtained in the arterial and pancreatic phases , using a triple - phase technique , in 23 patients affected by 29 confirmed endocrine pancreatic lesions . 
from a previous study [ 13 ] , we know that aortic enhancement is similar during the arterial and pancreatic phases but decreases in the portal phase ; this means that the evaluation of major peripancreatic arteries can be performed in the pancreatic phase as well as in the arterial phase . 
the portal phase is necessary to evaluate liver the parenchyma and major peripancreatic veins . tumour detection depends on attenuation characteristics of the normal pancreatic gland and the tumour , as already reported for pancreatic adenocarcinoma [ 13 ]  . 
pancreatic endocrine tumours can have different types of enhancement ( hypervascular , hypovascular or heterogeneous lesion ) ; in our experience we found all these enhancement patterns , with a majority of hypervascular lesions ( 55% )  . 
in our study , mean attenuation of the normal pancreatic gland and tumour was greater in the pancreatic phase than in the arterial and portal phases for both observers ; even the mean absolute tumour - to - gland attenuation difference was greater in the pancreatic phase for both radiologists , without any statistical difference between theeven in the case of a hypervascular pattern or small lesions ( < 2 cm ) , the mean absolute tumourto - gland attenuation difference was greater in the pancreatic phase for both radiologists , suggesting that these two types of lesions can be better detected in the pancreatic phase . 
the subjective contribution of the pancreatic phase to diagnostic confidence was as high as that of the arterial phase in the detection of hypervascular lesions , hypervascular liver metastases and arterial variations , whereas the pancreatic phase provided a greater contribution to the diagnostic confidence of hypovascular and heterogeneous lesions . 
as already demonstrated for pancreatic adenocarcinoma [ 13 ] , the arterial phase may be considered unnecessary and unhelpful . nellarticolo pi recente [ 9 ] si sostiene che i tumori endocrini pancreatici , specie se di piccole dimensioni , sono pi evidenti durante la fase arteriosa , ma la fase pancreatica non viene considerata . comunque , non stata mai effettuata alcuna determinazione statistica per stabilire se la fase pancreatica sia migliore rispetto a quella arteriosa nella valutazione dei tumori endocrini pancreatici . 
la novit di questo studio confrontare i dati ottenuti in fase arteriosa e in quella pancreatica , utilizzando una tecnica trifasica , in 23 pazienti affetti da 29 lesioni endocrine pancreatiche confermate , effettuando unanalisi statistica . 
da un precedente studio [ 13 ] sappiamo che lenhancement contrastografico aortico simile durante la fase arteriosa e la fase pancreatica , ma diminuisce durante la fase portale ; questo significa che la valutazione delle maggiori arterie peripancreatiche pu essere effettuata nella fase pancreatica cos come in quella arteriosa . la fase portale invece necessaria per valutare il parenchima epatico e le maggiori vene peripancreatiche . la detezione del tumore dipende dalle caratteristiche di attenuazione della ghiandola pancreatica sana e del tumore , cos come gi evidenziato per ladenocarcinoma pancreatico [ 13 ]  . 
il tumore endocrino pancreatico pu presentare differenti quadri di pattern contrastografico ( ipervascolare , ipovascolare , disomogeneo ) ; nella nostra esperienza , abbiamo osservato tutte queste caratteristiche di enhancement , con una prevalenza del pattern ipervascolare ( 55% )  . 
nei dati ottenuti , lattenuazione media della ghiandola pancreatica normale e del tumore maggiore nella fase pancreatica rispetto a quelle arteriosa e portale , per entrambi gli osservatori ; inoltre il valore assoluto della differenza di attenuazione media tumore - ghiandola maggiore nella fase pancreatica , per entrambi i radiologi , senza differenze statisticamente significative tra di loro . 
anche nei casi di lesioni ipervascolari o lesioni di piccole dimensioni ( < 2 cm ) , la differenza di attenuazione media tumore - ghiandola , in valore assoluto , maggiore in fase pancreatica , per entrambi i radiologi ; i nostri risultati perci suggeriscono che questi 2 tipi di lesione possono essere rilevati meglio in fase pancreatica . 
 + 39 - 011 - 6336311 , fax : + 39 - 011 - 6960310 , e - mail : andrea_veltri@infinito.it received : 18 july 2006 / accepted : 20 august 2006 / published online : 20 april 2007 abstract purpose . 
colour - doppler us enabled early detection and treatment of all vascular complications ( 9 / 40 , 22.5% of patients ; 13 complications in nine patients , eight arterial and five portal complications ; 1.4 for each patient with complications )  . 
us also detected biliary complications ( 11 patients , 27.5% : three cases of segmental ducts excluded from the anastomosis , four cases of stenosis of the biliodigestive anastomosis , one lithiasis , three stenoses associated with lithiasis ) , which were successfully managed in 75% of the cases treated with interventional radiology procedures ( percutaneous bilioplasty and / or lithotripsy )  . 
the radiologists role is fundamental for early sonographic diagnosis of post - olt complications in children . vascular complications are often associated in a single patient , and early treatment may improve the prognosis . 
le complicanze vascolari ( 9 / 40 pazienti , 22 , 5% ; 13 complicanze in 9 pazienti , 8 arteriose e 5 portali , 1 , 4 per paziente complicato ) sono state rilevate precocemente con leco - colordoppler , ricorrendo a tc o angiografia solo in rarissimi casi e consentendone il trattamento tempestivo . 
anche le complicanze biliari ( 11 pazienti , 27 , 5% : 3 dotti esclusi primariamente dallanastomosi , 4 stenosi dellanastomosi biliodigestiva , 1 litiasi e 3 stenosi con litiasi ) sono state evidenziate allecografia e trattate con successo nel 75% dei casi sottoposti a procedure di radiologia interventistica ( bilioplastica percutanea e / o trattamento della litiasi )  . 
la radiologia interventistica consente di affrontare in modo sicuro ed efficace molte complicanze biliari . key words paediatric liver transplantation split doppler ultrasound complications parole chiave trapianto di fegato pediatrico split eco - colordoppler complicazioni p . 
the main indications for surgery are cholestatic diseases ( particularly biliary atresia , the most common cause of olt ) , followed by hepatic cirrhosis and metabolic disease [ 1 ]  . 
in most cases , olt was performed for biliary atresia ( 23 / 40 , 57.5% ) , in four for tumours ( 10% , three hepatoblastomas and one hemangioendothelioma ) , in four ( 10% ) for congenital hepatic fibrosis , and in four ( 10% ) for metabolic diseases ( one case of type 1 oxalosis , one of methyl malonic acidaemia , one of fulminant wilsons disease and one of type 1a glycogenosis )  . 
in the remaining five patients , olt was performed because of cystic fibrosis , portocaval malformation , type 2 progressive familial intrahepatic cholestasis , posthepatitis cirrhosis ( due to hepatitis b and delta viruses ) and secondary biliary cirrhosis . 
four of these 40 patients ( 10% ) required a subsequent retransplantation : in three cases ( 7.5% ) due to vascular complications ( two hepatic artery thromboses on day 12 and day 69 , respectively ; one hepatic artery thrombosis associated with portal thrombosis on day 16 ) , and one due to biliary complications arising almost 11 months after the first operation ( table 1 )  . in 21 / 44 cases ( 47.7% ) , the entire liver was transplanted ; this was associated with a simultaneous kidney transplantation in four patients . 
le principali indicazioni allintervento sono le patologie colestatiche ( in particolare latresia delle vie biliari , causa pi frequente di olt ) , seguite dalla cirrosi epatica e dalle malattie metaboliche [ 1 ]  . 
la trombosi venosa portale non costituisce una controindicazione assoluta allolt , ma rende lintervento chirurgico molto pi complesso . le indagini radiologiche hanno due principali campi di applicazione : da un lato il bilancio pre - operatorio , per una corretta selezione dei pazienti , dallaltro il monitoraggio intrae soprattutto post - operatorio [ 25 ]  . 
tante sono le sfide per il radiologo nella sorveglianza dellolt in et pediatrica , anche se gi coinvolto in un programma di olt delladulto ; particolari problematiche , infatti , comportano la necessit di una sua maggiore disponibilit : il coinvolgimento gi in sala operatoria , la necessit di conoscenze chirurgiche appropriate , la minore collaborazione da parte del paziente e la maggiore assiduit dei controlli nel postolt precoce , la maggiore attenzione agli aspetti radioprotezionistici , fino alla massima abilit nelle procedure diagnostiche e terapeutiche mini - invasive . lo scopo di questo lavoro consiste nel riesaminare la casistica del centro trapianti epatici di torino , che conduce un programma di olt pediatrico in associazione a quello assai pi consolidato delladulto , per analizzare , nella nostra personale esperienza , limpegno e limportanza del medico radiologo nella gestione del paziente nel post - olt . materiali e metodi nel periodo compreso tra ottobre 1999 e settembre 2005 sono stati eseguiti presso il centro trapianti epatici del nostro ospedale 44 trapianti epatici pediatrici in 40 bambini , 20 maschi e 20 femmine , di et compresa tra 4 mesi e 14 anni ( media 4 , 6 anni )  . 
lolt stato eseguito nella maggior parte dei casi per atresia delle vie biliari ( 23 su 40 , 57 , 5% ) , in 4 per patologia tumorale ( 10% , 3 epatoblastomi e 1 emangioendotelioma ) , in 4 ( 10% ) per fibrosi epatica congenita , mentre 4 pazienti ( 10% ) erano affetti da malattia metabolica ( un caso di ossalosi di i tipo , uno di acidemia metilmalonica , uno di malattia di wilson fulminante e un caso di glicogenosi di tipo ia ) ; nei restanti 5 pazienti lolt stato eseguito rispettivamente per un caso di fibrosi cistica , una malformazione porto - cavale , un caso di colestasi intraepatica familiare progressiva di tipo 2 , una cirrosi post - epatitica ( da virus dellepatite b e delta ) e , infine , una cirrosi biliare secondaria . 
in 4 di questi 40 pazienti ( 10% ) stato successivamente necessario il ritrapianto , in tre casi ( 7 , 5% ) per complicanze vascolari ( due trombosi dellarteria epatica , in dodicesima e sessantanovesima giornata , e un caso di trombosi dellarteria epatica associata a trombosi portale , in sedicesima giornata ) e nellultimo , dopo quasi 11 mesi dal p . 
within these timeframes , all radiologically detectable complications were evaluated , primo intervento , per complicanze biliari ( tabella 1 )  . in 21 / 44 casi ( 47 , 7% ) stato trapiantato il fegato intero , associato a trapianto contemporaneo di rene in 4 pazienti ; in 22 casi ( 50% ) stato trapiantato il lobo epatico sinistro ( in prevalenza ii e iii segmento , solo raramente associati al lobo quadrato e / o caudato per esigenze anatomiche o chirurgiche ) e in un solo caso ( 2 , 3% ) il lobo destro . 
nel 95 , 5% dei casi lolt stato eseguito da donatore cadavere , mentre in 2 pazienti ( 4 , 5% ) il fegato split proveniva da donatore vivente . lo studio stato condotto retrospettivamente , analizzando dettagliatamente tutti gli esami radiologici diagnostici e interventistici eseguiti presso il nostro istituto nel periodo p . 
in all three cases , the vascular anastomoses were surgically reviewed before completing the operation . us scans performed on the first post - operative days almost constantly revealed right pleural effusions and ascites , as well as mainly perihepatic fluid collections . 
finally , the us reports described acceleration of arterial flow to the hilum in one patient and flow acceleration at the portal anastomosis in seven patients , which resolved spontaneously during the follow - up period . three patients with hepatic artery thrombosis ( including the case associated with portal thrombosis ) required retransplantation , whereas surgical review of the anastomosis proved sufficient in the three remaining cases , as in one of the cases of portal thrombosis . biliary complications included three cases of bile leaks caused by the exclusion of ducts from the anastomosis , which required repeat surgery , and five cases of more - orless pronounced dilatation of intrahepatic bile ducts , which was treated early by biliary drainage in one patient only . during the first 3 months after discharge , 237 colourdoppler us examinations ( 5.9 exams per patient on average ) , one ct study , one arteriography , one cavography , 19 hepatic biopsies , three abdominal two paracenteses , drainages ( all of which were us - guided ) , 15 transhepatic percutaneous cholangiographies , five bilioplasties of the biliary - digestive anastomosis ( bda ) , and two lithotripsies were performed . 
it confirmed the other two haemodynamically significant portal stenoses and the persistence of the segmental portal thrombosis ( detected during the hospital stay and unchanged throughout the follow - up ) , and demonstrated normalisation in the eight cases of arterial or portal flow acceleration only in the anastomosis . 
usguided peritoneal punctures included two cases of us - guided paracenteses due to abundant ascites , one case of drainage tube placement in a patient with an interhepatic diaphragmatic collection , and two cases of diagnostic needle puncture performed to investigate two loculated abdominal collections ( one subphrenic and the other in morrisons pouch ) in which fluid culture excluded a bacterial superinfection . 
in three patients , us confirmed the stability of a risultati complessivamente , durante la fase di ricovero , sono stati eseguiti 622 studi us , 18 dei quali intraoperatori , con una media di 1 esame ogni 1 , 3 giorni ; inoltre , sono state effettuate 4 tc con mdc e.v. , 1 studio rm , 1 arteriografia , 4 biopsie epatiche ecoguidate , 4 drenaggi di raccolte addominali e 2 toracentesi , sempre sotto guida us , e 7 colangiografie percutanee transepatiche . lecografia intraoperatoria ha rilevato 1 caso di ipoperfusione arteriosa , una vera e propria trombosi dellarteria epatica e 1 caso di inversione di flusso nel ramo portale ( per arterializzazione vicaria , secondaria a ipoperfusione da difetto tecnico dellanastomosi venosa ) ; in tutti i 3 casi stata eseguita la revisione chirurgica delle anastomosi vascolari prima di terminare lintervento . nei controlli ecografici durante le prime giornate postoperatorie versamento pleurico destro e ascite , cos come raccolte fluide prevalentemente periepatiche , sono risultate pressoch costanti . 
infine , nei referti us sono state genericamente descritte in 1 paziente accelerazione del flusso arterioso allilo e in 7 accelerazione del flusso in corrispondenza dellanastomosi portale , poi risoltesi spontaneamente nel follow - up . 
in 3 pazienti con trombosi dellarteria epatica ( compresa quella associata a trombosi portale ) , stato necessario il ritrapianto , mentre negli altri 3 casi stata sufficiente la revisione chirurgica dellanastomosi , cos come in 1 caso di trombosi portale . per quanto concerne le complicanze biliari , in 3 casi si sono verificati spandimenti biliari secondari alla presenza di dotti esclusi dallanastomosi , che hanno richiesto un nuovo intervento chirurgico , mentre in 5 casi stata dimostrata una dilatazione pi o meno accentuata delle vie biliari intraepatiche , che in un solo paziente stata trattata precocemente con il posizionamento di un drenaggio biliare . considerando la fase successiva alle dimissioni , ma limitatamente ai primi 3 mesi , sono stati eseguiti un totale di 237 eco - color - doppler ( con una media di 5 , 9 esami per paziente ) , 1 tc , 1 arteriografia , 1 cavografia , 19 biopsie epatiche , 2 paracentesi e 3 drenaggi di raccolte addominali ( tutti ecoguidati ) , 15 colangiografie percutanee transepatiche , 5 bilioplastiche dellanastomosi bilio - digestiva ( abd ) e 2 litotripsie . 
in tale periodo lesame us ha documentato la stabilizzazione di 2 pregresse stenosi arteriose e di 2 stenosi anastomotiche portali asintomatiche , ha confermato le altre 2 stenosi portali , emodinamicamente significative , e la persistenza della trombosi portale segmentaria ( rilevata durante il ricovero e rimasta invariata per tutta la durata del follow - up ) , e ha rilevato la normalizzazione del reperto negli 8 casi di sola accelerazione del flusso arterioso o portale in sede di anastomosi . 
in two other cases , the us finding associated with laboratory abnormalities prompted the use of percutaneous cholangiography , which identified bda stenosis , in one case associated with microlithiasis and with further stenoses of the intrahepatic bile ducts . 
in one patient , however , the anastomotic stenosis recurred associated with a stenosis at the intersection of the iiand iiidanza dellascite , in 1 paziente stato posizionato per alcuni giorni un catetere di drenaggio nella compagine di una raccolta interepato - diaframmatica e in 2 si proceduto allagocentesi diagnostica di altrettante raccolte addominali saccate ( una subfrenica e una nel recesso di morison ) , laddove lesame colturale ha escluso in ambedue i casi la sovrainfezione batterica . 
in 3 pazienti lecografia ha confermato la stabilit di un precedente riscontro di dilatazione delle vie biliari , ritenuto privo di significato clinico , mentre in altri 2 il reperto us , in associazione con lalterazione dep . 
further complications occurred in this stage of the follow - up : one lymphoproliferative disease ( which completely remitted by discontinuing immunosuppressive treatment for 6 months ) , one case of hepatic granulomas and reactive hilar lymph nodes ( both subjected to percutaneous us - guided needle biopsy ) due to infection by bartonella henselae ( cat - scratch disease transmitted by the donor ) and one gaseous embolisation of the portal trunk secondary to enteritis . in the third stage ( more than 3 months from discharge ) , us and transhepatic percutaneous cholangiography identified four new cases of bda stenosis , two associated with biliary lithiasis . 
in another patient , about 3 years after olt , the repeated us detection of biliary ectasia led us to perform mr cholangiography , which documented multiple filling defects at the level of the confluence and common bile duct . 
in addition to confirming this finding , percutaneous cholangiography also enabled bda bilioplasty and lithotripsy to be performed , with good long - term results . one of the two patients with haemodynamically significant portal stenoses underwent surgical review of the anastomosis . 
however , subsequent follow - up examinations revealed the absence of post - anastomotic flow and the onset of chronic liver disease ( with right - lobe hypotrophy and leftlobe hypertrophy ) as well as almost exclusively arterial perfusion . 
five cases necessitated surgery , four for refashioning the bda and one for retransplantation . at the end of the observation period , the patient survival rate was 100% and the organ survival rate was 91% . the considerable advances in surgery and radiology since 1963 ( the year of the first paediatric liver transplantation ) have significantly increased post - olt survival [ 610 ]  . among recent studies , evrard et al.s [ 11 ] retrospective rediscussion gli esami di laboratorio , ha indotto allesecuzione della colangiografia percutanea ; questa ha dimostrato la stenosi dellabd , in un caso associata a microlitiasi e a ulteriori stenosi dei dotti biliari intraepatici . 
ulteriori complicanze occorse in questa seconda fase di follow - up sono state una malattia linfoproliferativa ( poi completamente regredita sospendendo la terapia immunosoppressiva per 6 mesi ) , un caso con granulomi epatici e linfonodi ilari reattivi ( entrambi sottoposti ad agobiopsia percutanea ecoguidata ) da infezione da bartonella henselae ( malattia da graffio di gatto , trasmessa dal donatore ) e unembolizzazione gassosa del tronco portale secondaria a unenterite . nella terza fase ( oltre i tre mesi dalla dimissione ) , infine , us e colangiografia percutanea transepatica hanno dimostrato 4 nuovi casi di stenosi dellabd , 2 dei quali associati a litiasi biliare . 
in un ulteriore paziente , a distanza di circa 3 anni dallolt , il ripetuto rilievo us di ectasia delle vie biliari ha portato allesecuzione di una colangio - rm , che ha dimostrato multipli difetti di riempimento a livello della confluenza e del dotto epatico comune . 
la colangiografia percutanea , oltre a confermare il reperto , ha consentito lesecuzione di una bilioplastica dellabd e di una litotripsia , con buon risultato a distanza . quanto alle 2 stenosi portali emodinamicamente significative , in 1 paziente stata eseguita la revisione chirurgica dellanastomosi ; i controlli successivi , tuttavia , hanno evidenziato lassenza di flusso post - anastomotico e il progressivo sviluppo di unepatopatia cronica ( con ipotrofia del lobo destro e ipertrofia del sinistro ) , in presenza di una perfusione pressoch esclusivamente arteriosa . 
nellaltra paziente con precedente evidenza di stenosi portale si assistito , in questo terzo periodo , alla progressione della stessa in occlusione , con successivo tentativo di disostruzione / angioplastica percutanea , scarsamente efficace . nel complesso , durante lintero follow - up , le complicanze vascolari maggiori sono state in totale 13 , concentrate in 9 pazienti ( 22 , 5% ; 1 , 4 complicanze per ogni paziente complicato ) : 6 trombosi dellarteria epatica ( 2 associate a trombosi anche portale , una precoce e una tardiva , dopo la revisione dellarteria ) , 2 stenosi arteriose , 3 trombosi portali isolate ( 1 parziale e 2 complete ) ( tabella 2 )  . 
in 11 pazienti ( 27 , 5% ) si sono verificate complicanze biliari ; in 3 di questi sono stati precocemente diagnosticati dotti esclusi ; gli altri sono stati 4 stenosi della abd , 1 caso di litiasi e sludge biliare , e infine 3 pazienti con concomitanza di stenosi dellabd e sludge e litiasi biliare . 
 [ 12 ] reported survival rates of 88% , 82% and 82% at 1 , 3 and 5 years , respectively , in 249 paediatric olts carried out between 1986 and 1998 . 
our study , although our series was small due to our relatively short experience with paediatric olt ( dating from 1999 only ) , showed survival rates of 100% at 1 , 3 and 5 years . 
the results of our analysis allow us to state that diagnostic and interventional radiology also contributed to this success rate . in contrast , the rate of retransplantations at our centre ( 10% ) is similar to that reported by other recent studies . 
for example , the hamburg centre reported a retransplantation rate of 11.8% among the 170 paediatric olts performed between 2001 and 2004 , with a survival rate of 97% up to january 2005 [ 13 ]  . the incidence of the main post - olt biliary complications in our series was also in keeping with those reported by the main international liver transplantation centres . 
this may be related to sample size ( reference studies were considerably larger than ours ) but also to the learning curve of the staff involved in the paediatric olt programme , which only began in 1999 at our centre as opposed to the early 1980s at the main international centres . 
nonetheless , the successful management of complications in our series could also in part be ascribed to the radiologist , who played a central role in the early diagnosis and treatment of some of the complications . discussione grazie ai notevoli progressi medico - chirurgici , ma anche di quelli delle discipline radiologiche , dal 1963 ( anno del primo trapianto epatico pediatrico ) a oggi si assistito a un significativo incremento della sopravvivenza post - olt [ 610 ] ; infatti , tra le pi recenti casistiche , evrard et al . [ 11 ] riportano , dopo analisi retrospettiva di 500 olt pediatrici effettuati tra il 1984 ed il 2000 , una percentuale di sopravvivenza a 1 , 5 e 10 anni rispettivamente dell85% , 81% e 79% , mentre migliazza et al . 
 [ 12 ] , in 249 olt pediatrici eseguiti tra il 1986 ed il 1998 , hanno evidenziato tassi di sopravvivenza a 1 , 3 e 5 anni rispettivamente dell88% , 82% e 82% . 
nella nostra casistica , per quanto composta da un numero di pazienti ancora limitato vista la recente esperienza nel settore pediatrico ( datata solo dal 1999 ) , le percentuali di sopravvivenza a 1 , 3 e 5 anni sono state finora tutte del 100% ; alla luce dei risultati dalla nostra analisi , ragionevole pensare che a questo risultato abbia contribuito anche la radiologia diagnostica e interventistica . sovrapponibile ad altri studi di recente pubblicazione , invece , la percentuale di re - olt effettuati nel centro , attestata a oggi al 10% . 
per citare un esempio , il centro di amburgo riporta , nellambito di una casistica di 170 olt pediatrici eseguiti tra il 2001 e il 2004 , un tasso di ritrapianti dell11 , 8% , con una sopravvivenza del 97% al gennaio 2005 [ 13 ]  . anche per quanto riguarda lincidenza delle principali complicanze biliari nel post - olt , i risultati del nostro studio sono paragonabili a quelli riportati in letteratura dai principali centri internazionali di trapianto epatico , mentre lincidenza delle complicanze vascolari appare maggiore , risultando attualmente del 22 , 5% ( tabella 3 )  . 
la motivazione di questo secondo dato potrebbe essere legata alle dimensioni del campione ( le casistiche di confronto sono notevolmente pi ampie della nostra ) , ma anche alla curva di apprendimento dello staff medico - chirurgico coinvolto nel programma di olt pediatrico , iniziato come detto nel 1999 , rispetto agli inizi negli anni ottanta dei principali centri internazionali . ciononostante , la buona gestione delle complicanze nella nostra serie potrebbe essere in parte attribuibile anche al radiologo , visto il ruolo da lui assunto nella diagnosi precoce e nel trattamento di alcune delle complicanze stesse . limportanza delleco - color - doppler nella diagnosi precoce delle complicanze vascolari post - olt , infatti , sancita ormai da numerose esperienze cliniche [ 4 , 2023 ]  . 
questa metodica , non invasiva ed eseguibile anche al letto del malato , indicata nellimmediato periodo post - operatorio dei pazienti pediatrici con frequenza minima giornaliera , ma spesso anche pi assidua , specie nei casi che necessitano di uno stretto monitoraggio per la complessit dellintervento chirurgico ( anastomosi multiple o a rischio , difficolt di perfusione intraoperatoria , ecc . ) o per condizioni cliniche pi precarie . 
this noninvasive study , which can be performed at the patients bedside , if need be , should be performed with at least daily frequency in the immediate postoperative follow - up of paediatric patients . 
this frequency should be increased in cases requiring close monitoring because of the complexity of the operation ( multiple or risk anastomoses , intraoperative perfusion difficulties , etc . ) or because of a less stable clinical condition . 
in particular , the earliest possible diagnosis of hepatic artery thrombosis , one of the most feared complications due to the high mortality rates and the frequent need for immediate retransplantation , is a determinant for prognosis [ 2428 ]  . 
close radiological monitoring in the first few days post - olt is thus essential for detecting thrombosis at an early stage , when surgical review of the hepatic artery can resolve the thrombosis , thereby reducing parenchymal necrosis and especially ischaemic biliary damage , which may in turn eventually lead to severe biliary complications . 
in our experience , colour - doppler us provided early diagnosis of arterial thrombosis in six patients who were still asymptomatic : immediate surgical review of the anastomosis proved adequate in three of them , thereby improving their prognosis . 
in children , ct angiography ( which has supplanted angiography in the diagnosis of vascular complications , unless this is used to plan endovascular treatments ) is usually reserved for the study of cases with uncertain us findings , as it involves a considerable radiation dose and increased risk of kidney failure due to the use of intravenous iodinated contrast material [ 29 ]  . 
the other radiological modalities can be used after colour - doppler us , as needed and with lower frequency , in ascending order of invasiveness : contrastenhanced us , ct , mri and angiography , the latter being limited to cases requiring percutaneous treatment [ 4 ]  . on the basis of our personal experience , we stress the importance of a correct and integrated interpretation of us findings to avoid dangerous false positive results . 
this finding is mostly related to a difference in calibre between the donors and the receivers vessels , to a transient oedematous reaction ( as confirmed by the gradual spontaneous resolution on subsequent us scans ) or , finally , to kinking of the vascular anastomosis . 
lo stretto monitoraggio radiologico nelle prime giornate postolt dunque fondamentale per riconoscere la trombosi in fase iniziale , quando la revisione chirurgica dellarteria epatica pu essere risolutiva , riducendo la necrosi del parenchima epatico e soprattutto il danno ischemico alle vie biliari , foriero di successive complicanze biliari gravi . 
nella nostra esperienza , lesame eco - color - doppler ha diagnosticato precocemente la trombosi arteriosa in 6 pazienti ancora asintomatici , in 3 dei quali risultata sufficiente limmediata revisione dellanastomosi chirurgica , con evidente miglioramento della prognosi . 
nel paziente pediatrico langiotc ( che ha ormai soppiantato langiografia nella diagnosi delle complicanze vascolari , se non in previsione di trattamenti endovascolari ) viene di norma riservata allo studio dei casi di incerta interpretazione ecografica , comportando una notevole irradiazione e un aumentato rischio di insufficienza renale per la somministrazione endovenosa di mdc iodato [ 29 ]  . 
seguono , quando necessario e con frequenza di impiego nettamente inferiore , le altre metodiche radiologiche in ordine crescente di invasivit : lecografia con mdc , la tc , la rm e langiografia , questultima limitatamente ai casi in cui si prospetti un trattamento percutaneo [ 4 ]  . anche in base allesperienza personale , ci preme per sottolineare limportanza di una corretta e integrata interpretazione dei reperti us , onde evitare pericolosi falsi positivi . 
infatti , nellimmediato post - operatorio , relativamente frequente ( 20% nella nostra casistica ) il riscontro di unaccelerazione di flusso in sede anastomotica , soprattutto portale ; tale reperto per lo pi legato a una differenza di calibro tra vaso del donatore e quello del ricevente o a una temporanea reazione edematosa tissutale ( come confermato dalla progressiva risoluzione spontanea nei successivi controlli us ) , o infine a unangolatura dellanastomosi vascolare ( kinking )  . 
in questi casi , si devono effettuare controlli pi ravvicinati per monitorare le ripercussioni emodinamiche sulla circolazione intraepatica ed evidenziare eventuali segni precoci di sofferenza del parenchima epatico , o prevenire la progressione della stenosi fino alla tromp . 
in these cases , close monitoring is needed to check the haemodynamic effects on the intrahepatic circulation and detect any early signs of parenchymal distress , as well as to prevent the stenosis developing into a thrombosis ( as unfortunately occurred in two of our patients as a result of the surgeons reluctance to treat the complication in the absence of clinicallaboratory signs )  . as regards biliary complications , leaks from open bile ducts call for immediate reoperation . 
in centres providing a highly qualified interventional radiology service , interventional radiology plays a central role as the initial approach in bda or biliary stenoses , lithiasis and postbiopsy haematobilia . 
it also represents the only alternative to surgery , given that fashioning of the bda on the roux loop ( always adopted in paediatric olt ) makes endoscopic retrograde cholangiopancreatography technically impossible [ 3033 ]  . 
la radiologia interventistica , nei centri in cui sia disponibile un servizio di comprovata esperienza , assume invece un ruolo fondamentale come primo approccio nelle stenosi dellabd o dei dotti biliari , nella litiasi e nella emobilia post - bioptica , costituendo lunica alternativa alla chirurgia dal momento che il confezionamento dellabd su ansa alla roux ( costantemente adottata nellolt pediatrico ) rende tecnicamente impossibile lesecuzione di una colangiopancreatografia retrograda endoscopica [ 3033 ]  . 
in letteratura , la loro incidenza molto variabile ; ad esempio , kling et al . [ 34 ] riportano una percentuale pari al 33% , ben superiore al 7% segnalato da kim et al . 
nella loro esperienza [ 13 ]  . diversamente dalle stenosi biliari intraepatiche diffuse , che sono generalmente dovute a un danno ischemico , immunologico o infettivo , le stenosi dellabd sono generalmente il risultato della formazione di tessuto fibroso a livello anastomotico [ 35 ]  . 
in paediatrics , transhepatic percutaneous cholangiography and biliary drainage demand a higher degree of expertise and skill ( above all to perform the puncture , which always requires close us monitoring ; fig . 6 ) because of the small calibre of the intrahepatic biliary branch . 
a more recent study by the same author [ 37 ] on the percutaneous dilatation of paediatric post - olt stenoses reported a 25% rate of stenotic recurrences ( after one or more bilioplasty procedures ) requiring surgical review or retransplantation , and 15% of cases necessitating a stent to ensure anastomosis patency . in our study , interventional radiology procedures were successful in 75% of treated cases , with long - term patency of the bda and intraand extrahepatic bile ducts and absence of sludge or biliary lithiasis . 
in one patient , the ischaemic damage to the entire biliary system was such that repeated restenoses followed numerous bilioplasty attempts si biliare , le procedure interventistiche danno i migliori risultati a distanza . 
 [ 36 ] hanno segnalato la mancata opacizzazione dellalbero biliare nel 4 , 2% dei casi . un pi recente studio del medesimo autore [ 37 ] sulla dilatazione percutanea delle stenosi nel post - olt pediatrico riporta un 25% di recidive stenotiche ( dopo una o pi bilioplastiche ) tali da richiedere la revisione chirurgica o il ritrapianto , e un 15% di casi in cui stato necessario il posizionamento di uno stent per mantenere la perviet dellanastomosi . 
 anche nel nostro studio le manovre di radiologia interventistica sono state risolutive nel 75% dei casi trattati , con perviet a lungo termine dellabd e delle vie biliari intraed extra - epatiche , e assenza di sludge o litiasi biliare . 
in una paziente il danno ischemico allintero sistema biliare stato tale che numerosi tentativi di bilioplastica , eseguiti con successo nellimmediato , sono stati seguiti costantemente da restenosi ; si quindi tentata una revisione chirurgica , ma alla p . 
in the last case , however , cholangiography was successfully performed , but despite various attempts , the stenosis could not be negotiated , so the bda was refashioned . the greatest risk in repeating these procedures , which is compounded by the performance of other examinations using ionising radiation before or after olt , is the induction of subsequent neoplasms ( particularly haematological ) as an expression of stochastic damage . 
in order to reduce the risk as far as possible and limit the number of parenchymal punctures , us guidance is commonly used at our centre in the early steps of biliary drainage ( from transhepatic percutaneous cholangiography to catheter placement ) , followed by minimal short periods of pulsed radioscopy . fine stato necessario il ritrapianto . 
nellultimo caso , invece , stata eseguita con successo la colangiografia ma , nonostante diversi tentativi , non si riusciti a valicare la stenosi , per cui si ricorsi al riconfezionamento dellabd . il rischio maggiore insito nella ripetizione di queste procedure , incrementato dalleventuale esecuzione nel pree / o post - olt di ulteriori indagini radiologiche impieganti radiazioni ionizzanti , linduzione di successive neoplasie ( soprattutto ematologiche ) come espressione di danno stocastico . 
al fine di ridurre il pi possibile questo rischio , entrato ormai nella pratica comune del nostro istituto limpiego della guida ecografica nelle prime fasi del drenaggio biliare ( dalla colangiografia percutanea transepatica fino al posizionamento del catetere ) , anche per limitare il numero di punture parenchimali ; successivamente si utilizzano al minimo brevi periodi di radioscopia pulsata . conclusions conclusioni if the success of olt depends in part on the early diagnosis and appropriate treatment of complications , in our experience albeit with a small series the radiologist proved irreplaceable in all stages . 
by integrating the information obtained with the various diagnostic methods ( including liver biopsy carried out by the radiologist with us guidance ) , the radiologist contributes greatly to every diagnostic conclusion and participates actively in therapeutic procedures . 
in particular , interventional radiology techniques allow safe and minimally invasive postoperative complication management , often avoiding further reoperations and contributing to improved prognosis of these young patients . se il successo dellolt epatico dipende in parte dalla diagnosi precoce e dal trattamento appropriato delle complicanze , nella nostra pur limitata esperienza il medico radiologo si dimostrato da subito insostituibile . 
infatti , integrando le informazioni ottenute dalle varie metodiche ( compresa la biopsia epatica , eseguita sempre dal radiologo con guida ecografica ) , egli fornisce allo staff del trapianto un apporto fondamentale per ogni conclusione diagnostica e partecipa attivamente alla fase terapeutica . 
giovanni battista di torino , c.so bramante 88 / 90 , i - 10126 torino , italy , tel . : + 39 - 011 - 6333574 , e - mail : gciccarelli@molinette.piemonte.it received : 21 may 2006 / accepted : 18 october 2006 / published online : 20 april 2007 abstract purpose . 
definitive histological assessment of margin status , including status after reexcision , was infiltrated margins in 23 patients ( 23% ) and clear margins in 79 patients ( 77% )  . definitive histological assessment in 12 / 19 patients ( 63.15% ) with intraoperative reexcision , confirmed margin infiltration of the first specimen . 
in tutti i casi sono state eseguite le radiografie dei pezzi anatomici nelle due proiezioni ortogonali con ingrandimento diretto per valutare : presenza / assenza della lesione ; posizione della lesione nel pezzo anatomico ; direzione verso cui effettuare un eventuale ampliamento nei casi in cui la lesione era in prossimit di un margine . 
il confronto tra le diagnosi radiologiche e istopatologiche prima degli ampliamenti , quando effettuati , ha dato valori di sensibilit e di specificit rispettivamente del 66% e 86% e valore predittivo positivo e negativo , rispettivamente , del 74% e 81% . 
la valutazione istologica definitiva dei margini , considerando anche gli ampliamenti quando effettuati , risultata : margini infiltrati in 23 pazienti ( 23% ) e indenni in 79 casi ( 77% )  . in 12 / 19 casi ( 63 , 15% ) con ampliamento estemporaneo lesame istologico definitivo conferm che i margini del primo pezzo anatomico erano infiltrati : in queste pazienti lampliamento estemporaneo stato decisivo . 
la radiografia del pezzo operatorio risultata attendibile nel rilevare i margini non infiltrati ( valore predittivo positivo 74% ) e ci ha consentito di ridurre la percentuale di secondi interventi dal 31% al 20% . 
these lesions require excisional surgery after preoperative wire localisation to ensure the removal of a portion of parenchyma with the lesion exactly at the centre of the specimen [ 1 , 2 ]  . 
in these cases , for which breast - conserving surgery is used in part to guarantee an optimal cosmetic outcome , it is fundamental to assess the resection margins to prevent the risk of reintervention and / or local recurrence [ 3 , 4 ]  . 
correct surgical excision is dependent on the use of intraoperative specimen radiography in the two orthogonal projections to ensure an adequate amount of tissue has been removed [ 5 , 6 ]  . the aim of this study was to evaluate the diagnostic reliability of specimen radiography for the assessment of resection margins in breast - conserving surgery for impalpable lesions to avoid the need for reintervention to achieve clear margins . materials and methods this was a retrospective review of 123 consecutive patients ( age range 4187 years ) who between january and december 2004 underwent breast - conserving surgery for impalpable breast lesions detected on clinical and / or screening mammography . 
in all cases , the preoperative radiological and cytohistological diagnosis indicated suspicious lesions or definitely positive lesions ( r4 / 5 , c4 / 5 , b4 / 5 )  . 
all lesions were preoperatively marked with vegetable charcoal to allow the surgeon to correctly locate and excise the lesion . before concluding the operation , the surgeon sent the excised specimen to the radiology department for radiography : suture threads were applied on each surgical specimen in the operating room to identify and orient the resection margins ( one thread for the areolar margin ; two threads for the medial or lateral margin ; three threads for the cranial or caudal margin )  . all radiographs were obtained in the two orthogonal planes . 
specimen radiography was performed on an analogical mammography unit senographe dmr v2 ( ge ) using the direct magnification technique ( 1 : 5 or 1 : 8 ) , appropriate compression , kilovolt ( kv ) between 25 and 28 and milliampere second ( mas ) between 10 and 20 depending on specimen size . 
the images were printed using kodak min r film and a dedicated automatic developer kodak mini loader 2000 p . specimen radiographs were compared with the baseline mammograms to assess adequacy of the excision . 
the parameters considered in the radiological reports were : presence / absence of the lesion position of the lesion within the specimen ( relative to the direction in which to extend the excision in the case of resection margins ) close margins la crescente diffusione della mammografia clinica e dei programmi di screening ha portato allincremento dei reperti di lesioni mammarie sospette non palpabili da sottoporre ad intervento chirurgico previa localizzazione preoperatoria per consentire lexeresi chirurgica di una porzione di parenchima mammario con la lesione esattamente centrata nella compagine [ 1 , 2 ]  . 
in questi casi , in cui lapproccio chirurgico di tipo conservativo anche per ottenere risultati estetici ottimali , importante la valutazione dei margini di resezione per evitare il rischio di reinterventi di radicalizzazione e / o di recidive locali [ 3 , 4 ]  . 
una corretta escissione chirurgica non pu prescindere dallesecuzione , durante lintervento , della radiografia del pezzo operatorio effettuato nelle due proiezioni ortogonali per avere una ragionevole certezza di adeguata escissione [ 5 , 6 ]  . scopo del presente lavoro quello di valutare lattendibilit diagnostica della radiografia del pezzo operatorio nellanalisi dei margini di resezione degli interventi conservativi di resezione mammaria in lesioni non palpabili per evitare , nei casi di margini infiltrati , di dover programmare un secondo intervento chirurgico per radicalizzare la lesione . materiali e metodi si tratta di unanalisi retrospettiva effettuata in 123 pazienti consecutive , di et compresa tra 41 e 87 anni che , da gennaio a dicembre 2004 , sono state sottoposte a interventi conservativi per lesioni mammarie non palpabili diagnosticate con esami di senologia clinica e / o di screening mammografico . 
in tutti i casi la diagnosi radiologica e cito - istologica preoperatoria stata di lesioni sospette o francamente positive per lesioni neoplastiche ( r4 / 5 , c4 / 5 , b4 / 5 ) : in tutti i casi , in previsione dellintervento chirurgico , stata posizionata una traccia di carbone vegetale per consentire al chirurgo una corretta localizzazione della lesione e conseguente adeguata asportazione . il chirurgo , prima di considerare concluso lintervento , ha inviato in radiologia il pezzo anatomico asportato per lesecuzione della radiografia : su ogni frammento chirurgico sono stati applicati , in sala operatoria , alcuni fili di sutura per identificare i margini di resezione e consentirne un corretto orientamento spaziale ( 1 filo margine areolare ; 2 fili margine mediale o laterale ; 3 fili margine craniale o caudale )  . le radiografie sono sempre state effettuate secondo i due piani ortogonali : dapprima il pezzo operatorio stato posizionato sul piatto del mammografo orientato con i fili di repere come per effettuare una proiezione cranio - caudale . successivamente il pezzo stato ruotato lateralmente di 90 per effettuare una proiezione latero - laterale . 
le radiografie del pezzo operatorio sono state effettuate utilizzando un mammografo analogico senographe dmr v2 ( ge ) , con la tecnica dellingrandimento diretto ( 1 : 5 o 1 : 8 ) , con appropriata compressione , kv compresi tra 25 e 28 e mas tra 10 e 20 in rapporto alle dimensioni del pezzo operatorio : le img . 
after radiography , the surgical specimen was sent to the pathologist for histological assessment . evaluation of the diagnostic reliability of specimen radiography was performed by comparing the radiographic and histopathological diagnoses : at histology , the resection margins were considered to be infiltrated when the tumour was located on the sectioned surface or when the distance between the lesion and the resection margin was 2 m results lesion histology table 1 shows the definitive histological diagnoses in the 123 patients considered : as one patient had both a benign and a malignant lesion , the series comprised a total of 124 lesions . 
the diagnostic reliability of specimen radiography for the evaluation of resection margins was retrospectively assessed for 102 malignant lesions . lesion size magini sono state stampate utilizzando pellicole kodak min r e sviluppatrice automatica dedicata kodak mini loader 2000 p . 
i paramenti valutati e riportati nel referto radiologico sono stati : presenza / assenza della lesione ; posizione della lesione allinterno del pezzo anatomico ( in rapporto ai margini di resezione ) ; direzione verso cui effettuare un allargamento nei casi in cui la lesione si presentava in prossimit di un margine . nei casi in cui la lesione risultava presente ed in sede centrale si data indicazione al chirurgo di concludere lintervento ; nei casi in cui invece la lesione risultava in prossimit di un margine stato comunicata la direzione verso cui effettuare un allargamento dellescissione prima di considerare concluso lintervento . 
al termine dellesame radiologico il pezzo anatomico stato inviato al patologo per lesame istologico . la valutazione relativa allattendibilit diagnostica dei reperti radiologici stata fatta confrontando le diagnosi radiologiche con quelle istopatologiche : istologicamente i margini di resezione sono stati considerati infiltrati nei casi di lesione neoplastica in corrispondenza di una delle superfici di taglio ovvero nei casi in cui la distanza tra la lesione e il margine di resezione era 2 mm . infiltrating lesions had a diameter ranging from 6 to 20 mm ; extension of calcifications in the ductal carcinomas in situ varied between 3 and 80 mm . risultati istologia delle lesioni intraoperative radiography of resection margins and indication for immediate reexcision in 34 patients , specimen radiography raised a suspicion of infiltrated resection margins : the excision was extended intranella tabella 1 sono riportate le diagnosi istologiche definitive delle 123 pazienti oggetto di questo studio : poich in una paziente vi era concomitanza di una lesione benigna e di una maligna , la casistica composta , complessivamente , da 124 lesioni . 
lattendibilit diagnostica della radiografia del table 1 final pathological diagnosis of the 124 lesions tabella 1 istologia delle 124 lesioni benign lesions : 22 sclerosing adenosis : 8 fibroadenomas : 7 papillomas : 3 fibroadenosis : 2 hyperplasia : 2 lesioni benigne : 22 adenosi sclerosante : 8 fibroadenomi : 7 papillomi : 3 fibroadenosi : 2 iperplasia : 2 malignant lesions : 102 infiltrating carcinomas : 61 multifocal infiltrating carcinomas : 6 ductal carcinomas in situ : 35 lesioni maligne : 102 carcinomi infiltranti : 61 carcinomi infiltranti multifocali : 6 carcinomi duttali in situ : 35 g . 
in 68 cases , specimen radiography did not raise a suspicion of infiltrated margins : the excision was extended intraoperatively as a precautionary measure in eight cases , whereas it was not extended in the remaining 60 cases ( table 2 )  . 
there were 13 false negatives [ six ductal carcinoma in situ ( dcis ) , three infiltrating multifocal carcinomas and four infiltrating carcinomas ] and nine false positives , leading to sensitivity and specificity values of 66% and 86% , respectively , and positive and negative predictive values of 74% and 81% , respectively . histological assessment of resection margins overall , histological assessment of resection margins for the entire series , including the cases of immediate reexcision , yielded a diagnosis of positive margins in 23 patients ( 23% ) and negative margins in the remaining 79 cases ( 77% )  . 
in 21 / 34 cases ( 61.67% ) in which intraoperative specimen radiography was suspicious for margin involvement , definitive histology demonstrated negative resection margins : 19 / 21 underwent intraoperative reexcision , as suggested by the radiologists , whereas the remaining 2 / 21 cases did not . 
in 12 / 19 cases ( 63.15% ) with intraoperative reexcision , histological assessment confirmed that the margins of the first surgical specimen were positive ; therefore , in these patients , intraoperative reexcision enabled complete removal of the lesion during the same surgical procedure . 
the reasons for not following the radiologists advice in these 8 / 13 cases were deep infiltration towards the pectoralis fascia in three cases and procedures scheduled as excisional biopsies in extensive ( 48 cm ) intraductal carcinomas with a suspicion of multifocality , later confirmed by definitive histology . 
in 13 / 68 cases ( 19.11% ) with an intraoperative radiographic diagnosis of clear margins , histology revealed that the margins were in fact infiltrated : in four of these cases the surgeon decided to extend the excision intraoperatively as a precautionary measure ; this resulted in complete removal of the lesion during the same operation in three cases , whereas a second surgical procedure was scheduled in one case . 
vi sono stati 13 falsi negativi ( 6 cdis , 3 infiltranti multifocali e 4 infiltranti ) e 9 falsi positivi con valori di sensibilit e specificit rispettivamente del 66% e 86% e valore predittivo positivo e negativo del 74% e 81% . valutazione istologica sui margini di resezione sul totale della casistica la valutazione istologica dei margini di resezione , considerando anche gli ampliamenti , quando effettuati , stata di margini infiltrati in 23 pazienti ( 23% ) mentre nei restanti 79 casi ( 77% ) i margini sono risultati indenni allesame istologico definitivo . 
in 21 / 34 casi ( 61 , 67% ) in cui la diagnosi radiologica intraoperatoria pose il sospetto di margini infiltrati , lesame istologico finale dimostr margini di resezione indenni : 19 / 21 hanno avuto un ampliamento estemporaneo cos come consigliato dai radiologi mentre i restanti 2 / 21 casi , non ampliati , avevano margini negativi . 
in 12 / 19 casi ( 63 , 15% ) con ampliamento estemporaneo , lesame istologico conferm che i margini del primo pezzo anatomico erano positivi : in queste pazienti , pertanto lampliamento estemporaneo ha consentito di radicalizzare le lesioni nella stessa seduta operatoria . 
in questi 8 / 13 casi lindicazione radiologica non fu seguita in quanto : in 3 casi vi era infiltrazione in profondit , verso la fascia del muscolo pettorale mentre nei restanti 5 soggetti lintervento era stato programmato come biopsia escissionale in lesioni g . 
in contrast , of the 70 patients who did not have intraoperative reexcision , 17 ( 24% ) required further treatments to achieve complete lesion ablation : 14 patients underwent repeat surgical procedures and three , with deep lesions infiltrating the pectoralis fascia , were treated with chemoand / or radiotherapy . estese ( da 4 a 8 cm ) rappresentate da carcinomi intraduttali sospettate essere lesioni multifocali cos come confermato dallesame istologico definitivo . 
in 13 / 68 casi ( 19 , 11% ) con una valutazione radiologica intraoperatoria di margini indenni lesame istologico ha rilevato , invece , margini di resezione infiltrati : in 4 di questi casi stato effettuato un prudenziale ampliamento estemporaneo deciso dal chirurgo che in 3 casi ha consentito di radicalizzare la lesione nella stessa seduta mentre in 1 caso stato necessario programmare un secondo intervento . 
in 55 / 68 casi ( 80 , 88% ) con valutazione radiologica intraoperatoria di margini indenni , lesame istologico definitivo ha confermato i reperti radiologici ( fig . 4 ) : in 4 di questi casi , con margini negativi , il chirurgo ha comunque effettuato un ampliamento dellescissione anche se non consigliata dai reperti radiologici . discussion the rates of reintervention to achieve complete excision of a lesion after a histological diagnosis of positive resection margins are reported to be 30%85% among women who have undergone breast - conserving surgery [ 7 , 8 ]  . 
to reduce these rates , much emphasis has been placed on the intraoperative assessment of resection margins [ 9 ] , even though the risk of local recurrence is not solely correlated with margin status . 
in altre 3 pazienti ( 3% ) con margini di resezione infiltrati in profondit , verso la fascia del muscolo pettorale , il controllo dei margini di resezione infiltrati stato effettuato con radio e / o chemioterapia . 
fragment of mammary parenchyma ( left q - 1 ) containing the lesion identified at baseline : spiculations are seen close to the section surface in the lower dorsal position . 
radiografia pezzo operatorio ( a proiezione cranio caudale ; b proiezione laterale ) : frammento di parenchima mammario ( q1 sinista ) nella cui compagine si rileva la lesione riconosciuta nellesame di base con alcune spicule marginali in prossimit della superficie di taglio in sede dorsale inferiore . 
 [ 18 ] , in a study comprising only dcis , state that intraoperative radiography substantially reduces reintervention rates ( 22% ) and report achieving complete excision in 84% of patents who underwent intraoperative reexcision . 
nonetheless , the authors also state that radiological assessment alone is not sufficient , above all in ductal carcinomas in situ : in these cases , radiography may produce a substantial rate of false negative results , especially when calcifications are lacking due to the absence of necrosis . 
in addition , the authors conclude that only the long - term follow - up of these patients will be able to establish whether intraoperative assessment of margin status and immediate reexcision are truly useful in reducing local recurrence rates . in our study , the sensitivity , specificity and diagnostic accuracy of intraoperative specimen radiography before immediate reexcision , when done , were 66% , 86% and 78% , respectively , with a positive predictive value of 74% and a negative predictive value of 81% . 
 intraoperative reexcision modified margin status in in 17 ( 24% ) programmare ulteriori trattamenti per radicalizzare le lesioni : 14 pazienti sono state rioperate e 3 , con lesioni profonde infiltranti la fascia del muscolo pettorale , sono state trattate con chemioe / o radioterapia . discussione in letteratura sono riportate percentuali di reinterventi comprese tra il 30% e l85% in pazienti precedentemente sottoposte a chirurgia conservativa della mammella per radicalizzare lesioni quando lesame istologico dimostra margini di resezione infiltrati [ 7 , 8 ]  . 
per ridurre questa percentuale si data molta importanza alla valutazione intraoperatoria dei margini di resezione [ 9 ] anche se il rischio di recidiva locale non da correlare unicamente allo stato dei margini del pezzo operatorio . 
in particolare stato dimostrato che , specie nei carcinomi duttali in situ , la mammografia pu sottostimarne lestensione [ 1012 ] in rapporto alla multifocalit di questo istotipo , specie nelle pazienti di giovane et [ 13 ]  . 
in letteratura alcuni autori hanno riportato la scarsa utilit della radiografia del pezzo operatorio negli interventi di lesioni mammarie non palpabili : in alcuni lavori [ 14 , 15 ] sono state effettuate le radiografie in ununica proiezione e , in unaltro [ 16 ] , senza la tecnica dellingrandimento diretto . altri autori [ 17 ] sostengono invece di aver ridotto la percentuale di reinterventi , dal 12% al 5% , nelle pazienti sottoposte a chirurgia conservativa grazie alla valutazione rag . 
fragment of mammary parenchyma ( right q12 ) with microcalcifications close to outer marghistological examination : multiple foci of well - differentiated cribriform ductal carcinoma in situ ( dcis ) with foci in the axially portion . 
radiografia pezzo operatorio ( a proiezione cranio caudale ; b proiezione laterale ) : frammento di parenchima mammario ( q1 - 2 destra ) con alcune microcalcificazioni in prossimit del margine esterno . 
on the other hand , the radiological indication for immediate reexcision resulted in overtreatment in seven patients , with a probable impact on the final cosmetic outcome due to the removal of excessive breast tissue . the 13 false negative cases at intraoperative radiography were six intraductal carcinomas without microcalcification on the resection margins and seven infiltrating ductal carcinomas , three of which were multifocal . 
overall , our rate of reintervention due to infiltrated resection margins after breastconserving surgery ( 20% ) , which included both intraductal carcinomas and infiltrating ductal carcinomas , is in line with previous reports . 
the use of digital mammography , so far diologica intraoperatoria dei margini di resezione effettuata nelle due proiezioni ortogonali e con la tecnica dellingrandimento diretto ( 1 , 9 )  . 
 [ 18 ] , in una casistica rappresentata solo da carcinomi duttali in situ , affermano che la radiografia intraoperatoria riduce sensibilmente la percentuale di reinterventi ( 22% ) e riportano una percentuale dell84% di pazienti che , sottoposte ad un ampliamento dellescissione nella stessa seduta operatoria , hanno avuto un intervento radicale . 
nonostante questi dati , gli autori affermano peraltro che la valutazione radiologica non sufficiente , specie per quanto riguarda i carcinomi duttali in situ : lesame radiografico in questi casi pu essere gravato di una sensibile percentuale di falsi negativi specie nei casi in cui , per assenza di necrosi , mancano le microcalcificazioni . 
3a , b allargamento richiesto per sospetto radiologico di margini di resezione infiltrati . radiografia pezzo operatorio ( a proiezione cranio caudale ; b proiezione laterale ) : frammento di parenchima mammario ( q1 - 2 destra ) nella cui compagine si rilevano tutte le microcalcificazioni riscontrate nellesame di base : alcune microcalcificazioni si proiettano in prossimit del margine posteriore . 
esame istologico : carcinoma duttale infiltrante con margini di resezione indenni . della valutazione intraoperatoria dei margini di resezione e della rescissione estemporanea nel ridurre la percentuale di recidive locali . nel nostro studio i valori di sensibilit , specificit e accuratezza diagnostica dellesame radiologico del pezzo operatorio prima degli ampliamenti , quando effettuati , sono risultati essere , rispettivamente , del 66% , 86% e 78% con un valore predittivo positivo del 74% e valore predittivo negativo dell81% . 
la valutazione radiologia intraoperatoria stata utile per i chirurghi che hanno effettuato ampliamenti di escissione nella maggior parte dei casi in cui stata posta lindicazione radiologica . limited to a small number of centres due to its high costs , is likely to improve the results of the assessment of both intraductal and infiltrating ductal lesions , as previously reported [ 19 , 20 ] , on account of its high - contrast resolution , which is markedly higher than that of analogical mammography . conclusions it is generally accepted that during surgery for impalpable breast lesions , specimen radiography should be performed g . 
per contro , sulla base delle indicazioni radiologiche , in 7 pazienti vi stato un sovratrattamento che , verosimilmente , ha inciso sugli esiti estetici finali a causa di una eccessiva exeresi di parenchima mammario . i 13 casi che sono risultati falsi negativi alla radiografia intraoperatoria erano rappresentati da 6 carcinomi intraduttali senza microcalcificazioni sui margini di resezione e da 7 carcinomi duttali infiltranti di cui 3 multifocali . 
complessivamente nella nostra casistica , composta sia da carcinomi intraduttati sia da carcinomi duttali infiltranti , la percentuale di reinterventi per margini di resezione infiltrati dopo chirurgia conservativa ( 20% ) rientra in quanto riportato dalla letteratura . 
radiografia pezzo operatorio : frammento di parenchima mammario ( q1 sinistra ) che presenta , in posizione centrale , tutto il gruppo di microcalcificazioni rilevato nellesame di base con margini di resezione giudicati radiograficamente indenni . 
this ensures reasonable certainty of the adequacy of the excision , with a consequent reduction in reinterventions to achieve complete excision and in the risk of local recurrences . our results , which allowed us to reduce our rate of reintervention from 31% to 20% , in agreement with previous reports , are , however , susceptible to improvement to reduce the rate of false negatives due to the seven infiltrating ductal carcinomas . 
mazzarella , istituto di radiologia universitaria , azienda ospedaliero - universitaria santa maria della misericordia di udine , universit degli studi di udine , i - 33100 udine , tel . : + 39 - 0432 - 559266 , fax : + 39 - 0432 - 559867 , e - mail : radiologia.segr@med.uniud.it received : 28 july 2006 / accepted : 22 november 2006 / published online : 20 april 2007 abstract the introduction of systems for automated reading in mammography has been proposed to improve the sensitivity [ computer - aided detection ( cade ) systems ] and , more recently , the specificity [ computer - aided diagnosis ( cadi ) systems ] of the test . 
therefore the role of these systems in clinical practice is still debated , and their real contribution to the overall management of the diagnostic process is not yet clear . key words mammography breast cancer screening cade cadi artificial intelligence computer vision riassunto lintroduzione di sistemi di lettura automatizzata in mammografia stata da tempo proposta per aumentare la sensibilit del test ( sistemi cade , computer - aided detection ) e , pi recentemente , la sua specificit ( sistemi cadi , computer - aided diagnosis )  . 
tali sistemi sono ancora oggetto di discussione . molti studi hanno dimostrato che ne traggono giovamento i lettori in formazione e che , dal confronto con il computer , i radiologi sono indotti a migliorare la propria performance . 
il ruolo di tali sistemi quindi ancora dibattuto e il loro reale contributo al management complessivo del processo diagnostico non ancora chiaro . parole chiave mammografia tumore della mammella screening cade cadi intelligenza artificiale visione computerizzata introduction introduzione breast cancer is the second most common cause of cancer death in women [ 1 ]  . 
in fact , some of these unappreciated or unrecognised very subtle signs may have been seen by the readers but dismissed as being insignificant , but others may be strongly suspicious [ 24 ]  . 
thus , the basis of the problem is not having detected a potential abnormality or having failed in interpreting it ( that is , having misunderstood its nature )  . 
 therefore , a lesion can be missed owing , on the one hand , to mistakes in the visual search ( responsible for 30% of failures ) , and on the other hand , to mistakes in interpretation ( 70% of failures ) [ 6 ]  . 
the former may still be defined as perceptual errors ( the radioloists gaze lands on the location of the lesion for a time insufficient for its recognition ) and the latter as decision - making errors ( the lesion is detected , but a covert negative decision is made ) [ 7 ]  . different methods to reduce the likelihood of errors have been analysed : in the first place , double reading , which provides either double perception or double interpretation of lesions . 
it has been demonstrated that a single radiologist is more accurate when reading mammograms methodically than quickly and that two observers achieve an improvement in detection rate of 5%15% [ 810 ]  . 
furthermore , different readers miss different cancers , as is evidenced by the success of double reading , in which two readers independently read the films [ 11 ]  . 
the most accurate method of interpretation is double reading with arbitration , in which a third reader reviews cases about which the two readers disagree [ 11 , 12 ]  . 
this is a complex and time - consuming method , so that double reading , if performed without an efficient system , may be not only cost ineffective but even expensive and counterproductive . the development of computerised systems as second reader is an alternative . 
researchers have been developing algorithms to detect mammographic abnormalities for more than 30 years with the aim of either automating mammographic interpretation or , more realistically , providing a tool that will enhance human film - reading accuracy . 
a benchmark against which the efficacy of such tools can be measured is whether or not the accuracy of an individual reader could be improved to the extent that double reading was no longer necessary , as this would alleviate any shortage of film readers [ 5 ]  . 
the computer can detect cancers missed by the human reader , but not at the cost of producing too many false positives and thus an unacceptable amount of recalls . strutturale della mammella , sottigliezza dei reperti , affaticamento del radiologo [ 4 ]  . molti studi riportano che fino al 70% dei cancri persi allo screening sono visibili retrospettivamente sulla mammografia precedente [ 3 ]  . 
la mancata individuazione da parte dei radiologi condizionata dalla loro capacit di percezione , a sua volta influenzata dalla propria consapevolezza della prevalenza del cancro e dalla propria soglia decisionale [ 5 ]  . 
infatti , alcuni segni non valorizzati e / o riconosciuti , molto sottili , possono essere stati notati dai lettori e considerati non significativi , ma altri possono essere chiaramente sospetti [ 24 ]  . 
quindi il problema si basa sul non avere individuato una potenziale anormalit , oppure sulla mancanza di una sua corretta interpretazione ( ovvero non avere inquadrato la sua natura )  . da un lato , pertanto , una lesione pu non essere identificata per errori di strategia di ricerca ( responsabili del 30% delle mancate identificazioni ) , dallaltro per errori di interpretazione ( 70% degli errori ) [ 6 ]  . 
i primi possono essere ancora definiti come errori di percezione ( lo sguardo si posa sulla lesione , ma per un tempo insufficiente a riconoscerla ) ed i secondi come errori decisionali ( la lesione individuata , ma viene interpretata erroneamente come reperto negativo ) [ 7 ]  . sono stati analizzati diversi metodi per ridurre la probabilit di errore , in primo luogo la doppia lettura , che consente di acquisire o una doppia percezione della lesione o una sua doppia interpretazione . 
stato dimostrato che un singolo lettore che legge le mammografie metodicamente pi accurato di uno che le legge rapidamente ; tuttavia due lettori ottengono comunque un incremento del tasso di individuazione del 5%15% [ 810 ]  . 
il pi accurato metodo di interpretazione la doppia lettura con arbitraggio , in cui un terzo lettore rivede i casi su cui c disaccordo tra i primi due [ 11 , 12 ]  . 
tale metodologia comunque complicata e allunga i tempi , cosicch , se attuata senza un sistema efficiente , pu essere non solo non economica , ma addirittura dispendiosa e controproducente . unalternativa lo sviluppo di sistemi computerizzati che fungano da secondo lettore . 
i ricercatori da pi di 30 anni stanno elaborando algoritmi che individuino anormalit mammografiche , allo scopo di automatizzarne linterpretazione o , pi realisticamente , fornire uno strumento che potenzi laccuratezza umana di lettura dimmagine . 
un punto di riferimento rispetto al quale si pu misurare lefficacia di questi strumenti la loro capacit di migliorare laccuratezza di un singolo lettore a tal punto che non sia pi necessaria la doppia lettura , il che porrebbe rimedio alla scarsit di lettori , eliminando il secondo lettore [ 5 ]  . 
il computer potrebbe identificare cancri sfuggiti al lettore umano , ma non al prezzo di introdurre troppi falsi positivi e quindi un numero inaccettabile di richiami . le tecniche di computer - aided detection ( cade ) sono state applicate a una variet di immagini mediche , ma sono usate pi ampiamente in mammografia , dove i segni di cancro della mammella in stadio iniziale sono spesso molto fini . 
consigliabile che il radiologo legga la mammografia prima di vedere i risultati del cad e , solo successivamente , guardi i suggerimenti del computer e rivaluti le aree segnalate , in modo da rifiutarle o considerarle per richiamare la paziente . 
lo scopo del cad quello di attirare lattenzione del lettore su regioni potenzialmente anormali e di aumentare il grado di sospetto per segni di anormalit che sono stati visti , ma scartati come probabilmente normali . 
i sistemi computerizzati di analisi mammografica possono essere classificati in due categorie : sistemi cade ( computer - aided detection ) : identificano in modo computerizzato possibili anomalie mammografiche ; sistemi cadi ( computer - aided diagnosis ) : aiutano il radiologo a definire il grado di sospetto di una lesione identificata . in entrambi i casi il presupposto rappresentato dallanalisi computerizzata delle mammografie . analisi computerizzata delle mammografie le immagini mammografiche digitali possono essere analizzate dai sistemi computerizzati attraverso due processi , spesso interconnessi tra loro : visione computerizzata ; intelligenza artificiale . la visione computerizzata comincia con uno stadio di processazione [ 16 ] : le caratteristiche importanti dellimmagine vengono esaltate , quelle secondarie vengono de - enfatizzate . segue una fase detta di segmentazione , che separa le immagini in regioni con caratteristiche simili . 
degli algoritmi computerizzati , attraverso gli indici numerici ottenuti , fanno una stima della probabilit di malignit di una lesione . le tecniche di intelligenza artificiale sono utilizzate per convertire le misure derivanti dalla visione computerizzata in risultati diagnostici , grazie a reti neurali artificiali applicate agli algoritmi per la identificazione o caratterizzazione di lesioni sulla mammografia . 
le reti neurali artificiali sono programmi computerizzati che identificano relazioni tra i parametri di input e gli output desiderati ( come i reperti mammografici e la loro probabilit di malignit )  . 
1 esempio di segnalazioni di un sistema di computer - aided detection ( cade ) : le microcalcificazioni sono indicate da rettangoli , le masse da cerchi . computer - aided detection ( cade ) techniques have been applied to a variety of medical images but are used most widely in mammography , where signs of early breast cancer are often very subtle . 
the radiologist is expected to read mammograms before viewing the cad results and only later to look at the cad prompts , reviewing prompted areas to either dismiss them or to take them into consideration for recalling patients . 
the purpose of cad is to attract the readers attention to potentially abnormal regions and to increase the degree of suspicion associated with signs of abnormality that had previously been seen but dismissed as probably normal by the reader . 
computerised systems for mammographic analysis may be classified in two categories : cade systems , which perform a computerised detection of possible mammographic abnormalities computer - aided diagnosis ( cadi ) systems , which help radiologists define the grade of suspiciousness of a detected lesion . 
in both cases , the basis lies in the computer analysis of mammograms . computer analysis of mammograms mammographic images in digital format can be analysed by computer systems using two kinds of techniques , often enmeshed with each other : m . 
computer algorithms estimate the likelihood of malignancy of a lesion , thanks to the numerical indices generated . artificial intelligence techniques are used to merge computer vision measures into diagnostic output , thanks to artificial neural networks applied in algorithms for the detection or characterisation of lesions in mammography . 
different forms of artificial intelligence can also be combined to classify abnormalities more accurately than any individual approach [ 18 ]  . in summary , the information contained within images undergoes ( 1 ) elaboration , ( 2 ) extraction of parameters about image features and ( 3 ) classification of these parameters in terms of probability of lesion . 
the chosen threshold value will affect the systems sensitivity and specificity : the lower it is , the higher its sensitivity and the lower its specificity ( more false positives )  . so , classification of lesions results from a compromise between threshold value and an acceptable false positive rate [ 19 ]  . cade systems ( computer - aided detection ) cade systems localise on image areas of potential abnormalities , leaving the final decision to the radiologist . 
nel leggere le immagini , la rete neurale artificiale attribuisce ad ogni elemento un valore numerico , che pi alto pi sospetto ; viene fissata una soglia per tale valore , oltre la quale la regione corrispondente classificata come sospetta . 
la soglia prescelta condizioner sensibilit e specificit del sistema : pi essa bassa , maggiore sar la sensibilit e minore la specificit ( aumento dei falsi positivi ) , e viceversa . 
la classificazione delle lesioni deriva quindi da un compromesso tra soglia e numero di falsi positivi ritenuto accettabile [ 19 ]  . sistemi cade ( computer - aided detection ) i sistemi cade localizzano sulle immagini aree di potenziale anormalit , lasciando la decisione finale al radiologo . 
sono stati messi a punto molteplici algoritmi con questo scopo , volti ad individuare masse o calcificazioni . identificazione di masse la presenza di una massa il pi importante segno mammografico di tumore . 
regions labelled as suspicious by detection algorithms are not necessarily malignant . a number of algorithms are designed to detect particular kinds of masses , such as spiculated masses , because of their high likelihood of malignancy . 
the edge orientation can be computed in many different ways : using standard deviation of a local edge orientation histogram and spatial filters [ 22 ] ; statistical analysis of a map of pixel orientations computed at three spatial scales [ 23 ] ; extracting four features for each pixel at a multiresolution representation of mammograms using the discrete wavelet transform [ 24 ]  . other algorithms have been developed for the detection of not only spiculated masses . 
suspicious regions can be segmented by adaptive grey - level thresholding and then classified by a fuzzy binary decision tree , using features based on shape , size and contrast [ 21 ]  . 
mammograms can be divided into three categories ranging from fatty to dense tissue by histogram analysis techniques ; multiple threshold values are used to detect potential masses [ 25 ]  . 
pixel - based methods have the disadvantage of being computationally intensive . in region - based detection methods , regions of interest ( rois ) are extracted by segmentation or filtering technique . then , features describing important information ( such as shape and texture ) are extracted for each region , which is classified as suspicious or not . 
several methods are based on matched filtering : the image is filtered with a filter used as a model for a mass , and the output should correspond to the central dense nucleus in the hypothetical mass ; thus rois are defined . 
such methods can use an iris filter [ 27 ] , an adaptive densityweighted contrast - enhancement filter to enhance objects and suppress background structures , coupled with a simple edge detector [ 28 ] , or a single difference of gaussian ( dog ) filter to detect masses of approximately 1 cm in diameter , then classified by features based on size , contrast , circularity and laws texture features [ 29 ]  . 
lorientamento del margine pu essere calcolato in molti modi diversi : usando la deviazione standard di un istogramma di orientamento locale del margine e filtri spaziali [ 22 ] ; con lanalisi statistica di una mappa dellorientamento dei pixel calcolata su tre scale spaziali [ 23 ] ; estraendo quattro caratteristiche per pixel , su una rappresentazione mammografica a risoluzione multipla usando la trasformata wavelet discreta [ 24 ]  . sono stati sviluppati altri algoritmi per lidentificazione non solo di masse spiculate . 
le regioni sospette possono essere segmentate per mezzo di valori soglia di grigio di tipo adattativo e quindi classificate con un albero decisionale binario di tipo fuzzy , usando caratteristiche basate su forma , dimensioni e contrasto [ 21 ]  . 
si possono dividere le mammografie in tre categorie , da tessuto adiposo a tessuto denso , con tecniche di analisi di istogramma ; si usano multipli valori soglia per individuare potenziali masse [ 25 ]  . 
i metodi basati su pixel hanno lo svantaggio di richiedere unelevata complessit di calcolo . nei metodi basati su regione , le regioni di interesse ( roi , region of interest ) vengono estratte con tecniche di segmentazione o di filtro . 
molti metodi si basano sul filtraggio combaciato : allimmagine si applica un filtro che funge da modello di una massa e il risultato dovrebbe corrispondere al nucleo centrale denso dellipotetica massa ; in tal modo si definiscono delle regioni di interesse . 
questi metodi possono usare : un filtro a iride [ 27 ] ; un filtro adattativo di esaltazione del contrasto , per esaltare gli oggetti e sopprimere le strutture dello sfondo , associato ad un rivelatore di margini [ 28 ] ; un filtro dog ( difference of gaussian ) singolo , per individuare masse di circa 1 cm , poi classificate in base a dimensioni , contrasto , circolarit e caratteristiche strutturali laws [ 29 ]  . 
i metodi basati su regione sono vantaggiosi , dato che tengono conto delle dimensioni e della morfologia del reperto e richiedono processi di calcolo meno complessi dei processi basati su pixel . 
sia i metodi basati su pixel , sia quelli basati su regione hanno il limite di non compiere unanalisi su una gamma continua di scale , mentre le lesioni tumorali sono fenomeni biologici stocastici , che nelle immagini corrispondono a varie strutture e dimensioni distribuite su gamme di scale spaziali [ 20 ]  . i metodi sopra descritti compiono unanalisi su di una singola immagine mammografica . 
both pixel - based and region - based methods have the limitation that the analysis is not made over a continuous range of scales , whereas cancerous lesions are stochastic biological phenomena , corresponding , on images , to various structures and sizes over ranges of spatial scales [ 20 ]  . previously described methods perform analysis on a single mammograsome researchers have developed methods that use multiple images , analysing the symmetry between corresponding mammograms of each breast [ 34 ] or comparing current and prior images [ 35 ]  . 
nevertheless , such methods require difficult preprocessing steps . classification of suspicious regions the classification of suspicious regions as a mass or normal tissue is the second stage of mass - detection algorithms ; its purpose is to reduce the number of false positives . 
for this task , a neural network [ 36 ] or a template - matching technique [ 37 ] can be used . detection of microcalcifications microcalcifications are small calcium deposits due to benign or malignant processes . 
their main characteristics are size , shape or morphology , number and distribution . their size varies from 0.1 mm to 1 mm ( average 0.3 mm ) ; very small ones may be missed , especially if dense breast parenchyma overlaps . 
a number of effective methods have been designed for their detection based on localisation of high spatial frequencies ( wavelet transform ) falling within the range corresponding to microcalcifications [ 20 ]  . 
the effectiveness of the wavelet transform in the detection of microcalcifications , viewed as point discontinuities ( bright dots in the grey background of fat on usual images ) , is not found in the detection of masses , viewed as edges [ 3841 ]  . other multiscale and nonwavelet - based methods have been developed [ 42 , 43 ] based on the fact that calcifications have much higher intensity values than the surrounding tissue , but they are more likely to fail in detecting microcalcifications in dense background tissue . 
as for mass - detection methods , also for microcalcifications , a number of techniques to reduce false positives have been developed by classifying rois as containing microcalcifications or normal tissue [ 20 , 44 ]  . 
an enhancement stage ( global or local ) often messo a punto metodi che utilizzano immagini multiple , analizzando la simmetria fra le corrispondenti mammografie dei due lati [ 34 ] o paragonando le immagini attuali con le precedenti [ 35 ]  . 
tali metodi si basano per su complicati passaggi di pre - processing . classificazione delle regioni sospette la classificazione delle regioni sospette come massa o tessuto normale rappresenta il secondo passaggio degli algoritmi di identificazione ; il suo scopo ridurre il numero di falsi positivi . 
a tal fine si pu usare una rete neurale [ 36 ] o una tecnica di corrispondenza a una sagoma [ 37 ]  . identificazione di microcalcificazioni le microcalcificazioni sono piccoli depositi di calcio dovute a processi benigni o maligni . 
le dimensioni variano da 0 , 1 mm a 1 mm ( in media 0 , 3 mm ) ; quelle pi piccole possono sfuggire , specialmente se si sovrappone parenchima mammario denso . 
sono stati elaborati molti metodi efficaci per la loro identificazione , basati sulla localizzazione di frequenze spaziali elevate ( trasformata wavelet ) che rientrano nel range di rappresentazione delle microcalcificazioni [ 20 ]  . 
lefficacia della trasformata wavelet nel riconoscimento delle microcalcificazioni , viste come discontinuit puntuali ( punti bianchi sullo sfondo grigio del grasso nella rappresentazione usuale ) , non trova invece riscontro nella ricerca delle masse , che si manifestano come discontinuit a fronte [ 3841 ]  . sono stati proposti metodi di altro tipo , multi - scala e non basati sulla trasformata wavelet [ 42 , 43 ] , che sfruttano il fatto che le calcificazioni hanno valori di intensit molto pi alti del tessuto circostante , ma che hanno maggiore probabilit di fallire in caso di microcalcificazioni su uno sfondo di tessuto denso . 
come per i metodi di ricerca delle masse , anche per le microcalcificazioni si sono elaborate delle tecniche per ridurre i falsi positivi , attraverso la classificazione delle roi come contenenti microcalcificazioni o tessuto normale [ 20 , 44 ]  . 
il limite di questi metodi che essi esaltano non solo le calcificazioni , ma anche la struttura di sfondo e il rumore [ 20 ]  . sistemi cadi ( computer - aided diagnosis ) una volta identificato un reperto come potenzialmente anormale , bisogna caratterizzarlo , per poter decidere la gestione della paziente . 
gli scopi dei sistemi cadi sono : evitare che il radiologo classifichi come benigna una lesione maligna ; ridurre il numero di biopsie consigliate per lesioni in realt benigne ( ma senza ridurre la sensibilit )  . 
in such methods , the limitation is that they enhance not only calcifications but also background structure and noise [ 20 ]  . cadi systems ( computer - aided diagnosis ) once a finding has been identified as potentially abnormal , it must be characterised to allow patient management decision making . 
the aims of cadi systems are to prevent a malignant lesion from being characterised as benign by the radiologist and to reduce the number of biopsy recommendations for benign lesions ( but with no reduction of sensitivity )  . 
to characterise an roi as benign or malignant , a number of roi features ( extracted by computer vision techniques ) are used by artificial intelligence techniques ( such as artificial neural networks )  . the output of cadi systems can take different forms , such as the estimated likelihood of malignancy or a visual aid for the radiologist in decision making ( by displaying a variety of known lesions similar to the one at hand ) [ 4 ]  . diagnosis of masses masses are characterised by their shape ( round , oval , lobular , irregular ) and margins or boundary ( circumscribed , microlobulated , obscured , indistinct , spiculated ) [ 46 ]  . 
usually , the diagnostic process consists of three stages : ( 1 ) segmentation of mass boundary in roi , ( 2 ) feature extraction and ( 3 ) classification [ 20 ]  . segmentation mass segmentation may be manual , semiautomated or fully automated . 
the area overlap measure is used to report the performance of segmentation algorithms : it is the ratio of the area segmented automatically to the area segmented manually by an experienced radiologist . 
however , as there is interobserver variability in the manual segmentation by radiologists , it is more appropriate to evaluate whether the variance between the boundaries marked by a radiologist and a computer falls within the variance between radiologists [ 20 , 47 , 48 ]  . 
other segmentation algorithms can use fuzzy region - growing methods , shape and texture features based on grey - level cooccurrence matrices and region - growing techniques based on radial gradient or on simple probabilistic models [ 20 ]  . feature extraction several features extracted for diagnosis concern morphology and texture . 
textural features have been designed to capture important differences between malignant and benign masses that may not be evident to the huroi benigna o maligna , varie caratteristiche della roi ( estratte con tecniche di visione computerizzata ) vengono utilizzate da sistemi di intelligenza artificiale ( come reti neurali artificiali )  . loutput dei sistemi cadi pu essere di vario tipo , come una stima della probabilit che una lesione sia maligna oppure un aiuto visivo per il radiologo nel prendere una decisione ( mostrando una variet di lesioni note , simili a quella sotto esame ) [ 4 ]  . diagnosi di masse le masse si caratterizzano per la loro forma ( rotondeggiante , ovalare , lobulata , irregolare ) e per i margini ( circoscritti , microlobulati , mascherati , indistinti , spiculati ) [ 46 ]  . 
la misura dellarea di sovrapposizione si usa per esprimere la performance degli algoritmi di segmentazione : essa il rapporto tra larea segmentata automaticamente e quella segmentata manualmente da un radiologo esperto . 
tuttavia , essendoci variabilit interosservatore nella segmentazione manuale dei radiologi , pi appropriato valutare se la varianza tra i confini demarcati da un radiologo e quelli definiti da un computer rientra nella varianza tra radiologi [ 20 , 47 , 48 ]  . 
altri algoritmi di segmentazione possono usare : metodi fuzzy region growing ; caratteristiche morfologiche e strutturali basate su matrici di concomitanza di livelli di grigio ; tecniche region growing basate su gradiente radiale o su modelli probabilistici semplici [ 20 ]  . estrazione di caratteristiche molte delle caratteristiche estratte per la diagnosi riguardano morfologia e struttura . 
molti metodi calcolano queste caratteristiche a partire da matrici di concomitanza di livelli di grigio ( analisi di densit ) [ 20 ]  . classificazione le tecniche pi usate per classificare le masse come benigne o maligne impiegano reti neurali artificiali o lanalisi discriminante lineare . 
a number of methods compute these features from grey - level cooccurrence matrices ( density analysis ) [ 20 ]  . diagnosi di microcalcificazioni classification the most used techniques for classifying masses as benign or malignant employ artificial neural networks or linear discriminant analysis . 
other methods have also been considered for classifying masses into other categories : distinction between round , nodular or stellate masses ; classification of masses as fibroadenoma , cyst or cancer ; characterisation of the roughness of tumour boundaries [ 20 , 49 ]  . le microcalcificazioni in mammografia possono apparire come individuali o raggruppate in cluster ( tre o pi microcalcificazioni in unarea di 1 cm2 )  . 
the following steps are ( 1 ) segmentation of individual microcalcifications , ( 2 ) feature extraction and ( 3 ) classification [ 46 , 20 ]  . segmentation of individual microcalcifications segmentation is based on the analysis of the properties of individual calcifications ; it is difficult to perform due to the small size of microcalcifications , and probably it is of low interest , as the properties of the whole cluster are more useful for diagnosis than those of individual microcalcifications [ 20 ]  . feature extraction the features to be considered regard morphology and texture . 
morphological features depend on the effectiveness of the segmentation algorithsome common cluster features are number of microcalcifications , mean diameter of microcalcification area , standard deviation ( sd ) of their contrast and number of microcalcifications per unit area [ 20 ]  . classification a variety of methods for automatically classifying microcalcifications clusters as benign or malignant have been developed . 
thus , researchers have developed algorithms that do not use shape features but , for example , image structure features or cluster features [ 53 ]  . la segmentazione si basa sullanalisi delle propriet delle singole calcificazioni , difficile da eseguirsi per le loro piccole dimensioni e , verosimilmente , di scarso interesse , data la maggior importanza , ai fini diagnostici , rivestita dallintero cluster , piuttosto che dal singolo elemento [ 20 ]  . estrazione di caratteristiche le caratteristiche da considerare sono morfologiche e strutturali . 
alcune propriet frequentemente considerate per i cluster sono : numero delle microcalcificazioni , diametro medio dellarea delle microcalcificazioni , deviazione standard del loro contrasto , numero di microcalcificazioni per unit di superficie [ 20 ]  . classificazione esistono vari metodi per classificare automaticamente le microcalcificazioni come benigne o maligne . 
nel valutare la performance di un algoritmo cad , importante tener conto della sua sensibilit e specificit , oltre che del tipo di casi che costituiscono il database sotto esame . 
when evaluating the performance of a cad algorithm , it is important to consider its sensitivity and specificity , as well as the nature of the cases in the database under study . 
the performance of cad systems can be evaluated in two ways : by measuring the algorithy performance or by monitoring the performance of readers using the system [ 15 ]  . evaluation of algorithm performance to evaluate cad algorithm performance , algorithms are applied to a set of images , and the response to known truth is measured . 
in practice , a combination of random sampling and selection provides the best compromise between efficiency and accuracy . truth about lesion type is determined by means of pathology reports ; truth about lesion location on mammograms is usually obtained by asking expert mammographic film readers to annotate the images . 
correspondence between the truth and the algorithm response can be evaluated by using free - response receiver operating characteristic ( froc ) curves ( plots of sensitivity versus the number of false positives per image )  . 
this provides a good method of comparing algorithms [ 15 ]  . evaluation of the performance of readers using cad in addition to measuring algorithm performance , it is important to measure the performance of readers using cad . 
in retrospective studies , the inclusion of prior cases ( the previous screening films of subsequently detected cancers ) and sibilit pu non riflettere veramente una buona performance , se nella valutazione sono stati inclusi solo casi con anormalit ovvie . 
la performance dei sistemi cad pu essere valutata in due modi : misurando la performance degli algoritmi o quella dei lettori che li usano [ 15 ]  . valutazione della performance di un algoritmo per valutare la performance di un algoritmo cad , esso viene applicato a un set di immagini e si misura la corrispondenza alla verit nota . 
nella pratica , il miglior compromesso tra efficienza e accuratezza si ottiene combinando campionamento randomizzato e selezione . la verit sul tipo di lesione si determina in base ai referti anatomopatologici , mentre quella sulla sede mammografica delle lesioni si ottiene chiedendo a lettori esperti di mammografie di annotare le immagini . 
la corrispondenza tra verit e risposta dellalgoritmo pu essere valutata con le curve froc ( free - response receiver operating characteristic curves : diagrammi che rappresentano la sensibilit in funzione del numero di falsi positivi per caso )  . 
questo un buon metodo per paragonare gli algoritmi [ 15 ]  . valutazione della performance dei lettori con cad oltre a misurare la performance degli algoritmi , importante misurare quella dei lettori che utilizzano il cad . 
comunque , negli studi retrospettivi molto importante linclusione dei precedenti ( le mammografie di screening antecedenti a quelle della diagnosi di tumore ) e la conoscenza dello stato di tutti i casi ( referti anatomopatologici per le lesioni ; almeno una mammografia di screening negativa per i casi normali )  . 
al contrario , gli studi prospettici simulano ci che accade nella vita reale e nellattivit clinica ; tuttavia , la selezione randomizzata pi laboriosa per i lettori , dato che essi devono vedere un alto numero di casi normali per raggiungere un numero di tumori statisticamente significativo . 
on the contrary , prospective studies simulate what happens in real life and in clinical work ; nevertheless , random selection is more labour intensive for the readers , as they must read a large number of normal cases to reach a statistically significant amount of cancers . 
in both retrospective and prospective studies , if cases used for evaluation without cad and with cad are not the same , the two sets should be equivalent . readers in screening mammography are known to have variability in their performance [ 54 ]  . 
in studies conducted consecutively , comparing unprompted performance over a period with prompted performance over the following period , it should be noted that the readers will be more experienced in the second period . 
in studies in which readers differ in the unprompted and prompted conditions , a bias could also be due to the readers experience , performance and degree of training before starting the trial ( to achieve stable performance ) [ 15 ]  . trials on cade systems several trials have been performed to evaluate the effectiveness of cade systems , with the aim of introducing them into the clinical practice of screening mammography . 
on a set of 286 and 377 missed cancers , respectively , at a retrospective blinded analysis , a sensitivity of 79% [ 3 ] and 75.4% [ 55 ] was calculated for the radiologists without cad , with a false negative rate of 21% [ 3 ]  . 
the conclusions of both studies were that the cad system marked most of cancers missed at screening , so its use theoretically would reduce the false negative rate , particularly for lesions presenting as microcalcifications . 
furthermore , a cad system would significantly improve the radiologists sensitivity and , therefore , be useful in screening mammography , by reducing the number of missed cancers and helping in earlier cancer detection . 
who , in a retrospective study published in 2004 [ 56 ] , found that using two different cad systems tested on 120 mammograms , lutazione senza e con cad non sono gli stessi , i due set dovrebbero essere equivalenti . si sa che la performance dei lettori nello screening mammografico variabile [ 54 ]  . 
negli studi effettuati sequenzialmente , confrontando la performance senza cad nellarco di un periodo con quello con cad nel periodo successivo , si dovrebbe tener conto che i lettori , nel secondo periodo , avranno acquisito maggior esperienza . 
negli studi in cui i lettori con e senza cad sono diversi , un bias potrebbe anche essere dovuto alla diversit tra di loro per esperienza , performance e grado di addestramento che deve essere effettuato prima di iniziare lo studio ( per raggiungere una performance stabile ) [ 15 ]  . studi sui sistemi cade molteplici studi sono stati condotti per valutare lefficacia dei sistemi cade , al fine della loro introduzione nella pratica clinica di screening mammografico . 
la sensibilit stimata per un radiologo con il cad stata quindi del 91 , 4% ( pi alta del 21 , 2% rispetto alla sensibilit senza cad ) [ 55 ]  . 
le conclusioni di entrambi gli studi sono state che il sistema cad ha segnalato la maggior parte dei cancri persi allo screening , quindi il suo uso teoricamente ridurrebbe il tasso di falsi negativi , in particolare per le lesioni che si presentano come microcalcificazioni . 
inoltre , un sistema cad migliorerebbe in modo significativo la sensibilit del radiologo e , quindi , sarebbe utile nella mammografia di screening , riducendo il numero di cancri persi e favorendo la pi precoce scoperta dei tumori . 
 [ 57 ] in 2005 retrospectively investigated the impact of cad on tumours that , undergoing double reading , had been missed by one of the two readers : in a series of 33 such lesions and 75 negative cases , sensitivity was 51.5% for cad alone , 62.5% for radiologists alone and 86.2% for radiologists with cad . 
in particular , for those lesions they had originally missed , radiologists showed a sensitivity of 58.3% without cad and of 100% with cad ( meaning that about half of missed cancers would be detected )  . 
these conclusions are the best obtained theoretically , assuming that the readers would correctly respond to all prompts of the cad systein routine use of cad , as analysed below , this would not happen , and readers are more likely to dismiss the majority of cad prompts instead of correctly responding to the prospective trials are the most informative studies because they are applied to clinical practice . 
the increase in sensitivity related to the use of cad is more realistic in these studies , and the effect of cad systems on recall rates , essential for screening programmes , can be evaluated . 
a subsequent prospective clinical part of the burhenne study [ 3 ] showed no increase in the recall rates using the cad system . this is explained by the fact that cad brings possible lesions to the attention of the radiologist who reevaluates them , dismissing false positive marks . 
over a 12month period , each of 12 , 860 screening mammograms was interpreted by an experienced breast radiologist , first without cad and immediately after using cad , and the effects of cad were evaluated . 
the authors concluded that the use of cad in screening mammography increases the detection of early stage cancers without undue effects on the recall rate or positive predictive value for biopsy . 
 in 2004 , the results of a prospective trial were published showing the effects on recall rate and breast cancer detection rate after the introduction of a cad system into a clinical radiology practice , including all screening mammograms performed during 2000 , 2001 and 2002 [ 59 ]  . 
in this study , not all cases were analysed without and with cad ; the results lettura , erano stati persi da uno dei due lettori : su di un set costituito da 33 di queste lesioni e 75 casi negativi , la sensibilit stata per il cad da solo del 51 , 5% , per i radiologi da soli del 62 , 5% e per i radiologi con cad dell86 , 2% . 
in particolare , per le lesioni che in origine essi avevano perso , i radiologi hanno avuto una sensibilit senza cad del 58 , 3% , con cad del 100% ( si recupererebbero quindi circa la met dei cancri persi )  . 
nellimpiego routinario del cad , come si dir pi avanti , ci non accadrebbe ed pi probabile che i lettori rifiutino la maggior parte dei suggerimenti del cad , anzich rispondere correttamente ad essi . gli studi prospettici sono i pi informativi , perch applicati alla pratica clinica . 
in questi studi , laumento in sensibilit correlato alluso del cad pi realistico e si pu valutare leffetto del sistema cad sul tasso di richiami , essenziale nei programmi di screening . 
questo studio ha dunque mostrato che il cad pu ridurre il tasso di falsi negativi senza aumentare quello di richianel 2001 stato pubblicato il primo studio prospettico che valutava gli effetti del cad sulla lettura delle mammografie di screening in un centro senologico di comunit [ 58 ]  . nellarco di 12 mesi , 12860 mammografie di screening sono state lette ognuna da un radiologo esperto di mammella , prima senza cad e , subito dopo , con cad , e se ne sono valutati gli effetti . 
si osservato : un aumento accettabile del tasso di richiami ( dal 6 , 5% al 7 , 7% , incremento dovuto per met a microcalcificazioni ) ; nessuna modificazione del valore predittivo positivo della biopsia ( 38% ) ; un incremento del 19 , 5% del numero di cancri trovati ; un incremento ( dal 73% al 78% ) della proporzione di tumori scoperti in stadio precoce ( 0 e i )  . 
il fatto che il valore predittivo positivo della biopsia non sia stato influenzato stato spiegato col motivo che le biopsie venivano consigliate , correttamente , sulla base di reperti clinici e dellimaging al momento del richiamo e non considerando se il cad aveva segnalato o meno la lesione . gli autori hanno concluso che lutilizzo del cad nello screening mammografico migliora lindividuazione dei tumori in stadio precoce , senza effetti negativi sul tasso di richiami n sul valore predittivo positivo della biopsia . nel 2004 sono stati pubblicati i risultati di uno studio prospettico che mostrava gli effetti sul tasso di richiami e sul tasso di scoperta di tumori al seno dopo lintroduzione di un sistema cad nella pratica clinica radiologica , includendo tutte le mammografie di screening effettuate nel corso del 2000 , 2001 e 2002 [ 59 ]  . 
in questa analisi non si leggevano tutti i casi senza e con cad ; si sono confrontati i risultati dei casi letti da 24 radiologi senza cad con quelli di un diverso set di mammografie lette con il cad . 
gli esiti senza e con cad erano simili , sia per il tasso di richiami ( 11 , 39% contro 11 , 40% ) sia per il tasso di scoperta dei tumori ( 3 , 49% contro 3 , 55% per 1000 esami di screening )  . 
these observations clearly contrasted with those of freers and ulisseyss trial [ 58 ] in which mammograms were read without cad and immediately reviewed with cad : the authors suggest that such a protocol may have introduced a lower level of vigilance during the initial interpretation . 
 [ 59 ] analysis may have some bias : besides the presence or absence of cad , other differences may have existed between the two groups , such as differences in the number of cases read by certain readers or higher levels of vigilance in the cad group induced by the awareness of participating in a trial . another prospective trial evaluated the effect of cad on screening mammogram interpretation to determine whether the outcome was different from that on clinical mammography [ 61 ]  . 
the third prospective trial [ 60 ] by the same authors was designed to evaluate the impact of cad both on a single reading before and after prompting ( as in freers and ulisseys trial [ 58 ] ) and on two distinct sets of cases ( as in gur et al.s trial [ 59 ] )  . 
there was an increase in recall rate in the cad group compared with the non - cad group but without a statistically significant increase in detection rate , suggesting a negative impact on specificity . 
 [ 59 ] : the outcomes of 19 , 402 screening mammograms interpreted with cad over a 2 - year period were compared with those of 7 , 872 films interpreted without cad freer [ 58 ] , in cui le mammografie venivano lette senza cad e immediatamente rilette con cad : gli autori suggeriscono che un simile protocollo pu avere indotto un minor grado di vigilanza nellinterpretazione iniziale . 
 [ 59 ] pu avere qualche bias : oltre alla presenza o assenza del cad , tra i due gruppi possono esserci state altre differenze , come diversit nel numero di casi visti da alcuni lettori , o livelli di vigilanza maggiori nel gruppo con cad , indotti dalla consapevolezza di stare partecipando a un trial . un altro studio prospettico ha valutato leffetto del cad sullinterpretazione delle mammografie di screening , per capire se esso fosse diverso da quello sulle mammografie cliniche [ 61 ]  . 
il tasso di richiami dopo cad stato del 9 , 9% , leggermente superiore a quello di un simile periodo precedente alluso del cad ( 8 , 4% )  . 
il terzo studio , prospettico , degli stessi autori [ 60 ] stato disegnato per valutare limpatto del cad sia sulla singola lettura prima e dopo segnalazione ( come nel lavoro di freer e ulissey [ 58 ] ) , sia su due distinti set di casi ( come nello studio di gur [ 59 ] )  . 
si osservato un aumento nel tasso di richiami per il gruppo con cad rispetto al gruppo senza cad , senza tuttavia un significativo miglioramento del tasso di identificazione , indicando un effetto negativo sulla specificit . 
in definitiva , nessuno di questi tre studi ha dimostrato un effetto statisticamente significaivo del cad . recentemente un trial ha valutato in modo prospettico leffetto del cad su di un programma di screening mammografico regionale , confrontando i risultati annuali in periodi pre - cad e cad [ 65 ] e paragonando le conclusioni a quelle dei principali studi prospettici condotti in precedenza . 
il disegno dello studio era simile a quello di gur [ 59 ] : esito di 19402 mammografie lette con cad nellarco di 2 anni confrontato con quello di 7872 mammografie lette senza cad nellanno precedente . 
il tasso di riconoscimento nello screening con cad aumentato del 16 , 1% , in accordo con freer e ulissey ( aumento del 19 , 5% ) [ 58 ] , ma in contrasto con gur ( aumento del 1 , 7% ) [ 59 ]  . 
si osservato un aumento , seppur minore , nel tasso di richiami ( 8 , 1% ) , tasso di biopsie ( 6 , 7% ) e valore predittivo positivo delle biopsie ( 8 , 8% )  . gli autori hanno sottolineato alcuni bias del loro studio . data la rarit di tumori nella popolazione sotto screening , per osservare variazioni statisticamente significative servono m . 
the authors concluded that the increase in the proportion of early stage invasive cancers and younger patient age at diagnosis with cad are clinically and statistically significant , indicating the benefit of cad . if the performance of cad systems in the different type of lesions is analysed in detail , it appears to be clear that cad is more sensitive for lesions presenting as microcalcifications than for lesions presenting as masses . 
table 2 shows the results of the different studies comparing the two type of lesions , showing that cad sensitivity for microcalcifications ranges between 86% and 100% , whereas for masses it ranges between 67% and 87% [ 3 , 5861 , 63 , 64 , 6668 ]  . the only surprising finding was reported by birdwell et al . [ 61 ] : in their study , both cancers detected only by cad and missed by screening mammographic reading were masses ; these two lesions were clinically palpable and therefore would not have been missed at clinical evaluation . recently ( 2005 ) , an analysis evaluated the performance of a cad system for the detection of breast cancer based on mammographic appearance and histopathology [ 66 ]  . 
the prognosis was better for masses than for calcifications ( in small invasive tumours ) [ 70 ] , for ductal carcinoma in situ than invasive lesions and for smaller than larger tumours [ 71 ]  . 
so , even though mammographic appearance and histopathology did not appear to affect the overall performance of the cad system ( which showed a high sensitivity in any case ) , results were better for microcalcifications , and the detection rate was higher for dcis ( ductal carcinoma in situ ) and invasive lobular carcinomas . 
this indicated that cad may have an important role in reducing the occurrence of missed cancers , even for lesions that are difficult to detect , and in influencing prognosis . 
trial [ 65 ] in which the detection rate of small invasive cancers ( 1.0 cm or less ) increased ( 164% ) , especially for those with an associated dcis component . 
le differenze osservate nei due gruppi potrebbero essere dovute alla diversa distribuzione tra screening di prevalenza e screening di incidenza ( i tassi di diagnosi sono maggiori nel primo )  . 
comunque gli autori hanno concluso che con il cad vi un aumento clinicamente e statisticamente significativo nella percentuale di cancri diagnosticati in stadio pi precoce e in pazienti pi giovani , affermando il beneficio apportato dal cad . analizzando in dettaglio la performance del cad su diversi tipi di lesioni , sembra chiaro che il sistema pi sensibile per le microcalcificazioni che per le masse . 
la tabella 2 mostra i risultati dei vari studi relativamente ai due tipi di lesioni , mostrando che la sensibilit del cad per le microcalcificazioni va dall86% al 100% , mentre per le masse varia tra il 67% e l87% [ 3 , 5861 , 63 , 64 , 6668 ]  . 
 [ 61 ] : nel loro studio entrambi i cancri visti dal solo cad e persi allo screening erano masse ; comunque queste due lesioni erano clinicamente palpabili e quindi non sarebbero state perse allesame clinico . recentemente ( 2005 ) stata condotta unanalisi della performance del cad nellindividuare il tumore mammario in relazione al suo aspetto mammografico e alla sua istologia [ 66 ]  . 
la prognosi migliore per le masse rispetto alle microcalcificazioni ( nel caso di piccoli tumori invasivi ) [ 70 ] , per il carcinoma duttale in situ rispetto alle lesioni invasive , per i tumori piccoli rispetto ai grandi [ 71 ]  . per quanto riguarda listologia , la sensibilit del cad stata del 95% per il carcinoma duttale in situ , del 95% per il carcinoma lobulare invasivo , dell85% per il carcinoma duttale invasivo e del 90% per il carcinoma mammario invasivo ( ossia con caratteristiche duttali e lobulari )  . 
quindi , pur sembrando che laspetto mammografico e listologia non abbiano influenzato la performance complessiva del cad ( che ha mostrato in ogni caso unalta sensibilit ) , i risultati sono stati migliori per le microcalcificazioni , e il tasso di individuazione stato pi alto per i carcinomi duttali in situ e lobulari invasivi . 
ci indica che il cad pu avere un importante ruolo nel ridurre la frequenza dei cancri persi , anche per lesioni difficili da vedere , e nellinfluenzare la prognosi delle pazienti . 
questi risultati sono stati confermati anche dallo studio di cupples [ 65 ] , in cui il tasso di diagnosi di piccoli tumori invasivi ( 1 , 0 cm o meno ) aumentato ( 164% ) , specialmente per i tumori con associata una componente di carcinoma duttale in situ . 
il tasso di diagnosi di tumori in stadio precoce aumentato per lesioni corrispondenti a piccoli cluster di microcalcificazioni o a piccole masse , o entrambi , avvalorando lipotesi che gli algoritmi cad sono utili per le specifiche morfologie per cui sono stati progettati . stato valutato limpatto sul cad della densit mammaria ( un importante fattore che limita la sensibilit della mammografia ) [ 67 , 68 ]  . 
anyway overall cad detection of breast cancer proved not to be affected by breast density , suggesting that cad may be particularly advantageous in patients with dense breasts . assuming at this point that cad increases the sensitivity of readers in cancer detection , the correct timing in using cad during reading remains to be defined . 
initially , cad was supposed to be used before the radiologists reading in a so - called prereading session , with the aim of dismissing all negative , unprompted cases and to select only cases with prompts to be verified by the radiologist . 
tuttavia , nel complesso , il cad non si dimostrato influenzato dalla densit mammaria nella scoperta di tumori , sembrando quindi particolarmente vantaggioso per le pazienti con seni densi . assumendo , a questo punto , che il cad aumenti la sensibilit dei lettori nellindividuare i tumori , restano da definire i tempi corretti del suo utilizzo durante la lettura . 
inizialmente il cad era inteso come strumento da utilizzare prima della lettura del radiologo , in una sessione cosiddetta pre - lettura , allo scopo di scartare tutti i casi negativi non marcati , e di selezionare solo i casi con segnalazioni , che il radiologo doveva poi verificare . 
infatti , il cad ha perso dal 14% al 16% dei tumori trovati dai radiologi [ 3 , 61 ] , rimarcando il fatto che esso non pu sostituire il radiologo , ma rappresenta un metodo aggiuntivo . 
quindi , come precedentemente sottolineato , il cad dovrebbe essere considerato solo come unalternativa al secondo lettore ; i risultati del cad dovrebbero essere valutati dal radiologo dopo una prima lettura cieca , con lo scopo di riconsiderare aree potenzialmente sospette segnalate dal cad . comunque , questo protocollo presenta di per s delle lim . 
in fact , cad missed 14%16% of cancers detected by the radiologists [ 3 , 61 ] , emphasising that a cad system cannot replace the radiologist but is an adjunct method . 
therefore , as previously highlighted , cad should be considered an alternative to the second reader ; cad results should be viewed by the radiologist after a prior blind reading in order to reconsider areas potentially suspicious prompted by cad . 
in their 2004 study [ 56 ] in which a performance comparison was made not only between two different cad systems but also between cad and a simulation of independent double reading obtained by pairing up the single - radiologist conventional readings . 
this was explained by considering that , whereas double reading may correct certain systematic reading limitations of the single radiologists , in cad reading the readers diagnostic criteria are unchanged . 
 furthermore , the reaction of the radiologist to the several prompts it not obvious : too many prompts may distract the reader instead of attracting his attention , resulting in a nonoptimal use of cad sensitivity . 
this is an automation bias of omission ( failures to respond to system irregularities or events because automated devices fail to detect or indicate them ) that results from cognitive vigilance decrements [ 72 , 73 ]  . 
their data indicated that readers learnt to recognise patterns in shape , frequency and location that characterised false positive prompts and used this to assess the mammogram a priori to decide how much effort to invest in analysing it . 
according to the authors , this is an intuitive reaction , essential for establishing trust in system performance , but it requires a cognitive cost . in a study performed by zheng et al . , the false positive rate seemed to influence the readers ability to correctly classify prompts , but not significantly . 
una di queste stata evidenziata da ciatto et al . nel loro studio del 2004 [ 56 ] , nel quale , oltre a confrontare la performance di due diversi sistemi cad , la si anche paragonata con una simulazione di doppia lettura indipendente ottenuta combinando in coppie le letture convenzionali singole : la doppia lettura risultata pi sensibile , a parit di specificit , della lettura singola con cad . 
ci stato spiegato col fatto che , mentre la doppia lettura permette di correggere eventuali limiti sistematici di interpretazione dei singoli radiologi , nella lettura con cad i criteri diagnostici del lettore rimangono gli stessi . inoltre , la reazione del radiologo a numerose segnalazioni non scontata ; troppi suggerimenti possono distrarre il lettore , anzich attirarne lattenzione , comportando un uso non ottimale della sensibilit del cad . 
taylor e ulissey [ 60 ] hanno notato che unalta percentuale di tumori correttamente segnalati non sono stati richiamati : la spiegazione data che il lettore si sia fidato della sua prima impressione di benignit . la presenza di troppi segnali falsi positivi pu avere effetti negativi sulla performance dei radiologi . 
molte segnalazioni possono essere percepite come distraenti e , a volte , la loro assenza pu essere considerata pi informativa della loro presenza : questo un automation bias di omissione ( mancata risposta a irregolarit di sistema o a eventi , dovuta al fatto che strumenti automatici falliscono nel vederli o indicarli ) che deriva da cali di vigilanza cognitiva [ 72 , 73 ]  . 
secondo gli autori , questa una reazione intuitiva , base essenziale per riporre fiducia nella performance del sistema , ma che richiede un costo cognitivo . in uno studio condotto da zheng et al . , il tasso di falsi positivi parso influenzare labilit dei lettori nel classificare correttamente le segnalazioni , ma non in modo significativo . in questo trial , la performance dei radiologi nellindividuare fini anormalit mammografiche , in condizioni sperimentali , stata testata usando quattro sistemi cad a differenti livelli di tasso di veri positivi e falsi positivi ( quattro combinazioni di tassi alti e bassi ) [ 75 ]  . 
i risultati hanno mostrato come la performance dellosservatore fosse influenzata da quella intrinseca del sistema cad : sistemi ad alta performance possono migliorarla , sistemi a bassa performance peggiorarla . comunque , allaumentare del numero di segnalazioni si osservato un certo incremento del tasso di scarto di veri positim . 
the results showed that observer performance was affected by the inherent performance of the cad system : a high - performance system can improve it , a low - performance system can degrade it . 
once the abnormality was detected , the ability of the observer to classify it as benign or malignant was not significantly affected by the cuing mode . it is important to consider that the false positive rate of a cad system influences the users confidence in it . 
according to manufacturers experience , a false positive rate of nearly three per case is hardly accepted by the users [ 76 ] , and the highest rate tolerable is of about two false marks per case . 
as it has been observed that radiologists use prompts to economise on the effort required to deal with false positive prompts , the training session must provide balance between making an a priori assessment of prompt significance and carefully examining each prompted region . 
radiologists need training to make the best use of cade , that is , using prompts only as an aid for detection and not as evidence for interpretation [ 74 ]  . trials on cadi systems mammography has a poor positive predictive value , so that 65%85% of breast biopsies are performed on benign lesions [ 77 ]  . 
the goal is to reduce the number of false positives , maintaining a high rate of cancer detection . for microcalcifications , algorithms for their detection are better than algorithms for their diagnosis . 
a study published in 2002 compared the performance of a cadi system for diagnosis of previously detected lesions based on radiologistextracted findings on masses and calcifications [ 81 ]  . 
una volta individuata unanormalit , labilit dellosservatore nel classificarla come benigna o maligna non era significativamente influenzata dalla modalit di suggerimento . importante considerare che il tasso di falsi positivi del sistema cad influenza la fiducia degli utenti in esso . 
secondo lesperienza dei costruttori , un tasso di falsi positivi di quasi tre per caso difficilmente accettato dallutente [ 76 ] , e il pi alto tasso tollerabile di circa due per caso . 
queste considerazioni suggeriscono che i sistemi cad implicano il rischio di effetti dannosi sulla performance dei lettori , che si pu ridurre addestrando i radiologi alluso dello strumento . una prima esposizione ai suggerimenti del cad senza alcuna spiegazione pu condurre alla perdita di fiducia nel mezzo e a mancanza di attenzione verso segnalazioni corrette . 
poich si visto che i radiologi usano le segnalazioni per economizzare sullo sforzo di dover gestire i falsi positivi , laddestramento deve permettere di raggiungere un equilibrio tra definizione a priori del significato di una segnalazione e attento esame di ogni area marcata . 
i radiologi necessitano di un training per fare il migliore uso del cade , ossia usarne i suggerimenti solo come aiuto per lindividuazione , e non come evidenza per linterpretazione [ 74 ]  . studi sui sistemi cadi la mammografia ha uno scarso valore predittivo positivo , cosicch il 65%85% delle biopsie mammarie sono fatte su lesioni benigne [ 77 ]  . 
questo accresce il peso emozionale , fisico ed economico che grava su pazienti e cliniche [ 78 , 79 ] e riduce lefficacia dello screening mammografico [ 80 ]  . 
lobiettivo ridurre il numero di falsi positivi , mantenendo un alto tasso di individuazione dei tumori . per le microcalcificazioni , gli algoritmi per lindividuazione sono migliori di quelli per la diagnosi . 
il passaggio pi difficile la segmentazione delle calcificazioni : sarebbero desiderabili caratteristiche tali da impedire errori di segmentazione , cos come caratteristiche di cluster che colgano la disposizione spaziale delle calcificazioni . 
uno studio pubblicato nel 2002 ha comparato la performance di un sistema cadi nel classificare lesioni , precedentemente individuate , in base alle caratteristiche mammografiche di masse e calcificazioni estratte da un radiologo [ 81 ]  . 
la presenza di calcificazioni sovrapposte a una massa pu influenzare la classificazione di quella massa , per cui masse e calcificazioni dovrebbero essere considerate separatamente quando si valuta un sistema cadi . 
these new cases ( not used for classifier training and development and thus unknown to it ) are referred to as validation cases , and the evaluation of new data is referred to as classifier validation [ 82 ]  . 
these results were considered a preclinical success of the classifier as a potential aid in reducing the number of biopsies performed on benign masses and are consistent with those reported by other authors [ 83 ]  . 
a further analysis of the same data [ 85 ] evaluated the effects of cadi on interobserver variability in interpretation of mammograms by comparing decisions without and with cadi on clustered microcalcifications : by the use of cadi , variability was reduced by 46% , eliminating the disagreement between radiologists in two thirds of cases . also , in the classification of masses , cadi systems showed good results [ 86 ]  . 
on this topic , in 2002 , the first study was published in which the cases for interpretation were unknown both to the radiologist and to the computer : cases were distinct ( independent ) from those used for the training of the classification algorithm [ 87 ]  . 
in addition , it was observed that cadi can potentially reduce the difference in accuracy between community radiologists and mammographers ( improvements were larger for the former )  . in spite of these promising results , the commercialisation of such systems has been delayed , probably due to the difficulty in obtaining fda approval . 
at present , it may be hard to gain clear evidence from large clinical trials that cadi can improve radiologists specificity in identifying benign lesions , without any decrease in sensitivity , for malignant cases . 
this is partly due to the fact that cadi outputs are commonly given by a number , such as the percentage for likelihood of malignancy ( whereas cade marks the location of a suspicious lesion )  . 
oggi nessun sistema ancora stato promosso alla commercializzazione dalla fda ( food and drug administration ) americana [ 20 ]  . solo recentemente si cominciato a testare sistemi cadi , estesamente allenati , su dati nuovi non usati precedentemente . 
questi nuovi casi ( non usati nel training e sviluppo del classificatore e ad esso sconosciuti ) vengono chiamati casi di validazione , e la valutazione di nuovi dati si chiama validazione del classificatore [ 82 ]  . 
 [ 84 ] riportano che , per la classificazione dei cluster di microcalcificazioni , laccuratezza ( espressa come area sotto la curva roc ) migliorata con luso del cadi dallo 0 , 61 allo 0 , 75 . 
unulteriore analisi degli stessi dati [ 85 ] ha valutato gli effetti del cadi sulla variabilit interosservatore nellinterpretazione di mammografie , confrontando le decisioni senza e con cadi riguardo a cluster di microcalcificazioni : con luso del cadi , la variabilit si ridotta del 46% , eliminando il disaccordo tra radiologi in due terzi dei casi . anche nella classificazione delle masse i sistemi cadi hanno mostrato buoni risultati [ 86 ]  . 
a tale riguardo , nel 2002 stato pubblicato il primo studio in cui i casi da interpretare erano sconosciuti sia al radiologo che al computer : i casi erano distinti ( indipendenti ) da quelli usati per allenare lalgoritmo di classificazione [ 87 ]  . 
questo studio ha evidenziato un miglioramento dei risultati dei radiologi con luso del cadi : larea sotto la curva roc aumentata dallo 0 , 93% allo 0 , 96% , la sensibilit dal 94% al 98% . 
non si riscontrata differenza statisticamente significativa nella specificit : il computer non ha mostrato effetti sul numero di casi benigni mandati alla biopsia . in aggiunta , si osservato che il cadi potenzialmente riduce la differenza di accuratezza tra radiologi di comunit e mammografisti ( i primi hanno ottenuto maggiori benefici )  . nonostante questi risultati promettenti , la commercializzazione di tali sistemi ritardata , probabilmente per la difficolt a ottenere lapprovazione dellfda . 
pu essere al momento difficile trarre chiara evidenza , da ampi studi clinici , che il cadi permette di migliorare la specificit dei radiologi nellidentificare lesioni benigne senza ridurre la sensibilit per quelle maligne . 
ci in parte dovuto al fatto che i risultati del cadi sono comunemente espressi da un valore numerico , come la percentuale di probabilit di malignit ( mentre il cade evidenzia la sede di una lesione sospetta )  . 
i radiologi non hanno familiarit con questi valori , dato che finora le loro diagnosi si sono basate su allenamento ed esperienza clinica di percezione visiva di tanti casi , e sulla comprensione di m . 
comunque , possibile e auspicabile che , in futuro , i radiologi prendano familiarit con questo tipo di risultati [ 83 ]  . commercial cad systems at present , four cad systems have obtained fda approval and are commercially available . 
no cadi system has been approved by the fda . r2 technology sistemi cad in commercio attualmente , quattro sistemi cade hanno ottenuto lapprovazione dalla fda e sono disponibili in commercio . 
nessun sistema cadi stato approvato dalla fda . r2 technology r2 technologys image checker was the first commercial cade system approved by the fda , in 1998 [ 88 ]  . 
pilot studies demonstrated 87% and 90.7% sensitivity for masses and microcalcification clusters , respectively . cad and digital mammography cad analysis has most frequently been applied by digitising conventional film - screen mammograms . 
this requires an intermediate step for scanning the film into a laser scanner limage checker della r2 technology stato il primo sistema cade approvato dalla fda , nel 1998 , e commercializzato [ 88 ]  . 
 stato riportato che limage checker m1000 system , version 1.0 , segnala correttamente il 98 , 0% delle microcalcificazioni , il 74 , 7% delle masse e l83 , 4% di tutte le lesioni . intelligent system software la fda nel 2002 ha approvato il sistema cade della issi , il mammoreader , per lindividuazione di cluster di microcalcificazioni , masse , lesioni spiculate , distorsioni architetturali e densit asimmetriche . 
la sensibilit complessiva della prima versione del sistema approvata dalla fda era dell89 , 3% ( del 91 , 0% per i tumori con laspetto di microcalcificazioni , dell87 , 4% nei casi di masse maligne )  . cadx medical systems il secondlook della cadx medical systems ha ricevuto lapprovazione dalla fda nel 2002 [ 90 ]  . 
la prima versione approvata aveva una sensibilit dell85% per tumori trovati allo screening ( combinazione di masse e microcalcificazioni )  . eastman kodak company il kodak mammography cad engine stato approvato dalla fda nel 2004 [ 91 ]  . 
gli studi iniziali hanno mostrato una sensibilit dell87% e del 90 , 7% rispettivamente per masse e microcalcificazioni . cad e mammografia digitale lanalisi cad stata pi frequentemente applicata a mammografie analogiche digitalizzate . 
some authors noted that adaptive modelling with cad combined with digital mammography might yield greater diagnostic performance compared with nonadaptive cad methods for detection of masses [ 31 , 92 , 93 ]  . 
alcuni autori hanno notato che modelli cad adattativi combinati con la mammografia digitale potrebbero condurre a una migliore performance diagnostica , rispetto a metodi cad non adattativi , per lindividuazione di masse [ 31 , 92 , 93 ]  . 
il sistema image checker ha ricevuto dalla fda lapprovazione per combinare la sua tecnologia cad direttamente con il sistema di mammografia digitale fabbricato dalla general electric [ 92 ]  . unsolved problems screening mammography was the first radiologic branch for which the fda , in 1998 , approved a clinical cad system . since then , various studies have been performed to evaluate the use of cad in clinical practice with not completely concording results . 
currently , cade in mammography is accepted as a second reader : the radiologist first searches the mammograms for abnormalities , then the computer marks additional suspicious regions and the final decision is made by the radiologist . 
the ultimate results of studies of cad algorithms rest on problemi aperti la mammografia di screening stata la prima branca radiologica per la quale , nel 1998 , la fda ha approvato un sistema cad clinico . 
correntemente , il cade in mammografia accettato come secondo lettore : prima il radiologo cerca anormalit sulla mammografia , poi il computer indica ulteriori aree sospette e il radiologo prende la decisione finale . 
roc studies are well understood in certain contexts , but they are not immediately applicable to cad research . several other methods are available , but the choice is not easy . 
da incoraggiare unulteriore ricerca sui metodi di valutazione e sul loro uso . possible coming improvements cade and cadi system promise to be helpful in screening mammography , but their actual benefit has still to be assessed . 
probably , in the near future , algorithms for computer detection and classification of suspicious regions on mammograms will be further improved , with a progressive increase in the sensitivity and specificity of these systems . 
another promising technical issue is the development of interfaces for the application of cad technology directly to digital mammography systems , making easier the use of such devices and improving their performance . 
thus , effectiveness of screening mammography in the early diagnosis of breast cancer would improve , with further reduction of mortality . possibili sviluppi futuri i sistemi cade e cadi sono promettenti ausili alla mammografia di screening , ma il loro reale beneficio deve ancora essere definito . 
probabilmente , nel prossimo futuro , gli algoritmi per lindividuazione e la classificazione di regioni sospette sulle mammografie verranno ulteriormente migliorati , con progressivo incremento della loro sensibilit e specificit . 
un altro campo di possibile progresso tecnico lo sviluppo di interfacce per lapplicazione della tecnologia cad direttamente ai mammografi digitali , che ne rendano pi semplice lutilizzo e ne migliorino la performance . 
infine , via via che questi sistemi saranno progressivamente applicati allo screening routinario , i radiologi acquisiranno maggiore confidenza con essi , traendone il massimo beneficio in termini di efficienza . 
blanks rg , wallis mg , moss sm ( 1998 ) a comparison of cancer detection rates achieved by breast cancer screening programmes by number of readers , for one and two view mammography : results from the uk national health service breast screening programme . 
dinnes j , moss s , melia j et al ( 2001 ) effectiveness and cost - effectiveness of double reading of mammograms in breast cancer screening : findings of a systematic review . 
cova1 1struttura complessa di radiologia , 2struttura semplice di chirurgia vascolare , azienda ospedaliero - universitaria ospedali riuniti di trieste , strada di fiume 447 , i - 34149 trieste , italy correspondence to : f . 
pozzi mucelli , tel : + 39 - 040 - 3994372 , fax : + 39 - 040 - 3994500 , e - mail : fabio.pozzimucelli@alice.it received : 10 august 2006 / accepted : 22 november 2006 / published online : 20 april 2007 abstract purpose . 
the proximal endoleaks were treated by cuff deployment , whereas the distal endoleak was treated with a bifurcated graof the two patients with type ii endoleak , one was treated by translumbar puncture and coil embolisation , and the other was treated by superselective embolisation of the lumbar feeding vessel with nonresorbable particles . 
of the three patients with type iii endoleak , two were treated by deploying an aortouniiliac endograft inside the bifurcated graft and the other by implanting a cuff to restore continuity between the graft body and the contralateral limb . 
significant endoleaks should be treated promptly . endovascular treatment can be done with different techniques , but success in not constant due to adverse anatomical conditions and technical difficulties . key words endovascular treatment abdominal aorta aneurysm endoleak riassunto obiettivo . 
dei primi 5 , 4 erano prossimali e 1 distale e sono stati trattati con il posizionamento di cuffie prossimali ; lel distale stato trattato mediante posizionamento di protesi biforcata . 
laltro caso stato trattato mediante embolizzazione dopo cateterismo superselettivo dellafferenza lombare con agente embolizzante . dei tre casi con el di tipo 3 , 2 sono stati trattati mediante posizionamento di protesi aorto - monoiliaca e in un caso stata interposta una cuffia per ripristinare la continuit tra corpo principale e gamba contro - laterale . 
il trattamento endovascolare possibile con diverse modalit , tuttavia il successo tecnico non costante a causa di situazioni anatomiche sfavorevoli e di possibili difficolt tecniche . parole chiave trattamento endovascolare aneurisma aorta addominale endoleak f . 
this complication is usually readily recognised on follow - up imaging studies , especially with computed tomography ( ct ) but also with ultrasound ( us ) and magnetic resonance imaging ( mri ) , and is known as endoleak , a term denoting persistent blood flow within the aneurysm sac outside the endograft . this may occur as a result of different mechanisms : ( 1 ) inadequate seal between the endograft and the aortic wall at the proximal or distal attachment sites ( proximal or distal type i endoleak ) , ( 2 ) retrograde reperfusion of the aneurysm sac by collateral branches ( lumbar arteries or inferior mesenteric artery ) ( type ii endoleak ) , and ( 3 ) incorrect junction of the graft components ( main body and contralateral limb or main body and proximal or distal cuff ) ( type iii endoleak )  . 
other less common types of endoleak include type iv , which occurs due to excessive graft porosity , and type v , also named endotension , in which imaging studies identify sac expansion without a detectable leak [ 1 ]  . the aim of this paper is to describe our experience with endoleaks and illustrate the strategies employed to resolve them and their effectiveness . materials and methods from january 2000 to june 2006 , 134 patients ( 118 men , 16 women ; mean age 75.1 , range 5891 years ) underwent endovascular repair of an abdominal aorta aneurysm by deployment of a bifurcated aortic endograft ( 123 / 134 ) or an aortouniiliac endograft with occlusion of the contralateral iliac artery and a femorofemoral bypass ( 11 / 134 )  . 
all interventional procedures were carried out in an operating room with portable c - arm equipment ( eurocolumbus , milan , italy ) by an interventional radiologist , a vascular surgeon and an anaesthetist after surgical exposure of both femoral arteries . the patients received spinal or general anaesthesia . 
all patients underwent ct follow - up examinations at 1 , 6 , 12 and 24 months and yearly thereafter . il trattamento endovascolare degli aneurismi dellaorta addominale mediante il posizionamento di endoprotesi aortiche diventata un opzione terapeutica sempre pi utilizzata nella pratica clinica per la scarsa invasivit della procedura che la rende eseguibile anche in pazienti con controindicazioni allintervento tradizionale ( et avanzata , patologie concomitanti , addome ostile per pregressi interventi )  . 
tuttavia uno dei talloni dachille di questo intervento dato dalla sua incapacit di escludere completamente la sacca aneurismatica nella totalit dei casi con conseguente possibile aumento della pressione allinterno della sacca e sua possibile rottura . tale complicanza viene riconosciuta agevolmente nella maggior parte dei casi al follow - up mediante diagnostica per immagini , soprattutto con tomografia computerizzata ( tc ) ma anche mediante ecografia e risonanza magnetica e va sotto nome di endoleak ( el ) , termine che non appare traducibile in italiano con ununica parola , ma che sta a significare la persistenza di flusso ematico nella sacca aneurismatica al di fuori dellendoprotesi . 
esistono inoltre ulteriori due tipi di el meno frequenti che sono lel di tipo 4 da eccessiva porosit del tessuto protesico e lel di tipo 5 detto anche endotension : questo un tipo di el particolare in quanto limaging non evidenzia la riperfusione attiva della sacca aneurismatica , ma solo laumento di dimensioni della sacca [ 1 ]  . scopo di questo articolo di descrivere la nostra esperienza con tale tipo di complicanza e di illustrare le soluzioni adottate e la loro efficacia . materiali e metodi dal gennaio 2000 a giugno 2006 , 134 pazienti ( 118 m , 16 f ; et media : 75 , 1 ; range 5891 ) sono stati sottoposti a trattamento endovascolare per lesclusione di un aneurisma dellaorta addominale mediante posizionamento di endoprotesi aortica biforcata ( 123 / 134 ) o aorto - monoiliaca con occlusione dellarteria iliaca contro - laterale mediante occlusore e confenzionamento di by pass femoro - femorale ( 11 / 134 ) utilizzando diversi devices tra quelli disponibili sul mercato ( 91 casi : talent , medtronic , sunnyvale , ca , usa ; 26 casi : excluder , wl gore & associates , flagstaff , az , usa ; 13 casi : aneurx , medtronic , sunnyvale , ca , usa ; 1 caso : life path , edwards lifesciences , irvine , ca , usa ; 1 caso : aorfix , lombard medical , oxon , uk ) ( tabella 1 )  . 
both patients were successfully treated with conventional surgery a few days later . ct follow - up at 1 , 6 , 12 , 24 and 36 months in the 132 cases successfully treated by endograft deployment demonstrated the development of type i , ii and iii endoleaks in 22 patients ( 16% )  . 
twelve cases were primary endoleaks ( that is , present at the first follow - up study ) , whereas ten cases were secondary ( apparent at later follow - up studies )  . 
twelve of these endoleaks were not treated due to small size : four regressed spontaneously , two remained small and are stable and three remained small but are being monitored ; three patients were lost to follow - up ( two patients died from unrelated causes , and one is no longer traceable )  . 
of the ten patients undergoing endovascular treatment , five had type i endoleaks ( four proximal and one distal , the latter in the patient implanted with a straight graft at another centre ) , two had type ii and three had type iii endoleaks ( table 1 )  . with regard to type i endoleaks , exclusion was initially attempted in one case by prolonged dilatation with a valvuloplasty balloon catheter ( up to 30 minutes ) , leading to parproximal cuff proximal cuff proximal cuff bifurcated endograft proximal cuff translumbar embolisation superselective embolisation aortouniiliac graft aortouniiliac graft intermediate cuff outcome successful unsuccessful unsuccessful successful successful unsuccessful successful unsuccessful successful successful cuffia prossimale cuffia prossimale cuffia prossimale endoprotesi biforcata cuffia prossimale embolizzazione translombare embolizzazione superselettiva protesi aortomonoiliaca protesi aortomonoiliaca cuffia intermedia successo insuccesso insuccesso successo successo insuccesso successo insuccesso successo successo procedure sono state effettuate in sala operatoria utilizzando un apparecchiatura portatile con arco a c ( eurocolumbus , milano , italia ) in anestesia spinale o generale dopo esposizione chirurgica di entrambe le arterie femorali comuni da un equipe costituita oltre che dal radiologo interventista dal chirurgo vascolare e dallanestesista . 
tutti i pazienti sono stati sottoposti a ripetuti esami tc di controllo a 1 mese dallintervento , quindi a 6 , 12 , 24 mesi e dopo ogni anno . risultati il posizionamento dellendoprotesi stato possibile in 132 / 134 casi . 
in entrambi i casi a distanza di alcuni giorni stato effettuato lintervento convenzionale con successo . il controllo tc effettuato entro 1 mese dal trattamento endovascolare e quindi a 6 , 12 , 24 , 36 mesi nei 132 casi portati a termine con successo ha evidenziato la comparsa di el di tipo 1 , 2 e 3 in 22 pazienti ( 16% )  . 
in 12 casi si trattava di el primari ( presenti cio al primo controllo ) mentre in 10 casi erano el secondari ( insorti cio nei successivi controlli ) dodici di tali el non sono stati trattati perch di piccole dimensioni : 4 di questi sono spontaneamente regrediti , 2 sono stabili e sempre di dimensioni contenute e 3 sempre di picf . 
a proximal cuff was subsequently implanted , but this technique also failed to achieve complete exclusion of the endoleak , so the patient underwent surgery to remove the graft and fashion an aortobiiliac bypass . 
three other cases of proximal type i endoleak were directly treated by proximal cuff deployment : in one case , a single cuff was sufficient to exclude the endoleak , whereas in another case , the first cuff failed to achieve effective sealing at the proximal end and a further cuff was added in another session , which succeeded in completely excluding the endoleak . 
despite correct positioning , this cuff was unable to completely exclude the endoleak due to aortic tortuosity , so this patient also had a surgical conversion at a later date . the single case of distal type i endoleak arose , as stated , in a patient treated at another centre by deployment of a cole dimensioni sono sotto osservazione ( 3 sono andati persi al follow - up : 2 pazienti deceduti per cause non correlate alla patologia aneurismatica ; 1 paziente non pi reperibile )  . in 11 casi di el di entit pi significativa si proceduto ad un trattamento endovascolare in 10 casi ( combinato in 1 caso ) e chirurgico in 1 caso . 
di questi 10 casi di el trattati per via endovascolare 5 erano el di tipo 1 : 4 a sede prossimale ed 1 a sede distale ( il caso trattato altrove con protesi retta ) , 2 di tipo 2 e 3 di tipo 3 ( tabella 1 )  . per quanto riguarda gli el di tipo 1 in un caso stato tentato preliminarmente di ottenere la sua esclusione mediante f . 
successivamente si proceduto al posizionamento di una cuffia prossimale , ma anche questo trattamento non stato in grado di determinare la risoluzione completa dellel per cui il paziente stato sottoposto ad intervento chirurgico con rimozione della protesi e confezionamento di by pass aortobisiliaco . 
altri 3 casi di el di tipo 1 prossimale sono stati trattati direttamente con posizionamento di una cuffia prossimale : in un caso stato sufficiente il posizionamento di ununica cuffia per ottenere la risoluzione dellel , in un secondo caso la prima cuffia non stata sufficiente a determinare la corretta sigillatura prossimale della protesi per cui in una seconda seduta stata aggiunta una seconda cuffia con risoluzione completa dellel . 
nel terzo caso , in paziente monorene , a distanza di 6 mesi dal posizionamento della protesi vi fu la comparsa di un el di tipo 1 per parziale scivolamento caudale della protesi . 
a , b computed tomography ( ct ) : a large endoleak ( * ) is visible laterally to the distal portion of the straight endograft . b the maximum intensity projection ( mip ) image depicts well the graft angulation . 
in the first case , follow - up ct demonstrated sac reperfusion both anteriorly and posteriorly to the graangiography demonstrated that the anterior reperfusion was supplied by the inferior mesenteric artery . 
because this endoleak had significantly increased after 1 year , we attempted embolisation via direct translumbar puncture and occlusion by means of gianturco coils and an embolising agent ( spongostan )  . 
despite the partial failure , the patient was not converted to surgery because of poor general condition ; however , follow - up ct at approximately 1 year demonstrated no further expansion of the aneurysm sac . 
the third case of type iii endoleak occurred in a patient who had been implanted with a new concept endograft ( lifepath , edwards ) compared with those normally used . 
in this case , use of a double femoral - brachial approach and a snare device enabled us to restore continuity between the main body and via translombare e occlusione dello stesso mediante posizionamento di spirali di gianturco e agente embolizzante ( spongostan )  . 
nonostante tale trattamento a distanza di 24 ore si ebbe la rottura della sacca aneurismatica e il paziente venne sottoposto a intervento chirurgico in urgenza con rimozione dellendoprotesi e confezionamento di by pass aorto bisiliaco . 
in entrambi i casi si proceduto al posizionamento di una protesi aortomonoiliaca ( talent ) allinterno della protesi biforcata , quindi a posizionamento di occlusore a livello dellarteria iliaca comune controlaterale e confezionamento di bypass femoro - femorale . 
il paziente , nonostante il parziale insuccesso , non stato sottoposto ad ulteriore conversione chirurgica a causa delle condizioni generali scadenti , tuttavia ad un controllo tc a distanza di un anno circa , non si osservato pi alcun incremento della sacca aneurismatica . 
nel terzo caso di el di tipo 3 questo si verificato in un paziente in cui era stata utilizzata una protesi di concezione diversa ( lifepath edwards ) rispetto a quelle comunemente utilizzate . 
a a small endoleak is located anteriorly to the gra b angiography shows that the endoleak is due to anastomosis between the right gluteal superior artery and the lumbar artery . 
d tc di controllo dopo 12 mesi dallintervento : scomparsa dellendoleak . mento dei diametri della sacca aneurismatica , latteggiamento corretto di vigile attesa in quanto ai controlli successivi si pu ottenere una sua spontanea regressione [ 4 ]  . 
come si pu vedere dallesperienza qui riportata , il trattamento risolutivo pu essere diverso da caso a caso e va scelto in base a diversi criteri , quali le condizioni generali del paziente , la conformazione della protesi e le curvature dellaorta . 
a computed tomography ( ct ) , maximum intensity projection ( mip ) image : evidence of an anterior endoleak ( arrow ) between the proximal cuff and the main graft body . 
c angiografia intra - operatoria : il controllo dopo rilascio dellendoprotesi monoiliaca dimostra la persistenza di una dilatazione dellaorta nel tratto prossimale dovuto allincompleta sigillatura dellendoleak . tipo 1 lopzione teoricamente pi efficace laggiunta di una cuffia prossimale o distale per ottenere una adeguata sigillatura tra protesi e parete aortica . 
questo tipo di trattamento nella nostra esperienza tuttavia non sempre si rivelato efficace e ben in 3 / 4 casi in cui stato utilizzato la prima cuffia non stata sufficiente ad ottenere il successo tecnico e si dovuto in una seconda seduta aggiungere unulteriore cuffia per ottenere lesclusione dellel . 
nel caso di oversizing della cuffia si pu avere infatti che il tessuto protesico non sia correttamente disteso , ma presenti delle piccole ripiegature che consentirebbero il passaggio del sangue attraverso esse e quindi continuerebbero il rifornimento dellel . 
in medium endoleaks with enlarging aneurysm sac , treatment should be considered [ 5 ]  . as can be seen from our experience , treatment will differ from case to case and should be chosen on the basis of sevf . 
c tc di controllo dopo posizionamento di estensione protesica tra corpo principale e gamba controlaterale migrata caudalmente : risoluzione del quadro . eral criteria , including the patients general condition , graft configuration and aorta tortuosity . 
the most effective treatment for type i endoleak is ideally the insertion of an additional proximal or distal cuff to achieve an adequate seal between the graft and the aorta wall . 
in our experience , however , this form of treatment did not always prove effective , and as many as 3 / 4 cases required reintervention to implant an additional cuff and achieve endoleak exclusion . 
this option , however , is not always technically feasible due to the complexity of the catheterisation procedure , and it is not always effective in the long term [ 6 ]  . in our experience , the procedure was attempted twice , in one case with success whereas in the other case it was abandoned due to technical difficulty in achieving superselective catheterisation of the intermesenteric arcade . 
another possible technique involves a direct translumbar approach to the aneurysm sac , usually under ct guidance , and filling of the sac with coils or glue or thrombin [ 7 ]  . 
other authors [ 9 ] have reported very promising results with preventive embolisation of the aneurysm sac with fibrin glue provided that care is taken to prevent distal migration of the embolising agent . 
in our study , we also considered disconnection between the proximal cuff and the main graft body as type iii endoleaks ; however , such a situation has not been codified and may well be regarded as a type i endoleak . 
there are two main treatment options for type iii endoleaks : if the main graft body has become disconnected from a graft limb , attempts should be made to restore continuity of the graft components by adding an adequately sized cuff ; if the disconnection is between the proximal cuff and the main graft body the , options are either to fill the vascular component of the sac with metal coils or to implant an aortouniiliac graft inside the previous endograft , exclude the contralateral branch with an occluder and subsequently fashion a femorofemoral bypass [ 10 ]  . in our series , endoleaks occurred more frequently with talent endografts than with other devices ( aneurx , excluder )  . 
however , we believe this to be due to the fact that talent endografts tend to be used in more complex cases ( aneurysms with short or angulated necks , large size and wall calcifications ) rather than to a limitation of the talent endograft itself . 
our experience also shows that endoleaks occurred when we implanted different endografts from those commonly used , and this could be the consequence of inadequate experience with such devices . four out of 134 patients ( 2.9% ) treated with endograft implantation underwent surgical conversion . 
to these we should add the two patients in whom endovascular treatment failed and the one who underwent immediate surgical conversion owing to coverage of both renal arteries by a proximal cuff that had migrated cranially . 
this figure is , however , low if compared with other authors , who report a surgical convervece si soprasseduto a causa delle difficolt tecniche a ottenere il cateterismo superselettivo dellarcata di riolano . 
in alternativa a questa tecnica si pu utilizzare lapproccio diretto alla sacca aneurismatica per via translombare , in genere mediante guida tc e riempimento della sacca con spirali o colla o trombina [ 7 ]  . 
in alternativa alla puntura diretta per via translombare recentemente stato proposto lapproccio per via transcavale con risultati incoraggianti [ 8 ]  . altri autori [ 9 ] hanno proposto lembolizzazione preventiva della sacca aneurismatica con colla di fibrina ponendo attenzione a evitare la migrazione distale dellagente embolizzante con risultati estremamente promettenti . gli el di tipo 3 si hanno quando vi una disgiunzione tra corpo principale protesico ed estensione protesica o quando c un difetto protesico [ 1 ] ; nella nostra esperienza abbiamo considerato el di tipo 3 anche levenienza di disgiunzione tra cuffia prossimale e corpo principale protesico non essendo in realt codificata questa situazione ma potendosi in realt inquadrare anche come el di tipo 1 . 
nellel di tipo 3 le opzioni sono fondamentalmente 2 : nel caso di disgiunzione tra corpo principale ed estensione protesica bisogna cercare di ricostituire la continuit tra le componenti protesiche mediante laggiunta di una cuffia di calibro adeguato mentre nel caso di el tra cuffia prossimale e corpo principale le opzioni sono o il riempimento con spirali metalliche della componente vascolarizzata della sacca o il posizionamento di unendoprotesi aortomonoiliaca allinterno della precedente con esclusione della branca controlaterale mediante dispositivo occlusore e successivo bypass femorofemorale [ 10 ]  . in questa casistica gli el si sono manifestati pi frequentemente con la protesi talent rispetto ad altri tipi di protesi utilizzate ( aneurx , excluder ) , tuttavia riteniamo che questo non sia conseguente a un limite della protesi talent quanto al fatto che tale tipo di protesi viene utilizzata in casi pi complessi rispetto alle altre protesi : colletti corti , angolati , di calibro elevato e con calcificazioni parietali . 
dalla nostra esperienza emerge inoltre che abbiamo avuto el quando sono state utilizzate protesi diverse da quelle abituali e questo pu essere conseguenza di una inadeguata esperienza degli operatori con tali materiali . complessivamente nella nostra esperienza 4 pazienti su 134 trattati mediante posizionamento di endoprotesi sono andati incontro a conversione chirurgica pari pertanto al 2 , 9% . 
a questi 4 casi vanno aggiunti i 2 casi nei quali il trattamento endovascolare non era tecnicamente riuscito e un caso che andato incontro a conversione chirurgica immediata per la copertura di entrambe le arterie renali da parte di una cuffia prossimale migrata cranialmente per cui abbiamo avuto complessivamente 7 conversioni chirurgiche ( una acuta e 6 tardive ) su 134 casi ( 4 , 4% )  . 
 conclusions in conclusion , our experience shows that endovascular treatment of abdominal aorta aneurysms is feasible in a large proportion of patients , but success is not guaranteed in all cases ; in addition , the treatment of endoleaks , the most common complication of endovascular repair , although possible with a variety of endovascular techniques , does not always allow definitive resolution of the problevery careful selection of candidates and the use of endografts with proven longterm effectiveness on large patient series are required . portato dalleurostar data registry centre , che riporta un incidenza globale di reinterventi pari all8 , 7% [ 12 ]  . conclusioni in conclusione , riteniamo che dalla nostra esperienza emerga che il trattamento endovascolare di esclusione degli aneurismi dellaorta addominale sia una tecnica eseguibile in una ampia casistica di pazienti portatori di aneurismi tuttavia il successo non garantito nella totalit dei casi ed anche il trattamento della complicanza pi frequente , vale a dire lel , sebbene trattabile per via endovascolare e con diverse modalit , non sempre garantisce la risoluzione definitiva del problema . 
forty - two mri exams were performed with intravascular contrast media in 21 rats : tumours were induced by subcutaneous injection of colon carcinoma cells in 7 rats and mammary adenocarcinoma cells in 14 rats . 
perfusion and permeability parameters of the implanted tumours were evaluated by using two contrast media ( b22956 / 1 and gd - dtpa37albumin ) to establish response to treatment with two different antiangiogenic drugs ( tamoxifen and su6668 )  . 
in the mammary carcinoma experiment , vascular permeability measured by means of b22956 / 1 in the animals treated with the antiangiogenic drug ( 0.00433170.0040418 ml / min - 1 / ml - 1 ) was significantly less than in untreated animals ( 0.00904600.0043680 ml / min - 1 / ml - 1 ) , whereas no significant difference was observed with gd - dtpaalbumin ( 13.1413.94 ml / min - 1 / ml - 1 in treated animals and 18.0711.92 ml / min - 1 / ml - 1 in untreated animals )  . 
sono stati eseguiti 42 esami rm in 21 ratti di laboratorio a cui in 7 erano state preventivamente impiantate cellule di carcinoma del colon e in 14 cellule di adenocarcinoma mammario . 
sono stati valutati i parametri perfusionali e di permeabilit sul tumore impiantato mediante due mezzi di contrasto ( b22956 / 1 e albuminagd - dtpa37 ) al fine di stabilire la risposta al trattamento con due diversi farmaci antiangiogenici ( tamoxifen e su6668 )  . 
per lesperimento con cellule di adenocarcinoma mammario la permeabilit vascolare media misurata mediante il b22956 / 1 negli animali trattati con farmaco antiangiogenico ( 0 , 00433170 , 0040418 ml min - 1 ml - 1 ) significativamente minore che nei controlli ( 0 , 00904600 , 0043680 ml min - 1 ml - 1 ) , mentre nessuna differenza statisticamente significativa apprezzabile con gddtpaalbumina ( 13 , 1413 , 94 ml min - 1 ml - 1 nei trattati e 18 , 0711 , 92 ml min - 1 ml - 1 nei controlli )  . 
one of the major technical problems in the study of angiogenesis is the lack of methods ensuring significant , quantitative and repeatable measurements of the angiogenic process given the large number of techniques providing numerous but not necessarily comparable data . 
radiological research has also investigated the properties of the microcirculation , the anatomical - function unit of the vascular system , to increase knowledge of tumour characteristics and vascularity . animal models of human disease are fundamental for understanding the pathogenic mechanisms of diseases , especially during the different phases of pharmacological experiments . magnetic resonance imaging ( mri ) , with its multiple parameters and high spatial resolution that can reach 50100 m with specific scanners , has an recognised role in characterising animal models in vivo in preclinical studies [ 18 ] , thanks to its ability to provide metabolic , physiological and functional information . 
examples include evaluation of the functional response of the brain to stimuli or drugs [ 1 ] , assessment of organ viability after transplantation [ 2 ] , evaluation of cerebral blood volume and flow [ 3 ] , and characterisation of tumour neoangiogenesis present in tumours lager than 1 mm3 [ 46 , 9 , 10 ]  . 
imaging techniques of angiogenesis have potentially extended the clinical applications of mri , and their development has been triggered by advances in anticancer treatments , many of which aim to inhibit tumour microcirculation . 
intravascular contrast media can be used to measure both endothelial permeability and intravascular blood volume , both of which are related to angiogenesis : the first can be quantified as of the earliest stages of tumour development and the second only once the microcirculation has formed . 
 the aim of our work was to evaluate the applications of mri and in particular of dynamic contrast - enhanced mri ( dce - mri ) to the study of tumour microcirculation by using animal models assessed before and after treatment with antiangiogenic drugs . materials and methods we assessed the results of the use of dce - mri in two experiments conducted to test the effectiveness of two antiangiogenic drugs : tamoxifen , an oestrogen receptor ligand commonly used in hormone - dependent breast cancer treatment [ 11 ] , and su6668 , an inhibitor for vascular endothelial growth factor ( vegf ) receptors [ 12 ]  . 
in the first experiment , mammary adenocarcinoma cells ( american type culture collection ) were implanted subcutaneously in the flank of 14 la patologia neoplastica un importante campo di ricerca nellambito delle alterazioni microvascolari , al fine di studiare le correlazioni tra neoangiogenesi tumorale e grado di aggressivit dei tumori . 
uno dei pi rilevanti problemi tecnici nello studio dellangiogenesi la mancanza di metodiche che garantiscano misure significative , quantitative e ripetibili del processo angiogenico , a causa del gran numero di tecniche che forniscono una moltitudine di dati , non necessariamente comparabili . 
anche in campo radiologico si studiano le propriet del microcircolo , unit anatomo - funzionale del sistema vascolare , per migliorare la conoscenza delle caratteristiche e del grado di vascolarizzazione dei tumori . 
la risonanza magnetica ( rm ) , grazie alla molteplicit dei parametri e allalta risoluzione spaziale che pu raggiungere 50100 micron mediante scanner specifici , ha un ben riconosciuto potere nella caratterizzazione dei modelli animali in vivo negli studi pre - clinici [ 18 ] , in quanto consente di offrire informazioni metaboliche , fisiologiche e funzionali . 
esempi sono la valutazione della risposta funzionale del cervello , indotta da stimoli o farmaci [ 1 ] , la valutazione della vitalit degli organi dopo trapianto [ 2 ] , la valutazione del volume e del flusso ematico cerebrale [ 3 ] , e la caratterizzazione della neoangiogenesi tumorale , presente per volumi tumorali maggiori di 1 mm3 [ 46 , 9 , 10 ]  . 
le tecniche di imaging dellangiogenesi hanno potenzialmente esteso le applicazioni cliniche della rm ed il loro sviluppo stato spinto dai progressi nelle terapie antitumorali , molte delle quali hanno come bersaglio linibizione del microcircolo . 
mediante i mdc intravascolari si possono misurare sia la permeabilit dellendotelio che il volume ematico intravasale ; questi parametri sono entrambi correlati con langiogenesi : il primo quantificabile gi allinizio della crescita tumorale , il secondo solo quando il microcircolo formato . lo scopo del nostro lavoro di valutare le applicazioni della rm ed in particolare della risonanza magnetica dinamica con mezzo di contrasto ( dynamic contrast enhancement magnetic resonance imaging : dce - mri ) nello studio del microcircolo tumorale attraverso limpiego di modelli animali , valutati pree post - trattamento con farmaci antiangiogenici . materiali e metodi sono stati valutati i risultati della applicazione della tecnica dce - mri in due esperimenti compiuti per testare la validit di due farmaci antiangiogenici : il tamoxifen , un ligando del n . 
the animals were divided into two groups ( treated and controls ) : treated rats ( n = 7 ) received 6 mg / kg of tamoxifen daily , whereas control rats ( n = 7 ) received the propylene glycol vehicle . ten days after implantation , all animals were imaged by mri with b22956 / 1 and 24 h later with gd - dtpa37albumin . in the second experiment , human colon carcinoma cells , ht - 29 , were implanted subcutaneously in the flanks of ten nu / nu rats ( harlan , san pietro , italy ) weighing approximately 25 g . 
the first group ( n = 5 ) received a single dose of su6668 ( sugen inc . , san francisco , ca , usa ) , whereas the second group ( n = 5 ) received the vehicle only . 
 b22956 / 1 ( bracco , milan , italy ) , an experimental proteinbinding gadolinium chelate with a half - life of approximately 2030 min , was injected into the rats tail vein at a dose of 50 mol / kg . 
gd - dtpa37albumin , a macromolecular , t1relaxing , blood - pool contrast agent with a half - life of 3 h , was injected at a dose of 30 mol / kg in both experiments . images were acquired with a biospec scanner ( bruker , karlsruhe , germany ) equipped with a 4.7 - t , 33 - cm bore , horizontal magnet ( oxford ltd . , oxford , uk )  . 
the rats were anaesthetised with halothane and placed prone in a birdcage coil with a 7 - cm diameter ( the diameter was 3.5 cm for the animal experiments )  . 
coronal and transverse t2 - weighted fast spin echo ( fse ) sequences rapid acquisition with relaxation enhancement ( rare ) , te = 70 ms ] were used to locate the tumour and extratumoural tissue . 
 [ 13 ] in which the time dependence of the signal is converted into time dependence of the concentration of contrast medium and analysed by using pharmacokinetic models : the analysis is repeated pixel by pixel to obtain parametric maps [ 6 , 1315 ]  . 
in summary , measurement of the intensity signal in the tissue being examined ( tumoral and healthy ) can provide parameters for permeability ( kps : expresses the ability of macromolecules to extravasate into the interstitial space ) and perfusion ( fpv : expresses the fraction of plasma in millilitres per cubic centimetre of tissue , a measure of the vascular density )  . 
after the mri study , the animals were killed and the tumours excised ; 7 - m sections in planes corresponding to the mri study were then obtained that were stained with the vessel marker cd31 to obtain a mean vessel count . 
 recettore degli estrogeni , comunemente usato nella terapia ormono - dipendente del carcinoma mammario [ 11 ] , ed il su6668 , un inibitore recettoriale del fattore di crescita vasculo - endoteliale ( vascular endothelial growth factor : vegf ) [ 12 ]  . 
nel primo esperimento , cellule di adenocarcinoma mammario ( american type culture collection ) sono state impiantate sottocute nel fianco di 14 ratti ( charles river laboratories , italia ; peso tra i 76 g ed i 150 g )  . 
gli animali sono stati suddivisi in due gruppi ( trattati e controllo ) : ai ratti trattati ( n = 7 ) stata giornalmente somministrata una dose di tamoxifen di 6 mg / kg , mentre ai ratti del gruppo di controllo ( n = 7 ) stato somministrato solo il veicolo propilene - glicole . 
tutti gli animali sono stati esaminati mediante rm 10 giorni dopo limpianto usando come mezzo di contrasto ( mdc ) il b22956 / 1 e 24 ore dopo il gd - dtpa37albumina . nel secondo esperimento , cellule di colon carcinoma ht29 umano sono state impiantate sottocute nel fianco di 10 topi nu / nu ( harlan , san pietro , italia ) , di circa 25 g . 
i primi ( n = 5 ) hanno ricevuto una singola dose di su6668 ( sugen inc , san francisco , ca , usa ) ; i secondi hanno ricevuto solo il veicolo ( n = 5 )  . tutti gli animali sono stati monitorati tramite rm prima e 24 h dopo trattamento , mediante gd - dtpa37albumina . il b22956 / 1 ( bracco , milano , italia ) un chelato del gadolinio ancora in fase sperimentale , ligando per le proteine , a emivita plasmatica di circa 2030 minuti , ed stato somministrato nella vena della coda dei ratti in dose di 50 mol / kg . 
il gd - dtpa37albumina un mdc macromolecolare t1 rilassante intravascolare ( blood pool ) con emivita di circa 3 ore , iniettato in dose di 30 mol / kg in entrambi gli esperimenti . le immagini sono state acquisite mediante uno scanner biospec ( bruker , karlsruhe , germania ) equipaggiato con un magnete orizzontale operante a 4 , 7 t con unapertura da 33 cm ( oxford ltd , oxford , gran bretagna )  . 
gli animali sono stati anestetizzati mediante alotano e posti in posizione prona in una bobina di tipo bird - cage di 7 cm di diametro ( 3 , 5 cm di diametro per gli esperimenti fatti sul topo )  . 
sono state acquisite sequenze coronali e trasversali fast spin echo t2 - weighted ( rare , teeff = 70 ms ) per la localizzazione del tumore e dei tessuti extratumorali . 
successivamente stata acquisita una serie dinamica di immagini 3d spoiled - gradient echo ( spgr ) con i seguenti parametri : tr / te = 50 / 3 , 5 ms , flip angle = 90 , matrice 25612816 , fov 842 , 4 cm3 ( corrispondente a 0 , 310 , 31 mm2 e 1 , 5 mm di spessore di fetta ) , nex = 1 ; tempo di acquisizione per immagine 3d = 104 s ; dopo somministrazione di mdc sono state acquisite scansioni dinamiche di 22 immagini con 30 s di intervallo per un totale di circa 50 minuti a esame . 
 [ 13 ] , in cui la dipendenza temporale del segnale viene trasformata nella dipendenza temporale della concentrazione del mdc e analizzata mediante modelli farmacocinetici : lanalisi viene ripetuta pixel per pixel , ricavandone delle mappe parametriche [ 6 , 1315 ]  . 
in particular , this was evident at early time points after the injection , whereas the difference tended to decrease at later time points because of the persistence in the inner area of extravasated contrast material that is not drained . 
analysis of the r1tumour / r1blood ratio ( ratio between the variation in longitudinal relaxation rate in the tumour and blood ) in a region of interest ( roi ) selected on the rim of the tumour in the group treated with tamoxifen and in the control group enabled us to visually monitor the effect of therapy [ 11 ]  . 
without going into detail on the experimental theory , we were able to demonstrate that for a blood - pool contrast medium , r1tumour / r1blood is expressed by a linear relationship as a function of time ; the intercept of this line represents plasma volume ( fpv ) , and the slope represents permeability ( kps ) [ 15 ]  . 
dopo lesame rm gli animali sono stati sacrificati , il tumore resecato , e ne sono state ottenute sezioni da 7 m secondo piani corrispondenti alle immagini rm , marcate poi con cd31 , marcatore vasale , per ottenere la conta media dei vasi . 
lanalisi vasale delle sezioni stata ottenuta tramite software image proplus 4.0. risultati nel primo esperimento , in cui abbiamo studiato leffetto del tamoxifen sul modello di tumore mammario , abbiamo ottenuto una mappa dellenhancement della regione tumorale in una scala di falsi colori , sovrapposta allimmagine anatomica in scala di grigio . 
in particolare ci evidente a tempi brevi dopo liniezione , mentre la differenziazione tende a diminuire tardivamente a causa della permanenza nella zona interna del mezzo extravasato che non viene drenato . 
2a - f enhancement on an experimental model of colon carcinoma implanted in rats with the administration of gd - dtpa37albumin : early ( 3.3 min ) ( a ) and late ( 46.4 min ) ( b ) enhancement before treatment and posttreatment ( 24 h ) , with the same timing , after su6668 injection ( d , e )  . 
2a - f intensit di segnale ottenuto in un modello sperimentale di colon carcinoma umano impiantato su topi nudi mediante gd - dtpa37albumina : prima della somministrazione di una dose di su6668 in condizioni di enhancement precoce ( a ) e tardivo ( b ) rispettivamente 3 , 3 min e 46 , 4 min dopo liniezione di mdc , e post - trattamento 24 ore dopo la somministrazione del farmaco ( d , e ) con la stessa tempistica . 
we therefore observed that , in this specific histological tumour type , mammary adenocarcinoma , only the dce - mri technique that employs b22956 / 1 was able to quantify changes in vascular permeability , whereas the study performed with gd - dtpaalbumin was unable to reveal any effect . 
even in this tumour model , the increase in signal intensity occurred predominantly in the tumour periphery ; comparison of imaging and histological data ( not shown ) clearly shows that the enhancing outer portion corresponds to an area of highly vascular viable tissue , whereas the inner portion corresponds to predominantly necrotic tissue . 
comparison of the images of the same tumour obtained before and 24 h after administration of a single dose of su6668 revealed a substantial decrease in enhancement both in the viable area and , to a lesser extent , in the inner portion . 
senza entrare nel dettaglio della teoria sperimentale stato possibile dimostrare che , per un mdc blood pool il r1tumore / r1sangue espresso da una relazione lineare in funzione del tempo ; lintercetta di questa linea rappresenta il volume plasmatico ( fpv ) , e la pendenza rappresenta la permeabilit ( kps ) [ 15 ]  . 
quantitativamente infatti la permeabilit vascolare media misurata mediante il b22956 / 1 negli animali trattati ( 0 , 00433170 , 0040418 ml min - 1 ml - 1 ) significativamente minore che nei controlli ( 0 , 00904600 , 0043680 ml min - 1 ml - 1 ) , mentre nessuna differenza statisticamente significativa apprezzabile con gddtpaalbumina ( 13 , 1413 , 94 ml min - 1 ml - 1 nei trattati e 18 , 0711 , 92 ml min - 1 ml - 1 nei controlli )  . 
abbiamo quindi osservato che , in questo particolare istotipo tumorale , ladenocarcinoma mammario , solo la tecnica di dce - mri mediante b22956 / 1 in grado di quantificare le modificazioni di pern . 
3 r1tumore in una roi periferica di colon carcinoma , come quello mostrato in figura 2 in condizioni pre - trattamento ( ) e 24 ore dopo la somministrazione di su6668 ( ( cid : 2 ) )  . 
si noti leffetto del farmaco sulla pendenza della curva ( permeabilit vascolare ) e sullintercetta ( volume ematico )  . lanalisi quantitativa compiuta sullintero gruppo sperimentale ha mostrato una riduzione rispettivamente del 51% e del 59% su questi due parametri . single dose of su6668 , which allows visual monitoring of the effect of treatment . 
the histological sections shown in figure 2c , f belong to a treated animal and a control , respectively , and show that the number of vessels in the treated animal is far smaller than in the control . 
in particular , tumour microcirculation is characterised by some structural vessel abnormalities , such as sudden changes in calibre , endothelial fenestrations and interruptions in the basal membrane , which are reflected in functional alterations such as increased transcapillary permeability , irregular flow and arteriovenous shunting [ 5 , 7 ]  . 
tumour size has long been used as a parameabilit vascolare , mentre lesame eseguito con gddtpaalbumina non in grado di evidenziare alcun effetto . nel secondo modello sperimentale , in cui sono state utilizzate cellule di colon carcinoma umano , lenhancement ottenuto presentato in figura 2 . 
anche in questo modello tumorale laumento dellintensit di segnale avviene principalmente nella zona periferica del tumore ; attraverso il confronto tra le immagini e i dati istologici ( non mostrati ) , appare chiaro che la parte esterna che subisce enhancement corrisponde ad una zona di tessuto vitale altamente vascolarizzato , mentre la parte pi interna corrisponde a tessuto principalmente necrotico . 
dopo somministrazione della molecola su6668 , confrontando le immagini dello stesso tumore prima e 24 h dopo la somministrazione di una singola dose di farmaco , abbiamo riscontrato una sostanziale diminuzione dellenhancement sia nella zona vitale che , in misura minore , nella zona interna . i grafici mostrati in figura 3 riportano landamento di r1tumore ( che equivalente a r1tumore / r1sangue essendo r1sangue approssimativamente costante per gd - dtpaalbumina ) in una roi selezionata sul bordo del tumore rispettivamente prima e 24 ore dopo la somministrazione di una singola dose di su6668 , permettendo di monitorare visivamente leffetto della terapia . 
come si vede dalla figura , la somministrazione di su6668 ha un effetto sia sulla permeabilit ( pendenza ) che sul volume ematico ( intercetta ) : i valori medi di perfusione e permeabilit per tutti gli animali studiati nel modello sperimentale di colon carcinoma , misurati nella parte periferica del tumore , dopo somministrazione di farmaco antiangiogenico sono diminuiti del 51% ( da 5 , 21 , 1 a 2 , 50 , 8 ml / 100 ml di tessuto ) e del 59% ( da 0 , 001655 , 1 a 0 , 00674 , 8 ml min - 1 ml - 1 di tessuto ) rispettivamente . 
in particolare , il microcircolo tumorale caratterizzato da alcune anomalie strutturali dei vasi , quali variazioni improvvise di calibro , fenestrature dellendotelio ed interruzioni della membrana basale , che si riflettono in alterazioni funzionali come aumento della permeabilit transcapillare , irregolarit di flusso e formazione di shunt artero - venosi [ 5 , 7 ]  . 
le dimensioni tumorali sono state per lungo tempo utilizzate come parametro di valutazione della risposta farmacologica : esistono tuttavia dei limiti a questo criterio nella valutazione della risposta a farmaci antiangiogenici , i quali inibiscono la vascolarizzazione prima che ne conseguano effetti sulle dimensioni tumorali [ 7 , 8 ]  . 
4 rappresentazione anatomica del microcircolo . arteriola / arteriole shunt av / arterovenous shunt venula / venule capillari / capillaries metarteriola / metarteriole venula / venule blood flow meter for evaluating response to treatment : this criterion is , however , limited for the evaluation of response to antiangiogenic drugs , which inhibit vascularity before affecting tumour size [ 7 , 8 ]  . 
numerous studies point to perfusion as the most important quantifiable parameter correlated to tumour growth , as intratumoural microvessel density , which is directly proportional to perfusion , is related to indices of tumour aggressiveness , such as high presenting stage and / or shorter patient survival [ 13 , 14 ]  . dce - mri is based on postprocessing methods that employ specific algorithms for deriving physiodynamic parameters that are useful in assessing tumour microvascularity in vivo and monitoring antiangiogenic therapy . 
mris of an organ or mass are acquired before and at various time intervals after the administration of contrast material : this makes it possible to describe the signal - intensity changes due to perfusion by means of a time - intensity curve . 
dce - mri techniques have been used in experimental studies to monitor the microvascular characteristics of tumours in vivo and to analyse the therapeutic effect of drugs [ 5 , 7 , 8 , 15 ]  . 
preclinical studies have shown that dce - mri , though not yet commonly used as a diagnostic technique , is the most accurate method for identifying microcirculation characteristics , in particular when associated with intravascular contrast material [ 510 , 1418 ]  . 
because less than 5% of blood - pool agents leaks out of tumour vessels in a single pass , these agents can be used to measure both endothelial permeability and intravascular considerazioni anatomo - fisiologiche . 
in base alle esperienze di molti autori il parametro quantificabile pi importante correlato allo sviluppo tumorale la perfusione ; infatti la densit microvasale intratumorale , direttamente proporzionale alla perfusione , correlata ad indici di aggressivit come lelevata stadiazione alla presentazione e / o la diminuita sopravvivenza del paziente [ 13 , 14 ]  . 
la dce - mri una tecnica basata su metodi di post - processing che si avvalgono di specifici algoritmi per ricavare parametri fisiodinamici , utili nella valutazione in vivo della microvascolarizzazione tumorale ed in particolare nel monitorare la terapia antiangiogenica . 
le immagini rm di un organo o di una massa sono acquisite prima e a vari intervalli di tempo dopo la somministrazione di mdc : in questo modo possibile descrivere il mutamento nellintensit di segnale dovuto alla perfusione attraverso una curva tempo - intensit . 
le tecniche di dcemri sono state utilizzate , in studi sperimentali , per monitorare in vivo le caratteristiche microvascolari dei tumori , e nella caratterizzazione delleffetto terapeutico di farmaci [ 5 , 7 , 8 , 15 ]  . 
studi pre - clinici hanno dimostrato che la dce - mri , anche se non ancora di comune attivit diagnostica , la metodica pi accurata nella identificazione delle caratteristiche del microcircolo , in particolare mediante mdc intravascolare [ 510 , 1418 ]  . 
i mdc intravascolari in un singolo passaggio fuoriescono dai vasi tumorali in misura < 5% , perci con essi si possono misurare sia la permeabilit dellendotelio che il volume ematico intravasale , sfruttando la maggiore permanenza allinterno dei vasi e la lenta diffusione nellinterstizio rispetto ai mdc convenzionali . 
the parameters that can be obtained with this technique , permeability and intravascular blood volume , are both correlated with angiogenesis : the first can be quantified as of the earliest stages of tumour development , the second only when the microcirculation has formed . 
in all our experiments , we were able to distinguish at least two areas : a peripheral area that is viable and highly vascular , and an internal area that is less vascular and predominantly necrotic . 
the parametric distributions in fact have bimodal characteristics , reflecting segmentation of the tumour into a core and a peripheral area , for which a high capillary density correlates with histological malignancy grade . 
other authors have calculated the two neoangiogenesis parameters ( fpv and kps ) on human tumour models implanted in rats , with the aim of obtaining quantitative anatomical maps and correlating them with immunocytochemical and ultrastructural data [ 6 , 14 , 15 ]  . 
a further remark regards the importance of the distribution analysis of the parameters kps and fpv for evaluating the presence of necrosis is necessary : conventional imaging modalities are limited in quantifying necrosis in the tumour mass , whereas the quantitative approach used in recent studies can be exploited to establish the effects of physical - chemical treatments on the tumour [ 6 , 15 , 17 ]  . 
microcirculation heterogeneity was demonstrated by means of tumour segmentation in our experiments as well , which identified distinct areas of different angiogenesis on the basis of dynamic parameters correlated to the microvascular structure and function . 
it has been demonstrated that with macromolecular contrast agents this ratio follows a linear trend over time ; the intercept and the slope are proportional to the blood volume and vascular permeability , respectively , of the region being studied [ 11 , 19 , 20 ]  . in our experience dce - mri also proved very effective for monitoring the therapeutic effect after antiangiogenic treatment . 
in particular , in the experimental animal model of colon carcinoma cells , results could be seen as early as 24 h after administration , when no change in tumour volume had yet occurred . 
it has been observed that newly formed tumour microcirculation is impermeable to macromolecules , and reduction in permeability is an excellent surrogate marker of the biological action of drugs [ 21 ]  . 
finally , in the experiment with tamoxifen , we verified that the contrast agent b22956 / 1 , thanks to its binding with plasma proteins and therefore intermediate behaviour between a low - molecularweight agent and a pure macromolecular one , seems to have the right size and extravasation capability to be suitable for testing the effects of tamoxifen on the microcirculation . tenibili con questa tecnica , permeabilit e volume ematico intravasale , sono entrambi correlati con langiogenesi : il primo quantificabile gi allinizio della crescita tumorale , il secondo solo quando il microcircolo formato . il nostro lavoro dimostra come le tecniche dce - mri permettano di individuare allinterno della massa tumorale aree a diversa perfusione : in tutti gli esperimenti abbiamo potuto distinguere almeno due aree , una periferica , vitale e altamente vascolarizzata , ed una interna meno vascolarizzata e principalmente necrotica . 
le distribuzioni parametriche infatti presentano caratteristiche bimodali , riflettendo la segmentazione del tumore in una regione nucleare ed in una regione periferica , per la quale unalta densit capillare correla al grado istologico di malignit . 
altri autori in letteratura hanno calcolato i due parametri espressione di neoangiogenesi ( fpv e kps ) su modelli tumorali umani impiantati nel ratto , al fine di ottenere mappe quantitativo - anatomiche e correlarle con le informazioni immunocitochimiche ed ultrastrutturali [ 6 , 14 , 15 ]  . 
una ulteriore osservazione va compiuta sullimportanza della analisi distributiva dei parametri kps e fpv per valutare la presenza di necrosi : le metodiche radiologiche convenzionali riescono a fatica ad quantificare la necrosi nella massa neoplastica , mentre lapproccio quantitativo , utilizzato nei lavori recenti , pu essere sfruttato per stabilire gli effetti dei trattamenti fisico - chimici sulla massa tumorale [ 6 , 15 , 17 ]  . 
leterogeneit del microcircolo viene infatti dimostrata attraverso la segmentazione tumorale anche nei nostri esperimenti , i quali individuano aree distinte a diversa angiogenesi sulla base dei parametri dinamici correlati alla struttura ed alla funzione microcircolatoria . appare inoltre interessante confrontare landamento con il tempo del rapporto r1tumore / r1sangue , in particolare nella zona vitale e periferica . 
stato dimostrato che questo rapporto , con i mdc macromolecolari , ha un andamento lineare con il tempo ; lintercetta e la pendenza sono proporzionali rispettivamente al volume ematico ed alla permeabilit vascolare della regione esaminata [ 11 , 19 , 20 ]  . la dce - mri , nella nostra esperienza , si dimostrata molto efficace anche per monitorare leffetto terapeutico post - trattamento antiangiogenico . 
in particolare , nel modello sperimentale animale di cellule di colon carcinoma , possibile ottenere un riscontro gi dopo 24 ore , quando non si ha ancora nessuna modificazione del volume tumorale . 
stato infatti osservato che il microcircolo tumorale neoformato iperpermeabile alle macromolecole , e la riduzione della permeabilit un eccellente marker surrogato di attivit biologica dei farmaci [ 21 ]  . 
in ultimo , nellesperimento con il tamoxifen , abbiamo verificato come il mdc b22956 / 1 , grazie al legame con le proteine plasmatiche , e quindi con un comportamento intermedio tra un mezzo di contrasto a basso peso molecolare ed un macromolecolare puro , sembra avere la dimensione giusta e la capacit di extravasare , adatta a testare gli effetti di questo farmaco antiangiogenico sul microcircolo . 
 cisivo nel monitoraggio della terapia antitumorale [ 2225 ]  . conclusions dce - mri dedicated to the study of the microcirculation enables a noninvasive evaluation of tumour size , characteristics and vascularity . 
the technique may help identify the passage of a tumour from a quiescent to an aggressive phenotype early on and therefore enable initiation of adequate oncological treatment and quantification of changes in the microcirculation during treatment . 
mri and the development of quantitative mri methods provide a new concept of imaging , one in which emphasis is placed not only on morphology but also on biological properties of tissues to allow assessment of response to anticancer treatments . 
questo pu servire ad individuare precocemente il passaggio di un tumore da un fenotipo quiescente ad uno aggressivo , e quindi ad impostare un trattamento oncologico adeguato , quantificando le variazioni del microcircolo durante il trattamento . 
zuiani1 1institute of radiology , udine university , via colugna 50 , i - 33100 udine , italy 2institute of medical statistics , department of medical and morphological research , udine university , p.le kolbe 3 , i - 33100 udine , italy 3liver transplantation unit . 
this study was designed to establish whether the measurement of apparent diffusion coefficients ( adcs ) is clinically accurate in diagnosing liver fibrosis in a selected series of cirrhotic patients . 
twenty - eight cirrhotic patients ( mean age 58.1 years ) with histologically proven liver fibrosis and 29 healthy controls ( mean age 43.8 yeas ) underwent liver diffusion - weighted magnetic resonance ( mr ) using a 1.5 - tesla ( t ) magnet equipped with a phased - array coil . 
diffusion studies with parallel imaging [ generalized autocalibrating partially parallel acquisitions ( grappa ) ] were performed within a single breath - hold using a single - shot spin - echo echo - planar sequence ( te 74 ms ) using four b values : b = 0 , 150 , 250 and 400 s / mm2 . 
diffusion - weighted mri is an accurate tool in evaluating advanced liver fibrosis if an optimised single - shot spinecho echo - planar sequence with maximum intermediate b value is used . 
ventotto pazienti cirrotici ( et media 58 , 1 anni ) con fibrosi epatica comprovata allistologia e 29 controlli sani ( et media 43 , 8 anni ) sono stati sottoposti a rm pesata in diffusione utilizzando un magnete da 1 , 5 t equipaggiato con una bobina di superficie phased - array . 
lo studio in diffusione con parallel imaging ( grappa ) stato effettuato in singola apnea mediante una sequenza single - shot spin echo echo - planare ( te 74 ms ) , applicando quattro b - values : b = 0 , 150 , 250 and 400 s / mm2 . 
ladc medio risultato significativamente inferiore nei fegati cirrotici rispetto a quelli dei controlli ( 1 , 110 , 16 vs 1 , 540 , 1210 - 3 mm2 / s ) ( p < 0 , 0001 )  . 
lanalisi receiving operating characteristic ( roc ) ha mostrato unarea sotto la curva ( auc ) di 0 , 96 ( ci 95% : [ 0 , 87 ; 0 , 94 ] ) , dimostrando pi elevate sensibilit e specificit ( rispettivamente , 92 , 9% and 100% ) in corrispondenza di un cut - off adc di 1 , 3110 - 3 mm2 / s . 
limaging rm pesato in diffusione ( diffusionweighted mri ) uno strumento accurato nella valutazione della fibrosi epatica avanzata utilizzando una sequenza single - shot spin echo echo - planar ottimizzata con un massimo b - value di valore intermedio . 
a major focus of current clinical hepatology is the search for a technique providing noninvasive diagnosis and quantification of liver fibrosis [ 13 ]  . fibrosis complicates chronic liver diseases and progresses through different histological stages to final cirrhosis . 
noninvasive alternatives to biopsy such as transient elastography [ 15 ] , or biochemical scores such as the aspartate transaminase to platelets ratio index ( apri ) or fibrotest [ 16 , 17 ] , have been proposed , but their clinical role has yet to be established . 
several reports show that mean adcs measured by dw - mri are significantly lower in cirrhotic livers compared with noncirrhotic livers , as expected if the fibrotic distortion of lobular architecture restricts water molecule motion [ 612 , 1820 ]  . 
nevertheless , most of these studies were not targeted to selected series of patients , and the technical parameters employed in the different experiences varied widely in imaging hardware and sequence parameters , leading to discrepancies in mean adc values . 
the purpose of this study was to investigate the overall accuracy of a dw technique optimised to provide more reproducible results in diagnosing liver fibrosis in cirrhotic patients . materials and methods patients from march 2005 to april 2006 , 57 subjects were recruited for this cross - sectional study . 
twenty - eight patients were affected by liver cirrhosis ( 21 male and 7 female , age range 4174 years , mean 58.1 ) , with child - pugh class a in 24 cases , class b in 3 cases and class c in 1 case . 
al contrario , solo pochi lavori sono disponibili dedicati alle epatopatie diffuse in casistiche selezionate [ 1012 ]  . in ogni caso , uno dei maggiori argomenti di studio della epatologia corrente la ricerca di un mezzo di diagnosi e di quantificazione non invasiva della fibrosi epatica [ 13 ]  . 
la fibrosi complica le epatopatie croniche e progredisce , attraverso differenti stadi istologici , verso una cirrosi finale . lentit della fibrosi determinata , attualmente , attraverso la biopsia percutanea , associata con complicanze maggiori nello 0 , 3% dei pazienti e con una mortalit dello 0 , 018% [ 14 ]  . 
sono state proposte alternative non invasive alla biopsia , come la transient elastography [ 15 ] o scores biochimici quali lapri index o il fibrotest [ 16 , 17 ] , ma il loro ruolo clinico deve essere ancora stabilito . 
nondimeno , la maggior parte di questi studi non mirata su casistiche selezionate ed i parametri tecnici impiegati nelle varie esperienze sono tanto differenti , in termini di hardware e di parametri di sequenza , da determinare discrepanze nei valori degli adc medi . per quanto a nostra conoscenza , nessun autore , in precedenza , ha investigato laccuratezza della misurazione delladc nella diagnosi di fibrosi epatica avanzata . 
twentynine subjects were healthy blood - donor volunteers ( 21 men and 8 women , age range 2052 years , mean 43.8 ) , without previous history of significant systemic or liver diseases and / or known liver focal lesions . 
body mass index ( bmi ) was in the range of 1924 kg / m2 ( mean 20.5 ) , and laboratory indexes [ alanine aminotransferase ( alt ) , aspartate aminotransferase ( ast ) , bilirubin , glutamyl transferase ( gt ) , alkaline phosphatase ( alp ) , cholesterol level and hcv and hbv markers ] were within normal limits at the time of the last blood donation . 
subjects not fulfilling the above criteria and with concomitant alcohol and / or drug use were excluded from the study . magnetic resonance imaging mr examinations were performed using a 1.5 - tesla ( t ) system ( magnetom avanto ; siemens , erlangen , germany ) equipped with high - performance gradients ( maximum amplitude 45 mt / m )  . 
a six - element phased - array surface coil was used in conjunction with the built - in spine - array coil to improve signal reception ( total imaging matrix , siemens )  . a preliminary routine , unenhanced mr protocol was performed to select the anatomical region to examine and assess the presence of focal and / or diffuse liver signal alterations . the protocol included a true fast imaging with steady - state precession ( true - fisp ) sequence intermediate - weighted ( tr 3.69 ms , te 1.85 ms , flip angle 43 , matrix 220256 , fov 350350 mm , slices 20 , thickness 6.5 mm , intersection gap 30% , 1 average , acquisition time 11 s ) in the coronal plane followed by a multi - breath - hold , t1 - weighted , spoiled gradient echo ( spgre ) sequence , acquired in phase ( te 5.04 ms ) and out of phase ( te 2.38 s ) ( tr 100 ms , flip angle 70 , matrix 180256 , fov 350256 mm , slices 27 , thickness 6 mm , intersection gap 20% , acquisition time 40 s ) and a multibreath - hold t2 - weighted turbo spin - echo short - time inversion recovery ( tse - stir ) sequence ( tr 3770 ms , te 134 ms , ti 140 ms , matrix 154256 , fov 360270 mm , slices 27 , thickness 6 mm , intersection gap 20% , acquisition time 68 s ) , both in the transverse plane . 
a dynamic enhanced study using 0.1 ml / kg of gadobenate dimeglumine ( multihance , bracco , italy ) was subsequently performed in cirrhotic patients to exclude hypervascular , malignant focal lesions . 
era disponibile una precedente dimostrazione istologica di fibrosi epatica , documentante uno score ishak 6 , con massimo intervallo fra biopsia epatica ed mri di 3 anni ( media 1 , 3 anni )  . 
ventinove soggetti erano volontari sani , donatori di sangue ( 21 maschi ed 8 femmine , range di et 2052 anni , media 43 , 8 ) , senza storia di precedenti , significative malattie sistemiche ed epatiche e / o di lesioni epatiche focali note . 
il body mass index era compreso nellintervallo di 1924 kg / m2 ( media 20 , 5 ) , mentre gli indici di laboratorio ( alt , ast , bilirubina , gt , fosfatasi alcalina , colesterolemia , markers hcv ed hbv ) risultavano nel range di normalit al tempo dellultima donazione di sangue . 
i soggetti non rispondenti alle caratteristiche citate e con concomitante assunzione di alcool e / o farmaci sono stati esclusi dallo studio . imaging rm gli esami rm sono stati effettuati utilizzando un sistema a 1 , 5 t ( magnetom avanto , siemens , erlagen , germania ) , equipaggiato con gradienti altamente performanti ( massima amplitude di 45 mt / m )  . 
stata utilizzata una bobina phasedarray di superficie a 6 elementi , lavorante in congiunzione con la bobina spine implementata nel lettino porta - paziente , al fine di incrementare la ricezione del segnale ( total imaging matrix , siemens )  . stato effettuato uno studio preliminare di routine , senza mdc , allo scopo di selezionare la regione anatomica da esaminare e di evidenziare la presenza di alterazioni del segnale focali e / o diffuse a livello epatico . 
adc derives from linear regression analysis of the signal intensity measured at each gradient application following the equation : adc = ln s / s0 / ( b0 - b ) where b is the gradient factor , s is the signal intensity after application of the diffusion gradient , and s0 is the signal intensity at b = 0 s / mm2 . 
in this equation , is the gyromagnetic ratio , g and are the strength and the duration of the diffusion gradient pulse , respectively , and is the separation between the diffusion gradient pulses . 
further technical parameters were : tr ( cid : 2 ) , te 74 ms , epi factor 102 , matrix 192154 , fov 350230 mm , slices 15 , thickness 10 mm , interslice gap 38% , average 1 , bandwidth 1 , 532 hz / pixel , acquisition time 16 s . 
the sequence was obtained within a single breath in the transverse plane . phantom study a preliminary phantom study was performed to validate our system by applying the dw sequence with b = 0 , 150 , 250 , 400 , 600 and 800 s / mm2 to two tubes filled with 500 ml of water and acetone at ambient room temperature ( 21c )  . 
adcs of water and acetone were measured on corresponding adc maps . image analysis to eliminate the influence of liver diseases other than cirrhosis on adc measurement , two radiologists ( mb , cz ) blinded to the diagnosis and who were not readers of the dw images retrospectively reviewed the images . 
subjects with findings of previously unknown suspicious focal liver lesions were excluded from measurement , as were controls with diffuse / focal signal decrease due to steatosis and / or iron deposition on t1 - weighted out - of - phase and t2 - weighted images , respectively . 
steatosis and / or iron deposition was tolerated in cirrhotic patients as coexpression of disease [ 22 ]  . after application of the dw sequence , we obtained a set of images corresponding to each b value applied and an adc map , automatically calculated by a commercially available software ( leonardo syngo , siemens , germany )  . quantitative analysis of the adcs of liver parenchyma was performed by placing a circular region of interest ( roi ) of standard dimensions ( 1 cm2 ) on the adc map in right liver segments to avoid artefacts from abdominal wall and vascular motion . 
the roi was placed far from visible vascular and plicazione di due gradienti di diffusione ( motion - probing ) , prima e dopo limpulso a 180 e dalla acquisizione dei dati con un read - out epi [ 21 ]  . 
i gradienti motion probing erano unidirezionali , applicati lungo la direzione della codifica di strato ( asse z ) , in virt della dimostrata isotropicit del fegato [ 6 ]  . 
il valore delladc deriva da una analisi di regressione lineare dellintensit di segnale misurata ad ogni applicazione del gradiente , secondo la seguente equazione : adc = ln s / s0 / ( b0 - b ) , ove b il fattore di gradiente , s lintensit di segnale dopo lapplicazione del gradiente di diffusione , e s0 lintensit di segnale per b = 0 s / mm2 . 
in questa equazione il rapporto giromagnetico ; g e rappresentano , rispettivamente , la forza e la durata dellimpulso del gradiente di diffusione , e lintervallo fra gli impulsi dei gradienti di diffusione . 
gli ulteriori parametri tecnici erano : tr ( cid : 2 ) ; te 74 ms ; epi factor 102 ; matrice 192154 ; fov 350230 mm ; sezioni 15 ; spessore 10 mm ; gap 38% ; medie 1 ; bandwidth 1532 hz / pixel ; tempo di acquisizione 16 s . stato utilizzato un riempimento del k - spazio sequenziale in modalit partial - fourier 7 / 8 . 
la saturazione selettiva del segnale del grasso stata impiegata sistematicamente per sopprimere gli artefatti da chemical - shift . la sequenza stata acquisita in una sola apnea lungo il piano assiale . studio su fantoccio per validare il nostro sistema stato effettuato uno studio preliminare su fantoccio , applicando , a temperatura ambiente ( 21c ) , una sequenza dw con b = 0 , 150 , 250 , 400 , 600 ed 800 s / mm2 a due contenitori riempiti con 500 ml di acqua ed acetone e sottoponendo i dati ad una analisi di regressione lineare del log naturale dellintensit di segnale versus i b - values applicati . 
era stato stabilito di escludere dalla misurazione i soggetti con rilievo di lesioni focali non note sospette per malignit , cos come i controlli con decremento diffuso / focale del segnale riferibili a steatosi e / o a depositi emosiderinici , rispettivamente nelle immagini t1 - pesate in opposizione di - fase e t2pesate . 
1a , b to measure apparent diffusion coefficients ( adcs ) , three circular regions of interest ( rois ) were placed over areas of homogeneous parenchyma of right liver segments on b = 0 s / mm2 images ( a ) and then transported on the corresponding slices of the adc map ( b ) with a copy - paste operation . 
1a , b al fine di misurare i coefficienti di diffusione apparente ( adcs ) sono state posizionate , sulle immagini ottenute con b = 0 s / mm2 , tre regioni di interesse circolari ( rois ) in zone omogenee di parenchima epatico dei segmenti di destra ( a )  . 
it was decided to measure adcs only on good - quality images and in homogeneous areas of parenchyma not affected by major artefacts due to chemical shift , magnetic susceptibility , abdominal wall or vascular motion . 
 statistical analysis the shapiro - wilk test was used to check for data normality . adcs of cirrhotic patients and controls were compared using a t test or mann - whitney u test , depending on the normality check . 
positive predictive value ( ppv ) and negative predictive value ( npv ) were calculated assuming the prevalence of cirrhosis in the general population of our country ( 1% ) [ 23 ]  . 
statistical analysis was performed using medcalc statistical software , version 8.1.0 ( mariakerke , belgium )  . results phantom study the natural log of the signal intensities of water and acetone showed linear regression vs . 
lanalisi quantitativa degli adcs del parenchima epatico stata effettuata posizionando una regione di interesse ( roi ) circolare , di dimensioni standard ( 1 cm2 ) sulla mappa adc , nei segmenti epatici di destra , per evitare artefatti da motilit della parete addominale e vascolari . 
stato stabilito di misurare gli adcs solo nelle immagini di buona qualit ed in regioni omogenee di parenchima , prive di rilevanti interferenze di artefatti dovuti a chemical - shift , suscettibilit magnetica , motilit addominale o vascolare . analisi statistica la normalit dei dati stata verificata con il test di shapirowilk . 
il valore predittivo positivo ( ppv ) ed il valore predittivo negativo ( npv ) sono stati calcolati assumendo la prevalenza della cirrosi epatica nella popolazione generale del nostro paese ( 1% ) [ 23 ]  . 
2a , b graphs for apparent diffusion coefficients ( adcs ) of water ( a ) and acetone ( b ) show linear regression of the natural log of signal intensity vs . 
2a , b il grafico dei coefficienti di diffusione apparente ( adcs ) di acqua ( a ) ed acetone ( b ) mostra una regressione lineare del log naturale dellintensit di segnale versus i bvalues applicati . 
lanalisi statistica si avvalsa del software medcalc statistical , versione 8.1.0 ( mariakerke , belgio )  . patients and controls no focal liver lesions suspected for malignancy were detected in the 57 subjects . 
3a - d utilizzando una sequenza single shot spin echo echo - planare sono state ottenute immagini progressivamente pesate in diffusione di buona qualit , come evidente comparando la stessa sezione ottenuta con b = 0 s / mm2 ( a ) , b = 150 s / mm2 ( b ) , b = 250 s / mm2 ( c ) e b = 400 s / mm2 ( d )  . 
image quality was good , and in no case the presence of mild artefacts due to magnetic susceptibility or abdominal - wall motion precluded adc measurement , because they occurred in the same location , far from the right liver lobe . 
4 scatterplot of apparent diffusion coefficients ( adcs ) of cirrhotic patients ( child - pugh class a = 24 , b = 3 , c = 1 ; ishak score 6 = 28 ) and healthy volunteers ( n = 29 )  . 
as the reliability of routine laboratory tests , serum markers , quantitative liver function tests and methods such transient elastography in the diagnosis and quantification of liver fibrosis has yet to be established , percutaneous biopsy remains the gold standard [ 13 , 25 ]  . 
la qualit delle immagini dw risultata buona , ed in nessun caso la presenza di modici artefatti dovuti alla suscettibilit magnetica od alla motilit della parete addominale ha precluso la misurazione degli adcs , poich essi sono occorsi nelle medesime sedi , lontane dal lobo epatico destro . 
gli adcs sono risultati significativamente inferiori nei pazienti cirrotici rispetto ai controlli : 1 , 110 , 16 versus 1 , 540 , 12 10 - 3 mm2 / s , rispettivamente ( test t , p < 0 , 0001 ) ( tabelle 1 , 2 )  . 
laccuratezza complessiva stata stimata pari a 96 , 4% ( 55 / 57 ci 95% : [ 91 , 2% ; 99 , 9% ] )  . discussione la fibrosi rappresenta un marker istologico dellepatite cronica ( determinante il cosiddetto staging della malattia ) , che trova nella cirrosi il suo stadio finale , virtualmente irreversibile , in tutti gli score istologici utilizzati nella pratica clinica [ 24 ]  . 
poich laffidabilit nella diagnosi e nella quantificazione della fibrosi epatica dei test di laboratorio routinari , dei markers sierici , dei test quantitativi della funzionalit epatica e di metodi quali la transient elastography rimangono da stabilirsi , la biopsia percutanea rimane il gold standard [ 13 , 25 ]  . 
fatta eccezione per uno studio [ 27 ] nel quale stato utilizzato limaging rm turboflash ( siemens , erlagen , germania ) , tutti gli studi precedenti hanno impiegato una sequenza echo - planare [ 612 , 1820 ] , la maggior parte ricorrendo alla variante single - shot spin echo . 
tuttavia , gli artefatti dovuti al chemical - shift , alla suscettibilit magnetica ed alla motilit fisiologica compromettono ancora la qualit dellimmagine [ 26 ] e rischiano di alterare il posizionamento delle roi . 
for such reasons , dw - mri has been proposed as a noninvasive potential tool for the evaluation of liver fibrosis . the application of this technique to the upper abdomen has become possible with the advent of echo - planar imaging because of faster acquisition times , which reduce the effect of gross physiological motion [ 26 ]  . 
except for one study [ 27 ] in which turbo flash ( siemens , erlangen , germany ) was used , all previous studies were designed with an echo - planar mr sequence [ 612 , 1820 ] , mostly with the single - shot spin - echo variant . 
moreover , reducing acquisition time by means of parallel imaging ensured coverage of the entire liver , with no interference of artefacts on overall image quality and roi positioning . minato gli artefatti da chemical - shila riduzione del tempo di acquisizione grazie allimaging parallelo , inoltre , ha assicurato lacquisizione dellintero volume del fegato senza linterferenza di artefatti sulla qualit complessiva delle immagini e sul posizionamento delle roi . 
 [ 28 ] hanno dimostrato che il parallel imaging non compromette laccuratezza della misurazione delladc e che il suo uso corrisponde , paradossalmente , ad una migliore qualit dellimmagine , nonostante il teorico decremento del rapporto segnale / rumore . 
 [ 29 ] , i quali hanno utilizzato una sequenza finger - pulse - triggered echoplanare , negli studi precedenti le immagini dw sono state acquisite in una singola apnea per ogni b - value adottato [ 612 , 1820 ]  . 
in questa esperienza abbiamo ottenuto tutti i set di immagini corrispondenti ai b - values applicati ( 0 , 150 , 250 e 400 s / mm2 ) in una singola apnea inspiratoria , minimizzando gli effetti di section misregistration . 
 [ 28 ] demonstrated that parallel imaging does not compromise the accuracy of adc measurement and could correspond to a paradoxically improved image quality despite the theoretical decrease in the signal - to - noise ratio ( snr )  . 
 [ 29 ] who used a finger - pulsetriggered echo - planar sequence , all previous studies acquired dw images within a breath - hold for each adopted b value [ 612 , 1820 ]  . 
we obtained all sets of images corresponding to the b values applied ( 0 , 150 , 250 and 400 s / mm2 ) within a single breath - hold , minimising section misregistration . 
although the ideal te of a dw sequence should approximate the t2 relaxation time of the liver parenchyma ( 466 ms ) [ 30 ] to maximise the snr , tes in previous experiences were in the range of 54123 ms [ 612 , 1820 ]  . 
nonostante il te ideale di una sequenza dw debba approssimare il tempo di rilassamento t2 del parenchima epatico ( 466 ms ) [ 30 ] al fine di massimizzare il snr , i tes nelle precedenti esperienze erano compresi in un range di 54123 ms [ 612 , 1820 ]  . 
nel presente studio stato utilizzato un te di 74 ms come compromesso fra lottenimento di immagini di buona qualit acquisite in tempi rapidi ed una misurazione pi affidabile delladc utilizzando b - values pi alti . lo studio in diffusione del fegato poggia sullipotesi che la distorsione dellarchitettura lobulare , dovuta allaccumulo di fibre di collagene strettamente legate e povere di protoni , restringa il moto browniano dellacqua allinterno di un parenchima fibrotico . 
solo due studi si sono incaricati di comparare gli adcs dei pazienti cirrotici con quelli dei controlli , ma utilizzando una analisi retrospettiva [ 12 ] od impiegando una bobina body , responsabile di immagini caratterizzate da un basso snr [ 11 ]  . 
 dw - mri of the liver relies on the hypothesis that architectural lobular distortion due to the tightly bound and proton - poor collagen fibres restricts water brownian motion within liver fibrotic parenchyma . 
the most influencing factor in explaining these discrepancies is the set of adopted b values , with maximum b value varying from 55 to 1 , 200 s / mm2 [ 6 , 7 ]  . 
as a general rule , lower b values correspond to higher mean adcs , assuming an overestimation due to signal contamination from other intravoxel incoherent motions ( ivim ) , che ladc medio risulta significativamente inferiore nel primo gruppo . 
 gli adcs medi variavano ampiamente da 0 , 600 , 19 a 2 , 711 , 6210 - 3 mm2 / s nei pazienti cirrotici e da 0 , 690 , 31 a 3 , 551 , 7510 - 3 mm2 / s nei soggetti sani [ 6 , 20 ] , a causa delle differenze nellhardware rm e nel profilo delle sequenze . il fattore pi influente nello spiegare simili discrepanze il set di b - values adottati , con un massimo b compreso fra 55 e 1200 s / mm2 [ 6 , 7 ]  . 
come regola generale , b - values pi bassi corrispondono ad adcs medi pi elevati , verosimilmente sovrastimati a causa della contaminazione del segnale da parte di altri moti incoerenti intravoxel ( ivim ) , e particolarmente dalla microperfusione sanguigna . 
in the present study , a maximum b = 400 s / mm2 was adopted to prevent signal degradation related to higher b values . the aim of this study was to assess whether adc measurement using an optimised dw - mri technique is an accurate tool for diagnosing advanced liver fibrosis . 
to our knowledge , this is the first study to evaluate the accuracy of dwmri in diagnosing advanced liver fibrosis in a selected series of patients using an optimised protocol . 
come atteso , gli adcs ottenuti erano significativamente inferiori nei fegati cirrotici rispetto a quelli dei controlli : 1 , 110 , 16 versus 1 , 540 , 1210 - 3 mm2 / s , e sovrapponibili a quelli precedentemente riportati usando set di b - values simili [ 8 , 18 ]  . 
per quanto a nostra conoscenza , questo il primo studio ad indagare laccuratezza della rm in diffusione nel diagnosticare la fibrosi epatica avanzata su una casistica selezionata ed utilizzando un protocollo ottimizzato . 
la sensibilit e la specificit sono risultate del 92 , 9% e del 100% , rispettivamente , in corrispondenza di una soglia adc di discriminazione fra fegati severamente fibrotici e fegati sani di 1 , 3110 - 3 mm2 / s . 
in corrispondenza di una soglia di 1 , 3110 - 3 mm2 / s la sensibilit e la specificit sono risultate , rispettivamente , del 92 , 9% e del 100% . spondence with an adc cutoff of 1.3110 - 3 mm2 / s to discriminate between severely fibrotic and healthy livers . 
our results suggest that dw - mri is a promising technique for evaluating fibrosis , but before dw - mri can be considered as a possible substitute for liver biopsy , it is mandatory to determine whether there is a correspondence between adc and histological grading and , if so , whether it has clinical relevance in quantifying liver fibrosis before cirrhosis development . 
nevertheless , latter authors used a very low diffusion weighting , with a maximum b value of 250 s / mm2 . a potential limitation of this study is the relatively low diffusion weighting due to the intermediate maximum b factor ( 400 s / mm2 )  . 
 [ 32 ] suggested using higher b values to approximate the adc to the true diffusion coefficient , because at lower b values , the influence of perfusion significantly contributes to the adcs of abdominal organs . 
the present study does not demonstrate that the influence of the true diffusion coefficient at lower b values is sufficient for determining adc differences between normal and fibrotic livers , because the diagnostic accuracy of dw - mri using higher b values remains undetermined . 
 dw sia una tecnica promettente nel valutare questa condizione , ma per candidarla alla sostituzione della biopsia epatica mandatario determinare se esista una corrispondenza tra adc e staging istologico e se abbia rilevanza clinica nel quantificare la fibrosi epatica prima dello sviluppo di una cirrosi . 
questi ultimi autori , tuttavia , hanno utilizzato una pesatura in diffusione molto bassa , con un massimo b - value di 250 s / mm2 . una limitazione potenziale di questo studio la limitata pesatura in diffusione dovuta al massimo fattore b adottato ( 400 s / mm2 ) , di valore intermedio . 
 [ 32 ] hanno suggerito di utilizzare b - values pi elevati per approssimare ladc al coefficiente di diffusione vero , perch con b - values inferiori linfluenza della perfusione contribuisce significativamente nella determinazione degli adcs degli organi addominali . 
nondimeno , comparando fegati normali e cirrotici questi autori non hanno trovato significative differenze n nei rispettivi adcs ( 0 , 870 , 26 versus 0 , 840 , 2210 - 3 mm2 / s ) , n nel coefficiente di diffusione vero , n nella frazione di perfusione calcolata con una appropriata analisi matematica . 
although the effects of ageing on the human liver has not been clearly determined , in no case was progressive liver fibrosis identified as a marker of liver ageing [ 33 , 34 ] , suggesting that the degree of physiological liver fibrosis ( and , consequently , of the measured adcs ) does not vary significantly with age . 
sebbene gli effetti dellinvecchiamento sul fegato umano non siano stati completamente chiariti , in nessun caso la progressione della fibrosi epatica stata identificata come marker dellinvecchiamento [ 33 , 34 ] , suggerendo che il grado di fibrosi fisiologica ( e , di conseguenza , degli adcs misurati ) non vari significativamente con lavanzare dellet . conclusions conclusioni in conclusion , adc measurement is reproducible and rapid and unaffected by interferences from artefacts related to echo - planar imaging . 
nevertheless , because of the relatively high contribution of perfusion to determining the adc with the set of b values employed in the present study , the influence of the different intravoxel incoherent motions on determining the reported high diagnostic performance needs to be investigated . 
ciononostante , a causa del contributo relativamente elevato della perfusione nel determinare ladc con il set di b - values impiegato nel presente studio , deve essere ulteriormente chiarito il peso dei differenti ivims nella determinazione della riportata performance diagnostica . 
venezia1 1department of radiology , 2departement of oncology , siena university , policlinico santa maria , viale bracci 2 , i - 53100 siena , italy 3department of radiology , university la sapienza , viale regina elena 324 , i - 00161 rome , italy correspondence to : f.s. 
ferrari , tel : + 39 - 057 - 7233119 , fax : + 39 - 05 - 7744496 , e - mail : ferrari@unisi.it received : 17 july 2006 / accepted : 18 october 2006 / published online : 20 april 2007 abstract purpose . 
la tomografia computerizzata ha evidenziato necrosi completa nel 78% dei noduli trattati con la e nel 94% di quelli trattati con rfa ; lintervallo libero da malattia stato 16 , 508 , 1 mesi . 
i pazienti trattati con rfa hanno mostrato sopravvivenza pi lunga rispetto a quelli trattati con la , sebbene questa differenza non sia statisticamente significativa ( p = 0 , 3299 )  . 
la e rfa si sono dimostrati egualmente efficaci . tuttavia , rfa consente di ottenere migliori risultati nei pazienti con noduli pi piccoli e nei pazienti child - pugh a . parole chiave epatocarcinoma termoablazione laser ablazione con radiofrequenza ( rfa ) introduction introduzione hepatocellular carcinoma ( hcc ) is the fifth most common malignancy worldwide , with a 5.4% cancer mortality rate [ 1 , 2 ]  . 
cirrhosis is a precancerous condition with an annual rate of mail carcinoma epatocellulare ( hcc ) la quinta neoplasia maligna pi comune nel mondo , con un tasso di mortalit per cancro del 5 , 4% [ 1 , 2 ]  . 
in italia ha unincidenza di 7 , 5 / 100000 fra i maschi e di 2 , 4 / 100000 per le femmine . lepatite b e lepatite c sono le cause principali che determinano lo sviluppo di un hcc . 
the exact indications for each type of thermal ablation procedure still need to be clearly defined , so that the choice of ablation procedure is currently based on several factors . 
features of the technique , such as the size and shape of the ablation zone it generates , features of the hcc lesion such as size , location and number of nodules , and the availability of image - guided systems are all important factors in decision making [ 6 , 7 ]  . 
however , according to the current guidelines for the management of hcc , radiofrequency ablation ( rfa ) should be considered the standard ablation procedure for early unresectable hcc [ 8 ]  . 
 the aim of this study was to compare laser ablation ( la ) and rfa in treating small hcc and to evaluate the clinical outcomes in terms of long - term survival . 
 materials and methods patients from january 2003 to december 2005 , 81 cirrhotic patients ( 56 men and 25 women ) with a diagnosis of hcc and aged between 51 and 82 years ( average : 69.3 ) were included in this prospective trial . 
the hcc nodules were diagnosed by histological analysis of samples obtained with ultrasound ( us ) - guided biopsy using an 18 - gauge needle ( biomol bm 1820 , hs hospital service spa , italy )  . 
prior to any treatment , patients were informed of the benefits and risks of the treatments being proposed , and all patients signed a written consent for as prescribed by current laws , privacy and confidential treatment were assured for all patients . all patients were selected during follow - up of cirrhosis performed by upper abdominal us that had revealed the hcc nodules . 
histopathologic exams performed on all patients revealed a viral hepatitis origin in 79 patients ( 51 hcv , 17 hbv , 11 hbv + hcv ) and an alcoholic origin in two patients . before treatment , the patients were subdivided into groups using the child - pugh classification system ( 59 in child - pugh class a ; 22 in child - pugh class b )  . 
there were a total of 95 hcc nodules ( mean 1.17 per patient ) , with two nodules in 14 patients and mean diameter of 27.9 mm ( range 1040 mm )  . alpha - fetoprotein ( fp ) measurements before treatment were 474.6 ng / l on average ( range 3.57 , 720 ng / l ) ( table 1 )  . 
 forty - one patients were treated with la and 40 with rfa for a total of 128 sessions ( 66 la and 62 rfa ) ; 44 of 81 ( 54% ) underwent only a single session , whereas the other 37 ( 46% ) underwent two or three sessions , for a mean number of sessions per patient of 1.58 and a mean number of sessions per lesion of 1.34 ( table 2 )  . 
treatment groups were homogeneous with regard to hcc nodule dimensions , clinical / laboratory conditions ( with homogenous distribution of child - pugh class a and b ) , and mean age and male - to - female ratio ( table 1 )  . 
i soggetti con maggiore rischio sono quelli con infezione combinata da hbv e da hcv ; altri fattori di rischio includono let maggiore di 50 anni ed il sesso maschile [ 5 ]  . lablazione termica percutanea un trattamento accettato per i pazienti con piccolo hcc non chirurgicamente asportabile . 
le caratteristiche della tecnica ablativa ( tipo e dimensione della zona di necrosi che essa produce ) , le caratteristiche dei noduli di hcc ( dimensioni , sede e numero , disponibilit dei sistemi immagine - guidati ) , rivestono unimportanza considerevole in questa scelta [ 6 , 7 ]  . 
secondo le linee - guida correnti per il trattamento dellhcc , la termoablazione con radiofrequenza ( rfa ) dovrebbe essere considerata come il trattamento standard per lhcc non resecabile [ 8 ]  . lo scopo di questo lavoro confrontare la termo - ablazione laser ( la ) e la rfa nel trattamento del piccolo hcc e valutarne il risultato clinico in termini di sopravvivenza . materiali e metodi pazienti da gennaio 2003 a dicembre 2005 , 81 pazienti cirrotici ( 56 uomini e 25 donne ) portatori di hcc , di et compresa fra 51 e 82 anni ( media : 69 , 3 ) , sono stati inseriti nel gruppo di studio . 
i noduli di hcc erano stati diagnosticati istologicamente su campioni ottenuti mediante agobiopsia ecoguidata utilizzando un ago da 18 gauge ( biomol bm 1820 , hs hospital service spa , italia )  . 
in accordo con le leggi vigenti , la segretezza ed il trattamento dei dati personali sono stati assicurati a tutti i pazienti . tutti i pazienti del nostro studio sono stati selezionati nellambito del follow - up per cirrosi epatica ottenuto con ecografia delladdome superiore che ha evidenziato i noduli di hcc . 
lesame istopatologico eseguito per tutti i pazienti ha rivelato una natura post - epatitica della cirrosi in 79 pazienti ( 51 hcv , 17 hbv , 11 hbv + hcv ) e una natura alcolica in 2 pazienti . 
prima delle procedure di ablazione percutanea i pazienti sono stati divisi in due sottogruppi sulla base dello stadio della cirrosi epatica secondo child - pugh ( 59 pazienti in stadio child - pugh a e 22 in child - pugh b )  . 
il numero totale di noduli di hcc era 95 ( 1 , 17 in media per paziente ) , con 2 noduli in 14 pazienti ed un diametro medio delle lesioni di 27 , 9 millimetri ( range 1040 mm )  . 
other inclusion criteria were a performance status between 0 and 2 , cardiac and pulmonary function between 0 and 2 [ world health organization ( who ) ] and age ranging from 19 to 82 years . 
i sottogruppi di trattamento erano omogenei sia come di dimensioni dei noduli di hcc che come condizioni clinico / laboratoristiche ( con distribuzione delle classi a e b secondo child - pugh pressoch omogenea ) cos come in termini di et media e di rapporto maschi / femmine ( tabella 1 )  . 
patients with evidence of vascular tumour extension ( portal vein , one of two main portal branches or hepatic vein thrombosis ) , invasion of the main bile duct or extrahepatic metastases on computed tomography ( ct ) during the staging phase were excluded . 
multislice ct evaluation ( light speed 16 ct , ge medical systems , milwaukee , wi , usa ) was performed with three - phase technique ( 30 , 65 and 180 s ) following i.v. 
 pretreatment evaluation each patient underwent blood chemistry testing ( total and fractionated bilirubin , quicks time inr , albumin , platelets , ammonia , fp , ferritin and hepatic markers , if not already available ) , cardiac function and performance status testing . overall assessment of coagulation status was performed within 7 days of the percutaneous procedures , and all patients were asked about possible drug allergies and use of platelet aggregation inhibitors . 
the contrast agent , at a dose of 4 g , was administered as a bolus injection ( 23 s ) at a concentration of 400 mg / ml , and images were acquired at various time intervals : 1015 s , 2030 s and 1 , 2 , 3 , 4 , 5 and 6 min after the injection . 
with these time intervals , arterial , portal , and criteri di inclusione e di esclusione sono stati selezionati i pazienti con un nodulo unico di hcc delle dimensioni massime di 40 millimetri o con multipli noduli ( al massimo 3 ) ciascuno del diametro non superiore a 30 millimetri , non precedentemente trattati . 
gli altri criteri di inclusione sono stati un performance status tra 0 e 2 , una funzionalit cardiaca e polmonare fra 0 e 2 ( who ) e let ( 1982 anni )  . 
il rilievo del tempo di protrombina < 40% ( international normalized ratio , inr > 1 , 99 ) e / o numero di piastrine < 40000 / ml hanno determinato il rinvio delle procedure percutanee fino al ripristino dei valori adeguati in 22 pazienti . 
sono stati esclusi i pazienti che , sulla base di un esame di tomografia computerizzata ( tc ) eseguito durante la fase di stadiazione della malattia , hanno mostrato estensione vascolare del tumore ( vena porta , uno dei due rami portali principali o trombosi delle vene sovraepatiche ) , interessamento della via biliare principale o metastasi extraepatiche . la valutazione tc multislice ( light speed 16 ct , ge mdical systems , milwakee , usa ) stata ottenuta con tecnica trifasica ( 30 , 65 e 180 s ) dopo somministrazione endovenosa di bolo di 150 ml di mezzo di contrasto iodato ( ultravist 370 , schering , berlino , germania )  . 
i parametri principali dellesame erano : tempo di rotazione 0 , 7 secondi , pitch di 0 , 938 : 1 , collimazione 2 , 5 millimetri e velocit di scorrimento del tavolo 18 , 75 millimetri per rotazione dellelica . 
 before treatment , all patients also underwent a multislice ct scan ( light speed 16 ct , ge medical systems ) with the three - phase technique ( 30 , 65 and 180 s ) following an intravenous injection of a 150 - ml bolus of iodinated contrast medium ( ultravist 370 , schering )  . 
catheter inserted in an antecubital vethe time interval between pretreatment ct and the ablative procedure was 12 weeks . methods both la and rfa were performed under general anaesthesia and us guidance . 
depending on the hcc nodule size , up to four fibreoptics were positioned inside the lesion and then 5 w was applied for an exposure time of 6 min to reach 1 , 800 joules per fibre . 
at the end of the session , the fibres were withdrawn with the laser still on in order to induce hyperthermia along the needle retraction path and avoid seeding of neoplastic cells . 
 rfa was performed using a cool - tip radiofrequency system generator ( valleylab , tyco healthcare , bolder , co , usa , distributed by hs hospital service spa , aprilia , lt , italy )  . 
single electrodes with lengths of 15 , 20 and 25 cm and an active segment of 2 or 3 cm were used for hcc nodules 3 cm , whereas multiple cluster ( three - prong ) electrodes with lengths of 15 or 20 cm and an active segment of only 2.5 cm were used for hcc nodules > 3 cthe electrodes were cooled by means of an internal circuit fed by a peristaltic pump . 
 evaluation of treatment efficacy twenty - four to 48 h after treatment , all patients underwent liver us followed by triphasic ct evaluation , as described above , within 15 days . 
based on ct findings , tumour ablation ( treatment efficacy ) was defined as complete when no contrast uptake was seen in the ablation zone during the early arterial phase , or incomplete if the ablation zone appeared smaller than the initial hcc nodule and contrast uptake was seen within its margins . 
la valutazione globale dello stato coagulativo stata eseguita entro sette giorni delle procedure percutanee e tutti i pazienti sono stati interrogati riguardo ad eventuali allergie farmacologiche e ad eventuali assunzioni di farmaci antiaggreganti . 
il mezzo di contrasto , nella dose di 4 g , stato somministrato a bolo ( in 23 s ) in concentrazione di 400 mg / ml e le immagini sono state acquisite a vari intervalli di tempo , a partire da 1015 s , a 2030 s e a 1 , 2 , 3 , 4 , 5 e 6 minuti dopo liniezione . 
utilizzando questi intervalli sono state ottenute le fasi arteriosa , portale e parenchimale tardiva . nellambito della valutazione pre - trattamento percutaneo , tutti i pazienti hanno eseguito un esame tc multislice ( light speed 16 ct , ge medical systems , milwakee , usa ) con tecnica trifasica ( 30 , 65 e 180 s ) dopo somministrazione endovenosa di bolo di 150 ml di mezzo di contrasto iodato ( ultravist 370 , schering , berlino , germania )  . 
i parametri principali dellesame erano : tempo di rotazione 0 , 7 secondi , pitch 0 , 938 : 1 , collimazione 2 , 5 millimetri e velocit di scorrimento del tavolo 18 , 75 millimetri per rotazione dellelica . stata ottenuta soltanto una fase arteriosa ; il mezzo di contrasto stato iniettato a 4 ml / s tramite un accesso venoso da 18 gauge in una vena antecubitale del braccio . 
lintervallo di tempo fra la tc ed il trattamento ablativo variato fra 1 e 2 settimane . metodi sia la la che la rfa sono state effettuate in anestesia generale e sotto guida ecografica . la la stata effettuata usando una fonte di luce al neodymium yttrium - aluminium - garnet , nd - yag ( deka - mela , elen , firenze , italia ) , con una lunghezza donda continua di 1 , 064 tale sorgente stata convogliata con un beamsplitter ottico ( smart 1064 hcc , deka - mela , elen , firenze , italia ) munito di 4 fibre ottiche di quarzo di 300 m , flessibili , a punta piatta , sterili e prive del rivestimento esterno nel loro tratto terminale . 
a seconda della dimensione del nodulo di hcc sono state posizionate fino a 4 fibre nella lesione impiegando 5 w per 6 minuti in modo da erogare 1800 joules per fibra . 
terminato il trattamento , le fibre sono state retratte , con il laser acceso , in modo da indurre ipertermia durante il tragitto di ritorno dellago per evitare un possibile seeding di cellule neoplastiche . la rfa stata realizzata impiegando un generatore cool tip radiofrequency system ( valleylab , boulder , tyco healthcare , colorado , usa )  . 
sono stati utilizzati elettrodi a radiofrequenza closet - tip , tutti rigorosamente monouso , da 17 gauge , raffreddati internamente ( hs hospital service , aprilia , latina , italia ) , di tipo singolo con lunghezze di 15 , f.s. 
comparison of techniques and long - term results tumour ablation , patients underwent additional treatment sessions ( 33 in total : 21 for the la group and 12 for the ra group ) , whereas in the case of complete tumour ablation , patients were scheduled for follow - up . 
at 1 month and every 3 months thereafter , patients underwent alkaline phosphatase , total and fractionated bilirubin , transaminases , gamma glutamyl transpeptidase ( gt ) , carcinoembryonic antigen ( cea ) , albumin , quicks time and inr , complete blood count ( cbc ) and platelets and fp testing . the child - pugh class was reviewed , and upper abdominal ultrasound was performed to assess portal flow . 
 at 3 months and every 6 months thereafter , patients underwent triphasic ct for evaluation of the ablation zone and detection of local tumour progression and / or new hcc lesions . 
in evaluating disease recurrence , we distinguished between local tumour progression ( the presence of neoplastic tissue within the same liver segment as that of a treated hcc nodule ) and new hcc lesion ( the development of nodules in a different liver segment )  . 
in segment iv , neoplastic tissue arising farther than 5 cm from the site of the initial hcc was regarded as a new hcc lesion rather than as local tumour progression . 
 complications 20 , 25 cm e segmento attivo di 2 o 3 cm ( per noduli fino a 3 cm ) ; per i noduli pi grandi di 3 cm stato impiegato un tipo cluster ( elettrodo a tre punte ) con lunghezze di 15 o 20 cm e segmento attivo di 2 , 5 cgli elettrodi sono stati raffreddati per mezzo di un circuito interno alimentato da una pompa peristaltica . 
durante lablazione termica la pompa peristaltica , instillando acqua a 0c , ha permesso di mantenere la punta dellago ad una temperatura di 2025c . ogni seduta di rfa ha richiesto 1012 minuti al massimo della potenza , mantenendo limpedenza del circuito entro i 10 . 
alla fine del trattamento gli elettrodi sono stati estratti innalzando la temperatura per sterilizzare il percorso ed evitare il seeding cellulare . valutazione dellefficacia del trattamento a distanza di 2448 ore dalla conclusione della sessione di trattamento tutti i pazienti sono stati sottoposti ad una ecografia del fegato ed entro 15 giorni ad una tc con tecnica trifasica , come descritto prima . 
sulla base dei risultati tc , lablazione del tumore ( efficacia del trattamento ) stata definita come completa quando nella fase precoce arteriosa non stato osservata alcuna impregnazione di mezzo di contrasto nella zona di ablazione , o incompleta se la zona di ablazione risultata pi piccola rispetto al nodulo iniziale di hcc e ha presentato impregnazione allinterno entro i margini della zona di ablazione . 
nel caso di ablazione incompleta , i pazienti sono stati sottoposti ad ulteriori sessioni ( 33 in tutto , 21 per il gruppo la e 12 per il gruppo rfa ) , mentre nel caso di ablazione completa , i pazienti sono stati inclusi nel protocollo di follow - up . complications were classified according to the society of interventional radiology ( sir ) grading system [ 9 ]  . 
 follow - up statistical analysis all patients were followed up , and all data ( personal , clinical , laboratory and biopsy ) were collected and entered into a database . 
al primo mese e successivamente ogni tre mesi , sono stati dosati la fosfatasi alcalina , la bilirubina totale e frazionata , le transaminasi , le gamma glutamil - traspeptidasi ( gt ) , lantigene carcinoembrionale ( cea ) , lalbumina , il tempo di quick e linr , lemocromo con le piastrine e lfp . 
la classe child - pugh stata rivalutata ed stata effettuata unecografia delladdome superiore per controllare il flusso portaal terzo mese , ed in seguito ogni 6 mesi , stata eseguita una tc con tecnica trifasica per studiare la zona di ablazione , linsorgenza di recidiva locale e / o di nuove lesioni . 
nella valutazione complessiva della ripresa di malattia stata distinta la recidiva locale ( la presenza di tessuto neoplastico nel segmento epatico del nodulo di hcc sottoposto a trattamento ) , dalla nuova lesione di hcc ( linsorgenza di noduli in segmenti epatici diversi da quello del trattamento )  . 
nel iv segmento epatico , la rilevazione di tessuto neoplastico ad una distanza superiore a 5 centimetri dal nodulo iniziale di hcc stata considerata come un nuovo nodulo di hcc piuttosto che una recidiva locale . 
comparison of techniques and long - term results table 3 complete tumour ablation achieved during the first session and incidence of disease recurrence ( local tumour progression and new tumour foci ) showing disease - free interval sample disease recurrence complete tumour ablation no . 
in addition to the first session , scheduled for all of the 95 nodules , 33 additional sessions were performed : 13 of these ( 39.4% ) were required to achieve complete tumour ablation , 15 ( 45.4% ) to treat local tumour progression and 5 ( 15.2% ) to treat new hcc lesions . 
of these , 60% appeared 1224 months after treatment and the remaining 40% within the first 12 months ; no local tumour progression was observed later than 24 months after treatment . 
tutte le altre complicanze sono state considerate come minori . analisi statistica tutti i pazienti sono stati seguiti nel tempo e tutti i dati ( personali , clinici , di laboratorio e bioptici ) sono stati raccolti ed stato creato un database per questo studio . 
le curve di sopravvivenza sono state ottenute mediante il metodo kaplan - meier e le differenze tra di esse sono state analizzate attraverso il log - rank test . lanalisi dei fattori prognostici stata effettuata con il metodo di regressione di cox . 
comparison of techniques and long - term results sessions 1 session additional sessions complete tumour ablation local tumour progression new tumour foci total table 4 additional sessions total la , laser ablation ; rfa , radiofrequency ablation tabella 4 trattamenti aggiuntivi totale la , laser ablation ; rfa , radiofrequency ablation totale trattamenti prima sessione trattamenti aggiuntivi necrosi tumorale recidive locali nuovi noduli totale fig . 
1 incidenza complessiva di ripresa di malattia suddivisa per tipo di trattamento . tected during follow - up were both treated with the same technique as used in the original treatment . 
 during the weeks following the first session , fp levels returned to normal in all patients in whom treatment had been successful ; in cases of local tumour progression or new hcc foci , a new elevation of fp levels occurred . 
 cumulative survival rates were calculated for child - pugh a and b groups and for the la and rfa treatment groups with the kaplan - meier method ( table 5 )  . 
 univariate analysis of survival rates revealed statistically significant differences between child - pugh a and b groups ( p < 0.0001 ) , hcc nodules 2525 mm ( p = 0.0001 ) and patients with one hcc nodule vs . 
ottantadue noduli ( 86% ) hanno richiesto una singola seduta , mentre per gli altri 13 ( 14% ) stato effettuato pi di un trattamento ( tabella 3 )  . 
oltre alla prima sessione , prevista per tutti i 95 noduli , sono state effettuate 33 sessioni supplementari : 13 di queste ( 39 , 4% ) sono state necessarie per realizzare lablazione completa del tumore , 15 ( 45 , 4% ) per trattare la progressione locale del tumore e 5 ( 15 , 2% ) per trattare i nuovi noduli di hcc . 
ventuno sessioni supplementari sono state necessarie per il gruppo della la e 12 per il gruppo della rfa ( tabella 4 )  . la necrosi completa stata raggiunta nel 78% dei noduli trattati con la e nel 94% di quelli trattati con rfa . 
lintervallo libero da malattia risultato 16 , 508 , 1 mesi ( 15 , 457 , 99 per i pazienti trattati con la e 17 , 788 , 52 mesi per quelli sottoposti a rfa ) ( tabella 3 )  . sono stati osservati quindici casi di recidiva locale ( 15 , 8% di tutti i noduli trattati )  . 
il 60% di questi si sono manifestati fra 12 e 24 mesi dopo il trattamento , il restante 40% entro i primi 12 mesi ; nessuna recidiva locale si osservata oltre i 24 mesi . 
il 20% di questi pazienti ha presentato una nuova lesione tra 12 e 24 mesi e l80% tra 24 e 36 mesi ( intervallo libero da malattia 25 , 44 , 33 mesi )  . 
sia le recidive locali che i nuovi noduli individuati durante il follow - up sono stati trattati con la stessa metodica del primo trattamento . nel corso delle settimane successive alla fine del primo trattamento , i livelli sierici di fp sono rientrati nella norma in tutti i pazienti trattati con successo ; nei casi di ripresa di malattia o di comparsa di nuovi noduli di hcc si verificato un nuovo incremento dei valori di fp . 
comparison of techniques and long - term results table 6 log - rank test of patients age , gender , child - pugh class , maximum nodule diameter , number of hepatocellular carcinoma ( hcc ) nodules and type of treatment ( child - pugh class stratifications and max ) variable log - rank test child - pugh : a ( n = 59 ) vs . 
il modello cox indica che la classe child - pugh il fattore di sopravvivenza prognostico pi importante . discussione in uno studio prospettico , la rfa e liniezione percutanea di etanolo ( pei ) sono stati messi a confronto nel trattamento di 86 pazienti con hcc , unico o multifocale , delle dimensioni 30 mm ; lablazione completa stata ottenuta in 47 noduli su 52 totali trattati con rfa ( 90% ) ed in 48 su 60 noduli sottoposti a pei ( 80% ) , con una media rispettivamente di 1 , 2 e 4 , 8 sessioni [ 10 ]  . 
 [ 11 ] hanno effettuato uno studio randomizzato per confrontare lefficacia della rfa e della pei nel trattamento dei noduli di hcc 50 millimetri , in pazienti con al massimo 3 noduli e quadro di cirrosi compensata . 
dopo 2 anni di follow - up i pazienti tratti con rfa hanno mostrato una pi bassa percentuale di recidive locali ed un periodo libero da malattia pi lungo rispetto ai pazienti trattati con pei [ 11 ]  . 
 [ 12 ] hanno valutato lefficacia e la sicurezza della rfa in 88 pazienti per un totale di 101 noduli di hcc con diametro 35 mgli autori hanno osservato un tasso cumulativo di sopravvivenza ad 1 , 3 e 5 anni rispettivamente dell89% , del 62% e del 33% con un periodo libero da malattia medio di 19 mesi . 
inoltre , negli studi concernenti la rfa , i pazienti con noduli in prossimit dellilo epatico o della colecisti sono stati generalmente esclusi , sebbene secondo pacella [ 15 ] in questi casi sarebbe possibile la termoablazione mediante la con fibre sottili . per quanto riguarda il numero di sessioni di trattamento , i nostri risultati appaiono simili a quelli ottenuti da livraghi fig . 
3 cumulative survival curves ( kaplan - meier with rectilinear interpolation ) in relation to diameter of hepatocellular carcinoma ( hcc ) nodule : 25 mm ( n = 28 ) vs . 
 discussion in one prospective study , rfa and percutaneous ethanol injection ( pei ) were compared in 86 patients with single or multiple hcc 30 mcomplete tumour ablation was achieved in 47 out of 52 tumours treated with rfa ( 90% ) and in 48 out f.s. 
 [ 10 ] ( rfa con elettrodi raffreddati internamente ) , che hanno segnalato un valore di circa 1 , 2 sessioni per nodulo , con possibilit di trattare i piccoli noduli di hcc in una singola seduta nella maggior parte dei casi . nella nostra esperienza , la capacit della rfa di indurre ablazione tumorale completa nella prima sessione stata del 94% . 
confrontando questo valore con quello ottenuto mediante la la ( 78% ) , occorre notare che vi era una piccola differenza nel diametro medio dei noduli di hcc ( 28 , 9 millimetri nel gruppo la contro 26 , 7 millimetri nel gruppo rfa )  . 
la capacit di ablazione risulta effettivamente collegata alle dimensioni del tumore e alla semplicit del trattamento ( tempo pi breve e uso di singoli aghi anzich di aghi a grappolo )  . 
utilizzando la rfa con elettrodi raffreddati internamente nel trattamento di 51 noduli di hcc di dimensioni medio - grandi ( 3050 millimetri ) , livraghi et al . [ 16 ] hanno riportato le seguenti percentuali di ablazione : in 36 noduli ( 71% ) stata ottenuta completa ablazione , in 12 noduli ( 24% ) il 90%99% di ablazione e in 3 noduli ( 6% ) la percentuale di ablazione stata soltanto del 50%89% . 
tuttavia , noi consideriamo una percentuale pi bassa o pi alta del 90% di basso valore indicativo per la prognosi del paziente , che in ogni caso deve essere sottoposto ad ulteriori trattamenti . non abbiamo osservato complicanze durante le sessioni di trattamento . 
le complicanze minori ( dolore , febbre , versamento pleurico , ematomi sottocapsulari ) sono state da noi rilevate soltanto raramente ed in ogni caso sono state di importanza secondaria , in accordo con i dati pubblicati ( < 5% ) [ 12 , 17 ]  . il nostro parere , in accordo con le linee guida di barcellona [ 18 ] , di considerare lintero periodo libero da malattia , che nella nostra esperienza risultato essere di 17 , 78 mesi per i pazienti trattati con rfa , in linea con i risultati pubblicati . 
nel nostro studio abbiamo considerato come recidiva locale il riscontro di tessuto neoplastico nello stesso segmento del nodulo trattato , perch non proponibile un cut - off di distanza in mm , ad eccezione del iv segmento . 
un recente lavoro di harrison et al . [ 19 ] sullosservazione di ripresa di malattia mette in evidenza come la recidiva sia un evento frequente in pazienti con hcc non resecabile trattati con rfa . 
le percentuali di sopravvivenza osservate nei pazienti trattati con rfa sono sovrapponibili a quelle di altri studi analoghi [ 11 , 12 ]  . la stratificazione in sottogruppi child - pugh ha mostrato come la malattia epatica di base sia determinante ai fini della sopravvivenza . 
after a 2 - year follow - up , patients treated with rfa had a lower rate of local recurrence and a longer disease - free interval compared with those treated with pei [ 11 ]  . 
evaluated the efficacy and safety of rfa in 88 patients with 101 hcc nodules 35 mthe authors reported a cumulative survival rate of 89% , 62% and 33% at 1 , 3 and 5 years , respectively , and an average disease - free interval of 19 months . 
moreover , studies of rfa have generally excluded patients with lesions near the hepatic hilum or the gallbladder , whereas according to pacella et al . , these patients can be treated by la with thin fibres [ 15 ]  . as regards the number of treatment sessions , our results are similar to those of livraghi et al . 
 [ 10 ] ( who used rfa with internally cooled electrodes ) , who reported approximately 1.2 sessions per lesion , with most small hcc nodules being treated in a single session . 
6 cumulative survival curves ( kaplan - meier with rectilinear interpolation ) in relation to treatment , stratified by child - pugh class : a : radiofrequency ablation ( ra ) ( n = 28 ) vs . 
in our experience , minor complications ( such as pain , fever , pleural effusion , subcapsular haematoma ) were rare and of little significance , in agreement with previous studies ( < 5% ) [ 12 , 17 ]  . 
 in accordance with the barcelona guidelines [ 18 ] , we consider the entire disease - free interval , which was 17.78 months for patients treated with rfa in our study , in line with current data . 
local tumour progression was considered as any neoplastic tissue seen in the same segment as that of a previously treated hcc nodule , as no cutoff distance can be proposed ( with the exception of segment iv )  . 
however , the biological features of this tumour ( that is , an ab initio organ pathology ) make it clear that disease recurrence is not directly related to the procedure itself . 
una zona di ablazione pi grande o uguale in dimensioni al nodulo trattato stata ottenuta in 89 noduli su un totale di 92 ( 97% ) con una media di 1 , 1 sedute di trattamento per nodulo . 
durante il followup , 5 degli 89 noduli , in cui era stata ottenuta ablazione completa ( 6% ) , hanno mostrato una recidiva locale ( periodo libero da malattia medio di 14 , 8 mesi ) ed in 36 pazienti su 74 ( 49% ) sono stati osservati nuovi noduli di hcc ( periodo libero da malattia medio di 17 , 7 mesi )  . 
il tasso cumulativo di sopravvivenza a 1 , 3 e 5 anni stato rispettivamente del 99% , 68% e del 15% , senza significative differenza tra il gruppo child - pugh a ed il gruppo child - pugh b . 
sono state osservate soltanto 3 complicanze minori e nessuna complicanza maggiore . confrontata con la pei , la la presenta un rischio di impianto di cellule neoplastiche ( seeding ) pi basso e spesso riesce ad indurre la necrosi completa in una sola seduta di trattamento [ 20 ]  . 
 [ 21 ] hanno confrontato i risultati a distanza della la , della pei e della embolizzazione arteriosa transcatetere ( tace ) nel trattamento del piccolo hcc in 131 pazienti cirrotici . 
i pazienti sottoposti a la hanno mostrato una sopravvivenza ( statisticamente significativa ) pi lunga di quella dei pazienti trattati con tace e pei , cos che la la si dimostrata come il trattamento pi efficace per la sua ridotta invasivit , il numero limitato di sedute , la necrosi completa in quasi tutti i casi e la migliore sopravvivenza [ 21 ]  . 
an ablation zone larger than or the same size as the lesion was achieved in 89 of 92 nodules ( 97% ) , with an average of 1.1 sessions for each hcc . 
the cumulative survival rates were 99% , 68% and 15% at 1 , 3 and 5 years , respectively , without significant differences between childpugh class a and b patients . 
patients undergoing la had a statistically significant longer survival than those treated with tace and pei , so la proved to be the most effective treatment owing to its minimal invasiveness , reduced number of sessions , complete necrosis in almost all cases and better survival rates [ 21 ]  . 
in termini di tasso di sopravvivenza , la la si dimostrata come tecnica migliore rispetto sia alla pei che alla tace , con risultati sovrapponibili a quelli del trattamento combinato [ 22 ]  . il nostro gruppo di pazienti trattato con la stato sottoposto ad una media di 1 , 46 sessioni / nodulo di hcc , un valore maggiore rispetto a quello del gruppo rfa . 
se consideriamo la ripartizione delle sessioni aggiuntive di trattamento ( tabella 4 ) , possiamo notare che si sono rese necessarie 10 sedute per ottenere la completa ablazione nel gruppo la , mentre 3 sessioni sono state necessarie nel gruppo rfa . 
abbiamo osservato che nei noduli di hcc delle dimensioni di 34 cm stato pi difficile ottenere una completa ablazione in una sola seduta di trattamento utilizzando la la rispetto alla rfa , che ha il vantaggio di disporre degli aghi a grappolo . 
 [ 23 ] hanno rilevato che nei noduli di hcc trattati con la , il follow - up con tc ha mostrato ablazione completa di tutti i noduli < 40 mm , ma non in tutti i noduli > 50 m ferrari et al . 
 [ 22 ] hanno riportato che nel trattamento del grande hcc con la la vi sono differenze significative sia riguardo al tasso di sopravvivenza che nellablazione tumorale completa a favore dei pazienti con noduli di hcc < 50 mm rispetto a quelli con noduli 50 m nella nostra esperienza , il tasso di progressione tumorale locale e dei nuovi noduli di hcc si rivelato rispettivamente pi alto e pi basso in confronto ai dati presenti in letteratura [ 15 ]  . 
comparison of techniques and long - term results table 7 cox model for prognostic survival factors variable regression coefficient exp ( coefficient ) global 2 tabella 7 analisi multivariata secondo il modello di regressione di cox dei fattori prognostici sulla sopravvivenza regressione coefficiente exp ( coefficiente ) 2 globale p value exp , exponential ; hcc hepatocellular carcinoma child - pugh class largest diameter no . 
 our group of patients treated with la underwent an average of 1.46 sessions per hcc nodule , more than with rfa . if we consider the distribution of additional sessions ( table 4 ) , we can see that the la group required ten procedures to achieve complete tumour ablation , whereas the rfa group required three sessions . 
this difference is due to the lower rate of complete tumour ablation ( 78% ) obtained with la . we observed that in hcc nodules measuring 34 cm , it is more difficult to achieve complete ablation in a single la session compared with rfa , which has the advantage of using cluster needles . 
reported that in hcc nodules treated with la , ct follow - up demonstrated complete ablation of all lesions < 40 mm but not in all nodules > 50 mm [ 23 ]  . 
reported that in the treatment of large hcc with la , there are significant differences in terms of both survival and complete tumour ablation , with better results being achieved in patients with hcc nodules < 50 mm compared with those > 50 mm [ 22 ]  . 
 in our study , we had a higher rate of local tumour progression rate and a lower rate of new hcc nodules compared with previous reports [ 15 ]  . 
the survival rate of the la group was 88% , 56% and 23% at 12 , 36 and 60 months : compared with pacellas findings , our patients had a lower survival rate at 12 and 24 months but a higher survival rate at 60 months [ 15 ]  . 
il tasso di sopravvivenza del gruppo di pazienti trattati con la stato dell88% , 56% e 23% rispettivamente a 12 , 36 e 60 mesi ; il confronto con lo studio di pacella [ 15 ] mostra che a 12 e 24 mesi i nostri pazienti hanno un tasso di sopravvivenza pi basso , mentre risultato pi alto a 60 mesi . 
questa differenza potrebbe essere dovuta al fatto che i noduli di hcc del gruppo di studio di pacella erano in media pi piccoli dei nostri ( 24 mm vs 29 mm ) e che leffetto terapeutico si dimostrato nel breve periodo ; probabile che i pazienti vissuti pi a lungo fossero portatori di neoplasie meno aggressive . abbiamo confrontato i risultati a lungo termine della la e della rfa nel trattamento del piccolo hcc . 
i due gruppi erano omogenei senza nessuna sostanziale differenza di et , sproporzione fra maschi e femmine , classe child - pugh , numero dei noduli di hcc e valori sierici di fp . 
il diametro medio dei noduli di hcc trattati con rfa era di 26 , 7 mm , mentre quello dei noduli trattati con la era di 28 , 9 mil tasso di ablazione tumorale completa stato del 78% per la e del 94% per rfa . 
tuttavia necessaria una certa esperienza nellapproccio percutaneo ecoguidato . in accordo con i dati presenti in letteratura , il maggior numero di recidive stato osservato nei primi 2 anni successivi alla termo - ablazione , ma non si sono osservate differenze significative tra i due gruppi di trattamento . 
the mean diameter of the hcc nodules treated with rfa was 26.7 mm , whereas that of the nodules treated with la was 28.9 plications , as both methods are safe . 
these data , however , clearly refer to a small study group , and a larger number of patients and a finer stratification might have revealed significant differences ( though probably only as regards age and fp values )  . 
the latter p value is so high that it deserves consideration : in patients with more severe cirrhosis , the survival rate was conditioned by the underlying disease independent of treatment . 
it is likely that , used in smaller nodules , rfa is able to generate an optimal safety margin ( demonstrated by the higher rate of complete ablation ) while causing minimal damage to the liver parenchyma , already compromised by cirrhosis . 
 [ 22 ] sostengono che il paziente con un nodulo singolo di hcc avr un tasso di sopravvivenza pi alto rispetto a quello con hcc multifocale indipendentemente dalle dimensioni del nodulo . 
probabile che nel paziente con hcc multifocale il comportamento biologico sia differente rispetto al singolo nodulo di hcc , mostrando un andamento peggiore sia in termini di sopravvivenza che di ripresa di malattia . daltra parte , let , il sesso , i valori di fp pre - trattamento non sono rilevanti in termini di sopravvivenza ( tabella 6 )  . 
chiaro che questi dati si riferiscono ad un piccolo gruppo di studio ; presumibilmente con un numero pi alto di pazienti e con una pi fine stratificazione sarebbe stato possibile osservare alcune differenze significative ( anche se probabilmente solo per let ed i valori di fp )  . 
nel confronto dei tassi globali di sopravvivenza fra i pazienti trattati con le 2 tecniche non sono state osservate differenze statisticamente significative ( p = 0 , 3299 ) anche se la figura 5 e la tabella 5 mostrano che la rfa presenta tassi di sopravvivenza pi alti rispetto alla la . 
lo studio stratificato allappartenenza ad una classe child - pugh ha dimostrato che ci sono differenze statisticamente significative fra la sopravvivenza dei pazienti child - pugh a trattati con rfa e quelli trattati con la ( p = 0 , 0174 )  . 
questo ultimo dato ha un valore cos elevato che deve far riflettere : nei pazienti con una condizione cirrotica pi grave , il tasso di sopravvivenza stato determinato sostanzialmente dalla patologia di base qualunque sia stato il trattamento effettuato . 
la stratificazione dei pazienti in sottogruppi in relazione alla dimensione del nodulo di hcc ( noduli di hcc 25 mm vs noduli > 25 mm ) ha mostrato analoghi risultati : nel gruppo di pazienti con noduli di hcc pi piccoli , quelli trattati con rfa hanno un tasso di sopravvivenza pi alto rispetto a quelli trattati con la ( p = 0 , 0818 ) , mentre questa differenza non si osserva nel gruppo di pazienti con noduli di hcc pi grandi ( p = 0 , 7605 )  . 
 probabile che nel trattamento dei noduli di hcc pi piccoli la rfa riesca ad indurre un margine di sicurezza ottimale ( lo dimostra la pi alta percentuale di ablazione tumorale completa ) creando allo stesso tempo il minor danno possibile al parenchima epatico , compromesso dalla malattia cirrotica . conclusioni nella nostra esperienza , la la e la rfa si sono rivelate trattamenti ugualmente efficaci . 
fifty - two patients underwent us examinations for bloody nipple discharge , palpable retroareolar masses , retroareolar opacities or ductal pattern on mammography . us enabled visualisation of mammary - duct ectasia ( simple or pseudocystic , retroareolar and / or peripheral ) and focal masses ( endoluminal or periductal , with ill - defined or regular margins )  . all patients with nipple discharge underwent cytological evaluation . 
in 38 / 52 cases , us diagnosed mammary - duct ectasia and in 30 / 52 cases , the presence of focal masses ( mean size 7 mm )  . 
lus ha permesso lindividuazione dei dotti ectasici ( ectasie duttali semplici o pseudocistiche , retroareolari e / o periferiche ) e di eventuali noduli ( intraluminali e periduttali , con margini regolari o sfumati )  . 
pu considerarsi indagine complementare alla galattografia o sua valida alternativa nei casi in cui questa non risulti effettuabile . key words breast galactography ultrasonography papilloma benign ductal disease parole chiave mammella galattografia ecografia papilloma patologia duttale benigna introduction introduzione breast ultrasonography ( us ) is a widely used , noninvasive , easily reproducible and inexpensive imaging modality . 
rappresenta un valido supporto diagnostico alla mammografia , di cui incrementa i valori di sensibilit e specificit ; inoltre lecografia mammaria ormai considerata come indagine di primo livello nello studio di donne al di sotto dei 35 anni di l . 
multiple papillomas of terminal ducts in young patients are less common though important forms , as they may degenerate in 25% of cases and are considered precursors to ductal carcinoma in situ ( dcis ) [ 8 ]  . 
duct size and the intraductal productive process are fundamental for visualising these diseases : papillomas often cannot be characterised by using mammography alone , and a suspicion of papilloma calls for further investigations , such as galactography and / or breast us , also in view of the patients age [ 9 , 10 ]  . the aim of this study was to evaluate , on the basis of preliminary data derived from 13 months of work , the diagnostic contribution of breast us in the study of patients with suspected ductal disease by measuring the techniques sensitivity , specificity and positive and negative predictive values . materials and methods all breast us examinations performed at the policlinico umberto i of la sapienza university in rome between january 2005 and february 2006 were reviewed , and 52 women ( age range 2874 years ; mean 45 years ) with clinical or imaging findings suspicious for ductal disease were selected . inclusion criteria were as follows ( table 1 ) : 1 . 
presence of nodular opacity in the retroareolar region and / or of prominent retroareolar ducts on mammography [ 11 ] forty - five patients had undergone preliminary mammography , with the following results : 12 showed only signs of prominent retroareolar ducts , which were bilateral in seven and unilateral in five ; 13 patients had nodular opacities and 20 had negative mammograms . 
il ruolo di tale metodica si evoluto negli anni : dapprima utilizzata per la sola diagnosi di natura , solida o liquida , di una lesione ora ha assunto unimportanza fondamentale nella pratica diagnostica come guida , ad esempio , di procedure interventistiche come lago - aspirato , la biopsia con ago sottile e la localizzazione pre - bioptica di una lesione diagnosticata allesame mammografico [ 5 , 6 ]  . una grande variet di lesioni mammarie viene classificata con il termine di patologia duttale della mammella indicando con tale termine la patologia che interessa i dotti di maggior calibro . 
la maggior parte delle patologie duttali sono di tipo benigno e comprendono : lectasia duttale , il papilloma intraduttale singolo , i papillomi multipli , la papillomatosi del capezzolo e la papillomatosi giovanile [ 7 ]  . 
si manifesta nella maggior parte dei casi con secrezione sierosa o siero - ematica dal capezzolo , non una lesione precancerosa , ma tende a recidivare [ 9 ]  . 
i papillomi multipli , a carico dei dotti terminali e nei pazienti di giovane et , sono meno frequenti ma sono forme importanti perch possono degenerare nel 25% dei casi e sono considerati i precursori del carcinoma duttale in situ ( cdis ) [ 8 ]  . 
per ottenere la visualizzazione di tali patologie sono importanti le dimensioni del dotto e del processo produttivo intraduttale : spesso il papilloma non pu essere caratterizzato mediante il solo esame mammografico ed in caso di sospetto si rende necessaria la prosecuzione delle indagini con la galattografia e / o con lesecuzione dellecografia mammaria , anche in considerazione dellet della paziente [ 9 , 10 ]  . scopo del nostro lavoro valutare , in base ai dati preliminari ottenuti in 13 mesi di ricerca , il contributo diagnostico dellecografia mammaria nello studio di pazienti con sospetta patologia duttale della mammella calcolando i valori della sensibilit , specificit , il valore predittivo positivo ed il valore predittivo negativo . materiali e metodi sono state rivalutati tutti gli esami ecografici della mammella effettuati presso il policlinico umberto i di roma , universit la sapienza , dal gennaio 2005 al febbraio 2006 e sono state selezionate 52 pazienti di sesso femminile , di et compresa tra 28 e 74 anni ( et media di 45 anni ) che presentavano anamnesi sospetta per patologia duttale mammaria . 
all patients had undergone nipple discharge cytology , which was negative for the presence of cancer cells ( c2 ) in ten cases , and showed abnormalities suspicious for the presence of cellular atypia ( c3 ) or malignancy ( c4 ) in seven . 
 in group b ( patients without discharge ) , 23 / 35 patients presented with a palpable mass in the retroareolar region , associated with the typical signs of inflammation in two cases ; in 12 cases , prominent retroareolar ducts were present , associated with a retroareolar nodular opacity in one . breast us had been performed by radiologists with experience in breast us , with aloka prosound ssd - 5500 and siemens antares us scanners equipped with high - frequency linear - array transducers ( 7.510 , 1013 mhz ) for superficial tissues . 
radial and antiradial us scans were performed , with attention being paid to the entire ductal tree and following the lactiferous ducts from the retroareolar region towards the most peripheral branches , when visible . 
us allowed for differentiation between a normally appearing ductal tree in the retroareolar and peripheral regions and mammary - duct ectasia ( ducts larger than 2 mm in diameter )  . 
presenza di opacit nodulare nella regione retroareolare e / o di dotti retroareolari prominenti allesame mammografico [ 11 ]  . quarantacinque pazienti avevano effettuato preliminarmente lesame mammografico : in 12 la mammografia aveva riconosciuto unicamente aspetti riferibili ad una condizione di prominenza dei dotti retroareolari che in 7 casi era bilaterale e monolaterale in 5 ; in 13 erano presenti opacit nodulari retroareolari ed in 20 casi la mammografia risultava negativa . 
le 52 pazienti selezionate per il nostro studio sono state suddivise in due gruppi : il primo comprendeva 17 donne con secrezione ematica o sieroematica dal capezzolo ( gruppo a ) mentre laltro includeva 35 pazienti che non presentavano secrezione dal capezzolo ( gruppo b )  . nel gruppo a ( pazienti con secrezione dal capezzolo ) in 7 / 17 pazienti era stata effettuata la galattografia . 
le restanti 10 pazienti non avevano eseguito tale esame per i seguenti motivi : rifiuto in 5 pazienti , impossibilit nellincannulare il dotto in 4 e rottura del dotto incannulato in 1 paziente . tutte le pazienti avevano effettuato esame citologico della secrezione che mostrava in 10 casi reperto negativo per cellule tumorali ( c2 ) e in 7 alterazioni dubbie per la presenza di atipie cellulari ( c3 ) o sospette per malignit ( c4 )  . nel gruppo b ( pazienti senza secrezione ) in 23 / 35 pazienti era apprezzabile una tumefazione palpabile in sede retroareolare che in 2 casi si associava a segni caratteristici per la presenza di processo flogistico ; in 12 casi era presente prominenza dei dotti in sede retroareolare che in 1 caso si associava alla presenza di opacit nodulare in sede retroareolare . gli esami ecografici erano stati effettuati da operatori con specifica esperienza in diagnostica ecografica mammaria con ecografi aloka prosound ssd - 5500 e siemens antal . 
of patients us features definitive diagnostic categories negative mammary - duct ectasia benign nodules equivocal nodules negativi ectasie noduli benigni noduli dubbi tabella 2 classificazione ultrasonografica nelle categorie diagnostiche definitive n pazienti rilievi ecografici categorie diagnostiche definitive pattern ( either simple or pseudocystic ) or duct dilation associated with a solid nodular finding . 
on the basis of the relation between the nodule and the duct , nodules were distinguished into intraductal or periductal , and each nodule was assessed for margins ( welldefined and regular , or irregular and ill - defined ) , structure ( homogeneous or inhomogeneous ) , echogenicity ( hyperechoic , isoechoic or hypoechoic ) , posterior acoustic features ( posterior shadowing or enhancement ) and vascularity . 
after the scan , each patient was assigned a definitive diagnostic category in accordance , with the us classifications shown in table 2 [ 12 ]  . patients with normal ductal - tree findings on us ( negative finding : u1 ) or with benign lesions ( u2 ) , such as isolated duct ectasia or well - defined and regular nodules , were monitored by short - interval clinical and us follow - up ( at 3 , 6 and 12 months )  . 
patients with either equivocal findings ( u3 ) or findings suspicious for malignancy ( u4 ) underwent surgical biopsy : these included patients with ill - defined or irregular nodules and those with us evidence of a nodular mass , associated with abnormalities at discharge cytology that were either equivocal ( c3 ) or suspicious for malignancy ( c4 )  . 
the us diagnosis was later correlated with the histological findings in patients who had undergone surgical biopsy and with findings of the clinical and us follow - up in patients with conditions not considered suspicious for malignancy . 
the diagnostic accuracy , sensitivity , specificity , positive ( ppv ) and negative ( npv ) predictive values were calculated to establish the role of breast us in the diagnosis of ductal disease . results in group a ( 17 women with single - duct nipple discharge ) , galactography performed on seven patients showed a dilation res equipaggiati con trasduttori lineari ad alta frequenza ( 7 , 510 , 1013 mhz ) per i tessuti superficiali . 
sono state effettuate scansioni radiali ed antiradiali al capezzolo , prestando attenzione a tutto lalbero duttale seguendo i dotti galattofori a partire dalla regione retroareolare fino alle diramazioni pi periferiche , quando visibili . 
lesame ecografico ha permesso la distinzione tra la presenza di un regolare aspetto del disegno duttale in sede retroareolare e periferica e la presenza di ectasia duttale ( dotto di calibro superiore a 2 mm )  . 
in base al rapporto tra nodulo e dotto si sono distinti noduli intraduttali e periduttali e per ognuno sono stati definiti i margini ( netti e regolari o irregolari e sfumati ) , lecostruttura ( omogenea o disomogenea ) , lecogenicit ( iperecogena , isoecogena o ipoecogena ) , il comportamento posteriore del segnale acustico ( attenuazione acustica o rinforzo posteriore ) e la vascolarizzazione . 
al termine della scansione ecografica per ogni paziente stata scelta una categoria diagnostica conclusiva secondo le indicazioni della charta senologica , riportata in tabella 2 [ 12 ]  . le pazienti che allesame ecografico presentavano un regolare aspetto del disegno duttale ( reperto negativo : u1 ) o mostravano lesioni con caratteristiche di benignit ( u2 ) ad esempio una condizione di ectasia duttale isolata o unimmagine nodulare con margini netti e regolari sono state seguite con follow - up ravvicinati nel tempo ( 3 , 6 , 12 mesi ) , di tipo clinico ed ecografico . 
sono invece state sottoposte a biopsia chirurgica sia le donne in cui lesame ecografico era caratterizzato dalla presenza di reperti dubbi ( u3 ) o sospetti per malignit ( u4 ) : immagini nodulari con margini sfumati o l . 
breast us in this group of patients demonstrated a regular ductal tree pattern in three cases , mammary - duct ectasia of a portion of the ductal tree in nine cases and ductal dilation with nodules in five cases . 
at the time of writing , these patients had undergone clinical and sonographic follow - up at 3 - , 6and 12 - month intervals ( mean interval 6 months ) , with the following results : whereas the us pattern remained stable , the clinical findings had changed over time ( disappearance of nipple discharge in eight patients , reduced amount of discharge in two , and no significant change in symptoms in two )  . 
these patients underwent clinical and sonographic follow - up at 3 , 6 and 12 months , showing no substantial changes over time . in the remaining 25 patients , breast us identified 25 nodules , ten of which were isolated and 15 associated with mammary - duct ectasia : nineteen had well - defined regular margins ( 76% ) , and six had ill - defined or irregular margins irregolari , sia quelle in cui il reperto di una formazione nodulare messa in evidenza allesame ecografico si associava al risultato dellesame citologico della secrezione dal capezzolo caratterizzato da alterazioni dubbie ( c3 ) o sospette per malignit ( c4 )  . 
la diagnosi ottenuta con lesame ecografico stata successivamente confrontata con i risultati istologici , nelle pazienti sottoposte a biopsia chirurgica , e con i reperti riscontrati ai successivi follow - up clinico ed ecografico nelle pazienti con patologia considerata dagli operatori ecografici non sospetta per malignit . 
sono state calcolate laccuratezza diagnostica , la sensibilit , la specificit , il valore predittivo positivo ( vpp ) e negativo ( vpn ) dellecografia per definirne il ruolo nella diagnosi della patologia duttale mammaria . risultati nel primo gruppo di pazienti ( 17 donne con secrezione monorifiziale dal capezzolo ) , la galattografia eseguita in 7 pazienti dimostrava in 6 la dilatazione di una porzione dellalbero duttale a cui si associava in 2 pazienti un difetto di riempimento di un lume duttale , mentre in un caso non erano evidenti anomalie del dotto . 
lesame ecografico di questo gruppo di pazienti metteva in evidenza in 3 casi un regolare aspetto del disegno duttale , in 9 una condizione di ectasia duttale di una porzione dellalbero duttale ed in 5 pazienti la presenza di dilatazione duttale nel cui contesto si rilevavano noduli . 
1a , b a 48 - year - old woman with serosanguineous left - nipple discharge and cytological examination of the discharge negative for malignant cells ( c2 ) , without palpable lesions , underwent mammography and breast ultrasonography ( us )  . 
a mammogram shows a left fatty breast with a typical ductal pattern with prominent dilated ducts in the retroareolar region [ breast imaging reporting and data systems ( birads ) 2 ]  . 
1a , b una donna di 48 anni , con secrezione sieroematica dal capezzolo sinistro e citologia della secrezione negativa per cellule maligne ( c2 ) , senza lesioni palpabili , ha eseguito mammografia e successivamente valutazione ecografica . 
2a , b a 41 - year - old woman with serosanguineous left - nipple discharge and equivocal discharge cytology for the presence of some cellular atypia ( c3 ) , without palpable masses , underwent mammography and ultrasound ( us )  . 
a mammography shows heterogeneously dense breast tissue [ breast imaging reporting and data systems ( birads ) 3 ] , without mammographic evidence of malignancy ( birads final diagnostic category 2 )  . 
b us shows ductal ectasia in the left retroareolar region , with an associated image of a solid hypoechoic nodule , with ill - defined margins ( 9 mm ) inside a dilated mammary duct ( u3 )  . 
2a , b una donna di 41 anni con secrezione sieroemorragica dal capezzolo di sinistra e con citologia della secrezione dubbia per presenza di atipie cellulari ( c3 ) , senza lesioni palpabili ha eseguito la mammografia e successivamente la valutazione ecografica . 
a la mammografia evidenzia mammelle eterogeneamente dense ( bi - rads 3 ) , senza evidenza di presenza di malignit ( categoria diagnostica definitiva bi - rads 2 )  . 
b allecografia a sinistra , in sede retroareolare , si osserva la presenza di ectasia duttale con unimmagine nodulare solida ipoecogena ( 9 mm ) a margini sfumati nel contesto di un dotto mammario dilatato ( u3 )  . 
of the 19 well - defined nodules , 17 underwent sonographic and clinical follow - up at 3 , 6 , and 12 months , with no changes being recorded at follow - up us . 
questi casi sono stati seguiti esclusivamente mediante follow - up clinico ed ecografico a 3 , 6 , 12 mesi di distanza senza evidenza di sostanziali modifiche del quadro nel tempo . 
nelle restanti 25 pazienti lecografia ha identificato 25 noduli , di cui 10 isolati e 15 associati ad una condizione di ectasia duttale : 19 a margini netti e regolari ( 76% ) e 6 a margini sfumati o irregolari ( 24% )  . 
tutti i 19 casi con caratteristiche di benignit non hanno dimostrato modifiche dal punto di vista ecografico ai successivi follow - up a distanza di 3 , 6 , 12 menella tabella 3 viene riportato lo schema riassuntivo comprendente i reperti ecografici e liter clinico - strumentale a cui si sono sottoposte le 52 pazienti in esame . 
complessivamente lesame ecografico ha evidenziato in 14 casi la presenza di un aspetto regolare dei dotti ( in 10 casi con presenza di noduli e in 4 casi con assenza di alterazioni ecostrutturali associate ) e in 38 casi una condizione di ectasia duttale ( in 20 casi con presenza di noduli e in 18 casi con assenza di alterazioni ecostrutturali associate )  . 
3a , b a 32 - year - old woman complaining of a tender , palpable mass in the retroareolar region of the right breast , with typical signs of inflammation . 
us demonstrates in the right retroareolar region a periductal mass with irregular shape ( grossly oval ) , ill - defined margins and heterogeneous echostructure , in which some debris is visualised ( u3 )  . 
gli us dimostrano nella regione retroareolare destra una massa periduttale ( 12 mm ) con forma irregolare ( grossolanamente ovale ) , margini mal definiti ed ecostruttura disomogenea , nel cui contesto era riconoscibile materiale corpuscolato ( u3 )  . 
il quadro ecografico unitamente alla clinica erano indicativi per formazione ascessuale ; la paziente ha effettuato follow - up dopo adeguata terapia antinfiammatoria ed antibiotica . mensione media risultava di circa 7 mm ( 418 mm )  . 
complessivamente nella nostra casistica , sono state sottoposte a biopsia chirurgico 10 / 52 pazienti che allesame ecografico presentavano formazioni nodulari con caratteristiche morfologiche di sospetta malignit ( u4 )  . 
i risultati di tale procedura erano i seguenti : 5 papillomi singoli , 1 papilloma singolo con focolaio di cdis , 2 casi di papillomi multipli del capezzolo e 1 papillomatosi ; in una sola paziente lesame ha messo in evidenza la presenza di un fibroadenoma . 
le pazienti che allesame ecografico presentavano un regolare aspetto del disegno duttale ( reperto negativo : u1 ) o mostravano lesioni con caratteristiche di benignit ( u2 ) ad esempio una condizione di ectasia duttale isolata o unimmagine nodulare con margini netti e regolari sono state seguite con follow - up ravvicinati nel tempo ( 3 , 6 , 12 mesi ) , di tipo clinico ed ecografico . nella analisi statistica sono state considerate vere positive ( vp ) tutte le pazienti in cui lesame ecografico ha correttamente individuato la patologia mettendo tali reperti a confronto sia con i risultati dellesame istologico , a cui venivano sottoposte 10 pazienti , sia con i reperti del follow - up ecografico e clinico , nelle donne in cui la patologia individuata non presentava caratteristiche ecografiche sospette per malignit ( ad esempio lectasia duttale o la presenza di una formazione nodulare con margini netti e regolari )  . 
sono state definite invece vere negative ( vn ) le donne in cui lecografia non aveva messo in evidenza alcuna patologica ( assenza di anomalie duttali ) comparando tali reperti con i riscontri ecografici e clinici ottenuti nei successivi controlli a ogy ( fnac ) ; 5 / 6 cases necessitated further investigation by surgical biopsy due to cytology results that were equivocal ( cellular atypia ) or frankly suspicious for malignancy . 
none of the 19 cases of benign disease showed any change at 3 - , 6 - , and 12 - month follow - up us examinations . table 3 summarises the sonographic findings and clinicalimaging examinations performed on the 52 patients . 
overall , sonography demonstrated the presence of a normal ductaltree pattern in 14 cases ( in ten cases associated with nodules and in four cases without any associated structural changes ) and a condition of mammary - duct ectasia in 38 cases ( in 20 cases associated with nodules and in 18 cases without any associated structural changes )  . 
3a , b a 39 - year - old woman with sanguineous right - nipple discharge and equivocal discharge cytological for the presence of some cellular atypia ( c3 ) , without palpable masses , underwent mammography and ultrasonography ( us )  . 
a at mammography , the breast tissue is extremely dense [ breast imaging reporting and data systems ( birads ) 4 ] , and there is a need for additional imaging assessment ( birads final category 0 )  . 
b at us , a ductal ectasia is visible in the right retroareolar region , with some associated images of hypoechoic solid nodules with ill - defined margins ( 45 mm ) inside a dilated mammary duct ( u3 )  . 
4a , b una donna di 39 anni con secrezione emorragica dal capezzolo di destra e con citologia della secrezione dubbia per presenza di atipie cellulari ( c3 ) , senza lesioni palpabili ha effettuato mammografia ed ecografia . 
a la mammografia mostra mammelle a struttura estremamente densa ( bi - rads 4 ) , che necessitano di completamento diagnostico con altri esami strumentali ( categoria finale bi - rads 0 )  . 
b allecografia a destra , in sede retroareolare , si osserva la presenza di ectasia duttale con alcune immagini nodulari solide ipoecogene rispetto al parenchima mammario ( 45 mm ) a margini sfumati nel contesto di un dotto dilatato ( u3 )  . 
la successiva biopsia chirurgica ha confermato la presenza di papillomi multipli . neously hypoechoic in 15 cases , isoechoic in eight , inhomogeneously hypoechoic in five and homogeneously hyperechoic in two . 
overall , ten patients who had suspicious ( u4 ) nodular masses at sonography underwent surgical biopsy , with the following results : five solitary papillomas , one solitary papilloma with a dcis focus , two cases of multiple nipple papillomas and one papillomatosis ; fibroadenoma was diagnosed in one patient only . 
nel nostro studio sono stati riscontrati 46 vp e 3 vn ; in 1 solo caso , classificato come falso negativo ( fn ) , il reperto ecografico non mostrava immagini riferibili a patologia duttale sebbene il risultato dellesame citologico della secrezione dal capezzolo effettuato ad un controllo successivo a 12 mesi per la persistenza della sintomatologia mostrasse unalterazione dubbia per la presenza di atipie cellulari . 
in 2 casi ( falsi positivi , fp ) lecografia metteva in evidenza una formazione nodulare a margini sfumati che ai successivi approfondimenti , con prelievo con ago sottile in un caso e biopsia chirurgica nellaltro , risultavano essere due lesioni di natura benigna . 
lesame ecografico ha dimostrato una sensibilit del 97% , una specificit del 60% , un vpp del 95.8% , un vpn del 75% ed unaccuratezza diagnostica del 94% . discussione recentemente alcuni studi hanno sottolineato limportanza e lutilit dellimpiego dellecografia nello studio della patologia mammaria non solo come strumento in grado di definire la natura solida o liquida di una lesione ed eventuall . 
instead , we considered as true negatives ( tn ) all patients with a correct sonographic diagnosis of absence of pathological findings ( no ductal abnormalities ) confirmed by sonographic and clinical follow - up at 3 , 6 and 12 months . 
in one case only , classified as a false negative ( fn ) , sonography failed to demonstrate evidence of ductal disease , although nipple discharge cytology performed at 12 months due to persisting symptoms showed changes suggestive of cellular atypia . 
in two false positive ( fp ) cases , sonography demonstrated ill - defined nodular masses that proved to be benign at fnac in one case and at surgical biopsy in the other . 
sonography had 97% sensitivity , 60% specificity , 95.8% ppv , 75% npv and 94% diagnostic accuracy . discussion several studies recently emphasised the importance and usefulness of breast us in the study of breast diseases , not only mente di guidare la mano delloperatore nella esecuzione di manovre mini - invasive ( agoaspirati e agobiopsie ) , ma anche quale prima indagine di diagnostica strumentale nello studio del seno denso giovanile [ 3 , 4 , 8 , 13 ]  . in particolare alcuni autori hanno dimostrato la capacit dellecografia di poter effettuare la diagnosi della patologia duttale benigna e la diagnosi differenziale con la patologia maligna della mammella [ 1417 ]  . 
tra le condizioni patologiche benigne pi comuni sono comprese il papilloma mammario sia singolo ( spesso localizzato in sede retroareolare in contiguit con i dotti galattofori principali ) che multiplo ( a localizzazione pi periferica ad origine dai dotti lobari terminali ) e la papillomatosi giovanile , definita come singola entit patologica dal 1980 che si presenta nelle giovani donne in unet compresa tra i 23 ed i 32 anni [ 1822 ]  . 
 [ 7 ] riportano che il papilloma solitario si associ ad un incremento del rischio del 1 , 5%2% di sviluppare un carcinoma e ne consigliano lescissione chirurgica in tutti i casi diagnosticati , mentre cardenosa e eklund [ 23 ] dimostrano nel suo articolo che il papilloma solitario originantesi in sede centrale non debba l . 
in particular , some authors have demonstrated the ability of breast us to provide a diagnosis of benign ductal disease and differentiate it from breast malignancy [ 1417 ]  . 
among the most common benign diseases are solitary papilloma ( often retroareolar , close to the main lactiferous ducts ) , multiple papilloma ( more peripheral and originating from the terminal lobar ducts ) , and juvenile papillomatosis , described as a discrete entity in 1980 , which appears in young women 2332 years old [ 1822 ]  . 
 [ 7 ] reports that solitary papilloma is associated with a 1.5%2% increased risk of developing carcinoma , and surgical excision is suggested in all cases , whereas cardenosa and eklund [ 23 ] states that solitary papillomas originating from a central site should not be considered precancerous . the most common clinical manifestation of benign ductal diseases is the presence of serous or serosanguineous nipple discharge ( 64%88% of patients with papilloma )  . unilateral or bilateral nipple discharge may be associated with papilloma , an inflammatory process , or a breast carcinoma [ 20 , 24 ]  . 
one of the most important problems in diagnostic imaging is the poor sensitivity of mammography in the diagnosis of benign ductal disease ( mammography is negative in approximately 60% of cases )  . 
mammography may visualise well - circumscribed round masses prevalently near dilated ducts in the retroareolar region or else different forms of calcification ( round , eggshell , but also microcalcification clusters , which are difficult to differentiate from breast cancer ) ; however , correct mammographic visualisation is dependent on lesion size , which must be at least 1 cm in diameter [ 7 ]  . galactography is a valuable adjunct for the diagnosis of benign ductal disease , as it detects dilated and obstructed lactiferous ducts and / or of filling defects [ 2527 ]  . 
some galactographic findings are , however , nonspecific and do not permit differentiation between benign ductal disease and breast carcinoma , especially when areas of distortion or ill - defined ductal margins are depicted [ 7 , 28 ]  . 
other problems linked to the use of galactography include the management of young patients ( age < 35 years ) with nipple discharge , the inability or impossibility to cannulate a lactiferous duct or the patients refusal to undergo this test [ 28 ]  . in our experience , in six patients who were studied by breast us and galactography , there was concordance between the two techniques in the diagnosis of ductal disease , although us provided more detailed information on duct walls and the presence of nodular masses associated with duct dilation . 
furthermore , in the ten patients in whom galactography could not be performed , us provided a diagnosis of ductal disease that had been suspected on the basis of the clinical examination alone . in our study , in all cases confirmed by biopsy , us enabled the detection of ill - defined nodules with equivocal features , probably malignant or suspicious for malignancy , essere considerato come una lesione precancerosa . la manifestazione clinica pi frequente della patologia duttale benigna la presenza di secrezione sierosa o sieroematica dal capezzolo ( 64%88% delle pazienti con papilloma )  . 
la secrezione dal capezzolo , monoo bilaterale , pu per associarsi sia alla presenza di un papilloma sia ad un processo flogistico , sia ad un carcinoma mammario [ 20 , 24 ]  . una delle problematiche pi importanti nella diagnostica per immagini data dalla scarsa sensibilit dellesame mammografico alla diagnosi della patologia duttale benigna ( la mammografia risulta negativa in circa il 60% delle lesioni )  . 
alla mammografia si possono vedere delle masse circoscritte rotondeggianti prevalentemente in sede retroareolare in prossimit di dotti dilatati o la presenza di calcificazioni di varia morfologia ( rotondeggianti , ad uovo , ma anche come un cluster di microcalcificazioni , in questultimo caso di difficile diagnosi differenziale con il carcinoma mammario ) , ma per ottenerne la visualizzazione le lesioni devono raggiungere almeno un centimetro di diametro [ 7 ]  . lutilizzo della galattografia rappresenta un supporto nella diagnosi di tali lesioni tramite la visualizzazione di dotti galattofori dilatati ed ostruiti e / o di difetti di riempimento [ 2527 ]  . 
alcuni reperti galattografici sono per aspecifici , non permettendo di effettuare una diagnosi differenziale tra patologia duttale benigna e carcinoma mammario soprattutto nel caso in cui vengano individuate aree di distorsione o irregolarit dei margini di un dotto [ 7 , 28 ]  . 
altre problematiche allutilizzo della galattografia sono ad esempio il management di pazienti giovani ( et < 35 anni ) con secrezione dal capezzolo , lincapacit o limpossibilit nellincannulare un dotto galattoforo e il rifiuto della paziente a sottoporsi a tale esame [ 28 ]  . nella nostra esperienza in 6 casi sottoposti sia ad ecografia che a galattografia le due metodiche sono risultate concordi per la diagnosi di patologia duttale , ma lecografia ha in ogni caso fornito informazioni maggiori per quanto riguarda le pareti duttali e leventuale presenza di immagini nodulari associate al quadro di dilatazione dei dotti . 
inoltre nei 10 casi in cui non stato possibile effettuare la galattografia , lesame ecografico ha permesso di porre diagnosi di patologia duttale sospettata soltanto da rilievi clinici . nel nostro studio in tutti i casi che sono stati successivamente verificati con lesame bioptico lecografia ha permesso di riconoscere un nodulo a margini sfumati con caratteristiche dubbie , probabilmente maligne o sospette per malignit delle dimensioni medie di circa 7 min questi casi lecografia mediante lindividuazione della lesione ha permesso lesecuzione preventiva di un ago - aspirato e / o il reperage della lesione per la procedura bioptica . 
nei casi in cui le indagini si sono fermate allesame ecografico , lecografia stata importante per differenziare lectasia duttale associata alla presenza di noduli con caratteristiche di benignit dallectasia duttale semplice o pseudocistica , aspetti confermati poi nel successivo follow - up . 
in ogni caso pertanto lecografia stata in grado di evidenziare una patologia duttale che era stata sospettata clinicamente e / o mammograficamente ed ha permesso di differenziare la presenza di alterazioni che necessitano del solo follow - up da quelle che necessitano di exeresi chirurgica . 
in those cases studied by breast us only , the technique enabled the differentiation between mammary - duct ectasia associated with the presence of benign nodules and simple or pseudocystic - duct ectasia , findings that were later confirmed at follow - up . 
therefore , us proved constantly able to visualise ductal disease that had been suspected on clinical or mammographic examination and allowed us to distinguish between abnormalities requiring follow - up alone and those necessitating surgical excision . the main limitation of us was its inability to recognise ductal lesions as such where the duct was not ectatic and , more importantly , to relate nodules to the duct when these were in the most peripheral portion of the ductal tree . 
the limitations of our study lie both in the small number of patients ( n = 52 ) studied over a 13 - month period and in the limited number of cases ( ten patients ) in which the us findings could be correlated with the definitive histological diagnosis ; this was due to the impossibility of taking a biopsy in cases of clearly benign disease . 
all patients whose sonographic findings were considered not to be suspicious for malignancy and who therefore did not undergo biopsy were monitored by short - interval clinical and sonographic followup ( 3 , 6 and 12 months ) in order to minimise the risk of incorrect diagnoses provided by the first us examination . 
as regards the small number of patients enrolled , it should be noted that our work was based on preliminary data and that the final results will be presented and possibly published at a later date , as they are still being verified . however , despite the above - mentioned limitations , our study achieved an encouraging and statistically significant ppv ( 95.8% ) and npv ( 75% )  . 
the ppv indicated the percentage of cases in which us correctly identified the patients with ductal disease among those with positive sonographic findings and npv the number of patients not affected by ductal disease among those with negative us scans . 
in our study , breast us applied to the study of mammary - duct disease had 97% sensitivity and 60% specificity and a good level of diagnostic accuracy ( 94% )  . despite the limitations of this technique ( which is operator dependent and not panoramic ) , breast us performed on carefully selected women with suspected ductal disease proved to be a valuable and accurate diagnostic tool able to identify nodular lesions and / or mammary - duct ectasia , to differentiate intraductal and extraductal nodules , and to enable a diagnosis of solid lesions with benign features , requiring follow - up alone , and of nodules with equivocal or suspicious features , necessitating surgical biopsy . conclusions our preliminary data enabled us to consider high - frequency breast us as a particularly useful tool for the diagnosis of ductal disease , as it allows visualisation of dilated lactiferous ducts and of any nodules inside theif we consider that it is la metodica ecografica stato la capacit di riconoscere immagini nodulari di pertinenza duttale quando il dotto non risultava ectasico e soprattutto di riconoscere come di riferimento duttale formazioni nodulari situate nella porzione pi periferica dellalbero duttale . i limiti del nostro studio sono stati sia lutilizzo di un numero non elevato di pazienti ( n = 52 ) in un lasso di tempo di circa 13 mesi , sia lesiguit di casi ( 10 pazienti ) in cui si avuta una verifica tra i reperti ecografici ed i risultati istologici definitivi ; questultimo evento dovuto allimpossibilit di esecuzione di prelievo bioptico in condizioni patologiche di natura chiaramente benigna . 
a tal proposito tutte le pazienti i cui reperti ecografici venivano ritenuti dagli operatori non sospetti per patologia maligna , non sottoposte quindi a verifica bioptica , sono state comunque seguite con follow - up clinico ed ecografico ravvicinati nel tempo ( 3 , 6 , 12 mesi ) per minimizzare leventualit di essere incorsi in errore diagnostico con il primo esame ecografico . 
in merito allesiguit del numero delle pazienti prese in esame nel nostro lavoro , dobbiamo sottolineare che si tratta di uno studio che si basa su dati preliminari , i cui risultati definitivi verranno esposti ed eventualmente pubblicati in tempi successivi in quanto ad oggi ancora sottoposti a verifica . seppur , quindi , il nostro studio sia parzialmente limitato da le condizioni precedentemente elencate , abbiamo ottenuto comunque valori incoraggianti e statisticamente significativi , di vpp ( 95 , 8% ) e di vpn ( 75% ) che indicano nel primo caso in quale percentuale di casi la metodica ecografia ha correttamente individuato le pazienti realmente affette da patologia duttale tra le positive allecografia e nel secondo le pazienti realmente non affette tra quelle negative con la metodica stessa . 
lesame ecografico applicato alla studio della patologia duttale della mammella ha dimostrato nel nostro lavoro , una sensibilit e specificit rispettivamente del 97% e del 60% ed un buon valore dellaccuratezza diagnostica : 94% . pur con i limiti connessi alla metodica ecografica stessa ( operatore - dipendente e non panoramica ) lecografia eseguita in gruppi di donne strettamente selezionate per il sospetto di una patologia duttale si dimostrata un valido ed accurato strumento diagnostico : essa infatti in grado di individuare le lesioni nodulari e / o le ectasie duttali , di differenziare i noduli intraduttali da quelli extraduttali ed infine in grado di postulare un giudizio diagnostico sulle lesioni solide che presentano caratteristiche di benignit , per le quali corretto il follow - up e noduli che presentano caratteristiche diagnostiche dubbie o sospette per i quali necessario il ricorso alla biopsia chirurgica . conclusioni in base ai dati da noi preliminarmente ottenuti possibile quindi definire lecografia mammaria ad elevata frequenza uno strumento di elevata utilit nella diagnosi della patologia duttale in quanto permette la visualizzazione dei dotti galattofori dilatati e di immagini nodulariformi eventualmente presenti nel loro contesto . 
in these cases , breast us may prove very useful , not only as an adjunct to galactography , but also as a tool for classifying nodular lesions and detecting cases of mammary - duct ectasia when galactography cannot be performed . le , lecografia pu essere definita un esame strumentale complementare alla galattografia o una sua valida alternativa nei casi in cui questultima non risulti effettuabile . 
marini1 1dipartimento di scienze radiologiche , 2dipartimento di ostetricia e ginecologia , universit degli studi di roma la sapienza , via regina elena 324 , i - 00161 roma , italy correspondence to : a . 
halffourier single - shot turbo spin - echo ( haste ) , true fast imaging with steady precession ( fisp ) , t1 - weighted fast low angle shot ( flash ) two - dimensional ( 2d ) and diffusion - weighted ( dw ) sequences with apparent diffusion coefficient ( adc ) were obtained . 
abbiamo trovato una correlazione tra rapporto matrice germinale / diametro biparietale ( dbp ) ed et gestazionale e tra area germinativa e corticale quando espresse in rapporto al diametro intraoculare esterno ( dioe )  . 
la rm pu valutare in modo affidabile la maturazione encefalica nel periodo fetale . parole chiave risonanza magnetica sviluppo encefalico parametri biometrici girazione - solcazione mielinizzazione introduction introduzione central nervous system ( cns ) abnormalities are among the most common congenital malformations , but their early detection during pregnancy remains particularly challenging despite the considerable advances made in this field . 
alle anomalie di sviluppo del sistema nervoso centrale rappresentano le malformazioni congenite pi comuni la cui diagnosi precoce , nel corso della gravidanza , rimane particolarmente complessa nonostante i notevoli progressi coml . 
 the use of magnetic resonance imaging ( mri ) in the study of brain development disorders has shown that the technique offers new diagnostic possibilities in understanding the connections between aetiological factors and disorders of foetal brain maturation [ 2 ]  . 
furthermore , the development of fast sequences , in particular half - fourier singleshot turbo spin - echo ( haste ) sequences and steady - state free precession ( true fisp ) , with very short scan times , has revolutionised mri . 
a wide range of fast sequences is now available , including echoplanar sequences , t1and t2weighted fast gradient - echo ( fgre ) sequences and the more recent diffusion - weighted ( dw ) sequences [ 3 ]  . few studies have used mri to analyse foetal brain maturation patterns , but it has been reported that cortical gyration and sulcation reflect cerebral maturation [ 4 , 5 ] and that both are closely correlated with gestational age ( ga ) [ 6 , 7 ]  . 
in addition , mri can also provide a reliable evaluation of the orderly and predictable changes in cerebral parenchymal layering and myelination [ 8 ] that reflect the maturation process . 
 the aim of this prospective study was to establish the normal pattern of development and maturation of the foetal brain according to ga and offer an overview of the numerous possibilities of mri . materials and methods patient population and acquisition protocol the study protocol was approved by our institutions ethics committee . 
at the time of the examination , ga , as determined by a us scan within the 12th gestational week ( gw ) ranged from week 19 to week 37 ; more specifically , the distribution of foetuses according to ga was 35 second - trimester foetuses and 21 third - trimester foetuses ( table 1 )  . 
written informed consent was obtained from all patients . our study included patients referred to us for maternal complications during the pregnancy or for suspected foetal abnormalities detected on a previous us scan that had , however , demonstrated normal cns development . 
maternal complications ( 25 cases ) included uterine leiomyomas , suspected deep vein thrombosis , hydronephrosis , epilepsy , and placental abnormalities , whereas foetal abnormalities ( 31 cases ) included hydronephrosis , large bladder , abnormal amount of amniotic fluid and cardiac and pulmonary malformations . normal brain development was confirmed by foetal mri , postnatal neurological examination or postnatal autopsy ( after the legal limit of pregnancy or spontaneous abortion )  . the mri study was performed with a 1.5 - tesla ( t ) unit ( siemens vision , avanto ) , with the patient lying supine , or piuti in questo campo . 
sebbene lecografia sia la modalit dimaging prenatale utilizzata di routine , essa presenta dei limiti nellaccertamento particolareggiato dello sviluppo cerebrale che , come noto , correlato alla funzionalit cerebrale e alla prognosi neurologica [ 1 ] , come nel caso di anomalie della migrazione neuronale e malattie della sostanza bianca . lutilizzo della risonanza magnetica ( rm ) per lo studio dei disordini dello sviluppo encefalico ha dimostrato che questa metodica pu offrire nuove possibilit diagnostiche nella comprensione dei collegamenti esistenti tra fattori eziologici e disturbi della maturazione cerebrale fetale [ 2 ]  . inoltre lo sviluppo di sequenze rapide , in particolare delle sequenze half fourier single - shot fast spin - echo ( haste ) e steady state free procession ( truefisp ) , con tempi di scansione molto brevi , ha rivoluzionato radicalmente limaging in rm . 
ad oggi sono disponibili una vasta gamma di sequenze veloci , incluse le sequenze eco planari , fast gradienteco t1 e t2 pesate e le pi recenti sequenze pesate in diffusione [ 3 ]  . pochi autori hanno analizzato il pattern di maturazione cerebrale del feto mediante rm ; stato riportato che lo sviluppo dei giri corticali cerebrali e la formazione dei solchi riflettono la maturazione cerebrale [ 4 , 5 ] e che entrambi sono intimamente correlati allet gestazionale [ 6 , 7 ]  . 
inoltre con la rm possibile valutare in modo affidabile anche i cambiamenti nella stratificazione del parenchima cerebrale e nella mielinizzazione che procedono attraverso fasi ordinate e prevedibili [ 8 ] , corrispondenti al processo di maturazione . obiettivo di questo studio stato stabilire , in modo prospettivo , il normale pattern di sviluppo e di maturazione del cervello fetale in relazione allet gestazionale offrendo una panoramica sulle vaste possibilit di utilizzo della rm . materiali e metodi popolazione di pazienti e protocollo di acquisizione il protocollo di studio stato approvato dal comitato etico del nostro policlinico . 
al momento dellesame let gestazionale ( ega ) , determinata da uno studio ultrasonografico eseguito entro la 12a settimana di gestazione ( sg ) , variava tra la 19a e la 37a settimana ; in particolare la distribuzione dei feti in relazione allega era la seguente : 35 feti al secondo trimestre e 21 al terzo trimestre ( tabella 1 )  . 
da tutte le pazienti fu ottenuto il consenso informato in forma scritta . il nostro studio includeva pazienti rivoltesi alla nostra attenzione in seguito a complicazioni di origine materna insorte durante la gravidanza o a sospette anomalie fetali , individuate mediante precedente esame ecografico il quale dimostrava tuttavia un normale sviluppo del sistema nervoso centrale ; per quanto riguardo le anomalie materne ( 25 casi ) esse includevano leiomiomi uterini , sospetta trombosi venol . 
of foetuses gestational week 2nd trimester 3rd trimester 2 trimestre 3 trimestre tabella 1 distribuzione della popolazione in relazione allet gestazionale settimana di gestazione n casi in the left lateral decubitus if she was unable to tolerate the supine position ( for example , caval compression )  . 
la normalit dello sviluppo cerebrale fu confermata dalla rm fetale , da un esame neurologico negativo eseguito dopo la nascita o dallautopsia post - natale ( dopo il termine legale della gravidanza o aborto spontaneo )  . lo studio rm stato eseguito con un magnete da 1 , 5 t ( siemens vision , avanto ) , con la paziente in posizione supina o in decubito laterale sinistro nei casi in cui la madre non tollerava la posizione supina ( es : compressione cavale ) ; alle donne era permesso di rilassarsi allinterno del magnete per qualche istante prima dellesame per ridurre il movimento spontaneo fetale . 
stato utilizzato il seguente protocollo : sequenze t2 pesate half - fourier single shot fast se ( haste , te = 90 , flip angle = 150 , slice thickness = 4 mm , gap = 0 , 25 , fov = 360 mm , tempo di acquisizione = 27 s ) per lo studio delle strutture superficiali , quali giri e solchi ; sequenze true fisp breath hold ( tr / te = 4 , 8 / 2 , 3 , flip angle = 70 , slice thickness = 6 mm , gap = 0 , 30 , fov = 350 mm , tempo di acquisizione = 14 s ) con segnale intermedio t1 - t2 e poco sensibili agli artefatti di movimento ; sequenze fast gradient echo t1 pesate con e senza saturazione del segnale del grasso ( flash 2d : tr / te = 362 / 4 , 8 , slice thickness = 4 mm , gap = 0 , 20 , fov = 350 mm , tempo di acquisizione = 19 s ) , utilizzate per completare lo studio cerebrale ; sequenze flair usate per fornire informazioni addizionali sullencefalo fetale ( per esempio il diametro dei ventricoli laterali o della cisterna magna ) che creano un maggiore contrasto con le strutture adiacenti agli spazi liquorali ; le immagini furono acquisite secondo piani assiali , coronali e sagittali ortogonali allencefalo fetale ; sequenze single - shot eco - planari pesate in diffusione su un piano assiale parallelo alla linea bicommessurale ( tr / te : 3600 / 92 , slice thickness = 3 mm , gap = 0 , 30 , fov = 280 mm , matrice 128128 , tempo di acquisizione = 45 s ; con valori di b compresi tra 400 e 700 ms / mm2 ) con gradienti applicati secondo i tre assi ortogonali dello spazio ( x , y , z ) e successiva ricostruzione delle mappe di adc . 
we used a lower b value ( 700 ms / mm2 ) than normally used in adults because of the fast water diffusion rates in the foetal brain . overall examination time was 1520 min , in part owing to foetal movements that forced us to repeat the acquisition in some cases . 
 image analysis mris of all foetuses were analysed in consensus by two expert radiologists who evaluated the biometric parameters and the thickness of the developmental areas of the brain cortex ( germinal matrix , intermediate layer and cortical mantle )  . 
the study of cerebral biometry included measurement of the various structures : biparietal diameter ( bpd ) at the level of the temporal ventricular horns , frontooccipital diameter ( fod ) on the midsagittal scan , transverse cerebellar diameter ( tced ) on the axial images at the level of the posterior fossa , internal and external intraocular diameters ( iiod , eiod ) and lateral ventricular diameter ( lvd ) on the axial or coronal scans , and the cm on the sagittal scans . 
moreover , we calculated the ventricle to brain ratio ( lvd / bpd ) , measured the developmental areas of the cerebral cortex ( thickness of the germinal matrix and cortical mantle at the level of the lateral ventricles on the axial or coronal images ) , and assessed parenchymal layering in the periventricular area , gyrus and sulcus formation , and myelination . 
for the adc maps , regions of interests ( roi ) were manually placed on the frontal and occipital white matter and on the grey matter of the basal ganglia . 
lo studio della biometria cerebrale includeva la misurazione di diverse strutture : diametro biparietale ( dbp ) sulle scansioni coronali a livello dei corni temporali dei ventricoli , il diametro fronto - occipitale ( dfo ) sulla scansione sagittale mediana , il diametro cerebellare trasverso ( dtce ) sulle scansioni assiali a livello della fossa posteriore , i diametri oculari interni and esterni ( dioi , dioe ) e i diametri dei ventricoli laterali ( dvi ) sulle scansioni assiali o coronali e la cisterna magna ( cm ) su quelle sagittali . 
stato inoltre calcolato il rapporto ventricolo - cerebrale ( dvi / dbp ) , effettuata la misurazione delle aree di sviluppo della corteccia cerebrale ( spessore della matrice germinale e del mantello corticale sulle scansioni assiali o coronali a livello ventricoli laterali ) , valutate la stratificazione del parenchima in corrispondenza dellarea periventricolare , la girazione - solcazione e la mielinizzazione . 
per quanto riguarda le mappe di adc sono state posizionate manualmente delle regioni di interesse ( roi ) in corrispondenza della sostanza bianca frontale e occipitale , e della sostanza grigia dei gangli della base . 
tutte le misurazioni sono state messe in relazione allet gestazionale ; le misurazione delle aree di sviluppo sono state espresse sia come valore assoluto sia come rapporto rispetto ai parametri biometrici cerebrali . analisi statistica lanalisi statistica stata effettuata con la determinazione del coefficiente di correlazione di spearman . 
per valori al di sopra di questi non vi una correlazione significativa tra le variabili esaminate . risultati i dati relativi alle correlazioni tra i diversi parametri biometrici e lepoca gestazionale mostrata in tabella 2 : tutti i parametri biometrici misurati sulle immagini rm , eccetto per il diametro dei ventricoli laterali ( coefficiente di correlazione : 0 , 069 , p = 0 , 712 ) e della cisterna magna ( coefficiente di correlazione : 0 , 340 , p = 0 , 088 ) , correlavano con let gestazionale con un indice di correlazione r compreso tra 0 , 7 e 0 , 6 ( p < 0 , 05 ) per i differenti indici biometrici ; in particolare la correlazione con let gestazionale si dimostrata pi forte per il dioe e il dbp che mostravano anche la crescita pi costante durante la gestazione . il periodo in cui stato possibile riconoscere la stratificazione parenchimale riassunto nella tabella 3 : 1719 settimane , lencefalo presentava una superficie liscia ed era possibile differenziare due strati . 
dopo la 22a settimana , in tutti i feti erano riconoscibili tre strati che comprendevano la corteccia immatura , lo strato intermedio e la matrice germinale : nelle immagini t1 pesate la zona intermedia appariva ipointensa mentre la zona germinale e la corteccia mostravano alta intensit di segnale ; mentre nelle immagini pesate in t2 questi strati presentavano un comportamento opposto e nelle immagini pesate in diffusione la zona germinale e l . 
non era presente una correlazione tra the gestational periods during which parenchymal layering became detectable are summarised in table 3 : at weeks 1719 , the brain had a smooth surface , and two layers could be differentiated . 
inoltre , stata trovata una correlazione negativa tra rapporto matrice germinale / dbp ed et gestazionale , come pure tra dvi / dioe ed et gestazionale ( coefficiente di correlazione : 0 , 559 , p = 0 , 001 )  . nei nostri casi la mielinizzazione fu osservata a partire dalla 23a settimana di gestazione quando in corrispondenza del tegmento stato possibile identificare unarea di elevato segnale sulle immagini t1 - pesate ; tutti i feti dopo la 30a sg mostravano la presenza di mielina a livello del margine posteriore della capsula interna . 
early mri studies were limited by foetal motion artefacts due to the long scanning times , but the introduction of fast imaging sequences has enabled the accurate study of foetal brain maturation , with excellent tissue contrast resolution and without the need for foetal sedation . 
mri now offers several advantages with respect to us , such as multiplanar imaging independent of foetal head position and better contrast between the brain and the cerebrospinal fluid . as a consequence , mri plays several roles , including confirming equivocal us findings , detecting other abnormalities that may affect foetal outcome or delivery management and lutilizzo della rm come strumento complementare allecografia prenatale stato riportato per la prima volta in letteratura nel 1983 [ 16 ]  . 
inizialmente gli studi con risonanza sono stati limitati dagli artefatti da movimento dovuti al lungo tempo di scansione , ma lintroduzione di sequenze veloci ha permesso di studiare la maturazione fetale cerebrale in modo accurato con un eccellente risoluzione di contrasto tra i tessuti senza la necessit di sedazione fetale . 
lo sviluppo e la maturazione avvengono secondo una stadiazione prevedibile che sulle immagini rm caratterizzata dallo spessore della matrice germinale e corticale , dalla comparsa dello strato intermedio nella corteccia , dalla girazione , dalla solcazione e dalla mielinizzazione [ 9 ]  . molti degli studi sulla risonanza in epoca prenatale sono stati eseguiti per descrivere la maturazione cerebrale nei feti normali focalizzandosi sulla descrizione della comparsa della solcazione , girazione e mielinizzazione [ 7 , 10 , 11 ]  . 
nel nostro studio , in accordo con studi precedenti , abbiamo trovato che la stratificazione del parenchima cerebrale si correla con let gestazionale come pure lo sviluppo di solchi e scissure . 
prima della 17a sg , la risoluzione spaziale non ci ha permesso di identificare le cellule migranti , mentre tra la 17a e la 19a sg stato possibile differenziare lo strato intermedio dalla matrice germinale in meno del 25% dei feti . 
 [ 13 ] , che descrissero tre strati tra la 20a e la 26a sg . abbiamo voluto fornire inoltre punti di riferimento per i parametri cerebrali misurabili cos da poter essere utilizzati per stabilire la normalit della maturazione cerebrale ; la rm si dimostrata una metodica accurata nella valutazione di indici cerebrali , talora difficili da misurare mediante fig . 
la mappa di adc mostra le rois tracciate su unimmagine assiale a livello dei gangli basali , della sostanza bianca frontale e occipitale . supporting the planning of foetal surgery [ 17 ]  . 
 the aim of our study was to verify whether it was possible to establish parameters of normalcy during cerebral development and maturation to be used in the diagnosis and management of cases of suspected foetal brain abnormality . 
limmagine t2 haste sagittale mostra lo sviluppo della girazione e della solcazione . lesame ultrasonografico , come il dioi , il dioe , e il dvi , ed ha inoltre permesso la valutazione dello spessore della zona corticale e germinale . 
va rilevato che la valutazione dei diametri cranici risultata pi semplice e ben definita rispetto alla valutazione del parenchima cerebrale , resa pi difficile dagli effetti di volume parziale che possono essere prodotti dallutilizzo di strati di 4 o 6 mm di spessore ; ci rende , peraltro , pi complessa lidentificazione di sottili anomalie soprattutto a livello del mantello corticale . 
comunque , i nostri risultati dimostrano che lo spessore della matrice corticale correlato sia con let gestazionale sia con i parametri biometrici cerebrali , con una correlazione che maggiore nei feti al ii trimestre di gravidanza , indicando un progressivo aumento del mantello corticale mano a mano che aumenta il volume encefalico . 
al contrario , lo spessore della matrice germinale non correlava n con let gestazionale n con alcun parametro biometrico . al fine di comparare i diversi parametri ottenuti abbiamo normalizzato le aree misurate in rapporto a diversi parametri biometrici , identificando come pi costanti il dbp ed il dioe . 
le aree di sviluppo cerebrale germinativa e corticale non risultano correlate tra di loro quando considerate in termini di spessore assoluto , ma lo diventano positivamente quando vengono valutate in rapporto a parametri di crescita costanti come i suddetti dbp e dioe . tale dato indicherebbe che , in relazione alle variazioni di volume del cervello , le due aree mantengono un rapporto di crescita costante . 
tuttavia larea germinativa rispetto al volume del cervello ( espressa quindi come rapporto area germinativa / dbp ) tendeva a ridursi progressivamente con il progredire dellepoca gestazionale , in particolare questo rapporto decresceva a partire dalla 15a sg . dopo una fase di crescita esponenziale dellarea germinativa infatti si ha una fase di crescita costante , come dimostrato dallinversione del rapporto con larea corticale / dioe ( o dbp ) , e quindi una riduzione della crescita in termini di volume del cervello in relazione allepoca gestazionale . 
limmagine t2 haste sagittale mostra lo sviluppo della girazione e della solcazione . cortical matrix , the appearance of the cortical intermediate zone , gyration , sulcation and myelination [ 9 ]  . 
before week 17 ga , spatial resolution was insufficient for detecting migrating cells , whereas between weeks 17 and 19 the intermediate zone of the germinal matrix was distinguishable in fewer than 25% of foetuses . 
 [ 13 ] , who described the appearance of the three layers between weeks 20 and 26 ga . we also sought to provide reference values for measurable cerebral parameters that could be used to establish normal brain maturation . 
mri enabled accurate evaluation of cerebral indices that may be difficult to measure with us , such as iiod , eiod and lvd , and allowed assessment of thickness of the cortical and germinal zones . 
it should , however , be noted that it was easier to evaluate cranial diameters than cerebral parenchyma owing to the partial volume effects generated by the use of section thicknesses of 4 mm or 6 min addition , such thickenesses also make it more difficult to identify subtle abnormalities , especially at the level of the cortical mantle . 
the germinal and cortical areas are not correlated with each another when considered in terms of absolute thickness , whereas they are positively correlated when they are evaluated in relation to constant growth parameters , such as the bpd and eiod . 
however , when considered in relation to brain volume , the germinal area ( expressed as germinal area / bpd ratio ) tended to decrease progressively with increasing ga , in particular , from week 15 ga onwards . 
 in fact , after an initial exponential growth , the germinal area goes through a phase of constant growth , as demonstrated by the inversion of the ratio with the cortical area / eiod ( or bpd ) , followed by a phase of reduced growth in terms of brain volume relative to ga . 
a similar progressive reduction was found for the lateral ventricular diameter expressed in relation to eiod and ga : in other words , with increasing ga the ventricles have a lower growth rate with respect to the remaining cerebral parenchyma . 
the volume of the lateral ventricles increases gradually before reaching a peak at 23 weeks and gradually decreasing with ga , starting from week 15 ga with the exponential increase in the thickness of the cerebral mantle . 
 imaging aspects given the small size of the foetal brain , an accurate study requires the smallest possible fov to obtain good images of the region of interest ( roi ) , with foetal anatomy filling the fov , especially for foetuses smaller than 24 weeks ga ; in addition , the maternal body and possible overlap artefacts should also be considered . 
 to visualise and measure the landmarks of the normal foetal brain , we used t2 - weighted haste sequences , which are known to be excellent at all gas [ 25 , 26 ]  . 
in our study , the true fisp sequences proved to be essential for studying cerebral maturation in the third trimester , in particular for visualising cerebral parenchyma and myelination , thanks to fast scan times , high snr , and high t1 / t2 contrast . 
 for the study of myelination , t1 - weighted fgre sequences ( flash 2d ) with and without fat suppression can provide important additional information , as they yield highquality images above all when acquired during maternal la matrice germinale si riduce rispetto al volume cerebrale totale , come riportato da studi precedenti [ 14 , 15 ]  . 
in maniera simile abbiamo riscontrato una diminuzione progressiva del diametro intraventricolare espresso in relazione al dioe e lepoca gestazionale , ovvero con il progredire della gestazione i ventricoli crescono meno rispetto al restante parenchima cerebrale . 
il volume dei ventricoli laterali aumenta gradualmente e raggiunge il picco a 23a sg ; al contrario , il rapporto tra diametro dei ventricoli laterali e spessore corticale , a partire dalla 15a sg decresce gradualmente con lavanzare della gestazione dato laumento in modo esponenziale dello spessore del mantello cerebrale . aspetti radiologici uno studio accurato dellencefalo fetale , date le sue piccole dimensioni , necessita del pi piccolo fov possibile , in modo da ottenere delle buone immagini della regione dinteresse , con lanatomia fetale che riempie il fov , soprattutto per i feti pi piccoli della 24a sg ; inoltre va considerato anche il corpo materno che pu creare artefatti da sovrapposizione . per visualizzare e misurare i punti di riferimento dellencefalo fetale normale , abbiamo usato sequenze t2 haste pesate , eccellenti in tutte le et gestazionali [ 25 , 26 ]  . 
nel nostro studio le sequenze truefisp sono state essenziali per lo studio della maturazione cerebrale nel terzo trimestre , in modo particolare nella visualizzazione del parenchima cerebrale e nella mielinizzazione grazie alla rapidit della scansione , allalto rapporto segnale / rumore , allelevato contrasto t1 / t2 . 
queste sequenze suppliscono con un buon contrasto tissutale il fov relativamente pi grande che pu limitare la visualizzazione dei dettagli pi piccoli [ 27 , 28 ]  . per lo studio della mielinizzazione le sequenze fast gradient - echo t1 - pesate ( flash 2d ) con e senza saturazione del grasso possono aggiungere importanti informazioni fornendo immagini di elevata qualit soprattutto quando acquisite in breath - hold materno . 
le modificazioni biochimiche che avvengono durante la gravidanza si riflettono nelle variazioni di intensit di segnale : laumento in contenuto di colesterolo e glicolipidi che accompagna la maturazione della mielina e laumento in densit cellulare porta ad uniperintensit di segnale nelle immagini t1 pesate . 
the biochemical changes occurring during pregnancy are reflected in variations in signal intensity : the increase in cholesterol and glycolipid content that accompanies myelin maturation and increased cell density results in high signal intensity on t1 - weighted images . 
this problem is often avoided by using flash 2d sequences with fat suppression ; in fact , because the foetal brain has a high content of relatively free water , fat suppression heightens the contrast between free water and the tightly bound water of myelin , the cortex and the basal ganglia [ 29 , 30 ]  . 
recently , dw sequences proved useful for the study not only of some brain diseases but also of brain development , allowing investigators to establish adc values of the normal foetal brain that add information on normal brain development [ 1820 , 24 ]  . 
in addition , snr and spatial resolution are not as good as those obtained in postnatal imaging . the immature brain is characterised by a high water content and relatively fast molecular diffusion . 
because the nonmyelinated foetal brain has lower diffusion anisotropy than the myelinated adult brain , during the second trimester , it is essential to generate isotropic diffusion images rather than to apply the diffusion gradient in a single direction . on dw images , the foetal brain is characterised by a low signal intensity in the subcortical white matter and a higher signal intensity in the cortex and deep grey matter . 
the mean adc value for white matter is higher than that of grey matter of the basal ganglia , as demonstrated by our study , because the basal ganglia are composed of densely packed cells compared with the nonmyelinated white matter , which contains larger amounts of interstitial water . 
as the brain matures , the adc values of the white matter decrease gradually as a result of myelin maturation ( hydrophobic ) and increase in relative anisotropy , as intracellular water tends to move along the length of the axon . 
this cerebral maturation is associated with an increase in the anisotropy index of white matter , which is appreciable during the so - called premyelinating state [ 21 , 23 ]  . 
anisotropy increases steadily between premyelination and postmyelination phases , making it possible to observe white matter maturation a few weeks before any change in signal intensity becomes evident in the t1 - t2 sequences . 
one of the main limitations of this study was the lack of data on the relative anisotropy of white matter during this period . conclusions foetal mri may provide a useful diagnostic tool for assessment of cns diseases in utero , not only because of its greater diagnostic capabilities in detecting structural malformations of the cerebral parenchyma or ventricles , but also for its ability to assess the steps in the development and matlelevata densit cellulare e quella microvascolare sono fattori importanti per limaging pesato in diffusione ( dwi ) utile nel nostro studio per visualizzare la maturazione della sostanza grigia e bianca . 
recentemente le sequenze dw si sono dimostrate importanti non solo in alcune malattie cerebrali ma anche per lo sviluppo dellencefalo , consentendo di stabilire anche i normali valori di adc del cervello fetale che aggiungono informazioni sul normale sviluppo cerebrale [ 1820 , 24 ]  . 
questo tipo di studio pi difficile di quello post - natale a causa della degradazione di qualit dellimmagine per artefatti da movimento materno - fetali e gli effetti di pulsatilit dellaorta . 
inoltre il rapporto segnale - rumore e la risoluzione spaziale sono peggiori di quelli ottenuti con limaging post - natale . lencefalo immaturo caratterizzato da un alto contenuto di acqua e da una diffusione molecolare relativamente rapida . 
dato che lencefalo fetale non mielinizzato ha una minore anisotropia di quello mielinizzato delladulto , durante il 2 trimestre essenziale generare immagini in diffusione isotropiche piuttosto che applicare il gradiente di diffusione in una sola direzione . nelle immagini dw lencefalo fetale caratterizzato da una bassa intensit di segnale a livello della sostanza bianca sottocorticale e da una maggiore intensit di segnale allinterno della corteccia e della sostanza grigia profonda ; mentre il valore medio di adc per la sostanza bianca pi alto rispetto a quello della sostanza grigia dei gangli basali , come dimostrato nel nostro studio , poich questi ultimi sono costituiti da cellule densamente impacchettate rispetto alla sostanza bianca non mielinizzata , che contiene una maggiore quantit di acqua nellinterstizio . 
con la maturazione encefalica si assiste ad un graduale declino nei valori di adc della sostanza bianca , che pu essere spiegato con la maturazione della mielina che idrofobica , e con un aumento dellanisotropia relativa poich la direzione del movimento dellacqua intracellulare preferenzialmente lungo la lunghezza dellassone . 
questa anisotropia cresce costantemente dalla fase premielinizzante a quella mielinizzante , cosicch stato possibile osservare la maturazione della sostanza bianca qualche settimana prima che i cambiamenti di segnale risultassero evidenti anche nelle sequenze t1 - t2 . uno dei limiti principali di questo studio stata proprio la mancanza di dati riguardo lanisotropia relativa della sostanza bianca in questo periodo . conclusioni la rm fetale pu rappresentare un importante supporto diagnostico clinico nella valutazione delle patologie del snc in utero , non solo per la maggiore capacit diagnostica nelle malformazioni strutturali del parenchima o dei ventricoli cerebrali , ma anche per la possibilit di valutare le tappe di sviluppo e maturazione del cervello fetale . 
further studies on larger population samples are needed to validate our findings and identify more reliable reference curves . developments in mri technology , including dw imaging , will further expand the role of foetal mri , making it an indispensable tool in prenatal medicine . verse epoche di gravidanza ha portato alla identificazione di alcuni parametri che appaiono idonei come indici di adeguato sviluppo e maturazione cerebrale . 
fifty - seven patients showing an occlusive or aneurysmal disease of the abdominal aorta and iliac arteries underwent intraarterial digital subtraction angiography ( dsa ) equipped with the ra function and a 3d workstation . 
we found that 3dra is able to generate images of the examined vessels with a very effective 3d appearance ; furthermore , it is able to create images of the lumen and wall of the vessel through two different modalities : endoviews and cross sections . 
different aspects of the arteries can be demonstrated in the angioscopic elaborations : the normal and stenotic lumen , artery bifurcations , the collateral vessel origins and the severity and extensions of atheromatous calcifications and their relationships to the vessel wall . 
we present a summary of the different radiological findings that can be demonstrated with this new imaging technique . key words rotational angiography three - dimensional angiography virtual reality iliac arteries riassunto obiettivo . 
cinquantasette pazienti portatori di patologia steno - ostruttiva o aneurismatica del distretto arterioso aortoiliaco sono stati sottoposti ad angiografia digitale con apparecchiatura in grado di effettuare acquisizioni rotazionali e con consolle di elaborazione tridimensionale di tali acquisizioni . 
langiografia rotazionale tridimensionale capace di generare immagini dei vasi indagati con un reale effetto tridimensionale ; inoltre in grado di creare immagini del lume e della parete vasale con due diverse modalit : angioscopia virtuale e sezioni ortogonali . 
in questo lavoro viene presentata una rassegna di diversi reperti radiologici che vengono forniti da questa nuova modalit di imaging . parole chiave angiografia rotazionale angiografia tridimensionale realt virtuale arterie iliache f . 
msct and mra are able to display arteries in different ways and , in addition to the axial plane , they are able to visualise arteries with multiplanar reformations ( mpr ) , maximum intensity projections ( mip ) , shaded surface displays ( ssd ) and volume rendering ( vr ) mode . 
furthermore , one of the most effective ways to visualise arteries is by means of virtual angioscopy , a technique that is quite easily achievable with modern workstations connected to the msct or mra unit . 
 however , in recent years , digital subtraction angiography ( dsa ) has also increased its ability to depict arteries , an improvement made possible by the introduction in clinical practice of rotational angiography ( ra ) and of its natural development three - dimensional rotational angiography ( 3dra )  . 
this new method is based on the three - dimensional ( 3d ) representation of vessel structures obtained from a single intraarterial injection of contrast mediuthe acquisition is performed using a motorised angiography c arm around the structure under examination . 
this technique was originally created to investigate intracranial vessels [ 69 ] , but increasing numbers of studies have also reported its use at the extracranial level [ 1017 ]  . 
the 3d images obtained in this way can be displayed with typical 3d viewing modes , such as vr , volume colour rendering ( vcr ) , shaded surface display ( ssd ) , gradient rendering ( gr ) , maximum intensity projection ( mip ) and ray sualso , 3dra is able to generate 3d views of the lumen wall of the investigated vessels from the inside with an effective virtual angioscopic appearance [ 18 ]  . another advantage is the possibility of matching the 3d ssd reconstruction of the calcified structures present at the same level using the data obtained from the rotational acquisition performed before contrast medium injection . 
 the purpose of this paper is to present some of the more negli ultimi anni si assistito ad una significativa evoluzione nella valutazione delle arteriopatie periferiche grazie ai sensibili miglioramenti di alcune modalit diagnostiche quali leco color doppler , la tomografia computerizzata multistrato ( tcms ) e langiografia mediante risonanza magnetica ( angio - rm ) che hanno il significativo vantaggio di fornire informazioni simili allangiografia convenzionale ma con inferiori rischi per il paziente . 
la tcms e langio - rm sono in grado di dimostrare le arterie con differenti modalit e oltre al piano assiale esse forniscono rielaborazioni bidimensionali multiplanari , o tridimensionali quali le elaborazioni mip ( maximum intensity projection ) , ssd ( shaded surface display ) o vr ( volume rendering )  . 
inoltre una delle modalit di visualizzazione delle arterie pi efficace la possibilit di generare immagini di angioscopia virtuale e questo ottenibile piuttosto facilmente con le moderne workstation collegate alle tcms ma anche alle apparecchiature di risonanza magnetica . 
con questa tecnica possibile creare immagini del lume interno dei vasi e navigare lungo il vaso utilizzando il set di dati ottenuto dalle acquisizioni della tcms e della risonanza magnetica [ 15 ]  . 
 [ 3 ] langioscopia virtuale fornisce una dettagliata rappresentazione del lume e consente di comprendere leffetto della malattia su di esso . tuttavia in questi ultimi anni anche langiografia digitale stata in grado di aumentare la sua capacit di rappresentazione delle arterie e questo grazie allintroduzione nella pratica clinica dellangiografia rotazionale e della sua naturale evoluzione , langiografia rotazionale tridimensionale ( ar3d )  . 
questo nuovo metodo si basa su una rappresentazione tridimensionale ( 3d ) della struttura vasale ottenuta da una singola iniezione intra - arteriosa di mezzo di contrasto . lacquisizione viene assunta utilizzando un arco a c motorizzato che ruota intorno alla struttura da esaminare . 
le immagini 3d cos ottenute possono essere visualizzate con le tipiche modalit di rappresentazione tridimensionale : volume rendering , shaded surface display ( ssd ) , gradient rendering ( gr ) , maximum intensity projection , sum , ecc . 
un altro vantaggio la possibilit di sovrapporre allelaborazione tridimensionale dei vasi ( in ssd ) lelaborazione 3d delle strutture calcifiche presenti allo stesso livello utilizzando i dati dellacquisizione rotazionale eseguita prima delliniezione del mezzo di contrasto . 
the procedures were performed in all cases on an in - patient basis after obtaining the appropriate informed consent . the examinations were performed with an angiographic and interventional system ( philips integris allura , philips medical systems , eindhoven , the netherlands ) , equipped with the ra option and connected to a workstation capable of displaying 3d reconstructions ( dell computer , round rock , tx , usa )  . 
in all cases , the examinations were performed using nonionic contrast material at a concentration of 350 mgi / ml ( iomeron , bracco , milan , italy )  . 
the standard procedure involved the placement of a straight or pigtail high - flow catheter with an arterial retrograde common femoral or brachial approach at the level of the abdominal suprarenal aorta in the case of investigation of an abdominal aortic aneurysm , and in the subrenal aorta in the case of evaluation of lesion to the iliac artery . 
the amount and flow - rate of contrast material for ra were 6472 ml at 89 ml / s based on a subjective evaluation of vessel size at preliminary angiography . 
in the case of investigations of vessels under the diaphragm , the rotational angioacquisition was done using the roll scan programme with the c arm placed lateral to the patient . 
the fundamental requirement for a correct clinical result is to place the vessel to be investigated at the isocenter of the systetwo ras are performed : a mask run to evaluate calcification and a contrast run made with the injection parameters mentioned above . 
 in un unica immagine , il lume vasale , la placca calcifica , ma possiamo anche visualizzare stent o altri dispositivi . scopo di questo lavoro di illustrare gli aspetti endovasali normali e patologici pi interessanti che si possono osservare con questa nuova modalit nella valutazione del distretto aorto - iliaco . materiali e metodi nel periodo compreso tra gennaio 2003 e dicembre 2005 , 57 pazienti ( 40 m , 17 f ; et : 4987 et media 70 , 8 ) sono stati sottoposti ad angiografia digitale del distretto arterioso aorto - iliaco per una lesione stenotica o aneurismatica precedentemente riconosciuta alla valutazione clinica o alleco color doppler , tc e / o rm . 
complessivamente sono stati eseguiti 46 esami del distretto iliaco e 11 esami dellaorta addominale mediante angiografia rotazionale del tratto sede di patologia e successive elaborazioni 3d . le procedure sono state portate a termine in tutti i casi in regime di ricovero ospedaliero , dopo aver ottenuto il consenso informato . 
stato utilizzato un sistema per angiografia e radiologia interventistica philips integris allura ( philips medical systems , best , olanda ) , equipaggiato con lopzione per lesecuzione delle acquisizioni rotazionali , connesso a una workstation in grado di fornire elaborazioni 3d ( dell computer corp , round rock , usa )  . 
la procedura standard si basa sullutilizzo di un approccio arterioso femorale retrogrado o un approccio brachiale e il posizionamento di un catetere ad elevato flusso diritto o pig - tail con estremit distale a livello di aorta soprarenale in caso di valutazione di un aneurisma aortico sottorenale e con estremit distale infrarenale in caso di studio di una lesione stenosante del distretto iliaco . 
il quantitativo totale di mdc e il flusso per lacquisizione rotazionale variano rispettivamente tra 64 e 72 ml a 89 ml / s in base ad una valutazione soggettiva delle dimensioni dei vasi alla preliminare angiografia . 
quindi si eseguono due acquisizioni rotazionali : una con funzione di maschera che risulta utile per la valutazione delle calcificazioni e unacquisizione durante liniezione del mdc con i parametri di iniezione sopraricordati . i due set di immagini bidimensionali sono quindi trasferiti alla workstation 3d . 
 the calcification detection data set is based on a rotational scan during which low kilovolt ( kv ) numbers are used to decrease the x - ray penetration rate and increase calcification visualisation . 
if any additional geometrical assessment is desired , a subreconstruction is made and the measurement tool is used to perform the measurements of , for example , plaque thickness or remaining lumen diameter . 
angioscopic evaluations can be obtained in two ways : ( 1 ) by using the automatic vessel analysis tool or ( 2 ) by using the cut - plane technique . 
 automatic vessel analysis tool this is a postprocessing function available on the workstation , which enables the operator to obtain different types of data of the examined vessel : evaluation of the diameter and area of the vessel and the degree of stenosis with graphic representation virtual stenting : 3d visualisation of a stent / stent - graft in the site of the stenosis and of how it fits to the vessel [ 15 ] endoview : 3d visualisation of the inside lumen of the vessel . 
tali correzioni sono necessarie a causa della morfologia curva dellintensificatore di immagini e dellinfluenza del campo magnetico ambientale . la correzione delle geometrie viene utilizzata per migliorare tutte le imperfezioni presenti nella acquisizione rotazionale causate da una traiettoria circolare non ideale . 
il risultato finale dellelaborazione da considerarsi privo di distorsioni . le elaborazioni 3d possono essere rappresentate con quattro differenti modalit di visualizzazione : mip , gr , ssd e vr e queste ultime due vengono utilizzate come standard . oltre alla rappresentazione 3d delle arterie , questa workstation in grado di eseguire accurate misure dei diametri vasali e ottenere rappresentazioni endoluminali virtuali dei vasi in esame . 
questultima fornisce una visualizzazione della parete interna vasale che viene utilizzata per la valutazione virtuale del lume vasale . vi sono inoltre degli ulteriori programmi che consentono la sovrapposizione tridimensionale delle due acquisizioni ( senza e con mdc ) e che utilizzano un programma che compensa gli artefatti da movimento . 
ovviamente essa in grado di dimostrare altrettanto efficacemente dispositivi endovascolari sufficientemente radiopachi . il riconoscimento delle calcificazioni si basa sullutilizzo in corso di acquisizione rotazionale di bassi valori di voltaggio con lo scopo di ridurre la penetrazione dei raggi x e di incrementare pertanto la visualizzazione delle calcificazioni . durante lacquisizione rotazionale iniziale , le calcificazioni non sono riconoscibili ad una valutazione effettuata a occhio nudo . 
b ar3d : shaded surface display ( ssd ) dellasse iliaco : lanalisi vasale automatica definisce il tratto da analizzare ( linea blu ) e il segmento giallo definisce il punto di maggior stenosi . 
with this renti tipi di informazioni sul vaso esaminato : valutazione del diametro e dellarea del vaso , il grado di stenosi con la corrispettiva rappresentazione grafica ; stenting virtuale : la visualizzazione 3d dello stent / endopprotesi nel sito della stenosi ed il suo adattamento al vaso [ 15 ] ; endoview : la visualizzazione 3d del lume del vaso . 
una volta che abbiamo deciso dove cominciare e finire la nostra indagine nel vaso patologico , con un semplice click del mouse posizioniamo i due anelli che delimitano linizio e la fine della valutazione e lo f . 
a ar3d con contemporanea visualizzazione delle strutture ossee in un caso di aneurisma bilaterale delle arterie iliache b un piano di taglio pu essere visualizzato e modificato nel suo orientamento : tutte le parti dal lato del piano rosso possono essere rimosse . 
b il colore dellarteria non si modifica a livello della stenosi . modality , by simply moving the mouse , a line is deployed and part of the artery can be easily removed . results analysis of 3d virtual angioscopy from 3dra enables different aspects of the investigated vessels to be visualised . the internal normal lumen wall of the artery is shown in virtual angioscopy with a pink colour in contrast to the red colour of the external lumen wall . 
con questa modalit , semplicemente muovendo il mouse si traccia una linea e parte dellarteria pu essere facilmente rimossa . langioscopia virtuale tridimensionale con ar3d offre la possibilit di visualizzare differenti aspetti dei vasi studiati . lume normale e lume stenotico . 
in questo tipo di valutazione la modalit sezione ortogonale risultata particolarmente efficace . stent e dispositivi vari abbiamo studiato pazienti nei quali erano presenti stent in arteria iliaca o endoprotesi a livello addominale . 
usando la modalit visualizzazione placche calcifiche questi devices sono stati correttamente visualizzati ed in particolare le calcified plaques in the iliac arteries were observed in 32 / 46 of the examined iliac cases . 
d la sezione ortogonale dimostra placche calcifiche ( strutture bianche ) che circondano il lume ( linea rossa ) e sezione ortogonale : placche calcifiche esterne al lume vasale . quantify lesions in aortoiliac arteries with high sensitivity and specificity and are less invasive with fewer risks [ 13 ]  . nevertheless , once the diagnosis has been made , a high percentage of patients may be treated endovascularly , and this must be done in an angiography suite . 
recent papers have demonstrated the possible contribution of 3dra in the evaldiscussione langiografia ha ridotto il proprio ruolo nella diagnosi delle malattie delle arterie periferiche come a livello delle arterie carotidi , dellaorta addominale , delle iliache e delle arterie infrainguinali poich la moderna diagnostica per imf . 
8a , b aortic stent - graa three - dimensional rotational angiography ( 3dra ) in a case of bifurcated aortic stent - graft ( excluder - gore )  . 
a 3dra with calciview : the small white points ( arrows ) at the origin and in the distal portion of the right common iliac artery represent the radiopaque markers of a nitinol stent ( luminexx - bard )  . 
a ar3d con visualizzazione delle placche calcifiche : i piccoli punti bianchi ( frecce ) allorigine ed al tratto distale dellarteria iliaca comune destra rappresentano i markers radiopachi dello stent in nitinol ( luminexx - bard )  . 
c catetere centimetrato in aorta addominale ectasica . magini utilizza modalit come eco color doppler , tc multistrato e angio - rm che sono capaci di rilevare e quantificare lesioni delle arterie aorto - iliache con unalta sensibilit e specificit e invasivit inferiore con minori rischi per i pazienti [ 13 ]  . 
ci nonostante , una volta fatta la diagnosi , in unalta percentuale dei casi , i pazienti possono essere trattati per via endovascolare e questo viene fatto in sala angiografica . 
a the preliminary angiogram shows a suboptimal opacification of the iliac arteries and a high degree of noise due to an unusual amount of bowel gas ( patient with previous total laryngectomy )  . 
d in the lower part of the figure , the catheter is visible with some artefacts mainly due to catheter movement during the rotational acquisition ( yellow arrow )  . 
a il preliminare angiogramma dimostra unopacizzazione sub - ottimale dellarteria iliaca ed un certo grado di rumore a causa di una inusuale quantit di aria nellintestino ( paziente operato di laringectomia totale ) b anche la rielaborazione 3d e langioscopia virtuale dimostrano un superiore livello di rumore sulla parete vasale . 
distalmente il catetere non pu essere separato dalle placche calciche ( freccia blu )  . uation of intracranial and extracranial arteries [ 618 ] , together with the usefulness of the technique in planning some types of endovascular treatment such as stent deployment [ 1315 ]  . 
in this study , we have analysed the contribution of virtual angioscopic reconstructions starting from 3dra and have shown that the quality of these images is satisfactory in a high percentage of ed extracraniche [ 617 ] e il contributo di questa tecnica nella programmazione di alcuni tipi di trattamenti endovascolari cosi come nel posizionamento degli stent [ 1315 ]  . langioscopia virtuale una nuova modalit di imaging dei vasi arteriosi e al momento poche pubblicazioni hanno focalizzato lattenzione su di essa e molti lavori fanno riferimento ad angioscopie virtuali eseguite con tc multistrato o con angio - rm . 
 zionale e riteniamo di aver dimostrato che la qualit delle immagini soddisfacente in unalta percentuale dei casi e che questa tecnica sia in grado di fornire ulteriori informazioni . conclusions we believe that the role of angioscopic imaging of arteries still needs to be defined , but in selected cases , the use of these images increases the confidence with which endovascular interventions are carried out . 
some limitations must , however , be taken in account when virtual angioscopy is done with 3dra : slightly longer examination time due to the operative protocol of rotational angiography inadequate results in cases of significantly aneurysmal arteries where the contrast medium opacification tends to be insufficient and the flow too slow to correctly opacify all the arteries of interest . 
 other limitations of virtual angioscopy images performed using all the techniques are the inability to correctly depict stenoses due to soft plaques because currently , only hyperdense plaque components are reconstructed in 3d elaborations . 
 conclusioni in conclusione noi riteniamo che , anche se il ruolo dellimaging angioscopico delle arterie deve essere ancora definito , in casi selezionati questo tipo di immagini aumenta la confidenza con cui gli interventi endovascolari sono eseguiti . 
crusco , via antica vena 18 , i - 06100 perugia , italy , tel . : + 39 - 075 - 393044 , fax : + 39 - 075 - 5783507 , e - mail : fcrusco@sirm.org received : 20 may 2006 / accepted : 12 september 2006 / published online : 20 april 2007 abstract purpose . 
conventional digital subtraction angiography ( dsa ) still represents the criterion standard for the diagnosis of vertebral artery dissection ( vad ) , but the main drawbacks of this technique include invasiveness , patient discomfort and risk of complications . we evaluated the potential of multidetector computed tomography angiography ( cta ) as a noninvasive tool providing highresolution images of the arterial lumen and wall by comparing the diagnostic accuracy of cta and colour - doppler ultrasonography ( cdus ) in detecting acute vad . 
we retrospectively reviewed 15 cases of vad in 15 patients ( five men and ten women , age range 2858 years ) who came to our attention between august 2001 and september 2005 . 
the diagnosis was made on the basis of appropriate clinical presentation , absence of atherosclerotic disease in the cerebrovascular circulation and evidence of distinctive ct features , which were subsequently confirmed by conventional angiography used as reference standard . 
the cdus examinations revealed ten out of 15 vad , with a sensitivity of 66% , a specificity of 60% , a positive predictive value of 55.5% and a negative predictive value of 70.5%. 
in five cases , cdus revealed nonspecific wall and flow alterations ; in eight patients , high resistance obstructive flow ; and in two patients , intimal flap with demonstration of the true and false lumen . 
the differences in cta and cdus sensitivity ( 100% vs 66% ) , specificity ( 95% vs 60% ) , and overall diagnostic accuracy ( 97% vs 62.8% ) , assessed by cross tabulations and compared by using the mcnemars riassunto obiettivo . 
langiografia con sottrazione dimmagine ( dsa ) rappresenta la metodica di riferimento nella diagnosi di dissezione acuta dellarteria vertebrale ( vad ) , tuttavia i principali limiti di questa tecnica comprendono linvasivit , il disagio per il paziente e il rischio di complicanze . 
abbiamo revisionato retrospettivamente 15 vad in 15 pazienti ( 5 uomini e 10 donne , et compresa tra 2858 anni ) , giunti alla nostra osservazione nel periodo agosto 2001settembre 2005 . 
la diagnosi stata posta in base ad una sintomatologia clinica appropriata , in base allesclusione di una malattia aterosclerotica del circolo cerebrovascolare e in base alla presenza di alcuni segni tomodensitometrici specifici , successivamente confermati con dsa , considerata come metodica gold standard . 
lecd risultata diagnostica in 10 / 15 vad angiograficamente dimostrate con risultante sensibilit del 66% , specificit del 60% , valore predittivo positivo del 55 , 5% e valore predittivo negativo del 70 , 5% . 
in 5 casi , con esame ecd , si sono evidenziate alterazioni parietali e flussimetriche non specifiche , in 8 pazienti flusso ostruttivo ad alta resistenza e in 2 pazienti stato possibile visualizzare un flap intimale con rilievo dei lumi vero e falso . 
la cta si dimostrata diagnostica in tutti i 15 casi di vad , con risultante sensibilit , specificit , valore predittivo positivo e valore predittivo negativo rispettivamente del 100% , 95% , 93 , 7% f . 
used as a complement to unenhanced brain ct , it has the advantage of being readily available and easy to perform . key words multidetector ct doppler ultrasonography vertebral artery dissection e 100% . 
la cta si dimostrata tecnica sensibile per la diagnosi di vad ; effettuata a completamento di uno studio tc dellencefalo senza mdc , ha il vantaggio di essere rapidamente disponibile e semplice da eseguire . parole chiave angio - tc eco color doppler vertebral artery dissection introduction introduzione acute vertebral artery dissection ( vad ) is one of the recognised causes of posterior circulation stroke and subarachnoid haemorrhage , with a reported annual incidence of 11.5 cases per 100 , 000 and no significant gender predilection . prompt detection of the condition , especially in young and middle - aged subjects , who account for 20% of cases , is mandatory [ 13 ]  . 
among neuroimaging tests , conventional digital subtraction angiography ( dsa ) has long been the criterion standard for diagnosis and followup of vad [ 4 ] , but this technique is not without risk . 
however , dsa is still irreplaceable in evaluating complications and providing a panoramic view of the vascular tree for planning surgical or endovascular treatment [ 5 ]  . colour - doppler ultrasonography ( cdus ) is the first - line screening tool for assessing the epiaortic vessels in patients with suspected dissection , but its major drawback is the lack of high specificity . 
head and neck imaging has recently seen major changes with the advent of the latest generation multidetector computed tomography ( mdct ) scanners with shorter examinations times , thinner sections and higher resolution . 
 materials and methods we retrospectively reviewed 15 cases of vad in 15 patients ( five men and ten women , age range 2858 years ) who came to our attention between august 2001 and september 2005 . the diagnosis was based on appropriate clinical presentation , absence of atherosclerotic disease in the cerebrovascular circulation and the presence of distinctive ct features subsequently confirmed by conventional angiography used as the reference standard . 
all patients with clinical suspicion of la dissezione acuta dellarteria vertebrale ( vad ) rappresenta una delle cause riconosciute di ictus nel territorio del circolo posteriore e di emorragia subaracnoidea con un incidenza annuale che si attesta intorno a 11 , 5 casi per 100000 abitanti / anno senza significative differenze di sesso . 
tra le indagini di neuroimaging lesame angiografico ( dsa ) considerata la metodica di riferimento per la diagnosi e il follow - up della vad [ 4 ] , ma tale tecnica non scevra da rischi . 
i limiti maggiori sono rappresentati dallinvasivit e soprattutto dallincapacit di analizzare direttamente la parete vasale , inoltre nel caso di lievi alterazioni parietali di media entit non completamente stenosanti lo studio pu essere non diagnostico . 
tuttavia la dsa rimane ancora insostituibile per lo studio delle complicanze e per una visione panoramica dellalbero vascolare , fornendo gli elementi necessari per pianificare gli interventi di tipo chirurgico e / o endovascolare [ 5 ]  . leco color doppler ( ecd ) rappresenta attualmente lindagine di screening di prima istanza dei vasi epiaortici nei pazienti con sospetto clinico di dissezione , tuttavia lo svantaggio maggiore la mancanza di elevata specificit . 
lapproccio allimaging del capo e del collo completamente cambiato negli ultimi anni grazie allavvento dei tomografi multistrato di ultima generazione , capaci di eseguire studi con tempi di scansione minori , con collimazioni pi sottili , con risoluzione pi elevata . 
scopo del presente studio quello di confrontare laccuratezza diagnostica dellecd e della cta nella diagnosi di dissezione acute dellarteria vertebrale . materiali e metodi abbiamo revisionato retrospettivamente 15 vad in 15 pazienti ( 5 uomini e 10 donne , et compresa tra 2858 anni ) , giunti alla nostra osservazione nel periodo agosto 2001 - setf . 
the main clinical presentations leading to imaging were posterior cervical pain and occipital headache in ten patients , visual impairment and facial nerve deficits in two patients , dysphagia with unilateral cerebellar ataxia in one patient and sensory and motor deficits in two patients . 
a region of interest ( roi ) was positioned in the carotid artery , and a threshold of 80 hu was selected , with a fixed delay of 6 s after beginning of the acquisition . 
in selected cases , we performed late - phase acquisitions after 34 m volume data were acquired in 3040 s by using a nominal section thickness of 1.25 mm , a table feed / rotation of 7.5 mm , pitch 1.5 and a gantry rotation period of 0.8 s , 120 kv and 230 ma . 
the axial - source ct images were postprocessed into thin - slab maximum intensity projection ( mip ) and three - dimensional ( 3d ) volume rendered ( vr ) reconstructions by using a dedicated workstation ( advantage windows 4.0 , ge medical systems )  . 
all cta images were evaluated by two expert neuroradiologists ( rs , fp ) who were aware of the clinical data but blinded to the us diagnosis . cases of discordant interpretation were solved by consensus . the time required for image interpretation was around 15 mcerebral angiography was done by two expert interventional neuroradiologists ( fp , am ) using dsa ( integris bn 3000 , philips medical systems , best , the netherlands )  . 
ct and dsa diagnostic criteria for vad were increased vessel calibre with aneurysmal pattern ( focal or fusiform dilatation with or without proximal or distal stenosis ) , evidence of a stenoocclusive pattern with tapering stenosis and direct visualisation of false lumen or segmental or long stenosis . 
la diagnosi stata posta in base ad una sintomatologia clinica appropriata , in base allesclusione di una malattia aterosclerotica del circolo cerebrovascolare e in base alla presenza di alcuni segni tomodensitometrici specifici , successivamente confermati con dsa , considerata come metodica gold standard . 
il quadro clinico desordio era caratterizzato da dolore cervicale posteriore e / o cefalea occipitale in 10 pazienti , deficit visivo e del faciale in 2 pazienti , disfagia ed atassia cerebellare unilaterale in un paziente , deficit sensitivi e motori in 2 pazienti . 
nessun paziente , al momento della diagnosi , presentava fattori di rischio per patologia vascolare n connettivopatie o presenza di potenziali sorgenti emboligene . tutti gli esami ecd ( acuson , aspen , usa ) sono stati eseguiti da un operatore esperto ( g.c. ) con sonda lineare ad alta frequenza 7 , 512 mhz , scansioni longitudinali e assiali sulle arterie vertebrali , valutazione della direzione di flusso e dello spettro doppler . 
la cta , effettuata con apparecchiatura 4 - canali ( lightspeed , qxi , ge medical systems , milwaukee , wi , usa ) , a complemento di uno studio diretto senza mdc dellencefalo , stata eseguita mediante iniezione ev di mdc iodato non - ionico a bolo singolo con volume di circa 140 ml ( visipaque320 , amersharm health , gran bretagna ) con flusso di 4 , 5 ml / s . 
per ottimizzare il contrast enhancement , lo scan delay stato selezionato in base a tecnica semiautomatica di bolus tracking ( smart prep ) dopo posizionamento di una roi in carotide , scelta di una soglia di 80 uh predefinita con ritardo fisso di 6 secondi dallinizio della scansione . 
in alcuni casi sono state inoltre eseguite delle scansioni in fase tardiva dopo circa 34 minuti . i dati volumetrici sono stati acquisiti durante unapnea di 3040 secondi , utilizzando spessore effettivo di strato di 1 , 25 mm , velocit letto portapazienti / rotazione 7 , 5 mm , pitch 1 , 5 , periodo di rotazione tubo radiogeno - detettori 0 , 8 s , kv 120 e ma 230 . 
nel post - processing abbiamo ricostruito , a partire dalle immagini assiali , immagini 3d - mip thin slab e 3d - vr utilizzando una workstation dedicata ( advantage windows 4.0 , ge medical systems )  . 
criteri diagnostici cta e dsa di dissezione sono stati : visibilit di un calibro vasale aumentato con pattern aneurismatico ( dilatazione settoriale o fusiforme con o senza stenosi prossimale o distale ) , visibilit di un pattern steno - occlusivo con assottigliamento progressivo del lume vasale , visualizzazione diretta del doppio lume , stenosi segmentale o lunga . 
concordance between readers 1 and 2 for the detection of vad by cta was calculated with the cohen k value according to the formula k = io - ie / 1 - ie , where io is the observed concordance and ie the expected concordance . analisi statistica trattamento con terapia anticoagulante e / o antiaggregante e / o procedura interventistica , stato effettuato con ecd e cta a 6 e 9 mesi . results among the 15 vad , the most common findings demonstrated by angiography were a stenoocclusive pattern in 11 patients ( three tapering stenoses with distal occlusion , four dissecting membrane with true and false lumen and visible intimal flap and four irregular segmental or long stenoses with string - sign appearance )  . 
four patients had aneurysmal an angiographic pattern with focal dilatation of 22.8 cten of the 15 vad ( 66% ) were located at segment v4 , three ( 20% ) at segment v3 and two ( 13% ) at segment v2 . 
of the four patients with aneurysmal angiographic pattern , three were treated with balloon or coil embolisation and the remaining one was managed conservatively . cdus revealed ten out of 15 vad , with a sensitivity of 66% , specificity of 60% , positive predictive value of 55.5% and negative predictive value of 70.5%. 
among the true positive cases , in eight , the diagnosis was based on indirect signs , such as high resistance obstructive flow with severely diminished systolic and absent or low diastolic flow ( figs . 1e , f , 2e )  . 
in the other two patients , the diagnosis was based on the evidence of the dissecting membrane with visualisation of the true and false lumen . cta enabled the correct identification of all 15 vad . the reported sensitivity , specificity , positive predictive value and negative predictive value were 100% , 95% , 93.7% and 100% , respectively . 
differences in cta versus cdus sensitivity ( 100% vs 66% ) , specificity ( 95% vs 60% ) and diagnostic accuracy ( 97% vs 62.8% ) were significant ( p value < 0.05 ; mcnemar test )  . 
la concordanza interosservatore per la detezione di vad con cta stata calcolata utilizzando il k statistico di cohen , in accordo alla formula : k = io - ie / 1 - ie , dove io la concordanza osservata e ie la concordanza attesa . risultati i reperti semeiologici riscontrati angiograficamente tra le 15 dissezioni rilevate sono stati : un pattern di tipo steno - occlusivo in 11 pazienti ( tre stenosi con assottigliamento progressivo del vaso fino allocclusione distale , segno della fiamma , quattro dissezioni vere e proprie con visualizzazione del doppio lume e del relativo flap intimale , quattro stenosi segmentarie irregolari o lunghe con aspetto string sign ) ed pattern era tipo aneurismatico in 4 pazienti , con dilatazione focale del lume vasale tra 2 e 2 , 8 cdieci dell1e 15 dissezioni ( 66% ) erano localizzate a livello del segmento v4 , 3 ( 20% ) a livello del segmento v3 e 2 ( 13% ) in corrispondenza del segmento v2 . 
tutti i pazienti con dimostrata dissezione steno - occlusiva hanno ricevuto un trattamento terapeutico anticoagulante o antiaggregante ; in tutti i casi si ottenuta una guarigione clinica pressoch completa con ricanalizzazione del vaso nei controlli a 69 mesi . 
dei 4 pazienti che presentavano pattern aneurismatico , tre sono stati sottoposti a trattamento percutaneo di angioplastica o embolizzazione con spirali , un paziente stato trattato conservativamente . lecd risultata diagnostica in 10 / 15 vad con una riportata sensibilit del 66% , specificit del 60% , valore predittivo positivo del 55 , 5% , e valore predittivo negativo del 70 , 5% . 
la diagnosi stata posta nei rimanenti 2 casi attraverso la visualizzazione diretta del doppio lume ; i dati statistici sono riportati in tabella 1 . la cta ha identificato correttamente tutte 15 le vad , con valori di sensibilit , specificit , valore predittivo positivo e valore predittivo negativo rispettivamente del 100% , 95% , 93 , 7% , 100% . 
1a - f dissezione spontanea della va in donna di 45 anni , che presentava cefalea occipitale , ad esordio acuto , con cervicalgia seguito da deficit sensitivo dellarto superiore . 
alla valutazione doppler si rileva flusso stenoostruttivo ad alta resistenza con riduzione del picco sistolico e con assente componente diastolica ( e , f )  . tissue disorders associated with an underlying structural defect of the arterial wall , such as marfan syndrome , ehlers danlos syndrome , fibromuscular dysplasia , pseudoxanthoma elasticum and osteogenesis imperfecta type ii , whereas enviparietali che mimavano una stenosi filiforme . 
tra cta e ecd sono risultate statisticamente significative ( p < 0 , 05 ) le differenze tra i valori sensibilit ( 100% vs 66% ) , specificit ( 95% vs 66% ) e accuratezza diagnostica ( 97% vs 62 , 8% )  . 
anomalie di lunghezza e decorso dei vasi quali kinkinge coiling sembrano incrementare il rischio di una dissezione [ 6 , 7 ]  . in ogni modo le cause di dissezione arteriosa sono attribuibili alla lacerazione dellintima oppure alla rottura dei vasa vasorum , con formazione di un falso lume o di un ematoma intramurale a seconda che ci sia o meno una comunicazione diretta con il lume vasale . 
se il versamento emorragico rimane confinato tra lamina elastica interna e tonaca media si ha stenosi oppure ostruzione del vaso , mentre se il danno si estende a coinvolgere lavventizia si pu avere un rigonfiamento sacculare o fusiforme negli strati pi esterni della parete ( aneurisma dissecante )  . 
la localizzazione pi frequente dellaneurisma dissecante nella regione del segmento v4 , in virt a tale livello di una lamina elastica interna spessa , dellassenza della lamina elastica esterna , di unavventizia sottile e di poche fibre elastiche nella tunica media [ 8 ]  . 
tuttavia la localizzazione pi frequente della dissezione , qualsiasi sia il pattern di presentazione , a livello del tratto extracranico , ed in particolare a livello del segmento v3 , perch mobile e maggiormente esposto a traumi anche lievi [ 14 ]  . 
axial and volume rendered ( vr ) computed tomography angiography ( cta ) ( a , b ) of the left v4 segment shows increased external diameter with dissection ( red arrow )  . 
le immagini assiali e le ricostruzioni vr ( a , b ) del segmento v4 di sinistra mostrano occlusione completa con aumento complessivo del calibro vasale su base dissecativa ; le corrispondenti immagini ecografiche dimostrano un flusso distale retrogrado dal vaso controlaterale ( c )  . ronmental factors include hypertension , tobacco use , oral contraceptives , abuse of sympathicomimetic drugs , events associated with hyperextension or rotation of the neck ( yoga , coughing , vomiting , sneezing ) , chiropractic manipulations and recent history of respiratory tract infection and traumatic events . 
arterial kinking or coiling seems to increase the risk of spontaneous dissection [ 6 , 7 ]  . pathological causes of the dissection are related to tearing of the intima or rupture of vasa vasorum , with formation of false lumen or an intramural haematoma , depending on the presence or absence of direct communication with the vessel lumen . 
in our patients , 13 / 15 dissections ( 86.6% ) occurred at segments v3 and v4 , in agreement with previous reports [ 9 ]  . typical clinical manifestations of vad include posterior cervical pain spreading to the shoulder and headache in the occipital area ; ischaemic symptoms are common and may be related to involvement of lateral medulla ( wallenbergs syndrome ) , thalamus and cerebral or cerebellar hemispheres . despite its relatively poor specificity ( 60% in our series ) , tendency to overestimate stenoses and inability to assess part of the cervical and intracranial va , cdus is the fastest and simplest method for the initial evaluation of patients with suspected vad and for the follow - up . 
typical us findings , such as irregular stenosis , dissecting membrane , localised increase in diameter of the artery , pseudoaneurysm , intramural haematoma and tapering stenosis with distal occlusion are detectable in more than 90% of cases [ 10 , 11 ]  . 
sonographic diagnosis of dissection of the third and fourth segments is based on indirect signs such as absence of flow , high resistance obstructive flow with severely diminished systolic and absent or low diastolic flow ( staccato flow ) , and diminished peak systolic velocity with at least 50% reduction compared with the contralateral side [ 11 ]  . cta is an important alternative in diagnostic screening , as it is able to provide high - resolution and high - contrast images of the arterial lumen and wall , allowing recognition of both vascular alterations and possible thromboembolic complications [ 12 ]  . 
the most reliable diagnostic ct criteria , consistent with the dsa il tipico quadro clinico di vad caratterizzato da dolore cervicale posteriore con irradiazione alla spalla e / o cefalea occipitale ; i sintomi ischemici sono comuni e interessano in maniera particolare la porzione laterale del midollo spinale ( manifestandosi in tal caso come sindrome di wallenberg ) , il talamo e gli emisferi cerebellari e cerebrali . 
nonostante la relativa bassa specificit ( 60% nella nostra casistica ) , la tendenza a sovrastimare il grado di stenosi e limpossibilit di esplorare parte del tratto cervicale e intracranico della va , lecd la tecnica pi rapida e semplice per liniziale inquadramento diagnostico dei pazienti con sospetta vad , e per il follow - up degli stessi . 
le tipiche alterazioni semeiologiche ecografiche ( lesioni di tipo steno - ostruttivo , alterazioni di parete con possibilit di visualizzare il flap intimale , incremento dimensionale segmentario del vaso occluso , lo pseudoaneurisma , lematoma intramurale e la stenosi filiforme con occlusione distale del vaso ) , sono riscontrabili in pi del 90% dei casi [ 10 , 11 ]  . 
la diagnosi ecografica di dissezione con localizzazione a livello dei segmenti v3 e v4 , pu essere basata su segni indiretti come lassenza di flusso , un picco sistolico seguito da flusso diastolico ridotto e / o assente , indicativo di alte resistenze distali ( staccato flow ) , un picco di velocit sistolica ridotto di almeno il 50% rispetto ai valori di picco del vaso controlaterale [ 11 ]  . la cta rappresenta unimportante alternativa , nella fase di screening diagnostico , in quanto fornisce immagini ad alta risoluzione ed alto contrasto del lume e della parete arteriosa , consentendo di riconoscere sia le alterazioni vascolari che le possibili complicanze trombo - emboliche [ 12 ]  . 
i criteri pi affidabili per la diagnosi , congrui a quelli della dsa , riflettono lanalisi del lume arterioso residuo , la sede della dissezione e la misurazione del calibro vasale complessivo ; nella nostra serie tutte e 15 le dissezioni presentavano aumento dimensionale segmentario del vaso occluso . 
in our series cta yielded a sensitivity of 100% , a specificity of 95% , a positive predictive value of 93.7% , a negative predictive value of 100% and a diagnostic accuracy of 97% . a limitation of our study was the lack of correlation with mri . 
the value of mri lies in its particularly high resolution in the posterior fossa and the capability for direct visualisation of intramural haematomas and other luminal abnormalities , such as aneurysmal dilatation , intimal flap or occlusion . the typical mri appearance of an intramural haematoma consists of an increased external diameter of the artery , an eccentric region of high signal intensity and narrowing of the arterial lumen . 
the region of high signal intensity is due to the methemoglobin blood products within the haematoma . for this reason , mri is superior to cta in depicting a subacute or chronic intramural haematoma [ 13 ]  . the differential diagnosis of vad , especially with stenoocclusive pattern with tapering stenosis , is sometimes difficult . 
these cases require accurate evaluation of patients history , neurologic examination , laboratory tests ( blood screening and coagulation test ) and imaging examinations [ echocardiography ( ecg ) , cdus of the epiaortic vessels ] to exclude potential cardioembolic sources , atheromas , vasculitis , hypoplasia or dysplasia and vasospasm . conclusions in conclusion , the results of our experience confirm previous findings [ 12 ]  . 
with this technique , visualisation of the intramural haematoma combined with staccato high - resistance obstructive flow with severely diminished systolic and absent or low diastolic flow , strongly indicate the presence of spontaneous vad . 
however , because of the frequent nonspecificity of cdus findings , patients with a clinical suspicion of vad and inconclusive or normal duplex scan findings should be further investigated by cta . 
 stra casistica sono stati riportati per la cta valori di sensibilit del 100% , specificit del 95% , un valore predittivo positivo del 93 , 7% , un valore predittivo negativo del 100% e unaccuratezza diagnostica del 97% . un limite del nostro studio stato la mancata correlazione tra cta e rm . 
la rm presenta infatti una migliore risoluzione a livello della fossa cranica posteriore , ed ha il vantaggio di visualizzare direttamente lematoma intramurale , la dilatazione aneurismatica , il flap intimale e locclusione . lematoma intramurale evidenziabile in rm sotto forma di un aumento del diametro vasale esterno , come ispessimento parietale eccentrico iperintenso che circonda a semiluna o a bersaglio il lume vascolare ristretto . 
per tale motivo , la rm distingue meglio , rispetto alla cta , tra ematoma intramurale subacuto e / o cronico [ 13 ]  . i pattern steno - occlusivi di dissezione , con stenosi filiforme associata , sono alcune volte di dubbia interpretazione , necessario pertanto unaccurata valutazione della storia dei pazienti , un attento esame neurologico , il ricorso ad esami laboratoristici ( esame emocromocitometrico , ves , test di emocoagulazione ) e strumentali ( ecg , ecocardiografia , ecd dei vasi epiaortici ) per escludere potenziali sorgenti emboligene cardiache , alterazioni ateromasiche o quadri vasculitici , ipoplasie , displasie e vasospami . conclusioni i risultati della nostra esperienza confermano quanto riportato in letteratura negli ultimi anni [ 12 ]  . 
in particolare , lecd risulta la tecnica pi rapida e semplice per liniziale inquadramento diagnostico , per una rapida visione dei vasi extracranici del collo , e per il follow - up . 
con questa tecnica la visualizzazione diretta dellematoma intramurale associata ad un flusso staccato , steno - ostruttivo , ad alta resistenza con picco di velocit sistolica ridotto , seguito da un flusso diastolico ridotto o assente , fortemente indicativa di una dissezione arteriosa spontanea . 
tuttavia a causa dellaspecificit dei reperti ecografici , pazienti con sospetto clinico di dissezione , in presenza di rilievi ecografici negativi o dubbi , dovrebbero essere sottoposti ad esame cta . 
i - 00168 rome , italy 2deptartment of radiology , neuroradiology section , ucsf university of california san francisco , san francisco , ca , usa correspondence to : a . 
by providing quantitative measurements of cerebral blood flow ( cbf ) and cerebral blood volume ( cbv ) , dynamic perfusion computed tomography ( p - ct ) allows visualisation of cerebral autoregulation mechanisms and represents a fast , available and reliable imaging option for assessing cerebral perfusion . 
thanks to its feasibility in emergency settings , p - ct is considered most useful , in combination with ct angiography , in acute ischaemic patients , as it is able to provide a fast and noninvasive assessment of cerebral perfusion impairment . 
in addition , p - ct can play a diagnostic role in other types of cerebrovascular disease to assess functional reserve , and in intracranial neoplasms , where it has a role in diagnosis , grading , biopsy guidance , and follow - up during treatment . 
this article illustrates the principles , technique and clinical applications of p - ct cerebral perfusion studies . key words brain ischemia brain neoplasms brain injury hemodynamics perfusion ct riassunto lo studio dellemodinamica cerebrale , ottenuto con le metodiche di imaging , con le sue varie ed attuali applicazioni , genera interesse crescente . 
la tc perfusione dinamica ( p - tc ) permette una valutazione quantitativa del flusso cerebrale ematico ( cbf ) e del volume cerebrale ematico ( cbv ) , offrendo cos una visualizzazione diretta dei meccanismi di autoregolazione cerebrale , e si pone come una valida alternativa ad altre modalit di misurazione della perfusione cerebrale , rispetto alle quali ha il maggior vantaggio di essere una tecnica prontamente disponibile ed accessibile , in condizioni di emergenza , nella maggior parte dei centri medici . 
per tale ragione la p - tc utile soprattutto nellischemia cerebrale acuta , condizione in cui , associata allangio - tc , offre in maniera rapida e non - invasiva , la valutazione eziologica dellipoperfusione , nonch delle sue ripercussioni emodinamiche e fisiopatologiche sul parenchima cerebrale . 
inoltre la p - tc trova utile impiego in pazienti con altre patologie cerebro - vascolari e per la diagnosi , il grading , la guida alle procedure bioptiche , ed il controllo durante la terapia , dei tumori intra - cranici . 
questo articolo si propone di riassumere i principi , la tecnica e le principali applicazioni cliniche degli studi di perfusione cerebrale basati sulla metodica tc . parole chiave ischemia cerebrale neoplasie cerebrali trauma cranico perfusione tc introduction introduzione rapid technological advances in functional imaging techniques have extended the scope of radiology , and in particular of neuroradiology , beyond the boundaries of morphological imaging . 
perfusion studies can now be carried out with magnetic resonance imaging ( mri ) and computed tomography ( ct ) as well as with the gold standard modalities used until now , such as positron emission tomography ( pet ) , single - photon emission tomography ( spect ) il rapido progresso tecnologico applicato alle tecniche di imaging funzionale ha spinto la radiologia in generale , e la neuroradiologia in particolare , oltre i confini della morfologia ; in questo contesto genera crescente interesse la valutazione a scopo diagnostico dellemodinamica cerebrale ( perfusione cerebrale )  . 
gli studi di perfusione ottenuti con rm e tc si sono affiancati alle metodiche fino ad ora impiegate e considerate gold standard , quali la tomografia ad emissione di positroni ( pet ) , la tomografia ad emissione di singolo fotone ( spect ) e la xenon - tc , con 1225 a . 
this is because the introduction of thrombolytic therapy for the treatment of stroke has highlighted the need for a fast and readily available technique capable of identifying the perfusion defect and evaluating its extent and severity [ 2 , 3 ]  . 
 in patients with acute stroke undergoing emergency evaluation , dynamic perfusion ct ( p - ct ) has been proposed as a particularly useful technique after unenhanced brain ct ( which rules out intracranial haemorrhage ) on account of its ease of use , reproducibility of quantitative measurements , ready availability , limited cost and tolerability [ 3 , 4 ]  . 
moreover , the use of p - ct may be extended to the evaluation of the cerebrovascular reserve in patients with haemodynamically significant stenoses of the intraor extracranial arteries even with acetazolamide challenge in potential candidates for temporary or permanent occlusion of the internal carotid artery ( balloon occlusion test ) [ 5 ] , or in patients with subarachnoid haemorrhage at risk of vasospasm [ 6 ]  . 
in addition to acute and chronic cerebrovascular disease , a further application of p - ct is the measurement of cerebral blood volume ( cbv ) and microvascular permeability ( ps ) in brain tumours [ 7 ]  . general technique p - ct derives information on brain haemodynamics by analysing the first passage through the cerebral vessels of an intravenous contrast bolus . 
because there is a direct linear relation between the concentration of contrast material and density , passage of contrast bolus results in an increase in density of the areas being examined that is proportional to the amount of contrast material present in the blood vessels . the blood - brain barrier ( bbb ) prevents the contrast material from spreading into the interstitium , so that under normal conditions the increase in density is only transient , occurring during the first intravascular passage of the bolus . 
p - ct is based on the physical - mathematical tracer kinetic model [ 8 ] , which assumes that the contrast bolus is instantaneous , is introduced into a single vessel , passes through a capillary network , remains totally intravascular and flows out through a single venous conduit . p - ct can be performed on any spiral ct scanner capable of cine mode scans , with the aid of an automatic injector . the anatomical coverage of p - ct along the craniocaudal axis is limited , as the scan is obtained without table motion at 510 mm for single - detector devices , at 20 mm for multidetector devices ( 232 ) and at 40 mm for the recent 64 - detector - row scanners . 
for this reason , the anatomical level to be studied is selected , generally on the scout view or initial morphological scan , and the perfusion study performed at that location using a cine scan without table motion . 
one possible study protocol , applicable to both singleand multislice scanners ( 232 slices ) involves 1 rotation / s for 50 s , 1226 relativi vantaggi e limiti [ 1 ]  . 
infatti lintroduzione della terapia trombolitica nel trattamento dellictus ischemico acuto ha reso evidente il bisogno di una tecnica rapida e prontamente disponibile per lidentificazione del deficit perfusionale e la valutazione della sua estensione e della sua entit [ 2 , 3 ]  . nei pazienti con ictus , in condizioni di emergenza , dopo la tc cerebrale di base senza mdc ( che esclude lemorragia intra - cranica ) la tc perfusione dinamica ( p - tc ) , per semplicit e rapidit di esecuzione , riproducibilit di misurazioni quantitative , disponibilit sul territorio , costi contenuti e tollerabilit da parte dei pazienti , si propone come metodica di particolare interesse ed utilit [ 3 , 4 ]  . 
la p - tc pu essere effettuata velocemente con qualsiasi apparecchiatura spirale , e le mappe di perfusione possono essere ottenute in breve tempo mediante una workstation dotata di apposito software . 
limpiego della p - tc pu inoltre essere esteso alla valutazione della riserva cerebro - vascolare in pazienti con stenosi arteriose emodinamicamente significative intrao extra - craniche anche con stress - test allacetazolamide in potenziali candidati ad occlusione temporanea o definitiva dellarteria carotide interna ( balloon occlusion test ) [ 5 ] , o in pazienti con emorragia sub - aracnoidea , a rischio di vasospasmo [ 6 ]  . 
poich esiste una relazione proporzionale lineare diretta tra concentrazione del mdc e densit , il passaggio del bolo di mdc induce un aumento della densit nelle aree esaminate , proporzionale alla quantit di mdc presente nei vasi . 
la presenza della barriera emato - encefalica ( bee ) impedisce al mdc di diffondersi dai vasi allinterstizio , cosicch , in condizioni normali , laumento di densit solo transitorio , durante il suo primo passaggio intra - vascolare . 
la p - tc basata sul modello fisico - matematico del tracciante cinetico ( kinetic tracer model ) [ 8 ] , il quale assume che il bolo di mdc sia pressoch istantaneo , sia immesso in un vaso unico , passi attraverso una rete capillare , rimanga totalmente intra - vascolare , e defluisca da un singolo collettore venoso . la p - tc pu essere effettuata su qualsiasi apparecchiatura tc con tecnologia spirale che sia in grado di effettuare scansioni in modalit cine , con lausilio di un iniettore automatico . 
la copertura anatomica della p - tc lungo lasse cranio - caudale limitata , poich la scansione si effettua a tavolo fermo , a 510 mm per le apparecchiature spirali a strato singolo , a 20 mm per le apparecchiature tc multia . 
the short scan delay is aimed at the acquisition of a first baseline scan before arrival of bolus and is applied independent of the patients cardiocirculatory condition or type of ct device used . 
for a four - detector - row scanner but also possible with other multislice devices allows the effective radiation dose to be contained below that calculated for a conventional brain ct study [ 10 , 11 ]  . 
lower milliampere settings result in a reduced signal - to - noise ratio ( snr ) and poorer densitometric resolution , with consequently less precision of the parametric measurements ( expressed by increased standard deviation values ) ; nevertheless , it represents a reasonable compromise between radiation - dose containment and diagnostic quality of the examination . 
use of the automatic injector and , if a dual syringe injector is available , of a saline flush after the contrast bolus allows administration of a fast and compact bolus [ 11 ]  . 
the images , generally acquired with 5 - mm thickness to avoid beam - hardening artefacts , are reconstructed with a thicknesses of 10 mm to increase the snr , and at 0.5 - s intervals to increase temporal resolution . data acquired during the cine scan are then analysed on a workstation running dedicated postprocessing software that generates and analyses the time - density curves . 
a region of interest ( roi ) is placed on an artery in the images to view the time - density curve , which reflects the compactness of the bolus . 
it is important to note that , although ideally one might expect the arterial curve to fall back to baseline density levels after the first pass of the bolus , in practice , even when the bolus is sufficiently compact and the bbb intact , the curve tends to remain on a plateau varying height above baseline ( usually 10%30% of the peak )  . 
the maximum slope model approximates the cerebral blood flow ( cbf ) value from the slope of the time - density curve , calcustrato , dotate di multiple file di detettori ( da 2 a 32 ) , a 40 mm per le recenti tc multidetettore a 64 strati . 
per tale ragione si seleziona il livello anatomico da studiare , generalmente sulla scout view o su una scansione morfologica iniziale , ed al livello selezionato si esegue lo studio di perfusione , che consiste in una scansione cine , a tavolo fermo . 
un possibile modello di protocollo di studio , applicabile con apparecchiature tc a strato singolo o multiplo ( 232 strati ) , prevede 1 rotazione / s per 50 s , con 57 secondi di ritardo rispetto alliniezione attraverso una cannula 1820 g , in una vena antecubitale , di 4050 ml di mdc iodato non ionico ( 300370 mg% ) a 45 ml / s [ 9 ]  . 
il breve ritardo tra liniezione del mezzo di contrasto e linizio della scansione finalizzato ad ottenere lacquisizione di una linea di base , prima dellarrivo del bolo , ed applicabile indipendentemente dalla condizione cardio - circolatoria del paziente e dal tipo di apparecchiatura tc utilizzata . 
 [ 10 , 11 ] per una apparecchiatura tc multistrato con quattro file di detettori , ma applicabile anche ad altri tipi di tc multistrato , permette di contenere la dose effettiva di radiazioni al di sotto di quella calcolata per un esame tc del cranio convenzionale . 
la limitazione dellamperaggio causa una diminuzione del rapporto segnale / rumore ed una ridotta capacit di risoluzione densitometrica , cui consegue una ridotta precisione delle misurazioni parametriche ( espressa dagli aumentati valori di deviazione standard ) , ma rappresenta un ragionevole compromesso tra contenimento della dose di radiazioni e qualit diagnostica dellesame . 
luso delliniettore automatico e , se si dispone di un iniettore a doppia siringa , di un bolo di soluzione fisiologica a seguire il mdc , permettono di somministrare un bolo rapido e compatto [ 11 ]  . 
le immagini , generalmente acquisite con spessori di 5 mm , per evitare artefatti da indurimento del fascio , vengono ricostruite a spessori di 10 mm , per aumentare il rapporto segnale / rumore , e a 0 , 5 s di intervallo , per incrementarne la risoluzione temporale . i dati acquisiti durante la scansione cine sono poi analizzati ad una workstation dotata di apposito software che produce ed analizza le curve tempo / densit . 
la compattezza del bolo di mezzo di contrasto determina la morfologia della curva , con ascesa ripida e discesa compresa nei 50 s di scansione . lates cbv as the area under the curve , and from these two parameters derives mean transit time ( mtt ) by solving the central volume equation . 
il modello maximum slope approssima il valore del cbf dalla pendenza ( slope ) della curva densit / tempo , calcola il cbv come larea sottesa alla stessa curva , e da questi due parametri deriva il mtt risolvendo lequazione del volume centrale ; questo modello non richiede la selezione di un arterial input function ( aif ) , ma necessita di velocit di iniezione del mdc molto alte ( > 6 ml / s ) , e fornisce solo misurazioni relative non quantitative [ 12 , 13 ] ; il modello di deconvoluzione si basa su un complesso processo matematico che richiede la scelta di un aif , ovvero di una curva densit / tempo di unarteria , con cui confrontare la curva ottenuta in corrifig . 
a maximum - slope model derives cerebral blood volume ( cbv ) values by calculating the area under the curve , cerebral blood flow ( cbf ) as the slope of the curve and mean transit time ( mtt ) by solving the central volume equation . 
again , cbv corresponds to the area under the curve , mtt to full width at half maximum ( fwhm ) and cbf is derived from the central volume equation . 
a il modello del maximum slope calcola il cbv integrando larea sotto la curva densit / tempo , il cbf secondo la tangente alla porzione ascendente della curva , e deriva il calcolo del mtt dallequazione del volume centrale . 
b il modello di deconvolution , tramite un arterial input function , trasforma la curva densit / tempo in una curva di funzione tissutale , in cui lintegrale dellarea sotto la curva esprime il cbv , il tempo alla met dellaltezza massima ( full width at half maximum fwhm ) rappresenta il mtt ed il cbf derivato dallequazione del volume centrale . 
the deconvolution method relies on a complex mathematical process that requires the use of an aif that is , the time - density curve of an artery with which to compare the curve obtained on the parenchymal pixels so as to correct for the effects of bolus dispersion and thus better reflect the postulates of the tracer kinetic model , which assumes a virtually instantaneous bolus input [ 14 ]  . 
the deconvolution model allows one to reduce the contrast injection rate ( 35 ml / s ) and provides quantitative measurements [ 1517 ] that have been validated by comparison with pet [ 18 ] , spect [ 19 ] and xe - ct [ 20 ]  . although some commercial software packages can automatically select the best aif , aif choice is one of the most controversial aspects of p - ct . 
partial - volume artefacts are practically unavoidable , as the imaging section has a thickness of 10 mm and the artery to be selected generally has a calibre of 24 mthe problem can be partially avoided by choosing an artery that runs perpendicular to the section for example , segment a2 of the anterior cerebral artery so that the roi is placed on a pixel corresponding to a voxel almost completely taken up by the vessel . 
more complex , in the case of cerebral ischaemia , is the problem of selecting an intracranial vessel that is ipsilateral or contralateral to the lesion ( generally segment m2 of the middle cerebral artery ) , or a vessel with proximal stenosis , generally at an extracranial location . 
although there is no consensus [ 21 , 22 ] and studies are underway , our advice is to choose the aif from a healthy vessel , often the anterior cerebral artery , and then compare the results with those obtained with an aif selected on the abnormal side . 
 the software then requires selection of a venous roi , which provides a reference measurement of blood density , considered free of partial - volume artefacts , such as the posterior descending portion of the superior sagittal sinus . 
this curve is used to derive mtt , identified by the width of the curve at spondenza dei pixel parenchimali , per correggere matematicamente gli effetti della dispersione del bolo e riavvicinarsi cos ai postulati teorici del kinetic tracer model , che , come detto , presuppone unimmissione pressoch istantanea del bolo [ 14 ]  . 
il modello di deconvoluzione permette di ridurre le velocit di somministrazione del bolo di mdc ( 35 ml / s ) e fornisce misurazioni quantitative [ 1517 ] , validate in studi di confronto con pet [ 18 ] , spect [ 19 ] e xetc [ 20 ]  . 
gli artefatti da volume parziale sono praticamente inevitabili , infatti , la sezione su cui si lavora ha uno spessore di 10 mm e larteria da selezionare ha generalmente un calibro di 24 mm ; per ovviare parzialmente a tale problema , si pu selezionare unarteria con decorso perpendicolare alla sezione , come nel caso del tratto a2 dellarteria cerebrale anteriore , in modo da posizionare la nostra roi su un pixel corrispondente ad un voxel quasi interamente occupato dal vaso . 
sebbene non esista definitivo consenso [ 21 , 22 ] , e siano ancora in corso studi al riguardo , il nostro consiglio di scegliere laif da un vaso ritenuto sano , spesso larteria cerebrale anteriore , e poi confrontare i risultati con quelli ottenuti con unaif scelta sul lato anormale . il software richiede poi la selezione di una roi venosa , che serve come misurazione di riferimento della densit del sangue , e viene considerata come esente da artefatti di volume parziale , come il caso del seno sagittale superiore nella sua porzione posteriore discendente . 
i parametri perfusionali sono il volume ematico cerebrale ( cerebral blood volume o cbv ) , il tempo medio di transito ( mean transit time o mtt ) ed il flusso ematico cerebrale ( cerebral blood flow o cbf ) ; alcuni software , inoltre , calcolano il tempo di picco ( time to peak o ttp )  . 
in this patient with severe stenosis of the proximal m1 segment of the right main carotid artery ( mca ) , mtt and cbf maps derived from an arterial input function ( aif ) on the anterior carotid artery ( aca ) ( healthy side ) show abnormal measurements in the right mca territory ( left column ) , whereas mtt and cbf measurements derived from an aif distal to the stenosis appear no longer abnormal ( right column )  . 
in questo paziente con stenosi serrata della porzione prossimale del tratto m1 dellacm di destra , la scelta dellaif sullaca ( lato sano ) produce mappe colore di mtt e cbf marcatamente alterate nel territorio di distribuzione dellacm destra ( colonna sinistra ) , mentre le mappe di mtt e cbf derivate da unaif sullacm destra , a valle della stenosi , appaiono sostanzialmente simmetriche ( colonna destra )  . 
5 software analysis of the arterial ( red ) and venous ( blue ) time - density curves generates the pixel - based parametric maps for mean transit time ( mtt ) , cerebral blood volume ( cbv ) and cerebral blood flow ( cbf )  . 
5 lanalisi matematica operata dal software sulla base della curva arteriosa ( in rosso ) e della curva venosa ( in blu ) genera le mappe parametriche con codice colore pixel per pixel per il mtt , il cbv ed il cbf . 
come accennato sopra , il pixel venoso , scelto da una struttura vascolare ampia , considerato essere esente da volume parziale , e quindi si assume la sua densit come unit di riferimento per il sangue ( 100 ml sangue / 100 g di tessuto ) ; la densit misurata nei singoli pixel tissutali viene poi rapportata alla misurazione venosa , ed espressa in percentuale di questa ( cbv = densit pixel parenchimale / densit pixel venoso ; es , densit nel pixel tissutale = 5% della densit nel pixel venoso cbv del pixel tissutale = 5 ml / 100 g ) ; ora pi chiaro come la sottostima della densit nella roi venosa , per artefatti di volume parziale , causi una sovrastima del cbv a livello tissutale e di riflesso , per lequazione del volume centrale cbf = cbv / mtt , anche del cbf . il cbf misura il volume di sangue distribuito a livello tissutale nellunit di tempo . 
6 in order to obtain quantitative measurements of cerebral blood volume ( cbv ) , cerebral blood flow ( cbf ) , mean transit time ( mtt ) and time to peak ( ttp ) , regions of interest ( rois ) are drawn on the different intracranial vascular territories . 
6 mediante posizionamento di apposite roi si possono ottenere misurazioni quantitative medie del cbv , cbf , mtt e ttp nei diversi territori di distribuzione delle principali arterie intra - craniche . 
it is expressed in [ s ] and is an index of the time that elapses between the beginning of contrast administration and maximum enhancement , or enhancement peak , in the roi . 
 mtt represents capillary transit time , that is , the time between arterial input in the capillary bed and venous outflow . it is expressed in [ s ] , is an sensitive index of cerebral perfusion pressure and , thanks to deconvolution , it is relatively less affected than is ttp by central haemodynamic changes such as cardiac failure or stenosis of the epiaortic arteries . mtt calculation is strictly dependent on the deconvolution process and therefore , in the event of asymmetrical perfusion as in ischaemia , on the choice of aif . 
in practice , mtt may be considered as the difference between the mean width of the time - density curve in a parenchymal pixel and the width of the curve in the reference artery ( aif ) [ 23 ]  . cbv measures the volume of cerebral blood at the capillary - tissue level , after appropriate exclusion from measurements of blood volume contained in large vessels , by means of density thresholds . 
the density measured in the single tissue pixels is then related to the venous density and expressed as a percentage of this ( cbv = parenchymal pixel density / venous pixel density ; e.g. : tissue pixel density = 5% venous pixel density = > cbv of tissue pixel = 5 ml / 100 g )  . 
it should now be clearer why an underestimation of density in the venous roi , due to partial - volume effects , leads to an overestimation of the cbv at the tissue level and consequently of cbf , given the central volume theorem cbf = cbv / mtt . cbf measures the volume of blood distributed at the tissue level in a unit of time . 
it is not measured directly but derived from the central volume theorem and is therefore dependent both on deconvolution and aif selection , which affect mtt , and on cbv measurement . 
 in brief , mtt indicates perfusion pressure , cbv reflects autoregulation mechanisms and capillary volume and cbf is the result of the above parameters . clinical applications acute ischaemic stroke thrombolysis is an approved therapy for acute ischaemic stroke [ 2 , 24 , 25 ] that aims to reperfuse the areas of ischaemic penumbra and limit the extent of the final area of infarction , thus reducing morbidity and disabling sequelae . the current indications for thrombolysis are based on a time window from symptom onset ( < 3h ) , findings of an unenhanced head ct ( no intracranial haemorrhage , no ct evidence of ischaemia of a portion of parenchyma exceeding 33% of the middle cerebral artery territory ) and absence of general contraindications for the drug [ 2 , 24 ]  . 
nevertheless , even such stringent criteria do not eliminate the significant risk of brain haemorrhage ( 15% ) [ 26 ] , and patient selection based on such criteria appears to be unsatisfactory . 
it is recognised that the time window alone is insufficient for accounting for the complex model of brain tissue viability , which in addition to a time factor includes a haemodynamic factor , a tissue factor and an intervention factor [ 27 ]  . 
as a result , individual visualisation of the extent of the infarcted and at - risk areas and of their relationship according to the pathophysiological model of infarct core and ischaemic penumbra has been proposed as a better tool for selecting patients for thrombolytic therapy . 
thrombolysis in patients with extensive cerebral infarctions and small areas of penumbra appears to be of little benefit and lead to a high risk of haemorrhage [ 25 , 28 , 29 ]  . 
on the other hand , although controversial , some studies have demonstrated that a significant proportion of patients with 1232 applicazioni cliniche ictus ischemico acuto la trombolisi una terapia approvata per lictus ischemico acuto [ 2 , 24 , 25 ] che ha lo scopo di riperfondere le aree di penombra ischemica e di ridurre lestensione dellarea finale di infarto , riducendo cos la morbilit e gli esiti invalidanti . 
le attuali indicazioni alla terapia trombolitica sono basate su una finestra temporale dallesordio clinico ( < 3 h ) , sul risultato della tc cranio in condizioni di base ( assenza di emorragia intracranica , assenza di segni tc di ischemia di una porzione di parenchima con estensione superiore al 33% del territorio vascolare dellarteria cerebrale media ) e sullassenza di controindicazioni generali al farmaco [ 2 , 24 ]  . la maggior parte dei pazienti colpiti da ictus ischemico non ricevono trattamento , poich i criteri di eligibilit sono molto restrittivi , soprattutto rispetto alla finestra temporale , anche perch in una significativa percentuale di casi il momento di insorgenza dei sintomi non determinabile con precisione ( classico il caso del cosiddetto wake - up stroke )  . 
ciononostante , perfino criteri cos restrittivi non eliminano il significativo rischio di emorragia intracranica ( 15% ) [ 26 ] e la selezione dei pazienti a cui somministrare la terapia trombolitica , basata su tali criteri , non appare soddisfacente . 
la finestra temporale infatti stata riconosciuta insufficiente a spiegare , da sola , lintricato modello della vitalit del tessuto cerebrale , che invece include , oltre al fattore tempo , un fattore emodinamico , un fattore tissutale ed un fattore terapeutico [ 27 ]  . 
perci la visualizzazione individuale dellestensione delle aree infartuate e di quelle a rischio , e del loro rapporto , secondo il modello fisiopatologico del core infartuale e della penombra ischemica , stato suggerito come un migliore strumento di selezione dei pazienti per il trattamento trombolitico . 
la trombolisi in pazienti con infarti cerebrali estesi e piccole aree di penombra , sarebbe di scarso beneficio e alto rischio emorragico [ 25 , 28 , 29 ] , mentre stato postulato e dimostrato in alcuni studi , ma ancora controverso , che una significativa percentuale di pazienti con limitate aree di infarto ed estese aree di penombra potrebbero beneficiare del trattamento di rivascolarizzazione anche oltre la classica finestra temporale delle 3 ore [ 30 , 31 ]  . il modello del core e della penombra [ 3234 ] postula che nel contesto di unarea di parenchima ipoperfusa , con elevati valori di mtt , spesso dipendente da circoli collaterali , si attuino meccanismi di autoregolazione che , inducendo vasodilatazione ed aumento del cbv , siano capaci di mantenere i valori del cbf sopra la soglia della morte cellulare neuronale ; le aree di parenchima caratterizzate da tali condizioni sono ritenute aree di penombra ischemica , ancora vitali , ad alto rischio di infarto , che potrebbero beneficiare di interventi di riperfusione . 
 limited areas of infarction and extensive areas of penumbra might benefit from revascularisation even beyond the 3 - h time window [ 30 , 31 ]  . the model of the infarct core and penumbra [ 3234 ] postulates that in the context of an area of hypoperfused parenchyma , with high mtt values , often supplied by collateral circulations , autoregulation mechanisms take place that , by inducing vasodilatation and increased cbv , are able to maintain cbf values above the threshold for neuronal death . 
where ischaemic injury is more severe and protracted , on the other hand , autoregulation is unable to maintain cbf , brain tissue sustains irreversible hypoxic damage and cbv values decrease . 
however , these pathophysiological aspects are complicated by other factors such as the duration of hypoperfusion , selective vulnerability of some neurons and physiological conditions during reperfusion [ 38 , 32 ]  . 
radiological evidence of the existence of a penumbra area has been provided by mri with combined diffusionand perfusion - weighted imaging ( dwipwi ) , the results of which have led to the pwi - dwi mismatch hypothesis [ 34 ]  . unenhanced head ct remains the first imaging modality in the assessment of patients with acute focal neurological symptoms ( stroke ) to exclude brain haemorrhage and evaluate the presence of early signs of ischaemia , such as greymatter hypoattenuation and sulcal effacement [ 35 ]  . it has been suggested that , by identifying the areas of cerebral infarction and those at risk of infarction ( ischaemic penumbra ) , the study of brain perfusion may help to select patients for thrombolytic therapy [ 15 ]  . 
other techniques for determining brain perfusion , such as xe - ct , spect and pet , although quantitative , are limited by poor availability in emergency settings and poor patient tolerance , whereas perfusion mri also suffers from an inability to provide quantitative data [ 3 ]  . 
availability in emergency settings , rapidity ( data acquisition < 5 min ) , cost and quantitative measurements probably make p - ct the technique of choice in the assessment of patients with ischaemic stroke [ 16 ]  . 
this ability of p - ct is based on the hypothesis that infarcted areas will exhibit high mtt values and low cbf and cbv values , whereas the areas at risk will show normal or increased cbv values [ 4 , 1517 , 21 , 39 , 40 ]  . 
cbv maps seem to be the least sensitive for ischaemia , with approximately 25% of acute infarctions failing to show any significant change in cbv , but are also the most specific for infarction areas [ 16 , 41 ]  . 
levidenza radiologica dellesistenza della penombra ischemica invece , stata dimostrata da studi combinati di rm con sequenze di diffusione ( dwi ) e perfusione ( pwi ) , dai cui risultati si derivato il concetto di mismatch pwi - dwi [ 34 ]  . la tc cerebrale in condizioni di base rimane la prima modalit di imaging usata per lo studio del paziente con sintomatologia neurologica focale acuta ( ictus ) , per escludere lemorragia intracranica e valutare la presenza di segni precoci di ischemia , quali lipodensit della sostanza grigia e la cancellazione dei solchi [ 35 ]  . stato suggerito che lo studio della perfusione cerebrale , identificando le aree di infarto cerebrale e quelle a rischio stage 1 stage 2 stage 3 cerebral perfusion pressure fig . 
7 the diagram illustrates the changes in mean transit time ( mtt ) , cerebral blood volume ( cbv ) , cerebral blood flow ( cbf ) and oxygen extraction fraction ( oxef ) in response to progressive reduction of cerebral perfusion pressure . 
in patients with stroke , the scan level is usually located in correspondence with the basal ganglia so as to visualise the three main supratentorial vascular territories ( fig 9 )  . 
one limitation of p - ct , especially when compared with mri , is a relative lack of sensitivity to lacunar infarctions [ 44 ] , exposure to ionising radiation and the use of iodinated contrast material . 
nonetheless , administration of iodinated nonionic di infarto ( aree di penombra ischemica ) , possa essere di ausilio nella selezione di pazienti candidati alla terapia trombolitica [ 15 ]  . 
le altre tecniche per misurare la perfusione cerebrale , quali xe - tc , spect e pet , sebbene quantitative , sono limitate dalla disponibilit in emergenza e dalla tolleranza del paziente , mentre la perfusione - rm soffre anche dellimpossibilit di fornire dati quantitativi [ 3 ]  . 
la ptc probabilmente la metodica di scelta , per disponibilit in condizioni di emergenza , per rapidit di esame ( acquisizione dati in < 5 min ) , costi contenuti , e misurazioni quantitative , nella valutazione del paziente con ictus ischemico [ 16 ]  . 
tale capacit della p - tc si basa sullipotesi che le aree infartuate presentino elevati valori di mtt , e ridotti valori di cbf e cbv , mentre nelle aree a rischio i valori di cbv siano normali o aumentati [ 4 , 1517 , 21 , 39 , 40 ]  . 
recenti studi [ 16 , 41 ] suggeriscono che le mappe di mtt siano le pi sensibili per delineare le aree ischemiche , seguite da quelle del cbf ; le mappe di cbv sembrano essere le meno sensibili allischemia , infatti , circa il 25% degli infarti acuti non mostra significative alterazioni di tale parametro , ma sono anche le pi specifiche per le aree di infarto [ 16 , 41 ]  . 
da ci deriva la raccomandazione di valutare prima le mappe di mtt e cbf alla ricerca di aree ipoperfuse , e se queste sono presenti , utilizzare le mappe di cbv per differenziare al loro interno le aree di penombra da quelle di infarto , considerando per che tali mappe possono essere normali anche in caso di infarto . 
 un importante studio prospettico [ 15 ] su pazienti affetti da ischemia cerebrale acuta , segna una pietra miliare nella validazione delle teorie su cui si basa la p - tc , mostrando significativa correlazione tra aree di ridotto cbv ( > 2 , 5 ml / 100 g ) alla p - tc di ammissione e le aree finali di infarto nei controlli a distanza , in pazienti con riperfusione , e altrettanto precisa correlazione tra aree con prolungato mtt ( > 1 , 5 volte rispetto al controlato ) e / o ridotto cbf ( riduzione > 34% rispetto al controlato ) alla p - tc di ammissione e larea finale di infarto , al controllo a distanza , in pazienti senza riperfusione . 
based on threshold values set by the operator , the software generates a colour map ( middle image in the bottom row ) where the colour green is attributed to pixels with increased mean transit time ( mtt ) , as is the case in ischaemic penumbra , and the colour red is attributed to pixels with low cerebral blood volume ( cbv ) , as is the case in the infarct core . 
sulla base di valori soglia predeterminati , il software attribuisce , nella mappa al centro nella fila in basso , il colore verde ai pixel con alterazioni perfusionali con le caratteristiche dei territori di penombra , ed il colore rosso ai pixel con caratteristiche di core infartuale . 
qualora si voglia raddoppiare la copertura anatomica , una seconda sca , nsione , ad un altro livello , pu essere effettuata osservando unattesa , rispetto alla scansione precedente , di 36 mun limite della p - tc , soprattutto in confronto alla rm , la relativa insensibilit agli infarti lacunari [ 44 ] , lesposizione alle radiazioni ionizzanti , e luso del mdc iodato . 
la somministrazione di mdc iodato non ionico in emergenza , anche senza preventiva valutazione della creatininemia , comunque risultata sicura in una larga serie di pazienti con ictus cerebrale acuto , sottoposti a p - tc , con esclusione dei pazienti con insufficienza renale nota , paraproteinemia nota , trapianto renale , assunzione di farmaci nefrotossici , e / o lunga storia di diabete mellito [ 45 ]  . in conclusione , sebbene la validit delle misurazioni quantitative della p - tc sia messa in discussione dalla loro variabilit legata alla scelta dellaif , al posizionamento delle rois ed agli artefatti da volume parziale [ 46 ] e sebbene ulteriori studi siano necessari per confrontare le misurazioni della p - tc con quelle delle altre metodiche di studio della perfusione cerebrale , i risultati sinora disponibili appaiono incoraggianti riguardo alla selezione di pazienti con estesa area di penombra ischemica , e quindi potenzialmente buoni candidati per la terapia trombolitica , ed inoltre , le misurazioni qualitative relative al controlato , offrendo dati affidabili , restano una valida alternativa , comunque indicativa dello stato della perfusionale cerebrale [ 40 ]  . infine utile qui ricordare che linterpretazione delle mappe di perfusione sicuramente facilitata e resa pi accurata dalla disponibilit di informazioni sullo stato anatomico vascolare intraed extra - cranico . 
con lavvento della tecnologia tc multidetettore , langio - tc , eseguita subito dopo la p - tc , con la somministrazione di un ulteriore bolo di 7090 ml di mdc , permette unaccurata valutazione della perviet delle arterie epiaortiche ed intra - craniche , nonch della presenza di circoli collaterali nelle patologie cerebrovascolari acute e pu avere un ruolo significativo nella selezione dei pazienti con ictus ischemico , ai fini di un corretto 1235 fig . 
9 un piano di scansione orientato lungo il tetto delle orbite , e posizionato circa 2 cm cranialmente a queste , consente la visualizzazione , nelle due fette di 10 mm , di una rappresentazione dei tre territori vascolari sopratentoriali : il territorio dellarteria cerebrale anteriore , della media e della posteriore . contrast material , even without preliminary serum creatinine assessment , proved to be safe in a large series of patients with acute cerebral stroke studied by emergency p - ct , after exclusion of those with known renal failure , known paraproteinaemia , kidney transplant , use of nephrotoxic drugs or a long - standing history of diabetes mellitus [ 45 ]  . in conclusion , although the validity of the quantitative measurements of p - ct has been questioned owing to variability related to aif choice , roi positioning and partialvolume artefacts [ 46 ] ; and although further studies are needed to compare p - ct measurements with those provided by other techniques for the study of brain perfusion , encouraging results have been obtained with regard to the selection of patients with an extensive area of ischaemic penumbra and therefore potential candidates for thrombolytic therapy . 
in addition , qualitative measurements of the contralateral side provide reliable data and offer a valuable alternative that is at any rate indicative of the state of cerebral perfusion [ 40 ]  . finally , it is useful to remember that the interpretation of perfusion maps is definitely facilitated and made more accurate by the availability of information on the state of the intraand extracranial vascular anatomy . 
with the advent of mdct technology , ct angiography , performed with the administration of an additional bolus of 7090 ml of contrast immediately after p - ct , allows accurate assessment of the patency of the epiaortic and intracranial arteries and of the presence of collateral circulations in acute cerebrovascular disease . 
in a context of acute cerebrovascular disease , p - ct combined with ct angiography therefore provides a rapid , efficient and practical tool for identifying the cause , extent and pathophysiology of ischaemia , nd for optimising treatment decisions . chronic ischaemic cerebral disease ( vascular reserve ) in patients with chronic cerebral ischaemia caused by stenosis of the intracranial arteries or epiaortic vessels , it is neca . 
nel contesto della patologia cerebro - vascolare acuta , quindi , la p - tc , combinata con langio - tc , rappresenta una soluzione rapida , efficiente e pratica per diagnosticare leziologia , lestensione e la fisiopatologia dellischemia , cos da ottimizzare la scelta terapeutica . patologia cerebrale ischemica cronica ( riserva vascolare ) nei pazienti con ischemia cerebrale cronica causata da stenosi arteriose intra - craniche o dei vasi epi - aortici , necessario distinguere le condizioni di stabile compenso emodinamico , dalle situazioni in cui il compenso instabile , ed il parenchima cerebrale sottoposto ad uno stress emodinamico e metabolico [ 48 ]  . 
tenendo presente il principio del volume centrale ( cbf = cbv / mtt ) , tipicamente , una stenosi arteriosa emodinamicamente significativa induce un prolungamento del mtt che innesca a sua volta i meccanismi dellautoregolazione cerebrale , con conseguente vasodilatazione , riflessa dallincremento del cbv , con cbf normale o lievemente diminuito . 
questo quadro perfusionale tipico per non fornisce informazioni sulla gravit dellipoperfusione , n sulle capacit residue del circolo cerebrale di adattarsi ad ulteriori modificazioni emodinamiche , ovvero sullesistenza di una riserva cerebro - vascolare . 
la valutazione della riserva cerebro - vascolare si pu ottenere osservando come la perfusione cerebrale reagisce in risposta ad uno stress emodinamico , appositamente provocato mediante somministrazione di un agente vasoattivo . 
i pazienti che hanno esaurito la riserva cerebro - vascolare presentano gi in condizioni di base vasodilatazione massima nelle aree ipoperfuse e non sono quindi in grado di rispondere allo stress emodinamico indotto dallacetazolamide . 
si ritiene che tali pazienti siano a rischio elevato di infarto cerebrale e possano beneficiare di interventi di rivascolarizzazione per aumentare il cbf nelle aree ipoperfuse [ 48 ]  . 
di 1000 mg di acetazolamide pu individuare i pazienti a rischio di infarto tra i portatori di stenosi arteriose epi - aortiche o intra - craniche [ 48 ]  . 
dopo la somministrazione di acetazolamide un incremento del cbf pari al 20%40% rispetto alle condizioni di base considerato normale , un incremento di meno del 5% considerato indicativo di insufficienza emodinamica , mentre la riduzione paradossa del cbf rispetto alla condizione di base segno di furto vascolare , indicativo di tessuto ad alto rischio di infarto [ 49 ]  . 
lacetazolamide generalmente ben tollerata ; sono stati descritti effetti collaterali lievi quali parestesie e cefalea e sebbene siano stati riportati casi di attacchi ischemici transitori , leventuale ischemia indotta sempre stata reversibile [ 48 ]  . 
10 computed tomography angiography ( cta ) , used to complement perfusion ct in this patient with acute right hemiplegia and aphasia , clearly shows left m1 occlusion ( red arrow on exam at 2.5 h ) , which is the cause of the perfusion abnormalities visible on the colour map . 
10 langio - tc cerebrale , esame complementare alla perfusione - tc , dimostra chiaramente , in questo paziente con esordio acuto di emiplegia destra ed afasia , locclusione del tratto m1 dellarteria cerebrale media di sinistra ( freccia rossa nellesame a 2 , 5 h ) , responsabile delle alterazioni perfusionali evidenziate dalla mappa colore . 
il controllo angio - tc a 24 h di distanza , dopo trattamento fibrinolitico , dimostra la ricanalizzazione del vaso ( freccia rossa )  . essary to distinguish between situations of stable haemodynamic compensation and those in which compensation is unstable and the brain parenchyma is subject to haemodynamic and metabolic stress [ 48 ]  . 
bearing in mind the central volume theorem ( cbf = cbv / mtt ) , a haemodynamically significant arterial stenosis will typically result in a prolonged mtt , which in turn will trigger cerebral autoregulation mechanisms , with consequent vasodilatation reflected by an increase in cbv , with normal or slightly decreased cbf . 
this typical perfusion pattern does not , however , give information on the severity of hypoperfusion or on the residual capacity of the cerebral circulation to adjust to further haemodynamic changes in other words , on the existence of a cerebrovascular reserve . 
patients who have exhausted the cerebrovascular reserve show maximal vasodilatation in the hypoperfused areas already at baseline and are therefore unable to respond to the haemodynamic stress induced by acetazolamide . these patients are believed to be at high risk for cerebral infarction and to benefit from revascularisation procedures to increase cbf in hypoperfused areas [ 48 ]  . 
11 perfusion - computed tomography ( p - ct ) before and after right internal carotid endarterectomy.in this patient with mild but progressive left hemisyndrome , ct angiography and p - ct ( upper row ) show severe right internal carotid stenosis causing hypoperfusion of the whole right cerebral hemisphere ( there is a foetal origin of the right posterior cerebral artery , not shown in the figure )  . 
lo studio angio - tc e p - tc ( fila superiore ) , in questo paziente con emisindrome sn lieve ma ingravescente , mostra stenosi serrata del bulbo carotideo destro , cui si associa ipoperfusione di gran parte dellemisfero cerebrale destro ( il paziente portatore di unorigine fetale dellarteria cerebrale posteriore destra , rifornita per via comunicante posteriore ; non mostrata nella figura ) , testimoniata dal prolungamento del mtt , dalla riduzione del cbf e dal lieve aumento del cbv , espressione dei meccanismi di autoregolazione . 
il controllo angio - tc e p - tc ( fila inferiore ) eseguito tre giorni dopo lintervento di endoarterectomia carotidea destra documenta la ricostituzione del lume vascolare e la risoluzione del deficit perfusionale emisferico destro . those with stenosis of the epiaortic or intracranial arteries [ 48 ]  . 
an increase less than 5% is considered indicative of haemodynamic insufficiency , whereas a paradoxical reduction of cbf relative to baseline is a sign of vascular shunting and thus of tissue at a high risk of infarction [ 49 ]  . 
acetazolamide is generally well tolerated ; the reported side effects are mild , such as paraesthesia and headache , and although there have been cases of transient ischaemic attacks , the induced ischaemia was always reversible [ 48 ]  . 
angiographic evidence of vasospasm is present in 60%80% of patients with sah , whereas 30% of patients present symptoms of vasospasm , and half of these develop cerebral infarction [ 51 ]  . 
transcranial doppler ultrasound is the most emorragia sub - aracnoidea e vasospasmo il vasospasmo una complicanza frequente dellemorragia sub - aracnoidea ( esa ) nella fase subacuta precoce [ 6 ]  . levidenza angiografica di vasospasmo presente nel 60%80% dei pazienti con esa , il 30% ne presenta i sintomi , e la met di questi sviluppa un infarto cerebrale [ 51 ]  . leco - doppler transcranico la modalit pi usata per il follow - up non invasivo in questi pazienti , per guidare le scelte terapeutiche e controllarne lefficacia , ma , oltre ad essere operatore dipendente , non offre misurazioni quantitative a livello tissutale ed gravata da scarsa specificit [ 52 ]  . 
anche se non sono ancora disponibili studi in grado di fornire valori di soglia dei parametri di perfusione , la misurazione del cbf , cbv e mtt con p - tc , associata a studi anatomici vascolari con angio - tc , potrebbe rappresentare un utile strumento diagnostico per il follow - up non invasivo dei pazienti con vasospasmo conseguente ad esa [ 6 ] , fornendo informazioni utili al trattamento medico ed anche alla scelta della tempistica chirurgica . trauma cranico la predizione della prognosi nei pazienti con trauma cranico severo rimane un compito complesso e controverso . 
however , it is operator dependent , unable to provide quantitative measurements at the tissue level and suffers from limited specificity [ 52 ]  . even though no study has yet been able to provide threshold values for the perfusion parameters , p - ct measurement of cbf , cbv and mtt , combined with vascular anatomy studies with ct angiography , might represent a valuable diagnostic tool for the noninvasive follow - up of patients with sah - related vasospasm [ 6 ] , as it provides information useful for medical management of patients and for choosing the best timing for surgery . head trauma predicting outcomes in patients with severe head trauma remains a complex and controversial issue . 
a finding of cerebral hypoperfusion , in generally hypotensive patients , indicates a loss of cerebrovascular autoregulation and is thought to be a predictor of the development of cerebral oedema , whereas normal or increased perfusion values would indicate a positive outcome [ 54 ]  . brain tumours in the study of brain tumours , there is growing interest in the noninvasive assessment of tumour vascularity [ 55 ]  . 
some brain tumours are characterised by neoangiogenesis and hypervascularity , which result in increased microvascular permeability [ measured as permeability surface area product ( ps ) or as contrast transfer coefficient ( k - trans ) , in ml / 100g per minute ] and increased cbv , due to the presence of numerous tortuous vascular structures , with immature , disrupted or absent bbb [ 56 ]  . 
contrast enhancement , the key diagnostic element in morphological imaging , is a poorly specific finding that in tumours may be caused by bbb abnormalities , hypervascularity , extent of the interstitial space or a combination of these factors . 
if the extreme disruption of microvascular permeability of some tumours causes excessive leakage of contrast material during the first pass of 1238 zionale possiede alta sensibilit nellindividuazione di lesioni intra - craniche che necessitano di intervento neurochirurgico , ma non offre validi elementi di tipo prognostico . 
il riscontro di ipoperfusione cerebrale , in pazienti generalmente ipotesi , indica la perdita dellautoregolazione cerebro - vascolare e sarebbe in grado di predire lo sviluppo di edema cerebrale , mentre valori di perfusione normali o aumentati rappresenterebbero indicatori prognostici positivi [ 54 ]  . tumori intra - cranici nello studio delle neoplasie intra - craniche crescente interesse rivolto alla valutazione non - invasiva della vascolarizzazione tumorale [ 55 ]  . 
alcuni tumori intracranici sono caratterizzati da neo - angiogenesi ed ipervascolarizzazione , che risultano in aumentata permeabilit vascolare ( misurata come permeability surface product ( ps ) o come coefficiente di trasferimento di contrasto ( k - trans ) , in [ ml / 100 g / min ] ) , e incremento del cbv , per la presenza di strutture vascolari pi numerose , tortuose , con barriera emato - encefalica immatura , danneggiata o assente [ 56 ]  . 
il contrastenhancement , elemento diagnostico chiave dellimaging morfologico , un reperto poco specifico , che nei tumori pu essere determinato dallalterazione della bee , dallipervascolarizzazione , dallampiezza dello spazio interstiziale o dalla concomitanza dei suddetti fattori . 
numerosi studi [ 55 , 56 ] dimostrano che nei gliomi , la ps ed il cbv , misurati con tecniche di rm - perfusione ( con sequenze contrast - enhanced t2 * - w , basate sulla suscettibilit magnetica , e contrast - enhanced t1 - w ) , correlano con lindice mitotico , il grading istologico e laggressivit biologica . 
se lestrema alterazione della permeabilit vascolare in alcuni tumori causa uno stravaso eccessivo del mezzo di contrasto gi durante il primo passaggio del bolo , le misurazioni del cbv , per essere accurate , necessitano di appropriate strategie di correzione ( ad esempio procedure di gamma - fitting della curva densit - tempo )  . 
in tali tumori , ipervascolarizzati e con alterata permeabilit , le misurazioni della ps o del k - trans , sembrano essere pi utili , perch correlano pi strettamente con il grado dei glomi . 
inoltre anche la risposta alle terapie anti - angiogenetiche recentemente introdotte , con riduzione della crescita tumorale , trova il suo corrispettivo in una riduzione dei valori di ps [ 57 ]  . 
in this patient with head trauma and left parietal bone fracture , p - ct shows a large area of hypoperfused brain parenchyma in the left temporoparietooccipital region , well beyond the limits of the hypodense contusion documented by enhanced ct . 
in questo paziente con trauma cranico e frattura parietale sinistra lo studio p - tc mostra una vasta area di ipoperfusione temporo - parieto - occipitale sn , caratterizzata da aumentati valori di mtt e ridotti valori di cbf e cbv , estesa ben oltre i limiti della lesione contusiva ipodensa temporo - parietale sinistra , adiacente alla frattura , visibile nellesame tc morfologico . 
in such hypervascular tumours with disrupted permeability , ps or k - trans measurements appear to be more useful , as they correlate more closely with the grade of gliomas . 
however , in the subgroup of highgrade gliomas [ world health organisation ( who ) iii - iv ] , k - trans was directly related to length of survival . 
measurement of bbb permeability by p - ct or p - mri is based on the same mathematical models , the most frequently used of which is the patlak model [ 59 ]  . 
this model describes a method to measure the transfer - rate constant of contrast material from the vessel to the interstitium , through a mathematical comparison ( deconvolution ) between the timedensity curve or a time - signal curve obtained in tumour tiscon la sopravvivenza ; questa evidenza viene spiegata dagli autori come possibile effetto dellaumentata permeabilit vascolare nel tumore , che permetterebbe una migliore penetrazione degli agenti chemioterapici ed anti - angiogenici . 
la misurazione della permeabilit della bee ottenuta con ptc o con p - rm si fonda sulluso degli stessi modelli matematici , tra i quali , uno dei pi usati il modello di patlak [ 59 ]  . 
questo modello descrive un metodo per misurare la costante di trasferimento del mezzo di contrasto dal vaso allinterstizio , operando un processo di confronto matematico ( deconvoluzione ) tra una curva densit - tempo o segnale - tempo rilevata nel tessuto tumorale ( dove presente stravaso di mdc ) ed una curva rilevata nel lume di unarteria di riferimento o aif ( dove si assume non avvenga stravaso di mdc )  . 
le tecniche di imaging di perfusione trovano utilit nello studio dei tumori intra - cranici nel tentativo di facilitare la distinzione tra tumore primitivo e metastatico , nel rendere pi accurato il grading , nella valutazione della risposta alle terapie antiangiogenetiche , e nella diagnosi differenziale tra radionecrosi e recidiva tumorale ; inoltre si sta affermando il ruolo dellimaging perfusionale per la scelta del bersaglio delle procedure bioptiche , scelta basata sulla individuazione delle aree tumorali a maggiore aggressivit 1239 a . 
perfusion - imaging techniques have been found useful in the study of brain tumours to facilitate the distinction between primary or metastatic tumour , make grading more accurate , evaluate response to antiangiogenic agents and differentiate radiation necrosis from tumour recurrence . 
in addition , the role of perfusion imaging is also gaining ground in guiding biopsy procedures , where the biopsy target is chosen based on identification of the most malignant area in a heterogeneous tumour [ 56 ]  . in contrast to p - mri , only a few small studies are available on the use of p - ct in human brain tumours [ 7 , 60 , 61 ]  . the examination is performed using a similar technique to that described for ischaemic disease , and the scan level corresponds to the tumour site . 
cbv and permeability measurements are made by positioning several small rois over the tumour mass , taking care to exclude large vascular structures from the measurements , and the measurements in the rois are compared with those of a mirror area on the contralateral side . 
the most recent scientific data , many of which are still unpublished , suggest that it is the maximum rather than the mean values of cbv and ps in the tumour that correlate with histopathological grading , as is also the case with histological assessment , which assigns a who grade on the basis of the most malignant portion of the tumour . in theory , p - ct could offer several advantages over pmri in terms of spatial resolution , insensitivity to paramagnetic susceptibility artefacts ( in cases with haemorrhage , calcifications , metallic implants ) , linear correlation between contrast concentration and density and quantitative cbv and permeability measurements , even in hypervascular tumours . in practice , however , no published study has compared the results of the two methods on representative series of patients with brain tumours . 
on the other hand , radiation dose , potential toxicity of iodinated contrast material and limited anatomical coverage of p - ct still justify the predominant use of mri , a modality that remains crucial in the morphological imaging of tumours [ 7 ]  . limitations , artefacts and controversies although the ability of p - ct to provide quantitative measurements has been confirmed by comparison with pet , spect and xe - ct , its accuracy has not yet been unquestionably demonstrated , probably as a result of heterogeneous study methodologies adopted by the various authors . 
furthermore , the quantitative measurements are dependent on several variables , such as the software used , bolus dispersion ( caused by too slow an injection rate , insufficient cardiac function , haemodynamically significant arterial stenoses ) , aif selection , partial - volume artefacts , the misleading contribution of 1240 nel contesto delleterogeneit della neoplasia [ 56 ]  . 
 contrariamente a quanto verificatosi per gli studi di rmperfusione , sono disponibili solo pochi e limitati studi sulluso della p - tc nei tumori cerebrali negli uomini [ 7 , 60 , 61 ]  . 
per la misurazione della permeabilit preferibile disporre di curve densit / tempo allequilibrio invece che limitate al primo passaggio del bolo ; quindi oltre i 50 s di scansione , si continuano ad acquisire immagini in modalit cine , per circa 3 min , al ritmo di 1 scansione ogni 15 s . 
le misurazioni del cbv e della permeabilit si effettuano posizionando multiple piccole roi nel contesto della massa tumorale , avendo cura di escludere dalla misurazione le grosse strutture vascolari , e si confrontano ad unarea speculare nel controlato . 
i pi recenti dati scientifici , molti ancora non pubblicati , suggeriscono che pi dei valori medi di cbv e ps nel contesto della lesione tumorale , siano i valori massimi a correlare con il grading istopatologico , cos come accade peraltro per lesame istologico , che assegna il grado who in base alla porzione del tumore a pi alta malignit . in teoria la p - tc potrebbe avere vantaggi rispetto alle tecniche di rm - perfusione , in termini di risoluzione spaziale , insensibilit agli artefatti di suscettibilit paramagnetica ( in casi con emorragia , calcificazioni , impianti metallici ) , correlazione lineare tra concentrazione di mdc e densit , e misurazioni quantitative di cbv e permeabilit , anche in tumori ipervascolari . 
daltra parte , la dose di radiazioni , la potenziale tossicit del mdc iodato , la limitata copertura anatomica , rappresentano fattori che ancora giustificano luso prevalente della rm , metodica comunque irrinunciabile nellimaging morfologico nei tumori [ 7 ]  . limitazioni , artefatti e controversie sebbene la capacit della p - tc di fornire misurazioni quantitative sia stata confermata , come precedentemente detto , da studi comparativi con pet , spect e xe - tc , la sua accuratezza non ancora stata provata in maniera incontrovertibile , probabilmente anche a causa di metodologie di studio non omogenee tra i diversi autori . 
le misurazioni quantitative sono inoltre dipendenti da multiple variabili , quali il software impiegato , la dispersione del bolo ( causata da uniniezione troppo lenta , uninsufficiente funzione cardiaca , stenosi arteriose emodinamicamente significative ) , la scelta dellaif , gli artefatti da volume parziale , lingannevole contributo del liquor e delle strutture vascolari alle misurazioni , il posizionamento delle roi , ed infine le significative differenze perfusionali tra sostanza grigia e sostanza bianca . 
although commercial software packages for analysis of perfusion data are relatively easy to use , operators need to master the issues inherent to the examination and postprocessing procedures and require training in using thedata derived from perfusion studies conducted by expert radiologists have been shown to have good reproducibility [ 62 ] , whereas no study has evaluated reproducibility of data among nonexpert radiologists . 
in patients with ischaemic stroke , thrombolytic therapy , when indicated , should be initiated as soon as possible , so diagnostic imaging needs to be timely , accurate and fast . 
complementation of a conventional ct study of the brain with pct and ct angiography usually requires 10 - 12 min , whereas postprocessing with automatic software takes no longer than 3 min to provide colour - coded parametric maps that can guide the clinical treatment decisions . 
the disadvantage of this small delay in imaging procedures is widely compensated for by the acquisition of diagnostic information of major clinical importance , above all in those patients in the 3to 6 - h time window and those with an unknown time interval from symptom onset of symptoms , who are currently excluded from treatment . 
 as is known , p - ct employs ionising radiation and potentially nephrotoxic , hyperosmolar and allergenic iodinated contrast material , so the use of the technique requires individual clinical assessment , appropriate indications and strategies to contain the radiation dose . 
it is therefore a valuable alternative to other modalities for the measurement of brain perfusion , compared to which it has the advantage of being readily available and accessible even in emergency settings . 
for this reason , p - ct proves most useful in acute ischaemic stroke where , used in combination with ct angiography , it offers a complete overview of the causes of hypoperfusion and its haemodynamic and pathophysiological effects on the brain in a fast , noninvasive manner . 
p - ct is also helpful in patients with other , acute or chronic , cerebrovascular diseases ; in the follow - up of patients with sah ; in preand postoperative assessment of patients undergoing cerebral revascularisation procedures ; and in brain tumours for diagnosis , grading , biopsy guidance and monitoring treatment response . further studies are required to establish the accuracy , reliability and reproducibility of the quantitative measurements , but available data appear encouraging and indicate a major clinical impact . di post - processing e di un periodo di training per il loro uso ; una buona riproducibilit stata dimostrata , nei dati estratti dagli studi di perfusione , tra radiologi esperti [ 62 ] , mentre studi di questo tipo non sono ancora stati condotti per valutare la riproducibilit tra medici non esperti . 
ulteriori svantaggi della p - tc , soprattutto nelle applicazioni che riguardano la patologia ischemica , come gi detto , sono la limitata copertura anatomica e la scarsa sensibilit verso gli infarti lacunari . 
nei pazienti colpiti da ictus ischemico di fondamentale importanza che il trattamento trombolitico sia iniziato , se indicato , il pi rapidamente possibile , ed quindi auspicabile che la fase diagnostica radiologica sia tempestiva , accurata e veloce . 
il completamento di un esame tc convenzionale dellencefalo con lo studio perfusionale e angiotc richiede solitamente 1012 minuti , mentre le procedure di post - processing , con software automatici , richiedono non pi di 3 minuti per ottenere mappe parametriche colore ai fini di decisioni clinico - terapeutiche ; solo valutazioni quantitative accurate , solitamente non necessarie in situazioni di emergenza , richiedono tempi di post - processing pi lunghi . 
lo svantaggio di questo modesto ritardo nelle procedure di imaging di solito ampiamente compensato dallacquisizione di informazioni diagnostiche di grande rilevanza clinica , soprattutto in quei pazienti nella finestra delle 36 ore ed in quelli con intervallo sconosciuto dallinsorgenza dei sintomi , attualmente esclusi dal trattamento . la p - tc , come ovvio , utilizza radiazioni ionizzanti , e mdc iodato potenzialmente nefrotossico , iperosmolare e allergenico , pertanto limpiego di tale metodica necessita di valutazione clinica individualizzata , indicazioni appropriate , e strategie di contenimento della dose di radiazioni . conclusioni in conclusione , la p - tc permette una valutazione quantitativa affidabile e veloce del cbf e del cbv , offrendo cos una visualizzazione diretta dei meccanismi di autoregolazione cerebrale , e ponendosi come valida alternativa alle altre modalit di misurazione della perfusione cerebrale , rispetto alle quali ha il maggior vantaggio di essere una tecnica prontamente disponibile ed accessibile , anche in condizioni di emergenza . 
per tale ragione la p - tc utile soprattutto nella patologia ischemica cerebrale acuta , situazione in cui , con il concomitante impiego dellangio - tc , offre in maniera rapida e non - invasiva , una completa panoramica della causa dellipoperfusione , nonch delle sue ripercussioni emodinamiche e fisiopatologiche sul parenchima cerebrale . 
krestin2 1dipartimento di radiologia e dipartimento cuore , imaging cardiovascolare non invasivo , azienda ospedaliera di parma , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia , universit degli studi di verona , verona , italy 4dibimel , sezione di scienze radiologiche , universit di palermo , palermo , italy 5unit operativa di riabilitazione cardiovascolare , fondazione don gnocchi onlus , parma , italy correspondence to : f . 
cademartiri , imaging cardiovascolare non invasivo , dipartimento di radiologia , azienda ospedaliero - universitaria di parma , via gramsci 14 , i - 43100 parma , italy , tel . : + 39 - 052 - 1703222 , fax : + 39 - 052 - 1703630 , e - mail : filippocademartiri@hotmail.com received : 23 november 2006 / accepted : 19 march 2007 / published online : 13 december 2007 abstract purpose . 
in the 202 consecutive patients , the prevalence of anatomical variants was : left dominant circulation ( 7% ) , absent left main ( 5% ) , presence of intermediate branch ( 17% ) , aortic origin of conus branch ( 13% ) and circumflex origin of sinus node branch ( 15% )  . 
anatomical variants and anomalies of the coronary arteries are quite common and should be known and recognised promptly by the operators . key words 64 - slice ct coronary anatomy coronary artery variants coronary artery anomalies prevalence riassunto obiettivo . 
nei 202 pazienti consecutivi arruolati per lo studio la prevalenza delle varianti anatomiche risultata : dominanza sinistra ( 7% ) , tronco comune assente ( 5% ) , presenza di ramo intermedio ( 17% ) , origine aortica del ramo del cono ( 13% ) , origine dalla circonflessa dellarteria del nodo del seno ( 15% )  . 
le varianti e le anomalie coronariche sono un reperto molto comune che deve quindi essere riconosciuto agevolmente dalloperatore . parole chiave tc multistrato anatomia coronaria varianti delle arterie coronarie anomalie delle arterie coronarie prevalenza introduction introduzione effectively visualising the coronary arteries is a challenge , not only due to their rapid movement during the cardiac cycle , but also because of their small diameter , their tortuous la visualizzazione delle arterie coronarie rappresenta una sfida non solo per il loro rapido movimento durante il ciclo cardiaco , ma anche per il calibro ridotto , il decorso tortuo1117 f . 
recognising coronary artery anomalies is therefore important for correct diagnosis and treatment of patients , whether or not they are affected by atherosclerosis . the literature contains numerous descriptions of coronary artery anomalies based on conventional coronary angiography ( ca ) but still very few based on msct , and the latter are mostly review articles or case reports [ 35 ]  . the introduction of the technique allows a different anatomical approach that could change the perception of these variants . the aim of this study was to describe the prevalence of coronary artery variants and anomalies in a consecutive population of patients studied with ct coronary angiography ( ctca )  . materials and methods two hundred and two consecutive patients ( 146 men , 56 women , mean age 60 11 years , range 2183 ) with suspected coronary artery disease and already scheduled for conventional ca underwent ctca before ca in the context of a validation study of ctca . 
only patients with a sinus rhythm who had never undergone percutaneous angioplasty or bypass surgery and who were capable of holding their breath for 12 s were included in the study . 
the ethics committee in our department approved the study protocol , and all patients provided informed consent . patient preparation patients with a heart rate ( hr ) greater than 65 beats per minute ( bpm ) were administered 45 munutes before examination , in the absence of contraindications , a single oral dose of 100 mg metoprolol tartrate ( selokeen , astrazeneca pharmaceutics )  . 
apparecchiature di tomografia computerizzata multistrato ( tcms ) allo stato dellarte , ovvero a 64 strati , consentono di collocare la valutazione non invasiva delle arterie coronarie nella routine clinica in virt delle elevate prestazioni ed accuratezza della metodica [ 1 , 2 ]  . le anomalie delle arterie coronariche sono presenti alla nascita ma solo una piccola percentuale di esse si rende manifesta nei primi anni di vita . 
gran parte di esse infatti viene scoperta per caso durante langiografia coronarica o rappresenta addirittura solamente un puro reperto autoptico . ci nonostante alcune di esse possono manifestarsi con sintomi come angina pectoris , infarto miocardico , sincope , aritmie pi o meno severe o addirittura arresto cardiaco configurando il quadro di morte improvvisa . 
il riconoscimento di anomalie coronariche importante quindi per una diagnosi appropriata e per il trattamento del paziente , sia esso affetto o meno da malattia aterosclerotica . nella letteratura esistono delle descrizioni delle anomalie coronariche basate sulla ac mentre ne esistono ancora poche basate sulla tcms , peraltro per lo pi costituite da revisioni della letteratura o descrizione di singoli casi particolarmente significativi [ 35 ]  . 
lintroduzione di questa tecnologia consente un diverso approccio anatomico che pu mutare la percezione di queste varianti . pertanto lo scopo di questo lavoro quello di fornire una prevalenza di varianti ed anomalie coronariche in una popolazione consecutiva di pazienti sottoposti ad angiografia coronarica tc ( ac - tc )  . materiali e metodi duecentodue pazienti consecutivi ( 146 maschi , 56 femmine , et media 6011 anni , range 2183 anni ) con sospetta malattia coronarica e gi indirizzati a coronarografia convenzionale ( ac ) sono stati sottoposti ad angiografia coronarica tc ( ac - tc ) preliminarmente allesecuzione della ac nellambito di studi di validazione della metodica . 
solo i pazienti con ritmo sinusale , mai sottoposti ad angioplastica percutanea o ad intervento chirurgico per il posizionamento di by - pass e capaci di trattenere il respiro per almeno 12 secondi , sono stati inclusi nello studio . 
i pazienti nei quali esistevano delle controindicazioni assolute alla somministrazione endovenosa di mezzo di contrasto iodato ( ad esempio allergia nota , insufficienza renale o disordini tiroidei ) sono stati esclusi dallo studio . 
il comitato etico del nostro dipartimento ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . preparazione del paziente ai pazienti con una frequenza cardiaca ( fc ) superiore a 65 battiti per minuto ( bpm ) stata somministrata , 45 minuti prima della scansione , se non presenti delle controindicazioni , una singola dose orale di 100 mg di metoprololo tartrato ( selokeen , astrazeneca pharmaceutics )  . 
the study protocol involved a preliminary acquisition without intravenous iodinated contrast material to quantify coronary artery plaque . the parameters used for the two scans ( a ) quantification of plaque and ( b ) ctca were : 1 . 
images were reconstructed with the following parameters : effective slice thickness 3 mm , reconstruction increment 1.5 mm , field of view ( fov ) 150180 mm , dedicated convolution kernel for the calcium score . the time windows were positioned at 60% of the rr interval 2 . 
number of slices per rotation 322 , slice thickness 0.6 mm , gantry rotation time 330 ms , table feed 3.84 mm / rotation ( pitch 0.2 ) , 120 kv , 900 mas . 
prospective modulation of the x - ray tube was not used . patients were administered 100 ml of iodinated contrast material ( iomeprol , iomeron 400 , bracco , milan , italy ) with an automatic injector at 5 ml / s ( stellant , medrad , pittsburgh , pa , usa ) connected to a 20 - gauge cannula positioned in an antecubital vethe bolus tracking technique was used to optimise enhancement of the coronary arteries ( care bolus , siemens , forchheim , germany )  . 
angiography - scan data were obtained during a single breath - hold ( 912 s )  . dedicated software ( windose , institute of medical physics , erlangen , germany ) was used to calculate the radiation dose during the angiographic scan ( mean value 15.2 msv for women and 21.4 msv for men )  . 
retrospective reconstructions were performed based on the electrocardiogram ( ecg ) signal to obtain an image quality not affected by motion artefacts in the end - diastolic and end - systolic phases . coronary angiography ( ca ) ca was performed within 2 weeks of the ctca . 
cardiac catheterisation and ca were performed with standard protocols , with spider - view projections , right anterior oblique ( rao ) for the left coronary artery and left anterior oblique ( lao ) for the right coronary artery . 
a single observer unaware of the ctca results identified the coronary segments using a 17 - segment modified american heart association classification . data collection and statistical analysis all examinations judged to be of insufficient quality by two observers were excluded from the sample . 
all examinations were analysed on an off - line dedicated workstation using all the available applications ( viewing , 3d , inspace , circulation ) to achieve an accurate assessment . 
the observers obtained multiplanar reconstructions ( mpr ) , curved multiplanar reconstructions ( cmpr ) , maximum intensity projecta per via orale una dose addizionale di 1 mg di lorazepam ( temesta , wyeth - ayerst )  . protocollo di scansione e ricostruzione delle immagini per lo studio mediante tc stato utilizzato uno scanner a 64 strati ( sensation 64 , siemens , forchheim , germania )  . 
numero di strati per rotazione 322 , tempo di rotazione del gantry 330 ms , avanzamento / rotazione 6 mm ( pitch 0 , 2 ) , voltaggio del tubo radiogeno kv 120 , potenza del tubo radiogeno mas 150 . 
le immagini sono state ricostruite con i seguenti parametri : spessore di strato effettivo 3 mm , incremento di ricostruzione 1 , 5 mm , campo di vista ( fov ) 150180 mm , filtro di convoluzione dedicato per il calcium score . 
numero di strati per rotazione 322 , spessore di strato 0 , 6 mm , tempo di rotazione 330 ms , avanzamento per rotazione 3 , 84 mm ( pitch 0 , 2 ) , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 900 mas , spessore di strato effettivo ricostruito 0 , 60 , 75 mm , incremento di ricostruzione 0 , 4 mm , campo di vista ( fov ) 150180 mm , filtro di convoluzione medium - smooth . 
non stata utilizzata la modulazione prospettica del tubo radiogeno . sono stati somministrati 100 ml di mezzo di contrasto iodato ( iomeprol , iomeron 400 , bracco , milano ) alla velocit di 5 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 20 gauge preventivamente posizionata in una vena antecubitale . 
utilizzando un software dedicato ( windose , istituto di fisica medica , erlangen , germania ) stata calcolata la dose di radiazioni ionizzanti alla quale i pazienti sono stati esposti durante la scansione angiografica ( valore medio 15 , 2 msv per le donne e 21 , 4 msv per gli uomini )  . 
sono state effettuare delle ricostruzioni retrospettive basate sul segnale ecg per ottenere una qualit dellimmagine priva di artefatti da movimento in fase telediastolica e tele - sistolica . angiografia coronarica ( ac ) lac stata eseguita entro 2 settimane dallac - tc . 
la tecnica di cateterizzazione cardiaca e lesecuzione dellangiografia coronarica sono state eseguite seguendo i protocolli standardizzati , ottenendo in particolare le proiezioni spider view , oad per la arteria coronaria sinistra e oas per larteria coronaria destra . 
the same observers also assessed the presence of coronary anomalies on the basis of the type of origin and course , whether they were intrinsic to the coronary itself , or terminal . 
the proximal tract of the rca was the origin of the right conus branch in 59% of cases and the origin of the sinuatrial nodal branch in 64% of cases . 
the dellac - tc , ha identificato i segmenti coronarici utilizzando una classificazione in 17 segmenti modificata rispetto a quella fornita dallamerican heart association . raccolta dati ed analisi statistica due osservatori in consenso hanno escluso dal campione tutti gli esami la cui qualit stata giudicata insufficiente da entrambi i lettori . 
tutti gli esami sono stati analizzati su piattaforma di lavoro dedicata off - line utilizzando tutte le applicazioni disponibili ( viewing , 3d , inspace , circulation ) per raggiungere una valutazione accurata . 
gli stessi osservatori hanno infine valutato in consenso anche la presenza di anomalie coronariche sulla base della tipologia : di origine e decorso , intrinseche alla coronaria stessa , di terminazione . 
i dati sono stati espressi come prevalenze in numero assoluto e percentuale sul totale dei reperti descritti . risultati gli esami sono risultati tutti di qualit diagnostica e adatti alla valutazione . table 1 main anatomical variants of the coronary tree tabella 1 principali varianti anatomiche dellalbero coronarico main anatomical variants type principali varianti anatomiche tipo coronary dominance origin of the conus branch artery origin of the sinus node artery pda variants lm lenght intermediate branch number of diagonal branches number of marginal branches right , left , mixed rca ; rca ostium ; aorta rca ; cx ; both pathways are present early pda ; double 12 cm ; < 1cm ; > 2cm single or double 12 , > 2 12 , > 2 dominanza coronarica origine arteria del cono della polmonare origine arteria del nodo del seno varianti adp lunghezza del tcs presenza di un ramo intermedio numero di rami diagonali numero di rami marginali destra ; sinistra ; bilanciata acd ; ostio acd ; aorta acd ; acx ; entrambe le vie presenti emergenza precoce ; doppia adp 12 cm ; < 1 cm ; > 2 cm singolo o doppio 12 , > 2 12 , > 2 rca , right coronary artery ; cx , circumflex artery ; lm , left main ; pda , posterior descending artery acd , arteria coronarica destra ; acx , arteria circonflessa ; tcs , tronco comune sinistro ; adp , arteria discendente posteriore 1120 f . 
i rami settali sono stati visualizzati nell89% dei pazienti . analisi delle anomalie coronariche : le anomalie dellalbero coronarico riscontrate nella nostra popolazione comprendono 51 casi pari al 25% dei pazienti osservati . alcuni pazienti presentano multiple anomalie cos ripartite e riassunte in tabella 4 : 1 . 
anomalie di terminazione delle coronarie con decorso anomalo in 1 paziente ( 0 , 5% )  . discussione la tcms in grado di visualizzare con efficacia lanatomia complessa e variabile delle arterie coronarie sfruttando le tecfig . 
termination anomalies of the coronary arteries with an anomalous course were identified in one patient ( 0.5% ) discussion msct is able to effectively visualise the complex and variable anatomy of the coronary arteries by exploiting postprocessing techniques , thus providing valuable support to interventional cardiologists and heart surgeons [ 615 ]  . 
on the basis of the most recent published data obtained with ca , normal is defined as any morphological characteristic of the coronary circulation observed in more than 1% of a nonselected sample . a normal variant , therefore , is a characteristic observed in more than 1% of the same sample , whereas an anomaly is a condition observed in less than 1% [ 20 ]  . coronary dominance indicates which system of coronary arteries supplies the inferolateral aspect of the left ventricle [ 21 ]  . 
in 80%90% of the population the posterior descending artery ( pda ) is a branch of the rca and runs from the base of the heart to the apex in a mirror image of the lad . 
in right coronary dominance the rca gives rise to a right posterolateral ( rpl ) branch , which crosses the posterior interventricular sulcus and continues on the left side to supply the dorsal aspect of the left ventricle . 
esistono in letteratura numerosi criteri per classificare ed indicare le anomalie coronariche ; basandoci sui dati pi recenti ritrovati nella letteratura , peraltro ottenuti da casistiche di angiografia coronarica ; viene definita normale qualsiasi caratteristica morfologica del circolo coronarico osservata in pi dell1% in un campione non selezionato ; variante normale , una caratteristica osservata in pi dell1% dello stesso campione ; anomalia una condizione osservata in meno dell1% [ 20 ]  . la dominanza coronarica indica quale sistema di vasi coronarici vicaria il flusso sanguigno verso la parete infero - laterale del ventricolo sinistro [ 21 ]  . 
quando la dominanza coronarica del sistema destro la acd d origine un ramo postero - laterale destro ( pld ) , che attraversa il solco interventricolare posteriore e continua sul lato sinistro per la vascolarizzazione della parete dorsale del ventricolo sinistro . il ramo pld pu diventare di importanza notevole quando la acx occlusa , poich pu essere in grado di sostenere la vascolarizzazione della parete postero - inferiore del ventricolo sinistro . 
dai dati ottenuti nella nostra analisi emerge una stretta concordanza con quanto riportato in letteratura , ovvero una prevalenza nella dominanza destra . il primo ramo della acd larteria del cono che decorre sulla superficie antero - laterale del tratto di efflusso del ventricolo destro . 
conventional angiogram ( a ) , volume rendering ( vr ) ( b ) and maximum intensity projection ( mip ) ( c ) images of a right coronary artery ( rca ) arising from the left sinus of valsalva with an interarterial course . 
conventional angiogram ( d ) , vr ( e ) and multiplanar reconstruction ( mpr ) ( f ) images of a left coronary artery arising from the rca with a septal course . 
acc ( g ) , immagini vr ( h ) e cmpr ( i ) di acx con origine dal seno di valsalva destro e decorso retroaortico , sottoposta a stent . nance is mixed with an intermediate vascularisation pattern . data from our analysis show a strong agreement with the data reported in the literature , i.e. 
in una piccola percentuale di casi lacd pu dare origine anche ad un ampio ramo lungo il margine acuto del cuore fino a continuarsi con ladp ( emergenza precoce delladp )  . 
conventional angiogram ( a ) , volume rendering ( vr ) ( b ) and maximum intensity projection ( mip ) images ( c ) displaying an aneurysm of the circumflex artery . 
myocardial bridging of mid - left anterior descending artery displayed by conventional angiogram during systole ( d ) , vr ( e ) and mpr cross - section images ( f )  . 
sometimes , however , the rca can trifurcate at the crux , giving rise to two branches ( double pda ) for the supply of the base of the heart and an rpl branch for the supply of the dorsal aspect of the left ventricle . the length of the main lca is usually 12 cm , whereas lower values are very common and higher values more rare [ 22 ]  . 
the anomalies that prove to be haemodynamically significant , however , can lead to angina pectoris , syncope , arrhythmia , myocardial infarct or sudden death , as well as promote the onset and progression of coronary atherosclerosis or prove responsible for complications and technical difficulties during angioplasty and heart surgery . 
this anomaly could create problems during heart surgery , since the surgeon unaware of its anomalous course could mistakenly cut it . in addition , native coronary arteries are normally positioned at the origin of the aortic arch with an orientation of 120 and 150 , respectively . 
the cases we observed included 1128 zazione della base del cuore , e ad un ramo pld , per la vascolarizzazione della parete dorsale del ventricolo sinistro . la lunghezza del tcs comunemente di circa 12 cm , anche se possono essere riscontrati valori inferiori ( molto frequenti ) o superiori ( pi rari ) [ 22 ]  . 
le anomalie che risultano invece emodinamicamente significative possono indurre angina pectoris , sincope , aritmia , infarto miocardico , morte improvvisa , favorire linsorgenza e la progressione della malattia aterosclerotica coronarica o rendersi responsabili di complicanze e difficolt tecniche durante angioplastica ed interventi di cardiochirurgia . 
il chirurgo , infatti , potrebbe erroneamente reciderla non conoscendone il decorso anomalo . normalmente inoltre le arterie coronarie native sono posizionate allorigine dellarco aortico con un orientamento di 120 e 150 gradi rispettivamente . 
in caso di riposizionamento chirurgico della valvola o di una sua sostituzione importante conoscere questa condizione . alcune anomalie vengono definite anche come maligne proprio per il loro potenziale patologico e sulla base della loro rilevanza clinica ( benigne ; rilevanti correlate ad ischemia miocardia ; severe associate a morte improvvisa ; critiche associate a malattia coronarica ) , facilitandone cos la gestione ed il follow - up clinico [ 25 ]  . 
a questa classificazione si pu sovrapporre una classificazione anatomica che divide le anomalie coronariche sulla base dellorigine ( assenza del tronco comune sinistro , figura 6 , coronaria con origine dallopposto seno coronarico , figura 7 ) , del decorso ( interarterioso , settale e retroaortico , figura 7 ) , dellanatomia intrinseca ( aneurismi , ponti miocardici , figura 8 ) , e della terminazione ( fistole , figura 9 ) [ 4 , 20 ]  . 
tra i casi osservati emergono alcune di queste anomalie : la fistola coronarica una anomalia coronarica in grado di determinare o predisporre ad un evento ischemico miocardico ed a scompenso cardiaco congestizio , in quanto , drenando nelle sezioni cardiache di destra , pu determinare uno shunt sinistrof . 
coronary fistula is a anomaly capable of causing or creating the predisposition for a myocardial ischaemic event and congestive heart failure in that drainage in the right cardiac sections can lead to leftright shunt with volume overload . 
this anomaly in adults is associated with myocardial ischaemia , a higher risk of coronary disease and volume overload . coronary anomalies are a relatively frequent finding in the context of noninvasive coronary diagnostic imaging . knowledge of the characteristics and consequences of different types of anomalies allows the radiologists to judge the finding appropriately . 
nonetheless , it needs to be emphasised that the performance of ctca for suspected coronary anomaly or to exclude its presence should be carefully considered together with the cardiologist to avoid exposing a young patient to an excessive dose of ionising radiation . to date , conventional ca has been the technique of choice for the diagnosis of coronary artery anomalies . 
the diagnosis of coronary artery anomalies is very often established on the basis of the impossibility of finding the coronaries in their normal anatomical position , and therefore of characterising their ostium . in a few short years msct has modified the entire perception of coronary diagnosis by demonstrating the feasibility of a noninvasive approach . 
the complex and tortuous coronary anatomy can be easily depicted with msct . in our case series , we wanted to emphasise the importance of coronary variants and anomalies by demonstrating their prevalence in a broad population of consecutive patients treated at our tertiary referral centre . 
in our experience , the prevalence of coronary artery anomalies was 25% of cases ( 51 / 202 ) , a much higher value than reported in the literature . this can , however , be explained by the fact that the centre where the examinations were performed is a tertiary referral centre for patients with cardiovascular disease . 
in addition , it should be borne in mind that the study population was not made up of a single ethnic group but was , rather , heterogeneous , as it included patients originating from other continents and with a different and currently unknown prevalence of coronary artery anomalies . most of the coronary artery variants encountered had a minimal clinical risk , such as myocardial bridging , which was present in 12.9% of cases , a figure higher than in condestro con sovraccarico di volume . 
nelladulto questa anomalia si pu associare ad ischemia miocardica , ad un pi elevato rischio di malattia coronarica e ad un sovraccarico cardiaco . le anomalie coronariche sono un reperto relativamente frequente nel contesto dellimaging diagnostico non invasivo coronarico . 
langiografia coronarica con tcms consente grazie alle tecniche di post - processing ( mpr , cmpr , mip , vr ) una pi chiara visualizzazione delle anomalie coronariche rispetto allac . 
la ac - tcms stata recentemente considerata come test appropriato per la valutazione di una sospetta anomalia coronarica , al pari della angiografia coronarica mediante risonanza magnetica [ 2 ]  . 
occorre , tuttavia , puntualizzare che lindicazione allesecuzione di una ac - tcms per sospetta anomalia coronarica o per escluderne la presenza deve essere ben ponderata in cooperazione con il cardiologo , al fine di evitare ad un paziente di giovane et uneccessiva esposizione a radiazioni ionizzanti . sino ad oggi , la coronarografia convenzionale ha rappresentato la tecnica di riferimento per la diagnosi delle anomalie coronariche . 
la diagnosi di ac stabilita , molto spesso , sulla base dellimpossibilit di trovare la coronaria nella normale sede anatomica e , quindi , di cateterizzarne lostio . la tomografia computerizzata multistrato ( tcms ) ha modificato in pochi anni lintera percezione della diagnostica coronarica , portando in primo piano la fattibilit di un approccio non invasivo . 
questa metodica , infatti , offre uneccellente risoluzione spaziale con la possibilit di effettuare mpr ( ricostruzioni multiplanari ) , mip ( maximum intensity projections ) e vr ( volume rendering )  . 
la complessa e tortuosa anatomia coronarica pu essere agevolmente dimostrata mediante la tcms . nella casistica presentata abbiamo voluto sottolineare limportanza delle varianti e delle anomalie coronariche dimostrandone la prevalenza in una ampia popolazione di pazienti consecutivi afferenti presso un centro di iii livello . nella nostra esperienza , la prevalenza delle anomalie coronariche del 25% dei casi ( 51 / 202 ) , valore molto superiore a quanto osservato in letteratura , ma spiegabile a causa del fatto che il centro dove sono stati effettuati gli esami rappresenta centro di iii livello , di riferimento per patologie cardiovascolari . 
va tenuto conto del fatto , poi , che la popolazione di studio non rappresenta un solo gruppo etnico ma abbastanza eterogenea , poich coinvolge pazienti originanti da altri continenti e con prevalenze di anomalie coronariche quindi differenti , e attualmente non nota . delle varie varianti la maggioranza hanno scarsa rilevanza clinica , come ad esempio i ponti miocardici , la cui prevalenza risulta essere del 12 , 9% , dato anchesso superiore a 1129 f . 
in contrast , the finding of an anomalous origin or course can be clinically relevant , such as the anomalous origin of the coronary ostium from the opposite coronary sinus ( which manifests as origin in the main lca or of divided origin )  . 
in these cases , the potential compression of a single coronary vessel if it passes between the aorta and the pulmonary artery can cause ischaemia , myocardial infarct and sudden death . quanto riscontrato nelle casistiche angiografiche e pi vicino alle prevalenze evidenziate in studi autoptici [ 27 ] , mentre pu avere rilevanza clnica il reperto di anomalie di origine e decorso , quali ad esempio lanomala origine dellostio coronarico dallopposto seno coronarico ( che si estrinseca come origine in tronco comune oppure origine divisa )  . 
in questi casi la potenziale compressione di un singolo vaso coronarico se passa tra aorta ed arteria polmonare , pu provocare episodi ischemici , infarto miocardico e morte improvvisa . conclusions the anatomical complexity and variability of the coronary circulation benefits from the flexibility of the various postprocessing techniques introduced by ctca and implemented by the use of a 64 - slice scanner with isotropic voxel . 
radiologist training needs to focus on both anatomical and technical features to satisfy the criteria of professional competence and expertise required for the study of such a highly specialised area of diagnostic imaging . ctca is currently capable of providing highly accurate anatomical imaging of the cardiac vessels . 
both the arterial and the venous vessels can be visualised , although with slightly different protocols with regard to the timing of contrast administration . among all the applications requiring knowledge of the anatomy of the cardiac vessels , ctca constitutes the noninvasive diagnostic technique capable of depicting the highest number of coronary segments , particularly the distal segments . 
therefore , in patients affected by coronary artery disease , it is reasonable to expect that ctca , due to its intrinsically fast execution , noninvasiveness and low cost , will become the ideal instrument for assessing patients with a low risk of coronary artery disease and for the follow - up of percutaneous and / or surgical procedures in the coronary vascular area . conclusioni la complessit e la variabilit anatomica del circolo coronarico si giova della flessibilit delle varie metodiche di postprocessing introdotte dalla ac - tcms ed implementate dalluso di scanner a 64 strati con voxel isotropico . 
il training del medico radiologo deve necessariamente focalizzarsi su entrambi gli aspetti , anatomico e tecnico , per soddisfare quei criteri di competenza professionale ed expertise necessari per lapproccio ad un area di imaging altamente specializzata . attualmente la coronarografia tc in grado di fornire un imaging anatomico dei vasi cardiaci con elevata accuratezza . 
sia il comparto arterioso che quello venoso possono essere dimostrati , anche se con protocolli lievemente differenti legati al timing del mdc . in tutte quelle applicazioni nelle quali la conoscenza dellanatomia dei vasi del cuore importante , la coronarografia tc costituisce ad oggi la metodica diagnostica non invasiva in grado di visualizzare il maggior numero di segmenti coronarici ed in particolare anche quelli distali . 
this study was done to evaluate the diagnostic role of enteroclysis with multidetector computed tomography ( mdct ) and single - detector ct ( sdct ) in patients affected by smallbowel crohns disease . 
in comparison with double - contrast enteroclysis , sensitivity , specificity and diagnostic accuracy were 90% , 71% and 89% for sdct and 92% , 83% and 90% for mdct . 
mdct is superior to sdct because it allows a better spatial resolution and improves depiction of the pathological patterns of crohns disease . key words crohns disease ct enteroclysis multidetector ct riassunto obiettivo . 
quarantacinque pazienti sono stati sottoposti ad enteroclisi - tc a singolo detettore ( n = 20 ) o multidetettore ( n = 25 ) previa somministrazione di metilcellulosa tramite sondino naso - digiunale . 
confrontando i dati tc con quelli del clisma del tenue , abbiamo riscontrato valori di sensibilit , specificit ed accuratezza diagnostica rispettivamente del 90% , 71% e 89% con la tcsd e del 92 , 83 e 90% con la tcmd . 
la tcmd da preferire alla tcsd per la sua migliore risoluzione spaziale e perch consente una migliore rappresentazione dei segni patologici di malattia di crohn . parole chiave malattia di crohn tc enteroclisi tc multidetettore introduction introduzione crohns disease is a chronic granulomatous disease that causes transmural inflammation of the small bowel . 
complications ( abscess , fistula , stenosis ) are common and can be seen in over 40% of patients [ 1 ]  . conventional radiology techniques ( small - bowel barium examination , double - contrast enema ) visualise the small la malattia di crohn una malattia granulomatosa cronica che determina infiammazione transmurale dellintestino tenue . 
the added value of computed tomography ( ct ) is that it directly depicts the bowel wall , perienteric fat , mesentery , vessels and lymph nodes , as well as local complications of crohns disease and associated pathological conditions [ 2 ]  . 
the sensitivity of small - bowel ct is not well known and depends mainly on the quality of the study , severity of the inflammation and presence of mesenteric and intraperitoneal abnormalities . the diagnostic approach to small - bowel disease has recently been refined by the advent of spiral ct , which offers better spatial resolution and the possibility of generating multiplanar reconstructions . 
another technique proposed for the study of the small bowel is ct enteroclysis , where contrast material is administered through a nasojejunal tube , and contiguous axial images are obtained after complete distension of the small bowel [ 3 ]  . 
the function of ct enteroclysis is to overcome the individual pitfalls of ct and small - bowel enema and combine the advantages of the two techniques into a single study . 
the theoretical advantage of ct enteroclysis is the ability to simultaneously depict intraluminal , mural and extraintestinal complications of crohns disease [ 2 , 3 ]  . the aim of this study was to evaluate the diagnostic accuracy of ct enteroclysis with singleand multidetector detector techniques in symptomatic patients with a clinical suspicion or firm diagnosis of crohns disease . materials and methods we prospectively and consecutively evaluated 45 patients ( 22 men , 23 women ) aged 2570 years ( mean age 43 years ) presenting with a suspected or known diagnosis of crohns disease on the basis of clinical , laboratory and / or endoscopic findings . 
on the day before the procedure , they took a mixture of a and b sennosides with a cup of tea with sugar at 8 : 00 h , 15 mg of magnesium sulphate in three quarters of a glass of warm water at 17 : 00 h , followed by 3 l of water over the next 45 h ; at 21 : 00 h they had a cup of clear soup and fasted from 21 : 00 h onwards . all patients were intubated with a 12to 16 - fr nasojejunal tube ( create medic co . , yokohama , japan ) introduced under fluoroscopic guidance . 
patients were then taken into the ct room where contrast material ( 2 , 000 ml of 0.5% methylcellulose ) was administered manually with 60 - ml syringes , with care being taken to ensure a constant and continuous injection rate of about two syringes per minute . 
il valore aggiunto della tc quello di permettere la visualizzazione diretta della parete intestinale , del tessuto adiposo periviscerale , del mesentere , dei vasi e dei linfonodi , nonch delle complicanze locali di malattia di crohn e patologie associate [ 2 ]  . 
la sensibilit dello studio tc nelle malattie del tenue non ben conosciuta e si affida principalmente alla qualit dellindagine , alla severit dellinfiammazione e alla presenza di alterazioni mesenteriche ed intraperitoneali . 
lapproccio diagnostico allo studio del piccolo intestino stato negli ultimi anni ulteriormente modificato grazie allo sviluppo della tecnica spirale che ha consentito una migliore risoluzione spaziale e la possibilit di elaborare ricostruzioni multiplanari . 
contemporaneamente , nello studio del tenue stata proposta la tc enteroclisi in cui il mezzo di contrasto ( mdc ) viene somministrato attraverso un sondino naso - digiunale e dopo la totale distensione del piccolo intestino vengono riprese immagini assiali contigue dello stesso [ 3 ]  . 
la funzione di questa indagine quella di supplire alle carenze individuali della tc e del clisma del tenue , quindi di combinare i vantaggi di ciascuna tecnica in ununica metodica di studio . 
il teorico vantaggio della tc enteroclisi la capacit di mostrare contemporaneamente le complicanze intraluminali , murali ed extramurali della malattia di crohn [ 2 , 3 ]  . lo scopo di questo studio valutare laccuratezza diagnostica della tc enteroclisi effettuata con tecnica a singolo detettore e multidetettore in pazienti sintomatici con sospetto clinico o diagnosi certa di malattia di crohn . materiali e metodi sono stati valutati prospettivamente e consecutivamente 45 pazienti ( 22 uomini , 23 donne ) , di et compresa tra 25 e 70 anni ( et media 43 anni )  . 
il giorno prima dellesame i pazienti hanno ingerito alle ore 8 : 00 una miscela di sennosidi a e b con una tazza di t zuccherato e alle 17 : 00 15 mg di solfato di magnesio sciolti in 3 / 4 di un bicchiere di acqua tiepida , seguita dallassunzione di 3 litri di acqua nelle 45 ore successive . 
il digiuno stato rispettato delle 21 : 00 in poi . a tutti i pazienti stato introdotto sotto guida fluoroscopica un sondino naso - digiunale , del calibro 12 - 16 f ( create medic co , yokohama , giappone )  . 
the contrast - enhanced study was acquired 40 s after iv administration of 130150 ml contrast material ( ultravist 370 , schering ag , berlin , germany ) at a flow rate of 3 ml / s . axial images were processed on a computer workstation ( advantage windows , ge medical system ) to obtain 2d coronal and , if necessary , sagittal constructions . 
following ct , the nasojejunal tube was not removed , and after 68 h , all patients underwent a small - bowel barium enema according to the herlinger method [ 4 ] with digital technique . 
all ct images were assessed for the following signs : presence , site and number of abnormal bowel segments , degree of wall thickening , degree of mural enhancement [ hounsfield units ( hu ) ] , target sign , comb sign , perienteric stranding , fistulas , fibrofatty proliferation , lymphadenopathy , abscesses and other signs ( adhesions , incidental findings in the other abdominal organs , benign or malignant neoplasms of the small bowel )  . 
we evaluated small - bowel distension , which was classified according to a 4 - point scale for each segment ( 0 : no distension ; 1 : incomplete distension ; 2 : partial distension ; 3 : complete distension )  . 
the coronal and sagittal reconstructions were compared with the axial images to assess whether they provided additional information . images obtained with the small - bowel enema were checked for the following signs : oedematous folds , erosions , aphthoid and linear ulcers , fistulas , cobblestoning , micronodules , wall thickening , prestenotic dilatations , mesenteric inflammation and other signs ( adhesions , radiological findings suspicious for benign or malignant neoplasm )  . 
the ct and barium enema results were compared with those of retrograde 1190 sondino stata fissata a valle del treiz tramite linsufflazione di aria in un palloncino in modo da prevenire reflussi di mezzo di contrasto nello stomaco . 
i pazienti sono stati quindi condotti in sala tc ove il mezzo di contrasto ( 2000 ml di metilcellulosa allo 0 , 5% ) stato somministrato manualmente usando siringhe da 60 ml . 
abbiamo cercato di ottenere uniniezione costante e continua , circa 2 siringhe al minuto . al fine di evitare spasmi , ottenere unomogenea distensione del piccolo intestino , ridurre il disagio e la tensione addominale stato somministrato ai pazienti un farmaco anticolinergico ( n - butilscopolamina )  . 
abbiamo somministrato 10 mg di farmaco quando il paziente ha cominciato ad avvertire dolore addominale e 10 mg subito prima dellacquisizione delle immagini tc . venti pazienti sono stati studiati con tecnica tc spirale a singolo detettore ( tcsd ) ( prospeed , advantage sx spiral scanner , ge medical system , milwakee , usa ) con i seguenti parametri di acquisizione : collimazione 5 mm , intervallo 8 mm , ricostruzione 4 mm , kv 120 , mas 300 . 
venticinque pazienti sono stati studiati con tc multidetettore a 16 strati ( tcmd ) ( lightspeed pro16 , ge medical system , milwakee , usa ) con i seguenti parametri di scansione : collimazione 1 , 25 mm , velocit di scorrimento del tavolo 13 , 75 mm / rot , kv 120 , mas 500 , pitch 1 , 375 , tempo di rotazione 0 , 6 s . al termine dellinfusione di metilcellulosa lesame tc stato eseguito prima e durante la somministrazione di mdc iodato ev . 
nei pazienti in cui allesame preliminare senza mdc iodato veniva riscontrata una inadeguata distensione del piccolo intestino abbiamo somministrato altri 200250 ml di metilcellulosa prima di procedere allo studio tc con mdc ev . 
questultimo stato acquisito 40 secondi dopo la somministrazione ev di 130150 ml di mezzo di contrasto ( ultravist 370 , schering ag , berlino , germania ) iniettato alla velocit di 3 ml / s . con una computer workstation ( advantage windows , ge medical system ) le immagini assiali sono state rielaborate con ricostruzioni 2d , coronali ed eventualmente sagittali . 
il sondino non stato rimosso al termine dellesame tc e dopo 68 ore tutti i pazienti sono stati studiati con clisma del tenue effettuato secondo il metodo di herlinger [ 4 ] con tecnica digitale . 
sono stati somministrati 200250 ml di una sospensione di solfato di bario ( prontobario 60% , bracco , milano , italia ) seguiti dallinfusione di 10002000 ml ( in media 1200 ml ) allo 0 , 5% di metilcellulosa . 
sono stati eseguiti radiogrammi nelle proiezioni postero - anteriore , antero - posteriore , con e senza compressione delle anse . i risultati dello studio tc e del clisma del tenue sono stati confrontati e valutati da due radiologi esperti in radiologia gastroenterologica . 
abbiamo anche valutato la distensione delle anse del piccolo intestino che per ciascun segmento stata classificata con una scala di 4 punti ( 0 : distensione assente ; 1 : distensione incompleta ; 2 : distensione parziale ; 3 : distensione completa )  . 
le ricostruzioni coronali e sagittali sono state confrontate con le immagini assiali ed abbiamo valutato le eventuali informazioni aggiuntive da esse ottenibili . le immagini ottenute con clisma del tenue sono state analizzate ricercando i seguenti segni : edema delle pliche , erosioni , ulcerazioni aftoidi e lineari , fistole , aspetto ad acciottolato , micronoduli , ispessimenti parietali , dilatazioni prestenotiche , infiammazione mesenterica , altri segni ( aderenze , alterazioni radiologiche sospette per presenza di neoplasia benigna o maligna )  . 
in these loops , wall thickness ranged from 4 mm to 10 mm ( mean 6.5 mm ) , loop diameter was between 12 and 30 mm ( mean 21 mm ) and lumen diameter between 2 and 18 mm ( mean 8 mm )  . 
complete distension was observed in 27 / 45 ( 61% ) patients in the proximal jejunum , in 35 / 45 ( 77% ) in the distal jejunum , in 40 / 45 ( 88% ) in the proximal ileum , in 39 / 45 table 1 ct signs in patients with crohns disease target sign deep ulcers / sinus tracts perienteric stranding comb sign fibrofatty proliferation stenosis fistulas lymphadenopathy ( > 1 cm ) adhesions abscess segno del bersaglio ulcere profonde / sinus tract strie perienteriche segno del pettine proliferazione fibroadiposa stenosi fistole linfoadenopatie ( > 1 cm ) segni indiretti di aderenze ascesso signs sdct ; number of patients mdct ; number of patients sdct , single - detector computed tomography ; mdct , multidetector computed tomography tabella 1 segni tc nei pazienti con morbo di crohn segni tcsd ; numero pazienti tcmd ; numero pazienti tcsd , tomografia computerizzata a singolo detettore ; tcmd , tomografia computerizzata multidetettore 1191 l.m. 
i valori di densit dei segmenti coinvolti ottenuti dallo studio senza contrasto erano compresi tra 16 e 57 hu e il loro livello di enhancement dopo mdc variava tra 82 e 208 hu . 
il segno del bersaglio stato osservato in 14 pazienti , ulcere profonde / sinus tract in 4 , lo stranding perienterico in 13 , il segno del pettine in 7 . 
una completa distensione stata osservata in 27 / 45 ( 61% ) pazienti nel digiuno prossimale , in 35 / 45 ( 77% ) nel digiuno distale , in 40 / 45 ( 88% ) nellileo prossimale , in 39 / 45 ( 86% ) nellileo distale , in 41 / 45 ( 92% ) nellultima ansa ileale . 
5 tc multidetettore : due anse ileali appaiono a pareti ispessite ( frecce nere ) ; limitrofa ad esse ( freccia bianca ) presente formazione ascessuale . ( 86% ) in the distal ileum and in 41 / 45 ( 92% ) in the last ileal loop . 
the three false positive castable 2 degree of small - bowel distension on ct 0 : absent 1 : incomplete 2 : partial 3 : complete pj , proximal jejunum ; dj , distal jejunum ; pi , proximal ileum ; di , distal ileum ; lil , last ileal loop tabella 2 grado di distensione delle anse dellintestino tenue allesame tc 0 : assente 1 : incompleta 2 : parziale 3 : completa dp , digiuno prossimale ; dd , digiuno distale ; ip , ileo prossimale ; id , ileo distale ; uai , ultima ansa ileale 1193 l.m. 
abbiamo quindi riscontrato valori di sensibilit , specificit ed accuratezza diagnostica del 90% , 71% e 89% con tecnica a singolo detettore e del 92% , 83% e del 90% con tecnica multidetettore . 
essa ha confermato i reperti di normalit in 5 pazienti e un morbo di crohn in 20 , un quadro di ileite aspecifica in 1 , ileite da reflusso in 1 e ileite ischemica in 1 . 
i due terzi dei casi di leite aspecifica , diagnosticati dallenteroclisi tc , presentavano endoscopicamente un quadro compatibile con morbo di crohn . small - bowel ct allows visualisation of the entire organ and , with adequate bowel distension and elimination of respiratory and peristaltic artefacts , enables evaluation of the type and luso della tc nello studio del piccolo intestino consente la visualizzazione dellintero organo e , previa unadeguata didiscussione discussion fig . 
8a , b esempio di migliore visualizzazione dellansa patologica ( frecce ) con tecnica multidetettore ( a ) rispetto alla tecnica a singolo detettore ( b )  . extent of mural enhancement after administration of iv iodinated contrast material . 
as with conventional radiology , accurate bowel cleansing is essential for the quality of the study . because wall thickening is a characteristic feature of crohns disease , optimal bowel distension is essential . 
oral contrast agents have the disadvantage of not perstensione delle anse e leliminazione di artefatti respiratori e dei movimenti peristaltici , la valutazione del tipo e dellestensione dellenhancement parietale dopo somministrazione di mdc iodato ev . 
come nella radiologia tradizionale unaccurata pulizia intestinale il requisito fondamentale per questo tipo di studio . lispessimento parietale rappresenta una caratteristica fondamentale della malattia intestinale e per tale motivo essenziale avere la ottimale distensione delle anse . 
ct enteroclysis combines the advantages of ct with those of small - bowel enema into a single technique [ 5 ]  . in 1992 , klppel [ 6 ] conducted the first study of ct enteroclysis in small - bowel inflammatory diseases , highlighting the techniques diagnostic accuracy in evaluating mucosal abnormalities , mural thickening , fistulas and extraintestinal complications . clinical suspicion guides the choice of contrast material . it is generally preferable to use hypodense contrast agents , except in patients with intestinal obstruction , in whom positive agents are found to be more useful [ 5 , 6 ]  . 
hypodense contrast agents provide better depiction of the inner aspect of the bowel loop , allowing evaluation of the type of mural enhancement after iv administration of iodinated contrast material . 
because no infusion pump was available , we administered the contrast agent manually , trying to ensure a steady and continuous infusion . the examination was carried out after completing the methylcellulose infusion . 
moreover , to ensure uniform loop distension and reduce patient discomfort , we administered two doses of iv smooth - muscle relaxant : the first dose was given before the infusion of approximately 11.5 l of methylcellulose to reduce patient discomfort , the second just il primo requisito quindi per un ottimale studio tc ottenere unadeguata distensione del lume mediante unoculata scelta del tipo e della modalit di somministrazione del mezzo di contrasto . 
i mezzi di contrasto somministrati per via orale hanno lo svantaggio di non fare ottenere una uniforme distensione delle anse del piccolo intestino ; tale problema superato con lutilizzo dellenteroclisi tc , caratterizzata tuttavia da invasivit , tempo e costi maggiori . 
kloppel nel 1992 [ 6 ] ha realizzato il primo studio sulla tc enteroclisi nelle malattie infiammatorie dellintestino tenue mettendo in risalto laccuratezza diagnostica di questa tecnica nella valutazione delle alterazioni della mucosa , dellispessimento parietale , delle fistole e delle complicanze extra - intestinali . 
in tutti i pazienti preferibile lutilizzo di mezzi di contrasto ipodensi eccetto che per i pazienti con ostruzione intestinale nei quali un mezzo di contrasto positivo pi utile [ 5 , 6 ]  . 
un mezzo di contrasto ipodenso consente una migliore definizione dellaspetto interno dellansa intestinale , specialmente per valutare il tipo di enhancement parietale dopo la somministrazione di mdc iodato ev [ 7 ]  . 
essa ben conosciuta , sicura , non tossica , largamente utilizzata nello studio tradizionale e non viene assorbita per cui si evita il rischio di emodiluizione ; ha allincirca la stessa densit dellacqua , quindi determina un ottima differenza di contrasto tra il contenuto delle anse intestinali e lenhancement della parete intestinale . 
nei casi in cui le scansioni di base senza mdc iodato documentavano una scarsa distensione delle anse , stata somministrata unulteriore dose di metilcellulosa prima di procedere con linfusione di mdc iodato . 
inoltre , per ottenere unomogenea distensione delle anse e ridurre il disagio al paziente abbiamo somministrato ev due dosi di ipotonizzante : la prima dose stata somministrata dopo linfusione di circa 11 , 5 l di metilcellulosa in modo da ridurre il discomfort del paziente , la seconda subito prima dellesame tc . 
in tal modo abbiamo ottenuto una distensione completa del digiuno prossimale nel 61% dei pazienti , del digiuno distale nel 77% , dellileo prossimale nell88% , dellultima ansa ileale nel 92% . 
anche se la distensione delle anse migliore quando viene usata una pompa peristaltica [ 8 , 9 ] , in accordo con quanto evidenziato in letteratura [ 10 , 12 ] riteniamo possibile ottenere una sufficiente distensione delle anse anche con linfusione manuale del mezzo di contrasto . un altro elemento indispensabile per lo studio tc del morbo di crohn la somministrazione ev del mezzo di contrasto iodato . 
non tutti gli autori sono concordi sul tempo di attesa dopo la somministrazione del mezzo di contrasto iodato : alcuni ritengono utile unacquisizione arteriosa precoce ( 25 s ) [ 8 ] o arteriosa tardiva 1197 l.m. 
10a , b allesame tc a singolo detettore ( a ) evidente ispessimento parietale dellultima ansa ileale ( freccia ) ; nel clisma del tenue ( b ) essa non dissociabile dalle anse vicine . before starting the ct study . 
this enabled us to achieve complete distension of the proximal jejunum in 61% of patients , of the distal jejunum in 77% , of the proximal ileum in 88% and of the last ileal loop in 92% . 
even if loop distension is improved by the use of a peristaltic pump [ 8 , 9 ] , in agreement with the literature [ 10 , 12 ] , we believe adequate bowel distension can also be achieved by manual injection of the contrast agent . another fundamental aspect of the ct study of crohns disease is the iv administration of iodinated contrast material . 
not all authors agree on the timing of the scan after contrast administration : some prefer an early arterial acquisition ( 25 s ) [ 8 ] or late arterial acquisition ( 40 s ) [ 9 , 13 ] , whereas other prefer a portal phase ( 6070 s ) [ 14 ]  . 
in our study we decided to perform a single acquisition 40 s after iv administration of contrast material , because we preferred to study the small - bowel loops in the arterial phase . during acute inflammation , the thickened bowel wall often shows the so - called target sign , characterised by the alternation of concentric highand low - attenuation rings , on postcontrast images . 
the target sign was originally attributed to crohns disease but is now regarded as a nonspecific sign [ 14 ] ; the differential diagnosis includes crohns disease , ischaemia , infectious enteritis , actinic enteritis , vasculitis and graft - versus - host dis1198 ( 40 s ) [ 9 , 13 ] , altri prediligono una fase portale ( 6070 s ) [ 14 ]  . 
noi abbiamo deciso di realizzare una singola acquisizione a 40 s dalla somministrazione ev di mdc , poich abbiamo preferito effettuare uno studio delle anse dellintestino tenue in fase arteriosa . quando presente uninfiammazione acuta , la parete intestinale ispessita spesso mostra dopo iniezione endovena del mdc iodato il cosiddetto segno del bersaglio ( target sign ) caratterizzato dallalternanza di anelli concentrici ad alta e bassa densit . 
laspetto a bersaglio era originariamente attribuito al morbo di crohn , ma oggi si ritiene essere un segno aspecifico [ 14 ] ; la diagnosi differenziale include : malattia di crohn , ischemia , enteriti infettive , enteriti attiniche , vasculiti e grast - versushost - disease . 
il segno del pettine ( comb sign ) si evidenzia come una ipervascolarizzazione del mesentere coinvolto che si manifesta sotto forma di dilatazione arteriosa mesenterica , tortuosit , prominenza e dilatazione dei vasi retti [ 14 ]  . 
tale segno stato osservato in 7 pazienti del nostro studio . nonostante gli sviluppi tecnologici , per la nostra esperienza ancora utile la combinazione dello studio tc enteroclisi con il tradizionale clisma del tenue . 
the comb sign reflects hypervascularity of the involved mesentery , which manifests as mesenteric arterial dilatation , tortuosity , prominence and dilatation of the vasa recta [ 14 ]  . 
the comb sign was seen in seven patients in our study . despite technological advances , we find the combination of ct enteroclysis and conventional barium enema to be still useful , as it produces a better diagnostic definition , allowing identification of false positive and false negative cases on ct [ 9 , 16 , 17 ]  . 
moreover , the conventional study proved superior in characterising mucosal abnormalities , especially in the early phase , and complemented the ct findings , allowing for a diagnosis of reflux ileitis and ischaemic ileitis in two cases . 
abscesses were present in 2 / 45 patients , fistulas in 3 / 45 , perienteric stranding in 13 / 45 and fibrofatty proliferation in 5 / 45 . with regard to the comparison between the two ct techniques , it should be stressed that , as expected , the multidetector technique allowed for shorter scan times and reduced respiratory artefacts and patient discomfort while providing better spatial resolution and better depiction of pathological patterns . 
however , sensitivity , specificity and diagnostic accuracy of the two techniques are similar ( table 4 ) , as a result of the fact that both techniques are able to demonstrate the typical signs of disease , even though their visualisation is better with the multidetector technique . 
in our study , mpr did not , however , reveal any abnormalities that had not already been demonstrated in the axial scans , although they significantly increased our confidence in image interpretation and helped us better evaluate the longitudinal extent of intestinal involvement , as previously reported in the literature [ 19 , 21 ]  . 
the coronal images , especially with those obtained with the multidetector technique , were particularly well accepted by the clinicians and surgeons , given their familiarity with frontal views . even though crohns disease is the most common disease of the small bowel , we should not forget that ct enteroclysis is able to detect other pathological conditions , such as neoplasms . 
in our study , we found only two cases of carcinoid tumour , probably as a result of the preliminary clinical selection of patients with suspected or known crohns disease . 
 in conclusion , we believe that mdct should be preferred to sdct owing to its better spatial resolution and because it ne produce una migliore definizione diagnostica permettendo di identificare i casi tc falsi positivi e falsi negativi [ 9 , 16 , 17 ]  . 
nel nostro studio , infatti , 3 falsi positivi erano dovuti a scarsa distensione delle anse e 4 falsi negativi erano dovuti ad una fase iniziale di malattia e / o localizzazione prossimale di crohn . 
ascessi erano presenti in 2 / 45 pazienti , fistole in 3 / 45 , stranding perienterico in 13 / 45 , proliferazione fibroadiposa in 5 / 45 . per quanto riguarda il confronto tra le due tecniche tc vogliamo sottolineare che , come atteso , la tecnica multidetettore ha ridotto i tempi di scansione , gli artefatti respiratori e il disagio per il paziente , permettendo una migliore risoluzione spaziale e realizzando una migliore rappresentazione degli elementi patologici . 
tale dato in accordo con la letteratura [ 1517 , 19 , 20 ] .tuttavia i valori di sensibilit , specificit ed accuratezza diagnostica sono simili con le due metodiche ( tabella 4 )  . 
tuttavia le ricostruzioni multiplanari non hanno nel nostro studio mostrato alcuna alterazione che non fosse gi stata documentata nelle scansioni assiali anche se hanno migliorato significativamente la nostra confidenza nella interpretazione delle immagini e ci hanno aiutato a valutare meglio lestensione longitudinale dellinteressamento intestinale , come gi riportato in letteratura [ 19 , 21 ]  . 
le immagini coronali sono state inoltre particolarmente apprezzate dai clinici e dai chirurghi data la loro familiarit con esse , in particolare quelle ottenute con tecnica multidetettore . anche se il morbo di crohn la patologia dellintestino tenue pi frequente , non dobbiamo dimenticare che la tc enteroclisi in grado di documentare altre condizioni patologiche , come ad esempio le neoplasie . 
nel nostro studio abbiamo riscontrato solo due casi di carcinoide verosimilmente in rapporto alla preliminare selezione clinica che ci ha fatto studiare prevalentemente pazienti con sospetto o noto morbo di crohn . in conclusione noi riteniamo che la tcmd enteroclisi sia da preferire alla tcsd per la sua migliore risoluzione spaziale e perch consente una migliore rappresentazione dei segni patologici di malattia di crohn . 
in our opinion , in selected patients ( nondiagnostic ct , negative ct with a strong clinical suspicion of small bowel disease ) , ct findings still need to be combined with those from small - bowel enema to obtain all the information needed for a correct diagnosis and for planning treatment in patients with crohns disease . 
the ultimate goal is to improve visualisation of early lesions with ct in order to obtain all the necessary information for correct patient evaluation with a single examination . nione i dati tc ancora necessitano in pazienti selezionati ( tc non diagnostica , tc negativa con quadro clinico altamente suggestivo di patologia dellintestino tenue ) di essere combinati con quelli derivanti dal clisma del tenue in modo da ottenere tutte le informazioni necessarie per la corretta diagnosi e la pianificazione terapeutica dei pazienti con malattia di crohn . 
in ct - guided transthoracic needle biopsy , the final diagnosis and lesion size affect diagnostic accuracy : benign lung lesions and lesions smaller than 1.5 cm or larger than 5.0 cm in diameter provide lower diagnostic yield . key words lung biopsy computed tomography ( ct ) guidance accuracy riassunto obiettivo . 
i valori di sensibilit , specificit , valore predittivo positivo , valore predittivo negativo ed accuratezza , riferiti ad una diagnosi di malignit , sono risultati rispettivamente del 90 , 2% , 99 , 0% , 99 , 8% , 67 , 3% e 91 , 7% . 
la diagnosi finale ( benignit versus malignit ) e le dimensioni della lesione influenzano laccuratezza diagnostica della metodica : addensamenti polmonari di natura benigna e lesioni con diametro < 1 , 5 cm o > 5 cm sono caratterizzati da livelli minori di accuratezza diagnostica . parole chiave polmone biopsia tomografia vomputerizzata ( tc ) guida accuratezza diagnostica 1142 a.m. 
computed tomography ( ct ) - guided needle lung biopsy was first reported by haaga and alfidi in 1976 [ 5 ] , and since then , the techniques excellent efficacy and accuracy and acceptable morbidity and mortality rates ( 0.07% , or one death every 1 , 429 procedures ) have been widely demonstrated [ 616 ]  . 
whether carried out with fine - needle - aspiration cytology ( fnac ) or core biopsy ( cb ) , the biopsy provides adequate material for cytological or histological examination and , if necessary , for microbiological evaluation [ 1113 , 1721 ]  . 
cb is more sensitive in defining benign lesions and in characterising diffuse or lymphoproliferative diseases of the lung , where the assessment of the tissue architecture is instrumental to the diagnosis ( accuracy > 80% for cb and 50%70% for fnac ) [ 9 , 2225 ]  . 
lesions smaller than 1 cm are easier to sample with fnac [ 19 , 22 , 23 ]  . the reported sensitivity of fnac varies and is positively affected by the presence of the cytopathologist on site during the biopsy procedure [ 26 , 27 ]  . 
immediate cytological assessment increases the techniques sensitivity and reduces the number of inadequate samples and false negative results [ 2628 ] , as the on - site cytopathologist can judge the adequacy , quantity and quality of the sample , suggest the need to repeat the procedure or request cb with histological assessment [ 22 , 26 ]  . several studies have investigated the factors affecting diagnostic accuracy of ct - guided transthoracic needle biopsies . 
it is well established that the most important factor is the final diagnosis , as malignant lesions ( regardless of histological type ) are characterised by greater sensitivity compared with benign masses . 
other variables ( lesion depth , number of passes , cavitations and necrotic centre , morphology , location , radiologists experience , needle diameter and presence of pneumothorax and / or bleeding ) were not found to be significant [ 32 ]  . the purpose of this paper is to present our experience with a large cohort of patients and discuss the results achieved in relation to diagnostic accuracy . 
in particular , we extensively analyse a number of variables ( relating to the patient , the lesion or the procedure ) in an attempt to correlate them to potential influences on diagnostic accuracy and reach a conclusive judgement on the efficacy of the procedure . 
lagobiopsia polmonare tc guidata fu riportata in letteratura per la prima volta nel 1976 da haaga [ 5 ] e da allora numerosi autori ne hanno dimostrato lestrema efficacia ed accuratezza associate ad un accettabile tasso di morbidit e mortalit ( 0 , 07% , ovvero un decesso ogni 1429 manovre effettuate ) [ 616 ]  . 
il prelievo , eseguito tramite aspirazione con ago sottile ( fine needle aspiration citology , fnac ) o con ago tranciante ( core biopsy , cb ) , consente di ottenere , rispettivamente , materiale sufficiente per lesame citologico o istologico ed infine , se necessario , per una valutazione microbiologica [ 1113 , 1721 ]  . 
la cb ha maggiore sensibilit nella definizione delle lesioni benigne e nella caratterizzazione delle malattie polmonari diffuse o linfoproliferative , nelle quali la valutazione dellarchitettura tissutale importante per la diagnosi ( valori di accuratezza > 80% per la cb e tra il 50% ed il 70% per la fnac ) [ 9 , 2225 ]  . 
le lesioni di dimensioni inferiori al centimetro risultano essere pi facilmente campionabili mediante fnac [ 19 , 22 , 23 ]  . la sensibilit della fnac variabile nelle casistiche riportate in letteratura ed positivamente influenzata dalla presenza in sala radiologica del citopatologo al momento del prelievo [ 26 , 27 ]  . 
il citopatologo , infatti , in grado di dare indicazione sulladeguatezza del prelievo , sulla quantit e qualit del materiale campionato , pu suggerirne leventuale ripetizione o richiedere lintegrazione con lesame istologico dopo cb [ 22 , 26 ]  . alcuni autori hanno analizzato le variabili che influenzano laccuratezza diagnostica delle agobiopsie transtoraciche tc guidate . 
da tempo assodato come il pi importante fattore in questo senso sia la diagnosi finale corretta , dato che le lesioni maligne ( indipendentemente dallistotipo ) sono caratterizzate da livelli di sensibilit significativamente maggiori rispetto agli espansi di origine benigna . 
considerando altre variabili , tsukada stato il primo a dimostrare come la graduale riduzione delle dimensioni della lesione conducesse ad un proporzionale decremento nei valori di accuratezza diagnostica [ 13 ]  . 
i risultati di tsukada sono per stati successivamente confermati da yeow che , in una coorte di 649 soggetti , ha riscontrato come sia la diagnosi finale sia le dimensioni della lesione influenzassero il valore di accuratezza [ 20 ]  . 
the study population comprised 154 subjects who underwent surgical resection ( for whom definitive postoperative histological assessment was available ) and nonsurgical patients who had completed at least 12 months of follow - up ( 454 subjects )  . 
the population included 402 men and 206 women , with a mean age of 65.7 years [ ( median 67 ; standard deviation ( sd ) 9.4 years with 95% confidence interval ( ci ) ; range 2987 years )  . 
exclusion criteria were lesions < 5 mm in diameter ( calculated as the mean of the long and short axis ) , significant changes in blood - coagulation profile , contralateral pneumonectomy , patients inability to maintain a lying position and / or to follow verbal or visual instructions and patients refusal to accept the potential risks associated with the procedure and sign the informed consent form . all biopsies were performed according to a standard protocol by the same interventional radiologist ( ac ) under ct guidance with a spiral dual - detector - row scanner . 
after positioning the patient on the ct table in prone , supine or lateral decubitus , depending on lesion location , an initial localisation scan was obtained by acquiring the entire mass on 5mm - thick contiguous transverse sections . 
then , optimal access ( skin entry site and needle path ) was defined on ct images , taking care to sample the lesion away from low - density areas , which are often central and indicative of necrosis [ 13 , 17 , 18 ]  . 
after having established the entry site and chosen the type and length of the needle ( depending on lesion depth and , whenever possible , the shortest route [ 33 ] ) , the needle entry site was anaesthetised ( 2% lidocaine ) , the needle , or the needle guide in the case of cb , positioned and the patient instructed to hold his or her breath . at this point ct scans were obtained to visualise the needle tip in relation to the lesion . 
in particolare verranno estensivamente analizzate alcune variabili ( riferite al paziente , alla lesione od alla procedura ) nel tentativo di correlarle a potenziali influenze sui valori di accuratezza per formulare un giudizio critico conclusivo sulla efficacia della procedura interventistica . materiali e metodi popolazione di studio in un intervallo temporale compreso tra novembre 2002 ed agosto 2005 sono stati consecutivamente sottoposti a procedura interventistica transtoracica tc guidata per laccertamento della diagnosi ( agoaspirazione transtoracica con ago sottile o con ago spinale o biopsia con ago tranciante ) 608 pazienti , per un totale di 612 procedure . 
la coorte in studio ai fini della formulazione di un giudizio di accuratezza della metodica ha compreso tutti i 154 soggetti resecati ( per i quali risultata disponibile la valutazione istologica definitiva postoperatoria ) ed i pazienti non chirurgici che avessero conseguito un follow - up non inferiore a 12 mesi ( 454 soggetti )  . la popolazione ha pertanto incluso 402 soggetti di sesso maschile e 206 femminile , con unet media di 65 , 7 anni ( mediana 67 anni ; ds9 , 4 anni con ic 95% ; intervallo 2987 anni )  . 
i pazienti sono afferiti in parte con proposta di prestazione ambulatoriale ed in parte in regime di ricovero ordinario . sono state considerate tutte le lesioni intraparenchimali ( centrali e periferiche ) , ovvero gli espansi circondati da tessuto polmonare areato o a diretto contatto con le strutture ilari e / o la superficie pleurica il cui epicentro cadesse allinterno del polmone ( dimensione media delle lesioni 36 , 8 mm ; mediana 31 , 5 mm ; ds20 , 5 mm con ic 95% ; intervallo 7103 mm )  . protocollo bioptico nessun paziente risultato anamnesticamente positivo per diatesi emorragica o ha presentato alterazioni della crasi ematica e del profilo emocoagulativo . 
i soggetti in trattamento anti - aggregante e / o anticoagulante hanno sospeso tale terapia per un periodo antecedente la biopsia di 7 giorni . sono stati raccolti dal radiologo un breve raccordo anamnestico ed il consenso informato . 
al momento di ogni biopsia , risultata disponibile una precedente tc diagnostica . i criteri di esclusione da noi adottati sono stati : lesioni con diametro ( calcolato sulla media delle dimensioni degli assi maggiore e minore ) < 5 mm ; alterazioni significative dellasa.m. 
biopsies were carried out by needle aspiration with a 21 - gauge fine needle or a 20gauge spinal needle ( with the single needle technique ) , or by core biopsy with an 18 - gauge cutting needle ( and coaxial technique )  . our initial approach in pulmonary nodules always uses a chiba fine needle ( especially for small lesions ) , except in cases of a second attempt after a previous inconclusive procedure . 
this made it possible to have an evaluation of material adequacy and an extemporary general indication about the nature of the lesion within minutes of the procedure [ 2628 ]  . 
in the case of inadequate or insufficient samples for cytology or histology , the biopsy procedure was repeated immediately : in particular , 190 / 612 procedures ( 31.0% ) required more than one sampling ( mean 1.32 samples per procedure ; range 14 )  . to assess possible complications ( pneumothorax , needletrack bleeding ) , postprocedural ct scans were acquired 35 min after the procedure ( time required for the cytopathologist to prepare the slides and judge their adequacy )  . data collection : definition and selection of variables multiple discrete or continuous variables , relating to the patient , the lesion or the procedure , were considered . 
dopo aver posizionato il paziente sul lettino tc in decubito prono , supino o laterale a seconda della localizzazione della lesione , si proceduto ad una prima centratura della lesione attraverso lacquisizione dellintero espanso su sezioni trasverse contigue di 5 mm di spessore . 
successivamente , sulle immagini tc a monitor si pianificata la migliore via di accesso ( come punto di ingresso cutaneo e tragitto dellago ) al fine di campionare la lesione avendo cura di evitare regioni di ipodensit , spesso centrali ed indicative di necrosi , nel suo contesto [ 13 , 17 , 18 ]  . 
dopo aver definito il punto di ingresso dellago e scelto la tipologia e la lunghezza dellago ( a seconda della profondit della lesione e pianificando , ogni qual volta sia stato possibile , il tragitto pi breve [ 33 ] ) si effettuata unanestesia locale in corrispondenza del punto cutaneo di ingresso ( lidocaina 2% ) , quindi si posizionato lago , o lago guida per le biopsie trancianti , chiedendo al paziente di mantenere lapnea . 
per gli espansi di difficile centratura ( 162 / 612 procedure , 26 , 5% del totale ) quali piccoli noduli centrali o integralmente coperti da strutture ossee , lago bioptico stato introdotto nei tessuti molli sino alla superficie pleurica evitandone accuratamente la trasgressione . 
in alcuni casi si effettuato pi di un passaggio pleurico , dal momento che o la lesione - bersaglio non stata raggiunta dalla punta dellago al primo tentativo nonostante i riorientamenti intraparenchimali dellago o , nei prelievi senza ausilio della tecnica coassiale , il materiale risultato inadeguato e si ricorsi ad un nuovo prelievo . 
in particolare , 350 / 612 procedure ( 57 , 2% ) hanno richiesto un solo passaggio pleurico ( media 1.5 passaggi pleurici per procedura ; intervallo 14 )  . 
il prelievo stato effettuato tramite agoaspirazione con ago sottile 21 gauge ( g ) o con ago spinale 20 g ( con tecnica ad ago singolo ) , o biopsia con ago tranciante 18 g ( utilizzando la tecnica coassiale )  . 
 per i noduli polmonari sempre preferito da noi un iniziale approccio con ago sottile di chiba ( soprattutto nelle lesioni di piccole dimensioni ) , tranne nei casi di un secondo tentativo dopo un precedente prelievo non conclusivo . nellevenienza della ripetizione iterativa viene considerata la possibilit di utilizzare un ago di calibro maggiore ( spinale ) od un tranciante . 
final diagnoses were based on the surgical outcomes ( surgical patients ) or the imaging data and clinical - radiological follow - up for a period of at least 12 months ( response to first - line chemotherapy or antibiotic treatment designed on the basis of the biopsy ; unchanged imaging findings in the absence of treatment )  . 
in relation to malignant diagnoses , we considered : true positives for malignancy : all cases classified as malignant at transthoracic needle biopsy and confirmed by histology of the surgical specimen ; cytohistology of an additional biopsy from a distant metastatic lesion ; imaging evidence ( radiology or nuclear medicine ) of distant metastases ; partial or complete response to first - line chemotherapy ; clinical course . 
in surgical cases , we assessed the reliability of the needle biopsy in providing precise characterisation with specific histological type a negative finding ( benign lesion ) was classified as a true negative for malignancy at fnac or cb when its benign nature was confirmed by subsequent surgery or biopsy or when the lesion appeared stable , smaller or had totally disappeared at follow - up ct ( 12 - month follow - up ) in an untreated patient or a patient treated with appropriate antibiotic , but not antineoplastic , therapy [ 18 , 22 ] false positives for malignancy : all cases with a positive biopsy not confirmed by surgery false negatives for malignancy : all cases with a negative ( benign at fnac / cb ) or indeterminate result ( absence of cellular atypia , presence of atypical cells not otherwise specified , presence of nonspecific or granulomatous inflammatory reaction , insufficient material or blood contamination ) at transthoracic needle biopsy with positive surgical outcome or disease progression at follow - up imaging . the quality of each sample obtained by fine - needle transthoracic biopsy was scored from 0 to 3 , according to the following criteria : 0 = slides containing exclusively blood components ( blood contamination ) without epithelial cells ; 1 = finding of nonspecific benign cells ( inflammatory ; type i and ii pneumocytes ; atypical cells not otherwise specified ) ; 2 = presence of morphologically malignant cells , without characterisation of histological type or without differentiation between small - cell or non - small - cell cancer ; 3 = slides containing benign or malignant cells with definite histological characterisation . 
samples with scores 0 , 1 and 2 ( when justified by inability to differentiate between small - cell and non - small - cell cancer ) were considered nondiagnostic and therefore classed as false negatives in relation to the final diagnosis . 
samples with scores of 2 and 3 were considered adequate . size 1146 the dimensions of each lesion were measured on screen using a dedicated programme ( electronic callipers ) , in the two maximum orthogonal axial diameters , on the preliminary localisation scan reconstructed from the raw data with adequate window and level settings for lungs . 
in tutti i casi stato utilizzato una lunghezza dello scatto della pistola bioptica pari a 3 , 3 cm . la presenza del citopatologo in sala radiologica , essenziale nei prelievi citoaspirativi , ha costituito elemento caratterizzante tutte le procedure . 
in caso di materiale inadeguato od insufficiente ad unanalisi citologica od istologica si provveduto alla immediata ripetizione del prelievo : in particolare 190 / 612 procedure ( 31 , 0% ) hanno richiesto pi di un prelievo ( media 1 , 32 campioni per procedura con intervallo 14 )  . per valutare linsorgenza di complicanze ( pneumotorace , soffusione emorragica lungo il tragitto dellago ) sono state acquisite , circa 35 minuti dopo il prelievo ( nel tempo richiesto dal citopatologo per preparare gli strisci e dare giudizio di idoneit ) , scansioni tc di controllo . raccolta dei dati : definizione e selezione delle variabili sono state considerate molteplici variabili , a valore discreto o continuo , riferite al paziente , alla lesione od alla stessa manovra interventistica . 
per entrambe le categorie sono stati calcolati , attraverso la costruzione di tabelle 22 , i livelli di accuratezza ( sensibilit , specificit , valore predittivo positivo e negativo , proporzione di falsi positivi e negativi , accuratezza globale della metodica ) correlando il risultato della biopsia transtoracica con la diagnosi finale . 
la diagnosi definitiva stata ottenuta attraverso lanalisi del dato chirurgico ( per i pazienti resecati ) , dei dati di imaging e del follow - up clinico / radiologico per un periodo non inferiore a 12 mesi ( risposta a trattamenti chemioterapici di i linea o a trattamenti antibiotici impostati sulla base del risultato bioptico transtoracico ; stazionariet radiologica dei reperti in assenza di terapia )  . 
a questo proposito sono stati considerati , in rapporto alle diagnosi maligne : veri positivi per malignit i casi classificati maligni allagobiopsia transtoracica e confermati : dal dato istologico sul pezzo operatorio ; dal dato cito - istologico derivante da una ulteriore aggressione bioptica di una lesione metastatica a distanza ; dallevidenza strumentale ( indagini radiologiche e di medicina nucleare ) di metastasi a distanza ; dalla risposta parziale o completa a trattamenti chemioterapici di i linea ; dal decorso clinico . 
nei casi resecati stata valutata laffidabilit dellagobiopsia transtoracica nel fornire una precisa caratterizzazione con specificit di istotipo ; un esito negativo ( ovvero di natura benigna ) stato classificato vero negativo per malignit alla fnac o cb in caso di successiva conferma chirurgica o bioptica o se a.m. 
we recorded data on the presence of single or multiple pulmonary lesions and lobar location specifying possible contact or close proximity to an interlobar fissure , the hilum or major intrapulmonary vessels . 
the depth of the consolidation was defined as the distance between the entry site on the pleural surface and the proximal edge of the lesion , measured along the needle path on lung window settings [ 13 , 32 , 3436 ]  . 
i prelievi con punteggio 0 , 1 e 2 ( se per questi ultimi non stata possibile una differenziazione tra neoplasia a piccole cellule e non ) sono stati considerati non diagnostici e quindi classificati come falsi negativi in rispetto alla diagnosi finale . 
i prelievi con punteggio 2 e 3 sono stati invece considerati adeguati . needle type and calibre dimensioni in all procedures , we used either a single needle ( 21 - gauge chiba needle ; 20 - gauge spinal needle ; 18 - gauge cutting needle with coaxial technique ) or , in the event of multiple biopsies , a consecutive combination of different needles . 
the choice of the type of needle was based on parameters such as lesion size , clinical suspicion ( history , clinical and imaging data ) , operators preferences and the presence of the cytopathologist . 
during each anale dimensioni di ogni lesione sono state misurate a monitor mediante programma dedicato ( calibro elettronico ) , nei due diametri assiali ortogonali massimi , sulle scansioni di centratura preliminari ricostruite dai dati grezzi attraverso adeguata finestra e livello per parenchima polmonare . 
stata quindi calcolata la media aritmetica relativa alle misurazioni ottenute per ciascuna lesione in esame . morfologia e localizzazione le lesioni sono state suddivise in noduli e masse , se caratterizzate da un diametro trasverso massimo < o 30 mm rispettivamente . 
sono state considerate consolidazioni gli infiltrati cuneiformi , di natura fluida o cellulare , a distribuzione segmentaria o lobare , associati o meno a broncogramma aereo . sono stati registrati i dati relativi alla presenza di lesioni polmonari singole o multiple , la localizzazione lobare specificando leventuale contatto o la stretta vicinanza ad una scissura interlobare , allilo o a strutture vascolari intrapolmonari di rilievo . 
la profondit delladdensamento stata considerata quale distanza tra il punto di ingresso della superficie pleurica sino al margine prossimale della lesione , misurata lungo il tragitto dellago su finestra per parenchima polmonare [ 13 , 32 , 3436 ]  . 
the variables of the two groups in each category were correlated . differences between the groups were examined using the nonparametric mann - whitney u test or variance analysis according to kruskal - wallis , when indicated . 
differences between proportions were analysed with pearsons 2 test or students t test . parameters considered significant in determining diagnostic accuracy were further stratified and correlated to accuracy with the aid of contingency graphs and tables . 
a p value < 0.05 was taken as significant in all cases . results in calculating the methods diagnostic accuracy , we considered all 608 patients included in the study : there were 154 surgical patients ( for whom postoperative surgical evaluation was considered the gold standard against which the interventional technique was compared ) there were 454 nonsurgical patients who had completed , as at august 2006 , an imaging , clinical and treatment - response follow - up of at least 12 months ; in these cases the final diagnosis was inferred from the benign or malignant behaviour of the lesion we considered 612 procedures ; the quality of each of the 612 samples was assigned a discrete score from 0 to 3 at the end of each procedure in 435 / 612 procedures ( 71.1% ) , the needle biopsy recovered benign or malignant cells , allowing specific cytohistological characterisation ( score 3 )  . 
of these , 52 were benign , 382 were malignant and only one revealed the presence of a hamartochondroma associated with a primary squamous cell carcinoma of the lung there were 75 / 612 samples ( 12.2% ) that demonstrated definitely malignant cells ( score 2 ) , without providing information on histological type . 
four samples demonstrated the presence of definitely neoplastic cells ( probably epithelial ) without providing discrimination between small - cell and non - small - cell cancer , which is essential for therapy . 
in addition , the only false positive result in our cohort was encountered among these four cases : a suspected carcinoma not otherwise specified ( fnac ) was found at surgery to be an excavated granuloma characterised by severe cellular dysplasia due to previous tuberculous infection in 46 / 612 cases ( 7.5% ) , the sample was scored 1 , as 19 / 46 samples ( 41.3% ) demonstrated exclusively normal lung 1148 mento lineare di parenchima polmonare trasgredito dallago . caratteristiche interne sono state considerate laspetto solido ( se con finestra mediastinica risultava visualizzabile almeno il 50% della superficie dellespanso rispetto a quanto visibile con finestra polmonare ) , la presenza di escavazioni ( aree allinterno della lesione con valori di attenuazione propri dellaria ) , calcificazioni e broncogramma aereo . 
 stata inoltre valutata , con criterio visivo ed attraverso lausilio della misurazione digitale dei dati di attenuazione mediante roi , la densit basale della lesione per ricercare eventuali aree di disomogeneit riferibili a necrosi . tipo di ago e calibro per tutte le procedure si ricorso alluso esclusivo di un unico ago ( chiba 21 g ; spinale 20 g ; tranciante 18 g con tecnica coassiale ) o ad associazione consecutiva di diversi aghi nel caso di prelievi multipli . 
la scelta di tipologia dellago stata posta secondo alcuni parametri quali le dimensioni della lesione , il sospetto clinico ( su basi anamnestiche , obiettive e di imaging ) e le preferenze delloperatore , oltre che la presenza dellanatomopatologo in sala radiologica . 
in particolare , lago sottile di chiba ha trovato esclusivo impiego in 470 / 612 procedure ( 76 , 8% ) , lago spinale in 76 ( 12 , 4% ) , il tranciante in 35 ( 5 , 7% ) , lassociazione chibaspinale in 27 ( 4 , 4% ) e lassociazione chiba - spinale - tranciante in 4 ( 0 , 7% )  . complicanze analisi statistica la comparsa di pneumotorace o di sfumate opacit parenchimali con aspetto radiologico a vetro smerigliato ( da impegno alveolare per emorragia ) stata registrata per ogni procedura . lanalisi statistica stata condotta con lutilizzo del programma statistica 6.1 ( statsoft software , per windows ) e mirata alla valutazione dellaccuratezza della procedura . 
i pazienti sono stati , in ogni sessione analitica , suddivisi in due gruppi omogenei per variabili discrete a soluzione dicotomica ( si / no ) ed analizzati per le diverse variabili , discrete o continue , che si ipotizzava influenzare i livelli di accuratezza : i gruppi sono stati suddivisi tra le diagnosi corrette e le diagnosi non corrette o non possibili a causa dellinadeguatezza del prelievo agobioptico . 
le differenze tra i gruppi sono state esaminate utilizzando i tests non parametrici mann - whitney u - test o analisi della varianza secondo kruskal - wallis , quando indicati . 
le differenze tra le proporzioni sono state analizzate con il test 2 di pearson od il test t di student . i parametri considerati significativi , nel determinare i livelli di accuratezza diagnostica , sono stati ulteriormente stratificati e correlati allaccuratezza con lausilio di grafici a.m. 
the discordance between the biopsy result and the final diagnosis is due to sampling errors , with sampling of surrounding healthy lung parenchyma or perilesional reactive inflammatory tissue there were 56 / 612 samples ( 9.1% ) scored 0 owing to sample inadequacy ( blood contamination ) and which were therefore classed as nondiagnostic . 
in 35 / 56 samples ( 60.7% of samples with a score of 0 ) , the lesion was subsequently found to be malignant . a final diagnosis based on the criteria previously described could be obtained for all 612 procedures : 17.0% ( 104 / 612 ) of lesions were found to be benign , whereas 83.0% ( 508 / 612 ) were malignant . 
the 458 cases positive for malignancy , with subsequent confirmation ( one malignant case at biopsy was subsequently found to be a false positive ) comprised 411 primary lung cancers , seven nonepithelial neoplasms and 40 metastatic tumours with secondary localisation to the lung ( table 1 )  . of these 458 patients , 46 ( 7.6% ) had a history of neoplastic disease at another location . 
of these 46 , the metastatic origin of the lung lesion was demonstrated in 40 , whereas in the remaining six cases , the primary nature of the lung nodule was demonstrated with the aid of immunocytochemistry and comparison with cytology and / or histology of the extrapulmonary neoplasm , when available . among the 459 cases of malignancy diagnosed at biopsy , o tabelle di contingenza . 
in tutti i casi stato considerato significativo un valore di p < 0 , 05 . risultati per calcolare laccuratezza diagnostica della metodica sono stati inclusi nello studio 608 pazienti : centocinquantaquattro sono i soggetti sottoposti ad intervento chirurgico ( per i quali disponibile lesame istologico post - operatorio , considerato il gold standard di raffronto con la metodica interventistica )  . quattrocentocinquantaquattro sono , invece , i pazienti non chirurgici che presentano ad agosto 2006 un followup di imaging , clinico e di risposta terapeutica non inferiore a 12 mesi ; in base al comportamento benigno o maligno della lesione in esame stata , quindi , dedotta la diagnosi finale . complessivamente sono state considerate 612 procedure . per ciascuno dei 612 campioni ottenuti , a conclusione di ogni procedura stato attribuito un punteggio discreto da 0 a 3 per asserirne la qualit : in 435 / 612 procedure ( 71 , 1% dei casi ) si sono ottenute , dal prelievo agobioptico , cellule benigne o maligne che hanno permesso una precisa caratterizzazione citoistologica della lesione ( punteggio 3 )  . 
di queste 52 sono risultate benigne , 382 di natura maligna , mentre in 1 solo caso si registrata la presenza di un amartocondroma associato ad un carcinoma polmonare primitivo del tipo squamocellulare ; in 75 / 612 prelievi ( 12 , 2% dei casi ) sono state riscontrate cellule di sicura origine maligna ( punteggio 2 ) , ma non stato possibile trarre conclusioni sullistotipo . 
in contrast , 50 procedures were false negative for malignancy ( negative result at biopsy , with malignant cells detected at repeat biopsy , surgery or follow - up )  . 
table 3 summarises the cytological diagnoses of the 52 cases that were negative for malignancy at biopsy . if we consider only benign lesions at final diagnosis assenza di una suddivisione , critica ai fini terapeutici , in tumore a piccole cellule e non . 
questi ultimi casi pongono importanti problematiche in termini di gestione del paziente per il fatto che non si pu pianificare il corretto iter terapeutico , impedendo in questo modo allagobiopsia di porsi a termine delliter diagnostico . 
inoltre , tra questi 4 casi si riscontrato lunico risultato bioptico falso positivo dellintera coorte : un sospetto carcinoma di non pi precisa caratterizzazione ( fnac ) si poi dimostrato essere , dopo resezione chirurgica , una granulomatosi escaa final diagnoses are based on the retrospective analysis of the outcome of surgery , repeated biopsy , imaging , and clinical follow - up for at least 12 months . 
 malignant pulmonary lesions : sensitivity 90.2% ( 458 / 508 ) , specificity 99.0% ( 103 / 104 ) , positive predictive value 99.8% ( 458 / 459 ) , negative predictive value 67.3% ( 103 / 153 ) , false positive rate 0.22% ( 1 / 459 ) , false negative rate 10.9% ( 50 / 508 ) , accuracy 91.7% [ ( 458 + 103 ) / 612 ] , overall diagnostic accuracy 83.3% [ ( 458 + 52 ) / 612 ] ( for all lesions , benign and malignant ) table 2 results of 612 computed - tomography - guided transthoracic needle biopsies final diagnosisa malignant biopsy diagnosis malignant benign / inadequate total diagnosi bioptica maligno benigno - inadeguato totale 1150 tabella 2 risultati di 612 procedure agobioptiche polmonari diagnosi finalea maligno benign 103 ( 52 / 51 ) benigno 103 ( 52 / 51 ) total totale a la diagnosi finale deriva dallanalisi retrospettiva dei risultati della chirurgia , di uneventuale successiva agobiopsia transtoracica e dallesito del followup clinico / radiologico pari ad un periodo non inferiore ai 12 mesi . 
conversely , in 51 cases , the benign nature of the lesion could not be defined because of sample inadequacy ( 30 samples scored 1 and 21 scored 0 )  . with regard to malignant lesions , 99.8% of malignancies at vata caratterizzata da severa displasia cellulare in relazione alla pregressa infezione tubercolare ; in 46 / 612 casi ( 7 , 5% ) stato attribuito , al campione prelevato , un punteggio pari a 1 , dal momento che in 19 / 46 casi ( 41 , 3% ) si sono riscontrate esclusivamente cellule normali proprie del tessuto polmonare ( pneumociti di i e ii ordine ) , in 14 / 46 ( 30 , 4% ) cellule flogistiche in assenza di significative atipie ed in 13 / 46 ( 28 , 3% ) cellule atipiche non ulteriormente caratterizzabili , ma neanche classificabili come sicuramente maligne . 
in 16 di questi 46 prelievi ( 34 , 7% dei prelievi a punteggio 1 ; 2 , 6% sul totale delle procedure ) le lesioni campionate sono poi risultate di natura maligna . 
la discordanza tra risultato bioptico e diagnosi finale dovuta ad errori di campionamento , per prelievo di parenchima polmonare sano limitrofo o di tessuto flogistico reattivo perilesionale ; infine 56 / 612 prelievi ( 9 , 1% ) hanno ottenuto un punteggio pari a zero a causa dellinadeguatezza del materiale analizzato dallanatomopatologo ( campioni ematici ) e sono quindi stati classificati come non diagnostici . 
in 35 / 56 prelievi ( 60 , 7% dei campioni a punteggio 0 ) la lesione poi risultata maligna . per tutte le 612 procedure stato possibile ottenere una diagnosi finale con i criteri gi ampiamente descritti : il 17 , 0% ( 104 / 612 ) delle lesioni risultato di natura benigna , mentre lo 83 , 0% ( 508 / 612 ) maligna . 
lagobiopsia transtoracica percutanea ha conseguito un risultato diagnostico in 511 casi su 612 ( 83 , 5% , prelievi a punteggio 2 e 3 ) , mentre in 101 procedure ( 16 , 5% , prelievi a punteggio 0 e 1 ) non stato possibile fornire un giudizio affidabile . 
i 458 casi positivi per malignit , con conferma successiva ( un caso maligno alla biopsia poi risultato un falso positivo ) hanno compreso 411 carcinomi polmonari primitivi , 7 neoplasie non epiteliali e 40 tumori metastatici con localizzazione secondaria al polmone ( tabella 1 )  . di questi 458 pazienti , 46 ( 7 , 6% ) presentavano un precedente anamnestico di malattia neoplastica in altra sede . 
tra questi ultimi , in 40 si dimostrata lorigine metastatica della lesione polmonare , mentre nei restanti 6 casi stato possibile definire la natura primitiva del nodo polmonare attraverso lausilio della immunocitochimica ed il confronto , quando disponibile , con i reperti citologici e / o istologici del tumore extrapolmonare . tra i 459 riscontri risultati maligni allagobiopsia , solo in un caso la diagnosi definitiva non ha confermato il dato configurando quindi la presenza di un unico falso positivo per malignit . 
si sono invece registrate 50 procedure false negative per malignit ( risultato negativo per cellule neoplastiche con esito maligno alla ripetizione della procedura , allintervento chirurgico od al follow - up )  . 
in tabella 2 vengono riportati i risultati conseguiti , in termini di affidabilit della metodica , sulla corretta diagnosi delle lesioni maligne . la tabella 3 riassume le diagnosi citologiche nei 52 casi risultati negativi per malignit allagobiopsia . analizzando le sole lesioni benigne alla diagnosi finale ( 104 / 612 , 17% ) , lagobiopsia ha permesso di conseguire un sicuro giudizio di benignit con diagnosi specifica in soli 52 1151 a.m. 
a specific judgement of benignity of the biopsy sample could , however , be made in only 34% of samples , characterised by the definite absence of neoplastic cells ( 52 / 153 ) ( table 2 )  . 
finally , table 4 demonstrates that lesion depth ( the portion of aerated lung traversed by the needle ) , morphology and lobar location ; the presence of calcification , cavitation and necrotic centre ; and the occurrence of complications ( pneumothorax and bleeding ) have no influence on the diagnostic accuracy of transthoracic ct - guided needle biopsy . discussion with the use of percutaneous transthoracic needle biopsy , and in particular of fnac , as an initial minimally invasive procedure for evaluating the nature of pulmonary lesions , this study obtained an overall diagnostic accuracy of 84% , with levels of 92% and 67% for malignant and benign lesions , respectively . 
in 51 lesioni benigne non invece stato possibile stabilirne la natura a causa dellinadeguatezza del prelievo ( 30 prelievi a punteggio 1 e 21 prelievi a punteggio 0 )  . riferendosi agli addensamenti polmonari di natura maligna , il 99 , 8% delle lesioni considerate maligne allagobiopsia poi stata confermata ( 458 / 459 , valore predittivo positivo per malignit ) , mentre il 67 , 3% dei prelievi con assenza di cellule tumorali ( prelievi classificati come benigni , od inadeguati ) risultato benigno ( 103 / 153 , valore predittivo negativo per malignit )  . 
stato comunque possibile dare un giudizio specifico di benignit del prelievo agobioptico solo nel 34% dei campioni , caratterizzati dalla sicura assenza di cellule tumorali ( 52 / 153 ) ( tabella 2 )  . 
la sensibilit e la specificit per la diagnosi di malignit sono risultate del 91% e 99% rispettivamente , con una proporzione di falsi positivi trascurabile ( 0 , 22% ) ed una proporzione di falsi negativi dell11% . 
questo valore raggiunge l88 , 2% ( 540 / 612 ) se , tra le diagnosi agobioptiche corrette , si includono i 30 prelievi a punteggio 1 poi risultati benigni ( ovvero reperti considerati allagobiopsia negativi per cellule neoplastiche in assenza di una specifica diagnosi )  . 
in tabella 4 riassunto linsieme di variabili che si supposto esercitare una influenza sui livelli di accuratezza della metodica : le uniche variabili associate con significativit statistica ad una riduzione dei livelli di accuratezza diagnostica sono risultate la discrimante della diagnosi finale ( categoria benigno versus maligno ) e le dimensioni della lesione . 
la tabella 4 dimostra , infine , come la profondit della lesione ( ovvero la quota di parenchima polmonare aerato attraversata dallago ) , la sua morfologia e localizzazione lobare , la presenza di calcificazioni , cavitazioni e centro necrotico , oltrech loccorrenza di complicanze ( pneumotorace e sanguinamento ) non esercitino alcuna a.m. 
anumber of procedures ; bpearsons 2 test for categoric variables ; caverage lesion diameter in two axial planes ; ns , not significant tabella 4 correlazione per variabili , con la diagnosi finale , di risultati corretti ed errati od indeterminati allagobiopsia transtoracica variabile na ( 612 ) diagnosi finale errata o indeterminata n = 102 corretta n = 510 52 ( 50 , 0 ) 458 ( 90 , 2 ) 30 ( 66 , 6 ) 362 ( 87 , 3 ) 118 ( 77 , 6 ) 52 ( 50 , 0 ) 50 ( 9 , 8 ) 15 ( 33 , 3 ) 53 ( 12 , 7 ) 34 ( 22 , 4 ) i valori in parentesi sono riferiti in % . 
agrandezza del campione ; btest 2 di pearson per variabili categoriche ; cconsiderata quale dimensione media tra i due assi ( maggiore e minore ) ortogonali della lesione ; ns , non significativo . 
however , they are also dependent on the severity with which sample adequacy is judged : a sample without neoplastic cells should not be considered negative for malignancy ( consider sampling errors , for example ) unless they provide a precise and specific diagnosis of benignity ( 100% specificity is desirable in benign lesions )  . 
many studies [ 13 , 29 , 32 , 37 , 38 ] have reported substantially lower levels of diagnostic accuracy for benign lung lesions ( range 52%91% ) compared with malignant lesions influenza sui valori di accuratezza diagnostica dellagobiopsia transtoracica tc guidata . discussione attraverso lutilizzo dellagobiospia transtoracica percutanea , ed in particolar modo della fnac , quale iniziale procedura mini - invasiva nella valutazione di natura degli addensamenti polmonari si ottenuta , in questo studio , unaccuratezza diagnostica globale dell84% con valori di accu1153 a.m. 
1a - c relationship between mean lesion size and number of observations for the entire group of lesions ( a ) and in regard to the presence ( b ) or the absence ( c ) of a necrotic centre . 
1a - c correlazione tra diametro medio della lesione e numero di casi per tutte le lesioni ( a ) e suddividendo queste ultime per presenza ( b ) od assenza ( c ) di centro necrotico . 
la sensibilit della metodica per lesioni maligne risultata del 90% ( con valori di specificit del 99% ) , mentre per lesioni benigne la sensibilit risultata del 50% , ma con specificit del 100% . 
questi dati dimostrano come , nellinquadramento diagnostico delle lesioni benigne , la fnac risulti inferiore alla cb [ 20 , 24 ] , ma paiono anche giustificati dalla severit di giudizio di idoneit cui vengono sottoposti i campioni : un prelievo con assenza di cellule neoplastiche non deve essere considerato negativo per patologia tumorale ( si considerino , ad esempio , gli errori di campionamento ) , a meno che sia possibile formulare una precisa e specifica diagnosi di benignit ( sono auspicabili valori di specificit per lesioni benigne pari al 100% )  . 
molteplici studi in letteratura [ 13 , 29 , 32 , 37 , 38 ] riportano valori di accuratezza diagnostica sensibilmente inferiori per lesioni polmonari benigne ( con intervallo compreso tra il 52% ed il 91% ) se paragonate a lesioni maligne ( intervallo compreso tra l86% ed il 100% ) , sia nel prelievo aspirativo sia tranciante ; inoltre , considerando esclusivamente gli addensamenti benigni , la cb presenta valori di accuratezza e sensibilit significativamente maggiori rispetto alla fnac ( accuratezza superiore all80% versus 50%70% ) [ 9 , 2225 ]  . 
i livelli di accuratezza e sensibilit riportati dal nostro studio sono in linea con i riscontri fnac della letteratura , ma non dimensioni lesione ( cm ) lesion size ( cm ) fig . 
 ctest t di student ( per campioni indipendenti e per gruppi ) , p < 0 , 05 considerata significativa : il diametro medio delle lesioni con ( 57 , 7 mm ) e senza ( 34 , 0 mm ) necrosi differisce con significativit statistica . raggiungono i valori riportati dalla cb , elemento comunque non contraddittorio dal momento che solo nel 6 , 4% delle procedure stato utilizzato un ago tranciante ( singolarmente od in associazione con altri aghi )  . la documentazione di cellule sicuramente maligne , nella pressoch totalit dei casi , prova certa della natura maligna dellespanso . 
nella nostra coorte lunico caso classificato come maligno ( neoplasia di origine epiteliale ) e poi risultato benigno ( granulomatosi escavata ) alla diagnosi finale trova esplicazione nel fatto che la lesione benigna ha sviluppato atipie cellulari tali da farla risultare sospetta allindagine citologica per espanso di natura maligna . nonostante gli insuccessi siano sensibilmente minori per le lesioni maligne , tuttavia si evidenziato un 11% di falsi negativi nellambito di tali addensamenti ( integralmente costituiti da prelievi a punteggio 01 )  . 
in aggiunta , la nostra esperienza indica come la sola ispezione ad occhio nudo del campione ottenuto ( in termini di integrit del frustolo bioptico o di cellularit o di carattere ematico del prelievo aspirativo ) inaffidabile nel predirne ladeguatezza [ 30 , 32 , 34 , 36 , 38 ] ed quindi auspicabile la presenza dellanatomopatologo nel corso della seduta bioptica . 
la ripetizione del prelievo dovrebbe essere presa in considerazione ogni qual volta si verifichi discordanza tra risultato bioptico , presentazione clinica e caratteristiche tc ( prima di passare ad accertamenti diagnostici invasivi di ii livello ) [ 13 ]  . lanalisi della nostra coorte ha evidenziato come le uniche variabili in grado di influenzare , in termini statisticamente significativi , laccuratezza diagnostica della metodica siano la diagnosi finale ( benignit versus malignit ) e le dimensioni della lesione ( nodi con diametro medio inferiore ad 1 , 5 cm o masse di dimensioni superiori a 5 cm sono caratterizzati da livelli di minore accuratezza diagnostica )  . 
riferendosi a questultimo aspetto , gli studi presenti in letteratura esprimono giudizi discordanti in merito allinfluenza delle dimensioni della lesione sui livelli di accuratezza dia1155 dimensioni lesione ( cm ) lesion size ( cm ) fig . 
3 relazione esistente tra dimensione della lesione e presenza di necrosi : il grafico dimostra come lincidenza di necrosi si incrementi gradualmente allaumentare delle dimensioni delle lesioni ; la maggior proporzione di necrosi si riscontrata nelle lesioni di 6 cm , ovvero quelle caratterizzate da minor accuratezza diagnostica . ( from 86% to 100% ) , achieved with both fnac and cb . 
accuracy and sensitivity levels found in our study are similar to those previously reported for fnac but fail to reach those reported for cb , a finding that is not contradictory given that only 6.4% of procedures were carried out with a cutting needle ( used alone or in combination with other needles )  . demonstration of definitely malignant cells is proof of the a.m. 
4 il grafico box & whisker dimostra una differenza significativa in termini di dimensioni nel gruppo di lesioni senza ( 3 , 4 cm1 , 8 ) e con necrosi centrale intralesionale ( 5 , 7 cm1 , 8 )  . 
il diametro medio delle lesioni in assenza e presenza di necrosi differisce significativamente ( p < 0 , 001 ) ( ds , deviazione standard ; n , no ; s , si )  . malignant nature of the mass in virtually all cases . 
in our cohort , the only case classified as malignant ( epithelial neoplasm ) at biopsy and found to be benign ( excavated granuloma ) at final diagnosis is explained by the fact that the lesion had developed cellular atypia that made it suspicious for malignancy at cytological assessment . although there were substantially fewer failures in malignant lesions , the false negative rate was 11% in this group ( all for samples with a score of 01 )  . 
in addition , our experience shows that gross inspection of the sample ( in terms of integrity of the biopsy specimen , cellularity or blood contamination of the aspirate ) is unreliable in predicting adequacy [ 30 , 32 , 34 , 36 , 38 ] , making the presence of a pathologist during the biopsy procedure strongly desirable . 
found that diagnostic accuracy declined progressively with decreasing lesion size : from 100% to 93% , 87% , 79% and 67% for lesions > 5 cm , 35 cm , 23 cm , 12 cm and < 1 cm , respectively [ 13 ]  . 
reported accuracy levels of approximately 88% for lesions > 2 cm when the mean number of needle passes was 2.5 , whereas when only a single specimen was obtained , accuracy decreased to 83% [ 29 ]  . the results of our study are similar to those reported by yeow et al . 
 [ 20 ] , who found , with a mean number of passes of three ( without a pathologist present ) , lower levels of diag1156 gnostica [ 13 , 20 , 30 , 36 , 37 ]  . 
tsukada ha riscontrato un graduale e progressivo decremento dei valori di accuratezza diagnostica man mano che le dimensioni delle lesioni si riducevano : dal 100% al 93% , 87% , 79% e 67% per lesioni rispettivamente > 5 cm , tra 3 e 5 cm , tra 2 e 3 cm , tra 1 e 2 cm e < 1 cm [ 13 ]  . 
lucidarme ha riscontrato valori di accuratezza di circa l88% per lesioni > 2 cm con un numero medio di prelievi per biopsia di 2.5 , mentre laccuratezza si riduceva all83% in caso di unico prelievo per seduta bioptica [ 29 ]  . nel nostro studio si sono ottenuti risultati simili a quelli descritti da yeow [ 20 ] che riportava , con una media di 3 prelievi bioptici a seduta ( in assenza di un medico anatomopatologo in sala ) , livelli inferiori di accuratezza diagnostica per lesioni < 1 , 5 cm e > 5 cm ( dell84% e 93% rispettivamente ) quando paragonati a lesioni con diametro compreso tra 1 , 5 e 5 cm ( 96% )  . 
nel nostro lavoro vengono , invece , riportati valori di accuratezza diagnostica globale ( per lesioni maligne e benigne ) del 68% per lesioni < 1 , 5 cm , del 78% per lesioni > 5 , 0 cm e dell87% per le lesioni comprese tra 1 , 5 e 5 , 0 cm . la maggior accuratezza diagnostica riportata da yeow giustificata dal fatto che in tutti i casi stata eseguita una cb con tecnica coassiale ( caratterizzata da livelli di accuratezza diagnostica maggiori rispetto alla fnac ) , mentre nel nostro studio solo il 6% delle manovre stato eseguito con tale procedura , riservando la fnac a tutti gli altri casi . 
in aggiunta , avendo la disponibilit del citopatologo in sala radiologica , risultato sensibilmente minore il numero di prelievi per seduta ( 1 , 3 prelievi versus 3 , 0 )  . 
il numero di prelievi , essendo variabile nei diversi studi , potrebbe costituire un determinante elemento confondente in grado di influenzare laccuratezza diagnostica al pari delle dimensioni della lesione [ 20 , 29 , 37 ]  . 
con una media di 1 , 3 prelievi per procedura , il nostro studio pone come limite dimensionale critico , al di sotto del quale si verifica una sensibile riduzione di accuratezza diagnostica , il valore di 1 , 5 cquesto risultato in linea con le a.m. 
is explained by the fact that they used cb with coaxial technique ( which is more accurate than fnac ) in all cases , whereas we used cb for only 6% of procedures and fnac for the remaining cases . 
the number of needle passes should , however , be kept to a minimum , as this variable is significantly related to higher rates of pneumothorax [ 32 ] ; the presence on site of a cytopathologist during the procedure is instrumental to establishing a correct diagnosis . the substantial reduction in diagnostic accuracy in small lesions could be due to sampling errors resulting from increased technical difficulty in the localisation phase [ 11 ]  . such difficulties are further supported by the higher rate of complications within this class of lesions : yeow et al . 
 [ 32 ] reported a 17 times higher risk of pneumothorax and a six times higher risk of bleeding for lesions smaller than 2 cm . in view of the lower diagnostic accuracy for small lung nodules ( whether sampled by fnac or cb ) and the higher complication rate , fine - needle aspiration should always be preferred to cb for lesions smaller than 1 cm , as suggested by laurent et al . 
when sampling these nodules , in fact , it is impossible to avoid inclusion of portions of healthy aerated lung tissue , as the biopsy core is 1.3cm long ( shortest throw - length setting ) [ 29 , 32 , 37 ]  . 
diffuse bleeding may also occur as a result of the surrounding healthy parenchyma not being able to provide an adequate tamponade effect [ 29 , 32 , 37 ]  . 
finally , in a nonnegligible number of cases , the material recovered proves inadequate due to the abundant presence of blood . despite the fact that throw lengths of 10 mm can be used to avoid bleeding in lesions smaller than 1.5 cm , boiselle et al . reported a diagnostic accuracy of 62% with this approach [ 39 ]  . 
comunque auspicabile conseguire il minimo numero di campionamenti possibili per procedura dal momento che tale variabile significativamente correlata ad una maggior proporzione di pneumotoraci [ 32 ] ; elemento indispensabile , a garanzia dellobiettivo di ottenere una corretta diagnosi , risulta essere la presenza del citopatologo durante la seduta bioptica . la sensibile riduzione di accuratezza diagnostica per lesioni di ridotte dimensioni potrebbe trovare una valida esplicazione in errori di campionamento , dovuti a maggiori difficolt tecniche nella fase di centratura bioptica [ 11 ]  . 
le difficolt procedurali trovano ulteriore conferma nella maggior proporzione di complicanze riscontrabile in questa categoria di lesioni : yeow [ 32 ] riporta , infatti , un rischio di pneumotorace 17 volte maggiore e di sanguinamento 6 volte superiore per lesioni di diametro inferiore ai 2 cin ragione della minor accuratezza diagnostica per i piccoli noduli polmonari ( che siano sottoposti a fnac o a cb ) ed alla pi alta percentuale di complicanze riscontrate , risulta sempre opportuno preferire alla cb , come gi suggerito da laurent e yeow [ 20 , 30 ] , il prelievo aspirativo con ago sottile per le lesioni di dimensione inferiore al centimetro . 
infatti , risulta impossibile evitare , nel campionamento di questi piccoli nodi , porzioni di tessuto aerato sano , dal momento che il frustolo bioptico ha lunghezza pari ad 1 , 3 cm ( limite inferiore della lunghezza dello scatto dellago tranciante ) [ 29 , 32 , 37 ]  . 
pu inoltre verificarsi un sanguinamento diffuso dal momento che il parenchima circostante sano , interessato anchesso dal campionamento , non in grado di fornire un adeguato effetto tampone [ 29 , 32 , 37 ]  . 
nonostante si possano utilizzare lunghezze di scatto pari a 10 mm per evitare il sanguinamento in lesioni inferiori ad 1 , 5 cm , boiselle ha riportato , in tali condizioni , unaccuratezza diagnostica pari al 62% [ 39 ]  . 
questo valore risulta inferiore al 67% da noi ottenuto utilizzando esclusivamente , per tali lesioni , lagoaspirato e con un tasso di sanguinamento perilesionale di minor entit . analizzando il parametro dimensionale , quale variabile determinante laccuratezza diagnostica della procedura , si sono riscontrati decrementi di accuratezza per lesioni con dimensione maggiore ai 5 cquesta evenienza viene compresa se si considera la presenza di necrosi centrale , che risulta di frequente riscontro nelle masse polmonari > 5 cm ( nella nostra casistica percentuale tc di necrosi tumorale per lesioni sino a 5 cm compresa tra lo 0% ed il 15% , per masse 5 cm tra il 12% ed il 41% )  . 
risulta quindi evidente come , nelle grosse masse polmonari , sia necessario disporre di indagini tc acquisite con infusione di mezzo di contrasto per individuare aree lesionali necrotiche al fine di evitarle durante il campionamento . 
inoltre , in assenza di un anatomopatologo in sala , nellevenienza allispezione visiva di frustoli particolarmente fragili e frammentati o di prelievi citologici ottenuti con agoaspirato , particolarmente ematici , si dovrebbero 1157 a.m. 
moreover , when no on - site pathologist is present and the biopsy cores appear particularly fragile and fragmented or the aspirate particularly bloody on gross inspection , further samples should be obtained taking care to direct the needle to different areas of the lesion [ 32 , 40 , 41 ]  . the presence of cavitations within a lung mass does not appear to influence the diagnostic accuracy of either fnac , as demonstrated in our study , or cb , as shown by yeow et al . 
similarly , diagnostic accuracy was not significantly affected by the presence of calcification or a frankly necrotic centre ; by lesion depth ( from the pleural surface ) , morphology or location ; or by the occurrence of complications such as pneumothorax and bleeding . 
no evaluation was made with regard to needle size or the radiologists experience , variables that are ascribed different significance in the various studies [ 20 , 41 ]  . conclusions in conclusion , transthoracic ct - guided needle biopsy of pulmonary lesions is a highly accurate procedure , especially in malignant lesions . 
however , to enhance the likelihood of success and achieve a correct diagnosis , awareness of the variables affecting its effectiveness is crucial : benign lesions , nodules smaller than 1.5 cm and masses larger than 5 cm are associated with substantially lower accuracy rates . 
analogamente , la presenza di calcificazioni o di centro francamente necrotico , od ancora la profondit della lesione ( rispetto al piano pleurico ) o la morfologia o la localizzazione od infine la comparsa di complicanze , quali lo pneumotorace od il sanguinamento , non hanno significativamente alterato i valori di accuratezza diagnostica della procedura . 
non si sono , invece , formulate valutazioni relative al calibro dellago o allesperienza del radiologo prelevatore , parametri che assumono , a seconda dei diversi studi presenti in letteratura , significato diverso [ 20 , 41 ]  . conclusioni in conclusione , lagobiopsia transtoracica tc guidata di espansi polmonari metodica ad elevata accuratezza diagnostica , specie per le lesioni di natura maligna . 
risulta comunque indispensabile , al fine di implementare le probabilit di successo della procedura in termini di raggiungimento della corretta diagnosi , la conoscenza delle variabili in grado di inficiare tale efficacia : le lesioni benigne ed i nodi di dimensioni minori ad 1 , 5 cm o le masse superiori a 5 cm sono correlate a valori di accuratezza diagnostica sensibilmente inferiori . 
from january 2005 to september 2006 , 23 patients ( 10 men and 13 women ; mean age 41.38.6 years ) affected by als were evaluated with digital cineradiography to assess the grade of dysphagia . 
the cineradiographic technique enabled us to differentiate patients with disorders of the oral ( 17 / 23 ) and / or pharyngeal ( 19 / 23 ) swallowing phase from those without swallowing dysfunction ( 4 / 23 )  . 
in 14 / 23 patients , passage of contrast medium into the upper airways was observed during swallowing , whereas in 5 / 23 cases , aspiration of contrast medium into the lower airways was recorded . 
in addition , the study proved useful for planning speech therapy and for follow - up in patients with als . key words swallowing dysphagia amyotrophic lateral sclerosis cineradiography riassunto obiettivo . 
dal gennaio 2005 al settembre 2006 , 23 pazienti ( 10 uomini e 13 donne ; et media 41 , 38 , 6 anni ) affetti da sla e classificati secondo la classificazione als severity scale ( alsss ) di hillel sono stati sottoposti a studio videofluorografico della deglutizione . 
la tecnica videofluorografica utilizzata ha permesso di differenziare i pazienti con alterazioni deglutitorie , 17 / 23 con alterazioni della fase orale e 19 / 23 con alterazioni della fase faringea ( 19 / 23 pazienti ) , da quelli che non presentavano alterazioni 4 / 23 . 
lo studio videofluorografico della deglutizione una tecnica dotata di elevata capacit diagnostica per la valutazione dei deficit deglutitori , essendo in grado di identificarne il grado di compromissione e le cause determinanti . lo studio dinamico della deglutizione si inoltre dimostrato utile nellapproccio alla terapia logopedica e nel follow - up dei pazienti affetti da sla . parole chiave deglutizione disfagia sclerosi laterale amniotrofica cineradiografia introduction introduzione amyotrophic lateral sclerosis ( als ) is a progressive neurodegenerative disease that involves the upper motor neurons of the cerebral cortex and the lower motor neurons of the brainstem and spinal cord while sparing the sensory component , motor control systems and cognition . 
als is found la sclerosi laterale amiotrofica ( sla ) una malattia neurodegenerativa progressiva che coinvolge sia i motoneuroni primari della corteccia cerebrale che quelli secondari del tronco encefalico e del midollo spinale , risparmiando la componente sensitiva , i sistemi di controllo dei movimenti e 1173 g . 
pseudobulbar palsy , with exclusive involvement of the upper motor neurons . regardless of onset , as the disease progresses , both upper and lower motor neurons are involved , and the diagnosis is based on their simultaneous involvement and exclusion of all possible diagnostic alternatives [ 2 ]  . 
involvement of muscles of the oral cavity , pharynx and larynx is most frequent and earliest in patients affected by the bulbar form , and the consequent dysphagia leads to serious nutritional deficit that , over time , requires tube feeding or percutaneous gastrostomy [ 3 ]  . 
dysphagia is one of the main indicators of the clinical course of the disease , such that there are a number of classifications of its severity , some of which take into account swallowing disorders . 
the most important classification is the hillel als severity scale ( alsss ) [ 5 , 6 ] , which classifies patients according to five classes of severity : normal eating habits ( neh ) , early eating problems ( eep ) , dietary consistency changes ( dcc ) , needs tube feeding ( ntf ) and nothing by mouth ( nbm )  . the videofluoroscopic swallowing study ( vfss ) is the gold standard for assessing swallowing dysfunction , particularly in patients suffering from neurological diseases [ 714 ] , in that it provides accurate analysis of the mechanisms of the oral and pharyngeal phases of swallowing , identification of possible alterations responsible for symptoms , and planning of appropriate speech therapy . 
on the basis of the responses received , patients were divided as follows : 12 patients in the neh group ( mean age 38.4 years ) , seven patients in the eep group ( mean age 41 years ) , three patients in the dcc group ( mean age 50 years ) and one patient in the ntf group ( age 53 years ) ; there were no patients belonging to the nbm group . 
la sla diffusa in tutto il mondo ( incidenza 11 , 5 casi per 100000 pazienti ) [ 1 ] e di solito insorge dopo la seconda decade di vita ( m / f 1 , 5 : 1 ) , con frequenza progressivamente maggiore nelle decadi successive ; la prognosi infausta con attesa di vita di 35 anni dalla prima diagnosi . 
questa malattia pu presentarsi in tre forme che differiscono oltre che dal punto di vista clinico , dal punto di vista fisio - patologico e anatomo - patologico : 1 . 
paralisi pseudobulbare , con coinvolgimento esclusivo dei motoneuroni primari . indipendentemente dallesordio , nella progressione della malattia vengono coinvolti entrambi i gruppi di motoneuroni , primari e secondari e la diagnosi viene posta nel caso di un loro interessamento simultaneo con esclusione di tutte le altre possibilit diagnostiche alternative [ 2 ]  . 
il coinvolgimento dei muscoli della cavit orale , del faringe e del laringe pi frequente e pi precoce nei pazienti affetti dalla forma bulbare della malattia , e la disfagia conseguente determina gravi deficit nutrizionali che , nel tempo , rendono necessaria lalimentazione mediante luso di sondino naso - gastrico o il ricorso alla gastrostomia percutanea [ 3 ]  . 
la disfagia rappresenta uno dei principali indicatori di progressione della malattia , tanto che sono state formulate diverse classificazioni di gravit della malattia , alcune delle quali tengono in considerazione proprio la sintomatologia disfagica dei pazienti . 
fra queste classificazioni la pi importante la classificazione di severit della sla ( als severity scale , alsss ) di hillel [ 5 , 6 ] , che raggruppa i pazienti secondo cinque classi di gravit : normali abitudini alimentari ( normal eating habitus , naa ) , problemi deglutitori iniziali ( early eating problems , eep ) , cambiamenti della consistenza della dieta ( dietary consistency changes , dcc ) , alimentazione mediante sondino naso - gastrico ( needs tube feeling , ntf ) e impossibile alimentazione per via orale ( nothing by mouth , nbm )  . 
lo studio della deglutizione mediante videofluorografia ( vdfg ) rappresenta il gold standard per la valutazione dei disturbi della deglutizione , specie nei pazienti affetti da malattie neurologiche [ 714 ] , permettendo una accurata analisi dei meccanismi della fase orale e faringea della deglutizione , lindividuazione delle eventuali alterazioni responsabili della sintomatologia e la programmazione di unadeguata terapia logopedica . 
nominal abnormality : patients report slight indicators such as food lodging in the recesses of the mouth or sticking in the throat early eating problems ( eep ) dietary consistency changes ( dcc ) 7 . 
oral and pharyngeal secretions managed with aspirator and / or medications secretions cannot be managed noninvasively tabella 1 questionario per la classificazione di pazienti secondo la alsss normali abitudini alimentari ( naa ) i pazienti lamentano alcuni disturbi deglutitori lievi alterazioni : i pazienti lamentano lievi problemi come il ristagno di cibo nella bocca o in gola 10 . 
alimentazione mediante sondino naso - gastrico , con occasionale assunzione orale del cibo ; meno del 50% dellalimentazione avviene per via orale impossibile alimentazione per via orale ( nbm ) 2 . 
only in two patients ( one in the dcc group and one in the ntf group ) was the acquisition of sequences at 25 frames per second ( matrix 512512 ) necessary to adequately evaluate swallowing dysfunction . 
in 22 patients in the neh , eep and dcc groups , the study was first performed using boluses of approximately 5 ml high - density barium ( 250% weight / volume , prontobario hd , bracco , milan , italy )  . 
in patients where penetration ( the passage of the e 13 femmine , et media 41 , 38 , 6 anni ) disfagici affetti da sla sono stati sottoposti a studio videofluografico della deglutizione . 
prima dellesecuzione dellesame stato somministrato un questionario al fine di suddividere i pazienti secondo la classificazione di severit della sla di hillel ( als severity scale , alsss ) ( tabella 1 )  . 
in base alle risposte fornite questi sono stati suddivisi come segue : 12 pazienti del gruppo naa ( et media 38 , 4 anni ) , 7 del gruppo eep ( et media 41 anni ) , 3 del gruppo dcc ( et media 50 anni ) ed 1 del gruppo ntf ( et 53 anni ) ; nessun paziente apparteneva al gruppo nbm . 
lo studio della deglutizione stato eseguito con apparecchio telecomandato con arco a c digitale ( telecomandato polifunzionale eurocolumbus tr3d , milano , italia ) dotato di intensificatore di brillanza da 16 pollici , macchia focale da 0 , 6 a 1 , 2 mm e massima differenza di potenziale di 150 pkv in grafia e 120 pkv in scopia . 
sono state acquisite sequenze cineradiografiche digitali con 12 immagini / secondo e matrice 5121024 ; solo in 2 pazienti ( uno della classe dcc ed uno della classe ntf ) stata necessaria 1175 g . 
transport of the bolus into the pharynx ( swallowing with small boluses , transport of the bolus into the pharynx prior to the triggering of the oral phase of swallowing ) 6 . 
aspiration of the bolus into the airways ( transport of the bolus below the level of the vocal cords , into the trachea and / or the bronchial tree ) 11 . 
compensatory manoeuvres in the event of laryngeal penetration and / or tracheobronchial aspiration , we assessed the depth of the aspiration ( enhancement in the trachea only , in the trachea and one bronchis or in both bronchi )  . 
we assessed the statistical difference of changes in the swallowing phase of the various classes using fishers exact test ( spss 10.1 , spss , chicago , il , usa )  . 1176 lacquisizione , per una adeguata valutazione funzionale dei deficit deglutitori , di sequenze con frame - rate di 25 immagini / secondo ( matrice 512512 )  . 
in 22 pazienti appartenenti ai gruppi naa , epp e dcc lo studio stato condotto utilizzando inizialmente dei boli di 5 ml circa di bario ad alta densit ( 250% peso - volume , prontobario hd , bracco , milano , italia )  . 
per i pazienti che mostravano fenomeni di penetrazione ( passaggio del bolo nel lume laringeo al di sopra del piano delle corde vocali vere ) e / o aspirazione ( passaggio del bolo in trachea o nei bronchi ) sono state acquisite anche sequenze cineradiografiche durante la deglutizione di bario fluido ( 60% pesovolume , prontobario 60% , bracco , milano , italia ) , e di pasta baritata ( 116% peso - volume , prontobario 110% , bracco , milano , italia ) spalmata su cracker o mescolata a mollica di pane . 
al fine di individuare eventuali meccanismi di compenso si proceduto ad una ulteriore valutazione invitando questi pazienti ad assumere adeguate posture , con capo in posizione flessa ed estesa , somministrando la stessa tipologia e quantit di bario di quella utilizzata per la valutazione a capo in posizione neutra . 
al fine di ridurre il possibile rischio di complicanze gravi , come linsorgenza di fenomeni di edema polmonare , nellunico paziente del gruppo ntf stato utilizzato come mdc una soluzione al 50% di acqua e mezzo di contrasto ( mdc ) iodato non ionico idrosolubile ( iopamidolo , gastromiro bracco , milano , italia ) con le stesse modalit sopra descritte . 
passaggio del bolo in faringe ( deglutizione per piccoli boli , passaggio del bolo in faringe prima dellinnesco della fase orale della deglutizione ) ; ristagno del bolo nel faringe ( vallecule glosso - epiglottiche e / o seni piriformi ) ; escursione craniale dellosso ioide e dellepiglottide ; tempo di innesco della fase orale ; eventuale ristagno del bolo nel cavo orale ; capacit di trattenere il bolo nel cavo orale ; 8 . 
attivit contrattile dei muscoli faringei ; fenomeni di penetrazione del bolo nella via aerea ( passaggio del bolo nel lume laringeo senza superamento del piano passante per le corde vocali vere ) ; 10 . 
fenomeni di aspirazione del bolo nella via aerea ( passaggio del bolo nelle vie aeree al di sotto del piano delle corde vocali , in trachea e / o nellalbero bronchiale ) ; g . 
in five patients ( 41.6% ) , bolus stasis in the pharynx caused episodes of postdeglutitive subepiglottic penetration ( with boluses of more than 15 ml ) ; only in one case did this provoke coughing . 
none of the these patients suffered coughing fits during the examination . swallowing with the head flexed resulted in the disappearance of intradeglutitive penetration , whereas only one patient with postdeglutitive penetration benefited from the change . 
i diversi parametri presi in considerazione sono stati quindi raggruppati secondo la suddivisione in classi alsss ( tabella 2 )  . classe naa otto / 12 pazienti ( 66 , 7% ) presentavano alterazioni deglutitorie identificabili alla vdfg . 
le immagini dimostrano la presenza di fenomeni di penetrazione intra - deglutitoria ( a , freccia ) conseguente ad un ritardato movimento dellepiglottide con successiva aspirazione in trachea ( b , asterisco )  . 
nessuno di questi pazienti ha accusato accessi di tosse durante lesame . invitando i pazienti a deglutire con il capo in posizione flessa stato possibile evidenziare la scomparsa dei fenomeni di penetrazione intra - deglutitoria , mentre solo un paziente con penetrazione post - deglutitoria ha giovato del cambiamento posturale . 
in nessun paziente del gruppo naa sono state dimostrate alterazioni del movimento dellosso ioide o della contrazione del muscolo crico - faringeo , n assunzione spontanea di posture facilitanti latto deglutitorio . classe epp in 5 / 7 ( 71 , 4% ) pazienti del gruppo eep sono state riscontrate alterazioni della fase orale della deglutizione con riduzione della motilit della lingua . 
infine 3 ( 42 , 8% ) pazienti mostravano fenomeni di penetrazione post - deglutitoria , 1 paziente ( 14 , 3% ) fenomeni di penetrazione intra - deglutitoria e 1 ( 14 , 3% ) di penetrazione pre - deglutitoria . 
precoce passaggio del bolo in faringe con verniciamento dellepiglottide ( freccia bianca ) e dei seni piriformi ( punta di freccia ) e conseguente penetrazione del bolo in laringe ( freccia grigia )  . the neh group were there alterations in hyoid elevation or cricopharyngeal contraction , nor were spontaneous compensatory manoeuvres observed . eep class in 5 / 7 patients ( 71.4% ) in the eep group , alterations of the oral phase of swallowing were encountered , with a reduction in lingual motility . 
in four of these ( 57.1% ) , triggering of the oral phase of swallowing was delayed due to lingual motility alterations and stasis of the bolus in the oral cavity , whereas in one patient , nonpropulsive movements of the tongue were present , which provoked early triggering of the oral phase that , once begun , proceeded regularly . 
incontinence of the labial rhyme ( a , arrow ) , leakage from the back of the mouth in the oral phase ( b , arrow ) and postdeglutitive penetration ( c , arrow )  . 
le immagini mostrano lincapacit a contenere il bolo nel cavo orale ( a , freccia ) con precoce passaggio in faringe ( b , freccia ) e penetrazione del bolo ( c , freccia )  . 
nelle prove con diversi atteggiamenti posturali si evidenzia la riduzione dei fenomeni di penetrazione ( d , freccia ) nella posizione del capo flesso , e la loro persistenza ( e , freccia ) nella deglutizione a capo esteso . 
la deglutizione di un bolo di maggiore consistenza ( f , freccia ) determina una lieve riduzione dei fenomeni di penetrazione . in one patient ( 14.3% ) , hyoid elevation was reduced , whereas in another ( 14.3% ) , there was an associated incomplete epiglottic tilting . 
in no case were there significant alterations to cricopharyngeal contraction , nor were there cases of coughing fits due to aspiration or penetration of the bolus . dcc class all patients in the dcc class presented alterations in both phases of swallowing due to extensive changes in lingual motility and contraction and coordination of the pharyngeal muscles . 
none of these patients experienced coughing fits as a result of penetration or aspiraspontaneamente il capo durante latto deglutitorio con conseguente riduzione dei fenomeni di aspirazione e / o penetrazione . 
invitando i pazienti ad assumere adeguate posture durante la deglutizione , si evidenziato un miglioramento del quadro radiologico nel paziente con penetrazione intra - deglutitoria e in uno dei due pazienti con aspirazione del bolo . nessun cambiamento stato apprezzabile nel secondo paziente con aspirazione del bolo . 
tutti i parametri presi in esami in questo studio si presentavano alterati con aspirazione in trachea e nel bronco destro gi un bolo di 5 ml . lassunzione di posture dedicate durante la deglutizione non ha determinato sostanziali modificazioni del quadro radiologico deglutitorio . in generale , riunendo i dati di tutti i 23 pazienti dello studio sono stati individuate alterazioni della fase orale della deglutizione in 17 pazienti ( 73 , 9% ) , alterazioni della fase fa1181 g . 
patient with head flexed during swallowing of high - density contrast mediuin this position the epiglottic tilt was improved , and subsequently aspiration into airways was reduced ( a , yellow arrow )  . 
la delgutizione a capo flesso in avanti , eseguita con bario ad alta densit , mostra la riduzione dellampiezza dei fenomeni di penetrazione ( a , freccia gialla ) del bolo rispetto alla deglutizione a capo in posizione neutra ; la deglutizione a capo esteso invece determina un incremento della penetrazione del bolo in laringe ( b , freccia bianca )  . 
swallowing with the head extended brought no improvement ; on the contrary , it led to deeper aspiration in one patient . 1182 ringea in 19 ( 82 , 6% )  . 
in 14 pazienti ( 60 , 9% ) stato inoltre possibile identificare la presenza di fenomeni di penetrazione ( 1 pre - deglutitoria , 5 intra - deglutitoria e 8 post - deglutitoria ) ed in 5 ( 21 , 7% ) fenomeni di aspirazione intra - deglutitoria . 
la deglutizione a capo flesso in avanti ha determinato sostanziali miglioramenti nei pazienti con penetrazione e / o aspirazione intra - deglutitoria ed in un paziente con penetrazione post - deglutitoria . 
lassunzione della postura a capo esteso non ha determinato miglioramenti del quadro radiologico , determinando , al contrario , un maggiore approfondimento del grado di aspirazione in un paziente . analizzando la distribuzione dellet nelle quattro classi dello studio mediante il test di student non stata riscontrata alcuna differenza significativa ( p > 0 , 05 )  . 
abbiamo anche differenziato i pazienti che lamentavano lievi ed iniziali alterazioni deglutitorie ( classe naa ) dai pazienti che lamentavano disfagia di grado moderato e severo ( classi eep , dcc e nft ) , valutandone la differenza statistica con il test esatto di fisher . 
this neurodegenerative form is characterised by the presence of complex symptoms , which at times are common to different forms [ 2 ] , thus making differential diagnosis difficult [ 16 , 17 ]  . 
dysphagia is , in fact , the most common and significant aspect of the bulbar form of the disease , as this can lead to nutritional deficit and death if not adequately treated [ 18 , 19 ]  . 
 [ 13 ] formulated a classification ( alsss ) that differentiates patients on the basis of dysphagia severity and has proved useful in assessing disease progression . various studies have demonstrated the importance of vfss in the diagnosis of dysphagia in relation to a number of diseases [ 510 , 2023 ] and have obtained a good correlation between radiological findings and patients alsss class [ 24 , 25 ]  . 
in contrast , there were no statistically significant differences between groups with respect to age distribution ( p > 0.05 ) nor between the neh group and the other groups with respect to the pharyngeal phase of swallowing and the possible presence of penetration and / or aspiration of the bolus into the airways ( p = 0.59 in both cases )  . the absence of statistical significance regarding age distribution was foreseeable in that disease onset is prevalent in the second or third decade of life and has an unfavourable prognosis and limited life expectancy [ 1 ]  . 
the difference in alterations in the oral phase of swallowing between neh patients and the other groups may be explained by the fact that as long as the oral phase is normal , the patients perceive no significant disturbances , becoming accustomed to and minimising the symptoms of dysphagia . 
this process of tolerance , however , is not present in the advanced stages of the disease when dysphagia becomes so disabling that it causes prodiscussione la sla , descritta per la prima volta da charcot nel 1869 [ 15 ] una malattia neurologica a prognosi infausta causata dalla perdita progressiva delle cellule delle corna anteriori del midollo spinale e dei motoneuroni dei tratti cortico - spinali . 
questa forma neurodegenerativa si caratterizza per la presenza di sintomi complessi e a volte comuni a diverse forme [ 2 ] , rendendo difficoltosa la diagnosi differenziale [ 16 , 17 ]  . 
proprio la disfagia laspetto pi comune e rilevante della forma bulbare della malattia , potendo determinare deficit nutrizionali tali da condurre allexitus se non adeguatamente trattati [ 18 , 19 ]  . 
al fine di classificare i pazienti affetti da sla e di programmarne la terapia , hillel e collaboratori hanno formulato una classificazione ( alsss ) che distingue i pazienti in base alla gravit del grado di disfagia , dimostrandosi utile anche per la valutazione della progressione della malattia . 
 diversi autori hanno dimostrato limportante ruolo svolto dalla vdfg nella diagnosi della disfagia in vari processi patologici [ 510 , 2023 ] , ottenendo una buona correlazione fra il riscontro radiologico e la classe alsss di appartenenza dei pazienti [ 24 , 25 ]  . 
abbiamo correlato la classe di appartenenza dei singoli pazienti intervistati alle alterazioni riscontrabili allesame videofluorografico , e dai dati del nostro studio stata apprezzata una differenza statisticamente significativa tra il gruppo di pazienti naa e quello composto dai pazienti degli altri gruppi riguardo le alterazioni della fase orale ( p = 0 , 036 )  . 
viceversa non vi sono state differenze statisticamente significative fra i diversi gruppi in relazione alla distribuzione in et ( p > 0 , 05 ) e fra il gruppo naa ed i restanti gruppi in relazione alle alterazioni della fase faringea della deglutizione e alla eventuale presenza di fenomeni di penetrazione e / o aspirazione del bolo alimentare nelle vie aeree ( p = 0 , 59 in entrambi i casi )  . 
la mancata significativit statistica della distribuzione per et nelle diverse classi era prevedibile , dal momento che la malattia insorge gi dalla ii - iii decade di vita ed ha prognosi infausta con breve attesa di vita [ 1 ]  . 
la differenza nelle alterazioni della fase orale della deglutizione fra i pazienti naa e gli altri gruppi potrebbe invece essere spiegata dal fatto che fin quando lattivit orale della deglutizione regolare il paziente non avverte disturbi significativi , assuefacendosi e minimizzando i sintomi della disfagia . 
questa assuefazione , al contrario , non si realizza nelle fasi avanzate della malattia quando la disfagia diviene talmente invalidante da determinare profonde modificazioni della dieta e dello stato nutrizionale del paziente . 
si pu quindi dedurre che le alterazioni della fase orale della deglutizione sono le prime ad essere avvertite dai pazienti , anche se si manifestano tardivamente , cio quando sia la fase faringea della deglutizione sia la capacit di protezione delle vie aeree da parte delle strutture laringee sono compromesse . 
it is therefore likely that alterations to the oral phase of swallowing are the first to be noticed by patients , even if they manifest late , that is , when both the pharyngeal phase of swallowing and the ability to protect the airways with the laryngeal structures are already compromised . 
in fact , analysis of individual data from our study revealed a discrepancy between clinical symptomatology , assigned objectively on the basis of the questions put to the patients and expressed by the patient belonging to a particular class according to hillel , and the presence of swallowing alterations demonstrated with vfss . this was particularly evident in the neh and eep classes , whereas the correlation appeared greater in the higher classes . 
in particular , in the neh class , bolus penetration was present in eight patients and aspiration in one patient , and in the eep class , penetration was present in five patients and aspiration in one patient . 
only in one of these patients was the cough reflex triggered by the passage of bolus into the airways . indeed the absence of the cough reflex can lead to an increase in morbidity and mortality , thus placing the patients at greater risk of recurrent episodes of aspiration pneumonia , which in patients suffering from nutritional deficit can even lead to death [ 26 , 27 ]  . 
this can be explained by the fact that in most cases , the amount of bolus passing into the pharynx was limited , with most of the retention in the valleculae and posterior portion of the epiglottis . 
indeed , predeglutitive penetration was the result of bolus leakage into the pharynx when the laryngeal aperture was not protected by laryngeal elevation or epiglottic tilting . in contrast , in cases of intradeglutitive penetration and / or aspiration , the cause was to be found in reduced hyoid elevation and epiglottic tilting and reduction in contraction of the pharyngeal constrictor muscles . lastly , postswallowing penetration and / or aspiration was the result of bolus stasis in the valleculae and pyriform si1184 somministrate ai pazienti ed espressa dallappartenenza ad una specifica classe secondo hillel , e la presenza di alterazioni deglutitorie evidenziabili allesame vdfg . 
in particolare nella classe haa 8 pazienti mostravano penetrazione ed 1 paziente aspirazione del bolo , mentre nella classe eep la penetrazione era presente in 5 pazienti e fenomeni di aspirazione in 1 paziente . 
 proprio la mancata comparsa del riflesso tussigeno pu comportare un incremento dei tassi di morbosit e mortalit , ponendo i pazienti in una condizione di elevato rischio per lo sviluppo di episodi ricorrenti di polmonite ab ingestis che , in pazienti debilitati per il deficit nutrizionale , possono anche portare allexitus [ 26 , 27 ]  . 
 per quanto riguarda la valutazione delle singole alterazioni riscontrate nel gruppo di studio , le alterazioni della fase orale della deglutizione sono conseguenti alla comparsa di movimenti non propulsivi della lingua in 13 / 23 pazienti ( 56 , 5% ) con ritardato innesco della fase orale della deglutizione , ed al ristagno del bolo nel cavo orale in 8 / 23 pazienti ( 34 , 8% )  . 
ci spiegabile dal fatto che nella maggior parte dei casi il passaggio del bolo in faringe stato di lieve entit , raccogliendosi , per lo pi , nelle vallecule glosso - epiglottiche e nel dorso dellepiglottide . 
le alterazioni della fase faringea , invece , sono state causate prevalentemente da una riduzione dellattivit contrattile del faringe in 18 / 23 pazienti ( 78 , 3% ) e dalle alterazioni del movimento del laringe e dellepiglottide in 10 / 23 pazienti ( 43 , 5% )  . 
infatti , i fenomeni di penetrazione pre - deglutitoria sono stati conseguenti ad un precoce passaggio del bolo in faringe , quando lhaditus laringeo non viene protetto dal movimento di escursione della laringe e dellepiglottide . 
invece , nei casi di penetrazione e / o aspirazione intra - deglutitoria la causa da ricercarsi nellalterato movimento dellosso ioide e dellepiglottide e nella riduzione della capacit contrattile dei muscoli costrittori del faringe . 
in questo caso , similmente a quanto avviene nella penetrazione pre - deglutitoria , il bolo pu passare in laringe in una fase in cui lhaditus laringeo non protetto dal movimento di escursione della laringe e dellepiglottide . 
in accordo con i dati della letteratura [ 28 , 29 ] , i 19 pazienti che mostravano fenomeni di penetrazione e / o aspirazione sono stati valutati con bolo di diversa densit e consistenza al fine di riprodurre la consistenza dei cibi compresi nella normale g . 
in this case , in a similar manner to that seen in predeglutitive penetration , bolus can pass into the larynx in a phase in which the laryngeal aperture is not protected by laryngeal elevation and epiglottic tilting . 
in agreement with the literature [ 28 , 29 ] , the 19 patients who displayed penetration and / or aspiration were assessed with boluses with different densities and consistencies with the aim of reproducing the consistency of food included in the patients normal diet . 
in all cases , the patients rated the consumption of high - density barium the easiest , and this preference was justified by the greater viscosity of the bolus , which facilitates compaction in the mouth and transport to the pharynx . 
only in the patient in the ntf group was a solution of water and hydrosoluble iodinated contrast material used to reduce the risks of massive bolus aspiration into the airways . 
this approach proved just as diagnostic as the use of boluses with barium at differing densities , enabling adequate assessment of swallowing alterations . previous studies have already shown how posture changes can improve swallowing in dysphagic patients [ 30 ]  . 
flexing the head forwards lead to significant swallowing improvements in the cases of intraand postdeglutitive penetration and / or aspiration , whereas there were no changes in the case of predeglutitive penetration . 
in contrast , swallowing with the head extended increased the degree of aspiration in one patient in the dcc group and brought no changes in the radiological picture in the other patients although vfss has already been used to assess patients affected by als classified according to alsss [ 24 , 25 ] , this is the first study to our knowledge that highlights the possible compensatory mechanisms that can be implemented to improve swallowing in these patients . with regard to cricopharyngeal muscle activity , data in the literature appear to disagree in that some studies report an elevated frequency of patients with evidence of muscular hypertonia [ 31 , 32 ] , whereas others report normal contraction [ 33 ]  . 
we therefore feel that further studies are required to clarify discrepancies in the literature regarding involvement of this important muscle in the clinical course of als . there are a number of limitations to our study . 
firstly , the patient population was not evenly distributed across the various classes : however , the disease has a low incidence , and its progressive and rapid clinical course often does not allow patients belonging to the dcc and ntf classes to undergo dynamic examinations . 
in tutti i casi i pazienti hanno giudicato pi agevole lassunzione del bario ad alta densit , e questa preferenza pu essere giustificata dalla maggiore viscosit del bolo che rende pi facile il suo compattamento nel cavo orale e il successivo passaggio in faringe . 
solo nel paziente del gruppo nft si preferito , per ridurre i rischi conseguenti ad una possibile massiva aspirazione del bolo nelle vie aeree , utilizzare una soluzione di acqua e mezzo di contrasto iodato idrosolubile . 
dai dati del nostro studio si evince come alcuni pazienti tendono ad assumere spontaneamente delle posture volte alla facilitazione dellatto deglutitorio , con riduzione dei fenomeni di penetrazione e / o aspirazione . per i pazienti che non presentano spontaneamente atteggiamenti posturali di compenso si provveduto ad acquisire sequenze cineradiografiche deglutitorie invitando i pazienti a flettere ed estendere il capo . 
la flessione del capo in avanti ha determinato significativi miglioramenti dellatto deglutitorio nei casi di penetrazione e / o aspirazione intrae post - deglutitoria del bolo , mentre non ha determinato modificazioni nei casi di penetrazione pre - deglutitoria . 
viceversa , latteggiamento deglutitorio con il capo esteso ha determinato un approfondimento del grado di aspirazione in un paziente della classe dcc e nessuna modificazione del quadro radiologico negli altri pazienti . 
 sebbene in letteratura siano gi presenti degli studi di valutazione videofluorografica della deglutizione in pazienti affetti da sla classificati secondo la alsss [ 24 , 25 ] , a conoscenza dellautore questo il primo lavoro che evidenzia i possibili meccanismi di compenso posturale che possono essere intrapresi per migliorare la capacit deglutitoria di questi pazienti . 
 riguardo lattivit del muscolo crico - faringeo i dati della letteratura appaiono discordanti evidenziando in alcuni casi lelevata frequenza di pazienti con evidenza di ipertono muscolare [ 31 , 32 ] , o aspetto contrattile normale [ 33 ]  . 
solo in un paziente del nostro studio stata riscontrata unalterazione funzionale del muscolo crico - faringeo ; riteniamo che ulteriori studi vadano eseguiti per chiarire la divergenze dei dati in letteratura riguardo il coinvolgimento di questo importante muscolo nellevoluzione della sla . 
innanzi tutto il campione di pazienti incluso non omogeneamente distribuito fra le diverse classi , ma la malattia presenta bassa incidenza , inoltre la sua evoluzione rapida e progressiva spesso non consente ai pazienti appartenenti alle classi dcc e nft di sottoporsi ad esami dinamici . 
altra limitazione del nostro studio data dal fatto che i pazienti non sono stati sottoposti ad esame manometrico del faringe , per meglio correlare il riscontro sintomatologico con le alterazioni fun1185 g . 
nonetheless , as the study aimed at identifying swallowing alterations in patients affected by als in relation to their alsss classification , we feel that manometric assessment was not indispensable . zionali e con lo studio videofluorografico . 
tuttavia il presente studio finalizzato allindividuazione delle alterazioni deglutitorie in pazienti affetti da sla in relazione alla loro appartenenza alle diverse classi di hillel , rendendo , a nostro avviso , non indispensabile la valutazione manometrica . conclusions in patients affected by als , swallowing alterations are very frequent and affect both the oral and pharyngeal phases of swallowing . 
vfss therefore proved to be a technique with high diagnostic capabilities in the assessment of swallowing dysfunction of patients with als in that it is able to identify both the degree and causes of swallowing impairment . 
vfss is therefore a useful instrument in the assessment of the degree of dysphagia , both in preparation for speech therapy and in the follow - up of patients with als . conclusioni nei pazienti affetti da sla le alterazioni deglutitorie sono molto frequenti ed interessano entrambe le fasi della deglutizione , orale e faringea . 
dai dati ottenuti si pu affermare come nelle fasi iniziali la sintomatologia riferita , standardizzata dallappartenenza dei singoli pazienti ad una specifica classe di hillel , tenda a sottostimare le alterazioni deglutitorie proprie della sla . 
lo studio videofluorografico della deglutizione si quindi dimostrato una tecnica dotata di elevata capacit diagnostica per la valutazione dei deficit deglutitori dei pazienti affetti da sla , essendo in grado di identificarne il grado di compromissione e le cause determinanti . 
the purpose of this paper is to help refine the differential diagnosis among these diseases through the use of multidetector ct ( mdct ) imaging . riassunto alcune malattie di non frequente riscontro interessano localmente o diffusamente le vie aeree centrali . 
in questo gruppo di patologie sono incluse : la granulomatosi di wegener , la policondrite ricorrente , la tracheobroncopatia osteocondroplastica , lamiloidosi , la papillomatosi , il rinoscleroma , la sarcoidosi e la tubercolosi . 
lo scopo del seguente pictorial essay quello di tracciare la diagnosi differenziale fra queste malattie mediante imaging tc multidetettore ( tcmd )  . key words trachea bronchi ct stenosis parole chiave trachea bronchi ct stenosi introduction introduzione wall thickening and airways stenosis may be associated with lung diseases or with systemic diseases of varying aetiology : infectious , postinfectious , inflammatory , idiopathic and , rarely , neoplastic . 
computed tomography ( ct ) and bronchoscopy are still the techniques of choice for the study of the central airways . axial ct imaging is sufficient in most cases , as it provides information on the airway lumen and walls and on extraluminal structures . 
besides , where multidetector ct ( mdct ) scanners are available , it is easy in day - today practice to add isotropic multiplanar reconstructions ( mpr ) ( straight or curvilinear ) that are useful for demonstrating the presence of stenoses and increasing accuracy when evaluating the extent of wall abnormalities . 
volumerendering ( vr ) techniques provide images that are more immediately comprehensible to bronchoscopists than are congli ispessimenti parietali e le stenosi delle vie aeree possono essere associati a patologie polmonari o a malattie sistemiche a diversa eziologia : infettiva , post - infettiva , infiammatoria , idiopatica , e raramente neoplastica . 
inoltre , qualora si disponga di apparecchi tc multidetettore ( tcmd ) , risulta semplice nella pratica quotidiana aggiungere ricostruzioni multiplanari isotropiche ( rettilinee o curvilinee ) che sono utili nel dimostrare la presenza di stenosi e nel rendere pi accurata la valutazione 1132 a . 
although it cannot replace diagnostic sampling and does not have the interventional capabilities of bronchoscopy , 3d bronchoscopic imaging can help select candidates for bronchoscopy and may prove essential where bronchoscopy is inconclusive or unable to cross a particularly tight stenosis . the purpose of this pictorial essay is to illustrate , through the use of modern ct imaging techniques , the main characteristics of central - airway alterations that can be observed in wegeners granulomatosis , relapsing polychondritis , tracheobronchopathia osteochondroplastica , amyloidosis , papillomatosis , rhinoscleroma , sarcoidosis and tuberculosis . wegeners granulomatosis wegeners granulomatosis is a disease of unknown aetiology characterised by necrotising granulomatous vasculitis that may involve all organs and , in particular , the upper and lower airways , lungs and kidneys [ 1 ]  . 
tracheobronchial involvement occurs with a frequency between 16% and 23% [ 2 , 3 ] and is often a late complication of the disease , although rare cases of isolated involvement of the tracheobronchial tree have also been reported [ 14 ]  . 
 although chest radiography is also able to identify tracheal stenoses and / or wall thickenings ( especially in the subglottic region ) , these lesions are better characterised by ct . the most frequent ct finding is a nodule or eccentric parietal soft tissue mass associated with alterations of the tracheal rings , which may display calcifications or irregularities caused by erosion . 
further radiographic findings include parenchymal nodules generally bilateral and widely distributed cavitations , airspace consolidation , ground - glass opacities and unilateral / bilateral pleural effusion . relapsing polychondritis relapsing polychondritis is a systemic inflammatory disease , probably of autoimmune aetiology , characterised by inflammation episodes of the cartilage , with destruction and fibrosis . 
le tecniche di resa volumetrica ( volume - rendering techniques , vrt ) possono fornire immagini che sono pi immediate e comprensibili da parte dei broncoscopisti rispetto alle immagini assiali convenzionali ; queste tecniche forniscono un imaging 3d tracheobronchiale sia secondo prospettive esterne che interne ( broncoscopia virtuale )  . 
anche se non pu sostituire il campionamento diagnostico e le capacit interventistiche della broncoscopia , limaging broncoscopico 3d di aiuto nel selezionare i pazienti candidati alla broncoscopia e pu risultare fondamentale qualora la broncoscopia appaia inconcludente o non riesca a valicare una stenosi particolarmente serrata . lo scopo del presente pictorial essay quello di illustrare le caratteristiche principali , mediante moderno imaging tc , delle alterazioni delle vie aeree centrali che si osservano nella granulomatosi di wegener , policondrite ricorrente , tracheobroncopatia osteocondroplastica , amiloidosi , papillomatosi , rinoscleroma , sarcoidosi e tubercolosi . granulomatosi di wegener la granulomatosi di wegener una patologia ad eziologia sconosciuta , caratterizzata da una vasculite necrotizzante granulomatosa , che pu interessare tutti gli organi , con particolare predilezione per le alte e basse vie respiratorie , il polmone ed il rene [ 1 ]  . 
il coinvolgimento tracheale e bronchiale si presenta con una frequenza dal 16% al 23% [ 2 , 3 ] e rappresenta spesso una complicanza tardiva della malattia , sebbene siano stati riportati anche rari casi di isolato coinvolgimento dellalbero tracheo - bronchiale [ 14 ]  . 
flogosi e ulcerazioni , conseguenti allinfiammazione granulomatosa [ 5 ] , interessano la mucosa e la sottomucosa , mentre il coinvolgimento degli anelli cartilaginei meno comune , ma pu determinare deformazioni tracheali . 
il reperto tc pi frequente quello di un nodulo o massa di tessuto molle eccentrica parietale , associata ad alterazioni degli anelli tracheali che possono mostrare calcificazioni o irregolarit dovute allerosione . 
c ricostruzione in vr della stenosi tracheale . policondrite ricorrente la policondrite ricorrente una patologia infiammatoria sistemica a probabile eziologia autoimmune , caratterizzata da episodi di infiammazione del tessuto cartilagineo , con distruzione e fibrosi . 
le cartilagini delle orecchie , delle articolazioni e delle pinne nasali sono alcuni dei bersagli preferenziali della malattia ; il coinvolgimento delle vie respiratorie , pi frequentemente a carico della laringe e della parte superiore della trachea [ 7 ] , si osserva fino al 50% dei casi [ 8 ] , ed spesso associato ad una significativa morbilit e mortalit . la diagnosi di policondrite recidivante clinica e non richiede reperti istologici . 
le pareti mostrano quasi sempre the preferred sites of the disease ; the respiratory tract , more frequently the larynx and the upper trachea [ 7 ] , are involved in up to 50% of cases [ 8 ]  . 
ct is essential in establishing involvement of the respiratory tract because biopsy samples are difficult to obtain through bronchoscopy , which may encounter insurmountable obstacles and even exacerbate the inflammation . 
the use of expiratory scans is important because in most cases , they may identify areas of air trapping and bronchomalacia , which may be early , and the only , signs of disease . 
b limmagine di broncoscopia virtuale mostra chiaramente come la parete tracheale sia diffusamente tappezzata da noduli sottomucosi . mental bronchi , and rarely the larynx and subglottic area . they develop in the submucosa and often communicate with the tracheal perichondriu the nodules are generally 13 mm in size , [ 10 ] , but at advanced stages , they may coalesce to form plaque - like lesions that deform and obstruct the airways [ 11 , 12 ]  . 
i noduli hanno in genere dimensioni di 13 mm [ 10 ] , ma in fase avanzata la loro coalescenza pu dare origine a lesioni simili a placche , che provocano deformazione ed ostruzione delle vie aeree [ 11 , 12 ]  . le prime alterazioni radiologiche possono essere rappresentate da atelettasia o addensamenti su base infettiva per polmoniti ricorrenti . 
4a axial computed tomography image shows diffuse , calcified thickening of the walls of the main bronchi that does not involve the posterior wall in a patient affected by tracheobronchial amyloidosis . 
b curved coronal reconstruction shows some calcified nodules in the lower right lobe ( white arrow ) and an ipsilateral tracheal calcified wall thickening near the carina ( curved white arrow ) in a patient with systemic amyloidosis . 
4a limmagine tc assiale mette in evidenza un diffuso ispessimento calcifico delle pareti dei bronchi principali senza risparmio della parete posteriore , in un paziente affetto da amiloidosi tracheo - bronchiale . 
b in un paziente affetto da amiloidosi sistemica la ricostruzione curva sul piano coronale mostra alcuni noduli calcifici nel lobo inferiore destro ( freccia bianca ) ed un ispessimento parietale calcifico omolaterale della trachea in prossimit della carena ( freccia curva bianca )  . 
tracheobronchial involvement is the most common and is characterised by multiple submucosal and muscular deposits of amyloid plaques and nodules , which may cause wall atrophy [ 17 ]  . 
nonetheless , in 14% of patients , the amyloid deposit is isolated and may simulate a bronchial neoplasm [ 18 , 19 ]  . chest radiography may reveal a nodular and irregularly stenosing appearance of the tracheal lumen , but in 25% of cases , the study is negative [ 20 ]  . 
ct shows a nodular thickening or , more rarely , smooth , circumferential parietal thickening of the trachea and main bronchi , with luminal narrowing [ 21 , 22 ]  . 
there is also a possibility of iatrogenic transmission at the tracheal and pulmonary levels following tracheotomy and prolonged intubation with positive pressure ventilation . papillomas are benign but may undergo malignant transformation and become squamous cell carcinomas in 3%5% of cases [ 23 ]  . tracheal papilloma is usually multiple and generally caused by spread from the larynx ; the lower respiratory tract may also be affected , with cough , haemoptysis , asthma - like symptoms , recurrent pneumonia or atelectasis [ 24 , 25 ]  . 
progressive lung involvement leads to the appearance of nodules , cavitated nodules and cystic , air - filled lung lesions . rhinoscleroma rhinoscleroma is a chronic , progressive , granulomatous infection caused by klebsiella rhinoscleromatis , a gram - negative bacterium more frequently found in asia , north africa and central and south america . 
 1138 mulare una neoplasia endobronchiale [ 18 , 19 ]  . lesame radiografico del torace pu evidenziare un aspetto nodulare ed irregolarmente stenosante del lume tracheale , ma nel 25% dei casi lindagine risulta negativa [ 20 ]  . la tc mostra un ispessimento nodulare o , pi raramente , parietale circonferenziale liscio della trachea , dei bronchi , con restringimento del lume [ 21 , 22 ]  . 
a livello parenchimale si pu evidenziare una reticolazione interlobulare liscia o nodulare con opacit lineari intralobulari ( pattern interstiziale ) oppure multiple opacit rotondeggianti , ma anche uniche con diametro variabile sino ad alcuni cm ( pattern nodulare )  . papillomatosi la papillomatosi squamocellulare delle vie respiratorie una rara affezione , determinata da uninfezione da papilloma virus umano ( hpv11 - hpv6 ) , in genere acquisito alla nascita da madre infetta . 
i papillomi sono benigni , ma possono andare incontro a trasformazione maligna e diventare carcinomi squamosi nel 3%5% dei casi [ 23 ]  . il papilloma della trachea solitamente multiplo e determinato in genere da una disseminazione laringea ; si pu verificare anche un coinvolgimento del tratto respiratorio inferiore con comparsa di tosse , emottisi , sintomi simil asmatici , polmoniti ricorrenti o atelettasia [ 24 , 25 ]  . 
la progressiva estensione a livello polmonare determina la comparsa di noduli , noduli cavitati e lesioni polmonari cistiche a contenuto aereo . rinoscleroma il rinoscleroma una infezione cronica , progressiva , granulomatosa causata dal batterio gram negativo klebsiella rhinoscleromatis , di pi frequente riscontro in asia , nord africa e nellamerica centro - meridionale . 
it typically affects the hilar and mediastinal lymph nodes and lung parenchyma , but in 1%3% of cases , it may involve the larynx and trachea , mainly the upper subglottic portion . 
at a parenchymal level , millimetre - sized nodules with sharp margins and lymphatic distribution may be detected ( bronchovascular bundle , interlobular septa and subpleura )  . tuberculosis ( tb ) the prevalence of tracheobronchial stenoses in tb ranges from 40% in autoptic studies of patients with tb to 10% in patients with tb who undergo bronchoscopy [ 27 ]  . 
on gross pathology , granulomatous masses , ulcerations , necrosis of the tracheobronchial walls and , finally , fibrotic stenoses may be prevalent , although these findings may often coexist . ct allows differentiation between the active phase of disease in which the trachea is stenotic with irregular wall thickening from the fibrotic phase in which the trachea is narrowed but has a smooth and normally thick wall . 
in addition , it visualises the extent of irregular and circumferential narrowing of tracheobronchial structures [ 28 ]  . conclusions modern diagnostic imaging and in particular mdct allows identification of stenoses in the central airways with greater accuracy than with conventional diagnostics , especially in the case of extensive , not particularly tight , stenoses . 
interessa tipicamente i linfonodi ilari e mediastinici ed il parenchima polmonare , tuttavia nell1%3% dei casi pu coinvolgere la laringe e la trachea , soprattutto nella porzione superiore sub - glottica . le stenosi tracheali possono essere determinate da formazioni granulomatose della mucosa o della sottomucosa che aggettano allinterno del lume o da compressione estrinseca ( linfonodi ingranditi , fibrosi mediastinica )  . 
a livello parenchimale si possono riscontrare noduli di dimensioni millimetriche e margini netti con distribuzione linfatica ( fascio broncovascolare , setti interlobulari e subpleurica )  . tubercolosi ( tbc ) nella tbc la prevalenza di stenosi tracheo - bronchiali varia dal 40% in casistiche autoptiche in pazienti con tbc al 10% nei pazienti con tbc sottoposti a broncoscopie [ 27 ]  . 
a seconda dello stadio della malattia , da un punto di vista anatomo - patologico possono prevalere formazioni granulomatose , ulcerazioni , e necrosi delle pareti tracheo - bronchiali e infine stenosi fibrotiche , anche se questi reperti spesso possono coesistere . la tc permette di distinguere la fase attiva della malattia , in cui la trachea stenotica con un ispessimento di parete irregolare , dalla fase fibrotica in cui la trachea ristretta , ma con una parete liscia e di spessore normale ; inoltre ben visualizzabile lestensione dei restringimenti irregolari e circonferenziali delle strutture tracheo - bronchiali [ 28 ]  . conclusioni la moderna diagnostica per immagini ed in particolare la tcmd consente lindividuazione delle stenosi delle vie aeree centrali con accuratezza superiore della diagnostica convenzionale specie per quanto riguarda stenosi estese e non molto serrate ; pu fornire una diagnosi precisa o quantomeno ridurre significativamente la gamma delle diagnosi differenziali ed integrare la valutazione fibrobroncoscopica . la tabella 1 riporta schematicamente le caratteristiche principali che pi spesso sono responsabili di stenosi tra1139 a . 
zompatori1 1section of radiology , 2section of respiratory diseases , department of clinical sciences , university of parma , barbieri ospedale maggiore di parma , via gramsci 14 , i - 43100 parma , italy 3department of radiology , university of chieti correspondence to : n . 
we analysed thin - section cts and pulmonary function tests ( pfts ) of six healthy subjects and 31 patients affected by lung fibrosis , including 17 with a usual interstitial pneumonia pattern ( uip group ) , and 14 with a predominant pattern of ground - glass opacities without honeycombing ( non - uip group )  . 
together with the histogram features , fibrosis ratio ( defined as the ratio of nonfibrotic ct lung volume divided by total ct lung volume ) contributed to objectively differentiate fibrotic lungs from normal lungs . 
the visual score is still the main radiological method of quantifying the extent of abnormalities in patients with uip , whilst the range of density 700 to 400 hu can be helpfully applied in a predominant pattern of ground - glass and reticular opacities without honeycombing . key words idiomatic interstitial fibrosis high resolution computed tomography pulmonary function test riassunto obiettivo . 
abbiamo analizzato scansioni tc a strato sottile di sei soggetti sani e di 31 pazienti con fibrosi polmonare , compresi 17 con un pattern di polmonite interstiziale usuale ( gruppo di uip ) e 14 con un pattern predominante di groundglass senza honey - combing ( gruppo non - uip )  . 
insieme agli istogrammi , lindice fibrotico volumetrico ( definito come il rapporto tra il volume di polmone non fibrotico e il volume polmonare totale ) ha contribuito nel differenziare in modo obiettivo i polmoni fibrotici dai polmoni normali . 
lo score visivo ancora il metodo radiologico principale per quantificare lestensione della patologia in pazienti con uip , mentre lintervallo di densit 700400 hu pu essere vantaggiosamente applicato in un pattern predominante a groundglass e reticolare senza honey - combing . parole chiave fibrosi interstiziale idiomatica tomografia computerizzata ad alta risoluzione test di funzionalit polmonare 1160 n . 
interstitial fibrosis is a nonspecific pathological endpoint that can occur as a consequence of granulomatous diseases , collagen vascular diseases , certain drug therapies and recurring exposure to organic and inorganic antigens . 
therefore , it is crucial to develop methods for quantitative imaging of the lung that allow one to diagnose early disease , follow - up disease progression and evaluate the effects of treatment . structure - function studies have shown that high - resolution computed tomography ( hrct ) has a crucial role in diagnosis and management of patients with iips and other interstitial disorders [ 14 ]  . 
by providing images of the entire lungs , hrct ( unlike histopathological evaluation ) represents a noninvasive tool for monitoring disease extent , and it can be also correlated with pfts , which provide , instead , a global statement of lung function . 
several studies including large numbers of idiopathic pulmonary fibrosis ( ipf ) patients reported strong correlations between histological findings and functional impairment [ 5 , 6 ] ; nevertheless , these are consistently weaker than correlations observed between lung function impairment and ct scores [ 3 , 79 ]  . previous studies on ct evaluation of lung fibrosis can be categorised as visual and computer - based assessment . 
despite the relevance of a radiologists interpretation , it is increasingly accepted that the human observer , without the aid of computer - based image evaluation tools , is poorly reproducible in quantifying extent of disease [ 10 ]  . 
 computer - aided diagnosis ( cad ) has been widely used to quantify extent of emphysema ; nonetheless , quantitative cad might also be used to better evaluate the extent of lung fibrosis . 
in particular , in order to assess complex lung patterns , fractal and texture - based analyses as well as multiple neural networks have been used [ 1114 ]  . 
therefore , we still need a unique objective method for quantifying lung fibrosis and in particular the most aggressive idiopathic variants . we studied two different groups of patients with lung fibrosis to evaluate whether simple ct computer scores ( histogram features , ranges of density and one novel volumetric index ) provide a more precise discrimination between normal and pathologic areas of the lungs and a correlation between morphological and functional indices better than the visual score does . patients and methods subjects six healthy controls and 31 individuals with lung fibrosis la fibrosi polmonare pu presentarsi secondo diverse configurazioni cliniche . 
la fibrosi interstiziale uno stadio patologico terminale non specifico , che pu verificarsi come conseguenza di malattie granulomatose , connettivopatie , alcune terapie farmacologiche e ricorrente esposizione ad antigeni organici ed inorganici . 
i medici che hanno in cura i pazienti affetti da fibrosi polmonare sono frequentemente tenuti a prendere decisioni complesse riguardo al trattamento : se e quando iniziarlo , intensificarlo , o interromperlo . 
perci fondamentale sviluppare metodi di imaging quantitativo del polmone che permettano di diagnosticare precocemente la malattia , seguirne il decorso e valutare gli effetti della terapia . studi morfologici e funzionali hanno dimostrato che la tc ad alta risoluzione ( hrct ) ha un ruolo fondamentale nella diagnosi e nella gestione dei pazienti affetti da pii ed altri disordini interstiziali [ 14 ]  . 
fornendo immagini dei polmoni per intero , la hrtc ( a differenza della valutazione istopatologica ) rappresenta uno strumento non invasivo per il monitoraggio dellestensione della malattia e pu anche essere correlata con ( pfr ) , che invece forniscono solo una valutazione globale della funzionalit polmonare . 
diversi studi che includevano un numero considerevole di pazienti con fibrosi polmonare idiopatica ( ipf ) , hanno dimostrato forti correlazioni fra i reperti istologici e lalterazione funzionale [ 5 , 6 ] ; tuttavia , queste sono consistentemente pi deboli di quelle osservate tra lalterazione funzionale e gli score tc [ 3 , 79 ]  . 
nonostante limportanza dellinterpretazione del radiologo , si sempre pi concordi nel ritenere che la semplice osservazione , senza laiuto di strumenti di valutazione dellimmagine assistiti dal computer , sia scarsamente riproducibile nel quantificare lestensione della patologia [ 10 ]  . la diagnosi assistita computerizzata ( cad ) , che stata ampiamente utilizzata per quantificare lestensione dellenfisema , pu essere anche impiegata per valutare lestensione della fibrosi polmonare . 
in particolare , per analizzare i pattern pi complessi del polmone , sono stati utilizzati sistemi di analisi frattale , della texture e anche reti neurali multiple [ 1114 ]  . 
the control group included three men and three women ( mean age 46 years , range 2962 )  . all were nonsmokers , had no history of pulmonary disease , had normal lung function and were taking no medication . thirty - one patients , 19 men and 12 women ( mean age 64 years , range 3483 ) were retrospectively selected to obtain two groups of patients with usual interstitial pneumonia ( uip ) , and non - uip pattern . 
all patients were referred for thin - section ct scan of the lung on the basis of a clinicalfunctional restrictive presentation and a positive chest radiograph compatible with diffuse interstitial lung disease . uip pattern was defined according to well - established criteria and consistent mainly with reticular lines , traction bronchiectasis and honeycombing in a basal - predominant distribution [ 15 ] ; diagnosis was histological in five cases ( uip group , n = 17 )  . 
in the non - uip group ( n = 14 ) , six patients were affected by chronic extrinsic allergic alveolitis ( eaa ) and eight patients by lung fibrosis of undetermined cause despite accurate clinical , functional and radiological assessment . 
patients with asbestos exposure , sarcoidosis , connective tissue diseases and prior environmental exposure to any fibrogenic agent were not included in the study . lung - function testing , ct examination and lung biopsy had been undertaken for clinical reasons under request of patients clinicians . 
 ct and computer analysis all patients underwent thin - section ct examination of the entire thorax using a 16 - slice scanner ( sensation 16 , siemens medical solutions , forchheim , germany ) without i.v. 
scanning parameters were : 120 kvp , 100 mas , rotation time 0.5 s , feed / rotation 18 mm , the smallest possible field of view ( fov ) covering both lungs , bone filter and collimation 0.75 mm with 1 - mm reconstruction . 
the images were printed , adopting a window level of 600 hu and a window width of 1 , 600 hu for the parenchyma . to evaluate presence and extent of lung abnormalities , two chest radiologists blindly and independently evaluated all ct scans using three scans at preestablished levels : the origin of the great vessels , the carina and the right inferior pulmonary ve the radiologists were unaware of the patients lung functional data . 
the overall extent of these abnormalities was determined for each entire lung using a four - point scale ( 0 = no involvement ; 1 = 1%25% involvement ; 2 = 26%50% ; 3 = 51%75% ; and 4 = 76%100% )  . these data were used to calculate interobserver agreement . subsequently , a consensus reading was performed to obtain only one visual score for the disease extent / functional correlations . 
trentuno pazienti affetti da fibrosi polmonare , 19 maschi e 12 femmine ( et media di 64 anni , range 3483 ) , sono stati selezionati retrospettivamente in modo da ottenere due gruppi di pazienti rispettivamente con pattern di tipo polmonite interstiziale usuale ( uip ) , e pattern non uip . 
tutti i pazienti sono stati segnalati per lesecuzione di indagine hrtc sulla base di una presentazione clinico - funzionale di tipo restrittivo e di una radiografia del torace positiva , compatibile con quadro di polmonite interstiziale diffusa . il quadro di uip stato definito secondo i criteri ben consolidati letteratura che prevedono essenzialmente allhrtc la presenza di addensamenti reticolari , bronchiectasie da trazione ed honey - combing a distribuzione prevalentemente basale [ 15 ] ; la diagnosi stata supportata da dati istologici ottenuti con biopsia chirurgica in 5 casi ( gruppo uip , n = 17 )  . 
nel gruppo non uip ( n = 14 ) , 6 pazienti erano affetti da alveolite allergica estrinseca cronica ( aee ) , e 8 pazienti da fibrosi polmonare di causa indeterminata . 
pazienti con esposizione allasbesto , malattie del tessuto connettivo e precedente esposizione ambientale ad agenti fibrogenici non sono stati inclusi nel gruppo di studio . le pfr , lesame tc , e la biopsia polmonare sono stati eseguiti per ragioni cliniche previa richiesta del medico curante . 
i pazienti hanno fornito anche il loro consenso informato allo studio . tc e analisi computerizzata tutti i pazienti sono stati sottoposti a scansioni tc a strato sottile di tutto il torace usando uno scanner a 16 strati ( sensation 16 - siemens medical solutions , forchheim , germania ) , senza iniezione endovenosa del mezzo di contrasto . 
il sincronizzatore respiratorio non stato utilizzato ; gli esami sono stati eseguiti in una singola apnea ( inspiratoria completa , con decubito prono soltanto per i soggetti patologici ) , dopo aver adeguatamente istruito i pazienti . 
i parametri di scansione utilizzati erano : 120 kvp , 100 mas , tempo di rotazione 0 , 5 s , avanzamento / rotazione 18 mm , campo di vista pi piccolo possibile ( fov ) che comprendesse entrambi i polmoni , filtro di convoluzione per tessuti duri , collimazione 0 , 75 mm con ricostruzioni di 1 millimetro di spessore . 
le immagini sono state stampate applicando una finestra con livello di 600 hu e ampiezza di 1600 hu . al fine di valutare la presenza e lestensione delle lesioni , 2 radiologi toracici hanno esaminato in doppio cieco tutte le scansioni tc utilizzando tre livelli prestabiliti : lorigine dei grandi vasi , la carena tracheale ed alla vena polmonare inferiore di destra . 
b applicazione della maschera di densit con intervallo di 700400 hu . we uses 1 - mm sections for visual score , which were subsequently scored semiautomatically by the system software ( pulmo - siemens ) that allows lung - density and structure testing . 
after obtaining frequency histograms of thin - section ct scans , relative data were transferred into a different software package that calculated indices , such as mean lung attenuation ( mla ) , skewness ( representing the extent of asymmetry of histograms ) and kurtosis ( representing the peakness of histograms )  . 
finally , using the entire ct data set , we constructed a fibrosis ratio , which we define as the ratio of the non - fibrotic ct lung volume ( 1 , 024 to 500 hu ) divided by total ct lung volume ( 1 , 024 to 200 hu )  . pulmonary function tests lung function was evaluated within 1 week from the hrct exam by a flow - sensing spirometer and a body plethysmograph connected to a computer for data analysis . 
the following parameters were recorded and expressed as a percentage of the theoretical values : total lung capacity ( tlc ) , forced expiratory volume in 1 s ( fev1 ) and forced vital capacity ( fvc )  . 
diffusing capacity for carbon monoxide ( dlco ) was evaluated during a single breath - hold and considered valid only if the inspiratory volume was at least 90% of the forced vc . 
finally , a composite physiologic index ( cpi ) was derived in the uip pattern group 7 . the formula for cpi was as follows : conoscenza dei parametri funzionali dei pazienti . 
lestensione globale di queste anormalit stata determinata per ogni polmone usando una scala a 4 punti ( 0 = assenza delle lesioni ; 1 = 1%25% di estensione ; 2 = 26%50% ; 3 = 51%75% ; 4 = 76%100% )  . 
questi dati sono stati utilizzati per calcolare laccordo interosservatore ; successivamente stata fatta una lettura consensuale per ottenere un solo score visivo da porre in correlazione con i dati funzionali . 
stata inoltre valutata leventuale presenza di enfisema , di noduli , delle bronchiectasie da trazione e la distribuzione delle lesioni . le stesse sezioni da 1 mm usate per lo score visivo , sono state successivamente analizzate semi - automaticamente da un software ( pulmo - siemens ) che valuta la densit e la struttura del polmone . 
dopo aver ottenuto gli istogrammi di densit delle sezioni selezionate , i relativi dati sono stati analizzati mediante un secondo software che ha calcolato indici come la attenuazione polmonare media ( mla ) , lo skewness ( rappresentante il grado di asimmetria degli istogrammi ) e la kurtosis ( rappresentante il grado del picco degli istogrammi )  . 
three patients la funzionalit polmonare stata valutata entro una settimana dallesame hrtc mediante uno spirometro rilevatore di flusso ed un pletismografo , collegati ad un calcolatore per analizzarne i dati . 
questi sono stati espressi come percentuale dei valori teorici : capacit polmonare totale ( cpt ) , volume espiratorio forzato in 1 secondo ( fev1 ) , capacit vitale forzata ( cvf )  . 
la capacit di diffusione del monossido di carbonio ( dlco ) stata valutata durante un singolo respiro e considerata valida solo se il volume inspiratorio risultasse almeno pari al 90% della cvf . 
la formula per il cpi era la seguente : 91 ( 0 , 65 percentuale del predetto dlco ) ( 0 , 53 percentuale del predetto cvf ) + ( 0 , 34 percentuale del predetto fev1 ) analisi statistica i dati dei due gruppi sono stati comparati il t test di student . un valore di p < 0 , 05 stato considerato statisticamente significativo . 
il coefficiente di correlazione lineare di pearson stato usato per esaminare la correlazione tra ciascuno degli indici tc , gli score visivi e i test di funzionalit polmonare , ovvero il dlco e cpi . 
 uip , polmonite interstiziale usuale ; mla , densit media polmonare ; dlco , capacit di diffusione del monossido di carbonio ; cpi , indice composito funzionale also had coexisting mild to severe centrilobular emphysema predominant in the upper lobes . 
la mla , la skewness e la kurtosis degli istogrammi di densit sono risultati in media rispettivamente : 758 , 4 hu47 , 2 , 10 , 4 , 82 , 5 . 
le medie degli intervalli di densit pi basso ( 700200 hu ) , intermedio ( 700400 hu ) e pi alto ( 500200 hu ) erano rispettivamente 27 , 7%16 , 1% , 22 , 9%13 , 3% , 9 , 8%4 , 9% . 
confrontando gli istogrammi di densit del gruppo uip e quelli del gruppo non uip , non sono state osservate differenze statisticamente significative ( p > 0 , 05 )  . soggetti normali le scansioni tc dei soggetti normali non hanno mostrato alcuna alterazione polmonare . mla , skewness , kurtosis degli istogrammi di frequenza erano in media rispettivamente 837 , 5 hu29 , 4 , 3 , 50 , 5 , 18 , 84 , 5 . 
le medie degli intervalli di densit pi basso ( 700200 hu ) , intermedio ( 700400 hu ) e pi alto ( 500200 hu ) erano rispettivamente 8 , 3%2 , 4% , 6 , 5%2 , 1% , 3%0 , 8% . 
i risultati di queste analisi hanno indicato che lo score visivo era inoltre lunico strumento di predizione del cpi , con un valore di r2 di 0 , 38 ( p < 0 , 05 )  . 
although the correlation between visual score and dlco differed little from the correlation between visual score and cpi , visual score did not provide any significant predictive value for dlco . in the non - uip group , correlation between intermediate discussione nel nostro studio abbiamo cercato di verificare se i dati ottenuti col software di analisi della densit potessero distinguere soggetti normali , pazienti uip e non uip . 
 i risultati sono espressi secondo i coefficienti di correlazione di pearson ( r ) e i corrispondenti valori di r2 ranges of density ( 700 to 400 hu ) and dlco ( r = 0.71 , p < 0.05 ) was stronger than the visual score and other ct indices . 
moreover , in mild fibrotic disease , there is no definite dichotomy between the density of the normal and abnormal lung ( such as in emphysema ) ; hence , there could be disadvantages in using only ranges of density information . 
inoltre , una forma lieve della patologia fibrotica non comporta una netta dicotomia di densit tra il polmone normale e quello patologico ( come nellenfisema ) , limitando cos lutilit degli intervalli di densit . 
 al contrario si visto che gli istogrammi nei pazienti patologici erano significativamente diversi da quelli dei soggetti sani ( p < 0 , 05 ) , e tale differenza era gi evidente allispezione visiva . 
nei pazienti uip abbiamo notato una minore attenuazione media , una maggiore asimmetria , ed un picco pi acuto ( tabella 2 ) rispetto a quanto riportato negli studi di harvey et al . 
entrambi i gruppi uip e non uip avevano unestensione della patologia modicamente limitata e simile , come anche confermato dagli score visivi , dagli intervalli di densit e dal grado dinvalidazione funzionale . 
data are pearsons product moment correlation coefficients ( r ) and the corresponding r2 values mla , densit media polmonare ; dlco , capacit di diffusione del monossido di carbonio . 
i risultati sono espressi secondo i coefficienti di correlazione di pearson ( r ) skewness kurtosis 700 to 200 hu 700 to 400 hu 500 to 200 hu fibrosis ratio visual score 1168 n . 
in healthy subjects , the first - order histogram of ct attenuation is sharply peaked ( kurtotic ) and skewed to the left in comparison with the gaussian normal distribution . 
both the uip group and nonuip groups had limited and similar extent of disease , as confirmed by visual scores as well as by the range of density and functional impairment . 
indeed , analysing a wider part of the lung , the histogram features could be relatively insensitive to textural changes . to further improve the differentiation between patients and controls , we constructed a fibrosis ratio that provided information about the fibrosis fraction . 
it is well known that data derived from the density - mask technique ( histogram features and ranges of density ) are not sufficient to obtain an accurate statement of disease extent in patients with lung fibrosis . 
however , it has never been proved that these widely available tools can quantify fibrosis extent better than the visual score can , which is subjective and suffers the drawback of a moderate level of interobserver and intraobserver variation . in the uip group , visual score was the only predictor of functional impairment . 
in a study by best et al . , fvc showed the greatest magnitude of correlation with histogram features , while dlco showed the least correlation ; the correlation between kurtosis and dlco was similar to our correlation ( r = 0.37 ) [ 17 ]  . 
perhaps it is impossible to restrict the alterations of uip inside a threshold of score visivo per lestensione di malattia fosse simile sia per il gruppo uip che per il gruppo non uip ( rispettivamente 39 , 7%14 , 5% e 39 , 5%21 , 2% ) , non si sono notate differenze tra gli istogrammi dei 2 gruppi ( p > 0 , 05 )  . 
 [ 21 ] i quali riportavano che gli istogrammi di densit della polmonite interstiziale non specifica ( nsip ) erano meno deviati a sinistra ed avevano un picco pi largo di quelli uip . 
peraltro , analizzando una porzione pi ampia del polmone , le caratteristiche dellistogramma possono essere relativamente indifferenti ai cambiamenti strutturali . per migliorare ulteriormente la distinzione tra malati e sani , abbiamo formulato un indice fibrotico che fornisse informazioni riguardo il rapporto tra grado di fibrosi e polmone sano . 
il valore normale stato sempre tra 0 , 99 e 1 , 0 , ossia assenza di fibrosi , mentre un rapporto pi basso era indicativo di una quantit significativa di fibrosi ( p < 0 , 05 )  . abbiamo quindi analizzato la relazione morfologico - funzionale . 
era gi noto che i dati ottenuti dalla maschera di densit ( istogrammi ed intervalli di densit ) non fossero sufficienti per ottenere un preciso resoconto dellestensione della patologia nei pazienti con fibrosi polmonare . 
tuttavia non mai stato dimostrato come questi strumenti , largamente diffusi , potessero quantificare lestensione della fibrosi rispetto allo score visivo , un metodo soggettivo che risente dellinconveniente di una variabilit intered intra - osservatore . nel gruppo uip lo score visivo risultato essere lunico sistema per predire significativamente il danno funzionale . esso ha mostrato una buona correlazione con il cpi ( r = 0 , 60 , r2 = 0 , 38 , p < 0 , 05 )  . 
gli istogrammi sono stati insoddisfacenti , con solo la mla che mostrava una moderata correlazione con il cpi ( r = 0 , 55 , p < 0 , 05 )  . 
 [ 17 ] la cvf ha mostrato la maggiore correlazione con gli indici degli istogrammi , mentre il dlco ha mostrato la minore ; la correlazione tra kurtosis ed il dlco era simile alla nostra ( r = 0 , 37 ) [ 17 ]  . 
per esempio , i nostri intervalli di densit non tengono in considerazione lo spazio cistico dellhoneycombing ( spazi morti ) , e questo potrebbe spiegare la mancanza di correlazione con gli indici funzionali . 
le dimensioni degli spazi morti cistici ( honey - combing alla tc ) , contribuiscono alla mancanza di perfusione del polmone fibrotico e sono correlate alla riduzione del dlco e meno agli indici volumetrici pfr [ 2628 ]  . 
for example , our ranges of density did not take into account the cystic space of honeycombing ( dead spaces ) on ct , and this can explain the lack of correlation with the functional indices . 
the extent of cystic dead spaces contributes to the lack of perfusion of the fibrotic lung and is linked to the reduction of dlco and less to the volumetric pft indices [ 2628 ]  . 
fibrosis ratio in the uip group was not a predictor of dlco or cpi . in the uip group , dlco and cpi were carried out because they have the strongest correlation with the morphologic extent of disease , histologically and on the ct [ 3 , 68 ]  . 
cpi is a new powerful severity variable that accounts for coexisting emphysema , whereas in patients without emphysema on ct , cpi did not reflect the disease extent better than did dlco [ 7 ]  . 
although the non - uip group might have contained some cases of nsip , organising pneumonia ( op ) or uip with atypical imaging features , the inclusion criteria of these patients were not thought to be subject to significant selection bias . 
however , it was clearly more difficult to establish the extent of patchy ground - glass , in or out of areas of reticulation , than scoring the extent of honeycombing or reticulation alone . 
a weighting factor should be applied to the estimates of each level to correct for the differing contribution given by each level ( an upper zone section has a small cross - sectional area , and therefore contributes to the total lung volume less than a lower zone section does ) [ 26 , 30 ]  . a confounding factor in the non - uip group could be the lobular areas of air trapping , which was not taken into ac1170 gruppo uip non si correlato significativamente alla dlco o al cpi . nel gruppo uip , il dlco e il cpi sono stati ricavati poich sono gli indici a maggiore correlazione con lestensione della patologia , valutata sia istologicamente che alla tc [ 3 , 68 ]  . 
 [ 9 ] ritengono che non ci siano differenze di risultati se considerati unitamente i pazienti con e senza enfisema ; tuttavia lenfisema nei pazienti con uip un noto fattore di confondimento , potendo influenzare gli indici di funzionalit polmonare . 
la nostra analisi non stata ristretta ai soli pazienti senza enfisema a causa del numero ridotto dei soggetti dello studio e pertanto non abbiamo potuto stabilire precisamente se lenfisema fosse effettivamente un fattore fuorviante . 
 [ 7 ] , tre pazienti uip con coesistente enfisema sono stati probabilmente sufficienti per fornire una correlazione solo tra lo score visivo e il cpi ( r = 0 , 60 , r2 = 0 , 38 , p < 0 , 05 )  . le correlazioni morfologico - funzionali sono risultate significativamente diverse nel gruppo non uip . 
sebbene questo gruppo possa aver contenuto alcuni casi di nsip , o di polmonite organizzante ( op ) , o uip con caratteristiche di imaging atipiche , i criteri di selezione di questi pazienti non sono stati ritenuti essere fonte di significativo bias . 
tuttavia , chiaramente pi difficile stabilire lestensione delle irregolarit ground - glass , allinterno o allesterno delle aree di reticolazione , che misurare lestensione dellhoney - combing o la sola reticolazione . 
un fattore di ponderazione dovrebbe essere applicato per la valutazione di ogni livello , per correggerne il diverso contributo relativo ( la sezione trasversale di una zona superiore , rispetto ad una sezione basale , ha una minor area e quindi contribuisce meno al volume polmonare totale ) [ 26 , 30 ]  . un fattore fuorviante nel gruppo non uip potrebbero essere le aree lobulari di air - trapping che non erano state prese in considerazione dal nostro sistema di valutazione . 
according to hansell et al . [ 2 ] , there is no independent relationship between the extent of decreased attenuation on ct and indices of gas transfer . however , patients in that study had mainly subacute eaa , where the cellular component of bronchiolitis may be more extensive [ 2 ]  . 
despite the limited number of cases , our experience indicated a significant inverse correlation between the extent of fibrosis and expiratory air trapping , possibly because the extent of cellular bronchiolitis with heterogeneous distribution , which may persist in chronic eaa , is usually quantitatively exceeded by fibrosis [ 4 ]  . in conclusion , despite a poor correlation with functional data , fibrosis ratio together with the histogram features can differentiate fibrotic from normal lungs . 
nonostante il limitato numero di casi , la nostra esperienza indica una significativa correlazione inversa tra lestensione della fibrosi e lair - trapping espiratorio , forse perch lestensione della bronchiolite cellulata a distribuzione eterogenea che pu trovarsi nellaee cronica , di solito superata quantitativamente dalla fibrosi [ 4 ]  . in conclusione , abbiamo dimostrato che , nonostante la scarsa correlazione con i dati funzionali , lindice fibrotico assieme agli istogrammi pu distinguere i polmoni fibrotici da quelli normali . 
la stretta correlazione tra il cpi e lo score visivo nei pazienti affetti da uip suggerisce che il nostro sistema di valutazione pu essere vantaggiosamente applicato . nessun altro indice tc , inclusi gli intervalli di densit , lindice fibrotico e gli istogrammi possono correlarsi al cpi o al dlco nei pazienti uip . 
crusco , via antica vena 18 , i - 06100 - perugia , italy , tel . : + 39 - 075 - 393044 / 328 - 2896943 , fax : + 39 - 075 - 5783488 , e - mail : fcrusco@sirm.org received : 20 may 2006 / accepted : 4 april 2007 / published online : 13 december 2007 abstract the aim of this review is to provide starting from anatomical , surgical and pathophysiological data elements for evaluating the status of coronary artery bypass grafts with multidetector computed tomography ( ct ) , taking into consideration the most common conduits used ( left and right internal mammary arteries , saphenous vein , radial artery , gastroepiploic artery ) and early and late complications ( stenosis or obstruction , vasospasm , aneurysms and pseudoaneurysms , malposition )  . 
finally , we offer general guidelines for reporting the examination results . key words multidetector ct coronary artery bypass graft riassunto scopo del seguente lavoro di revisione fornire , a partire da dati di anatomia , chirurgia e fisiopatologia , gli elementi utili ai fini della valutazione con tc multidetettore dello stato di perviet dei bypass aortocoronarici , prendendo in considerazione i condotti pi comunemente utilizzati ( arteria mammaria sinistra e destra , vena safena , arteria radiale , arteria gastroepiploica ) e le eventuali complicanze precoci e tardive ( steno - ostruzione , vasospasmo , aneurismi e pseudoaneurismi , malposizionamenti ) , legate ad essi . 
infine vengono fornite alcune indicazioni di massima come guida alla refertazione dellesame . parole chiave tc multidetettore bypass aortocoronarico introduction introduzione surgical myocardial revascularisation by coronary artery bypass grafting ( cabg ) , aims at restoring and normalising coronary blood flow in hypoperfused ischaemic territories by grafting arterial and venous conduits from the aorta to the diseased coronary artery beyond the stenosis . 
surgical revascularisation is indicated in subjects with threeor two - vessel coronary disease with involvement of the proximal left anterior descending ( lad ) artery , left main coronary artery disease and depressed left ventricular function ( left ventricle ejection fraction < 45% ) [ 1 ]  . monitoring patients after cabg involves routine clinical follow - up every 46 months during the first year after surgery and where treatment has been successful , every year thereafter . 
use of electrocardiogram ( ecg ) stress testing as la terapia chirurgica di rivascolarizzazione miocardica mediante bypass aortocoronarico ( cabg ) ha come scopo il ripristino e la normalizzazione del flusso coronarico nei territori ischemici ipoperfusi , mediante limpianto a livello della porzione sottostenotica della coronaria nativa patologica , di condotti arteriosi o venosi . 
una rivascolarizzazione chirurgica indicata nei soggetti con patologia coronarica trivasale o bivasale con interessamento della lad prossimale , malattia del tronco comune , funzionalit ventricolare sinistra globale compromessa ( frazione di eiezione ventricolare sinistra < 45% ) [ 1 ]  . il monitoraggio dei pazienti sottoposti a cabg viene effettuato routinariamente mediante follow - up clinico ogni 46 mesi entro il primo anno dallintervento , mentre nei sog1087 f . 
the clinical utility of the test is , however , limited by its low sensitivity for ischaemia detection and localisation and the frequent finding , even in healthy subjects , of ecg abnormalities independent of possible ischaemia recurrence [ 2 , 3 ]  . echocardiography and myocardial scintigraphy are regarded as second - line , noninvasive imaging techniques and are used to establish the cardiac origin of angina by identifying graft stenosis or obstruction and / or coronary disease progression and to evaluate coronary functional reserve , a key element for assessing the effectiveness of the revascularisation procedure . 
these tests , performed after induction of physical or pharmacological stress ( dipyridamole or adenosine in scintigraphy ; dobutamine in echocardiography ) , reveal ischaemic territories as changes in regional wall motion , systolic function and overall end - systolic volume , or as regional perfusion defects , respectively [ 46 ]  . 
generally , decisions to use stress imaging are guided by the presence of ischaemic symptoms , with the only exception being asymptomatic highrisk patients ( with poor left ventricular function , multivessel disease , disease of the proximal left anterior descending artery , diabetes , high - risk occupations ) more than 5 years after surgery , in whom it is reasonable to perform stress single photon emission computed tomography ( spect ) imaging to stratify risk , evaluate prognosis , determine disease progression and obtain information to guide treatment [ 7 , 8 ]  . coronary angiography is currently considered the reference standard for evaluating bypass patency and planning further percutaneous or surgical revascularisation procedures [ 9 ]  . 
the main indication for coronary angiography is evidence of high - risk criteria at noninvasive stress testing ( multisegment regional wall motion abnormalities and / or reversible moderate to severe perfusion defects ) , regardless of time since surgery . 
these include age ( > 80 years ) , a functional class iv , left main disease , associated cardiac valve disease , left ventricular ejection fraction < 30% and severe noncardiac disease [ 9 , 11 ]  . 
consideration of these data related to the invasiveness of the procedure and the need to reduce the costs deriving from the substantial number of conventional coronary angiography exams not followed by percutaneous interventional procedures ( 20%27% negative , 2%58% unnecessary ) has encouraged the use of multidetector ct ( mdct ) as an alternative noninvasive cardiac imaging test for the evaluation of graft patency [ 12 ]  . 
il ricorso allecg da sforzo , quale test strumentale di primo livello , indicato in caso di comparsa di sincope , modifica della pregressa sintomatologia anginosa o comparsa di una sintomatologia suggestiva di alterazioni del ritmo e anomalie della conduzione ; il valore clinico del test tuttavia limitato a causa della bassa sensibilit nellidentificazione e nella localizzazione di ischemia e per il riscontro frequente , anche in pazienti sani , di anomalie del tracciato elettrocardiografico indipendenti dalleventuale recidiva ischemica [ 2 , 3 ]  . laccertamento della genesi cardiaca del dolore anginoso , mediante lidentificazione della steno - ostruzione del graft e / o della progressione di malattia nelle coronarie native , e la valutazione della riserva funzionale coronarica , considerata elemento fondamentale nella valutazione di efficacia della procedura di rivascolarizzazone , viene demandato allecocardiografia e alla miocardioscintigrafia , considerate tecniche di imaging non invasivo di secondo livello . 
questi test , eseguiti con induzione di stress fisico o farmacologico ( dipiridamolo o adenosina nel test scintigrafico , dobutamina in quello ecocardiografico ) , identificano i territori ischemici rispettivamente sotto forma di alterazioni della motilit parietale regionale , della funzione sistolica e del volume telesistolico globale e sotto forma di deficit perfusionali regionali [ 46 ]  . 
in linea generale , il ricorso alle metodiche di stress imaging guidato dalla positivit dei sintomi ischemici , con ununica eccezione , nei pazienti asintomatici ad alto rischio ( cio con ridotta funzione ventricolare sinistra , malattia coronarica multivasale , malattia della discendente anteriore prossimale , diabete , occupazione professionale a rischio ) , a oltre 5 anni dallintervento , nei quali pu essere considerata ragionevole leffettuazione di una stressspect per stratificare il rischio , valutare la prognosi , determinare la progressione di malattia e ottenere informazioni per approntare uneventuale terapia [ 7 , 8 ]  . la coronarografia considerata , attualmente , il gold standard diagnostico per la valutazione dello stato di perviet dei bypass e la procedura di riferimento per la pianificazione di eventuali ulteriori interventi di rivascolarizzazione , eseguibili per via percutanea o per via chirurgica [ 9 ]  . 
la principale indicazione allesecuzione dellesame rappresentata , dallevidenza con le metodiche di stress imaging non invasivo , di criteri ad alto rischio ( vale a dire anomalie della motilit parietale regionale multisegmentarie e / o difetti di perfusione moderati - severi reversibili ) qualsiasi sia il periodo postoperatorio . 
il rilievo , nellimmediato postoperatorio , di una elevazione di alcuni markers biochimici considerati indicatori in grado di predire levento ischemico da precoce ostruzione del graft ( livelli di ck - mb > 70 u / l a 6 ore dallintervento , livelli di troponina cardiospecifica i > 20 ng / ml a 1224 ore dallintervento ) , costituisce unulteriore indicazione allesecuzione dellesame , anche in assenza di dati derivati dallo stress imaging [ 10 ]  . il rischio di complicanze maggiori ( morte , infarto del miocardio , ictus ) durante cateterismo cardiaco minimo ma non trascurabile , inferiore all1% , tuttavia alcuni fattori si associano ad aumento del tasso di mortalit fino a 10 volte . tra questi let ( > 80 anni ) , una classe funzionale iv , una method has a reported sensitivity of 96% , specificity of 95% , positive predictive value of 81% , negative predictive value of 99% and interobserver agreement of 95% [ 13 , 14 ]  . mdct : general scanning principles one prerequisite for a correct study of cabgs , or the native coronaries , is that the heart rate ( hr ) must be kept < 65 bpbradycardia may be obtained by means of - blockers , administered orally 23 days before the examination or intravenously ( i.v. ) on the same day . 
 after a baseline unenhanced scan to assess calcification of the native coronary arteries and the position of the metal clips , the contrast - enhanced study is performed with i.v. 
injection of 100120 ml of nonionic iodinated contrast material ( 350400 mgi / ml ) at a rate of 34 ml / s via a dual - syringe automatic injector , followed by a 30to 50 - ml bolus of saline solution . 
contrast enhancement is optimised using the bolus tracking technique , with acquisition starting when a predefined enhancement threshold is reached ( 100150 hu in the left ventricle or ascending aorta )  . 
once the phase of the cardiac cycle with the best diagnostic quality has been identified , usually mid - to - end diastolic postprocessing is performed on the native axial images to obtain multiplanar reconstructions ( mpr ) , curved mpr ( cmpr ) , maximum intensity projections ( mip ) and three - dimensional volume rendering ( 3d - vr ) to assess the course ( proximal anastomosis , graft body , distal anastomosis ) and type of bypass gracoverage of the entire study volume [ field of view ( fov ) 150200 mm ] using 16 - slice mdct requires collimations of 0.751 mm with a 15to 20 - s inspiratory breath - hold . 
table 1 shows the technical parameters of studies carried out with 4 - , 16and 64 - slice scanners . vascular structures internal mammary artery ( ima ) better long - term patency ( 85%90% at 10 years ) currently makes the internal mammary arteries the conduits of choice in surgical revascularisation procedures [ 1517 ]  . 
lanalisi di tali dati , connessi allinvasivit della procedura , e la necessit di ridurre i costi legati allelevato numero di coronarografie convenzionali non seguite da procedure di interventistica percutanea ( il 20%27% di queste risultano negative , il 2%58% non sono necessarie ) , ha favorito il ricorso alla tc multidetettore ( tcmd ) quale metodica alternativa di imaging cardiaco non invasivo utile ai fine della valutazione dello stato di perviet dei graft [ 12 ]  . in tal senso , numerosi lavori di comparazione con la coronarografia convenzionale , hanno ormai validato lefficacia delle apparecchiature a 16 canali nella detezione di patologia dei graft ; con tale metodica sono stati riportati valori di sensibilit del 96% , specificit del 95% , valore predittivo positivo dell81% , valore predittivo negativo del 99% e accordo inter - osservatore nelle interpretazione delle immagini pari al 95% [ 13 , 14 ]  . tcmd : principi generali di scansione prerequisito fondamentale per un corretto studio dei cabg il mantenimento , analogamente a quanto avviene nello studio delle coronarie , di una frequenza cardiaca < 65 bpm . leffetto bradicardizzante pu essere ottenuto mediante il ricorso a - bloccanti , somministrabili per os nei 23 giorni precedenti lesame o endovena il giorno stesso dellesame . in tcmd il volume di studio esteso a comprendere , per i graft venosi , lanastomosi prossimale su aorta ascendente e lanastomosi distale sui diversi territori delle coronarie ; per lo studio dei graft con mammaria interna non necessario includere lorigine succlavia prossimale . dopo unacquisizione diretta senza mezzo di contrasto , utile per valutare lentit delle calcificazioni delle coronarie native e il decorso delle clips metalliche , lo studio contrastografico viene eseguito mediante somministrazione endovenosa , utilizzando un iniettore automatico a doppia siringa , di 100120 ml di mdc iodato non ionico ( 350400 mgi / ml ) , alla velocit di 34 ml / s , seguiti da un bolo di 3050 ml di soluzione salina . 
per ottimizzare il contrast enhancement viene utilizzata la tecnica del bolus tracking , e il ritardo per linizio della scansione viene selezionato a partire dal raggiungimento di una soglia predefinita ( 100150 uh in ventricolo sinistro o aorta ascendente )  . le immagini sono ricostruite con gating ecg di cardiosincronizzazione retrospettiva e finestre temporali r - r variabili ; a partire dalle immagini assiali native , identificata la fase del ciclo cardiaco con la migliore qualit diagnostica , in genere meso - telediastolica , si procede allutilizzazione nel post - processing di ricostruzioni multiplanari ( mpr ) , curve ( cmpr ) , proiezioni di massima intensit ( mip ) e volume rendering tridimensionale ( 3d - vr ) , valutando , ai fini della valutazione di perviet dei cabg decorso ( anastomosi prossimale , corpo del graft , anastomosi distale ) e tipo di bypass . con tecnica tcmd a 16 canali , al fine di coprire lintero volume di studio ( fov 150200 mm ) necessario impiegare 1089 f . 
the graft is generally used in situ , that is , with a natural proximal origin at the level of the left subclavian artery and a distal anastomosis below the stenosis or occlusion on the native coronary . 
when present , graft stenosis or occlusion generally occurs at the distal anastomosis owing to the retrograde progression of coronary disease facilitated by the small diameter and high resistance of the coronary branch [ 18 ]  . 
 the right internal mammary artery ( rima ) , rarely used as an in situ graft for the right coronary artery ( rca ) territory , is more commonly implanted as a free graft ( with proximal anastomosis on the ascending aorta and distal anastomosis on the target coronary ) or composite graft , with proximal fig . 
1 immagini 3d - vr di bypass in situ lima - lad , normalmente pervio . 1090 collimazioni di 0 , 751 mm , con risultante apnea inspiratoria di 1520 secondi . 
in tabella 1 sono riportati i parametri tecnici legati allo studio con scanner a 4 , 16 e 64 canali . strutture vasali arteria mammaria interna ( ima ) attualmente il graft arterioso con mammaria interna , grazie alla sua migliore perviet a distanza ( 85%90% a 10 anni ) , rappresenta il condotto di prima scelta nel trattamento chirurgico di rivascolarizzazione [ 1517 ]  . 
il graft generalmente utilizzato in situ , cio con origine prossimale naturale a livello dellarteria succlavia sinistra e anastomosi distale eseguita su coronaria nativa a valle della steno - ostruzione . 
la steno - ostruzione del graft , quando presente , avviene in genere in sede di anastomosi distale , per progressione retrograda della patologia coronarica nativa , favorita dal piccolo calibro e dalle elevate resistenze del ramo coronario [ 18 ]  . la mammaria interna destra ( rima ) , raramente utilizzata come graft in situ per il territorio della coronaria destra ( rca ) , pi spesso utilizzata come graft libero ( con anastomosi prossimale su aorta ascendente e anastomosi distale su coronaria target ) , o composito , con anastomosi prossimale su graft con lima e anastomosi distale sul territorio della circonflessa ( lcx ) , con configurazione risultante f . 
utilizzando entrambe le mammarie si ottiene una rivascolarizzazione miocardica totalmente arteriosa , ne consegue una riduzione delle recidive anginose e un migliore tasso di perviet a 1 anno , rispetto allutilizzo , in associazione alla lima , del graft venoso con vena safena ( sv )  . 
il limite di impiego di entrambe le mammarie interne per costituito dal rischio , nei pazienti diabetici , obesi o anziani , di infezioni e deiscenze sternali secondarie alla devascolarizzazione completa della parete toracica anteriore . 
per tali motivi la patologia del graft venoso , rispetto a quella del graft arterioso , si associa ad una maggiore instabilit di placca , ed responsabile del anastomosis on a lima graft and distal anastomosis on the left circumflex artery ( lcx ) territory , with a resulting yor t - shaped configuration [ 19 ]  . 
the use of both mammary arteries allows totally arterial myocardial revascularisation and consequently fewer angina recurrences and better 1 - year patency rates compared with the use of lima combined with a saphenous vein ( sv ) grathe limitation of using both internal mammary arteries is the risk , in diabetic , obese or elderly patients , of sternal infections or dehiscence due to complete devascularisation of the anterior chest wall . 
for these reasons , venous grafts disease is associated with greater plaque instability and is responsible for 53% of angina episodes occurring within 5 years , 76% between 5 and 10 years , and 92% beyond 10 years . 
in the same periods , progression of atherosclerosis in the native vessels is responsible for 47% , 24% and 8% of ischaemic events , respectively [ 20 , 21 ]  . 
sv grafts are normally anastomosed proximally on the anterior wall of the ascending aorta ( on the left side , with a partially protected course above the pulmonary artery for grafts to the lad territory or lcx ; on the right side for those to the rca territory ) and distally below the stenosis or obstruction of the native coronary . radial artery ( ra ) with the recent advances in surgical harvesting techniques allowing minimal endothelial damage , the characteristic features of the conduit ( relatively large diameter with well - represented muscular wall that facilitates anastomosis ) and the use of calcium antagonists postoperatively to reduce the tendency towards vasospasm , the radial artery has come to be considered a valuable alterative to ima grafts [ 22 , 23 ]  . short - term patency rates are similar to those of lima , whereas midto long - term rates are comparable with those of sv grafts ( 89% at 4 years ) [ 24 ]  . 
2 three - dimensional volume rendering images of triple coronary artery bypass grafting : free radial artery on the left circumflex artery ( lcx - mo ) , left internal mammary artery on left anterior descending artery and saphenous vein on lcx . despite limitations due to the technical difficulty of the procedure , the gastroepiploic artery has been generally been used as fig . 
 complications graft stenosis and occlusion during the immediate postoperative period , the major cause of graft stenosis or occlusion is thrombosis , a complication that arises within a month of surgery in 10%15% of cases [ 16 ]  . 
the first recognised cause is the endothelial injury sustained while harvesting the vessel , ligating the collaterals in the case of arterial grafts or as a result of mechanical trauma due to excessive pulling or stretching in the case of short grafts . 
the use of mechanical aortic connectors for creation of the proximal anastomosis with sv appears to be associated with a higher incidence of thrombosis . after the first postoperative month , stenosis or occlusion of venous grafts is due to arterialisation resulting from exposure to high - pressure levels leading to intimal hyperplasia , medial thickening and atherogenesis . 
in arterial grafts , which are more resistant and with higher patency rates than venous grafts , the most common cause is retrograde progression of coronary artery atherosclerosis from the distal anastomosis . 
occlusion of an arterial graft ( which tends to be an all - or - nothing phenomenon ) is characterised by exclusive visualisation of the metal clips without evidence of a central contrast column ( empty railway sign )  . 
specifically , the causes of elevated vasoreactivity of the radial artery lie in its wall thickness , the density and arrangement of the muscle cells in the tunica media , denervation during harvesting and competitive flow with the native coronaries involved in the distal anastomosis [ 25 ]  . 
several measures have been devised to minimise vasospasm , including preoperative prophylaxis with calcium antagonists or intraoperative treatment with topical - adrenergic antagonists . the corresponding mdct finding is diffuse , or less commonly focal , uniform narrowing of the arterial graft , with increased distance between the vascular column and the lateral metal clips , without evident intraluminal defects and thus with normal opacification . 
the narrowing , corresponding to 70%99% stenosis , is equivalent to the angiographic string 1092 53% degli episodi anginosi che si verificano entro i 5 anni , del 76% degli episodi tra i 5 e i 10 anni , del 92% di quelli oltre i 10 anni . 
normalmente i graft con sv vengono anastomizzati in sede prossimale sulla parete anteriore dellaorta ascendente ( sul lato sinistro , con un decorso parzialmente protetto al di sopra dellarteria polmonare per i graft sul territorio della lad o della lcx , sul lato destro per quelli sul territorio della rca ) , distalmente a valle della lesione stenotica od ostruttiva della coronaria nativa . arteria radiale ( ra ) grazie al recente miglioramento delle tecniche chirurgiche di isolamento che hanno portato ad una minimizzazione del danno endoteliale , alle particolari caratteristiche anatomiche del condotto ( calibro relativamente ampio con parete muscolare ben rappresentata che facilita la costruzione delle anastomosi ) e grazie allutilizzo di calcio - antagonisti nel post - operatorio in grado di ridurre la tendenza al vasospasmo , larteria radiale considerata ad oggi una valida alternativa ai graft con ima [ 22 , 23 ]  . 
il tasso di perviet equivalente a quello della lima nel breve termine mentre risulta paragonabile a quello dei graft con sv nel periodo medio - lungo ( 89% a 4 anni ) [ 24 ]  . 
il primum movens riconosciuto il danno endoteliale che pu verificarsi nella fase di isolamento del vaso , in quella di legatura dei collaterali nel caso di graft arteriosi , o come conseguenza di traumi meccanici da eccessiva trazione o stiramento del vaso nel caso di graft con lunghezza ridotta . 
lostruzione del graft arterioso ( che avviene in genere con fenomeno tutto o nulla ) si caratterizza per la sola visibilit delle clips metalliche senza evidenziazione della colonna centrale di mdc ( segno del binario vuoto , empty railway sign )  . 
specificatamente le cause dellelevata vasoreattivit dellarteria radiale sono da ricondurre allintrinseco spessore parietale , alla densit e alla particolare organizzazione delle cellule muscolari della tonaca media , alla denervazione subita durante lisolamento dallavambraccio , al flusso competitivo con le coronarie native target dellanastomosi distale [ 25 ]  . 
per minimizzare il vasospasmo sono stati considerati diversi provvedimenti , tra i quali una profilassi preoperatoria con calcio - antagonisti o un trattamento farmacologico intraoperatorio con antagonisti - adrenergici per via topica . laspetto mdct corrispondente quello del restringimento uniforme diffuso , o meno comunemente focale , del graft arterioso , con aumentata distanza tra colonna vascolare e clips metalliche laterali , in assenza di difetti endoluminali evidenti e cio con normale opacizzazione da mdc . 
tale restringimento , corrispondente ad una stenosi del 70%99% , lequivalente del segno della stringa angiografico e piuttosto che uno spasmo fisso deve essere considerato come il risultato di un rimodellamento vascolare negativo secondario ad una risposta adattativa ad una bassa richiesta di perfusione periferica per fenomeni di flusso competitivo [ 26 ]  . 
queste considerazioni sono supportate dallevidenza di una bassa incidenza di ischemia nei territori perfusi da graft con restringimento diffuso . aneurismi e pseudoaneurismi eventuali pseudoaneurismi asintomatici si formano generalmente entro i primi 6 mesi dallintervento e sono correlati 1093 fig . 
4 restringimento uniforme diffuso di bypass lima su lad , espressione di rimodellamento vascolare negativo . sign and , rather than a fixed spasm , should be considered the result of negative vascular remodelling due to an adaptive response to a low demand for peripheral perfusion because of competitive flow phenomena [ 26 ]  . 
the complications of aneurysms are mainly related to compression of adjacent structures , but thrombosis , embolisation , fistulisation and rupture with possible haemomediastinum may also occur . malposition and iatrogenic complications graft malposition may result from kinking , frequently of the proximal portion of a venous graft due to excessive length or coiling of the gra both conditions are linked to surgical technique and are associated with an increased risk of endothelial damage and subsequent thrombotic stenosis or occlusion . 
generally , however , any iatrogenic endothelial trauma affecting the graft during surgery will promote graft thrombosis . extracardiac complications within the first week after surgery , the presence of a moderate unilateral left pleural effusion , which tends to resolve spontaneously , is considered paraphysiological , and only 1%4% of patients develop a clinically relevant massive effusion requiring drainage by thoracentesis [ 28 ]  . 
likewise , the incidence of pericardial effusion during the immediate postoperative period is fairly high ( 22%85% ) ; this resolves spontaneously in most patients and becomes haemodynamically significant with cardiac tamponade in only 0.8%6% of cases [ 29 ]  . 
potentially lethal , with a mortality rate of approximately 25% , are deep sternal wound infections complicated by mediastinitis , which occur in 1%4% of patients [ 30 ]  . 
finally , pulmonary embolism , which tends to have a silent clinical course , is a further complication that arises in 0.4%9.5% of cases after cabg [ 31 ]  . 
 artefacts cardiac and respiratory motion artefacts in the presence of cardiac arrhythmias characterised by elevated or irregular hr , there is a critical reduction in the diastolic phase , the duration of which falls below the temporal resolution of the scanner . 
dilatazioni aneurismatiche vere e proprie sono complicanze rare e tardive , che si verificano ad oltre 5 anni di distanza dallintervento , pi spesso a carico dei graft venosi come effetto dellaterosclerosi [ 27 ]  . 
le complicanze degli aneurismi sono legate alla compressione delle struttura adiacenti per effetto massa ma possono essere rappresentate anche dalla trombosi , dallembolizzazione , dalla fistolizzazione , dalla rottura con potenziale emomediastino . malposizionamento e complicanze iatrogene un malposizionamento pu verificarsi per un kinking , pi frequentemente a carico della porzione prossimale di un graft venoso o per eccessiva lunghezza e tortuosit del graft stesso ( coiling )  . 
in linea generale , comunque , durante lintervento chirurgico , qualsiasi trauma endoteliale iatrogeno del graft ne favorisce la trombosi . complicanze extracardiache entro la prima settimana dallintervento la presenza di un modesto versamento pleurico unilaterale sinistro , con tendenza spontanea alla risoluzione , considerata parafisiologica solo l1%4% dei pazienti post - cabg sviluppano un versamento massivo , clinicamente rilevante , tale da richiedere una toracentesi evacuativa [ 28 ]  . 
allo stesso modo lincidenza di un versamento pericardico nellimmediato postoperatorio piuttosto elevata ( 22%85% ) ; nella maggior parte dei casi questo si risolve spontaneamente e solo nello 0 , 8%6% dei casi risulta emodinamicamente significativo appalesandosi come tamponamento cardiaco [ 29 ]  . 
potenzialmente fatali , con una mortalit di circa il 25% , sono le infezioni retrosternali profonde complicate da mediastinite , che si verificano nell1%4% dei pazienti [ 30 ]  . 
infine , lembolia polmonare , pi spesso con decorso clinico silente , un ulteriore complicanza del paziente post - cabg , manifestandosi nello 0 , 4%9 , 5% dei casi [ 31 ]  . artefatti artefatti da movimento cardiaco e respiratorio in presenza di aritmie cardiache caratterizzate da frequenza cardiaca troppo elevata o irregolare si ha una riduzione critica della fase diastolica , la cui durata risulta inferiore alla risoluzione temporale dello scanner . 
6 artefatti da indurimento del fascio con conseguente effetto blooming e mascheramento del lume vasale . tion during the last phase of an inspiratory breath - hold makes it difficult to visualise the coronary segments and distal anastomoses , especially on the right side , as , compared with the lad and lcx , the rca is affected by greater variations in velocity and thus in position during the different phases of the cardiac cycle . 
a reduction of cardiac motion artefacts can be achieved by decreasing the hr with - blocker premedication or by a more appropriate selection of the r - r interval for reconstruction . respiratory motion artefacts produce the same effects and can be differentiated from cardiac motion artefacts on the basis of the presence of linear misregistrations beyond the cardiac contours and even in the chest wall . 
cabg visualisation may also be partly affected by superimposition of adjacent anatomical structures with regular contrast enhancement , such as the left atrial auricles . la normale accelerazione cardiaca durante lultima fase dellapnea inspiratoria rende particolarmente difficoltosa la visualizzazione dei segmenti coronarici e delle anastomosi distali , specie a destra , in considerazione del fatto che la rca subisce , rispetto alla lad e alla lcx , le maggiori modifiche di velocit e quindi le maggiori escursioni di posizione durante le diverse fasi cardiache . 
la riduzione degli artefatti da movimento cardiaco pu essere ottenuta diminuendo la frequenza cardiaca mediante premedicazione con - bloccanti o mediante una selezione pi appropriata dellintervallo r - r di ricostruzione . gli artefatti da movimento respiratorio si manifestano con gli stessi effetti e la differenziazione rispetto agli artefatti da movimento cardiaco viene effettuata sulla base della presenza delle misregistrazioni lineari oltre i profili cardiaci , anche nel contesto della parete toracica . 
la riduzione di tali artefatti si ottiene riducendo i tempi dellapnea inspiratoria e istruendo il paziente a mantenere il respiro prima delleffettuazione dellesame [ 32 ]  . indurimento del fascio radiogeno clips metalliche , fili di sutura sternali , fili di pacemaker , ma anche calcificazioni aterosclerotiche nelle coronarie native , possono produrre artefatti a strisce da indurimento del fascio . 
il conseguente effetto di eccessiva luminosit di tali strutture ( blooming ) , oltre che determinare un aumento artefattuale delle dimensioni delloggetto in esame , pu contribuire , per leffetto di volume parziale , ad inficiare il corretto studio del lume vascolare , rendendo non valutabili i segmenti vasali o evidenziando pseudostenosi , specie in sede 1095 f . 
for example , poor vascular enhancement may be a direct consequence of the incorrect use of bolus tracking and inappropriate scan delay settings , of altered flow dynamics in elderly patients or of inappropriate choice of contrast volume or concentration . 
pitch selection is fundamental , above all in patients with a long r - r interval and hr < 50 bpm , in whom failure to apply a low pitch to cover the entire course of the grafts will produce blurring [ 32 ]  . 
 to avoid these technical problems , patency should always be evaluated on the combined axial , mpr , mip and vr images , as a bypass graft not visualised on vr images and erroneously thought to be obstructed may instead be patent and only detectable on mip or mpr images . reporting guide a prerequisite for the mdct study of cabg is prior knowledge of the type of surgical procedure performed on the patient . 
detailed anatomical information is required on the number and type of bypass grafts ( arterial or venous , in situ , free , composite , sequential ) and the exact location of the proximal and distal anastomoses . 
assessment of the distal anastomosis is a critical step in the examination due to relative hypermotility during the cardiac phases and the presence of more distally located metal clips , which account for a greater susceptibility to motion artefacts and beam hardening with blooming effects , respectively . 
in any case , assessment of the native coronary flow distal to the anastomosis is mandatory . the judgement of patency must be based on the degree of stenosis : patency ( complete uniform opacification of the graft without critical stenoses ) ; critical stenosis ( stenosis > 50% ) ; occlusion ( graft not visible due to lack of enhancement )  . 
in the presence of a diffuse uniform narrowing of arterial grafts , above all in ra grafts , with increased distance between vascular column and lateral metal clips and a vessel diameter1 mm , one should consider the possibility of vasospasm due to functional remodelling with preserved patency . 
la visualizzazione dei cabg pu essere inoltre parzialmente inficiata dalla sovrapposizione di strutture anatomiche adiacenti a regolare impregnazione contrastografica , quali le auricole atriali a sinistra . artefatti di ordine tecnico alcuni artefatti sono causati da errori tecnici eseguiti in fase di acquisizione dei dati , cos un enhancement vascolare insufficiente pu essere la diretta conseguenza di un errato utilizzo della temporizzazione mediante bolus tracking con inizio della scansione inappropriato , di un alterata dinamica di flusso nei pazienti anziani , di uninappropriata scelta del volume o della concentrazione del mezzo d contrasto iodato . 
la scelta del pitch di fondamentale importanza specie nei pazienti con intervallo r - r lungo e fc < 50 bpm , nei quali la mancata applicazione di un pitch basso per coprire lintero decorso dei graft causa di effetto blurring [ 32 ]  . per ovviare a tali problemi tecnici , la valutazione di perviet deve essere sempre effettuata , nel post - processing , su immagini assiali , mpr , mip e vr combinate , pu accadere infatti che un cabg non visualizzabile in vr ed erroneamente ritenuto ostruito , sia pervio e visualizzabile nelle sole immagini mip o mpr . guida alla refertazione pre - requisito essenziale per lo studio dei cabgs con mdct la conoscenza , a priori , del tipo di intervento chirurgico effettuato dal paziente . 
sono necessarie precise e dettagliate informazioni di tipo anatomico riguardanti il numero ed il tipo dei bypass confezionati ( arteriosi o venosi , in situ , liberi , compositi , sequenziali ) e lesatta collocazione delle anastomosi prossimali e distali . 
in ogni caso dobbligo la valutazione del flusso coronarico nativo distale rispetto allanastomosi . il giudizio di perviet deve essere fornito in base allentit della stenosi : perviet ( completa e uniforme opacizzazione del graft in assenza di stenosi critiche ) , stenosi critica ( stenosi > 50% ) , ostruzione ( assenza di visibilit del graft per mancata opacizzazione dello stesso )  . 
in presenza di un diffuso ed uniforme restringimento dei graft arteriosi , specie di quelli con ra , con aumento della distanza tra colonna vascolare e clips metalliche laterali e calibro vasale 1 mm , si deve prendere in considerazione un vasospasmo da rimodellamento funzionale con mantenuta perviet . dal punto di vista tecnico la valutazione dello stato di perviet dei cabg deve essere eseguita integrando le singole informazioni ottenute dalle differenti tecniche di visualizzazione delle immagini nel post - processing ( mpr , mip , vr ) e non pu prescindere in ogni caso da una valutazione iniziale delle immagini assiali native . 
le immagini vr , grazie alla visione panoramica 3d , sono molti utili nella definizione della complessa anatomia dei graft e dovrebbero essere usate , insieme alle assiali native , come base per la interpretazione dei reperti . 
gli svantaggi successiva dellanalisi singola delle mpr oblique o curve e delle mip ( rispettivamente dipendenza dallorientamento manuale del piano di vista con stenosi falsamente positive o negative nel primo caso e sovrastima delle stenosi per effetto di sovraproiezione nel secondo ) , possono essere evitati utilizzando entrambe le tecniche in maniera complementare [ 34 ]  . 
in questo modo possibile ottenere le informazioni maggiori sia sullo stato dei graft , sia su quello delle anastomosi distali . doveroso segnalare , quando presenti , tutti quei reperti cardiaci morfologici non coronarici ritenuti clinicamente rilevanti ( anomalie dello spessore parietale , delle cavit cardiache o dellorigine dei principali vasi mediastinici , masse cardiache trombotiche o non , esiti aneurismatici post - infartuali )  . infine buona regola concludere lesame contrastografico con una scansione estesa a tutto il torace , cos facendo , tra le altre cose , possibile escludere tutte quelle eventuali patologie extravascolari che si presentano clinicamente con dolore toracico tale da mimare unangina ricorrente . 
in questa classe di pazienti la diagnosi differenziale del dolore toracico include infatti il versamento pleurico , il versamento pericardico , lembolia polmonare e linfezione delle suture sternali . nei casi in cui si ha una dimostrazione di patologia si pone il problema della scelta del tipo di metodica di rivascolarizzazione da utilizzare , per tale motivo le informazioni di tipo anatomico fornite dalla tcmd sono cruciali ai fini della selezione dei pazienti da avviare a trattamento percutaneo ( angioplastica con o senza stenting ) o chirurgico . tale scelta risulta guidata dalla localizzazione e dellestensione della malattia . 
si raccomanda una rivascolarizzazione per via percutanea nei pazienti non ad alto rischio , con funzione ventricolare preservata che presentano integrit del graft con lima e stenosi focali subtotali , specialmente 1097 fig . 
7 immagini 3 dvr dellanastomosi prossimale del corpo del graft e dellanastomosi distale di triplice bypass sv - da , lima - lad d1 , ra - lcx . tion techniques ( mpr , mip , vr ) and cannot be separated from an initial assessment of the native axial images . 
vr images , providing a 3d panoramic view , are very useful to define the complex anatomy of grafts and should be used together with the native axial images as a basis for subsequent interpretation of findings . 
the drawbacks of the individual analysis of oblique or curved mpr images and mip images ( dependence on manual orientation of the plane with falsepositive or false - negative stenoses in the first case and overestimation of stenosis due to overprojection in the second ) can be overcome by using the two techniques in a complementary manner [ 34 ]  . 
 it is important to note any noncoronary morphological cardiac findings thought to be clinically relevant ( abnormalities of wall thickness , of the cardiac cavities or of the origin of the main mediastinal vessels , thrombotic or nonthrombotic cardiac masses , postinfarct aneurysm )  . finally , the contrast - enhanced study should be completed with a scan extending to the entire chest to be able to exclude , among others , the presence of possible extravascular disease manifesting with chest pain and mimicking recurrent angina . 
in this class of patients , the differential diagnosis of chest pain includes pleural effusion , pericardial effusion , pulmonary embolism and sternal wound infection . evidence of disease calls for decisions on the type of revascularisation procedure to be used , and the anatomical information provided by mdct is instrumental in selecting patients for percutaneous ( angioplasty with or without stenting ) or surgical treatment . 
repeat surgery is preferred in high - risk patients ( especially those with multivessel disease of the native arteries with left main involvement ) and those with reduced ventricular function , with diabetes , and with severe graft impairment due to chronic total occlusions [ 35 ]  . 
 in patients with severe graft impairment , the panoramic view provided by mdct allows one to provide the surgeon with all the anatomical data needed to plan the repeat operation and minimise the risks of surgery . 
for these reasons , the radiologist needs to provide detailed information on the morphology and course of the native and grafted vessels and the relationship between these and mediastinal structures , the sternum and the chest wall [ 36 ]  . 
si preferisce invece un reintervento chirurgico nei pazienti ad alto rischio ( soprattutto in presenza di malattia nativa multivasale con interessamento del tronco comune sinistro ) , con ridotta funzione ventricolare , diabetici , in presenza di grave compromissione dei graft , come nel caso di ostruzioni totali croniche degli stessi [ 35 ]  . in questa ultima classe di pazienti , la tcmd consente , grazie alla sua visione panoramica , lottenimento di tutti quei dati anatomici necessari al chirurgo per pianificare il re - intervento e minimizzare i rischi connessi a questo . 
lachman mosby elsevier , philadelphia ( 2007 ) isbn - 13 : 978 - 0 - 323 - 01931 - 6 published online : 13 december 2007 this is the fifth edition of a masterpiece book that , through the years , has been a trusty companion to paediatric radiologists and paediatricians , expanding from edition to edition to become more and more complete , being nicknamed the second bible in this field , with caffeys the first . 
the first address syndromes and metabolic disorders , now merged in a single section in contrast to the previous edition , making it easier to use and research the 860 pages , the largest section in the volume . 
these sections are followed by 46 pages listing the pertaining literature ( 22 , 500 entries and 4 , 500 literature references ! )  . as stated by the author in his short preface , this edition has been enriched by 90 new syndromes and metabolic diseases and 35 new skeletal dysplasias : whenever possible , each entity has its appropriate omim number , appropriate locus , gene name and protein involved . 
several new tables have been also prepared ( mucopolysaccharidoses / mucolipidoses entities ; general radiological features of chromosome abnormalities , for example )  . there are two appendices , as well : the first list the international nosology and classification of genetic disorders of bone 2006 ( also to be found in the american journal of medical genetics ) ; the second is a short , pithy chapter titled teaching approach to the skeletal dysplasias . 
in few pages with great clarity describe the path to be followed when one is confronted with a suspected skeletal dysplasia : how to define , describe with proper and corrects terminology ( and not jargon ) what the findings are and correctly classify them . the number of pages increased from 1 , 135 in the fourth edition to the 1 , 365 in this edition ; due to printing art miracles , volume sizes are the same but the weight is reduced ( from 3 , 600g to 3 , 290g : this matters too ! ) : font size compression and paper thickness explain these results . a small ticket , to be found at the back of the front cover , allows , by means of a personal username , free access to a web site . 
this link makes it possible and easy to expand the research or at least narrow its field , and through clinical signs or questa la quinta edizione di unopera che ha accompagnato nel corso degli anni , diventando sempre pi estesa e completa il cammino dei radiologi pediatri e dei pediatri , assumendo le caratteristiche di unaltra bibbia e di testo fondamentale in questo campo , dopo quella del caffey . il volume diviso in tre sezioni : le prima riguarda le sindromi e le malattie metaboliche , ora comprese in un unico capitolo a differenza di quanto non fosse nella quarta edizione , rendendone pi facile la consultazione ed il reperimento . 
la seconda sezione si occupa delle displasie scheletriche svolte in 243 pagine e la terza dedicate ai gamuts : 168 pagine di elenchi completate da 46 riguardanti la letteratura pertinente ( 22500 opzioni e 4500 voci bibliografiche ! )  . come precisato dallautore nella breve prefazione , ledizione attuale si arricchita di 90 nuove sindromi e malattie metaboliche e di 35 nuove displasie scheletriche : ove possibile stato riportato il numero omim , il locus genetico , il nome del gene e la proteina interessata delle affezioni trattate . 
sono state inoltre introdotte alcune nuove tabelle ( malattie da accumulo ; aspetti radiologici generali della malattie cromosomiche , per esempio )  . completano il volume due appendici , la prima , dedicata allinternational nosology and classification of genetic disorders of bone2006 ( pubblicata anche su american journal of medical genetics ) e la seconda , sotto forma di breve , ma succoso capitolo dal titolo teaching approach to the skeletal dysplasias in cui sinteticamente , ma con grande chiarezza , viene descritto il percorso da seguire quando si ha da confrontarsi con una sospetta displasia scheletrica per definirla , descriverla con termini appropriati e corretti ed eventualmente classificarla . complessivamente si passati dalle 1135 pagine della quarta edizione alle 1365 della attuale , ma miracolo dellarte tipografica le dimensioni del volume non sono diverse da quelle del precedente , ma il suo peso ridotto ( da 3600 g a 3290 : anche questo conta ! ) : compressione dei caratteri e carta pi leggera spiegano il risultato . 
 this book is of essential importance , and must absolutely be at hand in the daily practice of all of those dealing with these types of problems , be they general or paediatric radiologists , paediatricians , geneticists or orthopaedic specialists . 
the book is in good company with others on the topic , such as sprangers bone dysplasias , castriota - scanderbegs abnormal skeletal phenotypes and canepas dysmorphic syndromes and constitutional diseases of the skeleton . 
sic transit gloria mundi ! surely not the memory of a great and modest colleague depicted smiling in a photograph taken in the company of lachman that opens and illuminates the first page , followed by a moving , short memorial . 
 permette di ampliare la ricerca e di ottenere diagnosi o di restringere il campo di ricerca attraverso la diagnosi differenziale di segni clinici o di aspetti radiologici . opera fondamentale che non deve assolutamente mancare a chi si occupa di questo tipo di problemi sia radiologo , pediatra , genetista od ortopedico da consultare quotidianamente e da affiancare ad altre opere sullargomento , tipo bone dysplasias dello spranger ; abnormal skeletal phenotypes di castriotascanderbeg e sindromi dismorfiche e malattie costituzionale dello scheletro di canepa . peccato che questa nuova edizione dovr farmi mettere in pensione la precedente , in cui faceva mostra di s una bella dedica del taybi , ora da conservare come un tesoro . 
the purpose of this article is to illustrate a case where acquisition of digital imaging know - how by a modern radiotherapy division has helped to solve a technical problem while allowing substantial savings through the use of free and open - source resources . 
the system developed , called the dicom router , implemented two kinds of routing : manual and automatic , both oriented to link the images acquired with the existing electronic clinical records . 
the need to operate with more than one provider creates a series of integration issues , so that it becomes economically appealing to acquire internally the knowledge needed to interact more precisely with providers of big information technology ( it ) solutions . 
by using them , in - house it technicians are able to implement valuable technical solutions for smallto medium - sized informatization problems , which would otherwise remain unsolved except with great economic efforts . key words open source dicom low cost riassunto obiettivo . 
scopo di questo lavoro presentare un caso in cui lacquisizione in seno ad un moderno reparto di radioterapia del know how relativo allimaging digitale ha consentito di risolvere un problema con un cospicuo risparmio economico grazie allutilizzo di risorse free ed open source . 
stato realizzato un dispositivo , detto dicom router , che implementa due tipologie di instradamento : automatica e manuale , entrambe orientate allintegrazione delle immagini acquisite con il sistema di cartelle cliniche informatizzate . laspetto legato allinstabilit dellhardware stato poi risolto con una tecnica di ridondanza dei dispositivi . 
la necessit di operare con pi fornitori crea una serie di problemi di integrazione per cui spesso diventa economicamente accattivante lidea di acquisire in seno al reparto il know how per dialogare in maniera pi precisa e disambigua con i fornitori di grandi soluzioni informatiche . questa necessit ben si sposa con le possibilit offerte da tecnologie software open source ben documentate ed accessibili a tutti . 
infatti , con luso di queste , il personale tecnico informatico in seno al reparto pu implementare valide soluzioni per i piccoli / medi problemi di informatizzazione che , altrimenti , resterebbero insormontabili o economicamente molto impegnativi . parole chiave open source dicom low cost 1252 r . 
in recent years , however , new technologies have appeared in the field of information technology ( it ) , which allow substantial savings while maintaining the same level of product quality . this result is obtained thanks to the particular type of licence terms , the project conception and the developers attitude . the birth of these technologies ( the most famous of which is probably linux [ 1 ] ) is the beginning not only of a new way of thinking software , but also of a new way of working and sharing knowledge [ 2 ]  . 
this new scenario , together with increased information needs , provides a fertile environment for acquiring , directly in the clinical division , the competence and know - how necessary to manage digital imaging problems internally . here will describe a specific case that required the development of a system , called the dicom router , which is able to route in a complex manner digital diagnostic images , integrating them in the information system used in a modern radiotherapy division . 
this system allows radiographers to send images to the correct destinations with a single operation and to associate images from other divisions to the correct electronic clinical record by modifying the contents of the digital imaging and communications in medicine ( dicom ) files [ 3 ]  . materials and methods to handle both diagnostic and therapeutic information within the information system , in 2004 , our division bought a software programme for managing electronic clinical records ( normally only text data ) and a commercial dicom - compliant pacs server ( dicomed p@cs web ) for managing digital images . 
 the dicom sources initially consisted of a ge prospeed s fast computed tomography ( ct ) scanner , a vidar scanner , two precise linac systems for portal images and two different contouring stations for digital reconstructed radiograph ( drr ) images ( plato and oncentra masterplan )  . 
in addition , there is also a magnetic resonance imaging ( mri ) scanner located in the hospitals radiology division and a cdrom reader to view diagnostic images acquired at other hospitals . despite the presence of a good number of valuable , free open - source solutions [ 47 ] , the need for a flexible , simply configurable , and quickly integratable system , combined with the presence of an it technician , prompted us to develnegli ultimi anni , in molti reparti clinici che trattano limaging digitale , si osservato un aumento della necessit di informatizzare la filiera al fine di poter fruire delle potenzialit offerte dai sistemi informativi per immagini medicali ( pacs ) e dei benefici che ne derivano , soprattutto legati alla maggiore disponibilit dei dati . 
tuttavia , da qualche anno , parallelamente alle soluzioni tradizionali dei grandi gruppi produttori di software , si sono affermate sulla scena dellinformation technology ( it ) alcune tecnologie che consentono , per tipologia di licenza , per concezione progettuale , per mentalit dei realizzatori , di operare considerevoli economie mantenendo invariata la qualit di prodotto . 
la nascita di queste tecnologie ( la pi nota , probabilmente , linux [ 1 ] ) linizio non solo di un nuovo modo di pensare la realizzazione del software , ma anche di usarlo , condividendo in modo aperto le informazioni [ 2 ]  . 
questo nuovo contesto , unitamente alle sempre maggiori necessit informatiche , terreno fertile per lacquisizione in seno ai reparti clinici del know - how necessario a gestire , per quanto possibile internamente , le problematiche tecniche legate allimaging digitale . 
 in accordo con questidea mostreremo un caso specifico che ha richiesto la creazione di un sistema , detto dicom router , in grado di veicolare in maniera complessa delle immagini diagnostiche digitali integrandole con il sistema informatizzato in uso in un moderno reparto di radioterapia . 
tale sistema consente ai tecnici sanitari di radiologia ( tsr ) , con un solo invio , di veder recapitate le immagini alle corrette destinazioni e di associare le immagini acquisite anche da altri reparti alla corretta cartella clinica informatizzata tramite la modifica del contenuto dei files dicom [ 3 ]  . materiali e metodi il reparto , al fine di gestire su supporto informatico le informazioni cliniche , diagnostiche e terapeutiche di ogni paziente , si dotato nel 2004 di un sistema di cartelle cliniche informatizzate ( per la gestione dei dati testuali dei pazienti ) e di un pacs server commerciale dicom compatibile ( dicomed p@cs web ) per la gestione delle immagini digitali associate ai pazienti . 
oltre a questi da aggiungere anche una rmn di un reparto di radiologia dello stesso ospedale ed il supporto cd con il quale talvolta il paziente presenta delle immagini diagnostiche condotte presso altri ospedali . in merito alla metodologia di sviluppo , nonostante siano gi disponibili soluzioni open source e free molto valide 1253 r . 
all these technologies were adopted not only because they are free , but also because they are stable , mature and flexible and sometimes also used by pacs vendors . the hardware used is a personal computer ( pc ) with intel pentium iv processor , 256 megabyte random access memory ( ram ) , hard disk drive ( hdd ) 80 gigabyte and a pc with pentium ii processor , 128 megabyte ram and hdd 40 gigabyte . results the system developed , called the dicom router , is able to acquire images from the divisions dicom sources and to route them to the right targets . 
we thus obtained a redundant system that ensures a good level of reliability given the low likelihood of a double system crash . the two systems were realised and configured as a primary system ( the one with the better hardware ) and a secondary system ( the one with worse hardware )  . 
in particular , the estimated dos time in the case of a server crash ranges from 180 to 240 s , considered sufficient for the needs of our division . to better understand the general system architecture , two aspects need to be considered : one relating to the routing architecture ( manual and automatic ) , and one relating to the security architecture service ( fault tolerance )  . architecture for automatic routing according to the dicom standard , a node in a dicom network is identified by a triplet : < ip address , ae title ( aet ) , tcp port > this allows one to define a number of dicom nodes on the same computer by modifying the parameters of the port and / or the aet . 
in our case , the options provided by the storescp command of the dcmtk libraries made this implementation possible , allowing us to define several dicom nodes on our dicom router : node 1 : < 1.1.36.223 , dicom_router , 105 > node 2 : < 1.1.36.223 , dicom_router , 106 > node 3 : < 1.1.36.223 , dicom_router , 107 > node 4 : < 1.1.36.223 , dicom_router , 108 > node 5 : < 1.1.36.223 , dicom_router , 109 > these different nodes manage the incoming images in different ways ; thus , when a new dicom source is connected to the network and wants to send images to a destination through the dicom router , it is sufficient to configure the node corresponding to the kind of routing wanted as a target on the source . 
pi nello specifico , i due sistemi sono stati realizzati e configurati come sistema primario ( quello con hardware migliore ) e sistema secondario ( quello con hardware peggiore )  . 
il ruolo del secondario solo quello di monitorare i servizi del primario e , nel momento in cui questi non risultino correttamente funzionanti , forzarlo a spegnimento , se possibile , e prendere la sua identit diventando esso stesso primario . 
ci dovrebbe consentire al tecnico informatico di poter intervenire per risolvere i problemi che hanno afflitto il primario originale con un minimo disservizio ( dos , denial of service ) per gli utenti . 
in particolare , per il sistema proposto , si stima il dos causato da un crash del server primario allincirca in 180 , 240 secondi , il che ritenuto tollerabile per le esigenze del reparto . per meglio comprendere larchitettura del sistema generale considereremo separatamente laspetto legato allarchitettura di instradamento ( routing ) , sia manuale che automatica , e quello legato allarchitettura di messa in sicurezza del servizio ( fault tolerance )  . architettura di routing automatico secondo lo standard dicom un nodo della rete identificato da una tripletta : < indirizzo ip , ae title ( aet ) , porta tcp > ci implica la possibilit di definire pi nodi dicom su una stessa macchina modificando la porta e / o laet . 
nel nostro caso , le opzioni messe a disposizione dal comando storescp fornito dalle librerie dcmtk , hanno reso possibile questa implementazione , consentendo di realizzare un dicom router che consta di pi nodi dicom : fig . 
2 the lines labelled 1 indicate the routing of images coming from computed tomography ( ct ) : as shown , they come in the dicom router and from there are sent to the treatment planning system and picture archiving and communication systems ( pacs ) server . 
2 gli archi etichettati come 1 indicano linstradamento di alcune immagini generate dalla tac : come si pu notare queste entrano nel dicom router ed escono in direzione del treatment planning system ( tps ) e del pacs server . 
analogamente , gli archi etichettati come 2 , sempre generati dalla tac , entrano nel dicom router e , sfruttando un nodo dicom differente dal precedente , vengono instradate verso altre destinazioni ( pacs server ed una sistema di contouring contouring station )  . 
this is feasible only for images produced in our division ; for images produced in other radiology divisions ( in the same or in different hospitals ) , this is not possible . 
thus , it is not possible for images produced outside our division to implement automatic routing because the images stored on the pacs server with a wrong patient id would be matched to the wrong electronic clinical record . 
in our case , the only services requiring a database are collateral ( the viewer and the manual routing interface ) , and the data have quite a short lifespan ( no longer than 1 day )  . regarding dicom routing services , the two computers were perfectly replicated in terms of services working on diffig . 
3 sezioni per la modifica delle tag dicom e della spedizione a differenti nodi . 1256 nodo 1 : < 1.1.36.223 , dicom_router , 105 > nodo 2 : < 1.1.36.223 , dicom_router , 106 > nodo 3 : < 1.1.36.223 , dicom_router , 107 > nodo 4 : < 1.1.36.223 , dicom_router , 108 > nodo 5 : < 1.1.36.223 , dicom_router , 109 > questi differenti nodi gestiscono le immagini in ingresso instradandole in maniera differente . 
mentre ci pu essere ammissibile per le immagini prodotte allinterno del reparto , per le immagini prodotte presso altre radiologie ( anche dello stesso ospedale ) , questo non possibile . 
non possibile , quindi , per immagini di questo tipo ( come del resto anche per le immagini ottenute da cd di altri ospedali ) pensare ad un routing automatico , in quanto verrebbero spedite al server ed associate a cartelle cliniche sbagliate . 
partendo dallassunto che questa situazione si possa verificare quando per qualche motivo il server primario si sia scollegato dalla rete ( perch guasto o per motivi di crash di switch ) , la sostituzione di identit mediamente operata in 180 secondi , 240 nel caso peggiore . 
oltre a ci , sia sul primario che sul secondario ogni minuto schedulato il lancio di un agente che verifica , tramite un comando echoscu , il corretto funzionamento dei servizi dicom sulle differenti porte . 
nel momento in cui il comando non riceve loutput corretto , il sistema , primario o secondario che sia , viene forzato al riavvio ( reboot )  . nel momento in cui il server primario si accende o torna in rete dopo una sconnessione temporalmente rilevante , si affaccia alla rete con un altro indirizzo ip e manda un segnale alleventuale server che ha lindirizzo corretto del primario per forzarlo a cambiare indirizzo in quello del secondario . 
cos facendo , se anche il server primario venisse riacceso , o lipotetico switch di rete venisse riparato , non correremmo il rischio di avere conflitti di indirizzi ip nella rete . inoltre , entrambe le macchine sono sotto gruppo di continuit con spegnimento ( shutdown ) pilotato oltre i 3 minuti di mancata alimentazione ( power fault )  . il sistema cos realizzato , opera ininterrottamente da pi di un anno . discussione il sistema , nel suo complesso , ha consentito di verificare che lattuale disponibilit di software free , stabile e maturo , consente ad un qualunque reparto di attrezzarsi con del personale tecnico idoneo al fine di risolvere una serie di problematiche che , altrimenti , chiederebbero lintervento di aziende esterne . 
4 visualizzatore delle immagini dicom acquisite . ferent transmission control protocol ( tcp ) ports ( both have routing services with the same rules ) but differ in one aspect : the internet protocol ( ip ) address . 
the two pc are organised as follow : when the secondary server is not able to ping the primary server but is able to ping other servers in the network , it changes its ip address into that of the primary server , making itself identical ( for the rest of the net ) to the primary server . 
assuming that this case is compatible with a situation where the primary server is disconnected from the net ( due to damage , disc crashes or maybe a switch that has crashed somewhere ) , the identity substitution is operated in 180 s in the best case and 240 in the worst . 
furthermore , both the primary and the secondary servers have an agent , scheduled to start every minute , that checks , through an echoscu command , the state of the dicom services working on different ports . 
a bad output of this command is interpreted by the agent as a problem , so it forces the system to reboot ( primary or secondary , depending on which is giving problems )  . 
another rule requires that when the primary server is reconnected to the network after a temporally significant disconnection , it presents itself on the network with a third ip address and sends a signal to the server acting as the primary server to change its ip address and become a secondary server . 
thus , if a primary server is turned on after a system crash or the switch damage has been repaired , we should not have a conflict of ip addresses in the network . for security reasons , both computers are in a security power area driven by an uninterruptible power supply ( ups ) with controlled shutdown after 3 min of power down fault . discussion the system developed demonstrated that the availability of free and open - source software that is stable and well tested r . 
in our case , for example , the choice of operating system allowed economic savings with respect to a windows solution which , at the same stability level , usually requires an expensive server licence . 
moreover , the absence of the various viruses traditionally present on a windows platform allowed us to avoid the cost of the antivirus and the need to install the numerous windows patches . 
the advantages of this solution are not to be measured only in terms of savings but also in terms of quality : the daily presence of an in - house technician in the division increases his or her awareness of the divisions needs and refines his or her ability to produce a good analysis and develop more efficient solutions . the technical solution adopted , adequate for our aims , was evaluated concurrently with another possible routing technique that involves defining a single dicom node and searching for the right routing policy on a database using source information as a key . 
although more elegant , this method has some problems : it is more complex to implement , it allows only one possible routing for each source and is exposed to problems of concurrent access to a slow device ( the fact that image acquisition is a fast process if compared with database consultation , the system could be slowed , leading to time out )  . 
in particular , in our tests , the simultaneous transmission of images from several multislice ct scanners caused a crash of the mysqld daemon and , in a few cases , of the operating system . the architecture adopted , with several dicom nodes , was justified by its flexibility , simplicity and resulting stability . 
in fact , we think it is reasonable to suppose that the creation of many dicom nodes to be able to cope with many routing rules is not a good idea . 
for this reason , we believe to have achieved , with good margins , system stability with respect to this problem . termini di manualistica , evitando lacquisto di costose licenze per le librerie dicom . i costi nascosti dati dalladozione , in seno al reparto , di un informatico per la gestione dellinformation technology ( it ) hanno s rappresentato un costo fisso ingente ma comunque basso se valutato rispetto al costo giornaliero di quanto richiesto da aziende esterne . 
i vantaggi di questa soluzione non sono misurabili solo in quantit di denaro risparmiata ma anche in qualit di soluzione realizzata : la presenza fissa di un informatico in reparto , infatti , fa s che questi , essendo quotidianamente a contatto con il reparto , sia molto pi consapevole delle esigenze degli utenti e conseguentemente pi abile a condurre lanalisi e a fornire soluzioni efficienti . la soluzione tecnica utilizzata , pur essendo utile agli scopi preposti , stata valutata concorrentemente rispetto ad una tecnica alternativa di routing la quale prevedeva di definire un unico nodo dicom e ricavare il tipo di instradamento in funzione della diagnostica di provenienza . 
questo approccio alternativo , sicuramente pi elegante , avrebbe per sofferto di alcuni problemi : una maggiore complessit di implementazione , la possibilit per una sorgente di aver associato solo un tipo di instradamento per le immagini prodotte e lesposizione a problemi di accesso concorrente ad una risorsa lenta ( infatti dato che lacquisizione delle immagini pu essere molto veloce rispetto ai tempi di consultazione di un database il sistema , acquisita limmagine , troverebbe un collo di bottiglia su questultimo nella ricerca dellinstradamento opportuno )  . 
in particolare , il secondo problema , con carichi di lavoro particolarmente pesanti , nei nostri test ( pi tc multislice che spedivano in contemporanea ) , si tradotto in un crash del demone mysqld ed in alcuni casi in un crash del sistema operativo . in merito a questa osservazione , la scelta routing adottata che prevede pi nodi dicom , si giustificata sulla base del fatto che rappresenta una soluzione flessibile , leggera in termini di peso computazionale e semplice : da ci ne deriva una intrinseca maggiore stabilit . 
lunico elemento che potrebbe fungere da soglia decisionale sono i pesanti limiti dal punto di vista del numero di instradamenti possibili . ragionevole supporre che , nel caso in cui si debbano gestire molte sorgenti con esigenze di instradamento troppo differenti , la scelta di creare molti nodi dicom sul dicom router non sia percorribile . 
intuitivo aspettarsi che , oltre un certo numero di porte aperte , sopratutto quando il sistema sotto stress , si possano verificare dei dos dovuti al crash di qualche servizio . 
tuttavia , dati i nostri test , risultata una ottima stabilit anche per quindici porte aperte e , dato che per le esigenze del reparto ne sono apparse pi che sufficienti sei , riteniamo di essere con ottimi margini nella regione di stabilit del sistema rispetto a tale problema . conclusions conclusioni compared with a few years ago , in a technological scenario that is continuously growing in several directions , the need to operate with more than one provider creates a rispetto a pochi anni addietro , in uno scenario tecnologico in continua ed eterogenea crescita , la necessit di operare con pi aziende fornitrici crea una serie di problemi di inte1258 r . 
by using them , technical operators with no great experience are able to implement valuable technical solutions for small to medium informatization problems , which would otherwise remain unsolved except at considerable expense . 
on the basis of these two concepts , this project not only solved a specific technical problem , it also gave internal personnel hands - on experience of the possibilities that open - source technologies combined with internal know - how can offer , compared with the costly traditional solutions provided by the major it companies . grazione per cui spesso diventa economicamente accattivante lidea di acquisire in seno al reparto il know how per dialogare in maniera pi precisa e disambigua con i fornitori di grandi soluzioni informatiche . 
cos facendo personale tecnico non eccessivamente specializzato pu implementare valide soluzioni tecniche per i piccoli / medi problemi di informatizzazione che , altrimenti , resterebbero insormontabili o economicamente molto impegnativi . 
in ct - guided transthoracic needle biopsy , the final diagnosis and lesion size affect diagnostic accuracy : benign lung lesions and lesions smaller than 1.5 cm or larger than 5.0 cm in diameter provide lower diagnostic yield . key words lung biopsy computed tomography ( ct ) guidance accuracy riassunto obiettivo . 
i valori di sensibilit , specificit , valore predittivo positivo , valore predittivo negativo ed accuratezza , riferiti ad una diagnosi di malignit , sono risultati rispettivamente del 90 , 2% , 99 , 0% , 99 , 8% , 67 , 3% e 91 , 7% . 
la diagnosi finale ( benignit versus malignit ) e le dimensioni della lesione influenzano laccuratezza diagnostica della metodica : addensamenti polmonari di natura benigna e lesioni con diametro < 1 , 5 cm o > 5 cm sono caratterizzati da livelli minori di accuratezza diagnostica . parole chiave polmone biopsia tomografia vomputerizzata ( tc ) guida accuratezza diagnostica 1142 a.m. 
computed tomography ( ct ) - guided needle lung biopsy was first reported by haaga and alfidi in 1976 [ 5 ] , and since then , the techniques excellent efficacy and accuracy and acceptable morbidity and mortality rates ( 0.07% , or one death every 1 , 429 procedures ) have been widely demonstrated [ 616 ]  . 
whether carried out with fine - needle - aspiration cytology ( fnac ) or core biopsy ( cb ) , the biopsy provides adequate material for cytological or histological examination and , if necessary , for microbiological evaluation [ 1113 , 1721 ]  . 
cb is more sensitive in defining benign lesions and in characterising diffuse or lymphoproliferative diseases of the lung , where the assessment of the tissue architecture is instrumental to the diagnosis ( accuracy > 80% for cb and 50%70% for fnac ) [ 9 , 2225 ]  . 
lesions smaller than 1 cm are easier to sample with fnac [ 19 , 22 , 23 ]  . the reported sensitivity of fnac varies and is positively affected by the presence of the cytopathologist on site during the biopsy procedure [ 26 , 27 ]  . 
immediate cytological assessment increases the techniques sensitivity and reduces the number of inadequate samples and false negative results [ 2628 ] , as the on - site cytopathologist can judge the adequacy , quantity and quality of the sample , suggest the need to repeat the procedure or request cb with histological assessment [ 22 , 26 ]  . several studies have investigated the factors affecting diagnostic accuracy of ct - guided transthoracic needle biopsies . 
it is well established that the most important factor is the final diagnosis , as malignant lesions ( regardless of histological type ) are characterised by greater sensitivity compared with benign masses . 
other variables ( lesion depth , number of passes , cavitations and necrotic centre , morphology , location , radiologists experience , needle diameter and presence of pneumothorax and / or bleeding ) were not found to be significant [ 32 ]  . the purpose of this paper is to present our experience with a large cohort of patients and discuss the results achieved in relation to diagnostic accuracy . 
in particular , we extensively analyse a number of variables ( relating to the patient , the lesion or the procedure ) in an attempt to correlate them to potential influences on diagnostic accuracy and reach a conclusive judgement on the efficacy of the procedure . 
lagobiopsia polmonare tc guidata fu riportata in letteratura per la prima volta nel 1976 da haaga [ 5 ] e da allora numerosi autori ne hanno dimostrato lestrema efficacia ed accuratezza associate ad un accettabile tasso di morbidit e mortalit ( 0 , 07% , ovvero un decesso ogni 1429 manovre effettuate ) [ 616 ]  . 
il prelievo , eseguito tramite aspirazione con ago sottile ( fine needle aspiration citology , fnac ) o con ago tranciante ( core biopsy , cb ) , consente di ottenere , rispettivamente , materiale sufficiente per lesame citologico o istologico ed infine , se necessario , per una valutazione microbiologica [ 1113 , 1721 ]  . 
la cb ha maggiore sensibilit nella definizione delle lesioni benigne e nella caratterizzazione delle malattie polmonari diffuse o linfoproliferative , nelle quali la valutazione dellarchitettura tissutale importante per la diagnosi ( valori di accuratezza > 80% per la cb e tra il 50% ed il 70% per la fnac ) [ 9 , 2225 ]  . 
le lesioni di dimensioni inferiori al centimetro risultano essere pi facilmente campionabili mediante fnac [ 19 , 22 , 23 ]  . la sensibilit della fnac variabile nelle casistiche riportate in letteratura ed positivamente influenzata dalla presenza in sala radiologica del citopatologo al momento del prelievo [ 26 , 27 ]  . 
il citopatologo , infatti , in grado di dare indicazione sulladeguatezza del prelievo , sulla quantit e qualit del materiale campionato , pu suggerirne leventuale ripetizione o richiedere lintegrazione con lesame istologico dopo cb [ 22 , 26 ]  . alcuni autori hanno analizzato le variabili che influenzano laccuratezza diagnostica delle agobiopsie transtoraciche tc guidate . 
da tempo assodato come il pi importante fattore in questo senso sia la diagnosi finale corretta , dato che le lesioni maligne ( indipendentemente dallistotipo ) sono caratterizzate da livelli di sensibilit significativamente maggiori rispetto agli espansi di origine benigna . 
considerando altre variabili , tsukada stato il primo a dimostrare come la graduale riduzione delle dimensioni della lesione conducesse ad un proporzionale decremento nei valori di accuratezza diagnostica [ 13 ]  . 
i risultati di tsukada sono per stati successivamente confermati da yeow che , in una coorte di 649 soggetti , ha riscontrato come sia la diagnosi finale sia le dimensioni della lesione influenzassero il valore di accuratezza [ 20 ]  . 
the study population comprised 154 subjects who underwent surgical resection ( for whom definitive postoperative histological assessment was available ) and nonsurgical patients who had completed at least 12 months of follow - up ( 454 subjects )  . 
the population included 402 men and 206 women , with a mean age of 65.7 years [ ( median 67 ; standard deviation ( sd ) 9.4 years with 95% confidence interval ( ci ) ; range 2987 years )  . 
exclusion criteria were lesions < 5 mm in diameter ( calculated as the mean of the long and short axis ) , significant changes in blood - coagulation profile , contralateral pneumonectomy , patients inability to maintain a lying position and / or to follow verbal or visual instructions and patients refusal to accept the potential risks associated with the procedure and sign the informed consent form . all biopsies were performed according to a standard protocol by the same interventional radiologist ( ac ) under ct guidance with a spiral dual - detector - row scanner . 
after positioning the patient on the ct table in prone , supine or lateral decubitus , depending on lesion location , an initial localisation scan was obtained by acquiring the entire mass on 5mm - thick contiguous transverse sections . 
then , optimal access ( skin entry site and needle path ) was defined on ct images , taking care to sample the lesion away from low - density areas , which are often central and indicative of necrosis [ 13 , 17 , 18 ]  . 
after having established the entry site and chosen the type and length of the needle ( depending on lesion depth and , whenever possible , the shortest route [ 33 ] ) , the needle entry site was anaesthetised ( 2% lidocaine ) , the needle , or the needle guide in the case of cb , positioned and the patient instructed to hold his or her breath . at this point ct scans were obtained to visualise the needle tip in relation to the lesion . 
in particolare verranno estensivamente analizzate alcune variabili ( riferite al paziente , alla lesione od alla procedura ) nel tentativo di correlarle a potenziali influenze sui valori di accuratezza per formulare un giudizio critico conclusivo sulla efficacia della procedura interventistica . materiali e metodi popolazione di studio in un intervallo temporale compreso tra novembre 2002 ed agosto 2005 sono stati consecutivamente sottoposti a procedura interventistica transtoracica tc guidata per laccertamento della diagnosi ( agoaspirazione transtoracica con ago sottile o con ago spinale o biopsia con ago tranciante ) 608 pazienti , per un totale di 612 procedure . 
la coorte in studio ai fini della formulazione di un giudizio di accuratezza della metodica ha compreso tutti i 154 soggetti resecati ( per i quali risultata disponibile la valutazione istologica definitiva postoperatoria ) ed i pazienti non chirurgici che avessero conseguito un follow - up non inferiore a 12 mesi ( 454 soggetti )  . la popolazione ha pertanto incluso 402 soggetti di sesso maschile e 206 femminile , con unet media di 65 , 7 anni ( mediana 67 anni ; ds9 , 4 anni con ic 95% ; intervallo 2987 anni )  . 
i pazienti sono afferiti in parte con proposta di prestazione ambulatoriale ed in parte in regime di ricovero ordinario . sono state considerate tutte le lesioni intraparenchimali ( centrali e periferiche ) , ovvero gli espansi circondati da tessuto polmonare areato o a diretto contatto con le strutture ilari e / o la superficie pleurica il cui epicentro cadesse allinterno del polmone ( dimensione media delle lesioni 36 , 8 mm ; mediana 31 , 5 mm ; ds20 , 5 mm con ic 95% ; intervallo 7103 mm )  . protocollo bioptico nessun paziente risultato anamnesticamente positivo per diatesi emorragica o ha presentato alterazioni della crasi ematica e del profilo emocoagulativo . 
i soggetti in trattamento anti - aggregante e / o anticoagulante hanno sospeso tale terapia per un periodo antecedente la biopsia di 7 giorni . sono stati raccolti dal radiologo un breve raccordo anamnestico ed il consenso informato . 
al momento di ogni biopsia , risultata disponibile una precedente tc diagnostica . i criteri di esclusione da noi adottati sono stati : lesioni con diametro ( calcolato sulla media delle dimensioni degli assi maggiore e minore ) < 5 mm ; alterazioni significative dellasa.m. 
biopsies were carried out by needle aspiration with a 21 - gauge fine needle or a 20gauge spinal needle ( with the single needle technique ) , or by core biopsy with an 18 - gauge cutting needle ( and coaxial technique )  . our initial approach in pulmonary nodules always uses a chiba fine needle ( especially for small lesions ) , except in cases of a second attempt after a previous inconclusive procedure . 
this made it possible to have an evaluation of material adequacy and an extemporary general indication about the nature of the lesion within minutes of the procedure [ 2628 ]  . 
in the case of inadequate or insufficient samples for cytology or histology , the biopsy procedure was repeated immediately : in particular , 190 / 612 procedures ( 31.0% ) required more than one sampling ( mean 1.32 samples per procedure ; range 14 )  . to assess possible complications ( pneumothorax , needletrack bleeding ) , postprocedural ct scans were acquired 35 min after the procedure ( time required for the cytopathologist to prepare the slides and judge their adequacy )  . data collection : definition and selection of variables multiple discrete or continuous variables , relating to the patient , the lesion or the procedure , were considered . 
dopo aver posizionato il paziente sul lettino tc in decubito prono , supino o laterale a seconda della localizzazione della lesione , si proceduto ad una prima centratura della lesione attraverso lacquisizione dellintero espanso su sezioni trasverse contigue di 5 mm di spessore . 
successivamente , sulle immagini tc a monitor si pianificata la migliore via di accesso ( come punto di ingresso cutaneo e tragitto dellago ) al fine di campionare la lesione avendo cura di evitare regioni di ipodensit , spesso centrali ed indicative di necrosi , nel suo contesto [ 13 , 17 , 18 ]  . 
dopo aver definito il punto di ingresso dellago e scelto la tipologia e la lunghezza dellago ( a seconda della profondit della lesione e pianificando , ogni qual volta sia stato possibile , il tragitto pi breve [ 33 ] ) si effettuata unanestesia locale in corrispondenza del punto cutaneo di ingresso ( lidocaina 2% ) , quindi si posizionato lago , o lago guida per le biopsie trancianti , chiedendo al paziente di mantenere lapnea . 
per gli espansi di difficile centratura ( 162 / 612 procedure , 26 , 5% del totale ) quali piccoli noduli centrali o integralmente coperti da strutture ossee , lago bioptico stato introdotto nei tessuti molli sino alla superficie pleurica evitandone accuratamente la trasgressione . 
in alcuni casi si effettuato pi di un passaggio pleurico , dal momento che o la lesione - bersaglio non stata raggiunta dalla punta dellago al primo tentativo nonostante i riorientamenti intraparenchimali dellago o , nei prelievi senza ausilio della tecnica coassiale , il materiale risultato inadeguato e si ricorsi ad un nuovo prelievo . 
in particolare , 350 / 612 procedure ( 57 , 2% ) hanno richiesto un solo passaggio pleurico ( media 1.5 passaggi pleurici per procedura ; intervallo 14 )  . 
il prelievo stato effettuato tramite agoaspirazione con ago sottile 21 gauge ( g ) o con ago spinale 20 g ( con tecnica ad ago singolo ) , o biopsia con ago tranciante 18 g ( utilizzando la tecnica coassiale )  . 
 per i noduli polmonari sempre preferito da noi un iniziale approccio con ago sottile di chiba ( soprattutto nelle lesioni di piccole dimensioni ) , tranne nei casi di un secondo tentativo dopo un precedente prelievo non conclusivo . nellevenienza della ripetizione iterativa viene considerata la possibilit di utilizzare un ago di calibro maggiore ( spinale ) od un tranciante . 
final diagnoses were based on the surgical outcomes ( surgical patients ) or the imaging data and clinical - radiological follow - up for a period of at least 12 months ( response to first - line chemotherapy or antibiotic treatment designed on the basis of the biopsy ; unchanged imaging findings in the absence of treatment )  . 
in relation to malignant diagnoses , we considered : true positives for malignancy : all cases classified as malignant at transthoracic needle biopsy and confirmed by histology of the surgical specimen ; cytohistology of an additional biopsy from a distant metastatic lesion ; imaging evidence ( radiology or nuclear medicine ) of distant metastases ; partial or complete response to first - line chemotherapy ; clinical course . 
in surgical cases , we assessed the reliability of the needle biopsy in providing precise characterisation with specific histological type a negative finding ( benign lesion ) was classified as a true negative for malignancy at fnac or cb when its benign nature was confirmed by subsequent surgery or biopsy or when the lesion appeared stable , smaller or had totally disappeared at follow - up ct ( 12 - month follow - up ) in an untreated patient or a patient treated with appropriate antibiotic , but not antineoplastic , therapy [ 18 , 22 ] false positives for malignancy : all cases with a positive biopsy not confirmed by surgery false negatives for malignancy : all cases with a negative ( benign at fnac / cb ) or indeterminate result ( absence of cellular atypia , presence of atypical cells not otherwise specified , presence of nonspecific or granulomatous inflammatory reaction , insufficient material or blood contamination ) at transthoracic needle biopsy with positive surgical outcome or disease progression at follow - up imaging . the quality of each sample obtained by fine - needle transthoracic biopsy was scored from 0 to 3 , according to the following criteria : 0 = slides containing exclusively blood components ( blood contamination ) without epithelial cells ; 1 = finding of nonspecific benign cells ( inflammatory ; type i and ii pneumocytes ; atypical cells not otherwise specified ) ; 2 = presence of morphologically malignant cells , without characterisation of histological type or without differentiation between small - cell or non - small - cell cancer ; 3 = slides containing benign or malignant cells with definite histological characterisation . 
samples with scores 0 , 1 and 2 ( when justified by inability to differentiate between small - cell and non - small - cell cancer ) were considered nondiagnostic and therefore classed as false negatives in relation to the final diagnosis . 
samples with scores of 2 and 3 were considered adequate . size 1146 the dimensions of each lesion were measured on screen using a dedicated programme ( electronic callipers ) , in the two maximum orthogonal axial diameters , on the preliminary localisation scan reconstructed from the raw data with adequate window and level settings for lungs . 
in tutti i casi stato utilizzato una lunghezza dello scatto della pistola bioptica pari a 3 , 3 cm . la presenza del citopatologo in sala radiologica , essenziale nei prelievi citoaspirativi , ha costituito elemento caratterizzante tutte le procedure . 
in caso di materiale inadeguato od insufficiente ad unanalisi citologica od istologica si provveduto alla immediata ripetizione del prelievo : in particolare 190 / 612 procedure ( 31 , 0% ) hanno richiesto pi di un prelievo ( media 1 , 32 campioni per procedura con intervallo 14 )  . per valutare linsorgenza di complicanze ( pneumotorace , soffusione emorragica lungo il tragitto dellago ) sono state acquisite , circa 35 minuti dopo il prelievo ( nel tempo richiesto dal citopatologo per preparare gli strisci e dare giudizio di idoneit ) , scansioni tc di controllo . raccolta dei dati : definizione e selezione delle variabili sono state considerate molteplici variabili , a valore discreto o continuo , riferite al paziente , alla lesione od alla stessa manovra interventistica . 
per entrambe le categorie sono stati calcolati , attraverso la costruzione di tabelle 22 , i livelli di accuratezza ( sensibilit , specificit , valore predittivo positivo e negativo , proporzione di falsi positivi e negativi , accuratezza globale della metodica ) correlando il risultato della biopsia transtoracica con la diagnosi finale . 
la diagnosi definitiva stata ottenuta attraverso lanalisi del dato chirurgico ( per i pazienti resecati ) , dei dati di imaging e del follow - up clinico / radiologico per un periodo non inferiore a 12 mesi ( risposta a trattamenti chemioterapici di i linea o a trattamenti antibiotici impostati sulla base del risultato bioptico transtoracico ; stazionariet radiologica dei reperti in assenza di terapia )  . 
a questo proposito sono stati considerati , in rapporto alle diagnosi maligne : veri positivi per malignit i casi classificati maligni allagobiopsia transtoracica e confermati : dal dato istologico sul pezzo operatorio ; dal dato cito - istologico derivante da una ulteriore aggressione bioptica di una lesione metastatica a distanza ; dallevidenza strumentale ( indagini radiologiche e di medicina nucleare ) di metastasi a distanza ; dalla risposta parziale o completa a trattamenti chemioterapici di i linea ; dal decorso clinico . 
nei casi resecati stata valutata laffidabilit dellagobiopsia transtoracica nel fornire una precisa caratterizzazione con specificit di istotipo ; un esito negativo ( ovvero di natura benigna ) stato classificato vero negativo per malignit alla fnac o cb in caso di successiva conferma chirurgica o bioptica o se a.m. 
we recorded data on the presence of single or multiple pulmonary lesions and lobar location specifying possible contact or close proximity to an interlobar fissure , the hilum or major intrapulmonary vessels . 
the depth of the consolidation was defined as the distance between the entry site on the pleural surface and the proximal edge of the lesion , measured along the needle path on lung window settings [ 13 , 32 , 3436 ]  . 
i prelievi con punteggio 0 , 1 e 2 ( se per questi ultimi non stata possibile una differenziazione tra neoplasia a piccole cellule e non ) sono stati considerati non diagnostici e quindi classificati come falsi negativi in rispetto alla diagnosi finale . 
i prelievi con punteggio 2 e 3 sono stati invece considerati adeguati . needle type and calibre dimensioni in all procedures , we used either a single needle ( 21 - gauge chiba needle ; 20 - gauge spinal needle ; 18 - gauge cutting needle with coaxial technique ) or , in the event of multiple biopsies , a consecutive combination of different needles . 
the choice of the type of needle was based on parameters such as lesion size , clinical suspicion ( history , clinical and imaging data ) , operators preferences and the presence of the cytopathologist . 
during each anale dimensioni di ogni lesione sono state misurate a monitor mediante programma dedicato ( calibro elettronico ) , nei due diametri assiali ortogonali massimi , sulle scansioni di centratura preliminari ricostruite dai dati grezzi attraverso adeguata finestra e livello per parenchima polmonare . 
stata quindi calcolata la media aritmetica relativa alle misurazioni ottenute per ciascuna lesione in esame . morfologia e localizzazione le lesioni sono state suddivise in noduli e masse , se caratterizzate da un diametro trasverso massimo < o 30 mm rispettivamente . 
sono state considerate consolidazioni gli infiltrati cuneiformi , di natura fluida o cellulare , a distribuzione segmentaria o lobare , associati o meno a broncogramma aereo . sono stati registrati i dati relativi alla presenza di lesioni polmonari singole o multiple , la localizzazione lobare specificando leventuale contatto o la stretta vicinanza ad una scissura interlobare , allilo o a strutture vascolari intrapolmonari di rilievo . 
la profondit delladdensamento stata considerata quale distanza tra il punto di ingresso della superficie pleurica sino al margine prossimale della lesione , misurata lungo il tragitto dellago su finestra per parenchima polmonare [ 13 , 32 , 3436 ]  . 
the variables of the two groups in each category were correlated . differences between the groups were examined using the nonparametric mann - whitney u test or variance analysis according to kruskal - wallis , when indicated . 
differences between proportions were analysed with pearsons 2 test or students t test . parameters considered significant in determining diagnostic accuracy were further stratified and correlated to accuracy with the aid of contingency graphs and tables . 
a p value < 0.05 was taken as significant in all cases . results in calculating the methods diagnostic accuracy , we considered all 608 patients included in the study : there were 154 surgical patients ( for whom postoperative surgical evaluation was considered the gold standard against which the interventional technique was compared ) there were 454 nonsurgical patients who had completed , as at august 2006 , an imaging , clinical and treatment - response follow - up of at least 12 months ; in these cases the final diagnosis was inferred from the benign or malignant behaviour of the lesion we considered 612 procedures ; the quality of each of the 612 samples was assigned a discrete score from 0 to 3 at the end of each procedure in 435 / 612 procedures ( 71.1% ) , the needle biopsy recovered benign or malignant cells , allowing specific cytohistological characterisation ( score 3 )  . 
of these , 52 were benign , 382 were malignant and only one revealed the presence of a hamartochondroma associated with a primary squamous cell carcinoma of the lung there were 75 / 612 samples ( 12.2% ) that demonstrated definitely malignant cells ( score 2 ) , without providing information on histological type . 
four samples demonstrated the presence of definitely neoplastic cells ( probably epithelial ) without providing discrimination between small - cell and non - small - cell cancer , which is essential for therapy . 
in addition , the only false positive result in our cohort was encountered among these four cases : a suspected carcinoma not otherwise specified ( fnac ) was found at surgery to be an excavated granuloma characterised by severe cellular dysplasia due to previous tuberculous infection in 46 / 612 cases ( 7.5% ) , the sample was scored 1 , as 19 / 46 samples ( 41.3% ) demonstrated exclusively normal lung 1148 mento lineare di parenchima polmonare trasgredito dallago . caratteristiche interne sono state considerate laspetto solido ( se con finestra mediastinica risultava visualizzabile almeno il 50% della superficie dellespanso rispetto a quanto visibile con finestra polmonare ) , la presenza di escavazioni ( aree allinterno della lesione con valori di attenuazione propri dellaria ) , calcificazioni e broncogramma aereo . 
 stata inoltre valutata , con criterio visivo ed attraverso lausilio della misurazione digitale dei dati di attenuazione mediante roi , la densit basale della lesione per ricercare eventuali aree di disomogeneit riferibili a necrosi . tipo di ago e calibro per tutte le procedure si ricorso alluso esclusivo di un unico ago ( chiba 21 g ; spinale 20 g ; tranciante 18 g con tecnica coassiale ) o ad associazione consecutiva di diversi aghi nel caso di prelievi multipli . 
la scelta di tipologia dellago stata posta secondo alcuni parametri quali le dimensioni della lesione , il sospetto clinico ( su basi anamnestiche , obiettive e di imaging ) e le preferenze delloperatore , oltre che la presenza dellanatomopatologo in sala radiologica . 
in particolare , lago sottile di chiba ha trovato esclusivo impiego in 470 / 612 procedure ( 76 , 8% ) , lago spinale in 76 ( 12 , 4% ) , il tranciante in 35 ( 5 , 7% ) , lassociazione chibaspinale in 27 ( 4 , 4% ) e lassociazione chiba - spinale - tranciante in 4 ( 0 , 7% )  . complicanze analisi statistica la comparsa di pneumotorace o di sfumate opacit parenchimali con aspetto radiologico a vetro smerigliato ( da impegno alveolare per emorragia ) stata registrata per ogni procedura . lanalisi statistica stata condotta con lutilizzo del programma statistica 6.1 ( statsoft software , per windows ) e mirata alla valutazione dellaccuratezza della procedura . 
i pazienti sono stati , in ogni sessione analitica , suddivisi in due gruppi omogenei per variabili discrete a soluzione dicotomica ( si / no ) ed analizzati per le diverse variabili , discrete o continue , che si ipotizzava influenzare i livelli di accuratezza : i gruppi sono stati suddivisi tra le diagnosi corrette e le diagnosi non corrette o non possibili a causa dellinadeguatezza del prelievo agobioptico . 
le differenze tra i gruppi sono state esaminate utilizzando i tests non parametrici mann - whitney u - test o analisi della varianza secondo kruskal - wallis , quando indicati . 
le differenze tra le proporzioni sono state analizzate con il test 2 di pearson od il test t di student . i parametri considerati significativi , nel determinare i livelli di accuratezza diagnostica , sono stati ulteriormente stratificati e correlati allaccuratezza con lausilio di grafici a.m. 
the discordance between the biopsy result and the final diagnosis is due to sampling errors , with sampling of surrounding healthy lung parenchyma or perilesional reactive inflammatory tissue there were 56 / 612 samples ( 9.1% ) scored 0 owing to sample inadequacy ( blood contamination ) and which were therefore classed as nondiagnostic . 
in 35 / 56 samples ( 60.7% of samples with a score of 0 ) , the lesion was subsequently found to be malignant . a final diagnosis based on the criteria previously described could be obtained for all 612 procedures : 17.0% ( 104 / 612 ) of lesions were found to be benign , whereas 83.0% ( 508 / 612 ) were malignant . 
the 458 cases positive for malignancy , with subsequent confirmation ( one malignant case at biopsy was subsequently found to be a false positive ) comprised 411 primary lung cancers , seven nonepithelial neoplasms and 40 metastatic tumours with secondary localisation to the lung ( table 1 )  . of these 458 patients , 46 ( 7.6% ) had a history of neoplastic disease at another location . 
of these 46 , the metastatic origin of the lung lesion was demonstrated in 40 , whereas in the remaining six cases , the primary nature of the lung nodule was demonstrated with the aid of immunocytochemistry and comparison with cytology and / or histology of the extrapulmonary neoplasm , when available . among the 459 cases of malignancy diagnosed at biopsy , o tabelle di contingenza . 
in tutti i casi stato considerato significativo un valore di p < 0 , 05 . risultati per calcolare laccuratezza diagnostica della metodica sono stati inclusi nello studio 608 pazienti : centocinquantaquattro sono i soggetti sottoposti ad intervento chirurgico ( per i quali disponibile lesame istologico post - operatorio , considerato il gold standard di raffronto con la metodica interventistica )  . quattrocentocinquantaquattro sono , invece , i pazienti non chirurgici che presentano ad agosto 2006 un followup di imaging , clinico e di risposta terapeutica non inferiore a 12 mesi ; in base al comportamento benigno o maligno della lesione in esame stata , quindi , dedotta la diagnosi finale . complessivamente sono state considerate 612 procedure . per ciascuno dei 612 campioni ottenuti , a conclusione di ogni procedura stato attribuito un punteggio discreto da 0 a 3 per asserirne la qualit : in 435 / 612 procedure ( 71 , 1% dei casi ) si sono ottenute , dal prelievo agobioptico , cellule benigne o maligne che hanno permesso una precisa caratterizzazione citoistologica della lesione ( punteggio 3 )  . 
di queste 52 sono risultate benigne , 382 di natura maligna , mentre in 1 solo caso si registrata la presenza di un amartocondroma associato ad un carcinoma polmonare primitivo del tipo squamocellulare ; in 75 / 612 prelievi ( 12 , 2% dei casi ) sono state riscontrate cellule di sicura origine maligna ( punteggio 2 ) , ma non stato possibile trarre conclusioni sullistotipo . 
in contrast , 50 procedures were false negative for malignancy ( negative result at biopsy , with malignant cells detected at repeat biopsy , surgery or follow - up )  . 
table 3 summarises the cytological diagnoses of the 52 cases that were negative for malignancy at biopsy . if we consider only benign lesions at final diagnosis assenza di una suddivisione , critica ai fini terapeutici , in tumore a piccole cellule e non . 
questi ultimi casi pongono importanti problematiche in termini di gestione del paziente per il fatto che non si pu pianificare il corretto iter terapeutico , impedendo in questo modo allagobiopsia di porsi a termine delliter diagnostico . 
inoltre , tra questi 4 casi si riscontrato lunico risultato bioptico falso positivo dellintera coorte : un sospetto carcinoma di non pi precisa caratterizzazione ( fnac ) si poi dimostrato essere , dopo resezione chirurgica , una granulomatosi escaa final diagnoses are based on the retrospective analysis of the outcome of surgery , repeated biopsy , imaging , and clinical follow - up for at least 12 months . 
 malignant pulmonary lesions : sensitivity 90.2% ( 458 / 508 ) , specificity 99.0% ( 103 / 104 ) , positive predictive value 99.8% ( 458 / 459 ) , negative predictive value 67.3% ( 103 / 153 ) , false positive rate 0.22% ( 1 / 459 ) , false negative rate 10.9% ( 50 / 508 ) , accuracy 91.7% [ ( 458 + 103 ) / 612 ] , overall diagnostic accuracy 83.3% [ ( 458 + 52 ) / 612 ] ( for all lesions , benign and malignant ) table 2 results of 612 computed - tomography - guided transthoracic needle biopsies final diagnosisa malignant biopsy diagnosis malignant benign / inadequate total diagnosi bioptica maligno benigno - inadeguato totale 1150 tabella 2 risultati di 612 procedure agobioptiche polmonari diagnosi finalea maligno benign 103 ( 52 / 51 ) benigno 103 ( 52 / 51 ) total totale a la diagnosi finale deriva dallanalisi retrospettiva dei risultati della chirurgia , di uneventuale successiva agobiopsia transtoracica e dallesito del followup clinico / radiologico pari ad un periodo non inferiore ai 12 mesi . 
conversely , in 51 cases , the benign nature of the lesion could not be defined because of sample inadequacy ( 30 samples scored 1 and 21 scored 0 )  . with regard to malignant lesions , 99.8% of malignancies at vata caratterizzata da severa displasia cellulare in relazione alla pregressa infezione tubercolare ; in 46 / 612 casi ( 7 , 5% ) stato attribuito , al campione prelevato , un punteggio pari a 1 , dal momento che in 19 / 46 casi ( 41 , 3% ) si sono riscontrate esclusivamente cellule normali proprie del tessuto polmonare ( pneumociti di i e ii ordine ) , in 14 / 46 ( 30 , 4% ) cellule flogistiche in assenza di significative atipie ed in 13 / 46 ( 28 , 3% ) cellule atipiche non ulteriormente caratterizzabili , ma neanche classificabili come sicuramente maligne . 
in 16 di questi 46 prelievi ( 34 , 7% dei prelievi a punteggio 1 ; 2 , 6% sul totale delle procedure ) le lesioni campionate sono poi risultate di natura maligna . 
la discordanza tra risultato bioptico e diagnosi finale dovuta ad errori di campionamento , per prelievo di parenchima polmonare sano limitrofo o di tessuto flogistico reattivo perilesionale ; infine 56 / 612 prelievi ( 9 , 1% ) hanno ottenuto un punteggio pari a zero a causa dellinadeguatezza del materiale analizzato dallanatomopatologo ( campioni ematici ) e sono quindi stati classificati come non diagnostici . 
in 35 / 56 prelievi ( 60 , 7% dei campioni a punteggio 0 ) la lesione poi risultata maligna . per tutte le 612 procedure stato possibile ottenere una diagnosi finale con i criteri gi ampiamente descritti : il 17 , 0% ( 104 / 612 ) delle lesioni risultato di natura benigna , mentre lo 83 , 0% ( 508 / 612 ) maligna . 
lagobiopsia transtoracica percutanea ha conseguito un risultato diagnostico in 511 casi su 612 ( 83 , 5% , prelievi a punteggio 2 e 3 ) , mentre in 101 procedure ( 16 , 5% , prelievi a punteggio 0 e 1 ) non stato possibile fornire un giudizio affidabile . 
i 458 casi positivi per malignit , con conferma successiva ( un caso maligno alla biopsia poi risultato un falso positivo ) hanno compreso 411 carcinomi polmonari primitivi , 7 neoplasie non epiteliali e 40 tumori metastatici con localizzazione secondaria al polmone ( tabella 1 )  . di questi 458 pazienti , 46 ( 7 , 6% ) presentavano un precedente anamnestico di malattia neoplastica in altra sede . 
tra questi ultimi , in 40 si dimostrata lorigine metastatica della lesione polmonare , mentre nei restanti 6 casi stato possibile definire la natura primitiva del nodo polmonare attraverso lausilio della immunocitochimica ed il confronto , quando disponibile , con i reperti citologici e / o istologici del tumore extrapolmonare . tra i 459 riscontri risultati maligni allagobiopsia , solo in un caso la diagnosi definitiva non ha confermato il dato configurando quindi la presenza di un unico falso positivo per malignit . 
si sono invece registrate 50 procedure false negative per malignit ( risultato negativo per cellule neoplastiche con esito maligno alla ripetizione della procedura , allintervento chirurgico od al follow - up )  . 
in tabella 2 vengono riportati i risultati conseguiti , in termini di affidabilit della metodica , sulla corretta diagnosi delle lesioni maligne . la tabella 3 riassume le diagnosi citologiche nei 52 casi risultati negativi per malignit allagobiopsia . analizzando le sole lesioni benigne alla diagnosi finale ( 104 / 612 , 17% ) , lagobiopsia ha permesso di conseguire un sicuro giudizio di benignit con diagnosi specifica in soli 52 1151 a.m. 
a specific judgement of benignity of the biopsy sample could , however , be made in only 34% of samples , characterised by the definite absence of neoplastic cells ( 52 / 153 ) ( table 2 )  . 
finally , table 4 demonstrates that lesion depth ( the portion of aerated lung traversed by the needle ) , morphology and lobar location ; the presence of calcification , cavitation and necrotic centre ; and the occurrence of complications ( pneumothorax and bleeding ) have no influence on the diagnostic accuracy of transthoracic ct - guided needle biopsy . discussion with the use of percutaneous transthoracic needle biopsy , and in particular of fnac , as an initial minimally invasive procedure for evaluating the nature of pulmonary lesions , this study obtained an overall diagnostic accuracy of 84% , with levels of 92% and 67% for malignant and benign lesions , respectively . 
in 51 lesioni benigne non invece stato possibile stabilirne la natura a causa dellinadeguatezza del prelievo ( 30 prelievi a punteggio 1 e 21 prelievi a punteggio 0 )  . riferendosi agli addensamenti polmonari di natura maligna , il 99 , 8% delle lesioni considerate maligne allagobiopsia poi stata confermata ( 458 / 459 , valore predittivo positivo per malignit ) , mentre il 67 , 3% dei prelievi con assenza di cellule tumorali ( prelievi classificati come benigni , od inadeguati ) risultato benigno ( 103 / 153 , valore predittivo negativo per malignit )  . 
stato comunque possibile dare un giudizio specifico di benignit del prelievo agobioptico solo nel 34% dei campioni , caratterizzati dalla sicura assenza di cellule tumorali ( 52 / 153 ) ( tabella 2 )  . 
la sensibilit e la specificit per la diagnosi di malignit sono risultate del 91% e 99% rispettivamente , con una proporzione di falsi positivi trascurabile ( 0 , 22% ) ed una proporzione di falsi negativi dell11% . 
questo valore raggiunge l88 , 2% ( 540 / 612 ) se , tra le diagnosi agobioptiche corrette , si includono i 30 prelievi a punteggio 1 poi risultati benigni ( ovvero reperti considerati allagobiopsia negativi per cellule neoplastiche in assenza di una specifica diagnosi )  . 
in tabella 4 riassunto linsieme di variabili che si supposto esercitare una influenza sui livelli di accuratezza della metodica : le uniche variabili associate con significativit statistica ad una riduzione dei livelli di accuratezza diagnostica sono risultate la discrimante della diagnosi finale ( categoria benigno versus maligno ) e le dimensioni della lesione . 
la tabella 4 dimostra , infine , come la profondit della lesione ( ovvero la quota di parenchima polmonare aerato attraversata dallago ) , la sua morfologia e localizzazione lobare , la presenza di calcificazioni , cavitazioni e centro necrotico , oltrech loccorrenza di complicanze ( pneumotorace e sanguinamento ) non esercitino alcuna a.m. 
anumber of procedures ; bpearsons 2 test for categoric variables ; caverage lesion diameter in two axial planes ; ns , not significant tabella 4 correlazione per variabili , con la diagnosi finale , di risultati corretti ed errati od indeterminati allagobiopsia transtoracica variabile na ( 612 ) diagnosi finale errata o indeterminata n = 102 corretta n = 510 52 ( 50 , 0 ) 458 ( 90 , 2 ) 30 ( 66 , 6 ) 362 ( 87 , 3 ) 118 ( 77 , 6 ) 52 ( 50 , 0 ) 50 ( 9 , 8 ) 15 ( 33 , 3 ) 53 ( 12 , 7 ) 34 ( 22 , 4 ) i valori in parentesi sono riferiti in % . 
agrandezza del campione ; btest 2 di pearson per variabili categoriche ; cconsiderata quale dimensione media tra i due assi ( maggiore e minore ) ortogonali della lesione ; ns , non significativo . 
however , they are also dependent on the severity with which sample adequacy is judged : a sample without neoplastic cells should not be considered negative for malignancy ( consider sampling errors , for example ) unless they provide a precise and specific diagnosis of benignity ( 100% specificity is desirable in benign lesions )  . 
many studies [ 13 , 29 , 32 , 37 , 38 ] have reported substantially lower levels of diagnostic accuracy for benign lung lesions ( range 52%91% ) compared with malignant lesions influenza sui valori di accuratezza diagnostica dellagobiopsia transtoracica tc guidata . discussione attraverso lutilizzo dellagobiospia transtoracica percutanea , ed in particolar modo della fnac , quale iniziale procedura mini - invasiva nella valutazione di natura degli addensamenti polmonari si ottenuta , in questo studio , unaccuratezza diagnostica globale dell84% con valori di accu1153 a.m. 
1a - c relationship between mean lesion size and number of observations for the entire group of lesions ( a ) and in regard to the presence ( b ) or the absence ( c ) of a necrotic centre . 
1a - c correlazione tra diametro medio della lesione e numero di casi per tutte le lesioni ( a ) e suddividendo queste ultime per presenza ( b ) od assenza ( c ) di centro necrotico . 
la sensibilit della metodica per lesioni maligne risultata del 90% ( con valori di specificit del 99% ) , mentre per lesioni benigne la sensibilit risultata del 50% , ma con specificit del 100% . 
questi dati dimostrano come , nellinquadramento diagnostico delle lesioni benigne , la fnac risulti inferiore alla cb [ 20 , 24 ] , ma paiono anche giustificati dalla severit di giudizio di idoneit cui vengono sottoposti i campioni : un prelievo con assenza di cellule neoplastiche non deve essere considerato negativo per patologia tumorale ( si considerino , ad esempio , gli errori di campionamento ) , a meno che sia possibile formulare una precisa e specifica diagnosi di benignit ( sono auspicabili valori di specificit per lesioni benigne pari al 100% )  . 
molteplici studi in letteratura [ 13 , 29 , 32 , 37 , 38 ] riportano valori di accuratezza diagnostica sensibilmente inferiori per lesioni polmonari benigne ( con intervallo compreso tra il 52% ed il 91% ) se paragonate a lesioni maligne ( intervallo compreso tra l86% ed il 100% ) , sia nel prelievo aspirativo sia tranciante ; inoltre , considerando esclusivamente gli addensamenti benigni , la cb presenta valori di accuratezza e sensibilit significativamente maggiori rispetto alla fnac ( accuratezza superiore all80% versus 50%70% ) [ 9 , 2225 ]  . 
i livelli di accuratezza e sensibilit riportati dal nostro studio sono in linea con i riscontri fnac della letteratura , ma non dimensioni lesione ( cm ) lesion size ( cm ) fig . 
 ctest t di student ( per campioni indipendenti e per gruppi ) , p < 0 , 05 considerata significativa : il diametro medio delle lesioni con ( 57 , 7 mm ) e senza ( 34 , 0 mm ) necrosi differisce con significativit statistica . raggiungono i valori riportati dalla cb , elemento comunque non contraddittorio dal momento che solo nel 6 , 4% delle procedure stato utilizzato un ago tranciante ( singolarmente od in associazione con altri aghi )  . la documentazione di cellule sicuramente maligne , nella pressoch totalit dei casi , prova certa della natura maligna dellespanso . 
nella nostra coorte lunico caso classificato come maligno ( neoplasia di origine epiteliale ) e poi risultato benigno ( granulomatosi escavata ) alla diagnosi finale trova esplicazione nel fatto che la lesione benigna ha sviluppato atipie cellulari tali da farla risultare sospetta allindagine citologica per espanso di natura maligna . nonostante gli insuccessi siano sensibilmente minori per le lesioni maligne , tuttavia si evidenziato un 11% di falsi negativi nellambito di tali addensamenti ( integralmente costituiti da prelievi a punteggio 01 )  . 
in aggiunta , la nostra esperienza indica come la sola ispezione ad occhio nudo del campione ottenuto ( in termini di integrit del frustolo bioptico o di cellularit o di carattere ematico del prelievo aspirativo ) inaffidabile nel predirne ladeguatezza [ 30 , 32 , 34 , 36 , 38 ] ed quindi auspicabile la presenza dellanatomopatologo nel corso della seduta bioptica . 
la ripetizione del prelievo dovrebbe essere presa in considerazione ogni qual volta si verifichi discordanza tra risultato bioptico , presentazione clinica e caratteristiche tc ( prima di passare ad accertamenti diagnostici invasivi di ii livello ) [ 13 ]  . lanalisi della nostra coorte ha evidenziato come le uniche variabili in grado di influenzare , in termini statisticamente significativi , laccuratezza diagnostica della metodica siano la diagnosi finale ( benignit versus malignit ) e le dimensioni della lesione ( nodi con diametro medio inferiore ad 1 , 5 cm o masse di dimensioni superiori a 5 cm sono caratterizzati da livelli di minore accuratezza diagnostica )  . 
riferendosi a questultimo aspetto , gli studi presenti in letteratura esprimono giudizi discordanti in merito allinfluenza delle dimensioni della lesione sui livelli di accuratezza dia1155 dimensioni lesione ( cm ) lesion size ( cm ) fig . 
3 relazione esistente tra dimensione della lesione e presenza di necrosi : il grafico dimostra come lincidenza di necrosi si incrementi gradualmente allaumentare delle dimensioni delle lesioni ; la maggior proporzione di necrosi si riscontrata nelle lesioni di 6 cm , ovvero quelle caratterizzate da minor accuratezza diagnostica . ( from 86% to 100% ) , achieved with both fnac and cb . 
accuracy and sensitivity levels found in our study are similar to those previously reported for fnac but fail to reach those reported for cb , a finding that is not contradictory given that only 6.4% of procedures were carried out with a cutting needle ( used alone or in combination with other needles )  . demonstration of definitely malignant cells is proof of the a.m. 
4 il grafico box & whisker dimostra una differenza significativa in termini di dimensioni nel gruppo di lesioni senza ( 3 , 4 cm1 , 8 ) e con necrosi centrale intralesionale ( 5 , 7 cm1 , 8 )  . 
il diametro medio delle lesioni in assenza e presenza di necrosi differisce significativamente ( p < 0 , 001 ) ( ds , deviazione standard ; n , no ; s , si )  . malignant nature of the mass in virtually all cases . 
in our cohort , the only case classified as malignant ( epithelial neoplasm ) at biopsy and found to be benign ( excavated granuloma ) at final diagnosis is explained by the fact that the lesion had developed cellular atypia that made it suspicious for malignancy at cytological assessment . although there were substantially fewer failures in malignant lesions , the false negative rate was 11% in this group ( all for samples with a score of 01 )  . 
in addition , our experience shows that gross inspection of the sample ( in terms of integrity of the biopsy specimen , cellularity or blood contamination of the aspirate ) is unreliable in predicting adequacy [ 30 , 32 , 34 , 36 , 38 ] , making the presence of a pathologist during the biopsy procedure strongly desirable . 
found that diagnostic accuracy declined progressively with decreasing lesion size : from 100% to 93% , 87% , 79% and 67% for lesions > 5 cm , 35 cm , 23 cm , 12 cm and < 1 cm , respectively [ 13 ]  . 
reported accuracy levels of approximately 88% for lesions > 2 cm when the mean number of needle passes was 2.5 , whereas when only a single specimen was obtained , accuracy decreased to 83% [ 29 ]  . the results of our study are similar to those reported by yeow et al . 
 [ 20 ] , who found , with a mean number of passes of three ( without a pathologist present ) , lower levels of diag1156 gnostica [ 13 , 20 , 30 , 36 , 37 ]  . 
tsukada ha riscontrato un graduale e progressivo decremento dei valori di accuratezza diagnostica man mano che le dimensioni delle lesioni si riducevano : dal 100% al 93% , 87% , 79% e 67% per lesioni rispettivamente > 5 cm , tra 3 e 5 cm , tra 2 e 3 cm , tra 1 e 2 cm e < 1 cm [ 13 ]  . 
lucidarme ha riscontrato valori di accuratezza di circa l88% per lesioni > 2 cm con un numero medio di prelievi per biopsia di 2.5 , mentre laccuratezza si riduceva all83% in caso di unico prelievo per seduta bioptica [ 29 ]  . nel nostro studio si sono ottenuti risultati simili a quelli descritti da yeow [ 20 ] che riportava , con una media di 3 prelievi bioptici a seduta ( in assenza di un medico anatomopatologo in sala ) , livelli inferiori di accuratezza diagnostica per lesioni < 1 , 5 cm e > 5 cm ( dell84% e 93% rispettivamente ) quando paragonati a lesioni con diametro compreso tra 1 , 5 e 5 cm ( 96% )  . 
nel nostro lavoro vengono , invece , riportati valori di accuratezza diagnostica globale ( per lesioni maligne e benigne ) del 68% per lesioni < 1 , 5 cm , del 78% per lesioni > 5 , 0 cm e dell87% per le lesioni comprese tra 1 , 5 e 5 , 0 cm . la maggior accuratezza diagnostica riportata da yeow giustificata dal fatto che in tutti i casi stata eseguita una cb con tecnica coassiale ( caratterizzata da livelli di accuratezza diagnostica maggiori rispetto alla fnac ) , mentre nel nostro studio solo il 6% delle manovre stato eseguito con tale procedura , riservando la fnac a tutti gli altri casi . 
in aggiunta , avendo la disponibilit del citopatologo in sala radiologica , risultato sensibilmente minore il numero di prelievi per seduta ( 1 , 3 prelievi versus 3 , 0 )  . 
il numero di prelievi , essendo variabile nei diversi studi , potrebbe costituire un determinante elemento confondente in grado di influenzare laccuratezza diagnostica al pari delle dimensioni della lesione [ 20 , 29 , 37 ]  . 
con una media di 1 , 3 prelievi per procedura , il nostro studio pone come limite dimensionale critico , al di sotto del quale si verifica una sensibile riduzione di accuratezza diagnostica , il valore di 1 , 5 cquesto risultato in linea con le a.m. 
is explained by the fact that they used cb with coaxial technique ( which is more accurate than fnac ) in all cases , whereas we used cb for only 6% of procedures and fnac for the remaining cases . 
the number of needle passes should , however , be kept to a minimum , as this variable is significantly related to higher rates of pneumothorax [ 32 ] ; the presence on site of a cytopathologist during the procedure is instrumental to establishing a correct diagnosis . the substantial reduction in diagnostic accuracy in small lesions could be due to sampling errors resulting from increased technical difficulty in the localisation phase [ 11 ]  . such difficulties are further supported by the higher rate of complications within this class of lesions : yeow et al . 
 [ 32 ] reported a 17 times higher risk of pneumothorax and a six times higher risk of bleeding for lesions smaller than 2 cm . in view of the lower diagnostic accuracy for small lung nodules ( whether sampled by fnac or cb ) and the higher complication rate , fine - needle aspiration should always be preferred to cb for lesions smaller than 1 cm , as suggested by laurent et al . 
when sampling these nodules , in fact , it is impossible to avoid inclusion of portions of healthy aerated lung tissue , as the biopsy core is 1.3cm long ( shortest throw - length setting ) [ 29 , 32 , 37 ]  . 
diffuse bleeding may also occur as a result of the surrounding healthy parenchyma not being able to provide an adequate tamponade effect [ 29 , 32 , 37 ]  . 
finally , in a nonnegligible number of cases , the material recovered proves inadequate due to the abundant presence of blood . despite the fact that throw lengths of 10 mm can be used to avoid bleeding in lesions smaller than 1.5 cm , boiselle et al . reported a diagnostic accuracy of 62% with this approach [ 39 ]  . 
comunque auspicabile conseguire il minimo numero di campionamenti possibili per procedura dal momento che tale variabile significativamente correlata ad una maggior proporzione di pneumotoraci [ 32 ] ; elemento indispensabile , a garanzia dellobiettivo di ottenere una corretta diagnosi , risulta essere la presenza del citopatologo durante la seduta bioptica . la sensibile riduzione di accuratezza diagnostica per lesioni di ridotte dimensioni potrebbe trovare una valida esplicazione in errori di campionamento , dovuti a maggiori difficolt tecniche nella fase di centratura bioptica [ 11 ]  . 
le difficolt procedurali trovano ulteriore conferma nella maggior proporzione di complicanze riscontrabile in questa categoria di lesioni : yeow [ 32 ] riporta , infatti , un rischio di pneumotorace 17 volte maggiore e di sanguinamento 6 volte superiore per lesioni di diametro inferiore ai 2 cin ragione della minor accuratezza diagnostica per i piccoli noduli polmonari ( che siano sottoposti a fnac o a cb ) ed alla pi alta percentuale di complicanze riscontrate , risulta sempre opportuno preferire alla cb , come gi suggerito da laurent e yeow [ 20 , 30 ] , il prelievo aspirativo con ago sottile per le lesioni di dimensione inferiore al centimetro . 
infatti , risulta impossibile evitare , nel campionamento di questi piccoli nodi , porzioni di tessuto aerato sano , dal momento che il frustolo bioptico ha lunghezza pari ad 1 , 3 cm ( limite inferiore della lunghezza dello scatto dellago tranciante ) [ 29 , 32 , 37 ]  . 
pu inoltre verificarsi un sanguinamento diffuso dal momento che il parenchima circostante sano , interessato anchesso dal campionamento , non in grado di fornire un adeguato effetto tampone [ 29 , 32 , 37 ]  . 
nonostante si possano utilizzare lunghezze di scatto pari a 10 mm per evitare il sanguinamento in lesioni inferiori ad 1 , 5 cm , boiselle ha riportato , in tali condizioni , unaccuratezza diagnostica pari al 62% [ 39 ]  . 
questo valore risulta inferiore al 67% da noi ottenuto utilizzando esclusivamente , per tali lesioni , lagoaspirato e con un tasso di sanguinamento perilesionale di minor entit . analizzando il parametro dimensionale , quale variabile determinante laccuratezza diagnostica della procedura , si sono riscontrati decrementi di accuratezza per lesioni con dimensione maggiore ai 5 cquesta evenienza viene compresa se si considera la presenza di necrosi centrale , che risulta di frequente riscontro nelle masse polmonari > 5 cm ( nella nostra casistica percentuale tc di necrosi tumorale per lesioni sino a 5 cm compresa tra lo 0% ed il 15% , per masse 5 cm tra il 12% ed il 41% )  . 
risulta quindi evidente come , nelle grosse masse polmonari , sia necessario disporre di indagini tc acquisite con infusione di mezzo di contrasto per individuare aree lesionali necrotiche al fine di evitarle durante il campionamento . 
inoltre , in assenza di un anatomopatologo in sala , nellevenienza allispezione visiva di frustoli particolarmente fragili e frammentati o di prelievi citologici ottenuti con agoaspirato , particolarmente ematici , si dovrebbero 1157 a.m. 
moreover , when no on - site pathologist is present and the biopsy cores appear particularly fragile and fragmented or the aspirate particularly bloody on gross inspection , further samples should be obtained taking care to direct the needle to different areas of the lesion [ 32 , 40 , 41 ]  . the presence of cavitations within a lung mass does not appear to influence the diagnostic accuracy of either fnac , as demonstrated in our study , or cb , as shown by yeow et al . 
similarly , diagnostic accuracy was not significantly affected by the presence of calcification or a frankly necrotic centre ; by lesion depth ( from the pleural surface ) , morphology or location ; or by the occurrence of complications such as pneumothorax and bleeding . 
no evaluation was made with regard to needle size or the radiologists experience , variables that are ascribed different significance in the various studies [ 20 , 41 ]  . conclusions in conclusion , transthoracic ct - guided needle biopsy of pulmonary lesions is a highly accurate procedure , especially in malignant lesions . 
however , to enhance the likelihood of success and achieve a correct diagnosis , awareness of the variables affecting its effectiveness is crucial : benign lesions , nodules smaller than 1.5 cm and masses larger than 5 cm are associated with substantially lower accuracy rates . 
analogamente , la presenza di calcificazioni o di centro francamente necrotico , od ancora la profondit della lesione ( rispetto al piano pleurico ) o la morfologia o la localizzazione od infine la comparsa di complicanze , quali lo pneumotorace od il sanguinamento , non hanno significativamente alterato i valori di accuratezza diagnostica della procedura . 
non si sono , invece , formulate valutazioni relative al calibro dellago o allesperienza del radiologo prelevatore , parametri che assumono , a seconda dei diversi studi presenti in letteratura , significato diverso [ 20 , 41 ]  . conclusioni in conclusione , lagobiopsia transtoracica tc guidata di espansi polmonari metodica ad elevata accuratezza diagnostica , specie per le lesioni di natura maligna . 
risulta comunque indispensabile , al fine di implementare le probabilit di successo della procedura in termini di raggiungimento della corretta diagnosi , la conoscenza delle variabili in grado di inficiare tale efficacia : le lesioni benigne ed i nodi di dimensioni minori ad 1 , 5 cm o le masse superiori a 5 cm sono correlate a valori di accuratezza diagnostica sensibilmente inferiori . 
krestin2 1dipartimento di radiologia e dipartimento cuore , imaging cardiovascolare non invasivo , azienda ospedaliera di parma , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia , universit degli studi di verona , verona , italy 4dibimel , sezione di scienze radiologiche , universit di palermo , palermo , italy 5unit operativa di riabilitazione cardiovascolare , fondazione don gnocchi onlus , parma , italy correspondence to : f . 
cademartiri , imaging cardiovascolare non invasivo , dipartimento di radiologia , azienda ospedaliero - universitaria di parma , via gramsci 14 , i - 43100 parma , italy , tel . : + 39 - 052 - 1703222 , fax : + 39 - 052 - 1703630 , e - mail : filippocademartiri@hotmail.com received : 23 november 2006 / accepted : 19 march 2007 / published online : 13 december 2007 abstract purpose . 
in the 202 consecutive patients , the prevalence of anatomical variants was : left dominant circulation ( 7% ) , absent left main ( 5% ) , presence of intermediate branch ( 17% ) , aortic origin of conus branch ( 13% ) and circumflex origin of sinus node branch ( 15% )  . 
anatomical variants and anomalies of the coronary arteries are quite common and should be known and recognised promptly by the operators . key words 64 - slice ct coronary anatomy coronary artery variants coronary artery anomalies prevalence riassunto obiettivo . 
nei 202 pazienti consecutivi arruolati per lo studio la prevalenza delle varianti anatomiche risultata : dominanza sinistra ( 7% ) , tronco comune assente ( 5% ) , presenza di ramo intermedio ( 17% ) , origine aortica del ramo del cono ( 13% ) , origine dalla circonflessa dellarteria del nodo del seno ( 15% )  . 
le varianti e le anomalie coronariche sono un reperto molto comune che deve quindi essere riconosciuto agevolmente dalloperatore . parole chiave tc multistrato anatomia coronaria varianti delle arterie coronarie anomalie delle arterie coronarie prevalenza introduction introduzione effectively visualising the coronary arteries is a challenge , not only due to their rapid movement during the cardiac cycle , but also because of their small diameter , their tortuous la visualizzazione delle arterie coronarie rappresenta una sfida non solo per il loro rapido movimento durante il ciclo cardiaco , ma anche per il calibro ridotto , il decorso tortuo1117 f . 
recognising coronary artery anomalies is therefore important for correct diagnosis and treatment of patients , whether or not they are affected by atherosclerosis . the literature contains numerous descriptions of coronary artery anomalies based on conventional coronary angiography ( ca ) but still very few based on msct , and the latter are mostly review articles or case reports [ 35 ]  . the introduction of the technique allows a different anatomical approach that could change the perception of these variants . the aim of this study was to describe the prevalence of coronary artery variants and anomalies in a consecutive population of patients studied with ct coronary angiography ( ctca )  . materials and methods two hundred and two consecutive patients ( 146 men , 56 women , mean age 60 11 years , range 2183 ) with suspected coronary artery disease and already scheduled for conventional ca underwent ctca before ca in the context of a validation study of ctca . 
only patients with a sinus rhythm who had never undergone percutaneous angioplasty or bypass surgery and who were capable of holding their breath for 12 s were included in the study . 
the ethics committee in our department approved the study protocol , and all patients provided informed consent . patient preparation patients with a heart rate ( hr ) greater than 65 beats per minute ( bpm ) were administered 45 munutes before examination , in the absence of contraindications , a single oral dose of 100 mg metoprolol tartrate ( selokeen , astrazeneca pharmaceutics )  . 
apparecchiature di tomografia computerizzata multistrato ( tcms ) allo stato dellarte , ovvero a 64 strati , consentono di collocare la valutazione non invasiva delle arterie coronarie nella routine clinica in virt delle elevate prestazioni ed accuratezza della metodica [ 1 , 2 ]  . le anomalie delle arterie coronariche sono presenti alla nascita ma solo una piccola percentuale di esse si rende manifesta nei primi anni di vita . 
gran parte di esse infatti viene scoperta per caso durante langiografia coronarica o rappresenta addirittura solamente un puro reperto autoptico . ci nonostante alcune di esse possono manifestarsi con sintomi come angina pectoris , infarto miocardico , sincope , aritmie pi o meno severe o addirittura arresto cardiaco configurando il quadro di morte improvvisa . 
il riconoscimento di anomalie coronariche importante quindi per una diagnosi appropriata e per il trattamento del paziente , sia esso affetto o meno da malattia aterosclerotica . nella letteratura esistono delle descrizioni delle anomalie coronariche basate sulla ac mentre ne esistono ancora poche basate sulla tcms , peraltro per lo pi costituite da revisioni della letteratura o descrizione di singoli casi particolarmente significativi [ 35 ]  . 
lintroduzione di questa tecnologia consente un diverso approccio anatomico che pu mutare la percezione di queste varianti . pertanto lo scopo di questo lavoro quello di fornire una prevalenza di varianti ed anomalie coronariche in una popolazione consecutiva di pazienti sottoposti ad angiografia coronarica tc ( ac - tc )  . materiali e metodi duecentodue pazienti consecutivi ( 146 maschi , 56 femmine , et media 6011 anni , range 2183 anni ) con sospetta malattia coronarica e gi indirizzati a coronarografia convenzionale ( ac ) sono stati sottoposti ad angiografia coronarica tc ( ac - tc ) preliminarmente allesecuzione della ac nellambito di studi di validazione della metodica . 
solo i pazienti con ritmo sinusale , mai sottoposti ad angioplastica percutanea o ad intervento chirurgico per il posizionamento di by - pass e capaci di trattenere il respiro per almeno 12 secondi , sono stati inclusi nello studio . 
i pazienti nei quali esistevano delle controindicazioni assolute alla somministrazione endovenosa di mezzo di contrasto iodato ( ad esempio allergia nota , insufficienza renale o disordini tiroidei ) sono stati esclusi dallo studio . 
il comitato etico del nostro dipartimento ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . preparazione del paziente ai pazienti con una frequenza cardiaca ( fc ) superiore a 65 battiti per minuto ( bpm ) stata somministrata , 45 minuti prima della scansione , se non presenti delle controindicazioni , una singola dose orale di 100 mg di metoprololo tartrato ( selokeen , astrazeneca pharmaceutics )  . 
the study protocol involved a preliminary acquisition without intravenous iodinated contrast material to quantify coronary artery plaque . the parameters used for the two scans ( a ) quantification of plaque and ( b ) ctca were : 1 . 
images were reconstructed with the following parameters : effective slice thickness 3 mm , reconstruction increment 1.5 mm , field of view ( fov ) 150180 mm , dedicated convolution kernel for the calcium score . the time windows were positioned at 60% of the rr interval 2 . 
number of slices per rotation 322 , slice thickness 0.6 mm , gantry rotation time 330 ms , table feed 3.84 mm / rotation ( pitch 0.2 ) , 120 kv , 900 mas . 
prospective modulation of the x - ray tube was not used . patients were administered 100 ml of iodinated contrast material ( iomeprol , iomeron 400 , bracco , milan , italy ) with an automatic injector at 5 ml / s ( stellant , medrad , pittsburgh , pa , usa ) connected to a 20 - gauge cannula positioned in an antecubital vethe bolus tracking technique was used to optimise enhancement of the coronary arteries ( care bolus , siemens , forchheim , germany )  . 
angiography - scan data were obtained during a single breath - hold ( 912 s )  . dedicated software ( windose , institute of medical physics , erlangen , germany ) was used to calculate the radiation dose during the angiographic scan ( mean value 15.2 msv for women and 21.4 msv for men )  . 
retrospective reconstructions were performed based on the electrocardiogram ( ecg ) signal to obtain an image quality not affected by motion artefacts in the end - diastolic and end - systolic phases . coronary angiography ( ca ) ca was performed within 2 weeks of the ctca . 
cardiac catheterisation and ca were performed with standard protocols , with spider - view projections , right anterior oblique ( rao ) for the left coronary artery and left anterior oblique ( lao ) for the right coronary artery . 
a single observer unaware of the ctca results identified the coronary segments using a 17 - segment modified american heart association classification . data collection and statistical analysis all examinations judged to be of insufficient quality by two observers were excluded from the sample . 
all examinations were analysed on an off - line dedicated workstation using all the available applications ( viewing , 3d , inspace , circulation ) to achieve an accurate assessment . 
the observers obtained multiplanar reconstructions ( mpr ) , curved multiplanar reconstructions ( cmpr ) , maximum intensity projecta per via orale una dose addizionale di 1 mg di lorazepam ( temesta , wyeth - ayerst )  . protocollo di scansione e ricostruzione delle immagini per lo studio mediante tc stato utilizzato uno scanner a 64 strati ( sensation 64 , siemens , forchheim , germania )  . 
numero di strati per rotazione 322 , tempo di rotazione del gantry 330 ms , avanzamento / rotazione 6 mm ( pitch 0 , 2 ) , voltaggio del tubo radiogeno kv 120 , potenza del tubo radiogeno mas 150 . 
le immagini sono state ricostruite con i seguenti parametri : spessore di strato effettivo 3 mm , incremento di ricostruzione 1 , 5 mm , campo di vista ( fov ) 150180 mm , filtro di convoluzione dedicato per il calcium score . 
numero di strati per rotazione 322 , spessore di strato 0 , 6 mm , tempo di rotazione 330 ms , avanzamento per rotazione 3 , 84 mm ( pitch 0 , 2 ) , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 900 mas , spessore di strato effettivo ricostruito 0 , 60 , 75 mm , incremento di ricostruzione 0 , 4 mm , campo di vista ( fov ) 150180 mm , filtro di convoluzione medium - smooth . 
non stata utilizzata la modulazione prospettica del tubo radiogeno . sono stati somministrati 100 ml di mezzo di contrasto iodato ( iomeprol , iomeron 400 , bracco , milano ) alla velocit di 5 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 20 gauge preventivamente posizionata in una vena antecubitale . 
utilizzando un software dedicato ( windose , istituto di fisica medica , erlangen , germania ) stata calcolata la dose di radiazioni ionizzanti alla quale i pazienti sono stati esposti durante la scansione angiografica ( valore medio 15 , 2 msv per le donne e 21 , 4 msv per gli uomini )  . 
sono state effettuare delle ricostruzioni retrospettive basate sul segnale ecg per ottenere una qualit dellimmagine priva di artefatti da movimento in fase telediastolica e tele - sistolica . angiografia coronarica ( ac ) lac stata eseguita entro 2 settimane dallac - tc . 
la tecnica di cateterizzazione cardiaca e lesecuzione dellangiografia coronarica sono state eseguite seguendo i protocolli standardizzati , ottenendo in particolare le proiezioni spider view , oad per la arteria coronaria sinistra e oas per larteria coronaria destra . 
the same observers also assessed the presence of coronary anomalies on the basis of the type of origin and course , whether they were intrinsic to the coronary itself , or terminal . 
the proximal tract of the rca was the origin of the right conus branch in 59% of cases and the origin of the sinuatrial nodal branch in 64% of cases . 
the dellac - tc , ha identificato i segmenti coronarici utilizzando una classificazione in 17 segmenti modificata rispetto a quella fornita dallamerican heart association . raccolta dati ed analisi statistica due osservatori in consenso hanno escluso dal campione tutti gli esami la cui qualit stata giudicata insufficiente da entrambi i lettori . 
tutti gli esami sono stati analizzati su piattaforma di lavoro dedicata off - line utilizzando tutte le applicazioni disponibili ( viewing , 3d , inspace , circulation ) per raggiungere una valutazione accurata . 
gli stessi osservatori hanno infine valutato in consenso anche la presenza di anomalie coronariche sulla base della tipologia : di origine e decorso , intrinseche alla coronaria stessa , di terminazione . 
i dati sono stati espressi come prevalenze in numero assoluto e percentuale sul totale dei reperti descritti . risultati gli esami sono risultati tutti di qualit diagnostica e adatti alla valutazione . table 1 main anatomical variants of the coronary tree tabella 1 principali varianti anatomiche dellalbero coronarico main anatomical variants type principali varianti anatomiche tipo coronary dominance origin of the conus branch artery origin of the sinus node artery pda variants lm lenght intermediate branch number of diagonal branches number of marginal branches right , left , mixed rca ; rca ostium ; aorta rca ; cx ; both pathways are present early pda ; double 12 cm ; < 1cm ; > 2cm single or double 12 , > 2 12 , > 2 dominanza coronarica origine arteria del cono della polmonare origine arteria del nodo del seno varianti adp lunghezza del tcs presenza di un ramo intermedio numero di rami diagonali numero di rami marginali destra ; sinistra ; bilanciata acd ; ostio acd ; aorta acd ; acx ; entrambe le vie presenti emergenza precoce ; doppia adp 12 cm ; < 1 cm ; > 2 cm singolo o doppio 12 , > 2 12 , > 2 rca , right coronary artery ; cx , circumflex artery ; lm , left main ; pda , posterior descending artery acd , arteria coronarica destra ; acx , arteria circonflessa ; tcs , tronco comune sinistro ; adp , arteria discendente posteriore 1120 f . 
i rami settali sono stati visualizzati nell89% dei pazienti . analisi delle anomalie coronariche : le anomalie dellalbero coronarico riscontrate nella nostra popolazione comprendono 51 casi pari al 25% dei pazienti osservati . alcuni pazienti presentano multiple anomalie cos ripartite e riassunte in tabella 4 : 1 . 
anomalie di terminazione delle coronarie con decorso anomalo in 1 paziente ( 0 , 5% )  . discussione la tcms in grado di visualizzare con efficacia lanatomia complessa e variabile delle arterie coronarie sfruttando le tecfig . 
termination anomalies of the coronary arteries with an anomalous course were identified in one patient ( 0.5% ) discussion msct is able to effectively visualise the complex and variable anatomy of the coronary arteries by exploiting postprocessing techniques , thus providing valuable support to interventional cardiologists and heart surgeons [ 615 ]  . 
on the basis of the most recent published data obtained with ca , normal is defined as any morphological characteristic of the coronary circulation observed in more than 1% of a nonselected sample . a normal variant , therefore , is a characteristic observed in more than 1% of the same sample , whereas an anomaly is a condition observed in less than 1% [ 20 ]  . coronary dominance indicates which system of coronary arteries supplies the inferolateral aspect of the left ventricle [ 21 ]  . 
in 80%90% of the population the posterior descending artery ( pda ) is a branch of the rca and runs from the base of the heart to the apex in a mirror image of the lad . 
in right coronary dominance the rca gives rise to a right posterolateral ( rpl ) branch , which crosses the posterior interventricular sulcus and continues on the left side to supply the dorsal aspect of the left ventricle . 
esistono in letteratura numerosi criteri per classificare ed indicare le anomalie coronariche ; basandoci sui dati pi recenti ritrovati nella letteratura , peraltro ottenuti da casistiche di angiografia coronarica ; viene definita normale qualsiasi caratteristica morfologica del circolo coronarico osservata in pi dell1% in un campione non selezionato ; variante normale , una caratteristica osservata in pi dell1% dello stesso campione ; anomalia una condizione osservata in meno dell1% [ 20 ]  . la dominanza coronarica indica quale sistema di vasi coronarici vicaria il flusso sanguigno verso la parete infero - laterale del ventricolo sinistro [ 21 ]  . 
quando la dominanza coronarica del sistema destro la acd d origine un ramo postero - laterale destro ( pld ) , che attraversa il solco interventricolare posteriore e continua sul lato sinistro per la vascolarizzazione della parete dorsale del ventricolo sinistro . il ramo pld pu diventare di importanza notevole quando la acx occlusa , poich pu essere in grado di sostenere la vascolarizzazione della parete postero - inferiore del ventricolo sinistro . 
dai dati ottenuti nella nostra analisi emerge una stretta concordanza con quanto riportato in letteratura , ovvero una prevalenza nella dominanza destra . il primo ramo della acd larteria del cono che decorre sulla superficie antero - laterale del tratto di efflusso del ventricolo destro . 
conventional angiogram ( a ) , volume rendering ( vr ) ( b ) and maximum intensity projection ( mip ) ( c ) images of a right coronary artery ( rca ) arising from the left sinus of valsalva with an interarterial course . 
conventional angiogram ( d ) , vr ( e ) and multiplanar reconstruction ( mpr ) ( f ) images of a left coronary artery arising from the rca with a septal course . 
acc ( g ) , immagini vr ( h ) e cmpr ( i ) di acx con origine dal seno di valsalva destro e decorso retroaortico , sottoposta a stent . nance is mixed with an intermediate vascularisation pattern . data from our analysis show a strong agreement with the data reported in the literature , i.e. 
in una piccola percentuale di casi lacd pu dare origine anche ad un ampio ramo lungo il margine acuto del cuore fino a continuarsi con ladp ( emergenza precoce delladp )  . 
conventional angiogram ( a ) , volume rendering ( vr ) ( b ) and maximum intensity projection ( mip ) images ( c ) displaying an aneurysm of the circumflex artery . 
myocardial bridging of mid - left anterior descending artery displayed by conventional angiogram during systole ( d ) , vr ( e ) and mpr cross - section images ( f )  . 
sometimes , however , the rca can trifurcate at the crux , giving rise to two branches ( double pda ) for the supply of the base of the heart and an rpl branch for the supply of the dorsal aspect of the left ventricle . the length of the main lca is usually 12 cm , whereas lower values are very common and higher values more rare [ 22 ]  . 
the anomalies that prove to be haemodynamically significant , however , can lead to angina pectoris , syncope , arrhythmia , myocardial infarct or sudden death , as well as promote the onset and progression of coronary atherosclerosis or prove responsible for complications and technical difficulties during angioplasty and heart surgery . 
this anomaly could create problems during heart surgery , since the surgeon unaware of its anomalous course could mistakenly cut it . in addition , native coronary arteries are normally positioned at the origin of the aortic arch with an orientation of 120 and 150 , respectively . 
the cases we observed included 1128 zazione della base del cuore , e ad un ramo pld , per la vascolarizzazione della parete dorsale del ventricolo sinistro . la lunghezza del tcs comunemente di circa 12 cm , anche se possono essere riscontrati valori inferiori ( molto frequenti ) o superiori ( pi rari ) [ 22 ]  . 
le anomalie che risultano invece emodinamicamente significative possono indurre angina pectoris , sincope , aritmia , infarto miocardico , morte improvvisa , favorire linsorgenza e la progressione della malattia aterosclerotica coronarica o rendersi responsabili di complicanze e difficolt tecniche durante angioplastica ed interventi di cardiochirurgia . 
il chirurgo , infatti , potrebbe erroneamente reciderla non conoscendone il decorso anomalo . normalmente inoltre le arterie coronarie native sono posizionate allorigine dellarco aortico con un orientamento di 120 e 150 gradi rispettivamente . 
in caso di riposizionamento chirurgico della valvola o di una sua sostituzione importante conoscere questa condizione . alcune anomalie vengono definite anche come maligne proprio per il loro potenziale patologico e sulla base della loro rilevanza clinica ( benigne ; rilevanti correlate ad ischemia miocardia ; severe associate a morte improvvisa ; critiche associate a malattia coronarica ) , facilitandone cos la gestione ed il follow - up clinico [ 25 ]  . 
a questa classificazione si pu sovrapporre una classificazione anatomica che divide le anomalie coronariche sulla base dellorigine ( assenza del tronco comune sinistro , figura 6 , coronaria con origine dallopposto seno coronarico , figura 7 ) , del decorso ( interarterioso , settale e retroaortico , figura 7 ) , dellanatomia intrinseca ( aneurismi , ponti miocardici , figura 8 ) , e della terminazione ( fistole , figura 9 ) [ 4 , 20 ]  . 
tra i casi osservati emergono alcune di queste anomalie : la fistola coronarica una anomalia coronarica in grado di determinare o predisporre ad un evento ischemico miocardico ed a scompenso cardiaco congestizio , in quanto , drenando nelle sezioni cardiache di destra , pu determinare uno shunt sinistrof . 
coronary fistula is a anomaly capable of causing or creating the predisposition for a myocardial ischaemic event and congestive heart failure in that drainage in the right cardiac sections can lead to leftright shunt with volume overload . 
this anomaly in adults is associated with myocardial ischaemia , a higher risk of coronary disease and volume overload . coronary anomalies are a relatively frequent finding in the context of noninvasive coronary diagnostic imaging . knowledge of the characteristics and consequences of different types of anomalies allows the radiologists to judge the finding appropriately . 
nonetheless , it needs to be emphasised that the performance of ctca for suspected coronary anomaly or to exclude its presence should be carefully considered together with the cardiologist to avoid exposing a young patient to an excessive dose of ionising radiation . to date , conventional ca has been the technique of choice for the diagnosis of coronary artery anomalies . 
the diagnosis of coronary artery anomalies is very often established on the basis of the impossibility of finding the coronaries in their normal anatomical position , and therefore of characterising their ostium . in a few short years msct has modified the entire perception of coronary diagnosis by demonstrating the feasibility of a noninvasive approach . 
the complex and tortuous coronary anatomy can be easily depicted with msct . in our case series , we wanted to emphasise the importance of coronary variants and anomalies by demonstrating their prevalence in a broad population of consecutive patients treated at our tertiary referral centre . 
in our experience , the prevalence of coronary artery anomalies was 25% of cases ( 51 / 202 ) , a much higher value than reported in the literature . this can , however , be explained by the fact that the centre where the examinations were performed is a tertiary referral centre for patients with cardiovascular disease . 
in addition , it should be borne in mind that the study population was not made up of a single ethnic group but was , rather , heterogeneous , as it included patients originating from other continents and with a different and currently unknown prevalence of coronary artery anomalies . most of the coronary artery variants encountered had a minimal clinical risk , such as myocardial bridging , which was present in 12.9% of cases , a figure higher than in condestro con sovraccarico di volume . 
nelladulto questa anomalia si pu associare ad ischemia miocardica , ad un pi elevato rischio di malattia coronarica e ad un sovraccarico cardiaco . le anomalie coronariche sono un reperto relativamente frequente nel contesto dellimaging diagnostico non invasivo coronarico . 
langiografia coronarica con tcms consente grazie alle tecniche di post - processing ( mpr , cmpr , mip , vr ) una pi chiara visualizzazione delle anomalie coronariche rispetto allac . 
la ac - tcms stata recentemente considerata come test appropriato per la valutazione di una sospetta anomalia coronarica , al pari della angiografia coronarica mediante risonanza magnetica [ 2 ]  . 
occorre , tuttavia , puntualizzare che lindicazione allesecuzione di una ac - tcms per sospetta anomalia coronarica o per escluderne la presenza deve essere ben ponderata in cooperazione con il cardiologo , al fine di evitare ad un paziente di giovane et uneccessiva esposizione a radiazioni ionizzanti . sino ad oggi , la coronarografia convenzionale ha rappresentato la tecnica di riferimento per la diagnosi delle anomalie coronariche . 
la diagnosi di ac stabilita , molto spesso , sulla base dellimpossibilit di trovare la coronaria nella normale sede anatomica e , quindi , di cateterizzarne lostio . la tomografia computerizzata multistrato ( tcms ) ha modificato in pochi anni lintera percezione della diagnostica coronarica , portando in primo piano la fattibilit di un approccio non invasivo . 
questa metodica , infatti , offre uneccellente risoluzione spaziale con la possibilit di effettuare mpr ( ricostruzioni multiplanari ) , mip ( maximum intensity projections ) e vr ( volume rendering )  . 
la complessa e tortuosa anatomia coronarica pu essere agevolmente dimostrata mediante la tcms . nella casistica presentata abbiamo voluto sottolineare limportanza delle varianti e delle anomalie coronariche dimostrandone la prevalenza in una ampia popolazione di pazienti consecutivi afferenti presso un centro di iii livello . nella nostra esperienza , la prevalenza delle anomalie coronariche del 25% dei casi ( 51 / 202 ) , valore molto superiore a quanto osservato in letteratura , ma spiegabile a causa del fatto che il centro dove sono stati effettuati gli esami rappresenta centro di iii livello , di riferimento per patologie cardiovascolari . 
va tenuto conto del fatto , poi , che la popolazione di studio non rappresenta un solo gruppo etnico ma abbastanza eterogenea , poich coinvolge pazienti originanti da altri continenti e con prevalenze di anomalie coronariche quindi differenti , e attualmente non nota . delle varie varianti la maggioranza hanno scarsa rilevanza clinica , come ad esempio i ponti miocardici , la cui prevalenza risulta essere del 12 , 9% , dato anchesso superiore a 1129 f . 
in contrast , the finding of an anomalous origin or course can be clinically relevant , such as the anomalous origin of the coronary ostium from the opposite coronary sinus ( which manifests as origin in the main lca or of divided origin )  . 
in these cases , the potential compression of a single coronary vessel if it passes between the aorta and the pulmonary artery can cause ischaemia , myocardial infarct and sudden death . quanto riscontrato nelle casistiche angiografiche e pi vicino alle prevalenze evidenziate in studi autoptici [ 27 ] , mentre pu avere rilevanza clnica il reperto di anomalie di origine e decorso , quali ad esempio lanomala origine dellostio coronarico dallopposto seno coronarico ( che si estrinseca come origine in tronco comune oppure origine divisa )  . 
in questi casi la potenziale compressione di un singolo vaso coronarico se passa tra aorta ed arteria polmonare , pu provocare episodi ischemici , infarto miocardico e morte improvvisa . conclusions the anatomical complexity and variability of the coronary circulation benefits from the flexibility of the various postprocessing techniques introduced by ctca and implemented by the use of a 64 - slice scanner with isotropic voxel . 
radiologist training needs to focus on both anatomical and technical features to satisfy the criteria of professional competence and expertise required for the study of such a highly specialised area of diagnostic imaging . ctca is currently capable of providing highly accurate anatomical imaging of the cardiac vessels . 
both the arterial and the venous vessels can be visualised , although with slightly different protocols with regard to the timing of contrast administration . among all the applications requiring knowledge of the anatomy of the cardiac vessels , ctca constitutes the noninvasive diagnostic technique capable of depicting the highest number of coronary segments , particularly the distal segments . 
therefore , in patients affected by coronary artery disease , it is reasonable to expect that ctca , due to its intrinsically fast execution , noninvasiveness and low cost , will become the ideal instrument for assessing patients with a low risk of coronary artery disease and for the follow - up of percutaneous and / or surgical procedures in the coronary vascular area . conclusioni la complessit e la variabilit anatomica del circolo coronarico si giova della flessibilit delle varie metodiche di postprocessing introdotte dalla ac - tcms ed implementate dalluso di scanner a 64 strati con voxel isotropico . 
il training del medico radiologo deve necessariamente focalizzarsi su entrambi gli aspetti , anatomico e tecnico , per soddisfare quei criteri di competenza professionale ed expertise necessari per lapproccio ad un area di imaging altamente specializzata . attualmente la coronarografia tc in grado di fornire un imaging anatomico dei vasi cardiaci con elevata accuratezza . 
sia il comparto arterioso che quello venoso possono essere dimostrati , anche se con protocolli lievemente differenti legati al timing del mdc . in tutte quelle applicazioni nelle quali la conoscenza dellanatomia dei vasi del cuore importante , la coronarografia tc costituisce ad oggi la metodica diagnostica non invasiva in grado di visualizzare il maggior numero di segmenti coronarici ed in particolare anche quelli distali . 
i - 00168 rome , italy 2deptartment of radiology , neuroradiology section , ucsf university of california san francisco , san francisco , ca , usa correspondence to : a . 
by providing quantitative measurements of cerebral blood flow ( cbf ) and cerebral blood volume ( cbv ) , dynamic perfusion computed tomography ( p - ct ) allows visualisation of cerebral autoregulation mechanisms and represents a fast , available and reliable imaging option for assessing cerebral perfusion . 
thanks to its feasibility in emergency settings , p - ct is considered most useful , in combination with ct angiography , in acute ischaemic patients , as it is able to provide a fast and noninvasive assessment of cerebral perfusion impairment . 
in addition , p - ct can play a diagnostic role in other types of cerebrovascular disease to assess functional reserve , and in intracranial neoplasms , where it has a role in diagnosis , grading , biopsy guidance , and follow - up during treatment . 
this article illustrates the principles , technique and clinical applications of p - ct cerebral perfusion studies . key words brain ischemia brain neoplasms brain injury hemodynamics perfusion ct riassunto lo studio dellemodinamica cerebrale , ottenuto con le metodiche di imaging , con le sue varie ed attuali applicazioni , genera interesse crescente . 
la tc perfusione dinamica ( p - tc ) permette una valutazione quantitativa del flusso cerebrale ematico ( cbf ) e del volume cerebrale ematico ( cbv ) , offrendo cos una visualizzazione diretta dei meccanismi di autoregolazione cerebrale , e si pone come una valida alternativa ad altre modalit di misurazione della perfusione cerebrale , rispetto alle quali ha il maggior vantaggio di essere una tecnica prontamente disponibile ed accessibile , in condizioni di emergenza , nella maggior parte dei centri medici . 
per tale ragione la p - tc utile soprattutto nellischemia cerebrale acuta , condizione in cui , associata allangio - tc , offre in maniera rapida e non - invasiva , la valutazione eziologica dellipoperfusione , nonch delle sue ripercussioni emodinamiche e fisiopatologiche sul parenchima cerebrale . 
inoltre la p - tc trova utile impiego in pazienti con altre patologie cerebro - vascolari e per la diagnosi , il grading , la guida alle procedure bioptiche , ed il controllo durante la terapia , dei tumori intra - cranici . 
questo articolo si propone di riassumere i principi , la tecnica e le principali applicazioni cliniche degli studi di perfusione cerebrale basati sulla metodica tc . parole chiave ischemia cerebrale neoplasie cerebrali trauma cranico perfusione tc introduction introduzione rapid technological advances in functional imaging techniques have extended the scope of radiology , and in particular of neuroradiology , beyond the boundaries of morphological imaging . 
perfusion studies can now be carried out with magnetic resonance imaging ( mri ) and computed tomography ( ct ) as well as with the gold standard modalities used until now , such as positron emission tomography ( pet ) , single - photon emission tomography ( spect ) il rapido progresso tecnologico applicato alle tecniche di imaging funzionale ha spinto la radiologia in generale , e la neuroradiologia in particolare , oltre i confini della morfologia ; in questo contesto genera crescente interesse la valutazione a scopo diagnostico dellemodinamica cerebrale ( perfusione cerebrale )  . 
gli studi di perfusione ottenuti con rm e tc si sono affiancati alle metodiche fino ad ora impiegate e considerate gold standard , quali la tomografia ad emissione di positroni ( pet ) , la tomografia ad emissione di singolo fotone ( spect ) e la xenon - tc , con 1225 a . 
this is because the introduction of thrombolytic therapy for the treatment of stroke has highlighted the need for a fast and readily available technique capable of identifying the perfusion defect and evaluating its extent and severity [ 2 , 3 ]  . 
 in patients with acute stroke undergoing emergency evaluation , dynamic perfusion ct ( p - ct ) has been proposed as a particularly useful technique after unenhanced brain ct ( which rules out intracranial haemorrhage ) on account of its ease of use , reproducibility of quantitative measurements , ready availability , limited cost and tolerability [ 3 , 4 ]  . 
moreover , the use of p - ct may be extended to the evaluation of the cerebrovascular reserve in patients with haemodynamically significant stenoses of the intraor extracranial arteries even with acetazolamide challenge in potential candidates for temporary or permanent occlusion of the internal carotid artery ( balloon occlusion test ) [ 5 ] , or in patients with subarachnoid haemorrhage at risk of vasospasm [ 6 ]  . 
in addition to acute and chronic cerebrovascular disease , a further application of p - ct is the measurement of cerebral blood volume ( cbv ) and microvascular permeability ( ps ) in brain tumours [ 7 ]  . general technique p - ct derives information on brain haemodynamics by analysing the first passage through the cerebral vessels of an intravenous contrast bolus . 
because there is a direct linear relation between the concentration of contrast material and density , passage of contrast bolus results in an increase in density of the areas being examined that is proportional to the amount of contrast material present in the blood vessels . the blood - brain barrier ( bbb ) prevents the contrast material from spreading into the interstitium , so that under normal conditions the increase in density is only transient , occurring during the first intravascular passage of the bolus . 
p - ct is based on the physical - mathematical tracer kinetic model [ 8 ] , which assumes that the contrast bolus is instantaneous , is introduced into a single vessel , passes through a capillary network , remains totally intravascular and flows out through a single venous conduit . p - ct can be performed on any spiral ct scanner capable of cine mode scans , with the aid of an automatic injector . the anatomical coverage of p - ct along the craniocaudal axis is limited , as the scan is obtained without table motion at 510 mm for single - detector devices , at 20 mm for multidetector devices ( 232 ) and at 40 mm for the recent 64 - detector - row scanners . 
for this reason , the anatomical level to be studied is selected , generally on the scout view or initial morphological scan , and the perfusion study performed at that location using a cine scan without table motion . 
one possible study protocol , applicable to both singleand multislice scanners ( 232 slices ) involves 1 rotation / s for 50 s , 1226 relativi vantaggi e limiti [ 1 ]  . 
infatti lintroduzione della terapia trombolitica nel trattamento dellictus ischemico acuto ha reso evidente il bisogno di una tecnica rapida e prontamente disponibile per lidentificazione del deficit perfusionale e la valutazione della sua estensione e della sua entit [ 2 , 3 ]  . nei pazienti con ictus , in condizioni di emergenza , dopo la tc cerebrale di base senza mdc ( che esclude lemorragia intra - cranica ) la tc perfusione dinamica ( p - tc ) , per semplicit e rapidit di esecuzione , riproducibilit di misurazioni quantitative , disponibilit sul territorio , costi contenuti e tollerabilit da parte dei pazienti , si propone come metodica di particolare interesse ed utilit [ 3 , 4 ]  . 
la p - tc pu essere effettuata velocemente con qualsiasi apparecchiatura spirale , e le mappe di perfusione possono essere ottenute in breve tempo mediante una workstation dotata di apposito software . 
limpiego della p - tc pu inoltre essere esteso alla valutazione della riserva cerebro - vascolare in pazienti con stenosi arteriose emodinamicamente significative intrao extra - craniche anche con stress - test allacetazolamide in potenziali candidati ad occlusione temporanea o definitiva dellarteria carotide interna ( balloon occlusion test ) [ 5 ] , o in pazienti con emorragia sub - aracnoidea , a rischio di vasospasmo [ 6 ]  . 
poich esiste una relazione proporzionale lineare diretta tra concentrazione del mdc e densit , il passaggio del bolo di mdc induce un aumento della densit nelle aree esaminate , proporzionale alla quantit di mdc presente nei vasi . 
la presenza della barriera emato - encefalica ( bee ) impedisce al mdc di diffondersi dai vasi allinterstizio , cosicch , in condizioni normali , laumento di densit solo transitorio , durante il suo primo passaggio intra - vascolare . 
la p - tc basata sul modello fisico - matematico del tracciante cinetico ( kinetic tracer model ) [ 8 ] , il quale assume che il bolo di mdc sia pressoch istantaneo , sia immesso in un vaso unico , passi attraverso una rete capillare , rimanga totalmente intra - vascolare , e defluisca da un singolo collettore venoso . la p - tc pu essere effettuata su qualsiasi apparecchiatura tc con tecnologia spirale che sia in grado di effettuare scansioni in modalit cine , con lausilio di un iniettore automatico . 
la copertura anatomica della p - tc lungo lasse cranio - caudale limitata , poich la scansione si effettua a tavolo fermo , a 510 mm per le apparecchiature spirali a strato singolo , a 20 mm per le apparecchiature tc multia . 
the short scan delay is aimed at the acquisition of a first baseline scan before arrival of bolus and is applied independent of the patients cardiocirculatory condition or type of ct device used . 
for a four - detector - row scanner but also possible with other multislice devices allows the effective radiation dose to be contained below that calculated for a conventional brain ct study [ 10 , 11 ]  . 
lower milliampere settings result in a reduced signal - to - noise ratio ( snr ) and poorer densitometric resolution , with consequently less precision of the parametric measurements ( expressed by increased standard deviation values ) ; nevertheless , it represents a reasonable compromise between radiation - dose containment and diagnostic quality of the examination . 
use of the automatic injector and , if a dual syringe injector is available , of a saline flush after the contrast bolus allows administration of a fast and compact bolus [ 11 ]  . 
the images , generally acquired with 5 - mm thickness to avoid beam - hardening artefacts , are reconstructed with a thicknesses of 10 mm to increase the snr , and at 0.5 - s intervals to increase temporal resolution . data acquired during the cine scan are then analysed on a workstation running dedicated postprocessing software that generates and analyses the time - density curves . 
a region of interest ( roi ) is placed on an artery in the images to view the time - density curve , which reflects the compactness of the bolus . 
it is important to note that , although ideally one might expect the arterial curve to fall back to baseline density levels after the first pass of the bolus , in practice , even when the bolus is sufficiently compact and the bbb intact , the curve tends to remain on a plateau varying height above baseline ( usually 10%30% of the peak )  . 
the maximum slope model approximates the cerebral blood flow ( cbf ) value from the slope of the time - density curve , calcustrato , dotate di multiple file di detettori ( da 2 a 32 ) , a 40 mm per le recenti tc multidetettore a 64 strati . 
per tale ragione si seleziona il livello anatomico da studiare , generalmente sulla scout view o su una scansione morfologica iniziale , ed al livello selezionato si esegue lo studio di perfusione , che consiste in una scansione cine , a tavolo fermo . 
un possibile modello di protocollo di studio , applicabile con apparecchiature tc a strato singolo o multiplo ( 232 strati ) , prevede 1 rotazione / s per 50 s , con 57 secondi di ritardo rispetto alliniezione attraverso una cannula 1820 g , in una vena antecubitale , di 4050 ml di mdc iodato non ionico ( 300370 mg% ) a 45 ml / s [ 9 ]  . 
il breve ritardo tra liniezione del mezzo di contrasto e linizio della scansione finalizzato ad ottenere lacquisizione di una linea di base , prima dellarrivo del bolo , ed applicabile indipendentemente dalla condizione cardio - circolatoria del paziente e dal tipo di apparecchiatura tc utilizzata . 
 [ 10 , 11 ] per una apparecchiatura tc multistrato con quattro file di detettori , ma applicabile anche ad altri tipi di tc multistrato , permette di contenere la dose effettiva di radiazioni al di sotto di quella calcolata per un esame tc del cranio convenzionale . 
la limitazione dellamperaggio causa una diminuzione del rapporto segnale / rumore ed una ridotta capacit di risoluzione densitometrica , cui consegue una ridotta precisione delle misurazioni parametriche ( espressa dagli aumentati valori di deviazione standard ) , ma rappresenta un ragionevole compromesso tra contenimento della dose di radiazioni e qualit diagnostica dellesame . 
luso delliniettore automatico e , se si dispone di un iniettore a doppia siringa , di un bolo di soluzione fisiologica a seguire il mdc , permettono di somministrare un bolo rapido e compatto [ 11 ]  . 
le immagini , generalmente acquisite con spessori di 5 mm , per evitare artefatti da indurimento del fascio , vengono ricostruite a spessori di 10 mm , per aumentare il rapporto segnale / rumore , e a 0 , 5 s di intervallo , per incrementarne la risoluzione temporale . i dati acquisiti durante la scansione cine sono poi analizzati ad una workstation dotata di apposito software che produce ed analizza le curve tempo / densit . 
la compattezza del bolo di mezzo di contrasto determina la morfologia della curva , con ascesa ripida e discesa compresa nei 50 s di scansione . lates cbv as the area under the curve , and from these two parameters derives mean transit time ( mtt ) by solving the central volume equation . 
il modello maximum slope approssima il valore del cbf dalla pendenza ( slope ) della curva densit / tempo , calcola il cbv come larea sottesa alla stessa curva , e da questi due parametri deriva il mtt risolvendo lequazione del volume centrale ; questo modello non richiede la selezione di un arterial input function ( aif ) , ma necessita di velocit di iniezione del mdc molto alte ( > 6 ml / s ) , e fornisce solo misurazioni relative non quantitative [ 12 , 13 ] ; il modello di deconvoluzione si basa su un complesso processo matematico che richiede la scelta di un aif , ovvero di una curva densit / tempo di unarteria , con cui confrontare la curva ottenuta in corrifig . 
a maximum - slope model derives cerebral blood volume ( cbv ) values by calculating the area under the curve , cerebral blood flow ( cbf ) as the slope of the curve and mean transit time ( mtt ) by solving the central volume equation . 
again , cbv corresponds to the area under the curve , mtt to full width at half maximum ( fwhm ) and cbf is derived from the central volume equation . 
a il modello del maximum slope calcola il cbv integrando larea sotto la curva densit / tempo , il cbf secondo la tangente alla porzione ascendente della curva , e deriva il calcolo del mtt dallequazione del volume centrale . 
b il modello di deconvolution , tramite un arterial input function , trasforma la curva densit / tempo in una curva di funzione tissutale , in cui lintegrale dellarea sotto la curva esprime il cbv , il tempo alla met dellaltezza massima ( full width at half maximum fwhm ) rappresenta il mtt ed il cbf derivato dallequazione del volume centrale . 
the deconvolution method relies on a complex mathematical process that requires the use of an aif that is , the time - density curve of an artery with which to compare the curve obtained on the parenchymal pixels so as to correct for the effects of bolus dispersion and thus better reflect the postulates of the tracer kinetic model , which assumes a virtually instantaneous bolus input [ 14 ]  . 
the deconvolution model allows one to reduce the contrast injection rate ( 35 ml / s ) and provides quantitative measurements [ 1517 ] that have been validated by comparison with pet [ 18 ] , spect [ 19 ] and xe - ct [ 20 ]  . although some commercial software packages can automatically select the best aif , aif choice is one of the most controversial aspects of p - ct . 
partial - volume artefacts are practically unavoidable , as the imaging section has a thickness of 10 mm and the artery to be selected generally has a calibre of 24 mthe problem can be partially avoided by choosing an artery that runs perpendicular to the section for example , segment a2 of the anterior cerebral artery so that the roi is placed on a pixel corresponding to a voxel almost completely taken up by the vessel . 
more complex , in the case of cerebral ischaemia , is the problem of selecting an intracranial vessel that is ipsilateral or contralateral to the lesion ( generally segment m2 of the middle cerebral artery ) , or a vessel with proximal stenosis , generally at an extracranial location . 
although there is no consensus [ 21 , 22 ] and studies are underway , our advice is to choose the aif from a healthy vessel , often the anterior cerebral artery , and then compare the results with those obtained with an aif selected on the abnormal side . 
 the software then requires selection of a venous roi , which provides a reference measurement of blood density , considered free of partial - volume artefacts , such as the posterior descending portion of the superior sagittal sinus . 
this curve is used to derive mtt , identified by the width of the curve at spondenza dei pixel parenchimali , per correggere matematicamente gli effetti della dispersione del bolo e riavvicinarsi cos ai postulati teorici del kinetic tracer model , che , come detto , presuppone unimmissione pressoch istantanea del bolo [ 14 ]  . 
il modello di deconvoluzione permette di ridurre le velocit di somministrazione del bolo di mdc ( 35 ml / s ) e fornisce misurazioni quantitative [ 1517 ] , validate in studi di confronto con pet [ 18 ] , spect [ 19 ] e xetc [ 20 ]  . 
gli artefatti da volume parziale sono praticamente inevitabili , infatti , la sezione su cui si lavora ha uno spessore di 10 mm e larteria da selezionare ha generalmente un calibro di 24 mm ; per ovviare parzialmente a tale problema , si pu selezionare unarteria con decorso perpendicolare alla sezione , come nel caso del tratto a2 dellarteria cerebrale anteriore , in modo da posizionare la nostra roi su un pixel corrispondente ad un voxel quasi interamente occupato dal vaso . 
sebbene non esista definitivo consenso [ 21 , 22 ] , e siano ancora in corso studi al riguardo , il nostro consiglio di scegliere laif da un vaso ritenuto sano , spesso larteria cerebrale anteriore , e poi confrontare i risultati con quelli ottenuti con unaif scelta sul lato anormale . il software richiede poi la selezione di una roi venosa , che serve come misurazione di riferimento della densit del sangue , e viene considerata come esente da artefatti di volume parziale , come il caso del seno sagittale superiore nella sua porzione posteriore discendente . 
i parametri perfusionali sono il volume ematico cerebrale ( cerebral blood volume o cbv ) , il tempo medio di transito ( mean transit time o mtt ) ed il flusso ematico cerebrale ( cerebral blood flow o cbf ) ; alcuni software , inoltre , calcolano il tempo di picco ( time to peak o ttp )  . 
in this patient with severe stenosis of the proximal m1 segment of the right main carotid artery ( mca ) , mtt and cbf maps derived from an arterial input function ( aif ) on the anterior carotid artery ( aca ) ( healthy side ) show abnormal measurements in the right mca territory ( left column ) , whereas mtt and cbf measurements derived from an aif distal to the stenosis appear no longer abnormal ( right column )  . 
in questo paziente con stenosi serrata della porzione prossimale del tratto m1 dellacm di destra , la scelta dellaif sullaca ( lato sano ) produce mappe colore di mtt e cbf marcatamente alterate nel territorio di distribuzione dellacm destra ( colonna sinistra ) , mentre le mappe di mtt e cbf derivate da unaif sullacm destra , a valle della stenosi , appaiono sostanzialmente simmetriche ( colonna destra )  . 
5 software analysis of the arterial ( red ) and venous ( blue ) time - density curves generates the pixel - based parametric maps for mean transit time ( mtt ) , cerebral blood volume ( cbv ) and cerebral blood flow ( cbf )  . 
5 lanalisi matematica operata dal software sulla base della curva arteriosa ( in rosso ) e della curva venosa ( in blu ) genera le mappe parametriche con codice colore pixel per pixel per il mtt , il cbv ed il cbf . 
come accennato sopra , il pixel venoso , scelto da una struttura vascolare ampia , considerato essere esente da volume parziale , e quindi si assume la sua densit come unit di riferimento per il sangue ( 100 ml sangue / 100 g di tessuto ) ; la densit misurata nei singoli pixel tissutali viene poi rapportata alla misurazione venosa , ed espressa in percentuale di questa ( cbv = densit pixel parenchimale / densit pixel venoso ; es , densit nel pixel tissutale = 5% della densit nel pixel venoso cbv del pixel tissutale = 5 ml / 100 g ) ; ora pi chiaro come la sottostima della densit nella roi venosa , per artefatti di volume parziale , causi una sovrastima del cbv a livello tissutale e di riflesso , per lequazione del volume centrale cbf = cbv / mtt , anche del cbf . il cbf misura il volume di sangue distribuito a livello tissutale nellunit di tempo . 
6 in order to obtain quantitative measurements of cerebral blood volume ( cbv ) , cerebral blood flow ( cbf ) , mean transit time ( mtt ) and time to peak ( ttp ) , regions of interest ( rois ) are drawn on the different intracranial vascular territories . 
6 mediante posizionamento di apposite roi si possono ottenere misurazioni quantitative medie del cbv , cbf , mtt e ttp nei diversi territori di distribuzione delle principali arterie intra - craniche . 
it is expressed in [ s ] and is an index of the time that elapses between the beginning of contrast administration and maximum enhancement , or enhancement peak , in the roi . 
 mtt represents capillary transit time , that is , the time between arterial input in the capillary bed and venous outflow . it is expressed in [ s ] , is an sensitive index of cerebral perfusion pressure and , thanks to deconvolution , it is relatively less affected than is ttp by central haemodynamic changes such as cardiac failure or stenosis of the epiaortic arteries . mtt calculation is strictly dependent on the deconvolution process and therefore , in the event of asymmetrical perfusion as in ischaemia , on the choice of aif . 
in practice , mtt may be considered as the difference between the mean width of the time - density curve in a parenchymal pixel and the width of the curve in the reference artery ( aif ) [ 23 ]  . cbv measures the volume of cerebral blood at the capillary - tissue level , after appropriate exclusion from measurements of blood volume contained in large vessels , by means of density thresholds . 
the density measured in the single tissue pixels is then related to the venous density and expressed as a percentage of this ( cbv = parenchymal pixel density / venous pixel density ; e.g. : tissue pixel density = 5% venous pixel density = > cbv of tissue pixel = 5 ml / 100 g )  . 
it should now be clearer why an underestimation of density in the venous roi , due to partial - volume effects , leads to an overestimation of the cbv at the tissue level and consequently of cbf , given the central volume theorem cbf = cbv / mtt . cbf measures the volume of blood distributed at the tissue level in a unit of time . 
it is not measured directly but derived from the central volume theorem and is therefore dependent both on deconvolution and aif selection , which affect mtt , and on cbv measurement . 
 in brief , mtt indicates perfusion pressure , cbv reflects autoregulation mechanisms and capillary volume and cbf is the result of the above parameters . clinical applications acute ischaemic stroke thrombolysis is an approved therapy for acute ischaemic stroke [ 2 , 24 , 25 ] that aims to reperfuse the areas of ischaemic penumbra and limit the extent of the final area of infarction , thus reducing morbidity and disabling sequelae . the current indications for thrombolysis are based on a time window from symptom onset ( < 3h ) , findings of an unenhanced head ct ( no intracranial haemorrhage , no ct evidence of ischaemia of a portion of parenchyma exceeding 33% of the middle cerebral artery territory ) and absence of general contraindications for the drug [ 2 , 24 ]  . 
nevertheless , even such stringent criteria do not eliminate the significant risk of brain haemorrhage ( 15% ) [ 26 ] , and patient selection based on such criteria appears to be unsatisfactory . 
it is recognised that the time window alone is insufficient for accounting for the complex model of brain tissue viability , which in addition to a time factor includes a haemodynamic factor , a tissue factor and an intervention factor [ 27 ]  . 
as a result , individual visualisation of the extent of the infarcted and at - risk areas and of their relationship according to the pathophysiological model of infarct core and ischaemic penumbra has been proposed as a better tool for selecting patients for thrombolytic therapy . 
thrombolysis in patients with extensive cerebral infarctions and small areas of penumbra appears to be of little benefit and lead to a high risk of haemorrhage [ 25 , 28 , 29 ]  . 
on the other hand , although controversial , some studies have demonstrated that a significant proportion of patients with 1232 applicazioni cliniche ictus ischemico acuto la trombolisi una terapia approvata per lictus ischemico acuto [ 2 , 24 , 25 ] che ha lo scopo di riperfondere le aree di penombra ischemica e di ridurre lestensione dellarea finale di infarto , riducendo cos la morbilit e gli esiti invalidanti . 
le attuali indicazioni alla terapia trombolitica sono basate su una finestra temporale dallesordio clinico ( < 3 h ) , sul risultato della tc cranio in condizioni di base ( assenza di emorragia intracranica , assenza di segni tc di ischemia di una porzione di parenchima con estensione superiore al 33% del territorio vascolare dellarteria cerebrale media ) e sullassenza di controindicazioni generali al farmaco [ 2 , 24 ]  . la maggior parte dei pazienti colpiti da ictus ischemico non ricevono trattamento , poich i criteri di eligibilit sono molto restrittivi , soprattutto rispetto alla finestra temporale , anche perch in una significativa percentuale di casi il momento di insorgenza dei sintomi non determinabile con precisione ( classico il caso del cosiddetto wake - up stroke )  . 
ciononostante , perfino criteri cos restrittivi non eliminano il significativo rischio di emorragia intracranica ( 15% ) [ 26 ] e la selezione dei pazienti a cui somministrare la terapia trombolitica , basata su tali criteri , non appare soddisfacente . 
la finestra temporale infatti stata riconosciuta insufficiente a spiegare , da sola , lintricato modello della vitalit del tessuto cerebrale , che invece include , oltre al fattore tempo , un fattore emodinamico , un fattore tissutale ed un fattore terapeutico [ 27 ]  . 
perci la visualizzazione individuale dellestensione delle aree infartuate e di quelle a rischio , e del loro rapporto , secondo il modello fisiopatologico del core infartuale e della penombra ischemica , stato suggerito come un migliore strumento di selezione dei pazienti per il trattamento trombolitico . 
la trombolisi in pazienti con infarti cerebrali estesi e piccole aree di penombra , sarebbe di scarso beneficio e alto rischio emorragico [ 25 , 28 , 29 ] , mentre stato postulato e dimostrato in alcuni studi , ma ancora controverso , che una significativa percentuale di pazienti con limitate aree di infarto ed estese aree di penombra potrebbero beneficiare del trattamento di rivascolarizzazione anche oltre la classica finestra temporale delle 3 ore [ 30 , 31 ]  . il modello del core e della penombra [ 3234 ] postula che nel contesto di unarea di parenchima ipoperfusa , con elevati valori di mtt , spesso dipendente da circoli collaterali , si attuino meccanismi di autoregolazione che , inducendo vasodilatazione ed aumento del cbv , siano capaci di mantenere i valori del cbf sopra la soglia della morte cellulare neuronale ; le aree di parenchima caratterizzate da tali condizioni sono ritenute aree di penombra ischemica , ancora vitali , ad alto rischio di infarto , che potrebbero beneficiare di interventi di riperfusione . 
 limited areas of infarction and extensive areas of penumbra might benefit from revascularisation even beyond the 3 - h time window [ 30 , 31 ]  . the model of the infarct core and penumbra [ 3234 ] postulates that in the context of an area of hypoperfused parenchyma , with high mtt values , often supplied by collateral circulations , autoregulation mechanisms take place that , by inducing vasodilatation and increased cbv , are able to maintain cbf values above the threshold for neuronal death . 
where ischaemic injury is more severe and protracted , on the other hand , autoregulation is unable to maintain cbf , brain tissue sustains irreversible hypoxic damage and cbv values decrease . 
however , these pathophysiological aspects are complicated by other factors such as the duration of hypoperfusion , selective vulnerability of some neurons and physiological conditions during reperfusion [ 38 , 32 ]  . 
radiological evidence of the existence of a penumbra area has been provided by mri with combined diffusionand perfusion - weighted imaging ( dwipwi ) , the results of which have led to the pwi - dwi mismatch hypothesis [ 34 ]  . unenhanced head ct remains the first imaging modality in the assessment of patients with acute focal neurological symptoms ( stroke ) to exclude brain haemorrhage and evaluate the presence of early signs of ischaemia , such as greymatter hypoattenuation and sulcal effacement [ 35 ]  . it has been suggested that , by identifying the areas of cerebral infarction and those at risk of infarction ( ischaemic penumbra ) , the study of brain perfusion may help to select patients for thrombolytic therapy [ 15 ]  . 
other techniques for determining brain perfusion , such as xe - ct , spect and pet , although quantitative , are limited by poor availability in emergency settings and poor patient tolerance , whereas perfusion mri also suffers from an inability to provide quantitative data [ 3 ]  . 
availability in emergency settings , rapidity ( data acquisition < 5 min ) , cost and quantitative measurements probably make p - ct the technique of choice in the assessment of patients with ischaemic stroke [ 16 ]  . 
this ability of p - ct is based on the hypothesis that infarcted areas will exhibit high mtt values and low cbf and cbv values , whereas the areas at risk will show normal or increased cbv values [ 4 , 1517 , 21 , 39 , 40 ]  . 
cbv maps seem to be the least sensitive for ischaemia , with approximately 25% of acute infarctions failing to show any significant change in cbv , but are also the most specific for infarction areas [ 16 , 41 ]  . 
levidenza radiologica dellesistenza della penombra ischemica invece , stata dimostrata da studi combinati di rm con sequenze di diffusione ( dwi ) e perfusione ( pwi ) , dai cui risultati si derivato il concetto di mismatch pwi - dwi [ 34 ]  . la tc cerebrale in condizioni di base rimane la prima modalit di imaging usata per lo studio del paziente con sintomatologia neurologica focale acuta ( ictus ) , per escludere lemorragia intracranica e valutare la presenza di segni precoci di ischemia , quali lipodensit della sostanza grigia e la cancellazione dei solchi [ 35 ]  . stato suggerito che lo studio della perfusione cerebrale , identificando le aree di infarto cerebrale e quelle a rischio stage 1 stage 2 stage 3 cerebral perfusion pressure fig . 
7 the diagram illustrates the changes in mean transit time ( mtt ) , cerebral blood volume ( cbv ) , cerebral blood flow ( cbf ) and oxygen extraction fraction ( oxef ) in response to progressive reduction of cerebral perfusion pressure . 
in patients with stroke , the scan level is usually located in correspondence with the basal ganglia so as to visualise the three main supratentorial vascular territories ( fig 9 )  . 
one limitation of p - ct , especially when compared with mri , is a relative lack of sensitivity to lacunar infarctions [ 44 ] , exposure to ionising radiation and the use of iodinated contrast material . 
nonetheless , administration of iodinated nonionic di infarto ( aree di penombra ischemica ) , possa essere di ausilio nella selezione di pazienti candidati alla terapia trombolitica [ 15 ]  . 
le altre tecniche per misurare la perfusione cerebrale , quali xe - tc , spect e pet , sebbene quantitative , sono limitate dalla disponibilit in emergenza e dalla tolleranza del paziente , mentre la perfusione - rm soffre anche dellimpossibilit di fornire dati quantitativi [ 3 ]  . 
la ptc probabilmente la metodica di scelta , per disponibilit in condizioni di emergenza , per rapidit di esame ( acquisizione dati in < 5 min ) , costi contenuti , e misurazioni quantitative , nella valutazione del paziente con ictus ischemico [ 16 ]  . 
tale capacit della p - tc si basa sullipotesi che le aree infartuate presentino elevati valori di mtt , e ridotti valori di cbf e cbv , mentre nelle aree a rischio i valori di cbv siano normali o aumentati [ 4 , 1517 , 21 , 39 , 40 ]  . 
recenti studi [ 16 , 41 ] suggeriscono che le mappe di mtt siano le pi sensibili per delineare le aree ischemiche , seguite da quelle del cbf ; le mappe di cbv sembrano essere le meno sensibili allischemia , infatti , circa il 25% degli infarti acuti non mostra significative alterazioni di tale parametro , ma sono anche le pi specifiche per le aree di infarto [ 16 , 41 ]  . 
da ci deriva la raccomandazione di valutare prima le mappe di mtt e cbf alla ricerca di aree ipoperfuse , e se queste sono presenti , utilizzare le mappe di cbv per differenziare al loro interno le aree di penombra da quelle di infarto , considerando per che tali mappe possono essere normali anche in caso di infarto . 
 un importante studio prospettico [ 15 ] su pazienti affetti da ischemia cerebrale acuta , segna una pietra miliare nella validazione delle teorie su cui si basa la p - tc , mostrando significativa correlazione tra aree di ridotto cbv ( > 2 , 5 ml / 100 g ) alla p - tc di ammissione e le aree finali di infarto nei controlli a distanza , in pazienti con riperfusione , e altrettanto precisa correlazione tra aree con prolungato mtt ( > 1 , 5 volte rispetto al controlato ) e / o ridotto cbf ( riduzione > 34% rispetto al controlato ) alla p - tc di ammissione e larea finale di infarto , al controllo a distanza , in pazienti senza riperfusione . 
based on threshold values set by the operator , the software generates a colour map ( middle image in the bottom row ) where the colour green is attributed to pixels with increased mean transit time ( mtt ) , as is the case in ischaemic penumbra , and the colour red is attributed to pixels with low cerebral blood volume ( cbv ) , as is the case in the infarct core . 
sulla base di valori soglia predeterminati , il software attribuisce , nella mappa al centro nella fila in basso , il colore verde ai pixel con alterazioni perfusionali con le caratteristiche dei territori di penombra , ed il colore rosso ai pixel con caratteristiche di core infartuale . 
qualora si voglia raddoppiare la copertura anatomica , una seconda sca , nsione , ad un altro livello , pu essere effettuata osservando unattesa , rispetto alla scansione precedente , di 36 mun limite della p - tc , soprattutto in confronto alla rm , la relativa insensibilit agli infarti lacunari [ 44 ] , lesposizione alle radiazioni ionizzanti , e luso del mdc iodato . 
la somministrazione di mdc iodato non ionico in emergenza , anche senza preventiva valutazione della creatininemia , comunque risultata sicura in una larga serie di pazienti con ictus cerebrale acuto , sottoposti a p - tc , con esclusione dei pazienti con insufficienza renale nota , paraproteinemia nota , trapianto renale , assunzione di farmaci nefrotossici , e / o lunga storia di diabete mellito [ 45 ]  . in conclusione , sebbene la validit delle misurazioni quantitative della p - tc sia messa in discussione dalla loro variabilit legata alla scelta dellaif , al posizionamento delle rois ed agli artefatti da volume parziale [ 46 ] e sebbene ulteriori studi siano necessari per confrontare le misurazioni della p - tc con quelle delle altre metodiche di studio della perfusione cerebrale , i risultati sinora disponibili appaiono incoraggianti riguardo alla selezione di pazienti con estesa area di penombra ischemica , e quindi potenzialmente buoni candidati per la terapia trombolitica , ed inoltre , le misurazioni qualitative relative al controlato , offrendo dati affidabili , restano una valida alternativa , comunque indicativa dello stato della perfusionale cerebrale [ 40 ]  . infine utile qui ricordare che linterpretazione delle mappe di perfusione sicuramente facilitata e resa pi accurata dalla disponibilit di informazioni sullo stato anatomico vascolare intraed extra - cranico . 
con lavvento della tecnologia tc multidetettore , langio - tc , eseguita subito dopo la p - tc , con la somministrazione di un ulteriore bolo di 7090 ml di mdc , permette unaccurata valutazione della perviet delle arterie epiaortiche ed intra - craniche , nonch della presenza di circoli collaterali nelle patologie cerebrovascolari acute e pu avere un ruolo significativo nella selezione dei pazienti con ictus ischemico , ai fini di un corretto 1235 fig . 
9 un piano di scansione orientato lungo il tetto delle orbite , e posizionato circa 2 cm cranialmente a queste , consente la visualizzazione , nelle due fette di 10 mm , di una rappresentazione dei tre territori vascolari sopratentoriali : il territorio dellarteria cerebrale anteriore , della media e della posteriore . contrast material , even without preliminary serum creatinine assessment , proved to be safe in a large series of patients with acute cerebral stroke studied by emergency p - ct , after exclusion of those with known renal failure , known paraproteinaemia , kidney transplant , use of nephrotoxic drugs or a long - standing history of diabetes mellitus [ 45 ]  . in conclusion , although the validity of the quantitative measurements of p - ct has been questioned owing to variability related to aif choice , roi positioning and partialvolume artefacts [ 46 ] ; and although further studies are needed to compare p - ct measurements with those provided by other techniques for the study of brain perfusion , encouraging results have been obtained with regard to the selection of patients with an extensive area of ischaemic penumbra and therefore potential candidates for thrombolytic therapy . 
in addition , qualitative measurements of the contralateral side provide reliable data and offer a valuable alternative that is at any rate indicative of the state of cerebral perfusion [ 40 ]  . finally , it is useful to remember that the interpretation of perfusion maps is definitely facilitated and made more accurate by the availability of information on the state of the intraand extracranial vascular anatomy . 
with the advent of mdct technology , ct angiography , performed with the administration of an additional bolus of 7090 ml of contrast immediately after p - ct , allows accurate assessment of the patency of the epiaortic and intracranial arteries and of the presence of collateral circulations in acute cerebrovascular disease . 
in a context of acute cerebrovascular disease , p - ct combined with ct angiography therefore provides a rapid , efficient and practical tool for identifying the cause , extent and pathophysiology of ischaemia , nd for optimising treatment decisions . chronic ischaemic cerebral disease ( vascular reserve ) in patients with chronic cerebral ischaemia caused by stenosis of the intracranial arteries or epiaortic vessels , it is neca . 
nel contesto della patologia cerebro - vascolare acuta , quindi , la p - tc , combinata con langio - tc , rappresenta una soluzione rapida , efficiente e pratica per diagnosticare leziologia , lestensione e la fisiopatologia dellischemia , cos da ottimizzare la scelta terapeutica . patologia cerebrale ischemica cronica ( riserva vascolare ) nei pazienti con ischemia cerebrale cronica causata da stenosi arteriose intra - craniche o dei vasi epi - aortici , necessario distinguere le condizioni di stabile compenso emodinamico , dalle situazioni in cui il compenso instabile , ed il parenchima cerebrale sottoposto ad uno stress emodinamico e metabolico [ 48 ]  . 
tenendo presente il principio del volume centrale ( cbf = cbv / mtt ) , tipicamente , una stenosi arteriosa emodinamicamente significativa induce un prolungamento del mtt che innesca a sua volta i meccanismi dellautoregolazione cerebrale , con conseguente vasodilatazione , riflessa dallincremento del cbv , con cbf normale o lievemente diminuito . 
questo quadro perfusionale tipico per non fornisce informazioni sulla gravit dellipoperfusione , n sulle capacit residue del circolo cerebrale di adattarsi ad ulteriori modificazioni emodinamiche , ovvero sullesistenza di una riserva cerebro - vascolare . 
la valutazione della riserva cerebro - vascolare si pu ottenere osservando come la perfusione cerebrale reagisce in risposta ad uno stress emodinamico , appositamente provocato mediante somministrazione di un agente vasoattivo . 
i pazienti che hanno esaurito la riserva cerebro - vascolare presentano gi in condizioni di base vasodilatazione massima nelle aree ipoperfuse e non sono quindi in grado di rispondere allo stress emodinamico indotto dallacetazolamide . 
si ritiene che tali pazienti siano a rischio elevato di infarto cerebrale e possano beneficiare di interventi di rivascolarizzazione per aumentare il cbf nelle aree ipoperfuse [ 48 ]  . 
di 1000 mg di acetazolamide pu individuare i pazienti a rischio di infarto tra i portatori di stenosi arteriose epi - aortiche o intra - craniche [ 48 ]  . 
dopo la somministrazione di acetazolamide un incremento del cbf pari al 20%40% rispetto alle condizioni di base considerato normale , un incremento di meno del 5% considerato indicativo di insufficienza emodinamica , mentre la riduzione paradossa del cbf rispetto alla condizione di base segno di furto vascolare , indicativo di tessuto ad alto rischio di infarto [ 49 ]  . 
lacetazolamide generalmente ben tollerata ; sono stati descritti effetti collaterali lievi quali parestesie e cefalea e sebbene siano stati riportati casi di attacchi ischemici transitori , leventuale ischemia indotta sempre stata reversibile [ 48 ]  . 
10 computed tomography angiography ( cta ) , used to complement perfusion ct in this patient with acute right hemiplegia and aphasia , clearly shows left m1 occlusion ( red arrow on exam at 2.5 h ) , which is the cause of the perfusion abnormalities visible on the colour map . 
10 langio - tc cerebrale , esame complementare alla perfusione - tc , dimostra chiaramente , in questo paziente con esordio acuto di emiplegia destra ed afasia , locclusione del tratto m1 dellarteria cerebrale media di sinistra ( freccia rossa nellesame a 2 , 5 h ) , responsabile delle alterazioni perfusionali evidenziate dalla mappa colore . 
il controllo angio - tc a 24 h di distanza , dopo trattamento fibrinolitico , dimostra la ricanalizzazione del vaso ( freccia rossa )  . essary to distinguish between situations of stable haemodynamic compensation and those in which compensation is unstable and the brain parenchyma is subject to haemodynamic and metabolic stress [ 48 ]  . 
bearing in mind the central volume theorem ( cbf = cbv / mtt ) , a haemodynamically significant arterial stenosis will typically result in a prolonged mtt , which in turn will trigger cerebral autoregulation mechanisms , with consequent vasodilatation reflected by an increase in cbv , with normal or slightly decreased cbf . 
this typical perfusion pattern does not , however , give information on the severity of hypoperfusion or on the residual capacity of the cerebral circulation to adjust to further haemodynamic changes in other words , on the existence of a cerebrovascular reserve . 
patients who have exhausted the cerebrovascular reserve show maximal vasodilatation in the hypoperfused areas already at baseline and are therefore unable to respond to the haemodynamic stress induced by acetazolamide . these patients are believed to be at high risk for cerebral infarction and to benefit from revascularisation procedures to increase cbf in hypoperfused areas [ 48 ]  . 
11 perfusion - computed tomography ( p - ct ) before and after right internal carotid endarterectomy.in this patient with mild but progressive left hemisyndrome , ct angiography and p - ct ( upper row ) show severe right internal carotid stenosis causing hypoperfusion of the whole right cerebral hemisphere ( there is a foetal origin of the right posterior cerebral artery , not shown in the figure )  . 
lo studio angio - tc e p - tc ( fila superiore ) , in questo paziente con emisindrome sn lieve ma ingravescente , mostra stenosi serrata del bulbo carotideo destro , cui si associa ipoperfusione di gran parte dellemisfero cerebrale destro ( il paziente portatore di unorigine fetale dellarteria cerebrale posteriore destra , rifornita per via comunicante posteriore ; non mostrata nella figura ) , testimoniata dal prolungamento del mtt , dalla riduzione del cbf e dal lieve aumento del cbv , espressione dei meccanismi di autoregolazione . 
il controllo angio - tc e p - tc ( fila inferiore ) eseguito tre giorni dopo lintervento di endoarterectomia carotidea destra documenta la ricostituzione del lume vascolare e la risoluzione del deficit perfusionale emisferico destro . those with stenosis of the epiaortic or intracranial arteries [ 48 ]  . 
an increase less than 5% is considered indicative of haemodynamic insufficiency , whereas a paradoxical reduction of cbf relative to baseline is a sign of vascular shunting and thus of tissue at a high risk of infarction [ 49 ]  . 
acetazolamide is generally well tolerated ; the reported side effects are mild , such as paraesthesia and headache , and although there have been cases of transient ischaemic attacks , the induced ischaemia was always reversible [ 48 ]  . 
angiographic evidence of vasospasm is present in 60%80% of patients with sah , whereas 30% of patients present symptoms of vasospasm , and half of these develop cerebral infarction [ 51 ]  . 
transcranial doppler ultrasound is the most emorragia sub - aracnoidea e vasospasmo il vasospasmo una complicanza frequente dellemorragia sub - aracnoidea ( esa ) nella fase subacuta precoce [ 6 ]  . levidenza angiografica di vasospasmo presente nel 60%80% dei pazienti con esa , il 30% ne presenta i sintomi , e la met di questi sviluppa un infarto cerebrale [ 51 ]  . leco - doppler transcranico la modalit pi usata per il follow - up non invasivo in questi pazienti , per guidare le scelte terapeutiche e controllarne lefficacia , ma , oltre ad essere operatore dipendente , non offre misurazioni quantitative a livello tissutale ed gravata da scarsa specificit [ 52 ]  . 
anche se non sono ancora disponibili studi in grado di fornire valori di soglia dei parametri di perfusione , la misurazione del cbf , cbv e mtt con p - tc , associata a studi anatomici vascolari con angio - tc , potrebbe rappresentare un utile strumento diagnostico per il follow - up non invasivo dei pazienti con vasospasmo conseguente ad esa [ 6 ] , fornendo informazioni utili al trattamento medico ed anche alla scelta della tempistica chirurgica . trauma cranico la predizione della prognosi nei pazienti con trauma cranico severo rimane un compito complesso e controverso . 
however , it is operator dependent , unable to provide quantitative measurements at the tissue level and suffers from limited specificity [ 52 ]  . even though no study has yet been able to provide threshold values for the perfusion parameters , p - ct measurement of cbf , cbv and mtt , combined with vascular anatomy studies with ct angiography , might represent a valuable diagnostic tool for the noninvasive follow - up of patients with sah - related vasospasm [ 6 ] , as it provides information useful for medical management of patients and for choosing the best timing for surgery . head trauma predicting outcomes in patients with severe head trauma remains a complex and controversial issue . 
a finding of cerebral hypoperfusion , in generally hypotensive patients , indicates a loss of cerebrovascular autoregulation and is thought to be a predictor of the development of cerebral oedema , whereas normal or increased perfusion values would indicate a positive outcome [ 54 ]  . brain tumours in the study of brain tumours , there is growing interest in the noninvasive assessment of tumour vascularity [ 55 ]  . 
some brain tumours are characterised by neoangiogenesis and hypervascularity , which result in increased microvascular permeability [ measured as permeability surface area product ( ps ) or as contrast transfer coefficient ( k - trans ) , in ml / 100g per minute ] and increased cbv , due to the presence of numerous tortuous vascular structures , with immature , disrupted or absent bbb [ 56 ]  . 
contrast enhancement , the key diagnostic element in morphological imaging , is a poorly specific finding that in tumours may be caused by bbb abnormalities , hypervascularity , extent of the interstitial space or a combination of these factors . 
if the extreme disruption of microvascular permeability of some tumours causes excessive leakage of contrast material during the first pass of 1238 zionale possiede alta sensibilit nellindividuazione di lesioni intra - craniche che necessitano di intervento neurochirurgico , ma non offre validi elementi di tipo prognostico . 
il riscontro di ipoperfusione cerebrale , in pazienti generalmente ipotesi , indica la perdita dellautoregolazione cerebro - vascolare e sarebbe in grado di predire lo sviluppo di edema cerebrale , mentre valori di perfusione normali o aumentati rappresenterebbero indicatori prognostici positivi [ 54 ]  . tumori intra - cranici nello studio delle neoplasie intra - craniche crescente interesse rivolto alla valutazione non - invasiva della vascolarizzazione tumorale [ 55 ]  . 
alcuni tumori intracranici sono caratterizzati da neo - angiogenesi ed ipervascolarizzazione , che risultano in aumentata permeabilit vascolare ( misurata come permeability surface product ( ps ) o come coefficiente di trasferimento di contrasto ( k - trans ) , in [ ml / 100 g / min ] ) , e incremento del cbv , per la presenza di strutture vascolari pi numerose , tortuose , con barriera emato - encefalica immatura , danneggiata o assente [ 56 ]  . 
il contrastenhancement , elemento diagnostico chiave dellimaging morfologico , un reperto poco specifico , che nei tumori pu essere determinato dallalterazione della bee , dallipervascolarizzazione , dallampiezza dello spazio interstiziale o dalla concomitanza dei suddetti fattori . 
numerosi studi [ 55 , 56 ] dimostrano che nei gliomi , la ps ed il cbv , misurati con tecniche di rm - perfusione ( con sequenze contrast - enhanced t2 * - w , basate sulla suscettibilit magnetica , e contrast - enhanced t1 - w ) , correlano con lindice mitotico , il grading istologico e laggressivit biologica . 
se lestrema alterazione della permeabilit vascolare in alcuni tumori causa uno stravaso eccessivo del mezzo di contrasto gi durante il primo passaggio del bolo , le misurazioni del cbv , per essere accurate , necessitano di appropriate strategie di correzione ( ad esempio procedure di gamma - fitting della curva densit - tempo )  . 
in tali tumori , ipervascolarizzati e con alterata permeabilit , le misurazioni della ps o del k - trans , sembrano essere pi utili , perch correlano pi strettamente con il grado dei glomi . 
inoltre anche la risposta alle terapie anti - angiogenetiche recentemente introdotte , con riduzione della crescita tumorale , trova il suo corrispettivo in una riduzione dei valori di ps [ 57 ]  . 
in this patient with head trauma and left parietal bone fracture , p - ct shows a large area of hypoperfused brain parenchyma in the left temporoparietooccipital region , well beyond the limits of the hypodense contusion documented by enhanced ct . 
in questo paziente con trauma cranico e frattura parietale sinistra lo studio p - tc mostra una vasta area di ipoperfusione temporo - parieto - occipitale sn , caratterizzata da aumentati valori di mtt e ridotti valori di cbf e cbv , estesa ben oltre i limiti della lesione contusiva ipodensa temporo - parietale sinistra , adiacente alla frattura , visibile nellesame tc morfologico . 
in such hypervascular tumours with disrupted permeability , ps or k - trans measurements appear to be more useful , as they correlate more closely with the grade of gliomas . 
however , in the subgroup of highgrade gliomas [ world health organisation ( who ) iii - iv ] , k - trans was directly related to length of survival . 
measurement of bbb permeability by p - ct or p - mri is based on the same mathematical models , the most frequently used of which is the patlak model [ 59 ]  . 
this model describes a method to measure the transfer - rate constant of contrast material from the vessel to the interstitium , through a mathematical comparison ( deconvolution ) between the timedensity curve or a time - signal curve obtained in tumour tiscon la sopravvivenza ; questa evidenza viene spiegata dagli autori come possibile effetto dellaumentata permeabilit vascolare nel tumore , che permetterebbe una migliore penetrazione degli agenti chemioterapici ed anti - angiogenici . 
la misurazione della permeabilit della bee ottenuta con ptc o con p - rm si fonda sulluso degli stessi modelli matematici , tra i quali , uno dei pi usati il modello di patlak [ 59 ]  . 
questo modello descrive un metodo per misurare la costante di trasferimento del mezzo di contrasto dal vaso allinterstizio , operando un processo di confronto matematico ( deconvoluzione ) tra una curva densit - tempo o segnale - tempo rilevata nel tessuto tumorale ( dove presente stravaso di mdc ) ed una curva rilevata nel lume di unarteria di riferimento o aif ( dove si assume non avvenga stravaso di mdc )  . 
le tecniche di imaging di perfusione trovano utilit nello studio dei tumori intra - cranici nel tentativo di facilitare la distinzione tra tumore primitivo e metastatico , nel rendere pi accurato il grading , nella valutazione della risposta alle terapie antiangiogenetiche , e nella diagnosi differenziale tra radionecrosi e recidiva tumorale ; inoltre si sta affermando il ruolo dellimaging perfusionale per la scelta del bersaglio delle procedure bioptiche , scelta basata sulla individuazione delle aree tumorali a maggiore aggressivit 1239 a . 
perfusion - imaging techniques have been found useful in the study of brain tumours to facilitate the distinction between primary or metastatic tumour , make grading more accurate , evaluate response to antiangiogenic agents and differentiate radiation necrosis from tumour recurrence . 
in addition , the role of perfusion imaging is also gaining ground in guiding biopsy procedures , where the biopsy target is chosen based on identification of the most malignant area in a heterogeneous tumour [ 56 ]  . in contrast to p - mri , only a few small studies are available on the use of p - ct in human brain tumours [ 7 , 60 , 61 ]  . the examination is performed using a similar technique to that described for ischaemic disease , and the scan level corresponds to the tumour site . 
cbv and permeability measurements are made by positioning several small rois over the tumour mass , taking care to exclude large vascular structures from the measurements , and the measurements in the rois are compared with those of a mirror area on the contralateral side . 
the most recent scientific data , many of which are still unpublished , suggest that it is the maximum rather than the mean values of cbv and ps in the tumour that correlate with histopathological grading , as is also the case with histological assessment , which assigns a who grade on the basis of the most malignant portion of the tumour . in theory , p - ct could offer several advantages over pmri in terms of spatial resolution , insensitivity to paramagnetic susceptibility artefacts ( in cases with haemorrhage , calcifications , metallic implants ) , linear correlation between contrast concentration and density and quantitative cbv and permeability measurements , even in hypervascular tumours . in practice , however , no published study has compared the results of the two methods on representative series of patients with brain tumours . 
on the other hand , radiation dose , potential toxicity of iodinated contrast material and limited anatomical coverage of p - ct still justify the predominant use of mri , a modality that remains crucial in the morphological imaging of tumours [ 7 ]  . limitations , artefacts and controversies although the ability of p - ct to provide quantitative measurements has been confirmed by comparison with pet , spect and xe - ct , its accuracy has not yet been unquestionably demonstrated , probably as a result of heterogeneous study methodologies adopted by the various authors . 
furthermore , the quantitative measurements are dependent on several variables , such as the software used , bolus dispersion ( caused by too slow an injection rate , insufficient cardiac function , haemodynamically significant arterial stenoses ) , aif selection , partial - volume artefacts , the misleading contribution of 1240 nel contesto delleterogeneit della neoplasia [ 56 ]  . 
 contrariamente a quanto verificatosi per gli studi di rmperfusione , sono disponibili solo pochi e limitati studi sulluso della p - tc nei tumori cerebrali negli uomini [ 7 , 60 , 61 ]  . 
per la misurazione della permeabilit preferibile disporre di curve densit / tempo allequilibrio invece che limitate al primo passaggio del bolo ; quindi oltre i 50 s di scansione , si continuano ad acquisire immagini in modalit cine , per circa 3 min , al ritmo di 1 scansione ogni 15 s . 
le misurazioni del cbv e della permeabilit si effettuano posizionando multiple piccole roi nel contesto della massa tumorale , avendo cura di escludere dalla misurazione le grosse strutture vascolari , e si confrontano ad unarea speculare nel controlato . 
i pi recenti dati scientifici , molti ancora non pubblicati , suggeriscono che pi dei valori medi di cbv e ps nel contesto della lesione tumorale , siano i valori massimi a correlare con il grading istopatologico , cos come accade peraltro per lesame istologico , che assegna il grado who in base alla porzione del tumore a pi alta malignit . in teoria la p - tc potrebbe avere vantaggi rispetto alle tecniche di rm - perfusione , in termini di risoluzione spaziale , insensibilit agli artefatti di suscettibilit paramagnetica ( in casi con emorragia , calcificazioni , impianti metallici ) , correlazione lineare tra concentrazione di mdc e densit , e misurazioni quantitative di cbv e permeabilit , anche in tumori ipervascolari . 
daltra parte , la dose di radiazioni , la potenziale tossicit del mdc iodato , la limitata copertura anatomica , rappresentano fattori che ancora giustificano luso prevalente della rm , metodica comunque irrinunciabile nellimaging morfologico nei tumori [ 7 ]  . limitazioni , artefatti e controversie sebbene la capacit della p - tc di fornire misurazioni quantitative sia stata confermata , come precedentemente detto , da studi comparativi con pet , spect e xe - tc , la sua accuratezza non ancora stata provata in maniera incontrovertibile , probabilmente anche a causa di metodologie di studio non omogenee tra i diversi autori . 
le misurazioni quantitative sono inoltre dipendenti da multiple variabili , quali il software impiegato , la dispersione del bolo ( causata da uniniezione troppo lenta , uninsufficiente funzione cardiaca , stenosi arteriose emodinamicamente significative ) , la scelta dellaif , gli artefatti da volume parziale , lingannevole contributo del liquor e delle strutture vascolari alle misurazioni , il posizionamento delle roi , ed infine le significative differenze perfusionali tra sostanza grigia e sostanza bianca . 
although commercial software packages for analysis of perfusion data are relatively easy to use , operators need to master the issues inherent to the examination and postprocessing procedures and require training in using thedata derived from perfusion studies conducted by expert radiologists have been shown to have good reproducibility [ 62 ] , whereas no study has evaluated reproducibility of data among nonexpert radiologists . 
in patients with ischaemic stroke , thrombolytic therapy , when indicated , should be initiated as soon as possible , so diagnostic imaging needs to be timely , accurate and fast . 
complementation of a conventional ct study of the brain with pct and ct angiography usually requires 10 - 12 min , whereas postprocessing with automatic software takes no longer than 3 min to provide colour - coded parametric maps that can guide the clinical treatment decisions . 
the disadvantage of this small delay in imaging procedures is widely compensated for by the acquisition of diagnostic information of major clinical importance , above all in those patients in the 3to 6 - h time window and those with an unknown time interval from symptom onset of symptoms , who are currently excluded from treatment . 
 as is known , p - ct employs ionising radiation and potentially nephrotoxic , hyperosmolar and allergenic iodinated contrast material , so the use of the technique requires individual clinical assessment , appropriate indications and strategies to contain the radiation dose . 
it is therefore a valuable alternative to other modalities for the measurement of brain perfusion , compared to which it has the advantage of being readily available and accessible even in emergency settings . 
for this reason , p - ct proves most useful in acute ischaemic stroke where , used in combination with ct angiography , it offers a complete overview of the causes of hypoperfusion and its haemodynamic and pathophysiological effects on the brain in a fast , noninvasive manner . 
p - ct is also helpful in patients with other , acute or chronic , cerebrovascular diseases ; in the follow - up of patients with sah ; in preand postoperative assessment of patients undergoing cerebral revascularisation procedures ; and in brain tumours for diagnosis , grading , biopsy guidance and monitoring treatment response . further studies are required to establish the accuracy , reliability and reproducibility of the quantitative measurements , but available data appear encouraging and indicate a major clinical impact . di post - processing e di un periodo di training per il loro uso ; una buona riproducibilit stata dimostrata , nei dati estratti dagli studi di perfusione , tra radiologi esperti [ 62 ] , mentre studi di questo tipo non sono ancora stati condotti per valutare la riproducibilit tra medici non esperti . 
ulteriori svantaggi della p - tc , soprattutto nelle applicazioni che riguardano la patologia ischemica , come gi detto , sono la limitata copertura anatomica e la scarsa sensibilit verso gli infarti lacunari . 
nei pazienti colpiti da ictus ischemico di fondamentale importanza che il trattamento trombolitico sia iniziato , se indicato , il pi rapidamente possibile , ed quindi auspicabile che la fase diagnostica radiologica sia tempestiva , accurata e veloce . 
il completamento di un esame tc convenzionale dellencefalo con lo studio perfusionale e angiotc richiede solitamente 1012 minuti , mentre le procedure di post - processing , con software automatici , richiedono non pi di 3 minuti per ottenere mappe parametriche colore ai fini di decisioni clinico - terapeutiche ; solo valutazioni quantitative accurate , solitamente non necessarie in situazioni di emergenza , richiedono tempi di post - processing pi lunghi . 
lo svantaggio di questo modesto ritardo nelle procedure di imaging di solito ampiamente compensato dallacquisizione di informazioni diagnostiche di grande rilevanza clinica , soprattutto in quei pazienti nella finestra delle 36 ore ed in quelli con intervallo sconosciuto dallinsorgenza dei sintomi , attualmente esclusi dal trattamento . la p - tc , come ovvio , utilizza radiazioni ionizzanti , e mdc iodato potenzialmente nefrotossico , iperosmolare e allergenico , pertanto limpiego di tale metodica necessita di valutazione clinica individualizzata , indicazioni appropriate , e strategie di contenimento della dose di radiazioni . conclusioni in conclusione , la p - tc permette una valutazione quantitativa affidabile e veloce del cbf e del cbv , offrendo cos una visualizzazione diretta dei meccanismi di autoregolazione cerebrale , e ponendosi come valida alternativa alle altre modalit di misurazione della perfusione cerebrale , rispetto alle quali ha il maggior vantaggio di essere una tecnica prontamente disponibile ed accessibile , anche in condizioni di emergenza . 
per tale ragione la p - tc utile soprattutto nella patologia ischemica cerebrale acuta , situazione in cui , con il concomitante impiego dellangio - tc , offre in maniera rapida e non - invasiva , una completa panoramica della causa dellipoperfusione , nonch delle sue ripercussioni emodinamiche e fisiopatologiche sul parenchima cerebrale . 
this study was done to evaluate the diagnostic role of enteroclysis with multidetector computed tomography ( mdct ) and single - detector ct ( sdct ) in patients affected by smallbowel crohns disease . 
in comparison with double - contrast enteroclysis , sensitivity , specificity and diagnostic accuracy were 90% , 71% and 89% for sdct and 92% , 83% and 90% for mdct . 
mdct is superior to sdct because it allows a better spatial resolution and improves depiction of the pathological patterns of crohns disease . key words crohns disease ct enteroclysis multidetector ct riassunto obiettivo . 
quarantacinque pazienti sono stati sottoposti ad enteroclisi - tc a singolo detettore ( n = 20 ) o multidetettore ( n = 25 ) previa somministrazione di metilcellulosa tramite sondino naso - digiunale . 
confrontando i dati tc con quelli del clisma del tenue , abbiamo riscontrato valori di sensibilit , specificit ed accuratezza diagnostica rispettivamente del 90% , 71% e 89% con la tcsd e del 92 , 83 e 90% con la tcmd . 
la tcmd da preferire alla tcsd per la sua migliore risoluzione spaziale e perch consente una migliore rappresentazione dei segni patologici di malattia di crohn . parole chiave malattia di crohn tc enteroclisi tc multidetettore introduction introduzione crohns disease is a chronic granulomatous disease that causes transmural inflammation of the small bowel . 
complications ( abscess , fistula , stenosis ) are common and can be seen in over 40% of patients [ 1 ]  . conventional radiology techniques ( small - bowel barium examination , double - contrast enema ) visualise the small la malattia di crohn una malattia granulomatosa cronica che determina infiammazione transmurale dellintestino tenue . 
the added value of computed tomography ( ct ) is that it directly depicts the bowel wall , perienteric fat , mesentery , vessels and lymph nodes , as well as local complications of crohns disease and associated pathological conditions [ 2 ]  . 
the sensitivity of small - bowel ct is not well known and depends mainly on the quality of the study , severity of the inflammation and presence of mesenteric and intraperitoneal abnormalities . the diagnostic approach to small - bowel disease has recently been refined by the advent of spiral ct , which offers better spatial resolution and the possibility of generating multiplanar reconstructions . 
another technique proposed for the study of the small bowel is ct enteroclysis , where contrast material is administered through a nasojejunal tube , and contiguous axial images are obtained after complete distension of the small bowel [ 3 ]  . 
the function of ct enteroclysis is to overcome the individual pitfalls of ct and small - bowel enema and combine the advantages of the two techniques into a single study . 
the theoretical advantage of ct enteroclysis is the ability to simultaneously depict intraluminal , mural and extraintestinal complications of crohns disease [ 2 , 3 ]  . the aim of this study was to evaluate the diagnostic accuracy of ct enteroclysis with singleand multidetector detector techniques in symptomatic patients with a clinical suspicion or firm diagnosis of crohns disease . materials and methods we prospectively and consecutively evaluated 45 patients ( 22 men , 23 women ) aged 2570 years ( mean age 43 years ) presenting with a suspected or known diagnosis of crohns disease on the basis of clinical , laboratory and / or endoscopic findings . 
on the day before the procedure , they took a mixture of a and b sennosides with a cup of tea with sugar at 8 : 00 h , 15 mg of magnesium sulphate in three quarters of a glass of warm water at 17 : 00 h , followed by 3 l of water over the next 45 h ; at 21 : 00 h they had a cup of clear soup and fasted from 21 : 00 h onwards . all patients were intubated with a 12to 16 - fr nasojejunal tube ( create medic co . , yokohama , japan ) introduced under fluoroscopic guidance . 
patients were then taken into the ct room where contrast material ( 2 , 000 ml of 0.5% methylcellulose ) was administered manually with 60 - ml syringes , with care being taken to ensure a constant and continuous injection rate of about two syringes per minute . 
il valore aggiunto della tc quello di permettere la visualizzazione diretta della parete intestinale , del tessuto adiposo periviscerale , del mesentere , dei vasi e dei linfonodi , nonch delle complicanze locali di malattia di crohn e patologie associate [ 2 ]  . 
la sensibilit dello studio tc nelle malattie del tenue non ben conosciuta e si affida principalmente alla qualit dellindagine , alla severit dellinfiammazione e alla presenza di alterazioni mesenteriche ed intraperitoneali . 
lapproccio diagnostico allo studio del piccolo intestino stato negli ultimi anni ulteriormente modificato grazie allo sviluppo della tecnica spirale che ha consentito una migliore risoluzione spaziale e la possibilit di elaborare ricostruzioni multiplanari . 
contemporaneamente , nello studio del tenue stata proposta la tc enteroclisi in cui il mezzo di contrasto ( mdc ) viene somministrato attraverso un sondino naso - digiunale e dopo la totale distensione del piccolo intestino vengono riprese immagini assiali contigue dello stesso [ 3 ]  . 
la funzione di questa indagine quella di supplire alle carenze individuali della tc e del clisma del tenue , quindi di combinare i vantaggi di ciascuna tecnica in ununica metodica di studio . 
il teorico vantaggio della tc enteroclisi la capacit di mostrare contemporaneamente le complicanze intraluminali , murali ed extramurali della malattia di crohn [ 2 , 3 ]  . lo scopo di questo studio valutare laccuratezza diagnostica della tc enteroclisi effettuata con tecnica a singolo detettore e multidetettore in pazienti sintomatici con sospetto clinico o diagnosi certa di malattia di crohn . materiali e metodi sono stati valutati prospettivamente e consecutivamente 45 pazienti ( 22 uomini , 23 donne ) , di et compresa tra 25 e 70 anni ( et media 43 anni )  . 
il giorno prima dellesame i pazienti hanno ingerito alle ore 8 : 00 una miscela di sennosidi a e b con una tazza di t zuccherato e alle 17 : 00 15 mg di solfato di magnesio sciolti in 3 / 4 di un bicchiere di acqua tiepida , seguita dallassunzione di 3 litri di acqua nelle 45 ore successive . 
il digiuno stato rispettato delle 21 : 00 in poi . a tutti i pazienti stato introdotto sotto guida fluoroscopica un sondino naso - digiunale , del calibro 12 - 16 f ( create medic co , yokohama , giappone )  . 
the contrast - enhanced study was acquired 40 s after iv administration of 130150 ml contrast material ( ultravist 370 , schering ag , berlin , germany ) at a flow rate of 3 ml / s . axial images were processed on a computer workstation ( advantage windows , ge medical system ) to obtain 2d coronal and , if necessary , sagittal constructions . 
following ct , the nasojejunal tube was not removed , and after 68 h , all patients underwent a small - bowel barium enema according to the herlinger method [ 4 ] with digital technique . 
all ct images were assessed for the following signs : presence , site and number of abnormal bowel segments , degree of wall thickening , degree of mural enhancement [ hounsfield units ( hu ) ] , target sign , comb sign , perienteric stranding , fistulas , fibrofatty proliferation , lymphadenopathy , abscesses and other signs ( adhesions , incidental findings in the other abdominal organs , benign or malignant neoplasms of the small bowel )  . 
we evaluated small - bowel distension , which was classified according to a 4 - point scale for each segment ( 0 : no distension ; 1 : incomplete distension ; 2 : partial distension ; 3 : complete distension )  . 
the coronal and sagittal reconstructions were compared with the axial images to assess whether they provided additional information . images obtained with the small - bowel enema were checked for the following signs : oedematous folds , erosions , aphthoid and linear ulcers , fistulas , cobblestoning , micronodules , wall thickening , prestenotic dilatations , mesenteric inflammation and other signs ( adhesions , radiological findings suspicious for benign or malignant neoplasm )  . 
the ct and barium enema results were compared with those of retrograde 1190 sondino stata fissata a valle del treiz tramite linsufflazione di aria in un palloncino in modo da prevenire reflussi di mezzo di contrasto nello stomaco . 
i pazienti sono stati quindi condotti in sala tc ove il mezzo di contrasto ( 2000 ml di metilcellulosa allo 0 , 5% ) stato somministrato manualmente usando siringhe da 60 ml . 
abbiamo cercato di ottenere uniniezione costante e continua , circa 2 siringhe al minuto . al fine di evitare spasmi , ottenere unomogenea distensione del piccolo intestino , ridurre il disagio e la tensione addominale stato somministrato ai pazienti un farmaco anticolinergico ( n - butilscopolamina )  . 
abbiamo somministrato 10 mg di farmaco quando il paziente ha cominciato ad avvertire dolore addominale e 10 mg subito prima dellacquisizione delle immagini tc . venti pazienti sono stati studiati con tecnica tc spirale a singolo detettore ( tcsd ) ( prospeed , advantage sx spiral scanner , ge medical system , milwakee , usa ) con i seguenti parametri di acquisizione : collimazione 5 mm , intervallo 8 mm , ricostruzione 4 mm , kv 120 , mas 300 . 
venticinque pazienti sono stati studiati con tc multidetettore a 16 strati ( tcmd ) ( lightspeed pro16 , ge medical system , milwakee , usa ) con i seguenti parametri di scansione : collimazione 1 , 25 mm , velocit di scorrimento del tavolo 13 , 75 mm / rot , kv 120 , mas 500 , pitch 1 , 375 , tempo di rotazione 0 , 6 s . al termine dellinfusione di metilcellulosa lesame tc stato eseguito prima e durante la somministrazione di mdc iodato ev . 
nei pazienti in cui allesame preliminare senza mdc iodato veniva riscontrata una inadeguata distensione del piccolo intestino abbiamo somministrato altri 200250 ml di metilcellulosa prima di procedere allo studio tc con mdc ev . 
questultimo stato acquisito 40 secondi dopo la somministrazione ev di 130150 ml di mezzo di contrasto ( ultravist 370 , schering ag , berlino , germania ) iniettato alla velocit di 3 ml / s . con una computer workstation ( advantage windows , ge medical system ) le immagini assiali sono state rielaborate con ricostruzioni 2d , coronali ed eventualmente sagittali . 
il sondino non stato rimosso al termine dellesame tc e dopo 68 ore tutti i pazienti sono stati studiati con clisma del tenue effettuato secondo il metodo di herlinger [ 4 ] con tecnica digitale . 
sono stati somministrati 200250 ml di una sospensione di solfato di bario ( prontobario 60% , bracco , milano , italia ) seguiti dallinfusione di 10002000 ml ( in media 1200 ml ) allo 0 , 5% di metilcellulosa . 
sono stati eseguiti radiogrammi nelle proiezioni postero - anteriore , antero - posteriore , con e senza compressione delle anse . i risultati dello studio tc e del clisma del tenue sono stati confrontati e valutati da due radiologi esperti in radiologia gastroenterologica . 
abbiamo anche valutato la distensione delle anse del piccolo intestino che per ciascun segmento stata classificata con una scala di 4 punti ( 0 : distensione assente ; 1 : distensione incompleta ; 2 : distensione parziale ; 3 : distensione completa )  . 
le ricostruzioni coronali e sagittali sono state confrontate con le immagini assiali ed abbiamo valutato le eventuali informazioni aggiuntive da esse ottenibili . le immagini ottenute con clisma del tenue sono state analizzate ricercando i seguenti segni : edema delle pliche , erosioni , ulcerazioni aftoidi e lineari , fistole , aspetto ad acciottolato , micronoduli , ispessimenti parietali , dilatazioni prestenotiche , infiammazione mesenterica , altri segni ( aderenze , alterazioni radiologiche sospette per presenza di neoplasia benigna o maligna )  . 
in these loops , wall thickness ranged from 4 mm to 10 mm ( mean 6.5 mm ) , loop diameter was between 12 and 30 mm ( mean 21 mm ) and lumen diameter between 2 and 18 mm ( mean 8 mm )  . 
complete distension was observed in 27 / 45 ( 61% ) patients in the proximal jejunum , in 35 / 45 ( 77% ) in the distal jejunum , in 40 / 45 ( 88% ) in the proximal ileum , in 39 / 45 table 1 ct signs in patients with crohns disease target sign deep ulcers / sinus tracts perienteric stranding comb sign fibrofatty proliferation stenosis fistulas lymphadenopathy ( > 1 cm ) adhesions abscess segno del bersaglio ulcere profonde / sinus tract strie perienteriche segno del pettine proliferazione fibroadiposa stenosi fistole linfoadenopatie ( > 1 cm ) segni indiretti di aderenze ascesso signs sdct ; number of patients mdct ; number of patients sdct , single - detector computed tomography ; mdct , multidetector computed tomography tabella 1 segni tc nei pazienti con morbo di crohn segni tcsd ; numero pazienti tcmd ; numero pazienti tcsd , tomografia computerizzata a singolo detettore ; tcmd , tomografia computerizzata multidetettore 1191 l.m. 
i valori di densit dei segmenti coinvolti ottenuti dallo studio senza contrasto erano compresi tra 16 e 57 hu e il loro livello di enhancement dopo mdc variava tra 82 e 208 hu . 
il segno del bersaglio stato osservato in 14 pazienti , ulcere profonde / sinus tract in 4 , lo stranding perienterico in 13 , il segno del pettine in 7 . 
una completa distensione stata osservata in 27 / 45 ( 61% ) pazienti nel digiuno prossimale , in 35 / 45 ( 77% ) nel digiuno distale , in 40 / 45 ( 88% ) nellileo prossimale , in 39 / 45 ( 86% ) nellileo distale , in 41 / 45 ( 92% ) nellultima ansa ileale . 
5 tc multidetettore : due anse ileali appaiono a pareti ispessite ( frecce nere ) ; limitrofa ad esse ( freccia bianca ) presente formazione ascessuale . ( 86% ) in the distal ileum and in 41 / 45 ( 92% ) in the last ileal loop . 
the three false positive castable 2 degree of small - bowel distension on ct 0 : absent 1 : incomplete 2 : partial 3 : complete pj , proximal jejunum ; dj , distal jejunum ; pi , proximal ileum ; di , distal ileum ; lil , last ileal loop tabella 2 grado di distensione delle anse dellintestino tenue allesame tc 0 : assente 1 : incompleta 2 : parziale 3 : completa dp , digiuno prossimale ; dd , digiuno distale ; ip , ileo prossimale ; id , ileo distale ; uai , ultima ansa ileale 1193 l.m. 
abbiamo quindi riscontrato valori di sensibilit , specificit ed accuratezza diagnostica del 90% , 71% e 89% con tecnica a singolo detettore e del 92% , 83% e del 90% con tecnica multidetettore . 
essa ha confermato i reperti di normalit in 5 pazienti e un morbo di crohn in 20 , un quadro di ileite aspecifica in 1 , ileite da reflusso in 1 e ileite ischemica in 1 . 
i due terzi dei casi di leite aspecifica , diagnosticati dallenteroclisi tc , presentavano endoscopicamente un quadro compatibile con morbo di crohn . small - bowel ct allows visualisation of the entire organ and , with adequate bowel distension and elimination of respiratory and peristaltic artefacts , enables evaluation of the type and luso della tc nello studio del piccolo intestino consente la visualizzazione dellintero organo e , previa unadeguata didiscussione discussion fig . 
8a , b esempio di migliore visualizzazione dellansa patologica ( frecce ) con tecnica multidetettore ( a ) rispetto alla tecnica a singolo detettore ( b )  . extent of mural enhancement after administration of iv iodinated contrast material . 
as with conventional radiology , accurate bowel cleansing is essential for the quality of the study . because wall thickening is a characteristic feature of crohns disease , optimal bowel distension is essential . 
oral contrast agents have the disadvantage of not perstensione delle anse e leliminazione di artefatti respiratori e dei movimenti peristaltici , la valutazione del tipo e dellestensione dellenhancement parietale dopo somministrazione di mdc iodato ev . 
come nella radiologia tradizionale unaccurata pulizia intestinale il requisito fondamentale per questo tipo di studio . lispessimento parietale rappresenta una caratteristica fondamentale della malattia intestinale e per tale motivo essenziale avere la ottimale distensione delle anse . 
ct enteroclysis combines the advantages of ct with those of small - bowel enema into a single technique [ 5 ]  . in 1992 , klppel [ 6 ] conducted the first study of ct enteroclysis in small - bowel inflammatory diseases , highlighting the techniques diagnostic accuracy in evaluating mucosal abnormalities , mural thickening , fistulas and extraintestinal complications . clinical suspicion guides the choice of contrast material . it is generally preferable to use hypodense contrast agents , except in patients with intestinal obstruction , in whom positive agents are found to be more useful [ 5 , 6 ]  . 
hypodense contrast agents provide better depiction of the inner aspect of the bowel loop , allowing evaluation of the type of mural enhancement after iv administration of iodinated contrast material . 
because no infusion pump was available , we administered the contrast agent manually , trying to ensure a steady and continuous infusion . the examination was carried out after completing the methylcellulose infusion . 
moreover , to ensure uniform loop distension and reduce patient discomfort , we administered two doses of iv smooth - muscle relaxant : the first dose was given before the infusion of approximately 11.5 l of methylcellulose to reduce patient discomfort , the second just il primo requisito quindi per un ottimale studio tc ottenere unadeguata distensione del lume mediante unoculata scelta del tipo e della modalit di somministrazione del mezzo di contrasto . 
i mezzi di contrasto somministrati per via orale hanno lo svantaggio di non fare ottenere una uniforme distensione delle anse del piccolo intestino ; tale problema superato con lutilizzo dellenteroclisi tc , caratterizzata tuttavia da invasivit , tempo e costi maggiori . 
kloppel nel 1992 [ 6 ] ha realizzato il primo studio sulla tc enteroclisi nelle malattie infiammatorie dellintestino tenue mettendo in risalto laccuratezza diagnostica di questa tecnica nella valutazione delle alterazioni della mucosa , dellispessimento parietale , delle fistole e delle complicanze extra - intestinali . 
in tutti i pazienti preferibile lutilizzo di mezzi di contrasto ipodensi eccetto che per i pazienti con ostruzione intestinale nei quali un mezzo di contrasto positivo pi utile [ 5 , 6 ]  . 
un mezzo di contrasto ipodenso consente una migliore definizione dellaspetto interno dellansa intestinale , specialmente per valutare il tipo di enhancement parietale dopo la somministrazione di mdc iodato ev [ 7 ]  . 
essa ben conosciuta , sicura , non tossica , largamente utilizzata nello studio tradizionale e non viene assorbita per cui si evita il rischio di emodiluizione ; ha allincirca la stessa densit dellacqua , quindi determina un ottima differenza di contrasto tra il contenuto delle anse intestinali e lenhancement della parete intestinale . 
nei casi in cui le scansioni di base senza mdc iodato documentavano una scarsa distensione delle anse , stata somministrata unulteriore dose di metilcellulosa prima di procedere con linfusione di mdc iodato . 
inoltre , per ottenere unomogenea distensione delle anse e ridurre il disagio al paziente abbiamo somministrato ev due dosi di ipotonizzante : la prima dose stata somministrata dopo linfusione di circa 11 , 5 l di metilcellulosa in modo da ridurre il discomfort del paziente , la seconda subito prima dellesame tc . 
in tal modo abbiamo ottenuto una distensione completa del digiuno prossimale nel 61% dei pazienti , del digiuno distale nel 77% , dellileo prossimale nell88% , dellultima ansa ileale nel 92% . 
anche se la distensione delle anse migliore quando viene usata una pompa peristaltica [ 8 , 9 ] , in accordo con quanto evidenziato in letteratura [ 10 , 12 ] riteniamo possibile ottenere una sufficiente distensione delle anse anche con linfusione manuale del mezzo di contrasto . un altro elemento indispensabile per lo studio tc del morbo di crohn la somministrazione ev del mezzo di contrasto iodato . 
non tutti gli autori sono concordi sul tempo di attesa dopo la somministrazione del mezzo di contrasto iodato : alcuni ritengono utile unacquisizione arteriosa precoce ( 25 s ) [ 8 ] o arteriosa tardiva 1197 l.m. 
10a , b allesame tc a singolo detettore ( a ) evidente ispessimento parietale dellultima ansa ileale ( freccia ) ; nel clisma del tenue ( b ) essa non dissociabile dalle anse vicine . before starting the ct study . 
this enabled us to achieve complete distension of the proximal jejunum in 61% of patients , of the distal jejunum in 77% , of the proximal ileum in 88% and of the last ileal loop in 92% . 
even if loop distension is improved by the use of a peristaltic pump [ 8 , 9 ] , in agreement with the literature [ 10 , 12 ] , we believe adequate bowel distension can also be achieved by manual injection of the contrast agent . another fundamental aspect of the ct study of crohns disease is the iv administration of iodinated contrast material . 
not all authors agree on the timing of the scan after contrast administration : some prefer an early arterial acquisition ( 25 s ) [ 8 ] or late arterial acquisition ( 40 s ) [ 9 , 13 ] , whereas other prefer a portal phase ( 6070 s ) [ 14 ]  . 
in our study we decided to perform a single acquisition 40 s after iv administration of contrast material , because we preferred to study the small - bowel loops in the arterial phase . during acute inflammation , the thickened bowel wall often shows the so - called target sign , characterised by the alternation of concentric highand low - attenuation rings , on postcontrast images . 
the target sign was originally attributed to crohns disease but is now regarded as a nonspecific sign [ 14 ] ; the differential diagnosis includes crohns disease , ischaemia , infectious enteritis , actinic enteritis , vasculitis and graft - versus - host dis1198 ( 40 s ) [ 9 , 13 ] , altri prediligono una fase portale ( 6070 s ) [ 14 ]  . 
noi abbiamo deciso di realizzare una singola acquisizione a 40 s dalla somministrazione ev di mdc , poich abbiamo preferito effettuare uno studio delle anse dellintestino tenue in fase arteriosa . quando presente uninfiammazione acuta , la parete intestinale ispessita spesso mostra dopo iniezione endovena del mdc iodato il cosiddetto segno del bersaglio ( target sign ) caratterizzato dallalternanza di anelli concentrici ad alta e bassa densit . 
laspetto a bersaglio era originariamente attribuito al morbo di crohn , ma oggi si ritiene essere un segno aspecifico [ 14 ] ; la diagnosi differenziale include : malattia di crohn , ischemia , enteriti infettive , enteriti attiniche , vasculiti e grast - versushost - disease . 
il segno del pettine ( comb sign ) si evidenzia come una ipervascolarizzazione del mesentere coinvolto che si manifesta sotto forma di dilatazione arteriosa mesenterica , tortuosit , prominenza e dilatazione dei vasi retti [ 14 ]  . 
tale segno stato osservato in 7 pazienti del nostro studio . nonostante gli sviluppi tecnologici , per la nostra esperienza ancora utile la combinazione dello studio tc enteroclisi con il tradizionale clisma del tenue . 
the comb sign reflects hypervascularity of the involved mesentery , which manifests as mesenteric arterial dilatation , tortuosity , prominence and dilatation of the vasa recta [ 14 ]  . 
the comb sign was seen in seven patients in our study . despite technological advances , we find the combination of ct enteroclysis and conventional barium enema to be still useful , as it produces a better diagnostic definition , allowing identification of false positive and false negative cases on ct [ 9 , 16 , 17 ]  . 
moreover , the conventional study proved superior in characterising mucosal abnormalities , especially in the early phase , and complemented the ct findings , allowing for a diagnosis of reflux ileitis and ischaemic ileitis in two cases . 
abscesses were present in 2 / 45 patients , fistulas in 3 / 45 , perienteric stranding in 13 / 45 and fibrofatty proliferation in 5 / 45 . with regard to the comparison between the two ct techniques , it should be stressed that , as expected , the multidetector technique allowed for shorter scan times and reduced respiratory artefacts and patient discomfort while providing better spatial resolution and better depiction of pathological patterns . 
however , sensitivity , specificity and diagnostic accuracy of the two techniques are similar ( table 4 ) , as a result of the fact that both techniques are able to demonstrate the typical signs of disease , even though their visualisation is better with the multidetector technique . 
in our study , mpr did not , however , reveal any abnormalities that had not already been demonstrated in the axial scans , although they significantly increased our confidence in image interpretation and helped us better evaluate the longitudinal extent of intestinal involvement , as previously reported in the literature [ 19 , 21 ]  . 
the coronal images , especially with those obtained with the multidetector technique , were particularly well accepted by the clinicians and surgeons , given their familiarity with frontal views . even though crohns disease is the most common disease of the small bowel , we should not forget that ct enteroclysis is able to detect other pathological conditions , such as neoplasms . 
in our study , we found only two cases of carcinoid tumour , probably as a result of the preliminary clinical selection of patients with suspected or known crohns disease . 
 in conclusion , we believe that mdct should be preferred to sdct owing to its better spatial resolution and because it ne produce una migliore definizione diagnostica permettendo di identificare i casi tc falsi positivi e falsi negativi [ 9 , 16 , 17 ]  . 
nel nostro studio , infatti , 3 falsi positivi erano dovuti a scarsa distensione delle anse e 4 falsi negativi erano dovuti ad una fase iniziale di malattia e / o localizzazione prossimale di crohn . 
ascessi erano presenti in 2 / 45 pazienti , fistole in 3 / 45 , stranding perienterico in 13 / 45 , proliferazione fibroadiposa in 5 / 45 . per quanto riguarda il confronto tra le due tecniche tc vogliamo sottolineare che , come atteso , la tecnica multidetettore ha ridotto i tempi di scansione , gli artefatti respiratori e il disagio per il paziente , permettendo una migliore risoluzione spaziale e realizzando una migliore rappresentazione degli elementi patologici . 
tale dato in accordo con la letteratura [ 1517 , 19 , 20 ] .tuttavia i valori di sensibilit , specificit ed accuratezza diagnostica sono simili con le due metodiche ( tabella 4 )  . 
tuttavia le ricostruzioni multiplanari non hanno nel nostro studio mostrato alcuna alterazione che non fosse gi stata documentata nelle scansioni assiali anche se hanno migliorato significativamente la nostra confidenza nella interpretazione delle immagini e ci hanno aiutato a valutare meglio lestensione longitudinale dellinteressamento intestinale , come gi riportato in letteratura [ 19 , 21 ]  . 
le immagini coronali sono state inoltre particolarmente apprezzate dai clinici e dai chirurghi data la loro familiarit con esse , in particolare quelle ottenute con tecnica multidetettore . anche se il morbo di crohn la patologia dellintestino tenue pi frequente , non dobbiamo dimenticare che la tc enteroclisi in grado di documentare altre condizioni patologiche , come ad esempio le neoplasie . 
nel nostro studio abbiamo riscontrato solo due casi di carcinoide verosimilmente in rapporto alla preliminare selezione clinica che ci ha fatto studiare prevalentemente pazienti con sospetto o noto morbo di crohn . in conclusione noi riteniamo che la tcmd enteroclisi sia da preferire alla tcsd per la sua migliore risoluzione spaziale e perch consente una migliore rappresentazione dei segni patologici di malattia di crohn . 
in our opinion , in selected patients ( nondiagnostic ct , negative ct with a strong clinical suspicion of small bowel disease ) , ct findings still need to be combined with those from small - bowel enema to obtain all the information needed for a correct diagnosis and for planning treatment in patients with crohns disease . 
the ultimate goal is to improve visualisation of early lesions with ct in order to obtain all the necessary information for correct patient evaluation with a single examination . nione i dati tc ancora necessitano in pazienti selezionati ( tc non diagnostica , tc negativa con quadro clinico altamente suggestivo di patologia dellintestino tenue ) di essere combinati con quelli derivanti dal clisma del tenue in modo da ottenere tutte le informazioni necessarie per la corretta diagnosi e la pianificazione terapeutica dei pazienti con malattia di crohn . 
fourteen patients ( nine men and five women , mean age 49 years , range 2266 years ) underwent an mr examination on a 1.5 - t systeseven patients had a history of hypertension or crf , one had takayasu disease and one had nephrovascular hypertension . 
the imaging protocol consisted of t1and t2 - weighted sequences followed by a se - epi acquisition with a diffusion gradient of 600 s / mm2 and sense factor 2 and pixel - by - pixel adc map reconstruction . 
further studies with scintigraphic correlation are needed to confirm these results and to establish reference values for this imaging technique . key words magnetic resonance imaging diffusion - weighted imaging kidney glomerular filtration rate riassunto scopo . 
quattordici pazienti ( 9 maschi e 5 femmine , et media 49 anni , range 2266 ) sono stati sottoposti ad esame rm con sistema ad alto campo 1 , 5 t ; in 5 pazienti non vi erano dati anamnestici e bioumorali di nefropatia , mentre in 7 era presente storia di ipertensione arteriosa e / o irc ingravescente , in 1 di malattia di takayasu e in 1 di ipertensione nefrovascolare . 
il protocollo prevedeva acquisizioni t1 e t2 dipendenti , nonch una sequenza seepi pesata in diffusione ( b - factor 600 s / mm2 ) con fattore sense 2 e ricostruzione di mappe delladc . 
non stata rilevata una differenza significativa delladc tra stadio i e stadio ii ( p = 0 , 27 ) e tra stadio ii e stadio iii ( p = 0 , 39 ) , mentre la differenza stata significativa tra pazienti in stadio iii e iv ( p < 0 , 01 )  . 
si rilevata una significativa correlazione tra la clearance della creatinina ( clcr ( cg ) ) e l adc parenchimale ( r = 0 , 79 ; p < 0 , 01 )  . 
la rm - dw permette di ottenere valori quantitativi del coefficiente di diffusione correlabili con la funzione renale separata , senza somministrare mezzo di contrasto e con rapidi tempi desame . ulteriori studi di correlazione con i dati scintigrafici e su pi ampie casistiche sono necessari al fine di confermare tali risultati e stabilire valori di riferimento per questa metodica . parole chiave risonanza magnetica diffusione reni filtrato glomerulare 1201 s.f. 
this impact on health and health care costs increases at least tenfold if the increased risk of cardiovascular disease among patients with kidney disease is taken into account , as this condition is the main cause of death among this population [ 2 ]  . 
whereas haemodialysis and transplant are expensive but necessary forms of therapy in the terminal phase , prevention of endstage renal failure through an attempt to slow down the progression of kidney damage is undoubtedly useful for the prognosis and management of these patients , especially considering that patients on dialysis have a mortality rate ten times greater than patients with kidney disease not undergoing dialysis [ 2 ]  . 
the therapy to adopt , therefore , needs to be based on the correct identification of patients at risk and procedures for assessing response to therapy that are minimally invasive , relatively simple and repeatable and obviously sensitive to the slightest alteration in kidney function . in addition to biochemical markers , numerous recent studies have investigated the potential of imaging techniques , and especially magnetic resonance imaging ( mri ) , in the assessment of early renal damage [ 37 ]  . 
 the technique of diffusion - weighted imaging ( dwi ) , through the use of sequences highly sensitive to proton motion such as single - shot echoplanar imaging ( ss - epi ) sequences , is capable of measuring the diffusion of water protons in the extracellular compartments and therefore proton motion in the tubular system of the kidneys [ 8 ]  . 
this measurement was made possible by using the appropriate gradient pulses ( or b factor ) [ 9 ] : the greater the motion of water molecules , the greater the decrease in signal , which can be used to quantify the apparent diffusion coefficient ( adc ) , which is measured in millimetres per second2 . 
the shortcomings of these sequences include a low signal - to - noise ratio ( snr ) , low spatial and contrast resolution and the need for relatively long echo time ( te ) [ 10 ]  . 
in addition , they are relatively sensitive to off - resonance effects , such as an inhomogeneous field , magnetic susceptibility and chemical shift , features that are often present in abdominal imaging [ 11 ]  . 
this technology , which is based on the subdivision of the signal originating from arrays of multiple receiver coils and the determination of sensitivity maps , is capable of reducing the gradient echo train and accelerating the filling of the k - space . 
the resulting increase in bandwidth per pixel in the direction of the phase encoding and reduction in the epi factor produce a net increase in image quality [ 12 ]  . with regard to the kidneys , a number of studies reported significantly reduced diffusion coefficients in the case of acute and crf ; in particular , the adc of the cortex appears to be strongly correlated with creatininaemia [ 813 ]  . the aim of the present study was to assess the adc para1202 la prevalenza dellinsufficienza renale cronica ( irc ) notevolmente aumentata negli ultimi decenni , con un significativo incremento dei costi relativi alla dialisi ed ai trapianti renali , corrispondenti secondo alcune recenti fonti a circa il 2% del budget sanitario annuo in europa [ 1 ]  . 
tale impatto sulla salute e sui costi sanitari viene poi almeno decuplicato dallaumentato rischio di patologie cardiovascolari documentato nei pazienti nefropatici , che sono le principali cause di mortalit in questa popolazione [ 2 ]  . 
se lemodialisi ed il trapianto sono le misure terapeutiche dispendiose ma necessarie nella fase terminale , per la prognosi di questi pazienti e per il loro management complessivo sicuramente utile la prevenzione dellirc terminale cercando di ridurre la velocit di progressione del danno renale , soprattutto se si tiene presente che i pazienti dializzati hanno un tasso di mortalit dieci volte superiore ai nefropatici non dializzati [ 2 ]  . 
lapproccio terapeutico deve quindi fare seguito alla corretta identificazione dei pazienti a rischio e allindividuazione di procedure di valutazione della risposta terapeutica che siano scarsamente invasive , relativamente semplici e ripetibili e , ovviamente , sensibili alle minime modificazioni della funzione renale . oltre i markers bioumorali , a tale scopo numerosi studi sono stati compiuti negli ultimi anni per indagare le potenzialit delle tecniche di imaging e soprattutto della risonanza magnetica ( rm ) nella valutazione del danno renale precoce [ 37 ]  . in particolare la tecnica di diffusione ( diffusion - weighted imaging , dwi ) consente attraverso lutilizzo di sequenze particolarmente sensibili a movimenti protonici , come le sequenze echo - planari single - shot ( ss - epi ) , di misurare la capacit di diffusione dei protoni di acqua nei compartimenti extracellulari e quindi , a livello renale , soprattutto dei movimenti protonici del sistema dei tubuli [ 8 ]  . 
tale misurazione resa possibile utilizzando impulsi di gradienti di campo appropriati ( o b - factor ) [ 9 ] : tanto pi vi movimento protonico maggiore sar il decremento di segnale , dal quale si pu ottenere una vera e propria quantificazione del coefficiente di diffusione ( apparent diffusion coefficient , adc ) , misurabile in mm2 / s . 
il limite di tali sequenze sta nel basso rapporto segnale - rumore , nella bassa risoluzione spaziale e di contrasto , nonch nella necessit di utilizzare te relativamente lunghi [ 10 ]  . 
inoltre esse presentano una elevata sensibilit agli effetti tipo off - resonance , come inomogeneit di campo , suscettibilit magnetica e chemical - shift , spesso frequenti nellimaging addominale [ 11 ]  . 
five underwent abdominal mr to characterise hepatic lesions and , as they showed no significant serum creatinine alterations and had no history of risk factors for kidney disease , were enrolled in the study as healthy controls . 
in base a questa equazione , i 9 pazienti con positiva anamnesi per patologia renale o comunque con fattori predisponenti , sono stati cos classificati : 4 in stadio 1 , 2 stadio 2 , 1 in stadio 3 e 2 in stadio 4 . 
in fase di post - processing , sono state ottenute automaticamente delle mappe di diffusione , applicando la relazione di le bihan modificata per il calcolo del coefficiente apparente di diffusione adc pixel - per - pixel : adc = ( lg si0 - lgsi1 ) / b1 - b0 [ 15 ] dove si0 e si1 sono le intensit di segnale misurate nelle immagini corrispondenti ai fattori di diffusione rispettivamente b0 e b1 . 
on the basis of this equation , the nine patients with a positive history of renal disease or predisposing factors were classified as follows : four in stage 1 , two in stage 2 , one in stage 3 and two in stage 4 . 
during the postprocessing phase , diffusion maps were automatically obtained by applying the le bihan equation modified for the calculation of the pixel - by - pixel adc : adc = ( lgsi0 - lgsi1 ) / b1 - b0 [ 15 ] where si0 and si1 are the signal intensities measured on 1204 s.f. 
nei 9 pazienti con fattori di rischio per danno renale , classificati in stadio 14 secondo lequazione di cockroft - gault , i valori di gfr erano compresi tra 215 , 23 e 19 , 46 ml / min . i dati relativi ai valori di diffusione ( adc ) nella popolazione esaminata sono riassunti nella tabella ( tabella 2 )  . 
il parametro diffusione prima e dopo somministrazione di furosemide non ha mostrato significative variazioni ( p = 0 , 7 ) ; in particolare la somministrazione di furosemide ha determinato una riduzione della correlazione lineare tra adc e clcr ( cg )  . 
a region of interest ( roi ) was then manually placed along the borders of each kidney to exclude the renal sinus in the reference se - epi images ( b = 0 )  . 
dw acquisition obtains a reference image with b = 0 s / mm2 ( a ) and an isotropic image with b = 600 s / mm2 ( b ) , based on which an apparent diffusion coefficient ( adc ) map can be calculated ( c )  . 
lacquisizione pesata in diffusione permette di ottenere unimmagine di riferimento ( a ) con b = 0 e limmagine ottenuta con b = 600 s / mm2 ( b ) , a partire dalle quali possibile calcolare una mappa delladc ( c )  . 
in patients with documented kidney damage , no significant difference was measured in terms of adc between stages 1 and 2 ( p = 0.27 ) or stages 2 and 3 ( p = 0.39 ) , whereas a marked difference in parenchymal diffusion was limpatto della terapia sulla progressione della irc fortemente influenzato dalla individuazione precoce del danno parenchimale renale e delle sue incipienti ripercussioni sulla funzione dorgano . 
tale applicazione stata resa possibile dallo sviluppo di sistemi ad elevati gradienti di campo oltre che ad alto campo magnetico stazionario , a cui si associata una significativa evoluzione tecnologica delle bobine e delle sequenze cosiddette veloci . 
tra le sequenze che sfruttano le possibilit intrinseche della risonanza di produrre contrasto tra differenti tessuti , una tecnica molto promettente in ambito addominale e di rapida acquisizione il dwi [ 1518 ]  . 
esso sfrutta la capacit della rm di produrre e misurare il movimento dei protoni liberi di acqua nei tessuti , dipendente da numerosi fattori , tra cui principalmente la presenza di barriere ( membrane cellulari , accumulo di matrice extra - cellulare , ecc )  . 
there were no significant variations in adc values before and after administration of furosemide ( p = 0.7 ) ; in fact , the administration of furosemide caused a reduction in the linear correlation between adc and clcr ( cg )  . 
this application has been made possible by the development of systems with high field gradients and high static magnetic fields , together with a significant technological development of coils and so - called fast sequences . 
the latter offer a variety of possibilities for the assessment , at least theoretically , of functional renal parameters , such as renal blood flow and gfr , by exploiting the intrinsic characteristics of mr contrast resolution or by using paramagnetic contrast agents similar to inulin [ 7 ]  . 
included among the sequences that exploit the intrinsic possibilities of resonance to produce contrast between different tissues is dwi , a fast technique that has proved highly promising in abdominal imaging [ 15 , 1618 ]  . 
6a - c bowel gas produces a magnetic susceptibility artefact in the inferior pole of the left kidney , both in the reference image with b = 600 s / mm2 diffusion - weighted and in the apparent diffusion coefficient map ( arrows )  . 
6a - c artefatto da sensibilit alla suscettibilit magnetica a livello del polo inferiore del rene sinistro , causato dalla presenza di aria colica presente sia nellimmagine di riferimento e con b = 600 s / mm2 che nella mappa delladc ( frecce )  . 
it has been shown that the b value negatively influences the snr of the image , even though it does render the sequence less sensitive to the motion of capillary flow and breathing ( or pseudodiffusion ) [ 16 ]  . 
this obtained a mean adc value in the healthy subjects and those in stage 1 ( only the presence of risk factors ) of 2.440.2410 - 3 mm2 / s , which is in line with the figures reported in the literature . 
in patients with kidney damage documented by a reduction of clcr ( cg ) , there was a progressive and significant reduction in adc ( p < 0.01 ) , with significant changes between stages 3 and 4 . 
 [ 13 ] identified a linear correlation between creatininaemia and adc ( r = 0.75 ) in the cortex and a significant but weaker correlation in the medulla ( r = 60 ) , whereas a recent preliminary study showed a significant difference between renal adc in healthy volunteers and in patients affected by crf ( p < 0.01 ) [ 8 ]  . 
though conducted on a small population , our study indicates that adc can be used as a parameter for renal damage , as it is capable of distinguishing between patients with parenchymal damage and patients with initial damage , as well as between patients in stage 3 and patients in stage 4 , although standard reference values are to be hoped for . 
in this sense , a technical standard for the acquisition appears unrealistic , given the marked 1208 diente di diffusione utilizzato ( 5001300 s / mm2 ) [ 13 , 17 , 1921 ]  . 
noto che questultimo parametro influenza negativamente il segnale / rumore dellimmagine , anche se rende meno sensibile ai movimenti da flusso capillare o respiro ( o pseudodiffusione ) la sequenza [ 16 ]  . 
in questa ottica abbiamo utilizzato un elevato fattore b di 600 s / mm2 associato ad una acquisizione in respiro sospeso , in modo da mantenere un adeguato segnale / rumore , ottenendo un valore medio di adc nei soggetti sani ed in quelli in stadio i ( presenza di soli fattori predisponenti ) di 2 , 440 , 2410 - 3 mm2 / s , in linea con quanto riportato in letteratura ; nei pazienti con danno renale documentato dalla riduzione della clcr ( cg ) si assistito ad una progressiva e significativa riduzione delladc ( p < 0 , 01 ) con modificazioni significative tra iii e iv stadio . 
 [ 13 ] hanno evidenziato una correlazione lineare tra creatininemia e adc ( r = 0 , 75 ) della corticale renale e significativa ma meno marcata con la midollare ( r = 0 , 60 ) , mentre un recente studio preliminare ha evidenziato una significativa differenza tra adc renale in volontari sani ed in pazienti affetti da irc ( p < 0 , 01 ) [ 8 ]  . 
lutilizzo della furosemide per uno studio dinamico in diffusione non ha apportato sostanziali vantaggi nei pazienti in cui stato effettuato : non abbiamo infatti riscontrato alcuna differenza in termini di adc nelle acquisizioni pree post - furosemide ( p = 0 , 7 ) , in linea con quanto peraltro gi segnalato in letteratura [ 22 ]  . 
per quanto limitata dalla esiguit della casistica , la presente esperienza indica che ladc pu essere utilizzato come parametro di danno renale , in quanto capace di distinguere i soggetti con danno parenchimale da quelli con danno iniziale e quelli in stadio 3 dai soggetti in stadio 4 , anche se valori di riferimento standardizzati sarebbero auspicabili . 
morphological findings on t1and t2 - weighted images ( a , b ) show a right renal volume reduction with lower cortical - to - medullar differentiation more evident on t1 ( b )  . 
le acquisizioni morfologiche preliminari t1 e t2 pesate ( a , b ) documentano una riduzione del volume del rene destro con minore differenziazione cortico - midollare , pi marcata in t1 ( b )  . 
the assessment of standardisation parameters in the context of the chosen technique could be the aim of future studies . the incidence of artefacts , particularly those caused by magnetic susceptibility related to the presence of the vertebral column or bowel gas , was decidedly low in our study , thanks to the sequence characteristics used and the particular application of sense technology , with a consequent reduction in off - resonance artefacts related to epi . 
this fact , which has already been emphasised in several studies of the brain [ 23 ] , was recently reported in a study of the abdomen , where parallel imaging was also associated with the use of the diffusion tensor with a significant increase in signal [ 8 ]  . overall , our data confirm the possibility of using the technique to assess renal function , above all , with reference to the functioning of a single kidney . 
questo dato , gi sottolineato in alcuni studi sul distretto encefalico [ 23 ] , stato riportato in ambito addominale in un recente lavoro , nel quale limaging parallelo peraltro associato alluso del tensore di diffusione , con un importante aumento del segnale [ 8 ]  . nel complesso i dati ottenuti confermano le possibilit di tale metodica nella valutazione della funzione renale , soprattutto in riferimento a quella del singolo rene . 
further studies are required to standardise both the technique , particularly in dwi , and the calculation , as well as to validate clinical indications on larger patient samples . i dati presenti in letteratura ed i risultati del presente studio consentono di proporre la rm in diffusione del rene come metodica di riferimento per una corretta valutazione dei parametri di funzione parenchimale in associazione ad una elevata accuratezza di valutazione morfologica sia del parenchima che dellasse vascolare . 
taouli b , martin aj , quayyum a et al ( 2004 ) parallel imaging and diffusion tensor imaging for diffusion weighted mri of the liver : preliminary experience in healthy volunteers . 
mc cullough pa ( 2003 ) beyond serum creatinine : defining the patient with renal insufficiency and why ? rev cardiovasc med 4 [ suppl 1 ] : s2s6 15 . 
bammer r , feeling sl , augustin m et al ( 2001 ) improved diffusion - weighted single - shot echo - planar imaging ( epi ) in stroke using sensitivity encoding ( sense )  . 
bartolozzi1 1division of diagnostic and interventional radiology , 2division of pathology , university of pisa , via roma 67 , i - 56100 pisa , italy 3azienda ospedaliera universitaria pisana , pisa , italy correspondence to : c . 
fifty - five patients with mammographic microcalcifications classified as bi - rads categories 3 , 4 or 5 underwent mri and biopsy with stereotactic vacuum - assisted biopsy ( vab )  . 
mri was performed with a 1.5 - tesla ( t ) unit , and t1 coronal three - dimensional ( 3d ) fast low - angle shot sequences were acquired before and after injection of paramagnetic contrast agent ( 0.1 mmol / kg )  . 
lesame rm stato eseguito con una unit da 1 , 5 tesla e sono state acquisite sequenze coronali t1 3d fast lowangle shot sequences prima e dopo liniezione di mezzo di contrasto paramagnetico ( 0 , 1 mmol / kg )  . 
lesame istologico ha rilevato 26 cancri duttali in situ ( cdis ) e cancri duttali microinvasivi ( cd mic ) , 3 iperplasie duttali atipiche ( ida ) e 26 condizioni benigne . 
la sensibilit della mammografia risultata 77% , la specificit stata 59% , il valore predittivo positivo ( vpp ) 61% , il valore predittivo negativo ( vpn ) 74% , laccuratezza diagnostica 67 , 2% . 
la sensibilit globale della rm stata 73% , la specificit 76% , il valore predittivo positivo ( vpp ) 73% , il valore predittivo negativo ( vpn ) 76% , laccuratezza diagnostica 74 , 5% . 
during the last 20 years , the prevalence of dcis has grown from less than 5% before the start of mammographic screening to 15%30% in women regularly checked with mammography [ 6 ]  . 
the 30%50% decrease in mortality is related to early diagnosis and correct management [ 7 ]  . mammography has high sensitivity and low specificity , the positive predictive value ( ppv ) being 15%30% for malignant nonpalpable lesions [ 6 ]  . 
recent studies have shown that breast magnetic resonance imaging ( mri ) with intravenous contrast injection has outstanding sensitivity for the diagnosis of invasive carcinomas ( 88%100% ) and a high negative predictive value ( npv ) [ 6 ]  . 
 considering that dcis is multifocal in more than 50% of cases and bilateral in about 30% of patients [ 1 , 15 ] , and also considering that the possible evolution into an infiltrating form depends on the histological subtype and size and adequacy of resection [ 16 , 17 ] , mri could help in early diagnosis and surgical planning , giving useful information about disease extension [ 14 ]  . 
the aim of our study was to evaluate the role of mri in patients with breast imaging reporting and data systems ( bi - rads ) 35 microcalcifications . la dimostrazione di microcalcificazioni spesso il solo segno del tumore , essendo il primo indizio riscontrato alla mammografia in circa il 70% dei carcinomi duttali in situ ( dcis ) [ 15 ]  . 
durante gli ultimi venti anni , la prevalenza del dcis cresciuta da meno del 5% prima dellinizio dello screening mammografico al 15%30% nella popolazione esaminata regolarmente con la mammografia [ 6 ]  . 
la riduzione della mortalit del 30%50% in relazione con la diagnosi precoce e con il corretto trattamento [ 7 ]  . la mammografia ha un alta sensibilit ed una bassa specificit , infatti il valore predittivo positivo ( vpp ) del 15%30% per le lesioni maligne non palpabili [ 6 ]  . 
recenti studi hanno dimostrato che la risonanza magnetica della mammella ( rm ) con somministrazione di mezzo di contrasto per via endovenosa , ha una notevole sensibilit nella diagnosi del carcinoma invasivo ( 88%100% ) ed un alto valore predittivo negativo ( vpn ) [ 6 ]  . 
invece dimostrata lutilit della rm nella pianificazione chirurgica [ 14 ]  . considerando che il dcis multifocale in pi del 50% dei casi , bilaterale in circa il 30% delle pazienti [ 1 , 15 ] e che la possibile evoluzione in una forma infiltrante dipende dal sottotipo istologico , dalle dimensioni e dalladeguatezza della exeresi chirurgica [ 16 , 17 ] , la rm potrebbe essere di aiuto nella diagnosi precoce e nella pianificazione dellintervento , dando informazioni utili sullestensione della malattia [ 14 ]  . lo scopo del nostro studio quello di valutare il ruolo della rm in pazienti con microcalcificazioni birads 35 . materials and methods we selected 55 patients ( age range 3776 years , mean 5611 years ) with bi - rads 35 microcalcifications on mammography who underwent mri and stereotactic biopsy using vacuum - assisted biopsy ( vab ) between november 2002 and november 2004 . 
mammographic magnification was performed in the view that best visualised the microcalcifications , and the microcalcification extension was evaluated in the standard views . all mammograms were evaluated in a blinded fashion by two radiologists with 15 years experience in breast imaging . materiali e metodi abbiamo selezionato 55 pazienti ( et compresa tra 37 e 76 anni , et media 5611 anni ) con microcalcificazioni birads 35 alla mammografia , che si sono sottoposte ad esame rm e a biopsia sotto guida stereotassica con tecnica di retroaspirazione ( vacuum assisted biopsy : vab ) da novembre 2002 a novembre 2004 . 
i reperti controversi sono stati ulteriormente valutati da entrambi i radiologi per raggiungere un consenso . il nostro gold standard stata la microistologia e listologia per le pazienti sottoposte ad intervento chirurgico . 
lo studio rm stato sempre eseguito prima della microistologia . la rm stata effettuata con un apparecchio da 1 , 5 t ( symphony , siemens ) in tutte le pazienti tranne in 6 in cui stata usata una macchina da 1 , 5 t ( ge , medical system )  . tutte le pazienti sono state studiate in posizione prona utilizzando una bobina dedicata per la mammella . 
il protocollo di studio rm ha incluso un sequenza trasversale t1 di localizzazione , una sequenza sagittale t2 con saturazione del grasso ed una sequenza t1 gradient eco 3d - flash ( te 2 , 5 ms , tr 12 , 7 ms , tempo di acquisizione meno di 2 minuti , fa 30 , spessore di strato 3 mm , interslice gap 0 mm , nex 1 , fov 35 , dimensione della matrice 256160 , dimensione del pixel 1 , 41 , 4 ) , con una serie di 6 acquisizione coronali . 
stato usato il gadoteridolo ( prohance , bracco , milano ) come agente di contrasto paramagnetico con boli di iniezione di 0 , 1 mmol / kg di peso corporeo . 
i processi di rielaborazione delle immagini usate sono stati : sottrazione ; ricostruzioni mip ; ricostruzioni mpr ; curve intensit / tempo nella regione di interesse . sono state identificate secondo lo score di fisher 3 tipi di curve . 
i risultati dello studio rm sono stati classificati secondo lo score di fisher in 5 categorie bi - rads : rm 12 ( fisher score 02 ) : negativo - benigno ; rm 3 ( fisher score 3 ) : probabilmente benigno ; rm 45 ( fisher score 48 ) : probabilmente maligno / maligno . sono state eseguite biopsie sotto guida stereotassica usando il mammografo giotto ims equipaggiato con tavolo prono ed un sistema di aspirazione mammotome ethicon endo - surgery ( amburgo ) con ago di 11 gauge ( g )  . 
il materiale stato inviato allesame microistologico in due differenti contenitori separando i frustoli con le microcalcificazioni da quelli senza microcalcificazioni evidenziate dalla radiografia . lintervento chirurgico stato effettuato in quelle pazienti con diagnosi microistologica di malignit o di lesione altamente sospetta . 
mammografia : le proiezioni cranio - caudale ( cc ) e medio - laterale obliqua ( mlo ) mostrano microcalcificazioni nei quadranti superoed infero - esterni birads 4 e 5 . all cases of microcalcifications were classified according to the method proposed by the american college of radiology [ 18 ] , and those classified as bi - rads 35 were selected . controversial findings were re - evaluated by the two radiologists to reach a consensus . 
mri imaging was performed with 1.5 - tesla ( t ) unit ( symphony , siemens ) in all patients but six , who were examined with a 1.5 - t unit ( ge medical system )  . 
the imaging protocol included a transverse t1 localising sequence , a sagittal fat - saturated t2 sequence and a t1 three - dimensional ( 3d ) fast low - angle shot ( flash ) gradient echo ( te 2.5 ms , tr 12.7 ms , acquisition time less than 2 min , fa 30 , slice thickness 3 mm , interslice gap 0 mm , nex 1 , fov 35 , matrix size 256160 , pixel size 1.41.4 ) , with a series of six coronal acquisitions . 
rm : le immagini mpr sagittali ( a ) ed assiali ( b ) e le mip assiali ( c ) evidenziano multiple aree di captazione contrastografica dendritica e nodulare che interessano lintera mammella sinistra . mmol / kg of body weight . 
postprocessing techniques used were : subtraction maximum intensity projection ( mip ) reconstructions multiplanar reformatting ( mpr ) reconstructions time - intensity curves in the region of interest ( roi )  . three types of curves were identified according to fisher score parameters considering enhancement morphology , we identified the following possibilities : absent enhancement , dendritic enhancement , nodular enhancement and coexistence of dendritic and nodular enhancement . 
results of the mri study were classified into five bi - rads categories according to the fisher score : mri 12 ( fisher score 02 ) negative / benign , mri 3 ( fisher score 3 ) probably benign and mri 45 ( fisher score 48 ) : probably malignant / malignant . biopsy was performed under stereotactic guidance using the giotto ims mammography system equipped with a prone table and a mammotome ethicon endo - surgery ( hamburg ) aspiration device with an 11 - gauge needle . 
considerando la difficolt di una valutazione accurata dellestensione del cdis allanatomia patologica , abbiamo diviso la mammella alla mammografia e alla rm in 5 porzioni : quadrante supero - esterno , quadrante supero - interno , quadrante infero - interno , quadrante infero - esterno , regione retroareolare e abbiamo confrontato tumorale evidenziata lestensione dallimaging con lestensione riscontrata allistologia . risultati la microistologia ha riscontrato 26 lesioni maligne , 29 lesioni benigne incluse 3 iperplasie duttali atipiche ( ida ) ( tabella 1 )  . 
la chirurgia eseguita nelle 29 pazienti ( 17 con carcinoma duttale in situ , cdis , 9 con cancro duttale microinvasivo , cdi mic , e 3 con ida ) , ha confermato in tutti i casi i dati microistologici . 
magnetic resonance imaging ( mri ) : regions of interest in the subtracted images show multiple areas of contrast enhancement with types iii and ii time - intensity curves [ breast imaging reporting and data systems ( bi - rads ) 5 ]  . 
rm : regioni di interesse nelle immagini sottratte post - contrastografiche mostrano multiple aree di captazione contrastografica con curve intensit / tempo di tipo ii e iii ( birads 5 )  . 
stata quindi eseguita una mastectomia sinistra e listologia ha rivelato multipli foci di cdis g2 e g3 . material was sent for microhistological evaluation in two separate containers , one containing the specimens with microcalcifications and the other specimens without microcalcifications . 
in consideration of the difficulties in accurately evaluating dcis extent at pathology , we decided to divide the breast at mammography and mri into five portions : upperouter quadrant , upper - inner quadrant , lower - outer quadrant , lower - inner quadrant and retroareolar region ; we compared si e g3 in 11 casi . 
surgery , performed in 29 patients [ 17 with dcis , nine with ductal microinvasive cancer ( dcmic ) and three with adh ] , confirmed the microhistological data in all cases . 
among the 55 patients studied , mammographic findings were classified as birads 3 : 23 cases , bi - rads 4 : 25 cases andbi - rads 5 : seen cases . 
of the 48 patients with mri contrast enhancement , the time - intensity curve correlated with histology was type i in ten benign lesions and one malignant lesion , type ii in nine benign lesions and nine malignant lesions and type iii in four benign lesions and 15 malignant lesions . 
in the 26 cancers , enhancement morphology logia 17 lesioni benigne e 6 maligne , nelle mammografie birads 4 abbiamo riscontrato 11 lesioni benigne e 14 maligne , nelle mammografie bi - rads 5 abbiamo riscontrato 1 lesione benigna e 6 maligne . 
nelle 48 pazienti con captazione contrastografica alla rm , la curva intensit / tempo correlata allistologia era di tipo i in 10 lesioni benigne e in 1 lesione maligna , di tipo ii in 9 lesioni benigne ed in 9 lesioni maligne e di tipo iii in 4 lesioni benigne e 15 lesioni maligne . nelle 7 pazienti che non presentavano captazione di mezzo di contrasto alla rm , 6 casi risultavano allistologia lesioni benigne e 1 caso cdis ( tabella 4 )  . 
nei 26 cancri la morfologia della captazione contrastografica risultata dendritica in 3 casi , nodulare in 8 casi , sia dendritica che nodulare in 14 casi e completamente assente in un caso ( tabella 5 )  . 
dei 9 casi di cdi mic la maggior parte dei casi avevano una captazione sia dendritica che nodulare ( n = 5 ) ; nei restanti casi la captazione era dendritica ( n = 2 ) e nodulare ( n = 2 )  . per quanto riguarda le forme maligne : nel 3 , 8% dei casi non era presente captazione contrastografica , nel 3 , 8% dei casi le curva intensit / tempo erano di tipo i , nel 34 , 6% le curve intensit / tempo erano di tipo ii e nel 57 , 7% di tipo iii . la sensibilit della mammografia stata del 77% ( 20 / 26 ) , la specificit del 59% ( 17 / 29 ) , il valore predittivo positivo ( vpp ) risultato del 63% ( 20 / 32 ) , il vpn del 74% ( 17 / 23 ) , laccuratezza diagnostica risultata del 67 , 2% ( 37 / 55 )  . 
dei 12 casi di falsi positivi in mammografia con bitable 1 histological results tabella 1 risultati istologici histology dcis / dc mic atypical ductal hyperplasia typical ductal hyperplasia fibroadipose tissue sclerosing adenosis fibroadenoma typical epithelium total istologia cdis / cd mic iperplasia duttale atipica iperplasia duttale tipica tessuto fibroadiposo adenosi sclerosante fibroadenoma epitelio tipico totale dcis , ductal carcinoma in situ ; dcmic , ductal microinvasive carcinoma cdis , carcinoma duttale in situ ; cd mic , carcinoma dentale microinvasivo a . 
as regards the nine dc mic , the majority of cases showed both nodular and dendritic enhancement ( n = 5 ) ; in the remaining cases , enhancement was dendritic ( n = 2 ) and nodular ( n = 2 )  . 
among the five false negative cases of mammographic bi - rads category 3 , mri correctly identified three cancers . of the 12 false positive cases of mammographic bi - rads category 45 , mri correctly identified nine benign lesions . however , the fisher exact test did not show a statistically rads 4 - 5 , la rm ha identificato correttamente 9 lesioni benigne . 
per quanto riguarda lestensione della neoplasia , confrontando i reperti mammografici , rm e listologia abbiamo riscontrato : una concordanza dellestensione neoplastica alla rm e allistologia in 22 / 26 casi ( 84 , 6% ) ; una sovrastima della rm in 3 / 26 casi ( 11 , 5% ) ; in 1 / 26 assenza di captazione contrastografica alla rm per cui non stato possibile valutare lestensione della malattia . abbiamo avuto una sottostima dellestensione neoplastica alla mammografia in 16 / 26 ( 73% ) e una corretta valutazioa . 
with regard to disease extension , comparison of mammographic and mri findings with histology found concordance between mri and histological disease extent in 22 / 26 cases ( 84.6% ) ; overestimation at mri in 3 / 26 cases ( 11.5% ) ; and lack of mri contrast uptake in 1 / 26 cases , preventing evaluation of disease extension . 
nellanalisi dellestensione della neoplasia la rm risultata migliore della mammografia ( test z : p < 0 , 01 )  . in tutti i casi eccetto uno ( multicentrico alla rm e multifocale alla mammografia ) lapproccio chirurgico stato deciso in base allesame rm . 
pathology mammography magnetic resonance imaging tabella 8 confrontro tra estensione neoplastica allimaging e in anatomia patologica mammografia risonanza magnetica sottostima rispetto allanatomia patologica sovrastima rispetto allanatomia patologica valutazione corretta rispetto allanatomia patologica on the basis of the mri findings . 
a mammography : craniocaudal and mediolateral oblique views of the left breast show a cluster of microcalcifications [ breast imaging reporting and data systems ( bi - rads ) 4 ] in the upper outer quadrant . 
b subtracted magnetic resonance imaging ( mri ) : dendritic and nodular irregular enhancement with types i and ii time - intensity curves with low increase of contrast enhancement [ breast imaging reporting and data systems ( bi - rads 4 ) ]  . 
a mammografia : le proiezioni cranio - caudale e medio - laterale obliqua della mammella sinistra mostrano un cluster di microcalcificazioni ( birads 4 ) nel quadrante supero - esterno . 
b immagini rm sottratte : irregolare captazione contrastografica dendritica e nodulare con curve intensit / tempo i e ii con basso incremento della captazione contrastografica ( birads 4 )  . 
a mammography : mediolateral oblique view shows microcalcifications in the retro - areolar region [ breast imaging reportingand data systems ( bi - rads ) 5 ] and other foci ( bi - rads 4 ) in the inner and outer quadrants . 
b magnetic resonance imaging ( mri ) maximum intensity projection ( mip ) : coronal and sagittal views show nodular enhancement in the upper quadrants in the para - areolar region of the right breast , associated with vascular asymmetry ipsilateral to the area of enhancement . 
c subtracted magnetic resonance imaging ( mri ) : nodular contrast enhancement with type iii time - intensity curve [ breast imaging reporting and data systems ( bi - rads ) 5 ] , vacuum - assisted biopsy of retroareolar microcalcifications : g3 dcis . 
a mammografia : la proiezione medio - laterale obliqua mostra microcalcificazioni in regione retroareolare ( birads 5 ) ed altri foci ( birads 4 ) nei quadranti infero - esterni . 
b rm : le immagini mip coronali e sagittali mostrano captazione contrastografica nodulare nei quadranti superiori in regione para - areolare nella mammella destra associata ad unasimmetria vascolare ipsilaterale allarea di captazione contrastografica . 
in one case , surgical treatment was planned on the basis of the mammographic findings rather than considering the mri finding of multifocality , and the patient had a recurrence of disease 1 year later . discussion many studies on dynamic mri [ 6 ] have reported high sensitivity values ( 90%100% ) for the diagnosis of invasive carcinoma , with a specificity of 80% [ 14 , 1923 ]  . 
concerning sensitivity and specificity of mri in the diagnosis of dcis and evaluation of isolated microcalcifications , the published values are ( sensitivity : lower and highly variable 33%100% ) [ 21 , 2426 ]  . 
the relatively low number of dcis cases included in the published studies [ 20 , 21 ] seems to be related to the reluctance of investigators to enrol patients with radiological evidence of microcalcifications . 
 the high variability of mri diagnostic accuracy in evaluating microcalcifications reported in the different studies is related to lesion size [ 6 , 27 , 28 ] , histological variability of tumours [ 20 , 24 ] , tumour angiogenesis [ 24 , 29 , 30 ] , criteria for mri evaluation such as type of enhancement , enhancement pattern , distribution in the breast ( multiple foci ) , margins ( regular , irregular ) [ 21 , 24 , 27 , 30 , 31 ] and use of different pulse sequences and scan planes [ 23 ]  . 
 [ 32 ] , for example , in an analysis of morphological and dynamic features of in situ and microinvasive breast cancer on contrast - enhanced mri , detected the typical enhancement criteria in only 50% of cases , without a significant statistical difference in enhancement pattern among the various histological grades of dcis and between pure and microinvasive dcis . 
in our study , the sensitivity of contrast - enhanced mri , according to the fisher score , was higher ( 77% vs . 50% in viehwegs study ) , with only one false negative mri result corrected by mammography . 
however , the false negative ( n = 7 ) and false positive ( n = 7 ) mris strengthen the concept that mammography is the technique of choice for detecting microcalcifications and that stereotactic biopsy is mandatory for characterising bi - rads 35 microcalcifications . 
information from conventional imaging and in particular mammography is useful to avoid mri false negative results . various studies [ 25 , 32 ] suggest a role for contrast - enhanced mri in the detection of dcis , especially for depicting further tumour foci close to or far from the main lesion that are not visible on mammography due to the absence of microcalcifications or masses or distortions [ 33 , 34 ]  . 
at the same time , it is well known that some areas of dcis can be completely noncalcified and that some sites of dcis can contain calcificadiscussione numerosi studi sulla rm dinamica [ 6 ] hanno riportato elevate valori di sensibilit ( 90% - 100% ) nella diagnosi di carcinoma invasivo , con una specificit dell80% [ 14 , 1923 ]  . riguardo alla sensibilit e specificit dellimaging rm nella diagnosi del carcinoma duttale in situ ( cdis ) e nella valutazione delle microcalcificazioni isolate , i valori pubblicati in letteratura sono pi bassi e variabili ( sensibilit : 33%100% ) [ 21 , 2426 ]  . 
il numero relativamente basso di cdis incluso negli studi pubblicati [ 20 , 21 ] sembra da correlare allavversione ad arruolare allesame rm pazienti con evidenza radiologica di microcalcificazioni . lalta variabilit dellaccuratezza diagnostica nella valutazione delle microcalcificazioni , fino ad ora pubblicata in diversi studi , correlata a : dimensioni della lesione [ 6 , 27 , 28 ] , variabilit istologica dei tumori [ 20 , 24 ] , angiogenesi tumorale [ 24 , 29 , 30 ] , criteri di valutazione della rm come tipo e morfologia della captazione contrastografica , distribuzione nella mammella ( foci multipli ) , margini ( regolari , irregolari ) [ 21 , 24 , 27 , 30 , 31 ] e tecnica di risonanza come differenti sequenze e piani di scansioni [ 23 ]  . 
nel nostro studio la sensibilit riportata per la rm dinamica , in accordo allo score di fischer , risultata pi alta ( 77% rispetto al 50% di viehweg ) con un solo caso di falso negativo corretto dalla mammografia . 
tuttavia i falsi negativi ( n = 7 ) e i falsi positivi ( n = 7 ) rafforzano il concetto che la mammografia la tecnica di scelta per individuare le microcalcificazioni e che la biopsia stereotassica obbligatoria per la caratterizzazione delle microcalcificazioni birads 35 . 
informazioni dallimaging tradizionale ed in particolare dalla mammografia sono utili per evitare i falsi negativi della rm . inoltre vari studi [ 25 , 32 ] suggeriscono un ruolo per la rm con somministrazione di mezzo di contrasto nella diagnosi di cdis specialmente per individuare ulteriori foci neoplastici vicini o lontani dalla lesione principale , che non sono visibili alla mammografia per lassenza di microcalcificazioni , masse o distorsioni [ 33 , 34 ]  . 
questi dati sono particolarmente interessanti se consideriamo levidenza di multifocalit ( 53% ) e multicentricit ( 27% ) osservate in pazienti sottoposte a mastectomia [ 30 , 35 ]  . 
la maggior prevalenza di multicentricit osservata nel cdis che nel cdi e la progressione delle forme in situ non adeguatamente trattate in forme di cancro invasivo richiede unaccurata valutazione dellestensione di malattia specialmente in donne candidate a chirurgia mammaria a . 
the higher prevalence of multicentricity observed in dcis than in dci and the progression of inadequately treated dcis into invasive forms require accurate evaluation of disease extension , especially in cases of candidates to breast - conserving surgery [ 36 , 37 ]  . 
even if the biological and clinical impact of these small foci of dcis is uncertain [ 3840 ] , according to the literature [ 41 ] , the risk of local recurrence after conservative therapy is high in patients with large multifocal tumours and low if the multifocal neoplasm is microscopic . furthermore , it is well known that histological measurement of dcis is difficult due to the difficulty in following a duct on serial sections . 
as regards histological grading , increased vascularisation was associated with more greatly differentiated dcis , which are well detected by contrast - enhanced mri , with a high positive predictive value for g3 and g2 forms . 
 even though our study has a selection bias due to the mammographic detection of microcalcifications , our data suggest that the high ppv of mri in g3 dcis can be useful mainly to depict further dcis foci not associated with mammographic signs . 
these data are in keeping with a recent publication [ 21 ] that emphasised the sensitivity of contrastenhanced mri in the detection of high - grade dcis ( g2 and g3 )  . 
however , recent studies have demonstrated that the same genetic profile is correlated with the same histological grade in both in situ and invasive cancers [ 39 , 43 ]  . 
mri could therefore be useful , especially in identifying the most aggressive forms , thereby helping in surgical planning and once the natural course of the disease and the different biological potential of dcis subtypes are better understood possibly in improving the prognosis , as early detection and correct treatment are the most important prognostic factors in breast cancer . conclusions mri cannot be considered a diagnostic tool for evaluating microcalcifications . 
anche se ad oggi limpatto clinico e biologico di questi piccoli foci di cdis incerto [ 3840 ] , in accordo ai dati di letteratura [ 41 ] il rischio di recidiva locale dopo chirurgia conservativa alto nelle pazienti con grossi tumori multifocali e basso se la neoplasia multifocale microscopica . inoltre ben noto che il cdis difficile da misurare istologicamente per la difficolt a seguire un dotto interessato in sezioni seriali . 
per quanto riguarda il grading istologico nella nostra esperienza abbiamo osservato una vascolarizzazione aumentata associata a forme di cdis pi differenziate che sono ben individuate con la rm dinamica , con elevato valore predittivo positivo per le forme g2 e g3 . anche se il nostro studio ha un bias nei criteri di inclusione rappresentato dallindividuazione mammografica delle microcalcificazioni , i nostri dati suggeriscono che lelevato valore predittivo positivo della rm nei casi di cdis g3 pu essere utile soprattutto ad individuare i foci ulteriori di cancro in situ non associati a segni mammografici . 
questi dati sono allineati con una recente pubblicazione [ 21 ] che enfatizza la sensibilit della rm dinamica nella diagnosi delle forme di cancro in situ di alto grado ( g2 e g3 )  . 
cos la rm potrebbe essere utile nell identificare specialmente le forme pi aggressive di cdis aiutando nella pianificazione dellintervento chirurgico e , una volta che siano chiariti il corso naturale della malattia e che i differenti potenziali biologici dei sottotipi di cdis , probabilmente migliorare la prognosi . infatti la diagnosi precoce del cancro mammario ed il corretto trattamento sono i fattori prognostici pi importanti . conclusioni la rm non pu essere considerata lo strumento diagnostico per valutare le microcalcificazioni . 
one hundred and seven patients with a clinical and laboratory suspicion of acute pulmonary embolism who had already undergone chest radiography were divided into four groups according to the time interval between onset of clinical suspicion and performance of the two diagnostic examinations ( 024 h , 2448 h , 048 h , 27 days )  . 
perfusion lung scintigraphy and multislice ct demonstrated elevated concordance if performed within 7 days of the onset of suspicion of acute pulmonary embolisconcordance was higher if the examinations were completed within 2448 h . 
in suspected acute pulmonary embolism , it is mandatory to reach a correct diagnosis within few hours 48 at the most . key words acute pulmonary embolism perfusion lung scintigraphy spiral computed tomography diagnostics of urgency imagings riassunto obiettivo . 
centosette pazienti con sospetto clinicolaboratoristico di epa , che avevano gi eseguito un rx torace , sono stati divisi in 4 gruppi in base allintervallo di tempo tra il sospetto clinico e lesecuzione di entrambe le indagini ( 024 ore , 2448 ore , 048 ore , 27 giorni )  . 
spp e tcsm sono risultate positive in 29 / 107 ( 27 , 1% ) e negative in 78 / 107 ( 72 , 89% ) : concordanza positiva ( cp ) in 22 casi e concordanza negativa ( cn ) in 71 . 
nel sospetto di epa importante effettuare una rapida e corretta diagnosi in poche ore , 48 al massimo . parole chiave embolia polmonare acuta scintigrafia polmonare perfusiva tc spirale multislice diagnostica per immagini durgenza introduction introduzione acute pulmonary embolism ( ape ) is the third most common acute cardiovascular disease after ischaemic heart disease and stroke [ 1 ]  . 
the yearly incidence of ape in western lembolia polmonare acuta ( epa ) rappresenta la terza pi comune patologia acuta dellapparato cardiovascolare dopo la cardiopatia ischemica e lo stroke [ 1 ]  . 
deep vein thrombosis ( dvt ) is the most common cause of pulmonary embolism ; the other principal primary and secondary risk factors are summarised in table 1 [ 2 ]  . 
in spite of the recent important advances in imaging and laboratory diagnostics , approximately 70% of cases of pulmonary embolism are identified at autopsy [ 3 ]  . in cases with an early diagnosis by multislice spiral computed tomography ( msct ) and perfusion lung scintigraphy ( pls ) , anticoagulation therapy proved to be effective in approximately 75% of patients [ 4 ]  . 
thanks to its ability to perform fast subcentimetre acquisitions with optimisation of vascular enhancement after the injection of contrast material , msct permits visualisation of the entire pulmonary artery tree down to the subsegmental level [ 5 ]  . perfusion lung scintigraphy ( pls ) plays an important role in the diagnosis of ape . 
the aim of our study was to compare and integrate the data provided by pls and by msct in cases of emergency diagnoses of ape in nuclear medicine and radiology departments operating around the clock . materials and methods from may 2002 to june 2004 , we retrospectively reviewed 107 consecutive patients ( 50 women and 57 men ) with ages ranging from 20 to 80 years ( mean age 60 + 18 ) , with a clinical and laboratory suspicion of ape . 
the first - level diagnostic approach included an assessment of predisposing factors , primary disease , symptoms ( dyspnoea , chest pain , cough , haemoptysis , syncope ) and clinical signs ( tachypnoea , tachycardia , signs of deep vein thrombosis , fever , cyanosis )  . 
furthermore , all patients had undergone chest radiography before pls and msct . pls was performed with a gamma starcam 4000 xc / t camera ( ge medical systems , west milwaukee , wi , usa ) after administration of 185 mbq of macroaggregated albumin ( number of particles between 300 , 000 and 50 , 000 and diameter from 120 to 70 m ) with 99 mtc . 
all images were acquired with the planar technique in the anterior , posterior , right and left posterior oblique and right and left anterior oblique projections using the following acquisition parameters : 128128 matrix and 500750 kcounts per projection . 
la trombosi venosa profonda ( tvp ) la pi comune causa di embolia polmonare ed i principali fattori di rischio primari e secondari sono riassunti nella tabella 1 [ 2 ]  . 
nonostante gli importanti e recenti sviluppi della diagnostica strumentale e di laboratorio , circa il 70% degli eventi embolici polmonari sono riconosciuti allesame autoptico [ 3 ]  . nei casi diagnosticati tempestivamente con la tomografia computerizzata spirale multistrato ( tcsm ) e con la scintigrafia polmonare perfusiva ( spp ) , il trattamento anticoagulante si dimostrato efficace in circa il 75% dei pazienti [ 4 ]  . pertanto la tcsm si propone come metodica utile nella valutazione del paziente con sospetta epa . 
infatti , la tcsm per la possibilit di eseguire in tempi rapidi acquisizioni subcentimetriche e di ottimizzare lopacizzazione delle strutture vascolari dopo iniezione di mdc , consente di visualizzare le diramazioni dellalbero arterioso polmonare fino al livello subsegmentario [ 5 ]  . la scintigrafia polmonare perfusiva ( spp ) ha un ruolo importante nella diagnosi di epa . 
questa tecnica non invasiva , a bassa dose di radiazioni , consente una valutazione della perfusione ematica polmonare anche in pazienti critici , non collaboranti e portatori di dispositivi metallici [ 6 ]  . 
scopo del nostro studio stato quello di comparare ed integrare i dati forniti dalla spp e dalla tcsm nella diagnosi in urgenza dellepa in centri di medicina nucleare e radiodiagnostica che svolgono indagini urgenti 24 ore su 24 . materiali e metodi nel periodo compreso tra maggio 2002 e giugno 2004 stata eseguita unanalisi retrospettiva che ha portato a selezionare 107 pazienti consecutivi ( 50 donne e 57 uomini ) di et compresa tra i 20 e gli 80 anni ( et media di 6018 ) , con sospetto clinico - laboratoristico di epa . 
per un inquadramento diagnostico in prima istanza sono stati valutati i fattori predisponenti , la patologia di base , i sintomi ( dispnea , dolore toracico , tosse , emottisi , sincope ) e i segni clinici ( tachipnea , tachicardia , segni di trombosi venosa profonda , febbre , cianosi )  . 
i criteri di inclusione sono stati : lesecuzione sia della spp che della tcsm entro 7 giorni dal sospetto clinico - laboratoristico di epa ; non aver intrapreso alcuna terapia trombolitica . 
inoltre , tutti i pazienti avevano eseguito una rx del torace prima della spp e / o della tcsm . la spp stata effettuata utilizzando una gamma camera starcam 4000 xc / t ( ge medical systems , west milwaukee , wisconsin , usa ) previa somministrazione di 185 mbq di macroaggregati di albumina ( numero di particelle variabile da 300000 a 50000 e diametro compreso tra 120 e 70 micron ) marcati con 99 mtc . 
interpretation criteria for pls were those suggested by the prospective investigative study of acute pulmonary embolism ( pisaped ) study , as reported in table 2 [ 7 ]  . msct was considered positive in the presence of eccentric filling defects or of complete occlusion of the pulmonary artery lumen , whether associated or not to the presence of areas of parenchymal hypoventilation . 
all data provided by pls and msct were independently evaluated by two nuclear physicians and two radiologists and included an assessment of which of the two studies had been ordered and performed first . the patients were grouped based on the time interval between the initial clinical suspicion and performance of the two examinations , namely , 024 h , 2448 h , 0 - 48 hours , and 27 days . 
cohens test was used for analysis of concordance between the results of the two investigations , both on the overall patient population enrolled and for the four subgroups ( 024 h , 2448 h , 048 h , 27 days )  . results pls and msct were positive in 29 / 107 ( 27.1% ) cases and negative in 78 / 107 ( 72.89% ) cases , with a positive concordance ( pc ) in 22 cases and negative concordance ( nc ) in 71 ( table 3 )  . 
in the subgroup of patients who had undergone pls and msct within 24 h of the initial clinical suspicion of ape , pls was positive in 12 / 49 ( 24.48% ) cases and negative in 37 / 49 ( 75.51% ) cases , whereas msct was positive in 17 / 49 ( 34.69% ) cases and negative in 32 / 49 ( 65.30% ) cases , with pc in 12 cases ( fig . 1 ) and nc in 32 cases ( table 4 )  . 
furthermore , 35 patients had undergone pls first , and 14 had undergone msct first . in the subgroup of patients who had undergone pls and msct from 24 to 48 h from the first clinical suspicion of ape , pls was positive in 5 / 20 ( 25% ) cases and negative in 15 / 20 ( 75% ) cases , whereas msct was positive in 3 / 20 ( 15% ) cases and negative in 17 / 20 ( 85% ) cases , with pc in three cases and nc in 15 ( table 5 )  . 
moreover , 13 patients had undergone pls first , and seven had undergone msct first . no state acquisite con tecnica planare in proiezione anteriore , posteriore , obliqua posteriore destra e sinistra , obliqua anteriore destra e sinistra utilizzando i seguenti parametri di acquisizione : matrice 128128 e conteggi per proiezione 500750 kcounts . la tc stata effettuata con apparecchiatura tcsm ( mx 8000 , philips medical system , cleveland , ohio , usa )  . 
i parametri di acquisizione utilizzati sono stati i seguenti : collimazione 2 , 5 mm , pitch 1 , 25 , incremento 1 mm , tempo di rotazione 0 , 5 s , kvp / mas - 120 / 100 . 
lesame stato eseguito con paziente in decubito supino e le scansioni sono state condotte dalle cupole diaframmatiche allo stretto toracico superioil mezzo di contrasto uroangiografico ( ultravist 370 , schering , berlin , germania ) stato iniettato nella vena cubitale attraverso un ago da 16 gauge utilizzando un iniettore automatico ( mk - iv , medrad , pittsburgh , pennsylvania , usa ) con i seguenti parametri : volume 8090 ml , flusso 33 , 5 ml / s . 
il ritardo di inizio delle scansioni stato determinato con lesecuzione di un bolus test , ed risultato variabile tra 9 e 15 s ( fase arteriosa polmonare ) , mentre la fase tardiva stata eseguita dopo 4550 s . 
i criteri dinterpretazione per la spp sono quelli proposti dallo studio prospettico pisa - ped e riportati in tabella 2 [ 7 ]  . la tcsm stata considerata positiva in presenza di difetti di riempimento eccentrici o occludenti lintero lume delle arterie polmonari , associati o meno alla presenza di aree dipoventilazione parenchimale . 
tutti i dati forniti dalla spp e dalla tcsm sono stati valutati indipendentemente da due medici nucleari e da due medici radiologi ed stato anche valutato quale dei due esami era stato richiesto ed eseguito per primo . i pazienti arruolati sono stati raggruppati in base allintervallo di tempo trascorso tra linsorgenza del sospetto clinico e lesecuzione di entrambe le indagini , ovvero 024 ore , 2448 ore , e 27 giorni . 
il test di cohen stato utilizzato per lanalisi della concordanza dei risultati delle due indagini sia per il gruppo di tutti i pazienti arruolati che per i quattro sottogruppi suddivisi in base allintervallo di tempo per lesecuzione delle due indagini 024 ore , 2448 ore , 048 ore , 48 ore7 giorni . risultati la spp e la tcsm sono risultate positive in 29 / 107 ( 27 , 1% ) e negative in 78 / 107 ( 72 , 89% ) , con una concordanza positiva in 22 casi e negativa in 71 ( tabella 3 )  . 
nel sottogruppo dei pazienti che avevano eseguito la spp e la tcsm entro 24 ore dallinsorgenza del sospetto clinico di epa , la spp risultata positiva in 12 / 49 ( 24 , 48% ) e negativa in 37 / 49 ( 75 , 51% ) , mentre la tcsm risultata positiva in 17 / 49 ( 34 , 69% ) e negativa in 32 / 49 ( 65 , 30% ) con g . 
pls ( a ) shows no perfusion in the inferior right lobe , with positive concordance with msct ( b ) , which shows an occlusive thrombus in the right inferior lobe ( white arrow )  . 
la ssp ( a ) mostra assenza di perfusione in corrispondenza del lobo inferiore destro con concordanza positiva con la tcsm ( b ) che mostra la presenza di un trombo occludente nel ramo lobare inferiore destro dellarteria polmonare ( freccia piena )  . 
la tcsm ( b ) dimostra la presenza di un trombo parzialmente occludente ( freccia )  . in the subgroup of patients who had undergone pls and msct within 48 h from the first clinical suspicion of ape , pls was positive in 17 / 69 ( 24.63% ) cases and negative in 52 / 69 ( 75.36% ) cases , while msct was positive in 20 / 69 ( 28.98% ) cases and negative in 49 / 69 ( 71% ) cases , with pc in 15 cases and nc in 47 ( table 6 )  . 
inoltre 35 pazienti avevano effettuato prima la spp e 14 prima la tcsm . nel sottogruppo dei pazienti che avevano eseguito la spp e la tcsm tra 24 e 48 ore dallinsorgenza del sospetto clinico di epa , la spp risultata positiva in 5 / 20 ( 25% ) e negativa in 15 / 20 ( 75% ) , mentre la tcsm risultata positiva in g . 
secondary antithrombin iii deficit protein c deficit factor v leiden protein s deficit plasminogen deficit factor xii deficit hyperhomocysteinaemia anti - cardiolipin antibody congenital dysfibrinogenaemia thrombomodulin tabella 1 fattori di rischio per le tromboembolie venose a . 
concordance between results 3 / 20 ( 15% ) e negativa in 17 / 20 ( 85% ) con una concordanza positiva in 3 casi e negativa in 15 ( tabella 5 )  . 
inoltre 24 pazienti avevano effettuato prima la spp e 14 prima la tcsm . nella tabella 8 riportata lanalisi della concordanza tra la spp e la tcsm nei gruppi di pazienti che hanno effettuato le due indagini entro 24 ore , tra 2448 ore , entro 48 ore , tra 27 giorni ed entro 7 giorni dal sospetto clinico di epa . 
tale concordanza stata maggiore quando le due indagini sono state eseguite entro 24 ore dal sospetto clinico , continua a mantenere valori elevati se le indagini sono eseguite entro 48 ore , mentre si riduce notevolmente se gli esami sono stati eseguiti entro 7 giorni dal sospetto clinico . inoltre fra i 22 pazienti con concordanza positiva tra la spp e la tcsm , 12 hanno eseguito entrambi gli esami entro le 24 ore , 3 entro 48 ore , 7 entro una settimana . 
tra i pazienti con concordanza positiva tra le due indagini nellintera casistica studiata , il 54 , 54% ( 12 / 22 ) apparteneva al sottogruppo studiato entro 24 ore dal sospetto clinico di epa , il 13 , 6% ( 3 / 22 ) al sottogruppo studiato entro 48 ore , il rimanente 31 , 81% ( 7 / 22 ) al sottogruppo studiato entro 7 giorni dal sospetto clinico di epa . 
tra i pazienti con concordanza negativa tra le due indagini nellintera casistica studiata , il 45 , 07% ( 32 / 71 ) apparteneva al sottogruppo studiato entro 24 ore dal sospetto clinico di epa , il 21 , 12% ( 15 / 71 ) al sottogruppo studiato entro 48 ore , il rimanente 33 , 80% ( 24 / 71 ) al sottogruppo studiato entro 7 giorni dal sospetto clinico di epa . in 11 pazienti con spp positiva in fase acuta , questo esame stato ripetuto anche dopo terapia trombolitica prima della dimissione dei pazienti ed ha dimostrato il positivo effetto del trattamento ( miglioramento in 3 , completa normalizzazione della perfusione polmonare in 8 pazienti )  . discussione la diagnosi di embolia polmonare spesso difficile e la mortalit nei casi non trattati , si aggira intorno al 30% , g . 
presence of wedgeshaped areas of hyperperfusion single or multiple wedge - shaped perfusion defects with or without corresponding radiographic parenchymal alterations . absence of wedge - shaped areas of hyperperfusion tabella 2 criteri di interpretazione della spp ( pisa - ped ) diagnosi risultati normale anormale compatibile con epa anormale non compatibile con epa difetti di perfusione non assenza di difetti perfusivi difetti di perfusione cuneiformi singoli o multipli con o senza corrispondenti alterazioni radiografiche parenchimali . 
concordance was higher when the two studies were performed within 24 h of the initial clinical suspicion and remained high when they were performed within 48 h , whereas it decreased markedly if the two studies were performed within 7 days of the initial clinical suspicion . furthermore , among the 22 patients with pc between pls and msct , 12 had undergone both exams within 24 h , three within 48 h , and seven within 1 week . 
among patients with pc between the two investigations , 54.54% ( 12 / 22 ) belonged to the subgroup studied within 24 h of the initial clinical suspicion of ape , 13.6% ( 3 / 22 ) to the subgroup studied within 48 h , and the remaining 31.81% ( 7 / 22 ) to the subgroup studied within 7 days . 
among patients with nc between the two examinations , 45.07% ( 32 / 71 ) belonged to the subgroup studied within 24 h of the initial clinical suspicion of ape , 21.12% ( 15 / 71 ) to the subgroup studied within 48 h , and the remaining 33.80% ( 24 / 71 ) to the subgroup studied within 7 days . mentre si riduce al 2%8% se viene intrapresa una adeguata terapia anticoagulante [ 4 ]  . 
nel 90% dei casi il sospetto di epa motivato dalla presenza di tosse , dispnea , dolore toracico , sincope , tachipnea , cianosi e tachicardia [ 7 , 9 ]  . 
lassenza di questi sintomi ha un valore predittivo negativo del 94% , mentre il valore predittivo positivo rimane basso , pari al 53% , anche considerando lassociazione di pi segni e sintomi riferibili ad epa . 
la radiografia del torace , il dosaggio dei d - dimeri , lemogasanalisi e lecg permettono di orientare la diagnosi e di monitorare le condizioni generali del paziente , ma non consentono una diagnosi definitiva . 
la radiografia del torace solo in rari casi permette di riconoscere lembolia polmonare tuttavia lintegrazione con la spp pu risultare utile per definire la diagnosi di epa [ 11 ]  . la spp permette la visualizzazione diretta della perfusione polmonare attraverso lidentificazione di difetti perfusivi di tipo segmentario e pertanto riveste un ruolo centrale nelliter diagnostico non invasivo di epa . 
la spp un esame semplice , rapido , economico , senza controindicazioni e anche se eseguito con tecnica planare in una sola proiezione permette di riconoscere embolie gravi , per le quali un trattamento terapeutico tempestivo necessario per salvare la vita del paziente . 
la classificazione delle immagini scintigrafiche perfusive suggerita dallo studio pisaped , da noi utilizzata , basata sullidentificazione della presenza e della morfologia di difetti perfusivi , indipendentemente dal loro numero [ 7 ]  . 
dai risultati del suddetto studio appare che la combinazione di una probabilit clinica intermedia o alta con una scintigrafia compatibile con epa ha un elevato valore predittivo positivo ( 98% ) e che una bassa probabilit clinica combinata con un spp anormale , non compatibile con epa , ha un elevato valore predittivo negativo di malattia ( 98% ) [ 7 ]  . nei centri di medicina nucleare , che eseguono indagini 24 ore su 24 in regime durgenza , come il nostro , la spp risultata lesame pi frequentemente richiesto per primo , poich fornisce i dati utili per una gestione terapeutica immediata del paziente . 
nei presidi sanitari in cui la spp non sia rapidamente disponibile la tcsm rappresenta una valida alternativa per documentare le occlusioni totali o parziali delle arterie polmonari [ 1216 ]  . 
tuttavia anche se la tcsm permette di riconoscere embolie pluri - , monoo subsegmentarie , rilevando eventuali riduzioni di densit parenchimale e di vascolarit , non in grado di valutare le modifig . 
of patients who underwent msct first : 30 nudi pazienti che hanno effettuato prima la spp : 77 nudi pazienti che hanno effettuato prima la tcsm : 30 plspls + total plspls + total sppspp + totale sppspp + totale table 4 results for patients undergoing perfusion lung scintigraphy ( pls ) and multislice computed tomography ( msct ) within 024 h tabella 4 risultati della spp e tcsm nel gruppo di pazienti studiati nellintervallo di tempo 024 ore msctmsct + total tcsmtcsm + totale no . 
of patients who underwent msct first : 14 nudi pazienti che hanno effettuato prima la spp : 35 nudi pazienti che hanno effettuato prima la tcsm : 14 in 11 patients with a positive pls in the acute phase , the examination was repeated after thrombolytic therapy and before discharge , and it confirmed the positive effect of treatment ( improvement in three , complete normalisation of lung perfusion in eight )  . discussion the diagnosis of pulmonary embolism is often difficult , and mortality in untreated cases is around 30% , whereas it drops to 2%8% if adequate anticoagulation therapy is initiated [ 4 ]  . 
in 90% of cases , the suspicion of ape is based on the presence of cough , dyspnoea , chest pain , syncope , tachypnoea , cyanosis and tachycardia [ 7 , 9 ]  . 
the absence of these symptoms has a 94% negative predictive value ( npv ) , whereas the positive predictive value ( ppv ) remains low , at 53% , even when the association of several signs and symptoms typical of ape is considered . therefore , other tests need to be used to recognise pulmonary embolism within the first hours after symptom onset . chest radiography , d - dimer , blood gas analysis and electrocardiogram ( ecg ) may suggest a diagnosis and help monitor the patients general condition , although they do not provide a definite diagnosis . 
chest radiography allows recognicazioni funzionali e quindi leffetto emodinamico di emboli o stenosi vascolari che determinano alterazioni della perfusione polmonare [ 17 , 18 ]  . nella nostra esperienza il test di cohen ha documentato una buona concordanza in tutti e 107 i pazienti selezionati . la concordanza risultata maggiore quando lintervallo temporale tra insorgenza del sospetto clinico e lesecuzione delle due indagini era minimo . 
tale non concordanza tra le due indagini spiegabile con la presenza di emboli parzialmente occludenti , che in realt non determinavano alterazioni perfusive significative e quindi di scarso o assente significato funzionale . 
tale non concordanza stata riscontrata nel 3 , 5% ( 2 su 57 ) di pazienti che avevano eseguito prima la spp e poi la tcsm studiati nellintervallo 048 ore e nel 6 , 54% ( 7 su 107 ) di pazienti dellintera casistica studiati nei 7 giorni successivi linsorgenza del sospetto clinico . 
lattivazione dei meccanismi trombolitici con frammentazione dellembolo nelle 48 ore7 giorni dopo linsorgenza del sospetto clinico pu spiegare questa non concordanza . nessun paziente che aveva eseguito entrambe le indagini entro le 24 ore dallinsorgenza del sospetto clinico ha mostrato spp positiva e tcsm negativa . 
of patients who underwent msct first : 7 nudi pazienti che hanno effettuato prima la spp : 13 nudi pazienti che hanno effettuato prima la tcsm : 7 plspls + total plspls + total sppspp + totale sppspp + totale table 6 results for patients undergoing perfusion lung scintigraphy ( pls ) and multislice computed tomography ( msct ) within 048 h tabella 6 risultati della spp e tcsm nel gruppo di pazienti studiati nellintervallo di tempo 048 ore msctmsct + total tcsmtcsm + totale no . 
of patients who underwent msct first : 12 nudi pazienti che hanno effettuato prima la spp : 57 nudi pazienti che hanno effettuato prima la tcsm : 12 tion of pulmonary embolism in sporadic cases only ; however , integration with pls may be useful to confirm the diagnosis of ape [ 11 ]  . pls allows direct visualisation of lung perfusion through the identification of perfusion defects at the segmental level , thus playing a key role in the noninvasive assessment of ape . 
pls is an easy - to - perform , fast , and inexpensive examination that does not present contraindications and , even when performed with the standard planar technique in a single projection , is able to recognise severe embolism necessitating urgent life - saving treatment . 
the classification of scintigraphic perfusion images suggested by the pisa - ped study , which we used , is based on identifying the presence and morphology of perfusion defects , independent of their number [ 7 ]  . 
the results of the above study suggest that the combination of an intermediate to high clinical probability with scintigraphic findings consistent with ape has a high ppv ( 98% ) , and that a low clinical probability combined with abnormal pls findings not consistent with ape has a high npv for this disease ( 98% ) [ 7 ]  . in nuclear medicine centres that perform emergency examinations 24 h / day , as we do , pls was found to be most frequently requested first , as it provides useful information for immediate patient management . 
la tcsm ha il grande pregio di fornire una visione panoramica di tutto il torace e di riconoscere differenti patologie ( atelettasie , focolai broncopneumonici , focolai emorragici ed enfisema )  . 
nei pazienti con spp anormale in cui la tcsm ha mostrato coesistenti patologie cardio - polmonari lintegrazione dei dati pu permettere di attribuire o meno significato embolico alle alterazioni di perfusione riscontrate alla spp [ 19 ]  . in letteratura sono stati suggeriti diversi algoritmi diagnostici sullimpiego delle differenti tecniche di diagnostica per immagini nellepa . 
i criteri di scelta delliter diagnostico devono , tuttavia , tener conto del valore clinico , della reale disponibilit delle diverse indagini , della situazione clinica del paziente ( stabile o instabile ) e della presenza di concomitanti patologie cardio - polmonari . 
this lack of concordance between the two techniques may be explained by the presence of partial occlusions causing no significant changes in perfusion and , subsequently , of little or no functional significance . 
this lack of concordance was identified in 3.5% ( 2 of 57 ) of patients who had undergone pls first and then msct , studied in the 0to 48 - h interval , and in 6.54% ( 7 of 107 ) of patients studied within 7 days of initial clinical suspicion . 
activation of thrombolytic mechanisms with embolus fragmentation during the 27 day period after the initial clinical suspicion may explain this lack of concordance . no patient who underwent both exams within 24 h of the initial clinical suspicion had a positive pls and a negative msct . 
msct has the advantage of providing a panoramic view of the entire chest and visualising different diseases ( atelectasis , bronchopulmonary foci , haemorrhagic foci , and emphysema )  . 
in patients with an abnormal pls , in which msct demonstrated concurrent cardiopulmonary diseases , integration of the data may be necessary to decide whether or not the perfusion alterations seen at pls are ascribable to embolism [ 19 ]  . several diagnostic imaging algorithms have been suggested for the detection of ape . 
other authors suggest the use of msct in cases of pls alterations not typical of pulmonary embolism , advising against its use as a stand - alone technique [ 20 , 21 ]  . however , the criteria for planning the diagnostic workup must take into account the clinical value of techniques , their availability , the patients clinical condition ( stable or unstable ) and the presence of concurrent cardiopulmonary diseases . 
on the other hand , in stable patients with complex radiologic findings , msct should be performed first , because the chances of a nondiagnostic scintigraphy are high in these cases . 
however , msct is preferred for patients with preexisting lung disease or when a differential diagnosis with mediastinal diseases is needed . table 7 results for patients undergoing perfusion lung scintigraphy ( pls ) and multislice computed tomography ( msct ) within 27 days msctmsct + total no . 
of patients with positive exams patients who underwent pls first : 15 patients who underwent msct first : 7 024 h 12 / 49 ( 24.48% ) 2448 h 3 / 20 ( 15.00% ) 27 days 7 / 38 ( 18.42% ) tabella 9 sequenza temporale degli esami spp e tcsm dei 22 pazienti con concordanza positiva raggruppati in base allintervallo di tempo tra insorgenza del sopetto clinico e completamento degli esami di diagnostica per immagini intervallo tra le due indagini numero pz con spp e tcsm positive pz che hanno effettuato prima la spp : 15 pz che hanno effettuato prima la tcsm : 7 024 ore 12 / 49 ( 24 , 48% ) 2448 ore 3 / 20 ( 15 , 00% ) 27 gg 7 / 38 ( 18 , 42% ) conclusions conclusioni in a large group of patients recruited in hospitals with round - the - clock emergency nuclear medicine and radiology services and that follow strict image interpretation criteria , pls and msct proved to have a high concordance when the exams were performed within 7 days of the initial clinical suspicion of ape . 
therefore , a clinical suspicion of ape needs to be confirmed by emergency examinations performed within hours 48 at the most . when both pls and msct are available , pls is the first exam to be ordered for a clinical suspicion of ape . 
although no diagnostic protocol has been universally adopted , pls is the first technique to identify the site and extent of the embolism , thus providing indirect evidence of pulmonary embolismsct is an accurate technique for the diagnosis of ape , and because it can provide information even on other pathological processes , it can confirm or exclude the diagnosis suspected at pls . when both diagnostic techniques are not available , either pls or msct are valuable tools for identifying the presence of severe ape necessitating urgent treatment . in unampia casistica di pazienti arruolati in grandi ospedali con centri di medicina nucleare e radiodiagnostica che effettuano indagini 24 ore su 24 , utilizzando rigorosi criteri di interpretazione delle immagini , la spp e la tcsm hanno dimostrato unelevata concordanza quando eseguite entro 7 giorni dallinsorgenza del sospetto di epa . 
la concordanza pi elevata se le due indagini sono completate entro 2448 ore . pertanto nel sospetto clinico di epa importante accertare la diagnosi con esami durgenza in poche ore , massimo 48 . la spp il primo esame richiesto nel sospetto clinico di epa quando sono disponibili entrambe le tecniche diagnostiche . 
pur non essendo unanimemente accettato un protocollo diagnostico , la spp rappresenta la tecnica di primo approccio per stabilire la sede e lestensione del processo embolico , fornendo levidenza indiretta dellembolia polmonare . 
la malformazione vascolare polmonare stata chiusa in 3 minuti e la saturazione percutanea di ossigeno passata dal 73% al 93% . la fistola da emodialisi stata chiusa con 1 dispositivo in 4 minuti . 
lavp un efficace sistema per la chiusura di grossi vasi periferici e di malformazioni vascolari , a costi contenuti , che consente unembolizzazione sicura e a basso rischio di complicanze , con risparmio in termini di tempo e di dose erogata . key words amplatzer vascular plug transcatheter embolisation vascular disease parole chiave amplatzer vascular plug embolizzazione transcatetere patologia vascolare introduction introduzione percutaneous embolisation has become a valid option and often the first - line treatment for acute bleeding , temporary or permanent devascularisation of benign or malignant hypervascular tumours [ uterine fibroids , hepatocellular carcinoma ( hcc ) ] , the closure of congenital or acquired arteriovenous lembolizzazione percutanea divenuta ormai una valida alternativa e spesso la metodica di prima istanza nel trattamento di sanguinamenti acuti , ma anche nella devascolarizzazione temporanea o permanente di tumori ipervascolarizzati benigni o maligni ( fibromi uterini , hcc ) , nella chiusura c . 
several embolisation devices are available , each with its own characteristic features : a fibrin sponge is used for temporary ( about 48 h ) embolisation , polyvinyl alcohol ( pva ) microspheres are commonly used for permanent embolisation , whereas detachable balloons , glue , metal coils and plugs are used for definitive embolisation . this paper describes our experience with a new system for definitive embolisation , the amplatzer vascular plug ( avp ) , a versatile device that was successfully used in the closure of arteries ( internal iliac and subclavian ) , a pulmonary arteriovenous malformation , a haemodialysis fistula , and a gastric varix in a subject with portal hypertension . materials and methods the avp ( aga medical corporation , golden valley , mn , usa ) is a new device approved by the u.s. 
food and drug administration for peripheral embolisation of arteries and veins and that uses the same technology as other amplatzer devices used for occluding interatrial and interventricular defects and patent foramen ovale . 
the system is preloaded inside a 100 - cm - long guiding catheter : 5 fr for plugs with a diameter of 48 mm , 6 fr for plugs with a diameter of 1012 mm and 8 fr for plugs with a diameter of 1416 mthe system ranges in size from 4 mm di malformazioni vascolari arterovenose congenite o acquisite e nella chiusura di varici . 
esistono in commercio numerosi dispositivi embolizzanti ciascuno con caratteristiche preponderanti rispetto agli altri : per lembolizzazione temporanea si utilizza la spugna di fibrina ( 48 h circa ) ; per quella permanente sono comunemente impiegate le microsfere in alcol polivinilico ( pva ) ; per lembolizzazione definitiva infine ci si avvale dei palloni staccabili , della colla , delle spirali metalliche e dei plug . gli autori descrivono la loro esperienza nellutilizzo di un nuovo sistema per lembolizzazione definitiva , lamplatzer vascular plug ( avp ) , un dispositivo dallutilizzo versatile , specie nei vasi di grosso diametro , che stato utilizzato con successo nella chiusura di arterie ( iliache interne e succlavie ) , di una malformazione arterovenosa polmonare , di una fistola da emodialisi e di una varice gastrica in soggetto con ipertensione portale . materiali e metodi lavp ( aga medical corporation , golden valley , mn , usa ) un nuovo dispositivo approvato dalla food and drug administration per lembolizzazione periferica di vasi arteriosi e venosi che utilizza la stessa tecnologia di altri device amplatzer utilizzati per occludere difetti interatriali , interventricolari e forami ovali . 
il sistema caricato allinterno di un catetere portante ( 100 cm di lunghezza ) da 5 fr per plug da 4 a 8 mm di diametro , da 6 fr per plug da 10 a 12 mm di diametro e da 8 fr per plug da 14 a 16 mm di diametro . 
il sistema disponibile in misure che vanno da 4 mm di diametro fino a 16 mm con un incremento di 2 muna volta raggiunta la sede in cui si vuole rilasciare il dispositivo basta ritirare il catetere in modo da far uscire il plug e girare in senso antiorario la guida metallica per liberare il device . 
in accordo con la casa produttrice si raccomanda di scegliere un dispositivo con un oversize almeno del 20% rispetto al diametro del vaso da trattare per evitare una possibile migrazione distale . 
le peculiarit del sistema sono la sua disponibilit in unampia gamma di misure , anche molto grandi , la possibilit di riposizionamento prima del rilascio definitivo , il minor rischio di migrazione rispetto alle spirali e un breve tempo per occludere definitivamente il vaso . presso il nostro centro sono state eseguite 11 occlusioni vascolari con lutilizzo del nuovo dispositivo avp : 5 arterie iliache interne nella prevenzione dellendoleak di tipo ii dopo posizionamento di endoprotesi aortoiliaca ; 3 arterie succlavie di sinistra per il trattamento di endoleak di ii tipo successivo al posizionamento di endoprotesi dellaorta toracica con copertura dellarteria succlavia sinistra ( ass ) ; 1 fistola arterovenosa polmonare ; 1 fistola da emodialisi e 1 grossa varice in un paziente con emorragia da varice gastrica portatore di tips . 
positive features include the availability of a wide range of sizes , even very large ; the possibility of repositioning the device before its definitive release ; lower risk of migration compared with coils ; and short occlusion times . 
 our centre performed 11 vascular occlusions using the new avp : five internal iliac arteries to prevent type ii endoleaks after aortoiliac stent - graft placement , three left subclavian arteries to treat type ii endoleaks after thoracic aorta stent - graft placement with coverage of the left subclavian artery ( lsa ) , one pulmonary arteriovenous malformation , one haemodialysis fistula , and one large gastric varix due to haemorrhage in a patient with transjugular intrahepatic portosystemic shunt ( tips )  . 
the patients were studied with a multidetector computed tomography ( mdct ) scanner ( somatom sensation 6 , siemens , germany ) , mdct workstation ( leonardo , siemens , germany ) , angiographic equipment ( axiom fa , siemens , germany ) and ultrasound ( us ) ( technos , esaote , italy )  . 
chest mdct done to assess the pulmonary arteries showed a large solitary arteriovenous fistula with two afferent arteries arising from two branches of the right lower lobar pulmonary artery and drainage into the inferior pulmonary vein of the right lower lobe . 
la mdct del torace effettuata per la valutazione delle arterie polmonari ha dimostrato una grossa e solitaria fistola arterovenosa polmonare con due arterie afferenti , provenienti da due rami dellarteria polmonare lobare inferiore di destra , e drenaggio nella vena polmonare inferiore del lobo inferiore del polmone destro . 
langiografia selettiva dellarteria polmonare destra , eseguita attraverso la vena femorale comune di destra , ha confermato la diagnosi posta con la mdct dimostrando un diametro da 10 mm e 4 mm delle due arterie afferenti . 
la chiusura del vaso di maggiori dimensioni stata eseguita utilizzando la tecnica standard gi descritta , con un avp da 12 mm ( oversize del 20% rispetto al vaso nativo ) , mentre la seconda arteria afferente , di minori dimensioni ( 4 mm di diametro ) , stata cateterizzata mediante la tecnica buddy wire : tale sistema consiste nellutilizzo di due guide allinterno dello stesso catetere , per garantire maggior portanza , facilitando il posizionamento del device in vasi a decorso pi complesso . 
 stata utilizzata una guida coronarica da 0 , 014 ( guidant spartacore middle weight ) come buddy wire che stata posizionata oltre il segmento scelto per il rilascio del dispositivo , dando stabilit al catetere , prima del passaggio del device . 
2a multidetector computed tomography ( mdct ) angiography of the abdominal aorta and iliac arteries : anterior volume - rendered ( vr ) image shows an aneurysm of the right common iliac artery ( arrowhead )  . 
c angiography 8 min after release of the avp shows the outline of the device ( arrows ) and complete absence of flow within the right internal iliac artery from the systemic blood flow . 
2a angio - mdct dellaorta addominale e delle arterie iliache : ricostruzione vrt ( volume rendering technique ) che dimostra la presenza un aneurisma dellarteria iliaca comune di destra ( testa di freccia )  . 
c controllo angiografico a 8 minuti dal rilascio dellamplatzer vascular plug , dimostra la sagoma del device rilasciato ( frecce ) e la completa assenza di flusso nellarteria iliaca interna destra dal circolo sistemico arterioso . 
3a angiography of the thoracic aorta after stent - grafting in a patient with type b dissection of the thoracic aorta demonstrates the presence of a type i + type ii endoleak ( arrowheads ) from the left subclavian artery . 
b follow - up multidetector computed tomography ( mdct ) angiography at 1 month ; sagittal maximum intensity projections ( mip ) image confirmed the type i + type ii endoleak ( arrowhead ) from the left subclavian artery and the presence of partial thrombosis of the false lumen ( * )  . 
c similar projection 5 min after release of the amplatzer vascular plug ( avp ) shows the outline of the device ( arrows ) , with the exclusion of the origin of the left subclavian artery , the patency of the left vertebral and internal mammary artery and the absence of endoleaks . 
3a angiografia dellaorta toracica dopo il posizionamento di endoprotesi toracica in un paziente con dissecazione dellaorta toracica di tipo b che dimostra un endoleak di tipo misto ( tipo i + ii ) ( teste di freccia ) dallarteria succlavia sinistra . 
b controllo angio - mdct a un mese , ricostruzione sagittale mip ( maximum intensity projections ) , che conferma la presenza di un endoleak di tipo misto ( tipo i + ii ) ( testa di freccia ) dallarteria succlavia sinistra e la presenza di trombosi parziale del falso lume ( * )  . 
c sucessivo controllo a 5 minuti dal rilascio dellamplatzer vascular plug che mette in evidenza la sagoma del device rilasciato ( frecce ) con la completa chiusura dellorigine dellarteria succlavia sinistra , la perviet dellarteria vertebrale e mammaria interna e lassenza dellendoleak . 
4a angiography shows a persistent passage of contrast material across the previously ligated haemodialysis arteriovenous anastomosis and two large aneurysms ( arrowheads ) that end in a cul - de - sac at the level of the basilic vesome collateral veins , with reverse flow , can be seen to originate from the efferent vein and course towards the hand ( arrows )  . 
b angiography performed 2 min after amplatzer vascular plug ( avp ) deployment shows a considerable reduction in the passage of contrast ( arrow ) through the device ( arrowhead ) into the basilic venote the good patency of the artery below . 
4a langiografia mette in evidenza la persistenza del passaggio di mdc attraverso lanastomosi arterovenosa da emodialisi precedentemente legata chirurgicamente e i due grossi aneurismi ( testa di frecce ) che terminano a fondo cieco a livello della vena basilica efferente : si notano inoltre alcune vene collaterali che si dipartono dalla vena efferente e si dirigono , a flusso invertito , verso la mano ( frecce )  . 
b il controllo angiografico eseguito dopo 2 minuti dallapertura del plug dimostra una marcata riduzione del passaggio di mdc ( freccia ) attraverso il dispositivo ( testa di freccia ) nella vena basilica efferente . 
c il controllo dopo altri 3 minuti evidenzia la totale chiusura della fistola , lassenza delle vene collaterali e la perviet dellasse arterioso a valle . 10 mm and 4 mm of the two afferent arteries . 
closure of the larger vessel was achieved by applying the standard technique , with a 12 - mm avp ( 20% larger than the native vessel ) , whereas the smaller afferent artery ( 4 mm ) was catheterised using the buddy wire technique , which consists of using two guidewires within the same catheter , to ensure better support and facilitate deployment of the device in more tortuous vessels . 
dopo aspirazione del trombo portale , effettuata mediante catetere tipo portante da 8 fr ( jr 4.0 , medtronic , mn , usa ) , stata eseguita una seconda angiografia che ha dimostrato la parziale riduzione del trombo e la persistenza di flusso nella varice : si quindi optato per la sua embolizzazione definitiva . 
5a portography shows , in a patient with transjugular intrahepatic portosystemic shunt ( tips ) , a filling defect ( arrowhead ) of the portal vein at the outlet of the superior mesenteric vein due to probable thrombus . 
5a portografia evidenzia , in un paziente portatore di tips , un difetto di riempimento ( testa di freccia ) della porta a livello dello sbocco della vena mesenterica superiore , da verosimile apposizione trombotica ; ben evidente inoltre la vena gastrica sinistra dilatata ( freccia ) con la presenza di spirali metalliche , da precedente embolizzazione . 
b posizionamento del plug ( testa di freccia ) allinterno della varice prima del rilascio definitivo : si riconoscono molto bene i due markers radiopachi posizionati alle due estremit del device . 
after thromboaspiration with an 8 - fr guiding catheter ( jr 4.0 , medtronic , mn , usa ) , a second angiography showed partial reduction of the thrombus and persistence of flow in the varix : we therefore opted for definitive embolisation . 
portography carried out 5 min after the procedure showed flow reduction through the device but incomplete closure ; two 12 - mm platinum coils ( nester , cook , bloomington , in , usa ) were endoprotesi aortoiliaca stato eseguito il giorno successivo per tre pazienti e due giorni dopo lembolizzazione per gli altri due . 
lembolizzazione unilaterale dellarteria iliaca interna stata tollerata da tutti e 5 i pazienti senza la comparsa di complicanze minori o maggiori quali claudicatio glutea , ischemia glutea o rettosigmoidea , disfunzioni sessuali o urologiche ; il periodo di ospedalizzazione stato in media 5 giorni dopo il posizionamento dellendoprotesi . 
il controllo angio - mdct a 1 mese ha evidenziato una buona rivascolarizzazione da parte di circoli collaterali delle due branche di divisione delliliaca interna trattata , anteriore e posteriore , senza passaggio di contrasto nel tronco comune e ha dimostrato la corretta posizione del plug con perfetta chiusura del vaso solo alla sua origine . 
 nei 3 pazienti a cui stata occlusa larteria succlavia sinistra , la mdct effettuata prima della dimissione e a 1 mese di distanza dal posizionamento dellendoprotesi aortica ha dimostrato la persistenza di endoleak di tipo ii dallarteria succlavia sinistra per due pazienti e in un paziente un endoleak misto : tipo i + tipo ii , ovvero dovuto sia ad una imperfetta sigillatura della protesi sulla parete aortica sia ad una riperfusione attraverso la succlavia : si pertanto optato per locclusione del vaso alla sua origine . 
prima di effettuare il trattamento i pazienti sono stati sottoposti a mdct e a studio eco - color doppler dei tronchi sovraortici e del circolo intracranico per escludere stenosi , ipoplasia o varianti anatomiche delle arterie carotidi , succlavie , vertebrali e del circolo del willis . 
i pazienti sono stati sottoposti quindi ad angiografia selettiva della ass che ha confermato la diagnosi di endoleak di tipo ii in due pazienti ed endoleak misto , tipo i + tipo ii , in un paziente , con perviet della vertebrale . 
tutti i pazienti sono stati dimessi due giorni dopo la procedura di occlusione : nessuno dei 3 pazienti ha avuto complicanze maggiori ( sindrome da furto della succlavia )  . 
il corretto posizionamento dellavp e lavvenuta occlusione dellarteria succlavia stato dimostrato anche mediante mdct di controllo . la fistola arterovenosa polmonare stata completamente esclusa con lutilizzo di due dispositivi avp , uno per ciascuna delle due arterie afferenti . 
il controllo angiografico ha dimostrato una chiusura totale dei due vasi embolizzati : in circa 3 minuti per il vaso maggiore e in minor tempo per quello di minori dimensioni . la saturazione percutanea di ossigeno in condizioni basali salita dal 73% al 93% subito dopo la procedura e si mantenuta stabile per i successivi 6 mesi di follow - up ; lemogasanalisi ha dimostrato normali pressioni di ossigeno e di anidride carbonica . 
il controllo clinico a 1 , 3 , 6 mesi ha dimostrato lassenza di sintomi respiratori , saturazione di ossigeno superiore al 95% in condizioni basali e un radiogramma del torace a tre mesi ha confermato una corretta e stabile posizione dei devices . nella fistola da emodialisi leco - color doppler ha dimostrato la presenza di due grosse dilatazioni vascolari anecogene , con presenza di flusso allinterno , a livello della piega del gomito . 
langiografia dellarto superiore , eseguita con accesso trans - omerale anterogrado 4 fr , ha confermato la presenza di una fistola arterovenosa in cui la legatura chirurgica della vena basilica efferente , eseguita 6 mesi prima , sia a livello dellanastomosi sia poco pi a valle , non aveva garantito una completa chiusura della connessione arterovenosa ; liperafflusso conseguente ha portato allo sviluppo di due grossi aneurismi venosi . 
al fine di escludere il flusso nei due aneurismi e nelle vene collaterali senza ricorrere ad una seconda legatura chirurgica si deciso , in accordo con il paziente , di chiudere definitivamente la fistola per via percutanea mediante avp . 
langiografia eseguita a 4 minuti dal posizionamento ha dimostrato una completa ed efficace chiusura della fistola con assenza di pasresults in the five patients undergoing closure of the common iliac artery , correct avp position was evaluated by means of a manual injection of contrast medium through the guiding catheter ; once in the correct position , the device was unscrewed and released . 
postprocedure angiography confirmed complete occlusion of the vessel within less than 8 mthe aortoiliac endografts were positioned on the following day in three patients and after 2 days in the other two . 
unilateral embolisation of the iia was tolerated by all five patients without minor or major complications , such as gluteal claudication , gluteal or rectosigmoid ischaemia and sexual or urological dysfunctions ; length of hospital stay was 5 days after endograft placement . 
mdct angiography at 1 month showed good revascularisation of the anterior and posterior branches of the treated iia by collateral circulations , without passage of contrast material in the common trunk , and demonstrated the correct position of the plug with perfect closure of the vessel origin . in the three patients who underwent occlusion of the lsa , mdct performed at discharge and 1 month after aortic endograft placement showed the persistence of type ii endoleak from the lsa in two patients and a mixed , type i and type ii , endoleak in one . 
these were both due to imperfect endograft sealing along the aortic wall and to reperfusion through the subclavian artery : we therefore decided to occlude the artery at its origbefore the embolisation procedure , the patients underwent mdct and colour - doppler us of the supraaortic trunks and intracranial vessels to exclude stenosis , hypoplasia or anatomical variants of the carotid , subclavian , vertebral arteries and the circle of willis . 
the patients were then studied by selective angiography of the lsa , which confirmed the type ii endoleak in two patients and the mixed type i and type ii endoleak in the other , with a patent vertebral artery . 
postprocedural angiography confirmed complete occlusion of the origin of the subclavian artery within less than 5 mthe patients were discharged 2 days after the procedure without developing major complications ( subclavian steal syndrome )  . 
correct avp positioning and successful subclavian artery occlusion were also demonstrated by follow - up mdct . the pulmonary arteriovenous malformation was completely excluded using two plugs , one for each of the two afferent arteries . 
baseline percutaneous oxygen saturation rose from 73% to 93% immediately after the procedure and remained stable for the following 6 months ; blood gas analysis demonstrated normal pressure of oxygen and carbon dioxide . 
arm angiography , done with 4 - fr antegrade humeral access , confirmed the presence of an arteriovenous fistula in which surgical ligation of the efferent basilic vein performed 6 months earlier at the level of the anastomosis and slightly below it had failed to guarantee complete closure of the arteriovenous communication . 
in order to exclude flow in the two aneurysms and in the collateral veins without performing a second surgical ligation , we decided in agreement with the patient to attempt definitive percutaneous closure of the fistula with an avp . 
angiography performed after 4 min demonstrated complete and effective closure of the fistula with absence of contrast in the basilic vein , two aneurysms and collateral veins and patency of the arm artery . 
colour - doppler us at 1 and 3 months confirmed the definitive closure of the fistula with complete resolution of the arm oedema and total thrombosis , with absence of flow in the two aneurysms . 
after placement of the two coils and the second plug , embolisation was achieved within about 5 mcolour - doppler us at 1 and 3 months demonstrated good patency of the tips , and angiography at 3 months confirmed varix closure . 
 discussion the avp has recently been shown to be effective in the occlusion of internal iliac arteries [ 1 ] , the treatment of pulmonary arteriovenous malformations [ 2 , 3 ] and as an occlusion system for a splenorenal shunt arising after tips [ 4 ]  . 
in our experience , avp was used to achieve vascular occlusion in five different arterial and venous settings . endograft placement in the abdominal aorta has become a valid alternative to conventional surgery and is increasingly the treatment of choice in elderly patients and subjects with high surgical risk . 
about 20% of abdominal aorta aneurysms have an iliac component [ 6 ] , and often the neck of the distal common iliac artery is insufficient to provide an adequate landing zone for the grawhen the aneurysm involves the common iliac artery as far as the origin of the iia , it is necessary to cover the iia with the graft and saggio di mdc nella vena basilica e di conseguenza nei due aneurismi e nelle vene collaterali con perviet dellasse arterioso dellarto . 
il controllo clinico ed eco - color doppler effettuato a 1 e a 3 mesi ha confermato la buona e definitiva chiusura della fistola con risoluzione completa delledema dellarto e trombosi totale , con assenza di flusso nei due aneurismi . la grossa varice gastrica stata chiusa con 2 avp e 2 spirali in platino dato il diametro particolarmente ampio e la persistenza di flusso dopo limpianto del primo plug . 
i controlli eco - color doppler a 1 e 3 mesi hanno mostrato buona perviet della tips e il controllo angiografico a 3 mesi ha confermato la chiusura della varice . discussione recentemente lefficacia dellavp stata dimostrata per locclusione di arterie iliache interne [ 1 ] , nel trattamento di fistole arterovenose polmonari [ 2 , 3 ] e come sistema per locclusione di uno shunt spleno - renale in seguito al posizionamento di tips [ 4 ]  . 
la descrizione della validit dellavp relativamente ad una casistica ampia e al trattamento di patologie vascolari pluridistrettuali , non stata ancora riportata , a nostra conoscenza , da alcun autore . nellesperienza qui riportata lavp stato utilizzato per locclusione vascolare in 5 diverse patologie , sia sul versante arterioso sia su quello venoso . il posizionamento di endoprotesi dellaorta addominale , ormai una valida alternativa alla chirurgia tradizionale e sempre pi spesso il trattamento di scelta in pazienti anziani e ad alto rischio operatorio ; i vantaggi , come noto , sono la minore invasivit , la minor durata della procedura e dellospedalizzazione , la ridotta perdita di sangue e la ridotta morbillit e mortalit rispetto alla chirurgia aperta [ 5 ]  . 
circa il 20% degli aneurismi dellaorta addominale ha una componente aneurismatica iliaca [ 6 ] e spesso il colletto dellarteria iliaca comune distale insufficiente per assicurare un adeguato atterraggio della protesi . 
quando la patologia aneurismatica coinvolge larteria iliaca comune fino allorigine dellarteria iliaca interna ( aii ) risulta necessario ricoprire con la protesi laii ed estendere la protesi fino allarteria iliaca esterna . 
nellottica quindi di prevenire un endoleak di ii tipo ( da vasi collaterali ) e quindi garantire una buona esclusione dellaneurisma raccomandata la chiusura , pre - posizionamento di endoprotesi , della aii [ 710 ]  . 
lembolizzazione prossimale della aii , utilizzando le spirali tradizionali , una tecnica relativamente sicura ed efficace ed stata riportata da molti autori [ 8 , 10 , 11 ]  . 
i maggiori difetti delle spirali sono la necessit di utilizzarne spesso un numero molto elevato , prima di riuscire a chiudere adeguatamente il vaso , lalto costo e la durata della procedura ; inoltre pu residuare un flusso anterogrado attraverso le spirali , si pu avere una dislocazione distale delle stesse o una protrusione allinterno del lume delliliaca comune o esterna [ 12 , 13 ]  . 
da marzo 2005 abbiamo iniziato ad utilizzare lavp al posto delle spirali per embolizzare preventivamente le arterie iliache interne ; questo dispositivo consente unottima occlusione prossimale del vaso allorigine , prima c . 
therefore , to prevent a type ii endoleak ( due to collaterals ) and guarantee adequate exclusion of the aneurysm , closure of the iia before endograft placement is recommended [ 710 ]  . 
in addition , there may be residual antegrade flow through the coils , distal migration , or protrusion within the lumen of the common or external iliac artery [ 12 , 13 ]  . 
in march 2005 , we started using the avp instead of coils for preventive embolisation of iias ; the device allows excellent proximal occlusion at the vessel origin , before the bifurcation , guaranteeing better revascularisation of the collateral branches of the contralateral hypogastric artery and reducing complications due to hypoperfusion . even thoracic aorta endovascular repair has been approved as a less invasive treatment compared with conventional surgery [ 14 ]  . 
the most important anatomical prerequisite for correct positioning of the stent - graft is the presence of a neck of adequate length ( at least 1520 mm ) distal to the lsa orighowever , descending thoracic aorta lesions often involve the distal aortic arch , with a proximal neck less than 15 mm : in these cases one technique enabling safe device fixation is the creation of a more proximal landing zone with deliberate overstenting of the lsa ostium [ 5 , 15 , 16 ]  . this procedure can only be done after excluding abnormalities of the vertebral and carotid arteries and the circle of willis and if the left internal mammary artery has not been used for a coronary bypass . 
all proximal endoleaks have an incidence of 0%23% for early endoleaks ( detected during stent - graft placement ) and 0%5% for late endoleaks , and they may be related to aneurysm morphology , dissection or even technical expertise [ 15 ]  . 
if this type of endoleak ( type ii from the subclavian artery ) persists , it needs to be promptly repaired because of the direct connection between the aneurysmal sac or false lumen and systemic arterial pressure . 
our three patients underwent avp embolisation of the origin of the subclavian artery because they had developed a type ii or mixed ( type i and ii ) endoleak from the subclavian artery , which was overstented at its origin due to an inadequate proximal neck . 
the use of metal coils is not advised for subclavian occlusion [ 15 ] due to the high risk of distal embolisation and the likelihood of not being able to block flow completely . 
these are abnormal , direct communications between pulmonary arteries and veins without a capillary bed , which are caused by the formation of an aneurysmal sac or a tangle of tortuous vessels [ 1820 ]  . 
treatment opdella biforcazione nei suoi due rami , garantendo una migliore rivascolarizzazione da rami collaterali dellipogastrica controlaterale riducendo in questo modo possibili complicanze da ipoperfusione . anche il trattamento endovascolare della patologia dellaorta toracica ormai stato approvato come trattamento meno invasivo rispetto alla chirurgia tradizionale [ 14 ]  . 
il pi importante requisito anatomico per il corretto posizionamento dellendoprotesi la presenza di un colletto minimo di 1520 mm distalmente allorigine dellostio dellass . tuttavia la patologia dellaorta toracica discendente spesso coinvolge larco aortico distale con un colletto prossimale inferiore a 15 mm : in tali casi una delle tecniche per un sicuro fissaggio del dispositivo un atterraggio pi prossimale con la copertura volontaria dellostio dellass [ 5 , 15 , 16 ]  . tale procedura pu essere effettuata soltanto escludendo prima patologie a carico delle arterie vertebrali , delle carotidi , del circolo del willis e se la mammaria interna sinistra non stata utilizzata per un bypass coronarico . un endoleak di tipo ii dalla ass pu insorgere dopo posizionamento di endoprotesi dellaorta discendente ma ad oggi non riportata in letteratura lesatta incidenza . 
la percentuale di tutti gli endoleak prossimali varia dallo 0% al 23% per gli endoleak precoci ( dimostrati al momento del posizionamento della protesi ) e dallo 0% al 5% per quelli tardivi e possono essere legati allanatomia dellaneurisma o dissezione o anche allesperienza delloperatore [ 15 ]  . 
questo tipo di endoleak ( tipo ii dalla succlavia ) se persiste richiede una tempestiva correzione a causa della diretta comunicazione tra la sacca aneurismatica o il falso lume e la pressione arteriosa sistemica . 
i nostri 3 pazienti sono stati sottoposti ad embolizzazione dellorigine della succlavia con avp , poich avevano sviluppato un endoleak di tipo ii o misto ( tipo i + tipo ii ) dalla succlavia che stata ricoperta dallendoprotesi alla sua origine per la presenza di un colletto prossimale insufficiente . 
lutilizzo delle spirali metalliche per locclusione della succlavia non consigliabile [ 15 ] per il forte rischio di embolizzazione distale e per lalta probabilit di non riuscire a bloccare totalmente il flusso : il nuovo dispositivo avp consente unimmediata , sicura e rapida occlusione allorigine del vaso senza complicanze emboliche distali . 
per questultima caratteristica lavp assume unimportante ruolo nel trattamento delle fistole arterovenose polmonari ( favp ) ; questultime sono delle anormali connessioni dirette tra arterie e vene polmonari con lesclusione del letto capillare dovute alla formazione di una sacca aneurismatica o ad un groviglio di canali vascolari tortuosi [ 1820 ] : estremamente eterogenea la presentazione clinica [ 18 , 21 , 22 ]  . 
le opzioni terapeutiche includono lembolizzazione percutanea o lescissione chirurgica [ 2 ]  . data la minore invasivit e lo sviluppo di nuovi materiali embolizzanti il trattamento percutaneo divenuto il trattamento di scelta per la maggior parte dei pazienti [ 2325 ]  . 
la ricanalizzazione della favp pu avvenire in una percentuale compresa tra il 5% e il 10% dei pazienti trattati [ 26 , 27 ] : pertanto , la scelta di un materiale embolizzante appropriato e laccurata localizzazione del sito dove iniziare lembolizzazione di cruciale importanza [ 23 , 24 ]  . 
recanalisation of pavf may occur in 5%10% of treated patients [ 26 , 27 ] , so the choice of appropriate embolising material and accurate localisation of the site where embolisation is to be started are crucial [ 23 , 24 ]  . 
these considerations are even more important in massive fistulas , which are more difficult to occlude with coils or detachable balloons due to the risk of distal migration [ 25 , 28 ]  . 
we believe the avp to be safer and easier to use than the above - mentioned devices owing to the simplicity and small size of the release system and , more importantly , because it was designed for vascular use and is therefore more specific and better suited to the tubular morphology of vessels seen in pavf . haemodialysis fistulas often develop complications , one of the most common being aneurysm formation [ 31 , 32 ]  . possible treatment options include surgery , endovascular treatment or both . 
we opted for the avp because its release is controlled and it can be placed precisely at the level of the neck where it readily adheres to the vessel without risking distal migration . 
to our knowledge , no author has described the use of the avp as an embolising device for the closure of a haemodialysis fistula . the efficacy of tips is well documented in the treatment of variceal bleeding refractory to endoscopic treatment [ 36 , 37 ]  . 
although tips alone is sufficient to stop variceal bleeding in many cases [ 3840 ] , in some patients with large collateral veins , it may not be enough ; embolisaton of the varix therefore becomes indispensable [ 4144 ] , as in the case treated by us . 
even very large coils ( 20 mm15 cm ) are susceptible to distal migration , and the same applies to other materials such as sclerosing agents , glue and gelatine sponge particles , which are not very effective and only increase the risk of systemic embolisation . 
in our opinion , the avp is the vascular occluder that best adapts to large vessels such as gastric varices ; in addition , it can be used is combination with coils to make vascular occlusion even more rapid . our experience indicates that the avp is an extremely versatile occlusion system that is suitable for variety of vessel to pi difficile occluderle con le spirali o i palloni staccabili a causa della possibilit di migrazione distale [ 25 , 28 ]  . 
migliori risultati sono stati ottenuti in passato con lutilizzo di vari device , ad uso cardiologico realizzati per il trattamento della perviet del dotto arterioso di botallo e dei difetti settali cardiaci , quali il gianturco - grifka , composto prevalentemente da un sacco in nylon flessibile e una guida occludente , il cardioseal , costituito da un doppio ombrellino ciascuno con quattro molle metalliche e stoffa di poliestere e lamplatzer duct occluder , realizzato con una maglia guida in nitinolo con estremit a disco [ 24 , 29 , 30 ]  . 
noi riteniamo che lavp , sia pi sicuro e facile da utilizzare rispetto ai precedenti devices menzionati , per la semplicit e le ridotte dimensioni del sistema di rilascio ma soprattutto , essendo un dispositivo dedicato allimpiego vascolare , risulta pi specifico e meglio conformabile allanatomia tubulare del vaso come nel caso delle malformazioni arterovenose polmonari . le fistole da emodialisi , sono gravate da alcune complicanze tra cui una delle pi comuni la formazione di aneurismi [ 31 , 32 ]  . 
lapproccio endovascolare pu avvalersi del posizionamento di uno stent ricoperto a livello arterioso , in modo da escludere la zona di anastomosi , oppure lembolizzazione a livello anastomotico arterioso della fistola [ 3335 ]  . 
nel nostro caso , poich la fistola era localizzata a livello del gomito , lutilizzo di uno stent ricoperto era controindicato e pertanto lunica indicazione terapeutica percutanea era lembolizzazione transcatetere . 
abbiamo preferito utilizzare un avp perch ha un rilascio controllato e pu essere posizionato esattamente a livello del colletto , aderendo prontamente al vaso senza rischio di migrazione distale sia sul versante arterioso sia su quello venoso . 
a nostra conoscenza nessun autore , prima dora , ha descritto limpiego dellavp come sistema embolizzante per la chiusura di una fistola arterovenosa da emodialisi . lefficacia della tips stata ben provata nel trattamento del sanguinamento da varici resistenti al trattamento endoscopico [ 36 , 37 ]  . 
in molti casi la tips da sola sufficiente a bloccare il sanguinamento delle varici [ 3840 ] tuttavia in alcuni pazienti con grosse vene collaterali pu non bastare ; pertanto in tali soggetti lembolizzazione della varice risulta indispensabile [ 4144 ] , come nel caso da noi trattato . 
il grande diametro di questi vasi collaterali costituisce il principale problema nella scelta del materiale embolizzante : anche spirali metalliche molto grandi ( 20 mm15 cm ) possono facilmente migrare distalmente . 
ugualmente vale per altri materiali come agenti sclerosanti , colla , particelle di spugna di gelatina che non hanno una grande efficacia e aumentano solo il rischio di embolizzazione sistemica . 
a nostro giudizio lavp il dispositivo di occlusione vascolare che meglio si adatta a vasi di grosse dimensioni come le varici gastriche : pu inoltre essere utilizzato in associazione alle spirali per rendere ancora pi rapida locclusione vascolare . in conclusione , in base alla nostra esperienza , possiamo affermare che lavp si rivelato un sistema di occlusione vascolare estremamente versatile , adatto quindi a vasi di diametro eterogeneo , facile da usare , preciso nel rilascio , c . 
ridolfi , via varthema 44 , bologna , italy , tel . : + 39 - 051 - 6235444 , fax : + 39 - 051 - 6235444 , e - mail : marcelloridolfi@yahoo.it * il lavoro spetta in parti uguali agli autori received : 21 march 2006 / accepted : 20 august 2006 / published online : 19 march 2007 abstract purpose . 
thirty - eight patients ( 15 men and 23 women ; mean age 55 years ; age range 3579 ) with neck pain were examined and divided into two groups : ( 1 ) patients already identified as rheumatic and referred for further investigation of the atlantoaxial region ; ( 2 ) patients with symptoms confined to the cervical spine , with inconclusive radiographic findings . unenhanced ct of the cervical spine ( tomoscan sr 7000 philips , eindhoven , netherlands ) was performed in all patients . 
ct demonstrated calcific deposits around the dens in 12 patients ( three men and nine women ) , in the transverse and alar ligaments , and in the anterior atlantooccipital membrane . 
crystals located in the transverse ligament of the atlas give rise to the crowned dens syndrome , usually in patients affected by severe degenerative lesions of the atlantoaxial joint and peripheral chondrocalcinosis . 
i soggetti sono stati suddivisi in due gruppi : ( 1 ) pazienti gi diagnosticati come reumatici , di cui lo specialista richiedeva un ulteriore approfondimento diagnostico della zona atlo - epistrofica ; ( 2 ) pazienti con sintomatologia desordio circoscritta al rachide cervicale , di cui la radiologia convenzionale era risultata poco significativa . 
tutti i pazienti sono stati sottoposti a tc volumetrica della colonna cervicale ( tomoscan sr 7000 philips , eindhoven , olanda ) , senza somministrazione per via endovenosa di mezzo di contrasto . 
lesame tc risultato positivo , per depositi calcifici a livello del dente , in 12 pazienti ( 3 maschi e 9 femmine ) , con calcificazioni a livello del legamento trasverso , di quelli alari e della membrana atlo - occipitale anteriore . 
radiography of other joints ( wrist , knee , pubic symphysis ) may help to ascertain whether the disease is due to calcium pyrophosphate dihydrate or hydroxyapatite crystals , and is therefore recommended for routine patient management . magnetic resonance imaging ( mri ) is indicated for the study of neurological complications . key words crowned dens syndrome cppd crystal deposition disease transverse ligament of the atlas computed tomography localizzazione , generalmente asintomatica ; quando i cristalli hanno sede nel legamento trasverso dellatlante , si realizza la sindrome del dente incoronato , abitualmente in pazienti con lesioni degenerative avanzate dellarticolazione atlo - epistrofica e con evidente condrocalcinosi periferica . 
nella sindrome del dente incoronato la tc rappresenta il gold standard diagnostico , potendo identificare la forma e la sede delle calcificazioni e le eventuali erosioni ossee . lesame radiografico di altri distretti articolari ( carpo , ginocchio , sinfisi pubica , spalla ) pu agevolare il riconoscimento eziologico della malattia , se da cppd o da ha , ed pertanto raccomandato nella gestione routinaria del paziente . 
limpiego della rm indicato nello studio della complicanze neurologiche . parole chiave sindrome del dente incoronato malattia da deposito di cristalli di cppd legamento trasverso dellatlante tomografia computerizzata introduction introduzione the crowned dens syndrome ( cds ) is a clinical - radiological entity characterised by calcification of the ligaments surrounding the odontoid process of the axis and by acute attacks of cervicooccipital pain , with fever , rigidity and general signs of inflammation lasting from days to several weeks [ 1 ]  . 
the crystal deposits , in most cases calcium pyrophosphate dihydrate ( cppd ) but also hydroxyapatite ( ha ) , may remain asymptomatic or cause chronic cervical pain and spinal cord compression [ 2 ]  . the classic presenting triad ( headache , fever and morning cervical pain ) was first described by le goff in 1980 [ 3 , 4 ] , who distinguished these acute attacks from those seen in common osteoarthritis and in crystal diseases of the distal cervical vertebrae or thoracic - lumbar spine [ 5 ]  . 
furthermore , atypical cases of cds can simulate both the painful cervicobrachial syndrome ( with shoulder weakness and stiffness ) , as well as occipitotemporal headache ( which mimics atypical rheumatic polymyalgia and / or giant cell arteritis )  . 
according to available data [ 710 ] , computed tomography ( ct ) imaging at the c1c2 level is still the reference standard and is superior to magnetic resonance imaging ( mri ) in identifying these calcifications , especially when they are small [ 11 ]  . the aim of this paper was to illustrate a series of cases of cds seen not only in crystal deposition diseases but also in other rheumatic and nonrheumatic conditions and to provide an assessment of ct imaging patterns and an analysis of the best use of current imaging techniques . 
 la sindrome del dente incoronato ( sdi ) rappresenta unentit clinico - radiologica caratterizzata dallassociazione di calcificazioni dei legamenti attorno al dente dellepistrofeo e da attacchi acuti periodici di cervicalgia occipitale con febbre , rigidit e segni generali di flogosi , di durata molto variabile , da pochi giorni ad alcune settimane [ 1 ]  . colpisce prevalentemente il sesso femminile , con et media al momento della diagnosi tra i 60 ed i 70 anni . 
i depositi di cristalli , nella maggior parte dei casi di pirofosfato di calcio diidrato ( cppd ) , ma anche di idrossiapatite ( ha ) , possono rimanere asintomatici oppure essere responsabili di dolore cronico cervicale e di compressione midollare [ 2 ]  . la tipica descrizione della sindrome , caratterizzata dalla triade cefalea , febbre e cervicalgia mattutina , stata riferita nel 1980 da le goff [ 3 , 4 ] , che distinse questi attacchi acuti da quelli osservati nelle delle malattie da microcristalli a localizzazione vertebrale cervicale distale o dorso - lombare , e da quelli della comune malattia artrosica [ 5 ]  . 
inoltre casi atipici di sdi possono simulare sia la sindrome dolorosa cervico - brachiale ( con debolezza e rigidit della spalla ) che la cefalea occipitale e temporale ( che mima la polimialgia reumatica atipica e / o larterite a cellule giganti )  . 
secondo la letteratura [ 710 ] , lesame tc focalizzato a livello di c1 - c2 rimane il gold standard della diagnostica per immagini ed superiore alla rm nellidentificare queste calcificazioni , soprattutto se minute [ 11 ]  . scopo del presente lavoro stata lillustrazione di alcuni materials and methods between 2001 and 2004 , 38 patients ( 15 men and 23 women ; age range 4572 years ; mean age 55 ) were referred by both general practitioners and specialists ( orthopaedic surgeons , rheumatologists , neurologists , and oncologists ) for investigation of neck pathe patients were divided into two groups : the first ( 16 cases , three men and fifteen women ) consisted of patients with a known clinicalrheumatologic diagnosis [ rheumatoid arthritis ( ra ) , diffuse idiopathic skeletal hyperostosis ( dish ) , etc . ] established on the basis of pain and / or dysfunction at the level of the atlantoaxial joint and alterations demonstrated by conventional radiography , and for whom the specialist had requested further diagnostic investigation the second group ( 22 cases , 12 men and fifteen women ) consisted of patients referred by rheumatologists , general practitioners and other specialists ( orthopaedic surgeon , neurologist , oncologist ) , with initial symptoms confined to the lower cervical spine , often with a history of trauma , and with inconclusive radiographic findings . data collected for each patient included signs and symptoms of the illness , social status and daily working activity , physical examination and laboratory tests , clinical diagnosis and radiographic findings . 
 the disorders affecting the patients ( table 1 ) were distributed as follows : 11 cases of rheumatoid arthritis ( ten women and one man ) , two of cppd crystal deposition disease ( both women ) , one of systemic sclerosis ( a woman ) , one of osteoarthritis ( a man ) , one of seronegative spondyloarthritis ( a man ) , four of neoplasm ( one woman and three men ) with suspected cervical metastases , one ( a man ) of malignant haematological disease ( lymphoma ) , one ( a woman ) of postmenopausal osteoporosis , ten ( five men and five women ) of recent or previous traumatic injury with suspected involvement of the skull base and first cervical vertebrae ( dens fracture , frank atlantoaxial luxation or subluxation ) and six of algo - dysfunctional syndrome of the cervical spine ( three men and three women )  . 
evaluation with ct imaging casi di sindrome del dente incoronato non solamente nellambito delle malattie da deposito di microcristalli , ma anche in altre malattie reumatiche ( i.e. , artrite reumatoide ) e non , la valutazione dei loro aspetti iconografici tc e il giudizio sul miglior impiego delle tecniche attuali di imaging . materiale e metodi nel periodo 20012004 sono stati esaminati 38 pazienti , di cui 15 maschi e 23 femmine , di et compresa fra i 45 ed i 72 anni ( media 55 ) , affetti da cervicalgia , inviati sia dal medico di base che dallo specialista ( ortopedico , reumatologo , neurologo , oncologo ) per gli accertamenti del caso . 
i pazienti sono stati divisi in due gruppi : il primo ( formato da 16 pazienti , di cui 3 maschi e 13 femmine ) , dove la diagnosi clinico - reumatologica era gi stata effettuata ( ar , dish , ecc . ) per la comparsa di sintomatologia algica e / o disfunzionale a livello della cerniera atlo - epistrofica , con alterazioni gi dimostrate in maniera inequivocabile dallesame radiografico convenzionale , e di cui lo specialista richiedeva un ulteriore approfondimento diagnostico a livello della suddetta zona ; il secondo gruppo ( formato da 22 casi , di cui 12 maschi e 10 femmine ) comprendeva pazienti inviati non dal reumatologo , ma dal medico di base e da altri specialisti ( ortopedico , neurologo , oncologo ) , la cui sintomatologia desordio era circoscritta al rachide cervicale , specie in sede prossimale , talvolta su base post - traumatica , e di cui la diagnostica per immagini convenzionale era risultata poco significativa . i dati raccolti per ogni paziente comprendevano tutti i segni ed i sintomi relativi alla malattia denunciata ; lo stato sociale e lattivit lavorativa giornaliera ; gli esami fisico e di laboratorio ; la diagnosi clinica ; i reperti ottenuti con la radiografia convenzionale . 
la visualizzazione delle immagini stata sempre effettuata in modo da avere finestra e livello di finestra sia per i tessuti molli ( i.e. , legamento trasverso ) che per le strutture ossee . 
in particolare , per lo scheletro , lampiezza della finestra stata di 1500 hu e il livello + 300 hu ; per le parti molli rispettivamente 350 hu e + 50 hu . 
non stato somministrato mezzo di contrasto . per quanto riguarda la patologia dei nostri pazienti , la cui distribuzione riportata nella tabella 1 , questa era cos rappresentata : 11 pazienti affetti da artrite reumatoide ( di cui 10 femmine e 1 maschio ) ; 2 casi portatori di malattia da p.n. 
ct demonstrated calcific deposits in the periodontoid structures ( transverse ligament of the atlas , crossed ligament , and alar ligaments ) in 12 patients , three of whom were men and nine who were women ( table 2 )  . 
ct appearance of calcifications was one of thin calcium deposits forming a cppd , entrambi di sesso femminile ; 1 caso di sclerosi sistemica ( femmina ) ; 1 caso di artrosi ( maschio ) ; 1 caso di spondiloartrite sieronegativa ( maschio ) ; 4 pazienti oncologici ( 1 femmina e 3 maschi ) con sospetta localizzazione replicativa cervicale ; 1 caso ( maschio ) affetto da patologia ematologia maligna ( linfoma ) ; 1 caso ( femmina ) con osteoporosi postmenopausale ; 10 pazienti ( 5 maschi e 5 femmine ) affetti da patologia traumatica , recente e pregressa , di cui si sospettava interessamento della base del cranio e delle prime vertebre cervicali ( frattura del dente dellepistrofeo e / o sublussazione e lussazione franca atlo - epistrofica ) e infine 6 pazienti affetti da patologia imprecisata ( 3 maschi e 3 femmine ) algico - disfunzionale cervicale . 
in essi la malattia prevalente era rappresentata dallartrite reumatoide ( ar ) 10 femmine e 1 maschio cui facevano seguito la malattia da cppd ( 2 casi ) , la sclerosi sistemica , lartrosi e la spondiloartrite sieronegativa ( 1 caso , rispettivamente )  . risultati lesame tc della giunzione atlo - epistrofica stato eseguito sulla base della sintomatologia clinica denunciata dal patable 2 patients with crowned dens syndrome ( cds ) and positive computed tomography ( ct ) findings rheumatic diseases no . 
evaluation with ct imaging women 9 rheumatoid arthritis men 3 cppd crystal deposition disease systemic sclerosis rheumatoid arthritis osteoarthritis seronegative spondyloarthritis femmine 9 artrite reumatoide maschi 3 malattia da cppd sclerosi sistemica artrite reumatoide osteoartrosi spondilite sieronegativa transverse ligament ( 4 ) alar ligaments ( 2 ) alar ligaments transverse ligament transverse ligament alar ligaments transverse ligament + atlooccipital anterior membrane legamento trasverso ( 4 ) legamenti alari ( 2 ) legamenti alari legamento trasverso legamento trasverso legamenti alari legamento trasverso + membrana atlo - occipitale anteriore tabella 2 pazienti con sindrome del dente incoronato e tc positiva malattia reumatica casi , n sede delle calcificazioni shell around the dens and located both posteriorly ( on axial images the deposits , they appeared inhomogeneous and probably located on the transverse ligament ) and at the level of the dens apex and base ( on coronal ct reformations due to involvement of the alar and apical ligaments )  . 
 [ 13 , 14 ] identified nonurate crystals in the synovial fluid of patients clinically presenting gout - like attacks ( hence the initial name pseudogout )  . these cppd crystals were characterised by a weak positive birefringence at polarised light microscopy , a finding that distinguished them from the monosodium urate crystals of gout . 
the radiographic features of the disease had , however , been already described by zitnan and sitaj in 1963 , who had called it polyarticular chondrocalcinosis [ 15 ]  . 
bennet , in particular , noted the presence of chalky , rhomboid - shaped crystals [ 16 ] during the autopsy of a patient in ireland with polyarticular chondrocalcinosis . ziente ( principalmente rappresentata da rigidit nucale e cefalea , con o senza incapacit funzionale ) o nellambito del follow - up diagnostico , soprattutto nei casi affetti da cppd dove lesame radiografico tradizionale aveva gi dimostrato la presenza di calcificazioni nelle sedi tipiche della malattia ( i.e. , ginocchio , polso )  . 
lesame tc risultato positivo per depositi calcifici in corrispondenza delle strutture viciniori al dente dellepistrofeo ( legamento trasverso dellatlante , legamento crociato , legamenti alari ) in 12 pazienti , di cui 3 maschi e 9 femmine , la cui distribuzione riportata nella tabella 2 . 
i tre soggetti erano affetti da ar ( anni 69 ) , da osteoartrosi ( anni 70 ) e da spondilite sieronegativa ( anni 48 ) ( fig . 1 ) , con calcificazioni a livello rispettivamente del legamento trasverso , di quelli alari e della membrana atlo - occipitale anteriore . 
liconografia delle calcificazioni era rappresentata da tenui depositi calcifici a guscio , attorno al dente dellepistrofeo , sia in sede posteriore ( nelle immagini tc sul piano assiale , di tipo disomogeneo , verosimilmente a carico del legamento trasverso ) , sia in corrispondenza dellapice e della base del dente stesso ( nelle immagini tc ricostruite sul piano coronale , per interessamento dei legamenti alari e del legamento apicale )  . 
the term chondrocalcinosis is very general , as it suggests apparent radiological and pathological calcification of the cartilage ( which could be due to cppd , ha , tricalcium phosphate or a combination of the three )  . 
although articular and periarticular calcifications can appear in cppd disease , similar calcifications can also be produced by other crystals [ 15 , 19 , 20 ]  . cppd crystal deposition disease is classified into sporadic , hereditary or secondary forms [ 16 ]  . 
the clinical presentation ranges from an incidental radiographic finding to discussione sebbene la malattia da deposito di pirofosfato di calcio diidrato ( cppd ) sia la pi comune artropatia da microcristalli [ 12 ] , tuttavia la scoperta di questi nelle strutture intra - articolari risale allinizio degli anni 60 , quando mccarty insieme ad hollander , kohn e faires [ 13 , 14 ] identific cristalli non uratici nel liquido sinoviale di pazienti che clinicamente presentavano attacchi simil - gottosi ( da ci il termine di pseudogotta dato inizialmente alla malattia )  . questi cristalli di cppd erano caratterizzati da una bassa birifrangenza positiva quando esaminati al microscopio a luce polarizzata , fenomeno che li distingueva da quelli di urato monosodico della gotta . 
the radiological presentation [ 2123 ] is characterised by calcifications in and around the joints and by structural articular changes ( pyrophosphate arthropathy )  . the knee , the wrist , the pubic symphysis and the hip are most commonly affected . 
the spine may be the only site of cppd disease [ 20 , 24 ] and is generally asymptomatic [ 12 ]  . crystals may be identified both in the nucleus pulposus of p.n. 
questultimo , in irlanda , durante lautopsia di un paziente affetto da condrocalcinosi poliarticolare , evidenzi la presenza di cristalli romboidali , di aspetto gessoso [ 16 ]  . i numerosi studi di resnick et al . 
 [ 12 , 17 ] hanno messo ordine nelle svariate nomenclature con cui la malattia era conosciuta , in quanto diversi sinonimi sono stati usati in maniera intercambiabile tra di loro , causando in passato una certa confusione . 
in effetti , il termine condrocalcinosi molto generico , in quanto indica una evidente calcificazione radiologica ed anatomopatologica della cartilagine ( che pu riferirsi alla presenza di cristalli di cppd , di ha , di fosfato tricalcico o alla combinazione dei tre suddetti )  . 
la dizione malattia da deposito di cristalli di cppd ( cppd crystal deposit disease ) si riferisce specificatamente a un disordine caratterizzato dalla esclusiva presenza di cristalli di cppd dentro o intorno alle articolazioni . 
le calcificazioni articolari e periarticolari possono comparire nella malattia di cppd ; tuttavia altri cristalli possono produrre calcificazioni analoghe [ 15 , 19 , 20 ]  . la malattia da cppd si classifica in forma sporadica , ereditaria o secondaria [ 16 ]  . 
infine , i cristalli di cppd possono depositarsi nel legamento trasverso dellatlante e nei legamenti alari , realizzando la c.d. sindrome del dente incoronato [ 1 , 68 ] , la cui definizione , in accordo con diversi autori [ 7 , 8 , 26 ] , dovrebbe comprendere calcificazioni di ogni componente articolare in questa sede ( membrana sinoviale , capsula articolare , legamenti )  . 
inoltre , sullapice del dente sinseriscono tre legamenti : il legamento apicale del dente e i due legamenti alari [ 6 ]  . clinicamente , la sdi dovuta a depositi di ha [ 27 ] una condizione ben definita , ancorch rara , che colpisce donne giovani e di media et , caratterizzata da intensa cervicalgia p.n. 
computed tomography ( ct ) of the atlantoaxial region : images in the axial plane ( a , b ) and reformatted in the coronal ( c , d ) and sagittal planes ( e )  . 
tc atlo - epistrofica : scansioni sul piano assiale ( a , b ) e ricostruzione elettronico sul piano coronale ( c , d ) e sagittale ( e )  . 
in some cases , there may be involvement of the yellow ligaments and posterior longitudinal ligaments , with secondary myelopathy , spinal cord compression and vertebral stenosis [ 25 ]  . 
in particular , it is important to consider the cruciform ligament , which is composed of both part of the transverse ligament of the atlas and its vertical extensions ( superior and inferior longitudinal fibres )  . 
in addition , three ligaments are inserted on the dens apex : the apical ligament and the two alar ligaments [ 6 ]  . clinically , cds due to ha crystal deposits [ 27 ] is a welldefined , though rare , condition that affects young and middle - aged women and is characterised by intense cervical pain [ 28 ] that resolves within days or weeks after treatment with nonsteroid anti - inflammatory drugs ; it does not cause spinal compression [ 4 ]  . 
the clinical picture caused by cppd crystal deposits is more complex , as it may be asymptomatic or associated with a variety of clinical manifestations , some of which are severe [ 29 , 30 ] , such as spinal cord compression [ 31 , 32 ] related in some cases to a slightly calcific mass between the dens and the transverse ligament . 
crystal deposits can be found in older patients ( 5.7% ) with evident peripheral joint chondrocalcinosis [ 11 ] and advanced degenerative lesions of the atlantoaxial joint , and they tend to worsen with age [ 9 ]  . 
 in contrast with previous studies [ 24 , 7 , 12 ] that consider cppd crystal deposition disease as the most frequent form of crowned dens syndrome , only two women in our series [ 28 ] , risolvibile in un tempo variabile da pochi giorni ad alcune settimane con trattamento anti - infiammatorio non steroideo , senza causare compressione bulbare [ 4 ]  . 
il quadro clinico sostenuto , invece , dai cristalli di cppd pi complesso , perch pu essere asintomatico o associarsi a manifestazioni cliniche varie , talora anche gravi [ 29 , 30 ] , quali la compressione midollare [ 31 , 32 ] , determinata da una massa talora finemente calcifica localizzata tra il dente dellepistrofeo e il legamento trasverso . 
i depositi cristallini si osservano in pazienti pi anziani ( 5 , 7% ) , con evidente condrocalcinosi delle articolazioni periferiche [ 11 ] e lesioni degenerative avanzate dellarticolazione atlo - epistrofica e si aggravano con lavanzare dellet [ 9 ]  . 
 nella nostra casistica , in contrasto con la letteratura [ 24 , 7 , 12 ] che indica nella malattia di cppd levenienza pi frequente di sdi , solamente due casi entrambi di sesso femminile presentavano calcificazioni peri - odontoidee . una di queste ( et 69 anni ) denunciava dolore ad entrambe le ginocchia , dove lesame radiografico dimostrava la presenza di calcificazioni moniliformi a carico di entrambi i menischi . 
analoghe calcificazioni erano presenti nella cartilagine triangolare del polso . altre malattie associate alla sdi sono lar , la ra - dish [ 33 ] , le connettiviti sistemiche , le sequele di traumi , sublussazioni e lussazioni franche . 
in particolare , nellar linteressamento dello scheletro assile [ 34 ] risulta significativo nel tratto cervicale ( 60%80% dei casi ) ; esso pu essere asintomatico oppure manifestarsi con dolore , limitazione funzionale e sindromi neurologiche anche gravi [ 20 ]  . 
qualunque sia il distretto interessato , le lesioni anatomo - patologiche sono quelle tipiche della malattia , rappresentate dalla flogosi cronica della membrana sinoviale , con formazione successiva di erosioni ossee ed indebolimento strutturale delle zone dinserzione dei legamenti . 
computed tomography ( ct ) of atlantoaxial region , images in the axial plane ( a , b ) , and reformatted images in the coronal ( c ) and sagittal ( d ) planes . 
in one ( 69 years old ) , who had pain in both knees , radiography demonstrated minute mottled calcifications in the meniscus and in the triangular cartilage of the wrist , typical of cppd crystal deposit disease . the diseases associated with cds are ra , ra - dish [ 33 ] , systemic connectivitis , trauma , frank subluxations and luxations . 
ra in particular involves the axial skeleton [ 34 ] and especially the cervical region ( in 60%80% of cases ) ; this may be asymptomatic , or present with pain , functional impairment and even severe neurological syndromes [ 20 ]  . whatever the area involved , the lesions are pathologically those of ra : chronic inflammation of the synovial membrane , bone erosions and weakening of the ligament insertions . 
laxity of the articular capsule and atlantoaxial joint ligaments causes an abnormal separation ( more than 2.5 mm ) no in sede atlo - epistrofica , con secondarie alterazioni della stabilit e della funzionalit regionale : ostacolata rotazione del capo ed instabilit articolare secondo tre direttrici fondamentali ( anteriore , laterale e verticale )  . 
la lassit delle strutture capsulo - legamentose della giunzione atlo - epistrofica determina lallontanamento anomalo ( > 2 , 5 mm ) tra arco anteriore dellatlante e dente dellepistrofeo , dando luogo alla lussazione atlo - assiale [ 20 ]  . 
nella nostra casistica sono soprattutto i pazienti affetti da ar quelli che hanno denunciato la maggiore incidenza della sdi , con prevalenza del sesso femminile ( 10 femmine e 1 maschio ) , specie in quei casi affetti da malattia reumatica inveterata . lassociazione tra ar e calcificazioni legamentose periodontoidee risulta di non facile interpretazione , dato che non ancora identificato un rapporto di causa ed effetto , tenuto between the anterior arch of the atlas and the odontoid process , resulting in atlantoaxial luxation [ 20 ]  . 
the association between ra and periodontoid calcification is not easy to interpret in that no causal relationship has yet been identified in the light of the natural evolution of ra [ 36 ]  . 
 whereas ct is indicated for the study of cortical bone and periodontoid calcifications , mri with paramagnetic contrast material is the modality of choice for the study of synovial abnormalities , as it is the only technique able to demonstrate the inflamed pannus ( hypervascular , hypovascular and fibrous ) , articular effusion and cord compression [ 37 ]  . the diagnosis of cds is not always straightforward given the broad spectrum of presentations . 
nevertheless , ct can fail to detect cds , especially if it is carried out too late after an acute attack , because the calcifications may have been reabsorbed in the meantime [ 8 ]  . 
the characteristic ct pattern is a narrow and irregular horseshoe calcification surrounding the odontoid process , at times related to osteophytes in the upper margin of the anterior arch of the atlas , as well as calcification of the transverse ligament . 
the main calcification is often surrounded by other smaller calcifications at the apex of the dens [ 10 ]  . differential diagnosis includes calcification of the tendon of the longus colli muscle , where the clinical features of cds are accompanied by pharyngeal pain and dysphagia , incorrectly suggesting meningitis , spondylodiscitis or retropharyngeal abscess . 
other radiographic appearances not to be confused with cds are disc calcifications , calcified adenopathy , sesamoid bones in the transverse ligament , ossification of the common posterior vertebral ligament , and periatlantic calcifications [ 28 , 39 , 40 ]  . 
 [ 28 ] have described 23 cases , five cases and one case of cds , respectively , with clinical presentations varying from febrile nuchal pain ( in acute forms ) to spinal compression ( in chronic forms )  . 
 se la tc indicata per lo studio della corticale ossea e delle calcificazioni periodontoidee , la rm metodica elettiva per lo studio delle lesioni sinoviali , essendo lunica tecnica capace di visualizzare il panno infiammatorio ( ipervascolarizzato , ipovascolarizzato e fibroso ) , il versamento articolare e la compressione midollare , impiegando mezzo di contrasto paramagnetico [ 37 ]  . la diagnosi della sdi non sempre facile , dato lampio spettro di presentazione dellaffezione : infatti , altre manifestazioni cliniche , come la meningite , il dolore cervico - brachiale e lemicrania occipito - temporale , possono aggiungersi al classico episodio acuto febbrile di cervicalgia [ 1 ]  . con la tc la dimostrazione delle minute calcificazioni nellarea del processo odontoideo estremamente facilitato , con sensibilit superiore alla rm [ 38 ]  . 
tuttavia la tc pu fallire nella diagnosi di sdi , specie se questa eseguita tardivamente dopo lattacco acuto , perch nel frattempo le calcificazioni possono riassorbirsi [ 8 ]  . 
laspetto tc caratteristico quello di una sottile ed irregolare calcificazione a ferro di cavallo attorno al processo odontoideo , che in alcuni casi pu essere riferito , oltre che alla calcificazione del legamento trasverso , anche a neoformazioni osteofitosiche a carico del profilo superiore dellarco anteriore dellatlante . 
questa calcificazione principale spesso circondata da altre pi piccole , situate allapice del dente [ 10 ]  . la diagnosi differenziale va posta con le calcificazioni del tendine del muscolo lungo del collo , che oltre al quadro clinico della sdi associa dolore faringeo e disfagia che evocano a torto meningite , spondilodiscite o ascesso retrofaringeo . 
altri aspetti radiografici da non confondere con la sdi sono : le calcificazioni discali , le adenopatie calcifiche , la presenza di un sesamoide nel legamento traverso , lossificazione del legamento vertebrale comune posteriore , le ossificazioni soprannumerarie peri - atlantiche [ 28 , 39 , 40 ]  . 
treves [ 39 ] , constantin [ 7 ] e denes [ 28 ] hanno descritto , rispettivamente , 23 casi , 5 casie 1 caso caratterizzati da un quadro clinico variabile da episodi di nucalgia febbrile nelle forme acute a quadri di compromissione midollare nelle forme croniche . lo studio di treves [ 39 ] ha dimostrato , con lesame tc , la presenza di calcificazioni atlo - odontoidee nel 90% dei casi di sdi : 8 pazienti su 12 di questo gruppo non avevano mai p.n. 
evaluation with ct imaging [ 39 ] demonstrated with ct the presence of atlantoaxial calcifications in 90% of cases : eight of 12 patients had never suffered from neck pa therefore , in the presence of febrile cervical pain , the discovery of periodontoid calcifications suggests cds and excludes meningitis . conclusion in cds , ct is the gold standard imaging modality in that it allows identification of the different radiographic patterns of the disease : simple band of calcification or double band of thin calcifications in the transverse ligament , irregular calcifications crowning the dens apex , and bone erosions of the dens itself . 
however , radiography of other joints ( wrist , knee , pubic symphysis and shoulder ) can help establish whether the disease is due to cppd crystal deposit disease or ha crystals and is therefore recommended for routine patient management . 
although cds is traditionally associated with crystal deposition diseases , it may be accompanied by other diseases affecting the joints , such as ra with involvement of the proximal cervical spine ( as seen in our study ) , ra - dish , and other forms of systemic connectivitis ( systemic sclerosis )  . 
pertanto , in presenza di cervicalgia febbrile , la scoperta di calcificazioni periodontoidee suggestiva di sdi , escludendo quella di meningite . conclusione nella sindrome del dente incoronato la tc rappresenta lesame gold standard , permettendo di identificare i diversi aspetti radiografici : calcificazioni semplici a banda o in doppia filiera sottile in corrispondenza del legamento trasverso ; calcificazioni irregolari a corona sopra e intorno allapice del dente ; lesioni ossee di tipo erosive del dente stesso . 
invece lesame radiografico di altri distretti articolari ( carpo , ginocchio , sinfisi pubica , spalla ) pu agevolare il riconoscimento eziologico della malattia , se da cppd o da ha , ed pertanto raccomandato nella gestione routinaria del paziente . 
la sdi , infatti , tradizionalmente associata alle malattie da microcristalli , ma altre malattie articolari si accompagnano ad essa , in primis lartrite reumatoide con compromissione della colonna cervicale prossimale ( come si evince anche dalla nostra casistica ) , seguita dalla ra - dish e da altre connettiviti sistemiche ( sclerosi sistemica )  . 
obliquecoronal 3dvr images were significantly superior to obliquecoronal sts - mip images in the evaluation of vertebrobasilar vessels ( p < 0.05 ) ; in all other cases , 3dvr images were equivalent to sts - mip images . 
le immagini sono state valutate consensualmente da 2 radiologi con lintervento di un terzo radiologo per risolvere le discordanze al fine di classificare parametri relativi alla qualit delle immagini e alladeguadezza per la definizione della patologia . 
le immagini ottenute con tecnica sts - mip sono risultate significativamene superiori alle immagini ottenute con tecnica sts - mpr nella valutazione dei diversi parametri presi in esame ( p < 0 , 05 )  . 
le immagini riformattate con tecnica sts - mip dovrebbero far parte del protocollo standard per la valutazione dei vasi epiaortici e del distretto intracranico non tralasciando di analizzare le immagini sorgenti . 
le immagini riformattate con tecnica 3dvr rivestono invece un ruolo importante in una fase successiva in cui lidentificazione della patologia stata effettuata con le immagini sts - mip e sorgenti . parole chiave tc angio - tc arterie cervico - craniali g . 
previous studies have demonstrated that cta of the intracranial circulation is equivalent if not superior to conventional angiography in demonstrating intracranial aneurysms 4 mm in size or smaller [ 36 ] and that cta of the epiaortic vessels is equivalent to colour - doppler ultrasound ( us ) in measuring the degree of carotid stenosis [ 79 ]  . however , as there are numerous reformatting techniques of cta images currently available on processing workstations , and as they influence the final quality of the examination , the radiologist needs to be aware of the advantages and limitations offered by the various reformatting techniques in order to optimise the cta examination [ 2 ]  . 
the reformatting techniques of ct images should be distinguished from image reconstruction in that they do not alter the image voxels ( i.e. , the raw data ) but use projectional techniques to visualise the image voxels in orthogonal or arbitrary planes . 
projectional include multiplanar reformatting ( mpr ) , which can be combined with the maximum intensity projection ( mip ) algorithm for visualising pixels with maximum brightness , or the sliding - thin - slab ( sts ) technique for visualising sections with variable thickness . 
although the term image reconstruction is commonly used in place of reformatting , it should be borne in mind that image reconstruction is the procedure that transforms the acquired raw data into ct images . techniques with projectional techniques , the reformatted image is what the observer would see two - dimensionally from their observation point looking through the volume being studied . with this technique , the cta images are displayed two - dimensionally in orthogonal or arbitrary planes ( mpr ) , with the possible addition of the mip algorithm to highlight opacified vascular structures that , as with bone , present the maximum brightness of the pixels . 
in addition , to improve visualisation of vascular structures , the sts technique can be used to select voxel groups of varying thickness to include or exclude them from the image and improve assessment of the structures being studied . with the 3dvr technique , density values of the ct images are assigned with properties such as visibility or nonvisibility , transparency and colour to represent the various anatomical structures on the basis of the properties assigned . in this way , the reformatted image is what the observer would see three - dimensionally from their observation point looking at the volume as if it were illuminated by an external light source , thus enabling the vessels to be visualised through structures rendered invisible or more or less transparent . because assigning the properties of visibility , colour and transparency to voxels is predefined in the various workstalutilizzo di apparecchi di tomografia computerizzata multidetettore ( tcmd ) in ambito neuroradiologico ha consentito il notevole miglioramento dellesame angio - tc per la valutazione del circolo carotideo , vertebrale e intracranico in virt dellacquisizione con voxel isotropico submillimetrico e della possibilit di ottenere riformattazioni multiplanari degli assi vascolari [ 1 , 2 ]  . 
in letteratura stato dimostrato come langio - tc del circolo intracranico sia equivalente se non superiore allangiografia convenzionale nella dimostrazione degli aneurismi intracranici di 4 mm o inferiori [ 36 ] e come lesame angio - tc dei vasi epiaortici sia equivalente alleco - color doppler per la misurazione del grado di stenosi carotidea [ 79 ]  . tuttavia , poich le tecniche di riformattazione delle immagini angio - tc oggi disponibili sulle workstation di elaborazione sono molteplici e poich esse influenzano la qualit finale dellesame , necessario che il radiologo conosca i vantaggi e i limiti offerti dalle diverse tecniche di riformattazione per ottimizzare lesame angio - tc [ 2 ]  . 
le tecniche di riformattazione delle immagini tc vanno distinte dalle ricostruzioni delle immagini in quanto non alterano i voxel dellimmagine , ovvero i dati grezzi , ma consentono una visualizzazione su piani ortogonali o arbitrari dei voxel dellimmagine utilizzando tecniche di tipo proiettivo come la riformattazione multiplanare ( mpr ) che pu avvalersi dellalgoritmo di visualizzazione dei pixel con la massima intensit luminosa denominato maximun intensity projection ( mip ) o ancora della tecnica di visualizzazione a spessore variabile denominata sliding - thin - slab ( sts )  . 
bench nelluso comune il termine ricostruzioni delle immagini viene comunque utilizzato piuttosto che riformattazione necessario ricordare che la ricostruzione delle immagini il procedimento che consente di trasformare i dati grezzi acquisiti nelle immagini tc . attraverso le tecniche di visualizzazione di tipo proiettivo limmagine riformattata ci che losservatore vedrebbe in modo bidimensionale dal suo punto di osservazione guardando attraverso il volume in esame . 
con questa tecnica le immagini angio - tc vengono rappresentate in modo bidimensionale su piani ortogonali o arbitrari ( mpr ) aggiungendo eventualmente lalgoritmo mip per enfatizzare le strutture vascolari opacizzate che come losso presentano la massima intensit luminosa dei pixel . 
inoltre , per migliorare la visualizzazione delle strutture vascolari di interesse , possibile utilizzare la tecnica sts per selezionare gruppi di voxel con spessore variabile per includere o escludere nellimmagine rappresentata gruppi di voxel e migliorare la valutazione delle strutture di interesse . con le tecniche di visualizzazione 3d di volume ( 3dvr ) ai valori di densit delle immagini tc vengono invece assegnate propriet quali se visibili o meno , la trasparenza e il colore per rappresentare le diverse strutture anatomiche in base alle propriet assegnate . 
in this study , we compared cta images of the cervicocranial arteries reformatted with sts - mpr , sts - mip and 3dvr techniques . materials and methods the cervicocranial arteries of 20 patients ( 15 men and five women , age range 5576 years , mean 66 years ) referred for cta assessment of cerebrovascular disease in the period from october 2005 to january 2006 were reviewed . 
the volume acquisition was performed during administration of 90 ml of iodinated nonionic contrast agent at a concentration of 370 mg / ml through an antecubital vein , with an 18 - gauge needle cannula using an automatic injector ( envision , medrad , pittsburgh , pa , usa ) at a flow rate of 4 ml / s . 
to obtain optimal enhancement of the arteries , the delay time between beginning the contrast agent administration and scan acquisition was calculated with the bolus test technique by measuring the enhancement curve at one of the common carotid arteries . 
the acquisition volume was set in the caudocranial direction from the aortic arch to the vertex so as to include the epiaortic vessels and the circle of willis . scan parameters were 250 mas , 120 kv , collimation 400.625 mm , pitch 0.67 , gantry rotation time 0.5 s and acquisition time 10 s . image processing and assessment the images were processed on a dedicated workstation ( extended brilliance workspace , philips , best , the netherlands ) using a standard procedure to obtain the following reformatted images : sts - mip , sts - mpr and 3dvr reformatted images in the three orthogonal planes with a slice thickness of 38 mm for visualisation of the individual arterial branches of the circle of willis , and in the obliquecoronal plane parallel to the clivus with a slice thickness of 510 mm for the visualisation in a single plane of both the basilar artery and the vertebral arteries in the intracranial tract . curvilinear reformations were not performed in that this technique is highly operator dependent and therefore cannot be standardised . 
images were transferred to a pacs mensionale dal suo punto di osservazione guardando il volume in esame come se fosse illuminato da una fonte esterna che ne consente la visione attraverso strutture rese invisibili o pi o meno trasparenti . poich lassegnazione delle propriet di visibilit , colore e trasparenza ai voxel predefinita nelle diverse workstation in base al protocollo desame e al distretto anatomico esaminato lasciando margini di modifica dei parametri alloperatore , i risultati ottenuti sono intrinsecamente soggetti a variabilit in base alla workstation in uso e al grado di addestramento delloperatore contrariamente a quanto si ottiene con le tecniche di tipo proiettivo . 
in questo lavoro vengono confrontate le immagini angio - tc del distretto arterioso cervico - craniale riformattate con tecnica sts - mpr , sts - mip e 3dvr . materiali e metodi sono stati valutati gli esami angio - tc del distretto arterioso cervico - craniale di 20 pazienti ( 15 maschi e 5 femmine di et compresa tra 55 e 76 anni , et media 66 anni ) eseguiti nel periodo ottobre 2005 - gennaio 2006 su richiesta dello specialista neurologo per patologia cerebrovascolare . 
in 1 paziente era nota la dissecazione di entrambe le arterie carotidi comuni e interne con doppio lume documentato con esame eco - color doppler . in 1 paziente era nota la stenosi dellarteria oftalmica destra documentata con esame eco doppler . gli esami sono stati effettuati utilizzando un tomografo multistrato a 40 linee di detettori ( brillance ct , philips , best , olanda )  . 
lacquisizione volumetrica stata effettuata durante infusione di 90 ml di mdc iodato non ionico alla concentrazione di 370 mg / ml attraverso accesso venoso antecubiltale con agocannula da 18 g utilizzando un iniettore automatico ( envision , medrad , pittsburgh , usa ) con flusso di 4 ml / s . 
il tempo di ritardo tra linizio dellinfusione del mdc e laquisizione delle scansioni per ottenere lopacizzazione ottimale del distretto arterioso stato calcolato con la tecnica del bolus test misurando la curva di enhancement in corrispondenza di una delle arterie carotidi comuni . 
stato impostato il volume di acquisizione delle scansioni con direzione caudo - craniale dallarco aortico fino al vertice in modo da comprendere i vasi epiaortici e il poligono di willis . 
i parametri di scansione utilizzati sono stati : 250 mas , 120 kv , collimazione 400 , 625 mm , pitch 0 , 67 , tempo di rotazione 0 , 5 s , durata delle acquisizioni 10 s . elaborazione e analisi delle immagini le immagini sono state elaborate su workstation dedicata ( extended brillance workstation , philips , best , olanda ) utilizzando una procedura standardizzata per realizzare le seguenti riformattazioni : riformattazione sts - mip , sts - mpr g . 
the following parameters were rated for each examination and for each reformation technique ( sts - mip , sts - mpr and 3dvr ) using a scale from 1 to 5 : the possibility of tracing the middle cerebral arteries e 3dvr nei 3 piani ortogonali con spessore dello strato di 38 mm per la visualizzazione dei singoli rami arteriosi del poligono di willis e in proiezione coronale obliqua , con inclinazione del piano parallelo al clivus , spessore dello strato di 510 mm , per visualizzare in un unico piano sia larteria basilare che le arterie vertebrali nel tratto intracranico . non stata presa in considerazione la riformattazione curvilinea in quanto questa tecnica fortemente operatore - dipendente e quindi non standardizzabile . 
the values were considered significant for p < 0.05. results tables 2 and 3 summarise the results of the spearman rank test for the three image reformatting techniques ( sts - mip , sts - mpr and 3dvr ) in the assessment of the various parameters studied and the significance of the test . 
le immagini sono state valutate utilizzando parametri di visualizzazione standard ( ingrandimento del 50% ; valori di finestra compresi tra 200 e 250 uh ; livello / centro compreso tra 150 e 250 uh )  . 
per ciascun esame e per ciascuna tecnica di riformattazione ( sts - mip , sts - mpr e 3dvr ) sono stati classificati , utilizzando un scala di misura ordinale con punteggio da 1 a 5 , i seguenti parametri : possibilit di delineare le arterie cerebrali medie ( acm ) , le arterie cerebrali anteriori ( aca ) , le arterie cerebrali posteriori ( acp ) , larteria basilare ( ab ) , le arterie carotidi comuni ( acc ) , la biforcazione carotidea ( bc ) , le arterie carotidi interne ( aci ) , i sifoni carotidei ( sc ) e le arterie vertebrali ( av ) ( 5 = ramo arterioso delineato in tutta la sua estensione , 1 = ramo arterioso non riconoscibile o riconoscibile solo per breve tratto ) ; omogeneit dellopacizzazione dei vasi ( 5 = eccellente , 1 = non soddisfacente ) ; sovrapposizione di strutture ossee ( 5 = nessuna influenza , 1 = influente fino a impedire la visualizzazione dei vasi ) ; identificazione di calcificazioni parietali ( 5 = eccellente , 1 = non soddisfacente ) ; adeguatezza delle ricostruzioni per delineare la patologia ( 5 = adeguato , 1 = non soddisfacente )  . analisi statistica i risultati sono stati confrontati utilizzato il test dei ranghi di spearman che ha fornito la correlazione tra i punteggi ottenuti nella valutazione dei diversi parametri presi in esame con le diverse tecniche di riformattazione ( sts - mip , stsmpr e 3dvr )  . 
lipotesi nulla del test di spearman in questo caso che non vi siano differenze significative nei punteggi ottenuti nella valutazione dei diversi parametri presi in esame con le tre tecniche di riformattazione delle immagini ( ovvero che le diverse tecniche siano equivalenti ) mentre lipotesi alternativa che vi siano differenze significative tra le diverse tecniche nella valutazione dei parametri presi in esame . 
i valori sono stati considerati significativi per p < 0 , 05 . risultati in tabella 2 e 3 sono riportati i valori della correlazione di spearman per le tre tecniche di riformattazione delle immagini ( sts - mip , sts - mpr e 3dvr ) nella valutazione dei diversi parametri presi in considerazione e la significativit del test . 
in termini di omogeneit di opacizzazione dei vasi la riformattazione sts - mip risultata superiore sia alla sts - mpr che alla 3dvr ( p < 0 , 05 )  . 
circa ladeguatezza delle immagini rispetto la definizione della patologia , in generale le immagini sts - mip si sono dimostrate pi accurate delle altre immagini ( mip vs mpr p < 0 , 05 ; mip vs 3dvr p < 0 , 05 )  . a questo proposito bisogna fare alcune considerazioni : g . 
1a - c axial sliding - thin - slab ( sts ) multiplanar reformatting ( mpr ) ( a ) , sts maximum intensity projection ( mip ) ( b ) and three - dimensional volume rendering ( 3dvr ) computed tomography angiography ( cta ) images ( c ) of circle of willis . 
2a - c sagittal sliding - thin - slab ( sts ) multiplanar reformatting ( mpr ) ( a ) , sts maximum intensity projection ( mip ) ( b ) and three - dimensional volume rendering ( 3dvr ) computed tomography angiography ( cta ) images ( c )  . 
3a - f oblique - coronal three - dimensional volume rendering ( 3dvr ) ( a - c ) and d - f sliding - thin - slab ( sts ) maximum intensity projection ( mip ) images of vertebral arteries and basilar trunk . 
3a - f immagini sul piano coronale - obliquo 3dvr ( a - c ) e sts - mip ( d - f ) della biforcazione tra arterie vertebrali e arteria basilare . 
4a - d sagittal sliding - thin - slab ( sts ) maximum intensity projection ( mip ) a and b three - dimensional volume rendering ( 3dvr ) ; c coronal sts - mip and d 3dvr images of the carotids . 
la significativa riduzione di sovrapposizione di strutture ossee sulle immagini 3dvr rende pi agevole la valutazione del decorso degli assi carotidei . discussion ct angiography with mdct of epiaortic vessels and intracranial circulation has undergone considerable improvements in recent years as a result of technological advances in mdct scanners and image processing software now available on commercial workstations . 
nonetheless , there are areas of dispute regarding the diagnostic value of the various reformation techniques and their clinical use , which is still being assessed and undergoing standardisation [ 2 , 10 ]  . 
in addition , most studies published to date have centred their attention on the assessment of quantitative parameters , such as measurement of the degree of carotid artery stenosis with comparison of findings obtained with mip and mpr reconstructions [ 1114 ]  . 
per la valutazione del doppio lume ( punta di freccia ) ci si avvalsi sia delle immagini sts - mip che delle immagini sorgenti . discussione lesame angio - tc con tcmd dei vasi epiaortici e del circolo intracranico ha subito negli ultimi anni notevoli miglioramenti in funzione degli avanzamenti tecnologici delle apparecchiature tc multidetettore e del software di elaborazione delle immagini oggi ampiamente disponibile sulle workstation commerciali . 
tuttavia in letteratura esistono controversie circa il valore diagnostico delle diverse tecniche di riformattazione delle immagini e sul loro utilizzo clinico che ancora oggetto di valutazione e standardizzazione [ 2 , 10 ]  . 
peraltro la maggior parte dei lavori pubblicati incentra la sua attenzione sulla valutazione di parametri quantitativi come la misurazione del grado di stenosi delle carotidi comparando i risultati ottenuti con le ricostruzioni mip e mpr [ 1114 ]  . 
oltre alla riformattazione mip e mpr disponibile la riformattazione 3d con algoritmo vr , notevolmente migliorata grazie allacquisizione con voxel isotropico consentita dalla tcmd a 16 strati o superiori [ 1 , 2 ]  . 
le immagini sts sono state introdotte nella pratica clinica per lo studio tc del torace [ 1618 ] e successivamente per la valutazione angio - tc della vascolarizzazione del donatore di rene [ 19 ] e di fegato [ 2022 ]  . 
le immagini sts , che possono essere visualizzate con algoritmo mip o con la tecnica mpr , presentano come caratteristica saliente un elevato contrasto e una ridotta incidenza di artefatti da volume parziale [ 19 ]  . questa caratteristica legata al fatto che , a differenza delle fig . 
7a - f basilar artery aneurysaxial a sliding - thin - slab ( sts ) multiplanar reformatting ( mpr ) and b sts maximum intensity projection ( mip ) images . 
axial a sliding - thin - slab ( sts ) multiplanar reformatting ( mpr ) , b sts maximum intensity projection ( mip ) and c three - dimensional volume rendering ( 3dvr ) images of the circle of willis . 
sagittal a sliding - thin - slab ( sts ) multiplanar reformatting ( mpr ) , b sts maximum intensity projection ( mip ) c and three - dimensional volume rendering ( 3dvr ) images . 
grossolane calcificazioni del sifone carotideo ( punta di freccia ) meglio apprezzabili nelle immagini sts - mip . provement thanks to acquisition with isotropic voxels made possible with 16 - slice or more mdct [ 1 , 2 ]  . more recently , the sts technique has been used [ 15 ]  . 
sts images were introduced into clinical practice in chest ct studies [ 1618 ] and later for cta assessment of kidney vascularisation [ 19 ] and liver donors [ 2022 ]  . 
this characteristic is related to the fact that in contrast to mip , mpr or 3dvr images , the sts technique involves selection of a very thin volume to be examined and therefore a very limited number of voxels with respect to the entire volume , thus reducing the interference of partial volume and the overlapping of other structures [ 19 , 23 , 24 ]  . 
poich lalgoritmo mip seleziona i pixel con soglia luminosa elevata , le immagini sts - mip sono pi adatte alla valutazione delle placche calcifiche rispetto le immagini sts - mpr [ 2 , 25 ]  . 
10a - i immagini riformattate sul piano assiale con algoritmo mip con spessore variabile ( sts ) da a 0 , 7 mm a i 3 , 4 mm con incremento di 0 , 3 mm ( a - i ) in corrispondenza delle arterie cerebrali medie . results of our study reveal some of the features of the reformatting planes used . 
it should be borne in mind that with the use of the oblique coronal plane adopted for this study , visualisation of the vertebrobasilar plane is easier given the possibility of displaying the vertebrobasilar axis completely and in a single plane . 
the aim of the study in fact was not comparison of diagnostic accuracy between cta and conventional angiography or colourdoppler us , which has already been established in the literature [ 39 ]  . 
this choice was prompted because by optimising arterial enhancement with the bolus test technique , we deliberately overlooked the venous district , thus avoiding possible interferences in the images , a feature not taken into consideration in other similar studies [ 23 ]  . opportuno ricordare che sono disponibili altre tecniche di analisi vascolare , denominate in modo diverso a seconda delle workstation di elaborazione in uso , quali ladvanced vessels analysis ( ava ) disponibile su workstation extended brillance philips , che permette di effettuare misurazioni quantitative del grado di stenosi e la riformattazione curvilinea . 
the aim of this study was to evaluate magnetic resonance imaging ( mri ) patterns in the affected vertebrae before and after vertebroplasty by determining changes in signal intensity and size and distribution of bone cement within the vertebra at follow - up carried out at 1 week , 6 months and 12 months . 
acrylic cement appears as an intraspongy focal area of t1 and t2 hypointensity that is mostly oval ( 34% ) or rounded ( 26.8% ) ; this appearance tends to become stable 6 months after treatment . 
la conoscenza delle modificazioni nel tempo del cemento e la reazione del tessuto osseo limitrofo fondamentale per una corretta interpretazione dellimaging post vertebroplastica . parole chiave vertebroplastica polimetilmetacrilato rm radiologia interventistica introduction introduzione first described by herv deramond in 1984 , percutaneous vertebroplasty ( pvp ) has undergone progressive technical and methodological refinement over the past few years , and now , many centres have adopted this procedure with success [ 1 , 2 ]  . 
the injection can be performed via posterior or lateral transpedicular approach in the lumbar spine , transpedicular or intercostal - transverse approach in the dorsal spine and anterolateral approach in the cervical spine [ 6 , 7 ]  . 
the aim of the procedure is to stabilise the vertebra , relieve pain , and improve patient mobility [ 8 ]  . awareness of the main imaging changes arising in treated vertebrae is therefore fundamental , and magnetic resonance imaging ( mri ) is the most widely used modality for examinations before and after treatment [ 9 , 10 ]  . 
the aim of this study was to evaluate mri patterns before and after vertebroplasty to document changes in signal intensity and size and distribution of bone cement within the treated vertebra [ 11 ]  . materials and methods between january and october 2004 , 14 nonconsecutive patients ( nine women and five men , age range 3589 years ) were examined for a total of 41 pathological vertebrae . 
candidates for the procedure were selected in accordance with eligibility criteria of the american college of radiology [ 12 ]  . to evaluate the imaging changes after pvp , all patients underwent mri at baseline and 1 week and 1 , 6 and 12 months after treatment [ 13 , 14 ]  . 
the imaging protocol used consisted of t1 - weighted spin - echo ( se ) sequences ( tr 400 , minimal te , slice thickness 4 mm , interval 0.5 mm , fov 31 cm , examination time 2 h 40 min ) , t2 - weighted se sequences ( tr 2 , 350 ms , te 103.5 ms , slice thickness 4 mm , interval 0.5 mm , fov 31 cm , examination time 4 min 04 s ) and t2weighted short tau inversion recovery ( stir ) sequences ( tr 3 , 000 ms , te 23 ms , slice thickness 4 mm , interval 0.5 mm , fov 31 cm , examination time 4 h ) ; all images were acquired in the sagittal plane . 
 mri signal intensity was evaluated in three distinct regions of the vertebra , before and after treatment ( at baseline , at 1 week and at 1 , 6 and 12 months ) by manually placing regions of interest ( rois ) within the vertebral body . 
these measurements , which expressed absolute roi values , were made at the periphery of the vertebral body , in the area adjacent to the treated area and in the treated area itself , at baseline and rela vpp consiste nelliniezione di polimetilmetacrilato ( pmm ) ( un cemento sintetico che polimerizza rapidamente , a temperatura ambiente , con una reazione esotermica ) , sotto guida tc e / o fluoroscopica , allinterno di un corpo vertebrale divenuto patologico a causa di osteoporosi [ 3 ] , metastasi , angiomi , mieloma multiplo o trauma [ 4 , 5 ]  . 
liniezione pu essere eseguita , a seconda del tratto di colonna vertebrale interessato dal processo patologico , per via trans - peduncolare posteriore o laterale nel tratto lombare , trans - peduncolare o intercosto - trasversa nel segmento dorsale e con approccio antero - laterale nel segmento cervicale [ 6 , 7 ]  . 
il fine ultimo della procedura quello di stabilizzare la vertebra , ridurre la sintomatologia dolorosa ed eventualmente di migliorare , come conseguenza , la mobilit del paziente [ 8 ]  . a tal proposito fondamentale descrivere e saper riconoscere le principali modificazioni della vertebra trattata con particolare rilievo allimaging post vpp ; tra le varie metodiche utilizzate nei controlli prima e dopo il trattamento la risonanza magnetica ( rm ) sicuramente la pi utilizzata [ 9 , 10 ]  . scopo del nostro lavoro stato quello di valutare e descrivere la semeiotica rm prima e dopo vertebroplastica , al fine di documentare le modificazioni dellintensit del segnale , delle dimensioni e della distribuzione del cemento allinterno della vertebra trattata [ 11 ]  . materiali e metodi tra gennaio e ottobre 2004 , sono stati esaminati 14 pazienti non consecutivi per un totale di 41 vertebre patologiche : i pazienti di cui 9 donne e 5 uomini , avevano unet compresa tra 35 e 89 anni . 
al fine di valutare le modificazioni dellimaging dopo vpp , tutti i pazienti sono stati studiati con esame rm prima del trattamento e seguiti nel tempo con esami di follow - up a distanza di 1 settimana , 1 , 6 e 12 mesi dal trattamento [ 13 , 14 ]  . 
i pazienti trattati erano affetti da : osteoporosi ( 8 / 14 casi , 57% ) [ 15 ] , mieloma multiplo ( 3 / 14 casi , 21 , 5% ) e fratture post - traumatiche ( 3 / 14 casi , 21 , 5% )  . le procedure di vertebroplastica sono state eseguite mediante approccio trans - peduncolare monolaterale in tutti i pazienti . 
il protocollo di studio ha previsto lutilizzo di sequenze se t1 pesate ( tr 400 , te minimo , spessore dello strato 4 mm , intervallo 0 , 5 mm , fov 31 cm , tempo di esame 2 min e 40 s ) , sequenze se t2 pesate ( tr 2350 ms , te 103 , 5 ms , spessore dello strato 4 mm , intervallo 0 , 5 , fov 31 cm , tempo esame 4 min e 4 s ) e sequenze stir t2 pesate ( tr 3000 ms , te 23 ms , spessore dello strato 4 mm , intervallo 0 , 5 , fov 31 cm , tempo di esame 4 min ) ; tutte le immagini sono state acquisite nel piano sagittale . la valutazione delle immagini rm stata eseguita , per consenso , da due radiologi e sono state prese in considerazione le caratteristiche dellintensit di segnale , le modalit r . 
intensit del segnale rm : stata valutata lintensit del segnale in tre differenti regioni della vertebra , prima e dopo il trattamento ( 1 settimana , 1 mese , 6 mesi e 12 mesi ) mediante il posizionamento manuale di aree roi nel contesto del corpo vertebrale . 
tali misurazioni , espressione di valore roi assoluto , sono state effettuate a livello della parte periferica della vertebra , della zona limitrofa allarea trattata ed a livello dellarea trattata . 
a seconda del loro aspetto morfologico , le vertebre sono state inoltre classificate , secondo la semeiotica classica prima e dopo il trattamento , in vertebra plana , vertebra con avvallamento della limitante somatica superiore , con avvallamento della limitante somatica inferiore e vertebra con aspetto a lente biconcava . 
i dati ottenuti sono stati elaborati mediante test statistico t di student , con ic del 95% . risultati la valutazione stata effettuata su un numero complessivo di 41 vertebre trattate di cui 10 dorsali ( quattro d11 e sei d12 ) , 31 lombari ( nove l1 , sei l2 , sette l3 sei l4 e tre l5 )  . relativamente alla distribuzione del cemento nel contesto del soma della vertebra trattata , la distribuzione disomogenea stata riscontrata nel 26 , 8% nel controllo dopo una settimana del trattamento e nel 12 , 2 % dopo 1 mese dal trattamento ; la distribuzione omogenea non stata mai evidenziata ; la distribuzione puntiforme del cemento stata riscontrata nel 7 , 3% dei casi dopo 1 settimana e dopo 1 mese dal trattamento ; la distribuzione a carta geografica stata evidenziata nel 14 , 6% dei casi dopo una settimana ed stata riscontrata nel 19 , 5% dei casi ad un mese dal trattamento ; la distribuzione ovalare del cemento , presente nel 21 , 9% dopo una settimana stata riscontrata nel 34 , 1% ad un mese dal trattamento mentre la distribuzione rotondeggiante , presente nel 29 , 2% dei casi ad 1 settimana , era presente nel 26 , 8% dei casi ad un mese dal trattamento ( tabella 1 )  . 
la morfologia della distribuzione del cemento osservata nel contesto del soma vertebrale a distanza di un mese dal trattamento non si in seguito modificata nei successivi controlli a sei mesi e ad un anno dal trattamento . relativamente al parametro delle altezze dei somi vertebrali , il test statistico ha evidenziato : una deviazione stanfig . 
liperintensit che circondava il cemento appare ridotta ad un esile alone . dard media di 17 , 1 nel pre - vertebroplastica e di 16 , 7 nel post - vertebroplastica in corrispondenza del muro anteriore ; una deviazione standard media di 11 , 4 pre - vertebroplastica e di 11 , 0 nel post - vertebroplastica in corrispondenza della porzione centrale del soma ; una deviazione standard media di 19 , 3 pre - vertebroplastica e di 18 , 8 nel post - vertebroplastica in corrispondenza del muro posteriore ( tabella 2 )  . 
before and after treatment , vertebrae were morphologically classified according to classic imaging patterns into vertebra plana , vertebra with concavity of the superior endplate , vertebra with concavity of the inferior endplate and biconcave vertebra . 
data obtained were processed using the students t test with 95% confidence interval ( ci )  . results a total of 41 vertebrae , ten dorsal ( four d11 and six d12 ) and 31 lumbar ( nine l1 , six l2 , seven l3 , six l4 and three l5 ) , were evaluated . 
c osteoporosi ( 12 mesi dopo vpp ; stir t2w ) l1 - l2 : lipointensit del cemento appare invariata , mentre apprezzabile una marcata riduzione dellalone di iperintensit dovuta alledema circostante . 1 month ; in no case was it homogeneous . 
la valutazione dellintensit del segnale con posizionamento di una roi perifericamente allarea trattata ha dimostrato : nelle sequenze se t2 prima del trattamento un valore medio di 80 , 658 , 30 , ad una settimana dal trattamento un valore di 101 , 678 , 34 , ad un mese dal trattamento un valore medio di 125 , 335 , 5 , a sei mesi dal trattamento un valore medio di 100 , 208 , 42 , ad un anno dal trattamento un valore medio di 98 , 518 , 91 . stata rilevata una variabilit statisticamente significativa nella modifica dellintensit del segnale esclusivamente nelle sequenze t1 ( p = 0 , 002 , < 0 , 05 ) mentre non sono emerse differ . 
nel controllo a 1 mese e a 6 mesi non sono state notate variazioni frequenza della morfologia post - vertebroplastica 1 settimana , n ( % ) post - vertebroplastica 1 , 6 , 12 mesi , n ( % ) concavity were observed in 31% and 29% of cases , respectively , whereas vertebra with inferior endplate concavity and vertebra plana were detected in 19% and 21% of cases , respectively ; these percentages remained unchanged before and after vertebroplasty . 
 results of the evaluation of signal intensity based on the roi positioned peripherally to the treated area were as follows : a mean value of 140.255.20 at baseline , 148.675.79 at 1 week , 206.59.5 at 1 month , 163.339.83 at 6 months and 163.359.88 at 12 months in t1 - weighted se sequences ; a mean value of 82.256.20 at baseline and 113.256.22 at 1 week , 134.51.5 , at 1 month 60.750.83 at 6 months and 61.510.91 at 12 months in t2 - weighted stir sequences ; and a mean value of 80.658.30 at baseline and 101.678.34 at 1 week , 125.335.5 at 1 month , 100.208.42 at 6 months and 98.518.91 at 12 months in t2 - weighted se sequences . 
levoluzione e la diffusione della vertebroplastica impone la conoscenza delle principali variazioni del soma trattato con le varie metodiche di imaging ; ci al fine di valutare e correttamente interpretare limaging dopo trattamento [ 21 ]  . 
considerata la diffusione della rm nello studio del rachide cervico - dorso - lombare e lincidenza degli esami rm abbiamo focalizzato la nostra attenzione alla descrizione delle modificazioni delle modificazioni rm del comportamento della vertebra trattata [ 22 ]  . al fine di approfondire le modificazioni del segnale rm dopo vertebroplastica abbiamo analizzato la vertebra trattata prima del trattamento ed a distanza di un mese , sei mesi ed un anno dal trattamento , valutando sia la morfologia sia le alterazioni di intensit del segnale ; tali reperti sono fondamentali in rm ai fini descrittivi e per la comprensione delle variazioni indotte dal trattamento . 
with regard to vertebral size , the material injected into the vertebra could have produced either vertebral expansion increase in size and consequent morphological changes or diffusion of the cement within the vertebra with little or no effect on size . 
this demonstrates that the acrylic cement distributes diffusively within the spongy bone trabeculae , causing no appreciable bone expansion ; it also shows that restoration of normal vertebral size and morphology should not be expected on postvertebroplasty mri . 
si evince , pertanto , che il cemento acrilico si distribuisce nelle trabecole della spongiosa ossea del soma vertebrale con un comportamento diffusivo , senza un reale e consistente effetto di espanso e che il ripristino delle dimensioni della vertebra e della sua normale morfologia non debbano essere considerati degli elementi attesi allimaging rm nel post trattamento . relativamente alla valutazione della intensit del segnale , abbiamo notato , in accordo con la letteratura [ 22 , 23 ] , una variazione di essa nelle regioni periferiche allarea trattata correlabile a presenza di edema intra - spongioso . 
lanalisi dei risultati suggerisce , quindi , che il comportamento del segnale atteso nellarea limitrofa al cemento debba presupporre un modesto incremento della intensit in t1 e in t2 dopo trattamento , che tale incremento del segnale cominci ad essere rilevato sin dalla prima settimana dopo la procedura e che divenga pi evidente nei controlli ad un mese dal trattamento per poi stabilizzarsi , con riduzione della sua intensit a sei mesi e a dodici mesi dal trattamento . 
i dati derivanti dal confronto delle dimensioni delle vertebre non sono risultati statisticamente significativi per la presenza di un p > 0 , 05 . signal intensity between t1 and t2 sequences before and after treatment were not statistically significant . 
 vertebroplasty is a minimally invasive procedure indicated for the treatment of neck and arm pain , chest pain and back pain caused by vertebral collapse due to osteoporosis [ 3 , 8 ] , metastases , invasive angiomas and myelomas . 
clinical studconclusions controllo a sei mesi dal trattamento e che il segnale rimasto invariato ad un anno . per quanto riguarda la distribuzione del cemento i reperti morfologici pi frequenti sono rappresentati dalla distribuzione ovalare e rotondeggiante ; la prima stata riscontrata nel 21 , 9% dopo una settimana e nel 34 , 1% ad un mese dal trattamento mentre la seconda presente nel 29 , 2% dei casi ad 1 settimana presente nel 26 , 8% ad un mese dal trattamento . conclusioni la vertebroplastica una metodica terapeutica mini - invasiva che ha la sua indicazione elettiva , ove la terapia medica risulti inefficace , nel trattamento delle cervico - brachialgie , delle toracoalgie , delle lombalgie dovute a crolli vertebrali da osteoporosi [ 3 , 8 ] ed indicata per altre cause di crolli vertebrali ( metastasi , angiomi invasivi e mielomi )  . 
nellimaging pree post - vertebroplastica la risonanza magnetica considerata metodica di riferimento [ 10 ] per la valutazione corretta del contenente e del contenuto ; in particolare per la capacit della metodica ies have demonstrated an immediate improvement in symptoms and quality of life [ 11 , 14 ] following treatment . 
in preand post - vertebroplasty imaging , mri is considered the reference standard [ 10 ] due to its ability to correctly evaluate both container and content and assist in patient selection by excluding those cases showing ependymal infiltration by secondary lesions . 
the information provided by mri [ 21 ] is instrumental in the evaluation of both the efficacy and possible complications of pvp [ 9 ] , and awareness of the stages influencing post - vertebroplasty mri is fundamental . 
 in our experience , post - vertebroplasty mri is characterised by three main features : the signal from the cement , the signal from the area adjacent to the cement and the effect produced on vertebral size and morphology . 
acrylic cement appeared as an oval ( 34% ) or rounded ( 26.8% ) focal area within the spongy bone , and this appearance tended to stabilise 6 months after treatment . 
 bone marrow oedema in the area adjacent to the cement [ 22 , 23 ] was also observed in our experience ; in particular , it was evident 1 week to 6 months after treatment and tended to stabilise with only moderate residual hyperintensity in t2 in the following period . 
stability of vertebral size after treatment is the result of the diffusive as opposed to expansive cement distribution pattern within the spongy bone , which means that there is no change in shape or size of the vertebra after treatment . 
le informazioni che la rm [ 21 ] in condizione di fornire sono , quindi , fondamentali sia ai fini della valutazione dellefficacia del trattamento che delle eventuali complicanze della vpp [ 9 ] ; pertanto opportuno puntualizzare le tappe che condizionano limaging rm dopo vertebroplastica . dalla nostra esperienza limaging rm dopo vertebroplastica caratterizzato da tre elementi fondamentali : il segnale del cemento , il segnale dellarea limitrofa alla localizzazione del cemento , leffetto indotto dalla procedura sulle dimensioni e sulla morfologia della vertebra . 
il cemento acrilico si presenta come una area focale intraspongiosa di forma prevalentemente ovalare ( 34% ) , rotondeggiante ( 26 , 8% ) e tale aspetto tende a stabilizzarsi dopo sei mesi dal trattamento . 
il razionale di tale comportamento del segnale del cemento indotto dalla carenza di spettro di idrogeno nel materiale amorfo e pu porre problemi di diagnosi differenziale o con residui ferromagnetici intraspongiosi da trattamento chirurgico o con presenza in sede intraspongiosa di materiali in grado di produrre artefatti di fase ( ad esempio il titanio ) , con emangiomi con componente cavernosa intraspongiosa ( in t1 ) , con fenomeni di vacuum intraspongiosi ; a tal proposito una corretta anamnesi fondamentale per linquadramento del paziente . latteso edema della spongiosa ossea nellarea limitrofa al cemento , descritto dalla letteratura [ 22 , 23 ] , stato riscontrato anche nella nostra esperienza ; in particolare abbiamo verificato come esso sia evidente soprattutto tra una settimana e sei mesi dal trattamento e tenda a stabilizzarsi nel periodo successivo con modesto residuo di iperintensit in t2 . 
simonetti universit degli studi di roma tor vergata , dipartimento di diagnostica per immagini e radiologia interventistica , policlinico universitario tor vergata , viale oxford 81 , i - 00133 roma , italy correspondence to : e . 
turbo spin echo ( tse ) t1 - , t2and t2spectral selection attenuated inversion recovery ( spair ) weighted imaging and spectroscopy for the selective evaluation of water and fat content were performed . 
the anisotropic study and the subsequent assessment of colour and vector maps can provide a noninvasive tool for assessing the risk of fracture due to osteoporosis . key words osteoporosis vertebral collapse 3 - tesla mr diffusion imaging tractography riassunto obiettivo . 
il calcolo dellanisotropia e la valutazione grafica colorimetrica e vettoriale forniscono un nuovo strumento non invasivo per valutare losteoporosi vertebrale . parole chiave osteoporosi frattura vertebrale rm a 3 tesla immagini in diffusione trattografia introduction introduzione bone mineral density ( bmd ) is perhaps the best index available for assessing the risk of osteoporotic fracture . 
these figures have been confirmed by other clinical studies that showed that the risk of a new fracture within the first year of a previous compression fracture increases from 5 to 25 times [ 2 ]  . 
hanno riportato che ad ogni riduzione di una deviazione standard della bmd corrisponde un aumento del 60% del rischio di frattura vertebrale [ 1 ]  . tali dati sono stati inoltre confermati da ulteriori studi clinici in cui si dimostrato che il rischio di una nuova frattura vertebrale entro il primo anno da una precedente frattura e . 
the aim of this study was therefore to assess the possibility of a multiparameter characterisation , and not only imaging , of vertebral osteoporosis using 3 - tesla ( t ) mr . compressiva aumenta dalle 5 alle 25 volte [ 2 ]  . 
lo scopo del nostro lavoro pertanto quello di valutare la possibilit di una caratterizzazione multiparametrica , e non solo di imaging , dellosteoporosi vertebrale mediante rm a 3 tesla . materials and methods in our study , 30 subjects underwent an mr examination of the lumbar spine . 
these included ten healthy volunteers ( three men and seven women ) aged between 31 and 68 years without metabolic bone diseases ( in particular , osteoporosis t - score - 1 ) or neoplastic disease in any district ; ten female patients aged between 55 and 78 years with osteoporosis ( t - score - 2.5 ) but without vertebral fractures identifiable with conventional radiology ; and ten female patients aged between 60 and 75 years with a single osteoporotic lumbar vertebral fracture identified in a prior radiographic examination of the spine and with dual x - ray absorptiometry ( dexa ) positive for osteoporosis , a negative history of recent traumatic events and the absence of other metabolic and neoplastic bone diseases . 
all patients were informed of the experimental nature of the examination , and they all signed informed consent before undergoing the study . the morphological , metabolic and functional images were acquired with a high - field device ( 3.0 t ) ( philips intera achieva , best , netherlands ) , with a maximum gradient strength and slew rate set to 80 mt / m and 200 mt / m / ms , respectively , using a body coil for signal transmission and a synergy spine phased - array coil for signal reception . 
 the study of the lumbar spine was performed with the following sequences : t2 - weighted turbo spin echo ( tse ) in the sagittal plane the entire including lumbarsacral tract ( tr shortest , te 120 ms , slice thickness 4 mm with an interval between the sections of 0.4 mm , fov 300 mm and a 512512 matrix ) the acquisition volume t1 - weighted tse in the sagittal plane ( tr shortest , te 7.2 ms , slice thickness 4 mm with an interval between sections of 0.4 mm , fov 300 mm and a 512512 matrix ) t2 - weighted tse with selective fat suppression [ spectral selection attenuated inversion recovery ( spair ) ] in the sagittal plane aimed at assessing the presence of bone marrow oedema , an index of recent fracture in collapsed vertebral bodies and of algodystrophic changes in response to biomechanical stress in noncollapsed vertebral bodies . on the basis of the t2 - weighted images , especially the spair images , two independent observers identified the vertebral bodies with altered signal intensity , which were selected for placement of the spectroscopy acquisition volume . spectroscopic acquisition in the healthy subjects was optimised in the mid - lumbar vertebral bodies in accordance with the literature . 
the volume of interest ( voi ) for spectroscopic analysis was chosen on the basis of the t2 and t2materiali e metodi nel nostro studio sono stati sottoposti ad esame rm del rachide lombare 30 soggetti : 10 volontari sani ( 3 maschi e 7 femmine ) , di et compresa tra 31 e 68 anni , esenti da patologie metaboliche dellosso ( in particolare osteoporosi , t - score - 1 ) e da patologie neoplastiche di qualsiasi distretto ; 10 pazienti di sesso femminile di et compresa tra 55 e 78 anni con osteoporosi ( t - score - 2 , 5 ) ma esenti da fratture vertebrali evidenziabili con esami di radiologia tradizionale ; 10 pazienti di sesso femminile di et compresa tra 60 e 75 anni con frattura vertebrale lombare singola a genesi osteoporotica , evidenziata ad un precedente esame radiografico del rachide e dexa positiva per osteoporosi , anamnesi negativa per eventi traumatici recenti , in assenza di altre patologie metaboliche e neoplastiche dellosso . 
tutti i pazienti sono stati informati sul carattere sperimentale dellesame ed hanno firmato un consenso prima di essere sottoposti allindagine . le immagini morfologiche , cos come quelle metaboliche e funzionali , sono state acquisite con unapparecchiatura ad alto campo ( 3 , 0 tesla ) ( philips intera achieva , best , netherlands ) equipaggiata con gradienti di ampiezza massima e tempo di salita di 80 mt / m e 200 mt / m / ms rispettivamente , utilizzando la bobina del corpo per la trasmissione degli impulsi di eccitazione e una bobina sinergy spine phased - array per la ricezione del segnale . lo studio del rachide lombare stato eseguito mediante le seguenti sequenze : tse t2 pesata sul piano sagittale includendo nel volume dacquisizione lintero tratto lombo - sacrale ( tr shortest , te 120 ms , spessore di sezione 4 mm con intervallo tra le sezioni di 0 , 4 mm , fov di 300 mm e una matrice di 512512 ) ; tse t1 pesata sul piano sagittale ( tr shortest , te 7 , 2 ms , spessore di sezione 4 mm con intervallo tra le sezioni di 0 , 4 mm , fov di 300 mm , matrice di 512512 ) ; tse t2 pesata con soppressione selettiva del segnale del tessuto adiposo ( spair ) sul piano sagittale , al fine di valutare leventuale presenza di edema intraspongioso , indice di frattura recente per i somi vertebrali crollati e di trasformazione da sostituzione algodistrofica per adattamenti intrinseci da sofferenza biomeccanica per quelli non crollati . sulla base delle immagini t2 pesate , soprattutto spair , sono state individuate da due osservatori indipendenti le vertebre con alterata intensit di segnale , selezionate per il successivo posizionamento del volume di acquisizione spettroscopica . 
acquisition was performed with a point - resolved spectroscopy ( press ) sequence ( double spin - echo point resolved spatially localised spectroscopic sequence ) with the two - dimensional ( 2d ) technique and echo time ( 40 ms ) optimised for quantitative assessment of water and fats , with single voxel analysis . field homogeneity was adjusted through an automatic procedure of localised three - dimensional ( 3d ) shimming . 
the following acquisition parameters were used : tr 2 , 000 ms , te 40 ms , spectral width 2.00 hz , matrix 512512 , nominal voxel resolution 25 mm25 mm15 macquisition time of the spectroscopy sequence was on average 2 min for each vertebral body examined . we performed three acquisitions with voxels positioned at the level of l2 , l3 and l4 in healthy patients and osteoporotic patients without vertebral collapse . 
the spectra obtained were processed with fourier transformation . the fat content was expressed as the percentage of the fat signal intensity in respect to total signal intensity ( fat fraction : ff )  . 
a p value lower than 0.05 was considered statistically significant . diffusion - weighted ( dw ) images were acquired with single - shot spin - echo echoplanar imaging ( se - epi ) in the sagittal plane , with a duration of 35 s ( tr 3 , 500 ms , te 62 ms , fov 200 mm , flip angle 90 , matrix 256256 , b - value set to 0 and 400 mm2 / s , three sections 5 - mm thick with a 1 - mm gap )  . 
the apparent diffusion coefficient ( adc ) was calculated by positioning regions of interest ( rois ) in the vertebral bodies examined with spectroscopy of varying size so as to almost entirely cover the body . 
the diffusion tensor images were acquired with the same technique and using the same acquisition parameters , with sampling of the random motion of free water in 32 directions in space ( directional resolution high )  . 
acquisition time was about 2 min . the fractional anisotropy ( fa ) was then calculated , a parameter that describes the degree of variation of diffusion in space ( a value between 0 = highly isotropic with the direction of water molecule diffusion being highly random , and 1 = anisotropic , with the preferential motion of water molecules being highly directional ) and the main direction of water molecule diffusion . 
this parameter , which can be derived from the tensor , is linked with the possibility of mapping the spatial orientation of tissue structures ; the technique is also known as fibre tracking or tractography [ 3 ]  . images obtained with the diffusion tensor imaging ( dti ) sequence were first analysed on the acquisition console to identify the presence of motion artefacts and image distortions related to the presence of eddy currents . 
lacquisizione stata effettuata con sequenza press ( double spin - echo point - resolved spatially localized spectroscopic sequence ) con tecnica bidimensionale ( 2dsi ) e tempo di eco ( 40 ms ) ottimizzato per la valutazione quantitativa dellacqua e dei lipidi , con analisi single voxel . lomogeneizzazione del campo magnetico stata effettuata con una procedura automatica di shimming tridimensionale localizzato . 
i parametri di acquisizione utilizzati sono stati i seguenti : tr 2000 ms , te 40 ms , ampiezza spettrale 2000 hz , matrice di 512512 , risoluzione nominale del voxel di 25 mm25 mm15 mil tempo di acquisizione della sequenza spettroscopica stato in media di 2 minuti per ogni corpo vertebrale in esame . nei pazienti sani ed in quelli osteoporotici senza crollo vertebrale sono state effettuate tre acquisizioni con voxel posizionati a livello di l2 , l3 ed l4 . 
il coefficiente di diffusione apparente ( adc ) stato calcolato posizionando delle rois nel contesto dei corpi vertebrali gi sede dellanalisi spettroscopica , di dimensioni variabili in modo da comprendere quasi completamente lintero soma . 
le immagini del tensore di diffusione sono state acquisite con la medesima tecnica , utilizzando i medesimi parametri di acquisizione , campionando i movimenti casuali dellacqua libera su 32 direzioni dello spazio ( directional resolution high )  . 
la durata dellacquisizione stata di circa 2 minuti . stato quindi calcolato il grado di anisotropia ( fractional anisotropy : fa ) , che descrive la entit di variazione della diffusione nello spazio ( valore compreso tra 0 = altamente isotropico con direzione di diffusione delle molecole di acqua assolutamente casuale , e 1 = anisotropico , con movimento preferenziale delle molecole di acqua altamente direzionato ) , e la direzione principale di diffusione delle molecole di acqua . 
data were then processed with a dedicated software package ( pride v4 fiber tracking 4.1 , idl , research systems , boulder , co , usa )  . a single rectangular roi was positioned on the images acquired with the b - value set to 0 in the same vertebral bodies assessed with spectroscopy imaging ( using the criteria for analysis of the morphological images mentioned above )  . all rois were then automatically transposed onto the corresponding image on the grey - scale maps of mean diffusivity ( md ) and fa generated by the software package . 
md values , expressed as a value of adc , and fa values were then calculated as the mean of the values derived from each pixel of the roi examined . 
extremely anisotropic structures are shown with a colour varying from black to deep blue , areas with intermediate anisotropy are shown with a colour varying from orange to purple and isotropic structures are shown in grey scale . 
the structural anatomy of the vertebral body was assessed with the representation of the preferential direction of the fibres on a directionally encoded colour ( dec ) map [ 4 ]  . this information was obtained pixel per pixel on the basis of the vector corresponding to the highest value [ 5 ] , in which red indicates the fibres that run in the left - right direction , green the fibres that run in the anterior - posterior direction , and blue the fibres that run in the superior - inferior direction . 
to this end , an roi was manually traced on the images acquired with a b - value set to 0 along the internal margin of the vertebral body cortex . 
the fibres represented in this way were superimposed on the non - dw echoplanar images ( b = 0 ) and codified by assigning them the colour corresponding to the preferential direction in accordance with the model outlined above . 
i dati sono stati poi rielaborati con software dedicato ( pride v4 , fiber tracking 4.1 , idl , research systems , boulder , co ) allanalisi del dti e al fiber tracking . una singola roi rettangolare stata posizionata sulle immagini acquisite con b factor uguale a 0 in corrispondenza degli stessi somi valutati con imaging spettroscopico ( utilizzando i criteri precedentemente visti per lanalisi delle immagini morfologiche )  . 
tutte le roi sono state poi trasposte automaticamente sullimmagine corrispondente sulle mappe in scala di grigi di diffusivit media ( md ) e di anisotropia frazionaria ( fa ) generate dal software di analisi . 
strutture estremamente anisotropiche appaiono di un colore che varia dal nero al blu ; aree con anisotropia intermedia sono rappresentate con un colore che va dallarancione al viola ; strutture isotropiche sono rappresentate in scala di grigio . 
lanatomia strutturale del corpo vertebrale stata valutata , rappresentando su di una mappa a colori ( directionally - encoded color , dec ) la direzione preferenziale delle fibre [ 4 ]  . questa informazione stata ottenuta pixel per pixel sulla base del vettore corrispondente al valore pi grande [ 5 ] nel quale il colore rosso indica le fibre che decorrono lungo la direzione destra - sinistra , il verde quelle lungo la direzione anteriore - posteriore ed il blu quelle lungo la direzione superiore - inferiore . 
il software di ricostruzione ha poi effettuato automaticamente lestrazione delle fibre concatenando , in ciascun voxel , il vettore principale con quelli dei voxel vicini . tale elaborazione risultata in una progressiva definizione della traiettoria della diffusivit preferenziale che corrisponde verosimilmente alla direzione delle trabecole dellosso spongioso del corpo vertebrale . 
le fibre cos rappresentate sono state sovrapposte alle immagini ecoplanari non pesate in diffusione ( b value = 0 ) e codificate assegnando loro il colore corrispondente alla direzione preferenziale secondo lo schema visto precedentemente . 
il tempo complessivo necessario allelaborazione dei dati del tensore di diffusione , compreso il trasferimento dei dati dalla stazione di acquisizione a quella di elaborazione e lanalisi trattografica , stato in media di circa 20 minuti . 
la valutazione qualitativa degli spettri ha evidenziato una risoluzione spettrale sufficiente a separare la risonanza dellacqua ( 4 , 7 ppm ) da quella dei lipidi ( 1 , 3 ppm )  . 
il picco dellacqua nei soggetti sani risultato significativamente pi elevato di quello dei lipidi , con andamento inverso man mano che let dei pazienti aumentava ed i valori di t - score diminuivano ( inversione del rapporto acqua / lipidi )  . 
la risoluzione spettrale della sequenza ha inoltre permesso di evidenziare un aumento degli acidi grassi saturi ( in particolare il metilene : 1 , 3 ppm ) nettamente superiore rispetto agli acidi grassi insaturi ( protoni oleofinici : 5 , 35 ppm ) [ 7 ] nei pazienti osteoporotici rispetto a quelli sani . 
il valore medio della frazione lipidica ( ff ) misurato nei corpi vertebrali dei volontari sani ottenuto dalle tre misurazioni risultato pari a 34%10 , 6% ( range compreso tra 29%9 , 6% e 56 , 3%11 , 2% ) , con incremento medio annuo di circa il 2% e valori leggermente pi alti nei maschi . 
nel gruppo dei pazienti osteoporotici la ff media calcolata stata 65 , 5%10% ( range compreso tra 55 , 2%9 , 8% e 74 , 5%11 , 2% )  . 
con questa sequenza molto meglio evidente liperintensit della spongiosa ossea di l1 , segno di edema intraspongioso e quindi di frattura recente . spectroscopy we acquired 104 spectra with the single voxel technique , excluding 12 spectra from the study that were not assessable due to motion artefacts and excessive background noise . 
the water peak in healthy subjects was significantly higher than the fat peak , with an inverse progression as patient age increased and t - score decreased ( inversion of the water / fat ratio )  . 
the spectral resolution of the sequence also revealed a notably higher increase in saturated fatty acids ( especially methylene : 1.3 ppm ) than unsaturated fatty acids ( olefinic protons : 5.25 ppm ) [ 7 ] in osteoporotic patients compared with healthy patients . 
spectroscopic analysis of vertebral bodies with a clearly hyperintense signal in the t2 - weighted sequences in osteoporotic patients , however , revealed an apparently retained water / fat ratio . 
in some cases of osteoporotic patients , there was an overlapping of ff values with those of postmenopausal patients with a normal t score . proton - diffusion and tensor - diffusion imaging we positioned 104 rois in as many vertebral bodies and calculated the adc and fa values . 
the images obtained with dti were used to process the colour and vector maps . four uncooperative patients were excluded from the study . nella tabella 1 sono riassunti i valori medi di ff correlati al t - score ed allet dei pazienti sottoposti ad esame spettroscopico . 
in alcuni casi di pazienti osteoporotici si verificata una sovrapposizione dei valori di ff con quelli di pazienti con normale t - score in et postmenopausale . diffusione protonica e tensore di diffusione sono state posizionate 104 rois in altrettanti corpi vertebrali e calcolati i relativi valori di coefficiente di diffusione apparente ( adc ) e di anisotropia frazionata ( fa )  . 
il calcolo della fa in tale gruppo ha infatti mostrato un valore medio di 0 , 29 ( valore tendente allisotropia ) con range tra 0 , 23 e 0 , 36 . 
3 analisi spettroscopica con relativo calcolo della componente lipidica ( 1 , 3 ppm ) e dellacqua in un volontario sano di sesso femminile di 39 anni che mostra normale rapporto acqua / lipidi ( ff 40 , 5% ) e . 
esiste una differenza significativa tra i valore di ff dei soggetti non osteporotici e quello dei soggetti osteoporotici indipendentemente dalla presenza di frattura vertebrale . the remaining data obtained were analysed and compared . in the group of healthy volunteers , the mean adc value obtained from measurements in the three vertebral bodies ( l2 , l3 and l4 ) was 0.480.0510 - 3 mm2 / s ( range between 0.440.0810 - 3 mm2 / s and 0.520.0710 - 3 mm2 / s )  . 
in fact , the colour maps derived from the data revealed a gradation of colours with reference to the entire vertebral body , which is compatible with a structure characterised by intermediate anisot - score - 1 ( p < 0 , 001 )  . 
il calcolo della fa nei soggetti con t - score - 2 , 5 ha mostrato un valore medio di 0 , 5 ( valore tendente allanisotropia ) con range tra 0 , 45 e 0 , 54 , ma il dato importante che tale valore aumentava proporzionalmente alla diminuzione del t - score . 
diffusion - weighted imaging ( dwi ) ( a ) and apparent diffusion coefficient ( adc ) map ( b ) with the regions of interest ( rois ) allowing quantitative analysis of the degree of both mean diffusivity and anisotropy within vertebral bodies of l2 , l3 and l4 . 
immagine pesata in diffusione ( a ) e rispettiva mappa di adc ( b ) con il posizionamento delle roi per lanalisi quantitativa del grado di diffusivit media e di anisotropia allinterno dei somi vertebrali l2 , l3 ed l4 . 
8 confronto tra valori medi di adc in soggetti sani di et giovane ( iii decade , 3040 anni ) e soggetti sani ed osteoporotici in et post - menopausa . 
quantitative histological studies performed on bone biopsies with regard to the changes in bone with age have shown the progressive , gradual and constant increase in the content of fats in bone marrow [ 9 ] , with greater evidence found in osteoporotic subjects [ 10 ]  . 
bone marrow is known to consist primarily of saturated , monounsaturated and polyunsaturated fatty acids [ 11 ] , but it is unknown if ( and how ) that composition varies in osteoporosis . 
a very recent study carried out by yeung et malmente agenti possano causare un evento fratturativo in un corpo vertebrale , n tanto meno il livello specifico dove tale rischio pi alto . 
studi istologici quantitativi eseguiti su biopsie ossee relativi alle modificazioni dellosso legate allet hanno mostrato il progressivo , graduale e costante aumento del contenuto di lipidi nel midollo osseo [ 9 ] , con maggiore evidenza nei soggetti osteoporotici [ 10 ]  . 
noto che il midollo osseo consiste primariamente di acidi grassi saturi , monoinsaturi e polinsaturi [ 11 ] , ma non noto se ( o come ) tale composizione varia nellosteporosi . 
 [ 12 ] con tomografo a risonanza magnetica da 1 , 5 t , in cui sono stati messi a confronto i risultati della spettroscopia effettuata a livello di l3 di una popolazione di donne in post - menopausa osteoporotiche con lo spettro ottenuto da un fantoccio di olio di mais , ha dimostrato che il contenuto di acidi grassi insaturi nel midollo osseo , calcolato come porzione della frazione lipidica totale ( ff ) , presentava una evidente tendenza al decremento quando si passava da soggetti sani a soggetti osteoporotici di pari et e sesso , e che contestualmente esisteva un aumento degli acidi grassi saturi . 
the findings demonstrated that the content of unsaturated fatty acids in bone marrow , calculated as a portion of the total ff , was clearly lower in osteoporotic subjects than in healthy subjects of the same age and gender , whereas the level of saturated fats was higher in the first group . 
the data obtained in our spectroscopic study fully confirm the findings of yeung , and even enable improved separation of the various molecular components of the spectrum and increased accuracy of assessing the individual fat peaks . 
this supports the fact that the techniques that benefit the most from the use of a 3 - t magnetic i dati ottenuti dal nostro studio di spettroscopia confermano pienamente i risultati riportati da yeung , ed anzi consentono di separare meglio le varie componenti molecolari dello spettro e di aumentare laccuratezza nella valutazione dei singoli picchi lipidici . 
questo a riprova del fatto che a risentire maggiormente in maniera positiva dellutilizzo di un campo magnetico a 3t dovrebbe essere proprio limaging spettroscopico ( 1h - mrsi ) , la valutazione della diffusione protonica ( dwi ) ed il calcolo del tensore di diffusione ( dti )  . la relazione esistente tra frazione di lipidi midollari e debolezza ossea pu essere spiegata da diversi fattori . 
 [ 9 ] suggested that with increasing age , the increase in bone marrow fats is even more marked than the reduction in red marrow , probably because the yellow marrow tends not only to replace the loss of bone but also the loss of red marrow . 
in fact , it is thought that the quality of bone marrow plays an important role in vertebral mechanical resistance and that an increase in fats can negatively influence this . 
our data show that postmenopausal patients with a t score - 2.5 reveal a consistent increase in ff when compared with healthy postmenopausal subjects . ff values , however , were not significantly different from those of patients with a normal t score of the same gender and age . 
this may mean that both the spectroscopic analysis and the dwi can identify early changes in the microarchitecture of the cancellous bone of the vertebral body , even when the t score is normal , and therefore before the phenomenon can be detected with dexa . currently available imaging techniques such as dexa assess the final structural result of osteoporosis , but they fail to provide information regarding the physiopathology of the disease . 
our study reveals an adc value in postmenopausal patients with a t score - 2.5 significantly lower ( p < 0.01 ) than the premenopausal group , a finding that is in agreement with the latest studies [ 17 ]  . 
 [ 18 ] were significantly different , but they were not used for comparison because the b value used in that study was below 250 mm2 / s . the lower diffusivity of water in the vertebral bodies of older patients compared with younger patients may indicate changes in the composition of bone marrow correlated with age . 
in particolare , dunnill [ 9 ] ha suggerito che , con laumentare dellet , lincremento dei lipidi midollari ancora pi marcato della riduzione del midollo rosso , presumibilmente perch il midollo giallo va a rimpiazzare tanto il midollo rosso quanto la perdita di osso . una quantit superiore di cellule adipose pertanto necessaria per rimpiazzare la perdita di osso trabecolare e riempire gli spazi prima occupati dal midollo rosso . 
i nostri dati hanno mostrato che pazienti in et postmenopausale con tscore - 2 , 5 presentavano un consistente aumento della frazione lipidica ( ff ) se comparati a soggetti sani di pari sesso in et pre - menopausa . i valori di ff non sono stati invece significativamente diversi da quelli di pazienti con t - score normale , ma di pari sesso ed et . 
tale dato stato confermato anche dal calcolo delladc effettuato negli stessi gruppi di soggetti e potrebbe significare che sia lanalisi spettroscopica che limaging di diffusione possono riflettere cambiamenti precoci nella microarchitettura della spongiosa ossea del corpo vertebrale quando ancora il t - score risulta normale e quindi prima che tale fenomeno sia rilevabile con la dexa . le attuali tecniche di imaging come la dexa valutano il risultato strutturale finale dellosteoporosi ma non danno infatti informazioni circa la fisiopatologia . 
questo studio ha evidenziato , nei soggetti in et post - menopausa con t - score - 2 , 5 , un valore di adc significativamente pi basso ( p < 0 , 01 ) rispetto al gruppo di soggetti di et pre - menopausa , in accordo con i pi recenti studi presenti in letteratura [ 17 ]  . 
 [ 18 ] sono risultati significativamente diversi , ma non sono stati confrontati perch in tale studio sono stati utilizzati valori di b inferiori a 250 mm2 / s . la minore diffusivit dellacqua nei corpi vertebrali dei soggetti pi anziani comparata con quella dei soggetti pi giovani potrebbe essere un indicatore delle alterazioni nella composizione del midollo osseo correlate allet . 
questi risultati sono in accordo con i dati del nostro studio , e suggeriscono che laumento del grasso midollare associato con losteoporosi potrebbe rendere ragione dei valori delladc significativamente pi bassi . 
the increase in fats within the trabeculae of vertebral bodies may reduce extracellular diffusion and lead to a reduction in adc values . with regard to data provided by dti , the analysis of adc and fa proved to be the most reliable . 
we retrospectively evaluated the results of percutaneous stereotactic vab with 11 - gauge needles performed over a period of 34 months on 228 nonpalpable suspicious breast lesions detectable on mammography only [ breast imaging reporting and data system ( bi - rads ) 3 : 25.9% ; bi - rads 4 : 67.1% ; bi - rads 5 : 7% ]  . 
in cases of discordance , repeat biopsy or surgical excision were recommended ; in cases of benign lesions , we urged a follow - up of at least 6 months and for borderline and malignant lesions a surgical excision . 
we obtained a suitable post - vab mammographic or histological evaluation for 78 benign lesions , 17 borderline lesions and 76 malignant lesions , with one ( 1.3% ) false negative ( fn ) case , two ( 11.8% ) underestimations of borderline lesions , 14 ( 18.4% ) underestimations of malignant lesions and no ( 0% ) false positive cases . 
percutaneous histological vab with an 11 - gauge needle proved to be , as reported in previous studies , a reliable method for diagnosing nonpalpable , mammographically detectable only breast lesions , with an underestimation rate lower than core biopsy and a fn rate similar to that of surgical biopsy , without any significant complications . key words vacuum - assisted breast biopsy breast neoplasms mammography riassunto obiettivo . 
sono stati valutati retrospettivamente i risultati delle vab eseguite sotto guida stereotassica , con ago da 11 g , nellarco di 34 mesi in corrispondenza di 228 lesioni mammarie infracliniche sospette , visibili solo mammograficamente ( bi - rads 3 : 25 , 9% ; bi - rads 4 : 67 , 1% ; birads 5 : 7% )  . 
si consigliava , per le discordanze , re - biopsia o biopsia chirurgica , per le lesioni benigne follow - up mammografico di almeno 6 mesi , per le lesioni borderline e le maligne lintervento chirurgico . 
alla vab sono state diagnosticate 123 ( 54% ) lesioni benigne ( con 6 casi di discordanza imaging - istololgia ) , 26 ( 11 , 4% ) lesioni borderline , 79 ( 34 , 6% ) lesioni maligne . 
 disponibile un adeguato riscontro mammografico o istologico successivo alla vab per 78 lesioni benigne , 17 borderline , 76 maligne , con : 1 ( 1 , 3% ) falso negativo , 2 ( 11 , 8% ) sottostime di lesioni borderline , 14 ( 18 , 4% ) sottostime di lesioni maligne , nessun ( 0% ) falso positivo . 
la vab istologica percutanea con ago da 11 g si dimostrata , in accordo con la letteratura , metodica affidabile nella diagnosi delle lesioni mammarie infracliniche visibili solo mammograficamente , con tasso di sottostima inferiore alla core biopsy e percentuale di falsi negativi sovrapponibile alla biopsia chirurgica su repere , in assenza di significative complicanze . parole chiave biopsia mammaria vacuum - assisted neoplasie mammarie mammografia c . 
surgical biopsy is considered the gold standard for this evaluation , but it is expensive , invasive , may cause intense psychological stress for the patient and can be often responsible for deep and superficial scars , possibly impairing later imaging examinations . 
the aim was to overcome the known limits of fine - needle - aspiration biopsy ( fnab ) , such as interobserver variability , the high percentage of inadequate tissue samples , the low reproducibility of results and an inability in malignant lesions to differentiate between in situ and invasive carcinomas [ 1 , 2 ]  . 
percutaneous biopsy has overcome these problems by almost constantly providing with 14gauge needles sufficient material for histological diagnosis , with results totally comparable to those of surgical excision ( sensitivity 85%97% in different reports ) and furnishing , with good accuracy , information about tumour invasiveness [ 36 ]  . 
the first experiences [ 9 , 10 ] with core biopsy used sonographic guidance , but subsequently core biopsy was applied to nonpalpable lesions detectable only by mammography [ 11 ]  . 
the vab device uses vacuum suction to pull breast tissue through the aperture of the needle while a cutter rotates at high speed , thus retrieving core specimens and acquiring multiple tissue samples with a single insertion of the probe . 
the aim of this study was to evaluate our experience with vab , focusing on its accuracy and clinical relevance in patient management decisions . materials and methods between march 2003 and december 2005 , 224 consecutive women with a total of 228 lesions underwent stereotactic vab . 
all patients had previously been studied by mammography with standard mediolateral - oblique ( mlo ) and craniocaudal ( cc ) views , supported by further views ( magnification or particular views on suspicious finding ) when necessary ( 69% of cases )  . 
mammographic findings were the folla diffusione della mammografia quale metodica di screening per il carcinoma della mammella , in grado di ridurre la mortalit per tale patologia , ha comportato un riscontro sempre pi frequente di lesioni di piccole dimensioni che richiedono , per una precisa caratterizzazione , una valutazione anatomopatologica . 
per tale inquadramento la biopsia chirurgica rappresenta sicuramente il gold standard , ma gravata da costi elevati , da una discreta invasivit e , inoltre , comporta uno stress emotivo per la paziente e pu causare frequentemente cicatrici superficiali e profonde che , a volte , compromettono la successiva valutazione strumentale . 
la necessit era quella di superare i limiti della citologia , quali la dipendenza dei risultati dallesperienza specifica degli operatori , lelevata percentuale di prelievi inadeguati , la scarsa riproducibilit e limpossibilit di diagnosi differenziale , nel caso di lesioni maligne , tra forme in situ ed infiltranti [ 1 , 2 ]  . 
il prelievo percutaneo per esame istologico superava queste difficolt , essendo in grado di fornire , nella pressoch totalit dei casi , grazie allimpiego di aghi da 14 gauge , materiale sufficiente per la diagnosi , con risultati paragonabili a quelli della biopsia chirurgica ( sensibilit 85%97% nelle diverse casistiche ) e permettendo di porre , con buona accuratezza , diagnosi di lesione in situ o infiltrante [ 36 ]  . 
sul campione istologico della biopsia percutanea inoltre possibile effettuare le valutazioni immunoistochimiche per definire , in fase preoperatoria , il profilo biologico della neoplasia e , in particolare , lo stato dei recettori ormonali [ 7 , 8 ]  . 
le prime applicazioni di tali prelievi [ 9 , 10 ] riguardarono lesioni visibili allecografia ; successivamente la tecnica venne applicata anche alle lesioni infracliniche visibili solo mammograficamente [ 11 ]  . in questo specifico settore i risultati non furono altrettanto entusiasmanti , tanto che la biopsia chirurgica su repere rimase per lungo tempo la procedura di riferimento [ 12 ]  . per tale motivo , nel 1995 venne proposta una particolare tecnica di prelievo istologico percutaneo , chiamata vacuum - assisted ( vab )  . 
tale modalit prevede linserimento dellago una sola volta e consente di prelevare successivamente numerosi frustoli tissutali , tranciando il tessuto con un mandrino tagliente e rotante e , contemporaneamente , creando una forte aspirazione . 
patients with lesions classed as bi - rads 4 and 5 underwent vab because of diagnostic suspicion , whereas those with bi - rads 3 lesions underwent vab for the following reasons : personal history of previous or synchronous cancer of the same or the contralateral breast ( 29 cases ) , scheduled liver transplantation ( one case ) , family history of breast carcinoma ( 24 cases ) and patient anxiety ( 5 cases )  . prior to biopsy , a coagulation history was obtained , and any coagulation treatment , if possible , was interrupted 48 h before and 24 h after the procedure ; any intolerance to local anaesthetics was excluded . 
we used a digital device ( giotto , ims srl , bologna , italy ) , and mammobed , with a directional vab probe ( mammotome , ethicon endo - surgery , johnson & johnson ) and an 11 - gauge automated needle . 
in cases of microcalcifications , specimen radiographs were obtained to document calcification retrieval . we obtained 12 specimens per lesion in 214 ( 93.8% ) patients and 18 in 11 ( 4.8% ) patients , due to the unsuccessful retrieval of calcifications in the first specimen radiographs . 
in two cases ( 0.9% ) , tissue sampling was interrupted ( nine and eight specimens ) because of abundant bleeding and vasovagal reaction , respectively ; in another case ( 0.4% ) , we only harvested three specimens because of patient discomfort , necessitating discontinuation of the procedure . 
in small lesions completely removed by vab , a nonmagnetic marker clip was deployed at the biopsy site to facilitate preoperative localisation in patients who would require additional surgery . histopathologic results were correlated with mammographic findings by both the radiologist and the pathologist in all cases . 
in cases of discordance , repeat biopsy or surgical excision was ordered ; patients with benign lesions were scheduled for 6 - month follow - up , in agreement with literature , whereas surgical excision was recommended for borderline or malignant lesions [ 1820 ]  . within the study period , 245 consecutive women were referred to us to under stereotactic vab , but only 224 with 228 lesions underwent vab . 
for 15 patients , the diagnostic indication was considered incorrect : in six cases , the diagnostic problem was solved through magnification or parresults materiali e metodi dal marzo 2003 al dicembre 2005 sono state sottoposte a biopsia percutanea vacuum assisted condotta sotto guida stereotassica 224 pazienti , per un totale di 228 lesioni mammarie infracliniche sospette , visibili solo mammograficamente . 
tutte le pazienti avevano eseguito una mammografia nelle due proiezioni cranio - caudale e obliqua e , quando necessario , ulteriori proiezioni e / o ingrandimenti mirati ( 69% dei casi ) sul reperto sospetto . 
la tipologia delle lesioni era cos distribuita : microcalcificazioni 194 ( 85% ) , opacit con microcalcificazioni 20 ( 8 , 8% ) , opacit 12 ( 5 , 3% ) , aree di distorsione architetturale 2 ( 0 , 9% )  . 
il diametro massimo delle lesioni era compreso tra 3 e 60 mm , con un diametro medio di 9 , 7 mm ; 176 ( 77 , 2% ) lesioni erano di dimensioni inferiori o uguali ai 10 mm , 29 ( 12 , 7% ) comprese tra 10 e 20 mm , 23 ( 10 , 1% ) superiori ai 20 mle lesioni di maggiori dimensioni corrispondevano a estesi focolai di microcalcificazioni . le lesioni venivano preliminarmente valutate , relativamente al grado di sospetto , in accordo con la classificazione bi - rads ( breast imaging reporting and data system ) dellamerican college of radiology [ 16 ]  . 
lindicazione al prelievo percutaneo mediante vab era implicita nel gruppo delle lesioni bi - rads 4 ( sospette ) e 5 ( maligne ) , mentre nel gruppo bi - rads 3 era riconducibile a problematiche particolari e , precisamente : in circa met delle pazienti ( 29 casi ) si registrava una anamnesi personale di neoplasia della mammella ( con un tumore sincrono , o precedentemente diagnosticato , nella stessa mammella o in quella controlaterale ) ; nei restanti casi , 1 paziente doveva sottoporsi ad un trapianto di fegato , 24 avevano una storia familiare di tumore della mammella e 5 avevano richiesto espressamente di essere sottoposte a biopsia , piuttosto che effettuare un followup a sei mesi . al momento in cui veniva comunicato lappuntamento per la biopsia a tutte le pazienti veniva fatta una breve anamnesi , tesa innanzitutto a stabilire se esse fossero affette da patologie della coagulazione o se assumessero terapie anticoagulanti e , qualora possibile , queste venivano sospese 48 ore prima e fino a 24 ore dopo la procedura ; venivano raccolte informazioni relativamente ad eventuali intolleranze agli anestetici locali . 
stato utilizzato un mammografo digitale giotto ( ims srl , bologna , italia ) abbinato a un letto mammobed delle stessa ditta , con dispositivo di prelievo vab ( mammotome ethicon endo - surgery , inc . johnson & johnson company )  . 
in tutti i casi sottoposti a biopsia per la presenza di microcalcificazioni , veniva effettuata la radiografia dei frustoli , per verificarne la presenza . il numero di prelievi eseguiti era in genere di 12 ; in particolare , in 214 casi ( 93 , 8% ) sono stati ottenuti 12 frustoli ; in 11 casi ( 4 , 8% ) sono stati ottenuti 18 frustoli in seguito al mancato rilievo di microcalcificazioni visibili radiologicac . 
vab could not be performed in the other six patients because of too superficial lesion location ( four cases ) or insufficient mammary thickness due to small breasts ( two cases )  . 
in six cases [ four ( 3.3% ) with a diagnosis of fat tissue , one ( 0.8% ) with normal breast tissue and one ( 0.8% ) with fcm ] , the histological results were in discordance with radiological findings . thus , two patients had repeat biopsies , which provided a diagnosis of fcm in one case but definitive diagnosis is not available in the second , as that biopsy was performed elsewhere . 
for the patient with a diagnosis of normal glandular tissue , due to the low grade of radiological suspicion ( bi - rads 3 ) , we chose radiological follow - up , at which the lesion remained unchanged . 
in the last case , surgical biopsy was performed because of radiologicalhistomente nei primi prelievi ; in 2 casi ( 0 , 9% ) sono stati ottenuti rispettivamente 9 e 8 frustoli , dal momento che la procedura stata sospesa per linsorgenza di un abbondante sanguinamento e per una reazione vaso - vagale ; in un ultimo caso ( 0 , 4% ) , in cui linterruzione della procedura stata determinata dallinsorgenza di una sintomatologia dolorosa , abbiamo prelevato 3 frustoli . 
nei casi di piccole lesioni , estesamente asportate dalla biopsia , veniva posizionata una clip metallica a - magnetica nella sede del prelievo , per consentire leventuale reperaggio della lesione in caso di successiva necessit di asportazione chirurgica . in tutti i casi stata valutata in riunione congiunta , radiologo - patologo , la congruit tra reperto anatomo - patologico e imaging . 
nei casi discordanti stata consigliata la rebiopsia , oppure la biopsia chirurgica , nelle lesioni benigne veniva consigliata la mammografia di controllo a 6 mesi , come raccomandato dalla letteratura ; lintervento chirurgico stato consigliato in tutte le lesioni maligne e borderline [ 1820 ]  . risultati nellarco di tempo considerato sono pervenute alla nostra osservazione , con indicazione alla biopsia stereotassica , 245 pazienti : 224 / 245 di esse sono state sottoposte a biopsia percutanea vacuum - assisted , per un totale di 228 lesioni . non sono state sottoposte alla procedura 15 pazienti in quanto lindicazione allesame non era corretta . 
in particolare in 6 casi il dubbio diagnostico stato risolto con lesecuzione di radiogrammi mirati e / o altre proiezioni mammografiche ( 3 casi ) , ecografia ( 2 casi ) e risonanza magnetica ( 1 caso ) ; nei restanti 9 casi stato possibile eseguire la c . 
non stato possibile procedere alla biopsia in altre 6 pazienti in quanto la lesione era localizzata vicino alla superficie cutanea ( 4 casi ) o nel contesto di mammelle di piccole dimensioni ( 2 casi )  . 
tutte le biopsie hanno fornito materiale adeguato per la diagnosi ( 100% )  . i risultati anatomopatologici sono stati i seguenti : lesioni benigne 123 ( 54% ) , lesioni borderline 26 ( 11 , 4% ) ; lesioni maligne 79 ( 34 , 6% ) , di cui 57 ( 72% ) carcinomi in situ e 22 ( 28% ) carcinomi infiltranti . 
il risultato istologico era in disaccordo con il quadro radiologico in 6 casi [ 4 ( 3 , 3% ) con diagnosi di tessuto adiposo , 1 caso ( 0 , 8% ) di tessuto ghiandolare normale e 1 caso di mfc ]  . 
nella paziente con diagnosi di tessuto ghiandolare normale , in relazione al basso grado di sospetto radiologico ( bi - rads 3 ) , si optato per un follow - up , che ha confermato la stabilit del quadro . 
in una paziente stata consigliata la biopsia chirurgica per una discrepanza tra quadro radiologico e istologico ; si trattava di un cluster di microcalcificazioni , classificato come bi - rads 4 , risultato alla vab una mfc e , alla successiva chirurgia , una iperplasia papillare epiteliale tipica . altre 2 pazienti con lesioni benigne alla biopsia percutanea sono state sottoposte a biopsia chirurgica per i seguenti motivi : una paziente stata sottoposta a quart per un carcinoma duttale infiltrante con componente in situ nello stesso quadrante e laltra paziente , che presentava una diagnosi di adenoma tubulare , stata sottoposta , per suo espresso desiderio , a escissione chirurgica . 
in 21 casi ( 29% ) disponibile un follow - up di almeno 24 mesi , considerato ottimale per confermare la benignit della lesione . sono disponibili i dati relativi a 78 lesioni benigne , con il riscontro di 1 falso negativo e 77 veri negativi . 
le lesioni borderline ( tabella 2 ) erano 26 ( 11 , 4% ) , cos distribuite : noduli scleroelastotici 8 ( 30 , 8% ) , carcinomi lobulari in situ ( clis ) 7 ( 26 , 9% ) , iperplasie lobulari atipiche ( ila ) 5 ( 19 , 2% ) , lesioni papillari 4 ( 15 , 4% ) , iperplasia duttale atipica ( ida ) 1 ( 3 , 8 % ) ; iperplasia colonnare atipica con ida 1 ( 3 , 8% )  . 
in the central , retroareolar region of the right breast , linear microcalcifications over an area of architectural distortion ( similar to a radial scar ) , with an extension of 25 mm , are shown [ breast imaging reporting and data system ( bi - rads ) 4 ]  . 
nei settori centrali retroareolari della mammella destra si apprezzano minute calcificazioni lineari sottese ad unarea di convergenza architetturale ( tipo radial scar ) , con unestensione complessiva di circa 25 mm ( bi - rads 4 )  . 
biopsia chirurgica , eseguita sei mesi dopo in relazione allincremento delle microcalcificazioni e per discordanza imaging - istologia : diagnosi istologica di cdis . logical discordance ( a cluster of microcalcifications classified as bi - rads 4 proved to be fibrocystic mastopathy at vab and usual epithelial , papillary hyperplasia at subsequent surgical biopsy )  . two more patients with benign lesions underwent surgical excision . 
in one case , at 6 - months follow - up , ultrasonography depicted a new lesion , which was located in the same quadrant as the initial finding but had no relation with it . 
in the literature , this approach is considered mandatory in the case of a percutaneous diagnosis of borderline lesions [ 2026 ]  . fifteen patients underwent surgical excision ( one was treated elsewhere , so data about her final diagnosis were lost ) , whereas 11 refused surgery and preferred to undergo followup . 
in particular , three patients have been followed up for at least 6 months ( 15 , 29 and 30 months , respectively ) , whereas six patients have been followed up only for a short period ( just recently biopsied ) ; data about the remaining two patients are not available . 
of the 14 patients who underwent surgical biopsy , percutaneous diagnosis was confirmed in 12 ( 85.7% ) , whereas two ( 14.3% ) patients were found to have a carcinoma . 
 histological diagnoses of the 79 lesions identified as malignant at vab were ( table 3 ) : 54 ( 68.3% ) dcis , three ( 3.8% ) dcis with microinfiltration , eight ( 10.1% ) invasive ductal carcinoma ( dci ) with dcis , five ( 6.3% ) dci , two ( 2.5% ) lci , one ( 1.3% ) invasive ductal - lobular carcinoma ( dlci ) , one ( 1.3% ) dlci with dcis , two ( 2.5% ) dcis in a papillary lesion , one ( 1.3% ) dci with lcis , one ( 1.3% ) dlci with lcis and one ( 1.3% ) papillary carcinoma in situ . quindici pazienti hanno effettuato la biopsia chirurgica ( una in altra sede senza riscontro istologico ) , 11 pazienti hanno rifiutato lintervento e optato per un follow - up . 
3 pazienti , in particolare , sono in follow - up da pi di 6 mesi ( una da 15 mesi , una da 29 mesi e una da 30 mesi ) mentre in altre 6 non c un sufficiente follow - up ( la biopsia ancora recente ) ; in 2 casi i dati non sono disponibili . 
si pertanto avuta una variazione diagnostica in 2 / 7 casi di clis ( 28 , 6% )  . nei 79 casi diagnosticati come lesioni maligne alla biopsia percutanea ( tabella 3 ) , le diagnosi erano cos distribuite : carcinoma duttale in situ ( cdis ) 54 ( 68 , 3% ) , cdis con microinvasione 3 ( 3 , 8% ) , carcinoma duttale infiltrante ( cdi ) con cdis 8 ( 10 , 1% ) , cdi 5 ( 6 , 3% ) , carcinoma lobulare infiltrante ( cli ) 2 ( 2 , 5% ) , carcinoma duttulo - lobulare infiltrante ( cdli ) 1 ( 1 , 3% ) , cdli con cdis 1 ( 1 , 3% ) , sospetta lesione papillare con carcinoma in situ 2 ( 2 , 5% ) , cdi con clis 1 ( 1 , 3% ) , cdli con clis 1 ( 1 , 3% ) , carcinoma papillare in situ 1 ( 1 , 3% )  . 
in 76 / 79 pazienti stato effettuato lintervento chirurgico ed disponibile la diagnosi definitiva , 3 / 79 sono state operate in altra sede e di esse non abbiamo a disposizione i dati . 
in 5 casi la lesione maligna era cos piccola da non consentire il reperimento allintervento chirurgico : si trattava di 2 casi di lesione papillare con cdis in cui allintervento stata trovata solo la lesione c . 
in tutti questi casi si trattava di lesioni inferiori ai 5 mcomplessivamente , quindi , abbiamo informazioni attendibili sul risultato istologico dellintervento chirurgico in 76 ( 96 , 2% ) lesioni maligne , 14 ( 53 , 8% ) borderline e 5 ( 4% ) benigne , sul risultato della re - biopsia in 1 ( 0 , 8% ) lesione benigna , mentre abbiamo un follow - up di almeno 6 mesi per 3 ( 11 , 5% ) lesioni borderline e 72 ( 58 , 5% ) lesioni benigne . in 45 ( 36 , 6% ) lesioni benigne , 9 ( 34 , 6% ) lesioni borderline e 3 ( 3 , 8% ) lesioni maligne non stato possibile recuperare informazioni sicure : frequentemente , infatti , le pazienti venivano inviate presso il nostro istituto per lesecuzione della biopsia e ritornavano alla sede di provenienza per il follow - up . complessivamente , abbiamo potuto valutare i dati di 78 / 123 lesioni benigne , 17 / 26 lesioni borderline e 76 / 79 lesioni maligne ( per un totale di 171 / 228 lesioni ) con i seguenti risultati : considerando borderline come negativi : 92 veri negativi ( vn ) , 3 falsi negativi ( fn ) , 76 veri positivi ( vp ) , 0 falsi positivi ( fp ) , sensibilit 96 , 2% , specificit 100% , valore predittivo negativo ( vpn ) 96 , 8% e valore predittivo positivo ( vpp ) 100% ; considerando borderline come positivi : 77 vn , 1 fn , 78 vp , 15 fp , sensibilit 98 , 7% , specificit 83 , 7% , vpn 98 , 7% e vpp 83 , 9% . per quanto riguarda lincidenza delle neoplasie maligne rispetto alla diagnosi radiologica espressa con i criteri bifig . 
a small cluster ( 10 mm ) of fine , granular microcalcifications with duct - like distribution are shown in the inferior periareolar region [ breast imaging reporting and data system ( bi - rads ) 4 ]  . 
in sede para - areolare inferiore sinistra riconoscibile un piccolo focolaio di tenui microcalcificazioni granulari con decorso simil - duttale , esteso su unarea di circa 10 mm ( birads 4 )  . 
3 vacuum - assisted biopsy ( vab ) surgical excision concordance . granular and heterogeneous ( with regard to morphology , dimensions and density ) microcalcifications , involving an area of 7 mm , are shown in upper quadrants of the left breast [ breast imaging reporting and data system ( birads ) 4 ]  . 
al passaggio tra i quadranti superiori della mammella sinistra sono riconoscibili alcune microcalcificazioni granulari , polimorfe per morfologia , dimensioni e densit , coinvolgenti unarea di circa 7 mm ( bi - rads 4 )  . 
two clusters of granular microcalcifications with segmental distribution towards the nipple are shown in the external periareolar region of the right breast . the deeper ones are projected on a small , ill - defined density [ breast imaging reporting and data system ( bi - rads ) 5 ]  . 
in sede para - areolare esterna destra si riconoscono due focolai di microcalcificazioni granulari a distribuzione segmentale dirette verso la regione del capezzolo ; in particolare le microcalcificazioni localizzate nei settori pi profondi si proiettano su di una piccola opacit a margini sfumati e mal definiti ( bi - rads 5 )  . 
biopsia chirurgica : diagnosi istologica di cdi con cdis . pathology results on the surgical specimen were available for 76 of 79 patients , whereas three patients underwent surgical intervention elsewhere . 
five very small malignancies were not retrieved in the surgical specimen : in two cases of papillary lesions with dcis , only papillary lesions were identified ; in two cases of dcis , histological evaluation of the surgical specimen revealed fcm and alh in one case and fcm and epitheliosis in the second . 
non ci sono stati casi di episodi infettivi n di ematomi che richiedessero lintervento terapeutico : gli ematomi evidenziati presentavano sempre dimensioni inferiori ai 4 cm ( in due casi il sanguinamento prolungato ha richiesto losservazione in ospedale per qualche ora )  . 
in all these cases , lesions had a diameter < 5 min summary , data about surgical excision were available for 76 ( 96.2% ) malignant lesions , 14 ( 53.8% ) borderline lesions and five ( 4% ) benign lesions ; about repeat biopsy for one ( 0.8% ) benign lesion ; whereas three ( 11.5% ) borderline and 72 ( 58.5% ) benign lesions have been followed up for at least 6 months . 
no cases of relevant scarring was observed on follow - up mammograms . discussion histological percutaneous biopsy for pathologic diagnosis of breast lesions core biopsy represents an effective alternative to surgical biopsy , which is an invasive and expensive method that may cause postsurgical scars , which can impair following diagnostic evaluation and be responsible , even though rarely , for fn results . 
compared with cytology , the complexity and costs of core biopsy are higher , but its inadequate sampling rate and fn rate are significantly lower ( less than 1%2% ) [ 14 , 19 , 23 ]  . 
its sensitivity , with 14 - gauge probes and 17 - mm tissue acquisition aperture , ranges from 85% to 97% , and its specificity is 100% according to different studies [ 27 ]  . 
moreover , its performance is similar to that of surgical biopsy , so that it can be used for decision making in patient management : follow - up for benign lesions , surgery for borderline and malignant lesions , with the possibility in the latter case of shortening the number of surgical steps compared with lesions diagnosed by surgical biopsy [ 20 , 2830 ]  . 
 discussione la biopsia istologica percutanea per la diagnosi anatomopatologica delle lesioni mammarie , detta anche core biopsy , rappresenta una valida alternativa alla biopsia chirurgica , indagine invasiva , costosa , che pu comportare cicatrici post - operatorie in grado di limitare le possibilit diagnostiche e che non scevra da una percentuale , seppur limitata , di falsi negativi . 
la complessit ed i costi della biopsia istologica percutanea sono superiori a quelli della citologia ma , rispetto a questa , la percentuale di inadeguati e falsi negativi nettamente inferiore ( meno dell1%2% ) [ 14 , 19 , 23 ]  . la sensibilit del metodo , utilizzando aghi da 14 g con finestra di prelievo di 17 mm , varia nelle diverse casistiche tra l85% ed il 97% e la specificit del 100% [ 27 ]  . 
i risultati ottenibili con biopsia istologica percutanea , sono del tutto sovrapponibili a quelli della biopsia chirurgica ed essa pu essere pertanto utilizzata per decidere il management della paziente : follow - up nel caso delle lesioni benigne , intervento chirurgico nel caso delle lesioni borderline e delle maligne , con possibilit in questultimo caso di ridurre il numero dei tempi chirurgici rispetto alle lesioni diagnosticate con biopsia chirurgica [ 20 , 2830 ]  . tuttavia , nel caso delle lesioni di piccole dimensioni , in particolare quelle visibili solo mammograficamente , quali focolai di microcalcificazioni , piccole opacit e aree di distorsione parenchimale , e quindi nelle lesioni da biopsiare sotto guida stereotassica , i risultati sono inferiori e la probabilit che la core biopsy consenta di evitare la biopsia chirurgica diagnostica minore [ 31 ]  . 
per cercare di superare tali difficolt e migliorare i risultati , stata introdotta la biopsia percutanea istologica con dispositivi vacuum - assisted che , essendo dotata della possibilit di aspirare , in grado di ridurre la contaminazione ematica della sede di biopsia e , soprattutto , aspirando il tessuto nella finestra di prelievo dellago , consente di ottenere , a parit di calibro , frustoli di maggiore volume ( circa 3 volte ) [ 32 , 33 ]  . 
questo metodo utile , in particolare , nel caso di lesioni di piccole dimensioni , nelle quali lago pu , a volte , non essere posizionato esattamente allinterno della lesione , ma in sua prossimit , per cui risulta particolarmente vantaggioso il meccanismo di aspirazione , che consente di richiamare verso lago , e conseguentemente prelevare , anche il tessuto adiacente . 
questo metodo inoltre efficace in tutti i casi di lesioni borderline e in situ , nei quali lanatomopatologo richiede una elevata quantit di tessuto per porre una diagnosi corretta . laccuratezza diagnostica di tale metodica , riportata dai dati della letteratura , del tutto confrontabile con i dati della biopsia chirurgica su repere , senza peraltro essere gravata da possibili problematiche , quali la dislocazione del repere , che riducono la sensibilit della biopsia chirurgica nelle lesioni infracliniche . 
un significativo miglioramento viene ottenuto anche nelle cosiddette lesioni borderline , anche se in queste ultime persiste , sebbene meno frequentemente , il rischio di sottostima istologica , il che non consente di evitare lintervento chirurgico [ 19 ]  . il sistema vab per il prelievo sotto guida stereotassica pi complesso e costoso di quelli utilizzati per i prelievi core biopsy sotto guida ecografica e richiede , preferibilmente , una unit per biopsia dotata di un tavolo per lesecuzione c . 
 ( % ) tabella 4 frequenza di lesioni maligne per classe breast imaging reporting and data system ( bi - rads ) categoria bi - rads lesioni totali n ( % ) lesioni maligne n ( % ) 59 ( 25.9 ) 153 ( 67.1 ) 16 ( 7 ) 59 ( 25 , 9 ) 153 ( 67 , 1 ) 16 ( 7 , 1 ) 7 ( 11.9 ) 56 ( 36.6 ) 16 ( 100 ) 7 ( 11 , 9 ) 56 ( 36 , 6 ) 16 ( 100 , 0 ) bi - rads 3 bi - rads 4 bi - rads 5 bi - rads 3 bi - rads 4 bi - rads 5 nonetheless , for small lesions and particularly for those detectable at mammography only such as microcalcification clusters , small opacities and areas of parenchymal distortion , which require biopsy under stereotactic guidance the results are poorer and the possibility of avoiding diagnostic surgical biopsy using core biopsy is lower [ 31 ]  . 
these devices , thanks to blood suctioning , can reduce hematic contamination of the sampled area and , most of all , aspirate tissue into the needle acquisition aperture , allow retrieval of larger samples ( about three times as much ) , with the needle calibre being equal [ 32 , 33 ]  . 
this is particularly useful in the case of small lesions for which the needle may be positioned not exactly within the lesion but just close to it : because of the use of vacuum , tissue can be acquired at a distance from the probe , not just within the line of fire . 
this method is also very advantageous in those scenarios , such as borderline and in situ lesions , in which pathologists need a large volume of tissue to make a correct diagnosis . the reported diagnostic accuracy of this technique is very similar to that of surgical biopsy with a localising wire , and vab is free of risks such as wire displacement that reduce the sensitivity of open surgery in nonpalpable breast lesions . a substantial improvement has also been achieved for borderline lesions , even though in these cases histological underestimation cannot be avoided and surgery excision remains mandatory [ 19 ]  . a stereotactically guided vab system is more complex and expensive than sonographically guided core biopsy and should be performed with a prone stereotactic table . 
advantages of the prone table include more working room and decreased likelihood of patient motion and vasovagal reaction ; besides , this design offers the technologist and physician a larger area in which to work and to correctly perform the procedure . 
add - on units attachable to a common mammography unit are very inexpensive but do not isolate the patient , who is more likely to move or feel discomfort as a redella biopsia con paziente prona . 
in tal modo la paziente non vede direttamente la procedura ed raro che si muova o che presenti reazioni vaso - vagali ; il tecnico ed il medico , inoltre , hanno pi spazio per lavorare e quindi effettuare correttamente la procedura . 
le cosidette add - on units , dispositivi applicati ad un comune mammografo , hanno il vantaggio di comportare costi minori ma lo svantaggio di non isolare dalla procedura la paziente cosicch questa , essendo maggiormente coinvolta , pu pi facilmente muoversi o accusare disagio . 
gli aghi utilizzati inizialmente erano da 14 g , successivamente sono stati introdotti quelli da 11 g e 8 g ; attualmente vengono considerati ottimali aghi da 11 g [ 20 , 32 , 34 ]  . la procedura prevede lidentificazione della lesione da sottoporre e biopsia sui tre radiogrammi standard ( craniocaudale , obliquo medio - laterale e medio - laterale , questultimo utile per meglio precisare la posizione della lesione in senso cranio - caudale ) ; successivamente vengono effettuati i radiogrammi di dettaglio sulla mammella compressa , a paziente posizionata sul lettino ; dopo aver identificato le coordinate x e y , vengono eseguite 2 proiezioni inclinate a + 15 e - 15 per consentire il calcolo della profondit ( z )  . 
successivamente , in anestesia locale , si esegue una piccola incisione cutanea con la lama di un bisturi , onde poter entrare nel tessuto mammario con lago , che viene poi indirizzato sul bersaglio identificato . 
in seguito , senza che lago venga pi spostato , si procede al prelievo dei frustoli che , secondo alcuni autori , devono essere in numero superiore o uguale a 20 , mentre , secondo altri , anche in numero di 12 consentono analoghi risultati [ 35 , 36 ]  . 
riteniamo che sia eccessivo ricorrere ad un numero superiore di frustoli , a meno che non sussistano indicazioni particolari , quali la mancata dimostrazione radiografica di microcalcificazioni nei frustoli [ 37 ] ( che ci ha indotto a raggiungere il numero di 18 frustoli in 11 4 , 8% casi ) o la presenza di un focolaio di microcalcificazioni particolarmente esteso . 
needles initially used were 14 gauge , then 11 - gauge and 8 - gauge needles were introduced ; at the moment , 11 - gauge probes seem to be the best choice [ 20 , 32 , 34 ]  . the first step of the procedure is lesion localisation in three standard view mammograms ( craniocaudal , mediolateraloblique and mediolateral , with the latter being useful to localise the lesion in craniocaudal direction )  . 
the highest precision in performing the procedure is needed to avoid sampling errors . after the local anaesthetic has been injected , a small skin incision is made using a bistoury , the probe is inserted , and the needle is then fired at the targeted site . 
according to some authors , at least 20 specimens are needed ; according to others , 12 samples are enough to obtain the same accuracy [ 35 , 36 ]  . 
in fact , in our opinion , a higher number of specimens is necessary in special cases only , for example , when calcifications are not demonstrated on specimen radiographs [ 37 ]  . 
the frequency of malignant lesions according to bi - rads categories was 100% in birads 5 ( 16 / 16 lesions ) , which is in agreement with published data ( 81%97% )  . 
of 153 lesions classified as birads 4 , 56 ( 36.6% ) were malignant , showing a slightly higher rate than published data , which report a proportion of 23%25% [ 28 , 38 , 39 ]  . 
finally , seven ( 11.9% ) of the 59 lesions classified as bi - rads 3 proved to be malignant , higher proportion than previously reported ( less than 2% ) [ 16 , 28 , 40 ]  . 
despite our limited sample size , it can be stated that our data , apparently in disagreement with those reported in the literature , are affected , as previously reported [ 40 , 41 ] , by difficulties in bi - rads category interpretation for microcalcifications , which suffers from subjectivity due to the lack of objective reference parameters . 
this leads to an underestimation of microcalcifications , with an incorrect tendency to classify bi - rads 3 lesions that should be included in the bi - rads 4 category . of the 123 lesion with a vab diagnosis of benignity , 78 had a follow - up of at least 6 months or a repeat biopsy or riale legata alla maggiore probabilit di identificare aree di infiltrazione neoplastica . 
in 2 ( 0 , 9% ) casi il numero contenuto a 89 prelievi stato condizionato da una reazione vaso - vagale e dallinsorgenza di unemorragia abbondante ; in 1 ( 0 , 4% ) caso la procedura stata interrotta dopo 3 prelievi per il sopraggiungere di una intensa sintomatologia dolorosa . 57 / 79 ( 72% ) lesioni maligne identificate alla biopsia percutanea corrispondevano a lesioni non invasive . 
la maggior parte delle lesioni della casistica personale era di piccole dimensioni , in particolare 176 / 228 ( 77 , 2% ) misuravano meno di 10 mm , in 194 / 228 ( 85% ) casi corrispondevano a focolai di microcalcificazioni . 
la percentuale di lesioni maligne per categoria bi - rads risultata del 100% nella categoria bi - rads 5 ( 16 / 16 lesioni maligne ) , risultato che si accorda con i dati della letteratura ( range compreso tra 81% e 97% )  . 
nella categoria bi - rads 4 sono state incluse 56 lesioni maligne su un totale di 153 lesioni , pari al 36 , 6% , con un tasso di malignit leggermente superiore rispetto ai dati della letteratura , che riportano percentuali del 23%25% [ 28 , 38 , 39 ]  . 
sette / 59 lesioni classificate come bi - rads 3 sono risultate maligne , con una percentuale dell11 , 9% , pi elevata rispetto a quella riportata in letteratura ( inferiore al 2% ) [ 16 , 28 , 40 ]  . 
con i limiti dovuti allesiguit del campione valutato , si pu affermare che i nostri dati , apparentemente in lieve disaccordo con quelli della letteratura , risentono , come gi sottolineato da altri autori [ 40 , 41 ] , della difficolt nellinterpretazione delle categorie bi - rads riguardanti le microcalcificazioni , che rimane spesso gravata da soggettivit per lassenza di parametri oggettivi di riferimento . 
si denoterebbe , quindi , un certo atteggiamento di sottostima dei casi che si presentano mammograficamente come microcalcificazioni , ovvero una erronea tendenza ad inquadrare lesioni appartenenti alla categoria bi - rads 4 in quella inferiore . tra le 123 lesioni diagnosticate benigne alla vab , in 78 si potuto avere un follow - up di almeno 6 mesi , o lesito di una re - biopsia , o di una biopsia chirurgica , che hanno consentito di classificare 77 casi come veri negativi e 1 caso falso negativo . 
dopo la diagnosi istologica su vab di tessuto adiposo , in relazione alla discrepanza radiologico - patologica , si ritenuto opportuno eseguire , in accordo con la paziente poco propensa ad essere sottoposta subito alla biopsia chirurgica , uno stretto follow - up , che , a distanza di 6 mesi , ha dimostrato un incremento delle microcalcificazioni , imponendo lesecuzione della biopsia chirurgica , che ha portato alla diagnosi di cdis . 
questo rilievo conferma come sia indispensabile un adeguato follow - up delle lesioni benigne ai fini di migliorare i risultati complessivi della metodica . relativamente alle 26 lesioni borderline , abbiamo informazioni in 14 / 15 casi sottoposti a biopsia chirurgica e in 3 / 11 in follow - up . 
i dati completi a nostra disposizione si riferiscono perci a 17 pazienti , delle quali la diagnosi stata confermata in 15 casi , mentre in 2 ( entrambi clis ) la bioc . 
after histological diagnosis of fatty tissue on vab , because of imaginghistologic discordance , a strict follow - up was advised ( as the patient refused an immediate repeat biopsy )  . 
complete data at our disposal regard 17 patients : in 15 cases , the diagnosis has been confirmed , whereas in two cases ( both lcis ) , excisional biopsy demonstrated dcis , and dcis with a microfocus of lci , respectively . 
considering fn cases of borderline lesions revealed to be underestimations at open surgery an interpretation that is still under discussion and is wekened by the general indication in these cases of performing surgical excision [ 23 ] we had three fn results , with a proportion ( 3.1% ) that is still in agreement with the published data [ 12 , 43 , 44 ]  . 
on the contrary , this underestimation rate is significantly lower than the rate reported for core biopsy , 20%50% [ 48 , 49 ] , and explains why vab is generally considered better for correctly planning the therapy . 
in two cases of papillary lesions with dcis , only papillary lesions were identified ; in two cases of dcis , histological examinations of the surgical specimens revealed fcm and alh in one case and fcm and epitheliosis in the second ; one case of dcis with suspected microinfiltration was not confirmed by surgery . 
the first four lesions were very small less than 5 mm in diameter a characteristic related to the possibility of even complete lesion removal by vab [ 19 ]  . 
in the last case , we can suppose an artefact due to epithelium displacement , which occurs when the needle , fired into the tissue , displaces ductal cells out of the duct away from the target lesion . 
this displacement can deceive the pathologist , who is , however , aware of this phenomenon , which occurs more frequently with core biopsy devices than with vab [ 19 ]  . 
for these reasons , we can consider these cases not to be fp , so we can state that , in our experience , we did not find any fp or overestimations . psia chirurgica ha reso possibile rispettivamente la diagnosi di cdis e di cdis con un microfocolaio di cli . 
2 / 7 clis diagnosticati alla vab sono risultati sottostime rispetto alla diagnosi su pezzo chirurgico , con una percentuale pari all11 , 8% delle lesioni borderline considerate , e al 28 , 6% nellambito del sottogruppo dei clis , riscontro paragonabile ai dati della letteratura [ 42 ]  . 
se si considerano falsi negativi anche le diagnosi di lesioni proliferative rivelatesi sottostime allescissione chirurgica , opinione peraltro discutibile , data la convinzione generalizzata [ 23 ] della necessit di eseguire un intervento chirurgico in questi casi , in totale si sarebbero verificati 3 casi di falsi negativi , con una percentuale ( 3 , 1% ) che rimarrebbe in accordo con i dati della letteratura [ 12 , 43 , 44 ]  . 
tale percentuale di falsi negativi , particolarmente contenuta , sarebbe sostanzialmente confrontabile anche con i falsi negativi della biopsia chirurgica su repere [ 45 ]  . per quanto riguarda le pazienti con diagnosi di malignit posta alla biopsia percutanea , tutte operate , siamo a conoscenza dei dati relativi allintervento in 76 / 79 ( 96 , 2% ) di esse . 
abbiamo riscontrato una concordanza nella diagnosi in 62 / 76 ( 81 , 6% ) pazienti , mentre nelle rimanenti 14 tutti casi di cdis alla vab stata posta diagnosi di forma infiltrante in 8 casi ( 10 , 5% ) e microinfiltrante in 6 ( 7 , 9% )  . questa variazione stata documentata nel 18 , 4% dei casi , dato che non si discosta in modo significativo da quelli della letteratura ( 5%15% ) [ 19 , 43 , 46 , 47 ]  . 
tale risultato differisce invece in maniera significativa dai valori di sottostima riportati per la core biopsy ( 20%50% ) [ 48 , 49 ] e rende ragione del maggior valore nella pianificazione terapeutica generalmente riconosciuto al prelievo vacuum - assisted . 
si trattava di : due lesioni papillari con associato un focolaio di cdis alla biopsia percutanea , nei quali la chirurgia ha riscontrato solo la lesione papillare ; due casi di cdis alla biopsia percutanea con reperto , su pezzo chirurgico , di solo mfc e ila in un caso e mfc ed epiteliosi nellaltro ; un caso di cdis con sospetta microinfiltrazione alla biopsia percutanea , non confermato alla chirurgia . 
in 4 casi si trattava di lesioni molto piccole , inferiori a 5 mm , per le quali riconosciuta la possibilit , con il prelievo vab , di asportare buona parte e talora anche la totalit della lesione [ 19 ] ; in 1 caso ipotizzabile , pi che la completa asportazione della lesione , la presenza di un artefatto da dislocazione , che consiste nel trascinamento delle cellule duttali al di fuori del dotto da parte dellago posizionato nel tessuto mammario . 
in relazione a tali considerazioni , questi casi possono non essere considerati come falsi positivi e ci ci permette di affermare di non aver riscontrato , nella nostra esperienza , casi falsi positivi , n sovrastime . conclusioni complessivamente i dati della casistica personale , seppur ancora non particolarmente numerosa , ci consentono di afc . 
we defined it as the only fn result , as we did not consider as fn the histological underestimations of borderline lesion ( vab diagnosis ) vs . malignant lesion ( surgical biopsy ) , because surgical excision is in any case planned for all of them [ 20 ]  . 
thus , we can state that this method may replace surgical biopsy for diagnosing nonpalpable lesions detectable by mammography only , allowing good patient management , with an overall reduction of costs and time for final surgery and , most probably , a positive effect on the patients outcome . fermare , in accordo con la letteratura , che la biopsia istologica percutanea vacuum - assisted si dimostrata una metodica notevolmente affidabile nella diagnostica delle piccole lesioni visibili solo mammograficamente , con un unico falso negativo e con una percentuale di sottostima in cdis del 10 , 5% nelle forme infiltranti e del 7 , 9% in quelle microinfiltranti , senza alcun caso di falsa positivit . 
tali risultati , abbinati ad una corretta gestione dei casi benigni ( valutazione della concordanza imaging / istologia nel giudicare ladeguatezza del prelievo e follow - up mammografico a 6 mesi ) , ci hanno consentito di recuperare lunico falso negativo senza significativo ritardo diagnostico , non dovendo considerare clinicamente rilevanti le sottostime istologiche di lesioni proliferative riscontrate con vab vs lesione maligna diagnosticata alla chirurgia , in quanto tali lesioni vengono sottoposte a verifica chirurgica [ 20 ]  . 
ridolfi , via varthema 44 , bologna , italy , tel . : + 39 - 051 - 6235444 , fax : + 39 - 051 - 6235444 , e - mail : marcelloridolfi@yahoo.it * il lavoro spetta in parti uguali agli autori received : 21 march 2006 / accepted : 20 august 2006 / published online : 19 march 2007 abstract purpose . 
thirty - eight patients ( 15 men and 23 women ; mean age 55 years ; age range 3579 ) with neck pain were examined and divided into two groups : ( 1 ) patients already identified as rheumatic and referred for further investigation of the atlantoaxial region ; ( 2 ) patients with symptoms confined to the cervical spine , with inconclusive radiographic findings . unenhanced ct of the cervical spine ( tomoscan sr 7000 philips , eindhoven , netherlands ) was performed in all patients . 
ct demonstrated calcific deposits around the dens in 12 patients ( three men and nine women ) , in the transverse and alar ligaments , and in the anterior atlantooccipital membrane . 
crystals located in the transverse ligament of the atlas give rise to the crowned dens syndrome , usually in patients affected by severe degenerative lesions of the atlantoaxial joint and peripheral chondrocalcinosis . 
i soggetti sono stati suddivisi in due gruppi : ( 1 ) pazienti gi diagnosticati come reumatici , di cui lo specialista richiedeva un ulteriore approfondimento diagnostico della zona atlo - epistrofica ; ( 2 ) pazienti con sintomatologia desordio circoscritta al rachide cervicale , di cui la radiologia convenzionale era risultata poco significativa . 
tutti i pazienti sono stati sottoposti a tc volumetrica della colonna cervicale ( tomoscan sr 7000 philips , eindhoven , olanda ) , senza somministrazione per via endovenosa di mezzo di contrasto . 
lesame tc risultato positivo , per depositi calcifici a livello del dente , in 12 pazienti ( 3 maschi e 9 femmine ) , con calcificazioni a livello del legamento trasverso , di quelli alari e della membrana atlo - occipitale anteriore . 
radiography of other joints ( wrist , knee , pubic symphysis ) may help to ascertain whether the disease is due to calcium pyrophosphate dihydrate or hydroxyapatite crystals , and is therefore recommended for routine patient management . magnetic resonance imaging ( mri ) is indicated for the study of neurological complications . key words crowned dens syndrome cppd crystal deposition disease transverse ligament of the atlas computed tomography localizzazione , generalmente asintomatica ; quando i cristalli hanno sede nel legamento trasverso dellatlante , si realizza la sindrome del dente incoronato , abitualmente in pazienti con lesioni degenerative avanzate dellarticolazione atlo - epistrofica e con evidente condrocalcinosi periferica . 
nella sindrome del dente incoronato la tc rappresenta il gold standard diagnostico , potendo identificare la forma e la sede delle calcificazioni e le eventuali erosioni ossee . lesame radiografico di altri distretti articolari ( carpo , ginocchio , sinfisi pubica , spalla ) pu agevolare il riconoscimento eziologico della malattia , se da cppd o da ha , ed pertanto raccomandato nella gestione routinaria del paziente . 
limpiego della rm indicato nello studio della complicanze neurologiche . parole chiave sindrome del dente incoronato malattia da deposito di cristalli di cppd legamento trasverso dellatlante tomografia computerizzata introduction introduzione the crowned dens syndrome ( cds ) is a clinical - radiological entity characterised by calcification of the ligaments surrounding the odontoid process of the axis and by acute attacks of cervicooccipital pain , with fever , rigidity and general signs of inflammation lasting from days to several weeks [ 1 ]  . 
the crystal deposits , in most cases calcium pyrophosphate dihydrate ( cppd ) but also hydroxyapatite ( ha ) , may remain asymptomatic or cause chronic cervical pain and spinal cord compression [ 2 ]  . the classic presenting triad ( headache , fever and morning cervical pain ) was first described by le goff in 1980 [ 3 , 4 ] , who distinguished these acute attacks from those seen in common osteoarthritis and in crystal diseases of the distal cervical vertebrae or thoracic - lumbar spine [ 5 ]  . 
furthermore , atypical cases of cds can simulate both the painful cervicobrachial syndrome ( with shoulder weakness and stiffness ) , as well as occipitotemporal headache ( which mimics atypical rheumatic polymyalgia and / or giant cell arteritis )  . 
according to available data [ 710 ] , computed tomography ( ct ) imaging at the c1c2 level is still the reference standard and is superior to magnetic resonance imaging ( mri ) in identifying these calcifications , especially when they are small [ 11 ]  . the aim of this paper was to illustrate a series of cases of cds seen not only in crystal deposition diseases but also in other rheumatic and nonrheumatic conditions and to provide an assessment of ct imaging patterns and an analysis of the best use of current imaging techniques . 
 la sindrome del dente incoronato ( sdi ) rappresenta unentit clinico - radiologica caratterizzata dallassociazione di calcificazioni dei legamenti attorno al dente dellepistrofeo e da attacchi acuti periodici di cervicalgia occipitale con febbre , rigidit e segni generali di flogosi , di durata molto variabile , da pochi giorni ad alcune settimane [ 1 ]  . colpisce prevalentemente il sesso femminile , con et media al momento della diagnosi tra i 60 ed i 70 anni . 
i depositi di cristalli , nella maggior parte dei casi di pirofosfato di calcio diidrato ( cppd ) , ma anche di idrossiapatite ( ha ) , possono rimanere asintomatici oppure essere responsabili di dolore cronico cervicale e di compressione midollare [ 2 ]  . la tipica descrizione della sindrome , caratterizzata dalla triade cefalea , febbre e cervicalgia mattutina , stata riferita nel 1980 da le goff [ 3 , 4 ] , che distinse questi attacchi acuti da quelli osservati nelle delle malattie da microcristalli a localizzazione vertebrale cervicale distale o dorso - lombare , e da quelli della comune malattia artrosica [ 5 ]  . 
inoltre casi atipici di sdi possono simulare sia la sindrome dolorosa cervico - brachiale ( con debolezza e rigidit della spalla ) che la cefalea occipitale e temporale ( che mima la polimialgia reumatica atipica e / o larterite a cellule giganti )  . 
secondo la letteratura [ 710 ] , lesame tc focalizzato a livello di c1 - c2 rimane il gold standard della diagnostica per immagini ed superiore alla rm nellidentificare queste calcificazioni , soprattutto se minute [ 11 ]  . scopo del presente lavoro stata lillustrazione di alcuni materials and methods between 2001 and 2004 , 38 patients ( 15 men and 23 women ; age range 4572 years ; mean age 55 ) were referred by both general practitioners and specialists ( orthopaedic surgeons , rheumatologists , neurologists , and oncologists ) for investigation of neck pathe patients were divided into two groups : the first ( 16 cases , three men and fifteen women ) consisted of patients with a known clinicalrheumatologic diagnosis [ rheumatoid arthritis ( ra ) , diffuse idiopathic skeletal hyperostosis ( dish ) , etc . ] established on the basis of pain and / or dysfunction at the level of the atlantoaxial joint and alterations demonstrated by conventional radiography , and for whom the specialist had requested further diagnostic investigation the second group ( 22 cases , 12 men and fifteen women ) consisted of patients referred by rheumatologists , general practitioners and other specialists ( orthopaedic surgeon , neurologist , oncologist ) , with initial symptoms confined to the lower cervical spine , often with a history of trauma , and with inconclusive radiographic findings . data collected for each patient included signs and symptoms of the illness , social status and daily working activity , physical examination and laboratory tests , clinical diagnosis and radiographic findings . 
 the disorders affecting the patients ( table 1 ) were distributed as follows : 11 cases of rheumatoid arthritis ( ten women and one man ) , two of cppd crystal deposition disease ( both women ) , one of systemic sclerosis ( a woman ) , one of osteoarthritis ( a man ) , one of seronegative spondyloarthritis ( a man ) , four of neoplasm ( one woman and three men ) with suspected cervical metastases , one ( a man ) of malignant haematological disease ( lymphoma ) , one ( a woman ) of postmenopausal osteoporosis , ten ( five men and five women ) of recent or previous traumatic injury with suspected involvement of the skull base and first cervical vertebrae ( dens fracture , frank atlantoaxial luxation or subluxation ) and six of algo - dysfunctional syndrome of the cervical spine ( three men and three women )  . 
evaluation with ct imaging casi di sindrome del dente incoronato non solamente nellambito delle malattie da deposito di microcristalli , ma anche in altre malattie reumatiche ( i.e. , artrite reumatoide ) e non , la valutazione dei loro aspetti iconografici tc e il giudizio sul miglior impiego delle tecniche attuali di imaging . materiale e metodi nel periodo 20012004 sono stati esaminati 38 pazienti , di cui 15 maschi e 23 femmine , di et compresa fra i 45 ed i 72 anni ( media 55 ) , affetti da cervicalgia , inviati sia dal medico di base che dallo specialista ( ortopedico , reumatologo , neurologo , oncologo ) per gli accertamenti del caso . 
i pazienti sono stati divisi in due gruppi : il primo ( formato da 16 pazienti , di cui 3 maschi e 13 femmine ) , dove la diagnosi clinico - reumatologica era gi stata effettuata ( ar , dish , ecc . ) per la comparsa di sintomatologia algica e / o disfunzionale a livello della cerniera atlo - epistrofica , con alterazioni gi dimostrate in maniera inequivocabile dallesame radiografico convenzionale , e di cui lo specialista richiedeva un ulteriore approfondimento diagnostico a livello della suddetta zona ; il secondo gruppo ( formato da 22 casi , di cui 12 maschi e 10 femmine ) comprendeva pazienti inviati non dal reumatologo , ma dal medico di base e da altri specialisti ( ortopedico , neurologo , oncologo ) , la cui sintomatologia desordio era circoscritta al rachide cervicale , specie in sede prossimale , talvolta su base post - traumatica , e di cui la diagnostica per immagini convenzionale era risultata poco significativa . i dati raccolti per ogni paziente comprendevano tutti i segni ed i sintomi relativi alla malattia denunciata ; lo stato sociale e lattivit lavorativa giornaliera ; gli esami fisico e di laboratorio ; la diagnosi clinica ; i reperti ottenuti con la radiografia convenzionale . 
la visualizzazione delle immagini stata sempre effettuata in modo da avere finestra e livello di finestra sia per i tessuti molli ( i.e. , legamento trasverso ) che per le strutture ossee . 
in particolare , per lo scheletro , lampiezza della finestra stata di 1500 hu e il livello + 300 hu ; per le parti molli rispettivamente 350 hu e + 50 hu . 
non stato somministrato mezzo di contrasto . per quanto riguarda la patologia dei nostri pazienti , la cui distribuzione riportata nella tabella 1 , questa era cos rappresentata : 11 pazienti affetti da artrite reumatoide ( di cui 10 femmine e 1 maschio ) ; 2 casi portatori di malattia da p.n. 
ct demonstrated calcific deposits in the periodontoid structures ( transverse ligament of the atlas , crossed ligament , and alar ligaments ) in 12 patients , three of whom were men and nine who were women ( table 2 )  . 
ct appearance of calcifications was one of thin calcium deposits forming a cppd , entrambi di sesso femminile ; 1 caso di sclerosi sistemica ( femmina ) ; 1 caso di artrosi ( maschio ) ; 1 caso di spondiloartrite sieronegativa ( maschio ) ; 4 pazienti oncologici ( 1 femmina e 3 maschi ) con sospetta localizzazione replicativa cervicale ; 1 caso ( maschio ) affetto da patologia ematologia maligna ( linfoma ) ; 1 caso ( femmina ) con osteoporosi postmenopausale ; 10 pazienti ( 5 maschi e 5 femmine ) affetti da patologia traumatica , recente e pregressa , di cui si sospettava interessamento della base del cranio e delle prime vertebre cervicali ( frattura del dente dellepistrofeo e / o sublussazione e lussazione franca atlo - epistrofica ) e infine 6 pazienti affetti da patologia imprecisata ( 3 maschi e 3 femmine ) algico - disfunzionale cervicale . 
in essi la malattia prevalente era rappresentata dallartrite reumatoide ( ar ) 10 femmine e 1 maschio cui facevano seguito la malattia da cppd ( 2 casi ) , la sclerosi sistemica , lartrosi e la spondiloartrite sieronegativa ( 1 caso , rispettivamente )  . risultati lesame tc della giunzione atlo - epistrofica stato eseguito sulla base della sintomatologia clinica denunciata dal patable 2 patients with crowned dens syndrome ( cds ) and positive computed tomography ( ct ) findings rheumatic diseases no . 
evaluation with ct imaging women 9 rheumatoid arthritis men 3 cppd crystal deposition disease systemic sclerosis rheumatoid arthritis osteoarthritis seronegative spondyloarthritis femmine 9 artrite reumatoide maschi 3 malattia da cppd sclerosi sistemica artrite reumatoide osteoartrosi spondilite sieronegativa transverse ligament ( 4 ) alar ligaments ( 2 ) alar ligaments transverse ligament transverse ligament alar ligaments transverse ligament + atlooccipital anterior membrane legamento trasverso ( 4 ) legamenti alari ( 2 ) legamenti alari legamento trasverso legamento trasverso legamenti alari legamento trasverso + membrana atlo - occipitale anteriore tabella 2 pazienti con sindrome del dente incoronato e tc positiva malattia reumatica casi , n sede delle calcificazioni shell around the dens and located both posteriorly ( on axial images the deposits , they appeared inhomogeneous and probably located on the transverse ligament ) and at the level of the dens apex and base ( on coronal ct reformations due to involvement of the alar and apical ligaments )  . 
 [ 13 , 14 ] identified nonurate crystals in the synovial fluid of patients clinically presenting gout - like attacks ( hence the initial name pseudogout )  . these cppd crystals were characterised by a weak positive birefringence at polarised light microscopy , a finding that distinguished them from the monosodium urate crystals of gout . 
the radiographic features of the disease had , however , been already described by zitnan and sitaj in 1963 , who had called it polyarticular chondrocalcinosis [ 15 ]  . 
bennet , in particular , noted the presence of chalky , rhomboid - shaped crystals [ 16 ] during the autopsy of a patient in ireland with polyarticular chondrocalcinosis . ziente ( principalmente rappresentata da rigidit nucale e cefalea , con o senza incapacit funzionale ) o nellambito del follow - up diagnostico , soprattutto nei casi affetti da cppd dove lesame radiografico tradizionale aveva gi dimostrato la presenza di calcificazioni nelle sedi tipiche della malattia ( i.e. , ginocchio , polso )  . 
lesame tc risultato positivo per depositi calcifici in corrispondenza delle strutture viciniori al dente dellepistrofeo ( legamento trasverso dellatlante , legamento crociato , legamenti alari ) in 12 pazienti , di cui 3 maschi e 9 femmine , la cui distribuzione riportata nella tabella 2 . 
i tre soggetti erano affetti da ar ( anni 69 ) , da osteoartrosi ( anni 70 ) e da spondilite sieronegativa ( anni 48 ) ( fig . 1 ) , con calcificazioni a livello rispettivamente del legamento trasverso , di quelli alari e della membrana atlo - occipitale anteriore . 
liconografia delle calcificazioni era rappresentata da tenui depositi calcifici a guscio , attorno al dente dellepistrofeo , sia in sede posteriore ( nelle immagini tc sul piano assiale , di tipo disomogeneo , verosimilmente a carico del legamento trasverso ) , sia in corrispondenza dellapice e della base del dente stesso ( nelle immagini tc ricostruite sul piano coronale , per interessamento dei legamenti alari e del legamento apicale )  . 
the term chondrocalcinosis is very general , as it suggests apparent radiological and pathological calcification of the cartilage ( which could be due to cppd , ha , tricalcium phosphate or a combination of the three )  . 
although articular and periarticular calcifications can appear in cppd disease , similar calcifications can also be produced by other crystals [ 15 , 19 , 20 ]  . cppd crystal deposition disease is classified into sporadic , hereditary or secondary forms [ 16 ]  . 
the clinical presentation ranges from an incidental radiographic finding to discussione sebbene la malattia da deposito di pirofosfato di calcio diidrato ( cppd ) sia la pi comune artropatia da microcristalli [ 12 ] , tuttavia la scoperta di questi nelle strutture intra - articolari risale allinizio degli anni 60 , quando mccarty insieme ad hollander , kohn e faires [ 13 , 14 ] identific cristalli non uratici nel liquido sinoviale di pazienti che clinicamente presentavano attacchi simil - gottosi ( da ci il termine di pseudogotta dato inizialmente alla malattia )  . questi cristalli di cppd erano caratterizzati da una bassa birifrangenza positiva quando esaminati al microscopio a luce polarizzata , fenomeno che li distingueva da quelli di urato monosodico della gotta . 
the radiological presentation [ 2123 ] is characterised by calcifications in and around the joints and by structural articular changes ( pyrophosphate arthropathy )  . the knee , the wrist , the pubic symphysis and the hip are most commonly affected . 
the spine may be the only site of cppd disease [ 20 , 24 ] and is generally asymptomatic [ 12 ]  . crystals may be identified both in the nucleus pulposus of p.n. 
questultimo , in irlanda , durante lautopsia di un paziente affetto da condrocalcinosi poliarticolare , evidenzi la presenza di cristalli romboidali , di aspetto gessoso [ 16 ]  . i numerosi studi di resnick et al . 
 [ 12 , 17 ] hanno messo ordine nelle svariate nomenclature con cui la malattia era conosciuta , in quanto diversi sinonimi sono stati usati in maniera intercambiabile tra di loro , causando in passato una certa confusione . 
in effetti , il termine condrocalcinosi molto generico , in quanto indica una evidente calcificazione radiologica ed anatomopatologica della cartilagine ( che pu riferirsi alla presenza di cristalli di cppd , di ha , di fosfato tricalcico o alla combinazione dei tre suddetti )  . 
la dizione malattia da deposito di cristalli di cppd ( cppd crystal deposit disease ) si riferisce specificatamente a un disordine caratterizzato dalla esclusiva presenza di cristalli di cppd dentro o intorno alle articolazioni . 
le calcificazioni articolari e periarticolari possono comparire nella malattia di cppd ; tuttavia altri cristalli possono produrre calcificazioni analoghe [ 15 , 19 , 20 ]  . la malattia da cppd si classifica in forma sporadica , ereditaria o secondaria [ 16 ]  . 
infine , i cristalli di cppd possono depositarsi nel legamento trasverso dellatlante e nei legamenti alari , realizzando la c.d. sindrome del dente incoronato [ 1 , 68 ] , la cui definizione , in accordo con diversi autori [ 7 , 8 , 26 ] , dovrebbe comprendere calcificazioni di ogni componente articolare in questa sede ( membrana sinoviale , capsula articolare , legamenti )  . 
inoltre , sullapice del dente sinseriscono tre legamenti : il legamento apicale del dente e i due legamenti alari [ 6 ]  . clinicamente , la sdi dovuta a depositi di ha [ 27 ] una condizione ben definita , ancorch rara , che colpisce donne giovani e di media et , caratterizzata da intensa cervicalgia p.n. 
computed tomography ( ct ) of the atlantoaxial region : images in the axial plane ( a , b ) and reformatted in the coronal ( c , d ) and sagittal planes ( e )  . 
tc atlo - epistrofica : scansioni sul piano assiale ( a , b ) e ricostruzione elettronico sul piano coronale ( c , d ) e sagittale ( e )  . 
in some cases , there may be involvement of the yellow ligaments and posterior longitudinal ligaments , with secondary myelopathy , spinal cord compression and vertebral stenosis [ 25 ]  . 
in particular , it is important to consider the cruciform ligament , which is composed of both part of the transverse ligament of the atlas and its vertical extensions ( superior and inferior longitudinal fibres )  . 
in addition , three ligaments are inserted on the dens apex : the apical ligament and the two alar ligaments [ 6 ]  . clinically , cds due to ha crystal deposits [ 27 ] is a welldefined , though rare , condition that affects young and middle - aged women and is characterised by intense cervical pain [ 28 ] that resolves within days or weeks after treatment with nonsteroid anti - inflammatory drugs ; it does not cause spinal compression [ 4 ]  . 
the clinical picture caused by cppd crystal deposits is more complex , as it may be asymptomatic or associated with a variety of clinical manifestations , some of which are severe [ 29 , 30 ] , such as spinal cord compression [ 31 , 32 ] related in some cases to a slightly calcific mass between the dens and the transverse ligament . 
crystal deposits can be found in older patients ( 5.7% ) with evident peripheral joint chondrocalcinosis [ 11 ] and advanced degenerative lesions of the atlantoaxial joint , and they tend to worsen with age [ 9 ]  . 
 in contrast with previous studies [ 24 , 7 , 12 ] that consider cppd crystal deposition disease as the most frequent form of crowned dens syndrome , only two women in our series [ 28 ] , risolvibile in un tempo variabile da pochi giorni ad alcune settimane con trattamento anti - infiammatorio non steroideo , senza causare compressione bulbare [ 4 ]  . 
il quadro clinico sostenuto , invece , dai cristalli di cppd pi complesso , perch pu essere asintomatico o associarsi a manifestazioni cliniche varie , talora anche gravi [ 29 , 30 ] , quali la compressione midollare [ 31 , 32 ] , determinata da una massa talora finemente calcifica localizzata tra il dente dellepistrofeo e il legamento trasverso . 
i depositi cristallini si osservano in pazienti pi anziani ( 5 , 7% ) , con evidente condrocalcinosi delle articolazioni periferiche [ 11 ] e lesioni degenerative avanzate dellarticolazione atlo - epistrofica e si aggravano con lavanzare dellet [ 9 ]  . 
 nella nostra casistica , in contrasto con la letteratura [ 24 , 7 , 12 ] che indica nella malattia di cppd levenienza pi frequente di sdi , solamente due casi entrambi di sesso femminile presentavano calcificazioni peri - odontoidee . una di queste ( et 69 anni ) denunciava dolore ad entrambe le ginocchia , dove lesame radiografico dimostrava la presenza di calcificazioni moniliformi a carico di entrambi i menischi . 
analoghe calcificazioni erano presenti nella cartilagine triangolare del polso . altre malattie associate alla sdi sono lar , la ra - dish [ 33 ] , le connettiviti sistemiche , le sequele di traumi , sublussazioni e lussazioni franche . 
in particolare , nellar linteressamento dello scheletro assile [ 34 ] risulta significativo nel tratto cervicale ( 60%80% dei casi ) ; esso pu essere asintomatico oppure manifestarsi con dolore , limitazione funzionale e sindromi neurologiche anche gravi [ 20 ]  . 
qualunque sia il distretto interessato , le lesioni anatomo - patologiche sono quelle tipiche della malattia , rappresentate dalla flogosi cronica della membrana sinoviale , con formazione successiva di erosioni ossee ed indebolimento strutturale delle zone dinserzione dei legamenti . 
computed tomography ( ct ) of atlantoaxial region , images in the axial plane ( a , b ) , and reformatted images in the coronal ( c ) and sagittal ( d ) planes . 
in one ( 69 years old ) , who had pain in both knees , radiography demonstrated minute mottled calcifications in the meniscus and in the triangular cartilage of the wrist , typical of cppd crystal deposit disease . the diseases associated with cds are ra , ra - dish [ 33 ] , systemic connectivitis , trauma , frank subluxations and luxations . 
ra in particular involves the axial skeleton [ 34 ] and especially the cervical region ( in 60%80% of cases ) ; this may be asymptomatic , or present with pain , functional impairment and even severe neurological syndromes [ 20 ]  . whatever the area involved , the lesions are pathologically those of ra : chronic inflammation of the synovial membrane , bone erosions and weakening of the ligament insertions . 
laxity of the articular capsule and atlantoaxial joint ligaments causes an abnormal separation ( more than 2.5 mm ) no in sede atlo - epistrofica , con secondarie alterazioni della stabilit e della funzionalit regionale : ostacolata rotazione del capo ed instabilit articolare secondo tre direttrici fondamentali ( anteriore , laterale e verticale )  . 
la lassit delle strutture capsulo - legamentose della giunzione atlo - epistrofica determina lallontanamento anomalo ( > 2 , 5 mm ) tra arco anteriore dellatlante e dente dellepistrofeo , dando luogo alla lussazione atlo - assiale [ 20 ]  . 
nella nostra casistica sono soprattutto i pazienti affetti da ar quelli che hanno denunciato la maggiore incidenza della sdi , con prevalenza del sesso femminile ( 10 femmine e 1 maschio ) , specie in quei casi affetti da malattia reumatica inveterata . lassociazione tra ar e calcificazioni legamentose periodontoidee risulta di non facile interpretazione , dato che non ancora identificato un rapporto di causa ed effetto , tenuto between the anterior arch of the atlas and the odontoid process , resulting in atlantoaxial luxation [ 20 ]  . 
the association between ra and periodontoid calcification is not easy to interpret in that no causal relationship has yet been identified in the light of the natural evolution of ra [ 36 ]  . 
 whereas ct is indicated for the study of cortical bone and periodontoid calcifications , mri with paramagnetic contrast material is the modality of choice for the study of synovial abnormalities , as it is the only technique able to demonstrate the inflamed pannus ( hypervascular , hypovascular and fibrous ) , articular effusion and cord compression [ 37 ]  . the diagnosis of cds is not always straightforward given the broad spectrum of presentations . 
nevertheless , ct can fail to detect cds , especially if it is carried out too late after an acute attack , because the calcifications may have been reabsorbed in the meantime [ 8 ]  . 
the characteristic ct pattern is a narrow and irregular horseshoe calcification surrounding the odontoid process , at times related to osteophytes in the upper margin of the anterior arch of the atlas , as well as calcification of the transverse ligament . 
the main calcification is often surrounded by other smaller calcifications at the apex of the dens [ 10 ]  . differential diagnosis includes calcification of the tendon of the longus colli muscle , where the clinical features of cds are accompanied by pharyngeal pain and dysphagia , incorrectly suggesting meningitis , spondylodiscitis or retropharyngeal abscess . 
other radiographic appearances not to be confused with cds are disc calcifications , calcified adenopathy , sesamoid bones in the transverse ligament , ossification of the common posterior vertebral ligament , and periatlantic calcifications [ 28 , 39 , 40 ]  . 
 [ 28 ] have described 23 cases , five cases and one case of cds , respectively , with clinical presentations varying from febrile nuchal pain ( in acute forms ) to spinal compression ( in chronic forms )  . 
 se la tc indicata per lo studio della corticale ossea e delle calcificazioni periodontoidee , la rm metodica elettiva per lo studio delle lesioni sinoviali , essendo lunica tecnica capace di visualizzare il panno infiammatorio ( ipervascolarizzato , ipovascolarizzato e fibroso ) , il versamento articolare e la compressione midollare , impiegando mezzo di contrasto paramagnetico [ 37 ]  . la diagnosi della sdi non sempre facile , dato lampio spettro di presentazione dellaffezione : infatti , altre manifestazioni cliniche , come la meningite , il dolore cervico - brachiale e lemicrania occipito - temporale , possono aggiungersi al classico episodio acuto febbrile di cervicalgia [ 1 ]  . con la tc la dimostrazione delle minute calcificazioni nellarea del processo odontoideo estremamente facilitato , con sensibilit superiore alla rm [ 38 ]  . 
tuttavia la tc pu fallire nella diagnosi di sdi , specie se questa eseguita tardivamente dopo lattacco acuto , perch nel frattempo le calcificazioni possono riassorbirsi [ 8 ]  . 
laspetto tc caratteristico quello di una sottile ed irregolare calcificazione a ferro di cavallo attorno al processo odontoideo , che in alcuni casi pu essere riferito , oltre che alla calcificazione del legamento trasverso , anche a neoformazioni osteofitosiche a carico del profilo superiore dellarco anteriore dellatlante . 
questa calcificazione principale spesso circondata da altre pi piccole , situate allapice del dente [ 10 ]  . la diagnosi differenziale va posta con le calcificazioni del tendine del muscolo lungo del collo , che oltre al quadro clinico della sdi associa dolore faringeo e disfagia che evocano a torto meningite , spondilodiscite o ascesso retrofaringeo . 
altri aspetti radiografici da non confondere con la sdi sono : le calcificazioni discali , le adenopatie calcifiche , la presenza di un sesamoide nel legamento traverso , lossificazione del legamento vertebrale comune posteriore , le ossificazioni soprannumerarie peri - atlantiche [ 28 , 39 , 40 ]  . 
treves [ 39 ] , constantin [ 7 ] e denes [ 28 ] hanno descritto , rispettivamente , 23 casi , 5 casie 1 caso caratterizzati da un quadro clinico variabile da episodi di nucalgia febbrile nelle forme acute a quadri di compromissione midollare nelle forme croniche . lo studio di treves [ 39 ] ha dimostrato , con lesame tc , la presenza di calcificazioni atlo - odontoidee nel 90% dei casi di sdi : 8 pazienti su 12 di questo gruppo non avevano mai p.n. 
evaluation with ct imaging [ 39 ] demonstrated with ct the presence of atlantoaxial calcifications in 90% of cases : eight of 12 patients had never suffered from neck pa therefore , in the presence of febrile cervical pain , the discovery of periodontoid calcifications suggests cds and excludes meningitis . conclusion in cds , ct is the gold standard imaging modality in that it allows identification of the different radiographic patterns of the disease : simple band of calcification or double band of thin calcifications in the transverse ligament , irregular calcifications crowning the dens apex , and bone erosions of the dens itself . 
however , radiography of other joints ( wrist , knee , pubic symphysis and shoulder ) can help establish whether the disease is due to cppd crystal deposit disease or ha crystals and is therefore recommended for routine patient management . 
although cds is traditionally associated with crystal deposition diseases , it may be accompanied by other diseases affecting the joints , such as ra with involvement of the proximal cervical spine ( as seen in our study ) , ra - dish , and other forms of systemic connectivitis ( systemic sclerosis )  . 
pertanto , in presenza di cervicalgia febbrile , la scoperta di calcificazioni periodontoidee suggestiva di sdi , escludendo quella di meningite . conclusione nella sindrome del dente incoronato la tc rappresenta lesame gold standard , permettendo di identificare i diversi aspetti radiografici : calcificazioni semplici a banda o in doppia filiera sottile in corrispondenza del legamento trasverso ; calcificazioni irregolari a corona sopra e intorno allapice del dente ; lesioni ossee di tipo erosive del dente stesso . 
invece lesame radiografico di altri distretti articolari ( carpo , ginocchio , sinfisi pubica , spalla ) pu agevolare il riconoscimento eziologico della malattia , se da cppd o da ha , ed pertanto raccomandato nella gestione routinaria del paziente . 
la sdi , infatti , tradizionalmente associata alle malattie da microcristalli , ma altre malattie articolari si accompagnano ad essa , in primis lartrite reumatoide con compromissione della colonna cervicale prossimale ( come si evince anche dalla nostra casistica ) , seguita dalla ra - dish e da altre connettiviti sistemiche ( sclerosi sistemica )  . 
one hundred and seven patients with a clinical and laboratory suspicion of acute pulmonary embolism who had already undergone chest radiography were divided into four groups according to the time interval between onset of clinical suspicion and performance of the two diagnostic examinations ( 024 h , 2448 h , 048 h , 27 days )  . 
perfusion lung scintigraphy and multislice ct demonstrated elevated concordance if performed within 7 days of the onset of suspicion of acute pulmonary embolisconcordance was higher if the examinations were completed within 2448 h . 
in suspected acute pulmonary embolism , it is mandatory to reach a correct diagnosis within few hours 48 at the most . key words acute pulmonary embolism perfusion lung scintigraphy spiral computed tomography diagnostics of urgency imagings riassunto obiettivo . 
centosette pazienti con sospetto clinicolaboratoristico di epa , che avevano gi eseguito un rx torace , sono stati divisi in 4 gruppi in base allintervallo di tempo tra il sospetto clinico e lesecuzione di entrambe le indagini ( 024 ore , 2448 ore , 048 ore , 27 giorni )  . 
spp e tcsm sono risultate positive in 29 / 107 ( 27 , 1% ) e negative in 78 / 107 ( 72 , 89% ) : concordanza positiva ( cp ) in 22 casi e concordanza negativa ( cn ) in 71 . 
nel sospetto di epa importante effettuare una rapida e corretta diagnosi in poche ore , 48 al massimo . parole chiave embolia polmonare acuta scintigrafia polmonare perfusiva tc spirale multislice diagnostica per immagini durgenza introduction introduzione acute pulmonary embolism ( ape ) is the third most common acute cardiovascular disease after ischaemic heart disease and stroke [ 1 ]  . 
the yearly incidence of ape in western lembolia polmonare acuta ( epa ) rappresenta la terza pi comune patologia acuta dellapparato cardiovascolare dopo la cardiopatia ischemica e lo stroke [ 1 ]  . 
deep vein thrombosis ( dvt ) is the most common cause of pulmonary embolism ; the other principal primary and secondary risk factors are summarised in table 1 [ 2 ]  . 
in spite of the recent important advances in imaging and laboratory diagnostics , approximately 70% of cases of pulmonary embolism are identified at autopsy [ 3 ]  . in cases with an early diagnosis by multislice spiral computed tomography ( msct ) and perfusion lung scintigraphy ( pls ) , anticoagulation therapy proved to be effective in approximately 75% of patients [ 4 ]  . 
thanks to its ability to perform fast subcentimetre acquisitions with optimisation of vascular enhancement after the injection of contrast material , msct permits visualisation of the entire pulmonary artery tree down to the subsegmental level [ 5 ]  . perfusion lung scintigraphy ( pls ) plays an important role in the diagnosis of ape . 
the aim of our study was to compare and integrate the data provided by pls and by msct in cases of emergency diagnoses of ape in nuclear medicine and radiology departments operating around the clock . materials and methods from may 2002 to june 2004 , we retrospectively reviewed 107 consecutive patients ( 50 women and 57 men ) with ages ranging from 20 to 80 years ( mean age 60 + 18 ) , with a clinical and laboratory suspicion of ape . 
the first - level diagnostic approach included an assessment of predisposing factors , primary disease , symptoms ( dyspnoea , chest pain , cough , haemoptysis , syncope ) and clinical signs ( tachypnoea , tachycardia , signs of deep vein thrombosis , fever , cyanosis )  . 
furthermore , all patients had undergone chest radiography before pls and msct . pls was performed with a gamma starcam 4000 xc / t camera ( ge medical systems , west milwaukee , wi , usa ) after administration of 185 mbq of macroaggregated albumin ( number of particles between 300 , 000 and 50 , 000 and diameter from 120 to 70 m ) with 99 mtc . 
all images were acquired with the planar technique in the anterior , posterior , right and left posterior oblique and right and left anterior oblique projections using the following acquisition parameters : 128128 matrix and 500750 kcounts per projection . 
la trombosi venosa profonda ( tvp ) la pi comune causa di embolia polmonare ed i principali fattori di rischio primari e secondari sono riassunti nella tabella 1 [ 2 ]  . 
nonostante gli importanti e recenti sviluppi della diagnostica strumentale e di laboratorio , circa il 70% degli eventi embolici polmonari sono riconosciuti allesame autoptico [ 3 ]  . nei casi diagnosticati tempestivamente con la tomografia computerizzata spirale multistrato ( tcsm ) e con la scintigrafia polmonare perfusiva ( spp ) , il trattamento anticoagulante si dimostrato efficace in circa il 75% dei pazienti [ 4 ]  . pertanto la tcsm si propone come metodica utile nella valutazione del paziente con sospetta epa . 
infatti , la tcsm per la possibilit di eseguire in tempi rapidi acquisizioni subcentimetriche e di ottimizzare lopacizzazione delle strutture vascolari dopo iniezione di mdc , consente di visualizzare le diramazioni dellalbero arterioso polmonare fino al livello subsegmentario [ 5 ]  . la scintigrafia polmonare perfusiva ( spp ) ha un ruolo importante nella diagnosi di epa . 
questa tecnica non invasiva , a bassa dose di radiazioni , consente una valutazione della perfusione ematica polmonare anche in pazienti critici , non collaboranti e portatori di dispositivi metallici [ 6 ]  . 
scopo del nostro studio stato quello di comparare ed integrare i dati forniti dalla spp e dalla tcsm nella diagnosi in urgenza dellepa in centri di medicina nucleare e radiodiagnostica che svolgono indagini urgenti 24 ore su 24 . materiali e metodi nel periodo compreso tra maggio 2002 e giugno 2004 stata eseguita unanalisi retrospettiva che ha portato a selezionare 107 pazienti consecutivi ( 50 donne e 57 uomini ) di et compresa tra i 20 e gli 80 anni ( et media di 6018 ) , con sospetto clinico - laboratoristico di epa . 
per un inquadramento diagnostico in prima istanza sono stati valutati i fattori predisponenti , la patologia di base , i sintomi ( dispnea , dolore toracico , tosse , emottisi , sincope ) e i segni clinici ( tachipnea , tachicardia , segni di trombosi venosa profonda , febbre , cianosi )  . 
i criteri di inclusione sono stati : lesecuzione sia della spp che della tcsm entro 7 giorni dal sospetto clinico - laboratoristico di epa ; non aver intrapreso alcuna terapia trombolitica . 
inoltre , tutti i pazienti avevano eseguito una rx del torace prima della spp e / o della tcsm . la spp stata effettuata utilizzando una gamma camera starcam 4000 xc / t ( ge medical systems , west milwaukee , wisconsin , usa ) previa somministrazione di 185 mbq di macroaggregati di albumina ( numero di particelle variabile da 300000 a 50000 e diametro compreso tra 120 e 70 micron ) marcati con 99 mtc . 
interpretation criteria for pls were those suggested by the prospective investigative study of acute pulmonary embolism ( pisaped ) study , as reported in table 2 [ 7 ]  . msct was considered positive in the presence of eccentric filling defects or of complete occlusion of the pulmonary artery lumen , whether associated or not to the presence of areas of parenchymal hypoventilation . 
all data provided by pls and msct were independently evaluated by two nuclear physicians and two radiologists and included an assessment of which of the two studies had been ordered and performed first . the patients were grouped based on the time interval between the initial clinical suspicion and performance of the two examinations , namely , 024 h , 2448 h , 0 - 48 hours , and 27 days . 
cohens test was used for analysis of concordance between the results of the two investigations , both on the overall patient population enrolled and for the four subgroups ( 024 h , 2448 h , 048 h , 27 days )  . results pls and msct were positive in 29 / 107 ( 27.1% ) cases and negative in 78 / 107 ( 72.89% ) cases , with a positive concordance ( pc ) in 22 cases and negative concordance ( nc ) in 71 ( table 3 )  . 
in the subgroup of patients who had undergone pls and msct within 24 h of the initial clinical suspicion of ape , pls was positive in 12 / 49 ( 24.48% ) cases and negative in 37 / 49 ( 75.51% ) cases , whereas msct was positive in 17 / 49 ( 34.69% ) cases and negative in 32 / 49 ( 65.30% ) cases , with pc in 12 cases ( fig . 1 ) and nc in 32 cases ( table 4 )  . 
furthermore , 35 patients had undergone pls first , and 14 had undergone msct first . in the subgroup of patients who had undergone pls and msct from 24 to 48 h from the first clinical suspicion of ape , pls was positive in 5 / 20 ( 25% ) cases and negative in 15 / 20 ( 75% ) cases , whereas msct was positive in 3 / 20 ( 15% ) cases and negative in 17 / 20 ( 85% ) cases , with pc in three cases and nc in 15 ( table 5 )  . 
moreover , 13 patients had undergone pls first , and seven had undergone msct first . no state acquisite con tecnica planare in proiezione anteriore , posteriore , obliqua posteriore destra e sinistra , obliqua anteriore destra e sinistra utilizzando i seguenti parametri di acquisizione : matrice 128128 e conteggi per proiezione 500750 kcounts . la tc stata effettuata con apparecchiatura tcsm ( mx 8000 , philips medical system , cleveland , ohio , usa )  . 
i parametri di acquisizione utilizzati sono stati i seguenti : collimazione 2 , 5 mm , pitch 1 , 25 , incremento 1 mm , tempo di rotazione 0 , 5 s , kvp / mas - 120 / 100 . 
lesame stato eseguito con paziente in decubito supino e le scansioni sono state condotte dalle cupole diaframmatiche allo stretto toracico superioil mezzo di contrasto uroangiografico ( ultravist 370 , schering , berlin , germania ) stato iniettato nella vena cubitale attraverso un ago da 16 gauge utilizzando un iniettore automatico ( mk - iv , medrad , pittsburgh , pennsylvania , usa ) con i seguenti parametri : volume 8090 ml , flusso 33 , 5 ml / s . 
il ritardo di inizio delle scansioni stato determinato con lesecuzione di un bolus test , ed risultato variabile tra 9 e 15 s ( fase arteriosa polmonare ) , mentre la fase tardiva stata eseguita dopo 4550 s . 
i criteri dinterpretazione per la spp sono quelli proposti dallo studio prospettico pisa - ped e riportati in tabella 2 [ 7 ]  . la tcsm stata considerata positiva in presenza di difetti di riempimento eccentrici o occludenti lintero lume delle arterie polmonari , associati o meno alla presenza di aree dipoventilazione parenchimale . 
tutti i dati forniti dalla spp e dalla tcsm sono stati valutati indipendentemente da due medici nucleari e da due medici radiologi ed stato anche valutato quale dei due esami era stato richiesto ed eseguito per primo . i pazienti arruolati sono stati raggruppati in base allintervallo di tempo trascorso tra linsorgenza del sospetto clinico e lesecuzione di entrambe le indagini , ovvero 024 ore , 2448 ore , e 27 giorni . 
il test di cohen stato utilizzato per lanalisi della concordanza dei risultati delle due indagini sia per il gruppo di tutti i pazienti arruolati che per i quattro sottogruppi suddivisi in base allintervallo di tempo per lesecuzione delle due indagini 024 ore , 2448 ore , 048 ore , 48 ore7 giorni . risultati la spp e la tcsm sono risultate positive in 29 / 107 ( 27 , 1% ) e negative in 78 / 107 ( 72 , 89% ) , con una concordanza positiva in 22 casi e negativa in 71 ( tabella 3 )  . 
nel sottogruppo dei pazienti che avevano eseguito la spp e la tcsm entro 24 ore dallinsorgenza del sospetto clinico di epa , la spp risultata positiva in 12 / 49 ( 24 , 48% ) e negativa in 37 / 49 ( 75 , 51% ) , mentre la tcsm risultata positiva in 17 / 49 ( 34 , 69% ) e negativa in 32 / 49 ( 65 , 30% ) con g . 
pls ( a ) shows no perfusion in the inferior right lobe , with positive concordance with msct ( b ) , which shows an occlusive thrombus in the right inferior lobe ( white arrow )  . 
la ssp ( a ) mostra assenza di perfusione in corrispondenza del lobo inferiore destro con concordanza positiva con la tcsm ( b ) che mostra la presenza di un trombo occludente nel ramo lobare inferiore destro dellarteria polmonare ( freccia piena )  . 
la tcsm ( b ) dimostra la presenza di un trombo parzialmente occludente ( freccia )  . in the subgroup of patients who had undergone pls and msct within 48 h from the first clinical suspicion of ape , pls was positive in 17 / 69 ( 24.63% ) cases and negative in 52 / 69 ( 75.36% ) cases , while msct was positive in 20 / 69 ( 28.98% ) cases and negative in 49 / 69 ( 71% ) cases , with pc in 15 cases and nc in 47 ( table 6 )  . 
inoltre 35 pazienti avevano effettuato prima la spp e 14 prima la tcsm . nel sottogruppo dei pazienti che avevano eseguito la spp e la tcsm tra 24 e 48 ore dallinsorgenza del sospetto clinico di epa , la spp risultata positiva in 5 / 20 ( 25% ) e negativa in 15 / 20 ( 75% ) , mentre la tcsm risultata positiva in g . 
secondary antithrombin iii deficit protein c deficit factor v leiden protein s deficit plasminogen deficit factor xii deficit hyperhomocysteinaemia anti - cardiolipin antibody congenital dysfibrinogenaemia thrombomodulin tabella 1 fattori di rischio per le tromboembolie venose a . 
concordance between results 3 / 20 ( 15% ) e negativa in 17 / 20 ( 85% ) con una concordanza positiva in 3 casi e negativa in 15 ( tabella 5 )  . 
inoltre 24 pazienti avevano effettuato prima la spp e 14 prima la tcsm . nella tabella 8 riportata lanalisi della concordanza tra la spp e la tcsm nei gruppi di pazienti che hanno effettuato le due indagini entro 24 ore , tra 2448 ore , entro 48 ore , tra 27 giorni ed entro 7 giorni dal sospetto clinico di epa . 
tale concordanza stata maggiore quando le due indagini sono state eseguite entro 24 ore dal sospetto clinico , continua a mantenere valori elevati se le indagini sono eseguite entro 48 ore , mentre si riduce notevolmente se gli esami sono stati eseguiti entro 7 giorni dal sospetto clinico . inoltre fra i 22 pazienti con concordanza positiva tra la spp e la tcsm , 12 hanno eseguito entrambi gli esami entro le 24 ore , 3 entro 48 ore , 7 entro una settimana . 
tra i pazienti con concordanza positiva tra le due indagini nellintera casistica studiata , il 54 , 54% ( 12 / 22 ) apparteneva al sottogruppo studiato entro 24 ore dal sospetto clinico di epa , il 13 , 6% ( 3 / 22 ) al sottogruppo studiato entro 48 ore , il rimanente 31 , 81% ( 7 / 22 ) al sottogruppo studiato entro 7 giorni dal sospetto clinico di epa . 
tra i pazienti con concordanza negativa tra le due indagini nellintera casistica studiata , il 45 , 07% ( 32 / 71 ) apparteneva al sottogruppo studiato entro 24 ore dal sospetto clinico di epa , il 21 , 12% ( 15 / 71 ) al sottogruppo studiato entro 48 ore , il rimanente 33 , 80% ( 24 / 71 ) al sottogruppo studiato entro 7 giorni dal sospetto clinico di epa . in 11 pazienti con spp positiva in fase acuta , questo esame stato ripetuto anche dopo terapia trombolitica prima della dimissione dei pazienti ed ha dimostrato il positivo effetto del trattamento ( miglioramento in 3 , completa normalizzazione della perfusione polmonare in 8 pazienti )  . discussione la diagnosi di embolia polmonare spesso difficile e la mortalit nei casi non trattati , si aggira intorno al 30% , g . 
presence of wedgeshaped areas of hyperperfusion single or multiple wedge - shaped perfusion defects with or without corresponding radiographic parenchymal alterations . absence of wedge - shaped areas of hyperperfusion tabella 2 criteri di interpretazione della spp ( pisa - ped ) diagnosi risultati normale anormale compatibile con epa anormale non compatibile con epa difetti di perfusione non assenza di difetti perfusivi difetti di perfusione cuneiformi singoli o multipli con o senza corrispondenti alterazioni radiografiche parenchimali . 
concordance was higher when the two studies were performed within 24 h of the initial clinical suspicion and remained high when they were performed within 48 h , whereas it decreased markedly if the two studies were performed within 7 days of the initial clinical suspicion . furthermore , among the 22 patients with pc between pls and msct , 12 had undergone both exams within 24 h , three within 48 h , and seven within 1 week . 
among patients with pc between the two investigations , 54.54% ( 12 / 22 ) belonged to the subgroup studied within 24 h of the initial clinical suspicion of ape , 13.6% ( 3 / 22 ) to the subgroup studied within 48 h , and the remaining 31.81% ( 7 / 22 ) to the subgroup studied within 7 days . 
among patients with nc between the two examinations , 45.07% ( 32 / 71 ) belonged to the subgroup studied within 24 h of the initial clinical suspicion of ape , 21.12% ( 15 / 71 ) to the subgroup studied within 48 h , and the remaining 33.80% ( 24 / 71 ) to the subgroup studied within 7 days . mentre si riduce al 2%8% se viene intrapresa una adeguata terapia anticoagulante [ 4 ]  . 
nel 90% dei casi il sospetto di epa motivato dalla presenza di tosse , dispnea , dolore toracico , sincope , tachipnea , cianosi e tachicardia [ 7 , 9 ]  . 
lassenza di questi sintomi ha un valore predittivo negativo del 94% , mentre il valore predittivo positivo rimane basso , pari al 53% , anche considerando lassociazione di pi segni e sintomi riferibili ad epa . 
la radiografia del torace , il dosaggio dei d - dimeri , lemogasanalisi e lecg permettono di orientare la diagnosi e di monitorare le condizioni generali del paziente , ma non consentono una diagnosi definitiva . 
la radiografia del torace solo in rari casi permette di riconoscere lembolia polmonare tuttavia lintegrazione con la spp pu risultare utile per definire la diagnosi di epa [ 11 ]  . la spp permette la visualizzazione diretta della perfusione polmonare attraverso lidentificazione di difetti perfusivi di tipo segmentario e pertanto riveste un ruolo centrale nelliter diagnostico non invasivo di epa . 
la spp un esame semplice , rapido , economico , senza controindicazioni e anche se eseguito con tecnica planare in una sola proiezione permette di riconoscere embolie gravi , per le quali un trattamento terapeutico tempestivo necessario per salvare la vita del paziente . 
la classificazione delle immagini scintigrafiche perfusive suggerita dallo studio pisaped , da noi utilizzata , basata sullidentificazione della presenza e della morfologia di difetti perfusivi , indipendentemente dal loro numero [ 7 ]  . 
dai risultati del suddetto studio appare che la combinazione di una probabilit clinica intermedia o alta con una scintigrafia compatibile con epa ha un elevato valore predittivo positivo ( 98% ) e che una bassa probabilit clinica combinata con un spp anormale , non compatibile con epa , ha un elevato valore predittivo negativo di malattia ( 98% ) [ 7 ]  . nei centri di medicina nucleare , che eseguono indagini 24 ore su 24 in regime durgenza , come il nostro , la spp risultata lesame pi frequentemente richiesto per primo , poich fornisce i dati utili per una gestione terapeutica immediata del paziente . 
nei presidi sanitari in cui la spp non sia rapidamente disponibile la tcsm rappresenta una valida alternativa per documentare le occlusioni totali o parziali delle arterie polmonari [ 1216 ]  . 
tuttavia anche se la tcsm permette di riconoscere embolie pluri - , monoo subsegmentarie , rilevando eventuali riduzioni di densit parenchimale e di vascolarit , non in grado di valutare le modifig . 
of patients who underwent msct first : 30 nudi pazienti che hanno effettuato prima la spp : 77 nudi pazienti che hanno effettuato prima la tcsm : 30 plspls + total plspls + total sppspp + totale sppspp + totale table 4 results for patients undergoing perfusion lung scintigraphy ( pls ) and multislice computed tomography ( msct ) within 024 h tabella 4 risultati della spp e tcsm nel gruppo di pazienti studiati nellintervallo di tempo 024 ore msctmsct + total tcsmtcsm + totale no . 
of patients who underwent msct first : 14 nudi pazienti che hanno effettuato prima la spp : 35 nudi pazienti che hanno effettuato prima la tcsm : 14 in 11 patients with a positive pls in the acute phase , the examination was repeated after thrombolytic therapy and before discharge , and it confirmed the positive effect of treatment ( improvement in three , complete normalisation of lung perfusion in eight )  . discussion the diagnosis of pulmonary embolism is often difficult , and mortality in untreated cases is around 30% , whereas it drops to 2%8% if adequate anticoagulation therapy is initiated [ 4 ]  . 
in 90% of cases , the suspicion of ape is based on the presence of cough , dyspnoea , chest pain , syncope , tachypnoea , cyanosis and tachycardia [ 7 , 9 ]  . 
the absence of these symptoms has a 94% negative predictive value ( npv ) , whereas the positive predictive value ( ppv ) remains low , at 53% , even when the association of several signs and symptoms typical of ape is considered . therefore , other tests need to be used to recognise pulmonary embolism within the first hours after symptom onset . chest radiography , d - dimer , blood gas analysis and electrocardiogram ( ecg ) may suggest a diagnosis and help monitor the patients general condition , although they do not provide a definite diagnosis . 
chest radiography allows recognicazioni funzionali e quindi leffetto emodinamico di emboli o stenosi vascolari che determinano alterazioni della perfusione polmonare [ 17 , 18 ]  . nella nostra esperienza il test di cohen ha documentato una buona concordanza in tutti e 107 i pazienti selezionati . la concordanza risultata maggiore quando lintervallo temporale tra insorgenza del sospetto clinico e lesecuzione delle due indagini era minimo . 
tale non concordanza tra le due indagini spiegabile con la presenza di emboli parzialmente occludenti , che in realt non determinavano alterazioni perfusive significative e quindi di scarso o assente significato funzionale . 
tale non concordanza stata riscontrata nel 3 , 5% ( 2 su 57 ) di pazienti che avevano eseguito prima la spp e poi la tcsm studiati nellintervallo 048 ore e nel 6 , 54% ( 7 su 107 ) di pazienti dellintera casistica studiati nei 7 giorni successivi linsorgenza del sospetto clinico . 
lattivazione dei meccanismi trombolitici con frammentazione dellembolo nelle 48 ore7 giorni dopo linsorgenza del sospetto clinico pu spiegare questa non concordanza . nessun paziente che aveva eseguito entrambe le indagini entro le 24 ore dallinsorgenza del sospetto clinico ha mostrato spp positiva e tcsm negativa . 
of patients who underwent msct first : 7 nudi pazienti che hanno effettuato prima la spp : 13 nudi pazienti che hanno effettuato prima la tcsm : 7 plspls + total plspls + total sppspp + totale sppspp + totale table 6 results for patients undergoing perfusion lung scintigraphy ( pls ) and multislice computed tomography ( msct ) within 048 h tabella 6 risultati della spp e tcsm nel gruppo di pazienti studiati nellintervallo di tempo 048 ore msctmsct + total tcsmtcsm + totale no . 
of patients who underwent msct first : 12 nudi pazienti che hanno effettuato prima la spp : 57 nudi pazienti che hanno effettuato prima la tcsm : 12 tion of pulmonary embolism in sporadic cases only ; however , integration with pls may be useful to confirm the diagnosis of ape [ 11 ]  . pls allows direct visualisation of lung perfusion through the identification of perfusion defects at the segmental level , thus playing a key role in the noninvasive assessment of ape . 
pls is an easy - to - perform , fast , and inexpensive examination that does not present contraindications and , even when performed with the standard planar technique in a single projection , is able to recognise severe embolism necessitating urgent life - saving treatment . 
the classification of scintigraphic perfusion images suggested by the pisa - ped study , which we used , is based on identifying the presence and morphology of perfusion defects , independent of their number [ 7 ]  . 
the results of the above study suggest that the combination of an intermediate to high clinical probability with scintigraphic findings consistent with ape has a high ppv ( 98% ) , and that a low clinical probability combined with abnormal pls findings not consistent with ape has a high npv for this disease ( 98% ) [ 7 ]  . in nuclear medicine centres that perform emergency examinations 24 h / day , as we do , pls was found to be most frequently requested first , as it provides useful information for immediate patient management . 
la tcsm ha il grande pregio di fornire una visione panoramica di tutto il torace e di riconoscere differenti patologie ( atelettasie , focolai broncopneumonici , focolai emorragici ed enfisema )  . 
nei pazienti con spp anormale in cui la tcsm ha mostrato coesistenti patologie cardio - polmonari lintegrazione dei dati pu permettere di attribuire o meno significato embolico alle alterazioni di perfusione riscontrate alla spp [ 19 ]  . in letteratura sono stati suggeriti diversi algoritmi diagnostici sullimpiego delle differenti tecniche di diagnostica per immagini nellepa . 
i criteri di scelta delliter diagnostico devono , tuttavia , tener conto del valore clinico , della reale disponibilit delle diverse indagini , della situazione clinica del paziente ( stabile o instabile ) e della presenza di concomitanti patologie cardio - polmonari . 
this lack of concordance between the two techniques may be explained by the presence of partial occlusions causing no significant changes in perfusion and , subsequently , of little or no functional significance . 
this lack of concordance was identified in 3.5% ( 2 of 57 ) of patients who had undergone pls first and then msct , studied in the 0to 48 - h interval , and in 6.54% ( 7 of 107 ) of patients studied within 7 days of initial clinical suspicion . 
activation of thrombolytic mechanisms with embolus fragmentation during the 27 day period after the initial clinical suspicion may explain this lack of concordance . no patient who underwent both exams within 24 h of the initial clinical suspicion had a positive pls and a negative msct . 
msct has the advantage of providing a panoramic view of the entire chest and visualising different diseases ( atelectasis , bronchopulmonary foci , haemorrhagic foci , and emphysema )  . 
in patients with an abnormal pls , in which msct demonstrated concurrent cardiopulmonary diseases , integration of the data may be necessary to decide whether or not the perfusion alterations seen at pls are ascribable to embolism [ 19 ]  . several diagnostic imaging algorithms have been suggested for the detection of ape . 
other authors suggest the use of msct in cases of pls alterations not typical of pulmonary embolism , advising against its use as a stand - alone technique [ 20 , 21 ]  . however , the criteria for planning the diagnostic workup must take into account the clinical value of techniques , their availability , the patients clinical condition ( stable or unstable ) and the presence of concurrent cardiopulmonary diseases . 
on the other hand , in stable patients with complex radiologic findings , msct should be performed first , because the chances of a nondiagnostic scintigraphy are high in these cases . 
however , msct is preferred for patients with preexisting lung disease or when a differential diagnosis with mediastinal diseases is needed . table 7 results for patients undergoing perfusion lung scintigraphy ( pls ) and multislice computed tomography ( msct ) within 27 days msctmsct + total no . 
of patients with positive exams patients who underwent pls first : 15 patients who underwent msct first : 7 024 h 12 / 49 ( 24.48% ) 2448 h 3 / 20 ( 15.00% ) 27 days 7 / 38 ( 18.42% ) tabella 9 sequenza temporale degli esami spp e tcsm dei 22 pazienti con concordanza positiva raggruppati in base allintervallo di tempo tra insorgenza del sopetto clinico e completamento degli esami di diagnostica per immagini intervallo tra le due indagini numero pz con spp e tcsm positive pz che hanno effettuato prima la spp : 15 pz che hanno effettuato prima la tcsm : 7 024 ore 12 / 49 ( 24 , 48% ) 2448 ore 3 / 20 ( 15 , 00% ) 27 gg 7 / 38 ( 18 , 42% ) conclusions conclusioni in a large group of patients recruited in hospitals with round - the - clock emergency nuclear medicine and radiology services and that follow strict image interpretation criteria , pls and msct proved to have a high concordance when the exams were performed within 7 days of the initial clinical suspicion of ape . 
therefore , a clinical suspicion of ape needs to be confirmed by emergency examinations performed within hours 48 at the most . when both pls and msct are available , pls is the first exam to be ordered for a clinical suspicion of ape . 
although no diagnostic protocol has been universally adopted , pls is the first technique to identify the site and extent of the embolism , thus providing indirect evidence of pulmonary embolismsct is an accurate technique for the diagnosis of ape , and because it can provide information even on other pathological processes , it can confirm or exclude the diagnosis suspected at pls . when both diagnostic techniques are not available , either pls or msct are valuable tools for identifying the presence of severe ape necessitating urgent treatment . in unampia casistica di pazienti arruolati in grandi ospedali con centri di medicina nucleare e radiodiagnostica che effettuano indagini 24 ore su 24 , utilizzando rigorosi criteri di interpretazione delle immagini , la spp e la tcsm hanno dimostrato unelevata concordanza quando eseguite entro 7 giorni dallinsorgenza del sospetto di epa . 
la concordanza pi elevata se le due indagini sono completate entro 2448 ore . pertanto nel sospetto clinico di epa importante accertare la diagnosi con esami durgenza in poche ore , massimo 48 . la spp il primo esame richiesto nel sospetto clinico di epa quando sono disponibili entrambe le tecniche diagnostiche . 
pur non essendo unanimemente accettato un protocollo diagnostico , la spp rappresenta la tecnica di primo approccio per stabilire la sede e lestensione del processo embolico , fornendo levidenza indiretta dellembolia polmonare . 
bartolozzi1 1division of diagnostic and interventional radiology , 2division of pathology , university of pisa , via roma 67 , i - 56100 pisa , italy 3azienda ospedaliera universitaria pisana , pisa , italy correspondence to : c . 
fifty - five patients with mammographic microcalcifications classified as bi - rads categories 3 , 4 or 5 underwent mri and biopsy with stereotactic vacuum - assisted biopsy ( vab )  . 
mri was performed with a 1.5 - tesla ( t ) unit , and t1 coronal three - dimensional ( 3d ) fast low - angle shot sequences were acquired before and after injection of paramagnetic contrast agent ( 0.1 mmol / kg )  . 
lesame rm stato eseguito con una unit da 1 , 5 tesla e sono state acquisite sequenze coronali t1 3d fast lowangle shot sequences prima e dopo liniezione di mezzo di contrasto paramagnetico ( 0 , 1 mmol / kg )  . 
lesame istologico ha rilevato 26 cancri duttali in situ ( cdis ) e cancri duttali microinvasivi ( cd mic ) , 3 iperplasie duttali atipiche ( ida ) e 26 condizioni benigne . 
la sensibilit della mammografia risultata 77% , la specificit stata 59% , il valore predittivo positivo ( vpp ) 61% , il valore predittivo negativo ( vpn ) 74% , laccuratezza diagnostica 67 , 2% . 
la sensibilit globale della rm stata 73% , la specificit 76% , il valore predittivo positivo ( vpp ) 73% , il valore predittivo negativo ( vpn ) 76% , laccuratezza diagnostica 74 , 5% . 
during the last 20 years , the prevalence of dcis has grown from less than 5% before the start of mammographic screening to 15%30% in women regularly checked with mammography [ 6 ]  . 
the 30%50% decrease in mortality is related to early diagnosis and correct management [ 7 ]  . mammography has high sensitivity and low specificity , the positive predictive value ( ppv ) being 15%30% for malignant nonpalpable lesions [ 6 ]  . 
recent studies have shown that breast magnetic resonance imaging ( mri ) with intravenous contrast injection has outstanding sensitivity for the diagnosis of invasive carcinomas ( 88%100% ) and a high negative predictive value ( npv ) [ 6 ]  . 
 considering that dcis is multifocal in more than 50% of cases and bilateral in about 30% of patients [ 1 , 15 ] , and also considering that the possible evolution into an infiltrating form depends on the histological subtype and size and adequacy of resection [ 16 , 17 ] , mri could help in early diagnosis and surgical planning , giving useful information about disease extension [ 14 ]  . 
the aim of our study was to evaluate the role of mri in patients with breast imaging reporting and data systems ( bi - rads ) 35 microcalcifications . la dimostrazione di microcalcificazioni spesso il solo segno del tumore , essendo il primo indizio riscontrato alla mammografia in circa il 70% dei carcinomi duttali in situ ( dcis ) [ 15 ]  . 
durante gli ultimi venti anni , la prevalenza del dcis cresciuta da meno del 5% prima dellinizio dello screening mammografico al 15%30% nella popolazione esaminata regolarmente con la mammografia [ 6 ]  . 
la riduzione della mortalit del 30%50% in relazione con la diagnosi precoce e con il corretto trattamento [ 7 ]  . la mammografia ha un alta sensibilit ed una bassa specificit , infatti il valore predittivo positivo ( vpp ) del 15%30% per le lesioni maligne non palpabili [ 6 ]  . 
recenti studi hanno dimostrato che la risonanza magnetica della mammella ( rm ) con somministrazione di mezzo di contrasto per via endovenosa , ha una notevole sensibilit nella diagnosi del carcinoma invasivo ( 88%100% ) ed un alto valore predittivo negativo ( vpn ) [ 6 ]  . 
invece dimostrata lutilit della rm nella pianificazione chirurgica [ 14 ]  . considerando che il dcis multifocale in pi del 50% dei casi , bilaterale in circa il 30% delle pazienti [ 1 , 15 ] e che la possibile evoluzione in una forma infiltrante dipende dal sottotipo istologico , dalle dimensioni e dalladeguatezza della exeresi chirurgica [ 16 , 17 ] , la rm potrebbe essere di aiuto nella diagnosi precoce e nella pianificazione dellintervento , dando informazioni utili sullestensione della malattia [ 14 ]  . lo scopo del nostro studio quello di valutare il ruolo della rm in pazienti con microcalcificazioni birads 35 . materials and methods we selected 55 patients ( age range 3776 years , mean 5611 years ) with bi - rads 35 microcalcifications on mammography who underwent mri and stereotactic biopsy using vacuum - assisted biopsy ( vab ) between november 2002 and november 2004 . 
mammographic magnification was performed in the view that best visualised the microcalcifications , and the microcalcification extension was evaluated in the standard views . all mammograms were evaluated in a blinded fashion by two radiologists with 15 years experience in breast imaging . materiali e metodi abbiamo selezionato 55 pazienti ( et compresa tra 37 e 76 anni , et media 5611 anni ) con microcalcificazioni birads 35 alla mammografia , che si sono sottoposte ad esame rm e a biopsia sotto guida stereotassica con tecnica di retroaspirazione ( vacuum assisted biopsy : vab ) da novembre 2002 a novembre 2004 . 
i reperti controversi sono stati ulteriormente valutati da entrambi i radiologi per raggiungere un consenso . il nostro gold standard stata la microistologia e listologia per le pazienti sottoposte ad intervento chirurgico . 
lo studio rm stato sempre eseguito prima della microistologia . la rm stata effettuata con un apparecchio da 1 , 5 t ( symphony , siemens ) in tutte le pazienti tranne in 6 in cui stata usata una macchina da 1 , 5 t ( ge , medical system )  . tutte le pazienti sono state studiate in posizione prona utilizzando una bobina dedicata per la mammella . 
il protocollo di studio rm ha incluso un sequenza trasversale t1 di localizzazione , una sequenza sagittale t2 con saturazione del grasso ed una sequenza t1 gradient eco 3d - flash ( te 2 , 5 ms , tr 12 , 7 ms , tempo di acquisizione meno di 2 minuti , fa 30 , spessore di strato 3 mm , interslice gap 0 mm , nex 1 , fov 35 , dimensione della matrice 256160 , dimensione del pixel 1 , 41 , 4 ) , con una serie di 6 acquisizione coronali . 
stato usato il gadoteridolo ( prohance , bracco , milano ) come agente di contrasto paramagnetico con boli di iniezione di 0 , 1 mmol / kg di peso corporeo . 
i processi di rielaborazione delle immagini usate sono stati : sottrazione ; ricostruzioni mip ; ricostruzioni mpr ; curve intensit / tempo nella regione di interesse . sono state identificate secondo lo score di fisher 3 tipi di curve . 
i risultati dello studio rm sono stati classificati secondo lo score di fisher in 5 categorie bi - rads : rm 12 ( fisher score 02 ) : negativo - benigno ; rm 3 ( fisher score 3 ) : probabilmente benigno ; rm 45 ( fisher score 48 ) : probabilmente maligno / maligno . sono state eseguite biopsie sotto guida stereotassica usando il mammografo giotto ims equipaggiato con tavolo prono ed un sistema di aspirazione mammotome ethicon endo - surgery ( amburgo ) con ago di 11 gauge ( g )  . 
il materiale stato inviato allesame microistologico in due differenti contenitori separando i frustoli con le microcalcificazioni da quelli senza microcalcificazioni evidenziate dalla radiografia . lintervento chirurgico stato effettuato in quelle pazienti con diagnosi microistologica di malignit o di lesione altamente sospetta . 
mammografia : le proiezioni cranio - caudale ( cc ) e medio - laterale obliqua ( mlo ) mostrano microcalcificazioni nei quadranti superoed infero - esterni birads 4 e 5 . all cases of microcalcifications were classified according to the method proposed by the american college of radiology [ 18 ] , and those classified as bi - rads 35 were selected . controversial findings were re - evaluated by the two radiologists to reach a consensus . 
mri imaging was performed with 1.5 - tesla ( t ) unit ( symphony , siemens ) in all patients but six , who were examined with a 1.5 - t unit ( ge medical system )  . 
the imaging protocol included a transverse t1 localising sequence , a sagittal fat - saturated t2 sequence and a t1 three - dimensional ( 3d ) fast low - angle shot ( flash ) gradient echo ( te 2.5 ms , tr 12.7 ms , acquisition time less than 2 min , fa 30 , slice thickness 3 mm , interslice gap 0 mm , nex 1 , fov 35 , matrix size 256160 , pixel size 1.41.4 ) , with a series of six coronal acquisitions . 
rm : le immagini mpr sagittali ( a ) ed assiali ( b ) e le mip assiali ( c ) evidenziano multiple aree di captazione contrastografica dendritica e nodulare che interessano lintera mammella sinistra . mmol / kg of body weight . 
postprocessing techniques used were : subtraction maximum intensity projection ( mip ) reconstructions multiplanar reformatting ( mpr ) reconstructions time - intensity curves in the region of interest ( roi )  . three types of curves were identified according to fisher score parameters considering enhancement morphology , we identified the following possibilities : absent enhancement , dendritic enhancement , nodular enhancement and coexistence of dendritic and nodular enhancement . 
results of the mri study were classified into five bi - rads categories according to the fisher score : mri 12 ( fisher score 02 ) negative / benign , mri 3 ( fisher score 3 ) probably benign and mri 45 ( fisher score 48 ) : probably malignant / malignant . biopsy was performed under stereotactic guidance using the giotto ims mammography system equipped with a prone table and a mammotome ethicon endo - surgery ( hamburg ) aspiration device with an 11 - gauge needle . 
considerando la difficolt di una valutazione accurata dellestensione del cdis allanatomia patologica , abbiamo diviso la mammella alla mammografia e alla rm in 5 porzioni : quadrante supero - esterno , quadrante supero - interno , quadrante infero - interno , quadrante infero - esterno , regione retroareolare e abbiamo confrontato tumorale evidenziata lestensione dallimaging con lestensione riscontrata allistologia . risultati la microistologia ha riscontrato 26 lesioni maligne , 29 lesioni benigne incluse 3 iperplasie duttali atipiche ( ida ) ( tabella 1 )  . 
la chirurgia eseguita nelle 29 pazienti ( 17 con carcinoma duttale in situ , cdis , 9 con cancro duttale microinvasivo , cdi mic , e 3 con ida ) , ha confermato in tutti i casi i dati microistologici . 
magnetic resonance imaging ( mri ) : regions of interest in the subtracted images show multiple areas of contrast enhancement with types iii and ii time - intensity curves [ breast imaging reporting and data systems ( bi - rads ) 5 ]  . 
rm : regioni di interesse nelle immagini sottratte post - contrastografiche mostrano multiple aree di captazione contrastografica con curve intensit / tempo di tipo ii e iii ( birads 5 )  . 
stata quindi eseguita una mastectomia sinistra e listologia ha rivelato multipli foci di cdis g2 e g3 . material was sent for microhistological evaluation in two separate containers , one containing the specimens with microcalcifications and the other specimens without microcalcifications . 
in consideration of the difficulties in accurately evaluating dcis extent at pathology , we decided to divide the breast at mammography and mri into five portions : upperouter quadrant , upper - inner quadrant , lower - outer quadrant , lower - inner quadrant and retroareolar region ; we compared si e g3 in 11 casi . 
surgery , performed in 29 patients [ 17 with dcis , nine with ductal microinvasive cancer ( dcmic ) and three with adh ] , confirmed the microhistological data in all cases . 
among the 55 patients studied , mammographic findings were classified as birads 3 : 23 cases , bi - rads 4 : 25 cases andbi - rads 5 : seen cases . 
of the 48 patients with mri contrast enhancement , the time - intensity curve correlated with histology was type i in ten benign lesions and one malignant lesion , type ii in nine benign lesions and nine malignant lesions and type iii in four benign lesions and 15 malignant lesions . 
in the 26 cancers , enhancement morphology logia 17 lesioni benigne e 6 maligne , nelle mammografie birads 4 abbiamo riscontrato 11 lesioni benigne e 14 maligne , nelle mammografie bi - rads 5 abbiamo riscontrato 1 lesione benigna e 6 maligne . 
nelle 48 pazienti con captazione contrastografica alla rm , la curva intensit / tempo correlata allistologia era di tipo i in 10 lesioni benigne e in 1 lesione maligna , di tipo ii in 9 lesioni benigne ed in 9 lesioni maligne e di tipo iii in 4 lesioni benigne e 15 lesioni maligne . nelle 7 pazienti che non presentavano captazione di mezzo di contrasto alla rm , 6 casi risultavano allistologia lesioni benigne e 1 caso cdis ( tabella 4 )  . 
nei 26 cancri la morfologia della captazione contrastografica risultata dendritica in 3 casi , nodulare in 8 casi , sia dendritica che nodulare in 14 casi e completamente assente in un caso ( tabella 5 )  . 
dei 9 casi di cdi mic la maggior parte dei casi avevano una captazione sia dendritica che nodulare ( n = 5 ) ; nei restanti casi la captazione era dendritica ( n = 2 ) e nodulare ( n = 2 )  . per quanto riguarda le forme maligne : nel 3 , 8% dei casi non era presente captazione contrastografica , nel 3 , 8% dei casi le curva intensit / tempo erano di tipo i , nel 34 , 6% le curve intensit / tempo erano di tipo ii e nel 57 , 7% di tipo iii . la sensibilit della mammografia stata del 77% ( 20 / 26 ) , la specificit del 59% ( 17 / 29 ) , il valore predittivo positivo ( vpp ) risultato del 63% ( 20 / 32 ) , il vpn del 74% ( 17 / 23 ) , laccuratezza diagnostica risultata del 67 , 2% ( 37 / 55 )  . 
dei 12 casi di falsi positivi in mammografia con bitable 1 histological results tabella 1 risultati istologici histology dcis / dc mic atypical ductal hyperplasia typical ductal hyperplasia fibroadipose tissue sclerosing adenosis fibroadenoma typical epithelium total istologia cdis / cd mic iperplasia duttale atipica iperplasia duttale tipica tessuto fibroadiposo adenosi sclerosante fibroadenoma epitelio tipico totale dcis , ductal carcinoma in situ ; dcmic , ductal microinvasive carcinoma cdis , carcinoma duttale in situ ; cd mic , carcinoma dentale microinvasivo a . 
as regards the nine dc mic , the majority of cases showed both nodular and dendritic enhancement ( n = 5 ) ; in the remaining cases , enhancement was dendritic ( n = 2 ) and nodular ( n = 2 )  . 
among the five false negative cases of mammographic bi - rads category 3 , mri correctly identified three cancers . of the 12 false positive cases of mammographic bi - rads category 45 , mri correctly identified nine benign lesions . however , the fisher exact test did not show a statistically rads 4 - 5 , la rm ha identificato correttamente 9 lesioni benigne . 
per quanto riguarda lestensione della neoplasia , confrontando i reperti mammografici , rm e listologia abbiamo riscontrato : una concordanza dellestensione neoplastica alla rm e allistologia in 22 / 26 casi ( 84 , 6% ) ; una sovrastima della rm in 3 / 26 casi ( 11 , 5% ) ; in 1 / 26 assenza di captazione contrastografica alla rm per cui non stato possibile valutare lestensione della malattia . abbiamo avuto una sottostima dellestensione neoplastica alla mammografia in 16 / 26 ( 73% ) e una corretta valutazioa . 
with regard to disease extension , comparison of mammographic and mri findings with histology found concordance between mri and histological disease extent in 22 / 26 cases ( 84.6% ) ; overestimation at mri in 3 / 26 cases ( 11.5% ) ; and lack of mri contrast uptake in 1 / 26 cases , preventing evaluation of disease extension . 
nellanalisi dellestensione della neoplasia la rm risultata migliore della mammografia ( test z : p < 0 , 01 )  . in tutti i casi eccetto uno ( multicentrico alla rm e multifocale alla mammografia ) lapproccio chirurgico stato deciso in base allesame rm . 
pathology mammography magnetic resonance imaging tabella 8 confrontro tra estensione neoplastica allimaging e in anatomia patologica mammografia risonanza magnetica sottostima rispetto allanatomia patologica sovrastima rispetto allanatomia patologica valutazione corretta rispetto allanatomia patologica on the basis of the mri findings . 
a mammography : craniocaudal and mediolateral oblique views of the left breast show a cluster of microcalcifications [ breast imaging reporting and data systems ( bi - rads ) 4 ] in the upper outer quadrant . 
b subtracted magnetic resonance imaging ( mri ) : dendritic and nodular irregular enhancement with types i and ii time - intensity curves with low increase of contrast enhancement [ breast imaging reporting and data systems ( bi - rads 4 ) ]  . 
a mammografia : le proiezioni cranio - caudale e medio - laterale obliqua della mammella sinistra mostrano un cluster di microcalcificazioni ( birads 4 ) nel quadrante supero - esterno . 
b immagini rm sottratte : irregolare captazione contrastografica dendritica e nodulare con curve intensit / tempo i e ii con basso incremento della captazione contrastografica ( birads 4 )  . 
a mammography : mediolateral oblique view shows microcalcifications in the retro - areolar region [ breast imaging reportingand data systems ( bi - rads ) 5 ] and other foci ( bi - rads 4 ) in the inner and outer quadrants . 
b magnetic resonance imaging ( mri ) maximum intensity projection ( mip ) : coronal and sagittal views show nodular enhancement in the upper quadrants in the para - areolar region of the right breast , associated with vascular asymmetry ipsilateral to the area of enhancement . 
c subtracted magnetic resonance imaging ( mri ) : nodular contrast enhancement with type iii time - intensity curve [ breast imaging reporting and data systems ( bi - rads ) 5 ] , vacuum - assisted biopsy of retroareolar microcalcifications : g3 dcis . 
a mammografia : la proiezione medio - laterale obliqua mostra microcalcificazioni in regione retroareolare ( birads 5 ) ed altri foci ( birads 4 ) nei quadranti infero - esterni . 
b rm : le immagini mip coronali e sagittali mostrano captazione contrastografica nodulare nei quadranti superiori in regione para - areolare nella mammella destra associata ad unasimmetria vascolare ipsilaterale allarea di captazione contrastografica . 
in one case , surgical treatment was planned on the basis of the mammographic findings rather than considering the mri finding of multifocality , and the patient had a recurrence of disease 1 year later . discussion many studies on dynamic mri [ 6 ] have reported high sensitivity values ( 90%100% ) for the diagnosis of invasive carcinoma , with a specificity of 80% [ 14 , 1923 ]  . 
concerning sensitivity and specificity of mri in the diagnosis of dcis and evaluation of isolated microcalcifications , the published values are ( sensitivity : lower and highly variable 33%100% ) [ 21 , 2426 ]  . 
the relatively low number of dcis cases included in the published studies [ 20 , 21 ] seems to be related to the reluctance of investigators to enrol patients with radiological evidence of microcalcifications . 
 the high variability of mri diagnostic accuracy in evaluating microcalcifications reported in the different studies is related to lesion size [ 6 , 27 , 28 ] , histological variability of tumours [ 20 , 24 ] , tumour angiogenesis [ 24 , 29 , 30 ] , criteria for mri evaluation such as type of enhancement , enhancement pattern , distribution in the breast ( multiple foci ) , margins ( regular , irregular ) [ 21 , 24 , 27 , 30 , 31 ] and use of different pulse sequences and scan planes [ 23 ]  . 
 [ 32 ] , for example , in an analysis of morphological and dynamic features of in situ and microinvasive breast cancer on contrast - enhanced mri , detected the typical enhancement criteria in only 50% of cases , without a significant statistical difference in enhancement pattern among the various histological grades of dcis and between pure and microinvasive dcis . 
in our study , the sensitivity of contrast - enhanced mri , according to the fisher score , was higher ( 77% vs . 50% in viehwegs study ) , with only one false negative mri result corrected by mammography . 
however , the false negative ( n = 7 ) and false positive ( n = 7 ) mris strengthen the concept that mammography is the technique of choice for detecting microcalcifications and that stereotactic biopsy is mandatory for characterising bi - rads 35 microcalcifications . 
information from conventional imaging and in particular mammography is useful to avoid mri false negative results . various studies [ 25 , 32 ] suggest a role for contrast - enhanced mri in the detection of dcis , especially for depicting further tumour foci close to or far from the main lesion that are not visible on mammography due to the absence of microcalcifications or masses or distortions [ 33 , 34 ]  . 
at the same time , it is well known that some areas of dcis can be completely noncalcified and that some sites of dcis can contain calcificadiscussione numerosi studi sulla rm dinamica [ 6 ] hanno riportato elevate valori di sensibilit ( 90% - 100% ) nella diagnosi di carcinoma invasivo , con una specificit dell80% [ 14 , 1923 ]  . riguardo alla sensibilit e specificit dellimaging rm nella diagnosi del carcinoma duttale in situ ( cdis ) e nella valutazione delle microcalcificazioni isolate , i valori pubblicati in letteratura sono pi bassi e variabili ( sensibilit : 33%100% ) [ 21 , 2426 ]  . 
il numero relativamente basso di cdis incluso negli studi pubblicati [ 20 , 21 ] sembra da correlare allavversione ad arruolare allesame rm pazienti con evidenza radiologica di microcalcificazioni . lalta variabilit dellaccuratezza diagnostica nella valutazione delle microcalcificazioni , fino ad ora pubblicata in diversi studi , correlata a : dimensioni della lesione [ 6 , 27 , 28 ] , variabilit istologica dei tumori [ 20 , 24 ] , angiogenesi tumorale [ 24 , 29 , 30 ] , criteri di valutazione della rm come tipo e morfologia della captazione contrastografica , distribuzione nella mammella ( foci multipli ) , margini ( regolari , irregolari ) [ 21 , 24 , 27 , 30 , 31 ] e tecnica di risonanza come differenti sequenze e piani di scansioni [ 23 ]  . 
nel nostro studio la sensibilit riportata per la rm dinamica , in accordo allo score di fischer , risultata pi alta ( 77% rispetto al 50% di viehweg ) con un solo caso di falso negativo corretto dalla mammografia . 
tuttavia i falsi negativi ( n = 7 ) e i falsi positivi ( n = 7 ) rafforzano il concetto che la mammografia la tecnica di scelta per individuare le microcalcificazioni e che la biopsia stereotassica obbligatoria per la caratterizzazione delle microcalcificazioni birads 35 . 
informazioni dallimaging tradizionale ed in particolare dalla mammografia sono utili per evitare i falsi negativi della rm . inoltre vari studi [ 25 , 32 ] suggeriscono un ruolo per la rm con somministrazione di mezzo di contrasto nella diagnosi di cdis specialmente per individuare ulteriori foci neoplastici vicini o lontani dalla lesione principale , che non sono visibili alla mammografia per lassenza di microcalcificazioni , masse o distorsioni [ 33 , 34 ]  . 
questi dati sono particolarmente interessanti se consideriamo levidenza di multifocalit ( 53% ) e multicentricit ( 27% ) osservate in pazienti sottoposte a mastectomia [ 30 , 35 ]  . 
la maggior prevalenza di multicentricit osservata nel cdis che nel cdi e la progressione delle forme in situ non adeguatamente trattate in forme di cancro invasivo richiede unaccurata valutazione dellestensione di malattia specialmente in donne candidate a chirurgia mammaria a . 
the higher prevalence of multicentricity observed in dcis than in dci and the progression of inadequately treated dcis into invasive forms require accurate evaluation of disease extension , especially in cases of candidates to breast - conserving surgery [ 36 , 37 ]  . 
even if the biological and clinical impact of these small foci of dcis is uncertain [ 3840 ] , according to the literature [ 41 ] , the risk of local recurrence after conservative therapy is high in patients with large multifocal tumours and low if the multifocal neoplasm is microscopic . furthermore , it is well known that histological measurement of dcis is difficult due to the difficulty in following a duct on serial sections . 
as regards histological grading , increased vascularisation was associated with more greatly differentiated dcis , which are well detected by contrast - enhanced mri , with a high positive predictive value for g3 and g2 forms . 
 even though our study has a selection bias due to the mammographic detection of microcalcifications , our data suggest that the high ppv of mri in g3 dcis can be useful mainly to depict further dcis foci not associated with mammographic signs . 
these data are in keeping with a recent publication [ 21 ] that emphasised the sensitivity of contrastenhanced mri in the detection of high - grade dcis ( g2 and g3 )  . 
however , recent studies have demonstrated that the same genetic profile is correlated with the same histological grade in both in situ and invasive cancers [ 39 , 43 ]  . 
mri could therefore be useful , especially in identifying the most aggressive forms , thereby helping in surgical planning and once the natural course of the disease and the different biological potential of dcis subtypes are better understood possibly in improving the prognosis , as early detection and correct treatment are the most important prognostic factors in breast cancer . conclusions mri cannot be considered a diagnostic tool for evaluating microcalcifications . 
anche se ad oggi limpatto clinico e biologico di questi piccoli foci di cdis incerto [ 3840 ] , in accordo ai dati di letteratura [ 41 ] il rischio di recidiva locale dopo chirurgia conservativa alto nelle pazienti con grossi tumori multifocali e basso se la neoplasia multifocale microscopica . inoltre ben noto che il cdis difficile da misurare istologicamente per la difficolt a seguire un dotto interessato in sezioni seriali . 
per quanto riguarda il grading istologico nella nostra esperienza abbiamo osservato una vascolarizzazione aumentata associata a forme di cdis pi differenziate che sono ben individuate con la rm dinamica , con elevato valore predittivo positivo per le forme g2 e g3 . anche se il nostro studio ha un bias nei criteri di inclusione rappresentato dallindividuazione mammografica delle microcalcificazioni , i nostri dati suggeriscono che lelevato valore predittivo positivo della rm nei casi di cdis g3 pu essere utile soprattutto ad individuare i foci ulteriori di cancro in situ non associati a segni mammografici . 
questi dati sono allineati con una recente pubblicazione [ 21 ] che enfatizza la sensibilit della rm dinamica nella diagnosi delle forme di cancro in situ di alto grado ( g2 e g3 )  . 
cos la rm potrebbe essere utile nell identificare specialmente le forme pi aggressive di cdis aiutando nella pianificazione dellintervento chirurgico e , una volta che siano chiariti il corso naturale della malattia e che i differenti potenziali biologici dei sottotipi di cdis , probabilmente migliorare la prognosi . infatti la diagnosi precoce del cancro mammario ed il corretto trattamento sono i fattori prognostici pi importanti . conclusioni la rm non pu essere considerata lo strumento diagnostico per valutare le microcalcificazioni . 
la malformazione vascolare polmonare stata chiusa in 3 minuti e la saturazione percutanea di ossigeno passata dal 73% al 93% . la fistola da emodialisi stata chiusa con 1 dispositivo in 4 minuti . 
lavp un efficace sistema per la chiusura di grossi vasi periferici e di malformazioni vascolari , a costi contenuti , che consente unembolizzazione sicura e a basso rischio di complicanze , con risparmio in termini di tempo e di dose erogata . key words amplatzer vascular plug transcatheter embolisation vascular disease parole chiave amplatzer vascular plug embolizzazione transcatetere patologia vascolare introduction introduzione percutaneous embolisation has become a valid option and often the first - line treatment for acute bleeding , temporary or permanent devascularisation of benign or malignant hypervascular tumours [ uterine fibroids , hepatocellular carcinoma ( hcc ) ] , the closure of congenital or acquired arteriovenous lembolizzazione percutanea divenuta ormai una valida alternativa e spesso la metodica di prima istanza nel trattamento di sanguinamenti acuti , ma anche nella devascolarizzazione temporanea o permanente di tumori ipervascolarizzati benigni o maligni ( fibromi uterini , hcc ) , nella chiusura c . 
several embolisation devices are available , each with its own characteristic features : a fibrin sponge is used for temporary ( about 48 h ) embolisation , polyvinyl alcohol ( pva ) microspheres are commonly used for permanent embolisation , whereas detachable balloons , glue , metal coils and plugs are used for definitive embolisation . this paper describes our experience with a new system for definitive embolisation , the amplatzer vascular plug ( avp ) , a versatile device that was successfully used in the closure of arteries ( internal iliac and subclavian ) , a pulmonary arteriovenous malformation , a haemodialysis fistula , and a gastric varix in a subject with portal hypertension . materials and methods the avp ( aga medical corporation , golden valley , mn , usa ) is a new device approved by the u.s. 
food and drug administration for peripheral embolisation of arteries and veins and that uses the same technology as other amplatzer devices used for occluding interatrial and interventricular defects and patent foramen ovale . 
the system is preloaded inside a 100 - cm - long guiding catheter : 5 fr for plugs with a diameter of 48 mm , 6 fr for plugs with a diameter of 1012 mm and 8 fr for plugs with a diameter of 1416 mthe system ranges in size from 4 mm di malformazioni vascolari arterovenose congenite o acquisite e nella chiusura di varici . 
esistono in commercio numerosi dispositivi embolizzanti ciascuno con caratteristiche preponderanti rispetto agli altri : per lembolizzazione temporanea si utilizza la spugna di fibrina ( 48 h circa ) ; per quella permanente sono comunemente impiegate le microsfere in alcol polivinilico ( pva ) ; per lembolizzazione definitiva infine ci si avvale dei palloni staccabili , della colla , delle spirali metalliche e dei plug . gli autori descrivono la loro esperienza nellutilizzo di un nuovo sistema per lembolizzazione definitiva , lamplatzer vascular plug ( avp ) , un dispositivo dallutilizzo versatile , specie nei vasi di grosso diametro , che stato utilizzato con successo nella chiusura di arterie ( iliache interne e succlavie ) , di una malformazione arterovenosa polmonare , di una fistola da emodialisi e di una varice gastrica in soggetto con ipertensione portale . materiali e metodi lavp ( aga medical corporation , golden valley , mn , usa ) un nuovo dispositivo approvato dalla food and drug administration per lembolizzazione periferica di vasi arteriosi e venosi che utilizza la stessa tecnologia di altri device amplatzer utilizzati per occludere difetti interatriali , interventricolari e forami ovali . 
il sistema caricato allinterno di un catetere portante ( 100 cm di lunghezza ) da 5 fr per plug da 4 a 8 mm di diametro , da 6 fr per plug da 10 a 12 mm di diametro e da 8 fr per plug da 14 a 16 mm di diametro . 
il sistema disponibile in misure che vanno da 4 mm di diametro fino a 16 mm con un incremento di 2 muna volta raggiunta la sede in cui si vuole rilasciare il dispositivo basta ritirare il catetere in modo da far uscire il plug e girare in senso antiorario la guida metallica per liberare il device . 
in accordo con la casa produttrice si raccomanda di scegliere un dispositivo con un oversize almeno del 20% rispetto al diametro del vaso da trattare per evitare una possibile migrazione distale . 
le peculiarit del sistema sono la sua disponibilit in unampia gamma di misure , anche molto grandi , la possibilit di riposizionamento prima del rilascio definitivo , il minor rischio di migrazione rispetto alle spirali e un breve tempo per occludere definitivamente il vaso . presso il nostro centro sono state eseguite 11 occlusioni vascolari con lutilizzo del nuovo dispositivo avp : 5 arterie iliache interne nella prevenzione dellendoleak di tipo ii dopo posizionamento di endoprotesi aortoiliaca ; 3 arterie succlavie di sinistra per il trattamento di endoleak di ii tipo successivo al posizionamento di endoprotesi dellaorta toracica con copertura dellarteria succlavia sinistra ( ass ) ; 1 fistola arterovenosa polmonare ; 1 fistola da emodialisi e 1 grossa varice in un paziente con emorragia da varice gastrica portatore di tips . 
positive features include the availability of a wide range of sizes , even very large ; the possibility of repositioning the device before its definitive release ; lower risk of migration compared with coils ; and short occlusion times . 
 our centre performed 11 vascular occlusions using the new avp : five internal iliac arteries to prevent type ii endoleaks after aortoiliac stent - graft placement , three left subclavian arteries to treat type ii endoleaks after thoracic aorta stent - graft placement with coverage of the left subclavian artery ( lsa ) , one pulmonary arteriovenous malformation , one haemodialysis fistula , and one large gastric varix due to haemorrhage in a patient with transjugular intrahepatic portosystemic shunt ( tips )  . 
the patients were studied with a multidetector computed tomography ( mdct ) scanner ( somatom sensation 6 , siemens , germany ) , mdct workstation ( leonardo , siemens , germany ) , angiographic equipment ( axiom fa , siemens , germany ) and ultrasound ( us ) ( technos , esaote , italy )  . 
chest mdct done to assess the pulmonary arteries showed a large solitary arteriovenous fistula with two afferent arteries arising from two branches of the right lower lobar pulmonary artery and drainage into the inferior pulmonary vein of the right lower lobe . 
la mdct del torace effettuata per la valutazione delle arterie polmonari ha dimostrato una grossa e solitaria fistola arterovenosa polmonare con due arterie afferenti , provenienti da due rami dellarteria polmonare lobare inferiore di destra , e drenaggio nella vena polmonare inferiore del lobo inferiore del polmone destro . 
langiografia selettiva dellarteria polmonare destra , eseguita attraverso la vena femorale comune di destra , ha confermato la diagnosi posta con la mdct dimostrando un diametro da 10 mm e 4 mm delle due arterie afferenti . 
la chiusura del vaso di maggiori dimensioni stata eseguita utilizzando la tecnica standard gi descritta , con un avp da 12 mm ( oversize del 20% rispetto al vaso nativo ) , mentre la seconda arteria afferente , di minori dimensioni ( 4 mm di diametro ) , stata cateterizzata mediante la tecnica buddy wire : tale sistema consiste nellutilizzo di due guide allinterno dello stesso catetere , per garantire maggior portanza , facilitando il posizionamento del device in vasi a decorso pi complesso . 
 stata utilizzata una guida coronarica da 0 , 014 ( guidant spartacore middle weight ) come buddy wire che stata posizionata oltre il segmento scelto per il rilascio del dispositivo , dando stabilit al catetere , prima del passaggio del device . 
2a multidetector computed tomography ( mdct ) angiography of the abdominal aorta and iliac arteries : anterior volume - rendered ( vr ) image shows an aneurysm of the right common iliac artery ( arrowhead )  . 
c angiography 8 min after release of the avp shows the outline of the device ( arrows ) and complete absence of flow within the right internal iliac artery from the systemic blood flow . 
2a angio - mdct dellaorta addominale e delle arterie iliache : ricostruzione vrt ( volume rendering technique ) che dimostra la presenza un aneurisma dellarteria iliaca comune di destra ( testa di freccia )  . 
c controllo angiografico a 8 minuti dal rilascio dellamplatzer vascular plug , dimostra la sagoma del device rilasciato ( frecce ) e la completa assenza di flusso nellarteria iliaca interna destra dal circolo sistemico arterioso . 
3a angiography of the thoracic aorta after stent - grafting in a patient with type b dissection of the thoracic aorta demonstrates the presence of a type i + type ii endoleak ( arrowheads ) from the left subclavian artery . 
b follow - up multidetector computed tomography ( mdct ) angiography at 1 month ; sagittal maximum intensity projections ( mip ) image confirmed the type i + type ii endoleak ( arrowhead ) from the left subclavian artery and the presence of partial thrombosis of the false lumen ( * )  . 
c similar projection 5 min after release of the amplatzer vascular plug ( avp ) shows the outline of the device ( arrows ) , with the exclusion of the origin of the left subclavian artery , the patency of the left vertebral and internal mammary artery and the absence of endoleaks . 
3a angiografia dellaorta toracica dopo il posizionamento di endoprotesi toracica in un paziente con dissecazione dellaorta toracica di tipo b che dimostra un endoleak di tipo misto ( tipo i + ii ) ( teste di freccia ) dallarteria succlavia sinistra . 
b controllo angio - mdct a un mese , ricostruzione sagittale mip ( maximum intensity projections ) , che conferma la presenza di un endoleak di tipo misto ( tipo i + ii ) ( testa di freccia ) dallarteria succlavia sinistra e la presenza di trombosi parziale del falso lume ( * )  . 
c sucessivo controllo a 5 minuti dal rilascio dellamplatzer vascular plug che mette in evidenza la sagoma del device rilasciato ( frecce ) con la completa chiusura dellorigine dellarteria succlavia sinistra , la perviet dellarteria vertebrale e mammaria interna e lassenza dellendoleak . 
4a angiography shows a persistent passage of contrast material across the previously ligated haemodialysis arteriovenous anastomosis and two large aneurysms ( arrowheads ) that end in a cul - de - sac at the level of the basilic vesome collateral veins , with reverse flow , can be seen to originate from the efferent vein and course towards the hand ( arrows )  . 
b angiography performed 2 min after amplatzer vascular plug ( avp ) deployment shows a considerable reduction in the passage of contrast ( arrow ) through the device ( arrowhead ) into the basilic venote the good patency of the artery below . 
4a langiografia mette in evidenza la persistenza del passaggio di mdc attraverso lanastomosi arterovenosa da emodialisi precedentemente legata chirurgicamente e i due grossi aneurismi ( testa di frecce ) che terminano a fondo cieco a livello della vena basilica efferente : si notano inoltre alcune vene collaterali che si dipartono dalla vena efferente e si dirigono , a flusso invertito , verso la mano ( frecce )  . 
b il controllo angiografico eseguito dopo 2 minuti dallapertura del plug dimostra una marcata riduzione del passaggio di mdc ( freccia ) attraverso il dispositivo ( testa di freccia ) nella vena basilica efferente . 
c il controllo dopo altri 3 minuti evidenzia la totale chiusura della fistola , lassenza delle vene collaterali e la perviet dellasse arterioso a valle . 10 mm and 4 mm of the two afferent arteries . 
closure of the larger vessel was achieved by applying the standard technique , with a 12 - mm avp ( 20% larger than the native vessel ) , whereas the smaller afferent artery ( 4 mm ) was catheterised using the buddy wire technique , which consists of using two guidewires within the same catheter , to ensure better support and facilitate deployment of the device in more tortuous vessels . 
dopo aspirazione del trombo portale , effettuata mediante catetere tipo portante da 8 fr ( jr 4.0 , medtronic , mn , usa ) , stata eseguita una seconda angiografia che ha dimostrato la parziale riduzione del trombo e la persistenza di flusso nella varice : si quindi optato per la sua embolizzazione definitiva . 
5a portography shows , in a patient with transjugular intrahepatic portosystemic shunt ( tips ) , a filling defect ( arrowhead ) of the portal vein at the outlet of the superior mesenteric vein due to probable thrombus . 
5a portografia evidenzia , in un paziente portatore di tips , un difetto di riempimento ( testa di freccia ) della porta a livello dello sbocco della vena mesenterica superiore , da verosimile apposizione trombotica ; ben evidente inoltre la vena gastrica sinistra dilatata ( freccia ) con la presenza di spirali metalliche , da precedente embolizzazione . 
b posizionamento del plug ( testa di freccia ) allinterno della varice prima del rilascio definitivo : si riconoscono molto bene i due markers radiopachi posizionati alle due estremit del device . 
after thromboaspiration with an 8 - fr guiding catheter ( jr 4.0 , medtronic , mn , usa ) , a second angiography showed partial reduction of the thrombus and persistence of flow in the varix : we therefore opted for definitive embolisation . 
portography carried out 5 min after the procedure showed flow reduction through the device but incomplete closure ; two 12 - mm platinum coils ( nester , cook , bloomington , in , usa ) were endoprotesi aortoiliaca stato eseguito il giorno successivo per tre pazienti e due giorni dopo lembolizzazione per gli altri due . 
lembolizzazione unilaterale dellarteria iliaca interna stata tollerata da tutti e 5 i pazienti senza la comparsa di complicanze minori o maggiori quali claudicatio glutea , ischemia glutea o rettosigmoidea , disfunzioni sessuali o urologiche ; il periodo di ospedalizzazione stato in media 5 giorni dopo il posizionamento dellendoprotesi . 
il controllo angio - mdct a 1 mese ha evidenziato una buona rivascolarizzazione da parte di circoli collaterali delle due branche di divisione delliliaca interna trattata , anteriore e posteriore , senza passaggio di contrasto nel tronco comune e ha dimostrato la corretta posizione del plug con perfetta chiusura del vaso solo alla sua origine . 
 nei 3 pazienti a cui stata occlusa larteria succlavia sinistra , la mdct effettuata prima della dimissione e a 1 mese di distanza dal posizionamento dellendoprotesi aortica ha dimostrato la persistenza di endoleak di tipo ii dallarteria succlavia sinistra per due pazienti e in un paziente un endoleak misto : tipo i + tipo ii , ovvero dovuto sia ad una imperfetta sigillatura della protesi sulla parete aortica sia ad una riperfusione attraverso la succlavia : si pertanto optato per locclusione del vaso alla sua origine . 
prima di effettuare il trattamento i pazienti sono stati sottoposti a mdct e a studio eco - color doppler dei tronchi sovraortici e del circolo intracranico per escludere stenosi , ipoplasia o varianti anatomiche delle arterie carotidi , succlavie , vertebrali e del circolo del willis . 
i pazienti sono stati sottoposti quindi ad angiografia selettiva della ass che ha confermato la diagnosi di endoleak di tipo ii in due pazienti ed endoleak misto , tipo i + tipo ii , in un paziente , con perviet della vertebrale . 
tutti i pazienti sono stati dimessi due giorni dopo la procedura di occlusione : nessuno dei 3 pazienti ha avuto complicanze maggiori ( sindrome da furto della succlavia )  . 
il corretto posizionamento dellavp e lavvenuta occlusione dellarteria succlavia stato dimostrato anche mediante mdct di controllo . la fistola arterovenosa polmonare stata completamente esclusa con lutilizzo di due dispositivi avp , uno per ciascuna delle due arterie afferenti . 
il controllo angiografico ha dimostrato una chiusura totale dei due vasi embolizzati : in circa 3 minuti per il vaso maggiore e in minor tempo per quello di minori dimensioni . la saturazione percutanea di ossigeno in condizioni basali salita dal 73% al 93% subito dopo la procedura e si mantenuta stabile per i successivi 6 mesi di follow - up ; lemogasanalisi ha dimostrato normali pressioni di ossigeno e di anidride carbonica . 
il controllo clinico a 1 , 3 , 6 mesi ha dimostrato lassenza di sintomi respiratori , saturazione di ossigeno superiore al 95% in condizioni basali e un radiogramma del torace a tre mesi ha confermato una corretta e stabile posizione dei devices . nella fistola da emodialisi leco - color doppler ha dimostrato la presenza di due grosse dilatazioni vascolari anecogene , con presenza di flusso allinterno , a livello della piega del gomito . 
langiografia dellarto superiore , eseguita con accesso trans - omerale anterogrado 4 fr , ha confermato la presenza di una fistola arterovenosa in cui la legatura chirurgica della vena basilica efferente , eseguita 6 mesi prima , sia a livello dellanastomosi sia poco pi a valle , non aveva garantito una completa chiusura della connessione arterovenosa ; liperafflusso conseguente ha portato allo sviluppo di due grossi aneurismi venosi . 
al fine di escludere il flusso nei due aneurismi e nelle vene collaterali senza ricorrere ad una seconda legatura chirurgica si deciso , in accordo con il paziente , di chiudere definitivamente la fistola per via percutanea mediante avp . 
langiografia eseguita a 4 minuti dal posizionamento ha dimostrato una completa ed efficace chiusura della fistola con assenza di pasresults in the five patients undergoing closure of the common iliac artery , correct avp position was evaluated by means of a manual injection of contrast medium through the guiding catheter ; once in the correct position , the device was unscrewed and released . 
postprocedure angiography confirmed complete occlusion of the vessel within less than 8 mthe aortoiliac endografts were positioned on the following day in three patients and after 2 days in the other two . 
unilateral embolisation of the iia was tolerated by all five patients without minor or major complications , such as gluteal claudication , gluteal or rectosigmoid ischaemia and sexual or urological dysfunctions ; length of hospital stay was 5 days after endograft placement . 
mdct angiography at 1 month showed good revascularisation of the anterior and posterior branches of the treated iia by collateral circulations , without passage of contrast material in the common trunk , and demonstrated the correct position of the plug with perfect closure of the vessel origin . in the three patients who underwent occlusion of the lsa , mdct performed at discharge and 1 month after aortic endograft placement showed the persistence of type ii endoleak from the lsa in two patients and a mixed , type i and type ii , endoleak in one . 
these were both due to imperfect endograft sealing along the aortic wall and to reperfusion through the subclavian artery : we therefore decided to occlude the artery at its origbefore the embolisation procedure , the patients underwent mdct and colour - doppler us of the supraaortic trunks and intracranial vessels to exclude stenosis , hypoplasia or anatomical variants of the carotid , subclavian , vertebral arteries and the circle of willis . 
the patients were then studied by selective angiography of the lsa , which confirmed the type ii endoleak in two patients and the mixed type i and type ii endoleak in the other , with a patent vertebral artery . 
postprocedural angiography confirmed complete occlusion of the origin of the subclavian artery within less than 5 mthe patients were discharged 2 days after the procedure without developing major complications ( subclavian steal syndrome )  . 
correct avp positioning and successful subclavian artery occlusion were also demonstrated by follow - up mdct . the pulmonary arteriovenous malformation was completely excluded using two plugs , one for each of the two afferent arteries . 
baseline percutaneous oxygen saturation rose from 73% to 93% immediately after the procedure and remained stable for the following 6 months ; blood gas analysis demonstrated normal pressure of oxygen and carbon dioxide . 
arm angiography , done with 4 - fr antegrade humeral access , confirmed the presence of an arteriovenous fistula in which surgical ligation of the efferent basilic vein performed 6 months earlier at the level of the anastomosis and slightly below it had failed to guarantee complete closure of the arteriovenous communication . 
in order to exclude flow in the two aneurysms and in the collateral veins without performing a second surgical ligation , we decided in agreement with the patient to attempt definitive percutaneous closure of the fistula with an avp . 
angiography performed after 4 min demonstrated complete and effective closure of the fistula with absence of contrast in the basilic vein , two aneurysms and collateral veins and patency of the arm artery . 
colour - doppler us at 1 and 3 months confirmed the definitive closure of the fistula with complete resolution of the arm oedema and total thrombosis , with absence of flow in the two aneurysms . 
after placement of the two coils and the second plug , embolisation was achieved within about 5 mcolour - doppler us at 1 and 3 months demonstrated good patency of the tips , and angiography at 3 months confirmed varix closure . 
 discussion the avp has recently been shown to be effective in the occlusion of internal iliac arteries [ 1 ] , the treatment of pulmonary arteriovenous malformations [ 2 , 3 ] and as an occlusion system for a splenorenal shunt arising after tips [ 4 ]  . 
in our experience , avp was used to achieve vascular occlusion in five different arterial and venous settings . endograft placement in the abdominal aorta has become a valid alternative to conventional surgery and is increasingly the treatment of choice in elderly patients and subjects with high surgical risk . 
about 20% of abdominal aorta aneurysms have an iliac component [ 6 ] , and often the neck of the distal common iliac artery is insufficient to provide an adequate landing zone for the grawhen the aneurysm involves the common iliac artery as far as the origin of the iia , it is necessary to cover the iia with the graft and saggio di mdc nella vena basilica e di conseguenza nei due aneurismi e nelle vene collaterali con perviet dellasse arterioso dellarto . 
il controllo clinico ed eco - color doppler effettuato a 1 e a 3 mesi ha confermato la buona e definitiva chiusura della fistola con risoluzione completa delledema dellarto e trombosi totale , con assenza di flusso nei due aneurismi . la grossa varice gastrica stata chiusa con 2 avp e 2 spirali in platino dato il diametro particolarmente ampio e la persistenza di flusso dopo limpianto del primo plug . 
i controlli eco - color doppler a 1 e 3 mesi hanno mostrato buona perviet della tips e il controllo angiografico a 3 mesi ha confermato la chiusura della varice . discussione recentemente lefficacia dellavp stata dimostrata per locclusione di arterie iliache interne [ 1 ] , nel trattamento di fistole arterovenose polmonari [ 2 , 3 ] e come sistema per locclusione di uno shunt spleno - renale in seguito al posizionamento di tips [ 4 ]  . 
la descrizione della validit dellavp relativamente ad una casistica ampia e al trattamento di patologie vascolari pluridistrettuali , non stata ancora riportata , a nostra conoscenza , da alcun autore . nellesperienza qui riportata lavp stato utilizzato per locclusione vascolare in 5 diverse patologie , sia sul versante arterioso sia su quello venoso . il posizionamento di endoprotesi dellaorta addominale , ormai una valida alternativa alla chirurgia tradizionale e sempre pi spesso il trattamento di scelta in pazienti anziani e ad alto rischio operatorio ; i vantaggi , come noto , sono la minore invasivit , la minor durata della procedura e dellospedalizzazione , la ridotta perdita di sangue e la ridotta morbillit e mortalit rispetto alla chirurgia aperta [ 5 ]  . 
circa il 20% degli aneurismi dellaorta addominale ha una componente aneurismatica iliaca [ 6 ] e spesso il colletto dellarteria iliaca comune distale insufficiente per assicurare un adeguato atterraggio della protesi . 
quando la patologia aneurismatica coinvolge larteria iliaca comune fino allorigine dellarteria iliaca interna ( aii ) risulta necessario ricoprire con la protesi laii ed estendere la protesi fino allarteria iliaca esterna . 
nellottica quindi di prevenire un endoleak di ii tipo ( da vasi collaterali ) e quindi garantire una buona esclusione dellaneurisma raccomandata la chiusura , pre - posizionamento di endoprotesi , della aii [ 710 ]  . 
lembolizzazione prossimale della aii , utilizzando le spirali tradizionali , una tecnica relativamente sicura ed efficace ed stata riportata da molti autori [ 8 , 10 , 11 ]  . 
i maggiori difetti delle spirali sono la necessit di utilizzarne spesso un numero molto elevato , prima di riuscire a chiudere adeguatamente il vaso , lalto costo e la durata della procedura ; inoltre pu residuare un flusso anterogrado attraverso le spirali , si pu avere una dislocazione distale delle stesse o una protrusione allinterno del lume delliliaca comune o esterna [ 12 , 13 ]  . 
da marzo 2005 abbiamo iniziato ad utilizzare lavp al posto delle spirali per embolizzare preventivamente le arterie iliache interne ; questo dispositivo consente unottima occlusione prossimale del vaso allorigine , prima c . 
therefore , to prevent a type ii endoleak ( due to collaterals ) and guarantee adequate exclusion of the aneurysm , closure of the iia before endograft placement is recommended [ 710 ]  . 
in addition , there may be residual antegrade flow through the coils , distal migration , or protrusion within the lumen of the common or external iliac artery [ 12 , 13 ]  . 
in march 2005 , we started using the avp instead of coils for preventive embolisation of iias ; the device allows excellent proximal occlusion at the vessel origin , before the bifurcation , guaranteeing better revascularisation of the collateral branches of the contralateral hypogastric artery and reducing complications due to hypoperfusion . even thoracic aorta endovascular repair has been approved as a less invasive treatment compared with conventional surgery [ 14 ]  . 
the most important anatomical prerequisite for correct positioning of the stent - graft is the presence of a neck of adequate length ( at least 1520 mm ) distal to the lsa orighowever , descending thoracic aorta lesions often involve the distal aortic arch , with a proximal neck less than 15 mm : in these cases one technique enabling safe device fixation is the creation of a more proximal landing zone with deliberate overstenting of the lsa ostium [ 5 , 15 , 16 ]  . this procedure can only be done after excluding abnormalities of the vertebral and carotid arteries and the circle of willis and if the left internal mammary artery has not been used for a coronary bypass . 
all proximal endoleaks have an incidence of 0%23% for early endoleaks ( detected during stent - graft placement ) and 0%5% for late endoleaks , and they may be related to aneurysm morphology , dissection or even technical expertise [ 15 ]  . 
if this type of endoleak ( type ii from the subclavian artery ) persists , it needs to be promptly repaired because of the direct connection between the aneurysmal sac or false lumen and systemic arterial pressure . 
our three patients underwent avp embolisation of the origin of the subclavian artery because they had developed a type ii or mixed ( type i and ii ) endoleak from the subclavian artery , which was overstented at its origin due to an inadequate proximal neck . 
the use of metal coils is not advised for subclavian occlusion [ 15 ] due to the high risk of distal embolisation and the likelihood of not being able to block flow completely . 
these are abnormal , direct communications between pulmonary arteries and veins without a capillary bed , which are caused by the formation of an aneurysmal sac or a tangle of tortuous vessels [ 1820 ]  . 
treatment opdella biforcazione nei suoi due rami , garantendo una migliore rivascolarizzazione da rami collaterali dellipogastrica controlaterale riducendo in questo modo possibili complicanze da ipoperfusione . anche il trattamento endovascolare della patologia dellaorta toracica ormai stato approvato come trattamento meno invasivo rispetto alla chirurgia tradizionale [ 14 ]  . 
il pi importante requisito anatomico per il corretto posizionamento dellendoprotesi la presenza di un colletto minimo di 1520 mm distalmente allorigine dellostio dellass . tuttavia la patologia dellaorta toracica discendente spesso coinvolge larco aortico distale con un colletto prossimale inferiore a 15 mm : in tali casi una delle tecniche per un sicuro fissaggio del dispositivo un atterraggio pi prossimale con la copertura volontaria dellostio dellass [ 5 , 15 , 16 ]  . tale procedura pu essere effettuata soltanto escludendo prima patologie a carico delle arterie vertebrali , delle carotidi , del circolo del willis e se la mammaria interna sinistra non stata utilizzata per un bypass coronarico . un endoleak di tipo ii dalla ass pu insorgere dopo posizionamento di endoprotesi dellaorta discendente ma ad oggi non riportata in letteratura lesatta incidenza . 
la percentuale di tutti gli endoleak prossimali varia dallo 0% al 23% per gli endoleak precoci ( dimostrati al momento del posizionamento della protesi ) e dallo 0% al 5% per quelli tardivi e possono essere legati allanatomia dellaneurisma o dissezione o anche allesperienza delloperatore [ 15 ]  . 
questo tipo di endoleak ( tipo ii dalla succlavia ) se persiste richiede una tempestiva correzione a causa della diretta comunicazione tra la sacca aneurismatica o il falso lume e la pressione arteriosa sistemica . 
i nostri 3 pazienti sono stati sottoposti ad embolizzazione dellorigine della succlavia con avp , poich avevano sviluppato un endoleak di tipo ii o misto ( tipo i + tipo ii ) dalla succlavia che stata ricoperta dallendoprotesi alla sua origine per la presenza di un colletto prossimale insufficiente . 
lutilizzo delle spirali metalliche per locclusione della succlavia non consigliabile [ 15 ] per il forte rischio di embolizzazione distale e per lalta probabilit di non riuscire a bloccare totalmente il flusso : il nuovo dispositivo avp consente unimmediata , sicura e rapida occlusione allorigine del vaso senza complicanze emboliche distali . 
per questultima caratteristica lavp assume unimportante ruolo nel trattamento delle fistole arterovenose polmonari ( favp ) ; questultime sono delle anormali connessioni dirette tra arterie e vene polmonari con lesclusione del letto capillare dovute alla formazione di una sacca aneurismatica o ad un groviglio di canali vascolari tortuosi [ 1820 ] : estremamente eterogenea la presentazione clinica [ 18 , 21 , 22 ]  . 
le opzioni terapeutiche includono lembolizzazione percutanea o lescissione chirurgica [ 2 ]  . data la minore invasivit e lo sviluppo di nuovi materiali embolizzanti il trattamento percutaneo divenuto il trattamento di scelta per la maggior parte dei pazienti [ 2325 ]  . 
la ricanalizzazione della favp pu avvenire in una percentuale compresa tra il 5% e il 10% dei pazienti trattati [ 26 , 27 ] : pertanto , la scelta di un materiale embolizzante appropriato e laccurata localizzazione del sito dove iniziare lembolizzazione di cruciale importanza [ 23 , 24 ]  . 
recanalisation of pavf may occur in 5%10% of treated patients [ 26 , 27 ] , so the choice of appropriate embolising material and accurate localisation of the site where embolisation is to be started are crucial [ 23 , 24 ]  . 
these considerations are even more important in massive fistulas , which are more difficult to occlude with coils or detachable balloons due to the risk of distal migration [ 25 , 28 ]  . 
we believe the avp to be safer and easier to use than the above - mentioned devices owing to the simplicity and small size of the release system and , more importantly , because it was designed for vascular use and is therefore more specific and better suited to the tubular morphology of vessels seen in pavf . haemodialysis fistulas often develop complications , one of the most common being aneurysm formation [ 31 , 32 ]  . possible treatment options include surgery , endovascular treatment or both . 
we opted for the avp because its release is controlled and it can be placed precisely at the level of the neck where it readily adheres to the vessel without risking distal migration . 
to our knowledge , no author has described the use of the avp as an embolising device for the closure of a haemodialysis fistula . the efficacy of tips is well documented in the treatment of variceal bleeding refractory to endoscopic treatment [ 36 , 37 ]  . 
although tips alone is sufficient to stop variceal bleeding in many cases [ 3840 ] , in some patients with large collateral veins , it may not be enough ; embolisaton of the varix therefore becomes indispensable [ 4144 ] , as in the case treated by us . 
even very large coils ( 20 mm15 cm ) are susceptible to distal migration , and the same applies to other materials such as sclerosing agents , glue and gelatine sponge particles , which are not very effective and only increase the risk of systemic embolisation . 
in our opinion , the avp is the vascular occluder that best adapts to large vessels such as gastric varices ; in addition , it can be used is combination with coils to make vascular occlusion even more rapid . our experience indicates that the avp is an extremely versatile occlusion system that is suitable for variety of vessel to pi difficile occluderle con le spirali o i palloni staccabili a causa della possibilit di migrazione distale [ 25 , 28 ]  . 
migliori risultati sono stati ottenuti in passato con lutilizzo di vari device , ad uso cardiologico realizzati per il trattamento della perviet del dotto arterioso di botallo e dei difetti settali cardiaci , quali il gianturco - grifka , composto prevalentemente da un sacco in nylon flessibile e una guida occludente , il cardioseal , costituito da un doppio ombrellino ciascuno con quattro molle metalliche e stoffa di poliestere e lamplatzer duct occluder , realizzato con una maglia guida in nitinolo con estremit a disco [ 24 , 29 , 30 ]  . 
noi riteniamo che lavp , sia pi sicuro e facile da utilizzare rispetto ai precedenti devices menzionati , per la semplicit e le ridotte dimensioni del sistema di rilascio ma soprattutto , essendo un dispositivo dedicato allimpiego vascolare , risulta pi specifico e meglio conformabile allanatomia tubulare del vaso come nel caso delle malformazioni arterovenose polmonari . le fistole da emodialisi , sono gravate da alcune complicanze tra cui una delle pi comuni la formazione di aneurismi [ 31 , 32 ]  . 
lapproccio endovascolare pu avvalersi del posizionamento di uno stent ricoperto a livello arterioso , in modo da escludere la zona di anastomosi , oppure lembolizzazione a livello anastomotico arterioso della fistola [ 3335 ]  . 
nel nostro caso , poich la fistola era localizzata a livello del gomito , lutilizzo di uno stent ricoperto era controindicato e pertanto lunica indicazione terapeutica percutanea era lembolizzazione transcatetere . 
abbiamo preferito utilizzare un avp perch ha un rilascio controllato e pu essere posizionato esattamente a livello del colletto , aderendo prontamente al vaso senza rischio di migrazione distale sia sul versante arterioso sia su quello venoso . 
a nostra conoscenza nessun autore , prima dora , ha descritto limpiego dellavp come sistema embolizzante per la chiusura di una fistola arterovenosa da emodialisi . lefficacia della tips stata ben provata nel trattamento del sanguinamento da varici resistenti al trattamento endoscopico [ 36 , 37 ]  . 
in molti casi la tips da sola sufficiente a bloccare il sanguinamento delle varici [ 3840 ] tuttavia in alcuni pazienti con grosse vene collaterali pu non bastare ; pertanto in tali soggetti lembolizzazione della varice risulta indispensabile [ 4144 ] , come nel caso da noi trattato . 
il grande diametro di questi vasi collaterali costituisce il principale problema nella scelta del materiale embolizzante : anche spirali metalliche molto grandi ( 20 mm15 cm ) possono facilmente migrare distalmente . 
ugualmente vale per altri materiali come agenti sclerosanti , colla , particelle di spugna di gelatina che non hanno una grande efficacia e aumentano solo il rischio di embolizzazione sistemica . 
a nostro giudizio lavp il dispositivo di occlusione vascolare che meglio si adatta a vasi di grosse dimensioni come le varici gastriche : pu inoltre essere utilizzato in associazione alle spirali per rendere ancora pi rapida locclusione vascolare . in conclusione , in base alla nostra esperienza , possiamo affermare che lavp si rivelato un sistema di occlusione vascolare estremamente versatile , adatto quindi a vasi di diametro eterogeneo , facile da usare , preciso nel rilascio , c . 
in our experience , the use of abdominal endografts with suprarenal fixation did not lead to any significant increase in morphological and / or functional renal complications compared with those with infrarenal fixation . key words ct angiography abdominal aortic aneurysm stent graft suprarenal fixation renal complication riassunto obiettivo . 
sono stati analizzati retrospettivamente tutti gli esami angio - tc di controllo ( follow - up a 1 , 6 , 12 mesi e quindi 1 / anno ) e i test di laboratorio eseguiti su 102 pazienti sottoposti a posizionamento di endoprotesi ad aggancio soprarenale ( 60 pazienti , gruppo a ) o sottorenale ( 42 pazienti , gruppo b )  . 
la lunghezza del colletto prossimale risultata inferiore nel gruppo a ( 2 , 14 cm0 , 84 cm ) rispetto al gruppo b ( 3 , 41 cm1 , 21 cm )  . 
nel nostro studio limpianto di endoprotesi addominali ad aggancio soprarenale non ha determinato un aumento significativo di complicanze renali morfologiche e / o funzionali rispetto ai pazienti trattati con endoprotesi ad aggancio sottorenale . parole chiave angiografia ct aneurisma aortico addominale stent - graft aggancio soprarenale complicazioni renali a.r. 
the conventional approach to aaa is surgery , which is associated with a mortality rate of 1.4%6.5% , which increases to 20% if the patients are at high surgical risk due to severe concomitant disease and reaches 50% when surgery is performed in an emergency setting due to aneurysm rupture [ 3 , 4 ]  . 
 over the last few years , a less invasive alternative to open surgery has been introduced with excellent results : the imaging - guided intraluminal positioning of a covered stent - graft . success of endovascular repair in terms of aneurysm exclusion and absence of perioperative and postoperative complications is dependent on accurate patient selection to ensure that only aneurysms with a morphology that corresponds to well - established indications are treated [ 57 ]  . 
on the other hand , the indications for endovascular repair are continuously evolving as a result of the growing experience of surgeons and the improved versatility and applicability of the new stent - grafts [ 5 ]  . 
one example is the new generation of endografts with suprarenal fixation that , by extending the proximal anchorage point cranially , have broadened the inclusion criteria to aneurysms with hostile i.e. 
however , the meshes of the uncovered metallic portion of the graft , which ensure suprarenal fixation , overlap with the ostia of the renal arteries and may cause damage to the renal arteries , the renal parenchyma and renal function . 
published results are conflicting so that the issue remains controversial [ 813 ]  . the purpose of our study was to compare the rate of morphological and functional renal complications after placement of suprarenal and infrarenal aortic stent - grafts for endovascular abdominal aortic aneurysm repair ( evar )  . materials and methods patients from january 2000 to june 2004 , we positioned aortic endografts in 140 patients with abdominal aortic aneurysms . 
indications for endovascular repair and procedure planning ( graft selection ) were defined by a team of vascular surgeons and interventional radiologists on the basis of the aneurysms clinical and morphological characteristics [ derived from preprocedural computed tomography ( ct ) angiography ] along the guidelines proposed by the italian transfemoral endovascular aneurysm management ( team ) group and by the sezione di studio di radiologia vascolare ed interventistica ( vascular and interventional radiology study section ) ( sirm ) [ 14 ]  . 
in particular , inclusion criteria for endovascular repair were : age 65 years ; aneurysm sac diameter < 7 cm ; proximal neck length 15 mm ; proximal neck diameter < 30 mm ; proximal neck angulation > 120 ; proximal laneurisma dellaorta addominale una patologia di notevole rilevanza clinica , con unincidenza stimata in 2040 casi su 100000 abitanti per anno ed responsabile dell1 , 7% dei decessi nei soggetti con et compresa tra 65 e 74 anni [ 1 , 2 ]  . 
il trattamento tradizionale dellaneurisma dellaorta addominale di tipo chirurgico ed gravato da un rischio di mortalit variabile tra l1 , 4% e il 6 , 5% , che pu aumentare sino al 20% se lintervento effettuato in pazienti ad alto rischio chirurgico per gravi patologie concomitanti e raggiunge il 50% quando lintervento viene effettuato in emergenza per rottura dellaneurisma stesso [ 3 , 4 ]  . negli ultimi anni stata proposta ed utilizzata sempre pi diffusamente una metodica alternativa alla chirurgia tradizionale , meno invasiva , che consiste nel posizionamento imaging - guidato per via endoluminale di uno stent - graft ricoperto e che ha dimostrato risultati estremamente soddisfacenti . 
il successo del trattamento endovascolare , in termini di esclusione dellaneurisma ed assenza di complicanze perie post - operatorie , dipende da unaccurata selezione dei pazienti al fine di trattare solamente quei casi nei quali le caratteristiche morfologiche dellaneurisma siano perfettamente rispondenti ad indicazioni ben codificate . 
daltra parte , le indicazioni al trattamento endovascolare sono in continua evoluzione , sia per la crescente esperienza degli operatori , che tendono ad applicare questa procedura ad una quota sempre maggiore di pazienti , sia per la disponibilit di nuovi modelli di endoprotesi con maggiori caratteristiche di versatilit ed applicabilit [ 5 ]  . 
un esempio rappresentato dalle nuove generazioni di protesi ad aggancio soprarenale che , estendendo cranialmente la sede di ancoraggio prossimale , hanno consentito di ampliare i criteri di inclusione anche ad aneurismi con colletti definiti ostili , ossia corti , tortuosi o angolati , riducendo potenzialmente il rischio di migrazione caudale dello stent - graft e di endoleak di tipo i prossimale [ 6 , 7 ]  . 
tuttavia , la porzione metallica scoperta delle protesi , deputata allaggancio soprarenale , si sovrappone con le sue maglie allostio delle arterie renali con potenziali effetti dannosi sulle arterie renali , sul parenchima renale e sulla funzionalit renale . 
gli studi presenti in letteratura a tale proposito riferiscono risultati contrastanti tali da mantenere ancora aperta tale problematica [ 813 ]  . lo scopo del nostro lavoro stato quello di confrontare il tasso di complicanze renali morfologiche e funzionali , dopo posizionamento di endoprotesi aortiche ad aggancio sopra e sottorenale per il trattamento endovascolare dellaneurisma dellaorta addominale ( evar )  . materiali e metodi pazienti da gennaio 2000 a giugno 2004 , 140 pazienti con aneurisma dellaorta addominale sono stati sottoposti presso il nostro centro a posizionamento di endoprotesi aortica . 
sixty patients ( group a ) ( 58 men ; two women ; mean age : 71.3 years , range : 6286 years ) received suprarenal endografts ( 55 talent , medtronicave ; five zenith , cook ) , whereas the remaining 42 patients ( group b ) ( 41 men ; one woman ; mean age : 69.1 years , range : 6189 years ) received infrarenal endografts ( 25 aneurx ; 17 excluder , gore )  . mean neck length was 2.140.84 cm ( range 0.85.5 cm ) in group a and 3.411.21 cm ( range 25.3 cm ) in group b , whereas the rate of hostile necks was 41.7% ( 25 / 60 patients ) in group a and 14.3% ( 6 / 42 patients ) in group b . 
in particular , in group a , the proximal neck was short ( < 1.5 cm ) in eight patients , tortuous in 12 patients , angulated ( > 120 ) in six patients , and showed significant thrombotic appositions in 15 patients and ulcerations in five patients . 
in group b , no patient had a short proximal neck ( < 1.5 cm ) ; the proximal neck was tortuous in four patients , angulated ( > 120 ) in three patients , and had significant thrombotic appositions in five patients and ulcerations in one patient ( table 1 )  . diagnostic procedures and clinical laboratory evaluation after endovascular repair , all patients underwent clinical / laboratory follow - up with creatinine clearance ( crcl ) and systemic arterial pressure ( ap ) monitoring and imaging follow - up with ct angiography at 1 , 6 and 12 months and yearly thereafter . 
renal function was evaluated by calculating crcl using the cockcraft and gault equation [ 15 ] : crcl = ( 140patients age ) patients weight ( kg ) / 72serum creatinine ( mg / 100 ml )  . 
any changes in renal function were defined on the basis of the comparison between the pretreatment crcl values and those obtained at the last follow - up test at least 1 year after the procedure . 
both the crcl and the ap values were obtained from patients medical records and reviewed by a team member not involved in the interpretation of ct images . follow - up ct angiography was done with a multidetector technique ( somatom volume zoom , siemens , medical solutions , forchheim ) before and during administration of 120 ml of contrast agent ( 300 mgi / ml ; 3 ml / s flow rate )  . 
precontrast acquisition was carried out with 42.5 - mm collimation , procedura ( scelta della protesi ) sono state definite da unequipe mista di chirurghi vascolari e radiologi interventisti sulla base di criteri clinici e caratteristiche morfologiche dellaneurisma ( queste ultime desumibili dallesame angio - tc eseguito prima del trattamento ) , tenendo conto delle linee guida proposte dal team ( transfemoral endovascular aneurysm management ) italiano , a cura della sezione di studio di radiologia vascolare ed interventistica della sirm [ 14 ]  . 
in particolare , i criteri di inclusione al trattamento endovascolare utilizzati sono stati : et del paziente 65 anni ; diametro della sacca aneurismatica < 7 cm ; lunghezza del colletto prossimale 15 mm ; diametro del colletto prossimale < 30 mm ; angolazione del colletto prossimale > 120 ; colletto prossimale con calcificazioni parietali coinvolgenti meno della met della sua circonferenza in assenza di significativa apposizione trombotica ; angolazione arterie iliache > 90 ( < 90 in assenza di diffuse calcificazioni ) ; diametro arteria iliaca esterna > 7 mm e < 14 mlindicazione al trattamento endovascolare stata inoltre posta nei pazienti giudicati ad elevato rischio chirurgico ( gravi condizioni cardiorespiratorie , addome ostile ) , indipendentemente dallet del paziente e dalle caratteristiche morfo - strutturali dellaneurisma . tutti i pazienti sottoposti ad evar e provvisti di documentazione completa riguardante i dati del follow - up strumentale e clinico - laboratoristico ad almeno 1 anno dalla procedura sono stati inclusi nel nostro studio . 
in 60 pazienti ( gruppo a ) ( maschi 58 ; femmine 2 ; et media : 71 , 3 anni ; range : 6286 anni ) stata posizionata una protesi ad aggancio soprarenale ( 55 talent , medtronic - ave ; 5 zenith , cook ) , mentre nei restanti 42 pazienti ( gruppo b ) ( maschi 41 ; femmine 1 ; et media : 69 , 1 anni ; range : 6189 anni ) stata posizionata una protesi ad aggancio sottorenale ( 25 aneurx ; 17 excluder , gore )  . la lunghezza media del colletto era di 2 , 140 , 84 cm ( range 0 , 85 , 5 cm ) nel gruppo a e 3 , 411 , 21 cm ( range 25 , 3 cm ) nel gruppo b , mentre la percentuale di colletti ostili era di 41 , 7% ( 25 / 60 pazienti ) e 14 , 3% ( 6 / 42 pazienti ) per il gruppo a e b rispettivamente . 
in particolare nel gruppo a il colletto prossimale risultato corto ( < 1 , 5 cm ) in 8 pazienti , tortuoso in 12 pazienti , angolato ( > 120 ) in 6 pazienti e ha mostrato significative apposizioni parietali trombotiche e / o ulcerazioni , in 15 e 5 pazienti rispettivamente . 
negli 8 pazienti con colletto prossimale < 1 , 5 cm , la decisione di ricorrere al trattamento endovascolare derivata dalla presenza di fattori di rischio per lintervento chirurgico tradizionale . nel gruppo b , nessun paziente presentava un colletto prossimale definito corto ( < 1 , 5 cm ) ; il colletto prossimale risultato tortuoso in 4 pazienti , angolato ( > 120 ) in 3 pazienti , con significative apposizioni parietali trombotiche ed ulcerazioni in 5 ed 1 paziente , rispettivamente ( tabella 1 )  . indagini strumentali e valutazione clinico - laboratoristica tutti i pazienti sottoposti a trattamento endovascolare sono stati controllati nel tempo con un follow - up clinico - laboratoristico , mediante il monitoraggio della clearance della creatinina ( clcr ) e della pressione arteriosa sistemica , e a.r. 
the contrast study was carried out with 41 - mm collimation , pitch = 6 , gantry rotation speed = 0.5 s , slice thickness = 1.25 mm , and reconstruction interval = 1 mthe voi extended from a plane passing through the coeliac trunk to one passing through the common femoral arteries , with an average acquisition time of 25 s . 
axial and three - dimensional ( 3d ) images were reviewed on a dedicated workstation ( leonardo , siemens , medical solutions , forchheim ) to confirm the development and / or progression of steno - occlusive lesions of the renal arteries and the presence of ischaemic parenchymal changes ( renal infarction )  . 
steno - occlusion of the renal arteries was evaluated on a 4 - point scale : grade 0 = no stenosis ; grade 1 = < 50% stenosis ; grade 2 = > 50% stenosis : grade 3 = occlusion . 
alterations of the urographic effect associated with changes in the size of the renal parenchyma were interpreted as evidence of renal infarction . renal infarctions occupying less than 20% of the entire kidney volume were considered small . strumentale , mediante esame angio - tc a 1 , 6 e 12 mesi e quindi 1 / anno dopo la procedura . 
la funzionalit renale stata valutata mediante il calcolo della clearance della creatinina ( clcr ) utilizzando la formula di cockcraft [ 15 ] : clcr = ( 140 - et del pz ) peso del pz ( kg ) / 72livello sierico della creatinina ( mg / 100 ml )  . 
la presenza / assenza di variazioni della funzionalit renale stata definita dal confronto dei valori della clcr pre - trattamento con quelli ottenuti nellultimo controllo , eseguito almeno 1 anno dalla procedura . 
in tutti i pazienti sono stati inoltre misurati e comparati i valori della pressione arteriosa sistemica pre - trattamento con quelli ottenuti nellultimo controllo , ovvero almeno 1 anno dopo evar . 
i valori della clcr e della pressione arteriosa sono stati ottenuti dalla revisione delle cartelle cliniche dei pazienti , effettuata da uno dei componenti dellequipe non coinvolto nella interpretazione delle immagini tc . gli esami angio - tc di controllo sono stati eseguiti con tecnica multistrato ( somatom volume zoom , siemens , medical solutions , forchheim ) prima e durante somministrazione di 120 ml di mdc ( 300 mgi / ml ; flusso 3 ml / s )  . 
lacquisizione senza somministrazione di mdc stata eseguita con collimazione di 42 , 5 mm , pitch 6 , velocit di rotazione del sistema tubo radiogeno - detettori di 0 , 5 s , spessore dello strato ed intervallo di ricostruzione di 5 mm , campo di vista ( fov ) , in media , di 240 mm volume di interesse ( voi ) estea.r. 
at follow - up after 1 year , there was only one case of progression from a grade 1 to a grade 2 stenosis ( 1 / 9 , 11.1% ) whereas the remaining eight cases were unchanged . 
among the 115 arteries free of stenosis before treatment , ct angiography at 1 year identified three new grade 2 stenoses ( 3 / 115 , 2.6% ) so da d12 alla sinfisi pubica . 
lacquisizione con mdc stata eseguita con collimazione di 41 mm , pitch 6 , velocit di rotazione del sistema tubo radiogeno - detettori di 0 , 5 s , spessore dello strato di 1 , 25 mm ed intervallo di ricostruzione di 1 mil voi stato esteso da un piano passante per il tripode celiaco sino ad un piano passante per le arterie femorali comuni , con un tempo di acquisizione medio di 25 s . 
il ritardo di scansione stato individuato per ogni paziente mediante un sistema automatico di bolus tracking ( care bolus , siemens ) e posizionamento di una roi ( region of interest ) nel lume dellaorta addominale soprarenale . lanalisi delle immagini tc ( esami pree post - trattamento ) stata effettuata retrospettivamente in consensus da due radiologi esperti in procedure endovascolari ed angiotc , valutando le immagini assiali e 3d su una stazione dedicata ( leonardo , siemens , medical solutions , forchheim ) al fine di verificare linsorgenza e / o la progressione di patologia steno - ostruttiva a carico delle arterie renali e la presenza di alterazioni parenchimali renali su base ischemica ( infarto renale )  . 
la valutazione della patologia steno - ostruttiva delle arterie renali stata effettuata utilizzando una scala a 4 gradi : grado 0 = assenza di stenosi ; grado 1 = stenosi < 50% ; grado 2 = stenosi > 50% : grado 3 = occlusione . 
gli infarti renali occupanti meno del 20% dellintero volume del rene sono stati considerati piccoli infarti . analisi statistica i dati clinico - laboratoristici e strumentali ottenuti in entrambi i gruppi di pazienti sono stati confrontati con il test t di student , al fine di verificare la presenza di differenze significative in termini di complicanze sul parenchima renale , sulle arterie renali e sullandamento della clearance della creatinina , considerando significativa una differenza di p < 0 , 05 . 
la valutazione statistica stata effettuata mediante lo stata statistical software ( release 8.2 , college station , tx ; stata corp lp )  . risultati in nessun paziente si sono verificati problemi tecnici al momento del posizionamento e rilascio dellendoprotesi , n la necessit di conversione chirurgica intraoperatoria e / o in fase intra / peri - procedurale . 
i due gruppi di pazienti sono risultati statisticamente simili dal punto di vista epidemiologico ( et : 71 , 3 anni versus 69 , 1 anni , p = ns ; distribuzione m / f : 58 / 2 versus 41 / 1 , p = ns )  . 
at follow - up , only one lesion was found to have progressed from a grade 1 to a grade 2 stenosis ( 1 / 8 , 12.5% ) ; the remaining seven case were unchanged . 
inoltre non si sono osservate differenze statisticamente significative n in termini di numero di pazienti con riduzione della clcr maggiore o uguale al 20% ( 11 , 86% nel gruppo a versus 7 , 1% , nel gruppo b , p > 0 , 05 ) , n in termini di decremento medio della clcr in questo gruppo selezionato di pazienti ( - 38 , 97% versus - 30% , p > 0 , 05 )  . 
multidetector computed tomography ( mdct ) angiography , three - dimensional ( 3d ) ( a , c , d ) and axial ( b ) images ; digital subtraction angiogram ( dsa ) ( e , f )  . 
lesame tc eseguito ad 1 anno dalla procedura di evar ( c , d ) documenta la comparsa di una stenosi eccentrica dellarteria renale destra ( frecce ) , non presente allesame tc pre - evar ( a , b ) ( frecce )  . 
regolare perviet dellarteria renale destra ( a ) ( freccia ) che al controllo a 12 mesi dallimpianto appare ostruita ( b ) ( freccia ) con conseguente infarto renale omolaterale ( punta di freccia )  . discussion in abdominal endografts with suprarenal fixation , the proximal anchorage point can be extended upwards to the renal arteries thanks to the presence of a portion of the prosthesis not covered by the graft ( free - flow section )  . 
nel follow - up , solo 1 stenosi progredita da grado 1 a grado 2 ( 1 / 8 , 12 , 5% ) mentre le rimanenti 7 sono rimaste immodificate . 
la valutazione delle 76 arterie renali indenni da stenosi prima del trattamento non ha documentato linsorgenza di alcuna nuova lesione steno - ostruttiva . nel gruppo a si documentata la comparsa di un rene grinzo , secondario allocclusione dellarteria renale principale omolaterale , e di un infarto polare inferiore secondario a.r. 
computed tomography ( ct ) axial images ( a , b ) show that the endograft covers one left lower polar artery , with resulting infarction of the lower kidney pole ( c ) ( arrow )  . 
 appare pertanto giustificata la tendenza a verificare leffetto nel tempo di queste protesi a livello della funzionalit renale , delle arterie renali e del parenchima renale [ 13 , 1620 ]  . in letteratura sono presenti diversi studi comparativi tra le protesi ad aggancio soprarenale e quelle ad aggancio sottorenale con risultati contrastanti . 
these figures were confirmed by bockler et al . , who reported a 19% rate of renal infarction in patients treated with suprarenal stent - grafts ( 398 patients ) compared with 3.7% in those treated with infrarenal stentgrafts ( 265 patients ) [ 21 ]  . 
studied 55 patients treated with infrarenal stent - grafts and 32 patients with suprarenal stent - grafts , finding a higher incidence of progression of steno - occlusive lesions in the group with suprarenal grafts [ 20 ]  . 
on 99 , 192 , and 113 patients , respectively [ 2426 ]  . dotto su 130 pazienti , di cui 69 trattati con protesi ad aggancio soprarenale e 61 con protesi ad aggancio sottorenale , si osservata una maggiore percentuale di piccoli infarti renali con lutilizzo di protesi ad aggancio soprarenale rispetto allaggancio sottorenale ( 5 , 8% versus 1 , 6% ) , seppure in assenza di differenze significative in termini di funzionalit renale [ 19 ]  . 
tale dato appare confermato dal lavoro di bockler che riporta una percentuale di infarti renali pari al 19% nel gruppo di pazienti trattati con protesi ad aggancio soprarenale ( 398 pazienti ) e 3 , 7% nel gruppo trattato con protesi ad aggancio sottorenale ( 265 pazienti ) [ 21 ]  . 
nello studio di lau , condotto su 55 pazienti trattati con protesi ad aggancio sottorenale e 32 pazienti con protesi aggancio soprarenale , si documentato una maggiore incidenza di progressione di patologia steno - ostruttiva nel gruppo di pazienti con protesi ad aggancio soprarenale [ 20 ]  . 
al contrario , nellesperienza di malina e marin lutilizzo di protesi ad aggancio soprarenale non ha aumentato il rischio di complicanze sulle arterie renali , sul parenchima renale e sulla funzionalit renale [ 22 , 23 ]  . 
tali risultati appaiono confermati anche dagli studi condotti da kramer , burks e surowiec rispettivamente su 99 , 192 e 113 pazienti [ 2426 ]  . nel nostro studio la valutazione retrospettiva degli esami angio - tc , pree post - evar , non ha documentato differenze statisticamente significative in termini di insorgenza / progressione delle lesioni steno - ostruttive delle arterie renali ( 11 , 1% nel gruppo a versus 12 , 5% nel gruppo b ) n in termini di alterazioni parenchimali renali . 
a significant finding is the tendency for renal function to decline in all patients undergoing evar , regardless of the type of graft employed ; as previously reported , this decline in renal function appears similar to that occurring after open surgery . 
in the case of surgery , the decline is secondary to distal embolisation phenomena connected with the operation , to the possible development of renal ischaemia after renal artery clamping or to possible renal artery injury ( dissection , occlusion ) during the operation [ 12 ]  . 
 patologia steno - ostruttiva delle arterie renali e di alterazioni parenchimali renali associata allutilizzo di protesi ad aggancio soprarenale ( 3 , 5% versus 0% ) , seppur senza differenze statisticamente significative tra i due gruppi di pazienti . la valutazione dei livelli della pressione arteriosa non ha documentato significative variazioni post - trattamento , sia in assoluto sia paragonando i due gruppi . 
tale risultato coincide con i dati riportati in letteratura secondo i quali le protesi ad aggancio soprarenale non modificano in maniera significativa i valori di pressione arteriosa del paziente [ 22 , 23 ]  . lanalisi ad un anno dalla procedura della funzionalit renale in termini di variazione della clcr registrate nei due gruppi , non ha documentato differenze statisticamente significative ( - 8 , 75 nel gruppo a versus - 6 , 40 nel gruppo b )  . 
risultati simili sono emersi anche confrontando il numero di pazienti con decremento della clcr maggiore o uguale al 20% ( 11 , 86% versus 7 , 1% ) ; in tali pazienti , inoltre , il decremento della clcr ( - 38 , 97% versus - 30% ) risultato statisticamente simile . 
un dato rilevante rappresentato dalla costante tendenza al decremento della funzionalit renale in tutti i pazienti sottoposti ad evar , indipendentemente dal tipo di protesi utilizzata ; come riportato anche in letteratura tale decremento della funzionalit renale appare del tutto simile a quanto si verifica dopo terapia chirurgica convenzionale . 
in caso di trattamento chirurgico , tale decremento secondario ai fenomeni di embolizzazione distale connessi con lintervento , alla possibile insorgenza di ischemia renale post - clampaggio delle arterie renali o in rapporto ai possibili insulti ( dissezione , occlusione ) provocati sulle arterie renali durante lintervento [ 12 ]  . conclusion conclusioni in conclusion , our study shows that the use of grafts with suprarenal fixation has broadened the indications for evar , with no significant increase in complications affecting renal function , renal arteries or renal parenchyma . 
however , we believe that further studies with longer follow - up periods and larger population samples are needed to evaluate the real risk of using suprarenal grafts as regards the development of renal artery steno - occlusive lesions and ischaemic damage to the renal parenchyma . the tendency of renal function to decline in all patients after evar should encourage us to put in place appropriate pretreatment hydration protocols and limit the use of iodinated contrast agents during the procedure and the follow - up by restricting the number of ct angiography examinations and resorting to alternative techniques such as magnetic resonance ( mr ) angiography and contrast - enhanced ultrasonography [ 27 ]  . in conclusione , dai dati del nostro studio emerge che lutilizzo di protesi ad aggancio soprarenale consente di ampliare le indicazioni allevar , in assenza di un incremento significativo di complicanze in termini di alterazioni della funzionalit renale , delle arterie renali e del parenchima renale . 
bolzano , italy , tel . : + 39 - 047 - 1908494 , fax : + 39 - 047 - 1908908 , e - mail : mosavr@yahoo.com received : 23 june 2006 / accepted : 27 july 2006 / published online : 22 february 2007 abstract purpose . 
cta is fast and relatively noninvasive , and its sensitivity appears similar to that of dsa in detecting and evaluating intracranial aneurysms , even those smaller than 3 mm . this study confirms the value of cta as the primary imaging technique in subarachnoid haemorrhage , with dsa reserved for selected patients . key words multislice ct angiography cerebral aneurysm riassunto obiettivo . 
in un periodo di 20 mesi 130 pazienti con diagnosi tc di emorragia subaracnoidea acuta non traumatica sono stati arruolati per uno studio prospettico e sottoposti ad angiotc multistrato ( 16 detettori ) ed angiografia digitale sottrattiva ( 57 maschi , 73 femmine ; et media 59 , 5 anni )  . 
langio - tc una metodica veloce e poco invasiva e la sua sensibilit nellindividuazione degli aneurismi analoga a quella dellangiografia digitale sottrattiva anche se di dimensioni inferiori ai 3 mquesto studio conferma la validit dellangiotc come tecnica di imaging di elezione nella diagnosi di emorragie subaracnoidee . 
langiografia digitale sottrattiva pu essere riservata solo a pazienti selezionati . parole chiave angio - tc multistrato aneurisma cerebrale introduction introduzione nontraumatic subarachnoid haemorrhage ( sah ) is a neurological emergency characterised by extravasation of blood into the spaces lining the central nervous system , which are normally filled with liquor . 
nonaneurysmal sah , including the perimesencephalic end systolic area ( esa ) , is in contrast characterised by a good prognosis and rare neurological complications [ 2 ]  . the global incidence of sah , which varies from region to region , is about 10.5 cases per 100 , 000 inhabitants per year and has remained stable over the last 30 years . 
the main negative prognostic factors include level of consciousness , age and the quantity of blood at initial head computed tomography ( ct ) scan [ 3 , 4 ]  . the principle variable risk factors are cigarette smoking , hypertension , use of cocaine and alcohol abuse . 
first - degree family members of patients with sah have an increased risk ; there are also hereditary diseases of the connective tissue associated with intracranial aneurysms and sah , such as polycystic kidney disease , ehlers - danlos syndrome ( type iv ) , pseudoxanthoma elasticum and fibromuscular dysplasia [ 5 ]  . on the basis of these prognostic criteria , an sah should always be suspected in patients with the typical presentation of sudden and severe headache associated with nausea , vomiting , neck stiffness , photophobia or loss of consciousness . the physical examination may reveal retinal haemorrhage , evidence of meningeal irritation , reduced level of consciousness and / or focal or unilateral neurological deficit . 
this fact supports the extensive use of ct that , if correctly performed , is capable of identifying an sah in 100% of cases within 12 h of symptom onset and in 93% of cases within 24 h [ 7 , 8 ]  . 
head ct is also able to identify the presence of intraparenchymal haematomas , hydrocephalus , cerebral oedema and , in some cases , can suggest the probable site of aneurysmal rupture [ 9 ]  . 
lumbar puncture is a valuable diagnostic examination in cases of negative ct and suspected sah . for exact localisation of the source of extravasated blood , the diagnostic protocol involves performing digital subtractive angiography ( dsa ) or ct angiography ( cta )  . 
whereas dsa is the gold standard for identifying cerebral aneurysms , cta is gaining increasing acceptance , thanks to its immediacy and noninvasiveness and a specificity and sensitivity comparable with dsa . 
cta also has a significant advantage in that it can be performed immediately following the baseline ct examination , which enables a significant shortening of examination times and the possibility of initiating treatment immediately [ 1023 ]  . the aim of this paper is to present a consecutive series of 130 patients diagnosed with sah in a single institution ( ospedale centrale regionale di bolzano ) who underwent cta and / or dsa and to analyse their sensitivity , specificity and diagnostic accuracy , comparing them with the data in the literature . le normalmente percorsi da liquido cerebrospinale . 
lesa non aneurismatica , inclusa lesa perimesencefalica , caratterizzata da buona prognosi e rare complicanze neurologiche [ 2 ]  . lincidenza mondiale aggregata dellesa , che varia da regione a regione , di circa 10 , 5 casi / 100000 abitanti per anno ed rimasta stabile negli ultimi 30 anni . 
i familiari di primo grado di pazienti con esa hanno fattore di rischio aumentato ; vi sono inoltre patologie ereditarie del tessuto connettivo associate ad aneurismi intracranici ed esa quali la malattia policistica renale , la sindrome di ehlers - danlos ( tipo iv ) , lo pseudoxantoma elastico e la displasia fibromuscolare [ 5 ]  . sulla base di tali dati prognostici unesa deve essere sempre sospettata in pazienti con presentazione tipica : cefalea violenta ed improvvisa associata a nausea , vomito , dolore cervicale , fotofobia o perdita di coscienza . 
in assenza dei classici segni e sintomi la diagnosi di esa pu essere confusa con diagnosi di emicrania e cefalea muscolo - tensiva in circa il 50% dei casi [ 6 ]  . 
tali dati supportano luso estensivo che viene fatto della tomografia assiale computerizzata ( tc ) che , se eseguita correttamente , in grado di rivelare unesa nel 100% dei casi entro 12 ore dallesordio sintomatologico e nel 93% entro 24 ore [ 7 , 8 ]  . 
la tc del cranio inoltre in grado di discriminare la presenza di ematomi intraparenchimali , idrocefalo , edema cerebrale e pu , in alcuni casi , suggerire la probabile sede della rottura aneurismatica [ 9 ]  . 
la rachicentesi mantiene una validit diagnostica nel caso di tc negativa e quadro clinico sospetto per esa . il percorso diagnostico prevede quindi , per lesatta localizzazione della sorgente del sanguinamento , lesecuzione di unangiografia digitale sottrattiva ( dsa ) oppure di un angiotc ( atc )  . 
lo studio angiografico cerebrale a sottrazione digitale rappresenta il gold standard per levidenziazione degli aneurismi cerebrali ; latc viene sempre pi utilizzata per limmediatezza e la non invasivit associate a specificit e sensibilit comparabili con la dsa . 
contrast enhancement was provided by the intravenous antecubital administration of an 80ml bolus of nonionic iodinated contrast material ( iomeron 350 mgi / ml , bracco , milan , italy ) at a 4 - ml / s flow rate followed by 50 ml saline solution at the same rate . 
the sample volume was positioned in an internal carotid artery with a threshold of + 30 hu . after acquisition data transfer to the postprocessing station ( leonardo , siemens , erlangen , germany ) , image analysis was performed interactively by the radiologist using various postprocessing techniques , including two ( 2d ) and three - dimensional ( 3d ) multiplanar reconstructions ( mpr ) , maximum intensity projections ( mip ) and volume rendering ( vr )  . each cta and dsa examination was assessed independently by the performing radiologist , and the aneurysms were classified according to the following scheme ( table 1 ) : site : aneurysms originating from the anterior circulation : internal carotid artery , ophthalmic artery , anterior choroidal artery , anterior communicating artery , anterior cerebral artery ( a1 , a2 ) , pericallosal artery , callosal - marginal artery , middle cerebral artery ( m1 , m2 , m3 ) , posterior communicating artery aneurysms originating from the posterior circulation : basilar artery , apex of the basilar artery , posteroinferior cerebellar artery , anteroinferior cerebellar artery , anterosuperior cerebellar artery , posterior cerebral artery . size : giant aneurysms : 25 mm large aneurysms : 1325 mm medium aneurysms : 513 mm small aneurysms : 35 mm very small aneurysms : < 3 mm nel periodo compreso tra giugno 2004 e febbraio 2006 ogni paziente con diagnosi tc di esa non traumatica stato sottoposto a atc ( somatom sensation 16 , siemens , erlangen , germania ) e , successivamente , a dsa ( multistar plus top , siemens , erlangen , germania )  . 
sono stati arruolati 130 pazienti consecutivi , 57 maschi e 73 femmine con et media di 59 , 515 , 2 anni ( range 2091 anni ) ; 91 pazienti provenienti dal pronto soccorso dellospedale centrale regionale di bolzano e 39 da altre strutture ospedaliere . latc stata eseguita con sistema a 16 detettori ( somaton sensation 16 , siemens , erlangen , germania ) con i seguenti parametri di acquisizione e ricostruzione : scansione sul piano assiale estesa dal soma della prima vertebra cervicale al vertice , collimazione 0 , 75 mm , tempo di rotazione 0 , 5 s , fov 230 mm , feed / rot 6 , 5 , 120 kv , 210 mas , ricostruzione in tempo reale 3 mm / 3 mm con fov 120 , ricostruzione per il postprocessing 1 mm / 0 , 5 mm con fov 80 . 
per lopacizzazione arteriosa sono stati somministrati in bolo , per via endovenosa antecubitale , 80 ml di mezzo di contrasto iodato non ionico ( iomeron 350 mgi / ml , bracco , milano , italia ) al flusso di 4 ml / s seguiti da 50 ml di soluzione salina allo stesso flusso . 
in the event of positive cta , only those patients whose cta findings were not complete for the purposes of surgical planning or were to undergo endovascular therapy were required to undergo dsa . 
cta and dsa findings were compared with regard to sensitivity , specificity and diagnostic accuracy . angioarchitettura : presenza o meno di vasi ad origine dalla sacca aneurismatica . tutti i pazienti con atc negativa sono stati sottoposti entro 48 ore a dsa . 
in caso di atc positiva sono stati inviati allo studio angiografico solamente i pazienti con quadro atc non esaustivo ai fini della programmazione chirurgica o quelli indirizzati allapproccio terapeutico endovascolare . infine , quando i reperti atc sono stati giudicati sufficienti per la pianificazione chirurgica , i pazienti sono stati sottoposti allintervento chirurgico senza ulteriori esami diagnostici . 
i dati atc ed angiografici sono stati confrontati in termini di sensibilit , specificit ed accuratezza diagnostica . all cta and dsa examinations were technically assessable . all patients who presented for the cta examination without assisted ventilation were studied without sedation ; about 60% of these required sedation at dsa . 
all cta and dsa procedures were without complications ( allergic reactions , acute renal failure or extravasation at the site of venous injection , more serious neurological complications or complications at the site of arterial catheterisation )  . all 21 patients with a negative cta underwent dsa . 
of the 109 patients with positive cta , 79 underwent emergency dsa to clarify the cta findings and plan therapy , and five underwent dsa during endovascular embolisation on average 13 days after the acute event ( 135.5 days , range 720 days )  . 
in 25 cases , the cta findings were considered complete for surgical purposes , such that these patients unrisultati tutti gli esami atc e dsa eseguiti sono risultati tecnicamente valutabili . 
tutte le procedure eseguite , atc e dsa , sono state esenti da complicazioni ( reazioni allergiche , ira o stravasi in sede di iniezione venosa , complicanze neurologiche maggiori o nella sede di cateterismo arterioso )  . tutti i 21 pazienti con atc negativa sono stati sottoposti a dsa . 
tra i 109 pazienti con atc positiva 79 sono stati sottoposti a dsa urgente per chiarire i reperti atc al fine della pianificazione terapeutica , 5 hanno eseguito lo studio angiografico durante la procedura di embolizzazione endova1325 513 total dimensioni ( mm ) 1325 513 totale results m . 
1 percorso diagnostico dei 130 pazienti arruolati nello studio . derwent dsa post - operatively only . of the 105 patients who underwent dsa , cta findings were confirmed in 104 : in 20 cases where the findings were negative and in 84 cases with the presence of one or more aneurysms . 
in 25 casi il quadro atc stato giudicato esaustivo ai fini dellintervento chirurgico , pertanto questi pazienti sono stati sottoposti a dsa solo come controllo post - operatorio . tra i 105 pazienti sottoposti a dsa il quadro atc stato confermato in 104 : in 20 casi per la negativit del reperto ed in 84 per la presenza di uno o pi aneurismi . 
solo in un caso la dsa ha dimostrato la presenza di un aneurisma del circolo anteriore delle dimensioni di 2 mm non riconosciuto allatc ; lidentificazione di questo piccolo aneurisma stata comunque possibile alla valutazione retrospettiva delle immagini . 
nei 25 pazienti sottoposti al trattamento chirurgico senza la valutazione dsa pre - operatoria stata riscontrata unottima corrispondenza tra le informazioni fornite dallatc ed il quadro chirurgico per quanto riguarda le dimensioni , la morfologia e langioarchitettura . 
2a - i a 41 - year - old woman : axial ( a ) , coronal ( b ) and sagittal ( c ) multiplanar reconstruction ( mpr ) images show a large aneurysm at the bifurcation of the left middle cerebral artery . 
axial ( d ) , coronal ( e ) and sagittal ( f ) maximum intensity projection ( mip ) images obtained with a 10 - mm - thin section more clearly show the aneurysms morphology , its multilobular profiles and relationship with surrounding vessels . 
volume rendering ( vr ) posteroanterior image ( h ) better shows vessels of cranial base and the aneurysvr and transparent vr images ( i ) : this last reconstruction shows a better three - dimensional ( 3d ) image of the aneurysmal sac and surrounding vessels . 
le ricostruzioni mpr assiale ( a ) , coronale ( b ) e sagittale ( c ) dimostrano un aneurisma di grandi dimensioni alla biforcazione dellarteria cerebrale media di sinistra . 
le ricostruzioni mip a strato sottile ( 10 mm ) assiale ( d ) , coronale ( e ) e sagittale ( f ) meglio definiscono la morfologia dellaneurisma , i profili polilobati ed i suoi rapporti con i vasi circostanti . 
3a - i a 51 - year - old woman : coronal ( a ) , axial ( b ) , sagittal ( c ) maximum intensity projection ( mip ) and volume rendering ( vr ) ( d - f ) images show a medium - sized aneurysm at the bifurcation of the right middle cerebral artery ( large arrow ) , a small one at the bifurcation of the left middle cerebral artery ( thin arrow ) and a very small aneurysm of the anterior communicating artery ( arrowhead )  . 
le ricostruzioni mip coronale ( a ) , assiale ( b ) , sagittale ( c ) e vrt ( d - f ) dimostrano un aneurisma di medie dimensioni alla biforcazione dellarteria cerebrale media destra ( freccia grande ) , un aneurisma di piccole dimensioni alla biforcazione dellarteria cerebrale media sinistra ( freccia sottile ) ed un aneurisma molto piccolo allarteria comunicante anteriore ( punta di freccia )  . 
4a - d a 38 - year - old woman : axial ( a ) , coronal ( b ) , sagittal ( c ) maximum intensity projection ( mip ) and volume rendering ( vr ) ( d ) images show a medium - sized aneurysm with a long neck of the right internal carotid artery ( arrow )  . 
ricostruzioni mip assiale ( a ) , coronale ( b ) , sagittale ( c ) e vrt ( d ) di un aneurisma di medie dimensioni dellarteria carotide interna destra con lungo colletto ( freccia )  . 
most aneurysms were of medium sized ( n = 67 ; 50% ) , followed by small ( n = 34 ; 25.4% ) , very small ( n = 16 ; 11.9% ) and large ( n = 16 ; 11.9% ) ( table 1 )  . overall , cta identified 108 of the 109 aneurysms seen at dsa and 25 aneurysms confirmed at surgery . 
6a , b a 60 - year - old man : axial ( a ) and coronal ( b ) maximum intensity projection ( mip ) images show a large , partially thrombosed , aneurysm at the bifurcation of the right middle cerebral artery ( arrow )  . 
7a - d an 81 - year - old man : axial ( a ) , coronal ( b ) paracoronal ( c ) maximum intensity projection ( mip ) and digital subtraction angiography ( dsa ) ( d ) images show a large aneurysm ( arrow ) with a wide neck of the significantly calcified left vertebral artery . 
ricostruzioni mip assiale ( a ) , coronale ( b ) , para - coronale ( c ) e corrispettivo dsa ( d ) di un aneurisma di grandi dimensioni con ampio colletto dellarteria vertebrale sinistra ( freccia ) , estesamente calcifica . 
filiforme larteria vertebrale destra ( b , punta di freccia )  . we also encountered excellent agreement between cta and dsa with regard to assessing the aneurysmal neck and angioarchitecture . 
these data were available for 92 of the 134 aneurysms in our study : we excluded the aneurysm not identified at cta , the 25 aneurysms treated surgically prior to dsa and the 16 aneurysms < 3 mm , the small size of which hindered realistic measurement of the neck . 
in 12 medium and large aneurysms prevalently located in the middle cerebral artery , the presence of a vessel originating directly from the aneurysmal sac was identified . complessivamente con atc sono stati riconosciuti 108 dei 109 aneurismi visualizzati con dsa cui vanno sommati i 25 aneurismi confermati allatto chirurgico . 
pertanto i valori di sensibilit e specificit raggiungono rispettivamente il 98 , 8% ed il 100% , la predittivit positiva del 100% e la predittivit negativa del 95 , 2% , con unaccuratezza diagnostica del 99 , 0% ( tabella 2 )  . abbiamo riscontrato unottima corrispondenza tra atc e dsa anche nella valutazione del colletto aneurismatico e dellangioarchitettura ; tali dati sono disponibili per 92 dei m . 
the technological developments of multidetector ct and especially the introduction and diffusion in clinical practice of 16 - slice scanners have led to improved spatialtemporal resolution , thus enabling an accurate and minimally invasive study of cerebral aneurysms , even in the event of acute sah . the possibility of performing cta immediately following a ct diagnosis of sah , along with the noninvasiveness of the technique , speed of execution and high diagnostic sensitivity and specificity , increasingly promote cta as a highly reliable technique in studying cerebral aneurysms . our prospective study involving 130 patients shows that in all cases , cta was technically feasible and was well tolerated by all patients . 
all examinations could be assessed , and there were no major motion artefacts . however , a limitation to our study was the absence of patients who had previously undergone neurosurgery or endovascular embolisation ; hence , we have no direct experience with artefacts caused by metal clips or coiled springs . 
in this respect , it should be noted that previous studies have demonstrated the validity of cta even in the post - operative follow - up [ 24 ]  . shorter acquisition times and increased spatial resolution are two important advantages introduced by 16 - slice scanners . 
the increased acquisition speed not only enables an exclusively arterial acquisition for the entire scan duration but also reduces the incidence of motion artefacts , which can seriously compromise image quality to the point of rendering the images nondiagnostic . 
this should not be underestimated in this type of patient , who is at times drowsy , at times suffering from psychomotor agitation and often uncooperative 134 aneurismi oggetto del nostro studio : abbiamo escluso laneurisma non riconosciuto con atc , i 25 aneurismi trattati chirurgicamente prima dellesecuzione dellangiografia ed i 16 aneurismi < 3 mm le cui piccole dimensioni non consentivano una reale definizione della base dimpianto . 
le due metodiche sono state concordi nel definire 48 aneurismi con colletto stretto e 44 aneurismi a larga base dimpianto . in 12 aneurismi di medie e grandi dimensioni , prevalentemente localizzati allarteria cerebrale media , stata identificata lemergenza di un vaso direttamente dalla sacca aneurismatica . discussione lo studio degli aneurismi cerebrali stato per lungo tempo affidato alla dsa , metodica invasiva , non priva di rischi per il paziente e caratterizzata da lunghi tempi di esecuzione . gli sviluppi tecnologici della tomografia computerizzata multidetettore ed in particolare lintroduzione e la diffusione nella pratica clinica delle apparecchiature a 16 strati , hanno portato ad un miglioramento della risoluzione spazio - temporale permettendo uno studio accurato e poco invasivo degli aneurismi cerebrali anche in caso di esa in fase acuta . la possibilit di effettuare latc subito dopo la diagnosi tc di esa , la non invasivit e la rapidit di esecuzione associate ad elevate sensibilit e specificit diagnostiche propongono sempre pi latc quale metodica altamente affidabile nello studio degli aneurismi cerebrali . questo studio prospettico relativo a 130 pazienti evidenzia che latc si dimostrata tecnicamente sempre eseguibile e ben tollerata dal paziente ; tutti gli esami sono risultati valutabili , in particolare non si sono registrati grossolani artefatti da movimento . per contro un limite di questo studio lassenza di pazienti gi precedentemente sottoposti ad interventi neurochirurgici o ad embolizzazione endovascolare : non abbiamo quindi esperienza diretta con gli artefatti da clips o spirali metalliche . 
a tale riguardo va aggiunto che precedenti studi hanno dimostrato la validit dellatc anche nei controlli post - operatori [ 24 ]  . la riduzione dei tempi di acquisizione e laumento della risoluzione spaziale sono due importanti vantaggi introdotti dagli apparecchi a 16 strati . 
la maggiore velocit di acquisizione non solo consente di ottenere unacquisizione esclusivamente arteriosa per tutta la durata della scansione , ma riduce lincidenza degli artefatti da movimento che possono inficiare la qualit delle immagini sino a renderle non diagnostiche . 
questo aspetto non va sottovalutato in questa tipologia di paziente : talvolta soporoso , talvolta in stato di agitazione psicomotoria e spesso comunque poco collaborante e poco incline a mantenere limmobilit del capo anche per pochi secondi . 
per nessuno dei pazienti sottoposti ad atc stata necessaria la sedazione , al contrario pi della met dei pazienti sottoposti a dsa ha richiesto lintervento dellanestesista al fine di ottenere immagini diagnostiche , prive di artefatti da movimento . un esame atc viene eseguito in circa 10 minuti cui va m . 
in contrast , a cerebral dsa study requires angiographic experience , and when performed by an expert has a duration of 4560 min , to which is added about 10 min for reporting the findings . the move from 4to 16 - slice devices has further increased spatial resolution . 
various studies performed with 4slice scanners have already demonstrated excellent diagnostic accuracy regarding aneurysms larger than 4 mm while underlining the limitations for smaller aneurysms [ 14 , 17 , 20 , 25 ]  . 
 mpr , which were assessed in cine mode in the three orthogonal planes in space , help confirm the presence of the aneurysm or determine whether it was not identified in the axial plane alone . 
mpr performed in various oblique planes or curved mpr along the vessel course helps define the relations with the surrounding vascular and bone structures and the size of the sac and neck , as well as parietal calcifications and partial thromboses . 
nonetheless , these easy - to - use reconstructions return a plastic , 3d - like image of the main vascular branches for most of their course , which often helps in the recognition of aneurysmal protrusions . 
these reconstructions , which are the most similar to traditional angiographic images , can be applied particularly sommato un tempo medio di elaborazione - lettura delle immagini di circa 1520 minuti : il referto quindi disponibile dopo 2530 minuti dallarrivo del paziente alla tc . 
al contrario lesecuzione di una panangiografia cerebrale richiede esperienza angiografica ed in mani esperte ha una durata media di 4560 minuti cui vanno sommati circa 10 minuti per la refertazione . il passaggio dai 4 ai 16 strati ha incrementato ulteriormente la risoluzione spaziale : questo ha permesso di aumentare le potenzialit diagnostiche dellatc soprattutto nellambito degli aneurismi di dimensioni molto piccole . 
diversi studi , condotti con apparecchi a 4 strati , hanno gi dimostrato lottima accuratezza diagnostica per gli aneurismi di dimensioni superiori ai 4 mm e sottolineato i limiti per quelli di dimensioni pi piccole [ 14 , 17 , 20 , 25 ]  . 
le ricostruzioni mpr secondo vari piani obliqui o mpr curvate lungo il decorso di un vaso aiutano a definire i rapporti con le strutture vasali ed ossee , le dimensioni della sacca e del suo colletto , calcificazioni parietali o trombosi parziali . le ricostruzioni in proiezione di massima intensit ( mip ) proiettano nel piano di ricostruzione solo i voxel pi luminosi del volume scelto : si tratta di ricostruzioni bidimensionali con perdita dellinformazione spaziale . 
tuttavia queste ricostruzioni , di facile applicazione , ci restituiscono unimmagine plastica , simil - 3d , delle principali diramazioni vasali per gran parte del loro decorso che spesso aiuta nel riconoscimento delle protrusioni aneurismatiche . 
le ricostruzioni mip , le pi vicine allimmagine angiografica tradizionale , trovano applicazione soprattutto nella valutazione delle diramazioni arteriose che si allontanano dal poligono di willis mentre non consentono una valutazione corretta delle strutture in stretto rapporto con la base cranica per lelevata attenuazione dellosso . 
it should also be borne in mind that very small aneurysms can be masked by vascular structures if the latter are projected in the same plane as the reconstruction . vr is a 3d reconstruction technique that requires definition of a threshold attenuation value ( measured in hounsfield units ) for selecting reconstruction voxels . 
these images help in interpreting the vascular relations and can be used to help in surgical planning , as they simulate the intraoperative view . postprocessing performed with a reduced fov enables improved spatial resolution . 
reconstructions in the various planes in space enable recognition and therefore sufficiently adequate characterisation of morphology , size , neck and development of an aneurysm as well as its relation to adjacent vessels and surrounding structures . 
the volumetric reconstructions , which are easy to obtain and have a high visual impact , return a plastic image that is often more useful in defining the aneurysms relations and development than in diagnosing it . 
it should also be borne in mind that only thin - section mpr , which are more laborious and less intuitive , enable correct identification of small irregularities of the sacs profile or partial thrombosis , where present . conclusions our study confirms the data in the literature . 
the ability of cta to define the relevant anatomical characteristics for surgical treatment , such as aneurysmal neck morphology , parietal calcification , sac thrombosis and relations with adjacent structures , as well as 3d reconstruction of the neurovascular angioarchitecture means that fundamental additional information can be supplied for deciding the next treatment steps . the results obtained in this study confirm the data in the literature and encourage the use of cta in routine clinical practice , with recourse to dsa only in selected cases or cases with uncertain diagnosis . 
at our institute , this study determined a change in managing patients with acute nontraumatic sah : in the event of positive cta finding for the presence of an aneurysm , in most cases , patients are scheduled for surgery without undergoing a dsa study . given the aetiology of nontraumatic sah and its highlevel of risk in the event of an incorrect diagnosis , fundamental requisites for cta study include correct technical execution and careful and interactive image assessment : where there is doubt , patients should undergo dsa . 
with regard to the future , cta is also a promising technique for follow - up to verify exclusion of the aneurysmal sac after endovascular or surgical procedures . essere mascherati dalle strutture vascolari se queste si proiettano nello stesso piano di ricostruzione . lelaborazione volume rendering technique ( vrt ) una tecnica di ricostruzione tridimensionale che richiede la definizione di un valore soglia di attenuazione ( in unit hounsfield ) per la selezione dei voxel di ricostruzione . 
queste immagini facilitano linterpretazione dei rapporti vascolari e possono essere di aiuto nella pianificazione dellapproccio chirurgico , simulando la visione intraoperatoria . le rielaborazioni con field of view ( fov ) ridotto consentono una migliore risoluzione spaziale : le ricostruzioni secondo i vari piani dello spazio permettono di riconoscere e quindi di caratterizzare in maniera adeguata morfologia , dimensioni , base dimpianto e sviluppo di un aneurisma oltre ai suoi rapporti con i vasi adiacenti e le strutture circostanti . 
le ricostruzioni volumetriche ( vrt ) facili da ottenere e di sicuro impatto visivo , restituiscono unimmagine plastica spesso pi utile nella definizione dei rapporti e dello sviluppo dellaneurisma che non nella sua diagnosi ; sono spesso richieste dai neurochirurghi perch meglio rispecchiano la spazialit e la visualizzazione intraoperatoria . 
non va dimenticato tuttavia che solo le ricostruzioni multiplanari sottili , pi laboriose e meno intuitive , ci consentono di identificare correttamente eventuali piccole irregolarit dei profili della sacca o la sua parziale trombosi . conclusioni questo studio conferma i dati della letteratura : latc una metodica poco invasiva , rapida , altamente sensibile e specifica nella diagnosi di aneurismi cerebrali nelle esa . 
la capacit dellatc di definire caratteristiche anatomiche rilevanti per il trattamento chirurgico quali la morfologia del colletto aneurismatico , le calcificazioni parietali , la trombosi della sacca ed i rapporti con le strutture adiacenti e la ricostruzione tridimensionale dellangioarchitettura neurovascolare consentono di fornire informazioni aggiuntive fondamentali per decidere il successivo trattamento dei pazienti . 
nella nostra realt questo studio ha determinato un cambiamento nella gestione del paziente con esa acuta non traumatica : in caso di reperto angio - tc positivo per la presenza di un aneurisma la maggior parte dei pazienti viene portata allintervento chirurgico senza lesecuzione della dsa . considerando leziologia dellesa non traumatica e la sua pericolosit in caso di errata diagnosi , uno studio atc non pu prescindere da unesecuzione tecnicamente corretta e da una valutazione attenta ed interattiva delle immagini : nei casi dubbi il ricorso alla dsa rappresenta tuttora lopzione di scelta . 
passariello1 1dipartimento di scienze radiologiche , universit degli studi di roma la sapienza , policlinico umberto i , v.le regina elena 324 , i - 00161 roma , italy 2servizio di fisica radiologica , dipartimento di scienze radiologiche , universit degli studi di roma la sapienza , roma , italy correspondence to : m . 
we present our initial clinical experience with a recently introduced 64 - detector computed tomography ( 64 - mdct ) scanner that makes use of a periodic motion of the focal spot in the longitudinal direction ( z - flying focal spot ) , which enables it to reach a final spatial resolution of 0.40.40.4 mm3 and a temporal resolution of 83 ms . 
a total of 114 patients ( 108 men , six women ; age range 3677 years , mean 63.1 years ) underwent retrospective electrocardiogram ( ecg ) - gated examination of the coronary arteries using a 64 - mdct scanner ( somatom sensation 64 , siemens medical solutions , germany )  . 
acquisition parameters were the following : collimation 640.6 mm , 800 quality reference milliampere second ( mas ) , 120 kvp , 0.33 - s gantry rotation time and pitch 0.2. 
administration of 80 ml of contrast agent ( iomeron 400 mgi / dl , bracco , italy ) + 30 ml of saline at 4 / s and delay time determined using a bolus triggering technique . 
oral betablockers were administered to patients with heart rate ( hr ) > 75 bpto reduce radiation exposure , an automatic exposure control system was applied in all cases to adapt tube current to patient size and anatomic shape ( care dose 4d , siemens medical solutions , germany )  . 
the optimal temporal window for raw data reconstruction was chosen from an initial preview of images reconstructed with different phase settings ( range 0%95% rr interval with 5% gap ) at a selected anatomical level in the mid part of the right coronary artery . 
in patients with hr < 60 bmp , the best reconstruction intervals were identified in the end - systolic ( 30%35% of the rr interval ) and end - diastolic ( 60%65% of the rr interval ) phases ; with faster hr ( > 80 bmp ) , high image quality was observed in end - systole ( 30%35% of the rr interval )  . 
nel presente lavoro introduciamo la nostra esperienza preliminare e lottimizzazione del protocollo di acquisizione di un apparecchio tcms in grado di acquisire 64 strati per rotazione ( tcms - 64 ) grazie allutilizzo di un movimento periodico della macchia focale lungo lasse longitudinale z che consente di raggiungere una risoluzione spaziale di 0 , 40 , 40 , 4 mm3 e temporale di 83 ms . 
114 pazienti ( 108 maschi e 6 femmine , intervallo di et 3677 anni , media 63 , 1 ) sono stati sottoposti ad esame con tcms delle arterie coronarie utilizzando uno scanner tcms - 64 ( somatom sensation 64 , siemens medical solutions , germania )  . 
i parametri di acquisizione sono stati i seguenti : collimazione 640 , 6 mm , 800 quality reference mas , 120 kvp , tempo di rotazione 0 , 33 s e pitch 0 , 2 . 
in tutti i pazienti le immagini sono state acquisite dopo somministrazione ev di 80 ml di mdc ( iomeron 400 mgi / dl , bracco , italia ) + 30 ml di soluzione fisiologica con ritardo di scansione calcolato con tecnica bolus triggering . 
in tutti i casi stato utilizzato un sistema di limitazione automatica della dose ( care dose 4d , siemens medical solutions , forchheim , germania ) in grado di modulare la corrente emessa del tubo in relazione ai valori di attenuazione della regione che si sta studiando . 
la finestra temporale ottimale per la ricostruzione dei dati grezzi stata scelta da uniniziale preview di immagini ricostruite in differenti fasi del ciclo cardiaco ( tra 0%95% dellintervallo r - r ogni 5% ) rilevato ad un livello anatomico predefinito nel tratto medio dellarteria coronaria di destra . 
durante lacquisizione tcms stata registrata una fc media di 65 , 619 , 2 bpm ( intervallo : 4496 bpm ) con bradicardizzazione effettuata in 16 / 114 pazienti ( 14 , 0% )  . 
the 64 - mdct scanner diagnostic performance for coronary ct angiography is further improved with better spatial and temporal resolution and faster scan times ; besides , initial clinical results are promising . 
nei pazienti con fc < 60 bpm , la migliore finestra temporale nella quale effettuare la ricostruzione delle immagini stata individuata rispettivamente nelle fasi telesistolica ( 35% dellintervallo r - r ) e meso - telediastolica ( 65%70% dellintervallo r - r ) ; nei casi con fc di base elevata ( > 80 bpm ) , la migliore fase per la ricostruzione delle immagini risultata la telesistole ( 35% dellintervallo r - r )  . 
il ctdi volumetrico ( ct dose index volume ) risultato in media di 36 , 538 , 30 mgy per paziente con un range compreso tra 27 , 2 e 61 , 9 mgy corrispondenti ad un eff mas . 
se confrontato con unacquisizione effettuata a amperaggio costante , lutilizzo del sistema di limitazione automatica della dose ha consentito una riduzione media del ctdi volumetrico del 33 , 3% per paziente ( p < 0 , 001 )  . 
la nostra esperienza clinica iniziale ha evidenziato come lultima generazione di tomografi tcms - 64 apra nuovi scenari per la gestione clinica del paziente coronaropatico . lutilizzo di sistemi idonei di modulazione automatica dellintensit di corrente del tubo radiogeno appare tuttavia indispensabile per limitare la dose di esposizione del paziente che rappresenta , allo stato attuale , il limite principale allutilizzo clinico della metodica . parole chiave arterie coronarie tc multidetettore coronaropatia infarto miocardico dose di esposizione in tc introduction introduzione since the introduction of multidetector computed tomography ( mdct ) into clinical practice in 1998 , diagnostic imaging of the heart and coronary arteries has been one of the main fields of interest for this technique [ 1 , 2 ]  . 
despite the major epidemiological , health and economic implications of ischaemic heart disease [ 3 ] , the study of the coronary tree using noninvasive techniques was for years a difficult problem to solve due to intrinsic technical limitations . 
the coronary artery circulatory is , in fact , a difficult vascular district to assess using the various imaging techniques available due not only to the small diameter and tortuous course of the arteries but also to the complex cardiorespiratory movements . the high spatial and temporal resolution obtainable with the most recent 16 - , 32 - , 40and 64 - detector mdct devices , coupled with the possibility of achieving adequate cardiac synchronisation , has enabled these limitations to be overcome , at least in part , thus revolutionising the management of patients with heart disease [ 7 , 8 ]  . 
the numerous clinical studies published in recent years have demonstrated the high level of diagnostic accuracy of mdct with regard to both assessment of coronary artery stenosis and follow - up of coronary artery bypass graft patency [ 916 ]  . the volume acquired for studying coronary arteries can be used for performing functional studies on volumes , calculating the ejection fraction and myocardial mass of both ventricles , and assessing regional motion and identifying the presfin dalla sua introduzione in ambito clinico nel 1998 , la diagnostica per immagini del cuore e delle arterie coronarie ha rappresentato uno dei campi di maggior interesse della tc multistrato ( tcms ) [ 1 , 2 ]  . 
malgrado le rilevanti implicazioni epidemiologiche ed economico - sanitarie della cardiopatia ischemica [ 3 ] , lo studio dellalbero coronarico con metodiche di tipo non invasivo stato per molti decenni un problema di difficile soluzione per limiti tecnici intrinseci , rimanendo dominio quasi esclusivo della coronarografia selettiva , procedura gravata da una non trascurabile mortalit e morbilit [ 46 ]  . 
il circolo arterioso coronarico rappresenta infatti un distretto vascolare di difficile valutazione per le diverse metodiche di imaging sia per il piccolo calibro ed il decorso tortuoso delle sue arterie , che per la complessit dei movimenti cardio - respiratori . lelevata risoluzione spaziale e temporale ottenibile soprattutto con i pi recenti apparecchi tcms a 16 , 32 , 40 e 64 canali e la possibilit di ottenere unadeguata cardiosincronizzazione ha consentito di superare almeno in parte tali limitazioni , dando luogo ad una rivoluzione nella gestione del paziente coronaropatico [ 7 , 8 ]  . 
i numerosi studi clinici pubblicati in questi ultimi anni hanno ormai ampiamente dimostrato come la tcms rappresenti una metodica dalla elevata accuratezza diagnostica sia per quanto riguarda la valutazione delle stenosi coronariche che il follow - up della perviet dei by - pass aorto - coronarici [ 916 ]  . il volume acquisito per studiare le arterie coronarie pu anche essere utilizzato per effettuare studi funzionali sui volumi , per calcolare la frazione di eiezione e la massa miom . 
nonetheless , clinical use of coronary artery mdct is currently hindered by several limitations [ 20 ] : imaging of coronary stents that due to their metallic struts generate beam - hardening artefacts and hinder accurate assessment of the state of the intrastent vascular lumen [ 21 , imaging of extensively calcified coronary arteries , also due to beam - hardening artefacts [ 23 ] elevated patient heart rate ( hr ) ( > 65 bmp ) , which causes progressive shortening of the electrocardiogram ( ecg ) rr interval and a consequent shortening of the end - diastolic phase in which image acquisition occurs , thus leading to motion artefacts [ 24 , 25 ] rhythm disturbances , which render cardiac synchronisation impossible [ 25 ] accuracy in assessing regional motion caused by the relatively low temporal resolution of mdct , especially when compared with other techniques such as magnetic resonance imaging ( mri ) and , above all , ecg [ 17 ]  . clearly then , most limitations of mdct depend on the resolution limitations of the technique , and therefore , as achenbach emphasised in 2004 , the key to obtaining increasingly accurate diagnostic imaging lies in increasing both spatial and temporal resolutions [ 26 ]  . in this context , we present our early clinical experience with the latest - generation 64 - mdct device in noninvasive coronary artery imaging . 
development of this latest generation of mdct in fact leads to a potential increase in radiation exposure , which could limit the clinical use of 64 - mdct , especially if proposed as a potential screening tool . materials and methods study population between january and may 2005 , 114 patients ( 108 men and six women ; age range 3677 years , mean 63.1 years ) underwent mdct angiography of the coronary arteries . 
all examinations were performed using a 64 - mdct device with a 0.33 - s gantry rotation time ( somatom sensation 64 , siemens medical solutions , forchheim , germany ) and images acquired with retrospective ecg gating . 
clinical indications for the examination were the following : typical ( n = 16 ) or atypical ( n = 7 ) chest pain in patients with a clinical indication for coronarography follow - up at 69 months of the patency of treated coronary stents ( n = 37 for a total of 63 stents )  . 
the findings of the comparison of the two techniques will therefore not be presented here , as this falls beyond the scope of the present study . follow - up of patency of aortocoronary bypass grafts ( n = 40 for a total of 48 bypasses : 32 venous grafts and 16 arterial grafts ) cardica di entrambi i ventricoli , per valutare la cinesi regionale e per identificare la presenza di aree di miocardio infartuato o non - riperfuso correlando lo stato di un vaso coronarico con quello del suo territorio di pertinenza vascolare [ 1719 ]  . 
allo stato attuale , limpiego clinico della tcms delle arterie coronarie presenta tuttavia alcune rilevanti limitazioni [ 20 ] : imaging degli stent coronarici , che a causa della loro trama metallica generano artefatti da indurimento del fascio che impediscono di valutare in modo accurato lo stato del lume vascolare intra - stent [ 21 , 22 ] ; imaging delle coronarie estesamente calcifiche , sempre per linsorgenza di artefatti da indurimento del fascio [ 23 ] ; frequenza cardiaca ( fc ) elevata del paziente ( > 65 battiti per minuto bpm ) , che determina un progressivo accorciamento dellintervallo r - r elettrocardiografico ( ecg ) e conseguentemente della durata della fase telediastolica in cui avviene lacquisizione delle immagini determinando linsorgenza di artefatti da movimento [ 24 , 25 ] ; turbe del ritmo , con impossibilit di ottenere una adeguata cardiosincronizzazione [ 25 ] ; accuratezza nella valutazione della cinesi regionale determinata dalla relativamente bassa risoluzione temporale della tcms soprattutto se confrontata con altre metodiche di riferimento quali la risonanza magnetica e soprattutto lecocardiografia [ 17 ]  . appare quindi evidente come la gran parte delle attuali limitazioni della tcms dipenda da limiti di risoluzione della metodica e pertanto , come sottolineato da achenbach nel 2004 , la chiave per ottenere prestazioni diagnostiche sempre pi accurate lincremento della risoluzione sia spaziale che temporale [ 26 ]  . in questa ottica , nel presente lavoro introduciamo la nostra esperienza clinica preliminare con apparecchiatura tcms di ultima generazione a 64 strati nellimaging non - invasivo delle arterie coronarie , analizzando anche la problematica dosimetrica . 
lo sviluppo di questa nuova generazione di tcms comporta , infatti , un potenziale incremento della dose di esposizione del paziente che rappresenta un possibile fattore limitante limpiego clinico della tcms - 64 soprattutto se si vuole proporre la metodica come potenziale strumento di screening . materiali e metodi popolazione di studio nel periodo compreso tra gennaio e maggio 2005 , 114 pazienti [ 108 maschi , 6 femmine , et compresa tra 3677 anni ( aa ) media 63 , 1 aa ] sono stati sottoposti ad unangiografia con tcms delle arterie coronarie . 
tutti gli esami sono stati effettuati utilizzando unapparecchiatura di tcms - 64 dotata di velocit di rotazione del sistema tubo radiogeno - detettori di 0 , 33 secondi ( somatom sensation 64 , siemens medical solutions , forchheim , germania ) ed acquisendo i dati con gating elettrocardiografico ( ecg ) di tipo retrospettivo . 
therefore , to obtain high - quality images , the hr was empirically slowed in all patients who at the time of the examination had a basal hr > 75 bmp . 
this was achieved using the following drug regimen : oral administration of 40 mg of beta - blockers 6090 min before the examination ( chlorhydrate , propranolol , inderal , astrazeneca ) , and monitoring arterial blood pressure and pulse rate . image acquisition protocol and automatic exposure control system for the examination , the patient was asked to lie supine on the ct table with arms behind the head . 
three electrodes were placed on the chest ( the first on right emithorax , the second 1 cm under the clavicle and the third on the left flank ) to monitor the patients ecg and obtain a tracing with a lead similar to l1 in which the p wave , the qrs complex and the t wave could be distinguished . 
in all cases , the examination was performed following iv administration of nonionic iodinated contrast material and covering a volume from the tracheal carina to the cardiac base ; for the study of coronary bypass grafts , acquisition was extended to include a volume comprising the proximal anastomosis and the cardiac base . 64 - mdct sensation 64 scanner utilizes an automatic exposure control system [ combined applications to reduce exposure ( care ) dose 4d , siemens medical solutions , forchheim , germany ] that combines both angular ( x - y axis or angular modulation system ) and z - axis ( or z - axis modulation system ) tube current modulation [ 2731 ]  . in practice , beginning with the initial topogram as a reference , the amperage is automatically modulated along the entire acquisition volume on the basis of the angular attenuation coefficient ( mean density of a tissue with respect to the tube rotation angle in the x - y axis ) of the anatomical region being studied and on the basis of the attenuation values of the different tissues along the z - axis , with data detected on the basis of the previous slice ( on - line modulation )  . 
for example , in a total - body study , lower amperages are used for rizzare , in pazienti con indicazione clinica alla coronarografia ; controllo a distanza di 69 mesi della perviet di stent coronarici medicati ( n = 37 per un totale di 63 stent )  . 
non verranno quindi riportati di seguito i risultati sul confronto tra le due metodiche poich non rappresenta lobiettivo specifico del presente lavoro ; controllo a distanza della perviet di by - pass aorto - coronarici ( n = 40 per un totale di 48 by - pass ; 32 graft venosi e 16 arteriosi ) ; pazienti sottoposti a scintigrafia miocardica perfusionale a riposo e dopo sforzo con risultati diagnostici non conclusivi ( n = 3 ) ; pazienti sottoposti ad esame ecocardiografico a riposo e dopo stress farmacologico con dobutamina con risultati diagnostici non conclusivi ( n = 11 )  . tutti i pazienti hanno firmato un consenso informato in cui veniva chiaramente spiegato il tipo di procedura a cui si sottoponevano ed i potenziali rischi . 
i criteri di esclusione per lo studio sono stati i seguenti : nota ipersensibilit ai mezzi di contrasto ( mdc ) iodati ; insufficienza renale ( creatininemia > 2 mg / dl ) ; insufficienza cardiaca conclamata ; aritmie cardiache maggiori ; insufficienza respiratoria ; asma bronchiale nei pazienti con indicazione al pre - trattamento con farmaci beta - bloccanti ( controindicazione assoluta alla somministrazione di beta - bloccanti )  . preparazione del paziente lelevata frequenza cardiaca rappresenta uno dei principali fattori in grado di influenzare negativamente la qualit diagnostica dellesame determinando un accorciamento dellintervallo r - r elettrocardiografico con insorgenza di artefatti da movimento [ 24 , 25 ]  . 
per tale motivo , al fine di ottenere massima qualit delle immagini nella nostra esperienza iniziale la bradicardizzazione stata effettuata empiricamente in tutti i pazienti che , al momento di effettuare lesame , presentavano fc basale > 75 bpm , utilizzando il seguente schema di preparazione farmacologica : somministrazione per os di 40 milligrammi ( mg ) di farmaco - bloccante 6090 minuti prima dellesame ( propranolo cloridrato , inderal , astrazeneca ) , monitorando pressione arteriosa ( pa ) e polso ( fc )  . protocollo di acquisizione delle immagini e sistema di limitazione automatica della dose al momento dellesame il paziente stato invitato a sdraiarsi in posizione supina sul lettino della tc con le braccia dietro la testa . 
posizionando tre elettrodi sul torace ( rispettivamente a livello dellemitorace destro e sinistro , un cm al di sotto della clavicola ed in corrispondenza del fianco sinistro ) stato possibile monitorare lecg del paziente , fino ad m . 
based on the initial topogram in the anteroposterior ( ap ) and lateral position ( a ) , care dose 4d automatically modulates tube current during each tube rotation according to the patients angular attenuation profile . 
1a , b sistema di modulazione automatica della dose : partendo dal topogramma iniziale ( a ) , lamperaggio viene modulato automaticamente lungo tutto il volume di acquisizione in base al coefficiente angolare di attenuazione della regione anatomica che si sta studiando . 
in tutti i casi lesame stato eseguito dopo somministrazione endovenosa ( ev ) di mdc iodato non ionico coprendo un volume cranio - caudale compreso tra la carena tracheale e la base cardiaca ; per lo studio dei bypass coronarici lacquisizione stata estesa in modo da includere un volume compreso tra lanastomosi prossimale e la base cardiaca . lo scanner di tcms - 64 utilizza un sistema di limitazione automatica della dose ( combined applications to reduce exposure , care dose 4d , siemens medical solutions , forchheim , germania ) in grado di combinare la modulazione della corrente emessa dal tubo radiogeno sia in relazione al valori di attenuazione angolare ( xy - axis o angular modulation system ) della regione in esame che attraverso un sistema di modulazione della dose lungo lasse z ( o z - axis modulation system ) [ 2731 ]  . in pratica , partendo come riferimento dal topogramma inim . 
contrast material was administered using a dual - head automatic injector ( medrad stellant dual ; medrad , palo alto , pa , usa ) in which the two syringes containing contrast material and saline solution , respectively , were connected by a y - shaped connector equipped with a one - way valve to prevent reflux . 
use of saline solution reduces the total volume of contrast material administered to the patient , thus compressing the iodine bolus and at the same time reducing the presence of beam - hardening artefacts at the level of the superior vena cava [ 32 ]  . acquisition delay was chosen using the bolus triggering technique , which involves positioning a region of interest ( roi ) in correspondence with the aortic arch and monitoring passage of the contrast material bolus with a series of low - dose dynamic scans ( 120 kvp , 30 mas ) with 1 - s intervals [ 33 ]  . 
in this way , the effective ctdi volume could be measured prior to the examination , even in conditions of constant tube - current intensity throughout the acquisition ( without the use of care dose 4d )  . an estimate of the dose absorbed [ expressed in milligray ( mgy ) ] was then made using the care dose 4d system , and this estimate was compared with the dose to which the patient would have otherwise been exposed without the use of current modulation . 
tuttavia il sistema di mudulazione della dose utilizzato in modalit cardiosincronizzata effettua una semplice riduzione del milliamperaggio in base ai valori di attenuazione individuale del paziente . i parametri tecnici utilizzati sono stati i seguenti : collimazione 3220 , 6 mm ; spessore strato 0 , 75 mm ; incremento 0 , 4 mm ; tempo di rotazione del sistema tubo radiogeno / detettori 0 , 33 s ; pitch 0 , 2 ; quality reference mas : 800 ; effective mas : variabile in relazione alle caratteristiche individuali del paziente ; 120 kvp ; filtri di convoluzione per la ricostruzione delle immagini : b20f ( tessuti molli ) e b46f ( utilizzato per la valutazione degli stent coronarici )  . somministrazione del mezzo di contrasto in tutti i pazienti stato utilizzato un mdc ad alta concentrazione di iodio ( 400 mgi / 100 ml , iomeron 400 , bracco , milano , italia ) seguito da un bolo di soluzione fisiologica . 
il mdc stato somministrato utilizzando un iniettore automatico a doppia testata ( medrad stellant dual , medrad , palo alto pa , usa ) in cui le due siringhe contenenti rispettivamente mdc e soluzione fisiologica sono state collegate tra loro tramite raccordino a y dotato di valvola unidirezionale per impedire il reflusso . 
lutilizzo della soluzione fisiologica consente di ridurre il volume totale di mdc somministrato al paziente , compattando il bolo di iodio e riducendo contemporaneamente la presenza di artefatti da indurimento del fascio a livello della vena cava superiore [ 32 ]  . per la scelta del ritardo di acquisizione stata utilizzata la tecnica del bolus triggering posizionando una regione di interesse in corrispondenza dellarco aortico e monitorizm . 
transverse images of 20 different cardiac cycle phases ( 0%95% of rr interval with 5% gap ) obtained at a predefined anatomical level in the middle part of the right coronary artery ( a )  . 
in this patient with a heart rate of 58 bmp , best image quality with minimal motion artefacts is observed in the end - systolic phase ( 20%25% of rr ) and the midto enddiastolic phase ( 70% of the rr )  . 
maximum intensity projection ( mip ) image obtained in the same patient , reconstructing images at 65% of the rr interval , allows the presence of disease throughout the course of the right coronary artery to be excluded ( b )  . 
2a , b esempio di preview series per la selezione della migliore finestra temporale ( percentuale intervallo r - r ) delle immagini utilizzando gating cardiaco di tipo retrospettivo . immagini assiali delle 20 successive serie di ricostruzioni ( dal 0% al 95% dellintervallo rr con gap del 5% ) , ottenute sulla medesima scansione , a livello del terzo medio della cdx ( a ) ; in questo paziente , con fc di 58 bpm , la minor presenza di artefatti da movimento si osserva nelle immagini ricostruite al 20%25% ( intervallo che corrisponde alla telesistole ) e tra il 60% ed il 70% dellintervallo r - r ( fase meso - telediastolica )  . 
this tends to improve temporal resolution by using the raw data derived from multiple cardiac cycles ( up to a maximum of three cycles ) to reconstruct the images [ 35 ]  . zando il passaggio del bolo di mdc attraverso una serie di scansioni dinamiche a bassa dose ( 120 kvp 30 mas ) con intervalli di 1 secondo [ 33 ]  . 
la soglia predefinita per linizio della scansione stata di 100 unit hounsfield ( hu ) con intervallo di tempo tra raggiungimento del valore soglia ed inizio dellacquisizione stessa di 7 secondi . la somministrazione del mdc stata effettuata con protocollo di tipo monofasico utilizzando i seguenti parametri [ 34 ] : 80 ml di mdc + 30 ml di fisiologica con flusso di 4 ml / s con durata totale della somministrazione di 27 , 5 secondi . image postprocessing valutazione dose di esposizione after identifying the best reconstruction interval , the images were processed using a dedicated workstation connected to tutti i pazienti sono stati studiati con utilizzo del software care dose 4d . 
volume rendering algorithms , in contrast , were used mainly in patients being studied for evaluation of aortocoronary bypasses and in all cases where the intuitive 3d approach of this algorithm enabled concise and easily recognisable representation of the state and site of coronary disease . 
this approach provides the patient with images that are easier to understand . given the large number of images obtained on average for each examination ( around 2 , 000 ) , in all cases , images were digitally stored on a compact disc equipped with software for viewing the images in dicom3 format ( digital imaging communication in medicine )  . 
all data from the mdct examination ( except the raw data ) were then archived using the picture archive and communication system ( pacs ) ( lifeweb image manager , veania imaging technologies , italy )  . results the mdct examination was carried out without complications in all patients . 
hr was slowed down in 16 / 114 patients ( 14.0% ) ; there were no cases of complications or side effects as a result of administration of oral - blockers . 
in one patient with severe chronic obstructive pulmonary disease ( copd ) and a baseline hr of 96 bmp , even though the hr could not be slowed due to contraindications for - blockers , the examination was performed nonetheless for clinical requirements . the optimal interval for image reconstruction varied in relation to patients hr during data acquisition . 
they cordi riferimento del ctdi volumetrico ( ct dose index volume ) quale parametro della dose assorbita durante lacquisizione delle immagini con gating ecg di tipo retrospettivo . il valore di ctdi viene definito automaticamente dallo scanner sulla base del topogramma in relazione alla intensit di corrente applicata durante lacquisizione . 
in tal modo , preliminarmente allesame , stato possibile registrare leffettivo valore di ctdi volumetrico anche in condizioni di costante intensit di corrente del tubo durante lintera acquisizione ( senza utilizzo del care dose 4d )  . stata quindi effettuata una stima della dose assorbita ( espressa in mgy ) utilizzando il sistema care dose 4d confrontandola con la dose a cui sarebbe stato sottoposto il paziente senza lutilizzo della tecnica di modulazione . 
in alternativa le immagini sono state ricostruite con unaltra consolle dedicata ( vitrea 2 , vital images inc , minnesota , usa )  . per standardizzare la ricostruzione 3d dei dati e fornire al medico di riferimento delle immagini il pi possibile comprensibili stato da noi utilizzato uno schema in cui sono state effettuate per ciascun paziente almeno 6 set di ricostruzioni : m . 
tale approccio consente di sfruttare al meglio lelevata risoluzione spaziale della metodica ottenendo unimmagine a spessore estremamente sottile ( 0 , 6 mm ) lungo tutto il decorso del vaso . 
gli algoritmi in volume rendering sono stati invece utilizzati prevalentemente nei pazienti inviati per studio dei by - pass aorto - coronarici e in tutti quei casi in cui lintuitivo approccio 3d di questo tipo di algoritmo ha consentito di ottenere una rappresentazione sintetica e facilmente intuibile di stato e sede della coronaropatia fornendo al paziente immagini di pi semplice comprensione . considerando il grande numero di immagini ottenute in media per ciascun esame ( circa 2000 ) , in tutti i casi stata fornita una documentazione di tipo digitale con compact disc ( cd ) su cui stato installato un software per la lettura delle immagini in formato dicom3 ( digital imaging communication in medicine )  . 
tutti i dati dellesame tcms ( esclusi i dati grezzi ) sono stati poi archiviati tramite sistema pacs ( lifeweb image manager , ferrania imaging technologies , italia )  . risultati lesame tcms stato effettuato senza alcuna complicanza in tutti i pazienti studiati . 
la bradicardizzazione stata effettuata in 16 / 114 pazienti ( 14 , 0% ) ; in nessun caso si sono avute complicanze o effetti collaterali conseguenti alla somministrazione di - bloccanti orali . 
in un paziente con bpco severa e fc basale di 96 bpm , pur non essendo stata effettuata la bradicardizzazione per la presenza di controindicazione clinica alla somministrazione di farmaco - bloccante lesame stato ugualmente eseguito per esigenze cliniche . lintervallo ottimale per la ricostruzione delle immagini variato in relazione alla fc del paziente durante lacquisizione dei dati . 
3a , b a 64 - mdct angiography performed at 6 - months follow - up after drug - eluting coronary stent implantation on the left anterior descending ( lad ) artery . 
a curved multiplanar reformation shows the presence of a metallic stent with the characteristic railway track ( arrowheads ) appearance located in the proximal part of the vessel ; the presence of contrast within and distally to the stent indirectly indicates patency ( arrows )  . 
b three - dimensional volume rendering reconstruction ; the use of dedicated cardiac software enables visualisation of the stented coronary vessel ( arrow ) along an automatically generated centreline displayed in the transverse and longitudinal axes of lad . 
a la ricostruzione multiplanare curva ( cpr ) , generata lungo lasse longitudinale dellarteria discendente anteriore , dimostra la presenza di flusso allinterno ed a valle dello stent ( frecce ) , che presenta peraltro tipico aspetto a binario ( punte di freccia )  . 
b immagine tridimensionale ottenuta con tecnica volume rendering ; utilizzando un software dedicato di campionatura selettiva del vaso in esame , possibile riprodurre , in modo pratico e veloce , il tratto di arteria selezionata ( freccia ) permettendo una visualizzazione del lume vascolare intra - stent con tecnica cpr ; in tal modo si ottiene una rappresentazione dellarteria sia secondo il suo asse trasversale che longitudinale . 
in cases with higher baseline hr ( > 80 bmp ) , the best phase for image reconstruction proved to be the end - systolic phase ( 35% rr )  . 
in patients with intermediate hr ( 60 bmp ) , no ideal reconstruction window was identified , and the rr interval used varied significantly from patient to patient . in 11 patients ( 9.6% ) , the reconstructed images were affected by artefacts due to either extrasystole during data acquisition ( n = 8 ) or inability to maintain breath - hold for the duration of the acquisition ( n = 3 )  . 
the study of only the coronary district produced the following values : ctdi volume per la ricostruzione dei dati grezzi corrispondenti alle fasi telesistolica ( 35% r - r ) e meso - telediastolica ( 65%70% rr )  . 
nei casi con fc di base elevata ( > 80 bpm ) , la migliore fase per la ricostruzione delle immagini risultata la telesistole ( 35% dellintervallo r - r )  . 
sulla base delle informazioni fornite dallesame , la paziente stata esclusa dal trattamento e dimessa evitando ulteriore accertamento diagnostico con esame coronarografico e prolungamento della ospedalizzazione . infine , nel gruppo di pazienti in cui lindicazione clinica allesame tcms - 64 era stata posta sulla base di test funzionali ecocardiografici ( n = 11 ) o scintigrafici ( n = 3 ) non conclusivi , in 6 / 14 casi sono state evidenziate immagini tcms64 compatibili con stenosi coronariche emodinamicamente significative ( mono o multivasali ) e clinicamente silenti ( fig . 7 ) ; solamente in questi 6 pazienti stato successivamente effettuato lesame coronarografico convenzionale . aspetti dosimetrici il ctdi volumetrico ( ct dose index volume ) stato in media di 36 , 538 , 30 mgy per paziente con un range compreso m . 
volume rendering reconstruction shows complete occlusion of the stent positioned in the proximal part of the vessel ( short arrow ) , with compensatory enlargement of the first diagonal branch ( long arrow ) ( a )  . thanks to the high spatial resolution achievable using a collimation of 0.6 mm , the stents metallic structure is visualised in detail ( b )  . 
4a - d coronarografia con tcms - 64 per follow - up di stent posizionato su arteria discendente anteriore 3 anni prima ; elaborazione delle immagini effettuata con workstation siemens utilizzando software syngo inspace 4d . 
le immagini ricostruite con algoritmo in volume rendering mostrano occlusione dello stent posizionato nel tratto prossimale della da ( freccia corta ) e lipertrofia compensatoria del primo ramo diagonale , che appare tortuoso ed aumentato di calibro ( freccia lunga ) ( a )  . 
nel particolare ( ingrandito ) lelevata risoluzione spaziale dellacquisizione a 0 , 6 mm di collimazione , permette di ottenere dettagli fini come la chiara definizione della trama metallica dello stent ( b )  . 
i pazienti sottoposti a studio dei by - pass coronarici , a causa del pi ampio volume cranio - caudale acquisito , presentavano valori medi di ctdi volumetrico pi elevati ( 38 , 77 , 9 mgy ) con un milliamperaggio effettivo di circa 645 , 389 , 8 . 
per il solo studio del distretto coronarico i valori dosimetrici sono risultati i seguenti : ctdi volumetrico 33 , 036 , 39 mgy , effective mas 498 , 1693 , 27 . il valore medio di ctdi volumetrico a cui sarebbe stato m . 
volume rendering image shows patency of the arterial y - shaped mammary graft connected with the left anterior descending ( lad ) artery and the first marginal branch ( arrow ) ; in the same reconstruction , venous conduit occlusion is observed at the proximal anastomosis level ( arrowhead )  . 
le immagini ricostruite con tecnica volume rendering dimostrano perviet del bypass arterioso ad y con arteria mammaria interna sinistra ( amis ) su da e primo ramo marginale ottuso ( freccia ) ; nelle stesse scansioni si evidenzia occlusione del graft aorto - coronarico venoso allorigine , con caratteristica estroflessione sulla parete aortica dellanastomosi prossimale ( punta di freccia )  . discussion patient exposure to ionising radiation is the main limitation to the clinical use of 64 - mdct , especially if it is to be used as a potential screening tool in asymptomatic patients . 
despite the patients high heart rate during image acquisition ( 96 bmp ) , maximum intensity projection ( mip ) reconstructions ( a ) show multiple stenotic lesions on the right coronary artery ( arrows ) , with subocclusive stenosis at the proximal third of the vessel . 
a 60% stenosis is also observed in the proximal portion of the left anterior descending ( lad ) artery , caused by soft tissue plaque ( arrow ) ( b )  . 
della paziente al momento dellacquisizione ( 96 bpm ) , le ricostruzioni mip ( a ) documentano la presenza di multiple alterazioni stenosanti lungo tutto il decorso della coronaria destra ( frecce ) con stenosi subocclusiva in corrispondenza del terzo prossimale del vaso . 
le ricostruzioni sono state effettuate con workstation siemens e software syngo inspace 4d . sottoposto il paziente senza lutilizzo della tecnica di modulazione risultato di 54 , 690 , 89 mgy con differenza statisticamente significativa tra ctdi volumetrico con sistema care dose e senza care dose ( p < 0 , 001 )  . 
come noto , lutilizzo del gating cardiaco retrospettivo comporta una continua e relativamente elevata esposizione del paziente ai raggi x per la necessit di effettuare lacquisizione dei dati durante lintera durata della scansione e di registrare contemporaneamente i dati dellecg per poi ricostruire le immagini in una fase definita del ciclo cardiaco [ 1 , 2 , 7 , 36 ]  . altra peculiarit tecnica dellimaging tcms delle arterie coronarie lutilizzo di bassi valori di pitch spirale ( pitch di 0 , 2 con tcms - 64 ) e notevolmente sovrapposti ( pitch < numero di strati ) che nasce dallesigenza di effettuare il campionamento dei dati per la ricostruzione delle immagini da strati sovrapposti e privi di gap nel volume acquisito , ma comporta un ulteriore significativo aumento della dose di esposizione [ 7 , 36 , 38 ]  . 
in aggiunta , rispetto alle precedenti generazioni , nella tcms - 64 lutilizzo di collimazioni submillimetriche ( 640 , 6 mm ) si associa ad un intrinseco incremento del rumore nelle immagini acquisite che pu essere limitato aumentando lamperaggio ( intensit di corrente emessa dal tubo radiogeno ) durante la scansione stessa per mantenere il rapporto segnale / rumore entro ottimali livelli diagnostici . nel nostro studio , il ctdi volume risultato in media di 36 , 538 , 30 mgy per paziente , con valori medi di 38 , 77 , 9 mgy nei pazienti con richiesta clinica per studio dei by - pass coronarici con un valore medio di mas di 567 , 83108 , 35 . rispetto ai dati disponibili in letteratura che riportano per apparecchiature a 4 e 16 canali rispettivamente ctdi volume medi di 3645 , 6 mgy e 43 , 3 mgy [ 35 ] , lutilizzo del sistema di modulazione della dose ha consentito di ottenere nella nostra popolazione valori medi di dose assorbita complessivamente inferiori rispetto alle precedenti generazioni tcms pur mantenendo una buona qualit diagnostica degli esami effettuati . 
i valori di dose efficace ottenuti sono risultati in media di 9 , 53 , 4 msv . malgrado in alcuni pazienti si siano raggiunti anche i 17 , 1 msv , questo dato preliminare , sempre se confrontato con i valori di dose efficace riportati in letteratura con apparecchiature a 4 e 16 strati ( rispettivamente 7 , 111 , 9 msv e 8 , 8 msv ) dimostra come , nella media dei pazienti , tale parametro dosimetrico non risulti significativamente superiore rispetto a quelli riportati con precedenti sistemi tcms [ 3841 ]  . 
appare tuttavia rilevante sottolineare come , a prescindere dallimpiego di sistemi di controllo dosimetrico , lesame tcms - 64 delle coronarie con cardiosincronizzazione comporti una esposizione del paziente in termini di dose efficace quasi doppia rispetto ai 57 msv di un esame tc standard del torace [ 38 , 42 ]  . nella nostra esperienza preliminare , lutilizzo del sistema care dose 4d appare quindi indispensabile per mantenere lesposizione del paziente entro livelli accettabili consentendo di ridurre lesposizione media del paziente del fig . 
7 a 64 - mdct angiography performed in a patient with atypical chest pa multiplanar reconstruction ( mpr ) of left anterior descending ( lad ) artery shows diffuse coronary artery disease with multiple vessel wall abnormalities ; note the presence of a noncalcified soft - tissue - attenuation lesion ( arrowheads ) in the proximal part of the artery , causing a > 60% narrowing of the lumen . 
la ricostruzione multiplanare ottenuta su piano curvo ( cpr ) lungo lasse longitudinale della da , documenta multiple alterazioni parietali a densit mista in corrispondenza del tratto prossimale dellarteria discendente anteriore ( da ) e la presenza di placca a densit mista , prevalentemente morbida , con riduzione significativa ( > 60% ) del lume vasale ( punte di freccia )  . 
lelaborazione delle immagini effettuata con workstation siemens utilizzando software syngo inspace 4d . to record ecg data to reconstruct images in a precise phase of the heart cycle [ 1 , 2 , 7 , 36 ]  . another technical peculiarity coronary artery mdct is the use of low spiral pitch ( 0.2 pitch with 64 - mdct ) and considerable overlap ( pitch < < number of slices ) , which arises from the need to sample data for image reconstruction with overlapping slices and no gap , but this leads to a further significant increase in radiation exposure [ 7 , 36 , 38 ]  . 
8 nella figura viene riportata la distribuzione del ctdi volumetrico ( in mgy ) utilizzando il sistema di compensazione care dose 4d , espresso in funzione del carico anodico effettivo . 
it should be borne in mind , however , that regardless of the use of an automatic dose control system , the 64 - mdct examination of the coronary arteries with cardiac gating involves exposing the patient to almost twice the effective radiation dose of a standard ct chest examination ( 57 msv ) [ 38 , 42 ]  . in our preliminary experience , the use of the care dose 4d systems appears indispensable for maintaining exposure within acceptable levels , allowing a 33.5% reduction in mean exposure compared with a similar acquisition performed without an automatic dose control syste the overall dose can be further reduced ( up to 50% compared with an acquisition without care dose 4d ) by using an ecg pulsing system , which is based on the premise that the best phase in the heart cycle for image reconstruction is the mid to end diastole , that is , the maximum immobility phase of the heart and coronary arteries [ 43 ]  . 
in this manner , during data acquisition , tube current is brought to the maximum level in the midto end - diastolic phase , where the maximum snr is required , and progressively reduced to the minimum towards the end - systolic phase . failure to use an ecg pulsing protocol in our study population derives from the evidence that the best rr interval for image reconstruction , especially in patients with elevated hr , is the end - systolic phase ( 30%35% ) , thus confirming the initial experience of wintersperger et al . 
the reduced snr of images acquired in the systolic phase resulting from an acquisition with an ecg 33 , 5% rispetto ad una analoga acquisizione senza modulazione automatica della corrente . 
la dose complessiva pu essere ulteriormente ridotta ( fino al 50% rispetto ad una acquisizione senza protocollo care dose 4d ) utilizzando un sistema di modulazione ecg - controllato dellemissione del tubo radiogeno ( sistema ecg - pulsing ) che si basa sul presupposto che la miglior fase del ciclo cardiaco nella quale effettuare la ricostruzione delle immagini sia la meso - telediastole , cio la fase di maggiore immobilit del cuore e delle arterie coronarie [ 43 ] ; in tal modo , durante lacquisizione dei dati , la corrente del tubo radiogeno viene portata a livello massimo in fase meso - telediastolica , dove necessario avere un massimo rapporto segnale / rumore e ridotta progressivamente al minimo verso la telesistole . la mancata utilizzazione di un protocollo di modulazione ecg - controllato nella nostra popolazione di pazienti deriva tuttavia dallevidenza che , particolarmente in pazienti con elevata fc , il migliore intervallo r - r per la ricostruzione delle immagini risultato essere la fase telesistolica ( 30%35% ) confermando liniziale esperienza riportata da wintersperger et al . 
although the technique needs to be validated with systematic comparisons with clinical , laboratory and coronarographic data , the latest generation of 64 - mdct scanners offers new possibilities for clinical management of patients with coronary artery disease . the increase in spatial and temporal resolution translates into improved diagnostic image quality with respect to previous generations of multidetector devices . 
thus , 64 - mdct is a noninvasive technique capable of identifying patients requiring interventional or surgical procedures such as selective coronarography with primary angioplasty or stent placement , or surgical revascularisation with bypass grafts . the use of suitable systems for the automatic control of radiation exposure seems nonetheless indispensable in order to limit patient dose , which given the current state of affairs is the main limitation to the clinical use of the technique . nella nostra esperienza clinica iniziale , lutilizzo della tcms - 64 ha fornito risultati molto promettenti . 
bonomo , i - 70031 andria ( ba ) , italy 2dipartimento di scienze radiologiche , irccs casa sollievo della sofferenza , i - 71013 san giovanni rotondo ( fg ) , italy 3dipartimento di radiologia , fondazione s . 
giglio , cefal ( pa ) , italy 4istituto di radiologia , universit di novara , italy 5istituto di radiologia , universit di ancona , italy correspondence to : t . 
scarabino , via napoli 56 , i - 70031 andria ( ba ) , italy , tel . : + 39 - 0883 - 299140 , fax : + 39 - 0883 - 299220 , e - mail : tscarabino@hotmail.com received : 19 may 2006 / accepted : 12 july 2006 / published online : 22 february 2007 abstract ever since the introduction of magnetic resonance ( mr ) , imaging with 1.5 tesla ( t ) has been considered the gold standard for the study of all areas of the body . 
indeed , their high gradient power and field intensity ( 3.0 t ) allow adjunctive and more advanced diagnostic methodologies to be performed with excellent resolution in a fraction of the acquisition time required with earlier machines . 
pi recentemente , lintroduzione di unit rm con intensit di campo di 3 , 0 t per applicazioni cliniche nuove ed avanzate ha comportato notevoli vantaggi , soprattutto in campo neuroradiologico . 
i loro alti gradienti ed intensit di campo infatti consentono di applicare metodologie diagnostiche nuove ed avanzate con eccellente risoluzione in una frazione del tempo di acquisizione richiesto dalle attrezzature precedenti . 
continuous advances in hardware ( gradients , coils ) and software ( acquisition and processing sequences ) have made magnets more compact , powerful and flexible , greatly improving patient comfort . 
higher - field units were introduced some years ago for clinical research purposes , principally in neuroradiology , and are spreading fast ( especially in the usa ) despite their dallavvento della risonanza magnetica ( rm ) le apparecchiature con intensit di campo magnetico di 1 , 5 tesla ( t ) sono considerate il gold standard per coprire le varie applicazioni cliniche in tutti i distretti corporei . 
tali apparecchiature , in virt di continui progressi che hanno interessato lhardware ( gradienti , bobine ) e il software ( sequenze di acquisizione e di elaborazione ) , sono diventate sempre pi compatte , potenti e versatili , con conseguente migliore confort del paziente . 
they are being employed not only in research and with a broader scope compared with traditional research but also in daily clinical practice to support new and sophisticated clinical applications , with considerable practical benefits . 
in the first year , the machine was employed to optimise the various morphological and functional acquisition sequences ( diffusion , perfusion , spectroscopy , cortical activation ) both in vitro ( using dedicated dummies ) and in vivo ( in healthy controls ) and the various postprocessing techniques ( with dedicated software ) with a view to creating a large database as the starting point for research on patients . 
naturally , special attention was devoted to the safety problems related to the machines use , especially issues of patient comfort in the tunnel and compatibility of various biomedical devices . after optimisation of study sequences and protocols , our research programme focused on improving morphofunctional mr imaging of the bra the higher signal - to - noise ratio ( snr ) of the 3.0 - t magnet made it possible to obtain images with greater spatial , contrast and time resolutions in shorter acquisition times compared with lower - field systems , resulting in greater patient comfort and reduction of motion artefacts . the patients studied at 3.0 t exhibited a wide and representative range of conditions that were successfully investigated using standardised dedicated sequences and protocols . 
disadvantages , which include a greater specific absorption rate ( sar ) , greater acoustic noise are not particularly severe and in newer systems are largely reduced by improved hardware and software [ 14 ]  . 
tali sistemi sono ormai diventati una realt e , nonostante lalto costo , si stanno sempre pi diffondendo ( specie in usa ) per essere utilizzati non solo nel campo della ricerca , peraltro molto pi ampia rispetto alla ricerca tradizionale , ma anche e soprattutto nella pratica clinica quotidiana per far fronte a nuove e pi sofisticate applicazioni cliniche con conseguenti importanti benefici pratici . da 5 anni il servizio di neuroradiologia del nostro istituto scientifico dotato di una apparecchiatura rm whole body ( signa horizon lx , general electric medical system , milwaukee , usa ) dotata di magnete superconduttivo , a schermatura attiva , con intensit di campo magnetico 3 , 0 t , gradienti di potenza di 50 millitesla al metro ( mt / m ) e slew rate di 150 mt / m / s . 
il sistema rm 3 , 0 t in dotazione stato utilizzato nel primo anno di lavoro , una volta acquisita lautorizzazione ministeriale alluso , per ottimizzare le diverse sequenze di acquisizione , morfologiche e funzionali ( diffusione , perfusione , spettroscopia , attivazione corticale ) , sia in vitro ( utilizzando fantocci dedicati ) che in vivo ( con controlli sani ) , e le diverse modalit di post - processing ( utilizzando software dedicati ) al fine di creare un ampio database , punto di partenza per studi di ricerca su paziente . 
naturalmente , particolare attenzione stata data alle problematiche di sicurezza inerenti luso di tale apparecchiatura ( con riferimento in particolare alla qualit di confort del paziente in esame e alla rm - compatibilit di vari dispositivi biomedicali )  . ottenuta lottimizzazione di sequenze e protocolli di studio , lobiettivo del nostro programma di ricerca stato quello di migliorare limaging morfo - funzionale cerebrale con rm . 
sfruttando il pi alto rapporto segnale / rumore ( s / r ) possibile con lapparecchiatura 3 , 0 t , stato infatti possibile ottenere immagini con pi alta risoluzione spaziale , di contrasto e temporale , in tempi peraltro ridotti rispetto ai sistemi di pi basso campo , con conseguente miglioramento del confort del paziente e riduzione degli artefatti da movimento . i pazienti sottoposti a rm 3 , 0 t hanno esibito un ampio e rappresentativo spettro di patologia che stata esaminata adeguatamente utilizzando sequenze e protocolli ben definiti e personalizzati . si quindi proceduto allo studio di diverse patologie seguendo le linee dei progetti di ricerca approvati dalla direzione scientifica del nostro istituto , previa autorizzazione del comitato etico . 
lo scopo del lavoro quello di illustrare le caratteristiche semeiologiche peculiari dellimaging cerebrale morfologico e angiografico a 3 , 0 t mettendo in risalto i relativi vantaggi e svantaggi rispetto a sistemi rm di pi basso campo . studio morfologico di base gli studi rm del cervello possono essere suddivisi in due grandi categorie , morfologici e funzionali , sulla base del tipo di informazione che si ricerca . 
lo studio morfologico di base ( detto anche convenzionale o anatomico ) riguarda limaging di tessuto , spazi periliquorali , vascolatura e fasci di fibre , mentre lo studio funzionale in senso lato comprende lo studio delle funzioni cerebrali ( fmri ) limaging di perfusione t . 
 because the user interface and sequence parameters are the same as those employed with 1.5 - t systems , at 3.0 t , in theory , the same images should be obtained with the advantage of high - field strength , i.e. 
 t1 imaging as t1 relaxation times are longer at higher magnetic fields , entailing reduction in the relative differences among different tissue types , it is generally difficult to obtain t1 - weighted images with sufficient contrast when using a 3.0 - t unit [ 6 ]  . 
for this reason , snr optimisation in the same sample using a higher - field unit requires longer time to repetition ( tr ) [ and a smaller flip angle ( fa ) ] , resulting in longer scanning times . 
t1 saturation for a given tr is greater at 3.0 t , resulting in reduced signal gain . in other words , the snr per unit of time would be optimised with the shortest possible tr / t1 . 
the possibility that the snr gain connected with the high magnetic field may substantially be offset by a longer t1 highlights the importance of optimising the imaging parameters [ 3 ]  . 
 e di diffusione , e lo studio metabolico con la spettroscopia . lo studio di rm di base si presenta a 3 , 0 t con un imaging di qualit pi alta rispetto a quello ottenuto a pi basso campo in virt di una serie di vantaggi quali un pi alto rapporto s / r , una maggiore risoluzione spaziale e temporale a fronte di alcuni svantaggi , quali lincremento del specific absorption rate ( sar ) e del rumore acustico , peraltro non particolarmente significativi e comunque in gran parte risolvibili mediante hardware e software di pi recente introduzione [ 14 ]  . 
dato che i tempi di rilassamento sono campo - dipendenti e influenzano il contrasto dellimaging , le sequenze di imaging a 1 , 5 t non possono infatti essere trasferite a 3 , 0 t . 
a ci si aggiunge la deposizione tissutale dellenergia di rf che , essendo eccessiva , va anche considerata per adattare e ottimizzare i protocolli clinici di imaging per luso a 3 , 0 t . 
 fast spgr allows thinner slices to be obtained in a shorter time and provides images suitable for reformatting in all three planes using a single volumetric acquisition of the whole brain , thus disclosing a larger number of lesions than can be depicted using se t1 - weighted sequences acquired in a single plane . 
infatti , non solo il t1 aumenta con laumentare del campo magnetico , ma addirittura converge , determinando una distribuzione meno ampia dei valori di t1 tra i diversi tipi di tessuto . 
per tale motivo per ottimizzare il rapporto s / r dello stesso campione a campo pi alto il tr deve essere pi lungo ( come anche il flip angle deve essere pi corto ) con conseguente allungamento dei tempi desame . utilizzando tr pi lunghi , il vantaggio in intensit di segnale a campo pi alto risulta essere inferiore in unit di tempo . la saturazione t1 per un dato tr infatti pi ampia a 3 , 0 t con conseguente riduzione del guadagno in segnale . 
quindi in virt del fatto che il guadagno nel rapporto s / r derivante dallalto campo pu essere sostanzialmente controbilanciato dallallungamento del t1 , risulta importante lottimizzazione dei parametri di imaging [ 3 ]  . lincremento del t1 rappresenta il pi grande problema per lo studio cerebrale a 3 , 0 t acquisito con sequenza se t1 pesata in cui il contrasto t1 appunto inaccettabile [ 1 , 2 , 4 , t . 
for instance , when studying primary and secondary brain tumours , administration of a gadolinium - based agent yields greater contrast between tumour and normal brain tissue both in single and in multiple doses . 
it also detects more metastases and demonstrates different patterns of enhancement that may be useful to assess the degree of malignancy and monitor response to therapy [ 2628 ]  . 
the greater sensitivity of 3.0 - t contrast - enhanced investigations has also been demonstrated in multiple sclerosis , with a 21% increase in the number of enhancing lesions detected , a 30% increase in enhancing lesion volume and a 10% increase in total lesion volume relative to scanning at 1.5 t [ 29 ]  . 
using a standard dose , the contrast - to - noise ratio ( cnr ) is two and a half times greater than with 1.5 - t systems [ 13 ]  . 
double or triple doses can result in meningeal contrast uptake , a common nonpathological finding at 3.0 t that at lower field strengths may , however , mimic carcinomatosis or meningitis and should thus be avoided . 
to enhance sensitivity or highlight minimal changes in the blood - brain barrier , a double dose of contrast agent may be employed in selected investigations of brain metastases or inflammatory disease [ 30 , 31 ]  . 
high spatial resolution fast spin echo ( fse ) - weighted images are especially effective at 3.0 t , as they provide more anatomical detail and better contrast due to the greater snr , which allows the use of thinner slices and broader matrices [ 1 , 2 , 4 , 32 ]  . 
tale sequenza inoltre caratterizzata da ipersegnale delle grosse strutture vascolari arteriose che comunque non inficia linterpretazione delle immagini . mentre gli studi t1 pesati sono tradizionalmente meno informativi e richiedono pi tempo , un tipico studio flair t1 pesato del cervello consente , insieme allutilizzo dellimaging parallelo , lapplicazione di protocolli a pi alta risoluzione con tempi desame pi brevi rispetto ai campi ad intensit 1 , 5 t . 
naturalmente tale aspetto diventa problematico se dobbiamo acquisire pi studi , senza e con mdc , o pi proiezioni . in rapporto al maggiore effetto inflow del mdc e alla maggiore soppressione del fondo , limaging t1 con mdc sicuramente un vantaggio del 3 , 0 t rispetto al 1 , 5 t . 
nello studio ad esempio dei tumori cerebrali primitivi e secondari la somministrazione del gadolinio produce un maggior contrasto tra lesione tumorale e parenchima normale sia a singola dose e a dose multipla , permette di rilevare un maggior numero di metastasi , pu dimostrare differenti pattern di impregnazione che risultano utili per definire il grado di malignit e per monitorare la risposta alla terapia [ 2628 ]  . 
rispetto al 1 , 5 t infatti alcuni autori hanno documentato un incremento del 21% del numero delle lesioni con impregnazione patologica , del 30% nel volume di impregnazione e del 10% del volume totale delle lesioni [ 29 ]  . 
il rapporto contrasto / rumore ( c / r ) risulta infatti maggiore rispetto allo studio con sistemi rm 1 , 5 t ( di ben 2 , 5 volte ) utilizzando una dose standard [ 13 ]  . 
da evitare la dose doppia o tripla responsabile di impregnazioni meningee , reperti comuni non patologici a 3 , 0 t ( con sistemi 1 , 5 t tali quadri possono simulare una carcinomatosi o una meningite )  . 
3 imaging fse t2 ad alta definizione della sezione mediana del cervello . infiammatoria per incrementare la sensibilit o per stressare le minime alterazioni della barriera emato - encefalica ( bee ) , una dose doppia pu essere preferita [ 30 , 31 ]  . 
di solito nello studio t1 con mdc la fast ge t1 pesata viene preferita , al posto delle tradizionali se , che presentano un contrasto minore a parit di tempo dacquisizione . 
ne consegue una migliore risoluzione spaziale ( e quindi maggiore dettaglio anatomico ) e di contrasto , possibili per effetto di un pi alto rapporto s / r che permette luso di spessore di strato inferiori e di matrici pi ampie [ 1 , 2 , 4 , 32 ]  . 
2a , b studio di microadenoma ipofisario prima ( a ) e dopo mdc endovena ( b ) con sequenza fse - xl t1 ( tr / te 600 / 12 , etl 5 , fov 180 mm , spessore di strato 2 , 5 mm / 0 , 5 , matrice 224192 , zip 512 , 29 / fase )  . creased deposition of radiofrequency ( rf ) energy , which in turn requires long tr or pulse refocalisation angles well below 180 . 
in addition , the broader bandwidth , smaller echo space , shorter minimum tr and te and shorter fse sequences employed at higher field strengths result in improved image quality , artefact reduction and enhanced diagnostic performance in much shorter examination times , which is to the patients benefit . 
these sequences allow excellent visualisation of the basal or mesencephalic nuclei by virtue of their iron content despite the intrinsically lower sensitivity of fse to magnetic susceptibility in 3.0 - t compared with 1.5 - t systems [ 5 ]  . 
4a - d high - definition ( hd ) study of the inner ear using a 3d fast imaging employing steady state acquisition ( fiesta ) sequence [ time to repetition ( tr ) 4.3 , echo time ( te ) 1.5 , flip angle ( fa ) 50 , band width ( bw ) 62 khz , field of view ( fov ) 170 , slice thickness 0.6 mm , matrix 256256 , zero fill interpolation processing ( zip ) 512 , 2 , number of excitations ( nex ) , 4 : 43 ]  . 
4a - d studio ad alta definizione dellorecchio interno con sequenza 3d fiesta ( tr / te 4 , 3 / te 1 , 5 , flip angle 50 , bw 62 khz , fov 170 , spessore di strato 0 , 6 mm , matrice 256256 , zip 512 , 2 nex , 4 : 43 ) : singole partizioni ( a ) , zoom ( b ) , mip ( c ) , elaborazione con ricostruzione di volume ( d )  . rhage , which at 3.0 t is characterised by greater hypointensity in the acute and early subacute phases [ 33 ]  . 
 flair imaging flair sequences , which are generally included in all imaging protocols , are also sharper and more sensitive at 3.0 t sono pi bassi , quindi il tempo in fse si riduce , la qualit aumenta , gli artefatti si riducono . 
con tale sequenza sono ben apprezzabili i nuclei della base o del mesencefalo che risaltano maggiormente ( per effetto del loro contenuto di ferro ) , nonostante la nota intrinseca minore sensibilit alla suscettibilit magnetica della fse , rispetto a sistemi 1 , 5 t [ 5 ]  . una variazione di semeiotica del segnale sembra interessare anche le emorragie cerebrali caratterizzate in particolare da una maggiore ipointensit a 3 , 0 t in fase acuta e subacuta precoce rispetto allintensit di segnale rilevabile a 1 , 5 t [ 33 ]  . 
a tal proposito il c / r e lintensit di segnale a 1 , 5 t e 3 , 0 t sono sostanzialmente equivalenti per cui di solito comunque non vi sono particolari problemi per interpretare correttamente let dellemorragia . 
first , it allows performance of all angiographic sequences applied routinely in clinical practice with lowerfield systems , such as 2d and 3d time of flight ( tof ) and phase contrast ( pc ) , as well as ultrafast dynamic sequences acquired after contrast agent bolus administration [ contrastenhanced mra ( ce - mra ) ]  . 
as with routine mr scanning , the technical parameters of angiographic sequences need to ge ( t2 * ) quali ad esempio la ciss ( constructive interference in the steady state ) particolarmente indicata nello studio dellorecchio interno . 
la maggiore sensibilit si ha anche grazie alluso di te pi lunghi , necessari per i tempi di rilassamento modificati a 3 , 0 t , che permettono un buon contrasto ed un rumore accettabile . 
il rilievo di piccole lesioni richiede infatti lottimizzazione del c / r piuttosto che del rapporto s / r e questo viene ottenuto appunto con te pi lunghi ( 120 ms ) anche se tale allungamento incrementa oltre il contrasto anche il rumore ma in modo accettabile . inoltre , contrariamente a quanto accade per sistemi 1 , 5 t , in virt della sostanziale mancanza di differenza del t1 del liquor ( che essenzialmente un liquido ) tra 1 , 5 t e 3 , 0 t , il tempo di inversione ( ti ) richiesto per annullare il liquor rimane dello stesso valore ( 2 , 250 millisecondi circa ) [ 5 ]  . tale caratteristica non valida in altre sequenze ir , sia in quelle in cui si cerca di massimizzare il contrasto tra differenti tessuti ( ad esempio tra sostanza bianca e sostanza grigia ) sia in quelle con soppressione del grasso , nelle quali invece il ti deve essere incrementato del 25%40% . 
le note aree di sostanza bianca soprattutto periventricolare fisiologicamente iperintense con sistemi a pi basso campo ( 1 , 5 t ) sono ancora pi accentuate a 3 , 0 t per cui c bisogno di una particolare attenzione per distinguerle da patologie reali ( ad esempio sclerosi laterale amiotrofica ) [ 1 ]  . 
in addition , the change in t1 relaxation time , namely , increased t1 , yields greater background suppression of stationary tissues due to the decrease of r1 , i.e. 
the rate of longitudinal or spin - lattice relaxation , with greater flow enhancement , as blood r1 is roughly constant thereby improving vessel - tissue contrast [ 19 , 22 , 36 ]  . 
this advantage makes magnetisation transfer application less effective than it is with 1.5 t systems [ 37 , 38 ]  . the effect is mainly evident using the 3d tof technique , as the short tr usually saturates stationary tissues but not moving blood [ 7 , 39 ] , and the tag persists for a longer time . these effects lead to greater vessel detail and conspicuity , especially in disclosing small - calibre vessels , including surface vessels not clearly depicted at 1.5 t [ 23 , 25 ]  . 
il recente sviluppo di nuovi hardware ( nuove coil ) o lutilizzo di pi recenti software ( imaging parallelo ) potranno ridurre tale inconveniente . studio angiografico con il 3 , 0 t lo studio angiografico si avvantaggia in modo significativo rispetto a sistemi rm di pi basso campo ( fig . 7 ) [ 1 , 2 , 4 , 35 ]  . 
innanizitutto un sistema rm a 3 , 0 t permette di eseguire tutte le sequenze angiografiche utilizzate di solito nella pratica clinica con sistemi a pi basso campo quali le pi comuni time of flight ( tof ) o phase contrast ( pc ) , entrambe con modalit 2d o 3d , od anche quelt . 
therefore , contrast administration further improves imaging at 3.0 t due to the high snr , which can be transformed into spatial resolution : resolution on a plane le ultrarapide utilizzate con tecnica dinamica dopo somministrazione a bolo del mdc ( contrast enhancement magnetic resonance angiography , ce - mra )  . 
tale vantaggio , che rende peraltro non particolarmente efficace ( come invece accade con sistemi 1 , 5 t ) luso della magnetization transfer ( mt ) [ 37 , 38 ] apprezzabile soprattutto quando si utilizza la tecnica angiografica 3d tof in quanto il breve tr satura di solito i tessuti stazionari ma non il sangue in movimento [ 7 , 39 ]  . 
tali effetti comportano un incremento del dettaglio e della conspicuity vascolare con in particolare evidenza di vasi di pi piccolo calibro , anche superficiali ( di iv ordine ) , non chiaramente identificabili con sistemi rm 1 , 5 t [ 23 , 25 ]  . per lo stesso motivo lutilizzo di campi magnetici elevati ( 3 , 0 t ) sembra in grado di migliorare la cospicuit dei vasi intracranici del neonato o di ridurre ulteriormente i tempi di acquisizione [ 40 ]  . 
lo studio angio - rm a 3 , 0 t in pazienti portatori di tali dispositivi biomedicali ( purch gi testati ) pu essere quindi eseguito senza particolari rischi [ 33 , 45 ]  . i benefici ottenuti a 3 , 0 t , evidenti soprattutto nella patologia vascolare malformativa ( specie aneurismatica ) e atefig . 
time - resolved imaging of contrast kinetics ( tricks ) images [ 3d time of flight spoiled gradient recalled ( tof - spgr ) , time to repetition ( tr ) 3.7 , echo time ( te ) 1.3 , matrix 224192 , slice thickness 1.8 mm , field of view ( fov ) 28 , temporal resolution 2.5 s , 8 phases ] of multiple vascular phases : contrast enhancement of arteries ( a ) , capillaries ( b ) and veins ( c )  . 
in tale modo possibile visualizzare diverse fasi vascolari : arterie ( a ) , capillari ( b ) e vene ( c )  . ments are increased at higher - field strengths resulting in artefacts caused by the susceptibility of biomedical devices such as the aneurysm clips commonly used in interventional and therapeutic neuroradiological procedures , the newer devices do not seem to present major safety or compatibility problems [ 42 , 44 ]  . 
resolution quality tends to be privileged in clinical practice , with acquisition of a larger number of slices of rerosclerotica cerebrale , rendono ancora pi competitiva langiografia con rm , nonostante una minore risoluzione spaziale rispetto allangiografia convenzionale ( dsa ) , ormai sempre pi utilizzata in campo intervenzionistico - terapeutico piuttosto che diagnostico [ 46 ]  . conclusioni grazie al suo alto rapporto s / r , la mri ad alto campo in grado , di supportare nuove applicazioni diagnostiche o di migliorare le metodiche esistenti . 
in virt dellalto rapporto s / r il neuroradiologo pu scegliere di eseguire un imaging cerebrale a 3 , 0 t in un tempo uguale a quello ottenibile con un sistema 1 , 5 t privilegiando in tal caso una pi alta qualit delle immagini ( incrementando la matrice e / o riducendo lo spessore di strato e / o il fov ) oppure di avere un imaging di qualit pari al quello di un sistema 1 , 5 t in un tempo inferiore privilegiando in tal caso il confort del paziente , od anche pu scegliere di ridurre la dose del mezzo di contrasto somministrato . 
di solito nella pratica clinica si cerca di privilegiare la risoluzione acquisendo pi fette , di spessore sottile , con campi di vista pi piccoli , con matrici pi ampie e in tempi comparabili a quelli con i sistemi 1 , 5 t . 
spesso in rapporto al quesito clinico e al tipo di paziente in esame , si cerca di trovare un compromesso tra risoluzione e velocit ( riducendo ad esempio il numero delle eccitazioni ) [ 34 ]  . lalto rapporto s / r per effetto dellalto campo pu in realt essere ottenuto anche a 1 , 5 t utilizzando i pi recenti hardware ( bobine riceventi di superficie , single o in arrays ; gradienti pi performanti capaci di ridurre il te ) e t . 
however , this cannot be done in the case of unstable or poorly co - operative patients , or it may be impossible for cost reasons ( reduced patient flow )  . 
lastly , the higher snr of high - field mr systems is a resource that neuroradiologist can exploit in clinical practice , as the higher the snr , the more the imaging protocols can be adjusted . acknowledgments to technical staff : c . 
il caso di pazienti instabili , non collaboranti , come anche ci possono essere altre motivazioni ad esempio di natura economica ( la riduzione del flusso dei pazienti )  . 
non solo , anche a 1 , 5 t possibile un incremento delle dimensioni della matrice : in tal caso per la conseguente riduzione delle dimensioni del voxel comporterebbe maggiore granulosit dellimaging . 
pertanto il maggiore rapporto s / r da alto campo sicuramente unottima arma che il neuroradiologo pu sfruttare nella pratica clinica : maggiore il rapporto s / r , maggiori sono infatti le possibilit del neuroradiologo di modificare i protocolli di imaging . rigraziamenti allo staff tecnico : c . 
 correspondence to : giuseppe caruso , via liguria , 21 , i - 90144 palermo , italy , tel . : + 39 - 91 - 6552315 , fax : 39 - 91 - 6552337 , e - mail : carusogi@libero.it received : 23 march 2006 / accepted : 18 august 2006 / published online : 22 february 2007 abstract purpose . 
a total of 1 , 729 ( 1 , 012 women and 717 men ; age range 2882 ; mean age 51 ) patients underwent contrastenhanced sonography of the liver . 
the examination was performed with a low mechanical index ( mi < 0.09 ) after injection of sulphur - hexafluoride - filled microbubbles , using different sonographic equipment and different contrast - specific algorithms . 
heterogeneous delayed liver enhancement was observed in six patients in the late phase ( 180 s ) , with the presence of multiple , partially confluent , hyperechoic areas peripheral to the portal vessels . 
the pattern appeared spontaneously between 1 and 4 h after the examination and was associated with the presence of an anomalous echogenicity in the superior mesenteric veno patient experienced adverse reactions . 
1729 pazienti ( 1012 donne e 717 uomini ; et compresa tra 2882 , media 51 ) sono stati sottoposti ad esame ecografico del fegato dopo somministrazione di ecoamplificatore esafluoruro di zolfo e basso indice meccanico ( mi < 0 , 09 )  . 
limpregnazione anomala del parenchima epatico potrebbe essere secondaria allintrappolamento nei sinusoidi epatici di gas proveniente dal microcircolo intestinale attraverso il sistema entero - portale . key words ultrasound microbubbles liver parole chiave ecografia microbolle fegato introduction introduzione sonographic contrast agents consist of microbubbles containing an inert gas or air with a diameter < 5 m surrounded by a shell or a membrane that provides transpulmonary stability and provides transpulmonary stability and increasing their persistence in the circulation . 
the total volume of mii mezzi di contrasto utilizzati in ecografia sono costituiti da microbolle ( diametro < 5 m ) contenenti gas inerte o aria , e stabilizzate da membrane a composizione differente , che ne garantiscono la stabilit attraverso il circolo transpolmonare aumentandone la persistenza in circolo . 
the second relies on detection of ultrasound ( us ) - induced physical phenomena , such as microbubble destruction , fusion or splitting [ 4 ]  . the purpose of this paper is to report a pattern of heterogeneous late - phase hepatic enhancement with anomalous duration and distribution associated with stratified hypoor hyper - echogenicity in the superior mesenteric vein , which was observed after infusion of sonovue contrast mediuan aetiological hypothesis is also presented . materials and methods from december 2001 to august 2004 , 1 , 729 patients ( 1 , 012 women and 717 men ; age range 2882 years ; mean age 51 ) underwent contrast - enhanced sonography of the liver after injection of sonovue contrast medium ( bracco , milan , italy )  . sonovue is a suspension of hexafluoride sulphur microbubbles ( mean diameter 3 m ) with a phospholipidic shell . 
the elective technique consisted of a bolus injection of 4.8 ml of contrast medium at a rate of approximately 1 ml / s , followed by a 5ml saline flush . 
sebbene si tratti essenzialmente di sostanze blood - pool , il loro comportamento nelle diverse fasi post - contrastografiche sovrapponibile a quello dei mezzi di contrasto organo - iodati , con la differenza che non si ha una vera fase interstiziale . lintroduzione del mezzo di contrasto nel circolo periferico permette di identificare tre diverse fasi della perfusione vascolare epatica , analogamente a quanto possibile ottenere allesame tc dinamico del fegato dopo somministrazione di mezzo di contrasto organo - iodato : fase arteriosa , a 2030 s : in questa fase lenhancement dovuto alla presenza del mezzo di contrasto nelle arterie di piccolo calibro ; fase portale e tardiva , a 60 e 180 s , rispettivamente : nonostante il mezzo di contrasto ecoamplificatore non passi nellinterstizio ma rimanga nei vasi , lenhancement osservato in fase portale e specialmente in fase tardiva , sembra essere dovuto alla persistenza delle microbolle nei sinusoidi o al loro up - take da parte delle cellule del kupffer e delle cellule del sistema reticolo - endoteliale [ 2 , 3 ] ; ipotesi comunque queste che devono essere avvalorate da ulteriori studi di farmacocinetica . le tecniche di imaging ecografico contrasto - specifiche sono due : la prima quella dellimaging non - distruttivo in cui limmagine viene costruita sfruttando la risposta non lineare delle microbolle , senza che queste vengano distrutte ; la seconda tecnica utilizza limaging distruttivo , che determina la distruzione , la fusione e lo splitting delle microbolle [ 4 ]  . scopo del nostro lavoro quello di riportare un fenomeno caratterizzato dalleterogeneo enhancement del parenchima epatico in fase tardiva , anomalo per durata e distribuzione , associato ad un pattern stratificato ipo - iper - ecogeno della vena mesenterica superiore dopo somministrazione di sonovue . 
sulla scorta di una serie di osservazioni abbiamo avanzato una ipotesi eziologica . materiali e metodi dal dicembre 2001 allagosto 2004 , 1729 pazienti ( 1012 donne - 717 uomini , di et compresa tra 28 e 82 anni ; et media 51 anni ) , hanno eseguito un esame ecografico del fegato con ecoamplificatore . 
il sonovue una sospensione di microbolle di esafluoruro di zolfo ( diametro medio 3 , 3 m ) , stabilizzate da una membrana fosfolipidica ; si presenta come una polvere liofilizzata in atmosfera di solfuro esafluoride posta allinterno di un flaconcino di plastica . 
una volta ricostituita , la sospensione appare come soluzione lattescente e rimane stabile per al massimo 6 ore [ 5 ]  . liniezione del mezzo di contrasto stata effettuata 510 minuti dopo la ricostituzione dello stesso . 
la tecnica consiste nelliniezione a bolo di 4 , 8 ml di mezzo di contrasto a velocit di 1 ml / s , seguita dalla infusione di 5 ml di soluzione g . 
use of these algorithms allowed real - time imaging of all vascular phases ( arterial , portal and late ) and was dependent on the availability of the us device at the time of examination ( table 1 )  . 
all examinations were performed as follows : fundamental ( b - mode ) imaging and contrast - specific algorithm without contrast agent contrast - enhanced us in the arterial phase ( 2030 s ) contrast - enhanced us in the portal and late phase ( 60 and 180 s ) contrast - enhanced us in the second late phase ( 240 s )  . patients who showed heterogeneous late - phase hepatic enhancement were examined using the b - mode technique and stimulated acoustic emission ( sae ) , both performed with a high mi ( 1.2 ) ; insonation with high mi is useful for microbubble distribution , leading to possible rapid disappearance of the heterogeneous enhancement pattern . two of the six patients underwent a second contrast - enhanced us after 24 h and 9 days , respectively , using the same us system and the same contrast agent at the same dose . 
tutti gli esami sono stati eseguiti con le stesse modalit come riportato di seguito : imaging fondamentale ( b - mode ) e algoritmo contrastospecifico senza mezzo di contrasto ; ecografia con mezzo di contrasto : fase arteriosa a 2030 s ; ecografia con mezzo di contrasto : fase portale e tardiva a 60 e 180 s rispettivamente ; ecografia con mezzo di contrasto : seconda fase tardiva a 240 s . i pazienti nei quali stato osservato , in fase tardiva , leterogeneo enhancement epatico sono stati sottoposti a esame ecografico con tecnica b - mode in e con stimulated acustic emission ( sae ) entrambe ad elevato indice meccanico ( mi = 1 , 2 ) , allo scopo di determinare la distruzione delle microbolle di mezzo di contrasto con leventuale rapida scomparsa delleterogeneo enhancement . due dei sei pazienti hanno eseguito un secondo esame ecocontrastografico a 24 ore e a 9 giorni rispettivamente , utilizzando la stessa apparecchiatura ecografica , lo stesso mezzo di contrasto , nella stessa dose . 
nei due pazienti in cui stata somministrata per la seconda volta lo stesso mezzo di contrasto nella stessa dose ( a distanza rispettivamente di 24 ore e 9 giorni ) il fenomeno non si ripresentato . 
nessuno dei sei pazienti ha presentato sintomi , n sono state osservate alterazioni della pressione arteriosa . discussione leterogeneo enhancement epatico stato descritto per la prima volta da okada [ 6 ] : egli ha osservato un fenomeno simile in sei pazienti dopo somministrazione di levovist ( 5 casi ) e di echogen ( 1 caso )  . 
1 immagine ottenuta dopo somministrazione di ecoamplificatore con coherent contrast imaging , fase tardiva ( 4 minuti ) : presenza di multiple aree iperecogene parzialmente confluenti nel contesto del parenchima epatico perifiericamente ai vasi portali ( frecce )  . 
 observation of these findings was possible thanks to the use of second - generation sonographic contrast agents , which allow real - time examination of hepatic vascular perfusion : this suggests that gas is present in the enteroportal circulation but not in the other vessels , which could account for the origin of the hepatic phenomenon . 
4 fundamental ( b - mode ) imaging , late phase ( 40 min ) : marked hyperechogenicity ( 1 ) can be seen in the superior mesenteric vein ( between the two arrows )  . 
4 immagine in basale ( b - mode ) ; fase tardiva a 40 minuti : possibile dimostrare una marcata iperecogenicit ( 1 ) nel lume della vena mesenterica superiore ( compresa tra le due frecce )  . 
liperecogenicit appare localizzata in sede ventrale mentre lipoecogenicit in sede declive come fase gassosa in fase fluida ( 2 )  . discussion heterogeneous hepatic enhancement was first described by okada [ 6 ] , who reported a similar phenomenon occurring in six patients after injection of levovist ( five cases ) and echogen ( one case )  . 
to the best of our knowledge , heterogeneous hepatic enhancement has never been observed following administration of sonovue contrast mediuunlike the agents employed by okada , sonovue relies on a low mi to provide real - time imaging of hepatic perfusion [ 7 ]  . 
il fenomeno si verificato con mezzi di contrasto diversi ( per tipo di gas e natura della membrana delle microbolle ) e con tecniche di insonazione diverse : una ad alto indice meccanico con distruzione delle microbolle ( levovist ed echogen ) ; laltra a basso indice meccanico con fenomeni di risonanza delle microbolle ( sonovue ) [ 8 ]  . il levovist un agente epato - specifico ; ha unemivita breve e il suo effetto dopo linsonazione dura solo alcuni secondi . 
moreover , has liver - specific parenchymal uptake after blood - pool clearance ; it is short - lived , and once an area has been scanned for a few seconds , the effect disappears . 
it is best seen with relatively high acoustic power settings ( although still within accepted levels for diagnostic imaging ) and shows a tendency to cluster at the level of the focal zone , where the power is maximal [ 9 , 10 ]  . 
in contrast , sonovue is purely a vascular agent , with no evidence of selective uptake ; it shows a spleen - specific enhancement that lasts longer ( 5 min ) than the blood - pool and liver enhancement phases [ 11 ]  . 
 moreover , the gas microbubbles responsible for this phenomenon are larger than the contrast agent microbubbles and are unable to cross the hepatic sinusoids , the calibre of which is 4050 in addition , this anomalous echogenicity was observed in the vena porta and superior vein only , and not in the splenic vein , hepatic vein , aorta or inferior vena cava . 
echogenicity is similar , but more intense , to the pattern seen in cases of free gas migration into the portal vessels during intestinal ischaemia , necrotic enterocolitis or in other cases of intestinal pneumatosis [ 12 , 13 ]  . 
the possibility that this phenomenon is due to free gas ( thus not incorporated in the shell ) in the superior mesenteric vein and portal vessel is confirmed by several other observations : the stratification pattern seen in the superior mesenteric vein never occurs when the gas is contained in a membrane , as in the case of contrast microbubbles , but only when the gas is free ( intestinal pneumatosis ) the phenomenon persists even after the mi has been increased , an event that should cause immediate microbubble destruction the distribution inside the periportal sinusoids is similar to that seen after injection of free co2 in the hepatic artery ( portal angioechography ) for transient obstruction in the internal sinusoids [ 14 , 15 ]  . a probable explanation for the heterogeneous hepatic enhancement is that the free gas in the superior mesenteric vein is gas emboli originating in the intestinal microcirculation and transported to the liver via enteroportal circulation . 
the pattern of heterogeneous hepatic enhancement is due to entrapment in the hepatic sinusoids of these gas emboli , which have different insonation properties from the microbubbles . several studies have reported that sonographic contrast agents may be responsible for biological damage to the cell membranes and endothelium both in vitro and in vivo [ 1720 ]  . 
di contro , il sonovue , un agente puramente vascolare , non mostra uptake selettivo epatico , mentre presenta una fase spleno - specifica , della durata di circa 5 minuti [ 11 ]  . 
il volume globale di gas contenuto nelle dosi somministrate dellordine di microlitri , invece il fenomeno osservato da noi massivo . inoltre , le microbolle di gas responsabili di questo fenomeno sono di dimensioni maggiori di quelle costituenti il mezzo di contrasto : esse non sono in grado di attraversare i sinusoidi epatici il cui calibro di 4050 abbiamo , inoltre , notato che solo la vena porta e la vena mesenterica superiore presentavano unanomala ecogenicit , non la vena splenica , n le vene sovraepatiche , laorta o la vena cava inferiore . questo anomalo aspetto ecogeno simile , ma pi intenso , al pattern che si osserva nei casi di migrazione di gas libero nei vasi portali in corso di ischemia intestinale , di enterocolite necrotizzante o in altri casi di pneumatosi intestinale [ 12 , 13 ]  . 
la possibilit che laspetto descritto sia da imputare a gas libero ( non incorporato in una membrana ) nella vena mesenterica superiore e nei vasi portali confermato da altre osservazioni : il pattern stratificato allinterno della vena mesenterica superiore non mai osservabile nel caso in cui il gas trovi allinterno di una membrana come nel caso delle microbolle di mezzo di contrasto ; si osserva solo nel caso di gas libero ( pneumatosi intestinale ) ; il fenomeno persiste anche innalzando gli indici meccanici , evento che dovrebbe determinare la distruzione immediata delle microbolle ; la distribuzione allinterno dei sinusoidi periportali sovrapponibile a quanto osservabile dopo iniezione di co2 libera nellarteria epatica ( ecocarbossigrafia ) , per transitorio ostacolo allinterno dei sinusoidi [ 14 , 15 ]  . in base a queste osservazioni si pu ipotizzare che il fenomeno del disomogeneo enhancement epatico sia il risultato di gas libero nella vena mesenterica superiore proveniente da emboli di gas formatisi a livello del microcircolo intestinale e da qui trasportati al fegato attraverso il circolo enteroportale . 
 [ 21 ] demonstrated that in mice and rats , sonographic contrast agents cause inflammation , necrosis and ulceration of the cecum and proximal colon ( cecocolonic area ) , even with a single intravenous administration of a gas - carrier contrast agent . 
 [ 16 ] reported that intestinal lesions in mice and rats after sonographic contrast agent administration are related to the formation of large intravascular gas bubbles in the cecal and colonic wall . 
another probable explanation for heterogeneous hepatic enhancement is microbubble fusion in vivo inside the sinusoids and mesenteric vessels : these microbubble macroaggregates have different insonation properties than the separate microbubbles because of their different size [ 22 ]  . our study has two limitations . 
second , we are unable to explain why this phenomenon is so rare and why it did not occur again in the same two patients after 24 h and 9 days , respectively . 
 [ 16 ] hanno osservato che le lesioni intestinali riscontrate nei topi e nei ratti dopo somministrazione di mezzo di contrasto ecografico sono correlate alla formazione di macrobolle di gas nella parete colica e cecale . 
unaltra probabile spiegazione alleterogeneo enhancement epatico la fusione delle microbolle in vivo allinterno dei sinusoidi e nei vasi mesenterici : questi macroaggregati , in ragione delle loro diverse dimensioni , presenterebbero caratteristiche di insonazione diverse da quelle delle microbolle [ 22 ]  . il nostro lavoro presenta due limiti : il primo relativo al fatto che le lesioni intestinali descritte da dirven et al . 
 [ 16 ] sono state osservate solo in animali di piccola taglia ( topi e ratti ) , non in animali di taglia maggiore ( porcellini dindia , conigli o cani )  . 
il secondo limite , legato al fatto che non siamo in grado di spiegare perch il fenomeno sia cos raro e perch non si sia ripresentato negli stessi pazienti a 24 h e 9 giorni rispettivamente . nonostante non sia stato possibile chiarire la genesi del fenomeno , le alterazioni osservate sono reversibili e non compromettono la compliance del paziente . 
caramella , radiologia diagnostica e interventistica , via roma 67 , i - 56126 pisa , italy , tel . : + 39 - 050 - 992509 , fax : + 39 - 050 - 551461 , e - mail : caramella@med.unipi.it received : 23 may 2006 / accepted : 07 august 2006 / published online : 22 february 2007 abstract purpose . 
mri exams were done with a scanner operating at 1.5 tesla ( t ) using an endorectal coil . all patients underwent radical prostatectomy within 2 weeks from the imaging assessment . 
our study suggests that by using image fusion between colour - doppler trus and endorectal mri , it is possible to improve the accuracy of pathological staging in patients who are candidates for radical prostatectomy . key words prostate cancer , imaging prostatic cancer , staging image fusion riassunto obiettivo . 
valutare il ruolo della fusione di immagini nella stadiazione del carcinoma prostatico in un campione di 32 pazienti valutati pre - operatoriamente con ecografia transrettale ( trus ) color - doppler e risonanza magnetica ( rm )  . 
il nostro studio suggerisce che la fusione di immagini tra trus color - doppler e rm permette di migliorare laccuratezza della stadiazione istopatologica in pazienti candidati a prostatectomia radicale . parole chiave carcinoma della prostata , imaging carcinoma della prostata , stadiazione fusione di immagini introduction introduzione the incidence of prostatic cancer doubles with every decade of ageing , reaching 70% over 80 years . 
although no uniform treatment regimen exists , patients with tumours confined to the prostate ( clinical stages t1 or t2 ) and with a life expectancy of 10 or more years are often considered to be good candidates for radical prostatectomy . 
those with stage t3 lesions are usually treated with radiation therapy and those with stage t4 lesions with hormonal therapy . transrectal ultrasound ( trus ) examination , either conventional or colour - doppler , must be considered as the first imaging approach , together with prostate - specific antigen ( psa ) screening . 
in the literature , some concerns have been raised concerning the ability of trus to preoperatively assess pericapsular tumour invasion [ 1 ] , although colourdoppler trus was shown to improve depiction of prostatic vasculature as well as lesion detection and targeting [ 24 ]  . magnetic resonance imaging ( mri ) has been used as a staging modality in the preoperative evaluation of patients with clinically localised prostate cancer considered to be candidates for radical prostatectomy . 
il carcinoma prostatico origina nella zona periferica della ghiandola come una lesione nodulare con la tendenza ad invadere la porzione centrale della ghiandola e a sconfinare oltre la capsula negli stadi pi avanzati . 
quando il tumore insorge nella porzione centrale , la diagnosi differenziale con un nodulo benigno risulta difficile e per tale motivo ci possono essere errori di interpretazione . la decisione terapeutica per il carcinoma della prostata dipende dalla accuratezza nella stadiazione di malattia . 
sebbene non esista un unico tipo di trattamento , pazienti con tumore localizzato alla prostata ( stadio clinico t1 o t2 ) e con aspettativa di vita superiore a 10 anni sono spesso considerati buoni canditati per un intervento di prostatectomia radicale , mentre pazienti con lesioni allo stadio t3 o t4 sono trattati rispettivamente con radioterapia e con terapia ormonale . lesame ecografico transrettale ( trus ) , convenzionale o con color - doppler , il primo approccio strumentale da utilizzare insieme alla valutazione del psa . 
sebbene in letteratura alcuni studi abbiano messo in discussione la capacit pre - operatoria della trus di valutare lestensione extra - capsulare del tumore [ 1 ] , stato ampiamente appurato che lutilizzo del color - doppler migliori notevolmente non solo la possibilit di valutare la vascolarizzazione prostatica , ma anche di rilevare la presenza delle lesioni stesse [ 24 ]  . 
la risonanza magnetica ( rm ) stata utilizzata come indagine strumentale nella stadiazione pre - operatoria dei pazienti con tumore prostatico localizzato e pertanto candidati alla prostatectomia radicale . scopo del nostro studio stato quello di valutare il possibile ruolo della fusione di immagini nella stadiazione del carcinoma prostatico e a tal fine sono stati valutati pre - oparatoriamente con trus ( convenzionale e color - doppler ) e con rm con bobina endorettale , 32 pazienti con diagnosi clinica di carcinoma della prostata . materiali e metodi pazienti in un periodo di tempo compreso tra gennaio 2004 e luglio 2005 , abbiamo valutato con trus e rm 32 pazienti ( et media 66 , 5 anni ; et compresa tra 53 e 75 anni ; psa medio 9 , 2 ; psa compreso tra 5 , 47 ng / ml e 15 , 7 ng / ml ) , successivamente sottoposti ad intervento di prostatectomia radicale . tutti i pazienti hanno firmato il consenso informato in accordo con il protocollo di studio , approvato istituzionalmente . materials and methods patient demographics a total of 32 patients ( median age 66.5 years , age range 5375 years ; median psa 9.2 , psa range 5.4715.7 ng / ml ) who underwent trus and mri followed by radical prostatectomy between january 2004 and july 2005 were included in this study . 
colour flow imaging was adjusted to the low - flow programme in every case ( threshold of velocity detection , 2.3 cm / s ) , and the colour - doppler gain was set just below the colour noise threshold . 
 vascularity of hypoechoic nodules of the peripheral zone was evaluated by comparison with that of an adjacent or contralateral peripheral zone without using a grading systea hypoechoic image or an area with a subtle decrease in echo structure was considered hypervascular if it contained more vessels than the adjacent peripheral zone . 
as benign prostatic hyperplasia has a heterogeneous pattern and commonly contains hyperplastic nodules , colour - doppler sonography was not used to detect suspicious abnormalities originating in the transition zone . magnetic resonance imaging prostate imaging was performed using a 1.5 - tesla ( t ) siemens scanner ( magnetom symphony maestro ; siemens medical solutions , erlangen , germany ) with a combined phased - array coil and endorectal coil ( mrinnervu ; medrad , indianola , ia , usa )  . 
the following pulse sequences were used : axial fast spin echo ( fse ) : turbo factor 23 , rotation time ( tr ) 4 , 400 ms , echo time ( te ) 119 ms , slice thickness 3 mm , field of view ( fov ) 180 mm , gap 0.8 mm , matrix 230256 coronal fse : turbo factor 25 , tr 3 , 070 ms , te 107 ms , slice thickness 3 mm , fov 180 mm , gap 0.8 mm , matrix 256256 sagittal fse : turbo factor 25 , tr 4 , 820 ms , te 112 ms , slice thickness 3 mm , fov 180 mm , gap 0.8 mm , matrix 224320 axial t1 fse : turbo factor 3 , tr 619 ms , te 11 ms , slice thickness 3 mm , fov 180 mm , gap 0.8 mm , matrix 230256 pathologic evaluation all patients underwent radical retropubic prostatectomy within 2 weeks from imaging assessment . 
the remainder of the gland was serially sliced from the apex to the base at 3to 4 - mm intervals , and slices were submitted for paraffin la vascolarizzazione dei noduli ipoecogeni localizzati nella porzione ghiandolare periferica stata confrontata con quella della porzione ghiandolare periferica adiacente o controlaterale , senza utilizzare nessun sistema di classificazione . unimmagine ipoecogena o unarea con ecostruttura modicamente ipoecogena veniva considerata ipervascolarizzata se presentava pi vasi rispetto alla zona periferica adiacente . al contrario un nodulo ipoecogeno era considerato ipovascolarizzato se il numero dei vasi era simile o minore a quello della zona periferica adiacente . 
inoltre , anche se lecografia transrettale convenzionale non evidenziava nessuna anomalia , il color - doppler veniva comunque utilizzato per valutare la presenza di eventuali aree della zona periferica a maggior vascolarizzazione . 
poich liperplasia prostatica benigna ha una struttura eterogenea e comunemente contiene noduli iperplastici , il color - doppler non stato utilizzato per la ricerca di zone sospette poste nella zona di transizione . gli esami di rm sono stati eseguiti con un magnete da 1 , 5 t siemens ( magnetom symphony maestro , siemens medical solutions , erlangen , germania ) , mediante uso combinato della bobina phased - array ed endorettale ( mrinnervu , medrad , indianola , usa )  . 
il palloncino della bobina endorettale stato sempre gonfiato utilizzando circa 40 cm3 di aria e successivamente tirato delicatamente indietro per garantire la completa copertura della prostata , dallapice sino alla base . 
poich il sanguinamento post - bioptico pu dunque rendere difficoltoso lo studio di rm ponendo un limite alla diagnosi di carcinoma prostatico , nei casi in cui il paziente avesse eseguito la biopsia prima dellesame rm , lindagine veniva condotta dopo un periodo di tempo minimo di almeno 4 settimane dalla esecuzione della biopsia stessa . 
per tutti i pazienti sono state sempre utilizzate le seguenti sequenze rm : fse sul piano assiale : turbo factor 23 , tr 4400 ms , te 119 ms , spessore di fetta 3 mm , fov 180 mm , gap 0 , 8 mm , matrice 230256 ; fse sul piano coronale : turbo factor 25 , tr 3070 ms , te 107 ms , spessore di fetta 3 mm , fov 180 mm , gap 0 , 8 mm , matrice 256256 ; fse sul piano sagittale : turbo factor 25 , tr 4820 ms , te 112 ms , spessore di fetta 3 mm , fov 180 mm , gap 0 , 8 mm , matrice 224320 ; fse - t1 sul piano assiale : turbo factor 3 , tr 619 ms , te 11 ms , spessore di fetta 3 mm , fov 180 mm , gap 0 , 8 mm , matrice 230256 . anatomia patologica tutti i pazienti sono stati sottoposti a prostatectomia radicale retropubica dopo circa due settimane dalla valutazione strumentale . 
la parte rimanente della ghiandola stata invece tagliata in fette da 34 mm dalla base allapice e le sezioni ottenute sono state messe in paraffina . le vescicole seminali sono state sezionate e trattate separatamente . 
after paraffin embedding , microslices were placed on glass slides and stained with hematoxylin and eos at pathologic analysis , a gleason score was assigned according to the current protocol at our institution . 
the whole mounts were then digitised using a high - resolution scanner : these constituted the tumour maps . as surgical removal and fixation can result in deformation of the gland , and as it is impossible to section identical planes with the two techniques , an exact correspondence between pathologic slices and mr sections was not expected . 
the most closely corresponding transverse t2 - weighted images and pathologic step - section slices were paired on the basis of the following anatomic landmarks : ( a ) the presence of urinary bladder and seminal vesicle tissue in superior slices , ( b ) the slice with the largest diameter and progressive changes in slice diameter , ( c ) the slice where the ejaculatory ducts enter the veru montanum , ( d ) the anteriorposterior and left - right position of the ejaculatory ducts and urethra and the shape of the urethra , ( e ) the thickness of the peripheral zone and the position of the pseudocapsule and ( f ) the presence , size , and shape of the transition zone . 
the precision of matching in the superior - inferior direction was estimated as being within one transverse slice ( 3 mm )  . data analysis trus and mr images as well as the digitised whole - mount axial pathological sections were transferred to a graphic workstation to perform image fusion . 
in three cases , image fusion was not possible , as geometrical distortion prevented reliable registration between the three data sets , and in four cases only , sagittal colour - doppler trus images were available . 
sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) were calculated by carefully analysing the fusion images in which the pathological section served as gold standard for assessing the staging obtained by trus alone , by mri alone and by the combination of mri and trus . results step - section histopathology demonstrated stage pt2b in four patients , pt2c in 14 patients , pt3a in three patients and pt3b in four patients . 
il vetrino stato successivamente digitalizzato con uno scanner ad alta risoluzione . poich la rimozione chirurgica e la fissazione possono determinare una deformazione della ghiandola e poich non possibile ottenere gli stessi piani di sezione della rm , non c stata unesatta corrispondenza tra le sezioni istologiche ed i piani acquisiti con la rm . 
la corrispondenza lungo lasse cranio - caudale delle immagini sottoposte a fusione stata stimata essere nellordine dello spessore di una fetta assiale ( 3 mm )  . analisi dei dati le immagini della trus , di rm e quelle digitalizzate dalle sezioni istopatologiche sono state successivamente inviate ad una workstation grafica al fine di eseguirne una loro fusione , tecnicamente possibile in 25 / 32 casi . 
infatti , mentre in 3 casi ci non stato possibile per la presenza di distorsioni geometriche che hanno impedito una accurata sovrapposizione delle immagini stesse , in 4 casi la sola disponibilit delle immagini sagittali di trus color - doppler ha impedito la fusione con le sezioni istopatologiche , ovviamente presenti solo sul piano assiale . 
la sensibilit , la specificit , il valore predittivo positivo ( vpp ) ed il valore predittivo negativo ( vpn ) sono stati calcolati analizzando attentamente la fusione delle immagini , nelle quali la sezione istopatologica serviva come gold standard per determinare la stadiazione ottenuta con la sola trus , con la sola rm e dalla combinazione di entrambe queste metodiche . risultati le sezioni istopatologiche hanno evidenziato uno stadio pt2b in 4 pazienti , pt2c in 14 pazienti , pt3a in 3 pazienti , pt3b in 4 pazienti . 
la correlazione tra trus e sezioni istopatologiche ha dimostrato che la trus aveva consentito una corretta stadiazione in 20 / 25 casi ( accuratezza 80% , sensibilit 29% , specificit 100% , vpp 100% , vpn 78% )  . 
la correlazione tra rm e sezioni istopatologiche ha dimostrato che la rm aveva consentito una corretta stadiazione in 22 / 25 casi ( accuratezza 88% , sensibilit 64% , specificit 100% , vpp 100% , vpn 84% )  . 
image fusion between mri and pathological sections showed that mri allowed correct staging in 22 / 25 cases ( accuracy 88% , sensitivity 64% , specificity 100% , ppv 100% , npv 84% )  . 
image fusion between trus , mri and pathological sections proved that trus and mri allowed correct staging in 23 / 25 cases ( accuracy 92% , sensitivity 71% , specificity 100% , ppv 100% , npv 90% )  . 
the three types of image fusion produced the results summarised in table 1 . discussion as nonpalpable prostatic cancers ( stage t1c ) originating in the peripheral zone have increased the use of trus - guided biopsies , we evaluated how useful it was to correlate trus ( grayscale and colour - doppler mode ) with endorectal mri , or rather , whether the fusion of images coming from these two techniques could improve diagnosis . 
unfortunately , radical prostatectomy specimens have shown that 30%51% of diazione in 23 / 25 casi ( accuratezza 92% , sensibilit 71% , specificit 100% , vpp 100% , vpn 90% )  . 
i risultati dei tre tipi di fusione sono riportati nella tabella 1 . discussione poich i tumori prostatici non palpabili della zona periferica ( stadio t1c ) hanno portato ad un uso sempre maggiore della biopsia trans - rettale eco - guidata , noi abbiamo valutato quanto possa essere utile correlare la trus ( convenzionale e color - doppler ) con la rm ed in particolare , se la fusione delle immagini appartenenti a queste due metodiche , potesse agevolare la nostra diagnosi . 
la prima la sua nota dipendenza dalloperatore , seguita dalla presenza di un limitato campo di vista , il quale oltre a non consentire una completa valutazione di tutta la struttura ghiandolare , come sua diretta conseguenza , c . 
section 20 / 25 22 / 25 23 / 25 tabella 1 confronto di tre tipi di fusione dimmagini tra color - doppler trans - rettale ( trus ) , risonanza magnetica ( rm ) e sezioni istopatologiche ( macrosezioni ) fusione di immagini pazienti , n sensibilit , % specificit , % accuratezza , % trus + macrosezioni rm + macrosezioni rm + trus + macrosezioni 20 / 25 22 / 25 23 / 25 these nonpalpable tumours display no abnormalities on trus [ 5 ]  . 
the first important and well - known limit is the strict operator dependence of trus , followed by its small fov , which does not allow depiction of nearby prostate structures , and its poor sensitivity for capsular irregularities . 
moreover , the anterior location ( transition zone ) of t1c - stage tumours reduces the diagnostic value because it is well established that trus is of limited value for revealing transitional - zone cancer [ 6 ]  . the use of colour - doppler ultrasound ( us ) does not substantially improve the accuracy of grayscale us . 
although it can improve the visibility of subtle nonpalpable grayscale abnormalities in a minority of cases , it fails to detect strictly isoechoic nonpalpable tumours , probably for reasons similar to those mentioned for grayscale trus . 
however , colourdoppler trus may add only minor information and , in particular , it seems to be superior to trus in two circumstances : the first is the significantly greater rate of high gleason grades in hypervascular tumours [ 7 ] ; the second is the better detection of tumours smaller than 3 mm , which are best resolved with colour - doppler mode . mri , performed with the combined use of phased - array and endorectal coils , provides a large fov with high spatial resolution , optimising local and distant staging of prostate carcinoma during a single mri session . 
for tumour ( t ) staging , the accuracy of endorectal coils is > 90% , also thanks to the added diagnostic value of phased - array coils that allows evaluation of nodal involvement ( n ) and detailed imaging of all anatomical structures above the pelvic floor [ 818 ]  . thus , if grayscale trus and colour - doppler trus may differentiate low - risk , nonpalpable prostate tumours which are hypovascular ( and invisible in 90% of cases ) from high - risk carcinomas ( t2 stage ) which are visible and hypervascular mri is superior because it is more sensitive and more specific in detecting all possible signal changes , ranging from small tumoural foci to coarser lesions associated or unassociated with extraprostatic tumour spread . 
inoltre , poich la trus difficilmente riesce a rilevare piccole lesioni , queste vengono spesso misconosciute ; infine la localizzazione anteriore ( zona di transizione ) dei tumori prostatici allo stadio t1c , riduce la capacit diagnostica della trus stessa , per la sua nota difficolt nellidentificare una neoplasia localizzata nella zona di transizione [ 6 ]  . luso del color - doppler non migliora laccuratezza dellecografia convenzionale in modo significativo . 
sembra comuqnue che in una minoranza di casi il suo utilizzo possa migliorare la visualizzazione di piccole alterazioni non palpabili ; tuttavia la trus color - doppler non riesce a delimitare con precisione le lesioni isoecogene non palpabili , probabilmente per le stesse ragioni descritte per la trus convenzionale . 
comunque , nonostante la trus color - doppler aggiunga solo informazioni secondarie sembra che sia comunque superiore alla trus convenzionale in due circostanze : la prima nel rilevare tumori ipervascolarizzati con gleason elevato [ 7 ] ; la seconda per la sua superiorit nellidentificare neoplasie di dimensioni inferiori ai 3 mm , meglio apprezzate grazie allausilio del color - doppler . la rm , mediante luso combinato della bobina phasedarray ed endorettale , fornisce invece una visione panoramica ad alta risoluzione spaziale , permettendo una stadiazione locale e a distanza del carcinoma . 
per la stadiazione tumorale ( t ) , laccuratezza della bobina endorettale superiore al 90% anche grazie allutilizzo combinato della bobina phased - array , che permette di valutare non solo un eventuale coinvolgimento linfonodale ( n ) ma anche tutte le restanti strutture anatomiche della pelvi [ 818 ]  . cos , anche se la trus , convenzionale e color - doppler , pu discriminare i tumori prostatici non palpabili , ipovascolarizzati e a basso rischio ( non apprezzabili nel 90% dei casi ) dai carcinomi palpabili , ipervascolarizzati e ad alto rischio ( stadio t2 ) , la rm risulta essere una metodica nettamente superiore in quanto pi sensibile e specifica nel rilevare tutte le possibili alterazioni di segnale , dai piccoli focolai tumorali alle lesioni pi grossolane associate ad eventuali sconfinamenti extraghiandolari . 
 combined analysis by using fusion images obtained from colour - doppler trus and mr images improves tumour detection and staging . in this study , we performed an additional type of analysis : the fusion between preoperative images and whole - mount radical prostatectomy specimens after having digitised the latter by means of a high - end digitiser . 
such image fusion allows immediate and intuitive assessment of the capabilities of trus , mri and fused trus and mri data in delineating local tumour extent by providing direct comparison with whole - mount prostatectomy specimens . 
tale fusione permette unimmediata ed intuitiva valutazione delle capacit della trus , della rm e delle immagini sovrapposte delle due metodiche nel delineare lestensione locale del tumore grazie al confronto diretto con le macrosezioni anatomo - patologiche ottenute dal pezzo chirurgico . conclusioni il nostro studio conferma in maniera indiscutibile lelevata attendibilit della rm come strumento diagnostico nella stadiazione del carcinoma prostatico in fase pre - operatoria . 
infatti abbiamo rilevato , non solo una buona corrispondenza tra le alterazioni evidenziate con la rm , in quanto sempre presenti nelle sezioni istopatologiche , ma anche una loro precisa corrispondenza anatomica . 
la fusione delle immagini dimostra quindi come la trus color - doppler fornisca solo miglioramenti marginali nel definire una corretta stadiazione della patologia che invece viene sicuramente ottenuta con la rm 1 , 5 t condotta con bobina endorettale . 
radiologia , ospedale di cernusco s / n , azienda ospedaliera di melegnano , milano , italy 3divisione di epidemiologia e biostatistica , istituto europeo di oncologia , milano , italy 4istituto di scienze radiologiche , facolt di medicina e chirurgia , universit degli studi di milano correspondence to : m . 
our preliminary data show that ceus can be used to obtain more accurate measurements than conventional us for the follow - up of patients with metastases in fatty liver . key words contrast - enhanced ultrasound ultrasound contrast agent breast cancer liver metastasis riassunto obiettivo . 
i nostri dati preliminari mostrano come la ceus possa essere utilizzata per ottenere parametri pi accurati di quelli della us per il follow - up delle pazienti con metastasi in fegato steatosico . parole chiave ecografia con mezzo di contrasto mezzo di contrasto ecografico cancro della mammella metastasi epatiche p . 
in italy , approximately 33 , 000 women are diagnosed with breast cancer each year , and 300 , 000 women have been diagnosed in the past , almost half of them in the past 5 years . 
most women who develop breast cancer can be treated with conservative surgery and adjuvant therapy ( chemotherapy or hormone therapy or both , depending on the biological features of the tumour ) , which substantially reduce the incidence of recurrence and metastasis or control their evolution . breast cancer patients receiving hormone therapy or chemotherapy frequently develop liver steatosis . 
in europe , it is preferred to other , more sensitive modalities , such as multidetector computed tomography ( mdct ) and magnetic resonance imaging ( mri ) because of the relative invasiveness of mdct and the high cost and limited availability of mri [ 5 , 6 ]  . 
this difference may be minimal , especially in small lesions , preventing the operator from visualising thein addition , changes in normal hepatic structure related to metabolic disorders such as diffuse or focal steatosis may make it difficult to detect lesions and determine their nature and extent [ 7 ]  . the need to improve the diagnostic accuracy of us , especially in difficult conditions , as is fatty liver disease , has recently led to the diffusion of contrast - enhanced us ( ceus )  . preliminary studies have demonstrated that ceus is more accurate than conventional us in identifying and characterising focal hepatic lesions , in part because the sonographic contrast medium appears able to reduce the parenchymal heterogeneity resulting from steatosis [ 8 , 9 ]  . correct determination of focal lesion size is fundamental because comparison between preand post - treatment dimensions is the most commonly used method to evaluate treatment response [ 10 ]  . 
 the purpose of this prospective study was to assess the accuracy of ceus in determining the diameter of liver metastases in patients operated on for breast cancer who have developed fatty liver disease and to compare it with that of us using mdct as the reference standard . materials and methods case series we enrolled 12 consecutive patients with liver metastases from resected breast cancer who had been treated with chemotherapy and / or hormone therapy and had moderate or severe fatty liver disease on us [ 11 ] that made sonographic assessment and measurement of the lesions difficult . 
we exil carcinoma della mammella il tumore pi frequente nelle donne dei paesi occidentali ; in italia si ammalano ogni anno circa 33000 donne e vivono ormai 300000 donne che hanno avuto in passato una diagnosi di cancro della mammella , di cui quasi la met negli ultimi 5 anni . 
infatti il carcinoma della mammella ha una prognosi relativamente buona : in italia , circa l80% delle donne ammalatesi nella prima met degli anni novanta era viva a 5 anni dalla diagnosi . 
la maggior parte delle donne che si ammalano di tumore della mammella oggi pu essere curata con chirurgia conservativa e ricevere trattamenti adiuvanti ( chemioterapici e / o ormonoterapia , secondo le caratteristiche biologiche del tumore ) , che riducono sensibilmente lincidenza di recidive o metastasi o ne controllano levoluzione . le pazienti con carcinoma mammario , sottoposte a ormonoterapia o chemioterapia , sviluppano con una certa frequenza una steatosi epatica . 
diversi lavori hanno dimostrato una stretta correlazione tra queste terapie e linsorgenza di una steatosi non alcolica [ 13 ] , specie nelle donne in sovrappeso [ 4 ]  . 
lecografia ( us ) la metodica di pi largo impiego per lo studio del fegato nella stadiazione e nel follow up delle pazienti con carcinoma mammario e , soprattutto in europa , la si preferisce a metodiche dotate di maggiore sensibilit quali la tomografia computerizzata multidetettore ( tcmd ) o la risonanza magnetica ( rm ) per la relativa invasivit della prima e lalto costo e la scarsa disponibilit della seconda [ 5 , 6 ]  . 
inoltre lalterazione della normale struttura epatica determinata da disordini metabolici quali la steatosi diffusa o focale , pu generare difficolt nellindividuare le lesioni e nel determinarne la natura e lestensione [ 7 ]  . la necessit di migliorare laccuratezza diagnostica dellus , particolarmente nelle condizioni difficili , come ad esempio nel fegato steatosico , ha visto di recente diffondersi lecografia con mezzo di contrasto ( ceus )  . 
studi preliminari hanno messo in evidenza una maggior accuratezza diagnostica della ceus nei confronti della us , sia nellindividuazione , sia nella caratterizzazione delle lesioni focali epatiche , anche perch il mezzo di contrasto ecografico sembra in grado di ridurre la disomogeneit parenchimale dovuta alla steatosi [ 8 , 9 ]  . la corretta determinazione delle dimensioni delle lesioni focali di fondamentale importanza se si considera che il confronto tra le dimensioni pree post - trattamento il metodo pi usato per la valutazione della risposta alla terapia farmacologia [ 10 ]  . questo studio prospettico si propone di valutare laccuratezza della ceus nel definire il diametro delle metastasi epatiche in pazienti operate per carcinoma mammario che abbiano sviluppato una steatosi epatica e di paragonarla p . 
for the purposes of the study , we focused on lesions whose topographic characteristics on initial us would ensure easy identification at the following diagnostic studies ( ceus and mdct )  . 
all patients were informed of the aims of the study and provided written informed consent for the use of contrast media . ultrasound the study was done with digital us scanners equipped with dedicated software for low - mechanical - index studies ( sequoia , siemens medical solutions , mountain view , ca , usa and logiq 500 , ge medical systems , milwaukee , wi , usa ) and 3 to 5 mhz transducers . 
the study was done at baseline and after injection of 2 ml / kg of iodinated contrast medium ( iomeron 300 , bracco imaging ) at a rate of 4 ml / s , followed by 40 ml saline solution at a rate of 4 ml / s in the arterial ( 30 s ) , portal ( 7080 s ) and late phase ( 180 s )  . scans were acquired with a collimation of 20 mm , slice thickness of 5 mm , pitch 1.75 , and table feed of 35 mm / rotation . 
 assessment criteria up to a maximum of three liver lesions per patient were measured with electronic callipers on the us , ceus and mdct images considering the largest diameter , in accordance with the response evaluation criteria in solid tumors ( recist ) criteria [ 12 ]  . 
 con quella di us , utilizzando la tcmd come metodica di riferimento . materiali e metodi casistica sono state arruolate nello studio 12 pazienti consecutive con metastasi epatiche da carcinoma mammario operato , che hanno eseguito trattamento medico sistemico con chemioterapia e / o ormonoterapia e con presenza di steatosi epatica di grado moderato o severo allus [ 11 ] , tale da rendere difficoltosa la valutazione ecografica e la misurazione delle lesioni . sono state escluse pazienti con performance status compromesso [ 45 ] , con ascite tale da ostacolare lindagine us e con controindicazioni al mdc ecografico o organoiodato . tutte le pazienti sono state sottoposte a us , ceus e tcmd . per gli scopi dello studio sono state identificate quelle lesioni che , al primo esame ecografico , presentavano caratteristiche topografiche tali da essere facilmente identificabili ai successivi esami diagnostici ( ceus e tcmd )  . 
tutte le pazienti sono state informate dello scopo dello studio e hanno sottoscritto i moduli specifici per la somministrazione dei mezzi di contrasto . ecografia lo studio si avvalso di ecografi digitali dotati di software dedicato ad esami con basso indice meccanico : sequoia ( siemens , medical solutions , view , ca , usa ) e logiq 500 ( ge , medical system , milwaukee , wi , usa ) , con sonde di frequenza variabile da 3 a 5 mhz . 
il mezzo di contrasto utilizzato stato il sonovue ( bracco imaging , milano , italia )  . la valutazione ecografica stata eseguita in condizioni basali e dopo iniezione endovenosa di mdc in bolo di 2 , 4 ml seguito da circa 5 ml di soluzione fisiologica . 
la ceus stata eseguita in imaging continuo a basso indice meccanico con scansioni panoramiche e mirate sulla lesione principale . sono state analizzate tre fasi distinte della perfusione epatica : fase arteriosa ( 1530 s dopo liniezione ) , fase portale ( 3060 s ) e fase tardiva ( da 60 s fino alla perdita delle microbolle : 240360 s )  . tc multidetettore results we studied 25 focal lesions in 12 subjects ( mean : 2.2 lesions per patient )  . 
lesame stato effettuato in condizioni basali e dopo iniezione endovenosa di 2 ml / kg di mdc organo - iodato ( iomeron300 , bracco imaging ) , con flusso di 4 ml / s seguito da 40 ml di soluzione fisiologica con flusso di 4 ml / s , nelle fasi arteriosa parenchimale ( 30 s ) , portale ( 7080 s ) e tardiva ( 180 s )  . 
comparison of us and ceus results shows that in five cases , the use of sonographic contrast medium enabled measurement of lesions that were confirmed on mdct but poorly defined on us because of marked steatosis . 
although not recommended in study protocols for evaluating results [ 12 ] , us is widely used in routine clinical practice owing to its lower economic and biological cost compared with that of mdct and mri . 
detection and accurate measurement of secondary lesions before and after treatment , which guides the clinicians decision to confirm or change treatment strategy , is therefore crucial not only for mdct and mri , but also for us . 
 use of sonovue , a second - generation contrast agent , has shown that ceus is significantly more accurate than conventional us in detection and characterisation of hepatic lesions [ 8 , 15 ]  . 
the microbubbles of second - generation contrast agents persist in the vessels up to 360 s , allowing plenty of time for a detailed study of the entire organ and depiction of secondary lesions , which are visualised in the late phase ( 60360 s ) when the surrounding parenchyma becomes homogeneous . 
sonovue proved to be well tolerated and free of side effects , in agreement with the literature [ 16 ]  . compared with conventional us , use of sonographic contrast medium allowed us to obtain measurements that were closer to those demonstrated by mdct . 
the lack of homogeneity of fatty liver also produced diagnostic doubt between a skip area and a secondary lesion ; in this case , ceus provided the correct diagnosis by demonstrating the homogeneous vascularity and echogenicity of the liver parenchyma [ 17 ]  . 
le misurazioni rilevate con us , ceus e tcmd sono state analizzate con il metodo di altmanbland [ 13 , 14 ]  . risultati sono state studiate 25 lesioni focali in 12 soggetti , con una media di 2 , 2 lesioni per paziente . 
i diametri delle lesioni misurate con us e confrontati con i valori di riferimento ottenuti con tcmd sono riportati in figura 3 . la ceus ha consentito di misurare tutte le 24 metastasi confermate dalla tcmd : i diametri misurati con ceus sono paragonati a quelli misurati con tcmd in figura 4 . 
paragonando i risultati ottenuti con us con quelli ottenuti con ceus , si osserva che in 5 casi il mezzo di contrasto ecografico ha permesso di misurare le lesioni che il grado marcato di steatosi rendeva mal definite allecografia convenzionale e confermate alla tcmd ; in un caso la lesione stata meglio definita allecografia basale ; in tre casi le misure ottenute con ecografia basale e quelle con ceus si sono equivalse . 
1a - c focal lesion in the viiviii hepatic segment , which was difficult to measure on ultrasound ( us ) images ( a ) but clearly defined by contrastenhanced us ( ceus ) ( b )  . 
1a - c lesione focale al settimo - ottavo segmento epatico , difficile da misurare con lecografia convenzionale ( a ) , ben parametrabile allecografia con mezzo di contrasto ( b )  . 
sebbene lecografia non sia un metodo consigliato per la valutazione dei risultati nei protocolli di studio [ 12 ] , di fatto ampiamente usata nella pratica clinica quotidiana per un minor costo , economico e biologico , rispetto alla mdtc o alla risonanza magnetica . 
anche con lecografia risulta pertanto determinante non solo lindividuazione , ma anche la precisa valutazione dimensionale delle lesioni secondarie pre e post trattamento che determina la decisione del clinico di confermare o cambiare la linea terapeutica . lutilizzo di un mezzo di contrasto ecografico di ii generazione , il sonovue , ha dimostrato come la ceus sia significativamente pi accurata dellecografia convenzionale nella diagnosi e nella caratterizzazione delle lesioni epatiche [ 8 , 15 ]  . 
lintroduzione dei mezzi di contrasto ecografici di seconda generazione permette una persistenza delle microbolle allinterno dei vasi fino a 360 s , e fornisce perci il tempo necessario per una valutazione approfondita di tutto lorgano , considerando che le lesioni secondarie si evidenziano meglio nella fase tardiva ( da 60 a 360 s ) con lomogeneizzazione del parenchima circostante . 
il sonovue si dimostrato ben tollerato ed , in accordo con i dati riportati in letteratura [ 16 ] , non abbiamo osservato alcun effetto collaterale . lutilizzo del mezzo di contrasto ecografico ha permesso di ottenere misure delle lesioni pi simili a quelle ottenute con la tcmd , rispetto a quelle definite con lecografia convenzionale . 
la disomogeneit del fegato interessato dalla steatosi ha creato anche un dubbio diagnostico tra una skip area ed una lesione ripetitiva ; in questo caso la ceus ha permesso di formulare la diagnosi corretta dimostrando la vascolarizzazione e lecogenicit omogenea del parenchima epatico [ 17 ]  . 
nella nostra casistica lutilizzo di mdc ecografico ha permesso di parametrare 5 lesioni ( il 20 , 8% delle metastasi considerate ) che con ecografia convenzionale erano solo intuibili a causa del marcato grado di steatosi ; inoltre ha permesso di riconoscere un falso positivo . 
le 5 lesioni non misurabili con us non avevano dimensioni inferiori alle altre ( range : 1577 mm rispetto a 1183 mm dellintera casistica ) , ma probabile che sia stata proprio la steatosi ad ostacolare lecografia convenzionale . 
the five lesions that could not be measured with us were no smaller than the others ( range : 1577 mm compared with 1183 mm ) , but it is likely that steatosis prevented detection on conventional us . comparison between us and ceus showed that by enhancing the contrast between the lesion and surrounding tissue , sonovue provides better visualisation and definition of lesion contours and consequently more accurate measurement . 
 the availability of a reliable method for measuring secondary lesions is all the more important if we consider the recent attempts made to provide oncological imaging professionals with guidelines and protocols to standardise assessment criteria across different settings [ world health organization ( who ) [ 18 ] and recist [ 11 ] ]  . 
this appears to justify endeavours to identify a modality that is not only able la possibilit di avere a disposizione una metodica affidabile nella misurazione delle lesioni secondarie appare sempre pi importante se si pensa come negli ultimi anni si sia cercato di fornire agli operatori che si occupano di imaging oncologico , linee guida e protocolli quanto pi uniformabili ai diversi ambienti ( criteri world health organization who [ 18 ] e criteri response evalutation criteria solid tumors recist [ 11 ] )  . 
sembra quindi giustificato lo sforzo di cercare una metodica che valuti la risposta alla terapia oncologica in modo accurato , ma anche quanto pi possibile accessibile ed accettabile da parte del paziente , che necessariamente dovr sottoporsi a controlli ravvicinati nel tempo . 
la tcmd conferma la morfologia e le dimensioni rilevate dallecografia con mezzo di contrasto ( c )  . to accurately evaluate treatment response but is also accessible and acceptable to patients , who will necessarily have to undergo close follow - up examinations . 
although according to protocols mdct remains the gold standard for evaluation of solid hepatic lesions , it should be noted that these guidelines do not take into account radiation protection issues or the patients age [ 19 ]  . 
despite a slight increase in costs and in view of the increasing diffusion of scanners with contrast - specific software , ceus is a safe and accurate method for evaluation of treatment response to secondary hepatic lesions , particularly in the presence of structural alterations of the liver parenchyma such as steatosis . non tengono presente alcun criterio radioprotezionistico , neppure in considerazione dellet della paziente [ 19 ]  . lutilizzo del mdc non modifica le caratteristiche dellindagine ecografica , e cio la rapidit di esecuzione , il basso costo , la non invasivit e la buona accettabilit da parte delle pazienti . 
power doppler ultrasound ( us ) with time - intensity curves was used to study renal graft function both in the absence of disease and with complications ( acute tubular necrosis and chronic rejection ) in an attempt to identify pathognomonic patterns . 
fifty - six asymptomatic renal transplant patients ( 36 men and 20 women ) , 19 of whom had altered creatinine clearance levels , were studied by power doppler us with time - intensity curves followed by biopsy . 
although confirmation by a larger series is required , our findings appear to indicate pathognomonic patterns in patients with chronic rejection and acute tubular necrosis . key words ultrasound power doppler us contrast agent kidney transplantation chronic rejection acute tubular necrosis riassunto obiettivo . 
in questo lavoro stato utilizzato il power doppler con le curve intensit / tempo per lo studio della funzionalit del rene trapiantato in assenza di malattia e con complicanze ( necrosi tubulare acuta e rigetto cronico ) , al fine di individuare pattern patognomonici . 
cinquantasei pazienti con rene trapiantato , 36 maschi e 20 femmine , con assenza di sintomi e affetti da alterati livelli di clearance della creatinina , sono stati studiati con il power doppler con le curve intensit / tempo e successivamente sottoposti ad esame bioptico . 
sono stati individuati tre gruppi di pazienti in base ai dati emersi dallo studio delle curve i / t : gruppo a : 27 pazienti presentavano curve con picco massimo di intensit raggiunto dopo un tempo compreso tra 5065 secondi dalla somministrazione ev del mdc . 
i dati ottenuti dalle curve hanno mostrato significative variazioni a seconda delle condizioni del rene ( assenza di malattia , rigetto cronico , necrosi tubulare acuta )  . i risultati ottenuti potrebbero rappresentare , a nostro giudizio , pattern patognomonici nei pazienti con rigetto cronico e necrosi tubulare acuta ; tali dati devono essere naturalmente confermati su pi ampia casistica . parole chiave ecografia power doppler mezzo di contrasto rene trapiantato rigetto cronico necrosi tubulare acuta r . 
the use of sonographic contrast material has further improved the study of graft vascularity [ 58 ] ; in particular , the study of the peripheral vasculature and intraparenchymal arteries provides important information on complications , above all in the case of chronic renal failure , chronic rejection and acute tubular necrosis [ 9 ]  . the most interesting and promising recent development in regards to us appears to be the use of sonographic contrast material to plot contrast - distribution curves known as time - intensity curves [ 1012 ]  . 
following intravenous administration of contrast material , graphs are plotted that express signal intensity values , or contrast material concentration , in the structure being examined ; this enables the study of enhancement patterns and provides important functional information for the diagnosis . 
the transplanted kidney is well suited to this type of investigation given its superficial position and the fact that it is barely affected by respiratory motion conditions that facilitate sonographic evaluation . 
the method has already been successfully used in the study of other organs [ 1618 ]  . we studied the transplanted kidney using power doppler us with time - intensity curves as well as duplex doppler us to measure the resistive index ( ri ) and correlated the results with the biopsy findings to identify pathognomonic patterns for the differential diagnosis of the complications associated with renal transplant . 
 il color e power doppler , grazie alla capacit di studiare accuratamente la vascolarizzazione renale , possono fornire numerose informazioni sul rene trapiantato [ 1 , 2 ] e le principali complicanze del trapianto [ 3 ]  . 
lutilizzo del mdc ecografico ha permesso un ulteriore progresso nello studio della vascolarizzazione del rene trapiantato [ 58 ] ; in particolare lo studio della vascolarizzazione periferica e delle arterie intra - parenchimali fornisce importanti informazioni sulle complicanze del trapianto specialmente nel caso dellinsufficienza renale cronica , rigetto cronico e necrosi tubulare acuta [ 9 ]  . recentemente lo sviluppo pi interessante e promettente dellecografia sembra essere rappresentato dallutilizzo del mdc ecografico per la determinazione delle curve di distribuzione del mdc conosciute come le curve intensit / tempo [ 1012 ]  . 
dopo aver somministrato per via ev il mdc si ottengono dei grafici che esprimono i valori di intensit di segnale provenienti dalla struttura in esame relativi alla concentrazione del mdc ; in questo modo possibile studiare la dinamica di enhancement ed avere importanti informazioni di tipo funzionale per la diagnosi . 
il rene trapiantato si presta bene a questo tipo di indagine per la sua collocazione superficiale e la scarsa mobilit con gli atti del respiro , condizioni che favoriscono lo studio ecografico . 
in dettaglio : 37 dei 56 pazienti erano asintomatici e non presentavano alterazioni degli esami di laboratorio ; 10 dei pazienti asintomatici sono stati assunti come gruppo di controllo . dopo compilazione del consenso informato tutti i pazienti sono stati sottoposti ad esame con power doppler con mdc per la determinazione delle curve intensit / tempo ( i / t ) per lo studio della dinamica di enhancement del rene trapiantato e ad esame duplex doppler per la misurazione degli indici di resistenza . 
 stato utilizzato un apparecchio ecografico idea 5 ( esaote biomedica , genova , italia ) equipaggiato con un software brevettato dallesaote per la realizzazione delle curve intensit / tempo ; stata utilizzata una sonda convex da 3 , 5 mhz con una frequenza di ripetizione degli impulsi ( prf ) di 1 , 2 khz per lesecuzione delle curve i / t e la r . 
to sample the curves time and signal - intensity values , we placed the reference line at the beginning of enhancement and at the maximal enhancement peak using the cursor . 
enhancement beginning and maximal enhancement peak values were calculated during postprocessing according to the following criteria : beginning enhancement value was sampled on the x - axis at the point where the time / intensity curve began to rise , that is , when signal intensity began to increase as a result of the arrival of the contrast material in the renal vessels the maximal enhancement peak value was sampled on the y - axis at the point where the curve reached its maximum height and which corresponded to the highest concentration of contrast material and therefore to maximum signal intensity . we therefore considered the following parameters : time to enhancement beginning time to enhancement peak . the ri was measured in the renal artery and interlobar arteries of the upper and lower pole and the middle third of the kidney . 
the same examiner performed all examinations , and all patients subsequently underwent biopsy of the renal graft . results on the basis of beginning enhancement and peak enhancement values derived from the time - intensity curves , we identified three groups of patients in addition to the control group . 
per campionare i valori di tempo e di intensit delle curve stata posizionata , con il cursore , la linea di riferimento allinizio dellenhancement e nel picco di massima intensit del segnale ; in dettaglio il valore di inizio enhancement e di raggiungimento del picco massimo di intensit sono stati calcolati in post - processing secondo i seguenti criteri : il valore di inizio enhancement stato campionato nellasse delle ascisse nel punto in cui la curva intensit / tempo si impenna e cio quando il valore dellintensit del segnale comincia ad aumentare in rapporto allingresso del mdc nei vasi renali ; il valore di picco di intensit massima stato campionato nellasse delle ordinate nel punto in cui la curva raggiunge la massima altezza e che corrisponde alla massima concentrazione e quindi al valore massimo di intensit del segnale . sono stati quindi presi in considerazione i seguenti parametri : tempo di inizio enhancement ; tempo di raggiungimento del picco massimo di intensit del segnale . gli indici di resistenza sono stati misurati nellarteria renale , nelle interlobari del polo superiore , inferiore e del terzo medio del rene . 
i valori degli indici di resistenza erano compresi tra 0 , 73 e 0 , 79 . gruppo c : tre pazienti , con valori di clearance della creatinina compresi tra 3260 ml / min , presentavano curve i / t con valori di inizio enhancement compresi tra 2530 r . 
i valori degli indici di resistenza erano compresi tra 0 , 68 e 0 , 74 . gruppo di controllo : i 10 pazienti selezionati , con valori di clearance della creatinina compresi tra 90112 ml / min , presentavano curve con inizio enhancement compreso tra 1525 secondi dalla somministrazione ev del mdc e picco massimo di intensit raggiunto dopo un tempo compreso tra 5065 secondi dalla somministrazione ev del mdc . 
i valori degli indici di resistenza erano compresi tra 0 , 62 e 0 , 68 . i dati degli ir rapportati alla clearance della creatinina sono riassunti nella tabella 1 . la misurazione degli ir , nei complessivi 56 pazienti , assumendo 0 , 70 come valore soglia ( < 0 , 70 assenza di malattia ; > 0 , 70 presenza di malattia ) , ha dimostrato 17 veri positivi , 31 veri negativi , 6 falsi positivi e 2 falsi negativi ( sensibilit 89% , specificit 83% , valore predittivo positivo 73% , valore predittivo negativo 93% )  . 
la curva intensit / tempo presenta rapido wash - in e rapido e wash - out . can be studied by diagnostic imaging techniques that provide direct or indirect information on the presence of disease . 
some routinely used methods , such as urography , computed tomography ( ct ) , magnetic resonance imaging ( mri ) and scintigraphy , have drawbacks related to the use of ionising radiation ( urography , ct ) or radioisotopes ( scintigraphy ) , and high cost ( ct , mri , scintigraphy )  . 
these changes generally translate into a reduction of renal perfusion that is directly proportional to disease severity [ 19 ]  . in our study , we used power doppler us for the advantages it offers compared with colour doppler us : less noise , and independence from the insonation angle and flow velocity [ 2022 ]  . 
the ability to demonstrate low - flow signals , such as those in the cortical region , has increased the methods potential to identify avascular areas ( infarction , acute pyelonephritis , etc . ) or areas with strongly impaired non si sono verificate reazioni dintolleranza al mdc ecografico . lesame bioptico non ha evidenziato malattia nei pazienti del gruppo a e del gruppo di controllo ; nei pazienti del gruppo b ha permesso diagnosi di rigetto cronico e nei pazienti del gruppo c diagnosi di necrosi tubulare acuta . discussione e conclusioni le patologie che possono provocare alterazioni della funzionalit e dellenhancement del parenchima renale sono numerose ; esse possono essere studiate con tecniche di diagnostica per immagini in grado di fornire informazioni dirette o indirette sullo stato della malattia . 
alcune di queste metodiche , utilizzate di routine , come lurografia , la tc , la rm e la scintigrafia , presentano alcuni svantaggi legati al rischio dellutilizzo di radiazioni ionizzanti ( urografia , tc ) o radioisotopi ( scintigrafia ) e inoltre sono gravate da costi elevati ( tc , rm , scintigrafia )  . 
 ri comparison between subjects without disease and those with disease ( acute or chronic rejection , acute tubular necrosis , cyclosporine toxicity , etc . ) generally provides an indication of disease presence but does not show significant differences among diseases and therefore does not allow a differential diagnosis [ 24 ]  . 
cut - off values between the groups were as follows : group a ( patients without disease ) : enhancement onset under 25 s and time to peak enhancement less than 65 s group b ( patients with chronic rejection ) : enhancement ai fini della diagnosi soprattutto grazie allo studio degli indici di resistenza dei vasi renali , legati ai cambiamenti che si verificano a livello della vascolarizzazione renale in corso di malattie ( vasculiti , alterazioni endoteliali , edema sub - intimale , ostruzione dei vasi ecc . ) ; tali cambiamenti si traducono generalmente in una riduzione del flusso renale , pi evidente quanto pi grave la malattia [ 19 ]  . nel nostro lavoro abbiamo utilizzato il power doppler per i vantaggi che offre rispetto al color doppler : riduzione del rumore , indipendenza dallangolo di insonazione e dalla velocit di flusso [ 2022 ]  . 
la capacit di dimostrare segnali a basso flusso come quelli della regione corticale renale ha , infatti , aumentato le potenzialit della metodica nellidentificazione daree avascolari ( infarti , pielonefriti acute ecc . ) o fortemente compromesse ( rigetto acuto , cronico , nefrotossicit da ciclosporina ecc . ) ; inoltre la correlazione con la rm ne ha evidenziato lelevata sensibilit nellidentificazione delle aree prive di flusso [ 23 ]  . 
nella nostra casistica tale metodica ha prontamente evidenziato riduzione della vascolarizzazione in quasi tutti i pazienti del gruppo b e c affetti da malattia ( fig . 4 ) , senza evidenziare , tuttavia , significative variazioni tra i due gruppi . lo studio comparativo degli indici di resistenza dei soggetti in assenza di malattia e dei soggetti con malattia ( rigetto acuto , cronico , necrosi tubulare acuta , tossicit da ciclosporina ecc . ) generalmente mette in evidenza la malattia , r . 
la curva intensit / tempo presenta lento wash - in e lento e wash - out . onset under 60 s and time to peak enhancement less than 235 s group c ( patients with acute tubular necrosis ) : enhancement onset under 30 s and time to peak enhancement less than 130 s . 
 biopsy demonstrated the presence of graft disease in all patients in group b ( n = 16 , chronic rejection ) and group c ( n = 3 , acute tubular necrosis )  . 
 on the basis of their greater sensitivity and specificity compared with ri measurements , time - intensity curves could , in our opinion , represent pathognomonic patterns in renal graft diseases and provide important information for the differential diagnosis . 
if confirmed by larger series , these data could open up new perspectives for the sonographic study of the kidney , both transplanted and native . ma non dimostra significative variazioni tra le suddette e quindi non ne permette la diagnosi differenziale [ 24 ]  . 
 curve i / t descrivono la dinamica di enhancement del rene ; infatti nei pazienti con assenza di malattia il mdc giunge rapidamente nel rene trapiantato , raggiungendo altrettanto rapidamente il picco dintensit per poi abbandonare il rene altrettanto rapidamente . 
nei reni con rc ( rigetto cronico ) e nta ( necrosi tubulare acuta ) il mdc raggiunge pi lentamente il picco di massima concentrazione e staziona pi a lungo nel rene . 
il lento raggiungimento della massima concentrazione del mdc e la ritenzione prolungata del mdc risultano quindi essere elementi legati allo stato di malattia del rene trapiantato e attribuibili quindi alla ridotta funzionalit del rene . 
 in base ai risultati ottenuti , maggiore sensibilit e specificit , rispetto alla misurazione degli indici di resistenza , le curve i / t potrebbero rappresentare , a nostro giudizio , dei pattern patognomonici nelle malattie del rene trapiantato e fornire inoltre importanti informazioni per la diagnosi differenziale delle complicanze . 
fortuna amirsys inc , salt lake city , utah ( 2005 ) isbn 1 - 4160 - 2333 - x ; isbn 0 - 8089 - 2324 - 2 ( international english edition ) in the online version of the book review unfortunately g . 
di radiodiagnostica , fondazione irccs policlinico san matteo , piazzale golgi , 19 , i - 27100 pavia radiol med ( 2007 ) 112 : 145146 doi 10.1007 / s11547 - 007 - 0129 - 5 geriatric radiology radiologia geriatrica springer - verlag italia , ( 2006 ) isbn 88 - 470 - 0485 - 3 published online : 22 february 2007 g . 
cammarota the ageing , with declining birth rates and increasing numbers of elderly individuals not only those over 65 but especially those in more advanced age groups has brought about a series of social , economic and healthcare problems . 
 with increasing frequency , doctors , whether specialists or not , are confronted with complex clinical scenarios arising in the same patient , which make management problematic and require special competences . 
over the past few years , advances in knowledge about the biology and physiology of ageing have made it possible to plan medical interventions that have the potential to slow down the functional decline that often accompanies old age and to prevent or delay the onset of disability or dependency that follow a state of disease . 
 with the use of multidimensional evaluation tools , geriatricians are able to analyse medical , physical and socioeconomic needs of elderly and especially frail elderly patients , plan personalised healthcare interventions and monitor their efficacy over time . 
multidimensional evaluation relies on the use of a variety of diagnostic methods , and healthcare professionals working as a team are able to provide the best diagnostic tests and treatment solutions for each patient and fully differentiate between physiology and pathology in the ageing process . in this context , radiology and more generally diagnostic imaging play a valuable role in the care of these patients . 
in elderly and especially geriatric patients , comorbidities , a rapidly changing clinical situation and physical and cognitive problems frequently make it difficult for radiologists to provide clinicians with the answers they expect . 
at this time of continuous technological progress , however , radiology provides not only the easy - to - perform diagnostic tests that are routinely used in the elderly , but also new imaging techniques that , if correctly applied , can be used to diagnose and monitor the evolution of disease states that are often difficult to manage clinically . 
negli ultimi anni il miglioramento delle conoscenze sulla biologia e la fisiologia dellinvecchiamento ha permesso di pianificare interventi potenzialmente in grado di rallentare il declino funzionale che spesso accompagna linvecchiamento e di prevenire o ritardare linsorgenza della disabilit e della dipendenza in seguito ad uno stato morboso . 
il geriatra , attualmente , utilizzando gli strumenti della valutazione multidimensionale , in grado di analizzare i bisogni di ordine medico , fisico , psichico e socio - economico del paziente anziano , in particolare dellanziano fragile , di programmare interventi personalizzati per il paziente e di controllarne nel tempo lefficacia . la valutazione multidimensionale si avvale di differenti metodologie diagnostiche e di numerosi operatori medici e non medici che , lavorando in maniera congiunta , riescono ad offrire le migliori soluzioni diagnostico - terapeutiche per il paziente ed a distinguere pienamente il limite tra il fisiologico e il patologico nel processo di invecchiamento . in questottica la radiologia , ed in genere la diagnostica per immagini , trova una giusta collocazione nella cura del paziente anziano . 
frequentemente in questo paziente , in particolare in quello geriatrico , a causa della comorbilit , di un quadro clinico che si modifica nel breve termine e di problemi di ordine fisico e cognitivo non facile ottenere dalla radiologia le risposte che il clinico si aspetta . 
la radiologia , oltre gli esami diagnostici di facile esecuzione utilizzati di routine anche nei pazienti anziani , in unepoca di continuo progresso tecnologico fornisce frequentemente nuove metodologie di indagine di cui anche il paziente anziano pu usufruire , se correttamente applicate , per la diagnosi e per seguire levoluzione nel tempo di un quadro morboso spesso di difficile gestione clinica . 
in molti casi una buona collaborazione tra geriatra e radiologo consente di scegliere lesame pi specifico per il singolo caso e di discutere insieme in caso di discordanze tra risultati di esami diagnostici e quadro clinico . 
 importante per il radiologo conoscere i quadri clinici pi frequenti presenti nel paziente anziano , spesso diversi da quello adulto , e per il geriatra apprendere le possibilit ed i limiti della moderna radiologia e le applicazioni nei suoi pazienti . 
ben venga dunque un testo di radiologia geriatrica scritto in prevalenza da radiologi , ma anche da alcuni geriatri nella parte introduttiva , dove book review applications in geriatric patients . 
geriatric radiology is therefore a much - need text , written for the most part by radiologists but also by some geriatricians who discuss the problems related to ageing in the introductory section . the book presents the imaging patterns of the most important body systems that undergo changes as a result of both physiological ageing processes and pathological processes that arise from or are complicated by ageing . 
besides offering in - depth descriptions with short sections on radiological anatomy and the clinical indications for the single examinations , the text is illustrated by images that make the process of learning and keeping up to date both easy and pleasant . geriatric radiology is an excellent reference book for geriatricians , radiologists , internists and for all those involved in treating the clinical problems of elderly individuals . vengono presi in esame i problemi legati allinvecchiamento . nel volume sono riportati i quadri radiologici e pi in generale di diagnostica per immagini dei pi importanti apparati che subiscono modificazioni sia per processi fisiologici di invecchiamento che a causa di patologie insorgenti o complicate in seguito allinvecchiamento . 
casella 7 , i - 90145 palermo , italy , tel . : + 39 - 091 - 6552330 , fax : + 39 - 091 - 6552337 , e - mail : sparacia@unipa.it received : 21 november 2005 / accepted : 30 march 2006 / published online : 22 february 2007 abstract purpose . 
images were continuously acquired at the basal ganglia over 40 s during injection of 90 ml of iodinated contrast medium injected at a rate of 9 ml / s with a 9 - s delay . 
z - axis coverage was 20 m all patients underwent diffusion - weighted magnetic resonance imaging ( dwi ) within 12 h of perfusion ct to define the extent of the infarct . 
perfusion ct data were analysed in regions of interests ( rois ) on regional cerebral blood volume ( rcbv ) , regional cerebral blood flow ( rcbf ) and mean transit time ( mtt ) maps placed in various parts of the perfusiondeficient territory and in the contralateral hemisphere . 
normal ct findings with abnormal ct perfusion parameters were seen in the region of infarction and in the viable tissue ( penumbra ) within a 1.5 - cm distance from the infarct margin as outlined on dwi images . 
le immagini sono state acquisite in modo continuo per una durata di 40 s attraverso la regione dei nuclei della base durante infusione di 90 ml di mdc non ionico ad una velocit di 9 ml / s con un ritardo di 9 s . 
lestensione lungo lasse z delle scansioni stata di 20 mtutti i pazienti sono stati sottoposti ad esame rm con sequenze pesate in diffusione ( dwi ) entro 12 ore dallesame tc di perfusione per delineare lestensione della lesione infartuale . 
i dati di perfusione cerebrale del flusso ematico cerebrale regionale ( rcbf ) , volume ematico cerebrale regionale ( rcbv ) e del tempo medio di transito ( mtt ) sono stati misurati con regioni di interesse ( roi ) posizionate in diverse aree di deficit perfusionale e nelle aree indenni corrispondenti dellemisfero cerebrale controlaterale . 
in tutti i pazienti lesame tc di base non dimostrava anomalie di densit da riferire a lesioni ischemiche in fase acuta mentre sono state rilevate anomalie dei parametri di perfusione cerebrale sia nelle regioni infartuate delineate nelle immagini dwi che nelle aree limitrofe ipoperfuse poste entro 1 , 5 cm di distanza dal margine del core lesionale ( dwi positiva )  . 
il prolungamento dellmtt stata lanomalia di perfusione pi frequentemente riscontrata nel tessuto ipoperfuso e nel tessuto infartuato con differenze significative ( p < 0 , 0001 ) rispetto i valori di mtt del tessuto sano . 
la media per i valori di mtt stata di 9 , 8 s nel core lesionale , 5 , 1 s nel tessuto ipoperfuso ( esterno al core lesionale ma entro 1 , 5 cm ) e 3 , 4 s nelle corrispondenti aree g . 
lanalisi delle curve roc ha dimostrato che il prolungamento dellmtt per valori superiori a 6 , 05 s consente di distinguere il tessuto infartuato con un valore predittivo positivo del 100% ( sensibilit = 84 , 6% ; specificit = 100% ; accuratezza = 92 , 3% ; p < 0 , 0001 )  . 
in selected patients , thrombolytic therapy , the intravenous administration of recombinant tissue - type plasminogen activator ( rtpa ) within 36 h of onset of neurological symptoms , is a valid treatment option to prevent disease progression and reduce the extent of disability [ 15 ]  . 
the rationale for this treatment is to restore cerebral perfusion through recanalisation in an attempt to salvage tissue in ischaemic penumbra , in other words , cerebral tissue in which perfusion values have not fallen below the viability threshold and therefore are not infarcted [ 3 ]  . 
as a consequence , discrimination of viable and ischaemic tissue using quantitative cerebral perfusion parameters measured by diagnostic imaging techniques is fundamental in selecting patients for thrombolytic therapy [ 3 , 4 , 610 ]  . 
 the cerebral perfusion threshold that defines irreversible tissue damage has been determined by positron emission tomography ( pet ) , which also provided a better understanding of the pathophysiology of brain ischaemia [ 7 , 8 ]  . 
cerebral perfusion has been assessed using nuclear medicine techniques , such as xenon - computed tomography ( ct ) , pet and single - photon emission tomography ( spect ) and diagnostic imaging methods , such as magnetic resonance imaging ( mri )  . 
however , the routine use of these techniques is hindered by the limited availability of equipment , high costs and difficulty performing the exams in uncooperative patients with acute cerebral ischaemia [ 6 , 7 , 10 ]  . in recent years , development of ct and especially multislice ct scanners has made available a study technique that nei paesi occidentali lischemia cerebrale rappresenta la terza causa di morte e la principale causa di disabilit nella popolazione adulta . 
la terapia trombolitica , basata sulla somministrazione endovena dellattivatore tissutale del plasminogeno ( recombinant tissue - type plasminogen activator : rtpa ) rappresenta , in pazienti selezionati , una opzione terapeutica valida entro le prime 36 ore dallinsorgenza dei sintomi neurologici per prevenire la progressione della malattia e ridurre il grado di disabilit [ 15 ]  . 
il ripristino dei valori di perfusione cerebrale conseguente alla ricanalizzazione rappresenta il razionale di questa terapia nel tentativo di salvare i tessuti in penombra ischemica , ovvero il tessuto cerebrale in cui i valori di perfusione cerebrale non sono scesi al disotto della soglia vitale e quindi in cui non si prodotta una lesione infartuale [ 3 ]  . 
conseguentemente , la possibilit di discriminare il tessuto cerebrale vitale da quello ischemico utilizzando parametri quantitativi di perfusione cerebrale misurati con tecniche di diagnostica per immagini fondamentale per selezionare i pazienti da sottoporre a terapia trombolitica [ 3 , 4 , 610 ]  . la soglia di perfusione cerebrale che definisce il danno tissutale irreversibile stata definita mediante studi di tomografia ad emissione di positroni ( pet ) che hanno consentito anche una migliore comprensione della fisiopatologia dellischemia cerebrale [ 7 , 8 ]  . 
tuttavia , per la sua limitata disponibilit e gli alti costi , la valutazione mediante pet non praticabile nei pazienti con ischemia cerebrale acuta , pertanto necessario identificare una tecnica di rapida esecuzione , ampiamente disponibile , che consenta di definire e quantificare il deficit di perfusione cerebrale . 
per la valutazione della perfusione cerebrale sono state utilizzate metodiche di medicina nucleare quali la xenon - tc , la pet e la tomografia ad emissione di fotone singolo ( spect ) , e metodiche di diagnostica per immagini , segnatamente la risonanza magnetica ( rm )  . 
perfusion ct , which is done during the infusion of a bolus of iodinated contrast medium , is particularly indicated in patients with acute ischaemia , as it is fast to perform and offers the possibility of ruling out haemorrhagic complications on the preliminary precontrast ct scan [ 10 , 11 ]  . 
time - concentration curves can be traced for a given region of interest ( roi ) , which reflect perfusion in that region , and the different cerebral perfusion parameters can be derived from their analysis . 
a mathematical operation , known as deconvolution of the arterial and tissue enhancement curves , allows calculation of mean transit time ( mtt ) of the contrast bolus from the arteries to the veins of the cerebral circulation . 
regional cerebral blood volume ( rcbv ) is calculated as the area under the curve ( auc ) of a parenchymal pixel divided by the auc of an arterial pixel . 
the theory underlying this technique is the central volume principle , which relates cbf , cbv and mtt in the following equation : cbf = cbv / mtt the aim of cerebral perfusion ct is therefore to identify tissue in ischaemic penumbra that is , viable tissue with reduced perfusion that can be salvaged with thrombolytic therapy initiated within the first 36 h of onset of neurological symptoms [ 1113 ]  . 
the reliability and reproducibility of perfusion parameter measurements provided by ct have been validated in the literature [ 14 , 15 ] , but controversies exist as to which parameter is best for discriminating between viable and infarcted tissue [ 16 ]  . 
 the aim of this study was to determine the haemodynamic parameters detected with perfusion ct in the infarct core and its periphery . materials and methods thirteen patients ( five men and eight women ; age range 4490 years , mean age 63.3 years ) with acute nonhaemorrhagic cerebral ischaemia in the territories of the middle ( n = 11 ) or anterior cerebral artery ( n = 2 ) were studied within 3 h of onset of neurological symptoms . 
cerebral perfusion images were obtained with a 4 - detector - row multislice spiral unit ( volume zoom ; siemens , erlangen , germany ) with scans through the basal ganglia perpendicularly to the occipital segment of the superior sagittal sinus , below the confluence of the sinuses , to visualise the lutilizzo nella pratica clinica di queste metodiche limitata dalla disponibilit delle apparecchiature , degli alti costi e dalla difficolt di eseguire lesame in pazienti non collaboranti affetti da ischemica cerebrale acuta [ 6 , 7 , 10 ]  . negli ultimi anni , grazie allevoluzione delle apparecchiature di tomografia computerizzata ( tc ) , in particolare con lintroduzione dei tomografi multistrato , stata sviluppata una tecnica di studio che consente la valutazione dei parametri di perfusione cerebrale mediante tc . 
lo studio tc di perfusione cerebrale , che si esegue durante infusione a bolo di mezzo di contrasto ( mdc ) iodato , risulta particolarmente indicato in pazienti con ischemia cerebrale acuta per la rapidit di esecuzione dellesame e per la possibilit di escludere le complicanze emorragiche allesame tc senza mdc che si esegue preliminarmente [ 10 , 11 ]  . 
la tc perfusionale una tecnica relativamente nuova che consente di rilevare le modificazioni di concentrazione del mdc iodato durante il transito del bolo attraverso le arterie cerebrali . possono quindi essere tracciate curve tempo - concentrazione per una data regione di interesse che riflettono la perfusione in quella data regione . 
attraverso un procedimento matematico noto come deconvoluzione delle curve di enhancement arterioso e tissutale si calcola il tempo medio di transito ( mtt ) del bolo di mdc nel passaggio dai vasi arteriosi del circolo cerebrale a quelli venosi . 
la teoria alla base di questa tecnica il principio del volume ematico centrale che mette in relazione il flusso ematico cerebrale ( cbf ) con il volume ematico cerebrale ( cbv ) e con il tempo medio di transito ( mtt ) nella seguente equazione : cbf = cbv / mtt lobiettivo dello studio tc di perfusione cerebrale quindi di identificare il tessuto in penombra ischemica , ovvero il tessuto vitale ma con ridotta perfusione , e dunque salvabile con terapia trombolitica attuata tempestivamente , entro le prime 36 ore dalla comparsa dei sintomi neurologici [ 1113 ]  . 
lattendibilit e la riproducibilit dei risultati relativi alla misurazione di parametri di perfusione cerebrale con tc perfusionale trova riscontro in letteratura [ 14 , 15 ] , tuttavia esistono controversie circa il parametro perfusionale da utilizzare per discriminare il tessuto vitale dal tessuto infartuato [ 16 ]  . scopo del presente lavoro di determinare i parametri emodinamici rilevati con tc perfusionale nel contesto del core lesionale ed alla sua periferia . materiali e metodi sono stati studiati 13 pazienti ( 5 maschi e 8 femmine di et compresa tra 44 e 90 anni , et media 63 , 3 anni ) affetti da ischemia cerebrale in fase acuta nel territorio di distribuzione dellarteria cerebrale media ( n = 11 ) o dellarteria cerebrale anteriore ( n = 2 ) , non complicata da emorragia , entro 3 ore dallinsorg . 
1a axial magnetic resonance ( mr ) diffusion weighted image ( dwi ) , and b calculation of perfusion computed tomography ( ct ) maps for regional cerebral blood flow ( rcbf ) , regional blood volume ( rcbv ) and mean transit time ( mtt ) in a patient with left thalamic stroke . 
1a immagine rm assiale pesata in diffusione ( dwi ) e b calcolo delle mappe di perfusione tc per i parametri rcbv , rcbf e mtt in un paziente affetto da ischemia cerebrale acuta in sede talamica sinistra . 
le immagini dwi sono state utilizzate per delineare le dimensioni finali dellarea infartuale ( core lesionale ) e tracciare sulle corrispondenti mappe di perfusione una roi entro una distanza di 1 , 5 cm dal margine del core lesionale ( per misurare i valori di perfusione nellarea peri - infartuale )  . three supratentorial vascular territories in a single scan . 
z - axis scan coverage was 20 m a 90 - ml bolus of nonionic contrast medium ( 320 mg / ml iodine concentration ) was injected into an antecubital vein at a rate of 9 ml / s via an automatic power injector ( envision ; medrad , pittsburgh , pa , usa ) and an 18 - gauge catheter . 
after a 9 - s delay from bolus administration , scans were acquired continuously for 40 s with the following parameters : 80 kv , 200 mas , 10 - mm thickness , 1 - s rotation time , 512512 matrix . 
in tutti i casi stato richiesto il consenso informato prima dellesecuzione dellesame o al paziente o al parente pi vicino in accordo con le linee guida del nostro ospedale . preliminarmente stato eseguito un esame tc dellencefalo senza mdc per escludere la presenza di emorragia cerebrale o di ischemia in fossa cranica posteriore . 
le immagini di perfusione cerebrale sono state ottenute con tomografo spirale multistrato a 4 linee di detettori ( volume zoom ; siemens , erlangen , germania ) attraverso la regione dei nuclei della base con angolazione perpendicolare al segmento occipitale del seno sagittale superiore , al disotto della confluenza dei seni , in modo da visualizzare in ununica scansione i tre territori vascolari sovratentoriali . 
lestensione delle scansioni lungo lasse z stata di 20 msono stati iniettati in una vena antecubitale 90 ml di mdc non ionico ( concentrazione di iodio pari a 320 mg / ml ) ad una velocit di 9 ml / s con catetere da 18 gauge utilizzando un iniettore aug . 
le scansioni sono state acquisite con un ritardo di 9 s dal bolo di mdc in modo continuo per una durata di 40 s con i seguenti parametri : 80 kv , 200 mas , sezioni di 10 mm , tempo di rotazione 1 s , matrice 512512 . 
le mappe di perfusione rcbf , rcbv e mtt sono state calcolate utilizzando una workstation dedicata ( vitrea ; vital images , minnetonka , usa )  . entro 12 ore dallesame tc di perfusione stato effettuato un esame rm di controllo con sequenze pesate in diffusione ( dwi ) per confermare la presenza di lesioni infartuali . 
in tabella 1 sono riportati i valori medi dei tre paramentri di perfusione considerati ( mtt , rcbf , rcbv ) nelle tre regioni di interesse ( core lesionale , tessuto ipoperfuso , regioni corrispondenti controlaterali )  . 
lunico parametro che ha mostrato una variazione significativa ( livello di significativit accettato per questo studio : p < 0 , 0001 ) stato lmtt con un valore medio di 5 , 1 s nelle aree ipoperfuse e di 9 , 8 s nel tessuto infartuato rispetto al tessuto sano che presentava valori medi di 3 , 41 s . lanalisi mediante curve roc ha consentito di individuare un valore cut - off di 6 , 05 s per lmtt come valore discriminante tra tessuto ipoperfuso ed il tessuto infartuato cos g . 
2a axial magnetic resonance ( mr ) diffusion weighted image ( dwi ) , and b perfusion computed tomography ( ct ) maps for regional cerebral blood flow ( rcbf ) , regional blood volume ( rcbv ) and mean transit time ( mtt ) in a patients with left peripheral middle cerebral artery ( mca ) stroke . 
2a immagine rm assiale pesata in diffusione ( dwi ) e b mappe tc di perfusione per i parametri rcbf , rcbv e mtt in un paziente affetto da ischemia cerebrale acuta nel territorio di distribuzione superficiale dellarteria cerebrale media si sinistra . 
ampia area di alterazione dellmtt estesa oltre 1 , 5 cm rispetto il core lesionale identificato nellimmagine dwi . the ability to discriminate infarcted and salvageable areas . this has become increasingly relevant with the development of recanalising treatment with thrombolytic agents . 
 ct during acute cerebral ischaemia may inconstantly demonstrate indirect signs , such as artery hyperattenuation due to thrombosis and a mass effect with effacement of the subarachnoid spaces due to oedema [ 1923 ]  . 
evaluation of possible discrepancies between lesion extent , as delineated by dwi , and the extent of the hypoperfused area enables definition of tissue in ischaemic penumbra , which is the target of recanalisation therapy [ 16 ]  . 
3a axial magnetic resonance ( mr ) diffusion weighted image ( dwi ) , and b perfusion computed tomography ( ct ) maps for regional cerebral blood flow ( rcbf ) , regional cerebral blood volume ( rcbv ) and mean transit time ( mtt ) in a patient with left middle cerebral artery ( mca ) stroke . 
3a immagine rm assiale pesata in diffusione ( dwi ) e b mappe tc di perfusione per i parametri rcbf , rcbv e mtt in un paziente affetto da ischemia cerebrale acuta nel territorio di distribuzione dellarteria cerebrale media si sinistra . 
ampia area di alterazione dellmtt estesa oltre 1 , 5 cm rispetto il core lesionale identificato nellimmagine dwi . the constant evolution of multidetector ct ( mdct ) scanners in recent years has led to the development of techniques for the study of cerebral perfusion , with very similar results to those obtained with perfusion mri . 
in particular , it has been demonstrated that the parameters determined by perfusion ct are reliable for defining hypoperfused cerebral tissue [ 14 , 15 ]  . to better appreciate the results of our perfusion ct study , we need to make reference to previous reports [ 24 , 25 ] that have demonstrated a significant correlation between perfusion abnormalities measured on the basis of cbf ( on both ct and mri ) and abnormalities revealed by dwi . 
this is important , as it demonstrates that a reduction in cbf greater than 66% corresponds to the infarcted tissue identified on dwi [ 26 ] , even in the early phase [ 24 , 25 ]  . 
assuming that areas with a cbf reduction > 66% are the infarcted areas [ 26 ] and that these correspond to the final infarct , as identified by diffusion abnormalities , we can hypothesise that the salvageable tissue ( ischaemic penumbra ) is situated within the difference between the area with altered mtt and the area with altered cbf ( < 66% ) , or the mismatch bete affetto da ischemia cerebrale [ 710 , 17 ]  . 
in questo settore , la ricerca stata focalizzata oltre che alla possibilit di delineare in fase precoce il focolaio ischemico , anche alla capacit di discriminare larea infartuata dalle aree salvabili . 
obiettivo della terapia ricanalizzante il ripristino dei valori di perfusione cerebrale , ovvero salvare , se presenti , i tessuti in penombra ischemica sfruttando lesigua finestra terapeutica [ 18 ]  . 
questa terapia non esente da rischi , in particolare di emorragia cerebrale , e conseguentemente necessaria una attenta selezione dei pazienti [ 35 , 18 ]  . lesame tc in corso di ischemia cerebrale acuta , pu mettere in evidenza , in maniera incostante , segni indiretti quali liperdensit delle arterie in relazione a trombosi e leffetto massa con la cancellazione degli spazi subaracnoidei per la presenza delledema [ 1923 ]  . 
tuttavia , soltanto con lesame rm con sequenze pesate in diffusione possibile individuare il focolaio ischemico in fase iperacuta sin dai primi minuti dallinsorgenza della sintomatologia clinica [ 6 , g . 
areas of perilesional oligaemia may be included within the perfusion abnormality identified by mtt , and this sensitivity in part accounts for the results of this and other studies in which mtt proved to be the most sensitive parameter for identifying penumbra . 
despite these possible limitations , it should be considered that studies correlating perfusion maps and final injury and applying the alberta stroke program early ct score ( aspects ) to perfusion maps obtained the best correlations with final injury in nonreperfused patients with analysis of cbf and mtt maps [ 27 ]  . 
 it can therefore be stated that mtt is a highly sensitive parameter for the definition of infarcted or salvageable tissue , whereas cbf has greater specificity [ 28 , 29 ]  . 
in bearing with previous reports [ 28 ] , interpretation of mtt maps in our study proved to be straightforward , as the healthy areas were homogeneously normal , and the areas with perfusion alterations were readily recognised by their inhomogeneous colour distribution . 
it should be noted , however , that progression from ischaemia to infarction depends not only on cerebral perfusion but also on duration of blood flow reduc15 , 17 ]  . 
anche con lesame rm di diffusione non tuttavia possibile discriminare il tessuto vitale , ipoperfuso , dalla lesione infartuale ed necessario ricorrere a tecniche di studio di perfusione cerebrale con rm [ 17 ]  . 
la valutazione di eventuali discrepanze tra lentit della lesione delineata in diffusione e lentit dellarea ipoperfusa consente poi di definire il tessuto in penombra ischemica , che costituisce lobiettivo della terapia ricanalizzante [ 16 ]  . negli ultimi anni , con la continua evoluzione degli apparecchi tc spirale multidetettore , stata perfezionata la tecnica di studio di perfusione cerebrale con risultati sovrapponibili a quelli ottenuti con rm di perfusione . 
 per comprendere i risultati ottenuti con lesame tc perfusionale bisogna fare riferimento ai risultati riportati in letteratura [ 24 , 25 ] che dimostrano come esista una correlazione significativa tra le anomalie di perfusione misurate attraverso il cbf ( sia con tc che con rm ) e le anomalie rilevate nelle immagini dwi . 
questo dato rilevante perch dimostra che una riduzione maggiore del 66% del cbf corrisponde al tessuto infartuato cos come identificato nelle immagni dwi [ 26 ] anche in fase precoce [ 24 , 25 ]  . 
assumendo che le aree con riduzione del cbf > 66% siano le aree infartuate [ 26 ] e che queste corrispondano allinfarto finale definito dalle anomalie di diffusione , possiamo ipotizzare che il tessuto salvabile ( in penombra ischemica ) sia compreso nella differenza tra larea con alterato mtt e larea con alterato cbf ( < 66% ) ovvero dalla discrepanza tra mtt e dwi [ 26 ]  . 
nellambito dellalterazione perfusionale identificata dallmtt possibile includere aree di oligoemia perilesionale e tale sensibilit spiega in parte i risultati ottenuti in questo ed in altri studi in cui lmtt si rivelato il parametro pi sensibile nellidentificazione del tessuto in penombra . pur con queste possibili limitazioni bisogna comunque considerare che negli studi di correlazione tra mappe di perfusione e danno finale , utilizzando gli alberta stroke program early ct score ( aspects ) per le mappe di perfusione , le migliori correlazioni con il danno finale nei pazienti senza riperfusione si ottengono mediante lanalisi delle mappe di cbf e mtt [ 27 ]  . si pu pertanto affermare che per la definizione del tessuto infartuato o salvabile lmtt un parametro altamente sensibile mentre il cbf invece dotato di maggior specificit [ 28 , 29 ]  . 
nella nostra esperienza le mappe mtt sono risultate di facile interpretazione , come peraltro riportato in letteratura [ 28 ] , in quanto le aree sane sono omogeneamente normali e le aree con alterata perfusione risultano facilmente identificabili dalla disomogenea distribuzione del colore . 
in particolare , le alterazioni di perfusione cerebrale sono state espresse da un marcato incremento dellmtt . utilizzando questo parametro stato possibile definire un valore soglia che discriminasse tra tessuto ischemico e non . lanalisi delle curve roc dimostra infatti che per valori di mtt superiori o uguali a 6 , 05 s possibile identificare il tessuto infartuato mentre con valori medi di mtt di 5 , 1 s , e quindi inferiori a 6 , 05 s , viene identificato il tessuto in penombra ( p < 0 , 0001 )  . 
4 receiver operating characteristic ( roc ) curves for perfusion computed tomography ( ct ) parameters [ regional cerebral blood volume ( rcbv ) , regional cerebral blood flow ( rcbf ) and mean transit time ( mtt ) ]  . 
4 curve roc ( receiver operator characteristic ) dei parametri di perfusione cerebrale rcbv , rcbf e mtt per identificare il valore cut - off tra infarto e tessuto sano . 
il prolungamento dellmtt per valori medi di 5 , 1 s identifica il tessuto in penombra ischemica mentre per valori uguali o superiori a 6 , 05 s identifica il tessuto infartuato con una sensibilit dell84 , 6% , specificit del 100% , valore predittivo positivo del 100% , valore predittivo negativo del 86 , 7% e accuratezza del 92 , 3% ( p < 0 , 0001 )  . 
asse x : 1specificit ( falsi positivi ) ; asse y : sensibilit ( veri positivi ) ; az , area sotto la curva . tion and the greater vulnerability of specific neuronal populations [ 30 , 31 ]  . 
 zione del flusso ematico e dalla maggiore vulnerabilit di specifiche popolazioni neuronali [ 30 , 31 ]  . conclusions conclusioni perfusion ct with latest - generation mdct scanners is a rapid technique that can be used to complete unenhanced ct , with only slightly longer examination times . 
 the disadvantages of this study protocol are increased exposure to ionising radiation and use of iodinated contrast material , which requires assessment of renal function and possible predisposition to allergies . 
in addition , cerebral perfusion ct allows limited coverage of the cerebral parenchyma , although this is destined to increase with increased detector numbers . la tc perfusionale una tecnica di studio di rapida esecuzione utilizzando tomografi multidetettore di ultima generazione e pu essere eseguita a completamento dellesame tc di base con un modesto prolungamento del tempo desame . ci particolarmente utile considerando la necessit di sfruttare la ristretta finestra terapeutica per il trattamento trombolitico . 
questa tecnica di studio quindi complementare allo studio tc di base e fornisce informazioni diagnostiche aggiuntive di grande rilievo clinico . gli svantaggi di questo protocollo desame sono correlati allaumento della dose di radiazioni ionizzanti al paziente e allutilizzo del mezzo di contrasto iodato che richiede la valutazione dei parametri di funzionalit renale e delleventuale diatesi allergica . 
eastwood jd , lev mh , azhari t et al ( 2002 ) ct perfusion imaging with deconvolution analysis : a pilot study of patients with acute middle cerebral artery stroke . 
wintermark m , fischbein nj , smith ws et al ( 2005 ) accuracy of dynamic perfusion ct with deconvolution in detecting acute hemispheric stroke . ajnr am j neuroradiol 26 : 104112 15 . 
ogasawara k , sasaki m , tomitsuka n et al ( 2005 ) early revascularization in a patient with perfusion computed tomography / diffusion - weighted magnetic resonance imaging mismatch secondary to acute vertebral artery occlusion . 
schellinger pd , chalela ja , kang dw et al ( 2005 ) diagnostic and prognostic value of early mr imaging vessel signs in hyperacute stroke patients imaged < 3 hours and treated with recombinant tissue plasminogen activator . 
eastwood jd , lev mh , wintermark m et al ( 2003 ) correlation of early dynamic ct perfusion imaging with whole - brain mr diffusion and perfusion imaging in acute hemispheric stroke . ajnr am j neuroradiol 24 : 18691875 25 . 
wintermark m , reichhart m , cuisenaire o et al ( 2002 ) comparison of admission perfusion computed tomography and qualitative diffusionand perfusionweighted magnetic resonance imaging in acute stroke patients . 
schaefer pw , roccatagliata l , ledezma c et al ( 2006 ) first - pass quantitative ct perfusion identifies thresholds for salvageable penumbra in acute stroke patients treated with intra - arterial therapy . 
grandin cb , duprez tp , smith am et al ( 2002 ) which mr - derived perfusion parameters are the best predictors of infarct growth in hyperacute stroke ? comparative study between relative and quantitative measurements . 
powers wj , grubb rl , darriet d , raichle me ( 1985 ) cerebral blood flow and cerebral metabolic rate of oxygen requirements for cerebral function and viability in humans . 
 correspondence to : giuseppe caruso , via liguria , 21 , i - 90144 palermo , italy , tel . : + 39 - 91 - 6552315 , fax : 39 - 91 - 6552337 , e - mail : carusogi@libero.it received : 23 march 2006 / accepted : 18 august 2006 / published online : 22 february 2007 abstract purpose . 
a total of 1 , 729 ( 1 , 012 women and 717 men ; age range 2882 ; mean age 51 ) patients underwent contrastenhanced sonography of the liver . 
the examination was performed with a low mechanical index ( mi < 0.09 ) after injection of sulphur - hexafluoride - filled microbubbles , using different sonographic equipment and different contrast - specific algorithms . 
heterogeneous delayed liver enhancement was observed in six patients in the late phase ( 180 s ) , with the presence of multiple , partially confluent , hyperechoic areas peripheral to the portal vessels . 
the pattern appeared spontaneously between 1 and 4 h after the examination and was associated with the presence of an anomalous echogenicity in the superior mesenteric veno patient experienced adverse reactions . 
1729 pazienti ( 1012 donne e 717 uomini ; et compresa tra 2882 , media 51 ) sono stati sottoposti ad esame ecografico del fegato dopo somministrazione di ecoamplificatore esafluoruro di zolfo e basso indice meccanico ( mi < 0 , 09 )  . 
limpregnazione anomala del parenchima epatico potrebbe essere secondaria allintrappolamento nei sinusoidi epatici di gas proveniente dal microcircolo intestinale attraverso il sistema entero - portale . key words ultrasound microbubbles liver parole chiave ecografia microbolle fegato introduction introduzione sonographic contrast agents consist of microbubbles containing an inert gas or air with a diameter < 5 m surrounded by a shell or a membrane that provides transpulmonary stability and provides transpulmonary stability and increasing their persistence in the circulation . 
the total volume of mii mezzi di contrasto utilizzati in ecografia sono costituiti da microbolle ( diametro < 5 m ) contenenti gas inerte o aria , e stabilizzate da membrane a composizione differente , che ne garantiscono la stabilit attraverso il circolo transpolmonare aumentandone la persistenza in circolo . 
the second relies on detection of ultrasound ( us ) - induced physical phenomena , such as microbubble destruction , fusion or splitting [ 4 ]  . the purpose of this paper is to report a pattern of heterogeneous late - phase hepatic enhancement with anomalous duration and distribution associated with stratified hypoor hyper - echogenicity in the superior mesenteric vein , which was observed after infusion of sonovue contrast mediuan aetiological hypothesis is also presented . materials and methods from december 2001 to august 2004 , 1 , 729 patients ( 1 , 012 women and 717 men ; age range 2882 years ; mean age 51 ) underwent contrast - enhanced sonography of the liver after injection of sonovue contrast medium ( bracco , milan , italy )  . sonovue is a suspension of hexafluoride sulphur microbubbles ( mean diameter 3 m ) with a phospholipidic shell . 
the elective technique consisted of a bolus injection of 4.8 ml of contrast medium at a rate of approximately 1 ml / s , followed by a 5ml saline flush . 
sebbene si tratti essenzialmente di sostanze blood - pool , il loro comportamento nelle diverse fasi post - contrastografiche sovrapponibile a quello dei mezzi di contrasto organo - iodati , con la differenza che non si ha una vera fase interstiziale . lintroduzione del mezzo di contrasto nel circolo periferico permette di identificare tre diverse fasi della perfusione vascolare epatica , analogamente a quanto possibile ottenere allesame tc dinamico del fegato dopo somministrazione di mezzo di contrasto organo - iodato : fase arteriosa , a 2030 s : in questa fase lenhancement dovuto alla presenza del mezzo di contrasto nelle arterie di piccolo calibro ; fase portale e tardiva , a 60 e 180 s , rispettivamente : nonostante il mezzo di contrasto ecoamplificatore non passi nellinterstizio ma rimanga nei vasi , lenhancement osservato in fase portale e specialmente in fase tardiva , sembra essere dovuto alla persistenza delle microbolle nei sinusoidi o al loro up - take da parte delle cellule del kupffer e delle cellule del sistema reticolo - endoteliale [ 2 , 3 ] ; ipotesi comunque queste che devono essere avvalorate da ulteriori studi di farmacocinetica . le tecniche di imaging ecografico contrasto - specifiche sono due : la prima quella dellimaging non - distruttivo in cui limmagine viene costruita sfruttando la risposta non lineare delle microbolle , senza che queste vengano distrutte ; la seconda tecnica utilizza limaging distruttivo , che determina la distruzione , la fusione e lo splitting delle microbolle [ 4 ]  . scopo del nostro lavoro quello di riportare un fenomeno caratterizzato dalleterogeneo enhancement del parenchima epatico in fase tardiva , anomalo per durata e distribuzione , associato ad un pattern stratificato ipo - iper - ecogeno della vena mesenterica superiore dopo somministrazione di sonovue . 
sulla scorta di una serie di osservazioni abbiamo avanzato una ipotesi eziologica . materiali e metodi dal dicembre 2001 allagosto 2004 , 1729 pazienti ( 1012 donne - 717 uomini , di et compresa tra 28 e 82 anni ; et media 51 anni ) , hanno eseguito un esame ecografico del fegato con ecoamplificatore . 
il sonovue una sospensione di microbolle di esafluoruro di zolfo ( diametro medio 3 , 3 m ) , stabilizzate da una membrana fosfolipidica ; si presenta come una polvere liofilizzata in atmosfera di solfuro esafluoride posta allinterno di un flaconcino di plastica . 
una volta ricostituita , la sospensione appare come soluzione lattescente e rimane stabile per al massimo 6 ore [ 5 ]  . liniezione del mezzo di contrasto stata effettuata 510 minuti dopo la ricostituzione dello stesso . 
la tecnica consiste nelliniezione a bolo di 4 , 8 ml di mezzo di contrasto a velocit di 1 ml / s , seguita dalla infusione di 5 ml di soluzione g . 
use of these algorithms allowed real - time imaging of all vascular phases ( arterial , portal and late ) and was dependent on the availability of the us device at the time of examination ( table 1 )  . 
all examinations were performed as follows : fundamental ( b - mode ) imaging and contrast - specific algorithm without contrast agent contrast - enhanced us in the arterial phase ( 2030 s ) contrast - enhanced us in the portal and late phase ( 60 and 180 s ) contrast - enhanced us in the second late phase ( 240 s )  . patients who showed heterogeneous late - phase hepatic enhancement were examined using the b - mode technique and stimulated acoustic emission ( sae ) , both performed with a high mi ( 1.2 ) ; insonation with high mi is useful for microbubble distribution , leading to possible rapid disappearance of the heterogeneous enhancement pattern . two of the six patients underwent a second contrast - enhanced us after 24 h and 9 days , respectively , using the same us system and the same contrast agent at the same dose . 
tutti gli esami sono stati eseguiti con le stesse modalit come riportato di seguito : imaging fondamentale ( b - mode ) e algoritmo contrastospecifico senza mezzo di contrasto ; ecografia con mezzo di contrasto : fase arteriosa a 2030 s ; ecografia con mezzo di contrasto : fase portale e tardiva a 60 e 180 s rispettivamente ; ecografia con mezzo di contrasto : seconda fase tardiva a 240 s . i pazienti nei quali stato osservato , in fase tardiva , leterogeneo enhancement epatico sono stati sottoposti a esame ecografico con tecnica b - mode in e con stimulated acustic emission ( sae ) entrambe ad elevato indice meccanico ( mi = 1 , 2 ) , allo scopo di determinare la distruzione delle microbolle di mezzo di contrasto con leventuale rapida scomparsa delleterogeneo enhancement . due dei sei pazienti hanno eseguito un secondo esame ecocontrastografico a 24 ore e a 9 giorni rispettivamente , utilizzando la stessa apparecchiatura ecografica , lo stesso mezzo di contrasto , nella stessa dose . 
nei due pazienti in cui stata somministrata per la seconda volta lo stesso mezzo di contrasto nella stessa dose ( a distanza rispettivamente di 24 ore e 9 giorni ) il fenomeno non si ripresentato . 
nessuno dei sei pazienti ha presentato sintomi , n sono state osservate alterazioni della pressione arteriosa . discussione leterogeneo enhancement epatico stato descritto per la prima volta da okada [ 6 ] : egli ha osservato un fenomeno simile in sei pazienti dopo somministrazione di levovist ( 5 casi ) e di echogen ( 1 caso )  . 
1 immagine ottenuta dopo somministrazione di ecoamplificatore con coherent contrast imaging , fase tardiva ( 4 minuti ) : presenza di multiple aree iperecogene parzialmente confluenti nel contesto del parenchima epatico perifiericamente ai vasi portali ( frecce )  . 
 observation of these findings was possible thanks to the use of second - generation sonographic contrast agents , which allow real - time examination of hepatic vascular perfusion : this suggests that gas is present in the enteroportal circulation but not in the other vessels , which could account for the origin of the hepatic phenomenon . 
4 fundamental ( b - mode ) imaging , late phase ( 40 min ) : marked hyperechogenicity ( 1 ) can be seen in the superior mesenteric vein ( between the two arrows )  . 
4 immagine in basale ( b - mode ) ; fase tardiva a 40 minuti : possibile dimostrare una marcata iperecogenicit ( 1 ) nel lume della vena mesenterica superiore ( compresa tra le due frecce )  . 
liperecogenicit appare localizzata in sede ventrale mentre lipoecogenicit in sede declive come fase gassosa in fase fluida ( 2 )  . discussion heterogeneous hepatic enhancement was first described by okada [ 6 ] , who reported a similar phenomenon occurring in six patients after injection of levovist ( five cases ) and echogen ( one case )  . 
to the best of our knowledge , heterogeneous hepatic enhancement has never been observed following administration of sonovue contrast mediuunlike the agents employed by okada , sonovue relies on a low mi to provide real - time imaging of hepatic perfusion [ 7 ]  . 
il fenomeno si verificato con mezzi di contrasto diversi ( per tipo di gas e natura della membrana delle microbolle ) e con tecniche di insonazione diverse : una ad alto indice meccanico con distruzione delle microbolle ( levovist ed echogen ) ; laltra a basso indice meccanico con fenomeni di risonanza delle microbolle ( sonovue ) [ 8 ]  . il levovist un agente epato - specifico ; ha unemivita breve e il suo effetto dopo linsonazione dura solo alcuni secondi . 
moreover , has liver - specific parenchymal uptake after blood - pool clearance ; it is short - lived , and once an area has been scanned for a few seconds , the effect disappears . 
it is best seen with relatively high acoustic power settings ( although still within accepted levels for diagnostic imaging ) and shows a tendency to cluster at the level of the focal zone , where the power is maximal [ 9 , 10 ]  . 
in contrast , sonovue is purely a vascular agent , with no evidence of selective uptake ; it shows a spleen - specific enhancement that lasts longer ( 5 min ) than the blood - pool and liver enhancement phases [ 11 ]  . 
 moreover , the gas microbubbles responsible for this phenomenon are larger than the contrast agent microbubbles and are unable to cross the hepatic sinusoids , the calibre of which is 4050 in addition , this anomalous echogenicity was observed in the vena porta and superior vein only , and not in the splenic vein , hepatic vein , aorta or inferior vena cava . 
echogenicity is similar , but more intense , to the pattern seen in cases of free gas migration into the portal vessels during intestinal ischaemia , necrotic enterocolitis or in other cases of intestinal pneumatosis [ 12 , 13 ]  . 
the possibility that this phenomenon is due to free gas ( thus not incorporated in the shell ) in the superior mesenteric vein and portal vessel is confirmed by several other observations : the stratification pattern seen in the superior mesenteric vein never occurs when the gas is contained in a membrane , as in the case of contrast microbubbles , but only when the gas is free ( intestinal pneumatosis ) the phenomenon persists even after the mi has been increased , an event that should cause immediate microbubble destruction the distribution inside the periportal sinusoids is similar to that seen after injection of free co2 in the hepatic artery ( portal angioechography ) for transient obstruction in the internal sinusoids [ 14 , 15 ]  . a probable explanation for the heterogeneous hepatic enhancement is that the free gas in the superior mesenteric vein is gas emboli originating in the intestinal microcirculation and transported to the liver via enteroportal circulation . 
the pattern of heterogeneous hepatic enhancement is due to entrapment in the hepatic sinusoids of these gas emboli , which have different insonation properties from the microbubbles . several studies have reported that sonographic contrast agents may be responsible for biological damage to the cell membranes and endothelium both in vitro and in vivo [ 1720 ]  . 
di contro , il sonovue , un agente puramente vascolare , non mostra uptake selettivo epatico , mentre presenta una fase spleno - specifica , della durata di circa 5 minuti [ 11 ]  . 
il volume globale di gas contenuto nelle dosi somministrate dellordine di microlitri , invece il fenomeno osservato da noi massivo . inoltre , le microbolle di gas responsabili di questo fenomeno sono di dimensioni maggiori di quelle costituenti il mezzo di contrasto : esse non sono in grado di attraversare i sinusoidi epatici il cui calibro di 4050 abbiamo , inoltre , notato che solo la vena porta e la vena mesenterica superiore presentavano unanomala ecogenicit , non la vena splenica , n le vene sovraepatiche , laorta o la vena cava inferiore . questo anomalo aspetto ecogeno simile , ma pi intenso , al pattern che si osserva nei casi di migrazione di gas libero nei vasi portali in corso di ischemia intestinale , di enterocolite necrotizzante o in altri casi di pneumatosi intestinale [ 12 , 13 ]  . 
la possibilit che laspetto descritto sia da imputare a gas libero ( non incorporato in una membrana ) nella vena mesenterica superiore e nei vasi portali confermato da altre osservazioni : il pattern stratificato allinterno della vena mesenterica superiore non mai osservabile nel caso in cui il gas trovi allinterno di una membrana come nel caso delle microbolle di mezzo di contrasto ; si osserva solo nel caso di gas libero ( pneumatosi intestinale ) ; il fenomeno persiste anche innalzando gli indici meccanici , evento che dovrebbe determinare la distruzione immediata delle microbolle ; la distribuzione allinterno dei sinusoidi periportali sovrapponibile a quanto osservabile dopo iniezione di co2 libera nellarteria epatica ( ecocarbossigrafia ) , per transitorio ostacolo allinterno dei sinusoidi [ 14 , 15 ]  . in base a queste osservazioni si pu ipotizzare che il fenomeno del disomogeneo enhancement epatico sia il risultato di gas libero nella vena mesenterica superiore proveniente da emboli di gas formatisi a livello del microcircolo intestinale e da qui trasportati al fegato attraverso il circolo enteroportale . 
 [ 21 ] demonstrated that in mice and rats , sonographic contrast agents cause inflammation , necrosis and ulceration of the cecum and proximal colon ( cecocolonic area ) , even with a single intravenous administration of a gas - carrier contrast agent . 
 [ 16 ] reported that intestinal lesions in mice and rats after sonographic contrast agent administration are related to the formation of large intravascular gas bubbles in the cecal and colonic wall . 
another probable explanation for heterogeneous hepatic enhancement is microbubble fusion in vivo inside the sinusoids and mesenteric vessels : these microbubble macroaggregates have different insonation properties than the separate microbubbles because of their different size [ 22 ]  . our study has two limitations . 
second , we are unable to explain why this phenomenon is so rare and why it did not occur again in the same two patients after 24 h and 9 days , respectively . 
 [ 16 ] hanno osservato che le lesioni intestinali riscontrate nei topi e nei ratti dopo somministrazione di mezzo di contrasto ecografico sono correlate alla formazione di macrobolle di gas nella parete colica e cecale . 
unaltra probabile spiegazione alleterogeneo enhancement epatico la fusione delle microbolle in vivo allinterno dei sinusoidi e nei vasi mesenterici : questi macroaggregati , in ragione delle loro diverse dimensioni , presenterebbero caratteristiche di insonazione diverse da quelle delle microbolle [ 22 ]  . il nostro lavoro presenta due limiti : il primo relativo al fatto che le lesioni intestinali descritte da dirven et al . 
 [ 16 ] sono state osservate solo in animali di piccola taglia ( topi e ratti ) , non in animali di taglia maggiore ( porcellini dindia , conigli o cani )  . 
il secondo limite , legato al fatto che non siamo in grado di spiegare perch il fenomeno sia cos raro e perch non si sia ripresentato negli stessi pazienti a 24 h e 9 giorni rispettivamente . nonostante non sia stato possibile chiarire la genesi del fenomeno , le alterazioni osservate sono reversibili e non compromettono la compliance del paziente . 
passariello1 1dipartimento di scienze radiologiche , universit degli studi di roma la sapienza , policlinico umberto i , v.le regina elena 324 , i - 00161 roma , italy 2servizio di fisica radiologica , dipartimento di scienze radiologiche , universit degli studi di roma la sapienza , roma , italy correspondence to : m . 
we present our initial clinical experience with a recently introduced 64 - detector computed tomography ( 64 - mdct ) scanner that makes use of a periodic motion of the focal spot in the longitudinal direction ( z - flying focal spot ) , which enables it to reach a final spatial resolution of 0.40.40.4 mm3 and a temporal resolution of 83 ms . 
a total of 114 patients ( 108 men , six women ; age range 3677 years , mean 63.1 years ) underwent retrospective electrocardiogram ( ecg ) - gated examination of the coronary arteries using a 64 - mdct scanner ( somatom sensation 64 , siemens medical solutions , germany )  . 
acquisition parameters were the following : collimation 640.6 mm , 800 quality reference milliampere second ( mas ) , 120 kvp , 0.33 - s gantry rotation time and pitch 0.2. 
administration of 80 ml of contrast agent ( iomeron 400 mgi / dl , bracco , italy ) + 30 ml of saline at 4 / s and delay time determined using a bolus triggering technique . 
oral betablockers were administered to patients with heart rate ( hr ) > 75 bpto reduce radiation exposure , an automatic exposure control system was applied in all cases to adapt tube current to patient size and anatomic shape ( care dose 4d , siemens medical solutions , germany )  . 
the optimal temporal window for raw data reconstruction was chosen from an initial preview of images reconstructed with different phase settings ( range 0%95% rr interval with 5% gap ) at a selected anatomical level in the mid part of the right coronary artery . 
in patients with hr < 60 bmp , the best reconstruction intervals were identified in the end - systolic ( 30%35% of the rr interval ) and end - diastolic ( 60%65% of the rr interval ) phases ; with faster hr ( > 80 bmp ) , high image quality was observed in end - systole ( 30%35% of the rr interval )  . 
nel presente lavoro introduciamo la nostra esperienza preliminare e lottimizzazione del protocollo di acquisizione di un apparecchio tcms in grado di acquisire 64 strati per rotazione ( tcms - 64 ) grazie allutilizzo di un movimento periodico della macchia focale lungo lasse longitudinale z che consente di raggiungere una risoluzione spaziale di 0 , 40 , 40 , 4 mm3 e temporale di 83 ms . 
114 pazienti ( 108 maschi e 6 femmine , intervallo di et 3677 anni , media 63 , 1 ) sono stati sottoposti ad esame con tcms delle arterie coronarie utilizzando uno scanner tcms - 64 ( somatom sensation 64 , siemens medical solutions , germania )  . 
i parametri di acquisizione sono stati i seguenti : collimazione 640 , 6 mm , 800 quality reference mas , 120 kvp , tempo di rotazione 0 , 33 s e pitch 0 , 2 . 
in tutti i pazienti le immagini sono state acquisite dopo somministrazione ev di 80 ml di mdc ( iomeron 400 mgi / dl , bracco , italia ) + 30 ml di soluzione fisiologica con ritardo di scansione calcolato con tecnica bolus triggering . 
in tutti i casi stato utilizzato un sistema di limitazione automatica della dose ( care dose 4d , siemens medical solutions , forchheim , germania ) in grado di modulare la corrente emessa del tubo in relazione ai valori di attenuazione della regione che si sta studiando . 
la finestra temporale ottimale per la ricostruzione dei dati grezzi stata scelta da uniniziale preview di immagini ricostruite in differenti fasi del ciclo cardiaco ( tra 0%95% dellintervallo r - r ogni 5% ) rilevato ad un livello anatomico predefinito nel tratto medio dellarteria coronaria di destra . 
durante lacquisizione tcms stata registrata una fc media di 65 , 619 , 2 bpm ( intervallo : 4496 bpm ) con bradicardizzazione effettuata in 16 / 114 pazienti ( 14 , 0% )  . 
the 64 - mdct scanner diagnostic performance for coronary ct angiography is further improved with better spatial and temporal resolution and faster scan times ; besides , initial clinical results are promising . 
nei pazienti con fc < 60 bpm , la migliore finestra temporale nella quale effettuare la ricostruzione delle immagini stata individuata rispettivamente nelle fasi telesistolica ( 35% dellintervallo r - r ) e meso - telediastolica ( 65%70% dellintervallo r - r ) ; nei casi con fc di base elevata ( > 80 bpm ) , la migliore fase per la ricostruzione delle immagini risultata la telesistole ( 35% dellintervallo r - r )  . 
il ctdi volumetrico ( ct dose index volume ) risultato in media di 36 , 538 , 30 mgy per paziente con un range compreso tra 27 , 2 e 61 , 9 mgy corrispondenti ad un eff mas . 
se confrontato con unacquisizione effettuata a amperaggio costante , lutilizzo del sistema di limitazione automatica della dose ha consentito una riduzione media del ctdi volumetrico del 33 , 3% per paziente ( p < 0 , 001 )  . 
la nostra esperienza clinica iniziale ha evidenziato come lultima generazione di tomografi tcms - 64 apra nuovi scenari per la gestione clinica del paziente coronaropatico . lutilizzo di sistemi idonei di modulazione automatica dellintensit di corrente del tubo radiogeno appare tuttavia indispensabile per limitare la dose di esposizione del paziente che rappresenta , allo stato attuale , il limite principale allutilizzo clinico della metodica . parole chiave arterie coronarie tc multidetettore coronaropatia infarto miocardico dose di esposizione in tc introduction introduzione since the introduction of multidetector computed tomography ( mdct ) into clinical practice in 1998 , diagnostic imaging of the heart and coronary arteries has been one of the main fields of interest for this technique [ 1 , 2 ]  . 
despite the major epidemiological , health and economic implications of ischaemic heart disease [ 3 ] , the study of the coronary tree using noninvasive techniques was for years a difficult problem to solve due to intrinsic technical limitations . 
the coronary artery circulatory is , in fact , a difficult vascular district to assess using the various imaging techniques available due not only to the small diameter and tortuous course of the arteries but also to the complex cardiorespiratory movements . the high spatial and temporal resolution obtainable with the most recent 16 - , 32 - , 40and 64 - detector mdct devices , coupled with the possibility of achieving adequate cardiac synchronisation , has enabled these limitations to be overcome , at least in part , thus revolutionising the management of patients with heart disease [ 7 , 8 ]  . 
the numerous clinical studies published in recent years have demonstrated the high level of diagnostic accuracy of mdct with regard to both assessment of coronary artery stenosis and follow - up of coronary artery bypass graft patency [ 916 ]  . the volume acquired for studying coronary arteries can be used for performing functional studies on volumes , calculating the ejection fraction and myocardial mass of both ventricles , and assessing regional motion and identifying the presfin dalla sua introduzione in ambito clinico nel 1998 , la diagnostica per immagini del cuore e delle arterie coronarie ha rappresentato uno dei campi di maggior interesse della tc multistrato ( tcms ) [ 1 , 2 ]  . 
malgrado le rilevanti implicazioni epidemiologiche ed economico - sanitarie della cardiopatia ischemica [ 3 ] , lo studio dellalbero coronarico con metodiche di tipo non invasivo stato per molti decenni un problema di difficile soluzione per limiti tecnici intrinseci , rimanendo dominio quasi esclusivo della coronarografia selettiva , procedura gravata da una non trascurabile mortalit e morbilit [ 46 ]  . 
il circolo arterioso coronarico rappresenta infatti un distretto vascolare di difficile valutazione per le diverse metodiche di imaging sia per il piccolo calibro ed il decorso tortuoso delle sue arterie , che per la complessit dei movimenti cardio - respiratori . lelevata risoluzione spaziale e temporale ottenibile soprattutto con i pi recenti apparecchi tcms a 16 , 32 , 40 e 64 canali e la possibilit di ottenere unadeguata cardiosincronizzazione ha consentito di superare almeno in parte tali limitazioni , dando luogo ad una rivoluzione nella gestione del paziente coronaropatico [ 7 , 8 ]  . 
i numerosi studi clinici pubblicati in questi ultimi anni hanno ormai ampiamente dimostrato come la tcms rappresenti una metodica dalla elevata accuratezza diagnostica sia per quanto riguarda la valutazione delle stenosi coronariche che il follow - up della perviet dei by - pass aorto - coronarici [ 916 ]  . il volume acquisito per studiare le arterie coronarie pu anche essere utilizzato per effettuare studi funzionali sui volumi , per calcolare la frazione di eiezione e la massa miom . 
nonetheless , clinical use of coronary artery mdct is currently hindered by several limitations [ 20 ] : imaging of coronary stents that due to their metallic struts generate beam - hardening artefacts and hinder accurate assessment of the state of the intrastent vascular lumen [ 21 , imaging of extensively calcified coronary arteries , also due to beam - hardening artefacts [ 23 ] elevated patient heart rate ( hr ) ( > 65 bmp ) , which causes progressive shortening of the electrocardiogram ( ecg ) rr interval and a consequent shortening of the end - diastolic phase in which image acquisition occurs , thus leading to motion artefacts [ 24 , 25 ] rhythm disturbances , which render cardiac synchronisation impossible [ 25 ] accuracy in assessing regional motion caused by the relatively low temporal resolution of mdct , especially when compared with other techniques such as magnetic resonance imaging ( mri ) and , above all , ecg [ 17 ]  . clearly then , most limitations of mdct depend on the resolution limitations of the technique , and therefore , as achenbach emphasised in 2004 , the key to obtaining increasingly accurate diagnostic imaging lies in increasing both spatial and temporal resolutions [ 26 ]  . in this context , we present our early clinical experience with the latest - generation 64 - mdct device in noninvasive coronary artery imaging . 
development of this latest generation of mdct in fact leads to a potential increase in radiation exposure , which could limit the clinical use of 64 - mdct , especially if proposed as a potential screening tool . materials and methods study population between january and may 2005 , 114 patients ( 108 men and six women ; age range 3677 years , mean 63.1 years ) underwent mdct angiography of the coronary arteries . 
all examinations were performed using a 64 - mdct device with a 0.33 - s gantry rotation time ( somatom sensation 64 , siemens medical solutions , forchheim , germany ) and images acquired with retrospective ecg gating . 
clinical indications for the examination were the following : typical ( n = 16 ) or atypical ( n = 7 ) chest pain in patients with a clinical indication for coronarography follow - up at 69 months of the patency of treated coronary stents ( n = 37 for a total of 63 stents )  . 
the findings of the comparison of the two techniques will therefore not be presented here , as this falls beyond the scope of the present study . follow - up of patency of aortocoronary bypass grafts ( n = 40 for a total of 48 bypasses : 32 venous grafts and 16 arterial grafts ) cardica di entrambi i ventricoli , per valutare la cinesi regionale e per identificare la presenza di aree di miocardio infartuato o non - riperfuso correlando lo stato di un vaso coronarico con quello del suo territorio di pertinenza vascolare [ 1719 ]  . 
allo stato attuale , limpiego clinico della tcms delle arterie coronarie presenta tuttavia alcune rilevanti limitazioni [ 20 ] : imaging degli stent coronarici , che a causa della loro trama metallica generano artefatti da indurimento del fascio che impediscono di valutare in modo accurato lo stato del lume vascolare intra - stent [ 21 , 22 ] ; imaging delle coronarie estesamente calcifiche , sempre per linsorgenza di artefatti da indurimento del fascio [ 23 ] ; frequenza cardiaca ( fc ) elevata del paziente ( > 65 battiti per minuto bpm ) , che determina un progressivo accorciamento dellintervallo r - r elettrocardiografico ( ecg ) e conseguentemente della durata della fase telediastolica in cui avviene lacquisizione delle immagini determinando linsorgenza di artefatti da movimento [ 24 , 25 ] ; turbe del ritmo , con impossibilit di ottenere una adeguata cardiosincronizzazione [ 25 ] ; accuratezza nella valutazione della cinesi regionale determinata dalla relativamente bassa risoluzione temporale della tcms soprattutto se confrontata con altre metodiche di riferimento quali la risonanza magnetica e soprattutto lecocardiografia [ 17 ]  . appare quindi evidente come la gran parte delle attuali limitazioni della tcms dipenda da limiti di risoluzione della metodica e pertanto , come sottolineato da achenbach nel 2004 , la chiave per ottenere prestazioni diagnostiche sempre pi accurate lincremento della risoluzione sia spaziale che temporale [ 26 ]  . in questa ottica , nel presente lavoro introduciamo la nostra esperienza clinica preliminare con apparecchiatura tcms di ultima generazione a 64 strati nellimaging non - invasivo delle arterie coronarie , analizzando anche la problematica dosimetrica . 
lo sviluppo di questa nuova generazione di tcms comporta , infatti , un potenziale incremento della dose di esposizione del paziente che rappresenta un possibile fattore limitante limpiego clinico della tcms - 64 soprattutto se si vuole proporre la metodica come potenziale strumento di screening . materiali e metodi popolazione di studio nel periodo compreso tra gennaio e maggio 2005 , 114 pazienti [ 108 maschi , 6 femmine , et compresa tra 3677 anni ( aa ) media 63 , 1 aa ] sono stati sottoposti ad unangiografia con tcms delle arterie coronarie . 
tutti gli esami sono stati effettuati utilizzando unapparecchiatura di tcms - 64 dotata di velocit di rotazione del sistema tubo radiogeno - detettori di 0 , 33 secondi ( somatom sensation 64 , siemens medical solutions , forchheim , germania ) ed acquisendo i dati con gating elettrocardiografico ( ecg ) di tipo retrospettivo . 
therefore , to obtain high - quality images , the hr was empirically slowed in all patients who at the time of the examination had a basal hr > 75 bmp . 
this was achieved using the following drug regimen : oral administration of 40 mg of beta - blockers 6090 min before the examination ( chlorhydrate , propranolol , inderal , astrazeneca ) , and monitoring arterial blood pressure and pulse rate . image acquisition protocol and automatic exposure control system for the examination , the patient was asked to lie supine on the ct table with arms behind the head . 
three electrodes were placed on the chest ( the first on right emithorax , the second 1 cm under the clavicle and the third on the left flank ) to monitor the patients ecg and obtain a tracing with a lead similar to l1 in which the p wave , the qrs complex and the t wave could be distinguished . 
in all cases , the examination was performed following iv administration of nonionic iodinated contrast material and covering a volume from the tracheal carina to the cardiac base ; for the study of coronary bypass grafts , acquisition was extended to include a volume comprising the proximal anastomosis and the cardiac base . 64 - mdct sensation 64 scanner utilizes an automatic exposure control system [ combined applications to reduce exposure ( care ) dose 4d , siemens medical solutions , forchheim , germany ] that combines both angular ( x - y axis or angular modulation system ) and z - axis ( or z - axis modulation system ) tube current modulation [ 2731 ]  . in practice , beginning with the initial topogram as a reference , the amperage is automatically modulated along the entire acquisition volume on the basis of the angular attenuation coefficient ( mean density of a tissue with respect to the tube rotation angle in the x - y axis ) of the anatomical region being studied and on the basis of the attenuation values of the different tissues along the z - axis , with data detected on the basis of the previous slice ( on - line modulation )  . 
for example , in a total - body study , lower amperages are used for rizzare , in pazienti con indicazione clinica alla coronarografia ; controllo a distanza di 69 mesi della perviet di stent coronarici medicati ( n = 37 per un totale di 63 stent )  . 
non verranno quindi riportati di seguito i risultati sul confronto tra le due metodiche poich non rappresenta lobiettivo specifico del presente lavoro ; controllo a distanza della perviet di by - pass aorto - coronarici ( n = 40 per un totale di 48 by - pass ; 32 graft venosi e 16 arteriosi ) ; pazienti sottoposti a scintigrafia miocardica perfusionale a riposo e dopo sforzo con risultati diagnostici non conclusivi ( n = 3 ) ; pazienti sottoposti ad esame ecocardiografico a riposo e dopo stress farmacologico con dobutamina con risultati diagnostici non conclusivi ( n = 11 )  . tutti i pazienti hanno firmato un consenso informato in cui veniva chiaramente spiegato il tipo di procedura a cui si sottoponevano ed i potenziali rischi . 
i criteri di esclusione per lo studio sono stati i seguenti : nota ipersensibilit ai mezzi di contrasto ( mdc ) iodati ; insufficienza renale ( creatininemia > 2 mg / dl ) ; insufficienza cardiaca conclamata ; aritmie cardiache maggiori ; insufficienza respiratoria ; asma bronchiale nei pazienti con indicazione al pre - trattamento con farmaci beta - bloccanti ( controindicazione assoluta alla somministrazione di beta - bloccanti )  . preparazione del paziente lelevata frequenza cardiaca rappresenta uno dei principali fattori in grado di influenzare negativamente la qualit diagnostica dellesame determinando un accorciamento dellintervallo r - r elettrocardiografico con insorgenza di artefatti da movimento [ 24 , 25 ]  . 
per tale motivo , al fine di ottenere massima qualit delle immagini nella nostra esperienza iniziale la bradicardizzazione stata effettuata empiricamente in tutti i pazienti che , al momento di effettuare lesame , presentavano fc basale > 75 bpm , utilizzando il seguente schema di preparazione farmacologica : somministrazione per os di 40 milligrammi ( mg ) di farmaco - bloccante 6090 minuti prima dellesame ( propranolo cloridrato , inderal , astrazeneca ) , monitorando pressione arteriosa ( pa ) e polso ( fc )  . protocollo di acquisizione delle immagini e sistema di limitazione automatica della dose al momento dellesame il paziente stato invitato a sdraiarsi in posizione supina sul lettino della tc con le braccia dietro la testa . 
posizionando tre elettrodi sul torace ( rispettivamente a livello dellemitorace destro e sinistro , un cm al di sotto della clavicola ed in corrispondenza del fianco sinistro ) stato possibile monitorare lecg del paziente , fino ad m . 
based on the initial topogram in the anteroposterior ( ap ) and lateral position ( a ) , care dose 4d automatically modulates tube current during each tube rotation according to the patients angular attenuation profile . 
1a , b sistema di modulazione automatica della dose : partendo dal topogramma iniziale ( a ) , lamperaggio viene modulato automaticamente lungo tutto il volume di acquisizione in base al coefficiente angolare di attenuazione della regione anatomica che si sta studiando . 
in tutti i casi lesame stato eseguito dopo somministrazione endovenosa ( ev ) di mdc iodato non ionico coprendo un volume cranio - caudale compreso tra la carena tracheale e la base cardiaca ; per lo studio dei bypass coronarici lacquisizione stata estesa in modo da includere un volume compreso tra lanastomosi prossimale e la base cardiaca . lo scanner di tcms - 64 utilizza un sistema di limitazione automatica della dose ( combined applications to reduce exposure , care dose 4d , siemens medical solutions , forchheim , germania ) in grado di combinare la modulazione della corrente emessa dal tubo radiogeno sia in relazione al valori di attenuazione angolare ( xy - axis o angular modulation system ) della regione in esame che attraverso un sistema di modulazione della dose lungo lasse z ( o z - axis modulation system ) [ 2731 ]  . in pratica , partendo come riferimento dal topogramma inim . 
contrast material was administered using a dual - head automatic injector ( medrad stellant dual ; medrad , palo alto , pa , usa ) in which the two syringes containing contrast material and saline solution , respectively , were connected by a y - shaped connector equipped with a one - way valve to prevent reflux . 
use of saline solution reduces the total volume of contrast material administered to the patient , thus compressing the iodine bolus and at the same time reducing the presence of beam - hardening artefacts at the level of the superior vena cava [ 32 ]  . acquisition delay was chosen using the bolus triggering technique , which involves positioning a region of interest ( roi ) in correspondence with the aortic arch and monitoring passage of the contrast material bolus with a series of low - dose dynamic scans ( 120 kvp , 30 mas ) with 1 - s intervals [ 33 ]  . 
in this way , the effective ctdi volume could be measured prior to the examination , even in conditions of constant tube - current intensity throughout the acquisition ( without the use of care dose 4d )  . an estimate of the dose absorbed [ expressed in milligray ( mgy ) ] was then made using the care dose 4d system , and this estimate was compared with the dose to which the patient would have otherwise been exposed without the use of current modulation . 
tuttavia il sistema di mudulazione della dose utilizzato in modalit cardiosincronizzata effettua una semplice riduzione del milliamperaggio in base ai valori di attenuazione individuale del paziente . i parametri tecnici utilizzati sono stati i seguenti : collimazione 3220 , 6 mm ; spessore strato 0 , 75 mm ; incremento 0 , 4 mm ; tempo di rotazione del sistema tubo radiogeno / detettori 0 , 33 s ; pitch 0 , 2 ; quality reference mas : 800 ; effective mas : variabile in relazione alle caratteristiche individuali del paziente ; 120 kvp ; filtri di convoluzione per la ricostruzione delle immagini : b20f ( tessuti molli ) e b46f ( utilizzato per la valutazione degli stent coronarici )  . somministrazione del mezzo di contrasto in tutti i pazienti stato utilizzato un mdc ad alta concentrazione di iodio ( 400 mgi / 100 ml , iomeron 400 , bracco , milano , italia ) seguito da un bolo di soluzione fisiologica . 
il mdc stato somministrato utilizzando un iniettore automatico a doppia testata ( medrad stellant dual , medrad , palo alto pa , usa ) in cui le due siringhe contenenti rispettivamente mdc e soluzione fisiologica sono state collegate tra loro tramite raccordino a y dotato di valvola unidirezionale per impedire il reflusso . 
lutilizzo della soluzione fisiologica consente di ridurre il volume totale di mdc somministrato al paziente , compattando il bolo di iodio e riducendo contemporaneamente la presenza di artefatti da indurimento del fascio a livello della vena cava superiore [ 32 ]  . per la scelta del ritardo di acquisizione stata utilizzata la tecnica del bolus triggering posizionando una regione di interesse in corrispondenza dellarco aortico e monitorizm . 
transverse images of 20 different cardiac cycle phases ( 0%95% of rr interval with 5% gap ) obtained at a predefined anatomical level in the middle part of the right coronary artery ( a )  . 
in this patient with a heart rate of 58 bmp , best image quality with minimal motion artefacts is observed in the end - systolic phase ( 20%25% of rr ) and the midto enddiastolic phase ( 70% of the rr )  . 
maximum intensity projection ( mip ) image obtained in the same patient , reconstructing images at 65% of the rr interval , allows the presence of disease throughout the course of the right coronary artery to be excluded ( b )  . 
2a , b esempio di preview series per la selezione della migliore finestra temporale ( percentuale intervallo r - r ) delle immagini utilizzando gating cardiaco di tipo retrospettivo . immagini assiali delle 20 successive serie di ricostruzioni ( dal 0% al 95% dellintervallo rr con gap del 5% ) , ottenute sulla medesima scansione , a livello del terzo medio della cdx ( a ) ; in questo paziente , con fc di 58 bpm , la minor presenza di artefatti da movimento si osserva nelle immagini ricostruite al 20%25% ( intervallo che corrisponde alla telesistole ) e tra il 60% ed il 70% dellintervallo r - r ( fase meso - telediastolica )  . 
this tends to improve temporal resolution by using the raw data derived from multiple cardiac cycles ( up to a maximum of three cycles ) to reconstruct the images [ 35 ]  . zando il passaggio del bolo di mdc attraverso una serie di scansioni dinamiche a bassa dose ( 120 kvp 30 mas ) con intervalli di 1 secondo [ 33 ]  . 
la soglia predefinita per linizio della scansione stata di 100 unit hounsfield ( hu ) con intervallo di tempo tra raggiungimento del valore soglia ed inizio dellacquisizione stessa di 7 secondi . la somministrazione del mdc stata effettuata con protocollo di tipo monofasico utilizzando i seguenti parametri [ 34 ] : 80 ml di mdc + 30 ml di fisiologica con flusso di 4 ml / s con durata totale della somministrazione di 27 , 5 secondi . image postprocessing valutazione dose di esposizione after identifying the best reconstruction interval , the images were processed using a dedicated workstation connected to tutti i pazienti sono stati studiati con utilizzo del software care dose 4d . 
volume rendering algorithms , in contrast , were used mainly in patients being studied for evaluation of aortocoronary bypasses and in all cases where the intuitive 3d approach of this algorithm enabled concise and easily recognisable representation of the state and site of coronary disease . 
this approach provides the patient with images that are easier to understand . given the large number of images obtained on average for each examination ( around 2 , 000 ) , in all cases , images were digitally stored on a compact disc equipped with software for viewing the images in dicom3 format ( digital imaging communication in medicine )  . 
all data from the mdct examination ( except the raw data ) were then archived using the picture archive and communication system ( pacs ) ( lifeweb image manager , veania imaging technologies , italy )  . results the mdct examination was carried out without complications in all patients . 
hr was slowed down in 16 / 114 patients ( 14.0% ) ; there were no cases of complications or side effects as a result of administration of oral - blockers . 
in one patient with severe chronic obstructive pulmonary disease ( copd ) and a baseline hr of 96 bmp , even though the hr could not be slowed due to contraindications for - blockers , the examination was performed nonetheless for clinical requirements . the optimal interval for image reconstruction varied in relation to patients hr during data acquisition . 
they cordi riferimento del ctdi volumetrico ( ct dose index volume ) quale parametro della dose assorbita durante lacquisizione delle immagini con gating ecg di tipo retrospettivo . il valore di ctdi viene definito automaticamente dallo scanner sulla base del topogramma in relazione alla intensit di corrente applicata durante lacquisizione . 
in tal modo , preliminarmente allesame , stato possibile registrare leffettivo valore di ctdi volumetrico anche in condizioni di costante intensit di corrente del tubo durante lintera acquisizione ( senza utilizzo del care dose 4d )  . stata quindi effettuata una stima della dose assorbita ( espressa in mgy ) utilizzando il sistema care dose 4d confrontandola con la dose a cui sarebbe stato sottoposto il paziente senza lutilizzo della tecnica di modulazione . 
in alternativa le immagini sono state ricostruite con unaltra consolle dedicata ( vitrea 2 , vital images inc , minnesota , usa )  . per standardizzare la ricostruzione 3d dei dati e fornire al medico di riferimento delle immagini il pi possibile comprensibili stato da noi utilizzato uno schema in cui sono state effettuate per ciascun paziente almeno 6 set di ricostruzioni : m . 
tale approccio consente di sfruttare al meglio lelevata risoluzione spaziale della metodica ottenendo unimmagine a spessore estremamente sottile ( 0 , 6 mm ) lungo tutto il decorso del vaso . 
gli algoritmi in volume rendering sono stati invece utilizzati prevalentemente nei pazienti inviati per studio dei by - pass aorto - coronarici e in tutti quei casi in cui lintuitivo approccio 3d di questo tipo di algoritmo ha consentito di ottenere una rappresentazione sintetica e facilmente intuibile di stato e sede della coronaropatia fornendo al paziente immagini di pi semplice comprensione . considerando il grande numero di immagini ottenute in media per ciascun esame ( circa 2000 ) , in tutti i casi stata fornita una documentazione di tipo digitale con compact disc ( cd ) su cui stato installato un software per la lettura delle immagini in formato dicom3 ( digital imaging communication in medicine )  . 
tutti i dati dellesame tcms ( esclusi i dati grezzi ) sono stati poi archiviati tramite sistema pacs ( lifeweb image manager , ferrania imaging technologies , italia )  . risultati lesame tcms stato effettuato senza alcuna complicanza in tutti i pazienti studiati . 
la bradicardizzazione stata effettuata in 16 / 114 pazienti ( 14 , 0% ) ; in nessun caso si sono avute complicanze o effetti collaterali conseguenti alla somministrazione di - bloccanti orali . 
in un paziente con bpco severa e fc basale di 96 bpm , pur non essendo stata effettuata la bradicardizzazione per la presenza di controindicazione clinica alla somministrazione di farmaco - bloccante lesame stato ugualmente eseguito per esigenze cliniche . lintervallo ottimale per la ricostruzione delle immagini variato in relazione alla fc del paziente durante lacquisizione dei dati . 
3a , b a 64 - mdct angiography performed at 6 - months follow - up after drug - eluting coronary stent implantation on the left anterior descending ( lad ) artery . 
a curved multiplanar reformation shows the presence of a metallic stent with the characteristic railway track ( arrowheads ) appearance located in the proximal part of the vessel ; the presence of contrast within and distally to the stent indirectly indicates patency ( arrows )  . 
b three - dimensional volume rendering reconstruction ; the use of dedicated cardiac software enables visualisation of the stented coronary vessel ( arrow ) along an automatically generated centreline displayed in the transverse and longitudinal axes of lad . 
a la ricostruzione multiplanare curva ( cpr ) , generata lungo lasse longitudinale dellarteria discendente anteriore , dimostra la presenza di flusso allinterno ed a valle dello stent ( frecce ) , che presenta peraltro tipico aspetto a binario ( punte di freccia )  . 
b immagine tridimensionale ottenuta con tecnica volume rendering ; utilizzando un software dedicato di campionatura selettiva del vaso in esame , possibile riprodurre , in modo pratico e veloce , il tratto di arteria selezionata ( freccia ) permettendo una visualizzazione del lume vascolare intra - stent con tecnica cpr ; in tal modo si ottiene una rappresentazione dellarteria sia secondo il suo asse trasversale che longitudinale . 
in cases with higher baseline hr ( > 80 bmp ) , the best phase for image reconstruction proved to be the end - systolic phase ( 35% rr )  . 
in patients with intermediate hr ( 60 bmp ) , no ideal reconstruction window was identified , and the rr interval used varied significantly from patient to patient . in 11 patients ( 9.6% ) , the reconstructed images were affected by artefacts due to either extrasystole during data acquisition ( n = 8 ) or inability to maintain breath - hold for the duration of the acquisition ( n = 3 )  . 
the study of only the coronary district produced the following values : ctdi volume per la ricostruzione dei dati grezzi corrispondenti alle fasi telesistolica ( 35% r - r ) e meso - telediastolica ( 65%70% rr )  . 
nei casi con fc di base elevata ( > 80 bpm ) , la migliore fase per la ricostruzione delle immagini risultata la telesistole ( 35% dellintervallo r - r )  . 
sulla base delle informazioni fornite dallesame , la paziente stata esclusa dal trattamento e dimessa evitando ulteriore accertamento diagnostico con esame coronarografico e prolungamento della ospedalizzazione . infine , nel gruppo di pazienti in cui lindicazione clinica allesame tcms - 64 era stata posta sulla base di test funzionali ecocardiografici ( n = 11 ) o scintigrafici ( n = 3 ) non conclusivi , in 6 / 14 casi sono state evidenziate immagini tcms64 compatibili con stenosi coronariche emodinamicamente significative ( mono o multivasali ) e clinicamente silenti ( fig . 7 ) ; solamente in questi 6 pazienti stato successivamente effettuato lesame coronarografico convenzionale . aspetti dosimetrici il ctdi volumetrico ( ct dose index volume ) stato in media di 36 , 538 , 30 mgy per paziente con un range compreso m . 
volume rendering reconstruction shows complete occlusion of the stent positioned in the proximal part of the vessel ( short arrow ) , with compensatory enlargement of the first diagonal branch ( long arrow ) ( a )  . thanks to the high spatial resolution achievable using a collimation of 0.6 mm , the stents metallic structure is visualised in detail ( b )  . 
4a - d coronarografia con tcms - 64 per follow - up di stent posizionato su arteria discendente anteriore 3 anni prima ; elaborazione delle immagini effettuata con workstation siemens utilizzando software syngo inspace 4d . 
le immagini ricostruite con algoritmo in volume rendering mostrano occlusione dello stent posizionato nel tratto prossimale della da ( freccia corta ) e lipertrofia compensatoria del primo ramo diagonale , che appare tortuoso ed aumentato di calibro ( freccia lunga ) ( a )  . 
nel particolare ( ingrandito ) lelevata risoluzione spaziale dellacquisizione a 0 , 6 mm di collimazione , permette di ottenere dettagli fini come la chiara definizione della trama metallica dello stent ( b )  . 
i pazienti sottoposti a studio dei by - pass coronarici , a causa del pi ampio volume cranio - caudale acquisito , presentavano valori medi di ctdi volumetrico pi elevati ( 38 , 77 , 9 mgy ) con un milliamperaggio effettivo di circa 645 , 389 , 8 . 
per il solo studio del distretto coronarico i valori dosimetrici sono risultati i seguenti : ctdi volumetrico 33 , 036 , 39 mgy , effective mas 498 , 1693 , 27 . il valore medio di ctdi volumetrico a cui sarebbe stato m . 
volume rendering image shows patency of the arterial y - shaped mammary graft connected with the left anterior descending ( lad ) artery and the first marginal branch ( arrow ) ; in the same reconstruction , venous conduit occlusion is observed at the proximal anastomosis level ( arrowhead )  . 
le immagini ricostruite con tecnica volume rendering dimostrano perviet del bypass arterioso ad y con arteria mammaria interna sinistra ( amis ) su da e primo ramo marginale ottuso ( freccia ) ; nelle stesse scansioni si evidenzia occlusione del graft aorto - coronarico venoso allorigine , con caratteristica estroflessione sulla parete aortica dellanastomosi prossimale ( punta di freccia )  . discussion patient exposure to ionising radiation is the main limitation to the clinical use of 64 - mdct , especially if it is to be used as a potential screening tool in asymptomatic patients . 
despite the patients high heart rate during image acquisition ( 96 bmp ) , maximum intensity projection ( mip ) reconstructions ( a ) show multiple stenotic lesions on the right coronary artery ( arrows ) , with subocclusive stenosis at the proximal third of the vessel . 
a 60% stenosis is also observed in the proximal portion of the left anterior descending ( lad ) artery , caused by soft tissue plaque ( arrow ) ( b )  . 
della paziente al momento dellacquisizione ( 96 bpm ) , le ricostruzioni mip ( a ) documentano la presenza di multiple alterazioni stenosanti lungo tutto il decorso della coronaria destra ( frecce ) con stenosi subocclusiva in corrispondenza del terzo prossimale del vaso . 
le ricostruzioni sono state effettuate con workstation siemens e software syngo inspace 4d . sottoposto il paziente senza lutilizzo della tecnica di modulazione risultato di 54 , 690 , 89 mgy con differenza statisticamente significativa tra ctdi volumetrico con sistema care dose e senza care dose ( p < 0 , 001 )  . 
come noto , lutilizzo del gating cardiaco retrospettivo comporta una continua e relativamente elevata esposizione del paziente ai raggi x per la necessit di effettuare lacquisizione dei dati durante lintera durata della scansione e di registrare contemporaneamente i dati dellecg per poi ricostruire le immagini in una fase definita del ciclo cardiaco [ 1 , 2 , 7 , 36 ]  . altra peculiarit tecnica dellimaging tcms delle arterie coronarie lutilizzo di bassi valori di pitch spirale ( pitch di 0 , 2 con tcms - 64 ) e notevolmente sovrapposti ( pitch < numero di strati ) che nasce dallesigenza di effettuare il campionamento dei dati per la ricostruzione delle immagini da strati sovrapposti e privi di gap nel volume acquisito , ma comporta un ulteriore significativo aumento della dose di esposizione [ 7 , 36 , 38 ]  . 
in aggiunta , rispetto alle precedenti generazioni , nella tcms - 64 lutilizzo di collimazioni submillimetriche ( 640 , 6 mm ) si associa ad un intrinseco incremento del rumore nelle immagini acquisite che pu essere limitato aumentando lamperaggio ( intensit di corrente emessa dal tubo radiogeno ) durante la scansione stessa per mantenere il rapporto segnale / rumore entro ottimali livelli diagnostici . nel nostro studio , il ctdi volume risultato in media di 36 , 538 , 30 mgy per paziente , con valori medi di 38 , 77 , 9 mgy nei pazienti con richiesta clinica per studio dei by - pass coronarici con un valore medio di mas di 567 , 83108 , 35 . rispetto ai dati disponibili in letteratura che riportano per apparecchiature a 4 e 16 canali rispettivamente ctdi volume medi di 3645 , 6 mgy e 43 , 3 mgy [ 35 ] , lutilizzo del sistema di modulazione della dose ha consentito di ottenere nella nostra popolazione valori medi di dose assorbita complessivamente inferiori rispetto alle precedenti generazioni tcms pur mantenendo una buona qualit diagnostica degli esami effettuati . 
i valori di dose efficace ottenuti sono risultati in media di 9 , 53 , 4 msv . malgrado in alcuni pazienti si siano raggiunti anche i 17 , 1 msv , questo dato preliminare , sempre se confrontato con i valori di dose efficace riportati in letteratura con apparecchiature a 4 e 16 strati ( rispettivamente 7 , 111 , 9 msv e 8 , 8 msv ) dimostra come , nella media dei pazienti , tale parametro dosimetrico non risulti significativamente superiore rispetto a quelli riportati con precedenti sistemi tcms [ 3841 ]  . 
appare tuttavia rilevante sottolineare come , a prescindere dallimpiego di sistemi di controllo dosimetrico , lesame tcms - 64 delle coronarie con cardiosincronizzazione comporti una esposizione del paziente in termini di dose efficace quasi doppia rispetto ai 57 msv di un esame tc standard del torace [ 38 , 42 ]  . nella nostra esperienza preliminare , lutilizzo del sistema care dose 4d appare quindi indispensabile per mantenere lesposizione del paziente entro livelli accettabili consentendo di ridurre lesposizione media del paziente del fig . 
7 a 64 - mdct angiography performed in a patient with atypical chest pa multiplanar reconstruction ( mpr ) of left anterior descending ( lad ) artery shows diffuse coronary artery disease with multiple vessel wall abnormalities ; note the presence of a noncalcified soft - tissue - attenuation lesion ( arrowheads ) in the proximal part of the artery , causing a > 60% narrowing of the lumen . 
la ricostruzione multiplanare ottenuta su piano curvo ( cpr ) lungo lasse longitudinale della da , documenta multiple alterazioni parietali a densit mista in corrispondenza del tratto prossimale dellarteria discendente anteriore ( da ) e la presenza di placca a densit mista , prevalentemente morbida , con riduzione significativa ( > 60% ) del lume vasale ( punte di freccia )  . 
lelaborazione delle immagini effettuata con workstation siemens utilizzando software syngo inspace 4d . to record ecg data to reconstruct images in a precise phase of the heart cycle [ 1 , 2 , 7 , 36 ]  . another technical peculiarity coronary artery mdct is the use of low spiral pitch ( 0.2 pitch with 64 - mdct ) and considerable overlap ( pitch < < number of slices ) , which arises from the need to sample data for image reconstruction with overlapping slices and no gap , but this leads to a further significant increase in radiation exposure [ 7 , 36 , 38 ]  . 
8 nella figura viene riportata la distribuzione del ctdi volumetrico ( in mgy ) utilizzando il sistema di compensazione care dose 4d , espresso in funzione del carico anodico effettivo . 
it should be borne in mind , however , that regardless of the use of an automatic dose control system , the 64 - mdct examination of the coronary arteries with cardiac gating involves exposing the patient to almost twice the effective radiation dose of a standard ct chest examination ( 57 msv ) [ 38 , 42 ]  . in our preliminary experience , the use of the care dose 4d systems appears indispensable for maintaining exposure within acceptable levels , allowing a 33.5% reduction in mean exposure compared with a similar acquisition performed without an automatic dose control syste the overall dose can be further reduced ( up to 50% compared with an acquisition without care dose 4d ) by using an ecg pulsing system , which is based on the premise that the best phase in the heart cycle for image reconstruction is the mid to end diastole , that is , the maximum immobility phase of the heart and coronary arteries [ 43 ]  . 
in this manner , during data acquisition , tube current is brought to the maximum level in the midto end - diastolic phase , where the maximum snr is required , and progressively reduced to the minimum towards the end - systolic phase . failure to use an ecg pulsing protocol in our study population derives from the evidence that the best rr interval for image reconstruction , especially in patients with elevated hr , is the end - systolic phase ( 30%35% ) , thus confirming the initial experience of wintersperger et al . 
the reduced snr of images acquired in the systolic phase resulting from an acquisition with an ecg 33 , 5% rispetto ad una analoga acquisizione senza modulazione automatica della corrente . 
la dose complessiva pu essere ulteriormente ridotta ( fino al 50% rispetto ad una acquisizione senza protocollo care dose 4d ) utilizzando un sistema di modulazione ecg - controllato dellemissione del tubo radiogeno ( sistema ecg - pulsing ) che si basa sul presupposto che la miglior fase del ciclo cardiaco nella quale effettuare la ricostruzione delle immagini sia la meso - telediastole , cio la fase di maggiore immobilit del cuore e delle arterie coronarie [ 43 ] ; in tal modo , durante lacquisizione dei dati , la corrente del tubo radiogeno viene portata a livello massimo in fase meso - telediastolica , dove necessario avere un massimo rapporto segnale / rumore e ridotta progressivamente al minimo verso la telesistole . la mancata utilizzazione di un protocollo di modulazione ecg - controllato nella nostra popolazione di pazienti deriva tuttavia dallevidenza che , particolarmente in pazienti con elevata fc , il migliore intervallo r - r per la ricostruzione delle immagini risultato essere la fase telesistolica ( 30%35% ) confermando liniziale esperienza riportata da wintersperger et al . 
although the technique needs to be validated with systematic comparisons with clinical , laboratory and coronarographic data , the latest generation of 64 - mdct scanners offers new possibilities for clinical management of patients with coronary artery disease . the increase in spatial and temporal resolution translates into improved diagnostic image quality with respect to previous generations of multidetector devices . 
thus , 64 - mdct is a noninvasive technique capable of identifying patients requiring interventional or surgical procedures such as selective coronarography with primary angioplasty or stent placement , or surgical revascularisation with bypass grafts . the use of suitable systems for the automatic control of radiation exposure seems nonetheless indispensable in order to limit patient dose , which given the current state of affairs is the main limitation to the clinical use of the technique . nella nostra esperienza clinica iniziale , lutilizzo della tcms - 64 ha fornito risultati molto promettenti . 
bolzano , italy , tel . : + 39 - 047 - 1908494 , fax : + 39 - 047 - 1908908 , e - mail : mosavr@yahoo.com received : 23 june 2006 / accepted : 27 july 2006 / published online : 22 february 2007 abstract purpose . 
cta is fast and relatively noninvasive , and its sensitivity appears similar to that of dsa in detecting and evaluating intracranial aneurysms , even those smaller than 3 mm . this study confirms the value of cta as the primary imaging technique in subarachnoid haemorrhage , with dsa reserved for selected patients . key words multislice ct angiography cerebral aneurysm riassunto obiettivo . 
in un periodo di 20 mesi 130 pazienti con diagnosi tc di emorragia subaracnoidea acuta non traumatica sono stati arruolati per uno studio prospettico e sottoposti ad angiotc multistrato ( 16 detettori ) ed angiografia digitale sottrattiva ( 57 maschi , 73 femmine ; et media 59 , 5 anni )  . 
langio - tc una metodica veloce e poco invasiva e la sua sensibilit nellindividuazione degli aneurismi analoga a quella dellangiografia digitale sottrattiva anche se di dimensioni inferiori ai 3 mquesto studio conferma la validit dellangiotc come tecnica di imaging di elezione nella diagnosi di emorragie subaracnoidee . 
langiografia digitale sottrattiva pu essere riservata solo a pazienti selezionati . parole chiave angio - tc multistrato aneurisma cerebrale introduction introduzione nontraumatic subarachnoid haemorrhage ( sah ) is a neurological emergency characterised by extravasation of blood into the spaces lining the central nervous system , which are normally filled with liquor . 
nonaneurysmal sah , including the perimesencephalic end systolic area ( esa ) , is in contrast characterised by a good prognosis and rare neurological complications [ 2 ]  . the global incidence of sah , which varies from region to region , is about 10.5 cases per 100 , 000 inhabitants per year and has remained stable over the last 30 years . 
the main negative prognostic factors include level of consciousness , age and the quantity of blood at initial head computed tomography ( ct ) scan [ 3 , 4 ]  . the principle variable risk factors are cigarette smoking , hypertension , use of cocaine and alcohol abuse . 
first - degree family members of patients with sah have an increased risk ; there are also hereditary diseases of the connective tissue associated with intracranial aneurysms and sah , such as polycystic kidney disease , ehlers - danlos syndrome ( type iv ) , pseudoxanthoma elasticum and fibromuscular dysplasia [ 5 ]  . on the basis of these prognostic criteria , an sah should always be suspected in patients with the typical presentation of sudden and severe headache associated with nausea , vomiting , neck stiffness , photophobia or loss of consciousness . the physical examination may reveal retinal haemorrhage , evidence of meningeal irritation , reduced level of consciousness and / or focal or unilateral neurological deficit . 
this fact supports the extensive use of ct that , if correctly performed , is capable of identifying an sah in 100% of cases within 12 h of symptom onset and in 93% of cases within 24 h [ 7 , 8 ]  . 
head ct is also able to identify the presence of intraparenchymal haematomas , hydrocephalus , cerebral oedema and , in some cases , can suggest the probable site of aneurysmal rupture [ 9 ]  . 
lumbar puncture is a valuable diagnostic examination in cases of negative ct and suspected sah . for exact localisation of the source of extravasated blood , the diagnostic protocol involves performing digital subtractive angiography ( dsa ) or ct angiography ( cta )  . 
whereas dsa is the gold standard for identifying cerebral aneurysms , cta is gaining increasing acceptance , thanks to its immediacy and noninvasiveness and a specificity and sensitivity comparable with dsa . 
cta also has a significant advantage in that it can be performed immediately following the baseline ct examination , which enables a significant shortening of examination times and the possibility of initiating treatment immediately [ 1023 ]  . the aim of this paper is to present a consecutive series of 130 patients diagnosed with sah in a single institution ( ospedale centrale regionale di bolzano ) who underwent cta and / or dsa and to analyse their sensitivity , specificity and diagnostic accuracy , comparing them with the data in the literature . le normalmente percorsi da liquido cerebrospinale . 
lesa non aneurismatica , inclusa lesa perimesencefalica , caratterizzata da buona prognosi e rare complicanze neurologiche [ 2 ]  . lincidenza mondiale aggregata dellesa , che varia da regione a regione , di circa 10 , 5 casi / 100000 abitanti per anno ed rimasta stabile negli ultimi 30 anni . 
i familiari di primo grado di pazienti con esa hanno fattore di rischio aumentato ; vi sono inoltre patologie ereditarie del tessuto connettivo associate ad aneurismi intracranici ed esa quali la malattia policistica renale , la sindrome di ehlers - danlos ( tipo iv ) , lo pseudoxantoma elastico e la displasia fibromuscolare [ 5 ]  . sulla base di tali dati prognostici unesa deve essere sempre sospettata in pazienti con presentazione tipica : cefalea violenta ed improvvisa associata a nausea , vomito , dolore cervicale , fotofobia o perdita di coscienza . 
in assenza dei classici segni e sintomi la diagnosi di esa pu essere confusa con diagnosi di emicrania e cefalea muscolo - tensiva in circa il 50% dei casi [ 6 ]  . 
tali dati supportano luso estensivo che viene fatto della tomografia assiale computerizzata ( tc ) che , se eseguita correttamente , in grado di rivelare unesa nel 100% dei casi entro 12 ore dallesordio sintomatologico e nel 93% entro 24 ore [ 7 , 8 ]  . 
la tc del cranio inoltre in grado di discriminare la presenza di ematomi intraparenchimali , idrocefalo , edema cerebrale e pu , in alcuni casi , suggerire la probabile sede della rottura aneurismatica [ 9 ]  . 
la rachicentesi mantiene una validit diagnostica nel caso di tc negativa e quadro clinico sospetto per esa . il percorso diagnostico prevede quindi , per lesatta localizzazione della sorgente del sanguinamento , lesecuzione di unangiografia digitale sottrattiva ( dsa ) oppure di un angiotc ( atc )  . 
lo studio angiografico cerebrale a sottrazione digitale rappresenta il gold standard per levidenziazione degli aneurismi cerebrali ; latc viene sempre pi utilizzata per limmediatezza e la non invasivit associate a specificit e sensibilit comparabili con la dsa . 
contrast enhancement was provided by the intravenous antecubital administration of an 80ml bolus of nonionic iodinated contrast material ( iomeron 350 mgi / ml , bracco , milan , italy ) at a 4 - ml / s flow rate followed by 50 ml saline solution at the same rate . 
the sample volume was positioned in an internal carotid artery with a threshold of + 30 hu . after acquisition data transfer to the postprocessing station ( leonardo , siemens , erlangen , germany ) , image analysis was performed interactively by the radiologist using various postprocessing techniques , including two ( 2d ) and three - dimensional ( 3d ) multiplanar reconstructions ( mpr ) , maximum intensity projections ( mip ) and volume rendering ( vr )  . each cta and dsa examination was assessed independently by the performing radiologist , and the aneurysms were classified according to the following scheme ( table 1 ) : site : aneurysms originating from the anterior circulation : internal carotid artery , ophthalmic artery , anterior choroidal artery , anterior communicating artery , anterior cerebral artery ( a1 , a2 ) , pericallosal artery , callosal - marginal artery , middle cerebral artery ( m1 , m2 , m3 ) , posterior communicating artery aneurysms originating from the posterior circulation : basilar artery , apex of the basilar artery , posteroinferior cerebellar artery , anteroinferior cerebellar artery , anterosuperior cerebellar artery , posterior cerebral artery . size : giant aneurysms : 25 mm large aneurysms : 1325 mm medium aneurysms : 513 mm small aneurysms : 35 mm very small aneurysms : < 3 mm nel periodo compreso tra giugno 2004 e febbraio 2006 ogni paziente con diagnosi tc di esa non traumatica stato sottoposto a atc ( somatom sensation 16 , siemens , erlangen , germania ) e , successivamente , a dsa ( multistar plus top , siemens , erlangen , germania )  . 
sono stati arruolati 130 pazienti consecutivi , 57 maschi e 73 femmine con et media di 59 , 515 , 2 anni ( range 2091 anni ) ; 91 pazienti provenienti dal pronto soccorso dellospedale centrale regionale di bolzano e 39 da altre strutture ospedaliere . latc stata eseguita con sistema a 16 detettori ( somaton sensation 16 , siemens , erlangen , germania ) con i seguenti parametri di acquisizione e ricostruzione : scansione sul piano assiale estesa dal soma della prima vertebra cervicale al vertice , collimazione 0 , 75 mm , tempo di rotazione 0 , 5 s , fov 230 mm , feed / rot 6 , 5 , 120 kv , 210 mas , ricostruzione in tempo reale 3 mm / 3 mm con fov 120 , ricostruzione per il postprocessing 1 mm / 0 , 5 mm con fov 80 . 
per lopacizzazione arteriosa sono stati somministrati in bolo , per via endovenosa antecubitale , 80 ml di mezzo di contrasto iodato non ionico ( iomeron 350 mgi / ml , bracco , milano , italia ) al flusso di 4 ml / s seguiti da 50 ml di soluzione salina allo stesso flusso . 
in the event of positive cta , only those patients whose cta findings were not complete for the purposes of surgical planning or were to undergo endovascular therapy were required to undergo dsa . 
cta and dsa findings were compared with regard to sensitivity , specificity and diagnostic accuracy . angioarchitettura : presenza o meno di vasi ad origine dalla sacca aneurismatica . tutti i pazienti con atc negativa sono stati sottoposti entro 48 ore a dsa . 
in caso di atc positiva sono stati inviati allo studio angiografico solamente i pazienti con quadro atc non esaustivo ai fini della programmazione chirurgica o quelli indirizzati allapproccio terapeutico endovascolare . infine , quando i reperti atc sono stati giudicati sufficienti per la pianificazione chirurgica , i pazienti sono stati sottoposti allintervento chirurgico senza ulteriori esami diagnostici . 
i dati atc ed angiografici sono stati confrontati in termini di sensibilit , specificit ed accuratezza diagnostica . all cta and dsa examinations were technically assessable . all patients who presented for the cta examination without assisted ventilation were studied without sedation ; about 60% of these required sedation at dsa . 
all cta and dsa procedures were without complications ( allergic reactions , acute renal failure or extravasation at the site of venous injection , more serious neurological complications or complications at the site of arterial catheterisation )  . all 21 patients with a negative cta underwent dsa . 
of the 109 patients with positive cta , 79 underwent emergency dsa to clarify the cta findings and plan therapy , and five underwent dsa during endovascular embolisation on average 13 days after the acute event ( 135.5 days , range 720 days )  . 
in 25 cases , the cta findings were considered complete for surgical purposes , such that these patients unrisultati tutti gli esami atc e dsa eseguiti sono risultati tecnicamente valutabili . 
tutte le procedure eseguite , atc e dsa , sono state esenti da complicazioni ( reazioni allergiche , ira o stravasi in sede di iniezione venosa , complicanze neurologiche maggiori o nella sede di cateterismo arterioso )  . tutti i 21 pazienti con atc negativa sono stati sottoposti a dsa . 
tra i 109 pazienti con atc positiva 79 sono stati sottoposti a dsa urgente per chiarire i reperti atc al fine della pianificazione terapeutica , 5 hanno eseguito lo studio angiografico durante la procedura di embolizzazione endova1325 513 total dimensioni ( mm ) 1325 513 totale results m . 
1 percorso diagnostico dei 130 pazienti arruolati nello studio . derwent dsa post - operatively only . of the 105 patients who underwent dsa , cta findings were confirmed in 104 : in 20 cases where the findings were negative and in 84 cases with the presence of one or more aneurysms . 
in 25 casi il quadro atc stato giudicato esaustivo ai fini dellintervento chirurgico , pertanto questi pazienti sono stati sottoposti a dsa solo come controllo post - operatorio . tra i 105 pazienti sottoposti a dsa il quadro atc stato confermato in 104 : in 20 casi per la negativit del reperto ed in 84 per la presenza di uno o pi aneurismi . 
solo in un caso la dsa ha dimostrato la presenza di un aneurisma del circolo anteriore delle dimensioni di 2 mm non riconosciuto allatc ; lidentificazione di questo piccolo aneurisma stata comunque possibile alla valutazione retrospettiva delle immagini . 
nei 25 pazienti sottoposti al trattamento chirurgico senza la valutazione dsa pre - operatoria stata riscontrata unottima corrispondenza tra le informazioni fornite dallatc ed il quadro chirurgico per quanto riguarda le dimensioni , la morfologia e langioarchitettura . 
2a - i a 41 - year - old woman : axial ( a ) , coronal ( b ) and sagittal ( c ) multiplanar reconstruction ( mpr ) images show a large aneurysm at the bifurcation of the left middle cerebral artery . 
axial ( d ) , coronal ( e ) and sagittal ( f ) maximum intensity projection ( mip ) images obtained with a 10 - mm - thin section more clearly show the aneurysms morphology , its multilobular profiles and relationship with surrounding vessels . 
volume rendering ( vr ) posteroanterior image ( h ) better shows vessels of cranial base and the aneurysvr and transparent vr images ( i ) : this last reconstruction shows a better three - dimensional ( 3d ) image of the aneurysmal sac and surrounding vessels . 
le ricostruzioni mpr assiale ( a ) , coronale ( b ) e sagittale ( c ) dimostrano un aneurisma di grandi dimensioni alla biforcazione dellarteria cerebrale media di sinistra . 
le ricostruzioni mip a strato sottile ( 10 mm ) assiale ( d ) , coronale ( e ) e sagittale ( f ) meglio definiscono la morfologia dellaneurisma , i profili polilobati ed i suoi rapporti con i vasi circostanti . 
3a - i a 51 - year - old woman : coronal ( a ) , axial ( b ) , sagittal ( c ) maximum intensity projection ( mip ) and volume rendering ( vr ) ( d - f ) images show a medium - sized aneurysm at the bifurcation of the right middle cerebral artery ( large arrow ) , a small one at the bifurcation of the left middle cerebral artery ( thin arrow ) and a very small aneurysm of the anterior communicating artery ( arrowhead )  . 
le ricostruzioni mip coronale ( a ) , assiale ( b ) , sagittale ( c ) e vrt ( d - f ) dimostrano un aneurisma di medie dimensioni alla biforcazione dellarteria cerebrale media destra ( freccia grande ) , un aneurisma di piccole dimensioni alla biforcazione dellarteria cerebrale media sinistra ( freccia sottile ) ed un aneurisma molto piccolo allarteria comunicante anteriore ( punta di freccia )  . 
4a - d a 38 - year - old woman : axial ( a ) , coronal ( b ) , sagittal ( c ) maximum intensity projection ( mip ) and volume rendering ( vr ) ( d ) images show a medium - sized aneurysm with a long neck of the right internal carotid artery ( arrow )  . 
ricostruzioni mip assiale ( a ) , coronale ( b ) , sagittale ( c ) e vrt ( d ) di un aneurisma di medie dimensioni dellarteria carotide interna destra con lungo colletto ( freccia )  . 
most aneurysms were of medium sized ( n = 67 ; 50% ) , followed by small ( n = 34 ; 25.4% ) , very small ( n = 16 ; 11.9% ) and large ( n = 16 ; 11.9% ) ( table 1 )  . overall , cta identified 108 of the 109 aneurysms seen at dsa and 25 aneurysms confirmed at surgery . 
6a , b a 60 - year - old man : axial ( a ) and coronal ( b ) maximum intensity projection ( mip ) images show a large , partially thrombosed , aneurysm at the bifurcation of the right middle cerebral artery ( arrow )  . 
7a - d an 81 - year - old man : axial ( a ) , coronal ( b ) paracoronal ( c ) maximum intensity projection ( mip ) and digital subtraction angiography ( dsa ) ( d ) images show a large aneurysm ( arrow ) with a wide neck of the significantly calcified left vertebral artery . 
ricostruzioni mip assiale ( a ) , coronale ( b ) , para - coronale ( c ) e corrispettivo dsa ( d ) di un aneurisma di grandi dimensioni con ampio colletto dellarteria vertebrale sinistra ( freccia ) , estesamente calcifica . 
filiforme larteria vertebrale destra ( b , punta di freccia )  . we also encountered excellent agreement between cta and dsa with regard to assessing the aneurysmal neck and angioarchitecture . 
these data were available for 92 of the 134 aneurysms in our study : we excluded the aneurysm not identified at cta , the 25 aneurysms treated surgically prior to dsa and the 16 aneurysms < 3 mm , the small size of which hindered realistic measurement of the neck . 
in 12 medium and large aneurysms prevalently located in the middle cerebral artery , the presence of a vessel originating directly from the aneurysmal sac was identified . complessivamente con atc sono stati riconosciuti 108 dei 109 aneurismi visualizzati con dsa cui vanno sommati i 25 aneurismi confermati allatto chirurgico . 
pertanto i valori di sensibilit e specificit raggiungono rispettivamente il 98 , 8% ed il 100% , la predittivit positiva del 100% e la predittivit negativa del 95 , 2% , con unaccuratezza diagnostica del 99 , 0% ( tabella 2 )  . abbiamo riscontrato unottima corrispondenza tra atc e dsa anche nella valutazione del colletto aneurismatico e dellangioarchitettura ; tali dati sono disponibili per 92 dei m . 
the technological developments of multidetector ct and especially the introduction and diffusion in clinical practice of 16 - slice scanners have led to improved spatialtemporal resolution , thus enabling an accurate and minimally invasive study of cerebral aneurysms , even in the event of acute sah . the possibility of performing cta immediately following a ct diagnosis of sah , along with the noninvasiveness of the technique , speed of execution and high diagnostic sensitivity and specificity , increasingly promote cta as a highly reliable technique in studying cerebral aneurysms . our prospective study involving 130 patients shows that in all cases , cta was technically feasible and was well tolerated by all patients . 
all examinations could be assessed , and there were no major motion artefacts . however , a limitation to our study was the absence of patients who had previously undergone neurosurgery or endovascular embolisation ; hence , we have no direct experience with artefacts caused by metal clips or coiled springs . 
in this respect , it should be noted that previous studies have demonstrated the validity of cta even in the post - operative follow - up [ 24 ]  . shorter acquisition times and increased spatial resolution are two important advantages introduced by 16 - slice scanners . 
the increased acquisition speed not only enables an exclusively arterial acquisition for the entire scan duration but also reduces the incidence of motion artefacts , which can seriously compromise image quality to the point of rendering the images nondiagnostic . 
this should not be underestimated in this type of patient , who is at times drowsy , at times suffering from psychomotor agitation and often uncooperative 134 aneurismi oggetto del nostro studio : abbiamo escluso laneurisma non riconosciuto con atc , i 25 aneurismi trattati chirurgicamente prima dellesecuzione dellangiografia ed i 16 aneurismi < 3 mm le cui piccole dimensioni non consentivano una reale definizione della base dimpianto . 
le due metodiche sono state concordi nel definire 48 aneurismi con colletto stretto e 44 aneurismi a larga base dimpianto . in 12 aneurismi di medie e grandi dimensioni , prevalentemente localizzati allarteria cerebrale media , stata identificata lemergenza di un vaso direttamente dalla sacca aneurismatica . discussione lo studio degli aneurismi cerebrali stato per lungo tempo affidato alla dsa , metodica invasiva , non priva di rischi per il paziente e caratterizzata da lunghi tempi di esecuzione . gli sviluppi tecnologici della tomografia computerizzata multidetettore ed in particolare lintroduzione e la diffusione nella pratica clinica delle apparecchiature a 16 strati , hanno portato ad un miglioramento della risoluzione spazio - temporale permettendo uno studio accurato e poco invasivo degli aneurismi cerebrali anche in caso di esa in fase acuta . la possibilit di effettuare latc subito dopo la diagnosi tc di esa , la non invasivit e la rapidit di esecuzione associate ad elevate sensibilit e specificit diagnostiche propongono sempre pi latc quale metodica altamente affidabile nello studio degli aneurismi cerebrali . questo studio prospettico relativo a 130 pazienti evidenzia che latc si dimostrata tecnicamente sempre eseguibile e ben tollerata dal paziente ; tutti gli esami sono risultati valutabili , in particolare non si sono registrati grossolani artefatti da movimento . per contro un limite di questo studio lassenza di pazienti gi precedentemente sottoposti ad interventi neurochirurgici o ad embolizzazione endovascolare : non abbiamo quindi esperienza diretta con gli artefatti da clips o spirali metalliche . 
a tale riguardo va aggiunto che precedenti studi hanno dimostrato la validit dellatc anche nei controlli post - operatori [ 24 ]  . la riduzione dei tempi di acquisizione e laumento della risoluzione spaziale sono due importanti vantaggi introdotti dagli apparecchi a 16 strati . 
la maggiore velocit di acquisizione non solo consente di ottenere unacquisizione esclusivamente arteriosa per tutta la durata della scansione , ma riduce lincidenza degli artefatti da movimento che possono inficiare la qualit delle immagini sino a renderle non diagnostiche . 
questo aspetto non va sottovalutato in questa tipologia di paziente : talvolta soporoso , talvolta in stato di agitazione psicomotoria e spesso comunque poco collaborante e poco incline a mantenere limmobilit del capo anche per pochi secondi . 
per nessuno dei pazienti sottoposti ad atc stata necessaria la sedazione , al contrario pi della met dei pazienti sottoposti a dsa ha richiesto lintervento dellanestesista al fine di ottenere immagini diagnostiche , prive di artefatti da movimento . un esame atc viene eseguito in circa 10 minuti cui va m . 
in contrast , a cerebral dsa study requires angiographic experience , and when performed by an expert has a duration of 4560 min , to which is added about 10 min for reporting the findings . the move from 4to 16 - slice devices has further increased spatial resolution . 
various studies performed with 4slice scanners have already demonstrated excellent diagnostic accuracy regarding aneurysms larger than 4 mm while underlining the limitations for smaller aneurysms [ 14 , 17 , 20 , 25 ]  . 
 mpr , which were assessed in cine mode in the three orthogonal planes in space , help confirm the presence of the aneurysm or determine whether it was not identified in the axial plane alone . 
mpr performed in various oblique planes or curved mpr along the vessel course helps define the relations with the surrounding vascular and bone structures and the size of the sac and neck , as well as parietal calcifications and partial thromboses . 
nonetheless , these easy - to - use reconstructions return a plastic , 3d - like image of the main vascular branches for most of their course , which often helps in the recognition of aneurysmal protrusions . 
these reconstructions , which are the most similar to traditional angiographic images , can be applied particularly sommato un tempo medio di elaborazione - lettura delle immagini di circa 1520 minuti : il referto quindi disponibile dopo 2530 minuti dallarrivo del paziente alla tc . 
al contrario lesecuzione di una panangiografia cerebrale richiede esperienza angiografica ed in mani esperte ha una durata media di 4560 minuti cui vanno sommati circa 10 minuti per la refertazione . il passaggio dai 4 ai 16 strati ha incrementato ulteriormente la risoluzione spaziale : questo ha permesso di aumentare le potenzialit diagnostiche dellatc soprattutto nellambito degli aneurismi di dimensioni molto piccole . 
diversi studi , condotti con apparecchi a 4 strati , hanno gi dimostrato lottima accuratezza diagnostica per gli aneurismi di dimensioni superiori ai 4 mm e sottolineato i limiti per quelli di dimensioni pi piccole [ 14 , 17 , 20 , 25 ]  . 
le ricostruzioni mpr secondo vari piani obliqui o mpr curvate lungo il decorso di un vaso aiutano a definire i rapporti con le strutture vasali ed ossee , le dimensioni della sacca e del suo colletto , calcificazioni parietali o trombosi parziali . le ricostruzioni in proiezione di massima intensit ( mip ) proiettano nel piano di ricostruzione solo i voxel pi luminosi del volume scelto : si tratta di ricostruzioni bidimensionali con perdita dellinformazione spaziale . 
tuttavia queste ricostruzioni , di facile applicazione , ci restituiscono unimmagine plastica , simil - 3d , delle principali diramazioni vasali per gran parte del loro decorso che spesso aiuta nel riconoscimento delle protrusioni aneurismatiche . 
le ricostruzioni mip , le pi vicine allimmagine angiografica tradizionale , trovano applicazione soprattutto nella valutazione delle diramazioni arteriose che si allontanano dal poligono di willis mentre non consentono una valutazione corretta delle strutture in stretto rapporto con la base cranica per lelevata attenuazione dellosso . 
it should also be borne in mind that very small aneurysms can be masked by vascular structures if the latter are projected in the same plane as the reconstruction . vr is a 3d reconstruction technique that requires definition of a threshold attenuation value ( measured in hounsfield units ) for selecting reconstruction voxels . 
these images help in interpreting the vascular relations and can be used to help in surgical planning , as they simulate the intraoperative view . postprocessing performed with a reduced fov enables improved spatial resolution . 
reconstructions in the various planes in space enable recognition and therefore sufficiently adequate characterisation of morphology , size , neck and development of an aneurysm as well as its relation to adjacent vessels and surrounding structures . 
the volumetric reconstructions , which are easy to obtain and have a high visual impact , return a plastic image that is often more useful in defining the aneurysms relations and development than in diagnosing it . 
it should also be borne in mind that only thin - section mpr , which are more laborious and less intuitive , enable correct identification of small irregularities of the sacs profile or partial thrombosis , where present . conclusions our study confirms the data in the literature . 
the ability of cta to define the relevant anatomical characteristics for surgical treatment , such as aneurysmal neck morphology , parietal calcification , sac thrombosis and relations with adjacent structures , as well as 3d reconstruction of the neurovascular angioarchitecture means that fundamental additional information can be supplied for deciding the next treatment steps . the results obtained in this study confirm the data in the literature and encourage the use of cta in routine clinical practice , with recourse to dsa only in selected cases or cases with uncertain diagnosis . 
at our institute , this study determined a change in managing patients with acute nontraumatic sah : in the event of positive cta finding for the presence of an aneurysm , in most cases , patients are scheduled for surgery without undergoing a dsa study . given the aetiology of nontraumatic sah and its highlevel of risk in the event of an incorrect diagnosis , fundamental requisites for cta study include correct technical execution and careful and interactive image assessment : where there is doubt , patients should undergo dsa . 
with regard to the future , cta is also a promising technique for follow - up to verify exclusion of the aneurysmal sac after endovascular or surgical procedures . essere mascherati dalle strutture vascolari se queste si proiettano nello stesso piano di ricostruzione . lelaborazione volume rendering technique ( vrt ) una tecnica di ricostruzione tridimensionale che richiede la definizione di un valore soglia di attenuazione ( in unit hounsfield ) per la selezione dei voxel di ricostruzione . 
queste immagini facilitano linterpretazione dei rapporti vascolari e possono essere di aiuto nella pianificazione dellapproccio chirurgico , simulando la visione intraoperatoria . le rielaborazioni con field of view ( fov ) ridotto consentono una migliore risoluzione spaziale : le ricostruzioni secondo i vari piani dello spazio permettono di riconoscere e quindi di caratterizzare in maniera adeguata morfologia , dimensioni , base dimpianto e sviluppo di un aneurisma oltre ai suoi rapporti con i vasi adiacenti e le strutture circostanti . 
le ricostruzioni volumetriche ( vrt ) facili da ottenere e di sicuro impatto visivo , restituiscono unimmagine plastica spesso pi utile nella definizione dei rapporti e dello sviluppo dellaneurisma che non nella sua diagnosi ; sono spesso richieste dai neurochirurghi perch meglio rispecchiano la spazialit e la visualizzazione intraoperatoria . 
non va dimenticato tuttavia che solo le ricostruzioni multiplanari sottili , pi laboriose e meno intuitive , ci consentono di identificare correttamente eventuali piccole irregolarit dei profili della sacca o la sua parziale trombosi . conclusioni questo studio conferma i dati della letteratura : latc una metodica poco invasiva , rapida , altamente sensibile e specifica nella diagnosi di aneurismi cerebrali nelle esa . 
la capacit dellatc di definire caratteristiche anatomiche rilevanti per il trattamento chirurgico quali la morfologia del colletto aneurismatico , le calcificazioni parietali , la trombosi della sacca ed i rapporti con le strutture adiacenti e la ricostruzione tridimensionale dellangioarchitettura neurovascolare consentono di fornire informazioni aggiuntive fondamentali per decidere il successivo trattamento dei pazienti . 
nella nostra realt questo studio ha determinato un cambiamento nella gestione del paziente con esa acuta non traumatica : in caso di reperto angio - tc positivo per la presenza di un aneurisma la maggior parte dei pazienti viene portata allintervento chirurgico senza lesecuzione della dsa . considerando leziologia dellesa non traumatica e la sua pericolosit in caso di errata diagnosi , uno studio atc non pu prescindere da unesecuzione tecnicamente corretta e da una valutazione attenta ed interattiva delle immagini : nei casi dubbi il ricorso alla dsa rappresenta tuttora lopzione di scelta . 
bonomo , i - 70031 andria ( ba ) , italy 2dipartimento di scienze radiologiche , irccs casa sollievo della sofferenza , i - 71013 san giovanni rotondo ( fg ) , italy 3dipartimento di radiologia , fondazione s . 
giglio , cefal ( pa ) , italy 4istituto di radiologia , universit di novara , italy 5istituto di radiologia , universit di ancona , italy correspondence to : t . 
scarabino , via napoli 56 , i - 70031 andria ( ba ) , italy , tel . : + 39 - 0883 - 299140 , fax : + 39 - 0883 - 299220 , e - mail : tscarabino@hotmail.com received : 19 may 2006 / accepted : 12 july 2006 / published online : 22 february 2007 abstract ever since the introduction of magnetic resonance ( mr ) , imaging with 1.5 tesla ( t ) has been considered the gold standard for the study of all areas of the body . 
indeed , their high gradient power and field intensity ( 3.0 t ) allow adjunctive and more advanced diagnostic methodologies to be performed with excellent resolution in a fraction of the acquisition time required with earlier machines . 
pi recentemente , lintroduzione di unit rm con intensit di campo di 3 , 0 t per applicazioni cliniche nuove ed avanzate ha comportato notevoli vantaggi , soprattutto in campo neuroradiologico . 
i loro alti gradienti ed intensit di campo infatti consentono di applicare metodologie diagnostiche nuove ed avanzate con eccellente risoluzione in una frazione del tempo di acquisizione richiesto dalle attrezzature precedenti . 
continuous advances in hardware ( gradients , coils ) and software ( acquisition and processing sequences ) have made magnets more compact , powerful and flexible , greatly improving patient comfort . 
higher - field units were introduced some years ago for clinical research purposes , principally in neuroradiology , and are spreading fast ( especially in the usa ) despite their dallavvento della risonanza magnetica ( rm ) le apparecchiature con intensit di campo magnetico di 1 , 5 tesla ( t ) sono considerate il gold standard per coprire le varie applicazioni cliniche in tutti i distretti corporei . 
tali apparecchiature , in virt di continui progressi che hanno interessato lhardware ( gradienti , bobine ) e il software ( sequenze di acquisizione e di elaborazione ) , sono diventate sempre pi compatte , potenti e versatili , con conseguente migliore confort del paziente . 
they are being employed not only in research and with a broader scope compared with traditional research but also in daily clinical practice to support new and sophisticated clinical applications , with considerable practical benefits . 
in the first year , the machine was employed to optimise the various morphological and functional acquisition sequences ( diffusion , perfusion , spectroscopy , cortical activation ) both in vitro ( using dedicated dummies ) and in vivo ( in healthy controls ) and the various postprocessing techniques ( with dedicated software ) with a view to creating a large database as the starting point for research on patients . 
naturally , special attention was devoted to the safety problems related to the machines use , especially issues of patient comfort in the tunnel and compatibility of various biomedical devices . after optimisation of study sequences and protocols , our research programme focused on improving morphofunctional mr imaging of the bra the higher signal - to - noise ratio ( snr ) of the 3.0 - t magnet made it possible to obtain images with greater spatial , contrast and time resolutions in shorter acquisition times compared with lower - field systems , resulting in greater patient comfort and reduction of motion artefacts . the patients studied at 3.0 t exhibited a wide and representative range of conditions that were successfully investigated using standardised dedicated sequences and protocols . 
disadvantages , which include a greater specific absorption rate ( sar ) , greater acoustic noise are not particularly severe and in newer systems are largely reduced by improved hardware and software [ 14 ]  . 
tali sistemi sono ormai diventati una realt e , nonostante lalto costo , si stanno sempre pi diffondendo ( specie in usa ) per essere utilizzati non solo nel campo della ricerca , peraltro molto pi ampia rispetto alla ricerca tradizionale , ma anche e soprattutto nella pratica clinica quotidiana per far fronte a nuove e pi sofisticate applicazioni cliniche con conseguenti importanti benefici pratici . da 5 anni il servizio di neuroradiologia del nostro istituto scientifico dotato di una apparecchiatura rm whole body ( signa horizon lx , general electric medical system , milwaukee , usa ) dotata di magnete superconduttivo , a schermatura attiva , con intensit di campo magnetico 3 , 0 t , gradienti di potenza di 50 millitesla al metro ( mt / m ) e slew rate di 150 mt / m / s . 
il sistema rm 3 , 0 t in dotazione stato utilizzato nel primo anno di lavoro , una volta acquisita lautorizzazione ministeriale alluso , per ottimizzare le diverse sequenze di acquisizione , morfologiche e funzionali ( diffusione , perfusione , spettroscopia , attivazione corticale ) , sia in vitro ( utilizzando fantocci dedicati ) che in vivo ( con controlli sani ) , e le diverse modalit di post - processing ( utilizzando software dedicati ) al fine di creare un ampio database , punto di partenza per studi di ricerca su paziente . 
naturalmente , particolare attenzione stata data alle problematiche di sicurezza inerenti luso di tale apparecchiatura ( con riferimento in particolare alla qualit di confort del paziente in esame e alla rm - compatibilit di vari dispositivi biomedicali )  . ottenuta lottimizzazione di sequenze e protocolli di studio , lobiettivo del nostro programma di ricerca stato quello di migliorare limaging morfo - funzionale cerebrale con rm . 
sfruttando il pi alto rapporto segnale / rumore ( s / r ) possibile con lapparecchiatura 3 , 0 t , stato infatti possibile ottenere immagini con pi alta risoluzione spaziale , di contrasto e temporale , in tempi peraltro ridotti rispetto ai sistemi di pi basso campo , con conseguente miglioramento del confort del paziente e riduzione degli artefatti da movimento . i pazienti sottoposti a rm 3 , 0 t hanno esibito un ampio e rappresentativo spettro di patologia che stata esaminata adeguatamente utilizzando sequenze e protocolli ben definiti e personalizzati . si quindi proceduto allo studio di diverse patologie seguendo le linee dei progetti di ricerca approvati dalla direzione scientifica del nostro istituto , previa autorizzazione del comitato etico . 
lo scopo del lavoro quello di illustrare le caratteristiche semeiologiche peculiari dellimaging cerebrale morfologico e angiografico a 3 , 0 t mettendo in risalto i relativi vantaggi e svantaggi rispetto a sistemi rm di pi basso campo . studio morfologico di base gli studi rm del cervello possono essere suddivisi in due grandi categorie , morfologici e funzionali , sulla base del tipo di informazione che si ricerca . 
lo studio morfologico di base ( detto anche convenzionale o anatomico ) riguarda limaging di tessuto , spazi periliquorali , vascolatura e fasci di fibre , mentre lo studio funzionale in senso lato comprende lo studio delle funzioni cerebrali ( fmri ) limaging di perfusione t . 
 because the user interface and sequence parameters are the same as those employed with 1.5 - t systems , at 3.0 t , in theory , the same images should be obtained with the advantage of high - field strength , i.e. 
 t1 imaging as t1 relaxation times are longer at higher magnetic fields , entailing reduction in the relative differences among different tissue types , it is generally difficult to obtain t1 - weighted images with sufficient contrast when using a 3.0 - t unit [ 6 ]  . 
for this reason , snr optimisation in the same sample using a higher - field unit requires longer time to repetition ( tr ) [ and a smaller flip angle ( fa ) ] , resulting in longer scanning times . 
t1 saturation for a given tr is greater at 3.0 t , resulting in reduced signal gain . in other words , the snr per unit of time would be optimised with the shortest possible tr / t1 . 
the possibility that the snr gain connected with the high magnetic field may substantially be offset by a longer t1 highlights the importance of optimising the imaging parameters [ 3 ]  . 
 e di diffusione , e lo studio metabolico con la spettroscopia . lo studio di rm di base si presenta a 3 , 0 t con un imaging di qualit pi alta rispetto a quello ottenuto a pi basso campo in virt di una serie di vantaggi quali un pi alto rapporto s / r , una maggiore risoluzione spaziale e temporale a fronte di alcuni svantaggi , quali lincremento del specific absorption rate ( sar ) e del rumore acustico , peraltro non particolarmente significativi e comunque in gran parte risolvibili mediante hardware e software di pi recente introduzione [ 14 ]  . 
dato che i tempi di rilassamento sono campo - dipendenti e influenzano il contrasto dellimaging , le sequenze di imaging a 1 , 5 t non possono infatti essere trasferite a 3 , 0 t . 
a ci si aggiunge la deposizione tissutale dellenergia di rf che , essendo eccessiva , va anche considerata per adattare e ottimizzare i protocolli clinici di imaging per luso a 3 , 0 t . 
 fast spgr allows thinner slices to be obtained in a shorter time and provides images suitable for reformatting in all three planes using a single volumetric acquisition of the whole brain , thus disclosing a larger number of lesions than can be depicted using se t1 - weighted sequences acquired in a single plane . 
infatti , non solo il t1 aumenta con laumentare del campo magnetico , ma addirittura converge , determinando una distribuzione meno ampia dei valori di t1 tra i diversi tipi di tessuto . 
per tale motivo per ottimizzare il rapporto s / r dello stesso campione a campo pi alto il tr deve essere pi lungo ( come anche il flip angle deve essere pi corto ) con conseguente allungamento dei tempi desame . utilizzando tr pi lunghi , il vantaggio in intensit di segnale a campo pi alto risulta essere inferiore in unit di tempo . la saturazione t1 per un dato tr infatti pi ampia a 3 , 0 t con conseguente riduzione del guadagno in segnale . 
quindi in virt del fatto che il guadagno nel rapporto s / r derivante dallalto campo pu essere sostanzialmente controbilanciato dallallungamento del t1 , risulta importante lottimizzazione dei parametri di imaging [ 3 ]  . lincremento del t1 rappresenta il pi grande problema per lo studio cerebrale a 3 , 0 t acquisito con sequenza se t1 pesata in cui il contrasto t1 appunto inaccettabile [ 1 , 2 , 4 , t . 
for instance , when studying primary and secondary brain tumours , administration of a gadolinium - based agent yields greater contrast between tumour and normal brain tissue both in single and in multiple doses . 
it also detects more metastases and demonstrates different patterns of enhancement that may be useful to assess the degree of malignancy and monitor response to therapy [ 2628 ]  . 
the greater sensitivity of 3.0 - t contrast - enhanced investigations has also been demonstrated in multiple sclerosis , with a 21% increase in the number of enhancing lesions detected , a 30% increase in enhancing lesion volume and a 10% increase in total lesion volume relative to scanning at 1.5 t [ 29 ]  . 
using a standard dose , the contrast - to - noise ratio ( cnr ) is two and a half times greater than with 1.5 - t systems [ 13 ]  . 
double or triple doses can result in meningeal contrast uptake , a common nonpathological finding at 3.0 t that at lower field strengths may , however , mimic carcinomatosis or meningitis and should thus be avoided . 
to enhance sensitivity or highlight minimal changes in the blood - brain barrier , a double dose of contrast agent may be employed in selected investigations of brain metastases or inflammatory disease [ 30 , 31 ]  . 
high spatial resolution fast spin echo ( fse ) - weighted images are especially effective at 3.0 t , as they provide more anatomical detail and better contrast due to the greater snr , which allows the use of thinner slices and broader matrices [ 1 , 2 , 4 , 32 ]  . 
tale sequenza inoltre caratterizzata da ipersegnale delle grosse strutture vascolari arteriose che comunque non inficia linterpretazione delle immagini . mentre gli studi t1 pesati sono tradizionalmente meno informativi e richiedono pi tempo , un tipico studio flair t1 pesato del cervello consente , insieme allutilizzo dellimaging parallelo , lapplicazione di protocolli a pi alta risoluzione con tempi desame pi brevi rispetto ai campi ad intensit 1 , 5 t . 
naturalmente tale aspetto diventa problematico se dobbiamo acquisire pi studi , senza e con mdc , o pi proiezioni . in rapporto al maggiore effetto inflow del mdc e alla maggiore soppressione del fondo , limaging t1 con mdc sicuramente un vantaggio del 3 , 0 t rispetto al 1 , 5 t . 
nello studio ad esempio dei tumori cerebrali primitivi e secondari la somministrazione del gadolinio produce un maggior contrasto tra lesione tumorale e parenchima normale sia a singola dose e a dose multipla , permette di rilevare un maggior numero di metastasi , pu dimostrare differenti pattern di impregnazione che risultano utili per definire il grado di malignit e per monitorare la risposta alla terapia [ 2628 ]  . 
rispetto al 1 , 5 t infatti alcuni autori hanno documentato un incremento del 21% del numero delle lesioni con impregnazione patologica , del 30% nel volume di impregnazione e del 10% del volume totale delle lesioni [ 29 ]  . 
il rapporto contrasto / rumore ( c / r ) risulta infatti maggiore rispetto allo studio con sistemi rm 1 , 5 t ( di ben 2 , 5 volte ) utilizzando una dose standard [ 13 ]  . 
da evitare la dose doppia o tripla responsabile di impregnazioni meningee , reperti comuni non patologici a 3 , 0 t ( con sistemi 1 , 5 t tali quadri possono simulare una carcinomatosi o una meningite )  . 
3 imaging fse t2 ad alta definizione della sezione mediana del cervello . infiammatoria per incrementare la sensibilit o per stressare le minime alterazioni della barriera emato - encefalica ( bee ) , una dose doppia pu essere preferita [ 30 , 31 ]  . 
di solito nello studio t1 con mdc la fast ge t1 pesata viene preferita , al posto delle tradizionali se , che presentano un contrasto minore a parit di tempo dacquisizione . 
ne consegue una migliore risoluzione spaziale ( e quindi maggiore dettaglio anatomico ) e di contrasto , possibili per effetto di un pi alto rapporto s / r che permette luso di spessore di strato inferiori e di matrici pi ampie [ 1 , 2 , 4 , 32 ]  . 
2a , b studio di microadenoma ipofisario prima ( a ) e dopo mdc endovena ( b ) con sequenza fse - xl t1 ( tr / te 600 / 12 , etl 5 , fov 180 mm , spessore di strato 2 , 5 mm / 0 , 5 , matrice 224192 , zip 512 , 29 / fase )  . creased deposition of radiofrequency ( rf ) energy , which in turn requires long tr or pulse refocalisation angles well below 180 . 
in addition , the broader bandwidth , smaller echo space , shorter minimum tr and te and shorter fse sequences employed at higher field strengths result in improved image quality , artefact reduction and enhanced diagnostic performance in much shorter examination times , which is to the patients benefit . 
these sequences allow excellent visualisation of the basal or mesencephalic nuclei by virtue of their iron content despite the intrinsically lower sensitivity of fse to magnetic susceptibility in 3.0 - t compared with 1.5 - t systems [ 5 ]  . 
4a - d high - definition ( hd ) study of the inner ear using a 3d fast imaging employing steady state acquisition ( fiesta ) sequence [ time to repetition ( tr ) 4.3 , echo time ( te ) 1.5 , flip angle ( fa ) 50 , band width ( bw ) 62 khz , field of view ( fov ) 170 , slice thickness 0.6 mm , matrix 256256 , zero fill interpolation processing ( zip ) 512 , 2 , number of excitations ( nex ) , 4 : 43 ]  . 
4a - d studio ad alta definizione dellorecchio interno con sequenza 3d fiesta ( tr / te 4 , 3 / te 1 , 5 , flip angle 50 , bw 62 khz , fov 170 , spessore di strato 0 , 6 mm , matrice 256256 , zip 512 , 2 nex , 4 : 43 ) : singole partizioni ( a ) , zoom ( b ) , mip ( c ) , elaborazione con ricostruzione di volume ( d )  . rhage , which at 3.0 t is characterised by greater hypointensity in the acute and early subacute phases [ 33 ]  . 
 flair imaging flair sequences , which are generally included in all imaging protocols , are also sharper and more sensitive at 3.0 t sono pi bassi , quindi il tempo in fse si riduce , la qualit aumenta , gli artefatti si riducono . 
con tale sequenza sono ben apprezzabili i nuclei della base o del mesencefalo che risaltano maggiormente ( per effetto del loro contenuto di ferro ) , nonostante la nota intrinseca minore sensibilit alla suscettibilit magnetica della fse , rispetto a sistemi 1 , 5 t [ 5 ]  . una variazione di semeiotica del segnale sembra interessare anche le emorragie cerebrali caratterizzate in particolare da una maggiore ipointensit a 3 , 0 t in fase acuta e subacuta precoce rispetto allintensit di segnale rilevabile a 1 , 5 t [ 33 ]  . 
a tal proposito il c / r e lintensit di segnale a 1 , 5 t e 3 , 0 t sono sostanzialmente equivalenti per cui di solito comunque non vi sono particolari problemi per interpretare correttamente let dellemorragia . 
first , it allows performance of all angiographic sequences applied routinely in clinical practice with lowerfield systems , such as 2d and 3d time of flight ( tof ) and phase contrast ( pc ) , as well as ultrafast dynamic sequences acquired after contrast agent bolus administration [ contrastenhanced mra ( ce - mra ) ]  . 
as with routine mr scanning , the technical parameters of angiographic sequences need to ge ( t2 * ) quali ad esempio la ciss ( constructive interference in the steady state ) particolarmente indicata nello studio dellorecchio interno . 
la maggiore sensibilit si ha anche grazie alluso di te pi lunghi , necessari per i tempi di rilassamento modificati a 3 , 0 t , che permettono un buon contrasto ed un rumore accettabile . 
il rilievo di piccole lesioni richiede infatti lottimizzazione del c / r piuttosto che del rapporto s / r e questo viene ottenuto appunto con te pi lunghi ( 120 ms ) anche se tale allungamento incrementa oltre il contrasto anche il rumore ma in modo accettabile . inoltre , contrariamente a quanto accade per sistemi 1 , 5 t , in virt della sostanziale mancanza di differenza del t1 del liquor ( che essenzialmente un liquido ) tra 1 , 5 t e 3 , 0 t , il tempo di inversione ( ti ) richiesto per annullare il liquor rimane dello stesso valore ( 2 , 250 millisecondi circa ) [ 5 ]  . tale caratteristica non valida in altre sequenze ir , sia in quelle in cui si cerca di massimizzare il contrasto tra differenti tessuti ( ad esempio tra sostanza bianca e sostanza grigia ) sia in quelle con soppressione del grasso , nelle quali invece il ti deve essere incrementato del 25%40% . 
le note aree di sostanza bianca soprattutto periventricolare fisiologicamente iperintense con sistemi a pi basso campo ( 1 , 5 t ) sono ancora pi accentuate a 3 , 0 t per cui c bisogno di una particolare attenzione per distinguerle da patologie reali ( ad esempio sclerosi laterale amiotrofica ) [ 1 ]  . 
in addition , the change in t1 relaxation time , namely , increased t1 , yields greater background suppression of stationary tissues due to the decrease of r1 , i.e. 
the rate of longitudinal or spin - lattice relaxation , with greater flow enhancement , as blood r1 is roughly constant thereby improving vessel - tissue contrast [ 19 , 22 , 36 ]  . 
this advantage makes magnetisation transfer application less effective than it is with 1.5 t systems [ 37 , 38 ]  . the effect is mainly evident using the 3d tof technique , as the short tr usually saturates stationary tissues but not moving blood [ 7 , 39 ] , and the tag persists for a longer time . these effects lead to greater vessel detail and conspicuity , especially in disclosing small - calibre vessels , including surface vessels not clearly depicted at 1.5 t [ 23 , 25 ]  . 
il recente sviluppo di nuovi hardware ( nuove coil ) o lutilizzo di pi recenti software ( imaging parallelo ) potranno ridurre tale inconveniente . studio angiografico con il 3 , 0 t lo studio angiografico si avvantaggia in modo significativo rispetto a sistemi rm di pi basso campo ( fig . 7 ) [ 1 , 2 , 4 , 35 ]  . 
innanizitutto un sistema rm a 3 , 0 t permette di eseguire tutte le sequenze angiografiche utilizzate di solito nella pratica clinica con sistemi a pi basso campo quali le pi comuni time of flight ( tof ) o phase contrast ( pc ) , entrambe con modalit 2d o 3d , od anche quelt . 
therefore , contrast administration further improves imaging at 3.0 t due to the high snr , which can be transformed into spatial resolution : resolution on a plane le ultrarapide utilizzate con tecnica dinamica dopo somministrazione a bolo del mdc ( contrast enhancement magnetic resonance angiography , ce - mra )  . 
tale vantaggio , che rende peraltro non particolarmente efficace ( come invece accade con sistemi 1 , 5 t ) luso della magnetization transfer ( mt ) [ 37 , 38 ] apprezzabile soprattutto quando si utilizza la tecnica angiografica 3d tof in quanto il breve tr satura di solito i tessuti stazionari ma non il sangue in movimento [ 7 , 39 ]  . 
tali effetti comportano un incremento del dettaglio e della conspicuity vascolare con in particolare evidenza di vasi di pi piccolo calibro , anche superficiali ( di iv ordine ) , non chiaramente identificabili con sistemi rm 1 , 5 t [ 23 , 25 ]  . per lo stesso motivo lutilizzo di campi magnetici elevati ( 3 , 0 t ) sembra in grado di migliorare la cospicuit dei vasi intracranici del neonato o di ridurre ulteriormente i tempi di acquisizione [ 40 ]  . 
lo studio angio - rm a 3 , 0 t in pazienti portatori di tali dispositivi biomedicali ( purch gi testati ) pu essere quindi eseguito senza particolari rischi [ 33 , 45 ]  . i benefici ottenuti a 3 , 0 t , evidenti soprattutto nella patologia vascolare malformativa ( specie aneurismatica ) e atefig . 
time - resolved imaging of contrast kinetics ( tricks ) images [ 3d time of flight spoiled gradient recalled ( tof - spgr ) , time to repetition ( tr ) 3.7 , echo time ( te ) 1.3 , matrix 224192 , slice thickness 1.8 mm , field of view ( fov ) 28 , temporal resolution 2.5 s , 8 phases ] of multiple vascular phases : contrast enhancement of arteries ( a ) , capillaries ( b ) and veins ( c )  . 
in tale modo possibile visualizzare diverse fasi vascolari : arterie ( a ) , capillari ( b ) e vene ( c )  . ments are increased at higher - field strengths resulting in artefacts caused by the susceptibility of biomedical devices such as the aneurysm clips commonly used in interventional and therapeutic neuroradiological procedures , the newer devices do not seem to present major safety or compatibility problems [ 42 , 44 ]  . 
resolution quality tends to be privileged in clinical practice , with acquisition of a larger number of slices of rerosclerotica cerebrale , rendono ancora pi competitiva langiografia con rm , nonostante una minore risoluzione spaziale rispetto allangiografia convenzionale ( dsa ) , ormai sempre pi utilizzata in campo intervenzionistico - terapeutico piuttosto che diagnostico [ 46 ]  . conclusioni grazie al suo alto rapporto s / r , la mri ad alto campo in grado , di supportare nuove applicazioni diagnostiche o di migliorare le metodiche esistenti . 
in virt dellalto rapporto s / r il neuroradiologo pu scegliere di eseguire un imaging cerebrale a 3 , 0 t in un tempo uguale a quello ottenibile con un sistema 1 , 5 t privilegiando in tal caso una pi alta qualit delle immagini ( incrementando la matrice e / o riducendo lo spessore di strato e / o il fov ) oppure di avere un imaging di qualit pari al quello di un sistema 1 , 5 t in un tempo inferiore privilegiando in tal caso il confort del paziente , od anche pu scegliere di ridurre la dose del mezzo di contrasto somministrato . 
di solito nella pratica clinica si cerca di privilegiare la risoluzione acquisendo pi fette , di spessore sottile , con campi di vista pi piccoli , con matrici pi ampie e in tempi comparabili a quelli con i sistemi 1 , 5 t . 
spesso in rapporto al quesito clinico e al tipo di paziente in esame , si cerca di trovare un compromesso tra risoluzione e velocit ( riducendo ad esempio il numero delle eccitazioni ) [ 34 ]  . lalto rapporto s / r per effetto dellalto campo pu in realt essere ottenuto anche a 1 , 5 t utilizzando i pi recenti hardware ( bobine riceventi di superficie , single o in arrays ; gradienti pi performanti capaci di ridurre il te ) e t . 
however , this cannot be done in the case of unstable or poorly co - operative patients , or it may be impossible for cost reasons ( reduced patient flow )  . 
lastly , the higher snr of high - field mr systems is a resource that neuroradiologist can exploit in clinical practice , as the higher the snr , the more the imaging protocols can be adjusted . acknowledgments to technical staff : c . 
il caso di pazienti instabili , non collaboranti , come anche ci possono essere altre motivazioni ad esempio di natura economica ( la riduzione del flusso dei pazienti )  . 
non solo , anche a 1 , 5 t possibile un incremento delle dimensioni della matrice : in tal caso per la conseguente riduzione delle dimensioni del voxel comporterebbe maggiore granulosit dellimaging . 
pertanto il maggiore rapporto s / r da alto campo sicuramente unottima arma che il neuroradiologo pu sfruttare nella pratica clinica : maggiore il rapporto s / r , maggiori sono infatti le possibilit del neuroradiologo di modificare i protocolli di imaging . rigraziamenti allo staff tecnico : c . 
bonomo , i - 70031 andria ( bat ) , italy 2dipartimento di scienze radiologiche , irccs casa sollievo della sofferenza , i - 71013 san giovanni rotondo ( fg ) , italy 3dipartimento di radiologia , fondazione s . 
giglio , cefal ( pa ) , italy 4dipartimento di fisica , irccs stella maris , pisa , italy 5istituto di radiologia , universit di napoli , italy 6istituto di radiologia , universit di pisa , italy 7istituto di neurologia , universit di campobasso , italy 8istituto di psichiatria , universit di bari , italy 9istituto di radiologia , universit politecnica delle marche , ancona , italy correspondence to : t . 
scarabino , via napoli 56 , i - 70031 andria ( bat ) , italy tel . : + 39 - 0883 - 299140 , fax : + 39 - 0883 - 299220 , e - mail : tscarabino@hotmail.com received : 19 may 2006 / accepted : 8 september 2006 / published online : 22 february 2007 abstract the aim of this paper is to illustrate the technical , methodological and diagnostic features of functional imaging ( comprising spectroscopy , diffusion , perfusion and cortical activation techniques ) and its principal neuroradiological applications on the basis of the experience gained by the authors in the 5 years since the installation of a high - field magnetic resonance ( mr ) magnet . these mr techniques are particularly effective at 3.0 tesla ( t ) owing to their high signal , resolution and sensitivity , reduced scanning times and overall improved diagnostic ability . 
the most common perfusion study ( with intravenous injection of a contrast agent ) benefits from the greater snr and higher magnetic susceptibility by achieving dramatically improved signal changes , and thus greater reliability , using smaller doses of contrast agent . functional mr imaging ( fmri ) is without doubt the modality in which high - field strength has had the greatest impact . 
images acquired with the blood - oxygen - level - dependent ( bold ) technique benefit from the greater snr afforded by 3.0 - t magnets and from their stronger magnetic susceptibility effects , providing higher signal and spatial resolution . 
this enhances reliability of the localisation of brain functions , making it possible to map additional riassunto lo scopo del lavoro quello di illustrare le caratteristiche tecnico - metodologiche e semeiologiche dellimaging funzionale ( comprendente lo studio di spettroscopia , diffusione , perfusione , attivazione corticale ) con cenni sulle principali applicazioni in campo neuroradiologico sulla base dellesperienza acquisita in 5 anni dallinstallazione di unapparecchiatura ad alto campo . 
tali modalit di studio rm risultano particolarmente migliorate a 3 , 0 t grazie ai numerosi vantaggi ( alto segnale , alta risoluzione , alta sensibilit , tempi ridotti , alta capacit diagnostica )  . 
ne consegue uno studio spettroscopico ad alta risoluzione , in tempi peraltro ridotti , non solo dei metaboliti comuni ma anche e soprattutto di quelli che , in virt della loro bassa concentrazione , difficilmente sono rilevabili con sistemi 1 , 5 t . 
lo studio di perfusione pi diffuso ( con mdc esogeno ) , in virt del maggiore s / r e della pi alta suscettibilit magnetica a 3 , 0 t , caratterizzato da variazioni di segnale drasticamente migliorate con conseguente maggiore affidabilit utilizzando peraltro minori quantit di mdc . 
le immagini ottenute con la tecnica bold infatti se ne avvantaggiano a 3 , 0 t in virt del maggiore s / r e dei maggiori effetti di suscettibilit magnetica con conseguente pi alto segnale e pi alta risoluzione spaziale . 
the data presented and results obtained to date show that 3.0 - t morphofunctional imaging can become the standard for highresolution investigation of brain disease . in definitiva sulla base dei risultati finora ottenuti , si evince che limaging morfo - funzionale ottenuto a 3 , 0 t potr in futuro diventare lo standard per lo studio ad alta definizione della patologia cerebrale . key words magnetic resonance fmri high field parole chiave risonanza magnetica imaging funzionale con rm alto campo introduction introduzione the function of the new 3.0 - tesla ( t ) magnetic resonance ( mr ) systems is to enable high spatial , contrast and time resolution morphological investigation of the brathis is essential for diagnosis but also indeed , especially to provide physiological , metabolic and functional information capable of enhancing the diagnostic power of standard mr in terms of sensitivity and specificity . 
it is well established that standard mr , the modality of choice to investigate pathological central nervous system ( cns ) conditions , is not despite its high sensitivity suitable for characterising all brain tissue abnormalities . 
hence the need for integrating morphological parameters with physiological , metabolic and functional data that may predate anatomical changes , thus promoting early diagnosis and treatment and therefore better patient outcomes . 
these data can also be obtained with mr , especially if high - field units are used . the aim of the work was to illustrate technical , methodological and diagnostic characteristics of functional mr imaging ( fmri ) [ including spectroscopy ( mrs ) , diffusionweighted imaging ( dwi ) , perfusion - weighted imaging ( pwi ) and cortical activation ] and its main neuroradiological applications based on a 5 - year experience with a high - field magnet . 
the material presented comes from work performed by the medical and technical team of the neuroradiology and physics unit of our institution in collaboration with largely italian and some foreign neuroradiologists , neuropsychiatrists , neurophysiologists , psychologists , bioengineers , physicists and other neuroimaging experts . 
the work is supplemented with literature data from other similar experiences to provide an exhaustive review of the state of the art of this field . proton spectroscopy il ruolo dei nuovi sistemi di risonanza magnetica ( rm ) 3 , 0 t deve essere quello di permettere uno studio morfologico cerebrale ad alta risoluzione spaziale , temporale e di contrasto , essenziale per la diagnosi , ma anche e soprattutto di fornire informazioni fisiologiche , metaboliche e funzionali , capaci di aumentare il potere diagnostico della rm di base in termini di sensibilit e specificit . 
a tutti noto che lo studio morfologico di base con rm , considerato lesame delezione per patologie del sistema nervoso centrale , nonostante la sua indubbia sensibilit , non sempre specifico nel caratterizzare tessuto cerebrale anomalo . 
da qui la necessaria integrazione dei parametri morfologici con quelli fisiologici , metabolici e funzio nali individuabili anche con rm , specie se eseguito con apparecchiature ad alto campo , che possono invece precedere le alterazioni anatomiche , favorendo una diagnosi e un trattamento precoci e quindi un migliore outcome del paziente . lo scopo del lavoro quello di illustrare le caratteristiche tecnico - metodologiche e semeiologiche dellimaging funzionale con rm ( comprendente lo studio di spettroscopia , diffusione , perfusione , attivazione corticale ) con cenni sulle principali applicazioni in campo neuroradiologico . 
il materiale raccolto in questo lavoro frutto dellesperienza acquisita in 5 anni dallinstallazione di tale apparecchiatura da parte dellequipe medica e tecnica delle unit operative di neuroradiologia e di fisica sanitaria del nostro centro in collaborazione con neuroradiologi , neuropsichiatri , neurofisiologi , psicologi , bioingegneri , fisici o comunque esperti di neuroimaging il cui apporto multidisciplinare essenziale per sfruttare al massimo le potenzialit di tale apparecchiatura . 
lo scritto stato completato con i risultati di altre esperienze similari raccolte dalla letteratura al fine di fornire uno stato dellarte completo sulla tematica in oggetto . the increased signal - to - noise ratio ( snr ) and greater spatial and temporal chemical shift resolution of high - field units yield improved spectroscopic imaging compared with lowerfield mr [ 17 ]  . increment of snr and chemical - shift resolution studio di spettroscopia protonica con lalto campo la spettroscopia migliora rispetto ai pi bassi campi grazie ad un incremento del rapporto segnale / rumore ( s / r ) , della risoluzione del chemical shift , spaziale e temporale [ 17 ]  . in theory , the passage from 1.5 - t to 3.0 - t systems should double the snr ; in practice , however , the improvement is only around 20%46% . 
a linear rise would only be possible if other factors , such as t1 and t2 relaxation time values or the radiofrequency ( rf ) effect did not change significantly incremento del s / r e della risoluzione del chemical shift teoricamente , il s / r dovrebbe raddoppiare passando da 1 , 5 t a 3 , 0 t , ma in pratica il miglioramento solo del 20%46% . 
to this should be added the coils lower sensitivity and poorer volume homogeneity as well as registration errors caused by the wider chemical shift , which can degrade spectra quality , thus partially offsetting the advantages of the higher field [ 46 ]  . even though the position of spectrum peaks is constant on the parts per million ( ppm ) scale [ e.g. 
the greater amplitude of the chemical shift of metabolites yields better spectral resolution and hence a more clear - cut separation between adjacent peaks , which may overlap at lower magnetic field strength . 
the increased linewidth is related to reduced t2 values and heightened local magnetic field inhomogeneity of the higher fields . field inhomogeneity can be reduced by greater and more appropriate shimming . 
the same holds for gammaaminobutyric acid ( gaba ) , usually obscured at 1.5 t by a number of other substances , including macromolecules , cr , glutamine , glutamate and extracerebral lipid contamination . two different techniques can be adopted to detect the signal from coupling protons : ( 1 ) te averaging , with acquisition of different te with subsequent sampling capable of separating selected metabolites ; and ( 2 ) editing , using additional selective rf pulses with acquisition of the sole coupled spin signal [ 9 , 10 ]  . 
the wider range of chemical - shift frequencies found at higher magnetic fields enables the use of selective pulses at lower frequency , thereby shortening the te . increment of spatial resolution in high - field magnets , voxel size can be reduced without a significant loss in snr [ 11 ]  . 
a ci vanno aggiunti la pi bassa sensibilit della bobina e la pi bassa omogeneit del suo volume , la presenza di errori di misregistrazione da pi largo chemical shift che possono degradare la qualit dello spettro vanificando in parte i vantaggi dellalto campo [ 46 ]  . anche se la posizione dei picchi dello spettro costante utilizzando la scala parti per milione ( ppm ) ( ad esempio il n - acetyl - aspartato , naa a 2 , 02 ppm ) , la frequenza di risonanza differente ( per lnaa 127 hz a 1 , 5 t , 254 hz a 3 , 0 t )  . 
questa maggiore ampiezza di frequenza del chemical shift dei metaboliti permette una migliore risoluzione spettrale e quindi una migliore separazione dei picchi vicini che possono invece sovrapporsi a pi basso campo . 
in realt questo importante vantaggio pu non essere sfruttato del tutto negli studi di spettroscopia in vivo in quanto anche lampiezza del picco ( linewidth ) ( in hz ) dei metaboliti incrementa ( almeno di un fattore due ) per cui la separazione tra i singoli picchi vicini non risulta considerevolmente migliorata a 3 , 0 t . 
lo stesso vale per il gaba di solito oscurato in uno studio condotto con rm 1 , 5 t da una serie di altre sostanze comprendenti macromolecole , creatina , glutamina , glutamato , contaminazione lipidica extracerebrale . 
1a , b magnetic resonance spectroscopy ( mrs ) glx ( glutamate and glutamine ) : spectra obtained from grey matter in a healthy subject using point - resolved spectroscopy ( press ) ( a ) and echo - time ( te ) - averaged press ( b ) sequences . 
in conventional spectroscopy sequences ( a ) , the resonances between 2 and 2.6 ppm are assigned to a mixture of glutamate ( glu ) and glutamine ( gln ) or glx . 
 incremento della risoluzione spaziale increment of time resolution one of the general limitations of lower - field spectroscopy , the long examination time , can be overcome using high - field units . 
in particular , single - volume spectra can be obtained at 3.0 t with an snr similar to that of 1.5 - t magnets in a quarter of the time , or the time for single - volume three - dimensional ( 3d ) studies can be reduced by 26% using a higher snr than that in 1.5 - t systems [ 12 ]  . 
this increases the number of protocols that can be acquired with different te and enables a larger number of brain regions and larger brain volumes to be analysed . con lalto campo possibile ridurre le dimensioni del voxel , senza una significativa perdita di s / r [ 11 ]  . 
noto che il s / r per unit di tempo della spettroscopia linearmente proporzionale al volume del voxel per cui riducendo il voxel si abbassa anche il s / r . 
a 3 , 0 t voxel al di sotto di 1 cc ( limite a 1 , 5 t ) possono essere ottenuti invece con un buon s / r in un tempo dacquisizione accettabile simile a quanto ottenuto con un 1 , 5 t . 
la pi alta risoluzione spaziale permette di distinguere differenti strutture anatomiche , normali e patologiche con conseguenti significativi vantaggi nello studio di piccole strutture quali lippocampo , i nuclei basali , le placche di sclerosi multipla , piccole lesioni con conseguenti importanti implicazioni cliniche . metabolite quantitation incremento della risoluzione temporale metabolite quantitation , another important problem in spectroscopy , benefits from the advantages offered by higher field strength [ 46 ]  . 
in addition , the relaxation times of individual brain metabolites are inversely proportional to magnetic field strength and present distinct regional variations in brain parenchyma ( especially the t2 of naa ) , probably due to local paramagnetism and different white / grey matter composition [ 14 ]  . 
these features make it possible to increase the b value to enhance the anisotropic effect , thus improving the quality of more complex examinations such as anisotropy , diffusion tensor and tractography ( dti ) , which are poorly displayed on 1.5 - t images , even with multiple excitations , due to insufficient snr [ 15 ]  . 
in fact , reconstructed dti trajectories reflect more accurately the underlying axonal fibres , particularly crossing or bifurcating bundles . uno dei limiti generali della spettroscopia a pi basso campo , e cio i lunghi tempi desame , pu essere superato con lalto campo . 
in particolare possibile ottenere con il 3 , 0 t spettri a volume singolo con s / r similari a 1 , 5 t ma in 1 / 4 di tempo oppure studi a volume singolo 3d possono essere ridotti del 26% mantenendo un pi alto s / r rispetto a 1 , 5t [ 12 ]  . 
ci permette di eseguire pi protocolli , con differenti tempi di eco ( te ) , analizzare pi sedi e pi ampi volumi cerebrali . quantizzazione dei metaboliti in virt dei vantaggi che lalto campo fornisce in spettroscopia , anche la quantizzazione dei metaboliti , altro importante problema della spettroscopia , migliora con lalto campo [ 46 ]  . 
peraltro i tempi di rilassamento dei singoli metaboliti cerebrali , oltre a presentare una proporzionalit inversa con lintensit del campo magnetico , evidenziano distinte variazioni regionali nel contesto del parenchima cerebrale ( specialmente il t2 di naa ) verosimilmente attribuibili al locale paramagnetismo e alla differente composizione sostanza bianca / sostanza grigia [ 14 ]  . 
in rapporto a questultimo parametro e al tipo di metabolita cerebrale in esame dipende il guadagno del segnale in spettroscopia a 3 , 0 t . per effetto della riduzione del t2 con lalto campo , studi di spettroscopia con te lunghi subiscono una maggiore perdita di s / r a 3 , 0 t rispetto a 1 , 5 t ed un incremento della linewidth del picco che peraltro dipende , oltre che dal t2 , dalle disomogeneit microscopiche e macroscopiche del corpo . 
in tal modo possibile incrementare il b - value per aumentare lanisotropicit e quindi migliorare la qualit di fenomeni pi complessi quali lanisotropia , il tensore di diffusione e la trattografia ( dti ) , non chiaramente rilevabili con sistemi 1 , 5 t , pur utilizzando multiple eccitazioni , in quanto il s / r non sufficiente [ 15 ]  . 
inoltre laumento lineare del segnale rm comportando una riduzione degli effetti di volume parziale particolarmente utile per ricostruire il percorso delle fibre con dti in quanto le traiettorie cos ricostruite rispecchiano pi precisamente le fibre assonali sottostanti , particolarmente i fasci che si incrociano o si biforcano . lo studio di diffusione particolarmente utilizzato nel rilievo di lesioni ischemiche iperacute con peraltro b - value t . 
4a , b multimodal magnetic resonance ( mr ) study [ contrast - enhanced spin echo ( se ) t1 , fast spin echo ( fse ) t2 , apparent diffusion coefficient ( adc ) map ] : comparison of low - grade astrocytoma ( a ) to glioblastoma ( b )  . 
4a , b studio rm multimodale ( se t1 dopo mdc , fse t2 e mappa di adc ) : confronto tra astrocitoma a basso grado ( a ) e glioblastoma ( b )  . 
in such cases , parallel imaging or new techniques such as periodically rotated overlapping parallel lines with enhanced reconstruction ( propeller ) radial k - space filling can solve this problein fact , diffusion studies adopt echoplanar techniques in which all phase - encoding steps are acquired with one rf excitation , thus accumulating phase errors responsible for susceptibility effects and image distortion . 
dti data sufficient for brain fibre tracking can be obtained in healthy subjects in < 2 min , with 2mm slice thickness , 700 s / mm2 b factor and at least six motion - probing gradient directions [ 19 ]  . 
a tal proposito usando un sistema a 3 , 0 t queste tecniche di pesatura in diffusione forniscano un maggiore contenuto di informazioni per lo studio dei tumori cerebrali , specialmente per valutare il coinvolgimento della sostanza bianca peritumorale , che pu dimostrare edema e / o infiltrazione neoplastica . 
nei gliomi a basso grado le fibre della sostanza bianca sono solo compresse e dislocate , non infiltrate o distrutte come in quelli ad alto grado : i cambiamenti rilevati alla dti possono quindi dipendere dallinfiltrazione tumorale . 
per questa ragione la dti pu essere considerata un metodo valido per rilevare uninvasione occulta della sostanza bianca da parte del glioma e quindi fornire informazioni utili per pianificare il trattamento [ 17 ]  . un grosso problema dello studio della diffusione a 3 , 0 t t . 
5a - c ischemia cerebrale iperacuta del lobulo parietale destro : dwi ( a ) , mappa di adc ( b ) , main eigenvector map area di interesse ( c )  . weighted acquisitions , avoid ambiguity in reconstructing diffusion tensor parameters , increase the snr and decrease the influence of signal distortion [ 20 ]  . a diffusion sequence based on single - shot fast spin echo ( fse ) has recently been proposed to address the problem of susceptibility , as this sequence is not affected by the spatial distortion that usually limits conventional acquisitions with echoplanar imaging ( epi ) sequences [ 21 ]  . perfusion studies perfusion mr imaging benefits from the advantages of highfield units both in examinations using exogenous contrast agents [ dynamic susceptibility contrast ( dsc ) ] and those based on endogenous contrast agents [ arterial spin labelling ( asl ) ]  . dynamic susceptibility contrast ( dsc ) dsc is without doubt the faster and more widely used technique in clinical practice . 
the higher snr and magnetic susceptibility of 3.0 - t compared with 1.5 - t units result in imrappresentato dalle pi ampie distorsioni delle immagini ( specie in aree di alta suscettibilit , quali ad esempio quelle vicino ai seni paranasali ) , conseguenza dei maggiori effetti di suscettibilit presenti a pi alto campo . 
in questi casi limaging parallelo o luso di nuove tecniche di riempimento del k - space ( cd propeller , periodically rotated overlapping parallel lines with enhanced reconstruction ) possono risolvere tale inconveniente . 
gli studi di diffusione infatti utilizzano tecniche ecoplanari in cui tutti gli step di codifica di fase sono acquisiti con ununica eccitazione di rf con quindi accumulo di errori di fase , causa di effetti di suscettibilit e di distorsione delle immagini . 
utilizzando limaging parallelo a 3 , 0 t , possibile anche ottenere dati del tensore di diffusione ( dti ) sufficienti a seguire il percorso delle fibre in soggetti sani in meno di 2 min con uno spessore di strato di 2 mm , un fattore b - value di 700 s / mm2 , almeno 6 diverse direzioni spaziali di gradienti [ 19 ]  . 
 recentemente per ovviare a tali inconvenienti stato anche proposto luso di una sequenza di diffusione basata su una fast spin echo ( fse ) single shot che non risulta appunto affetta da distorsioni spaziali che di solito invece limitano lacquisizione convenzionale con sequenze ecoplanari ( epi ) [ 21 ]  . studio di perfusione limaging mediante rm con valutazione della perfusione trae vantaggio dalluso di campi magnetici elevati sia utilizzando mezzo di contrasto ( mdc ) esogeno ( dsc , dynamic susceptibility contrast ) che mdc endogeno ( asl , arterial spin labelling )  . dsc sicuramente la pi veloce e la pi usata nella pratica clinica . 
alla potenza di campo di 1 , 5 t la misurazione dei parametri emodinamici limitata dal basso rapporto s / r dato che il passaggio del mdc cos rapido che non consente di raccogliere dati sufficienti a calcolare questi parametri con precisione . 
ci si nota in particolare in condizioni come lischemia , in cui la ipo - perfusione limita la quantit di mdc presente nei voxel . sfruttando lelevato rapporto s / r offerto dai sistemi a 3 , 0 t si possono ottenere informazioni utilizzando voxel pi piccoli ( accentuazione della risoluzione spaziale ) ad intervalli di tempo pi brevi ( incremento della risoluzione temporale )  . i gradienti rapidi inoltre consentono di usare un te breve con risoluzione temporale attorno a 1 s , il tempo necessario per seguire il passaggio del bolo di mdc attraverso lencefalo ed i suoi vasi ematici . 
questo non possibile con apparecchiature da 1 , 5 t in quanto le immagini sono in genere acquisite a bassa risoluzione spaziale per ottimizzare la velocit di acquisizione , ed anche aumentando il numero delle sezioni impossibile analizzare lintero encefalo . inoltre luso frequente nei sistemi a 3 , 0 t di sequenze t2 * pesate con valutazione della presa di contrasto e della perfusione offre alcuni potenziali vantaggi . 
in particolare , tempi di rilassamento t2 e t2 * pi brevi ed un aumentato rapporto s / r [ 24 , 25 ] possono consentire di ottenere una maggiore caduta di segnale t2 * utilizzando la stessa quantit di bolo di mdc nella fase di transito capillare [ 26 ]  . 
a tale proposito , anche se a 1 , 5 t gli studi strutturali dopo somministrazione di mdc sono solitamente effettuati utilizzando 0 , 1 mmol / kg di peso corporeo di mdc , nella maggior parte dei casi si usa 0 , 2 mmol di gadolinio chelato , per gli studi di perfusione dsc [ 23 , 2729 ]  . 
la maggiore sensibilit delle apparecchiature a campo magnetico di 3 , 0 t per la suscettibilit magnetica significa che lo stesso effetto pu essere ottenuto somministrando dosi di mdc paramagnetico molto pi piccole di quelle comunet . 
this cannot be achieved with 1.5 - t devices with which images are usually acquired at low spatial resolution to optimise acquisition speed and , even when the number of slices is increased , the whole brain cannot be covered . the frequent use of t2 * sequences with contrast - enhanced and perfusion studies also offers some potential advantages . 
in particular , shorter t2 and t2 * relaxation times and increased snr [ 24 , 25 ] may allow a greater t2 * signal drop to be obtained for a given amount of contrast bolus during capillary passage [ 26 ]  . 
in this respect , although structural contrast - enhanced brain imaging at 1.5 t is usually performed with 0.1 mmol / kg of body weight , 0.2 mmol of gadolinium chelate is the most widely used dose and is considered optimal for dsc perfusion studies [ 23 , 2729 ]  . 
the enhanced sensitivity of 3.0 - t fields to magnetic susceptibility means that the same effect can be obtained with much smaller doses of paramagnetic contrast medium than those usually injected for lower - field perfusion imaging . 
the dose can even be halved without compromising the sensitivity of intensity / time curves from which the relative cerebral blood volume ( rcbv ) and mean transit time ( mtt ) values are calculated . 
in fact , when using epi sequences , the problems of increased b0 inhomogeneity and magnetic susceptibility differences at airtissue interfaces lead to signal drop - out and geometric distortions , most notably in the phase - encode direction [ 30 ]  . 
 other drawbacks inherent in t2 * sequence susceptibility are systematic overestimation of perfusion due to the difference in relaxivity of the paramagnetic contrast agent between larger vessels ( from which the input function is obtained ) and capillaries , problems defining a good input function because of low spatial resolution on t2 * - weighted epi and , finally , problems assessing a damaged blood - brain barrier . the latter is a critical element in evaluating brain tumour perfusion because relaxivity is different when the contrast agent is confined to a small compartment as opposed to being distributed in the interstitial space [ 31 ]  . 
in particolare , gli effetti di suscettibilit pi forti determinano una completa assenza di segnale in occasione del primo passaggio di gadolinio , specialmente nella sostanza grigia , e compromettono laccuratezza dei calcoli di caduta di segnale nonch la sensibilit ad eventuali deficit di perfusione ( fig . 7 ) [ 23 ] ; la dose pu anche essere dimezzata senza compromettere la sensibilit delle curve intensit / tempo dalle quali si ottengono i valori di volume ematico cerebrale relativo ( rcbv ) e tempo di transito medio ( mtt )  . 
la dose standard di mdc non quindi necessaria per studi di perfusione effettuati a 3 , 0 t , e la dose pu essere ulteriormente ridotta somministrando concentrazioni pi elevate ( 1 molare )  . come per la diffusione anche lo studio di perfusione ad alto campo limitato dai problemi causati dagli artefatti da suscettibilit magnetica che aumentano di pari passo con laumento del campo magnetico . 
a 3 , 0 t infatti la distorsione dellimmagine pu essere critica , in particolare se si usano sequenze epi , come nella maggior parte dei protocolli per gli studi di perfusione dsc . 
infatti lutilizzo delle sequenze epi comporta gli svantaggi di un aumento della disomogeneit del b0 e differenze di suscettibilit magnetica a livello delle interfacce aria - tessuto che determinano una caduta di segnale e distorsioni geometriche evidenti maggiormente nella direzione della codifica di fase [ 30 ]  . 
a 3 , 0 t la maggiore suscettibilit magnetica richiede dosi o concentrazioni inferiori rispetto a sistemi 1 , 5 t ( per cortesia della general electric )  . sequences [ 3d fast field echo ( ffe ) t1 weighted or 3d fast low - angle shot ( flash ) t1 weighted ] [ 31 , 32 ] or selection of appropriate te has recently been proposed to minimise these negative effects [ 33 ]  . 
ne deriva un migliore rapporto s / r in quanto la marcatura decade pi lentamente e , cosa pi importante , una minore sensibilit per differenze del tempo di arrivo arterioso in quanto sono consentiti ritardi pi lunghi post - marcatura . 
tale aumentata sensibilit circa il rapporto s / r pu essere sfruttata per ridurre il tempo di scansione ( meno di 5 min rispetto agli oltre 15 di un sistema a 1 , 5 t ) , per acquisire immagini a pi alta risoluzione o per applicare tempi di ritardo post - marcatura pi lunghi . una recente applicazione della asl limaging del territorio di perfusione regionale al fine di visualizzare il territorio t . 
8a , b perfusion study of a normal brain using an endogenous contrast agent [ arterial spin labelling ( asl ) ] at 1.5 tesla ( t ) ( a ) and 3.0 t ( b )  . 
this results in a better snr because the label decays more slowly . more importantly , it results in less sensitivity to arterial arrival time differences because longer postlabelling delays are enabled . 
such increased snr sensitivity can be harnessed in order to decrease scanning time ( < 5 min compared with > 15 min at 1.5 t ) , acquire higher - resolution images , or apply longer postlabel delay times . a recent application of asl is in the study of regional perfusion territory imaging in order to visualise the vascular territory supplied by a specific labelled vessel . 
selective labelling may be useful in patients with high - grade vascular stenosis or complete vascular occlusion to guide the choice between angioplasty and stenting , evaluate cerebrovascular bypass grafts or estimate the likelihood of an embolic or atherothrombotic event in a patient with multiple bright regions on dwi [ 3742 ]  . 
 it is important to note that at one time the only way to obtain such information was by invasive catheter angiography . these data may be helpful to achieve a better understanding of vascular dynamics in patients at high risk of stroke or those being considered for corrective surgical procedures [ 43 ]  . cortical activation studies functional imaging ( fmri ) is without doubt the field in which the greater snr and magnetic susceptibility effects of 3.0 - t magnetic fields have had the strongest impact , parvascolare irrorato da uno specifico vaso marcato . 
la marcatura selettiva pu essere utile nei pazienti con stenosi vascolare elevata od occlusione completa in modo da guidare la scelta fra angioplastica e stenting , per valutare impianti di by - pass cerebrovascolare , o per stimare la probabilit di eventi aterotrombotici od embolici in pazienti con reperto allimaging pesato in diffusione di molteplici zone a segnale elevato [ 3742 ]  . importante notare che in passato lunico modo per ottenere questa informazione era langiografia per cateterismo selettivo , metodo invasivo . 
tali dati possono essere utili per ottenere una migliore comprensione delle dinamiche vascolari nei pazienti ad alto rischio di ictus o nei pazienti valutati per procedure chirurgiche correttive [ 43 ]  . studio di attivazione corticale sicuramente il settore che si maggiormente avvantaggiato con lalto campo e che , in virt del pi alto s / r e dei maggiori effetti di suscettibilit magnetica , ha avuto limpatto maggiore con in particolare pi elevata risoluzione spaziale e temporale dellimaging funzionale ( fmri )  . per ottenere vantaggi reali dallaumento di risoluzione necessario luso congiunto di strategie di acquisizione in grado di migliorare il rapporto s / r . 
infatti , oltre alla possibilit di migliorare il rapporto s / r intrinseco delle sequenze di impulsi e lutilizzo di antenne ad elevato rapporto s / r , limpiego di unit ad alto campo magnetico la soluzione che ha conseguito il maggiore successo nellaumentare il rapporto s / r per gli studi di attivazione corticale . 
indeed , besides the possibility of improving intrinsic pulse - sequence snr and the adoption of high snr coils , the most successful option for gaining snr is to use high - magnetic - field - intensity fmri units . 
in fact , the difference in magnetic susceptibility between blood which contains paramagnetic deoxyhaemoglobin and surrounding diamagnetic tissue on which difference the bold effect is based increases with the strength of the main magnetic field , determining larger mr signal changes between baseline and activated states if high - field units are used [ 45 ]  . 
as regards the magnitude of the field dependence of the bold effect , it has been considered to vary from linear to quadratic [ 4547 ] , exhibiting an inhomogeneous spatial distribution principally depending on the relationship between voxel dimension and the dimension of blood vessels contained in thein particular , studies of the field dependence of the transverse relaxation rate [ 47 ] showed that the bold effect is proportional to b0 if the voxels contain large vessels ( venules and veins ; d > 10 m ) , and that it drops to less than linear if vessels are larger than voxels . 
another , potentially more important , advantage of the higher b0 is that as the field strength increases , the field gradient around the capillaries becomes larger and extends further into the parenchyma , thus involving a greater amount of brain tissue in producing the functional signal . 
per quanto riguarda lentit della dipendenza delleffetto bold dallintensit del campo magnetico , si ritiene che essa passi da lineare a quadratica [ 4547 ] , con una distribuzione spaziale non omogenea che dipende principalmente dalla relazione fra la dimensione dei voxel e quella dei vasi contenuti al loro interno . 
in particolare studi sulla dipendenza dallintensit di campo dellentit di rilassamento trasversale [ 47 ] hanno dimostrato che leffetto bold proporzionale a b0 nei voxel che contengono vasi pi grandi ( venule e vene con diametro superiore a 10 m ) e cala a una relazione meno che lineare se i vasi sono pi grandi dei voxel . 
un altro vantaggio potenzialmente pi importante dellelevato b0 che con laumento dellintensit di campo il gradiente di campo attorno ai capillari diventa pi grande e si estende maggiormente nel parenchima , coinvolgendo pertanto una maggiore quantit di tessuto cerebrale nella produzione del segnale funzionale . 
nei gradienti di campo i vettori di magnetizzazione allinterno dei voxel possono corrispondere a fasi diverse , determinando una diminuzione del tempo effettivo di rilassamento trasversale t2 *  . contemporaneamente la diminuzione del t2 * del sangue ad elevato b0 riduce il contributo relativo delle grandi vene . cos la pesatura del contributo di segnale proveniente dai capillari diviene pi significativa ed il segnale funzionale pi strettamente correlato con lattivit neuronale [ 4852 ]  . le sequenze ge - epi sono attualmente preferite a sequenze se - epi in quanto consentono una migliore discriminazione dei vasi piccoli dai vasi grandi . 
the map obtained at 3.0 t shows more clearly the spatial extension of the activation , particularly in the supplementary motor area , and a better correspondence of the activated area with the anatomy of the motor systethe intensity of the fmri signal [ blood oxygen level dependent ( bold ) % ] doubles in the passage from the 1.5 - t to the 3.0 - t magnetic field . 
9 mappe di attivazione corticale motoria ottenute sul piano coronale a 1 , 5 t ( sinistra ) e 3 , 0 t ( destra ) durante un esperimento con schema a blocchi e pressione del pulsante alla frequenza di 0 , 5 hz . 
la mappa ottenuta a 3 , 0 t dimostra pi chiaramente lestensione spaziale dellattivazione , specie della regione motoria supplementare , ed una migliore corrispondenza dellarea attivata con lanatomia del sistema motorio . 
lintensit del segnale fmri ( bold% ) raddoppia passando da 1 , 5 t a 3 , 0 t . in synthesis , the use of high magnetic field strength fmri units considerably improves the flexibility and specificity of functional studies . 
thanks to high - field studies , fundamental neural dynamics taking place at a very small dimensional scale in specific laminar , columnar and multicolumnar domains have become directly visible , enabling more reliable localisation of brain functions , with the possibility of mapping additional areas in the millimetre or even submillimetre scale . 
these properties are especially useful when investigating minimal changes and when using paradigms requiring extra snr ( indeed , one method to measure the benefits of high field strengths is to determine the extent of activation elicited by a given paradigm )  . 
 conclusions comparison of data acquired by our team at 3.0 t and lower field strength showed that the numerous and important advantages of high - field morphofunctional imaging ( high signal , resolution and sensitivity , short acquisition times , additional and more advanced applications , enhanced diagnostic potential ) make it a promising candidate as the future standard for the study of pathological brain conditions . 
technological advances are expected to overcome some minimal limitations , such as field inhomogeneity , susceptibility and chemical - shift artefacts , high specific absorption rate ( sar ) , acoustic noise and cost , nonsignificant diagnostic differences , and scarce diffusion . 
these advances will promoting magnetico hanno consentito di visualizzare direttamente dinamiche neurali fondamentali che si verificano a scale di dimensioni molto piccole a livello di strutture laminari , colonnari e multicolonnari . 
tale beneficio particolarmente apprezzabile quando si studiano variazioni minime , o quando si utilizzano paradigmi che richiedono un s / r extra ( un modo per misurare i benefici dellalto campo appunto quello di determinare lestensione dellattivazione per un dato paradigma )  . a ci si aggiunge la possibilit di eseguire studi fmri in tempi ridotti e di seguire lattivazione corticale durante la stimolazione anche in tempo reale ( real time fmri )  . conclusioni sulla base dei nostri risultati finora ottenuti , rispetto alle precedenti esperienze con sistemi rm a pi basso campo , si evince che limaging morfo - funzionale ottenuto con un sistema rm 3 , 0 t , grazie ai suoi numerosi ed importanti vantaggi ( alto segnale , alta risoluzione , alta sensibilit , tempi ridotti , metodologie di studio aggiuntive e pi avanzate , maggiori capacit diagnostiche ) , potr in futuro diventare lo standard per lo studio della patologia cerebrale . 
il superamento di alcune minime limitazioni ( disomogeneit di campo , artefatti da suscettibilit e da chemical shift , sar elevato , rumore acustico , costi , variazioni semeiologiche non significative , scarsa diffusione ) , grazie ai futuri progressi tecnologici , sicuramente favorir sempre di pi lo studio anatomico , fisiologico , metabolico e funzionale del cervello nella pratica clifurther anatomical , physiological , metabolic and functional brain investigations in clinical practice and especially in research applied to it , as higher contrast , space and time resolution compared with the lower fields result in greater diagnostic power in terms of sensitivity and specificity . however , these systems are not to be considered the gold standard for all clinical applications and body districts . 
indeed , knowledge of technical , diagnostic and application characteristics of all field intensities is crucial for correct and optimal use of the different units based on study requirements . for all these reasons , we support the current restrictions on the use of such systems which provide excellent results , especially in neuroradiological imaging to university and hospital research centres and facilities already equipped with other mr systems employed in routine clinical practice that desire to conduct research . 
 the multidisciplinary approach adopted at our institution , with the collaboration of neuroradiologists , neuropsychiatrists , neurophysiologists , psychologists , bioengineers , physicists and other neuroimaging experts , has proved essential for optimal magnet utilisation . 
infatti essenziale conoscere le caratteristiche tecniche , semeiologiche e applicative di ogni sistema rm a diversa intensit di campo in modo da utilizzare in maniera adeguata ed ottimale le diverse apparecchiature in base alle proprie esigenze di studio . per questo motivo pensiamo sia giusto al momento confinare in centri di ricerca ( universitari o ospedalieri ) o comunque in strutture gi dotate con altri sistemi rm utilizzati per la routine clinica e che vogliano far ricerca , luso di tali sistemi che attualmente risultano ottimali soprattutto per limaging neuroradiologico . essenziale per lutilizzo ottimale di tali apparecchiature risultato lapporto multidisciplinare di diverse collaborazioni scientifiche che il nostro centro ha instaurato con neuroradiologi , neuropsichiatri , neurofisiologi , psicologi , bioingegneri , fisici o comunque esperti di neuroimaging . rigraziamenti allo staff tecnico : c . 
cova1 1uco di radiologia , 2uco di anatomia patologica , universit di trieste , ospedale di cattinara , strada di fiume 449 , i - 34149 trieste , italy correspondence to : f . 
this study was done to evaluate the effectiveness of cooperation between the radiologist and the cytopathologist in ultrasound - guided fine - needle aspiration biopsy ( fnab ) of thyroid nodules . 
la stretta collaborazione tra radiologo e citologo consente di ottimizzare i risultati . parole chiave nodulo tiroideo ecografia nodulo tiroideo , agoaspirazione introduction introduzione cytological assessment is a fundamental step in the diagnosis of nodular thyroid disease . 
fine - needle aspiration biopsy ( fnab ) of thyroid nodules is normally performed by a radiologist under ultrasound ( us ) guidance and , in some settings , by a clinician or a cytopathologist . 
le agoaspirazioni tiroidee vengono solitamente eseguite con guida ecografica dal radiologo e , in talune realt operative , dal clinico o dal citologo stesso , ma sussistono anche situazioni in cui lagoaspirazione viene effettuata dal clinico con la sola guida rappresentata dal reperto palpatorio [ 1 ]  . 
a retrospective analysis of 10 years of fnab of thyroid nodules and the operational changes that occurred during the course of these years provides an opportunity to assess the results of the cooperation between the radiologist and the cytopathologist . tuibile che una stretta collaborazione tra le figure professionali coinvolte possa migliorare lappropriatezza nella selezione dei pazienti candidati allagoaspirazione ed anche i suoi risultati [ 2 ] , ma una quantificazione di questi aspetti pu non essere immediata . 
lanalisi retrospettiva dellattivit di 10 anni di agoaspirazioni tiroidee e dei cambiamenti operativi verificatisi in questo lasso di tempo ci offre la possibilit di analizzare i risultati della collaborazione tra radiologo e citologo . materials and methods our analysis first considered the number of us - guided fnab of thyroid nodules carried out at our department between 1995 and 2005 . 
a number of operational changes occurred during these years that justify the choice of this time frame : 1994 was the last year in which fnab of thyroid nodules were performed by the radiologist alone , who was in charge of obtaining the sample and preparing the material ( smearing and fixation )  . 
as of january 1995 , a cytopathologist has worked alongside the radiologist in the sonography room ; the biopsy is still performed by the radiologist , but the cytopathologist prepares the material and possibly assesses its adequacy immediately . 
we therefore collected data for 1995 ( start of the radiologist - cytopathologist cooperation ) , 1999 ( consolidation of the cooperation ) and 2005 ( time chosen for data validation given the longterm interval )  . the peculiarity of the trieste province all fnab assessments are centralised in a single pathology department also enabled us to analyse data from other departments , where fnab procedures are carried out by clinicians using direct - palpation biopsy . 
we therefore analysed the number of fnab procedures , both us guided and palpation guided , in the trieste province during the 3 sample years ( 1995 , 1999 and 2005 )  . 
we then considered the number of fnab judged to be nondiagnostic by the cytopathologist , dividing them into us - guided and non - us - guided procedures , in the same 3 years . 
finally , we evaluated discrepancies between the cytological and histological diagnoses in the cases that underwent surgery in 1995 , 1999 , 2005 ( cytological diagnosis suggestive of benign lesion with histological evaluation of malignant lesion and vice versa )  . the us - guided fnab procedures were carried out with a variety of linear - array probes , from the initial 5 - mhz probes to the present 5to 10 - mhz multifrequency probes . 
two aspirations per nodule are considered sufficient in most cases ; additional aspirations are obtained in large or strongly suspicious nodules or when the cytopathologist judges the first specimens to be inadequate , for example , due to excess blood contamination . smearing is done on slides previously been treated with sulphochromic solution to ensure optimal cleanliness and greater adhesion of cells . 
the needle is detached and a few materiali e metodi nella nostra valutazione abbiamo inizialmente preso in esame il numero di agoaspirazioni tiroidee ecoguidate effettuate presso la nostra unit clinica operativa dal 1995 al 2005 . in questo lasso di tempo si sono verificati dei cambiamenti operativi che giustificano la scelta di questo periodo : il 1994 stato lultimo anno in cui le agoaspirazioni tiroidee sono state effettuate dal solo medico radiologo , che effettuava il prelievo e si faceva carico del trattamento del materiale ( striscio e fissazione )  . 
abbiamo quindi ritenuto che la raccolta dei dati andasse effettuata relativamente al 1995 ( inizio della attivit comune di radiologo e citologo ) , al 1999 ( momento scelto come espressione del consolidamento di questa attivit ) e al 2005 ( momento scelto per la validazione dei dati dopo un lungo intervallo temporale )  . la particolare condizione che si verifica nella nostra provincia , ove tutti gli agoaspirati afferiscono ad una sola struttura di anatomia patologica , ci ha anche permesso unanalisi dei dati relativi ad altre realt operative ove lagoaspirazione viene effettuata dal clinico sulla guida del reperto palpatorio . 
sono state inoltre valutate le discordanze tra diagnosi citologica e diagnosi istologica nei casi sottoposti ad intervento chirurgico nel 1995 , 1999 , 2005 ( diagnosi citologica orientativa per lesione benigna con riscontro istologico di lesione maligna e viceversa )  . le agoaspirazioni ecoguidate sono state effettuate avvalendosi di sonde lineari , diverse nel corso degli anni , inizialmente da 5 mhz , attualmente di frequenza variabile ( 510 mhz )  . 
la procedura stata effettuata con tecnica a mano libera utilizzando aghi non trancianti da 2527 g con lunghezza di 2 , 5 cm ai quali viene collegato un sistema di aspirazione , rappresentato da una semplice siringa . 
nella maggioranza dei casi venivano ritenute sufficienti due agoaspirazioni per nodulo , ricorrendo ad aspirazioni ulteriori in caso di noduli voluminosi , noduli fortemente sospetti o qualora il citologo non ritenesse adeguati i primi prelievi ad esempio per abbondante contaminazione ematica . la procedura di striscio utilizza preparati portaoggetti precedentemente trattati con soluzione solfocromica , al fine f . 
the needle is then reattached to the syringe and the aspirate expelled onto the slide by applying slight pressure on the plunger ; the aspirate is then quickly smeared onto the slide in an even and gentle manner , and fixed immediately . 
fixation is achieved by rapid immersion of the slides into a fixative solution , usually 95% alcohol , for 1015 mmicroscopic evaluation is normally done with papanicolaou staining . di garantire condizioni ottimali di pulizia e maggiore adesivit delle cellule al vetrino . 
estratto lago dalla siringa ed aspirati alcuni ml di aria , lago viene successivamente reinserito e il materiale agoaspirato viene distribuito sul vetrino praticando una lieve pressione sullo stantuffo della siringa e quindi rapidamente strisciato , manovra che deve essere uniforme e non traumatica , seguita da immediata fissazione . la fissazione si esegue mediante immersione rapida dei vetrini in liquido fissativo , solitamente alcool 95% , per circa 1015 minuti . 
la successiva valutazione al microscopio si avvale solitamente della colorazione secondo papanicolau . results risultati table 1 shows the number of us - guided fnab of thyroid nodules carried out at our department between 1995 and 2005 . 
that number rose steadily , both in absolute terms and relative to those performed on other body regions , from a total of 63 in 1995 ( 7% of the total ) , to 117 in 1999 ( 13% of the total ) and 395 in 2005 ( 29% of the total )  . 
table 2 shows the number of fnab of thyroid nodules ( divided into us - guided and palpation - guided ) performed in our province during the 3 sample years . 
the number of us - guided procedures , done by the radiologist with an on - site cyla tabella 1 riporta il numero di agoaspirazioni tiroidee ecoguidate effettuate nella nostra uco dal 1995 al 2005 . 
si osserva un progressivo aumento del numero delle agoaspirazioni tiroidee , sia in termini assoluti , sia in termini percentuali rispetto alle agoaspirazioni eseguite in altri distretti corporei . nel 1995 sono state infatti eseguite 63 agoaspirazioni tiroidee ecoguidate ( 7% del totale ) , salite a 117 nel 1999 ( 13% del totale ) ed a 395 nel 2005 ( 29% del totale )  . 
la tabella 2 riporta il numero di agoaspirazioni tiroidee nella nostra provincia ( distinte in ecoguidate e non ) nei tre anni campione ( 1995 , 1999 , 2005 )  . 
si osserva inoltre il progressivo incremento delle procedure ecoguidate effettuate a partire dal 1995 in collaborazione tra radiologo e citologo ( passate dal 25% al 94% del totale ) ed una progressiva riduzione dei prelievi inadeguati ai fini diagnostici ( passati dal 14% al 4% )  . 
la tabella 3 prende in esame concordanze e discordanze tra riscontro citologico dopo agoaspirazione ( nel 1995 , 1999 e 2005 ) e riscontro istologico nei pazienti successivamente sottoposti ad intervento chirurgico . 
emerge la progressiva riduzione delle discordanze che nel 1995 riguardavano il 38% dei casi , mentre nel 2005 riguardavano solamente il 13% dei casi . fnab of thyroid nodules is a nontraumatic procedure that is virtually free of complications and provides good results in terms of diagnosis [ 3 , 4 ]  . 
it is generally accepted that fnab of thyroid nodules should be performed under ultrasound guidance [ 49 ] as this makes it possible to sample lesions discussione lagoaspirazione tiroidea indagine pressoch atraumatica , sostanzialmente priva di complicanze e che fornisce buoni risultati sotto il profilo diagnostico [ 3 , 4 ]  . 
only sporadic reports have indicated higher rates of inadequate specimens with us - guided fnab procedures , probably as a result of the smaller size of nodules sampled and the greater blood contamination of aspirates from sonographically suspicious areas [ 14 ]  . 
however , the reported inadequacy rates of us - guided fnab are indeed nonnegligible and vary depending on the technique , the operators experience and , although there is no agreement on this , nodule size [ 3 , 13 , 1517 ]  . 
one recent study [ 3 ] reported a rate of inadequate specimens as high as 23% despite the fact that the procedures had been carried out by a single operator with seven to ten passes per nodule . we are convinced that through technical refinement and above all closer cooperation between the radiologist and the cytopathologist these results can be considerably improved , as has already been highlighted in the literature [ 2 , 1921 ]  . whereas very thin needles ( usually 27 gauge in our case ) and the use of forced aspiration can in part improve the results , the presence of an on - site cytopathologist is mandatory both to cooperate in collecting the patients anamnestic data and carry out the biopsy and , more importantly , to provide the expertise required in smearing the slide and assessing the adequacy of the specimen . 
this approach has markedly improved our results , as demonstrated by the reduction in the number of inadequate samples from 14% in 1995 , when cooperation was started , to 4% in 2005 , following 10 years of cooperation between the radiologist and cytopathologist . 
clearly , this set - up requires the presence of two staff physicians to perform the procedure , but we believe this to be widely compensated for by the results obtained and the minimal need to repeat the procedure due to inadequate sampling . 
 the marked increase in us - guided fnab indicates that the benefits of the approach have been readily perceived by the physicians working in this area , who have started to refer growing numbers of patients to radiology departments . moreover , besides improving adequacy rates , cooperation has also increased the expertise of the cytopathologist , as clearly demonstrated by the reduction in cytologyhistology discrepancies over the years considered . 
optimisation of results therefore depends on the close cooperation between the radiologist and the cytopathologist . ba essere ecoguidata [ 49 ] perch ci permette di effettuarla in lesioni di pochi millimetri o nei punti sospetti ( ad esempio in gettoni solidi di lesioni strutturalmente complesse ) anche se si tratta di lesioni voluminose palpatoriamente facilmente apprezzabili [ 10 , 11 ]  . 
solo lavori sporadici segnalano una maggiore percentuale di prelievi inadeguati nellagoaspirazione ecoguidata probabilmente per le minori dimensioni dei noduli e per la maggiore contaminazione ematica di agoaspirati mirati in zone ecograficamente sospette [ 14 ]  . 
tuttavia anche lagoaspirazione ecoguidata risulta gravata in letteratura da una percentuale di prelievi inadeguati non trascurabile , variabile alla luce della diversa tecnica utilizzata , dalla diversa esperienza delloperatore e delle diverse dimensioni dei noduli , anche se su questultimo aspetto non vi identit di vedute [ 3 , 13 , 1517 ]  . 
va rilevato come una pubblicazione recente [ 3 ] abbia riportato una percentuale di prelievi inadeguati del 23% pur se le aspirazioni venivano effettuate da un solo operatore e venivano eseguiti da 7 a 10 passaggi per nodulo . nostro convincimento che laffinamento tecnologico , ma soprattutto la maggior collaborazione tra radiologo e citologo , possano migliorare notevolmente questi risultati , come gi sottolineato in letteratura [ 2 , 1921 ]  . da un lato luso di aghi sottilissimi ( solitamente di 27 g nel nostro caso ) ed il ricorso allaspirazione forzata sono in grado di ottimizzare i risultati , dallaltro appare fondamentale la presenza fisica del citologo , con la possibilit di raccogliere assieme dati anamnestici e di effettuare assieme il prelievo , affidando alla sua esperienza la manovra di strisciamento sul vetrino e la valutazione delladeguatezza del campione . 
ci ha consentito un deciso miglioramento dei nostri risultati , come testimoniato dalla riduzione nel numero di agoaspirati considerati inadeguati ai fini diagnostici passati dal 14% del 1995 , allinizio della attivit in comune , al 4% del 2005 , dopo 10 anni di collaborazione . 
chiaro che questa organizzazione prevede la presenza di due dirigenti medici per leffettuazione della procedura , ma riteniamo ci sia ampiamente controbilanciato dai risultati ottenuti e dalla ridottissima necessit di effettuare eventuali nuove aspirazioni a fronte di una prima valutazione di inadeguatezza . lincremento nettissimo della quota di agoaspirazioni ecoguidate testimonia come questi vantaggi siano stati chiaramente percepiti dai medici coinvolti in questo settore , che hanno indirizzato una quota sempre pi consistente di pazienti alla struttura radiologica . 
va ancora sottolineato come la collaborazione tra radiologo e citologo abbia consentito , accanto al miglioramento in termini di adeguatezza del prelievo , anche di affinare lesperienza del citologo e ne sono chiara testimonianza il minor numero di discordanze tra citologia e istologia negli anni esaminati . 
giovagnoni3 1dipartimento diagnostica per immagini , ausl 3 umbria , ospedale foligno , perugia , italy 2dipartimento diagnostica per immagini , ausl 2 umbria , ospedale assisi , perugia , italy 3istituto di radiologia , universit politecnica delle marche , ospedale torrette , ancona , italy correspondence to : f . 
18 , i - 06087 perugia , italy , tel . : + 39 - 075 - 393044 , fax : + 39 - 075 - 5783488 , e - mail : fcrusco@sirm.org received : 19 january 2006 / accepted : 07 august 2006 / published online : 11 june 2007 abstract purpose . 
the reported sensitivity and specificity for electrocardiogram ( ecg ) testing , stress echocardiography and radionuclide myocardial perfusion imaging were 45% and 82% , 86% and 90% , and 68% and 84% , respectively . 
in our view , the completion of such randomised trials combined with the development of newgeneration scanners is required to correctly define the role of mdct in the follow - up assessment of patients who have undergone cabg . 
per ecg da sforzo , ecocardio - stress e scintigrafiastress la letteratura riporta valori di sensibilit e specificit rispettivamente del 45% e dell82% , dell86% e del 90% , del 68% e dell84% . 
gli studi tc selezionati , 15 prospettici , 1 retrospettivo , tutti di validazione mediante comparazione con la coronarografia convenzionale ed eseguiti con metodica multidetettore , hanno complessivamente coinvolto 705 pazienti per un numero totale di 1974 segmenti di cabg esaminati . 
le applicazioni della tcmd nel work - up diagnostico dei pazienti post - cabg , sono derivate da prove di tipo indiretto e lefficacia della metodica , dovrebbe essere valutata nel contesto di studi randomizzati , coinvolgenti anche le altre metodiche di stress imaging non invasivo . 
this has helped to limit inadequate healthcare behaviours and improve the health of the community , thanks to the delivery of healthcare services characterised by the best costbenefit ratio [ 1 ]  . 
the new approach is also a valuable tool for helping physicians keep abreast of new knowledge deriving from scientific advances and for continuing medical education aiming at actively impacting clinical practice . clinical reasoning based on evidence - based medicine ( ebm ) is , in other words , the application of a correct , validated and reproducible method that starts with the reading and critical appraisal of studies reported in the biomedical literature [ 2 ]  . 
a particularly challenging field for the application of ebm tools is in regard to the definition of the role of the new multidetector computed tomography ( mdct ) scanners in the diagnostic workup of patients with coronary artery disease . 
this paper , in particular , will consider the role of mdct in the follow - up of patients who have undergone revascularisation by coronary artery bypass grafting ( cabg )  . in the monitoring of post - cabg patients , stress electrocardiography ( ecg ) , which is also routinely performed in asymptomatic cases , is considered a first - line test [ 3 ]  . 
in symptomatic patients with recurrent ischaemia , however , second - line tests such as stress echocardiography and cardiac scintigraphy are required to confirm that the angina has a cardiac origin through the detection of graft stenoocclusion or disease progression in the native coronaries and to assess coronary flow reserve , considered fundamental for evaluating the efficacy of a revascularisation procedure [ 2 ]  . 
 coronary angiography is still regarded as the gold standard for assessing the patency of cabg and , in patients with known disease , for selecting the best strategy for myocardial revascularisation ( percutaneous or repeat surgery ) [ 3 , 4 ]  . 
however , the small , though not negligible , risks connected with the procedure , the high number of studies performed for diagnostic purposes only without leading to interventional treatment , and the invasiveness of the procedure have prompted the search for an equally accurate but less invasive procedure for assessing graft patency . 
recently , several reports have appeared on the diagnostic potential of latest - generation mdct scanners in the diagnosis of coronary disease and the assessment of the patency of bypass grafts and stents [ 519 ]  . 
however , owing both to the lack of relevant randomised clinical trials and the novelty of lintroduzione da parte della comunit scientifica internazionale , di un nuovo approccio metodologico basato sullutilizzazione di comportamenti pratici e linee guida basate sulle migliori prove di efficacia , ha permesso la riduzione del divario esistente tra risultati delle ricerche e pratica clinica corrente , contribuendo a diminuire i comportamenti assistenziali inadeguati e a migliorare lo stato di salute della comunit , grazie allerogazione di prestazioni sanitarie caratterizzate dal miglior rapporto costo / beneficio [ 1 ]  . 
questo approccio rappresenta anche uno dei pi validi strumenti per favorire laggiornamento del medico , inteso come acquisizione di nuove conoscenze derivanti dal progresso scientifico , e come formazione permanente tesa a modificare attivamente i comportamenti nella pratica clinica . il ragionamento clinico basato sulle evidenze in medicina ( ebm ) rappresenta , in altri termini , lapplicazione di un percorso metodologico corretto , valido , riproducibile , che ha come punto di partenza la lettura e linterpretazione critica delle esperienze presenti nella letteratura scientifica [ 2 ]  . 
da un punto di vista speculativo , un campo particolarmente stimolante dove poter utilizzare gli strumenti messi a disposizione dalla ebm , quello della reale definizione del ruolo delle nuove apparecchiature di tc multidetettore ( tcmd ) nel work up diagnostico del paziente con malattia coronarica . 
 in questo primo contributo in particolare verr considerato il ruolo della tcmd nel follow - up dei pazienti sottoposti a rivascolarizzazione mediante bypass aorto - coronarici ( cabg )  . come noto nel monitoraggio dei pazienti post - cabg , lelettrocardiogramma ( ecg ) da sforzo , eseguito di routine anche nei pazienti asintomatici , considerato il test di primo livello [ 3 ]  . 
nei pazienti sintomatici con recidiva ischemica , al contrario , va accertata la genesi cardiaca del dolore anginoso tramite lidentificazione della steno - ostruzione del graft o della progressione di malattia nelle coronarie native e va valutata la riserva coronaria , considerata elemento fondamentale nella valutazione della efficacia della procedura di rivascolarizzazione , attraverso test di secondo livello quali lecocardiografia e la miocardioscintigrafia da stress [ 2 ]  . 
 la coronarografia considerata , ad oggi , il gold standard per la valutazione dello stato di perviet dei cabg e , nei pazienti con patologia accertata , per la scelta della strategia di rivascolarizzazione miocardica ( eseguibile per via percutanea o mediante nuovo intervento chirurgico ) [ 3 , 4 ]  . 
i minimi , ma non trascurabili , rischi connessi alla procedura , lelevato numero di esami eseguiti esclusivamente con finalit diagnostica e senza successivo trattamento interventistico , linvasivit della procedura , hanno alimentato linteresf . 
the aim of this paper is to define , on the basis of the available clinical evidence , the role of mdct as a noninvasive diagnostic imaging test in the follow - up of patients after cabg . materials and methods we conducted a systematic review of the literature by searching for studies dealing with the clinical and imaging follow - up of patients after cabg , using pubmed ( medline database ) as a search engine . 
the search was done by entering multiple phrases containing the following combinations of search terms : coronary artery bypass graft , revascularisation , follow - up , outcome , management , stress testing , coronary angiography , imaging , noninvasive and computed tomography . 
all papers were printed , read and analysed , and those considered assessable for the purposes of our study were selected on the basis of language of publication ( english ) , date of publication ( after 1990 ) , imaging technique ( ecg , scintigraphy , mdct ) , level of evidence according to ebm criteria ( table 1 ) , number of patients involved and number of cabg studied . 
tuttavia , sia per la mancanza di trials clinici randomizzati sia per lancora troppo recente utilizzo , il ruolo di tale metodica nel followup dei pazienti sottoposti a rivascolarizzazione chirurgica , nella pratica clinica , non ancora definito con certezza . scopo del seguente lavoro definire , alla luce delle evidenze cliniche presenti in letteratura , il ruolo attuale della tcmd come strumento diagnostico di imaging non invasivo nel follow - up dei pazienti sottoposti a cabg . materiali e metodi stata eseguita una revisione sistematica tramite ricerca bibliografica riguardo gli studi rilevanti presenti in letteratura inerenti il follow - up clinico - strumentale dei pazienti sottoposti a cabg , utilizzando come motore di ricerca pubmed ( medline database )  . 
tale ricerca stata effettuata inserendo frasi multiple con le seguenti combinazioni di parole chiave : coronary artery bypass graft , revascularization , follow - up , outcome , management , stress testing , coronary angiography , imaging , noninvasive , computed tomography . una volta stampati , letti e analizzati , sono stati considerati valutabili , ai fini del nostro studio , quei lavori , in lingua inglese , considerati pertinenti in base a data di pubblicazione ( successiva al 1990 ) , tecnica di studio ( ecocardiografia , scintigrafia , tcmd ) , stratificazione del livello di affidabilit secondo i criteri dellebm ( tabella 1 ) , numero di pazienti coinvolti e numero di cabg studiati . 
sono stati inoltre revisionate le linee guida e le raccomandazioni redatte negli ultimi 5 anni dalle principali societ di cardiologia , medicina table 1 classification of the various types of clinical studies based on evidence - based medicine ( ebm ) level type of study meta - analysis or high - quality randomised controlled trial lower - quality randomised clinical trial nonrandomised cohort study with prospective or retrospective controls , phase iii trial study of quasi - experimental design , descriptive study , comparative study , correlation study , retrospective case - control study case series without control group tabella 1 classificazione dei diversi tipi di studi clinici in base allebm livello tipo di studio metanalisi o trials clinico controllato e randomizzato di alto potere trials clinico randomizzato di pi basso potere studio di coorte non randomizzato , con controlli concorrenti o storici , studio fase iii studio di altro disegno quasi sperimentale , studio descrittivo , studio comparativo , studio di correlazione , studio retrospettivi tipo caso controllo studio di casistica serie casi senza gruppo di controllo f . 
these were assessed in two separate groups , the first comprising studies involving conventional noninvasive imaging tests with physical or pharmacological stress ( ecg , echocardiography and scintigraphy ) and the second comprising studies performed using mdct . 
in the first group , we selected five studies on the diagnostic accuracy of scintigraphy and echocardiography ( all with a level of evidence of iii / iv ) [ 2832 ] , one meta - analysis ( level of evidence i ) on the role of testing in patients after cabg [ 33 ] , and seven studies on risk stratification , prognosis , and determination of disease progression ( all involving the use of scintigraphy ) [ 3440 ]  . the results of the single studies are shown in tables 2 , 3 and 4 . 
the sensitivity and specificity values were 45% and 82% , respectively , for stress ecg , 86% and 90% for stress echocardiography , and 68% and 84% for stress scintigraphy . 
sono stati valutati separatamente due gruppi , il primo comprendente gli studi riguardanti le metodiche tradizionali di imaging non invasivo con induzione di stress fisico o farmacologico ( ecg , ecocardiografia e scintigrafia ) , il secondo comprendente gli studi effettuati con tcmd . 
nel primo gruppo sono stati selezionati opportunamente 5 studi inerenti author level of evidence method pts time since cabg symptoms sensitivity specificity lakkis [ 28 ] deluca [ 29 ] kafka [ 30 ] crouse [ 31 ] elhendy [ 32 ] 51 months chest pain ; 40% atypical symptoms thallium - 201 spect scintigraphy , exercise stress tc - 99m - sestamibi scintigraphy , 144 non specified non specified dipyridamole stress echocardiography , exercise stress echocardiography , exercise stress echocardiography , dobutamine stress 182 2 weeks 21 years 125 6 weeks 16 years 5 years non specified chest pain chest pain pts , patients ; cabg , coronary artery bypass graft ; spect , single photon emission computed tomography 9496 3067 tabella 2 metodiche di stress imaging non invasivo : accuratezza diagnostica autore livello di evidenza metodica lakkis [ 28 ] intervallo post - cabg 51 mesi sintomatologia sensibilit specificit dolore toracico ; 80 40% sintomi atipici deluca [ 29 ] 144 non specificato non specificata 9496 3067 scintigrafia - spect con tallio - 201 , stress fisico scintigrafia con tc - 99m sestamibi , stress con dipiridamolo ecocardio , stress fisico ecocardio , stress fisico ecocardio , stress con dobutamina kafka [ 30 ] crouse [ 31 ] elhendy [ 32 ] pz , pazienti ; gabg , coronary artery bypass graft ; spect , single photon emission computed tomography 182 2 settimane 21 anni 125 6 settimane 16 anni 5 anni dolore toracico 79 dolore toracico 98 non specificata 78 f . 
tables 6 and 7 report the indications and contraindications , respectively , for the use of coronary angiography in post - cabg patients provided by the acc / aha in their 1999 report ( task force on practice guidelines committee on coronary angiography ) [ 5 , 6 ]  . 
fifteen of them were prospective and one was retrospective ; all were validation studies comparing mdct with conventional coronary angiography ( level of evidence iv ) [ 10 , 11 , 1427 ]  . 
of the 16 studies , four were performed with 4 - detector - row mdct , one with 8 - detector - row mdct , ten with 16 - detector - row mdct and one with 64 - detector - row mdct . 
overall , the studies involved 705 patients for a total of 1 , 974 cabg segments . laccuratezza diagnostica della scintigrafia e dellecocardiografia , ( tutti con livello di evidenza iii / iv ) [ 2832 ] , 1 metanalisi , ( con livello di evidenza i ) , sul ruolo dei test nel paziente post - cabg [ 33 ] , 7 studi sulla stratificazione del rischio , prognosi , determinazione della progressione di malattia ( tutti riguardanti la scintigrafia ) [ 3440 ]  . i risultati dei singoli studi sono riportati nelle tabelle 24 . 
da questi , risulta una sensibilit e una specificit per lecg da sforzo rispettivamente del 45% e dell82% , per lecocardio - stress dell86% e del 90% , per la scintigrafiastress del 68% e dell84% . 
le linee guida dellamerican college of cardiology / american hearth association ( acc / aha ) per lesecuzione di test da sforzo nel paziente postcabg sono riportate nella tabella 5 [ 3 ]  . 
class iii : conditions for which there is evidence and / or general agreement that the procedure or treatment is not useful / effective and in some cases may be harmful tabella 5 linee guida acc / aha per lesecuzione di test da sforzo nel paziente post - cabga classe i valutazione di pazienti con sintomi ricorrenti suggestivi di ischemia dopo rivascolarizzazione classe iib monitoraggio periodico di pazienti selezionati , asintomatici , ad alto rischio , ( ridotta funzione ventricolare sinistra , malattia coronaria multivasale , malattia della discendente anteriore prossimale , diabete , occupazione professionale a rischio ) al fine di escludere restenosi , ostruzione del graft o progressione di malattia coronaria nativa classe iii monitoraggio periodico , di routine , in pazienti asintomatici senza specifiche indicazioni aclasse i : test per i quali c accordo e consenso relativamente allutilit e allefficacia . 
classe ii : test per i quali si hanno evidenze conflittuali o divergenze di opinioni relativamente allutilit e allefficacia ; iia : il peso dellevidenza / opinione risulta in favore dellutilit / efficacia della metodica ; iib : lutilit / efficacia non ben stabilita . 
classe iii : test , che possono talvolta risultare dannosi , per i quali c accordo e consenso riguardo linutilit / inefficacia the percentage of assessable segments ranged from 62% to 100% . 
recurrent angina arising in the immediate follow - up period is generally related to postoperative problems , whereas angina recurring months or years after surgery is more frequently due to stenoocclusion of the graft or progression of the atherosclerotic disease of the coronary arteries [ 4345 ]  . 
gli studi tcmd selezionati , 15 prospettici , 1 retrospettivo , tutti di validazione della metodica mediante comparazione con la coronarografia convenzionale ( livello di evidenza iv ) , sono riportati in tabella 8 [ 10 , 11 , 1427 ]  . 
infine la tabella 9 riporta le principali indicazioni terapeutiche ( trattamento percutaneo versus chirurgico ) riguardo il management della sindrome coronarica acuta nel paziente post - cabg [ 41 , 42 ]  . discussione patogenesi e fisiopatologia della recidiva ischemica nei pazienti post - cabg nei pazienti sottoposti ad intervento di rivascolarizzazione f . 
recurrent angina without high - risk criteria on noninvasive testing occurring > 1 year postoperatively . asymptomatic patients in whom a deterioration in serial noninvasive testing has been documented but who are not at high risk on noninvasive stress testing class iii 1 . 
symptomatic ischaemia in patients who are not candidates for repeat revascularisation . routine angiography in asymptomatic patients , unless as part of an approved research protocol aclass iia : weight of evidence / opinion is in favour of usefulness / efficacy . 
class iii : conditions for which there is evidence and / or general agreement that the procedure or treatment is not useful / effective and in some cases may be harmful tabella 6 indicazioni dellacc / aha alla coronarografia nel paziente post - cabga classe iia 1 . 
evidenza con stress imaging non invasivo di criteri ad alto rischio ( i.e anomalie della motilit parietale regionale multisegmentarie riscontrate allecocardiografia da stress e / o difetti di perfusione moderati - severi reversibili dopo scintigrafia da stress ) qualsiasi sia il periodo postoperatorio . 
 pazienti asintomatici , nei quali stato documentato un deterioramento del bypass in test seriali non invasivi , in assenza di criteri ad alto rischio allo stress imaging classe iii 1 . 
 coronarografia di routine in pazienti asintomatici , a meno che questi non facciano parte di un protocollo di ricerca approvato aclasse i : test per i quali c accordo e consenso relativamente allutilit e allefficacia . 
classe ii : test per i quali si hanno evidenze conflittuali o divergenze di opinioni relativamente allutilit e allefficacia ; iia : il peso dellevidenza / opinione risulta in favore dellutilit / efficacia della metodica ; iib : lutilit / efficacia non ben stabilita . 
 role of conventional noninvasive stress - imaging techniques ( echocardiography and scintigraphy ) although stress ecg is the first - line investigation for the assessment of post - cabg patients , it has poor sensitivity and is unable to locate the site of ischaemia [ 28 , 30 , 33 ]  . 
stress mediante cabg , il rischio di una recidiva ischemica pi elevato in presenza di sesso maschile , et > 80 anni , presenza dei comuni fattori di rischio coronarico ( ipertensione , fumo , diabete , ipercolesterolemia )  . 
una recidiva anginosa che si verifica nellimmediato follow - up , legata , in genere , a problemi inerenti il periodo peri - operatorio , mentre , una ricorrenza anginosa a distanza di mesi o anni dallintervento pi frequentemente dovuta alla steno - occlusione del graft o alla progressione di malattia aterosclerotica nelle coronarie native [ 4345 ]  . 
in patients unable to exercise adequately , the acc / aha recommend the use of intravenous dipyridamole or adenosine for scintigraphy and dobutamine for echocardiography [ 3 , 51 ]  . 
its sensitivity for single - vessel stenosis varies dependla patologia dei graft venosi si associa ad una maggiore instabilit di placca ed responsabile del 53% degli episodi anginosi che si verificano entro i 5 anni , del 76% degli episodi tra i 5 e i 10 anni , del 92% di quelli oltre i 10 anni . 
la progressione dellaterosclerosi nei vasi nativi , causa , negli stessi periodi , rispettivamente del 47% , 24% e 8% degli eventi ischemici [ 44 , 50 ]  . ruolo delle metodiche tradizionali di stress imaging non invasivo ( ecocardiografia e scintigrafia ) lecg da sforzo rappresenta lindagine di primo livello nella valutazione dei pazienti post - cabg , tuttavia tale test dotato di bassa sensibilit ed incapace a localizzare il sito ischemico [ 28 , 30 , 33 ]  . 
lecocardiografia e la scintigrafia dopo induzione di stress sono considerate metodiche diagnostiche di secondo livello che utilizzano limaging per definire lo stato perfusionale e il recupero funzionale del miocardio rivascolarizzato . 
nei pazienti che non possono sostenere un adeguato esercizio fisico , lacc / aha raccomanda lutilizzo di dipiridamolo o adenosina ev nel test scintigrafico e di dobutamina in quello ecocardiografico [ 3 , 51 ]  . lecocardiografia identifica le aree ischemiche sotto forma di anomalie della motilit parietale regionale e come modificazione della funzione sistolica globale e del volume telesistolico . 
la sensibilit nellidentificazione di stenosi coronariche con tale metodica maggiore se la compromissione multivasale ( 23 regioni ) piuttosto che monovasale ( sensibilit 96% versus 77% ) [ 30 ]  . 
la sensibilit in caso di stenosi monovasale varia inoltre in base ai diversi territori coinvolti ( lad : 64% , clx : 50% , rca : 45% ) [ 32 ]  . 
limaging con spect incrementa laccuratezza diagnostica della metodica [ 2830 ]  . il ruolo dello stress imaging non invasivo nei pazienti sottoposti a cabg dipende da due fattori principali : 1 presenza dei sintomi ischemici , 2 tempo trascorso dallintervento . in base a quanto riportato dalle linee guida dellamerican college of cardiology / american hearth association / american society nuclear cardiology ( acc / aha / asnc ) , entro i primi 5 anni dallintervento , i pazienti asintomatici non ad alto rischio , non devono essere sottoposti a screening con stress - test non invasivi [ 4 ]  . 
per quanto riguarda i pazienti asintomatici ad alto rischio ( cio con ridotta funzione ventricolare sinistra , malattia coronaria multivasale , malattia della discendente anteriore prossimale , diabete , occupazione professionale a rischio ) c invece disaccordo tra quanto espresso nelle linee guida dellacc / aha del 2002 , e quanto riportato da quelle dellacc / aha / asnc del 2003 [ 4 , 5 ]  . 
al contrario , le seconde , concludono che il peso dellevidenza giustifica lesecuzione di test stress routinari ( livello di evidenza iia ) e raccomandano una spect dopo sforzo a 35 anni dalla rivascolarizzazione primitiva . 
the utility of scintigraphy is related to the possibility of identifying new areas of ischaemia prevalently caused by gsv stenoocclusions , which show up as areas of poor myocardial perfusion . 
trattamento percutaneo versus chirurgico pci + stent per le lesioni focali dei graft venosi , specie se subtotali e per le lesioni ostiali ( anastomosi prossimale ) dei graft arteriosi ; maggior vantaggio si ha nelle stenosi acute ( < 30 gg ) pci da sola per le lesioni anastomotiche distali , sia dei graft arteriosi sia di quelli venosi repeat - cabg per stenosi multiple e / o diffuse dei graft , specie se totali e croniche , soprattutto per graft connessi alla lad ( spect ) imaging increases the diagnostic accuracy of the method [ 2830 ]  . 
on the basis of the guidelines of the ( acc / aha / asnc ) , within the first 5 years of surgery , asymptomatic patients who are not at high risk should not be screened with noninvasive stress tests [ 4 ]  . 
as for high - risk asymptomatic patients ( with reduced left ventricular function , multivessel coronary artery disease , proximal lad artery disease , diabetes , high - risk occupation ) , there is no agreement between the acc / aha 2002 guidelines and the acc / aha / asnc 2003 guidelines [ 4 , 5 ]  . 
the acc / aha 2002 guidelines do not recommend periodic monitoring with noninvasive stress testing in this class of patients , whereas the acc / aha / asnc 2003 guidelines conclude that the weight of evidence justifies the use of routine stress tests ( level of evidence iia ) and recommend a stress spect 35 years after initial revascularisation . 
neither guideline recommends the use of stress tests for asymptomatic patients later than 5 years after revascularisation , although the fact that gsv grafts start to occlude at 5 years has led some authors to advocate a routine stress - spect exam regardless of symptoms to stratify the risk , assess the prognosis , determine disease progression and obtain information to guide possible treatment [ 36 , 39 ]  . conventional coronary angiography coronary angiography is considered the gold standard in assessing cabg patency and choosing the best strategy for cardiac revascularisation . 
tra le complicanze cosiddette minori devono essere annoverate quelle vascolari locali al sito di cateterizzazione ( ematoma retroperitoneale , fistola arterovenosa , pseudoaneurisma , trombosi arteriosa ) e quelle determinanti aritmie cardiache ( tachicardia - fibrillazione ventricolare , aritmie atriali , disturbi di conduzione )  . 
tra questi let ( < 1 anno , > 80 anni ) , una classe funzionale iv , una malattia del tronco comune della coronaria sinistra , cardiopatie valvolari associate , una frazione di eiezione ventricolare sinistra < 30% , gravi patologie di natura non cardiaca [ 6 ]  . 
nei pazienti bypassati il rischio di complicanze inoltre maggiore rispetto a quello della popolazione standard . la principale indicazione allesecuzione dellesame rappresentata , dallevidenza con stress imaging non invasivo , di criteri ad alto rischio ( ad esempio , anomalie della motilit parietale regionale multisegmentarie riscontrate allecocardiografia da stress e / o difetti di perfusione moderati - severi reversibili dopo scintigrafia da stress ) qualsiasi sia il periodo postoperatorio . 
nei pazienti in cui si ha una dimostrazione coronarografica di patologia si pone il problema della scelta del tipo di nuova rivascolarizzazione da effettuare , percutanea ( pci ) o ancora chirurgica ( repeat - cabg , r - cabg )  . 
si raccomanda lesecuzione della pci ( stent ) nelle stenosi subtotali , specie se acute , che si verificano nei pazienti con funzione ventricolare preservata , mentre si preferisce un reintervento chirurgico mediante rcabg nelle stenosi multiple , di vecchia data , in pazienti con malattia multivasale e ridotta funzione ventricolare [ 41 , 46 , 47 , 5256 ]  . 
these include age ( < 1 year , > 80 years ) , functional class iv , disease of the left coronary common trunk , associated valve disease , left ventricular ejection fraction < 30% , and severe noncardiac disease [ 6 ]  . 
in patients with bypass grafts , the risk of complications is even higher than in the standard population . the main indication for coronary angiography is evidence on noninvasive stress imaging of high - risk criteria ( multisegment regional wall motion abnormalities on stress echocardiography and / or reversible moderate to severe perfusion defects on stress scintigraphy ) whatever the postoperative period . 
patients with evidence of disease on coronary angiography pose the problem of choosing whether to perform percutaneous ( pci ) or surgical [ repeat cabg ( rcabg ) ] revascularisation . 
pci ( stent ) is recommended in subtotal , especially acute , stenoses in patients with preserved ventricular function , whereas r - cabg is preferred for multiple , long - standing stenoses in patients with multivessel disease and reduced ventricular function [ 41 , 46 , 47 , 5256 ]  . more than 40% of coronary angiography examinations conducted in haemodynamics laboratories are not followed by percutaneous or surgical revascularisation procedures but are only performed for diagnostic purposes [ 57 ]  . 
the resulting increase in costs , combined with the complications and risks connected with the method , has prompted a search for techniques with equal diagnostic yield but less invasiveness . the recent introduction of ct scanners with 4 , 16 , 32 and 64 detector rows with improved spatial and temporal resolution ( enabling the simultaneous acquisition of multiple submillimetre slices with quasi - isotropic voxels and the possibility of cardiac gating ) has revolutionised cardiovascular imaging by allowing the study of grafts with a high level of diagnostic accuracy . mdct : general scanning technique all of the studies selected were fairly homogenous in terms of scanning technique . 
in clinical practice , the study volume extends to include the proximal anastomosis on the ascending aorta for venous grafts as well as the distal anastomosis of the different territories of the coronary arteries ; for the study of lima grafts , inclusion of the origin of the proximal subclavian artery is not required . 
after an unenhanced scan to assess the extent of calcification of the native coronaries and the course of the metal clips , a contrast - enhanced study is performed after intravenous administration via a dual - syringe automatic injector of 100120 ml nonionic iodinated contrast material ( 300 400 mgi / ml ) at a flow rate of 34 ml / s , followed by a bolus of 3050 ml saline solution . 
for optimal enhancement , nearly all of the studies used the bolus tracking technique to determine scan delay , with the acquisition starting when a predefined threshold of enhancement was reached ( 100150 hu in the left ventricle or ascending aorta )  . 
images were reconstructed with retrospective ecg gating and variable r - r temporal windows and postin ogni caso pi del 40% delle coronarografie condotte nei laboratori di emodinamica non sono seguite da procedure di rivascolarizzazione percutanea o chirurgica , ma sono eseguite esclusivamente in senso diagnostico [ 57 ]  . 
il relativo aggravio dei costi , associato alle complicanze e ai non trascurabili rischi connessi alla metodica , ha spinto la ricerca verso strumenti con potenzialit diagnostiche altrettanto elevate , ma meno invasivi . 
recentemente lintroduzione dei nuovi scanner a 4 , 16 , 32 e 64 canali , grazie al miglioramento della risoluzione spaziale e temporale ( con la possibilit che ne deriva di acquisire simultaneamente slice multiple con spessore submillimetrico , voxel quasi - isotropico e con la possibilit di eseguire esami accurati con opportuna cardiosincronizzazione ) , ha rivoluzionato limaging cardiovascolare rendendo possibile lo studio dei graft con elevata accuratezza diagnostica . tcmd : principi generali di scansione per quanto riguarda i principi generali di scansione , i diversi studi selezionati sono abbastanza omogenei tra loro . 
nella pratica clinica il volume di studio esteso a comprendere lanastomosi prossimale su aorta ascendente per i graft venosi oltre che lanastomosi distale sui diversi territori delle coronarie ; per lo studio dei graft con mammaria interna non necessario includere lorigine succlavia prossimale . 
dopo unacquisizione diretta senza mezzo di contrasto , utile per valutare lentit delle calcificazioni delle coronarie native e il decorso delle clips metalliche , lo studio contrastografico viene eseguito mediante somministrazione endovenosa , utilizzando un iniettore automatico a doppia siringa , di 100120 ml di mdc iodato non ionico ( 300400 mgi / ml ) , alla velocit di 34 ml / s , seguiti da un bolo di 3050 ml di soluzione salina . 
per ottimizzare il contrast enhancement , in quasi tutti gli studi viene utilizzata la tecnica del bolus tracking , e il ritardo per linizio della scansione viene selezionato a partire dal raggiungimento di una soglia predefinita ( 100150 uh in ventricolo sinistro o aorta ascendente )  . 
le immagini sono ricostruite con gating ecg di cardiosincronizzazione retrospettiva e finestre temporali r - r variabili , a partire da quelle assiali native , nel post - processing , si procede allutilizzazione di ricostruzioni multiplanari ( mpr ) , curve ( cmpr ) , proiezioni di massima intensit ( mip ) e volume rendering tridimensionale ( 3d - vr ) , valutando , ai fini della valutazione di perviet dei cabg decorso ( anastomosi prossimale , graft body , anastomosi distale ) e tipo di bypass . 
il giudizio di perviet fornito in base allentit della stenosi : perviet ( stenosi < 50% ) , stenosi critica ( stenosi > 50% ) , ostruzione ( mancata opacizzazione del bypass )  . tcmd e cabg : applicazioni attuali della metodica e potenzialit diagnostiche in base allanalisi critica della letteratura prima dellavvento della tcmd , i primi studi di valutazione dello stato dei bypass con tomografia computerizzata , sono stati eseguiti con tecnica a fascio elettronico ( ebct )  . 
the judgement of patency was based on the degree of stenosis : patent ( stenosis < 50% ) , critical stenosis ( stenosis > 50% ) , occlusion ( no opacification of the bypass graft )  . mdct and cabg : current applications and diagnostic potential on the basis of a critical appraisal of the literature before the advent of mdct , early studies assessing the state of bypass grafts with ct used the electron beam technique ( ebct )  . 
despite its high level of diagnostic performance in identifying graft occlusion ( 95%100% sensitivity and 89%100% specificity ) , ebct never became widely used because of its poor spatial resolution and above all its limited availability [ 79 ]  . 
one of the first studies to compare the diagnostic performance of ct with that of coronary angiography was conducted in 2001 by ropers et al . , who studied 65 patients ( 182 grafts in total ) with a 4 - detector - row scanner [ 14 ]  . 
the authors reported sensitivity and specificity values of 97% and 98% , respectively , for the demonstration of complete graft occlusion and of 75% and 92% , respectively , for the demonstration of significant stenosis > 50% . 
thirty - eight percent of the grafts that were patent at coronary angiography could not be assessed with mdct owing to metal clip , respiration and motion artefacts , poor graft opacification and arrhythmias arising during the examination . 
similar results were obtained by nieman et al . , who used the same method in a sample of 24 patients and 86 grafts [ 15 ]  . the more recent studies , comparing 16and 64 - detectorrow scanners with coronary angiography , all attest to the efficacy of mdct in determining the patency or stenoocclusion of grafts [ 10 , 11 , 16 , 1827 ]  . 
 the contribution to the literature of the above studies appears , however , to be somewhat limited , and an accurate analysis shows that the studies , performed in single centres and on small patient populations , provide conflicting results that are generally of little value for establishing the true role of mdct in the diagnostic workup of this specific class of patients . 
instead , selection of the study samples were heterogeneous , not so much in terms of exclusion criteria , which are standardised ( renal failure , heart failure , respiratory failure , known allergy to iodinated contrast material , heart rate > 65 70 bpm ) as in terms of inclusion criteria . 
in at least two studies [ 16 , 19 ] by the same team , asymptomatic patients only underwent the ct examination , whereas in another , retrospective , study , out of a total of 27 patients , 16 had recurrent episodes of angina and 11 were asymptomatic and undergoing routine clinical and imaging follow - up [ 18 ]  . 
uno dei primi studi di comparazione della performance diagnostica della tc nei confronti del gold - standard coronarografico , effettuato con tcmd a 4 - canali , stato quello di ropers nel 2001 , condotto su 65 pazienti per un numero complessivo di 182 graft [ 14 ]  . 
lautore ha riportato valori di sensibilit e specificit , nella dimostrazione dellostruzione completa del graft , rispettivamente del 97% e 98% , e nella dimostrazione di stenosi significativa > 50% rispettivamente del 75% e 92% . 
il 38% dei graft che risultarono pervi alla coronarografia non poterono essere valutati con tcmd , a causa degli artefatti da clips metalliche , da respiro e da movimento , e a causa della scarsa opacizzazione del graft e delle aritmie durante lesame . 
i recenti lavori sullargomento , effettuati con scanner a 16 e 64 canali , testimoniano tutti , tramite comparazione con la coronarografia , lelevata efficacia della metodica nella valutazione di perviet o steno / ostruzione dei graft [ 10 , 11 , 16 , 1827 ]  . il contributo in letteratura apportato dai sopraccitati studi appare tuttavia non completamente esaustivo e da unanalisi accurata si scopre che gli stessi , eseguiti da singoli centri coinvolgendo un numero complessivamente esiguo di pazienti , forniscono risultati non univoci , in genere poco utili per stabilire leffettivo ruolo della tecnica nel work - up diagnostico di questa classe specifica di pazienti . 
invece la selezione del campione di studio disomogenea , non tanto per i criteri di esclusione , che sono standardizzati ( insufficienza renale , insufficienza cardiaca , insufficienza respiratoria , comprovata allergia al mezzo di contrasto iodato , frequenza cardiaca > 6570 bpm ) , quanto per i criteri di inclusione . 
in almeno due studi [ 16 , 19 ] , eseguiti peraltro dallo stesso gruppo , vengono sottoposti ad esame tc esclusivamente pazienti asintomatici , in un altro , retrospettivo , su un totale di 27 pazienti , 16 riferiscono episodi di angina ricorrente , 11 sono asintomatici in follow - up clinico - strumentale routinario [ 18 ]  . 
infine , nei rimanenti lavori , vengono studiati pazienti sintomatici , senza che venga fornita alcuna indicazione riguardo la positivit o meno dello stress imaging non invasivo ( ecocardiografia e / o scintigrafia da sforzo ) e riguardo leventuale attinenza ai criteri di accesso alla coronarografia raccomandati dallacc / aha del 1999 ( task force on practice guidelines committee on coronary angiography ) [ 5 ]  . 
nel lavoro di martuscelli uno dei criteri di esclusione dallesame la presenza di angina instabile , che per il quadro di presentazione sintomatologico del 20% del totale dei pazienti post - cabg [ 11 , 58 ]  . i dati statistici forniti dai diversi studi tendono ad essere discordanti . 
ad esempio schlosser , in uno studio condotto su 48 pazienti ( riferiti alla coronarografia e prima sottoposti a tcmd a 16 canali ) , con un totale di 131 graft valutati , rif . 
for example , in one study of 48 patients ( referred for coronary angiography and first studied by 16 - detector - row ct ) with a total of 131 grafts assessed , schlosser et al . 
reported a sensitivity of 96% , a specificity of 95% and a positive predictive value ( ppv ) of 81% and a negative predictive value ( npv ) of 99% [ 10 ]  . 
in the same study , the authors admit that as regards arterial cabg , only 76% of distal anastomoses to the anterior descending artery and 60% of distal anastomoses to diagonal branches could be visualised . 
 ( assessable segments , 95% ) [ 11 , 19 , 25 ]  . the statistical differences among the studies are also reflected in the different diagnostic evaluation of the distal anastomoses . 
distal anastomoses are notably particularly difficult to study owing to their relative mobility compared with the relatively fixed proximal anastomoses and graft body , their size ( generally < 2 mm , at the limit of mdct spatial resolution ) and the beam - hardening effect caused by metal clips . 
mdct scanners with 16 and 64 detector rows provide better results in the assessment of the proximal anastomosis , graft body and distal anastomosis compared with 4 - detector - row scanners . 
however , there are no statistically significant differences between 16 and 64 detector rows in the visualisation of the distal anastomosis ( 16 - mdct : assessability 92% , 64 - mdct : assessability 94% ) [ 12 , 24 , 26 ]  . 
 the literature data on the native coronary arteries in patients with suspected coronary disease cannot be transferred to the native coronaries of post - cabg patients , which are more difficult to assess due to severe atherosclerosis and calcification and often previous treatment with angioplasty and porta valori di sensibilit del 96% , specificit del 95% , valore predittivo positivo pari a 81% e valore predittivo negativo del 99% [ 10 ]  . 
nello stesso lavoro si ammette che , relativamente ai cabg arteriosi , stato possibile visualizzare solamente il 76% delle anastomosi distali sulla discendente anteriore e il 60% delle anastomosi distali sui rami diagonali . 
come gi detto , risultati sovrapponibili a chiurlia sono ottenuti da rossi ( sensibilit e specificit : 100% ; 91 , 4% dei segmenti di cabg valutabili ) , martuscelli ( sensibilit e specificit : 97% e 100% ; 88% dei segmenti di cabg valutabili ) e bursstahler ( 95% dei segmenti di cabg valutabili ) [ 11 , 19 , 25 ]  . 
come noto , a causa della relativa mobilit rispetto allanastomosi prossimale e al graft body , relativamente fissi , a causa delle dimensioni ( in genere , < 2 mm , ai limiti della risoluzione spaziale della tcmd ) , e per leffetto di beam hardening da clips metalliche , lo studio di tali segmenti anatomici particolarmente difficoltoso . 
le apparecchiature tcmd a 16 e 64 canali , forniscono , rispetto alla 4 canali , risultati migliori in termini di valutabilit dellanastomosi prossimale , del graft body e dellanastomosi distale . 
ai fini della visualizzazione di questultima , tuttavia , non si evidenziano , tra scanner a 16 e 64 canali , differenze statisticamente significative ( 16 - tcmd : valutabilit 92% , 64 - tcmd : valutabilit 94% ) [ 12 , 24 , 26 ]  . i dati della letteratura sulle coronarie native nei pazienti con sospetta malattia coronarica non sono trasferibili alle coronarie native dei pazienti bypassati , pi difficili da valutare in quanto severamente ateromasiche , ossia calcifiche , e spesso precedentemente trattate con angioplastica e stenting . 
a tal proposito , in questa coorte di pazienti , nieman [ 15 ] riporta una percentuale di segmenti nativi valutabili pari al 66 , 4%69 , 2% ed una sensibilit globale nella osservazione di stenosi significative , sempre nei segmenti nativi , pari al 52 , 9%69 , 6% . nonostante tali limitazioni , la tcmd , indubbiamente , presenta anche alcuni importanti vantaggi , i maggiori dei quali legati alla non invasivit e alla riduzione dei costi di esame rispetto alla coronarografia convenzionale . 
 [ 15 ] reported a percentage of assessable native segments of 66.4%69.2% and an overall sensitivity in the detection of significant stenosis in native segments of 52.9%69.6%. despite these limitations , there are undoubtedly several advantages in using mdct , the most important being related to noninvasiveness and reduced cost of the examination compared with conventional coronary angiography . 
interobserver agreement in image interpretation is high paradoxically higher for the assessment of the distal anastomosis and graft body compared with the proximal anastomosis independently of the use of thin - slab mip , mpr or vrt images [ 10 ]  . 
nonetheless , image interpretation cannot be divorced from the assessment of the native coronary arteries , which has lower reproducibility and must be performed by highly qualified staff with specific experience in cardiac imaging . 
the accf / aha / american college of physicians ( acp ) task force on clinical competence and training has recently published a statement to this effect , with the aim of identifying the most appropriate training pathways to enhance the professional competence of the physician ( radiologist or cardiologist ) interpreting the images [ 59 ]  . another advantage of mdct is its ability to detect other possible extravascular diseases that present clinically with chest pain and may mimic recurrent angina . 
in this class of patients , the differential diagnosis of chest pain includes pleural effusion , pericardial effusion , pulmonary embolism and infection of the sternal sutures [ 13 ]  . 
 in perspective , mdct could provide the information required for planning coronary revascularisation procedures . this field of application is above all justified by the need to reduce the small but nonnegligible risks and the costs related to the high number of diagnostic coronary angiograms that are not followed by percutaneous interventional procedures ( more than 40% of the total ) either because they are negative for graft disease ( or for disease progression in the native coronaries ) or because their findings warrant r - cabg . 
the unnecessary cost of invasive procedures could be reduced if mdct were used to screen symptomatic patients for focal , stenotic or substenotic acute or subacute graft disease to be referred for therapeutic coronary angiography . 
 recommendations for mdct in patients after cabg all in all , the clinical utility of mdct in the diagnostic workup of patients after cabg has not yet been correctly evaluated . 
ideally , it should be assessed in randomised trials ( involving also other noninvasive stress imaging methods , such as stress echocardiography and scintigraphy ) in which slab , mpr o vrt [ 10 ]  . 
in linea generale i valori di riproducibilit , nella valutazione dei bypass , sono elevati per il calibro maggiore e per il fatto che i cabg sono relativamente svincolati dal battito cardiaco . 
in ogni caso linterpretazione delle immagini non pu prescindere dalla valutazione delle coronarie native , che si associano a valori di riproducibilit minori , e deve essere affidata a figure professionali altamente qualificate e con esperienza specifica nel settore dellimaging cardiaco . 
a tal proposito lamerican college of cardiology foundation / american heart association / american college of physicians ( accf / aha / acp ) task force on clinical competence and training ha recentemente pubblicato uno statement su tale argomento , con lo scopo di individuare il percorso formativo pi corretto possibile , implementando lesperienza professionale del medico ( radiologo o cardiologo ? ) che interpreta le immagini [ 59 ]  . altro vantaggio della tcmd correlato alla capacit della stessa di evidenziare eventuali altre patologie extravascolari che si presentano clinicamente con dolore toracico e che possono mimare unangina ricorrente . 
in questa classe di pazienti la diagnosi differenziale del dolore toracico include il versamento pleurico , il versamento pericardico , lembolia polmonare e linfezione delle suture sternali [ 13 ]  . 
la tcmd pu fornire inoltre informazioni supplementari riguardo reperti incidentali non relati allesame coronarografico . in prospettiva , la tcmd , potrebbe offrire gli elementi necessari alla pianificazione di eventuali interventi di rivascolarizzazione coronarica . 
questo possibile campo di applicazione trova un senso soprattutto alla luce della necessit di ridurre i rischi , minimi ma non trascurabili , e i costi legati allelevato numero di coronarografie diagnostiche non seguite da procedure di interventistica percutanea ( pi del 40% del totale ) , o perch negative per patologia dei graft ( o progressione di malattia coronarica dei vasi nativi ) o perch indirizzanti verso un nuovo trattamento di tipo chirurgico mediante repeat cabg . 
la riduzione dei costi inutili legati alle procedure invasive , potrebbe essere ottenuta utilizzando la tcmd come filtro in grado di screenare quei pazienti sintomatici , con patologia dei graft focale , stenotica o substenotica , acuta o subacuta , da avviare selettivamente alla coronarografia con finalit terapeutiche . 
lidentificazione di stenosi multiple , croniche , in pazienti con malattia multivasale , potrebbe evitare il ricorso alla coronarografia e porre invece , da subito , lindicazione alla rivascolarizzazione chirurgica . raccomandazioni allesame tcmd nel paziente post - cabg in definitiva , ad oggi , lutilit clinica dellesame nel work - up diagnostico dei pazienti post - cabg , non ancora stata correttamente valutata . 
idealmente questa dovrebbe essere valutata nel contesto di studi randomizzati ( coinvolgenti anche le altre metodiche di stress imaging non invasivo , quali lecocardiografia e la scintigrafia da stress ) in cui pazienti con sospetta patologia dei graft sono assegnati a un iter diagnostico con o senza tcmd . 
in fact , no such studies , which should be conducted on an adequate number of patients , have yet been performed due to ethical as well as technical reasons . 
the evidence available on the role of mdct is therefore only indirect and derived from studies that compared its efficacy with that of coronary angiography , considered the gold standard . 
le prove disponibili sul ruolo della tcmd sono pertanto solo di tipo indiretto , derivabili da quei lavori che hanno valutato lefficacia della modalit rispetto alla coronarografia , considerata il gold standard . 
this was due to the fact that neither colour or power doppler are suitable for correct management of the signals produced by microbubble insonation , as they are limited by the heavy presence of artefacts . microbubbles may be insonated by a characteristic frequency named resonance or fundamental frequency ( f0 ) by using a high or low transmit power . 
contrast - specific us techniques have recently undergone an important technical development with the introduction of innovative algorithms able to register selectively the harmonic signals produced by microbubbles and to suppress the signal produced by stationary tissues . 
the different contrast - specific us techniques may be distinguished by their basic principle into pseudo - doppler , harmonic , phase - modulation , amplitude - modulation and phaseand amplitude - modulation techniques . 
 key words ultrasound microbubble harmonic ultrasound pulse inversion contrast - specific techniques riassunto lintroduzione dei mezzi di contrasto ecografici a base di microbolle ha determinato una importante evoluzione della tecnologia ecografica rappresentata dalla introduzione di tecniche ecografiche contrasto - specifiche . 
la ragione di questo legata al fatto che il color ed il power doppler tradizionali non sono in grado di gestire correttamente il segnale prodotto dalla insonazione delle microbolle essendo gravati dalla presenza di artefatti . 
se le microbolle vengono invece insonate a bassa potenza emettono , oltre alla frequenza di risonanza , frequenze armoniche ( 2f , 3f , 4f ) determinate dal comportamento fisico non lineare delle microbolle . 
le tecniche contrasto - specifiche hanno visto recentemente un particolare sviluppo tecnologico grazie alla introduzione di algoritmi innovativi in grado di registrare selettivamente il segnale prodotto dalle microbolle e di sopprimere il segnale prodotto dai tessuti stazionari . 
in base al loro principio di funzionamento le tecniche ecografiche contrastospecifiche si possono distingure in tecniche pseudo - doppler , armoniche , a modulazione di fase , a modulazione di ampiezza , ed a modulazione di ampiezza e di fase . parole chiave ecografia microbolle ecografia armonica pulse inversion tecniche contrasto - specifiche introduction introduzione microbubble contrast agents for ultrasound ( us ) have aroused increasing interest in recent years , and contrast - enhanced us ( ceus ) is a rapidly evolving field with many clinical applications . 
the observation that microbubbles may be employed as us contrast agents is not recent , as the first description dates back to 1968 [ 1 ] when contrast phenomena were observed in the aorta during cardiac catheterization after injection of saline solution . 
this was caused by air microbubbles that were produced by cavitation during the ini mezzi di contrasto impiegati in ecografia ( ultrasound ; us ) hanno suscitato un interesse sempre crescente negli ultimi anni , e lecografia con mezzo di contrasto divenuta una tecnica in rapida evoluzione con molte applicazioni in ambito clinico . 
la scoperta delle microbolle come mezzi di contrasto in ecografia non cos recente dato che la descrizione della loro prima applicazione risale al 1968 [ 1 ] quando si osserv la presenza di enhancement allinterno dellaorta durante la somministrazione di soluzione salina nel corso di una procee . 
in particular , innovative us techniques , known as contrast - specific techniques , were introduced to register selectively the harmonic signal produced by the nonlinear physical behaviour of microbubbles . 
this was because conventional colour and power doppler are unable to manage the harmonic signals produced by microbubble insonation , as they are limited by the presence of artefacts , including blooming and jail - bar artefacts [ 2 ]  . 
the recently introduced sulphur hexafluoride or perfluorocarbon - filled microbubbles offer both an excellent safety profile and a longer persistence in the peripheral circulation than do air - filled microbubbles . microbubble contrast agents have a shell of biocompatible material , such as proteins , lipids or biopolymers . 
they are injectable intravenously and can pass through the pulmonary capillary bed after a peripheral injection , as their diameter ( 310 m ) is below that of red blood cells . 
low - solubility low - diffusibility gases , such as perfluorocarbons and sulphur hexafluoride gas , are employed to improve the persistence of microbubbles in the peripheral bloodstrea the physical properties of microbubble contrast agents are closely related not only to their gas content and to the peripheral shell chemical composition but also to the frequency of the us beam , the pulse repetition frequency and , above all , the acoustic power employed for insonation [ 2 ]  . 
tale effetto era determinato dalle microbolle daria prodotte da un fenomeno fisico di cavitazione durante la somministrazione attraverso il catetere . da allora molti sforzi sono stati fatti per aumentare le possibili applicazioni cliniche delle microbolle . 
la ragione di questo legata al fatto che il color ed il power doppler tradizionali non sono in grado di gestire il segnale prodotto dalla insonazione delle microbolle essendo gravati dalla presenza di artefatti tra cui il blooming ed il jail bar [ 2 ]  . composizione chimica delle microbolle i mezzi di contrasto a base di microbolle sono stati approvati nella maggior parte dei paesi europei , e vengono oggi largamente impiegati anche in asia ed in canada . 
negli stati uniti la food and drug administration limita per il momento limpiego delle microbolle solo al settore ecocardiografico . le microbolle di recente introduzione a base di gas esafluoruro di zolfo o di perfluorocarburi possiedono un profilo di sicurezza elevato ed una maggiore stabilit nel circolo periferico rispetto alle microbolle a base di aria . 
le microbolle vengono somministrate per via endovenosa , e sono in grado di attraversare il letto capillare polmonare dato che presentano un diametro ( 310 m ) inferiore a quello dei globuli rossi . per migliorare la stabilit delle microbolle nel circolo periferico sono state impiegate due strategie principali : rivestire le microbolle con una capsula di composizione chimica stabile nel circolo periferico , oppure utilizzare gas a basso coefficiente di diffusione attraverso la caspula [ 3 , 4 ]  . 
la capsula periferica presenta uno spessore variabile tra 10 a 200 nm , e pu essere rigida ( ad esempio se costituita da albumina denaturata oppure biopolimeri ) , oppure pi flessibile ( ove vengano utilizzati fosfolipidi )  . 
i gas caratterizzati da una bassa solubilit e da una bassa diffusibilit in acqua come il perfluorocarburo e lesafluoruro di zolfo , determinano un aumento della stabilit delle microbolle nel circolo periferico . le propriet fisiche delle microbolle sono strettamente correlate non solo al loro contenuto gassoso ed alla composizione chimica della loro capsula periferica , ma anche alla frequenza del fascio di us impiegato , alla frequenza di ripetizione dellimpulso , e soprattutto alla potenza di insonazione impiegata [ 2 ]  . 
i diversi mezzi di contrasto a base di microbolle sono elencati nella tabella 1 . tecniche di insonazione per ottenere un segnale armonico utile per la costruzione dellimmagine le microbolle devono essere insonate mediante la loro specifica frequenza fondamentale , detta anche di table 1 microbubble ultrasound contrast agents perfluorocarbon - filled sulphur - hexafluoride - filled sonovue e . 
 tutti gli agenti possiedono una capsula a base di fosfolipidi eccetto : acaspula a base di galattosio ; bcapsula a base di albumina ; ccapsula a base di cianoacrilato ; dagente a cambiamento di fase : una emulsione di perflenapent liquido su liquido che contiene dodecafluoropentano in forma liquida in fase dispersa e che passa alla forma gassosa alla temperatura corporea formando microbolle con diametro compreso tra 38 m powee ( db ) foundamental frequency resonance frequency fig . 
1 lo spettro di intensit acustica delle microbolle a base di esafluoruro di zolfo rispettivamente per una bassa ( linea tratteggiata ) ed alta potenza di insonazione ( linea continua )  . 
i tessuti stazionari presentano un unico picco di emissione in corrispondenza della frequenza fondamentale ( risonanza ) per gentile concessione di springer science and business media , da [ 2 ]  . transmission frequency ( mhz ) ( rarefactional ) pressure that the transmitted us pulse achieves during its travel through a medium of specified attenuation coefficient , and fc is the centre frequency of the pulse . 
a more correct and reproducible manner is to express the insonation transmit power as mega pascal ( mpa ) , which is reported on the screen of some us devices . 
la formula che lo rappresenta la seguente : indice meccanico = p - / ( cid : 2 ) fc , dove pindica il picco massimo di pressione negativa ( rarefazione ) che limpulso ultrasonoro trasmesso raggiunge in un mezzo con uno specifico indice di attenuazione , mentre fc rappresenta la frequenza centrale della banda di e . 
one group of methods , commonly known as high - transmit - power insonation , uses large pulse amplitudes ( about 1 mpa ) and produces microbubble destruction with emission of an irregular wideband harmonic signal , similar to an explosion , and named stimulated acoustic emission ( sae )  . 
the threshold for destruction is variable and depends on a number of different factors , such as microbubble size , shell material and filling gas and the attenuation of the us beam power by the overlaying tissues . 
these methods are generally employed to insonate air - filled microbubble contrast agents with a soft shell , presenting a low harmonic behaviour at low - transmit - power insonation , and are limited by the transiency of the signal , which persists only for 23 frames . 
this leads to asymmetric or nonlinear oscillations , which contain both fundamental and harmonic frequencies multiple of the fundamental frequency . this insonation method is employed with sulphur hexafluoride or perfluorocarbon - filled microbubbles and allows realtime scanning given the long persistence of the signal . contrast - specific us techniques the different contrast - specific us techniques [ 6 ] may be distinguished by their basic principles into pseudo - doppler , harmonic , phase - modulation , amplitude - modulation , and phaseand amplitude - modulation techniques . 
pseudo - doppler techniques rely on the sae effect , which corresponds to the emission of a wideband signal when the microbubbles are destroyed by a high - transmit - power insonation . 
 stimulated acoustic emission ( sae ) in this mode , the microbubbles appear as a random colour mosaic extending over a limited depth range close to the focus of the transmitted us [ 7 ]  . 
un indice maggiormente ripoducibile invece rappresentato dalla potenza acustica di insonazione espressa in mpa ( mega pascal ) che viene riportata sul monitor operativo di alcuni ecografi . esistono due diverse tecniche per insonare le microbolle [ 5 ]  . 
la prima tecnica rappresentata dalla insonazione ad alta potenza acustica ( circa 1 mpa ) e determina la distruzione delle microbolle con la conseguente emissione di un segnale irregolare ad ampia banda , simile ad uno scoppio , e definito emissione acustica stimolata ( stimulated acoustic emission , sae )  . 
la soglia per raggiungere la distruzione delle microbolle variabile e dipende da numerosi fattori quali le dimensioni , la composizione chimica della capsula ed il gas presente allinterno delle microbolle , nonch dal grado di attenuazione della potenza del fascio ultrasonoro prodotto dai tessuti soprastanti . 
queste tecniche vengono generalmente impiegate per insonare le microbolle a base di aria con una capsula poco resistente e che presentano uno scarso comportamento armonico a bassa potenza di insonazione e sono limitate dalla scarsa persistenza del segnale che perdura al massimo 23 frames . 
questo limite pu essere in parte risolto impiegando una insonazione di tipo intermittente con basso frame rate ( una immagine prodotta ogni 23 secondi ) in modo da limitare la distruzione delle microbolle . la seconda tecnica rappresentata dalla insonazione delle microbolle a bassa potenza acustica ( 3070 kpa )  . 
con questa tecnica si riduce la probabilit di rottura delle microbolle , e la produzione di frequenze armoniche da parte dei tessuti stazionari , mentre si sfrutta pienamente il comportamento fisico non lineare delle microbolle . 
la tecnica a bassa potenza di insonazione viene impiegata con microbolle a base di esafluoruro di zolfo oppure di perfluorocarburo , e consente la esecuzione di una scasione ecografica in tempo reale data la lunga persistenza del segnale . tecniche ecografiche contrasto - specifiche in base al loro principio di funzionamento le tecniche ecografiche contrasto - specifiche [ 6 ] si possono distingure in tecniche pseudo - doppler , armoniche , a modulazione di fase , a modulazione di ampiezza , ed in tecniche a modulazione di ampiezza e di fase . 
il raggio delle microbolle presenta un grado di compressione durante la fase positiva dellimpulso ultrasonoro uguale al grado di espansione durante la fase negativa . le microbolle dimostrano invece un comportamento fisico non lineare se la potenza di insonazione viene progressivamente aumentata mantenendo la frequenza di risonanza ( b )  . 
questo comportamento non lineare determina la produzione di frequenze armoniche per gentile concessione di springer science and business media , da [ 2 ]  . acoustic power radius acoustic power radius struction and to the following absence of microbubbles after destruction . 
this phenomenon of loss of correlation is interpreted as a movement by the us systethe effect quickly disappears over a few frames due to the destruction of the microbubbles . cadence agent detection imaging ( adi ) this technique involves the transmission of two identical high - amplitude pulses and the temporary storage of the two resulting echo sequences before the second is subtracted from the first . 
queste tecniche sono limitate dalla forte presenza di artefatti e dalla scarsa persistenza del segnale . emissione acustica stimolata ( stimulated acoustic emission , sae ) in questa tecnica il segnale prodotto dalla insonazione delle pseudo - doppler harmonic phase modulation amplitude modulation gray - scale harmonic pulse inversion power modulation phase and amplitude modulation cadence contrast pulse sequencing e . 
quaia : contrast - specific ultrasound techniques table 2 contrast - specific ultrasound techniques stimulated acoustic emission cadence agent detection imaging advanced dynamic flow tissue signature imaging tabella 2 tecniche contrasto - specifiche pseudo - doppler imaging armonico modulazione di fase modulazione di ampiezza gray - scale harmonic pulse inversion power modulation modulazione di fase e di ampiezza cadence contrast pulse sequencing stimulated acoustic emission cadence agent detection imaging advanced dynamic flow tissue signature imaging coherent contrast imaging power pulse inversion contrast tissue discriminator vascular recognition imaging coded harmonic angio coherent contrast imaging power pulse inversion contrast tissue discriminator vascular recognition imaging coded harmonic angio flash echo imaging harmonic power doppler imaging contrast tuned imaging c cube extended pure harmonic detection ultraharmonic imaging subharmonic imaging 1.5 harmonic imaging flash echo imaging harmonic power doppler imaging contrast tuned imaging c cube extended pure harmonic detection ultraharmonic imaging subharmonic imaging 1.5 harmonic imaging bles produce strong echoes from the first pulse , but many are destroyed or substantially damaged in the process , so the echoes produced by the second pulse will be different both in intensity and morphology . 
the user can choose to display an image made up of either the subtracted echoes ( microbubble signal only ) , the echoes from the second transmission ( tissue only ) or a combination of the two , with the contrast image presented as a coloured overlay on the tissue b - mode image . microbolle appare come un mosaico di colori che si estende ad una profondit limitata e che maggiormente evidente in prossimit del punto di massima focalizzazione [ 7 ]  . 
il suo principio si basa infatti sulla iniziale identificazione delle microbolle da parte del primo impulso , e sulla loro immediata scomparsa determinata dalla loro distruzione con conseguente mancata identificazione delle microbolle da parte degli impulsi successivi ad elevata potenza . 
il fenomeno di perdita di correlazione viene interpretato come movimento da parte del sistema ecografico e advanced dynamic flow this is a wideband frequency technique that employs a lower pulse amplitude and fewer pulse transmissions per line ( from two to four ) in comparison with the pseudo - doppler techniques . 
this reduces the rate of bubble destruction , allowing real - time imaging , albeit at a lower frame rate ( four to five frames / s ) in comparison with conventional us imaging . 
this doppler threshold value is easily exceeded if microbubble contrast agents are employed resulting in the presence of artefacts such as blooming ( presence of doppler signal not determined by the mean frequency shift ) and clutter ( low frequency doppler signal produced by stationary tissues overlapping the real doppler signal )  . to limit blooming and clutter , the b - mode and doppler power for a pixel are compared , and the larger one is used to set the pixel grey level [ 6 ]  . 
the tissue and contrast information can be displayed separately ( a , b ) or simultaneously ( c ) by overlapping the colour map and the tissue image in b - mode . 
il contributo dei tessuti stazionari e del mezzo di contrasto possono essere visualizzati separatamente ( a , b ) , oppure simultaneamente mediante la sovrapposizione della mappa colore allimmagine dei tessuti in b - mode ( c )  . 
leffetto scompare rapidamente dopo alcuni frames a causa della distruzione massiva delle microbolle . cadence agent detection imaging ( adi ) questa tecnica si basa sulla trasmissione di due impulsi di uguale ampiezza , sulla registrazione temporanea dei due echi prodotti e sulla successiva sottrazione del secondo dal primo eco . 
la distruzione della microbolle produce invece due echi diversi dato che il primo impulso determina una significativa distruzione delle microbolle e , conseguentemente , il secondo impulso riscontra un numero minore di microbolle e produce un segnale di diversa intensit e morfologia . 
ci determina la formazione di un segnale complesso quando i due echi vengono sottratti che viene usato per rappresentare la distribuzione delle microbolle in ambito parenchimale per mezzo di una mappa colore . 
loperatore pu scegliere di visualizzare limmagine ottenuta solo con la sottrazione dei due echi ( esclusivo segnale delle microbolle ) , con i soli echi derivanti dal secondo impulso trasmesso ( esclusivo segnale dei tessuti ) , oppure una combinazione dei due con limmagine prodotta dalle microbolle rappresentata come mappa colore sovrapposta alla immagine dei tessuti in b - mode . advanced dynamic flow una tecnica che impiega una larga banda di frequenze in trasmissione , ed una minore potenza di insonazione ed un minor numero di impulsi ( da 2 a 4 ) per ogni linea di vista rispetto alle tecniche pseudo - doppler precedenti . 
quaia : contrast - specific ultrasound techniques a pixel will not display a power doppler signal if the b - mode signal for that pixel is large , whereas the pixels with a strong clutter will merge relatively inconspicuously with those showing strong b - mode stationary tissue signals . tissue signature imaging the tissue signature imaging mode is based on the same basic principles as the advanced dynamic flow , even though it represents the power doppler signals as grey - scale levels . this technique represents both harmonic signals produced by microbubble destruction and the nonlinear fundamental signals from stationary tissues in a gray - scale map . 
as the second harmonic ( double of the insonating frequency ) has the highest amplitude among the harmonics , it is the most relevant harmonic frequency for contrast - specific us imaging , even though the signal may be persistent or transient depending on acoustic power employed . 
le frequenze doppie rispetto alla frequenza fondamentale vengono selettivamente registrate per mezzo di un filtro passa - alto che elimina le frequenze fondamentali ( rettangolo )  . do viene ridotta la percentuale di distruzione delle microbolle permettendo quindi un imaging in tempo reale anche se con un numero di frames ridotto ( 45 frames / secondo ) rispetto allimaging ecografico convenzionale . 
questo valore soglia viene facilmente superato dopo la somministrazione delle microbolle e produce la presenza di artefatti quali il blooming ( presenza di segnale doppler non reale ) ed il clutter ( segnale doppler a bassa frequenza prodotto dai tessuti stazionari che si sovrappone al segnale doppler reale )  . 
per limitare il blooming ed il clutter la intensit del segnale b - mode e doppler vengono paragonati in ogni pixel ed il segnale a maggiore intensit viene impiegato come riferimento per regolare il livello della scala dei grigi [ 6 ]  . 
questo sistema evita la presenza del blooming e del clutter dato che un pixel non potr per principio dimostrare un segnale power doppler se il segnale b - mode per quel pixel molto intenso , mentre i pixel con forte presenza di clutter saranno soppressi dai pixel viciniori con forte segnale b - mode proveniente dai tessuti stazionari . tissue signature imaging rappresenta una tecnica che utilizza il medesimo principio delladvanced dynamic flow rappresentando per il segnale power doppler come scala di grigi . 
la seconda armonica ( frequenza doppia rispetto alla frequenza fondamentale ) la frequenza armonica di maggior importanza per limaging contrasto - specifico dato che possiede la maggiore ampiezza tra le frequenze armoniche prodotte anche se il suo segnale pu essere persistente oppure transitorio in relazione alla potenza acustica impiegata . 
moreover , if the transmit pulse bandwidth ( centred at the fundamental frequency fo ) and the receive bandwidth ( centred at 2fo ) overlap , then a portion of the echo from linear scattering will contaminate the harmonic receive signal , reducing the difference between microbubble agent and stationary tissue and , consequently , the contrast resolution of the technique . 
 flash echo imaging this technique employs intermittent high - transmit - power insonation to produce microbubble destruction , with a progressively increasing interscan delay leading to progressive microbubble accumulation in the scanning plane [ 8 ]  . 
sebbene questo sistema di filtraggio permette di eliminare gli echi che provengono dai tessuti stazionari che presentano prevalentemente un comportamento lineare , il sistema determina necessariamente una riduzione della ampiezza della banda di frequenze utilizzata determinando quindi una bassa risoluzione spaziale assiale . 
inoltre , ove la banda di frequenza del segnale trasmesso ( centrata sulla frequenza fondamentale f0 ) si sovrapponga a quella del segnale in ricezione ( centrata su 2f0 ) si riduce la differenza del segnale prodotto dalle microbolle e dai tessuti stazionari con una riduzione della risoluzione di contrasto della tecnica . harmonic power - doppler imaging flash echo imaging this technique is also known as harmonic power - doppler imaging by high - pass signal filtering . 
with conventional colour doppler , moving scatterers in a region of interest produce a low - frequency shift ( clutter signal ) , which has a doppler shift frequency nearly identical to that of the moving blood . 
 contrast - tuned imaging ( cnti ) this technique involves the transmission of the specific resonance frequency of sulphur - hexafluoride - filled microbubbles and the selective registration of the harmonic frequencies . 
this allows a significant reduction of the insonation power with reduction of the nonlinear harmonic behaviour of the stationary tissues and a selective production of harmonic frequencies from microbubbles . questa tecnica utilizza in modo intermittente una alta potenza di insonazione per distruggere le microbolle e , aumentando progressivamente il ritardo tra una insonazione e laltra , determina un progressivo accumulo delle microbolle nel piano di scansione [ 8 ]  . 
pi lungo il ritardo tra le singole scansioni e maggiore laccumulo delle microbolle pi elevata lintensit del segnale prodotto . power doppler armonico questa tecnica anche conosciuta come power doppler armonico con filtraggio passa - alto del segnale . 
lutilizzo di un filtro passa - alto consente di cancellare il segnale prodotto dai tessuti e di registrare selettivamente il segnale doppler prodotto dalle microbolle . c - cube contrast tuned imaging ( cnti ) this is a harmonic , intermittent , high - transmit - power technique that relies on the transmission of two identical us pulses down each ray line and on the comparison of returning echo signals . 
this enables the identification of nonlinear harmonic response from microbubbles from the different intensity on the two echoes due to microbubble destruction by the first us pulse [ 5 ]  . 
 extended pure harmonic detection ( ephd ) this technique consists of the transmission of a low - transmit - power us pulse characterised by a frequency equal to the resonance frequency of the microbubbles and absence of distortions or harmonic components . 
as a result , only the real harmonic signals generated by the microbubble resonance questa tecnica basata sulla trasmissione della specifica frequenza di risonanza che caratterizza le microbolle a base di esafluoruro di zolfo e sulla selettiva registrazione del segnale armonico prodotto . 
questo permette una notevole riduzione della potenza acustica di insonazione con una conseguente riduzione del comportamento armonico non lineare dei tessuti stazionari ed una selettiva produzione di frequenze armoniche da parte delle microbolle . c - cube una tecnica armonica intermittente ad alta potenza di insonazione che si basa sulla trasmissione di due impulsi identici lungo ogni linea di vista e sul confronto dei relativi echi . questo rende possibile lindividuazione della risposta non lie . 
the nonlinear nature of microbubble oscillation under the influence of sound pressure generates phase - shifted signals that identify the received harmonic signal as being originated by the contrast agent and not the surrounding tissue . 
with ultraharmonic imaging , a combination of highand low - pass filters can be used to selectively display only ultraharmonic frequencies where the signal to noise ratio ( snr ) is intrinsically greater . 
adenoma epatico ( freccia ) valutato mediante scansioni eseguite in fase arteriosa ( a ) , portale ( b ) e tardiva ( c ) dopo la somministrazione delle microbolle . 
la chiara cospicuit della lesione rispetto al background determinato dai tessuti stazionari evidente nella fase arteriosa ed determinata dalla notevole risoluzione di contrasto della tecnica . neare armonica delle microbolle che producono una differenza di intensit tra i due echi determinata dalla distruzione delle microbolle da parte del primo impulso [ 5 ]  . extended pure harmonic detection ( ephd ) questa tecnica consiste nella trasmissione di un impulso a bassa potenza acustica caratterizzato da una frequenza corrispondente alla frequenza fondamentale delle microbolle e che risulta inoltre privo di distorsioni e di qualsiasi componente armonica . 
la insonazione delle microbolle alla frequenza di risonanza determina la generazione di una variazione di fase nel segnale riflesso rispetto a quello trasmesso che caratterizza univocamente il segnale armonico generato dalle microbolle rispetto a quello generato dai tessuti stazionari . 
this , combined with the fact that nonlinear propagation of ultrasound in tissue does not generate a subharmonic component , suggests that subharmonic detection might offer an imaging method with greater contrast between microbubble and tissue echoes . 
this imaging technique reduces tissue echoes without generating motion artefacts , such as those seen in the pseudo - doppler imaging technique . contrast between tissues and bubbles is improved by 20 db compared with the second harmonic imaging technique . 
the newer modalities also share a common feature , namely , the transmission of multiple us pulses per scan line , followed by processing of the received radiofrequency signals from each line . 
le frequenze ultra - armoniche originano in minima parte dalla trasmissione non lineare degli ultrasuoni attraverso i tessuti stazionari , mentre esse vengono prodotte efficacemente dalle microbolle mediante insonazione a bassa oppure alta potenza . 
una combinazione di filtri passa - alto e passa - basso viene impiegata per rappresentare selettivamente le frequenze ultra - armoniche che producono un rapporto segnale - rumore pi elevato rispetto alle frequenze armoniche tradizionali . subharmonic imaging quando le microbolle vengono insonate vengono prodotti anche alcuni echi che presentano una frequenza che la met della frequenza di insonazione , unitamente ad echi con una frequenza pari alla frequenza di insonazione oppure alla seconda e terza armonica o anche a frequenze armoniche di ordine superiore . 
la prima certamente rappresentata dalla risposta non lineare delle microbolle ad un impulso di insonazione . la seconda causa invece rappresentata dalle oscillazioni continue delle microbolle dopo il termine della insonazione . lintensit della frequenza sub - armonica inoltre maggiore quando gli impulsi trasmessi contengono un elevato numero di cicli , e nelle microbolle che presentano una capsula meno rigida . 
questo elemento , unitamente al fatto che la propagazione non lineare degli ultrasuoni nei tessuti non genera delle frequenze subarmoniche , suggerisce che il rilevamento delle frequenza subarmoniche rappresenta una tecnica in grado potenzialmente di produrre una maggiore risoluzione di contrasto tra gli echi provenienti dalle microbolle e quelli provenienti dai tessuti . 
in particolare la banda di frequenza utilizzata presenta una frequenza centrale pari a 3 / 2 della frequenza fondamentale , e produce selettivamente echi dalle microbolle e non dai tessuti stazionari . 
per un mezzo non lineare come le microbolle , gli echi risultanti non sono copie invertite luno dellaltro e la loro somma produce un risultato diverso da zero ( c )  . better discrimination between tissue and microbubble contrast agents , and to overcome the requirement of the use of a narrow - band signal for harmonic imaging with the consequently reduced spatial axial resolution . 
in pulse inversion , two sequential us waves that are inverted replicas of each other are transmitted into tissue , and the resulting echoes are summed [ 6 ]  . 
if a high acoustic power of insonation is employed for imaging , however , tissue harmonics are not eliminated by pulse inversion and are incompletely cancelled , and tissue and microbubble second harmonics may still overlap . the advantage of the pulse inversion method over the harmonic techniques is that overlap between the fundamental and second harmonic spectra does not matter , and there is no need to restrict the transmission spectrum to the lower half of the transducer frequency range . 
the tissue - contrast discrimination that can be achieved by pulse inversion is limited by any tissue movement between the two transmissions . where there is tissue movement , the positions of the tissue interfaces in the second echo sequence will not match those fig . 
le tecniche pi recenti sono in particolare caratterizzate dalla trasmissione di multipli impulsi per ogni linea di vista , e dalla successiva elaborazione dei segnali ricevuti secondo ogni linea di vista . 
lo scopo delle tecniche a modulazione di fase di differenziare il segnale lineare prodotto dai tessuti stazionari da quello non lineare prodotto dalle microbolle con il fine di aumentare la risoluzione di contrasto ed il rapporto segnale / rumore . 
queste tecniche impiegano una bassa potenza acustica di insonazione e consentono una lunga persistenza del segnale prodotto dalle microbolle con la possibilit di eseguire le scansione in modo continuo ed in tempo reale . pulse inversion harmonic imaging ( pulse inversion a due impulsi ) questa tecnica stata introdotta per superare due importanti limiti dellimaging armonico : fornire una migliore discriminazione tra i tessuti stazionari e le microbolle , e superare il vincolo imposto dalluso di una stretta banda di frequenze con conseguente riduzione della risoluzione spaziale assiale . nella tecnica pulse inversion due impulsi ultrasonori sequenziali , di uguale ampiezza , ma di fase opposta , vengono trasmessi allinterno del tessuto e gli echi relativi vengono sommati [ 6 ]  . 
ove venga utilizzata una elevata potenza di insonazione le armoniche tissutali non vengono eliminate dato che anche i tessuti stazionari posseggono un comportamento non lineare se insonati ad alta potenza causando una sovrapposizione tra le frequenze armoniche provenienti dai tessuti e le frequenza provenienti dalle microbolle . il vantaggio della tecnica pulse inversion rispetto alla tecniche di imaging armonico costituito dal fatto che la sovrapposizione tra la frequenza fondamentale e la seconda armonica non costituisce un problema , e non quindi necessario ridurre la banda di frequenze in trasmissione . 
leffetto viene limitato se i tessuti stazionari si muovono nello spazio temporale compreso tra i due impulsi in opposizione di fase in quanto ci determina una variazione delle interfacce tissutali che producono il primo ed il secondo eco e quindi una imperfetta eliminazione del segnale lineare . microflow imaging in the first , and cancellation of the linear signal will not be perfect . microflow imaging this technique is based on the summation of multiple consecutive frames , and it represents a multi - intensity projection algorithm of pulse inversion data . 
 contrast tissue discriminator contrast tissue discriminator is a low - transmit - power multipulse mode based , like the phase inversion mode , on the pulse subtraction method using alternating phases . 
the reduction in frame rate that represents a limitation of pulse inversion can be avoided by transmitting only one pulse per scan line but by inverting the transmitted pulse on alternate scan lines [ 6 ]  . 
the sum of the two echo sequences represents an average of the two contributing lines and is therefore displayed as a synthetic line situated midway between thesumming the echo sequences from adjacent lines therefore cancels out echoes from linear scatterers , as in the two - pulse method described in the previous section . 
the avoidance of a frame - rate penalty comes at the expense of a slightly imperfect cancellation of the fundamental frequencies , as not all points in a pair of overlapping beams experience matching but inverted versions of the same pulse wavefor power pulse inversion ( pulse inversion with three transmissions ) power pulse inversion is a technique in which a series of us pulses ( 3 ) are transmitted at a high pulse repetition interval along each line [ 11 ]  . 
three interrogations of a line with alternately inverted pulses can greatly reduce the effect of tissue motion , which limits the usual pulse inversion mode . each transmitted pulse is an inverted copy of the previous pulse . 
the processing amounts to forming an average of the first and third echo sequences ( by adding them together and dividing by two ) and adding this to the second echo sequence . 
if the tissue velocity is not too great , the difference in phase between echoes from the first and third pulses ( less than a millisecond apart ) will be small , say less than 30 or so , and the average echo sequence will then be a close approximation to one with half the phase shift , corresponding to what would have been returned if an imaginary pulse had been transmitted midway in time between these two real pulses . 
as for the two - pulse method , adding the average echo sequence from the two noninverted pulses to the real sequence from the second ( inverted ) pulse will give cancellation of linear tissue echoes but not of microbubble echoes . the use of multiple pulses reduces motion artefacts while preserving true contrast signal ( noise cancels but real signals add )  . 
 vascular recognition imaging a generalisation of the pulse inversion method , combines the nonlinear detection performance of pulse inversion imaging with the motion discrimination capabilities of colour and power doppler . 
inoltre , al fine di dare continuit alla linea del vaso viene aumentata la persistenza del segnale sullo schermo . contrast tissue discriminator questa tecnica contrasto - specifica utilizza una bassa potenza di insonazione e si basa sul principio della tecnica pulse inversion consistente nella sottrazione degli echi utilizzando la modulazione della fase . 
gli echi che provengono dai tessuti stazionari vengono cancellati , mentre gli echi che derivano dalle microbolle vengono selettivamente rappresentati . coherent contrast imaging una tecnica a modulazione di fase ad alto frame rate . 
la riduzione del frame rate che rappresenta uno dei limiti della pulse inversion pu essere superata trasmettendo un singolo impulso per linea ma invertendo la fase degli impulsi a linee di vista alterne . 
viene calcolata la media del contributo di ciascuna linea di vista ed il risultato produce una ulteriore linea di vista in posizione intermedia tra le due linee di vista precedenti . 
la sommazione della sequenza degli echi derivanti da linee di vista adiacenti cancella le interfacce a comportamento lineare come avviene nelle tecniche a due impulsi in opposizione di fase in successione . 
tutto ci avviene a spese di una imperfetta cancellazione delle frequenze fondamentali , dato che due punti adiacenti sono sottoposti a due versioni coerenti ma invertite della stesso impulso ultrasonoro . power pulse inversion ( pulse inversion a tre impulsi ) la power pulse inversion una tecnica in cui una serie di impulsi ultrasonori ( 3 ) di fase invertita luno rispetto allaltro vengono trasmessi con unalta frequenza di ripetizione e ad intervalli regolari lungo ogni linea di vista [ 11 ]  . 
inviando lungo ogni linea di vista tre impulsi successivi e di fase invertita si ottiene una riduzione delleffetto derivante dal movimento dei tessuti stazionari tra 2 impulsi successivi che rappresenta uno dei limiti principali della tecnica pulse inversion . 
se la velocit del movimento tissutale non troppo elevata la differenza di fase tra gli echi che derivano dal primo e del terzo impulso ( inferiore a un ms ) sar ridotta ( < 30 ) , e la media tra il primo ed il terzo eco rappresenter quindi una approssimazione molto vicina a met della variazione di fase corrispondendo alla riflessione che si sarebbe ottenuta se un ipotetico impulso fosse stato trasmesso al centro della finestra temporale compresa e . 
come per la tecnica pulse inversion a due impulsi , aggiungendo la media degli echi ottenuta dal primo e dal terzo impulso al secondo impulso , che presenta fase opposta rispetto al primo ed al terzo , si ottiene la cancellazione degli echi prodotti dai tessuti stazionari ma non degli echi prodotti dalla insonazione delle microbolle . lutilizzo di multipli impulsi riduce quindi gli artefatti da movimento ed allo stesso tempo mantiene il contrasto tra i tessuti stazionari e le microbolle . 
lo svantaggio di questa tecnica laumento della percentuale di distruzione delle microbolle a causa dei multipli impulsi di insonazione . vascular recognition imaging questa tecnica , unisce la capacit di registrare gli echi prodotti dal comportamento non lineare delle microbolle con la capacit di discriminare la direzione del movimento tipico del color e power doppler . 
gli echi derivanti dai primi tre impulsi vengono sommati in modo ponderato ( 1 , 2 , 1 ) per produrre un segnale privo della frequenza fondamentale , e similmente gli echi che provengono dagli ultimi tre impulsi vengono sommati in modo ponderato per produrre un secondo segnale privo della frequenza fondamentale . 
la differenza di fase tra i due segnali armonici principali cos calcolati fornisce una stima della velocit delle microbolle , mentre la radice quadrata della loro ampiezza fornisce una stima della quantit di microbolle presenti . 
il fatto che vengano utilizzati un minor numero di impulsi rispetto alle tecniche color e power doppler tradizionali determina la presenza di una accuratezza minore nella misurazione del segnale doppler . coded harmonic angio questa tecnica combina la tecnica pulse inversion con la tecnica di trasmissione degli impulsi a codici con il fine di aumentare la sensibilit per il segnale prodotto dalle microbolle e sopprimere il segnale proveniente dai tessuti stazionari . essa consiste nella trasmissione di una serie di impulsi codificati e nella loro decodificazione in fase di ricezione . 
un codice consiste in una serie di variazioni predefinite della frequenza e della fase allinterno di un impulso ultrasonoro . questo codice presente negli echi utili per la formazione dellimmagine ma non nel rumore , e quindi questa tecnica determina anche un miglioramento del rapporto segnale / rumore . 
the microbubbles directed towards the transducer are represented in red ( arrow ) , those flowing away from the transducer are visualised in blue , whereas the stationary microbubbles in the liver sinusoids are visualised in green . 
le microbolle con un flusso diretto vero il trasduttore vengono rappresentate in rosso ( freccia ) , in blu se presentano un flusso in allontanamento , ed in verde se sono stazionarie a livello dei sinusoidi epatici . volves transmitting four pulses , alternately inverted , along each scan line . 
the echoes from the first three are summed with weights ( 1 , 2 , 1 ) to give one fundamental - free signal , and the echoes from the last three are summed the same way to give a second fundamental - free signal . 
a disadvantage of using only a few transmission / receive sequences for each scan line is that the accuracy of doppler frequency measurement is much less than in conventional colour flow imaging . 
 coded harmonic angio coded harmonic angio sonography combines phase - inversion harmonic imaging with a coded transmission pulse technique that boosts weak microbubble signal and suppresses tissue signals by transmitting coded pulse sequences and decoding them on receipt . 
this code is present in genuine echoes but not in noise , so by using a special matched filter , designed to respond strongly to the transmitted code , snr can be also improved by this contrast - specific technique . 
if second harmonic components are present in an echo , this quarter cycle shift at the fundamental frequency will become a half a cycle shift at the second harmonic frequency . 
thus , the code of the second harmonic component of an echo will be modified from that transmitted , whereas the fundamental component will retain the code of the transmitted pulse . 
the pulses are transmitted at two power levels , where the first and third pulses are half - height amplitude relative to the second pulse . because all pulses are transmitted at a low acoustic power , little nonlinear tissue backscatter is generated . 
subsequently , the received echoes from the half - height transmitted pulses are scaled and subtracted from the full - height signal , which results in effective removal of tissue clutter . 
amplitude and phase modulation technique cadence contrast pulse sequencing ( cps ) the contrast pulse sequencing technique works by interrogating each scan line a number of times with pulses having various amplitudes and phases . 
a processor first amplifies the echo sequence from each transmission by a particular weighting factor ( for example 2 or 1 ) and then sums all the weighted echo sequences . 
by suitable choice of transmission pulses and weighting factors , it is possible to isolate or suppress the linear fundamental echoes from stationary tissues . the amplitude and phase modulation contrast - specific techniques produce high sensitivity to the microbubble nonlinear harmonic signals and optimal suppression of the linear quando un eco codificato corrisponde perfettamente con quello di riferimento i segnali elettrici del circuito in uscita sono alti . 
una discordanza nella posizione di una sola cifra produce invece un segnale elettrico di bassa intensit . possibile sopprimere selettivamente tutti gli echi che presentano un codice uguale al codice di trasmissione , e quindi il segnale delle frequenze fondamentali prodotte dai tessuti stazionari . 
in uneco che presenti la frequenza seconda armonica , lo spostamento di fase pari ad un quarto di ciclo che si riscontra nella frequenza fondamentale corrisponde ad uno spostamento di fase pari a met ciclo per la frequenza seconda armonica . 
tecnica a modulazione di ampiezza power modulation a basse energie acustiche di insonazione il segnale tissutale pu anche essere soppresso alternando la potenza acustica di insonazione piuttosto che la fase . 
conseguentemente gli echi caratterizzati da unintensit pari alla met di quella degli impulsi trasmessi vengono sottratti dagli echi di ampiezza regolare con il risultato di rimuovere il contributo dei tessuti stazionari . 
tecnica a modulazione di fase e di ampiezza cadence contrast pulse sequencing ( cps ) la tecnica contrast pulse sequencing funziona trasmettendo multipli impulsi dotati di ampiezza e fase variabile lungo ogni linea di vista . 
10 a - d principle of cadence contrast pulse sequencing . three pulses are transmitted along each line , and the first and the third are half the amplitude of the second pulse , which presents an opposed phase with respect to the others ( a ) , and the returning echoes are summed . 
tre impulsi in successione vengono inviati ogni linea di vista , il primo e lultimo impulso possiedono la met dellampiezza del secondo impulso che presenta fase invertita rispetto agli altri ( a ) , e gli echi rispettivi vengono sommati . 
per un mezzo lineare la somma risultante zero ( b )  . per un mezzo non lineare come le microbolle la somma produce un risultato diverso da zero sia per le frequenza non lineari fondamentali ( c ) che per le frequenze non lineari armoniche ( d )  . non linear foundamental non linear harmonic fig . 
angioma epatico ( freccia ) valutato mediante scansioni eseguite in fase arteriosa ( a ) , portale ( b ) e tardiva ( c ) dopo la somministrazione delle microbolle . 
pinto 1 , i - 71100 foggia , italy 2unit sanitaria locale ba 4 , ospedale di venere , via ospedale di venere 1 , i - 70012 carbonara , bari , italy 3universit degli studi di bari , istituto di chirurgia maxillo - facciale , piazza g . 
chieffi 40 , i - 70051 barletta , italy , tel . : + 39 - 339 - 2452701 , e - mail : paomi03@libero.it received : 13 august 2006 / accepted : 26 september 2006 / published online : 11 june 2007 abstract purpose . 
this study was done to evaluate the use of multidetector computed tomography ( mdct ) in the evaluation of jaw osteonecrosis , a recently described medical entity in patients receiving long - term intravenous or oral bisphosphonates , and to help radiologists recognise it to enable early diagnosis and appropriate management . 
jaw osteonecrosis is an established medical entity discovered in patients who have undergone treatment with bisphosphonates and dental extraction or other oral surgery . mdct with multiplanar ( mpr ) , volume rendering ( vr ) and three - dimensional ( 3d ) reconstructions allows accurate assessment of affected bone structures , enabling early diagnosis and suitable treatment planning . 
radiologists should be aware of the risk of osteonecrosis in patients treated with bisphosphonates and be able to distinguish it from other bone diseases ( osteomyelitis and osteoradionecrosis ) with which it enters the differential diagnosis . key words jaw osteonecrosis bisphosphonates oral surgery mdct riassunto obiettivo . 
la tc - md con ricostruzioni multiplanari ( mpr ) , volume rendering ( vr ) e 3d consente una valutazione accurata dellosteonecrosi mascellare associata a terapia con bifosfonati fornendo informazioni utili sulle strutture ossee coinvolte per un adeguato planning terapeutico . 
i medici radiologi devono essere a conoscenza del rischio di osteonecrosi al quale vanno incontro i pazienti trattati con bifosfonati ed essere in grado di distinguerla da altri processi patologici dellosso ( osteomielite e osteoradionecrosi ) con le quale entra in diagnosi differenziale . parole chiave mascella osteonecrosi bisfosfonati chirurgia orale tc - md p . 
although the mechanism of action of bisphosphonates essentially involves a powerful inhibition of bone resorption , the manner in which they block the destruction of hydroxyapatite and interfere with osteoclast function is still unclear [ 4 ]  . 
in addition to this , they have an antiangiogenic action that inhibits proliferation of endothelial cells . at the molecular level , bisphosphonates have been shown to influence osteoclast activity by modulating a cell - surface receptor or an intracellular enzyme [ 5 , 6 ]  . a precise causal relationship between bisphosphonate therapy and jaw osteonecrosis has yet to be established . nonetheless , risk factors have been identified and guidelines published for the prevention , early diagnosis , and management of this side effect , and there are multidisciplinary recommendations for reducing the incidence of jaw osteonecrosis in patients undergoing treatment with bisphosphonates and requiring oral surgery [ 7 ]  . 
dental extraction is often the triggering event , exposing bone to changes and alterations , even though the appearance of spontaneous gingival lesions , toothache , loosening of teeth and numbness is not uncommon . 
 the aim of this study was to use multidetector computed tomography ( mdct ) to evaluate jaw - bone changes caused by bisphosphonate - related osteonecrosis to provide a radiological description of this disease entity and help radiologists differentiate it from osteomyelitis and osteoradionecrosis and enable , with the aid of an accurate history and clinical assessment , its early diagnosis and appropriate treatment . 
 materials and methods thirty - eight patients presenting with pain in the mouth and temporomandibular joints , soft tissue infection , altered taste , numbness , and lip paraesthesia were examined by mdct . all patients had a history of neoplasm or osteoporosis , bisphosphonate use and recent oral surgery . 
ten of the patients had breast cancer , 12 had multiple myeloma , five had prostate cancer , nine had osteoporosis , one had breast cancer and osteoporosis and one had multiple myeloma and pancreatic cancer . all patients with neoplastic disease at the time of the mdct scan had received 4 mg monthly of intravenous zoledronate for periods ranging from 12 to 35 months . 
the patient with breast cancer and osi bifosfonati svolgono una azione inibitrice sullattivit degli osteoclasti e sono attualmente utilizzati per la cura dellosteoporosi , dellipercalcemia associata a patologie maligne e delle lesioni metastatiche osteolitche secondarie a tumore mammario , mieloma multiplo , malattia di paget , tumore prostatico [ 13 ]  . 
sebbene il meccanismo dazione di questi farmaci sia principalmente basato sul potente effetto inibitore che esercitano sul riassorbimento osseo , resta poco chiaro come questi blocchino la distruzione dellidrossiapatite e interferiscano sulla funzione degli osteoclasti [ 4 ]  . 
a livello molecolare , stato dimostrato , che i bifosfonati influenzano lattivit degli osteoclasti attraverso la modulazione di un recettore di superficie cellulare o un enzima intracellulare [ 5 , 6 ]  . una precisa relazione causale fra la terapia con bifosfonati e losteonecrosi della mascella non stata ancora stabilita . 
esiste per una identificazione dei fattori di rischio e lo sviluppo di linee guida per la prevenzione , la diagnosi precoce , il management terapeutico ed esistono raccomandazioni multidisciplinari per ridurre lincidenza delle osteonecrosi dellosso mascellare nei pazienti sottoposti a terapia con bifosfonati e che devono far ricorso a chirurgia orale [ 7 ]  . 
una estrazione dentaria spesso il primum movens dellesposizione ossea alle modificazioni ed alterazioni ossee , anche se non insolita la comparsa di lesioni gengivali spontanee , mal di denti , mobilit degli stessi e perdita della sensibilit . 
fattori sfavorevoli sono la presenza di comorbilit dentarie , che includono carie , ascessi , periodontiti ecc , concomitanti terapie steroidee , chemio e radio - terapia [ 8 ]  . scopo del nostro lavoro stato quello di valutare con tcmd le alterazioni dellosso mascellare riferibili ad osteonecrosi da bifosfonati per una maggiore riconoscibilit radiologica di tale tipo di osteonecrosi , anche con lausilio di una corretta anamnesi e una opportuna valutazione clinica , per una diagnosi differenziale con losteomielite e le osteoradionecrosi , una diagnosi precoce di osteonecrosi ed un adeguato planning terapeutico . materiali e metodi sono stati esaminati con tc - md 38 pazienti , giunti alla nostra osservazione con algie a livello del cavo orale e delle articolazioni temporo - mandibolari , infezioni dei tessuti molli , alterazioni del gusto e della sensibilit , parestesia delle labbra . 
six of the 38 patients ( three with breast cancer , two with prostate cancer and one with multiple myeloma ) had also received radiotherapy . all patients had undergone oral radiography and orthopantomography prior to ct imaging ; some had also had a biopsy , whereas others were to undergo biopsy within days of the ct study . 
in most patients ( n = 25 ) , small areas of increased bone density , as in new bone apposition , could be seen peripherally to the lesions , forming intraoral spicules . 
i pazienti con osteoporosi erano stati sottoposti a terapia con alendronato ( 70 mg / settimana ) o alendronato e clodronato ( 10070 mg / settimana ) , somministrati per via orale . 
levento scatenante losteonecrosi era stato per tutti i pazienti unestrazione dentaria tranne che per la paziente affetta da carcinoma mammario e da osteoporosi che aveva subito invece un trattamento endodontico . 
sei dei 38 pazienti ( 3 con carcinoma mammario , 2 con carcinoma prostatico e 1 con mieloma multiplo ) erano stati sottoposti anche a trattamento radioterapico . tutti i pazienti , prima dellesame tc , avevano gi effettuato un esame radiografico endorale ed ortopantomografico ; ad alcuni di essi era gi stato effettuato anche un prelievo bioptico ; altri sarebbero stati sottoposti a biopsia nei giorni successivi lesame tc . 
perifericamente alle lesioni erano presenti , nella maggior parte dei pazienti ( 25 ) , piccole aree di addensamento osseo , come da neoapposizione , che formavano delle vere e proprie spicule endo - orali . 
lindagine tc ha mostrato una grossolana alterazione osteostrutturale di tipo necrotico del processo alveolare sinistro della mascella superiore con interessamento del processo nasale e del processo zigomatico omolaterali e del pavimento del seno mascellare corrispondente , ben visibili nelle immagini tc assiali ( a , b ) , coronali ( c ) e nelle ricostruzioni in vr ( d , e )  . schwartz in 1982 [ 9 ]  . 
other authors described patients with metastasis and jaw osteonecrosis after chemotherapy [ 2 ]  . the toxic effects of chemotherapy for head and neck cancers , especially on vascular and bony structures , have been il follow - up dopo terapia ha mostrato risultati incoraggianti che per andrebbero validati con controlli a pi ampia distanza di tempo . 
a nelle immagini tc sono ben visibili lalterazione morfostrutturale a prevalente carattere litico destruente della regione molare della mandibola di sinistra ( immagini assiale , a e b ; coronale , c ; vr , d ) , associata a moderata reazione periostale laminata del margine interno ( freccia in b ) ed esterno ( freccia in a ) dellosso mandibolare , e la disomogeneit e lispessimento delle parti molli superficiali , associate a tumefazione e perdita del profilo interno della regione tonsillare ( testa di freccia in b )  . discussed for more than 20 years ( maduro et al . , 2003 [ 10 ] )  . avascular jaw necrosis was thought to be a chemically induced disease [ 11 ] and was grouped among the jaw alterations known as phosphorus necrosis [ 12 ]  . 
 in the united states , recent reports of a characteristic jawbone alteration , which never occurs after a single treatment with pamidronate or zoledronate [ 13 ] , have attributed the origin of jaw osteonecrosis to the widespread use of bisphosphonates , which are recommended by the american society of clinical oncology ( asco ) for the treatment of bone metastasis to breast cancer [ 14 , 15 ]  . 
sugli effetti tossici , in particolar modo di quelli vascolari ed ossei , della chemioterapia nel trattamento dei tumori della testa e del collo si discute da oltre 20 anni ( maduro et al . , 2003 [ 10 ] )  . 
multidetector computed tomography ( mdct ) : an extensive morphostructural lytic - destructive alteration involves the mandibular body , well visible in axial ( a ) and coronal ( c ) projections , the palatine and alveolar maxillary processes in the right median - paramedian area ( b , c ) , the petrous apex and the basilar part of the occipital bone , and the clivus with extension to the posterior clinoid processes ( d )  . 
tc : vasta alterazione morfostrutturale a carattere litico destruente in corrispondenza del corpo della mandibola , ben visibile in proiezione assiale ( a ) , coronale ( c ) , dei processi palatino ed alveolare del mascellare in sede mediana - paramediana destra ( b , c ) , dellapice della rocca petrosa sinistra nonch della pars basilare dellosso occipitale e del clivus con interessamento dei processi clinodei posteriori ( d )  . 
e ricostruzione in volume rendering ( vr ) con software dedicato per lo studio dellosso : bene identifica e delimita alterazioni ossee dellosso mascellare superiore ed inferiore . antibiotici a lungo termine e la lunga durata della terapia agevolava ovviamente la estensione della patologia stessa . negli stati uniti , recenti descrizioni di un caratteristica alterazione dellosso mascellare , che non si verifica mai in seguito ad un solo trattamento con pamidronato o zoledronato [ 13 ] , hanno attribuito al largo uso di bifosfonati , raccomandati dallamerican society of clinical oncology ( asco ) per il trattamento di metastasi ossee secondarie a carcinoma mammario [ 1415 ] la causa delle lesioni osteonecrotiche mascellari . 
the changes in bone metabolism associated with surgical treatment and implant trauma seem to be key factors in the development of osteonecrosis . a tooth extraction is the most common trigger [ 11 , 13 , 15 , p . 
multidetector computed tomography ( ct ) examination shows the presence of a morphostructural alteration of the upper maxillary left alveolar process that is heterogeneously dense due to the presence of multiple lytic areas ( a )  . 
lesame tc dimostra la presenza di una alterazione morfostrutturale del processo alveolare sinistro dellosso mascellare superiore che presenta densitometria disomogenea per la presenza di multiple areole litiche ( a )  . 
si associano irregolare ispessimento dei tessuti gengivali corrispondenti e la presenza di sottile tramite fistoloso che mette in comunicazione la cavit orale ed il seno mascellare omolaterale ( b ) , meglio evidente nella immagine vr ( c ) , completamente occupato da essudato con ispessimento della mucosa di rivestimento . sunzione di questi farmaci e linsorgenza di osteonecrosi mascellare . 
le modificazioni del metabolismo osseo associate ad un insulto chirurgico o ad un trauma protesico sembrano essere i fattori chiave nello sviluppo delle osteonecrosi . unestrazione dentaria la pi comune causa scatenate [ 11 , 13 , 15 , 16 ] anche se esistono casi in cui si verificano lesioni spontanee ed in zone non precedentemente interessate da avulsioni dentarie . 
la localizzazione delle lesioni dai dati della letteratura risulta essere come segue : nel 38%80 , 5% nella mascella superiore , nel 14%63% nella mascella inferiore e nel 5 , 5%23% in entrambe le mascelle [ 2 , 13 , 17 ] e concorda con i risultati del nostro studio . la diagnosi di osteonecrosi da bifosfonati dovrebbe essere basata principalmente su evidenze cliniche e reperti radiografici , oltre che su una accurata anamnesi . 
culture microbiche ( aerobico ed anaerobico ) consentono la identificazione dei patogeni responsabili della secondaria infezione [ 5 ]  . le indagini radiologiche rivestono un ruolo importante nella definizione del planning terapeutico . 
la tc - md risulta per essere tecnica fondamentale per il management terapeutico del pa16 ] , even though there have been cases of lesions arising spontaneously in areas not subjected to dental extractions . the most commonly reported sites of jaw osteonecrosis are the upper jaw in 38%80.5% of cases , the lower jaw in 14%63% and both jaws in 5.5%23% [ 2 , 13 , 17 ] ; this is in agreement with the findings of our study . the diagnosis of bisphosphonate - related jaw osteonecrosis primarily relies on clinical and radiographic evidence and an accurate history . 
the intrinsic features of cr high spatial and contrast resolution and its being ideally suited for the study of bone , associated with continuous technological evolution and the possibility of multiplanar reconstructions ( mprs ) , vr and 3d imaging ensured , in our experience , a correct diagnosis and accurate staging of the osteonecrotic lesions as well as the detection of complications . currently , no established treatment exists for this type of drug - induced lesion . 
although it may seem reasonable to think that withdrawal of intravenous bisphosphonates might improve the rate of regression of the disease , this has not yet been proposed as a form of management [ 18 ] , because there is no evidence of a clinical improvement of osteonecrosis [ 17 ]  . 
this is accounted for by the fact that bisphosphonates are avidly bound to the bone matrix around the active osteoclasts and , not being metabolised , they remain there in high concentrations over long periods of time [ 4 ]  . 
there has been much discussion about the treatment strategies to be adopted : antibiotic therapy , conservative or reconstructive surgery and hyperbaric oxygen therapy [ 17 , 19 ]  . 
le caratteristiche intrinseche della tomografia computerizzata con la sua elevata risoluzione spaziale e di contrasto e la sua prerogativa di essere la tecnica gold standard per lo studio dellosso , associate al continuo progresso tecnologico e alla possibilit di effettuare ricostruzioni mpr , su tutti i piani dello spazio , vr e 3d , nella nostra esperienza , hanno garantito unaccurata diagnosi ed un adeguato bilancio destensione delle lesioni osteonecrotiche nonch la identificazione di eventuali complicanze associate . non esiste attualmente un trattamento definito per questo particolare tipo di lesioni farmaco - indotte . 
anche se pu sembrar ragionevole pensare che la sospensione della somministrazione intravenosa di bifosfonati possa migliorare la percentuale di regressione di tale fenomeno , non c nessuno che ancora lo proponga come gestione terapeutica [ 18 ]  . 
questo pu essere ben spiegato considerando che i bifosfonati restano avidamente legati alla matrice ossea che circonda gli osteoclasti attivi e , non essendo metabolizzati , ivi permangono a concentrazioni ossee elevate per periodi lunghi di tempo [ 4 ]  . 
molto si discute sulle strategie terapeutiche da adottare : terapia antibiotica , chirurgia conservativa e o ricostruttiva e terapia iperbarica [ 17 , 19 ]  . conclusions conclusioni jaw osteonecrosis is an established disease entity encountered in association with bisphosphonate use and following dental extractions or other oral surgical procedures . 
mdct with mpr , vr and 3d reconstructions helps accurate diagnosis and provides detailed information about the structures involved and is therefore useful for appropriate treatment planning and for follow - up . 
radiologists need to be aware of the risk of osteonecrosis in patients receiving bisphosphonate treatment and should be able to differentiate it from other bone diseases , such as osteomyelitis and osteoradionecrosis [ 20 ] , even with the help of an accurate history and thorough clinical assessment . losteonecrosi della mascella ormai una accertata entit nosografica che si riscontra in associazione a terapia con bifosfonati ed in seguito ad estrazione dentaria o altra chirurgia orale . 
la tc - md con ricostruzioni mpr , vr e 3d consente di farne una accurata diagnosi e di fornire precise informazioni sulle strutture coinvolte per un adeguato planning terapeutico e per il follow - up . 
adelaide di torino , via zuretti 29 , i - 10126 torino , italy correspondence to : a barile , tel . : + 39 - 086 - 2414258 , fax : + 39 - 086 - 2311277 , e - mail : antonio.barile@cc.univaq.it received : 20 september 2005 / accepted : 30 august 2006 / published online : 11 june 2007 abstract purpose . 
postprocessing was done on an independent workstation ( advantage windows , ge medical system ) , with functool ( ge ) software , which allowed a quantitative evaluation of enhancement as a function of time . 
the lesions identified in the 39 patients included 23 soft tissue tumours ( 12 benign , 11 malignant ) and 16 bone tumours ( ten benign , six malignant )  . 
comparing the time - intensity diagrams of lesions of the same histological type , we found typical enhancement patterns for some bone tumours only , especially for bone , cartilaginous , fibrohistiocytic and pseudoinflammatory lesions . 
gli esami rm dinamici sono stati eseguiti con apparecchiature rm dotate di un magnete da 1 , 5 t e da 1 , 0 t , tramite bobine di superficie dedicate scelte in funzione del distretto da studiare prima e dopo somministrazione ev di mdc utilizzando sequenze rapide ed ultrarapide in successione . 
la post - elaborazione stata eseguita in tutti i casi tramite il software functool installato su una workstation indipendente ( advantage windows , ge medical system ) , che ha permesso , attraverso il posizionamento di una roi , di effettuare una valutazione quantitativa dellenhancement in funzione del tempo . 
le lesioni dei 39 pazienti esaminati sono risultate essere : 23 tumori dei tessuti molli di cui 12 benigni e 11 maligni e 16 lesioni ossee , di cui 10 benigne e 6 maligne . 
confrontando le curve intensittempo ( tic ) delle lesioni appartenenti ad uno stesso istotipo sono state identificate curve tipiche per alcune lesioni tumorali ossee ( serie ossea , cartilaginea , fibroistiocitica ) e per le lesioni infiammatorie . non stato possibile identificare una curva tipica allinterno dello stesso istotipo per le lesioni dei tessuti molli . 
la rm perfusionale ha mostrato un discreto livello di sensibilit e specificit nella diagnosi differenziale tra lesioni ad elevata ed a bassa attivit biologica e solo in alcuni casi stato possibile riscontrare una correlazione tra pattern perfusionale e istologia della lesione . 
i valori di pendenza dovrebbero quindi essere usati insieme con le immagini spin echo convenzionali e con altri dati diagnostici e clinici per restringere le possibili diagnosi differenziali e per poter predire con una significativa attendibilit la natura della lesione . key words perfusion mri musculoskeletal tumours contrast agents tumour perfusion parole chiave risonanza magnetica perfusionale tumori muscolosheletrici mezzi di contrasto perfusione tumorale a . 
primary bone tumours account for approximately 20% of all skeletal tumours , and they frequently affect young subjects , in whom they exhibit an aggressive growth pattern and high mortality and disability rates . 
the typical presenting complaint is an asymptomatic mass , although there may be mechanical symptoms caused by compression , traction or trapping of muscles and nerves [ 3 ]  . 
 in view of the development of surgical techniques and the possibilities offered by chemotherapy , the early diagnosis and accurate staging of the disease are becoming fundamental for radical treatment . 
clinically suspected musculoskeletal tumours are usually identified by radiography and computed tomography ( ct ) in the case of bone tumours , and ultrasound ( us ) and conventional magnetic resonance imaging ( mri ) in the case of soft tissue neoplasms [ 3 ]  . 
 dynamic contrast - enhanced mri relies on dynamic imaging through the use of fast or ultrafast sequences that allow one to follow the early enhancement kinetics of the tissue being studied [ 4 ]  . 
the study was prospective and included patients aged 1386 years with a first diagnosis of musculoskeletal tumour . twenty - three patients had soft tissue tumours , and 16 had bone tumours . 
patients were excluded if they had already undergone contrast - enhanced diagnostic studies of any kind ( ultrasound , ct , mri or scintigraphy ) , if they had undergone cytological or bioptic examination , and if they had received neoadjuvant therapy ( chemotherapy or radiotherapy )  . all mri studies were performed using 1.0 - t and 1.5 - t magnets ( signa , ge medical system , milwaukee , wi , usa ) , with dedicated surface - array coils selected on the basis of the region to be studied . 
for the conventional mri studies , t1 spin - echo , t2 spin - echo , t1 sequences with fat lapparato muscoloscheletrico costituito da una componente ossea e da tessuti molli ovvero muscoli , tendini , grasso , tessuto fibroso , vasi e nervi [ 1 , 2 ]  . 
i tumori primitivi dellosso rappresentano circa il 20% della totalit delle forme neoplastiche a localizzazione scheletrica , colpiscono frequentemente let giovanile , nella quale sono caratterizzati da un atteggiamento aggressivo e da un importante indice di mortalit e di invalidit . 
il quadro di esordio pi comune rappresentato da una massa asintomatica , possono essere tuttavia presenti sintomi meccanici riferibili a compressione , alla trazione o allintrappolamento di muscoli e nervi [ 3 ]  . vista levoluzione delle tecniche chirurgiche e le possibilit offerte dalla chemioterapia , una diagnosi precoce ed una accurata stadiazione della patologia si rendono sempre pi importanti e fondamentali per raggiungere la radicalit del trattamento . 
lindividuazione di una neoplasia muscoloscheletrica clinicamente sospettabile compete di solito allesame radiografico ed alla tomografia computerizzata ( tc ) per le lesioni ossee , allecografia ed alla risonanza magnetica ( rm ) tradizionale per le lesioni dei tessuti molli [ 3 ]  . lo studio contrastografico dinamico con rm si fonda su un imaging dinamico mediante lutilizzo di sequenze rapide o ultrarapide che consentono di seguire la cinetica di impregnazione precoce con mdc del tessuto in studio [ 4 ]  . 
lo scopo di questo studio quello di valutare le potenzialit ed i limiti della rm perfusionale nella caratterizzazione delle lesioni tumorali muscoloscheletriche . materiali e metodi nel periodo compreso tra gennaio 2003 e settembre 2005 sono stati valutati gli esami rm standard e rm perfusionali di 39 pazienti . 
nello studio prospettico sono stati inclusi pazienti con patologia neoplastica muscoloscheletrica alla prima diagnosi con et compresa tra i 13 e gli 86 anni , 23 presentavano tumori dei tessuti molli e 16 tumori ossei . 
i criteri di esclusione dal reclutamento dei pazienti per questo studio sono stati : pazienti che avevano gi effettuato esami diagnostici contrastografici di qualsiasi tipologia ( ecografia , tc , rm o scintigrafia ) ; pazienti che erano gi stati sottoposti ad esame citologico o bioptico ; pazienti che erano stati sottoposti a terapie neoadiuvanti ( chemioterapia , radioterapia )  . gli esami rm sono stati eseguiti con apparecchiature rm con magneti da 1 , 0 e 1 , 5 t ( signa , ge medical system , milwakee , wi , usa )  . 
we then performed eight 19 - s scans in fast succession , with a scan delay that varied with the region being studied but that never exceeded 20 s so as to ensure good arterial - phase perfusion in all cases . 
the last scan was performed 5 min after the infusion of contrast material . postprocessing was carried out with functool software installed on an independent workstation ( advantage windows , ge medical system ) , which allows a quantitative assessment of enhancement as a function of time in a given region of interest ( roi )  . 
the rois were uniform and measured 20 mm2 in all cases , and the software - generated curves were based on graphs in which the x - axis represented a time scale reporting the progressive number of images acquired and the y - axis represented enhancement expressed as a percentage . the resulting time - intensity curves provided a graphic representation of contrast perfusion during and immediately after the administration of contrast material , from which we could derive quantitative information about the lesions : time to enhancement , wash - in ( positive slope ) , peak enhancement , and wash - out ( negative slope )  . thirty - four patients then underwent surgical excision of the tumour , and for each one , we were able to compare and confirm the imaging diagnosis , including the areas where perfusion patterns were measured , against the histological type and grade provided by gross pathology and histopathology . 
the remaining five patients underwent biopsy and histological assessment of the histological type and grade . results the lesions of the 39 patients included 23 soft tissue tumours , 12 of which were benign and 11 malignant , and 16 bone tumours , ten of which benign and six malignant . 
 una volta individuato il piano migliore per studiare la lesione , e dopo aver effettuato una prima acquisizione precontrasto , stato somministrato tramite catetere endovenoso da 20 gauge posizionato nella vena basilica o cefalica un bolo di mdc paramagnetico ( gadolinium - dtpa , 0 , 1 mmol / kg ) utilizzando un iniettore automatico , alla velocit di 2ml / s seguito da 10 ml di soluzione fisiologica . 
sono state quindi eseguite in rapida successione 8 scansioni della durata di 19 secondi ciascuna , con un ritardo di acquisizione della sequenza , dalliniezione del bolo iniziale , dipendente dal distretto in esame ma comunque non superiore ai 20 secondi per ottenere in tutti i casi una buona perfusione in fase arteriosa . 
lultima scansione stata eseguita a 5 minuti di distanza dallinfusione di mdc . la post - elaborazione stata eseguita in tutti i casi tramite il software functool installato su una workstation indipendente ( advantage windows , ge medical system , milwaukee , wi , usa ) , che ha permesso , attraverso il posizionamento di una roi , di effettuare una valutazione quantitativa dellenhancement in funzione del tempo . 
la roi in tutti i casi stata di 20 mm2 ; il software ha fornito la curva risultante rappresentata su assi cartesiani , aventi per ascissa la successione temporale delle sequenze effettuate e per ordinata lenhancement misurato in percentuale . 
questo ha permesso di ricavare informazioni quantitative sulle lesioni : tempo di inizio enhancement , frazione di wash - in ( inclinazione della curva ) , massimo enhancement e frazione di wash - out ( pendenza negativa )  . trentaquattro pazienti sono stati quindi sottoposti ad intervento chirurgico escissionale e di ognuno stato possibile confrontare e confermare la diagnosi strumentale , comprese le aree di misurazione del comportamento perfusionale della lesione , con esame macroscopico ed istologico per la valutazione dellistotipo e del grading . 
i restanti 5 pazienti sono stati invece sottoposti ad esame bioptico con successiva valutazione istologica dellistotipo e del grading . risultati le lesioni dei 39 pazienti esaminati sono risultate essere : 23 tumori dei tessuti molli di cui 12 benigni e 11 maligni e 16 lesioni ossee di cui 10 benigne e 6 maligne . 
la pendenza delle curve intensit - tempo raffrontata con i risultati del grading delle lesioni ottenuti allesame istologico ha evidenziato sensibilit e specificit rispettivamente del 64% / 58% per i tumori dei tessuti molli e del 86% / 67% per i tumori ossei . nei tumori ossei ( tabella 1 ) , lesioni ad alta ed a bassa aggressivit biologica presentavano una cinetica contrastografica perfusionale differente ed abbastanza caratteristica ; a . 
tumour growth , in fact , requires a permissive microenvironment , and the tumour itself ensures this through the induction of neoangiogenesis , without which the lesion could not grow larger than 1 or 2 mm [ 15 ]  . 
in dynamic mri , images are acquired during and immediately after bolus injection to study the dynamic , physiological phenomenon of the distribution of contrast material in the capillaries and in the interstitial spaces of the tissues ( perfusion ) [ 4 ]  . 
with the first pass of contrast material through the capillaries , a fast , unidirectional diffusion occurs in the tissue as a result of the high concentration gradient between the intravascular and interstitial space : in normal tissues , approximately 50% of the circulating contrast material diffuses from the blood into the extravascular compartment . 
infatti , affinch ci si verifichi necessaria la presenza di un microambiente permissivo ; il tumore stesso rende possibile ci grazie allinduzione di fenomeni neoangiogenetici senza i quali la lesione non potrebbe raggiungere dimensioni di pi di uno o due millimetri [ 15 ]  . 
nella rm dinamica , le immagini vengono acquisite durante e immediatamente dopo la somministrazione del bolo al fine di studiare quel fenomeno dinamico e fisiologico che la distribuzione del mdc nei capillari e negli spazi interstiziali dei tessuti ( perfusione ) [ 4 ]  . 
the interval between the end of the first pass and the equilibrium state depends on the size of the interstitial space and may vary from up to 20 s in lesions with a small interstitial space to more than 35 min in tissues with a larger interstitial ziale : nel tessuto normale circa il 50% del mdc circolante diffonde dal sangue al compartimento extravascolare . 
dopo il primo passaggio , la velocit di diffusione si riduce rapidamente perch la concentrazione media del contrasto rimesso in circolo diminuita a causa dellulteriore diluizione del sangue e del parziale accumulo nello spazio interstiziale di tutto il corpo [ 6 ]  . 
the enhancement curve of the tumour area ( a ) ( arrow a ) is characterised by a very fast and high wash - in and by a fast wash - out with a descending trend . 
a la curva di enhancement dellarea tumorale ( freccia a ) si caratterizza per un rapidissimo ed elevato wash - in ed un rapido wash - out con tendenza a scendere . 
the enhancement curve of the tumour area ( a ) ( arrow a ) is characterised by a very fast and high wash - in and high wash - out with a plateau trend . 
the enhancement curve of the tumour area ( a ) ( arrow a ) is characterised by a moderate arterial wash - in , a plateau and a moderate wash - out . 
4a , b curva intensit - tempo delle lesioni simil - infiammatorie ( osteoma osteoide della metafisi distale del femore ( b ) con segnalazione dei roi di misurazione )  . 
liposarcoma del cavo popliteo ( c ) ; d la curva di enhancement dellarea tumorale ( freccia b ) mostra un wash - in arterioso , rapido wash - out con tendenza a scendere . space [ 6 , 7 ]  . 
only in highly vascular lesions with a small interstitial space is there seen a very early wash - in with a rapidly rising slope of the time - intensity curve and an equally early wash - out within the first minutes of contrast injection [ 8 ]  . the aim of contrast - enhanced dynamic mri is to detect and depict differences in early intravascular and interstitial distribution of contrast [ 9 , 10 ]  . 
capillary perfusion , the rate of diffusion and the amount of water - soluble contrast material temporarily accumulated in the interstitial space may vary considerably from tissue to tissue : these processes are influmo di 20 secondi in lesioni con uno spazio interstiziale ridotto a pi di 35 minuti in tessuti con uno spazio interstiziale pi grande [ 6 , 7 ]  . 
solo nelle lesioni altamente vascolarizzate , con uno spazio interstiziale ridotto , abbiamo un wash - in precocissimo caratterizzato da una alta pendenza della curva intensit - tempo e un wash - out altrettanto precoce entro il primo minuto dalliniezione del bolo [ 8 ]  . lo scopo dello studio perfusionale dinamico tramite rm di individuare e descrivere le differenze nella distribuzione iniziale intravascolare e interstiziale del mdc [ 9 , 10 ]  . 
the enhancement curve of the tumour area ( b ) ( arrow a ) is characterised by a fast and early wash - in , a plateau trend and a slow , progressive and uniform washout . 
tgc delle guaine dei flessori del ginocchio ( a ) ; b la curva di enhancement dellarea tumorale ( freccia a ) presenta un rapido enhancement precoce , una tendenza al plateau ed un wash - out lento , progressivo e costante . 
as can be inferred from our results , among bone tumours , we were able to identify some typical timeintensity curves both for lesions with low and high biological aggressiveness and for some histological types of tumour . 
however , some remarks need to be made on the absolute significance of these curves : although there is a statistically significant difference in the slope values of benign and malignant lesions and in the appearance of the different curves within different histological types of tumour , these data should always be related to all the information provided by the different diagnostic modalities ( radiography , ct , mri )  . some typically benign but vascular lesions ( eosinophilic granuloma , gct , osteoid osteoma ) may , depending on the stage of lesion when the study is conducted ( active , calm etc . ) , display very similar slope values to malignant tumours . 
come si evince dai nostri risultati stato possibile , per i tumori dellosso , identificare alcune curve intensit tempo tipiche sia per lesioni a bassa che ad alta aggressivit biologica sia nel differenziare alcuni istotipi tumorali . 
 tuttavia necessario fare delle considerazioni sul significato assoluto di tali curve : infatti bench ci sia una differenza statisticamente rilevante nel valore delle pendenze delle lesioni benigne e di quelle maligne ed anche nellaspetto delle diverse curve nellambito di differenti istotipi tumorali , questi dati devono essere sempre considerati nel complesso delle informazioni ottenute dalle diverse metodiche diagnostiche ( esame radiografico , tc , rm )  . infatti alcune lesioni tipicamente benigne ma discretamente vascolarizzate e perfuse [ granuloma eosinofilo , tumore a cellule giganti del sacro ( tgc ) , osteoma osteoide ] possono avere , a seconda della fase in cui lo studio viene eseguito ( attiva , calma , ecc . ) valori di pendenza molto simili a quelli dei tumori maligni . 
al contrario , possono essere osservati tumori istologicamente maligni con valori di pendenza della curva di perfusione relativamente bassi ( tumori altamente necrotici , condrosarcomi con ridotta vascolarizzazione )  . 
although bone tumours exhibit typical curves among the different histological types , the final diagnosis and the attempt to characterise the lesion should always take into account the data provided by the different diagnostic imaging modalities . 
 soft tissue lesions do not exhibit typical curves among the different histological types , and therefore , the definitive diagnosis is dependent on all the diagnostic information provided by conventional imaging modalities ( ultrasound and mri ) and ultimately by biopsy . dal nostro studio si pu evincere che grazie ai progressi tecnologici delle apparecchiature rm e dei software ad esse collegati oggi possibile sfruttare nel migliore dei modi le informazioni relative alla fase contrastografica delle lesioni muscoloscheletriche . 
fabrizzi azienda ospedaliero - universitaria ospedali riuniti - ancona , servizio di radiologia presidio salesi , via corridoni 11 , i - 60123 ancona , italy correspondence to : c . 
the ct images were reviewed blinded to the histological findings , and attention was paid to the number and size of cysts so as to classify the lesions into the three groups described by stocker et al . 
areas with small - sized cysts ( < 2 cm ) were detected by ct in two patients ( 33.3% ) , areas with large cysts ( > 2 cm ) were seen in three cases ( 50% ) whereas in the remaining case , the diagnosis was mixed type i and type ii cam . 
ct proved to be accurate in identifying and characterising cam and provided important information on lesion site and extension . key words cystic adenomatoid malformation paediatric chest ct malformative lung lesion riassunto obiettivo . 
le immagini tc sono state rivalutate in ceco rispetto ai reperti istologici ponendo attenzione al numero e alle dimensioni delle cisti cos da classificare le lesioni nei tre tipi descritti da stocker . 
aree con cisti di piccole dimensioni ( < 2 cm ) sono state evidenziate alla tc in 2 pazienti ( 33 , 3% ) , aree con cisti voluminose ( > 2 cm ) sono state osservate in 3 casi ( 50% ) , mentre nel restante caso stata posta diagnosi di mac di tipo misto i e ii . 
la classificazione tc di stocker risultata concordante con lesame anatomo - patologico in 4 casi , mentre nei restanti 2 casi le lesioni sono state classificate come tipo i o ii alla tc e come lesioni miste ( tipo i e ii ) allistopatologia . 
lesame tc risultato essere una metodica accurata nellidentificare e caratterizzare la mac fornendo inoltre importanti informazioni sulla sede ed estensione della lesione . parole chiave malformazione adenomatoide - cistica tc del torace pediatrico lesioni malformative del polmone introduction introduzione c . 
this structural feature promotes the creation of a valve mechanism , with pulmonary hyperexpansion , compression of the normal lung and development of severe respiratory distress [ 6 , 7 ]  . 
classified cam into three types on the basis of the clinical and histological findings [ 10 ] : type i ( 50% ) : multiple large cysts , with a diameter greater than 2 cm , or a single large cyst surrounded by numerous smaller cysts type ii ( 42% ) : multiple small cysts , most smaller than 1 cm ; this type is frequently associated ( 26% of cases ) with other congenital malformations type iii ( 3% ) : malformation made up of numerous small cysts with a diameter less than 0.5 cm with cuboidal epithelium and most often collapsed walls , forming a solid mass ; it is the least common form and has the worst prognosis , with a remarkable incidence of foetal prematurity and hydrops due to cardiac compression and vena cava obstruction computed tomography ( ct ) is required for determining the type and extension of cam , information needed for surgical planning and for identifying possible coexisting malformations . 
the aim of our study was to assess the accuracy of ct in classifying the different types of cam , taking histopathology as the gold standard . materials and method we retrospectively reviewed six cases of cam ( four males and two females ; age range : 1 day to 9 years ) studied between 2000 and 2004 . 
in two cases ct , was carried out with a helical scanner ( tomoscan av e1 philips , japan ) and in four cases with a multislice device ( light speed ultra , general electric , healthcare , milwaukee , wi , usa )  . 
ct scans were carried out without contrast matela malformazione adenomatoide - cistica ( mac ) fu descritta per la prima volta come entit distinta da chin e tang nel 1949 [ 1 ]  . 
rappresenta circa il 25% di tutte le lesioni polmonari congenite ed caratterizzata da una proliferazione adenomatoide dei bronchioli terminali con formazione di masse solide , cistiche o miste allinterno del parenchima polmonare ; la vascolarizzazione ha origine dalla circolazione bronchiale , ma raramente pu dipendere da un vaso anomalo sistemico [ 25 ]  . 
le cisti , che comunicano sia tra loro sia con lalbero bronchiale , sono prive di tessuto cartilagineo di supporto a livello della connessione con i bronchi : questa caratteristica strutturale facilita linstaurarsi di un meccanismo a valvola , con iperespansione polmonare , compressione del polmone normale e comparsa di un grave distress respiratorio [ 6 , 7 ]  . 
questo rischio , associato a quello di una degenerazione maligna del tessuto adenomatoide va considerato nella decisione se trattare o meno chirurgicamente un paziente asintomatico [ 8 , 9 ]  . 
la mac stata classificata da stocker in base al quadro clinico e istologico in tre tipi [ 10 ] : i tipo ( 50% ) : cisti multiple e grandi , con un diametro superiore a 2 cm , o singola grande cisti circondata da numerose cisti pi piccole ; ii tipo ( 42% ) : cisti multiple e di piccole dimensioni , la maggior parte inferiori ad 1 cquesto tipo di lesione frequentemente associato ( 26% circa dei casi ) ad altre malformazioni congenite ; iii tipo ( 3% ) : malformazione formata da numerose piccole cisti dal diametro inferiore a 0 , 5 cm con un epitelio cuboidale e con pareti il pi delle volte collabite , cos da costituire nel suo complesso una massa solida . 
la forma pi rara e a prognosi peggiore , con notevole incidenza di prematurit e di idrope fetale per compressione cardiaca e ostruzione venocavale . la tc indispensabile nella determinazione del tipo e dellestensione della mac , informazioni necessarie per una corretta pianificazione chirurgica , e per lidentificazione di eventuali lesioni malformative coesistenti . 
scopo del nostro studio valutare laccuratezza della tc nel classificare i diversi tipi di mac assumendo come gold standard il riscontro anatomo - patologico . materiali e metodi abbiamo rivalutato in modo retrospettivo 6 casi di mac ( 4 maschi e 2 femmine ; range di et : 1 giorno9 anni ) che tra il 2000 e il 2004 sono giunti alla nostra osservazione . 
tutti i pazienti , alla luce del sospetto diagnostico ecografico prenatale o della sintomatologia clinica , sono stati sottoposti ad esame radiografico e tc del torace , e ad intervento chirurgico di lobectomia . 
patients 5 patients 1 patient symptoms asymptomatic patients symptomatic patients site < 5 months 9 years 3 asymptomatic 2 respiratory distress 1 recurrent lung infections chest x - ray : 2 negative ; 1 triangular opacity 2 opacities ; 1 hyperlucency 3 upper lobe ( 2 right - 1 left ) 1 lingula 2 left lower lobe n pazienti 5 pazienti 1 paziente sintomi pazienti asintomatici pazienti sintomatici sede < 5 mesi 9 anni 3 asintomatici 2 distress respiratorio 1 infezione polmomare ricorrente 2 negative 1 opacit triangolare 2 opacit 1 iperdiafania 3 lobo polmonare superiore ( 2 dx - 1 sn ) 1 lingula 2 lobo polmonare inferiore sn rial in four cases and with the intravenous administration of a bolus of iodinated contrast material in the remaining two cases . 
the classification of lesions obtained with ct was then correlated with the histopathological findings . results the patients age , gender , symptoms and radiographic findings are shown in table 1 . 
the lesions were located in the upper lung lobe in three cases ( two in the right lobe , one in the left lobe ) , in the lingula in one case and in the lower left lobe in the remaining two cases . 
le immagini sono state acquisite con uno spessore di strato di 5 mm , pitch 1 e ricostruite a 2 , 5 mm ( 120 kv , 50 ma , 1 s ) lesame tc stato eseguito senza mezzo di contrasto ( mdc ) in 4 casi mentre nei restanti 2 si resa necessaria la somministrazione di mdc iodato a bolo per via endovenosa . 
si proceduto poi a confrontare la classificazione delle lesioni effettuata con la tc con i corrispettivi reperti anatomo - patologici . risultati le caratteristiche dei pazienti per quanto riguarda let , il sesso , la sintomatologia e i reperti radiografici sono descritti nella tabella 1 . 
2 rx : iperdiafania rotondeggiante con orletto periferico . no in tre casi il lobo polmonare superiore ( 2 a destra , 1 a sinistra ) , in un caso la lingula e nei restanti 2 il lobo polmonare inferiore sinistro . 
le due lesioni localizzate nel lobo polmonare inferiore sinistro hanno necessitato , in aggiunta allindagine tc , di un esame di rm per meglio evidenziare il tipo di vascolarizzazione , sistemica o polmonare , cos da porre diagnosi differenziale tra mac e sequestro polmonare . il diametro massimo delle cisti stato 8 cm con un range variabile da 0 , 5 a 10 cm ( media 4 , 5 cm )  . 
la classificazione tc di stocker risultata concordante con lesame anatomo - patologico in 4 casi ( 66 , 7% ) , mentre nei restanti 2 casi ( 33 , 3% ) le lesioni sono state classificate come tipo i o ii alla tc e come lesioni miste ( tipo i e ii ) allistopatologia ( tabella 2 )  . 
in un caso la classificazione tc risultata corretta ma lesame istopatologico ha evidenziato la coesistenza di sequestro polmonare . discussione la mac una lesione malformativa dovuta ad un arresto focale dello sviluppo polmonare prima della 17a settimana di fig . 
mac di tipo misto i e ii . with histopathology in four cases ( 66.7% ) , whereas in the remaining two cases ( 33.3% ) , the lesions were classified as type i and type ii at ct and as mixed ( type i and ii ) at histopathology ( table 2 )  . 
in one case , ct classification was correct , but histopathology revealed the coexistence of pulmonary sequestration . discussion cam is a malformation due to focal arrest in foetal lung development before the 17th week of gestation and may be associated , in 4%26% of cases , with other congenital abnormalities . 
the diagnosis is generally provided by prenatal ultrasound , which has a good degree of accuracy in classifying lesions ( 77% ) but is rarely able to identify coexisting sequestration . 
when the diagnosis is prenatal , the lesion is asymptomatic at birth in 71% of cases , and in 56% it regresses spontaneously despite a possible initial enlargement [ 11 , 12 ]  . 
during the first days of life , radiography typically shows a homogeneous opacity due to the presence of fluid in the alveoli ; the appearance then becomes cystic , with multiple hyperlucent areas due to fluid reabsorption and pneumatization of the lesion . 
quando la diagnosi posta in utero la lesione asintomatica alla nascita nel 71% dei casi e nel 56% regredisce spontaneamente nonostante un possibile iniziale ingrandimento [ 11 , 12 ]  . 
nei primi giorni di vita laspetto radiografico tipico quello di una opacit omogenea per la presenza di liquido allinterno degli alveoli che poi evolve verso laspetto cistico con multiple aree radiotrasparenti dovuto al riassorbimento dei fluidi e alla pneumatizzazione della lesione . 
per un fenomeno di airtrapping le cisti possono andare incontro ad un rapido ingrandimento con shift controlaterale del mediastino e conseguente distress respiratorio [ 13 ]  . la tc la metodica pi sensibile nella diagnosi di mac . pu evidenziare il persistere di anomalie parenchimali anche a fronte di un esame eco - radiografico negativo . 
it may reveal the persistence of parenchymal abnormalities even when ultrasound and radiography are negative . ct is also necessary for determining the type and extension of cam , for identifying possible coexisting lesions and for differentiating between cam and extralobar pulmonary sequestration , which consists of a portion of lung tissue without bronchial and vascular connections . 
in congenital lobar emphysema , the hyperexpansion of a lobe , generally an upper lobe or the right middle lobe , may generate a mass effect and be confused with cam : the ct identification of hyperexpanded but normal lung parenchyma will easily lead to a diagnosis of congenital lobar emphysema . interstitial pulmonary emphysema may mimic cam when it is complicated by extensive air collections , even though these are typically associated with linear collections . 
on ct , cam may appear as an area of small - sized cysts ( < 2 cm ) associated with other lesions ( areas of consolidation or lager cysts ) , as macrocystic lesions ( > 2 cm ) or as hypodense areas made up of microcysts . 
at times , airfluid levels are visible in some cysts , above all in type i and type ii cysts [ 14 , 15 ]  . recent studies have reported that cam may be accompanied by microscopic foci of bronchioloalveolar carcinoma , mucosal hyperplasia and atypical nonmucinous adenomatous hyperplasia . 
in addition , in type iv , there is not only a risk of pleuropulmonary blastoma developing over time but also the possibility that the two entities coexist from the beginning within the same lesion [ 16 , 17 ]  . the treatment of precancerous lesions is still debated , as the risk of developing a neoplasm , generally rhabdomyosarcoma , seems to be independent of surgical resection of cam altra patologia che pu entrare in diagnosi differenziale lenfisema lobare congenito , le cisti broncogene e lernia diaframmatica . 
nellenfisema lobare congenito liperespansione di un lobo , in genere un lobo superiore o il lobo medio di destra , pu determinare un effetto massa ed essere confuso con la mac : alla tc lidentificazione di parenchima polmonare iperespanso ma normale , pu facilmente far porre la diagnosi di enfisema lobare congenito . 
lenfisema polmonare interstiziale pu mimare la mac quando complicato con ampie raccolte aeree , anche se queste si associano tipicamente a raccolte di tipo lineare e , soprattutto , preceduto da una ventilazione a pressione positiva con barotrauma . 
allesame tc la mac si pu presentare come unarea formata da cisti di piccole dimensioni ( < 2 cm ) associata ad altre lesioni ( aree di consolidazione o cisti di dimensioni maggiori ) , come lesioni macrocistiche ( > 2cm ) o come aree ipodense formate da microcisti . 
a volte visibile in alcune cisti , soprattutto nel tipo i e ii , un livello aria - fluido [ 14 , 15 ]  . recenti studi hanno messo in evidenza come la mac possa accompagnarsi a foci microscopici di carcinoma bronchioloalveolare , di iperplasia mucosa e di iperplasia adenomatosa atipica non mucinosa . 
nel tipo iv di mac inoltre c il rischio non solo di sviluppo negli anni del blastoma pleuropolmonare , ma anche la possibilit che queste due entit coesistano fin dallinizio allinterno della stessa lesione [ 16 , 17 ]  . nellottica di una lesione precancerosa la pianificazione terapeutica tuttora dibattuta in quanto il rischio di sviluppare una lesione neoplastica , in genere il rabdomiosarcoma , sembra essere indipendente dallasportazione chirurgica della mac [ 18 ]  . 
la recidiva dopo asportazione chirurgica comunque eccezionale . i risultati ottenuti con questo studio , in linea con i dati presenti in letteratura , hanno confermato come lesame radiografico sia poco sensibile nei pazienti asintomatici . 
recurrence after surgical removal is , however , an exceptionally rare occurrence . the results obtained in our study , in agreement with the literature data , confirmed that chest radiography has poor sensitivity in asymptomatic patients . 
symptoms were virtually absent in the cases of prenatal diagnosis , whereas recurrent lung infections in the eldest patient ( 9 years ) prompted the clinician to request a ct scan . 
when chest radiography is negative , ct should nonetheless be performed , as it has higher sensitivity above all in the detection of small lesions . in our study , ct correlated with histopathology in 66.7% of cases , whereas in 33.3% , histopathology revealed areas with mixed lesions ( types i and ii )  . 
mixed grading is common in cam due to the presence of different types in different areas within the same lesion . the diagnosis of cam in a context of pulmonary sequestration is not always straightforward , and in most , cases only histology is able to distinguish between the two entities . 
in particular , the differential diagnosis with extralobar sequestration proves difficult when cam is located in the lower lobes and the cystic component is poorly represented ( type iii )  . 
in addition , the use of contrast material also visualises the relationships between the lesion and the bronchial tree and large mediastinal vessels , which is essential for surgical planning . 
in two cases in our study , despite the use of an automatic system for tracking peak enhancement ( smartprep ) , the childs hyperkinetic circulation and small vessel diameter did not allow a correct vascular study of the arterial supply to the lesion . 
in both cases , we used mri , which successfully detected the bronchial origin of the anomalous vessel in one case but was unable to visualise the origin in the second case . to obtain a good ct study , thin - slice acquisitions are usually sufficient , even with low kilovoltage and amperage settings ( low dose )  . 
contrast material should always be used in doubtful cases in which the site and morphological features are not typical of cam or when the surgeon requires precise spatial visualisation of the lesion because of its closeness to mediastinal vessels . 
contrast material is also indispensable when there is a doubt between lobar sequestration and cam : in this case , use of an automatic peak enhancement tracking system can help to identify the bronchial or systemic origin of the anomalous vessel . ( 9 anni ) sono state le infezioni polmonari ricorrenti ad indurre il clinico a richiedere un esame tc . 
nel nostro studio la tc risultata essere concordante con lesame isto - patologico nel 66 , 7% dei casi mentre nel 33 , 3% listopatologia ha evidenziato aree con lesioni miste ( tipo i e ii )  . 
il grading misto frequente nella mac per la presenza di tipi differenti nelle diverse aree allinterno della stessa lesione . la diagnosi di mac su sequestro polmonare non sempre agevole e nella maggior parte dei casi solo lesame istologico riesce a differenziare le due entit . 
specialmente quando la mac si trova a livello dei lobi inferiori e la componente cistica poco rappresentata ( tipo iii ) , la diagnosi differenziale con il sequestro extralobare risulta difficoltosa . 
in questo caso solo il comportamento contrastografico della lesione alla tc consente di differenziarla dal sequestro : la mac infatti presenta una vascolarizzazione bronchiale e non sistemica come il sequestro . 
lutilizzo del mezzo di contrasto ( mdc ) inoltre permettere di studiare non solo la vascolarizzazione della lesione , ma anche il rapporto di questa con lalbero bronchiale e con i grossi vasi mediastinici , elementi indispensabili per la pianificazione chirurgica . 
nel nostro studio in due casi , nonostante lausilio del localizzatore automatico del picco massimo di enhancement ( smart - prep ) , il circolo ipercinetico del bambino e il piccolo calibro dei vasi , non ha permesso un corretto studio vascolare dellafferenza arteriosa della lesione per cui stato necessario ricorrere alla rm che ha evidenziato lorigine bronchiale del vaso anomalo in un caso mentre nel restante anche la rm non stata in grado di visualizzarne lorigine . per ottenere un buon esame tc in genere sufficiente un esame a strato sottile , anche a basso voltaggio e amperaggio ( low dose ) ; lutilizzo del mdc dovrebbe essere sempre effettuato soprattutto nei casi dubbi , in cui la sede e le caratteristiche morfologiche non sono dirimenti per mac o , qualora il chirurgo , data la stretta vicinanza con i grossi vasi mediastinici , necessiti di una precisa visualizzazione spaziale della lesione . 
il mezzo di contrasto , inoltre , indispensabile qualora sussista il dubbio tra sequestro lobare e mac : in questo caso lutilizzo del localizzatore automatico del picco massimo di enhancement utile per evidenziare lorigine sistemica o bronchiale del vaso anomalo . conclusioni conclusions given the close correlation between ct and histopathology , ct may be considered indispensable when cam is suspected , both to differentiate it from other pulmonary malformations and to study its morphological features , elements that are useful for surgery and prognosis . 
lagalla1 1dipartimento di biotecnologie mediche e medicina legale sezione di diagnostica per immagini , 2dipartimento di medicina interna , policlinico universitario , via del vespro 127 , i - 90127 palermo , italy correspondence to : t.v. 
lecografia cs in grado di individuare xta in pazienti con ife ed esame clinico negativo , offrendo una migliore qualit dellimmagine rispetto allhrus . key words achilles tendon familial hypercholesterolemia ultrasonography xanthomas parole chiave tendine dachille ipercolesterolemia familiare ecografia xantomi introduction introduzione familial hypercholesterolaemia ( fh ) is an inherited autosomal dominant disorder of lipoprotein metabolism characterised by a defect in the low - density lipoprotein ( ldl ) receptor gene [ 1 ]  . 
this leads to progressively rising ldl cholesterol levels , lipid deposition in the achilles tendon in the lipercolesterolemia familiare ( if ) una malattia ereditaria del metabolismo delle lipoproteine a trasmissione autosomica dominante , caratterizzata dal difetto di un singolo gene , quello del recettore per le lipoproteine a bassa densit ( ldl ) [ 1 ]  . 
fh may manifest in the heterozygous form ( hfh ) , with an incidence of 1 / 500 individuals in the general population , or in the homozygous form , with an incidence of 1 / 1 , 000 , 000 [ 4 ]  . 
common clinical criteria for a diagnosis of hfh include an early history of coronary atherosclerosis , increased total cholesterol levels and the presence of tendon xanthomas , usually affecting the achilles tendons , the extensor tendons of the hand and elbow , and the patellar tendons [ 6 ]  . 
ultrasonography ( us ) in particular is a reliable method for measuring the tendon thickness and identifying possible lipid deposition , both in the form of xanthomas , which appear as focal or confluent hypoechoic areas , and as a diffuse and heterogeneous tendon thickening with or without calcification , even when the physical examination is completely normal [ 7 , 8 ]  . recently , a new sonographic technique has been introduced real - time spatial compound sonography ( cs ) which relies on the possibility of electronically steering the us beam generated by the array of transducer elements in order to obtain three to nine , in part overlapping , scans of an object from multiple view angles [ 9 ]  . 
application of this technique to the sonographic study of various organs and systems , especially the musculoskeletal system , has led to improved image quality compared with conventional sonography as a result of a reduction in background noise , spurious echoes and other acoustic artefacts , such as anisotropy [ 1013 ]  . the primary aim of this study was to evaluate the incidence and sonographic patterns of achilles tendon xanthomas ( atx ) in patients with hfh and clinically normal tendons studied with high - resolution ultrasound ( hrus )  . the secondary aim was to assess the contribution of cs technology in terms of image quality . materials and methods patients after obtaining approval by our institutions ethics committee , over a period of 2 years , we recruited 40 consecutive patients with genetically proven hfh . 
all patients ( 19 men and 21 women , age range 1174 years , mean age 46.9 years ) underwent hrus and cs of both achilles tendons after providing their written informed consent . 
lif pu presentarsi in forma eterozigote ( ife ) , con unincidenza di 1 / 500 individui nella popolazione generale o in forma omozigote , con unincidenza pari a 1 / 1000000 [ 4 ]  . 
i criteri clinici usualmente presi in considerazione nella diagnosi di ife sono costituiti , soprattutto , da una storia di precoce aterosclerosi coronarica , dallaumento della concentrazione di colesterolo totale e dalla presenza di xantomi tendinei , questi ultimi pi frequentemente apprezzabili in corrispondenza dei tendini dachille , dei tendini estensori delle mani , del gomito e dei tendini patellari [ 6 ]  . 
in considerazione delle sue caratteristiche anatomo - strutturali ( sede , dimensioni ) , il tendine dachille pu essere facilmente esaminato e , in particolare , lecografia risulta un metodo affidabile per misurare il suo spessore ed individuare leventuale accumulo di lipidi , sia sotto forma di veri e propri xantomi , evidenziabili come aree ipoecogene focali o confluenti , sia come diffuso e disomogeneo ispessimento tendineo , accompagnato o meno dalla presenza di calcificazioni , anche quando lesame obiettivo locale sia del tutto negativo [ 7 , 8 ]  . recentemente , stata introdotta una nuova tecnica ecografica real time spatial compound sonography ( cs ) la quale sfrutta la possibilit di angolare elettronicamente il fascio ultrasonoro generato dalla linea di elementi trasduttori al fine di effettuare diverse ( da tre a nove ) scansioni , in parte sovrapposte , di un oggetto da diversi angoli di vista [ 9 ]  . 
lapplicazione di tale tecnica allo studio ecografico di vari organi ed apparati , con particolare riferimento al sistema muscolo - scheletrico , ha mostrato una migliore qualit dellimmagine rispetto allecografia convenzionale , principalmente grazie alla riduzione del rumore di fondo , degli echi spuri e di altri artefatti acustici , quali lanisotropia [ 1013 ]  . lobiettivo principale di questo lavoro stato quello di valutare lincidenza e gli aspetti ecografici degli xantomi del tendine dachille in pazienti con ife ed esame clinico dei tendini negativo , studiati con ecografia ad elevata risoluzione ( hrus )  . 
quale obiettivo secondario , stato valutato leventuale apporto fornito dalla tecnologia cs in termini di qualit dellimmagine . materiale e metodi pazienti durante un periodo di due anni , ottenuta lapprovazione da parte del comitato etico , 40 pazienti consecutivi ( 19 uomini e 21 donne , et 1174 anni , media 46 , 9 anni ) affetti da ife geneticamente accertata , sono stati sottoposti , previa acquisizione del consenso informato in forma scritta , ad ecografia ad alta risoluzione ( hrus ) e cs di entrambi i tendini t.v. 
once set , the technical parameters remained unchanged throughout the sonographic examination . the achilles tendons were scanned axially and longitudinally with the patients in the prone position and holding their ankles flexed over the edge of the couch with the tendon at maximum extension to facilitate contact between the probe and the tendon [ 7 ]  . 
for tendons that did not appear thickened , measurements were made 2 - cm cranially from the distal insertion . each study consisted of the acquisition of four images , two axial and two longitudinal , obtained with conventional us and cs techniques , respectively . 
overall examination time was 57 min . on - site analysis the morphological criteria used for diagnosing xanthoma were : ( 1 ) tendon thickening intended as maximum anteroposterior diameter greater than 7.1 mm , a value by at least two standard deviations ( sd ) higher than the normal sonographic values ( 5.70.7 mm ) , and ( 2 ) evidence of unior multifocal hypoechoic lesions , the largest diameter of which was also measured . 
structural abnormalities were classified as ( 1 ) no lesions , ( 2 ) unior multifocal hypoechoic lesions and ( 3 ) diffuse alterations [ 4 , 6 , 15 , 16 ]  . 
 off - site analysis the digital images stored on the workstation were retrospectively reviewed by two expert radiologists not involved in the sonographic examinations and blinded to the patients clinical data and examination technique . 
coherent wave interface or speckle , caused by excessive background noise , which gives a grainy appearance to an otherwise homogeneous region , reducing image contrast and spatial resolution 3 . 
lateral acoustic shadows , the degree of evidence of normal fibril structures and possible lesions ( visibility and sharpness in relation to the adjacent fibril structures ) [ 9 , 12 ]  . the reviewers consensually expressed their judgement on dachille . 
i tendini dachille sono stati esaminati mediante scansioni sui piani assiale e longitudinale , col paziente in posizione prona e caviglie flesse al di fuori del lettino da esame con il tendine in massima estensione per facilitare il contatto tra la sonda ed il tendine [ 7 ]  . 
ogni studio stato completato con lacquisizione di quattro immagini , due sul piano assiale e due su quello longitudinale , ottenute rispettivamente con metodica ecografica convenzionale e con tecnica compound . 
tutte le immagini sono state archiviate sul disco rigido in dotazione allunit ecografica e poi inviate , sotto forma di dati grezzi , ad un personal computer ( pc ) collegato allecografo attraverso una connessione in standard ethernet . 
definitely absent in particular , reduction of anisotropy was defined as the correct visualisation without interruptions of the tendon fibres , whereas reduction of the other artefacts was described in terms of reduced speckle and clutter . 
statistical analysis was done using the t test for paired samples , with statistical significance set at p < 0.05. results sixty - six out of 80 tendons showed no significant changes in size ( anteroposterior diameter : 4.26.9 mm , mean : 5.5 mm ) or structure . 
fourteen out of 80 ( 17.5% ) tendons in seven ( 6.2% ) patients ( four men , three women , age : 2457 years , mean : 47.3 years ) showed dimensional and / or morphostructural alterations ( table 1 )  . 
nine tendons in five patients ( two men , three women , age : 4357 years , mean : 50.8 years ) showed 12 focal hypoechoic areas classified as xanthomas ( largest diameter : 4.19.8 mm , mean : 7.1 mm ) , five of which were located on the left and seven on the right . 
the number of alterations identified by hrus and cs was equal . the degree of evidence of structural abnormalities in the 80 achilles tendons studied with hrus and cs is shown in table 2 . 
atx are extremely rare in the other forms of hyperlipidaemia , such as type iii hyperlipoproteinaemia , cerebrotendinous xanthomatosis , apolipoprotein b hyperproducnate da due esperti radiologi , non coinvolti negli esami ecografici e tenuti alloscuro dei dati clinico - anamnestici della tecnica utilizzata per ogni esame . 
le immagini sono state presentate in ordine casuale ed stata nascosta ogni informazione riguardo ai parametri tecnici e / o ai dati anagrafici . agli esaminatori stato chiesto di valutare , per ciascuna immagine , la qualit complessiva in relazione alla presenza o meno di artefatti , quali : 1 . 
coherent wave interface o speckle , riconducibile ad un eccessivo rumore di fondo che conferisce un aspetto granulare ad una regione altrimenti omogenea , riducendo il contrasto e la risoluzione spaziale dellimmagine ; 3 . 
le ombre acustiche laterali e altri artefatti acustici , nonch al grado di evidenza delle normali strutture fibrillari che di eventuali lesioni ( visibilit e chiarezza rispetto alle strutture fibrillari tendinee adiacenti ) [ 9 , 12 ]  . 
 i due radiologi hanno espresso , in consenso , la loro valutazione graduandola su una scala di cinque livelli ed il grado di evidenza delle anomalie strutturali stato conseguentemente distinto in : 1 . 
 in particolare , la riduzione dellanisotropia stata definita come la corretta rappresentazione , senza soluzione di continuit , delle fibre tendinee , mentre la riduzione degli altri artefatti stata descritta in termini , soprattutto , di riduzione dello speckle e del clutter . 
lanalisi statistica stata effettuata utilizzando il test t di student per campione doppio con livello di significativit statistica fissato a p < 0 , 05 . risultati sessantasei / 80 tendini non hanno presentato , allindagine ecografica , significative alterazioni dimensionali ( diametro antero - posteriore : 4 , 26 , 9 mm , media : 5 , 5 mm ) n morfostrutturali . 
quattordici / 80 ( 17 , 5% ) tendini in 7 ( 6 , 2% ) pazienti ( quattro maschi , tre femmine , et : 2457 anni , media 47 , 3 anni ) hanno mostrato alterazioni dimensionali e / o morfostrutturali ( tabella 1 )  . 
atx are accompanied by an enlargement of the tendon caused not only by fat deposition but also by oedema and inflammation , which may lead to achillodynia , as reported at least once in their lifetime by 30% of patients with hfh , and , rarely , to tendon rupture [ 16 , 18 ]  . 
the recent discovery of effective pharmacological treatments has placed much emphasis on the early diagnosis of hfh , above all to prevent atherosclerosis , which has a particularly poor prognosis when the coronaries are involved due to the increased risk of fatal ischaemic events [ 2 , 3 , 19 ]  . 
xanthomas , however , which are often the first clinical sign of hfh and usually manifest in the fourth decade of life , are often missed on clinical examination , whereas they are perfectly identifiable on us . 
in 9 / 80 tendini di 5 pazienti ( due maschi , tre femmine ; et : 4357 anni , media : 50 , 8 anni ) sono state identificate 12 aree focali ipoecogene classificate come xantomi ( diametro maggiore : 4 , 19 , 8 mm , media : 7 , 1 mm ) , cinque delle quali localizzate a sinistra e sette a destra . 
di contro , gli xantomi del tendine dachille sono estremamente rari nelle altre forme di iperlipidemia quali liperlipoproteinemia di tipo iii , la xantomatosi cerebrotendinea , liperproduzione di apolipoproteina b e liper - b - sitosterolemia [ 6 , 8 , 17 ] .gli xantomi del tendine dachille sono accompagnati da incremento dimensionale del tendine , causato non solo dal deposito di lipidi , ma anche da fenomeni di edema e flogosi , che possono condurre ad achillodinia , riferita almeno una volta nella vita dal 30% dei pazienti con ife , e , seppur raramente , a rottura tendinea [ 16 , 18 ]  . 
recentemente , la scoperta di terapie farmacologiche efficaci ha posto grande enfasi sulla diagnosi precoce di ife , soprattutto al fine di prevenire i fenomeni aterosclerotici , particolarmente infausti quando a localizzazione coronarica , a causa dellaumentato rischio di eventi ischemici mortali [ 2 , 3 , 19 ]  . 
tuttavia , gli xantomi , usualmente presenti a partire dalla quarta decade di vita e pur costituendo spesso la prima manifestazione clinica di ife , non di rado risultano misconosciuti allesame clinico , mentre risultano fig . 
infatti la radiologia convenzionale , storicamente impiegata come prima tecnica di studio , consente , nella proiezione laterale e con adeguati parametri di esposizione , unicamente la determinazione dello spessore tendineo e lindividuazione di eventuali calcificazioni del tendine , rimanendo pur sempre una tecnica proiettiva ed esponendo il paziente a radiazioni ionizzanti [ 20 ]  . 
questultimo limite condiviso anche dalla tomografia computerizzata ( tc ) , la quale , pur fornendo misurazioni accurate delle dimensioni del tendine achilleo grazie allintrinseco contrasto esistente tra il tendine stesso ed il circostante tessuto adiposo , non in grado di misurare valori di densit che differiscano sostanzialmente in pazienti normo o ipercolesterolemici [ 16 ]  . la risonanza magnetica , infine , non in grado di evidenziare , al di l delle alterazioni morfodimensionali e un aspecifico aspetto puntato , vere e proprie lesioni ascrivibili con certezza a xantomi tendinei [ 2022 ]  . in accordo ai dati di letteratura , la nostra esperienza conferma losservazione che lecografia , in una piccola ma non trascurabile percentuale di pazienti con tendine dachille valutato come del tutto normale allesame clinico , in grado di evidenziare significative alterazioni tendinee , quali ispessimento , calcificazioni o ancora la presenza di veri e propri xantomi [ 7 , 8 , 15 , 19 ]  . 
la minore percentuale di pazienti con ife e lesioni xantomatose achillee riscontrata nel nostro studio ( 6 , 2% ) rispetto a quanto riportato in letteratura ( 29%33 , 1% ) da mettere in relazione , almeno in parte , al gruppo di pazienti selezionato , che non presentava apprezzabili alterazioni tendinee allesame clinico [ 6 , 19 , 23 ]  . 
inoltre , la popolazione numericamente limitata e la tipologia del nostro studio non consentono di confermare i dati epidemiologici acquisiti su campioni di pi vaste proporzioni , che indicano come i soggetti con ife e con xantomi del tendine dachille tendano ad essere di sesso maschile , pi anziani e a presentare livelli di colesterolo totale e ldl pi elevati rispetto ai pazienti senza xantomi [ 19 ]  . la cs una tecnica ultrasonografica la cui applicazione ha condotto ad un miglioramento della definizione dellimmagine ecografica , che alcuni studi hanno riportato essere utile anche ai fini diagnostici , ad esempio in ambito muscoloscheletrico ed in particolare nel distretto anatomico della cuffia dei rotatori [ 9 , 12 , 13 , 24 ]  . 
questa tecnica , diversamente dallecografia b - mode convenzionale nella quale ogni immagine ottenuta da un solo angolo di insonazione , effettuando la media dei segnali ricevuti , in grado di ridurre gli artefatti , migliorando sensibilmente il rapporto segnale rumore e la risoluzione dellimfig 3 left achilles tendon in a 53 - year - old man with heterozygous familial hypercholesterolemia ( hfh )  . 
scansione sagittale che dimostra un tendine diffusamente ispessito , disomogeneo , con perdita della normale ecostruttura fibrillare ( frecce piccole ) e grossolane calcificazioni nel suo contesto ( freccia grande ) ( caso 7 della tabella 1 )  . ing modality for the assessment of atx [ 4 , 8 , 14 , 15 ]  . 
traditionally the first - line imaging technique , conventional radiography in the lateral projection and with adequate exposure settings allows determination of tendon thickness and detection of calcification only but remains a projective technique that exposes the patient to ionising radiation [ 20 ]  . 
this last limitation is shared by computed tomography ( ct ) which , while providing accurate measurement of tendon size thanks to the intrinsic contrast between achilles tendon and the surrounding fat , is unable to measure density values that differ substantially in patients with normal and elevated cholesterol levels [ 16 ]  . 
magnetic resonance imaging ( mri ) is only able to detect changes in shape and size and a nonspecific pointed appearance but cannot demonstrate lesions unequivocally referable to tendon xanthomas [ 2022 ]  . in agreement with the literature , our experience confirms that in a small but nonnegligible series of patients with clinically normal achilles tendon , us can demonstrate significant tendon alterations , such as thickening , calcification or the presence of xanthomas [ 7 , 8 , 15 , 19 ]  . 
the smaller proportion of patients with hfh and atx seen in our study ( 6.2% ) compared with previous reports ( 29%33.1% ) is in part related to our study sample not having appreciable tendon abnormalities on clinical examination [ 6 , 19 , 23 ]  . 
in addition , the limited number of patients included and the study design did not allow us to confirm or refute the epidemiological data derived from larger series , according to which subjects with hfh and atx tend to be older males with higher total and ldl cholesterol levels than those without tendon xanthomas [ 19 ]  . 
 cs is an ultrasonographic technique that has improved the definition of sonographic images and that has been reported to have diagnostic value , for example , in musculoskeletal imaging and in particular in rotator cuff studies t.v. 
4a high - resolution ultrasonography ( hrus ) sagittal image of the right achilles tendon in a 31 - year - old woman with heterozygous familial hypercholesterolemia ( hfh ) shows a normal - sized tendon ( small arrows ) ; speckle ( grainy appearance ) is clearly appreciable . 
4a immagine longitudinale del tendine di achille destro ( frecce piccole ) in una donna di 31 anni affetta da ife ottenuta mediante ecografia in scala di grigi convenzionale : notare le dimensioni normali del tendine e laspetto complessivamente granuloso dellimmagine . 
b real - time spatial compound sonography del medesimo tendine che evidenzia una migliore visibilit del nodulo stesso con riduzione della granulosit dellimmagine , permettendo cos una migliore definizione della fine struttura fibrillare del tendine . [ 9 , 12 , 13 , 24 ]  . 
cs in unlike conventional b - mode imaging in which each image is obtained from a single insonation angle ; by averaging multiple signals , cs reduces artefacts , substantially improving the signal - to - noise ratio and image resolution [ 13 ]  . 
only by analysing the tendon fibres perpendicularly is it , in fact , possible to discriminate with any certainty areas of echostructural alteration from the normal fibril network , consisting of the interfaces between the connective tissue septa of the endomysium and the parallel collagen fibre bundles [ 14 , 15 ]  . 
solo analizzando perpendicolarmente le fibre del tendine possibile , infatti , discriminare con sicurezza eventuali aree di alterazione ecostrutturale rispetto al normale disegno fibrillare , costituito dalle interfacce tra i setti connettivali dellendomisio ed i fasci di fibre collagene a decorso parallelo [ 14 , 15 ]  . in particolare , la presenza di aree ipoecogene focali o un aspetto diffusamente disomogeneo vengono considerati , in pazienti con ife ma senza storia clinica di traumi o tendinite , come altamente suggestivi di xantomi , anche in assenza di conferma istologica [ 4 ]  . 
however , although us is reliable for detecting focal hypoechoic areas on a generally hyperechoic tendon and for determining the extent of tendon thickening , it appears to be subject to a greater error margin in the evaluation of echostructural heterogeneity [ 6 ]  . 
furthermore , as already suggested for conventional us , cs could be used to monitor regression of xanthomas and / or the reduction in tendon size in patients receiving therapy [ 27 ]  . there are some limitations to our study . 
in particular , the assessment of image quality was conducted in a subjective fashion , and a double - blind review of cases would have allowed us to determine interand intraobserver variability . cremento dimensionale del tendine , la valutazione della disomogeneit ecostrutturale appare soggetta ad un pi ampio margine di errore [ 6 ]  . 
daltra parte , nella serie presa in esame , tale migliore qualit dellimmagine , per quanto utile per una maggiore confidenza diagnostica , non si tradotta in un pi elevato tasso di identificazione di xantomi achillei . 
inoltre , lecografia cs potrebbe essere utilizzata , come gi suggerito per lecografia convenzionale , per monitorare la regressione degli xantomi e / o la riduzione delle dimensioni del tendine in pazienti sottoposti a terapia [ 27 ]  . il nostro studio presenta dei limiti . 
in particolare , la valutazione della qualit dellimmagine stata condotta in maniera soggettiva e una revisione dei casi in doppio cieco avrebbe consentito il calcolo della variabilit intraed interosservatore . conclusione conclusion in conclusion , cs sonography proved useful in the evaluation of the achilles tendon in patients with hfh and normal clinical examination , as it provided early evidence of xanthomas , thereby supplying the clinician with useful information for patient management and optimisation of therapy . 
civeira f , international panel on radiol med ( 2007 ) 112 : 620 doi 10.1007 / s11547 - 007 - 0167 - z dallanatomia allimmagine silvia magnaldi luciana travan 2nd edn . 
poletto editore isbn 88 - 86786 - 94 - 8 published online : 11 june 2007 as with the first edition , and , indeed , even more so , this revised edition of dallanatomia allimmaginesucceeds in completely fulfilling its objectives . with its brilliant layout , excellent drawings and clear radiological images , the book presents radiological anatomy in a straightforward and intuitive manner . 
also excellent are the captions and cross - references in the illustrations that allow quick and easy recognition of the anatomical structures discussed in the text . anche e ancor pi nella nuova edizione il libro dallanatomia allimmagine risponde in modo completo ai suoi obiettivi . con la sua brillante impostazione editoriale , gli ottimi disegni e la chiara iconografia radiologica , il libro propone lanatomia radiologica in modo semplice e intuitivo . 
al tempo stesso il libro molto completo in tutte le sue parti . vengono illustrati ad uno ad uno gli apparati , a partire dal muscolo - scheletrico , proseguendo con il cardio - vascolare , il linfatico , il digerente , il respiratorio , luro - genitale , lendocrino , per concludere con il sistema nervoso . la trattazione prevede un testo molto ben articolato che guida liconografia e le tabelle . 
giovagnoni4 1dipartimento diagnostica per immagini , ausl 3 umbria , ospedale foligno , perugia , italy 2dipartimento diagnostica per immagini , ausl 2 umbria , ospedale assisi , perugia , italy 3sc cardiochirurgia , ospedale s . 
crusco , via antica vena 18 , i - 06087 perugia , italy , tel . : + 39 - 075 - 393044 , fax : + 39 - 075 - 5783488 , e - mail : fcrusco@sirm.org received : 17 may 2006 / accepted : 3 october 2006 / published online : 11 june 2007 abstract purpose . 
sixteen - slice mdct scanners enable accurate analysis of cabg status and are a useful noninvasive diagnostic tool for midterm clinical follow - up of patients who have undergone cabg involving the use of ra . key words radial artery coronary artery bypass graft multidetector ct riassunto obiettivo . 
cinquantuno pazienti , per un totale di 50 bypass con ami , 55 con sv e 51 con ar , sono stati sottoposti ad esame tcmd a 16 canali con intervallo temporale dallintervento chirurgico pari a 324 mesi . 
il giudizio di perviet stato valutato come grado 0 ( perviet completa ) , grado 1 ( stenosi focale , > 70% ) e grado 2 ( ostruzione del graft )  . 
la perviet dei bypass con ar stata influenzata dai diversi territori dellanastomosi distale con valori del 79 , 4% nel territorio distale della circonflessa ( acs ) , del 72 , 7% in quello della discendente anteriore ( ada ) e del 50% in quello della coronaria destra ; nel caso dei bypass con ar il tasso globale di ostruzione risultato del 20 , 0% nel caso dei graft semplici , del 18 , 2% nel caso dei graft sequenziali e del 20 , 0% nel caso dei graft compositi . 
la tcmd a 16 canali , consentendo unanalisi accurata dello stato di perviet dei graft , deve essere considerata una metodica diagnostica non - invasiva particolarmente utile nel follow - up a medio termine dei pazienti sottoposti a bypass aortocoronarico comprendente lutilizzazione dellarteria radiale . parole chiave arteria radiale intervento di bypass dellarteria coronarica tc multidetettore f . 
thus , follow - up examinations are essential . conventional coronary angiography is still considered the gold standard for the evaluation of native coronary arteries and cabg , but recent studies have shown that contrast - enhanced coronary computed tomography angiography ( cta ) , a noninvasive and less expensive diagnostic tool , enables accurate assessment of both coronary arteries [ in terms of high negative predictive value ( npv ) ] and graft patency [ 29 ]  . moreover , multidetector - row ct ( mdct ) appears to be a useful technique able to detect postoperative complications in patients presenting with chest pain resembling recurrent angina secondary to graft occlusion [ 10 ]  . 
 among cabg strategies , left internal mammary artery ( lima ) and saphenous vein ( sv ) grafts have been extensively used with good clinical results , whereas radial artery ( ra ) or gastroepiploic artery grafts are a second alternative , as are aortocoronary or composite conduits [ 1113 ]  . 
midand long - term patency rates of these grafts have been evaluated only by angiographic studies in symptomatic patients , and the findings , especially those related to ra grafts , are inconsistent and nonconclusive [ 1418 ]  . 
in asymptomatic patients , radionuclide myocardial perfusion imaging ( mpi ) seems to be a valid method for risk stratification , prognosis and determination of disease progression [ 19 , 20 ]  . to our knowledge , there are no recent midto long - term follow - up studies on cabg assessment focusing on ra patency in asymptomatic patients , performed with mdct coronary angiography . 
the purpose of our observational study was to evaluate the 3 - year outcome of patients who have undergone cabg involving the use of ra grafts in comparison with lima and sv grafts by using 16 - mdct coronary angiography . materials and methods patient population over an 8 - month period , between april 2005 and october 2005 , 51 consecutive patients with at least triple - cabgs involving ra usage were enrolled in our observational study . all of them were referred to us by a single hospital cardiothoracic department that acted as a recruitment and data control centre . 
all asymptomatic patients ( 51 ) who had undergone a routine diagnostic work - up [ including exercise electrocardiographic ( ecg ) testing ] were eligible for the ct study . 
patients with allergies to iodinated contrast media , renal ( serum creatinine level > 2.00 mg / dl ) , respiratory or cardiac failure [ new york heart association ( nyha ) iv ] , cardiac arrhythuna delle procedure pi frequentemente ed estesamente eseguita in campo cardiochirurgico la rivascolarizzazione miocardica mediante bypass aortocoronarico ( cabg ) , trattamento di scelta nei pazienti sintomatici con malattia coronarica . 
la prognosi post - chirurgica strettamente dipendente dalla perviet dei bypass , e poich entro i primi 10 anni dallintervento i bypass possono andare incontro a restenosi , con una probabilit che aumenta al passare del tempo , necessario un follow - up strumentale [ 1 ]  . langiografia coronarografica convenzionale ( ac ) considerata il gold standard diagnostico per la valutazione delle coronarie native e dei bypass , tuttavia , recentemente , alcuni studi hanno dimostrato il valore dellangio - tc multidetettore ( tcmd ) , metodica meno costosa e non - invasiva , che consente unanalisi accurata sia delle coronarie native ( specificatamente nei termini di un elevato valore predittivo negativo ) sia dello stato di perviet dei graft [ 29 ]  . 
la tcmd inoltre metodica utile nella osservazione di eventuali complicanze postoperatorie che diventano palesi clinicamente con dolore toracico tale da mimare unangina ricorrente da ostruzione del graft [ 10 ]  . nellambito delle diverse opzioni chirurgiche , i bypass pi comunemente utilizzati , associati ai risultati clinici migliori , sono quelli arteriosi con mammaria interna ( ami ) e quelli venosi con vena safena ( vs ) , mentre quelli con arteria radiale ( ar ) e gastroepiploica sono considerati condotti aortocoronarici semplici o compositi di seconda scelta [ 1113 ]  . 
il tasso di perviet a medio e lungo termine dei graft stato valutato solamente mediante studi angiografici in pazienti sintomatici con risultati , soprattutto per quanto riguarda i condotti con ar , spesso discordanti e non conclusivi [ 1418 ]  . nel sottogruppo di pazienti asintomatici , la metodica di scelta per la stratificazione dei rischi , la determinazione della prognosi e la stima della progressione di malattia , considerata la miocardioscintigrafia perfusionale [ 19 , 20 ]  . per quanto ci dato sapere non esistono in letteratura studi di follow - up a medio - lungo termine in pazienti asintomatici per la stima di perviet dei bypass con ar eseguiti con tecnica tcmd . 
obiettivo del nostro studio osservazionale perci quello di valutare , utilizzando langio - tcmd eseguita con apparecchiatura a 16 canali , lo stato di perviet a 3 anni dei bypass con ar in comparazione con quelli eseguiti con ami e sv . materiali e metodi popolazione di studio sono stati arruolati 51 pazienti , consecutivamente sottoposti , tra aprile e ottobre del 2005 , ad esame tcmd per valutare gli esiti di un intervento di triplice bypass aortocoronarico comprendente lar . 
thirty - five of the 51 ( 68.6% ) ra were free grafts ( aorta single anastomoses ) , 11 ( 21.5% ) were sequential grafts ( aorta multiple anastomoses ) and 5 ( 9.8% ) were composite grafts with the sv . 
of the 51 ra segments , 11 ( 21.5% ) were grafted onto the left anterior descending artery ( lad ) , 27 ( 52.9% ) onto the left circumflex coronary artery ( lcx ) , 6 ( 11.7% ) onto the right coronary artery ( rca ) and 7 ( 13.7% ) sequentially onto the lad - lcx territory . 
the study was approved by the local ethics committee , and informed consent was obtained from all patients . ( 51 ) in follow - up clinico - diagnostico precedentemente sottoposti ad ecg da stress . 
trentacinque / 51 segmenti ( 68 , 6% ) di bypass con ar erano condotti semplici ( aorta - aranastomosi coronarica singola ) , 11 / 51 ( 21 , 5% ) bypass di tipo sequenziale ( aortaar - anastomosi coronarica multipla ) , infine 5 ( 9 , 8% ) segmenti erano condotti compositi con origine da vs . 
intervallo di 324 mesi tra procedura chirurgica ed esame tcmd 36 ( range 5078 , et media 64 ) 15 ( range 5569 , et media 62 ) campione di studio sesso maschi femmine intevallo temporale tra procedura 324 mesi chirurgica ed esame tcmd segmenti esaminati numero numero totale dei segmenti graft venosi graft arteriosi lima segmenti con ra valore semplice ( aorta - anatomosi singola ) sequenziale ( aorta - nastomosi multiple ) composito ( sv - anastomosi singola ) distribuzione anastomosi distale sequenziale lad - lcx tipo di graft sv , vena safena ; lima , arteria mammaria sinistra ; ra , arteria radiale ; lad , discendente anteriore sinistro ; lcx , arteria coronarica circonflessa sinistra ; rca , arteria coronarica destra ct scanning protocol ct scans were obtained by using a 16 - mdct scanner ( philips brilliance 16 , philips medical systems , best , the netherlands )  . 
mean standard deviation ( sd ) interval between cardiac surgery and ct examination was 324 months . after a scout image with the patient in a supine position , scan coverage was selected from the carina to the apex of the heart in the cephalic to caudal direction to include the maximum extent of the grafts . 
in order to minimise heart rate , all patients received oral - blockers ( metoprolol 100 mg ) 23 days before the examination ; the heart rate range was 5415.3 bpafter a precontrast scan to assess the calcium burden and the course of target surgical clips , contrast - enhanced mdct was performed by administering 110 ml of low osmolar nonionic high - concentration contrast medium ( iomeprol , iomeron 400 , bracco , milan , italy ) via a dual - head anastomizzati nel territorio dellarteria discendente anteriore ( ada ) , 27 ( 52 , 9% ) in quello dellarteria circonflessa sinistra ( acs ) , 6 ( 11 , 7% ) in quello della coronaria destra , 7 ( 13 , 7% ) erano anastomizzati sequenzialmente su territorio dellada in sede prossimale e su quello della acs . 
lo studio stato approvato dal comitato etico locale previo ottenimento di un consenso informato da parte dei pazienti arruolati . protocollo di imaging la scansione stata eseguita con scanner tcmd a 16 canali ( philips brilliance 16 , philips medical systems , best , olanda ) , con un intervallo medio tra intervento chirurgico ed effettuazione dellesame di 324 mesi . 
a partire da una scout view del paziente in posizione supina , il volume di studio stato esteso in senso cranio - caudale a comprendere la massima estensione dei bypass . 
to achieve optimal contrast enhancement , the scan delay was determined by using the bolus - tracking technique after positioning a region of interest ( roi ) in the ascending aorta . 
all scans were reconstructed by using retrospective gating ( 37.5%50%62.5%75%87.5% of the r - r interval ) , with 1 - mm - thick images reconstructed every 0.5 m the cardiac phase with the least motion was chosen for further evaluation . image processing and analysis the data sets obtained were reviewed on a dedicated workstation ( mx view ; philips medical systems , best , the netherlands ) , and image interpretation was based on evaluation of axial source , multiplanar reconstructions ( mpr ) , maximum - intensity projections and volume - rendering images ( vr )  . 
advanced software tools [ arterial tree , curved multiplanar reformation along the vessel centre line , vascular two - dimensional ( 2d ) or three - dimensional ( 3d ) mapping , virtual and angioscopy ] were used in single cases . 
in the absence of clear and conclusive ct parameters to define cabg patency , we used the following three - point scale to assess the grade of single graft patency . 
concordance between readers 1 and 2 for the detection of occlusion or significant conduit stenosis by mdct was calculated by the cohen frequenza cardiaca , in tutti i pazienti si proceduto ad una premedicazione farmacologica con - bloccante ( 100 mg di metoprololo per os a partire da 23 giorni prima delleffettuazione dellesame ) : nella nostra coorte di pazienti la frequenza cardiaca media riportata stata di 5415 , 3 bpdopo unacquisizione diretta senza mezzo di contrasto , utile per quantificare lentit delle calcificazioni aterosclerotiche ed il decorso delle clips chirurgiche , si proceduto allo studio contrastografico mediante somministrazione endovenosa , con iniettore automatico a doppia siringa ( stellant , medrad , pittsburgh , usa ) e agocannula 1820 gauge posizionata in vena antecubitale di braccio , di 110 ml di mdc iodato non ionico ipo - osmolare ad alta concentrazione ( iomeprol 400 mgi / ml , iomeron , bracco , italia ) , alla velocit di 4 ml / s , seguito da un bolo di 40 ml di soluzione salina alla stessa velocit . 
per ottimizzare il contrast enhancement , lo scan delay stato selezionato in base alla tecnica del bolus tracking dopo posizionamento di una roi in aorta ascendente e scelta di una soglia di 150 uh predefinita come limite per istruire il paziente ad inspirare e trattenere lapnea . 
lacquisizione stata effettuata con i seguenti parametri : configurazione detettori 160 , 75 , spessore effettivo di strato 1 mm , indice di ricostruzione 0 , 5 mm , periodo di rotazione del tubo radiogeno 420 ms , pitch 0 , 20 , 3 , mas 500 , kvp 120 , fov 150200 mm con matrice 512512 . 
le immagini sono state ricostruite con spessore di 1 mm e indice di ricostruzione di 0 , 5 mm , gating ecg retrospettivo e finestre temporali variabili pari a 32 , 5%50%62 , 5% - 75% - 87 , 5% dellintervallo r - r : la successiva valutazione stata eseguita sulla ricostruzione giudicata migliore . analisi delle immagini il dataset di immagini assiali native stato inviato ad una stazione di lavoro dedicata ( mx view ; philips medical systems , best , olanda ) , dove si proceduto allutilizzazione di ricostruzioni multiplanari ( mpr ) , curve ( cmpr ) , proiezioni di massima intensit ( mip ) e volume rendering tridimensionale ( 3d - vr )  . 
coronary artery bypass graft ( cabg ) patency at 16 - detector - row computed tomography angiography ( cta ) : in this 60 - year - old man , three - dimensional ( 3d ) colour volume - rendered ( vr ) images ( a ) and corresponding curved multiplanar reconstruction ( cmpr ) ( b ) show perfect patency of the radial artery ( ra ) graft anastomosed to the obtuse marginal branch of the left circumflex coronary artery ( lcx ) artery ( white thick arrow ) and left internal mammary artery ( lima ) graft anastomosed via the diagonal branch to the left anterior descending ( lad ) coronary artery ( white thin arrow )  . 
in questuomo di 60 anni sottoposto ad esame tcmd a 16 canali , le immagini 3d volume rendering ( a ) e le corrispondenti ricostruzioni multiplanari curve ( b ) , dimostrano la perviet completa del bypass con arteria radiale anastomizzato distalmente sul ramo marginale ottuso della circonflessa ( freccia bianca spessa ) e di quello con mammaria sinistra anastomizzato in modo sequenziale su ramo diagonale e sulla discendente anteriore ( freccia bianca sottile )  . 
in questo caso esemplificativo la perviet di grado 0 ben dimostrabile in base allopacizzazione completa dei bypass senza evidenza di stenosi critiche nel corpo degli stessi o in corrispondenza dei siti anastomotici prossimale e distale . - value according to the formula = io - ie / 1 - ie , where io is the observed concordance and ie the expected concordance . results best image quality of all segments was obtained at a reconstruction interval of 62.5% to 75% of the cardiac cycle . 
the diagnostic quality of the images of all of the 101 arterial and 55 venous segments , all of the proximal anastomoses and 153 / 156 ( 98% ) distal anastomoses examined was sufficient to make them suitable for analysis . 
out of the 156 bypass graft segments examined , 131 ( 84.0% ) were classified as patent , 20 ( 12.8% ) as occluded and 5 ( 3.2% ) as significantly stenotic . 
among patent segments ( grade 0 ) , complete opacification with no critical stenosis was noted in 122 segments ( 78.2% ) , whereas diffuse narrowing was reported in 11 segments , which were all arterial . 
ai fini della valutazione statistica , in accordo a quanto riportato dal trial multicentrico raps ( radial artery patency study ) il diffuso restringimento del graft con ar , stato incluso in un giudizio di perviet di grado 1 [ 21 ]  . 
la concordanza interosservatore per la osservazione di stenosi del 70%99% e ostruzione del graft , stata calcolata utilizzando il statistico di cohen , in accordo alla formula = io - ie / 1 - ie dove il valore di io identifica la concordanza osservata e ie la concordanza attesa . risultati ai fini della visualizzazione dei segmenti lintervallo di ricostruzione r - r giudicato migliore per la valutazione degli stessi risultato essere quello compreso tra il 62 , 5% e il 75% del f . 
slab maximum intensity projection ( mip ) image ( a ) and corresponding volume - rendered ( vr ) image ( b ) in a 49 - year - old patient with radial artery ( ra ) bypass graft to left circumflex coronary artery ( lcx ) arterial territory demonstrate isolated surgical clips ( white thick arrow ) , appearing as bright structures without visible opacification between them at the expected site of the ra grathis finding is consistent with complete occlusion of the ra bypass granote the normal patency of the left internal mammary artery ( lima ) graft to left anterior descending ( lad ) artery and saphenous vein ( sv ) to the lcx artery . 
in questuomo di 49 anni con bypass con arteria radiale sul territorio della circonflessa , le immagini slab - mip ( a ) e le corrispondenti volume - rendering ( b ) , dimostrano la presenza delle sole clips chirurgiche ( freccia bianca spessa ) , senza visibile opacizzazione della colonna di mdc tra loro . 
la qualit diagnostica delle immagini stata giudicata idonea per la valutazione di perviet in tutti i segmenti arteriosi e venosi studiati ( rispettivamente 101 e 55 ) , in tutte le anastomosi prossimali e in 153 / 156 ( 98% ) anastomosi distali . 
su un totale di 156 segmenti esaminati , 131 ( 84 , 0% ) sono risultati pervi , 20 ( 12 , 8% ) ostruiti e 5 ( 3 , 2% ) significativamente stenotici . 
tra i segmenti giudicati pervi ( grado 0 ) , 122 ( 78 , 2% ) sono risultati completamente opacizzati in assenza di stenosi focali , mentre un restringimento diffuso del graft stato riportato in 11 segmenti , tutti arteriosi . in tabella 2 sono elencate le percentuali di ostruzione dei diversi tipi di segmenti visualizzati nellintera coorte di pazienti . 
dalla comparazione dei risultati ottenuti nei diversi gruppi , mediante applicazione del test di fischer , si evince come la percentuale di ostruzione riportata per i graft con ar sia significativamente maggiore ( p < 0 , 001 ) rispetto a quella riportata per i graft con ami e vs . 
il tasso di perviet migliore risultato essere quello per i bypass con ami , seguito da quello per i bypass con vs e infine da quello per i bypass con ar . 
la percentuale di perviet riportata per i segmenti di vs stata dell83 , 6% , infine per i segmenti di ar si sono riscontrati i valori di perviet minori , pari al 74 , 5% . nella classe di segmenti con ar un restringimento diffuso ( string sign ) era presente in 7 / 51 casi ( 13 , 7% ) ; al contrario tale aspetto semeiologico non stato riscontrato in nessun segmento confezionato con vs o ami . 
nella stessa classe una stenosi focale , in sede anastomotica distale , si evidenziata in 3 / 51 segmenti ( 5 , 9% ) ; il territorio di distribuzione dellanastomosi distale associato alla migliore percentuale di perviet risultato , sempre nel caso dei bypass con ar , quello della acs ( 79 , 4% ) seguito da quello della ada ( 72 , 7% ) e infine da quello della coronaria destra ( 50% )  . in tabella 3 sono riportate specificatamente le percentuali di ostruzione dei bypass con ar in base al sottotipo di condotto utilizzato : 20 , 0% nel caso dei bypass semplici ( aorta - radiale - anastomosi coronarica singola ) , 18 , 2% e 20 , 0% nel sottogruppo di bypass compositi ( aorta - safena - radialeanastomosi coronarica singola )  . 
stante il limitato valore numerico del campione di studio , lanalisi condotta con test di fischer non ha dimostrato alcuna correlazione tra il tipo di graft utilizzato ed il territorio di distribuzione dello stesso ( test non significativo : p > 0 , 5 )  . 
il valore del statistico per la diagnosi di perviet e stenosi significativa del dei graft arteriosi e venosi , risultato di 0 , 86 . discussione la coronarografia considerata , ad oggi , grazie allelevata risoluzione spaziale ed alla possibilit intrinseca di effettuare trattamenti di interventistica percutanea dopo la fase diagnostica , il gold standard per la valutazione dello stato di perviet dei bypass aortocoronarici . 
in the ra group , 3 / 51 ( 5.9% ) segments showed significant focal stenosis at the distal anastomosis ; the specific coronary artery receiving the di rivascolarizzazione chirurgica complessa , non sempre possibile , con tale metodica , studiare correttamente lanatomia dei condotti [ 23 ]  . 
tra le metodiche non invasive utili ai fini della valutazione dei pazienti dopo interventi di rivascolarizzazione miocadica eseguita per via chirurgica o per via percutanea , figurano i test da sforzo ( stress - test ) eseguiti mediante elettrocardiografia , miocardioscintigrafia perfusionale o ecocardiografia . 
the - value for interobserver variation in the detection of patency and significant stenoses of arterial and venous conduits was 0.86. discussion conventional coronary angiography , thanks to its high spatial resolution and the possibility of simultaneous interventional procedures , is still the gold standard for the evaluation of cabg patency . 
with the recent improvements in spatial and temporal resolution , resulting in decreased motion - related artefacts , ecg - synchronised mdct has become an emerging and useful technique for noninvasive cardiac imaging . 
initial studies with 4 - detector - row ct scanners yielded promising assessments of the native coronary arteries and graft patency , reporting 93% sensitivity and 97.8% specificity in the detection of graft occlusion and 80% sensitivity and 96% specificity in the detection of significant graft stenosis [ 24 ]  . 
sixteen - detector - row ct scanners , thanks to faster gantry rotation , decreased slice thickness , better spatial resolution , reduced respiratory and cardiac motion artefacts and nearly isotropic voxel size , reliably depict cabgs with higher diagnostic accuracy : sensitivity is 96% , specificity 95% , positive predictive value ( ppv ) 81% and npv 99% [ 4 ]  . potential advantages of mdct over conventional coronary angiography in the postoperative evaluation of patients treated with cabg surgery include the opportunity to perform a noninvasive study that does not require hospitalisation and the possibility of detecting ancillary findings ( a case of pulmonary neoplasm in our series ) and early and late exprincipali : 1 presenza dei sintomi ischemici , 2 tempo trascorso dallintervento [ 19 ]  . 
lintroduzione delle recenti apparecchiature tcmd con gating cardiaco , grazie al miglioramento della risoluzione spaziale e temporale , con la conseguente riduzione degli artefatti da movimento cardiaco e respiratorio , ha reso disponibile una metodica di imaging cardiaco non invasivo estremamente utile . 
i primi studi di valutazione delle coronarie native e dello stato di perviet dei graft , effettuati con scanner a 4 canali , hanno riportato valori di sensibilit e specificit elevati , rispettivamente del 93% e del 97 , 8% nella dimostrazione di ostruzione del graft , dell80% e del 96% nella dimostrazione di stenosi emodinamicamente significativa [ 24 ]  . 
tuttavia , con suddetta metodica , il numero dei segmenti valutabili ai fini diagnostici , pari al 62%67% , non risult essere particolarmente elevato [ 2 , 24 ]  . 
lo sviluppo della tecnologia a 16 canali , grazie alla maggiore rapidit di rotazione del sistema tubo radiogeno - detettori ed ai ridotti spessori di strato , fattori risultanti in un netto miglioramento della risoluzione spaziale , e grazie ancora alla riduzione degli artefatti da movimento respiratorio e cardiaco ed alla possibilit di sfruttare voxel quasi - isotropici , ha consentito lo studio dei bypass con elevata accuratezza diagnostica , con valori di sensibilit del 96% , specificit del 95% , valore predittivo positivo dell81% e valore predittivo negativo del 99% [ 4 ]  . 
 i vantaggi della tcmd a 16 canali , rispetto alla ac , nella valutazione dei pazienti post - cabg , sono correlati principalmente alla possibilit di eseguire uno studio non invasivo che non richiede lospedalizzazione del paziente , ed alla capacit della stessa di evidenziare eventuali patologie incidentali ( un caso di embolia polmonare nella nostra serie di studio ) o patologie extravascolari , ad esordio precoce o tardivo nel postoperatorio , che si presentano clinicamente con dolore toracico e che possono mimare unangina ricorrente . 
in questa classe di pazienti la diagnosi differenziale del dolore toracico include il versamento pleurico , il versamento pericardico , lembolia polmonare e linfezione delle suture sternali [ 10 ]  . inoltre la tcmd fornisce una pianificazione pre - operatoria particolarmente utile nei casi in cui si prospetti un re - intervento di rivascolarizzazione chirurgica , in relazione alla sua comprovata superiorit nei confronti della radiografia del torace e della ac , nel definire la corretta anatomia topografica dei graft e delle strutture mediastiniche adiacenti [ 10 , 25 ]  . nella nostra serie di studio le scansioni tc sono state acquisite con successo , senza significative complicanze per i pazienti e con buona tollerabilit dellesame da parte di questi . sono stati considerati qualitativamente valutabili ai fini diagnostici , tutti i segmenti arteriosi e tutti quelli venosi , ad eccezione di tre casi di mancata visibilit delle anastomosi distali . 
in base alla nostra esperienza , le ricostruzioni 3dvr di rendering tridimensionale , grazie alla capacit di visione panoramica , risultano particolarmente utili nella definizione della complessa anatomia dei graft e dovrebbero essere utilizzate come guida iniziale , insieme allintegrazione fornita dallo studio delle immagini assiali native , per facilitare la successiva analisi di perviet vasale , meglio eseguibile , sia per quanto riguarda il decorso del graft sia per la valutaf . 
in addition , mdct is very useful in preoperative planning before repeat cabg surgery because of its superiority over chest radiographs and conventional coronary angiography in defining the position of patent grafts and vital mediastinal structures [ 10 , 25 ]  . in our series , ct scans were acquired successfully in all patients without any complications , and the exam was well tolerated by all patients . 
based on our experience , 3d vr images , thanks to their panoramic view , are very useful in the depiction of complex graft anatomy and are used as an initial tool , together with 2d axial images , to facilitate subsequent vessel interpretation . 
by contrast , thin - slice maximum intensity projection and multiplanar reconstruction images provide the best visualisation of the graft and anastomosis sites during follow - up . regarding ra , all of the proximal and 48 / 51 ( 94.1% ) of distal anastomoses were suitable for analysis . 
in the series by khan et al . , no difference in the assessment of distal anastomoses was found between 4and 16 - detector - row ct technology [ 23 ]  . 
to maximise visualisation of distal anastomoses , we reduced motion artefacts by using recommended r - r reconstruction intervals at 62.5%75% to evaluate cabg grafted to lad or lcx arterial territory and at 50% of the cardiac cycle to visualise cabg grafted onto the rca artery [ 26 ]  . 
we also resorted to shifting the reconstruction intervals whenever necessary . because of their marked tendency to develop atherosclerosis and intimal hyperplasia , sv grafts have reduced longterm patency compared with lima grafts , with a reported 10 - year patency rate of about 60% [ 1 , 11 , 12 , 27 , 28 ]  . 
this observation has induced surgeons to prefer using other arteries as an alternative to lima arterial grafts for cabg . ra has become the most popular of these conduits , thanks to its particular anatomic features , which offer the advantages of a relatively large diameter and thick muscular walls that facilitate the construction of anastomoses and to the introduction of recent improvements in graft harvesting techniques and drug therapy to prevent spasm [ 29 , 30 ]  . 
whereas the early angiographic patency rates of ra exceed 90% , approaching those of lima [ 31 , 32 ] and higher than those of sv , the results of three recent large midto long - term studies were inconsistent [ 14 , 16 , 17 ]  . 
by contrast , zacharias et al . , in 190 symptomatic patients with zione dei siti anastomotici , mediante tecniche mip e mpr . riguardo i bypass con ar , stato possibile valutare tutte le anastomosi prossimali e 48 / 51 ( 94 , 1% ) delle anastomosi distali . 
la visualizzazione del sito anastomotico distale rappresenta il principale problema inerente lo studio dei graft , a causa degli artefatti da indurimento del fascio e delleffetto volume parziale determinati dalle clips limitrofe . 
a tal proposito , khan , nel proprio studio , non ha riscontrato differenze statisticamente significative tra scanner tcmd a 4 e 16 canali nella valutazione di perviet dellanastomosi distale [ 23 ]  . 
i dati del nostro studio sono in linea rispetto a quanto riportato da schlosser e dewey [ 4 , 5 ] , riguardo la valutabilit dellanastomosi distale , variabile nelle loro serie tra il 74% ed il 99% . 
nella nostra serie abbiamo cercato di implementare e massimizzare la visualizzazione dellanastomosi distale , minimizzando consensualmente gli artefatti da movimento , ricorrendo nella scelta della finestra temporale ottimale , allintervallo r - r 62 , 5%75% del ciclo cardiaco nel caso dei bypass anastomizzati distalmente su territorio della ada e della acs , ed allintervallo r - r 50% nel caso dei condotti anastomizzati su territorio della coronaria destra [ 26 ]  . 
 a causa della maggiore suscettibilit nello sviluppo della degenerazione aterosclerotica e delliperplasia intimale , i bypass con vs sono associati , rispetto a quelli con ami , a percentuali di perviet , nel lungo periodo , pi basse , intorno al 60% a 10 anni dallintervento [ 1 , 11 , 12 , 27 , 28 ]  . 
questa considerazione fisiopatologica ha indirizzato i chirurghi a cercare un condotto arterioso , utilizzabile come bypass , alternativo alla ami , e a tal proposito lar divenuto il condotto pi comunemente utilizzato , grazie alle sue intrinseche propriet anatomiche ( diametro e spessore parietale muscolare relativamente ben rappresentati , tali da facilitare la costruzione delle anastomosi ) , ai miglioramenti recenti nella tecnica di isolamento del vaso e alla introduzione di terapie farmacologiche ad hoc per prevenire lo spasmo arterioso [ 29 , 30 ]  . 
mentre studi angiografici hanno dimostrato che il tasso di perviet per i bypass con ar , nel breve termine , risulta superiore al 90% , valore comparabile rispetto a quello riportato per lami e superiore rispetto a quello riportato per la vs [ 31 , 32 ] , tre recenti studi angiografici hanno invece fornito dati discordanti riguardo la perviet dello stesso graft nel periodo medio - lungo [ 14 , 16 , 17 ]  . 
nella serie riportata da khot su 398 graft con ar , in un totale di 310 pazienti sintomatici in follow - up angiografico a 565511 giorni dallintervento , stata riscontrata per i graft con ar una percentuale di perviet del 51 , 3% , di ostruzione del 33 , 7% , di stenosi severa del 15 , 1% , valori peggiori rispetto a quelli riscontrati per i graft con ami e con vs [ 14 ]  . 
al contrario , dallanalisi di perviet effettuata da zacharias su 242 graft con ar , utilizzati come seconda scelta a confronto con vs rispetto a bypass dominante ami - ada , in 190 pazienti sintomatici ( follow - up a 668518 giorni dallintervento ) , si evinto un tasso di ostruzione del 31 , 8% , minore di quello riportato per vs , pari al 36 , 7 [ 16 ]  . 
on 177 ra grafts reported a 4 - year ra patency rate of 89% and a 5 - year svg patency rate of 95% [ 17 ]  . our results , with a 74.5% ra patency rate , are consistent with those reported by khot et al  . 
our patients were not matched for ra versus sv ; in fact in our cohort , ra was generally used as the third conduit of choice in cabg strategy ( after dominant lima and sv ) , with the primary objective of providing adequate global vascularisation in the perioperative period . 
considered the string sign as a sign of occlusion , diffusely narrowed grafts were considered to be patent in our study in accordance with the radial artery patency study group [ 21 ]  . 
despite the possible stenosis , this arterial conduit is still capable of responding to increased myocardial oxygen demand , and the corresponding string sign seems to be an active process of negative vascular remodelling related to an adaptive response to low flow demand rather than a fixed spasthe considerations about vascular graft remodelling are supported by the evidence that ischaemia is uncommon in myocardial territories supplied by grafts with angiographic string sign and sometimes even in regions supplied by occluded arterial ra grafts , thanks to the establishment of collateral pathways . 
this consideration explains the absence of signs or symptoms of ischaemia in the vast majority of our patients with occluded ra [ 34 ]  . a limitation of our study is the lack of validation of cabg patency with the gold standard conventional coronary angiography . 
however , considering the relatively large vessel calibre , the relative independence of grafts from heart rate compared with native coronary arteries and the high diagnostic quality of state - of - art mdct scanners , we thought that correlation with this technique was not necessary . 
thus , our study focused on the reliability of 16 - mdct in evaluating midterm status of ra used as cabg . viet a 5 anni per graft con vs pari al 95% [ 17 ]  . i risultati del nostro studio , con un tasso di perviet del 74 , 5% , sono in linea rispetto a quanto riportato da khot e tatoulis con la precisazione che nella nostra coorte di pazienti i graft con ar sono stati utilizzati , non a confronto diretto con i graft con vs , ma , generalmente , come condotti di terza scelta dopo posizionamento di due graft dominanti , il primo con ami , il secondo con vs , con lo scopo di fornire un apporto di vascolarizzazione supplementare rispetto ai due graft dominanti nel periodo peri - operatorio . 
in base alla nostra esperienza il principale segno diretto di perviet vasale dei graft con ar rappresentato dalla dimostrazione della colonna di mdc centrata tra le clips chirurgiche , presenti sui due lati . 
al contrario la sola visibilit delle clips metalliche senza evidenziazione della colonna centrale di mdc stato considerato segno evidente di ostruzione completa del graft . nonostante nei propri studi zacharias e tatoulis abbiano considerato il restringimento diffuso del graft ( string - sign ) come un segno di ostruzione , nel nostro lavoro tale reperto , in accordo a quanto espresso dal radial artery patency study group [ 21 ] , stato considerato come segno di perviet . 
infatti i graft con ar si evidenziano spesso con laspetto di restringimento diffuso in relazione alla tendenza allo spasmo dovuta allelevato spessore parietale e alla vasoreattivit intrinseca del vaso nativo [ 33 ]  . 
nonostante la presunta stenosi il condotto arterioso risulta alloccorrenza in grado rifornire con un congruo apporto ematico le diverse richieste perfusionali del miocardio ; in tal senso lo string - sign , piuttosto che uno spasmo fisso , dovrebbe essere considerato come un processo adattativo di rimodellamento vascolare negativo in risposta alle esigenze di flusso periferico . 
le considerazioni sul rimodellamento vascolare sono supportate dallevidenza che levento ischemico risulta piuttosto raro nei territori di miocardio riforniti da graft con restringimento angiografico diffuso e , talvolta , grazie allinstaurarsi di circoli collaterali , anche da graft con ar completamente ostruiti . 
in tal modo pu essere spiegata , a nostro parere , la mancanza di segni e sintomi di ischemia nella maggior parte dei nostri pazienti con graft con ar ostruiti [ 34 ]  . la principale limitazione del nostro studio stata la mancanza di validazione dei dati di perviet dei graft ottenuti con tcmd con il gold standard diagnostico , la ac . 
tuttavia , considerato il calibro vasale relativamente ampio , la relativa indipendenza dei bypass dalla frequenza cardiaca rispetto alle coronarie native , lelevata qualit diagnostica degli scanner allo stato dellarte , abbiamo ritenuto non strettamente necessaria tale correlazione . 
 conclusion conclusione in conclusion , our study shows that , by enabling accurate analysis of cabg status , 16 - mdct scanners are useful noninvasive diagnostic tools for clinical routine midterm followup of patients who have undergone cabg involving the use of ra . 
krestin2 1dipartimento di radiologia e dipartimento cuore , azienda ospedaliero - universitaria di parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dibimel , sezione di scienze radiologiche , universit di palermo , italy correspondence to : f . 
cademartiri , viale rustici 2 , i - 43100 parma , italy , tel . : + 39 - 0521 - 961833 , e - mail : filippocademartiri@hotmail.com received : 20 february 2006 / accepted : 13 june 2006 / published online : 11 june 2007 abstract purpose . 
ninety - five patients ( 72 men and 23 women , mean age 588 years ) with previous percutaneous coronary intervention with stenting and suspected restenosis underwent 64 - ct ( sensation 64 , siemens )  . 
the scan parameters were : slices 322 , individual detector width 0.6 mm , rotation time 0.33 s , feed 3.84 mm / rotation , 120 kv , 900 mas . 
after the intravenous administration of iodinated contrast material ( iomeprol 400 mgi / ml , iomeron , bracco ) and a bolus chaser ( 40 ml of saline ) , the scan was completed in < 12 s . 
all coronary segments with a stent were assessed on 64 - ct by two observers in consensus and judged as : patent , with intimal hyperplasia ( lumen reduction of < 50% ) , with in - stent restenosis ( 50% ) , or with in - stent occlusion ( 100% )  . 
we found that 64 - ct has a high diagnostic accuracy for the detection of in - stent restenosis in a selected patient population . key words coronary angiography multislice computed tomography 64 - slice ct coronary stents riassunto obiettivo . 
in 95 pazienti ( 72 maschi e 23 femmine , et media 588 anni ) precedentemente sottoposti a posizionamento di stent intra - coronarico e con sospetta re - stenosi , stata effettuata una 64 - tc ( sensation 64 , siemens )  . 
i parametri di scansione erano : strati 322 ( sovracampionamento sullasse z mediante flying focal spot ) , collimazione individuale 0 , 6 mm , tempo di rotazione 0 , 33 s , avanzamento 3 , 84 mm / rot , kv 120 , ma 900 . 
dopo la somministrazione di mezzo di contrasto iodato ( iomeprolo 400 mgi / ml , iomeron ; 100 ml a 5 ml / s ) e bolus chaser ( 40 ml di soluzione fisiologica a 5 ml / s ) , la scansione stata completata in meno di 12 s . 
tutti i segmenti coronarici con uno stent sono stati valutati da due osservatori in consenso e giudicati come segue : pervi , con iperplasia intimale intra - stent ( iis ; riduzione del lume < 50% ) , con re - stenosi intra - stent ( ris ; 50% ) , o con occlusione intra - stent ( ois ; 100% )  . 
nei rimanenti 91 pazienti sono stati valutati 102 stent ( 31 in arteria coronaria destra ; 10 del tronco comune sinistro ; 54 della arteria discendente anteriore ; 7 nellarteria circonflessa )  . 
la 64 - tc fornisce una accuratezza diagnostica elevata nella rilevazione della re - stenosi intrastent in una popolazione selezionata di pazienti . parole chiave coronarografia tomografia computerizzata multistrato tc 64 strati stent coronarici introduction introduzione f . 
these scanners have proved on average more effective at assessing stenosis in native coronary arteries [ 1114 ]  . the placement of coronary artery stents has significantly reduced the development of restenosis when compared with angioplasty [ 15 , 16 ]  . 
traditionally , follow - up of stents has been performed with coronarography . studies of the diagnostic accuracy of msct using 4and 16 - slice scanners in the evaluation of restenosis of coronary arteries have demonstrated progressive improvement , although they have been hindered by significant limitations such as artefacts and small case series [ 2129 ]  . 
we report on the diagnostic accuracy of a 64 - slice scanner in the identification of in - stent restenosis of coronary artery stents . materials and methods population ninety - five patients ( 72 men and 23 women , mean age 588 years ) were enrolled in the study , all with suspected obstructive coronary artery disease who had previously undergone coronary artery angioplasty for the purposes of percutaneous stent deployment or simply for follow - up in the context of other studies being undertaken at our institute . 
exclusion criteria for the study were more than one stent per vessel in the coronary artery tree , a single stent with a diameter of less than 2.5 mm , aortocoronary bypass , atrial fibrillation , known allergy to iodinated contrast material and kidney failure ( serum creatinine > 120 mmol / l )  . 
patients with a heart rate greater than 65 beats per minute ( bpm ) received an oral dose of 100 mg metoprolol tartrate 4560 min prior to the examination . as many of the patients had been treated in peripheral hospitals , we were only able to identify the exact type of stent deployed in a limited number of patients . 
the mean time interval between 64 - ct examination and conventional coronarography ( cc ) la tomografia computerizzata multistrato ( tcms ) ha avuto nei recenti 5 anni notevoli miglioramenti tecnologici che hanno esitato in una serie di nuove applicazioni , prima fra tutte quella cardiaca e coronarica [ 13 ]  . 
questa tecnologia si dimostrata mediamente pi efficace nella valutazione delle stenosi nelle coronarie native [ 1114 ]  . il posizionamento di stent coronarici ha significativamente ridotto levenienza di re - stenosi se comparata con langioplastica [ 15 , 16 ]  . 
tradizionalmente , il follow - up degli stent ha avuto bisogno della coronarografia . le casistiche di accuratezza diagnostica per restenosi mediante tcms sugli stent coronarici con tecnologia a 4 e 16 strati hanno descritto risultati progressivamente migliorati ma sempre con significative limitazioni , artefatti e casistiche esigue [ 2129 ]  . 
riportiamo laccuratezza diagnostica di uno scanner a 64 strati nella rilevazione delle restenosi intra - stent degli stent coronarici . materiali e metodi popolazione novantacinque pazienti ( 72 maschi e 23 femmine , et media 588 anni ) con sospetta malattia coronarica ostruttiva precedentemente sottoposti ad angioplastica coronarica con posizionamento di stent per via percutanea o per semplice follow - up nel contesto di altri studi in corso nella nostra istituzione , sono stati arruolati per lo studio . 
i pazienti con pi di uno stent per vaso nellalbero coronarico , con singoli stent di diametro inferiore a 2 , 5 mm , con bypass aorto - coronarico , con fibrillazione atriale , con allergia nota al mezzo di contrasto iodato ed insufficienza renale ( creatinina sierica > 120 mmol / l ) sono stati esclusi dallo studio . 
ai pazienti con frequenza cardiaca superiore a 65 battiti per minuto ( bpm ) , 4560 minuti prima della scansione , sono stati somministrati per os 100 mg di metoprolo - tartrato . essendo molti dei pazienti seguiti in ospedali periferici , non stato possibile risalire con precisione al tipo di stent impiantato se non in un ridotto numero di pazienti . 
the study was approved by the hospital ethics committee , and all patients provided written informed consent . scan and image reconstruction the angiography scan was performed with a 64 - slice spiral ct scanner ( sensation 64 cardiac , siemens , germany ) equipped with a 32 - row detector and periodic motion of the focal spot ( z - flying focal spot ) capable of achieving an effective z - axis spatial resolution of 0.4 m contrast enhancement was achieved through the antecubital intravenous administration of 100 ml of nonionic iodinated contrast material ( iomeprol 400 mgl / ml , iomeron , bracco , italy ) at an injection rate of 5 ml / s followed by 40 ml of saline solution at the same rate . 
the region of interest ( roi ) was placed in the ascending aorta with a threshold of + 100 hu [ 31 ]  . the scan and reconstruction parameters were number of detectors / collimation 322 / 0.6 mm , gantry rotation time 330 ms , table feed / rotation 3.84 mm ( pitch 0.2 ) , 120 kvp , 900950 mas , field of view 150 mm , effective slice thickness 0.75 mm , reconstruction increment 0.4 mm , soft - tissue convolution kernel dedicated for stents ( b30fb46f )  . the images were reconstructed with a predetermined offset based on the patients electrocardiogram ( ecg ) signal [ 1 ]  . 
at the operators discretion , additional reconstructions in the end - systolic phase were performed ( + 225 / + 275 / + 325 ms from the r wave )  . image assessment the images were sent to a dedicated workstation ( leonardo , siemens , germany ) where the available reconstructions were assessed using all of the conventional postprocessing techniques [ axial images , multiplanar reconstructions ( mpr ) , curved mpr ( cmpr ) , maximum intensity projections ( mip ) and volume rendering ( vr ) ]  . 
 i parametri di scansione e ricostruzione sono : numero di detettori / collimazione 322 / 0 , 6 mm , tempo di rotazione del tubo radiogeno 330 ms , avanzamento / rotazione 3 , 84 mm ( pitch 0 , 2 ) , kvp 120 , ma 900950 , campo di vista 150 mm , spessore effettivo dello strato 0 , 75 mm , incremento di ricostruzione 0 , 4 mm , filtro di convoluzione per tessuti molli e dedicato per stent ( b30fb46f )  . le immagini sono state ricostruite con modalit retrospettiva basata sul segnale ecg [ 1 ]  . 
le finestre temporali di ricostruzione utilizzate sono state 300 ms , 350 ms , e 400 ms dalla successiva onda r ( tecnica del ritardo assoluto inverso ) [ 1 ]  . 
quando ritenuto opportuno dalloperatore sono state eseguite ulteriori ricostruzioni in fase tele - sistolica ( + 225 / + 275 / + 325 ms dallonda r )  . analisi delle immagini le immagini sono state inviate ad una stazione di lavoro dedicata ( leonardo , siemens , germania )  . 
le ricostruzioni disponibili sono state valutate con tutte le convenzionali tecniche di post processing ( immagini assiali , ricostruzioni multiplanari - mpr , riformattazione centroluminale - cmpr , proiezione di massima intensit - mip , e volume rendering - vr )  . due osservatori in consenso hanno valutato tutti gli stent dei pazienti . 
1a - d example of a patent stent with 64 - slice computed tomography ( ct ) coronary angiography in a patient who underwent percutaneous coronary intervention with stenting of the left circumflex . 
conventional coronary angiography shows a nudge of the vessel profile proximal to the stent ( a ) ( arrowhead )  . the stent appears patent with 64 - ct ( b , d )  . 
in particolare la sezione ortogonale allasse del vaso ( c ) consente di apprezzare la presenza di contrasto allinterno del lume . conventional diagnostic coronarography coronarografia convenzionale diagnostica cc was performed with a standard technique in a time interval ranging from 1 week prior to and 1 week after msct examination . 
a value 50% indicated significant stenosis . la coronarografia convenzionale ( cc ) stata effettuata con tecnica standard in un range tra una settimana prima ed una settimana dopo lac - tcms . 
un valore 50% indica una stenosi significativa . statistical analysis analisi statistica dei dati the diagnostic accuracy of 64 - ct in identifying significant restenoses ( 50% reduction of the diameter of the lumen ) was assessed using quantitative cc as a reference standard . laccuratezza diagnostica della 64 - tc per la rilevazione di re - stenosi significative ( 50% di riduzione del diametro luminale ) stata valutata utilizzando la cc quantitativa come stanf . 
2a - d example of in - stent restenosis with 64 - slice computed tomography ( ct ) coronary angiography in patient who underwent percutaneous coronary angioplasty and stenting on the left anterior descending . 
mediante 64 - tc si osserva una area ipodensa parzialmente eccentrica che inizia sul margine prossimale dello stent e si estende al suo interno determinando una restenosi significativa ( b , d )  . 
i risultati sono stati suddivisi per vaso ( arteria coronaria destra acd ; tronco comune sinistro tcs ; arteria discendente anteriore ada ; arteria circonflessa acx ) e per segmenti prossimali ( 1 , 5 , 6 , 11 ) e distali ( 24 , 710 , 1215 ) secondo la classificazione a 15 segmenti dellamerican heart association [ 32 ]  . 
tutti i valori di accuratezza diagnostica sono stati espressi mediante intervalli di confidenza del 95% . four of the 95 patients initially enrolled were excluded , two because their heart rate exceeded 65 bpm during the scan dei 95 pazienti inizialmente reclutati , 4 sono stati esclusi . due a causa di valori di frequenza cardiaca durante la scanrisultati results table 1 diagnostic accuracy of msct - ca for in - stent restenosis 50% f . 
msct - ca , multislice computed tomography coronary angiography ; no . , number of stents ; ppv , positive predictive value ; npv , negative predictive value ; rca , right coronary artery ; lm , left main coronary artery ; lad , left anterior descending coronary artery ; cx , circumflex coronary artery ; na , non - assessable . tabella 1 accuratezza diagnostica della angiografia coronarica ac - tcms per le restenosi intra - stent 50% . vessels vasi tutti n ( % ) 31 ( 30 ) 10 ( 10 ) 54 ( 53 ) 7 ( 7 ) n ( % ) 31 ( 30 ) 10 ( 10 ) 54 ( 53 ) 7 ( 7 ) sensibilit specificit 100 ( 47100 ) 85 , 7 ( 4299 ) 100 ( 15100 ) 92 , 85 ( 6699 ) 100 ( 86100 ) 30 ( 665 ) 93 , 9 ( 8398 ) 100 ( 29100 ) 88 , 63 ( 8094 ) 100 ( 47100 ) 66 , 66 ( 2992 ) 100 ( 15100 ) 56 , 52 ( 3476 ) 100 ( 86100 ) 100 ( 29100 ) 97 , 9 ( 8899 ) 100 ( 29100 ) 98 , 73 ( 9399 ) i valori di sensibilit , specificit , valore predittivo positivo e negativo sono espressi in percentuale , mentre quelli riportati tra parentesi si riferiscono ai rispettivi intervalli di confidenza al 95% . 
the study population was therefore reduced to 91 patients ( 70 men and 21 women , mean age 588 years ) , with a total of 102 stents ( mean 1.1 stent per patient )  . sixty - one patients ( 67% ) were already undergoing treatment with beta - blockers , and 33 ( 36% ) received an additional dose in accordance with the above - mentioned protocol . 
the sensitivity for the identification of restenosis by vessel was 100% for the rca , 86% for the lad and 100% for the cx . sione , superiori ai 65 bpm ed altri due per aver mostrato una qualit delle immagini a livello dello stent non compatibile con una valutazione diagnostica ( ad esempio , artefatti da movimento ed eccessivo rumore delle immagini )  . 
la sede degli stent era nel 30% ( n = 31 ) dei casi la coronaria destra , nel 10% ( n = 10 ) dei casi il tronco comune , nel 53% ( n = 54 ) dei casi la discendente anteriore , e nel 7% ( n = 7 ) la coronaria circonflessa . 
la sensibilit , specificit , valore predittivo positivo e negativo per tutti gli stent nella rilevazione delle ris + ois sono risultate 92 , 9% , 88 , 6% , 56 , 5% , e 98 , 7% , rispettivamente . 
la sensibilit per la rilevazione di restenosi per vaso risultata del 100% per lacd e del 86% per la ada e 100% per la cx . discussion studies on electron beam tomography ( ebt ) report a sensitivity of 78% and a specificity of 98% for high - grade in - stent restenosis [ 33 ]  . 
the method adopted , however , was completely different , as the study involved a multisection dynamic assessment , which measured the temporal variation of la letteratura riguardante studi con electron beam ct ( ebt ) riferisce una sensibilit del 78% ed una specificit del 98% per le stenosi intrastent di alto grado [ 33 ]  . 
the same study , building on the previous dynamic study [ 33 ] , used the degree of enhancement of the native vessel distal to the stent as a criterion for vessel patency [ 35 ]  . 
in our study , however , this proved to be a reliable measure only in one of four cases of occlusion ; in the remaining three cases , distal enhancement was normal due to collateral circulation . as with calcifications , stents are characterised by high density , which at ct leads to an enlargement of the image known as blooming [ 36 ]  . 
in small vessels such as the coronary arteries , the negative effect of the artefact is increased by the fact that its size is in the same order as the diameter of the vessel [ 36 ]  . the use of scanners with hardware and software solutions capable of improving spatial resolution promises to make the visualisation of the in - stent lumen feasible [ 9 , 37 , 38 ]  . 
the incidence of restenosis has in fact been considerably reduced , particularly following the introduction of drug - eluting stents , and this suggests the need for enrolling large patient populations to be able to achieve values of diagnostic accuracy with a sufficient level of statistical significance . 
this would , in fact , require a sensitivity of 90% or greater and an npv of 98% . the data obtained in this study on a group of 91 patients with 102 stents using a 64 - slice scanner reveal a higher diagnostic accuracy , with a sensitivity of 92% and specificity of 89% . 
the improvement with respect to earlier studies can be attributed to the technologically superior equipment used , although such direct comparisons between different devices should be made with great care given the considerable variations in the characteristics of the populations and the scan protocols . 
undoubtedly the reduction in the voxel size ( 0.4 mm3 ) linked to the z - flying focal spot plays an important role , and associated with this is the reduction in residual motion artefacts related to the improved temporal resolution ( 185 ms effective scan time ) and the use of dedicated convolution kernels ( medium - sharp b46f )  . the main limitation of the present study essentially trattandosi di una valutazione dinamica multi - sezione che misurava la variazione temporale dellattenuazione nel vaso nativo distalmente allo stent [ 33 ]  . 
questa metodologia era la sola utilizzabile stante la incapacit della ebt di visualizzare il lume del vaso allinterno dello stent [ 33 , 34 ]  . uno studio basato su msct a 4 canali ha dimostrato che impossibile in tutti gli stent visualizzare il lume , indipendentemente dal tipo di stent e dal suo diametro [ 35 ]  . 
lo stesso studio descrive come criterio per la perviet , rifacendosi allo studio dinamico precedente [ 33 ] , il grado di opacizzazione del vaso nativo distalmente allo stent [ 35 ]  . 
nella nostra esperienza , questo criterio stato affidabile in uno solo dei 4 casi di occlusione ; nei rimanenti tre casi stata osservato un grado di opacizzazione normale dovuto a circolo collaterale . gli stent cos come le calcificazioni sono caratterizzati da una densit elevata che alla tc determina un ingrandimento dellimmagine che viene definito blooming [ 36 ]  . 
questo artefatto multifattoriale deriva da effetto volume parziale , indurimento del fascio ed interpolazione e pu essere attenuato utilizzando dei filtri di convoluzione a pi alta frequenza ( fig . 3 ) [ 36 ]  . 
nei vasi di piccole dimensioni , come le coronarie , leffetto negativo dellartefatto aumentato dal fatto che la sua dimensione dello stesso ordine di grandezza del diametro del vaso [ 36 ]  . limpiego di apparecchiature con soluzioni hardware e software in grado di migliorare la risoluzione spaziale promette di rendere fattibile la visualizzazione del lume intrastent [ 9 , 37 , 38 ]  . 
infatti , soprattutto dallintroduzione degli stent medicati , lincidenza della restenosi si ridotta sensibilmente e questo presuppone larruolamento di ampie popolazioni di pazienti per raggiungere valori di accuratezza diagnostica che abbiano una sufficiente potenza statistica . 
per poterlo fare infatti sarebbe necessario avere una sensibilit del 90% o superiore ed un valore predittivo negativo superiore al 98% . la casistica presentata in questo lavoro , ottenuta su apparecchiatura a 64 strati , in un gruppo di 91 pazienti con 102 stent mostra una accuratezza diagnostica superiore con una sensibilit del 92% ed una specificit dell89% . 
il migliore risultato rispetto agli studi precedenti si spiega con la tecnologia superiore utilizzata , tuttavia ancora arduo fare paragoni diretti tra tecnologie considerando le considerevoli variazioni nelle caratteristiche delle popolazioni e nei protocolli di scansione . 
sicuramente la riduzione delle dimensioni del voxel ( 0 , 4 mm3 ) legata al sovra - campionamento sullasse z gioca un ruolo importante a questo si associano , la riduzione degli artefatti da movimento residuo legati f . 
the image at the top shows the traditional filter ( mediumsmooth ; b30f ) and the image at the bottom shows a higher dedicated filter for stents ( medium - sharp ; b46f )  . 
in alto il filtro tradizionale ( medium - smooth ; b30f ) ed in basso un filtro pi elevato ma dedicato per gli stent ( medium - sharp ; b46f )  . 
si nota come il filtro determini un aumentato rumore di fondo dellimmagine e come produca anche un incremento della attenuazione del lume coronarico allinterno dello stent . regards the inclusion criteria of the patients , which restricted the analysis to patients with a regular heart rate < 65 bp a further limitation connected with the technique is the relatively high level of exposure to ionising radiation , estimated at 15.2 msv for men and 21.4 msv for women [ 4043 ]  . although the introduction of drug - eluting stents has proved favourable for patients , it has made assessment of the diagnostic accuracy of msct in the follow - up of stents somewhat difficult . 
these new - generation stents in fact have displayed lower rates of restenosis at 6 months and lower prevalence of complete occlusions compared with earlier studies [ 1719 , 4451 ]  . future developments the recent introduction of new technologies characterised by an increased number of slices per rotation or multiple detectors will , over time , improve the visualisation of coronary artery stents but only if there is a concomitant increase in spatial resolution . 
a device capable of scanning 128 slices per rotation with an individual detector width similar to that of previous technology will only be able to increase the speed of completing the examination . 
a detector with a lower individual width will be able to achieve greater spatial resolution but only at the cost of the higher radiation dose required to obtain image quality in line with the other parameters . one simple and desirable solution lies in the development of stent materials that are less radiopaque or more radiotransparent . 
another possibility currently being tested is the use of absorbable stents made from biological materials that alla migliore risoluzione temporale ( 185 ms effettivi ) ed allutilizzo di filtri dedicati ( medium - sharp b46f )  . la limitazione principale del presente studio legata essenzialmente ai criteri di inclusione dei pazienti che hanno ristretto lanalisi ai pazienti con frequenza cardiaca regolare e < 65 bp una ulteriore limitazione , correlabile alla metodica , legata alla elevata esposizione a radiazioni ionizzanti stimata in 15 , 2 e 21 , 4 msv per maschio e femmina , rispettivamente [ 4043 ]  . lintroduzione di stent coronarici medicati ( drug - eluting stents o des ) , sebbene favorevole ai pazienti , rende difficoltosa la valutazione dellaccuratezza diagnostica della tcms nel follow - up degli stent . 
infatti , questi stent di nuova generazione hanno dimostrato delle ridotte percentuali di re - stenosi a 6 mesi ed una ridotta prevalenza di occlusioni complete se comparate con le precedenti casistiche [ 1719 , 4451 ]  . sviluppi futuri la recente introduzione di nuove tecnologie caratterizzate da un numero aumentato di strati per rotazione o di multipli sistemi tubo - detettore potranno migliorare eventualmente la visualizzazione degli stent coronarici , ma verosimilmente solo se porteranno ad un concomitante incremento della risoluzione spaziale . 
un dettetore di ampiezza individuale inferiore porter invece una maggiore risoluzione spaziale a prezzo di una dose di radiazioni superiore necessaria per ottenere una qualit delle immagini a parit degli altri parametri . una soluzione semplice ed auspicabile potrebbe essere legata allo sviluppo di materiale meno radio - opachi o ancof . 
the table shows how distal runoff was initially used for assessing patency , but with technological advances , the authors began primarily to use criteria of direct visualisation studies no . 
the projectile effect is when an object is attracted by the magnet with the risk , as reported in literature , of hitting the patient , operators and / or the instrument . objects which typically can undergo this effect are oxygen and helium cylinders , iv stands , cleaning trolleys , chairs , lamp holders , scissors , forceps , clampers , traction weights , monitoring instruments , and especially metallic splinters within the patient . twisting ( torsion ) typically occurs with cerebral vascular clamps and cochlear implants . 
burns can be caused when electrically conductive material is introduced within the magnet , for example , ecg electrodes , monitoring cables and coils which are in contact with the patients skin , as well as tattoos and eye - liners that contain iron - oxides . 
the risk for patients can be reduced by specific educational programs within individual radiology departments which include other specializations and external referring physicians with the aim of developing a standardized safety protocol . key words mr safety foreing body pacemaker pregnancy riassunto la presenza di un campo magnetico statico ( bo ) allinterno della sala rm , di un campo di radiofrequenza ( rf ) , di gradienti dinamici variabili nel tempo e di forte rumore durante lesame comportano il possibile verificarsi di eventi con implicazioni per la sicurezza del paziente . 
oggetti che tipicamente possono subire questo effetto sono : bombole di ossigeno , piantane per le fleboclisi , bombole di elio , carrelli delle pulizie , sedie , fissatori di lampadine , forbici e clamper , pesi da trazione , pulsossimetri . 
ustioni : in genere sono causate dallintroduzione di materiale elettrico conduttivo allinterno del magnete come elettrodi ecg , cavi del pulsossimetro , bobine in contatto con la superficie cutanea del paziente , ma anche tatuaggi , eye - liner che contengono ossido di ferro . 
artefatti : si possono verificare artefatti dovuti a emissione di rf da parte di dispositivi , che viene considerata rumore dalla bobina di ricezione , oppure vuoto di segnale da componente metallica , che pu mascherare o simulare una patologia . 
in 1992 , 100 , 000 , 000 mr examinations were performed in the usa alone ; today , given the increase in the number of available tomographs and routine clinical applications , it would be impossible to calculate how many are performed throughout the world . the number of serious accidents involving patients that have occurred since the introduction of mr for clinical purposes in 1984 are fortunately few , at least in part because of the growing attention being paid to safety issues [ 1 ]  . 
long - term exposure , such as that which may be experienced by an mr operator or a patient with a chronic disease requiring serial investigations over time , is still a subject of scientific debate insofar as in vitro studies have demonstrated potentially harmful effects on tissues that are apparently below the threshold of clinical significance [ 2 ]  . 
 literature concerning patient safety mainly concentrates on the two scenarios that largely reflect serious accidents that have happened in the past : interactions between the mf and ferromagnetic materials , and the malfunctioning of cardiac pacemakers ( pm )  . 
in specific terms , the presence inside the mr room of a static mf ( b0 ) , a field of radiofrequency ( rf ) , dynamic gradients varying over time and the loud noise occurring during the examination create an environment in which events may occur that threaten patient safety . 
here we review the different types of dangerous interactions in general before going into more detail about some of the situations that more frequently involve radiologists in the everyday management of patients who have to undergo mr imaging . 
we conclude with the current guidelines for performing an mr examination during pregnancy and lactation . la risonanza magnetica ( rm ) una metodica sempre pi diffusa sul territorio e sempre pi richiesta dal clinico o dal chirurgo , anche in virt della recente affermazione del body e cardiac imaging . 
nel 1992 , solo negli usa , sono stati eseguiti 100000000 di esami rm ; oggi , con lincremento del numero di tomografi disponibili e delle applicazioni entrate nella routine clinica , nel mondo vengono eseguiti un numero di esami rm difficilmente calcolabile . dallintroduzione della rm per uso clinico , nel 1984 , ad oggi , gli incidenti gravi a danno del paziente si contano per fortuna sulle dita delle mani , anche grazie ad una sempre maggiore sensibilit al tema della sicurezza [ 1 ]  . 
lesposizione a breve termine al campo magnetico di tutte le intensit di utilizzo clinico ( da 0 , 2 a 3 , 0 tesla ) e anche fino a 8 tesla ( a scopo di ricerca ) , stato approvata dalla fda americana come non dannosa per lorganismo : questa situazione - tipo quanto si verifica per il paziente in generale . 
lesposizione a lungo termine , quale potrebbe essere quella di un operatore di rm interventistica , o di un paziente con malattia cronica che esegue controlli seriati nel tempo , ancora sotto osservazione scientifica in quanto studi in vitro hanno dimostrato effetti potenzialmente dannosi per i tessuti , apparentemente sotto una soglia di significativit clinica [ 2 ]  . lattenzione sulla sicurezza del paziente si concentra in letteratura maggiormente su due tipologie di situazioni , anche sulla base degli incidenti gravi riportati dalla letteratura scientifica : linterazione del campo magnetico con materiale ferromagnetico e il malfunzionamento di pacemaker cardiaci . nello specifico , la presenza di un campo magnetico statico ( bo ) allinterno della sala rm , di un campo di radiofrequenza ( rf ) , di gradienti dinamici variabili nel tempo e di forte rumore durante lesame , creano una situazione ambientale che pu comportare il possibile verificarsi di eventi con implicazioni per la sicurezza del paziente . 
passeremo in rassegna in generale le diverse tipologie di interazioni pericolose per entrare nello specifico di alcune situazioni che pi frequentemente interessano tutti i giorni il radiologo nella gestione del paziente che deve sottoporsi ad indagine di risonanza magnetica . 
depending on the type of magnet and the intensity of the generated field , mf lines extend for a certain distance into the environment ( the fringe field ) and , to varying extents , attract objects to the centre of the magnet . 
an object in zone 2 is not only subject to a rotational interaction but also to a translational force directed towards the centre of the magnet that ceases only when it enters zone 1 . 
ferromagnetic objects near a static mf can become projectiles when they are attracted to the magnet as a result of : the strength of the mf the magnetic susceptibility of the object the mass of the object the distance of the object from the magnet the orientation of the object in relation to the mf . 
 the following is a modified list of a usa register listing the objects attracted inside the magnet during 2001 [ health devices alerts ( hda ) ] as shown in table 1 . in addition to damaging the magnet , the direct consequence of a projectile effect can be patient injury , and there are reports in the literature of injuries or fatalities affecting patients [ 3 , 4 ] , which have often involved helium or oxygen cylinders . twisting twisting refers to the deflection or torsion of magnetic objects that tend to orient themselves parallel to the direction of the b0 . 
typically , objects that can be dangerous for patients when subjected to this effect are vascular clips and cochlear implants , but there are various parts of implants or other objects that can be twisted and thus affect implant functioning or cause damage to the patient . 
at the ocular level , with the possibility of seriously damaging eyesight . vascular clips one of the reasons for screening patients is precisely that of identifying beforehand and possibly solving the impasse in which radiologists using mr often find themselves : how to manage a patient who is potentially bearing a ferromagnetic clip . 
questo fenomeno comporta un rischio di impatto sia con il paziente o loperatore che si trovino nel tragitto , sia per il magnete che ne pu risultare seriamente danneggiato . a seconda del tipo di magnete e dellintensit del campo generato , esistono linee di campo magnetico che si estendono per una certa distanza nellambiente ( campo disperso fringe field )  . 
tale distribuzione determina in varia misura lattrazione verso il centro del magnete . il campo magnetico statico suddiviso per convenzione in zona 1 ( larea circostante lisocentro magnetico , che contenuta allinterno del magnete ) e zona 2 ( larea esterna al magnete che strutturata con gradienti di intensit decrescente in senso centrifugo )  . 
oggetti ferromagnetici portati vicino al cm statico possono cio diventare proiettili per una forza di attrazione con il magnete determinata da : forza del cm ; suscettibilit magnetica delloggetto ; massa delloggetto ; distanza dal magnete ; orientamento delloggetto nei confronti del cm . esiste una registro negli usa che a tutto il 2001 riportava una lista di oggetti attirati dentro il magnete ( hda , health devices alerts ) , che riportiamo , modificata , nella tabella 1 . la conseguenza diretta del verificarsi di un effetto proiettile risiede oltre che nel possibile danneggiamento del magnete , nel possibile ferimento del paziente . 
ci sono reports in letteratura di danno o esiti fatali a carico del paziente [ 3 , 4 ] , che spesso hanno interessato bombole di elio o di ossigeno . twisting il termine twisting si riferisce alla deflessione / torsione degli oggetti magnetici che tendono a orientarsi parallelamente alla direzione del bo . 
in practice , patients often arrive for their appointment without any precise information concerning the type or model of the clip , or with a potentially unreliable certification of compatibility . in the case of endocranial clips , it is always necessary to require written certification from the neurosurgeon [ 5 ] ; if the clip is made of titanium or a titanium alloy , the examination can go ahead [ 6 , 7 ]  . 
if it is certified as being mr compatible but not made of titanium , it is possible to take 1995 as a dividing line : there are substantially no risks in the case of clips used after that date , but there is a certain risk of significant interactions with clips implanted earlier . 
of course , if the clip is declared to be ferromagnetic or otherwise incompatible with mr , the examination must be cancelled . abdominal haemostatic clips are also frequently identified during the screening procedure and , unless they are expressly declared as being compatible with mr , it is necessary to check radiologically in order to assess their radiopacity and , therefore , their metal component : if they are visible upon computed tomography ( ct ) or x - rays , they could be made of a metal alloy and will need to be certified . 
once again , mr - compatible materials have been increasingly used since the mid - 1990s , and there is likely to be an extremely low risk of incompatibility in the case of those positioned more recently . it is true that some of the sutures still used in gastroinuna delle ragioni per cui esiste il modulo di screening per il paziente proprio quella di anticipare e possibilmente risolvere limpasse nella quale si pu trovare spesso il radiologo che si occupa di rm : la gestione di un paziente potenzialmente portatore di una clip emostatica ferromagnetica . la possibilit di identificare uno di questi casi nella sede della compilazione del modulo di screening per le controindicazioni alla rm , permette da una parte di evitare grossolani errori quale potrebbe essere lintroduzione nello scanner rm di un paziente con clip non compatibile , in una sede critica quale un vaso arterioso cerebrale per esempio , e dallaltra la possibilit di richiedere al paziente di procurarsi una certificazione scritta di compatibilit della clip presso il proprio curante o il chirurgo che lha operato , e quindi di non rischiare di saltare lappuntamento per mancanza di informazione [ 5 ]  . 
in realt nella pratica si pone spesso il problema del paziente che si presenta alla data dellesame senza informazioni precise sul tipo e modello della clip , o con una non sicura certificazione di compatibilit . per quanto attiene alle clip vascolari endocraniche di fatto occorre sempre esigere una certificazione scritta da parte del neurochirurgo [ 5 ]  . 
se viene certificata come compatibile con la rm ma non costituita di titanio , si pu prendere la data del 1995 come spartiacque , oltre la quale non vi sono sostanzialmente rischi , prima della quale vi invece un certo rischio di interazione significativa . 
naturalmente se la clip dichiarata non compatibile con lambiente rm o come ferromagnetica , non si autorizzati a procedere con lesame rm . per quanto riguarda le clip emostatiche addominali , altro frequente riscontro durante la procedura di screening , salvo che non siano dichiarate espressamente come compatibili con la rm , occorre eseguire uno screening radiologico per valutarne la radiopacit e quindi la componente metallica : se visibili alla tc o in rx , potrebbero essere di lega metallica e occorre una loro certificazione . 
anche in questo ambito dalla met degli anni 90 si assistito ad un sempre maggiore uso di materiali compatibili con la rm , e il criterio di vicinanza temporale del loro posizionamento gioca a favore per un bassissimo rischio che non siano compatibili . per quanto attiene le suture per interventi gastro - intestinali , sono ancora oggi usati materiali che possono subire una certa interazione con il campo magnetico , ma senza rischi significativi per la salute del paziente , mantenendo la regola di aver permesso almeno il processo di cicatrizzazione e quindi almeno 1521 giorni dallintervento . corpi estranei la gestione di un paziente portatore di corpo estraneo endoorbitario deve prevedere unaccurata anamnesi , che non pu prescindere dallattenta analisi del modulo delle controindicazioni alla rm . 
it can be useful to repeat the questions just before entering the mr room because patients often fail to remember the presence of an eye splinter when they are first asked . 
the best strategy is to exclude the presence of a radiopaque foreign body by means of an orbital radiograph , which should always be performed in the case of a retained splinter , a history of a foreign body without precise memory of its removal , or when this was not followed by a thorough ophthalmological examination excluding the presence of other remnants . 
however , as clearly documented in the literature , radiography is not indicated as a form of blanket screening for all of the population at risk ( usually assessed on the basis of their working activities ) [ 9 ]  . 
however , not all bullets have the same ferromagnetic properties : most hunting bullets made in the usa are not ferromagnetic [ 10 ] , but those made for military purposes are and are subject to various degrees of rotation when exposed to the action of the mf . grenade fragments contain steel and are ferromagnetic [ 11 ]  . 
as bullets , pellets and shrapnel may always be contaminated by metallic material , the risk / benefit ratio of an mr examination should always be assessed in people carrying such foreign bodies . 
before undergoing an mr examination , any patient who declares himself or herself to be a bearer of metal bullets or shrapnel should have a standard radiograph of the affected body district to provide information about its position and nature [ 12 ]  . 
in a recent study , no neurological changes or painful reactions were observed in patients with spinal lesions due to the presence of bullets or metal fragments who underwent mr examinations using a 1.5 - t machine [ 13 ]  . 
none of the 13 metallic suture threads tested showed any interactions with the 1.5 - t field , whereas two ( flexon suture and steel suture , united states surgical , new haven , ct ) showed a slight deflection when exposed to a 3t field ; however , these forces were not sufficient to mobilise the stitches in situ [ 14 , 15 ]  . 
la strategia in questo caso prevede lesclusione della presenza di un corpo estraneo radiopaco con una radiografia delle orbite , da eseguirsi sempre nel caso di scheggia ritenuta o di storia clinica di pregresso corpo estraneo senza ricordo esatto di rimozione o senza che questa sia stata seguita da unaccurata visita oftalmologica che ne abbia escluse altre residue . 
la radiografia non invece indicata come screening a tappeto su tutta la popolazione a rischio ( in genere sulla base dellattivit lavorativa ) , come ben documentato anche il letteratura [ 9 ]  . la rm pu essere unindagine utile o indispensabile in pazienti giunti allattenzione del medico con ferite da arma da fuoco recenti o pregresse . 
non tutti i proiettili hanno per le stesse propriet ferromagnetiche ; la maggior parte dei proiettili da caccia sportiva fabbricati negli stati uniti non sono ferromagnetici [ 10 ] , i proiettili per uso militare sono invece ferromagnetici e sono soggetti a vari gradi di rotazione quando sottoposti allazione del campo magnetico . le schegge di granata contengono acciaio e sono ferromagnetiche [ 11 ]  . 
in ogni caso va sempre considerato che proiettili , pallottole e schegge possono essere contaminate da materiale metallico quindi bisogna sempre valutare il rapporto rischio / beneficio di unindagine di rm in pazienti portatori di tali corpi estranei . 
prima di sottoporre ad indagine rm un paziente che dichiara di essere portatore di schegge o proiettili metallici andrebbe eseguita una radiografia standard del distretto corporeo colpito per ottenere utili informazioni sulla posizione del corpo estraneo e sulla sua natura [ 12 ]  . 
la presenza di proiettili o schegge metalliche nel canale spinale di pazienti paralizzati rappresenta una controindicazione solo relativa allindagine rm ; in un recente studio infatti non si sono osservate modificazioni del quadro neurologico o reazioni dolorose in pazienti con lesioni midollari portatori di proiettili o schegge metalliche in sede endocanalare spinale sottoposti ad esame rm con apparecchiatura da 1 , 5 t [ 13 ]  . i fili di sutura possono essere fatti di diversi materiali , metallici e non . 
nessuno dei 13 fili di sutura metallici testati ha mostrato interazioni con il campo da 1 , 5 t , mentre 2 ( flexon suture e steel suture , united states surgical , north haven , ct ) hanno mostrato una lieve deflessione quando sottoposti allazione del campo da 3 t ; tali forze non erano per sufficienti a mobilizzare il filo in situ [ 14 , 15 ]  . artefatti si possono verificare artefatti dovuti a : emissione rf da parte di dispositivi , che viene considerato rumore dalla bobina di ricezione ; vuoto di segnale da componente metallica , che pu mascherare o simulare una patologia . lartefatto da clip vascolare ferromagnetica pu essere a . 
 the artefact due to a ferromagnetic vascular clip can be an aid when the findings of a previous mr examination are available , when the type of clip implanted is not known at the time of the current investigation , and its ferromagnetism needs to be assessed to decide whether or not it is safe to proceed . device malfunction ( electronic or mechanical ) such malfunctions include devices with analogic valves , electric motors , transformers , relays and switches , prostheses that use magnetisation to remain attached to a patient ( some dental devices ) , and some implants that are activated electronically , magnetically or mechanically . 
echocardiography ( ecg ) traces may be distorted , with alterations in t waves . pacemakers the presence of a cardiac pm has accompanied the development of mr over the years since the beginning as an absolute contraindication capable of threatening a patients life . 
animal and in vitro studies first documented the risk of pm malfunction in the 1980s [ 16 ] , and there were reports of at least ten deaths due to taking patients bearing pms into the mr roothe principal considerations concerning the safety of these devices were first put into a structured form in a review by mathur - de vre published in 1987 [ 17 ]  . 
on the basis of this contraindication , an increasing proportion of the population ( currently estimated at several million persons ) could not undergo mr even in the presence of one of the neurological , neurosurgical or oncological diseases , or common non - lifethreatening conditions such as musculoskeletal diseases , for which mr is the most accurate diagnostic examination . however , recent studies carried of bearers of pms undergoing mr examinations in emergency settings , together with technological advances in the pms themselves , have gradually modified these views . 
since 1996 , technological developments have led to a substantial reduction in the proportion of ferromagnetic material inside pms , and redesigns of their electronic architecture and programming , reductions in the distance between the electrodes and changes in the materials ( mp35n an alloy that is less susceptible to magnetism ) have considerably reduced their sensitivity to electromagnetic interference [ 18 ]  . the known effects of mr on cardiac pms are due to the static mf , the temporary rf field and the gradients ( additional mfs ) , and are shown in table 2 . 
il tracciato ecg pu risultare distorto con alterazioni delle onde t . pacemaker la presenza di un pacemaker ( pm ) cardiaco ha accompagnato lo sviluppo della rm negli anni fin da subito come controindicazione assoluta , in grado di porre a rischio la vita del paziente . 
negli anni 80 [ 16 ] studi su animali e studi in vitro avevano in effetti documentato il rischio di malfunzionamento del pacemaker ; a questi dati sperimentali inoltre si deve aggiungere che in letteratura sono stati riportati almeno 10 decessi dovuti a introduzione in sala rm di pazienti con pm . 
le principali considerazioni sulla sicurezza di questi dispositivi sono state elicitate per la prima volta in modo strutturato nella review di mathur - de vre , nel 1987 [ 17 ]  . 
stando a tale controindicazione , una quota sempre maggiore di popolazione , calcolato ad oggi in alcuni milioni di persone , non potrebbe essere sottoposta ad una risonanza magnetica , pur in presenza di patologia neurologica , neurochirurgica od oncologica , oppure di patologie non life - threatening ma molto diffuse nella popolazione come le patologie muscolo - scheletriche , per le quali la rm rappresenta lesame maggiormente diagnostico . tuttavia , negli ultimi anni , studi effettuati in situazioni di reale urgenza su pazienti portatori di stimolatore cardiaco sottoposti a risonanza magnetica , unitamente al progressivo sviluppo tecnologico dei pacemaker , hanno gradualmente modificato questi concetti . 
lo sviluppo tecnologico dei pm , a partire dal 1996 , porta ad una netta riduzione della quota di materiale ferro - magnetico allinterno degli stimolatori cardiaci ; la riprogettazione dellarchitettura elettronica e della programmazione , la riduzione della distanza tra gli elettrodi e il cambiamento dei materiali ( una lega con minor suscettibilit magnetica mp35n ) hanno ridotto la sensibilit alle interferenze elettromagnetiche [ 18 ]  . gli effetti noti della risonanza magnetica sui pacemaker cardiaci derivano dal campo magnetico statico ( cm ) , dal campo di radiofrequenza temporaneo ( rf ) e dai gradienti ( campi magnetici addizionali ) e sono esposti nella tabella 2 . certamente a livello clinico la complicanza potenziale pi importante da temere il decesso del paziente . 
in one in vivo study using 0.5 - t magnets , sommer describes 18 patients in whom the only recorded effect was that of the passage to the asynchronous mode [ 24 ]  . 
 in this regard , a checklist of recommendations has recently been proposed to be used when an mr examination is scheduled for patients bearing a pm [ 25 ]  . 
this was originally considered a relative contraindication but has since proved not to be insofar as studies have shown the absence of cardiac symptoms and no effects on the ecg [ 26 ]  . however , metallic endocardial guides have not yet been shown to be innocuous . furthermore , it is less dangerous to carry out the examination in a different area possibly far from the heart ( such as the head or distal joints ) , as this reduces the effects on the pm because the magnetic isocentre is shifted to the area of study . 
together with the use of coils that work as both receivers and transmitters , this certainly reduces the effect of the rf field , which is at its greatest in the isocentre . all of the above has led to the development of special low - field magnets such as those dedicated to the study of distal joints . 
in this case , the thoracic effects of the magnetic and rf fields are minimal because only the limb is inserted inside the magnet , and there is no absolute contraindication to examining patients with pms [ 27 ]  . 
 implantable cardioverters / defibrillator ( icds ) in addition to the problems raised by pms , icds also have problems of their own involving ( 1 ) batteries and ( 2 ) sensito , che si sono sottoposti a esame rm , tutti per senza monitoraggio o precauzioni allingresso [ 23 ] e soprattutto senza che fosse stata valutata la dipendenza o meno del ritmo cardiaco dal pm . in letteratura per sono presenti da tempo anche articoli riguardanti studi rm su pazienti con pacemaker , senza che vengano riportati decessi , n complicanze . 
si tratta purtroppo spesso di studi o reports abbastanza disomogenei , sia per la selezione del paziente che per il tipo di studio rm condotto . vari studi hanno dimostrato come sempre a basso campo non si osservino effetti sullattivit del pm , quando questo sia spento o posto in modalit asincrona . 
questa che era considerata una controindicazione relativa si poi rivelata non reale , in quanto vi sono studi che hanno dimostrato lassenza di sintomi cardiaci o effetti sullecg [ 26 ]  . 
non vi sono invece dimostrazioni di innocuit a carico di guide metalliche endocardiche . risulta inoltre meno pericoloso condurre lesame su una zona diversa e possibilmente lontana dal cuore , come la testa o le articolazioni distali , perch si riducono gli effetti magnetici sul pm dal momento che lisocentro magnetico risulta spostato nellarea di studio e questo , insieme allutilizzo di bobine che funzionino sia in trasmissione che in ricezione , riduce sicuramente leffetto del campo di rf , che massimo allisocentro . questo ha portato allo sviluppo di particolari magneti a basso campo come quelli dedicati allo studio delle articolazioni distali , per i quali gli effetti del cm e delle rf a livello del torace sono minimi , in quanto si inserisce solo larto nel piccolo magnete ; in tale condizione non vi una cona . 
it happens in the case of 1 - mt ( 10 gauss ) fields , which is why it is recommended not to exceed 5 gauss when examining patients bearing pms [ 19 ]  . 
the magnetic responsiveness of the latest - generation pms can be deactivated in such a way as to maintain the synchronous mode batteries and reed switches contain ferromagnetic parts and can theoretically be dislocated by the mf ( which is minimum at the isocentre and increases with the distance from it ) and the torsion ( which is maximum at the isocentre )  . 
as the direction of the b0 of closed magnets is often parallel to the axis of the patient , when a patient is lying down , the pm is also aligned with the torsion . 
however , when a patient enters the magnet room on foot , the torsion ( which tends to align paramagnetic structures with the axis of the mf ) is at its maximuin the past , patients were asked to wear an elastic pressure bandage over the pectoral pocket in order to reduce mobilisation of the device . 
the electrodes are made of an alloy ( mp35n ) that includes nickel , cobalt , chrome and molybdenum and are therefore not ferromagnetic ( c ) electrocardiogram ( ecg ) variations polarised blood flow acts as a conductor and can cause electrical alterations by superimposing electrical potentials on surface ecg measurements , thus increasing the t wave ; however , this is not very relevant insofar as the p and r waves do not seem to be affected 2 . 
temporary radiofrequency ( rf ) field ( a ) heating . the presence of instruments with electrical conduction characteristics can amplify the local electrical field and make it difficult to predict peak specific absorption rate ( sar )  . 
in this way , it is possible that thermal damage occurs at the ends of the stimulating electrodes and therefore at the interface between the myocardium and the point of the electrode . 
this phenomenon does not occur in wide and compact metal structures such as the pm generator , but it is observed in the stimulating electrodes , even when they are disconnected or insulated [ 20 ] ( b ) altered stimulation rhythm this happens because of direct interference with the pm electronics or because the induction of currents above the activation threshold of the atrial electrode activates ventricular stimulation ( c ) pm reprogramming or resetting called phantom programming , the spontaneous reprogramming of the pm during examination occurred in the past , but current pms have safety controls that prevent it from happening 3 . 
variable field gradients over time ( a ) induced voltages ( b ) reed switch these are possible insofar as the gradients are local mfs that vary rapidly over time , but the induced currents are below the threshold of excitability for cardiac fibrillation ( between 100 and 1000 a / cm2 )  . 
in 1993 , lauck postulated that it was not the stimulation capacity of the device that was affected but the detection of the autochthonous rhythm insofar as this current could be mistaken for pulsation . 
even the most recent icds can give rise to difficulties due to magnetic torsion , the forces of which have been measured in vitro [ 29 ] and found to be above the threshold for clinical detection . 
furthermore , icds are more sensitive than pms : e.g. they can be induced to recognise a ventricular tachyarrhythmia that does not exist , automatically provide the defibrillation to treat it , and thus actually cause a ventricular tachyarrhythmia which may even go unrecognised because the mfs can prevent its detection . 
effetti del cm ( a ) chiusura / apertura del reed - switch determina il passaggio da modalit sincrona , cio on demand , a modalit asincrona , con un ritmo ( b ) dislocazione del pacemaker ( c ) variazioni nellelettrocardiogramma 2 . 
effetti del campo di radiofrequenza temporaneo ( rf ) ( a ) riscaldamento pre - fissato e potenziale competizione con il ritmo di base del cuore . avviene per campi di 1 mt ( 10 gauss ) e da qui nasce la raccomandazione di non fare superare la linea dei 5 gauss ai pazienti portatori di pm [ 19 ]  . nei pm di ultima generazione possibile disattivare la responsivit magnetica e mantenere quindi la modalit sincrona . le batterie e i reed - switch contengono parti ferro - magnetiche e possono teoricamente essere dislocate dalla forza magnetica ( minima allisocentro e incrementante allontanandosi da esso ) e dalla forza di torsione ( massima a livello dellisocentro )  . dal momento che i magneti di tipi chiuso hanno spesso la direzione del b0 parallela allasse del paziente , il pm , a paziente sdraiato , si trova allineato anchesso nei confronti della forza di torsione ; quando il paziente invece entra nella sala magnete , ed in piedi , la forza di torsione che tende ad allineare le strutture paramagnetiche allasse del cm , risulta invece massima . 
questo fenomeno non avviene in strutture metalliche compatte , larghe , come il generatore del pacemaker , mentre si osserva negli elettrodi stimolatori , anche quando disconnessi o isolati [ 20 ]  . ( b ) alterazione del ritmo di stimolazione questo fenomeno avviene o per interferenza diretta con lelettronica del pacemaker , o per induzione di correnti sopra la soglia di attivazione dellelettrodo striale , attivando una stimolazione ventricolare . ( c ) riprogrammazione o resettaggio si chiama programmazione fantasma e si tratta di una riprogrammazione spontanea del dispositivo durante lesame rm . 
effetti dei gradienti di campo variabili nel tempo ( a ) voltaggi indotti sono possibili in quanto i gradienti sono campi magnetici locali rapidamente variabili nel tempo , ma le correnti indotte sono sotto la soglia di eccitabilit per la fibrillazione cardiaca ( nel range tra 100 e 1000 a / cm2 )  . lauck nel 1993 ha postulato che non ne venga affetta la capacit di stimolazione del dispositivo ma quella di riconoscimento del ritmo autoctono , in quanto tale corrente potrebbe essere scambiata per pulsazione . 
tale fenomeno sarebbe pi probabile nei pm monopolari [ 21 ]  . ( b ) reed - switch apertura e chiusura con il variare dei gradienti . rf waves the main biological effects associated with exposure to rf fields are due to their thermogenic properties because at the frequencies used for clinical purposes , some of the absorbed energy is converted into heat . 
the heat is caused by the enattualmente i pi recenti icd possono porre problematiche per le forze di torsione magnetica , che sono state misurate in vitro [ 29 ] e risultano oltre che misurabili anche sopra la soglia di riconoscimento clinico . 
the specific absorption rate ( sar , expressed in watts / kilogram ) was introduced in an attempt to limit bodily exposure to the rf field , and modern mr machinery is equipped with an sar self - limiting systeheating is less with low - field 0.5 - t magnets than with 1.5 - t magnets because the absorption is proportional to the frequency of the rf field . 
a 5 - min pause between sequences can allow total dissipation of the heat , and the use of sequences that involve a rapid switch from one gradient to another ( such as gradient recalled echo ) should be limited . automaticamente fornire il trattamento di defibrillazione , inducendo cos realmente una tachiaritmia ventricolare , che tra laltro potrebbe non essere riconosciuta in quanto i campi magnetici possono anche prevenire il suo riconoscimento . gli effetti biologici principali associati allesposizione a campi di rf sono dovuti alle caratteristiche termogeniche del campo rf . 
il riscaldamento causato dallenergia trasmessa dallimpulso rf che genera un campo elettrico che a sua volta induce correnti elettriche ; tali correnti possono determinare riscaldamento . per limitare lesposizione del corpo al campo rf stato introdotto il sar , specific absorption rate , espresso in watt per kg . 
il fenomeno del riscaldamento minore in magneti a basso campo ( 0 , 5 t ) rispetto a magneti da 1 , 5 t dal momento che lassorbimento di potenza proporzionale alla frequenza del campo rf ; il sar varia a seconda della sequenza utilizzata ; alcune sequenze , come le gradient echo ad esempio , hanno un sar minore di altre ( spin echo )  . 
una pausa di 5 minuti tra una sequenza e la successiva pu permettere la totale dissipazione del calore ; andrebbe limitato luso delle sequenze che comportino un veloce switch tra i gradienti ( come le gradient - recalled echo )  . le ustioni in genere sono causate dallintroduzione di materiale elettrico conduttivo allinterno del magnete . 
tipici oggetti che teoricamente possono scaldarsi per effetto di questi fenomeni sono gli elettrodi per ecg , i cavi del pulsossimetro , gli accessori rm ( estremi di bobine rf ) in contatto con la superficie cutanea del paziente , ma anche ( anche se con danni minori ) tatuaggi ricchi di pigmento a base di ossido ferroso . linduzione di correnti elettriche pu anche di per se stesso essere un pericolo potenziale per linterazione con altri dispositivi , ma non per impianti bio - medicali passivi . la recente diffusione del piercing a scopo decorativo o rituale un fenomeno da considerare prima di sottoporre un paziente ad esame di rm . 
il piercing pu mobilizzarsi o surriscaldarsi durante lesame rm e causare danni variabili in rapporto alla massa delloggetto , alla sua sede e alle sue propriet ferromagnetiche ; il piercing andrebbe dunque rimosso prima dellesame rm . 
se ci non possibile o se il paziente rifiuta di rimuoverlo , il paziente va informato dei potenziali rischi cui va incontro sottoponendosi allesame e vanno applicati dispositivi ( cerotti o bendaggi ) per stabilizzare loggetto . 
typical objects of this kind are ecg electrodes , the cables of pulse oximeters , and mr accessories ( such as the ends of rf coils ) , which may come into contact with a patients skhowever , such objects also ( albeit with less damaging effect ) include tattoos rich in iron - oxide - based pigments . 
the induction of electrical currents can per se be a potential danger because of their interactions with other devices , but not passive biomedical implants . the recent spread of decorative or ritual piercings is something that needs to be considered before submitting a patient to an mr examination , as the jewellery may contain nonferromagnetic metals , ferromagnetic metals or even nonmetallic materials . 
if this is not possible , or the patient refuses , he or she should be informed of the potential risks and the objects should be held firm by means of a adhesive plaster or bandage . 
to prevent burns , insulating material ( bandage or adhesive tape ) should be placed between the object and the underlying skin , and patients should also be told to inform the operator if they feel any sensation of heat at the site of the piercing or feel the object move during the examination [ 30 ]  . mr is frequently used to examine the head , neck , limbs and other anatomical regions that are common sites of tattoos . 
both permanent tattoos and cosmetics ( especially mascara and other makeup made using black pigments ) contain particles of iron oxides or other metals that , by interacting with the mf , can cause sensations of heat , pins and needles , swelling or local irritation during an examination [ 31 , 32 ]  . 
radiologists should check whether patients have any permanent tattoos before beginning the examination and , although it is not a contraindication , patients should be warned of the possible side effects and told to inform the operator if they feel any sensation of heat at the site of the tattoo . 
any cosmetic containing iron oxides or other ferromagnetic metals should be removed before starting an mr examination . permanent contraceptive devices the presence of metallic contraceptive devices could cause damage due to overheating or displacement and can generate artefacts that may reduce the diagnostic accuracy of the examination . 
the results of various studies indicate that these devices are safe when pala rm una metodica di imaging frequentemente utilizzata nello studio della testa , del collo , degli arti e di altre regioni anatomiche che sono comune sede di tatuaggi . 
sia tatuaggi permanenti che cosmetici ( in particolare mascara e altri trucchi con pigmenti neri ) contengono particelle di ossidi di ferro o di altri metalli che , interagendo con il campo magnetico , possono provocare sensazioni di calore , formicolii , gonfiore , irritazione locale durante lesecuzione dellesame rm [ 31 , 32 ]  . 
il medico radiologo deve verificare se il paziente che sta per sottoporre ad esame rm portatore di tatuaggi permanenti ; in caso affermativo ci non costituisce controindicazione allesecuzione dellindagine , tuttavia il paziente deve essere avvisato dei possibili effetti collaterali e invitato a segnalare alloperatore eventuali sensazioni di calore nella sede del tatuaggio . 
i cosmetici contenenti ossidi di ferro o altri metalli ferromagnetici andrebbero rimossi prima dellesecuzione dellesame rm . dispositivi contraccettivi permanenti la presenza di un dispositivo contraccettivo metallico potrebbe causare danni dovuti al surriscaldamento delloggetto o alla mobilizzazione dello stesso e pu generare artefatti che possono ridurre laccuratezza diagnostica dellesame di rm . gli iud ( intra - uterine devices ) sono dispositivi contraccettivi intrauterini che possono essere costituiti interamente di materiale non metallico ( plastica ) o di materiali non metallici con componenti metalliche ( tipicamente il rame il metallo utilizzato )  . 
i risultati di diversi studi indicano che questi dispositivi sono sicuri per i pazienti esaminati con magneti da 1 , 5 t o inferiori [ 35 , 36 ]  . 
le parti metalliche possono generare artefatti che sono tuttavia poco significativi considerando la bassa suscettivit magnetica del rame e le dimensioni relativamente piccole degli iud . recentemente stato sviluppato un nuovo dispositivo metallico per la contraccezione permanente chiamato essure ( conceptus , san carlos , usa ) , costituito da una microspirale posizionata nella porzione prossimale delle tube di falloppio ove induce una risposta tissutale di tipo fibrotico che determina lancoraggio del dispositivo e locclusione tubarica . 
la sicurezza dellessure stata valutata da shellock [ 37 ] utilizzando un magnete da 1 , 5 t ( general electric medical systems , milwaukee , wi ) mediante un test ex - vivo noto come test dellangolo di deflessione e misurando con un termometro rm - compatibile le variazioni di temperatura del dispositivo inserito in un fantoccio ( riempito con un gel semisolido ) forgiato in modo da simulare il tronco umano . 
essure is made of stainless steel , platinum , iridium , nickel - titanium , silver and polyethylene fibres , and its safety has been evaluated by shellock [ 37 ] , who used a 1.5 - t magnet ( general electric medical systems , milwaukee , wi , usa ) in an ex vivo deflection angle test and an mr - compatible thermometer to measure the variations in temperature of a device inserted into a dummy filled with a semisolid gel and modelled in such a way as to simulate a human trunk . 
the study revealed no interactions between essure and the mf ( deflection angle : 0 ) , and the maximum thermal variation during the examination was 0.6c , which can be sustained by human tissue and is therefore innocuous . 
the generated artefacts ( essentially a signal blank that was more extended in gradient - echo than in t1 - weighted spin - echo sequences ) would only be a problem if the area to be examined were directly adjacent to the implanted device . 
as far as is currently known , essure does not represent a risk for patients bearing it , and they can safely be examined using magnets of 1.5 t or less [ 37 ]  . most diaphragms used for contraceptive purposes contain metal rings to keep them in position , some of which are made of ferromagnetic materials and are therefore strongly attracted by the static mf ( at least of the 1.5 - t magnets used for the studies )  . 
however , it has been observed ( shellock unpublished data , 1996 ) that patients wearing them do not perceive any disturbance and , in particular , have not reported any sensation of heat or displacement during the examination . 
in brief , the presence of a diaphragm should not be considered a contraindication to an mr examination involving magnets of 1.5 t or less [ 3840 ]  . gradients gradients can cause neuromuscular stimulation , particularly in areas where soft tissue and bone are close together ( anatomical margins and angles such as the elbow , iliac crest , greater trochanter , etc . ) , because the difference in impedance leads to the accumulation of electricity and thus lowers the threshold of nervous excitability . 
the consequences are shocks and paresthesias which , however , do not leave sequelae and so do not need to be considered a real risk for patients . noise is generated by the gradients . 
in the presence of a fixed mf , rapid changes in current give rise to lorentz noise variazione termica durante lesame stata di 0 , 6c , sostenibile dai tessuti umani e quindi innocua . 
gli artefatti generati ( essenzialmente vuoto di segnale , pi esteso nelle sequenze in echo di gradiente rispetto alle spin echo t1 - pesate ) non costituiscono un problema a meno che larea oggetto dello studio rm non sia strettamente limitrofa al dispositivo impiantato . 
allo stato attuale delle conoscenze lessure non rappresenta un rischio per le pazienti ed sicuro sottoporre ad esame rm con magneti da 1 , 5 t o inferiori pazienti che ne siano portatrici [ 37 ]  . la maggior parte dei diaframmi utilizzati per la contraccezione contengono anelli metallici che mantengono in sede il dispositivo . 
alcuni di questi anelli metallici sono fatti di materiali ferromagnetici e vengono dunque fortemente attratti dal campo magnetico statico ( studi condotti su magneti da 1 , 5 t )  . stato comunque osservato ( shellock dati non pubblicati , 1996 ) che pazienti portatrici di diaframmi sottoposte ad esame rm non percepivano alcun disturbo , e in particolare non riferivano senso di calore n avvertivano sensazioni di movimento del dispositivo durante lesame . 
in definitiva , la presenza di diaframma non deve essere considerata una controindicazione allesame di rm su magneti da 1 , 5 t o inferiori [ 3840 ]  . gradienti i gradienti possono determinare stimolazione neuro - muscolare , in particolare in aree di maggior vicinanza tessuto molle tessuto osseo ( bordi e spigoli anatomici , come gomito , cresta iliaca , grande trocantere ecc ) dove si verifica per differenza di impedenza elettrica un accumulo elettrico , con conseguente abbassamento della soglia di eccitabilit nervosa e conseguente stimolazione nervosa . 
ne conseguono parestesie o scosse , che comunque sono temporanee e non lasciano reliquati ; questi effetti non sono pertanto da considerarsi un reale rischio per il paziente . rumore il rumore viene generato dai gradienti ; le rapide variazioni di corrente infatti , in presenza del campo magnetico fisso , sviluppano forze di lorentz , che , mettendo in vibrazione le strutture delle bobine stesse producono i tipici rumori di tamburellamento a bassa tonalit , knocking . 
il rumore pu causare disturbi variabili dal semplice fastidio fino alla perdita temporanea o permanente delludito ; gli effetti sono maggiormente significativi se il paziente anziano , psichiatrico o sotto terapia farmacologica ototossica , oppure nel caso del feto o del neonato , in cui limmaturit dellorecchio interno pu comportare un maggior rischio di lesione permanente . il rumore generato dipende dal tipo di sequenze ( le fast gradient , turbo spin echo e le echo planar sono le pi rumorose ) e dai parametri delle stesse ( sezioni sottili , fov piccoli e short tr and et )  . 
il potenziale rischio di noxa acustica pu essere controllato facendo indossare sempre le cuffie forces that , by making the structures of the coils vibrate , produce the typically deep noises of knocking that may even reach 115 db , whereas the limit threshold is 90 db . 
the effects are more significant if the patient is elderly , suffering from a psychiatric disorder or receiving ototoxic drug therapy , or in the case of a foetus or new born in whom the immaturity of the inner ear may lead to greater risk of a permanent lesion . the generated noise depends on the type of sequences ( the noisiest are fast gradient , turbo spin - echo and echo planar sequences ) and their parameters ( thin sections , small fov , short tr and et )  . 
the risk of hearing damage can be controlled by always having the patients wear earmuffs or earplugs ; when examining a foetus or new born , there are special sequences ( often supplied by the manufacturer of the mr equipment ) that reduce peak noise levels at the expense of greater sequence length . mr during pregnancy and postpartum technological developments over the last 20 years have made it possible to use mr to examine foetuses because the introduction of fast and ultrafast sequences has overcome the problem of artefacts due to foetal movement . 
the largest field of application for foetal mr is neurological imaging , because it is used not only to assess cerebral development [ 4348 ] but also as a means of diagnosing central nervous system diseases [ 49 ] ( agenesia of the corpus callosum [ 50 ] , hydrocephalus [ 51 ] , cerebral ischaemia [ 52 ] , neural tube defects [ 53 ] , schizencephaly [ 54 ] and abnormalities of the posterior cranial fossa [ 55 ] ) ; however , mr is now also used to study other foetal anatomical districts , such as the lungs [ 56 ] , liver [ 57 ] , neck [ 58 ] and urogenital system [ 59 ]  . foetal exposure the following are circumstances that can lead to a foetus being exposed to the biological effects of the static mfs and gradients : a pregnant patient agrees to undergo an mr examination being unaware of her condition a pregnant patient requires a diagnosis that only mr can direct mr visualisation of the foetus is necessary to clear up diagnostic doubts after ultrasound screening a pregnant woman is enrolled as a volunteer in a research protocol . it has also recently been demonstrated that mr is useful in evaluating the condition and functioning of the placenta a . 
sebbene limaging neurologico sia il pi vasto campo di applicazione della rm fetale , sia per la valutazione dello sviluppo cerebrale [ 4348 ] che per la diagnosi di patologie del sistema nervoso centrale [ 49 ] ( agenesie del corpo calloso [ 50 ] , idrocefalo [ 51 ] , ischemia cerebrale [ 52 ] , difetti del tubo neurale [ 53 ] , schizencefalia [ 54 ] , anormalit delle strutture della fossa cranica posteriore [ 55 ] ) , la rm viene oggi impiegata anche nello studio di altri distretti anatomici fetali quali i polmoni [ 56 ] , il fegato [ 57 ] , il collo [ 58 ] , il sistema uro - genitale [ 59 ]  . esposizione fetale lesposizione fetale agli effetti biologici del campo magnetico statico e di gradienti di campo pu avvenire nelle seguenti circostanze : la paziente , non consapevole di essere incinta , sottoposta ad esame rm ; la paziente , in stato di gravidanza , necessita una diagnosi che solo la rm pu fornire ; la diretta visualizzazione del feto mediante la rm pu essere necessaria per dirimere dubbi diagnostici dopo screening ecografico ; donne volontarie in gravidanza arruolate in protocolli di ricerca . stato inoltre recentemente dimostrato che la rm utile nella valutazione delle condizioni e della funzionalit della placenta [ 60 , 61 ] , del volume di liquido amniotico [ 62 ] e delle variazioni del flusso sanguigno cerebrale in gravidanza [ 63 , 64 ]  . molto difficile stabilire i rischi fetali derivanti dallesposizione di donne incinte in rapporto alla variabilit dellintensit dei campi magnetici , dei gradienti e delle sequenze di impulsi di radiofrequenza utilizzati nei diversi centri nella pratica clinica quotidiana . provide rischi per il feto a . 
however , it is still not clear what foetal damage can be caused by exposure to static mfs and field gradients , and most of the available data come from experimental animal studies . 
exposed chicken embryos to different static mfs and field gradients whose intensity varied over time and observed no effect on embryonal mortality , hatching rate or viability of the chicks [ 66 ]  . 
obtained no statistically significant data demonstrating any effects of prolonged exposure to 4 - t mfs on the foetal growth or postnatal development of exposed mice [ 68 ]  . 
found no statistically significant differences in the rate of uterine growth between a group of 74 pregnant women undergoing mr and a control group of 148 unexposed women [ 70 ]  . 
studies of humans have shown that an increase in embryonal temperature of 2c for more than 24 h can cause neural tube defects and craniofacial deformations [ 71 ]  . 
however , it has been established by law that magnet rooms must be equipped with cooling systems capable of maintaining an ambient temperature of less than 24c with less than 60% humidity . i campi magnetici statici utilizzati nella routine clinica vanno da 0 , 2 a 2 t , centri specialistici utilizzano campi a 3 t e in alcuni centri di ricerca vengono impiegati campi magnetici dellintensit di 8 t . 
tuttora non vi chiarezza sui danni fetali derivanti dallesposizione a campi magnetici statici e a gradienti di campo e i dati che possediamo derivano prevalentemente da studi sperimentali su animali . 
 [ 65 ] hanno riscontrato effetti embriotossici su topi esposti durante la fase centrale della gravidanza ad un campo magnetico dellintensit di 0 , 35 t , behr et al . 
 [ 66 ] hanno esposto embrioni di pollo a differenti campi magnetici statici e a gradienti di campo di intensit variabile nel tempo e non hanno osservato alcuna influenza sulla mortalit embrionaria , sul tasso di schiusura delle uova e sulla vitalit dei polli . 
 [ 68 ] non hanno ottenuto dati statisticamente significativi che dimostrassero effetti dellesposizione prolungata a campi magnetici di 4 t sulla crescita fetale e sullo sviluppo post - natale di topi esposti . 
 [ 69 ] in particolare non hanno riscontrato un incremento della morbilit a 3 anni in 20 bambini studiati in utero con rm a 0 , 5 t , analogamente myers et al . 
 [ 70 ] non hanno osservato differenze statisticamente significative nella velocit di crescita uterina tra un gruppo di 74 donne incinte sottoposte ad esame rm ed un gruppo di controllo di 148 donne non esposte . 
occorrono ulteriori trials clinici su pi vasta scala campionaria per determinare il reale effetto dellesposizione a campi elettromagnetici e onde di radiofrequenza sullo sviluppo endouterino . danno termico lesposizione fetale a radiofrequenze si traduce in un aumento della temperatura corporea che potenzialmente dannoso . 
studi su esseri umani hanno stabilito che un aumento della temperatura embrionale di 2c per pi di 24 ore pu determinare difetti del tubo neurale e deformazioni cranio - facciali [ 71 ]  . 
it has been demonstrated that the foetal hearing apparatus suffers from loud noises ; in particular , if pregnant women remain in very noisy environments ( > 99 db ) , this can shorten the pregnancy , lead to low birth weight and cause foetal hearing loss [ 72 ]  . 
noise intensity is proportional to mf intensity , varying from about 75 db in the case of a field of 0.2 t up to 115 db in a field of 3 t [ 73 ]  . 
some researchers have tried to establish the degree to which the maternal abdomen attenuates the noise by introducing a microphone into the stomach of a male volunteer , but this experimental model does not faithfully reproduce the foetus in all pregnancy phases [ 74 ]  . further human safety studies are needed to clarify the real risks of using mr in the early phases of pregnancy and so , as things stand , it is ethically correct to avoid undertaking mr examinations during the first trimester except in the case of an diagnostic - therapeutic urgency that cannot be delayed . given the current state of knowledge , it is deontologically and ethically correct to limit embryo / foetal exposure and therefore the indications for mr in the case of a pregnant patient to : 1 . 
the presence of neurological , neurosurgical or oncological diseases affecting the mother . use of paramagnetic contrast media during pregnancy contrast media containing gadolinium cross the placental barrier in humans and animals [ 75 ] ; however , there are no published descriptions of teratogenic or mutagenic effects on the foetus related to the administration of paramagnetic contrast media in pregnant women . 
there is , however , a reservation arising from the scientific observation that once excreted by foetal kidneys , the chelate of gadolinium remains in the amniotic fluid and is ingested through the gastrointestinal tube and re - excreted numerous times : the persistence of the molecule in a closed compartment such as the fetoplacental system could lead to the dissociation of the gadolinium ion ( which is toxic per se ) from the chelate , thus giving rise to a risk of toxicity that is still not fully known . on the basis of the above considerations , a paramagnetic contrast medium could theoretically be administered to pregnant women even though , in practical terms , it is better not to inject it unless it is absolutely necessary . 
stato dimostrato che lapparato uditivo fetale soffre il forte rumore ; in particolare la permanenza di donne in gravidanza in ambienti molto rumorosi ( > 99 db ) pu provocare accorciamento della gravidanza , basso peso alla nascita e perdita delludito nel feto [ 72 ]  . 
lintensit del rumore proporzionale allintensit del campo magnetico e in particolare varia da circa 75 db per un campo di 0 , 2 t fino 115 db in un campo dellintensit di 3 t [ 73 ]  . 
alcuni ricercatori hanno cercato di stabilire il grado di attenuazione del rumore da parte delladdome materno introducendo un microfono nello stomaco di un volontario di sesso maschile ; questo modello sperimentale non riproduceva per fedelmente il feto in tutte le fasi della gravidanza [ 74 ]  . occorrono ulteriori studi di sicurezza sulluomo per fare chiarezza sui reali rischi dellimpiego della rm nella prime fasi della gravidanza per cui , allo stato attuale delle nostre conoscenze , eticamente corretto evitare di effettuare esami di rm nel primo trimestre di gravidanza in assenza di una improcrastinabile urgenza diagnostico - terapeutica . 
a patologie della madre in ambito neurologico , neurochirurgico od oncologico . uso di mezzi di contrasto paramagnetici durante la gravidanza mezzi di contrasto contenenti gadolinio attraversano la barriera placentare sia nelluomo che nellanimale [ 75 ] ; tuttavia non sono descritti in letteratura effetti teratogeni o mutageni sul feto legati alla somministrazione di mezzi di contrasto paramagnetici a donne incinte e studi effettuati su animali non hanno documentato teratogenicit o effetti sullo sviluppo post - natale dopo somministrazione di gadopentato dimeglumina , gadoteridolo , gadobenato dimeglumina o gadoversetamide [ 7679 ]  . 
tuttavia vi una riserva che nasce dalla constatazione scientifica che il chelato di gadolinio una volta escreto dai reni fetali nel liquido amniotico , rimanendo in quel comparto viene ingerito nel tubo gastrointestinale e riescreto , numerose volte : la persistenza della molecola in un comparto chiuso come il sistema feto - placentare potrebbe portare alla dissociazione dello ione gadolinio ( di per s tossico ) dal chelato con un rischio di tossicit non del tutto noto . in base a tali considerazioni in linea teorica potrebbe essere somministrato mezzo di contrasto paramagnetico a donne incinte , anche se dal punto di vista pratico meglio mantenere un atteggiamento conservativo e quindi non iniettarlo a meno che non sia assolutamente necessario . 
these considerations initially led to the suggestion that women undergoing an mr examination with the use of a paramagnetic contrast medium should stop breast feeding during the 24 h following its intravenous injection [ 83 ]  . 
however , more recent studies have shown that the amount of medium transferred via breast milk is more than 100 times less than the maximum intravenous gadolinium dose recommended for neonatal use . 
furthermore , the intestinal absorption of ingested gadolinium is extremely small ( 0.04%0.08% of the amount ingested ) , and the absorbed amount is rapidly excreted by the kidney [ 80 , 81 ]  . 
on the basis of these findings , we believe that breast feeding can be continued without reservation after the administration of paramagnetic contrast media to the mother . lalta risoluzione di contrasto per i tessuti molli e la multiplanariet hanno condotto ad un largo impiego della rm nel post - partu molte delle nuove applicazioni della rm richiedono lutilizzo di mezzo di contrasto paramagnetico cos che la prole di donne in allattamento diviene indirettamente potenziale destinataria di tale agente . 
sebbene la farmacocinetica dei mezzi di contrasto paramagnetici extracellulari sia simile a quella dei mezzi di contrasto iodati , essi sono caratterizzati da un profilo di sicurezza di gran lunga maggiore : le reazioni anafilattiche sono molto rare e non c evidenza di nefrotossicit . i mezzi di contrasto paramagnetici vengono filtrati ed eliminati dal rene ma anche la ghiandola mammaria pu contribuire , sebbene in piccola parte , allescrezione trasferendo cos , attraverso il latte materno , una piccolissima quantit di mezzo di contrasto paramagnetico ( 0 , 011%0 , 04% della dose totale di gd - dtpa )  . 
queste considerazioni hanno condotto in passato a suggerire alle donne sottoposte ad esami rm con mezzo di contrasto paramagnetico la sospensione dellallattamento durante le 24 ore seguenti liniezione endovenosa del mdc [ 83 ]  . pi recenti studi hanno tuttavia evidenziato che la dose di mezzo di contrasto paramagnetico trasferita al feto attraverso il latte materno pi di 100 volte inferiore alla dose endovenosa massima di gadolinio raccomandata per uso neonatale ; inoltre lassorbimento intestinale di gadolinio ingerito estremamente basso ( 0 , 04%0 , 08% di quello ingerito ) , e la quota assorbita viene rapidamente escreta dallemuntore renale [ 80 , 81 ]  . 
the aims of this study were to evaluate the association of testicular microlithiasis with testicular neoplasm , to assess the accuracy of ultrasonography ( us ) in comparison with histology in detecting microlithiasis , and to identify the prevalent cytohistological features that accompany testicular cancer . 
at us examination , testicular cancer was associated with microlithiasis in seven out of 13 patients ( 53.8% ) ( the distribution pattern of microlithiasis was intranodular in two , perinodular in two and both intraand perinodular in three ) , and colour - doppler us showed perinodular and intranodular vascularity . 
dal 2004 al 2005 , sono giunti alla nostra osservazione e sottoposti ad indagine ecografica 14 pazienti , di cui 13 operati per neoplasia maligna , di et compresa tra 19 e 43 anni e solo un caso di 60 anni . 
due pazienti ( 15 , 3% ) presentavano microlitiasi testicolare in precedente indagine ecografica e due pazienti ( 15 , 3% ) presentavano alterazioni dello spermiogramma . allindagine ecografica la neoplasia testicolare maligna nel 53 , 8% ( 7 / 13 ) era associata alla presenza di microlitiasi testicolare ( in 2 / 7 in sede intranodulare , in 2 / 7 in sede perinodulare e in 3 / 7 casi in sede peri - intranodulare ) e presentava vascolarizzazione peri ed intranodulare alleco color doppler . 
le microlitiasi testicolari e le alterazioni del liquido seminale rappresentano fattore di rischio nelle neoplasie maligne del testicolo : infatti , complessivamente , il 30 , 6% ha sviluppato una eteroplasia maligna . 
some authors have indicated incidences of 0.5%0.60% [ 1 , 2 ] , 0.68% [ 3 ] , 2% [ 4 ] , 5% [ 5 ] and 9% [ 6 ] , whereas for others [ 7 ] , the incidence cannot be determined as no studies have assessed the prevalence of microlithiasis in the general population . 
this discrepancy was found to be related to an incomplete analysis of the data collected because of unavailability of histological reports for some cases [ 8 ] or the use of us probes with frequencies less than 10 mhz [ 9 ]  . 
 opinions concerning the association between microlithiasis and testicular cancer are conflicting , with no mention of microlithiasis as a risk factor in recent reviews and no levels of evidence [ 10 , 11 ]  . 
tubular hyalinisation is the end stage of tubular atrophy and includes the absence of both germ cells and sertoli cells , with alterations of the lamina propria and leydig cells ; according to some authors , these changes may be detected histologically in the parenchyma adjacent to the neoplastic lesion [ 12 ] , leading to the hypothesis that testicular cancers arise in a predisposing environment . 
 materials and methods between 2004 and 2005 , 14 patients were referred to us for us examination , 13 of whom underwent surgery for testicular neoplastheir age ranged from 19 to 43 years , except for one patient aged 60 years . 
the us examination evaluated the number of testicular lesions , their echostructure , their vascularity with colourle microlitiasi testicolari ( mt ) sono unanomalia non frequente del parenchima testicolare rappresentata della presenza di depositi calcifici nei tubuli seminiferi e / o nellinterstizio . 
lincidenza stimata in letteratura appare molto variabile : per alcuni autori , intorno allo 0 , 5%0 , 60% [ 1 , 2 ] , allo 0 , 68% [ 3 ] , al 2% [ 4 ] , al 5% [ 5 ] al 9% [ 6 ] , mentre per altri [ 7 ] , non pu essere definita , in quanto non esistono lavori che valutano la prevalenza della mt nella popolazione generale . 
infatti , la maggior parte dei lavori esamina pazienti giunti allosservazione per patologia testicolare e non risulta mai essere stata effettuata indagine di screening . in letteratura , risultano rari gli articoli che correlano il reperto ecografico di mt col rilievo istologico . 
da alcuni autori riportata la discrepanza esistente fra levidenza ecografica e il riscontro istologico di mt [ 7 ] : tale dato risult gravato da una incompleta analisi dei dati raccolti per la mancata disponibilit , in alcuni casi , del reperto istologico [ 8 ] o dallutilizzo di sonde ecografiche con frequenze inferiori a 10 mhz [ 9 ]  . 
recentemente , lutilizzo di sonde ad elevata frequenza e la maggior sensibilizzazione di radiologi ed urologi a questa problematica ha incrementato il rilievo dellincidenza della mt . allo stato attuale , le opinioni in merito allassociazione fra mt e neoplasia testicolare maligna ( ntm ) sono divergenti , in quanto le mt non vengono citate come fattore di rischio in recenti revisioni di letteratura e non vi sono livelli di evidenza riguardo queste [ 10 , 11 ]  . 
la scleroialinosi dei tuboli seminiferi ( sct ) rappresenta lo stadio terminale dellatrofia tubulare ed include lassenza sia delle cellule germinali che delle cellule di sertoli , con alterazioni della lamina propria e delle cellule di leydig ; detta alterazione , per alcuni autori , pu essere riscontrata istologicamente nel tessuto parenchimale adiacente la lesione neoplastica [ 12 ] , prospettando lipotesi che la ntm insorga su un terreno predisposto . lo scopo del lavoro stato quello di analizzare se esistono correlazioni fra la mt e le ntm , valutando , inoltre , laffidabilit dellecografia nel rilevare la microlitiasi rispetto lesame istologico . materiali e metodi dal 2004 al 2005 , sono stati sottoposti ad indagine ultrasonografica con ecografo hitachi h21 ( kashiwa , giappone ) , sonda lineare da 7 , 512 mhz , con modulo color e power doppler , 14 pazienti , di cui 13 operati per ntm , di et compresa tra 19 e 43 anni e un solo paziente di 60 anni . 
1a - c ultrasound ( us ) scan of the testis performed on 27 january 2004 shows microlithiasis in a 38 - year - old patient ( a )  . 
1a - c comparsa di neoplasia seminomatosa in pregressa microlitiasi testicolare : ( a ) il 27 / 1 / 2004 rilievo ecografico di mt in paziente di 38 anni ; ( b ) il 25 / 8 / 2005 comparsa di lesione sospetta per ntm in paziente con pregresso riscontro di mt ; ( c ) rilievo istologico di ntm e mt . per criteri di benignit della lesione , stata eseguita nodulectomia . 
allindagine ecografica si posta lattenzione nel definire il numero delle lesioni testicolari , lecostruttura , la vascolarizzazione con eco color e power doppler e la presenza di mt nella lesione eteroplastica o nel parenchima testicolare adiacente alla neoplasia . 
lesame istologico , oltre a fornire la diagnosi definitiva del tipo istologico in esame , ha ricercato la presenza di mt nel focolaio neoplastico o nel parenchima testicolare esaminato , nonch eventuali alterazioni nel parenchima circostante la ntm . risultati i sintomi di esordio che hanno indotto i pazienti ad eseguire la visita urologica e lesame ecografico sono stati : in 6 dolore scrotale , in 4 la comparsa di tumefazione intrascrotale , in 2 la comparsa di localizzazioni secondarie ( in 1 paziente adenopatia sovraclaveare e in 1 paziente lesioni polmonari ) e in 2 pazienti alterazioni dello spermiogramma ed infertilit . 
besides providing a definitive diagnosis for histological type of lesion , histology aimed to detect the presence of microlithiasis within the neoplasm or in the testicular parenchyma being examined , as well as in the parenchyma surrounding the testicular cancer . results the presenting symptoms leading to consultation of a urologist and us examination were scrotal pain in six patients , intrascrotal swelling in four , the development of secondary localisations in two ( supraclavicular adenopathy in one and pulmonary lesion in the other ) and altered sperm function and infertility in two . 
in nessuno dei pazienti erano presenti segni di ostruzione delle vie seminali e nel 53 , 8% ( 7 / 13 ) dei pazienti con ntm erano presenti mt rig.c. 
la neoplasia benigna , operata di nodulectomia , non presentava allindagine ecografica mt , dato confermato successivamente dal reperto istologico che non evidenzi neanche scleroialinosi nel tessuto adiacente alla neoplasia . allesame istologico , 9 casi erano seminomi , 2 casi forme miste , 1 caso carcinoma embrionario , 1 caso tumore del sacg.c. 
6a , b seminoma con mt in sede intraed extranodulare : a reperto us ; b reperto istologico . finding was later confirmed by histology , which , in addition , did not detect hyalinisation in the adjacent parenchyma . at histology , nine cases were seminomas , two were mixed germ - cell tumours , one was embryonal carcinoma , one was a yolk - sac tumour and one was a benign sertoli - cell tumour . 
nine out of 13 cases of testicular cancer ( 69.2% ) had microcalcifications ( in 2 / 9 cases intranodular , in 5 / 9 perinodular and in 2 / 9 periand intranodular )  . 
in 12 cases ( 92.3% ) , there was tubular hyalinisation in the parenchyma surrounding the testicular cancer . discussion the origin of testicular microlithiasis is unclear , and most authors [ 1316 ] hypothesise that the microliths are intratubular calcifications arising from calcium salt deposits in degenerated germ cells [ 13 ] or in intratubular secretions [ 14 ]  . 
according to more recent studies , the microliths may have an extratubular origin and penetrate the seminiferous tubule subsequently [ 15 ] , and some authors believe that microlithiasis may be correlated with a dysfunction of the sertoli cells , indicating anomalous gonadal embryogenesis [ 1 , 16 ]  . us examination has a decisive role in confirming a clinical suspicion or identifying a disease that requires surgical verification . 
us is also fundamental in patients with known risk factors that have either a high level of evidence ( family history , cryptorchidism , contralateral germ - cell neoplasm , gonadal dysgenesis ) or an intermediate level of evidence ( infertility , dizygous twins , testicular atrophy ) [ 10 ] , to disclose early changes in testicular parenchyma . 
risk factors with a low or controversial level of evidence are scrotal trauma , inguinal hernia , testicular ectopia , previous infections ( meningitis , pneumonia , tuberculoses ) , mumps orchitis , testicular torsion , varicocele , early puberty , down syndrome , acne , co vitellino e 1 caso tumore a cellule di sertoli variet sclerosante . 
in 9 casi su 13 ( 69 , 2% ) di ntm , sono state rilevate microcalcificazioni ( in 2 / 9 casi in sede intranodulare ; in 5 / 9 perinodulari e in 2 / 9 peri e intranodulari )  . 
in 12 casi ( 92 , 3% ) , era presente sct nel parenchima circostante la ntm . discussione lorigine della mt non chiara e la maggior parte degli autori [ 1316 ] ipotizza che queste formazioni siano calcificazioni intratubulari che originano da depositi di sali di calcio in cellule germinali degenerate [ 13 ] o in secrezioni intratubulari [ 14 ]  . 
secondo studi pi recenti , i microliti possono avere unorigine extratubulare , penetrando successivamente nel tubulo seminifero [ 15 ] e , per alcuni autori , le mt possono essere correlate ad una disfunzione delle cellule del sertoli , indicando una embriogenesi gonadica anomala [ 1 , 16 ]  . lindagine ecografica assume un ruolo decisivo nel confermare un sospetto clinico o nel rilevare una patologia che necessita di verifica chirurgica . 
inoltre , lecografia si rileva metodica insostituibile nei pazienti con fattori di rischio accertati con alto livello di evidenza ( familiarit , criptorchidismo , neoplasia germinale controlaterale , disgenesia gonadica ) o con medio livello di evidenza ( infertilit , gemelli dizigoti , atrofia testicolare ) [ 10 ] , nello svelare precoci alterazioni nel parenchima testicolare . 
vengono definiti fattori di rischio con basso o controverso livello di evidenza : il trauma scrotale , lernia inguinale , lectopia testicolare , pregresse infezioni ( meningite , polmonite , tbc ) , orchite parotitica , torsione testicolare , varicocele , pubert precoce , sindrome di down , acne , hiv , alopecia androgenica e non vi menzione alcuna in merito la mt [ 10 ]  . alcuni autori riconoscono che le mt possono essere associate a differenti patologie non neoplastiche : atrofia testig.c. 
however , the most commonly held views in the literature are those that support a correlation between microlithiasis and testicular cancer [ 1 , 3 , 4 , 6 , 1930 ]  . 
if confirmed by future prospective studies , this fact should , in our opinion , lead us to suspect the existence of an environment predisposing to the development of testicular cancer and therefore the possibility of identifying the population at risk of such cancer . 
this hypothesis is not supported by other studies [ 5 , 31 ] , and many authors question this association [ 3236 ] and do not recommend monitoring these patients [ 36 ]  . 
in our view , the prevalence of retrospective studies on microlithiasis in symptomatic patients , the ongoing technological evolution with the use of high - frequency probes and increasingly sophisticated instruments call for longitudinal prospective studies to shed light on this issue . 
our results show that testicular microliths are associated with testicular cancer in 53.8% at us and in 69.2% at histology and confirm the diagnostic accuracy of us in detecting the presence and distribution of microlithiasis . 
this discrepancy is related to the difficulty experienced by us in discriminating between healthy and neoplastic tissue in some cases of heterogeneous parenchyma with poor cleavage planes . these data , in agreement with previous studies that report a 6%46% incidence of germ - cell tumours in patients with microlithiasis [ 1 , 6 ] , support the hypothesis of a correlation between microlithiasis and the development of testicular cancer and should lead us to consider the possibility of obtaining a biopsy in all patients presenting with this type of alteration [ 30 ]  . some authors believe that the presence of unilateral microlithiasis has a high likelihood of being associated with testicular cancer , such that biopsy is justified in these cases , whereas the presence of diffuse bilateral microlithiasis , although potentially concealing a carcinoma in situ , justifies sonographic monitoring only [ 37 ]  . 
 perilesional microlithiasis , detected at us in 5 / 13 patients ( 38.4% ) and at histological examination in 7 / 13 patients ( 53.8% ) , which is external to the cancer and associated with tubular hyalinisation in the adjacent parenchyma , supports , in our opinion , the hypothesis of an environment that predisposes to cancer development and may therefore represent , as held by other authors , a premalignant condition [ 6 ]  . 
such considerations justify the view that clinical and imaging monitoring is justified in these patients . almost all of the patients examined ( 92.3% ) had tubular hyalinisation in the tissue surrounding the testicular cancer , as reported by previous studies [ 12 , 38 ] , as a result not only of autoimmune processes but also of ischaemic or obstructive events that may account for the development of a cancer in a predisposing environment . 
this is also supported by the colare , infertilit , criptorchidismo , anormalit cromosomiche ( sindromi di down o klinefelter ) ; esiti di orchite , sarcoidosi , infarto cronico [ 9 , 17 , 18 ]  . 
tuttavia , in letteratura sono prevalenti le tesi che sostengono lipotesi di correlazione fra lesistenza delle mt e la ntm [ 1 , 3 , 4 , 6 , 1930 ] ; tale rilievo , se confermato da ulteriori studi prospettici , deve far sospettare , a nostro avviso , lesistenza di un terreno favorente lo sviluppo della ntm e , quindi , la possibilit di individuare la popolazione a rischio di insorgenza della eteroplasia testicolare . 
tale ipotesi non risulta per essere sostenuta da altri studi [ 5 , 31 ] , e molti autori pongono in dubbio questa associazione [ 3236 ] e sconsigliano il monitoraggio di questi pazienti [ 36 ]  . 
a nostro avviso , la prevalenza di studi retrospettivi sulla mt in soggetti sintomatici , la continua evoluzione tecnologica con utilizzo di sonde ad elevata frequenza e strumentazioni sempre pi sofisticate , invocano studi longitudinali prospettici che possano fare chiarezza sullargomento . 
dai nostri risultati si evince che le mt sono associate alla ntm rispettivamente nel 53 , 8% allindagine ultrasonografica e nel 69 , 2% allesame istologico , confermando una buona accuratezza diagnostica dellecografia nel rilievo della presenza e della distribuzione della mt . 
in un solo paziente la mt allecografia era stata individuata nella porzione esterna della lesione eteroplastica , mentre allesame istologico questa era al di fuori della neoplasia . tale incongruenza da riferire alla difficolt in alcuni casi , in presenza di tessuto parenchimale disomogeneo e con scarsi piani di clivaggio , a discriminare ecograficamente il tessuto sano da quello neoplastico . tali dati , in accordo con altri della letteratura che riportano una incidenza del tumore a cellule germinali in pazienti con mt che varia dal 6% al 46% [ 1 , 6 ] , sono di sostegno allipotesi che vi sia una correlazione fra la mt e lo sviluppo della ntm , tale da considerare leventualit di effettuare la biopsia in tutti i pazienti che presentano questa alterazione [ 30 ]  . 
 alcuni autori sostengono che la presenza di mt raggruppate monolateralmente abbia una elevata probabilit di associarsi a ntm , tale da giustificare la biopsia , mentre la presenza di mt diffuse e bilaterali , pur potendo celare un carcinoma in situ , giustifica solo un monitoraggio ecografico [ 37 ]  . la mt perilesionale , evidenziata in 5 / 13 pazienti allecografia ( 38 , 4% ) e in 7 / 13 pazienti allesame istologico ( 53 , 8% ) , esterna alla neoplasia ed associata alla presenza di sct nel tessuto parenchimale testicolare adiacente alla neoplasia , deve far ipotizzare , a nostro avviso , la presenza di un ambiente predisponente allo sviluppo della lesione neoplastica e quindi , come gi sostenuto da alcuni autori , possa rappresentare condizione di premalignit [ 6 ]  . 
a nostro parere , tali considerazioni supportano lipotesi che sia giustificato il monitoraggio clinico - strumentale in questi pazienti . in quasi tutti i pazienti ( 92 , 3% ) da noi esaminati sono stati rilevati nel tessuto circostante la ntm fenomeni di sct , a conferma di quanto gi sostenuto da altri autori [ 12 , 38 ] , come conseguenza non solo di processi autoimmuni , ma di fenomeni ischemici ed ostruttivi che potrebbero giustificare linsorgenza della neoplasia su di un territorio predisposto . 
 two of the 13 patients with testicular cancer had poor sperm function ; this finding has already been reported in the literature and , according to some authors , 9% of patients with a diagnosis of germ - cell tumour were infertile before the diagnosis [ 39 , 40 ]  . 
furthermore , our study indicated that us with high - frequency probes is reliable in detecting and visualising microlithiasis compared with the histological examination ; in contrast to previous studies [ 7 ] , we believe this finding to be useful for identifying patients that are potentially at higher risk of developing testicular cancer . in our view , testicular microlithiasis is a risk factor for the development of testicular cancer if there are more than ten microliths per testis , or if present in a retained or atrophic testis , in a patient who has undergone surgery for retained testis , or in subjects of a critical age ( 1640 years ) without signs of seminal duct obstruction . 
 in 2 dei 13 pazienti con ntm erano presenti alterazioni dello spermiogramma ; questo reperto gi stato osservato in letteratura e secondo alcuni autori il 9% di pazienti con diagnosi di tumore germinale presentava infertilit prima della diagnosi [ 39 , 40 ]  . 
pertanto , per alcuni autori , la mt si associa ad alterazioni del liquido seminale con ipofertilit [ 41 ] e , come peraltro da noi sostenuto , tali fattori sono correlati ad un alto rischio nello sviluppo della ntm . nella nostra casistica , nel 53 , 8% dei casi , leco color doppler stato in grado di mettere in risalto in sede intrae peri - lesionale la vivace vascolarizzazione , indice , qualora presente , della neoangiogenesi tipica delle forme eteroplastiche , con la presenza , in 2 casi , di fistola artero - venosa ; questultimo dato risulta utile a nostro avviso nel rafforzare lipotesi diagnostica di eteroplasia . 
dai nostri dati emerge inoltre laffidabilit dellecografia con sonde ad elevata frequenza nel rilevare e nellevidenziare le mt testicolari rispetto al dato istologico ; tale elemento , in contrapposizione con altri autori [ 7 ] , risulta utile nellindividuare cos i pazienti che potenzialmente risultano pi a rischio della popolazione generale a sviluppare la ntm . a nostro parere le mt rappresentano fattore di rischio per lo sviluppo di ntm se sono di numero maggiore di 10 per testicolo , o se sono presenti in testicolo ritenuto , atrofico o in paziente operato per testicolo ritenuto , o in soggetti di et critica ( 1640 anni ) e che non presentano segni ostruttivi alle vie seminali . conclusions conclusioni our experience indicates that us is reliable in detecting testicular microlithiasis compared with the histological examination and suggests that patients with this alteration may be more predisposed to testicular cancer compared with the general population . 
further longitudinal prospective studies are required to validate the evidence of a parenchymal environment predisposing to the development of testicular cancer . dalla nostra esperienza emersa laffidabilit dellecografia nel rilevare le mt rispetto lesame istologico e lipotesi che pazienti con mt siano maggiormente predisposti , rispetto alla popolazione generale , allo sviluppo di un processo neoplastico . 
giovagnorio2 1dipartimento di scienze radiologiche , policlinico umberto i , universit degli studi sapienza di roma , italy 2cadi - icot latina , universit degli studi sapienza di roma polo pontino , roma , italy correspondence to : g . 
toti 6 , i - 74020 avetrana , taranto , tel . : + 39 - 347 - 7361067 , e - mail : glo.fan@gmail.com received : 16 may 2006 / accepted : 21 july 2006 / published online : 11 june 2007 abstract purpose . 
abbiamo eseguito 50 artro - tc gassose per instabilit di spalla , utilizzando scansioni a collimazione sottile ; i dati grezzi sono stati trasferiti ad una workstation e rielaborati con algoritmi di riformattazione multiplanari ( mpr ) e di rendering volumetrici ( vr )  . 
abbiamo diagnosticato 8 lesioni del cercine anterosuperiore ( i gruppo ) ; 32 lesioni del cercine antero - inferiore ( ii gruppo ) ; 2 lesioni del cercine posteriore ( iii gruppo )  . 
pathogenetically , the disorder has been divided into traumatic [ traumatic unidirectional bankart surgery ( tubs ) ] , atraumatic multidirectional bilateral rehabilitation inferior capsular shift ( ambri ) , and acquired instability overstress ( aios ) [ 5 ]  . 
a variety of diagnostic techniques have been used over the years , including conventional arthrography , ct arthrography , magnetic resonance imaging ( mri ) and mr arthrography , which provide useful information on the status of intraand periarticular structures , in particular , the fibrocartilaginous glenoid labrum , the glenohumeral ligaments , the joint capsule and the bone structures . an accurate definition of the site and extent of injury will guide the surgical strategy ( arthroscopy or arthrotomy ) , which is often necessary to restore normal shoulder articulation and function . 
the current trend is to reconstruct the labrum using arthroscopy , as it allows for less invasiveness and faster functional recovery , although the association of a labral lesion with major bone lesions ( hill - sachs or bankart lesions ) generally requires open surgery [ 610 ]  . 
the aim of this paper is to describe our experience with air - contrast 64slice ct arthrography in shoulder instability . materials and methods from november 2005 to march 2006 , we performed 50 ct arthrography examinations on 34 men and 16 women ( age range 1759 years , mean 38 ) , with a history of luxation - subluxation and / or clinical signs of acute or chronic instability . in eight patients , the instability had persisted after a previous stabilising surgical procedure . 
air - contrast ct arthrography was used to evaluate the following structures : glenoid labrum , articular capsule and recesses , glenohumeral ligaments , humeral socket , insertions of rotator cuff tendons , width of the subacromial space , and presence of effusions in the deltoid subacromial bursa and in intra - articular sites . 
in particular , glenoid labrum lesions were subdivided on the basis of their position : 123 oclock ( anterosuperior ) ( group 1 ) , 36 oclock ( anteroinferior ) ( group 2 ) and 612 oclock ( posterior ) ( group 3 ) ; superior labral anterior - posterior ( slap ) lesions were considered part of group 1 . 
the instability was secondary to the presence of one or more alterations at various levels ( labrum , capsule , socket , glenohumeral ligaments and rotator cuff )  . after obtaining the patients informed consent , 20 cc of gaseous contrast material ( air ) was injected in the articulation , via a posterior access and without fluoroscopic guidance , to obtain adequate image contrast , maximum capsule distension and differentiation of the various intra - articular components . 
the examination was conducted with a 64 - slice spiral volume ct scanner ( lightspeed vct , ge ) acquiring thin - collimation ( submillimetre ) scans in the axial planes . the data ( isotropic voxels ) were transferred to a graphics lincapacit di mantenere la testa omerale centrata nella cavit glenoidea conseguente ad uno squilibrio tra gli stabilizzatori statici ( morfologia della glena e dellapparato capsulo - labro - legamentoso ) e dinamici ( complesso muscolotendineo della cuffia dei rotatori e muscoli periscapolari ) della spalla . 
nel corso degli anni sono state messe a punto diverse tecniche diagnostiche , quali lartrografia tradizionale , lartro - tc , lrm e lartrorm , indispensabili per fornire utili informazioni sullo stato delle strutture endoe periarticolari , nel caso specifico del cercine fibrocartilagineo glenoideo , dei legamenti glenomerali , della capsula articolare e delle strutture ossee . una precisa definizione della sede e dellentit della lesione indirizza la scelta chirurgica ( artroscopica o artrotomica ) , spesso necessaria per il ripristino della normale articolarit e funzionalit della spalla . 
la tendenza attuale di ricorrere con frequenza sempre maggiore alla ricostruzione labiale con accesso artroscopico , per i vantaggi legati alla minore invasivit e al pi rapido recupero funzionale , anche se lassociazione di lesione labiale e importanti lesioni ossee ( hill - sachs o bankart ) indirizza generalmente verso un intervento chirurgico a cielo aperto [ 610 ]  . 
scopo del presente lavoro quello di esporre la nostra esperienza in materia di artro - tc gassosa con apparecchiatura a 64 strati nellinstabilit di spalla . materiali e metodi da novembre 2005 a marzo 2006 sono state eseguite 50 artro - tc in 34 maschi e 16 femmine , di et compresa tra 17 e 59 anni ( et media 38 anni ) , con anamnesi positiva per episodi di lussazione - sublussazione e / o segni clinici di instabilit acuta o cronica . 
con lartro - tc gassosa sono state valutate le seguenti strutture : il cercine glenoideo ; la capsula articolare e i recessi ; i legamenti gleno - omerali ; la glena omerale ; le inserzioni dei tendini della cuffia dei rotatori ; lampiezza dello spazio subacromiale ; la presenza di versamento nella borsa sub - acromion deltoidea ed in sede intra - articolare . 
in particolare , le lesioni del cercine glenoideo sono state suddivise in base alla posizione : da ore 12 a ore 3 ( antero - superiore ) ( i gruppo ) , da ore 3 a ore 6 ( antero - inferiore ) ( ii gruppo ) e da ore 6 a ore 12 ( posteriore ) ( iii gruppo ) ; le slap lesion sono state considerate facenti parte del i gruppo . 
il quadro di instabilit era secondario alla presenza di una o pi alterazioni a vari livelli ( cercine , capsula , glena , legamenti gleno - omerali e cuffia dei rotatori )  . previo consenso informato , senza controllo scopico , stata eseguita , attraverso un accesso posteriore , liniezione intra - articolare di circa 20 cc di mdc gassoso ( aria ) , necessaria per ottenere un sufficiente contrasto dimmagine , la distensione massima della capsula e la differenziazione delle varie componenti endoarticolari . 
using three - dimensional ( 3d ) reconstruction software ( navigator plus ) in ten cases selected randomly from group 2 , we also performed virtual arthroscopy , a perspective reconstruction of the glenohumeral joint that simulates the view of a fibreoptic endoscope . 
the acquisition parameters were as follows : 200 kv , 40 mas , slice thickness 0.6 mm , reconstruction interval 0.6 mm , fov 18 cm18 cm and matrix 512512 . 
total examination time ( including preparation and acquisition ) was around 10 mimages were analysed both in the different spatial planes ( axial , coronal , sagittal and oblique ) , and by performing perspective volume reconstructions allowing evaluation of bone structures first ( glenoid fossa and humeral head ) and then of soft tissues ( glenoid labrum and air - distended capsule )  . the patients then underwent diagnostic and / or therapeutic conventional stabilising arthroscopy , and the results were correlated with those of air - contrast ct arthrography to calculate the techniques sensitivity , specificity and diagnostic accuracy . results the diagnoses of air - contrast ct arthrography and conventional arthroscopy were identical in 42 / 50 cases of instability secondary to disorders of the capsular - labral - ligamentous and / or bone complexes . 
in 6 / 50 cases , the results were discordant , as ct arthrography failed to detect four glenoid labrum lesions from 12 to 3 oclock ( group 1 ) and two lesions from 3 to 6 oclock ( group 2 )  . 
in 2 / 50 patients , aircontrast ct arthrography proved nondiagnostic owing to failure to achieve capsular distension because of air leakage in the anteroinferior articular recess in one case and capsulitis in the other ; these patients were consequently excluded from our study . sensitivity and specificity values of mdct arthrography in the overall recognition of the various lesions of the fibrocartilaginous labrum were 88% and 100% , respectively . group 1 and group 2 labral lesions were diagnosed easily , with a calculated sensitivity of 94% ( two false negatives ) and 100% , respectively . 
i dati ottenuti ( voxel isotropici ) sono stati trasferiti ad una workstation grafica ( advantage , ge ) e rielaborati con algoritmi di riformattazione multiplanare ( mpr ) e di rendering volumetrici ( vr )  . 
utilizzando un programma di ricostruzione 3d ( navigator plus ) in 10 casi scelti in maniera random nel ii gruppo stata inoltre effettuata lartroscopia virtuale , una ricostruzione prospettica dellarticolazione gleno - omerale che simula la visione di un endoscopio a fibre ottiche . 
procedendo in senso cranio - caudale , dallarticolazione acromionclaveare alla porzione inferiore dellarticolazione glenoomerale , lindagine stata condotta con paziente supino e braccio in posizione neutrale , utilizzando i seguenti parametri : 200 kv ; 40 ma ; spessore di strato 0 , 6 mm ; intervallo di ricostruzione 0 , 6 mm ; fov 18 cm18 cm ; matrice 512512 . il tempo totale della procedura ( preparazione e acquisizione ) stato di 10 min circa . 
le immagini sono state analizzate sia nei vari piani dello spazio ( assiale , coronale , sagittale e obliquo ) , che eseguendo ricostruzioni volumetriche prospettiche che permettessero di valutare prima le strutture ossee ( fossa glenoidea e testa omerale ) e poi i tessuti molli ( labbro glenoideo e capsula distesa dallaria )  . i pazienti sono stati sottoposti , infine , ad esame artroscopico convenzionale diagnostico e / o terapeutico di stabilizzazione della spalla , e i risultati sono stati confrontati con quelli dellartro - tc gassosa , calcolandone sensibilit , specificit e accuratezza diagnostica . risultati le diagnosi dellartro - tc gassosa e dellartroscopia convenzionale sono state sovrapponibili in 42 / 50 casi di instabilit , secondaria a patologie del complesso capsulo - labro - legamentoso e / o osseo . 
in 6 / 50 casi i risultati non sono stati sovrapponibili , in quanto allartro - tc gassosa non abbiamo riconosciuto : 4 lesioni a livello del cercine glenoideo da ore 12 a ore 3 ( i gruppo ) e 2 lesioni da ore 3 a ore 6 ( ii gruppo )  . 
in 2 / 50 pazienti , lartro - tc gassosa non stata diagnostica a causa della mancata distensione capsulare secondaria rispettivamente a fuga di gas nel recesso articolare antero - inferiore e a fenomeni capsulitici ; questi pazienti sono stati pertanto esclusi dallo studio . i valori di sensibilit e specificit dellartro - tcmd nel riconoscimento complessivo delle varie lesioni del cercine fibrocartilagineo sono risultati pari rispettivamente all88% e al 100% . 
the axial section shows an abnormal configuration of the anterior labrum and of its junction with the capsule ( * ) , as well as the separation of soft tissue from the coracoid process by interposed injected air ( a )  . 
a la sezione assiale mostra anomala configurazione del labbro anteriore e della sua giunzione con la capsula ( * ) , ed interposizione di aria tra il processo coracoideo e i tessuti molli . 
2a - c la sezione assiale mostra lassit capsulare , completo scollamento del margine glenoideo libero antero - inferiore ( lesione di bankart vera ) ( a ) ; corrispettivo artroscopia convenzionale ( b ) e virtuale ( c )  . gion recorded the highest number of false negative results ( 4 ) despite the techniques ability to recognise the subtlest and most complex lesions ; sensitivity was 66% . 
5 capsula ridondante anteriormente ; avulsione completa del cercine glenoideo antero - inferiore ; legamento gleno - omerale medio ( * ) separato dalla parete capsulare , assottigliato e a densit disomogenea ( lesione di perthes )  . discussion shoulder stability depends on a complex of bone structures and soft tissues that surround and make up the glenohumeral joint . 
4 capsula ridondante con presenza di ampi recessi in sede anteriore e posteriore ; cercine glenoideo normale ; tendine del sottoscapolare ( * ) separato dalla capsula , di aspetto sinuoso , integro . diagnosticate facilmente ; stata calcolata una sensibilit rispettivamente del 94% ( 2 falsi negativi ) e del 100% . le difficolt diagnostiche maggiori si sono presentate nelle lesioni del cercine da ore 12 a ore 3 ( i gruppo ) ; a tale livello , infatti , nonostante siano state evidenziate le lesioni pi fini e complesse , si anche riscontrato il maggior numero di falsi negativi ( 4 ) ; la sensibilit stata del 66% . 
la sensibilit risultata sempre del 100% nella diagnosi delle alterazioni delle strutture ossee e / o dei tessuti molli associate alle varie lesione del cercine . discussione la stabilit della spalla dipende da un insieme di strutture ossee e di tessuti molli che circondano e formano larticolazione gleno - omerale . 
non esiste una singola anormalit che di per s responsabile dellinstabilit , ma una combinazione di differenti fattori che interagiscono fra di loro : anormalit del labbro glenoideo ; lassit o lesione capsulare ; legamenti gleno - omerali insufficienti o lesionati ; anomalie di forma e sviluppo della glenoide ; fratture di hill - sachs o bankart quali esiti di pregresse lussazioni [ 1113 ]  . lartro - tc un metodo accurato per la valutazione dellarticolazione della spalla ; fornisce infatti importanti e utili informazioni su morfologia e rapporti delle strutture endo e periarticolari [ 11 ]  . 
questa tecnica ha giocato un ruolo determinante nella diagnostica dellinstabilit di spalla fino a quando lrm basale e lartro - rm non sono state considerate il gold standard nello studio di tale patologia , in quanto dotate di multiplanariet , sensibilit e specificit intrinseca superiori [ 1 , 14 , 15 ]  . 
retrazione del tendine del bicipite ( a ) , assenza del tendine del sovraspinoso ( b )  . ct arthrography is an accurate technique for the evaluation of the shoulder joint and provides significant and useful information on the morphology and relationships of intraand periarticular structures [ 11 ]  . 
the technique played a fundamental role in the diagnosis of shoulder instability until baseline mri and mr arthrography became the gold standard in the study of this disorder in view of their multiplanar capabilities and superior intrinsic sensitivity and specificity [ 1 , 14 , 15 ]  . 
as a result , ct arthrography has taken on a secondary role , being indicated only in disorders of the glenoid labrum , glenohumeral ligaments , the long head of the biceps ruolo secondario , trovando indicazione nella patologia del labbro glenoideo , dei legamenti gleno - omerali , del capo lungo del bicipite e della cuffia dei rotatori solo nel caso di controindicazioni o di dubbi diagnostici allrm ; ha mantenuto invece un ruolo primario nello studio delle patologie ossee proprie della spalla , quali fratture , tumori , artriti , alterazioni ossee secondarie proprie dellinstabilit e dellartrosi [ 5 ]  . in uno studio prospettico di chandnani et al . 
 [ 14 ] del 1993 , stata sottolineata la maggiore sensibilit dellartrorm rispetto allrm e allartro - tc ( 96% vs 93% e 73% ) nel diagnosticare sia le alterazioni del cercine fibrocartilagineo g.p. 
it has , instead , maintained its primary role in the study of shoulder bone disorders , such as fractures , tumours , arthritis and bone alterations secondary to instability and arthrosis [ 5 ]  . a 1993 prospective study by chandnani et al . 
confirmed the better accuracy of mr arthrography in identifying the capsular - labral - ligamentous injuries responsible for shoulder instability , as the method provides panoramic and precise views of the lesions [ 6 ]  . in our opinion , ct arthrography offers several advantages in the study of the shoulder . 
it does not require arthroscopy , so the time required to introduce the gaseous contrast material into the articular cavity and perform the scan is very short , if compared with other examinations [ 15 ]  . 
the gaseous contrast agent air in this specific case has no contraindications and is free , unlike radiopaque or paramagnetic agents , which are nonetheless considered harmless [ 17 , 18 ]  . with the advent of spiral and in particular multislice technology , ct has improved considerably . 
the faster rotation speed of the x - ray tube and the use of thin collimations with larger volume acquisitions compared with conventional ct have allowed for improved temporal and spatial resolution in the z axis [ 19 , 20 ]  . 
in particular , latest - generation 64 - slice mdct scanners , as the one used by us , enable the acquisition of 64 submillimetre slices ( 0.6 mm ) per rotation and , by combining an isotropic spatial resolution ( 0.4 mm3 ) with a rotation speed of around 0.33 s , they allow optimal image quality to be routinely achieved and visualisation of the finest details . 
submillimetre and isotropic voxels were indeed particularly useful in postprocessing , with the creation of 3d images and multiplanar reconstructions in the sagittal , oblique , and coronal planes with no step - like defect in the outline , and hence with a high diagnostic quality [ 19 , 22 ]  . after these voxels have been processed with dedicated software , they can also be used to perform virtual arthroscopy of the articulation . 
not only did it provide an additional view of the joint , which confirmed our results , but it also generated more realistic , intuitive and didactic images , which are consequently more useful to orthopaedic surgeons planning surgery [ 22 , 23 ]  . a number of papers dating between 2003 and 2005 concluded that mdct arthrography has greater diagnostic accuracy than does mri / mr arthrography in the study , for example , of cartilaginous lesions of the ankle , hip , and elbow joints or in the rupture of interosseous ligaments of the wrist [ 2427 ]  . despite these results , bitzer et al . 
in a 2004 study assessing the diagnostic accuracy of mdct arthrography and mr arthrography in 29 patients affected by chronic instability reaffirmed the higher sensitivity and specificity of mr glenoideo e del legamento gleno - omerale inferiore , che la patologia della cuffia dei rotatori , utilizzando un apparecchio rm a 1 , 5 t e una tc di 3a generazione [ 14 ]  . 
 [ 6 ] , nel 2003 , hanno confermato la maggiore accuratezza dellartro - rm nellidentificare le lesioni capsulo - labro - legamentose determinanti instabilit di spalla , in quanto metodica panoramica e precisa in tali lesioni [ 6 ]  . lartro - tc , a nostro avviso , offre diversi vantaggi nello studio della spalla . 
non richiesto un controllo scopico , pertanto lintroduzione in cavit articolare del mdc gassoso e lesecuzione della scansione necessitano di un tempo minimo , se paragonato ad altre indagini [ 15 ]  . 
il mdc gassoso , nel caso specifico laria , del tutto privo di controindicazioni e di costi , a differenza dei mdc radiopachi o paramagnetici , comunque considerati innocui [ 17 , 18 ]  . con lavvento della tc spirale in particolare multistrato , la tecnica migliorata notevolmente . 
laumento della velocit di rotazione del tubo radiogeno e limpiego di collimazioni sottili con acquisizioni volumetriche pi estese rispetto alla tc convenzionale , hanno consentito di incrementare la risoluzione temporale e spaziale lungo lasse z [ 19 , 20 ]  . 
in particolare gli scanner dellultima generazione di tcms a 64 strati , da noi utilizzati , consentono lacquisizione di 64 strati sub - millimetrici ( 0 , 6 mm ) per rotazione e , combinando una risoluzione spaziale isotropica ( 0 , 4 mm3 ) e una velocit di rotazione pari a circa 0 , 33 s , permettono di raggiungere routinariamente unottima qualit di immagine e la visualizzazione dei pi fini dettagli . 
i voxel submillimetrici ed isotropici sono stati infatti particolarmente vantaggiosi nel post - processing , creando immagini 3d e ricostruzioni multiplanari , nei piani sagittale , obliquo e coronale esenti da qualsiasi difetto a gradino del contorno e dotate pertanto di alta qualit diagnostica [ 1922 ]  . questi voxel , rielaborati da software dedicati , possono inoltre essere utilizzati per eseguire lartroscopia virtuale dellarticolazione . 
nel nostro studio , la valutazione artroscopica virtuale , effettuata in maniera sperimentale in 10 artro - tc , stata particolarmente utile ; stata in grado infatti non solo di fornire un ulteriore punto di vista dellarticolazione , avvalorando i nostri risultati , ma anche di elaborare immagini pi realistiche , intuitive e didattiche , e pertanto pi utili nella pianificazione dellintervento chirurgico da parte del chirurgo ortopedico [ 22 , 23 ]  . in letteratura , dal 2003 al 2005 , sono stati pubblicati diversi lavori in cui si conclude che lartro - tcmd ha una maggiore accuratezza diagnostica a confronto con lrm / artro - rm nello studio , per esempio , delle lesioni della cartilagine articolare della caviglia , dellanca , del gomito , o nella rottura dei legamenti interossei del polso [ 2427 ]  . nonostante questi risultati , bitzer et al . 
 [ 15 ] , in uno studio del 2004 , valutando laccuratezza diagnostica dellartro - tcmd e dellartro - rm in 29 pazienti affetti da instabilit cronica , hanno ribadito una superiore sensibilit e specificit dellartro - rm rispetto allartro - tcmd nello studio delle lesioni del labbro glenoideo ( 96% vs 76% e 96% vs 92% )  . 
in a paper by waldt et al . , published in 2005 , which compared mr arthrography , ct arthrography and anatomical dissection , mdct proved to be more accurate than mri in evaluating the superior labrum insertion ( 84% vs 79% ) and the anteroposterior extension of the sublabral recess ( 81% vs 59% ) [ 28 ]  . 
the results of our study appear to be in perfect agreement with the findings of the most recent literature . in our study , the different labrum lesions ( groups 1 , 2 and 3 ) were diagnosed with mdct - arthrography with 88% sensitivity and 100% specificity . 
the best results were obtained in particular in groups 2 and 3 , with sensitivity values of 94% and 100% , respectively , and in the diagnosis of associated lesions ( capsular , hill - sachs , bankart and rotator cuff lesions ) , where sensitivity and specificity both reached 100% . 
the excellent level of diagnostic accuracy proved essential in guiding and , in some cases , modifying the surgical approach . comparavano lartro - rm , lartro - tc e la dissezione anatomica , lartro - tcmd si dimostrata pi accurata dellartrorm nel valutare linserzione del labbro superiore ( 84% vs 79% ) e lestensione antero - posteriore del recesso sottolabiale ( 81% vs 59% ) [ 29 ]  . 
i risultati del nostro studio sono apparsi perfettamente in linea con i dati della letteratura pi recente . le varie lesioni del cercine ( i , ii e iii gruppo ) allartrotcmd sono state diagnosticate con una sensibilit dell88% e una specificit del 100% . 
i migliori risultati si sono evidenziati in particolare nel ii gruppo e iii gruppo , in cui la sensibilit ha raggiunto valori del 94% e 100% , e nella diagnosi delle lesioni associate ( capsulari , di hill - sachs , di bankart e cuffia dei rotatori ) , in cui sensibilit e specificit sono state rispettivamente del 100% . 
pittore 20 , i - 00136 roma , italy , tel . : + 39 - 065 - 8703056 , fax : + 39 - 065 - 8703039 , e - mail : g.regine@sirm.org received : 4 april 2005 / accepted : 5 june 2006 / published online : 11 june 2007 abstract purpose . 
between march 2004 and april 2005 , 277 patients with blunt abdominal trauma were evaluated . twenty - eight out of 277 patients had renal lesions , the severity of which was graded according to the organ injury severity scale of the american association for the surgery of trauma ( aast )  . 
in modo particolare lecografia con mdc risulta tecnica affidabile per la valutazione del trauma renale di basso grado e nel followup dello stesso riducendo il ricorso a ripetuti esami tc con riduzione della dose radiante . 
i limiti sono dati dagli alti costi della tecnica se condotta su popolazione non selezionata . key words contrast - enhanced sonography renal trauma parole chiave ecografia con mezzo di contrasto trauma renale introduction introduzione the current diffusion of sonographic contrast agents has extended the indications of ultrasound ( us ) imaging [ 1 ]  . 
in particular , second - generation contrast agents have not only attualmente la diffusione e lutilizzo dei mezzi di contrasto ecografici ha potenziato ed arricchito di nuove indicazioni lesame ecografico [ 1 ]  . 
the study population included patients with minor blunt abdominal trauma with or without haematuria , patients who were stable but had undergone parasurgical renal procedures during the previous 12 h ( lithotripsy , renal artery stenting , postbiopsy monitoring ) and patients with acute abdomen , haematuria , and minimal but sudden drop in blood - cell count . 
for paediatric patients or patients under the age of 18 years , the parents informed consent was obtained before proceeding to contrast - enhanced us . in all cases , baseline us was integrated by the contrast study performed on a dedicated scanner ( sequoia , siemens , germany ) , with low mechanical index and contrast - specific software [ coherent contrast imaging ( cci ) 222 patients ; cadence contrast pulse sequence ( cps ) 55 patients ]  . 
patients were administered a bolus of 2.4 ml of second - generation contrast material ( sonovue ) followed by about 10 cc saline solution via peripheral vethe examination consisted of an assessment of the liver parenchyma , followed by the splenic and renal parenchyma and by the supraand submesocolic peritoneal recesses , and generated both static images and dynamic clips lasting around 20 s each taken at various times during the examination , depending on the findings . 
there were no early or late allergic reactions to the intravenous contrast material , which appeared to be very well tolerated by patients and fairly easy to use for the operators , who had received specific training in its correct preparation . patients with positive us findings underwent mdct ( light speed ultra , ge , usa ) before and after the intravenous administration of iodinated contrast material , with a specific multiphase acquisition protocol that allowed correct staging of the lesion and assessment of the integrity of the urinary tract . 
in addition , our study evaluated contrast - enhanced us in the follow - up of renal injuries using the same examination protocol as used for the initial assessment . the lesions were classified into five grades of increasing severity according to the american association for the surgery of trauma ( aast ) classification : grade 1 , subcapsular haematoma ; grade 2 , superficial renal lacerations with perirenal haematoma ; grade 3 , renal lacerations deeper than 1 cm without extension into the collecting system or evitrasto ecografici di ii generazione ha permesso non solo di incrementare le potenzialit diagnostiche dellecografia nellidentificazione e caratterizzazione delle lesioni epatiche [ 2 , 3 ] , ma anche di identificare e studiare le lesioni traumatiche di altri organi addominali : milza e fegato in modo particolare [ 4 ]  . lo scopo del presente contributo quello di definire le indicazioni , le potenzialit diagnostiche ed i limiti dellesame ecografico con mezzo di contrasto di ii generazione nel trauma renale , in base alla nostra esperienza maturata in un dea di ii livello . materiali e metodi nel periodo compreso tra marzo 2004 ed aprile 2005 sono stati valutati con esame ecografico basale e dopo somministrazione di mdc ev di ii generazione ( sonovue , bracco , italia ) 277 pazienti con trauma addominale chiuso minore , con o senza ematuria , pazienti stabili , ma sottoposti nelle 12 ore precedenti a procedure parachirugiche in ambito renale ( litotrissia , posizionamento di stent vascolari in arteria renale , monitoraggio post - bioptico ) e che avevano manifestato un quadro di addome acuto , ematuria , minima ma improvvisa riduzione dellemocromo . 
per la valutazione di pazienti pediatrici o comunque minori si procedeva allesame eco - contrastografico previo consenso dei genitori . lesame ecografico basale stato sempre integrato da quello contrastografico adoperando apparecchio ultrasonografico ( sequoia , siemens , germania ) dedicato , con tecniche a basso indice meccanico , software specifico in modalit cci ( coherent contrast imaging , 222 pazienti ) e cps ( cadence pulse sequence , 55 pazienti ) dopo somministrazione , tramite accesso venoso periferico , di una quantit di mdc di ii generazione ( sonovue , bracco , italia ) pari a 2 , 4 ml in unico bolo seguito da circa 10 cc di soluzione fisiologica con valutazione prima del parenchima epatico , poi di quello splenico ed infine di quello renale e dei recessi peritoneali sovra e sottomesocolici con documentazione iconografica sia statica che con clips della durata di circa 20 secondi ognuna , eseguite in momenti variabili , in rapporto al reperto diagnostico emerso . 
non si sono mai verificate reazioni allergiche immediate o tardive dopo somministrazione del mdc ev che apparso molto ben tollerato dai pazienti ed abbastanza maneggevole da usare dagli operatori preventivamente formati alla corretta preparazione dello stesso . i pazienti che presentavano un quadro positivo venivano sottoposti ad esame tc multidetettore ( light speed ultra , ge , usa ) prima e dopo somministrazione di mdc iodato ev , con protocollo di acquisizione specifico , multifasico , al fine di stadiare in modo corretto la lesione e di documentare lintegrit o meno della vie escretrice urinaria . 
the patient was instead monitored by contrast - enhanced us performed 12 and 48 h after the initial assessment and a further baseline examination 1 week later , with resolution of the pathological findings . the lesions identified on contrast - enhanced us were classified into three main groups based on a comparison between contrast - enhanced us , aast classification and mdct findings : ( 1 ) minor injury : presence of perirenal haematoma without evidence of renal parenchymal alteration 3 min after the i.v. 
administration of contrast ( 8 cases ) , essentially corresponding to aast grade 1 ; ( 2 ) moderate injury : perirenal haematoma with parenchymal laceration not extending to the renal hilum ( 14 cases ) , corresponding to aast grades 2 and 3 ; ( 3 ) severe injury : characterised by a deep laceration extending to all parenchymal components with involvement of the hilar region , a condition only in part corresponding to aast grades 3 and 4 , as the method does not allow us to establish whether or not the collecting system is intact ( 6 cases )  . discussion and conclusions our study shows that contrast - enhanced us has a high level of diagnostic accuracy in the assessment of renal trauma . 
it should be noted that the technique offers additional advantages over conventional us ( typically , absence of ionising radiation , fast examination times , and ready accessibility ) , in that it allows accurate evaluation of heavily vascular parenchymas such as the spleen , the liver and the kidneys . this enables the identification of lacerations - contusions and nali adoperando lo stesso protocollo desame descritto per la valutazione desordio . le lesioni identificate sono state classificate in cinque diversi gradi di gravit crescente secondo quanto definito dallaast : grado 1 , ematoma subcapsulare ; grado 2 , lacerazione superficiale renale con ematoma perirenale ; grado 3 , lacerazione renale profonda ( superiore al centimetro ) senza interessamento del sistema escretore e evidenza di stravaso urinario ; grado 4 , lacerazione interessante la struttura cortico - midollare ed il sistema escretore , coinvolgimento dellarteria renale principale , trombosi di unarteria segmentaria senza evidenti lacerazioni parenchimali ; grado 5 , grave lesione destruente il nefroparenchima che appare sovvertito con devascolarizzazione , distruzione dellarteria renale , occlusione port - traumatica dellarteria renale [ 5 ]  . risultati nei 277 pazienti valutati , di cui 45 con macroematuria posttraumatica , lecografia basale ha identificato 5 casi positivi per lesione parenchimale renale con associato ematoma perirenale . 
la tcms , integrata da ricostruzione mpvr , conferma il quadro dellesame eco - contrastografico ( c , d )  . haematomas , which appear as more or less irregularly hypoechoic and avascular areas . 
in some cases , it also visualises active bleeding as a hyperechoic blush of contrast material secondary to the interruption of a vascular structure ( fig . 3a , b ; clip 3 ) [ 4 , 69 ]  . 
a further advantage of contrast - enhanced us compared with conventional us is the better and more precise depiction of peritoneal and retroperitoneal fluid collections that results from improved definition of enterocolic wall structures , bladder and abdominal organs [ 10 ]  . nonetheless , there are also some limitations to the technique that have to be borne in mind : cost of the contrast material , need for scanners with dedicated software , need for operators familiar with this type of examination , and longer examination times . 
moreover , contrast - enhanced us does not demonstrate lesions to the urinary tract but only provides discussione e conclusioni dalla nostra esperienza emerge lelevata accuratezza diagnostica delleco - contrastografia nella valutazione del trauma renale . 
vi da precisare che tale tecnica presenta alcuni ulteriori vantaggi rispetto a quelli tipici dellesame ecografico classico ( assenza di radiazioni ionizzanti , rapidit di esecuzione , facilit di accesso ) che sono rappresentati da buona valutazione dei parenchimi fortemente vascolarizzati come milza , fegato e reni . 
2a - c baseline ultrasound ( us ) depicts the perirenal fluid collection ( a )  . contrast - enhanced us with cadence contrast pulse sequencing shows both the free fluid collection and the upper pole laceration ( arrow ) ( b )  . 
quadro tc corrispondente ( c )  . indirect evidence of injuries to the renal vascular pedicle by depicting areas of renal infarction . as regards the first point , in our experience , the use of contrast - enhanced us appears unjustified in all cases of minor injury without haematuria . 
the findings in our patients indicate that contrast - enhanced us was more likely to be positive in the following conditions , listed in order of decreasing frequency : in the presence of traumatic gross haematuria , gross haematuria or microhaematuria following renal biopsy or lithotripsy performed during the previous 12 h , traumatic micro - haematuria and normal urinalysis . 
for this reason , we have adopted the following approach in the workup of minor trauma : baseline us for stable patients with normal urinalysis , followed by contrast - enhanced us after obtaining consent to the use of the contrast agent , only in the event of a diagnostic doubt . 
in patients with a minor trauma and gross or microhaematuria or those who have undergone potentially harmful procedures within the previous 12 h , baseline us is always followed by the contrast examination . this approach allows a more accurate screening of patients not only for renal lesions but also for commonly associated injuries to other organs . 
in addition , it allows considerable savings in terms of both financial and staff resources . ct , preferably with a multidetector technique , remains the gold standard imaging test in the polytrauma patient , as it allows assessment of the renal parenchyma and vasculature and the urinary tract [ 5 , 6 , 1114 ]  . 
sonography with secondgeneration contrast material should be regarded as a technique that allows only definitely positive cases to be selected zione delle strutture parietali enterocoliche , della vescica e dei vari organi endoaddominali [ 10 ]  . accanto ai vantaggi vi da tener conto anche degli svantaggi : elevato costo del mezzo di contrasto , necessit di apparecchi ecografici con software dedicati , abitudine da parte delloperatore a questa tipologia desame , allungamento dei tempi desame . 
lecografia con mdc , inoltre , non documenta le lesioni delle vie escretrici urinarie ma indirettamente quelle del peduncolo vascolare renale identificando aree infartuali parenchimali renali . per il primo punto , dalla nostra esperienza , non sembra giustificato luso delleco - contrastografia in tutti i traumi minori senza ematuria . 
infatti come riportato nei risultati dei pazienti esaminati , la possibilit di una positivit dellesame eco - contrastografico era pi alta , con frequenza decrescente , in pazienti con macroematuria post - traumatica , macroematuria o micrometaturia in pazienti sottoposti nelle 12 ore precedenti a procedure bioptiche renali o di litotrissia , microematuria post - traumatica , pazienti con esame delle urine normale . 
evidence of active blush ( white arrow ) in the right perirenal space with free fluid collection ( asterisk ) ( a )  . multidetector computed tomography ( mdct ) confirms the findings , with optimal definition of perirenal and retroperitoneal extension . 
la clip allegata conferma il quadro ecografico ( b , c )  . delle urine nella norma , nel caso di dubbio diagnostico si procede , previo consenso alleco - contrasto . 
in pazienti con trauma minore con macroo microematuria , o sottoposti nelle 12 ore precedenti a procedure potenzialmente lesive , lecografia basale viene seguita in ogni caso dalleco - contrasto . 
questa condotta inoltre permette un notevole risparmio sia in termini di risorse economiche che gestionali del personale preposto . resta da ricordare che comunque il gold standard nel paziente traumatizzato resta sempre la tc , meglio se multidetettore , tecnica che permette di valutare sia laspetto parenchimale , vascolare ed escretore del rene [ 5 , 6 , 1114 ]  . leco - contrastografia con mdc di ii generazione deve essere considerata come metodica in grado di avviare alla valutazione tc quei pazienti sicuramente positivi per documentare lintegrit della via escretrice e del peduncolo vascolare [ 1416 ]  . 
lecografia con mdc appare metodica fondamentale nel follow - up delle lesioni riducendo cos lesposizione radiante in pazienti spesso giovani , a volte pediatrici , considerando anche che frequentemente la terapia del trauma renale di tipo conservativo [ 4 , 17 , 18 ]  . si ribadisce inoltre che la metodica non pu essere applicata nel soggetto politraumatizzato stabile in quanto questo tipo di paziente deve essere studiato con esame tc comprendente distretti corporei multipli [ 19 , 20 ]  . 
per questo motivo , nella nostra casistica , non compaiono casi di lesioni renali di alto grado in quanto si tratta di situazione critiche , spesso associate a lesioni di altri organi , che necessitano di valutazione tc che permette un adeguato bilancio del trauma . for ct assessment of the integrity of the urinary tract and vascular pedicle [ 1416 ]  . 
scuro 10 , 37134 verona , italy 2dipartimento di scienze radiologiche , policlinico umberto i , universit la sapienza , rome , italy 3reparto di chirurgia e gastroenterologia , policlinico g . 
over a period of 3 months , we prospectively studied 100 consecutive patients ( 36 men and 64 women ; age range 1587 years ; mean age 63 years ) referred to our institute for us imaging of the liver . volumetric acquisition of the liver was achieved with a 3d transducer ( 2.05.0 mhz ) and a logiq 9 us scanner . 
three categories were established : 1 = presence of focal liver lesions ; 2 = doubtful finding ; 3 = absence of focal liver lesions . concordance between volume us and conventional us was calculated by using the k statistic . 
all volume us examinations were technically adequate , allowing exploration of all hepatic sectors , except for five cases that were marred by major respiratory motion artefacts . conventional and volume us identified the same number of focal liver lesions , with the exception of four cases of doubtful findings at volume us . 
in un periodo di tre mesi , sono stati studiati consecutivamente , in modo prospettico , 100 pazienti ( 36 uomini e 64 donne ; range di et : 1587 anni ; media : 63 anni ) giunti alla sezione di ecografia del nostro istituto in regime di ricovero per eseguire un esame ecografico del fegato . 
gli esami ecografici convenzionale e volumetrico hanno identificato lo stesso numero di lesioni focali epatiche , ad eccezione di 4 casi radiol med ( 2009 ) 114 : 792801 conclusions . 
the identification of focal liver lesions on automated volume us is possible , and the examination shows a high level of concordance with conventional us . keywords ultrasound volume ultrasound liver focal liver lesions detection 3d risultati dubbi per la presenza di lesione focale epatica allesame ecografico volumetrico . 
lidentificazione delle lesioni focali epatiche su acquisizioni volumetriche automatiche del fegato possibile , risultando elevata la concordanza a tal fine dellesame volumetrico ecografico rispetto allesame ecografico convenzionale . parole chiave ecografia ecografia volumetrica fegato lesioni focali epatiche identificazione 3d introduction introduzione ultrasound ( us ) is the first - line imaging modality in the study of focal liver lesions [ 1 , 2 ] on account of its ready availability , inexpensiveness , safety and repeatability . conventional us has , however , been shown to have low sensitivity ( 40%71% ) for detecting hepatic metastases [ 35 ] and even lower levels ( 20%38.5% ) for focal liver lesions < 3 cm [ 6 , 7 ]  . 
the introduction of sonographic contrast agents has significantly improved detection and characterisation of focal liver lesions , achieving results often comparable to those of computed tomography ( ct ) and magnetic resonance ( mr ) imaging [ 3 , 810 ]  . 
conventional us is still the initial screening examination for chronic liver disease and oncological follow - up , and its role today remains firmly established in the detection of focal liver lesions [ 1 , 11 ]  . 
nonetheless , us suffers several limitations , both intrinsic and related to the patient ( obesity and bowel gas ) and / or site of the lesion under investigation , and extrinsic and related to the operators experience [ 12 , 13 ]  . 
automated 3d imaging of the liver could lead to reduced subjectivity of us examinations , allowing a reliable retrospective review of examinations following acquisition , similarly to what happens with other digital modalities such as ct and mr imaging . 
this technological application should therefore reduce operator dependency and enhance the effectiveness of cancer screening by improving the localization of lesions , an important aspect in planning conventional or minimally invasive surgical procedures . the aim of this study was to establish the reliability of automated 3d liver imaging in the detection of focal liver lesions by assessing the concordance between volume us and conventional us examinations . lecografia la metodica di imaging di primo livello nello studio delle lesioni focali epatiche [ 1 , 2 ]  . 
lesame ecografico convenzionale ha mostrato tuttavia bassa sensibilit , tra il 40% e 71% nellidentificazione di metastasi epatiche [ 35 ] raggiungendo addirittura valori ancor pi bassi , compresi tra il 20% e 38 , 5% per lesioni focali epatiche inferiori ai 3 cm [ 6 , 7 ]  . 
lintroduzione dei mezzi di contrasto ha apportato un significativo miglioramento nellidentificazione e nella caratterizzazione delle lesioni focali epatiche , con risultati paragonabili in molti casi alla tc e alla rm [ 3 , 810 ]  . 
lesame ecografico convenzionale risulta tuttora il primo esame nello screening delle epatopatie croniche e nei follow - up oncologici ed il suo ruolo , oggigiorno , rimane legato allidentificazione delle lesioni focali epatiche [ 1 , 11 ]  . nonostante ci rimangono alcuni limiti dellecografia di tipo intrinseco , derivanti dal paziente ( obesit e meteorismo ) e / o dalla sede della lesione in studio , sia estrinseci , legati allesperienza delloperatore [ 12 , 13 ]  . 
lacquisizione volumetrica automatica del fegato potrebbe portare ad una riduzione della soggettivit dellindagine ecografia consentendo una affidabile revisione dellesame retrospettiva e successiva allesecuzione tecnica dellesame stesso , analogamente a quanto avviene per altre metodiche di imaging digitali come tc ed rm . questapplicazione tecnologica dovrebbe quindi ridurre la dipendenza delloperatore e incrementare lefficienza dello screening di tumori con una pi accurata localizzazione delle lesioni , fatto questo di particolare importanza nella programmazione terapeutica chirurgica , o con tecniche mini - invasive percutanee . materials and methods patients over a period of 3 months , we prospectively studied 100 consecutive patients ( 36 men and 64 women ; age range 1587 years ; mean age 63 years ) referred to our unit to undergo us imaging of the liver . 
indications for the examination were renal colic , acute pyelonephritis , abdominal colic , arterial hypertension , fever , oncological evaluation , oncological follow - up and follow - up for chronic liver disease . 
 conventional us conventional us was carried out on a logiq 9 us scanner ( ge , healthcare , wauwatosa , wi , usa ; ge medical systems , milwaukee , wi , usa ) using a 3.55 mhz convex - array probe . 
to ensure optimal image quality , 2d b - mode imaging was optimised by appropriate setting of the speckle reduction , gain , rejection , and auto - optimisation parameters . 
conventional us was performed with scans in the epigastric , right hypochondriac and right intercostal region with the patient in the supine position , followed by right intercostal region with the patient in left lateral decubitus . 
 volume us volume us of the entire liver was performed with a volumetric convex - array 4d3c transducer ( 2.05.0 mhz ) using the same logiq 9 scanner and the volume us software volume imaging protocol ( vip )  . 
prior to acquisition , we set the spatial resolution function to maximum ( hi2 ) to improve overall quality of the 3d image and the angle of the volume window to 75 to acquire the largest amount of data possible for each single scan . 
the examination involved an initial volumetric acquisition of the left lobe of the liver , followed by an acquisition of the central sectors with the transducer placed at the level of the hepatic hilum , and finally acquisition of the paramedian and posterior segments of the right lobe with a more lateral scan . 
some patients with hepatomegaly necessitated additional scans ( up to a maximum of seven scans )  . data storage and review data were stored in digital imaging and communications in radiol med ( 2009 ) 114 : 792801 lo scopo del nostro lavoro di stabilire laffidabilit dellacquisizione volumetrica automatica del fegato nellidentificazione delle lesioni focali epatiche , valutando la concordanza tra gli esami ecografici volumetrico e convenzionale . materiali e metodi pazienti in un periodo di tre mesi , sono stati studiati consecutivamente , in modo prospettico , 100 pazienti ( 36 uomini e 64 donne ; range di et : 1587 anni , media : 63 anni ) giunti alla sezione di ecografia del nostro istituto in regime di ricovero per eseguire un esame ecografico del fegato . 
le indicazioni allesecuzione dellindagine erano : colica renale , pielonefrite acuta , coliche addominali , ipertensione arteriosa , febbre , valutazione oncologica , follow - up oncologico , follow - up per epatopatie croniche . 
 ecografia convenzionale lesame ecografico convenzionale stato eseguito con apparecchio ecografico logiq 9 ( ge , healthcare , wauwatosa , wi , usa ; ge medical systems , milwaukee , wi , usa ) , mediante sonda convex 3 , 55 mhz . 
per garantire la migliore qualit di immagine , stata effettuata una ottimizzazione dellimaging 2d b - mode mediante unadeguata impostazione dei parametri speckle reduction imaging , gain , rejection , auto optimization . 
lesame convenzionale stato condotto con scansioni in regione epigastrica , in ipocondrio di destra ed in regione intercostale destra in posizione supina , quindi in regione intercostale destra con decubito sul fianco sinistro . 
 ecografia volumetrica lacquisizione volumetrica dellintero fegato stata effettuata mediante sonda 4d3c convex volumetrica ( 2 , 05 , 0 mhz ) su medesima apparecchiatura ecografica logiq 9 con software volumetrico ecografico vip ( volume imaging protocol )  . 
prima di effettuare lacquisizione , sono stati regolati la funzione spatial resolution , impostata al massimo livello ( hi2 ) per un miglioramento della qualit dellimmagine volumetrica complessiva e langolo della finestra volume , impostato a 75 in modo da comprendere il massimo dei dati acquisibili per ogni singola scansione . 
lesame si svolto inizialmente con lacquisizione volumetrica del lobo sinistro del fegato ; quindi posizionando la sonda allaltezza dellilo epatico si radiol med ( 2009 ) 114 : 792801 medicine ( dicom ) format on a workstation equipped with logiqworks software , which was used to review the cases . volumes acquired frame by frame are displayed in a loop format ( volume review ) , which enables review of the entire volume , providing virtual scans of examined portions of the liver . 
multiplanar and volumetric reviews and reconstructions were possible on both the us system and the workstation , which offered the possibility of varying parameters such as baseline gain , time gain compensation or automatic optimisation during postprocessing . 
concordance between volume and conventional us with regard to the presence or absence of focal liver lesions was calculated by using the k statistic . results patients out of 100 patients studied , 39 were found to have focal liver lesions . 
in particular , 37 benign focal lesions were identified in 32 patients ( hepatic cysts in 23 patients for a total of 28 lesions ; hepatic angiomas in eight patients ; focal nodular hyperplasia in one patient ) , and 13 malignant focal lesions were identified in seven patients ( metastases in four patients for a total of ten lesions ; hepatocellular carcinoma in three patients )  . 
of the 23 patients with hepatic cysts , 17 had had the cysts detected at a previous us examination compared with which the cysts had remained unchanged in ottenuta lacquisizione dei settori centrali ; infine la scansione pi laterale ha acquisito i segmenti paramediani e posteriori del lobo destro . 
talora si sono rese necessarie scansioni aggiuntive ( fino ad un massimo di 7 scansioni ) in pazienti con epatomegalia . archiviazione e revisione i dati sono stati archiviati in formato dicom ( digital imaging and communication in medicine ) su una workstation fornita di software logiqworks . 
sono state possibili rivalutazioni e ricostruzioni multiplanari e volumetriche , sia sullapparecchio ecografico sulla workstation , mantenendo la possibilit di variare in post - processing i parametri quali ad esempio il guadagno basale o il tgc ( time gain compensation ) o lottimizzazione automatica . 
la concordanza dellacquisizione volumetrica con lesame ecografico convenzionale circa la presenza / assenza di lesioni focali epatiche stata calcolata con il k test . risultati pazienti su 100 pazienti studiati , in 39 sono state identificate lesioni focali epatiche . 
in particolare , in 32 pazienti sono state riconosciute 37 lesioni focali benigne ( cisti epatiche in 23 pazienti per un totale di 28 lesioni ; angiomi epatici in 8 pazienti ; iperplasia focale nodulare in 1 paziente ) , ed in 7 pazienti sono state identificate 13 lesioni focali maligne ( metastasi in 4 pazienti per un totale di 10 lesioni ; carcinoma epato - cellulare in 3 pazienti )  . 
 796 radiol med ( 2009 ) 114 : 792801 size ; in the remaining six patients , the cysts were a new finding . conventional us all examinations were technically adequate , enabling sonographic exploration of all hepatic sectors . 
examination time for exploration of the liver to identify or rule out the presence of focal liver lesions varied from 3 to 8 min in relation to the patients build and liver size , with a median time of 5 m tutte le lesioni focali maligne erano state precedentemente diagnosticate con imaging tc ed rm e giungevano alla nostra osservazione in corso di follow - up oncologico . cinque angiomi e liperplasia focale nodulare erano state precedentemente diagnosticate con esame rm ed giungevano per un follow - up ecografico . 
mentre nei restanti sei pazienti le cisti epatiche risultavano un nuovo rilievo . volume us ecografia convenzionale all 3d examinations were technically adequate , enabling sonographic exploration of all hepatic sectors , with the exception of five that were marred by severe respiratory motion artefacts . 
in view of the fact that during this time the system is unable to acquire scans , this time interval was added to each volumetric scan in calculating overall examination time . 
thus , when three volumetric scans were used to acquire the entire liver , overall examination time was approximately 133 = 39 + 503 = 189 s , whereas in the cases requiring seven scans , examination time was 137 = 91s + 503 = 241 s . 
overall time for a diagnostic volume us examination of the liver thus ranged from a minimum of 189 + 1210 = 309 s ( approximately 5 min ) to a maximum of 241 + 1210 = 361 s ( approximately 6 min )  . 
il tempo di esecuzione impiegato per il solo studio del fegato esclusivamente ai fini di identificazione / esclusione di lesioni focali epatiche risultato variabile , a seconda della corporatura del paziente e delle dimensioni del fegato , da 3 ad 8 minuti con un valore mediano pari a 5 minuti . 
 ecografia volumetrica tutti gli esami volumetrici sono risultati tecnicamente adeguati , in relazione alla esplorabilit ecografica di tutti i settori epatici , tranne 5 gravati da importanti artefatti da movimento respiratorio . 
per ottenere lacquisizione dellintero parenchima epatico sono state necessarie da 3 a 7 scansioni volumetriche automatiche della durata di 13 secondi ciascuna , con una media di 4 , 64 acquisizioni / paziente . 
in considerazione del fatto che nel corso di questo arco temporale lapparecchiatura non pu espletare scansioni , lo stesso stato sommato ad ogni scansione volumetrica ai fini del calcolo del tempo complessivo di esecuzione dellindagine . quindi nel caso di tre scansioni volumetriche per lacquisizione dellintero impiegato circa fegato , abbiamo 133 = 39 + 503 = 189 s . 
il tempo impiegato per la revisione dei volumi risultato dal numero di volte che ciascun filmato stato ripetuto per la lettura diagnostica che risultato variabile da 8 a 17 ( mediana = 12 )  . 
il tempo complessivo per un esame diagnostico volumetrico del fegato quindi risultato variabile da un minimo di 189 + 1210 = 309 s pari a circa 5 min ad un massimo di 241 + 1210 = 361 s pari a circa 6 min . gli esami ecografici convenzionale e volumetrico hanno identificato lo stesso numero di lesioni focali epatiche radiol med ( 2009 ) 114 : 792801 fig . 
istantanea ( frame ) del filmato dellacquisizione volumetrica del lobo epatico di destra visionato in modalit volume review . piccola lesione rotondeggiante solida ipoecogena ( freccia ) si identifica alla cupola epatica . table 1 concordance between volume ( vus ) and conventional ( us ) ultrasound presence doubtful absence total presence doubtful absence total kappa statistic presenza dubbio assenza totale k statistica 0.92 0 , 92 tabella 1 concordanza tra esame ecografico volumetrico ( vus ) e convenzionale ( us ) presenza assenza dubbio totale conventional us did not substantially increase the examination time to identify or rule out the presence of focal liver lesions . 
in tutti e 4 i casi dubbi si era in presenza di un fegato disomogeneamente steatosico allindagine ecografica . la concordanza tra acquisizione volumetrica automatica del fegato ed esame ecografico convenzionale ( tabella 1 ) risultata elevata ( k = 0 , 92 )  . 
non stato riscontrato un sostanziale aumento dei tempi di esecuzione dellindagine diagnostica ecografica finalizzata alla identificazione / esclusione di lesioni focali epatiche utilizzando lesame volumetrico rispetto al convenzionale . discussione le nuove tecnologie applicate agli ultrasuoni hanno consentito di ottenere un metodo che acquisisce ad ogni scansione dati volumetrici grazie ai quali possibile ricostruire lintero organo visualizzandolo nellarco di secondi . 
le misurazioni tridimensionali , originariamente , avvenivano con sistemi a mano libera ( free - hand ) e vennero utilizzati principalmente in ambito ginecologico , ostetrico e senologico [ 14 , 15 ]  . 
successivamente sono stati introdotti sistemi automatici che , modificando meccanicamente il trasduttore facendolo traslare o ruotare a predefiniti intervalli spaziali o 798 radiol med ( 2009 ) 114 : 792801 fig . 
la dinamicit dellesame ecografico convenzionale ha consentito di riferire la lesione ad area indenne da statosi . discussion the application of new technologies to us have led to the development of a technique that acquires volumetric data at each scan , thanks to which it is possible to reconstruct and display the entire organ within seconds . 
automated systems were subsequently introduced in which mechanical assemblies make the transducer translate or rotate at predefined spatial or angular intervals ( linear scanning , tilt scanning , rotational scanning )  . these automated systems have allowed organs to be imaged without requiring the usual freehand scans and thus dramatically reducing scanning time , which has always been one of the greater technical limitations of us imaging [ 16 ]  . 
the images must be acquired during breathholding to limit artefacts due to respiratory motion [ 17 , 18 ]  . the data are then sent in dicom format to a workstation where new virtual 3d scans can be obtained of the initial volume of data in any plane . 
the us system used in our study is equipped with the vip volume imaging software angolari ( linear scanning , tilt scanning , rotational scanning ) , hanno consentito di campionare un organo senza le consuete scansioni manuali da parte delloperatore , riducendo drasticamente i tempi di acquisizione dellesame , che da sempre uno dei limiti tecnici pi evidenti dellesame ecografico [ 16 ]  . 
recentemente sono state anche introdotte sonde ( 2d array ) che , attraverso lemissione di un fascio ultrasonoro piramidale che copre il volume di interesse , consentono immagini 3d real - time . 
possibile quindi acquisire ad ogni scansione dati volumetrici grazie ai quali ricostruire lintero organo , visualizzandolo nellarco di secondi . le immagini devono essere acquisite in apnea per limitare artefatti legati a movimenti respiratori [ 17 , 18 ]  . 
i dati vengono poi inviati in formato dicom ad una workstation permettendo di effettuare nuove scansioni virtuali in 3d , in qualsiasi piano di scansione , partendo dal volume dei dati acquisito inizialmente . 
lapplicazione di questo sistema ci ha permesso di ottimizzare il lavoro del medico e di renderlo pi veloce , consentendo di studiare lintero volume epatico in modo rapido e senza dover modificare il decubito del paziente . 
il tempo impiegato nelle elaborazioni in post - processing dei dati volumetrici stato tra i 5 e i 10 minuti ( per i casi dubbi ) che , se valutato nellambito di uno studio ecografico volumetrico , comporta comunque una gestione vantaggiosa dei pazienti in termini di tempi di esecuzione e risoluzione dei radiol med ( 2009 ) 114 : 792801 protocol . 
application of this system allowed us to optimise and speed up the radiologists work by enabling a rapid study of the entire liver volume without having to change the patients position . 
the time required for postprocessing of the volume data was 510 min ( for doubtful cases ) that , if evaluated within the context of volume us , entails a fast patient management in terms of examination time and diagnostic interpretation compared with conventional us . 
the data set of 3d us images can be viewed and processed using techniques common to other digital imaging modalities such as ct and mr imaging , including arbitrary - plane slicing , multiplanar reformatting , nonplanar slicing , volume rendering or surface rendering [ 19 , 20 ]  . 
volume us in fact provides greater morphological , anatomical and pathological details [ 22 ] and could improve the follow - up of focal liver lesions by providing objective and repeatable visualisation of lesions at subsequent examinations . 
 maintaining the possibility of varying the imaging parameters during postprocessing volume reviews and multiplanar and 3d reconstructions on the us system and at the workstation proved to be helpful for clearing doubts regarding the presence and site of some focal liver lesions . in our study , no major differences were found between studying the liver with the vip protocol and conventional baseline us in detecting focal liver lesions . 
 [ 3 ] , the 40% sensitivity and 63% specificity of unenhanced us in detecting metastatic liver lesions are substantially lower than the values reached after contrast administration : 83% and 84% , respectively . 
the objectivity of the volumetric study would heighten the repeatability of contrast - enhanced examinations , especially in detecting metastases in the late phase , which is useful if not indispensable for follow - up during chemotherapy or antineoangiogenic treatments . quesiti diagnostici rispetto allesame ecografico convenzionale . 
il dataset delle immagini ecografiche tridimensionali pu essere visualizzato e adoperato , utilizzando tecniche comuni alle altre metodiche di imaging digitale , come la tc e la rm , ossia secondo piani arbitrari , ricostruzioni multiplanari , non planari o basate sullanalisi della superficie o sullanalisi del volume [ 19 , 20 ]  . 
lecografia volumetrica infatti , fornisce maggiori dettagli morfologici , anatomici e patologici [ 22 ] , ma soprattutto potrebbe permettere un miglior follow - up delle lesioni focali garantendo di visualizzare in successivi controlli , in maniera oggettiva e ripetibile le formazioni segnalate . 
 grazie allapporto delle acquisizioni volumetriche si pu , in tempi brevi , avere i medesimi risultati dellesame ecografico convenzionale per quanto riguarda il numero di lesioni focali epatiche identificate secondo i risultati ottenuti . 
in particolare nel presente studio la funzione volume review ha permesso di rivedere lintero volume ottenendo scansioni virtuali delle porzioni di fegato studiate ; ogni filmato stato ripetuto il numero di volte necessario per lettura diagnostica . le rivalutazioni e ricostruzioni multiplanari e volumetriche , sia sullapparecchio ecografico che sulla workstation , mantenendo la possibilit di variare in post - processing i parametri dellimmagine si sono rivelate utili nel dirimere i dubbi sulla presenza di alcune focalit epatiche e la loro sede . 
nel nostro lavoro , in definitiva non abbiamo rilevato importanti differenze tra lo studio del fegato mediante applicazione del protocollo vip rispetto allesame ecografico basale convenzionale nella identificazione delle lesioni focali epatiche . 
 [ 3 ] la sensibilit e specificit dellesame ecografico basale nella ricerca di lesioni epatiche metastatiche del 40% e 63% rispettivamente , sono sicuramente inferiori ai valori raggiunti dopo somministrazione di mdc , vale a dire del 83% e 84% rispettivamente . 
in un lavoro pubblicato recentemente , lesame ecografico con mezzo di contrasto ( ceus ) ha consentito di identificare il 17% in pi di metastasi epatiche da carcinoma del colon - retto , rispetto allesame basale ; laccuratezza diagnostica che raggiunge la ceus , oggi , compresa tra l85%96% [ 23 , 24 ]  . 
la oggettivit dellesame volumetrico favorirebbe la ripetibilit degli esami contrastografici , specie nella identificazione delle lesioni ripetitive in fase tardiva , utile se non indispensabile nel follow - up in corso di trattamenti chemioterapici o antineoangiogenetici . moreover , by providing a 3d visualisation of lesional microand macrovascularity , the use of contrast media in inoltre lapplicazione del mezzo di contrasto allecografia 3d - 4d seppur ancora limitato , visualizzando in 3d la micro800 radiol med ( 2009 ) 114 : 792801 3d4d us , albeit still limited , could constitute a useful tool for preoperative planning before tumour resection , offering optimal information on vascular anatomy . 
giaccone , palermo , italy 4department of radiology and cardiology , university hospital , parma , italy 5department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands 6cardiology unit , public hospital san gennaro , asl napoli 1 , napoli , italy 7department of diagnostic and interventional radiology , public hospital ferrarotto , catania , italy correspondence to : g . 
runza , via francesco garrano 149 , po box 96018 , pachino , italy , tel . : + 39 - 329 - 9471038 , fax : + 39 - 0931 - 594735 , e - mail : grunza@sirm.org received : 30 march 2008 / accepted : 6 october 2008 / published online : 30 may 2009 springer - verlag 2009 abstract purpose . 
from november 2006 to june 2007 , 21 patients , [ 11 men , ten women ; age standard deviation ( sd ) : 62.710.8 years ] with a history of ascending aorta replacement underwent ecg - gated mdct and were prospectively included in our study . 
ascending aorta replacement had been performed with different surgical techniques : bentall - de bono ( four patients , 19% ) , tirone - david ( five patients , 23% ) , and modified tironedavid with creation of aortic neosinuses ( 12 patients , 57% )  . 
the aortic valve area ( 3.40.2 cm2 ) , the diameter of the sinotubular junction ( 31.61.8 mm ) , the diameter of the neosinuses in the case of modified tirone - david riassunto obiettivi . 
dal novembre 2006 al giugno 2007 sono stati inclusi prospetticamente nel nostro studio 21 pazienti ( 11 maschi , 10 femmine ; et media 62 , 710 , 8 anni ) non consecutivi sottoposti ad intervento di sostituzione dellaorta ascendente . 
i pazienti sono stati sottoposti a sostituzione dellaorta ascendente mediante intervento di bentall - de bono ( 4 pazienti , 19% ) , tirone - david ( 5 pazienti , 23% ) e tirone - david modificato con ricostruzione dei neo - seni ( 12 pazienti , 57% )  . 
in tutti i pazienti la tcmd cardio - sincronizzata ha permesso una chiara valutazione dellanulus valvolare , della radice aortica e dellaorta ascendente per cui stato possibile effettuare accurate misurazioni . 
accurate clinical and therapeutic characterisation of this complex group of diseases requires complete evaluation of the aorta and its main branches and , in particular , of the coronary tree . 
an accurate imaging technique is thus needed that is capable of confirming the clinical suspicion of cardiovascular disease and providing a correct , definitive and timely diagnosis [ 1 ]  . conventional angiography has long been the method of choice for evaluating the thoracoabdominal aorta , but it presents the significant disadvantage of being invasive [ 1 ]  . noninvasive or semiinvasive imaging techniques , such as transthoracic echocardiography ( tte ) , transoesophageal echocardiography ( mr ) ( toe ) , magnetic imaging and multidetector computed tomography ( mdct ) , have all proved to be effective techniques for aortic disease imaging [ 24 ]  . resonance the most frequently used noninvasive technique in clinical practice is ct , as it is readily available and enables , thanks to the recent development of multidetector technology , the simultaneous evaluation of the aorta and coronary tree [ 511 ]  . 
conventional angiography and mr angiography are instead seldom used as initial imaging techniques [ 12 ]  . in fact , thanks to the use of cardiac synchronisation software , mdct has expanded its clinical applications in aortic pathology to become a basic step not only for preoperative nellambito delle patologie cardio - vascolari le alterazioni dellaorta toraco - addominale occupano un posto di primo piano per la necessit di un precoce riconoscimento data la rapidit della loro evoluzione verso condizioni di massima urgenza . 
si tratta di un gruppo complesso di patologie che richiedono per un corretto inquadramento clinico - terapeutico una valutazione completa non solo dellaorta , ma anche dei principali rami arteriosi che da essa prendono origine e principalmente lalbero coronarico . 
da qui la necessit di una tecnica di imaging accurata che possa confermare il sospetto clinico di una patologia cardiovascolare e fornire una diagnosi corretta , completa e quanto pi rapida possibile [ 1 ]  . langiografia convenzionale per molto tempo ha rappresentato la tecnica di scelta nella valutazione dellaorta toraco - addominale , ma presenta quale considerevole svantaggio linvasivit [ 1 ]  . 
di contro , tecniche strumentali noninvasive o semi - invasive quali lecocardiografia trans - toracica ( tte ) , lecocardiografia trans - esofagea ( tee ) , la risonanza magnetica ( rm ) e la tomografia computerizzata multidetettore ( tcmd ) si sono tutte dimostrate efficaci nellimaging della patologia aortica [ 24 ]  . nella pratica clinica , il principale strumento diagnostico non - invasivo utilizzato , poich pi facilmente disponibile nelle strutture ospedaliere , la tc , che grazie al recente sviluppo della tecnologia multidetettore consente una contemporanea valutazione non invasiva dellaorta e dellalbero coronarico [ 511 ]  . 
langio - tc rappresenta , attualmente , lindagine iniziale pi utilizzata per le patologie dellaorta , soprattutto in caso di patologia acuta ; la tte e la tee sono considerate le indagini alternative perch facilmente eseguibili anche in condizioni di emerlangiografia genza al letto del paziente instabile ; radiol med ( 2009 ) 114 : 705717 planning but also for postoperative imaging following surgical replacement of the ascending aorta [ 13 , 14 ]  . the aim of this study was to define the role of ecggated mdct in the evaluation of the postoperative ascending aorta , with special reference to the techniques contribution to the anatomical and functional evaluation of the aortic root following conservative surgery . materials and methods study population from november 2006 to june 2007 , we prospectively enrolled 21 nonconsecutive patients ( 11 men , ten women ; mean age 62.710.8 years ) who had undergone replacement of the ascending aorta . 
the study included patients treated with the bentall - de bono procedure ( n = 4 , 19% ) , tirone - david ( n = 5 , 23% ) and modified tirone - david with the creation of neosinuses ( n = 12 , 57% )  . 
inclusion criteria were heart rate < 70 bpm ( spontaneous or induced after - blocker administration ) and 15to 20 - s inspiratory breath - holding capacity to prevent respiratory motion artefacts from impairing adequate image evaluation and interpretation . 
exclusion criteria were heart rate > 70 bpm , respiratory failure ( unstable clinical condition hindering adequate breath - holding during the scan ) , severe heart failure ( patients with elevated heart rate are usually unable to maintain a supine position ) , severe renal impairment ( serum creatinine > 2 mg / dl ) , hyperkinetic arrhythmias ( e.g. , atrial fibrillation , in particular with rapid ventricular response , extrasystole , etc . ) , thyroid disorders , known allergy to iodinated contrast agents and pregnancy . mdct scan protocol the study was conducted with an mdct scanner ( brilliance 64 , philips medical systems , eindhoven , the netherlands ) with 64 detector rows , each with a minimum thickness of 0.625 m this configuration of 640.625 mm enables the study of a volume corresponding to 40 mm along the patients longitudinal axis during each gantry rotation . all mdct angiographic studies were preceded by an unenhanced baseline scan to evaluate the distribution and amount of coronary calcium ( calcium scoringtm )  . 
calcium scoring was done with the following scan protocol : prospective ecg gating , number of detectors / collimation 161.25 mm , slice thickness 2.5 mm , rotation time 4 s , voltage 120 kv , current 100 mas , craniocaudal scan direction and convenzionale e langio - rm vengono invece raramente utilizzate come modalit iniziale di imaging [ 12 ]  . 
infatti , grazie alle possibilit di utilizzare software per la cardiosincronizzazione , la tcmd ha ampliato il ventaglio delle sue applicazioni cliniche nella patologia aortica rappresentando un tappa fondamentale non solo nel planning preoperatorio , ma anche negli interventi chirurgici di sostituzione dellaorta ascendente [ 13 , 14 ]  . scopo dello studio definire il ruolo della tcmd cardiosincronizzata nella valutazione dellaorta ascendente postchirurgica , con particolare attenzione al contributo che la tecnica pu fornire nella valutazione anatomica e funzionale della radice aortica dopo chirurgia conservativa . materiali e metodi popolazione di studio dal novembre 2006 al giugno 2007 sono stati arruolati prospetticamente un totale di 21 pazienti ( 11 maschi , 10 femmine ; et media 62 , 710 , 8 anni ) non consecutivi sottoposti ad intervento di sostituzione dellaorta ascendente . sono stati inclusi nello studio pazienti sottoposti a sostituzione dellaorta ascendente mediante intervento di bentallde bono ( 4 pazienti , 19% ) , tirone - david ( 5 pazienti , 23% ) e tirone - david modificato con ricostruzione dei neo - seni ( 12 pazienti , 57% )  . 
criteri di inclusione : frequenza cardiaca < 70 bpm ( spontanea o indotta dalla somministrazione di - bloccante ) ; capacit di unapnea inspiratoria per 1520 secondi , consentendo di evitare artefatti dovuti ai movimenti respiratori che impediscono unadeguata valutazione ed interpretazione dellimmagine . 
criteri di esclusione : frequenza cardiaca > 70 bpm ; insufficienza respiratoria ; stato clinico instabile che pu impedire unadeguata apnea durante la scansione ; scompenso cardiaco severo : generalmente sono pazienti non in grado di mantenere la posizione supina con una elevata frequenza cardiaca ; grave compromissione renale ( creatinina sierica > 2 mg / dl ) ; presenza di aritmie ipercinetiche ( ad esempio : fibrillazione atriale , soprattutto con alta risposta ventricolare , extrasistolia , ecc . ) ; disordini tiroidei ; allergia nota ai mezzi di contrasto iodati ; gravidanza . protocollo di scansione tcmd lo studio stato condotto con unapparecchiatura tcmd ( brilliance 64 , philips medical systems , eindhoven , olanda ) con una matrice composta da 64 file di detettori , ciascuno dello spessore minimo di 0 , 625 m la configurazione 708 radiol med ( 2009 ) 114 : 705717 density threshold for calcium detection 130 hu . 
to monitor the arrival of the contrast material , a circular a region of interest ( roi ) was drawn over the ascending aorta , and consecutive axial scans were obtained at that level with a 10s delay from the beginning of the injection . 
scans were always triggered automatically , with a fixed delay of 8.1 s after the threshold enhancement of + 90 hu had been reached within the roi ( table 2 )  . 640 , 625 mm permette di studiare per ogni rotazione il volume corrispondente a 40 mm lungo lasse longitudinale del paziente . tutte le tcmd angiografiche sono state precedute da una scansione senza somministrazione endovenosa di mdc mirata alla valutazione della distribuzione e quantificazione del calcio coronarico ( calcium scoringtm )  . 
il protocollo di scansione per lo score del calcio stato : modalit di sincronizzazione prospettica al tracciato ecg , numero di detettori / collimazione 161 , 25 mm , spessore di strato 2 , 5 mm , tempo di rotazione 4 s , voltaggio del tubo radiogeno 120 kv , tensione del tubo radiogeno 100 mas , direzione della scansione cranio - caudale , soglia di densit per lindividuazione del calcio 130 unit hounsfield ( uh )  . 
all data sets were studied on a workstation ( extended brilliance workspace , version 3.0.1.3200 , philips medical systems , eindhoven , the netherlands ) equipped with cardiac software ( cardiac review and comprehensive cardiac )  . image analysis the evaluation included the replaced portion of the aorta ( valve , root and ascending portion ) and the remnants of the thoracic aorta ( aortic arch and descending aorta )  . 
allo scopo di ottimizzare lopacizzazione dei vasi arteriosi coronarici la sincronizzazione dellinizio della scansione con il passaggio del bolo di mezzo di contrasto stata eseguita mediante tecnica del bolus tracking . 
per monitorare larrivo del mezzo di contrasto , stata posizionata una regione circolare di campionamento ( regione dinteresse , roi ) nel tratto ascendente del lume aortico , quindi , sono state ottenute delle scansioni assiali consecutive sempre allo stesso livello , con un ritardo di 10 secondi dallinizio delliniezione . 
la scansione sempre partita automaticamente con un ritardo fisso di 8 , 1 secondi dopo il raggiungimento allinterno della roi di una soglia di + 90 uh ( tabella 2 )  . ricostruzioni dei dataset sono state effettuate delle ricostruzioni retrospettive basate sul segnale elettrocardiografico per ottenere una qualit dellimmagine priva di artefatti da movimento . 
1 immagini mpr su differenti piani per la valutazione dei diametri della giunzione sino - tubulare dell ' anulus e dei seni di valsalva . telesistolica ( 40% dellintervallo r - r ) e quella telediastolica ( 70% dellintervallo r - r )  . 
tutti i dataset sono stati valutati su una workstation ( extended brilliance workspace , version 3.0.1.3200 , philips medical systems , eindhoven , olanda ) dotata di software cardiaco dedicato ( cardiac review e comprehensive cardiac )  . analisi delle immagini oltre al tratto di aorta sostituito ( valvola , radice e ascendente ) la valutazione stata estesa anche ad i restanti tratti dellaorta toracica ( arco e discendente )  . 
2 immagine mip ( maximum intensity projection ) della radice aortica e dellaorta toracica per la misurazione dei diametri del graft in dacron sul piano sopravalvolare ( a ) ed in prossimit dellanastomosi distale ( b ) , dellarco aortico ( c ) e dellaorta discendente ( d )  . results risultati in 18 patients , ecg - gated mdct provided a clear depiction of the aortic valve annulus , aortic root and ascending aorta , enabling accurate measurements of the valve area , sinotubular junction diameter , neosinus diameter in modified in 18 pazienti la tcmd cardiosincronizzata ha permesso una chiara valutazione dellanulus valvolare , della radice aortica e dellaorta ascendente per cui stato possibile effettuare accurate misurazioni . 
grazie a questi dati , stato possibile calcolare larea valvolare , il diametro della radiol med ( 2009 ) 114 : 705717 giunzione sino - tubulare , il diametro dei neo - seni nel caso di tirone - david modificato e la distanza minima cuspidigraft in fase sistolica . 
tutti i valori ottenuti sono rientrati nel range di normalit dimostrando una buona correlazione ( r = 0 , 89 ) con quelli della tte ( tabella 3 )  . 
3 esempio dei criteri qualitativi / quantitativi utilizzati per la valutazione della distanza tra i lembi valvolari e il graft impiantato ( frecce curve )  . tirone - david procedures and the minimum distance between cusps and the graft during systole . 
4a , b a 72 - year - old man who underwent ascending aorta replacement with bentall - de bono technique for aneuryscomputed tomography ( ct ) angiography performed 6 months approximately after surgery . 
a maximum intensity projection ( mip ) reconstruction showing the mechanical aortic valve ( red curved arrows ) , the prosthetic tube ( arrowheads ) and the distal anastomosis of the graft ( arrows )  . 
b multiplanar reconstruction ( mpr ) images on the supravalvular plane illustrating the centre of the reimplanted coronary ostia and the suture material ( arrows )  . cdx , right coronary artery ; tc , left ma fig . 
a ricostruzione mip rappresentativa della valvola meccanica aortica ( frecce rosse curve ) , del tubo protesico ( punte di freccia ) e dellanastomosi distale del graft ( frecce )  . 
a three - dimensional volume - rendered ( 3d - vr ) reconstructions of the heart and thoracic aorta displaying the distal anastomosis of the dacron graft reinforced with a teflon felt strip ( arrowheads ) and the reimplanted coronary ostia ( arrows )  . 
tepi , epiaortic vessels ; arao , aortic arch ; aoa , ascending aorta ; ao , d descending aorta ; cdx , right coronary artery ; iva , left descending coronary artery ; vdx , right ventricle ; vsn , left ventricle ; tap , pulmonary artery ; adx , right atriuc mpr image in an oblique - axial plane of the native aortic valve . 
a ricostruzione 3d - vr del cuore e dellaorta toracica in cui visualizzata lanastomosi distale del tubo in dacron rinforzato con un anello in teflon ( punte di freccia ) e degli osti coronarici reimpiantati ( frecce )  . 
tepi , tronchi epiaortici ; arao , arco aortico ; aoa , aorta ascendente ; aod , aorta discendente ; cdx , arteria coronaria destra ; iva , arteria discendente anteriore ; vdx , ventricolo destro ; vsn , ventricolo sinistro ; tap , tronco arteria polmonare ; adx , atrio destro . 
una frequenza cardiaca < 70 bpm , spontanea o indotta da bloccanti considerata sufficiente per aumentare il tempo diastolico e la durata telediastolica , momento in cui il cuore , la radice aortica e le coronarie sono quasi privi di movimento [ 15 , 16 ]  . 
 la valutazione della radice aortica di fondamentale importanza per il cardiochirurgo in quanto rappresenta il tratto di aorta che subisce maggiormente lo stress meccaradiol med ( 2009 ) 114 : 705717 fig . 
electrocardiographically ( ecg ) - gated multidetector computed tomography ( mdct ) scan reduces the artefacts secondary to heart beat and allows for accurate evaluation of the dacron graft implanted onto the native aortic valve and of the neosinuses . 
maximum intensity projection ( mip ) in the oblique - sagittal plane ( panel a ) and three - dimensional volume - rendered ( 3d - vr ) ( panel b ) reconstructions of the thoracic aorta to assess the distal anastomosis of the dacron graft ( arrows ) , the neosinuses ( arrowheads ) and the centre of the reimplanted coronary ostia . 
6 uomo di 54 anni sottoposto ad intervento di sostituzione dellaorta ascendente con tecnica tirone - david e ricostruzione dei neo - seni di valsalva . lacquisizione tcmd cardiosincronizzata riduce gli artefatti da movimento pulsatile del vaso e consente unaccurata valutazione della radice aortica e dei neo - seni ricostruiti . 
ricostruzioni mip su piano parasagittale ( immagine a ) e 3d - vr ( immagine b ) dellaorta toracica per la valutazione dellanastomosi distale del graft in dacron ( frecce ) , dei neo - seni ( punte di freccia ) e della sede di impianto degli osti coronarici . 
7 a 59 - year - old man with type a aortic dissection ( according to the stanford classification ) and chest pain of recent onset who underwent replacement of the ascending aorta and aortic valve ( bentall - de bono technique )  . 
c three - dimensional volume - rendered ( 3d - vr ) reconstruction of the heart and aorta displaying the distal anastomosis of the dacron graft , the periprosthetic leakage of contrast material ( arrows ) and the intimal flap in the descending aorta lumen ( arrowheads )  . d maximum intensity projection ( mip ) reformation showing angulation of the aortic graft ( thin arrow ) and the partially calcified intimal flap involving the aortic arch , the descending aorta ( arrowheads ) and the ostium and proximal tract of the left carotid artery ( thick arrow )  . 
7 uomo di 59 anni con dissezione aortica tipo a ( secondo stanford ) sottoposto ad intervento di sostituzione dellaorta ascendente e della valvola aortica ( tecnica bentall - de bono ) e dolore toracico di recente insorgenza . 
c ricostruzione 3d - vr del cuore e dellaorta in cui possibile evidenziare lanastomosi distale della protesi , lo spandimento di mdc periprotesico ( frecce ) ed il flap intimale che coinvolge laorta discendente ( punte di freccia )  . 
d ricostruzione mip che dimostra langolazione della protesi aortica ( freccia sottile ) ed il flap intimale parzialmente calcifico che coinvolge larco , laorta discendente ( punte di freccia ) , lostio ed il tratto prossimale dellarteria carotide sinistra ( freccia spessa )  . 
e , f ricostruzioni 3d - vr del cuore e dellaorta toracica in cui si evidenzia il flap intimale ( punte di freccia )  . radiol med ( 2009 ) 114 : 705717 discussion the latest generation of mdct scanners , with their high spatial and temporal resolution , allows images to be acquired during a single short breath - hold and thus with a high level of anatomical detail [ 5 ]  . 
ecg - gated acquisitions improve the quality of the study by markedly reducing cardiac motion artefacts and providing a clear depiction of the aortic root [ 15 , 16 ]  . 
a heart rate < 70 bpm , whether spontaneous or induced by - blockers , is considered sufficient to increase diastolic time and duration of end - diastole , when the heart , aortic root and coronary arteries are nearly motionless [ 15 , 16 ]  . evaluation of the aortic root is of primary importance for the cardiac surgeon . 
this portion of the aorta is most affected by mechanical stress during surgery , influences valve dynamics and is a common site of complications , as it provides the point of proximal fixation of the gra multiplanar reconstruction ( mpr ) and volume rendering ( vr ) techniques provide the cardiac surgeon with a comprehensive depiction of the aorta , the heart and implanted structures . mdct already represents the gold standard for ruling out the possible major complications of surgery , such as periprosthetic leakage or pseudoaneurysm formation [ 17 ]  . mpr images in standard and curved planes allow for extremely accurate and reliable measurements of the graft and remaining native aorta despite intrinsic bends and possible tortuosity . 
these measurements are essential , as their comparison with the reference values provides the cardiac surgeon with the necessary elements to assess the outcome of surgery . in the case of modified tirone - david procedures with neosinus creation , the distance between the valve leaflets and the graft wall during the systolic phase can also be measured . 
this measurement is regarded as a prognostic index for neosinus creation because a sufficient distance to ensure no contact between the cusps and the graft guarantees integrity of the valve leaflets over time . conventional angiography has long represented the method of choice for evaluating the thoracoabdominal aorta , despite its considerable invasiveness [ 1 ]  . 
noninvasive imaging techniques such as toe , tte and mr angiography have also proved to be effective in imaging aortic diseases [ 24 ] , even though they present some disadvantages : semiinvasiveness and difficult visualisation of the aortic arch due to the interposition of the trachea in the case of toe , and relatively long imaging times , limited availability , and artefacts linked to the presence of the prosthesis in the case of mr angiography . 
in clinical practice , rapidity and simplicity make tte an excellent method for studying the aortic root , although the technique is limited in depicting the middledistal ascending aorta in most cases and does not permit visualisation of the descending aorta . 
additionally , the examination may be undermined by the lack of a suitable nico durante lintervento , ne influenza la dinamica valvolare e costituendo la porzione di ancoraggio prossimale della protesi , pi coinvolta nellinsorgenza di complicanze . 
grazie alle tecniche di ricostruzione mpr e 3d - vr possibile fornire al cardiochirurgo una rappresentazione completa dellaorta , del cuore e delle strutture che ha impiantato . la tcmd rappresenta gi il gold standard per escludere le possibili maggiori complicanze legate allintervento quali spandimento periprotesico o formazioni di pseudoaneurismi [ 17 ]  . 
le immagini mpr nei piani standard e curvilinei , inoltre , consentono di effettuare misurazioni altamente accurate ed attendibili della protesi e della restante aorta nativa malgrado le curve intrinseche del vaso e leventuale tortuosit di decorso . 
queste misurazioni sono di fondamentale importanza , in quanto rapportate a valori di riferimento , forniscono al cardiochirurgo degli elementi per giudicare lesito dellintervento . nel caso di interventi di tirone - david modificato con ricostruzione dei neo - seni , si pu valutare in fase sistolica anche la distanza delle cuspidi valvolari dalla parete della protesi impiantata . 
questa misurazione viene considerata come indice prognostico sulle ricostruzioni dei neoseni , dal momento che , se questa distanza tale da evitare la concussione delle cuspidi con la protesi , lintegrit dei lembi valvolari nel tempo garantita . langiografia convenzionale per molto tempo ha rappresentato la tecnica di scelta nella valutazione dellaorta toraco - addominale , ma presenta , chiaramente , quale considerevole svantaggio linvasivit [ 1 ]  . 
di contro , altre tecniche strumentali non - invasive quali la tee , la tte e langio - rm si sono dimostrate efficaci nellimaging della patologia aortica [ 24 ] , sebbene presentino alcuni svantaggi : la semi - invasivit e le difficolt nella visualizzazione dellarco aortico per linterposizione della trachea nel caso della tee ; i tempi di esecuzione dellindagine piuttosto lunghi , la limitata disponibilit sul territorio , e gli artefatti legati alla presenza delle protesi nel caso dellangio - rm . 
nella pratica clinica , la tte rappresenta , ancora , una modalit eccellente per limaging della radice aortica , in virt della rapidit e semplicit dellindagine , ma presenta limitazioni nella visualizzazione dellaorta ascendente medio - distale , nella maggior parte dei casi , e non consente la visualizzazione dellaorta discendente . 
lo strumento diagnostico non - invasivo pi utilizzato rappresentato , pertanto , dalla tc , che risulta facilmente disponibile nelle strutture ospedaliere e che , grazie al recente sviluppo della tecnologia multidetettore con la possibilit di acquisire scansioni cardiosincronizzate , consente una contemporanea 716 radiol med ( 2009 ) 114 : 705717 acoustic window due to body habitus and artefacts related to the presence of prostheses . 
it is readily available in all hospitals and , with the recent development of the ecg - gated multidetector technique , allows for the simultaneous noninvasive evaluation of the ascending aorta , aortic root and coronary artery tree , almost free of cardiac motion artefacts [ 511 ]  . 
mdct technology with ecg gating has , however , overcome these limitations , and the accurate measurements obtained with multiplanar imaging increase the cardiac surgeons confidence in formulating a judgement on the outcome of ascending aorta replacement procedures . 
speed , noninvasiveness , panoramic imaging and depiction of postoperative complications represent further advantages of mdct angiography compared with the other available imaging modalities . valutazione non invasiva e pressoch priva di artefatti da movimento cardiaco dellaorta ascendente , della radice aortica e dellalbero coronarico [ 511 ]  . 
le accurate misurazioni ottenute grazie alla multiplanarit offerta dellimaging mediante tcmd consentono , inoltre , al cardiochirurgo una migliore confidenza nel formulare un giudizio sullesito dellintervento di sostituzione dellaorta ascendente . 
la rapidit , la non invasivit , la panoramicit , la capacit di identificare le complicanze post - chirurgiche costituiscono ulteriori punti di forza dellangiografia tcmd sopra le altre metodiche disponibili . 
mdct is a reliable tool for the anatomical and functional evaluation of the aortic root , and it provides the cardiac surgeon with new and detailed information needed to formulate a prognostic judgement on the outcome of surgery . conclusioni la tcmd considerata attualmente un momento diagnostico obbligatorio nel paziente con sospetta o nota patologia aortica . 
since the 1970s , technological innovation has been accompanied by the development of methods for the multidisciplinary assessment of the technical , scientific , economic , ethical and social aspects inherent in the use of new technologies . 
because the application of hta is still in its early stages in italy , it is necessary to promote its development by drawing on consolidated international experiences . keywords health technology assessment clinical efficacy of diagnostic procedures evidence - based medicine ( ebm ) health policy riassunto obiettivo . 
dagli anni 70 ad oggi linnovazione scientifica andata di pari passo con lo sviluppo di un metodo di valutazione multidisciplinare che si occupa di analizzare gli aspetti tecnici , scientifici , economici , etici , legali e sociali conseguenti allapplicazione delle nuove tecnologie . 
dato che in italia lapplicazione dellhta ancora ad uno stadio precoce , risulta necessario incentivarne lutilizzo assumendo le gi consolidate esperienze internazionali . parole chiave health technology assessment efficacia clinica delle procedure diagnostiche evidence based medicine ( ebm ) health policy 674 introduction the incessant development and innovation of health technology over the past few decades has called for the parallel development of methods for evaluating the appropriateness of health services and the outcomes and costs of new technologies . 
this latter aspect is evaluated in terms of efficacy ( ability to improve the patients well - being in relation to a specific health problem ) , safety ( the risks inherent in the use of a new technology and assessment of their acceptability ) , cost effectiveness and ethical , social and legal implications . hta is able to provide scientific evidence to inform different decision - making levels , from agencies licensing new pharmaceuticals or medical technologies to health care institutions deciding whether to purchase new equipment or how it should be managed . 
hta therefore integrates the expertise of multiple disciplines capable of supplying the evidence base required for the optimal application of technologies , systems and procedures in medicine . materials and methods our work consisted of three phases . 
in this phase we made use of search tools such as pubmed [ 1 ] , google [ 2 ] , the cochrane central register of controlled trials [ 3 ] , the database of the cochrane collaboration reviews [ 4 ] , the health technology assessment database [ 5 ] and the national health system ( nhs ) economic evaluation database [ 6 ] of the centre for reviews and dissemination ( crd ) , the health evidence network ( hen ) web site [ 7 ] , the web sites of the online journals care [ 8 ] and point of care bulletin [ 9 , 10 ] and the data contained in the trento charter drafted by the italian network of health technology assessment in 2006 [ 11 ]  . 
following a critical analysis of the data obtained from the web site of the international network of agencies for health technology assessment ( inahta ) [ 12 ] , we defined the current composition of this network . 
using the web site of the european network of health technology assessment ( eunethta ) [ 13 ] , we identified the main collaborative projects within the european union health care policies , whereas on the basis of the information provided by the italian network for hta [ 11 ] , we systematically analysed the italian national and regional hta projects . 
the third phase allowed us to define the potential impact of hta on the decision - making radiol med ( 2009 ) 114 : 673691 introduzione lincessante sviluppo ed innovazione delle tecnologie nel campo medico sanitario che si avuto negli ultimi decenni ha richiesto una contemporanea crescita di metodologie , atte a valutare lappropriatezza delle prestazioni , degli effetti prodotti e dei costi delle nuove strumentazioni . 
lhta se da una parte quindi necessario per la valutazione di una o pi propriet tecniche , dallaltra deve considerare limpatto socio economico che la stessa tecnologia pu condizionare . questultima di conseguenza dovr essere valutata congiuntamente sul piano dellefficacia ( capacit di migliorare lo stato di salute del paziente rispetto ad una precisa problematica ) , della sicurezza ( considerazione dei rischi nellutilizzo di una nuova tecnologia e valutazione della loro accettabilit ) , del rapporto tra costi ed efficacia , nonch degli aspetti etici , sociali e medico - legali . lhta in grado di supportare scientificamente diversi livelli decisionali , dalle agenzie che autorizzano limmissione sul mercato di un farmaco o di unaltra tecnologia sanitaria , alle organizzazioni sanitarie che spesso si trovano a doverne valutare lopportunit di acquisto o la modalit di gestione . 
si tratta dunque di una tecnica che integra gli sforzi di molteplici discipline atte a produrre le informazioni necessarie alla luce delle evidenze scientifiche al fine di unottimale applicazione delle tecnologie , sistemi e procedure in medicina . materiali e metodi il lavoro si articolato in tre fasi distinte . 
la prima fase si basata sulla revisione della letteratura recente per lidentificazione dei principi , dei metodi e degli strumenti dellhta , utilizzando come motori di ricerca pubmed [ 1 ] , google [ 2 ] , il database bibliografico cochrane central register of controlled trials [ 3 ] , i database di pubblicazioni e revisioni scientifiche della cochrane collaboration [ 4 ] , lhealth technology assessment database [ 5 ] e lnhs economic evaluation database [ 6 ] del centre for reviews and dissemination ( crd ) , il sito dellhen ( health evidence network ) [ 7 ] , i siti internet delle riviste scientifiche on - line care [ 8 ] e point of care bulletin [ 9 , 10 ] , i dati ottenuti dalla carta di trento , stilata dal network italiano di health technology assessment nel 2006 [ 11 ]  . la seconda fase stata quella della valutazione dello stato attuale dellhta a livello internazionale sia extra - europeo che europeo e nazionale italiano . 
in seguito allanalisi critica dei dati ottenuti dal sito internet dellinternational network of agencies for health technology assessment [ 12 ] si definita la composizione attuale di tale esperienza radiol med ( 2009 ) 114 : 673691 process in health care institutions by analysing several successful cases of hta applied at the institutional level . results hta refers to a systematic , multidisciplinary process of evaluating health technologies and consists of the in - depth assessment of technical attributes , efficacy , clinical safety , indications for use , economic impact and ethical , social and legal implications of the technology . 
in particular , health technology refers to any intervention that may be used to promote health , to prevent , diagnose or treat disease and for patient rehabilitation and management . 
this includes medical equipment , medical devices , pharmaceuticals , diagnostic systems , medical and surgical procedures and patient care pathways , as well as the institutional and organisational settings in which health care is provided [ 11 ]  . 
utilizzando il sito del european network of health technology assessment ( eunethta ) [ 13 ] si sono identificate le principali esperienze di collaborazione dellambito delle politiche per la salute dellue , mentre sulla base delle evidenze prodotte nellambito del network italiano di hta [ 11 ] sono state presentate in maniera sistematica le esperienze di hta a livello nazionale e nelle singole regioni italiane . 
la terza fase ha permesso di definire il potenziale contributo dellhta al processo di decision making allinterno delle aziende sanitarie , analizzando alcuni casi eccellenti di applicazione di tale metodologia a livello organizzativo . risultati lacronimo ( health technology assessment ) hta definisce un processo di valutazione globale e multidisciplinare delle tecnologie utilizzate per lassistenza sanitaria e consiste in una verifica dettagliata delle caratteristiche tecniche , dellefficacia , della sicurezza clinica , delle indicazioni duso , dellimpatto economico nonch degli aspetti etici , sociali e medico - legali della tecnologia stessa . 
in particolare per tecnologia sanitaria si intendono tutti gli interventi usati nel promuovere la salute , prevenire , diagnosticare e trattare una malattia , nellattuare una riabilitazione e nel gestire i pazienti . 
in altre parole , una tecnologia sanitaria comprende le attrezzature sanitarie , i dispositivi medici , i farmaci , i sistemi diagnostici , le procedure mediche e chirurgiche ed i percorsi assistenziali , nonch gli assetti strutturali ed organizzativi nei quali viene erogata lassistenza sanitaria [ 11 ]  . 
in particolare , lhta valuta i seguenti aspetti : performance , applicabilit e indicazioni : la sensibilit e la specificit dei test diagnostici ; la conformit , affidabilit , semplicit di utilizzo , di manutenzione , di sicurezza di uno strumento o procedura sanitaria ; sicurezza clinica : considerazione dei rischi nellutilizzo di una nuova tecnologia ; efficacia : il beneficio che si ottiene sia utilizzando una tecnologia in relazione ad un preciso problema in condizioni ideali ( efficacia teorica : efficacy ) sia in condizioni generali di routine ( efficacia nella pratica : effectiveness ) ; data dal rapporto tra i risultati finali in termini di miglioramento della salute attribuibile alle prestazioni sanitarie erogate ( output ) e le prestazioni stesse ( outcome ) ; economicit ( costo , costo - efficienza , costo - beneficio ) : riguarda , a livello microeconomico , i costi , le tariffe e le modalit di rimborso ; a livello macroeconomico si riferisce , invece , alle conseguenze che nuove tecnologie possono avere sui costi della sanit a livello nazionale o agli effetti che una tecnologia pu avere sullallocazione 676 radiol med ( 2009 ) 114 : 673691 moreover , in view of the longer life expectancy of patients , a more consistent use of technologies and procedures during their lifetime will result in less discomfort , a more trusting relationship with the health care system and improved diagnostictherapeutic performance . 
 with regard to diagnostic imaging , the primary purpose of hta is to ensure the use of technologies that guarantee the most accurate and robust information from diagnostic imaging tests to optimise and increase the efficiency of both the physicians clinical and treatment decisions and the patients outcome . there are several key points to be considered to ensure that the health policy goals of an hta programme are attained : 1 . 
the evaluation of health technologies is not only a necessity for the governance of health care systems but also an opportunity that allows them to deliver qualified health services while controlling expenditure and ensuring a sustainable social and ethical impact . an hta project involves nine steps : 1 . 
in tema di implicazioni sociali particolarmente importante considerare che una strategia di valutazione multidisciplinare porta ad una migliore definizione ed applicazione di progetti che caratterizzano ed ampliano i diritti dellutente del sistema sanitario : definizione dei livelli essenziali di assistenza ; utilizzo delle migliori tecnologie / procedure in termini di costo - beneficio ; migliore informazione al paziente sulle tecnologie / procedure utilizzate . inoltre , vista laumentata aspettativa di vita del paziente , un uso pi coerente delle tecnologie e procedure a cui verr sottoposto nel corso della sua vita comporta sia una riduzione dei disagi , sia un miglior rapporto di fiducia con il sistema sanitario , nonch un miglioramento della qualit della performance diagnostico - terapeutica . 
 per quanto riguarda la diagnostica per immagini lo scopo primario quello di assicurare lutilizzo di tecnologie che garantiscano le pi accurate e solide informazioni possibili dagli esami di diagnostica per immagini per ottimizzare e rendere pi efficienti sia le decisioni cliniche e di trattamento del medico , sia loutcome del paziente . esistono dei punti fondamentali su cui un health technology assessment deve vertere affinch si possano ottenere gli obiettivi di politica sanitaria che si propone : 1 . 
prima di partire con un determinato studio deve esistere tra gli attori interessati e le autorit competenti un coordinamento in modo da ottimizzare i risultati ottenibili , la qual cosa non pu che venir favorita dallesistenza di organismi specificatamente votati allattivit di hta [ 14 ]  . 
useful sources for data and evidence include electronic databases of published literature , electronic databases of clinical and administrative data , institutional or noninstitutional reports and publications , special inventories and specialised generating evidence for an hta project may involve collecting new data . 
tale passaggio , identificato in letteratura come research question , rappresenta una specificazione , in termini empirici , della policy question : significa , in altre parole , inquadrare il problema oggetto di studio 678 radiol med ( 2009 ) 114 : 673691 5 . 
some of the possible effects of an hta project are : acquisition or adoption of a new technology changes to the frequency of use reduction or increase of a technology new allocation of resources within regional or national health care services changes to marketing plans for a given technology [ 8 ]  . hta in the field of diagnostic imaging can make use of a hierarchical model where the general rule holds true that for an imaging examination to be efficacious at a higher level , it must be efficacious at lower levels , although the reverse is not true [ 15 ]  . 
the value of the use of a hierarchical model is based on three key concepts : the concept of the global systems view of diagnosis the production and use of diagnostic information is a continuum a hierarchical model is well - suited to cost - efficiency analysis the use of this type of model to evaluate the various aspects ( technical and nontechnical ) of medical procedures is recommended , as it is simple to use , easily repeatable and helps to ensure important steps are not overlooked by sulla base dellevidenza scientifica , di ben definiti strumenti e misure dellefficacia . 
linterpretazione delle prove implica un processo di classificazione degli studi al fine di conferire a ciascuno di essi un peso e la conseguente opportunit di includerli o meno nella sintesi . 
table 1 shows a model for evaluating clinical efficacy that develops over six successive levels : in level 1 , the properties of a specific imaging technique are evaluated in traditional physical terms such as resolution , sharpness , greyscale and specific measures for digital imaging , as well as the potential for artefacts and operator error . level 2 takes into account that images must be read by a human observer in order to obtain diagnostic information and that accuracy is a function of both image technical quality and interpretation by a human observer . in level 3 , the efficacy of a diagnostic test is evaluated based on the assumption that the imaging information can affect the physicians diagnostic thinking : the more the examination influences the diagnosis , the more helpful it is to the diagnostic process . essere indirizzati ai tre livelli macro - , mesoe micro -  . 
monitoraggio dellimpatto ottenuto dalla valutazione . alcuni degli effetti a cui un hta pu condurre sono : acquisizione o adozione di una nuova tecnologia ; cambiamento della frequenza duso in termini riduttivi o di incremento di una tecnologia ; nuova allocazione di risorse nellambito sanitario regionale o nazionale ; level 4 evaluates the impact of a diagnostic test on the modificazione della pianificazione di marketing di una physicians choice of treatment . determinata tecnologia [ 8 ]  . level 5 analyses the positive impact of a diagnostic test on patient outcome in terms of reduction of morbidity , reduction in number of required health procedures , improved life expectancy and improved quality of life . level 6 addresses the cost benefit and cost - effectiveness of diagnostic imaging procedures to ascertain whether their impact on society is acceptable . table 2 describes the levels of hta of the diagnostic performance of a given technology : level a assesses whether the technology provides good - quality images that are anatomically representative ; level b evaluates whether imaging allows accurate diagnoses to be made ; level c determines the diagnostic impact of imaging ; level d considers the therapeutic impact of the technology ; level e addresses the impact of imaging on the patients health . table 3 illustrates the hta evaluation of the cost - effectiveness of a technology at each level technical and diagnostic performance , diagnostic and therapeutic impact and impact on health . 
2 shows a hierarchical model that includes implementation of a new diagnostic imaging technology in clinical practice to ensure correct use of the imaging system [ 1621 ]  . it should be noted that each hierarchical model starts from an initial assessment of technical / scientific features before passing on to aspects of efficacy , efficiency , patient outcome ( improved survival and morbidity ) and impact on society . 
in more detail , this model requires that each new technology is systematically evaluated on the basis of evidenceper quanto riguarda un esempio di valutazione che sia applicabile in modo specifico alla diagnostica per immagini , si pu utilizzare un modello gerarchico nel quale vale la regola generale che un esame per essere efficace ad un livello alto deve esserlo necessariamente ad un livello pi basso , e non viceversa [ 15 ]  . 
la validit delluso di un modello gerarchico si basa su tre concetti principali : il concetto di globalit della diagnosi ; le informazioni diagnostiche sono un processo continuo ; quello gerarchico un modello che si applica bene allanalisi costo - efficienza . lutilizzo di questo tipo di modello per valutare i vari aspetti tecnici e non delle procedure sanitarie particolarmente consigliato perch di semplice utilizzo , facilmente ripetibile ed aiuta a non trascurare nessun passaggio importante mantenendo un ordine adeguato nel considerare i vari processi costitutivi della procedura stessa . nelle tabelle 13 e fig . 
rapid advances in the field of diagnostic imaging lead the radiologist to continuously adopt new technologies to obtain more and better diagnostic information and to modify the management and ultimately the health of the patient . 
in fact , owing to the lack of clear rules , development strategies and shared and homogeneous health plans in current clinical practice , it takes less than 1 year to introduce new technologies into routine practice , and their introduction is often based on misconceptions that lead to an uneven distribution of technologies and consequently of available resources . 
new technologies and contrast media are thought to necessarily provide better , more diagnostic , images on the basis of subjective views or technical parameters , such as increased spatial or temporal resolution , new acquisition techniques and new visualisation filters . machines and software are introduced before they have been tested in the optimistic conviction that they will no doubt prove useful . 
in collaboration with the university of york , inahta has created a database of reports produced by affiliated subjects . inahta consists of 45 agencies in 23 countries worldwide . another organisation is health technology assessment international ( htai ) , an international scientific society that succeeded the international society for technology assessment in health care ( istahc ) in 2003 . 
for the first time , an italian sits on the board of directors , and the agency set up a specific interest group devoted to hospital - based hta . the cochrane collaboration is an international network of nonprofit institutions set up in 1993 with the aim of nella tabella 2 si descrivono i livelli della valutazione hta delle performance diagnostiche di una tecnologia : nel livello a necessario appurare se la tecnologia valutata garantisce una buona qualit delle immagini e se queste siano anatomicamente rappresentative ; nel livello b si valuta se le immagini ottenute garantiscano che si giunga alla formulazione di una diagnosi accurata ; nel livello c si determina limpatto diagnostico delle immagini ; nel livello d si stima limpatto terapeutico della tecnologia in discussione ed , infine , nel livello e si stima limpatto delle immagini ottenute sulla salute del paziente . 
nella tabella 3 si descrive liter nella valutazione hta del costo - beneficio di una tecnologia sia a livello tecnico , sia di performance ed impatto diagnostico , sia come impatto terapeutico e , in ultimo , come impatto sulla salute . 
2 viene descritto un modello gerarchico che comprende anche , come ultimo passaggio , limplementazione di ogni nuova tecnologia diagnostica per immagini nella pratica clinica , in modo tale da farne derivare un corretto uso dellimaging [ 1621 ]  . 682 radiol med ( 2009 ) 114 : 673691 table 2 hta of diagnostic performance of a technology [ 23 ] level a : technical performance does the technology result in good - quality images that are anatomically representative ? level b : diagnostic performance does imaging allow accurate diagnoses to be made ? level c : diagnostic impact does imaging change diagnostic confidence or the use of subsequent diagnostic tests ? level d : therapeutic impact does the imaging contribute to the management plan ? level e : impact on health does imaging lead to an improvement in patient survival or morbidity ? tabella 2 valutazione hta delle performance diagnostiche di una tecnologia [ 23 ] livello a : performance tecnica la tecnologia valutata garantisce una buona qualit delle immagini e che queste siano anatomicamente rappresentative ? livello b : performance diagnostica le immagini ottenute garantiscono che si giunga alla formulazione di una diagnosi accurata ? livello c : impatto diagnostico le immagini ottenute possono cambiare la sicurezza diagnostica o intervenire sullattitudine alluso di ulteriori esami diagnostici ? livello d : impatto terapeutico limaging contribuisce alla modifica del piano terapeutico ? livello e : impatto sulla salute le immagini ottenute possono condurre ad un miglioramento della sopravvivenza o della morbilit del paziente ? collecting , critically appraising and disseminating information about the effectiveness of health interventions from an evidence - based medicine ( ebm ) perspective through an electronic database called cochrane library that is freely accessible on the internet . 
a major goal of the cochrane collaboration is to sensitise the scientific community , the media and the general public to the risks inherent in the lack of methodological transparency in the world of research and scientific production . the earliest hta experiences developed in the united states in 1972 with the creation of the office of technology assessment ( ota )  . 
this was succeeded by similar agencies , among which is the agency for healthcare research and quality , whose mission it is to investigate health care access , health care costs and outcomes . 
the agency is active in more than 90 projects that aim to test and evaluate the si noti come ogni modello gerarchico parte dalla valutazione iniziale degli aspetti tecnico / scientifici per poi passare a considerare aspetti di efficacia , efficienza , outcome del paziente in termini di miglioramento della sopravvivenza e morbilit , impatto sulla societ ; come gi accennato i primi livelli dellorganigramma devono sempre essere verificati prima di passare al gradino successivo , in modo da scandire i corretti steps nella procedura di valutazione . 
descrivendolo in maniera pi approfondita , questo modello prevede la necessit della valutazione step - by - step di ogni nuova tecnologia sanitaria , tramite studi scientificamente basati , prima dellimplementazione di tale tecnologia . 
i rapidi progressi nel campo della diagnostica per immagini spingono infatti il radiologo alla continua implementazione di nuove tecnologie , perseguendo lobiettivo di ottenere informazioni diagnostiche rilevanti , maggiori e migliori , e modificare il comportamento gestionale del paziente , in sintesi migliorarne la salute . 
in realt nella pratica clinica attuale , in assenza di regole precise , piani di sviluppo e programmi sanitari condivisi e omogenei , si impiega meno di un anno per portare una nuova tecnologia alluso routinario , sulla base di convinzioni errate che conducono ad una distribuzione disomogenea delle tecnologie e conseguentemente delle risorse disponibili . 
si pensa infatti che le nuove tecnologie e i nuovi mezzi di contrasto debbano necessariamente fornire immagini migliori , pi diagnostiche delle vecchie , solo su base soggettiva o di parametri tecnici quali unaumentata risoluzione spaziale o temporale , nuove tecniche di acquisizione , nuovi filtri di visualizzazione e si sostituiscono macchine e software postulando ottimisticamente una loro sicura utilit prima che siano state realmente testate . 
in questo processo non da escludere la pressione del mercato sanitario che identifica la nuova macchina con un grande radiologo e un grande affare , portando allacquisto delle nuove tecnologie a seguito di logiche politico - finanziarie contingenti . stato di realizzazione attuale dellhta per quanto riguarda lo sviluppo attuale dellhta , a livello internazionale presente linahta ( international network of agencies for health technology assessment ) , istituito nel 1993 , che un network di agenzie ed istituzioni con lobiettivo di coordinare lattivit internazionale di hta e di supportare i membri nella definizione di metodiche comuni e condivise di valutazione . 
ad oggi aderiscono radiol med ( 2009 ) 114 : 673691 table 3 hta of cost - effectiveness of a technology at each level [ 23 ] level a : technical performance cost per patient examined level b : diagnostic performance cost per correct diagnosis level c : diagnostic impact cost per invasive test avoided level d : therapeutic impact cost per surgical or medical plan altered level e : impact on health cost per improvement in quality - adjusted life years ( qaly ) tabella 3 valutazione hta del costo - beneficio di una tecnologia ad ogni livello [ 23 ] livello a : performance tecnica costo per paziente esaminato . livello b : performance diagnostica costo per diagnosi corretta . livello c : impatto diagnostico costo di ogni esame invasivo evitato . livello d : impatto terapeutico costo per ogni piano terapeutico medico o chirurgico che viene cambiato in seguito all utilizzo dellesame diagnostico . livello e : impatto sulla salute costo per il miglioramento della qualit della vita c orretto sulla aspettativa di vita ( qaly ) most effective method for transferring research into practice , supporting and promoting evidence - based practice and translating recommendations into resources for providers , patients and health care systems . 
the united states is also home to the most important hta centre worldwide , the emergency care research institute ( ecri )  . canada has six agencies that deal with hta , five of which were created by provincial authorities ( british columbia , alberta , saskatchewan , ontario , quebec ) and only one that works at the national level . 
canadian universities are also particularly interested in hta and often collaborate with the agencies on hta projects . at the european level , two organisations act as coordinators of the various hta programmes . 
hta is particularly well - developed in sweden , france , the united kingdom , spain , germany , holland and denmark [ 14 ]  . allinahta 45 agenzie appartenenti a 23 paesi di tutto il mondo . 
altra organizzazione lhtai ( health technology assessment international ) , societ scientifica internazionale di valutazione delle tecnologie sanitarie , nata nel 2003 dalla chiusura dellistahc ; nellambito di tale agenzia per la prima volta un italiano siede nel board of directory ed stata promossa la costituzione di uno specifico gruppo di interesse dedicato allhospital - based hta . 
bisogna citare anche la cochrane collaboration , network internazionale di enti no - profit nato nel 1993 allo scopo di raccogliere , valutare criticamente e diffondere le informazioni relative alla efficacia degli interventi sanitari , nellottica della cosiddetta evidence based medicine ( ebm ) , attraverso un database elettronico denominato cochrane library , accessibile da tutti su internet . 
un importante compito che la cochrane collaboration cerca di svolgere quello di sensibilizzare sia il mondo scientifico , dei media ed il pubblico pi in generale sui rischi che derivano da una mancanza di trasparenza metodologica nel mondo della ricerca e della produzione scientifica . le prime esperienze di hta si sono sviluppate in america nel 1972 con la costituzione delloffice of technology assessment ( ota )  . 
in seguito alla sua chiusura sono nate altre agenzie simili fra cui la agency for healthcare research and quality la cui missione fondamentale quella di indagare laccesso ai servizi da parte dei cittadini , i costi sanitari e gli esiti ; attualmente lagenzia parte attiva in pi di 90 progetti volti a testare e valutare le metodologie pi efficaci per trasferire i risultati della ricerca nella pratica , per supportare e promuovere la pratica clinica basata sulle evidenze disponibili , per utilizzare le raccomandazioni in termini di migliore utilizzo delle risorse , per lofferta di servizi sanitari , ma anche , e soprattutto , per i pazienti e per il sistema sanitario nel suo complesso . 
 anche presente il maggiore centro di hta del mondo , quello dellecri . provinciali in canada esistono principalmente sei agenzie che si occupano di hta , cinque di queste sono state create dalle autorit ( british columbia , alberta , saskatchewan , ontario e quebec ) e solo una opera a livello nazionale . 
lattivit di produzione di hta reports molto intensa grazie al fatto che esistono dei precisi mandati a livello istituzionale per la realizzazione degli studi e anche grazie alla cultura e allesperienza ormai pluriennale in materia . 
inoltre , anche le universit sono particolarmente attente allhta e si creano spesso collaborazioni con le agenzie per la realizzazione dei lavori . a livello europeo esistono due organizzazioni che fungono da coordinatori delle varie attivit di hta . 
lhta particolarmente sviluppato in svezia , francia , regno unito , spagna , 684 radiol med ( 2009 ) 114 : 673691 germania , olanda , danimarca [ 14 ]  . la svezia da sempre uno dei paesi leader a livello europeo nellutilizzo dellhta nella programmazione di politiche sanitarie . 
oltre che a livello macro , sono poi nate molte altre iniziative che hanno coinvolto le universit , i medici e altri gruppi di professionisti sanitari ( microe meso - )  . 
laspetto molto positivo che nel corso degli anni limpatto dei report di hta via via aumentato e i decision makers hanno fatto riferimento sempre pi ai loro risultati per stabilire priorit e prendere decisioni . 
lanaes ( agenzia nazionale per laccreditamento e la valutazione in sanit ) lagenzia che si occupa pi di altre del hta con particolare riferimento a nuovi dispositivi , procedure , programmi sanitari e offerta di servizi sanitari . listituzione di riferimento in uk il national institute of clinical excellence ( nice ) [ 22 ] il quale , tecnicamente , opera solo nel territorio inglese anche se , informalmente , influenza le scelte di sanit pubblica in scozia e nellirlanda del nord . 
il ministero della salute inglese richiede valutazioni delle tecnologie al nice sulla base delleffettivo beneficio in termini sanitari di una nuova tecnologia nonch delleffettivo miglioramento nella razionalizzazione delle risorse del sistema sanitario nel suo insieme . 
importante sottolineare che in italia , dove non presente un organismo di riferimento per lhta , frequentemente si fa riferimento allattivit del nice . in spagna esiste una agenzia di hta che stata costituita a livello centrale ( aets , agencia de evaluacin de tecnologas sanitarias ) e altre tre agenzie che operano a livello locale , in particolare , in andalusia ( aetsa , agencia de evaluacin de tecnologas sanitarias de andalucia ) , in catalogna ( cahta ) e nei paesi baschi ( osteba )  . lagenzia catalana lunica che viene finanziata ( anche se in piccola parte , 20% ) dal settore privato , rimanendo comunque un ente no profit . 
 per quanto riguarda litalia , limportanza dellhta viene evidenziata dal piano sanitario nazionale 20062008 e dal riconoscimento nellambito del progetto mattoni ospedali di riferimento dellesigenza , per gli ospedali chiamati a diventare ospedali di riferimento , di adottare metodi fig . 
modificato da [ 16 ]  . sweden has always been a leader in europe in the use of hta for planning health policies , and sweden was home to the first national hta agency : the swedish council on hta ( sbu )  . 
sbu was created in 1987 and is directed by a board of representatives of the main organisations involved in the swedish health syste a scientific advisory committee is responsible for research activities that are carried out by a network of more than 300 national experts . in addition to the macro level , other initiatives have been started at the micro and meso levels ( involving universities , physicians and other groups of health professionals )  . 
a very positive aspect is that the impact of hta reports over the years has progressively increased , and policy makers increasingly make reference to them when setting priorities and making decisions . in france , hta involves numerous agencies that collaborate with one another , each one reporting to the ministry of health . 
the national agency for accreditation and assessment in health care ( anaes ) is the agency that is most closely involved in hta , with special emphasis on new devices , procedures , health plans and health services . the reference institution in the united kingdom is the national institute of clinical excellence ( nice ) [ 22 ] , which technically operates in england only , although it informally influences public health care decisions in scotland and radiol med ( 2009 ) 114 : 673691 northern ireland . 
the english department of health commissions nice to carry out technology assessments to establish the effective health benefits of a new technology and effective improvements in the rationalisation of resources of the national health systeit should be noted that in italy , which lacks a reference body for hta , nice reports are frequently referred to . spain has one central hta agency agencia de evaluacin de tecnologas sanitarias ( aets ) and three local agencies operating in andalusia : agencia de evaluacin de tecnologas sanitarias de andalucia ( aetsa ) , catalonia ( cahta ) and in the basque country ( osteba )  . 
the catalan agency receives limited funding ( 20% ) from the private sector only , but it remains a nonprofit organisation . it is also the most active of the four spanish agencies in terms of research and production of hta reports . 
 with regard to italy , the importance of hta is highlighted by the 20062008 national health plan and by the recognition that hospitals applying for benchmark hospital status according to the mattoni project on benchmark hospitals need to adopt hta methods and tools [ 9 , 10 ]  . diffusion of hta in italy has been characterised by several experiences with hospital - based hta by hospital trusts and institutions that are part of the italian hta network . 
the 2003 budget set up the national commission on medical devices ( cud ) as a consultative technical body of the ministry of health whose task it is to define and update the inventory of medical devices and to classify all products into classes and subclasses . 
among its activities , cud set up a working group to evaluate new and old medical technologies employing medical devices and to analyse their clinical benefits and costs to issue data sheets for each medical device . 
in fact , whereas no proper hta projects have been carried out at the central level , interesting studies have been completed at the local level ( veneto region , autonomous province of trento ) , even though the impact of hta in italy is still very limited . however , in 2003 , a project funded by the ministry of health led to the creation of the italian network for health technology assessment ( ni - hta ) [ 11 ] , which laid down the national reference principles for hta in the trento charter ( 2006 )  . 
members are : assessorato alla sanit della regione molise ( regional health department for molise ) agostino gemelli university hospital direzione sanitaria della azienda socio sanitaria n2 e strumenti di hta [ 9 , 10 ]  . 
nel nostro paese la diffusione dellhta stata caratterizzata in particolare dalla moltiplicazione delle esperienze di quello che viene definito hospital based hta da parte di aziende sanitarie ed organizzazioni riunite nel network italiano di hta . 
la finanziaria 2003 ha istituito la cud ( commissione unica sui dispositivi medici ) in qualit di organo consultivo tecnico del ministero della salute , che ha il compito di definire e aggiornare il repertorio dei dispositivi medici e di classificare tutti i prodotti in classi e sottoclassi specifiche . 
nellambito delle proprie attivit , ha istituito un gruppo di lavoro con il compito di valutare nuove e vecchie tecnologie mediche che richiedono luso di dispositivi medici , analizzarne i benefici clinici e i costi correlati al fine di redigere delle schede informative sui dispositivi medici valutati . 
oltre alla cud importante sottolineare che ci sono delle realt locali che fanno ben sperare per la promozione e lo sviluppo dellhta in italia . infatti , mentre a livello centrale non sono stati realizzati dei veri e propri progetti di ta , sono stati conclusi , a livello regionale , studi interessanti ( veneto , provincia autonoma di trento ) , anche se limpatto del ta in italia ancora molto esiguo . 
sempre nel 2003 , sulla base di un progetto finanziato dal ministero della salute , stato costituito il network italiano di health technology assessment ( nihta ) [ 11 ] , che ha espresso nella carta di trento ( 2006 ) i principi di riferimento nazionali per la valutazione della tecnologia . 
fanno parte del network italiano : lassessorato alla sanit della regione molise , il policlinico agostino gemelli , la direzione sanitaria della azienda socio sanitaria n 2 isontina , lirccs policlinico s . 
dannunzio di chieti , il dipartimento delle tecnologie biomediche dellistituto superiore di sanit , lagenzia per i servizi sanitari regionali sezione innovazione , sperimentazione e sviluppo , lirccs casa sollievo della sofferenza opera padre pio , la direzione generale sanit della regione lombardia . 
matteo ( san matteo research and university hospital ) of pavia azienda provinciale per i servizi sanitari di trento ( trento province health care trust ) sezione di epidemiologia e sanit pubblica dipartimento di medicina e scienze dellinvecchiamento delluniversit g . 
the aim of the project and network is to identify common minimum structural , organisational and functional requisites for the routine performance of hta projects at the regional and institutional level within the italian national health service . 
another organisation involved in hta in italy is the italian cochrane centre ( cci ) , established in 1994 with the aim of promoting the activities of the cochrane collaboration in ospedaliera di verona , listituto dermopatico dellimmacolata , lospedale bambino ges , il dipartimento di sanit pubblica e microbiologia delluniversit di torino , losservatorio tecnologie di assobiomedica , lazienda locale socio - sanitaria di rovigo , lazienda sanitaria locale 10 di firenze , il dipartimento di medicina e sanit pubblica delluniversit di verona , lazienda ospedaliera santa maria della misericordia di udine , la societ italiana dei farmacisti ospedalieri e lazienda sanitaria di bressanone . 
obiettivo del progetto , e quindi del network , di proporre una base di discussione per lidentificazione di requisiti comuni minimi strutturali , organizzativi e funzionali per lavvio routinario di attivit di hta a livello regionale e aziendale nellambito del ssn . altra organizzazione coinvolta nellhta in italia il centro cochrane italiano ( cci ) , nato nel 1994 con lo scopo di promuovere in italia ed in alcuni paesi delleuropa meridionale ( spagna , portogallo , francia , grecia ) le attivit della cochrane collaboration . 
il centro cochrane italiano ha sviluppato rapporti di collaborazione con le autorit e le agenzie regionali e nazionali incaricate di promuovere linnovazione e la qualit dellassistenza nel servizio sanitario nazionale . 
nel 2000 il cci ha collaborato formalmente alla realizzazione del piano nazionale per le linee guida ( pnlg ) , coordinato dallagenzia per i servizi sanitari regionali e dallistituto superiore di sanit . 
nel mese di gennaio 2007 stata fondata la si - hta ( societ italiana di health technology assessment ) al termine di un percorso che si sviluppato attraverso vari progetti formativi , programmi di ricerca , attivit in aziende ospedaliere ed universitarie e ha posto litalia , al pari dei paesi pi avanzati , nella condizione di avere una comunit scientifico - professionale dedicata alla valutazione delle tecnologie in sanit . 
nata per fare in modo che i professionisti che si occupano di technology assessment possano incontrarsi per far crescere la cultura del technology assessment nei nostri sistemi regionali e per promuovere la multidisciplinariet basandosi sui principi della carta di trento . 
questo programma , iniziato nel 1995 e coordinato dal centro cochrane italiano , che opera allinterno dellistituto di ricerche farmacologiche mario negri di milano , ha visto la partecipazione di 21 aziende sanitarie e ospedali dellitalia centrale e settentrionale , tra il 1995 e il 1997 , con lobiettivo di introdurre i principi e metodi dellhta nei processi decisionali a radiol med ( 2009 ) 114 : 673691 italy and other southern european countries ( spain , portugal , france and greece )  . 
in this context , the cci offers technical and methodological assistance to health professionals collaborating with the international cochrane groups and organises courses and workshops on the methods used . the cci collaborates with the regional and national authorities and agencies in charge of promoting innovation and quality of care in the national health service . 
in january 2007 , the italian society of health technology assessment ( si - hta ) was established following a series of educational projects , research programmes and activities in hospital and university institutions . 
si - hta was established to allow hta professionals to promote the culture of hta within italys regional health systems and encourage a multidisciplinary approach based on the principles contained in the trento charter . the most interesting national experience is the tripss project , an acronym that translates the english grip ( getting research into practice )  . 
this project , launched in 1995 and coordinated by the cci from the mario negri institute for pharmacological research in milan , saw the participation of 21 health care and hospital trusts of central and northern italy between 1995 and 1997 . 
its aim was to incorporate hta principles and methods in clinical and managerial decision - making processes and to introduce clinical quality of care into the appraisal systems of the health care trusts . 
these efforts have uncovered a series of problems , the most important of which is the separation between the regulations governing the national health system and the principles of efficacy and appropriateness . in this context , four projects have been developed that deal with preoperative assessment , cardiac decompensation , pregnancy and breast cancer . 
among the elements identified as relevant for the transfer of scientific knowledge to clinical practice , mention should be made of continuing education , budgeting , appropriate use of economic incentives and auditing and monitoring of clinical practice . 
projects developed in the veneto region evaluated the appropriate use of coronary angiography and angioplasty , the appropriate use of hospitals and the development of clinical guidelines in the framework of the tripss project . 
the tripss project was followed by tripss ii ( 19992003 ) that , taking advantage of the new rules that were being introduced , aimed to establish an integrated approach among health professionals and managers to define and safeguard quality of care . 
questo sforzo ha portato alla luce una serie di problemi , primo fra tutti lo scollamento tra il quadro normativo di riferimento del servizio sanitario nazionale e i principi di efficacia e appropriatezza . 
fra gli elementi identificati come rilevanti per facilitare il trasferimento delle conoscenze scientifiche nella pratica clinica vanno citati la formazione permanente , il budgeting , luso appropriato degli incentivi economici e i processi di auditing e monitoring della pratica clinica . 
nella regione veneto sono state sviluppate iniziative per valutare lutilizzo appropriato dellangiografia coronarica e dellangioplastica , luso appropriato degli ospedali e lo sviluppo di linee guida cliniche nellambito del progetto tripss . 
il progetto tripss , conclusosi nel 1997 , stato seguito dal tripss ii , lanciato nel 1999 e terminato nel 2003 che , approfittando degli strumenti normativi che si stavano configurando , si proponeva di definire un approccio integrato tra professionisti e managers per la definizione e salvaguardia della qualit dellassistenza . 
lo scopo principale di tale progetto di valutare una metodologia per limplementazione nella pratica clinica di interventi di documentata efficacia e di definire i requisiti essenziali per la realizzazione di tali programmi . 
nonostante siano progetti separati e distinti , possono essere visti come tre passi nella costruzione di un percorso per il trasferimento dei risultati che , partendo da un modello semplicistico basato principalmente sulla diffusione e divulgazione dei risultati , arriva a modelli pi articolati che hanno ridefinito il rapporto tra informazione e pratica clinica . discussione tutti i sistemi sanitari dei paesi occidentali si confrontano quotidianamente con una domanda di servizi sempre pi qualificata e , contemporaneamente , si assiste ad una rapida evoluzione sia delle tecnologie nel settore sanitario sia delle conoscenze in campo scientifico in tema di salute . 
although the tripss projects are separate and distinct , they may be seen as three steps towards the transfer of research to practice that , starting from a simple model based on the diffusion and dissemination of results , arrives at more complex models that have redefined the relationship between information and clinical practice . 
 discussion all national health systems in western countries are facing , on the one hand , an increasing demand for quality health care and , on the other hand , a rapid development of both technologies and scientific knowledge concerning health . this results in the development of new and complex procedures for prevention , diagnosis and treatment that entail high costs for the health care systems . 
in this context , health care policy making clearly needs to be guided by up - to - date scientific evidence and knowledge about the technical , economic , social , legal and ethical implications of decisions . 
such guidance can be provided by hta , which has been referred to as a bridge between scientific innovation and the technical , economic and organisational decisions of policy makers . 
it is a complex and systematic multidisciplinary assessment of the health care , economic , social and ethical impacts both direct and indirect and shortand long term of existing and new health technologies . 
the hta process involves identifying the technologies to be assessed , gathering and analysing existing evidence , synthesising data and sharing the findings and ensuring the diffusion and dissemination of resulting suggestions and recommendations . 
hta is able to support decision making at different levels from agencies authorising the marketing of a drug or health technology to health care institutions deciding whether to purchase new equipment or how it should be managed . 
an hta is principally conseguenza , nascono nuove procedure complesse in tema di prevenzione , diagnosi e trattamento in medicina che , daltro canto , comportano elevati costi economici da sostenere da parte delle strutture sanitarie . 
in questo contesto , si evidenzia chiaramente la necessit di guidare le scelte in tema di politica sanitaria in modo da tenere conto sia delle evidenze scientifiche mediche pi attuali , ma anche degli aspetti tecnici , economici e , pi in generale , delle implicazioni sociali , giuridiche , etiche di queste stesse decisioni in campo sanitario , trovando una integrazione che funga da ponte tra linnovazione scientifica e le decisioni tecniche , economiche e gestionali dei policy makers in campo sanitario . 
lhta un metodo di valutazione accurato delle nuove tecnologie sanitarie per gli aspetti sia scientifici , in termini di appropriatezza e di efficacia , sia per gli aspetti economici , sociali , giuridici ed etici ; si tratta di una valutazione multidisciplinare complessa e sistematica delle conseguenze assistenziali , economiche , sociali ed etiche provocate in modo diretto ed indiretto , nel breve e nel lungo periodo , dalle tecnologie sanitarie esistenti e da quelle di nuova introduzione . 
lhta prevede , quindi , lidentificazione delle tecnologie che necessitano di una valutazione , la raccolta delle evidenze gi esistenti e lanalisi dei dati , la sintesi delle informazioni e la distribuzione dei risultati ottenuti nonch la diffusione e la disseminazione dei conseguenti suggerimenti e raccomandazioni ; si tratta , perci , di un metodo utilizzato per promuovere la salute , prevenire e trattare una malattia , migliorare la riabilitazione o definire criteri di cura e assistenza a lungo termine . 
lhta in grado di supportare scientificamente diversi livelli decisionali , dalle agenzie che autorizzano limmissione sul mercato di un farmaco o di unaltra tecnologia sanitaria , alle organizzazioni sanitarie che spesso si trovano a doverne valutare lopportunit di acquisto o la modalit di gestione . 
un hta si basa principalmente sulla ricerca e verifica delle evidenze scientifiche secondo levidence based medicine ( fondare ogni decisione clinica , diagnostica o gestionale sulla migliore prova di efficacia disponibile nella letteratura medica , al fine di portare direttamente i risultati pi aggiornati della ricerca scientifica nella pratica quotidiana ) : ci comporta la partecipazione dei ricercatori e degli esperti nellambito di indagine , ma anche degli operatori sanitari e dei decisori che , senza la disponibilit delle migliori prove di efficacia , non sono messi nelle condizioni necessarie per decidere se adottare o meno una nuova tecnologia ; accanto agli aspetti prettamente clinici , ne vanno anche evidenziati altri come , ad esempio , quelli sociali , culturali ed etici , che coinvolgono principalmente i cittadini / utenti / pazienti del servizio sanitario pubblico , radiol med ( 2009 ) 114 : 673691 based on research and the analysis of scientific evidence according to the principles of ebm ( all decisions clinical , diagnostic or organisational must be grounded in the best available evidence to allow the transfer of the most recent scientific evidence into routine practice )  . 
this implies the participation of researchers and experts in the field but also of health professionals and decision makers who , in the absence of the current best evidence , are unable to decide whether or not to adopt a new technology . 
these mainly concern the relationship between citizens / users / patients of the public health system and the health system itself and represent an attempt to reconcile , in the decision - making process , the certainty of scientific evidence with the active participation of the effective or potential user . 
hta should therefore be considered a systemic and multidisciplinary process that is indispensable for informing decisions and ensures the optimisation of solutions pursued and the transparency of the decision - making process for all players . 
hta may represent a powerful link between the technicalscientific and the decision - making domains , provided that decision makers can guarantee the conditions for its performance and become accustomed to requesting it . 
one problem that hta has had to face since its inception is the poor communication among the various disciplines involved in the process . firstly , economic assessment is often completely unrelated to the needs of scientific knowledge and technologies . secondly , the various local hta projects often remain unknown and isolated within the international scientific setting . 
to overcome these problems , public and private hta agencies , especially international ones , have set up a wide communication and collaboration network to promote and publicise projects dealing with the assessment and implementation of scientific evidence and health technologies . this network , which is both publicly and privately funded , ensures continuity to the hta process , allowing available technologies to keep up to date with the new scientific knowledge . 
this way , hta may achieve its final goal of transferring the results of theoretical assessments to practical applications that may effectively impact the health system by informing decisions on investments and resource allocation . 
indeed , any hta project can and must act to support health care decisions at all levels [ 1113 ] : macro level : health policy decisions at the national / international level meso level : institutional decisions regarding the acquisition of new technologies or new procedures nonch il servizio stesso nel tentativo di conciliare , nelleffettuazione delle scelte , le garanzie di evidenza scientifica con la partecipazione attiva del loro destinatario effettivo o potenziale : , infatti , ormai universalmente riconosciuto che quando il cittadino partecipa al processo decisionale la sua soddisfazione maggiore e gli esiti clinici migliorano . lhta va , dunque , considerato come un processo sistemico e multidisciplinare indispensabile per la corretta istruzione delle dinamiche decisionali e garante della ottimizzazione delle soluzioni perseguite , oltre che della trasparenza di tali dinamiche nei confronti di tutti gli attori coinvolti ; lhta pu rappresentare un potente strumento di collegamento tra lambito tecnico - scientifico e quello decisionale , posto che questultimo ne garantisca i presupposti per la sua attuazione e , soprattutto , che si abitui a richiederne leffettuazione . 
un problema , non trascurabile nemmeno attualmente , con cui lhta si dovuto scontrare fin dai suoi primi passi la scarsa comunicabilit tra i vari settori che si occupano di questo tipo di disciplina : per prima cosa , la valutazione economica spesso completamente scollegata dalle esigenze delle conoscenze scientifiche e delle tecnologie ; in secondo luogo , i vari progetti di hta a livello locale spesso rimangono sconosciuti e isolati nella realt scientifica internazionale . 
per sopperire a queste problematiche , negli anni le societ pubbliche e private che si occupano di hta a livello soprattutto internazionale hanno sviluppato una fitta rete di comunicazione e collaborazione allo scopo di sviluppare e rendere pubblici i progetti che si occupano di valutazione ed implementazione delle conoscenze scientifiche e delle tecnologie sanitarie ; inoltre lesistenza di questa stessa rete , che attinge sia a finanziamenti pubblici che privati , garantisce una continuit nel tempo di lavoro , necessaria perch le tecnologie a disposizione si mantengano sempre aggiornate e allaltezza delle nuove conoscenze . 
la funzione dellhta pu cos giungere al culmine del suo scopo : portare il risultato di considerazioni valutative teoriche ad una applicazione pratica reale , che possa avere un effettivo impatto sul sistema sanitario in quanto in grado di indirizzare le scelte di investimento e di allocazione delle risorse : infatti un hta pu e deve fungere da supporto nelle decisioni sanitarie a vario livello [ 1113 ] : livello macro : decisioni di politica sanitaria a livello nazionale / internazionale ; livello meso : decisioni aziendali di investimento su nuove tecnologie o sullacquisizione di nuove procedure ; livello micro : decisioni cliniche da parte del medico o di una equipe di medici . questo riveste grande importanza nella definizione dei livelli di assistenza ottimali , nel garantire luso delle 690 radiol med ( 2009 ) 114 : 673691 micro level : clinical decisions by the individual physician or team of physicians this is crucial for defining optimal levels of care and for guaranteeing the use of the most effective technologies and procedures with a view to better coordinating the distribution and delivery of health care services . conclusioni migliori tecnologie e procedure riconosciute dalle evidenze scientifiche per poter coordinare al meglio le modalit di distribuzione e di erogazione di queste tecnologie . conclusions the recent creation of ni - hta and si - hta in italy represents a major step forward as it testifies to a growing interest in hta and marks the beginning of a new phase in the countrys health policy . 
it is increasingly accepted that decisions concerning the use of a drug , diagnostic system or health care process must be preceded by the analysis and definition of various factors including appropriateness , effectiveness , safety , and future sustainability . the lack of planning and common rules makes it necessary to encourage the use of hta to place italy on a par with countries with a longer hta tradition and to exploit the method to guide the development , assessment and use of imaging technologies , thereby enhancing the quality and cost - effectiveness of care . 
hta must therefore be seen as a multidisciplinary effort where physicians with their different clinical and organisational specialisations are often the key players who draw on the contribution of other nonmedical professionals ( physicists , economists , clinical engineers , sociologists , etc . ) to produce valid reports and inform , even at the peripheral level , research , teaching and clinical activity to enhance their effectiveness and efficiency . la recente costituzione in italia del ni - hta e della si - hta ha rappresentato un passo in avanti perch dimostra il crescente interesse sul tema e segnala lavvio di una nuova stagione per la politica sanitaria nel nostro paese . 
 progressivamente cresciuta la consapevolezza che le decisioni che riguardano luso di un farmaco , di un sistema diagnostico , di un processo assistenziale devono essere precedute da un momento di analisi e di definizione di vari fattori quali lappropriatezza , lefficacia , la sicurezza , la sostenibilit futura della stessa tecnologia sanitaria . 
la carenza di programmazione e di regole condivise rende necessario incentivare lutilizzo di tale metodologia per porre la nostra nazione al pari dei paesi pi avanzati nella gestione dellhta e per sfruttarla come strumento per guidare lo sviluppo , la valutazione e lutilizzo delle tecnologie in radiologia al fine di incrementare la qualit e il cost - effectiveness delle cure mediche . 
le complicanze pi comuni sono state la deiscenza del sistema di bendaggio ( 5 , 1% ) , lo scivolamento anteriore del bendaggio ( 3 , 5% ) e linfezione del port ( 1 , 6% )  . 
il bendaggio gastrico per via laparoscopica una procedura relativamente a basso rischio , ampiamente eseguita per trattare lobesit patologica . limaging gioca un ruolo importantissimo nella valutazione precoce e nellindividuazione delle complicanze . parole chiave bendaggio gastrico per via laparoscopica complicanze radiologiche chirurgia bariatrica obesit patologica radiol med ( 2009 ) 114 : 802810 introduction lifestyle diseases such as obesity are on the rise in singapore , similar to most nations that have undergone rapid economic growth . 
the more severe form of obesity , known as grade iii obesity or morbid obesity , is associated with the development of health problems such as dyslipidaemia , hypertension , diabetes mellitus , arthritis and obstructive sleep apnea [ 2 , 3 ]  . 
medical treatment ( conservative treatment ) has been found to be less effective in producing sustainable weight loss ( 5%8% weight loss at 2 years ) compared with bariatric surgery ( average weight loss of 16%35% in 2 years ) [ 4 ]  . surgery for morbid obesity , commonly known as bariatric surgery , is defined as gastrointestinal surgery that produces weight loss in the morbidly obese . 
another malabsorptive procedure , the biliopancreatic diversion with or without duodenal switch is associated with a high percentage of weight loss with a low risk of significant weight regain . however , the effectiveness of the malabsorption of biliopancreatic diversion with or without duodenal switch requires the patient to be supplemented with vitamins above and beyond that of the normal population , with lifelong follow - up . 
another procedure is the endoscopic insertion of an intragastric balloon , a short - term form of weight loss treatment , through the insertion of silicone balloons filled with saline and designed to occupy gastric volume and increase satiety [ 5 ]  . currently , lagb is one of the most frequently performed laparoscopic bariatric operations in many countries [ 6 , 7 ] , including in singapore . 
this study aims to review the complications of lagb , with particular emphasis on the radiological features and the role of imaging in assessing these complications . materials and methods lagb was introduced at our hospital on 30 january 2001 as part of a multidisciplinary weight management programme , and up to 3 october 2006 , 322 patients underwent this procedure . 
eligibility criteria for lagb were the asian adaptation of the criteria set by the society of american gastroenterological surgeons ( sages ) [ 21 ] and the american society of bariatric surgeons ( asbs ) [ 22 ] , namely : 1 . 
 information prospectively entered into the study database included : personal details , race , gender , presurgery polysomnography results , continuous positive airway pressure ( cpap ) requirement , preoperative very low calorie diet ( vlcd ) , age at operation , preoperative weight , height , preoperative bmi , lagb operative details including type of band used and complications , presence of comorbidities such as hypertension , diabetes mellitus , hyperlipidaemia , and postoperative follow - up information . the pars flaccida surgical technique was employed . 
in most patients , the inamed 10 ( allergan inc , irvine , ca , usa ) initially and the swedish band ( johnson & johnson , new jersey , usa ) subsequently 804 radiol med ( 2009 ) 114 : 802810 were used . 
two other bands were less frequently used , namely , the ami ( agency for medical innovations , gtzis , austria ) and the vanguard ( allergan inc , irvine , ca , usa )  . a small virtual 15 - ml gastric pouch was left above the band . 
this placement was later standardised to a site at the midline over the xiphisternu prophylactic broad - spectrum intravenous antibiotics were given at the induction of anaesthesia , and 80 mg of gentamicin was placed at the access port site before skin closure . 
measures to minimise risk of deep vein thrombosis included administering subcutaneous heparin , graduated compression stockings providing calf pumps and padded adjustable leg supports ( yellowfins , acton , ma , usa ) during the surgery , with early ambulation and physiotherapy after the operation . on the first postoperative day , the patient underwent a contrast swallow to confirm satisfactory band placement . the patient was discharged if the contrast swallow was normal and upon a successful trial of liquid ingestion . liquid diet was given for 2 weeks and pureed diet for a further 2 weeks . 
the first adjustment of the band was carried out 56 weeks after lagb , and at that time , between 1 and 3 ml of normal saline was injected into the port using the noncoring 20 - gauge deflected point huber needle ( inamed , santa barbara , ca , usa ) , depending on the band used . 
 on subsequent clinic visits , the band was tightened by incremental injections of normal saline ( ranging from 0.2 to 1 ml , depending on the band used ) into the port . 
band adjustments by percutaneous adjustment of the amount of saline in the band were generally carried out by the surgeon in his clinic except for difficult cases such as patients whose ports were located posterior to the abdominal skin folds or who could not hold their breath adequately to immobilise the port to facilitate port adjustment in the clinic . 
adjustments were aimed at : ( 1 ) sustainable , progressive small amount of weight loss , ( 2 ) sensation of early satiety after meals ( 3 ) and without severe and persistent heartburn or difficulty in swallowing . if a patient became pregnant , the band was completely emptied for the entire duration of pregnancy . 
if the patient did not lose weight despite repeated band tightening , a bandogram [ 24 ] using a water - soluble contrast agent was performed under fluoroscopic guidance to assess for leakage from the port , tubing or band . early films were taken initially with the system filled to half its capacity . 
if no leakage was demonstrated , the system was filled to its maximum capacity , and delayed films were taken after the contrast agent had been left in situ for 10 min to demonstrate small leaks . this study was planned as a study of consecutive lagb patients , and the mean and range of the patient demographic details were presented . 
lagb patients were mainly young adults with a mean age of 35.9 years and a mean bmi of 41.9. ethnic distribution differed from that of the general population in that there was a disproportionately larger number of malays and indians ( table 1 )  . of 313 patients who underwent lagb , 46 developed a total of 51 complications , giving an overall complication rate or 16.3%. 
one patient with anterior band slippage developed acute gastric volvulus and underwent emergency surgery , whereas the rest of the patients with anterior slippage underwent early elective surgery to reduce the slippage or to replace the band . 
il bario mostra un esofago distale dilatato ( frecce ) secondario a chiusura serrata del bendaggio ( punta di freccia ) radiol med ( 2009 ) 114 : 802810 fig . 
limmagine tc assiale mostra lirregolarit del tessuto molle sottocutaneo e la densit intraperitoneale ( frecce ) che rappresenta una fistola cronica a partenza dal port infetto , gi rimosso . three ports ( 1% ) had twisted around the tubing > 90 , making port adjustment even under fluoroscopic guidance impossible . 
to reduce the number of patients with rotated , displaced ports and to make needle adjustment easier , the port position was later standardised and placed anterior to the lower end of the xiphisternu since then , there were no more tubingand port - related problems . there were five ( 1.6% ) cases of port - site infection that fig . 
in one of the nondiabetic patients , the infected port was removed . however , upon complete infection resolution , the second port became infected and had to be removed . respiratory failure postoperatively in our series , one death ( 0.3% ) occurred during the early postoperative period due to aspiration pneumonia . 
the second mortality was a patient who had a perforation detected on the first postoperative day after lagb , after which the band was removed and the patient was discharged well . 
three months later , a second attempt to insert a gastric band failed due to extensive perioesophageal fibrosis . during the postoperative period , he developed a splenic abscess complicated by septic shock and succumbed to multiorgan failure . 
post - lagb patients complicated by early perforation may be asymptomatic or present with epigastric pain with / or without left shoulder - tip pathe first postoperative day contrast swallow demonstrates free extravasation at the perforation site . 
another postulated theory for early band perforation is subclinical infection around the band leading to eventual breakdown in small parts of the band [ 9 ]  . in our institution , 3.5% of lagb patients were complicated by anterior band slippage , the commonest complication in our series and also in most other series [ 27 , 28 ]  . 
oesophageal dilatation postlagb might be caused by preexisting oesophageal dysmotility [ 29 ] , overtightening or successive overzealous tightening of the band stoma , leading to oesophagus gastrification and secondary achalasia . 
 [ 30 ] found that gastric perforation may be underreported , with an incidence rate of 7.5% of gastric erosion on routine gastroscopy studies , of which all patients were asymptomatic at diagnosis . 
 [ 31 ] found that band migration through the gastric wall is a late complication , which should be suspected in patients who have late weight gain , chronic port - cutaneous fistula , neglected insidious development of peritonitis , left subphrenic abscess and protracted port - site infection . 
this typically occurs as a late complication and is postulated to be due to chronic ischaemia caused by pressure from the gastric band on the gastric walls [ 9 ] .there is no consensus regarding the mechanism of this potentially fatal complication [ 12 , 32 ]  . 
the variation in the incidence of this complication in our series compared with other series may be due to the difference in the length of follow - up in post - lagb patients , the variation in schedule of port injection , the amount of saline present in the system and the protocol for gastroscopy of post - lagb patients . 
this difference may be related to the length of follow - up , the position in which the port was placed and the expertise of the surgeons performing adjustments in the clinic . 
patients may gain weight if there is a leakage in the systeduring band tightening , if saline can be freely injected but is not aspirated in the correct amount , the surgeon should suspect a banding - system leak . 
due to the presence of a transverse skin fold of the anterior abdominal wall , the port may lie obliquely , thus causing difficulty in port adjustment in the clinic . 
under fluoroscopic control in a supine position , the omental apron can be adjusted by slight pressure on the abdomen or by the patient holding up the omental apron cranial to the transverse abdominal skin fold until the port is parallel to the fluoroscopic table top , facilitating easy assess to the port . 
in another group of patients who had achieved significant weight loss , the anterior abdominal adipose layer was reduced , and the securing suture may have come undone . during respiration , this mobile port slides on the adipose tissue , thus making the port injection difficult without fluoroscopy . 
strict aseptic technique during port adjustment can help to lower the incidence of infection . in conclusion , laparoscopic adjustable band surgery is a widely practiced method for achieving weight reduction in morbidly obese patients . 
simonetti1 1imaging diagnostics , molecular imaging , interventional radiology , and radiation therapy department , 2public health and cellular biology department , 3pathologic anatomy section , university tor vergata ( ptv ) , viale oxford 81 , 00133 rome , italy correspondence to : c.a. 
our clinical results confirm the diagnostic accuracy of both the mammotome and vacora systems , whereas our cost analysis shows that there is a considerable difference , mostly related to the initial investment . keywords breast vacuum - assisted breast biopsy mammotome vacora cost - effectiveness riassunto scopo . 
presso il nostro centro , dal gennaio a giugno 2006 sono state sottoposte a caratterizzazione istologica mediante prelievo vab 238 lesioni mammarie . di queste 5 / 238 sono state escluse dalla nostra casistica per numero insufficiente di frustoli prelevati . 
i risultati clinici confermano laccuratezza diagnostica di entrambi i sistemi mentre , ai fini della valutazione economica delle procedure , il fattore determinante linvestimento iniziale . parole chiave mammella biopsia mammaria vuotoassistita mammotome vacora costo - efficacia 744 introduction technological progress and the advent of increasingly sophisticated equipment combined with the diffusion of breast cancer screening programmes have led to the detection of a greater number of early lesions . 
in the past , surgical biopsy was considered the only technique capable of characterising these lesions , which very frequently proved benign and did not require surgery [ 14 ]  . 
major technological advances over the past few years have led to the introduction of vacuum - assisted biopsy ( vab ) systems allowing minimally invasive sampling of cores of tissue . 
the purpose of this study was to conduct a cost - effectiveness analysis on two vab systems ( mammotome and vacora ) to optimise the choice of breast biopsy systems . materials and methods two vab systems are currently available at our department : mammotome ( ethicon endo - surgery , cincinnati , oh , usa ) and vacora breast biopsy system ( bard biopsy system , tempe , az , usa )  . 
five out of 238 lesions were excluded from the series , as bleeding prevented sampling of the minimum number of tissue cores established for our study ( at least 18 cores )  . 
however , the vacora system was used for lesions visible on magnetic resonance imaging ( mri ) only , as it is the only mri - compatible device available at our department . 
 before the biopsy procedure , all patients underwent blood tests to assess coagulation status ( complete blood count , prothrombin time , thromboplastin time , antithrombin iii , fibrinogen ) and electrocardiograall patients received detailed information about the procedure , its benefits and radiol med ( 2009 ) 114 : 743756 introduzione lavanzamento tecnologico e la disponibilit di apparecchiature sempre pi sofisticate parallelamente alla maggior diffusione dei programmi di screening , ha portato negli ultimi decenni allindividuazione di un maggior numero di lesioni in fase precoce . 
in passato la biopsia chirurgica veniva considerata come unica possibilit per caratterizzare tali lesioni , che troppo spesso risultavano di natura benigna rendendo dunque inutile lintervento [ 14 ]  . 
negli ultimi anni , grazie ai notevoli progressi tecnologici , sono stati introdotti in commercio sistemi bioptici vuoto assistiti , che consentono il prelievo mini - invasivo di frustoli di tessuto . tali sistemi offrono unaccuratezza diagnostica pressoch sovrapponibile alla biopsia chirurgica , rispetto alla quale hanno tuttavia numerosi vantaggi . 
tali sistemi sono minimamente invasivi , ben tollerati , con assenti sequele cicatriziali , e conducono ad una significativa riduzione dei costi rispetto agli interventi chirurgici tradizionali [ 59 ]  . 
in una realt caratterizzata da risorse economiche sempre pi limitate , lanalisi costo - efficacia uno degli strumenti pi utili per supportare il processo decisionale nella scelta delle tecnologie da impiegare a scopo diagnostico . 
lobiettivo del lavoro quello dunque di confrontare due dispositivi bioptici vuoto assistiti ( mammotome e vacora ) in termini di analisi costo - efficacia per lottimizzazione del processo decisionale nella scelta dei sistemi bioptici in ambito senologico . materiali e metodi nel nostro dipartimento sono disponibili due sistemi di prelievo vuoto - assistito : mammotome ( biopsys ethicon endo - surgery , cincinnati , oh , usa ) ; vacora breast biopsy system ( bard biopsy system , tempe , az , usa )  . 
dal gennaio 2006 al giugno 2006 , sono state prese in considerazione 238 lesioni mammarie consecutive sottoposte a caratterizzazione istologica mediante prelievo vab in pazienti con et compresa tra i 30 ed i 74 anni ( et media 52 anni )  . 
di queste il prelievo vab stato effettuato in 108 / 233 pazienti con il sistema mammotome ed in 125 / 233 con il sistema vacora ; 5 / 238 lesioni sono state escluse dalla nostra casistica in quanto , a causa del sanguinamento , stato possibile prelevare un numero di frustoli radiol med ( 2009 ) 114 : 743756 risks and the possible diagnostic alternatives . 
lesions were located using methods previously described in the literature for each of the imaging modalities [ 1416 ]  . the breast was disinfected , and a local anaesthetic was applied ( 10 cc of 2% lidocaine hydrochloride )  . 
the mammotome system was used with us guidance in 58 / 108 lesions ( 24.9% ) ( 515 mm in diameter , mean 10 mm ) and with mammographic guidance in 50 / 108 cases ( 21.4% ) of clustered microcalcifications . 
la scelta del sistema da utilizzare non si basata sulle caratteristiche iconografiche delle lesioni , bens le pazienti sono state inviate ad uno o allaltro sistema in maniera del tutto casuale . 
 prima della procedura di biopsia percutanea mammaria tutte le pazienti sono state sottoposte ad esami ematochimici , al fine di valutare lassetto coagulativo ( emocromo con conta piastrinica , tempo di protrombina , tempo di tromboplastina , antitrombina iii , fibrinogeno ) ed elettrocardiogramma . 
 la scelta della guida strumentale si basata sullindagine diagnostica che meglio consentiva di individuare la lesione , preferendo quando possibile quella ecografica , sia per il costo minore che per la semplicit e rapidit nellesecuzione della procedura [ 10 ]  . 
la localizzazione delle lesioni avvenuta per ogni guida strumentale con modalit gi descritte in letteratura [ 1416 ]  . si proceduto dunque alla disinfezione della mammella da sottoporre a procedura ed alla somministrazione di anestetico locale ( 10 cc di lidocaina cloridrato diluita al 2% )  . 
il sistema mammotome stato utilizzato in 58 / 108 ( 24 , 9% ) lesioni sotto guida ecografica ( con diametro lesionale compreso tra 5 e 15 mm , valore medio di 10 mm ) ed in 50 / 108 ( 21 , 4% ) casi di microcalcificazioni raggruppate in cluster sotto guida stereotassica con apparecchio dedicato ( tavolo prono fischer mammotest plus / stm )  . 
il prelievo stato effettuato sotto guida ecografica in lesioni nodulari ( 47 / 58 ) , sbarramenti del fascio ultrasonoro ( 9 / 58 ) e su aree di disomogeneit ecostrutturale ( 2 / 58 ) ; sotto guida stereotassica in casi di microcalcificazioni ( 50 / 50 ) , di cui 9 ( 9 / 50 ) apprezzabili allesame mammografico in corrispondenza di aree di distorsione parenchimale da pregresso 746 radiol med ( 2009 ) 114 : 743756 after hormone replacement therapy had been discontinued for at least 2 months . 
one week after the biopsy , an excisional biopsy of all lesions diagnosed as malignant ( invasive carcinoma or carcinoma in situ ) or as atypical ductal hyperplasia was performed , and the final histological diagnoses were compared with those obtained with vab . cost analysis considered the fixed and variable costs for each procedure performed with the mammotome or vacora systems under us , mx or mri guidance . 
the precise determination of indirect costs was thought to be irrelevant to the purposes of the study , as these costs are not directly related to the procedure but to general and administrative costs common to all hospital activities . 
staff costs refer to the cost of each medical and paramedical staff unit ( radiologist , nurse , radiology technician and auxiliary nurse ) directly involved in the procedure and calculated for the mean duration of the procedures . 
for each category , we determined the cost per hour based on working hours under the contract ( radiologist 37.98 / h , nurse 24.66 / h , radiology technician 24.66 / h and auxiliary nurse 22.62 / h ) and the cost per minute , and the latter was multiplied by the mean time each staff unit was engaged in the procedure . 
this item therefore includes the cost of anaesthesia , drugs , dressing material and other disposable items ( gloves , coats , caps , sterile drapes , containers , disposable scalpel , and vab kit )  . 
in particular , with regard to the mammotome system , the items considered included the tubing set , the fluid container and the 11 - gauge probe used for the usand mx - guided procedures , which costs less than the mri - compatible probe . 
the cost of the metal clips is virtually the same with the mammotome or vacora systeour cost analysis assumed the use of metal intervento chirurgico su patologia maligna . il sistema vacora stato utilizzato per il prelievo vab in 58 / 125 ( 24 , 9% ) lesioni sotto guida ecografica ( con diametro lesionale compreso tra 5 e 15 mm , valore medio di 10 mm ) , 50 / 125 ( 21 , 4% ) lesioni sotto guida stereotassica con apparecchio dedicato ( tavolo prono fischer mammotest plus / stm )  . 
inoltre sotto guida rm sono state sottoposte a prelievo vab 17 / 125 ( 7 , 4% ) lesioni ( con diametro lesionale compreso tra 5 e 10 mm , valore medio di 7 , 5 mm )  . 
sono state caratterizzate sotto guida ecografica lesioni nodulari ( 41 / 58 ) , sbarramenti del fascio ultrasonoro ( 8 / 58 ) e aree di disomogeneit ecostrutturale ( 9 / 58 ) ; sotto guida stereotassica microcalcificazioni ( 50 / 50 ) , di cui 7 ( 7 / 50 ) su cicatrice chirurgica da pregressa patologia maligna . in pazienti con il prelievo sotto guida rm stato effettuato su lesioni non individuabili allimaging tradizionale con seguente distribuzione : 7 / 17 casi per la ricerca di foci maligni addizionali in pazienti candidate allintervento chirurgico per patologia maligna sospetta allimaging mammo - ecografico ; 5 / 17 casi per una corretta valutazione della cicatrice chirurgica in pazienti gi sottoposte ad intervento chirurgico per patologia maligna ; 3 / 17 casi per ricerca di focolai di carcinoma mammario occulto in pazienti con linfonodi positivi per metastasi da carcinoma mammario senza evidenza di lesioni primitive allesame mammografico ed ecografico ( cup syndrome ) ; in 2 / 17 casi la rm stata eseguita familiarit per carcinoma mammario . 
dopo una settimana dalla procedura bioptica stata eseguita la biopsia escissionale di tutte le lesioni diagnosticate come maligne ( carcinoma invasivo o in situ ) o come iperplasia duttale atipica ( adh ) e le diagnosi istologiche definitive sono state confrontate con quelle ottenute con il vab . 
 per quanto riguarda lanalisi dei costi relativi ad ogni singola procedura , effettuata rispettivamente con il sistema mammotome e vacora sotto guida ecografica , stereotassica e rm , sono stati presi in considerazione i costi fissi ed i costi variabili . 
to determine depreciation of the mammotome and vacora systems , handpieces and drivers we assumed a typical depreciation period of 5 years and divided the annual cost by the number of procedures per year , estimated by projecting the number performed in the 6 months considered over a 12 - month period . 
annual maintenance of the imaging devices ( us scanner , fisher table or mammography unit , mri scanner ) was instead calculated by considering the total hours of use for each device , again assuming an obsolescence period of 5 years , 45 working weeks per year , and 40 h of work per week . 
 results clinical efficacy all procedures were completed successfully , and no significant complications occurred , with the exception of five cases of bleeding that resolved after manual compression of the breast . 
in 13 / 58 mammotome procedures and in 14 / 58 vacora procedures performed under us guidance , the postprocedural mammograms and sonograms confirmed the complete excision of the nodular lesion . 
the results obtained with the mammotome system were 16 / 108 ( 14.8% ) cases of invasive carcinoma , 22 / 108 ( 20.4% ) cases of carcinoma in situ and 12 / 108 ( 11.1% ) of atypical ductal hyperplasia . 
the results obtained with the vacora system were 24 / 125 ( 19.2% ) cases of invasive carcinoma , 26 / 125 ( 20.8% ) of carcinoma in situ and 16 / 125 ( 12.8% ) of atypical ductal hyperplasia . 
discordant results at mammotome biopsy concerned five lesions diagnosed as carcinomas in situ that turned out to be invasive carcinomas and two lesions diagnosed as atypical ductal hyperplasia that were characterised as carcinomas in situ on excisional biopsy . 
as for the vacora system , six cases of carcinoma in situ turned out to be invasive carcinomas , and two cases of atypical ductal hyperplasia were characterised as carcinomas in situ at final histology ( table 2 )  . all lesions with benign histological examination of cores removed under us and mx guidance were followed up by us and mammography at 6 , 12 and 24 months and were all presi in considerazione solamente i costi diretti delle singole procedure e si ritenuta non necessaria la puntuale determinazione dei costi indiretti , in considerazione del peso marginale che questi rappresentano rispetto allobiettivo dello studio in quanto non direttamente imputabili al costo della singola procedura . 
 in particolare i costi diretti considerati sono stati quelli fissi , che consistono essenzialmente nel costo delle apparecchiature oggetto di analisi ed ausiliarie e vengono quindi indicati nella tabella 1 sotto la voce tecnologia . 
tale voce comprende il costo relativo ai due sistemi ( mammotome e vacora ) , utilizzati sotto guida ecografica ( us ) , stereotassica ( mx ) e di risonanza magnetica ( rm )  . 
per quanto riguarda i costi variabili , essi si compongono del costo del personale e materiale di consumo . la voce costo del personale comprende il costo relativo alle unit di personale sanitario e tecnico , ( medico radiologo , infermiere , tecnico di radiologia ed ausiliario ota ) , direttamente coinvolte nella procedura , per la durata media degli interventi rilevata nei casi trattati . 
il relativo costo determinato partendo dal costo annuo ( comprensivo di oneri diretti e riflessi ) di ciascuna qualifica professionale previsto nel contratto nazionale , calcolando il costo ora in base allorario settimanale previsto da contratto ( medico radiologo 37 , 98 euro / h , infermiere 24 , 66 euro / h , tecnico di radiologia 24 , 66 euro / h ed ausiliario ota 22 , 62 euro / h ) , ottenendo quindi il costo / minuto e quindi moltiplicando il costo / minuto per il tempo medio di impiego di ciascuna unit di personale nelle specifiche procedure valutato in base alla nostra esperienza . 
in tale voce quindi compreso il costo dellanestesia , dei farmaci , del materiale di medicazione e di altro materiale monouso ( guanti , camici , cuffie , telini sterili , contenitori , bisturi monouso , nonch del kit monouso )  . 
in particolare per quanto concerne il sistema mammotome sono state prese in considerazione le voci relative al set di tubi , al contenitore dei fluidi ed infine alla sonda 11 gauge , utilizzata nel nostro studio , sia per le procedure effettuate sotto guida ecografica che stereotassica , il cui costo risulta inferiore a quello della sonda rm - compatibile . 
in particular , the mammotome system had 84.4% sensitivity and 100% un periodo di ammortamento , come per tutte le alte tecnologie , di 5 anni e quindi di ripartire il costo annuo sul numero di esami annuali calcolati proiettando il numero degli esami effettuati nei sei mesi considerati sui 12 mesi . 
 il canone di manutenzione annuo per le guide strumentali ( ecografo , tavolo di fisher o mammografo , rm ) invece stato calcolato considerando le ore di utilizzo complessivo delle singole apparecchiature , ipotizzando sempre un periodo di obsolescenza di 5 anni , 45 settimane lavorative annuali e 40 ore di attivit settimanali . 
the vacora system had 86.2% sensitivity and 100% specificity , whereas the rate of underestimation was 23.1% for carcinoma in situ and 12.5% for atypical ductal hyperplasia . risultati efficacia clinica cost analysis the initial costs of the two devices are significantly different . the purchase price of the mammotome system is 42 , 217.20 inclusive of vat plus 5 , 028 for the ultrasonic handpiece , 9 , 733.20 for the stereotactic driver , and 27 , 231.60 for the upgrade required to use the system under mri guidance . 
the fixed costs are higher with the mammotome system owing to its higher purchase price and maintenance costs and the need for ultrasonic handpieces , mx drivers and dedicated programmes ( for mri guidance ) , which are not required with the vacora systethe variable costs are also higher for the mammotome system , independently of the guiding device , owing to the higher cost of supplies , with staff and procedures time being equal . 
results of the cost analysis for the two systems used under us , mx and mri guidance are shown in tables 35 , respectively . hospital reimbursement in the period considered , day surgery and outpatient procedures were reimbursed by the regional bodies according to the regional tariff nomenclature for ambulatory care specialist services approved with resolution no . 
 note that the outpatient tariffs for the us - guided procedures would not be sufficient to cover the costs for the hospital , regardless of whether the mammotome or vacora system was used . 
to date , no regional reimbursement exists for procedures performed under mri guidance , probably because they are still uncommonly performed in the lazio regional health service . discussion in recent years , several papers have widely confirmed the diagnostic value of percutaneous vab performed with con lutilizzo di entrambi i sistemi tutte le procedure sono state portate a termine con successo e non si sono verificate significative complicanze periprocedurali , ad eccezione di 5 casi di sanguinamento che si sono risolti con la compressione manuale della mammella . 
in 13 delle 58 procedure effettuate con il sistema mammotome ed in 14 delle 58 procedure eseguite con il sistema vacora sotto guida ecografica , i controlli mammo - ecografici postprocedura hanno confermato lavvenuta escissione totale della lesione nodulare . 
i risultati ottenuti al prelievo vab con il sistema mammotome sono stati rispettivamente : 16 / 108 ( 14 , 8% ) casi di carcinoma invasivo , 22 / 108 ( 20 , 4% ) casi di carcinoma in situ e 12 / 108 ( 11 , 1% ) casi di iperplasia duttale atipica . 
i risultati ottenuti al prelievo vab con il sistema vacora sono stati rispettivamente : 24 / 125 ( 19 , 2% ) casi di carcinoma invasivo , 26 / 125 ( 20 , 8% ) casi di carcinoma in situ e 16 / 125 ( 12 , 8% ) casi di iperplasia duttale atipica . 
per quanto riguarda il sistema mammotome , cinque delle lesioni diagnosticate come carcinoma in situ si sono rilevate carcinomi invasivi e due delle lesioni diagnosticate adh sono state caratterizzate come carcinoma in situ alla biopsia escissionale . 
con il sistema vacora sei casi di carcinoma in situ si sono rivelati carcinoma invasivo e due casi di adh sono stati caratterizzati come carcinoma in situ allistologico definitivo ( tabella 2 )  . tutte le lesioni diagnosticate come benigne alla diagnosi istologica dei frustoli asportati sotto guida ecografica e stereotassica sono state inserite in un programma di follow - up mammo - ecografico ogni 6 / 12 / 24 mesi e si per tutte confermata la non evolutivit allimaging . 
le lesioni caratterizzate come benigne alla diagnosi istologica su frustoli asportati sotto guida rm ( 3 / 17 ) , sono state rivalutate con esame rm dinamico dopo 1 settimana dalla procedura . 
both systems allow preoperative diagnosis and determination of the main biological prognostic markers ( receptor status , proliferation and c - erb overexpression indices ) that are essential for treatment planning [ 8 , 12 ]  . 
in particolare con il sistema mammotome i valori sono del 84 , 4% di sensibilit e 100% di specificit ; nella nostra serie la sottostima del carcinoma in situ risultata del 22 , 7% mentre per ladh pari al 16 , 7% . 
con il sistema vacora i valori di sensibilit e specificit sono stati rispettivamente del 86 , 2% e del 100% , mentre la sottostima per il carcinoma in situ pari al 23 , 1% e per ladh del 12 , 5% . 
il costo di acquisto del sistema mammotome di 42217 , 20 euro , iva inclusa , a cui si aggiungono 5028 euro per il manipolo ecografico , 9733 , 20 euro per il driver stereotassico ed infine 27231 , 60 euro per laggiornamento necessario per lutilizzo del sistema sotto guida rm . 
i costi fissi risultano maggiori nel caso di utilizzo del mammotome in quanto il prezzo di acquisto del sistema e della manutenzione maggiore ed inoltre lutilizzo di tale sistema richiede lutilizzo di manipoli ecografici , drivers stereotassici e programmi dedicati ( nel caso della guida rm ) non richiesti invece nel caso di utilizzo del vacora . 
anche i costi variabili risultano superiori nel caso di utilizzo del mammotome indipendentemente dalla guida utilizzata in quanto la voce materiali di consumo maggiore , a parit di personale impiegato e di durata delle procedure . 
vacora allows single cylindrical cores consistent in size and weight ( 150170 mg ) to be sampled during a single probe insertion [ 18 ]  . sensitivity and specificity of the two technologies observed in our study are in line with those previously reported [ 19 , 20 ] for both systems . 
the rate of underestimation of invasive cancer as carcinoma in situ was close to 23% in our series , whereas that of carcinoma in situ as atypical ductal hyperplasia was 12%16% . all tissue samples obtained with the two devices were intact and judged adequate for histological examination and , although the vacora samples were larger and heavier than the mammotome samples , there were no cases of interpretation difficulties or significant diagnostic differences in the material obtained . 
the higher fixed costs are due to the higher purchase price and a need for more accessories ; the higher variable costs are related to a greater use of supplies . 
the staff cost is equivalent , as the composition and time commitment of the medical and paramedical team are the same . with regard to the mammotome accessories , it should be regione lazio n . 
anche se linvasivit delle procedure minima , ma data la delicatezza dellintervento nonch i risvolti psicologici per la paziente , i prelievi vab vengono generalmente eseguiti , con entrambe le tecnologie , in regime di day surgery . 
 si nota che le tariffe ambulatoriali per le procedure eseguite sotto guida ecografia risulterebbero non sufficienti a coprire i costi della struttura sia nel caso che venga usato il mammotome che nel caso in cui venga usato il vacora . 
entrambe i sistemi consentono di ottenere campioni tissutali adeguati al fine di una diagnosi preoperatoria , permettendo di conoscere i principali markers biologico - prognostici ( assetto recettoriale , indici di proliferazione e sovraespressione di c - erb ) indispensabili per la pianificazione terapeutica delle lesioni mammarie maligne [ 8 , 12 ]  . 
il sistema mammotome permette tramite un unico inserimento della sonda il prelievo di multipli frustoli di tessuto la cui ispezione risulta semplice , in quanto il sistema consente un controllo visivo costante del prelievo durante la procedura . 
il sistema vacora un sistema che offre maggiore maneggevolezza , rispetto al sistema mammotome , essendo un sistema palmare ( 3640200 mm ) dotato di basso peso ( 400 g )  . 
la sottostima del carcinoma in situ rispetto al carcinoma infiltrante stata , nella nostra serie , prossima al 23% , mentre per liperplasia duttale atipica rispetto al carcinoma in situ stata variabile dal 12% al 16% circa . i campioni tissutali sono risultati integri e adeguati al fine dellesame istologico con entrambi i dispositivi utilizzati , e bench con il sistema vacora essi siano risultati di dimensioni e peso maggiori a quelli prelevati con il sistema mammotome , in nessun caso vi sono stati problemi interpretativi da parte dellanatomo patologo , n significative differenze ai fini della diagnosi sul materiale ottenuto . 
 dalla nostra analisi dei costi emerge che sia i costi fissi che i costi variabili , e quindi i costi totali , sono superiori per le procedure effettuate con mammotome piuttosto che con il vacora . 
questa differenza trova origine , per quanto concerne i costi fissi , nel maggior costo di acquisto delle apparecchiature e nella necessit di una dotazione strumentale maggiore nel caso del mammotome e nel maggior utilizzo di materiale di consumo per quanto riguarda i costi variabili . 
cost - effectiveness analysis allows the objective assessment of new technologies and the rationalisation of resources , leading to the protection of public health at affordable healthcare costs . ( 42217 , 20 euro iva compresa ) a cui devono essere aggiunti il manipolo da utilizzare sotto guida ecografia ( 5028 , 00 euro iva compresa ) , il driver necessario per la guida stereotassica ( 9733 , 20 euro iva compresa ) e laggiornamento in rm ( 27231 , 60 euro iva compresa )  . 
cornalba1 1servizio di radiologia diagnostica e interventistica , universit di milano , ospedale san paolo , milano , italy 2servizio di radiologia , istituto humanitas , bergamo , italy 3reparto di ginecologia ostetricia , clinica mangiagalli , milano , italy correspondence to : g . 
pompili , via di rudin 8 , 20142 milano , italy , tel . : + 39 - 02 - 81844798 , e - mail : gpompili@sirm.org received : 12 may 2008 / accepted : 18 july 2008 / published online : 29 may 2009 springer - verlag 2009 abstract purpose . 
fifty - eight women ( age range 1430 years , mean 20.9 ) with primary amenorrhea were studied with mri performed with a 1.0 - t superconducting magnet ( philips nt intera )  . 
t1 - weighted images were acquired in the axial and coronal planes ( tr 470 , te 15 , fov 350 , 4 - mm sections with a 0.6 - mm intersection gap , nsa 3 )  . 
valutare laccuratezza della rm in donne con amenorrea primaria , con sospetta sindrome mayerrokitansky - kuster - hauser ( mrkh ) ( assenza congenita di vagina e utero con presenza di ovaie normali )  . 
immagini turbo spin - echo t2 pesate sono state acquisite sui piani sagittale , assiale e coronale con i seguenti parametri : tr 47506686 , te 100120 , fov 350375 , sezioni di 45 mm con interspazio di 0 , 40 , 5 mm i , nsa 6 . 
immagini t1 pesate sono state acquisite sui piani assiale e coronale ( tr 470 , te 15 , fov 350 , sezioni di 4 mm di spessore con interspazio di 0 , 6 mm , nsa 3 )  . 
due radiologi esperti hanno valutato gli esami in consenso per stabilire la presenza , sede e morfologia di vagina , utero , ovaie , reni ed eventuali ulteriori malformazioni pelviche . 
la sensibilit della rm stata dell81 , 42% e c stato un buon accordo con la laparoscopia ( k cohen 0 , 55 ) e un completo accordo nella identificazione delle cavitazione dei residui tra rm e ecografia intraoperatoria . 
strong cooperation between radiologists and surgeons is highly recommended . ( 82 , 1% ) , policistica in 10 ( 17 , 8% ) ; sede pelvica in 47 ( 83 , 6% ) , extrapelvica in 8 ( 14 , 5% )  . 
una forte cooperazione tra radiologo e chirurgo fortemente raccomandata . keywords magnetic resonance ( mr ) mrkh , mayer rokitansky kuster hauser syndrome utero - vaginal agenesis mllerian anomalies primary amenorrhea parole chiave risonanza magnetica ( rm ) mrkh , sindrome di mayer rokitansky kuster hauser agenesia utero - vaginale anomalie mlleriane amenorrea primaria introduction introduzione the mayer - rokitansky - kuster - hauser ( mrkh ) syndrome is a congenital mllerian anomaly characterised by inadequate development of the mllerian ducts , leading to combined uterovaginal aplasia . 
this syndrome is considered infrequent , but with an incidence of 1 : 4 , 000 female live births , it is a significant cause of mllerian anomalies , and the second most frequent cause of primary amenorrhea , second only to gonadal dysgenesis [ 1 ]  . 
mllerian buds may be observed , which represent more or less developed uterine horns , sometimes with functioning endometriuthe ovaries and fallopian tubes are usually present and normally formed [ 4 ]  . 
the syndrome is often associated with phenotypic alterations of the urinary and skeletal systems [ 5 ]  . the aim of our study was to evaluate the possible diagnostic role of magnetic resonance imaging ( mri ) as an alternative to laparoscopy in allowing adequate anatomical study of the patient before proceeding with surgical creation of a neovagina . la sindrome di mayer - rokitansky - kuster - hauser ( mrkh ) una anomalia congenita mlleriana caratterizzata da un insufficiente sviluppo dei dotti di mller , con conseguente aplasia utero - vaginale combinata . 
questa sindrome considerata una malattia rara , ma con unincidenza di 1 : 4000 nate vive , un ' importante causa di malformazioni mlleriane , e la seconda causa pi frequente di amenorrea primaria , seconda solo alle disgenesie gonadiche [ 1 ]  . la causa dellanomalia interviene durante lembriogenesi con arresto dello sviluppo dei dotti paramesonefrici a 7 settimane dalla fertilizzazione [ 2 ]  . 
la sindrome mkrh si caratterizza con normalit dei genitali esterni , assenza o ridotto sviluppo dei due terzi superiori della vagina e dellutero in luogo del quale possono essere riconoscibili i residui mlleriani rappresentativi di abbozzi uterini pi o meno sviluppati , talora con endometrio funzionale contestuale . 
la sindrome si associa frequentemente ad alterazioni fenotipiche dellapparato urinario e scheletrico [ 5 ]  . scopo del nostro lavoro di valutare il possibile ruolo diagnostico della risonanza magnetica come strumento diagnostico alternativo alla laparoscopia , per fornire un adeguato studio anatomico della paziente prima del trattamento chirurgico volto alla creazione di una neovagina . materials and methods study population materiali e metodi popolazione esaminata our study comprised 58 consecutive patients referred to our radiology department between november 2004 and february 2008 . 
patients were adolescents and young women , with age ranging from 14 to 30 years [ mean 20.9 ; lo studio ha preso in considerazione 58 pazienti consecutive presentatesi presso il nostro servizio di radiologia nel periodo compreso tra novembre 2004 e febbraio 2008 . 
the patients , selected by means of a series of investigations to identify possible mrkh syndrome , had undergone gynaecological examination and ultrasonography , which had raised a suspicion of uterine agenesis or hypoplasia associated with unassessable vagina . mri technique patients arrived at our department with a distended bladder and without specific intestinal preparation . 
the following images were acquired : axial and coronal t1 - weighted tr / te 470 / 15 ms , flip angle 90 , fov / rfov 350 / 80% , thickness / interval 4 / 0.6 mm , nsa 3 axial and coronal t2 - weighted turbo spin - echo ( tse ) tr / te 4 , 750 / 120 ms , flip angle 90 , fov / rfov 375 / 80% , thickness / interval 5 / 0.5 mm , nsa 6 sagittal t2 - weighted turbo spin - echo ( tse ) tr / te 6 , 686 / 100 ms , flip angle 90 , fov / rfov 375 / 80% , thickness / interval 4 / 1.0 mm , nsa 6 axial images were acquired from the vaginal canal up to the iliac crests . mr image analysis a diagnosis of mrkh syndrome was established on the basis of failure to visualise the uterus and absence of a normally developed vaginal canal . 
the canal is better appreciable on sagittal and axial t2 - weighted images where it appears as a lowsignal - intensity structure between the urethra and the bladder neck anteriorly and the rectum posteriorly . 
on t2 , it is possible to evaluate potential cavitation of the popolazione presa in esame rappresentata da adolescenti e giovani donne , di et compresa tra i 14 anni e i 30 anni ( media 20 , 9 ; deviazione standard 4 , 0 ) , con storia di amenorrea primaria . 
le pazienti , selezionate attraverso una serie di indagini volte a definire uneventuale diagnosi di sindrome mrkh , erano state sottoposte ad una visita ginecologica e ad un esame ecografico con responso di sospetta agenesia o ipoplasia uterina accompagnata al riscontro di una vagina insondabile . tecnica di studio rm le pazienti sono giunte allo studio senza specifica preparazione intestinale , a vescica repleta . 
tutti gli esami del nostro studio sono stati effettuati con un magnete 1 , 0 t ( nt intera , philips medical system , best , olanda ) utilizzando una bobina multicanale a 4 elementi . 
sono state acquisite immagini : t1 pesate assiali e coronali tr / te 470 / 15 ms , flip angle 90 , fov / rfov 350 / 80% , spessore / intervallo 4 / 0 , 6 mm , nsa 3 . t2 pesate assiali e coronali turbo spin - echo ( tse ) tr / te 4750 / 120 ms , flip angle 90 , fov / rfov 375 / 80% , spessore / intervallo 5 / 0 , 5 mm , nsa 6 . t2 pesate sagittali turbo spin - echo ( tse ) tr / te 6686 / 100 ms , flip angle 90 , fov / rfov 375 / 80% , spessore / intervallo 4 / 1 , 0 mm , nsa 6 . le immagini assiali sono state acquisite dal canale vaginale fino alle creste iliache . analisi immagini rm la diagnosi di mrkh stata posta in seguito alla mancata visualizzazione dellutero e allassenza di un canale vaginale normalmente sviluppato . due radiologi esperti hanno valutato in consenso , mediante risonanza magnetica : 1 . 
presenza o assenza o incompletezza del canale vaginale . il canale meglio apprezzabile nelle immagini pesate in t2 sul piano sagittale e assiale come struttura a basso segnale tra luretra e il collo vescicale anteriormente e il retto posteriormente . 
a t2 axial turbo spin echo ( tse ) ( tr 4 , 750 ms ; te 120 ms ; thickness 4 mm ) : hypointense structure between the urethra and rectum indicating vaginal bud ( arrow )  . 
a t2 assiale tse ( tr 4750 ms ; te 120 ms ; spessore 4 mm ) : struttura a segnale ipointenso tra uretra e retto , espressione di abbozzo vaginale ( freccia )  . 
presence , morphology and location of the ovaries . ovaries have reduced signal intensity on t1 and mixed signal intensity on t2 due to the marked hyperintensity of the follicular structures and to the low signal intensity of the fibromuscular component . 
 stata infine valutata la qualit delle indagini rm con rating 0 ( esame insufficiente ) , 1 ( sufficiente ) , 2 ( buono ) , 3 ( ottimo )  . radiol med ( 2009 ) 114 : 811826 fig . 
t2 axial turbo spin echo ( tse ) ( tr 4 , 750 ms ; te 120 ms ; thickness 4 mm ) : cavitated mllerian bud with a target appearance ( arrow )  . 
41 ( tabella 3 )  . t2 assiali tse ( tr 4750 ms ; te 120 ms ; spessore 4 mm ) : strutture in sede para - annessiale , a segnale ipointenso con area iperintensa centrale , rappresentative di residui mlleriani cavitati bilaterali ( frecce )  . two different types of intervention are possible , both performed with the laparoscopic technique : the vecchietti method and the davydov procedure . 
the former is based on the constant pressure exerted on the pseudohymenal membrane by a vaginal dilator connected via two perlon wires to a traction device on the pubis , with progressive upward stretching of the vestibular dome [ 14 , 15 ]  . 
the davydov technique , by contrast , uses peritoneum from the douglas pouch to create the vaginal dome , fornices and lining of the vaginal canal [ 1619 ]  . 
the time elapsed between mri and surgery was 1180 ( mean 90 , median 60 ) days . intervento chirurgico le pazienti dello studio sono state sottoposte ad un intervento chirurgico , mirato alla creazione di un canale vaginale con asse , lunghezza e capacit secretoria normali , in grado di garantire normali rapporti sessuali [ 13 ]  . 
il primo intervento si fonda sulla pressione continua che un tutore vaginale , collegato con due fili di perlon ad un apparecchio per trazione applicato sopra al pube , esercita sulla membrana pseudo - imenale , con progressivo stiramento verso lalto della cupola vestibolare [ 14 , 15 ]  . 
lintervento secondo davydov si basa invece sullimpiego del peritoneo per la creazione della cupola vaginale , i fornici ed il rivestimento del canale vaginale ottenuto attraverso la dissezione dello spazio rettovescicale [ 1619 ]  . 
il tempo intercorso tra lesame di risonanza magnetica e lintervento chirurgico stato di 1180 giorni ( media 90 giorni , mediana 60 giorni )  . analisi statistica lanalisi dei dati forniti dallindagine rm stata condotta al fine di determinare laccuratezza diagnostica della stessa nella valutazione della sindrome verificando quanto i giudizi formulati corrispondano effettivamente alla realt fornita dal metodo di riferimento ( gold standard ) , rappresentato , in questo studio , dalla laparoscopia . 
oltre alla determinazione dellaccuratezza diagnostica della rm , mediante lutilizzo di tabelle di contingenza di tipo 33 , abbiamo valutato laffidabilit dei nostri risultati calcolando il livello di concordanza cio la misura del grado di accordo tra le due indagini , al di l del grado di concordanza tra le metodiche che ci si aspetterebbe se le due indagini fossero indipendenti , fornita dalla k di cohen . 
il grado di accordo , e quindi il valore di k ottenuto dallo studio , stato considerato facendo riferimento alla scala di valutazione impiegata per valutare la concordanza di queste stesse tecniche nello studio di reinhold et al . 
a t2 coronal turbo spin echo ( tse ) ( tr 4 , 750 ms ; te 120 ms , thickness 4 mm ) : ovaries present bilaterally in extrapelvic location , situated laterally to the psoas muscle ( arrows )  . 
a t2 coronale tse ( tr 4750 ms ; te 120 ms , spessore 4 mm ) : ovaie in sede extrapelvica bilateralmente , situate lateralmente al muscolo psoas ( frecce )  . 
rene dislocato in sede pelvica , posteriormente e lateralmente alla vescica che risulta improntata sul profilo destro . table 1 rating scale for cohens k test ( from [ 20 ] ) tabella 1 scala di valutazione dei valori di k di cohen ( da [ 20 ] ) < 0 , 4 0 , 40 , 59 0 , 60 , 74 > 0 , 75 poor agreement fair agreement good agreement excellent agreement < 0 , 4 0 , 40 , 59 0 , 60 , 74 > 0 , 75 accordo basso accordo discreto accordo buono accordo eccellente statistical analysis risultati we determined the diagnostic accuracy of mri in the evaluation of mrkh syndrome by verifying the extent to which the mri findings reflected the real situation demonstrated by the reference method ( gold standard ) in this study , laparoscopy . 
in addition to measuring diagnostic accuracy , we used 33 contingency tables to evaluate the reliability of our results by calculating the level of concordance that is , the level of agreement between the two techniques beyond that expected by mere chance with cohens k test . 
the levels of agreement ( k values ) were based on the scale adopted for evaluating the concordance between these two techniques in a previous study on uterovaginal anomalies by reinhold et al . 
in addition , we carried out a descriptive analysis of the anatomical findings of mri for patients who underwent mri only . delle 58 pazienti che hanno eseguito lesame di risonanza magnetica , 56 hanno ricevuto conferma diagnostica di mrkh , con descrizione dei riscontri pelvici correlati . 
le restanti pazienti hanno rimandato la laparoscopia al momento in cui saranno pronte ad eseguire il successivo intervento chirurgico . in 18 pazienti lintervento stato eseguito secondo vecchietti e in 23 pazienti si effettuata invece una creazione di neovagina secondo davydov . 
in questo modo stata possibile la valutazione dellaccuratezza statistica radiol med ( 2009 ) 114 : 811826 dellindagine strumentale nella diagnosi della sindrome e nella valutazione anatomica del quadro associato . 
 la tabella 2 riporta i risultati ottenuti con la sola indagine rm in tutte le 56 pazienti affette da sindrome mkrh . in 2 pazienti lesame stato viziato da artefatti di movimento ( paziente 22 e 43 ) ed pertanto risultato di scarsa qualit tecnica ma sufficiente per porre diagnosi di sindrome mrkh ( rating 1 )  . 
 stata possibile una diagnosi di mrkh in tutti i casi di malattia , la rm ha quindi dimostrato una sensibilit diagnostica pari al 100% . in nessun caso , inoltre , stata posta diagnosi di mrkh in assenza di malattia ; in 2 casi sui 58 totali stata posta diagnosi differente e , trattandosi di veri negativi , la specificit diagnostica risultata essere a sua volta del 100% . in 34 pazienti ( 60 , 7% ) stata individuata la presenza bilaterale di rudimenti . 
in 10 pazienti ( 17 , 9% ) i residui sono risultati essere monolaterali , mentre in 12 pazienti ( 21 , 4% ) si riscontrata lassenza di abbozzi uterini ( tabella 4 )  . in 54 pazienti le ovaie sono state individuate bilateralmente mentre due pazienti hanno presentato un solo ovaio monolaterale . 
la localizzazione delle ovaie risultata normalmente pelvica in 48 pazienti ( 85 , 7% ) , mentre in 8 pazienti ( 14 , 3% ) si apprezzata la presenza di annessi in sede extrapelvica , bilaterale in 6 pazienti , monolaterale in 2 . 
in un caso stata individuata la presenza di una voluminosa cisti emorragica e in un altro di una cisti semplice di discrete dimensioni ( tabella 5 )  . il canale vaginale risultato essere completamente assente in 38 pazienti ( 67 , 8% )  . 
in 15 pazienti ( 26 , 8% ) stato possibile riconoscere il terzo inferiore del canale mentre in 2 casi la maggior estensione del canale ha suggerito la presenza dei due terzi inferiori . 
in 1 paziente , invece , il canale vaginale stato classificato come normoconformato seppur di dimensioni minime poich caratterizzato da uno sviluppo comunque presente ( tabella 6 )  . la presenza di versamento liquido in cavit pelvica stata segnalata in 33 pazienti ( 58 , 9% ) localizzato pi frequentemente ( 30 / 33 ) posteriormente alla vescica dove troviamo normalmente il cavo retto - uterino del douglas . con la rm stata valutata lassociazione della sindrome con le anomalie del sistema renale . 
grosso residuo mlleriano cavitato a sede retrovescicale ( 43 cm con cavit di 7 mm ) con aspetto a bersaglio : in questa paziente il successivo intervento chirurgico render possibile la creazione di un piccolo utero funzionale . results of the 58 patients studied by mri , 56 had diagnostic confirmation of mrkh , with demonstration of characteristic pelvic findings , whereas two patients received a different diagnosis ( one morris syndrome and one isolated vaginal atresia )  . 
this allowed us to determine the accuracy of mri in diagnosing the syndrome and in evaluating the associated anatomical findings . that obtained table 2 shows the results obtained with mri alone in all 56 patients affected by mrkh syndrome . 
in no case was a diagnosis of rokitansky syndrome established in the absence of disease ; in two out of 58 cases , a different diagnosis was established and , because the results were true negative , diagnostic specificity was also 100% . bilateral buds were present in 34 patients ( 60.7% ) and unilateral buds in ten ( 17.9% ) , whereas there was no evidence of uterine buds in 12 ( 21.4% ) ( table 4 )  . the ovaries were present bilaterally in 54 patients , whereas two patients had one unilateral ovary only . 
of the latter , one patient had previously undergone adnexectomy . location of the ovaries was pelvic in 48 patients ( 85.7% ) and extrapelvic in eight ( 14.3% ) and bilateral in six and unilateral in two . 
in one case , we detected a large haemorrhagic cyst , and in another case , a fairly large simple cyst ( table 5 )  . the vaginal canal was completely absent in 38 patients ptosi e ectopia renale . 
in 2 ( 3 , 6% ) pazienti , invece , si riscontrata una regolare posizione anatomica di un rene , associata ad una localizzazione pelvica del rene controlaterale . in 1 caso ( 1 , 8% ) si riscontrata una modesta ptosi renale monolaterale ( tabella 7 )  . delle 56 pazienti con mrkh che hanno eseguito lesame di risonanza magnetica , 41 hanno poi programmato lintervento e la laparoscopia preoperatoria , permettendo il confronto dei dati anatomici ottenuti con le due indagini ( tabella 3 )  . 
in 24 pazienti sia la rm che la laparoscopia hanno condotto allindividuazione di residui bilaterali , in 6 pazienti stata concordemente riscontrata la presenza di un unico residuo monolaterale ed in 2 pazienti i residui erano , invece , assenti . 
in 15 patients ( 26.8% ) , it was possible to recognise the lower third of the cavity , whereas in two cases , the greater length of the canal suggested the presence of the lower two thirds . 
in one patient , the vaginal canal was classified as having normal morphology but very small size ( table 6 )  . fluid collection within the pelvic cavity was seen in 33 patients ( 58.9% ) , most frequently located posterior to the bladder ( 30 / 33 ) , where the rectouterine douglas pouch is normally found . 
with regard to the evaluation of associated urinary anomalies , despite the many possible alterations , we concentrated on the main ones , namely , agenesis , ptosis and renal ectopia . 
in one case ( 1.8% ) , there was moderate unilateral renal ptosis ( table 7 )  . of the 56 patients with mrkh who underwent mri , 41 laparoscopy and underwent subsequent preoperative surgery , allowing comparison of the anatomical information obtained with the two techniques ( table 3 )  . 
the information concerning the presence or absence of buds was concordant in 32 / 41 patients ( 78% )  . both techniques demonstrated bilateral buds in 24 patients , a single unilateral bud in six and the absence of buds in two . individuazione bilaterale di residui alla laparoscopia , la rm stata in grado di documentare la presenza di un solo residuo in 2 pazienti mentre , nelle restanti cinque , non sono stati individuati entrambi . 
inoltre , in 1 paziente con riscontro di struttura rudimentale monolaterale alla laparoscopia , stata posta diagnosi di mancato riscontro alla rm . in una sola paziente , delle 8 con residuo monolaterale , la rm ha posto diagnosi di residuo bilaterale . 
la sensibilit diagnostica dellindagine rm nellindividuazione dei residui 33 / 39 , 85% ; con un intervallo di confidenza , per un livello di confidenza del 95% , compreso tra 70% e 93% ( 0 , 703 < p < 0 , 927 ; 82%11 , 5% )  . 
la specificit risulta invece essere del 100% ( 2 / 2 ) poich non sono mai stati individuati residui mlleriani dove questi non erano presenti , ma ragionando anche in questo caso per reperti , la specificit scende a 11 / 12 , 91% . 
in particolare si avuto un accordo sulla presenza e localizzazione delle gonadi con localizzazione table 4 identification of mllerian buds on magnetic resonance imaging radiol med ( 2009 ) 114 : 811826 bilateral 34 / 56 ( 60.7% ) bilateral 10 / 56 ( 17.9% ) bilateral 12 / 56 ( 21.4% ) rudimentary uterus no . 
of patients patients percentage table 5 identification of the ovaries on magnetic resonance imaging regular 46 / 56 ( 82.1% ) polycistic ovaries 10 / 56 ( 17.9% ) pelvic 48 / 56 ( 85.7% ) extrapelvic 8 / 56 ( 14.3% ) conformation localization no . 
of patients patients percentage radiol med ( 2009 ) 114 : 811826 table 6 identification of the vaginal canal on magnetic resonance imaging absent 38 / 56 ( 67.8% ) 1 / 3 lower 15 / 56 ( 26.8% ) 2 / 3 lower 2 / 56 ( 3.6% ) hypoplasia 1 / 56 ( 1.8% ) portion of the vagina no . 
of patients patients percentage identified at in seven patients with bilateral buds laparoscopy , mri was able to demonstrate the presence a solitary bud in two patients , whereas neither of the buds was identified in the other five . 
specificity was 100% ( 2 / 2 ) , as mllerian buds were never detected when they were not present ; however , based on the findings , specificity falls to 11 / 12 ( 91% )  . 
the level of concordance between the two techniques was k = 0.55. nine patients also underwent intraoperative ultrasonography , which allowed us to correlate the information concerning the possible cavitation of the buds ( table 8 )  . 
in particular , an agreement was reached concerning the presence and location of the ovaries , with bilateral pelvic location in 29 patients , bilateral extrapelvic in six , unilateral extrapelvic in one and solitary pelvic ovary in two . 
in two cases , there was disagreement regarding the location of the ovaries , whereas pelvica bilaterale in 29 pazienti , extrapelvica bilaterale in 6 , extrapelvica monolaterale in una , monovaio pelvico in 2 pazienti . 
in due casi si avuta discordanza riguardo alla sede degli annessi mentre in un terzo caso una gonade riconosciuta allesame rm non sono state poi visualizzate allesame laparoscopico . discussione nonostante la sindrome mrkh sia una condizione rara , frequenti cause di essa rappresenta una delle pi amenorrea primaria [ 11 ]  . 
la popolazione del nostro studio infatti rappresentata da giovani pazienti , valutate comunque in et post - pubere , con et compresa tra i 14 e i 30 anni , con una media di 20 , 9 anni . 
a queste indagini seguono esami strumentali rappresentati , in prima istanza , dallecografia . i risultati ecografici rischiano per di essere inconclusivi o incompleti , rendendo cos necessarie ulteriori indagini diagnostiche al fine di ottenere informazioni pi dettagliate e oggettive [ 8 , 9 ]  . 
of patients patients percentage in the third , case one ovary recognised at mri was not visualised by laparoscopy . discussion although mrkh syndrome is a rare condition , it represents the second more frequent causes of primary amenorrhoea [ 11 ]  . 
ultrasonography , in fact , does not always allow the recognition of mllerian buds and of ovaries with extrapelvic location , and this information is necessary for characterising the patients anatomical situation and defining the best surgical strategy [ 23 ]  . until a few years ago , detailed anatomical definition was provided by diagnostic laparoscopy , mri having only riconoscimento dei residui mlleriani e delle ovaie a localizzazione extrapelvica , dati invece necessari per inquadrare la situazione anatomica della paziente e definire la miglior soluzione chirurgica [ 23 ]  . fino a qualche anno fa la definizione dettagliata anatomica della sindrome veniva fornita in sede laparoscopica diagnostica mentre solo in tempi pi recenti che si resa disponibile una metodica alternativa non invasiva quale la rm . 
 [ 9 ] , al preventivo studio ecografico non erano state individuate strutture anatomiche poi correttamente descritte allindagine rm . lindagine ecografica , inoltre , in quanto operatoredipendente , conduce a risultati che possono risultare divergenti se eseguita pi di una volta , senza poter garantire loggettivit necessaria alla programmazione dellintervento chirurgico . 
lo studio rm in grado di valutare in modo accurato le anomalie utero - vaginali grazie alla possibilit di uno studio multiplanare , e grazie alladozione di sequenze diversamente pesate , volte a garantire la migliore visualizzazione delle diverse strutture indagate [ 2 , 5 ]  . nel nostro studio , al fine di fornire tutte le informazioni utili alla programmazione del successivo intervento , sono state indagate le strutture dello scavo pelvico , associate allo studio delle logge renali . 
nella nostra esperienza su 58 pazienti la rm si dimostrata metodica assai efficace nella radiol med ( 2009 ) 114 : 811826 table 8 evaluation of possible cavitation of mllerian buds : comparison between magnetic resonance imaging and laparoscopy buds cavitation ( n = 9 patients ) cavitated buds not cavitated buds absent buds recently become available as a noninvasive alternative tool . in a study by fedele et al . 
 furthermore , because ultrasonography is an operatordependent technique , it may provide conflicting results when performed several times , and it fails to guarantee the neutrality required for surgical planning . 
mri can accurately evaluate uterovaginal anomalies thanks to multiplanar imaging and the use of differently weighted sequences , allowing the best visualisation of all structures being examined [ 2 , 5 ]  . in our study , to obtain all the information required for surgical planning , we studied the structures of the pelvic pouch and renal compartment . 
in our experience on 58 patients , mri proved to be an effective technique in the diagnosis of mrkh syndrome , with 100% sensitivity ( 56 / 56 patients )  . 
furthermore , it enabled correct identification of the cause of primary amenorrhoea in the two remaining patients , with 100% specificity . the search for structures consistent with mllerian buds allowed their detection in 33 / 41 patients ( 80% )  . 
inoltre stato anche possibile identificare correttamente la causa di amenorrea primaria nelle due restanti pazienti con una specificit della nostra metodica del 100% . la ricerca di strutture compatibili con residui mlleriani ha condotto a una loro identificazione in 33 / 41 pazienti ( 80% )  . 
i dati forniti dalle due indagini hanno mostrato un grado di concordanza discreto dato da k = 0 , 55 . comunque importante considerare che in 2 pazienti in cui stato effettuato lesame rm , le immagini sono risultate compromesse da artefatti di movimento . 
se la valutazione si limita a considerare gli esami tecnicamente validi , il livello di accordo nella valutazione dei residui mlleriani risulta buono ( k = 0 , 62 )  . 
poich nella nostra esperienza gli artefatti da movimento erano perlopi determinati dalla impellenza minzionale della paziente potrebbe essere utile in futuro , per quanto possibile , controllare ecograficamente lo stato di distensione vescicale prima dellinizio dellindagine rm . da ritenersi che rm e laparoscopia forniscano risultati in sostanziale accordo tra di loro nella valutazione dei residui mlleriani , soprattutto per esami tecnicamente validi . uno degli aspetti clinici pi rilevanti nelle pazienti portatrici di sindrome mkrh costituito dalla comparsa in fase post pubere di dolori pelvici ciclici . 
lo studio della causa di tali sintomi negli anni ha portato a riconoscerne come causa principale laccumulo di materiale emorragico a livello degli abbozzi uterini dotati di endometrio funzionale [ 2 ]  . 
because the motion artefacts were chiefly caused by the patients urge to urinate , it may be useful to check the level of bladder distension by ultrasound before starting the mri study . 
mri and laparoscopy provide substantially concordant results in the evaluation of mllerian buds , above all in the case of technically adequate examinations . one of the most important clinical features of mrkh syndrome is the development of cyclic pelvic pain in the postpuberal period . 
the study of these symptoms over the years has shown that their main cause is accumulation of haemorrhagic material within uterine buds with a functioning endometrium [ 2 ]  . 
however , surgical evaluation of cavitation in these studies was only indirect and based on the size of the buds and was consequently far less reliable than evaluation with mri . 
in contrast , in our study , laparoscopic ultrasonography provided direct evaluation , indicating the effective capability of mri to provide precise information . to our knowledge , no other studies have compared the two techniques in the evaluation of functioning buds in these terms , so it is reasonable to state that mri is completely reliable in the preoperative evaluation of the presence of a functioning endometriuin our experience , laparoscopic ultrasonography has become unnecessary , and we have limited its use to a few selected cases of larger buds eligible for the potential creation of a small functioning uterus . in the evaluation of the ovaries , and in particular of their location and morphology , mri and laparoscopy produced identical results in all but three patients ( 38 / 41 , 93% ) ( table 3 )  . 
as a consequence , mri proved to be a reliable technique in this evaluation . tale reperto poteva essere solo sospettato clinicamente e accertato in fase laparoscopica con uno studio ecografico intraoperatorio o con una valutazione anatomo - patologica del residuo asportato . 
purtroppo un limite nella valutazione di questo aspetto , rappresentato dal piccolo numero di pazienti in cui stato possibile il confronto coi dati laparoscopici . lavori precedenti [ 20 , 23 ] , pur sempre limitati da un basso numero di pazienti , hanno indagato questaspetto concludendo per una migliore accuratezza dellindagine rm . 
in questi studi , tuttavia , la valutazione chirurgica della cavitazione era stata solo indiretta e basata sulla dimensione del residuo , risultando pertanto assai meno affidabile della valutazione rm . 
per quanto ci dato di conoscere non esistono altri lavori in letteratura che abbiano confrontato in questi termini le due indagini nella valutazione dei residui funzionali e possiamo pertanto affermare che la rm totalmente affidabile nella valutazione prechirurgica della presenza di endometrio funzionale . 
nella nostra esperienza ci ha via via reso superfluo il ricorso allecografia intralaparoscopica limitandone luso a casi mirati di residui dimensionalmente rilevanti eleggibili per la potenziale creazione di un piccolo utero funzionante . nella valutazione delle gonadi , e in particolare della loro localizzazione e morfologia , rm e laparoscopia hanno condotto a risultati concordi in tutte le pazienti con eccezione di tre casi ( 38 / 41 , 93% ) ( tabella 3 )  . 
anche per questa valutazione la rm risultata dunque metodica affidabile . dai nostri dati quindi emersa una significativa accuratezza dellindagine rm nello studio dellanatomia pelvica ed in particolare delle gonadi e dei residui mlleriani . 
si ottenuto , infatti , un discreto grado di concordanza nellindividuazione di residui ed un ottima valutazione della cavitazione degli abbozzi stessi . il livello di accuratezza raggiunto dalla rm permette , cos , di rimandare lesplorazione laparoscopica , esame invasivo e costoso , che necessita di anestesia e ospedalizzaradiol med ( 2009 ) 114 : 811826 our data indicate that mri has a significant level of diagnostic accuracy in the study of pelvic anatomy and in particular of the ovaries and mllerian buds . 
detection of buds showed a good level of concordance , and evaluation of possible cavitation was excellent . the level of accuracy achieved by mri allows patients to postpone laparoscopic exploration , an invasive and expensive procedure requiring anaesthesia and hospitalisation , to when they feel ready to face surgery [ 2 , 5 ]  . 
in particular , mri is able to depict the vaginal canal , even when budary , which in most cases corresponds to the lower third of the canal that is , to the portion of ectodermal origin that is not systematically affected by the mllerian anomaly owing to its different embryologic orig mri identification of a vaginal bud between the rectum and bladder is surgically useful , as it may be used to guide in the creation of a vaginal canal . the ability of mri to study associated urinary anomalies is important for preoperative evaluation . 
generally , in urinary anomalies , especially in the presence of a kidney in pelvic location or of a ptosic kidney , the vecchietti technique is preferred , as it is less invasive and minimises the risk of possible renal or ureteral injury . differentiating mrkh syndrome from other mllerian anomalies and more specifically from malformations of the distal genital tract is a necessity dictated not only by the different surgical strategies required by each anomaly but also by the different reproductive potential and psychological impact . in agreement with previous studies based on smaller patient samples , we believe that mri is an essential tool in the diagnosis and anatomical evaluation of mrkh syndrome , as it provides an in - depth study of the pelvis [ 20 , 23 ] and makes it possible to postpone the more invasive and expensive laparoscopic exploration until the time of surgery , when patients are anaesthetised and hospitalised . in our opinion , cooperation between the radiologist and the surgical team is fundamental for correct preoperative management of these young patients . 
identification of cavitated mllerian buds with endometrial tissue indicates the possibility of creating a functioning uterus or , alternatively , suggests their removal . zione , al momento in cui la paziente si sentir pronta ad affrontare lintervento [ 2 , 5 ]  . 
in particolare la rm in grado di rilevare la presenza di un canale vaginale , anche se ridotto a struttura rudimentale , corrispondente , nella maggior parte dei casi , al terzo inferiore del canale di derivazione ectodermica , che non risulta sistematicamente interessato dallanomalia mlleriana , data la diversa origine embriologica . 
lidentificazione alla rm di un abbozzo vaginale tra retto e vescica chirurgicamente utile perch pu essere utilizzato come guida alla creazione del tunnel vaginale . molto importante nella valutazione prechirurgica risulta la capacit della rm di indagare anche lassociazione della sindrome con anomalie dellapparato urinario . 
generalmente in caso di anomalie del sistema renale , ed in particolare in presenza di rene pelvico o comunque ptosico , infatti preferibile il ricorso ad unoperazione secondo vecchietti che , per la minor invasivit delloperazione , riduce il rischio di uneventuale lesione renale o ureterale . 
tale necessit dovuta , non solo al diverso trattamento chirurgico che spetta a ciascuna anomalia , ma anche al diverso potenziale riproduttivo e conseguente impatto psicologico delle differenti forme di presentazione . in accordo con altri studi precedenti [ 20 , 23 ] , basati su un numero inferiore di pazienti , riteniamo che la rm sia strumento diagnostico essenziale nella diagnosi e nella valutazione anatomica della sindrome mrkh fornendo uno studio dettagliato della pelvi della paziente . 
hasbargen1 1department of obstetrics and gynecology , 2department of radiology , ludwig - maximilians - university munich , campus grosshadern , marchioninistrasse 15 , 80337 munich , germany correspondence to : m . 
on biplanar topograms , multiplanar reconstructions of 1 - mm slices , volume - rendered images of the same data and volumerendered images based on 5 - mm - thick images . interobserver agreement and variability were determined by bland - altman analysis . 
with a correlation coefficient of 0.98 , interobserver agreement was best for assessing 3d volumerendered images reconstructed from 1 - mm - thick slices . interobserver variability was very good for sagittal outlet and midpelvic diameter , transverse inlet diameter and obstetric conjugate ( correlation coefficients 0.960.99 ) but limited for intertuberous and interspinous distance . 
sono state ottenute 6 misurazioni pelvimetriche da due osservatori indipendenti in quattro data sets per ogni paziente , cio topogrammi in due proiezioni , ricostruzioni multiplanari con scansioni dello spessore di 1 mm , immagini volumetriche degli stessi dati ed immagini volumetriche basate su scansioni dello spessore di 5 mla variabilit e la concordanza interosservatore sono state determinate secondo lanalisi bland - altman . 
con un coefficiente di correlazione di 0 , 98 , la concordanza tra gli osservatori stata migliore nella valutazione delle immagini volumetriche tridimensionali ricostruite da scansioni dello spessore di 1 mla variabilit interosservatore stata molto buona per il diametro sagittale esterno e per il diametro intermedio della pelvi , per il diametro dellinserzione trasversa e per la coniugata ostetrica ( coefficiente di correlazione 0 , 960 , 99 ) , ma limitata per la distanza tra le tuberosit e tra le spine ischiatiche . 
pertanto , la pelvimetria - tc 828 radiol med ( 2009 ) 114 : 827834 keywords ct - pelvimetry cephalopelvic disproportion dystocia interobserver variability adatta ad acquisire lesatta conoscenza dellanatomia pelvica per identificare i parametri rilevanti per distocia negli studi retrospettivi . parole chiave pelvimetria - tc sproporzione cefalopelvica distocia variabilit interosservatore introduction about two thirds of all caesarean sections are performed due to dystocia or are indirectly related to cephalopelvic disproportion because they are scheduled for elective caesarean after cephalopelvic disproportion at first delivery [ 1 ]  . 
cephalopelvic disproportion should be diagnosed when there is an adequately dilated cervix and sufficient contractions of the uterus but the fetal head does not descend into the birth canal [ 2 ]  . 
the need for a reliable method to detect women at risk for dystocia has been recognised since the eighteenth century , and various approaches to pelvimetry have been used to identify small pelvis as indication for caesarean section . 
conventional x - ray and ct pelvimetry have been largely abandoned since mri pelvimetry became available , as exposure to ionising radiation , especially of the foetus , can be avoided [ 310 ]  . 
the results should be useful to identify the postprocessing method with the best reproducibility and to estimate the required radiation exposure for low - dose exams . the study can also indicate necessary slice thickness for pelvimetry on previously existing ct scans , either to perform measurements for an individual patient or to retrospectively evaluate pelvimetric measurements of large patient groups for study purposes . 
 materials and methods available ct data ct pelvimetry was performed in 25 female patients based on ct data that had been acquired in routine clinical care . the retrospective evaluation is warranted by the universitys ethics committee guidelines and adhered to the world medical association declaration of helsinki . 
ct data sets of 15 consecutive women referred for abdominal ct postpartum in 2007 had been obtained on 64 - slice ct scanners ( somatom sensation 64 or somatom definition , siemens , forchheim , germany ) with 0.6 - mm collimation at 120 kvp tube potential and 250 mas reference tube current time product with dose modulation . 
 additionally , pelvimetric measurements were acquired in ct data sets of ten women with known multiple myeloma who had undergone low - dose ct to screen for osteolysis and additionally had had a normal routine abdominal ct scan for other reasons within the last 2 years . 
the routine scans had been obtained with the routine parameters given above , whereas the low - dose scans had been acquired with a reduced tube current of 83 reference mas . 
a human cadaver skeleton was also scanned with the mentioned normal and low - dose protocols to validate ct - pelvimetric measurements , with manual measurements by ruler as external reference . 
radiation dose was calculated for each exam based on the ct dose index ( ctdi ) and the scan length , which are represented in radiol med ( 2009 ) 114 : 827834 fig . 
the equivalent dose can be calculated from the dlp with a conversion factor of 0.017 msv / mgy * cm for the pelvis [ 11 ]  . pelvimetry based on these images , pelvimetry was performed retrospectively by two independent blinded radiologists on a 3d workstation ( siemens multi - modality workplace , siemens , forchheim , germany ) using topograms , multiplanar reconstructions and volume - rendered images . 
these included the obstetric conjugate as the shortest distance between promontory and symphysis , the sagittal outlet as the distance between the inferior inner aspect of the symphysis and the distal end of the sacrum , and the midpelvic sagittal diameter from the 830 radiol med ( 2009 ) 114 : 827834 fig . 
c ricostruzione para - assiale che mostra le spine ischiatiche , la regione caudale della sinfisi e il sacro cos da poter misurare la distanza tra le spine ed il diametro intermedio della pelvi . 
as a fourth method , the same reconstructions were done based on 5 - mm - thick slices , and all measurements were obtained equally on 3d volume - rendered images . to assess clinical usability in daily routine , we clocked the times needed to measure all six pelvimetric numbers needed for pelvimetry by the different methods . 
le linee indicano la coniugata ostetrica , il diametro intermedio della pelvi e quello sagittale esterno . statistical analysis results all continuous variables are displayed as mean and standard deviation ( sd )  . 
 ex vivo ct pelvimetry agreed well with manual measurements , with a maximal deviation of 2 mm for the intertuberous distance and errors of 01 mm for the other pelvimetric distances , indicating that there is virtually no relevant systematic error . 
 regarding assessment of the different pelvimetric distances with the different methods in detail , sds of interobserver variability were generally lower for cross - sectional and 3d approaches compared with the topogram - based measurements ( table 2 )  . 
 also , variability was lower for obstetric conjugate ( m ) , transverse inlet ( c ) , sagittal midpelvic ( q ) and sagittal outlet ( s ) than for interspinal ( h ) and intertuberous ( i ) distance . regarding the different pelvimetric distances in summary , interobserver variability of 2d and 3d measurements was very low , with an sd < 2% for m , c , q and s distances , whereas variability was higher for h and i ( table 3 )  . 
 ct dose index ranged from 11 to 15 mgy at standard tube voltage of 120 kvp and a reference tube current time product of 220 mas ( ref ) with automatic exposure control , resulting in tube current values of 142180 mas . 
the impression was that a further reduction of tube current would be possible if the assessment of pelvic dimensions is the only purpose of the exa regarding reading time for measuring the various pelviradiol med ( 2009 ) 114 : 827834 metric dimensions , there were significant differences between the different postprocessing approaches . 
the topogram - based approach was performed fastest , with an average reading time of 12030 s , whereas the 3d methods required 18624 and 18015 s for 1 - mm and 5 - mm data sets , respectively . 
in comparison with the interobserver variability reported for standard mri pelvimetry in literature [ 13 ] , ct offers an at least comparable accuracy . our results indicate that a very easy , fast and accurate determination of pelvimetric dimensions can be achieved with 3d volume - rendered reconstructions , which therefore can be regarded as the method of choice . 
although the best accuracy is achieved with this approach , measurements on volume - rendered images derived from 5 - mm - thick slices achieve a comparable agreement as 2d cross - sectional reconstructions from 1 - mm data sets . 
with a standard deviation of 2% corresponding to 23 mm for most pelvimetric distances , the accuracy of these 2d and 3d measurements seems acceptable , whereas the sd of interobserver variability for the topogram - based assessment with about 5% sd may be clinically relevant . 
the round shape of the ischiadic tuber and the continuous transition between the spinous process and the ligaments inserting there with variable density and calcification can be assumed to represent the reasons for this difference [ 14 ]  . 
still , taking into account the availability of mri as an alternative method without ionising radiation , the indication for ct pelvimetry is very limited , especially in pregnant women [ 15 ]  . 
regarding the fact that dystocia can be life threatening for mother and foetus , ct may still represent an adequate diagnostic tool in critical situations if mri is not readily available or is contraindicated for other reasons , or in nonpregnant women with a history of dystocia . 
also , the results should apply similarly to mri data sets acquired with 3d pulse sequences ( e.g. vibe ) , which would release dependence on a precise primary data acquisition . 
low - dose protocols do not significantly affect accuracy and can contribute to significant dose savings , although radiation exposure may restrict the prospective application of ct pelvimetry in general . 
mazzucato piccin nuova libraria , padova , eds . isbn 978 - 88 - 299 - 1980 - 2 published online : 17 july 2009 springer - verlag 2009 the book anatomia radiologica : tecniche e metodologie in radiodiagnostica ( radiological anatomy : techniques and modalities in diagnostic imaging ) by fernando mazzucato has now reached its third edition . 
it is a pleasure to recall that many radiologists and radiographers have used and studied this textbook and that many of the teaching faculty in the postgraduate schools of radiology and undergraduate courses for radiology and radiotherapy technicians recommend it to their students . the book has always enjoyed considerable success , as testified by the numerous reprints , and its popularity is justified by its clear ability to meet the real needs of radiologists . 
the third volume is in fact entirely devoted to computed tomography ( ct ) , magnetic resonance imaging ( mri ) and positron emission tomography ( pet ) - ct . 
the approach and layout of prior editions have been maintained , with numerous images , drawings and diagrams , many of which are in colour . the three volumes offer complete coverage of technical , methodological and anatomical aspects at the level of all body organs and systems . 
in the first volume , considerable space is given to physics and technique , equipment , analogue and digital radiographic images , as well as to radiology information systems ( ris ) and picture il volume anatomia radiologica tecniche e metodologie in radiodiagnostica di fernando mazzucato giunto alla sua terza edizione . 
fa piacere sottolineare che su questo libro hanno studiato e si sono formati molti radiologi e tecnici radiologi , e molti di coloro che ricoprono incarichi di responsabilit nelle scuole di specializzazione di radiologia e nei corsi di laurea per tecnici di radiologia , per immagini e radioterapia consigliano questo libro ai propri studenti . il libro ha sempre riscosso grande successo , come testimoniato dalle numerose ristampe , perch evidentemente orientato verso le reali necessit del radiologo . 
infatti , il terzo volume interamente dedicato alla tomografia computerizzata ( tc ) , alla risonanza magnetica ( rm ) , alla tomografia ad emissione di positroni ( pet )  . inoltre , ledizione attuale comprende una nuova parte dedicata alla radiologia interventistica , a testimonianza del ruolo fondamentale di questa disciplina per il radiologo . lopera si avvale della ormai consolidata impostazione caratterizzata da una ricca iconografia , numerosi disegni e schemi didattici , molti dei quali a colori . i tre volumi presentano con grande completezza gli aspetti tecnici , metodologici e anatomici a livello di tutti gli organi e apparati . 
nel primo volume trovano ampio spazio la parte di fisica e tecnica , le apparecchiature , limmagine 836 radiol med ( 2009 ) 114 : 835836 archiving and communications systems ( pacs )  . 
 the second volume comprises most of the chapters dealing with the various organs and systems and in particular the digestive system , the liver , the biliary system , the spleen , the pancreas , the urinary system and retroperitoneum , the male and female reproductive systems , the breast and the nervous systethe volume ends with three chapters devoted to sonography in internal medicine and obstetrics and gynaecology and to doppler sonography . the third volume is the most extensive , as it deals mainly with heavy equipment , with ample space given to ct , mri and pet - ct . 
the final section is devoted to diagnostic and especially interventional angiography , with chapters also covering extravascular interventional radiology . although the book was written in collaboration with other well - known authors , it is nice to note that fernando mazzucatos work of coordinator clearly transpires through all of the chapters , such that it is easy to predict that this new edition will enjoy a success equal to that achieved by the earlier editions . radiografica analogica e digitale ; vengono inoltre presi in esame i sistemi informativi in radiologia ( ris ) e i sistemi per larchiviazione e la comunicazione delle immagini ( pacs )  . 
nel primo volume trovano ampia trattazione due capitoli fondamentali dedicati allo scheletro e articolazioni e allapparato cardiorespiratorio , con i quali deve iniziare la formazione dello specialista radiologo e del tecnico di radiologia . 
 il secondo volume contiene la maggior parte dei capitoli dedicati ai vari organi e apparati , e precisamente allapparato digerente , al fegato , alle vie biliari , alla milza , al pancreas , allapparato urinario e al retroperitoneo , allapparato genitale maschile e femminile , alla mammella e infine al sistema nervoso . 
il volume termina con tre capitoli dedicati allecografia internistica , ostetrico - ginecologica e al doppler . il terzo volume molto corposo in quanto dedicato principalmente alle macchine pesanti e pertanto trovano ampio spazio la tc , la rm e la pet . 
during a 13 - month period , 55 consecutive patients under evaluation for aortic ( 40 / 55 ) or mitral valve ( 15 / 55 ) disease before potential valve replacement underwent ctca using a 64 - detector - row scanner within 2 months of cca for comparative purposes . 
the diagnostic accuracy of 64 - row ctca for ruling out the presence of significant coronary stenoses in patients undergoing valve surgery is excellent and allows ctca to be used as a gatekeeper for invasive cca in these patients . 
mdct is a necessary preoperative examination that provides useful information for identifying potential operative complications of surgical procedures . keywords multidetector - row computed tomography conventional coronary angiography coronary artery disease valvular heart disease cardiac surgery riassunto obiettivo . 
in un periodo di 13 mesi , mediante tc a 64 detettori stata eseguita ac - tcms in 55 pazienti consecutivi affetti da patologia valvolare aortica ( 40 / 55 ) o mitralica ( 15 / 55 ) seguita da acc in un periodo minore di 2 mesi . 
laccuratezza diagnostica della ac - tcms 64 detettori per escludere la presenza di stenosi coronariche significative nei pazienti candidati allintervento valvolare eccellente , consente di utilizzarla come esame di prima istanza e di riservare la acc a pazienti selezionati . 
mdct un esame pre - operatorio che fornisce informazioni utili per identificare potenziali complicanze delle procedure chirurgiche . parole chiave tomografia computerizzato multistrato angiografia coronarica convenzionale malattia aterosclerotica coronarica malattia valvolare cardiaca chirurgia cardiaca radiol med ( 2009 ) 114 : 728742 introduction introduzione stenosis of the calcified aorta is the most common valvular heart disease in elderly patients , with a prevalence of 2%7% in the population > 65 years of age [ 1 ] and is associated with increased mortality [ 2 ]  . 
bicuspid aortic valve with fusion of the right coronary cusp and the noncoronary cusp is a common anomaly affecting 1%2% of the population and is the second most common cause of valvular disease requiring surgery [ 3 ]  . 
the surgical approach , in fact , can vary significantly according to whether the valve is bicuspid or tricuspid [ 4 ]  . valvular calcifications should be seen as a manifestation of multidistrict atherosclerotic disease , whether or not they cause valvular stenosis [ 5 ]  . 
in patients with concomitant valvular and coronary artery disease , the combined procedure of valve replacement and coronary artery bypass grafting ( cabg ) reduces perioperative and postoperative mortality and morbidity with respect to valve replacement surgery alone [ 6 ]  . 
recent guidelines recommend conventional coronary angiography ( cca ) before valvular surgery in men > 35 years of age , in premenopausal women with significant vascular risk factors and in postmenopausal women [ 7 ]  . 
as cca is a costly and invasive procedure with a mortality rate of 0.15% and morbidity rate of 1.5% [ 8 ] , an alternative , less invasive and less expensive procedure is desirable . 
thanks to its high spatial and temporal resolution , multidetectorrow computed tomography ( mdct ) with cardiac gating is able to visualise the coronary artery lumen and walls and enables accurate identification of the atherosclerotic plaque and quantification of induced stenosis [ 9 ]  . 
with multiplanar and 3d postprocessing of the data sets acquired with cardiac - gated mdct , evaluation can be made of the number of leaflets , presence of annular and valvular calcifications and valvular kinetics [ 10 ]  . 
in addition , the use of dedicated software makes possible the evaluation of ventricular function parameters , which is particularly useful in the clinical characterisation of patients referred for heart valve surgery . the aims of our study were therefore to evaluate the utility of mdct in the preoperative assessment of patients with aortic or mitral valve disease and to determine whether ct coronary angiography ( ctca ) can be used as a valid alternative to invasive cca in patients referred for heart valve surgery , so that the latter technique may be reserved for patients with significant cad . la stenosi aortica calcifica la pi comune patologia valvolare cardiaca nei pazienti anziani , con una prevalenza del 2%7% nella popolazione maggiore di 65 anni [ 1 ] ed associata ad aumentato rischio di mortalit [ 2 ]  . 
la valvola aortica di tipo bicuspide con fusione della cuspide coronarica destra e della cuspide non coronarica unanomalia comune con incidenza pari all1%2% della popolazione ed la seconda causa pi frequente di patologia valvolare che richiede intervento chirurgico [ 3 ]  . 
in fase preoperatoria , la valutazione della morfologia valvolare , il diametro dellanulus e la presenza di calcificazioni dellanulus e della valvola utile per pianificare lapproccio chirurgico . la strategia chirurgica cambia significativamente se la valvola bicuspide o tricuspide [ 4 ]  . 
nei pazienti in cui concomita malattia valvolare e coronarica , lintervento chirurgico combinato di sostituzione valvolare e bypass coronarico in unico tempo riduce la mortalit e morbilit perioperatoria e postoperatoria rispetto allesecuzione della sola sostituzione valvolare [ 6 ]  . 
le recenti linee guida raccomandano di eseguire coronarografia convenzionale ( acc ) in ogni paziente candidato allintervento valvolare se di et maggiore di 35 anni per gli uomini e nelle donne in fase post - menopausale o premenopausale se concomitano significativi fattori di rischio vascolare [ 7 ]  . 
dato che la acc una procedura invasiva che comporta un tasso di mortalit pari allo 0 , 15% e morbilit del 1 , 5% ed una metodica costosa [ 8 ] , auspicabile unindagine alternativa meno invasiva e meno costosa . 
la tc multistrato con sincronizzazione ecg essendo dotata di elevata risoluzione spaziale e temporale permette la visualizzazione del lume e della parete coronarica , inoltre consente laccurata identificazione delle placche ateromasiche e la quantificazione del grado di stenosi indotto [ 9 ]  . 
elaborando con tecnica multiplanare e 3d i dataset acquisiti con tc multidetettore con sincronizzazione ecg possibile valutare anche il numero dei lembi valvolari , lo spessore dei lembi , la presenza di calcificazioni della valvola e dellanulus e la cinetica valvolare [ 10 ]  . 
 pertanto il nostro studio ha lobiettivo di valutare lutilit della tc multistrato in fase preoperatoria nei 730 materials and methods patient population between january 2006 and january 2008 , we used ctca to examine 84 patients referred for aortic or mitral valve replacement surgery who were without contraindications to the use of nonionic iodinated contrast mediuno patients were excluded on the basis of heart rate , body mass index ( bmi ) or the presence of arrhythmias . 
the remaining 55 patients ( 29 men and 26 women , mean age 738 years ) , who underwent cca within 2 months of ctca , made up our study population . our institutional ethics committee approved the study protocol , and all patients provided informed consent . patient preparation all patients ( 35 / 55 , 64% ) with a heart rate > 65 beats per minute ( bpm ) , a left ventricular ejection fraction > 40% in the absence of arterial hypotension , asthma and obstructive respiratory disease received a 5 - mg intravenous dose of beta blockers ( propranolol , inderal )  . 
patients affected by bronchial asthma ( 4 / 55 , 7% ) with heart rate > 65 bpm received a 5 - mg intravenous dose of calcium - channel blocker ( verapamil , isoptin )  . 
in addition to the beta blockers and calcium - channel blockers , some patients ( 6 / 55 , 11% ) without contraindications received ten drops sublingually of benzodiazepine ( bromazepam , lexotan )  . 
in all patients , a preliminary unenhanced scan was performed to quantify the presence of calcium in the coronary arteries , the valves and the aorta . the parameters used for the scan , image reconstruction and data set creation are summarised in tables 13 . 
intendiamo valutare anche se la coronarografia mediante tomografia computerizzata ( ac - tcms ) pu essere una valida alternativa alla coronografia invasiva nei pazienti candidati alla sostituzione valvolare cardiaca in modo tale da riservare questultima indagine solo ai pazienti con malattia coronarica significativa . materiali e metodi popolazione esaminata da gennaio 2006 a gennaio 2008 abbiamo esaminato mediante ac - tcms 84 pazienti candidati allintervento di sostituzione valvolare aortica o mitralica , senza controindicazioni alluso del mezzo di contrasto iodato non ionico ( mdc )  . 
per il nostro studio , da questo gruppo di 84 pazienti abbiamo escluso un totale di 29 pazienti : 20 di questi perch non hanno eseguito successivamente lacc e 9 perch hanno eseguito lacc con un intervallo di tempo maggiore di 2 mesi dalla tc . 
i restanti 55 pazienti ( 29 maschi , 26 femmine ; et media 738 anni ) costituenti la nostra popolazione di studio hanno eseguito acc entro 2 mesi dalla ac - tcms . 
 il comitato etico della nostra istituzione ha approvato il protocollo di studio e tutti i pazienti hanno fornito il consenso informato . preparazione dei pazienti a tutti i pazienti ( 35 / 55 , 64% ) con frequenza maggiore di 65 battiti per minuto ( bpm ) , frazione di eiezione del ventricolo sinistro > 40% in assenza di ipotensione arteriosa , asma e malattia respiratoria ostruttiva , stata somministrata per via endovenosa una fiala di beta - bloccante da 5 mg ( propanololo , inderal )  . 
ai pazienti affetti da asma bronchiale ( 4 / 55 , 7% ) con frequenza maggiore a 65 bpm stato somministrato per via endovenosa ca - antagonista da 5 mg ( verapamil cloridrato , isoptin )  . 
oltre al beta - bloccante o ca - antagonista , in alcuni pazienti ( 6 / 55 , 11% ) privi di controindicazione ( ipersensibilit alle benzodiazepine , al principio attivo o ad uno qualsisi degli eccipienti ) , sono state somministrate 10 gocce per via sublinguale di benzodiazepina ( bromazepam , lexotan )  . 
in nessun caso sono stati somministrati nitroderivati . esame tc parametri di acquisizione tutti gli esami sono stati eseguiti mediante uno scanner a radiol med ( 2009 ) 114 : 728742 table 1 computed tomography coronary angiogram ( ctca ) scan protocol no . 
di strati spessore del detettore tempo rotazione pitch gantry volt ampere scansione senza mdc scansione con mdc 0 , 5 mm 0 , 5 mm 0 , 25 ms 0 , 25 ms variabile con i bpm variabile con i bpm 120 kv 120 kv 200 ma 500 ma table 2 image reconstruction protocol effective slice thickness reconstruction increment field of view convolution kernel unenhanced scan contrast - enhanced scan 3 mm 0.5 mm 3 mm 0.3 mm 270320 270320 calcium score coronary fc05 tabella 2 parametri di ricostruzione delle immagini spessore strato effettivo incremento di ricostruzione scansione senza mdc scansione con mdc 3 mm 0 , 5 mm 3 mm 0 , 3 mm campo di vista 270320 270320 filtro di convoluzione calcium score coronarie fc05 table 3 dataset reconstruction parameters technique using r - r interval percentage technique using absolute prospective delay technique using absolute reverse delay toshiba best phase technique ecg editing ecg , electrocardiograph tabella 3 parametri di ricostruzione dei dataset tecnica della percentuale dell ' intervallo r - r tecnica del ritardo prospettivo assoluto tecnica del ritardo assoluto inverso tecnica " best phase " toshiba ecg editing ecg , elettrocardiogramma parameters 70%75% 175 , 225 , 275 , 325 ms ( - ) 275 , ( - ) 300 , ( - ) 350 , ( - ) 400 ms automatic valori di ricostruzione 70%75% 175 , 225 , 275 , 325 ms ( - ) 275 , ( - ) 300 , ( - ) 350 , ( - ) 400 ms automatica total 100% ( 55 / 55 ) 100% ( 55 / 55 ) 100% ( 55 / 55 ) 27% ( 15 / 55 ) 38% ( 21 / 55 ) n . 
the angiographic scan was performed in 1114 s , corresponding to the length of a single breath hold . image analysis image analysis was done at a vitrea 2.0 workstation ( vital image , minnesota , mn , usa ) with axial , multiplanar ( mpr ) , curved planar ( cpr ) , 3d , maximum intensity projection ( mip ) and volume - rendered ( vr ) reconstructions . 
quantification of the aortic calcium burden by assigning a 5 - point score , corresponding to absence of aortic calcium ( 0 ) , mild ( 1 ) , moderate ( 2 ) , moderate to severe ( 3 ) and severe ( 4 ) , and location of the plaques with reference to the valvular plane 2 . 
il tempo totale medio di scansione stato di 16 secondi circa . protocollo di iniezione sono stati somministrati 90110 ml di mdc ( iomeron 400 , bracco , milano , italia ) alla velocit di 45 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocanula da 1820 gauge precedentemente posizionata in una vena ante cubitale , seguiti da soluzione salina ( nacl 40 ml a 45 ml / s )  . 
analysis of coronary stenosis using a 17 - segment modified american heart association ( aha ) classification . each segment was classified as normal , with stenosis < 50% or with stenosis 50% . 
the segments distal to a chronic occlusion were excluded due to insufficient filling of contrast medium from collateral branches . coronary angiography examination all ccas were done within 360 days after ctca with a phillips integrix 3000 or ge innova 3100 . 
each segment was classified as normal , with stenosis < 50% or with stenosis 50% . stenoses were evaluated in two orthogonal views and classified as significant if mean luminal reduction exceeded 50% . in addition , measurements of aortic pressure , left ventricular pressure and transvalvular gradient were made for each examination , as well as an evaluation of valvular lanalisi delle immagini stata condotta mediante workstation vitrea 2.0 ( vital image , minnesota , usa ) con ricostruzioni assiali , multiplanari ( mpr ) , piani curvi ( cpr ) , 3d , massima intensit di proiezione ( mip ) , e volume rendering ( vr )  . 
i segmenti distali a unocclusione cronica sono stati esclusi per linsufficente riempimento di mdc determinato dai rami collaterali . radiol med ( 2009 ) 114 : 728742 regurgitation ( expressed with a score from 0 to 4 ) and of the number of valve cusps and their motility . 
lastly , aortography was performed in each patient . esame coronarografico statistical analysis the diagnostic accuracy of ctca was evaluated by comparing the findings with the reference standard cca and evaluating sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) and the relative 95% confidence intervals ( cis )  . 
we also calculated the positive likelihood ratio [ sensitivity / ( 1 - specificity ) ] and negative likelihood ratio [ ( 1 - sensitivity ) / specificity ]  . 
we performed a subanalysis that compared patients with aortic disease ( group a ) and patients with mitral valve disease ( group b ) and a subanalysis comparing patients with and without angina pectoris ( ap )  . results demographic characteristics of the patient population are summarised in table 4 . 
a large proportion of patients showed aortic stenosis ( 21 / 55 , 38% ) , no patient had isolated mitral stenosis and 14 patients ( 14 / 55 , 25% ) had mitral stenosis with regurgitation . 
patients with elevated heart rate were not excluded , nor were patients with arrhythmias at the time of the examination , and no selection was made on the basis of bmi . 
two examinations ( 2 / 55 , 3% ) , in patients with severe aortic stenosis , were marred by severe motion artefacts precluding ctca evaluation of the coronary arteries , so they were excluded from the analysis . 
in one patient affected by aortic stenosis and aneurysm of the ascending aorta ( 77 cm ) , the operator performing the cca failed to cannulate the ostium of the dominant left coronary artery despite numerous attempts , so on this vessel , ctca replaced cca as the reference technique . patient - based analysis ctca showed absence of significant disease in 31 patients . three cases were incorrectly evaluated as positive , thus producing a specificity of 91% . 
the operator correctly identified all 19 patients with at least one significant stenosis , tutte le acc sono state eseguite dopo ac - tcms , in un range di tempo compreso tra 3 e 60 giorni dallesecuzione della ac - tcms , con philips integrix 3000 o ge innova 3100 . 
un cardiologo con esperienza pluriennale angiografica , senza conoscere il risultato della ac - tcms , ha analizzato tutti i segmenti coronarici utilizzando la classificazione a 17 segmenti modificato dellamerican heart association ( aha )  . 
 inoltre per ogni esame stata misurata la pressione aortica , pressione ventricolare sinistra , gradiente transvalvolare , valutazione del rigurgito valvolare ( espresso con punteggio da 0 a 4 ) , valutazione del numero delle cuspidi valvolari e la loro motilit . 
infine stata eseguita laortografia in ogni paziente . analisi statistica laccuratezza diagnostica della ac - tcms stata valutata confrontando i risultati con la acc che rappresenta lo standard di riferimento e valutando la sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) con il relativo intervallo di confidenza al 95% . 
abbiamo eseguito una subanalisi selezionando i pazienti con patologia aortica ( gruppo a ) comparandola con patologia valvolare mitralica ( gruppo b ) e una subanalisi differenziando pazienti con e senza angina pectoris ( ap )  . risultati le caratteristiche demografiche della popolazione sono riportate in tabella 4 . 
la maggioranza dei pazienti esaminati presentava stenosi aortica ( 21 / 55 , 38% ) , nessun paziente presentava stenosi mitralica isolata e 14 pazienti ( 14 / 55 , 25% ) presentavano steno - insufficienza mitralica . non sono stati esclusi i pazienti che presentavano elevata frequenza cardiaca , n aritmie al momento dellesame , n sulla base del bmi . 
di questi 734 radiol med ( 2009 ) 114 : 728742 table 4 patient demographics tabella 4 caratteristiche della popolazione aortic stenosis , aortic regurgitation , aortic stenosis with regurgitation other valve disease male symptom angina pectoris no angina pectoris previous myocardial infarction risk factors hypertension high cholesterol level diabetes mellitus smoking family history of cad obesity ( bmi 30 kg / m2 ) coronary calcium score agatston cs volumetric cs valvular calcium score volumetric cs aortic calcium type of cardiac surgery aortic valve stenosis ( group 1 ) aortic valve regurgitation ( group 2 ) aortic valve stenosis with regurgitation ( group 3 ) mitral valve stenosis ( group 4 ) mitral valve regurgitation ( group 5 ) mitral valve stenosis with regurgitation ( group 6 ) cad absent cad not significant one vessel disease multivessel disease nyha class class i class ii class iii 749 ( 8943 ) 749 ( 8943 ) 7410 ( 4988 ) 29 ( 29 / 55 , 53% ) 16 39 25 23 11 2 , 434 0.98 21 ( 21 / 55 , 38% ) 9 ( 9 / 55 , 16% ) 10 ( 10 / 55 , 18% ) 14 ( 14 / 55 , 25% ) 1 ( 1 / 55 , 2% ) 38% ( 20 / 53 ) 26% ( 14 / 53 ) 9% ( 5 / 53 ) 26% ( 14 / 53 ) stenosi aortica , steno - insufficienza aortica , insufficienza aortica patologia di altre valvole maschi sintomi angina pectoris no angina pectoris precedente im fattori di rischio ipertensione ipercolesterolemia diabete mellito fumo familiarit di cad obesit ( body mass index 30 kg / m2 ) calcium score coronarico c.s. 
due esami ( 2 / 55 , 3% ) relativi a pazienti affetti da stenosi aortica severa presentavano artefatti da movimento del torace cos marcati da non consentire la valutazione ac - tcms dei vasi coronarici , pertanto sono stati esclusi dallanalisi . 
in un paziente affetto da stenosi aortica severa ed aneurisma dellaorta ascendente ( 77 cm ) , loperatore della coronarografia non riuscito ad incannulare lostio della coronaria sinistra dominante nonostante tentativi , pertanto nellanalisi di questo vaso la ac - tcms ha sostituito la acc come metodica di riferimento . i numerosi radiol med ( 2009 ) 114 : 728742 736 radiol med ( 2009 ) 114 : 728742 table 6 coronary artery and valvular calcium score results in patients with aortic or mitral valve disease patients with aortic valve disease patients with mitral valve disease coronary artery volumetric calcium score valvular volumetric calcium score ascending aorta calcium burden ( 04 ) 2 , 527 0.92 tabella 6 risultati del calcium score coronarico e valvolare nei pazienti con valvulopatia aortica e mitralica pazienti con patologia valvolare aortica pazienti con patologia valvolare mitralica 1 , 101 1101 c.s. 
ten patients with no aortic calcium plaques ( classified as 0 ) had aortic stenosis ( 10 / 21 , 48% ) , two had aortic regurgitation ( 2 / 9 , 22% ) , four had aortic stenosis with regurgitation ( 4 / 10 , 40% ) , eight had mitral regurgitation ( 8 / 14 , 57% ) and one has mitral stenosis with regurgitation ( 1 / 1 , 100% )  . 
the mean aortic calcium score of the patients with aortic stenosis ( n = 21 ) was 0.92 , whereas it was 0.98 for patients with aortic regurgitation ( n = 9 ) , 0.87 for patients with aortic stenosis with regurgitation ( n = 10 ) , 1.00 for patients with mitral regurgitation ( n = 14 ) and 0.00 for patients with mitral stenosis and regurgitation ( n = 1 )  . 
in the study population , ctca identified ten ( 10 / 55 , 18% ) patients with an ascending aorta > 40 mof these patients , six had aortic valve regurgitation , corresponding to 67% ( 6 / 9 ) of all patients with aortic valve regurgitation . 
the following anatomical variants were identified : four cases of common origin of the innominate artery and left common carotid artery , one case of origin of the left vertebral artery from the aortic arch , one case of arteria lusoria and two cases of separate origin of the left anterior descending and left circumflex arteries . 
in addition , the radiologist identified the presence of one saccular aneurysm ( 9 mm ) of the left anterior descending artery and left circumflex artery ( 6.8 mm ) , two patients with marked thickening of the medial mitral valve leaflet , one patient with thickening of the right aortic valve leaflet and one patient with left ventricular apical thrombus . vessel - based analysis analysis of the prevalence of cad showed that the right analisi per paziente la ac - tcms ha documentato assenza di malattia significativa in 31 pazienti , 3 casi sono stati erroneamente valutati come positivi , riportando un valore di specificit pari al 91% . 
i pazienti affetti da patologia valvolare aortica presentavano un valore di calcio valvolare medio calcolato secondo lindice volumetrico pari a 2527 ; per i pazienti affetti da patologia valvolare mitralica tale valore risultato pari a 1101 . 
dei pazienti con assenza di placche calcifiche aortiche ( classificate come 0 ) , 10 erano affetti da stenosi aortica ( 10 / 21 , 48% ) , 2 da insufficienza aortica ( 2 / 9 , 22% ) , 4 da stenoinsufficienza aortica ( 4 / 10 , 40% ) , 8 da insufficienza mitralica ( 8 / 14 , 57% ) 1 da steno - insufficienza mitralica ( 1 / 1 , 100% )  . 
i pazienti affetti da stenosi aortica ( n = 21 ) presentavano una media di calcio aortico pari a 0 , 92 ; i ( n = 9 ) pazienti con insufficienza aortica di 0 , 98 ; i pazienti ( n = 10 ) con steno - insufficienza aortica di 0 , 87 ; i pazienti ( n = 14 ) con insufficienza mitralica pari a 1 ; i pazienti ( n = 1 ) con steno - insufficienza mitralica 0 . 
nella popolazione in studio la actcms ha identificato 10 ( 10 / 55 , 18% ) pazienti con aorta ascendente maggiore di 40 mm ; di questi pazienti in 6 presentavano insufficienza aortica , che corrispondono al 67% ( 6 / 9 ) del totale dei pazienti affetti da insufficienza valvolare aortica . 
sono state individuate le seguenti variante anatomiche : 4 origine comune del tronco anonimo e della carotide comune di sinistra , 1 origine della vertebrale sinistra dallarco aortico , 1 arteria lusoria , 2 origini separate dellarteria discendente anteriore e della circonflessa . 
inoltre il radiologo ha documentato la presenza di 1 aneurisma sacciforme ( 9 mm ) dellarteria discendente anteriore e dellarteria circonflessa ( 6 , 8 mm ) , due pazienti con lembo valvolare mitralico marcato mediale , un paziente con ispessimento del lembo valvolare aortico destro e un paziente con trombo apicale del ventricolo sinistro . ispessimento del analisi per vaso dallanalisi della prevalenza di malattia dei vasi coronarici risultato che la coronaria destra il vaso con la pi elevata localizzazione di stenosi significative ( 28% )  . 
dal confronto tra ac - tcms e acc emerso che la ac - tcms raggiunge la pi alta sensibilit e specificit ( rispettivamente del 100% e 98% ) nella valutazione del tronco comune , con il riscontro di 0 falsi negativi e 1 falso positivo . la minore sensibilit e specificit ( rispettivamente del 82% e 93% ) stata raggiunta nella valutazione della circonflessa con 2 falsi negativi e 3 falsi positivi . 
1 la ricostruzione multiplanare curva ( a destra ) mostra la coronaria destra priva di lesioni , confermata dallangiografia convenzionale ( a sinistra )  . coronary artery was the vessel most commonly affected by significant stenosis ( 28% )  . 
comparison between ctca and cca revealed that ctca achieved the highest level of sensitivity and specificity ( 100% and 98% , respectively ) in the evaluation of the left main coronary artery , with no false negatives and one false positive . 
the lowest sensitivity and specificity ( 82% and 93% , respectively ) was reached in the evaluation of the left circumflex artery , with two false negatives and three false positives . 
the sensitivity and ppv of ctca were therefore 80% and 82% , respectively . subanalysis of patients with aortic valve disease versus mitral valve disease in group a patients ( aortic stenosis , aortic stenosis with regurgitation , aortic regurgitation ) , the prevalence of disease was 45% , whereas in group b ( mitral stenosis , mitral stenosis with regurgitation ) it was 13% . 
the agatston calcium score ( 731 ) and the volumetric calcium score subanalisi per pazienti con patologia valvolare aortica versus patologia mitralica nei pazienti del gruppo a ( stenosi , steno - insufficienza ed insufficienza aortica ) abbiamo riscontrato prevalenza di 738 radiol med ( 2009 ) 114 : 728742 fig . 
4 limmagine volume - rendered ac - tcms ( a sinistra ) e la ricostruzione multiplanare ( a destra ) dimostrano la perviet della coronaria sinistra confermata dalla acc ( al centro )  . ( 2577 ) in patients in group b were greater than in those in group a ( 693 and 2 , 434 , respectively )  . 
3 ricostruzione multiplanare curva e relativa sezione trasversa ( a destra ) dimostrano una stenosi > 50% allorigine del ramo interventricolare posteriore della coronaria destra ( a ) confermata dalla cag ( a sinistra ) ; b ramo postero - laterale indenne . malattia del 45% , mentre i pazienti del gruppo b ( stenosi , steno - insufficienza mitralica ) del 13% . 
il calcium score coronarico secondo agatston ( 731 ) e il calcium score valvolare volumetrico ( 2577 ) dei pazienti del gruppo b sono risultati maggiori dei pazienti del gruppo a ( rispettivamente : 693 e 2434 ) , ma in modo non significativo . 
dai risultati della diagnosi delle stenosi coronariche maggiori o uguali al 50% , emerso che nei pazienti del gruppo a la ac - tcms ha riportato sensibilit del 100% , specificit dell86% e valore predittivo positivo dell85% per la presenza di 3 falsi positivi , mentre nei pazienti del gruppo b del 100% , del 100% e del 100% rispettivamente . subanalisi dei pazienti con angina pectoris nella popolazione oggetto di studio i pazienti che riferivano angina pectoris ( ap ) sono stati 16 mentre in 39 hanno negato tale sintomo . 
escludendo i 2 pazienti con stenosi e steno - insufficienza aortica con marcati artefatti da respirazione che negavano di essere affetti da ap , i 36 pazienti rimanenti senza ap presentavano inferiore prevalenza di malattia ( 22% ) rispetto ai pazienti con ap ( 38% )  . 
laccuratezza diagnostica delle stenosi coronariche significative dei pazienti con ap stata valutata mediante sensibilit ( 100% ) , specificit ( 90% ) , valore predittivo positivo ( 86% ) e valore predittivo negativo ( 100% )  . radiol med ( 2009 ) 114 : 728742 86% and ppv of 85% , with the presence of three false positives , whereas the rates in group b were 100% , 100% and 100% , respectively . discussione subanalysis of patients with angina pectoris of the 55 patients in the study population , 16 reported ap and 39 denied having symptoms . 
with the exclusion of the two patients with stenosis and stenosis with regurgitation whose examinations were compromised by thoracic wall motion artefacts , the prevalence of disease in the remaining 36 patients without ap ( 22% ) was lower than in the group of patients with ap ( 38% )  . 
the diagnostic accuracy of significant coronary stenoses of patients with ap was evaluated with sensitivity ( 100% ) , specificity ( 90% ) , ppv ( 86% ) and npv ( 100% )  . discussion it has been demonstrated that there is a significant independent correlation between the progression of calcifications in coronary arteries and in the aortic valve , thus suggesting similar mechanisms [ 11 ]  . 
in our study , it was also seen that groups of patients with a volumetric coronary artery calcium score > 1 , 000 had similar percentages of risk factors to the group of patients with volumetric aortic valve calcium score > 1 , 000 , with a greater prevalence of hypertension and hypercholesterolaemia . 
we found no significant differences in the aortic calcium burden between the groups of patients affected by aortic and mitral valve disease . with regard to the clinical characterisation of patients with aortic valve disease , the following parameters are traditionally evaluated : measurement of aortic velocity , mean transaortic pressure gradient and continuity equation valve area [ 12 ]  . 
some authors , however , contend that percutaneous coronary intervention in patients with symptoms of angina or dyspnoea with aortic valvular stenosis and significant cad is a safe procedure able to improve symptoms in most cases and postpone heart valve surgery [ 14 ]  . there is therefore an indication for performing cca prior to valve replacement surgery in patients with severe aortic valve stenosis and angina pectoris to decide , in the case of significant cad , whether or not to perform cabg together stato dimostrato che esiste una correlazione indipendente significativa tra la progressione delle calcificazioni nelle arterie coronarie e nella valvola aortica , suggerendo simili meccanismi patogenetici [ 11 ]  . 
anche nel nostro studio , il gruppo di pazienti con calcium score coronarico volumetrico maggiore di 1000 , presentavano percentuali di fattori di rischio simili al gruppo di pazienti con calcium score volumetrico valvolare aortico maggiore di 1000 , con maggiore prevalenza di ipertensione e ipercolesterolemia . non abbiano riscontrato differenze significative del carico di calcio aortico tra i gruppi di pazienti affetti da patologia valvolare aortica e mitralica . 
 per quanto riguarda linquadramento clinico del paziente affetto da patologia valvolare aortica , tradizionalmente si valutano i seguenti parametri : velocit del sangue attraverso la stenosi valvolare , gradiente pressorio medio tra ventricolo sinistro e aorta e larea di apertura valvolare [ 12 ]  . 
tuttavia stato dimostrato che la sintomatologia del paziente il miglior indicatore della significativit emodinamica della stenosi valvolare , pertanto unaccurata anamnesi essenziale perch influenza in modo significativo la pianificazione terapeutica [ 13 ]  . 
invece secondo altri autori lintervento coronarico percutaneo ( icp ) condotto su pazienti sintomatici per angina o dispnea con stenosi valvolare aortica e mac significativa , una procedura sicura che provoca miglioramento dei sintomi nella maggior parte dei casi e permette di posporre lintervento di sostituzione valvolare [ 14 ]  . 
quindi esiste indicazione nei pazienti con stenosi valvolare aortica severa e angina pectoris , prima della sostituzione valvolare ad effettuare acc per decidere , in caso di mac significativa , se effettuare rivascolarizzazione con by - pass nello stesso tempo chirurgico dellintervento valvolare . 
nel caso di un paziente con stenosi valvolare aortica moderata e angina pectoris , se presente mac significativa , consigliabile eseguire in un primo tempo la rivascolarizzazione percutanea e quindi verificare la risoluzione del sintomo anginoso ; se tale sintomo persiste la causa potrebbe essere valvolare , pertanto opportuno procedere con la sostituzione valvolare [ 12 ]  . 
con il nostro studio abbiamo dimostrato che la ac - tcms possiede unelevata sensibilit , specificit e valore predittivo negativo ( 100% , 91% , 100% ) nella valutazione della mac rispetto alla acc nei pazienti candidati alla sostituzione valvolare . 
in the case of a patient with moderate aortic stenosis and angina pectoris , if significant cad is present , it is advisable to perform percutaneous revascularisation and then verify resolution of the angina . 
our study shows that ctca has high sensitivity , specificity and npv ( 100% , 91% , 100% , respectively ) in the evaluation of cad when compared with cca in patients referred for heart valve surgery . 
in particular , the elevated negative predictive value suggests ctca may be used in the preoperative phase to identify patients with no cad , thus ensuring that in this large group of patients ( 31 / 55 , 58% ) , no further costly and invasive examinations are performed . 
a comparison of 64slice ct in the analysis of cad with 16 - slice [ 13 , 16 ] and 40 - slice [ 17 ] scanners reveals that the diagnostic performance in our study is greater than that obtained with scanners with fewer detectors and comparable with that obtained with 64 - slice scanners on a patient population without mitral valve disease [ 18 ] , a condition known to be associated with a higher rate of ventricular arrhythmias [ 19 ] that worsen the diagnostic quality of the examination [ 20 ]  . current guidelines recommend valve replacement surgery in the presence of mitral regurgitation with significant symptoms or initial left ventricular dysfunction with ventricular dimension reaching 45 mm in the end - diastolic phase . 
surgery may also be indicated , even in the absence of symptoms or signs of left ventricular dysfunction if atrial fibrillation appears or pulmonary pressure exceeds 50 mmhg [ 7 ]  . 
in our experience , all images regarding patients with atrial fibrillation were considered of sufficiently diagnostic quality such that atrial fibrillation does not appear to be an exclusion criterion for patients referred for ctca . 
in these patients , high - quality images of the coronary tree can be obtained by positioning the time window in the end - systolic phase [ 22 ]  . 
this is because although the width of the r - r interval varies in each cardiac cycle in patients with atrial fibrillation , the difference of the width between end - diastolic intervals is greater than endsystolic intervals and between the rapid filling intervals in diastole , because their individual duration is shorter [ 22 ]  . 
in addition , images reconstructed with absolute delay tend to be of higher quality than images reconstructed with relative delay [ 22 ]  . lelevato valore predittivo negativo ci permette di proporre luso della ac - tcms in fase preoperatoria per individuare i pazienti senza mac evitando che siano condotte su questo numeroso gruppo ( 31 / 53 , 58% ) indagini pi invasive e pi costose . 
confrontando i risultati della tc 64 - strati nellanalisi della mac con studi condotti su scanner a 16 [ 3 , 16 ] e 40 - strati [ 17 ] , la performance diagnostica nel nostro studio non solo risulta migliore a quella ottenuta da scanner con minor numero di detettori ma addirittura comparabile a quella condotta con scanner a 64 - strati su una popolazione di pazienti senza patologia mitralica [ 18 ] , che presenta notoriamente maggiore incidenza di aritmie ventricolari [ 19 ] che peggiorano la qualit diagnostica dellesame [ 20 ]  . le attuali linee guida raccomandano lintervento di sostituzione valvolare mitralica per insufficienza mitralica in caso di sintomi importanti o allesordio di disfunzione ventricolare sinistra tipo dilatazione ventricolare con dimensione ventricolare di 45 mm in fase tele - diastolica . lintervento chirurgico pu inoltre essere indicato anche in assenza di sintomi o segni di disfunzione ventricolare sinistra se compare fibrillazione atriale o se la pressione polmonare supera i 50 mmhg [ 7 ]  . 
nella nostra esperienza tutte le immagini relative a pazienti con fibrillazione atriale sono state considerate di sufficente qualit diagnostica pertanto abbiamo riscontrato che la fibrillazione atriale non costituisce un fattore di esclusione della popolazione da sottoporre a ac - tcms . 
la spiegazione di questo risultato che sebbene lampiezza dellintervallo r - r varia in ogni ciclo cardiaco nei pazienti con fibrillazione atriale , la differenza di ampiezza tra gli intervalli tele - diastolici maggiore di quella tele - sistolici e tra gli intervalli di riempimento rapido nella diastole perch minore la loro singola durata [ 22 ]  . 
la presenza di severa aterosclerosi aortica responsabile dellaumento del rischio di morte radiol med ( 2009 ) 114 : 728742 cerebral ischaemic events constitute a highly relevant complication for the approximately 1 million patients who undergo heart surgery each year throughout the world [ 23 ]  . the presence of severe aortic atherosclerosis is responsible for the increased risk of intraoperative mortality due to infarction , hypoxic encephalopathy , stroke or transient ischaemic attack [ 23 ]  . 
mdct is able to identify the lesions that increase surgical risk : aortic atherosclerotic plaque , intracardiac thrombus and nodules on the valve leaflets . identification of these lesions requires modification of the surgical approach and the use of alternative techniques to minimise the risk of embolism [ 23 ]  . 
moreover , in our study , mdct proved decisive in the preoperative phase for the choice of the most appropriate surgical approach in the two patients with bicuspid aortic valve and aneurysm of the ascending aorta , in the ten patients with ascending aorta > 40 mm and in the patient with aneurysm ( 77 cm ) of the ascending aorta in whom cca was incomplete due to the failure to cannulate the left coronary artery . limitations and prospects in order to perform the evaluation of the aortic arch and coronary arteries in a single angiographic scan , we used a field of view that was larger along the z axis , such that the effective dose delivered to the patient was greater than in similar studies where the calcium burden of the aortic arch was not evaluated [ 24 ]  . our study was not done with a double - blind analysis of the ctca and cca images but by a single , highly experienced operator . 
as a result , we are unable to comment on the effective reproducibility of the excellent results achieved . a continuation of our study with a greater number of patients will allow us to verify the existence of a correlation between valvular calcium score , valvular diameter and aortic velocity measured with magnetic resonance imaging and pressure gradient measured with catheterisation and compare our findings with the data reported in the literature [ 10 ]  . 
we believe it would also be useful to investigate the existence of a correlation between aortic calcium score and intraand postoperative neurological events . conclusions ctca was demonstrated to have high sensitivity , specificity and npv in the evaluation of cad in patients referred for heart valve surgery , regardless of bmi , heart rate and arrhythmias , which tend to be particularly frequent in patients with mitral valve disease . 
inoltre la tc stata decisiva in fase preoperatoria per scegliere lapproccio chirurgico migliore nei due pazienti con valvola aortica bicuspide ed aneurisma dellaorta ascendente , nei 10 pazienti con aorta ascendente maggiore di 40 mm e nel paziente con aneurisma ( 77 cm ) dellaorta ascendente in cui la acc stata incompleta per il fallimento di incanulazione della coronaria sinistra . limiti e prospettive per eseguire in ununica scansione angiografica la valutazione dellarco aortico e delle coronarie abbiamo utilizzato un fov di dimensioni maggiori lungo lasse z , pertanto la dose effetiva del paziente risultata superiore rispetto ad altri studi analoghi in cui non si valutava il carico ateromasico dellarco aortico [ 24 ]  . 
 il nostro studio non stato condotto con analisi delle immagini della ac - tcms e della acc in doppio cieco , ma in singolo operatore con esperienza specifica pluriennale , pertanto non conosciamo riproducibilit delleccellente risultato riportato . 
 leffettiva la nostra proseguendo indagine con un numero maggiore di pazienti abbiamo intenzione di verificare lesistenza di una correlazione tra calcium score valvolare , diametro della valvola e velocit del flusso transvalvolare mediante misurazione con rm e gradiente pressorio misurato tramite cateterismo e intendiamo confrontare tale risultato con i dati rilevati in letteratura [ 10 ]  . 
riteniamo utile lesistenza di una correlazione tra calcium score aortico ed eventi neurologici intrae post - operatori . conclusioni nei pazienti candidati alla sostituzione valvolare cardiaca , senza esclusioni sulla base del valore di bmi , della frequenza cardiaca , della presenza di aritmie peraltro frequenti particolarmente nei pazienti con patologia mitralica , la ac - tcms ha dimostrato elevata sensibilit , specificit e valore predittivo negativo nella valutazione della mac . 
in particolare , lelevato valore predittivo negativo della ac - tcms consente di utilizzare tale metodica in fase preoperatoria per individuare i pazienti senza mac 742 radiol med ( 2009 ) 114 : 728742 negative predictive value of ctca makes it possible to use the technique in the preoperative phase to identify patients without cad and avoid the need for invasive and costly cca in these patients . the elevated accuracy of ctca in the evaluation of aortic atherosclerosis , an important surgical risk factor , and in the identification of aortic aneurysms is a further point in favour of the introduction of the technique in the diagnostic protocol of patients referred for heart valve surgery . evitando che siano condotte su questo gruppo indagini pi invasive e pi costose come la acc . 
 lelevata accuratezza diagnostica della tcms nella valutazione dellaterosclerosi aortica che costituisce importante fattore di rischio operatorio e nellidentificazione della patologia aneurismatica aortica rappresenta ulteriore elemento favorente lintroduzione di tale metodica nelliter diagnostico dei pazienti candidati alla sostituzione valvolare cardiaca . 
cademartiri1 , 4 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria di parma , parma , italy 2fondazione - irccs - sdn , napoli , italy 3dipartimento di radiologia , universit degli studi di napoli federico ii , napoli , italy 4dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , paesi bassi correspondence to : f . 
cademartiri , dipartimento di radiologia , c / o piastra tecnica piano 0 , azienda ospedaliero - universitaria , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703516 , fax : + 39 - 052 - 1703630 , e - mail : filippocademartiri@hotmail.com received : 11 september 2008 / accepted : 18 november 2008 / published online : 23 june 2009 springer - verlag 2009 abstract purpose . 
results were compared with students t test for paired samples , pearsons r correlation coefficient and r2 coefficient of determination ; ejection fraction differences were assessed with bland - altman analysis . 
le scansioni 2d cine b - ssfp sono state utilizzate per la valutazione funzionale del ventricolo sinistro e i data - set ottenuti sono stati valutati utilizzando due software dedicati : viewforum versione 4.2 e argus versione va60c . 
nella nostra esperienza i software radiol med ( 2009 ) 114 : 718727 keywords cardiac magnetic resonance left ventricular volumes quantitative software ejection fraction . comunemente utilizzati forniscono risultati sovrapponibili in un tempo comparabile . parole chiave risonanza magnetica cardiaca volumi ventricolo sinistro software quantitativo frazione di eiezione introduction introduzione cardiac performance is key to determining disease stage and evaluating the effectiveness of treatment over time [ 1 ]  . an accurate , reproducible and quantitative evaluation of left ventricular ( lv ) function is possible , and the examination that guarantees the best results in terms of accuracy and reproducibility is magnetic resonance ( mr ) imaging [ 2 ]  . 
in particular , using two - dimensional ( 2d ) cine gradient - echo balanced steady - state free precession ( ge b - ssfp ) sequences , high - quality images are obtained that have excellent spatial , temporal and contrast resolution [ 3 , 4 ]  . these 2d gradient - echo balanced sequences are the standard of reference in the evaluation of ventricular volumes [ 5 , 6 ]  . 
the aim of our study was to compare the lv volume values obtained with two semiautomated dedicated software packages . materials and methods patients from march to august 2007 , all patients undergoing cardiac mr imaging were prospectively enrolled in the study ( 46 patients )  . 
exclusion criteria were absolute or relative contraindications to mr imaging [ 7 ] , and inclusion criteria were breath - hold capacity of at least 10 s for at least 5 consecutive times . mr imaging all images were acquired with a 1.5 - t scanner ( achieva , philips medical systems , best , the netherlands ) characterised by a maximum achievable gradient strength of 66 mt / m , and a maximum slew rate of 180 mt / m / ms . during the cine b - ssfp sequences , the maximum gradient strength was 33 mt / m and the maximum slew rate was 180 mt / m / ms . 
the 2d cine b - ssfp sequence was performed in the la performance cardiaca rappresenta attualmente un elemento cardine nel determinare lo stadio della malattia e nel valutare nel tempo lefficacia di uneventuale terapia [ 1 ]  . 
la valutazione della funzione ventricolare sinistra pu essere fatta in maniera accurata , riproducibile ed in maniera quantitativa ; lesame che garantisce migliori risultati di accuratezza e riproducibilit la risonanza magnetica ( rm ) [ 2 ]  . 
in particolare utilizzando sequenze 2d cine gradient echo balanced steady - state free precession ( ge bssfp ) si ottengono immagini di ottima qualit grazie alleccellente risoluzione spaziale , temporale e di contrasto [ 3 , 4 ]  . 
scopo del nostro lavoro stato confrontare i valori dei volumi cardiaci del ventricolo sinistro ottenuti da due differenti software semiautomatici dedicati . materiali e metodi pazienti dal marzo ad agosto 2007 , tutti i pazienti che sono stati sottoposti a rm cardiaca sono stati arruolati prospetticamente nello studio ( 46 pazienti )  . 
criteri di inclusione : capacit di mantenere unapnea di almeno 10 secondi per almeno 5 volte consecutive . imaging rm tutte le immagini sono state acquisite con uno scanner da 1 , 5 t ( achieva , philips medical systems , best , olanda ) caratterizzato da una massima forza di gradiente sviluppabile 66 mt / m e massimo slew / rate sviluppabile 180 mt / m / ms . 
durante le sequenze cine b - ssfp la massima forza di gradiente raggiungibile stata 33 mt / m e il massimo slew / rate pari a 180 mt / m / ms . 
sono stati utilizzati 720 table 1 study population patient characteristics ( n = 46 ) male / female ( no . ) mean age ( years ) mean weight ( kg ) mean heart rate ( bpm ) value range shown in parentheses caratteristiche dei pazienti ( n = 46 ) uomini / donne ( n ) et media ( anni ) peso medio ( kg ) frequenza cardiaca media ( bpm ) valore range mostrato tra parentesi 29 / 17 51 ( range 1683 ) 74.7 ( range 46113 ) 65.7 ( range 44102 ) 29 / 17 51 ( range 1683 ) 74 , 7 ( range 46113 ) 65 , 7 ( range 44102 ) tabella 1 caratteristiche generali della popolazione esaminata short axis , with coverage of the entire lv . 
evaluations were made blindly by an experienced operator who determined , for each patient , the ejection fraction ( ef ) , end - diastolic volume ( edv ) , end - systolic volume ( esv ) , stroke volume ( sv ) and cardiac output ( co ) with the two software packages , according to the criteria published in the literature [ 8 ]  . 
once the end - diastolic and end - systolic phases had been identified , the endocardial and epicardial contours were traced on the end - diastolic views . the endocardial contours were then propagated to all of the other cardiac phases , and the errors made by the software during propagation were corrected . 
the papillary muscles and the subendocardial trabeculae were included in the lv cavity [ 9 , 10 ]  . the time required by the operator to make the evaluations on the two consoles was also recorded . 
interobserver variability was assessed by having a second operator reevaluate all 46 patients with the argus software . radiol med ( 2009 ) 114 : 718727 una bobina a 5 elementi ed un elettrocardiogramma vettoriale per la ricezione del segnale e per la sincronizzazione cardiaca . 
altri parametri relativi alla sequenza 2d utilizzata : tr 3 , 1 , te 1 , 53 ; flip angle 60 ; banda 1249 , 7 hz / pixel ; risoluzione in plane 22 , 3 mm ; spessore di strato 8 mm ; intervallo tra strati 2 mm ; risoluzione temporale 31 , 525 , 93 ms ( dipendente dalla frequenza cardiaca ) ; fasi cardiache 30 ; sense off ; half scan on . 
le valutazioni sono state effettuate in cieco da un operatore esperto che ha effettuato le misurazioni volumetriche della frazione di eiezione ( fe ) , del volume tele - diastolico ( vtd ) , del volume tele - sistolico ( vts ) , della gittata sistolica ( gs ) e della gittata cardiaca ( gc ) utilizzando i due software per ciascun paziente seguendo i criteri pubblicati in letteratura [ 8 ]  . dopo aver identificato le fasi di telediastole e telesistole sono stati tracciati i contorni endocardici ed epicardici sulle immagini in telediastole ; i contorni endocardici sono stati poi propagati a tutte le altre fasi acquisite e si poi proceduto a correggere gli errori commessi dal software durante la propagazione . 
per una stima della variabilit intra - osservatore stata effettuata per due volte la valutazione di 20 pazienti utilizzando il software viewforuper una stima della variabilit interosservatore tutti i 46 pazienti sono stati valutati una seconda volta sul software argus da un secondo operatore . analisi statistica tutti i dati sono stati raggruppati e sono stati analizzati mediante test t di student per dati appaiati , test di correlazione ( r ) , di determinazione r2 e test di bland - altman . risultati la valutazione della volumetria del ventricolo sinistro effettuata con i due software non ha mostrato differenze radiol med ( 2009 ) 114 : 718727 fig . 
in a la finestra nella quale viene effettuata la segmentazione dei contorni endocardici ed epicardici . in b la finestra che mostra i risultati dellanalisi volumetrica . statistical analysis all data were collected and analysed with the student t test for paired data , the correlation coefficient ( r ) , the determination coefficient ( r2 ) and the bland - altman test . results evaluation of lv volume with the two software packages showed no significant differences ( table 2 )  . 
il tempo impiegato dalloperatore per calcolare i suddetti parametri utilizzando il software viewforum rispetto al software argus stato rispettivamente di 7 , 62 , 78 min vs 7 , 522 , 4 min ( p > 0 , 50 ; r = 0 , 85 ; r2 = 0 , 73 )  . 
the graph shows minimal dispersion of the data calculated with the two packages compared with the straight regression line for all ejection fraction values ( r2 = 0.82 ) : software performance does not decline in the six patients with depressed ef ( < 30% )  . 
il grafico dimostra una minima dispersione dei dati raccolti utilizzando i due software rispetto alla retta di regressione per tutti i valori di frazione di eiezione ( r2 = 0 , 82 ) : nei 6 pazienti con frazione deiezione depressa ( < 30% ) non si osserva un calo della performance dei due software . 
analisi di bland - altman della frazione di eiezione risultante dal calcolo dei volumi del ventricolo sinistro su workstation viewforum e argus ; sono stati utilizzati dei limiti di concordanza di 1 , 96 ds . 
to obtain more accurate and reproducible results in a la risonanza magnetica rappresenta attualmente lesame di riferimento per la valutazione volumetrica del ventricolo sinistro e lesame standard deve sempre comprendere acquisizioni dinamiche per lo studio di volumi e contrattilit . 
limplementazione degli scanner con nuovi software dedicati caratterizzati da interfacce pi intuitive e algoritmi pi sofisticati ugualmente importante rispetto allottimizzazione e / o introduzione di nuove sequenze per ottenere risultati pi accurati e riproducibili in minor tempo . lintroduzione di nuovi software dovrebbe essere preceduta da test di validazione rispetto a software conosciuti in popolazioni eterogenee di pazienti . 
i parametri volumetrici studiati dal secondo operatore non hanno mostrato differenze significative ( p > 0 , 05 ) vts ( ml ) gs ( ml ) fe ( % ) gc ( l / min ) fe , frazione di eiezione ; vtd , volume tele - diastolico ; vts , volume tele - sistolico ; gs , gittata sistolica ; gc , gittata cardiaca ; ds , deviazione standard ; min , valore minimo ; max , valore massimo fig . 
software packages may differ in several aspects : incorrect programming ( now extremely rare ) , use of different algorithms to identify enddiastolic and end - systolic phases and algorithms used for identifying the endo / epicardial contours during the propagation phase . 
error in the search for contours during the propagation phase makes the analysis time consuming , as a large number of images need to be corrected ( around 180240 images )  . in our study , we compared the performance of two common cardiac software programmes for the evaluation of ventricular function with 2d cine b - ssfp sequences . 
intraobserver and interobserver reproducibility , as measured with the viewforum and argus software , respectively , proved to be excellent in relation to the operators experience and to the intuitive display . limitations although our study sample was small , it comprised a similar number of patients to the main published series on the topic . we did not consider all of the software packages available on the market . 
nevertheless , the two packages investigated are most common and well - established platforms for the evaluation of lv volume in cardiac mr imaging . di propagazione ha conseguenze negative sul timeconsuming dellanalisi in quanto le correzioni devono essere fatte su un numero di immagini non trascurabile ( circa 180240 immagini )  . nel nostro studio stata confrontata la performance di due comuni software cardiologici dedicati alla valutazione della funzione ventricolare mediante sequenze 2d cine bssfp . 
la riproducibilit intra - osservatore dei risultati , valutata con software viewforum , e la variabilit inter - osservatore , valutata con software argus , si sono dimostrate ottime in relazione allesperienza delloperatore e alla semplicit dellinterfaccia di visualizzazione . limitazioni il numero di pazienti analizzato non stato elevato , tuttavia , le principali casistiche focalizzate su design similare fanno riferimento a numeri analoghi . 
tuttavia , si tratta di due piattaforme tra le pi diffuse e consolidate per la valutazione volumetrica del ventricolo sinistro in cardio - rm . conclusioni conclusions the software packages for the quantitative evaluation of lv volumes used in our study showed an excellent level of concordance , and all measurements were obtained within a reasonable time , compatible with average reporting times in routine clinical practic i software per valutazione volumetrica quantitativa del ventricolo sinistro utilizzati nel nostro studio hanno mostrato ottima concordanza nella valutazione dei volumi ventricolari e i risultati sono stati ottenuti in tempi ragionevoli , compatibili con un tempo medio di refertazione nel contesto clinico routinario . 
torricelli1 1dipartimento integrato dei servizi diagnostici e per immagine , cattedra e servizio di radiologia 1 , 2dipartimento integrato di emergenza - urgenza , 3dipartimento di statistica , universit degli studi di modena e reggio emilia , azienda ospedaliero universitaria policlinico , via del pozzo 71 , 41100 modena , italy correspondence to : f . 
diastolic wall thickness ( dwt ) , dobutamine - induced systolic wall thickening ( swt ) and de transmural extension were quantitatively assessed in vessel - related segments , calculating the contribution of viable tissue to swt , expressed as viability index ( vi ) = [ swt ( 100 de ) ] / 100 . 
ventitr pazienti con cto sono stati sottoposti rm con contrasto e dobutamina a bassa dose . sono stati valutati quantitativamente spessore telediastolico ( dwt ) , telesistolico ( swt ) e enhancement tardivo ( de ) nei segmenti relativi al vaso occluso , calcolando il contributo del tessuto vitale a swt , espresso come viability index ( vi ) = [ swt ( 100 - de ) ] / 100 . 
 parole chiave occlusione coronarica cronica percutaneous coronary intervention rm con dobutamina a bassa dose introduction introduzione chronic total coronary occlusions ( cto ) are observed in 35%50% of patients with significant coronary disease undergoing diagnostic angiography [ 1 , 2 ]  . 
although there have been numerous advances in the field of percutaneous coronary intervention , cto treatment remains a major challenge and is a frequent reason for referrals to cardiac surgery . 
furthermore , a large proportion of patients with cto is managed medically , the prognosis of which may vary depending on the extent of viable myocardium and ischaemia [ 4 ]  . 
the different approaches to cto are due to the fact that improvement after revascularisation is not easily predictable [ 5 ]  . in patients with cto , the vessel - related myocardium may show contractile impairment and yet be partly healthy and partly necrotic . 
the presence of severe chronic contractile dysfunction is no longer considered a contraindication to revascularisation : it has been demonstrated that patients with hibernating myocardium have a better outcome if treated invasively rather than with medical therapy [ 9 , 10 ]  . 
furthermore , retrospective observational reports [ 11 ] have documented the clinical impact of successful percutaneous cto revascularisation on long - term survival , and other studies have demonstrated statistically significant improvements in left ventricular function and regional wall motion with successful cto recanalisation [ 1219 ]  . low - dose dobutamine ( ld ) and delayed - enhancement ( de ) magnetic resonance imaging ( mri ) can evaluate contractile reserve and viability in myocardium subtended by cto in order to identify patients with potential viable myocardium that may benefit from revascularisation . 
diversi miglioramenti sono avvenuti negli ultimi anni nel campo della cardiologia interventistica , tuttavia il trattamento delle cto rimane una delle sfide maggiori per il cardiologo interventista , essendo campo di lavoro specifico per il cardiochirurgo . 
i differenti approcci alla terapia delle cto sono dovuti alla difficile valutazione del miglioramento post - rivascolarizzazione [ 5 ]  . nei pazienti con cto , il miocardio vascolarizzato dal vaso cronicamente occluso pu mostrare una alterazione contrattile ed essere contemporaneamente in parte vitale ed in parte necrotico . 
la presenza di alterazione contrattile severa e cronica non pi considerata una controindicazione alla rivascolarizzazione : stato infatti dimostrato che pazienti che presentano miocardio ibernato hanno un outcome migliore se trattati invasivamente rispetto a pazienti trattati con la sola terapia medica [ 9 , 10 ]  . 
moreover , change in left ventricular ejection fraction ( lvef ) was analysed . materials and methods study population between december 2006 and september 2007 , we enrolled 23 patients ( 21 men ; 91% ) ; mean age 65.710.6 years , with single chronic coronary occlusion . 
cto was defined as a complete occlusion of a major coronary artery for at least 3 months as obtained from previous angiogram or a clinical history of prolonged anginal chest pain or myocardial infarction . 
twochamber , four - chamber and multiple short - axis views were acquired using the fast gradient echo technique ( 8 - mm thick ; 0.8 - mm gap in multislice acquisition )  . 
acquisition parameters were te = 4.5 ms , tr = 2.2 ms , flip angle = 55 , acquired voxel = 2.034.148.0 , reconstructed voxel = 1.521.538.0 , acquisition matrix = 192256 . 
short - axis breath - hold valutare la riserva contrattile e la vitalit del miocardio sotteso alla cto , permettendo di identificare pazienti selezionati con miocardio potenzialmente vitale che potrebbero beneficiare dalla rivascolarizzazione . 
la concordanza tra rm con mezzo di contrasto e con dobutamina a bassa dose alta nei casi estremi ( infarti transmurali o subendocardici ) ma non nei segmenti con estensione intermedia del danno miocardico . 
in questo gruppo di pazienti pertanto lintegrazione della valutazione dellestensione e della transmuralit del tessuto cicatriziale esito di infarto con la valutazione quantitativa della riserva contrattile permetterebbe una identificazione ottimale dei segmenti con probabilit maggiore di ripresa funzionale post - rivascolarizzazione [ 20 ]  . lo scopo del nostro studio stato di valutare quantitativamente il valore della rm con dobutamina a bassa dose e con studio del de per predire la ripresa funzionale nei pazienti con cto da sottoporre a rivascolarizzazione percutanea con impianto di stent medicati . 
la perviet del vaso trattato e la ripresa funzionale sono stati verificati a 6 mesi mediante angiografia coronarica e rm a riposo . inoltre la modificazione della frazione di eiezione ( fe ) ventricolare sinistra stata analizzata . materiali e metodi popolazione di studio sono stati arruolati 23 pazienti ( 21 maschi ; 91% ) tra dicembre 2006 e settembre 2007 ( et media 65 , 710 , 6 anni ) con occlusione coronarica cronica di un singolo vaso . la cto stata definita come occlusione completa di un vaso coronarico maggiore per almeno tre mesi sulla base di valutazione angiografica o storia clinica di prolungato dolore toracico o infarto miocardico . 
le caratteristiche della popolazione di pazienti sono descritte nella tabella 1 . protocollo di studio rm a riposo lesame rm stato eseguito utilizzando un magnete superconduttivo a 3 tesla ( intera cv , philips medical system , best , olanda ) , con intensit di picco di 33 mt / m , tempo di picco di 0 , 2 ms e ripidit di 150 mt / m / s . 
sono state acquisite sezioni cardiache su pi piani ( piano due camere , piano quattro camere e multipli assi corti ) utilizzando sequenze veloci ad eco di gradiente ( 8 mm spessore ; 0 , 8 mm intervallo nelle acquisizioni multislice )  . 
lacquisizione in asse corto ha utilizzato un fattore sense pari a 1 , 6 ; due fette sono state acquisite in una singola apnea . rm con dobutamina a bassa dose la dobutamina stata somministrata per via endovenosa senza rimuovere il paziente dal magnete , con monitoraggio constante dellelettrocardiogramma , della pressione sanguigna e con sorveglianza visiva del paziente . 
multipli assi corti e immagini sul piano quattro camere sono stati acquisiti utilizzando la stessa sequenza e geometria dellesame a riposo . rm con studio del delayed enhancement la distribuzione tardiva del contrasto stata ottenuta 15 minuti dopo la somministrazione di gadolinio - dota ( 0 , 1 mmol / kg ) utilizzando una sequenza 3d ad eco di gradiente con modalit inversion recovery , con un pre - impulso di inversione ottimizzato per la massima soppressione del segnale del miocardio . 
i parametri della sequenza sono stati : spessore = 5 mm , te = 1 , 32 ms , tr = 4 , 4 ms , flip angle = 15 gradi , voxel acquisito = 1 , 372 , 1410 , 0 , voxel ricostruito = 1 , 371 , 375 , 0 , fattore turbo = 37 , matrice di acquisizione = 256256 . cad , coronary artery disease ; pci , percutaneous coronary intervention acquisition was completed with parallel imaging using a sense factor of 1.6. 
 follow - up low - dose dobutamine mri without removing the patient from the magnet , dobutamine was administered intravenously under continuous electrocardiography ( ecg ) , blood pressure and visual monitoring . a cardiologist was present throughout dobutamine infusion . a 6 mesi dopo la procedura di rivascolarizzazione ciascun paziente stato sottoposto a follow - up clinico , angiografico e mediante rm . 
al followup stata valutata la ripresa funzionale per definire lefficacia della procedura percutanea di rivascolarizzazione . 696 radiol med ( 2009 ) 114 : 692704 using a perfusion pump , we administered an increasing dobutamine dose of 5 and 10 mg / kg per minute for 3 min each [ 21 ]  . 
multiple short - axis and four - chamber views were acquired using the same sequence and geometry settings as the rest of the study . delayed - enhancement mri delayed - enhancement distribution was evaluated 15 min after gadolinium - dota ( 0.1 mmol / kg ) injection using a 3d inversion recovery gradient turbo field echo sequence , with prepulse delay optimised for maximum myocardial signal suppression . 
imaging parameters were thickness = 5 mm , te = 1.32 ms , tr = 4.4 ms , flip angle = 15 , acquired voxel = 1.372.1410.0 , reconstructed voxel = 1.371.37.0 , turbo factor = 37 , acquisition matrix = 256256 . follow - up six months after successful angioplasty , patients underwent clinical , angiographic and mri follow - up examinations , the latter consisting in a rest cine and delayed - enhancement study performed with the same technique as in the baseline study . 
at follow - up , functional recovery was evaluated to define a successful percutaneous coronary intervention ( pci ) procedure . data evaluation image analysis was performed on an off - line workstation ( viewforum release 4.2 ; philips medical system , best , the netherlands )  . 
global function , with end - diastolic ( edv ) and end - systolic volume ( esv ) and ejection fraction were quantified on short - axis images using the simpson rule , manually defining stolic and end - systolic borders on each tomographic slice . de quantification was performed for each segment related to the occluded vessel with a quantitative approach with a semiquantitative method , as previously validated [ 23 , 24 ]  . 
this semiquantitative analysis was based on manual contour tracing ( endocardial and epicardial borders of left ventricle ) and two regions of interest ( rois ) were manually set : one in the centre of infarction and the other in the centre of normal myocardium with normal kinesis . 
from this follows the automatic threshold delineation and valutazione dei dati lanalisi delle immagini stata effettuata su una workstation off - line ( viewforum release 4.2 ; philips medicai system , best , olanda )  . 
la funzione globale con i volumi telediastolico , telesistolico e con la frazione di eiezione sono stati quantificati sulle immagini asse corto utilizzando la regola di simpson , definendo manualmente i contorni in fase telediastolica e telesistolica su ogni fetta acquisita . la quantificazione del de stata effettuata per ogni segmento correlato al vaso cronicamente occluso con un approccio quantitativo con approccio semiquantitativo , come precedentemente validato [ 23 , 24 ]  . 
lanalisi semiquantitativa stata basata sulla delineazione manuale dei contorni endocardici ed epicardici del ventricolo sinistro e successivamente sono state posizionate due regioni di interesse ( roi ) : una nel centro del miocardio infartuato e una nel centro di miocardio sano normocinetico . 
da ci , segue la delineazione automatica del tessuto infartuato sulla base di un valore di intensit di segnale soglia derivante dalla media delle intensit del tessuto infartuato e normale . 
come riportato in letteratura se il miocardio sotteso ad una coronaria cronicamente occlusa presentava un enhancement transmurale il paziente non stato incluso nella popolazione di studio da rivascolarizzare , data la scarsa possibilit di presenza di miocardio vitale nel segmento sotteso a tale vaso . ogni esame di rm per lo studio di vitalit ( esame a riposo , sotto stress dobutaminico e post - rivascolarizzazione ) stato visionato in modalit cine per una valutazione visuale della cinesi . 
inoltre nel territorio di interesse stata calcolata la riserva contrattile espressa come lispessimento indotto dalla dobutamina ed stato calcolato sottraendo allispessimento sistolico medio indotto dallo stress dobutaminico , lispessimento sistolico medio a riposo . 
inoltre , considerando sia il de che swt , stato calcolato quanto del tessuto contribuente radiol med ( 2009 ) 114 : 692704 quantification of scar tissue , given the media of signal intensity between infarcted and normal myocardiuaccording to the literature , if the occluded coronary - related tissue presented a transmural de , the patient was not considered for revascularisation , as the possibility of having viable tissue in that segment was very scarce . 
 for viability evaluation , each mri study ( rest , during dobutamine infusion and after revascularisation ) was previewed in a cine mode to visually analyse the kinesis . considering normal coronary artery distribution territories , viability parameters were measured in the myocardial territory related to the occluded coronary . 
systolic wall thickening ( swt ) of the segments to be studied was evaluated at rest before and after revascularisation and calculated by subtracting mean dwt from mean systolic thickness . 
additionally , in the territory of interest , contractile reserve was expressed as dobutamine - induced swt and was calculated by subtracting from the mean dobutamine - induced swt the mean swt at rest . 
moreover , considering both de and swt , we calculated how much of the tissue contributing to stress wall thickening corresponded to potentially viable tissue , defined by the viability index [ ( vi ) = [ swt ( 100de ) ] / 100 ]  . 
the infarct region was defined viable , as proposed in the literature , if 50% of segments fulfilled the morphological and functional mri viability criteria [ 25 ]  . functional recovery of the infarct region after successful revascularisation was defined at follow - up mri as a rest swt 2 mm in the previous dysfunctional segments related to the occluded vessel . stenting technique all conventional angiograms before revascularisation were evaluated by two independent observers . 
all patients received a bolus of unfractionated heparin ( 70 iu / kg ) before angioplasty to obtain a timi flow of 3 and a residual stenosis of the artery [ infarct - related artery ( ira ) ] < 30% . 
after the procedure , patients were treated with aspirin and clopidogrel for 12 months and then with aspirin alone . allispessimento sotto stress corrisponde a tessuto potenzialmente vitale , definito da un indice di vitalit ( ( vi ) = [ swt ( 100de ) ] / 100 )  . 
la regione infartuata stata definita vitale , come proposto in letteratura , se 50% dei segmenti sottesi al vaso cronicamente occluso soddisfacevano i criteri rm morfologici e funzionali di vitalit [ 25 ]  . la ripresa funzionale della regione infartuata post - rivascolarizzazione stata definita alla rm di follow - up come lispessimento sistolico a riposo 2 mm nei segmenti precedentemente disfunzionali sottesi al vaso cronicamente occluso . tecnica di stenting tutti gli angiogrammi pre - rivascolarizzazione sono stati valutati da due osservatori indipendenti . 
a tutti i pazienti stata somministrata una dose eparina nonfrazionata ( 70 iu / kg ) prima dellangioplastica , per ottenere un timi flow di 3 ed una stenosi residua dellarteria ( infarct related artery , ira ) < 30% . 
dopo la procedura i pazienti sono stati trattati con aspirina e clopridogel per 12 mesi e successivamente solo con aspirina . analisi statistica i risultati sono stati espressi come valore mediodeviazione standard . 
dwt , swt , de e vi sono stati paragonati alla ripresa funzionale post - rivascolarizzazione ; lanalisi statistica stata effettuata con un modello di regressione lineare ( stata software 2006 )  . 
se un parametro funzionale variato significativamente stato comparato ai parametri rm di vitalit descritti in precedenza ( correlazione di pearson )  . risultati il cto era la coronaria destra in 13 casi , la discendente anteriore in 6 e la circonflessa in 4 . 
in tre casi ( due con malattia della coronaria destra e uno della discendente anteriore ) le immagini acquisite durante stress dobutaminico non sono state di 698 statistical analysis results are expressed as mean valuesstandard deviation ( sd )  . 
if a functional parameter varied significantly , it was related to the ld - mri viability parameters described above ( pearson correlation )  . results cto was located in the right coronary artery in 13 patients , the left descending artery in six and the circumflex artery in four . 
in three cases ( two right coronary arteries and one left descending artery ) stress - induced mri images were not suitable for diagnosis , so they were excluded from the final statistical analysis . 
four patients did not fulfil the defined criteria for myocardial viability ( one right coronary , one left and two circumflex artery ) and were therefore excluded from the revascularisation procedure . mean mri time was 4512 min . revascularisation of the occluded vessel was performed within 2 weeks ( 95 days ) after ld - mri ; revascularisation was successful in 14 / 16 cases , as in two cases the invasive procedure was complicated , with perforation and dissection of the right coronary ostium due to the highly calcified vessel . 
the overall mean procedure time was approximately 12161 min . follow - up rest , cine and de - mri were performed in the remaining 14 patients 6 months after the invasive procedure . 
mean mri time was 309 m at follow - up coronary angiography , all the treated vessels were found to be patent . regarding baseline mri , we evaluated 20 patients ( 110 segments related to the occluded vessel )  . 
purtroppo 4 pazienti non hanno soddisfatto i criteri rm richiesti per lidentificazione di vitalit e sono stati esclusi dalla procedura di rivascolarizzazione ( uno con malattia della coronaria destra , uno della discendente anteriore e due della arteria circonflessa )  . 
la durata media della rm stata di 4512 minuti . la rivascolarizzazione del vaso cronicamente occluso stata effettuata entro due settimane ( 95 giorni ) dallesame rm ; la procedura stata efficace in 14 / 16 casi , in quanto in due casi stata complicata da perforazione e dissezione dellostio del vaso a causa di severe calcificazioni ( arteria coronaria destra )  . 
il tempo medio della procedura percutanea stato circa di 12161 minuti . la rm di follow - up eseguita a riposo e con studio del de stata effettuata in 14 pazienti a 6 mesi dalla procedura di riperfusione . 
alla coronarografia di follow - up stata confermata la perviet di tutti i vasi trattati . per quanto concerne lesame rm di base sono stati valutati 20 pazienti ( 110 segmenti sottesi al vaso cronicamente occluso )  . 
per quanto concerne i 16 pazienti considerati per la rivascolarizzazione i valori medi di dwt , swt e vi presentati erano di 8 , 032 , 35 , 2 , 641 , 56 e 1 , 771 , 48 ; il valore medio di de era 41 , 9730 , 32 . 
si riscontrato una correlazione diretta statisticamente significativa tra il recupero funzionale e swt ( coefficiente 1 , 779 ; p = 0 , 015 ) e vi ( coefficiente 2 , 032 ; p = 0 , 011 )  . 
la valutazione statistica riassunta nella tabella 2 . considerando i parametri funzionali dei 14 pazienti che sono stati sottoposti a rivascolarizzazione , al follow - up si evidenziato un miglioramento significativo unicamente della frazione di eiezione del ventricolo di sinistra [ delta 95% ci 4 , 47 ( da 8 , 128 a 0 , 815 , p = 0 , 0203 ) ]  . 
follow - up rest mri shows the improvement of kinesis at the same level ( g , h ) , with no change in infarct extension ( i )  . 
revascularisation was performed , but wall motion did not improve ( c ) , and delayed enhanced images ( e , f ) show increase in infarction distribution that involves a papillary muscle . 
la rm a riposo mostra ipocinesia della parete infero - laterale del ventricolo sinistro ( a ) che migliora dopo somministrazione di dobutamina a bassa dose ( b )  . 
 stata effettuata una rivascolarizzazione del vaso occluso ma la cinesi non migliorata alla rm di follow - up a riposo ( c ) e lestensione dellinfarto appare aumentata per coinvolgimento di un muscolo papillare ( e , f )  . 
one widely accepted criterion that suggests viability in chronic infarction is considered an end - diastolic thickness > 5.5 mm , predicting vitality of the vessel - related territory with a sensitivity and specificity of 92% and 52% , respectively [ 9 , 29 ]  . in addition , de imaging has become a very accurate marker of infarct identification , with almost perfect correlation with [ 28 ]  . 
un criterio largamente accettato , ma non pi considerato sufficiente , che suggerisce la persistenza di miocardio vitale in un territorio cronicamente infartuato la presenza di spessore telediastolico > 5 , 5 mm , che ha una sensibilit e specificit rispettivamente di 92% e 52% , nel predire la vitalit del territorio relazionato ad un vaso cronicamente occluso [ 9 , 29 ]  . 
la rm mediante lo studio del delayed enhancement identifica con correlazione pressoch perfetta rispetto alla tomografia ad emissione di positroni la presenza di tessuto necrotico sia di classificarne la transmuralit [ 30 ]  . 
questo dato ritenuto essere inversamente correlato alla ripresa funzionale post - riperfusione : se linfarto si estende al 75% dello spessore di parete la ripresa funzionale avviene nel 7% dei casi , mentre se interessa il 702 radiol med ( 2009 ) 114 : 692704 positron emission tomography , thanks to the possibility of recognising the presence of necrotic tissue and classifying its transmurality [ 30 ]  . 
if infarction corresponds to 75% of wall thickness , functional recovery occurs in 7% of cases , whereas if infarction only corresponds to 25% , recovery occurs in 82% of cases [ 31 , 32 ]  . 
one functional approach to identifying hibernating myocardium is cardiac dobutamine imaging , as the response to dobutamine stress is related to the coexistence of both viable and necrotic tissue in an infarcted area and can therefore be considered superior to the sole quantification of scar tissue with de imaging [ 21 ]  . 
the clinical and prognostic importance of ld - mri has not been clearly defined , as previous studies demonstrated sensitivity and specificity of 89% and 94% , respectively , which dropped to 50% and 81% when patients with ejection fraction < 35% and multiple kinesis alterations were considered [ 25 , 33 ]  . the detection of viable tissue is important for selecting patients whose left ventricular function might benefit from revascularisation , due to the presence of potentially salvageable myocardium . in our study , we tested a comprehensive cardiac ldmri approach preinterventionally in order to identify hibernating myocardium , as under drug stress , contractility improves in dysfunctional but viable myocardium , and gadolinium storage in necrotic tissue permits evaluation of the extent of damaged tissue . 
moreover , the introduced index defined as vi , combining the two different parameters necessary for viability evaluation , is even more closely related to functional recovery than de or swt taken alone , as its coefficient and p value are more powerful than those of de and swt alone . 
 our study reflects previous findings regarding de and swt but also adds the new possibility of discriminating between patients with the same de score according to the amount of viable tissue contributing to systolic stress thickening . 
the viability index proposed can be used as a more to predict post - revascularisation accurate parameter contractile recovery , describing the healthy tissue that contributes to stress thickening in cto subtended area . this is a small step forward in the treatment of cto in patients who might benefit from the revascularisation procedure . 
a large amount of data suggests that drugeluting stents offer better long - term patency rates and freedom from restenosis and repeated revascularisation than bare - metal stents in patients with cto [ 34 , 38 ] , and in our study , all patients received drug - eluting stents . furthermore , left ventricular function is around 4% and can be considered increase observed in global the 25% dello spessore di parete , la ripresa avviene nell82% dei casi [ 31 , 32 ]  . 
un approccio funzionale allidentificazione di miocardio ibernato con limaging cardiaco con stress dobutaminico si correla alla coesistenza di miocardio vitale e necrotico allinterno di una stessa area infartuata e tale approccio pu essere considerato superiore alla sola quantificazione del tessuto cicatriziale allimaging rm di delayed enhancement [ 21 ]  . 
limportanza clinica e prognostica della rm con stress dobutaminico non stata ancora definita chiaramente anche se studi preliminari mostrano una sensibilit e specificit del 89% e 94% rispettivamente , che si abbassano per al 50% e 81% in pazienti con frazione di eiezione < 35% e / o multiple alterazioni della cinesi [ 25 , 33 ]  . 
la detection di tessuto vitale importante per selezionare pazienti in cui la frazione di eiezione potrebbe trarre beneficio da una procedura di rivascolarizzazione , in base alla presenza di miocardio potenzialmente vitale . 
 nello studio qui descritto , abbiamo testato un approccio rm comprensivo prima della procedura di rivascolarizzazione per identificare miocardio ibernato , dato che sotto stress dobutaminico a bassa dose la contrattilit migliora in caso di miocardio disfunzionale ma vitale e laccumulo di gadolinio nel tessuto necrotico permette di valutare lestensione del danno tissutale . 
inoltre lindice di vitalit introdotto , definito come vi , ottenuto da una combinazione tra i due differenti parametri necessari per lidentificazione di vitalit , ancora pi correlato al recupero funzionale rispetto al de e swt considerati singolarmente , dato che il suo coefficiente ed il suo valore p hanno una potenza statistica maggiore . 
 il nostro studio riflette quanto attualmente riportato in letteratura riguardo de ed swt ma inoltre aggiunge la possibilit di discriminare in pazienti con la medesima estensione necrotica ( simile estensione di de ) la quantit di tessuto vitale residuo . 
lindice di vitalit proposto pu essere utilizzato come parametro pi accurato per predire il recupero funzionale post - rivascolarizzazione , descrivendo il tessuto vitale che contribuisce allispessimento sotto stress in unarea sottesa ad un vaso cronicamente occluso . questo pu essere considerato un piccolo passo in avanti nel trattamento delle cto in pazienti che potrebbero beneficiare dalla procedura di rivascolarizzazione . 
molti dati attuali suggeriscono che gli stent medicati offrano percentuali maggiori di perviet a lungo termine , assenza di restenosi e , quindi , di procedure di ri - vascolarizzazione rispetto agli stent metallici in pazienti con cto [ 3438 ] e nella casistica qui riportata tutti i pazienti hanno ricevuto stent medicati . 
inoltre , il globale aumento osservato nella frazione di eiezione del ventricolo di sinistra di circa il 4% e pu essere considerato significativo anche nel follow - up a breve termine ( 6 mesi ) come riportato da un recente lavoro radiol med ( 2009 ) 114 : 692704 significant even in this short - term follow - up , as reported in a recent study where the trend in left ventricular function improvement was evaluated both in shortand long - term follow - up [ 19 ]  . 
as demonstrated , restoring blood flow to dysfunctional but viable myocardium led to a functional benefit for patients , shown by a decrease in mean esv with substantial identity of edv that caused increase in lvef . moreover the low rate of complications during intervention ( two cases out of 16 ; 12.5% ) is in line with the current literature [ 11 ] and should not prevent patients with potentially viable myocardium from being revascularised percutaneously . 
the definition of cto was more than 3 months in this study , whereas previous studies defined cto as 7 days to 3 months of occlusion time [ 38 ]  . 
 another limit is the use of a viability index that was not previously validated in the literature ; however , we decided to employ it because it enhances the contribution of viable tissue to dobutamine response in the cto vessel - related segments . 
low - dose dobutamine infusion was not preformed at follow - up mri but might provide further insight into the mechanisms underlying recovery of function of viable myocardium . dove il trend di crescita della frazione di eiezione stato valutato sia a breve che a lungo termine [ 19 ]  . 
ripristinare il flusso sanguigno in un territorio miocardico disfunzionale ma vitale migliora la funzione cardiaca dei pazienti , come dimostrato da una diminuzione del volume telesistolico con una sostanziale identit del volume telediastolico ( assenza di rimodellamento ) che porta ad un incremento della frazione di eiezione . 
inoltre la bassa frequenza di complicanze peri - procedurali ( 2 casi su 16 ; 12 , 5% ) in linea con la letteratura [ 11 ] e non dovrebbe precludere a pazienti con miocardio potenzialmente vitale di essere riperfusi in modo percutaneo . 
inoltre la definizione di cto nel nostro lavoro stata identificata come occlusione maggiore di tre mesi , mentre in altri studi stata considerate da sette giorni a tre mesi [ 38 ]  . 
 un ulteriore limite dello studio lutilizzo di un indice di vitalit non precedentemente validato in letteratura , tuttavia si voluto sottolineare il contributo del miocardio vitale allo stress dobutaminico nel territorio sotteso ad un vaso cronicamente occluso . 
lesame rm di follow - up stato condotto senza linfusione di dobutamina , anche se ci potrebbe essere utile nellidentificare meccanismi sottesi al recupero funzionale del miocardio vitale in pazienti con cto . 
twenty - seven patients with bowel infarction due to vascular obstruction were evaluated with multidetector ct ( mdct ) to establish the prognostic value of ct findings and their correlation with the origin of the ischaemia . 
bowel - wall hyperdensity ( 2 / 9 venous occlusions ) , loss of wall enhancement ( 1 / 9 venous occlusions , 2 / 18 arterial occlusions ) and wall thickening ( 8 / 9 venous obstructions , 2 / 18 arterial occlusions ) were predictive of good outcome . 
sono state valutate le immagini tc multidetettore ( tcmd ) di 27 pazienti con infarto intestinale da occlusione vascolare e sono state ricercate : significativit prognostica delle alterazioni evidenziate , correlazioni con la natura dellischemia . 
leziologia della patologia in rapporto alla prognosi risultata altamente significativa , con mortalit del 89% nelle forme arteriose e del 11% in quelle venose . liperdensit parietale ( 2 / 9 occlusioni venose ) , lassenza di enhancement ( 1 / 9 occlusioni venose , 2 / 18 occlusioni arteriose ) , lispessimento di parete ( 8 / 9 occlusioni venose , 2 / 18 occlusioni arteriose ) sono risultati significativi di evoluzione benigna , mentre la dilatazione delle anse ( 4 / 9 occlusioni venose , 13 / 18 occlusioni arteriose ) , la pneumatosi parietale ( 1 / 9 occlusioni venose , 17 / 18 occlusioni arteriose ) , laria nelle vene mesenteriche ( 2 / 9 occlusioni venose , 11 / 18 occlusioni arteriose ) , laria nei rami portali ( 1 / 9 occlusioni venose , 4 / 18 occlusioni arteriose ) , lo pneumoperitoneo ( 8 / 18 occlusioni arteriose ) e il retropneumoperitoneo ( 1 / 18 occlusioni arteriose ) sono risultati indici prognostici sfavorevoli . 
the longer life expectancy of the general population and the resulting degenerative vascular diseases have led to a steady increase in the incidence of this disease . bowel infarction is typically classified as occlusive or nonocclusive on the basis of aetiology . 
in the occlusive forms , the abnormality may involve the arterial or venous vessels ( coeliac trunk branches , superior mesenteric artery , inferior mesenteric artery and corresponding venous vessels )  . 
the nonocclusive forms are less frequent and generally caused by a rapid fall in systemic pressure or by hypovolaemia due to haemorrhagic , cardiogenic or septic shock . multidetector computed tomography ( mdct ) thanks to increased spatial resolution , high - quality multiplanar reconstructions ( mpr ) , maximum intensity projections ( mip ) , three - dimensional rendering and shorter acquisition times is now able to allow visualisation of early signs of bowel ischaemia and infarction and has become the gold standard for diagnosis [ 36 ]  . 
mdct also allows for aetiological diagnosis of the infarction which is fundamental in planning treatment in acute patients and has replaced angiography as a diagnostic study because despite having a sensitivity of 87% [ 7 ] , angiography is now exclusively reserved for therapeutic procedures . despite of our better knowledge and improved diagnostic techniques , bowel infarction is still frequently a fatal disease , with reported mortality rates between 50% and 90% [ 13 , 8 ] , depending in part on aetiology [ 9 ]  . 
 the aim of this study was to identify possible correlations between ct findings and outcomes of patients affected by occlusive bowel infarction . materials and methods we retrospectively reviewed 27 patients with bowel infarction who were examined at our department between october 2005 and january 2008 . 
patients were identified through a search of our electronic archive system using terms such as ischaemia , infarction and intestinal necrosis . thus , we obtained a list of 40 patients , 13 of whom were excluded : six , because they had circumscribed ischaemia linfarto intestinale rappresenta una causa non abituale , ma spesso sottostimata , di addome acuto non traumatico ed determinato da unalterazione dellapporto ematico alla regione mesenterica , che pu causare una necrosi della parete intestinale [ 1 , 2 ]  . 
lincremento della vita media della popolazione generale e le conseguenti patologie degenerative vascolari hanno favorito un costante aumento dellincidenza di questa patologia . linfarto intestinale viene classicamente suddiviso in occlusivo e non occlusivo in base alla differente eziologia . nelle forme occlusive , lalterazione pu interessare i vasi arteriosi o venosi ( rami di divisione del tronco celiaco , arteria mesenterica superiore , arteria mesenterica inferiore e vasi venosi corrispondenti )  . 
le forme non occlusive , meno frequenti , sono generalmente causate da un rapido decremento della pressione sistemica o dallipovolemia in rapporto a shock emorragico , cardiogeno o settico . la tomografia computerizzata multidetettore ( tcmd ) , grazie allincremento della risoluzione spaziale , allalta qualit delle ricostruzioni multiplanari mpr , mip e 3d e ai ridotti tempi di esecuzione , in grado di rilevare i segni precoci dellischemia e dellinfarto intestinale e rappresenta attualmente il gold standard per il riconoscimento di questa patologia [ 36 ]  . 
inoltre essa consente una diagnosi di tipo eziologico dellinfarto , fondamentale ai fini della pianificazione terapeutica per il paziente acuto ed ha ormai sostituito in fase diagnostica langiografia , che , pur presentando una sensibilit del 87% [ 7 ] , attualmente ha un ruolo quasi esclusivamente terapeutico . 
 nonostante lincremento delle conoscenze riguardo questa condizione clinica ed il miglioramento delle tecniche diagnostiche , linfarto intestinale risulta ancora spesso letale , con un tasso di mortalit descritto in letteratura compreso tra il 50% ed il 90% [ 13 , 8 ] , variabile anche in rapporto alla sua eziologia [ 9 ]  . 
i pazienti sono stati identificati 782 radiol med ( 2009 ) 114 : 780791 secondary to strangulation and the remaining seven because they underwent unenhanced ct only due to poor general condition . all 27 selected cases were affected by occlusive ischaemia : 18 ( 67% ) of the arterial and nine ( 33% ) of the venous type . 
only 15 patients ( 56% ) underwent surgery ; of these , nine ( 60% ) died and six ( 40% ) survived . the definite diagnosis was provided by surgery , with histology of the resected intestinal segment in 15 patients and by autopsy in five cases . 
postprocessing time was approximately 15 mct images were assessed for the following parameters : wall enhancement , considered pathological when inhomogeneous , marked and persistent , or absent wall thickness , considered normal when less than 5 mm , with distended bowel loops ; in the absence of distension , the wall was considered pathological when its thickness was greater than approximately 1 cm bowel - loop dilatation , defined as a small - bowel diameter > 2.5 cm and large - bowel diameter > 8 cm parietal pneumatosis , defined as the presence of small air bubbles within the bowel wall , irrespective of extent presence of gas within the mesenteric venules and portal venous system pneumoperitoneum / pneumoretroperitoneum ascites . finally , to define the arterial or venous nature of the vascular occlusion causing ischaemia , we evaluated the morphology and patency of the coeliac trunk , superior and inferior mesenteric arteries , superior mesenteric vein and portal trunk . ricercando nel nostro archivio computerizzato alcune parole chiave come ischemia , infarto , necrosi intestinale . 
stata in tal modo ottenuta una lista di 40 pazienti , da cui ne sono stati esclusi 13 , 6 con ischemia circoscritta secondaria a strangolamento ed i restanti 7 poich , per le precarie condizioni cliniche , erano stati valutati esclusivamente con scansioni eseguite senza iniezione di mezzo di contrasto endovenoso . 
il gruppo di pazienti considerato includeva 14 soggetti di sesso maschile ( 52% ) e 13 di sesso femminile ( 48% ) , con un intervallo di et compreso tra 42 e 92 anni ( et media 68 , 3 ; errore standard 5 , 3 )  . 
inoltre , soltanto 15 ( 56% ) sono stati trattati chirurgicamente e di questi 9 ( 60% ) sono deceduti e 6 ( 40% ) sono sopravvissuti . la diagnosi definitiva si basata sul controllo chirurgico con istologia del segmento intestinale asportato in 15 pazienti e sul controllo autoptico in 5 casi . 
 le apparecchiature utilizzate sono state : tcmd a 16 strati ( tsx - 101aaquilion 16 , toshiba medical system , tokio , giappone ) , tcmd a 4 strati ( mx 8000 , philips medical systems , royal philips electronic , best , olanda )  . in tutti i casi sono state eseguite scansioni prima e dopo iniezione endovenosa di mezzo di contrasto ( 120140 ml iniettati alla velocit di 33 , 5 ml / s ) , con acquisizione delle immagini in fase arteriolare , generalmente con un ritardo compreso tra 30 e 40 s dallinizio della somministrazione del mezzo di contrasto ed in fase venosa , con un ritardo compreso tra 60 e 90 s dallinizio della somministrazione del mezzo di contrasto . 
nel valutare le immagini tc sono stati considerati i seguenti parametri : enhancement parietale , considerato patologico quando disomogeneo , marcato e persistente , o assente ; spessore parietale , considerato normale quando inferiore a 5 mm , con anse distese ; in assenza di distensione , la parete stata considerata patologica in presenza di uno spessore superiore ad 1 cm circa ; dilatazione delle anse intestinali , diagnosticata in presenza di un diametro del tenue superiore a 2 , 5 cm e del colon superiore ad 8 cm ; radiol med ( 2009 ) 114 : 780791 statistical analysis the sample population was initially analysed using descriptive statistics and considering age , gender , aetiology of ischaemia ( arterial or venous ) , disease course ( dead or living patient ) and calculating mortality rates . 
we then examined the ability of ct to define the type of bowel ischaemia , and related the different densitometric alterations to the nature of the vascular occlusion and disease stage to determine the prognostic significance of the ct findings . 
the data obtained were considered to be statistically significant at a p value 0.05. results as shown in table 1 , disease aetiology in relation to outcome proved to be highly significant ( p = 0.0000001 ) , with 89% mortality for arterial infarctions ( 16 / 18 ) and 11% mortality for venous obstructions ( 1 / 9 )  . 
all cases of arterial obstruction regarded the main trunk of the superior mesenteric artery , which was associated with atheromatous wall alterations of the coeliac trunk in five cases and alterations of the inferior mesenteric artery in four . 
all venous obstructions involved the superior mesenteric vein , with associated involvement of the portal vein in four cases . analysis of the ct findings seen in the two types of vascular occlusion is shown in table 2 . 
wall hyperdensity was seen in 2 / 9 ( 23% ) venous occlusions and in none of the table 1 correlation between aetiology and outcome in bowel infarction pneumatosi parietale , diagnosticata in presenza di piccole bolle aeree nel contesto della parete , indipendentemente dalla entit ; presenza di aria nelle venule mesenteriche e nel sistema venoso portale ; pneumo - / retropneumoperitoneo ; ascite . 
 per definire , infine , la natura arteriosa o venosa dellocclusione vascolare responsabile dellischemia intestinale , sono state valutate la morfologia e la perviet del tronco celiaco , delle arterie mesenteriche superiore ed inferiore , della vena mesenterica superiore e del tronco portale . 
 analisi statistica lanalisi del nostro campione stata eseguita dapprima mediante statistica descrittiva , esaminando et , sesso , eziologia dellischemia ( arteriosa o venosa ) , evoluzione della patologia ( paziente deceduto o vivente ) e calcolando i valori percentuali di mortalit . 
successivamente , il campione stato suddiviso in gruppi al fine di confrontare leziologia della patologia ( gruppo degli infarti arteriosi versus quelli venosi ) , rispetto ai risultati terapeutici ( gruppo dei pazienti deceduti versus quelli viventi ) ed stata verificata la significativit statistica di tale dato , applicando il test del 2 e calcolando il valore di p . 
sono state , quindi , valutate le potenzialit della tc nel definire la natura dellischemia intestinale e le differenti alterazioni tomodensitometriche riconoscibili sono state correlate alla natura dellocclusione vascolare ed alla evoluzione della patologia , per determinare la loro significativit prognostica . 
i dati sono stati considerati statisticamente significativi per valori di p0 , 05 . risultati come riportato nella tabella 1 , leziologia della malattia , in rapporto alla prognosi , si rivelata altamente significaarterial infarctions ( n = 18 ) venous infarctions ( n = 9 ) chi - square test p value dead patients living patients dead patients living patients 16 ( 88% ) 2 ( 12% ) 1 ( 11% ) 8 ( 89% ) 0.0000001 tabella 1 correlazione tra eziologia e prognosi nellinfarto intestinale infarti arteriosi ( n = 18 ) infarti venosi ( n = 9 ) pazienti deceduti pazienti viventi pazienti deceduti pazienti viventi 16 ( 88% ) 2 ( 12% ) 1 ( 11% ) 8 ( 89% ) 119 valore p 0 , 0000001 784 radiol med ( 2009 ) 114 : 780791 fig . 
absence of wall enhancement was evident in 1 / 9 ( 12% ) venous occlusions and in 2 / 18 ( 12% ) arterial occlusions , and hence the incidence of this finding was very similar in the two forms . 
wall thickening was the most frequent abnormality in infarctions caused by venous occlusions , in which cases of thickening were marked and always > 15 mm . dilated bowel loops were present in 4 / 9 ( 45% ) venous occlusions and in 13 / 18 ( 73% ) arterial occlusions . 
lostruzione arteriosa interessava in tutti i casi il tronco principale dellarteria mesenterica superiore e si associavano alterazioni ateromasiche parietali a carico del tronco celiaco in 5 casi e dellarteria mesenterica inferiore in 4 . 
the presence of gas within the mesenteric venules was detected in 2 / 9 ( 23% ) venous occlusions and in 11 / 18 ( 62% ) arterial occlusions , with a clear prevalence in the arterial forms . 
likewise , the presence of gas within the portal branches was seen in 1 / 9 ( 12% ) venous occlusions and in 4 / 18 ( 23% ) arterial occlusions . 
in no case of venous occlusion was the presence of pneumoperitoneum / pneumoretroperitoneum detected , signs that were instead seen in 8 / 18 ( 45% ) and 1 / 18 ( 5% ) arterial occlusions , respectively . 
ascites was present in 6 / 9 ( 67% ) venous occlusions and in 12 / 18 ( 67% ) arterial occlusions , with a virtually identical incidence in the two forms . analysis of the ct findings in relation to disease course lanalisi delle alterazioni tc riscontrate in relazione alla natura dellocclusione vascolare riportata nella tabella 2 . 
uniperdensit parietale stata riscontrata in 2 / 9 ( 23% ) occlusioni venose , mai in quelle arteriose . lassenza di enhancement parietale risultata evidente in 1 / 9 ( 12% ) occlusioni venose ed in 2 / 18 ( 12% ) occlusioni arteriose , pertanto ha presentato unincidenza sovrapponibile nelle due forme . 
lispessimento parietale ha rappresentato lalterazione pi frequente negli infarti da occlusioni venose ed in tali casi , inoltre , lincremento dello spessore parietale risultato marcato e sempre superiore a 15 mla dilatazione delle anse intestinali stata riscontrata in 4 / 9 ( 45% ) occlusioni venose ed in 13 / 18 ( 73% ) occlusioni arteriose . 
la pneumatosi parietale stata riconosciuta 786 radiol med ( 2009 ) 114 : 780791 table 2 correlation between ct findings and type of vascular obstruction arterial infarctions ( n = 18 ) venous infarctions ( n = 9 ) tabella 2 alterazioni tc riscontrate in rapporto alla natura dellocclusione vascolare intramural hyperdensity loss of enhancement wall thickening loop dilation intramural pneumatosis mesenteric venous gas portal venous gas pneumoperitoneum pneumoretroperitoneum ascites 2 ( 12% ) 2 ( 12% ) 13 ( 73% ) 17 ( 95% ) 11 ( 62% ) 4 ( 23% ) 8 ( 45% ) 1 ( 5% ) 12 ( 67% ) infarti arteriosi ( n = 18 ) iperdensit parietale 2 ( 12% ) assenza di enhancement 2 ( 12% ) ispessimento parietale 13 ( 73% ) dilatazione anse pneumatosi 17 ( 95% ) aria nelle venule mesenteriche 11 ( 62% ) aria nella vena porta pneumoperitoneo retropneumoperitoneo ascite 4 ( 23% ) 8 ( 45% ) 1 ( 5% ) 12 ( 67% ) 2 ( 23% ) 1 ( 12% ) 8 ( 88% ) 4 ( 45% ) 1 ( 12% ) 2 ( 23% ) 1 ( 12% ) 6 ( 67% ) infarti venosi ( n = 9 ) 2 ( 23% ) 1 ( 12% ) 8 ( 88% ) 4 ( 45% ) 1 ( 12% ) 2 ( 23% ) 1 ( 12% ) 6 ( 67% ) is shown in table 3 . 
wall thickening was the most frequent alteration in surviving patients , with 9 / 10 ( 90% ) cases among survivors against 1 / 17 ( 6% ) among deceased patients . 
in 3 / 10 ( 30% ) surviving patients and 10 / 17 ( 59% ) deceased patients , gas was detected in the mesenteric venules , whereas in 1 / 10 ( 10% ) surviving patients and 4 / 17 ( 24% ) deceased patients , the presence of air was seen in the portal branches . 
none of the surviving patients showed pneumoperitoneum or pneumoretroperitoneum , which were instead present in 8 / 17 ( 47% ) and 1 / 17 ( 5% ) deceased patients , respectively . in 1 / 9 ( 12% ) occlusioni venose ed in 17 / 18 ( 95% ) occlusioni arteriose . 
la presenza di aria nelle venule mesenteriche stata riscontrata in 2 / 9 ( 23% ) occlusioni venose ed in 11 / 18 ( 62% ) occlusioni arteriose , con una evidente prevalenza nelle forme arteriose , come anche la presenza di aria nei rami portali , riconosciuta in 1 / 9 ( 12% ) occlusioni venose ed in 4 / 18 ( 23% ) occlusioni arteriose . 
in nessun caso di occlusione venosa stata rilevata la presenza di pneumoperitoneo o retropneumoperitoneo ; tali segni erano , invece , evidenti rispettivamente in 8 / 18 ( 45% ) e 1 / 18 ( 5% ) occlusioni arteriose . 
in 6 / 9 ( 67% ) occlusioni venose ed in 12 / 18 ( 67% ) occlusioni arteriose era presente ascite , che pertanto ha presentato una incidenza sovrapponibile nelle due forme . lanalisi delle alterazioni tc riscontrate in relazione allevoluzione della patologia riportata nella tabella 3 . uniperdensit parietale stata riscontrata in 2 / 10 ( 20% ) pazienti sopravvissuti , mai in pazienti deceduti . 
lispessimento parietale ha rappresentato lalterazione pi frequente nei pazienti sopravvissuti , con il riscontro di 9 / 10 ( 90% ) casi nel gruppo dei pazienti sopravvissuti e 1 / 17 ( 6% ) in quelli deceduti . 
la pneumatosi parietale stata riscontrata in 2 / 10 ( 20% ) pazienti sopravvissuti e 16 / 17 ( 95% ) pazienti deceduti ; lincidenza di tale alterazione ha mostrato , quindi , una netta prevalenza nel gruppo dei pazienti deceduti . 
in 3 / 10 ( 30% ) pazienti sopravvissuti e 10 / 17 ( 59% ) pazienti deceduti era evidente aria nelle venule mesenteriche , mentre in 1 / 10 ( 10% ) pazienti sopravvissuti e 4 / 17 ( 24% ) pazienti deceduti stata riscontrata la presenza di aria nei rami portali . 
in nessun paziente sopravvissuto stato rilevato pneumoperitoneo o retropneumoperitoneo , che al contrario erano evidenti rispettivamente in 8 / 17 ( 47% ) e 1 / 17 ( 5% ) pazienti deceduti . 
in 6 / 10 ( 60% ) pazienti sopravvissuti ed in 12 / 17 ( 71% ) pazienti deceduti era evidente , infine , ascite . la valutazione del valore prognostico dei reperti tc riscontrati nel nostro campione ha dimostrato una significativit statistica per tutti i segni esaminati ( p0 , 05 ) , ad eccezione della presenza di ascite ( p = 0 , 1 )  . 
in particolare , liperdensit , lassenza di enhancement e lispessimento di parete delle anse intestinali sono risultati significativi di evoluzione benigna di malattia , mentre la dilatazione delle anse , la pneumatosi parietale e porto - mesenterica e lo pneumo / retropneumoperitoneo hanno presentato una incidenza pi elevata nei pazienti deceduti . 
the presence of ascites did not provide any prognostic information , its incidence being almost identical among survivors and deceased patients . discussion thanks to its extraordinary capabilities , mdct is the most frequently used technique in the diagnostic approach to patients with suspected intestinal ischaemia , with reported sensitivity , specificity and positive and negative predictive values of 64%93% , 92%100% , 90%100% , and 94%98% , respectively [ 13 , 10 , 11 ]  . 
nonetheless , despite continuing progress in the field of abdominal imaging , the mortality rate of bowel infarction remains presentato unincidenza sovrapponibile nel gruppo dei pazienti sopravvissuti ed in quello dei pazienti deceduti . discussione nellapproccio diagnostico del paziente con sospetta ischemia intestinale la tcmd , per le sue straordinarie potenzialit , ormai divenuta lindagine pi utilizzata e presenta valori di sensibilit , specificit , valore predittivo positivo e negativo , riportati in letteratura , rispettivamente compresi tra 64%93% , 92%100% , 90%100% , 94%98% [ 13 , 10 , 11 ]  . 
nonostante i continui progressi nel campo dellimaging addominale , comunque , il tasso di mortalit in rapporto ad infarto intestinale ancora molto alto , con valori riportati in letteratura compresi tra il 50% ed il 90% [ 1 , 3 , 6 , 8 , 12 ] , e del 63% nella nostra esperienza . a tali insoddisfacenti risultati contribuiscono differenti fattori , ma certamente i pi importanti sono : clinica del paziente , eziologia dellischemia intestinale e grado del danno anatomico al momento della diagnosi . da un punto di vista clinico gli elementi pi importanti nella valutazione prognostica sono : ipertensione arteriosa , diabete mellito , et , fumo , familiarit per cardiopatia , vasculopatia periferica e / o cerebrale , coronaropatia , sintomi di ischemia mesenterica cronica , scompenso 788 radiol med ( 2009 ) 114 : 780791 very high , with reported values of 50%90% ( 63% in our experience ) [ 1 , 3 , 6 , 8 , 12 ]  . 
this unsatisfactory result is related to different factors , among which the most important are the patients clinical history , the aetiology of the intestinal ischaemia and the degree of anatomical damage at the time of diagnosis . clinically , the most important factors in evaluating prognosis are the following : arterial hypertension , diabetes mellitus , age , smoking history , family history of heart disease , peripheral and / or cerebral vascular disease , coronary disease , symptoms of chronic mesenteric ischaemia , heart failure , renal failure , previous myocardial infarction , previous surgery , chronic obstructive pulmonary disease , hypercholesterolaemia , atrial fibrillation , time elapsed between diagnosis and treatment , duration of symptoms , surgical treatment of the acute event and levels of metabolic acidosis [ 1216 ]  . as far as aetiology is concerned , the classification of bowel infarction into nonocclusive and occlusive forms , in relation to arterial or venous obstructions , is now universally recognised in the literature [ 24 , 9 , 17 ]  . 
nonocclusive forms account for 20%30% of cases of acute mesenteric ischaemia , are associated with often adverse outcomes with mortality rates of 58%70% [ 18 , 19 ] , and occur in conditions of systemic hypoperfusion characterised by low infarction , cardiac output : heart failure , myocardial arrhythmias , aortic failure , traumatic , haemorrhagic or septic shock [ 2 , 3 , 11 , 20 ]  . 
in particular , occlusions of the mesenteric arteries are more frequent than those of the corresponding veins [ 3 , 9 , 18 , 2123 ] , as seen in our patient population in which 67% of cases were arterial occlusions against 33% venous occlusions . 
among occlusive forms , the reported mortality rates of forms caused by arterial obstruction range from 17% to 90% , whereas those of lesions secondary to venous obstruction range from 0% to 30% [ 18 , 24 , 25 ]  . 
hence , the aetiology of ischaemia is an important prognostic factor , and its definition should be a fundamental goal of diagnostic imaging . until recently , the use of conventional ct scanners in the study of bowel ischaemia allowed detection of wall alterations , but only rarely was it possible to define disease aetiology [ 26 ]  . 
nowadays , diffusion of scanners with multislice acquisition systems that provide excellent vascular studies has increasingly facilitated this evaluation , allowing both detection and aetiological definition of the disease , as seen in our series [ 4 , 11 , 2729 ]  . another fundamental parameter for ct evaluation is the type of alterations , which have a different incidence in arterial or venous vascular obstructions and express the extent of anatomical damage . 
in this regard , as previously stated cardiaco , insufficienza renale , precedente infarto miocardico , precedente intervento chirurgico , broncopatia cronica ostruttiva , ipercolesterolemia , fibrillazione atriale , intervallo di tempo intercorso tra diagnosi e terapia , durata dei sintomi , trattamento di tipo chirurgico dellevento acuto e livelli di acidosi metabolica [ 1216 ]  . per quanto riguarda leziologia , ormai universalmente riconosciuta in letteratura [ 24 , 9 , 17 ] la suddivisione dellinfarto intestinale in forme non occlusive ed occlusive , in rapporto ad ostruzioni arteriose o venose . 
le forme non occlusive rappresentano il 20%30% dei casi di ischemia mesenterica acuta , si associano ad una prognosi pi spesso sfavorevole , con tasso di mortalit compreso tra il 58% ed il 70% [ 18 , 19 ] e si verificano nelle condizioni di ipoperfusione sistemica caratterizzate da una bassa gittata cardiaca : scompenso cardiaco , infarto del miocardio , aritmie , insufficienza aortica , shock traumatico , emorragico o settico [ 2 , 3 , 11 , 20 ]  . le forme occlusive risultano molto pi frequenti di quelle non occlusive , ed in particolare le occlusioni delle arterie mesenteriche sono pi frequenti di quelle dei vasi venosi corrispondenti [ 3 , 9 , 18 , 2123 ] , come anche riscontrato nel nostro campione in cui le occlusioni arteriose incidono nel 67% dei casi , mentre quelle venose nel 33% . 
nellambito delle forme occlusive , sono stati riportati valori di mortalit nelle forme secondarie ad ostruzione arteriosa compresi tra 17% e 90% , nelle forme secondarie ad ostruzione venosa , valori compresi tra 0% e 30% [ 18 , 24 , 25 ] ; nel gruppo di pazienti da noi studiati , la mortalit stata del 89% nelle forme arteriose e soltanto del 11% in quelle venose . 
 in passato , utilizzando le apparecchiature tradizionali , nello studio dellischemia intestinale era possibile riconoscere le alterazioni parietali , ma solo raramente era possibile una definizione eziologica della patologia [ 26 ]  . 
attualmente , al contrario , la diffusione di apparecchiature dotate di sistemi di acquisizione multistrato , che consentono eccellenti studi vascolari , ha reso agevole tale valutazione , per cui possibile non soltanto il riconoscimento della patologia , ma anche la sua definizione eziologica , cos come anche nella casistica personale [ 4 , 11 , 2729 ]  . 
in fact , parietal hyperdensity , the absence of enhancement and bowel - wall thickening all indicate a favourable outcome , whereas loop dilatation , parietal and portomesenteric pneumatosis and pneumoperitoneum / pneumoretroperitoneum are all indicators of unfavourable outcome . these findings are readily explained if we consider the correlation between progression of intestinal ischaemic damage and abnormalities visible on ct [ 2 , 4 , 17 , 28 , 29 ]  . bowel - wall hyperdensity reflects vasodilation , which is the first consequence of hypoxic damage . 
the absence of wall enhancement corresponds to the ensuing vasoconstriction ; bowel - loop thickening and dilatation are related to the increased capillary permeability , pneumatosis and the presence of air within the mesentericportal system are an expression of necrosis of the intestinal mucosa , whereas pneumoperitoneum / pneumoretroperitoneum corresponds to transmural extension of the necrosis [ 3 , 4 , 3032 ]  . 
therefore , wall hyperdensity , the absence of enhancement and wall thickening represent an early stage of the disease , in contrast to loop dilation , parietal and portomesenteric pneumatosis and pneumoperitoneum / pneumoretroperitoneum , which reflect an advanced stage of disease characterised by high mortality rates . furthermore , our experience suggests that hyperdensity and bowel - wall thickening are significantly correlated to forms of venous infarction , whereas loop dilatation , parietal pneumatosis , the presence of gas within the mesenteric venules and portal branches , as well as pneumoperitoneum / pneumoretroperitoneum are characteristic of forms related to arterial occlusions . 
on the other hand , the absence of wall enhancement and the presence of ascites are nonspecific ct findings with respect to the nature of ischaemia , as their incidence is almost the same in arterial and venous obstructions . these findings may have a temporal justification in that , in arterial obstructions , the pathophysiological events leading to wall necrosis occur in rapid succession , whereas a longer time interval is required for the initial vascular damage of venous occlusions to develop into frank anatomical damage . 
infatti , liperdensit parietale , lassenza di enhancement e lispessimento delle anse indicano una prognosi pi favorevole , mentre la dilatazione delle anse , la pneumatosi parietale e porto - mesenterica e lo pneumo - / retropneumoperitoneo rappresentano indici prognostici sfavorevoli . tali risultati appaiono agevolmente giustificabili , considerando la correlazione tra la progressione del danno ischemico intestinale e le alterazioni riscontrabili allesame tc [ 2 , 4 , 17 , 28 , 29 ]  . 
liperdensit parietale intestinale riflette il meccanismo di vasodilatazione , che rappresenta la prima conseguenza del danno ipossico ; lassenza di enhancement di parete corrisponde alla successiva vasocostrizione che rapidamente si instaura ; lispessimento e la dilatazione delle anse sono dovuti allincremento della permeabilit capillare ; la pneumatosi e la presenza di aria nel sistema mesenterico - portale sono espressione della necrosi della mucosa intestinale ed infine lo pneumo - / retropneumoperitoneo corrispondono allevoluzione transmurale della necrosi [ 3 , 4 , 3032 ]  . 
pertanto , liperdensit parietale , lassenza di enhancement e lispessimento parietale rappresentano una fase precoce della patologia , al contrario la dilatazione delle anse , la pneumatosi parietale e porto - mesenterica e lo pneumo - / retropneumoperitoneo rappresentano una patologia avanzata , gravata da un alto tasso di mortalit . dalla nostra esperienza emerge , inoltre , che liperdensit e lispessimento di parete delle anse intestinali si associano con elevata significativit a forme di infarto venoso , mentre la dilatazione delle anse , la pneumatosi parietale , la presenza di aria nelle venule mesenteriche e nei rami portali e lo pneumo - / retropneumoperitoneo presentano una maggiore incidenza nelle forme secondarie ad occlusioni arteriose . 
lassenza di enhancement di parete e la presenza di ascite hanno invece rappresentato alterazioni tc aspecifiche in relazione alla natura dellischemia , poich la loro incidenza risultata sovrapponibile nelle ostruzioni arteriose ed in quelle venose . la giustificazione di tali risultati probabilmente riconducibile ad un fattore temporale , poich nelle ostruzioni arteriose gli eventi fisiopatologici , che esitano nella necrosi parietale , si susseguono rapidamente ; al contrario , nelle forme venose , occorre un maggior intervallo di tempo affinch dal danno vascolare iniziale si arrivi ad una fase pi conclamata del danno anatomico . 
pertanto la possibilit di riconoscere in corso di esami tc alterazioni parietali riconducibili ad una fase pi precoce della patologia maggiore negli infarti da occlusione venosa , piuttosto che in quelli secondari ad ostruzione arteriosa . 
 [ 3 ] with regard to wall thickening and the target appearance of intestinal loops , which represents a favourable prognostic indicator and a sign more frequently associated with venous infarction owing to a larger intramural haemorrhagic component and superinfection . 
 [ 33 ] , who reported that portomesenteric pneumatosis is indicative of advanced bowel necrosis and correlates with unfavourable outcomes , above all when associated with other ischaemic wall abnormalities . by contrast , our results conflict with those obtained in other series [ 34 , 35 ] and those reported by wiesner [ 36 ] , who states that the outcome of patients with bowel ischaemia depends on severity and extent of the initial disease and that bowel wall and portomesenteric pneumatosis have no prognostic significance , as they are not generally indicative of transmural infarction and may also be seen in partial ischaemia . i nostri risultati concordano con quanto riportato da wiesner et al . 
 [ 3 ] per quanto riguarda lispessimento parietale , con aspetto a bersaglio delle anse intestinali , che rappresenta un indice prognostico favorevole e si associa pi frequentemente ad infarto di tipo venoso , in rapporto ad una maggiore componente emorragica intraparietale e superinfezione . 
 [ 33 ] , secondo i quali la pneumatosi porto - mesenterica indicativa di necrosi intestinale avanzata con prognosi sfavorevole , soprattutto quando associata ad altre alterazioni ischemiche parietali . tuttavia , i nostri risultati si differenziano da quelli ottenuti in altre casistiche [ 34 , 35 ] e dallo stesso wiesner [ 36 ] , i quali sostengono che la prognosi dei pazienti affetti da ischemia intestinale dipende dalla gravit e dalla estensione della patologia di base e che la pneumatosi parietale intestinale e porto - mesenterica causate da ischemia generalmente non indicano un infarto transmurale e pertanto non hanno significato prognostico , in quanto tali segni possono essere osservati anche in pazienti con ischemia solo parziale . 
mdct allows for correct diagnosis , contributes to appropriate treatment planning and provides important prognostic information thanks to its ability to define the nature of the disease and the extent of anatomical damage . la tcmd fondamentale e deve essere tempestivamente eseguita in tutti i pazienti con addome acuto da sospetta ischemia intestinale . 
lindagine , infatti , consente di diagnosticare tale situazione patologica , contribuisce ad una corretta impostazione terapeutica e fornisce importanti valutazioni prognostiche , essendo in grado di definire la natura della patologia e lentit del danno anatomico . 
pinto 187 , 71100 foggia , italy , e - mail : drfperfetto@libero.it received : 20 june 2007 / accepted : 26 march 2008 / published online : 30 may 2009 springer - verlag 2009 abstract purpose . 
we sought to identify breast magnetic resonance imaging ( mri ) criteria capable of influencing the differential diagnosis between radial scars related to benign proliferative disease and those associated with breast cancer with a view to proposing breast mri as a promising and cost - effective modality to be carried out between mammography and surgical biopsy . 
sulle immagini di risonanza magnetica , sono state identificate 27 lesioni di dimensioni comprese tra 7 mm e 30 mdelle 27 lesioni mammarie , 15 mostravano caratteristiche di lesioni benigne , 8 apparivano come lesioni maligne e 4 erano classificate come lesioni sospette alla rm . 
la valutazione della risonanza magnetica della mammella dimostrava che solo la percentuale di enhancement e lanalisi della curva intesit di 758 radiol med ( 2009 ) 114 : 757770 be considered a useful diagnostic tool that can guide the choice between follow - up or surgical excision of radial scars . keywords breast magnetic resonance radial scar breast cancer segnale / tempo sono realmente utili nella diagnosi differenziale tra lesioni mammarie benigne e maligne . 
riteniamo che la rm possa sicuramente costituire un valido ausilio diagnostico nella scelta decisionale per il follow - up o per lescissione chirurgica di una radial scar mammaria . parole chiave mammella risonanza magnetica radial scar tumore mammario introduction introduzione radial scar ( rs ) is one of the most frequent impalpable benign proliferative lesions of the breast ( 32% ) [ 1 ]  . 
rs is bilateral or multicentric in 43% [ 2 , 3 ] and 67% [ 4 , 5 ] of cases , respectively . according to the royal college of pathologists working group , breast lesions < 10 mm are defined as rs , whereas those > 10 mm are complex sclerosing lesions [ 6 , 7 ]  . mammography depicts these lesions as dendritic alterations of the breast parenchyma caused by trabecular distortion , with thin , long , radiating spicules against a central radiolucent fibroelastotic core [ 8 ]  . 
additionally , it may occur in association with breast cancer ( ductal carcinoma in situ , invasive ductal and tubular carcinoma ) in 29%35% of cases [ 912 ]  . 
the radiological differential diagnosis of rs thus constitutes a challenge that often results in surgical excision to obtain final histological characterisation [ 1315 ]  . breast magnetic resonance imaging ( mri ) has recently been shown to play an important role in the differential diagnosis between benign and malignant lesions . 
on the basis of the time - intensity curve , it has a reported sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy of 91% , 83% , 77% , 94% and 86% , respectively , whereas on the basis of lesion enhancement rate within the first minute of the examination , the values are 91% , 37% , 47% , 87% and 58% , respectively , [ 8 , 1618 ]  . 
 the purpose of our study was to identify possible breast mri criteria helping to differentiate between rs related to benign proliferative disease and those associated with breast cancer , with the aim of proposing breast mri as a promising and cost - effective modality to be carried out between mammography and surgical biopsy . 
secondo il royal college of pathologist working group le lesioni inferiori ai 10 mm vengono definite rs mentre quelle superiori ai 10 mm vengono definite lesioni sclerosanti complesse ( csl ) [ 6 , 7 ]  . 
laspetto mammografico tipico quello di unimmagine stellata , per la distorsione trabecolare , con tralci lungi e sottili convergenti verso un nucleo centrale radiotrasparente ( di natura sclero - elastosica ) [ 8 ]  . 
questa lesione , purtroppo , spesso non chiaramente distinguibile dal punto di vista morfologico da una lesione maligna ; frequente inoltre lassociazione tra rs e carcinoma ( carcinoma intraduttale in situ dcsi , carcinoma invasivo intraduttale e tubulare ) riportata in letteratura tra il 29% ed il 35% [ 912 ]  . 
pertanto la diagnosi mammografica di rs gravata da un importante problema diagnostico differenziale che spesso induce allescissione chirurgica della lesione per la sua tipizzazione istologica definitiva [ 1315 ]  . la risonanza magnetica ( rm ) della mammella , negli ultimi anni ha assunto un ruolo importante nella diagnosi differenziale tra lesioni benigne e carcinomi riportando in letteratura una sensibilit del 91% , una specificit del 83% ( vpp 77% , vpn 94% ) ed unaccuratezza diagnostica del 86% considerando come parametro discriminate solo la curva intensit - tempo ; considerando invece fattore discriminate la percentuale di contrast enhancement al primo minuto in letteratura si riporta una sensibilit del 91% , una specificit del 37 % ( vpp 47% , vpn 87% ) ed unaccuratezza diagnostica del 58% [ 8 , 1618 ]  . radiol med ( 2009 ) 114 : 757770 materials and methods from 1998 to june 2006 , we studied 20 patients with a mammographically detected focal architectural distortion . on mammography , eight lesions appeared probably benign [ breast imaging reporting and data system ( bi - rads ) category 3 ] ; eight were suspicious ( bi - rads category 4 ) and eight were highly suspicious for breast cancer ( birads category 5 )  . 
postprocessing , carried out on an easy vision philips console , allowed us to obtain subtraction images , detect lesion enhancement kinetics and evaluate the time - intensity curve within a region of interest ( roi ) ( no larger than nine pixels ) placed over the area of maximum enhancement . 
after acquisition of the native images , a 0.2 - ml / kg bolus of paramagnetic contrast medium was administered at a flow rate of 2 ml / s , followed by a 10 - cc saline flush . dynamic imaging was started after administration of contrast material . la finalit del nostro studio stata pertanto la ricerca , mediante rm , di criteri diagnostici differenziali tra rs determinate esclusivamente da fenomeni proliferativi di tipo benigno e rs associate ad una componente carcinomatosa , con lobiettivo di proporre la rm come test intermedio tra la mammografia e la biopsia chirurgica cost - effective . materiali e metodi dal 1998 al primo semestre del 2006 sono state reclutate 20 pazienti sulla base di un riscontro mammografico di disordine architetturale orientativo in 8 casi di lesione probabilmente benigna ( bi - rads 3 ) , in 8 casi per lesione sospetta ( bi - rads 4 ) ed in altri 8 casi con elevato sospetto di neoplasia ( bi - rads 5 )  . 
le lesioni sono state classificate in considerazione dellentit della distorsione architetturale , della presenza o meno di un nucleo denso centrale , delle sue dimensioni nonch della presenza di microcalcificazioni contestuali . 
tutte le 8 pazienti inquadrate nella categoria mammografica bi - rads 3 , come lesioni probabilmente benigne , hanno preferito volontariamente sottoporsi allintervento chirurgico , piuttosto che affrontare lo stress dei successivi controlli ; 3 di esse peraltro condizionate dalla familiarit materna per carcinoma mammario . 
 rm mammella tecnica desame gli esami sono stati eseguiti con apparecchio philips gyroscan da 1t , dotato di gradienti da 16 mts , con bobina dedicata , previo posizionamento di accesso venoso mediante ago - cannulla collegato ad iniettore automatico . 
il post - processing , oltre alla sottrazione delle immagini , ha previsto lo studio dellenhancement delle lesioni e la valutazione della curva intensit / tempo previo posizionamento di una roi non superiore a 9 pixel nel punto di massima intensit del segnale della lesione ; la ricostruzione tridimensionale stata ottenuta con tecnica mip ed mpr , mediante elaborazione della iii e vi fase dinamica . 
la scelta del piano assiale invece consente , a 760 diagnostic criteria all lesions were retrospectively evaluated on the basis of the morphological and dynamic criteria proposed by fischer et al . 
the enhancement rate is calculated with the following formula : enh = si postcontrast ( within the first minute ) si precontrast 100 si precontrast the enhancement rate is regarded as an important criterion for differentiating benign from malignant breast lesions . 
in particular , we considered : enhancement rate < 50% : score 0 enhancement rate between 50% and 100% : score 1 enhancement rate > 100% : score 2 [ 1924 ] radiol med ( 2009 ) 114 : 757770 nostro avviso , una migliore visualizzazione delle regioni retro - areolari e pre - pettorali che , spesso sul piano coronale , sono sedi di fenomeni artefattuali , specie nelle immagini sottratte . 
allacquisizione delle immagini in condizioni basali seguiva liniezione rapida di mdc paramagnetico in ragione di 0 , 2 ml / kg alla velocit di 2 ml / s con successiva iniezione di 10 cc di soluzione fisiologica . 
in questo gruppo abbiamo compreso le curve inizialmente classificate come ia e ib secondo il criterio di kuhl [ 22 ] ; incremento rapido dellintensit del segnale entro il primo minuto con successivo plateau ( + 10% , 10% ) : score 1 ; incremento rapido con massima intensit ( wash - in ) entro il primo minuto ed altrettanto rapido decremento del segnale ( wash - out > 10% ) : score 2 . radiol med ( 2009 ) 114 : 757770 all patients underwent excision biopsy with final pathological diagnosis . 
lesions with fischer scores between 0 and 2 were classified as benign , those with a score of 3 as probably benign , those with scores of 45 as suspicious and those with scores between 6 and 8 as malignant . results ten of the 20 patients examined had a family history of breast cancer . 
in three cases , mri revealed a double lesion where mammography had depicted one lesion only ( pathology diagnosed rs in two cases and rs with ductal epithelial hyperplasia in one )  . 
histopathological examination confirmed all of the 27 lesions detected on breast mri and revealed 16 benign proliferative lesions and three ductal hyperplasias ( in two cases associated with rs ) , one fat necrosis with inflammatory change and three invasive ductal carcinomas ( two tubular and one cribriform ) associated with rs and four ductal carcinomas in situ . 
eight lesions had a fischer score of valutazione della percentuale di impregnazione valutazione della percentuale di impregnazione della lesione entro il primo minuto dalliniezione del mdc calcolata mediante la seguente formula : enh = si post ( entro il primo minuto dopo mdc ) si pre100 si pre tale percentuale considerata un fattore discriminate nella tipizzazione delle lesioni . 
abbiamo considerato : percentuali inferiori al 50% : score 0 ; percentuali comprese tra 50% e 100% : score 1 ; percentuali superiori al 100% : score 2 [ 1924 ]  . tutte le pazienti esaminate sono state sottoposte a biopsia escissionale con esame istologico definitivo . abbiamo considerato benigne le lesioni che presentavano un fischer score compreso tra 0 e 2 ; probabilmente benigne le lesioni con uno score di 3 ; sospette quelle con uno score di 45 ed infine maligne quelle con uno score compreso tra 6 ed 8 . 
delle 24 lesioni individuate alla mammografia , la diagnosi istologica ha confermato 17 lesioni benigne e 7 maligne . table 1 correlation between mammographic features and histological examination mammography : bi - rads classification benign breast lesionsa malignant breast lesionsa bi - rads , breast imaging and reporting data system a histological diagnosis tabella 1 correlazione tra reperti mammografici e diagnosi istologica classificazione bi - rads mammografica lesioni benignea lesioni malignea bi - rads 3 bi - rads 4 bi - rads 5 total bi - rads 3 bi - rads 4 bi - rads 5 totale bi - rads , breast imaging and reporting data system a diagnosi istologica 762 radiol med ( 2009 ) 114 : 757770 fig . 
histology confirmed all 15 benign lesions seen at mri and revealed the benign nature la successiva rm ha rilevato 27 lesioni di dimensioni comprese tra 7 mm e 30 mm ; in 3 casi stata rilevata una doppia lesione a fronte della mammografia che evidenziava ununica lesione ( di esse allesame istologico sono risultate essere in 2 casi entrambe rs ed in 1 caso rs con associata iperplasia duttale )  . 
allesame istologico sono state confermate tutte le 27 lesioni rilevate con rm , di cui 16 erano lbp , 3 iperplasie duttali ( 2 associate a rs ) , 1 steatonecrosi radiol med ( 2009 ) 114 : 757770 fig . 
in 4 / 20 cases , ( 20% ) there was either no focal enhancement or enhancement that was not significantly different from the normal breast parenchyma around the roi . 
several authors have investigated the association between enhancement pattern and tissue characteristics such as microvessel density [ 25 ] in an attempt to differentiate between benign and malignant breast lesions and predict aggressiveness and prognosis of malignancies [ 2730 ]  . 
although the results have not been univocal , there is general agreement that rim type iii type ii type iii type iii type ii total tipo iii tipo ii tipo iii tipo iii tipo ii totale 3 ( 40% ) 1 ( 15% ) 1 ( 15% ) 2 ( 30% ) 1 ( 15% ) 7 / 7 ( 100% ) a malignant malignant malignant malignant malignant 3 ( 40% ) 1 ( 15% ) 1 ( 15% ) 2 ( 30% ) 1 ( 15% ) 7 / 7 ( 100% ) a maligna maligna maligna maligna maligna dendritica anche se lo stesso aspetto era ugualmente presente in 4 lesioni benigne . 
non abbiamo mai rilevato lesioni rotondeggianti od ovali a margini lisci . il pattern del contrast enhancement si mostrato omogeneo in 19 delle 20 lesioni benigne , ma anche in 3 delle 7 lesioni maligne ; il pattern centripeto ( rim enhancement ) si evidenziato in 3 delle 7 lesioni maligne ed in 1 lesione benigna . la percentuale di contrast enhancement , entro il primo minuto dalliniezione del mdc , nelle lesioni benigne confermate istologicamente stata : inferiore al 50% in 11 / 20 casi ( 55% ) ; con valore compreso tra il 50%100% in 5 / 20 casi ( 25% ) e senza enhacement di tipo focale o comunque con contrast enhancement non significativamente differente da quello del parenchima ghiandolare adiacente la regione dinteresse ( roi ) in 4 / 20 casi ( 20% )  . 
homogeneous contrast enhancement , a characteristic of benign lesions , can also be found in some malignant lesions , such as tubular carcinoma , which is sometimes associated with rs , probably as a result of its mainly fibrotic component [ 26 , 31 ]  . 
 enhancement rate and time - signal intensity curve were mx , mammografico ; rm , risonanza magnetica alesioni non rilevate allesame mammografico discussione la rm , a differenza della mammografia , fornisce importanti indicazioni non solo sulla morfologia , ma anche su alcuni aspetti bio - funzionali delle lesioni , come ad esempio la vascolarizzazione ( neoangiogenesi ) e la permeabilit capillare , che influenzano il pattern e lentit dellenhancement della lesione stessa [ 2527 ]  . 
molti autori hanno riportato in letteratura varie esperienze sulla correlazione tra modalit di enhancement e la presenza di alcune caratteristiche tissutali , come la densit microvascolare [ 25 ] , nel tentativo di differenziare le lesioni benigne da quelle maligne , e tra queste ultime di predirne il grado di malignit nonch la prognosi [ 2730 ]  . 
i risultati tuttavia non sono univoci , pur concordando che il cosiddetto rim enhancement ritenuto essere attualmente lunico aspetto pi indicativo di lesione maligna , con fattori istomorfologici e prognostici pi sfavorevoli , mentre lassenza di un significativo enhancement nel contesto di una lesione , comunque rilevabile morfologicamente , fortemente indicativo di lesione benigna [ 25 ]  . nella nostra esperienza , la morfologia ed il pattern di impregnazione di mdc non sono elementi discriminanti tra table 6 statistical evaluation histology diseased healthy total test + test total test + test totale tabella 6 valutazione statistica istologia malati sani totale found to be more helpful in that they reflected the neoangiogenesis that characterises the presence of breast cancer . our experience showed plateau and wash - out time - intensity curves in all malignant lesions , and an enhancement rate > 100% in 6 / 7 malignant lesions . 
it is well established that vascular endothelial growth factors and vessel permeability factors may be present in rs , even in the absence of neoplastic proliferation , a fact that may lead to false positive findings [ 3235 ]  . 
this may explain our single false positive case and the four breast lesions classified as suspicious at mri . therefore , if we take into account enhancement rate and time - intensity curve and we consider the four suspicious lesions as false positive results , breast mri had a sensitivity of 100% , a specificity of 75% , an accuracy of 81% , a ppv of 58% and a npv of 100% ( table 6 )  . conclusions our experience confirmed that breast mri has very high sensitivity ( 100% ) but lower specificity ( 75% ) , even in the study of rs . 
because morphological assessment , with either breast mri or conventional imaging , proved unreliable for characterising radiol med ( 2009 ) 114 : 757770 rs benigne e lesioni maligne ; tale dato era prevedibile poich si tratta di lesioni che determinano macroscopicamente unalterazione morfologica abbastanza simile . infatti , 16 lesioni benigne mostravano aspetto amorfo irregolare mentre non abbiamo mai rilevato lesioni maligne di forma rotondeggiante od ovalare , a margini lisci . 
lomogeneit o meno del contrast enhancement non discriminante nella diagnosi differenziale tra benignit e malignit . lomogeneit del contrast enhancement , caratteristica delle lesioni benigne , si ritrova infatti anche in alcune lesioni maligne , come ad esempio nel carcinoma tubulare , talvolta associato alle rs , probabilmente in ragione della sua prevalente componente fibrotica [ 26 , 31 ]  . 
la nostra esperienza ha dimostrato curve intensit / tempo del tipo plateau e wash - out in tutte le lesioni maligne , con una percentuale di enhancement > 100% in 6 delle 7 lesioni maligne . 
tuttavia in letteratura riportata nelle rs la presenza di fattori di crescita vasculo - endoteliali e di aumento della permeabilit vascolare , anche in assenza di proliferazione neoplastica , entrambe probabile causa di false positivit [ 3235 ] , come rilevato anche nella nostra esperienza con la presenza di 1 caso falso positivo e di 4 lesioni benigne con caratteristiche rm sospette . 
considerando quindi la percentuale del contrast enhancement e la curva intensit / tempo ed includendo tra i falsi positivi anche le 4 lesioni classificate come sospette alla rm , la sensibilit della metodica si rilevata essere del 100% , la specificit del 75% , laccuratezza dell81% , il vpp del 58% ed il vpn del 100% ( tabella 6 )  . conclusioni i risultati del nostro studio confermano lelevata sensibilit ( 100% ) della rm anche nello studio della radial scar mammaria , sebbene la specificit ( 75% ) non sia entusiasmante . 
tuttavia il dato di maggior interesse si rivelato il vpn ( 100% ) , basato essenzialmente sulla valutazione dellintensit del segnale nel tempo , determinata dalle modalit di impregnazione di mdc delle lesioni . 
poich lanalisi morfo - strutturale si dimostrata essere non affidabile al fine della tipizzazione di queste lesioni , sia mediante rm e maggiormente con le metodiche tradizionali , riteniamo che la rm costituisca un ausilio per il radio - senologo nella scelta radiol med ( 2009 ) 114 : 757770 rs , we believe that dynamic breast mri might be considered a useful diagnostic tool in guiding decisions towards follow - up care or surgical excision of rs . 
 decisionale per il follow - up o per lescissione chirurgica di una radial scar mammaria e quindi anche una indagine intermedia cost - effective , in considerazione della futuribile riduzione del numero delle biopsie chirurgiche . 
between april 2006 and february 2008 , 18 patients ( 13 males and five females , age range 842 years ) with blunt abdominal trauma were evaluated with computed tomography ( ct ) and ceus at the emergency department of our institution . 
as a noninvasive , versatile , easy to perform and repeatable technique with a low rate of adverse reactions , ceus is ideally suited for this purpose and allowed us to reduce the number of ct scans , especially in the follow - up of young patients . keywords contrast - enhanced ultrasound liver spleen trauma follow - up riassunto obiettivo . 
diciotto pazienti ( 13 maschi e 5 femmine ) di et compresa fra gli 8 e i 42 anni e con trauma addominale chiuso sono giunti alla nostra osservazione da aprile 2006 a febbraio 2008 . 
a tal proposito , lecografia con mdc , in virt della sua non invasivit , facilit di esecuzione , ripetibilit del mdc e assenza di documentate reazioni avverse allo stesso , la metodica ideale per la gestione del follow - up , riducendo il numero degli esami tc ai quali i pazienti , anche di giovane et , sono sistematicamente sottoposti . 
 parole chiave ecografia con mezzo di contrasto fegato milza trauma follow - up 772 introduction ultrasound ( us ) is one of the most common techniques performed in the initial evaluation of patients with abdominal trauma [ 1 ] , as it is a noninvasive , versatile and repeatable technique . 
however , it is limited by a low accuracy in detecting and determining the extent of hepatic injuries if compared with contrast - enhanced computed tomography ( ct ) , which is still considered the gold standard [ 2 ]  . 
us in abdominal trauma has been used to detect peritoneal effusion as an indirect sign of lesions of hollow or parenchymatous organs , an application known as focused assessment sonography for trauma ( fast ) among anglo - america authors [ 3 , 4 ]  . 
us can be considered extremely valid , especially in the follow - up of known hepatic or splenic lesions in patients treated conservatively . the recent introduction of contrast - enhanced us ( ceus ) based on sulphur - hexafluoride - filled microbubbles ( sonovue ) has improved the overall accuracy of us , thanks to the possibility of carrying out a real - time study of the region of interest [ 5 , 6 ]  . 
although the high diagnostic accuracy of ceus in the detection of both the presence and extension of lesions has been widely demonstrated , little is known about its value in the long - term follow - up of patients with liver and / or splenic trauma . 
the aim of our study was to assess the role of ceus in the follow - up of patients treated conservatively after minor abdominal trauma ( hepatic and / or splenic ) diagnosed in the emergency room with ceus and ct scans . materials and methods patients between april 2006 and february 2008 , we studied 18 patients ( 13 males and five females ; age range 842 years ; mean age 29 ) who arrived in our emergency room with blunt abdominal trauma . 
the remaining 11 patients ( enrolled in the study ) were haemodynamically stable and were studied with standard us , ceus and contrast - enhanced ct to exclude haemoperitoneum within 13 h after the trauma . 
lesion type and the patients clinical conditions justified an initial conservative treatment , and all patients were admitted to the intensive care unit where they underwent close clinical and laboratory monitoring . 
as radiol med ( 2009 ) 114 : 771779 introduzione lecografia per le sue caratteristiche di semplicit di esecuzione , ripetibilit e non invasivit , rappresenta la metodica di primo approccio nella valutazione dei pazienti che giungono con riferito trauma addominale [ 1 ]  . 
tuttavia ormai noto che lecografia ha una bassa accuratezza nella identificazione diretta della lesione dorgano e nella definizione dellestensione della stessa , lasciando pertanto alla tc con mdc il ruolo di tecnica di riferimento [ 2 ]  . 
lutilizzo dellecografia nei traumi addominali stato finalizzato per molto tempo , infatti , alla identificazione di versamenti peritoneali come segno indiretto di lesione dorgano cavo o parenchimatoso , ricordando pertanto la tecnica fast ( focused assessment sonography for trauma ) degli anglosassoni [ 3 , 4 ]  . 
la metodica ecografica pu essere ormai considerata come estremamente valida soprattutto nei follow - up dei pazienti con lesione traumatica a livello epatico e / o splenico ormai accertata e che sono stati sottoposti a trattamento conservativo . la recente introduzione dellecografia con mezzo di contrasto ( contrast - enhanced ultrasound , ceus ) a base di microbolle di esafluoruro di zolfo ( sonovue ) con uno studio real - time della regione dinteresse , ha fornito numerose informazioni supplementari rispetto a quelle date dalla sola ecografia di base , fornendo pertanto allecografia unaccuratezza complessiva maggiore [ 5 , 6 ]  . 
tuttavia esistono ancora poche evidenze scientifiche riguardanti laccuratezza diagnostica della ceus nel follow - up a lungo termine di pazienti con trauma epatico e / o splenico minore monitorati esclusivamente mediante ceus . 
scopo del nostro lavoro stato , pertanto , valutare il ruolo dellecografia con mdc nel follow - up di pazienti con trauma addominale minore ( splenico e / o epatico ) sottoposti a trattamento conservativo e valutati in acuto con lecocontrastografia e a tc con mdc . materiali e metodi pazienti nel periodo compreso fra aprile 2006 e febbraio 2008 sono giunti nel pronto soccorso del nostro ospedale 18 pazienti , 13 maschi e 5 femmine , di et compresa fra gli 8 e i 42 anni , et media 29 anni , che avevano riportato un trauma addominale chiuso . 
sette di questi ( 2 femmine e 5 maschi ) sono radiol med ( 2009 ) 114 : 771779 this finding was confirmed by the laboratory parameters , after 48 h of observation in the intensive care unit , the patients were moved to a surgical ward and discharged after 79 days . 
subsequently , when standard us showed a slightly inhomogeneous area at the level of the liver or spleen parenchyma with or without effusion , ceus was performed with the intravenous administration of the contrast agent sonovue ( bracco , milan , italy )  . 
this contrast agent consists of microbubbles containing an inert gas , sulphur hexafluoride , which resonates at low acoustic pressure ranges ( mechanical index < 0.2 ) , emitting a specific signal . 
by using a specific lowmechanical - index software programme ( contrast tuned imaging , cnti , esaote ) , it is possible to detect exclusively the echoes from the microbubbles and identify both the macroand microcirculation to obtain a dynamic exploration of organ perfusion [ 7 , 8 ]  . all patients were studied with a technos mpx unit equipped with cnti software , which enables selective tuning of the unit to the signal generated by the contrast microbubbles resonating in the sonicated tissue . 
we used convex - array 3.5 mhz variable - band probes ( ca 430 ) and low us beam energy with a 4050 kpa derated pressure and a mechanical index of 0.060.08. 
then , depending on the case and the size of the patients parenchymatous organs , the operator decided whether or not to use a complete volume of contrast agent , 4.8 cc , or half the dose . 
the injection of contrast material was continuous and immediately followed by an infusion of saline solution to prevent any contrast material remaining in the cannula and to flush the contrast material into the peripheral circulation . 
exploration lasted at least 56 min to estimate changes in vascularity during the different dynamic phases , taking care not to confuse areas of altered vascularity due to the trauma with the physiological inhomogeneous enhancement of the liver and spleen during the arterial phase . 
i restanti 11 pazienti allingresso si presentavano emodinamicamente stabili e pertanto venivano sottoposti in urgenza , in un arco di tempo variabile da unora a tre ore dal trauma , ad esame ecografico standard eseguito per la ricerca di emoperitoneo , ad ecografia con mdc e a tc addominale senza e con mdc e.v. 
per il tipo di lesione e per le condizioni cliniche stato deciso un iniziale trattamento conservativo ed i pazienti sono stati ricoverati in terapia intensiva per un sistematico monitoraggio clinico - laboratoristico . 
tale dato veniva anche confermato dai parametri laboratoristici per cui , dopo 48 ore di osservazione in terapia intensiva , i pazienti sono stati trasferiti nel reparto di chirurgia e successivamente dimessi in viiix giornata . il follow - up ecografico stato eseguito a 30 giorni e nei casi di persistenza di alterazioni strutturali parenchimali relative al trauma , veniva effettuato un ulteriore controllo a 90 giorni . tecnica desame tutti i pazienti sono stati sottoposti ad ecografia di base addominale per la valutazione degli organi parenchimatosi e dei recessi peritoneali addomino - pelvici . 
successivamente di fronte ad aree di fine disomogeneit strutturale a livello dei parenchimi epatico o splenico con o senza la presenza di versamento periviscerale , si procedeva alla somministrazione e.v. 
il sonovue ( bracco , milano , italia ) costituito da microbolle di un gas inerte , lesafluoruro di zolfo , dotate della capacit di risuonare a basse pressioni acustiche ( indice meccanico inferiore a 0 , 2 ) e di emettere uno specifico segnale . 
tramite un software specifico ( cnti ) a basso indice meccanico , possibile rilevare esclusivamente gli echi provenienti dalle microbolle riuscendo cos a visualizzare sia il macroche il microcircolo in esame fornendo pertanto una valutazione dinamica della perfusione dorgano [ 7 , 8 ]  . tutti i pazienti sono stati valutati con un ecografo technos ( mpx , esaote ) dotato di software contrasto - specifico contrast tuned imaging ( cnti , esaote ) che permette una sintonizzazione selettiva dellapparecchio con il segnale proveniente dalla risonanza delle microbolle del mezzo di contrasto presenti nel tessuto insonato . 
nel presente studio stata impiegata una potenza bassa del fascio us , con derated pressure di 4050 kpa cui corrisponde un indice meccanico basso di 0 , 060 , 08 . 
where standard us showed a slightly inhomogeneous area at the level of the spleen and segment viii of the liver , the administration of contrast material showed the presence of well - defined lacerated and contused foci appearing as hypoechoic streaks , bands or areas . 
the findings included mild hepatic lacerations without evidence of perihepatic effusion in three patients ; one liver laceration with perihepatic effusion showing a maximum thickness of 2 mm , more evident in morrisons pouch and at the subdiaphragmatic level in one patient ; and splenic lesions , two of which were associated with perisplenic effusion measuring 1.5 and 3 mm maximum thickness , respectively , in six patients . 
in no case was effusion observed along the paracolic gutters or in the pelvic fossa . no change was observed at follow - up performed after 12 , 24 and 48 h . 
the hepatic or splenic trauma was thus considered healed when it showed an echogenic signal homogeneous to the remaining parenchyma at standard us and regular distribution of contrast medium during the contrast - enhanced examination . discussion ceus has taken on an increasingly important role in the study of parenchymatous organs , in particular , the liver and spleen , thanks to the advent of contrast material based on sulphur - hexafluoride - filled microbubbles that permit visualisation of hypovascular lesions in a hypervascular background . 
splenic and hepatic perfusion is 150 ml / min , and this has always limited the usefulness of color doppler imaging , which is unable to evaluate hypovascular lesions in a hypervascular background [ 9 , 10 ]  . 
lesaminatore , in base alla costituzione del paziente e alla grandezza degli organi parenchimatosi da visualizzare , ha scelto se iniettare lintera dose di sonovue , pari a 4 , 8 cc , o met dose . 
liniezione di mezzo di contrasto era continua ed immediatamente seguita da una rapida infusione di soluzione fisiologica al fine di evitare che il mezzo di contrasto residuasse , seppur in misura minima , nellago - cannula e allo stesso tempo venisse vigorosamente spinto nel circolo periferico . 
subito dopo liniezione del mezzo di contrasto iniziato lo studio dinamico dei parenchimi ; losservazione durava almeno 56 minuti per valutare le modificazioni della vascolarizzazione nelle varie fasi dinamiche , tenendo presente che in fase arteriosa il fegato e ancora di pi la milza presentano fisiologicamente molte disomogeneit parenchimali da non confondere con aree di alterata vascolarizzazione indotte dal trauma . 
 importante considerare che al momento delliniezione veniva fatto partire il cronometro dellapparecchio che ci indicava le varie fasi dellesame ; sono state fatte delle registrazioni di alcuni secondi sulla lesione e sul restante parenchima in esame , che sono state archiviate e revisionate in un secondo tempo anche insieme al medico chirurgo . 
dopo circa dieci minuti il mezzo di contrasto stato eliminato per via respiratoria in modo pressoch completo ; in alcuni casi stata iniettata una ulteriore dose di sonovue ed stata eseguita una seconda valutazione ecocontrascografica . 
nessuno dei pazienti osservati ha presentato ipersensibilit precoce o ritardata al mezzo di contrasto . risultati nella nostra esperienza luso dellecografia con mdc ha evidenziato un netto miglioramento nella identificazione e nella valutazione della reale estensione della lesione dorgano sospettata o evidenziata allesame ecografico standard . 
in tutti i casi abbiamo evidenziato una buona corrispondenza tra tc e ceus per sede , numero abbiamo evidenziato : in 3 pazienti lacerazioni epatiche senza segni di versamento periepatico , in 1 paziente lacerazione visualizzati estensione pertanto lesioni . 
lecografia con mezzo di contrasto , a due ore dal trauma , mostra area lamellare ipovascolare che si estende a tutto spessore senza , tuttavia , coinvolgimento capsulare ( b )  . la tc con mezzo di contrasto conferma la sede e lestensione della lacerazione splenica ( c )  . 
il controllo a 30 giorni con ecografia con mezzo di contrasto mostra risoluzione completa della zona di lacerazione splenica ( d )  . hypervascular parenchyma , thus revealing minimal alterations of the microcirculation as well [ 11 , 12 ]  . 
 many authors have investigated the beneficial role of ceus for blunt abdominal trauma in the acute phase and demonstrated its extraordinary capabilities for detecting major hepatic , splenic and renal traumas . 
however , the usefulness of ceus in these cases is limited by the need to epatica con versamento periepatico di circa 2 mm di spessore massimo , pi evidente nello spazio del morrison e in sede sottodiaframmatica e in 6 pazienti lacerazioni spleniche di cui 2 accompagnate da versamento perisplenico rispettivamente di 1 , 5 e 3 mm di spessore massimo . 
2a - c lecografia epatica standard in paziente politraumatizzato mostra area di alterazione strutturale disomogeneamente iperecogena ( a )  . lecografia con mezzo di contrasto , a 3 ore dal trauma , documenta area caratterizzata da scarso enhancement in relazione a lesione epatica lacero - contusiva ( b )  . 
il controllo a 30 giorni con ecografia con mezzo di contrasto mostra risoluzione pressoch completa della lesione , residua piccola zona avascolare ( c )  . radiol med ( 2009 ) 114 : 771779 nei controlli a 12 , 24 e 48 ore non vi sono state modificazioni . 
pertanto abbiamo considerato risolto il trauma epatico o splenico quando la lesione traumatica mostrava ecogenicit omogenea al restante parenchima allesame standard e presentava regolare distribuzione del mezzo di contrasto durante la fase contrastografica dellesame . discussione negli ultimi anni lecocontrastografia ha acquisito una importanza via via maggiore nello studio degli organi parenchimatosi , in particolare del fegato e della milza , grazie allavvento della ceus che permette di visualizzare aree di ipovascolarizzazione in tessuti estremamente irrorati . 
il fegato e la milza infatti ricevono una frazione della gittata cardiaca pari a 150 ml di sangue ad ogni pulsazione ; tale caratteristica ha sempre limitato lutilit del color - doppler non in grado di valutare alterazioni ipovascolari in un contesto fortemente vascolarizzato [ 9 , 10 ]  . 
il sonovue al contrario permette di identificare perfettamente aree ipovascolari nel contesto di parenchimi ipervascolari svelando cos alterazioni del microcircolo anche di dimensioni estremamente limitate [ 11 , 12 ]  . molti autori hanno valutato quale sia il potenziale della ceus nella valutazione dei traumi addominali chiusi in fase acuta mettendo alla luce straordinarie capacit di individuazione di traumi epatici , splenici e renali maggiori . in questi casi tuttavia lutilit dellecocontrastografia limitata dalla necessit di effettuare una tc total body per poter valutare non solo la condizione addominale ma anche quella toracica ed encefalica nel minor tempo possibile [ 13 , 14 ]  . per quanto riguarda i traumi minori , i dati in letteratura sono altamente discordanti in quanto si passa da livelli di sensibilit pari al 90% a livelli pari al 41% . 
queste notevoli differenze nelle varie casistiche dipendono non solo dalle capacit delloperatore e dalla costituzione fisica del paziente ma anche dalle condizioni cliniche del traumatizzato che possono limitarne la collaborazione , la grandezza e la sede della lesione e leventuale assenza di versamento intraperitoneale [ 15 , 16 ]  . radiol med ( 2009 ) 114 : 771779 fig . 
3a - c contrast - enhanced ultrasound ( ceus ) performed 3 h after the trauma shows multiple confluent areas of altered enhancement at the right centrilobular level due to posttraumatic contusion in a patient with abdominal trauma ( a )  . 
3a - c lecografia epatica con mezzo di contrasto a 3 ore dal trauma in paziente con trauma addominale documenta multiple aree confluenti di alterato enhancement in sede centrolobare destra riferibili a contusioni post - traumatiche ( a )  . 
il controllo a 30 giorni con ecografia con mezzo di contrasto mostra marcata riduzione delle aree di contusione epatica ( c )  . perform whole - body ct for the purposes of neurological , thoracic and abdominal evaluation [ 13 , 14 ]  . with regard to less severe traumas , the literature data are controversial , with sensitivities of 90% and 41% both being reported . 
this remarkable variability depends not only on the operators skill and patients build but also on the patients clinical status , which may limit cooperation ; on the size and site of the lesion ; and on the possible absence of intraperitoneal effusion [ 15 , 16 ]  . during the follow - up phase , these problems are in part overcome , as the lack of urgency and knowledge of the lesion site allows for a more detailed baseline us and selection of the best acoustic window for visualising the region of interest . 
if used in these conditions , ceus achieves a detection power similar to that of ct or magnetic resonance ( mr ) imaging while allowing real - time study of lesions . in all cases in our series , on ceus , the lesions initially appeared as clearly hypoechoic streaks , bands or areas , with nella fase di follow - up una parte di queste problematiche risulta ridotta in quanto , non essendo pi in regime di urgenza e conoscendo il sito della lesione si potr tranquillamente effettuare una ecografia di base pi dettagliata al fine di utilizzare la finestra acustica migliore per visualizzare la regione di interesse e , solo successivamente , effettuare una ecografia con mdc [ 1719 ]  . 
se utilizzata in queste condizioni lecocontrastografia acquisisce un potere di identificazione assolutamente sovrapponibile a quello di una tc o di una rm con mdc offrendo inoltre lopportunit di uno studio dinamico real - time delle lesioni . nella nostra casistica infatti , in tutti i pazienti osservati , le lacerazioni sono state identificate come strie o bande o aree ipoecogene dopo iniezione e.v. 
con morfologia e dimensioni inizialmente sovrapponibili a quelle della tc e poi via via minori fino ad una pressoch completa restitutio ad integruil fatto di sostituire in maniera efficace la tc con una metodica non invasiva particolarmente importante in considerazione della giovane et dei pazienti , sia 778 radiol med ( 2009 ) 114 : 771779 similar shape and size to those seen on ct . 
the use of ceus guarantees the absence of problems arising from both ionising radiation and the nephrotoxic effects of ct contrast agents . conclusioni per la dose elevata di radiazioni ionizzanti sia per la possibilit di evitare la nefrotossicit del mezzo di contrasto iodato impiegato in tc . 
 conclusions given the high levels of sensitivity and specificity shown by ceus in the follow - up of minor traumatic liver and spleen lesions , one might consider the possibility of replacing ct with ceus in these cases . 
moreover , ceus shows a very low rate of adverse reactions and allows one to reduce the number of ct scans , which is particularly important in the follow - up of young patients . lecografia con mezzo di contrasto ha mostrato una specificit ed una sensibilit estremamente elevate nel follow - up delle lesioni traumatiche minori epatiche e spleniche tanto da poter essere completamente sostituita alla tc in questa fase diagnostica . 
pertanto lecografia con mdc grazie ad una serie di vantaggi quali la non invasivit , la facilit di esecuzione , la ripetibilit del mdc , lassenza di documentate reazioni avverse allo stesso , risulta essere la metodica ideale nel monitoraggio delle lesioni suddette , riducendo pertanto il numero degli esami tc di follow - up in pazienti peraltro di giovane et . 
simonetti department of diagnostic and molecular imaging , interventional radiology and radiation therapy , university of rome tor vergata , 81 oxford street , 00133 rome , italy correspondence to : s . 
vertebral fractures usually become evident because of pain of varying intensity that reduces the patients quality of life , producing functional limitations , depression , disability , height loss , spinal instability and kyphotic deformity associated with impaired lung capacity . 
vertebroplasty , as derived from our experience and a review of the literature data , has more than 70%90% effectiveness for short - term pain reduction and return to activity . 
the aim of this paper was to describe the state of the art of this spinal interventional radiology procedure and to examine the future directions of percutaneous vertebroplasty . keywords vertebroplasty cryoablation radiofrequency ablation spinal interventional radiology bone cement vertebral fracture riassunto la prima vertebroplastica percutanea stata condotta da un gruppo francese nel 1984 , e riportata in letteratura nel 1987 , per il trattamento di un emangioma doloroso cervicale . 
le fratture vertebrali vengono generalmente diagnosticate in relazione alla marcata algia , di vario grado , lamentata dal paziente , che determina riduzione della qualit della vita , limitazione funzionale , depressione , disabilit , riduzione in altezza , instabilit spinale e deformit cifotica associata a compromissione respiratoria . 
la vertebroplastica , in relazione a quanto derivato dalla nostra esperienza e dai dati presenti in letteratura , presenta una efficacia di oltre il 70%90% nella riduzione del dolore a breve termine con pronta ripresa delle attivit quotidiane . 
lo scopo di questo lavoro descrivere lo stato dellarte di questa procedura di radiologia interventistica spinale e di esaminare le future direzioni della vertebroplastica percutanea . parole chiave vertebroplastica crioablazione ablazione a radiofrequenza radiologia interventistica spinale cemento osseo frattura vertebrale background and state of the art background e stato dellarte a vertebral compression fracture ( vcf ) is defined as a decrease in vertebral height by 20% or more of its initial dimensions [ 1 , 2 ]  . 
reduction in vertebral body strength may result from infiltrative processes produced by benign or la frattura vertebrale compressiva ( vcf ) definita come una riduzione in altezza del soma vertebrale di almeno il 20% rispetto alle dimensioni iniziali [ 1 , 2 ]  . 
una riduzione della resistenza offerta dal corpo vertebrale pu essere radiol med ( 2009 ) 114 : 976983 malignant neoplasms or , more commonly , from bone mineral loss precipitated by osteoporosis . 
with regard to bone neoplasms , the skeletal system is the most common localisation of metastatic deposits , and in particular , the spinal column is frequently affected by metastatic dissemination [ 3 , 4 ]  . 
in particular , painful bone metastases commonly occur in advanced cancer patients , whom are difficult to manage because of pain , reduced mobility and performance status . in osteoporotic vertebral collapses , a conservative therapy is generally achieved with bed rest , bracing , analgesics and physical therapy [ 5 , 6 ]  . 
instead , current conventional treatments for patients with painful bone metastases are primarily palliative and include localised therapies ( fractionated external beam radiation therapy and surgery ) , systemic therapies ( chemotherapy , hormonal therapy , radiopharmaceuticals , and bisphosphonates ) and analgesics ( opioids and nonsteroidal anti - inflammatory drugs ) [ 3 , 4 ]  . 
however , in secondary bone tumours , few patients are surgical candidates . all painful vertebral collapses , regardless of the underlying disease , can be adequately treated through percutaneous injection of polymethylmethacrylate ( pmma ) bone cement into the vertebral body . 
first used by galibert et al . in 1984 as vertebroplasty , the procedure was successfully applied to the treatment of c2 aggressive haemangiomas [ 7 ] and subsequently used on vcf secondary to osteoporosis and osteolytic tumours [ 811 ]  . 
over the past year , much debate and controversy has surrounded the issue of the complications of vertebroplasty ( 22 papers ) and the comparison between vertebroplasty and kyphoplasty ( 21 papers ) ; many manuscripts concerned case reports ( 16 papers ) , technical aspects ( 26 papers ) , experimental tests ( 15 papers ) , cement assessments ( 19 papers ) , reviews ( 34 papers ) , preoperative magnetic resonance imaging ( mri ) evaluation ( 4 papers ) and unspecific discussion ( 41 papers )  . causata da processi infiltrativi , prodotti da neoplasie benigne o maligne , o pi comunemente , dalla perdita della componente minerale ossea dovuta allosteoporosi . losteoporosi la principale causa di vcf in europa e negli usa . 
per quanto concerne invece le neoplasie va ricordato come il sistema scheletrico sia la pi frequente sede di localizzazione metastatica ed in particolare il rachide rappresenti uno dei segmenti maggiormente colpiti [ 3 , 4 ]  . il sintomo pi frequentemente associato alle vcf rappresentato da un intenso dolore cronico altamente debilitante in grado di compromette in modo considerevole la qualit di vita dei pazienti . 
in particolare le metastasi ossee , che solitamente si presentano in pazienti oncologici in stadio avanzato , presentano una complessa gestione a causa dellintenso dolore e della severa compromissione psico - fisica che determinano nei pazienti . nei crolli vertebrali di natura osteoporotica un iniziale trattamento conservativo generalmente condotto attraverso lallettamento , corsetti ortopedici , terapia medica ( analgesici ) e riabilitativa [ 5 , 6 ]  . 
di contro nei pazienti con localizzazioni metastatiche spinali dolorose i trattamenti convenzionali hanno prevalentemente un intento palliativo ed includono : terapie localizzate ( radioterapia stereotassica e resezione chirurgica ) , terapie sistemiche ( chemioterapia , terapia ormonale , trattamento con radiofarmaci e bifosfonati ) e terapia antidolorifica ( oppioidi e fans ) [ 3 , 4 ]  . 
in alcuni casi la rt non pu essere utilizzata per insensibilit della neoplasia o per il raggiungimento della soglia di tollerabilit di tessuti precedentemente irradiati mentre la chemioterapia pu non essere indicata a causa della sua tossicit . 
dosi elevate di antidolorifici possono produrre effetti collaterali non tollerabili . la sola resezione chirurgica pu essere considerata potenzialmente curativa , tuttavia solo pochi pazienti con metastasi ossee rientrano tra i candidati a questo tipo di trattamento . tutte le vcf , indipendentemente dalla patologia sottostante , sono adeguatamente trattate attraverso liniezione percutanea di cemento osseo del tipo polimetilmetacrilato ( pmma ) allinterno del corpo vertebrale . 
nel 1984 per il trattamento di un angioma aggressivo di c2 [ 7 ] e denominata vertebroplastica , attualmente utilizzata con successo nel trattamento delle vcf secondarie ad osteoporosi o tumori osteolitici [ 811 ]  . ad oggi sono stati pubblicati 1208 lavori sulla vertebroplastica , con 224 review su questo argomento . 
solo nel 978 radiol med ( 2009 ) 114 : 976983 published results [ 1214 ] support the view that percutaneous vertebroplasty is the treatment of choice in painful vertebral fractures refractory to medical management . 
this approach involves specifically a strict assessment of patients based on accurate clinical and imaging examinations , assessment by a dedicated team of highly specialised operators and the use of high - quality imaging guidance . new technical aspects and future directions review of the literature shows that new tendencies are essentially directed towards the development of a new generation of injectable bone cements and the use of hybrid treatments obtained by combining vertebroplasty with other minimally invasive procedures [ radiofrequency ablation ( rfa ) , cryoablation , microwave ablation ( mwa ) ] [ 15 ]  . conventional pmma , with its inherent shortcomings including highly exothermic polymerisation , incorporation of toxic components in the formulation , and , critically , the exhibition of poor integration between cement and bone , has been compared with more recent alternative materials such as bisphenol - a - glycidyl dimethacrylate ( bis - gma ) , aluminium - free zinc - based glass polyalkenoate cement ( zngpc ) , bioactive and bioresorbable calcium sulphate cement ( csc ) and calcium phosphate cement ( cpc )  . recently , in the management of vertebral neoplasms , minimally invasive surgical techniques ( miss ) have been added to the therapeutic armamentarium as an alternative option to conventional treatments in order to improve the patients quality of life and duration of survival . 
to qualify for these treatments , patients must complain of unremitting spinal pain in the absence of symptomatic spinal cord or nerve root compression and refractory to conventional therapeutic options such as radiation therapy , chemotherapy , surgery and analgesics . radiofrequency ( rf ) is one of the most promising thermal ablation techniques for the treatment of nonresectable tumors , related to multifocality or poor clinical condition of the patient [ 16 ]  . 
the tip of shielded electrode needle placed in osteolytic lesions is used to concentrate the energy produced by alternating electric current operating in the range of rf ( 2001200 khz ) in order to produce local ionic agitation and subsequent frictional heat that leads to focal coagulation necrosis in living tissue [ 17 , 18 ]  . 
 the aim of performing rf heat ablation before vertebroplasty is to obtain thermal destruction of tumour tissue and thrombose the paravertebral and intravertebral venous plexus , thereby minimising procedure - related complications , before vertebral stabilisation through intrasomatic cement injection . 
nello scorso anno dibattiti e controversie sono state incentrate principalmente sulle complicanze procedurali ( 22 articoli ) , confronto tra vertebroplastica e chifoplastica ( 21 articoli ) , case report ( 16 articoli ) , aspetti tecnici ( 26 articoli ) , test sperimentali ( 15 articoli ) , valutazione dei cementi ( 19 articoli ) , review ( 34 articoli ) valutazione preoperatoria con mri ( 4 articoli ) ed argomentazione generiche ( 41 articoli )  . 
questa affermazione contempla specificatamente una ortodossa valutazione del paziente , attraverso una accurata valutazione clinico - strumentale , equipe dedicate super - specialistiche ed un imaging procedurale di elevata qualit . 
 nuovi aspetti tecnici e future direzioni le nuove tendenze sono essenzialmente rivolte , in accordo a quanto riportato in letteratura , allo sviluppo di nuove generazioni di cementi ossei iniettabili ed allutilizzo di trattamenti ibridi ottenuti combinando la vertebroplastica con altre procedure mini - invasive ( ablazione a radiofrequenza , rfa , crioablazione ed ablazione con microonde , mwa ) [ 15 ]  . il convenzionale polimetilmetacrilato con i suoi intrinseci difetti , quali la solidificazione ad elevata esotermia , la presenza di componenti tossici nella sua formulazione e soprattutto la dimostrazione di una scarsa integrazione tra cemento e tessuto osseo , stato confrontato con nuovi recenti materiali alternativi quali il bisfenol - a - glicidil dimetacrilato ( bis - gma ) , alluminio free , zinco based glass polialkenoato cemento ( zn - gpc ) , calcio - solfato cemento bioattivo e bioriassorbibile ( csc ) e calcio - fosfato cemento ( cpc )  . recentemente nella gestione delle neoplasie vertebrali , nuove tecniche mini - invasive sono state aggiunte allarmamentario terapeutico come alternativa ai trattamenti convenzionali con il fine di implementare la qualit di vita e la sopravvivenza dei pazienti . 
per essere candidato allesecuzione di queste procedure il paziente deve lamentare un dolore spinale non remittente , in assenza di compressioni midollari o radicolari sintomatiche , refrattario alle comuni terapie convenzionali , quali radioterapia , chemioterapia , chirurgia e terapia antidolorifica . la radiofrequenza ( rf ) rappresenta una delle pi promettenti tecniche di ablazione per il trattamento dei tumori non resecabili , in relazione alla multifocalit o alle radiol med ( 2009 ) 114 : 976983 immediate cell death and preliminary assessment of lesion size . 
la punta dellago - elettrodo , posta allinterno della lesione osteolitica , utilizzata per concentrare lenergia prodotta da una corrente alternata operante nel range della radiofrequenza ( 2001200 khz ) , in modo da ottenere una agitazione ionica localizzata ed un conseguente riscaldamento frizionale in grado di produrre una necrosi coagulativa tissutale [ 17 , 18 ]  . lablazione a radiofrequenza prima della vertebroplastica ha lobiettivo di ottenere la necrosi termo - indotta del tessuto tumorale e la trombosi del plesso venoso intra e paravertebrale , cos da ridurre le complicanze peri - procedurali , prima di stabilizzare il corpo vertebrale attraverso la somministrazione intraspongiosa di cemento osseo . 
il pmma viene quindi caricato allinterno di un sistema di iniezione dedicato e somministrato attraverso lago da vertebroplastica allinterno del corpo vertebrale sotto guida fluoroscopica continua [ 19 ]  . 
inoltre il congelamento , riducendo lattivit dei nocicettori e le trasmissioni sinaptiche , produce una parziale analgesia diminuendo cos il dolore intra - procedurale avvertito dal paziente . la crioablazione attualmente estesamente utilizzata con successo nel trattamento di molteplici neoplasie quali il tumore prostatico , renale , epatico , polmonare , mammario ed uterino . 
il funzionamento degli aghi da crioablazione ( 17 gauge = 1 , 47 mm ) basato sul rilascio e la rapida espansione di gas argon attraverso una porzione isolata della sonda che determina il congelamento con il raggiungimento di temperature inferiori ai 180c nellarco di pochi secondi . 
ai diversi cicli di congelamento / riscaldamento , il cui numero e durata dipende dalle caratteristiche della lesione e delle strutture circostanti , viene fatta seguire la somministrazione del pmma allinterno della lesione osteolitica somatica attraverso gli aghi da vertebroplastica . 
2 immagine tc assiale a livello di l5 documenta la presenza delliceball allinterno della lesione osteolitica vertebrale rappresentata da unarea di ridotta densit . and synaptic transmission so that patients do not experience pain during the procedure . cryoablation has been extensively used to successfully treat neoplasms in different organs , including the prostate , kidney , liver , lung , breast and uterus . 
after multiple freeze - thaw - freeze cycles performed for each lesion , the number and duration of which depend on the features of the lesion itself and the proximity of critical structures , the procedure is concluded by injecting pmma in the vertebral body osteolytic lesion through the vertebroplasty needle . 
different combined transpedicularly approaches to metastasis are aimed at freezing the entire circumference of the lesion ; 17 - gauge cryoprobes ( icerod , galil medical , yokneam , israel ; iceseed , galil medical , yokneam , israel ) are then introduced coaxially , up to the distant border of the lesion , immediately behind the vertebral cortical wall . 
the biopsy needles are then retracted slightly to obtain a better exposure of the tip of the freezing radiol med ( 2009 ) 114 : 976983 crioablazione da 17 g ( icerod o iceseed , galil medical , yokneam , israele ) sono quindi introdotti coassialmente sino al margine distale della lesione , subito al di sotto della superficie corticale vertebrale . 
sono attualmente disponibili in commercio due differenti tipi di sonde da crioablazione , licerod ( 16 mm41 mm ellissoide a 40c ) con una doppia camera per lespansione dei gas che permette di ottenere un ice - ball di maggiori dimensioni e liceseed ( 10 , 5 mm19 mm ellissoide a 40c ) con una sola camera despansione per i gas [ 20 , 21 ]  . il gas argon compresso attraversando lago da crioablazione ne determina il raffreddamento della punta e la formazione dellice - ball ( effetto joule - thomson )  . 
 intervallati da una i cicli di congelamento della durata di 10 min sono generalmente fase di riscaldamento passivo di 5 min in modo da permettere un adeguato scongelamento del tessuto lesionale circostante alla probe e permetterne la rimozione , prima della successiva somministrazione del pmma . 
le cellule che sopravvivono al primo insulto da congelamento muoiono successivamente per i danni strutturali ed ischemici subiti . dopo ogni ciclo di congelamento un controllo tc rileva la presenza dellice - ball intralesionale visualizzato come unarea di ipodensit che dalla punta dellago si diparte a coinvolgere la lesione neoplastica e parte del tessuto limitrofo , risparmiando la corticale vertebrale . 
entrambe le procedure combinate di ablazione a radiofrequenza o crioablazione e vertebroplastica sono eseguite sotto guida fluoroscopica e dopo somministrazione di anestesia locale . conclusioni attualmente la somministrazione percutanea di cemento osseo allinterno del soma vertebrale rappresenta un fig . 
the icerod ( 16 mm41 mm ellipsoid at 40c ) , with its double - chambered gas expansion , allows wider ice - ball formation in comparison with the iceseed ( 10.5 mm19 mm ellipsoid at 40c ) , which has a single gas chamber on the exposed tip [ 20 , 21 ]  . 
 generally , freezing cycles ( 10 min each ) are interspersed with a 5 - min passive thaw in order to defrost surrounding tissue and release probes for subsequent pmma injection . a double freeze / thaw cycle increases the statistical probability of intracellular ice formation and cell damage . 
after each freezing step , a ct scan reveals the presence of ice balls within the lesion , visualised as hypodense areas arising from the probe tips enveloping the greater part of the lesion and a small surrounding area , sparing the wall of the vertebral bone . during the last thaw phase , the pmma is prepared by combining the monomer and powder polymer and then delivering it into the vertebral body . 
according to published reports , new tendencies , in particular in interventional oncology , are essentially directed towards the development of hybrid treatments , obtained by combining vertebroplasty with other minimally invasive procedures . 
rf heat ablation or cryoablation and vertebroplasty have shown to be effective , simple and safe in treating vertebral collapse consequent to metastases and to provide early and long - lasting pain relief with evident increase in vertebral weight - bearing resistance . over the next few years , we will probably see the development and validation of other new procedures to be combined with vertebroplasty . approccio mini - invasivo per il trattamento delle fratture vertebrali compressive amieliche . 
in accordo con quanto riportato in letteratura le nuove tendenze soprattutto nellambito dellinterventistica oncologica mirano allo sviluppo di nuovi trattamenti ibridi ottenuti combinando la vertebroplastica ad altre procedure mini - invasive . 
la rfa o la crioablazione associate alla vertebroplastica si sono dimostrate procedure efficaci , semplici e sicure nel trattamento delle vcf conseguenti a localizzazione metastatica , in grado di garantire una repentina e duratura riduzione del dolore associata ad un significativo incremento della resistenza vertebrale . 
ct helps to detect a growing number of increasingly small lesions , but , as with chest radiography , the primary goal in the evaluation of small pulmonary nodules is to exclude malignancy . 
the role of the radiologist is therefore to help the clinician determine the most appropriate management strategy by using all available modalities [ ct , magnetic resonance ( mr ) imaging , positron emission tomography ( pet ) ] and evaluating the patients clinical history and the imaging features leading to a diagnosis of benignity or malignancy . 
imaging features include nodule size , margins , calcifications and fatty component , internal features ( cavitations , pseudocavitations , air bronchogram , halo sign ) , as well as advanced techniques for characterisation ( growth rate , contrast enhancement ) and management ( computer - aided diagnosis , bayesian analysis , neural networks )  . 
the aim of this paper is to summarise the approach to pulmonary nodules from the point of view of the radiologist , oncologist and thoracic surgeon . riassunto il ruolo della tc nella diagnostica dei noduli polmonari in continua espansione : con tale metodica , infatti , si individua un numero crescente di lesioni e di dimensioni sempre minori , ma come avveniva con le radiografie , il primo obiettivo nel valutare questi piccoli noduli escluderne la natura maligna . 
il ruolo del radiologo consiste quindi nellaiutare il clinico a scegliere la strategia diagnostica pi appropriata , adottando tutte le metodiche a sua disposizione ( tc , rm , pet ) e valutando la storia clinica e quegli aspetti radiologici che lo indirizzino verso una diagnosi di benignit o di malignit : dimensioni , margini , presenza di calcificazioni o di una componente adiposa , caratteristiche proprie del nodulo ( cavitazioni , pseudocavitazioni , broncogramma aereo , segno dellalone ) , integrati a tecniche avanzate di caratterizzazione ( tasso di crescita , contrast enhancement ) e di gestione ( diagnosi computer - assistita , analisi bayesiana , reti neurali )  . 
obiettivo di questo lavoro fare il punto della situazione sullapproccio al nodulo polmonare dal punto di vista del radiologo e delloncologo da un lato e del chirurgo toracico dallaltro . keywords pulmonary nodule computed tomography lung screening parole chiave nodulo polmonare tomografia computerizzata polmone diagnosi precoce 872 introduction the term solitary pulmonary nodule ( spn ) traditionally refers to a round or oval lesion 30 mm or less in diameter surrounded on at least two thirds of its perimeter by lung parenchyma and not associated with atelectasis or hilar adenopathy [ 1 , 2 ]  . 
this definition is predominantly based on information obtained from the standard chest radiograph . the expanding role of computed tomography ( ct ) in medical imaging has offered additional important insights , including that of focal opacity , a term encompassing solid , semisolid and nonsolid lesions of variable shape . 
 the incidence of spns , based on standard chest radiography , was believed to be approximately 150 , 000 new cases per year in the united states [ 3 ]  . 
however , the incidence has increased dramatically with the diffusion of ct equipment and especially of new - generation scanners that allow thin - slice imaging of the entire chest in a few seconds . 
 as with radiographically detected nodules , the first concern in evaluating an spn is to exclude malignancy . despite the availability of many diagnostic tests of variable invasiveness , it should be noted that diagnostic accuracy tends to decline as nodule size decreases . 
the role of the radiologist is therefore to help the clinician select the most appropriate management strategy . clinical presentation and differential diagnosis the majority of neoplastic spns are lung carcinomas , whereas metastases from extrapulmonary tumours account for approximately one third of all cancerous nodular lesions . our experience with a lung cancer screening programme has shown that approximately 97% of screen - detected pulmonary lesions are benign and likely to be related to granulomatous infectious diseases ( tuberculosis , histoplasmosis , coccidioidomycosis ) , which account for 80% of benign diseases , followed by hamartomas ( 11% of lung resections for benign pulmonary nodules ) ( unpublished personal data )  . 
the imaging features of an spn that is subsequently characterised as bronchogenic carcinoma are of a mass of variable diameter , with poorly defined or spiculated margins , commonly located in the upper lobes . 
the corona radiata sign is a common finding that may be ascribed surrounding tissues and obliteration of the small vessels and bronchioles . infiltration , oedema of to neoplastic although the presence and site of the primary tumour are generally known in the case of lung metastases from an extrapulmonary tumour , metastases may occasionally arise before the signs and symptoms of the primary tumour become manifest or many years after apparently radical surgery . 
in this case , the differential diagnosis must include radiol med ( 2009 ) 114 : 871889 introduzione con il termine nodulo polmonare solitario ( nps ) si indica tradizionalmente una lesione tondeggiante o ovalare di diametro non superiore ai 30 mm , circondata per almeno i due terzi da parenchima polmonare , in assenza di atelettasia o adenopatie ilari [ 1 , 2 ]  . 
questa definizione si basa soprattutto su informazioni ottenute dal radiogramma standard ; con la tc ( tomografia computerizzata ) , il cui ruolo nella diagnostica medica in continua espansione , sono emersi ulteriori aspetti che non si possono trascurare nel definire un nps . 
 lincidenza dei nps , calcolata sui radiogrammi standard del torace , stata stimata in passato intorno ai 150000 nuovi casi / anno negli usa [ 3 ] , ma lincidenza aumenta drasticamente considerando la diffusione sul territorio delle apparecchiature tc e soprattutto quelle di ultima generazione le quali consentono di acquisire immagini dellintero torace in pochi secondi utilizzando collimazioni sottili . cos come avveniva con le classiche radiografie , il primo obiettivo che ci si pone nel valutare un nps quello di escluderne la natura maligna . 
a tale fine sono disponibili numerosi tests diagnostici , pi o meno invasivi , ma occorre notare come la loro accuratezza diagnostica diminuisca con la riduzione delle dimensioni del nps . 
il ruolo del radiologo consiste quindi nellaiutare il clinico a scegliere la strategia diagnostica pi appropriata . clinica e diagnosi differenziale la maggior parte dei nps neoplastici costituita da carcinomi polmonari , mentre le metastasi da tumori extrapolmonari rappresentano allincirca un terzo di tutte le lesioni nodulari neoplastiche . 
dalla nostra esperienza , derivata da un programma di screening , emerso che allincirca il 97% delle lesioni polmonari riscontrate con questi programmi sono di natura benigna e le cause pi frequenti sono da ricercarsi nella patologia infettiva granulomatosa ( tubercolosi , istoplasmosi , coccidiomicosi ) , rappresentante l80% circa della patologia benigna , seguita dagli amartomi ( 11% circa delle resezioni polmonari per noduli benigni polmonari ) ( dati personali , non pubblicati )  . 
laspetto di un nps , che risulti poi essere un carcinoma broncogeno quello di una formazione , pi frequentemente localizzata a carico dei lobi superiori , di diametro variabile , a margini scarsamente definiti , o frastagliati . 
frequente il segno radiologico della corona raggiata , da attribuirsi ai fenomeni infiltrativi della neoplasia , alledema dei tessuti circostanti e a fenomeni obliterativi a carico di piccoli vasi e bronchioli . nel caso di metastasi polmonari da tumore primario extrapolmonare , in genere la presenza e la sede del tumore radiol med ( 2009 ) 114 : 871889 the possibility of a new primary bronchopulmonary malignancy or a benign lesion . metastases , which tend to occur in the subpleural regions of the lower lobes , may originate from cancers affecting any organ with venous drainage to the right heart and hence to the pulmonary vascular bed : head and neck carcinomas , renal carcinoma , testicular carcinoma , choriocarcinoma , osteosarcoma and soft - tissue sarcomas , melanoma and endocrine tumours ( thyroid and adrenal glands ) , in addition to breast and prostate cancer . 
most paediatric cancers , with the exception of neuroblastoma , tend to metastasise to the lungs . the following abnormalities may also appear as spns : pulmonary abscess ( in the initial phase of circumscribed parenchymal consolidation ) , tuberculoma , colonisation by ( especially aspergillus ) , amoebiasis , fungal hyphae echinococcosis , rheumatoid arthritis , wegeners granulomatosis , bronchogenic cyst , lung sequestration and arteriovenous fistula ( associated with rendu - oslers disease in 30%60% of cases )  . 
determining whether an spn is benign or malignant therefore requires the interpretation and integration of several clinical and radiological features by using the techniques described below . basic radiological evaluation criteria a small spn is more likely to be benign [ 46 ]  . 
similarly , lobulated contours , a sign of uneven growth of the cellular components , are often associated with malignant spns [ 11 ] , even though 25% of benign spns exhibit lobulated appearance [ 6 ]  . 
 ( 4 ) popcorn and primitivo sono note , ma occasionalmente possono manifestarsi prima che insorgano segni e sintomi della neoplasia primaria o molti anni dopo una resezione chirurgica apparentemente radicale . 
in questo caso la diagnostica differenziale deve considerare anche lipotesi di una nuova neoplasia maligna broncopolmonare primitiva o di una lesione benigna . le metastasi , la cui localizzazione preferenziale a carico dei lobi inferiori , in regione mantellare sottopleurica , possono derivare da tutti gli organi con drenaggio venoso diretto al cuore destro e quindi al letto vascolare polmonare : carcinomi della testa e del collo , del rene , del testicolo , corioncarcinomi , osteosarcomi e sarcomi delle parti molli , melanomi e tumori endocrini ( tiroide e ghiandola surrenale ) , oltre a carcinomi mammario e prostatico . anche la maggioranza dei tumori pediatrici , con leccezione del neuroblastoma , metastatizzano preferibilmente in ambito polmonare . possono apparire come nps anche lascesso polmonare ( nelliniziale fase di condensazione parenchimale circoscritta ) , il tubercoloma , la colonizzazione di cavit polmonari da parte di ife fungine ( per lo pi quelle dellaspergillo ) , lamebiasi , lechinococcosi , lartrite reumatoide , la granulomatosi di wegener , la cisti broncogena , il sequestro polmonare e la fistola artero - venosa ( nel 30%60% dei casi associata alla malattia di rendu - osler )  . 
stabilire , quindi , se un nps sia benigno o maligno richiede linterpretazione e lintegrazione di molteplici elementi clinici e radiologici con le tecniche che saranno ora esaminate . criteri radiologici elementari di valutazione dimensioni generalmente un nps di piccole dimensioni ha buone probabilit di essere benigno [ 46 ]  . 
tuttavia , le dimensioni ridotte non escludono con certezza un potenziale di malignit , poich il 15% delle lesioni maligne risultano di diametro inferiore a 10 mm [ 79 ]  . 
sebbene la maggior parte dei nps con margini lisci e regolari possa essere definita benigna , necessario ricordare che tale aspetto presente anche nel 21% delle lesioni maligne [ 10 ] ; analogamente i contorni lobulati , sinonimo di crescita non sincronizzata delle componenti cellulari , con zone a maggior tasso di crescita ed altre nelle quali la proliferazione minore , sono spesso associati alla 874 radiol med ( 2009 ) 114 : 871889 fig . 
2 nodulo completamente calcifico in sede apicale destra , visualizzato con la finestra del parenchima e del mediastino ( pregressa tbc )  . ( 5 ) punctate [ 15 ]  . 
the first four are typical of benign lesions ( in particular , the first three are typical of granulomas or infectious lesions such as histoplasmosis or tuberculosis , whereas popcorn calcifications are characteristic of hamartomas )  . 
pseudocavitation is not related to tissue necrosis but to lepidic growth , that is , to the proliferation of tumour cells around the alveolar wall , with sparing of air - filled areas . these features , when associated with air bronchogram , will lead to a diagnosis of a bronchioloalveolar adenocarcinoma [ 6 , 19 ]  . 
la cavitazione un fenomeno pi frequente in noduli di dimensioni superiori a 3 cm , ma stata osservata anche in lesioni di diametro di 7 mm [ 13 ]  . 
la pseudocavitazione deve il suo aspetto non a fenomeni di necrosi tissutale , ma alla crescita lepidica , ovvero alla proliferazione delle cellule tumorali intorno alla parete alveolare , con risparmio di aree a contenuto aereo . 
5a noduli a " vetro smerigliato " periferici , risultati essere all ' esame istologico definitivo un ' area di adenomatosi bronchiolo - alveolare e b un carcinoma bronchiolo - alveolare . haemorrhage , although it has also been seen in conjunction with other infections , vasculitis and neoplasms [ 20 ]  . nodules with ground - glass appearance are increasingly frequently detected at high - resolution ct ( hrct )  . 
recently , a close correlation was established between ct diagnoses of ground - glass spns and the histological findings of adenocarcinoma : the ground - glass component in adenocarcinomas is associated with lepidic growth or mucin production [ 19 , 22 ] , and its possible predominance over the solid component is related to prognosis . 
il segno dellalone , costituito da unarea di ground - glass che circonda una nodularit [ 1 ] , fu descritto per la prima volta da kuhlman in pazienti immunocompromessi con aspergillosi polmonare angioinvasiva precoce , correlandosi ad aree di emorragia polmonare , ma stato osservato anche in presenza di altre infezioni , vasculiti e neoplasie [ 20 ]  . 
recentemente si giunti a definire una stretta corrispondenza tra le diagnosi tc di nps a vetro smerigliato ed il corrispettivo istologico di adenocarcinoma : la componente a vetro smerigliato negli adenocarcinomi associata alla crescita lepidica o alla produzione di mucina [ 19 , 22 ] e la sua preponderanza o meno rispetto alla componente solida correlata alla prognosi . 
 [ 23 ] hanno evidenziato che la maggior presenza della componente solida nel contesto di nps ground - glass associata ad un comportamento maggiormente invasivo ( tipi c , d , e , f della classificazione noguchi , ovvero , rispettivamente , carcinomi bronchioloalveolari con presenza di proliferazione fibroblastica , carcinomi poco differenziati , tubulari e papillari , con un pattern di crescita di tipo compressivo ) [ 23 , 24 ]  . 
 [ 25 ] hanno dimostrato che la maggior presenza della componente ground - glass inversamente correlata , in adenocarcinomi periferici inferiori a 30 mm , alla probabilit di sviluppare recidive [ 25 ]  . 
il tempo di raddoppiamento ( ossia il tempo necessario affinch un nps raddoppi il suo volume ) per la maggior parte dei nps maligni si colloca tra i 30 ed i 400 giorni e corrisponde ad un aumento del diametro del nps del 26% [ 26 ]  . 
la stabilit dimensionale per un periodo superiore a due anni , ai controlli radiografici o tc , implica un tempo di radiol med ( 2009 ) 114 : 871889 component within ground - glass spns is associated with a more invasive behaviour ( noguchi type c , d , e , f ; or , respectively , bronchioloalveolar carcinoma with fibroblastic proliferation , poorly differentiated adenocarcinoma , tubular adenocarcinoma and papillary adenocarcinoma with a compressive growth pattern ) [ 23 , 24 ]  . 
for most malignant spns , doubling time ( the time required for a nodule to double in volume ) is between 30 and 400 days and corresponds to a 26% increase in diameter [ 26 ]  . 
6 evoluzione nell ' arco di 12 mesi di un nodulo ( carcinoma broncogeno )  . raddoppiamento di almeno 730 giorni ed generalmente considerata un affidabile indicatore di benignit [ 3 , 27 ] , sebbene recentemente anche questa assunzione sia stata messa in dubbio . 
infatti una rivalutazione dei dati in letteratura dimostra che il valore predittivo di benignit correlato alla stabilit dimensionale per una finestra di due anni solo del 65% [ 2830 ]  . 
per esempio un nps di 5 mm pu raddoppiare di volume in 6 mesi ( tasso di crescita indicante malignit ) , ma il diametro aumenter solamente di 1 , 25 mm , divenendo di 6 , 25 m questa minima crescita di diametro assai difficile da apprezzare , cosicch i nps maligni di piccole dimensioni possono raddoppiare di volume apparendo stabili radiologicamente , con un conseguente ritardo nella diagnosi . 
per superare questo problema stato proposto di misurare il tasso di crescita dei nps di piccole dimensioni con misurazioni seriali non tanto del diametro quanto del volume [ 31 ]  . 
a tale scopo esistono dei software che , attraverso algoritmi matematici acquisiti per mezzo di una roi applicata al nps stesso , in maniera pi o meno automatica , calcolano volume , dimensioni e massa . 
questi software volumetrici 3d hanno il limite di non permettere la corretta valutazione dei nps non solidi , mentre la loro affidabilit sembra essere buona nella valutazione dei nps parzialmente solidi , nel cui caso , essendo ad alto rischio di malignit , lo studio deve essere pi accurato e pi rapido [ 21 ]  . 
sono necessari ulteriori studi per determinare precisamente lefficacia di questi software nel calcolare lintervallo di raddoppiamento e decidere se integrarli nella pratica quotidiana , al fine di diminuire lintervallo di follow - up . contrast enhancement ( impregnazione contrastografica ) nella caratterizzazione del nps importante anche valutare il contrast - enhancement . 
alcuni studi presenti in letteratura hanno dimostrato che il flusso di sangue nei nps maligni quantitativamente e qualitativamente diverso rispetto ai nps benigni [ 32 , 33 ] ed il grado di enhancement direttamente correlato con la vascolarizzazione del nps e con la probabilit di malignit [ 34 ]  . 
con la tecnica definita come quantitative contrast - enhanced ct ( qect ) , la valutazione dellenhancement pu essere ottenuta per mezzo di scansioni sottili contigue ( 13 mm ) prima e dopo la somministrazione di mezzo di contrasto per via endovenosa con flusso di 2 ml / s ( dose totale di 420 mg / kg )  . 
le scansioni vengono acquisite ogni 30 secondi per 5 minuti e lindice di attenuazione viene misurato allinterno del nps stesso prima della somministrazione del mdc ed al raggiungimento del picco massimo di contrast - ehnancement . 
un enhancement inferiore a 15 uh fortemente indicativo di lesione benigna , mentre se 878 radiol med ( 2009 ) 114 : 871889 exhibiting faster or slower doubling times tend to be benign . 
dimensional stability for > 2 years on chest radiography or ct implies a doubling time of at least 730 days and is generally considered a reliable indicator of benignity [ 3 , 27 ]  . 
this assumption has , however , recently been challenged , with a review of the literature showing that the predictive value for benignity of 2 - year stability was only 65% [ 2830 ]  . 
software has been developed that provides semiautomated calculations of volume , size and mass by applying mathematical algorithms to data acquired in a region of interest ( roi ) placed over the spn . 
although this 3d volumetric software has limits in the evaluation of nonsolid spns , it appears to have a good level of reliability in semisolid spns , whose higher risk of malignancy warrants a more accurate and faster study [ 21 ]  . 
further research is needed to establish the true effectiveness of these software packages in calculating doubling time and decide whether they should be used in clinical practice to reduce the interval between follow - up examinations . contrast enhancement contrast enhancement is another factor to be assessed when evaluating an spn . 
some studies have shown that blood flow in malignant spns is quantitatively and qualitatively different from that in benign spns [ 32 , 33 ] and that the degree of enhancement is directly related to spn vascularity and the likelihood of malignancy [ 34 ]  . 
with quantitative contrast - enhanced ct ( qect ) , enhancement is evaluated on contiguous thin sections ( 13 mm ) acquired before and after intravenous administration of contrast material at a rate of 2 ml / s ( total dose 420 mg / kg )  . 
the scans are acquired every 30 s for 5 min , and the attenuation index is measured in the spn before contrast administration and once the maximum enhancement peak has been reached . 
per migliorare ulteriormente lattendibilit del contrast - enhancement , recentemente si provato ad operare una segmentazione automatica computerizzata dei nps ed una determinazione del valore medio di densit di tutti i voxel della lesione segmentata [ 29 ]  . 
 [ 32 ] , nel loro studio per lidentificazione precoce del cancro polmonare con tc a bassa dose , hanno utilizzato il contrast - enhancement in caso di nps inferiori a 8 mm . rmn ( risonanza magnetica nucleare ) il principio di base che consiste nel confermare o escludere la presenza di vascolarizzazione mediante esami dinamici applicabile anche alla risonanza magnetica ( rm ) [ 21 , 31 ]  . la rm dinamica offre il vantaggio potenziale di permettere lacquisizione di pi misure nel tempo e di conseguenza consente la valutazione dellandamento della curva di enhancement . 
 [ 36 ] hanno evidenziato un picco di aumento di contrasto pi alto nei nps maligni rispetto a quelli benigni e in aggiunta , valutando la pendenza della curva di enhancement ( che non pu essere derivata dalla qect utilizzando la tecnica usuale ) , hanno dimostrato che le lesioni maligne avevano una pendenza pi pronunciata rispetto alle lesioni benigne [ 36 ]  . 
questo studio , inoltre , differenziava le lesioni benigne ( ad esempio il granuloma ) dalle infezioni attive : la maggior parte delle lesioni benigne aveva un picco di aumento di contrasto molto basso , mentre le infezioni attive mostravano in media un aumento di contrasto persino maggiore rispetto ai tumori maligni , come confermato da kono et al . 
di conseguenza , il picco di aumento di contrasto e la pendenza della curva potrebbero consentire di distinguere tra lesioni benigne e tutte le altre ( lesioni maligne e infezioni attive ) , esistendo una sostanziale sovrapposizione tra lesioni maligne e infezione attiva per entrambi i parametri . 
la variazione di densit ( 94 , 6 hu ) del nodulo suggestiva per una lesione evolutiva maligna ( diagnosi post - chirurgica di carcinoma broncogeno )  . rispetto alla tc limita ancor di pi lutilizzo della rm per la valutazione dei nps di piccole dimensioni . 
pertanto , il valore della rm dinamica , rispetto alla qect , che disponibile ovunque ed a costi ridotti ( con valore predittivo negativo pari al 96% ) , deve ancora essere accertato . 
 pet ( tomografia ad emissione di positroni ) lutilit della pet , metodica in grado di fornire informazioni complementari a quella morfologica di tc e rm nella valutazione dei nps , stata oggetto di numerosi studi , molti dei quali hanno evidenziato una sensibilit ed una specificit del 90% circa [ 3840 ]  . 
tuttavia , a quanto ci risulta , non esistono studi che comparino laccuratezza della pet e della pet - tc nella valutazione del nps . esistono , inoltre , alcune potenziali limitazioni allutilizzo della pet nella pratica clinica che devono essere prese in considerazione . 
per esempio , numerosi processi infiammatori ed infettivi , come la tbc o le infezioni fungine , possono captare il fluorodesossiglucosio ( fdg ) e simulare la presenza di un nodulo maligno . 
quindi necessario conoscere in dettaglio lanamnesi patologica prossima e remota del paziente [ 41 , 44 ] e sfruttare le informazioni ottenute dalla sinergia di una metodica morfologica quale la tc con una funzionale quale la pet . 
to further improve the reliability of contrast enhancement , researchers have recently attempted to perform automated segmentation of spns and determination of the mean density value of all voxels in the segmented lesion [ 29 ]  . 
used contrast enhancement for spns < 8 mm [ 32 ]  . mri ( magnetic resonance imaging ) the primary goal of confirming or excluding lesion vascularity by means of a dynamic study also applies to magnetic resonance ( mr ) imaging [ 21 , 31 ]  . 
in agreement with the ct findings , ohno et al . observed a higher enhancement peak in malignant spns than in benign lesions and , by assessing the slope of the enhancement curve ( which cannot be derived from qect using the normal technique ) , demonstrated that malignant lesions had more pronounced slopes compared with benign lesions [ 36 ]  . the authors also distinguished between benign lesions ( e.g. granulomas ) and active infections : most benign lesions had a very low enhancement peak , whereas active infections generally presented enhancement peaks that were even higher than those of malignant tumours , a finding confirmed by kono et al . 
consequently , the enhancement peak and the slope of the enhancement curve might enable benign lesions to be differentiated from all other lesions ( malignant lesions and active infections ) , given the substantial similarity of both parameters in nonbenign lesions . 
thus , the value of dynamic mr imaging compared with qect , a widely available and inexpensive technique with 96% negative predictive value , has yet to be established . positron emission tomography ( pet ) the utility of pet , a method providing complementary information to the morphological data offered by ct and mr imaging , has been investigated in several studies , most of which have reported sensitivity and specificity values around 90% [ 3840 ]  . 
however , to our knowledge , no study has compared the accuracy of pet and pet - ct in the evaluation of spns . there are potential limitations to the use of pet in clinical practice . 
for example , numerous inflammatory and infectious processes , such as tuberculosis or fungal infections , may take up fluorodeoxyglucose ( fdg ) and mimic a malignancy ; similar findings have been observed in the presence of sarcoidosis , silicosis and other granulomatous processes [ 38 , 4143 ]  . 
differentiation thus requires a thorough knowledge of the patients recent and past medical history [ 41 , 44 ] and integration of information resulting from the combination of morphological ct imaging and functional pet imaging . 
 to distinguish malignant spns from inflammatory and maligni da processi infiammatori ed infettivi , alcuni autori sostengono lutilit di unacquisizione pet o pet - tc ad unora dalla somministrazione del fdg ( come avviene comunemente ) e di una seconda acquisizione dopo 24 ore circa [ 41 , 45 , 46 ]  . 
la ragione che sottende a questa seconda scansione che le lesioni maligne generalmente tendono a continuare ad accumulare il fdg col passare del tempo , mentre i processi infiammatori ed infettivi diminuiscono la captazione di fdg nel tempo . 
per quanto concerne le dimensioni , la maggior parte degli scanner pet in uso attualmente ha una risoluzione spaziale di circa 6 mm , a patto che la lesione sia metabolicamente molto attiva . 
tuttavia , falsi negativi possono aversi in caso di noduli primitivi o secondari con minor attivit metabolica , come nel caso del carcinoma bronchiolo - alveolare o dei carcinoidi [ 4749 ]  . 
il valore soglia di suv ( standardized up - take value ) minimo riportato in letteratura per definire come maligno un nodulo solitario di 2 , 5 [ 50 , 51 ]  . 
in realt dalle meta - analisi questa valutazione quantitativa non sembra migliorare i dati di efficacia rispetto alla sola valutazione qualitativa . futuri sviluppi : tc perfusionale , diagnosi computerassistita ( cad ) , analisi bayesiana e reti neurali la neoangiogenesi promuove la crescita del tumore assicurando il necessario nutrimento alle cellule neoplastiche e gioca un ruolo importante nella metastatizzazione , grazie alla mancanza di integrit della parete vasale [ 5254 ]  . 
i cambiamenti nel volume dei vasi , nella perfusione e nella permeabilit vascolare sono valutati mediante limaging di perfusione , che si basa sullanalisi di curve tempo - densit ( tdc ) calcolate per ogni pixel della sezione acquisita con scansioni consecutive , dopo iniezione a bolo di mezzo di contrasto iodato [ 55 ]  . 
lavvento delle tc 16 banchi ha consentito , grazie ai brevi tempi di acquisizione e alla migliore risoluzione temporale e spaziale sullasse z , di campionare i parametri fisiologici su un maggiore volume di tessuto ( 68 sezioni )  . alcuni autori hanno evidenziato come lenhancement di un tumore polmonare periferico e quello dellaorta avvengano con la stessa tempistica , a causa dellabbondante apporto vascolare derivante dalle arterie bronchiali [ 5658 ]  . 
inoltre , questo tipo di lesione mostra un abbondante interstizio ed una rete linfatica ridotta o assente , entrambi responsabili della ritenzione del mezzo di contrasto nel nodulo con caratteristico ritardato wash - out . le dimensioni del tumore nelle mappe parametriche ottenute con limaging di perfusione sono generalmente pi piccole di quelle valutabili nelle immagini originali per la presenza di processi essudativi , ma le mappe parametriche esprimono in maniera essenziale le differenze di perfusione radiol med ( 2009 ) 114 : 871889 infectious processes , some authors advocate performing a pet or pet - ct scan 1 h after administration of fdg ( as is usually the case ) and a second scan some 24 h later [ 41 , 45 , 46 ]  . 
the rationale for the second scan is the general tendency of malignant lesions to continue accumulating fdg over time , unlike inflammatory and infectious processes that show reduced fdg uptake with time . 
with regard to nodule size , most modern pet scanners have a spatial resolution of around 6 mm , provided that the lesion is metabolically active . false negative results may nonetheless occur in the event of primary or secondary nodules with lower metabolic activity , as in the case of bronchioloalveolar carcinoma and carcinoid tumours [ 4749 ]  . 
however , meta - analyses have shown that this quantitative assessment does not improve the techniques effectiveness compared with qualitative evaluation alone . future developments : perfusion ct , computer - aided diagnosis ( cad ) , bayesian analysis and neural networks neoangiogenesis promotes tumour growth by supplying neoplastic cells with the required nutrients , and it plays a major role in metastasisation as a result of the limited integrity of the vessel wall [ 5254 ]  . 
changes in vessel volume , perfusion and vascular permeability are assessed by means of perfusion imaging , which is based on analysis of time - density curves calculated for each pixel of the section acquired with consecutive scans after injection of a bolus of iodinated contrast material [ 55 ]  . 
the introduction of 16 - detector - row ct with its fast acquisition times and improved temporal and spatial resolution in the z - axis has allowed physiological parameters to be sampled over a larger volume of tissue ( six to sections )  . some authors have observed that enhancement of peripheral lung tumours and that of the aorta occur with the same timing owing to abundant vascular supply from the bronchial arteries [ 5658 ]  . 
furthermore , lung tumours show a large interstitial space and a reduced or absent lymphatic flow , both responsible for the retention of contrast material in malignant nodules and the characteristic delay in wash - out . on parametric maps obtained with perfusion imaging , tumour size is generally smaller than assessed on the original images owing to exudation processes . 
perfusion parametric maps , however , essentially express the perfusion differences between the different portions of the nodule , providing valuable guidance for ct - guided biopsies [ 55 ]  . computer - aided diagnosis ( cad ) can be understood as an integrated computerised system capable of locating an spn , acquiring information on its dimensions , calculating its volume and mass and comparing it with a database to enable differentiation of significant nodules from artefacfra le diverse parti del nodulo , fornendo una valida guida per le biopsie tc - guidate [ 55 ]  . il concetto di diagnosi computer - assistita ( cad ) pu essere tradotto come sistema informatico integrato in grado di localizzare un nps , acquisirne informazioni dimensionali , calcolarne volume e massa e paragonarlo ad un database che permette di discriminare una nodularit significativa da unimmagine costruita / fittizia . 
questa tecnica , utilizzata inizialmente come secondo lettore per lo screening mammografico , chiaramente necessita di una sorta di autoapprendimento che la porti ad una riduzione progressiva dei falsi positivi [ 5962 ]  . 
il cad pu assumere un ruolo cruciale per eliminare numerosi fattori ostacolanti una diagnosi efficace dei nps , come la variabilit interosservatore , le caratteristiche del nps , la tecnica di acquisizione e i metodi di visualizzazione [ 63 ]  . 
dato il suo potenziale nella localizzazione delle nodularit polmonari e nel successivo follow - up , con metodi di comparazione computerizzata delle dimensioni , tale tecnica permette di migliorare la sensibilit della tc , aumentando il numero di nps diagnosticati , e conseguentemente di migliorare lefficienza clinica [ 64 ]  . 
per mezzo del cad possibile analizzare larchitettura interna del nps per differenziare nps con attenuazione uniforme da altri con attenuazione non omogenea , ma lo stesso principio potrebbe essere applicato anche dopo somministrazione di mdc per la valutazione dellenhancement nei nps stessi [ 65 , 66 ]  . 
lintegrazione dei risultati di analisi cad con sistemi di database potrebbe essere utile per assistere le attivit cliniche , nonch per fornire dati indispensabili alla ricerca ( ad esempio per studiare lassociazione tra alcune caratteristiche dei nps ed il tasso di malignit )  . la probabilit di malignit di un nps pu essere determinata utilizzando lanalisi bayesiana , sistema complesso che somma tra loro segni radiologici ( margini , dimensioni , densit , ecc . ) e clinici ( et , abitudine tabagica ) , integrandoli ed assegnando un punteggio finale [ 67 ]  . 
viene valutato il likelihood ratio ( lr ) , definito come il rapporto tra il numero di lesioni maligne che presentano una determinata caratteristica ed il numero di lesioni benigne con la stessa caratteristica [ 68 ]  . 
per esempio , un lr di 5 , 54 per quanto concerne i margini spiculati significa che su 13 nps con questo aspetto , 11 risulteranno maligni e 2 benigni . inoltre , per migliorare le capacit diagnostiche della tc nella diagnosi differenziale tra nps benigni e maligni si prevede in futuro lutilizzo di reti neurali artificiali le quali , mediante lanalisi computerizzata ( cad ) delle caratteristiche morfologiche del nps , saranno in grado di esprimere una stima delle probabilit di malignit della lesione in esame [ 69 ]  . 882 radiol med ( 2009 ) 114 : 871889 tual structures . 
this technique , initially used as a second reader for mammographic screening , clearly requires a selflearning feature to progressively reduce the rate of false positive results [ 5962 ]  . 
cad may play a crucial role in eliminating some of the variables hampering the effective diagnosis of spns , such as interobserver variability , spn characteristics , acquisition technique and viewing methods [ 63 ]  . 
given the potential of cad for detecting and following up pulmonary nodules with computerised size comparison , it can improve the sensitivity of ct by increasing the number of detected spns and consequently maximising clinical efficiency [ 64 ]  . cad can analyse the internal architecture of spns to differentiate spns with homogeneous attenuation from those with heterogeneous attenuation , but the same principle could also be applied to assess enhancement of spns after contrast medium administration [ 65 , 66 ]  . 
integration of the results from cad analyses with database systems might assist in clinical work , as well as provide indispensable data for research ( for example , to study the association between certain features of spns and malignancy rates )  . the likelihood of spn malignancy can be determined using bayesian analysis , a complex system that combines imaging ( margins , size , density , etc . ) and clinical findings ( age , smoking history ) to assign a final score [ 67 ]  . 
the system calculates the likelihood ratio ( lr ) , defined as the ratio between the number of malignant and benign lesions exhibiting a certain feature [ 68 ]  . 
for example , an lr of 5.54 for spiculated margins means that out of 13 spns exhibiting this feature , 11 are malignant and two are benign . in the future , artificial neural networks will be used to improve the diagnostic capabilities of ct in differentiating between benign and malignant spns : computerised analysis of spn morphology will provide an estimation of the likelihood of malignancy [ 69 ]  . management of the spn the pulmonary oncologists opinion the management of spns remains a subject of debate . new - generation ct scanners are able to detect increasingly small spns and the numerous lung - cancer screening programmes using low - dose ct throughout the world require the development of effective diagnostic and therapeutic protocols for managing spns . 
data from one of the main low - dose ct screening programmes , in the united states , showed that none of the detected malignancies was < 5 mm [ 70 ] , and similar results were obtained in an analogous 5 - year research project conducted at our institute [ 71 ]  . these data , which await validation by studies that are still approccio al nodulo polmonare : lopinione dello pneumo - oncologo il management del nps un argomento assai dibattuto e tuttora non completamente definito in quanto le nuove apparecchiature tc consentono di riconoscere nps di dimensioni sempre pi piccole ed i numerosi programmi di screening con tc a bassa dose , applicati ormai in tutto il mondo , richiedono lo sviluppo di percorsi diagnostico - terapeutici efficaci per la gestione del nps . 
da uno dei principali programmi di screening con tc a bassa dose , condotto negli stati uniti , emerso che nessuna delle lesioni maligne diagnosticate presentava dimensioni inferiori a 5 mm [ 70 ] e risultati sovrapponibili sono stati conseguiti al termine di 5 anni di un lavoro di ricerca analogo , condotto nel nostro istituto [ 71 ]  . 
questi dati , che peraltro andranno consolidati e supportati da studi ancora in corso , suggeriscono limprobabilit che un nps di dimensioni inferiori a 5 mm possa essere maligno : al momento vanno quindi considerati inadeguati latteggiamento aggressivo o ricontrolli troppo ravvicinati . limpatto economico e limpegno di risorse necessari per gestire un numero cospicuo di soggetti che dovrebbero essere sottoposti ad ulteriori indagini ha reso necessaria lelaborazione di linee guida , applicabili al di fuori dei progetti di screening . 
tra queste , nella tabella 1 riportiamo le raccomandazioni proposte da macmahon che , basandosi sul solo criterio dimensionale , identifica percorsi differenziati in base al rischio clinico del soggetto , da seguire in caso di riscontro occasionale di nps [ 72 ]  . il singolo criterio dimensionale non tuttavia sufficiente e deve essere associato ad altri , quale quello morfologico . 
lidentificazione di caratteristiche radiologiche tipiche di un nps benigno consente di soprassedere ad ulteriori indagini ; al contrario , laspetto francamente maligno di una lesione pu indirizzare verso un atteggiamento meno conservativo ( per esempio , fnab al posto del follow - up )  . sempre da dati riportati in programmi di screening con lutilizzo della tac spirale , si evince che la presenza di nps multipli ( > 7 ) , di piccole dimensioni , raggruppati , fortemente indicativa di un processo flogistico , piuttosto che di forme maligne . 
table 1 summarises the recommendations of macmahon et al . , who identified , on the basis of nodule size alone , different management strategies for incidentally detected spns based on the subjects clinical risk [ 72 ]  . nodule size alone is , however , insufficient and should be combined with other criteria , such as morphological appearance . 
the detection of radiological features typical of soprattutto in soggetti anziani , risultando nella quasi totalit dei casi di natura post - tubercolare . il riscontro di un nps va inoltre inserito in un contesto globale , che prevede una attenta valutazione anamnestica e clinica . 
la scoperta occasionale di un nps con diametro massimo pari a 56 mm , in un soggetto di et avanzata ed in presenza di importanti co - morbilit , essendo assai ridotta la probabilit che leventuale malattia diventi sintomatica nellarco della vita futura , giustifica lastenersi da ulteriori accertamenti . 
thus , in the presence of multiple small parenchymal nodules , follow - up at 1 month after adequate antibiotic therapy is recommended , as this will facilitate differentiation between inflammation and a lung cancer manifesting as a dominant spn surrounded by small satellite nodules [ 73 , 74 ]  . lesion site is another major criterion . 
although there is a higher incidence of lung cancer in the upper lobes , subpleural spns with scar - like appearance are often seen at the apical level , especially in elderly subjects . 
an spn with a maximum diameter of 56 mm detected incidentally in an elderly person with significant comorbid conditions is unlikely to develop into a symptomatic cancer during the subjects lifetime and therefore does not require further investigation . 
by contrast , a patient without comorbid conditions and with a solid spn > 8 mm and a high risk of malignancy requires a more aggressive diagnostic approach . management of the spn the surgeons opinion the aim of spn diagnosis and management is to promptly operate on all patients with operable malignant nodules while avoiding unnecessary thoracotomy in patients with benign disease [ 75 ]  . 
in the absence of previous radiographs demonstrating the stability of an spn , three possible decision alternatives exist : ( 1 ) serial follow - up examinations , ( 2 ) further diagnostic investigations and ( 3 ) surgery for diagnostic / therapeutic purposes . 
a rational choice among these alternatives is based on the application of bayess theorem and decision analysis principles , which in turn are based on the estimation of the likelihood of malignancy of the spn [ 76 ]  . 
clinical risk factors include the patients age , smoking history , occupational exposure to known carcinogens and history of cancer . radiological signs include nodule size , margins and site . schematically , patients with a low risk of malignancy and ct findings consistent with a malignant lesion should undergo pet - ct and / or fine - needle aspiration biopsy , whereas those with a low risk of malignancy and ct findings consistent with a benign lesion may undergo serial ct scans [ 77 ]  . 
in patients with an intermediate risk of approccio al nodulo polmonare : lopinione del chirurgo lassunto alla base dellapproccio diagnostico - terapeutico al nps rimane quello di sottoporre senza indugio a intervento chirurgico i pazienti portatori di lesioni maligne resecabili , evitando al contempo di esporre ai rischi di una toracotomia non necessaria quelli portatori di lesioni benigne [ 75 ]  . 
in assenza di dati radiografici che ci consentano di affermare con certezza la natura non evolutiva di un nps , le possibili alternative a nostra disposizione comprendono : ( 1 ) lesecuzione di controlli seriati nel tempo ; ( 2 ) lesecuzione di ulteriori indagini diagnostiche ; ( 3 ) lintervento chirurgico con finalit diagnostico - terapeutiche . 
la scelta razionale fra queste alternative basata sullapplicazione dei principi del teorema di bayes e dellanalisi decisionale , che fanno a loro volta riferimento alla stima delle probabilit che il nps abbia natura maligna [ 76 ]  . 
schematicamente , nei pazienti con basso rischio di cancro e reperto tc suggestivo di lesione maligna , appare preferibile eseguire una pet / tc e / o una fna , mentre di fronte a un reperto tc suggestivo di lesione benigna consentita lesecuzione di controlli tc seriati [ 77 ]  . 
nei pazienti con rischio intermedio di cancro e reperto tc suggestivo di lesione maligna , appare indicato eseguire una fna oppure procedere demble allintervento chirurgico , mentre nei casi di lesione tc benigna pu ancora essere consentita lesecuzione di controlli periodici . 
infine , nei pazienti con rischio elevato di cancro e reperto tc di lesione maligna , in presenza di un rischio operatorio limitato ( vedi pi avanti ) , la scelta pi adeguata appare quella di procedere allintervento chirurgico . lultimo elemento indispensabile per una scelta razionale fra le possibili alternative a nostra disposizione nellapproccio al singolo paziente portatore di un nps costituito dalla valutazione del rischio operatorio cui questi sarebbe esposto nel caso di intervento chirurgico . 
 la valutazione del rischio operatorio tiene conto di numerosi fattori , fra i quali et e condizioni generali del paziente , eventuali comorbidit ( in primo luogo , cardiovascolari ) , riserva funzionale respiratoria e tipo di exeresi che si presume necessaria per la rimozione radicale della lesione . 
poich sia la stima delle probabilit di cancro che la valutazione del rischio operatorio costituiscono , al meglio , delle scienze inesatte , ai fini di una scelta radiol med ( 2009 ) 114 : 871889 malignancy and ct findings suggestive of malignancy , fineneedle aspiration ( fna ) or surgery are warranted , whereas those with benign ct results may undergo serial ct scans . finally , in patients with a high risk of cancer and a malignant ct finding , surgery is the preferred strategy provided that the patient is not at high surgical risk ( see below )  . the last important factor to be considered for a rational choice of diagnostic strategy in the individual patient with an spn is the patients surgical risk . 
evaluation of surgical risk includes several factors , such as age and general condition , possible comorbidities ( mainly cardiovascular ) , respiratory functional reserve and the type of resection necessary to radically remove the lesion . 
as estimation of the likelihood of malignancy and assessment of surgical risk are at best both inexact sciences , the patients preferences and attitude must also be taken into account to make a clinically oriented decision . 
nor should we neglect the inevitable impact of new imaging technologies on our diagnostic and therapeutic decisions [ 78 ]  . concluding remarks although the clinician and surgeon have a different initial approach to the patient with an spn , the key points in managing these patients are nonetheless shared by a multidisciplinary team [ 78 ]  . 
there are two main points : on the one hand , a watchfulwaiting approach through follow - up after 1 year in the case of small nodules , and on the other , a standard diagnostic workup jointly established by the radiologist , pulmonary oncologist and surgeon and that may be adjusted to the individual patient . 
benign features are lesion stability for at least 2 years ( with the exception of groundglass lesions , which require longer follow - up ) and the presence of fat or benign calcification patterns . on the basis of the experience acquired during a lung cancer screening programme started in 2000 , we have devised a protocol for managing patients at intermediate to high risk ( table 2 )  . 
this protocol , which we have strongly supported , has enabled us to compromise between a watchfulwaiting clinical approach and a more aggressive surgical approach . all the above considerations should be viewed in the light of new models describing the natural history of lung cancer [ 79 ]  . 
this is based on the classical model , which considers advanced lung cancer as the more - or - less rapid evolution of an early , limited and localised but at any rate curable precursor lesion . 
 n va dimenticata linfluenza che la continua evoluzione delle tecniche radiografiche necessariamente esercita sulle nostre indicazioni diagnostico - terapeutiche [ 78 ]  . commento conclusivo da quanto emerso nei due paragrafi precedenti si evince un approccio iniziale diverso tra clinico e chirurgo nellaffrontare i problemi del paziente con nodulo polmonare . 
tuttavia i punti chiave nella gestione di questi pazienti sono comunque condivisi essendo essa multidisciplinare ad opera di una equipe da tempo costituita [ 78 ]  . due sono i punti fondamentali : da una parte un atteggiamento attendistico mediante un follow - up annuale in caso di noduli di piccole dimensioni , dallaltra lutilizzo di un percorso diagnostico standardizzato condiviso da radiologo , pneumo - oncologo e chirurgo , che possa per anche adattarsi al singolo caso . 
indipendentemente da qualsiasi considerazione clinica , il primo passo che il radiologo deve effettuare consiste nel riconoscimento dei caratteri di benignit della lesione , grazie ai quali si pu evitare di proseguire nelliter diagnostico . 
tali criteri consistono nella stabilit della lesione per almeno 2 anni ( eccetto per le lesioni a vetro smerigliato ove consigliabile un pi lungo monitoraggio ) e la presenza di grasso o di calcificazioni di tipo benigno . basandoci sullesperienza acquisita grazie al progetto uno screening iniziato nel 2000 , abbiamo elaborato un nostro protocollo che utilizziamo nei pazienti con rischio intermedio o elevato ( tabella 2 )  . 
questo percorso , da noi fortemente voluto , ha consentito di fare da trait dunion tra lapproccio clinico pi di attesa e quello chirurgico pi aggressivo . tutte queste considerazioni devono essere interpretate anche alla luce dei nuovi modelli che descrivono la storia naturale del tumore polmonare [ 79 ]  . 
si evince , infatti , che il tumore polmonare identificato allo screening in stadio precoce non sia in realt precursore dello stadio avanzato , ma un lato di una stessa medaglia ( modello bipartito )  . 
should this hypothesis be confirmed , new scenarios might emerge with regard to both screening and management of pulmonary nodules . finally , by allowing detection of increasingly small nodules , modern technology has produced excellent results , and the use of neural networks and metabolic and perfusion imaging will enhance performance with regard to the characterisation of these lesions . 
guidelines will no doubt be of assistance in managing pulmonary nodules , but they should also be flexible in that , in the opinion of clinicians , surgeons and radiologists alike , each patient requires a different approach given the numerous variables affecting the choice of diagnostic and therapeutic management strategies . mata si aprirebbero nuovi scenari sia per quanto concerne lo screening sia per lapproccio al nodulo polmonare . in conclusione , possiamo affermare che la moderna tecnologia permette di ottenere grandi risultati consentendo di identificare noduli di dimensioni sempre pi piccole ed inoltre lutilizzo di reti neurali , dellimaging metabolico e perfusionale aumenteranno le performance per quanto riguarda la tipizzazione di queste lesioni . 
fugazzola1 1department of radiology , university of insubria , ospedale di circolo , varese , italy 2department of cardiology , university of insubria , ospedale di circolo , varese , italy 3department of cardiology , ospedale di circolo , varese , italy 4department of medical physics , ospedale di circolo , varese , italy correspondence to : d . 
lumia , university of insubria , ospedale di circolo , viale borri 57 , 21100 varese , italy , tel : + 39 - 0332 - 278763 , fax : + 39 - 0332 - 393535 , e - mail : domenicolumia@gmail.com received : 23 september 2008 / accepted : 12 december 2008 / published online : 1 july 2009 springer - verlag 2009 abstract purpose . 
we retrospectively examined the coronary mdct studies of 89 patients ( 73 males , 16 females , average age 62.5 years , range 3179 ) referred for suspected coronary artery disease . 
the lateral cardiac vein was visualised in 56 / 84 patients ( 67% ) and the posterior cardiac vein in 63 / 84 patients ( 75% ) , never both missing . 
 along the postero - lateral wall of the left ventricle , only one branch was present in 44 cases , two branches in 21 cases and three or more branches in 19 / 84 cases ( 22% )  . evaluation of the maximum diameter revealed that the lateral vein was dominant over the posterior vein in 20 / 40 cases . 
sono stati valutati retrospettivamente 89 pazienti consecutivi ( 73 maschi e 16 femmine , et media 62 , 5 anni , range di et 3179 ) , sottoposti ad angiotcms per sospetta patologia coronarica . 
la vena cardiaca laterale stata visualizzata in 56 / 84 casi ( 67% ) , mentre la vena cardiaca posteriore in 63 / 84 casi ( 75% ) ; in nessun caso mancavano entrambe . 
complessivamente in prossimit della parete postero - laterale del ventricolo sinistro stato possibile visualizzare un solo ramo in 44 casi , due rami in 21 casi , tre o pi rami in 19 casi . 
nei pazienti che presentavano due rami per la parete posterolaterale del ventricolo sinistro , valutando il calibro massimo della vena , la vena laterale stata considerata dominante sulla posteriore in 20 / 40 casi . 
pertanto , questa tecnica di imaging potrebbe essere proposta nel planning dei pazienti da sottoporre alla crt . parole chiave scompenso cardiaco terapia di resincronizzazione cardiaca tcms vene cardiache seno coronarico introduction introduzione since the launch of the first single - slice scanner , computed tomography ( ct ) has undergone incessant technological advances that have rapidly broadened its fields of use [ 1 , 2 ]  . the advent of multidetector - row systems has made ct study of the heart possible , despite the hearts involuntary motion and complex anatomy , which have been the main hurdles for noninvasive cardiac imaging [ 35 ]  . 
the use of cardiac synchronisation techniques and pharmacological agents for slowing the heart rate have in fact enabled the reduction of pulsatility artefacts and the attainment of submillimetre volumetric data sets of good diagnostic quality in any phase of the cardiac cycle [ 2 , 4 ]  . 
over the years , a number of non - coronary applications of cardiac ct have been developed , such as the study of cardiac masses ( thrombotic or neoplastic ) , evaluation of the left atrium and pulmonary veins , the study of myocardial function and imaging of cardiac veins [ 3 , 4 , 68 ]  . interest in the study of the coronary venous system deals with the diffusion of an innovative approach to the treatment of heart failure : cardiac resynchronisation therapy ( crt ) [ 9 , 10 ]  . 
the use of crt is based on clinical evidence that the deterioration of ventricular function in patients with heart failure is to a large extent related to the onset of an intramyocardial conduction disorder [ 11 , 12 ]  . 
crt aims to reduce symptoms and slow the progression of heart failure by resynchronising the activity of the left ventricle with those of the right ventricle and atriuin order to do so , a pacing lead for the left ventricle , in addition to leads for the right atrium and ventricle , needs to be implanted in a vein of the coronary venous system , preferably on the posterolateral wall of the left ventricle [ 913 ]  . the use of intravascular venous access offers a number of advantages over the minimally invasive thoracotomy approach [ 1214 ] because it eliminates the need for surgery and general anaesthesia in patients who already present haemodynamic instability . 
crt can nonetheless fail due to the marked anatomical variability ( number and course ) of the cardiac veins and the intrinsic difficulty in catheterising the coronary sinus [ 9 , 1214 ]  . the aim of our study was to evaluate the use of multidetector - row computed tomography ( mdct ) in assessing the sin dallintroduzione sul mercato del primo scanner a singolo strato , la tomografia computerizzata ( tc ) ha mostrato un rapido ed incessante sviluppo tecnologico che ne ha ampliato rapidamente i campi di utilizzo [ 1 , 2 ]  . 
la comparsa dei sistemi multidetettore ha consentito di estendere lo studio tc al cuore , nonostante da sempre la sua motilit involontaria e la sua complessa anatomia abbiano rappresentato i principali ostacoli allimaging non invasivo [ 35 ]  . 
lutilizzo delle tecniche di cardiosincronizzazione e limpiego della bradicardizzazione farmacologica hanno reso possibile infatti , la riduzione degli artefatti da pulsatilit , consentendo di ottenere dataset volumetrici submillimetrici di buona qualit diagnostica in qualsiasi fase del ciclo cardiaco [ 2 , 4 ]  . 
negli anni si sono sviluppate diverse applicazioni non coronariche della cardio - tc , come lo studio delle masse cardiache ( trombotiche o neoplastiche ) , la valutazione dellatrio sinistro e delle vene polmonari , lo studio della funzionalit miocardica ed infine limaging delle vene cardiache [ 3 , 4 , 68 ]  . linteresse per lo studio del sistema venoso coronarico legato al diffondersi di un approccio innovativo al trattamento dello scompenso cardiaco : la terapia di resincronizzazione cardiaca ( crt ) [ 9 , 10 ]  . 
il presupposto alluso della crt si basa sullevidenza clinica che il deterioramento della funzione ventricolare in pazienti con scompenso cardiaco in gran parte legato allinstaurarsi di disturbi della conduzione intramiocardica [ 11 , 12 ]  . 
la crt si pone quindi lobiettivo di migliorare i sintomi e rallentare la progressione dello scompenso attraverso la resincronizzazione dellattivit del ventricolo sinistro con quella del ventricolo e dellatrio destro ; per ottenere questo risultato necessario posizionare un elettrodo stimolatore per il ventricolo sinistro in aggiunta a quelli per latrio ed il ventricolo destro , in una vena del sistema venoso coronarico , preferibilmente in corrispondenza della parete postero - laterale del ventricolo sinistro [ 913 ]  . lutilizzo di un accesso endovascolare per via venosa presenta numerosi vantaggi rispetto a quello mediante mini - toracotomia [ 1214 ] , perch elimina la necessit di ricorrere ad un intervento chirurgico , con limpiego dellanestesia generale , in pazienti che gi presentano un radiol med ( 2009 ) 114 : 837851 anatomical variants of the coronary venous system in order to identify the most appropriate veins for placement of the pacing lead required for crt . materials and methods we retrospectively evaluated 89 consecutive patients ( 73 males and 16 females , mean age 62.5 years , range 3179 years ) who underwent mdct angiography for suspected coronary artery disease ( cad ) from september 2007 to may 2008 ( table 1 )  . 
patients with a heart rate > 70 bpm received a 100 mg oral dose of metoprolol 6090 min before the examination in addition to 0.6 mg of nitroglycerine administered sublingually 5 min prior to the beginning of the scan . 
exclusion criteria included a heart rate > 70 bpm even after pharmacological treatment or in patients with contraindications to beta - blocker administration , an inability to maintain the breath - hold during the scan , kidney failure ( creatinine > 2 mg / dl ) , heart and / or respiratory failure , refractory arrhythmia , pregnancy or a known hypersensitivity to iodinated contrast agents . all examinations were performed with a 64 - detectorrow multislice scanner ( aquilion 64 , toshiba medical systems corporation , otawara , japan ) with retrospective cardiac gating . 
among selected , two were excluded because of inadequate electrocardiography ( ecg ) gating due to an increase in the heart rate after contrast agent administration , one because of the patients precario equilibrio emodinamico . 
la crt comunque pu risultare talvolta inefficace a causa dellampia variabilit anatomica ( numero e decorso ) delle vene cardiache e delle difficolt intrinseche nelle procedure di cateterizzazione del seno coronarico [ 9 , 1214 ]  . scopo del nostro lavoro valutare lutilit della tomografia computerizzata multistrato ( tcms ) nellidentificazione delle varianti anatomiche del sistema venoso coronarico al fine di riconoscere quelle ritenute pi idonee per limpianto dellelettrocatetere necessario per la crt . materiali e metodi sono stati valutati retrospettivamente 89 pazienti consecutivi ( 73 maschi e 16 femmine , et media 62 , 5 anni , range di et 3179 ) , sottoposti ad angio - tcms per sospetta patologia coronarica ( cad ) nel periodo compreso tra settembre 2007 e maggio 2008 ( tabella 1 )  . 
nei pazienti con frequenza cardiaca > 70 bpm stata praticata una bradicardizzazione farmacologica con 100 mg di metoprololo per os , 6090 min prima dellesecuzione dellesame , in aggiunta a 0 , 6 mg di nitroglicerina per via sublinguale somministrata 5 minuti prima dellinizio della scansione . 
i criteri di esclusione dallo studio comprendevano una frequenza cardiaca superiore ai 70 bpm anche dopo trattamento farmacologico o in concomitanza di controindicazioni alla somministrazione di beta - bloccanti , lincapacit di mantenere unadeguata apnea inspiratoria durante la scansione , la presenza di insufficienza renale ( creatinina > 2 mg / dl ) , insufficienza cardiaca e / o respiratoria , aritmie cardiache non controllate dalla terapia , stato di gravidanza , nota ipersensibilit ai mezzi di contrasto iodati . tutti gli esami sono stati eseguiti con apparecchiatura multi - strato a 64 file di detettori ( aquilion 64 , toshiba medical systems corporation , otawara , giappone ) , mediante limpiego di sincronizzazione cardiaca con tecnica retrospettiva . 
lenhancement vascolare stato ottenuto mediante linfusione di un bolo di 90100 ml di mezzo di contrasto ( mdc ) iodato non ionico ( iomeprolo , iomeron 400 mgi / ml , bracco , milano , italia ) con velocit di flusso di 45 ml / s , seguito da bolo di 40 ml di soluzione fisiologica a 45 ml / s , utilizzando unagocannula da 18 gauge inserita in una vena antecubitale del braccio ed un iniettore automatico a doppia testa ( stellant d , medrad , pa , usa )  . 
the lateral cardiac vein ( lcv ) was visualised in 56 / 84 cases ( 67% ) and the posterior cardiac vein ( pcv ) in 63 / 84 cases ( 75% ) ; failure to visualise both veins occurred in no cases . 
the overall vein visualization along the postero - lateral wall of the left ventricle resulted as follows : one branch only in 44 / 84 cases ( 52% ) , two branches in 21 / 84 cases ( 25% ) and three or more branches in 19 / 84 cases ( 22% )  . 
near the lm bifurcation , it opens into the gcv , which lies in the left atrioventricular groove close to the left circumflex artery and in turn opens into the cs . 
 cs , coronary sinus ; gcv , great cardiac vein ; aiv , anterior interventricular vein ; mcv , middle cardiac vein ; lcv , lateral ( also marginal ) cardiac vein ; pcv , posterior cardiac vein ; scv , small cardiac vein ; lm , left main coronary artery ; d1 , first diagonal ; mo , obtuse marginal . 
 cs , seno coronario ; gcv , grande vena cardiaca ; aiv , vena inter - ventricolare anteriore ; mcv , vena cardiaca media ; lcv , vena cardiaca laterale ; pcv , vena cardiaca posteriore ; scv , piccola vena cardiaca ; lm , tronco comune ; d1 , primo diagonale ; mo , marginale ottuso . the distance between the postero - lateral veins and the cs was 62.5132.5 mm for the pcv and 58.6632.0 mm for the lcv . 
the mean diameters of the other tributaries of the cs were as follows : aiv 3.2 mm , mcv 4.6 mm , lcv 2.6 mm , pcv 3.4 mm and scv 2.2 mm ( table 3 )  . therefore , in 79 of the 84 patients ( 94% ) who underwent mdct coronary angiography for suspected cad , at least one venous branch with good diameter and regular course was identified along the postero - lateral wall of the left ventricle . 
in 5 / 84 patients ( 6% ) , the postero - lateral branch had a short course ( < 12 mm )  . una buona visualizzazione del circolo venoso coronarico . 
la vena cardiaca laterale ( lcv ) stata visualizzata in 56 / 84 casi ( 67% ) mentre la vena cardiaca posteriore ( pcv ) in 63 / 84 casi ( 75% ) ; in nessun caso mancavano entrambe . 
complessivamente in prossimit della parete postero - laterale del ventricolo sinistro stato possibile visualizzare un solo ramo in 44 / 84 casi ( 52% ) , due rami in 21 / 84 casi ( 25% ) , tre o pi rami in 19 / 84 casi ( 22% ) ; nei pazienti che presentavano due rami per la parete posterolaterale del ventricolo sinistro , valutando il calibro massimo della vena , la lcv stata considerata dominante sulla vena posteriore in 20 / 40 casi . 
2 multiplanar reconstruction ( mpr ) of the coronary venous systethe image displays the coronary sinus ( cs ) , the great cardiac vein ( gcv ) , the anterior interventricular vein ( aiv ) and the middle cardiac vein ( mcv )  . 
la figura mostra il seno coronarico ( cs ) , la grande vena cardiaca ( gcv ) , la vena interventricolare anteriore ( aiv ) e la vena cardiaca media ( mcv )  . 
cs , seno coronario ; gcv , grande vena cardiaca ; aiv , vena interventricolare anteriore ; mcv , vena cardiaca media ; lcv , vena cardiaca laterale ; pcv , vena cardiaca posteriore . 844 radiol med ( 2009 ) 114 : 837851 fig . 
angolo di confluenza inferiore a 90 , con possibilit di un facile cateterismo ( a ) ; angolo di confluenza superiore a 90 , che potrebbe comportare delle difficolt durante limpianto di elettrodo stimolatore per crt ( b )  . discussion heart failure is one of the major health problems of industrialised nations , partly as a result of the ageing population . pharmacological therapy alone is unable to produce la distanza delle vene della parete postero - laterale dal cs risultata 62 , 5132 , 5 cm per la pcv e di 58 , 6632 cm per la lcv . 
langolo di raccordo dei rami venosi della parete postero - laterale apparso inferiore a 90 in 59 pazienti ( 93 , 7% ) in corrispondenza della pcv e in 53 pazienti ( 94 , 6% ) in corrispondenza della lcv , superiore a 90 in 4 pazienti ( 6 , 3% ) in corrispondenza della pcv e in 3 pazienti ( 5 , 4% ) in corrispondenza della lcv . 
quindi in 79 degli 84 pazienti ( 94% ) sottoposti ad angio - tcms coronarica per sospetta cad , stato possibile visualizzare almeno un ramo venoso di buon calibro e decorso regolare in corrispondenza della parete posterolaterale del ventricolo sinistro ; in 5 / 84 pazienti ( 6% ) il ramo venoso postero - laterale visualizzato presentava breve decorso ( < 12 mm )  . discussione lo scompenso cardiaco costituisce uno dei maggiori problemi sanitari dei paesi industrializzati , anche in relazione al progressivo aumento dellet anagrafica della popolazione . 
la sola terapia farmacologica non sempre consente di raggiungere risultati soddisfacenti , mentre lassociazione di pi farmaci pu risultare mal tollerata dai pazienti pi anziani ; per tale motivo sono state sviluppate negli anni , terapie alternative [ 11 , 14 ]  . la crt rappresenta un approccio innovativo al paziente affetto da insufficienza cardiaca cronica [ 9 , 10 , 12 ]  . 
la crt agendo sulla meccanica cardiaca mediante limpianto di un pacemaker biventricolare , migliora lo stato clinico , la qualit della vita e la prognosi dei pazienti affetti da insufficienza cardiaca cronica avanzata associata ad incremento della durata del qrs , ripristinando una corretta sincronizzazione dellattivit di atri e ventricoli . 
 per il posizionamento di tali elettrodi , un approccio endovascolare per via venosa da preferire a quello chirurgico mediante mini - toracotomia , per gli ovvi vantaggi derivanti dallevitare ad un paziente in precarie condizioni cardiocircolatorie sia lanestesia generale che il trauma chirurgico . 
this has led to the development of alternative treatments [ 11 , 14 ]  . crt is an innovative approach to the patient affected by chronic heart failure [ 9 , 10 , 12 ]  . 
the technique involves implantation of three pacing leads to stimulate the right atrium , the right ventricle and the left ventricle [ 9 , 1518 ]  . for lead implantation , an intravascular approach with venous access is preferable to minimally invasive thoracic surgery because of the obvious advantage of sparing general anaesthesia and surgical trauma for patients with unstable haemodynamic status . 
the pacing leads destined for the right heart chambers can be positioned through a central venous catheter , generally with access from the left subclavian vestimulation of the left ventricle is performed with a usually bipolar pacing lead specially developed for placement in a cardiac vein , which is reached through catheterisation of the cs . the cs is a large vein that runs across the diaphragmatic sviluppato per limpianto in una vena cardiaca , che viene raggiunta mediante cateterizzazione del cs . 
il cs riceve inferiormente la pcv , che origina dalla parete posteriore del ventricolo stesso , e superiormente la vena obliqua dellatrio sinistro ( o di marshall ) , la quale discende medialmente dalla parete posteriore di tale atrio [ 1517 ]  . 
a complete study requires at least two fluoroscopic views in order to clearly visualise the anatomy , the angulation and the course of each vein [ 16 ]  . the limitations of this technique include invasiveness , examination duration , a not always optimal depiction of the cardiac veins , an inability to visualise both the vessels and the cardiac wall at the same time , a need for large amounts of contrast agent ( in some cases up to 500 ml per examination ) and the impossibility to selectively catheterise the cs and its tributaries in 4%5% of patients [ 10 , 16 , 2022 ]  . in recent years , mdct has been taking on an increasingly important role as a noninvasive modality for studying the cardiac veins , thanks to its high spatial and temporal resolution , cardiac gating and sophisticated image postprocessing and reconstruction techniques , which are able to produce detailed visualisation of the cardiac venous system [ 2027 ]  . trans - venoso ed impianto dellelettrocatetere in corrispondenza della regione mediale o basale della parete libera del ventricolo di sinistra , in una vena laterale o postero - laterale , zona del ventricolo sinistro che risulta essere quella maggiormente colpita dal processo di desincronizzazione [ 13 ]  . non tutti i pazienti risultano candidabili alla crt , a causa dellassenza di una vena cardiaca di calibro o lunghezza adeguata ad alloggiare lelettrocatetere o per la presenza di ostacoli alla procedura di cateterizzazione . 
la possibilit di ottenere una visualizzazione dettagliata del sistema venoso cardiaco risulta perci preziosa nella pianificazione della procedura di impianto dei pacemaker biventricolari [ 19 ]  . langiografia venosa retrograda con pallone occludente , attualmente rappresenta la metodica convenzionale di studio delle vene coronariche [ 9 , 20 ] : viene ottenuta mediante iniezione di mdc durante cateterizzazione selettiva del seno coronarico e delle vene tributarie . 
i limiti di questa metodica sono da ricercare nellinvasivit della procedura , nella durata dellesame , nella visualizzazione non sempre ottimale delle vene cardiache , nellimpossibilit di visualizzare contemporaneamente i vasi e la parete cardiaca , nella necessit di impiegare grandi quantit di mdc ( in alcuni casi fino a 500 ml per esame ) ed infine nellimpossibilit , riscontrata nel 4%5% dei pazienti , di procedere al cateterismo selettivo del seno coronarico e delle vene tributarie [ 10 , 16 , 2022 ]  . in questi ultimi anni la tcms , grazie allelevata risoluzione spaziale e temporale , alle tecniche di gating cardiaco , alle sofisticate capacit di processazione e ricostruzione delle immagini , che consentono di ottenere una visualizzazione dettagliata dellanatomia del sistema venoso coronarico , si sta proponendo come metodica non invasiva per lo studio delle vene cardiache [ 2027 ]  . 
5a - f anatomia normale e varianti del sistema venoso del seno coronarico ( tcms ricostruzioni 3dvr ) : anatomia normale ( a ) , sc bifido ( b ) , sc high riding ( c ) , sc varicoide ( d ) , sc filiforme ( e ) , sc windsock o ectasico ( f )  . 
the presence of anatomical conditions unsuitable for correct placement of the bipolar lead needs to be ruled out , such as accessory valve leaflets ( thebesian or vieussens ) in the cs , certain anatomical configurations of the cs ( bifid , high riding , varicoid , filiform , windsock or ectatic , diverticular , atresic ) ( fig . 5af ) , a left circumflex artery crossing the gcv and causing external compression , and unfavourable angles between the gcv non favorevoli ( 90 ) ad unagevole cateterizzazione . 
 lintento del nostro lavoro non quello di analizzare laccuratezza diagnostica della tcms nei confronti della venografia , ma di far risaltare i vantaggi che possono derivare dallutilizzo routinario della tcms nella valutazione del sistema venoso coronarico . 
in letteratura sono riportate percentuali di visualizzazione dei diversi segmenti venosi coronarici , variabili in relazione al calibro dei vasi considerati : il cs stato visualizzato nel 98% dei casi , la gcv nel 99% dei casi , la aiv nel 99% dei casi , la mcv nel 98% dei casi , la pvc nel 89% dei casi , la lcv nel 73% dei casi , la pvc nel 14% dei casi . 
il diametro medio del cs 848 radiol med ( 2009 ) 114 : 837851 postero - lateral veins and the gcv ( 90 )  . the aim of our study was not to analyse the diagnostic accuracy of mdct compared with venography but , rather , to highlight the advantages of the routine use of mdct in the evaluation of the coronary venous syste the literature reports detection rates of the various venous segments that vary in relation to the diameter of the vessels considered . 
possible explanations for this discrepancy include nonoptimal timing of contrast enhancement , much faster scan times with respect to the earlier multislice scanners ( 48and 16 slices ) and interobserver variability in the linear measurements of vessel diameter . even though postprocessing of new - generation angiographic images makes possible the creation of 3d volume rendering ( vr ) reconstructions immediately after retrograde venography [ 28 ] and linear measurements on 2d images , the vr and mpr images created from mdct acquisitions with isotropic voxels may provide additional advantages . 
in addition to clearly depicting the course of the vessel in relation to the left ventricular free wall and the left circumflex artery [ 28 ] , these reconstructions offer the possibility of evaluating the anatomy of the mitral valve and enable precise measurement of the diameter , or better of the section , of the cs and its branches . 
 the presence of reduced diameters , short vessels or sharp vascular angles can in fact make difficult or even impossible the insertion of the bipolar pacing [ 10 , 16 , 2123 ]  . normally the anatomy of the cardiac veins is not optimally visualised with the contrast - enhancement protocol used for the coronary arteries , with the exception of the juxta - atrial portions ( cs and mcv )  . 
this occurs because the veins situated more cranially , when the acquisitions are performed in the cranio - caudal direction , show valid contrast enhancement towards the end of the scan [ 1 ]  . undoubtedly , the visibility of the cardiac veins on the postero - lateral wall of the left ventricle could be improved by performing the scan in the caudo - cranial direction or by using an additional delay of 1215 s after reaching the enhancement threshold in the ascending aorta ( baseline hu + 100 hu ) [ 1 , 2 , 17 ]  . 
althrough our experience is still limited , this bolus - tracking method , which does not appear to be reported in the literature , risultato 13 , 2 mm , quello della gcv 6 , 8 m i diametri medi delle altre vene tributarie del seno coronarico sono risultati rispettivamente : aiv 3 , 9 mm , mcv 5 , 2 mm , pvc 3 , 9 mm e lcv 3 , 7 mm [ 2027 ]  . 
i dati riguardanti la percentuale di visualizzazione delle vene cardiache riportati in letteratura sono in buona parte sovrapponibili ai dati estrapolati dalla nostra esperienza fatta eccezione per la visualizzazione della lcv ( 73% vs 67% letteratura vs nostra casistica ) ed in maniera ancora pi significativa della pvc ( 89% vs 75% )  . 
possibile che il motivo di tali discrepanze risieda in un timing contrastografico non ottimizzato , in tempi di scansione estremamente pi veloci rispetto ai primi scanner multi - slice ( 4 - 8 - 16 strati ) ed infine nella variabilit inter - osservatore delle misure lineari del diametro vasale . 
 nonostante le implementazioni degli angiografi di nuova generazione permettano di creare in post - processing immagini 3d volume rendering ( vr ) subito dopo lesecuzione della venografia retrograda [ 28 ] e di eseguire misurazioni lineari su immagini bidimensionali , le ricostruzioni vr e mpr ricavate da acquisizioni tcms con voxel isotropico , possono fornire ulteriori vantaggi . 
queste ricostruzioni , oltre che mettere bene in evidenza il decorso dei vasi in relazione alla parete libera del ventricolo di sinistra e allarteria circonflessa [ 28 ] offrono la possibilit di valutare lanatomia dellanello mitralico e consentono di misurare in maniera precisa il diametro , o ancor meglio la sezione , del seno coronarico e dei suoi rami ; la presenza di calibri ridotti , di vasi a breve decorso o di brusche angolazioni vasali , possono infatti rendere difficoltoso , o addirittura impossibile , linserimento dellelettrocatetere bipolare durante la procedura di crt [ 10 , 16 , 2123 ]  . 
 normalmente lanatomia delle vene cardiache non viene visualizzata in maniera ottimale applicando il protocollo di studio contrastografico utilizzato per le arterie coronarie , ad eccezione delle porzioni iuxta - atriali ( seno coronarico e vena cardiaca media )  . 
questo avviene perch le vene situate pi cranialmente , quando lacquisizione viene effettuata in senso cranio - caudale , presentano un valido contrast enhancement verso il termine della scansione [ 1 ]  . 
 sicuramente effettuare lacquisizione della scansione in direzione caudo - craniale o lutilizzo di un ritardo aggiuntivo di 1215 secondi dal raggiungimento della soglia di attenuazione in aorta ascendente [ hu basale + 100 hu ] , consente di migliorare la visibilit delle vene cardiache lungo la parete postero - laterale del ventricolo sinistro [ 1 , 2 , 17 ]  . 
un ulteriore accorgimento , attualmente oggetto di studio presso il nostro centro , lutilizzo contemporaneo di due regioni di interesse ( roi ) in corrispondenza del seno coronarico e dellaorta discendente ; questa modalit di bolus tracking , che non ci risulta essere mai stata descritta , nella nostra casistica seppure ancor limitata , permetterebbe di ridurre al minimo la criticit del timing contrastografico del sistema venoso coronarico , specie in pazienti che a causa della radiol med ( 2009 ) 114 : 837851 could minimise the problem of contrast enhancement timing of the coronary venous system , particularly in patients presenting a severely depressed ejection fraction ( < 35% , nyha 34 ) due to desynchronicastion of the left ventricle . the limitations of our study include the use of a nonoptimal protocol for cardiac veins ( retrospective evaluation in patients with suspected cad ) , clinical heterogeneity of patients undergoing mdct with respect to those referred for crt and absence of a direct assessment of the effective clinical advantages of the use of mdct ( reduced procedure times , fewer unsuccessful attempts and lower overall dose delivered to the patient )  . finally , it should be noted that the study of the coronary veins with ecg - gated mdct angiography in the planning of crt cannot be correctly performed in the presence of a high heart rate ( > 70 bpm ) , frank arrhythmias and / or inability to maintain the breath - hold for an adequate duration ( around 10 s )  . 
in fact patients with severe heart failure could not tolerate supine position or present an absolute contraindication to pharmacological control of the heart rate [ 1 , 2 ]  . increased exposure to ionising radiation of the patient referred for crt should not be overlooked , as in addition to undergoing venography , the patient needs to undergo an mdct examination of the coronary venous systems for crt planning ( effective dose varying from 14 to 24 msv ) [ 1 , 16 ]  . 
of course the use and further development of dose modulation systems , such as ecg pulsing , to prospectively adjust the tube current intensity in order to deliver the maximum current only during the midto end - diastolic window will help reduce the dose delivered during this examination ( 1014 msv ) [ 2932 ]  . desincronizzazione del ventricolo sinistro presentano una frazione di eiezione gravemente despressa < 35% ( nyha 3 - 4 )  . 
 non inoltre possibile tralasciare lincremento di esposizione alle radiazioni ionizzanti del paziente candidato a crt , che oltre a doversi sottoporre a venografia , debba eseguire una tcms del sistema venoso coronarico durante il planning ( dose efficace variabile tra 1424 msv ) [ 1 , 16 ]  . certo che lutilizzo e lulteriore sviluppo di sistemi di modulazione , come lecg - pulsing , in grado di regolare lintensit di corrente del tubo radiogeno in modalit prospettica , sfruttando la massima corrente solo in corrispondenza della finestra temporale mesoe tele - diastolica , consentiranno di ridurre la dose erogata durante lesame ( 1014 msv ) [ 2932 ]  . conclusions introduction of the mdct study of cardiac veins as a preliminary examination in patients referred for crt may reduce procedure times , the number of unsuccessful procedures , the amount of contrast agent used and the overall dose delivered to the patient and operators during the venographic study . 
the use of a dedicated contrast enhancement protocol could further improve the diagnostic confidence of mdct , which already today as our study shows provides good visualisation of the coronary veins and can accurately define anatomical variants , as well as the course and angulation of the vessel in relation to the free wall of the left ventricle . 
 conclusioni lintroduzione dello studio delle vene cardiache mediante tcms come indagine preliminare nei pazienti da sottoporre a crt , potrebbe consentire di ridurre i tempi della procedura , il numero degli insuccessi , la quantit di mdc impiegata e la dose complessiva erogata a paziente ed operatori durante lo studio venografico . 
algarotti 8 , 00137 rome , italy , tel . : + 39 - 349 - 1946942 , fax : + 39 - 06 - 8276895 , e - mail : stepieri@excite.it received : 4 september 2008 / accepted : 12 november 2008 / published online : 25 june 2009 springer - verlag 2009 abstract purpose . 
between january 1997 and december 2005 , 23 patients ( 14 men and nine women ; age range 2148 years ) , after a previous study with computed tomography ( ct ) and / or magnetic resonance ( mr ) imaging , underwent percutaneous drainage of a tuberculous fluid collection in the psoas muscles . 
tra gennaio 1997 e dicembre 2005 , 23 pazienti ( 14 uomini e 9 donne ) , di et compresa tra i 21 ed i 48 anni , precedentemente studiati con tc e / o rm , sono stati sottoposti a drenaggio percutaneo di una raccolta fluida , di origine tubercolare , localizzata nei muscoli psoas . 
il massimo diametro trasverso stato di 7 cm , mentre quello longitudinale stato di 14 cil posizionamento del catetere di drenaggio sempre avvenuto con successo , con una permanenza del catetere di 536 giorni ( media 18 , 4 giorni ) ; la regressione della sintomatologia avvenuta gi allatto dellevacuazione della raccolta fluida . 
gli ascessi dei muscoli psoas rappresentano una seria complicanza nella localizzazione ossea della radiol med ( 2009 ) 114 : 984995 drainage catheter requires daily monitoring to identify when it can be safely removed without risk of recurrence . keywords tuberculosis psoas abscess percutaneous drainage tubercolosi , trattabili efficacemente con il drenaggio percutaneo , capace di risolvere subito la sintomatologia dolorosa . 
il catetere di drenaggio necessita di unassistenza giornaliera , per poter decidere il momento pi idoneo alla sua rimozione , senza andare incontro a recidive . parole chiave tubercolosi ascesso muscolo psoas drenaggio percutaneo introduction introduzione despite the systematic use of targeted therapy and serial laboratory testing , tuberculosis continues to be a major cause of morbidity and mortality , affecting more than 30 million people worldwide , especially in developing countries where hygienic conditions are poor [ 13 ]  . 
although past prevention and treatment strategies decreased its frequency in western countries [ 2 ] , recent trends in alcohol and drug abuse , the rising numbers of hiv and aids cases [ 4 ] and waves of migration from the third world have led to a resurgence of the disease in developed countries as well [ 5 ]  . in addition to primary and secondary pulmonary manifestations , tuberculosis may also affect the skeletal system , which is the most frequent extrapulmonary localisation [ 3 ]  . 
in particular , the thoracic and lumbar vertebral bodies and intervertebral discs are common sites of involvement , and the formation of paraspinal tuberculous abscesses is seen in approximately 50%75% of cases of bone tuberculosis [ 1 , 3 ]  . the clinical diagnosis of tuberculous abscesses is not easy , as the symptoms have indolent onset and gradual progression owing to the slow course of tuberculosis . 
diagnostic suspicion can be confirmed with computed tomography ( ct ) [ 6 ] or magnetic resonance ( mr ) imaging [ 7 , 8 ] , as both diagnostic modalities are able to document changes in the margins , size and density of the psoas muscles before and after contrast administration . whereas conservative management ( analgesics , immobilisation , external orthoses ) was the mainstay of treatment in the past , with surgery reserved for patients not responding to conservative treatment [ 9 ] and with disease in other anatomical regions [ 10 ] , today , percutaneous drainage is increasingly being used to treat the fluid collections [ 4 , 9 , 11 ]  . 
 la tubercolosi , nonostante limpiego sistematico di una terapia mirata e i controlli seriati di laboratorio , continua ad essere una importante causa di morbilit e mortalit e a colpire oltre 30 milioni dindividui nel mondo , specie nelle nazioni in via di sviluppo , caratterizzate da scarse condizioni igieniche [ 13 ]  . 
pur essendo pi rara nelle nazioni occidentali , grazie a politiche di prevenzione e cura , attuate in passato [ 2 ] , recentemente , labuso di alcool e droga , laumento dei casi di hiv e aids [ 4 ] e le notevoli ondate migratorie dal terzo mondo , hanno fatto registrare un aumento del numero di casi annui anche nelle nazioni pi progredite [ 5 ]  . oltre alle diverse manifestazioni polmonari , espressione della localizzazione primaria e secondaria della malattia , la tubercolosi in grado di coinvolgere anche il sistema scheletrico : questo infatti rappresenta la localizzazione extrapolmonare pi frequente [ 3 ]  . 
in particolare risultano colpiti i corpi vertebrali dorso lombari e i dischi intervertebrali ; inoltre , la formazione degli ascessi tubercolari paraspinali osservata in circa il 50%75% dei casi di tubercolosi ossea [ 1 , 3 ]  . la diagnosi clinica degli ascessi non agevole : i sintomi sono subdoli , ad esordio ritardato rispetto allinsorgenza della malattia : ci per la lenta evoluzione della tubercolosi ; molto spesso a richiamare lattenzione possono essere un dolore lombare inspiegabile o la comparsa di disturbi motori degli arti inferiori [ 5 ]  . 
al giorno doggi , la conferma del sospetto diagnostico avviene sia con la tc [ 6 ] , che con la rm [ 7 , 8 ] : entrambe le metodiche diagnostiche sono in grado di documentare le variazioni di margini , dimensioni e densit dei muscoli psoas , prima e dopo somministrazione di mezzo di contrasto . se le modalit conservative ( farmacoterapia basata sugli antidolorifici , immobilizzazione , applicazione esterna di tutori ) rappresentavano , nel recente passato , i capisaldi delle opzioni terapeutiche a disposizione del clinico , riservando alla chirurgia quei pazienti dove non era stata raggiunta una risoluzione del quadro clinico [ 9 ] , come per altre regioni anatomiche [ 10 ] , attualmente si fa sempre pi 986 materials and methods over a period of 7 years , 62 patients with psoas - muscle fluid collections were treated with percutaneous drainage at our centre . 
the patients , 14 men and nine women , age 2148 ( mean 39 ) years , had been admitted to different respiratory disease divisions of our hospital because of the gradual onset of nonspecific symptoms such as worsening fatigue , persistent mild evening fever , productive cough at times with blood - tinged sputum , and pain in the thoracic spine in nine patients and in the lumbar spine in 14 . 
pain had been partially controlled with analgesics and in three cases even with the occasional addition of opiates . diagnostic tests revealed the presence of a lung lesion on plain chest radiography or on subsequent ct scan ( 16 active lesions , seven sequelae ) , as well as associated findings at the level of the spine and psoas muscles . 
ct was performed on 16 patients with a conventional ct scanner ( rhota ctw 950 sr , esaote biomedica , genoa , italy ) and a protocol consisting of a study of the spine with a slice thickness of 5 mm before and after contrast administration ( optiray 300 , tyco healthcare spa , milan , italy )  . 
abscesses were considered appropriate for percutaneous drainage if they met the following criteria [ 7 ] : abscesses associated with spondylodiscitis , larger than 3 cm in diameter , causing pain refractory to systemic antituberculous chemotherapy , and associated with altered laboratory parameters ( neutrophil leukocytosis , elevated erythrocyte sedimentation rate )  . 
 in letteratura sono presenti pochi articoli che descrivono lapplicazione sistematica di questa procedura , tra laltro su un numero limitato di pazienti ; riportiamo la nostra esperienza nella gestione percutanea di tali quadri clinici , nel breve e medio termine , maturata su un discreto gruppo di pazienti . 
 materiali e metodi nellarco di 7 anni , nel nostro servizio sono stati complessivamente sottoposti a trattamento percutaneo 62 pazienti che presentavano una raccolta fluida allinterno dei muscoli psoas : solo 23 sono risultati di natura tubercolare e rappresentano il gruppo di popolazione oggetto del nostro articolo . 
questi pazienti , 14 uomini e 9 donne , di et compresa tra i 21 e i 48 anni ( et media 39 anni ) , erano stati ricoverati nelle varie unit pneumologiche della nostra azienda ospedaliera , per la progressiva comparsa di una sintomatologia aspecifica , caratterizzata da astenia ingravescente , febbricola serotina persistente , tosse produttiva , talvolta con striature ematiche , da dolori prevalentemente toracici in 9 pazienti e lombari in 14 . 
solo quattro pazienti presentavano anche disturbi alla deambulazione e incapacit a tenere la stazione eretta ; in due casi tale sintomatologia era insorta durante la gravidanza e si era aggravata durante lallattamento . 
la sintomatologia dolorosa era stata controllata in modo incompleto con antidolorifici , in tre casi anche con laggiunta saltuaria di oppiacei . nel corso dei vari accertamenti eseguiti in ambito ospedaliero , in tutti i pazienti stata riscontrata la presenza di una lesione polmonare alla radiografia diretta del torace o allapprofondimento diagnostico con la tc ( 16 in fase attiva , mentre in 7 erano presenti esiti ) e di una contemporanea alterazione a livello della colonna e dei muscoli psoas . 
lo studio tc stato eseguito su 16 pazienti , utilizzando una tc tradizionale ( rhota ctw 950 sr , esaote biomedica , genova , italia ) e un protocollo che prevedeva dopo liniziale scansione lo studio della colonna con uno spessore di sezione di 5 mm , prima e dopo la somministrazione di mezzo di contrasto ( optiray 300 , tyco healthcare spa , milano , italia ) ; lo studio rm stato eseguito su 7 pazienti , utilizzando lapparecchiatura da 1 , 0 t ( siemens , erlangen , germania ) , con scansioni sagittali e longitudinali t1 , prima e dopo somministrazione di mezzo di contrasto ( magnevist , schering , berlino , germania ) , e t2 spin echo ( tempo di ripetizione ms / tempo di echo ms , 500600 / 1520 nelle prime e 2 , 000 / 90 nel secondo caso )  . raccolta fluida , o ascesso , stata definita quella radiol med ( 2009 ) 114 : 984995 fig . 
gli ascessi venivano considerati appropriati per un drenaggio percutaneo secondo indicazioni gi riportate da altri autori [ 7 ] , che brevemente riassumiamo : dovevano essere associati ad una spondilodiscite , dovevano avere dimensioni superiori ai 3 cm di diametro , con una sintomatologia dolorosa che non aveva tratto beneficio dalla chemioterapia antitubercolare sistemica , con la presenza di unalterazione dei parametri di laboratorio ( leucocitosi neutrofila , aumento della ves )  . 
i criteri di esclusione sono stati il riconoscimento di un tessuto di granulazione paravertebrale o paraspinale associato con una raccolta fluida ipodensa , o la localizzazione epidurale della raccolta , con compressione midollare . 
coronal mr imaging confirms the presence of an abscess originating from the vertebral body of t11 - t12 . altered signal intensity can be seen in the vertebral bodies and intervertebral disc , along with a left - sided swelling with fluid characteristics involving the cranial portion of the ipsilateral psoas muscle . 
la rm nella scansione coronale conferma lesistenza di una formazione ascessuale a partenza dal corpo di d11 - d12 ; inoltre presente unalterazione di segnale nei corpi vertebrali e nel disco intersomatico , con presenza , a sinistra , di una tumefazione con caratteristiche liquide , che coinvolge la porzione craniale del muscolo psoas omolaterale . 
3a , b sonography prior to the interventional procedure with transducer oriented towards the lower pole of the ipsilateral kidney shows a 2.85 - cm hypoechoic mass with homogeneous and well - defined margins in the left paravertebral region ( a )  . 
3a , b lindagine ecografica propedeutica alla procedura interventistica , in sede paravertebrale sinistra , con sonda orientata verso il polo inferiore del rene omolaterale , mostra la presenza di una formazione ipoecogena , a margini omogenei e bene definiti , delle dimensioni di cm 2 , 8 per 5 circa ( a )  . 
grazie alla buona visibilit della lesione viene eseguito il drenaggio ecoguidato , con posizionamento di catetere pig tail 8 fr , a fori multipli terminali ( b )  . modality because it is faster and provides real - time monitoring throughout the drainage procedure . 
the initial puncture was performed under sonographic guidance with a 15 - cm - long 18 - gauge needle ( hs spa , aprilia , rome , italy ) inserted into the most distal portion of the fluid collection . 
the fluid was aspirated with a 10 - ml luer - lock syringe to confirm the position of the needle and guide the choice of drainage catheter based on the texture of the caseous material . 
con il paziente in posizione prona , dopo aver disinfettato larea cutanea dinteresse ed aver effettuato lanestesia locale , stata effettuata una piccola incisione cutanea con una punta di bisturi ( retto , n11 )  . 
successivamente , dopo iniezione di mezzo di contrasto ( optiray 240 , tyco healthcare spa , milano , italia ) per dimostrare lestensione della raccolta ed escludere eventuali comunicazioni fistolose , si proceduto al posizionamento di un filo guida idrofilico 0 , 038 , a punta j , lungo 80 cm , molto rigido ( terumo corporation , gamma international , roma , italia )  . 
si preferito impiegare la pi indaginosa tecnica di seldinger , e non la trocar , per evitare ulteriori traumatismi e dolori al paziente , visto lampio calibro del catetere necessario ad eseguire il drenaggio in prima battuta . 
tutto il materiale purulento stato aspirato ; parte stato inviato per le ricerche batteriologiche . tutti i cateteri sono stati lasciati drenare per gravit ; sono stati lavati quotidianamente con 100 ml di soluzione fisiologica , almeno tre volte al giorno , impiegando siringhe luer lock da 20 ml ; inoltre sono stati utilizzati anche per liniezione di farmaci anti - tubercolari in loco ( rifampicina 600 mg )  . 
il follow - up consistito in una ricerca mensile del mycobacterium tubercolaris , attraverso lesame dellespettorato ed accertamenti di laboratorio , e in una valutazione radiologica semestrale con la tc della colonna e la radiografia diretta del torace . 
la distruzione localizzata di uno o pi corpi vertebrali era visibile in tutti i pazienti : 3 / 23 avevano il coinvolgimento di un solo corpo vertebrale , 16 / 23 di due corpi vertebrali e 4 di tre corpi vertebrali . 
 tutti hanno fatto registrare la contemporanea presenza di un ascesso del muscolo psoas o di entrambi : 6 erano unicamente a destra , 3 a sinistra e 14 erano bilaterali : di cui 10 comunicanti . 
le dimensioni degli ascessi erano variabili : il massimo diametro trasverso era a livello lombare , probabilmente per la maggiore gravit , e raggiungeva i 7 cm , mentre il minimo era a livello dorsale e raggiungeva i 3 , 7 cm ( media 5 , 3 cm )  . 
la massima estensione longitudinale stata di 14 cm , mentre la minima stata di 6 , 3 cm ( media 9 , 8 cm ) tutti i pazienti sono stati sottoposti al drenaggio percutaneo in associazione con la chemioterapia sistemica ( rifampicina 600 mg , isoniazide 300 mg , etambutolo 1250 mg , pirazinamide 1500 mg ) e loco - regionale ( rifampicina 600 mg )  . 
il controllo radiografico , al termine della procedura di posizionamento del catetere di drenaggio , evidenzia le caratteristiche del catetere ( posto allinterno della porzione pi ampia della raccolta ascessuale , in grado di raccogliere per gravit anche la produzione pi craniale , grazie ai multipli fori laterali presenti , allinterno della porzione arrotolata del catetere tale conformazione garantisce latraumaticit del catetere ) e della raccolta appena drenata . the one - step trocar technique . 
all purulent material was aspirated , and part of it was sent for bacteriological testing . all catheters were left to drain by gravity and were flushed at least three times daily with 100 ml of saline solution injected through 20 - ml luer - lock syringes . 
after an initial finding of bilateral and confluent psoas muscle abscesses ( a ) , the first follow - up study 7 days after the procedure shows a significant bilateral reduction in the size of the collections ( b ) , more evident after 15 days ( c )  . 
da uniniziale reperto di ascessi dei muscoli psoas , bilaterali e confluenti ( a ) , il primo controllo radiologico del drenaggio , dopo 7 giorni dalla procedura , evidenzia una notevole riduzione bilaterale delle dimensioni delle raccolte ( b ) , pi evidenti dopo 15 giorni ( c )  . 
dopo 21 giorni , la raccolta sinistra praticamente guarita , mentre a destra permangono ancora dei residui , anche se la produzione giornaliera di essudato inferiore a 10 ml ( d )  . results all patients but one were immigrants . 
sono stati posizionati sempre , in prima istanza , cateteri di drenaggio 8 fr ; si fatto ricorso sistematicamente alla tecnica di seldinger , per evitare il traumatismo diretto di un catetere con calibro radiol med ( 2009 ) 114 : 984995 fig . 
confronto tra la originaria raccolta ascessuale nella porzione pi declive del muscolo psoas di sinistra ( a ) e controllo effettuato dopo 8 giorni di permanenza del catetere di drenaggio ( b )  . bodies was seen in all patients , with involvement of only one vertebra in 3 / 23 patients , two vertebrae in 16 / 23 and three vertebrae in 4 / 23 . 
 all patients had an associated abscess in either one or both psoas muscles : six were unilateral on the right side , three unilateral on the left and 14 bilateral ; ten were the communicating abscesses . 
the largest longitudinal extension was 14 cm , whereas the smallest was 6.3 cm ( mean 9.8 cm ) all patients underwent percutaneous drainage combined with systemic chemotherapy ( rifampicin 600 mg , isoniazid 300 mg , ethambutol 1 , 250 mg , pyrazinamide 1 , 500 mg ) and locoregional chemotherapy ( rifampicin 600 mg )  . 
all procedures were carried out with 8 - fr drainage catheters as a first choice , and the seldinger technique was used systematically to avoid any direct trauma being caused by the large - bore catheters used with trocar technique . 
 we observed no major complications and only two minor complications : in two patients , the catheter became dislodged due to excessive traction during daily catheter care and had to be replaced with a larger ( 10 - fr ) drainage catheter inserted via the existing pathway . 
 non si sono avute complicanze maggiori , ma solo 2 minori : in due pazienti si resa necessaria la sostituzione dei cateteri per una loro dislocazione a seguito di eccessiva trazione durante leffettuazione di una medicazione giornaliera : in tali pazienti stato posizionato un nuovo catetere di drenaggio , di dimensioni maggiori ( 10 fr ) , utilizzando il tramite preesistente . 
in nessuno dei pazienti , compresi quelli con recidiva polmonare , si dovuto ricorrere a drenaggio chirurgico per inefficacia dellatto interventistico , per cui il drenaggio risultato curativo nel 100% dei casi . 
 il periodo di drenaggio stato 536 giorni ( media 18 , 4 giorni ) , con un sensibile miglioramento della sintomatologia gi nelle prime fasi di posizionamento del catetere ed proseguito nei giorni successivi . 
il batterio tubercolare stato isolato in 18 dei 23 ascessi dei muscoli psoas , mentre negli altri la diagnosi stata indiretta , basata cio sui reperti della contemporanea localizzazione polmonare e sui reperti radiologici della colonna vertebrale . 
 durante i primi 12 mesi del periodo di controllo , ben 19 pazienti si sono presentati regolarmente , sottoponendosi sia agli esami di laboratorio sia ai controlli radiografici , mentre 4 non sono risultati pi reperibili . 
mentre tutti erano guariti per la spondilodiscite e le raccolte ascessuali , solo un paziente ha fatto registrare la ripresa della malattia polmonare per una resistenza allisoniazide , per cui si resa necessaria la somministrazione di una differente associazione di farmaci antitubercolari . 
the tuberculosis bacterium was isolated in 18 of the 23 psoas abscesses , whereas in the remainder , the diagnosis was reached indirectly on the basis of findings of the simultaneous involvement of the lung and spine . 
whereas the spondylodiscitis and abscesses had resolved in all cases , one patient had recurrence of pulmonary tuberculosis due to isoniazid resistance , leading to a treatment change . discussion the skeleton , and particularly the spine , is involved in 3% of cases of extrapulmonary tuberculosis . 
tubercularis can reach the spine through haematogenous spread , with embolisation to a site distant from the primary focus , or through direct extension from contiguous foci of infection ( rarely ) ; no cases of venous dissemination or direct seeding during surgery or interventional radiology procedures have been reported [ 12 , 13 ]  . spondylodiscitis starts in the inferior and anterior portion of the vertebral body , at the level of the metaphysis , which has a rich arterial supply . 
the inflammation spreads to the entire vertebral body along the medullary canals and to adjacent vertebrae along the longitudinal anterior ligament , with delayed disc involvement due to the lack of specific cartilage proteolytic enzyme in m . 
disc involvement leads to destruction and collapse of the vertebral body , resulting in severe spinal deformity . abscess formation is caused by the spread of the vertebral disease to neighbouring areas . 
however , because many of its compartments are not completely covered by septations , they may potentially become open and act as a route for disease dissemination , allowing spinal infection to spread . 
the size of the abscess appears to depend on the amount of fat displaced by the inflammatory process or fluid collection [ 14 ]  . although a final diagnosis of tuberculous abscess requires specimen cultures to confirm the presence of the bacterium , cultures often prove positive in only della malattia tubercolare . 
il mycobacterium tubercolaris pu raggiungere la colonna vertebrale attraverso una disseminazione ematogena , con una embolizzazione distante dalla sede di localizzazione dei germi , oppure con una propagazione da sedi dinfezione limitrofe ( rara ) , mentre non sono state segnalate disseminazioni per via venosa o per impianto diretto durante procedure chirurgiche o di radiologia interventistica [ 12 , 13 ]  . linizio della spondilodiscite si verifica nella porzione inferiore e anteriore del corpo vertebrale , a livello della metafisi , dove esiste una ricca vascolarizzazione arteriosa . si verifica un infarto osseo , causato dallembolizzazione settica , a cui fa seguito una reazione infiammatoria granulomatosa . 
dalla primitiva sede , linfiammazione si propaga a tutto il corpo vertebrale , lungo i canali midollari , e a quelli adiacenti lungo il legamento longitudinale anteriore , con coinvolgimento tardivo del disco o dei dischi interposti , grazie allassenza dellenzima proteolitico cartilagineo [ 6 , 13 ]  . 
il risultato di tale coinvolgimento la distruzione e il collasso del corpo vertebrale , con severa deformit della colonna . la formazione degli ascessi il risultato della progressione della malattia vertebrale nei territori circostanti : non trovando ostacoli , pu colpire il canale midollare , posteriormente e / o il retroperitoneo e i muscoli psoas , anteriormente e lateralmente . 
il retroperitoneo diviso in compartimenti da multiple fasce ; molti dei compartimenti non sono completamente ricoperti da tali sepimenti , per cui possono divenire potenzialmente aperti , costituire una rotta di propagazione , attraverso i quali la malattia pu diffondersi . linfezione della colonna pu quindi diffondersi ; le raccolte ascessuali possono comportare spesso una sintomatologia aspecifica , fino alla claudicatio , oppure mimare una lesione osteolitica . 
lestensione delle raccolte sembra dipendere dal grado di spostamento del grasso da parte del processo infiammatorio o del fluido accumulato [ 14 ]  . pur se per una diagnosi definitiva di ascesso tubercolare necessario un esame colturale per confermare la presenza del batterio , tuttavia molto spesso le colture sono positive solo nel 50%60% dei casi , per cui , come segnalato da altri autori [ 15 ] , la diagnosi di tubercolosi talvolta pu essere anche presuntiva , basata sulle caratteristiche di presentazione clinica , sui reperti radiologici allesordio ed a seguito della risposta alla terapia antitubercolare . 
 per quanto riguarda la terapia , il solo impiego dei farmaci antitubercolari associati al riposo a letto e alla terapia fisica hanno notevolmente migliorato i risultati clinici , ma necessitano di tempi molto lunghi per una piena ripresa funzionale . 
in passato , il ricorso alla chirurgia stato legato principalmente allesito non soddisfacente o non risolutivo della terapia conservativa , alla deformit spinale o allinstabilit della colonna , secondaria alle fratture patologiche ed alla presenza di una sintomatologia neurologica : la radiol med ( 2009 ) 114 : 984995 50%60% of cases . 
consequently , as reported by other authors [ 15 ] , the diagnosis of tuberculosis is at times presumptive and based on clinical presentation and imaging findings at onset and following response to antituberculous treatment . with regard to therapy , the use of antituberculous drugs combined with bed rest and physical therapy have significantly improved clinical outcomes , although a full functional recovery will take a long time . 
in the past , surgery was principally used in the case of unsatisfactory results of conservative management , spinal deformity or spinal instability secondary to pathological fractures , and neurological symptoms : anterior decompression , drainage , and debridement with posterior fusion have represented the mainstay of the surgical approach , with mortality rates ranging from 2% to 11% and recurrence rates between 10% and 20% [ 16 , 20 ]  . 
widely and successfully employed in other anatomical regions [ 11 ] , percutaneous drainage under sonographic or ct guidance may also be used in tuberculous abscesses of the psoas muscles to help accelerate healing with full remission of symptoms . 
whereas ct is superior to sonography in depicting the location and extent of the abscesses and their relations with neighbouring organs and in suggesting the most appropriate route for catheter insertion [ 6 ] , sonography has the advantage of being faster and enabling real - time monitoring of the entire procedure . 
 percutaneous drainage of a fluid collection includes various phases : locating the fluid collection , choosing the path to follow and placing one or more catheters [ 23 ]  . 
in consideration of the clinical situation , the imaging findings of extensive vertebral destruction and of abscess formation in the psoas muscles , all patients in our series underwent complete evacuation of the infected collection and never diagnostic aspiration only . 
the final drainage catheter was chosen according to the exudate characteristics , with 8 - fr catheters being used in all cases given that the exudate appeared moderately dense at initial needle puncture [ 9 ]  . 
in addition , our decision took into account the traumatic nature of the procedure in subjects already suffering severely and unable to tolerate placement of larger - bore catheters under local anaesthesia alone . 
the greater laboriousness of the seldinger technique is offset by the lower level of pain endured by the patient during the procedure . the choice of percutaneous drainage catheter proved optimal in terms of resolution of the clinical symptoms in decompressione anteriore , il drenaggio , lo sbrigliamento con la fusione posteriore hanno rappresentato i capisaldi dellopzione chirurgica , con percentuali di mortalit tra il 2% e l11% , e di recidive tra il 10% e il 20% [ 16 , 20 ]  . 
 ad affiancare tali opzioni terapeutiche , negli anni 8090 comparso il drenaggio percutaneo , effettuato in anestesia locale , sotto lassistenza di una tecnica per immagini , il cui obiettivo quello di favorire la risoluzione della raccolta fluida senza dover sottoporre il paziente ad un intervento chirurgico [ 21 ]  . 
gi ampiamente impiegato con successo in altre regioni anatomiche [ 11 ] , anche gli ascessi dei muscoli psoas di natura tubercolare possono giovarsi di tale procedura percutanea , con lausilio della guida ecografica o tc , contribuendo cos ad accelerare il processo di guarigione di queste complicanze della malattia tubercolare , con piena risoluzione della sintomatologia . mentre la tc pi sensibile degli ultrasuoni nel mostrare lesatta localizzazione e lestensione degli ascessi , la loro relazione con gli organi vicini e nel consigliare leventuale tragitto da seguire per posizionare il catetere di drenaggio , evitando il percorso organi e strutture [ 6 ] , lecografia ha il vantaggio di essere pi rapida e di seguire in tempo reale le varie fasi della procedura . 
 lungo la procedura di drenaggio percutaneo di una raccolta fluida comprende le varie fasi di localizzazione della raccolta stessa , la scelta della traiettoria da seguire , il posizionamento di uno o pi cateteri [ 23 ]  . 
visti il contesto clinico , i reperti radiologici di ampia distruzione dei corpi vertebrali e di formazione di ascessi nei muscoli psoas , nella nostra esperienza non abbiamo mai eseguito la sola aspirazione diagnostica , ma sempre il drenaggio completo della raccolta infetta . 
il definitivo catetere di drenaggio stato scelto sulla base delle caratteristiche dellessudato : stato sempre impiegato un catetere 8 fr , in relazione ad una non eccessiva densit della raccolta fluida , verificato gi al momento della iniziale puntura della raccolta con lago [ 9 ]  . 
anche per questi motivi abbiamo preferito non ricorrere alla tecnica trocar ; il maggior numero di passaggi della tecnica di seldinger compensato da una quota minore di dolore che il paziente deve sostenere durante la procedura . la scelta del catetere di drenaggio percutaneo si dimostrata ottimale per la risoluzione del quadro clinico , sia negli ascessi uniloculati , che in quelli pluriconcamerati . 
 la sintomatologia dolorosa notevolmente regredita , in maniera quasi istantanea , gi al momento delliniziale evacuazione della raccolta fluida , dopo la puntura il successivo con lago , rendendo meno doloroso 994 radiol med ( 2009 ) 114 : 984995 both unilocular and multilocular abscesses . 
bilateral and communicating abscesses were treated with the double drainage technique to allow the passage of the smaller fluid collection to the larger one and help close the communication between the two abscess cavities . 
these results are in line with other authors experiences [ 1719 ]  . there were no major complications ( septic shock , bacteremia , haemorrhage , bowel transgression , pleural transgression ) or minor complications ( except for catheter dislodgement during dressing removal )  . 
we had no cases of abscess recurrence , which may occur in the event of resistance to antituberculous medication ( in endemic areas , resistance to isoniazid is 4% ) , incorrect diagnosis ( tuberculous abscess misdiagnosed as bacterial abscess ) , early cessation of systemic antituberculous medication ( therapy should continue for at least 12 months ) and presence of large abscesses extending to different areas , not all drained by the catheter [ 15 , 17 ]  . 
furthermore , the chronic nature of tuberculous spondylitis and the persistence of a active tuberculous focus in the spine after catheter removal may also be responsible for recurrence [ 5 ]  . 
in genere , stato sufficiente posizionare un solo catetere di drenaggio per ogni raccolta fluida ; per gli ascessi bilaterali e comunicanti , stata scelta la tecnica del doppio drenaggio , per favorire dapprima il passaggio della raccolta fluida minore verso la maggiore e poi la chiusura della comunicazione tra le due cavit . 
non abbiamo avuto casi clinici con drenaggi curativi parziali , cio che hanno implicato il ricorso ad un intervento chirurgico per risolvere problemi sottostanti o eventuali fistole , a dimostrazione dellefficacia di questa procedura . 
questi risultati sono in linea con le esperienze di altri autori [ 1719 ]  . non abbiamo avuto complicanze maggiori ( shock settico , batteriemia , emorragia , lesione di anse intestinali , lesioni pleuriche ) , n minori ( se si eccettua la dislocazione del catetere di drenaggio avvenuta durante la rimozione energica della medicazione )  . 
nella nostra esperienza , non abbiamo avuto episodi di recidiva degli ascessi : il motivo di un tale evento da ascrivere alla resistenza ai farmaci antitubercolari ( nelle aree endemiche la resistenza allisoniazide del 4% ) , ad unerrata diagnosi ( ascesso tubercolare scambiato per batterico ) , ad una precoce interruzione della terapia antitubercolare sistemica ( la terapia dovrebbe essere continuata per almeno 12 mesi ) , alla presenza di larghi ascessi che si estendono verso aree differenti , non tutte drenate dal catetere [ 15 , 17 ]  . 
inoltre , la natura cronica della spondilite tubercolare e la persistenza di un focolaio tubercolare attivo nella colonna vertebrale dopo la rimozione del catetere possono essere responsabili della recidiva [ 5 ] : per questi motivi abbiamo voluto associare alla terapia sistemica anche quella loco - regionale , durante il periodo di permanenza del catetere di drenaggio , in modo da aumentare la concentrazione del farmaco nella sede dinfezione tubercolare ; cos in parte possibile spiegare lassenza di recidive nella nostra pur limitata esperienza . 
percutaneous drainage of these fluid collections , if performed by experienced operators , carries a low risk of morbidity and is much less traumatic than the surgical approach . percutaneous drainage requires daily care of the drainage catheter ( flushing with saline solution ) and monitoring over time to ascertain complete abscess resolution and patient recovery . 
percutaneous drainage is curative in 100% of cases . gli ascessi dei muscoli psoas risultano essere unevenienza non rara nella odierna pratica clinica , viste le continue ondate migratorie a cui litalia sottoposta . 
necessita di una gestione quotidiana del catetere di drenaggio ( lavaggio con soluzione fisiologica ) , di un monitoraggio nel tempo del paziente , per garantire la risoluzione completa delle raccolte ascessuali e la guarigione del paziente . 
muzzio1 , 2 1department of medical diagnostic sciences and special therapies , university of padua , via giustiniani 2 , padua , italy 2the veneto institute of oncology ( iov - irccs ) , via gattamelata 64 , padua , italy 3department of oncologic and surgical sciences , university of padua , via giustiniani 2 , padua , italy correspondence to : f . 
institutional review board approval and informed patient consent were obtained . colonic segmental radiopaque markers were counted and transit times calculated in 36 healthy subjects studied using a technique involving daily radiopaque marker ingestion and single radiological visit , with oral administration of 810 ml of a thick barium paste as a colonic trace for the marker count . 
the upper limit for colonic transit times was : 45.6 h in the colon as a whole , 31.2 h in the right colon , 19.2 h in the left colon and 16.8 h in the rectosigmoid . 
in healthy subjects , a barium trace affords optimal visibility of the different colonic segments , enabling accurate location of all markers and thus providing an anatomy - related , repeatable and reproducible fluoroscopic segmental marker count . 
trentasei adulti sani vengono studiati con tecnica di ingestione giornaliera di indicatori radiopachi , ingestione di 810 ml di bario - solfato denso per tracciare il colon e singolo controllo radiologico . 
limite superiore dei tempi di transito in ore : 45 , 6 nellintero colon , 31 , 2 nel colon destro , 19 , 2 nel colon sinistro e di 16 , 8 nel sigma - retto . 
nei soggetti sani , la traccia colica di bario fornisce visibilit ottimale dei segmenti colici , consentendo la localizzazione di tutti gli indicatori ed un conteggio fluoroscopico basato sullanatomia , ripetibile e riproducibile . 
suggeriamo di utilizzare i medesimi valori di riferimento per i tempi di transito colico normali negli italiani di entrambi i sessi . keywords colonic transit radiopaque markers normal value gender difference observer agreement parole chiave transito colico indicatori radiopachi valori normali differenza fra sessi accordo tra osservatori 926 introduction following clinical assessment based on medical history and physical examination , various function tests are used to assess functional constipation in adults , including evacuation proctography ( defaecography ) [ 1 , 2 ] , measurement of colonic transit time ( ctt ) by radiology or scintigraphy [ 3 , 4 ] , magnetic resonance imaging ( mri ) [ 5 , 6 ] , ultrasound us [ 7 , 8 ] , and anorectal and colonic manometry [ 9 , 10 ]  . 
in times of cross - sectional imaging , gastroenterologists seem to have lost interest in using radiopaque markers and scintigraphy to study transit in the assessment of chronic constipation [ 11 , 12 ]  . 
however , radiopaque marker transit studies can reveal slow transit constipation or normal colorectal transit times in patients complaining of constipation , enabling assessment of colonic transit segment by segment . 
the validity of the test has been questioned , particularly because of discrepancies in published colonic segmental transit time studies in distinguishing between different subtypes of constipation [ 9 ] , i.e. colonic dysfunction ( of the proximal or transverse colon ) or outlet obstruction ( involving the sigmoid colon and rectum ) [ 13 ]  . 
individual diversity [ 14 ] , different study methods [ 9 ] , difficulties in defining the different colonic segments when locating and counting retained markers on abdominal x - rays [ 15 ] and differences in the way transit times are defined and calculated might also help to explain discrepancies in published data and result in variations in the numerical reference values adopted for both constipated and normal subjects . 
 for instance , normal reference values for ctts have yet to be established for italian adults , and observer agreement in marker counts in healthy subjects has not been tested . 
the purposes of this study were to measure total and segmental ctt in 36 healthy italian adults with no symptoms of constipation and to estimate intraobserver repeatability and interobserver reproducibility for marker counts using a technique based on daily marker ingestion and single radiological visit . materials and methods subjects radiol med ( 2009 ) 114 : 925934 introduzione dopo laccertamento clinico basato sullanamnesi e lesame obiettivo , vari test funzionali vengono utilizzati per la valutazione della stipsi cronica negli adulti : la proctografia evacuativa ( defecografia ) [ 1 , 2 ] , la misura dei tempi di transito colico ( ttc ) con tecniche radiologiche o scintigrafiche [ 3 , 4 ] , la risonanza magnetica [ 5 , 6 ] , gli ultrasuoni [ 7 , 8 ] , la manometria anorettale e colica [ 9 , 10 ]  . 
per la disponibilit attuale delle tecniche di immagini tomografiche , sembra che i gastroenterologi non siano pi interessati alla misura dei ttc con indicatori radiopachi e con scintigrafia nella valutazione della stipsi cronica [ 11 , 12 ]  . comunque , lo studio del transito con indicatori radiopachi nei pazienti che lamentano stipsi distingue quelli con transito colico rallentato da quelli con transito colico normale e valuta il transito nei vari segmenti colici . 
la validit del test stata criticata soprattutto per la discrepanza dei risultati pubblicati negli studi dei tempi di transito colico segmentali per la differenziazione di sottotipi di stipsi [ 9 ] : inerzia colica ( disfunzione del colon prossimale o trasverso ) oppure stipsi per blocco alluscita ( disfunzione di sigma e retto ) [ 13 ]  . 
differenze individuali [ 14 ] , diversit delle tecniche radiologiche [ 9 ] , difficolt nella identificazione dei segmenti colici per la localizzazione ed il conteggio degli indicatori non espulsi visibili nei radiogrammi delladdome [ 15 ] e differenze nel modo in cui viene definito e calcolato il tempo di transito possono giustificare le discrepanze tra i dati pubblicati , con conseguente variabilit dei parametri di riferimento per gli asintomatici di controllo ed i pazienti con stipsi . 
finora , ad esempio , i valori normali di riferimento dei ttc ed il grado di accordo tra osservatori nel conteggio degli indicatori non sono stati misurati in adulti italiani sani . 
gli scopi di questo studio sono : misurare i ttc totale e segmentali in 36 adulti italiani che non avevano sintomi di stipsi e stimare la ripetibilit intraosservatore e la riproducibilit inter - osservatore del conteggio degli indicatori , utilizzando una tecnica che prevede lingestione quotidiana di indicatori ed un unico controllo radiologico . 
 thirty - six healthy volunteers ( 19 women , 17 men ; median age 60 years , range 4172 years ; median body mass index 22 kg / m2 , range 1625 kg / m2 ) were recruited from among subjects presenting for standard chest radiography at our radiology unit . 
individuals complaining of gastrointestinal symptoms specified in the rome iii criteria for functional bowel disorders [ 13 ] or with a history of gastrointestinal disease or abdominal surgery were excluded , as were women pregnant within the last year . 
all included subjects were negative on physical examination and had always been in good health , with no history of constipation or use of laxatives or other drugs known to affect gastrointestinal motility . 
on the days before and during the test period , volunteers kept to their usual dietary and social habits , as our aim was to conduct a real - life study . imaging technique ctts were measured using a technique described elsewhere [ 15 ]  . 
key steps in the technique included : ( 1 ) a brief preliminary fluoroscopy to ensure that supine fluoroscopic images focused on the colon and rectum for the count of all retained markers ; ( 2 ) saving fluoroscopic abdominal views . 
the right colon ( the caecum and ascending and right transverse colon ) , the left colon ( left transverse and descending colon ) and the rectosigmoid , based on the barium colonic trace , as previously reported [ 15 ]  . 
the markers were counted independently by two radiologists : one ( observer a ) an experienced gastrointestinal radiologist ; the other ( observer b ) with no specific training on marker counting and with 3 years of experience in radiology . 
total and segmental ctts were calculated from the distribution of the markers throughout the colon and in the above - specified three separate segments of the colon using the classic equation : t = tn / n , where t is the alla nostra radiologia per un esame radiografico standard del torace . 
tutti avevano frequenza dellalvo di almeno tre evacuazioni alla settimana ( media 1 , 380 , 69 [ ds ] evacuazioni al giorno ; range 0 , 433 , 14 evacuazioni al giorno )  . 
sono stati esclusi coloro che avevano sintomi gastrointestinali specificati nei criteri rome iii per le alterazioni intestinali funzionali [ 13 ] o anamnesi positiva per malattie gastrointestinali oppure per chirurgia addominale . sono state escluse anche le donne che avevano avuto una gravidanza entro il periodo di un anno dallindagine . 
inoltre , tutti i soggetti arruolati nello studio avevano un esame clinico negativo , avevano sempre goduto di un buono stato di salute , avevano anamnesi negativa per stipsi e non avevano mai assunto lassativi o farmaci che possono alterare la motilit gastrointestinale . 
tutte le donne in et fertile che hanno partecipato allo studio dovevano produrre un test di gravidanza ( gonadotropina corionica umana urinaria ) negativo , eseguito non oltre 48 ore prima dello studio . 
nei giorni precedenti e durante lesame , tutti i volontari dovevano continuare la loro alimentazione consueta e le loro abitudini di vita perch il nostro proposito stato di realizzare uno studio rispettoso della realt quotidiana . 
 calcolo dei dati gli indicatori presenti sono stati contati in tutti i soggetti e localizzati in tre segmenti colici tracciati dal bario : colon destro ( cieco , colon ascendente e met destra del colon 928 radiol med ( 2009 ) 114 : 925934 trasverso ) , colon sinistro ( met sinistra del colon trasverso e colon discendente ) e sigma - retto , come gi descritto [ 15 ]  . gli indicatori sono stati contati indipendentemente da due radiologi : uno ( osservatore a ) era un esperto radiologo gastrointestinale , laltro ( osservatore b ) aveva unesperienza radiologica di tre anni , ma non aveva una pratica specifica nel conteggio degli indicatori . 
non ci sono stati limiti di tempo per linterpretazione delle immagini fluroscopiche memorizzate il cui ordine di analisi stato casuale . ciascun osservatore ha ripetuto il conteggio degli indicatori dopo un intervallo di sei settimane e non conosceva i risultati ottenuti dal collega fino al completamento dello studio . 
pertanto , per calcolare il tempo di transito segmentale in ore il numero di indicatori contati in un dato segmento colico stato moltiplicato per 2 , 4 perch sono stati ingeriti quotidianamente dieci indicatori e lintervallo tra due ingestioni stato di 24 ore . 
la ripetibilit intra - osservatore dei conteggi per ciascun segmento colico , stata stimata con il coefficiente di ripetibilit ( cr ) che considera le variazioni intra - osservatore dei conteggi ( secondo conteggio verso primo conteggio , sia dellosservatore a che b )  . 
il cr stato calcolato con la formula : 1 , 96 ( cid : 2 ) ( cid : 3 ) 2sw , dove sw la deviazione standard intra - soggetto . il cr definisce i valori estremi delle differenze fra due conteggi fatti dallo stesso osservatore entro cui cade il 95% dei soggetti e pu essere rappresentato graficamente considerando le differenze tra i due conteggi effettuati da ogni osservatore e le loro medie . 
la riproducibilit inter - osservatore dei conteggi per ciascun segmento colico stata stimata con i limiti di accordo ( la ) per il 95% dei casi , valutando le variazioni inter - osservatore ( primo conteggio dellosservatore a verso il primo di b )  . 
the barium trace enables clear identification of the different anatomical segments of the colon and an easy segmental marker count , thus overcoming the potential drawback of the weak fluoroscopic signal . 
la traccia di bario consente lidentificazione sicura dei diversi segmenti anatomici del colon ed il facile conteggio segmentale degli indicatori , superando lo svantaggio potenziale della debolezza del segnale fluoroscopico . 
 transit time in a given colonic segment , t is the time between two marker ingestions , n is the number of markers counted in a given colonic segment , and n is the number of markers ingested daily [ 16 ]  . 
as ten markers were ingested daily and the interval between two ingestions was 24 h , the number of markers counted in a given colonic segment was multiplied by 2.4 to calculate the segmental transit time in hours . 
intraobserver repeatability for the marker counts in each colonic segment was assessed using the repeatability coefficient ( rc ) , considering the intraobserver variations ( second count vs first count for both observers )  . 
the rc was calculated using the formula : 1.96 ( cid : 2 ) ( cid : 3 ) 2sw , where sw is the standard within - subject deviation . the rc defines the range of the differences between two counts made by the same observer for 95% of the subjects , and it was analysed by plotting the differences between the counts repeated by each observer and their means . 
interobserver agreement on the marker counts for each colonic segment was assessed using 95% limits of agreement ( la ) , radiol med ( 2009 ) 114 : 925934 considering interobserver variations ( observer b versus a ; first count used )  . 
the la were calculated using the formula : is the mean difference and sd the standard 1.96sd , where d deviation of the differences , considering the two observers as two counting methods . 
the la define the range expected to include 95% of the differences between the two observers marker counts , and it was analysed by plotting the difference between the counts obtained by the two observers against the mean of the two values . 
8.2 ( sas institute inc . , cary , nc , usa )  . results total and segmental ctts were evaluated in 36 healthy adults using daily marker ingestion and a single radiological examination . 
the rc ( intraobserver repeatability ) showed that individual differences between repeat counts relating to the right colon , left colon and rectosigmoid were always less than two markers ( table 1 ) , meaning a strong repeatability of the counts . 
the p values for total and segmental ctts according to the two observers radiographic measurements ( a vs b , considering their first count ) ranged from 0.92 for the rectosigmoid to 0.97 for the whole colon , meaning that their measurements were statistically identical . table 2 summarises previously published values for total la mediads per poter confrontare i nostri risultati con quelli di altri autori . 
il cr ( ripetibilit intra - osservatore ) ha dimostrato differenze individuali tra i conteggi replicati sempre inferiori a 2 indicatori sia nel colon di destra che di sinistra e sigma - retto ( tabella 1 ) , a testimonianza di unottima ripetibilit del conteggio . 
infine , i valori di p relativi alle misure radiologiche dei ttc totale e segmentali ottenute dai due osservatori ( primo conteggio di a verso il primo di b ) erano compresi fra 0 , 92 per il sigma - retto e 0 , 97 per lintero colon , a dimostrazione che le misure del transito erano statisticamente identiche . 
la tabella 2 riassume i valori dei ttc totale e segmentali riportati in pubblicazioni precedenti dove stata utilizzata la tecnica di ingestione quotidiana degli indicatori con singolo controllo radiografico , in pi di 30 soggetti [ 1822 ] e fornisce la mediads ed il limite superiore della norma ottenuti nel presente studio ( primo conteggio dellosservatore a )  . 
la mediana dei tempi di transito colico totale , destro , sinistro e nel sigma - retto era rispettivamente di 45 , 6 ore , 31 , 2 ore , 19 , 2 ore e 16 , 8 ore . 
2a - c accordo inter - osservatore per il conteggio fluoroscopico degli indicatori in 36 soggetti adulti sani : nei grafici sono segnati i valori delle differenze individuali e delle medie dei conteggi effettuati da due osservatori e i la . 
esiste una notevole concordanza tra i conteggi dei due osservatori nel colon di destra ( a ) , nel colon di sinistra ( b ) e nel sigma - retto ( c )  . si notino i numerosi punti che cadono vicino alla linea dello zero . and segmental ctts in studies using daily marker ingestion and a single x - ray in series of more than 30 subjects [ 1822 ] , showing the total and segmental ctts expressed as the meansd and upper limits of normal for the present radiological marker study ( observer a , first count )  . 
table 3 shows the median total , right , left and rectosigmoid ctts for women and men and the correspondent upper limits of normal ( observer a , first count )  . tutti gli indicatori presenti nel colon era di 61 , 21%15 , 56% , 18 , 05%12 , 82% e 20 , 72%15 , 39% rispettivamente nel colon destro , sinistro e sigma - retto . 
la tabella 3 riporta la mediana dei tempi di transito colico totale , destro , sinistro e nel sigma - retto per le donne e gli uomini ed i limiti superiori della norma corrispondenti ( primo conteggio dellosservatore a )  . discussione stato proposto che i ttc segmentali possano essere utilizzati per classificare i pazienti stitici in sottogruppi fisiolopatologici [ 23 ] , ma altri autori non considerano validi gli studi sul transito colico segmentale con ingestione radiol med ( 2009 ) 114 : 925934 table 2 total and segmental colonic transit times in healthy adults expressed as the meansd and upper limit of normala author [ ref ] country / year no . 
such a technique only monitors the markers progress through the colon for 72 h , which is not long enough for patients with functional constipation because it has been demonstrated that the upper limit ( 95th percentile ) of the total ctt may be more than 220 h in constipated patients [ 3 ]  . 
an evidence - based review of the utility of physiological and imaging tests in evaluating chronic constipation identified valid evidence to support colonic transit study with radiopaque markers [ 24 ]  . 
other common physiological tests , such as colonic transit study using scintigraphy , anorectal manometry , the balloon expulsion quotidiana di indicatori per tre giorni e controllo radiologico in quarta giornata [ 11 ]  . 
questa tecnica monitora la progressione degli indicatori nel colon solo per 72 ore che un periodo insufficiente nei pazienti con stipsi funzionale perch stato dimostrato che negli stitici il limite superiore ( 95 percentile ) del ttc totale pari a pi di 220 ore [ 3 ]  . tuttavia uno studio di revisione sullutilit dei test fisiologici e con immagini , basata sullevidenza clinica , riconosce validit alla misurazione del transito colico con indicatori radiopachi nella valutazione della stipsi cronica [ 24 ]  . 
ad altri test fisiologici usuali , come la scintigrafia , la manometria anorettale , il test dellespulsione del palloncino , la manometria colica , viene attribuito lo stesso grado o un grado inferiore di utilit clinica basata sullevidenza [ 24 ]  . lo studio radiologico dei ttc fornisce unidea obiettiva dei disturbi dei pazienti con stipsi ed utile criterio nella selezione dei pazienti destinati alla terapia chirurgia [ 2527 ] o alle terapie con farmaci enterocinetici [ 2830 ]  . 
ctts give an objective idea of patients complaints of constipation and are useful in selecting patients for surgery [ 2527 ] and evaluating the effects of enterokinetic drugs [ 2830 ]  . 
we opted to use fluoroscopic abdominal views because it has been demonstrated that fluoroscopy exposes individuals to a median skin dose of 0.239 cgy , which is approximately a third of the radiation exposure of a classic abdominal x - ray obtained using a digital recording plate [ 15 ]  . 
i diversi segmenti colici sono identificati facilmente con scintigrafia [ 31 ] che ha il vantaggio di una dose di esposizione alle radiazioni minima : tra 1 , 1 e 9 , 0 msv allintero corpo [ 12 , 32 ] , a seconda del tempo impiegato dal radioisotopo nellattraversamento del colon . 
da parte nostra abbiamo scelto la fluoroscopia delladdome perch stato provato che lesposizione fluoroscopica dei soggetti , con una dose mediana alla cute di 0 , 239 cgy , circa un terzo dellesposizione per una radiografia standard delladdome , ottenuta usando una piastra digitale [ 15 ]  . 
gli autori hanno somministrato per bocca grosse capsule contenenti una soluzione salina di gadolinio ed hanno calcolato un ttc medio simile a quello calcolato con lesame radiologico [ 33 ]  . 
poich prevedibile che gli asintomatici di controllo abbiano un tempo di transito colico inferiore alle 72 ore , il calcolo del ttc sarebbe stato accurato con una tecnica di monitoraggio dei sani per 72 ore , ovvero con assunzione degli indicatori per tre giorni consecutivi [ 18 ]  . 
comunque abbiamo optato per la stessa tecnica usata negli stitici , ovvero gli indicatori sono assunti per dieci giorni consecutivi , per un confronto diretto delle radiol med ( 2009 ) 114 : 925934 as for constipated patients to enable a stricter comparison of the measurements obtained . 
the total ctt calculated in our study comes within the range shown in the series in table 2 , but our measurements tend to reveal longer right ctt and shorter rectosigmoid ctt than other studies ( table 2 )  . 
this was probably partly because any overlap of the pelvic caecum with the rectosigmoid may negatively affect marker count accuracy if no colonic barium trace is used to enhance the anatomical boundaries between the different colonic segments . 
some authors found that women had a slower ctt than men [ 18 , 34 ] , but we could find no significant ctt differences between women and men , in agreement with other reports [ 21 , 30 ]  . in conclusion , this study produced a set of normal ctts in healthy italian individuals . 
nel nostro studio , il ttc totale rientra nel range di quelli riportati in tabella 2 ; invece il tempo di transito nel colon destro e nel sigma - retto tende ad essere rispettivamente pi lungo e pi breve del corrispondente riportato in altri studi ( tabella 2 )  . 
probabilmente ci in parte dovuto al fatto che leventuale sovrapposizione di un cieco pelvico e del sigma - retto riduce laccuratezza del conteggio degli indicatori , in assenza di una traccia di bario che evidenzi i contorni dei diversi segmenti colici . alcuni autori hanno misurato un ttc pi lungo nelle donne che negli uomini [ 18 , 34 ] ; la nostra esperienza non dimostra significative differenze del ttc nei due sessi , in accordo con altri studi [ 21 , 30 ]  . in conclusione , questo studio fornisce una serie di misure dei ttc normali in adulti italiani sani . 
these were accounted for by the presence of a major lesion distracting the examiners attention from a less important associated lesion in one case , a false negative result in a patient examined on a incompletely radiolucent spinal board and underexposure of the coccyx region in an obese patient . six cases were related to an interpretation error by the radiologist . 
di queste , in una il rilievo di una lesione maggiore ha distolto lattenzione da una lesione associata di minore importanza ; un falso negativo stato osservato in paziente esaminato su barella spinale , non completamente radiotrasparente ; uno era per sottoesposizione della regione coccigea in soggetto obeso . in 6 casi vi stato errore interpretativo del radiologo . 
abbiamo individuato strumenti che speriamo atti a ridurre il livello di contenzioso . keywords radiology audit civil liability litigation clinical risk management parole chiave radiologia audit responsabilit civile contenzioso management del rischio clinico introduction introduzione claims for compensation and legal action against physicians for presumed error are an increasingly serious problem in all countries and in all medical specialties . 
litigations arising from these claims have led to a constant increase in insurance premiums paid by healthcare institutions and individual professionals , and these costs have become an increasingly important item in the expenditure of hospitals and their personnel . there are numerous strategies for reducing litigation that tackle different aspects of the probleone of them is based on the retrospective review of legal proceedings already underway to analyse the causes of the different litigation episodes and the possible personal or organisational factors responsible for the error with a view to planning corrective measures and drawing up guidelines to improve patient management in healthcare institutions [ 1 , 2 ]  . 
from a technical point of view , this approach follows the methods used in the clinical audit [ 38 ]  . the accident and emergency department is the healthcare facility with the highest healthcare expectations by the general public and is therefore the most common site of claims for damages due to inappropriate treatment , whether real or presumed . 
radiology is not the most frequently affected specialty among those operating in accident and emergency departments , but it does particularly lend itself to critical analysis and review of the contested episodes because of the existence of objective documents ( radiographs ) that testify to the patients clinical situation at the time of evaluation . 
interpretation errors of radiographs performed for a suspected fracture represent the most frequent cause of claims for damages against radiologists in italy [ 9 ]  . le richieste di risarcimento e le denunce contro i medici per presunti errori sono un problema di crescente gravit in tutti i paesi e per tutte le specialit mediche . 
il contenzioso risultante da queste richieste causa un continuo incremento delle tariffe assicurative a carico delle aziende sanitarie e dei singoli professionisti e queste sono diventate un importante capitolo di spesa aziendale e personale . 
tra queste , una si basa sullanalisi retrospettiva del contenzioso gi instauratosi analizzando le cause dei diversi episodi e i possibili fattori predisponenti allerrore , personali o organizzativi al fine di pianificare cambiamenti atti a evitare gli stessi e a stendere linee guida per migliorare il percorso dei pazienti nelle strutture sanitarie [ 1 , 2 ]  . 
da un punto di vista tecnico , questo approccio segue le modalit utilizzate nel corso degli audit clinici [ 38 ]  . il pronto soccorso la struttura sanitaria verso cui sono pi alte le aspettative di salute dei cittadini e , conseguentemente , pi frequenti le richieste di risarcimento danni per inappropriatezza delle cure , vera o presunta che sia . 
tra le varie unit operative del pronto soccorso , la radiologia non quella pi frequentemente chiamata in causa , ma si presta particolarmente ad una analisi critica degli episodi contestati perch esistono documenti oggettivi ( i radiogrammi ) a testimonianza della situazione clinica del paziente al momento della valutazione che possono essere rivalutati criticamente . 
una errata interpretazione degli esami radiografici eseguiti per sospetta frattura la prima causa , in ordine di frequenza , delle richieste di risarcimento danni nei confronti dei radiologi in italia [ 9 ]  . 998 radiol med ( 2009 ) 114 : 9961008 in this study , we reviewed the documentation regarding episodes that involved radiological services provided by radiologists in our hospitals accident and emergency radiology department over the period 20042006 to verify the causes of these episodes , identify the predisposing factors and plan the necessary corrective measures . nel nostro lavoro abbiamo rivalutato la documentazione relativa ai sinistri verificatisi nel corso delle prestazioni sanitarie fornite dai radiologi del dipartimento emergenza e accettazione ( dea ) della nostra azienda nel triennio 20042006 al fine di verificare le cause degli stessi , riconoscerne i fattori predisponesti e pianificare i necessari interventi correttivi . materials and methods we analysed the litigation database held by our institutions general and legal affairs office regarding the period 20042006 to extract episodes in which there was a failure to diagnose a fracture at the radiology unit of the accident and emergency department . 
for each patient , the radiology report and relevant images were collected from the radiology information and picture archiving system , as well as the data regarding admission , treatment and discharge from the accident and emergency department . each episode was studied using clinical audit techniques [ 5 , 6 ] , with an analysis of administrative aspects followed by clinical aspects . 
 with regard to the first component , we analysed all procedures relating to the collection and processing of data for the litigation episode against the radiology service of the accident and emergency department and the insurance outcome of each episode . 
type of event ( classified into five types : misdiagnosis or failure to diagnose , inappropriate treatment or failure to treat , onset of complications , falls , other ) 10 . 
di ciascun paziente sono stati tratti , dal sistema informativo e dallarchivio radiologico , i referti e le immagini radiografiche pertinenti e i dati relativi alla scheda di accettazione , trattamento e dimissione dal pronto soccorso . ciascun episodio stato studiato seguendo le tecniche utilizzate nel corso degli audit clinici [ 5 , 6 ] , analizzando in primo luogo la parte amministrativa e , quindi , la parte clinica per quanto riguarda la prima componente sono state analizzate le modalit globali di raccolta e trattamento del contenzioso riguardante la radiologia del dea e lesito assicurativo di ciascun episodio . 
list of documents contained in each file , in chronological order with regard to the clinical component , the images of each patient were evaluated by two radiologists in musculoskeletal radiology expert . 
the evaluation took place without the radiologists being aware that the images regarded cases of litigation and was performed separately . in the event of disagreement between the two experts , no attempt was made to reach a consensus . after the blinded review of the radiographs , a final judgement of each case was formulated by two radiologists , a forensic pathologist and the head of the general and legal affairs office . 
it aimed to understand whether the compensation claim was truly due to a diagnostic error arising from the performance or interpretation of the radiographic examination and , if so , to analyse the events that led to the error . analysis of overall results was then used to implement corrective measures to improve the organisational and technical aspects of patient management and to produce patient information sheets that we trust will influence patient expectations in relation to the service provided . results the number of compensation claims regarding accident and emergency services at our hospital in the 3 - year period was 84 ( 35 in 2004 , 29 in 2005 and 20 in 2006 )  . 
for those occurring in 2006 ( 20 cases ) , 14 claims were filed in 2006 and 6 in 2007 . with regard to the claimants names , several transcription errors were identified that were corrected to avoid association with different cases due to coincidence of names . transcription errors were also identified in the dates of some events , which had , as a result , been catalogued incorrectly . 
in addition , in some cases , even the compensation claims were unable to shed light on precisely what the presumed error was that had motivated the claim . the analysis then identified the service within the accident and emergency department that was involved in each 13 . 
elenco dei documenti presenti in ciascun fascicolo secondo un ordine cronologico . per quanto riguarda la parte clinica , le immagini di ogni paziente sono state sottoposte a valutazione da parte di due radiologi esperti in radiologia muscoloscheletrica . lanalisi ha avuto luogo senza che gli stessi fossero a conoscenza che le immagini riguardavano episodi di contenzioso ed stata svolta in modo disgiunto . 
questa ha considerato congiuntamente i documenti del file amministrativo , i referti , le immagini radiologiche , le cartelle cliniche del pronto soccorso e i risultati dellanalisi da parte degli esperti e ha cercato di comprendere se la richiesta risarcitoria era realmente dovuta ad un errore diagnostico avvenuto durante leffettuazione o linterpretazione dellindagine radiografica e , in caso positivo , di analizzare le modalit con cui si giunti allerrore . lanalisi dei risultati complessivi stata quindi utilizzata per costruire azioni correttive per migliorare le modalit organizzative e tecniche delle attivit e stilare informazioni da fornire ai pazienti che , speriamo , incidano sulle loro aspettative nei confronti del servizio fornito . 
 risultati i casi di richiesta risarcitoria relativi alle attivit svolte nel dea della nostra azienda ospedaliera sono stati , nel triennio analizzato , in numero di 84 ( 35 con evento verificatosi nel 2004 , 29 nel 2005 e 20 nel 2006 )  . 
per il 2006 ( 20 casi ) , 14 sono stati denunciati nello stesso anno e 6 nel 2007 . per quanto riguarda i nominativi dei richiedenti , sono stati identificati alcuni errori di trascrizione degli stessi che sono stati corretti in quanto associati a casi differenti per riguardavano anche la data di alcuni eventi che erano stati precedentemente catalogati , di conseguenza , in modo erroneo . 
errori trascrizione 1000 radiol med ( 2009 ) 114 : 9961008 claithe radiology service was involved in 22 events over the 3 - year period , subdivided as follows : in 2004 , seven events ; in 2005 , eight events ; in 2006 , seven events . tables 13 summarise the overall results ( subdivided by year )  . 
in another case ( fracture of the coccyx ) , the final judgement established that stata precisata , in quasi tutti i casi la descrizione dellevento con una terminologia pi opportuna ed accurata dal punto di vista medico - specialistico . 
inoltre , anche le richieste da cui muovevano le pretese risarcitorie non hanno permesso , in qualche caso , di capire a quali presunti errori fosse ascrivibile la motivazione della richiesta . si individuato quindi in ciascun fascicolo il reparto interessato allinterno del dea . 
radiologia risultava coinvolta in 22 eventi complessivi che , suddivisi nei tre anni , risultavano : nel 2004 : 7 eventi ; nel 2005 : 8 eventi ; nel 2006 : 7 eventi . 
no dislocation of third finger fracture of radius fracture of d12 no fracture no fracture a & e , accident and emergency department tabella 1 contenzioso relativo allanno 2004 frattura falange iv dito mano no frattura frattura capitello radiale frattura riscontrata frattura ginocchio frattura riscontrata sospetta frattura gomito dopo lussazione no frattura frattura iv dito lussazione iii dito frattura radio frattura d12 no frattura iv lussazione iii no frattura no frattura ps , pronto soccorso fracture visible with difficulty litigation not related to radiology litigation not related to radiology fracture identified on radiograph obtained 15 days after episode . 
 litigation closed without further consequences minimal fracture , not identified because attention distracted by dislocation fracture not seen fracture not seen , patient on spinal board frattura visibile con difficolt contenzioso non inerente la radiologia contenzioso non inerente la radiologia riscontrata frattura in esame rx 15 gg dopo lepisodio . 
yes / yes no fracture of radius yes / yes a & e , accident and emergency department tabella 2 contenzioso relativo allanno 2005 paziente lesione diagnosi ps esperto 1 esperto 2 epicrisi frattura d12 frattura piede no frattura no frattura fracture visible with difficulty . 
manca nella richiesta se frattura ossea o cartilaginea frattura non vista frattura non vista frattura radio frattura iv metacarpo frattura piede frattura riscontrata frattura riscontrata no frattura si , malleolo si , cuboide non valutabile . 
manca specifica ( dubbia ) ( dubbia ) frattura naso no frattura frattura rotula frattura polso no frattura frattura stiloide ulna no frattura radio si / si si / si ps , pronto soccorso the radiographic image was of suboptimal quality ( obese patient incorrectly imaged by the available equipment )  . yet another case of failure to diagnose ( vertebral fracture ) due to technical problems was seen in a patient examined on a spinal board . 
in addition , the different segments of the vertebral column were represented on different radiographs , with the fractured vertebra visualised at the periphery of only one of the images obtained . 
un ulteriore episodio , in cui il paziente reclamava un danno per omessa diagnosi di frattura associata a lussazione del gomito ( lussazione correttamente identificata e trattata ) , stato chiuso dallassicurazione aziendale senza seguito . 
 stata stilata una istruzione operativa riguardante lo studio dei pazienti su barella spinale che prevede una attenta centratura dei radiogrammi e un consulto con il radiologo prima di allontanare il paziente dalla sala desame . 
questi dovr porre particolare attenzione a che tutti i segmenti interessati dal trauma siano ben visualizzati , sottolineare sul referto le problematiche tecniche incorse ed eventualmente richiedere una ulteriore indagine dopo stabilizzazione del paziente . 
si raccomandato al radiologo di mantenere viva lattenzione su tutto quanto presente sul radiogramma anche dopo aver identificato una lesione , in quanto non infrequente il riscontro di lesioni multiple . 
si predisposto un foglio informativo per il paziente in cui , a fronte della possibilit di falsi negativi per lesioni impercettibili , si invita lo stesso a ripresentarsi presso il reparto in caso di persistenza della sintomatologia . 
nellambito delle programmazioni di rinnovo tecnologico in azienda , si messo in programma lacquisto di un apparecchio pi performante per il pronto soccorso , in grado di esaminare correttamente anche soggetti obesi . discussione le strategie per ridurre il contenzioso in medicina sono numerose e affrontano aspetti diversi del problema . 
da pi parti , anche a livello istituzionale , si sta cercando di sviluppare e promuovere la cultura di imparare dagli eventi avversi attraverso linee guida sul come trattare gli errori e gli episodi problematici [ 6 , 7 ]  . 
a further case , in which the patient was claiming damages for failure to diagnose a fracture associated with a dislocation of the elbow ( dislocation correctly identified and treated ) was closed by the insurance company without further consequences . 
on this 1004 radiol med ( 2009 ) 114 : 9961008 basis , the fracture was not considered due to an error by the radiologist . table 4 shows the cases divided into five groups . 
cases type specifications interpretation error of the radiologist litigation not related to radiology imperceptible fracture nonassessable episode litigation closed without compensation fracture of patella ( 1 ) , radius ( 1 ) , wrist ( 1 ) , lumbar vertebra ( 1 ) , femur ( 2 ) lesions correctly identified ; claim probably due to dissatisfaction with treatment 3 fractures not identified by one reviewer ; 1 fracture of finger not seen ( associated with dislocation ) ; 1 fracture not seen on spinal board ; 1 fracture of coccyx not seen in obese patient lacking clear description of lesion for which compensation was being claimed lesion not identifiable even retrospectively , visualised some time after trauma tabella 4 suddivisione degli episodi per tipologia n casi tipologia specificazioni errore interpretativo del radiologo contenzioso non ascrivibile alla radiologia fratture impercettibili episodi non valutabili contenzioso chiuso senza risarcimento frattura rotula ( 1 ) , radio ( 1 ) , polso ( 1 ) , vertebra lombare ( 1 ) , femore ( 2 ) lesioni correttamente identificate , contenzioso verosimilmente dovuto a insoddisfazione per la cura 3 fratture non riconosciute da uno dei revisori ; 1 frattura dito non vista ( associata a lussazione ) ; 1 frattura non vista su barella spinale ; 1 frattura coccige non vista in paziente obeso mancava chiara descrizione della lesione per cui si richiedeva il risarcimento lesione non riconoscibile anche in retrospettiva , visualizzata a distanza di tempo dal trauma radiol med ( 2009 ) 114 : 9961008 1005 device for the accident and emergency radiology department that is capable of correctly examining even obese patients . discussion there are numerous strategies for reducing litigation in medicine that tackle different aspects of the proble at various levels , including the institutional level , efforts are being made to promote a culture of learn from your mistakes with the use of guidelines on how to deal with errors and problem cases [ 6 , 7 ]  . 
numerous healthcare institutions have followed this type of approach , creating specific departments dedicated to clinical risk management [ 6 , 8 ]  . the philosophy characterising the function of these departments consists of a complex system of culture , policies , objectives , individuals , resources and procedures . 
at the same time , however , the system needs to be able to act immediately by identifying problems at an early stage , analysing them , recognising the mechanisms responsible for the error or mismanagement and correcting them [ 3 , 4 ]  . 
in addition , it needs to be able to perform the task of conciliation , following the principle whereby most cases of litigation arise from poor communication between the healthcare institution and the user . the approach adopted in our case series followed , from a technical point of view , the method used in the clinical audit [ 3 , 4 ] , with a retrospective analysis of administrative and clinical factors for each episode . 
the administrative analysis revealed that the claims for compensation did not immediately follow the event , with claims being filed in some cases as late as 3 years after the event . 
for classification purposes , therefore , the claims need to be ordered both by the date of the event and the date of the arrival of the claithis is able to produce useful and significant data regarding annual incidence . 
contemporaneamente , per , il sistema deve mettersi immediatamente in grado di agire identificando precocemente i problemi , analizzandoli , riconoscendo i meccanismi attraverso i quali si giunti allerrore o al disservizio e correggendo gli stessi [ 3 , 4 ]  . 
inoltre , deve essere capace di svolgere opera di conciliazione seguendo il principio per cui la gran parte del contenzioso nasce da cattiva comunicazione tra le strutture del sistema sanitario e il cittadino . 
 lapproccio seguito nella nostra casistica segue , da un punto di vista tecnico , le modalit utilizzate nel corso degli audit clinici [ 3 , 4 ] analizzando retrospettivamente fattori amministrativi e clinici di ciascun episodio . allanalisi amministrativa , la valutazione ha mostrato che le richieste danni non sono immediate rispetto allevento . 
peraltro , la progressiva riduzione numerica delle richieste negli anni fa ipotizzare che leventuale variazione possa essere solo di poche unit . sono state anche individuate difficolt nella attribuzione delle richieste . 
anche in questo caso , appare necessaria particolare attenzione alla catalogazione degli episodi perch le lettere di richiesta di risarcimento sono spesso oltremodo succinte e prive di elementi che consentono di ricostruire correttamente levento . per quanto riguarda la componente clinica , da sottolineare che lincidenza del problema delle diagnosi radiologiche errate in pronto soccorso stato esaminato estesamente in letteratura . 
la percentuale di diagnosi errate varia , a seconda degli articoli considerati , dal 1% al 1006 radiol med ( 2009 ) 114 : 9961008 possible difference is in the order of several units only . difficulties were also identified in the attribution of the claims . 
in this case , too , there appears to be a need for special care in classifying episodes , because the letters claiming compensation tend to be brief and without elements enabling a precise reconstruction of the event . with regard to the clinical component , the incidence of radiological misdiagnoses in the accident and emergency department has been widely discussed in the literature . 
there are , however , no studies that demonstrate a difference in the quality of radiological reports performed at the beginning or the end of a shiin our series , this factor may be taken into consideration to explain the episodes in which the radiologists error could not be attributed to anything other than a failure to identify a lesion . a further cause ( that explains one of the episodes ) is the presence of two associated lesions , whereby one is readily identifiable and the other is less evident . 
in the first instance , a patient was examined on an incompletely radiolucent spinal board , and the radiographs failed to guarantee an optimal evaluation of all of the segments requested by the study . 
we feel that it is useful to recommend that the radiologist note in the report any technical difficulties encountered during the examination , emphasising how the resulting radiographs cannot be used to rule out the presence of anything but patently evident lesions and inviting the requesting physician to have the patient undergo the examination again once stabilised , if necessary . with regard to the second episode , availability of a more appropriate device for the study of obese subjects might have 6% [ 1012 ]  . 
per quanto riguarda le fratture , due lavori affrontano specificatamente il problema riportando valori che vanno dal 2 , 8% al 3 , 7% [ 13 , 14 ]  . 
nella nostra casistica , questo fattore pu forse essere preso in considerazione per spiegare gli episodi in cui lerrore del radiologo non poteva essere riferito ad altro se non ad un deficit identificativo . una causa ulteriore ( spiega uno degli episodi ) la presenza di due lesioni associate , di cui una facilmente riconoscibile e la seconda di difficile identificazione . 
nel primo , un paziente stato esaminato su barella non completamente radiotrasparente e linsieme dei radiogrammi eseguiti non garantiva valutazione ottimale di tutti i segmenti di cui era richiesto lo studio . 
riteniamo sia utile raccomandare al radiologo segnalare nel referto la difficolt tecnica di esecuzione , sottolineando come i radiogrammi risultanti non consentano di escludere la presenza di lesioni men che grossolane e invitando il richiedente ad inviare nuovamente il paziente dopo stabilizzazione , se necessario . 
necessario tenere in considerazione questo fatto nelle programmazioni di sostituzione delle attrezzature radiografiche . un lavoro della letteratura riporta che il 33% dei casi di mancata diagnosi di frattura ha lesioni impercettibili al momento dellesame [ 14 ]  . 
this fact should be borne in mind when planning of the upgrade of radiological equipment . one study reported that 33% of cases of failure to diagnose a fracture were related to imperceptible lesions at the time of the examination [ 14 ]  . 
informing the radiologist of a specific clinical suspicion or an anatomical site requiring greater attention because it is particularly symptomatic can in fact influence their interpretation of dubious images or findings at the limit between normal and pathological , thus prompting additional views being taken that are better able to reveal an abnormality . 
 we believe it is useful to provide the patient with an information sheet reminding them the radiographic examination can return false - negative errors in the presence of small fractures and that such fractures are often identifiable several days later . 
the patient is therefore invited to return for a further evaluation in the event that symptoms persist . a correct characterisation was not possible in three cases . here , the radiographs showed no fractures and the administrative documentation gave no description of the episode and / or lesion able to reveal its nature . lastly , in six out of 22 cases , analysis of the episode demonstrated that the problem giving rise to the litigation did not originate from the radiological service ( the radiologist had correctly identified the lesion ) but was probably due to the overall treatment of the trauma or the aftereffects thereof . it should be noted that our series refers to litigation regarding the accident and emergency radiology department and does not enable an analysis of the rate of error in the diagnoses performed by radiologists who work in the department . 
the discrepancy between the rate of error reported in the literature and the litigation rate in our study is probably due to the fact that in clinical practice , very few cases can present evidence of harm due to error , and therefore the claim for compensation . however , we believe that the study we performed is still useful . 
una stretta collaborazione con il medico che ha visitato il paziente pu , in taluni casi , rivelarsi utile : la segnalazione di un sospetto clinico specifico o di sedi anatomiche su cui necessaria maggiore attenzione perch particolarmente sintomatiche pu infatti influire sullinterpretazione di immagini dubbie o di reperti al limite tra normale e patologico , inducendo talora lesecuzioni di proiezioni aggiuntive in grado di meglio svelare unalterazione . 
riteniamo utile fornire ai pazienti un foglio informativo su cui si ricorda che le indagini radiografiche possono presentare errori falso - negativi a fronte di piccole fratture e che queste possono essere spesso riconoscibili a distanza di pochi giorni . 
il paziente viene quindi invitato a ripresentarsi per una nuova valutazione qualora la sintomatologia persista . non stato possibile inquadrare correttamente tre casi . in essi i radiogrammi non mostravano fratture e la documentazione amministrativa non presentava una descrizione dellepisodio e / o della lesione sufficiente a comprenderne la natura . 
radiologia ( il radiologo aveva identificato correttamente la lesione ) ma , verosimilmente , riguardava il trattamento complessivo del trauma o i postumi dello stesso . importante sottolineare che la nostra casistica si riferisce al contenzioso relativo alla radiologia del dea e non consente di analizzare la percentuale di errore nelle diagnosi effettuate dai radiologi che lavorano nel reparto . in considerazione del fatto che , mediamente , si effettuano circa 50000 esami radiologici per anno in questa struttura , la percentuale di contenzioso si aggira intorno allo 0 , 0016% . 
la discrepanza tra le percentuali di errore riportate in letteratura e la nostra incidenza di contenzioso verosimilmente ascrivibile al fatto che , nella pratica clinica , solo in pochissimi casi si arriva allevidenza del danno da errore e , quindi , alla richiesta risarcitoria . riteniamo comunque che rimanga lutilit dellanalisi da noi effettuata . 
questa infatti ha consentito di rivisitare alcune prassi amministrative e riconoscere alcune criticit organizzative , tecniche o interpretative che ci hanno portato a individuare strumenti che speriamo atti a ridurre ulteriormente il gi basso livello di contenzioso ed a permettere la creazione di una pi dettagliata mappa del rischio , con la conseguente rivalutazione di premi e franchigie , al fine di favorire il recupero di risorse per lassistenza . 
802810 published online : 18 september 2009 springer - verlag 2009 radiological features of complications of laparoscopic adjustable gastric banding caratteristiche radiologiche delle complicanze del bendaggio gastrico per via laparoscopica t . 
bellomi1 , 2 1department of radiology , european institute of oncology , via ripamonti 435 , 20141 milan , italy 2school of medicine , university of milan , milan , italy 3department of pathology and laboratory medicine , european institute of oncology , milan , italy 4department of clinical haemato - oncology , european institute of oncology , milan , italy 5breast imaging unit , department of radiology , european institute of oncology , milan , italy correspondence to : s . 
magnetic resonance imaging ( mri ) features of these malignancies can be relevant in establishing the extent of disease and planning the appropriate therapeutic strategy , usually represented by chemoand radiotherapy , rather than surgery . 
for mass - like lesions , kinetic curve assessment of initial rise showed slow enhancement in one lesion , rapid enhancement in four lesions and medium enhancement in one lesion . 
mri features of primary breast lymphomas in this study cohort suggest that the occurrence of a pbnhl should be considered in the presence of large enhancing lesions of the breast , especially if associated with skin thickening . 
le caratteristiche alla risonanza magnetica ( rm ) di queste neoplasie possono essere importanti nello stabilire lestensione della malattia e nel pianificare la pi efficace strategia terapeutica , che di solito rappresentata da chemio - radioterapia , piuttosto che dallescissione chirurgica . 
il diametro principale medio delle lesioni alla rm risultato di 44 mm ( range 1269 ) ; 6 lesioni hanno mostrato un enhancement di tipo nodulare ; 1 lesione ha mostrato un enhancement di tipo non - nodulare . 
per le lesioni nodulari , la fase iniziale della curva contrastografica dellintensit del segnale nel tempo ha mostrato un enhancement lento in 1 lesione , intermedio in 1 lesione , rapido in 4 lesioni . 
le caratteristiche rm dei linfomi primitivi mammari riscontrate nella nostra casistica non si sono 916 radiol med ( 2009 ) 114 : 915924 in the assessment of response to therapy and diagnosis of recurrence . keywords primary breast lymphoma breast mri dimostrate patognomoniche della patologia , tuttavia la presenza di un linfoma primitivo mammario dovrebbe essere presa in considerazione in caso di lesioni mammarie di grandi dimensioni , dotate di contrastenhancement , specie se associate ad ispessimento cutaneo . la rm ha inoltre un ruolo importante nella valutazione della risposta alla terapia e nella diagnosi di recidiva . parole chiave linfoma mammella rm introduction introduzione primary lymphomas of the breast ( pbnhl ) are uncommon , accounting for 0.04%0.05% of all breast malignancies and < 1% of all non - hodgkins lymphomas . 
diagnostic imaging of these malignancies is particularly relevant in establishing disease extent and planning the most effective therapeutic strategy , which relies on chemotherapy plus radiotherapy , sparing patients unnecessary and potentially harmful surgical procedures . 
mammographic and ultrasonographic imaging findings of pbnhl have been reported to be nonspecific [ 2 , 3 ] , whereas mri findings have been described in single case reports [ 48 ] or in a study analysing multiple diagnostic modalities , where mri was performed in one case only [ 9 ]  . 
 the aim of this study was to ascertain the occurrence of specific mri features in pbnhl and assess the importance of mri in studying this rare pathology . i linfomi primitivi della mammella sono rari , costituendo lo 0 , 04%0 , 05% di tutte le neoplasie maligne della mammella e meno dell1% di tutti i linfomi non - hodgksolo l1% dei pazienti che si presentano con malattia extranodale ha un coinvolgimento mammario [ 1 ]  . 
limaging diagnostico di queste lesioni pu essere particolarmente rilevante nello stabilire lestensione della malattia e nel pianificare la strategia terapeutica pi efficace , che si fonda su chemioterapia e / o radioterapia , piuttosto che su procedure chirurgiche , non necessarie e potenzialmente dannose . 
limaging pu avere inoltre un ruolo importante nella valutazione della risposta alle terapie e nella diagnosi di recidiva . gli esami diagnostici oggi a disposizione per i tumori mammari sono rappresentati da mammografia , ecografia e risonanza magnetica ( rm )  . 
laspetto mammografico ed ecografico dei linfomi primitivi mammari risultato non specifico [ 2 , 3 ] , mentre laspetto rm stato descritto solo in singoli case report [ 48 ] e in uno studio che ha valutato le altre modalit diagnostiche ma la rm in un unico caso [ 9 ]  . 
ci si propone inoltre di valutare limportanza del contributo della rm nello studio di tale patologia rara . materials and methods patients materiali e metodi pazienti all patients provided signed informed consent , including the possibility of use of anonymous data for scientific purposes . 
seven patients with pbnhl who underwent a breast mri examination during the diagnostic pretreatment workup were retrospectively retrieved from the november 2001 to november 2007 database of our radiology department . 
the diagnosis of p bnhl was obtained by biopsy ( n = 4 ) or by surgery ( n = 3 ) according to : ( 1 ) specific morphological features , such as size , nuclear features , diffuse or follicular architectural pattern of proliferation ; ( 2 ) immunophenotypical features , such as the use of antibodies recognising the cd3 , cd5 , cd10 , cd20 , cd23 and tutte le pazienti hanno sottoscritto il consenso informato per lesame rm con contrasto e un consenso informato generico comprensivo della possibilit di utilizzo dei dati acquisiti e resi anonimi per scopi scientifici . 
dai database disponibili presso la divisione di radiologia relativi alle rm mammarie eseguite tra novembre 2001 e novembre 2007 , sono state selezionate retrospettivamente sette pazienti con linfoma mammario primitivo , sottoposte a rm durante liter diagnostico pree post - trattamento . 
la diagnosi di linfoma mammario primitivo era stata ottenuta su prelievi bioptici in 4 casi e sul pezzo chirurgico in 3 casi , sulla base di specifiche analisi basate sullo studio della morfologia cellulare ( dimensione , caratteristiche dei nuclei e crescita follicolare o diffusa ) ; sulle caratteristiche radiol med ( 2009 ) 114 : 915924 ki - 67 antigens ; and ( 3 ) according to molecular analyses , such as evaluation of the ig heavy chain gene rearrangement by polymerase chain reaction analysis at fr2 and fr3a . 
 breast mri technique all mri examinations were performed on a 1 - t signa horizon lx ( ge medical systems , milwaukee , wi , usa ) in use during the period considered ( 20012007 )  . 
the imaging sequence included a localising sequence followed by coronal t1 - weighted fatsuppressed fast spoiled gradient - echo sequences without breast compression with the following parameters : tr = 7 ms , te = 1.6 ms , flip angle = 10 , ti = 25 ms , receiver bandwidth = 32 khz , nex = 1 , matrix = 320320 , fov = 3618 cm . slice thickness ranged between 2 mm and 3 mm according to the volume of the entire breast in order to maintain the single volume acquisition time within 2 m the same sequence was acquired once before and five consecutive times starting 10 s after rapid intravenous contrast injection of 0.1 mmol / kg gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa ) ( magnevist bayer schering , germany ) at a flow rate of 2 ml / s , followed by a 20 - ml saline flush at the same flow rate . 
relative enhancement ( percentage changes of signal intensity course ) was calculated according to the following formula : sicsi / si100 , where sic and si represent signal intensities after and before contrast administration , respectively . interpretation of mri findings and lesion classification two radiologists retrospectively reviewed each preand post - treatment breast mri examination in consensus on a digital picture - archiving and communication system diagnostic workstation ( dynacad , invivo , orlando fl , usa ) also evaluating the maximum intensity projection ( mip ) images generated from the subtraction images . 
for each lesion , maximum diameter and longest orthogonal diameter in the same plane and distances of lesion to skin , to nipple and to chest wall were measured on the screen by using electronic callipers . 
 immunofenotipiche ( usando anticorpi specifici per gli antigeni cd3 , cd5 , cd10 , cd20 , cd23 e ki67 ) e sulle caratteristiche molecolari ( valutazione del riarrangiamento del gene codificante per le catene pesanti delle immunoglobuline tramite analisi pcr [ polymerase chain reaction ] delle regioni fr2 e fr3a )  . 
 risonanza magnetica tutti gli esami sono stati acquisiti con lapparecchio rm horizon lx 1t ( ge medical systems , milwaukee , wi , usa ) , in uso durante il periodo in esame ( 20012007 )  . 
dopo la sequenza di localizzazione sono state acquisite sezioni coronali fspgr t1 pesate con soppressione del grasso , senza compressione delle mammelle , secondo i seguenti parametri : tr = 7 ms , te = 1 , 6 ms , flip angle = 10 , ti = 25 ms , banda di ricezione = 32 khz , nex = 1 , matrice = 320320 , fov = 3618 c lo spessore delle sezioni variato da 2 a 3 mm , a seconda dello spessore complessivo della mammella , per mantenere il tempo di acquisizione totale inferiore ai 2 minuti per ciascuna acquisizione di volume . 
la stessa sequenza stata acquisita nelle condizioni basali e cinque volte dopo iniezione endovenosa rapida di mezzo di gadopentetato dimeglumina ( magnevist , bayer schering , germania ) 0 , 1 mmol / kg , velocit di flusso = 2 ml / s , seguita da un bolo di 20 ml di soluzione salina alla stessa velocit di flusso . 
lenhancement relativo ( percentuale di variazione dellintensit del segnale iniziale e tardivo ) stato calcolato sulla base della seguente formula : sic - si / si100 , dove sic e si rappresentano le intensit di contrasto del segnale rispettivamente dopo e prima la somministrazione di contrasto . interpretazione delle immagini rm e classificazione delle lesioni due radiologi hanno rivalutato retrospettivamente ciascun esame rm della mammella pree post - trattamento su una workstation di archiviazione digitale delle immagini ( dynacad , invivo corp . , orlando fl , usa ) , dove sono state valutate anche le ricostruzioni mip ( massima intensit di proiezione ) generate dalle immagini di sottrazione . 
per ogni lesione sono stati misurati a monitor : il diametro maggiore e il diametro massimo ad esso ortogonale nello stesso piano ; le distanze della lesione dalla cute , dal capezzolo e dalla parete toracica . 
 the noncontrast t1 appearance of lesions was described ogni lesione stata valutata secondo i criteri rm di 918 radiol med ( 2009 ) 114 : 915924 iso - , hyperor hypointense relative to breast parenchyma . 
the presence or absence of skin thickening in the same quadrant as the lesion was recorded and , if present , its distance from the lesion was also recorded . each lesion was evaluated according to the mr lexicon for enhancing breast lesions [ 10 , 11 ]  . 
for mass - like enhancement , descriptors used were shape ( round , oval , lobular , irregular or spiculated ) , margins ( smooth , lobular , irregular or spiculated ) and internal enhancement ( homogeneous , heterogeneous , rim enhancement , bright internal enhancing septations , dark septations ) [ 10 ]  . 
for nonmass enhancement , shape and borders are not assessable , and descriptors used were : distribution of contrast enhancement ( linear , linear branching , segmental , regional , patchy or diffuse enhancement ) [ 10 , 12 ] and internal contrast enhancement ( for linear or linear branching duct margins defined as smooth , undulating , or irregular borders , for segmental , regional , patchy or diffuse enhancement defined as homogenous , heterogeneous , clumped and stippled ) [ 10 , 11 ]  . kinetic curve assessment was performed by placing a freehand region of interest ( roi ) including the entire lesion in case of homogeneous internal pattern of contrast enhancement and on the most enhancing area for all other types of internal enhancement . 
delayed - phase enhancement was rated as persistent ( when curves exhibited steady signal intensity increase ) , plateau ( when curves exhibited fast early upstroke followed by plateau after the third postcontrast minute ) and washout ( when curves exhibited fast early upstroke followed by a loss of signal intensity after the third postcontrast minute )  . 
 an overall assessment category was eventually attributed to each lesion according to the mri breast imaging reporting and data system ( bi - rads ) categories introduced by the american college of radiology [ 11 , 1315 ]  . assessment categories included six classes : i = negative findings , ii = benign finding , iii = probably benign finding , iv = suspicious abnormality , v = highly suggestive of malignancy and vi = proven malignancy [ 14 ]  . 
 results the study population included seven women ( mean age 63 , range 4477 years ) with a histological diagnosis of pbnhl classified as follows : five diffuse large b - cell lymphoma ( dlbcl ) , one dlbcl with a focal ( accounting for 5% of neoplastic cells ) marginal zone [ mucosa - associated classificazione delle lesioni dotate di contrast - enhancement riportati in letteratura e internazionalmente accettati [ 10 , 11 ]  . 
secondo tali criteri le lesioni dotate di contrast - enhancement vengono classificate come : lesioni con enhancement nodulare ( mass - like enhancement ) , e lesioni con enhancement non nodulare ( non - mass like enhancement ) [ 10 , 11 ]  . per lenhancement nodulare , vengono comunemente valutate le seguenti caratteristiche : forma ( definita come rotonda , ovale , lobulare , irregolare , spiculata ) ; margini ( definiti come regolari , lobulari , irregolari o spiculati ) ; enhancement interno ( definito come omogeneo , eterogeneo , ad anello , con setti intralesionali contrastati , con setti intralesionali non contrastati ) [ 10 ]  . 
per le lesioni con enhancement non nodulare , forma e margini non sono valutabili , e pertanto in tali lesioni vengono comunemente valutate le seguenti caratteristiche : distribuzione del contrast enhancement ( definita come lineare , ramificata , segmentario , regionale , in regioni multiple , diffusa ) [ 10 , 12 ] ; enhancement interno ( definito a margini lisci , ondulati o irregolari per le lesioni lineari e ramificate ; definito come omogeneo , eterogeneo , addensato o puntinato per le lesioni segmentarie , regionali , in regioni multiple o diffuse ) [ 10 , 11 ]  . 
 lanalisi dinamica stata effettuata nelle lesioni nodulari posizionando una roi a mano libera comprendente tutta la lesione in caso di enhancement interno omogeneo , e nellarea dotata di maggior contrast - enhancement per tutti gli altri tipi di contrast - enhancement interno . 
lenhancement tardivo stato classificato come : persistente quando la curva mostrava un incremento dellintensit del segnale costante ; con plateau quando la curva mostrava una fase iniziale di incremento rapido seguita da una stabilit della curva anche dopo il terzo minuto dalliniezione del mezzo di contrasto ; con wash out quando la curva mostrava una fase iniziale di incremento rapido seguita da una diminuzione dellintensit del segnale dopo il terzo minuto dalliniezione del mezzo di contrasto . 
tale classificazione include 6 categorie : i = reperto negativo , ii = reperto francamente benigno , iii = reperto probabilmente benigno , iv = reperto sospetto per malignit , v = reperto altamente suggestivo di malignit , vi = reperto con diagnosi istologica di malignit [ 14 ]  . risultati lo studio ha incluso 7 donne ( et media 63 , range di et 4477 ) con diagnosi istologica di linfoma mammario primitivo , classificato come segue : 5 linfomi a grandi cellule b , 1 linfoma a grandi cellule b con una piccola componente della zona marginale ( che ammontava a meno del 10% delle cellule neoplastiche ) , 1 linfoma extranodale della zona marginale ( malt - linfoma )  . 
tutte le lesioni erano clinicamente palpabili prima del trattamento e localizzate come segue : 2 supero - esterne a destra , 1 supero - esterna sinistra , 1 radiol med ( 2009 ) 114 : 915924 lymphoid tissue ( malt ) ] component and one extranodal marginal zone ( malt ) lymphoma . 
all lesions were clinically palpable before treatment and were located as follows : two right upper - outer , one left upper - outer , one left upper - internal , one right lower - outer , one left lowerinternal and one right upper - internal . 
all patients with a diffuse large b - cell lymphoma received acod ( adriamicin - ciclophosphamide - vincristine - deltacortene ) [ chop - like chemotherapy ( ciclophosphamide - hydroxydaunorubicina - onsovin - prednisone ) ] for four to six cycles , followed by 4446 gy radiotherapy of the breast and positive nodes if present . 
 posttreatment mri examinations showed complete remission of local disease at the end of therapy for all seven patients , whereas for two of them ( one large b - cell lymphoma , one malt lymphoma ) , mri detected recurrence in the contralateral breast . 
the mean mri longest diameter was 44 mm ( range 1269 ) , and the mean longest orthogonal diameter measured in the same plane was 32 mm ( range 943 )  . 
the mean distance from the skin , the nipple and the chest wall was 15 mm ( range 423 ) , 43 mm ( range 670 ) and 21 mm ( range 549 ) , respectively . 
tutte le pazienti con linfoma diffuso a grandi cellule b hanno ricevuto chemioterapia acod ( adriamicin - ciclophosphamide - vincristinedeltacortene ) [ chop - like ( ciclophosphamide - hydroxydaunorubicina - onsovin - prednisone ) ] , per 4 o 6 cicli , seguita da 4446 gy di radioterapia della mammella e di eventuali linfonodi positivi , quando presenti . 
 gli esami rm post - trattamento hanno mostrato remissione completa della malattia locale alla fine delle terapie per le 7 pazienti , ma per 2 di loro ( 1 con linfoma a grandi cellule b , 1 con malt - linfoma ) la rm di follow - up ha dimostrato una recidiva nella mammella controlaterale . queste due pazienti sono state pertanto nuovamente sottoposte a chemioterapia , dopo la quale hanno mostrato remissione completa . 
le distanze medie dalla cute , dal capezzolo e dalla parete toracica sono risultate rispettivamente di 15 mm ( range 423 ) , 43 mm ( range 670 ) e 21 mm ( range 549 )  . 
laspetto t1 pre - contrasto risultato iso - intenso rispetto al parenchima mammario in cinque lesioni ( 4 linfomi a grandi cellule b , 1 maltlinfoma ) e iper - intenso in due lesioni ( entrambe linfomi a grandi cellule b )  . 
in 3 / 7 casi ( due linfomi diffusi a grandi cellule b e un lnh con una piccola componente della zona marginale ) , si osservato ispessimento cutaneo , la cui distanza dalla lesione era di 10 , 16 e 17 mper le caratteristiche rm di contrast - enhancement , sei lesioni sono state classificate come nodulari ( 5 linfomi a grandi cellule b , 1 malt - linfoma ) ; e una lesione come non - nodulare ( linfoma a grandi cellule b )  . 
per quanto riguarda le lesioni nodulari , la forma stata classificata come segue : rotonda n = 2 , lobulare n = 2 , ovale n = 1 , irregolare n = 1 . 
i margini sono stati valutati come : regolari n = 2 , irregolari n = 3 , spiculati n = 1 . lenhancement delle lesioni nodulari stato classificato come : omogeneo n = 2 , eterogeneo n = 2 , ad anello n = 2 . landamento iniziale della curva dinamica del segnale ha mostrato : enhancement lento n = 1 , enhancement intermedio n = 1 , enhancement rapido n = 4 . 
il picco medio di enhancement risultato del 110% ( range 78162 ) , dove il picco maggiore ( 162% ) apparteneva allunico linfoma a grandi cellule b che ha mostrato anche wash out tardivo . per lunica lesione con enhancement non nodulare , che era un linfoma a grandi cellule b , la distribuzione dellenhancement stata definita come enhancement in regioni multiple , con caratteristiche interne di tipo puntinato . 
1a - c post - gadolinium t1 - weighted breast magnetic resonance imaging ( mri ) ( a ) of a 69 - mm b - cell primary right breast lymphoma showing a masslike enhancement area , with lobular shape , irregular margins and heterogeneous contrast enhancement . 
kinetic curve assessment based on a freehand region of interest ( roi ) placed on the entire area ( b ) shows a 128% initial rise and a delayed plateau ( c )  . 
1a - c immagine rm mammaria t1 pesata post - gadolinio ( a ) di linfoma primitivo a grandi cellule b della mammella destra di 69 mm , che mostra un area solida , con forma loblulare , margini irregolari , ed eterogeneo contrastenhancement . 
la valutazione della curva dinamica basata sul posizionamento manuale di una roi nellintera area ( b ) mostra una crescita iniziale del 128% e un plateau tardivo ( c )  . 
in a recent study performed at stanford university and encompassing 10 , 125 lymphoma patients admitted from 1981 to 2005 , only 51 cases had lymphoma involving the breast [ 17 ]  . 
as a consequence , there are few data concerning the radiological features of breast lymphoma , which mainly arise from mammographic and ultrasonographic examinations [ 2 , 3 , 6 , 7 , 9 , 18 , 19 ] , which led to the conclusion that pbnhl does not show specific radiological features [ 2 , 3 ]  . 
described one or more than one primitivo della mammella , con o senza diffusione ai linfonodi regionali , in assenza di linfoma pre - esistente o simultaneo in altre sedi [ 2 , 4 ]  . 
il linfoma mammario , sia come sede primitiva che come sede secondaria di malattia , raro , rappresentando lo 0 , 04%0 , 53% di tutti i tumori maligni della mammella [ 5 , 16 ]  . 
la maggior parte di tali lavori ha valutato solo esami mammografici e ecografici [ 2 , 3 , 6 , 7 , 9 , 18 , 19 ] , e sostanzialmente tutti concordano sul fatto che i linfomi primitivi della mammella non hanno aspetti radiologici specifici [ 2 , 3 ]  . 
per quanto riguarda gli aspetti mammografici , i risultati descritti non sono omogenei : alcuni autori hanno descritto una o pi lesioni ben circoscritte senza microcalcificazioni e con reazione desmoplastica [ 2 ] ; con densit parenchimale diffusamente aumentata , anche associata ad ispessimento cutaneo [ 2 , 5 ] ; altri radiol med ( 2009 ) 114 : 915924 relatively well - circumscribed lesion without calcifications or desmoplastic reaction [ 2 ] ; soyupak et al . 
described bilateral miliary densities , especially during secondary involvement [ 20 ]  . at ultrasonography , primary and secondary breast lymphomas have been described as well or as poorly defined masses with a hypoto hyperechoic appearance , focal or diffuse heterogeneous parenchymal involvement [ 21 ] and variable attenuation [ 7 ]  . 
due to the rarity of this condition , mri findings of pbnhl have been previously described only as single case reports [ 48 ] or as single cases included in a larger series [ 9 ]  . 
in our study cohort , 2 / 7 lesions ( both dlbcl ) were hyperintense relative to breast parenchyma . a recent study has emphasised the importance of mri lesion size , suggesting that it may be helpful in predicting the likelihood of malignancy . 
this finding was not compared with mammographic and ultrasonographic images of the same time period because they were not available , but it was not mentioned in the radiological report and therefore probably not apparent . 
 in agreement with the above - mentioned studies [ 48 ] showing a rapid and strong contrast enhancement with an increase in signal intensity of > 80% in the first part of the curve , in our series , the mean peak of enhancement was 110% . 
unfortunately , this finding is generically expected for all malignant lesions , regardless of histological type , autori hanno descritto lesioni con margini netti o lievemente irregolari [ 8 ] ; altri ancora hanno descritto un coinvolgimento linfomatoso secondario con densit bilaterali miliariformi [ 20 ]  . 
 laspetto ecografico dei linfomi mammari primitivi o secondari stato variamente descritto come masse da ipoa iperecogene , ben defnite o poco definite , con coinvolgimento parenchimale eterogeneo focale o diffuso [ 21 ] , e con attenuazione variabile del fascio ultrasonoro [ 7 ]  . 
a causa della relativa rarit di questa patologia , gli aspetti rm dei linfomi primitivi sono stati finora descritti solo come report di singoli casi [ 48 ] o come singoli casi inclusi in casistiche pi numerose [ 9 ]  . 
nella nostra casistica , 2 / 7 lesioni ( entrambe linfomi a grandi cellule b ) hanno mostrato iperintensit rispetto al parenchima mammario , mentre le rimanenti 5 hanno mostrato sostanziale isointensit . 
tale reperto rm non stato da noi confrontato con gli esami ecografico e mammografico dello stesso periodo in quanto non disponibile , tuttavia esso non era riportato nel referto e pertanto verosimilmente non evidenziabile . 
 in accordo coi suddetti case report [ 48 ] che descrivevano un contrast - enhancement rapido e marcato dei linfomi mammari primitivi , con crescita iniziale dellintensit del segnale maggiore dell80% , nella nostra casistica il picco medio di enhancement stato del 110% . 
2a , b postgadolinium t1 - weighted breast mri of a b - cell primary left breast lymphoma showing a 12 - mm mass - like enhancing lesion , with round shape , smooth margins and homogenous contrast enhancement ( a )  . 
kinetics of the lesion , based on a freehand region of interest ( roi ) ( b ) showed a 92% initial rise and a postinitial plateau ( c )  . 
2a , b imamgine rm mammaria t1 post - gadolinio di un linfoma primitivo a cellule b della mammella sinistra , che mostra una lesione solida di 12 mm , con forma rotonda , margini regolari e omogeneo contrast - enhancement ( a )  . la cinetica della lesione , basata sul posizionamento manuale di una roi ( b ) , mostrava una crescita iniziale del 92% ed un plateau tardivo ( c )  . 
 at variance with a previous study [ 9 ] where the only pbnhl analysed by mri showed a washout , in this series , only one lesion showed a washout ( dlbcl ) , whereas the remaining lesions showed a plateau in five cases . 
in our series , we did not find multifocality or multicentricity at the time of diagnosis , but the diagnosis of multifocality or multicentricity of breast lymphomas may be less important than for other breast malignancies in that surgery is not the most appropriate therapy . 
however , the possibility of a differenza di uno studio precedente [ 9 ] , in cui il solo linfoma mammario analizzato con rm mostrava un wash out nella fase tardiva della curva contrastografica , nella nostra casistica soltanto 1 lesione ( linfoma a grandi cellule b ) ha mostrato un wash out , mentre le altre 5 lesioni con contrast - enhancement di tipo nodulare hanno mostrato un plateau . 
 [ 9 ] potrebbe dipendere dalle grandi dimensioni della lesione da lui analizzata ( 11 , 6 cm ) , che sostituiva quasi lintera mammella mentre le nostre lesioni , pur avendo un diametro mediamente grande ( 44 mm ) comprendevano un range tra 12 e 69 mm . relativamente al noto importante contributo della rm nella valutazione di multicentricit e multifocalit dei tumori mammari , kiresi et al . 
nella nostra casistica non erano presenti tumori multifocali alla diagnosi e comunque la diagnosi di multifocalit o multicentricit dei linfomi rispetto ad altri tumori mammari pu radiol med ( 2009 ) 114 : 915924 demonstrating multifocal and multicentric lesions by mri may be helpful during staging in order to eventually correctly evaluate response to treatment . 
indeed , the examination performed after treatment showed complete remission in all patients and , during follow - up , showed the occurrence of a contralateral relapse in two patients , both of whom underwent additional treatments , achieving a complete final remission . 
nevertheless , this technique may hamper immunophenotyping and molecular analyses , which are mandatory to correctly diagnose and subclassify nonhodgkins lymphoma lesions [ 2426 ] and to plan subsequent radiotherapy and chemotherapy instead of surgery . 
thus , when mri interpretation of enhancing lesions of the breast includes pbnhl in the differential diagnosis , the patient should undergo a core biopsy rather than an fnac . treatments , which include a possible limitation of our study is the lack of data relative to the t2 appearance of lesions . 
 another limitation of this study is the lack of data relative to the mammographic and ultrasonographic appearance of the lymphoma lesions and to the consequent lack of a comparison among different diagnostic methods . 
unfortunately , the cases included in this study had been evaluated by mammography and ultrasound in other hospitals , and only the written reports without images were available . however , this limitation may lead to a possible future study comparing mammographic , sonographic and mri appearance of breast lymphomas . 
 in conclusion , our data suggest that the occurrence of a pbnhl should be kept in mind , especially for large enhancing lesions and in the presence of skin thickening , in order to plan the most accurate diagnostic procedures , which should include core biopsy rather than fine - needle aspiration . 
furthermore , mri may also have an important role in monitoring the response to therapy and during follow - up in the diagnosis of recurrence . essere meno importante , in quanto la terapia pi appropriata non chirurgica . 
tuttavia la possibilit della rm di dimostrare eventuali lesioni multifocali e multicentriche pu essere importante nella valutazione basale per la valutazione della risposta alle terapie . in accordo a quanto affermato da espinosa et al . 
infatti , gli esami rm eseguiti dopo trattamento hanno mostrato una completa remissione di malattia in tutte le pazienti e , durante il follow - up , lesame rm ha mostrato la presenza di recidiva controlaterale in due pazienti , che sono state sottoposte ad ulteriori cicli di terapia medica , con successiva remissione completa . la diagnosi di una massa tumorale mammaria spesso basata sullanalisi citologica da ago - aspirato . 
tuttavia , lago - aspirato pu non consentire lesecuzione di analisi immunofenotipiche e molecolari , che sono fondamentali per la corretta diagnosi e classificazione dei linfomi non - hodgkin [ 2426 ] e per la conseguente pianificazione terapeutica che per i linfomi si basa su chemioterapia e radioterapia e non sulla chirurgia . 
pertanto , quando linterpretazione rm di lesioni mammarie include i linfomi nella diagnosi differenziale , potrebbe essere opportuno eseguire una biopsia piuttosto che un ago - aspirato . un limite del presente studio la mancanza di dati relativi allaspetto dei linfomi mammari nelle sequenze t2 . questo dovuto al fatto che la selezione delle pazienti con diagnosi istologica di linfoma mammario primitivo stata fatta retrospettivamente . 
tale limite rappresenta un possibile spunto di studio futuro che potrebbe confrontare i reperti mammografici , ecografici e rm dei linfomi primitivi della mammella . in conclusione , le caratteristiche rm dimostrate dai linfomi primitivi mammari nella nostra casistica non sono patognomoniche della patologia . 
tuttavia i nostri dati suggeriscono che la presenza di un linfoma mammario primitivo dovrebbe essere presa in considerazione in presenza di lesioni di grandi dimensioni dotate di contrastenhancement , specie se associate ad ispessimento cutaneo . tale sospetto dovrebbe suggerire lesecuzione di una biopsia invece che di un ago - aspirato per unaccurata diagnosi e pianificazione terapeutica . 
sartor. springer - verlag berlin heidelberg , 2009 isbn 978 - 3 - 540 - 32983 - 1 published online : 15 september 2009 springer - verlag 2009 the monumental and revolutionary steps in the development of technical procedures in coronary radiology that have taken place in the past few years are properly and clearly depicted in the second edition of this book . 
 to study and evaluate coronary events nowadays there is not only the old - fashioned invasive and in some respects dangerous arteriography ; but also non invasive techniques ( multidetector ct angiography and dual source tomography , 2d and 3d visualization techniques , mri coronary angiography ) that quikly provide and with no danger to the patient ( beware in any case high dose multidetector ct ) all possible information for the clinician and radiologist . 
all these modalities may in any case be implemented by conventional catheterization , quantitative angiography as well as intravascular ultrasound . following the introductory chapter on coronary anatomy , the results that can be obtained with all the above techniques are well described in two chapters ( invasive coronary catheterization ; non - invasive coronary imaging ) subdivided in ten sections . 
one longer chapter ( non - invasive measurements of coronary atherosclerosis ) which is divided in 6 sections , deals with the problem of coronary atherosclerosis and calcifications ( pathophysiology , detection , measure , epidemiology , calcium as indicator of disease , screening ) and how to evaluate and treat these according to the recommendations of the us and european societies of cardiac imaging and radiology as well as the cardiology societies on both sides of the ocean . the last chapter provides an overview of the problems with image visualization , how to obtain , store , retrieve and use these in the daily practice in the ever increasing and demanding world of hospital generated images ( dicom , pacs etc . ) many beautiful black and white and colour images are to i progressi giganteschi ed in un certo modo rivoluzionari nello sviluppo delle tecniche di indagine per lo studio delle coronarie che si avuto negli ultimi anni messo ben in evidenza e spiegato in modo chiaro nella seconda edizione di questo volume . 
montemezzi6 1centro di prevenzione senologica ( cps ) , po marzana , ulss 20 , verona , italy 2istituto di radiologia , universit degli studi di verona , policlinico g.b. 
di senologia clinica e screening mammografico , dipartimento di radiodiagnostica , trento , italy 4registro tumori , istituto oncologico veneto ( iov ) , padova , italy 5istituto per lo studio e la prevenzione oncologica ( ispo ) , firenze , italy 6dipartimento interaziendale di radiologia , verona , italy correspondence to : s . 
volta 171 , 50131 firenze , italy , tel . : + 39 - 055 - 5012275 , fax : + 39 - 055 - 5001623 , e - mail : stefano - ciatto@gmail.com received : 17 october 2008 / accepted : 13 january 2009 / published online : 23 june 2009 springer - verlag 2009 abstract purpose . 
le mammografie refertate come negative precedenti i ci sono state sottoposte a revisione con modalit cieca ( mescolate casualmente con controlli negativi in ragione 2 : 1 ) da tre radiologi esperti e classificati in base ai criteri delle linee guida europee ( oc = occulto , sm = segni minimi , es = errore di screening ) in base al giudizio di maggioranza . 
il tasso di incidenza proporzionale stato del 10 , 8% nel primo e del 40 , 0% nel secondo anno dellintervallo ( standard europeo rispettivamente < 30% o < 50% , )  . 
alla revisione i ci sono stati classificati come es , sm , o oc rispettivamente nel 15 , 0% , 14 , 0% , o 71 , 0% dei casi . 
la verifica degli indicatori precoci di efficacia basati sui ci fattibile in un programma corrente di screening e dovrebbe divenire una procedura di routine . parole chiave carcinoma mammario screening mammografia carcinomi di intervallo introduction introduzione interval cancers ( ics ) account for a relatively infrequent event in mammography screening practice , their frequency being reported to be lower than 0.1% of screened subjects [ 13 ]  . 
ics are categorised according to the year of diagnosis in the interval ( first or second ) and classified according to the presence of different degrees of interpretation error at review . 
ics , however , are the most reliable indicators of screening programme sensitivity . monitoring ic is recommended as a standard procedure by several institutions [ 13 ] , and ic surveys have been reported by some italian screening programmes [ 46 ]  . 
 ic survey is based on the assessment or their frequency ( proportional incidence : ratio of observed ic to cancers expected according to underlying baseline incidence , in absence of screening ) and on the review of screening mammograms preceding ic , originally reported as negative , and their classification according to categories predefined by the european guidelines [ 3 ]  . 
 our study aimed to report the proportional incidence and review of ic observed in an italian screening programme during 20002006 . materials and methods i carcinomi intervallo ( ci ) costituiscono un evento relativamente raro nella pratica dello screening mammografico , con un tasso inferiore allo 0 , 1% soggetti esaminati [ 13 ]  . definiti come tutti i carcinomi invasivi insorti a seguito di episodio negativo di screening e prima della successiva mammografia di screening , vengono categorizzati in base allanno di comparsa ( primo o secondo ) e classificati in base alla presenza o meno di un errore diagnostico alla revisione . 
il monitoraggio dei ci raccomandato come procedura standard da diverse istituzioni [ 13 ] ed stato oggetto di pubblicazione da parte di alcuni programmi di screening italiani [ 46 ]  . 
 lanalisi dei ci si basa classicamente sia sulla verifica della loro frequenza ( incidenza proporzionale , o rapporto tra ci osservati e carcinomi attesi in assenza di screening , questi ultimi pari alla incidenza di base ) , che sulla revisione dei radiogrammi di screening precedenti il ci , refertati come negativi , e classificati in base a categorie predeterminate , definite nelle linee guida europee [ 3 ]  . il presente studio si ripropone di presentare i dati relativi alla incidenza proporzionale e alla revisione dei ci osservati in un programma di screening italiano dal 2000 al 2006 . a population - based mammography screening programme , inviting resident women aged 5059 years , has been ongoing in verona since 1999 and is run by the centre for breast prevention of marzana hospital , local health unit 20 . 
the main characteristics of the programme have been already materiali e metodi un programma di screening mammografico biennale di popolazione rivolto alle donne residenti , dai 50 ai 69 anni di et , in corso a verona dal 1999 , gestito dal centro di radiol med ( 2009 ) 114 : 907914 reported : the most original feature is real - time diagnostic assessment of screen positives , a practice associated with higher recall rates [ 7 ] but also with good sensitivity levels , as recently reported for some programmes of the veneto region [ 6 ]  . 
this study refers to a period when single reading was in use , whereas conventional double reading has been recently adopted , according to european guidelines [ 3 ]  . the studied series was identified in the computerised database of the screening programme , and consists of 85 , 380 negative screening episodes during 20002006 . 
in order to identify ic occurring within 2 years of a negative screening episode , the screening database was linked to different sources , namely : ( a ) screening programme archives of detected cancers ( the screening unit also runs a breast clinic for symptomatic or self - referring subjects from the same population area ) ; ( b ) cancer registry archives of the veneto oncological institute ; and ( c ) hospital discharge records ( hdr ) made available from the veneto regional health authorities . 
the latter hdr archive , originally created for administrative purpose , is increasingly used as a support for clinical studies ( and for cancer registries ) , as it provides the final diagnosis and is rapidly available ( within a few months ) after discharge . 
hdr use to identify ic has been recently recommended in a ministry of health position paper [ 2 ] and has been employed with success in some italian screening experiences [ 5 , 6 ]  . ic proportional incidence was thus calculated as the ratio of observed ic ( identified according to the above - mentioned linkage process ) to cancers expected ( obtained by multiplying the age - specific underlying incidence rate by the number of women - year at risk )  . 
ic proportional incidence is a direct indicator of sensitivity according to the formula : sensitivity = 1 ( observed ic / expected cancers ) this formula is the most reliable to estimate screening sensitivity and is recommended by the european guidelines , which also provide reference standards for the maximum acceptable proportional incidence in the first ( reference < 30% ) or second ( reference < 50% ) year of the interval [ 3 ]  . finally , mammograms preceding ic were reviewed to assess radiologists responsibility . 
this number is different from the total of observed ic ( n = 95 ) considered to calculate proportional ic incidence as : ( a ) the review process also reviewed carcinomas in situ ( 7 of 100 cases ) , as recommended by european guidelines , which are excluded when assessing proportional incidence ; ( b ) some cases were not reviewed , as mammograms were not retrieved or had indelible marks that would have influenced review ; and ( c ) some reviewed cases were not included when assessing proportional incidence as they were too recent , occurring later than the considered period . 
le principali caratteristiche del programma sono gi state oggetto di pubblicazione : la pi peculiare certamente lesecuzione immediata degli approfondimenti diagnostici delle alterazioni rilevate alla mammografia , pratica che se risultata essere associata a un tasso di richiamo piuttosto elevato [ 7 ] consente comunque una buona sensibilit , come stimato in una recente valutazione di alcuni programmi della regione veneto [ 6 ]  . 
lo studio fa riferimento a un periodo in cui era in uso la lettura singola , recentemente implementata dalla doppia lettura in ottemperanza alle raccomandazioni europee [ 3 ]  . la casistica mammografica oggetto di studio stata identificata dallarchivio computerizzato del programma di screening ed pari a 85380 mammografie refertate come negative dal 2000 al 2006 . 
questultimo strumento , nato principalmente per uso amministrativo , viene sempre pi usato come supporto a studi clinici ( e a registri tumori ) , in quanto riporta la diagnosi di dimissione ed disponibile con breve latenza ( pochi mesi ) rispetto al ricovero . 
luso delle sdo per lidentificazione dei ci stato recentemente raccomandato da una position paper del ministero della salute [ 2 ] , ed stato gi usato con successo in esperienze di screening italiane [ 5 , 6 ]  . identificati in tal modo i ci nel biennio successivo allesame mammografico , si proceduto al calcolo dellincidenza proporzionale di ci : tale misura fa riferimento al rapporto tra ci effettivamente osservati e carcinomi attesi in assenza di screening ( questi ultimi calcolati in base agli anni - persona e ai tassi incidenza et specifici forniti dal registro tumori locale ) , corrisponde al reciproco della sensibilit , che viene calcolata secondo la formula : sensibilit = 1 ( ci osservati / carcinomi attesi ) tale formula quella pi affidabile per il calcolo della sensibilit ed raccomandata dalle linee guida europee che forniscono anche standard di riferimento per il rapporto osservati / attesi , pari ad un massimo del 30% per il primo anno , o del 50% per il secondo anno dellintervallo [ 3 ]  . infine sono stati rivalutati i radiogrammi di screening precedenti ai ci per verificare la presenza o meno di un 910 radiol med ( 2009 ) 114 : 907914 reviewed as : ( a ) screening error ( se : abnormality worthy of further diagnostic assessment ) ; ( b ) minimal sign ( ms : minimal changes , not enough to prompt diagnostic assessment , perceived by the reviewer only as a consequence of adopting a lower threshold for suspicion [ the attempt to maximise sensitivity is common in a test setting ] or with knowledge of ic side , site and features at diagnosis ) ; or ( c ) occult ( oc : no abnormality worthy of diagnostic assessment )  . 
as three reviewers were involved , review classification category was determined according to majority report : lesions identified by at least two reviewers were classified as se , lesions identified by one reviewer only were classified as ms and lesions not identified by any reviewer were classified as oc . 
involved reviewers ( a , b , c ) are expert radiologists currently involved in screening programmes and with at least 5 years of mammography practice , blinded to which were cases and controls in the set . 
table 1 shows observed ics and expected cancers , overall and by age group . observed / expected ratio ( o / e ) was 10.8% in the first and 40.0% in the second year of the interval . 
lo standard di buona pratica indicato nelle linee guida europee di una proporzione non superiore a 20 es ogni 100 ci sottoposti a revisione . essendo stato impiegato un numero dispari di revisori , la classificazione stata definita a maggioranza : sono stati classificati es le lesioni identificate da almeno 2 revisori , sm le lesioni identificate da un solo revisore , e oc le lesioni non identificate da alcun revisore . 
i tre revisori ( a , b , c ) sono radiologi esperti ( con almeno 5 anni di esperienza mammografica ) , coinvolti in programmi di screening di popolazione , e che non avevano visto in precedenza i casi in revisione . 
al fine di evitare una sovrastima dellerrore di interpretazione a maggior tutela del radiologo lettore , come raccomandato dal ministero della salute [ 2 ] , stata applicata la procedura della revisione cieca . tale procedura , che vede i casi di ci ( n = 100 ) mescolati a un elevato numero di controlli negativi verificati ( negativi anche allo screening successivo , n = 200 , in rapporto 2 : 1 ) , scelti a caso dalla stessa casistica di screening , risulta assai pi garantista per il radiologo lettore rispetto alla revisione semi - informata ( del solo esame di screening precedente il ci ) o informata ( del solo esame di screening precedente il ci , con disponibile anche la mammografia diagnostica che rivela lato , sede e morfologia del ci )  . 
positive predictive value for ic was 51.7% for se lincrocio con i diversi archivi ha portato allidentificazione per il periodo 20002006 di 95 ci , 28 comparsi nel primo anno dellintervallo e 67 nel secondo anno . 
la tabella 1 presenta i ci osservati e i carcinomi attesi , complessivi e per classe di et . il rapporto osservati / attesi risultato essere 10 , 8% per il primo e 40 , 0% per il secondo anno . 
assumendo lo stesso numero di anni - paziente nel primo e secondo anno , il rapporto osservati / attesi e la sensibilit nellintervallo biennale risultano rispettivamente 25 , 4% e 74 , 6% . i 100 casi e i 200 controlli selezionati per la revisione non differiscono significativamente per et ( et media casi = 59 , 7 , controlli = 57 , 0 anni , p = 0 , 58 ) , mentre differiscono significativamente per densit radiologica ( bi - rads casi : d1 = 41% , d2 = 32% , d3 = 17% , d4 = 10% ; controlli : d1 = 58% , d2 = 25% , d3 = 12 , 5% , d4 = 4 , 5% ) quando si considerino quattro categorie di densit ( d1 / 2 / 3 / 4 ; p = 0 , 02 ) e con significativit marginale quando se ne considerino due ( d1 - 2 / 3 - 4 ; p = 0 , 07 )  . 
i risultati della revisione dei radiogrammi di screening negativi sono riportai nella tabella 2 . la frazione di ci classificati come es stata del 15 , 0% , mentre la stessa categoria stata attribuita al 7 , 0% dei controlli negativi ( p = 0 , 04 )  . 
blind review of ic is the most correct methodology to assess potential reading errors [ 8 , 9 ] , as it tends to reproduce the current screening scenario , where radiologists are not aware of which cases will develop ic , among a large majority of true negative cases . 
blind review , recommended by the italian study group for mammography screening ( gisma ) [ 1 ] , has been recently suggested as a standard procedure by the italian ministry of health [ 2 ]  . 
 the choice of a 2 : 1 control / case ratio was motivated by the large number of cases to be reviewed and by the need to use a set of cases of a proper size to allow a relatively easy review process . 
the latter is no doubt higher than currently recommended at first screening ( 7% ) , although in the range of what is reported in similar studies [ 5 , 6 , 8 ]  . 
 la casistica in oggetto e sufficientemente ampia e studiata con una metodologia affidabile per la valutazione della performance del programma di screening in oggetto . lanalisi del tasso proporzionale dei ci nel primo e secondo anno successivo allo screening raccomandata dalle linee guida europee [ 3 ] , e lidentificazione dei ci mediante le sdo , raccomandata da autorit scientifiche e sanitarie nazionali [ 1 , 2 ] , risulta sufficientemente affidabile , dato il basso tasso di migrazione terapeutica extraregionale , ed stata gi usata con successo in altri studi analoghi [ 5 , 6 ]  . 
i tassi proporzionali di incidenza di ci osservati nel primo e secondo anno rientrano ampiamente nei limiti di sufficienza raccomandati ( primo anno 10 , 8% vs 30% raccomandato , secondo anno 40 , 0% vs 50% raccomandato )  . 
complessivamente la sensibilit del programma rispetto allintervallo biennale risulta essere del 74 , 6% , nella media rispetto a quanto osservato in centri di eccellenza [ 10 ]  . la revisione cieca dei ci risulta la modalit pi garantista rispetto al possibile errore diagnostico del radiologo [ 8 , 9 ] , in quanto si sforza di riprodurre la condizione corrente di screening ove il lettore ignaro di quali casi manifesteranno un ci tra una maggioranza di casi negativi . tale modalit di revisione , caldeggiata dal gruppo italiano di studio per lo screening mammografico ( gisma ) [ 1 ] , stata recentemente suggerita come quella ideale dal ministero della salute [ 2 ]  . 
 la scelta di accoppiare ad ogni caso solo due controlli deriva dallelevato numero di ci in studio e dalla necessit di costruire un set di dimensioni non eccessive per rendere agevole la revisione . 
 la scelta di definire le categorie di revisione ( ms o es ) non in base al giudizio di un solo revisore , ma in base alla maggioranza delle identificazioni della lesione da parte di un panel di revisori , appare pi affidabile , per le inevitabili differenze soggettive di giudizio delle anomalie radiologiche : che tali differenze di giudizio esistano ben evidente radiol med ( 2009 ) 114 : 907914 the choice of defining review categories ( ms or se ) according to majority detection rate of a reviewer panel rather than to a single reviewers judgement appears more reliable for the unavoidable interobserver variation in judging the degree of suspicion of perceived abnormalities . such a low reproducibility was confirmed in our study by the wide variation of recall rates of negative controls among reviewers . 
even when determined according to majority , se and ms categories maintained a substantially different positive predictive value for ic ( se = 51.7% , ms = 21.8% ) , as recommended in european guidelines . comparison between reviewers suggests that adopting significantly higher recall rates does not necessarily imply higher detection rates . 
as a collateral finding , we observed that ics are significantly associated with denser breast compared with a random sample of negative controls , thus confirming previous reports on the subject [ 11 ]  . overall , the study results suggest that the considered screening programme has a good performance as to sensitivity , as it fulfilled the standards recommended by european guidelines , a goal that is not frequently achieved by service screening programmes [ 5 , 6 , 9 ]  . 
further improvement is expected in ic rate thanks to the recent adoption of routine double reading , and a study is ongoing on this aspect , which will be the object of a future report . 
the experience reported here , together with a relatively limited number of italian studies on this subject to date [ 46 ] , confirms that the assessment of ic proportional incidence and blind review of ic are fairly easy and feasible procedures , which should not remain episodic but should be performed routinely , as they are probably the most reliable among the available recommended early indicators of screening efficacy [ 10 ]  . dal diverso tasso di richiamo osservato per i diversi revisori . 
la differenza di significato tra le categorie ms e es , enunciata nelle line guida europee , chiaramente rispettata , come dimostrato dal diverso valore predittivo positivo osservato per le due categorie ( es = 51 , 7% , sm = 21 , 8% )  . il confronto tra diversi revisori suggerisce che ladozione di tassi di richiamo eccessivamente elevati non ripaghi in termini di tasso di identificazione di ci : in questo studio infatti , differenze statisticamente molto significative del tasso di richiamo non si traducono in differenze significative nel tasso diagnostico di ci . 
come rilievo collaterale abbiamo osservato che i ci , rispetto a un campione random di controlli negativi , sono associati a una maggiore probabilit di seno denso , confermando cos quanto gi riportato in letteratura [ 11 ]  . la revisione ha fornito un risultato anchesso indicativo di buona pratica , con un tasso di ci classificato come es ben inferiore al massimo raccomandato dalle linee guida europee ( 15% vs 20% raccomandato )  . 
complessivamente i risultati di questo studio dimostrano che il programma di screening valutato ha una buona performance , in linea con quanto raccomandato dalle linee guida europee , risultato non sempre facilmente ottenuto dai correnti programmi di screening [ 5 , 6 , 9 ]  . 
un ulteriore miglioramento nella frequenza dei ci atteso a seguito delladozione della doppia lettura quale pratica routinaria , e uno studio attualmente in corso su questo aspetto sar oggetto di futura pubblicazione . 
lo studio dimostra anche che la valutazione del tasso proporzionale dei ci e la loro revisione fattibile con una ragionevole facilit , come dimostrato anche da un numero a tuttoggi assai limitato di studi italiani [ 46 ]  . 
mazzini 121 , 00195 rome , italy , tel . : + 39 - 06 - 20902419 , fax : + 39 - 06 - 20902469 , e - mail : orazio.schillaci@uniroma2.it received : 12 june 2008 / accepted : 5 november 2008 / published online : 4 july 2009 springer - verlag 2009 abstract purpose . 
the aim of our prospective study was to compare the diagnostic accuracy of early , delayed and dual - timepoint positron emission tomography ( pet ) acquisition with contrast enhanced computed tomography ( ct ) within a pet - ct examination in the evaluation of pulmonary solitary nodules ( spns )  . 
whole - body pet images were acquired at 50 min after fluorine18 - fluorodeoxyglucose ( 18f - fdg ) administration ( early ) , followed by a chest acquisition ( delayed )  . 
presso il nostro dipartimento sono stati sottoposti a valutazione pet - tc dual - time con mezzo di contrasto 30 pazienti con nodulo polmonare solitario . le immagini pet total - body sono state acquisite 50 minuti dopo la somministrazione di 18f - fdg ( fase precoce ) seguite da unacquisizione del torace ( fase tardiva )  . 
stato calcolato il valore di suvmax sulle immagini precoci e tardive : lincremento ( suvmax ) del suvmax tra fase precoce e fase tardiva 10% stato considerato suggestivo di malignit ; in valutazione tc invece stata considerato suggestivo di benignit lassenza di un significativo incremento di densit ( < 15 hu ) tra lacquisizione basale e quella postcontrastografica . 
la sensibilit , la radiol med ( 2009 ) 114 : 890906 dual - time - point suvmax values were 83% , 67% , 75% and 74% ; hu values were 94% , 34% , 67% , 96% ; ct morphologic evaluation values were 61% , 46% , 60% , 47% . 
area under the curve ( auc ) for early suvmax was 0.79 , for delayed suvmax 0.80 , for dual - time - point suvmax 0.85 , for hu 0.63 and for ct morphologic assessment 0.58. 
however , dual - time - point suvmax was most sensitive , whereas single - time - point suvmax was most specific . keywords dual - time - point suv single - time - point suv contrast - enhanced ct lung nodules specificit , il vpp e il vpn del suvmax ottenuto in fase precoce sono state del 77% , 91% , 79 , 5% e 66 , 7% rispettivamente ; in fase tardiva abbiamo ottenuto valori di 83% , 67% , 75% e 74% rispettivamente . 
la differenza del valore in hu ( hu ) tra acquisizione tc basale e quella post - contrastografica ha mostrato valori di sensibilit del 94% , di specificit del 34% , vpp del 67% e vpn del 96% . la valutazione tc morfologica ha riportato valori di sensibilit , specificit , di vpp e di vpn di 61% , 46% , 60% , 47% . 
nel nostro piccolo gruppo di pazienti il valore di suvmax sia in fase precoce che tardiva ha mostrato accuratezza sovrapponibile , le valutazioni tc morfologica e contrastografica hanno mostrato laccuratezza pi bassa . il valore di suvmax calcolato in dual - time ( suvmax ) ha mostrato laccuratezza diagnostica maggiore . 
about one third of spns in patients older than 35 years are malignant [ 2 ] and are often discovered accidentally during a routine chest x - ray , with radiological features such as size , location or calcification [ 2 , 3 ] helping to discriminate between benign and malignant nodularities . 
furthermore , the recent use of computed tomography ( ct ) as a screening technique for lung cancer has further increased the number of incidentally discovered pulmonary nodules in asymptomatic patients . 
the reported incidence of malignant lesions i noduli polmonari solitari ( nps ) sono definiti come lesioni polmonari ovalari o rotondeggianti con dimensioni fino a 3 cm di diametro , circondate da parenchima polmonare , non associate ad atelettasia o ispessimento parenchimale infiammatorio [ 1 ] ; le lesioni di dimensioni maggiori di 3 cm sono invece definite come masse e possono essere pi frequentemente di natura maligna . 
circa un terzo dei nps nei pazienti con et maggiore di 35 anni sono maligni [ 2 ] e spesso vengono rinvenuti incidentalmente durante lesecuzione di una radiografia ( rx ) del torace di routine , con caratteristiche radiografiche come dimensioni , localizzazione o calcificazioni [ 2 , 3 ] che aiutano a discriminare fra benignit o malignit . 
il recente impiego della tomografia computerizzata ( tc ) come tecnica di screening per il carcinoma del polmone ha repentinamente aumentato il numero di noduli polmonari scoperti in pazienti asintomatici . 
molti di 892 radiol med ( 2009 ) 114 : 890906 among solitary pulmonary nodules ranges from 5% to 69% [ 79 ] , the variability essentially depending on the imaging technique used and the population examined . 
on account of its ability to scan the whole lung in a few seconds using thin collimations , msct plays a crucial role in the noninvasive detection , characterisation and follow - up of pulmonary nodules . 
the increasing importance of thin - section ct , with or without intravenous ( i.v. ) contrast enhancement , in the study of spns is due to its capability of assessing the pattern of calcification within a nodule and precisely assessing its doubling time , margins , density , attenuation and contrast enhancement , therefore defining potential benignity or malignancy , e.g. 
popcorn or diffuse calcifications within a nodule suggest benignity , whereas eccentric calcifications are more frequently found in malignant lesions [ 2 , 3 ]  . however , the above - mentioned features may fail to confidently discriminate between benign and malignant spns , making management decision difficult . 
in fact , the use of msct in combination with 99mtc sestamibi single photon emission tomography ( spect - ct ) in spns has been proposed , with interesting future perspectives in differential diagnosis [ 10 ]  . 
over the last decade , diagnostic imaging of spns and staging of lung cancers have rapidly changed with the increasing use of pet scan , which measures the degree of fluorine18 - fluorodeoxyglucose ( 18f - fdg ) uptake or c11 - choline [ 11 ] within a lesion . 
in fact , it is possible to calculate standardised uptake value ( suv ) , that is , the ratio between the average radioactivity registered in a lesion and the administered amount of the same tracer . 
rationale for the use of 18f - fdg is the higher glucose metabolism displayed by malignant cells compared with benign cells , probably due to up - regulation of glucose transporters ( glut ) and hexokinase , with down - regulated synthesis of glucose - 6phosphatase [ 13 , 14 ]  . 
actually , whereas pet sensitivity and specificity are high for hypermetabolic solid spns 13 cm in size , false negatives are described for low metabolic neoplasms , such as bronchioloalveolar cell carcinoma and carcinoids or in solid nodules < 1 cm [ 15 ]  . 
false - positive results of pet examination include , on the other hand , some benign pulmonary conditions such as tuberculosis and sarcoidosis due to monocytes increased turnover [ 16 ] , which lowers pet positive predictive value ( ppv )  . 
dual - time - point pet acquisition has been proposed to discriminate between benign and malignant processes [ 16 ] , in the evaluation of suspected secondary liver lesions [ 17 ] and in distinguishing between benign and malignant lung nodules [ 18 , 19 ]  . 
a lesion is likely to be malignant if the suv increases over time , whereas it is likely to be benign if the suv is stable or decreases 10% [ 19 ]  . 
lincidenza riportata di lesioni maligne fra i nps varia dal 5% al 69% [ 79 ] : tale variabilit dipende essenzialmente dalla tecnica di imaging utilizzata e dalla popolazione esaminata . 
in virt della capacit di esaminare lintero torace con acquisizione di pochi secondi , la tcms gioca un ruolo cruciale nella individuazione non - invasiva , nella caratterizzazione e nel monitoraggio dei noduli polmonari . 
la crescente importanza della tc a strato sottile nello studio dei nps , con o senza somministrazione di mezzo di contrasto endovena ( mdc e.v. ) , dovuta alla sua capacit di descrivere pattern di calcificazione nellambito nodulare di determinare il tempo di raddoppiamento delle dimensioni , i margini , la densit , lattenuazione , limpregnazione dopo mdc e pertanto nel definirne la potenziale benignit o malignit ; ad esempio calcificazioni a pop - corn o diffuse sono suggestive di benignit mentre quelle eccentriche sono riscontrate pi spesso nei noduli maligni [ 2 , 3 ]  . 
 nella differenziale luso di metodiche ibride che permettano studi morfofunzionali pu agevolare la diagnosi e la gestione dei nps . a tale proposito stata recentemente proposta lintegrazione della tcms con la spect - tc con 99mtc - sestamibi nella valutazione dei noduli polmonari con interessanti prospettive [ 10 ]  . diagnostica nellultima decade limaging dei nps e la stadiazione del carcinoma polmonare sono stati velocemente modificati con lavvento della tomografia ad emissione di positroni ( pet ) che misura lintensit della captazione del 18f - fluorodeossiglucosio ( 18f - fdg ) o della 11c - colina [ 11 ] nellambito di una lesione . 
infatti possibile misurare lo standardised uptake value ( suv ) , valore di captazione standard , che il rapporto fra la radioattivit media misurata nella lesione e la dose di tracciante somministrata . nei nps un valore di suv di 2 , 5 viene impiegato come cutoff per differenziare lesioni benigne ( valore di suv inferiore ) da quelle maligne ( valore di suv maggiore ) [ 12 ]  . 
il razionale per lutilizzo del 18f - fdg laumentato metabolismo glucidico espresso dalle cellule maligne rispetto a quelle benigne , dovuto probabilmente alla maggiore espressione di trasportatori di glucosio ( glut ) e di esochinasi , con minor espressione della glucosio - 6 - fosfatasi [ 13 , 14 ]  . 
altro punto da considerare che sensibilit e specificit della pet sono state dimostrate elevate per le lesioni ad aumentato metabolismo glucidico con dimensioni da 1 a 3 cm , mentre falsi negativi sono descritti per quanto riguarda neoplasie a basso metabolismo , quali il carcinoma bronchiolo - alveolare e il carcinoide o in caso di noduli solidi con dimensioni inferiori al centimetro [ 15 ]  . radiol med ( 2009 ) 114 : 890906 vivo show that malignant cells tend to accumulate 18f - fdg over time , with an increase of suv > 10% , whereas mononucleate cells of the monocyte - macrophage system show stable or decreasing ( 10% ) suv [ 16 ]  . 
recently , 18f - fdg in - line pet - ct have demonstrated an emerging role in the evaluation of spns [ 20 ] and in lung carcinoma staging , in the assessment of response to chemo / radiation therapy and risk stratification of lung carcinoma [ 21 ]  . 
in previous studies , dual - time - point and single - time - point fdg - pet accuracies were calculated as a percentage of correct diagnoses in the entire sample . 
moreover , no studies compared dual - timepoint pet accuracy with contrast - enhanced ct diagnostic accuracy in a single clinical setting . the aim of the present study was to compare single - timepoint maximum suv max , dual - time - point suvmax and contrast - enhanced ct diagnostic accuracy by means of area under the receiver - operating characteristic ( roc ) curves in the evaluation of solitary pulmonary nodules . materials and methods patients from november 2006 to january 2007 , 35 patients underwent pet - ct examination for metabolic evaluation of spns after giving written informed consent to the examination . 
patients had either a known lung cancer history , or an oncological history with a newly discovered lung nodule suspicious for metastasis , or were referred for metabolic evaluation of an spn . 
finally , 30 patients ( 17 men and 13 women , mean age 59 , range 3680 ) were included in the study ( table 1 )  . twenty - four patients with lung nodules incidentally discovered at chest radiography or at high - resolution ct ( hrct ) performed for other reasons ( cough , chest pain ) and six oncology patients ( two with suspected recurrent lung cancer , two with colorectal carcinoma , one with liposarcoma , one with ovarian carcinoma ) were prospectively enrolled . dual - time - point pet and contrast - enhanced ct all patients fasted for at least 5 h before f18 - fdg i.v. 
this daltro canto esiste la possibilit di falsi positivi in pet per reperti polmonari benigni , come tubercolosi e sarcoidosi , a causa dellaumentato turn - over monocitario espresso [ 16 ] , che possono inficiare il valore predittivo positivo della metodica . 
 stata dunque proposta la pet con metodica di acquisizione dual - time per migliorare la performance nella diagnosi differenziale fra processi benigni e maligni [ 16 ] , ad esempio in caso di sospette lesioni secondarie epatiche [ 17 ] e dei noduli polmonari benigni e maligni [ 18 , 19 ] : una lesione ha maggiore probabilit di essere maligna se il valore di suv aumenta nel tempo mentre tendenzialmente benigna se tale valore rimane stabile o si riduce al di sotto del 10% [ 19 ]  . 
studi eseguiti sia in vitro che in vivo mostrano che le cellule maligne tendono ad accumulare il 18f - fdg nel tempo con incremento di suv fino al 10% , mentre le cellule del sistema monocito - macrofagico mostrano suv stabile o decrescente ( 10% ) [ 16 ]  . 
ultimamente la pet - tc con 18f - fdg ha dimostrato un ruolo emergente nella valutazione dei nps [ 20 ] , nella stadiazione , nella valutazione della risposta alla chemioterapia / radioterapia e nella stratificazione del rischio del carcinoma polmonare [ 21 ]  . 
in studi precedenti stata calcolata laccuratezza della pet con 18f - fdg in dual - time e in single - time come percentuale di diagnosi corretta nellintero campione ; tuttavia non ci sono studi che confrontino in ununica sessione laccuratezza diagnostica della pet dual - time con la tc con mdc . scopo del nostro studio confrontare la performance diagnostica del valore della pet con valore di suvmax in singola misurazione ( precoce o tardiva ) , della pet con valore di suvmax in dual - time e della tc con mdc con lutilizzo di curva roc nella valutazione del nodulo polmonare solitario ( nps )  . materiali e metodi pazienti da novembre 2006 a gennaio 2007 , 35 pazienti hanno eseguito lesame pet - tc per la caratterizzazione metabolica di nps , dopo consenso informato . 
i pazienti , sono stati inviati presso il nostro dipartimento per la caratterizzazione di nodulo polmonare evidenziato come reperto occasionale , per la stadiazione di carcinoma polmonare primitivo o per la valutazione di sospetto nodulo polmonare secondario ad altra patologia oncologica . 
sono stati inclusi nello studio pazienti con singolo nodulo polmonare . i noduli con dimensioni < 9 mm , dati i limiti del potere di risoluzione della metodica pet , sono stati esclusi dallo studio . 
infine il numero totale di pazienti arruolati patients table 1 patients gender clinical query tabella 1 pazienti pazienti 17 m , 13 f 59.3 years ( range 3680 ) 24 metabolic characterisation of spn 6 oncological history sesso quesito clinico 17 m , 13 f 59 , 3 anni ( range 3680 ) 24 caratterizzaione metabolica nps 6 storia oncologica system combines a high - speed ultra 16 - detector - row ( 912 detectors per row ) ct unit and a pet scanner with 10080 bismuth germanate ( bgo ) crystals in 24 rings . 
after nonenhanced ct , pet images were acquired 50 min after 18f - fdg i.v. administration , with a chest scan and early suv calculation ( two bed positions , 4 min per bed ) , followed by whole - body acquisition ( five to seven bed position , depending on the patient , 4 min per bed ) for delayed suv calculation 90 min after the i.v. 
total - body pet examination in the caudocranial direction , from upper thighs to vertex , was performed after 40 mimages were reconstructed using a standard iterative algorithm [ ordered subsets expectation maximisation ( osem ) ] after 2530 min of acquisition . 
administration of nonionic iodinated contrast material ( 100120 ml , 370 mgi / ml , 420 mgi / kg at 3 ml / s ) , obtaining two successive stacks of scans . 
the first comprised the upper abdomen with a 30 - s delay from the injection onset ; the second extended from the neck to the pelvis with a 60 - s delay . 
change of spn enhancement was assessed 2 , 3 and 4 min after contrast administration , using 3.75 - mm - thick volumetric scans . data analysis images were evaluated on a dedicated workstation by a nuclear physician and a radiologist , both aware of the clinical history of the patient . 
lung nodules were evaluated by radiol med ( 2009 ) 114 : 890906 risultato essere di 30 soggetti ( 17 uomini e 13 donne ; et media 59 anni ; range 3680 anni ) ( tabella 1 )  . 
ventiquattro pazienti presentavano noduli polmonari evidenziati come reperto occasionale in un esame rx del torace o tc ad alta risoluzione ( hrct ) precedentemente eseguiti per altri motivi ( tosse , dolore toracico , esami preoperatori di routine ) ; 6 pazienti presentavano una precedente storia clinica oncologica ( 2 pazienti con sospetta recidiva di carcinoma polmonare , 2 pazienti con carcinoma colorettale , 1 paziente con liposarcoma , 1 paziente con carcinoma ovarico )  . 
 tutti i pazienti sono stati mantenuti a digiuno per almeno 5 ore prima della somministrazione del 18f - fdg e in tutti il livello ematico di glucosio era nella norma . 
con adeguata idratazione ( 500 ml di soluzione salina di nacl 0 , 9% ) per ridurre la presenza di radiofarmaco nei reni . inoltre circa 600 cc di soluzione di contrasto sono stati somministrati per os , al fine di opacizzare le anse intestinali . 
questo sistema associa uno scanner tc di tipo high speed ultra con 16 file di detettori ( 912 detettori per fila ) con tomografo pet con 10080 cristalli di germinato di bismuto ( bgo ) disposti in 24 anelli . 
prima dellacquisizione stata eseguita una tc a basso amperaggio per la correzione dellattenuazione delle immagini pet ( 80 ma , 140 kv , campo visivo da 420 a 500 mm , spessore della sezione tc di 3 , 75 mm )  . 
del radiofarmaco con unacquisizione del torace per la misura del suv in fase precoce ( 2 lettini della durata di 4 minuti ciascuno ) seguite dallacquisizione whole body ( da 5 a 7 lettini , della durata di 4 minuti ciascuno ) per la misurazione del suv in fase tardiva , a distanza di 90 minuti dalla somministrazione del 18f - fdg . 
le immagini pet whole body sono state acquisite in direzione caudo - craniale dal terzo prossimale dei femori fino al cranio , e di seguito ricostruite utilizzando un algoritmo iterativo standard ( osem , ordered subsets expectation maximization ) dopo 2530 minuti di acquisizione . 
la tc diagnostica stata eseguita con il seguente protocollo : 120140 kv , amperaggio automatico ( 330350 ma ) , modalit di acquisizione 27 , 50 / 1 , 375 : 1 , velocit di rotazione del gantry 0 , 6 secondi , fov largo matrice di 512512 . 
liniezione di mezzo di contrasto iodato ( 100120 ml , 370 mgi / kg , 3 ml / s ) stata effettuata in due pacchetti consecutivi di scansioni : il primo comprendente laddome radiol med ( 2009 ) 114 : 890906 means of semiquantitative analysis ( suvmax ) , and suv > 2.5 was considered malignant [ 12 ]  . 
in lesions with low 18f - fdg uptake , the rois were extrapolated from the axial chest ct tomograms by placing it at the nodule equator . dual - time - point suv was calculated on early and delayed images according to the following formula : suvmax ( % ) = ( suvdelayed suvearly ) / suvearly100 . 
nodule density changes , between nonenhanced and contrast - enhanced ct scan , after the emission scan , were quantified to determine the significance of lesion enhancement using circular standardised rois ( 10 mm2 ) manually placed on the axial tomograms within the lesion . 
ct examination data sets were reprocessed and reconstructed according to the ala software instructions : 1.25 - mm slice thickness , 3.27mm interval to ensure correspondence with the spacing of the pet sections , and bone filter , applied to the nonenhanced acquisition . 
minimum follow - up was 10 months . statistical analysis the meanstandard error ( sem ) of the different variables ( early suvmax , delayed suvmax , dual - time - point suvmax , hu ) was calculated . 
in order to test variables normal distribution , the shapiro - wilk test was performed . according to the test results , mean values of the variables were compared using the nonparametric mann - whitney u test . 
statistical analysis was performed using a standard commercially available software package ( ncss 2007 )  . con un ritardo di 30 secondi rispetto alliniezione del mdc e il secondo esteso dal collo alla pelvi con un ritardo di 60 secondi . 
lenhancement post - contrastografico dei nps stato misurato al 2 , 3 e 4 minuto dopo la somministrazione del contrasto , utilizzando spessore di scansione di 3 , 75 m analisi dei dati le immagini sono state esaminate su consolle dedicata da un medico nucleare e da un radiologo , entrambi consapevoli della storia clinica del paziente . 
regioni di interesse ( roi , region of interest ) sferiche sono state utilizzate sulle immagini mip ( maximum intensity projection ) per calcolare il valore di suvmax ; nelle lesioni con scarsa captazione del 18f - fdg le roi sono state estrapolate da immagini assiali tc del torace posizionando il cursore al centro del nodulo . 
la variazione di suv ( suv ) sulle immagini precoci e tardive stato calcolata seguendo questa formula : suvmax ( % ) = ( suvtardivosuvprecoce ) / suvprecoce100 . lincremento di suv > 10% stato considerato suggestivo di malignit mentre un valore di suv stabile o decrescente stato considerato suggestivo di benignit [ 19 ]  . 
i cambiamenti nella densit del nodulo tra tc basale e tc post - contrasto sono stati misurati usando roi circolari standardizzate ( 10 mm2 ) posizionate manualmente sui tomogrammi assiali delle lesioni . 
i dati tc sono stati processati e ricostruiti secondo le istruzioni del software ala : 1 , 25 mm di spessore delle slices , intervallo fra le slices di 3 , 27 mm per assicurare la coincidenza tra sezioni pet e filtro per losso applicati allacquisizione basale . lenhancement post - contrastografico stato definito come differenza fra la densit della lesione misurata in unit hounsfield prima e dopo la somministrazione di mdc ( hu )  . 
eighteen of 30 nodules ( 60% ) were malignant , and 12 / 30 were benign ( 40% ) , as confirmed by pathological assays or clinical follow - up . 
among malignant lesions ( table 2 ) , seven were adenocarcinoma of the lung , two squamous cell carcinoma , one large - cell carcinoma , one carcinoid , one liposarcoma metastasis that responded to chemotherapy , two colorectal carcinoma that responded to chemotherapy , three lung cancer recurrence ( after chemoor radiation therapy ) and one ovarian carcinoma metastasis . 
 risultati caratteristiche dei noduli sono stati valutati complessivamente 30 noduli polmonari : il diametro massimo medio dei noduli maligni risultato di 22 , 136 , 8 mm ( range 9 , 5030 mm ) mentre quello dei noduli benigni risultato di 14 , 817 , 38 ( range 3 , 528 mm )  . 
le tabelle 2 e 3 mostrano le caratteristiche della popolazione in esame divisa in noduli maligni e benigni . diciotto / 30 noduli ( 60% ) sono risultati maligni , 12 / 30 ( 40% ) benigni , come confermato dai campioni istologici o dal monitoraggio clinico - strumentale . 
tra le lesioni maligne ( tabella 2 ) , sette si sono dimostrate adenocarcinoma del polmone , due carcinoma squamocellulare , uno carcinoma a grandi cellule , un carcinoide , una metastasi da liposarcoma ( risposta alla chemioterapia ) , due carcinoma colo - rettale ( risposta alla chemioterapia ) , tre recidive di carcinoma polmonare ( dopo chemioterapia o radioterapia ) , una metastasi da carcinoma ovarico . 
1a , b distinction between benign and malignant nodules obtained with the early and delayed maximum standardised uptake value ( suvmax ) value ( a ) and the suvmax ( b )  . 
1a , b distinzione tra noduli benigni e maligni ottenuta sia con il valore di suvmax precoce e tardivo ( a ) sia con il suvmax ( b )  . 
although 30% of the nonselected population with spn identified at first chest radiography has a 20%40% likelihood of being malignant [ 2 , 24 ] , radiol med ( 2009 ) 114 : 890906 differenza statistica significativa tra il valore di suv precoce e suv tardivo quando i pazienti sono stati classificati in riferimento a patologia benigna o maligna ( p = 0 , 93 e p = 0 , 090 , rispettivamente )  . 
analogamente non stata osservata differenza statistica significativa tra enhancement postcontrastografico dei noduli maligni rispetto a quello dei noduli benigni ( 36 , 2213 , 24 vs 23 , 8333 , 15 , p = 0 , 17 )  . applicato il test di fisher non stata osservata significativa correlazione fra i criteri morfologici documentati in tc e la malignit ( p = 0 , 58 )  . la sensibilit , la specificit , il valore predittivo positivo ( vpp ) e il valore predittivo negativo ( vpn ) del hu hanno presentato rispettivamente valori percentuali di : 94% , 34% , 67% e 96% . 
i valori massimi corrispondenti riscontrati sulla performance diagnostica del valore di suv tardivo sono stati : 77% , 66% , 74% , 66% ; i valori riscontrati per il valore di suv precoce : 77% , 91% , 79 , 5% , 66 , 7% ; infine i valori corrispondenti alla performance del valore di suvmax in dualtime hanno dimostrato : sensibilit 83% , specificit 70% , vpp 75% , vpn 74% . 
in quasi il 30% dei soggetti in popolazioni non selezionate con nps identificato al primo radiogramma del torace sussiste la probabilit tra il 20% e il 40 % che questo nodulo diventi maligno [ 2 , 24 ] ; nei due terzi di casi inoltre la tc o le radiografie standard non riescono a discriminare fra lesioni benigne e maligne sulla base della presenza di calcificazioni o degli aspetti tomodensitometrici [ 25 , 26 ]  . 
2a , b dual - time - point maximum standardised uptake value ( suvmax ) values ( a ) and early suvmax values ( b ) in the receiver - operating characteristic ( roc ) curves . 
larea roc del suvmax in dualtime pi alta di quella del suvmax in singola acquisizione ; comunque , per un tasso di falsi positivi minore di 0 , 20 , preferibile utilizzare il suvmax in singola acquisizione rispetto al suvmax in dual - time . in two thirds of cases , both ct and chest x - rays are unable to differentiate between benign and malignant lesions on the basis of calcifications or density features alone [ 25 , 26 ] moreover , 5 - year survival after resection of bronchogenic carcinoma ranges from 40% to 80% depending on the timing of diagnosis . 
recently , dual - time - point suv has been evaluated in lung carcinoma [ 16 , 19 , 29 ] , showing a better accuracy than single - time - point evaluation . 
morphologic evaluations of spns can help differentiate benign and malignant spns when they have typical benign or malignant features , but there may be overlap between nodule types in terms of morphologic presentations [ 22 , 30 ]  . 
in our series , no intralesional calcifications were evidenced , and the fisher exact test indicated no significant association between lesion 40%80% ci dipende dalla timing della diagnosi iniziale ; pertanto la diagnosi precoce delle lesioni maligne fondamentale al fine di iniziare un trattamento subitaneo e adeguato [ 27 , 28 ]  . 
ultimamente stata studiata lefficacia del valore diagnostico del suvmax in dual - time nella valutazione del carcinoma polmonare [ 16 , 19 , 29 ] , che ha dimostrato una maggiore accuratezza della valutazione in singola acquisizione . 
nel nostro studio stata osservata una differenza significativa tra noduli benigni e maligni per quanto riguarda i valori suvmax precoce , suvmax tardivo e suvmax in dual - time . secondo tali risultati il valore di suv con cut - off 2 , 5 rappresenta un affidabile criterio per differenziare i noduli benigni da quelli maligni ; tale dato stato riscontrato in uno studio analogo eseguito sulla performance della pettc con somministrazione di mezzo di contrasto nella valutazione dei nps . 
in questo studio stato valutato peraltro il valore di suv in singola acquisizione tardiva associato ai criteri morfologici tc [ 30 ]  . per quanto riguarda il valore hu densitometrico o per quanto concerne gli aspetti morfologici tc nel nostro studio non si sono osservate differenze significative . proprio la valutazione morfologica del nodulo polmonare solitario ( nps ) pu aiutare nella differenziazione di lesioni benigne e maligne quando queste presentino aspetti tipici di benignit o malignit . 
inoltre lefficacia diagnostica valutata misurando larea sotto la curva roc dellanalisi dellenhancement ( hu ) , risultata maggiore dellarea roc dellanalisi morfologica . probabilmente ci dovuto ai limiti connessi al numero di pazienti inclusi nel nostro studio . 
analogamente ad altri dati precedentemente pubblicati [ 19 , 31 ] , i nostri risultati hanno inoltre dimostrato che il suvmax in dual - time possiede maggiore accuratezza del suvmax in single - time ( suvmax dual - time : auc , 0 , 84 ; suvmax precoce : auc , 0 , 80 ; suvmax tardivo 0 , 79 )  . 
di conseguenza i valori di suvmax in dual - time hanno dimostrato sensibilit e vpn pi elevati se confrontati al valore di suvmax in singola acquisizione ( dual - time suvmax : 83% , 74% ; suvmax precoce : 77% , 66% ; suvmax tardivo : 77% , 66% )  . 
moreover , the area under the roc curve reflecting assessment of the enhancement of each lesion was greater than the area under the roc curves reflecting the irregularity of the shape . 
indeed , dual - timepoint suvmax values showed higher sensitivity and npv compared with single - time - point suv ( dual - time - point suv 83% , 74% ; early suvmax 77% , 66% ; delayed suvmax 77% , 66% )  . 
roc curve for dual - time - point suv is better than early suvmax curve in the high false positive range ( high sensitivity range ) , whereas early suvmax is better than dual - time - point suvmax in the false positive rate of < 0.20. noteworthy is that a diagnostic test should be judged relative to the clinical setting to which the test is applied . for the evaluation of a lung nodule , in low - risk populations ( nonsmokers , no history of neoplasm ) where the prevalence of lung cancer is very low , a high specificity and low false positive test such as early suvmax evaluation would be of preference . 
however , when screening for lung cancer in a high - risk population ( smokers , history of lung neoplasm , etc . ) , the diagnostic test should provide the best sensitivity , such as dual - time - point suvmax , even if the false positive rate is higher , as false negative test results may have serious consequences on patient survival in high - risk patients . figures 3 and 4 show two false negatives for semiquantitative suv evaluation but true positive for dual - time - point suv and hu evaluation . 
in both cases , nodule size was > 9 mm but < 1 cm , and single - time - point suv evaluation was probably affected by the suv threshold commonly used [ 12 ]  . 
nodules < 9 mm were excluded from this study , as our aim was to evaluate an suv with 2.5 cutoff , which was demonstrated to be not efficient in discriminating benign lung micro - nodules [ 32 ]  . 
daltro canto larea sotto la curva per il suvmax precoce risultata maggiore di quella del suvmax dual - time , utilizzando un cut - off di falsi positivi < 0 , 20 . 
per la valutazione di un nodulo polmonare in popolazioni a basso rischio ( non fumatori , non precedenti neoplasie ) , nei quali la prevalenza del carcinoma polmonare molto bassa , sarebbe preferibile ottenere un valore di specificit elevato associato a un basso tasso di falsi positivi , come verificatosi nella nostra valutazione del valore precoce di suvmax . daltro canto , quando si attui screening per carcinoma polmonare in popolazione ad alto rischio ( fumatori , storia di precedente neoplasia polmonare etc . ) il test diagnostico dovrebbe provvedere la maggiore sensibilit possibile , come nel caso del valore di suvmax in dual - time , anche se possibile che si verifichi un elevato tasso di falsi positivi ; si consideri infatti che un risultato di un test falso negativo avrebbe serie conseguenze sulla sopravvivenza del paziente nelle popolazioni ad alto rischio . 
le figure 3 e 4 mostrano 2 risultati falsi negativi nella valutazione semiquantitativa suv che invece si sono dimostrati veri positivi nelle valutazioni del suv in dual - time e della variazione di hu . 
in entrambi i casi le dimensioni del nodulo erano > 9 mm ma < 1 cm e la valutazione del suvmax in dual - time stata probabilmente influenzata dal valore soglia suv utilizzato [ 12 ]  . 
i noduli con dimensioni < 9 mm sono stati esclusi dal nostro studio , in quanto lo scopo era di valutare il valore di suv con cut - off di 2 , 5 , che stato dimostrato non affidabile nel discriminare fra micronoduli benigni e maligni [ 32 ]  . 
in ogni caso le lesioni polmonari 1 cm con assente o trascurabile captazione di 18f - fdg hanno una bassa probabilit di malignit ( < 5% ) [ 3 ]  . 
 la nostra analisi potrebbe anche essere limitata dal fatto che la metodologia roc utilizzata per attribuire laccuratezza diagnostica inficiata dallesperienza degli esaminatori e dal tasso di falsi negativi e falsi positivi nella popolazione arruolata . 
daltro canto lanalisi roc la misura pi accurata di una performance diagnostica rispetto alla valutazione percentuale di corretta diagnosi nellintero campione , mentre la curva roc mostra la sensibilit e i tassi di falsi positivi a tutti i valori di cut - off radiol med ( 2009 ) 114 : 890906 fig . 
3a immagini assiale precoce e tardiva coronale del paziente numero 2 in tabella 2 ( noduli maligni ) , con suvmax di 1 , 4 e 2 , 1 rispettivamente . 
questo paziente si dimostrato un falso negativo per lanalisi semiquantitativa suv ma vero positivo sia per lanalisi del suvmax in dual - time sia per la valutazione densitometrica in hu . 
 racy was affected by the readers experience and by false negative and false positive rates in the population enrolled . on the contrary , roc analysis is a more accurate measure of diagnostic performance than evaluation of the percentage of correct diagnoses in the entire sample , as roc curve displays sensitivities and false positive rates at all possible cutoff levels , thus allowing assessment of the performance of a test independently of the decision threshold . conclusions in our small series of patients , malignant and benign nodules showed significantly different early suvmax , delay suvmax and dual - time - point suvmax values , disponibili , valutando la performance del test indipendentemente dalla scelta del valore soglia . 
 conclusioni nella nostra piccola casistica di pazienti i noduli benigni e quelli maligni hanno dimostrato valori di suvmax precoce , suvmax tardivo e suvmax in dual - time significativamente differenti , mentre non sono state osservate differenze per quanto riguarda il hu o gli aspetti morfologici . 
questo paziente si dimostrato falso negative per lanalisi del suvmax in singola acquisizione e vero positivo per lacquisizione suvmax in dual - time e per la misura densitometrica in hu . whereas no differences were observed in terms of hu or morphologic features . 
di conseguenza , per la valutazione di un nodulo polmonare solitario in ambito clinico , in popolazione a basso rischio ( ad esempio in non - fumatori o con anamnesi negativa per precedenti neoplasie maligne ) , dove la prevalenza del carcinoma polmonare bassa , dovrebbe essere eseguito preferenzialmente un test ad alta specificit come il suvmax precoce . 
quando daltro canto si applichi screening per carcinoma polmonare in popolazione ad alto rischio ( ad esempio in soggetti fumatori o pazienti con precedenti oncologici ) il test diagnostico dovrebbe garantire la migliore sensibilit , come il valore di suvmax in dual - time , anche tenuto conto dellelevato tasso di falsi radiol med ( 2009 ) 114 : 890906 fig . 
pathological examination of the surgical specimen revealed the presence of atypical mycobacteriosis : single - time - point pet , dual - time - point suvmax and contrast - enhanced ct were all false positive for malignant pulmonary disease . 
la prima riga mostra visione assiale in tc e ricostruzione ala del nodulo polmonare ; la seconda riga mostra immagini pet assiali , precoce e tardiva , dello stesso nodulo ( suvmax 3 , 7 e 5 , 2 rispettivamente )  . 
il reperto anatomo - patologico dopo la resezione chirurgica ha dimostrato presenza di micobatteriosi atipica : la singola acquisizione pet , il suvmax in dual - time e la tc con contrasto si sono dimostrate falsamente positive per patologia polmonare maligna . 
 the false positive rate is higher , as false negative test results may have serious consequences on patient survival in a high - risk population . positivi , in quanto il risultato negativo di tale test potrebbe avere serie ripercussioni sulla sopravvivenza dei pazienti in popolazioni ad alto rischio . 
ventriglia2 1dipartimento di scienze radiologiche , 2dipartimento di pediatria , servizio di cardiologia pediatrica , sapienza universit degli studi di roma , policlinico umberto i , viale del policlinico 155 , 00161 rome , italy correspondence to : s . 
this is a prospective observational study of 83 pregnant women who underwent fetal cardiac mri : 43 patients ( cases ) had echocardiographic suspicion of congenital heart disease ; 40 patients ( controls ) did not . 
si stratta di uno studio osservazionale prospettico di 83 donne in gravidanza sottoposte ad esami di rm cardiaca fetale : 43 con il sospetto ecocardiografico di patologia cardiovascolare ( casi ) e 40 senza ( controlli )  . lo studio rm cardiaco fetale consiste in una fase statica con sequenze multiplanari ssfp ed in una fase dinamica con sequenze ssfp in tempo reale . 
le sequenze ssfp permettono uno studio rm morfologico del distretto cardiovascolare mentre radiol med ( 2009 ) 114 : 852870 sequences may provide adjunctive albeit suboptimal functional information . attualmente riescono ad aggiungere dati funzionali solamente in maniera subottimale . 
 keywords fetal heart fetal mri congenital heart disease cardiac malformations prenatal diagnosis parole chiave cuore fetale rm fetale malattie congenite cardiache malformazioni cardiache diagnosi prenatale introduction introduzione magnetic resonance imaging ( mri ) has taken on an increasingly important role in the evaluation of high - risk pregnancy . 
fetal mri is , in fact , considered a third - line modality for the study of complex fetal disease after prenatal screening ultrasound and specialist ultrasound in secondary care centres [ 1 , 2 ]  . 
currently , the main fetal indications for performing mri in pregnancy are central nervous system ( cns ) malformations , disease of the chest and neck region , some abdominal abnormalities and urinary tract malformations [ 3 , 4 ]  . up until now , however , the study of the heart and great vessels has been hindered by the intrinsic characteristics of the organ and the technological limitations of the current mri sequences . 
the high fetal heart rate requires elevated temporal resolution , the small size of the heart and the vessels requires elevated spatial resolution and the rapid blood flow requires sequences that are not sensitive to fluids in motion . ultrafast t2 - weighted sequences , which are commonly used for fetal mri , are instead highly sensitive to flow and visualise the blood - filled heart and vessels as structures characterised by a lack of signal [ 5 ]  . 
 the heart has therefore been considered the black hole of fetal mri , and the aorta and great vessels were only studied by evaluating the image negatives , as they were depicted as structures without signal . steady - state free precession ( ssfp ) sequences use the alternating application , between two successive radiofrequency pulses , of balanced gradients that cause each stationary magnetic spin to return to the phase prior to the application of the gradient . 
therefore , whether stationary or in motion , fluids are visualised as structures with elevated signal ( just like stationary fluids in t2 - weighted sequences ) and at the same time the elevated contrast resolution of the t1weighted sequences is maintained [ 6 , 7 ]  . in addition , thanks to the acquisition speed of the individual slices , these sequences also enable dynamic visualisation ( cine mri ) of the heart with the possibility of evaluating the contractility of the cardiac chambers [ 8 ]  . la risonanza magnetica ( rm ) ha acquisito un ruolo progressivamente importante nella valutazione delle gravidanze a rischio . 
la rm fetale infatti considerata metodica di terzo livello per lo studio delle patologie fetali complesse dopo lecografia ostetrica di screening e quella specialistica eseguita in centri di secondo livello [ 1 , 2 ]  . attualmente le principali indicazioni fetali per lesecuzione della rm in gravidanza sono le malformazioni del sistema nervoso centrale ( snc ) , le patologie del distretto cervicotoracico , alcune anomalie addominali e le malformazioni urinarie [ 3 , 4 ]  . 
 fino ad oggi tuttavia lo studio del cuore e dei grossi vasi stato ostacolato dalla presenza di peculiari caratteristiche di tali organi e dalla limitazione tecnologica delle attuali sequenze rm : lelevata frequenza cardiaca fetale richiede infatti unelevata risoluzione temporale ; le piccole dimensioni del cuore e dei vasi rendono necessario lutilizzo di unelevata risoluzione spaziale ; il rapido flusso sanguigno necessita di sequenze non sensibili ai fluidi in movimento . le sequenze ultraveloci t2 pesate , comunemente utilizzate per lo studio rm fetale , sono invece molto sensibili ai flussi e visualizzano il cuore ed i vasi , percorsi da sangue in movimento , come strutture caratterizzate da mancanza di segnale [ 5 ]  . 
 il cuore stato pertanto considerato il buco nero della rm fetale e laorta ed i grossi vasi sono stati studiati solo attraverso la valutazione in negativo delle immagini , essendo rappresentate come strutture senza segnale . 
 le sequenze steady state free precession ( ssfp ) utilizzano lapplicazione alternata , tra due impulsi di radiofrequenza successivi , di gradienti bilanciati che agiscono su ogni spin magnetico stazionario facendolo tornare alla fase precedente allapplicazione del gradiente . 
in tal modo i gradienti bilanciati mantengono sia la magnetizzazione longitudinale che trasversale e nellimmagine rappresentato sia il contrasto t1 che t2 : pertanto i fluidi , sia stazionari che in movimento , vengono visualizzati come strutture ad elevato segnale ( proprio come i fluidi stazionari nelle sequenze t2 pesate ) e , allo stesso tempo , viene mantenuta lelevata risoluzione di contrasto delle sequenze t1 pesate [ 6 , 7 ]  . inoltre tali sequenze grazie alla rapidit di acquisizione delle singole fette permettono anche la visualizzazione dinamica ( cine - rm ) del distretto cardiaco con la possibilit della valutazione della contrattilit delle camere cardiache [ 8 ]  . the aim of this study was to demonstrate the feasibility scopo di questo lavoro quello di dimostrare la 854 radiol med ( 2009 ) 114 : 852870 of identifying the main anatomical and pathological appearances of the fetal cardiovascular system by using fetal mri with ssfp . possibilit di riconoscere i principali aspetti anatomici e patologici del distretto cardiovascolare fetale attraverso lo studio rm fetale con sequenze ssfp . materials and methods between september 2007 and august 2008 , we performed a prospective observational study based on fetal mri of the cardiovascular region . 
for this study , we enrolled 43 cases represented by 43 pregnant women with echocardiographic suspicion of fetal congenital heart disease referred to our service from the paediatric cardiology division and 40 controls represented by 40 pregnant women without known cardiovascular or thoracic disease referred from the prenatal diagnosis centre with a suspicion of cns ( n = 27 ) or non - cns disease ( n = 13 )  . 
the group of cases included one twin pregnancy and 42 singleton pregnancies , whereas the control group consisted of 40 singleton pregnancies . mean maternal age was 30 ( range 2342 ) years among cases and 32 ( range 1844 ) years among controls , whereas mean gestational age was 29 weeks in both groups ( range 2038 and 2237 weeks in cases and controls , respectively )  . all women underwent fetal mri without sedation of mother or fetus after giving informed consent and filling in a questionnaire regarding their pregnancy and family history of congenital disease . 
fetal mri was performed in both cases and controls with a 1.5 - t system ( siemens magnetom avanto , erlangen , germany ) with one or two multichannel phased - array surface coils and a standard protocol . 
in each case , a localisation sequence was acquired to enable placement of the volumes investigated as well as a t2 - weighted half - fourier single - shot turbo spin - echo ( haste ) sequence with a thick slice ( 6 mm ) in the coronal plane to evaluate fetal lie ( longitudinal , transverse , oblique ) and presentation ( cephalic , breech , shoulder )  . 
a study with thin - slice t2 - weighted haste sequences was then performed ( tr 1 , 000 , te 118 / 151 , matrix 256134 , slice thickness 34 mm , fov 2720 cm ) with multiplanar orientation on the organ of interest and lastly on the cardiovascular region . the study of the heart involved two phases . 
t1 and t2 weighting was intermediate , and sequences were oriented in the three planes in materiali e metodi tra settembre 2007 ed agosto 2008 abbiamo eseguito uno studio osservazionale prospettico , basato sullesecuzione di esami rm fetali mirati allo studio del distretto cardio - vascolare . 
per questo studio abbiamo arruolato 43 casi comprendenti 43 donne in gravidanza con il sospetto ecocardiografico di patologia fetale cardio - vascolare , inviate presso il nostro servizio dal servizio di ecocardiografia del reparto di cardiologia pediatrica e 40 controlli comprendenti 40 donne in gravidanza senza patologia fetale cardiovascolare n toracica nota , inviate dal servizio di diagnosi prenatale del nostro policlinico per il sospetto di patologie del snc ( 27 ) o non - snc ( 13 )  . 
let media materna era di 30 anni ( range 2342 anni ) nel gruppo dei casi e 32 anni ( range 1844 anni ) nel gruppo dei controlli e let gestazionale media era di 29 settimane in entrambi i gruppi ( range 2038 e 2237 rispettivamente nei casi e nei controlli )  . tutte le donne sono state sottoposte ad esame di rm fetale senza sedazione n materna n fetale e previa raccolta del consenso scritto allesecuzione dellesame rm preceduto dalla compilazione di un questionario anamnestico sulla gravidanza in corso e sulla storia familiare per patologie congenite . 
lo studio rm fetale stato effettuato sia nei casi che nei controlli con un magnete da 1 , 5 tesla ( siemens magnetom avanto , erlangen , germania ) con una o due bobine di superficie multicanale phased array attraverso un protocollo standard comune . 
in ogni caso stata acquisita una sequenza di localizzazione che consente il posizionamento dei volumi indagati e una sequenza t2 half - fourier acquisition singleshot turbo spin echo ( haste ) a strato spesso ( 6 mm ) sul piano coronale per la valutazione della situazione ( longitudinale , trasversale , obliqua ) e della presentazione ( cefalica , podalica , di spalla ) fetale : lorientamento dei successivi pacchetti stato effettuato su quelli precedentemente acquisiti per ridurre al minimo i problemi dovuti al cambiamento della posizione fetale per il movimento spontaneo del feto . quindi stato effettuato uno studio con sequenze t2 haste a strato sottile ( tr 1000 , te 118 / 151 , matrice 256134 , spessore dello strato 34 mm , fov 27 20 cm ) con orientamento multiplanare sullorgano anatomico di interesse ed infine lo studio del distretto cardiovascolare . 
la fase statica prevede lacquisizione di sequenze a gradiente di eco ultraveloci con steady state free precession chiamate truefisp ( true fast imaging with steady state free precession ) sulla apparecchiatura rm da noi utilizzata ( tr / te 3 , 5 / 1 , 5 , matrice 256144 , spessore dello strato 34 mm , fov 40 30 cm ) , radiol med ( 2009 ) 114 : 852870 space orthogonal to the cardiac axis to identify the main cardiovascular structures and measure the cardiac axis . 
the entire study was performed and evaluated in consensus by two radiologists with longstanding experience in obstetric radiology . with regard to image interpretation in controls , the anatomical study of the heart involved evaluation of cardiac orientation , cardiac volume , morphology and volume of the cardiac chambers and structure of the myocardial walls , as well as a study of the integrity of the interventricular septum ( ivs ) and the interatrial septum ( ias ) with the oval foramen ( of )  . 
the anatomical study of the great vessels , instead , involved evaluation of the origin , diameter and course of the aorta ( ao ) , pulmonary artery ( pa ) , ductus arteriosus ( da ) , superior vena cava ( svc ) , inferior vena cava ( ivc ) and pulmonary veins ( pv )  . with regard to interpretation of images in the cases , the radiologists were always aware of the suspicion of cardiovascular disease based on echocardiography , and the examination was targeted towards evaluating mri signs of the disease being studied . 
direct signs were defined as morphological and volumetric abnormalities of the cardiac chambers and the myocardium , malrotations , septal defects and abnormalities of origin , course and diameter of the great vessels . 
in the cases , mri findings were compared with echocardiography performed after mri or at birth or with the postmortem findings , which were considered the standard of reference . con pesatura intermedia t1 e t2 , orientate sui tre piani dello spazio ortogonali allasse cardiaco per lidentificazione delle la misura principali strutture cardiovascolari e per dellangolazione dellasse cardiaco . 
la fase dinamica prevede lacquisizione di sequenze real - time cine - rm truefisp 2d chiamate tf2d sulla apparecchiatura da noi utilizzata ( tr / te 248 , 5 / 1 , 1 , matrice 19299 , spessore dello strato 34 mm , fov 3826 cm , fa 77 , risoluzione temporale 2 fette / secondo ) , ripetute in maniera dinamica ( per 40 volte ) ed orientate sulle precedenti scansioni statiche per ottenere piani rm simili ai principali piani di scansione ecocardiografici ( assiali , sagittali ed obliqui ) ed inclinati lungo i piani anatomici cardiaci fetali dellafflusso ed efflusso vascolare . lintero esame stato eseguito e valutato da due radiologi esperti in radiologia in ostetricia in consensus . 
 per quanto riguarda linterpretazione delle immagini nei controlli lo studio anatomico del cuore ha previsto la valutazione dellorientamento cardiaco , della volumetria cardiaca , della morfologia e volumetria delle camere cardiache e della struttura delle pareti miocardiche , nonch lo studio dellintegrit del setto interventricolare ( siv ) e di quello interatriale ( sia ) con il forame ovale ( fo )  . 
lo studio anatomico dei grossi vasi ha invece previsto la valutazione dellorigine , del calibro e del decorso dei vasi di efflusso cardiaco ( aorta , ao , arteria polmonare , ap ) e del dotto arterioso ( da ) e la valutazione del calibro e decorso dei vasi di afflusso ( vena cava superiore , vcs , vena cava inferiore , vci , vene polmonari , vp )  . per quanto riguarda linterpretazione delle immagini nei casi , i radiologi erano sempre a conoscenza della patologia cardiovascolare sospettata dallecocardiografia e lesame stato mirato alla valutazione degli aspetti di semeiotica rm della patologia oggetto di studio . sono stati individuati segni diretti ed indiretti di patologia cardiovascolare considerando come segni diretti le anomalie morfovolumetriche delle camere cardiache e del miocardio , le malrotazioni , i difetti settali e le anomalie di origine , decorso e calibro dei grossi vasi e come segni indiretti lassenza delle strutture anatomiche nella scansione di riferimento , laumento di calibro a monte di una stenosi vascolare , la presenza di cardiomegalia e versamento pericardico . 
the walls of the myocardium were instead visualised as hypointense structures with optimal contrast resolution le sequenze ssfp truefisp statiche e tf2d dinamiche hanno permesso una visualizzazione ottimale del cuore e dei grossi vasi in tutti i feti ( 40 / 40 ) : in particolare le camere cardiache ed il lume vascolare sono stati visualizzate come strutture ad elevata intensit di segnale per la presenza nel loro contesto di sangue in movimento ; le pareti del miocardio 856 radiol med ( 2009 ) 114 : 852870 fig . 
a four - chamber view with visualisation of the ventricular ( vs , left ventricle ; vd , right ventricle ) and atrial chambers ( as left atrium , ad right atrium ) , the ventricular ( siv ) and atrial septum ( sia ) and the atrioventricular plane . 
c three - vessel view with the origin of the pulmonary artery ( ap ) and the ductus arteriosus ( da ) continuing with the descending aorta ( aod ) , the aorta and superior vena cava ( vcs )  . 
a scansione 4 camere con visualizzazione delle cavit ventricolari ( vs , ventricolo sinistro e vd , ventricolo destro ) , delle cavit atriali ( as , atrio sinistro e ad , atrio destro ) , del setto interventricolare ( siv ) e del setto interatriale ( sia )  . 
c scansione tre vasi con la visualizzazione dellarteria ( ap ) e del dotto arterioso ( da ) che si continua nellaorta discendente ( aod ) , dellao e della vena cava superiore ( vcs )  . 
the static true - fisp sequences in planes orthogonal to the cardiac axis made possible the visualisation of all of the main cardiovascular structures of interest covered by echocardiographic screening during the second trimester morphological examination ( four - chamber views and views of the outflow tracts of the aorta and pulmonary trunk ) in 28 / 40 fetuses ( 70% )  . 
le sequenze statiche truefisp , orientate su piani ortogonali allasse cardiaco , hanno consentito di ottenere la visualizzazione di tutte le principali strutture cardiovascolari di interesse previste dallo screening ecografico durante lesame morfologico del ii trimestre ( 4 camere cardiache e tratto di efflusso dellaorta e del tronco polmonare ) in 28 / 40 feti ( 70% ) ed in particolare le camere cardiache sono state visualizzate in tutti i feti ( 100% ) , il tratto di efflusso dellaorta in 28 feti ( 70% ) e il tratto di efflusso del tronco polmonare in 33 feti ( 82 , 5% ) : i rimanenti 12 feti nei quali uno o entrambi i tratti di efflusso cardiaci non erano visualizzabili con le sequenze statiche presentavano rispettivamente unepoca gestazionale compresa tra 22 e 25 settimane in 9 casi e 26 e 30 settimane nei restanti 3 casi . 
 the dynamic tf2d sequences oriented according to le sequenze dinamiche tf2d , orientate secondo le radiol med ( 2009 ) 114 : 852870 table 1 frequency of projections obtained with fetal mri in normal fetuses planes views mri frequency transverse views sagittal views angulated views scansioni assiali scansioni sagittali scansioni oblique 4 - chamber 5 - chamber ( aortic origin ) 3 vessels ( pulmonary outflow tract ) aortic arch short axis of the left ventricle tricuspid - aortic cut long axis of the ductus arteriosus long axis of the aortic arch long axis of the left ventricle aortic arch and ductus arteriosus simultaneously 4 camere 5 camere ( origine dellaorta ) 3 vasi ( tratto di efflusso polmonare ) scansione assiale dellarco aortico asse corto del ventricolo sinistro scansione tricuspide - aorta asse lungo del dotto arterioso asse lungo dellarco aortico asse lungo del ventricolo sinistro scansione simultanea dellarco aortico e del dotto arterioso 40 / 40 21 / 40 17 / 40 6 / 40 38 / 40 11 / 40 22 / 40 33 / 40 18 / 40 11 / 40 40 / 40 21 / 40 17 / 40 6 / 40 38 / 40 11 / 40 22 / 40 33 / 40 18 / 40 11 / 40 tabella 1 frequenza delle proiezioni ottenute con rm cardiaca fetale nei controlli normali piano di scansione scansione frequenza visualizzazione rm standard echocardiographic scans produced mri planes that were comparable to the main echocardiographic scans with the frequency reported in table 1 . 
the five - chamber and long - axis views of the lv , which enable evaluation of the aorta origin , were obtained in 21 / 40 fetuses ( 52.5% ) and 18 / 40 fetuses ( 45% ) , respectively , with overall visualisation of the rv outflow tract in 38 / 40 fetuses ( 95% , in 17 with double scan ) and the lv outflow tract in 31 / 40 fetuses ( 77.5% , in six with double scan )  . the distinction between right and left cardiac chambers was possible in 32 / 40 fetuses ( 80% )  . 
in 12 fetuses , it was based on direct evidence of the presence of the moderator band at the rv apex , which was represented by a thin band projecting into the ventricular lumen in the fourand fivechamber views . 
in the remaining eight fetuses , the distinction was not possible because the moderator band scansioni ecocardiografiche standard , hanno permesso di ottenere piani rm comparabili alle principali scansioni ecocardiografiche con la frequenza riportata in tabella 1 . in particolare i piani previsti dallo screening ecografico durante lesame morfologico del ii trimestre ( scansione 4 camere , scansione tratti di efflusso ) sono stati riprodotti secondo tale frequenza : la scansione 4 camere stata ottenuta in tutti i controlli ( 40 / 40 feti , 100% ) ; la scansione asse corto del ventricolo sinistro ( vs ) e la scansione tre vasi che permettono la visualizzazione del tratto di efflusso del ventricolo destro ( vd ) rispettivamente in 38 / 40 feti ( 95% ) e 17 / 40 feti ( 42 , 5% ) ; la scansione 5 camere e la scansione asse la valutazione dellorigine dellaorta rispettivamente in 21 / 40 ( 52 , 5% ) ed in 18 / 40 feti ( 45% ) , con una complessiva visualizzazione del tratto di efflusso del vd in 38 / 40 feti ( 95% , in 17 con doppia scansione ) e del tratto di efflusso del vs in 31 / 40 ( 77 , 5% , in 6 con doppia scansione )  . lungo del vs che permettono la distinzione tra camere cardiache di destra e di sinistra stata possibile in 32 / 40 feti ( 80% ) : in 12 feti in base allevidenza diretta della presenza della banda moderatrice allapice del vd rappresentata da una tenue e sottile banda che aggetta nel lume ventricolare nelle scansioni 4 e 5 camere ; in 20 feti in base alla morfologia del vs che risultava pi profondo nella porzione che costituisce lapice rispetto al vd ; nei rimanenti 8 feti tale distinzione non stata possibile poich la banda moderatrice non era 858 radiol med ( 2009 ) 114 : 852870 was not recognisable and the morphology of the cardiac chambers appeared similar . 
the volume measurements of the cardiac chambers showed that the rv in the fetus is larger than the lv up until the 32nd week of gestation , whereas the atria are similar in size even at term . the ivs was well depicted in all fetuses and characterised by low signal intensity in the ssfp sequences . 
the ias was visualised in only 12 / 40 fetuses , where it appeared as a hypointense , slender and mildly fragmented structure . lastly , the flap of the oval foramen from right to left was only rarely visualised ( 3 / 40 fetuses , at weeks 32 , 34 and 38 of gestation , respectively ) in the cine mri tf2d views oriented in the short axis of the heart . 
the cardiac apex appeared directed towards the left , and the angle of the ivs on the midsagittal plane was a mean 455 in all fetuses . the atrioventricular plane was visualised in all fetuses in the fourand five - chamber views , although the opening and closing of the valves was perceived in the dynamic sequences in six fetuses only . 
the analysis of signal intensity of the myocardial wall also revealed a difference between the walls of the lv and rv , with a more marked signal hypointensity of the lv than the rv in 38 / 40 fetuses regardless of gestational age . with regard to the study of the cardiac outflow vessels , the origin of the ao and the pa were well visualised in 31 / 40 and 38 / 40 fetuses , respectively . 
measuring the diameter of those vessels revealed that the pa was on average slightly larger than the ao , which in turn was slightly larger than the svc and similar in size to the da . 
la volumetria delle camere cardiache ha mostrato che nel feto il vd risulta di dimensioni maggiori rispetto al vs fino alla 32 settimana di gestazione , mentre gli atri risultano di dimensioni comparabili anche a termine . il siv risultato ben visualizzabile in tutti i feti e caratterizzato da bassa intensit di segnale nelle sequenze ssfp ; il sia stato visualizzato solo in 12 / 40 feti nei quali appariva comunque come una struttura sottile e frammentata lievemente ipointensa ; il flap del forame ovale da destra verso sinistra stato infine visualizzato raramente ( 3 / 40 feti , rispettivamente alla 32 , 34 e 38 settimana di gestazione ) attraverso le scansioni cine - rm tf2d orientate sullasse corto del cuore . 
il piano atrioventricolare stato visualizzato in tutti i feti nelle scansioni 4 e 5 camere , tuttavia lapertura e la chiusura delle valvole stata percepita nelle sequenze dinamiche solamente in 6 feti . 
lanalisi dellintensit di segnale del miocardio parietale ha mostrato inoltre una differenza tra le pareti del vs e quelle del vd con una pi marcata ipointensit di segnale del vs rispetto al vd in 38 / 40 feti indipendentemente dallepoca gestazionale . per quanto riguarda lo studio dei vasi di efflusso cardiaco , lorigine dellao e dellap sono risultati ben visualizzabili rispettivamente in 31 / 40 feti e in 38 / 40 feti : la misura del calibro di tali vasi ha dimostrato che lap risulta in media di dimensioni poco maggiori dellao , la quale , a sua volta , mostra dimensioni poco maggiori della vcs e simili al da ; il decorso dei grossi vasi stato valutato attraverso varie scansioni assiali a diverse altezze e attraverso le scansioni asse lungo dellarco aortico e del fig . 
b long - axis view of the aortic arch with the origin of the aorta ( origine ao ) , the ascending tract , the arch and the descending tract ( aod ) and some of the head and neck vessels ( left carotid artery , csn ; left subclavian artery , ssn )  . 
ben documentabile il ventricolo destro ( vd ) e lorigine dellaorta ( ao )  . radiol med ( 2009 ) 114 : 852870 the pulmonary arteries were visualised in 10 / 40 fetuses as very small structures at the limit of the techniques spatial resolution arising from the pa with asymmetrical course from the hylar region to the periphery . 
the da , which in the fetus is a fundamental structure of the systemic circulation , was well visualised in 32 fetuses in transverse section in the three - vessel scan ( n = 17 ) and / or in the longitudinal section in the long - axis scan of the da ( n = 22 )  . the svc and the ivc were visualised with the tricuspidaorta scan in 11 fetuses . 
il da che nel feto costituisce una struttura fondamentale per la circolazione sistemica stato ben visualizzato in 32 feti , in sezione trasversale nella scansione 3 vasi ( 17 ) e / o in sezione longitudinale nella scansione asse lungo del dotto arterioso ( 22 )  . 
 per quanto riguarda i vasi di afflusso cardiaco la vcs e la vci sono state visualizzate con la scansione tricuspideaorta in 11 feti ; con maggiore difficolt in soli 5 feti stato possibile visualizzare anche le vene polmonari con una scansione paracoronale allaltezza degli atri . pathological appearance aspetti patologici at least one congenital heart disease was diagnosed with postnatal echocardiography or postmortem examination in 42 / 43 pathological fetuses , whereas the condition was ruled out in the remaining fetus ( table 2 )  . 
fetal mri with static ssfp true - fisp and dynamic tf2d sequences was able to visualise the pathological fetal heart in all 42 fetuses with congenital heart disease ( 42 true positives ) and successfully rule out hypoplastic left - heart syndrome in the normal fetus ( one true negative )  . 
mri was therefore diagnostic in 43 / 43 cases . however , even though mri identified the major disease in all cases , it also raised a suspicion of an ivs defect , which was ruled out at birth in two fetuses ( one fetus with cardiomegaly and one with cardiac rhabdomyomas ) ( two false positives ) and visualised a significant ivs defect corresponding at birth to multiple interventricular defects in a fetus with truncus arteriosus ( one diagnostic inaccuracy )  . congenital heart disease was diagnosed on the basis of the mri depiction of direct pathological signs in 21 fetuses , indirect pathological signs in six fetuses and both in 15 cases . 
however , as stated above , in the fetus with truncus arteriosus , this defect in fact corresponded to multiple adjacent interventricular defects at birth , whereas in two other fetuses , interventricular defect was ruled out at birth . 
 almeno una patologia congenita cardiaca stata diagnosticata attraverso lecocardiografia postnatale o lesame autoptico in 42 / 43 feti patologici mentre stata esclusa nel rimanente feto ( tabella 2 )  . 
lo studio rm fetale con le sequenze ssfp truefisp statiche e tf2d dinamiche ha permesso la visualizzazione del cuore fetale patologico in tutti i 42 feti portatori di patologia cardiaca ( 42 veri positivi ) , mentre nel feto normale alla nascita aveva escluso la sindrome del cuore sinistro ipoplastico ( 1 vero negativo ) : la rm risultata pertanto complessivamente diagnostica in 43 / 43 casi . 
 tuttavia lesame rm , pur diagnosticando la patologia maggiore in tutti i casi , ha anche sospettato la presenza di un difetto del siv escluso alla nascita in 2 feti ( 1 feto con cardiomegalia e 1 feto con rabdomiomi cardiaci ) ( 2 falsi positivi ) ed ha visualizzato un ampio difetto del siv corrispondente alla nascita a multipli difetti interventricolari in un feto con tronco arterioso ( 1 imprecisione diagnostica )  . 
 la patologia cardiaca stata diagnosticata attraverso la visualizzazione in rm dei segni patologici diretti in 21 feti , dei segni indiretti in 6 feti e attraverso entrambi in 15 casi . 
3a , b feto di 34 settimane con sindrome del cuore sinistro ipoplasico : a nella scansione 4 camere il ventricolo sinistro ( vsx ) appare molto ridotto in volume con lume quasi virtuale ; a , b il ventricolo destro ( vdx ) appare aumentato di volume con pareti di spessore maggiore che di norma e marcatamente ipointense in relazione ad ipertrofia del miocardio . 
4a - d feto di 35 settimane con miocardiopatia spongiosa : le pareti del miocardio ( frecce ) appaiono aumentate di spessore , con intensit di segnale ridotta e con struttura compatta . radiol med ( 2009 ) 114 : 852870 fig . 
7a - e feto di 27 settimane con trasposizione completa dei grossi vasi : nelle immagini in successione si evidenzia lorigine dellaorta ( ao ) dal ventricolo destro ( vdx ) e dellarteria polmonare ( ap ) dal ventricolo sinistro ( vsx ) in cuore con regolare connessione atrio - ventricolare . table 4 mri direct signs of abnormalities of the origin and course of the great vessels abnormalities of origin and course of the great vessels mri direct sign 1 truncus arteriosus 2 complete transposition of the great arteries 7 overriding aorta ( 6 tetralogy of fallot , 1 vsd ) 3 right - sided aortic arch vsd , ventricular septal defect ; ivs , interventricular sept a single great artery exiting heart overriding the ventricles the aorta arises from the right ventricle and the pulmonary artery arises from the left ventricle in a heart with normal atrioventricular connections the aorta arises in the middle of the heart and overrides both the ventricles right - to - right course of the aorta tabella 4 segni rm diretti delle anomalie di origine e decorso dei grossi vasi anomalie di origine e decorso dei grossi vasi segno rm diretto 1 tronco arterioso bilanciato 2 trasposizione completa dei grossi vasi 7 aorta a cavaliere ( 6 tetralogie di fallot , 1 div ) 3 arco aortico destroposto div , difetto interventricolare ; siv , setto interventricolare un unico vaso di efflusso arterioso che origina a cavaliere del siv origine dellartao dal ventricolo destro e della arteria polmonare dal ventricolo sinistro in un cuore con normale connessione atrioventricolare origine dellaorta in sede mediana a cavallo del siv e dei due ventricoli un arco aortico che mostra decorso da destra verso destra radiol med ( 2009 ) 114 : 852870 fig . 
magnetic resonance images show a small right ventricle ( vdx in b , * in a , c ) , a large right atrium ( adx in b ) and a ventricular septal defect ( arrow in c )  . 
8a - c feto di 32 settimane con atresia della tricuspide : si visualizza marcata riduzione volumetrica del ventricolo destro ( vdx in b , * in a e c ) , aumento volumetrico dellatrio destro ( adx in b ) , il difetto interventricolare ( freccia in c )  . 
as , atrio sinistro ; vs , ventricolo sinistro ; ao , aorta ; vcs , vena cava superiore . table 5 mri in direct signs of abnormalities of vessel size or valve anomalies abnormalities of the size of the vessels / valve anomalies mri indirect sign 2 pulmonary stenosis 6 fallot , 1 hypoplastic pa 1 coarctation of the aorta 1 tricuspid atresia 1 mitral - aortic disease increased size and hypertrophy of the rv increased size of the right ventricle increased size of the right ventricle and nonvisualisation of the ascending aorta and aortic arch increased size of the ra decreased size of the lv with myocardial hypertrophy and low - flow phenomena pa , pulmonary artery ; rv , right ventricle ; ra , right atrium ; lv , left ventricle tabella 5 segni rm indiretti delle anomalie di calibro dei vasi e delle anomalie valvolari anomalia di calibro dei vasi / anomalia valvolare segno rm indiretto 2 stenosi polmonari 6 tetralogie di fallot , 1 ipoplasia ap 1 coartazione dellaorta 1 atresia della tricuspide 1 patologia mitro - aortica dilatazione ed ipertrofia del vd dilatazione del vd dilatazione del vd e la scarsa visualizzazione dellaorta ascendente e dellarco dilatazione dellad riduzione volumetrica del vs con lipertrofia del miocardio e fenomeni di flusso lento endocavitari ap , arteria polmonare ; vd , ventricolo destro ; ad , atrio destro ; vs , ventricolo sinistro sequences ascribable to the presence of slow or turbulent flows were signs suggestive of incipient heart failure in three fetuses , one of which had a vein of galen aneurysm , one a malformation of the dural sinuses and one tuberous sclerosis . cardiache nelle sequenze t2 haste riconducibile alla presenza di flussi lenti o turbolenti sono segni che hanno fatto ipotizzare un incipiente scompenso cardiaco in 3 feti di cui 1 con aneurisma della vena di galeno , 1 con una malformazione dei seni durali e 1 con una sclerosi tuberosa . 
 discussion abnormalities of the cardiovascular system are the most common congenital diseases in the fetus , they can lead to intrauterine death and are often the cause of premature birth le anomalie congenite del distretto cardiovascolare sono le pi frequenti patologie congenite nel feto , possono portare ad discussione 866 radiol med ( 2009 ) 114 : 852870 fig . 
magnetic resonance images show a large heart with a cardiothoracic index of 0.41 , a pericardial effusion larger than 2 mm ( * in b - d ) and a large ductus arteriosus ( da ) ( a )  . 
9a - d feto di 34 settimane con cardiomegalia e versamento pericardico : il cuore appare aumentato di volume in toto con rapporto cardiotoracico di 0 , 41 ; si evidenzia la presenza di versamento pericardico > 2 mm ( * in b - d ) ; il dotto arterioso lievemente aumentato di dimensioni ( a )  . 
screening for fetal cardiovascular malformations is performed with obstetric ultrasound with four - chamber scans and outflow - vessel scans , although the reference standard for disease diagnosis is echocardiography [ 10 ]  . 
fetal echocardiography is performed in tertiary referral centres by paediatric cardiologists or obstetrician / gynaecologists and is a costly procedure reserved for women with specific risk factors for congenital cardiac diseases arising from family , personal or fetal indications [ 1113 ]  . fetal mri has been taking on an increasingly important role as a support modality to obstetric ultrasound in prenatal diagnosis of fetal malformations [ 14 ]  . 
to date , no negative effects have been demonstrated for the fetus exposed to magnetic fields less than or equal to 1.5 t , and fetal mri is advisable from the second trimester of pregnancy , when a preliminary ultrasound examination proves inadequate or diagnostically [ 1517 ]  . 
however , until recently , the cardiovascular system was difficult to evaluate with mri due to the techniques limitation in evaluating fluid in motion and the organs through which it travels and the need to adjust sequence parameters to the elevated fetal heart rate and the small size of the heart and vessels in the fetus [ 18 ]  . 
lo screening della patologia cardiovascolare fetale affidata allecografia ostetrica attraverso la scansione 4 camere e la scansione per i vasi di efflusso , tuttavia il gold standard per la diagnosi di tale patologia lecocardiografia [ 10 ]  . 
lecocardiografia fetale viene eseguita in centri ultraspecialistici da cardiologi pediatri o da ginecologi ostetrici ed un esame dispendioso riservato a donne con fattori di rischio specifici per le patologie cardiache congenite derivanti da indicazioni familiari , personali o da indicazioni fetali [ 1113 ]  . la rm fetale ha acquisito sempre maggior importanza come metodica di supporto allecografia ostetrica nella diagnosi prenatale delle malformazioni fetali [ 14 ]  . 
allo stato attuale non sono dimostrati effetti dannosi per il feto con campi di esposizione uguali o inferiori a 1 , 5 tesla e lesame rm fetale consigliato a partire dal secondo trimestre di gravidanza quando un preliminare esame ecografico risulti inadeguato o in conclusivo nella diagnosi [ 1517 ]  . tuttavia il distretto cardio - vascolare sembrava fino a poco tempo fa essere malvalutabile con la rm a causa dellostacolo tecnico della metodica nella valutazione dei fluidi in movimento e degli organi da essi attraversati come il sangue e il distretto cardio - vascolare e della necessit di adeguare i parametri tecnici delle sequenze allelevata radiol med ( 2009 ) 114 : 852870 with progressive technological improvement , sequences have been developed that are less sensitive to flow , faster and less subject to fetal movement , and thus produce better temporal and spatial resolution . 
in particular , ssfp sequences have been shown to be excellent for anatomical and functional study of the heart and great vessels in many studies of both adults and neonates [ 19 , 20 ]  . 
recently , these sequences have also been applied to mri study of the fetus and have proven able to identify the heart and great vessels in the uterus [ 21 , 22 ]  . our study confirms the possibility of visualising the fetal heart anatomy and great vessels with static ssfp true - fisp and dynamic tf2d sequences , with good contrast resolution between the blood contained in the cardiac chambers and the myocardial wall as well as the blood contained in the vessels and the vessel walls . in our study all the main anatomical structures were identified and followed in their course in all cases , with progressively reduced difficulty identifying the structures as the cardiac examinations were performed and familiarity with fetal images was acquired . 
in addition , cardiac and vascular structures of interest were visualised not only in the mri scans corresponding to the echocardiographic scans ( obtained with tf2d cine mri ) but also in contiguous scans oriented in planes orthogonal to the fetal cardiac axis ( obtained with static true - fisp sequences )  . this enabled anatomical continuity of the vascular structures to be followed , even in those cases where mri scans corresponding to the echocardiography could not be obtained . the greater difficulty visualising cardiac outflow vascular structures in the earlier weeks of gestation was most likely due to the smaller size of the vessels combined with greater fetal motion during mri acquisitions in this gestational period . 
indeed , the technical impossibility of triggering the fetal heart rate and the still limited temporal resolution of the current cine mri sequences ( two frames per second ) do not allow cardiac functionality to be tracked in real time . instead , cardiac motion is acquired in an artificial manner with its speed being dependent on the rapidity of slice acquisition and not on the real speed of atrioventricular contraction . 
it is therefore fundamental that whoever wishes to perform mri examinations of the fetal heart undergo training in the execution and reporting of fetal cardiac mri . the imaging technique should seek to maximise spatial resolution in both static and dynamic acquisitions by using a small fov , a sufficiently large matrix and thin slices . dynamic scans also require sequences with higher temporal resolution . 
lastly , orienting the data sets in the correct direction orthogonal to the heart and great frequenza cardiaca fetale e alle piccole dimensioni del cuore e dei vasi nel feto [ 18 ]  . con il progressivo miglioramento tecnologico sono state ideate sequenze meno sensibili ai flussi e sempre pi veloci e meno influenzabili dal movimento del feto , con risoluzioni sia temporale che spaziale pi performanti . 
in particolare le sequenze ssfp si sono dimostrate ottime sequenze per lo studio anatomico e funzionale del cuore e dei grossi vasi in numerosi lavori in letteratura sulladulto e sul neonato [ 19 , 20 ]  . 
recentemente queste sequenze sono state applicate anche nello studio rm del feto ed stata dimostrata in tal modo la possibilit di evidenziare il cuore e dei grossi vasi anche in utero [ 21 , 22 ]  . il nostro studio ha confermato la possibilit di visualizzare lanatomia del cuore e dei grossi vasi fetali con le sequenze ssfp truefisp statiche e tf2d dinamiche , con una buona risoluzione di contrasto tra il sangue contenuto nelle camere cardiache e il miocardio parietale cos come tra il sangue contenuto nei vasi e la parete vasale . nel nostro studio in ogni caso tutte le principali strutture anatomiche sono state riconosciute e seguite nel loro decorso , pur dovendo sottolineare una difficolt progressivamente minore in tale riconoscimento man mano che si eseguivano gli esami rm cardiaci e si acquisiva una maggiore familiarit con le immagini fetali . 
inoltre le strutture di interesse cardiache e vascolari sono state visualizzate non solo nelle scansioni rm corrispondenti alle scansioni ecocardiografiche ( ottenute con le cine - rm tf2d ) ma anche nelle scansioni contigue orientate sui piani ortogonali allasse cardiaco fetale ( ottenute con le sequenze statiche truefisp ) consentendo in ultima analisi di seguire la continuit anatomica delle strutture vascolari anche in quei casi in cui non si riuscivano ad ottenere scansioni rm corrispondenti allecocardiografia . da notare una maggiore difficolt di visualizzazione delle strutture vascolari di efflusso cardiaco nelle settimane di gestazione pi precoci probabilmente da metter in relazione alle minori dimensioni dei vasi ed al contemporaneo maggiore movimento del feto durante lacquisizione rm riscontrati in tali epoche gestazionali . 
la contrattilit cardiaca e la funzionalit valvolare sono invece attualmente non valutabili con la rm in maniera attendibile ; infatti limpossibilit tecnica di effettuare il trigger del battito cardiaco fetale e lancora limitata risoluzione temporale delle attuali sequenze cine rm ( 2 frame al secondo ) non permettono di seguire la funzionalit cardiaca in real time ma acquisiscono il movimento cardiaco in maniera artificiale , con velocit dipendente dalla rapidit di acquisizione delle fette e non dalla reale velocit di contrazione atrioventricolare . 
 per quanto riguarda infatti lesecuzione dellesame fondamentale sia nelle acquisizioni statiche che dinamiche ricercare la maggiore risoluzione spaziale possibile utilizzando piccoli fov , matrici sufficientemente grandi e 868 radiol med ( 2009 ) 114 : 852870 vessels is also fundamental in order to obtain images corresponding to those we are used to seeing in echocardiography . reporting of the examination requires recognition of the different anatomical structures and evaluation of their course in subsequent scans . 
in this sense , we believe that graphics software can be particularly useful for rotating and manipulating images to obtain the standard visualisation we are used to seeing on mri or ct studies of the adult , which depict the right cardiac chambers on the left of the image and the left cardiac chambers on the right of the image . in contrast , very few studies with significantly large patient populations have been published on the applicability of fetal mri study for evaluating congenital heart disease [ 23 ]  . 
our experience shows that fetal mri is able to visualise all the main congenital morphological abnormalities , whereas it cannot be used to evaluate cardiac rhythm or atrioventricular valvular abnormalities . in our study , fetal cardiac mri proved to be diagnostic in all 42 cases found to be truly pathological at postnatal echocardiography . 
in addition , in the only case of suspected cardiac disease at prenatal echocardiography that was excluded at the postnatal study , mri ruled out the disease ( one true negative )  . 
however , in the strictest sense of diagnostic accuracy , we need to emphasise the presence of two additional false positives in our series corresponding to two interventricular defects in a fetus with cardiomegaly and another with multiple rhabdomyomas that were ruled out at birth , as well as one diagnostic inaccuracy by depicting multiple interventricular defects as a single , large interventricular defect in a fetus with truncus arteriosus . 
these diagnostic findings , in fetuses at weeks 26 , 33 and 26 of gestation , respectively , seem to depend more on the still limited spatial resolution of the sequences rather than on the early gestational age . fetal cardiac mri relies on both direct and indirect signs that are sought after in all cases of suspected cardiovascular disease . 
marked malrotation can , for example , alter the anatomical planes we are used to seeing in the normal fetus , thus requiring sequence orientation in new planes obtained during the examination itself , leading to longer examination times and occasionally the need to repeat the sequences until the correct standard anatomical scan is obtained . even with these drawbacks , the study of fetal cardiac malformations is possible with mri and has the significant advantage that even the numerous extracardiac abnormalities , which are often associated with cardiac malformations , can be evaluated with a single examination and with the accuracy of mri , especially with regard to the fetal piccoli spessori di strato ; per le scansioni dinamiche inoltre altrettanto importante avvalersi di sequenze con la pi elevata risoluzione temporale . 
infine fondamentale orientare i pacchetti nella giusta direzione ortogonale al cuore e ai grossi vasi per ottenere immagini corrispondenti a quelle che siamo abituati a vedere in ecocardiografia . per quanto riguarda la refertazione , importante riconoscere le diverse strutture anatomiche e seguirne il decorso attraverso la valutazione delle scansioni successive ; a tale proposito risulta in nostra opinione molto utile lutilizzo di software grafici che permettono la rotazione ed il ribaltamento delle immagini per ottenere la visualizzazione standard come siamo abituati ad avere negli esami rm o tc delladulto delle camere cardiache di destra alla sinistra dellimmagine e di quelle di sinistra alla destra dellimmagine . 
 pochissimi lavori con casistiche di rilievo sono stati pubblicati invece sullapplicabilit dello studio rm fetale per la valutazione delle patologie congenite cardiache [ 23 ]  . secondo la nostra esperienza la rm fetale permette la visualizzazione delle principali patologie congenite morfologiche del distretto cardiaco mentre non pu essere utile per la valutazione delle anomalie del ritmo cardiaco e delle anomalie delle valvole atrio - ventricolari . nel nostro studio in tutti i 42 casi realmente patologici al controllo ecocardiografico postnatale la rm cardiaca fetale risultata diagnostica . 
se consideriamo tuttavia laccuratezza diagnostica pi fine dobbiamo sottolineare nella nostra casistica la presenza di 2 falsi positivi aggiuntivi corrispondenti a 2 div in un feto con cardiomegalia e uno con rabdomiomi poi esclusi alla nascita e di una imprecisione diagnostica nella descrizione di multipli div come un unico ampio div in un feto con tronco arterioso . 
tali dati peraltro diagnosticati rispettivamente in un feto a 26 , 33 e 26 settimane di gestazione sembrano dipendere maggiormente dallattuale ancora limitata risoluzione spaziale della sequenza piuttosto che dallepoca gestazionale precoce . 
certamente anche lo studio rm nel caso di anomalie cardiache complesse risulta pi difficile sia da impostare che da interpretare : le marcate anomalie di rotazione alterano per esempio i piani anatomici cui siamo normalmente abituati nel feto normale richiedendo lorientamento delle sequenze su nuovi piani ricavati durante lesame stesso con un prolungamento del tempo di esame e la necessit talvolta di ripetere le sequenze fino allottenimento della corretta scansione anatomica standard . pur con queste puntualizzazioni lo studio del cuore patologico nel feto possibile anche con la rm con il notevole vantaggio che in questo caso anche le numerose patologie extracardiache che spesso sono associate alle patologie radiol med ( 2009 ) 114 : 852870 bra of course , much still needs to be done from the technological perspective to obtain sequences with an optimal compromise between elevated spatial and contrast resolution and enabling real - time acquisition of mri images of the fetal heart that are capable of evaluating cardiac dyskinesia . the main limitation of our study is the knowledge on the part of the radiologists who performed and interpreted the fetal cardiac mri examinations of the presence or absence of a congenital heart disease suspected at fetal echocardiography and the type of congenital cardiac disease suspected in all cases . 
however , although this knowledge may have influenced the search for specific signs of the disease , it is typical of current clinical practice where mri is performed as a third - line investigation in the prenatal diagnosis of congenital disease and operators are inevitably aware of the findings of other previous investigations . in conclusion , fetal mri with ssfp sequences in static and dynamic acquisition enables evaluation of the normal fetal heart and identification of the main morphological alterations of the pathological fetal heart . cardiache possono essere valutate con un unico esame e con laccuratezza della metodica di rm soprattutto per quanto riguarda lencefalo fetale . 
certamente ancora molto deve essere fatto dal punto di vista tecnologico per ottenere sequenze con un ottimale compromesso tra elevata risoluzione spaziale e di contrasto che permettano di avere immagini rm in tempo reale del cuore fetale in grado di valutare anche le discinesie cardiache . 
 il principale limite del nostro studio la conoscenza da parte dei radiologi che hanno effettuato ed interpretato gli esami rm cardiaci fetali della presenza o assenza di una patologia congenita cardiaca sospettata allecocardiografia fetale e del tipo di cardiopatia congenita sospettata in tutti i casi . 
tuttavia tale fatto che potrebbe avere influenzato la ricerca di segni specifici della patologia rispecchia la corrente pratica clinica che prevede lesecuzione dellesame rm come esame di terzo livello nella diagnosi prenatale delle patologie congenite e pertanto impone inevitabilmente ed insostituibilmente la conoscenza dei rilievi delle altre metodiche precedentemente eseguite . in conclusione allo stato attuale la rm fetale con le sequenze ssfp in acquisizione statica e dinamica permette di valutare il cuore fetale normale e di riconoscere le principali alterazioni morfologiche del cuore fetale patologico . acknowledgements the authors thank the engineers at siemens , and particularly leonardo boccaccini , for their constant and fruitful cooperation in implementing the static true - fisp and cine mri sequences for studying the fetus . ringraziamenti gli autori ringraziano gli ingegneri della siemens in particolare ling . 
 + 39 - 045 - 8124301 , fax : + 39 - 045 - 8124775 , e - mail : riccardo.manfredi@univr.it received : 25 september 2008 / accepted : 23 october 2008 / published online : 14 may 2009 springer - verlag 2009 abstract purpose . 
images were assessed for tumour site and size , infiltration of the cervical stroma , infiltration of vaginal fornices and relationship between the tumour and the internal os of the endocervical canal and the presence and dimensions of pelvic and lumboaortic lymph nodes ( cutoff values 1 cm and 0.5 cm minimum axial diameter )  . 
the endocervix was the site of origin of 25% ( 13 / 53 ) of the cervical tumours and the exocervix the site of origin of 75% ( 40 / 53 )  . 
in the assessment of the lymph nodes , when using a cutoff value of 1 cm , mr imaging had a sensitivity , specificity and diagnostic accuracy of 28% , 100% and 89% , respectively . 
sono state sottoposte ad esame rm 53 pazienti con carcinoma della cervice uterina confermato istologicamente , candidate a chirurgia conservativa . lanalisi delle immagini ha compreso : localizzazione e dimensioni del tumore , infiltrazione dellanello stromale , infiltrazione dei fornici vaginali ed estensione oltre lorifizio uterino interno , presenza e dimensioni di linfonodi pelvici o lombo - aortici ( valore soglia 1 cm e 0 , 5 cm di diametro assiale minimo )  . 
nella valutazione dellinfiltrazione dei fornici vaginali la rm ha riportato una sensibilit del 67% , una specificit del 92% ed unaccuratezza diagnostica del 91% ; nella valutazione dellestensione oltre lorifizio uterino interno dell 86% , 93% e 92% , rispettivamente . 
la rm ha dimostrato unelevata accuratezza nella valutazione pre - operatoria dellestensione ( t ) radiol med ( 2009 ) 114 : 960975 imaging had a sensitivity , specificity and diagnostic accuracy of 33% , 92% and 83% , respectively . 
mr imaging had a high level of accuracy in the preoperative assessment of the extent of cervical tumour in patients eligible for conservative surgery . accuracy is lower in the evaluation of the pelvic and lumboaortic lymph nodes . keywords uterine neoplasms cervical cancer magnetic resonance imaging staging tumorale in pazienti candidate ad intervento chirurgico conservativo . 
laccuratezza minore nella valutazione dei linfonodi pelvici e lombo - aortici . parole chiave neoplasie dellutero carcinoma della cervice risonanza magnetica stadiazione introduction introduzione localized uterine cervical carcinoma [ stage iia , with tumour diameter < 4 cm , according to the classification of the international federation of gynaecologists and obstetricians ( figo ) ] may be treated with surgery or exclusive radiation therapy , with similar 5 - year survival rates [ 1 , 2 ]  . nonetheless , in many centres , surgery remains the treatment of choice [ 3 ]  . 
in patients with localized cervical carcinoma , radical surgery consisting of hysterectomy with parametrectomy extended to the pelvic wall , and pelvic and lumboaortic lymphadenectomy may represent overtreatment that exposes the patient to an increased risk of postoperative complications and morbidity [ 47 ]  . 
attempts to modulate the extent of surgical treatment while preserving the degree of oncological disease control may be justified both by the reduction of periand postoperative complications and by the lesser impact on the patients quality of life and sexual functioning . in this context , accurate preoperative clinical and imaging staging of local tumour extension and pelvic and lumboaortic lymph node involvement represent a primary medical need for the planning of surgical treatment . 
 magnetic resonance ( mr ) imaging has shown to be a valuable noninvasive diagnostic modality for evaluating parametrial invasion , which is key in distinguishing localised from advanced disease , leading to different treatment strategies [ 1315 ]  . 
to be able to plan a less aggressive surgical procedure , gynaecological oncologists need to be il carcinoma della cervice uterina localizzato allutero ( stadioiia , con diametro tumorale < 4 cm , secondo la classificazione della federazione internazionale di ginecologia e ostetricia figo ) , pu essere trattato mediante chirurgia o radioterapia esclusiva , con risultati a distanza simili in termini di sopravvivenza [ 1 , 2 ] ; tuttavia , la chirurgia il trattamento di scelta in molti centri [ 3 ]  . 
in pazienti con carcinoma della cervice localizzato allutero , un trattamento chirurgico radicale , che consiste in isterectomia con parametrectomia estesa alla parete pelvica e linfoadenectomia pelvica e lombo - aortica , pu risultare in un sovra - trattamento , esponendo la paziente ad un aumentato rischio di complicanze post - operatorie e di morbilit [ 47 ]  . 
ad eccezione delle neoplasie di grosse dimensioni ( bulky disease ) , le pazienti con carcinoma cervicale localizzato allutero sono infatti potenziali candidate ad una chirurgia meno aggressiva [ 811 ]  . 
un tentativo di modulare lestensione del trattamento chirurgico , preservandone comunque la radicalit oncologica , potrebbe essere giustificato sia dalla riduzione delle complicanze perie postoperatorie , che dal miglior impatto sulla qualit della vita delle pazienti e sulla loro vita sessuale . in questa ottica , unaccurata stadiazione pre - operatoria clinica e strumentale della diffusione locale del tumore e del coinvolgimento dei linfonodi pelvici e lombo - aortici , rappresenta una necessit medica di primaria importanza nella pianificazione del trattamento chirurgico . 
la stadiazione del carcinoma della cervice si basa su criteri clinici , codificati dalla figo ; la stadiazione clinica , tuttavia , comparata con quella chirurgica , ha mostrato un range di errore che va dal 20% al 39% , a seconda dello stadio della malattia [ 12 ]  . 
five were found to have locally advanced disease at mr imaging and were consequently treated with neoadjuvant therapy following a multidisciplinary assessment . the other two refused to undergo mr imaging . 
at histopathology , 39 / 53 ( 73% ) patients had squamous cell carcinoma , 9 / 53 ( 18% ) had adenocarcinoma and 5 / 53 ( 9% ) had adenosquamous cell carcinoma . 
 magnetic resonance imaging mr images were obtained with a 1.5 - t machine ( echospeed , ge medical system , milwaukee , wi , usa ) using a multichannel pelvic coil . 
to limit intestinal peristalsis , patients were instructed to fast for at least 4 h prior to the examination and received an intramuscular injection of 1 mg of butyl scopolamine ( buscopan , schering , germany ) 10 min before the examination . axial t1 - weighted spin - echo ( se ) images were acquired with the following parameters : tr / te 500 / 14 ms , slice thickness 4 mm , interval 1 mm , matrix 256256 . 
axial t2weighted rapid acquisition with relaxation enhancement ( rare ) fast spin - echo ( fse ) images were acquired with tr / te 4 , 000 / 85 ms , echo train length ( etl ) 12 , slice thickness 4 mm , interval 1 mm , matrix 256256 . 
 lo scopo di questo studio quello di determinare laccuratezza della rm nella stadiazione pre - operatoria di pazienti con carcinoma della cervice clinicamente localizzato , candidate ad un intervento chirurgico meno esteso . 
in accordo con i criteri di stadiazione della figo , tutte le pazienti presentavano una neoplasia della cervice uterina localizzata ( stadio < iib ) , alla visita ginecologica in narcosi , e sono state sottoposte a risonanza magnetica ( rm )  . 
sette pazienti sono state escluse dallo studio : 5 di queste avevano una malattia localmente avanzata allindagine rm e , di conseguenza , sono state sottoposte a trattamento neoadiuvante , a seguito di una valutazione multidisciplinare . 
allesame istopatologico 39 / 53 ( 73% ) pazienti avevano un carcinoma squamoso , 9 / 53 ( 18% ) pazienti un adenocarcinoma e 5 / 53 ( 9% ) pazienti un carcinoma adeno - squamoso . 
 risonanza magnetica le immagini rm sono state ottenute utilizzando un magnete da 1 , 5 t ( echospeed , ge medical system , milwaukee , wis ) , usando una bobina pelvica multicanale . 
interpretation differences were resolved by consensus ; evaluation was concordant in 92% of cases and discordant in 8% . in each patient , tumour extent and nodal involvement was assessed on the mr images . 
evaluation of the tumour , performed on t2 - weighted images , comprised site of origin , size , infiltration of the cervical stroma and vaginal fornices and relationships between tumour and internal os of the endocervical canal . 
tumour size was determined by measuring its maximum diameters in three planes and calculating its volume by multiplying the three diameters by 0.52 , according to the ellipsoid formula . tumour infiltration of the cervical stroma was assessed based on the interruption of stromal hypointensity on t2weighted images and classified as < 50% or > 50% of total stromal thickness . 
likewise , the vaginal fornices ( anterior , posterior , left and right ) were considered infiltrated in the presence of an interruption of the hypointensity of the vaginal wall on t2 - weighted images . 
the relationship between the tumour and the internal os of the endocervical canal allowed for the distinction between tumours confined to the cervix from those extending to the uterine body . 
the internal os was recognised as the point of constriction of the uterine contours and the point of evidence of the uterine arteries and , on t2 - weighted images , as the point at which the low signal intensity of the cervical stroma changed into the intermediate signal intensity of the myometrium . the presence , size and site of the pelvic and lumboaortic lymph nodes were also recorded . 
lymph nodes were classified as external iliac , internal iliac , common iliac , internal obturator , bilaterally and lumboaortic in agreement with the surgeons and pathologists [ 17 ]  . 
le immagini assiali t2 - dipendenti rare - fse ( rapid acquisition with relaxation enhancement - fast spin echo ) sono state ottenute con tr / te 4000 / 85 ms , lunghezza del treno di echi ( etl ) 12 , spessore di scansione 4 mm , intervallo 1 mm , matrice 256256 . 
le immagini sagittali e coronali oblique ( parallele allasse longitudinale del canale endocervicale ) t2 - dipendenti rare - fse sono state ottenute con i seguenti parametri : tr / te 35004000 / 90 ms , etl 12 , spessore di scansione 3 mm , intervallo 1 mm , matrice 256256 . sono state inoltre acquisite immagini assiali t2 - dipendenti rare - fse , usando una bobina per il corpo , fino agli ili renali , per valutare leventuale presenza di linfoadenomegalie della catena lombo - aortica . 
 analisi delle immagini lanalisi dellimmagine stata effettuata da due radiologi ( rm , bg ) con esperienza in diagnostica per immagini in ginecologia oncologica ( > 10 anni ) , e la valutazione stata eseguita senza conoscere i dati clinici . 
le discrepanze interpretative sono state risolte per consenso ; le valutazioni sono state concordi tra i due osservatori nel 92% dei casi e discordanti nel 8% . per ogni paziente sono stati analizzati mediante rm lestensione tumorale ed il coinvolgimento linfonodale . lanalisi del tumore , eseguita nelle immagini t2 - dipendenti , ha compreso : la sede di insorgenza , le dimensioni del tumore , linfiltrazione dello stroma cervicale e dei fornici vaginali , i rapporti tra la neoplasia e lorifizio interno del canale endocervicale . 
le dimensioni del tumore sono state determinate misurando i diametri massimi sui tre piani , e calcolandone il volume 3d moltiplicando i tre valori per 0 , 52 , secondo la formula dellellissoide . linfiltrazione tumorale dello stroma cervicale stata valutata in base allinterruzione dellipointensit stromale nelle immagini t2 - dipendenti e classificata come < 50% o > 50% del suo spessore totale . 
analogamente , i fornici vaginali ( anteriore , posteriore , sinistro e destro ) sono stati considerati infiltrati quando presente uninterruzione dell ipointensit , nelle immagini t2 - dipendenti , della parete vaginale . 
twenty - three out of 53 patients ( 43% ) underwent piver type 3 hysterectomies [ 14 ] , 17 / 53 ( 32% ) underwent type 2 , 9 / 53 ( 17% ) underwent type 4 and 4 / 53 ( 8% ) underwent piver type 1 . 
the cervix was separated from the uterine body , completely sectioned along the longitudinal plane ( 12 sections on average ) and stained with haematoxylin and eos the sections were analysed by a single pathologist ( gz ) according to the following criteria : presence and degree of infiltration of the cervical stroma measured from the basal membrane to the maximum penetration depth , involvement of the surgical margins ( positive or negative margins ) and infiltration of the vaginal fornices . 
subsequently , the pathologist documented the total number of lymph nodes , their position , presence / absence of metastatic foci , size of lymph nodes along the short axis and any metastatic foci detected in the lymph nodes . 
 finally , mr findings in regard to infiltration of the cervical stroma and vaginal fornices , relationship of the tumour with the internal os of the endocervical canal and the presence of pelvic or lumboaortic nodal metastases were consensually compared with histological findings by two radiologists ( rm , bg ) , a pathologist ( gz ) and a stroma cervicale cambia nellintermedia intensit di segnale del miometrio . sono stati inoltre rilevati la presenza , le dimensioni e la sede dei linfonodi pelvici e lombo - aortici . 
i linfonodi sono stati classificati in : iliaci esterni , iliaci interni , iliaci comuni , otturatori interni , bilateralmente e lombo - aortici , in accordo con i chirurghi ed i patologi [ 17 ]  . 
sono stati impiegati due valori soglia per distinguere i linfonodi metastatici da quelli infiammatori : 1 cm ( criterio 1 ) e 0 , 5 cm ( criterio 2 )  . infine laccuratezza della rm stata valutata in ciascuna paziente combinando tutti i parametri sopra menzionati , in modo da considerare la reale utilit dellindagine rm per il ginecologo oncologo al fine di pianificare la terapia pi appropriata per ciascuna paziente . tutte le pazienti sono state sottoposte ad un programma di follow - up che consiste in : esame clinico e test di papanicolau ( pap - test ) ogni 3 mesi per i primi 3 anni ed ogni 6 mesi per i seguenti 2 anni ; indagine rm ogni 6 mesi per i primi 2 anni e annuale per i seguenti 3 . 
durante il follow - up 49 / 53 pazienti ( 93% ) non hanno mostrato nessuna evidenza di recidiva di malattia , mentre 4 / 53 ( 7% ) hanno avuto una recidiva a diversa distanza di tempo : 1 paziente dopo 3 mesi dallintervento chirurgico , 1 paziente dopo 5 mesi , 1 paziente dopo 16 mesi ed 1 paziente dopo 20 mesi . 
 chirurgia / istopatologia linfoadenectomia tutte le pazienti sono state sottoposte ad intervento chirurgico entro un intervallo di tempo medio dalla rm di 18 , 8 giorni ( 155 giorni )  . 
ventitre / 53 pazienti ( 43% ) hanno subito unisterectomia di tipo 3 secondo piver [ 14 ] , 17 / 53 ( 32% ) di tipo 2 , 9 / 53 pazienti ( 17% ) di tipo 4 e 4 / 53 pazienti ( 8% ) sono state sottoposte ad unisterectomia di tipo 1 secondo piver . 
nei casi in cui il risultato della palpazione chirurgica e dellesame istologico intraoperatorio stato negativo , il chirurgo ha eseguito unisterectomia radicale . quando il risultato stato positivo , il chirurgo ha completato la procedura tramite isterectomia radicale e radiol med ( 2009 ) 114 : 960975 gynaecologist ( mds ) to determine the diagnostic accuracy of mr imaging . linfoadenectomia lombo - aortica fino allorigine dellarteria mesenterica inferiore . 
 statistical analysis sensitivity , specificity , positive and negative predictive values and diagnostic accuracy were calculated for infiltration of the vaginal fornices , tumour extension to the internal os of the endocervical canal and nodal involvement . 
with regard to nodal involvement , two series of values were calculated based on two cutoff values 1 cm and 0.5 cm measured along the short axis of the lymph node . 
interobserver variability was calculated using the k statistic . concordance between mr imaging and histopathological findings was calculated for each patient , taking into account all parameters described above . results at surgery / histopathology , 45 / 53 ( 85% ) patients had stage ib cervical carcinoma , 5 / 53 ( 9% ) stage ia and 3 / 53 ( 6% ) stage iia . 
le sezioni sono state analizzate da un solo anatomo - patologo ( gfz ) , secondo i seguenti criteri : presenza e grado di infiltrazione dello stroma cervicale , misurata dalla membrana basale fino alla massima profondit di infiltrazione ; coinvolgimento dei margini chirurgici da parte del tumore ( margini positivi o negativi ) ; infiltrazione dei fornici vaginali . 
successivamente , il patologo ha documentato il numero totale di linfonodi , la loro posizione , la presenza / assenza di focolai metastatici , le dimensioni dei linfonodi lungo lasse minore e dei focolai metastatici eventualmente rilevati nei linfonodi . 
 infine i rilievi della rm sullinfiltrazione dello stroma cervicale , sui fornici vaginali , sui rapporti della neoplasia con lorifizio interno del canale endocervicale , cos come la presenza di linfonodi metastatici pelvici o lombo - aortici , sono stati confrontati con i risultati dellistologia collegialmente da due radiologi ( rm , bg ) , un anatomo - patologo ( gfz ) ed un ginecologo ( mds ) , ed stata quindi determinata laccuratezza diagnostica della rm . analisi statistica fornici vaginali , la sensibilit , la specificit , i valori predittivi positivi e negativi , laccuratezza diagnostica sono stati calcolati per linfiltrazione dei tumorale allorifizio interno del canale endocervicale ed il coinvolgimento linfonodale ; per questo ultimo , sono state calcolate due diverse serie di valori , in base ai due valori soglia rispettivamente di 1 cm e 0 , 5 cm , misurati lungo lasse minimo del lestensione fig.1a , b cervical carcinoma : site of origin . sagittal t2 - weighted rapid acquisition with relaxation enhancement ( rare ) image ( tr / te 4 , 000 / 90 ms ) shows site of origin of the cervical neoplasa cervical carcinoma originating from the endocervix in a 54 - year - old woman . 
a sagittal t2 - weighted rapid acquisition with relaxation enhancement ( rare ) image ( tr / te 4 , 000 / 90 ms ) shows cervical carcinoma ( arrowhead ) in a 61 - year - old woman , which is infiltrating the underlying cervical stroma for < 50% of its thickness ( arrow )  . 
a immagine sagittale t2 - dipendente rare ( tr / te 4000 / 90 ms ) , che mostra il carcinoma della cervice uterina ( testa di freccia ) in una donna di 61 anni , che infiltra lo stroma cervicale sottostante per meno della met del suo spessore ( freccia )  . 
b immagine assiale t2 - dipendente rare ( tr / te 4000 / 90 ms ) della stessa paziente di a , che conferma linfiltrazione dello stroma cervicale da parte della neoplasia . 
c immagine assiale t2 - dipendente rare ( tr / te 4000 / 90 ms ) , che mostra infiltrazione dello stroma cervicale ( punta di freccia ) per pi della met del suo spessore da parte del carcinoma cervicale ( freccia curva ) , in una donna di 37 anni . ( 4% ) true positive results , 4 / 53 ( 7% ) false positive results and 1 / 53 ( 2% ) false negative result . 
la concordanza tra immagini di rm ed i reperti istopatologici stata calcolata per ciascuna paziente considerando tutti i parametri sopra menzionati . risultati alla chirurgia / istopatologia , 45 / 53 ( 85% ) pazienti avevano un carcinoma della cervice con stadio ib , 5 / 53 ( 9% ) con stadio ia e 3 / 53 ( 6% ) presentavano una malattia con stadio iia . 
neoplastic infiltration was present in 61 / 2 , 266 ( 3% ) lymph nodes , 44 / 61 ( 72% ) of which were pelvic and 17 / 61 ( 28% ) lumboaortic . 
positive pelvic nodes were located in the following sites : left common iliac in 14 / 44 ( 32% ) cases , left internal obturator in 15 / 44 ( 34% ) , right internal obturator in 6 / 44 ( 14% ) , left external iliac in 4 / 44 ( 9% ) , right external iliac in 4 / 44 ( 9% ) and left internal iliac in 1 / 44 ( 2% )  . 
la sensibilit , la specificit , il valore predittivo positivo e negativo e laccuratezza diagnostica delle immagini rm t2 - dipendenti sagittali , per infiltrazione tumorale attraverso lorifizio uterino interno sono stati 86% , 93% , radiol med ( 2009 ) 114 : 960975 fig . 
a coronal t2 - weighted rapid acquisition with relaxation enhancement ( rare ) image ( tr / te 4 , 200 / 90 ms ) shows infiltration of the right and the left vaginal fornices ( large arrows ) with obliteration of the hypointense vaginal wall ( small arrow ) in a 41year - old woman , the infiltration was confirmed at surgery . 
b the coronal t2 - weighted rare image ( tr / te 4 , 200 / 90 ms ) shows infiltration of the left vaginal fornix in a 27 - year - old woman . 
a immagine coronale t2dipendente rare ( tr / te 4200 / 90 ms ) , che mostra linfiltrazione dei fornici vaginali destro e sinistro ( freccia grande ) , caratterizzata dallobliterazione della parete vaginale ipointensa ( freccia piccola ) in una donna di 41 anni . 
b limmagine coronale t2 - dipendente rare ( tr / te 4200 / 90 ms ) , mostra linfiltrazione del fornice vaginale di sinistra in una donna di 27 anni . 
c nella stessa paziente , il prelievo istologico ( fissato con emotossilina ed eosina , 4 ) nel fornice vaginale di sinistra non ha confermato linfiltrazione , ma ha dimostrato solo la presenza di reazione infiammatoria iperplastica . 
conversely , with the cutoff value of 0.5 cm along the minimum axial diameter ( criterion 2 ) , its sensitivity , specificity , diagnostic accuracy and positive and negative predictive value were 33% , 92% , 83% , 43% and 89% , respectively ( table 1 )  . 
61 / 2266 ( 3% ) linfonodi mostravano infiltrazione neoplastica : tra questi ultimi 44 / 61 ( 72% ) erano pelvici e 17 / 61 ( 28% ) erano lombo - aortici ; tutte le pazienti con linfonodi neoplastici lombo - aortici avevano anche linfonodi pelvici neoplastici . 
i linfonodi pelvici positivi erano localizzati nelle seguenti sedi : iliaca comune di sinistra in 14 / 44 ( 32% ) casi , otturatoria interna sinistra in 15 / 44 ( 34% ) casi , otturatoria interna destra in 6 / 44 ( 14% ) casi , iliaca esterna sinistra in 4 / 44 ( 9% ) , iliaca esterna destra in 4 / 44 ( 9% ) ed iliaca interna sinistra in 1 / 44 ( 2% ) caso . 
allesame istologico , il diametro medio dei linfonodi metastatici , misurato lungo lasse minore , era di 0 , 5 cm ( intervallo 0 , 22 cm ) , mentre era di 0 , 8 cm ( intervallo 0 , 22 cm ) quando misurato lungo lasse maggiore ; il diametro radiol med ( 2009 ) 114 : 960975 medio dei focolai metastatici era di 0 , 5 cm ( intervallo 0 , 11 , 5 cm )  . 
 alla rm erano risultati positivi 80 linfonodi ; 29 / 80 ( 36% ) erano localizzati in sede otturatoria interna di sinistra , 22 / 80 ( 27% ) in sede otturatoria interna di destra , 14 / 80 ( 18% ) in sede iliaca esterna di destra , 8 / 80 ( 10% ) in sede iliaca esterna di sinistra , 3 / 80 ( 4% ) in sede iliaca comune di sinistra , 1 / 80 ( 1% ) era localizzato in sede iliaca comune destra e 3 / 80 ( 4% ) in sede lombo - aortica . 
in 9 / 12 pazienti ( 75% ) lerrore riguardava un solo parametro : 3 / 12 pazienti ( 25% ) mostravano linfonodi falsi negativi , 3 / 12 pazienti ( 25% ) mostravano fornici vaginali falsi positivi , ( 8% ) presentava un coinvolgimento 1 / 12 paziente dellorifizio uterino interno falsamente negativo , 1 / 12 paziente ( 8% ) presentava un coinvolgimento dellorifizio uterino interno falsamente positivo , e 1 / 12 paziente ( 8% ) mostrava fornici vaginali falsamente negativi . 
a sagittal t2 - weighted rapid acquisition with relaxation enhancement ( rare ) image ( tr / te 4 , 000 / 90 ms ) shows infiltration of the myometrium ( curved arrow ) by cervical cancer ( arrow ) beyond the internal os of the endocervical canal ( confirmed at surgery ) in a 62 - year - old woman . 
a immagine sagittale t2 - dipendente rare ( tr / te 4000 / 90 ms ) , che mostra linfiltrazione del miometrio ( freccia curva ) da parte del carcinoma cervicale ( freccia ) , attraverso lorifizio interno del canale endocervicale ( confermata alla chirurgia ) , in una donna di 62 anni . 
in 9 / 12 patients ( 75% ) , the error concerned one parameter only : 3 / 12 patients ( 25% ) showed false negative lymph nodes , 3 / 12 ( 25% ) had false positive vaginal fornices , 1 / 12 ( 8% ) had false negative extension to the internal os , 1 / 12 ( 8% ) had false positive extension to the internal os and 1 / 12 ( 8% ) had false negative vaginal discussione nelle pazienti con carcinoma della cervice uterina in stadio iniziale ( stadio figo < iia ) , la chirurgia il trattamento di scelta nella maggior parte dei centri , con leccezione delle neoplasie di diametro > 4 cm ( ib bulky ) [ 1 , 2 , 13 ]  . 
b in the same patient , the histopathology specimen ( hematoxylin and eosin stain , 10 ) confirmed the nodal metastases with complete invasion by neoplastic tissue . c in this other 35 - year - old patient , normal - size lymph nodes ( minimum diameter < 1 cm ) were detected on t2 - weighted axial images in the left external iliac space . 
b nella stessa paziente il prelievo istologico ( fissato con emotossilina e cosina , 10 ) , conferma le metastasi linfonodali , con invasione completa da parte di tessuto neoplastico . 
c in questaltra paziente di 35 anni , le immagini assiali t2 - dipendenti dello spazio iliaco esterno di sinistra , mostrano linfonodi con dimensioni nei limiti della norma ( diametro minimo < 1 cm )  . 
patients with early cervical carcinoma are potential candidates for a less extensive , but nonetheless oncologically radical , surgical operation that aims to reduce periand postoperative complications ( haemorrhage , fistula , bladder lymphocele , urinary lymphoedema , dysfunction ) and limit the heavy psychological impact of surgery on the patients quality of life and sexual functioning [ 8 , 18 ]  . 
this information regards , on the one hand , the tumour and specifically its size , location and infiltration of the internal os and vaginal fornices and on the other , the number , size and location of lymph nodes . 
 tumour size has prognostic implications , as it correlates with locoregional infiltration and nodal metastases [ 16 , 19 ]  . mr imaging allows direct measurement of tumour size , especially as regards its endocervical portion . 
nonetheless , the accuracy of mr imaging in determining tumour size has been widely demonstrated in previous studies [ 13 , 16 ]  . the depth of stromal infiltration is a major prognostic factor , as it is associated with the risk of nodal involvement [ 16 ]  . 
in our study , there was agreement between mr imaging and histopathology for parametrial infiltration in 40 / 53 ( 75% ) patients , with a tendency towards underestimation in 11 / 53 ( 21% )  . 
this is easily explained by the failure to visualize microscopic foci of infiltration . the fornices represent the upper third of the vagina , where the vaginal wall reflects back to merge with the cervical stroma . 
the presence of infiltration of the fornices indicates figo stage iia cervical carcinoma and implies a worse prognosis relative to tumour confined to the cervix ( stage ib )  . 
from the surgical point of view , infiltration of the vaginal fornices involves a more aggressive hysterectomy extending the upper vagina , consequently increasing the piver class [ 15 ]  . 
our study demonstrates a high specificity and accuracy , 92% and 91% , respectively , of mr imaging in evaluating infiltration of the vaginal fornices , but a low sensitivity ( 67% )  . 
given that the presence of false negative results for vaginal infiltration leads to undertreatment , it may be useful to introduce gadolinium chelates or air into the vagina to facilitate this evaluation [ 18 ] , or to perform a gynaecological examination under anaesthesia , as this allows direct visual inspection and biopsy of the fornices [ 13 , 20 ]  . 
in addition , in our study , there were four per la pianificazione del trattamento riguardano da una parte il tumore ed in particolare , le dimensioni , la localizzazione e linfiltrazione dellorifizio uterino interno e dei fornici vaginali , dallaltra i linfonodi , con il loro numero , le dimensioni e la localizzazione . 
un limite del nostro studio stato il mancato riscontro di una correlazione diretta tra la misurazione rm e quella istopatologica ; comunque , laccuratezza della rm nel determinare le dimensioni tumorali stata ampiamente dimostrata in precedenti studi [ 13 , 16 ]  . la profondit dellinfiltrazione stromale un importante fattore prognostico , in quanto si associa al rischio di diffusione linfonodale di malattia [ 16 ] ; inoltre , la sua integrit comporta un alto valore predittivo negativo per infiltrazione parametriale ( 96%99% ) [ 14 , 15 , 20 , 21 ]  . 
nel nostro studio c stata una concordanza rm / istopatologia per infiltrazione parametriale in 40 / 53 ( 75% ) pazienti , con una tendenza alla sottostima in 11 / 53 ( 21% ) , che pu essere facilmente spiegata dalla mancata visualizzazione dei focolai di infiltrazione microscopici . i fornici rappresentano il terzo superiore della vagina , dove la parete vaginale si ripiega per unirsi con lo stroma cervicale . 
la presenza di infiltrazione dei fornici , indica un carcinoma cervicale allo stadio iia , secondo la classificazione figo , ed implica una prognosi peggiore rispetto al tumore confinato alla cervice ( stadio ib )  . 
dal punto di vista chirurgico , linfiltrazione dei fornici vaginali comporta lesecuzione di unisterectomia pi estesa , che comprende anche la parte superiore della vagina , aumentando , di conseguenza , la classe nello schema secondo piver [ 15 ]  . 
il nostro studio dimostra unelevata specificit ed accuratezza , 92% e 91% rispettivamente , della rm nel valutare linfiltrazione dei fornici vaginali , ma una bassa sensibilit ( 67% )  . 
abbiamo riportato 1 falso negativo , in cui non siamo stati in grado di distinguere il tumore dalla parete vaginale . dato che la presenza di falsi negativi per infiltrazione vaginale comporta un sotto - trattamento , pu essere daiuto lintroduzione nel lume vaginale di chelati del gadolinio o di aria , per una loro pi agevole valutazione [ 18 ] , oppure affidarsi alla visita ginecologica in narcosi , in quanto questa in grado di visualizzare direttamente i fornici vaginali e permette di eseguire prelievi bioptici [ 13 , 20 ]  . 
nel nostro studio sono stati inoltre riportati 4 falsi positivi , due dei quali dovuti alla presenza di una reazione flogistica aberrante , che molto difficile da distinguere dallinfiltrazione neoplastica con la rm . 
questi falsi positivi hanno portato ad un sovra - trattamento , che comunque non ha interferito con la prognosi delle pazienti . 972 radiol med ( 2009 ) 114 : 960975 false positive results , two due to the presence of an aberrant inflammatory reaction , which is very difficult to distinguish from neoplastic infiltration on mr imaging . 
these false positive results led to overtreatment , which did not , however , interfere with the patients prognosis . the relationship between tumour and internal os of the endocervical canal and the presence of tumour extension to the uterine body constitute an important prognostic factor and are correlated with the risk of nodal involvement [ 1 ]  . moreover , this prognostic factor may be important in young patients ( < 35 years ) with localised cervical cancer who wish to have a pregnancy . 
this group of patients requires a surgical approach that combines radical excision of the tumour with conservation of the uterus to preserve fertility ( trachelectomy ) [ 9 , 2022 ]  . 
in our study , we achieved a high level of diagnostic accuracy ( 92% ) in determining the relationship between the tumour and the internal os of the endocervical canal , with a specificity of 93% and a negative predictive value of 98% . in women with cervical carcinoma , the presence of nodal metastasis is an important risk factor that has a radical impact on prognosis and treatment planning and is associated with parametrial involvement in nonadvanced stages of disease [ 10 , 11 ]  . 
to differentiate normal from metastatic lymph nodes on mr imaging , a dimensional criterion is used that involves a cutoff value of 1 cm measured along the short axis of the node [ 2329 ]  . 
in our study , mr accuracy in evaluating nodal metastasis was 89% , considering a cutoff value of 1 cm , and 83% with a cutoff value of 0.5 ctherefore , lowering the cutoff value from 1 cm to 0.5 cm leads to a higher false positive rate , with consequent reduction in specificity , accuracy and positive predictive value and a slight increase in sensitivity ( one patient ) ( table 1 )  . 
all lymph nodes that were found to be metastatic at histology and were false negative at mr imaging had a minimum axial diameter < 1cm and were thus not classified as pathological ( table 2 )  . 
in our study , surgically excised lymph nodes had a mean minimum diameter of 0.5 cm and maximum diameter of 0.8 cthe mean maximum diameter of small intraparenchymal metastases was 0.5 c the main limitation of diagnostic imaging lies in identifying small nodal metastases , as seen in our study . 
the presence of internal necrosis , which appears as an area of signal hyperintensity on t2 - weighted mr images , was of no assistance in our study : none of the 61 neoplastic lymph nodes showed this feature , which is more commonly found in large lymph nodes , as reported by other studies ( mean diameter 2.3 cm ) [ 30 ]  . il rapporto del tumore con lorifizio interno del canale endocervicale e la presenza di estensione del tumore al corpo dellutero sono un importante fattore prognostico e sono correlati al rischio di coinvolgimento linfonodale [ 1 ]  . inoltre , questo fattore prognostico pu essere importante nelle pazienti giovani ( < 35 anni ) con carcinoma cervicale localizzato che desiderano una gravidanza . 
in questo gruppo di pazienti richiesto un approccio chirurgico che combini lescissione radicale del tumore e la conservazione dellutero per preservare la fertilit ( trachelectomia ) [ 9 , 2022 ]  . 
nel nostro studio stato raggiunta unalta accuratezza diagnostica ( 92% ) nel determinare il rapporto tra tumore e orifizio interno del canale endocervicale , con una specificit del 93% ed un valore predittivo negativo del 98% . nelle donne con carcinoma della cervice la presenza di linfonodi metastatici un importante fattore di rischio che cambia radicalmente la prognosi e la pianificazione terapeutica ed associato a coinvolgimento del parametrio negli stadi non avanzati [ 10 , 11 ]  . 
nellimaging rm per differenziare i linfonodi normali da quelli metastatici viene utilizzato un criterio dimensionale che prevede un valore soglia di 1 cm misurato lungo il diametro minore [ 2329 ]  . laccuratezza della rm nellidentificare linfonodi metastatici varia dal 75% al 100% , con un valore medio del 86% [ 2329 ]  . 
nel nostro studio laccuratezza della rm nella valutazione dei linfonodi metastatici stata del 89% , considerando come valore soglia 1 cm , e del 83% considerando come valore soglia 0 , 5 cm ; quindi , abbassando il limite del valore soglia da 1 cm a 0 , 5 cm , aumentano i falsi positivi , con conseguente riduzione della specificit , dellaccuratezza e del valore predittivo positivo e con lieve aumento della sensibilit ( 1 paziente ) ( tabella 1 )  . 
tutti i linfonodi metastatici allistologia e falsi negativi alla rm , presentavano un diametro assiale minimo < 1 cm e , pertanto , non sono stati classificati come patologici ( tabella 2 )  . 
il diametro medio dei linfonodi asportati chirurgicamente nel nostro studio stato , infatti , di 0 , 5 cm il minimo e di 0 , 8 il massimo ; il diametro massimo medio delle piccole metastasi intraparenchimali stato di 0 , 5 c il limite pi grande della diagnostica per immagini stato quello di individuare le piccole metastasi linfonodali , come emerso dai dati del nostro studio . 
una possibile soluzione potrebbe essere lutilizzo di mezzo di contrasto ultrasmall superparamagnetic iron oxide ( uspio ) [ 30 ] , o la tomografia ad emissione di positroni [ 29 ]  . 
la presenza di necrosi interna , che si visualizza tramite rm come unarea di iperintensit nelle sequenze t2 - dipendenti , non ci stata daiuto nel nostro studio : dei 61 linfonodi neoplastici , nessuno mostrava questo reperto , che invece pi facile ritrovare in linfonodi di grandi dimensioni , come riportato in altri studi in cui il diametro medio era di 2 , 3 cm [ 30 ]  . nel nostro studio stata riportata unimportante discrepanza tra il numero di linfonodi asportati e quelli osservati radiol med ( 2009 ) 114 : 960975 table 2 evaluation of false negative lymph nodes on magnetic resonance ( mr ) imaging ( using a cutoff value of 1 cm ) compared with histopathology histopathology mr imaging total no . 
totale dei sede dei linfonodi diametro linfonodi metastatici metastatici massimo del linfonodo pi voluminoso ( cm ) dimensioni dei n totale di foci metastatici ( cm ) linfonodi visualizzati diametro minimo del linfonodo pi voluminoso ( cm ) istopatologia para - aortici para - aortici 10 , 4 0 , 80 , 4 10 , 4 10 , 8a 10 , 3 0 , 90 , 4 10 , 6 10 , 5a 0 , 70 , 5 0 , 50 , 5 0 , 90 , 8 10 , 5 1 , 20 , 7 0 , 50 , 2 0 , 70 , 4 1 , 20 , 5 1 , 2a 1 , 1a sede dei linfonodi non visualizzati non visualizzati non visualizzati non visualizzati non visualizzati non visualizzati para - aortici d , destra ; s , sinistra ; oi , otturatori interni ; ie , iliaci esterni ; ic , iliaci comuni aestensione extracapsulare 974 radiol med ( 2009 ) 114 : 960975 in our study , there was a major discrepancy between the number of excised lymph nodes and the number of nodes observed on mr imaging . 
most probably this was due to two factors : some lymph nodes were counted more than once at histology owing to sectioning , and others were too small to be visualised by mr imaging . in conclusion , mr imaging had relatively good accuracy ( 77% ) in evaluating all surgical factors that the gynaecological oncologist needs for planning treatment . 
molto probabilmente questo dovuto a due fattori : alcuni linfonodi sono stati contati pi di una volta allistologia a causa dei tagli ed altri linfonodi erano troppo piccoli per essere visualizzati con la rm . in conclusione , la rm ha dimostrato una discreta accuratezza ( 77% ) nel valutare tutti i fattori chirurgici di cui ha bisogno il ginecologo oncologo per pianificare il trattamento . 
magrassi , ii universit di napoli , azienda ospedaliera universitaria , 80100 napoli , italy 4dipartimento di scienze chirurgiche , radiologiche e odontostomatologiche , unit di oncologia chirurgica universit di perugia , ospedale s . 
andrea delle fratte , 06134 perugia , italy 5dipartimento di radiologia , ospedale di budrio , azienda sanitaria locale bologna , 40054 budrio , italy 6dipartimento di scienze della salute , sezione di diagnostica per immagini , universit del molise , c.da tappino , 86100 campobasso , italy correspondence to : m . 
we retrospectively reviewed the hepatic arterial - dominant phase ( hap ) , portal venous phase ( pvp ) and delayed - phase ( dp ) helical ct images of 47 patients with 52 atypical small ( 2cm ) hhs associated with 34 typical small hhs . 
sono stati valutati retrospettivamente gli esami tc trifasici in fase dominante - arteriosa ( fa ) , fase venosa portale ( fvp ) e fase tardiva ( ft ) , di 47 pazienti con 52 emangiomi epatici ( ee ) atipici di piccole dimensioni ( 2 cm ) associati a 34 ee tipici piccoli . 
on dp images , the appearance of atypical small hhs was identical to that of typical small hhs in all cases ( p < 0.0001 ) , with lesions showing homogeneous isoattenuation to the aorta or liver parenchyma without peripheral capsule . 
in ft laspetto degli ee atipici di piccole dimensioni ( isodensit rispetto allaorta o al parenchima epatico con assenza di capsula periferica ) risultato sovrapponibile a quello degli ee tipici di piccole dimensioni ( p < 0 , 0001 )  . 
unlike typical hhs , these lesions do not show globular or nodular peripheral enhancement similar to the attenuation of blood vessels at rapid ct with bolus administration of contrast material . 
to our knowledge , there have been only few reports investigating three - phase on hepatic arterialdominant phase ( hap ) , portal venous phase ( pvp ) , and delayed phase ( dp ) helical ct imaging in characterising hhs [ 7 ]  . 
the rationale for using three - phase helical ct is that the pvp is the most sensitive phase for lesion detection , whereas the hap and dp can supply additional information on the vascularity of the lesions that may help to clarify their nature [ 7 ]  . 
the purpose of this paper is to describe the findings of atypical small ( 2 cm ) hhs in non - cirrhotic liver to verify the usefulness of triple - phase helical ct . 
 materials and methods patients we retrospectively reviewed the ct images of 52 small ( < 2 cm ) hhs in 47 patients studied over the past 4 years lemangioma epatico ( ee ) rappresenta la neoplasia benigna pi frequente del fegato . 
lintroduzione nella pratica clinica della tomografia computerizzata ( tc ) spirale ha determinato un ulteriore aumento del riscontro di ee di piccole dimensioni ( 2 cm ) e di forme atipiche [ 2 ]  . queste ultime sono lesioni con aspetto inusuale che , diversamente dagli ee classici , non esibiscono , dopo iniezione a bolo di mezzo di contrasto ( mdc ) per vena , enhancement globulare e periferico , ad andamento centripeto . 
il rilievo di un ee atipico di piccole dimensioni , in particolare nel paziente oncologico , pone spesso problemi di diagnosi differenziale , poich tali lesioni possono simulare neoplasie epatiche benigne e maligne sia ipoche ipervascolari o metastasi . 
rari lavori , invece , su casistiche limitate , hanno valutato mediante tc trifasica in fase dominante - arteriosa ( fa ) , fase venosa portale ( fvp ) e fase tardiva ( ft ) laspetto degli ee atipici [ 7 ]  . 
il razionale della tc trifasica , nella caratterizzazione delle lesioni focali epatiche consiste in una maggiore sensibilit della fvp nellidentificazione delle lesioni , mentre la fa e la ft consentono di ottenere informazioni sulla loro vascolarizzazione e sulla loro possibile natura [ 7 ]  . 
scopo del presente studio quello di riportare i diversi aspetti degli ee atipici di piccole dimensioni ( 2 cm ) con tc spirale a singolo e multistrato trifasica nel paziente non - cirrotico , al fine di verificare laffidabilit diagnostica della metodica . 
patients ( 16 women and 31 men ; age range 2584 years , mean age 56.8 years ) underwent triple - phase ct to further investigate atypical small hhs classified as indeterminate lesions at ultrasonography ( us ) or single - phase or biphasic ct , or as part of preoperative staging or follow - up of known extrahepatic primary malignancies . exclusion criteria included steatosis , cirrhosis , elevated - fetoprotein levels , concurrent benign adenoma , focal nodular hyperplasia ( fnh ) or malignant hepatic tumours , or use of oral contraceptives in the 6 months prior to the study . lesions excluding the large ( > 2 cm ) hhs associated with atypical small hhs , the 52 atypical small hhs were solitary in 19 patients , ranging from one to three and / or coexisting with 34 typical small hhs in 28 patients . 
in the remaining patients , the final diagnosis was based on the clinical course or lack of change in lesion appearance or size for at least 25 ( range 648 ) months at follow - up with us , ct and magnetic resonance imaging ( mri )  . ct technique ct scans were obtained by using a single - detector - row helical ct scanner ( advantage ave 1 , philips medical systems , best , the netherlands ) in 26 patients and a 16detector - row helical ct scanner ( lightspeed plus and lightspeed plus 16 pro , ge healthcare , milwaukee , wi , usa ) in 21 patients . 
 materiali e metodi pazienti sono state analizzate retrospettivamente le immagini tc di 52 ee atipici di piccole dimensioni ( 2 cm ) , osservati nellarco degli ultimi quattro anni in 47 pazienti sottoposti al medesimo protocollo di studio con tecnica tc spirale trifasica . 
i pazienti ( 16 femmine e 31 maschi di et compresa tra 25 e 84 anni , et media 56 , 8 anni ) , sono stati sottoposti a tc trifasica in seguito al rilievo di ee atipici piccoli identificati come lesioni indeterminate riscontrate occasionalmente in corso di una precedente ecografia ( us ) , tc monoo bifasica oppure per una stadiazione preoperatoria o follow - up per neoplasia extraepatica primitiva maligna nota . 
 nessuno dei pazienti inclusi nello studio presentava steatosi epatica , cirrosi , elevati livelli di - fetoproteina , lesioni epatiche benigne adenoma , iperplasia nodulare focale ( inf ) o maligne , n assunzione di contraccettivi orali da almeno 6 mesi . 
 lesioni con esclusione degli ee epatici > 2 cm associati agli ee atipici di piccole dimensioni , i 52 ee epatici piccoli atipici in 19 pazienti erano unici ed in 28 pazienti in numero variabile da uno a tre e / o coesistenti con 34 ee tipici piccoli . 
la diagnosi di ee atipico in 7 dei pazienti con lesione unica stata confermata mediante esame istologico ( n = 2 ) e citologia aspirativa sotto guida ecografica ( n = 5 ) ; nei rimanenti pazienti la diagnosi radiologica stata confermata in base al decorso clinico ed allimmodificazione dellaspetto e delle dimensioni delle lesioni ad un follow - up radiologico con us , tc e / o risonanza magnetica ( rm ) variabile da 6 mesi a 48 mesi ( media , 25 mesi )  . 
 tecnica tc gli esami tc sono stati eseguiti con apparecchiatura tc spirale singolo strato ( advantage ave 1 ; philips medical systems , best , olanda ) in 26 pazienti e con tc 16 - strati / rotazione ( light speed plus and light speed pro 16 , ge healthcare , milwaukee , usa ) in 21 pazienti . 
il tempo di ritardo dallinizio delliniezione del mdc per vena , stato registrato a 30 secondi , 70 secondi e 5 minuti per la tc spirale a singolo strato ed a 35 secondi , 80 secondi e 5 minuti per la tc 16 - strati . 
 stata utilizzata una quantit media di 150 ml di mdc organo - iodato per paziente alla concentrazione di 300370 mgi / ml ( iopromide , ultravist schering , berlino , germania ) , 938 radiol med ( 2009 ) 114 : 935947 scanning parameters were : section thickness 2.5 mm and 5 mm and table feed 18.75 mm / s and 5 mm / s for the 16 - detector - row scanner and single - detector - row scanner , respectively . 
hap , pvp and dp images were reviewed for the presence of hhs . according to the literature [ 7 ] , the appearance of each lesion in each phase was described on the basis of the attenuation and homogeneity of the lesion in comparison with the aorta and recorded as follows : 1 . 
isoattenuating relative to the arterial syste atypical small hhs were defined as lesions with diameter < 2 cm and with unusual appearance on hap or pvp images with respect to classic forms . 
patterns of enhancement of atypical hhs were classified into three types : type 1 : hyperattenuating hh ( but less attenuating than the aorta ) either without ( type 1a ) or with transient hepatic attenuation difference ( thad ) around the lesion on hap images type 2 : homogeneously hypoattenuating hh in the ha or pvp ( type 2a ) and hypoattenuating area with brightdot sign in the hap or pvp ( type 2b )  . 
the bright - dot sign was defined as a tiny enhancing dot within an hh that did not progress to globular enhancement [ 4 ] type 3 : hypoattenuating hh with central enhancing area ( centrifugal enhancement pattern ) in the pvp . 
in accordo con i dati della letteratura [ 7 ] le caratteristiche di enhancement delle lesioni in ciascuna fase sono state classificate come segue , utilizzando come riferimento la densit dellaorta : 1 . 
 nel nostro studio sono stati definiti ee atipici di piccole dimensioni , lesioni con diametro 2 cm , che in corso di tc trifasica mostravano aspetti inusuali non riscontrabili nelle forme classiche in fa e fvp . 
tali lesioni , in base al pattern di enhancement , sono state distinte in tre tipi : tipo 1 , ee iperdenso ( ma con densit pi bassa rispetto allaorta ) in fa senza alterazione transitoria della densit epatica o thad ( transient hepatic attenuation difference ) ( tipo 1a ) o con associata thad ( tipo 1b ) ; tipo 2 , ee ipodenso , omogeneo in fa o fvp ( tipo 2a ) e ipodenso con puntiforme iperdensit intralesionale periferica in fa o fvp ( tipo 2b ) che non realizza un enhancement globulare [ 4 ] ; tipo 3 , ee ipodenso con iperdensit centrale in fvp e ad enhancement centrifugo . per ogni ee atipico di piccole dimensioni sono stati valutati : radiol med ( 2009 ) 114 : 935947 categorized as rapid if > 75% of the tumour volume enhanced ; intermediate if approximately 25%75% of the tumour volume enhanced and slow if < 25% of the tumour volume enhanced the qualitative ( visual ) analysis of the attenuation of atypical and typical small hhs during the dp . statistical analysis all the lesions were reviewed by three radiologists . 
statistical analysis was carried out using spss software for windows ( release 13.0 ; spss chicago , il , usa )  . results the results of triple - phase helical ct in atypical and typical small hhs are summarised in tables 1 and 2 , respectively . 
in fa stata correlata la presenza di thad con il tipo di enhancement delle lesioni ed in ft stato correlato laspetto degli ee atipici ( n = 52 ) di piccole dimensioni con quello delle forme tipiche ( n = 34 ) di piccole dimensioni . le differenze statistiche sono state calcolate mediante il test esatto di fisher . 
one type 1a lesion was resected , and pathology revealed the typical vascular pattern of cavernous hh consisting of multiple vascular spaces filled with blood , areas of fibrosis and organised thrombi . 
type 2a lesions showed hypoattenuation ( n = 2 ) risultati i risultati della tc trifasica relativi agli ee atipici e tipici di piccole dimensioni sono riportati rispettivamente nelle tabelle 1 e 2 . 
un ee atipico di tipo 1a stato asportato ; lesame istologico ha evidenziato la presenza di pattern vascolare tipico dellee cavernoso con ampie lacune vascolari ripiene di eritrociti e zone fibrotiche con piccoli vasi . 
1a - d triphasic helical ct of an atypical small hepatic haemangioma in the right liver lobe ( segment vi ) : type 1a , hyperattenuating area with rapid fill - in ( a - c ) and corresponding histological examination ( d )  . 
ct scan shows a homogeneous hyperattenuating lesion in the arterial phase ( a ) , substantially isoattenuating in the portal venous phase ( b ) and isoattenuating in the delayed phase at 5 minutes ( c ) after administration of contrast material . 
1a - d tc trifasica di un emangioma epatico atipico di piccole dimensioni nel lobo destro epatico ( segmento vi ) : tipo 1a , aspetto iperdenso a riempimento rapido ( a - c ) e corrispettivo esame istologico ( d )  . 
la lesione esibisce intenso omogeneo enhancement in fase arteriosa ( a ) ed aspetto sostanzialmente isodenso in fase venosa portale ( b ) e tardiva a 5 minuti ( c )  . 
2a - c triphasic helical ct of an atypical small hepatic haemangioma in the right liver lobe ( segment v ) : type 1b , hyperattenuating area with rapid fillin associated with transient hepatic attenuation difference ( thad )  . 
ct scans show a homogeneous hyperattenuating lesion with thad during the arterial phase ( a ) , which appears isoattenuating during the portal venous phase ( b ) and delayed phase at 5 minutes ( c ) after administration of contrast material . 
2a - c tc trifasica di un emangioma epatico atipico di piccole dimensioni nel lobo destro epatico ( segmento v ) : tipo 1b , aspetto iperdenso a riempimento rapido con thad . 
la lesione mostra intenso omogeneo enhancement e thad adiacente in fase arteriosa ( a ) ed aspetto isodenso ai vasi in fase venosa portale ( b ) e tardiva a 5 minuti ( c )  . 
six out of nine type 2a lesions underwent histological examination ( n = 1 ) or us - guided aspiration cytology completa di enhancement ( tipo 2a ) e forme ipodense con minimo puntiforme enhancement periferico ( bright - dot sign ) ( tipo 2b )  . 
il tipo 2a stato riscontrato in 9 dei 52 ee atipici ; tali lesioni in fa sono apparse ipodense ( n = 2 ) ed radiol med ( 2009 ) 114 : 935947 fig . 
3a - d triphasic helical ct of an atypical small hepatic haemangioma in the left liver lobe ( segment ii ) : type 2a , homogeneously hypoattenuating area during the portal - venous phase ( a - c ) and corresponding histological examination ( d )  . 
ct scans show an isoattenuating lesion in the arterial phase ( a ) , hypoattenuating in the portal venous phase ( b ) and isoattenuating in the delayed phase at 5 minutes ( d ) after administration of contrast material . 
3a - d tc trifasica di un emangioma epatico atipico di piccole dimensioni nel lobo sinistro epatico ( segmento ii ) : tipo 2b , aspetto ipodenso con completa assenza di enhancement in fase venosa portale e corrispettivo esame istologico ( d )  . 
la lesione isodensa in fase arteriosa ( a ) appare ipodensa in fase venosa portale ( b ) ed isodensa ai vasi in fase tardiva a 5 minuti ( c )  . 
 ( n = 5 ) : histology revealed extensive fibrosis with reduction of vascular channels , whereas aspiration cytology revealed few erythrocytes with predominant spindle cells , suggestive of fibrosis . 
in 6 delle 9 forme di tipo 2a la diagnosi stata ottenuta mediante esame istologico ( n = 1 ) e citologia aspirativa sotto guida ecografica ( n = 5 )  . 
lesame istologico ha dimostrato estesa fibrosi con riduzione dei vasi ; le 5 lesioni aspirate sotto guida ecografica hanno mostrato scarsi eritrociti con predominanza di cellule connettivali fusate espressione di fibrosi . 
 in ft stata osservata completa concordanza tra i tre osservatori in tutti i casi relativamente allaspetto degli ee atipici piccoli rispetto a quelli piccoli tipici ( p < 0 , 0001 ) con rilievo di lesioni isodense rispetto allaorta o al parenchima epatico ed assenza di capsula periferica . 
univoca concordanza tra i tre osservatori stata osservata in tutti i casi di ee atipico di piccole dimensioni di tipo 1a , 1b , 2a e 3 . concordanza elevata stata riscontrata , invece , nei casi di radiol med ( 2009 ) 114 : 935947 fig . 
4a - c triphasic helical ct of an atypical small hepatic haemangioma in the left liver lobe ( segment iv ) : type 2b , hypoattenuating area with slow fill - in and bright - dot sign . 
ct scan show isoattenuating lesion in the arterial phase ( a ) , hypoattenuating with peripheral bright dot in the portal venous phase ( b ) and isoattenuating in the delayed phase at 5 minutes ( c ) after administration of contrast material . 
4a - c tc trifasica di un emangioma epatico atipico di piccole dimensioni nel lobo sinistro epatico ( segmento iv ) : tipo 2b , aspetto ipodenso a riempimento lento con puntiforme iperdensit periferica ( bright - dot sign )  . 
la lesione isodensa in fa ( a ) appare ipodensa con puntiforme iperdensit periferica in fase venosa portale ( b ) e sostanzialmente isodensa ai vasi in fase tardiva a 5 minuti ( c )  . 
la lesione isodensa in fase arteriosa ( a ) , mostra aspetto ipodenso con puntiforme enhancement centrale in fase venosa portale ( b ) ed aspetto isodenso allaorta in fase tardiva a 5 minuti ( c )  . 
because the high incidence of atypical hh in radiological practice makes their surgical resection unfeasible , the accuracy of a radiological diagnosis of hh is based on follow - up imaging and changes in appearance and size over a long period of time [ 13 ]  . 
 the rationale for evaluating small ( 2 cm ) hhs by triplephase helical ct scans [ hepatic arterial - dominant phase ( hap ) , portal venous phase ( pvp ) , and delayed phase ( dp ) ] was that each phase of contrast enhancement provides useful information about the enhancement of lesions and thus helps to determine their vascularity . 
 [ 16 ] reported that thad is present in the 21% of atypical hh 2 cthad is thought to be related to the hyperdynamic status of rapidly enhancing small hhs where the large arterial inflow and consequently the large and rapid outflow results in early opacification of the draining vein and peritumoural enhancement [ 17 ]  . the incidence of atypical hypoattenuating or slow hhs ranges from 8% to 16% [ 4 , 17 ]  . 
such lesions include those with complete absence of enhancement ( that pose a significant diagnostic challenge and cannot be characterised by dual - phase ct ) [ 4 ] and hypoattenuating lesions with minimal enhancement or bright - dot sign , which has a considerable diagnostic value [ 4 , 18 ]  . 
 [ 19 ] reported that the histological examination of atypical hhs with inside - out pattern revealed fibrosis in variable degrees and a central area composed of numerous vascular spaces , which showed early and prolonged enhancement on dynamic bolus ct . 
 the aim of our study was to verify the usefulness of triple - phase helical ct in the diagnosis and to determine the enhancement pattern of small atypical hhs in noncirrhotic patient . 
la dizione radiologica ee atipico non quindi riconducibile ad una lesione vascolare di tipo capillare , ma esclusivamente allee cavernoso , eventualmente con alterazioni regressive ( infarto , necrosi , fibrosi , forme peduncolate , trombi , calcificazioni distrofiche )  . 
poich non proponibile lasportazione chirurgica per il numero elevato di casi riscontrati nella pratica radiologica , al fine di documentare con appropriatezza la diagnosi radiologica di ee , possiamo basarci sul follow - up ed evidenziare eventuali modificazioni del loro aspetto e delle dimensioni [ 13 ]  . 
a tal proposito va ricordato che una lesione che rimane stabile nel follow - up oltre ad un ee pu essere riferibile , sebbene pi raramente , ad un adenoma o a uniperplasia nodulare focale ( inf )  . nella valutazione degli ee atipici di piccole dimensioni ( 2 cm ) la tecnica tc trifasica , in fase dominante arteriosa ( fa ) , venosa - portale ( fvp ) e tardiva ( ft ) , trova il suo razionale nellidentificazione e nella valutazione del comportamento dellenhancement delle lesioni , elemento fondamentale per determinare la natura vascolare di una lesione in presenza di reperti atipici . 
 [ 16 ] , riportano che un differenza transitoria della densit del parenchima epatico o thad si riscontra nel 21% dei casi di ee atipici 2 csi tratta di unalterazione emodinamica dovuta al prevalente flusso arterioso degli ee atipici iperdensi di piccole dimensioni laddove un cospicuo afflusso arterioso ed il conseguente deflusso determinano una precoce opacizzazione della vena di drenaggio ed un enhancement peritumorale [ 17 ]  . relativamente agli ee atipici ipodensi lincidenza riportata in letteratura varia dal 8% al 16% [ 4 , 17 ] ; tali lesioni comprendono forme con completa assenza di enhancement ( per le quali si pongono le maggiori problematiche diagnostiche e che non possono essere caratterizzate con tecnica tc bifasica ) [ 4 ] , e forme ipodense con puntiforme minimo enhancement intralesionale periferico o segno del brightdot [ 4 , 18 ]  . 
in fact , 6 / 9 of type 2a hhs underwent histological examination ( n = 1 ) or us - guided aspiration cytology ( n = 5 )  . thirteen hypoattenuating hhs showed the bright - dot sign ( type 2b )  . 
 all atypical and typical small hhs exhibited isoattenuation or slight hyperattenuation relative to the aorta and no peripheral capsule on ct scan during dp ( 5 minutes after endovenous contrast material injection )  . 
hypervascular metastases , compared with hhs , have rapid wash - out and low attenuation on pvp and dp images [ 27 ] ; however , some metastases will show peripheral areas of low attenuation surrounding an enhanced centre on dp images [ 26 ]  . 
hypovascular metastases exhibit an enhancing rim ( probably due to well - perfused tumour tissue ) in the hap and fibrous tissue or central necrosis at histology [ 7 ]  . our study emphasises the role of adding dp acquisitions to the biphasic study for the diagnosis of atypical small hhs . 
in atypical hhs , the enhancement on dp is probably caused to longer retention of contrast material in large intravascular spaces , atipici di piccole dimensioni in pazienti non - cirrotici . 
nella serie esaminata , le forme con pattern iperdenso sono state le pi frequenti , riscontrate in 29 dei 52 ( 55% ) ee atipici di piccole dimensioni ; di queste 17 senza thad ( tipo 1a ) e 12 associate a thad ( tipo 1b )  . 
in un ee atipico di tipo 1a , asportato chirurgicamente , lesame istologico ha evidenziato aspetto tipico dellee cavernoso con ampie lacune vascolari ripiene di eritrociti e zone regressive fibrotiche con vasi di piccolo calibro . 
in 13 casi stato rilevato aspetto ipodenso con puntiforme iperdensit decentrata intralesionale o segno del bright - dot ( tipo 2b ) che , quando riconoscibile , assume particolare valore diagnostico . 
 in ft a 5 minuti dallinizio delliniezione del mdc per vena , tutti gli ee atipici , come quelli tipici di piccole dimensioni , sono apparsi isodensi o lievemente iperdensi allaorta e senza capsula periferica . 
tale aspetto risulta particolarmente valido nella diagnosi differenziale tra ee atipico 2 cm , lesioni ipervascolari [ adenoma , inf , carcinoma fibrolamellare epatocellulare , e metastasi ] e lesioni ipovascolari ( cisti < 1 , 5 cm , noduli di steatosi focale e metastasi ) [ 2026 ]  . 
 in tc multifasica gli ee atipici piccoli possono presentare aspetti sovrapponibili sia ai piccoli adenomi epatocelullari che ai noduli di inf senza cicatrice centrale ; appare in questi casi giustificato il ricorso alla risonanza magnetica ( rm ) con mdc epatotospecifico [ 23 , 24 ]  . 
le metastasi ipovascolari esibiscono orletto periferico di impregnazione ( tessuto neoplastico perfuso ) in fa e tessuto fibrotico o necrosi nella porzione centrale quando esaminate istologicamente [ 7 ]  . il nostro studio sottolinea limportanza della ft in associazione alla tecnica bifasica nella diagnosi di ee atipici di piccole dimensioni . 
negli ee atipici infatti , in ft lenhancement determinato probabilmente da una pi 946 radiol med ( 2009 ) 114 : 935947 resulting from slow flow , puddling and partial thrombosis [ 28 ]  . our study has several limitations . 
in agreement with the literature [ 29 , 30 ] , our study included patients who received a similar , if not identical , volume of contrast material with the same dose of iodine per body weight . 
particularly no change in the size or appearance of the lesion at six months as the main diagnostic criterion was used [ 3 , 4 , 6 , 13 , 15 , 18 ]  . 
however , in clinical practice , these disadvantages are offset by the benefits derived from the additional diagnostic information provided by the dp acquisition , which allows a confident diagnosis of hh and a significant reduction of further diagnostic investigations such as mri or biopsy . in summary , triple - phase helical ct can distinguish several types of atypical small hhs . 
dp acquisition ( after 5 minutes ) in association with biphasic ct technique further increases its value in the diagnosis of atypical hhs . the demonstration of patterns similar to typical forms is fundamental in establishing the vascular nature of the lesions and excluding nonvascular benign or malignant lesions . 
in accordo con la letteratura [ 29 , 30 ] , nella casistica sono stati inclusi pazienti in cui era stato somministrato un volume effettivo di mdc simile se non identico ovvero una quantit di contrasto con la stessa dose di iodio per peso corporeo . 
tuttavia , nella pratica clinica , linterpretazione delle immagini in ft , in associazione a quelle acquisite in fa e fvp , consente di ottenere informazioni utili ai fini della diagnosi di ee atipico determinando una sensibile riduzione di ulteriori indagini come la rm e la biopsia . in conclusione , la tc trifasica consente di distinguere vari tipi di ee atipici di piccole dimensioni . 
lacquisizione della ft a 5 minuti , in associazione ad un esame tc con tecnica bifasica , rafforza ulteriormente il ruolo di questa metodica nella diagnosi di ee atipico mostrando aspetti sovrapponibili a quelli delle forme tipiche ; tale elemento risulta essenziale nella conferma della natura vascolare delle lesioni , consentendo di escludere lesioni benigne e maligne di natura non vascolare . 
over a 23 - month period , 45 women ( mean age 58 years , range 2776 years ) with a known diagnosis of systemic sclerosis and a history of dysphagia underwent a dynamic and morphological study of the oral , pharyngeal and oesophageal phases of swallowing with videofluorography . 
the vfg swallow study identified alterations of epiglottal tilting associated with intraswallowing laryngeal penetration in 26 patients ( 57.8% ) , pooling of contrast agent in the valleculae and pyriform sinuses in 23 ( 51.1% ) and radiographic signs of nonspecific hypertrophy of the riassunto obiettivo . 
in un periodo di 23 mesi 45 pazienti di sesso femminile ( et media 58 anni ; range 2776 anni ) , con diagnosi certa di sclerodermia , che riferivano anamnesticamente disfagia sono stati sottoposti a studio dinamico e morfologico del tratto oro - faringeo della deglutizione e del tratto faringo - esofageo - cardiale mediante videofluorografia . 
tutti gli esami sono stati eseguiti con apparecchio telecomandato con arco a c digitale dotato di intensificatore di brillanza da 16 pollici , macchia focale da 0 , 6 a 1 , 2 mm e massima differenza di potenziale di 150 pkv in grafia e 120 pkv in scopia . 
per lo studio della deglutizione sono state acquisite sequenze cineradiografiche digitali con 12 immagini / secondo con matrice 512512 previa ingestione di boli progressivi di mdc baritato ad alta densit ( 250% p / v )  . 
la valutazione della peristalsi esofagea stata documentata con sequenze cineradiografiche digitali con 6 immagini / secondo , in ortostasi e clinostasi durante deglutizione di boli di bario ( 60% p / v ) ed , infine , stato effettuto , in clinostasi , il test del sifone dacqua ( wst ) per la valutazione del reflusso gastroesofageo ( gerd )  . 
lo studio della funzione deglutitoria , effettuato mediante vfg , ha evidenziato alterazioni del tilting epiglottico associato a fenomeni di penetrazione subepiglottica intradeglutitoria in 26 pazienti ( 57 , 8% ) , ristagno del mdc in corrispondenza delle vallecule glosso - epiglottiche e dei radiol med ( 2009 ) 114 : 948959 lingual and / or palatine tonsils in 18 ( 40% )  . 
indeed , in 40% of patients , radiographic signs were found that indicated nonspecific hypertrophy of the lingual tonsil and / or palatine tonsils and nonspecific signs of chronic pharyngeal inflammation , and gord was identified in 93% of patients , which in 40% of cases extended to the proximal third of the oesophagus . 
the data obtained were confirmed in 85% of cases with ph monitoring and in all cases with laryngoscopy . keywords scleroderma dysphagia gastro - oesophageal reflux disease videofluorography ( vfg ) seni piriformi in 23 ( 51 , 1% ) e segni radiografici di ipertrofia aspecifica della tonsilla linguale e / o delle tonsille palatine in 18 ( 40% )  . 
lo studio del viscere esofageo ha evidenziato la presenza di alterazioni della peristalsi nella totalit della popolazione ed in particolare 36 pazienti ( 80% ) manifestavano evidenti segni di atonia . 
infatti nel 40% dei pazienti , sono stati evidenziati segni radiografici riferibili ad unipertrofia aspecifica della tonsilla linguale e / o delle tonsille palatine segni aspecifici di flogosi cronica faringea ed stato , inoltre , identificato gerd , nel 93% dei pazienti che , nel 40% dei casi , si estendeva sino al iii prossimale del viscere . i dati ottenuti sono stati confermati nell85% anche da valutazione ph - metrica e nella totalit dei casi da valutazione laringoscopica . 
 parole chiave sclerodermia disfagia reflusso gastroesofageo videofluorografia ( vfg ) introduction introduzione scleroderma or systemic sclerosis ( ssc ) is a chronic disease of the connective tissue of unknown but probably autoimmune aetiology characterised by idiopathic fibrosis in multiple anatomical regions with involvement of the blood vessels , the skin and the internal organs [ 1 ]  . 
not always , however , is there a direct correlation between the clinical symptoms and la sclerodermia o sclerosi sistemica ( ssc ) una malattia cronica del tessuto connettivo ad eziologia sconosciuta , verosimilmente autoimmune , caratterizzata da fibrosi idiopatica pluridistrettuale con coinvolgimento dei vasi sanguigni , della cute e degli organi interni [ 1 ]  . 
i dati epidemiologici indicano una prevalenza di 12 , 625 casi per 100000 , incidenza di 0 , 06 e 1 , 9 / 100000 , et media 4565 anni con rapporto maschi / femmine di 1 / 4 [ 2 ]  . la patologia interessa il tratto gastroenterico , precocemente e severamente , con disordini della motilit conseguenti ad atrofia e fibrosi della muscolatura liscia , con prevalente coinvolgimento dellesofago , 75%90% dei casi [ 36 ] , specie nel tratto tratto medio e distale [ 7 ]  . 
le disfunzioni motorie stanno alla base delle alterazioni manometriche dello sfintere esofageo inferiore con conseguente insorgenza di reflusso acido gastro - esofageo ( gerd ) ed irritazione della mucosa esofagea , determinando una triade sintomatologica tipicamente caratterizzata da disfagia , generalmente descritta per i cibi solidi , epigastralgia e pirosi retro - sternale ( 50%90% dei casi ) [ 5 ]  . 
non sempre , per , vi una diretta correlazione tra la 950 radiol med ( 2009 ) 114 : 948959 the alterations recorded with manometry , ph monitoring and endoscopy [ 5 ]  . 
although these techniques are currently the reference methods for identifying motor alterations , gord , lesions of the mucosa and hiatus hernia [ 8 , 9 ] , none of them is able to provide direct information regarding the possible presence of primary alterations of swallowing of the food bolus . 
videofluorography ( vfg ) is the reference examination for the morphodynamic study of swallowing and is also a reliable technique for identifying oesophageal motor alterations , gord and hiatus hernia [ 1018 ]  . the aim of our study was to evaluate the role of vfg in the study of swallowing and oesophageal peristalsis in a group of patients with ssc . materials and methods from june 2005 to april 2007 , 45 women ( mean age 58 years , range 2776 years ) with ssc underwent a vfg study . the only inclusion criterion was a known diagnosis of ssc with a positive history of dysphagia . 
dynamic acquisitions were done with patients in the upright and supine positions during swallowing of progressive boluses ( 5 / 10 / 20 ml ) of barium ( 60% weight / volume ) ( prontobario bracco ) , and the water siphon test ( wst ) was done with the patient supine to evaluate the presence of gord . 
the following parameters were evaluated for each patient and each type of contrast agent with a morphological and functional study : vocal cord motility , soft palate motility , oral phase of swallowing , pharyngeal phase of swallowing , pooling of contrast agent in the valleculae and / or pyriform sinuses , oesophageal sintomatologia clinica e le alterazioni manometriche , phmetriche ed endoscopiche [ 5 ]  . 
le suddette metodiche rappresentano , oggi , le tecniche di riferimento per lidentificazione di alterazioni motorie , gerd , lesioni della mucosa ed ernia jatale [ 8 , 9 ]  . 
lo studio videofluorografico ( vfg ) lindagine di riferimento nello studio morfodinamico della deglutizione ed affidabile metodica anche nellidentificazione delle alterazioni motorie esofagee , del gerd e dellernia jatale [ 1018 ]  . 
 materiali e metodi da giugno 2005 ad aprile 2007 , 45 pazienti di sesso femminile ( et media 58 anni ; range 2776 anni ) affetti da sclerodermia sistemica sono stati sottoposti a studio videofluorografico . 
tutti gli esami sono stati eseguiti con apparecchio telecomandato con arco a c digitale ( telecomandato polifunzionale eurocolumbus tr3d , milano , italia ) dotato di intensificatore di brillanza da 16 pollici , macchia focale da 0 , 6 a 1 , 2 mm e massima differenza di potenziale di 150 pkv in grafia e 120 pkv in scopia . 
per lo studio della deglutizione sono state acquisite sequenze cineradiografiche digitali con 12 immagini / secondo con matrice 512512 , con paziente in ortostasi , mediante acquisizioni dinamiche durante la fonazione e durante deglutizione di boli progressivi ( 5 / 10 / 20 ml ) di bario ad alta densit ( 250% p / v ) ( bracco , milano , italia )  . 
la valutazione della peristalsi esofagea stata documentata con sequenze cineradiografiche digitali con 6 immagini / secondo con matrice 10241024 , con paziente in ortostasi e clinostasi mediante acquisizioni dinamiche durante deglutizione di boli progressivi ( 5 / 10 / 20 ml ) di bario ( 60% p / v ) ( prontobario , bracco ) ed , infine , stato effettuato , in clinostasi , il test del sifone dacqua ( wst ) per la valutazione del gerd . 
the study of the oesophageal phase instead showed the presence of generally hypotonic oesophageal dyskinesia in almost the entire patient population , with prevalent involvement of the middle and distal tract . 
per ogni paziente e per ogni tipo di mdc utilizzato sono stati valutati , mediante studio morfologico e funzionale , i seguenti parametri : motilit delle corde vocali ; motilit del palato molle ; fase orale della deglutizione ; fase faringea della deglutizione ; ristagno di mdc baritato nel contesto delle vallecule glosso - epiglottiche e / o dei seni piriformi , discinesia esofagea ; dilatazione esofagea ; deficit del clearing esofageo ; ernia jatale ; reflusso gastro - esofageo . tutti i pazienti sono stati sottoposti successivamente a valutazione laringoscopica , endoscopica e ph - metrica . 
1a , b fenomeni di penetrazione subepiglottica intradeglutitoria ( freccia ) ( a ) ; asimmetrico ribaltamento dellepiglottide per deficit a destra ( freccia ) da alterata motilit ( b )  . 952 radiol med ( 2009 ) 114 : 948959 fig . 
2a - d multiple hypopharyngeal findings due to hypertrophy of the lingual tonsil ( arrows ) , evaluated in the anteroposterior ( a , b ) and laterolateral ( c ) views . 
laryngoscopy confirmed the presence of laryngeal inflammation , with signs of arytenoid and interarytenoid oedema and reactive hypertrophy of the palatine tonsils and / or lingual tonsil in all patients . 
3a - d oesophageal motility disorder in upright ( a , b ) and supine ( c , d ) positions , with multiple antiperistaltic waves ( arrows )  . 
si apprezza inoltre formazione linfonodale calcifica ed ernia jatale da scivolamento ( punte di freccia )  . reflux oesophagitis in 34 ( 75% ) , the coexistence of sliding hiatus hernia and reflux oesophagitis in 34 ( 75% ) and the presence of sliding hiatus hernia alone in four ( 9% )  . 
the data obtained with the swallow study in patients with scleroderma were compared with those from 45 nonsclerodermic controls with a known history of modiche quote di mdc adese alla parete . 
5a - c impaired oesophageal clearing ( upright position ) with small amounts of contrast agent adhering to the walls ( arrow ) ( a ) ; sliding hiatus hernia with return to normal in the upright position ( arrows ) associated with multiple antiperistaltic waves ( arrowheads ) ( b , c )  . 
5a - c deficit di clearing esofageo ( decubito ortostatico ) con lieve verniciatura della parete viscerale ( frecce ) ( a ) ; ernia jatale da scivolamento riponibile in ortostasi ( frecce ) associata a multiple onde antiperistaltiche ( punte di freccia ) ( b , c )  . radiol med ( 2009 ) 114 : 948959 fig . 
6a , b reflusso gastro - esofageo con ricanalizzazione della colonna baritata sino al tratto medio - prossimale del viscere ( a ) e sino alla giunzione faringo - esofagea ( frecce ) ( b )  . gord and similar characteristics of age , gender and symptoms . 
the comparison revealed that in the controls , there was a substantially similar incidence of altered epiglottal motility ( n = 25 , 55.6% ) , of contrast agent pooling in the valleculae and pyriform sinuses ( n = 21 , 46.7% ) and of radiological signs attributable to hypertrophy of the lingual and / or palatine tonsils ( n = 16 , 35.6% ) ( table 1 )  . confermato la presenza di segni di flogosi laringea , con segni di edema aritenoideo , iteraritenoideo ed ipertrofia reattiva delle tonsille palatine e / o della tonsilla linguale , nella totalit dei pazienti esaminati . 
lindagine endoscopica ha confermato la presenza di ernia jatale da scivolamento in 38 pazienti ( 85% ) ed ha , inoltre , evidenziato segni di esofagite da reflusso in 34 di essi ( 75% ) , in 34 ( 75% ) la coesistenza di ernia jatale da scivolamento e segni di esofagite da reflusso ed in 4 ( 9% ) la presenza esclusivamente di ernia jatale da scivolamento . 
in rapporto allo scopo del lavoro , i dati ottenuti dallo studio della deglutizione dei paziente sclerodermici sono stati confrontati con quelli provenienti da una popolazione di controllo formata da 45 pazienti , non sclerodermici , con storia nota di gerd ed analoghe caratteristiche di et , sesso e sintomatologia . 
il confronto ha evidenziato come , nella popolazione di controllo , vi sia unincidenza sostanzialmente sovrapponibile , rispetto alla popolazione di studio , dei fenomeni di alterata motilit epiglottica presente in 25 pazienti ( 55 , 6% ) , del ristagno di mdc baritato in corrispondenza delle vallecule glossoepiglottiche e dei seni piriformi , presente in 21 di essi ( 46 , 7% ) ed , infine , dei segni radiologici riferibili ad ipertrofia della tonsilla linguale e / o palatine presente in 16 pazienti ( 35 , 6% ) ( tabella 1 )  . 
in esso si assiste , infatti , allinsorgenza di una progressiva atrofia e fibrosi della muscolatura liscia , conseguente ad un danno microvascolare su base ischemica da correlarsi ad abnorme deposito di collagene [ 36 ]  . 
tale evento , la cui causa primitiva risulta non essere nota , appare maggiormente evidente in corrispondenza della porzione medio - distale con progressiva compromissione della motilit e quindi della funzionalit globale del viscere [ 7 ]  . 
inoltre lesofago pu essere considerato un affidabile indicatore dellavanzamento globale della patologia mediante lincremento delleterogenea sinomatologia clinica , caratterizzata con maggiore frequenza da disfagia , epigastarlgia e pirosi retrosternale , correlata alle suddette progressive alterazioni . 
la severa compromissione esofagea , nei pazienti con ssc , da collegare a molteplici e coesistenti fattori come riduzione o assenza delle onde peristaltiche primarie e secondarie , ridotta pressione del les , associazione con ernia jatale , ritardato vuotamento gastrico e gerd . 
questultimo appare correlato sia ad una riduzione dellonda 956 radiol med ( 2009 ) 114 : 948959 table 1 oropharyngeal alterations in patients with and without scleroderma patients with scleroderma patients without scleroderma altered epiglottal motility contrast agent pooling in valleculae and / or pyriform sinuses radiological signs ascribable to hypertrophy of the lingual and / or palatine tonsil 26 ( 57.8% ) 23 ( 51.1% ) 18 ( 40% ) tabella 1 rilievo delle alterazioni oro - faringee in pazienti sclerodermici e non sclerodermici alterata motilit epiglottica ristagno mdc nelle vallecule glosso - epiglottiche e / o nei seni piriformi segni radiologici riferibili ad ipertrofia della tonsilla linguale e / o palatine 26 ( 57 , 8% ) 23 ( 51 , 1% ) 18 ( 40% ) 25 ( 55.6% ) 21 ( 46.7% ) 16 ( 35.6% ) 25 ( 55 , 6% ) 21 ( 46 , 7% ) 16 ( 35 , 6% ) pazienti sclerodermici pazienti non sclerodermici discussion the oesophagus is the gastrointestinal organ with the earliest and most frequent involvement in ssc . 
this event , the primary cause of which is unknown , appears particularly evident in the middledistal portion , with progressive compromise of motility and therefore overall function of the organ [ 7 ]  . 
in addition , the oesophagus can be considered a reliable indicator of the overall progression of disease , with the increase of the clinical symptoms more commonly dysphagia , chronic gastritis and retrosternal pyrosis being correlated with the above - mentioned alterations . 
severe oesophageal impairment in patients with ssc is linked to multiple coexisting factors such as the reduction or absence of primary and secondary peristaltic waves , reduced pressure of the lower oesophageal sphincter , association with hiatus hernia , delayed gastric emptying and gord . 
gord seems to be correlated with a reduction in the secondary peristaltic wave in the distal segment , a reduction in the physiological mechanism of oesophageal clearing and pressure changes of the lower oesophageal sphincter [ 5 , 7 ]  . 
in addition , the excessive exposure of various oesophageal segments to gastric acid leads to the onset of chronic inflammatory processes ( 33%66% ) , which in some cases can progress into a frank barretts oesophagus ( 13%16% ) and subsequent adenocarcinomatous degeneration ( 0.5% ) [ 9 ]  . the techniques most commonly used in the diagnostic workup of patients with ssc are manometry , endoscopy and ph monitoring . 
in particular , oesophageal manometry is considered the reference technique in the evaluation of motor alteration , given its ability in general to record reduced contraction in the distal 2 / 3 of the oesophagus and reduced pressure of the lower oesophageal sphincter . 
inoltre leccessiva esposizione dei diversi segmenti viscerali al succo acido gastrico permette linsorgenza di processi flogistici ( 33%66% ) cronici che , in alcuni casi , possono evolvere sino a configurare chiari quadri di metaplasia di barrett ( 13%16% ) e successivamente di degenerazione neoplastica adenocarcinomatosa ( 0 , 5% ) [ 9 ]  . 
in particolare , la manometria esofagea considerata la metodica di riferimento nella valutazione delle alterazioni motorie , documentando , in genere , la ridotta contrazione nei 2 / 3 distali del viscere ed una ridotta pressione del les , segni che , seppur presenti in corso di ssc , non sono specifici poich frequenti anche in altre patologie del tessuto connettivo come lamiloidosi , lalcolismo cronico , ecc [ 5 , 7 ]  . 
la ph - metria , oggi considerata metodica di riferimento nella diagnosi di gerd , permette lidentificazione qualitativa e quantitativa , delle alterazioni del ph intraesofageo presenti nel 54%90% dei pazienti affetti da ssc [ 8 ]  . 
lendoscopia , in ultimo , metodica di riferimento nella valutazione diretta della mucosa esofagea e , quindi , nellidentificazione sia dei quadri di esofagite da reflusso ( 60%75% ) sia dellernia jatale da scivolamento ( 85% ) [ 10 ]  . 
tuttavia nessuna delle suddette metodiche permette unaffidabile e sensibile valutazione , morfologica e funzionale , della fase orale e faringea della deglutizione , inoltre , non vi sono , nella recente letteratura , specifici studi che possano escludere la presenza di alterazioni primitive della deglutizione in corso di sclerosi sistemica [ 17 ]  . 
in questo contesto si colloca la vfg che si identifica come affidabile metodica radiologica nello studio della ssc , essendo in grado di radiol med ( 2009 ) 114 : 948959 signs are present in ssc , they are nonspecific and frequently seen in other connective tissue diseases such as amyloidosis , chronic alcoholism , etc . 
monitoring ph , which is currently considered the reference technique in the diagnosis of gord , is able to qualitatively and quantitatively identify the intraoesophageal ph alternations present in 54%90% of patients with ssc [ 8 ]  . 
finally , endoscopy is the reference technique for the direct evaluation of the oesophageal mucosa and therefore for identifying reflux oesophagitis ( 60%75% ) and sliding hiatus hernia ( 85% ) [ 10 ]  . 
vfg is in fact able to ensure detection and evaluation of changes not only to the oral and pharyngeal phases of swallowing , for which many authors suggest it is the reference standard [ 1216 ] , but also to the oesophageal phase , showing good sensitivity ( 70%90% ) in the identification of oesophageal motility disorders and gord and in the overall evaluation of the lower oesophageal sphincter [ 8 , 10 , 11 ]  . nonetheless , vfg is unable to identify the early signs of oesophagitis , which instead can be detected with endoscopy in 33%66% of patients [ 36 , 9 ]  . 
our study , therefore , was aimed at identifying primary alterations of the oral and pharyngeal phases and the overall evaluation of the oesophageal phase with the use of a variety of techniques . thanks to vfg , in all patients , we observed no signs indicating primary alterations of the swallowing mechanism and noted that both the oral and pharyngeal phases appeared morphologically and dynamically valid . 
this consideration was confirmed by direct radiological findings , such as positive wst , with identification of gord extending to the pharyngealoesophageal junction , and indirect signs such as hypertrophy of the lingual tonsil and the palatine tonsils [ 18 , 19 ]  . further confirmation was provided by laryngoscopy , ph monitoring and endoscopy . 
in addition , the vfg swallow study with direct fluorographic acquisitions investigated the morphology and function of the oesophageal phase , making possible the reliable evaluation of kinetic alterations and therefore the transit time of the barium bolus within the oesophagus in the different patient positions . 
the latter is crucial , because a progressive increase in transit time is directly correlated with a loss of physiological oesophageal kinesis and therefore with the progression of fibrosis , which is pathognomonic of the disease . 
in addition , vfg enabled evaluation of the incidence of concomitant diseases associated with ssc , such as hiatus hernia and gord , thus garantire lidentificazione e la valutazione delle alterazioni sia del tratto oro - farigeo , per il quale metodica di riferimento secondo molti autori [ 1216 ] , sia per il tratto faringo - esofageo - cardiale , con buona sensibilit , che si attesta tra 70%90% , nellidentificazione delle dismotilit esofagee e del gerd e nella valutazione complessiva della giunzione esofago gastrica [ 8 , 10 , 11 ]  . 
la vfg , tuttavia , non consente di evidenziare i segni precoci di esofagite , invece riscontrabili con lesame endoscopico nel 33%66% dei pazienti [ 36 , 9 ]  . 
il nostro studio , pertanto , stato mirato allidentificazione delle alterazioni primitive del tratto oro - faringeo ed alla valutazione complessiva del tratto farigo - esofageo - cardiale mediante lutilizzo di diverse metodiche . 
grazie alla vfg abbiamo costatato come in nessuno dei pazienti presi in esame vi sono segni riconducibili ad alterazioni primitive del meccanismo deglutitorio e come , sia la fase orale sia la fase faringea , nei loro diversi momenti , si presentino morfologicamente e dinamicamente valide . 
lidentificazione di un deficit del ribaltamento dellepiglottide , unica alterazione repertata , nel 57 , 8% dei pazienti , con conseguente penetrazione del mdc in sede subepiglottica risulta essere secondaria , infatti , ad insulto cronico da gerd . tale considerazione confermata da rilievi radiografici diretti , quali la positivit al wst con identificazione di gerd ad estensione sino alla giunzione faringo - esofagea , ed indiretti , lipertrofia della tonsilla linguale e delle tonsille palatine [ 18 , 19 ]  . 
inoltre lindagine videfluorografica , grazie allultilizzo di acquisizioni dirette in grafia ha indagato la morfologia e la funzionalit del tratto faringo - esofageo - cardiale permettendo cos la corretta ed affidabile valutazione delle alterazioni della cinetica e , quindi anche del tempo di transito del bolo baritato nel contesto del viscere esofageo nei diversi decubiti . 
inoltre la vfg ha permesso di valutare lincidenza di patologie concomitanti , associate al quadro di sclerosi sistemica , quali ernia jatale e gerd , costatando come vi sia unassociazione tra ipoe aperistalsi esofagea ed aumento del numero degli episodi di reflusso , che , secondo le recenti evidenze della letteratura , potrebbero non essere direttamente correlati alla pressione vigente in corrispondenza les [ 7 ]  . 
le verifiche gastroscopiche e phmetriche , come indagini di riferimento non radiologiche , hanno confermato ulteriormente lelevata affidabilit ( > 80% ) della metodica nellidentificazione e valutazione 958 radiol med ( 2009 ) 114 : 948959 that there demonstrating is an association between oesophageal hypo / aperistalsis and an increase in the number of reflux episodes , which may be directly correlated with the pressure of the lower oesophageal sphincter [ 7 ]  . 
this suggests that reflux is due to a reduction in clearing mechanisms more than the pressure of the lower oesophageal sphincter . gastroscopy and ph monitoring , as nonradiological reference techniques , further confirmed the high reliability ( > 80% ) of the technique in the identification and evaluation of both gord and hiatus hernia , reliability that has been emphasised several times in the recent literature . 
those values , however , are significantly lower in the identification of oesophagitis , the diagnosis of which is the exclusive realm of endoscopy . conclusions our study has shown that in patients affected by scleroderma with a subjective history of dysphagia , there is no primary deficit in the oral or pharyngeal phase of swallowing , in that no significant morphological and / or functional alterations can be appreciated , in either the preparatory or the transit phase of swallowing . 
in addition , our study population showed no compensatory mechanisms or manoeuvres , either in the oral or pharyngeal phase , events that instead are very common in the setting of primary swallowing alterations [ 20 ]  . 
therefore , our findings show that the alterations of epiglottal tilting associated with intraswallowing laryngeal penetration of high - density barium are secondary to chronic gord extending to the pharyngealoesophageal junction [ 18 ]  . 
this event is confirmed , on the one hand , by the identification in 40% of the study population of nonspecific hypertrophy of the lingual tonsil and / or palatine tonsils , which in adult subjects is an indirect sign of chronic pharyngeal inflammation [ 19 ] and , on the other , by the visualisation of gord in 97% of patients , which in 40% extended to the pharyngeal - oesophageal junction . 
our study also confirmed that vfg is a reliable modality for dynamic evaluation of both dynamic and morphological evaluation of the mechanisms and different phases underlying the swallowing reflex and is therefore able to demonstrate the presence of pathological conditions that can cause dysphagia . 
we can therefore conclude by emphasising that in patients with scleroderma , a systematic study of the oropharyngeal phase of swallowing with vfg is useful given the broad range of information that can be easily obtained with only a slight increase in radiation dose . 
moreover , we confirmed that vfg is a valid modality in the overall study of the oesophagus , although limitations to the technique remain , especially with regard to identification of superficial lesions of the oesophageal mucosa , the evaluation of which is the exclusive realm of endoscopy . sia del reflusso gastro - esofageo sia dellernia jatale , pi volte sottolineata nella recente letteratura , mentre tali valori si riducono drasticamente nellidentificazione delle esofagiti essendo la diagnosi di pertinenza esclusivamente endoscopica . 
 conclusioni il nostro studio ha evidenziato come , in pazienti affetti da sclerodermia che riferiscono anamnesticamente disfagia soggettiva , non vi alcun deficit primitivo della fase orale o faringea della deglutizione , in quanto non sono apprezzabili significative alterazioni morfologiche e / o funzionali sia nella fase preparatoria sia nella fase esecutiva del suddetto meccanismo . 
inoltre , nella nostra popolazione di studio , non stato osservato alcun meccanismo o atteggiamento compensatorio sia durante la fase orale si durante la fase faringea , eventi invece molto frequenti in corso di alterazioni primitive della deglutizione [ 20 ]  . quindi dai nostri dati si evince come le alterazioni del ribaltamento dellepiglottide ( tilting ) associate a fenomeni di penetrazione subepiglottica intradeglutitoria , del mdc baritato ad alta densit , sono secondarie ad insulto cronico da gerd ad estensione faringo - esofagea [ 18 ]  . tale evento confermato dallidentificazione , nel 40% dei pazienti in esame , di unipertrofia aspecifica della tonsilla linguale e / o delle tonsille palatine che , in soggetti adulti , segno indiretto di flogosi cronica faringea [ 19 ] e dalla visualizzazione nel 97% dei pazienti di gerd che nel 40% presentava unestensione sino alla giunzione faringoesofagea . 
il nostro studio , ha confermato , inoltre , come la videofluorografia rappresenta una metodica affidabile sia nella valutazione dinamica sia morfologica dei meccanismi e delle diverse fasi che sottendono al riflesso deglutitorio , permettendo leventuale dimostrazione dei quadri patologici che possono causare disfagia . 
inoltre lo studio da noi effettuato ha ulteriormente confermato come la metodica si dimostri altamente attendibile nella valutazione ed identificazione dei quadri patologici coinvolgenti anche il tratto faringo - esofageo - cardiale . 
quindi possiamo concludere sottolineando come , nei pazienti affetti da sclerodermia , sia utile effettuare , sistematicamente , anche lo studio della fase oro - faringea della deglutitizione , mediante vfg , in relazione alle molteplici informazioni e rilievi facilmente ottenibili , a fronte di un modesto incremento della dose radiogena somministrata al paziente . 
inoltre si conferma come la vfg rappresenti una valida metodica nello studio globale dellesofago pur permanendo i limiti della stessa , soprattutto , nellidentificazione delle lesioni superficiali della mucosa esofagea la cui valutazione permane di esclusiva pertinenza endoscopica . 
giaccone , via del vespro 127 , 90127 palermo , italy 2department of radiology , university of verona , italy 3department of cardiology , san gennaro hospital , naples , italy 4department of radiology and cardiology , university hospital , parma , italy 5department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands correspondence to : l . 
a total of 277 patients ( mean age 6011 years ) we consecutively examined with 64 - slice msct - ca for suspected or known coronary atherosclerosis were retrospectively reviewed for myocardial bridging . 
bridges were of variable length ( < 1 cm 58% ; 12 cm 32% ; > 2 cm 10% ) and depth ( superficial 69% , intramyocardial 31% ) and frequently localised in the mid - distal segment of the left anterior descending artery ( 95% )  . 
coronary segments proximal to the bridge showed no atherosclerotic disease ( 33% ) , positive remodelling ( 27% ) , < 50% stenosis ( 20% ) or > 50% stenosis ( 20% )  . 
in una popolazione di 277 pazienti ( et media 6011 ) , sottoposti consecutivamente ad ac - tcms con scanner a 64 - strati per malattia aterosclerotica coronarica sospetta o nota , stata ricercata la presenza di decorsi miocardici . 
ottantadue pazienti ( 30% , et media 5912 ) presentano decorso miocardico superficiale ( 69% ) o intramiocardico ( 31% ) , con lunghezza variabile ( < 1 cm : 58% ; 12 cm : 32% ; > 2 cm : 10% ) , frequentemente localizzato nel tratto medio - distale dellarteria coronaria discendente anteriore ( 95% )  . 
msct - ca is a reliable , noninvasive method that is able to depict myocardial bridging and associated atherosclerotic plaque in the proximal segments . keywords myocardial bridging coronary artery disease coronary angiography multislice computed tomography . > 50% ( 20% )  . 
la ac - tcms una metodica non invasiva efficace nel dimostrare i ponti miocardici e le placche aterosclerotiche associate presenti nei segmenti prossimali . parole chiave ponte miocardico coronaropatia aterosclerotica angiografia coronarica tomografia computerizzata multistrato introduction introduzione myocardial bridging is considered a congenital anomaly of the coronary arteries in which a segment of a major epicardial coronary artery courses intramurally through the myocardium beneath a muscle bridge [ 13 ]  . 
it is characterised by systolic compression of the intramyocardial segment and may cause angina , myocardial infarction , left ventricular dysfunction , paroxysmal atrioventricular block ( pavb ) , ischaemia during exertion and sudden death by cardiac arrest [ 13 ]  . 
the segment proximal to the bridge is more prone to formation of atherosclerotic plaque , whereas the intramyocardial segment is typically spared [ 3 ]  . the gold standard for diagnosing myocardial bridging is conventional coronary angiography ( cca ) , which shows characteristic compression of the intramyocardial segment on systolic angiograms . 
new imaging techniques have recently been used , such as intravascular ultrasound ( ivus ) , intracoronary doppler ( icd ) and noninvasive multislice computed tomography coronary angiography ( msct - ca ) [ 413 ]  . 
recent studies with 16and 64 - slice msct - ca have shown that myocardial bridging can be identified in a noninvasive manner , thanks to the techniques multiplanar capabilities and the flexibility of postprocessing tools , demonstrating a higher prevalence than reported in cca series [ 614 ]  . the purpose of our study was to retrospectively assess the prevalence of myocardial bridging and its association with coronary atherosclerosis in a large population of consecutive patients examined with 64 - slice msct - ca . il ponte miocardico considerato unanomalia congenita delle arterie coronarie nella quale un tratto di coronaria epicardica maggiore assume un decorso intramurale allinterno del miocardio al di sotto del ponte muscolare [ 13 ]  . 
 caratterizzato dalla compressione sistolica del segmento intramiocardico e pu causare angina , infarto del miocardio , disfunzione del ventricolo sinistro , blocco atrioventricolare ( bav ) parossistico , oltre che ischemia da sforzo e morte cardiaca improvvisa [ 13 ]  . 
tuttavia , il ponte miocardico asintomatico nella maggior parte dei casi . laterosclerosi coronarica associata con la presenza di ponti miocardici stata studiata principalmente nellarteria discendente anteriore ( ada )  . 
il segmento prossimale al ponte predisposto alla formazione di placche aterosclerotiche , mentre il segmento intramiocardico tipicamente risparmiato [ 3 ]  . il gold standard attuale per la diagnosi dei ponti miocardici langiografia coronarica convenzionale ( acc ) , che mostra la caratteristica compressione del tratto intramiocardico nellangiogramma sistolico . 
nuove tecniche di imaging sono state recentemente impiegate , quali lecografia intravascolare ( ivus ) , il doppler intracoronarico ( icd ) , e langiografia coronarica non invasiva mediante tomografia computerizzata ( tc ) multistrato ( ac - tcms ) [ 413 ]  . 
studi recenti con ac - tcms a 16 e 64 strati hanno dimostrato che i ponti miocardici possono essere non invasivamente individuati in virt della multiplanariet della metodica e della flessibilit dei mezzi di post - processing , con prevalenza pi elevata rispetto alle casistiche di acc [ 614 ]  . scopo del nostro studio quello di valutare retrospettivamente in una ampia popolazione consecutiva di pazienti sottoposti ad ac - tcms a 64 strati la prevalenza dei ponti miocardici e la loro associazione con laterosclerosi coronarica . 1026 materials and methods population radiol med ( 2009 ) 114 : 10241036 materiali e metodi popolazione a total of 277 consecutive patients ( 209 men , mean age 6011 years ) who had undergone 64 - slice msct - ca between 27 february 2007 and 30 march 2008 at our department were retrospectively reviewed to determine the prevalence of myocardial bridging . 
msct - ca had been performed for the following indications : atypical angina ( n = 107 ) , typical angina with a nonconclusive stress test ( n = 29 ) , high risk of major coronary events ( n = 63 ) , followup of proximal stents ( n = 36 ) and aortocoronary bypass grafts ( n = 25 ) , and evaluation of aneurysms of the ascending aorta ( n = 17 ) ( table 1 )  . 
the study protocol received the approval of the ethics committee . duecentosettantasette pazienti consecutivi ( 209 uomini , et media 6011 ) , sottoposti ad ac - tcms a 64 strati tra il 27 / 02 / 2007 ed il 30 / 03 / 2008 nel nostro dipartimento , sono stati valutati retrospettivamente per determinare la prevalenza dei ponti miocardici . 
i pazienti erano stati sottoposti ad ac - tcms con le seguenti indicazioni : angina atipica ( n = 107 ) , angina tipica con stress test non conclusivo ( n = 29 ) , alto rischio di eventi coronarici maggiori ( n = 63 ) , follow - up di stent prossimali ( n = 36 ) e by - pass aorto - coronarici ( n = 25 ) , e valutazione di aneurismi dellaorta ascendente ( n = 17 ) ( tabella 1 )  . 
il comitato etico ha approvato il protocollo di studio . scanning and reconstruction parameters parametri di scansione e ricostruzione all studies were carried out using a 64 - slice ct scanner ( brilliance 64 , philips medical systems , cleveland , oh , usa ) with the following parameters : slices / collimation 64 / 0.6 mm , rotation time 420 ms , effective temporal resolution ( with 180 algorithm ) 210 ms , 120 kv , 8001 , 040 mas , table speed 11.9 mm / s , effective slice thickness 0.8 mm , reconstruction increment 0.4 mm , submillimeter isotropic voxel , field of view 140240 mm ( extended cranially for evaluation of aortocoronary bypass grafts and ascending aorta aneurysms only )  . patients with heart rate > 65 bpm received 2040 mg of propranolol hydrochloride per os ( inderal , astrazeneca reims , reims , cedex , france ) 1 h before the scan . 
the patients information sheets recommended treatment with 2040 mg twice daily under medical supervision during the 3 days preceding the examination to reduce and regulate heart rate in patients with anxiety - related tachycardia . 
all patients were also administered 2.5 mg of diazepam ( tranquirit , aventis pharma , waterford , ireland ) 1 h prior to the scan . a 100to 120 - ml bolus of nonionic iodinated contrast agent ( iomeprol , iomeron 400 , bracco , milan , italy ) , depending on scan range , was injected at a flow rate of 5 ml / s using an automatic injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an 18 - gauge needle - cannula inserted into a right antecubital ve in order to optimise intraluminal enhancement of the coronary arteries , the beginning of the scan was synchronised with the passage of the contrast bolus by using the bolus tracking technique with a region of interest ( roi ) in the ascending aorta . 
nella nota informativa preliminare di preparazione allesame era stato consigliato un trattamento con 2040 mg due volte al giorno sotto controllo medico nei tre giorni precedenti lindagine per ridurre e regolarizzare la frequenza cardiaca nei pazienti con tachicardia su base ansiosa . 
allintera popolazione stata , altres , somministrata una dose di 2 , 5 mg di diazepam ( tranquirit , aventis pharma , waterford , irlanda ) unora prima della scansione . un bolo di 100120 ml di contrasto iodato non - ionico ( iomeprol , iomeron 400 , bracco , milano , italia ) , a seconda del range di scansione , stato iniettato con un flusso di 5 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 18 gauge , posizionata in una vena antecubitale destra . 
all data were analysed with postprocessing tools such as multiplanar reconstructions ( mpr ) , curved mpr ( cmpr ) , maximum intensity projection ( mip ) and volume rendering ( vr ) to visualise possible myocardial 1027 regione di interesse ( roi ) posizionata al livello dellaorta ascendente . 
il tempo di scansione risultante stato di 13 , 21 , 8 s ( range 11 , 720 , 1 s )  . i dati sono stati ricostruiti con tecnica retrospettiva alla fine della fase diastolica ( dal 65% all80% dellintervallo rr ) o alla fine della fase sistolica ( 40%45% ) per una migliore visualizzazione dellarteria coronaria destra ( acd )  . analisi delle immagini e dei dati gli esami ac - tcms sono stati revisionati da due radiologi con esperienza in tc coronarica [ 15 ] , che hanno caricato i set di dati in una workstation dedicata ( extended brilliance tm workspace , version 3.0.1.3200 , philips medical systems , cleveland , ohio , usa )  . 
tutti i dati sono stati analizzati mediante mezzi di post - processing quali ricostruzioni multiplanari ( mpr ) , mpr curve ( cmpr ) , proiezioni di massima intensit ( mip ) , e volume rendering ( vr ) per visualizzare i ponti miocardici e le placche aterosclerotiche eventualmente presenti . 
i segmenti sono stati classificati secondo lo schema dellamerican heart association ( aha )  . la prevalenza , la lunghezza ( < 1 cm , 12 cm , > 2 cm ) , e la localizzazione dei ponti miocardici sono state determinate . la profondit stata definita come superficiale o intramiocardica in base alla deviazione dei vasi nel miocardio . 
 stata , altres , valutata la presenza di placche aterosclerotiche ( no aterosclerosi , rimodellamento positivo , stenosi < 50% , stenosi > 50% ) nei segmenti prossimali e distali al ponte [ 16 ]  . 
sono state valutate anche eventuali lesioni aterosclerotiche nel tronco comune ( tcm ) , nella ada , nei rami diagonali , nella arteria circonflessa ( cx ) , nei rami marginali , nella acd e nel ramo intermedio ( ri ) , quando presente . la valutazione statistica stata eseguita con software dedicato ( spss 10 : 1 ; spss , chicago , iii )  . 
il test del chi - quadrato stato eseguito per verificare la differenza statistica riguardo alla presenza della aterosclerosi coronarica rispetto ai decorsi miocardici in rapporto alla sintomatologia ( dolore tipico o atipico )  . 
il test del chi - quadrato stato impiegato , anche , per analizzare la differenza statistica riguardo alla distribuzione dellaterosclerosi tra i segmenti prossimali e distali dei ponti miocardici , ed i restanti vasi coronarici . 
una p < 0 , 0001 stata considerata statisticamente significativa . il cramers v test stato impiegato per valutare la correlazione tra i segmenti prossimale e distale al ponte rispetto al grado di aterosclerosi . 
the prevalence , length ( < 1 cm , 12 cm , > 2 cm ) and location of myocardial bridges were determined . depth was defined as superficial or intramyocardial based on the vessels deviation in the myocardiuthe presence of atherosclerotic plaque was also assessed ( absence of atherosclerosis , positive remodelling , < 50% stenosis , > 50% stenosis ) in the segments proximal and distal to the bridging [ 16 ]  . 
any atherosclerotic lesions in the left main trunk ( lm ) , lad , diagonal branches , circumflex artery ( cx ) , marginal branches , rca and in the intermediate branch ( ib ) , if present , were also assessed . statistical analysis was performed using dedicated software ( spss 10 : 1 ; spss , chicago , il , usa )  . 
the chi - square test was used to verify statistical differences between the presence of coronary atherosclerosis and myocardial bridging in relation to symptoms ( typical or atypical pain )  . 
the chi - square test was also used to analyse the statistical difference , with reference to the distribution of atherosclerosis , between the proximal and distal segments of myocardial bridging and the remaining coronary vessels . 
the test was also used to assess the potential relationship between the segment proximal to the bridge and the other coronary vessels in relation to the degree of atherosclerosis . results single ( 90% ) or multiple ( 10% ) myocardial bridges of variable length ( < 1 cm in 58% , 12 cm in 32% and > 2 cm in 10% of cases ) were identified in 82 patients ( 30% , 56 men , mean age 6010 years , average heart rate 629 bpm ; table 1 )  . 
bridges were either superficial ( n = 63 , 69% ) without vessel deviation inside the myocardium or intramyocardial ( n = 28 , 31% ) with u - shaped deviation myocardiu bridges were frequently localised in the middistal segment of the lad ( n = 86 , 95% )  . 
sono stati individuati ponti superficiali ( n = 63 , 69% ) , senza deviazioni del vaso allinterno del miocardio , o intramiocardici ( n = 28 , 31% ) , con deviazioni a u nel miocardio . 
i ponti risultano frequentemente localizzati nel segmento medio - distale della ada ( n = 86 , 95% )  . conformemente allo schema aha , i ponti presentano la seguente distribuzione : segmento 7 , 40 casi ; segmento 8 , 32 casi ; segmenti 78 , 13 casi ; segmenti 67 , 1 caso ; segmento 9 , 1 caso ; segmento 11 , 1 casi ; segmento 14 , 1 caso ; segmento 16 , 2 casi . il ponte miocardico non rappresenta un fattore di rischio rilevante per laterosclerosi coronarica nella nostra popolazione ( or 0 , 49 per aterosclerosi coronarica ; or 0 , 47 per presenza di stenosi > 50% ) rispetto ai tradizionali fattori di rischio cardiovascolari ( colesterolemia : or 2 , 04 per aterosclerosi coronarica , or 1 , 25 per presenza di stenosi > 50% ; diabete : or 1 , 18 per aterosclerosi coronarica , or 1 , 17 per presenza di stenosi > 50% ; ipertensione : or 2 , 51 per aterosclerosi coronarica , or 0 , 64 per presenza di stenosi > 50% ; storia familiare : or 1 , 06 per aterosclerosi coronarica , or 1 , 17 per presenza di stenosi > 50% ; fumo : or 1 , 39 per aterosclerosi coronarica , or 1 , 4 per presenza di stenosi > 50% ; obesit : or 1 , 12 per aterosclerosi coronarica , or 0 , 79 per presenza di stenosi > 50% )  . 
tuttavia , solamente nel 29% dei pazienti con dolore atipico ( n = 11 ) o tipico ( n = 2 ) la ac - tcms ha identificato stenosi > 50% ( p < 0 , 05 rispetto alla popolazione che non presenta ponti miocardici )  . 
in seven patients with atypical ( n = 6 ) or typical ( n = 1 ) pain , msct - ca evidence of myocardial bridging without > 50% stenosis and stress electrocardiogram ( ecg ) evidence of nonspecific signs of ischaemia or rhythm alterations , myocardial bridging was considered clinically symptomatic , and drug therapy with - blockers was initiated . considering subjects with myocardial bridging , the coronary artery segments proximal to the bridge showed the following pattern of atherosclerosis : no sign of disease ( n = 30 , 33% ) , positive remodelling ( n = 25 , 27% ) , < 50% stenosis ( n = 18 , 20% ) and > 50% stenosis ( n = 18 , 20% ) ( table 2 )  . 
six noncalcified ( 46% ) , six mixed ( 46% ) and one calcified ( 8% ) atherosclerotic plaque were identified in the distal segments . the degree of atherosclerosis was also determined in the main coronary vessels : rca , lm , lad , diagonal branches , cx , marginal branches and ib ( found in 29% of the population )  . 
a moderate correlation ( cramers v = 0.52 ) was identified between segments proximal or distal to the bridge and the degree of atherosclerosis ( table 2 )  . discussion in 1737 , reyman first described a peculiar congenital coronary anomaly in which myocardial fibres are arranged to cover segments of a major coronary artery . 
myocardial bridging may be characterised by systolic compression of the intramymiocardico , i segmenti di coronaria prossimale al ponte presentano il seguente pattern aterosclerotico : nessun segno di malattia ( n = 30 , 33% ) , rimodellamento positivo ( n = 25 , 27% ) , stenosi < 50% ( n = 18 , 20% ) , stenosi > 50% ( n = 18 , 20% ) ( tabella 2 )  . 
nei segmenti distali sono state individuate 6 placche aterosclerotiche non calcifiche ( 46% ) , 6 miste ( 46% ) , e 1 calcifica ( 8% )  . lestensione dellaterosclerosi stata , anche , determinata nei principali vasi coronarici : acd , tcm , ada , rami diagonali , cx , rami marginali e ri ( presente nel 29% della popolazione )  . 
 stata riscontrata una discreta correlazione ( cramers v = 0 , 52 ) tra segmento prossimale o distale al ponte e grado di malattia aterosclerotica presente ( tabella 2 )  . discussione reyman descrisse nel 1737 per la prima volta una particolare anomalia congenita coronarica , nella quale le fibre miocardiche si dispongono a ricoprire tratti di unarteria coronaria maggiore . 
in un ponte superficiale ( o incompleto ) , il segmento non completamente ricoperto dalle fibre miocardiche , ma da un sottile strato di tessuto connettivo , nervi e tessuto adiposo [ 17 ]  . esiste una discrepanza tra la bassa prevalenza ( < 5% ) riportata dopo acc e la elevata prevalenza riportata negli studi autoptici ( 5%86% )  . 
in soggetti con coronarie angiograficamente normali , luso di test di provocazione pu aumentare la compressione sistolica del miocardio nel 40% dei casi [ 1 , 3 ]  . inoltre , la presenza di una lesione stenotica prossimale pu impedire la visualizzazione del successivo ponte . 
in a superficial ( or incomplete ) bridge , the segment is not completely covered by myocardial fibres but by a thin layer of connective tissue , nerves and fat tissue [ 17 ]  . there is some discrepancy between the low prevalence ( < 5% ) reported after cca and the high prevalence reported in post - mortem studies ( 5%86% )  . 
the lower depiction rate of angiography may , instead , be attributed to the prevalence of superficial bridges causing minimal compression undetectable by cca [ 1 , 3 ]  . 
a high prevalence of bridging has been reported in patients with hypertrophic obstructive cardiomyopathy [ 18 ]  . myocardial bridges may cause angina , myocardial infarction , left ventricular dysfunction , paroxysmal avb , prevalenza riportata nei pazienti con cardiopatia ipertrofica ostruttiva [ 18 ]  . i ponti miocardici possono causare angina , infarto del miocardio , disfunzione ventricolare sinistra , bav parossistico , ischemia da sforzo e morte cardiaca improvvisa . 
i pazienti possono presentarsi con dolore toracico atipico o equivalenti anginosi , senza una consistente associazione tra severit dei sintomi e lunghezza , profondit o grado di compressione sistolica del ponte [ 17 ]  . mentre i ponti miocardici brevi e superficiali sono sovente asintomatici e non richiedono intervento di alcun tipo , le opzioni di gestione per i ponti miocardici sintomatici possono essere farmacologiche ( - bloccanti e calcio - antagonisti ) o interventistiche ( stenting , bypass grafting e miotomia chirurgica ) in relazione alla profondit ed alla lunghezza del decorso [ 20 ]  . i ponti miocardici sono ritenuti una delle principali cause di infarto miocardico in circa il 6% dei pazienti che non presentano evidenza di aterosclerosi coronarica n alla acc , n alla autopsia [ 21 ]  . 
il ponte miocardico , invece , un evento sistolico alla acc , per cui la sua rilevanza radiol med ( 2009 ) 114 : 10241036 1031 ischaemia during exertion and sudden death by cardiac arrest . 
patients may present with atypical chest pain or anginal equivalents without any consistent association between the severity of symptoms and the length , depth or degree of systolic compression of the bridge [ 17 ]  . whereas short and superficial myocardial bridges are often asymptomatic and require no intervention , management options for symptomatic myocardial bridges may be pharmacological ( - blockers and calcium antagonists ) or interventional ( stenting , bypass grafting and surgical myotomy ) , depending on the depth and length of the bridge [ 20 ]  . myocardial bridging is considered one of the main causes of myocardial infarction in approximately 6% of patients with no evidence of coronary atherosclerosis on either cca or post - mortem examinations [ 21 ]  . 
ischaemia can be attributed to a combination of the following factors : sudden tachycardia ( compromising diastolic filling of coronary arteries ) , coronary spasm and systolic kinking of the coronaries ( leading to endothelial damage with resulting platelet activation and thrombosis ) [ 2 , 22 , 23 ]  . 
haemodynamic forces may explain the formation of atherosclerotic plaque close to the intramyocardial segment where the endothelium is flat , polygonal and polymorphic , indicating low shear stress [ 24 , 25 ]  . 
furthermore , local increase in wall tension may cause damage to the endothelium and fissuring of the plaque , resulting in the formation of proximal thrombi [ 27 ]  . cca is the imaging gold standard in diagnosing myocardial bridging . 
new invasive imaging techniques , such as ivus and icd , can be used to demonstrate the morphological and functional features of myocardial bridging [ 4 , 5 ]  . 
ivus studies support the absence of atherosclerosis in intramyocardial vessels , although at least 90% of patients show formation of atheromatous plaque in proximal tracts [ 4 ]  . few studies have investigated the feasibility of msct - ca for visualising myocardial bridging [ 614 ]  . 
the incidence ed il suo significato clinico sono stati messi in dubbio . lischemia pu essere attribuita alla combinazione dei seguenti fattori : improvvisa tachicardia ( tale da compromettere il riempimento diastolico delle coronarie ) , spasmo coronarico , kinking sistolico delle coronarie ( tale da determinare un danno endoteliale con conseguente attivazione piastrinica e trombosi ) [ 2 , 22 , 23 ]  . 
le forze emodinamiche possono spiegare la formazione di placche aterosclerotiche in prossimit del segmento intramiocardico , dove lendotelio piatto , poligonale e polimorfo , indicando la presenza di un ridotto shear stress [ 24 , 25 ]  . 
inoltre , un aumento locale della tensione di parete pu causare un danno endoteliale e la fissurazione della placca con conseguente formazione di trombi prossimali [ 27 ]  . il gold standard attuale di imaging , per la diagnosi di ponte miocardico la acc . 
nuove tecniche di imaging invasive , quali la ivus ed il icd , possono essere utilizzate per mostrare le caratteristiche morfologiche e funzionali del bridging miocardico [ 4 , 5 ]  . studi lassenza di aterosclerosi allinterno dei decorsi miocardici , sebbene almeno il 90% dei pazienti mostri la formazione di placche ateromasiche nei tratti prossimali [ 4 ]  . ivus supportano pochi studi hanno descritto la fattibilit della visualizzazione dei ponti miocardici mediante ac - tcms [ 614 ]  . lincidenza dei ponti miocardici diagnosticati con ac - tcms a 16 strati compresa tra il 3 , 5% ed il 5 , 7% [ 8 , 9 ]  . 
gli studi effettuati con tc a 64 strati riportano una prevalenza pi elevata , compresa tra il 10 , 9% ed il 44% , superiore alle casistiche angiografiche , ma non dissimile dai tassi riportati negli studi autoptici [ 1014 ]  . 
studies conducted with 64 - slice ct report a prevalence of bridging ( 10.9%44% ) that is higher than that reported for angiographic series but similar to postmortem studies [ 1014 ]  . 
the incidence of myocardial bridging ( 30% ) is consistent with that reported by post - mortem studies and higher than that found in most angiographic studies in which the low depiction rate can be attributed to superficial bridging and minimal compression . 
lincidenza dei ponti miocardici ( 30% ) in accordo con quella degli studi autoptici e pi elevata di quella riportata nella maggior parte degli studi angiografici , nei quali il basso tasso di riscontri attribuibile a decorsi superficiali responsabili di modeste compressioni . la ac - tcms offre , inoltre , diversi potenziali vantaggi . 
la prevalenza di malattia inferiore nella popolazione con ponte miocardico rispetto a quella che non presenta tale condizione anatomica ( aterosclerosi coronarica rilevata 78% vs 87% , stenosi > 50% 41% vs 60% , p < 0 , 05 )  . 
1a - d superficial myocardial bridging ( arrow ) of the middistal tract of the left anterior descending artery on vr ( a ) , mpr ( b ) and stretched - vessel mpr images ( c )  . 
1a - d ponte miocardico superficiale ( freccia ) del tratto medio - distale della arteria discendente anteriore mediante immagini vr ( a ) , mpr ( b ) , e stretch - vessel mpr ( c )  . 
decorso miocardico ( testa di freccia ) del tratto prossimale del primo ramo marginale mediante stretch - vessel mpr ( d )  . radiol med ( 2009 ) 114 : 10241036 1033 fig . 
2a - c superficial myocardial bridging ( white arrow ) of the mid - distal tract of the left anterior descending artery and intramyocardial course ( arrowhead ) of the first diagonal branch ( d1 ) : vr ( a ) and mpr ( b , c ) images . 
2a - c ponte miocardico superficiale ( freccia bianca ) del tratto medio - distale dellarteria discendente anteriore e decorso intramiocardico ( testa di freccia ) del primo ramo diagonale ( d1 ) : immagini vr ( a ) ed mpr ( b , c )  . 
with regard to the association with coronary atherosclerosis , and in agreement with the literature [ 1 , 35 , 9 , 2427 ] , the segments proximal to myocardial bridges show a distinctly different atherosclerotic pattern from that of the distal segments . 
in riferimento alla associazione con la aterosclerosi coronarica ed in accordo con la letteratura [ 1 , 35 , 9 , 2427 ] , i segmenti prossimali ai ponti miocardici presentano un pattern aterosclerotico significativamente differente rispetto ai segmenti distali . 
la actcms non invasiva stata , infatti , spesso eseguita nel tentativo di non sottoporre i pazienti alla diagnostica invasiva con acc , in virt dellalto valore predittivo della metodica [ 28 ]  . 
a tal proposito , scanner con pi elevata risoluzione temporale potrebbero fornire precise indicazioni circa la compressione sistolica [ 29 ]  . 1034 radiol med ( 2009 ) 114 : 10241036 fig . 
3a - f myocardial bridging ( arrow ) of the middle tract of the left anterior descending artery shown on vr ( a , d ) , mpr ( b ) and stretched - vessel mpr images ( c ) in a patient with atypical chest panonsignificant noncalcified plaque can be seen proximal to the myocardial bridging ( arrowhead )  . 
3a - f ponte miocardico ( freccia ) del tratto medio della arteria discendente anteriore visualizzato mediante immagini vr ( a , d ) , mpr ( b ) e stretch - vessel mpr ( c ) in paziente con dolore toracico atipico . 
angiografia coronarica convenzionale del ponte miocardico in fase telediastolica ( e ) e telesistolica ( f )  . diastolic images may enable evaluation of temporary luminal restriction in the myocardial segments [ 13 ]  . 
in this respect , scanners allowing higher temporal resolution may provide an accurate indication of systolic compression [ 29 ]  . finally , our study population reflects a selection bias , as a suspicion of coronary atherosclerosis and related clinical symptoms were the main reasons for the msct - ca examinations . 
despite the above limitations , msct - ca is defined as a reliable method for coronary imaging and an excellent tool for describing detected anomalies [ 30 ]  . infine , la popolazione del nostro studio presenta un bias di selezione poich il sospetto di aterosclerosi coronarica e la correlata sintomatologia clinica rappresentano il motivo principale dellesecuzione dellindagine ac - tcms . 
nonostante tali limitazioni , la ac - tcms definita attualmente come una metodica affidabile per limaging coronarico ed uno strumento eccellente per la descrizione di eventuali anomalie [ 30 ]  . conclusioni conclusions radiologists have the opportunity to assess myocardial i radiologi hanno la concreta opportunit di valutare la presenza dei ponti miocardici in vivo , grazie ai vantaggi della tecnologia tcms , quali lalta risoluzione spaziale e radiol med ( 2009 ) 114 : 10241036 1035 fig . 
4a - f decorso intramiocardico ( freccia ) del tratto medio della arteria discendente anteriore con associata placca non calcifica eccentrica prossimale che determina stenosi significativa ( testa di freccia ) : immagini vr ( a ) , mpr ( b ) , stretch - vessel mpr ( c ) , mip ( d ) , e sezioni mpr in corrispondenza della stenosi significativa ( e ) e del decorso intramiocardico ( f )  . bridges in vivo , thanks to the advantages offered by msct technology such as high spatial resolution and postprocessing flexibility . 
a 64 - slice msct - ca can provide exhaustive information on myocardial bridging and associated proximal atherosclerotic lesions , which may support clinical management and , where necessary , interventional planning . 
la ac - tcms a 64 strati pu fornire informazioni esaurienti riguardo i ponti miocardici e le associate lesioni aterosclerotiche prossimali , che possono supportare la gestione clinica ed , eventualmente , il planning interventistico dei cardiologi . 
di rudin 8 , 20142 milano , italy 3unit di radiologia , dipartimento di scienze medico - chirurgiche , universit degli studi di milano , irccs policlinico san donato , san donato milanese , italy correspondence to : s . 
the locations of the parathyroid glands were typical cervical ( n = 77 ) , thyrothymic ligament ( n = 3 ) , carotid sheath ( n = 2 ) , and mediastinum ( n = 3 )  . 
per - patient sensitivity and positive predictive values , respectively , were 84% ( 64 / 76 ) and 99% ( 64 / 65 ) for us , 68% ( 44 / 65 ) and 100% ( 44 / 44 ) for scintigraphy and 91% ( 59 / 65 ) and 98% ( 59 / 60 ) for both techniques combined . 
la sede di tali paratiroidi ingrandite , correttamente identificata dallecografia per 74 paratiroidi in 64 pazienti , era : cervicale tipica ( n = 77 ) , legamento tireotimico ( n = 3 ) , ricorrenziale ( n = 2 ) , mediastino ( n = 3 )  . 
in due pazienti stato identificato un microadenoma intratiroideo allesame istologico . sensibilit e valore predittivo positivo , per paziente , sono risultati 84% ( 64 / 76 ) e 99% ( 64 / 65 ) per lecografia , 68% ( 44 / 65 ) e 100% ( 44 / 44 ) per la scintigrafia e 91% ( 59 / 65 ) e 98% ( 59 / 60 ) per le due metodiche combinate , rispettivamente . 
lidentificazione e la localizzazione 1160 radiol med ( 2009 ) 114 : 11591172 inexpensive and widely available method , limiting the use of scintigraphy to those cases with negative and / or doubtful findings on us . keywords parathyroid glands primary hyperparathyroidism parathyroidectomy ultrasonography preoperatoria di paratiroidi ingrandite possono basarsi sullecografia , metodica assai diffusa e con costi contenuti , limitando lutilizzo della scintigrafia ai casi negativi e / o dubbi allecografia . parole chiave paratiroidi iperparatiroidismo primario paratiroidectomia ecografia introduction introduzione primary hyperparathyroidism is a disorder characterised by an overproduction of parathormone independently of the feedback of calcium homeostasis . 
the estimated incidence of this disorder in the general population is 40 / 100 , 000 cases per year and is four to five times higher among postmenopausal women [ 13 ]  . 
however , thanks to the possibility of localising the enlarged parathyroid glands preoperatively , the use of minimally invasive procedures with shorter procedure times is becoming increasingly frequent [ 1 , 4 ]  . 
 the parathyroid glands can be localised preoperatively by using different imaging techniques , including ultrasound ( us ) , scintigraphy , computed tomography ( ct ) and magnetic resonance ( mr ) imaging . 
although scintigraphy was once the most widely used preoperative localising technique , recent advances in us , including high - frequency probes and colour doppler and power doppler , have increased the diagnostic performance of us to levels comparable with those of scintigraphy , with clear benefits in terms of greater speed and reduced cost and dose [ 1 , 57 ]  . the purpose of our study was to retrospectively evaluate the diagnostic capabilities of preoperative us in patients with primary hyperparathyroidism by correlating and comparing the results with the surgical and histological findings . materials and methods this retrospective study received the approval of our ethics committee , which authorised the anonymous publication of the data even in the absence of individual patients informed consent . 
attualmente , grazie anche alla possibilit di identificare preoperatoriamente la sede delle paratiroidi ingrandite , sempre pi frequente lesecuzione di interventi mini - invasivi , con riduzione dei tempi dintervento [ 1 , 4 ]  . 
pi di recente i progressi della tecnica ecografica , con lutilizzo di sonde ad alta frequenza e la possibilit di avvalersi di color doppler e power doppler , la capacit diagnostica dellecografia equiparabile a quella della scintigrafia con indubbi vantaggi in termini di rapidit di esecuzione , e risparmio economico e dosimetrico [ 1 , 57 ]  . rendono scopo del nostro studio stato valutare retrospettivamente la capacit diagnostica dellecografia preoperatoria in pazienti affetti da iperparatiroidismo primario , rispetto ai reperti chirurgici e allesame istologico . materiali e metodi il presente studio retrospettivo stato autorizzato dal comitato etico , consentendo la pubblicazione dei dati in forma anonima anche senza disponibilit di specifico consenso informato da parte dei singoli pazienti . 
 popolazione we retrospectively reviewed patients with primary hyperparathyroidism [ increased serum parathormone ( pth ) with consequent hypercalcaemia and hypophosphataemia ] who had been operated on at the endocrine surgery department of our hospital between september 1999 and october 2006 . abbiamo valutato retrospettivamente i pazienti con iperparatiroidismo primario ( livelli ematici aumentati di paratormone [ pth ] con conseguente ipercalcemia ed ipoil reparto di chirurgia fosfatemia ) operati presso radiol med ( 2009 ) 114 : 11591172 1161 patients in whom preoperative us had been performed at another centre or not performed at all were excluded from the study . 
thus , the finally study population included 77 patients . imaging methods all 77 patients had undergone preoperative us of the neck , and 65 had also been studied by scintigraphy . 
where possible , in relation to the patients somatic structure and to the diagnostic requirements , the upper mediastinal region immediately below the jugulum was evaluated using a micro convex high - frequency transducer ( 48 mhz )  . 
the examination was completed with an evaluation of the lateral neck regions and with colour doppler and power doppler of identified expansive masses . predominantly perilesional vascularity was considered indicative of thyroid nodules , whereas predominantly intralesional vascularity indicated enlarged parathyroid glands . 
in particular , we did not evaluate the lower diagnostic capabilities of us in patients with thyroid goitre [ 3 ]  . subtraction scintigraphy was performed on 84% ( 65 / 77 ) of patients with 99mtc - sestamibi ( mibi ) and 99mtc - pertechnetate . 
scintigraphic studies performed at other centres had in some cases preceded the us scan , whereas at our hospital , scintigraphy was always performed to supplement doubtful or inconclusive us scans . 
the longest time interval between us and scintigraphy was approximately 3 months , and the maximum time between diagnostic investigations and surgery was 6 months . surgery three different kinds of surgical procedures were performed : neck dissection with either unilateral ( n = 54 ) or bilateral ( n = 23 ) neck exploration and minimally invasive video - assisted neck dissection ( localised parathyroid , absence of goitre or previous neck dissection ) ( n = 1 )  . 
la popolazione in esame risultata di 77 pazienti . metodiche dimaging tutti i 77 pazienti , prima dellintervento , sono stati sottoposti ad indagine ecografica del collo , 65 anche ad indagine scintigrafica . 
lesame ecografico , per cui stata utilizzata una sonda lineare ad alta frequenza ( 7 , 510 mhz ) , stato eseguito da un operatore dedicato ( 3 radiologi con pi di 10 anni di esperienza )  . 
per quanto stato possibile , in relazione alla struttura somatica del soggetto ed alla necessit diagnostica , stata valutata la regione del mediastino superiore immediatamente al di sotto del giugulo mediante lutilizzo di trasduttore microconvex ad alta frequenza ( 48 mhz )  . 
le paratiroidi ingrandite ( diametro > 4 mm ) sono state descritte come formazioni rotondeggianti ipoecogene rispetto al parenchima tiroideo , con ricca vascolarizzazione alla valutazione power doppler ; di ciascuna sono state registrate e classificate informazioni sulle dimensioni ( diametro massimo ) , il lato ( destro o sinistro ) e la sede ( superiore od inferiore )  . 
in particolare non abbiamo valutato linferiore capacit diagnostica in pazienti portatori di struma tiroideo [ 3 ]  . lesame scintigrafico , effettuato nell84% ( 65 / 77 ) dei pazienti , stato eseguito mediante tecnica di sottrazione digitale con il 99mtc - sestamibi ( mibi ) e 99mtc pertecnetato . in alcuni casi lesame scintigrafico , eseguito presso altre sedi , aveva preceduto lesame ecografico mentre presso il nostro centro la scintigrafia stata eseguita ad integrazione di ecografie dubbie o inconcludenti . 
il periodo massimo intercorso tra ecografia e scintigrafia stato di circa 3 mesi ; il periodo massimo intercorso tra indagini diagnostiche e successivo intervento chirurgico stato di 6 mesi . intervento chirurgico sono stati eseguiti tre diversi tipi di intervento : cervicotomia 1162 radiol med ( 2009 ) 114 : 11591172 according to the literature [ 2 , 8 ] , a fall in serum pth of more than 50% 10 min after parathyroidectomy compared with the level at anaesthesia induction confirms the complete removal of all hyperfunctioning parathyroid tissue and justifies the end of the surgical procedure . 
if there is no fall in serum pth , a histological examination is carried out to confirm the parathyroid nature of the resected tissue , and a further pth assay is performed . 
where the removal of multiple parathyroid glands does not lead to a fall in pth , the thyroid is partially or completely removed as a possible site of intrathyroid microadenoma . 
we considered as true positives all patients in whom us correctly detected at least one abnormal parathyroid gland ( on the right or left side of the neck )  . 
all patients with negative preoperative us and at least one pathological parathyroid at surgery and those with negative us and a surgical diagnosis of intrathyroid microadenoma were considered false negatives . 
false positives were defined as patients with a us finding of enlarged parathyroid glands not confirmed on surgery and those with incorrect us localisation of the enlarged parathyroid gland ( enlarged parathyroid gland on the right side of the neck described by us as being located on the left side or vice versa )  . 
 sensitivity and positive predictive value were then calculated for the two modalities separately and in combination and for the us and scintigraphy detection of parathyroid glands in relation to weight ( mann - whitney u test )  . comparison between the sensitivity of us and scintigraphy was based on the mcnemar test . results parathyroidectomy was performed in 77 patients 60 women ( 78% ) and 17 men ( 22% ) aged 2279 years ( table 1 )  . 
in two patients ( 3% ) , the procedure revealed no grossly enlarged parathyroid glands , and the histological diagnosis ( partial right lobectomy in one case , total thyroidectomy in the other ) was thyroid microadenoma . 
at surgery , 77 enlarged parathyroid glands were identified in the classic lateral neck position , three in the con esplorazione cervicale monolaterale ( n = 54 ) o bilaterale ( n = 23 ) e minicervicotomia videoassistita ( paratiroide localizzata , assenza di gozzo o di pregressa cervicotomia ) ( n = 1 )  . 
 in accordo con la letteratura [ 2 , 8 ] una caduta del livello serico di pth di oltre il 50% a 10 minuti dalla paratiroidectomia rispetto al valore allinduzione dellanestesia fornisce la conferma della rimozione di tutto il tessuto paratiroideo iperfunzionante e giustifica la fine dellintervento . 
in assenza di caduta del livello serico di pth si procede ad esame istologico per confermare la natura paratiroidea del tessuto asportato e ad ulteriore prelievo per il dosaggio del pth . 
se la natura paratiroidea confermata e non si ha riduzione tardiva del pth , si procede ad unulteriore paratiroidectomia ; in caso la rimozione di pi paratiroidi non si associ a discesa del pth si procede ad asportazione parziale o totale della tiroide possibile sede di microadenoma intratiroideo . in tutti i casi la natura della lesione asportata stata valutata con esame istologico . 
abbiamo considerato veri positivi tutti i pazienti con almeno una paratiroide patologica correttamente localizzata ( sede laterocervicale destra o sinistra ) allecografia ; falsi negativi i pazienti con ecografia preoperatoria negativa ed almeno una paratiroide patologica al riscontro operatorio ed i pazienti con ecografia negativa e diagnosi di microadenoma intratiroideo al riscontro operatorio . 
abbiamo considerato falsi positivi i pazienti con riscontro ecografico di paratiroidi ingrandite non confermate allintervento e quelli con errata localizzazione ecografica di paratiroide ingrandita ( paratiroide ingrandita in sede laterocervicale destra descritta a sinistra allesame ecografico o viceversa )  . 
 sono stati quindi calcolati sensibilit e valore predittivo positivo di ciascuna delle due metodiche e della loro combinazione come pure lidentificazione ecografica e scintigrafica delle paratiroidi in relazione al loro peso , per entrambe le tecniche ( test u di mann - whitney )  . 
il confronto tra la sensibilit dellecografia e quella della scintigrafia stato effettuato mediante test di mcnemar . risultati sono stati sottoposti a paratiroidectomia 77 pazienti , 60 radiol med ( 2009 ) 114 : 11591172 1163 table 1 population with primary hyperparathyroidism included in the study no . 
of patients percent of patients mean age ( years ) women total maschi femmine totale tabella 1 popolazione con iperparatiroidismo primario inclusa nello studio numero pazienti percentuale pazienti et media ( anni ) table 2 histological type and site of the removed parathyroid glands no . 
it produced 12 false negatives and incorrectly located the side of the lesion in one patient only ( correctly diagnosed by scintigraphy )  . femmine ( 78% ) e 17 maschi ( 22% ) , di et compresa tra 22 e 79 anni ( tabella 1 )  . 
in due pazienti ( 3% ) lintervento non ha evidenziato alcuna parala diagnosi tiroide macroscopicamente ingrandita e 1164 radiol med ( 2009 ) 114 : 11591172 table 3 histological characteristics of removed parathyroid glands . 
the diameter of abnormal parathyroid glands identified on us was 19.714.4 mm ; 16 mm ; 475 mm [ meanstandard deviation ( sd ) ; median ; range ]  . 
the us and scintigraphy results were concordant in 54% of patients who underwent both examinations ( 35 / 65 ) , with sensitivity and positive predictive value of 81% ( 52 / 64 ) and istologica ( lobectomia destra parziale in un caso , tiroidectomia totale nellaltro ) stata di microadenoma intratiroideo . 
allintervento chirurgico 77 paratiroidi ingrandite sono state identificate nella classica sede laterocervicale , 3 nel legamento tireotimico , 2 in sede ricorrenziale , 3 ectopiche nel mediastino superiore ( tabelle 2 e 3 )  . lecografia preoperatoria ha identificato correttamente fig . 
1a , b a 52 - year - old man with a 10 - year history of kidney stones and a 2 - year history of skeletal paus detected an enlarged left lower parathyroid gland that after removal was found to weigh 1 , 780 mg . 
il diametro delle paratiroidi anormali identificate allecografia risultato : 19 , 714 , 4 mm ; 16 mm ; 475 mm ( mediadeviazione standard ; mediana ; range )  . 
neither us nor scintigraphy detected the hypertrophic parathyroid gland at the level of the carotid sheath . we obtained the weight of 63 ( 74% ) of the 85 resected parathyroid glands . 
no weight was recorded for the following : 12 adenomatous parathyroid glands , five hyperplastic parathyroid glands , two intrathyroid microadenomas and three cases in which only fragments of the parathyroid gland were available . 
whereas in the past hyperparathyroidism tended to be detected in symptomatic patients with disorders due to hypercalcaemia ( kidney stones , fractures , neuromuscular syndrome ) , nowadays , it is increasingly discovered in asymptomatic patients . 
although medical treatment to control disease progression is an option in some cases , the only chance for cure remains surgery , which leads to a dramatic reduction of symptoms , a substantial fall in serum pth levels and normalisation of serum calcium levels [ 2 , 810 ]  . 
il confronto tra la sensibilit dellecografia e quella della scintigrafia ha mostrato un trend in favore dellecografia ( p = 0 , 134 , test di mcnemar )  . i casi in cui lecografia risultata falsamente negativa erano 9 pazienti con adenoma singolo , compresi una paratiroide in sede mediastinica e una in sede ricorrenziale ( in 6 di questi compresa la paratiroide ectopica in sede mediastinica la paratiroide patologica stata identificata con la scintigrafia ) , un paziente con adenoma duplice ( negativo anche alla scintigrafia ) e i due pazienti con microadenoma intratiroideo . delle 3 paratiroidi ectopiche intramediastiniche , tutte correttamente identificate alla scintigrafia , 2 , grazie alle dimensioni ed alla posizione subito sotto al giugulo , erano state sospettate anche allecografia . 
tutte le paratiroidi ingrandite situate nel legamento tireotimico sono state correttamente identificate , una di esse sulla base della sola ecografia in quanto il paziente non stato sottoposto ad esame scintigrafico . 
a ultrasound , axial view : symmetrical , regularly echoic thyroid gland ; on the right side , a hypoechoic intrathyroidal nodule ( arrowheads ) and an expansive hypoechoic mass ( arrow ) posterior to the thyroid lobe ( in the upper parathyroid gland site )  . 
b on the same side , a hypoechoic thyroidal nodule with peripheral vascularisation can be seen inside the thyroid gland , probably the reason why scintigraphy failed to detect the parathyroid lesion . 
a ecografia , scansione trasversale : la tiroide appare simmetrica con echi regolari ; a destra , oltre a nodulo ipoecogeno intraghiandolare ( punte di freccia ) , posteriormente al lobo ( nella sede della paratiroide superiore ) si rileva neoformazione espansiva ipoecogena ( freccia )  . 
la paziente esegue intervento chirurgico mini - invasivo con visualizzazione di ghiandola paratiroidea superiore destra aumentata di volume del peso di 300 mg ( diagnosi istologica di adenoma )  . 
3a , b a 29 - year - old woman with recurring bilateral renal colic and sudden growth of an anterior cervical mass on the left side of the neck . both scintigraphy and us confirmed the parathyroid nature of the mass . 
la diagnosi istologica stata di adenoma paratiroideo atipico del peso di 2100 mg . roidism , with hyperplasia ( 15%20% ) , multiple adenomas ( 4%5% ) and parathyroid carcinoma ( 1% ) being less frequent causes [ 2 , 9 , 11 ]  . 
the us examination does not enable even with the aid of doppler imaging the differential diagnosis between these disease entities , but it does allow recognition of the abnormal gland to be dissected [ 5 ]  . radiol med ( 2009 ) 114 : 11591172 frequente nelle donne ( 1 / 500 vs 1 / 2000 negli uomini ) , in particolare tra la quinta e la settima decade di vita [ 1 , 2 , 8 ]  . 
bench in alcuni casi si possa optare per la terapia medica e tenere sotto controllo la progressione di malattia , lunica possibilit di guarigione resta lintervento chirurgico che riduce drasticamente i sintomi e induce una caduta sostanziale dei livelli di pth e la normalizzazione della calcemia [ 2 , 810 ]  . 
 la maggior parte dei lavori in letteratura riporta come causa principale di iperparatiroidismo primario ladenoma singolo ( 80%90% dei casi ) , sono pi rari i casi di iperplasia ( 15%20% ) , di adenomi multipli ( 4%5% ) e di carcinoma paratiroideo ( 1% ) [ 2 , 9 , 11 ]  . 
la popolazione del nostro studio appare del tutto sovrapponibile con valori di circa 86% , 9% , 3% , 0% , rispettivamente ( tabella 3 )  . lesame ecografico non permette , neanche con lausilio del doppler , una diagnosi differenziale tra queste entit nosologiche , ma consente di riconoscere la ghiandola anormale su cui mirare lintervento chirurgico [ 5 ]  . lesecuzione dellintervento chirurgico in pazienti spesso asintomatici e , in cos larga misura , con lesione unica , ha posto lesigenza di interventi sempre meno invasivi . 
nel nostro studio , grazie allidentificazione della ghiandola interessata , circa il 70% dei pazienti ( 54 / 77 ) stato sottoposto ad esplorazione cervicale monolaterale , circa il 30 % ( 23 / 77 ) ad esplorazione cervicale bilaterale . 
i tempi medi di degenza e , di conseguenza , i costi sono ridotti [ 4 , 9 , 1116 ]  . in questo contesto ha assunto unimportanza sempre maggiore la corretta identificazione preoperatoria delle ghiandole patologiche . 
varie sono le tecniche di imaging capaci di identificare le paratiroidi ipertrofiche : ecografia , scintigrafia , tc , rm , tomografia computerizzata ad emissione di fotone singolo ( single photon emission computed tomography , spect )  . 
pi recentemente ad essa si affiancata lecografia , pi conveniente in termini di costi , disponibilit sul territorio , ripetitivit e dose per il paziente [ 1 , 79 , 17 , 18 ]  . 
nel nostro studio sono state prese in considerazione radiol med ( 2009 ) 114 : 11591172 1169 the use of surgery in often asymptomatic patients , most of whom have a single lesion only , has called for increasingly less invasive procedures . 
in our study , preoperative identification of the pathological gland led to unilateral neck exploration in approximately 70% of patients ( 54 / 77 ) and bilateral exploration in 30% ( 23 / 77 )  . 
unilateral transcervical access reduces operative time and morbidity by lowering transient and permanent postoperative hypocalcaemia and reducing the risk of compromising correctly functioning parathyroid glands . given that the contralateral glands are spared , the risk of permanent hypoparathyroidism is very low . 
mean hospitalisation stay is shorter and costs are reduced [ 4 , 9 , 1116 ]  . in this context , correct preoperative identification of abnormal glands has become increasingly important . several imaging techniques are able to detect hypertrophic parathyroid glands : us , scintigraphy , ct , mr imaging and single photon emission ct ( spect )  . 
more recently , us has taken on a significant role , as it is less expensive , readily available , repeatable and non - radiating [ 1 , 79 , 17 , 18 ]  . 
our study took into consideration us and scintigraphy only , as these are the techniques most commonly used by surgeons ( who consider ct , mri and spect third - line techniques to be reserved for exceptional cases )  . 
 [ 1 ] have emphasised that us sensitivity for detecting parathyroid glands , which was 34%82% in the 1980s , greatly improved beginning in the mid - 1990s , in parallel with technological developments ( highfrequency probes , colour and power doppler ) , reaching the current levels of 83%93% [ 1 , 17 , 1921 ]  . 
 the further advantages of us in addition to the abovementioned practical aspects are the possibility of detecting , measuring and characterising parathyroid lesions , which are usually solid , hypoechoic masses with welldefined margins and parenchymal vascularity . 
in cases of large neck nodules , where intraand extrathyroid formations are difficult to distinguish , the support of colour and power doppler proved useful in our experience [ 6 ]  . in our study , there was a trend in favour of us as opposed to scintigraphy in the identification of enlarged parathyroid glands and an impact of the weight of parathyroid glands on scintigraphic detection rates , confirming the usefulness of us as an initial diagnostic approach in primary hyperparathyroidis in agreement with published experiences , the sensitivity of scintigraphy alone ( 68% ) was lower than solo lecografia e la scintigrafia , essendo le tecniche pi richieste dai chirurghi ( i quali considerano tc , rm e spect tecniche di terzo livello e ne limitano la richiesta a casi eccezionali )  . 
 [ 1 ] si sottolinea come la sensibilit dellesame ecografico nella localizzazione delle paratiroidi , variabile dal 34% all82% negli anni ottanta , sia di gran lunga migliorata , di pari passo con i miglioramenti tecnologici ( sonde ad alta frequenza , utilizzo di color e power doppler ) , dalla met degli anni novanta , raggiungendo valori attorno all83%93% [ 1 , 17 , 1921 ]  . 
 vantaggi dellecografia sono sicuramente , oltre agli aspetti pratici gi elencati , la possibilit di localizzare , misurare e caratterizzare le lesioni paratiroidee ; solitamente , lesioni solide a margini ben definiti , ipoecogene , con vascolarizzazione di tipo parenchimale . 
lecografia , a differenza della scintigrafia , inoltre , consente unadeguata diagnosi differenziale con noduli tiroidei , linfonodi , residui timici , strutture vascolari [ 16 , 22 , 23 ]  . 
nel caso di lesioni nodulari voluminose a livello del collo , in cui era difficile distinguere tra formazioni intrao extratiroidee risultato utile , nella nostra esperienza , il supporto di color e power doppler [ 6 ]  . 
 nel presente studio abbiamo rilevato un trend in favore dellecografia nellidentificazione delle paratiroidi ingrandite in confronto alla scintigrafia ed uninfluenza del peso delle paratiroidi nella loro identificazione scintigrafica confermando lutilit dellecografia come prima indagine diagnostica nei casi di iperparatiroidismo primario . 
nel nostro studio , in accordo con numerosi lavori in letteratura , i valori di sensibilit del solo esame scintigrafico ( 68% ) sono inferiori a quelli della sola ecografia ( sensibilit dellesame ecografico pari a 84% considerando tutti i 77 pazienti ; 81% considerando solo i 65 pazienti sottoposti ad entrambi gli esami ) , ma raggiungono una significativit decisamente maggiore in caso di esecuzione combinata ( sensibilit di ecografia pi scintigrafia pari a 91% )  . 
il relativamente basso valore di concordanza ( 54% ) tra le due tecniche ottenuto nel nostro studio sicuramente limitato dal fatto che la maggior parte delle scintigrafie sono state eseguite su pazienti con ecografia dubbia o non conclusiva . 
the relatively low concordance ( 54% ) between the two techniques in our study is certainly dependent on the fact that most scintigraphy examinations were carried out on patients with inconclusive or doubtful us results . 
because of embryonic migration defects , in 25% of the population , the inferior parathyroid glands are located in the superior mediastinum [ 1 , 19 , 24 ]  . however , us succeeded in correctly identifying two ectopic glands ( located immediately below the jugulum ) out of three in our study . 
we believe the combination of us and scintigraphy is useful in cases with a clinical suspicion and negative us , given that the detection of abnormal parathyroid glands in ectopic locations is not an uncommon event [ 1 , 7 , 22 , 2426 ]  . a number of studies have reported a significant reduction in us sensitivity in detecting glands with lower weight compared with heavier ones ; a similar , though not statistically significant , trend is reported for scintigraphy [ 7 , 15 , 17 , 27 ]  . 
in our study , considering the difference between identified and missed parathyroid glands , the greatest significance was recorded in the evaluation of the two numerically balanced subgroups of scintigraphy ( 33 identified and 23 missed ) , confirming that limited spatial resolution plays a significant role in the us detection rates . 
the mcnemar test ( table 7 ) revealed only a trend in favour of us ( p = 0.1340 ) , not a statistically significant difference , a result most likely due to small sample size . 
however , in the choice of diagnostic tool , lack of invasiveness , wider availability and lower cost weigh heavily in favour of us , which should be the technique of choice , even in the vent of equivalent diagnostic performance . 
riteniamo comunque utile nei casi con sospetto clinico ed ecografia negativa , data la possibilit non infrequente di riscontrare paratiroidi anormali in sede ectopica , affiancare allecografia la scintigrafia [ 1 , 7 , 22 , 2426 ]  . in alcuni lavori si riporta una significativa riduzione di sensibilit dellecografia nellidentificazione di ghiandole di basso peso rispetto a quelle di peso maggiore , simile andamento , ma non statisticamente significativo , riguarda la sensibilit della scintigrafia [ 7 , 15 , 17 , 27 ]  . nel nostro studio , considerando la differenza tra le paratiroidi identificate e quelle non identificate , la maggiore significativit si ha nella valutazione dei due sottogruppi , numericamente bilanciati ( 33 identificate e 23 non identificate ) della scintigrafia , che conferma come la limitata risoluzione spaziale abbia un ruolo importante nellidentificazione delle ghiandole con questa tecnica . tuttavia la larga deviazione standard dei pesi ghiandolari indica che sono sicuramente coinvolti altri fattori , per esempio una concomitante patologia tiroidea . 
lo stesso si potrebbe dire per lecografia , anche se il non bilanciato rapporto tra i due sottogruppi ( 55 identificate versus 9 non identificate ) crea un limite statistico dovuto alle piccole dimensioni del campione ; inoltre , sempre considerando lecografia , la notevole differenza tra le mediane del peso ( 470 mg per le paratiroidi identificate , 180 mg per quelle non identificate ) si contrappone a valori simili delle medie ( 1022 , 5 mg versus 921 , 8 mg ) , a causa della presenza di singoli casi con peso di molto superiore alla media ( come nel caso di un adenoma paratiroideo ectopico con peso superiore alla media di pi di una ds )  . la minore influenza del peso delle paratiroidi nella sensibilit dellecografia rispetto a quella della scintigrafia il verosimile motivo dei maggiori livelli di sensibilit della stessa ecografia . 
il test di mcnemar ( tabella 7 ) ha mostrato solo un favore dellecografia ( p = 0 , 1340 ) , e non una significativit statistica , verosimilmente a causa delle ridotte dimensioni del campione . tuttavia , nella scelta tra i due mezzi diagnostici , la non invasivit , la maggior disponibilit e i minori costi giocano pesantemente a favore dellecografia che dovrebbe rappresentare comunque la tecnica di prima istanza anche nel caso di uguali performance diagnostiche . 
essi hanno anche realizzato unanalisi dei costi e concludono dicendo che il ricorso ad una metodica di iii livello come la spect solo nei casi di ecografia dubbia o negativa pu ridurre considerevolmente i costi dellimaging prima della paratiroidectomia . trend radiol med ( 2009 ) 114 : 11591172 1171 reported by tublin et al . 
their cost analysis showed that limiting the use of a third - line modality such as spect to cases of doubtful or negative us only can considerably reduce preoperative imaging costs . a few limitations of this study need to be acknowledged . firstly , its design was retrospective , even though the analysis was based on us diagnosis produced prospectively before surgery . 
the sensitivity of scintigraphy , ct and mr imaging is , however , even more affected in these cases [ 1 , 3 , 7 , 11 , 16 , 18 , 20 , 22 ]  . finally , us being an operator - dependent technique , our results are likely to be affected by the radiologists experience and by their long cooperation with the surgeons [ 1 , 9 , 10 ]  . 
different clinical settings and low levels of experience might undermine the reproducibility of our results . in conclusion , our study has shown that us represents the technique of choice for the detection of pathological parathyroid glands in patients with primary hyperparathyroidism and a high likelihood of single adenoma . 
un secondo limite quello relativo alla dimensione campionaria , non sufficiente a determinare una significativit statistica in favore della sensibilit dellecografia rispetto alla scintigrafia , ma solo un trend ( p = 0 , 1340 )  . 
i nostri risultati , infine , sono probabilmente dovuti anche allesperienza degli ecografisti , come ovvio per una tecnica operatore dipendente , e alla prolungata collaborazione con i chirurghi [ 1 , 9 , 10 ]  . 
contesti clinici differenti e minore esperienza specifica da parte dei colleghi radiologi potrebbero rendere non riproducibili i risultati del presente studio . in conclusione , il nostro studio ha mostrato che lesame ecografico rappresenta la tecnica di prima istanza nellidentificazione delle paratiroidi patologiche in soggetti con iperparatiroidismo primario e alta probabilit di adenoma singolo . 
42 chapters divided into 7 sections : technique ; neuro / ear - nose - throat ; cardiovascular imaging ; lung ; oncology ; intervention ; trauma imaging / acute care are intended to increase the readers confidence regarding the enormous and ever - increasing progress in multidetector imaging that has taken place since the publication of the second edition in 2002 . 
 much of what is described has its roots in the results of the 5th international symposium on multi - detector row ct . the aim and desire of the editors was to provide fundamental knowledge on this field , coupled with the latest ct scanner technology , updating the important clinical scenario . great importance is given to technical and also practical details , which are essential when using these ultrafast machines in order to fully exploit their enormous potential . 
chapters are devoted to indepth evaluation of the head and neck ( 6 chapters ) , cardiovascular system ( 11 chapters ) and lungs ( 3 chapters ) as well as oncology and intervention . 
importance is also given to multi - slice ct in the field of trauma . the book can be considered a salute to the mnich school of radiology , since most of the authors belong to this group , in conjunction with internationally known coauthors from europe and the usa . 
 in some of the chapters , the reader will need a pico della mirandolas memory due to the robust use of acronyms or short - listings , some of which are not defined . 
in some ways the subject index tries to obviate this phenomenon , yet one cannot always peruse the index in order to find ( not always ) what he is searching . 
in the text , unfortunately , some of the references to figures are incorrect as well as figure captions il lettore trover 614 pagine in questa terza edizione di multislice ct dal peso di 1.900 grammi , divisa in 42 capitali raggruppati in 7 sezioni dal titolo : technique ; neuro / ear - nose - throat ; cardiovascular imaging ; lung ; oncology ; intervention ; trauma imaging / acute care . 
scopo del volume di rendere edotto il lettore degli enormi e continui progressi nello studio per immagini con attrezzature multidetettore avvenuti nel corso di questi ultimi anni dalla data della seconda edizione nel 2002 . molto di quanto descritto trae le sue origini dalla presentazioni fatte al 5 simposio internazionale sulla tc con multidetettore : scopo e desiderio espresso dagli editori del volume stato di voler diffondere quanto pi possibile una conoscenza di base fondamentale in questo campi associata ai pi recenti progressi tecnologici nei riguardi anche delle ricadute nello scenario clinico da parte degli stessi . nel volume viene data grande importanza non solo ai dettagli tecnici ma anche a quelli pratici , che sono di assoluta e necessaria conoscenza nelluso di queste macchine ultra veloci in modo tale da poterne sfruttare al meglio le loro enormi potenzialit . 
vengono descritti nel dettaglio la preparazione del paziente e la radioprotezione dello stesso , luso dei mezzi di contrasto , langio - tc , lo studio con tomografia a doppio sorgente e linterpretazione delle immagini ottenute . 
vari capitoli sono dedicati ad una valutazione e studio in profondit della testa e del collo ( 6 capitoli ) del sistema cardiovascolare ( 11 capitoli ) , dei polmoni ( 3 capitoli ) come anche alloncologia ed allinterventistica . 
 il volume pu essere considerato il trionfo della scuola di radiologia di monaco di baviera dal momento che buona parte degli autori ne fa parte , in collaborazione con un gruppo di ben conosciuti co - autori europei ed americani . in alcuni dei capitoli chi legge dovr mettere in campo una memoria da pico della mirandola dato leccessivo , esorbitante uso di acronimi ed abbreviazioni , di cui alcune neppure spiegate . 
ballesio1 1dipartimento di scienze radiologiche , policlinico umberto i , universit sapienza di roma , roma , italy 2dipartimento di ginecologia e ostetricia , universit del sacro cuore di roma , roma , italy 3dipartimento di scienze ginecologiche , perinatologia e puericultura , policlinico umberto i , universit sapienza di roma , roma , italy correspondence to : s . 
savelli , via del risaro 81 , 00127 roma , italy , tel . : + 39 - 348 - 6709705 , fax : + 39 - 06 - 52372327 , e - mail : sarasavelli@hotmail.it received : 12 november 2008 / accepted : 7 january 2009 / published online : 5 september 2009 springer - verlag 2009 abstract purpose . 
to evaluate the additional diagnostic value of fetal mri to evaluate cerebral ventriculomegaly assessed by ultrasonography ( us ) for the possibility to change the diagnosis , the counseling and the management of pregnancy . 
from february 2006 to october 2008 , we studied 55 pregnant women by fetal mri ( mean age 28 years ) , 4 with twin pregnancy , for a total of 59 fetuses with mean gestational age of 27 weeks . 
the findings showed that the two techniques are substantially in agreement in defining the degree of vm , with the exception of some cases in which the disagreement could be attributed to the possible progression of the dilatation between the us and mri examinations , which sway between two days and two weeks . 
we proved a low correlation between us and mri in the evaluation of ventriculomegaly associated either with cns or non - cns anomalies : in fact while fetal mri detected 26 / 55 ( 47 , 3% ) vm associated with cns anomalies , us demonstrated only 18 / 55 ( 32 , 7% )  . 
nel periodo compreso fra febbraio 2006 ed ottobre 2008 , abbiamo sottoposto a risonanza magnetica 55 donne in stato di gravidanza ( et media 28 aa ) , 4 delle quali con gravidanze gemellari , per un totale di 59 feti di et gestazionale con et gestazionale media di 27 settimane . 
tutti i feti avevano diagnosi ecografica di ventricolomegalia : 29 feti con ventricolomegalia isolata e 26 feti con ventricolomegalia associata ; in particolare in questultimo gruppo 18 feti riportavano associazioni con anomalie del snc ed 8 feti con anomalie di altri distretti . 
emerso cos che le due metodiche sono sostanzialmente in accordo nel definire lentit della ventricolomegalia , fatta eccezione per alcuni casi nei quali la discordanza potrebbe attribuirsi alla possibile progressione della dilatazione nellarco di tempo intercorso fra ecografia e risonanza magnetica , variabile fra 2 giorni e 2 settimane . 
our experience demonstrated that fetal mri has an important role as adjunctive tool to sonography in the evaluation of cerebral ventriculomegaly for the additional informations given to parents and for the possibility to change the diagnosis , the counseling and the management of pregnancy . 
the condition may present in an isolated form or in association with other abnormalities of the central nervous system ( cns ) and / or other regions , and often represents the tip of the iceberg of a much more complex underlying pathological condition . 
vm is also known to be associated with chromosome disorders and intrauterine infectious diseases , especially cytomegalovirus . ultrasonography ( us ) is the first - line modality for the morphological study of the foetal brain and can easily identify the presence of vm . 
however , the technique is not free from the difficulty of studying the structure of the posterior cranial fossa in foetuses of advanced gestational age , which already show cranial ossification or critical conditions such as oligohydramnios , and maternal obesity , which can hamper the examination . 
there are also abnormalities of brain parenchyma that appear as findings at the limits of the resolution power of us and brain diseases with nonspecific characteristics [ 35 ]  . the aim of our study was to evaluate the role of magnetic resonance imaging ( mri ) in the diagnostic characterisation of vm for the consequences that a change in diagnosis can have on maternal counselling , pregnancy management and the planning of possible preand postnatal procedures in the setting of multidisciplinary patient management . le ventricolomegalie ( vm ) rappresentano lanomalia encefalica fetale di pi frequente riscontro con una prevalenza variabile fra 0 , 3 e 1 , 5 / 1000 nati [ 1 ] fino a valori riportati di circa 22 / 1000 nati [ 2 ]  . 
queste possono presentarsi in forma isolata o in associazione ad ulteriori anomalie del sistema nervoso centrale ( snc ) e / o di altri distretti , rappresentando spesso la punta delliceberg di un quadro patologico sottostante ben pi complesso . 
nota inoltre lassociazione delle ventricolomegalie con cromosomopatie e con patologie infettive intrauterine , prima fra tutte linfezione da citomegalovirus . lecografia rappresenta lindagine di prima scelta per lo studio morfologico dellencefalo fetale ed in grado di individuare facilmente la presenza di una ventricolomegalia . tuttavia essa non scevra da limiti , come la difficolt di studiare le strutture della fossa cranica posteriore in feti di et gestazionale avanzata che mostrano gi ossificazione cranica o in condizioni critiche quali loligo - anidramnios e lobesit materna , che possono ostacolare lesecuzione dellesame . 
esistono inoltre anomalie del parenchima cerebrale che si manifestano con reperti ai limiti del potere risolutivo dellecografia e patologie encefaliche con caratteristiche non specifiche [ 35 ]  . lo scopo del nostro studio valutare il ruolo della risonanza magnetica ( rm ) nellinquadramento diagnostico delle ventricolomegalie per le conseguenze che un cambiamento della diagnosi pu avere sul counselling materno , sul radiol med ( 2009 ) 114 : 10131023 materials and methods between february 2006 and october 2008 , we performed an mri evaluation of 55 pregnant women ( maternal age range 1839 years , mean 28 years ) , four with twin pregnancies , for a total of 59 foetuses with a gestational age range of 1938 weeks ( mean gestational age 27 weeks )  . 
the number of foetuses with vm identified at us was 55 , and these made up our study population . all foetuses were referred to our mri service with a us diagnosis of vm : 29 with isolated vm and 26 with associated vm . 
in the latter group , 18 showed associations with cns abnormalities and eight with abnormalities in other regions , one of these with a diagnosis of trisomy 21 and one with known cytomegalovirus infection . examinations were performed with a 1.5 - tesla scanner ( siemens magnetom avanto , siemens medical systems , erhlangen , germany ) using a phased - array coil positioned on the maternal pelvis . 
the study protocol of the foetal brain included the use of the following sequences : t2 - weighted half fourier acquisition single - shot turbo spin - echo ( haste ) : tr 1 , 500 ms ; te 151 ms ; slice thickness 4 mm ; fov 260350 mm ; matrix 192256 ; ta 20 s , in axial , coronal and sagittal planes of the foetal brain t1 - weighted 2d fast low - angle shot ( flash ) : tr 362 ms ; te 4.8 ms ; slice thickness 4 mm ; flip angle 70 ; fov 350300 mm , matrix 256192 ; ta 20 s , in axial or coronal planes . in some cases , when considered appropriate , the examination was performed with the following sequences : true fast imaging with steady - state precession ( fisp ) : tr 4.8 ms ; te 2.3 ; slice thickness 4 mm ; fov 400300 mm ; matrix 256144 ; ta 14 s , repeated in the same planes as the t2 - weighted haste sequences diffusion weighted imaging ( dwi ) : tr 8 , 000 ms , te 90 ms ; ti 185 ms ; slice thickness 5 mm ; fov 420300 mm ; matrix 192192 ; ta 45 s ; three b - factors ( diffusion gradients ) per plane : 0 , 200 and 700 s / mm2 , in the x , y , z orthogonal axes , acquired in axial or coronal planes of the foetal brain fluid - attenuated inversion recovery ( flair ) : tr 10 , 000 ms ; te 102 ; slice thickness 4 mm ; fov 300300 mm ; matrix 128128 ; acquisition time 40 s , in axial or coronal planes the measurement of ventricular diameters was performed in the axial and / or coronal planes , at the atrial level , in correspondence of the choroids plexuses . 
the management della gravidanza e sulla pianificazione di eventuali interventi pree post - natali , nellottica di una gestione multidisciplinare . 1015 materiali e metodi nel periodo compreso fra febbraio 2006 ed ottobre 2008 , abbiamo sottoposto a rm 55 donne in stato di gravidanza ( et materna compresa fra 18 e 39 anni , et media 28 anni ) , quattro delle quali con gravidanze gemellari , per un totale di 59 feti di et gestazionale ( eg ) compresa fra 19 e 38 settimane ( eg media 27 settimane )  . 
 tutti i feti venivano mandati al nostro servizio di rm con diagnosi ecografica di ventricolomegalia : 29 feti con ventricolomegalia isolata e 26 feti con ventricolomegalia associata ; in particolare in questultimo gruppo 18 feti riportavano associazioni con anomalie del snc ed 8 feti con anomalie di altri distretti , uno dei quali con diagnosi posta di trisomia 21 ed uno con infezione nota da citomegalovirus ( cmv )  . gli esami sono stati eseguiti con un magnete superconduttore da 1 , 5 tesla ( siemens magnetom avanto , siemens medical systems , erhlangen , germania ) , utilizzando una bobina phased array , posizionata sulla pelvi materna . 
le pazienti sono state esaminate in posizione supina o in decubito laterale qualora ne riportassero la necessit e non stata effettuata alcuna sedazione , n sulle donne n sul feto . per la localizzazione del feto sono state ottenute in primo luogo immagini di scanogramma multiplanare , poi , durante lesame , ciascuna sequenza servita come scanogramma per la successiva . 
where possible , we compared the findings with postnatal imaging findings or biopsy examinations , and only in five cases do we have follow - up information of the neonates from patient history data gathered directly from the mother or paediatrician . results we compared the diagnoses of the two modalities in terms of two parameters , i.e. 
the degree of dilatation of the lateral ventricles ( table 1 ) and on the basis of the presence / absence of abnormalities associated with vm ( table 2 )  . 
the findings showed that the two techniques are substantially in agreement in defining the degree of vm , with the exception of some cases in which the disagreement could be attributed to the possible progression of the dilatation in the interval between the us and mri examinations , which varied from 2 days to 2 weeks . s / mm2 , sugli assi ortogonali x , y , z , acquisite sui piani assiale o coronale dellencefalo fetale ; fluid - attenuation invertion recovery ( flair ) : tr 10000 ms ; te 102 ms ; spessore strato 4 mm ; fov 300300 mm ; matrice 128128 ; tempo di acquisizione 40 s , sui piani assiale o coronale . 
la soglia considerata di normalit era un diametro atriale inferiore a 10 mla classificazione adottata per definire il grado di dilatazione stata la seguente [ 6 , 7 ] : vm borderline : 10 mmda12 mm ; vm lieve : 13 mmda15 mm ; vm severa : da > 15 mm . i reperti rm sono stati confrontati con le relative indicazioni ecografiche . 
quando possibile abbiamo avuto il riscontro con esami strumentali post - natali o esami bioptici , ed in soli 5 casi disponiamo del follow - up dei piccoli pazienti attraverso dati anamnestici raccolti direttamente dalle madri o dai pediatri di riferimento . risultati a lesser degree of agreement was found with regard to the association of the cases of vm with further abnormalities abbiamo confrontato le diagnosi delle due metodiche rispetto a due parametri , ossia rispetto al grado di dilatazione table 1 degree of ventriculomegaly : us vs . 
in fact , mri revealed 26 / 55 ( 47.3% ) cases of vm associated with abnormalities of the cns against 18 / 55 ( 32.7% ) cases of diagnosis of association with other brain abnormalities identified with us . 
table 4 reports the diagnoses of associated abnormalities made at us and later not identified at mri . discussion the impact of vm on foetalneonatal morbidity and mortality is influenced by different factors , including : degree of dilatation unilateral or bilateral presentation symmetry / asymmetry of the dilatation regression , stability or progression of the condition association with additional abnormalities of the brain or other organs dei ventricoli laterali ( tabella 1 ) ed in base alla presenza / assenza di anomalie associate alla ventricolomegalia ( tabella 2 )  . 
emerso cos che le due metodiche sono sostanzialmente in accordo nel definire lentit della ventricolomegalia , fatta eccezione per alcuni casi nei quali la discordanza potrebbe attribuirsi alla possibile progressione della dilatazione nellarco di tempo intercorso fra ecografia e risonanza magnetica , variabile fra 2 giorni e 2 settimane . minor grado di accordo invece emerso dal confronto rispetto alla associazione delle ventricolomegalie con ulteriori anomalie sia del snc fetale che di altri organi e apparati ( tabella 2 )  . 
la rm ha infatti evidenziato 26 / 55 ( 47 , 3% ) vm associate ad anomalie del snc , versus 18 / 55 ( 32 , 7% ) diagnosi di associazione con ulteriori anomalie encefaliche poste con lecografia ; quanto alle associazioni con anomalie di altri distretti , la rm ne ha posto diagnosi in 10 / 55 casi ( 18 , 2% ) e lecografia in 8 / 55 feti ( 14 , 5% )  . 
la tabella 3 mostra tutte le anomalie del snc associate , sia quelle gi diagnosticate allesame ecografico morfologico , sia quelle inizialmente non riconosciute dallecografia e poi diagnosticate con rm . 
 [ 10 ] riportano che l86% delle ventricolomegalie isolate stabili o progressive presentano una morbilit / mortalit in percentuali molto elevate mentre altri autori riportano un normale sviluppo psicomotorio nel 90% dei casi di vm che si risolvono prima della nascita [ 11 ]  . studiare questi dati limportanza di sottolineano radiol med ( 2009 ) 114 : 10131023 1019 normal psychomotor development in 90% of cases of vm that resolve prior to birth [ 11 ]  . 
these figures emphasise the importance of thoroughly studying cases of vm , and some authors believe that the diagnosis of isolated vm should be a diagnosis of exclusion , thus justifying the use of mri despite the high costs and complexities of the examination . mri in fact provides a detailed study of the brain parenchyma , which makes possible not only the measurement of biometric values but also the evaluation of neuronal migration , gyration and sulcation and myelination . 
it also can identify haemorrhagic foci , porencephaly , cortical and subependymal tubers , abnormalities of the structures of the midline and partial and complete agenesis of the corpus callosum , and abnormalities of the posterior cranial fossa ( cysts , hypoplasia and agenesis of the cerebellar vermis ) [ 5 ]  . some studies in the literature [ 12 ] report in their own series a us classification error of isolated / associated vm in 37% of cases in which associated diseases are incorrectly identified , even by expert operators , with relative consequences on prognosis and management . 
indeed , whereas the failure to identify an agenesis of the corpus callosum can have mild consequences ( favourable prognosis in 85% of cases ) , this is not the case for other conditions such as abnormalities of neuronal migration , which significantly influence prognosis and often only appear as an alteration in mri signal [ 13 ] , and therefore difficult to identify with us . in a study on 214 foetuses with vm , levine et al . 
these were six cases ( 10.9% ) of cns abnormalities and two cases of abnormalities of other regions ( two cases of pulmonary hypoplasia with retarded parenchymal maturation )  . 
in another four cases , mri negated the us diagnosis of agenesis of the corpus callosum ( two cases ) , hypoplasia of the cerebellar vermis and cysts of the posterior cranial fossa . it should be noted that in our series , in agreement with the literature [ 15 ] , associated diseases identified with mri and not detected with us are for the most part abnormalities of the cerebral / cerebellar parenchyma , such as neuronal approfonditamente i casi di ventricolomegalia ed alcuni autori ritengono che la diagnosi di vm isolata debba essere una diagnosi di esclusione giustificando limpiego della risonanza magnetica a dispetto degli elevati costi e della complessit dellesame . 
la rm consente infatti un dettagliato studio del parenchima cerebrale permettendo , oltre alla misurazione dei valori biometrici , anche la valutazione della migrazione neuronale , della girazione e solcazione , e della mielinizzazione ; permette inoltre di identificare foci emorragici , cavit porencefaliche , tuberi subependimali e corticali , anomalie delle strutture della linea mediana ed agenesie parziali e complete del corpo calloso , anomalie delle strutture della fossa cranica posteriore ( cisti vermiane , ipoplasia ed agenesia del verme cerebellare ) [ 5 ]  . alcuni studi in letteratura [ 12 ] riportano nella propria casistica un errore ecografico di classificazione delle vm isolate / associate nel 37% dei casi in cui patologie associate non venivano riconosciute anche in mani esperte , con relative conseguenze sulla prognosi e sul management . 
infatti se il mancato riconoscimento di unagenesia del corpo calloso pu avere conseguenze talvolta modeste ( prognosi favorevole nell85% dei casi ) , ci non vero per altre condizioni come le anomalie di migrazione neuronale che influiscono in maniera rilevante sulla prognosi e che si manifestano spesso solo come alterazioni di segnale in rm [ 13 ] , pertanto difficilmente rilevabili ecograficamente . 
 [ 14 ] , in uno studio su 214 feti con ventricolomegalia , hanno notato che la rm comportava : cambiamento della diagnosi nel 23% circa dei casi gi anomali allecografia ; cambiamento del counselling nel 41% circa dei casi ; variazione del management nel 13 , 5% dei casi . 
nel nostro studio , la rm ha diagnosticato la presenza di anomalie associate alla ventricolomegalia in ulteriori 8 / 55 casi ( 14 , 5% ) rispetto allecografia , trattandosi in 2 casi di anomalie di altri distretti ( due ipoplasie polmonari con ritardo di maturazione parenchimale ) ed in 6 casi ( 10 , 9% ) di anomalie del snc . 
si evince pertanto che le vm possono rappresentare la punta delliceberg di un quadro patologico pi complesso caratterizzato dalla presenza di ulteriori anomalie , ed pertanto necessario approfondirne lo studio e seguirne levoluzione sia per monitorare la stabilit sia per diagnosticare anomalie che possono manifestarsi in et gestazionale pi avanzata . la rm diventa inoltre di cruciale importanza quando si debba individuare la causa determinante la ventricolomegalia , radiol med ( 2009 ) 114 : 10131023 1021 fig . 
3 feto alla 35a settimana di gestazione : vm severa monolaterale con parenchima cerebrale assottigliato e di alterato segnale ; le immagini mostrano inoltre ritardo della girazione e solcazione omolateralmente alla dilatazione . 
5 feto alla 31a settimana di gestazione : vm severa bilaterale , dilatazione del iii ventricolo , parenchima cerebrale assottigliato , ipoplasia cerebellare con polimicrogiria , dilatazione della cisterna magna . 
the correct characterisation can in fact have significant ramifications on the one hand for counselling and consequently for the management of the pregnancy in the legal context with regard to abortion , and on the other hand for the type of treatment in terms of the planning of a possible neurosurgical procedure [ 16 ]  . the literature does not provide specific indications regarding when further study of a diagnosis of vm is indicated with mri . 
cova1 1uco di radiologia , universit di trieste , ospedale di cattinara , strada di fiume 449 , 34149 trieste , italy 2uo di urologia , ospedale fondazione san raffaele giglio , contrada pietrapollastra , 90015 cefal , italy correspondence to : m . 
phosphodiesterase - 5 ( pde - 5 ) inhibitors have an established role in the treatment of erectile dysfunction , but there is increasing evidence that these drugs are effective also for the treatment of lower urinary tract symptoms and benign prostatic hyperplasia ( bph )  . 
the aim of this study was to investigate whether administration of tadalafil , a pde - 5 inhibitor , in patients with bph produces haemodynamic changes in the prostate that can be assessed using contrast - enhanced us ( ceus )  . 
changes in enhancement peak , time to peak ( ttp ) , sharpness of the bolus transit and area under the curve ( auc ) were considered for further analysis . 
gli inibitori della 5 - fosfodiesterasi ( pde - 5 ) hanno un ruolo ben definito nella terapia della disfunzione erettile , ma vi una crescente evidenza che questi farmaci siano efficaci anche per il trattamento dei disturbi delle basse vie urinarie e delliperplasia prostatica benigna ( ipb )  . 
dodici pazienti consecutivi con ipb sono stati studiati con ecocontrastografia prima e dopo la somministrazione di 20 mg di tadalafil . lecocontrastografia stata eseguita con un software contrastospecifico non distruttivo dopo somministrazione in bolo di sonovue ( 4 , 8 ml )  . 
le variazioni del picco di enhancement , del tempo di picco ( ttp ) , della ripidezza del transito del bolo e dellarea sotto la curva ( auc ) sono state valutate statisticamente . radiol med ( 2009 ) 114 : 11061114 1107 observed in the prostate after tadalafil administration , which can be detected with ceus . keywords prostate phosphodiesterase - 5 contrast enhanced ultrasound benign prostatic hyperplasia ( bph ) tadalafil risultati . 
nei pazienti con ipb dopo somministrazione di tadalafil si osservano variazioni della vascolarizzazione prostatica rilevabili con lecocontrastografia . parole chiave prostata 5 - fosfodiesterasi ecocontrastografia iperplasia prostatica benigna tadalafil introduction introduzione phosphodiesterases ( pde ) are intracellular enzymes that catalyse the hydrolysis of cyclic adenosine monophosphate ( camp ) and cyclic guanosine monophosphate ( cgmp )  . 
 several pde - 5 inhibitors are available , including sildenafil ( viagra , pfizer , italy ) , vardenafil ( levitra , bayer , italy ) and tadalafil ( cialis , lilly , italy )  . 
by inhibiting the enzyme reactions catalysed by pde - 5 , these drugs increase intracellular cgmp and reduce intracellular calcium , leading to an alteration of intracellular calcium - dependent processes , including relaxation of the smooth muscles of parenchyma and vessels [ 8 ]  . 
the therapeutic success achieved in this field recently prompted clinicians to search for new applications in treating lower urinary tract disorders in patients with benign prostatic hyperplasia ( bph ) and / or chronic prostatitis [ 1013 ]  . 
the most widely accepted hypothesis , based on studies conducted on prostate tissue specimens [ 15 , 16 ] , is that these agents act to relax prostatic smooth muscle , thereby increasing the washout of secretions [ 12 ]  . 
it is also likely that these agents relax the prostatic parenchymal vasculature , as demonstrated at the systemic and penile level [ 4 , 9 ] , which translates into changes in blood flow . the aim of this study was to establish whether the signal le fosfodiesterasi ( pde ) sono enzimi intracellulari che catalizzano lidrolisi delladenosin - monofosfato ciclica ( camp ) e della guanosin - monofosfato ciclica ( cgmp )  . esistono almeno 11 isoforme di tali enzimi , con varia distribuzione a carico dei diversi tessuti . 
la 5 - pde , in particolare , oltre che a livello penieno , espressa nei tessuti encefalici [ 1 ] , nel cuore [ 2 , 3 ] , nella muscolatura liscia dei vasi [ 4 ] , nella vescica [ 5 ] e nella prostata [ 6 , 7 ]  . 
 sono disponibili diversi farmaci inibitori della 5 - pde quali sildenafil ( viagra , pfizer italia ) , vardenafil ( levitra , bayer italia ) e tadalafil ( cialis , lilly italia )  . 
questi farmaci , inibendo le reazioni enzimatiche catalizzate dalla 5 - pde , producono un aumento del cgmp intracellulare ed una riduzione del calcio intracellulare , ci comporta unalterazione dei processi intracellulari calcio - dipendenti , tra cui il rilasciamento della muscolatura liscia dei parenchimi e dei vasi [ 8 ]  . 
il successo terapeutico in questo campo ha recentemente spinto i clinici a ricercare nuove applicazioni nel trattamento dei disturbi delle basse vie urinarie in pazienti con iperplasia prostatica benigna ( ipb ) e / o con prostatiti croniche [ 1013 ]  . 
lipotesi pi accreditata , basata su studi condotti su campioni di tessuto prostatico [ 15 , 16 ] , teorizza che tali farmaci producano essenzialmente un rilasciamento della muscolatura liscia prostatica che favorisce il drenaggio delle secrezioni [ 12 ]  . peraltro verosimile che questi farmaci producano il rilasciamento dei vasi parenchimali anche a livello prostatico , come stato dimostrato a livello sistemico e penieno [ 4 , 9 ] , evento che si traduce in variazioni dellapporto ematico . scopo di questo lavoro stabilire se nei pazienti con iperplasia prostatica benigna possibile misurare in 1108 radiol med ( 2009 ) 114 : 11061114 intensity of sonovue microbubbles can be determined in a reproducible manner in patients with bph and to assess whether tadalafil administration induces changes in prostate vascularity that can be detected with contrastenhanced ultrasound ( ceus )  . 
 materials and methods materiali e metodi twelve consecutive patients ( age range 3686 years ; mean age 66 years ) with bph underwent us examination of the prostate with the transrectal approach . 
a new - generation us unit ( iu22 , philips medical systems , bothell , wa , usa ) equipped with an end - fire broadband endocavitary transducer supporting nondestructive ceus imaging ( c9 - 5 , pulse inversion harmonic imaging , pihi ) was used . after a preliminary colour doppler us examination , an obliquetransverse scan plane was selected for the ceus study . 
 baseline ceus was conducted during the bolus injection of 4.8 ml sonovue , and digital video recordings were obtained for at least 2 min from the start of the injection . after baseline ceus , the patient was administered 20 mg oral tadalafil and was examined again 90 min after receiving the drug , with the same parameters as used for the baseline examinations . the digital clips obtained before and after tadalafil administration were retrospectively reviewed with dedicated software ( qontraxt v.360 , amid , rome , italy ) by two blinded independent readers who were not involved in scanning and were unaware of whether the scans had been obtained before or after tadalafil administration . 
the following changes in the enhancement curve parameters supplied by the software and indicative of enhancement kinetics before and after tadalafil administration were considered : enhancement peak ( expressed as a percentage , maximum intensity = 100% ) ; time to peak ( expressed in seconds ) ; sharpness of the bolus transit ( expressed in seconds - 1 ) ; area under the curve ( auc ; expressed in seconds - 1 )  . 
 stato utilizzato un ecografo di ultima generazione ( iu22 , philips medical systems , bothell , wa ) dotato di un trasduttore endocavitario endfire a larga banda abilitato allimaging ecografico non distruttivo con mezzo di contrasto ( c9 - 5 , pulse inversion harmonic imaging , pihi )  . dopo un preliminare esame eco - color doppler stato scelto un piano di scansione trasversale obliquo per lo studio ecocontrastografico della prostata . 
per ridurre al minimo la rottura delle microbolle la potenza acustica del trasduttore stata regolata su bassi livelli di indice meccanico ( im = 0 , 07 ) e mantenuta invariata per tutti i pazienti . per limitare le cause di variabilit nella valutazione dellenhancement , il guadagno stato regolato per ogni paziente prima delliniezione delle microbolle e mantenuto costante per tutta la durata dellesame . 
il paziente stato quindi esaminato nuovamente dopo 90 minuti dalla somministrazione del farmaco utilizzando gli stessi parametri dellesame di base . i filmati digitali ottenuti prima e dopo la somministrazione del farmaco sono stati analizzati retrospettivamente in forma anonima utilizzando un software dedicato ( qontraxt v.360 , amid , roma , italia ) da due lettori indipendenti non coinvolti nellesecuzione dellesame e che non sapevano se le scansioni erano state ottenute prima o dopo la somministrazione di tadalafil . 
sono state considerate le variazioni prima e dopo la somministrazione di tadalafil dei seguenti parametri della curva di enhancement , forniti automaticamente dal software , descrittivi della cinetica del contrasto : picco di enhacement ( espresso in percentuale , massima intensit = 100% ) ; tempo di picco ( espresso in secondi ) ; ripidezza del transito del bolo ( espresso in secondi - 1 ) ; area sotto la curva di enhancement ( espresso in secondi - 1 )  . 
le variazioni di questi parametri prima e dopo la somministrazione di tadalafil sono state valutate statisticamente utilizzando il test dei ranghi con segno di wilcoxon ( wilcoxon signed - rank test )  . 
i valori del picco di enhancement , del tempo di picco , della ripidezza del transito del bolo e dellarea sotto la curva ottenuti prima e dopo lassunzione di tadalafil sono riportati in tabella 1 . 
sotto leffetto del farmaco si osservato un aumento statisticamente significativo del picco di enhancement e dellarea sotto la curva ( p < 0 , 002 ) , mentre non sono state rilevate variazioni statisticamente significative dei restanti parametri . i diagrammi di bland - altman relativi alla variabilit interosservatore per i diversi parametri sono riportati in figura 3 . 
gli intervalli di confidenza ( ic ) al 95% per il picco di enhancement , per larea sotto la curva , per il 1110 radiol med ( 2009 ) 114 : 11061114 fig . 
immagini ottenute 10 s , 20 s , 37 s , 60 s dopo liniezione delle microbolle con un software contrastospecifico non distruttivo ( im = 0 , 07 )  . 
3a - d bland - altman plots show interobserver variability ( with two observers ) for the measurement of enhancement peak ( a in per cent of maximum enhancement ) ; time to peak ( b in seconds ) ; sharpness of the bolus transit ( c in s - 1 ) ; and area under the curve ( d in s - 1 ) in a randomly selected group of ten perfusion curves . 
3a - d diagrammi di bland - altman relativi alla variabilit interosservatore ( con 2 osservatori ) per le misure del picco di enhancement ( a , in percentuale del massimo enhancement ) ; del tempo di picco ( b , in secondi ) ; ripidezza del transito del bolo ( c , in secondi - 1 ) ; e dellarea sotto la curva ( d , in secondi1 ) in un gruppo di 10 curve di perfusione scelte a caso . 
questa variabilit accettabile se rapportata alle differenze medie tra le misure dei parametri ottenute dai due osservatori che erano rispettivamente di 31 , 62% , 4 , 41 s - 1 , 35 , 36 s e 0 , 146 s - 1 . discussion discussione studies conducted on the heart [ 17 ] , liver [ 18 ] , kidney [ 19 ] and other organs [ 2023 ] have demonstrated that ceus provides a useful and noninvasive tool for evaluating changes in the vascularity of the parenchyma and lesions . 
in studi condotti sul cuore [ 17 ] , sul fegato [ 18 ] , sul rene [ 19 ] e su altri organi [ 2023 ] hanno dimostrato che lecocontrastografia fornisce un utile strumento non invasivo per valutare variazioni della vascolarizzazione dei parenchimi e delle lesioni . 
in ambito prostatico lecocontrastografia 1112 radiol med ( 2009 ) 114 : 11061114 prostatic imaging , ceus has been proposed as a helpful technique for the detection and targeted biopsy of isoechoic neoplasms [ 2427 ]  . 
in fact , it is only in recent years that highly performing endocavitary transducers have become clinically available for the realtime , nondestructive , contrast - specific imaging of the prostate . 
by using this approach , we were able to demonstrate that prostatic blood flow was altered following tadalafil administration and that this change could be detected in a reproducible and noninvasive manner with ceus . 
moreover , we were unable to determine whether the changes observed in prostate vascularity were due to a local effect of tadalafil or to systemic effects resulting from a generalised relaxation of the smooth muscles of arteries . 
another limitation is related to the fact that enhancement of the prostatic parenchyma was evaluated by measuring variations in the intensity of the video signal on the sonographic images . more accurate measurements can be achieved by using specific software that quantifies the signal on a linear scale before logarithmic compression for video display [ 18 , 28 ]  . another limitation lies in the fact that the microbubbles were administered as a bolus and the enhancement measurements were fitted to a gamma - variate curve . 
with this method , the parameters reflecting parenchymal perfusion ( blood velocity , blood volume and blood flow ) can be extrapolated on condition that one can correct for microbubble recirculation [ 29 ]  . 
to perform this correction , one needs to know the concentration of microbubbles in blood and acquire enhancement curves both in the arteries supplying the organ and in the parenchyma . 
analysis of the enhancement curves of the prostatic parenchyma after bolus administration of microbubbles thus allows one to recognise changes in organ vascularity but not to obtain absolute measurements of flow parameters . 
other methodological approaches , such as evaluation of reperfusion kinetics after microbubble rupture during the continuous administration of contrast at a constant rate , allow for a more direct correlation between enhancement curve characteristics and perfusion parameters [ 19 ] , but they require administration of a larger dose of contrast material . 
one limitation that is common to all sonographic perfusion techniques is that any accurate and rigorous quantitative analysis of enhancement characteristics is made extremely stata proposta da alcuni autori come uno strumento utile per lindividuazione e leffettuazione di una biopsia mirata di neoplasie isoecogene [ 2427 ]  . 
utilizzando questo approccio il nostro studio dimostra che dopo somministrazione di tadalafil si verifica unalterazione del flusso ematico nel parenchima prostatico e che questa alterazione rilevabile in maniera riproducibile e non invasiva con lecocontrastografia . 
inoltre , non possibile stabilire se le variazioni osservate nella vascolarizzazione del parenchima prostatico siano dovute ad un effetto locale del tadalafil o ad effetti sistemici dovuti , in particolare , ad un rilasciamento generalizzato della muscolatura liscia delle arterie . un altro limite legato al fatto che lenhancement del parenchima prostatico stato valutato misurando le variazioni dellintensit del segnale video sulle immagini ecografiche . 
misurazioni pi accurate possono essere ottenute utilizzando software dedicati progettati per quantificare il segnale in scala lineare , prima della compressione logaritmica necessaria per la presentazione a video delle immagini [ 18 , 28 ]  . 
utilizzando questo approccio i parametri che descrivono la perfusione parenchimale ( velocit del sangue , frazione del volume ematico e flusso ematico ) possono essere estrapolati solo quando possibile effettuare una correzione per leffetto del ricircolo delle microbolle [ 29 ]  . 
per eseguire questa correzione necessario conoscere la concentrazione delle microbolle nel sangue e acquisire la curva di enhancement sia nelle arterie afferenti allorgano , sia nel parenchima . nel nostro caso non possibile misurare la curva di enhancement nelle arterie afferenti alla prostata per la disposizione anatomica sfavorevole ed il piccolo calibro . 
lanalisi delle curve di enhancement del parenchima prostatico dopo somministrazione in bolo delle microbolle permette pertanto di riconoscere variazioni della vascolarizzazione dellorgano , ma non di ottenere misurazioni assolute sulle caratteristiche del flusso . 
altri approcci metodologici , quali la valutazione della cinetica di riperfusione dopo rottura delle microbolle durante somministrazione continua del contrasto a velocit costante , permettono una correlazione pi diretta tra le caratteristiche delle curve di enhancement e i parametri di perfusione [ 19 ] , ma richiedono la somministrazione di una maggiore quantit di contrasto . 
anzidei , tel : + 39 - 06 - 4455602 , fax : + 39 - 06 - 490243 , e - mail : michele.anzidei@gmail.com received : 3 november 2008 / accepted : 24 february 2009 / published online : 22 september 2009 springer - verlag 2009 abstract purpose . 
in the mr imaging protocol , we acquired t2weighted turbo spin - echo ( tse ) sequences , true fast imaging steady - state free precession ( true - fisp ) and gadolinium - enhanced t1 - weighted volumetric interpolated breath - hold examination ( vibe ) 3d sequences . 
le immagini rm sono state acquisite con sequenze turbo spin echo ( tse ) t2 pesate ad alta risoluzione , true fast imaging with steady state precession ( truefisp ) e volumetric interpolated breath hold examination ( vibe ) 3d t1 pesate dopo somministrazione ev di chelati del gadolinio ( gdbopta )  . 
la rm si rivelata pi accurata della tc nella valutazione delle lesioni t1 ( 50% vs 37 , 5% ) , mentre la tc risultata pi affidabile nella valutazione delle lesioni t2 ( 81 , 2% vs 68 , 7% )  . 
patients with locally advanced lesions ( t3t4 ) are , instead , normally treated with neoadjuvant chemoradiotherapy with the aim of shrinking the tumour to make resection possible [ 3 , 4 ]  . stage t3t4 is , however , associated with worse outcomes [ 5 , 6 ]  . 
however , these methods suffer several limitations that preclude their use in routine practice : eus is invasive , of limited use in severely debilitated patients , highly operator dependent and with a field of view restricted to the gastric wall ; laparoscopy is considered a surgical and hence highly invasive technique that requires anaesthesia and hospitalisation . 
over the past 10 years , the widespread diffusion of multislice computed tomography ( ct ) scanners and implementation of volumetric imaging have enabled the noninvasive staging of gastric cancers , with a sensitivity of 85%90% in t staging [ 1316 ]  . 
although magnetic resonance ( mr ) imaging provides higher contrast resolution in the study of soft tissues and particularly the walls of hollow organs , it has never been considered a real alternative to ct [ 17 ] owing to its long acquisition times and susceptibility to motion artefacts ( breathing , peristalsis and cardiovascular pulsation )  . 
these limitations have recently been partially overcome with technological developments and the introduction of fast imaging , leading to a significant increase in the accuracy of mr imaging [ 18 , 19 ]  . 
 [ 20 ] compared the diagnostic performance of ct and mr imaging in the local staging of gastric tumours , reporting encouraging results with the use of old - generation scanners . 
the aim of our study was to prospectively evaluate the diagnostic accuracy of ct and mr imaging in the locoregional staging of gastric carcinei pazienti affetti da carcinoma gastrico la stadiazione dellestensione locale di malattia rappresenta il parametro principale nella pianificazione terapeutica ed determinante nella prognosi . 
pazienti con lesioni localizzate ( t1t2 ) possono essere trattati chirurgicamente con intento radicale , garantendo ottima sopravvivenza a lungo termine [ 1 , 2 ] ; pazienti con lesioni localmente avanzate ( t3t4 ) sono invece generalmente trattati con chemio - radioterapia neoadiuvante con lobiettivo di ridurre le dimensioni del tumore per renderne possibile la resezione [ 3 , 4 ] ; lo stadio t3t4 tuttavia correlato con una prognosi peggiore [ 5 , 6 ]  . lecoendoscopia ( eus ) [ 79 ] e la laparoscopia esplorativa [ 1012 ] sono tecniche affidabili nella stadiazione locale del carcinoma gastrico . 
tuttavia queste metodiche presentano limitazioni che ne impediscono lutilizzo nella routine diagnostica : leus una metodica invasiva , limitata nei pazienti defedati , fortemente operatore dipendente e con un campo di vista ristretto alla parete gastrica ; la laparoscopia invece considerata metodica del tutto chirurgica , altamente invasiva , che necessita di anestesia e di alti costi di ospedalizzazione . 
negli ultimi dieci anni lampia diffusione delle apparecchiature di tomografia computerizzata ( tc ) multistrato e limplementazione dellimaging volumetrico hanno reso fattibile la stadiazione non - invasiva del tumore gastrico , con una sensibilit dell85%90% [ 1316 ] nella stadiazione del parametro t . 
sebbene la risonanza magnetica ( rm ) permetta una risoluzione di contrasto superiore nello studio dei tessuti molli , ed in particolare della parete degli organi cavi , il suo utilizzo non stato finora considerato quale reale alternativa alla tc [ 17 ] , soprattutto per la lunga durata delle acquisizioni e per la suscettibilit agli artefatti da movimento ( respiro , peristalsi e pulsazioni cardiovascolari )  . 
attualmente queste limitazioni sono state almeno parzialmente superate : i recenti sviluppi tecnologici e lintroduzione del fast - imaging hanno apportato un significativo incremento dellaccuratezza diagnostica della rm [ 18 , 19 ]  . 
lo scopo del nostro studio stato di valutare prospetticamente radiol med ( 2009 ) 114 : 10651079 1067 noma using state - of - the - art imaging protocols and technology . laccuratezza diagnostica della tc e della rm nella stadiazione loco - regionale del carcinoma gastrico utilizzando protocolli di imaging e tecnologie allo stato dellarte . materials and methods materiali e metodi from january to october 2008 , we enrolled 40 patients ( 26 men , 14 women ; mean age 53.6 years ) with an endoscopic diagnosis of gastric carcinoma . 
scopolamine ( buscopan , boehringer international , ingelheim , germany ) to relax the stomach musculature and reduce peristalsis , and 1 l of water orally to distend the stomach . 
 a first scan of the upper abdomen was obtained without contrast agent administration ( 120 kv , slice thickness 3 mm , reconstruction increment 1.5 mm ) , and later scans ( 250 mas , 120 kv , slice thickness 1.5 mm and reconstruction increment 1.0 mm ) were acquired in the arterial ( upper abdomen ) and venous ( chestabdomenpelvis ) phases after contrast administration . 
optimal delay between contrast administration ( 0.5 ml / kg iomeron 350 bracco spa , milan , italy , at a flow rate of 4 ml / s ) , and the beginning of the arterial - phase scan was calculated using the bolus - tracking technique , with a region of interest ( roi ) placed at the level of the coeliac trunk , threshold set at 150 hu and delay set at 15 s after reaching the threshold . mr examinations were performed with a 1.5 - t scanner ( magnetom avanto , siemens medical solutions , erlangen , germany ; gradient strength 45 mt / m , slew rate 346 t / m / s , rise time 400 ms )  . 
precontrast images were obtained with t2 - weighted turbo spin echo ( tse ) and true fast imaging with steady - state precession ( truefisp ) sequences in the axial and coronal planes ( table 1 )  . after the intravenous administration of 15 ml gadolinium benzyloxyproprionic - tetraacetic acid ( gd - bopta ) ( multihance , bracco spa , milan , italy ) , images were acquired in the arterial and venous phases using t1 - weighted 3d volumetric interpolated breath - hold examination ( vibe ) sequences ( table 1 )  . 
both the ct and mr imaging studies were evaluated preoperatively by two groups of tra gennaio ed ottobre 2008 , sono stati arruolati 40 pazienti ( 26 uomini , 14 donne ; et media di 53 , 6 anni ) con diagnosi endoscopica di carcinoma gastrico . 
per 7 pazienti ( 17 , 5% ) stato programmata una chemioterapia neoadiuvante prima di una eventuale resezione e 3 ( 7 , 5% ) pazienti hanno subito interventi di chirurgia palliativa a causa dellestensione locale della malattia . 
circa 10 minuti prima dellesame sono stati iniettati 20 ml di scopolamina ( buscopan , boehringer international , ingelheim , germania ) per rilassare la muscolatura viscerale e ridurre la peristalsi ed stato somministrato 1 l di acqua per os per la distensione gastrica . 
una prima scansione delladdome superiore stata ottenuta senza mezzo di contrasto ( 120 kv , slice thickness 3 mm , recon increment 1 , 5 mm ) e successivamente sono state acquisite scansioni ( 250 mas , 120 kv , slice thickness 1 , 5 mm e recon increment 1 , 0 mm ) in fase postcontrastografica artero - portale ( addome superiore ) e venosa ( torace - addome - pelvi ) ; il ritardo ideale tra la somministrazione del mezzo di contrasto ( mdc ; 0 , 5 ml / kg di iomeron 350 bracco spa , milano , italia , ad una velocit di flusso di 4 ml / s ) e linizio della scansione artero - portale stato calcolato tramite tecnica di bolus - tracking , con una regione di interesse ( roi ) posizionata a livello del tripode celiaco , soglia a 150 uh e ritardo a 15 secondi dal raggiungimento della soglia . 
gli esami rm sono stati eseguiti con unapparecchiatura a 1 , 5 t ( magnetom avanto , siemens medical solutions , erlangen , germania ; intensit dei gradienti 45 mt / m , slew rate 346 t / m / s , tempo di risalita 400 msec )  . 
le immagini precontrasto sono state ottenute con sequenze turbo spin echo ( tse ) e true fast imaging with steady state precession ( truefisp ) t2 pesate acquisite su piani assiali e coronali ( tabella 1 )  . 
the t parameter was staged according to the tumour node metastasis ( tnm ) classification established by the american joint committee on cancer and by the international union against cancer [ 21 ]  . 
progression of tumour invasion on ct and mr images was classified as follows : t1 : slight enhancement and focal thickening of the inner layer of the gastric wall t2 : diffuse enhancement and thickening of the entire gastric wall without extramural spread t3 : diffuse enhancement and thickening of the entire gastric wall , with irregularities and invasion of the perivisceral fat t4 : infiltration of adjacent organs , including vascular structures the ct studies were evaluated using 1.5 - mm - thick multiplanar reconstructions ( mpr ) parallel and perpendicular to the lesion . 
mr studies were evaluated using both the precontrast sequences ( tse and true - fisp ) and the sequences obtained after gd - bopta administration ( vibe 3d )  . 
la progressione dellinvasione tumorale nelle immagini tc ed rm stata classificata come segue : t1 : sottile enhancement ed ispessimento focale dello strato interno della parete gastrica ; t2 : diffuso enhancement ed ispessimento dellintera parete gastrica senza estensione extramurale ; t3 : diffuso enhancement ed ispessimento dellintera parete gastrica con irregolarit e invasione del grasso periviscerale ; t4 : infiltrazioni degli organi adiacenti , incluse le strutture vascolari . gli esami tc sono stati valutati utilizzando delle ricostruzioni multiplanari ( mpr ) parallele ed ortogonali alla lesione con spessore di 1 , 5 mm ottenute dai dati grezzi . 
gli esami rm sono stati valutati utilizzando sia le sequenze pre - constrastografiche ( tse e truefisp ) che le sequenze ottenute dopo somministrazione gd - bopta ( vibe 3d )  . 
relativamente alla rm , la stadiazione del parametro t stata effettuata con una valutazione combinata , ma le tre sequenze sono state visualizzate indipendentemente per consentire anche un confronto intra - metodica . 
lagreement tra i due gruppi stato misurato con il radiol med ( 2009 ) 114 : 10651079 1069 technique were compared with statistical package ( spss , chicago , il , usa )  . 
the percentage of detected lesions and stage attributed based on each diagnostic histopathological findings for lesions staged t1t3 and with exploratory laparotomy for lesions staged t4 ; mcnemar test was used to evaluate the accuracy of each technique in lesion detection and staging . 
compared with the histological and laparoscopic findings , ct correctly staged 33 / 40 lesions with a sensitivity of 82.5% , and mr imaging staged 32 / 40 lesions with a sensitivity of 80% ( table 2 )  . 
there were no statistically significant differences between mr imaging and ct in either sensitivity or accuracy ( mcnemar test p > 0.05 ) : the two techniques were concordant in 35 ( 87.5% ) cases with regard to the presence or absence of disease and in 37 ( 92.5% ) cases with regard to disease stage . 
evaluation performed on t1 - weighted contrast - enhanced 3d vibe sequences alone resulted in nine ( 22.5% ) lesions being understaged , whereas evaluation of t2 - weighted tse sequences led to the understaging of ten ( 25% ) lesions ( table 4 )  . test di cohen ( scarso : = 0 , 210 , 40 , moderato : = 0 , 410 , 69 , buono : = 0 , 610 , 80 , eccellente = 0 , 811 , 00 )  . la percentuale di lesioni individuate e lo stadio attribuito da ciascuna metodica diagnostica sono stati confrontati con il risultato isto - patologico nelle lesioni stadiate come t1t3 e con la laparotomia esplorativa nelle lesioni stadiate come t4 ; il test di mcnemar stato utilizzato per valutare laccuratezza di ogni metodica sia nellindividuazione che nella stadiazione delle lesioni . 
 risultati lagreement tra i due gruppi di osservatori stato eccellente , sia per la tc ( = 0 , 957 ) che per la rm ( = 0 , 933 )  . rispetto ai reperti istologici e laparoscopici , la tc ha correttamente stadiato 33 / 40 lesioni neoplastiche con una sensibilit dell82 , 5% e la rm ha stadiato 32 / 40 lesioni con una sensibilit dell80% ( tabella 2 )  . 
non stata rilevata nessuna differenza statisticamente significativa tra rm e tc n per la sensibilit , n per laccuratezza ( test di mcnemar , p > 0 , 05 ) : le due metodiche si sono rivelate concordi in 35 ( 87 , 5% ) casi per la presenza o lassenza di malattia ed in 37 ( 92 , 5% ) casi per la stadiazione . 
la valutazione con le sole sequenze t1 pesate contrast enhanced ( ce ) - vibe 3d ha invece portato a sottostadiarne 9 ( 22 , 5% ) mentre valutando le sequenze t2 pesate tse erano state sottostadiate 10 lesioni ( 25% ) ( tabella 4 )  . discussione nello studio del carcinoma gastrico la scelta diagnostica per lidentificazione e la stadiazione delle lesioni ampia ed 1070 table 2 t staging at histopathologic examination , ct and mr imaging . 
all values are expressed as numbers and percentages histopathological examination radiol med ( 2009 ) 114 : 10651079 ct , computed tomography ; mr , magnetic resonance tabella 2 grado di stadiazione delle lesioni attribuito da ciascuna metodica . 
moreover , the possibility of routinely using multiplanar reconstruction and volume - rendering techniques represents an additional advantage for the accurate evaluation of the gastric wall and vascular infiltration . mr imaging , if performed with state - of - the - art technique and technology , is a potentially innovative modality for the study of gastric lesions . 
la tc e , pi recentemente , la rm sono state proposte quali alternative non invasive e con elevata accuratezza diagnostica per stadiazione e follow - up [ 13 , 2527 ]  . 
le pi recenti apparecchiature tc permettono di acquisire immagini con voxel isotropici e spessore di strato sub - millimetrico in tempi brevissimi [ 28 ] ; inoltre la possibilit di utilizzare di routine le tecniche di ricostruzione multiplanare e di volume rendering costituisce un ulteriore vantaggio per unaccurata valutazione della parete gastrica e dellinfiltrazione vascolare . 
la rm , se effettuata con criteri tecnici e tecnologie allo stato dellarte , una metodica potenzialmente innovativa per lo studio delle lesioni gastriche : rispetto alla tc , la superiore risoluzione di contrasto ottenibile sulle apparecchiature di ultima generazione pu consentire una miglior differenziazione dei diversi strati della parete incrementando laccuratezza nella stadiazione delle lesioni in stadio precoce . 
the extent of wall infiltration is better evaluated on true - fisp ( c ) and tse ( d ) sequences rather than on contrast - enhanced vibe sequences ( e ) and ct images . 
non si osservano fenomeni infiltrativi a carico degli strati profondi della parete ( stadio t1 ) , n nelle immagini tc ( a , b ) , n nelle sequenze rm ( c - e )  . 
lestensione della lesione appare meglio valutabile nelle sequenze truefisp ( c ) e tse ( d ) piuttosto che nelle sequenze vibe ( e ) acquisite dopo somministrazione di mdc e nelle immagini tc . 
i reperti descritti sono stati confermati allesame istologico macro ( f ) e microscopico ( g )  . contrast resolution obtained with the latest - generation scanners may improve discrimination of the various wall layers , thus increasing staging accuracy in early lesions . 
the new devices have almost completely overcome the limitations due to long examination times , allowing for significant improvements in the study of abdominal organs and a diagnostic performance almost identical to that of ct in many gastrointestinal imaging applications [ 7 , 2932 ]  . 
furtheri limiti dovuti alla durata dellesame , consentendo un significativo miglioramento nello studio degli organi addominali e garantendo performance diagnostiche sostanzialmente sovrapponibili a quelle della tc in molte applicazioni di imaging gastrointestinale [ 7 , 2932 ]  . 
inoltre la diffusione delle tecniche di imaging parallelo [ 33 , 34 ] ha ulteriormente colmato il gap esistente tra le due metodiche riguardo alla risoluzione spaziale / temporale ed al rapporto segnale rumore delle immagini rm . 
in this case , the involvement of the deep layers of the gastric wall is better seen on ct images ( a , b ) : on mr images ( c - e ) the lesion appears to be involving the superficial layer only . infiltration of the perigastric fat tissue can be excluded with both techniques . 
2a - g lesione a tutto spessore della grande curvatura gastrica ( punta di freccia ) , senza coinvolgimento del tessuto adiposo periviscerale ( stadio t2 )  . in questo caso le immagini tc ( a , b ) dimostrano meglio il coinvolgimento degli strati profondi di parete : nelle acquisizioni rm ( c - e ) la lesione sembra infatti limitata ai soli strati superficiali . 
i reperti sono stati confermati allesame istologico macro ( f ) e microscopico ( g )  . more , diffusion of parallel imaging techniques [ 33 , 34 ] has bridged the gap between the two modalities with regard to spatial / temporal resolution and signal - to - noise ratio of mr images . 
relativamente ai risultati del nostro studio , necessario notare che , anche se sono state utilizzate apparecchiature allo stato dellarte , linclusione di numerose lesioni in stadio t1 particolarmente impegnative da identificare e differenziare ha radiol med ( 2009 ) 114 : 10651079 1073 fig . 
the extension of the tumour and the infiltration of both gastric wall and extraparietal fat are clearly evaluated on both ct ( a , b ) and mr ( c - e ) images . 
with regard to the results of our study , it should be noted that despite the use of state - of - theart devices , the inclusion of several t1 lesions which are particularly difficult to detect and discriminate led to very similar diagnostic values as those obtained in previous reports . 
this difference was determinato valori diagnostici sovrapponibili a quelli delle precedenti esperienze : valutando globalmente la performance delle due metodiche , la tc risultata leggermente superiore alla rm con una sensibilit dell82 , 5% ed una accuratezza diagnostica del 76 , 7% contro l80% ed il 74 , 4% . 
tuttavia , tale differenza non si rivelata statisticamente significativa : il dato dimostra come entrambe le metodiche , se adeguatamente utilizzate , permettano di ottenere risultati non solo adeguati alla richiesta clinica in termini di accuratezza diagnostica , ma anche altamente riproducibili . 
4a - d extensive tumour of the antropyloric passage ( arrowhead ) with diffuse infiltration into the perivisceral fat tissue and involvement of the superoanterior aspect of the pancreatic head ( arrow ) ( stage t4 )  . 
4a - d avanzata neoplasia della regione antro - pilorica ( punta di freccia ) con diffusa infiltrazione extraparietale e coinvolgimento della porzione superiore della regione cefalo - pancreatica ( freccia ) ( stadio t4 )  . 
sia nelle immagini tc ( a , b ) che nelle sequenze rm ( c , d ) la lesione appare chiaramente visualizzabile , con perdita del piano di clivaggio adiposo rispetto alla testa del pancreas . 
 not , however , statistically significant , implying that when used correctly , either technique is capable of providing results that are not only sufficiently accurate for the clinical purpose but also highly reproducible . 
in routine practice , accurate staging is the cornerstone of treatment planning . thus , in terms of clinical relevance , the significance of the ppv and accuracy of the two modalities in our study is noteworthy : both mr imaging and ct reached 100% ppv for t1 , t3 and t4 lesions ; in t2 lesions , instead , ct had 81.2% ppv , whereas mr imaging reached 78.5% , with no statistically significant difference between the two modalities . 
there were very small differences in favour of mr imaging in stage t1 and of ct in stage t2 , but the low prevalence of these cases in our study population and the small number of patients studied ( not sufficient for statistically significant evaluations ) do not allow for any scientifically sound conclusions to be drawn on this topic . 
however , on an observational basis , only valid within our small patient population , the limitation of ct partially consisted of suboptimal contrast resolution for the detection of focal wall alterations ( t1 )  . 
in such cases , mr quotidiana , laffidabilit nella stadiazione il presupposto fondamentale per la scelta terapeutica ; al fine della rilevanza clinica pertanto interessante notare la significativit del vpp e dellaccuratezza delle due metodiche evidenziate dal nostro studio : sia la rm che la tc hanno ottenuto un vpp del 100% per le lesioni di tipo t1 , t3 e t4 ; per le lesioni in stadio t2 invece la tc ha ottenuto un vpp dell81 , 2% mentre la rm del 78 , 5% , senza evidenza di differenze statisticamente significative tra le due metodiche . 
laccuratezza ha mostrato un costante incremento dallo stadio t1 allo stadio t4 per entrambe le metodiche ; si sono evidenziate delle minime differenze a favore della rm nello stadio t1 e della tc nello stadio t2 , ma la ridotta percentuale di tali casi sul totale della popolazione e lesiguit del campione stesso ( non sufficiente per valutazioni statisticamente significative ) non consentono di estrapolare considerazioni scientificamente valide a tale riguardo . 
su una base osservazionale , e pertanto valida unicamente nellambito della nostra ristretta popolazione , il limite della tc si parzialmente manifestato nella risoluzione di contrasto non ottimale per la discriminazione di focali alterazioni parietali ( t1 ) ; a tale riguardo la rm ha mostrato una miglior capacit di identificare il tessuto patologico , anche se questo beneficio stato ottenibile in un unico caso , in cui peraltro alla tc la scarsa distensione dellantro gastrico ha radiol med ( 2009 ) 114 : 10651079 1075 table 3 positive predictive value , diagnostic accuracy and sensitivity of computed tomography ( ct ) and magnetic resonance ( mr ) imaging in the evaluation of the t parameter . 
studies using in vivo [ 38 ] and , with more interesting results , in vitro experimental technologies [ 18 , 29 ] have shown mr imaging to have excellent potential for accurately depicting the gastric wall layers , thus facilitating the diagnosis and differentiation of superficial lesions . 
in some cases of t2 lesions understaged as t1 on mr imaging , the parietal signal alteration due to neoplastic infiltration had wrongly been attributed to perilesional oedema / inflammatory reaction , leading to incorrect staging . 
on the subject of the diagnostic performance of mr imaging , it is interesting to note that the shorter examination times made possible by state - of - theart equipment allowed lesions to be accurately staged , even in patients with locally advanced disease who were potentially unable to sustain long breath - holds or prolonged immobility . 
finally , both techniques showed a moderate tendency to understage t3 lesions : in three cases at ct and in two cases at mr imaging , infiltration into the perivisceral fat , later confirmed at histology , could not be demonstrated . 
on this subject , in addition to the diagnostic limitations of each technique , we also need to consider the psychological influence exerted by the risk of precluding surgical treatment in patients with cancer stages within the ulteriormente ridotto la possibilit di identificare la lesione . studi con tecnologie sperimentali in vivo [ 38 ] e , con risultati pi interessanti , in vitro [ 18 , 29 ] hanno evidenziato come la rm abbia uneccellente potenzialit di visualizzare accuratamente gli strati della parete gastrica , potendo rendere pi facile la diagnosi e la differenziazione delle lesioni superficiali . 
tale capacit deve tuttavia essere attentamente considerata in sede di refertazione anche quale possibile fonte di pitfalls : in alcuni casi di lesioni t2 sottostadiate alla rm come t1 , lalterazione di segnale della parete dovuta allinfiltrazione neoplastica era stata erroneamente attribuita ad edema / reazione flogistica perilesionale , determinando unerrata determinazione dellestensione della patologia . ancora riguardo alla performance diagnostica della rm , interessante notare come la contenuta durata degli esami , ottenuta grazie allimpiego di apparecchiature allo stato dellarte , abbia permesso di ottenere unaccurata stadiazione anche nei pazienti con patologia localmente avanzata e pertanto potenzialmente poco cooperanti nel mantenimento di lunghe apnee o prolungata immobilit . 
entrambe le metodiche hanno mostrato infine una modesta tendenza a sottostimare le lesioni t3 : in 3 casi alla tc ed in 2 casi alla rm non stato possibile dimostrare linfiltrazione del tessuto adiposo periviscerale successivamente confermato allesame istologico . 
relativamente a tale dato , oltre ai limiti diagnostici di ciascuna metodica , senza dubbio da tenere in conto linfluenza psicologica esercitata dal rischio di poter precludere trattamenti chirurgici in pazienti con stadiazioni nei cutoff del protocollo terapeutico t2 / t3 e dunque la potenziale tendenza a dichiarare come immediatamente operabili lesioni 1076 radiol med ( 2009 ) 114 : 10651079 fig . 
on ct images ( a , b ) , mainly due to incomplete distension of the stomach , the lesion was wrongly interpreted as a nonspecific scarring of the gastric wall . 
at mr imaging ( c - e ) , adequate distension of the stomach and particularly of the antrum allows identification of the lesion that seems confined to the superficial wall layer , especially on the contrast - enhanced vibe ( e ) images . 
allesame rm ( c - e ) , unadeguata distensione dello stomaco e soprattutto della regione antrale consente di evidenziare chiaramente la formazione polipoide che appare limitata allo strato superficiale della parete , soprattutto nelle sequenze vibe ottenute dopo somministrazione di mdc ( e )  . 
i reperti sono stati confermati tramite resezione endoscopica ( f ) ed esame istologico microscopico ( g )  . t2 / t3 cutoff for treatment , which could lead one to report as immediately operable locally advanced lesions that are instead eligible for neoadjuvant therapy . 
tuttavia , il ridotto numero di lesioni osservabili per ogni stadio patologico , e maggiormente in relazione allo stadio t1 ( 10% dei casi ) ed allo stadio t4 ( 10% dei casi ) , comporta una riduradiol med ( 2009 ) 114 : 10651079 1077 table 4 mr sequences vs . 
concordance in the evaluation of the t parameter histopathological examination w , pesata ; tse , turbo spin echo ; truefisp , true fast imaging with steady state precession ; ce - vibe , contrast enhanced volumetric interpolated breath hold examination tabella 4 sequenze rm vs reperti istopatologici . 
clearly , further studies on larger patient populations are required for a more reliable comparison of the roles of ct and mr imaging . in conclusion , our results confirm that ct is the modality of choice in gastric carcinoma staging . 
from a purely clinical point zione dellattendibilit delle misurazioni statistiche sui nostri dati : saranno ovviamente necessari ulteriori studi che coinvolgano un maggior numero di pazienti per poter confrontare con maggior attendibilit i rispettivi ruoli di tc ed rm . 
 in conclusione , i risultati del nostro studio confermano la tc come metodica di elezione per la stadiazione del carcinoma gastrico ; la rm pu tuttavia essere considerata unalternativa non solo fattibile , ma anche affidabile ed in grado di garantire una performance diagnostica soddisfacente nella stadiazione locale . 
da un punto di vista strettamente clinico , attualmente appare ancora per difficile 1078 radiol med ( 2009 ) 114 : 10651079 of view , mr imaging cannot , however , compete with ct : the higher costs , the greater difficulty achieving a technically adequate examination and , more importantly , the inability to perform comprehensive staging with evaluation of extra - abdominal lymph nodes and metastases are all very real limitations , well beyond possible considerations on the ability to detect and characterise local extent of disease . poter proporre la rm come metodica in competizione con la tc : il costo , la maggior difficolt nellesecuzione di un esame tecnicamente valido e , soprattutto , la sostanziale impossibilit di effettuare una stadiazione completa , comprensiva della valutazione linfonodale e metastatica in sede extra - addominale rappresentano limiti rigidamente realistici , ben aldil delle possibili considerazioni sulla capacit di poter identificare e caratterizzare la semplice estensione locale della patologia . 
fugazzola1 1vascular and interventional radiology , department of radiology , university of insubria , 21100 varese , italy 2department of vascular surgery , university of insubria , 21100 varese , italy correspondence to : d . 
all patients underwent intentional exclusion of the left subclavian artery and placement of a straight graft ; four patients underwent supra - aortic vessel transposition and four underwent carotid - carotid bypass in one case combined with carotid - subclavian bypass . 
in tutti i pazienti stata esclusa intenzionalmente la succlavia sinistra e posizionata unendoprotesi retta ; in 4 pazienti stata effettuata una trasposizione completa dei tronchi epiaortici mentre in altri 4 pazienti stato effettuato un by - pass carotidocarotideo , in un caso associato a by - pass carotidosucclavio . 
sono necessari ulteriori studi per verificare i risultati a medio e lungo termine . keywords aortic arch aneurysm aortic aneurysms endovascular treatment hybrid treatment parole chiave aneurisma arco aortico aneurismi aortici trattamento endovascolare trattamento ibrido radiol med ( 2009 ) 114 : 11301140 introduction introduzione 1131 open surgery is considered the treatment of choice for isolated aortic arch aneurysms , as it involves prosthetic replacement of the arch and thus represents a definitive treatment [ 1 ]  . 
the recently proposed endovascular approach [ 2 , 3 ] excludes the aneurysm from the systemic circulation by using an endograft but does not prevent disease progression . endovascular treatment of descending thoracic aortic aneurysms with endograft placement in patients at high surgical risk has become a well - established approach , thanks to its lower invasiveness [ 47 ]  . 
similarly , in selected patients at high surgical risk it is now possible to adopt a hybrid approach in isolated aortic arch aneurysms with inadequate neck [ 8 ]  . 
treatment of zone 0 , the most proximal , involves complete transposition of the supra - aortic vessels by means of an aortoinattualmente il trattamento chirurgico convenzionale la terapia di scelta per gli aneurismi isolati dellarco aortico , in quanto prevede la sostituzione protesica dellarco e quindi la definitiva risoluzione della malattia [ 1 ] ; il trattamento endovascolare , proposto recentemente [ 2 , 3 ] , esclude dal circolo sistemico la dilatazione aneurismatica mediante unendoprotesi , ma non impedisce la progressione della malattia . ormai ben consolidato lapproccio solo endovascolare mediante stent - graft degli aneurismi dellaorta toracica discendente in pazienti ad alto rischio chirurgico in relazione alla minore invasivit [ 47 ]  . 
il trattamento prevede dapprima un intervento chirurgico di trasposizione dei vasi epiaortici e successivamente , realizzandosi delle zone nuove di atterraggio , si procede al posizionamento di stent - graft con esclusione della sacca aneurismatica dal circolo sistemico [ 3 ]  . in relazione alla classificazione di criado - ishimaru ( fig . 1 ) [ 9 ] , larco dellaorta viene suddiviso in 3 zone di atterraggio a cui corrispondono interventi chirurgici differenti . il trattamento della zona 0 , la pi prossimale , prevede la trasposizione completa dei vasi epiaortici mediante un bypass aorto - anonima e aorto - carotideo sinistro con o senza by - pass carotido - succlavio . 
la zona 2 , pi distale , pu essere trattata anche solo per via endovascolare con esclusione intenzionale dellarteria succlavia di sinistra nei casi in cui ci siano gli estremi affinch si realizzi il furto della succlavia ; negli altri casi viene effettuato un by - pass carotido - succlavio . il radiologo gioca un ruolo essenziale nel planning della procedura in quanto identifica mediante imaging la zona sana di atterraggio prossimale che prevede approcci chirurgici differenti e inoltre valuta lindicazione alla esclusione intenzionale della succlavia in relazione alla possibilit di documentare lintegrit dei vasi epiaortici e del circolo intracranico . 
zone 2 , the most distal , may be treated with endovascular treatment alone , with intentional exclusion of the left subclavian artery in cases likely to develop subclavian steal syndrome . 
imaging is used to identify the healthy proximal landing zone , and thus determine the surgical approach , and to document the integrity of the supra - aortic vessels and intracranial circulation , thus providing the indication for intentional exclusion of the subclavian artery . 
in our experience , the radiologist also plays a fundamental role in endograft placement and in preventing and treating endoleaks . the aim of our study was to evaluate the results of the hybrid treatment and to highlight the role of the radiologist in treatment planning and follow - up . materials and methods from december 2000 to december 2006 , we selected 14 patients ( nine men and five women ; mean age 66.2 years , range 5685 ) with isolated aortic arch aneurysms ( mean diameter 62 mm ; range 5572 mm ) located in zone 0 ( n = 4 ) , zone 1 [ n = 6 , two with bovine aortic arch configuration ( fig . 2 ) ] and zone 2 ( n = 4 )  . 
complete transposition of the supraaortic trunks was performed in four patients , whereas a carotidcarotid bypass was done in another four , in one case combined with a carotidsubclavian bypass . 
planning involved assessment of the integrity and diameter of the landing zones and patency of the supra - aortic vessels and willis circulation ( to identify stenosis of the vertebral arteries or carotids or abnormalities of the intracranial circulation ) , a search for possible areas of cerebral ischaemia and evaluation of the peripheral vascular point of access . 
stata effettuata una trasposizione completa dei tronchi epiaortici in 4 pazienti , mentre in altri 4 pazienti stato confezionato un by - pass carotido - carotideo , in un caso associato a bypass carotido - succlavio . 
i pazienti presentavano le seguenti comorbilit : ipertensione ( 8 casi ) ; cardiomiopatia ischemica ( 8 casi ) ; broncopneumopatia cronica ostruttiva ( 6 casi ) ; insufficienza renale cronica ( 4 casi ) e diabete ( 5 casi )  . il planning pre - procedura stato effettuato mediante angio - tomografia computerizzata multistrato ( angio - tcms ) ( lightspeedplus , ge , milwaukee , usa ; aquilion 64 , toshiba , tokyo , giappone ) con ricostruzioni multiplanari ( mpr ) e 3d per la valutazione dellintegrit e dei diametri della zona di atterraggio , della perviet dei vasi epiaortici e del circolo di willis ( per lidentificazione di stenosi a carico delle arterie vertebrali , carotidi o anomalie del circolo intra - cranico ) e per la ricerca di eventuali aree ischemiche cerebrali , nonch valutazione del sito daccesso vascolare periferico . 
solo in casi selezionati ( placche calcifiche in arterie vertebrali con impossibilit di valutazione della riduzione in calibro ) stata effettuata langiografia per lo studio in particolare dei vasi epiaortici e del circolo intracranico e successivamente , mediante simultaneo approccio trans - omerale , con pallone occlusore allorigine dellarteria succlavia di sinistra , stato effettuato un test con cateterismo selettivo trans - femorale dellarteria vertebrale di destra per verificare linversione di flusso dellarteria vertebrale sinistra in succlavia [ 10 ]  . sono stati considerati criteri di inclusione : pazienti senza pregresse aree ischemiche cerebrali e con regolare perviet del circolo di willis ; eventuali stenosi delle arterie carotidi sono state corrette prima del posizionamento della protesi ( 1 caso )  . 
nella selezione dei pazienti sono stati considerati criteri di esclusione locclusione intenzionale dellarteria succlavia di sinistra , i pazienti con arteria lusoria , con fistole dialitiche , quelli in cui larteria mammaria interna era stata utilizzata per un by - pass coronarico e in tutti i casi di steno - occlusione delle arterie vertebrali in cui non vi era indicazione alla ricanalizzazione endovascolare . 
a tutti i pazienti stata somministrata una profilassi antibiotica a breve termine ( vancomicina 2 g ) , associata alla somministrazione di 5000 ui di eparina , e quindi stato realizzato il cateterismo trans - omerale sinistro per la valutazione angiografica dellarco nelle prime fasi della procedura endovascolare . successivamente stata posizionata lendoprotesi radiol med ( 2009 ) 114 : 11301140 1133 fig 2a - c aortic arch aneurysm in a patient with bovine aortic arch configuration ( type iii )  . 
a intraoperative digital subtraction angiography ( dsa ) : large aortic arch aneurysm in a patient with left common carotid artery originating from the innominate artery ( type iii aortic arch )  . 
il controllo agiografico al termine della procedura dimostra il furto dellarteria succlavia , sinistra in assenza di endoleak di tipo ii ad origine dallarteria succlavia che pertanto non viene occlusa . intracranial circulation and subsequently , with simultaneous transhumeral approach and selective transfemoral catheterisation of the right vertebral artery , a balloon occlusion test with balloon positioned at the origin of the left subclavian artery to verify flow inversion from the left vertebral artery into the subclavian artery [ 10 ]  . inclusion criteria were patients without previous areas of cerebral ischaemia and with patenty of willis circulation . any carotid artery stenoses were repaired before endograft placement ( n = 1 )  . 
exclusion criteria included intentional occlusion of the left subclavian artery , patients with lusory arteries , dialysis fistulas , coronary bypass with internal mammary artery and all cases of stenosis / occlusion of the vertebral arteries without an indication for endovascular ( excluder , gore , flagstaff , az , usa , in 5 casi ; talent , medtronic , santa rosa , ca , usa , in 5 casi ; zenith , cook , bloomington , in , usa , in 4 casi ) mediante monitoraggio fluoroscopico in proiezione obliqua anteriore sinistra , con un oversizing del 15%20% . 
in 6 casi stata coperta intenzionalmente larteria succlavia di sinistra e solo in 3 casi stata embolizzata mediante posizionamento , per via transomerale , di vascular plug ( amplatzer , aga medical corporation , plymounth , mn , usa ) ( fig . 3d ) , per la presenza di un endoleak di tipo ii documentato al controllo angiografico post - procedura . 
all patients underwent short - term antibiotic prophylaxis ( vancomycin 2 g ) combined with 5 , 000 iu heparin , followed by left transhumeral catheterisation for angiographic assessment of the aortic arch during the initial phases of the endovascular procedure . the endograft [ excluder , gore , flagstaff , az , usa ( n = 5 ) ; talent , medtronic , santa rosa , ca , usa ( n = 5 ) ; zenith , cook , bloomington , in , usa ( n = 4 ) ] was subsequently placed under fluoroscopic guidance in the left anterior oblique projection , with 15%20% oversizing . 
follow - up was performed by msct angiography at 1 , 3 , 6 and 12 months , and yearly thereafter . results immediate technical success ( exclusion of the sac from the systemic circulation ) was achieved in all cases . 
three patients remained in the intensive care unit for 2 , 15 and 33 days , respectively . we had four cases of cerebral ischaemia ( three transient ischaemic attacks and one stroke ) related to zone - 0 procedures in two cases and zone - 1 procedures in the other two . postprocedural complications included one case of pneumonia and one of atrial fibrillation , both of which were treated medically . 
mean hospital stay was 12 days ( 10 days for zone 0 and 6.5 days for zone 2 )  . during a mean follow - up of 21 months ( range 1248 months ) , two patients died ( one of myocardial infarction and one of respiratory failure ) 26 and 36 months after the procedure , respectively . 
il followup stato espletato mediante angio - tcms a 1 , 3 , 6 e 12 mesi e successivamente annualmente . risultati stato ottenuto un successo tecnico immediato ( esclusione della sacca dalla circolazione sistemica ) in tutti i casi . 
tre pazienti sono stati ricoverati in terapia intensiva rispettivamente per 2 , 15 , 33 giorni . abbiamo osservato 4 ischemie cerebrali ( 3 ischemie cerebrali transitorie [ tia ] e 1 stroke ) , in 2 casi di ancoraggio della protesi in zona 0 e in 2 casi di ancoraggio nella zona 1 . 
lospedalizzazione media stata di 12 giorni ( 10 giorni per zona 0 e 6 , 5 per zona 2 )  . durante un follow - up medio di 21 mesi ( range 1248 mesi ) 2 pazienti sono deceduti ( 1 per infarto miocardico e 1 per insufficienza respiratoria , rispettivamente 26 e 36 mesi dopo le procedure )  . 
 [ 11 ] riportarono la prima esperienza di esclusione endovascolare di un aneurisma dellaorta addominale ( aaa ) ; sfortunatamente questo lavoro rimase a lungo sconosciuto in quanto pubblicato in lingua russa . 
3a - f posttraumatic chronic aortic arch pseudoaneurysa , b computed tomography angiography ( cta ) [ a : sagittal maximum intensity projection ( mip ) ; b : 3d volume rendering ( vr ) ] : chronic bilobate posttraumatic pseudoaneurysm with marginal calcified cap proximal to the origin of the left subclavian artery . 
d intraoperative dsa : endograft placement and occlusion of the origin of the left subclavian artery with vascular plug due to type - ii endoleak , with initial reverse flow of the vertebral artery ( black arrows ) to the mediodistal subclavian artery ( white arrows )  . 
d angiografia intra - operatoria : posizionamento dellendoprotesi e occlusione dellemergenza dellarteria succlavia mediante vascular plug per endoleak di tipo ii , con iniziale inversione di flusso dellarteria vertebrale ( frecce nere ) in arteria succlavia medio - distale ( freccie bianche )  . 
visibile un guscio calcifico lungo la convessit ( teste di frecce ) e la concavit ( freccia ) dellarco aortico . the other , from the innominate artery , by coil embolisation . in the other cases , msct angiography demonstrated the exclusion of the aneurysmal sac with no migration of the endografts from the landing zone . stanford [ 13 ] tratt 103 pazienti con aneurismi dellaorta toracica ; in 8 di questi pazienti lendoprotesi fu posizionata a valle dellarteria succlavia sinistra . 
the 3d vr reconstruction well depicts the short aneurysmal neck and the bovine aortic arch configuration ( type ii : arrows ) , an indication for transposition of the supra - aortic vessels . 
la ricostruzione 3d vr ben evidenza la presenza di breve colletto aneurismatico , la configurazione bovina dellarco ( tipo ii , frecce ) quindi vi indicazione alla trasposizione dei vasi epiaortici . 
trasposizione dei vasi epiaortici con by - pass aorto - anonima , aorto - carotideo ( freccia ) con legatura dei vasi a valle , del posizionamento di cuffia protesica ( testa di frecce ) e del furto dellarteria succlavia ( frecce )  . discussion just over 20 years have passed since balko et al . 
 [ 11 ] first described the endovascular exclusion of an abdominal aortic aneurysm ( aaa ) in a report that remained largely unknown , as it was written in russian . 
the need to develop an endograft large enough for the ascending aorta decidedly larger than the abdominal aorta that would not give rise to problems at the transfemoral access point [ 14 ]  . 
another hindrance to the use of this approach in aortic arch and ascending aortic aneurysms was the increased risk of endograft migration due to high blood pressure , mechanical stress produced by the heart and possible progression of aneurysmal disease . further problems may arise in relation to the different landing zones on the aorta , the angle between the aortic arch and the descending aorta , which is not well suited to the stiffness of endografts , and the anatomical peculiarity of the unendoprotesi di calibro maggiore , adeguata alle dimensioni dellaorta ascendente , decisamente maggiore di quelle dellaorta addominale , ma allo stesso tempo che non creasse difficolt sul sito di accesso trans - femorale [ 14 ] ; importante stata la creazione di un puntale protesico di ridotte dimensioni , atraumatico , che non danneggiasse la valvola aortica durante il posizionamento della protesi . 
un ulteriore freno allutilizzo di tale approccio nel trattamento degli aneurismi dellarco e dellaorta ascendente stato il maggiore rischio di sposizionamento dellendoprotesi a causa dellelevata pressione del flusso sanguigno , delle sollecitazioni meccaniche del cuore e delleventuale progressione della malattia aneurismatica . 
infine , altre difficolt possono derivare dalle diverse zone di atterraggio sullaorta , dallangolazione tra larco aortico e laorta discendente che mal si adatta alla rigidit delle protesi impiegate , e dallanatomia peculiare dellarco aortico dalla cui convessit nascono , a poca distanza luno dallaltro , i vasi epiaortici [ 14 ]  . 
queste difficolt di carattere tecnico , sono state in parte superate mediante lintroduzione di stent - graft di seconda generazione , ben pi flessibili di quelli fino ad allora impiegati , in grado di adattarsi meglio alla curvatura dellarco e dotati inoltre di efficaci sistemi di fissaggio ed ancoraggio [ 14 ]  . radiol med ( 2009 ) 114 : 11301140 1137 fig . 
b , c superselective dsa of the thyrocervical trunk : leakage of contrast material into the aneurysmal sac ( b : arrow ) and treatment with glue embolisation ( c )  . 
perviet dellendoprotesi in assenza di endoleak e riduzione dimensionale della sacca aneurismatica . 1138 radiol med ( 2009 ) 114 : 11301140 aortic arch , with the supra - aortic vessels arising at short intervals along its convex surface [ 14 ]  . 
the concavity of the aortic arch and emergence of the supra - aortic vessels from its convex surface make it difficult to seal this portion of the aorta with an endogra these technical difficulties have been partially overcome by second - generation endografts , which are much more flexible than the earlier devices and thus able to adapt better to the curvature of the arch , as well as being equipped with effective fixing and landing systems [ 14 ]  . in addition , during the planning phase , the use of msct angiography with its high spatial and temporal resolution and the possibility of performing electrocardiography - gated examinations can increase the diagnostic accuracy of msct by enabling the attenuation or elimination of cardiac motion artefacts , especially at the level of the ascending aorta and supra - aortic vessels , with 3d volume rendering ( vr ) , multiplanar reconstructions ( mpr ) and 3d virtual endoscopy ( ve )  . the combination of technical advances and technological developments in thoracic endografting allows endovascular treatment in a large number of patients affected by major aortic lesions and several comorbidities who would otherwise have no other alternative [ 8 ]  . 
according to the criado / ishimaru classification [ 9 ] , zone 0 of the aortic arch requires complete transposition of the supra - aortic vessels through aortoinnominate and left aortocarotid bypass , whereas zone 1 requires carotid - carotid and , if necessary , carotidsubclavian bypass [ 18 ]  . 
zone 2 may undergo endovascular treatment alone , with intentional exclusion of the left subclavian artery in cases likely to develop subclavian steal syndrome [ 18 ]  . hybrid treatment potentially reduces procedural morbidity and mortality and may thus represent the only therapeutic choice for a subset of patients at high surgical risk . 
however , manipulation of supra - aortic and aortic arch vessels , particularly in the presence of multiple atheromatous plaques , is not devoid of complications such as embolism and consequent cerebral ischaemia . 
in order to avoid ischaemic events , doubtful cases require a detailed angiographic study of the supra - aortic vessels followed by an occlusion test of the left subclavian artery and in aggiunta , lesecuzione nel planning di unangiotcms , grazie allelevata risoluzione spaziale e temporale , nonch alla possibilit in casi selezionati , di esecuzione di esami con sincronizzazione cardiaca ( ecg - gated ) permette di incrementare mediante ricostruzioni 3d volume rendering ( vr ) , ricostruzioni multiplanari ( mpr ) e 3d virtual endoscopy ( ve ) , le potenzialit diagnostiche della tcms , attenuando o eliminando i possibili artefatti da pulsatilit cardiaca , specie in corrispondenza dellaorta ascendente e sui tronchi sovra - aortici . quindi la combinazione tra avanzamenti tecnici e sviluppi tecnologici nellendo - grafting toracico permette attualmente di trattare per via endovascolare un numero di pazienti con importati lesioni aortiche e numerose comorbilit che altrimenti non avrebbero nessuna altra alternativa [ 8 ]  . 
il trattamento chirurgico convenzionale , prevedendo infatti larresto di circolo e la circolazione extracorporea , presenta degli indici di mortalit compresa tra 8 , 5% e 25 , 2% [ 1517 ] con danno neurologico permanente tra 4 , 2% e 12 , 8% [ 15 ]  . la suddivisione in zone di atterraggio in relazione alla necessit di interventi chirurgici differenti stata confermata nel corso del primo summit internazionale di thoracic aortic endografting a tokio nel 2001 [ 9 ]  . 
in accordo con la classificazione di criado - ishimaru [ 9 ] la zona 0 dellarco prevede la trasposizione completa dei vasi epiaortici mediante un by - pass aorto - anonima e aorto - carotideo sinistro ; la zona 1 prevede il confezionamento di un by - pass carotido - carotideo ed eventuale carotido - succlavio [ 18 ]  . 
la zona 2 pu essere tratta anche solo per via endovascolare con esclusione intenzionale dellarteria succlavia di sinistra nei casi in cui si possa realizzare il furto della succlavia [ 18 ]  . il trattamento ibrido potenzialmente riduce la morbilit e la mortalit costituendo , in alcuni pazienti ad alto rischio chirurgico , lunica possibilit terapeutica . 
al fine di evitare eventi ischemici , nei casi dubbi necessario eseguire uno studio di particolare angiografico dei vasi epiaortici con test di occlusione dellarteria succlavia di sinistra e valutazione dellinversione del flusso . 
 [ 19 ] dopo il posizionamento di endoprotesi tipo talent in zona 2 . il follow - up a lungo termine di queste procedure radiol med ( 2009 ) 114 : 11301140 1139 assessment of flow inversion . 
 [ 19 ] after positioning a talent endograft in zone 2 . long - term follow - up of these procedures is still inadequate , and published studies have reported on small patient populations [ 8 ]  . 
for this reason , some authors [ 20 ] have suggested surgical bending of the ascending aorta near landing zone 0 to ensure lasting fixation and sealing of the endogra although bending the proximal neck clearly increases the invasiveness of the procedure , it is thought to prevent endograft migration . 
in fact , in the case of complete transposition of the supra - aortic vessels , endoleak prevention requires either surgical ligation of the origin of the vessels [ 21 ] or subsequent embolisation in the event that a type - ii endoleak occurs [ 8 ]  . in our experience , all type - ii endoleaks were treated with endovascular embolisation owing to our conviction that we should limit overall procedure time in consideration of the type of patients selected . 
furthermore , with regard to the intentional exclusion of the left subclavian artery , our experience shows occlusion at the origin is only indicated when postprocedural dsa demonstrates a type - ii endoleak , a rare occurrence when the subclavian artery is not involved by the aneurys it is , however , possible to perform preliminary endovascular occlusion , although this might turn out to be useless due to increased flow towards the upper limb . limitato , sono state pubblicate solo casistiche numericamente ridotte [ 8 ] ; inoltre la perviet a lungo termine di questi bypass non stata ancora verificata . 
da qui alcuni autori [ 20 ] hanno proposto il bending chirurgico dellaorta ascendente in corrispondenza dellatterraggio in zona 0 , per garantire un fissaggio duraturo e per poter sigillare in maniera ermetica lendoprotesi . 
infatti , nei casi di trasposizione completa dei tronchi epiaortici la prevenzione dellendoleak richiede o la legatura chirurgica dellorigine degli stessi [ 21 ] o lembolizzazione in un secondo tempo se si realizza lendoleak di tipo ii [ 8 ]  . nella nostra esperienza gli endoleak di tipo ii sono stati trattati tutti per via endovascolare mediante embolizzazione per convinzione , anche chirurgica , di non eccedere sul tempo operatorio complessivo in relazione al tipo di pazienti selezionati , quindi di concentrare un primo tempo solo dedicato alla esclusione della sacca dalla circolazione sistemica e il successivo trattamento dei rifornimenti della sacca in ambiente radiologico mediante angiografo fisso . inoltre nella esclusione intenzionale dellarteria succlavia sinistra , nella nostra esperienza indicata locclusione allorigine solo nei casi in cui il controllo angiografico post - procedura dimostri lendoleak di tipo ii : fatto poco frequente se non direttamente coinvolta dallaneurisma . 
endovascular exclusion of isolated aortic arch aneurysms , in the small number of cases treated , allowed us to control the in conclusione , il trattamento ibrido una valida alternativa alla chirurgia convenzionale in pazienti ad alto rischio chirurgico per la minore invasivit con tassi di mortalit inferiori . 
questa tecnica ha un basso tasso di mortalit peri - operatoria , ma un tasso di complicanze non indifferente da insulto ischemico cerebrale , anche se pu essere nella maggior parte dei casi di tipo transitorio . 
 di fondamentale importanza il planning della procedura dove gioca un ruolo determinante il radiologo per la valutazione del calibro vascolare del sito daccesso , per la scelta del device pi idoneo allesclusione della sacca aneurismatica , per stabilire il tipo di intervento chirurgico in relazione alla scelta della zona di atterraggio e per dare gli estremi per la realizzazione dellinversione del flusso in arteria vertebrale di sinistra in quanto questo evita il bypass carotido - succlavio . 
renieri piccin nuova libraria s.p.a. , padova 2009 isbn 978 - 88 - 299 - 2002 - 0 published online : 9 october 2009 springer - verlag 2009 these soft - bound books complement one another and can be considered a short and simple crib for the much larger work , summa teologica ( deformit congenite dello scheletro ) published some years ago by canepa . their aim is to present , most of all to clinical genetists , paediatricans and orthopaedics , clues and bases for observing and diagnosing congenital bone diseases and congenital deformities of the skeleton . atlante disegnato lists 193 dysplasias , syndromes and chromosomal diseases . 
each page describes two conditions . at glance , in half a page each , one will find drawings extracted by deformit congenite dello scheletro , plus in the shortest possible text a listing ( a check - list one could call it ) of the main and most important diagnostic features of the described condition and type of genetic transmission , viability and main phenotypic expression . 
at the end of the book one will find some pages listing genetic features and loci of the single conditions ( heredity , mim , locus and gene involved )  . atlante elementare in 95 pages and 10 sub - headings addresses what one should know about the genetics clinical genetics of congenital deformities of the skeleton . 
as stressed in their short introduction by the authors , the book addresses geneticists and biologists in order to remind the firsts that clinical genetics is not an out - dated subject overrun by molecular genetics ; and to remind the second group that biology prevails over medicine in their study curricula . 
at the end of this book the listing of loci and genes is shorter than in the previous one ; actually here one will find a subject index . once one has read or perused the atlante elementare he / she will better understand the atlante disegnato and appreciate the research and effort put into the preparation and lay - out of both books . 
 scopo degli autori e dei volumi , di presentare a genetisti clinici , pediatri , ed ortopedici quali sono le tracce e le basi sulle quali sospettare e diagnosticare le malattie congenite dellosso e le deformit congenite dello scheletro . 
in mezza pagina , con un solo sguardo , si ritovano disegni con i tratti caratteristici dellaffezione , ed un elenco sintetico ( tipo check - list dei piloti ) delle pi importanti e significative caratteristiche diagnostiche della stessa , le modalit di trasmissione genetica , le possibilit di vita o non nonch il tipo di genotipo . 
alla fine del volume alcune pagine elencano le caratterisctiche genetiche ed i loci delle single affezioni ( ereditariet , mim , locus e gene interessato )  . latlante elementare descrive in 95 pagine e 10 capitoli ci che si dovrebbe sapere sulla genetica genetica clinica delle deformit congenite dello scheletro . 
come anche ben specificato , nella breve introduzione , da parte degli autori il volume ha come obiettivo di sensibilizzare i genetisti ed anche i biologi : i primi perch ricordino che la genetica clinica non qualche cosa da dimenticare a fronte della genetica molecolare ; i secondi perch ricordino che la biologia prevale sulla medicina nel loro corso di studio . 
 dopo avere letto o sfogliato latlante elementare il lettore potr meglio comprendere latlante disegnato ed apprezzare quanto di sforzo e ricerca stato profuso nella preparazione ed impostazione di entrambi i volumi . 
dato anche il prezzo modesto ( importante di questi tempi ) questi volumi dovrebbero avere una ampia diffusione nel campo di coloro che si occupano di bambini portatori di displasie o radiol med ( 2009 ) 114 : 11841185 1185 even though these conditions may be deemed to be in a world apart , both for diagnosis and therapy , due to their rarity they should not be overlooked or archived in some obscure corner of the mind . 
sensibilit , specificit , valore predittivo positivo e negativo per lus sono stati rispettivamente 70 , 2% , 59 , 2% , 74 , 7% e 53 , 7% ; per la ceus sono stati 96 , 4% , 98% , 98 , 8% e 94 , 1% . 
la metodica riconosce il sanguinamento attivo e le lesioni vascolari , evita lesposizione a radiazioni ionizzanti ed utile nel monitoraggio dei pazienti con trattamento conservativo . keywords ultrasonography contrast agent abdominal trauma parole chiave ecografia mezzo di contrasto trauma addominale radiol med ( 2009 ) 114 : 10801093 introduction introduzione 1081 trauma represents the most frequent cause of death in the population younger than 40 years [ 1 ] , and there is evidence that a prompt diagnosis can prevent severe consequences for the patient . 
because of this , in europe and in many centres in the usa , ultrasonography ( us ) , a modality that can be performed at the bedside without suspending first - aid procedures , has become the first - line investigation in evaluating abdominal trauma [ 510 ]  . 
emergency us performed to detect haemoperitoneum is termed focused assessment with sonography for trauma ( fast ) and has 81%94% sensitivity , 88%100% specificity and 86%98% diagnostic accuracy [ 1116 ]  . 
whereas it is generally recognised that us has a key role in unstable patients [ 20 ] , its use in stable patients remains controversial owing to its inability to exclude abdominal organ lesions , even in the presence of negative findings , with the result that patients need to undergo contrast - enhanced computed tomography ( ct )  . 
 contrast - enhanced us ( ceus ) relies on the use of contrast agents containing microbubbles filled with a gas other than air , which resonate at a low acoustic pressure emitting a specific signal . 
these real - time images allow identification of any solid organ lesion in a manner similar to ct but with the advantage of continuous exploration . initially used in the study of focal hepatic lesions , ceus was later successfully used to investigate a variety of conditions in other anatomical regions . 
one application is evaluating patients with blunt abdominal trauma , a field in which its success in recognising traumatic solid organ lesions has suggested its use in the triage of abdominal trauma [ 2125 ]  . the aim of this paper is to present our experience with the use of ceus in patients with blunt abdominal trauma and to assess its impact on clinical practice in the emergency department . materials and methods the study was conducted on a cohort of patients with blunt abdominal trauma in a university hospital featuring a level ii emergency department but with no trauma centre . between 2004 and 2008 , 1 , 462 patients underwent fast examination according to a shared protocol to detect il trauma costituisce la causa pi frequente di morte nella popolazione di et inferiore ai 40 anni [ 1 ]  . 
per tale motivo , in europa e in molti centri degli usa , lecografia ( us ) , eseguibile immediatamente al letto del paziente senza interrompere le manovre di soccorso , costituisce la metodica di primo approccio nella valutazione del trauma addominale [ 510 ]  . 
lus in urgenza , finalizzata alla ricerca dellemoperitoneo , chiamata focused assessment with sonography for trauma ( fast ) e ha una sensibilit dell81%94% , una specificit dell88%100% e unaccuratezza diagnostica dell86%98% [ 1116 ]  . 
il suo limite pi importante rappresentato dalla scarsa sensibilit , che varia tra il 41% e il 44% [ 1719 ] , nel riconoscimento diretto delle lesioni degli organi solidi delladdome . mentre lus ha un ruolo sicuramente riconosciuto nel paziente instabile [ 20 ] , la sua applicazione resta a tuttoggi pi discutibile nel paziente stabile , nel quale anche se negativa non in grado di escludere la presenza di lesioni degli organi addominali e quindi non permette di evitare lesecuzione di una tc con mezzo di contrasto ( mdc )  . lecografia con mezzo di contrasto , definita ceus ( dallinglese contrast - enhanced ultrasononography ) , si basa sullimpiego di mezzi di contrasto costituiti da microbolle ripiene di un gas diverso dallaria capaci di risuonare a bassa pressione acustica e di emettere un segnale specifico . 
con la tecnica a basso indice meccanico possibile ottenere in real time immagini quasi esclusivamente dipendenti dal segnale delle microbolle , identificando le eventuali lesioni degli organi solidi , in un modo del tutto simile a quello della tc , ma con il vantaggio dellesplorazione continua . 
tra queste la valutazione dei pazienti con trauma chiuso delladdome , campo in cui si dimostrata molto efficace nel riconoscimento delle lesioni traumatiche degli organi solidi al punto da venire proposta nel triage del trauma addominale [ 2125 ]  . 
 lo scopo del presente studio riportare la nostra esperienza nellimpiego della ceus nel paziente con trauma chiuso delladdome e di valutarne leffetto sulla pratica clinica in emergenza . 1082 radiol med ( 2009 ) 114 : 10801093 table 1 causes of traumatic lesion in 1462 patients including in the study materiali e metodi cause n . 
of this cohort , 133 consecutive patients ( 99 male and 34 female , mean age 40.2 years ) with a suspicion of abdominal lesion justified by accident dynamics ( direct impact , deceleration impact or impact with blunt object with a small surface ) or positive fast for free abdominal fluid and in stable haemodynamic conditions ( pulse pressure 90 mmhg , heart rate < 100 bpm , respiratory rate < 20 respirations per minute ) underwent ceus followed by contrast - enhanced ct . us scans were performed by experienced physicians ( radiologists or emergency physicians ) , whereas ct was performed by a second radiologist within 1 h after the us and ceus exams . 
the study was approved by the hospital ethics committee ( clinical study n1 / 2004 / o )  . patients were informed of the type of examination and study protocol , and consent was obtained from either the patients , or from their relatives in the case of minors . ultrasonography and contrast - enhanced ultrasonography examinations were performed with an atl 5000 hdi scanner , version 10.4 equipped with a 2 - 5 - mhz convexarray probe with a dedicated low mechanical index software for second - generation contrast agents . 
us was performed to search for haemoperitoneum with scans of the right upper quadrant , including the hepatorenal fossa and pleural space ; of the left upper quadrant , including the perisplenic region and pleural space ; of the epigastrium , including the pericardiac space ; of the right and left paracolic gutters ; and of the pelvis . solid abdominal organs were assessed for the presence of lesions in all patients . 
us was considered positive in the lo studio stato condotto in un ospedale universitario sede di un dipartimento di emergenza di 2 livello , ma non trauma center , su una coorte di pazienti con trauma chiuso delladdome . 
nel periodo 2004 - 2008 sono stati valutati 1462 pazienti , che sono stati sottoposti , secondo un protocollo condiviso , ad esame fast nel corso della valutazione primaria allinterno della sala urgenze . 
di questa coorte , 133 pazienti consecutivi ( 99 maschi e 34 femmine , di et media di 40 , 2 anni ) , con sospetta lesione addominale per la dinamica dellevento ( impatto diretto , da decelerazione o da corpo contundente di piccola superficie ) o con fast positiva per versamento addominale , in condizioni di stabilit emodinamica ( pressione sistolica 90 mmhg , frequenza cardiaca < 100 bpm , frequenza respiratoria > 20 respirazioni al minuto ) , sono stati sottoposti a ceus seguita da tc con mdc . gli esami ecografici sono stati eseguiti da medici dedicati ( radiologo o medico di pronto soccorso ) , mentre la tc stata eseguita da un secondo radiologo entro 1 ora dallesame us e ceus . 
i pazienti sono stati informati del tipo di indagine e del protocollo di studio , e il consenso stato ottenuto dal paziente o dai familiari presenti in caso di minori . ecografia ed ecografia con mezzo di contrasto gli esami sono stati eseguiti con un ecografo atl 5000 hdi , versione 10.4 , equipaggiato con sonda convex da 25 mhz e dotato di specifico software a basso indice meccanico per limpiego dei mezzi di contrasto di 2 generazione . stato utilizzato limaging armonico per massimizzare le performance diagnostiche dellus basale . 
lus stata effettuata per la ricerca dellemoperitoneo con scansioni del quadrante superiore destro , inclusa la fossa epatorenale e lo spazio pleurico ; del quadrante superiore sinistro , inclusa la regione perisplenica e lo spazio pleurico ; dellepigastrio , incluso lo spazio pericardico ; delle docce paracoliche destra e sinistra ; della pelvi . 
lus stata considerata positiva in presenza di versamento peritoneale o alterazione dellecostruttura parenchimale compatibile con una lesione traumatica . la ceus stata eseguita immediatamente dopo lus basale secondo un protocollo standardizzato nel quale lagente ecocontrastografico stato iniettato in due dosi di 2 , 4 ml per studiare gli organi solidi del quadrante superiore destro ( rene destro , fegato e pancreas ) e superiore sinistro ( rene sinistro e milza )  . 
tale procedura consente la radiol med ( 2009 ) 114 : 10801093 1083 presence of peritoneal effusion or changes to parenchymal echostructure consistent with a traumatic lesion . ceus was performed immediately after baseline us . 
a standard protocol was used consisting of the injection of two 2.4 - ml doses of contrast agent to study the solid organs in the right upper quadrant ( right kidney , liver and pancreas ) and left upper quadrant ( left kidney and spleen )  . 
this procedure allows evaluation of solid abdominal organs during the most favourable vascular phase for the detection of traumatic lesions . on us , lesions were recognised as a hypoor hyperechoic alteration within the organ being studied . 
passage of microbubbles outside a lacerated organ was defined as active bleeding . ct was performed within 1 h after ceus with and without nonionic contrast agent during the venous phase . 
in the presence of collections , a late - phase study at 315 min was performed to identify any active bleeding or urinoma . examination results were stored in digital form and subsequently assessed by two radiologists who graded the lesions on the basis of the organ injury scale of the american association for the surgery of trauma ( aast ) [ 26 ]  . statistical analysis for the purposes of statistical analysis , us and ceus were considered positive in the presence of a parenchymal change related to a traumatic lesion . 
the positive and negative lr were subsequently entered into the fagan nomogram in order to calculate , starting from the pre - test probability ( 63.2% prevalence in this study ) , the positive and negative post - test probability of disease . us and ceus exams were evaluated by two operators blinded to the final result , who defined the concordance of the two techniques compared with the standard of reference ( ct )  . valutazione degli organi solidi delladdome nella fase vascolare pi favorevole per lidentificazione delle possibili lesioni traumatiche . 
alla ceus la lesione traumatica stata descritta come un difetto di perfusione nel contesto dellorgano caratterizzato da una ipoecogenicit con limiti sfumati o ben definiti , con o senza interruzione del profilo dellorgano . 
in presenza di raccolte stato effettuato uno studio in fase tardiva , a 315 minuti , per evidenziare un eventuale sanguinamento attivo o un urinoma . gli esami , archiviati su supporto digitale , sono stati successivamente valutati da due radiologi e le lesioni graduate sulla base dellorgan injury scale of the american association for the surgery of trauma ( aast ) [ 26 ]  . analisi statistica per lanalisi statistica , us e ceus sono state considerate positive in presenza di unalterazione parenchimale riferibile ad una lesione traumatica . 
i valori di sensibilit , specificit , valore predittivo positivo e negativo , il rapporto di verosimiglianza ( likehood ratio , lr ) positivo e negativo , ed il numero necessario per la diagnosi ( number needed to diagnosis , nnd , cio il numero medio di pazienti da sottoporre al test in esame per diagnosticare correttamente la patologia in oggetto ) , tutti con il loro intervallo di confidenza al 95% ( ci 95% ) per us e ceus rispetto alla tc sono stati calcolati utilizzando i seguenti calcolatori on line [ 27 , 28 ]  . 
 gli esami us e ceus sono stati successivamente valutati da due operatori ciechi sul risultato finale , che hanno definito la concordanza tra le due metodiche rispetto alla metodica di riferimento ( tc )  . 
us identified free fluid or altered parenchymal echostructure in 59 of the 84 patients with lesions on ct and free fluid in 20 of the 49 patients without lesions on ct . 
la diagnosi definitiva di sede della lesione traumatica stata di frattura splenica ( 48 pazienti ) , epatica ( 21 pazienti ) , rene o surrene ( 13 pazienti ) e pancreas ( 2 pazienti ) ( tabella 2 )  . 
lus ha identificato versamento libero o alterazione dellecostruttura parenchimale in 59 degli 84 pazienti con lesioni alla tc , e versamento libero in 20 dei 49 pazienti senza alterazioni post1084 site fig . 
7 and 8 , respectively . discussion us is widely utilised in blunt abdominal trauma mainly as a result of its ease of use , which allows examinations to be il numero di pazienti veri positivi , falsi positivi , veri negativi e falsi negativi per us e ceus rispetto alla tc con mdc sono riportati rispettivamente in tabella 3 e tabella 4 . i valori di sensibilit , specificit , valore predittivo positivo e negativo per lus sono stati rispettivamente 70 , 2% , 59 , 2% , 74 , 7% e 53 , 7% ; per la ceus sono stati 96 , 4% , 98% , 98 , 8% e 94 , 1% . 
la ceus ha dimostrato un numero significativamente pi elevato di lesioni correttamente identificate rispetto alla us , fornendo una stretta correlazione tra le dimensioni delle lesioni misurate con la gradazione ottenuta con la tc ( tabella 6 )  . 
 in stable patients , on the other hand , organ damage needs to be precisely evaluated to initiate the most appropriate treatment , whether conservative , surgical or interventional [ 29 ]  . 
the use of contrast material significant improves the diagnostic discussione lus ampiamente utilizzata nel trauma chiuso delladdome soprattutto per le sue caratteristiche di maneggevolezza che ne consente lutilizzo allinterno dellarea di emergenza , al letto del paziente , senza interrompere le manovre di rianimazione . 
la scansione ecocontrastografica rileva un focolaio lacerativo del terzo medio della milza con fuoriuscita ( freccia ) di mdc ecografico dallorgano . radiol med ( 2009 ) 114 : 10801093 fig . 
c la tc dimostra la presenza di una piccola lesione del labbro mediale del rene ( freccia ) con raccolta perirenale . con il trattamento pi idoneo , conservativo , chirurgico o di radiologia interventistica [ 29 ]  . 
limpiego del mezzo di contrasto ecografico determina un significativo miglioramento delle performance diagnostiche dellus , che raggiunge una sensibilit quasi uguale a quella della tc . la societ europea di ultrasuoni in medicina e biologia ( efsumb ) ha recentemente riportato limpiego della ceus nelle sue linee guida in caso di tc non disponibile o contro - indicata per precedenti reazioni allergiche al mdc iodato ; tc non conclusiva per artefatti ; monitoraggio di lesioni traumatiche note ; trauma chiuso minore , soprattutto in et pediatrica [ 30 ]  . nella nostra esperienza , la ceus ha consentito di rilevare un maggior numero di lesioni rispetto allus e di definirne le dimensioni , i rapporti con la capsula e le eventuali situazioni di sanguinamento attivo . 
infatti , nella gestione del paziente traumatizzato , tale reperto , associato alla presenza di emoperitoneo , suggerisce unelevata probabilit di fallimento del trattamento conservativo ed orienta ad un rapido trattamento chirurgico o di embolizzazione [ 31 ]  . la mancanza di contrast - enhancement in parte o in tutto lorgano studiato , consente di porre la diagnosi di lesione vascolare . 
with improved detection and precise localisation of organ injuries , the emergency surgeon can receive in real time accurate lesion grading in accordance with the reference standard ct . also in our experience , we found the possibility of identifying areas of active bleeding as contrast extravasation from the lesion to be particularly useful . 
in fact , in managing trauma patients , this finding if associated with the presence of haemoperitoneum strongly predicts the failure of conservative treatment , indicating a need for a prompt surgical or embolisation procedure [ 31 ]  . the lack of contrast enhancement in part of or in the entire organ allowed us to establish a diagnosis of vascular lesion . 
in one of our cases , lack of perfusion of the left kidney in a young patient with a complex splenic laceration led to detection of an injury to the renal vascular pedicle , which was treated with simultaneous nephrectomy and splenectomy . in patients undergoing conservative treatment , ceus allows effective monitoring , as it does not require transferring the patient to the ct room and avoids any exposure to radiation and iodinated contrast agents . 
in our department , ceus has become the most frequent procedure performed in children , a setting in which it has recorded its major sione del rene sinistro , in un giovane traumatizzato con frattura complessa di milza , ha permesso di identificare lavulsione del peduncolo vascolare del rene , trattata con nefrectomia simultaneamente alla splenectomia . 
 nel paziente avviato al trattamento conservativo , la ceus rappresenta un efficace sistema di monitoraggio , evitando lo spostamento del paziente verso la sala tc e lesposizione a radiazioni ionizzanti ed al mdc iodato . tale procedura rappresenta , nella nostra realt , la maggioranza dei trattamenti in ambito pediatrico e proprio in tale ambito la metodica ha un importante impatto sulla gestione del paziente traumatizzato [ 31 , 32 ]  . 
questo aspetto pu essere di particolare impatto soprattutto nelle donne in et fertile , nelle quali frequente il riscontro di una piccola falda fluida nello scavo di douglas , il cui significato pu essere ambiguo . 
uno studio di brown et al , a questo proposito , concludeva che la presenza di una raccolta fluida isolata nel cul - di - sac in donne in et fertile poteva essere considerata fisiologica e che un follow - up clinico poteva essere sufficiente [ 33 ]  . 
probabilit pre - test e post - test di us ( linea rossa ) e ceus ( linea blu ) per pazienti veri negativi . impact on trauma evaluation [ 31 , 32 ]  . 
on this subject concluded that fluid collections isolated to the pouch of douglas in women of reproductive age could be considered physiological and requiring clinical follow - up only [ 33 ]  . 
in clinical practice , the finding of small peritoneal fluid collections in trauma patients is an indication for an immediate ct scan without and with contrast agent to exclude organ lesions . 
ceus allows for a rapid assessment of solid organs , potentially avoiding the need for ct and thus reducing exposure to radiation and iodinated contrast agents . ceus errors included one false splenic lesion and failure to detect one renal lesion and one adrenal haematoma . 
the false splenic lesion on ceus was correctly evaluated as an in un paziente traumatizzato determina limmediata esecuzione di una tc senza e con mdc per escludere eventuali lesioni dorgano . 
la ceus permette di valutare rapidamente gli organi solidi evitando potenzialmente lesecuzione della tc , e quindi riducendo lesposizione a radiazioni ionizzanti e al mdc iodato . gli errori della ceus sono stati rappresentati da 1 falsa lesione splenica e dalla mancata identificazione di 1 lesione renale e di un ematoma del surrene . 
i 2 pazienti con lesione del rene e del surrene , identificati solo con tc , sono stati entrambi casi di lesioni non chirurgiche , trattate conserva1092 radiol med ( 2009 ) 114 : 10801093 ischaemic lesion on ct . 
the two patients with renal and adrenal lesions , identified by ct only , were both cases of nonsurgical lesions , the missed detection of which did not modify patient outcome . clearly , ceus is burdened by the typical limitations of sonography , such as the less panoramic view in comparison with ct and the difficulty in examining large patients , even though the new us scanners accommodate this class of patients as well . as our study was conducted in a single centre , it considered a relatively small number of patients compared with the large series in the literature regarding us and ct . 
a multicentre study could allow us to investigate a statistically significant number of patients and better define the real advantages of this new technique . conclusions our prospective study , in line with other experiences reported in the literature , has confirmed that ceus is an accurate diagnostic tool that may find an indication for evaluating stable patients with abdominal trauma , in that it provides performance values approaching those of ct . 
in particular , we believe ceus to be useful in patients with minor abdominal trauma and in the presence of free peritoneal fluid , as it enables identification of the injured organ and definition of the severity of the injury without causing delays in the diagnostic workup . 
 conclusioni il nostro studio prospettico , in linea con altre esperienze della letteratura , ha confermato che la ceus uno strumento diagnostico accurato e che pu trovare indicazione trauma nella valutazione del paziente stabile con delladdome , in quanto consente di ottenere valori di performance che si avvicinano molto a quelli della tc . 
in particolare riteniamo che limpiego del mdc in ecografia sia particolarmente utile nel paziente con trauma minore delladdome , quando sia presente un versamento peritoneale , per identificare lorgano sede di lesione e graduare lentit del danno senza alcun ritardo nelliter diagnostico . la ceus , inoltre , dovrebbe essere eseguita anche in assenza di versamento libero , quando vi siano alterazioni degli esami di laboratorio ( ad esempio aumento delle transaminasi o delle amilasi , microematuria , anemizzazione ) o fratture ossee che pongano il sospetto di lesioni intra - addominali ( ultime coste , apofisi trasverse delle vertebre lombari ) e in tutti i casi in cui la dinamica del trauma sia definibile come maggiore [ 20 ]  . 
cova unit clinico operativa di radiologia , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , 34149 trieste , italy correspondence to : s . 
three readers independently reviewed the axial ct scans and multiplanar oblique and twoand three - dimensional reconstructions ( maximum intensity projection and volume rendering ) images to assess degree of stenosis according to four categories : 1 ( 0%49% stenosis ) ; 2 ( 50%99% stenosis ) ; 3 ( occluded ) ; 4 ( not evaluable )  . 
in 53 patients , 1 , 440 segments were evaluated ( infrarenal aorta and 16 arterial segments for each leg ; 42 bilateral studies , 11 unilateral studies )  . 
sixty - four - row multislice ct proved to be helpful in detecting haemodynamically significant lesions in peripheral arterial occlusive disease and improved the results obtained with 4and 16 - slice multidetector ct . 
tre radiologi hanno valutato le immagini assiali e le ricostruzioni multiplanari oblique e bi - tridimensionali ( maximum intensity projection [ mip ] , volume rendering [ vr ] ) , e hanno classificato le lesioni in 4 gradi : 1 = stenosi 0%49% , 2 = stenosi 50%99% , 3 = occlusione , 4 = non valutabile . 
langio - tc a 64 strati si dimostrata affidabile nella valutazione delle lesioni steno - ostruttive dellaoai ed stata in grado di migliorare ulteriormente i risultati ottenuti con tc a 416 strati . 
inoltre , grazie allelevata risoluzione spaziale e ad una tecnica rigorosa , non sono stati rilevate variazioni nei dati ottenuti al di sotto del ginocchio , superando un limite delle tc delle generazioni precedenti . 1116 radiol med ( 2009 ) 114 : 11151129 keywords 64 - row multislice computed tomography digital angiography peripheral arterial occlusive disease parole chiave tomografia computerizzata a 64 strati angiografia digitale arteriopatia ostruttiva arti inferiori introduction introduzione lifestyles occlusive arterial disease ( oad ) of the lower extremities is a disorder of leg arteries associated with a clinical situation resulting from altered tissue perfusion , which may evolve into chronic or acute ischaemia . 
in 95% of cases , it is caused by atherosclerosis [ 1 ] and manifests as a diffuse disease with constant involvement of other regions , such as the coronary and carotid arteries [ 2 ]  . 
in the remaining 5% of cases , oad has inflammatory causes ( buergers disease , takayasus arteritis , hortons arteritis ) or iatrogenic causes ( ergotamine , beta - blockers , etc )  . 
the main risk factors of oad of the lower extremities are the same as those identified for oad in other vascular districts , namely , age , smoking , diabetes , hypertension , hyperlipidaemia , hyperhomocysteinaemia , and male sex [ 35 ]  . for many years , angiography with arterial catheterisation , initially with conventional acquisition then with digital subtraction technique , was the mainstay diagnostic technique for planning surgical and endovascular treatment . however , it is an invasive technique that requires hospitalisation and is burdened by a small risk of immediate ( dissection , mobilisation of atheromatous plaques or microemboli ) and late ( pseudoaneurysms ) complications [ 6 , 7 ]  . 
over the last few years , other less invasive techniques have appeared alongside intra - arterial catheterisation angiography , such as colour - doppler ultrasound ( us ) and magnetic resonance ( mr ) imaging or computed tomography ( ct ) angiography . ct angiography performed with multislice scanners and a large number of detectors is a rapid , noninvasive and welltolerated technique that is less costly than digital angiography as a result of less utilisation of personnel and supplies , the outpatient nature of the procedure and smaller amount of contrast material required [ 8 ]  . the purpose of this study was to evaluate the diagnostic capabilities of 64 - slice ct angiography in the evaluation of haemodynamically significant lesions in lower - extremity arteries using digital subtraction angiography ( dsa ) as the gold standard . larteriopatia ostruttiva ( ao ) degli arti inferiori una patologia che colpisce le arterie degli arti inferiori , associata ad una condizione clinica conseguente allalterata perfusione ematica dei tessuti con evoluzione verso unischemia cronica e talvolta acuta . 
nel 95% dei casi si riconosce come causa laterosclerosi [ 1 ] e si manifesta come una malattia diffusa che coinvolge costantemente anche altri distretti quali le arterie coronarie e carotidi [ 2 ]  . 
i principali fattori di rischio di ao degli arti inferiori sono gli stessi riconosciuti per altre aree vascolari , vale a dire et , fumo , diabete , ipertensione , iperlipidemia , iperomocisteinemia , sesso maschile [ 35 ]  . per molti anni langiografia mediante cateterismo arterioso , dapprima con tecnica di acquisizione convenzionale e quindi mediante sottrazione digitale , ha rappresentato lindagine diagnostica fondamentale al fine della programmazione del trattamento terapeutico sia chirurgico che endovascolare . 
tuttavia tale tecnica risulta essere invasiva e necessita il ricovero del paziente e , seppur in basse percentuali , gravata da alcune complicanze sia immediate ( dissezione , mobilizzazione di placche ateromasiche o di microemboli ) che tardive ( pseudoaneurismi ) [ 6 , 7 ]  . negli ultimi anni , allangiografia mediante cateterismo arterioso si sono affiancate tecniche sicuramente meno invasive quali leco - color doppler e langiografia mediante risonanza magnetica ( rm ) o mediante tomografia computerizzata ( tc )  . 
questultima grazie alla tecnologia multistrato ad elevato numero di detettori , rappresenta una tecnica rapida e priva di invasivit , con unottima compliance da parte dei pazienti ed una significativa riduzione dei costi rispetto allangiografia digitale per minor impegno di personale e consumo di materiali , per il radiol med ( 2009 ) 114 : 11151129 materials and methods we retrospectively reviewed 53 patients who underwent 64slice ct angiography of the lower extremities followed by dsa within 36 days ( range 1966 days ) at our institute between january 2006 and april 2008 . 
indications for ct angiography included specific clinical symptoms ( intermittent claudication , leg pain , trophic changes to the skin , nail dystrophy , etc ) and findings on colour - doppler us . 
all patients gave their informed consent to both procedures . ct angiography ct angiography was performed with a ct scanner featuring 64 rows of solid - state detectors ( toshiba aquilion , toshiba medical systems , tokyo , japan ) , a toshiba megacool tube and a 60 - kw high - frequency xray generator , multiple kilovolt settings ( 80100120135 kv ) , and milliampere range of 50500 ma with steps of 10 ma [ 9 ]  . 
contrast material was injected in an antecubital vein via an 18 - 20 - gauge needle cannula connected to an automated power injector ( stellant sct 211 , medrad , indianola , ia , usa )  . 
the scan protocol included a double orthogonal scout view from the diaphragm to the feet , followed by a 30 - ml saline test injection to establish the venous access and injection of a single 80to 120 - ml contrast bolus , depending on patients height and build , at a flow rate of 4 ml / s . 
the entire scan volume was divided into two parts to facilitate postprocessing : the first , from the renal arteries to the knee , was reconstructed with a 40 - cm field of view ( fov ) , 512512 pixel matrix , 1 - mm slice thickness at an interval of 0.5 mm ; the second , from the knee to the foot , was 1117 carattere ambulatoriale della prestazione e per la minor quantit di mezzo di contrasto ( mdc ) necessaria per lesecuzione dellesame tc [ 8 ]  . lo scopo di questo studio quello di valutare le reali capacit diagnostiche dellangio - tc a 64 strati nella valutazione delle lesioni emodinamicamente significative delle arterie degli arti inferiori , utilizzando come gold standard langiografia digitale ( ad ) a sottrazione dimmagine . materiali e metodi nel nostro istituto , nel periodo tra gennaio 2006 e aprile 2008 , sono stati valutati retrospettivamente 53 pazienti , sottoposti , in seguito a sintomatologia clinica specifica ( claudicatio intermittens , sintomatologia dolorosa agli arti inferiori , alterazioni del trofismo cutaneo , distrofie ungueali , ecc . ) e sulla base di rilievi eco - color doppler , ad angio - tc a 64 strati delle arterie degli arti inferiori e successivamente , in un arco di tempo medio di 36 giorni ( min , 19 giorni ; max , 66 giorni ) , ad ad dello stesso distretto . 
tutti i pazienti hanno fornito un consenso informato ad entrambe le procedure . angio - tc gli esami di angio - tc sono stati eseguiti utilizzando un tomografo computerizzato a 64 strati di detettori allo stato solido ( toshiba aquilion , toshiba medical systems , tokyo , giappone ) composto da un tubo toshiba megacool e da un generatore di raggi x ad alta frequenza con una potenza di 60 kw , un range di kv disponibili tra 80 e 135 ( 80 / 100 / 120 / 135 ) ed un range di ma tra 50 e 500 con step di 10 ma [ 9 ]  . 
i parametri per lesecuzione dellangio - tc degli arti inferiori sono stati : uno spessore nominale di strato pari a 0 , 5 mm per 64 strati , un movimento del tavolo di 26 , 5 mm per rotazione , un pitch factor di 0 , 828 ( helical pitch : 53 ) ed un tempo di rotazione di 0 , 4 secondi ; sono stati utilizzati 120 kv e 230 ma con esposizione modulata per ridurre la dose ( sure exposure : standard )  . 
il paziente stato posto in posizione supina , con le caviglie dentro al poggiatesta e ginocchia e bacino in posizione neutrale , al fine di limitare gli artefatti da movimento durante lacquisizione delle immagini . 
il mdc stato iniettato attraverso unagocannula da 1820 g inserita in una vena a livello 1118 radiol med ( 2009 ) 114 : 11151129 reconstructed with 25 - cm fov , 512512 matrix , and 0.5mm slice thickness at an interval of 0.3 mm to minimise voxel size and maintain maximal spatial resolution in the most distal sectors where the arteries have smaller diameter . 
to optimise scan timing , we used the sure - start function , with a low - dose pulsed scan at the level of the infrarenal abdominal aorta 10 s after the beginning of the injection and placement of a region of interest ( roi ) over the aorta lumen to calculate the density increase inside the aorta . 
adequate opacification of the entire vascular axis of interest was thus achieved in all cases . software ( vitrea , vital images were automatically transferred to a workstation with dedicated images , minnetonka , mn , usa )  . 
in the presence of significant stenoses or heavily calcified arteries , further reconstructions such as curved multiplanar ( cmpr ) and vessel probe ( vp ) reconstructions were performed to improve depiction of the course of the diseased arteries and provide panoramic support for the information obtained from axial images . 
under angiographic guidance , a straight or pigtail 5 - french diagnostic catheter was placed in the infrarenal abdominal aorta . in the humeral approach , a hydrophilic guidewire and pigtail catheter were preferred . 
image acquisition was carried out with the successive fields technique : five separate adjacent fields were acquired from the aortoiliac to the tibioperoneal area , with a slight overlap to ensure inclusion of all segments of the arterial tree . 
il protocollo di acquisizione prevede , dopo lesecuzione di una doppia scout - view ortogonale dal diaframma ai piedi , uniniezione test di 30 ml di soluzione fisiologica per verificare laccesso venoso , e liniezione di un unico bolo di mdc pari a 80120 ml , a seconda dellaltezza e della costituzione fisica del paziente , ad un flusso di 4 ml al secondo ; liniezione del mdc seguita da un piccolo bolo ( 30 ml ) di soluzione fisiologica sempre ad un flusso di 4 ml / s . 
lintero volume stato suddiviso in due parti per agevolare il postprocessing : la prima , dalle arterie renali al ginocchio , ricostruita con campo di vista ( fov ) pari a 40 cm , matrice di 512512 pixel , spessore di strato pari 1 mm ad un intervallo di 0 , 5 mm ; la seconda , dal ginocchio al piede , ricostruita con fov di 25 cm , matrice di 512512 e spessore di strato pari a 0 , 5 mm ad un intervallo di 0 , 3 mm , per ridurre al minimo le dimensioni del voxel al fine di mantenere la massima risoluzione spaziale nei settori pi distali dove i vasi arteriosi presentano un calibro minore . 
to improve opacification of the leg arteries , some cases required injection of 40 ml instead of 30 ml of contrast agent during the acquisition of the most distal field . 
tutti i pazienti sono stati sottoposti a un cateterismo arterioso del tratto distale dellaorta addominale dopo puntura dellarteria femorale comune o dellarteria omerale con tecnica di seldinger : attraverso la guida angiografica stato posizionato un catetere diagnostico da 5 french a radiol med ( 2009 ) 114 : 11151129 1120 fig . 
ct angiography and dsa images were first examined separately by three radiologists with different levels of experience with angiography ( sc , fpm , ap ) and then , in the case of discordant interpretations , they were discussed jointly to reach a consensus . 
the arteries were evaluated by region and rated according to a previously reported scoring system [ 10 ] : 1 punta dritta o pig - tail a livello del tratto sottorenale dellaorta addominale . 
lacquisizione delle immagini stata poi effettuata con la modalit a campi successivi : sono stati acquisiti 5 campi distinti contigui a partire dal distretto aorto - iliaco sino a quello tibio - peroneale , in radiol med ( 2009 ) 114 : 11151129 1121 table 1 scoring system grade degree of stenosis tabella 1 punteggio di valutazione grado grado di stenosi < 50% 50%99% occlusion not evaluable < 50% 50%99% occlusione non valutabile minima parte sovrapposti per avere la certezza di non escludere dallo studio nessun tratto dellalbero arterioso in esame . 
per ciascun campo stato iniettato un bolo di mdc non ionico con concentrazione di iodio compresa tra 320 e 370 mgi / ml ( visipaque 320 , amersham health , princeton , new jersey , usa ; ultravist 370 , bayer - schering pharma ag , berlin , germania ) mediante iniettore automatico ( medrad mark v , indianola , usa ) di 2530 ml con un flusso di 15 ml / s . 
per ottenere un maggiore tenore di opacizzazione delle arterie della gamba , talvolta stato necessario iniettare 40 ml di mdc , anzich 30 ml , durante lacquisizione del campo pi distale . 
le immagini dellangio - tc e dellangiografia digitale sono state esaminate dapprima separatamente da tre radiologi con esperienza angiografica di diverso livello ( sc , fpm , ap ) e poi , nel caso di eventuali discordanze , ridiscusse insieme fino ad ottenere una concordanza di giudizio . 
le arterie sono state valutate distretto per distretto , assegnando uno score ricavato dalla letteratura [ 10 ] , che prevede lassegnazione di un punteggio pari a 1 se larteria risulta sana o con una stenosi minore del 50% , a 2 se presenta una stenosi tra il 50% ed il 99% , a 3 se occlusa , a 4 se non valutabile ( tabella 1 )  . 
3 la suddivisione dellalbero arterioso oggetto dello studio . for healthy arteries or arteries with < 50% stenosis , 2 for 50%99% stenosis , 3 for occlusion , and 4 for not evaluable arteries ( table 1 )  . 
in the event of multiple lesions in the same region , the lesion with the highest degree of stenosis was considered . separate evaluations were made for lesions of the following arteries : common iliac ( ci ) , internal iliac ( ii ) , external iliac ( ei ) , common femoral ( cf ) , deep femoral ( df ) , proximal ( sf1 ) and distal superficial femoral ( sf2 ) , supra - articular ( p1 ) and subarticular popliteal ( p2 ) , proximal ( at1 ) and distal ( at2 ) anterior tibial , tibioperoneal ( tr ) , proximal ( pe1 ) and distal peroneal ( pe2 ) , and proximal ( tp1 ) and distal ( tp2 ) posterior tibial . 
sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) , diagnostic accuracy and concordance in degree of stenosis between the two modalities were calculated for all segments , taking dsa as the gold standard [ 8 , 10 , 11 ]  . 
patients with a score of 1 were considered negative ( healthy ) , whereas those with scores of 2 and 3 that is , 1122 table 2 summary of statistical results dsa + dsa 64 - slice ct + 64 - slice ct total 1 , 017 1 , 048 tabella 2 riepilogo statistico dei nostri risultati atcms64 + atcms64 totale 1017 1048 total 1 , 028 1 , 440 totale 1028 1440 dsa , digital subtraction angiography ; ct , computed tomography atcms64 , angio - tomografia computerizzata a 64 strati ; ad , angiografia digitale radiol med ( 2009 ) 114 : 11151129 sullarteria iliaca comune ( ic ) , iliaca interna ( ii ) , iliaca esterna ( ie ) , femorale comune ( fc ) , femorale profonda ( fp ) , femorale superficiale prossimale ( fs1 ) e distale ( fs2 ) , poplitea sopra ( p1 ) e sottoarticolare ( p2 ) , tibiale anteriore prossimale ( ta1 ) e distale ( ta2 ) , tronco tibioperoneale ( tr ) , peroneale prossimale ( pe1 ) e distale ( pe2 ) e tibiale posteriore prossimale ( tp1 ) e distale ( tp2 )  . 
sul totale dei segmenti sono stati calcolati sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) , accuratezza diagnostica e la concordanza del grado di stenosi tra le due metodiche , ponendo come gold standard langiografia digitale [ 8 , 10 , 11 ]  . 
sono stati considerati negativi al test ( sani ) i pazienti con uno score di 1 e positivi al test ( malati ) i pazienti con uno score 2 e 3 ovvero i pazienti che presentavano un quadro di stenosi superiore al 50% oppure unocclusione completa del vaso [ 10 , 12 ]  . with > 50% stenosis or complete occlusion were considered positive ( diseased ) [ 10 , 12 ]  . risultati results the total number of segments considered for which comparisons were possible in the 53 patients was 1 , 440 ( table 2 )  . we excluded from the analysis segments that were not assessed with both methods , that is , a total of 309 segments in 11 patients for whom dsa was performed on one extremity only . 
with regard to overand underestimation , there were 31 cases ( 2.1% ) of significant overestimation with positive ct angiography ( > 50% stenosis or obstruction ) but negative dsa ( < 50% stenosis ) , 10 cases ( 0.7% ) of slight overestimation with occlusion on ct angiography but > 50% stenosis on dsa , 11 cases ( 0.8% ) of significant underestimation with negative ct angiography but positive dsa ( > 50% stenosis or occlusion ) , and 14 cases ( 1% ) of slight underestimation where ct angiography was positive for > 50% stenosis whereas dsa showed occlusion . 
concordance in the degree of stenosis was 95.4% ( table 3 )  . in addition , we analysed separately the data regarding the vascular segments below the knee , as the small size of the vessels and frequent calcifications make this area particularly critical . 
per quanto riguarda i casi di sovrae sottostime , sono stati evidenziati 31 casi ( 2 , 1% ) di sovrastima significativa con paziente positivo allangio - tc ( stenosi > 50% o ostruzione ) , ma negativo alla ad ( stenosi < 50% ) , 10 casi ( 0 , 7% ) di sovrastima lieve , con paziente occluso allangio - tc , ma con stenosi > 50% alla ad , 11 casi ( 0 , 8% ) di sottostima significativa , con paziente negativo allangio - tc , ma positivo alla ad ( stenosi > 50% o occlusione ) e 14 casi ( 1% ) di sottostima lieve con paziente positivo in angio - tc per una stenosi > 50% , in realt occluso alla ad . 
considerando i dati complessivi , stata riscontrata una sensibilit del 97 , 2% , specificit del 97 , 0% , vpp al 92 , 5% , vpn al 98 , 9% e accuratezza pari al 97 , 1% . 
la concordanza del grado di stenosi risultata pari a 95 , 4% ( tabella 3 )  . oltre ai dati complessivi , sono stati valutati separatamente i dati relativi ai segmenti dellalbero vascolare al di sotto del ginocchio , distretto questo particolarmente critico per le esigue dimensioni dei vasi e la frequente presenza di calcificazioni ; in questo caso il totale dei segmenti valutati corrisponde a 604 ( tabella 4 )  . 
in questo distretto sono stati riscontrati i valori di sensibilit pari a 97 , 5% , specificit 96 , 9% , vpp 95 , 5% , vpn 98 , 3% , accuratezza 97 , 2% , concordanza del grado di stenosi 93 , 5% ( tabella 5 )  . radiol med ( 2009 ) 114 : 11151129 1123 fig . 
sixty - four - slice ct angiography with its near - isotropic voxels produces very high - quality reconstructions in the three spatial planes , thereby modifying the diagnostic approach to a technique that formerly relied on evaluation of axial images only . multislice ct has overcome the problems of the early spiral ct devices ( limited craniocaudal coverage during a single contrast injection ) by enabling fast acquisition times , reduced contrast agent doses and increased spatial resolution , with the possibility of studying even the smallest vessels [ 18 , 19 ]  . 
recent studies report that the introduction of multislice ct scanners have increased the sensitivity and specificity of ct to levels very close to those of dsa , with the exception of small vessels [ 13 , 2022 ]  . 
the purpose of our study was to ascertain whether the latest - generation equipment can further improve sensitivity and specificity compared with the earlier 4and 16 - slice scanners , particularly in the study of small - calibre vessels . 
langio - tc a 64 strati grazie alla sostanziale isotropicit del voxel permette di ottenere ricostruzioni di qualit altissima nei tre piani dello spazio , modificando di fatto lapproccio diagnostico di tale metodica , un tempo legata alla sola valutazione delle immagini assiali . 
la tc multistrato ha ridimensionato le problematiche delle prime apparecchiature spirali ( limitata copertura cranio - caudale durante una singola iniezione del mdc ) , offrendo tempi di acquisizione brevi , una riduzione della dose di mdc ed un aumento della risoluzione spaziale che ha permesso lo studio anche dei vasi di minor calibro [ 18 , 19 ]  . 
le pubblicazioni pi recenti riportano che , con lintroduzione delle apparecchiature tc multistrato , la sensibilit e la specificit di questindagine risultano molto vicine a quella dellangiografia digitale , fatto salvo , anche in questo caso , per i vasi di calibro minore [ 13 , 2022 ]  . lobiettivo del nostro lavoro stato quello di verificare se le apparecchiature di ultima generazione siano in grado di apportare un ulteriore miglioramento dei valori di sensibiradiol med ( 2009 ) 114 : 11151129 1124 fig . 
the 3d mip ( a - c ) reformation apparently shows patency of the proximal and middle segments , of the peroneal ( arrows ) and of the left posterior tibial artery , respectively . 
the use of high - iodine - concentration contrast material has led to greater opacification of the arterial tree , with clear attenuation differences from the surrounding tissues , thus reducing postprocessing time [ 23 ]  . however , in our experience , postprocessing amounts to 20 min on average for each study for an experienced operator . the speed of the equipment significantly increases patient compliance , and images are virtually free from motion artefacts . 
langio - tc a 64 strati degli arti inferiori si rivelata , nel complesso , una tecnica di semplice esecuzione , rapida , con un tempo desame brevissimo , un tempo di preparazione del paziente molto contenuto , legato alla sola repertazione di un accesso venoso , ma con un notevole impegno di tempo per il post - processing . 
lutilizzo di mdc ad alta concentrazione di iodio ha permesso di ottenere una maggior opacizzazione dellalbero arterioso in modo da realizzare un netto distacco in termini di uh dai tessuti circostanti per ridurre il dispendio di tempo nel post - processing [ 23 ] , comunque quantificabile nella nostra esperienza in 20 minuti in media ad esame , per un operatore esperto . favorisce molto la compliance del paziente , risultando le immagini velocit dellapparecchiatura radiol med ( 2009 ) 114 : 11151129 1125 fig . 
b , d limmagine angiografica mostra una stenosi di modesta entit , inferiore al 50% , pertanto non significativa . overall analysis of our results indicates that in most cases ( 95.4% ) , there is excellent concordance between the results of 64 - slice ct angiography and dsa , with a further slight improvement over published data for older - generation ct scanners ( table 6 )  . 
our data are fully concordant with those reported in the literature , with slightly higher values for sensitivity , ppv and npv ; the very high npv of ct angiography emphasises its well - known reliability in demonstrating the real absence of disease in healthy patients . 
sixty - four - slice equipment has also overcome , through optimisation of the examination technique and very high spatial resolution , the problems reported in previous studies , allowing almost identical results in the leg vessels to those in the upper regions , thus overcoming the limitations due to the vessel diameter and the close relation with bone structures . 
all this would not , however , be possible without the necessary parallel evaluation of the reconstructed and axial images , which basically eliminates diagnostic errors due to incorrect reconstructions . praticamente esenti da artefatti da movimento . 
riportavano invece nel 2004 [ 21 ] i dati della tc spirale a 4 strati con valori di sensibilit del 93% , una specificit del 95% , un valore predittivo positivo del 90% ed un valore predittivo negativo del 97% ; nel 2005 willmann et al . 
 analizzando globalmente i risultati da noi ottenuti si evince che nella maggior parte dei casi ( 95 , 4% ) esiste una ottima concordanza tra i risultati forniti dallangio - tc a 64 strati e dallad con un ulteriore lieve miglioramento dei dati riportati in letteratura per apparecchiature tc delle precedenti generazioni ( tabella 6 )  . 
underestimations can be in part explained by heavily calcified vessels simulating vascular patency ; overestimates , instead , often result from inadequate opacification of a portion of vessel owing to slower blood circulation tiva dellesame angio - tc sottolinea lormai nota affidabilit nel dimostrare la reale assenza di patologia nei pazienti sani . 
lapparecchiatura a 64 strati ha inoltre permesso , con lottimizzazione della tecnica di esame e con laltissima risoluzione spaziale , di superare le problematiche emerse in tutti i lavori precedenti in letteratura e di ottenere quindi a livello dei vasi della gamba risultati pressoch identici a quelli del distretto superiore , superando di fatto i limiti dovuti al calibro vasale ed al rapporto stretto con le strutture ossee , comunque mai prescindendo dallindispensabile valutazione parallela delle immagini ricostruite ed assiali , che sostanzialmente azzera gli errori diagnostici da errate ricostruzioni . importante evidenziare anche il numero estremamente basso di sovrastime e sottostime che abbiamo rilevato , dato questo che rende lesame angio - tc a 64 strati , in termini di accuratezza diagnostica , sicuramente superiore alla angiorm , molto influenzata dal ritorno venoso e da stent che determinano artefatti da suscettibilit magnetica , e molto vicina al gold standard angiografico . 
le sottostime sono in parte spiegabili da vasi estremamente calcifici che simulano la perviet vascolare ; le sovrastime invece spesso sono derivate da uninsufficiente opacizzazione di un tratto vasale per un circolo pi rallentato anche monolateralmente . 
risulta chiaro come tali limiti , intrinseci alla tecnica tc , siano stati minimizzati migliorando la risoluzione spaziale lungo lasse z , mantenuta da noi volutamente il pi possibile elevata proprio a questo livello ed ottimizzando la tecnica dindagine . 
 [ 22 ] : 16 strati casistica personale : 64 strati 90 , 9 97 , 2 vpp , valore predittivo positivo ; vpn , valore predittivo negativo 92.4 92 , 4 92.5 92 , 5 98.9 98 , 9 97.1 97 , 1 studio sensibilit ( % ) specificit ( % ) vpp ( % ) vpn ( % ) accuratezza ( % ) unilaterally . 
these limitations inherent in the ct technique were clearly minimised by improving z - axis spatial resolution , which was intentionally kept as high as possible at this level , and by optimising the study technique . 
in diagnostic terms , compared with dsa , multislice ct angiography has two additional advantages : first , it is very accurate in evaluating eccentric stenoses , thanks to axial imaging of the vessel lumen ; for dsa to obtain the same information in those locations requires further oblique or lateral projections with increased patient exposure and contrast material dose . second , it visualises the segments located immediately after an obstruction , which angiography fails to depict [ 14 ]  . 
the same accuracy of information means ct angiography could replace dsa as an initial investigation in the preoperative evaluation of patients [ 14 ]  . langio - tc multistrato presenta due ulteriori vantaggi : essa risulta estremamente accurata nella valutazione delle stenosi eccentriche grazie alle immagini assiali del lume dei vasi , l dove per ottenere le stesse informazioni , la ad necessit di ulteriori proiezioni oblique o laterali con aumento di dose e di somministrazione del mezzo di contrasto al paziente ; in secondo luogo rende possibile la visualizzazione dei segmenti immediatamente successivi ad unostruzione che non risultano visibili in angiografia [ 14 ]  . in particolare langio - tc pu fornire un quadro globale dellalbero arterioso del paziente e pu servire a mirare lintervento del radiologo interventista velocizzando tale procedura , risparmiando mdc e dose al paziente grazie alla possibilit di scegliere il materiale pi adatto e lapproccio pi idoneo ( orientandosi magari verso un approccio omerale piuttosto che femorale , o una puntura in senso anterogrado omolaterale piuttosto che retrogrado controlaterale ) come gi suggerito da kock et al . 
 [ 8 ] ; le stesse informazioni rendono lindagine fruibile in prima istanza anche dal chirurgo vascolare al posto dellangiografia diagnostica , in previsione di un intervento chirurgico [ 14 ]  . conclusions conclusioni the study of oad of the lower extremities with 64 - slice ct angiography cannot be considered a screening method for asymptomatic patients but rather a valid alternative to mr angiography , especially in patients with absolute lo studio dellao degli arti inferiori con angio - tc a 64 strati non pu essere considerata una metodica di screening di pazienti asintomatici , ma si pone come valida alternativa allangio - rm , in primis nei pazienti con controindicazioni 1128 radiol med ( 2009 ) 114 : 11151129 contraindications to mr imaging . 
it should be proposed in patients with steno - obstructive disease diagnosed clinically and / or with colour doppler us or in patients with clear signs and symptoms and risk factors for obliterative arteriopathy such as hypertension , diabetes , hyperlipoproteinaemia and smoking , especially if combined . 
at our institute , diagnostic angiography has been virtually replaced by mr and ct angiography , its use being reserved for interventional procedures or in targeted studies on the basis of results of the diagnostic investigations . 
 assolute alla rm ; essa deve essere proposta a pazienti con patologia steno - ostruttiva gi inquadrata allesame obiettivo e / o strumentale mediante eco - color doppler , anche in evoluzione , oppure in pazienti con una chiara sintomatologia ed un corollario di fattori di rischio per arteriopatia obliterante quali ipertensione , diabete , dislipidemie , fumo , specialmente se in associazione , che abbisognino di una tecnica rapidamente disponibile , panoramica e molto affidabile . 
nel nostro istituto gli esami di angiografia diagnostica sono stati praticamente azzerati da angio - rm ed angio - tc , riservando interventista , allangiografia un ruolo esclusivamente comunque mirato in base ai risultati degli esami diagnostici . 
pedicelli , via trionfale 7130 , 00135 rome , italy , tel . : + 39 - 06 - 30156054 , fax : + 39 - 06 - 35501928 , e - mail : apedicelli@rm.unicatt.it received : 19 october 2008 / accepted : 21 november 2008 / published online : 22 september 2009 springer - verlag 2009 abstract purpose . 
clinically relevant improved mobility and reduction of pain and analgesics were observed , with overall significant results ( p < 0.0001 ) in all patients at 24 h after pvp and in 83 available patients at 6 months . 
pvp is a safe , rapid , effective and costeffective therapy for vcfs , requiring only brief hospital admission and with long - lasting clinical results , when performed under good - quality radiological guidance , when correct indications are respected and when it is associated with rehabilitation therapy in the follow - up . 
la vpp costituisce un trattamento sicuro , rapido , efficace , poco costoso , che richiede solo un ricovero breve e con risultati clinici duraturi qualora sia impiegato un sistema di guida radiologica di buona qualit , siano rispettate le corrette indicazioni e venga associata una terapia riabilitativa nel follow - up . rappresenta una valida alternativa alla terapia 1142 radiol med ( 2009 ) 114 : 11411158 immobilisation of frail and elderly patients at risk of clinical complications . keywords treatment efficacy osteoporosis fluoroscopy spinal fractures vertebroplasty conservativa , questultima gravata da elevati costi sanitari e che richiede spesso limmobilizzazione prolungata di pazienti fragili e anziani , a rischio di complicanze cliniche . parole chiave efficacia terapeutica osteoporosi fluoroscopia fratture vertebrali vertebroplastica introduction introduzione percutaneous vertebroplasty ( pvp ) involves the injection of polymethylmethacrylate ( pmma ) through a special needle into the vertebral body under radiological guidance . the main indication for the procedure is back pain associated with osteoporotic or osteolytic vertebral compression fracture that is refractory to conservative medical treatment [ 1 , 2 ]  . 
total direct costs were calculated at around 31.7 billion euro , which is forecast to increase to 76.7 billion in 2050 given the expected demographic changes across the continent [ 3 ]  . 
approximately 25%30% of the population affected by vcfs has such severe symptoms as to require medical attention [ 5 ] , with serious consequences for both patients and society at large , which is burdened by the significant healthcare costs for treatment and disability arising from this type of fracture . 
clinical consequences of vcfs such as acute and chronic pain , kyphosis , reduced mobility , respiratory difficulties , gastro - oesophageal reflux , bedridden status and depression can lead to reduced quality of life and are associated with an increase in mortality in proportion with the number of vcfs [ 6 ]  . traditional conservative therapy of symptomatic vcfs is often ineffective in the short term and can necessitate prolonged immobility and administration of high doses of analgesics with their associated side effects and a possible increase in risk and poor tolerance by this fragile patient population [ 7 ]  . 
while back pain may persist for 612 weeks , other complications can arise , such as respiratory infections , bedsores , venous thromboembolism and even death [ 8 ]  . 
currently , pvp and kyphoplasty are becoming valuable procedures for treating symptomatic vcfs , with the aim of obtaining pain relief and stabilisation of the fracture over the short term [ 1 , 2 , 9 ]  . in this study , we report our 3 - year experience with pvp for treating vcfs refractory to conservative therapy or in patients unable to tolerate prolonged immobility or orthopaedic braces because of associated reduction in quality of life , with special attention paid to optimization criteria of the procedure and overall patient management . la vertebroplastica percutanea ( vpp ) consiste nelliniezione di polimetilmetacrilato ( pmma ) attraverso uno speciale ago allinterno del corpo vertebrale sotto la guida radiologica . 
la principale indicazione alla procedura costituita dal dolore rachideo associato a frattura vertebrale su base osteoporotica o tumorale , refrattario al trattamento medico conservativo [ 1 , 2 ]  . 
i costi diretti totali sono stati calcolati intorno ai 31 , 7 miliardi di euro e dovrebbero aumentare a 76 , 7 miliardi nel 2050 in base ai cambiamenti attesi nella demografia europea [ 3 ]  . 
circa il 25%30% della popolazione colpita da fvc ha sintomi di tale gravit da richiedere lattenzione medica [ 5 ] , con serie conseguenze sia sui pazienti che sulla societ la quale deve caricarsi di onerosi costi sanitari per la terapia e la disabilit che consegue a questo tipo di frattura . 
conseguenze cliniche delle fvc quali dolore acuto e cronico , cifosi , ridotta mobilit , difficolt respiratorie , reflusso gastroesofageo , allettamento e depressione psicologica possono portare ad una ridotta qualit di vita e sono associate ad un incremento della mortalit a seconda della prevalenza del numero di fvc [ 6 ]  . 
la terapia conservativa tradizionale delle fvc sintomatiche spesso inefficace nel breve periodo e pu dover necessitare di una prolungata immobilizzazione e della somministrazione di elevate dosi di analgesici gravate da effetti collaterali , con un possibile aumento di pericoli e scarsa tolleranza da parte di una popolazione di pazienti fragili [ 7 ]  . 
mentre il dolore rachideo pu perdurare per 612 settimane , possono insorgere complicanze quali : polmonite , ulcere da decubito , tromboembolia venosa e persino il decesso [ 8 ]  . 
attualmente , la vpp e la cifoplastica stanno diventando validi strumenti per il trattamento delle fvc sintomatiche , con il fine di ottenere sollievo dal dolore e stabilizzazione della frattura in breve tempo [ 1 , 2 , 9 ]  . in questo lavoro riportiamo la nostra esperienza triennale con la vpp per il trattamento delle fratture vertebrali refrattarie alla terapia conservativa o in pazienti non in grado di sopportare lallettamento prolungato o il busto radiol med ( 2009 ) 114 : 11411158 materials and methods following the activation of pvp procedures in our radiology department , between september 2005 and september 2008 , we treated 120 consecutive patients with symptomatic vertebral fractures after obtaining informed consent . 
preliminary workup was based on a clinical and radiological examination [ magnetic resonance ( mr ) and / or computed tomography ( ct ) ] to establish the differential diagnosis of the back pain and to evaluate the correct indication for pvp ( table 1 )  . 
the inclusion criteria were : ( 1 ) focal pain on the median or paravertebral line , accentuated by digital pressure on the vertebral spinous process at the same level and associated with the radiological finding of one or multiple vertebral fractures ; ( 2 ) when an mr examination was available , signal hyperintensity of the fractured vertebral body on t2weighted and short - tau ( stir ) sequences ; ( 3 ) no radiological evidence of other spinal disorders that could account for the symptoms at the same level ; ( 4 ) absence of neurological signs ; and ( 5 ) ineffective medical treatment after at least 3 weeks . 
upon request by the referring physician due to marked intolerance of the patients to conservative treatment , 12 vcfs in ten patients were treated early , on average at 1 week from symptom onset . 
another 21 of the 120 treated patients instead suffered from old vcfs with little or no signal hyperintensity on t2 - weighted or stir sequences but with associated chronic pain persisting inversion recovery ortopedico perch causa di riduzione della qualit di vita , con particolare attenzione ai criteri di ottimizzazione della procedura e della gestione complessiva del paziente . 1143 materiali e metodi dopo lattivazione delle procedure di vpp nel nostro dipartimento di radiologia , da settembre 2005 a settembre 2008 abbiamo trattato 120 pazienti consecutivi con fratture vertebrali sintomatiche dopo consenso informato . 
la causa di frattura era losteoporosi in 102 casi , malattie linfoproliferative in 4 casi e metastasi ossee in 12 casi ; sono stati trattati anche 2 casi di angiomi vertebrali aggressivi . 
il work - up preliminare stato basato su un esame clinico e radiologico ( risonanza magnetica [ rm ] e / o tomografia computerizzata [ tc ] ) ai fini di una diagnosi differenziale del dolore rachideo e per valutare la corretta indicazione alla vpp ( tabella 1 )  . 
of treated vertebrae gender osteoporotic compression fracture primary or secondary tumour haemangioma m , male ; f , female ; mri , magnetic resonance imaging ; ct , computed tomography tabella 1 caratteristiche generali della popolazione trattata e tipologia degli esami radiologici preliminari patologia vertebrale numero pazienti numero vertebre trattate sesso preliminary radiological examinations x - ray esami radiologici preliminari frattura da osteoporosi neoplasia primaria o secondaria angioma m , maschio ; f , femmina ; rm , risonanza magnetica ; tc , tomografia computerizzata 1144 radiol med ( 2009 ) 114 : 11411158 fig . 
1 numero e distribuzione delle fvc trattate con vpp . listogramma mostra il numero ( asse verticale ) e la distribuzione ( asse orizzontale ) dei corpi vertebrali trattati con vpp nella nostra serie . for at least 1 year from symptom onset . 
the exclusion criteria were : ( 1 ) noncorrectable blood dyscrasias ; ( 2 ) effective medical therapy ; ( 3 ) stable and asymptomatic vertebral fracture ; and ( 4 ) local or systemic infection . 
pvp was performed with injection of pmma ( volume range 25 ml ) within the vertebral body with the use of a screw - type ( leveen ) or pressure syringe after transpedicular access . 
in all cases , the procedure was guided and monitored with low - dose digital fluoroscopy alone ( single plane tube , allura xper fd 20 with flat - panel detector , philips medical systems , the netherlands ) and performed with a 13 or 1011 - gauge vertebroplasty needle according to the pedicle diameter and the degree of access difficulty , as in the case of severe vertebral body collapse or vertebrae affected by heteroplastic lesions where a smaller bore needle was generally preferred . 
the vertebroplasty needle was introduced with the assistance of an orthopaedic hammer , although after our initial experience with the procedure , the hammer was in most cases only used to introduce and direct the needle through the pedicle , with further advancement within the vertebral body being easily performed with manual screwsettimana dallinsorgenza dei sintomi , su richiesta del medico curante a causa della marcata intolleranza da parte dei pazienti a sostenere la terapia conservativa . 
tra i 120 pazienti trattati , altri 21 soffrivano invece di vecchie fratture vertebrali con scarsa o assente iperintensit di segnale nelle sequenze rm t2w o stir , ma associate a dolore cronico perdurante da almeno 1 anno dallinsorgenza dei sintomi . 
tutti i trattamenti sono stati effettuati in condizioni di sterilit , dopo anestesia locale ( 78 ml di mepivacaina 2% per ogni singolo accesso percutaneo con infiltrazione anche del periostio peduncolare ) , il paziente in posizione prona , e hanno necessitato solamente di una blanda sedazione ( midazolam e / o fentanyl ) in 56 pazienti . 
la vpp stata effettuata con iniezione di pmma ( range volumetrico : 25 ml ) allinterno del corpo vertebrale per mezzo di siringa a vite ( di leveen ) o pistola a pressione e dopo accesso trans - peduncolare . 
la procedura sempre stata guidata e controllata esclusivamente da fluoroscopia digitale a bassa dose ( tubo monoplano , allura xper fd 20 con detettore flat - panel , philips medical systems , olanda ) ed eseguita con ago per vertebroplastica a becco di flauto di 13 o 1011 gauge , a seconda del diametro peduncolare e del grado di difficolt daccesso , come in caso di severo radiol med ( 2009 ) 114 : 11411158 1145 like manoeuvres without the need for any orthopaedic device . 
in the event of particular fluidity of the cement or the detection of cement in the perivertebral veins , the infusion of the pmma was immediately halted and between 30 and 45 s were allowed for polymerisation to reduce the fluidity and therefore the risk of cement leakage outside of the vertebral body . 
on the other hand , in the presence of particularly compact bone , as is often seen in severe vertebral collapse , the high resistance to penetration and diffusion of the pmma was almost always overcome by reinserting the stylet into the cement - filled needle . 
by manually pushing the stylet with constant force within the needle , the right pressure was obtained for the outflow and appropriate penetration of the pmma , even in cases where this could not be achieved with the leveen syringe or pressure needle alone , not even when exerting maximum pressure . 
after treatment , all patients were prescribed bedrest in the supine position for 23 h and then mobilised with discharge on the same day or after a short stay of 12 days , depending on the clinical conditions of the patient following the procedure . 
prior to discharge , each patient was advised about simple precautions to consider in their daily routine regarding the risk of further vertebral fractures , which persists in the presence of osteoporosis , and encouraged not only to regularly take medication for osteoporosis prescribed by their specialist but also to undergo rehabilitation therapy as soon as possible . in order to evaluate the results of the procedure , we measured pain [ visual analogue scale ( vas ) ] and the degree of mobility before treatment , 24 h after treatment and during long - term follow - up by means of a telephone interview . after the first evaluation of all patients at 24 h , subsequently , only patients with at least 6 months of follow - up were included in the study . 
the vas score for pain was evaluated in a range from 0 to 10 , where 0 represents the absence of pain and 10 the worst and intolerable pain , on the basis of the pain intensity numeric rating scale . 
the degree of mobility was calculated in a range from 0 to 5 , where 0 = normal mobility , 1 = mobility with assistance , 2 = mobility only for brief periods with assistance , 3 = mobility only for vital daily activities or for appointments and with assistance , 4 = need for a wheelchair and 5 = bedridden status . 
the use of analgesics was classified in a range from 0 to 4 , where 0 = no use of medication , 1 = use of oral nonsteroid anti - inflammatory drugs , 2 = oral opioids according to need , 3 = programmed use of opioids and collasso somatico vertebrale o su metameri sovvertiti da patologia eteroplasica ove generalmente si preferito luso dellago di minor calibro . 
lago da vpp stato introdotto con laiuto di un martello ortopedico , ma dopo le fasi iniziali di esperienza con la procedura , nella gran parte dei casi il martello stato utilizzato solo per introdurre e indirizzare lago attraverso il peduncolo , mentre il successivo avanzamento allinterno del corpo vertebrale stato sempre effettuato agevolmente con manovre di avvitamento manuale senza alcun ricorso al dispositivo ortopedico . 
in caso di particolare fluidit del cemento o al momento in cui si rilevato limpegno di vene perivertebrali da parte di questo , si sempre interrotta immediatamente linfusione del pmma e atteso tra i 30 e i 45 secondi di polimerizzazione per ridurne la fluidit e pertanto il rischio di stravaso extrasomatico . 
in caso , invece , di elevata compattezza ossea , come spesso osservato nei crolli vertebrali severi , lelevata resistenza alla penetrazione e diffusione del pmma stata pressoch sempre vinta grazie al reinserimento del mandrino nellago riempito di cemento : spingendo infatti il mandrino manualmente e con forza costante allinterno dellago si ottenuta la giusta pressione con fuoriuscita e penetrazione adeguata del pmma anche in questi casi ove con la sola siringa di leveen o pistola a pressione ci non era ottenibile neanche esercitando la massima pressione . 
dopo il trattamento tutti i pazienti sono stati messi a riposo a letto in decubito supino per 23 ore e quindi mobilizzati con dimissione nella stessa giornata o dopo un breve ricovero di 12 giorni a seconda delle condizioni cliniche successive allintervento . 
prima della dimissione stato effettuato un colloquio con ogni paziente al fine di indicare alcune semplici precauzioni da osservare nellattivit quotidiana in considerazione del rischio di ulteriori fratture vertebrali che persiste in presenza dellosteoporosi e per incoraggiare , oltre alla regolare assunzione di eventuale terapia per losteoporosi prescritta dallo specialista , una fisioterapia riabilitativa pi precoce possibile . per lanalisi dei risultati sono stati misurati degli score per il dolore ( con una visual analogue scale [ vas ] ) e il grado di mobilit prima , a 24 ore dal trattamento e durante un follow - up a lungo termine per mezzo di intervista telefonica . 
i pazienti colpiti da nuove fratture vertebrali sintomatiche prima dei 6 mesi , a livelli differenti da quelli trattati , non sono stati inclusi nelle misurazioni del follow - up . 
sono state adottate scale numeriche ( per il dolore , la mobilit e luso di analgesici ) 1146 radiol med ( 2009 ) 114 : 11411158 4 = opioids with infusion pump . 
the effectiveness of pvp was determined on the basis of comparative results of paired data using a nonparametric test ( wilcoxon signed - rank test )  . statistical significance was established for a value of p < 0.05. 
no major complications were recorded at treatment or during follow - up that could be associated with the procedure , not even in patients suffering from cardiopulmonary disease such as severe chronic obstructive pulmonary disease ( ten cases )  . 
the examination performed during and immediately after treatment revealed a total of 82 mild cases of cement leakage gi usate in lavori con ampie popolazioni di pazienti [ 1 , 10 ]  . 
il vas score per il dolore stato valutato in un range da 0 a 10 , dove 0 rappresenta lassenza di dolore e 10 il dolore peggiore e insopportabile , in base alla scala pain intensity numeric rating scale ( pi - nrs ) ; il grado di mobilit stato calcolato in un range da 0 a 5 ( 0 = mobilit normale ; 1 = mobilit con assistenza ; 2 = mobilit solo per brevi periodi e con assistenza ; 3 = mobilit solo per attivit vitali quotidiane o per appuntamenti e con assistenza ; 4 = necessit della sedia a rotelle ; 5 = allettamento ) ; luso di analgesici stato classificato in un range scalare da 0 a 4 ( 0 = nessun uso di farmaci ; 1 = uso di antinfiammatori nonsteroidei orali ; 2 = oppiacei orali alla bisogna ; 3 = uso programmato di oppiacei ; 4 = oppiacei tramite pompa di infusione )  . 
2a , b trattamento di vertebra dorsale medio - alta ( d5 ) con approccio transpeduncolare ( a ) e controllo post - vpp tramite immagini di ricostruzione assiali mpr thick slab da acquisizione radiografica rotazionale ( b ) , ove si nota distribuzione del pmma anche lungo il tragitto transpeduncolare dellago . radiol med ( 2009 ) 114 : 11411158 1147 fig . 
in this case a bipedicular approach is needed because the narrow pedicles do not allow the direct insertion of the needle towards the midline of the vertebral body ( c )  . 
in questo caso necessario un approccio bi - peduncolare poich i peduncoli stretti non permettono di orientare lintroduzione dellago in direzione della linea mediana del corpo vertebrale ( c )  . 
dopo iniezione del pmma si ottiene una buona e simmetrica distribuzione intravertebrale del cemento ( d )  . outside the vertebral body , of which 80 cases were completely asymptomatic ( 39 cases of perivertebral leakage within the segmental veins ; 23 cases of intradiscal leakage ; 18 cases of posterior epidural leakage )  . 
non si sono registrate complicanze maggiori al momento del trattamento o nel follow - up che potessero essere attribuibili alla procedura , neanche in pazienti sofferenti di diverse patologie cardio - polmonari , quali bronco - pneumopatie ostruttive 1148 radiol med ( 2009 ) 114 : 11411158 fig . 
dopo vpp , la radiografia nella stessa proiezione mostra una distribuzione omogenea del cemento allinterno del corpo vertebrale e della fissurazione con ripristino in altezza di 2 mm ( b )  . radiol med ( 2009 ) 114 : 11411158 1149 table 2 technical results and complications of percutaneous vertebroplasty ( pvp ) site of pvp no . 
of treated vertebrae perivertebral leak posterior / foraminal leak intradiscal leak partial somatic height restoration complications thoracic lumbar - sacral dorsale lombare - sacrale tabella 2 risultati tecnici e complicanze della vertebroplastica percutanea ( vpp ) sede vpp numero vertebre leak trattate perivertebrale leak posteriore / foraminale leak intradiscale parziale ripristino complicanze somatico in altezza 1 radiculopathy 1 pulmonary microembolism ; 1 radiculopathy 1 radiculopatia 1 microembolia polmonare ; 1 radiculopatia fig . 
in one case ( a 67 - year - old woman with bone metastases from breast cancer ) , an asymptomatic pulmonary microembolism was observed , which caused no clinical symptoms at 20 months . 
in another two cases ( 64 - and 76 - year - old women with osteoporotic vcf ) , posterior intraforaminal leakage of pmma was croniche di grado severo ( 10 casi )  . 
il controllo durante e immediatamente dopo il trattamento ha mostrato un totale di 82 modesti stravasi extra - vertebrali di cemento , risultati del tutto asintomatici in 80 casi ( 39 perivertebrali allinterno delle vene segmentarie ; 23 intra - discali ; 18 posteriori epidurali )  . 
nei casi in cui si riscontrata la coesistenza di una fissurazione da osteonecrosi in una vertebra fratturata , il pmma si distribuito sempre in modo omogeneo e compatto allinterno della fissurazione ( 72 livelli ) , senza che si siano mai verificati stravasi posteriori e 1150 radiol med ( 2009 ) 114 : 11411158 observed that caused transient radiculopathy , which was resolved with oral nonsteroid anti - inflammatory drugs for 1 month in both patients ( table 2 )  . 
the mean mobility score prior to treatment was 2.1 ( sd = 1.6 ) , whereas at 24 h after treatment , it had fallen to 0.2 ( sd = 0.5 ) , which was also highly statistically significant ( p < 0.0001 ) in terms of improvement of the degree of mobility after comparison of the data . 
at the time of writing , a revision of our data suggested a total of 95 patients had undergone pvp at least 6 months earlier . of these , two patients could not be contacted for follow - up , two had died of cancer and eight had been affected by 14 new symptomatic vcfs on different vertebrae from those treated and arising between 1 and 10 months after the procedure . 
it should be noted that the lowest overall scores over time were reported by patients who during the follow - up period had undergone rehabilitation , and specifically hydrotherapy , proprioceptive and postural training and / or magnetic laser therapy . 
in 1 caso ( femmina , 67 anni , con metastasi scheletriche da carcinoma mammario ) si osservata una microembolia polmonare di pmma asintomatica che non ha determinato manifestazioni cliniche neanche nel follow - up fino a 20 mesi . 
in altri 2 casi ( femmine , rispettivamente di 64 e 76 anni , con fvc osteoporotiche ) si documentato uno stravaso di pmma posteriore intra - foraminale che ha causato una transitoria radiculopatia risolta per mezzo di antinfiammatori non - steroidei orali per un mese in entrambe le pazienti ( tabella 2 )  . 
stato possibile dimettere i pazienti nella stessa giornata in 28 / 120 casi mentre negli altri casi , la maggior parte dei quali con et superiore a 70 anni , si preferito un ricovero con osservazione clinica per ulteriori 24 ore a causa della particolare fragilit dei pazienti , per moderato dolore nella sede di accesso percutaneo ( al fine di escludere lo sviluppo di eventuali ematomi ) e / o per il recupero funzionale dopo la somministrazione di farmaci sedativi durante il trattamento . nella nostra popolazione di pazienti , il vas score medio misurato per il dolore prima del trattamento stato di 6 , 8 ( deviazione standard [ ds ] = 1 , 8 ) e di 1 , 7 ( ds = 1 , 5 ) a 24 ore dal trattamento ; il confronto dei due gruppi di dati appaiati ha prodotto come risultato un valore statistico estremamente significativo in termini di riduzione del dolore ( p < 0 , 0001 )  . 
lo score medio di mobilit prima del trattamento risultava di 2 , 1 ( ds = 1 , 6 ) , mentre a 24 ore dal trattamento sceso a 0 , 2 ( ds = 0 , 5 ) , anchesso risultando estremamente significativo ( p < 0 , 0001 ) in termini di miglioramento del grado di mobilit dopo comparazione dei dati . 
di questi , 2 pazienti non erano pi reperibili per il controllo di follow - up , 2 pazienti erano deceduti per cancro , 8 pazienti erano stati colpiti da 14 nuove fvc sintomatiche , incorse tra 1 e 10 mesi dopo la procedura , su metameri diversi da quelli precedentemente trattati . 
la valutazione del grado di mobilit ha documentato un significativo miglioramento in tutti i pazienti poich solamente 14 casi avevano ancora necessit costante di supporto con busto ortopedico mentre tutti gli altri a quel tempo avevano una mobilit normale o necessitavano del supporto ortopedico solo occasionalmente . 
lo score medio delluso di farmaci analgesici prima del trattamento era di 1 , 9 ( ds = 0 , 8 ) , mentre era di 0 , 6 ( ds = 0 , 7 ) a 6 mesi di distanza negli 83 pazienti reperibili , risultando in una significativa riduzione delluso di farmaci ( p < 0 , 0001 )  . importante notare come gli score complessivamente pi bassi a distanza di tempo siano stati riportati dai pazienti che nel corso del follow - up si siano sottoposti a terapia riabilitativa e nello specifico : idrochinesiterapia , ginnastica propriocettiva e posturale e / o magneto - laser - terapia . 
i singoli gruppi di dati utilizzati per valutare lefficacia della vpp per tutti i pazienti sono riportati nelle tabelle 35 . allinterno del gruppo controllato nel follow - up , 50 pazienti erano stati sottoposti a esami radiologici della colonna vertebrale ( rx , rm o tc ) in diverse epoche dopo il trattamento percutaneo e in gran parte nel nostro istituto ove stato possibile revisionare le immagini per mezzo dellarchivio informatico . 
after percutaneous treatment of l2 and l3 , a new symptomatic fracture of l1 occurred , and pvp was performed at this level ( a , arrow ) after 3 days from symptom onset . 
dopo il trattamento percutaneo di l2 e l3 si verificata una nuova frattura sintomatica di l1 ed stata eseguita vpp su questo livello ( a , freccia ) dopo 3 giorni dalla comparsa dei sintomi . 
una radiografia di controllo a 6 mesi rileva un nuovo ulteriore cedimento , stavolta asintomatico , di l1 precedentemente trattata ( b , freccia ) con severa riduzione in altezza del soma e segni di cedimento sulla limitante somatica inferiore di d12 . communication system ( pacs )  . 
la vpp oggigiorno considerata una tecnica mininvasiva sicura ed efficace per il trattamento delle fratture vertebrali sintomatiche non responsive alla terapia medica conservativa ed caratterizzata da un rischio di complicanze estremamente basso . 
complicanze gravi sono riportate [ 12 , 13 ] , ma la maggior parte degli studi concorde sul fatto che tali evenienze possono essere ridotte al minimo utilizzando sistemi radiologici di guida di elevata qualit ed eseguendo le procedure in una sala angiografica , dove lapparecchiatura fluoroscopica migliore , piuttosto che in una sala operatoria dove sono riportate le complicanze pi gravi a causa della qualit inferiore del tubo a c [ 1 , 2 , 9 , 1316 ]  . 
la vpp pu essere eseguita in regime di day - surgery con significativo contenimento dei costi ospedalieri , e si dimostra essere una tecnica rapida e facile in mani esperte . 
pvp is today considered to be a safe and effective minimally invasive technique for treating symptomatic vertebral fractures refractory to conservative medical treatment and is characterised by an extremely low risk of complications . 
severe complications have been reported [ 12 , 13 ] , but most studies agree that these outcomes can be minimised with the use of high - quality radiological guidance systems and by performing the procedure in an angiography suite where the fluoroscopy equipment is better , rather than in an operating theatre where the most severe complications have been reported due to the inferior quality of the c - arm device [ 1 , 2 , 9 , 1316 ]  . 
 pvp can be performed as a day - surgery procedure with significant reductions in hospital costs , and it has proved to be a rapid and easily performed technique in expert hands . the calculation of the mean cost of materials we used for each procedure falls within the range estimated by the single commission for medical equipment of the italian ministry of health [ 17 ]  . 
in most cases , because all that was required was a vertebroplasty needle , a maximum dose of 5 ml of pmma and a leveen syringe for the injection , with no need for complex and expensive sets , costs were able to be kept within the minimum of the estimated range . percutaneous access and the absence of general anaesthesia , together with the possibility of treating elderly patients with no apparent age limit , are some of the main advantages of the technique . 
severe vertebral collapse ( < 1 / 3 of the normal vertebral height ) is considered by some authors to be a relative contraindication to the procedure due to technical difficulties regarding the approach [ 9 , 18 ] , as is the high risk in treating patients with severe cardiopulmonary disease due to the possibility of fat embolism and the cardiotoxic effect of pmma [ 14 , 19 , 20 ]  . 
in our series , we believe that the use of high - resolution digital fluoroscopy as the guidance system , the complete and continuous monitoring of vital signs , the possibility of a unilateral approach in most cases and the injection of cement limited to a maximum volume of 5 ml in a single vertebral body are decisive features for minimising risks and adverse effects . this , therefore , allowed us to treat even fragile patients with chronic obstructive pulmonary disease and cases of severe vertebral collapse without the onset of severe complications . our findings show that the use of the orthopaedic hammer , which is often poorly tolerated by patients from a psychological point of view , can be limited to introducing the needle . 
this favours greater tolerance of the procedure and as a consequence improved patient compliance , and 1153 medio dei materiali da noi utilizzati per singola procedura rientra nel range stimato dalla commissione unica dei dispositivi medici del ministero della salute ( sito web , sul portale del ministero della salute : lute.it / dispositivi / paginainterna.jsp ? id = 88&menu = commissione )  . 
nella maggior parte dei casi , essendo sufficiente lutilizzo dellago per vertebroplastica , una dose massima di 5 ml di pmma e la siringa di leveen per liniezione senza necessario ricorso a set pi complessi , articolati e dispendiosi , tali costi possono essere contenuti entro il minimo del range stimato . laccesso percutaneo e nessuna necessit di anestesia generale , insieme alla possibilit di trattare pazienti anziani senza apparente limite det , rappresentano alcuni dei principali vantaggi della tecnica . 
il collasso vertebrale severo ( < 1 / 3 della normale altezza somatica ) considerato da alcuni autori una relativa controindicazione alla procedura a causa delle difficolt tecniche di approccio [ 9 , 18 ] , cos come da considerarsi ad alto rischio il trattamento di pazienti con gravi malattie cardio - polmonari a causa della possibile embolia grassosa e delleffetto cardiotossico del pmma [ 14 , 19 , 20 ]  . 
nella nostra serie , riteniamo che lassistenza della fluoroscopica digitale ad alta risoluzione come sistema di guida , il completo e continuo monitoraggio dei parametri vitali , linutilit di un approccio bilaterale nella maggior parte dei casi e liniezione di cemento limitata ad un volume massimo di 45 ml in un singolo corpo vertebrale , siano stati decisivi a minimizzare i rischi e gli effetti avversi , consentendoci pertanto di trattare anche pazienti fragili con bronco - pneumopatie ostruttive croniche e casi di vertebra plana senza insorgenza di complicanze gravi . 
lintroduzione manuale pressoch sempre agevole e meno dolorosa e favorisce pertanto una maggiore tolleranza alla procedura a cui consegue una migliore collaborazione da parte del paziente , permettendo di ridurre i tempi di esecuzione e il ricorso a farmaci sedativi . 
 in caso di peduncoli vertebrali molto stretti , come a livello di vertebre toraciche alte , pu essere necessario un approccio paravertebrale o intercosto - vertebrale , ma ci comporta un maggiore rischio di pneumotorace o ematoma paraspinale [ 9 , 16 ]  . 
la buona visualizzazione fluoroscopica della struttura anatomica vertebrale ci ha permesso di trattare ogni paziente con un sicuro accesso trans - peduncolare anche sulle vertebre toraciche pi alte , che nella nostra serie stato a livello di d4 in 2 casi . dibattuto se debba essere somministrato un antibiotico al paziente che si sottopone a vpp e alcuni autori sostengono che la profilassi sia un imperativo solo per pazienti immunocompromessi [ 9 ]  . 
in accordo con i lavori maggiori 1154 radiol med ( 2009 ) 114 : 11411158 therefore reduces procedure times and the need for sedatives . in the presence of very narrow vertebral pedicles , as for example at the level of the high thoracic vertebrae , a paravertebral or intercostal - vertebral approach may be required , although this increases the risk of pneumothorax or paraspinal haematoma [ 9 , 16 ]  . 
good fluoroscopic visualisation of the vertebral structures allowed us to treat each patient with safe transpedicular access even in high thoracic vertebrae , which in our series was at the level of t4 in two cases . it is debatable as to whether antibiotics should be administered to patients undergoing pvp , and some authors suggest prophylaxis is a requirement only in immunocompromised patients [ 9 ]  . 
in agreement with the major studies to date [ 1 , 20 ] , we prefer to administer antibiotics to all patients prior to the procedure to avoid infections , a rare complication of pvp but one of the most feared , which may necessitate neurosurgery . our findings regarding the effectiveness of pvp in producing long - term pain relief from vcfs are in accordance with the literature [ 1 , 1416 , 1820 ]  . 
a significant improvement in mobility and reduction in the use of analgesics have also been reported by most authors , with an overall improvement of the patients quality of life . 
although some studies report better results associated with fewer complications in osteoporotic fractures compared with osteolytic fractures [ 16 ] , we found no significant differences in our series in terms of pain reduction and complications after pvp , regardless of the underlying disease . 
our data are therefore similar to most of the other studies in the literature , which report favourable outcomes in a variety of patient subgroups [ 1 , 15 ]  . 
this finding was supported by 21 cases in our series that showed a significant reduction in pain after treating an old vcf that had been symptomatic for more than 1 year . as stated in other studies [ 1 , 14 , 16 ] , we believe that the effectiveness and favourable clinical outcome of pvp are closely related to careful patient selection established by preliminary clinical and radiological workup . 
in particular , where available , spinal mr was considered the modality of choice for establishing the correct indication for the procedure on the basis of the society of interventional radiology guidelines [ 2 ]  . 
in agreement with most authors , we believe that the presence of signal hyperintensity due to bone marrow oedema on t2 - weighted and stir sequences is a determining sign for establishing the indication for pvp and predicting the positive outcome of the procedure . the reason pvp is able to produce its analgesic effect on [ 1 , 20 ] noi preferiamo la somministrazione dellantibiotico prima della procedura in tutti i casi , al fine di prevenire infezioni , una complicanza rara , ma tra le pi temibili della vpp , che pu richiedere un intervento neurochirurgico . i nostri risultati riguardanti lefficacia della vpp nel produrre un prolungato sollievo dal dolore per le fvc sono in linea con la letteratura [ 1 , 1416 , 1820 ]  . 
anche il significativo miglioramento della mobilit e la riduzione delluso di farmaci analgesici sono riportati dalla maggior parte degli autori con un complessivo miglioramento della qualit di vita dei pazienti . sebbene alcuni studi mostrino migliori risultati associati a minori complicanze nelle fratture osteoporotiche piuttosto che in quelle legate a patologie tumorali [ 16 ] , nella nostra serie non abbiamo trovato significative differenze in termini di riduzione del dolore e complicanze dopo vpp qualsiasi fosse la patologia di base . 
lo stesso risultato stato ottenuto in 21 dei nostri casi che hanno mostrato una significativa riduzione del dolore dopo trattamento di vecchie fvc con sintomatologia che perdurava da almeno 1 anno . come gi espresso in altri lavori [ 1 , 14 , 16 ] , riteniamo che lefficacia della vpp e lesito clinico favorevole siano strettamente dipendenti da unaccurata selezione dei pazienti stabilita dal work - up clinico e radiologico preliminare . 
in particolare , quando disponibile , la rm spinale da considerarsi la metodica di scelta al fine di stabilire la corretta indicazione alla procedura sulla base delle linee guida della society of interventional radiology [ 2 ]  . 
in accordo con la maggior parte degli autori , riteniamo che la presenza delliperintensit di segnale dovuta ad edema intraspongioso sulle sequenze t2w e stir , rappresenti un segno determinante per stabilire lindicazione alla vpp e predittivo dellesito positivo della procedura . non ancora chiara la ragione per cui la vpp sia una tecnica in grado di produrre un effetto antalgico nelle fvc . sono stati proposti diversi meccanismi che includono la stabilizzazione della frattura , la necrosi termica e la chemiotossicit tissutale , delle terminazioni nervose e dei recettori intraossei del dolore [ 14 , 16 , 20 ]  . un problema emergente da numerosi studi riguarda il rischio di sviluppare nuove fratture vertebrali dopo trattamento con vpp . 
nella nostra casistica , dopo il follow - up di 6 mesi , la percentuale di pazienti nei quali si sono verificate nuove fratture vertebrali dopo la procedura a livelli diversi da quelli trattati stata del 6 , 7%  . 
 [ 1 ] hanno riportato l8% di nuove fratture dopo un follow - up medio di 7 mesi ; la percentuale di nuove fratture riportate radiol med ( 2009 ) 114 : 11411158 1155 vcfs is still not clear . 
a number of mechanisms have been proposed , including fracture stabilisation , thermal necrosis and tissue , nerve endings and intraosseous pain receptors chemiotoxicity [ 14 , 16 , 20 ]  . a problem that has emerged from numerous studies regards the risk of developing new vertebral fractures after pvp treatment . 
in our series , after 6 months of follow - up , the percentage of patients in whom new vertebral fractures occurred after the procedure at levels other than those treated was 6.7%. 
recent studies suggest that increased rigidity of the treated vertebra , leakage of intradiscal cement , an elevated degree of restoration of the height of the vertebra or treating vertebral bodies at the thoracolumbar junction [ 27 , 28 ] may be risk factors for new vertebral fractures at levels adjacent to those treated and that a significant restoration of the anterior vertebral body height increases the risk of further fractures in the treated vertebrae [ 29 ]  . 
in our series we noted that all new fractures in previously treated vertebrae ( five cases ) occurred in the group of ten patients who underwent early pvp at around 1 week from symptom onset , but we were unable to establish whether this coincidence can be considered a causative factor of new fractures due to the small number of cases . with regard to the problems of new fractures , we agree with baroud et al . 
as pvp is a relatively new technique , prospective studies are required to conclusively define the cause ( s ) of new fractures at different levels and on previously treated vertebrae . 
on the basis of these preliminary studies , and given the known analgesic and stabilising effect of pvp regardless of the volume of pmma injected [ 14 , 16 , 31 ] , we believe that the volume of cement injected should be limited to a precautionary 23 ml , particularly during the treatment of vertebrae at the thoracolumbar junction , to reduce the risk of new fractures on adjacent vertebral bodies . 
this conservative approach also reduces the risk of extravertebral leakage of cement and fat embolism [ 1 , 14 , 31 ]  . in our study , we observed the best long - term results in patients who underwent rehabilitation therapy during the follow - up period . 
infatti , dimostrato che i pazienti che sviluppano una fvc da osteoporosi sono a rischio di nuove fratture entro un anno , con unincidenza del 19 , 2% [ 26 ]  . 
recenti studi suggeriscono che unaumentata rigidit della vertebra trattata , uno stravaso di cemento intradiscale , un elevato grado di ripristino in altezza del soma o il trattamento di metameri alla giunzione toracolombare [ 27 , 28 ] possano costituire dei fattori di rischio per nuove fratture vertebrali a livelli adiacenti a quelli trattati e che un significativo recupero in altezza del muro somatico anteriore aumenti il rischio di successive fratture in vertebre gi trattate [ 29 ]  . 
nella nostra serie abbiamo notato che tutti i nuovi cedimenti somatici in vertebre gi trattate ( 5 casi ) si sono verificati nel gruppo di 10 pazienti sottoposti a vpp precocemente a circa una settimana dallinsorgenza dei sintomi , ma non siamo in grado di stabilire se questa coincidenza possa ritenersi una possibile condizione causativa di nuova frattura in relazione allesiguo numero di casi . riguardo alla problematica delle nuove fratture concordiamo con lasserzione di baroud et al . 
 [ 30 ] per cui sebbene siano in aumento prove a supporto di alcune ipotesi riguardanti i fattori di rischio , bisogna essere cauti : la vpp una tecnica relativamente nuova e sono necessari studi prospettici per definire in modo conclusivo la / e causa / e di nuove fratture a livelli differenti e sulle stesse vertebre gi trattate . 
sulla base di questi studi preliminari ed essendo noto che leffetto antalgico e la stabilizzazione possono ottenersi dopo vpp indipendentemente dal volume di pmma iniettato [ 14 , 16 , 31 ] , la nostra opinione che si debba considerare in modo precauzionale di iniettare un volume di cemento limitato a 23 ml , in particolare durante il trattamento di vertebre al passaggio toraco - lombare , al fine di ridurre il rischio di nuove fratture su metameri adiacenti . 
questo approccio cauto riduce anche il rischio di stravasi di cemento extra - vertebrali e di embolia grassosa [ 1 , 14 , 31 ]  . nel nostro studio abbiamo osservato i migliori risultati a distanza nei pazienti che nel corso del follow - up avevano eseguito dei cicli di fisioterapia riabilitativa . 
il paziente colpito da fratture che hanno richiesto limmobilizzazione , lallettamento o comunque luso del busto ortopedico ha infatti necessit di ristabilire un buon tono ed equilibrio muscolare e la ripresa di una normale attivit fisica mirando a riacquistare lindipendenza e 1156 radiol med ( 2009 ) 114 : 11411158 an integral part of the postoperative management protocol for pvp . 
the patient suffering from fractures who required immobilisation , bedrest or the use of an orthopaedic brace in fact needed to reestablish good muscular tone and equilibrium and the recovery of normal physical activity and reacquire the independence and autonomy that the condition had limited . 
the probability of this being achieved was greater thanks to this therapy , which above all reduces the risk of new vertebral fractures over time [ 32 , 33 ]  . 
by relieving pain and stabilising the fracture , pvp in turn enabled the patient to undertake physiotherapy in a reduced time frame and without limitations . there are a number of limitations to our study . 
firstly , with regard to the technique , we were unable to make a comparison with a group of patients treated under ct guidance , because all of our cases were treated under fluoroscopic guidance . 
ct is considered the best guidance system for precise introduction of the pvp needle [ 9 , 34 ] , but in our opinion , and in agreement with most authors , most interventional radiologists are well versed with fluoroscopy , and this technique is fast , inexpensive and reliable as a guidance system for pvp if the operator has a good understanding of the radiographic anatomical landmarks . 
although both techniques are valid , the preference is obviously also influenced by the possibility of access and use of one or the other in accordance with type of activity and diagnostic workload of the individual centres and should be subject to the good quality of the equipment . the second limitation of our study was the absence of a comparison with a population treated with conservative therapy in order to establish whether pvp is more effective with respect to traditional medical treatment . 
during conservative therapy , complications and worsening of vertebral collapse may arise , which suggest early referral for pvp in patients at risk of prolonged immobilisation and who need high doses of analgesics [ 2 , 16 ]  . 
in addition , as occurred in our series , the patients are generally satisfied with the procedure , and they are the ones to request new treatment in the event of new symptomatic fractures . lastly , we were unable to determine the clinical importance of changes in the degree of pain after pvp because the pain intensity numerical rating scale does not provide information regarding the subjective nature of the paas with anselmetti et al . 
on a large patient population that puts forward a possible standard definition of major clinical improvement in chronic pain by establishing that a mean reduction of lautonomia che la patologia aveva limitato . 
la vpp , dal canto suo , alleviando il dolore e stabilizzando la frattura , permette al paziente di avviare in breve tempo la fisioterapia e affrontarla senza limitazioni . analizziamo alcuni limiti del nostro studio . 
innanzitutto , riguardo alla tecnica , non abbiamo termini di comparazione con un gruppo di pazienti trattati sotto guida tc giacch tutti i nostri casi sono stati trattati sotto guida fluoroscopica . 
la tc considerata il sistema di guida migliore per una esatta introduzione dellago da vpp [ 9 , 34 ] , ma nella nostra opinione e in accordo con la maggior parte degli autori , la gran parte dei radiologi interventisti ha unelevata dimestichezza con la fluoroscopia e questa metodica veloce , poco costosa e affidabile come sistema di guida per la vpp se loperatore ha una buona conoscenza dei reperi anatomici radiografici . 
se pur valide entrambe le metodiche , la preferenza ovviamente determinata anche dalla possibilit di accesso e utilizzo delluna o dellaltra a seconda del tipo di attivit e carico diagnostico dei singoli centri , e deve comunque essere subordinata alla buona qualit dellapparecchiatura . il secondo limite del nostro lavoro consiste nel mancato confronto con una popolazione trattata con terapia conservativa al fine di stabilire se la vpp sia pi efficace rispetto al trattamento medico tradizionale . 
tuttavia , alcuni studi prospettici preliminari , randomizzati e non - randomizzati [ 3537 ] , hanno comparato gruppi di pazienti sottoposti a vpp con pazienti trattati per mezzo della terapia conservativa . 
durante la terapia conservativa possono verificarsi complicanze e peggioramento del collasso vertebrale che suggeriscono lindicazione alla vpp precoce in pazienti a rischio di prolungata immobilizzazione e che necessitano di elevate dosi di farmaci analgesici [ 2 , 16 ]  . 
inoltre , come accaduto nella nostra casistica , i pazienti sono generalmente soddisfatti della procedura e richiedono essi stessi il nuovo trattamento in caso di nuove fratture sintomatiche . infine , non abbiamo potuto determinare limportanza clinica delle modificazioni del grado di dolore dopo vpp giacch la pi - nrs non fornisce informazioni sulla soggettiva natura del dolore . 
 [ 38 ] su di unampia popolazione , il quale propone una possibile definizione standard di importante miglioramento clinico del dolore cronico stabilendo che una riduzione media di circa il 30% nella pi - nrs rappresenta una differenza clinicamente importante . in conclusione , la vpp si dimostra essere una terapia radiol med ( 2009 ) 114 : 11411158 1157 approximately 30% in the pain intensity numerical rating scale is a clinically important difference [ 38 ]  . in conclusion , pvp has been shown to be an effective , safe , relatively inexpensive and minimally invasive procedure for symptomatic vcfs , with an extremely low rate of complications when performed under the guidance of goodquality equipment , such as low - dose digital fluoroscopy , and by experienced operators . 
the technique may be indicated as a day - surgery procedure when the clinical conditions of the patient allow it and are thoroughly evaluated and when vital signs are monitored before , during and after the procedure . 
careful selection of patients , evaluation of the correct indications and postoperative management that includes rehabilitation therapy are crucial for increasing the probability of a favourable outcome for the patient in both the short and long term . efficace , sicura , poco costosa e mininvasiva per le fvc sintomatiche , con una percentuale di complicanze estremamente bassa qualora eseguita sotto la guida di apparecchiature di buona qualit , quale la fluoroscopia digitale a bassa dose , e da parte di operatori esperti . 
la procedura effettuabile in regime di day - surgery qualora le condizioni cliniche del paziente lo consentano e siano valutate in modo accurato e quando i parametri vitali sono monitorati prima , durante e dopo la procedura . 
the choice made by radiologists in moral dilemmas is inspired by an adherence to moral principles , which in italy and elsewhere refer to the judaeo - christian tradition or to neo - darwinian relativism . whatever the choice , the radiologist is bound to adhere to that choice and to provide the patient with all the relevant information regarding his or her state of health . riassunto il continuo aumento della richiesta di esami radiologici che si verifica in tutti i paesi economicamente sviluppati riconosce tra le sue cause lintervento attivo dei pazienticonsumatori . 
il consumismo pone i radiologi di fronte ad un dilemma etico , tra il principio di autonomia e gli altri principi etici di beneficenza , non maleficenza e giustizia . la scelta operata da ciascun radiologo nei dilemmi morali sar ispirata dalladesione a principi morali , che nella nostra societ si riferiscono alla tradizione giudaicocristiana , o al relativismo neo - darwiniano . 
qualunque sia la scelta , il radiologo tenuto a rendere conto di essa e a comunicare al paziente tutte le informazioni rilevanti per il suo stato di salute . keywords ethics radiology medical consumerism autonomy accountability parole chiave etica radiologia consumismo medico autonomia accountability is there a problem of ethics in radiology ? esiste un problema etico in radiologia ? like all medical practitioners , the radiologist is faced with numerous ethical problems on a daily basis . 
this rather selfevident statement should not overlook the fact that often the healthcare professional , pressed by the needs of providing the service , has little time to dedicate to an ethical assessment and is forced to act upon impulse , following habitual actions or going along with the prevailing pressures . 
in the ordered sequence of operations that a modern radiological unit performs , it may appear that there is no margin for doubt , or even that it does not exist . 
of course , that is not so . the reason we are interested in this situation is that it il medico radiologo , come ogni medico , chiamato a misurarsi quotidianamente con numerosi problemi etici . 
questa affermazione banale non deve far dimenticare che spesso il sanitario , pressato dalle esigenze del servizio , ha ben poco tempo da dedicare allanalisi etica ed costretto ad agire dimpulso , seguendo labitudine o assecondando le pressioni prevalenti . 
nella sequenza ordinata di operazioni che una moderna sala radiologica esegue , pu cos sembrare che non vi sia alcuno spazio per il dubbio , o addirittura che esso non esista . 
la ragione per cui , come medici del lavoro , ci interessiamo di tale situazione che essa costituisce una 1174 radiol med ( 2009 ) 114 : 11731181 constitutes an effective threat to the health of healthcare professionals . moral conflicts can lead to stress and burnout in physicians , a stress - response syndrome characterised by emotional exhaustion , depersonalisation and reduced personal realisation . 
a recent norwegian study reported that more than 50% of medical practitioners are aware of having to professionally act in a manner contrary to their conscience , and that this is a cause of tension [ 1 ]  . 
the prospect of revealing the error , or even having to report behaviour of a colleague who is noncompliant with professional standards , is a serious decision that may compromise ones career or working conditions and is therefore highly stressful . 
specific research indicates that healthcare professionals are relatively intolerant of criticism of their own work and that in some cases medical practitioners avoid turning to ethics committees precisely because they fear criticism or hostility from their colleagues [ 2 ]  . 
in contrast , the less tolerant environments , in which discussion of ethical problems is more likely to be stifled both before relevant decisions are made and after the controversy has arisen , are a greater threat for the psychophysical well - being of those working in them . on a more general note , healthcare professionals complain of the lack of time available for caring for patients as they would like to , and they lament the commitments in contrast with their professional obligations . 
the time dedicated to administrative and bureaucratic activities , which is constantly on the increase in part due to the growing need for transparency limits the time available for caring for patients . 
for all physicians , ideal ethics constitute an important part of ones professional image , and being constrained to working in a manner out of line with these ideals can significantly reduce job satisfaction and induce stress [ 1 ]  . 
it can be said , therefore , that quality in medicine does not only depend on professional attitude but also on the ability to effettiva minaccia per la salute degli operatori . 
 i conflitti morali possono determinare nei medici uno stato di stress e la comparsa del burnout , una sindrome di risposta allo stress caratterizzata da esaurimento emotivo , depersonalizzazione e ridotta realizzazione personale . 
una recente indagine sui medici norvegesi ha documentato che oltre la met di essi consapevole di aver dovuto agire professionalmente in modo contrario alla propria coscienza , e che tale fatto motivo di tensione [ 1 ]  . 
tra i momenti di conflitto pi frequentemente indicati vi la necessit di affrontare errori clinici commessi da colleghi . lipotesi di rivelare lerrore , o addirittura di dover segnalare la condotta non conforme agli standard o alle norme deontologiche di un collega , ritenuta una decisione grave , suscettibile di compromettere la propria carriera o la condizione lavorativa , e quindi fortemente stressante . ricerche specifiche indicano che i medici hanno pochissima tolleranza per le critiche al proprio operato , e che in alcuni casi i medici evitano di rivolgersi ai comitati etici proprio perch temono critiche o ostilit da parte dei colleghi [ 2 ]  . daltro canto , gli ambienti di lavoro nei quali si soliti formulare e ricevere critiche sono anche quelli caratterizzati da maggiore collegialit e sostegno per gli errori , e quindi i meno stressanti . 
al contrario , gli ambienti meno tolleranti , nei quali si soliti sopprimere la discussione sui problemi etici sia prima di prendere decisioni rilevanti che dopo che la controversia si presentata , risultano maggiormente rischiosi per il benessere psicofisico di chi lavora . pi in generale , i medici lamentano la mancanza di tempo per prendersi cura come dovrebbero dei pazienti e gli impegni contrastanti con i propri doveri professionali . 
il tempo dedicato ad attivit amministrative e burocratiche , in continuo aumento anche per le accresciute esigenze di trasparenza , riduce la possibilit di occuparsi dei pazienti . inoltre i medici sentono come un problema rilevante dal punto di vista etico lesistenza di lunghe liste di attesa e il fatto che pazienti pi forti ( ad esempio , solventi ) hanno spesso la priorit rispetto ai pi bisognosi . le condizioni di lavoro di molti medici , caratterizzate da carichi di lavoro eccessivi e ristrettezza di tempo , possono ostacolare il raggiungimento dei desiderati livelli professionali ed etici nellattivit lavorativa . 
per tutti i medici , gli ideali etici costituiscono una parte importante della propria immagine professionale , ed essere costretti a lavorare in modo da non aderire a questi ideali pu significativamente ridurre la soddisfazione tratta dal lavoro ed indurre uno stato di stress [ 1 ]  . 
si pu ben dire quindi che la qualit in medicina non dipende solo dalle attitudini radiol med ( 2009 ) 114 : 11731181 1175 identify and resolve ethical conflicts [ 1 ]  . a recent study of ours on italian radiologists and radiation therapists reported an increase in work - related stress . this has been due on the one hand to an increasing workload , often in the presence of limited resources , and on the other to the introduction of increasingly sophisticated and invasive techniques that require greater professional commitment , and has increasingly penalised the time available to the physician to evaluate the examination or the treatment plan , and definitively to treat the patient [ 3 ]  . 
this involves issues , such as allocation of healthcare resources , which regard all aspects of medicine and especially involves radiology in relation to the high cost of some examinations and their limited availability . 
an ethical conflict can arise between the principle of autonomy of the patient requesting an inappropriate examination on the one hand , and the principles of nonmaleficence towards the patient , who would be unnecessarily exposed to the undesired effects of the radiological technique , and justice and beneficence towards other patients , who may have a greater need for the examination than the other . 
similar considerations can be made with regard to defensive radiology , which is responsible for a squandering of resources motivated by the sole intent of protecting oneself from possible accusations of malpractice . professionali , ma anche dalla capacit di identificare e risolvere i conflitti etici [ 1 ]  . una nostra recente indagine sui medici radiologi e radioterapisti italiani ha evidenziato lemergere di un accentuato stress da lavoro , riconducibile da un lato alle crescenti esigenze produttive , spesso in limitatezza di risorse , dallaltro allintroduzione di tecniche sempre pi sofisticate e di metodiche invasive , che richiedono un impegno professionale crescente , penalizzando sempre di pi il tempo a disposizione del medico per valutare lesame o il piano terapeutico , e in definitiva per la cura del malato [ 3 ]  . 
si tratta spesso di argomenti , come quelli relativi allallocazione delle risorse sanitarie , che riguardano tutta la medicina nel suo insieme , e coinvolgono la radiologia soprattutto in relazione allelevato costo di taluni esami ed alla loro limitata disponibilit . 
un conflitto etico pu sorgere tra il principio di autonomia del paziente che richiede un esame non appropriato ed i principi di non maleficenza verso lo stesso paziente , che sarebbe esposto indebitamente agli effetti indesiderati della tecnica radiologica , e i principi di giustizia e beneficenza verso altri pazienti che potrebbero avere maggiore bisogno dellesame . 
analoghe considerazioni possono essere fatte per la radiologia difensiva , che responsabile di una dissipazione di risorse motivata solo dallintento di difendersi da possibili accuse di malpractice . healthcare consumerism in radiology il consumismo sanitario in radiologia in radiology , the problem of healthcare consumerism is particularly evident . 
the number of examinations is on the increase at an annual rate of 5%11% in all developed countries , and the request appears to be infinite [ 4 ]  . 
multiple factors are responsible for this trend , the main ones being the development of new technology , the use of reimbursement systems per service , the endorsement of self - prescription by general practitioners , defensive medicine and defensive radiology . 
undeniably , the autonomy of the patient , with the abandonment of the traditional paternalism that left the power to decide to the physician , has led to an acceleration of the phenomenon . 
an increasing number of patients see the acquisition of computed tomography ( ct ) or magnetic resonance ( mr ) images a compulsory act and they feel disregarded if the physician fails to prescribe thein addition , many patients self - prescribe examinations on the basis of the conviction in radiologia il problema del consumismo sanitario particolarmente presente . 
molteplici fattori sono responsabili di questa tendenza : lo sviluppo di nuove tecnologie , luso di sistemi di rimborso a prestazione , lavallo alle auto - prescrizioni da parte dei medici di medicina generale , la medicina difensiva e radiologia difensiva sono le principali . 
sempre pi numerosi sono i pazienti che percepiscono lesecuzione di immagini di tomografia computerizzata ( tc ) o risonanza magnetica ( rm ) come un atto dovuto , e che si sentono trascurati se il medico rifiuta di prescriverli . 
molti pazienti , inoltre , si auto - prescrivono gli esami , sulla base del concetto che 1176 radiol med ( 2009 ) 114 : 11731181 that one examination too many is better than one too few . moreover , although the harmful effects of ionizing radiation have been known for a long time , and provisions have been made in italy that proscribe the unjustified use of diagnostic imaging , there appears to be no evidence of the application of professional or legal sanctions for unnecessary examinations . 
as a result , radiological examinations of the chest are indiscriminately performed as a matter of routine , even prior to a clinical examination . a number of competing factors are at play that lead to the failure of physicians to oppose performing clinically useless examinations . 
traditionally , radiologists have felt that concerns over patient autonomy are a useless waste of time [ 4 ] and that informing patients about the risks of a radiological examination is a way of making them unnecessarily apprehensive or even inducing them to refuse the examination . the individualistic interpretation of the principle of autonomy ends up downgrading the relationship between patient and physician to one between patient and technician , whereby the sole task of the radiologist is to satisfy the request . 
the systems of reimbursement for services encourage consumerism and competition between radiologists , with the effect of further downgrading the doctorpatient relationship to one of trade . on the other hand , it has been observed that patients are considered to be free to autonomously decide about much more relevant healthcare matters , such as abortion , so that there appears little ground for limiting them with regard to radiological examinations [ 5 ]  . standing against patient autonomy is the fact that patient knowledge is never neutral , balanced or based on evidence . often , radiology services do not provide adequate information in that the information is aimed at reassuring the patient or it does not accompany a verification of what the patient has understood . the prerequisite for an effectively autonomous decision is a state of psychophysical balance by the person making it . even healthy and asymptomatic subjects can exhibit a state of anxiety or fear of disease that may influence choice . patients may be subject to pressure from family members or the mass media , through which interest groups spread the notion that benefits may be obtained from new technology , particularly if this can be obtained without an economic cost , within the national health service . of course , patient autonomy offers important benefits for the healthcare profession . 
leaving the patient free to choose is a way of transferring professional responinduced meglio effettuare un controllo in pi che uno di meno di quello che in un secondo tempo si rivela necessario . 
per di pi , nonostante gli effetti nocivi delle radiazioni ionizzanti siano note da tempo , e siano in vigore nel nostro paese provvedimenti che proscrivono il ricorso ingiustificato a diagnostica radiologica , non si ha notizia dellapplicazione di alcuna sanzione professionale o legale per esami non necessari . 
si assiste cos allesecuzione di esami radiologici del torace come parte di routine indiscriminate , addirittura prima di una visita medica con finalit di certificazione . numerosi fattori concorrono perch i medici non si oppongano allesecuzione di esami clinicamente inutili . tradizionalmente i radiologi hanno sempre ritenuto che le preoccupazioni per lautonomia del paziente siano una inutile perdita di tempo [ 4 ] e che informare i pazienti sui rischi degli esami radiologici sia il modo di renderli inutilmente apprensivi o addirittura indurli a rifiutare lesame . linterpretazione individualistica del principio di autonomia finisce per ridurre il rapporto tra paziente e medico ad un rapporto tra paziente e tecnico , nel quale al radiologo spetta solo il compito di soddisfare la richiesta . 
i sistemi di rimborso a prestazione incoraggiano il consumismo e la competizione tra radiologi , con leffetto di appiattire ulteriormente la relazione medico - paziente ai soli aspetti mercantili . daltro canto stato osservato che i pazienti sono ritenuti liberi di decidere autonomamente su questioni sanitarie molto pi rilevanti , come ad esempio laborto , e non si vede perch debbano essere limitati nelle indagini radiologiche [ 5 ]  . contro lautonomia sta il fatto che le conoscenze del paziente non sono mai neutrali , bilanciate o basate sullevidenza . 
i servizi di radiologia spesso non forniscono informazioni adeguate , in quanto spesso le informazioni sono rivolte a rassicurare il paziente , o non si accompagnano ad una verifica di ci che il paziente ha compreso . 
 il pre - requisito perch una decisione sia effettivamente autonoma lo stato di equilibrio psicofisico di chi la adotta . anche i soggetti sani e asintomatici possono presentare uno stato dansia o di patofobia che pu influenzare la scelta . 
i malati , a maggior ragione , possono essere soggetti a pressioni da parte di familiari o mass - media , tramite i quali gruppi di interesse propalano lidea che si possa trarre vantaggio da ogni nuova tecnologia , soprattutto se questa ottenibile senza esborso economico , in regime di servizio sanitario nazionale . lautonomia del paziente offre naturalmente importanti vantaggi al medico . 
in this way , moreover , the declaimed autonomy of the patient ends up becoming an insidious form of paternalism aimed at protecting the radiologist . the increasing use of radiology leads to an inevitable reduction in resources earmarked for other healthcare activities . 
in this way , the autonomy of some patients ends up limiting the autonomy of others and violating the principle of equity . consumerism does not only concern radiology but all branches of medicine . 
the diagnosis of spastic colitis , which regards one third of all gastroenterological disease [ 7 ] , binds the physician to prescribing antispastic medication , which has not proven to be more effective than a placebo and which may have side effects . 
the failure to prescribe , in addition to being unacceptable for the patient , could expose the physician to legal consequences . how can ethical problems be resolved ? it seems clear that the problem of allowing access to diagnostic technology or treatment of unproven effectiveness or uncertain benefit essentially derives from the fact that resources are not infinite . 
on the other hand , it is known that 10% of patients are responsible for some 70% of healthcare costs [ 9 ]  . given the premise that all are agreed upon the need to allocate healthcare resources to obtain the greatest benefit , the question of who shall be responsible for making this allocation becomes crucial . 
should it be the patients themselves who go without a certain type of service to avoid taking healthcare resources away from others ? should it be physicians who balance treatment among their patients , withholding it from one in favour of another , with the aim of obtaining the greatest benefit for society as a whole ? or should it be a collective decision that establishes a system that binds medical practitioners to using resources only up to a certain level and not beyond ? clearly , the solution should be sought in a balance between the different individual , technical and collective aspects . patients expect that the physician acts in their interest to guarantee the best treatment possible . 
however , they should be aware that physicians are constrained to rationing their services for financial reasons that are beyond their dere un modo di trasferire a questultimo la responsabilit professionale . 
in questo modo , peraltro , la declamata autonomia del paziente finisce per diventare una forma subdola di paternalismo , a protezione del radiologo . lincremento delluso della radiologia determina inevitabilmente una contrazione delle risorse destinate ad altre attivit sanitarie . 
in questo modo , lautonomia di alcuni pazienti finisce per limitare quella di altri e violare anche il principio di equit . il consumismo non riguarda solo la radiologia , ma tutta la medicina . 
principi etici mal applicati sono responsabili di altre , anche pi gravi , distorsioni della spesa sanitaria . un esempio quello fornito da evans e hungin [ 6 ] , riguardo la sindrome del colon irritabile , patologia comune quanto priva di trattamenti di provata efficacia . 
la diagnosi di colite spastica , che riguarda un terzo delle patologie gastroenterologiche [ 7 ] vincola il medico a prescrivere un farmaco antispastico che non si rivelato pi efficace del placebo , e che pu presentare effetti collaterali . 
la mancata prescrizione , oltre ad essere inaccettabile per il paziente , potrebbe esporre il medico a conseguenze legali . come risolvere i problemi etici ? evidente che il problema di concedere laccesso a tecnologie diagnostiche o trattamenti di efficacia non documentata o di incerto beneficio deriva essenzialmente dal fatto che le risorse non sono infinite . 
 posto che tutti sono daccordo sulla necessit di allocare le risorse sanitarie in modo da ottenere il maggior beneficio , la questione di chi debba essere responsabile di questa allocazione diventa centrale . 
deve essere il paziente stesso a rinunciare a qualche tipo di servizi , per non sottrarre ad altri risorse sanitarie ? deve essere il medico a bilanciare i trattamenti tra i propri pazienti , negandoli ad uno a favore di un altro , nellottica di ricavare il maggiore beneficio per la popolazione ? o deve essere la collettivit a stabilire un sistema che vincoli i medici ad usare le risorse solo fino a un certo livello e non oltre ? la soluzione , evidentemente , va ricercata in un equilibrio delle diverse istanze individuali , tecniche e collettive . i pazienti si attendono che il medico agisca nel loro interesse , per assicurare loro le migliori cure possibili . 
the shortage of beds or the long waiting lists for performing a mr may induce the physician to putting off the referral or even cancelling it totally , thus playing an active role in the implicit limitation of resources . 
unfortunately , this does not always occur solely on the basis of clinical needs , in that more demanding patients end up obtaining the referral to the detriment of those with the same clinical needs but who are less insistent . 
these patients , in fact , limit their own access to medical treatment , due to time constraints or fear of disease , with possible clinically manifest consequences . taxpayers ( who coincide with the patients , before they show signs of the disease ) have a very different attitude to patients . 
overall , as a society , they demand that physicians make optimal use of healthcare resources , without waste or incongruities , and obtain the maximum possible improvement in the health of the population . 
certain highly advantageous procedures , such as screening for colon cancer and influenza vaccines , have limited success , whereas certain radiological examinations are overutilized in terms of real clinical needs . in addition to the healthcare ramifications of their decisions , physicians are also called on to consider the economic and psychological costs for patients . 
unfortunately , they are not always able to act in the exclusive interest of the patient . long waiting lists and reduced accessibility to those healthcare resources can induce them to modify their decisions to favour healthcare services that are more available than useful . 
in addition , they can find themselves in an ambiguous role , because society requires that they ration healthcare resources among their patients in order to provide the greatest collective benefit possible , even to the detriment of the individual case . 
there is the expectation that they propose treatment plans to the individual patient that may not be the most useful , for the purposes of making savings . clearly , this condition compromises the trust in the doctorpatient relationship . the need to distribute healthcare resources to all , and therefore the need to ration them , has no evident ethical solutions [ 10 ]  . 
by way of extreme simplification , these are the system of judaeo - christian values and the scientific relativist system that goes by the name of social darwinism . possono indurre il medico a rinviare la prescrizione o a volte di cancellarla del tutto , in questo espletando un ruolo attivo di limitazione implicita delle risorse . 
sfortunatamente , ci non sempre avviene solo sulla base delle esigenze cliniche , in quanto i pazienti pi esigenti finiscono per ottenere comunque la prescrizione , a scapito di coloro che , a parit di necessit clinica , pongono richieste meno insistenti . 
taluni pazienti , di fatto , auto - limitano il proprio accesso alle cure mediche , per esigenze di tempo o patofobia , talora con conseguenze clinicamente manifeste . i contribuenti ( che coincidono con gli stessi pazienti , prima che si sia manifestato levento morboso ) hanno un atteggiamento molto diverso da quello dei pazienti . 
essi chiedono in primo luogo di non dover sopportare personalmente i costi dellaumentato ricorso alle cure mediche . nellinsieme , come societ , essi chiedono che i medici facciano un uso ottimale delle risorse sanitarie , senza sprechi e incongruenze , ottenendo il massimo miglioramento della salute della popolazione . 
noto che procedure molto vantaggiose , come lo screening dei tumori del colon e la profilassi vaccinale anti - influenzale , hanno scarso successo , mentre alcuni esami radiologici sono sovra - utilizzati rispetto alle reali necessit cliniche . i medici sono chiamati a considerare , oltre alle conseguenze sanitarie delle loro decisioni , anche i costi economici e psicologici per i pazienti . 
inoltre essi si trovano in un ruolo ambiguo , perch la societ chiede che essi razionino i beni sanitari tra i pazienti , ricavando il maggior beneficio collettivo , anche se a discapito del singolo caso . 
evidentemente , questa condizione compromette il rapporto fiduciario tra paziente e medico . la necessit di distribuire a tutti , e quindi di razionare , le risorse sanitarie , non ha soluzioni eticamente ovvie [ 10 ]  . il dissidio etico pu essere risolto in modi diametralmente opposti , a seconda di quello che il sistema di valori di riferimento . 
in estrema semplificazione , essi sono il sistema di valori giudaico - cristiano e quello scientifico - relativista che va sotto il nome di darwinismo sociale . judaeo - christian tradition the holy bible ( i kings 17 : 12 ) narrates how the prophet nella sacra bibbia ( 1re 17 : 12 ) si narra che il profeta elia , inviato dal signore in un luogo di preghiera , durante una la morale giudaico - cristiana radiol med ( 2009 ) 114 : 11731181 1179 elijah was sent by the lord to a place of prayer during a period of high drought . 
he turned to a widow ( in jewish tradition representative of the most abject poverty and social isolation ) for some food and water , and against all logic , the woman agreed to give him her final reserves , which miraculously were not used up . this episode in the old testament has a corresponding one in the gospels with the story of the multiplication of the loaves ( matthew 14 : 1321 ) , although it may be more correct to speak of the distribution of the loaves . in contrast to what the term multiplication may lead one to believe , the episode in the new testament , like that in the old testament , bears no suggestion of the magical creation of the food . 
on the contrary , magic , even if beneficial as for example the transformation of stones into bread is proffered by satan as a temptation and explicitly rejected by jesus ( luke 4 : 34 )  . 
the apparently impromptu distribution of goods that are essential for survival is unexpectedly followed not by them being used up , but by the miraculous discovery of unexpected resources : the flour and oil were not used up for the entire famine , the loaves and the fishes were distributed among all and a large quantity remained , probably because by following jesus teachings they had brought food with them and spontaneously accepted to share it . 
in line with these teachings , the judaeochristian tradition calls for giving each person all that they need without reservations . social darwinism the judaeo - christian tradition is decisively countered in our society by a set of moral principles that goes by the name of social darwinissocial darwinism is a naturalistic form of ethics based on the theory of evolution proposed by charles darwin ( 18091882 ) , which aims at replacing former dominant ethical principles , or those transcendent principles of the judaeo - christian tradition or the philosophical principles of kantian teachings . 
the principles of natural selection proposed by darwin in his origins of species were applied to human beings under the influence of the principles of malthusianism , which point to the need to combat excessive population , and the thinking of spencer , who rejected the idea of treating the sick on the basis of the principle of survival of the fittest . 
this led to the work by ernst haeckel , who rejected the sanctity of human life and invoked infanticide , abortion and the elimination of the mentally ill while exalting the model of ancient sparta . the step towards mein kampf by hitler is intuitive and immediate . 
less well known , perhaps , is the fact that tremenda siccit , si rivolgesse ad una vedova ( cio alla figura che rappresentava nel mondo ebraico la pi estrema miseria ed isolamento sociale ) per avere da lei cibo e acqua , e che avendo la donna , contro ogni logica , accettato di dare fondo alle ultime sue riserve , queste miracolosamente non si esaurirono . lepisodio biblico ha una corrispondenza con quello riportato nei vangeli con il nome di moltiplicazione dei pani ( matteo 14 : 1321 ) , ma che sarebbe forse pi corretto indicare come distribuzione dei pani . 
 contrariamente a quello che il termine moltiplicazione potrebbe far intendere , nellepisodio del nuovo testamento , cos come in quello della bibbia , non c alcun cenno alla creazione magica di un alimento . 
al contrario , la magia anche benefica , ad esempio la trasformazione delle pietre in pane , proposta dal maligno come tentazione , ed esplicitamente respinta da ges ( luca 4 : 34 )  . 
la distribuzione , apparentemente improvvida , di beni indispensabili per la sopravvivenza seguita inaspettatamente non dal loro esaurimento , ma dal reperimento , questo s miracoloso , di risorse impreviste : la farina e lolio non si esauriscono per tutta la carestia , i pani e i pesci vengono distribuiti tra tutti e ne avanza una gran quantit : probabilmente perch quanti , seguendo la predicazione di ges , avevano portato con s risorse alimentari , accettano spontaneamente di condividerle . 
in linea con questi insegnamenti , la morale giudaico - cristiana impone di dare a ciascuno , senza riserve , tutto ci di cui ha bisogno . il darwinismo sociale alla morale giudaico - cristiana si contrappone decisamente nella nostra societ una morale che si pu indicare con il nome di darwinismo sociale . 
il darwinismo sociale una forma naturalistica di etica basata sulla teoria dellevoluzione di charles darwin ( 18091882 ) , che mira a sostituire i principi etici prima dominanti , quelli trascendenti della cultura giudaico - cristiana o quelli filosofici della deontologia kantiana . 
lapplicazione agli esseri umani dei principi di selezione naturale proposti da darwin nella sua opera fondamentale lorigine della specie , sotto linfluenza dei principi del malthusianesimo , secondo i quali occorre combattere leccesso della popolazione , e del pensiero di spencer , che rigettava lidea di occuparsi dei malati in ragione del principio di sopravvivenza del migliore , ha prodotto lopera di ernst haeckel , che rigetta la santit della vita umana e invoca linfanticidio , laborto e leliminazione dei malati di mente , esaltando il modello della civilt spartana . 
il passaggio al mein kampf di hitler 1180 radiol med ( 2009 ) 114 : 11731181 concepts in line with these ideologies have been expressed by modern scientists such as watson , who was awarded the nobel prize in 1962 for the discovery of the dna double helix and who felt that abortion was justified in the event it was demonstrated that the fetus was genetically predisposed towards homosexuality ; or contemporary bioethicists such as peter singer , who justify euthanasia if the quality of life is not satisfactory . reflecting upon the links between darwinism and nazism , the irish bioethicist omathuna noted in a recent work that the vitality of the principles of social darwinism more than 60 years after the fall of the nazi dominion bears witness to the persistence of some principles that significantly undermine the concept of human dignity [ 11 ]  . the first of these principles is that ethics have a relative and not absolute value . 
if ethics are modified with changing environmental conditions , then even the evaluation of human dignity is relative . the second principle is evolutionis if humans have gradually evolved from animals , then there is no reason for treating humans differently from animals . 
this does not necessarily translate into an increased level of attention for animals , but rather into attributing to humans a value lower than that of animals . the third principle refers to the observation that inequality exists in nature and leads to different degrees of ability to adapt . 
meno noto , forse , il fatto che concetti in linea con tali ideologie siano stati espressi da scienziati moderni come watson , lo scopritore della struttura ad elica del dna , premio nobel 1962 , che riteneva giustificato laborto nel caso si fosse dimostrato che il nascituro fosse geneticamente predisposto allomosessualit ; o da bioeticisti contemporanei come peter singer , che giustifica leutanasia se la qualit della vita non soddisfacente . in un recente lavoro , omathuna , bioeticista irlandese , riflettendo sui legami tra darwinismo e nazismo , osserva come la vitalit dei principi del darwinismo sociale , a pi di sessantanni dalla caduta del dominio nazista , sia testimoniata dalla persistenza di alcuni principi che mettono in crisi il concetto di dignit umana [ 11 ]  . il primo di tali principi che letica ha un valore relativo , non assoluto . 
ci non si traduce necessariamente in un aumento del livello di attenzione verso gli animali , ma pu al contrario consistere nellattribuzione ad esseri umani di un valore inferiore a quello degli animali . il terzo principio si riferisce allosservazione che lineguaglianza esiste in natura e conduce a diversi gradi di capacit di adattamento . 
per analogia , la razza e le abilit mentali sono considerate determinanti la dignit umana . from this follows the fourth principle , which states that some existences have such limited value as to be considered unworthy of being lived . dai precedenti , consegue il quarto principio , che alcune esistenze hanno cos scarso valore , da essere ritenute indegne di essere vissute . last is the fifth principle , whereby natural selection is based on survival of the fittest . 
as a consequence , helping disadvantaged humans corresponds to opposing the laws of nature and can compromise the well - being and , in the end analysis , the survival of the human species . it is no hard task to realise which of these principles has survived the fall of nazism in modern capitalist society . 
the growing economic pressure on healthcare systems throughout the world and the economic and social inequalities between countries could , as occurred in germany prior to the rise in nazism , lead to a recovery of the principles of relativism and social darwinis any decision regarding the criteria of healthcare management in particular and society in general must take into account the reference system of values , whether they be judaeo - christian or darwinian . 
di conseguenza , aiutare gli esseri umani svantaggiati corrisponde ad opporsi alle leggi della natura e pu compromettere il benessere e in ultima analisi la sopravvivenza della specie umana . non difficile rilevare quanto di questi principi sia sopravvissuto alla caduta del nazismo nelle moderne societ capitalistiche . 
le pressioni economiche crescenti esercitate sui sistemi sanitari di tutto il mondo e le ineguaglianze economiche e sociali tra diversi paesi , potrebbero , come gi accadde in germania prima dellavvento del nazismo , agire per una ripresa dei principi del relativismo e del darwinismo sociale . 
qualunque decisione sui criteri di gestione della sanit , e della societ pi in generale , non pu prescindere dal confronto con i sistemi di valori di riferimento , siano essi giudaico - cristiani o darwinisti . 
in particular , the physician should evaluate and correctly and comprehensibly explain the possible risks of radiation exposure . in general , the radiologist who aspires to judaeo - christian values should seek to protect the patient from their own choices if these are not sufficiently valid . 
by performing the requested examinations without regard to their appropriateness , the radiologist will obtain evident and immediate advantages by increasing his or her own personal case series and professional experience , avoiding an undermining of relations with patients , and increasing their own fame and earnings . in this case , as in other situations , the choice based on ethical or religious principles is neither painless nor without consequences . ciascun radiologo potr compiere dipende direttamente dalladesione ad un preciso sistema di valori . 
per evitare di incorrere nel paternalismo , il medico dovr informare i pazienti in modo completo ed esaustivo non solo sulle procedure possibili , ma anche sulle controindicazioni e rischi di ciascuna procedura . 
in particolare , egli tenuto a valutare ed esporre correttamente e in modo comprensibile al paziente il rischio stocastico da radiazioni . in generale , il radiologo che si ispira ai principi giudaico - cristiani dovr cercare di proteggere i pazienti dalle loro stesse scelte , se non sufficientemente valide . 
eseguendo gli esami richiesti senza preoccuparsi della loro appropriatezza il radiologo otterr evidenti e immediati vantaggi : potr aumentare la propria casistica ed esperienza professionale , eviter di mettere in crisi il rapporto con i pazienti , accrescer la propria fama e i propri guadagni . 
cademartiri1 , 2 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands correspondence to : f . 
cademartiri , dipartimento di radiologia e diagnostica per immagine , c / o piastra tecnica piano 0 , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 0521 - 703756 , fax : + 39 - 0521 - 704838 , e - mail : filippocademartiri@hotmail.com received : 13 november 2008 / accepted : 7 january 2009 / published online : 7 august 2009 springer - verlag 2009 abstract purpose . 
weighted ct dose index ( ctdi ) was measured by using an anthropomorphic phantom in spiral cardiac mode ( retrospective ecg gating ) at five pitch values adapted with two heart - rate - adaptive ecg pulsing windows using four algorithms : narrow pulsing window , with tube current reduction to 20% ( a ) and 4% ( b ) of peak current outside the pulsing window ; wide pulsing window , with tube current reduction to 20% ( c ) and 4% ( d )  . 
this feature is a potential limitation to its clinical use . as a result , algorithms have been developed that are able to modulate the radiation exposure without significantly deteriorating image quality at mdct coronary angiography ( mdct - ca ) [ 710 ]  . recently , it has been introduced dual - source ct ( dsct ) equipped with two x - ray tubes and two detectors mounted on the rotating gantry with an angular offset of 90 . 
single - source mdct [ 1013 ]  . in single - source scanners , the modulation modality allows a progressive reduction in radiation dose with a reduction in hr ( fixed - pitch protocol ) [ 1416 ]  . 
the scanners also have other special attributes : the collimation system is equipped with an additional bow - tie filter to limit the field of view ( fov ) to the cardiac region ; the dose can be adapted to the patients build [ combined applications to reduce exposure ( care ) dose 4d ] ; and as with single - source systems , an echocardiography ( ecg ) pulsing system can be used to vary the width of the application window by 100% of ma , as well la tomografia computerizzata multistrato ( tcms ) diventata un importante strumento diagnostico non invasivo per la patologia coronarica ( cad ) e cardiaca . 
tuttavia , lo sviluppo di apparecchiature sempre pi performanti ( per esempio tcms a 64 strati ) , comporta di regola un incremento della dose di esposizione alle radiazioni ionizzanti [ 46 ]  . 
questo fattore rappresenta una potenziale limitazione allimpiego clinico . sono stati pertanto sviluppati degli algoritmi capaci di modulare lesposizione alle radiazioni senza deteriorare significativamente la qualit dellimmagine mediante angiografia coronarica tcms ( ac - tcms ) [ 710 ]  . di recente stata introdotta sul mercato lapparecchiatura tcms a doppia sorgente ( dsct ) dotata di due tubi radiogeni e due detettori montati sulla pista di rotazione del gantry ad una compensazione angolare di 90 . 
questa configurazione determina una maggiore risoluzione temporale ( 83 ms ) e quindi una conseguente maggiore flessibilit di utilizzo a frequenza cardiaca elevata ( > 65 bpm ) rispetto alla tcms a singola sorgente [ 1013 ]  . nelle apparecchiature a singola sorgente la modalit di modulazione consentiva una progressiva riduzione della dose di radiazioni con la riduzione della frequenza cardiaca ( protocollo a pitch fisso ) [ 1416 ]  . 
inoltre , il sistema di collimazione equipaggiato con un addizionale cardiac bow - tie filter per limitare il field of view ( fov ) alla regione cardiaca ; la dose pu essere adattata al paziente in base alla radiol med ( 2009 ) 114 : 10371052 1039 as a system of ecg - controlled tube current modulation [ 13 ]  . 
with the combination of these techniques , dedicated dose - reduction algorithms can be applied according to the situation and the quantity of information that needs to be extrapolated from the examination . the aim of this study was to compare the difference of total radiation dose between two different pulsing windows and two different tube current modulation modalities at different hrs . materials and methods for this study , performed on a phantom , we used a firstgeneration dsct system ( siemens medical solutions , forchheim , germany )  . 
with a gantry rotation time of 330 ms and peak power of 80 kw / tube ( straton , siemens medical solution ) , a constant temporal resolution was obtained equal to a quarter of a gantry rotation ( 83 ms ) at the centre of the scan fov . 
this is one of the key differences with the conventional mdct systems , which can theoretically provide the same temporal resolution with multisegment reconstruction algorithms and a rhythmical and regular hr . the conventional indices of ct dose are also applicable to dsct because the doses regarding a single tube or both tubes simultaneously are the same value of combined doses . in dsct , the tube current value is calculated as the current time product per gantry rotation ( mas / rot ) with the sum of the mas of both x - ray tubes [ 13 , 1719 ]  . dose - reduction methods in cardiac dsct adaptive pitch - heart rate the pitch can be increased proportionally with increasing hr . 
the slowest heart beat during prescan monitoring is used for calculating the pitch . cardiac bow - tie filter conformazione corporea ( combined applications to reduce exposure [ care ] dose 4d ) ; pu essere utilizzato ( come per i sistemi a singola sorgente ) un sistema di modulazione cardio - sincronizzata dellemissione del tubo radiogeno ( electrocardiographic [ ecg ] - pulsing ) per variare larghezza della finestra di applicazione del 100% di amperaggio e un sistema di riduzione cardio - sincronizzata della corrente del tubo al di fuori della finestra di acquisizione ( ecg - controlled tube current modulation ) [ 13 ]  . 
 lo scopo di questo studio di confrontare la differenza di dose totale di radiazione tra due diverse finestre di pulsing e due diverse modalit di modulazione della corrente del tubo , a diversi valori di frequenza cardiaca . 
 materiali e metodi per questo studio su fantoccio stato utilizzato il sistema dual - source tc ( siemens medical solutions , forchheim , germania ) di prima generazione . principi di tcms a doppia sorgente il sistema dsct valutato dotato di due tubi radiogeni e due detettori montati ad una compensazione angolare di 90 . con un tempo di rotazione del gantry di 330 ms ed una potenza di picco di 80 kw / tubo ( straton , siemens medical solution ) , si ottenuta una costante risoluzione temporale pari ad un quarto del tempo di rotazione del gantry ( 83 ms ) , al centro del fov di scansione . 
per un imaging cardiaco dsct , sono necessari esclusivamente i dati provenienti da un solo ciclo cardiaco , quindi la risoluzione temporale indipendente dalla frequenza cardiaca ( fc ) del paziente e la modalit base di un sistema dsct corrisponde alla ricostruzione a singolo segmento . 
questa una delle maggiori differenze con i sistemi tcms convenzionali , che teoricamente possono fornire la stessa risoluzione temporale con algoritmi di ricostruzione multi - segmentari e con un battito cardiaco ritmico e regolare . 
i convenzionali indici di dose nella tomografia computerizzata ( tc ) sono applicabili anche in dsct , poich le dosi relative ad un singolo tubo o su entrambi i tubi radiogeni simultaneamente risultano nello stesso valore di dose combinate . 
in dsct , il valore della corrente del tubo viene calcolato come il prodotto della corrente al secondo per il tempo di rotazione del gantry ( mas / rot ) sommando i mas di entrambi i tubi [ 13 , 1719 ]  . 
 metodi di riduzione della dose in dsct cardiaco pitch heart rate - adattativo as the region of interest ( roi ) is the heart , the collimation il pitch pu aumentare parallelamente allaumento della frequenza cardiaca . 
questo adattamento porta ad una 1040 radiol med ( 2009 ) 114 : 10371052 system of the dsct is equipped with two bow - tie filters . the first is defined cardiac and is used to limit the fov to the cardiac region , whereas the second is the body filter , which is also present in 64 - slice mdct . riduzione dellesposizione alle radiazioni corrispondente ad una dose media direttamente proporzionale a 1 / pitch . 
il pi basso ritmo cardiaco rilevato durante il monitoraggio prescansione determina il valore del pitch . care dose 4d filtro bow - tie cardiaco this is an automatic exposure control system ( care dose 4d , siemens medical solution , forchheim , germany ) , which can combine automatic modulation of the tube current along the acquisition volume in relation to the angular attenuation coefficient of the examined region and to attenuation values of different tissues on the basis of data acquired from a single localiser radiograph ( on - line modulation ) [ 15 ]  . ecg - controlled tube current modulation tube current modulation during the entire cardiac cycle was introduced in cardiac ct to help reduce exposure by ~50% [ 1416 ]  . 
prior to the scan , the operator can manually select the width of the image acquisition window ( pulsing window = window of max ma , or 100% of ma ) in the r - r interval corresponding to the phase of greatest immobility of the heart and coronary arteries . 
thanks to a system of ecg - controlled tube current modulation , the radiation delivered can be reduced outside the pulsing window to 20% ( functional imaging ) or 4% ( mindose ) of the peak tube current , thus markedly reducing radiation exposure . 
modulation to 4% is applied to minimise the total time of radiation exposure [ 13 , 17 , 20 ]  . in mdct equipment , ecg - controlled tube current modulation requires a rhythmical and regular heart beat . when a patients heart beat is not regular , the optimal reconstruction interval of the raw data may occur during the window of reduced tube current , thus requiring an interpolation of the data of two adjacent heart beats . 
in dsct equipment , the algorithm that analyses the heart beat is able to recognise an r - r interval significantly different from the expected r - r interval and automatically widen the pulsing window ( ecg editing )  . 
this adaptation tends to increase the dose delivered to the patient but at the same time automatically optimises the acquisition data set , thus overcoming one of the main limitations of previous mdct equipment [ 10 , 11 , 13 ]  . three - dimensional adaptive noise reduction algorithm a further system of dose optimisation in dsct systems is the 3d reconstruction algorithm , which employs special adaptive convolution kernels ( b26 ) that are able to reduce poich la regione dinteresse quella cardiaca , il sistema di collimazione della dsct dotato di due bow - tie filters . 
il primo definito cardiac , per limitare il fov alla regione cardiaca ; il secondo il filtro body , presente anche in tc a 64 strati . care dose 4d il care dose 4d un sistema di limitazione automatico della dose ( siemens medical solution ) in grado di combinare la modulazione automatica della corrente del tubo radiogeno lungo il volume di acquisizione in relazione al coefficiente di attenuazione angolare della regione in esame e ai valori di attenuazione dei diversi tessuti , sulla base dei dati rilevati dallo strato precedente durante il topogramma ( on - line modulation ) [ 15 ]  . modulazione cardio - sincronizzata della corrente del tubo la modulazione dellemissione del tubo radiogeno durante lintera durata del ciclo cardiaco stata introdotta in cardio - tc , come aiuto per ridurre la dose di ~50% [ 1416 ]  . prima della scansione , loperatore pu selezionare manualmente la larghezza della finestra di acquisizione delle immagini ( finestra di pulsazione , o pulsing window vale a dire la finestra di massimo amperaggio [ max ma o 100% di ma ] ) nellintervallo r - r in corrispondenza della fase di maggior immobilit del cuore e delle arterie coronariche . 
grazie ad un sistema di modulazione cardio - sincronizzato della corrente del tubo , o ecg - controlled tube current modulation , lerogazione raggi pu essere ridotta al di fuori della finestra di pulsing al 20% ( functional imaging ) o al 4% ( mindose ) del valore nominale della corrente del tubo , per ridurre fortemente lesposizione alle radiazioni . 
la qualit delle immagini acquisite al 20% di ma permette lo studio cinetico - morfologico del ventricolo sinistro ; la modulazione al 4% viene applicata per ridurre al minimo i tempi totali di esposizione raggi [ 13 , 17 , 20 ]  . 
quando il ritmo cardiaco del paziente non regolare , lintervallo di ricostruzione ottimale dei dati grezzi potrebbe verificarsi durante la finestra di riduzione della corrente del tubo richiedendo un interpolazione dei dati dei due battiti cardiaci adiacenti . 
nellapparecchiatura dsct , lalgoritmo di analisi dellandamento del ritmo cardiaco permette di riconoscere un intervallo r - r significativamente differente da quello previsto e allargare automaticamente la finestra di pulsing ( ecg - editing )  . 
the common scan parameters were the following : two x - ray sources , 380 mas / rot with 120 kv , detector collimation 320.6 mm , slice collimation 640.6 mm ( zaxis flying focal spot ) ; gantry rotation time 330 ms . 
the pitch varied between 0.2 ( 45 bpm ) and 0.5 ( 120 bpm ) at low and high hrs , being automatically adapted by the device to the hr utilised : 45 , 60 , 75 , 90 and 120 bpthe craniocaudal range of the scan was 90 m images were reconstructed in single - segment modality with 0.75 - mm slice thickness , reconstruction increment 0.7 mm and mediumsmooth convolution kernel ( b31f )  . 
for each hr value , four series of reconstructions were done from 0% to 95% of the r - r interval with 5% steps for a total of 20 data sets . in dsct - ca a narrow pulsing window can be used in patients with low ( 65 bpm ) and hig ( 80 bpm ) hr without significant deterioration in image quality . 
however , in most patients with an intermediate hr ( 7075 bpm ) , a wider data acquisition window is required to obtain the best - quality data sets [ 2123 ]  . 
1 fantoccio tc cardiaco antropomorfico . mento determina un aumento della dose di esposizione del paziente , ma allo stesso tempo unottimizzazione automatica del data set di acquisizione , superando uno dei principali limiti delle apparecchiature tcms precedenti [ 10 , 11 , 13 ]  . algoritmo 3d adattativo di riduzione dal rumore come ulteriore sistema di ottimizzazione della dose , nel sistema dsct stato implementato un algoritmo di convoluzione adattativo di ricostruzione 3d ( kernel b26 ) , in grado di ridurre il rumore dellimmagine a parit di dose . 
il kernel b25 di un sistema 64 tc usa un algoritmo simile , ma implementato solo in 2 dimensioni : allinterno del piano dellimmagine ( x , y ) , ma non lungo lasse z . 
i parametri di scansione comuni sono : due sorgenti a raggi x ; 380 mas / rot ad una tensione di 120 kv , collimazione del detettore 320 , 6 mm , collimazione della slice 640 , 6 mm ( z - axis flying focal spot ) ; tempo di rotazione del gantry 330 ms . 
il pitch variava tra 0 , 2 ( 45 bpm ) e 0 , 5 ( 120 bpm ) , a basse ed elevate frequenze cardiache , adattato automaticamente dalla macchina alle frequenze cardiache utilizzate : 45 , 60 , 75 , 90 e 120 bpil range cranio - caudale di scansione era 90 mle immagini sono state ricostruite in modalit a singolo - segmento con spessore della slice 0 , 75 mm ; incremento 0 , 7 mm ; kernel di convoluzione medium - smooth ( b31f )  . 
per ogni valore di frequenza cardiaca sono state ricostruite 4 serie di ricostruzioni , dallo 0% al 95% dellintervallo r - r con passo del 5% , per un totale di 20 data set . in dsct - ca , nei pazienti con bassa ( 65 bpm ) ed alta frequenza cardiaca ( 80 bpm ) pu essere utilizzata una finestra di pulsazione stretta , senza significativo deterioramento della qualit dellimmagine . 
invece , nella maggioranza dei pazienti con frequenza cardiaca intermedia ( 7075 bpm ) necessaria una finestra di acquisizione dati ampia per ottenere la miglior qualit del data set [ 2123 ]  . lottimale finestra di pulsing a basse , intermedie , alte frequenze cardiache 65%76% ( fase telediastolica ) , 30%77% ( telediastole + telesistole ) , 31%47% ( fase telesistolica )  . 
 in questo studio stata valutata la dose di radiazione relativa allutilizzo degli algoritmi dsct di risparmio della dose , alla valutazione morfo - funzionale del ventricolo sinistro e alla frequenza cardiaca . 
the use of the optimal window produces a 64% reduction in exposure at both low and high hr [ 2123 ]  . our study evaluated radiation exposure in terms of hr , the morphofunctional evaluation of the left ventricle , and the use of the dsct algorithms for dose reduction . 
the constant hr produced by the ecg simulator did not allow evaluation of the ecg editing system . dose exposure evaluation we calculated the ct dose index volume [ ctdivol ( mgy ) , where ( j ) ( kg - 1 ) = ( gy ) ] and the dose - length product [ dlp ( mgy cm ) ] as parameters of absorbed dose ( table 2 )  . ctdivol considers the scan parameters ( kv , mas / rot , scan time ) and describes the mean dose relative to the scan volume , the type of equipment and the pitch . 
for the scan length used in our study ( 90 mm ) , the mean number of cardiac cycles required for to reconstruct the total scan volume varied between seven and six beats . 
il ctdivol mette in relazione i parametri di scansione ( kv , mas / rot , tempo di scansione ) e descrive la dose media relativa al volume di scansione , al tipo di apparecchiatura e al pitch . 
per la lunghezza di scansione utilizzata in questo studio ( 90 mm ) , il numero medio di cicli cardiaci necessari alla ricostruzione del volume totale di scansione variava tra 78 battiti . in unapparecchiatura dsct , lutilizzo dellalgoritmo di modulazione cardio - sincronizzato della corrente del tubo comporta una dose di radiazione proporzionale al valore medio della corrente applicata durante la scansione [ 13 ] : [ ( tminmamin ) + ( tmaxmamax ) ] / ( tmin + tmax ) dove tmin e tmax sono i tempi alla minima ( mamin ) e alla massima corrente del tubo ( mamax ) , rispettivamente , allinterno di un ciclo cardiaco . 
 [ ( tminmamin ) + ( tmaxmamax ) ] / ( tmin + tmax ) statistica where tmin and tmax are the times at the minimum ( mamin ) and maximum tube current ( mamax ) , respectively , within a cardiac cycle . 
in addition , we calculated the effective dose by using the conversion coefficient for the chest ( dpl0.017 ) ( table 2 )  . tutti i dati sono presentati come mediadeviazione standard ( ds )  . 
il confronto tra i valori di dlp e dlp effettivo stato effettuato mediante test t di student per dati appaiati e una p < 0 , 05 stata considerata significativa . 
the correlations were evaluated with the pearson r coefficient . risultati statistics results the scan time was ~810 s at low hr ( 60 bpm ) , 6 s at intermediate hr ( 75 bpm ) and ~45 s at high hr ( 90 bpm )  . 
con una finestra di acquisizione stretta , la modulazione della corrente al 4% di ma riduce la dose del 35 , 15% ( 2 , 51 msv ; p < 0 , 005 )  . 
pitch ( table feedgantry rotation time ) / slice collimation ; fc , heart rate , bpm beats per minute . pitch / fc ( 2 ) = pitch / hr ( 2 ) fig . 
il valore del pitch aumenta parallelamente allaumentare della frequenza cardiaca , sulla base del pi basso battito rilevato durante il monitoraggio pre - scansione . pitch = ( table feedtempo di rotazione ) / collimazione slice ; fc , frequenza cardiaca ; bpm , battiti per minuto . pitch / fc ( 2 ) = pitch / hr ( 2 ) dose exposure evaluation table 2 shows estimates of the ctdivol and dlp dose indices . 
the dose delivered beyond the scan range corresponds to the difference between dlp and effective dlp ( dlpe ) calculated for the scan length used in this study ( mgy 90 mm )  . 
la dose erogata oltre il range di scansione corrisponde alla differenza tra il dlp ed il dlp effettivo ( dlpe ) , calcolato per la lunghezza di scansione utilizzata in questo studio ( mgy90 mm )  . 
il dlpe risultato 5 , 651 , 48 msv , 3 , 660 , 86 msv , 7 , 62 , 48 msv , 5 , 91 , 87 msv , nel protocollo a , b , c e d , rispettivamente ( tabella 2 )  . il decreto legge 230 / 95 relativo alle norme radio - protezionistiche emanate dallinternational commission on radiological protection ( icrp ) , sancisce che il personale classificato non esposto alle radiazioni ionizzanti ( per esempio i pazienti ) suscettibile ad unesposizione globale annua < 1 msv . 
in patients with low , intermediate and high heart rates , the use of a narrow pulsing window produces a significant reduction in dose , with image quality remaining unchanged . 
nei pazienti con bassa , intermedia ed alta frequenza cardiaca , lutilizzo di una finestra di pulsazione stretta determina una significativa riduzione di dose , a parit di qualit di immagine . 
therefore , all the available dose reduction algorithms should be implemented . discussione lesposizione alle radiazioni ionizzanti rappresenta uno dei limiti allimpiego clinico delle apparecchiature tc multistrato nellimaging cardiaco non invasivo [ 13 ]  . 
come noto , in modalit spirale i dati sono continuamente raccolti attraverso il ciclo cardiaco per essere successivamente ricostruiti in una fase del ciclo cardiaco definita arbitrariamente [ 710 , 24 ]  . 
the graphs show the difference between the radiation dose delivered during the scan ( dlp ; a ) and the dose calculated for effective scan length of 90 mm ( dlpe ; b )  . 
i grafici mostrano la differenza tra la dose di esposizione erogata durante la scansione ( dlp ; a ) e la dose relativa leffettiva lunghezza di scansione di 90 mm ( dlpe ; b )  . 
therefore , on the basis of the data obtained , the choice of the optimal ecg pulsing window seems to be indispensable for achieving a significant reduction in exposure at low hr [ 710 , 22 , 23 ]  . dependence on minimum pulsing value on the basis of the scan parameters used , ( 120 kv , 380 mas / rot , slice thickness 0.75 , pitch - hr adaptive protocol ) , the dose delivered with 20% modulation to the maximum ma with narrow and wide pulsing window ( r = 0.99 ; p < 0.005 ) can be significantly reduced with modulation to 4% . 
 the results obtained suggest that : the use of the pitchhr adaptive protocol produces a reduction in dose proportional to the increase in hr in dsct - ca examinations with retrospective ecg gating , the use of dose - reduction algorithms , ecg pulsazione , narrow e wide pulsing window , modulate al 20% e al 4% del valore nominale della corrente del tubo . dipendenza dalla frequenza cardiaca nelle acquisizioni pulsate , ladattamento del valore di pitch alla frequenza cardiaca risulta in una significativa riduzione del ctdivol allaumentare della frequenza cardiaca ( 45120 bpm )  . 
determina una significativa riduzione di dose con e senza valutazione dei volumi del ventricolo sinistro ( r = 0 , 97 ; p < 0 , 05 ) , se confrontato con il protocollo wide pulsing window . 
quindi in base ai dati ottenuti , lottimale finestra ecg - pulsing sembra essere indispensabile per una significativa riduzione della dose a bassa ed elevata frequenza cardiaca [ 710 , 22 , 23 ]  . 
 dipendenza dal valore minimo di pulsazione sulla base dei parametri di scansione utilizzati ( 120 kv , 380 mas / rot , slice thickness 0 , 75 , pitch heart rate - adattativo ) , la dose erogata con modulazione al 20% di max ma mediante narrow e wide pulsing window ( r = 0 , 99 ; p < 0 , 005 ) pu essere significativamente ridotta con modulazione al 4% . 
 dai risultati ottenuti possibile dedurre che : lutilizzo del pitch heart rate - adattativo permette una riduzione di dose proporzionale allaumento della frequenza cardiaca ; nelle indagini dsct - ca eseguite mediante ecg - gated retrospettivo , lutilizzo degli algoritmi di risparmio della dose , ecg - pulsing e ecg - controlled tube current modulation , risultano in una riduzione di dose a tutte le frequenze cardiache , con i migliori risultati a basse ed alte frequenze cardiache ; la modulazione della corrente del tubo al 4% del valore nominale di ma al di fuori della finestra di 1050 radiol med ( 2009 ) 114 : 10371052 pulsing and ecg - controlled tube current modulation produces a reduction in dose at all hrs , with the best results at low and high hr tube current modulation to 4% of the peak tube current outside the pulsing window is recommended in cases where a cardiac motion - morphological evaluation of the left ventricle is not required , with a dose reduction proportional to the increase in hr . with respect to data in the literature that report exposure values for dsct systems of 12 / 9 msv ( hr 65 bpm ) , 15 / 12 msv ( hr 6679 bpm ) and 7 / 4 msv ( hr 80 bpm ) with the use of optimal pulsing window and modulation to 20% / 4% [ 22 , 23 ] , application of ecg pulsing and ecgcontrolled tube current modulation allowed us to achieve overall lower exposure values at all hrs [ 28 ]  . a recent study comparing prospective ecg triggering and retrospective ecg gating in dsct - ca [ 29 ] reported significantly lower values of effective dose with the use of prospective scan algorithms . 
dsct systems have not yet been equipped with a similar mobile system . limitations the optimisation of scan protocols in cardiac ct is based solely on the calculation of the dose of ionising radiation delivered derived from measurement on a phantom and on the basis of the algorithms developed for this study . 
in addition , not all dose - reduction algorithms available with this technique were evaluated , such as reduction and / or increase in tube voltage , the use of double voltage , the b26 convolution kernel , the care dose 4d system and ecg editing . 
however , the considerations formulated appear reasonable and take into account the technical features of dsct systems . recommendations for use results from our study suggest the use of tube current acquisizione - dati raccomandabile nei casi in cui non sia richiesta una valutazione cinetico - morfologica del ventricolo sinistro , per una riduzione di dose proporzionale allaumento della frequenza cardiaca . rispetto ai dati disponibili in letteratura che riportano per apparecchiature dsct valori di dose di 12 / 9 msv ( fc65 bpm ) , 15 / 12 msv ( fc 6679 bpm ) e 7 / 4 msv ( fc80 bpm ) con lutilizzo dellottimale finestra di pulsing e modulazione al 20% / 4% [ 22 , 23 ] , lapplicazione del sistema di modulazione ecg - pulsing ed ecg - controlled tube current modulation ha consentito di ottenere nel nostro studio valori di dose complessivamente inferiori , a tutti i valori di frequenza cardiaca [ 28 ]  . un altro recente studio eseguito mediante confronto ecg - prospettico vs ecg - retrospettivo in dsct - ca [ 29 ] , mostra valori di dose efficace significativamente inferiori mediante lapplicazione di algoritmi di scansione prospettici . 
questi algoritmi sembrano ridurre maggiormente la dose ed appaiono pi efficaci a bassa frequenza cardiaca . tuttavia , il principio su cui si basano non garantisce una perfetta coerenza tra la fase del ciclo cardiaca identificata e la fase effettiva . nel 2008 , sono stati introdotti ulteriori metodi di limitazione della dose su apparecchiature tc multistrato ( definition as + , siemens medical solutions ) che consistono in un nuovo sistema di collimazione mobile che si posiziona davanti alla finestra di uscita dei raggi x prima e dopo leffettiva lunghezza di scansione , formando uno scudo che frena le radiazioni erogate oltre il range di scansione . lapparecchiatura dsct non ancora dotata di un simile sistema mobile . 
 limitazioni lottimizzazione dei protocolli di scansione in tc del cuore si basa solo sul calcolo della dose di esposizione alle radiazioni ionizzanti risultata da misurazioni su fantoccio e in base agli algoritmi elaborati per questo studio . 
inoltre non sono stati valutati tutti gli algoritmi di risparmio della dose disponibili con questa metodica , quali : la riduzione e / o laumento del voltaggio del tubo radiogeno , lutilizzo del doppio voltaggio , il kernel di convoluzione b26 , il sistema care dose 4d ed ecg - editing . 
 raccomandazioni di utilizzo in generale , ad ogni valore di frequenza cardiaca , dovrebbe essere utilizzata una modulazione della corrente al 20% del valore nominale della corrente del tubo per una valutazione radiol med ( 2009 ) 114 : 10371052 1051 modulation to 20% of the peak tube current for a kineticfunctional evaluation of the left ventricle and in all other cases the minimisation of the pulsing value to spare patients unnecessary radiation exposure : low hr ( 65 bpm ) : use a narrow pulsing window corresponding to the end - diastolic phase of the cardiac cycle ( 65%76% of the r - r interval ) intermediate hr ( 65 bpm < hr < 80 bpm ) : use a wide pulsing window that includes end diastole and end systole ( 31%76% of the r - r interval ) high hr ( hr > 80 bpm ) : use a narrow pulsing window corresponding to the end - systolic phase ( 31%47% of the r - r interval )  . cinetico - funzionale del ventricolo sinistro ; in tutti gli altri casi , si dovrebbe prediligere una riduzione al minimo valore di pulsazione per preservare il paziente da uninutile esposizione alle radiazioni ionizzanti : frequenza cardiaca bassa ( fc65 bpm ) : utilizzare una finestra di pulsazione stretta in corrispondenza della fase telediastolica del ciclo cardiaco ( 65%76% dellintervallo r - r ) ; frequenza cardiaca intermedia ( 65 bpm < fc < 80 bpm ) : utilizzare una finestra di pulsing ampia che comprenda telediastole e telesistole ( 31%76% dellintervallo r - r ) ; frequenza cardiaca elevata ( fc > 80 bpm ) : utilizzare una finestra di pulsazione stretta in corrispondenza della fase telesistolica del ciclo cardiaco ( 31%47% dellintervallo r - r )  . conclusions conclusioni the dose - reduction algorithms available on dsct systems enable the effective dose to be kept below 10 msv in most cases , with the exception of low hr ( 12.68 msv at 4560 bpm ) with imaging protocol . 
when the mindose protocol is routinely applied ( foregoing the possibility of performing an evaluation of left ventricular volumes ) , the dose delivered on average is below 8 msv . the wide functional gli algoritmi di riduzione della dose disponibili su apparecchiatura dsct consentono di mantenere la dose efficacie al di sotto dei 10 msv nella maggior parte dei casi , ad eccezione delle basse frequenze cardiache ( 12 , 68 msv a 4560 bpm ) con protocollo wide functional imaging . 
this study evaluated the effectiveness of contrast - enhanced ultrasound ( ceus ) , performed immediately after percutaneous ethanol injection ( pei ) or radiofrequency thermal ablation ( rfta ) , by comparing results with the computed tomography ( ct ) follow - up . 
in the first group , ct identified complete necrosis in 28 / 54 ( 52% ) lesions , 21 ( 75% ) of which had avascular , one ( 4% ) isovascular and six ( 21% ) hypovascular patterns at ceus . 
in the second group , ct showed complete necrosis in 31 / 36 ( 86% ) lesions , all ( 100% ) of which had a corresponding avascular pattern at ceus . 
sensitivity , specificity , positive predictive value , negative predictive value and accuracy of the avascular pattern at ceus compared with ct findings were 75% , 69% , 72% , 72% and 72% for pei and 100% , 20% , 89% , 100% and 89% , for rfta , respectively . 
sono stati descritti tre pattern di enhancement alla ceus ( 1 , isovascolare ; 2 , ipovascolare ; 3 , avascolare ) e quindi confrontati con la tc di follow - up . 
nel primo gruppo , la tc ha evidenziato necrosi completa in 28 / 54 ( 52% ) lesioni , di cui 21 ( 75% ) con pattern ceus avascolare , 1 ( 4% ) isovascolare e 6 ( 21% ) ipovascolare . 
sensibilit , specificit , valore predittivo positivo e negativo ed accuratezza diagnostica per necrosi completa alla tc del pattern ceus avascolare sono 75% , 69% , 72% , 72% e 72% dopo pei , 100% , 20% , 89% , 100% e 89% dopo rfta . 
ceus performed immediately after percutaneous ablation of hepatocellular carcinoma to evaluate treatment efficacy is compulsory in the case of rfta but not for pei . keywords contrast - enhanced ultrasound hepatocellular carcinoma ablation therapy radiofrequency ethanol injection computed tomography conclusioni . 
la ceus al termine della procedura ablativa dellepatocarcinoma ai fini della valutazione del successo terapeutico mandatoria dopo rfta , ma non dopo pei . parole chiave ecografia con mdc carcinoma epatocellulare terapie ablative radiofrequenza alcolizzazione tomografia computerizzata introduction introduzione hepatocellular carcinoma ( hcc ) is one of the most common cancers in the world , representing about 85% of primary liver tumours , characterised by an incidence of about 500 , 000 new cases per year [ 1 , 2 ]  . 
based upon the high positive predictive value ( ppv ) and a good cost - effectiveness ratio [ 3 ] , the guidelines published by the american association for the study of liver diseases ( aasld ) recommend ultrasonography as the most useful imaging method for screening and surveillance . surgical resection is still considered to be the treatment of choice for curative therapy for hcc in patients with good hepatic functional reserve ( child - pugh class a and minimal portal hypertension : platelet count > 100 , 000 / mm3 and / or hepatic venous pressure gradient < 10 mmhg )  . however , patients in this category represent only about 15% [ 4 , 5 ]  . 
thus , in recent years , some nonsurgical treatments such as percutaneous ethanol injection ( pei ) [ 6 , 7 ] and radiofrequency thermal ablation ( rfta ) [ 8 , 9 ] were developed . 
the aim of these therapies is to treat patients who are not candidates for resection due to advanced age , underlying diseases , multinodular hccs or unfavorable locations , such as tumours too close to vascular and biliary structures [ 6 , 812 ] , by means of a complete coagulation tumor necrosis . 
usually , the response is monitored with computed tomography ( ct ) , magnetic resonance ( mr ) [ 1517 ] and , more recently , with contrast - enhanced ultrasonography ( ceus ) [ 1722 ]  . 
in most published studies , these examinations are not performed immediately lepatocarcinoma ( hcc ) una delle neoplasie pi comuni al mondo e costituisce l85% dei tumori primitivi del fegato , con incidenza pari a circa 500000 nuovi casi / anno [ 1 , 2 ]  . 
il principale fattore di rischio la cirrosi epatica , in partico ( virus lare quando secondaria ad dellepatite b , hbv , o virus dellepatite c , hcv ) o ad abuso di alcool . 
come raccomandato dalle linee guida pubblicate dallamerican association for the study of liver diseases ( aasld ) , lecografia addominale la tecnica dimmagine pi utilizzata per lo screening e la sorveglianza , avendo un alto valore predittivo positivo [ 3 ] e buon rapporto costoeffacacia . infezioni virali la resezione chirurgica tuttora considerata il gold standard per la terapia curativa dellhcc nei pazienti con buona riserva funzionale epatica ( child - pugh a e minima ipertensione portale : piastrine > 100000 / mm3 e / o gradiente pressorio venoso epatico < 10 mmhg )  . 
pertanto nel corso degli ultimi anni sono stati proposti alcuni tipi di trattamento percutaneo non chirurgico , come liniezione percutanea di etanolo ( pei ) [ 6 , 7 ] e la termoablazione con radiofrequenza ( rfta ) [ 8 , 9 ]  . 
lo scopo di tali trattamenti di poter trattare , mediante il raggiungimento di una completa necrosi coagulativa del tessuto tumorale , i pazienti considerati inoperabili per let avanzata , per comorbilit , per caratteristiche proprie del tumore , come la stretta adiacenza a strutture vascolari e biliari o per la multifocalit delle lesioni [ 6 , 812 ]  . 
inoltre , la resezione nei pazienti cirrotici con ridotta funzionalit epatica conduce ad un significativo rischio di insufficienza epatica post - chirurgica e di recidive post - chirurgiche per foci tumorali non diagnosticati allimaging pre - operatorio . 
 tali trattamenti mini - invasivi consentono peraltro di poter trattare pi volte il paziente , senza ridurre in maniera significativa la funzionalit epatica , con indici di sopravvivenza paragonabili a quelli del trattamento chirurgico [ 7 ]  . una precoce e corretta valutazione della risposta al trattamento rappresenta un importante fattore prognostico della sopravvivenza a lungo termine [ 13 , 14 ]  . 
generalmente , la risposta ai trattamenti viene valutata mediante tomografia computerizzata ( tc ) , risonanza magnetica ( rm ) 1096 radiol med ( 2009 ) 114 : 10941105 but 13 months after the procedure [ 16 , 1821 ]  . 
ceus has been proposed in the early posttreatment phase at 2448 h after the procedure [ 17 , 21 , 22 ]  . the aim of our study was to evaluate the efficacy of ceus , performed immediately after pei and / or rfta treatments , by comparing our results with the ct follow - up . materials and methods from december 2005 to december 2007 , 69 consecutive patients ( 55 men and 14 women ; mean age 69 years ; age range 2889 years ) with a proven diagnosis of hcc and candidates to percutaneous procedures ( pei or rfta ) were included in this prospective study , which was approved by the ethics committee of our institute . 
before all examinations and procedures , all patients gave written informed consent . the inclusion criteria were : ( a ) proven diagnosis of hcc by means of histology or derived from the agreement of two tumour main diagnostic modalities [ 23 ] ; ( b ) good detectability at us ; ( c ) cirrhosis with child - pugh risk class b7 or less ; ( d ) single hcc with main diameter < 5 cm ; ( e ) multinodular hcc ( up to three lesions ) with main diameter < 3 cm per lesion ; ( f ) absence of thrombosis of portal vein or distant metastases ; ( g ) prothrombin time > 50% and platelet count > 60109 / l ; ( h ) refused surgery . the exclusion criteria were : ( a ) cirrhosis with childpugh risk class b8 or more ; ( b ) single hcc with main diameter > 5 cm ; ( c ) multinodular disease with more than three lesions with main diameter > 3 cm per lesion ; ( d ) thrombosis of portal vein ; ( e ) distant metastases ; ( f ) refractory ascites ; ( g ) severe coagulopathy ; ( h ) underlying diseases with a poor life expectancy . 
 all patients , divided into two homogeneous groups , underwent conventional us and ceus before treatment . during the same interventional session , immediately after each single percutaneous procedure , ceus was performed to evaluate residual perfusion within the treated lesion . after 1 month , a contrast - enhanced ct as gold standard was performed to assess the degree of tumour necrosis . 
sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy of ceus after pei or rfta were evaluated and compared with ct findings . 
a p value < 0.05 was considered statistically significant . conventional ultrasonography and contrast - enhanced ultrasonograph the evaluation and precise localisation of the lesions to be [ 1517 ] e , pi di recente , con ecografia con mezzo di contrasto ( ceus ) [ 1722 ]  . 
alcuni autori hanno proposto lapplicazione della ceus nella precoce valutazione dei trattamenti , a 2448 ore dal termine della procedura [ 17 , 21 , 22 ]  . lo scopo del nostro studio stimare la reale efficacia dellecografia con mezzo di contrasto eseguita nellimmediato periodo post - pei e / o rfta , nel corso della stessa sessione interventistica , confrontando i risultati con la tc di follow - up . materiali e metodi da dicembre 2005 a dicembre 2007 sono stati inseriti prospetticamente nello studio 69 pazienti consecutivi ( 55 maschi e 14 femmine ; et media di 69 anni , range : 2889 anni ) con diagnosi certa di epatocarcinoma , candidati a procedure percutanee ( pei o rfta )  . 
sono stati quindi valutati sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) ed accuratezza diagnostica della ceus post - pei o rfta rispetto ai reperti riscontrati in tc . 
il confronto statistico stato effettuato utilizzando il test del 2e valori di p < 0 , 05 sono stati considerati statisticamente significativi . radiol med ( 2009 ) 114 : 10941105 1097 treated was performed by using a sequoia 512 ( acusonsiemens , erlangen , germany )  . 
a nonlinear imaging method that detects the reflected harmonics ( usually the second harmonic ) of a transmitted pulse or a phase inversion method can be used . when a suspected lesion was identified , it was measured routinely . then , the study protocol involved ceus before and immediately after the ablation therapy and performed by the same operator . 
harmonic microbubble - specific imaging with low acoustic us pressure ( 24 mhz transducer ; mechanical index < 0.2 ; 1213 frame rate / s ) was performed utilising the same machine . 
all ceus examinations were recorded on a magneto - optical disk syste a standard real - time dynamic study , in the arterial phase ( hyperechogenicity of the intrahepatic arterial branches ) about 1525 s after contrast injection , and in the portal venous phase ( hyperechogenicity of the portal vein and its intrahepatic branches ) about 4060 s after contrast injection and finally in the late sinusoidal phase ( hyperechogenicity of the hepatic veins ) from 120 s after contrast injection up to 5 min , was performed in all cases . successful treatment was defined when no focal and / or irregular enhancement within the treated lesion during the dynamic study was detected , whereas treatment failure was defined by the presence of residual enhancement within the treated lesion . three enhancement patterns were observed on the treated lesions compared with the liver parenchyma : ( 1 ) isovascular residual lesion perfusion ; ( 2 ) hypovascular residual lesion perfusion ; ( 3 ) avascular lesion perfusion . computed tomography ct was performed at 1 month after the procedure using 6or 64 - row multidetector scanners ( philips , eindhoven , the netherlands )  . 
a nonenhanced ct and a multiphase study after administration of 120140 ml of nonionic contrast agent ( ultravist 370 , schering , berlin , germany ) through an antecubital vein at a 3to 4 - ml / s flow rate were performed . 
scan parameters for all phases were a collimation of 5 mm , table feed / rotation 7.5 / 12 mm and a reconstruction interval of 5 / 3 m utilising a test bolus , the contrast - enhanced ct images were usually acquired with a delay time after contrast injection set at 2530 s for the arterial phase , at 6070 s for the portal venous phase and at > 23 min for the delayed interstitial phase . ecografia basale ed ecografia con mezzo di contrasto la valutazione e la precisa localizzazione delle lesioni da trattare stata eseguita utilizzando un ecografo sequoia 512 ( acuson - siemens , erlangen , germania )  . 
utilizzando una sonda convex multi - frequenza 4c stata eseguita una ecografia convenzionale b - mode del fegato , con scala di grigi , per identificare la lesione focale epatica . 
sono state utilizzate metodiche di imaging non - lineari in grado di identificare le armoniche riflesse ( solitamente la seconda armonica ) di un impulso trasmesso o metodiche di inversione di fase . 
quando una lesione focale sospetta veniva identificata , si procedeva alla sua misurazione . il protocollo di studio prevede quindi lesecuzione , da parte dello stesso operatore , di un esame ceus prima ed immediatamente al termine della procedura percutanea . viene iniettato esafluoruro di zolfo ( dosi di 2 , 4 ml ) in forma di microbolle ( sonovue , bracco , milano , italia ) in una vena antecubitale , con ago - cannula a 20 gauge , in bolo rapido , seguito da 5 ml di soluzione salina . 
 stato utilizzato un imaging armonico specifico per le microbolle , con bassa pressione acustica ( 24 mhz coherent contrast imaging ; indice meccanico < 0 , 2 ; 1213 frame rate / s ) sullo stesso ecografo . 
tutti gli esami ecografici con contrasto sono stati registrati su sistemi magneto - ottici . dopo liniezione del mezzo di contrasto , in tutti i casi stata effettuata unosservazione dinamica in real - time delle fasi contrastografiche : fase arteriosa ( definita dalliperecogenicit dei rami arteriosi intraepatici ) dopo circa 1525 secondi dalliniezione ; fase venosa portale ( definita dalliperecogenicit della vena porta e delle sue diramazioni intraepatiche ) dopo circa 4060 secondi dalliniezione ; fase sinusoidale tardiva ( definita dalliperecogenicit delle vene epatiche , per il progressivo passaggio delle microbolle dopo il loro accumulo a livello sinusoidale ) da 120 secondi a 5 minuti dalliniezione . 
 il successo terapeutico viene definito dallassenza di focale e / o irregolare impregnazione contrastografica nella lesione trattata durante lo studio dinamico , mentre il fallimento terapeutico definito dalla presenza di impregnazione residua nella lesione trattata . 
 sono stati pertanto descritti tre differenti pattern di enhancement a carico delle lesioni trattate , valutate a confronto con il parenchima epatico circostante : ( 1 ) perfusione lesionale residua isovascolare ; ( 2 ) perfusione lesionale residua ipovascolare ; ( 3 ) perfusione lesionale avascolare . tomografia computerizzata un mese dopo la procedura percutanea stata eseguita una tc di controllo , utilizzando macchine a 6 o 64 detettori ( philips , eindhoven , olanda )  . 
sono state effettuate scansioni sia prima che dopo la somministrazione endovenosa di 120140 m di mezzo di contrasto non ionico ( ultravist 370 , schering , berlino , germania ) , con velocit di flusso di 34 ml / s . 
per tutte le scansioni sono stati applicati i seguenti parametri : collimazione di 5 mm , rapporto tra la 1098 percutaneous ethanol injection patients lay down in supine or left lateral position , and after local anaesthesia ( lidocaine s.c. ) , a 20to 22 - gauge needle was percutaneously inserted under us guidance . 
 radiofrequency thermal ablation after total anaesthesia , the active needle electrode ( 1419 gauge ) was inserted percutaneously into the lesion under us guidance , inducing coagulation necrosis through interstitial reactive hyperthermia , without any systemic damage . 
the rf delivery system uses active - needle cooled and expandable electrodes with nine hooks , connected to a high frequency ( 150 - w ) generator ( rita model 1500 , rita medical system , ca , usa )  . 
finally , the needle was removed [ 2527 ]  . data analysis sensitivity , specificity , ppv , npv and accuracy of ceus after pei or rfta compared with ct in terms of presence / absence of residual perfusion remnant / recurrence were evaluated . 
al termine della procedura , la lesione trattata appare come unarea iperecogena [ 24 ]  . termoablazione con radiofrequenza previa anestesia generale , sotto guida ecografica viene inserito nel tessuto neoplastico da trattare un ago - elettrodo attivo ( 1419 g ) per via percutanea per indurre necrosi coagulativa mediante ipertermia reattiva interstiziale , senza alcun danno sistemico . 
il sistema per la termoablazione con radiofrequenza prevede lutilizzo di aghi - elettrodi espandibili a 9 uncini , con punta autoraffreddata , connessi ad un generatore ad alta frequenza a 150 watt ( rita modello 1500 , rita medical system , ca , usa )  . 
sotto guida ecografica stata eseguita una valutazione in tempo reale della procedura termoablativa , con evidenza di un alone iperecogeno . al termine della procedura , lago stato rimosso [ 2527 ]  . analisi dei dati la concordanza tra i risultati ottenuti con la ceus post - trattamento e con la tc eseguita ad un mese stata valutata calcolando sensibilit , specificit , vpp , vpn ed accuratezza diagnostica , in termini di presenza / assenza di perfusione residua sospetta per residuo di malattia a carico delle lesioni trattate . 
le sensibilit del pattern ceus avascolare dopo pei e dopo rfta e lefficacia delle due procedure ablative , in termini di percentuale di necrosi completa ottenuta , sono state valutate e confrontate tra loro con il test del 2 . 
valori di p < 0 , 05 sono stati considerati statisticamente significativi . risultati sono stati reclutati 69 pazienti per un totale di 90 lesioni tutte ipervascolarizzate in fase arteriosa , con numero medio radiol med ( 2009 ) 114 : 10941105 1099 fig . 
d alla tc di follow - up si osserva necrosi completa della lesione trattata ( freccia )  . suggestive for residual tumour in 25 / 54 ( 46% ) lesions , two of which ( 4% ) were characterised by an isovascular and 23 / 54 ( 42% ) by a hypovascular pattern . 
tutti i pazienti sono stati sottoposti a pei o rfta e quindi suddivisi in due gruppi : nel primo gruppo tutti i pazienti trattati con pei e nel secondo gruppo quelli trattati con rfta . la pei stata eseguita in 43 pazienti per un totale di 54 / 90 ( 60% ) noduli con diametro medio di 2 cm ( range : 0 , 54 , 8 cm )  . 
d alla tc di follow - up si osserva necrosi completa della lesione trattata ( freccia )  . thus , in 32 / 36 ( 89% ) cases ( 31 / 31 = 100% cases characterised by complete necrosis and 1 / 5 = 20% cases with residual tumour ) , ct confirmed ceus imaging . 
in 4 / 36 ( 11% ) cases , the agreement between ceus and ct was not satisfied due to 4 / 5 ( 80% ) false positives at ceus . 
 sensitivity , specificity , ppv , npv and accuracy of the avascular pattern at ceus immediately after pei and after rfta , respectively , compared with ct assessment of necrosis performed after 1 month were 75% , 69% , 72% , 72% and 72% for pei and 100% , 20% , 89% , 100% and 89% , for rfta ( table 2 )  . 
in nessun caso alla ceus post - rfta stato evidenziato pattern isovascolare ( tabella 1 )  . pertanto , in 32 / 36 ( 89% ) casi ( 31 / 31 = 100% dei casi con necrosi completa e 1 / 5 = 20% dei casi con residuo tumorale ) la tc ha confermato il reperto ceus ; in 4 / 36 ( 11% ) casi non c stata concordanza tra le due tecniche di immagine per il riscontro ceus di 4 / 5 ( 80% ) falsi positivi . 
 la sensibilit , la specificit , il vpp , il vpn e laccuratezza diagnostica del pattern avascolare alla ceus eseguito immediatamente dopo la procedura di pei rispetto alla necrosi completa dimostrata alla tc ad un mese erano rispettivamente di 75% , 69% , 72% , 72% e 72% . 
il pattern avascolare alla ceus eseguito immediatamente dopo la procedura di rfta rispetto alla tc eseguita un mese dopo ha mostrato invece valori di sensibilit , specificit , vpp , vpn ed accuratezza diagnostica pari a 100% , 20% , 89% , 100% e 89% ( tabella 2 )  . 
infine , la differenza tra lefficacia del trattamento mediante ablazione con radiofrequenza e con alcolizzazione risultata statisticamente significativa ( p < 0 , 05 )  . discussione nel corso degli ultimi anni sono state proposte diverse tecniche per il trattamento ablativo percutaneo dellepatocarcinoma in grado di offrire ottime possibilit terapeutiche ai pazienti non candidabili alla chirurgia . 
tra queste un posto di radiol med ( 2009 ) 114 : 10941105 1103 sensitivity after pei and after rfta showed a p value < 0.05 ( statistically significant difference )  . 
a statistically significant difference ( p < 0.05 ) between the necrosis obtained by rfta and pei was also demonstrated . discussion during recent years , several percutaneous ablation techniques were proposed to treat hcc , offering good therapeutic possibilities for patients who are not candidates for surgery . 
for lesions with a mean diameter from 2 to 4 cm , rfta achieved complete necrosis with fewer sessions [ 29 ]  . evaluation of the efficacy of percutaneous treatments is monitored by imaging techniques , such as contrastenhanced ct or mr [ 1517 ] and recently also by means of ceus [ 1722 ]  . 
high concordance between all these methods has been demonstrated , leading to an important role of ceus for the characterisation and follow - up for hccs [ 20 , 30 , 31 ]  . 
in these studies , ceus was not performed immediately but at least 2448 h or more after treatment [ 17 , 2122 ]  . although ceus is characterised by intrinsic limitations , it is more accessible than other methods and leads to a realtime evaluation of the dynamic vascularity of tissue , which is able to identify vascular structures around and within the lesion [ 1820 , 30 , 31 ]  . 
the correct timing to perform the evaluations is still under discussion , with authors performing the follow - up 1 month [ 21 ] or 2448 h after treatment [ 17 , 21 , 22 ]  . the most important question is the differential diagnosis at ct , the gold standard , between residual tumour and reactive hyperaemia , generally characterised by focal irregular enhancement and regular ring enhancement , respectively . some authors have suggested that a correct follow - up should be performed 3 months after treatment [ 16 ] , when reactive hyperaemia cannot be present , leading to less false positive diagnoses but with a later detection of residual tumour . 
regarding pei , quite a good agreement ( 72% ) between ceus and ct was shown , without any significant difference between cases with residual tumour ( 69% ) and with complete necrosis ( 75% )  . 
in other terms , false positives ( 31% ) and rilievo occupato dallablazione con etanolo ( pei ) e con radiofrequenza ( rfta ) [ 68 , 13 , 14 ]  . 
i risultati ottenuti dalle due tecniche in esame sono apparsi pressoch paragonabili per il trattamento di hcc ipervascolarizzati con diametro2 cm , ma con dimostrato minor rischio di complicanze per la prima [ 28 ] ; per lesioni con diametro compreso tra 2 e 4 cm , la rfta si dimostrata pi efficace nel raggiungimento di necrosi completa in un minor numero di sedute [ 29 ]  . 
 la valutazione dellefficacia dei trattamenti percutanei affidata allimaging radiologico , sostenuto da metodiche consolidate , quali tc e rm con mezzo di contrasto [ 1517 ] , e negli ultimi anni anche dalla ceus [ 1722 ]  . 
numerosi studi hanno dimostrato lelevata concordanza tra le suddette metodiche , decretando pertanto allecografia con mezzo di contrasto un ruolo chiave non solo per la caratterizzazione ed il follow - up degli hcc [ 20 , 30 , 31 ] , ma anche per la valutazione della vascolarizzazione residua nel contesto della lesione trattata [ 17 , 18 , 21 , 22 ]  . 
tuttavia , in questi studi la ceus non viene eseguita immediatamente al termine della procedura interventistica , ma ad almeno 2448 ore o pi dal trattamento [ 17 , 21 , 22 ]  . pur essendo gravato dai noti limiti intriseci della metodica , la ceus rimane senza dubbio di pi facile accesso e rapida esecuzione , consentendo una valutazione dinamica in tempo reale della lesione trattata dopo la somministrazione del mezzo di contrasto , con capacit di identificare vasi perio intra - lesionali [ 1820 , 30 , 31 ]  . 
alcuni autori hanno considerato lipotesi di un corretto follow - up ad un mese [ 21 ] o a 2448 ore dalla procedura percutanea [ 17 , 21 , 22 ]  . il principale limite sembra rappresentato dalla diagnosi differenziale tra residuo ed iperemia reattiva , valutati alla tc di controllo considerata come gold standard di riferimento , e caratterizzati generalmente il primo da impregnazione contrastografica focale , irregolare e la seconda da impregnazione a cercine perilesionale , regolare . 
 col nostro studio ci siamo proposti di valutare lefficacia della ceus effettuata immediatamente al termine della procedura percutanea , pei o rfta , durante la stessa seduta interventistica , in termini di affidabilit nel predire il successo terapeutico . 
per quanto concerne la pei , i risultati hanno dimostrato discreta concordanza ( 72% ) tra le due tecniche di immagine , senza differenza significativa tra il gruppo di casi con residuo tumorale ( 69% ) e quelli con necrosi completa ( 75% )  . 
in altre parole , i falsi positivi ( 31% ) ed i falsi negativi ( 25% ) sono confrontabili e questo esprime una moderata sensibilit dellindagine ( 75% )  . 
per quanto riguarda la rfta , abbiamo documentato una concordanza molto buona ( 89% ) tra i rilievi ceus e tc , in 1104 radiol med ( 2009 ) 114 : 10941105 false negatives ( 25% ) were comparable , resulting in a moderate sensitivity ( 75% )  . 
regarding rfta , a very good agreement ( 89% ) between ceus and ct results was obtained , particularly when the avascular pattern , suggestive for complete necrosis [ 68 , 13 , 14 ] , was detected within the treated lesion . 
furthermore , the high true positive rate ( 100% ) , the few true negative diagnoses ( 20% ) and the absence of false negative diagnoses indicate the greater efficacy of rfta in comparison with pei . finding an avascular pattern at ceus immediately after rfta is highly predictive of a therapeutic success in term of complete necrosis ( sensitivity 100% and ppv 89% ) than after pei ( sensitivity 75% and ppv 72% )  . particolare con assoluta affinit in caso di pattern avascolare ( 100% ) , espresso alle metodiche di imaging con mezzo di contrasto come assenza di flusso nel contesto della lesione trattata ed espressione pertanto di necrosi coagulativa completa [ 68 , 13 , 14 ]  . 
inoltre , considerando lelevata percentuale di veri positivi ( 100% ) , lesigua percentuale di veri negativi ( 20% ) e lassenza di falsi negativi , dal nostro studio risulta chiaramente evidente la maggior efficacia della rfta rispetto alla pei . 
 per concludere , il riscontro di pattern avascolare alla ceus eseguita immediatamente dopo la procedura percutanea fortemente predittivo per successo terapeutico ( sensibilit 100% e vpp 89% ) dopo rfta , ma non dopo pei ( sensibilit 75% e vpp 72% )  . 
this is made possible by using midto low - end scanners and simple acquisition techniques accessible to both radiologists and clinicians . major advantages include ready availability at the bedside , the absence of ionising radiation , high reproducibility and cost efficiency . 
when such artefacts are widely detected on anterolateral transthoracic lung scans , diffuse alveolar - interstitial syndrome can be diagnosed , which is often a sign of acute pulmonary oedema . 
this condition rules out exacerbation of copd as the main cause of acute dyspnoea . keywords lung ultrasound dyspnea pulmonary oedema alveolar - interstitial syndrome riassunto in questo lavoro viene discussa lutilit dellecografia polmonare nella diagnosi delle diverse cause di dispnea acuta in emergenza , in particolare focalizzando lattenzione sulla diagnosi differenziale tra ledema polmonare e la riacutizzazione della broncopneumopatia cronica ostruttiva ( bpco )  . 
quando tali artefatti sono diffusamente visualizzati nelle scansioni trans - toraciche antero - laterali , possibile diagnosticare la sindrome alveolo - interstiziale diffusa , che spesso un segno di edema polmonare acuto . 
questa condizione esclude la riacutizzazione di bpco quale causa di dispnea acuta . parole chiave ecografia polmonare dispnea edema polmonare sindrome alveolo - interstiziale 1054 introduction the new millennium , diagnostic imaging has with continued to advance rapidly on all fronts as a result of advances in technology and information systems . 
its application to chest diagnostics has always been considered impossible given the poor accessibility of the lung to ultrasound ( us ) , as opposed to the study of more superficial structures , both muscular and subcutaneous , where us has always been widely used and accepted . 
obstacles to the sonographic study of deep chest structures are related to both the air content of the lung and the bone component of the rib cage , which prevent penetration of the us beam and lead to the development of artefacts . 
this , combined with the widespread use of conventional radiology and the development of multidetector computed tomography ( mdct ) , has hindered the application of us imaging to the lung . 
in recent years , the use of us as a clinical tool in the emergency setting where the patients critical condition limits any clinical evaluation and impairs the quality of chest radiographs , as well as preventing access to more complex modalities such as mdct has become increasingly popular , leading to the development of new applications . 
evaluation of the lung is among the most innovative . the latest developments in lung us are based on the interpretation of a few signs ( mostly artefacts ) rather than on technological advances . 
analysis of the correlations of artefact patterns with clinical and radiological diagnoses in intensive care unit ( icu ) patients led to the important insights of lichtenstein et al . , the first to describe the potential of us in the diagnosis of alveolarinterstitial syndrome [ 1 ]  . 
growing interest in the practical applications of lung us bodes well for its future as an increasingly indispensable tool for intensivists , emergency medicine physicians and radiologists . this paper describes the clinical application of lung us in the recognition of alveolarinterstitial syndrome , focusing in particular on the differential diagnosis between pulmonary oedema and exacerbation of chronic obstructive pulmonary disease ( copd ) as causes of acute dyspnoea . the first part examines the reasons for the complexity of the differential diagnosis of the possible causes of acute dyspnoea ( in particular , cardiogenic and respiratory causes ) at the patients bedside in the emergency department and analyses the potential benefits of lung us compared with radiological techniques . 
the second part describes the us radiol med ( 2009 ) 114 : 10531064 introduzione nel nuovo millennio la diagnostica per immagini ha continuato a progredire a ritmi elevati su tutti i fronti , spinta dallo sviluppo tecnologico e dei sistemi informatici . lecografia b - mode non una nuova tecnologia , in quanto venne proposta per la prima volta per scopi medici pi di cinquanta anni fa . 
la sua applicazione nelle procedure diagnostiche delle malattie del torace sempre stata considerata impossibile per la scarsa accessibilit del polmone agli ultrasuoni , al contrario dello studio delle strutture pi superficiali , sia muscolari che sottocutanee , dove lecografia ha sempre mantenuto un ruolo diffusamente accettato . 
gli ostacoli allo studio ecografico delle strutture toraciche profonde sono dovuti sia al contenuto aereo polmonare sia alla componente ossea della gabbia toracica , che impediscono la progressione del fascio ultrasonoro e causano lo sviluppo di artefatti . 
questa considerazione , insieme al diffuso utilizzo della radiologia tradizionale ed al progressivo sviluppo della tomografia computerizzata multidetetettore ( tcmd ) , ha impedito per diversi anni lo sviluppo di metodiche ecografiche di imaging del polmone . negli ultimi anni , lutilizzo degli ultrasuoni come strumento clinico da applicare nel paziente in emergenza , laddove la criticit del malato limiti sia la valutazione clinica sia la qualit della radiografia del torace , precludendo anche laccesso a metodiche complesse quali la tcmd , sta ottenendo consensi crescenti che hanno portato allo sviluppo di nuove applicazioni . 
piuttosto che sul progresso tecnologico , i pi recenti sviluppi dellecografia polmonare si sono basati sulla scoperta del significato di alcuni segni ( per lo pi veri e propri artefatti )  . 
le analisi delle correlazioni di alcuni patterns di artefatti con le diagnosi cliniche e radiologiche in pazienti in unit di terapia intensiva ( uti ) , hanno condotto alle importanti intuizioni di lichtenstein et al . 
 [ 1 ] , i primi a descrivere le possibilit della diagnosi mediante ecografia della sindrome alveolo - interstiziale . questa condizione morbosa caratterizza molte patologie eterogenee che hanno in comune un diffuso coinvolgimento dellinterstizio polmonare con conseguente riduzione della capacit di scambio alveolo - capillare . 
il crescente interesse nelle sue applicazioni pratiche , fa prevedere per lecografia polmonare un futuro come strumento sempre pi indispensabile per il medico dellunit di terapia intensiva , per i medici di medicina durgenza ed anche per il radiologo . 
in lapplicazione clinica questo articolo descriveremo dellecografia polmonare nel riconoscimento della sindrome alveolo - interstiziale , focalizzando lattenzione tra edema soprattutto sulla diagnosi differenziale radiol med ( 2009 ) 114 : 10531064 1055 technique used for the diagnosis of alveolarinterstitial syndrome , providing the reader with the latest data published in the literature . differential diagnosis of acute dyspnoea the emergency diagnosis and management of adults with acute dyspnoea remains a major challenge , often with many pitfalls . 
in some cases , this problem cannot be readily solved , especially in emergency settings , and in elderly patients who often have associated disorders and atypical clinical presentations [ 2 , 3 ]  . 
the literature indicates that the diagnosis of each lung abnormality whether restrictive , obstructive , or due to increased ventricular filling pressure traditionally relies on the integration of different diagnostic information . 
this includes physical signs , case history and results of conventional diagnostic tests such as chest radiography , electrocardiogram and laboratory investigations [ 4 , 5 ]  . when taken individually , both the physical examination and the history have insufficient specificity [ 68 ]  . 
radiographic signs such as redistribution of blood flow to the apices , blurring of the pulmonary vessels , and cardiomegaly have good predictive value but depend on the quality of the examination and on the radiologists skill and experience [ 5 , 9 ]  . 
recent studies show that chest radiography is often misleading in the evaluation of patients with decompensated heart failure in emergency settings [ 10 ] and may lead to diagnostic errors and inappropriate treatment . 
blood natriuretic peptide ( bnp and nt - pro bnp ) assays have recently been described as accurate tests for diagnosing heart failure . however , the precise role of these peptides in the emergency room has still to be clarified and validated [ 1114 ]  . electrocardiography is not sufficiently accurate for a correct diagnosis [ 15 ]  . 
transthoracic echocardiography allows exclusion of left ventricular dysfunction or right heart overload but fails to identify diastolic dysfunction , which may be the main cause of cardiac failure in approximately 50% of cases [ 16 ]  . 
pulsed doppler and tissue doppler are recent additions that allow estimation of left ventricle filling pressures and , as a result , identification of diastolic dysfunction [ 17 , 18 ]  . 
however , although relatively easy to apply , these methods require complex and expensive equipment that is not always available to emergency physicians and radiologists . lung us has been shown to have greater diagnostic accuracy in differentiating the causes of acute dyspnoea in emergency settings compared with the traditional methods commonly employed in emergency departments ( ed )  . 
its polmonare e riacutizzazione della broncopneumopatia cronica ostruttiva ( bpco ) quali cause di dispnea acuta . nella prima parte esamineremo le motivazioni per cui la diagnosi differenziale tra le diverse cause di dispnea acuta ( in particolare cause cardiogene e cause respiratorie ) al letto del paziente in urgenza pu essere complessa ed analizzeremo i potenziali benefici dellecografia polmonare rispetto alle tecniche radiologiche . 
la seconda parte si propone di descrivere la tecnica ecografica utilizzata per la diagnosi della sindrome alveolo - interstiziale , fornendo un aggiornamento sui dati pi recenti pubblicati in letteratura . diagnosi differenziale della dispnea acuta la diagnosi e la gestione in urgenza dei pazienti adulti con dispnea acuta ancora oggi da considerare una grande sfida , spesso con molte insidie . 
alcune volte questo problema non facile da risolvere , in particolare in emergenza e nei pazienti anziani che spesso hanno patologie associate e presentazioni cliniche atipiche [ 2 , 3 ]  . 
noi sappiamo dalla letteratura che la diagnosi di ogni alterazione polmonare , sia essa restrittiva , da ostruzione al flusso aereo , da aumento della pressione di riempimento ventricolare cardiaco , tradizionalmente si basa sulla integrazione di vari dati diagnostici . 
tali sono i segni fisici , i dati anamnestici ed i risultati dei test diagnostici tradizionali quali radiografia del torace , elettrocardiogramma e dati di laboratorio [ 4 , 5 ]  . quando considerati singolarmente , sia lesame fisico che i dati anamnestici non sono dotati di sufficiente specificit [ 68 ]  . 
i segni radiografici , quali la redistribuzione del flusso verso gli apici , la sfumatura dei vasi polmonari e la cardiomegalia , dimostrano buoni valori predittivi , ma sono dipendenti dalla qualit dellesame e dallabilit ed esperienza dello specialista radiologo [ 5 , 9 ]  . 
inoltre , recenti studi riportano che la radiografia del torace spesso fuorviante nella valutazione dei pazienti con insufficienza cardiaca scompensata in emergenza [ 10 ] , potendo condurre ad errori diagnostici e conseguenti terapie inappropriate . 
lecocardiografia transtoracica permette di escludere la disfunzione del ventricolo sinistro o il sovraccarico cardiaco destro , ma non consente di identificare la disfunzione diastolica che in circa il 50% dei casi pu essere la causa principale della 1056 radiol med ( 2009 ) 114 : 10531064 major advantages , particularly over radiographic techniques , are the absence of ionising radiation , speed and the fact that it is unaffected by the patients breath - hold limitations or agitation [ 19 ]  . 
the required information can be obtained by using linear , abdominal and microconvex probes , but to analyse comet - tail artefacts , low frequencies have to be used to allow the us beam to reach the deeper structures . 
a review of the literature shows that there is disagreement as to the most effective probe , although the earliest published experience on us diagnosis of alveolarinterstitial syndrome was performed with a 5mhz microconvex probe [ 1 ]  . 
the most influential opinion on this subject is that of lichtensteins group , who consider the microconvex probe to be most effective , as it combines sufficient penetration depth to enable analysis of vertical artefacts with sufficient compactness to allow satisfactory analysis of the intercostal spaces [ 19 ]  . 
in our studies and daily experience , we have used a 3.5 - mhz convex abdominal probe that offers the advantage of combining a wider and more effective depiction of the pleural surfaces with the ability to examine deeper structures [ 20 ]  . 
this type of probe is also preferred by other authors because of the characteristics described above [ 21 ]  . sonographic signs the lung is characterised by a mixture of water and air , and disruption of their balance underlies the pathophysiology of lung diseases . 
the sonographic probe can detect this imbalance as a result of the very different acoustic impedance values of air and water , and the contrast between these two elements generates pulmonary artefacts that enable diagnosis . 
solo recentemente stato introdotto luso del doppler pulsato e del doppler tissutale che permettono la stima delle pressioni di riempimento del ventricolo sinistro , e quindi lidentificazione della disfunzione diastolica [ 17 , 18 ]  . 
si tratta per di metodiche che , pur essendo di applicazione relativamente facile , necessitano di sistemi complessi e costosi non sempre a disposizione del medico durgenza e del radiologo . lecografia polmonare ha dimostrato valori di accuratezza diagnostica pi elevati nella diagnosi differenziale delle cause di dispnea acuta in urgenza rispetto alle comuni metodiche che tradizionalmente vengono utilizzate nel dipartimento di emergenza ( dea )  . 
essa presenta alcuni sicuri vantaggi in particolare rispetto alle tecniche radiografiche , in quanto priva di radiazioni ionizzanti , una metodica di rapida ed immediata esecuzione , e non influenzata da due fattori quali limpossibilit a mantenere una sufficiente apnea inspiratoria o lo stato di agitazione del paziente [ 19 ]  . 
inoltre , consente di distinguere fra lesioni solide o liquide ( consolidamenti vs versamento ) e fornisce informazioni dinamiche , permettendo di osservare le strutture in movimento in tempo reale . apparecchiatura la visualizzazione delle patologie della parete toracica , della pleura e del polmone richiede una apparecchiatura ecografica b - mode di tipo convenzionale senza la necessit di ricorrere a tecniche e tecnologie pi sofisticate , quali lutilizzo del mezzo di contrasto o il color doppler . 
le informazioni necessarie possono essere ottenute utilizzando sonde lineari , addominali e microconvex , ma per lanalisi degli artefatti a coda di cometa dobbiamo avvalerci di basse frequenze in modo da permettere al fascio di ultrasuoni di estendersi alle strutture pi profonde . 
da una analisi della letteratura , vi discordanza di vedute su quale sia il tipo di sonda pi efficace , ma la prima esperienza pubblicata sulla diagnosi ecografica della sindrome alveolo - interstiziale stata eseguita utilizzando la sonda di tipo microconvex da 5 mhz [ 1 ]  . 
lopinione pi autorevole su questo argomento viene dal gruppo di lichtenstein , il quale considera la sonda microconvex come la pi indicata , in quanto unirebbe il vantaggio di penetrare sufficientemente in profondit per permettere lanalisi degli artefatti verticali con quello di essere abbastanza compatta da inserirsi negli spazi intercostali del torace [ 19 ]  . 
nei nostri studi ed esperienza quotidiana utilizziamo una sonda addominale convex da 3.5 mhz , la quale presenta il vantaggio di unire la possibilit di una pi ampia ed efficace visualizzazione dei foglietti pleurici con la capacit di esaminare le strutture pi profonde [ 20 ]  . altri autori concordano sulla preferenza di questo tipo di sonda per le caratteristiche descritte [ 21 ]  . radiol med ( 2009 ) 114 : 10531064 1057 between fig . 
the typical sonographic sign is a vertical artefact originally called comet tail or b - line [ 1 , 22 , 23 ] , or also lung comet by some authors [ 24 , 25 ]  . 
we know from the literature how to define b - lines , which exhibit the characteristics described above and should be distinguished from other similar artefacts that have different properties and meanings , such as eand z - lines . 
e - lines are vertical , similar to b - lines , but originate from the chest wall and not from the pleural line , as they segni ecografici il polmone caratterizzato da una commistione di aria e acqua , e il turbamento del loro equilibrio il principio che sta alla base della fisiopatologia delle malattie polmonari . la sonda ecografica in grado di rilevare questo squilibrio , in quanto aria ed acqua hanno valori di impedenza acustica opposta . 
3 scansione ecografica intercostale obliqua che dimostra la presenza di numerosi artefatti a coda di cometa o linee b , con una distanza tra di loro inferiore ai 7 mm ( quadro definito anche lung rockets )  . 
in the sonographic images on either side of the radiogram , the presence of multiple adjacent comet - tail artefacts ( at least three per scan and in all chest areas examined ) can be easily distinguished . 
4 tipico pattern ecografico della sindrome interstizio - alveolare diffusa ( ai lati ) e corrispondente radiografia del torace ( al centro ) in un paziente affetto da edema polmonare acuto cardiogeno . 
nelle immagini ecografiche ai lati della radiografia , facilmente distinguibile la presenza di multipli e ravvicinati artefatti a coda di cometa ( almeno 3 per scansione , presenti in tutti i settori toracici esaminati )  . 
z - lines are also vertical lines that , like b - lines , originate from the pleural line but end before the bottom of the screen , fading out within a few centimetres [ 23 ]  . 
their significance is still uncertahow many b - lines have to be identified in a lung scan to be considered pathological ? isolated b - lines may be detected in any chest scan , even in normal lungs . 
dal confronto con le immagini tc si evince come le linee b corrispondano ai setti interlobulari edematosi [ 1 ]  . tali strutture hanno uno spessore non superiore ai 700 radiol med ( 2009 ) 114 : 10531064 1059 pathological pattern is instead characterised by multiple blines seen in a single scan ( b + pattern )  . 
it has been demonstrated that the separation between individual lines should never exceed 7 mm , as this distance corresponds to that existing between two subpleural interlobular septa [ 1 ]  . these artefacts thus have the same clinical relevance as kerley b - lines , which can often be seen on chest radiographs of patients with interstitial oedema . 
the discrepancy between these criteria is due to the greater extension of the pleural line , which can be depicted with a linear probe rather than with a microconvex probe . 
our criterion for defining a b + scan with an abdominal convex probe is based on recognition of at least three artefacts per scan , with a maximum distance between adjacent b - lines of 7 mm [ 20 ]  . 
anterior areas extend from the sternal border line to the anterior axillary line and are divided into an upper and a lower half , located between the clavicle and the second / third intercostal spaces and between the third intercostal space and the diaphragm , respectively . 
once the sonographic image of the pleural line has been obtained by identifying the ribs and the so - called bat micrometri , quindi al di sotto della risoluzione degli ultrasuoni . 
sappiamo dalla letteratura come definire le linee b , che presentano le caratteristiche appena descritte e che devono essere distinte da altri artefatti simili , ma con propriet e significato differente , come le linee e e z . 
le linee e sono linee verticali simili alle linee b ma originano dalla parete toracica e non dalla linea pleurica , essendo presenti in caso di enfisema sottocutaneo [ 23 ]  . 
le linee z sono anchesse linee verticali che , come le linee b , originano dalla linea pleurica , estinguendosi per prima del fondo dello schermo e svanendo in pochi centimetri [ 23 ]  . 
quante linee b si devono individuare in una scansione polmonare per essere considerate patologiche ? linee b isolate possono essere rilevate in qualunque scansione toracica del polmone anche in polmoni normali . 
stato dimostrato che la separazione tra le singole linee non deve mai essere superiore a 7 mm , in quanto questa distanza riflette quella tra 2 setti interlobulari a localizzazione subpleurica [ 1 ]  . 
in alcuni casi gli artefatti ecografici a coda di cometa possono essere pi vicini , con distanza tra di loro fino a 3 mci corrisponderebbe al coinvolgimento dellinterstizio intralobulare , che si traduce nelle tecniche radiologiche con il classico pattern a vetro smerigliato oppure con pattern di microreticolazione se viene eseguita la tc ad alta risoluzione . 
per convenzione viene comunemente accettato che , utilizzando la sonda microconvex , sia sufficiente lindividuazione di tre linee b per considerare positiva una scansione polmonare . in uno studio eseguito con sonda lineare , reissig et al . 
il nostro criterio per definire una scansione con un pattern b + utilizzando una sonda convex addominale si basa sul riconoscimento di almeno tre artefatti per scansione , con una distanza tra le linee b adiacenti non superiore ai 7 mm [ 20 ]  . 
le aree anteriori sono comprese tra la linea margino - sternale e la linea ascellare anteriore , e sono suddivise in una met superiore ed una inferiore , rispettivamente comprese tra la clavicola e il secondo - terzo spazio intercostale e dal terzo spazio intercostale al diaframma . le aree laterali sono comprese tra la linea ascellare anteriore e quella posteriore e sono suddivise in una met superiore ed una inferiore o basale . 
una volta ottenuta limmagine ecografica della linea pleurica attraverso lindividuazione delle coste e la visualizzazione del cosiddetto segno del pipistrello ( bat sign , vedere la figura 6 e la didascalia per la spiegazione ) [ 23 ] , ruotiamo la sonda per ottenere una scansione intercostale che consenta di visualizzare la pi ampia estensione possibile della porzione di pleura ( scansione obliqua )  . 
il tempo necessario per eseguire lesame varia da pochi secondi a 12 minuti [ 1 , 20 ]  . la definizione di un esame ecografico polmonare positivo richiede alcune attente considerazioni . 
 [ 1 ] si espressero in modo generico , asserendo semplicemente che il riscontro di un pattern b + da ambo i lati nelle aree anteriori del torace sufficiente per la diagnosi di sindrome alveolointerstiziale [ 1 ]  . 
in una recentissima pubblicazione , gli stessi autori hanno proposto il protocollo blue ( bedside lung ultrasound examination ) nella insufficienza respiratoria acuta , che prevede la esclusione della diagnosi di edema polmonare acuto quando le scansioni anteriori non presentino linee b predominanti bilateralmente [ 27 ]  . 
5 schematic subdivision of the anterolateral chest wall into eight areas . areas 1 , 2 , 5 and 6 correspond to the upper and lower right and left anterior quadrants , respectively . 
6 a longitudinal sonographic lung scan displaying the typical bat sign . this pattern appears when the pleural line , in the middle , is surmounted by the two adjacent lateral ribs , resembling a flying bat . 
questa immagine si evidenzia quando la linea pleurica , disposta al centro , sovrastata dalle due coste , disposte ai lati , in maniera tale da simulare un pipistrello in volo . 
the time required to carry out the examination varies from a few seconds to 12 min [ 1 , 20 ]  . defining a lung us scan as positive requires careful consideration . 
made the general statement that the finding of a b + pattern on both sides in the anterior areas was sufficient to establish a diagnosis of alveolarinterstitial syndrome [ 1 ]  . 
in a recent publication , the same authors suggested employing the bedside lung ultrasound examination ( blue ) protocol for acute respiratory failure , a protocol that excludes a diagnosis of acute pulmonary oedema when the anterior scans show no predominant b - lines bilaterally [ 27 ]  . 
when applying lung us to cardiological settings , other authors have defined a positive examination as one characterised by multiple bilateral comet - tail artefacts disseminated along the anterolateral surface or restricted to the lateral surface of the lung [ 28 ]  . 
in our opinion , the routine practice of an ed , in particular , requires a more precise definition of a positive ( or pathological ) examination , as the diseases seen in the ed are more diverse and often less severe than those seen in the icu and cardiology departments . 
furthermore , that many b - lines may also be detected when performing lateralbasal scans in patients with normal lungs , with rates ranging from 14% to 28% [ 1 , 26 , 29 ]  . 
in our experience , multiple b - lines ( b + ) have been identified in transthoracic us scans in patients presenting to the ed with different diagnoses , even in the presence of normal lungs . 
another aspect to be emphasised is that b - lines may also be found in areas surrounding parenchymal consolidation of various origins [ 1 , 20 , 30 , 31 ]  . 
these findings may therefore be confusing when lung us is used to exclude alveolarinterstitial syndrome . this is why we believe that recognition of the b + pattern in at least two scans per hemithorax should be adopted as a criterion for diagnosing diffuse alveolarinterstitial syndrome when four anterolateral scans per hemithorax are performed [ 20 , 30 ]  . 
an probabilmente il criterio di limitare lesame polmonare alle scansioni toraciche anteriori sufficiente solo nei pazienti critici con insufficienza respiratoria severa , ricoverati in uti . applicando lecografia polmonare in ambiente cardiologico , altri autori hanno definito come positivo un esame caratterizzato dalla presenza di multipli artefatti a coda di cometa bilaterali e disseminati lungo la superficie antero - laterale o limitati alla superficie laterale del polmone [ 28 ]  . 
nella nostra opinione , specialmente nella pratica quotidiana di un dea , occorre una definizione pi precisa di ci che dovrebbe essere considerato positivo ( o patologico ) , in quanto le malattie sono pi varie e spesso meno gravi rispetto alle patologie presenti nelle uti ed in ambiente cardiologico . inoltre , i dati provenienti dalla letteratura dimostrano che molte linee b possono essere riconosciute anche nelle scansioni latero - basali di pazienti con polmoni normali . 
nella nostra esperienza su pazienti presentatisi in dea con diagnosi diverse , linee b multiple ( b + ) sono state evidenziate in scansioni ecografiche trans - toraciche anche in caso di polmoni normali . 
un altro punto da sottolineare che le linee b possono anche essere ritrovate in aree circostanti addensamenti parenchimali di varia origine [ 1 , 20 , 30 , 31 ]  . 
di conseguenza , la rilevazione di linee b in alcune aree del torace non necessariamente correlata con una patologia interstiziale diffusa del polmone . tali reperti possono quindi essere confondenti nel momento in cui venga applicata lecografia polmonare per escludere la sindrome alveolo - interstiziale . 
questo il motivo per cui secondo noi dovrebbe essere adottato il criterio del riconoscimento del pattern b + in almeno 2 scansioni per ciascun emitorace per porre diagnosi di sindrome alveolo - interstiziale diffusa , allorquando vengano effettuate 4 scansioni antero - laterali per emitorace [ 20 , 30 ]  . 
uno scorretto inquadramento diagnostico tra cause cardiogene o polmonari di dispnea acuta pu tradursi in un pericoloso ritardo terapeutico oppure nellimpiego di farmaci inutili . linterpretazione dei segni radiologici tradizionali di sovraccarico del piccolo circolo , quali la redistribuzione di flusso e ledema interstiziale , sono spesso discutibili e soggettivi specialmente nel caso di radiografie del torace di scarsa qualit tecnica . 
inoltre linterpretazione di un radiogramma del torace a paziente supino e poco collaborante piena di insidie e la corretta interpretazione delle immagini necessita 1062 radiol med ( 2009 ) 114 : 10531064 table 1 distribution of 85 positive scans ( b + lines ) recorded in the 8 individualized areas of transthoracic lung ultrasound in a group of 145 patients with normal lungs at chest radiography and clinical final diagnosis ( 30 ) tabella 1 distribuzione delle 85 scansioni positive ( linee b + ) ottenute nelle 8 aree esaminate in un gruppo di 145 pazienti con polmoni normali al radiogramma del torace e con normale diagnosi clinica finale ( 30 ) areas of thoracic ultrasound positive scans settori esaminati scansioni positive upper anterior right lower anterior right upper lateral right latero - basal right upper anterior left lower anterior left upper lateral left latero - basal left 2 , 8 18 , 6 22 , 8 antero - superiore destro anterinferiore destro latero - superiore destro latero - basale destro antero - superiore sinistro antero - inferiore sinistro latero - superiore sinistro latero - basale sinistro 2 , 8 18 , 6 22 , 8 cardiogenic or pulmonary causes of acute dyspnoea may lead to dangerous delays in treatment or use of unnecessary drugs . interpretation of the conventional radiology signs of overload of the pulmonary circulation , such as blood flow redistribution and interstitial oedema , are often questionable and subjective , especially in the case of poor - quality chest radiographs . 
interpretation of a chest radiogram of a supine and poorly cooperating patient is full of pitfalls , and correct interpretation may call for specific competences . the availability of a us scanner 24 h a day in the ed allows emergency physicians , intensivists or radiologists to confirm or exclude alveolar - interstitial syndrome and settle any interpretation doubts regarding the chest radiogram . two published studies have assessed the accuracy of lung us for recognising alveolarinterstitial syndrome , comparing us with chest radiography and the final clinical diagnosis . 
another study performed by intensivists in the ed concluded that us recognition of diffuse interstitial through b - line detection allows some involvement pulmonary diseases to be rapidly ruled out , in particular , copd exacerbation , which is one of the most common causes of acute dyspnoea [ 32 ]  . 
the same paper demonstrated that us signs of diffuse alveolarinterstitial syndrome were seen in all patients with pulmonary oedema but were absent in a vast majority of patients with copd exacerbation ( 100% sensitivity and 92% specificity ) [ 32 ]  . recently , the same group published the results of a thorough assessment of the effectiveness of lung us in the differential diagnosis of the main causes of respiratory failure , reporting excellent accuracy values [ 27 ]  . 
la disponibilit di un ecografo 24 ore su 24 in dea consente al medico durgenza , rianimatore o radiologo di confermare od escludere in qualsiasi momento la sindrome alveolo - interstiziale e dirimere alcuni dubbi interpretativi sul radiogramma del torace . ci sono due studi pubblicati che hanno valutato laccuratezza dellecografia polmonare nel riconoscimento della sindrome alveolo - interstiziale , ponendola a confronto con la radiografia del torace e la diagnosi clinica finale . 
il secondo studio stato eseguito in un dea , ed ha dimostrato risultati simili al precedente ( sensibilit 85 , 7% , specificit 97 , 7% , fattibilit 98 , 3% , variabilit inter - osservatori 4 , 9% ) [ 20 ]  . 
in un altro lavoro eseguito da rianimatori in dea , gli autori hanno concluso che il riconoscimento con esame ecografico di un coinvolgimento interstiziale diffuso grazie alla visualizzazione delle linee b , permette di escludere rapidamente alcune patologie polmonari ma specialmente la riacutizzazione di bpco , una delle cause di dispnea acuta di pi frequente riscontro [ 32 ]  . 
nello stesso lavoro stato dimostrato che i segni ecografici della sindrome alveolo - interstiziale diffusa erano presenti in tutti i pazienti con edema polmonare , ma assenti nella grande maggioranza dei pazienti con riacutizzazione di bpco ( sensibilit del 100% e specificit del 92% ) [ 32 ]  . 
recentemente lo stesso gruppo ha prodotto i risultati di una attenta valutazione della efficacia della tecnica ecografica polmonare nella diagnosi differenziale di tutte le principali cause di insufficienza respiratoria , dimostrando ottimi valori di accuratezza [ 27 ]  . 
l archiviazione dei dati permette di monitorare levoluzione della congestione polmonare durante il trattamento medico di pazienti affetti da scompenso cardiaco radiol med ( 2009 ) 114 : 10531064 1063 known that us allows acquisition and storage of digital films , and this is a further , undoubted advantage over the plain evaluation of clinical signs during a physical examination . 
data storage allows one to monitor the evolution of pulmonary congestion during medical management of acute cardiac decompensation and to observe the gradual resolution of the b + pattern [ 3335 ]  . 
a number of studies have documented that lung us targeted to detection of b + lines can be easily performed by general radiologists and even by clinicians , such as cardiologists , intensivists and emergency physicians [ 1 , 20 , 24 , 26 , 36 , 37 ]  . a further aspect to be emphasized is that the thickening of interlobular septa , as seen on high - resolution ct , is not a highly specific sign , as it can manifest in different interstitial diseases of various aetiology . 
the b + pattern cannot distinguish between the various acute and chronic diseases underlying the interstitial syndrome , such as cardiac decompensation , acute respiratory distress syndrome ( ards ) , interstitial pneumonia and pulmonary fibrosis . 
we are convinced that integration of us data with those from other emergency bedside investigations , patient history and physical examination can better guide the diagnosis , even in dubious cases . 
moreover , observation of changes in the lung us pattern during medical treatment can facilitate diagnosis for example , in the event of a failure to induce any reduction or disappearance of b - lines after diuretic therapy or continuous positive airway pressure ( c - pap ) , an event that would exclude the cardiogenic origin of alveolarinterstitial syndrome [ 33 ]  . finally , some theories exist concerning the possibility of differentiating between hydrostatic ( cardiac decompensation ) and ards by analysing the distribution of b - lines , pleural sliding and subpleural alveolar consolidation [ 21 ]  . these theories are still to be validated . 
these are readily identifiable us signs that represent the indirect visualisation of interlobular septal thickening due to oedema or fibrosis and intra - alveolar fluid and allow a bedside differential diagnosis between oedema and copd exacerbation as causes of acute dyspnoea in the emergency setting . we believe that lung us , in its new role as a visual stethoscope , will be rapidly taken up in the daily practice of radiologists , emergency physicians , intensivists , cardiologists and pneumologists . 
diversi studi hanno documentato come lecografia polmonare dedicata al riconoscimento delle linee b + possa essere facilmente eseguita da radiologi generali ed anche da clinici come i cardiologi , i rianimatori e i medici durgenza [ 1 , 20 , 24 , 26 , 36 , 37 ]  . a completamento delle precedenti osservazioni occorre sottolineare che lispessimento dei setti interlobulari , come accade per la tcar , non un segno molto specifico potendo essere presente in diverse patologie dellinterstizio polmonare con diversa eziologia . 
il pattern b + non in grado di distinguere tra le diverse malattie acute e croniche causa della sindrome interstiziale , come lo scompenso cardiaco , la sindrome da distress respiratorio acuto ( ards ) , la polmonite interstiziale e le fibrosi polmonari . 
siamo convinti che lintegrazione dellecografia con altri esami eseguibili in urgenza al letto del paziente e con i dati anamnestici e dellesame fisico , permetta un pi efficace orientamento diagnostico anche nei casi dubbi . 
inoltre , losservazione delle modifiche del pattern ecografico polmonare durante il trattamento medico pu facilitare lorientamento , come per esempio nel caso di una mancata riduzione o scomparsa delle linee b dopo terapia diuretica o ventilazione a pressione positiva continua ( c - pap ) , fenomeno che negherebbe lorigine cardiogena della sindrome alveolointerstiziale [ 33 ]  . 
infine , esistono alcune teorie ancora da validare che prevederebbero per esempio la diagnosi differenziale ecografica tra edema polmonare idrostatico ( scompenso cardiaco ) e lesionale ( ards ) attraverso lanalisi della distribuzione delle linee b , dello scorrimento pleurico e dei consolidamenti alveolari sub - pleurici [ 21 ]  . 
il riconoscimento ecografico al letto del paziente di una sindrome alveolo - interstiziale diffusa si basa sulla ricerca e riconoscimento degli artefatti verticali iperecogeni detti a coda di cometa o linee b . 
questi sono segni ecografici semplici da riconoscere che rappresentano la visualizzazione indiretta dei setti interlobulari ispessiti da edema o fibrosi e dei fluidi intralveolari , e permettono la diagnosi differenziale al letto del paziente tra edema o riacutizzazione di bpco come cause di dispnea acuta in emergenza . 
di fisica sanitaria , irccs casa sollievo della sofferenza , san giovanni rotondo , italy 6facolt di medicina , universit di bari , bari , italy 7dipartimento di radiologia , universit novara , novara , italy 8dipartimento di scienze neurologiche e psichiatriche dellet evolutiva , universit la sapienza , roma , italy 9dipartimento di radiologia , azienda ospedaliera universitaria , umberto i , torrette , ancona , italy correspondence to : t . 
scarabino , via napoli 56 , 70031 andria , italy , tel . : + 39 - 088 - 3299140 , fax : + 39 - 088 - 3299220 , e - mail : tscarabino@hotmail.com received : 10 september 2008 / accepted : 6 october 2008 / published online : 10 march 2009 springer - verlag 2009 abstract purpose . 
this study evaluated the sensitivity of a 3.0 - tesla ( t ) magnetic resonance imaging ( mri ) in measuring cerebral phenylalanine using proton magnetic resonance spectroscopy and in assessing mr - documented whitematter changes by means of diffusion studies ( diffusionweighted imaging , apparent diffusion coefficient map ; diffusion tensor imaging ) in patients with phenylketonuria . 
lampiezza del segnale della fenilalanina relativo al rapporto creatina / fosfocreatina incrementa linearmente con la fenilalanina ematica ( r = 0 , 7067 ; p < 0 , 001 )  . 
lo studio di diffusione ha 462 radiol med ( 2009 ) 114 : 461474 exhibiting mri changes as well as decreased apparent diffusion coefficient values , but fractional anisotropy indices were normal . 
in particular , the multimodal approach with mri , proton magnetic resonance spectroscopy and diffusion magnetic resonance imaging can provide more information than previous studies performed with low - field systems . 
in particolare lapproccio multimodale con imaging rm di base , di spettroscopia e di diffusione pu fornire maggiori informazioni rispetto ai precedenti studi acquisiti con sistemi a pi basso campo . keywords phenylketonuria magnetic resonance imaging ( mri ) proton mr spectroscopic imaging diffusion mri parole chiave fenilchetonuria risonanza magnetica studio di spettroscopia protonica con risonanza magnetica studio di diffusione con risonanza magnetica introduction introduzione phenylketonuria ( pku ) is a disorder of amino acid metabolism caused by an inborn error in the phenylalanine hydroxylase gene ( pha ) , which strongly reduces hepatic hydroxylation of phenylalanine ( phe ) to tyrosine [ 1 ]  . 
previous morphological mri studies have documented focal symmetrical lesions in periventricular and , especially , parieto - occipital white matter ( wm ) in pku patients with phe blood levels exceeding 10 mg / dl . these lesions , the significance of which is as yet unclear , seem to be due to a reversible structural myelin alteration , as they regress when blood phe levels fall [ 2 ]  . proton magnetic resonance spectroscopy ( 1h - mrs ) measures noninvasively the concentration of several brain metabolites in vivo and can help to further elucidate the cerebral metabolic characteristics of pku . 
it allows evaluation of several aspects of brain biochemistry that could shed light on the nature of wm lesions , including measurement of n - acetyl - containing moieties [ mainly n - acetylaspartate ( naa ) ] , choline - containing compounds ( cho ) , creatine ( cr ) and phosphocreatine ( pcr ) , and myo - inositol ( mi ) [ 3 ]  . 
in particular , changes in naa ( a marker of neuronal integrity ) la fenilchetonuria ( pku ) un disordine del metabolismo degli amminoacidi causata da una alterazione congenita del gene della fenilalanina - idrossilasi che determina una significativa riduzione , a livello epatico , della idrossilazione della fenilalanina ( phe ) in tirosina [ 1 ]  . 
i pazienti non diagnosticati e quindi non trattati possono sviluppare diversi segni e sintomi : in particolare ritardo mentale e nella crescita , crisi epilettiche , manifestazioni cutanee ( eczemi e ipopigmentazioni )  . 
la diagnosi neonatale ha radicalmente cambiato la prognosi della pku anche se in realt possiamo riscontrare alcuni sintomi e alterazioni neuro - radiologiche anche in pazienti trattati precocemente . la pku stata studiata sotto diversi aspetti . 
essa documenta la presenza di focali e simmetriche lesioni a livello della sostanza bianca periventricolare , specie a livello parieto - occipitale , evidenti in tutti i pazienti in cui il livello ematico di phe supera il valore di 10 mg / dl . 
tali lesioni , il cui significato non ancora chiaro , sembra siano dovute a una alterazione strutturale e reversibile della mielina : infatti esse regrediscono nel momento in cui il livello di phe decresce verso valori normali [ 2 ]  . la spettroscopia protonica con rm ( 1h - mrs ) misura in maniera non invasiva e in vivo la concentrazione a livello cerebrale di alcuni metaboliti fornendo ulteriori informazioni sulle caratteristiche metaboliche cerebrali della pku e soprattutto permettendo una pi chiara analisi biochimica delle alterazioni della sostanza bianca tipiche di questa radiol med ( 2009 ) 114 : 461474 or in mi ( a potential astrocytic marker ) suggest a possible neurochemical dysfunction , whereas cho is one measure of the degree of tissue myelination [ 4 , 5 ]  . 
despite continuing progress in 1h - mrs acquisition methods and the development of increasingly sophisticated quantification routines , its determination is affected by the detection threshold at 1.5 t ( > 200 mmol / kg ) [ 3 ]  . 
furthermore , the very large volume of interest ( voi ) applied at 1.5 t ( > 30 cc ) makes phe signal detection unreliable due both to concurrent line - broadening effects on the resonance and the presence of macromolecular contributions at 7.3 ppm [ 36 ]  . in recent years , diffusion - weighted mri ( dwi - mri ) has been introduced in clinical practice . 
however , these studies have failed to clarify the significance of dwi changes in relation to clinical findings . the aim of this work was to analyse the potential and advantages of a 3.0 - t system in the multimodal study of brain alterations of patients with pku . 
they were 17 male and 15 female subjects aged from 7 to 34 ( mean 18.9 , standard deviation 6.0 ) years , 21 with early and 11 with late diagnosis . 
in particolare andiamo a misurare la concentrazione di molecole contenenti il gruppo n - acetile ( in prevalenza ln - acetil - aspartato , naa ) , le macro - molecole contenenti colina ( cho ) , la creatina ( cr ) , la fosfocreatina ( pcr ) e il mio - inositolo ( mi ) [ 3 ]  . 
le variazioni di naa ( marker di integrit neuronale ) e di mi ( potenziale marker astrocitario ) suggeriscono una possibile disfunzione neurochimica mentre mediante la quantificazione della cho abbiamo un indice del grado della mielinizzazione tissutale [ 4 , 5 ]  . 
lo studio di 1h - mrs con unapparecchiatura a 1 , 5 tesla ( t ) ha permesso di quantificare i livelli cerebrali di phe in pazienti con pku : tali misurazioni hanno fornito dati interessanti sulla biochimica delle alterazioni della sostanza bianca in tale patologia [ 35 ]  . 
la valutazione dei livelli di phe , ottenuta utilizzando sistemi a 1 , 5 t , per ancora soggetta a delle limitazioni : nonostante i miglioramenti dei protocolli di acquisizione 1h - mrs e di quantificazione dei metaboliti c un limite intrinseco dovuto alla soglia di detezione del metabolita ( > 200 mmol / kg ) legato direttamente alla intensit del campo magnetico ( 1 , 5 t ) [ 3 ]  . 
inoltre la notevole ampiezza del volume di interesse ( voi ) in sistemi a 1 , 5 t ( > 30 cc ) rende il valore di phe non attendibile e ci dovuto sia a effetti concomitanti di allargamento sulla risonanza che allinterferenza delle altri componenti macromolecolari presenti a 7 , 3 ppm [ 36 ]  . negli ultimi anni sono state introdotte di routine nella pratica clinica le sequenze rm pesate in diffusione ( dwmri )  . 
 [ 8 ] hanno dimostrato in pazienti con pku la presenza di alterazioni di segnale in dwi che si sovrappongono sostanzialmente alle alterazioni rilevate in condizioni rm di base e che sono caratterizzate da iperintensit in t2 . 
le mappe del coefficiente di diffusione apparente ( adc ) invece documentano valori compatibili con una diffusione ristretta dei protoni . tali studi comunque non hanno ancora chiarito lorigine di tali alterazioni e una chiara correlazione col quadro clinico . lo scopo del nostro lavoro di analizzare le possibilit e i vantaggi della rm 3 , 0 t nello studio multimodale delle alterazioni cerebrali di pazienti con pku ed in particolare di valutare la sensibilit di un sistema rm ad alto campo nel misurare la phe cerebrale con la 1h - mrs e nel documentare le alterazioni della sostanza bianca rilevate con lo studio rm di base utilizzando gli studi di dw - mri . magnetic resonance technique materiali e metodi mr studies were performed with a 3.0 - t scanner ( signa horizon lx , general electric medical system , milwaukee , wi , usa ) with a standard quadrature transmit / receive birdcage head coil . 
wm involvement was assessed by morphological mr with sagittal fast spoiled gradient recalled ( fspgr ) t1 - weighted [ repetition time ( tr ) / echo time sono stati inclusi nello studio 32 pazienti con un tipico quadro biochimico - clinico della pku : 17 maschi e 15 femmine , et compresa tra 7 e 34 anni ( media 18 , 9 , deviazione standard 6 , 0 ) : 21 con diagnosi precoce e 11 con diagnosi tardiva di malattia . 
in tutti i pazienti stato valutato il valore ematico di phe ed stata effettuata una 464 radiol med ( 2009 ) 114 : 461474 ( te ) / flip angle ( fa ) 225 / minimum / 75 ms , acquisition time 1 min 57 s ] sequences ; axial fluid - attenuated inversion recovery ( flair ) ( tr / te / ti , inversion time , 11 , 000 / 130 / 2 , 250 ms , acquisition time 2 min 26 s ) and spin echo ( se ) t1 - weighted ( tr / te 500 / 10 ms , acquisition time 2 min 21 s ) sequences , and coronal fast spin echo ( fse ) t2weighted ( tr / te 5 , 000 / 55 / 20 ms , acquisition time 1 min 05 s ) sequences . 
standard mr scans were acquired using 5mm - thick slices , 1 - mm gap , matrix size 256192 , and field of view ( fov ) 22 cm . single - voxel 1h - mrs was performed using a short te point - resolved spectroscopy ( press ) sequence ( tr / te 2 , 000 / 35 ms , total averages 128 , spectral width 2 , 500 hz , 1 , 024 complex data points , acquisition time 4 min 56 s )  . 
a voxel volume of just 8 cc was placed in the altered periventricular deep wm . the diffusion studies [ dwi , adc maps and diffusion tensor imaging ( dti ) ] were performed in the axial plane using a pulsed gradient se echo - planar sequence ( tr / te 8 , 000 / minimum ms ; dwi acquisition time 44 s and for dti 6 min 57 s ) without ( b - value = 0 ) and with ( b - value = 1 , 000 s / mm2 ) diffusion gradients applied along 25 different directions to cover the three - dimensional space uniformly . 
 additional dwis were acquired in the axial plane , with identical parameters except for the b - value , which was set at values from 500 to 2 , 500 s / mm2 ( 500 , 1 , 000 , 1 , 500 , 2 , 000 and 2 , 500 ) for five different acquisitions . data analysis all postprocessing was performed on a unix workstation . wm changes were analysed on mri both qualitatively , with reference to signal intensity in the different pulse sequences , and semiquantitatively , with reference to their anatomical location ( frontal , temporal , occipital , cerebellar and in brainstem ) and extension ( deep and / or subcortical wm )  . 
wm involvement was scored on t2 - weighted images by raters who were unaware of patients clinical history , as follows : 1 for deep wm involvement only ( limited involvement ) ; 2 for involvement of deep and subcortical wm ( intermediate involvement ) ; 3 for greater involvement of brainstem and / or cerebellum ( severe involvement )  . 
 brain phe was quantified by computing the amplitude of the phe signal at 7.36 ppm relative to the cr / pcr peak at 3.05 ppm , considered as an internal reference , using the sage / idl software . 
the other metabolites ( naa , cho , cr / pcr , mi ) were analysed by means of lcmodel routines . the diffusion images were analysed assuming a monoexponential relation between signal intensity and the product of the b - matrix ( a 33 matrix expressing the relationship between signal attenuation and elements of the diffusion tensor matrix )  . 
trenta soggetti sani ( 9 maschi e 21 femmine ; et compresa tra 12 e 58 anni ; media 32 , 9 ) sono stati arruolati nello studio come gruppo di controllo per confrontare i dati ottenuti dallimaging rm . 
il consenso informato stato firmato da tutti i pazienti o da loro parenti prossimi . tecnica rm lo studio rm stato effettuato con unapparecchiatura rm 3 , 0 t ( signa horizon lx , general electric medical system , milwaukee , wi , usa ) dotata di bobina della testa standard in quadratura trasmittente / ricevente . 
le alterazioni della sostanza bianca sono state valutate con la rm di base utilizzando le sequenze : fast spoiled gradient recalled ( fspgr ) t1 - pesata ( tr , tempo di ripetizione , / te , tempo di echo , / fa , flip angle , 225 / minimum / 75 ms , tempo di acquisizione 1 min 57 s ) acquisita in proiezione sagittale ; fluid - attenuated inversion recovery ( flair ) ( tr / te / ti , tempo di inversione , 11000 / 130 / 2250 ms , tempo di acquisizione 2 min 26 s ) e spin echo ( se ) t1 - pesata ( tr / te 500 / 10 ms , tempo di acquisizione 2 min 21 s ) in proiezione sagittale ; fast spin echo ( fse ) t2 - pesata ( tr / te 5000 / 55 / 20 ms , tempo di acquisizione 1 min 05 s ) in proiezione coronale . 
il volume di interesse di 8 cc stato posizionato nelle aree di alterazione della sostanza bianca periventricolare profonda . lo studio in diffusione ( dwi , mappe adc e diffusion tensor imaging , dti ) stato ottenuto sul piano assiale utilizzando sequenze pulsed - gradient se eco - planari ( tr / te 8000 / minimum ms , tempo di acquisizione dwi 44 s e 6 min 57 s per il dti ) senza ( b - value = 0 ) e con gradienti di diffusione ( b - value = 1000 s / mm2 ) applicati lungo 25 direzioni per coprire uniformemente e tridimensionalmente il volume di interesse . ulteriori immagini pesate in diffusione sono state acquisite sul piano assiale con gli stessi parametri fatta eccezione per il b - value che stato impostato in valori variabili compresi tra 500 e 2500 s / mm2 ( 500 , 1000 , 1500 , 2000 e 2500 ) per un totale di cinque diverse acquisizioni . analisi dei dati la successiva elaborazione dei dati stata effettuata utilizzando una workstation unix . 
le alterazioni della sostanza bianca sono state analizzate sia qualitativamente , con riferimento alle variazioni di intensit di segnale nelle varie sequenze , che semi - quantitativamente considerando la loro radiol med ( 2009 ) 114 : 461474 tensor diagonalisation , of the main eigenvalues min , med , and max , were generated and the fractional anisotropy index ( fai ) , was derived from the eigenvalues for each pixel . 
 the analysis was performed on parieto - occipital wm , as all patients exhibited dwi changes in this region ; a spherical region of interest ( roi ) of uniform size ( ~45 mm2 ) was placed on the dwis and adc maps , and eigenvalues and fai values were then calculated . 
these data were confirmed by dti quantitative analysis , as decreased adc values but normal fai indices were found in the rois located on the hyperintense parieto - occipital wm ( table 1 )  . 
qualitative analysis of anisotropy images acquired with b - values > 1 , 000 s / mm2 showed an increased contrast between normal tissue and t2 / flair / dwi - mri hyperintense areas . 
il punteggio utilizzato stato calcolato come segue : 1 punto per lesioni interessanti solo la sostanza bianca profonda ( coinvolgimento limitato ) , 2 punti per lesioni interessanti anche la sostanza bianca sottocorticale ( coinvolgimento intermedio ) , 3 punti per leventuale coinvolgimento del tronco e / o del cervelletto ( coinvolgimento severo )  . il valore di phe cerebrale stato quantificato valutando lampiezza del picco di phe a 7 , 36 ppm in relazione al picco di cr / pcr a 3 , 05 ppm ( considerato come un valore interno costante e quindi di riferimento , usando il software sage / idl )  . 
gli altri metaboliti ( naa , cho , cr / pcr e mi ) sono stati analizzati utilizzando lcmodel software . le immagini in diffusione sono state analizzate utilizzando una relazione mono - esponenziale tra lintensit di segnale e il segnale prodotto della matrice b ( matrice 33 che esprime la relazione tra lattenuazione di segnale e gli elementi della matrice del tensore di diffusione )  . 
 lanalisi stata effettuata sulla sostanza bianca parietooccipitale poich tutti i pazienti presentavano alterazioni di segnale in dwi in questa regione ; una regione di interesse ( roi ) sferica e di misura uniforme ( ~45 mm2 ) stata posizionata sulle immagini pesate in diffusione , quindi mappe di adc , autovalori e valori di fai sono stati calcolati . 
the advantages of a higher mr field , with respect to the low - field system used to date , is a larger diagnostic ability in the management of patients with this pathology . 
resolution quality tends to be privileged in clinical practice , with acquisition of a larger number of slices of reduced thickness , use of smaller fov and broader matrices , and acquisition times similar to those of 1.5 - t ai soggetti normali . 
questi dati sono stati confermati dalla analisi quantitativa del dti : nelle regioni di interesse localizzate nelle aree iperintense della sostanza bianca parieto - occipitale stato trovato un valore di adc ridotto ma un normale valore di fai ( tabella 1 )  . 
lanalisi qualitativa delle immagini dellanisotropia , acquisite con b - value pi elevato di 1000 s / mm2 , mostra un aumento del contrasto tra il tessuto normale e le aree di iperintensit in t2 / flair / dw - mri . 
2a - e proton magnetic resonance spectroscopy allows detection of an abnormal phenylalanine ( phe ) signal at 7.36 pp values of the main metabolites [ n - acetylaspartate ( naa ) , choline - containing compounds ( cho ) , creatine ( cr ) / phosphocreatine ( pcr ) ] were normal ( a , arrow )  . 
all patients exhibit variable white - matter hyperintensities on t2 ( c ) and fast low - angle inversion recovery ( flair ) ( d ) scans , mainly in temporal , occipital and periatrial regions . 
in our work , instead , we found the optimum acquisition time as a tradeoff between a time - consuming multimodal acquisition and the patients comfort during the exafurther technological advances are expected to overcome some minor limitations of this system , such as field discussione in tale studio nei pazienti con pku si confermano i dati dei precedenti studi circa la frequenza e le caratteristiche delle alterazioni della sostanza bianca e le correlazioni tra il radiol med ( 2009 ) 114 : 461474 fig . 
a questo valore il confronto dellintensit di segnale sullasse x ( a ) e y ( b ) permette di rilevare una sottile variazione di segnale nella sostanza bianca alterata in relazione ad una parziale conservata anisotropia ( freccia gialla )  . inhomogeneity , susceptibility and chemical - shift artefacts , high specific absorption rate ( sar ) and acoustic noise . in detail , the use of higher fields for spectroscopy allows reduced acquisition time ( higher s / r ) and improved spectral resolution [ 18 , 19 ]  . 
as a result of such improvements ( increased snr and greater spectral resolution compared with 1.5 - t studies ) , the phe signal was easily detected and was measurable despite the low phe concentrations . 
the relative amplitude of the phe signal increased linearly with blood phe up to 1 , 200 micromoles , where growing dispersion of brain phe values was noted , suggesting a more marked interindividual variability , probably due to saturation of the specific phe transport system at the level of the bloodbrain barrier ( bbb )  . a short te ( 35 ms ) was applied better to detect the phe signal as well as those of the principal metabolites . 
furthermore , spectroscopic studies with longer te are subject to greater snr loss at 3.0 t than at 1.5 t due to t2 reduction at higher field strengths and increased peak line width in relation to reduced t2 and microscopic and macroscopic body inhomogeneities . 
these features allow an increased b - value to enhance the anisotropic effect , thus improving the quality of more complex examinations such as fai , diffusion tensor and tractography , which are poorly displayed on 1.5 - t images , even with multiple grado di severit e parametri clinici e laboratoristici . 
per ottenere maggiori informazioni sulla patogenesi di tali alterazioni abbiamo condotto con apparecchiatura a 3 , 0 t uno studio rm multimodale che ha compreso nel protocollo uno studio di base , di spettroscopia e di diffusione al fine di migliorare , sfruttando i vantaggi derivanti dalluso dellalto campo rispetto a quello dei tradizionali sistemi a 1 , 5 t , la capacit diagnostica che pu risultare utile nel management di tali pazienti [ 1517 ]  . in generale lintroduzione di magneti ad alto campo ha infatti portato dei benefici in campo neuroradiologico . 
il confronto delle immagini acquisite con sistemi a 3 , 0 t rispetto a quelle ottenute con 1 , 5 t ha mostrato degli indubbi vantaggi quali : aumento della risoluzione spaziale , temporale e di contrasto , intensit di segnale pi elevato , ridotto tempo di acquisizione , maggiori e pi avanzate applicazioni , elevata sensibilit ed eccellente potere diagnostico nelle sequenze con mezzo di contrasto . 
 il neuroradiologo quindi , grazie allalto s / r dellalto campo , utilizzando lo stesso tempo di un esame con sistemi a 1 , 5 t , pu ottenere immagini di qualit superiore ( aumentando la matrice o riducendo lo spessore di strato o il fov ) oppure immagini della stessa qualit di un basso campo ma in un tempo ridotto : ci si traduce in un maggior confort per il paziente e in una riduzione degli artefatti da movimento . 
la qualit della risoluzione tende ad essere privilegiata nella pratica clinica , grazie allacquisizione di un maggior numero di slices con uno spessore di strato ridotto tramite lutilizzo di un fov pi piccolo , di matrici pi ampie con un tempo di acquisizione risultante simile a quello speso se si utilizzano scanner a 1 , 5 t . 
4a , b comparison of proton magnetic resonance spectroscopy brain phenylalanine ( phe ) detection at 1.5 t ( a ) and 3.0 t ( b ) at 7.36 ppdetection of phe signal in the 1.5 - t study requires a 32 - cc volume of interest ( voi )  . 
4a , b confronto della fenilalanina cerebrale rilevata con la spettroscopia protonica a 1 , 5 t ( a ) e 3 , 0 t ( b ) a 7 , 36 ppla documentazione del segnale della fenilalanina a 1 , 5 t necessita di un voi di 32 cc . 
luso di un pi piccolo voi ( 8 cc ) riduce gli effetti da sovrapposizione con altri metaboliti quali istidina , omocarnosina , macromolecole presenti a 7 , 3 ppm . radiol med ( 2009 ) 114 : 461474 quale compromesso tra il tempo necessario per uno studio multimodale e che garantisse un adeguato confort per il paziente durante lesame . nello specifico in spettroscopia luso dellalto campo permette di ridurre i tempi di acquisizione ( in virt del pi alto s / r ) ma anche migliora la risoluzione spettrale [ 18 , 19 ] la maggior ampiezza del chemical shift dei metaboliti in esame permette infatti di avere una migliore risoluzione spettrale che si traduce in una pi definita separazione dei picchi adiacenti che invece con un sistema a pi basso campo andrebbero a sovrapporsi . 
in virt di tali miglioramenti ( aumento del s / r e migliore risoluzione spettrale ) possibile individuare e misurare pi facilmente il picco della phe , persino a basse concentrazioni . 
lampiezza relativa del picco di phe aumenta linearmente con la concentrazione ematica della stessa sino a un valore di 1200 micromoli oltre il quale si osserva una dispersione dei valori cerebrali di phe dovuta probabilmente a una variabilit individuale derivante dalla saturazione dei sistemi di trasporto della phe localizzati a livello della barriera emato - encefalica ( bee )  . stato utilizzato un te ridotto ( 35 ms ) per avere una migliore individuazione del segnale ( picco ) della phe e degli altri principali metaboliti in esame . 
utilizzando un te pi lungo si avrebbe una riduzione del rapporto s / r pi marcata con lutilizzo di sistemi a 3 , 0 t che con quelli a 1 , 5 t , per effetto della riduzione del segnale in t2 che si ha ad alto campo , dellaumento dellampiezza della linewidth causata dalla riduzione del segnale sempre in t2 e per le disomogeneit a livello microa macro - scopico . anche limaging pesato in diffusione beneficia dellaumento del rapporto s / r , della risoluzione spaziale e della accuratezza delle immagini [ 1517 ]  . 
si verifica in tal modo un miglioramento della qualit di alcune misurazioni come la fractional anisotropy ( fai ) , il tensore di diffusione ( dti ) e di alcune tecniche di ricostruzione come la trattografia . questi valori non sono ben rappresentati a causa del basso s / r utilizzando un sistema a 1 , 5 t anche se si dovesse aumentare il numero delle eccitazioni . 
infatti le ricostruzioni dei tratti assonali riflettono con maggior accuratezza la realt anatomica , specialmente a livello delle biforcazioni dei fasci . radiol med ( 2009 ) 114 : 461474 excitations , owing to the low snr . 
in fact , the reconstructed dti trajectories reflect more accurately the underlying axonal fibres , particularly crossing or bifurcating bundles . for some years , it has been possible to reconstruct threedimensional pathways of wm tracts by combining anisotropy characteristics and directionality , applying the technique known as fibre tracking or tractography . 
the method allows reconstruction of continuous fibre trajectories by sequentially piecing together discrete and shortly spaced estimates of fibre orientation to form continuous fibre trajectories [ 2022 ]  . the colour map is an easy method to show dti values , as it displays the main direction of wm fibres in three fundamental colours : green , blue and red . 
in particular , ontogenetically older fibre systems , such as the optic radiation , had a normal appearance . wm changes depicted in pku patients do not therefore necessarily reflect an altered organisation of cerebral myelin pathways detectable on dti . 
some mr findings in pku appear to be more consistent with reversible dysmyelination associated with an increased myelin turnover than with a demyelination process [ 2 , 15 , 25 , 26 , 29 , 30 ]  . our latest report of decreased adc values with preserved anisotropic diffusivity on dwi - mri and abnormal elevation of brain phe levels on 1h - mrs [ 31 ] seems to be in line with the hypothesis of water accumulation in myelin sheaths [ 7 ] due to an abnormally increased myelin turnover with consequent preservation of anisotropy , which can occur only in structures whose microscopic barriers have not been either destroyed or partially vacuolated . however , a third hypothesis consistent with these findings is that of intracellular accumulation of a hydrophilic metabolite produced by the phe hydroxylase defect , leading da alcuni anni possibile effettuare una ricostruzione tridimensionale del decorso delle fibre mieliniche . 
utilizzando le caratteristiche di anisotropia e tecniche note come il fiber tracking o trattografia si ricostruisce la direzione delle fibre nervose interpolando in modo sequenziale , stime discrete e poco spaziate dellorientamento della fibra per ottenere la sua traiettoria continua [ 2022 ]  . 
 ne derivano mappe a colori che costituiscono un metodo semplice per mostrare i valori del tensore di diffusione attraverso la visualizzazione delle principali direzioni delle fibre nervose in tre diversi colori ( grigio , blu e rosso )  . lapplicazione di tale tecnica nei pazienti con pku ci consente di poter valutare lintegrit delle fibre nervose nelle aree caratterizzate da riduzione dei valori di adc . 
al momento attuale il principale problema nella tecnica del fiber tracking e nella rappresentazione delle mappe a colori dovuto alla difficolt di ottenere una buona delineazione delle fibre mieliniche , senza una parziale contaminazione da parte dei tratti nervosi adiacenti [ 24 ]  . lanalisi del dti ha mostrato una riduzione dei valori di adc nelle aree iperintense nellimaging di base , in linea con i precedenti lavori in letteratura [ 7 , 8 ]  . 
in particolare le fibre ontogeneticamente pi vecchie come i tratti ottici appaiono normali . le alterazioni della sostanza bianca , viste nella pku , non necessariamente riflettono una alterazione architetturale del decorso delle fibre mieliniche , valutato con dti . 
le alterazioni della sostanza bianca nei pazienti con pku sono state documentate in molti studi effettuati con sistemi rm a pi basso campo , ma il loro significato non ancora stato chiarito [ 315 , 2528 ]  . 
alcuni pattern rm sembrano essere correlati pi con un reversibile processo di dismielinizzazione che con uno di demielinizzazione [ 2 , 15 , 25 , 26 , 29 , 30 ]  . in un precedente nostro lavoro la riduzione dei valori di adc con una preservazione dei valori di fa in diffusione e lanormale incremento dei livelli di phe cerebrale in spettroscopia protonica [ 31 ] potrebbero suggerire un accumulo di acqua nelle guaine mieliniche [ 7 ] dovuto a un incremento anomalo del turn - over mielinico stesso che si ha in strutture in cui le barriere microscopiche non sono state ancora del tutto degradate o vacuolizzate . 
 una terza ipotesi in linea con le nostre valutazioni che laccumulo di una metabolita idrofilico intracelllulare prodotto dalla phe - idrossilasi porta a un aumento del contenuto di acqua intracellulare . 
5a - d imaging di diffusione : mappa di adc ( a ) con selezione di una roi , mappa di fai ( b ) e a colori ( c ) ; i valori delle roi di adc e fa ( d ) misurati nelle aree di ciascun paziente ( punti ) e in range normali ( barra : meansd )  . to increased intracellular water content [ 31 ]  . 
the latter data require further examination given that no other abnormalities were detected by in vivo mrs examination , apart from the phe increase . pattern di dwi sia le anormalit dei valori ottenuti con la spettroscopia ( accumulo di phe con valori normali degli altri metaboliti )  . 
questi ultimi dati richiedono ulteriori studi dato che nessuna altra anomalia stata rilevata nellesame di spettroscopia in vivo a parte lincremento della phe . conclusions conclusioni the higher snr of high - field mr systems is a resource that neuroradiologists must exploit in clinical practice , as the higher the snr , the more the imaging protocols can be adjusted . 
i sistemi a 3 , 0 t permettono infatti di effettuare oltre a un accurato studio di base , anche delle valutazioni di carattere fisiologico , metabolico e funzionale che consentono di aumentare la sensibilit e la specificit del potere diagnostico della rm . sono comunque necessari ulteriori progressi tecnologici che permettano di superare alcune piccole limitazioni di tali sistemi rm come la disomogeneit del campo magnetico , radiol med ( 2009 ) 114 : 461474 inhomogeneity , susceptibility and chemical - shift artefacts , high sar and acoustic noise . the growing diffusion of high - field mr systems over the next few years will help a clearer understanding of the pathogenic role of signal abnormalities of the cerebral parenchyma in patients having several kinds of neurological diseases , such as pku . 
in addition , measurement of brain phe levels with 1h - mrs and dwi - mr parameters could become the technique of choice to monitor the influx of blood phe into brain tissue , especially during therapy in follow - up studies . gli artefatti da suscettibilit magnetica e da chemical shift , lelevato sar ( specific absorption rate ) e lalto rumore acustico . la crescente diffusione di tali sistemi nei prossimi anni permetter una migliore comprensione delle cause di alterazione del segnale in pazienti con patologie come la pku . 
guerci , radiologia padiglione barbieri , ospedale maggiore di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703660 , fax : + 39 - 052 - 1986352 , e - mail : leonardo.guerci@libero.it received : 12 august 2008 / accepted : 16 september 2008 / published online : 12 march 2009 springer - verlag 2009 abstract two women with profoundly different backgrounds were brought together in a destiny that saw their paths cross and join in the discovery of radioactivity : marie curie and blanche wittman . 
the discovery of radioactivity was the common denominator underlying the vicissitudes of their lives , the same radioactivity that was so acclaimed and of such incredible diagnostic and therapeutic potential while at the same time so underrated in the everyday life of the time that disregarded , almost disparagingly , the deleterious biologic effects it was capable of provoking . 
at the beginning of the twentieth century , those effects were in fact often underestimated or scarcely considered , and it was only after world war ii that there came an awareness of the ambiguous properties of ionising radiation . 
after numerous studies on radiation exposure , much of the current debate concerns the possible effects of exposure to small doses , such as those delivered in most radiological examinations . 
the theories proposed include the unorthodox theory of hormesis , which requires careful riassunto due donne , due storie profondamente diverse , unite da un destino che le incrocia e le unisce nella scoperta della radioattivit : marie curie e blanche wittman . 
la prima , una delle pi grandi donne e scienziate di tutti i tempi , unica nella storia ad aver vinto due premi nobel per la scienza , dotata di uno spirito umanitario fuori dal comune , dedic , nonostante lo scandalo sentimentale che la vide al centro della cronaca , la maggior parte della sua vita alla ricerca scientifica . 
la seconda , passata alla storia come la regina delle isteriche durante il suo ricovero nel famigerato manicomio della piti salpetrire di parigi , divenne alla sua guarigione una delle pi strette collaboratrici di m.me curie nellestrazione del radium dai fanghi della boemia , per ben 16 anni di duro lavoro , fino al momento della sua morte . 
ed proprio la scoperta della radioattivit il comun denominatore che sta alla base delle loro vicende umane , quella stessa radioattivit cos celebrata e dalle incredibili potenzialit diagnostiche e terapeutiche , ma allo stesso tempo cos svilita nella quotidianit della vita di quel tempo , che ignorava , talora quasi a sprezzo , gli effetti nocivi biologici in grado di provocare . 
nei primi anni del 900 tali effetti furono infatti spesso sottovalutati o scarsamente considerati , e fu solo dal secondo dopoguerra in poi che si manifest una forte presa di coscienza sulle ambigue propriet delle radiazioni ionizzanti . 
dopo numerosi studi condotti sullesposizione alle radiazioni ionizzanti , ci di cui molto si discute oggi riguarda principalmente i possibili effetti provocati dallesposizione a piccole dosi , come quelle erogate nella 348 radiol med ( 2009 ) 114 : 347357 reevaluation . 
much light has been shed on radiology since the time of blanche and marie , but there still remain many shadows to dispel , and this can only be done by serious and constant scientific commitment . keywords curie wittman ionizing radiation biological risk radiobiology maggior parte degli esami radiologici : tre le teorie proposte , una delle quali ( quella eretica della ormesi ) richiede di essere rivalutata con maggiore attenzione . molte luci si sono accese dai tempi della radiologia di blanche e marie , tuttavia al giorno doggi rimangono da chiarire ancora molte ombre , che solo un serio e costante impegno scientifico potr dissipare in futuro . parole chiave curie wittman radiazioni ionizzanti rischio biologico radiobiologia introduction introduzione a few years ago , the swedish writer p.o. 
enquist [ 1 ] wrote a charming book about two very different women brought together by the vagaries of life to work side by side and share hardships , danger and emotions linked with the early study of radioactivity : marie curie and blanche wittman . the clearly fictionalised vicissitudes narrated by enquist were the starting point for research that led us to analyse several aspects of the history of radiology . qualche anno fa , lo scrittore svedese p.o. 
enquist [ 1 ] ha dedicato un bel libro alla storia di due donne , molto diverse tra loro ma che i casi della vita hanno portato a lavorare fianco a fianco e a condividere fatiche , pericoli ed emozioni legate ai primi studi sulla radioattivit : marie curie e blanche wittman . 
a few days before she was awarded the prize in stockholm , a scandal over her affair with another famous physicist , paul langevin ( 18721946 ) broke out in paris . 
 this event was considered of such importance that the marie curie marie sklodowska , nata a varsavia , in polonia , nel 1867 , era figlia di un libero pensatore e di una cattolica praticante . 
pochi giorni prima della consegna del secondo nobel a stoccolma , a parigi scoppi lo scandalo per la relazione che la ancor giovane vedova aveva iniziato con un altro fisico famoso , paul langevin ( 18721946 )  . 
 radiol med ( 2009 ) 114 : 347357 questo evento ebbe una rilevanza tale che il fisico svante arrhenius , membro del comitato per il nobel , giunse a consigliare a marie di rifiutare il premio . 
lei stessa e la figlia irne ( allora diciassettenne ) , impararono a guidare questi automezzi , studiarono anatomia e , in compagnia di personale medico , prestarono a lungo la propria opera in zona di guerra . madre e figlia si sottoposero cos a forti dosi di raggi x senza alcuna protezione . 
negli stessi anni , marie fond un servizio di radioterapia militare , isolando personalmente il gas radioattivo ( radon ) in tubi di vetro che venivano spediti a diversi ospedali francesi . 
marie vers anche alla patria acquisita la maggior parte delle somme ricevute dalla fondazione nobel [ 3 ]  . dopo la fine della guerra , negli anni dal 1919 al 1934 , marie ormai una celebrit mondiale viaggi molto , recandosi anche pi volte negli stati uniti , dove incontr i presidenti harding e hoover , lanci raccolte di fondi per la ricerca e ottenne notevoli finanziamenti , nonostante la timidezza le impedisse di parlare in pubblico con facilit . 
during her stay in england , marie , deeply shocked by the parisian scandal , came into contact with the movement for womens suffrage , the leading member of which was emmeline pankhurst ( 18581928 ) , who was arrested on several occasions . back in paris after a break of 14 months , marie returned to her laboratory , as the scandal began to die down with the separation by mutual agreement of the langevins . 
marie and paul did not resume their affair , although their relationship remained friendly and fruitful on the professional level . at the outbreak of world war i , only two people remained on the premises of the radium institute , which was planned by marie and built in the latin quarter in the street renamed for the occasion in honour of pierre curie : marie , and a mechanic who was exempt from the draft due to a serious heart condition . although until then , maries main interest had been the radioactive phenomena , she realised the enormous diagnostic potential of artificial x - rays ( roentgen rays ) in saving the lives of wounded soldiers at the front . 
she set up 350 radiol med ( 2009 ) 114 : 347357 marie curie cominci a soffrire di disturbi fisici connessi alle radiazioni intorno al 1920 , con una doppia cataratta che richiese quattro dolorosi e , per lepoca , complicati interventi . 
negli ultimi anni , manifest una progressiva debolezza , dapprima attribuita erroneamente alla tubercolosi , finch uno specialista di ginevra cap che poteva trattarsi di una forma simil - tumorale di anemia aplastica , dovuta al danno midollare da radiazioni [ 4 ]  . quando mor , nel 1934 , 28 anni dopo il marito pierre , listituto da lei diretto era una delle massime realt scientifiche del tempo e molte applicazioni mediche e industriali delle scoperte dei curie testimoniavano gi delle vaste potenzialit applicative della radioattivit . 
negli anni compresi tra il 1919 ed il 1934 , listituto diretto da marie curie produsse 483 lavori scientifici o libri , 31 dei quali scritti da marie [ 3 ]  . marie venne sepolta due volte ; la prima a sceaux , con il marito pierre . 
il castello , in quegli anni , attirava la curiosit morbosa di frotte di visitatori , da sarah bernhardt ad axel munte , a numerosi giovani studiosi di neuropsichiatria , da broca a gilles de la tourette , al giovane freud . 
in sostanza , alla fine dell800 , non molto era cambiato nella vita degli internati da quando , un secolo prima , il castello era diretto dall illuminista dottor pinel , il quale aveva tentato con scarso successo , nel 1795 , loperazione insieme politica ed umanitaria di liberare i folli dalle catene . 
foucault ha scritto , a proposito del tentativo di pinel : le catene cadono , il folle si ritrova libero e in quel momento recupera la ragione la brutalit che appare nei dementi non che il riflesso della bestialit dei guardiani e ancora : a partire da pinel si vedr nella follia uno slancio venuto dal profondo , che oltrepassa i limiti dellindividuo e tende ad una apoteosi di se stesso [ 5 ]  . blanche , ricoverata dal 1878 al 1893 , divenne presto famosa come la regina delle isteriche , protagonista delle esibizioni organizzate e dirette settimanalmente dal dottor fig . 
marie and her daughter , irne ( aged 17 at the time ) , learned how to drive these vehicles , studied anatomy and , in the company of medical personnel , gave long - term service in the war zone . 
during the same period , marie established a military radiotherapy service and personally isolated the radioactive gas ( radon ) in glass tubes that were sent to various french hospitals . 
she also donated most of the money received from the nobel foundation to her adopted homeland [ 3 ]  . after the war , in the years between 1919 and 1934 , marie , who had become an international celebrity , travelled widely . 
the frail figure of this now elderly woman dressed constantly in black became legendary , and due to her austere appearance and moral force , marie was compared with a buddhist monk . launched very successful marie began to suffer from physical problems connected with radiation around 1920 , with the appearance of a double cataract that required four painful and for the times complicated operations . 
in her later years , she developed progressive weakness , which was at first erroneously attributed to tuberculosis until a specialist from geneva realised it could have been caused by aplastic anaemia , a tumour - like condition due to radiation - induced bone marrow damage [ 4 ]  . between 1919 and 1934 , the institute directed by marie produced 483 scientific papers or books , 31 of which were written by her [ 3 ]  . 
in those years , the piti salptrire attracted the morbid curiosity of a stream of visitors , from sarah bernhardt to axel munte and numerous neuropsychiatrists , from paul broca to georges gilles de la tourette and the young sigmund freud . 
in essence , at the end of the nineteenth century , little had changed in the lives of the patients from when a century earlier the hospital was directed by the enlightened physician philippe pinel , who , in 1795 , had attempted without success to perform the political and humanitarian task of freeing the inmates from their shackles . 
and at that moment they recovered their reasonthe brutality which appears in the demented is nought else than the reflection of the animality of the guardians and from pinel onwards , the classical mind recognised in madness an impulse from the depths which exceeded the juridical limits of the individual , ignoring fixed moral limits and tending towards an apotheosis of the self [ 5 ]  . blanche , who was hospitalised between 1879 and 1893 , soon became famous as the queen of hysterics , being the protagonist of the spectacular weekly lectures organised and directed by jean - martin charcot . 
the cures without support became real cures of false diseases , as in fact hysteria proved to be , which failed to outlive charcot . hysterical madness was a mixture of persuasion and mystification , even though , many years later , blanche stated that charcots weekly performances were not based on feigning . although charcot has been accused , and probably correctly , of misogyny [ 6 ] , in 1885 , he accepted into his group a brilliant young medical graduate , blanche edwards [ 7 ]  . after the death of charcot , blanche wittman , having been declared clinically cured , found temporary work as a technical assistant in the recently instituted radiology department of salptrire . 
indeed , roentgens discovery ( 1895 ) was made only 2 years after the death of charcot and was contemporary to freuds studies of hysteria . in 1898 , at the time of the dreyfus affair , blanche moved to the laboratory of the curies , with the thankless task of isolating radium from the pitchblende from sankt joachimsthal in bohemia and in which she remained for hours and hours each day immersed up to her knees in pitchblende . this was the beginning of the collaboration and cohabitation of blanche and marie , which lasted 16 years . 
after 4 years of work , the curies , with the help of several assistants , including blanche , managed to isolate 0.1 g of radium from tonnes of pitchblende . the lesions caused by the radioactive pitchblende caused blanche to have first her legs and then her left arm amputated . 
reduced virtually to a torso and forced to move about in a wooden cart , blanche had to stop working in the laboratory but remained until her death , in 1913 , within the curies family circle and their closest friends and collaborators , such as becquerel [ 8 ]  . ha potuto compiersi se non con la complicit del malato stesso . 
la follia isterica era un insieme di persuasione e di mistificazione anche se , parecchi anni dopo , blanche ebbe a dichiarare che gli spettacoli settimanali di charcot non erano basati sulla simulazione . 
nonostante charcot sia stato accusato , probabilmente con ragione , di misoginia [ 6 ] , nella sua quipe egli accett anche , nel 1885 , una giovane e brillante laureata in medicina , blanche edwards [ 7 ]  . 
 nel 1898 , allepoca dellaffare dreyfus , blanche si trasfer nel laboratorio dei coniugi curie , con lingrato compito di isolare il radium dai fanghi della pechblenda provenienti dalle cave di sankt joachimsthal in boemia e nei quali restava immersa fino alle ginocchia per ore ed ore , ogni giorno . 
da una tonnellata di fanghi e terriccio , dopo quattro anni di duro lavoro , i curie , con laiuto di alcuni aiutanti , tra cui blanche wittman , riuscirono ad isolare 0 , 1 grammi di radiu le lesioni provocate dai fanghi radioattivi portarono la povera blanche a subire progressivamente lamputazione delle gambe e del braccio sinistro . 
ridotta ad un torso e costretta a spostarsi su un carretto di legno , blanche cess ovviamente di lavorare nel laboratorio , ma rest fino alla morte , avvenuta nel 1913 , nella cerchia familiare dei curie e dei loro pi stretti amici e collaboratori , come il grande fisico henri becquerel [ 8 ]  . popularity and demonisation of ionising radiation at the beginning of the twentieth century , artificially produced x - rays and , to a lesser extent , the radiation emitted by newly discovered radioactive elements , had become quite fashionable . 
this popularity can be seen not only in the press of the time [ 9 ] but also in the numerous handmade articles and industrial products whose labels referred to the mysterious rays for publicity purposes , such as household products , detergents , postcards , razors , citrus squeezers , prophylactics , soap , spirits and a variety of other items [ 10 ]  . 
questa popolarit testimoniata , oltre che dalla stampa dellepoca [ 9 ] , anche da numerosi reperti , manufatti o prodotti industriali , che nelletichetta richiamavano i raggi misteriosi a scopo pubblicitario , come prodotti per la casa , detergenti , cartoline , rasoi , spremiagrumi , profilattici , sapone , alcolici ed apparecchi di ogni tipo [ 10 ]  . 
at circuses and trade fairs , as well as elegant salons , x - ray demonstrations were performed , mainly for the macabre fancy of observing the skeleton of friends and relatives in the penumbra of the fluoroscopic screen , illuminated by a weak green glow . 
to have her hand x - rayed , as roentgens wife berta had done several years earlier , the celebrated actress sarah bernhardt remained motionless on her knees for 5 min in a fashionable parisian salon [ 4 ]  . the new rays captured the imagination of the public , more so than the cinmotagraphe invented by the lumire brothers , auguste and louis , in the same year as roentgens discovery , for they embodied the guarantee of a better future , in a positivist vision of the world characterised by endless faith in progress . 
photographs of the time bear witness to the very slow growth in the awareness of the ambiguous properties of radiation , which can be a powerful weapon against disease in both diagnosis and treatment but also highly pathogenetic and therefore should be dominated and controlled , rather than used indiscriminately . 
nei circhi e nelle fiere di paese , come nei salotti eleganti , venivano eseguite dimostrazioni dei raggi x , principalmente per il gusto un po macabro di osservare lo scheletro di amici e parenti nella penombra dello schermo fluoroscopico , illuminata da una debole luminescenza verdastra . 
per farsi radiografare la mano , come aveva fatto pochi anni prima la moglie di roentgen , berta , la grande attrice sarah berhardt rimase immobile in ginocchio per 5 minuti in un salon parigino alla moda [ 4 ]  . i nuovi raggi catturavano limmaginazione del pubblico con grande intensit , pi dellinvenzione del cinematografo , che i fratelli lumire realizzarono nello stesso anno della scoperta di roentgen e rappresentavano la garanzia per un futuro migliore , in una visione del mondo ancora positivista , caratterizzata da grande fiducia nel progresso . liconografia del tempo testimonia di una presa di coscienza collettiva molto lenta delle ambigue propriet delle radiazioni , che possono costituire unarma potente contro le malattie nella diagnosi e nella terapia , ma anche risultare altamente patogene e dunque devono essere dominate e controllate , piuttosto che utilizzate indiscriminatamente . 
la invisibilit delle radiazioni portava ad una sottovalutazione degli effetti biologici . quando , un anno dopo la scoperta di roentgen , 354 radiol med ( 2009 ) 114 : 347357 could have ( unpredictable ) effects on the body . 
in 1903 , the first rudimentary forms of lead or leadrubber shields appeared , but they were seldom used , as their rigidity hampered free movement . the radiologists of the time performed hours of radioscopy every day without any protection whatsoever , and after several years of work , they developed paleness , weakening and severe asthenia . 
in 1925 , she was part of a commission of the french academy of medicine , which recommended the use of lead screens and periodic blood tests in subjects exposed to radiation in the workplace . 
hair and fingernails tended to fall out and not grow back . a list of radiation victims compiled in hamburg in 1936 and clearly incomplete bore the names of 220 physicians , physicists , chemists , technicians , nurses and religious workers . 
gendreau described the first case of occupational disease associated with radiation [ 4 ]  . workers in a watch factory established in 1914 ( radium corporation , newark , nj , usa ) used fine brushes to spread radioactive material ( known as glow in the dark ) on the watch faces to render them fluorescent in the dark . many of these watches were supplied to troops on the european fronts during world war i . 
the workers in the factory , who tended to moisten the brushes on their tongues , suffered severe ulcerations , jaw necrosis , tooth loss and various types of tumours . 
in 1929 , legal action was taken against the company , which defended itself by attributing the workers illnesses to symptoms of hysteria . the use of radiation for diagnostic and therapeutic purposes , particularly in the fight against cancer , was actively promoted as early as the latter phase of maries life after world war i . 
the biological effects of radiation became effectively controlled , and devices capable of delivering very low doses were developed without sacrificing diagnostic accuracy ( such as those quipped with image intensifiers and television chains )  . 
this growing sullamerican journal of the medical association , comparve il primo articolo sulle applicazioni mediche dei raggi x , il direttore della rivista ipotizz che la forma di energia appena scoperta potesse esercitare effetti ( imprevedibili ) sullorganismo ma , a parte il grande clinico inglese lister , nessuno raccolse queste osservazioni [ 4 ]  . 
nel 1903 comparvero le prime , rudimentali protezioni in piombo o in gomma piombifera ma pochi le utilizzarono , perch la loro rigidit ostacolava i movimenti . i radiologi praticavano ore di radioscopia ogni giorno , senza alcuna protezione e , dopo pochi anni di lavoro , accusavano pallore , deperimento e grave astenia . 
tiraboschi , da 15 anni in attivit come radiologo presso lospedale cittadino . lautopsia dimostr gravi lesioni a carico del midollo osseo e della milza ed il patologo ipotizz un ruolo eziologico delle radiazioni . 
nel 1925 marie fece parte di una commissione dellaccademia francese di medicina , che raccomand luso di schermi protettivi piombati e di test periodici del sangue in soggetti esposti professionalmente . 
i capelli e le unghie cadevano , per non ricrescere pi . una lista di vittime delle radiazioni , compilata ad amburgo nel 1936 e chiaramente incompleta , riporta 220 nomi di medici , fisici , chimici , tecnici , infermieri e religiosi . gendreau descrisse il primo caso di patologia lavorativa industriale legata alle radiazioni [ 4 ]  . 
 le operaie di una fabbrica di orologi fondata nel 1914 ( radium corporation , newark , new jersey ) utilizzavano sottili pennelli per spalmare materiale radioattivo ( detto : glow in the dark ) sui quadranti , allo scopo di renderli fluorescenti e consentire di leggere lora al buio . 
nel 29 venne istruito un processo e la ditta si difese attribuendo i disturbi delle operaie a sintomi isterici . limpiego delle radiazioni a scopo diagnostico e terapeutico , specie nella lotta contro i tumori , venne promosso attivamente gi nellultima fase della vita di marie curie , nel primo dopoguerra , ma solo nel secondo dopoguerra le conoscenze di radiobiologia raggiunsero un livello soddisfacente ; il controllo degli effetti biologici delle radiazioni divenne efficace e furono proposte apparecchiature in grado di erogare dosi molto basse , senza sacrificare radiol med ( 2009 ) 114 : 347357 awareness was certainly encouraged by the devastating effects of the atomic bombs dropped on hiroshima and nagasaki in japan in 1945 . 
it has been estimated that to obtain the same quantity of ( gamma ) radiation unleashed by the hiroshima bomb alone , millions of tonnes of the curies radium would be required . 
the nuclear proliferation in the cold war years and the chernobyl nuclear disaster in russia further contributed to the growing alarm that pervaded public opinion and the mass media in the second half of the twentieth century . the american philosopher john dewey wrote : the destructive use made of the fission of the nucleus of an atom has become the stock - in - trade of the assault upon science . what is so ignored as to be denied is that this destructive consequence occurred not only in a war but because of the existence of war , and that war as an institution antedates by unknown millennia the appearance on the human scene of anything remotely resembling scientific enquiry [ 11 ]  . today , the sustainability of medical imaging is being questioned [ 12 ]  . 
the so - called deterministic effects , which occur only in the presence of very high doses and coincide with cell death ( apoptosis ) , have a threshold effect and are not ( fortunately ) seen in individuals who undergo irradiation for diagnostic purposes or in personnel exposed to radiation in the workplace ( of course , radiotherapy is a case apart )  . the stochastic or random effects on the body are due to dna alterations produced by radiation , with consequent hereditary effects if these occur in germ cells or radioinduced tumours if they occur in somatic cells . 
particular concern regards computed tomography examinations , the number of which has increased 12 - fold over the last 20 years in europe and more than 20 - fold in the united states , with an increase of at least seven times the average dose per examination delivered to the population [ 15 ]  . laccuratezza diagnostica ( come gli impianti dotati di amplificatore di brillanza e di catene televisive )  . 
si pensi che , per ottenere la stessa quantit di radiazioni ( gamma ) prodotte dalla sola bomba di hiroshima , sarebbero stati necessari milioni di tonnellate del radium dei curie . 
la proliferazione nucleare negli anni della guerra fredda e la recente catastrofe nucleare di chernobyl hanno ulteriormente contribuito al crescente allarme , che ha pervaso lopinione pubblica ed i grandi media nella seconda met del novecento . 
si ignora che tale conseguenza distruttiva avvenuta non solo durante una guerra , ma a causa dellesperienza stessa della guerra , una istituzione nata parecchi millenni prima che comparisse sulla scena umana alcunch di lontanamente somigliante allindagine scientifica [ 11 ]  . oggi ci si interroga sulla sostenibilit dellimaging medico [ 12 ]  . 
per comprendere leffetto delle radiazioni bisogna tener conto del tipo di radiazioni coinvolte , della dose , cio della quantit di energia che esse trasferiscono nei tessuti e della variabile radiosensibilit dei tessuti stessi [ 13 ]  . 
i cosiddetti effetti deterministici , che si verificano solo per dosi molto elevate e coincidono con la morte delle cellule ( apoptosi ) , hanno un effetto - soglia e non si osservano ormai pi ( fortunatamente ) nelle persone sottoposte ad irradiazione per scopi diagnostici o in personale esposto lavorativamente ( diverso , ovviamente , il caso della radioterapia )  . 
 gli effetti stocastici o casuali sono dovuti ad alterazioni del dna prodotte dalle radiazioni , con conseguenti effetti ereditari se avvengono nelle cellule germinali o tumori radioindotti , se avvengono nelle cellule somatiche . 
le preoccupazioni riguardano soprattutto gli esami di tomografia computerizzata ( tc ) , il cui numero aumentato negli ultimi venti anni di 12 volte in europa e di oltre venti volte negli usa , con incremento di almeno 7 volte della dose media erogata per indagini radiologiche alla popolazione [ 15 ]  . state of the art and conclusions stato dellarte e conclusioni there are three theories with regard to the effects of low doses of ionising radiation . 
the best known and official doctrine , which has inspired international radiation protection laws , states that there is no threshold for stochastic effects and that even a single event or a very low dose can cause damage , the probability of which is linearly correlated with the dose ( linear nonthreshold [ lnt ] model )  . 
it has been estimated that one third of all computed tomography examinations could thus be avoided without sacrificing diagnostic accuracy . a second theory , which is not without biological and epidemiological evidence , suggests that the stochastic effects are in proportion to the dose , but in the case of low doses , there is a sort of practical threshold below which cell repair mechanisms manage to avoid damage . 
it may even be possible that the stochastic effects are not completely random , but at low doses only regard genetically predisposed individuals ( who may be identified with appropriate tests )  . the third theory , which goes contrary to accepted belief and is politically incorrect but supported by significant proof , some of which is experimental , is hormesis ( from the greek meaning to excite ) [ 16 ]  . 
moreover , life on earth evolved in conditions of environmental radioactivity much greater than the current average annual background level of around 3 msv , and the longevity of individuals exposed for professional or environmental reasons to small additional doses ( contemporary radiologists , aeroplane pilots or flight attendants , etc . ) is not lower but higher than the average , with a lower incidence of cancer . 
la lnt , estrapolata dagli effetti delle bombe atomiche sui sopravvissuti di hiroshima e nagasaki , considerata vera precauzionalmente , ma non vi sono prove certe che per dosi molto basse , come quelle coinvolte in quasi tutti gli esami di radiodiagnostica in et adulta , essa sia valida . 
la lnt ha ispirato il principio conosciuto con lacronimo alara ( as low as reasonably available ) , secondo il quale la dose erogata dovrebbe essere sempre la pi bassa ragionevolmente possibile in quelle condizioni cliniche [ 15 ]  . 
bisogna dunque mettere in atto ogni presidio tecnico per ridurre la dose erogata , senza che ci vada a discapito della accuratezza diagnostica e bisogna cercare di evitare esami inutili , di efficacia non dimostrata ( esempio : screening del tumore polmonare ) o sostituibili con altre metodiche di analoga efficacia diagnostica ( esempio : ecografia nella diagnosi della appendicite acuta )  . 
si calcola che almeno un terzo degli esami tc potrebbe cos essere evitato , senza pregiudizio per laccuratezza diagnostica . una seconda teoria , non priva di evidenze biologiche ed epidemiologiche , sostiene che gli effetti stocastici sono s proporzionali alla dose , ma che , quando si tratta di dosi piccole , esiste una sorta di soglia pratica , al di sotto della quale i meccanismi riparativi delle cellule e dei tessuti riescono ad evitare danni . 
anche possibile che gli effetti stocastici non siano poi del tutto casuali , ma che riguardino , per dosi basse , solo individui geneticamente predisposti ( ed individuabili con appositi test )  . la terza teoria , eretica e politicamente scorretta , ma sostenuta da notevoli elementi di prova anche sperimentali , lormesi ( dal termine greco che significa stimolazione ) [ 16 ]  . 
del resto , la vita sulla terra si evoluta in condizioni di radioattivit ambientale ben superiori allattuale fondo annuale medio di circa 3 millisievert e la longevit delle persone sottoposte professionalmente o per ragioni ambientali a piccole dosi aggiuntive ( i radiologi contemporanei , i piloti di aereo o le hostess ecc . ) non minore , ma maggiore della media , con minore incidenza di patologia neoplastica , il che sembra convalidare tale teoria . 
lormesi stata fortemente contrastata nei decenni scorsi , anche perch uno dei suoi ideatori ( arndt ) , oltre che psichiatra , era anche omeopata , ma le notevoli evidenze sembrano richiedere una pi seria valutazione di questa teoria , anche in campo radiologico [ 18 ]  . it is surprising that despite the widespread diffusion of clinical radiology and the advances in scientific knowledge that such an important question has still not received certain pu stupire che , nonostante la grande diffusione della radiologia medica e levoluzione delle conoscenze scientifiche , un problema di questa importanza non abbia ancora radiol med ( 2009 ) 114 : 347357 answers . 
maria delle croci , v.le randi 5 , 48100 ravenna , italy 2scuola di specializzazione in radiodiagnostica , universit degli studi di ferrara , corso giovecca 203 , 44100 ferrara , italy 3servizio di anatomia patologica , ospedale civile s.maria delle croci , v.le randi 5 , 48100 ravenna , italy 4istituto di radiodiagnostica , universit degli studi di ferrara , corso giovecca 203 , 44100 , ferrara , italy correspondence to : g . 
cdus revealed an inflammatory process in 277 patients ( 34.58% ) , testicular trauma in 112 ( 13.9% ) , funicular torsion or torsion of the vestigial remnant in 44 ( 5.4% ) , findings suggestive of testicular neoplasm in 35 ( 4.3% ) and no abnormality in 41.5%. 
mri , used to further investigate the cdus findings in 46 cases , showed three cases of intraparenchymal haematoma , one of intrascrotal cavernous body rupture , one of testicular abscess with intrascrotal fistula , two of testicular infarction and 15 of neoplasmri allowed the exclusion of focal abnormalities in ten patients with testicular microlithiasis , in three with chronic orchitis and in four with atrophic involution . 
on the basis of our experience , cdus is irreplaceable as an initial approach to patients affected by scrotal disease , whereas mri is an ideal second - line investigation . 
lecd ha rilevato : in 277 pazienti ( 34 , 58% ) processo flogistico , in 112 ( 13 , 9% ) trauma del testicolo , in 44 ( 5 , 4% ) torsione del funicolo o di un residuo embrionario , in 35 ( 4 , 3% ) alterazioni riconducibili ad eteroplasia testicolare mentre nel 41 , 5% non erano presenti alterazioni patologiche . 
in 46 casi si ricorsi alla rm per chiarimento o miglior definizione diagnostica del reperto ecd rilevando : 3 casi di ematoma intraparenchimale , 1 caso di rottura intrascrotale del corpo cavernoso , 1 caso di ascesso testicolare con fistola intrascrotale , 2 casi di infarto , 15 casi di eteroplasia . 
la rm utile in casi selezionati , potendo rilevare situazioni complesse e precedentemente insospettabili , risultando in un miglioramento della gestione del paziente e in un contenimento globale dei costi . 
 radiol med ( 2009 ) 114 : 414424 keywords scrotum mri color doppler ultrasound scrotal disorders ultrasonography parole chiave scroto rm eco - color doppler patologia scrotale ultrasonografia introduction introduzione colour doppler ultrasonography ( cdus ) plays a key role as a first - line approach to scrotal disease , as it can help solve diagnostic dilemmas and establish a precise diagnosis , thus leading to appropriate clinical and therapeutic decisions . nevertheless , when the cdus findings are difficult to interpret in relation to the patients clinical data and medical history , or when the clinical and sonographic findings are unjustified , magnetic resonance imaging ( mri ) may be used to elucidate or reveal unusual features [ 1 ]  . the value of mri as a second - line technique after inconclusive sonography [ 2 , 3 ] has rarely been addressed in the literature , and the few existing studies are dated and involve small patient populations . 
the aim of this study was to review our experience of the past 7 years in an attempt to validate the usefulness of cdus in the study of scrotal disease and evaluate the role of mri in selected cases . materials and methods from 2000 to 2007 , 801 male subjects aged from 0 to 87 years were referred to our department to undergo cdus of the scrotuexaminations were carried out on a ge logic 7 sonographic unit with a 715 mhz linear - array probe and colour doppler , power doppler , and b - flow imaging . patients included urgent cases referred from the emergency department and high - priority outpatients referred by the urologist to investigate suspicion of acute or subacute scrotal disease . transverse planes panoramic grey - scale scans were obtained in the longituto compare size and dinal and echogenicity on the two sides . 
colour doppler imaging was then performed , with optimisation of the scanner to obtain the highest sensitivity to slow flow , with low pulse repetition frequency ( prf ) , low wall filter and appropriate colour ga in patients with suspected torsion or infarction , the asymptomatic side was evaluated first to ensure that the parameters for flow evaluation had been set appropriately . mri was performed in 46 patients to confirm or elucidate the cdus findings . 
the criteria adopted to define inconclusive sonographic evaluation were unclear nature of the lesion , inability to delineate the lesion spatially in terms of site and / or extension , conflicting clinical and sonographic diagnosis and marked structural heterogeneity associated with conditions predisposing to malignancy , such as testicular leco - color doppler ( ecd ) riveste un ruolo di primo approccio nella patologia dello scroto risolvendo nella maggior parte dei casi lenigma diagnostico oppure delineando in modo esaustivo il quadro patologico , permettendo cos corrette decisioni e idonei approcci clinico - terapeutici . 
pur tuttavia , in presenza di quadri ecd di dubbia interpretazione alla luce del reperto clinico - anamnestico o in presenza di reperti clinico - ecografici ingiustificabili , la risonanza magnetica ( rm ) pu trovare applicazione per risolvere , chiarire o svelare aspetti a volte inusuali [ 1 ]  . solo pochi autori hanno esaminato il ruolo della rm come metodica di secondo livello in caso di reperti ecografici non esaustivi [ 2 , 3 ]  . 
finalit del lavoro stata quella di effettuare una revisione della nostra casistica degli ultimi 7 anni allo scopo di riconfermare lutilit dellecd nellapproccio alle patologie dello scroto e far emergere il ruolo della rm in casi selezionati . materiali e metodi dal 2000 al 2007 sono stati inviati al nostro servizio 801 pazienti maschi di et compresa tra 0 e 87 anni , per essere sottoposti ad indagine ecd dello scroto con ecografo ge logic 7 con sonda lineare 715 mhz con modulo color doppler , power doppler e b flow . 
i pazienti erano giunti alla nostra osservazione in regime di urgenza , in quanto inviati dal pronto soccorso , oppure in regime prioritario ambulatoriale su consiglio dello specialista urologo , nel sospetto di una patologia acuta o subacuta . sono state eseguite scansioni in scala di grigi quanto pi possibile panoramiche , sui piani longitudinale e trasversale , per confrontare le dimensioni e lecogenicit dei due lati . 
lo studio color doppler stato condotto successivamente , ottimizzando lapparecchiatura per ottenere la massima sensibilit ai flussi lenti , con una bassa pulse repetition frequency ( prf ) , bassi filtri di parete e un appropriato guadagno di colore . 
nei casi di sospetta torsione o infarto , il lato asintomatico stato valutato per primo , per assicurarsi che i parametri di valutazione del flusso fossero settati in modo opportuno . in 46 pazienti si ritenuto di procedere ad indagine rm , per confermare o chiarire il dato ecd , rilevando in alcuni 416 radiol med ( 2009 ) 114 : 414424 microlithiasis , testicular retention and chronic orchitis . mri was performed on a 1.5 - tesla philips achieva unit with a 14 - cm circular surface coil . 
for studying the scrotum in the three orthogonal planes , a t2 - weighted fast spin - echo sequence with a 1012 - cm field of view and a 256256 matrix was used . 
axial t1 - weighted spoiled gradient - echo images were also obtained to detect haemorrhage . only selected cases were studied with mri following intravenous administration of gadolinium with diethylenetriamine penta - acetic acid ( gd - dtpa ) ; in these cases , axial and coronal t1 - weighted spoiled gradient - echo sequences with fat saturation were obtained after contrast injection . definitive diagnoses were confirmed at surgery in the cases of funicular torsion , morgagnis hydatid torsion and inguinoscrotal hernia . 
in the case of inflammatory processes , thrombophlebitis of the pampiniform plexus , complicated cysts and scrotal trauma with intact tunica vasculosa , the diagnosis was declared ex adjuvantibus after successful medical treatment , as confirmed by lesion regression at serial us follow - up and resolution of clinical symptoms . results among the 801 patients examined , medical history , clinical data and cdus findings led to a definite diagnosis of inflammatory process in 277 patients , traumatic lesion in 112 , funicular torsion in 33 ( three cases appearing at birth , with intrauterine torsion ) and torsion of the hydatid of morgagni [ 4 , 5 ] in 11 . 
i criteri utilizzati per definire la valutazione ecografia non esaustiva sono stati : incerta natura della lesione , incapacit dellecografia di definire spazialmente la lesione in termini di sede e / o di estensione della stessa , la discrepanza tra la clinica e la diagnosi ecografia , la presenza di una marcata disomogeneit strutturale in presenza di condizioni predisponesti linsorgenza di neoplasie quali microlitiasi testicolare ( mt ) , ritenzione testicolare , orchite cronica . abbiamo impiegato unapparecchiatura philips achieva 1 , 5 tesla con una bobina di superficie , circolare da 14 cm . per la patologia del canale inguinale si studiata la pelvi mediante scansioni assiali usando un campo di vista pi ampio . 
per lo studio dello scroto sui 3 piani ortogonali sono stati utilizzati : una sequenza fast spin - eco pesata in t2 , un campo di vista 1012 cm e una matrice 256256 . 
sono anche state acquisite immagini assiali spoiled - gradient - eco t1 pesate , molto utili per identificare lemorragia . lacido dietilen - triamino - penta - acetico chelato con gadolinio ( gd - dtpa ) , per via endovenosa , stato somministrato solo in casi selezionati ; sono state condotte acquisizioni assiali e coronali dopo somministrazione del mezzo di contrasto , sfruttando sequenze spoiled - gradient - eco con saturazione per il grasso t1 pesate . 
per le lesioni di sospetta origine neoplastica si proceduto con esame citologico estemporaneo intraoperatorio seguito in caso di reperto dubbio o positivo da orchiectomia e in caso di negativit da nodulectomia . 
nei processi flogistici , nelle tromboflebiti del plesso pampiniforme , nelle cisti complicate e nei traumi del testicolo con conservazione dellintegrit della tunica vasculosa , la diagnosi stata confermata ex adjuvantibus dal successo della terapia medica , confermato dalla regressione delle lesioni nel corso di controlli ecografici seriati e dalla regressione del quadro clinico . 
 risultati tra gli 801 pazienti esaminati lanamnesi , i dati clinici e i reperti ecd hanno permesso la diagnosi definitiva di : processo flogistico in 277 pazienti , lesione traumatica in 112 , torsione del funicolo in 33 casi ( in 3 con comparsa alla nascita e torsione intrauterina ) e torsione dellidatide del morgagni [ 4 , 5 ] in 11 pazienti . 
in 15 patients , mri confirmed the suspicion of neoplastic lesion by showing t1 isohyperintensity and clear t2 hypointensity relative to the surrounding parenchyma . the use of contrast material allowed us to evaluate lesion vascularity ( with findings virtually coincident with cdus and b - flow imaging )  . 
in ten patients with testicular microlithiasis on cdus , mri enabled us to rule out alterations in signal intensity or enhancement that might indicate ecografica , sottoposti a rm come indagine di secondo livello , sono stati 46 pari al 5 , 74% . 
in 15 pazienti la rm ha confermato il sospetto di lesione neoplastica in base allaspetto isoiperintenso in t1 e francamente ipointenso in t2 rispetto al parenchima circostante . lutilizzo del mdc ha permesso di valutare la vascolarizzazione delle lesioni ( con reperto sostanzialmente sovrapponibile al dato ecd e b flow )  . 
in 10 pazienti con reperto ecd di mt la rm ha permesso di escludere con sicurezza alterazioni di segnale o di contrast - enhancement ( c.e. ) riferibili a lesioni parenchimali ( in 1 caso ha consentito di rilevare accumulo focale di calcio - pirofosfatodiidratato )  . 
in 4 pazienti affetti da ritenzione testicolare grazie alla rm stato possibile identificare la sede del testicolo atrofico non visibile ecograficamente , differeziando tale condizione dallagenesia testicolare , ed escludere una patologia eteroproduttiva a cui tali soggetti sono predisposti . 
3a - c cisti intrascotale con contenuto infiammatorio : a aspetto ecd ; b rm : sequenza pesata in t1 ; c rm sequenza pesata in t2 . parenchymal lesions ( in one case , it allowed detection of a focal accumulation of calcium - pyrophosphate - dihydrate )  . mri was also used to confirm the sonographic diagnosis of inguinoscrotal hernia in three cases , in which it showed the presence of intestinal loops in the scrotal region . 
in four patients with cryptorchidism , mri helped to locate the undescended testis , which was not visible at us , to differentiate this condition from testicular agenesis and to exclude possible malignancy . 
likewise , it enabled us to exclude nella nostra casistica i casi ritenuti dubbi e sottoposti a rm come indagine di secondo livello sono stati 46 pari al 5 , 74% . 
 radiol med ( 2009 ) 114 : 414424 areas of signal alteration or increased contrast enhancement in three patients with chronic orchitis in whom cdus had shown marked echostructural inhomogeneity . 
mri was also used to follow - up conservative treatment in two patients with scrotal trauma and cdus findings of discontinuity of the tunica albuginea and intact capsular vascularity . discussion in our series , mri was performed as a second - line investigation in 46 patients ( 5.74% ) with inconclusive cdus findings . 
this pattern , which has been previously described in the literature [ 6 ] , is particularly useful for solving interpretation doubts : it should be noted that 10%15% of testicular neoplasms are detected as a consequence of traumas [ 79 ]  . in one patient with a large intrascrotal collection , mri enabled a diagnosis of epididymo - orchitis with abscess formation and intrascrotal fistula , which could not be detected by cdus . 
on the basis of the literature and patients clinical data , we interpreted the findings as complicated testicular cysts , an interpretation that was confirmed ex adjuvantibus after symptom resolution with appropriate medical treatment . 
si tratta di un reperto , gi descritto in letteratura [ 6 ] , utile laddove sussistano dubbi interpretativi : si tenga conto che il 10%15% delle lesioni eteroplasiche testicolari vengono scoperte in conseguenza di un trauma [ 79 ]  . in un pazienze con voluminosa raccolta intrascrotale la rm ha permesso di rilevare orchiepididimite ascessualizzata con tramite fistolizzato in sede intrascrotale , difficilmente rilevabile allindagine ecd . 
analogamente basandoci su tali osservazioni e sulla clinica abbiamo interpretato i nostri reperti come cisti del testicolo complicate , confermate poi ex juvantibus dalla risoluzione del quadro dopo adeguata terapia medica . 
contrast - enhanced t1 sequences demonstrated the characteristic rim of enhancement delimiting the lesion [ 12 , 13 ]  . in 15 patients with cdus findings suggestive of testicular neoplasm , mri confirmed the diagnosis ( definitive histology revealed 11 cases of germ - cell tumour and four benign neoplasms , two of which were adenomatoid tumours and two sertoli - cell tumours )  . 
in these patients , mri also enabled preoperative staging by depicting possible infiltration of the tunica albuginea , tunica vaginalis , epididymis and / or of the para - epididymal tissues . 
in questi pazienti la rm ha inoltre permesso la stadiazione pre - operatoria , potendo definire tunica albuginea , della tunica vaginale , dellepididimo e / o dei tessuti paraepididimari . 
in letteratura si trovano opinioni discordanti sul significato della mt , tuttavia prevalgono le tesi che attribuiscono alla mt il ruolo di condizione precancerosa [ 1418 ]  . in un paziente che presentava formazione dubbia del testicolo , del diametro di circa 1 cm , in sede parailare , iperecogena e senza significativo flusso intralesione all ecd , la rm ha evidenziato alta intensit del segnale nelle sequenze pesate in t1 e basso segnale in t2 . 
tale reperto risulta invariato da 3 anni e , alla luce di quanto riferito da alcuni aa [ 1921 ] , pu essere attribuito ad accumulo di calcio - pirofosfato - diidratato . la rm non in grado di identificare la mt [ 2224 ] : questo aspetto pu facilitare il rilievo di aree di alterato segnale nel parenchima testicolare in pazienti affetti da questa condizione . 
perci , ove la disomogeneit ecostrutturale del parenchima associata alla mt non ha permesso lassoluta esclusione con lecd di lesioni eteroproduttive , siamo ricorsi alla rm che ha escluso alterazioni di segnale radiol med ( 2009 ) 114 : 414424 fig . 
5a - d infarto testicolare ; a immagine ecd ; b immagine rm pesata in t1 ; c immagine rm pesata in t2 ; d immagine rm con mdc . low signal intensity on t2 . 
this finding has remained unchanged for 3 years and , based on previous reports [ 1921 ] , it may be due to an accumulation of calciumpyrophosphate - dihydrate . mri is unable to depict testicular microlithiasis [ 2224 ] , and this may facilitate the detection of parenchymal areas with pathological signal in affected patients . 
therefore , when the parenchymal echostructural inhomogeneity associated with testicular microlithiasis did not allow malignant lesions to be confidently excluded with cdus , the patient was further studied with mri , which revealed no signal alterations or areas of contrast enhancement in the testis . similarly , mri proved useful in three patients with marked parenchymal echostructural alteration due to chronic inflammation , in whom it confirmed the cdus findings and revealed no focal alteration . four patients with atrophic testicular involution secondary to cryptorchidism and / or funicular torsion and who presented diffuse parenchymal echostructural alterations on cdus were also studied with mri to exclude focal parenchymal lesions . 
cryptorchidism is a well - known risk factor for nel testicolo , ma soprattutto non ha rilevato aree di potenziamento dopo mezzo di contrasto . con analogo significato la rm risultata utile in 3 pazienti con marcata alterazione ecostrutturale del parenchima per flogosi cronica , nei quali ha confermato il reperto ecd non rilevando alterazioni focali . sempre per escludere lesioni focali parenchimali sono stati sottoposti a rm 4 casi di involuzione atrofica del testicolo , secondaria a ritenzione testicolare e / o a torsione del funicolo , che presentavano sovvertimento ecostrutturale diffuso del parenchima allecd . 
la ritenzione testicolare rappresenta un noto fattore di rischio per linsorgenza di neoplasie testicolari [ 2527 ] e in questi pazienti consigliato il monitoraggio ecografico : a volte la marcata alterazione ecostrutturale del parenchima e / o la scarsit del flusso parenchimale all ecd nel testicolo atrofico , possono creare dubbi allecografista . 
6a - c trauma dello scroto con rottura della tunica albuginea e integrit della tunica vascolosa : a quadro ecd ; b controllo ecd ; c quadro rm in esiti di rottura della tunica albuginea post - traumatica . testicular neoplasm [ 2527 ] , and sonographic surveillance is recommended in all patients with this condition . 
our experience confirms the usefulness of mri to exclude cancerous lesions . in three cases , mri confirmed the cdus suspicion of omental herniation within the inguinal canal , thus proving its extreme utility in the study of this structure [ 7 ]  . a ruptured tunica albuginea is an indication for exploratory surgery [ 2832 ]  . 
our relatively limited experience demonstrates that surgery is required only in patients with compromised capsular vascularity , that is , of the tunica vasculosa that runs below the tunica albuginea . as is known , on reaching the lower pole of the testis , the testicular artery divides into branches that pierce the tunica albuginea and run along the periphery of the testis in a layer known as the tunica vasculosa . 
dalla nostra seppur limitata esperienza si evince che i pazienti da sottoporre a revisione chirurgica , sarebbero solo quelli con compromissione della vascolarizzazione capsulare e cio della tunica vasculosa che decorre sotto la tunica albuginea  . 
come noto larteria testicolare giunta in prossimit del polo inferiore del testicolo si suddivide in diversi rami , che decorrono alla periferia del testicolo al di sotto della tunica albuginea , formando la cos detta tunica vascolosa . 
da queste arterie capsulari si sviluppano branche centripete che penetrano nel parenchima testicolare decorrendo verso il mediastinum testis ove si arborizzano in rami ricorrenti [ 10 , 33 ]  . 
si pu radiol med ( 2009 ) 114 : 414424 parenchyma and run towards the testicular mediastinum , where they arborise into recurrent rami [ 10 , 33 ]  . 
consequently , it appears reasonable to believe that discontinuity of the tunica albuginea with normal capsular vascularity is an indication for conservative treatment and close clinical and imaging follow - up . conclusions in our experience , cdus is irreplaceable as a first - line approach to patients with scrotal disease . 
we have proposed cdus evaluation of tunica vasculosa integrity in cases of testicular rupture to determine the feasibility of a conservative approach , even in the presence of discontinuity of the tunica albuginea . testicular infarction ; mri is highly valuable in the diagnosis of intratesticular haematoma ; cysts with atypical , presumably inflammatory content ; testicular abscess with intrascrotal fistula ; and in the diagnosis and preoperative staging of testicular neoplasms . 
mri proved to be an ideal second - line modality to be used in selected complex cases , as it improved patient management , leading to fewer unnecessary surgical operations and lower overall costs . quindi sostenere lipotesi che la soluzione di continuit della tunica albuginea con integrit della vascolarizzazione capsulare rappresenti indicazione alla terapia conservativa , con stretto monitoraggio clinico - strumentale . conclusioni dalla nostra esperienza lindagine ecd appare di insostituibile utilit nel primo approccio al paziente con patologia scrotale . 
abbiamo proposto la valutazione con ecd dellintegrit della tunica vasculosa , nei casi di rottura del testicolo , al fine di valutare lipotesi di un approccio terapeutico conservativo , anche in presenza di soluzione di continuit della tunica albuginea . la rm si offre come metodica di insostituibile utilit nella diagnosi di ematoma intratesticolare , di cisti a contenuto atipico verosimilmente infiammatorio , di infarto testicolare , di ascesso testicolare con fistolizzazione intrascrotale nonch nella diagnosi e stadiazione preoperatoria delle eteroplasie testicolari . 
salvatore dipartimento di scienze biomorfologiche e funzionali ( dsbmf ) , universit degli studi di napoli federico ii , istituto di biostrutture e bioimmagini , consiglio nazionale delle ricerche ( cnr ) ; fondazione sdn ( irccs ) , napoli , italy correspondence to : s . 
the aim of this study was to directly compare the results of magnetic resonance cholangiopancreatography ( mrcp ) with those of ultrasonography ( us ) and multislice computed tomography ( msct ) in the diagnosis of pancreaticobiliary diseases . 
a total of 70 patients ( 41 men , 29 women ) aged 2289 years were studied either before ( n = 59 ) or after cholecystectomy ( n = 11 ) for biliary lithiasis . clinical signs and symptoms were jaundice ( n = 15 ) , abdominal pain ( n = 37 ) and proven biliary lithiasis ( n = 18 )  . mrcp was performed in all patients , whereas abdominal us was performed in 55 ( group 1 ) and msct in 37 ( group 2 ) patients . 
histology ( n = 27 ) , biopsy ( n = 5 ) , endoscopic retrograde cholangiopancreatography ( ercp ) ( n = 28 ) and / or clinicalimaging follow - up ( n = 10 ) were considered standards of reference . 
in particular , patients were classified as showing benign ( n = 47 ) or malignant ( n = 12 ) lesions or normal biliary anatomy ( n = 11 )  . 
in group 1 , the results of mrcp and us were concordant in the majority ( 92% ) of cases ; however , statistically significant discordance ( p < 0.01 ) was found in the evaluation of the extrahepatic ducts , with nine cases riassunto obiettivo . 
sono stati arruolati 70 pazienti ( 41 maschi , 29 femmine ) , di et compresa tra 22 e 89 anni , in fase diagnostica pre - chirurgica ( n = 59 ) o dopo colecistectomia per litiasi biliare ( n = 11 ) ; i pazienti presentavano ittero ( n = 15 ) , sintomatologia dolorosa addominale ( n = 37 ) e litiasi biliare documentata ( n = 18 )  . 
in tutti i pazienti stata eseguita la cprm ; in 55 casi stata effettuata us addominale ( gruppo 1 ) , mentre 37 pazienti sono stati sottoposti ad esame tcms ( gruppo 2 )  . 
stata eseguita unanalisi regionale nei principali distretti del sistema bilio - pancreatico : colecisti e dotto cistico , vie biliari intraepatiche ( vbi ) , via biliare principale ( vbp ) e dotto pancreatico principale . 
per linterpretazione dei risultati degli esami diagnostici , i dati istologici post - chirurgici ( n = 27 ) , bioptici ( n = 5 ) , della colangio - pancreatografia retrograda endoscopica ( cpre ) ( n = 28 ) o del follow - up ( 36 mesi ) clinico - strumentale ( n = 10 ) sono stati considerati gli standard di riferimento ; in particolare sono stati osservati 47 casi di lesioni biliari benigne , 12 lesioni maligne e 11 casi con normale anatomia delle vie biliari . radiol med ( 2009 ) 114 : 390402 ( 16% ) of middle - distal common bile duct stones being detected on mrcp only . 
the results of our study confirm the diagnostic potential of mrcp in the study of the pancreaticobiliary duct systein particular , the comparison between mrcp and us and msct indicates the superiority of mrcp in evaluating bile ducts and detecting stones in the common bile duct . keywords ultrasound computed tomography magnetic resonance biliary lithiasis risultati . 
nel gruppo 1 , stata osservata una concordanza globale dei risultati della cprm e dellecografia nel 92% dei casi ; tuttavia , stata riscontrata una discordanza del 16% ( n = 9 ) statisticamente significativa ( p < 0 , 01 ) tra i risultati delle due metodiche nella valutazione della vbp ove la cprm mostrava lesioni litiasiche in sede medio distale non evidenti allecografia . 
i risultati della nostra esperienza confermano le potenzialit diagnostiche della cprm nello studio del sistema duttale bilio - pancreatico ; in particolare , i dati di confronto con lecografia e la tcms dimostrano i vantaggi della cprm nella valutazione distrettuale dei dotti biliari con particolare riferimento alla coledocolitiasi . parole chiave ecografia tomografia computerizzata risonanza magnetica litiasi biliare introduction introduzione diagnostic imaging of pancreaticobiliary disease includes numerous techniques that are selected on the basis on the patients signs and symptoms , the diagnostic information sought , the techniques invasiveness and the therapeutic needs of each individual case . 
in particular , ultrasonography ( us ) and computed tomography ( ct ) , the most commonly used noninvasive modalities in the study of the pancreaticobiliary system , appear to have high specificity but lower sensitivity , especially in patients with common bile duct stones that require alternative techniques such as endoscopic retrograde cholangiopancreatography ( ercp ) [ 14 ]  . 
however , despite its high sensitivity , specificity and diagnostic accuracy and its inherent therapeutic possibilities , ercp is invasive and thus has limited use for diagnostic purposes alone [ 47 ]  . 
this has led to the use of other techniques , the most important of which is magnetic resonance cholangiopancreatography ( mrcp ) that allows for correct depiction of the pancreaticobiliary ducts without being invasive for the patient . 
the availability of multiple imaging modalities , each with different levels of invasiveness and accuracy , calls for protocols or guidelines to ensure that patients with pancreaticobiliary disease are managed correctly . comparative studies on the modalities used for diagnosing pancreaticobiliary disease indicate a fundamental la diagnostica per immagini delle malattie del sistema bilio - pancreatico rappresentata attualmente da numerose tecniche la cui scelta funzione di diversi fattori , quali la sintomatologia e le condizioni del paziente , linformazione diagnostica richiesta , linvasivit della metodica e le necessit terapeutiche di ogni singolo caso ; in particolare , lecografia ( us ) e la tomografia computerizzata ( tc ) , le pi comuni metodiche di imaging non invasivo utilizzate nello studio del sistema bilio - pancreatico , mostrano unelevata specificit ma una minore sensibilit diagnostica particolarmente nei pazienti affetti da calcolosi del coledoco , tanto che in tali casi si ricorre frequentemente a tecniche alternative quali ad esempio la colangio - pancreatografia retrograda endoscopica ( cpre ) [ 14 ]  . 
la cpre , nonostante lelevata sensibilit , specificit e accuratezza diagnostica e le possibilit terapeutiche intrinseche alla metodica stessa , mostra tuttavia uninvasivit che ne rende limitato il suo solo utilizzo diagnostico [ 47 ]  . 
pertanto , in base a tali considerazioni stato necessario ricorrere ad altre tecniche tra cui principalmente la colangio - pancreatografia con risonanza magnetica ( cprm ) che fornisce una corretta rappresentazione del sistema duttale bilio - pancreatico senza alcuna invasivit per il paziente ; dunque , la disponibilit di molteplici metodiche di diagnostica per immagini , 392 radiol med ( 2009 ) 114 : 390402 role for mrcp , which has high sensitivity , specificity and accuracy [ 3 , 4 , 811 ]  . 
the literature indicates that us has a good level of accuracy in the study of the extrahepatic common hepatic duct and of the intrahepatic bile ducts when dilated but performs less well in the assessment of the middle - distal portion of the extrahepatic ducts [ 10 , 1214 ]  . 
multislice ct technology allows reconstruction of three - dimensional volumetric images , with significant advantages in the evaluation of bile duct anatomy . however , given that ct cannot always visualise the cause of the obstruction because of the frequent isodensity of stones relative to bile , detection is based on the same indirect criteria as used at us , such as dilatation of the bile ducts above the stenosis . 
for this reason , it has been suggested that ct with biliary contrast material may help identify filling defects caused by the presence of radiolucent stones within the opacified bile duct lumen , especially in patients with contraindications to mrcp [ 15 ]  . the purpose of our study was to evaluate the role of mrcp compared with us and msct in diagnosing pancreaticobiliary disease . 
to this end , we performed a comparative analysis of the results of imaging in the main regions of the pancreaticobiliary system ( gallbladder , intrahepatic bile ducts , extrahepatic bile ducts , main pancreatic duct )  . materials and methods population a total of 70 patients ( 41 men , 29 women ) aged 2289 ( mean 58 ) years were retrospectively reviewed . 
patients were studied before ( n = 59 ) or after cholecystectomy for lithiasis ( n = 11 ) and were referred because of jaundice ( mean total bilirubin = 4.9 mg / ml ; mean direct bilirubin = 4.0 mg / ml ) ( n = 15 , 21% ) , abdominal pain ( n = 37 , 53% ) or bile stones detected on us ( n = 18 , 26% )  . 
for 55 patients , the results were compared with abdominal us scans ( group 1 ) and for 37 patients with abdominal ct scans ( group 2 )  . ultrasonography patients were imaged with an atl 5500 hdi unit after a 6h fast and in various positions ( supine , left lateral , upright )  . examinations were carried out with a 3.54 mhz probe initially placed subcostally during deep breath - holding or between the 10th and 11th rib , without breath - holding . 
transverse , longitudinal and oblique scans of the upper abdomen were performed , as reported in the literature [ 16 ]  . pi o meno invasive ed accurate , richiede la definizione di specifici protocolli diagnostici o linee guida clinicamente fondamentali per la corretta gestione dei pazienti affetti da malattie del sistema bilio - pancreatico . gli studi di confronto attualmente disponibili tra le varie metodiche di imaging impiegate nella valutazione diagnostica del sistema bilio - pancreatico dimostrano un ruolo fondamentale della cprm che ha mostrato elevati valori di sensibilit , specificit e accuratezza [ 3 , 4 , 811 ]  . 
in particolare , nei pazienti con calcolosi biliare , che rappresenta la condizione morbosa pi frequente , laccuratezza diagnostica delle varie tecniche nellidentificazione dei calcoli biliari varia in funzione della sede , delle dimensioni e della struttura delle lesioni litiasiche ; i dati riportati in letteratura mostrano una buona accuratezza dellecografia nello studio del dotto epatico comune nel suo tratto extra - epatico e dei dotti biliari intra - epatici se dilatati , ma una pi difficile valutazione del tratto medio - distale della via biliare principale [ 10 , 1214 ]  . 
levoluzione tecnologica in tc con la metodica multi - strato consente la ricostruzione di immagini tridimensionali volumetriche determinando un significativo vantaggio nella valutazione dellanatomia delle vie biliari ; tuttavia , la tc non potendo sempre identificare la causa dellostruzione per lisodensit che i calcoli possono mostrare rispetto alla bile , utilizza i medesimi criteri indiretti usati in us quali la dilatazione delle vie biliari a monte della lesione stenosante ; per tale motivo stato proposto , in particolare nei pazienti che non possono essere sottoposti alla cprm per controindicazioni tecniche , lutilizzo in tc di un mezzo di contrasto ad escrezione biliare al fine di identificare difetti di riempimento da formazioni litiasiche radiotrasparenti allinterno del lume biliare opacizzato dal mezzo di contrasto [ 15 ]  . lo scopo del nostro studio stato la valutazione del ruolo specifico della cprm nella diagnostica del sistema bilio - pancreatico in confronto ad altre tecniche per immagini quali lus e la tc ; a tale proposito , stata effettuata unanalisi regionale comparativa del risultato delle immagini nei principali distretti biliari ( colecisti , dotti intraed extra - epatici , dotto pancreatico principale )  . materiali e metodi popolazione sono stati valutati in una analisi retrospettiva 70 pazienti ( 41 maschi , 29 femmine ) di et compresa tra 22 e 89 anni ( et media 58 anni )  . 
i pazienti sono stati studiati in fase diagnostica pre - chirurgica ( n = 59 ) o dopo colecistectomia per litiasi ( n = 11 ) ; i pazienti sono stati valutati per ittero ( valore medio di bilirubina totale = 4 , 9 mg / ml ; valore medio di bilirubina diretta = 4 , 0 mg / ml ) ( n = 15 , 21% ) , dolore addoradiol med ( 2009 ) 114 : 390402 computed tomography the ct study was carried out with the multislice technique ( toshiba aquilion , with 4 detector rows ) after administration of both oral and intravenous contrast material . 
oral contrast material ( barium sulphate , prontobario tac , bracco , italy ) was administered at a dose of 10 ml per 200 ml of water approximately half an hour before the examination . 
early scans in the angiographic , arterial ( 30 s ) and portal ( 60 s ) phase permitted differentiation between portal vessels and bile ducts , whereas the late scans in the equilibrium phase ( 180300 s ) produced hepatobiliary parenchymal enhancement . 
 mr cholangiography all mrcp examinations were carried out after administration of 900 ml oral superparamagnetic contrast agent [ a suspension of silicon - coated iron oxide crystals ( ferumoxsil ) , lumirem , guebert ]  . 
patients were imaged on a high - field device ( intera 1.5 t , philips ) using a phased - array synergy body coil and dedicated breath - hold t2 - weighted sequences ( mrcp - rad - bh )  . 
the sequence was a 40 - mm - thick singleslab half - fourier sequence , with acquisition matrix 256 , reconstruction matrix 256512 , fov 250 mm , effective echo time ( teeff ) 1 , 050 ms , and repetition time ( tr ) 2 , 600 ms . 
in all patients , the cholangiographic acquisitions were complemented with axial and coronal sequences of the upper abdomen , t1 [ fastfield echo breath - hold ( ffe - bh ) ] sequences without fat suppression , tr / te 214 / 46 ms , fa 80 , matrix 192512 , slice thickness 5 mm , conventional t2 turbo spin echo ( tse ) ( with and without fat suppression ) , tr / te 831 / 80 ms , fa 80 , matrix 192512 , slice thickness 5 mm , and fatsuppressed t1 ffe - bh using a multiphase dynamic technique after intravenous administration of 0.1 mmol / kg body weight paramagnetic contrast material ( gadopentetic acid , magnevist , schering )  . 
 data analysis in the two patient groups , a regional analysis of the concordance or discordance of the results obtained with the two imaging techniques was carried out by comparing the main regions of the pancreaticobiliary system : gallbladder and cystic duct , intrahepatic bile ducts , extrahepatic bile ducts ( divided into common hepatic duct and common bile duct ) minale ( n = 37 , 53% ) o litiasi biliare documentata allecografia ( n = 18 , 26% )  . 
tutti i pazienti sono stati sottoposti ad cprm ; in 55 pazienti stato disponibile il confronto con lesame ecografico delladdome ( gruppo 1 ) , mentre in 37 pazienti stato disponibile il confronto con lesame tc delladdome ( gruppo 2 )  . ecografia lesame ecografico ( atl 5500 hdi ) stato eseguito con paziente a digiuno assoluto da almeno 6 ore , in vari decubiti ( supino , fianco sinistro ed ortostasi ) , in apnea inspiratoria profonda con sonda da 3 , 54 mhz posta inizialmente in sede sottocostale oppure , senza apnea respiratoria , a livello intercostale tra la x e la xi costa . 
in tutti gli studi ecografici , limpiego dellcolor doppler ha consentito di differenziare le immagini dei rami portali da quelle dovute a dilatazione delle vie biliari ; sono state eseguite scansioni trasversali , longitudinali ed oblique delladdome superiore , come riportato in letteratura [ 16 ]  . tomografia computerizzata lo studio tc stato eseguito con tecnica multistrato ( aquilion toshiba 4 file di detettori ) dopo somministrazione di mezzo di contrasto sia per via orale che endovenosa . 
il contrasto orale , prontobario tac ( solfato di bario , bracco ) , stato somministrato circa mezzora prima dellesame al dosaggio di 10 ml ogni 200 ml dacqua ; il mezzo di contrasto endovenoso organoiodato ( ultravist , schering 370 mg / i / kg ) stato iniettato ad un dosaggio di 120150 ml ( 3 ml / s per 25 secondi ) con tecnica dinamica multifasica standardizzata ( collimazione 3 mm ; pitch 0 , 871 , 25 ) ; le scansioni precoci in fase angiografica , arteriosa ( 30 s ) e portale ( 60 s ) hanno consentito la differenziazione tra i vasi portali e i dotti biliari , mentre le scansioni tardive allequilibrio ( 180300 s ) hanno offerto leffetto parenchimografico epato - biliare . 
 colangiografia rm tutti i pazienti , previa assunzione orale di mezzo di contrasto super - paramagnetico [ sospensione di cristalli di ossido di ferro rivestiti di silicone ( ferumoxsil ) lumirem , guebert ] alla dose di 900 ml , sono stati studiati con cprm utilizzando unapparecchiatura ad alto campo ( intera 1 , 5 t , philips ) e sequenze dedicate in apnea espiratoria t2 pesate ( cprm - rad - bh ) , usando una bobina phased array synergy body coil ; come sequenza stata usata la single slab half fourier , a singola fetta di 40 mm di spessore con matrice di acquisizione 256 e matrice di ricostruzione 256512 , un fov di 250 mm , con tempo di eco effettivo ( teeff ) di 1050 millisecondi , tempo di ripetizione ( tr ) di 394 radiol med ( 2009 ) 114 : 390402 and main pancreatic duct . 
the assessment criteria have been previously reported [ 19 , 20 ] and include : gallbladder ( degree of distension , dimorphism , heterogeneity of content and / or presence of filling defects , wall thickness and wall irregularity ) cystic duct ( calibre , normal tortuosity of course and filling defects ) , intrahepatic bile ducts ( increase in calibre > 2 mm , heterogeneity of content and / or presence of filling defects ) , common hepatic duct ( increase in calibre > 5 mm , heterogeneity of content and / or presence of filling defects ) , common bile duct ( increase in calibre > 7 mm , heterogeneity of content and / or presence of filling defects and regular course ) , and main pancreatic duct ( according to recently proposed criteria ) [ 21 ]  . 
 in the interpretation of results , postoperative histological ( n = 27 ) , bioptic ( n = 5 ) , ercp ( n = 28 ) findings and / or those of the clinicalimaging ( 36 months ) follow - up ( n = 10 ) were considered standards of reference . 
in particular , we tested the hypothesis that there is significant discordance between results observed in the two patient groups , as confirmed by the reference standards . results group 1 figure 1 shows the results of the comparative regional analysis of mrcp and us . 
in particular , 212 biliary regions were analysed : gallbladder and cystic duct in 47 cases , intrahepatic bile ducts in 55 , extrahepatic ducts in 55 and main pancreatic duct in 55 . 
in the evaluation of the gallbladder region , there was concordance between mrcp and us in 45 cases ( 96% ) , which included negative findings ( n = 17 ) , lithiasis ( n = 20 ) and inflammation ( n = 8 ) , as confirmed by postoperative histology ( n = 24 ) or follow - up ( n = 4 )  . 
le acquisizioni colangiografiche sono state integrate in tutti i pazienti da sequenze secondo piani di scansione assiali e coronali delladdome superiore , t1 ( ffe - bh ) senza soppressione del segnale del tessuto adiposo , tr / te pari a 214 / 46 ms , fa di 80 , matrice 192512 , spessore di scansione di 5 mm , t2 convenzionali tse ( con e senza soppressione del tessuto adiposo ) , tr / te pari a 831 / 80 ms , fa di 80 , matrice 192512 , spessore di scansione di 5 mm , e t1 ffe - bh con soppressione del segnale del tessuto adiposo con tecnica dinamica multi - fasica dopo somministrazione endovena di mdc paramagnetico ( acido gadopentetico , magnevist , schering ) al dosaggio di 0 , 1 mmol / kg peso corporeo ; la tecnica dinamica multi - fasica prevedeva la fase arteriosa a 30 secondi dalla somministrazione , la fase portale a 60 secondi e la fase allequilibrio a 180300 secondi . 
 analisi dei dati nei due gruppi in cui stata suddivisa la popolazione stata eseguita unanalisi regionale relativa alla concordanza o alla discordanza dei risultati ottenuti con le due metodiche poste a confronto nella valutazione dei principali distretti del sistema bilio - pancreatico : colecisti e dotto cistico , vie biliari intra - epatiche ( vbi ) , via biliare principale ( vbp ) , suddivisa in dotto epatico comune e dotto coledoco , e dotto pancreatico principale . 
due osservatori indipendenti non a conoscenza dei dati clinici hanno valutato gli esami di diagnostica per immagini ; i criteri di valutazione utilizzati per lanalisi degli esami diagnostici sono stati i seguenti come riportato in letteratura [ 19 , 20 ] : colecisti ( grado di distensione , dimorfismo , disomogeneit del contenuto e / o presenza di difetti di riempimento e spessore ed irregolarit della parete ) ; dotto cistico ( calibro , regolare tortuosit del decorso e difetti di riempimento ) ; vbi ( incremento di calibro > 2 mm , disomogeneit del contenuto e / o presenza di difetti di riempimento ) ; dotto epatico comune ( incremento di calibro > 5 mm , disomogeneit del contenuto e / o presenza di difetti di riempimento ) , coledoco ( incremento di calibro > 7 mm , disomogeneit del contenuto e / o presenza di difetti di riempimento e regolarit del decorso ) e dotto pancreatico principale secondo i criteri recentemente proposti [ 21 ]  . 
in ascissa sono indicati i distretti bilio - pancreatici : colecisti , vie biliari intraepatiche ( vbi ) , via biliare principale ( vbp ) e dotto pancreatico principale ( wirsung ) ; in ordinata stato riportato il valore percentuale di concordanza e discordanza dei risultati delle due metodiche . 
in the evaluation of the main pancreatic duct , there was concordance between mrcp and us in 52 cases ( 95% ) and , in particular , in cystic lesions of the main pancreatic duct ( n = 2 ) and pancreatic tumour ( n = 4 ) , as confirmed by ercp ( n = 2 ) or postoperative histology ( n = 4 ) ; mrcp and us were also concordant in yielding negative findings in the remaining 46 cases . 
 in the study of the extrahepatic bile ducts , there was concordance between mrcp and us in 46 cases ( 84% ) , which included negative findings ( n = 34 ) , lithiasis ( n = 7 ) and inflammation ( n = 5 ) , as demonstrated by ercp . 
based on statistical analysis , the 16% discordance between mrcp and us in the evaluation of the extrahepatic bile ducts was statistically significant ( p = 0.003 , mcnemar test )  . group 2 results of the comparative regional analysis between mrcp and ct are shown in fig . 
in particular , 143 biliary regions were analysed : gallbladder and cystic duct in 32 cases , intrahepatic bile ducts in 37 , extrahepatic bile ducts in 37 and main pancreatic duct in 37 . 
five patients were come affetti da lesioni benigne ( n = 47 ; 29 litiasi , 13 flogosi , 2 cirrosi biliari primitive , 2 cisti del dotto pancreatico principale e 1 lesione iatrogena ) o maligne ( n = 12 ; 4 colangiocarcinoma e 8 tumori del pancreas ) del sistema biliopancreatico ; nei restanti 11 pazienti non stata riscontrata evidenza strumentale di lesioni patologiche delle vie biliari e / o del pancreas per cui sono stati considerati liberi da malattia . al fine di valutare la significativit statistica dei risultati delle tecniche per immagini osservati nellanalisi regionale del sistema bilio - pancreatico eseguita nei due gruppi di pazienti in cui stata suddivisa la popolazione stato applicato in test di mc nemar , considerando un valore significativo della p < 0 , 05 [ 22 ] ; in particolare , lipotesi da dimostrare stata la significativit statistica della discordanza dei risultati osservati nei due gruppi di pazienti , supportata dai dati degli standard di riferimento . risultati gruppo 1 i risultati della analisi regionale comparativa lecografia e la cprm sono riportati nella fig . 
in particolare , sono stati analizzati 212 distretti biliari , di cui 47 relativi alla colecisti ed al dotto cistico , 55 corrispondenti alla vbi , 55 relativi alla vbp e 55 riguardo il dotto pancreatico principale ; in particolare , 8 pazienti sono stati studiati in follow - up post - colecistectomia per cui non stato valutato il distretto colecistico . 
2a - c gallbladder and common bile duct stones : ultrasonography ( us ) and magnetic resonance cholangiopancreatography ( mrcp ) concordance for the gallbladder and discordance for the common bile duct . 
a us : the image shows ectasia of the intrahepatic bile ducts caused by the presence of stones located near the hilub mrcp reveals signs of intrahepatic bile stones consisting of diffuse intrahepatic duct dilatation and filling defects ( arrow ) near the hilum ; a large stone can also be appreciated in the infundibulum of the gallbladder . 
in ascissa sono indicati i distretti bilio - pancreatici : colecisti , vie biliari intra - epatiche ( vbi ) , via biliare principale ( vbp ) e dotto pancreatico principale ( wirsung ) ; in ordinata riportato il valore percentuale di concordanza e discordanza dei risultati delle due metodiche . 
in the evaluation of the gallbladder region , there was concordance between mrcp and ct in 29 cases ( 91% ) , which included lithiasis ( n = 9 ) , as confirmed by postoperative data , and negative findings ( n = 20 )  . 
similarly , in the evaluation of the main pancreatic duct , there was concordance between mrcp and ct in most cases ( 92% ) , both with ( n = 11 ) and without ( n = 23 ) disease . 
among the cases with positive findings on both methods , ercp confirmed the presence of cystic lesions of the main pancreatic duct ( n = 2 ) , whereas postoperative histology confirmed the presence of a tumour of the head of the pancreas ( n = 8 ) or cholangiocarcinoma of the terminal common bile duct ( n = 1 )  . in contrast , in the study of the intrahepatic and extrahepatic ducts , the two methods yielded a rate of discordance of 19% ( n = 7 ) and 16% ( n = 6 ) , with positive findings on mrcp compared with ct in all cases . 
la valutazione del dotto pancreatico principale ha mostrato in 52 casi ( 95% ) risultati concordanti tra la rm e lecografia ; in particolare , il risultato stato concordante in termini di positivit degli esami in caso di lesioni cistiche del dotto pancreatico principale ( n = 2 ) o di tumori pancreatici ( n = 4 ) , come confermato dai dati della cpre ( n = 2 ) o dellistologia postchirurgica ( n = 4 ) ; al contrario , il risultato delle due tecniche stato concordante in termini di negativit nei rimanenti 46 casi . 
5a , b intrahepatic bile stones : discordance of computed tomography ( ct ) and magnetic resonance cholangiopancreatography ( mrcp ) findings . a ct shows intrahepatic bile duct dilatation , without stones inside . 
b la cprm in immagine assiale t2 pesata convenzionale conferma la dilatazione delle vie biliari intra - epatiche , ma identifica inoltre la presenza di due difetti di riempimento focali ( freccia ) a livello dei dotti biliari principali da lesioni litiasiche . discussion the availability of several imaging techniques , such as us , ct , mri and ercp , for evaluating patients with bile duct diseases requires selecting the most accurate and less invasive modality for each clinical problethis is also a prerequisite for defining the most appropriate diagnostic protocol according to the clinical presentation of each patient [ 23 ]  . in this study , we report the results of a direct comparison of mrcp , us and ct in a group of patients with clinicallaboratory evidence of biliary diseases , 47 of whom had benign lesions , 12 had malignant lesions and 11 were without evidence of organic lesions . 
in particolare , sono stati analizzati 143 distretti biliari , di cui 32 relativi alla colecisti ed al dotto cistico , 37 corrispondenti alla vbi , 37 relativi alla vbp e 37 riguardo il dotto pancreatico principale ; in particolare , 5 pazienti sono stati studiati in followup post - colecistectomia per cui non stato valutato il distretto colecistico . 
in base allanalisi statistica , la percentuale di discordanza ( 19% ) tra la rm e la tc nella valutazione della vbi ha mostrato una significativit al test di mc nemar ( p = 0 , 008 ) ; analogamente la percentuale di discordanza ( 16% ) tra la rm e la tc nella valutazione della vbp ha mostrato una significativit al test di mc nemar ( p = 0 , 01 )  . radiol med ( 2009 ) 114 : 390402 fig . 
6a - c extrahepatic bile duct lithiasis in a patient who underwent cholecystectomy for gallstones : discordant results between computed tomography ( ct ) and magnetic resonance cholangiopancreatography ( mrcp ) at the level of the common bile duct . 
a mrcp indicates dilatation of the segmental intrahepatic bile ducts and of the common hepatic duct that shows a saccular dilatation ; faint and inhomogeneous magnetic resonance imaging ( mri ) signal in the distal bile duct with evidence of multiple fine filling defects , with evidence of residual biliary flow ( arrow )  . 
a la cprm mostra lectasia delle vie biliari intra - epatiche segmentarie , dei dotti biliari principali e del dotto epatico che mostra una dilatazione sacciforme ; il segnale rm appare scarso e disomogeneo a livello del coledoco con evidenza di multipli e fini difetti di riempimento da litiasi , pur tuttavia con segni di flusso biliare residuo ( freccia )  . 
c la tc non mostra definiti segni di litiasi biliare a livello del coledoco intra - pancreatico ( freccia )  . discussione la disponibilit di varie tecniche di diagnostica per immagini , quali lecografia , la tc , la rm e la cpre , per la valutazione dei pazienti affetti da malattie delle vie biliari comporta necessariamente la scelta della metodica pi accurata e meno invasiva in relazione alla specifica problematica clinica ; tale considerazione rappresenta tra laltro il presupposto per la corretta definizione dei protocolli diagnostici in tali pazienti per le diverse patologie a seconda dellesordio clinico [ 23 ]  . in questo studio , riportiamo la nostra esperienza relativa al confronto diretto dei risultati della cprm con quelli dellecografia ( us ) e della tc in un gruppo di pazienti con evidenza clinico - laboratoristica di patologia delle vie biliari , di cui 47 con lesioni di tipo benigno , 12 con lesioni maligne e 11 senza evidenza di lesioni organiche delle vie biliari agli esami di diagnostica per immagini . 
in particolare , il confronto diretto delle tre tecniche per immagini ( cprm , us e tc ) stato eseguito mediante unanalisi regionale dei diversi distretti del sistema bilio - pancreatico quali la colecisti , le vbi , la vbp e il dotto pancreatico principale allo scopo di definire la tecnica di diagnostica pi idonea e valida nella valutazione del singolo distretto biliare in relazione al tipo di patologia ; in particolare , la valutazione dei risultati stata suddivisa in un primo gruppo di pazienti in cui stata eseguito un confronto tra cprm ed us ( gruppo 1 ) ed un secondo gruppo in cui stato effettuato un confronto tra cprm e tc ( gruppo 2 )  . 
 nel gruppo 1 , il confronto diretto tra cprm ed us ha dimostrato una validit diagnostica di entrambe le metodiche di imaging per la valutazione del distretto colecistico , delle vbi e del dotto pancreatico principale sia in caso di patologia benigna che maligna , oltre che nei casi di assenza di lesioni organiche del sistema duttale biliopancreatico . 
al contrario , i risultati comparativi relativi alla valutazione della vbp hanno dimostrato una differenza statisticamente significativa a vantaggio della cprm rispetto allus in particolare nellidentificazione di lesioni litiasiche localizzate a livello del tratto medio e distale della vbp ; tale risultato appare ragionevole in quanto il tratto medio o distale della vbp pu non essere ben studiato dallus per linterferenza del meteorismo intestinale o nei soggetti obesi . 
 [ 8 ] hanno riportato valori di sensibilit ( 91% ) ed accuratezza diagnostica ( 97% ) della cprm superiori a quelli dellus ( 38% e 89% ) ; analogamente , ferrari et al . 
 [ 10 ] nella loro casistica hanno riscontrato una percentuale di risultati falsi negativi allus significativamente superiore a quello della 400 radiol med ( 2009 ) 114 : 390402 and main pancreatic duct with the aim of establishing the most appropriate and reliable diagnostic technique for each region based on the type of disease . 
evaluation of results was divided into two groups : in one group , mrcp was compared with us ( group 1 ) , whereas in the second group , mrcp was compared with ct ( group 2 )  . 
 in group 1 , the comparison between mrcp and us demonstrated that both imaging methods are of value in evaluating the gallbladder region , intrahepatic bile ducts and main pancreatic duct in both benign and malignant diseases , as well as in cases without organic lesions of the pancreatobiliary systeby contrast , results of the evaluation of the extrahepatic bile ducts showed a statistically significant superiority of mrcp , especially in detecting stones in the middle - distal tract of the extrahepatic bile ducts . 
this result is reasonable , given that the middle or distal tract of the extrahepatic bile ducts is not well visualised on us owing to interference from intestinal gas or in obese subjects . 
 [ 8 ] reported high levels of sensitivity ( 91% ) and diagnostic accuracy ( 97% ) for mrcp compared with us ( 38% and 89% ) , and ferrari et al . 
on the other hand , before conventional or laparoscopic cholecystectomy for gallstones , it is crucial to ensure that there are no migrating stones in the common bile duct , as these can cause colic and jaundice in the postoperative period . 
in such cases , mrcp allows the degree of ductal dilatation , the location of the stone visualised as a biliary filling defect , the degree of stenosis caused by the lesion and any residual bile flow to be determined . 
in the diagnostic evaluation of patients with biliary malignancies , although our study showed no statistically significant difference in the analysis of the various biliary regions , mrcp with conventional t1and t2 - weighted sequences and intravenous paramagnetic contrast material has a higher contrast resolution than us and allows a detailed study of biliary tree anatomy ( site , degree , extent and cause of the stenosis , vascular and / or lymph node involvement ) [ 2 ]  . in group 2 , direct comparison between mrcp and ct demonstrated the diagnostic value of both techniques in evaluating the gallbladder and main pancreatic duct , both in cprm nellidentificazione della coledoco - litiasi a sede distale . 
per ovviare a tali limitazioni dellus convenzionale nello studio del tratto distale della vbp , lecografia endoscopica e le pi recenti tecniche ecografiche tridimensionali consentono uno studio pi dettagliato dellalbero biliare [ 11 , 24 , 25 ] ; in particolare , solo lapproccio usendoscopico mostra una sensibilit diagnostica superiore ( 100% ) rispetto a quello della cprm ( 88% ) [ 11 ]  . 
pertanto la cprm certamente la tecnica di diagnostica per immagini di scelta per la valutazione del tratto medio - distale della vbp , sede frequente di lesioni litiasiche ; del resto , prima di una colecistectomia per calcolosi con approccio laparoscopico o tradizionale , fondamentale accertarsi che non vi siano calcoli migranti nel coledoco che determinano coliche ed ittero nel post - intervento o , comunque , in tutti i casi di ittero da stasi necessario una studio accurato delle vie biliari extra - epatiche ; in particolare , la cprm consente di valutare con precisione il grado di dilatazione delle vie biliari , la sede della lesione litiasica identificata semeiologicamente come difetto di riempimento biliare , il grado di stenosi determinato dalla lesione stessa ed , eventualmente , il flusso biliare residuo . 
certamente per quanto riguarda la valutazione diagnostica dei pazienti con lesioni maligne delle vie biliari , nonostante i risultati del nostro studio non hanno mostrato differenze statisticamente significative nellanalisi regionale dei diversi distretti biliari , la cprm offre rispetto allus una maggiore risoluzione di contrasto in quanto , integrata dallimpiego delle sequenza t1 e t2 pesate convenzionali associate alla somministrazione endovenosa di mezzo di contrasto paramagnetico , consente di valutare dettagliatamente le condizioni anatomiche dellalbero biliare ( sede della stenosi , grado della stenosi , estensione della stenosi , causa stenosante , impegno vascolare e / o linfoghiandolare ) [ 2 ]  . 
 nel gruppo 2 , il confronto diretto tra cprm e tc ha dimostrato una validit diagnostica di entrambe le metodiche dimaging per la valutazione del distretto colecistico e del dotto pancreatico principale sia in caso di patologia benigna che maligna , oltre che nei casi di assenza di lesioni organiche del sistema duttale bilio - pancreatico . 
al contrario , i risultati comparativi relativi alla valutazione delle vbi e della vbp hanno dimostrato una differenza statisticamente significativa a vantaggio della cprm rispetto alla tc in particolare nel riconoscimento di lesioni litiasiche nella maggioranza dei casi ; solo in un caso la maggiore risoluzione di contrasto della cprm ha consentito di identificare correttamente una stenosi maligna da colangiocarcinoma della confluenza dei dotti biliari principali nel dotto epatico comune ( tumore di klatskin tipo iv )  . 
 [ 9 ] che dimostrano una maggiore sensibilit diagnostica della cprm ( 100% ) rispetto a quella della radiol med ( 2009 ) 114 : 390402 benign and malignant diseases and in the case of no organic lesions affecting the pancreaticobiliary ducts . 
conversely , results of the evaluation of the extrahepatic bile ducts demonstrated a statistically significant superiority of mrcp over ct , particularly for detecting bile stones of the intraor extrahepatic bile ducts . 
in one case only did the higher contrast resolution of mrcp allow correct identification of a malignant stenosis due to cholangiocarcinoma at the confluence of the main bile ducts into the common hepatic duct ( klatskin type iv tumour )  . 
indeed , despite the improved spatial and temporal resolution brought about by volumetric multislice ct and multiplanar reconstructions , it is well known that ct cannot detect stones that do not have calcium density . 
 [ 11 ] reported similar sensitivity ( 88% ) for mrcp and ct in detecting choledocholithiasis , with both techniques yielding the same number of false negatives due to stones smaller than 5 mdespite having similar accuracy to mrcp , ct cholangiography with biliary contrast agents should be considered only in patients who cannot undergo mrcp or in the case of diagnostic doubts on us and / or mri [ 17 ] owing to the risk of hypersensitivity reactions . 
with regard to malignant lesions , the high contrast resolution of mrcp with the different t1and t2 - weighted sequences enabled correct identification of a klatskin type iv tumour and accurate definition of its hilar and perihilar extension . 
the role of mrcp in patients with cholangiocarcinoma has previously been well documented by others [ 2628 ]  . in conclusion , results of our study suggest that compared with us and ct , mrcp provides greater diagnostic accuracy in evaluating the intrahepatic and extrahepatic bile ducts because it identifies a larger number of strictures secondary to gallstones and their impact on biliary dynamics ( prestenotic dilatation , poststenotic bile flow )  . 
the noninvasiveness , lack of ionising radiation , panoramic capabilities and high spatial and contrast resolution of mrcp in depicting the pancreatobiliary system are significant technical advantages that justify its routine clinical use as a supplement to us , with ct being restricted to patients with contraindications to mrcp or to settings where mri is not available . tc multi - strato ( 82% ) nella coledocolitiasi ; in questo studio , infatti , due casi con lesioni litiasiche del coledoco non risultavano adeguatamente riconosciute dalla tc che inoltre non identificava unostruzione del dotto epatico comune . 
infatti , nonostante i progressi tecnologici della tc , quali la metodica multistrato volumetrica e le ricostruzioni multiplanari che offrono vantaggi in termini di risoluzione spaziale e temporale , noto che lesioni litiasiche non a densit calcica possono non essere identificate dalla tc . 
 [ 11 ] hanno mostrato unanaloga sensibilit diagnostica ( 88% ) della cprm e della tc nel riconoscimento della coledocolitiasi , riportando le stesse false negativit dovute a lesioni litiasiche inferiori ai 5 millimetri . 
la tc con mezzo di contrasto ad escrezione biliare , pur avendo dei valori di accuratezza diagnostica paragonabili a quelli della cprm , a causa del rischio di reazioni da ipersensibilit va considerata come tecnica alternativa solo nei pazienti che non possono essere sottoposti alla cprm o in caso di dubbi diagnostici allesame ecografico e / o di risonanza magnetica [ 25 ]  . 
levent1 1department of radiology , medical faculty , atatrk university , erzurum , turkey 2department of radiology , bilim university , florence nightingale hospital , istanbul , turkey 3department of radiology , numune hospital , erzurum , turkey 4department of pediatric cardiology , medical faculty , atatrk university , erzurum , turkey correspondence to : m . 
sok no 5 , dadaskent , erzurum , turkey , tel . : + 90 - 442 - 2361212 / 1521 , fax : + 90 - 442 - 2361301 , e - mail : akkanrad@hotmail.com received : 28 september 2008 / accepted : 31 october 2008 / published online : 14 april 2009 springer - verlag 2009 abstract purpose . 
these 18 patients were initially referred due to indications such as chest pain ( n = 11 ) , risk - factor assessment ( n = 3 ) , coronary artery anomaly ( n = 1 ) , suspected aberrant right subclavian artery due to dysphagia ( n = 1 ) and coronary artery bypass graft ( n = 2 )  . 
diciotto pazienti presentavano una tasca o una sacca a livello del setto interventricolare , verosimile espressione di chiusura spontanea del difetto interventricolare ( prevalenza 0 , 66% )  . i reperti della tcms di questi 18 pazienti sono stati correlati con i reperti ecocardiografici . 
il nostro studio dimostra che lincidenza di chiusura spontanea del difetto del setto interventricolare , radiol med ( 2009 ) 114 : 370375 patients initially diagnosed with ventricular diverticula with an apical and marginal septum location may actually have spontaneously closed muscular vsd . 
 keywords cardiac ct heart mdct angiography closed muscular ventricular septal defect introduction ventricular septal defects ( vsds ) are the second most common congenital heart defect after bicuspid aortic valves , but their true rate of incidence is , surprisingly , unknown [ 1 ]  . the incidence rate of vsds among live births is 1.53.5 per 1 , 000 term infants and 4.57.0 per 1 , 000 premature infants [ 2 ]  . the natural history of vsd , including incidence of spontaneous closure ( sc ) , is also uncerta however , some studies have reported the sc rate of vsd to be 48% by 6.9 years ( the mean age ) and 72% in patients without congestive heart failure ( chf ) [ 13 ]  . 
radiologists have begun to interpret coronary artery diseases , and in reporting the results of images obtained for coronary artery disease , they have begun to evaluate nonvascular cardiac structures as well . one of these is sc of muscular vsd observed in the interventricular septu in this study , we describe the experience of our institutions ( two centres ) in using cardiac multidetector ct angiography ( mdcta ) to diagnose sc of muscular vsd . materials and methods the study included 2 , 725 consecutive patients referred to atatrk university hospital and florence nightingale hospital for mdcta . 
in questo modo , alcuni pazienti , ai quali inizialmente era stata fatta diagnosi di diverticoli ventricolari a livello apicale e marginale del setto , in realt possono aver avuto una chiusura spontanea del difetto del setto interventricolare . 
questo risultato pu incidere sulle percentuali precedentemente riportate sia per quanto riguarda i diverticoli ventricolari sia per quanto riguarda la chiusura spontanea del difetto del setto interventricolare . parole chiave tc cardiaca cuore angiografia tcms chiusura del difetto del setto interventricolare disease , congenital malformation , atypical chest pain , screening for coronary artery disease and inconclusive conventional angiography . 
images were reviewed by a radiologist and a cardiologist in consensus , and the following data were recorded : gender , age , degree of coronary artery disease and presence of any other cardiac abnormality . 
similar records for images of the central muscular region to those of the earlier cases ( sc of muscular vsd ) were noted in the apical and marginal areas of the interventricular septuthese cases , with no history of surgery , were evaluated for sc of vsd . however , in the literature , ventricular diverticulum has been reported in all locations of the ventricle wall except 372 radiol med ( 2009 ) 114 : 370375 the interventricular septu in our study , patients with similar lesions in the basal inferoseptal , apical septum and midinferoseptal locations were not included because these lesions could not be differentiated from ventricular diverticula [ 5 , 6 ]  . 
 the procedures used were in accordance with the recommendations found in the declaration of helsinki , and approval of the local ethics committee was obtained . results retrospective electrocardiogram ( ecg ) - gated reconstructions were generated every 10% during the 50%90% of the r - r interval . 
 mdct scan protocol mdct was performed using two different 16 - detector - row ct scanners ( sensation16 , siemens medical systems , forchheim , germany , and aquillon , toshiba medical systems , tokyo , japan ) during one breath - hold ( 1624 s )  . with the first scanner , the following parameters were used : 160.75 - mm collimation , 1 - mm slice thickness and 0.6 - mm reconstruction interval . 
the indications for mdcta were suspected coronary artery disease ( n = 2 , 310 ) , coronary artery anomaly ( n = 22 ) , coronary artery stent patency ( n = 220 ) and coronary artery bypass graft assessment ( n = 173 )  . 
these 18 patients were referred due to indications such as chest pain ( n = 11 ) , risk factor assessment ( n = 3 ) , coronary artery anomaly ( n = 1 ) , suspected aberrant right subclavian artery ( n = 1 ) and coronary artery bypass graft ( n = 2 )  . 
1a - c a 46 - year - old man with spontaneous closure of muscular ventricular septal defect in the interventricular septu multiplanar reformatted multidetector computed tomography angiography ( mdcta ) images from 16 - mdct single - source scanner show long - axis ( a , c ) and short - axis ( b ) views of vsd ( ventricular septal defect ) ( arrows )  . 
le immagini angiografiche con tc a 16 strati mostrano lasse lungo ( a , c ) e lasse corto ( b ) del difetto del setto ventricolare ( frecce )  . 
of vsd location of vsd other abnormalities degree of coronary artery disease radiol med ( 2009 ) 114 : 370375 table 1 patient characteristics . tabella 1 caratteristiche dei pazienti . patient vsd , ventricular septal defect ; lad , left arterial dilatation central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular none moderate none mild none severe moderate none none none mild none mild severe none severe mild none myocardial bridging at lad middle segment aberrant right subclavian artery prior coronary artery bypass grafting aortic valve disease origin of the left circumflex coronary artery from the right sinus of valsalva myocardial bridging at lad middle segment prior percutaneous coronary intervention prior coronary artery bypass grafting ventricular function with no evidence of regional wallmotion abnormalities . 
vsds create a volume load on the left side of the heart secondary to the left - to - right shunt at the ventricular level , causing left atrial and left ventricular dilatation . 
the inlet defect makes up 5%8% of all vsds and is posterior and inferior to the perimembranous defect . muscular vsds make up 5%20% of all vsds [ 7 ]  . 
2a , b immagini assiale ( a ) e sagittale ( b ) del cuore di una donna di 39 anni con chiusura spontanea del difetto del setto interventricolare , che non si pu distinguere dai diverticoli settali a localizzazione apicale . laboratory tests for the diagnosis are not available . 
in the literature , ventricular diverticula have been reported to be located on all the ventricular walls ( apical and marginal septum ) except on the interventricular septum [ 5 ]  . 
nevertheless , similar appearances were observed in the apical and marginal septum as well . because they could not be differentiated from ventricular diverticula , these patients were excluded from the study . 
naturally , this finding may affect previously reported rates of both ventricular diverticula and the incidence of sc of muscular vsd . this will negatively affect the incidence rates of ventricular diverticula reported in earlier studies . 
it appears that there is a very high incidence of asymptomatic small muscular vsds that close spontaneously . isolated ventricular noncompaction is another entity that should be considered in the differential diagnosis . 
diagnosis of ventricular noncompaction usually requires the finding of more than three deep intertrabecular recesses [ 11 , 12 ]  . other pathologies that should be differentiated from sc muscular vsd are other causes of acquired ventricular aneurysms : those that occur after myocardial infarction , myocardial inflammatory disease such as sarcoidosis or myocarditis , infectious endocarditis or trauma [ 13 ]  . 
additional causes of ventricular aneurysm include connective tissue disease and ventricular dysplasia , as seen in patients with arrhythmogenic right ventricular cardiomyopathy . often , the distinction between fibrous ventricular diverticula and these entities can be made only with knowledge of cardiac history and visualisation of an associated abnormalitye.g. 
the true incidence of muscular vsd may have been underreported in the literature because of limitations inherent in the previously available imaging techniques and differences in the patient populations studied . 
because cardiac mdcta is frequently performed in patients with symptoms of chest discomfort , and because chest pain may be a signal of a cardiac abnormality , the incidence of sc muscular vsd is probably higher in this population than in the general asymptomatic population . however , in our study , a higher incidence of sc muscular vsd was shown in a large patient population . 
at our institutions , almost all of the cardiac mdcta studies are prospectively interpreted by two reviewers in consensus to generate an official report , and most reports are generated by two of the most senior reviewers . 
second , although a strict criterion consistent with the pathologic description of muscular vsd was chosen for the identification of this entity , pathologic proof of diagnosis was not obtained in any of our patients . 
however , given that the true prognostic implication of muscular vsd is unknown and that treatment of this entity is controversial , there is no indication to pursue an invasive procedure to confirm the diagnosis in these patients . in summary , this study shows that the incidence of sc muscular vsd with central septum location is probably higher than expected . 
3 immagine assiale del cuore di un uomo di 52 anni con chiusura spontanea del difetto del setto interventricolare , che non si pu distinguere dai diverticoli settali a localizzazione basale . this study has some limitations . 
dwi with adc mapping provides functional information on fetal renal parenchyma development and may thus become a useful tool in the management of pregnancy and treatment of the newborn child . 
abbiamo studiato con esame rm 88 feti ( et gestazionale 1740 settimane ) , gi valutati con esame ecografico che escludeva malformazioni del tratto urinario . lapparato urinario fetale stato studiato con sequenze t2 pesate ultraveloci ; successivamente sono state acquisite sui reni fetali sequenze dwi ( con calcolo automatico delle mappe di adc ) ed i valori di adc messi in relazione con let gestazionale , suddividendo i feti in sei gruppi in base allet gestazionale . 
abbiamo riscontrato che i valori di adc , compresi fra 0 , 99 e 1 , 6210 - 3 mm2 / s ( media 1 , 22 ; 95% ci 1 , 191 , 25 ; deviazione standard 0 , 147 ) tendono a decrescere con laumentare delle settimane di gestazione . 
le sequenze dwi ed le mappe di adc , fornendo informazioni funzionali sullo sviluppo del parenchima renale fetale , risultano di grande utilit soprattutto nella gestione della gravidanza e nel management post - natale . 404 radiol med ( 2009 ) 114 : 403413 keywords fetus mri kidney diffusion adc parole chiave feto risonanza magnetica rene diffusione adc introduction introduzione prenatal ultrasound is the imaging modality of choice in the study of fetal anatomy , although its accuracy may be limited by pathological fetal conditions such as anhydramnios , oligohydramnios and complex malformations as well as maternal conditions such as obesity [ 17 ]  . 
magnetic resonance ( mr ) imaging provides a detailed morphological study of the fetal renal system anatomy as well as allowing assessment of possible urinary tract disorders , which may be isolated or associated with abnormalities of other organs or systems , especially of the gastrointestinal tract or lungs [ 810 ]  . prior to the introduction of ultrafast sequences [ 11 , 12 ] , the use of diffusion - weighted imaging ( dwi ) , which is extremely sensitive to motion , was confined to neuroradiology [ 13 ]  . 
in recent years , researchers have suggested the possibility of using dwi sequences with calculation of the apparent diffusion coefficient ( adc ) of water in the human kidney for the study of renal function in adults [ 16 , 17 ]  . the aim of our study was to apply dwi sequences to the study of the fetal kidney in order to verify the existence of a correlation between adc maps and gestational age in normal fetuses , as such additional functional information would be useful in the event of suspected urinary system abnormalities . materials and methods patients between june 2005 and april 2008 , 85 pregnant women with 88 fetuses ( gestational age 1740 weeks , mean 28 weeks ; maternal age 1844 years , mean 29 years ) were consecutively evaluated with mr imaging . 
patients had previously undergone obstetric ultrasound examination performed with aloka prosound ssd - 5500 equipment by one of three gynaecologists with > 10 years experience at the department of gynaecology and obstetrics of our teaching hospital . the clinical indications for the mr study were diverse , but in no case was there a suspicion of urinary tract malformations . 
in particular , the fetal organs with suspected malformations to be confirmed by mr imaging were the lultrasonografia pre - natale rappresenta limaging di prima scelta nello studio dellanatomia fetale , ma la sua accuratezza pu essere limitata da condizioni patologiche fetali , quali anidramnios , oligoidramnios , sindromi malformative complesse e condizioni di pertinenza materna , come lobesit [ 17 ]  . 
la rm consente un dettagliato studio morfologico dellanatomia fetale , con riguardo al tratto urinario , ma anche una valutazione delle eventuali patologie del tratto urinario stesso che possono presentarsi in forma isolata o associate ad anomalie di altri organi o apparati , soprattutto del tratto gastrointestinale e dei polmoni [ 810 ]  . prima del perfezionamento delle sequenze ultraveloci [ 11 , 12 ] , le sequenze pesate in diffusione , che sono estremamente sensibili al movimento , venivano utilizzate esclusivamente lavvento in neuroradiologia [ 13 ] ; con dellimaging ultrafast invece , la loro applicazione stata di molto ampliata [ 14 , 15 ]  . 
negli ultimi anni alcuni autori hanno prospettato la possibilit di utilizzare le sequenze rm pesate in diffusione ( dwi ) nello studio della funzionalit renale delladulto , calcolando il coefficiente di diffusione apparente dellacqua ( adc ) nel rene umano [ 16 , 17 ]  . il nostro scopo quello di applicare le sequenze dwi allo studio del rene fetale , per valutare lesistenza di una correlazione fra coefficiente di diffusione apparente ( mappe di adc ) ed et gestazionale nei feti sani ; tale dato rappresenta infatti unulteriore informazione , di tipo funzionale , utile soprattutto nel sospetto di patologia del tratto urinario . materiali e metodi pazienti da giugno 2005 ad aprile 2008 , abbiamo valutato in successione , mediante esame rm , 85 donne in gravidanza , con 88 feti ( et gestazionale 1740 settimane di amenorrea , media 28 settimane ; et materna range 1844 anni , media 29 anni )  . 
le pazienti erano gi state sottoposte ad esame ecografico ostetrico eseguito con apparecchio aloka prosound ssd - 5500 , da uno di tre ginecologi con esperienza decennale , del dipartimento di ginecologia ed ostetricia del nostro policlinico . 
in particolare gli organi sui quali pendeva il sospetto di malformazioni , da confermare con rm , erano : encefalo , cuore , distretto toracoaddominale per la presenza di ernie intestinali transdiaframmatiche , oppure vi era evidenza clinica di infezione materna da cmv o , ancora , esisteva il dato anamnestico di precedenti radiol med ( 2009 ) 114 : 403413 brain , the heart and the thoracoabdominal regions due to the presence transdiaphragm intestinal herniations . 
other included clinical evidence of maternal indications cytomegalovirus ( cmv ) infection or a history of previous pathological pregnancies ( spina bifida , genetic syndrome )  . patients were divided into six groups according to gestational age at the time of the mr examination . 
in particular , the following groups were defined : group a : 8 fetuses of 1720 weeks group b : 19 fetuses of 2124 weeks group c : 21 fetuses of 2528 weeks group d : 20 fetuses of 2932 weeks group e : 17 fetuses of 3336 weeks group f : 3 fetuses of 3740 weeks informed consent was obtained from the all patients prior to the examination , and the study was approved by the hospitals ethics committee . mr imaging mr imaging was performed using a superconducting 1.5tesla magnet ( siemens magnetom avanto ) with a phasedarray coil placed over the mothers pelvis . 
the multiplanar study of the urinary system was acquired by using the following : t2 - weighted halffourier single - shot turbo spin - echo ( haste ) sequences ( tr 1 , 900 , te 111 , fov 350300 mm , matrix 256256 , slice thickness 4 mm , acquisition time 20 s ) in the fetal axial , coronal and sagittal planes t2 - weighted thick - slab ( cholangiographic ) sequences ( tr 1 , 900 , te 111 , fov 350300 mm , matrix 256256 , slice thickness 4 mm , acquisition time 14 s ) with maximum intensity projection ( mip ) reconstructions , obtained in the fetal coronal plane t1 - weighted gradient - echo fast low - angle shot ( flash ) two - dimensional sequences ( tr / te = 362 / 4.8 , flip angle 70 , fov 350300 mm , matrix 256192 , slice thickness 4 mm , acquisition time 20 s ) were also acquired in the axial and coronal plane to rule out haemorrhage . axial or coronal single - shot echoplanar dwi sequences of the renal kidneys were subsequently acquired in all cases ( tr 8 , 000 , te 90 , ti 185 ms , fov 420300 mm , matrix 192192 , slice thickness 5 mm , total acquisition time 90 s ) with diffusion gradients applied along the three orthogonal directions ( x , y , z )  . 
three b - factor values were applied for each plane ( 0 , 200 and 700 s / mm2 ) ; the number of images acquired with the dwi sequences was 168 , that is , the sum of the images acquired with the three b factors applied in the three directions . 
in particolare si sono definiti i seguenti gruppi : gruppo a : 8 feti fra la 17 e la 20 settimana ; gruppo b : 19 feti fra la 21 e la 24 settimana ; gruppo c : 21 feti fra la 25 e la 28 settimana ; gruppo d : 20 feti fra la 29 e la 32 settimana ; gruppo e : 17 feti fra la 33 e la 36 settimana ; gruppo f : 3 feti fra la 37 e la 40 settimana . ogni esame stato effettuato previo consenso scritto delle donne ; il nostro studio stato approvato da una commissione etica di studi clinici del nostro ospedale . risonanza magnetica lesame rm stato condotto con magnete superconduttore da 1 , 5 tesla ( siemens magnetom avanto ) , utilizzando una bobina phased array , posizionata sulla pelvi materna . 
le pazienti sono state esaminate in posizione supina e non stata effettuata alcuna sedazione , n sulle donne n sul feto . per la localizzazione del feto sono state ottenute in primo luogo immagini di scanogramma multiplanare , poi , durante lesame , ciascuna sequenza servita come scanogramma per la successiva . 
lo studio multiplanare del sistema urinario stato ottenuto utilizzando : sequenze half - fourier single - shot turbo spin - echo ( haste ) t2 pesate ( tr 1900 , te 111 , fov 350300 mm , matrice 256256 , spessore di strato 4 mm , tempo di acquisizione 20 s ) , eseguite sui piani assiale , coronale e sagittale fetali ; sequenze thick slab ( colangiografiche ) t2 pesate ( tr 1900 , te 111 , fov 350300 mm , matrice 256256 , spessore di strato 4 mm , tempo di acquisizione 14 s ) , con successive ricostruzioni mip , eseguite sul piano coronale fetale ; sequenze flash ( fast low angle shot ) 2d gradient - echo t1 pesate ( tr / te = 362 / 4 , 8 , flip angle 70 , fov 350300 mm , matrice 256192 , spessore di strato 4 mm , tempo di acquisizione 20 s ) sui piani assiale o coronale , per escludere la presenza di eventuali emorragie . successivamente , in tutti i casi , sono state acquisite sui piani assiale o coronale dei reni fetali sequenze in diffusione single - shot echo - planare ( tr 8000 , te 90 , ti 185 ms , fov 420300 mm , matrice 192192 , spessore 5 mm , tempo di acquisizione totale 90 s ) con gradienti di diffusione applicati sui tre assi ortogonali ( x , y , z )  . 
sono stati applicati tre b - factor per piano ( 0 , 200 e 700 s / mm2 ) ; il numero di immagini acquisite con le sequenze pesate in dwi in totale di 168 , risultando tale cifra dalla somma delle immagini ottenute con i tre valori del b - factor applicati sui tre assi . 
il tempo di acquisizione totale dellesame rm fetale stato mediamente di 20 minuti ( 1645 min ) ; il tempo di elaborazione totale stato di circa 7 minuti ( 412 min )  . 
evaluation of fetal kidney adc was obtained by placing a region of interest ( roi ) over the renal parenchyma on all of the slices containing renal tissue and then averaging the results . 
normal renal function was confirmed after birth by means of studio dei reni stato effettuato dunque con acquisizione sui tre piani coronale , assiale e sagittale . per la misurazione dei valori di adc sono state selezionate le immagini non alterate da artefatti da movimento ; in 4 casi le sequenze pesate in diffusione risultavano alterate per artefatti da movimento in corso di acquisizione e sono state ripetute per la seconda volta al fine di ottenere immagini ottimali per il calcolo del valore di adc ; in un solo caso , non preso in considerazione nel nostro studio , non siamo riusciti ad ottenere immagini utili per calcolare il valore di adc . 
coronal t2 - weighted image ( a ) , diffusion - weighted image ( b ) and corresponding apparent diffusion coefficient ( adc ) map ( c ) , with regions of interest covering the entire area of the renal parenchyma . 
la figura mostra acquisizioni coronali sui reni fetali , sui quali sono state posizionate le roi : immagine t2 pesata antomica ( a ) , immagine pesata in diffusione ( b ) e relativa mappa di adc ( c )  . 
il valore medio di adc del parenchima renale in questo caso era di 1 , 5610 - 3 mm2 / s . radiol med ( 2009 ) 114 : 403413 fig . 
axial t2 - weighted image ( a ) , diffusion - weighted image ( b ) , and corresponding apparent diffusion coefficient ( adc ) map ( c )  . 
il miglior risultato stato espresso dallequazione di regressione : adc ( mm2 / s ) = 1 , 690 , 0169 ( eg ) ( r2 = 37 , 7% , r2 adj = 37 , 0% , p < 0 , 005 , correlazione di pearson = 0 , 614 )  . inoltre bisogna precisare che la correlazione pi significativa fra valore medio di adc ed et gestazionale stata riscontrata nei gruppi b , c , d ed e ( p < 0 , 005 ) ; nel gruppo a non si evidenziata correlazione adc / et gestazionale ( p = 0 , 321 ) , ma questo nel nostro studio pu dipendere dal numero inferiore di feti esaminati in tale epoca gestazionale . 410 radiol med ( 2009 ) 114 : 403413 fig . 
in group a , no correlation between adc and gestational age was identified ( p = 0.321 ) , but this finding may well depend on the small number of fetuses in this group . 
with regard to group f ( 3740 weeks ) , the mean adc values , considered individually , reflect the decreasing trend , but in consideration of the small number of fetuses in the group , this finding lacks statistical significance [ 8 ]  . 
dwi and adc determinations can also be performed in fetuses by using dw echoplanar sequences [ 2022 ] , and they can be used for the study of the urinary system [ 23 , 24 ]  . 
 clearly , fetal studies entail more difficulties than postnatal studies owing to possible artefacts due to maternal or fetal movement , aorta pulsations , lower signal - to - noise ratio and reduced spatial resolution [ 24 ]  . 
in a 3 - year follow - up of fetuses studied with mr imaging with echoplanar sequences , they found no abnormality ( including hearing deficit ) arising as a result of per quanto riguarda il gruppo f ( 3740 settimane ) i valori medi di adc riscontrati , considerati singolarmente sono in accordo allandamento decrescente , ma dato il numero esiguo di feti esaminati non hanno un valore statisticamente significativo [ 8 ]  . 
 discussione la rm considerata la sola metodica valida per calcolare la diffusione molecolare in vivo attraverso la misura del movimento browniano delle molecole dacqua in un tessuto . i valori di adc del parenchima renale , sono condizionati sia dal suddetto movimento browniano dellacqua , ma anche da altri fattori , quali la perfusione nella rete capillare e il flusso tubulare . 
le immagini pesate in diffusione e le determinazioni dei valori di adc sono realizzabili anche nei feti , utilizzando sequenze ecoplanari pesate in diffusione [ 2022 ] e possono essere sfruttate per lo studio del tratto urinario [ 23 , 24 ]  . certamente lo studio fetale comporta maggiori difficolt rispetto a quello post - natale , per i possibili artefatti da movimento materni e fetali , per la pulsatilit dellaorta e per il pi basso rapporto segnale - rumore e la minore risoluzione spaziale [ 24 ]  . 
 [ 26 ] noted that dwi sequences have considerably ( approximately six times ) lower specific absorption rates ( sar ) when compared with the t2 sequences used in fetal studies and may therefore be considered harmless for the fetus . 
in 2005 , gubhaju and black [ 27 ] proposed a functional estimate of fetal renal parenchyma on the basis of the morphological information provided by t2 - weighted sequences . 
they noted the existence of a positive linear correlation between fetal renal diameters and gestational age and suggested that this information may be useful not only for monitoring normal renal development but also for predicting possible renal function renal size being correlated with the number of nephrons . 
quantification of the mean adc value , in relation to gestational age , is a truly functional parameter that can help define normal renal function . in agreement with the recent literature [ 23 , 24 ] , in our series of fetuses without urinary system abnormalities , we observed a change in adc values in relation to gestational age and , in particular , the tendency of adc to decrease with increasing gestational age . 
this has been related to the development of the renal parenchyma ( increase in the number and size of nephrons , the functional unit of the kidney ) and hence to other contributing age - related factors , such as blood flow , tubular flow , water content or cell density [ 24 ]  . 
renal blood flow amounts to 2%4% of cardiac output during fetal life as against 20% in adult life [ 28 ]  . we must acknowledge some limitations to our study . 
in addition , it is worth noting that dwi sequences and related adc values have the sole aim of providing an indication of the correct development and normal functioning of the fetal kidney . 
in the event of abnormal findings , dwi with adc is unable to guide the diagnosis with regard to the nature of the kidney disease . this is , instead , achieved with ultrafast t2 sequences , which definitely have better spatial and contrast resolution and consequently excellent anatomical definition [ 29 ]  . however , the anatomical information offered by t2weighted sequences is complemented by the functional information provided by dwi , which allows identification of residual renal parenchyma [ 30 ] and assessment of whether its development , in relation to the adc values , reflects that expected for the fetuss gestational age . sequenze pesate in diffusione presentano un tasso di assorbimento specifico ( sar : specific absorption rates ) molto pi basso ( circa sei volte inferiore ) se comparato alle sequenze t2 pesate utilizzate nello studio fetale e dunque queste possono essere considerate innocue per i feti . 
nel 2005 , gubhaju e black [ 27 ] hanno proposto una stima di tipo funzionale del parenchima renale fetale in base al dato morfologico emergente dalle sequenze t2 pesate . 
costoro infatti hanno notato lesistenza di una correlazione positiva di tipo lineare fra diametri renali fetali ed et gestazionale ipotizzando che tale dato sia utile non solo per monitorare il normale sviluppo renale , ma anche per prevedere la possibile funzionalit renale , essendo le dimensioni dei reni correlate al numero di nefroni . 
la misura quantitativa del valore medio di adc , riferito a ciascuna et gestazionale , rappresenta un reale parametro funzionale utile a definire la normale funzionalit dei reni . in accordo con la recente letteratura [ 23 , 24 ] , nella nostra serie di feti , tutti senza anomalie del tratto urinario , abbiamo notato lesistenza di una variazione dei valori di adc con let gestazionale , in particolare emersa la tendenza di questi a decrescere con lavanzare delle settimane di gestazione : ci stato posto in relazione allo sviluppo parenchimale renale ( aumento del numero e delle dimensioni dei nefroni che rappresentano lunit funzionale del rene ) , e quindi a fattori concorrenti anchessi variabili con let gestazionale , quali il flusso ematico , il flusso tubulare , il contenuto dacqua o la densit cellulare [ 24 ]  . 
inoltre va ricordato che le sequenze pesate in dwi e i relativi valori di adc hanno il solo scopo di orientare circa il corretto sviluppo e dunque il normale funzionamento dei reni fetali , ma nelleventualit di un dato anomalo non consentirebbero di orientare la diagnosi di natura della nefropatia , che invece affidata alle sequenze t2 pesate ultraveloci , le quali sono sicuramente caratterizzate da una migliore risoluzione spaziale e di contrasto e dunque da uneccellente definizione anatomica [ 29 ]  . 
accanto al dato anatomico delle sequenze t2 pesate tuttavia le dwi forniscono il dato funzionale consentendo innanzitutto di identificare la presenza di parenchima renale residuo [ 30 ] e di valutare se il suo sviluppo , in rapporto ai valori di adc , in accordo con i valori attesi per let gestazionale . 412 conclusions conclusioni radiol med ( 2009 ) 114 : 403413 although our study is preliminary and further research on larger populations is needed , we believe that dwi sequences should be considered a useful adjunct to conventional t2 - weighted ultrafast imaging in the study of the fetal kidneys . 
midiri3 1dipartimento di radiologia e dipartimento cardio - polmonare , imaging cardiovascolare non invasivo , azienda ospedaliera di parma , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dibimel , sezione di scienze radiologiche , universit di palermo , palermo , italy 4dipartimento di radiologia , universit degli studi di verona , verona , italy 5dipartimento di radiologia , universit degli studi di trieste , trieste , italy correspondence to : f . 
cademartiri , viale rustici 2 , 43100 parma , italy , tel . : + 39 - 052 - 1961833 , e - mail : filippocademartiri@hotmail.com received : 8 august 2007 / accepted : 25 october 2007 / published online : 14 april 2009 springer - verlag 2009 abstract purpose . 
lm dimensions ( length , ostial and bifurcation diameters ) , quantitative [ location , hounsfield unit ( hu ) attenuation ] and qualitative ( composition , shape ) analysis of plaques within the lm were performed . 
stato esaminato un gruppo di 62 pazienti consecutivi ( 41 uomini , et media 6011 ) sottoposti ad ac - tcms con scanner a 64 strati per sospetta malattia aterosclerotica coronarica . 
sono state misurate le dimensioni del tcs ( lunghezza , diametri allostio ed alla biforcazione ) , nonch stata effettuata unanalisi quantitativa ( sede , densit hu ) e qualitativa ( composizione , forma ) delle placche in esso presenti . 
la ac - tcms mette in evidenza aspetti fondamentali del carico aterosclerotico del tcs dal momento che la rottura e la conseguente trombosi delle placche vulnerabili possono svilupparsi a partire da lesioni non significative alla acc . parole chiave coronaropatia aterosclerotica tronco comune sinistro tomografia computerizzata multistrato tc 64 strati placca vulnerabile introduction introduzione the distribution of fissured or rupture - prone plaques is known to be nonuniform throughout the coronary tree . histopathological and angiographic studies suggest that atheromas with a thin fibrous cap and necrotic lipid core at a high risk of rupture are not frequently encountered in the left main ( lm ) branch and the distal tracts of the coronary arteries [ 13 ]  . 
intravascular ultrasonography ( ivus ) has in fact shown that plaque fissuring rarely occurs in the lm or the distal tracts of the coronary arteries , whereas it is much more common in the proximal tract [ 4 ] , particularly the left anterior descending ( lad ) coronary artery [ 5 ]  . 
the nonuniform distribution of coronary atherosclerosis , with emphasis on the varying lipid content of the plaques , has recently been confirmed by studies with ivus [ 8 , 9 ]  . a number of studies have highlighted the ability of multidetector - row computed tomography ( mdct ) coronary angiography ( ca ) to distinguish between calcified , noncalcified and mixed plaques on the basis of the different attenuation values of each structure [ 10 , 11 ]  . 
the aim of our study was to quantify the coronary atherosclerotic burden of the lm and its bifurcation in a consecutive series of patients la distribuzione delle placche fissurate o prone alla rottura conosciuta non essere uniforme in tutto lalbero coronarico . 
studi istopatologici ed angiografici suggeriscono che gli ateromi con cappuccio sottile e core lipidico necrotico ad alto rischio di rottura non sono frequenti nel tronco comune sinistro ( tcs ) e nei tratti distali delle arterie coronarie [ 13 ]  . 
lecografia intravascolare ( ivus ) ha , infatti , mostrato che la fissurazione delle placche avviene raramente nel tcs o nel tratto distale delle arterie coronarie , mentre molto pi comune riscontrarla nel tratto prossimale [ 4 ] , specialmente nellinterventricolare anteriore ( iva ) [ 5 ]  . tuttavia , la ragione del perch placche vulnerabili o fissurate tendano a risparmiare il tcs ed i segmenti distali delle arterie coronarie sinistre non ancora nota . 
la distribuzione non uniforme dellaterosclerosi coronarica , con attenzione al differente contenuto lipidico delle placche , stata gi confermata da recenti studi condotti con ivus [ 8 , 9 ]  . diversi lavori mettono in evidenza le capacit della angiografia coronarica con tc multistrato ( ac - tcms ) nel distinguere tra placche calcifiche , non calcifiche e di aspetto misto , basandosi sulla diversa attenuazione dei raggi x di ciascuna struttura [ 10 , 11 ]  . 
the scan and reconstruction parameters were : number of detectors / collimation 322 / 0.6 mm , gantry rotation time 330 ms , feed / rotation 3.84 mm ( pitch 0.2 ) , kvp 120 , mas 900950 , field of view 150 mm , effective slice thickness 0.75 mm , reconstruction increment 0.4 mm and convolution kernels b30f and b46f . 
a 100 - ml bolus of nonionic iodinated contrast material ( iomeprol 400 mgi / ml , iomeron , bracco , italy ) was intravenously administered with antecubital access at a flow rate of 5 ml / s , followed by a bolus chaser of 40 ml of physiological solution at the same injection rate . 
the available reconstructions were examined with all the conventional postprocessing techniques [ native axial images , multiplanar reconstructions ( mpr ) , curved multiplanar reconstructions ( cmpr ) , maximum intensity projections ( mi ) p and volume rendering ( vr ) ]  . 
a semiquantitative analysis of the following lm characteristics was performed : length and diameter at the ostium and bifurcation , presence of atherosclerotic plaques ( at least 1 - mm thick ) , their position and involvement of the bifurcation , extension , eccentric development ( up to two thirds of the vessel circumference ) or concentric development ( covering 360 of the vessel circumference ) , composition ( calcified , noncalcified or mixed ) and density in hounsfield units ( hu )  . 
a quantitative analysis of the thickness ( vessel diameter vessel lumen ) and the area ( vessel area lumen area ) of the plaques visualised in the axial sections of the vessel was performed . 
in questo contesto , i dati sono stati correlati con le caratteristiche dimensionali del tcs . materiali e metodi un gruppo di 62 pazienti consecutivi ( 41 uomini , 21 donne , et media 6011 anni ) sottoposti ad ac - tcms per patologia coronarica nota o sospetta stato retrospettivamente esaminato per la valutazione del carico aterosclerotico nel tcs ed alla sua biforcazione . 
i parametri di scansione e ricostruzione sono : numero di detettori / collimazione 322 / 0 , 6 mm , tempo di rotazione del tubo radiogeno 330 ms , avanzamento / rotazione 3 , 84 mm ( pitch 0 , 2 ) , kvp 120 , mas 900950 , campo di vista 150 mm , spessore effettivo dello strato 0 , 75 mm , incremento di ricostruzione 0 , 4 mm , filtri di convoluzione b30f e b46f . 
stato somministrato per via endovenosa antecubitale un bolo di mezzo di contrasto iodato non ionico ( iomeprol 400mgi / ml , iomeron , bracco , italia ) da 100 ml ad una velocit di 5 ml / s seguito da un bolo da 40 ml di soluzione salina alla stessa velocit . 
per la somministrazione del mezzo di contrasto stato utilizzato un iniettore automatico a doppia testa ( stellant , medrad , usa )  . due radiologi con elevata esperienza in ac - tcms ( livello 3 ) [ 12 ] hanno esaminato su una stazione di lavoro dedicata ( leonardo , siemens , germania ) le caratteristiche del tcs . 
le ricostruzioni disponibili sono state valutate con tutte le convenzionali tecniche di post processing ( immagini assiali , ricostruzioni multiplanari - mpr , ricostruzioni multiplanari curve - cmpr , proiezioni di massima intensit - mip , e volume rendering - vr )  . 
stata effettuata unanalisi semiquantitativa delle caratteristiche seguenti del tcs : lunghezza e diametri allostio ed alla biforcazione , eventuale presenza di placche aterosclerotiche ( con almeno 1 mm di spessore ) , loro posizione e coinvolgimento della biforcazione , estensione , sviluppo eccentrico ( fino a 2 / 3 della circonferenza vaso ) o concentrico ( sui 360 della circonferenza del vaso ) , composizione ( calcifiche , non calcifiche o miste ) e densit in unit hounsfield ( hu )  . 
stata , altres , effettuata unanalisi quantitativa dello spessore ( diametro vasodiametro lume ) e dellarea ( area vaso - area lume ) delle placche presenti visualizzate nella sezione assiale del vaso . tutti i pazienti sono stati sottoposti ad angiografia coronarica convenzionale ( acc )  . 
i filmati sono stati poi analizzati da un operatore in cieco con un software radiol med ( 2009 ) 113 : 358369 the study population was divided into two groups on the basis of the presence ( n = 30 ) or absence ( n = 32 ) of plaques in the lm . 
vessel dimensions ( length and diameter at the ostium and bifurcation ) and plaques were correlated with the pearson test . quantitativo ( caas , pie medical , olanda )  . 
un valore 50% indica una stenosi significativa . la nostra popolazione stata suddivisa in due gruppi di pazienti sulla base della presenza ( n = 30 ) o meno di placche ( n = 32 ) nel tcs . 
the plaques prevalently involved the distal tracts of the lm ( 69% ) , the bifurcation ( 71% ) and the ostial tracts of the lad ( 57% ) and the left circumflex coronary artery ( lcx ) ( 31% )  . 
mpr in sezione che evidenziano una placca non calcifica non significativa e ne consentono un analisi semiquantitativa ( c , d )  . radiol med ( 2009 ) 113 : 358369 fig . 
3a - d conventional coronary angiography ( ca ) displays a significant lesion ( arrowhead ) at the ostium ( a )  . multiplanar reconstruction ( mpr ) using multidetector - row computed tomography ca : visualisation and length measurement of the left main ( lm ) coronary artery ( b )  . 
a moderate correlation ( r = 0.56 ) was found between lm diameter at the bifurcation ( mean diameter 6.31.3 mm ) and the corresponding plaque area ( mean area 20.8 mm2 ) in patients with plaques at the bifurcation ( n = 25 )  . 
most of these plaques were eccentric ( n = 20 , 80% ) , with a variable composition ( eight calcified , 12 mixed , five noncalcified ) , frequently ( 80% ) involving the proximal tracts of the lad or lcx . 
in ten patients ( 16% ) with nonsignificant atherosclerotic plaques ( < 50% of the lumen ) at mdct , conventional ca identified the presence of vessel wall irregularities of the lm . 
in the remaining 49 patients ( 79% ) , conventional ca identified a healthy lm , whereas mdct detected nonsignificant atherosclerotic lm plaques in 19 of these patients ( 31% )  . ( 71% ) ed i tratti ostiali dellarteria interventricolare anteriore ( 57% ) e della circonflessa ( 31% )  . 
le placche riscontrate presentavano estensione media di 54 mm , spessore medio di 20 , 8 mm , ed area media 1 , 80 , 9 mm2 . i diametri misurati allostio ed alla biforcazione del tcs erano significativamente aumentati nei pazienti con placche aterosclerotiche ( p < 0 , 05 )  . 
una correlazione moderata ( r = 0 , 56 ) stata riscontrata tra il diametro del tcs alla biforcazione ( diametro medio 6 , 31 , 3 mm ) e la corrispondente area della placca ( area media 20 , 8 mm2 ) dei pazienti con placche alla biforcazione ( n = 25 )  . 
tali placche si presentano nella maggior parte dei casi eccentriche ( n = 20 , 80% ) , con composizione variabile ( 8 calcifiche , 12 miste , 5 non calcifiche ) , coinvolgendo frequentemente ( 80% ) i tratti prossimali della iva o della circonflessa . 
visualisation of noncalcified plaque is limited to the size of the plaque and the size of the vessel , with greater accuracy when the analysis is limited to the proximal segments [ 10 ]  . 
noncalcified plaques were more frequently encountered in the first group , and as such , the severity of atherosclerosis is underestimated if calcified plaques only are taken into consideration [ 15 ]  . 
nei rimanenti 49 pazienti ( 79% ) la acc ha evidenziato un tcs indenne , mentre la ac - tcms ha dimostrato in 19 di questi ( 31% ) placche aterosclerotiche non significative del tcs . discussione la visualizzazione delle placche aterosclerotiche coronariche rappresenta una delle sfide pi recenti per la ac - tcms , nel tentativo di giungere a quella caratterizzazione tessutale che la acc non in grado di effettuare . 
la malattia aterosclerotica progredisce verso la stenosi clinicamente significativa con un carico crescente di placche , in principio non calcifiche , che scatenerebbero gli eventi acuti [ 6 , 7 , 13 ]  . 
la tc in virt della capacit di attribuire valori numerici di densit in hu alle strutture esaminate sembrerebbe il metodo di imaging ideale per visualizzare e quantificare i componenti della placca aterosclerotica che langiografia non riesce ad apprezzare [ 14 ]  . 
la visualizzazione delle placche non calcifiche limitata dalle dimensioni della placca e del vaso , con una migliore accuratezza quando si restringe lanalisi ai segmenti prossimali [ 10 ]  . 
 [ 15 ] hanno dimostrato una sostanziale differenza di composizione tra le placche dei pazienti con ima e quelle dei pazienti radiol med ( 2009 ) 113 : 358369 plaques in patients with acute ischemic events have a lower mean density than those in patients with stable angina [ 16 ]  . 
nonetheless , according to the most recent evidence , the attenuation values measured in hu within the plaque seem to be influenced by the intravascular attenuation and the convolution kernel used . 
used ivus to verify whether the distance of the plaque from the ostium influences plaque composition in terms of necrotic lipid content and therefore whether this is relevant to plaque fissuring [ 8 ]  . 
a later study by the same group clarified how the composition of plaques in the lm and the distal tracts is similar , whereas plaques in the proximal tracts of the coronary arteries are characteristically more vulnerable , with a necrotic lipid core . 
this core is greater in patients with acute coronary syndromes and is weakly associated with high levels of high - density lipoprotein ( hdl ) cholesterol , although there was no correlation with inflammatory markers . 
in patients with a short lm , the lipid cores tend to be concentrated between the bifurcation and the proximal tracts of the coronary arteries , whereas in patients with a long lm , they tend to appear more proximally , prior to the proximal coronary artery tracts [ 9 ]  . in light of these considerations , in our study , we described the presence of atherosclerosis in the lm correlated with vessel dimensions ( length , diameter ) using 64 - mdct and evaluated the characteristics of the atherosclerotic plaques present with a semiquantitative method . the length of the lm is commonly about 12 cm , even though it is frequently shorter and more rarely longer . 
a recent study demonstrated that measurements of the proximal diameters of the proximal coronary arteries at mdct are well correlated with measurements made with ivus and conventional ca [ 20 ]  . 
plaque distribution may be determined by anatomical factors that influence the shear stress ( length of the lm , diameters of the ostium and the bifurcation ) , by the lipid profile and by inflammatory con angina stabile . 
al riguardo i dati presenti in letteratura concordano : le placche dei pazienti con evento ischemico acuto hanno densit media minore di quella dei pazienti con angina stabile [ 16 ]  . 
 [ 8 ] hanno inizialmente verificato mediante icus come la distanza della placca dallostio sia un fattore determinante sulla composizione della stessa , in termini di contenuto lipidico necrotico , e , quindi , rilevante sulla propensione della stessa alla fissurazione . 
uno studio successivo dello stesso gruppo ha meglio chiarito come la composizione delle placche nel tcs e nei tratti distali sia simile , mentre nei tratti prossimali delle coronarie assuma pi spiccati caratteri di vulnerabilit , caratterizzati da un nucleo lipidico necrotico . 
di converso , un lungo tcs si associa a nuclei lipidici precoci immediatamente entro i tratti prossimali delle coronarie [ 9 ]  . alla luce di queste considerazioni , nel nostro studio abbiamo descritto landamento dellaterosclerosi nel tcs correlata alle dimensioni del vaso ( lunghezza , diametri ) mediante angiografia coronarica con tc a 64 strati e valutato le caratteristiche delle placche aterosclerotiche presenti con un metodo semiquantitativo . 
un recente studio ha dimostrato che le misure dei diametri prossimali delle arterie coronarie prossimali in tcms mostrano unottima correlazione con le misurazioni condotte durante icus ed acc [ 20 ]  . 
 [ 21 ] hanno recentemente confermato che la ac - tcms con 64 strati raggiunge risultati incoraggianti nellidentificazione e caratterizzazione di placche posizionate nei segmenti prossimali [ 21 ]  . 
tale distribuzione potrebbe 366 radiol med ( 2009 ) 113 : 358369 markers ( c - reactive protein , fibrinogen , interleukin - 6 , tumour necrosis factor - alpha )  . 
clearly , with hindsight , the clinical presentation mirrors the plaque typology present [ 9 , 15 ]  . one study reported that the rupture of coronary plaques occurs most frequently in the distal tract of the lm near the bifurcation [ 22 ]  . 
low - oscillation shear stress is known to induce a loss of flow - dependent endothelial dilation , an increase in the expression of adhesion molecules and a weakening of intercellular junctions , which in the end cause an increase in permeability to lipids and macrophages [ 23 ]  . 
due to the turbulence of highvelocity blood flow , which impacts the anatomical essere determinata da fattori anatomici ( lunghezza del tcs , diametri allostio ed alla biforcazione ) , che influenzano lo shear stress , dal profilo lipidico e probabilmente dai marker dellinfiammazione ( proteina c reattiva , fibrinogeno , interleuchina 6 , tnf - )  . 
certamente , a posteriori , la presentazione clinica riflette la tipologia di placche presenti [ 9 , 15 ]  . stato riportato che la rottura delle placche coronariche avviene pi frequentemente nel tratto distale del tcs in prossimit della biforcazione [ 22 ] nella nostra popolazione la maggior parte dei pazienti mostrava placche in questa area , con composizione non calcifica ed eccentricit prevalente . 
lo shear stress a bassa oscillazione conosciuto indurre una perdita del fisiologico allineamento flusso - orientato delle cellule endoteliali , un aumento dellespressione di molecole di adesione ed un indebolimento delle giunzioni intercellulari , che determinano , fig . 
4a - d forma e composizione di placche aterosclerotiche del tcs : placca eccentrica mista ( a ) ; placca non calcifica eccentrica alla biforcazione ( b ) ; placca ostiale calcifica ( c ) ; placca non calcifica alla biforcazione ( d )  . radiol med ( 2009 ) 113 : 358369 structures [ 24 ] , the proximal segments could be more exposed to shear stress [ 25 ]  . 
clearly , a parallel measurement of the shear stress and plaque composition along the vessels needs to be carried out in vivo to confirm these hypotheses . in our study , the plaques proved to be prevalently eccentric , particularly at the bifurcation , confirming the data in the literature [ 9 ]  . although coronary artery bypass grafting surgery is still the recommended first - choice treatment for significant lm stenosis ( 50% of the lumen ) , the introduction of drug - eluting stents with relatively low rates of in - stent restenosis has encouraged the alternative choice of angioplasty with stenting of the lm [ 26 ]  . 
the description of the progression of atherosclerosis in the lm and at the bifurcation is therefore of primary importance in the planning of stent deployment in that it can provide information on the type of stent to be used as well as the precise extent and the placement technique [ 27 ]  . 
i segmenti prossimali potrebbero a causa della turbolenza del flusso di sangue ad alta velocit che impatta contro le strutture anatomiche [ 24 ] essere pi esposti allo shear stress [ 25 ]  . 
nel nostro lavoro le placche risultano prevalentemente eccentriche , in particolare alla biforcazione , confermando il dato presente in letteratura [ 9 ]  . nonostante gli interventi di by - pass aorto - coronarico siano ancora lopzione terapeutica raccomandata per le stenosi significative del tcs ( 50% del lume ) , lintroduzione degli stent medicati ( drug - eluting stents - des ) con tassi di restenosi piuttosto bassi ha incoraggiato la scelta alternativa dellangioplastica del tcs con posizionamento di stent [ 26 ]  . la descrizione dellandamento dellaterosclerosi nel tcs ed alla biforcazione risulta , quindi , di primaria importanza nel planning di uno stent , nella misura in cui fornisce indicazioni sul tipo di stent da utilizzare , sulla sua precisa estensione e sulla tecnica di posizionamento [ 27 ]  . 
la ac - tcms ha raggiunto , allo stesso tempo , notevoli risultati nella valutazione degli stent del tcs nellescludere la restenosi intra - stent , come alternativa di primo livello alla cca [ 28 ]  . esistono , tuttavia , alcune limitazioni nel nostro studio . in primo luogo non stata effettuata una correlazione icus , ma solamente un riscontro acc , che conferma la bassa prevalenza di malattia significativa nel tcs [ 29 ]  . 
allo stato attuale , non vi ancora accordo circa le reali potenzialit della ac - tcms nello stimare le dimensioni delle placche , dal momento che le misurazioni sono senza dubbio influenzate da artefatti da volume parziale e movimento [ 10 ]  . 
la ricerca di un protocollo desame ottimizzato per la valutazione della placca e lo sviluppo di un software , che consenta alloperatore unaffidabile e riproducibile caratterizzazione , potrebbero essere valide soluzioni a queste problematiche . 
una questione da sollevare relativa a tutti gli attuali studi ac - tcms la significativa esposizione del paziente a radiazioni ionizzanti ( 914 msv ) , che ne deve obbligatoriamente limitare luso nei pazienti asintomatici ed in particolare nelle donne al di sotto dei 40 anni [ 30 ]  . conclusions conclusioni plaques in the lm have a specific appearance according to their anatomical location . 
in particolare , la ac - tcms fornisce dettagli anatomici del tcs ed informazioni morfologiche rilevanti circa lestensione dellaterosclerosi coronarica , dal momento che la rottura e 368 radiol med ( 2009 ) 113 : 358369 and consequent thrombosis of vulnerable plaques can develop from lesions characterised as nonsignificant at conventional ca . 
 + 39 - 081 - 5665201 , fax : + 39 - 081 - 5665201 , e - mail : salvatore.cappabianca@unina2.it received : 11 april 2008 / accepted : 28 july 2008 / published online : 11 march 2009 springer - verlag 2009 abstract purpose . 
plain chest radiographs and hrct scans of 42 consecutive patients with ntm pulmonary infection ( m / f 26 / 16 ; mean age 57 , range 4183 ) were retrospectively reviewed . 
abbiamo valutato gli esami rx / tc a strato sottile ( hrct spessore 1 mm / interslice 10 mm ) relativi a 42 casi consecutivi di infezione polmonare da ntmb , insorta in pazienti immunocompetenti ( m / f , 26 / 16 ; et media 57 anni ; range 4183 ) ; abbiamo eseguito il follow - up in 10 casi entro 18 mesi dalla diagnosi . 
la micronodulia ( < 10 mm ) pi frequente della macronodulia , la consolidazione segmentaria della lobare ; le cavitazioni , il tree - in - bud , le bronchiectasie sono pi frequenti nei lobi superiori . 
lhrct consente la corretta identificazione ed il monitoraggio a distanza del pattern che pi frequentemente si riscontra nella localizzazione polmonare dellinfezione : micronodulia diffusa , bronchiectasie , consolidazione segmentaria lobare superiore , cavit . 
although humans are exposed daily to the microorganisms , the incidence of ntm pulmonary infection is low , as the bacteria tend to colonise rather than infect their host [ 7 ]  . 
it is not completely clear whether ntm infection is responsible for the clinical presentation at disease onset , or whether this is a late manifestation of the infection . the most common pathogens causing ntm pulmonary infection are intracellular mycobacterium avium [ no longer distinguished from m . 
predisposing factors for ntm infection include interferon - gamma - deficiency cystic fibrosis , alcoholism , chronic obstructive pulmonary disease ( copd ) , alpha - 1 antitproteinase gene defects , pathological thinness , prior surgery ( especially gastrectomy ) , oesophageal disease and rib - cage anomalies ( pectus excavatum and kyphoscoliosis ) [ 13 ]  . 
the recent increase in the prevalence of ntm infections may therefore be correlated with the reduced incidence of tuberculosis ( tb ) in the general population in industrialised areas [ 9 ]  . 
fever , night sweats , weight loss , lethargy and symptoms related to chronic bronchopulmonary disease are more common in advanced stages of disease , thus making the recognition of the symptoms difficult in patients with underlying pulmonary disease [ 911 ]  . i micobatteri atipici ( ntmb ) sono microrganismi ubiquitari comunemente rinvenuti nellambiente e riconosciuti sempre pi frequentemente come causa di infezione cronica polmonare in soggetti immunocompetenti [ 15 ]  . 
linfezione da ntmb rappresenta lo 0 , 5%30% di tutte le infezioni micobatteriacee e , sebbene luomo sia quotidianamente esposto a tali microrganismi , lincidenza di infezioni polmonari da ntmb bassa perch essi colonizzano pi che infettare lospite [ 7 ]  . linfezione pu essere acquisita per inalazione , ingestione ed inoculazione diretta ; la trasmissione interumana rara [ 8 ]  . 
non del tutto chiaro se linfezione da ntmb sia responsabile di quadri patologici respiratori ab initio , ovvero se questi rappresentino una manifestazione tardiva della stessa . i patogeni pi frequentemente riscontrati come causa di infezioni polmonari micobatteriacee non tubercolari sono m . 
deficit di inf , fibrosi cistica , alcolismo , patologie croniche ostruttive polmonari , difetti genici dell1 - antiproteinasi , magrezza patologica , interventi chirurgici ( in particolare gastrectomia ) , patologie esofagee ed anomalie della gabbia toracica ( pectus excavatum e cifoscoliosi ) possono costituire fattori predisponenti alle infezioni da ntmb [ 13 ]  . 
lesposizione al bacillo tubercolare ed il vaccino antitubercolare con bcg possono dare unimmunit crociata con i micobatteri ; il recente incremento della prevalenza di tali infezioni potrebbe correlare , dunque , con la riduzione dellincidenza di tubercolosi nella popolazione generale delle aree industrializzate [ 9 ]  . 
febbre , sudorazione notturna , perdita di peso , letargia , sintomi spesso legati a broncopneumopatie croniche , sono pi comuni nelle fasi avanzate di malattia rendendo difficile , pertanto , il riconoscimento dei sintomi legati alle micobatteriosi in pazienti con patologia polmonare soggiacente [ 911 ]  . immunocompetent patients affected by mycobacterial i pazienti immunocompetenti affetti dalle micobatteriosi 378 radiol med ( 2009 ) 114 : 376389 infection can be divided into two groups : ( 1 ) adult males with preexisting chronic pulmonary disease such as copd and fibrosis [ 12 , 1416 ] and ( 2 ) young females without evident pulmonary disease or concomitant systemic disease [ 1416 ]  . 
nel primo gruppo la patologia tende a presentarsi in forma classica , ovvero in maniera quasi indistinguibile dalla forma attiva della tubercolosi ; nel secondo , invece , si riscontra , nella maggior parte dei casi , una forma non classica . 
 scopo del nostro lavoro stato quello di definire , analizzandoli retrospettivamente , i reperti hrct pi frequenti e significativi per la diagnosi di micobatteriosi polmonare atipica , correlando il dato tc con i reperti radiografici e levoluzione clinica della malattia . materials and methods we retrospectively reviewed the radiographic and hrct examinations performed between january 2004 and december 2007 on 42 immunocompetent patients ( m / f 26 / 16 , age range 4183 years ) with a clinical and radiographic suspicion of pulmonary ntm infection that was subsequently confirmed by using the american thoracic society 1997 criteria ( table 1 ) and 2007 criteria for the patients examined in the final year ( table 2 ) [ 11 , 19 ]  . the study included patients who underwent not only clinical and laboratory diagnosis of ntm infection but also radiography and hrct examinations to locate the pulmonary infection . 
nine additional patients were excluded due to bronchogenic carcinoma ( n = 6 ) , sarcoidosis ( n = 1 ) and diffuse interstitial pneumonia ( n = 2 ) because the hrct findings associated with these diseases may coincide and mask the signs of ntm pulmonary infection . 
the terminology recommended by the fleischner society [ 20 , 21 ] was used to define the hrct findings . radiographic and hrct examinations were separately evaluated by two groups of radiologists with equal experience and blinded to each others conclusions . 
radiographic findings correlated with the clinical findings leading to a suspicion of ntm infection included : cavitations , areas of consolidation , diffuse nodular opacities , fibrosis associated materiali e metodi abbiamo valutato retrospettivamente gli esami radiografici e di tc ad alta risoluzione ( hrct ) eseguiti nel periodo gennaio 2004dicembre 2007 relativi a 42 pazienti immunocompetenti ( m / f : 26 / 16 ; range di et 4183 anni ) con sospetto diagnostico clinico e radiografico di micobatteriosi atipica polmonare , successivamente accertato mediante i criteri dellamerican thoracic society del 1997 ( tabella 1 ) e del 2007 per i pazienti esaminati nellultimo anno ( tabella 2 ) [ 11 , 19 ]  . 
 nel nostro studio sono stati inclusi pazienti in cui oltre alla diagnosi clinico - laboratoristica di infezione da ntmb erano stati eseguiti , per dimostrare la localizzazione polmonare dellinfezione , esami radiografici del torace e studi hrct condotti con lutilizzo dei seguenti parametri : slice thickness 1 mm , avanzamento 10 mm e filtro di visualizzazione per osso . 
abbiamo escluso dal protocollo di valutazione tutti i pazienti con hiv , ipogammaglobulinemia , leucemia e quelli in terapia steroidea , in quanto deficit immunitari possono modificare notevolmente limaging delle infezioni polmonari da ntmb ; abbiamo inoltre escluso 9 pazienti perch affetti da carcinoma broncogeno ( n = 6 ) , sarcoidosi ( n = 1 ) , polmonite interstiziale diffusa ( n = 2 ) , poich i segni tc associati a tali malattie possono sovrapporsi ed in parte mascherare i reperti legati a polmonite da ntmb . 
nella definizione dei reperti tc stata impiegata la terminologia raccomandata dalla fleischner society [ 20 , 21 ]  . gli esami radiografici e di hrct sono stati valutati separatamente in cieco da due gruppi di radiologi di pari esperienza . 
allanalisi degli esami rx gli elementi semeiologici , che uniti al quadro clinico , hanno indotto al sospetto di infezione da ntmb sono stati : cavitazioni , aree consolidative , opacit nodulari diffuse , fibrosi associata a perdita di radiol med ( 2009 ) 114 : 376389 table 1 diagnostic criteria 1997 modified for immunocompetent patients only american thoracic society a . 
compatible signs / symptoms ( cough ; fatigue most common ; fever ; weight loss ; hemoptysis ; dyspnea may be present , particularly in advanced disease ) with documented deterioration in clinical status if an underlying condition is present b . 
at least three available sputum / bronchial wash samples within 1 year three positive cultures with negative afb smears , or two positive cultures and one positive afb smear b . 
single available bronchial wash and inability to obtain sputum samples positive culture with 2 + , 3 + , or 4 + growth , or positive culture with a 2 + , 3 + , or 4 + afb smear c . 
tissue biopsy any growth bronchopulmonary tissue biopsy granuloma and / or afb on lung biopsy with one or more positive cultures from sputum / bronchial wash any growth from usually sterile extrapulmonary site for a diagnosis of pulmonary disease , all three criteria : ( 1 ) clinical , ( 2 ) radiographic and ( 3 ) bacteriologic must be satisfied hrct , high - resolution computed tomography ; afb , acid - fast bacillus with volume loss , focal pleural thickening and pleural effusion . 
 hrct findings suggestive of ntm infection included : small nodules ( < 10 mm ) , nodules ( 1030 mm ) , tree - in - bud sign , parenchymal consolidation , cavitation and bronchiectasis . 
 alla tc sono stati ricercati , quali segni suggestivi di infezione da ntmb : micronoduli ( meno di 10 mm di diametro ) ; macronoduli ( diametro compreso tra 1030 mm ) ; tree - in - bud pattern ; consolidazioni parenchimali ; cavitazioni ; bronchiectasie . 
tutti i reperti patologici sono stati categorizzati impiegando precostituiti modelli sinottici al fine di ottenere la maggiore sovrapponibilit delle interpretazioni dei due gruppi di osservatori ; le differenze interpretative sono state risolte in consenso . 
nella definizione di sede delle lesioni abbiamo tenuto in considerazione la suddivisione in lobi dei polmoni , assumendo la lingula come 380 radiol med ( 2009 ) 114 : 376389 tabella 1 criteri diagnostici sec . 
segni / sintomi compatibili ( tosse , astenia , febbre , perdita di peso , emottisi , dispnea possono essere presenti , specie nella malattia in fase avanzata ) con un documentato deterioramento dello stato clinico se presente una condizione sottostante b . 
qualunque dei seguenti reperti allrx del torace ; se precedenti ad un anno , dovrebbe esserci evidenza di progressione infiltrati con o senza noduli ( persistent da pi di 2 mesi o progressivi ) cavitazioni solo noduli ( multipli ) b . 
almeno 3 campioni di espettorato disponibili / campioni di lavaggio bronchiale in un anno tre colture positive con striscio afb negativo o due colture positive ed uno striscio afb positivo oppure b . 
singolo lavaggio bronchiale disponibile ed impossibilit di ottenere campioni di espettorato coltura positiva con crescita 2 + , 3 + , o 4 + oppure coltura positive con striscio afb 2 + , 3 + , o 4 + oppure c . 
biopsia tissutale crescita dal tessuto bioptico broncopolmonare granuloma e / o afb su biopsia polmonare con uno o pi colture positive su espettorato / lavaggio bronchiale crescita da sedi extrapolmonari di solito sterili per la diagnosi di malattia polmonare , tutti e tre i criteri ( 1 ) clinico , ( 2 ) radiografico e ( 3 ) batteriologico devono essere soddisfatti hrtc , tc ad alta risoluzione ; afb , acid - fast bacillus months from diagnosis was possible in ten of the 42 patients after adequate medical treatment . 
in 2 dei 10 pazienti seguiti nel tempo , stato possibile correlare il dato radiologico con quello anatomo - patologico su campioni di lobectomia . among the 42 patients , 23 were affected by m . 
the most common clinical presentations were dyspnoea ( 50% ) , cough ( 46.4% ) , fever ( 42.8% ) risultati dei 42 pazienti inclusi nel nostro studio , 23 erano affetti da infezione da m . 
transbronchial or other lung biopsy with mycobacterial histopathologic features ( granulomatous inflammation or afb ) and positive culture for ntm or biopsy showing mycobacterial histopathologic features ( granulomatous inflammation or afb ) and one or more sputum or bronchial washings that are culture positive for ntm 4 . 
making the diagnosis of ntm lung disease does not , per se , necessitate the institution of therapy , which is a decision based on environmental contamination is firmly established or excluded potential risks and benefits of therapy for individual patients afb , acid - fast bacillus ; ntm , nontuberculous mycobacteria 1 . 
sintomi polmonari , opacit nodular o cavitazioni allrx del torace , o una hrct che mostri bronchiectasie multifocali con multipli tabella 2 criteri diagnostici ats 2007 clinici ( entrambi richiesti ) micronoduli 2 . 
biopsia transbronchiale o polmonare con caratteristiche istologiche da micobatteriosi ( infiammazione granulomata o afb ) e colture positive per ntmb o biopsie che mostrino caratteristiche istologiche da micobatteriosi ( infiammazione granulomata o afb ) ed uno o pi colture di espettorato o lavaggio bronchiale positive per ntmb 4 . 
il quadro clinico di presentazione pi frequentemente riscontrato era costituito da dispnea ( 50% ) , tosse ( 46 , 4% ) , febbre ( 42 , 8% ) ed espettorato ( 39 , 3% ) ; meno spesso emoftoe ( 28 , 6% ) , astenia ( 17 , 8% ) , dimagrimento ( 17 , 8% ) e dolore toracico ( 10 , 7% )  . 
the tree - inbud sign was present in 27 patients ( 40.5% ) , with location in the upper right lobe in seven patients ( 41.2% ) and in the middle lobe and the upper left lobe in five patients ( 29.4% ) ( table 3 )  . all patients were treated with combination therapy consisting of daily isoniazid , rifampin and ethambutol in the m . 
kansasii and 12 months of mac onset . conventional radiology was performed every 6 months , whereas hrct was carried out only after completion of ( 21 , 4% ) , gastroresezione ( 23 , 8% ) e patologia esofagea ( 11 , 9% ) erano quelle maggiormente riscontrate nel nostro gruppo di pazienti . 
3 parenchymal consolidation of the posterior segment of the right upper lobe with thick - walled cavitation associated with extensive bronchiectasis and scattered nodulation in both upper lobes in a patient with m . 
3 consolidazione parenchimale del segmento posteriore del lobo superiore destro con cavitazione a pareti spesse associati ad estesi fenomeni bronchectasici e nodulazioni sparse in entrambi i lobi superiori in paziente con infezione da m . 
due pazienti mostravano un quadro hrct sostanzialmente invariato ed in altri 2 si avuta resistenza alla terapia medica con progressione della patologia dimostrata dallaumento di estensione delle lesioni pre - esistenti e / o dalla comparsa di nuove lesioni cavitate , bronchiectasie , tree - in - bud e micronoduli , reperti che hanno reso necessario il ricorso alla terapia chirurgica . 
in two others , the infection was refractory to medical treatment , with disease progression demonstrated by the increase in the extension of preexisting lesions and / or the appearance of new cavitations , bronchial dilatation , tree - in - bud and small nodules . 
these findings led to surgical treatment , and gross pathology on the resected specimens showed a close correlation with the radiological findings . discussion the insidious nature of ntm pulmonary infections has been underlined in many studies . 
the symptoms can be underestimated for months or even years prior to diagnosis , especially in patients with preexisting pulmonary disease [ 9 ]  . dyspnoea , cough , expectoration and fever were the most common signs and symptoms in our patient population . 
the nonspecific nature of these signs and symptoms , which are often present in advanced chronic bronchopulmonary disease , confirm the diagnostic difficulties that can be nei pazienti con patologie polmonari preesistenti [ 9 ]  . dispnea , tosse , espettorato e febbre , sintomi e segni aspecifici , sono stati i pi frequenti nellambito del gruppo di pazienti selezionati per il nostro studio ; la aspecificit di tali sintomi e segni , che spesso sono presenti nelle broncopneumopatie croniche avanzate , confermano le difficolt di inquadramento diagnostico che possono verificarsi in pazienti affetti da polmoniti da ntmb . 
alcuni pazienti mantengono un quadro clinico e radiografico stabile per lungo tempo , mentre altri hanno una rapida progressione della malattia , che senza terapia opportuna , tende a risultare fatale . nella nostra casistica le micobatteriosi atipiche di pi frequente riscontro sono state quelle sostenute da m . kansasii e da mac e , nellambito della coorte di pazienti esaminati , in accordo con i dati presenti in letteratura , abbiamo potuto osservare che il m . 
kansasii colpisce prevalentemente uomini ( m / f = 20 / 3 ) con et media di circa 70 anni , mentre le infezioni da mac si riscontrano prevalentemente in donne ( m / f = 7 / 12 ) con et media di circa 57 anni . i pazienti immunocompetenti possono essere sostanzialmente ricondotti a due grossi gruppi : quello dei maschi anziani con patologia polmonare cronica e quello delle donne di et media senza storia di patologia polmonare . radiol med ( 2009 ) 114 : 376389 fig . 
b al controllo hrct a distanza di un anno , dopo terapia medica mirata , le bronchiectasie risultano aumentate di numero e dimensioni . encountered in patients with ntm pulmonary infections . the natural history of the infection is unpredictable in immunocompetent patients . 
some patients maintain stable clinical and radiological presentation over a long period , whereas others face rapid clinical progression , which may be fatal without appropriate treatment . the most frequent ntm in our patient population were m . 
in agreement with the literature , m . kansasii infections were prevalent among males ( m / f 20 / 3 ) with a mean age approximately 70 years , whereas mac infections were found mostly among women ( m / f 7 / 12 ) with a mean age of approximately 57 years . 
immunocompetent patients can be divided into two broad groups : elderly men with chronic pulmonary disease , and middle - aged women with no history of pulmonary disease . radiological patterns of ntm infection are not mycobacterium specific , and our findings , in agreement with the recent literature , demonstrated two different radiological presentations : a classic and a nonclassic for the classic form typical of m . 
kansasii infection and less commonly associated with mac infections manifests with areas of lobar or segmental consolidation , commonly situated in the upper lobes , whereas involvement of the i quadri radiologici in caso di micobatteriosi atipica non sono micobatterio specifici e la nostra esperienza , in accordo a quanto riportato nella letteratura recente , ci ha consentito di verificare che esistono due differenti tipi di presentazione radiologica dinfezione : una forma classica ed una non classica . 
kansasii , meno spesso legata ad infezione da mac , si manifesta di solito con aree di consolidazione lobare o segmentaria , pi frequentemente localizzate ai lobi superiori , mentre il coinvolgimento dei lobi inferiori pi raro . 
le caverne , reperto comune alla tubercolosi , sono eterogenee per dimensioni e spessore di parete ; queste caratteristiche non permettono di differenziare una tbc da uninfezione da ntmb , ma correlano semplicemente con i vari stadi evolutivi di malattia . 
la forma non classica , conosciuta anche come lady windermere syndrome , ha delle caratteristiche peculiari consistenti in bronchiectasie cilindriche 386 radiol med ( 2009 ) 114 : 376389 lower lobes is rarer . 
these features do not allow differentiation between tb and ntm infection ; rather , they are simply correlated with the various clinical stages of the disease . apical pleural thickening is another relatively common finding in ntm infections with a classic presentation and is often associated with progressive fibrosis and loss of parenchymal volume . 
the nonclassic form , also known as lady windermere syndrome , has atypical features consisting of mild to moderate cylindrical bronchiectasis and small nodules situated in the middle lobe and the lingula [ 22 , 23 ] , i.e. 
in our patient population , we included these two forms in the two broad categories described above [ 8 ]  . chest radiography of patients with ntm infections only provided information on the presence or absence of cavitations , consolidation , nodules , pleural thickening and volume loss . 
kansasii ( 100% ) predominantly in the upper lobes ( 30%39% ) and in patients with mac infection ( 52.6% ) predominantly in the middle lobe ( 70% ) and the lingula ( 50% ) [ 2325 ]  . 
a similar distribution was also observed for segmental consolidation . nodules the least common finding ( 45.2% ) were encountered more frequently in the upper lobes in m . kansasii infections ( 60% ) and in the middle lobe and lingula in mac infections ( 40% )  . 
lastly , the most common hrct findings in patients with mac infection were bronchiectasis involving the middle lobe and lingula , nodules no larger than 1 cm and focal consolidation [ 26 , 27 ]  . 
patients with preexisting pulmonary disease and mac infection very often present cavitary lesions . medio - moderate e micronoduli localizzati al lobo medio ed alla lingula [ 22 , 23 ] , sedi nelle quali le caverne , le consolidazioni e la perdita di volume sono molto meno comuni [ 23 ]  . 
in letteratura sono state descritte anche altre due forme di infezione polmonare , quella nodulare in pazienti asintomatici e quella consolidativa in pazienti con acalasia , che , nei nostri raggruppamenti , abbiamo fatto rientrare nelle due grandi categorie di pazienti appena descritte [ 8 ]  . lesame radiografico standard del torace in pazienti con infezioni da ntmb ci ha consentito solo di ottenere informazioni circa la presenza o meno di caverne , consolidazioni , macronoduli , ispessimenti pleurici e perdita di volume ; il ricorso alla hrct si reso necessario per una corretta valutazione dellinteressamento polmonare sia prima che dopo terapia . 
allesame tc la micronodulia ( 78 , 6% ) , le cavit ( 71 , 4% ) , le bronchiectasie ( 66 , 6% ) e la consolidazione segmentaria ( 66 , 6% ) sono stati gli aspetti maggiormente riscontrati alla diagnosi . 
kansasii ( 100% ) maggiormente ai lobi superiori ( 30%39% ) e nei pazienti con infezione da mac ( 52 , 6% ) maggiormente a livello del lobo medio ( 70% ) e della lingula ( 50% ) [ 2325 ]  . 
kansasii a livello del lobo superiore destro ( 43% ) , si localizzavano , nellinfezione da mac , al lobo superiore destro ( 33 , 3% ) , al lobo medio ( 33 , 3% ) nonch ai lobi inferiori ( 16 , 7% )  . 
in ultima analisi , nellinfezione da mac i reperti pi frequentemente riscontrati alla tc consistevano in bronchiectasie estese pi spesso al lobo medio ed alla lingula , noduli di diametro massimo di 1 cm e pochi piccoli foci di consolidazione [ 26 , 27 ]  . 
 in letteratura si tentato in numerose serie di trovare una correlazione tra tipo di micobatterio e spessore delle pareti delle caverne ; le caverne correlate ad infezione da mac tendono ad essere pi sottili e con meno opacizzazione parenchimale circostante [ 11 ]  . 
kansasii , sebbene il radiol med ( 2009 ) 114 : 376389 numerous studies in the literature have attempted to find a correlation between type of mycobacteria and the thickness of the cavitation walls . 
kansasii infections , although the most common radiological presentation is cavitations and small nodules in the upper lobes . the use of hrct , with its ability to demonstrate bronchiectasis and small nodules , and the knowledge that the infection tends to have a chronic course and slow progression have shown the importance of treating these patients with medical therapy [ 9 ] and performing adequate follow - up of the parenchymal lesions . 
over the years , there have been various studies aimed at experimenting new and prevalently multidrug protocols , which have had varying success ( 60%80% ) in the different series [ 28 ]  . our follow - up data show that bronchi affected by preexisting bronchiectasis tend to increase in size , and new areas of dilatation can form over time . 
some nodules can undergo cavitation , whereas other smaller nodules may disappear with appropriate therapy . surgical excision should be taken into consideration in patients with localised disease , especially if refractory to medical therapy [ 9 ]  . 
the histological findings , correlated with the corresponding radiological findings , showed that the centrilobular nodules correspond to granulomas and caseous material at the level of the terminal or respiratory bronchioles . 
nodules > 10 mm and lobar consolidation correspond to areas of central caseous granulomas , associated with nonspecific marginal inflammation and lymphocyte infiltration , which completely replaces the alveolar spaces . 
the wall of the cavitations consists of caseous material , epithelioid cells , multinucleated giant cells , granulomatous tissue and a fibrotic capsule . conclusions in agreement with the literature , our findings demonstrate that chest radiography exclusively has a first - line role in the quadro di presentazione pi frequentemente evidenziato consista in cavit e micronoduli ai lobi superiori . 
 con lutilizzo dellhrct , capace di dimostrare bronchiectasie e micronodulazioni , e con la consapevolezza che linfezione tende ad avere decorso cronico e lenta progressione , si dimostrata limportanza di trattare con terapia medica questi pazienti [ 9 ] e di seguire con adeguati followup levoluzione delle lesioni parenchimali . 
negli anni si sono susseguiti studi volti alla sperimentazione di nuovi protocolli , prevalentemente di tipo multifarmaco , che hanno portato al successo terapeutico in percentuali variabili ( 60%80% ) nelle differenti serie [ 28 ]  . i dati in nostro possesso , relativi ai controlli a distanza , hanno permesso di dimostrare che le bronchiectasie preesistenti tendono ad aumentare di dimensioni , mentre nuove aree bronchiectasiche possono formarsi nel tempo . 
la tc dimostra anche che , con il passare del tempo , la diffusione dei noduli si verifica in altri segmenti ; alcuni macronoduli possono escavarsi , mentre alcuni noduli di piccole dimensioni possono , con una valida terapia , scomparire . lexeresi chirurgica deve essere presa in considerazione in pazienti con patologia localizzata , specie se resistenti alla terapia medica [ 9 ] ; tuttavia localizzazioni bilaterali , et avanzata e concomitanti patologie croniche limitano il numero di candidati alla chirurgia [ 11 , 2830 ]  . 
dei nostri pazienti , infatti , soltanto 2 sono stati sottoposti ad intervento chirurgico di lobectomia ed i dati istologici , correlati con i corrispondenti reperti radiologici , hanno dimostrato che i noduli centrolobulari corrispondono a granulomi e materiale caseoso a livello dei bronchioli terminali o respiratori ; i noduli con diametro maggiore di 10 mm e la consolidazione lobare corrispondono ad aree di granulomi caseosi centrali , associati ad infiammazione aspecifica marginale ed infiltrato linfocitario che rimpiazza completamente gli spazi alveolari ; la parete delle caverne costituita da materiale caseoso , cellule epitelioidi , cellule giganti multinucleate , tessuto di granulazione e capsula fibrotica . 
 conclusioni i nostri dati , in accordo con quanto riportato dalla letteratura , dimostrano ampiamente come allo stato attuale lesame radiografico del torace abbia un ruolo esclusivamente di primo livello nelliter diagnostico delle infezioni polmonari da ntmb . 
sicuramente la tc ed in particolare la hrct hanno aperto nuovi scenari nella diagnostica per immagini delle infezioni polmonari da ntmb , permettendo lidentificazione di specifici pattern che spesso , ma non costantemente , 388 radiol med ( 2009 ) 114 : 376389 diagnostic work - up of ntm pulmonary infections . 
ct , and especially hrct , have opened up new horizons in the diagnostic imaging of ntm pulmonary infections by allowing the detection of specific patterns that are often though not always correlated with the different stages of disease and reliable indicators of the efficiency and effectiveness of treatment . 
only with the correct use of hrct can the sign be identified and correlated with other equally important findings to define the stage of the disease . currently , there is limited knowledge and awareness of this diagnostic possibility . 
the incidence of disease might therefore be much higher than reported in the literature , given the nonspecific nature of the clinical symptoms and the similar presentation of preexisting pulmonary disease and ntm infection at conventional radiography . possono essere correlabili alle differenti fasi evolutive della malattia ed essere indicatori attendibili della efficacia / efficienza delle terapie poste in atto . 
scarabino , via napoli 56 , 70031 andria ( ba ) , tel . : + 39 - 088 - 3299140 , fax : + 39 - 088 - 3299220 , e - mail : tscarabino@hotmail.com received : 29 february 2008 / accepted : 8 april 2008 / published online : 12 december 2008 springer - verlag 2009 abstract the objective of this study was to evaluate the potential role of newly developed , advanced magnetic resonance ( mr ) imaging techniques ( spectroscopy , diffusion and perfusion imaging ) in diagnosing brain gliomas , with special reference to histological typing and grading , treatment planning and posttreatment follow - up . 
these limitations can be overcome by supplementing the morphological data obtained with conventional mr imaging with the metabolic , structural and perfusional information provided by new mr techniques that are increasingly becoming an integral part of routine mr studies . 
in addition , the recent development of new , more effective , treatments for cerebral glioma strongly relies on morphofunctional mr imaging with its ability to provide a biological interpretation of these characteristically heterogeneous tumours . riassunto lo scopo del lavoro di illustrare le potenzialit delle nuove e pi avanzate modalit di studio rm ( spettroscopia , diffusione , perfusione ) nella diagnostica dei gliomi cerebrali , con particolare riferimento alla definizione dellistotipo e del grading , alla pianificazione del trattamento e al follow - up post - trattamento . 
necessario pertanto integrare le informazioni fornite dalla rm di base con le informazioni di carattere metabolico , strutturale ed emodinamico fornite dalle pi recenti tecniche rm , oramai parte integrante di uno studio di routine . 
the gold standard for establishing brain tumour histological type and grade is histopathology of tissue specimens obtained with stereotactic or open biopsy , both of which are invasive procedures [ 2 ]  . 
there is thus a need to use noninvasive modalities capable of providing a diagnosis closely corresponding to the histological diagnosis but without risks for the patient and affording a more global view not restricted to the surgical specimen . in this context , a key role may be played by magnetic resonance ( mr ) imaging supplemented by techniques that provide anatomicalpathological information of considerable diagnostic and clinical utility . 
under ideal conditions , conventional mr imaging with its multiplanar capabilities , ability to evaluate multiple parameters , excellent contrast resolution and lack of invasiveness helps to detect the lesion , identify its intra - axial site , define its precise location and hypothesise its nature . 
however , it has limited sensitivity and specificity in defining glioma type and grade [ 4 ] and does not always permit precise delineation of tumour margins or tumour differentiation from oedema and / or treatment effects ( recurrence vs radionecrosis ) [ 5 , 6 ]  . 
 the diagnostic limitations of conventional mr imaging can be overcome by new , advanced mr techniques that give metabolic , structural and perfusional information , thereby providing the surgeon with increasingly precise and comprehensive diagnoses . 
the aim of this paper is to illustrate the potential of the new mr techniques , such as spectroscopy , diffusion and perfusion imaging , in diagnosing brain gliomas , with special reference to histological typing and grading , treatment planning and posttreatment monitoring . 
the paper reviews data from the literature and the authors personal experience . i gliomi costituiscono circa il 70% dei tumori primitivi maligni cerebrali , e sono caratterizzati da una notevole eterogeneit nellaspetto neuropatologico , nellespressione genica e nella prognosi [ 1 ]  . 
una diagnosi precoce e soprattutto una approfondita valutazione della reale estensione del tumore e dei rapporti con le strutture anatomiche circostanti sono elementi importanti ai fini della prognosi e dellimpostazione delle diverse strategie terapeutiche . 
lesame gold standard per la diagnosi di tipo e grado di tumore cerebrale lo studio isto - patologico su tessuto prelevato attraverso stereotassi o resezione chirurgica , metodi entrambi invasivi [ 2 ]  . 
da qui la necessit di utilizzare modalit di studio non invasive che possano condurre ad una diagnosi il pi vicino possibile a quella istologica , senza rischi per il paziente e con un punto di vista pi ampio , non limitato al solo pezzo anatomico prelevato . in questa prospettiva si inserisce perfettamente la risonanza magnetica ( rm ) , corredata da una serie di metodiche complementari allimaging di base che , nellinsieme , offrono informazioni anatomo - patologiche di grandissima utilit diagnostica e clinica . 
in condizioni ideali , infatti , in virt di una serie di vantaggi , quali la multiplanariet , la multiparametricit , lottima risoluzione di contrasto , lassenza di invasivit , la rm di base consente di identificare la lesione , stabilirne la sede intrassiale , definirne una precisa localizzazione e proporre unipotesi di natura . 
inoltre la rm di base non sempre permette una precisa definizione dei margini della neoplasia n consente di distinguere con certezza il tumore dalledema e / o dagli effetti del trattamento ( recidiva vs radionecrosi ) [ 5 , 6 ]  . 
 le nuove ed avanzate modalit di studio rm , grazie alle informazioni metaboliche , strutturali ed emodinamiche che riescono a fornire , riducono i limiti diagnostici della sola rm di base permettendo diagnosi sempre pi precise ed esaustive per il chirurgo . 
lo scopo del lavoro di illustrare le potenzialit delle nuove e pi avanzate modalit di studio rm , quali la spettroscopia , la diffusione e la perfusione , nella diagnostica dei gliomi cerebrali con particolare riferimento alla definizione dellistotipo e del grading , alla pianificazione del trattamento e al follow - up post - trattamento . 
verranno presi in considerazione i dati della letteratura integrati con i risultati della nostra esperienza . 450 spectroscopy proton mr spectroscopy ( 1h - mrs ) is a noninvasive technique that provides metabolic information about normal and pathological tissue components [ 79 ]  . 
the physical principle underlying 1h - mrs is the chemical shift that varies in relation to differences in precession frequency of atoms belonging to different molecules ( metabolites )  . 
 the most commonly used metabolites in diagnosing gliomas are choline ( cho ) , creatine ( cr ) , n - acetyl - aspartate ( naa ) , lactate ( lac ) and lipid ( lip )  . 
il principio fisico sfruttato dalla 1h - mrs il chemical shift che varia in rapporto alle differenze di frequenza di precessione di atomi appartenenti a singole molecole ( metaboliti )  . 
 i metaboliti maggiormente coinvolti nella diagnostica dei gliomi sono la colina ( cho ) , la creatinina ( cr ) , ln - acetilaspartato ( naa ) , il lattato ( lac ) e i lipidi ( lip )  . 
combining this information with the morphostructural data from conventional mr imaging leads to a 15% increase in the number of correct diagnoses compared with conventional mr imaging alone , with no increase in incorrect diagnoses [ 10 ]  . 
the major challenge in interpreting the metabolic information of gliomas is related to the extreme heterogeneity among tumours of different grades , tumours of the same grade and even within individual tumours [ 11 ]  . 
lip is also essential for tumour grading , as it reflects tissue necrosis , which in turn is related to tumour grade , thereby permitting differentiation of grade iv from grades ii and iii lesions [ 7 , 9 ]  . 
 from a methodological point of view , several authors have demonstrated the usefulness of employing short echo time ( te ) ( 35 ms ) rather than intermediate te ( 144 ms ) sequences on high - field mr spectroscopy in grading gliomas , despite the different cho / cr and laclip ( ll ) / cr ratios obtained . 
in particular , if a single sequence must be chosen , the short te sequence is preferable because of the poor lactate inversion at intermediate te [ 12 ]  . in a recent study , by exploiting the potential of a highfield magnet , we were able to analyse the spatial distribution ormai noto che la 1h - mrs in grado di fornire informazioni sulle caratteristiche metaboliche dei tumori , ed in particolare dei gliomi , che complementariamente a quelle prettamente morfo - strutturali fornite dal solo imaging conducono ad un incremento di diagnosi corrette pari al 15% rispetto a quanto accade con la sola rm di base , senza alcun incremento di diagnosi non corrette [ 10 ]  . 
la difficolt maggiore nellinterpretazione delle informazioni metaboliche fornite dai glomi legata alla estrema eterogeneit tumorale tra differenti gradi , allinterno dello stesso grado ed anche allinterno del singolo tumore [ 11 ]  . 
la cho ha un ruolo importante in virt della diretta correlazione con la proliferazione cellulare tumorale che comunque non sempre correlata direttamente con il grading ( il caso del meningioma )  . 
anche i lip sono essenziali ai fini delle differenziazione tumorale : essi infatti esprimono la necrosi tissutale che , a sua volta , correlata al grado tumorale , permettendo cos di differenziare lesioni di grado iv da lesioni di ii e iii grado essendo correlati con la necrosi [ 7 , 9 ]  . 
in particular , in high - grade gliomas , cho is reduced in the central necrotic areas , elevated in the tumour mass and margins , reduced in peritumoural oedema and increased to normal levels in the surrounding healthy tissue ; naa is reduced in the central areas , increased in the periphery and normal in the surrounding healthy tissue ; lac - lip are substantially increased in the central necrotic areas and reduced in the tumour margins . 
in low - grade gliomas , cho is usually increased in the central areas , reduced in the margins and slightly increased in the surrounding healthy tissue ; naa is reduced in the mass and tumour margins and normal in the surrounding healthy tissue ; lac - lip are not detectable ( personal communication )  . 
 treatment planning supplementing conventional mr imaging with metabolic imaging improves the definition of tumour margins . conventional mr imaging alone does not allow distinction between infiltrated and noninfiltrated peritumoural oedema . this distinction is made possible by spectral analysis , as infiltrated oedema shows an abnormal cho / naa ratio , whereas the ratio is normal in pure vasogenic oedema . tumour extent can thus be defined beyond the margins detected by conventional imaging ( beyond the borders of contrast enhancement or peritumoural t2 hyperintensity ) , allowing differentiation of active tumour from normal oedematous tissue [ 1317 ]  . 
it has been reported that when radiosurgery includes peritumoural parenchymal areas with high cho and abnormal cho / naa ratio and hence infiltrated areas patient survival is prolonged [ 15 ]  . 
 posttreatment follow - up 1h - mrs has higher sensitivity than does conventional mr imaging in detecting tumour progression , as it can demonstrate spectral abnormalities beyond the limits of the radiation target , even in the absence of contrast enhancement or before an increase in contrast enhancement is detected [ 16 ]  . in particular , changes in cho and the magnitude of the cho / cr and cho / naa ratios are predictive of tumour progression . 
in particolare nei gliomi di alto grado la cho risulta ridotta nelle aree centrali necrotiche , aumentata nella massa e nei margini tumorali , ridotta nelle aree edematose e di nuovo incrementata fino ai livelli normali nel tessuto sano circostante ; lnaa invece ridotto nelle aree centrali , aumentato verso la periferia e raggiunge valori normali nel tessuto sano circostante ; i lac - lip risultano invece notevolmente aumentati nelle aree centrali necrotiche e ridotti ai margini della neoplasia . 
nei gliomi di basso grado , di solito , la cho elevata nelle aree centrali , si riduce verso i margini e persiste leggermente alta nel tessuto sano circostante ; lnaa ridotto nella massa e nei margini tumorali , raggiunge valori normali nel tessuto sano circostante ; i lac - lip non risultano per nulla rilevabili ( comunicazione personale )  . 
con la valutazione degli spettri ci invece possibile , dato che nelle aree edematose infiltrate da neoplasia presente uno spettro con anomalo rapporto cho / naa contrariamente a quello che accade in presenza di edema vasogenico puro caratterizzato dalla normalit di tale rapporto . 
in tal modo possibile delineare lestensione del tumore oltre i margini rilevati con limaging di base ( al di fuori dei bordi del contrast enhancement , ce , o delliperintensit peritumorale in t2 ) distinguendo il tumore attivo dal tessuto normale ed edematoso [ 1317 ]  . 
tali indicazioni sono utili al fine di effettuare una biopsia pi mirata e una terapia ( chirurgica o radiante ) maggiormente differenziata , in modo da risparmiare la maggior quota di tessuto sano . 
peraltro alcuni autori hanno evidenziato che quando la radiochirurgia include le aree parenchimali peritumorali con alta cho e alterato rapporto cho / naa e quindi infiltrate , vi un allungamento della sopravvivenza del paziente [ 15 ]  . 
 controllo post - trattamento la 1h - mrs presenta una sensibilit maggiore rispetto allo studio rm convenzionale nel rilevare una progressione neoplastica , evidenziando anomalie spettrali al di fuori della sede del letto chirurgico , anche in assenza di ce e comunque prima di un incremento dello stesso [ 16 ]  . 
per la cho , laumento oltre il 45% del valore normale misurato controlateralmente indice di progressione di malattia ; mentre un valore uguale o inferiore al 35% indicativo di stabilit [ 17 ]  . 
 tumour response to surgical and / or radiation therapy usually involves an initial reduction of cho , with possibly an increase in lac / lip , indicating radiation necrosis , which is characterised by the absence of any metabolic signals for up to several months [ 10 ]  . 
 in the follow - up after chemotherapy , the cho / cr and lac / cr ratios are the most reliable markers for assessing the response of low - grade gliomas . 
in the enhancing tumour regions , a significant association was detected between increased lac / cr during treatment and decreased progression - free survival time , whereas a low naa / cr in normalappearing brain tissue adjacent to nonenhancing tumour at baseline was associated with decreased progression - free survival time . 
an increase in cho / cr and lac / cr in normalappearing brain regions next to the tumour may be noted several months before mr imaging reveals disease progression [ 24 ]  . 
the result may be visualised in different , increasingly complex , forms , each of which information : ( 1 ) diffusion - weighted provides unique raggiunge una sensibilit del 93 , 8% e una specificit del 85 , 7% [ 18 ]  . 
essi sono significativamente pi alti nelle recidive rispetto al danno radiante e ancor pi alti rispetto alla sostanza bianca apparentemente sana ; naa / cr ha un andamento opposto [ 21 ]  . 
sensibilit , specificit ed accuratezza diagnostica dei rapporti cho / cr e cho / naa sono risultati rispettivamente del 94 , 1% , 100% e 96 , 2% [ 22 ]  . 
 la risposta di un tumore alla terapia chirurgica e / o radiante consiste , di solito , nella iniziale riduzione della cho e nella possibile comparsa del picco di lac / lip per la necrosi da irradiazione caratterizzata soprattutto dalla assenza di segnale metabolico che persiste per diversi mesi [ 10 ]  . 
 nel follow - up post - chemioterapia i rapporti cho / cr e lac / cr risultano essere i marker pi utili per il follow - up dei gliomi a basso grado . 
nelle aree con ce stata individuata una significativa associazione tra lincremento del lac / cr durante il trattamento e la riduzione della progressione / sopravvivenza , mentre nellimaging di base un basso naa / cr nel tessuto cerebrale apparentemente normale adiacente al tumore senza ce associato ad una ridotta progressione / sopravvivenza . 
un aumento di cho / cr e lac / cr nel tessuto cerebrale apparentemente normale adiacente al tumore pu evidenziarsi qualche mese prima della progressione di malattia in rm [ 24 ]  . 
the different cellularity of tissues corresponds to changes in the diffusivity of water molecules : the greater the cellularity and consequently the number of cell membrane interfaces , the lower the diffusivity . histological typing and grading besides the inverse relationship between the adc and cellularity ( an important parameter in grading ) , data on the possibility of discriminating histological type and grade are conflicting because of tissue heterogeneity [ 25 , 26 ]  . normally , it is not possible to distinguish low - grade from high - grade gliomas on the basis of dwi and adc values alone [ 27 ]  . 
dwi is , instead , far more useful in differentiating cystic from solid components of a mass and the tumour mass from necrosis or surrounding healthy tissue [ 28 , 29 ]  . 
 treatment planning dwi is not generally accepted as a useful parameter for determining the extent of tumour infiltration and differentiating infiltrated from vasogenic oedema owing to its intrinsic low spatial resolution [ 25 ]  . 
moreover , there is some overlap of the adc and fractional anisotropy ( fa ) values in peritumoural regions with high signal intensity on t2 and in the adjacent normal - appearing white matter between various types of brain tumour [ 30 ]  . 
dti is no doubt more useful for planning neurosurgery or radiotherapy in that it visualises white - matter tracts that may be displaced and oedematous ( as in low - grade gliomas , meningiomas or metastases ) , or infiltrated or destroyed ( as in high - grade tumours ) [ 31 ]  . information about the integrity of structures inside or outside the tumour obtained by visualising its relationships with critical cortical areas and white - matter tracts may guide treatment decisions ( radical or partial ) so as to optimise tumour resection and minimise permanent posttreatment neurological morbidity [ 32 ]  . 
the combination of dti and cortical activation maps ( fmri ) improves the accuracy of presurgical mapping by delineating the relationship between the tumour and white - matter tracts ( with dti ) and eloquent cortical areas ( with fmri )  . 
in the posttreatment follow - up of a high - grade glioma , it helps to differentiate the effects of radiotherapy from disease recurrence or progression [ 34 ]  . 
con il variare della cellularit di un tessuto varia infatti la diffusivit delle molecole dacqua : maggiore la cellularit , e quindi il numero delle interfacce di membrane cellulari , minore la diffusivit . istotipo e grading nonostante la presenza di una correlazione inversa tra adc e cellularit ( parametro importante per definire il grading ) , i dati riguardanti la possibilit di discriminare istotipo e grading tumorale sono contrastanti in virt della eterogeneit tissutale [ 25 , 26 ]  . 
di solito non possibile distinguere un glioma di basso grado da uno di alto grado utilizzando solo le immagini pesate in diffusione e i valori di adc [ 27 ]  . 
la dwi invece molto pi utile nel differenziare le componenti cistiche e solide di una massa , la massa tumorale dalla necrosi o dal tessuto sano circostante [ 28 , 29 ]  . 
 pianificazione del trattamento la dwi non da tutti considerato un parametro utile per determinare lestensione della infiltrazione tumorale e per differenziare linfiltrazione neoplastica dalledema vasogenico per lintrinseca limitazione della risoluzione spaziale [ 25 ]  . 
inoltre , vi sovrapposizione dei valori di adc e fa ( fractional anisotropy ) nelle aree peritumorali iperintense in t2 e nelladiacente sostanza bianca apparentemente normale tra tumori cerebrali di vario tipo [ 30 ]  . 
sicuramente pi importante il dti che fornisce informazioni utili per il planning neurochirurgico / radioterapeutico visualizzando i fasci di sostanza bianca che possono essere dislocati ed edematosi ( in gliomi di basso grado , meningiomi o metastasi ) , oppure infiltrati o distrutti ( in tumori di alto grado ) [ 31 ]  . 
le informazioni circa la integrit o meno delle strutture poste allinterno e al di fuori del tumore , infatti , evidenziando i rapporti della lesione con le aree corticali critiche e con i fasci di sostanza bianca , possono guidare la scelta del tipo di trattamento ( radicale o parziale ) , ottimizzando la resezione tumorale e riducendo al minimo il danno cerebrale e quindi la morbilit neurologica permanente post - trattamento [ 32 ]  . 
la combinazione del mapping dti con quello di attivazione corticale ( fmri ) fornisce un mapping prechirurgico ancora pi accurato , delineando i rapporti del tumore con i fasci di sostanza bianca ( con il dti ) e le aree corticali eloquenti ( con lfmri )  . 
 controllo post - trattamento ladc nellimmediato periodo post - operatorio pi utile del ce nel definire la persistenza o meno di patologia [ 33 ]  . nel follow - up di un glioma di alto grado trattato , esso permette di differenziare gli effetti della radioterapia dalla recidiva o progressione tumorale [ 34 ]  . 
in particular , the adc is significantly higher in radionecrosis than in tumour recurrence , even though there is some overlap [ 34 ]  . in the presence of an enhancing lesion , the adc is significantly higher in tumour recurrence than in radiation injury , whereas in white - matter tracts in peritumoural oedema , the adc is higher in radiation injury than in tumour recurrence . 
fa is significantly higher in the normalappearing white matter adjacent to the peritumoural oedema in radiation injury compared with tumour recurrence [ 35 ]  . perfusion imaging mr perfusion - weighted imaging ( pwi ) is a useful , noninvasive , and rapid technique that is increasingly being used in the characterisation of brain tumours [ 36 , 37 ]  . 
numerous techniques have been proposed for measuring brain perfusion parameters : cerebral blood volume , transit time , clearance , extraction fraction , cerebral blood flow and the permeability - surface area product [ 38 ]  . 
the most commonly used technique in clinical practice is dynamic susceptibilityweighted bolus - tracking mr imaging , which is based on the susceptibility effects obtained after intravenous injection of a bolus of paramagnetic contrast material and first - pass acquisition of t2 - weighted echoplanar ( epi ) sequences of the region of interest . 
 histological typing and grading when a tumour is present , there is increased microvessel density and neoangiogenesis , both of which are crucial histological criteria for determining glioma aggressiveness . this leads to increased cbv , which is considered one of the main predictors of tumour aggressiveness and survival , even though it is not synonymous for malignancy ( e.g. highly vascular benign tumours such as oligodendroglioma and meningioma ) [ 40 , 41 ]  . 
in particolare significativamente pi alto nella radionecrosi che nella recidiva tumorale anche se esiste un certo grado di sovrapposizione [ 34 ]  . in presenza di lesione con ce , ladc significativamente pi alto nella recidiva rispetto al danno radiante , mentre nei fasci di sostanza bianca nelledema perilesionale ladc risultato pi alto nel danno da irradiazione rispetto alla recidiva . 
la fa invece significativamente pi alto nella sostanza bianca apparentemente normale adiacente alledema perilesionale in presenza di danno radiante rispetto alla recidiva [ 35 ]  . perfusione limaging di perfusione ( pwi ) con rm una tecnica non invasiva , di rapida esecuzione e di indubbia utilit che viene sempre pi spesso utilizzata nella caratterizzazione delle neoformazioni cerebrali [ 36 , 37 ]  . 
numerose tecniche sono state proposte per misurare la perfusione a livello cerebrale , ed altrettanto numerosi sono i parametri che possono essere misurati : il volume ematico cerebrale , il tempo di transito , la clearance , la frazione di estrazione , il flusso ematico cerebrale e il prodotto tra superficie di permeabilit e flusso ematico [ 38 ]  . 
nella pratica clinica di solito si utilizza il metodo che si basa sulle caratteristiche di suscettibilit che si ottengono dopo somministrazione endovenosa a bolo di un mdc paramagnetico e nelle acquisizioni , nellarea di interesse , al primo passaggio del bolo , di sequenze ecoplanari ( epi ) pesate in t2 . 
ci comporta laumento del cbv considerato uno dei maggiori fattori predittivi di aggressivit neoplastica e di sopravvivenza in vari istotipi anche se non sinonimo di malignit ( il caso di tumori benigni molto vascolarizzati quali loligodendroglioma e il meningioma ) [ 40 , 41 ]  . 
 studies investigating the possibility of delimiting the true tumour margins with pwi have yielded conflicting results . in a recent study involving 36 patients with gliomas of different grades , we performed pwi with a 3 - tesla magnet , which allowed us to distinguish not only necrosis from tumour but also oedema mixed with tumour ( with high cbv ) from pure oedema ( with low cbv ) [ 45 ]  . 
there is a good correlation between cbv and 1h - mrs in delineating tumour margins . posttreatment follow - up cbv is significantly higher in tumour recurrence than in radionecrosis , although there is some overlap [ 27 ]  . 
given the recent development of new treatments aimed at reducing neoangiogenesis ( both pharmacological and targeted radiation ) , pwi may take on a primary role as a means to monitor their efficacy in a simple and rapid fashion . multimodal mr evaluations use of a single conventional or advanced mr imaging pattern for diagnosing gliomas may prove insufficient for histological typing and grading , treatment planning and posttreatment follow - up . 
hence the need for combined studies capable of enhancing the techniques diagnostic accuracy [ 4 , 4750 ]  . we recently conducted a multimodal study involving the combination of conventional mr imaging with spectroscopy , diffusion and perfusion imaging on 31 patients with cerebral gliomas of different grades . 
in una nostra recente esperienza che ha coinvolto 36 pazienti con glioma di diverso grado lo studio di perfusione effettuato con apparecchiatura a 3 tesla , oltre che permettere la distinzione tra necrosi e massa tumorale , ha permesso di differenziare ledema misto a tumore ( con alto cbv ) dalledema puro ( con basso cbv ) [ 45 ]  . 
esiste , comunque , una buona correlazione tra cbv e 1h - mrs nella delineazione dei margini tumorali . controllo post - trattamento il cbv significativamente pi alto nella recidiva tumorale rispetto alla radionecrosi , ma esiste un certo grado di sovrapposizione [ 27 ]  . 
con il recente interesse e sviluppo di nuove tecniche terapeutiche mirate a ridurre la neo - angiogenesi ( farmacologiche e radianti mirate ) la pwi pu assumere ruolo primario per valutare in maniera semplice ed immediata la loro efficacia . valutazioni rm multimodali luso di un solo pattern rm di base o avanzato per la diagnosi dei gliomi pu non bastare ai fini soprattutto di definire istotipo e grading , pianificazione del trattamento , follow - up up post - trattamento . 
da qui la necessit spesso di studi combinati capaci di aumentare laccuratezza diagnostica [ 4 , 4750 ]  . in una recente esperienza personale , abbiamo condotto uno studio multimodale abbinando alla rm di base una valutazione di spettroscopia , diffusione e perfusione . 
in tale studio che ha coinvolto 31 pazienti con glioma cerebrale di diverso grado , tutti i parametri utilizzati , ad eccezione delladc , hanno permesso di differenziare i gliomi di basso grado da quelli di alto grado . 
e infatti la ricerca dei dati semeiologici basilari sede di origine , modalit di crescita , caratterizzazione tissutale ed il confronto con let e le informazioni cliniche dei pazienti pu condurre alla corretta diagnosi pre - trattamento . 
1a - f contrast - enhanced t1 - weighted image ( a ) and fluid - attenuated inversion recovery ( flair ) image ( b ) , apparent diffusion coefficient ( c ) and cerebral blood volume ( d ) maps , localising flair image ( e ) and proton mr spectroscopy ( 1h - mrs ) spectra in regions of interest ( roi ) ( f ) in a 49 - yearold patient with a grade ii frontoparietal fibrillar astrocytoma . 
spectra 1 , 2 and 3 show the typical pattern of low - grade gliomas , characterised by elevated choline ( cho ) , abnormal cho / n - acetyl - aspartate ( naa ) ratio ( > 1 ) and absence of lactate and lipid ( lac - lip ) peak . 
1a - f immagine rm pesata in t1 dopo mezzo di contrasto ( a ) e flair ( b ) , mappe di coefficiente di diffusione apparente ( adc ) ( c ) e di volume ematico cerebrale ( cbv ) ( d ) , immagine localizzatrice flair ( e ) e spettri 1h - mrsi in regioni di interesse ( roi ) ( f ) , in un paziente di 49 anni con astrocitoma fibrillare di ii grado in sede fronto - parietale sinistra . 
gli spettri 1 , 2 e 3 presentano un pattern tumorale tipico dei glomi di basso grado , caratterizzato da elevata cho , anomalo rapporto cho / naa ( > 1 )  . 
2a - f contrast - enhanced t1 - weighted image ( a ) and fluid - attenuated inversion recovery ( flair ) image ( b ) , apparent diffusion coefficient ( adc ) ( c ) and cerebral blood volume ( cbv ) ( d ) maps localising t2 - weighted image ( e ) and proton mr spectroscopy ( 1h - mrs ) spectra in regions of interest ( roi ) ( f ) in a 56 - year - old patient with right temporooccipital glioblastoma multiforme . 
spectra 1 , 3 and 4 at the lesion margins show the typical tumoural pattern , characterised by elevated choline ( cho ) , abnormal cho / nacetyl - aspartate ( naa ) ratio ( > 1 ) and lactate and lipid ( lac / lip ) peak . 
spectra 5 and 6 , in a region of apparent oedema beyond the enhancing margins , show reduced levels of all metabolites ( relative to the normal spectra 7 , 8 and 9 ) but different patterns : spectrum 5 has a normal cho / naa ratio ( < 1 ) , suggesting noninfiltrated oedema ; spectrum 6 has a tumoural pattern suggesting infiltrating tumour cells . 
2a - f immagine rm pesata in t1 dopo mezzo di contrasto ( a ) e flair ( b ) , mappe di coefficiente di diffusione apparente ( adc ) ( c ) e di volume ematico cerebrale ( cbv ) ( d ) , immagine localizzatrice pesata in t2 ( e ) e spettri 1h - mrsi in regioni di interesse ( roi ) ( f ) , in una paziente di 56 anni con glioblastoma temporo - occipitale destro . 
gli spettri 1 , 3 e 4 , sui margini del glioblastoma , presentano il tipico pattern tumorale , caratterizzato da elevata cho , anomalo rapporto cho / naa ( > 1 ) e presenza di lac / lip ( ll )  . 
lo spettro 2 , allinterno dei margini impregnati , presenta una riduzione dei livelli di tutti i metabolici ad eccezione di ll che risulta ulteriormente incrementato ; in tale sede , ladc tende ad essere aumentato e il cbv ridotto . gli spettri 5 e 6 , in unarea apparentemente edematosa esterna ai margini impregnati , presentano nel complesso livelli ridotti di tutti i metaboliti ( rispetto agli spettri normali 7 , 8 e 9 ) , ma pattern differenti : lo spettro 5 ha un normale rapporto cho / naa ( < 1 ) e suggerisce la presenza di edema vasogenico non infiltrato ; lo spettro 6 ha un pattern tumorale e suggerisce la presenza di cellule tumorali infiltranti . 
in queste sedi , adc e cbv hanno un comportamento opposto , essendo il primo elevato e il secondo ridotto nellarea di edema puro e viceversa nellarea di edema infiltrato . 
the extreme heterogeneity of brain tumours and the limited specificity of mr imaging may make it difficult to arrive at a clear histological diagnosis , which is straightforward in typical cases only . 
furthermore , the wider availability of 3 - tesla mr equipment and awareness of its numerous advantages ( high signal , high resolution , high sensitivity , better quality , reduced examination times , additional and more advanced imaging techniques ) is stimulating the development and application of morphofunctional evaluation of brain tumours in routine neuroradiological practice [ 5658 ]  . 
this becomes all the more important if we consider the recent development of new and more effective antitumoural treatments that rely on a complete morphofunctional mr study to obtain a noninvasive in vivo neuropathological characterisation and thus a biological interpretation of the typical heterogeneity of such tumours . interpretazione non solo per il neuroradiologo , ma anche per il neuropatologo . 
tali tecniche , fornendo dati relativi al metabolismo cellulare , alla diffusione e allemodinamica , migliorano laccuratezza diagnostica , la sensibilit e la specificit della metodica rm [ 5355 ]  . 
inoltre , la maggiore diffusione sul territorio di apparecchiature con intensit di campo a 3 tesla , in virt dei numerosi vantaggi ( alto segnale , alta risoluzione , alta sensibilit , migliore qualit , tempi desame ridotti , metodologie di studio aggiuntive e pi avanzate ) sta favorendo lo sviluppo e lapplicazione nella pratica neuroradiologica di routine della valutazione morfo - funzionale della patologia cerebrale [ 5658 ]  . 
baffoni2 1uos neuroradiologia , 2uoc radiologia , 3uos di staff programmazione sanitaria e miglioramento qualit , 4direzione medica ospedaliera , 5uoc nefrologia e dialisi , 6uoc anestesia e rianimazione , 7uos di staff ufficio relazioni con il pubblico , 8uos di staff formazione ed aggiornamento , 9uos medicina legale , 10uos diabetologia e malattie metaboliche , 11uoc patologia clinica , 12uos allergologia , asur marche zona territoriale 11 , via zeppilli 18 , 63023 fermo , italy correspondence to : m.g. 
138 , 63023 fermo , italy , tel . : + 39 - 0734 - 6252246 , fax : + 39 - 0734 - 6253200 , e - mail : massimogiuliano.bonetti@tin.it received : 10 january 2008 / accepted : 9 may 2008 / published online : 25 march 2009 springer - verlag 2009 abstract purpose . 
the new documentation ( patient history / screening form and informed consent form ) is available on the hospital web site and requests serum creatinine determination with estimation of glomerular filtration rate ( gfr ) for every patient . 
un evento formativo di rinforzo per i medici invianti e la verifica del fg al momento della prenotazione dellesame sono giudicati indispensabili per la corretta programmazione delle indagini nei pazienti a rischio . radiol med ( 2009 ) 114 : 496508 keywords diagnostic imaging iodinated contrast media guidelines parole chiave diagnostica per immagini mezzi di contrasto organo - iodati linee guida introduction introduzione stimulated by the sirm emilia romagna and marche regional chapters and the experience of the modena university hospital and hospital trust ( protocollo sulluso dei mezzi di contrasto 26 / 9 / 2001 ) , the authors sought to implement the new national guidelines on the use of injectable iodinated contrast media ( icm ) issued by sirm ( italian society of medical radiology ) [ 1 , 2 ] to prevent icm toxicity at their institution . the project was presented and informally discussed with the institutions radiologists at two departmental meetings held in 2004 and 2005 , where the new documentation ( patient history / screening form and informed consent form ) was presented through a powerpoint slide show ( mgb , personal communication )  . 
one point that emerged from these preliminary meetings was the need to adopt a systematic approach to the problem of icm , as its use is still governed by consolidated practice and there is some resistance to change . 
critically review the list of laboratory tests ordered before icm administration ( for all patients : blood urea nitrogen , glucose , serum creatinine , serum protein and protein electrophoresis , urinalysis ) 3 . 
provide information about the comorbidities capable of increasing the risk of reaction to icm and to devise specific protocols for preventing organ damage and , where needed , for patient preparation 4 . 
create a tool capable of promoting the sharing of responsibility between the referring physician and the radiologist , as indicated in the directive euratom 43 / 97 and incorporated in our legislation [ 3 ] , by reviewing the patient history / screening form and informed consent form 5 . 
train radiology personnel in the first - line techniques and treatment to be used in the event of adverse reactions to alla luce dei recenti orientamenti sulluso del mezzo di contrasto organo iodato per via iniettiva ( mdc ) espressi dalla sirm ( societ italiana di radiologia medica ) [ 1 , 2 ] e stimolati in ambito regionale sirm emilia romagna e marche dallesperienza gi attuata nelle aziende ospedaliere policlinico e usl di modena ( protocollo sulluso dei mezzi di contrasto 26 / 9 / 2001 ) , abbiamo voluto implementare anche nella nostra realt operativa delle linee guida aggiornate sulla profilassi della tossicit da mdc . la preliminare presentazione e discussione informale della problematica con i colleghi radiologi nellambito di due riunioni di reparto negli anni 2004 e 2005 , tramite presentazione power - point ( m.g.b. , comunicazione personale ) comprensiva di una nuova modulistica per linformativa ed il consenso informato , ha indicato la necessit di un approccio organico alla problematica dei mdc , molto influenzata dalla prassi consolidata e poco incline alle novit . 
during a series of meetings held in the first semester of 2006 , the group jointly prepared the draft documentation the patient history / screening form ( to be filled in by the referring physician and by the patient ) and the informed consent form ( to be filled in by the radiologist and patient during the routine interview before the examination )  . 
the group devised specific protocols for patients at risk of adverse reactions to icm and / or for those requiring special preparation and identified the relevant contact telephone numbers to be given to the service users . in collaboration with the hospitals public relations department ( mfs ) , the new forms for radiological investigations , including those employing icm , were posted on the hospitals web site ( asp ? co_id = 6493 ) , together with links to sirm web pages providing practical information on patient preparation for imaging studies ( esami / ) and the national guidelines [ 5 ]  . in collaboration with the hospitals education and training department ( sm ) , two training courses were developed to illustrate the draft document on icm use , the national guidelines ( with special reference to the appropriateness of imaging procedures , harmful effects of radiation exposure and icm administration ) and the patient history / screening and consent forms posted on the hospital web site . 
all materials were supplied to the course participants as hypertexts on cd - rom . the first course , titled diagnostic imaging : national guidelines [ two afternoons for a total of 10 h , 10 continuing medical education ( cme ) credits ] was repeated in two sessions ( january and february 2007 ) and was addressed to medical , nursing and technical personnel of the radiology department . 
the same personnel were also enrolled in inhouse training sessions on first - aid techniques [ bls ( basic life support ) or blsd ( basic life support and defibrillation ) ]  . 
in addition to hospital trolleys with emergency medications , diagnostic imaging rooms were also provided with kits containing specific drugs for adverse reactions to contrast media [ chlorphenamine maleate ( trimeton 10 mg / ml vials , schering - plough ) ; ranitidine chloride ( ranitidine angenerico 50 mg / 5 ml , angelici ) ; hydrocortisone ( flebocortid 1g / 10 ml , sanofi aventis ) ; methylprednisolone hemisuccinate ( urbason 40 mg / ml , aventis ) ; adrenaline im ( 0.33 mg fastjekt adults , merck ; 0.165 mg fastjekt junior , merck ) ; and the telephone numbers of the anaesthetistresuscitator for emergencies . 
in una serie di riunioni nel primo semestre del 2006 stata quindi preparata una bozza di documento condivisa , comprensiva della nota informativa ( da compilarsi a cura del medico inviante e del paziente ) e del consenso informato ( da compilarsi a cura del medico radiologo e del paziente nel consueto colloquio pre - esame )  . 
sono stati previsti i percorsi per i pazienti a rischio per la somministrazione del mdc e / o con necessit di particolare preparazione e sono stati identificati i numeri telefonici di riferimento da fornire agli utenti . in collaborazione con la uos di staff ufficio relazioni con il pubblico [ m.f.s. ] , la modulistica relativa alle indagini radiologiche , comprese quelle con mdc , stata resa disponibile sul sito aziendale ( viewdoc.asp ? co_id = 6493 ) , assieme ad un link sulle informazioni pratiche per la preparazione dei pazienti alle indagini di imaging ( esami / ) ed alle linee guida nazionali di riferimemento [ 5 ]  . in collaborazione con la nostra uos di staff formazione ed aggiornamento [ s.m. ] sono stati preparati due progetti formativi per illustrare : la bozza del documento condiviso sui mdc , le linee guida nazionali di riferimento ( con particolare riguardo allappropriatezza delle indagini di imaging , agli effetti dannosi associati allesposizione alle radiazioni ionizzanti ed alla somministrazione dei mdc ) , fornite ai corsisti in versione ipertestuale di facile consultazione su cd , e la modulistica disponibile sul sito aziendale di cui sopra . 
 il primo progetto formativo , dal titolo la diagnostica per immagini : linee guida nazionali di riferimento ( due pomeriggi per un totale di 10 ore , 10 crediti ecm ) stato presentato in due edizioni ( gennaio e febbraio 2007 ) al personale medico , infermieristico e tecnico della nostra radiologia . 
at the same time , the report forms for serum creatinine used by the hospitals clinical laboratory services were integrated , with an estimation of glomerular filtration rate ( gfr ) to be calculated automatically by applying the simplified modification of diet in renal disease ( mdrd ) formula [ 6 ] , namely : gfr ( ml / min per 1.73 m2 ) = 186 ( serum creatinine ) 1.154 ( age ) 0.2030.742 ( if patient is female ) 1.210 ( if patient is african american )  . on 10 may 2007 , initial feedback was obtained at a meeting between the hospital director staff ( av ) , the radiologist ( mgb ) and several clinical directors ( surgery , urology , oncology ) who had experienced difficulties in applying the protocol , and the forms were reviewed . 
on 22 and 30 may 2007 , two meetings were held between the hospital director staff , the radiologist , the reference nephrologist ( mc ) and endocrinologist ( pp ) , the clinical director of the clinical laboratory services ( cc ) and the union and scientific representatives of the general practitioners and community paediatricians of our area . 
proposals to improve the clarity and usability of the forms were incorporated , and procedures were established for arranging a nephrological consultation in selected cases and for admitting outpatients to the nephrology and dialysis unit for treatment before and after contrast injection . 
the radiology department purchased an oven to heat the contrast medium to body temperature , weighing scales with a heightmeasuring rod , and a timer for timing the observation of patients after the examination with icm ( from a minimum of 30 min to a maximum of 60 min in high - risk patients )  . during the first week of june , the radiologist ( mgb ) incorporated all revisions to produce a final draft of the patient history / screening form and informed consent form . on 12 june 2007 , the final document was posted on the hospital trust web site and transmitted to the hospital clinical directors , to the district directors and to the head of primary care services ( general practitioners and specialist services )  . anestesia , analgesia , rianimazione e terapia intensiva ( siaarti ) [ 1 ]  . il secondo progetto formativo , dal titolo nuovi strumenti di lavoro per la diagnostica per immagini ( una mattina per un totale di 4 ore , 2 crediti ecm ) stato presentato in quattro edizioni ( febbraio e marzo 2007 ) al personale medico ( ospedalieri , medici di medicina generale , pediatri di libera scelta , emergenza territoriale , distretti , guardia medica , etc . ) della nostra zona territoriale . dopo la conclusione dei progetti formativi , il 23 marzo 2007 stata trasmessa nota ai responsabili delle uu.oo. ospedaliere ed ai responsabili dei due distretti della nostra zona territoriale con le informazioni relative allutilizzo del nuovo modello per gli esami di imaging con mdc da impiegare in via sperimentale , affinch fosse portato a conoscenza di tutto il personale interessato . 
contemporaneamente il laboratorio di analisi dellospedale ha aggiunto nei suoi referti della creatininemia la stima del filtrato glomerulare ( fg ) calcolata automaticamente secondo la formula mdrd semplificata [ 6 ] , che si ottiene come segue : fg ( ml / min / 1 , 73 m2 ) = 186 ( creatininemia ) 1 , 154 ( et ) 0 , 2030 , 742 ( se di sesso femminile ) 1 , 210 ( se di razza afroamericana )  . il 10 maggio 2007 si svolta in direzione sanitaria [ a.v. ] una riunione preliminare tra il radiologo del gruppo [ m.g.b. ] ed alcuni primari ospedalieri ( chirurgia , urologia , oncologia ) che avevano riscontrato problemi nellapplicazione del modello , con rivalutazione del modello stesso ed acquisizione di suggerimenti . 
il 22 e 30 maggio 2007 sono state svolte in direzione sanitaria [ a.v. ] due riunioni con il radiologo del gruppo [ m.g.b. ] , convocando il nefrologo [ m.c. ] e lendocrinologo di riferimento [ p.p. ] , il primario del laboratorio di analisi [ c.c. ] , i rappresentanti sindacali e scientifici dei medici di medicina generale e dei pediatri di libera scelta della nostra zona territoriale . 
il modello stato rivalutato a seguito della sperimentazione e di nuove acquisizioni della letteratura [ 7 ] e sono stati recepiti suggerimenti finalizzati alla sua chiarezza dei contenuti ed alla fattibilit di utilizzo . stata codificata la procedura per la consulenza del nefrologo nei casi indicati e per la presa in carico dei pazienti ambulatoriali da parte della uoc di nefrologia e dialisi per la somministrazione della terapia indicata pree post - somministrazione di mdc . 
in radiologia sono stati acquisiti un fornetto per scaldare a temperatura corporea il mdc , una bilancia con asta graduata per la misura dellaltezza e dei timer per la misurazione del periodo di osservazione ( minimo 30 minuti , fino a 60 minuti nei pazienti a rischio ) del paziente dopo lesame contrastografico . 500 results the training course diagnostic imaging : national guidelines was successfully attended by 74.5% of the medical , nursing and technical staff of the radiology department ( 38 of 51 invited )  . 
the bls or blsd courses were successfully attended by 80% of the same personnel ( 44 of 55 invited )  . the training course new working tools for diagnostic imaging was successfully attended by 57.2% of doctors of our area ( 206 of 360 invited )  . two - sided page , one side containing the final version of the document ( available on our hospital trusts web site asp ? co_id = 6493 > modulo mezzo di contrasto ) consists of the patient history / screening form for elective examinations with injectable icm and the informed consent form , and the other providing guidance notes for completion and useful telephone numbers . 
the form contains sections on indications for the examination and the patients clinical data ( inclusive of possible neoplasms and surgical operations ) , and any risk factors for the use of icm . 
if the gfr is less than 60 ml / min per 1.73 m2 of body surface , a nephrological consultation must be arranged before the examination to prevent possible nephrotoxic damage . 
for adults , among the various recommended methods [ 11 , 12 ] , we decided to continue using the classic cockcroftgault formula [ 13 ] , with which we are familiar . 
the formula was modified by replacing body weight in numerator position with ideal body weight ( useful also in obese or pathologically underweight patients ) : gfr = [ 140 - age ( in years ) ] ideal body weight ( in kg ) / [ 72 serum creatinine ( in mg / dl ) ]  . 
ospedaliere , ai direttori di distretto ed al responsabile delluos medicina di base e specialistica per lopportuna diffusione . risultati il progetto formativo la diagnostica per immagini : linee guida nazionali di riferimento stato seguito con profitto dal 74 , 5% del personale medico , infermieristico e tecnico della radiologia ( 38 persone su 51 convocati )  . 
il progetto formativo nuovi strumenti di lavoro per la diagnostica per immagini stato seguito con profitto dal 57 , 2% dei medici della nostra zona territoriale ( 206 persone su 360 convocati )  . il modello definitivo ( disponibile sul nostro sito aziendale allindirizzo co_id = 6493 > modulo mezzo di contrasto ) in due facciate , comprende un fronte ( informativa per gli esami di diagnostica per immagini programmati con mezzi di contrasto organo - iodati per via iniettiva , consenso informato ) ed un retro ( note , numeri di telefono utili )  . 
linformativa , necessaria per procedere allesecuzione dellesame , deve essere compilata e firmata dal medico inviante e dal paziente . dopo le notizie relative allindicazione allesame ed alla sintesi clinico - anamnestica del paziente ( comprensiva di eventuali neoplasie ed interventi chirurgici ) , vengono riportati gli eventuali fattori di rischio alluso del mdc . 
la valutazione di laboratorio della sola creatininemia ci ha fatto abbassare la spesa da 11 , 40 euro a 1 , 50 euro a paziente ( risparmio del 86 , 8% ) rispetto al passato . dalla cratininemia viene richiesto , nella nota informativa , di calcolare il fg stimato , usando le formule riportate nel retro del modulo . 
se il filtrato glomerulare risulta inferiore a 60 ml / min / 1 , 73 m2 di superficie corporea necessario ricorrere ad una consulenza nefrologica prima dellesecuzione dellesame con mezzo di contrasto organo - iodato per prevenire leventuale danno nefrotossico . 
per let pediatrica stata considerata la formula di schwartz [ 810 ] : fg = k altezza ( in cm ) / creatininemia ( in mg / dl ) , dove k uguale a 0 , 33 nel pretermine , 0 , 45 nel bambino nato a termine e fino a 12 mesi di et , 0 , 55 nel bambino dal compimento del primo anno fino a 13 anni , successivamente e fino a 18 anni 0 , 55 nelle femmine e 0 , 65 nei maschi . 
as a result , in consideration of the number of examinations with icm performed in patients older than 60 years at our centre ( 71% , and specifically , 57% of patients aged 6180 years and 14% of patients aged over 80 years ) , the clinical laboratory services have restricted the use of automatic gfr calculations from serum creatinine to patients aged 1860 years only until a large enough case series has been collected to enable comparison of the two formulas across our patient population . to date , at least 80% of patients have presented to the radiology department on the day of the examination without any indication of estimated gfr noted on the patient history / screening form by the referring physician , with no substantial difference between inpatients and outpatients . 
in all patients , the radiology department nursing and medical personnel independently evaluate this parameter , even when already calculated , by using the formulas reported on the back of the patient history / screening form . on average 20% of patients scheduled for an examination with icm have abnormal estimated gfr on the day of the examination ( < 60 ml / min per 1.73 m2 , significant renal insufficiency )  . 
the nephrologist assesses the patient for risk factors , quantifies the risk ( table 1 ) and prescribes the prophylactic treatment to be administered in connection with the examination , hydration with isotonic saline solution and administration of n - acetylcysteine . 
table 1 is derived from a study on the intra - arterial administration of contrast medium [ 14 ] , which used a semiquantitative method for calculating contrast - induced risk . the fact that the risk of contrast - induced nephropathy may be higher with intra - arterial contrast administration [ 15 ] allows for a greater safety margin in our patients , who receive intravenous icm . 
in particular , with regard to hydration , our policy is to administer 0.9% saline solution intravenously at a dose of 1.01.5 ml / kg per hour , as suggested by the recent literature [ 16 ]  . 
whereas there is no problem starting the infusion 12 h before the examination and afterwards continuing it for at least 12 h in inpatients , in outpatients we are obliged to reduce administration times to 3 h before and 6 h after the examination . 
in addition to hydration , patients receive 600 mg oral n - acetylcysteine twice daily the day before and the day of sica formula di cockcroft - gault [ 13 ] , modificata mettendo al numeratore , al posto del peso corporeo , il peso corporeo ideale ( utile anche nei pazienti obesi o patologicamente magri ) : fg = [ 140 - et ( in anni ) ] peso corporeo ideale ( in kg ) / [ 72 creatininemia ( in mg / dl ) ]  . 
a titolo esemplificativo , nel normotipo , i valori limite di creatininemia sono 40 anni : uomo > 1 , 67 ; donna > 1 , 42 ; 65 anni : uomo > 1 , 25 ; donna > 1 , 06 ; 80 anni : uomo > 1 , 00 ; donna > 0 , 85 . per quanto riguarda la formula mdrd semplificata , nella nostra preliminare esperienza ( periodo 1 aprile15 maggio 2007 ) abbiamo rilevato in alcuni pazienti anziani un valore di fg stimato maggiore della soglia di 60 a fronte di un valore inferiore alla medesima soglia nel calcolo eseguito con la formula di cockcroft - gault . 
di conseguenza , alla luce dellalta prevalenza di esami con mdc in pazienti di et superiore a 60 anni nella nostra realt operativa ( 71% , ed in particolare 57% dei pazienti con et compresa tra 61 e 80 anni e 14% dei pazienti con et superiore a 80 anni ) , il laboratorio di analisi ospedaliero dal giugno 2007 ha eseguito il calcolo automatico del fg dalla creatininemia solo nella fascia di et 1860 anni , in attesa di poter raccogliere una ampia casistica di confronto tra le due formule nella nostra popolazione . fino al momento attuale almeno l80% dei pazienti giunge in radiologia il giorno dellesame senza che sia riportato nella nota informativa il calcolo del fg da parte del medico inviante . 
in ogni paziente il personale infermieristico e medico della radiologia valuta indipendentemente questo parametro , anche se gi calcolato , impiegando le formule riportate nel retro del modulo . in media il 20% dei pazienti prenotati per un esame con mdc mostra il giorno dellesame un fg stimato patologico ( < 60 , insufficienza renale significativa )  . 
il paziente con insufficienza renale viene riprenotato nellagenda degli appuntamenti della radiologia e contemporaneamente indirizzato allambulatorio nefrologico per lopportuna valutazione e preparazione allesame con mdc ( consulenza nefrologica e profilassi dei danni da somministrazione di mezzo di contrasto )  . 
il nefrologo valuta il paziente per i fattori di rischio alla somministrazione del mdc , quantizza il rischio stesso ( tabella 1 ) e prescrive la profilassi , da eseguirsi in connessione allesame con mdc mediante idratazione con soluzione fisiologica isotonica e somministrazione di acetilcisteina . 
la tabella 1 stata derivata da uno studio eseguito per la somministrazione intra - arteriosa di mdc [ 14 ] , in cui si usata una metodica di calcolo semiquantitativo del rischio da mdc . 
the usefulness of n - acetylcysteine in preventing contrast - induced nephropathy [ 19 ] is still being debated in the literature ; however , until conclusive evidence becomes available , we believe it reasonable to continue its use , as it is inexpensive , simple to administer and free of side effects . 
in particolare per lidratazione del paziente abbiamo seguito i consigli della recente letteratura [ 16 ] con la somministrazione di soluzione fisiologica 0 , 9% per via venosa alla dose di 1 , 01 , 5 ml / kg / ora . mentre nel paziente ricoverato non abbiamo problemi ad iniziare linfusione 12 ore prima dellesame con mdc ed a continuarla per almeno 12 ore dopo lindagine , nel paziente ambulatoriale siamo obbligati a ridurre la tempistica a 3 ore prima ed a 6 ore dopo lindagine . 
allidratazione abbiamo aggiunto la somministrazione di acetilcisteina per os secondo queste dosi : 600 mg due volte al giorno , per due giorni a partire dal giorno precedente allesame con mdc [ 18 ]  . 
in letteratura lutilit dellacetilcisteina per la prevenzione della nefropatia da mdc assai controverso [ 19 ] , ma in attesa di conoscere dati conclusivi sullargomento , noi labbiamo impiegata perch poco costosa , somministrabile facilmente e priva di effetti collaterali . 
se ritenuto necessario il nefrologo prescrive un dosaggio della creatininemia dopo lesame con mdc ( a 12 , 24 , 36 o 48 ore a seconda del caso ) , considerando come nefropatia da mezzo di contrasto [ 20 ] un aumento del 25% della creatininemia entro 3 giorni dalla somministrazione del mdc . 
inoltre per prevenire leventuale acidosi lattica [ 21 ] , ai pazienti diabetici in terapia con metformina viene prescritta la sospensione del farmaco 48 ore prima dellesame con mdc , con ripresa della terapia antidiabetica orale 48 ore dopo , previa verifica della funzionalit renale . 
per gli esami non programmabili stato istituito un protocollo di profilassi rapido ( soluzione di bicarbonato di sodio 1 , 4% : 3 ml / kg in unora prima della somministrazione del mdc , seguiti da una dose di 1 ml / kg / ora per 6 ore dopo linfusione del mdc [ 22 ] )  . 
 in addition , to prevent possible lactic acidosis [ 21 ] , diabetic patients receiving metformin are instructed to discontinue the medication 48 h before and not resume it until 48 h after the examination , after renal function has been evaluated . 
a quick prophylactic protocol has been developed for nonelective examinations ( 1.4% sodium bicarbonate : 3 ml / kg 1 h before icm injection , followed by 1 ml / kg per hour for 6 h after icm injection [ 22 ] )  . 
these include hyperthyroidism ( table 2 ) , previous allergic reactions to iodinated substances and / or previous adverse reaction to icm and severe asthma or allergy ( evaluation by allergologist and anaesthesiologist before the day of the examination , with eventual desensitisation therapy prior to examination ) , need for sedation / general anaesthesia ( preliminary evaluation by anaesthesiologist in uncooperative patients )  . 
 the patient history / screening form then reminds the referring physician and the patient of the need to bring along to the examination any previous relevant documentation and requests information on the patients weight and height to dose the amount of icm required . 
with regard to the maximum dose of contrast medium , it was reported almost 20 years ago that in the case of renal insufficiency , the maximum dose should be 5 ml of icm per kilogram of body weight divided by the creatinine value [ 23 ]  . 
per quanto riguarda la dose massima di mdc da somministrare al paziente , quasi venti anni fa stato segnalato in letteratura che in caso di insufficienza renale bisogna considerare una dose limite di 5 ml di mdc per kg di peso corporeo diviso il valore della creatininemia [ 23 ]  . 
per i mdc attualmente in uso lesur [ 24 ] ha segnalato che nei pazienti adulti con normale funzionalit renale non si dovrebbero superare i 400 ml di mdc ( alla concentrazione di 300 mg di iodio per ml ) , mentre la dose andrebbe drasticamente ridotta nei pazienti con compromissione della funzionalit renale ( 150 ml se linsufficienza renale modesta , 100 ml se linsufficienza renale grave )  . 
anche il cin consensus working panel ha raccomandato di mantenersi ad una dose minore di 100 ml di mdc nei pazienti con fg < 60 ml [ 15 ]  . 
infine il paziente viene informato che sconsigliato ripetere un esame con mdc prima che sia trascorsa almeno una settimana da una precedente analoga somministrazione . segue la parte del consenso allatto radiologico , da compilare e firmare nel corso del colloquio preliminare tra il medico radiologo ed il paziente . 504 table 2 thyroid function radiol med ( 2009 ) 114 : 496508 evidence of manifest hyperthyroidism is a contraindication to the administration of iodinated contrast media . subjects at risk of thyrotoxicosis after iodinated contrast media ( icm ) administration are patients with basedow disease and multinodular toxic goitre , especially those living in areas with dietary deficiency of iodine and / or elderly patients . patients at risk should be monitored after icm administration by means of thyroid - stimulating hormone ( tsh ) and ft4 testing , preferably by an endocrinologist . in selected high - risk patients , tsh and ft4 testing may be performed , and prophylactic pharmacological treatment may be given prior to icm administration . 
 tabella 2 funzionalit tiroidea levidenza di franco ipertiroidismo una controindicazione alla somministrazione di mezzi di contrasto organo - iodati . sono a rischio di tireotossicosi dopo somministrazione di mezzi di contrasto organo - iodati i pazienti con morbo di basedow e gozzo multinodulare tossico , specie se residenti in aree geografiche a carenza iodica e / o anziani . questi pazienti a rischio dovrebbero essere monitorati dopo lesame con mezzi di contrasto organo - iodati mediante il dosaggio di tsh e ft4 , preferibilmente dallendocrinologo . in pazienti ad alto rischio selezionati possono essere indicati il dosaggio di tsh e ft4 ed una eventuale profilassi farmacologica tireostatica prima dellesame con mezzi di contrasto organo - iodati . used icm , the european society of urogenital radiology ( esur ) [ 24 ] stated that in adults with normal renal function , the maximum recommended dose is 400 ml icm ( at a concentration of 300 mg of iodine per millilitre ) , whereas this amount should be drastically reduced in patients with renal insufficiency ( 150 ml if moderate , 100 ml if severe )  . even the contrast - induced nephropathy consensus working panel recommended a dose of icm less than 100 ml in patients with gfr < 60 ml [ 15 ]  . 
finally , the patient is informed that it is inadvisable to repeat an examination with icm before at least 1 week has passed after a previous icm administration . the patient history / screening form is followed by the informed consent form , to be filled in and signed during the verbal interview between the radiologist and patient prior to the examination . discussion the aim of this paper is to share our experience in addressing the problem of icm use so as to assist others seeking to tackle the same problem in their setting . 
the excellent and exhaustive material made available by sirm [ 1 , 2 ] regarding the new guidelines for the use of injectable contrast media had had insufficient uptake among both discussione lo scopo del presente lavoro stato quello di voler condividere la nostra esperienza di fronte al problema dellimpiego dei mdc , perch possa essere di aiuto a chi si trovi nella propria realt operativa a dover affrontare unanaloga situazione . 
lottimo ed esaustivo materiale pubblicato in ambito societario [ 1 , 2 ] sui nuovi orientamenti nelluso del mdc per via iniettiva non aveva avuto nella nostra zona una sufficiente divulgazione , sia tra gli specialisti in radiologia che tra i medici invianti , per far sentire come necessario un cambiamento radicale nellapproccio al problema ( preparazione del paziente , nota informativa , consenso informato , addestramento del personale alla gestione delle reazioni avverse al mdc )  . 
di qui la necessit di una rivisitazione locale della problematica con i referenti non radiologi interessati ( nefrologo , anestesista rianimatore , endocrinologo , allergologo , medico legale , direzione medica ospedaliera ) , affrontata con entusiasmo da tutti i colleghi coinvolti . 
molto pi difficile nella nostra esperienza stata ( ed tuttora ) la condivisione della problematica con gli altri . per quanto riguarda il personale della radiologia , dal punto di vista concettuale , le perplessit ed i dubbi rilevati nelle riunioni di reparto del 2004 e del 2005 sono stati chiariti con la buona partecipazione del personale ai corsi bls o d - bls ed al progetto formativo la diagnostica per immagini : linee guida nazionali di riferimento , utile radiol med ( 2009 ) 114 : 496508 radiologists and referring physicians in our area , calling for a radical change in the approach to the problem ( patient preparation , patient history / screening , informed consent , training of personnel in the management of adverse reactions to icm )  . 
the issue of icm use was thus revisited locally with all the professionals , other than radiologists , involved in the process ( nephrologist , anaesthetistresuscitator , endocrinologist , allergologist , legal medicine specialist , hospital management ) , an opportunity that was met with enthusiasm by all concerned . 
 we experienced ( and still experience ) far more difficulty in sharing the project with other professionals . with regard to radiology department personnel , conceptually , the concerns and doubts aired at the meetings held in 2004 and 2005 were solved , with a good level of participation in the bls and blsd courses and the training course diagnostic imaging : national guidelines , which also served as a refresher course on indications for radiological procedures and the use of the various imaging modalities in individual clinical cases . in practice , whereas gfr calculation has become routine practice at our radiology department , there are still problems with the 20% of patients who are found to have a pathological gfr on the day of the examination , causing major logistic difficulties in rescheduling the examinations to a date compatible with management of the patients condition . the reason for this is , we believe , the fact that despite their moderately good level of participation in the course new working tools for diagnostic imaging and their extensive involvement in the project ( through meetings with their scientific and union representatives ) , referring physicians still do not feel the problem of icm use in a homogeneous manner . 
preliminary evaluation of the gfr appears to be the cornerstone of the entire process of preventing icm - induced toxicity , and advance gfr evaluation by the referring physician allows proper patient preparation to be planned . 
failure to evaluate the gfr exposes the patient to the risk of not being able to undergo contrast administration on the day of the examination ( scheduled with great difficulty given the normal waiting lists ) , with obvious consequences on patient care ; on the other hand , it is difficult for the radiology department to reschedule examinations for which there is no alternative and that become increasingly urgent over time . we therefore believe that serum creatinine determination with gfr calculation needs to be done at the time of referral , whether examinations are performed on inpatients , urgent outpatients or elective outpatients . 
furthermore , we believe that another refresher course on the subject , scheduled for 2009 for both physicians and nurses in our area , may be more effective than sending out formal and informal reminders for them to fill in the patient history / inoltre per aggiornare chi ne avesse bisogno anche sullindicazione agli esami e sulluso delle varie metodiche di imaging nel singolo caso clinico . dal punto di vista pratico , mentre ormai entrato nella routine lavorativa della nostra radiologia il calcolo del fg , grandi disagi ancora derivano da quel 20% di pazienti che vengono quotidianamente rinviati il giorno dellesame per il riscontro in diagnostica di un fg patologico , con grosse difficolt logistiche nel riprogrammare tali esami in tempi utili per la gestione della malattia del paziente . 
ci dovuto a nostro avviso al fatto che i medici invianti , nonostante la discreta partecipazione al progetto formativo nuovi strumenti di lavoro per la diagnostica per immagini ed al loro ampio e prezioso coinvolgimento ( attraverso gli incontri con le loro rappresentanze scientifiche e sindacali ) , non sentono ancora in maniera omogenea la problematica . e , fra tutti i fattori di rischio , la valutazione preliminare del fg appare nella nostra esperienza come il punto cardine di tutto il processo . 
la mancata valutazione preliminare del fg invece espone il paziente al rischio di non poter effettuare lesame con mdc il giorno dellappuntamento ( programmato con fatica viste le normali liste di attesa ) , con ovvie conseguenze sulla gestione della sua malattia , e la radiologia a non sapere quanto riprogrammare esami che bisogna in ogni caso fare e che pi tempo passa pi diventano urgenti . 
pensiamo quindi che sia necessario verificare il valore della creatininemia con il calcolo del fg gi al momento della prenotazione degli esami dei pazienti ricoverati ed ambulatoriali urgenti , nonch degli ambulatoriali programmati nel tempo . 
per questi ultimi , se a rischio per nefropatia da mdc , tale verifica andr ripetuta anche in stretta prossimit della data di esecuzione dellindagine con mdc . inoltre al proposito pensiamo che un nuovo progetto formativo di rinforzo sullargomento , gi in programma per lanno prossimo ( sia per i medici che per gli infermieri professionali della nostra zona territoriale ) , possa essere pi utile dei richiami informali e formali gi effettuati per una compilazione completa ( comprensiva del calcolo del fg ) della nota informativa . infatti utile ribadire come la prevalenza di insufficienza renale non nota nella popolazione elevata ( fg < 60 = 7 , 4% [ 25 ] )  . 
questo ovviamente risulta tanto pi vero quanto pi il soggetto anziano ( fisiologico calo della funzionalit renale di 1 ml / min per anno dopo i 2030 anni di et [ 26 ] ) , vasculopatico o sottoposto a terapia con farmaci nefrotossici ( tipo la chemioterapia )  . 
daltra parte essenziale cercare di evitare il pi possibile il danno della funzionalit renale dovuto alluso non prudente del mdc ( linsufficienza renale da mdc stata stimata come la terza causa di insufficienza renale acuta in ospedale [ 27 ] )  . 
a tal proposito 506 radiol med ( 2009 ) 114 : 496508 screening sheet completely ( including gfr calculation )  . it should be emphasised that the prevalence of undetected renal insufficiency in the general population is high ( gfr < 60 ml = 7.4% [ 25 ] )  . 
this is particularly true in the elderly ( renal function decreases physiologically by 1 ml / min per year after the age of 2030 years [ 26 ] ) and in subjects with vascular disease or undergoing treatment with nephrotoxic agents ( such as chemotherapy )  . 
on the other hand , it is important to minimise the risk of renal impairment due to the imprudent use of contrast media ( icm - induced nephrotoxicity is reported to be the third leading cause of acute renal failure in a hospital setting [ 27 ] )  . 
the possibility of a logistic support system in charge of prophylactic treatment before and after icm administration , such as the one activated at our nephrology and dialysis department , is thus essential . 
 owing to the lack of agreement in the literature on the subject of nephrological consultation ( only with gfr < 30 ml [ 28 ] ; in all patients with gfr < 60 ml [ 29 , 30 ] ) , we initially opted for nephrological consultation in all patients with gfr < 60 ml . 
the gfr threshold value required for nephrological consultation may be lowered in the future should it be demonstrated that this is not detrimental to the patient . because it is impossible to routinely request determination of actual gfr ( measured as creatinine clearance = urine creatinineurine volume in 1 min / serum creatinine ) , which requires 24 - h urine collection , we decided to use the cockcroftgault formula for gfr estimation [ 13 ] , which we have used successfully for many years . 
the method is also inexpensive ( it requires only serum creatinine determination : cost = 1.50 euro ) and is thus suitable for screening purposes . its main disadvantage , in our experience , is that it does not allow for the automatic calculation of gfr , as the hospital clinical laboratory does not record patients weight and height . 
 another recently proposed formula is the mdrd [ 31 ] : gfr = 170 ( serum creatinine ) 0.999 ( age ) 0.176 ( blood urea nitrogen ) 0.170 ( serum albumin ) 0.3180.762 ( if patient is female ) / 1.73 m2 ( of body surface )  . 
this led us to perform an in - depth comparison of the cockcroftgault and simplified mdrd formula in each patient in quindi riteniamo indispensabile lattivazione di un percorso che coinvolga il nefrologo per i pazienti a rischio . 
la possibilit di un supporto logistico competente per il paziente ambulatoriale per la profilassi pree post - somministrazione di mdc , come quello da noi attivato presso la nefrologia e dialisi ospedaliera , risulta quindi essenziale . avendo ritrovato in letteratura dati discordanti sullargomento ( consulenza nefrologica solo con fg < 30 [ 28 ] ; consulenza nefrologica in tutti i pazienti con fg < 60 [ 29 , 30 ] ) , abbiamo optato inizialmente per la consulenza nefrologica in tutti i pazienti con fg < 60 . 
anche se ci comporta un notevole carico di lavoro , vogliamo poter verificare in tutti questi pazienti eventuali modificazioni della funzionalit renale indotte dalluso del mdc , riservandoci in futuro di ridurre il valore del fg necessario per la consulenza nefrologica se dimostreremo nella nostra popolazione che ci possa essere fatto senza detrimento per il paziente . non essendo possibile nella routine pratica richiedere la valutazione reale del fg ( misurato come clearance della creatinina = creatinina urinaria volume urinario al minuto / creatinina plasmatica ) , che necessita della raccolta completa delle urine delle 24 ore , tra le formule a disposizione per la stima del fg , abbiamo scelto quella di cockcroft - gault [ 13 ] perch la usiamo con soddisfazione clinica da molti anni . 
il suo svantaggio principale nella nostra esperienza quello di non consentire un calcolo automatico del fg , dal momento che non vengono registrati al laboratorio di analisi il peso e laltezza dei pazienti . 
tale formula , validata , utile soprattutto nei pazienti con insufficienza renale avanzata , si presterebbe ad una valutazione automatica del fg da parte del laboratorio di analisi , ma necessit di pi dosaggi ( costo = 4 , 5 euro ) rispetto alla cockcroft - gault e quindi ha un costo maggiore . 
nella letteratura inoltre il suo confronto con la formula di cockcroft - gault non ne ha ancora dimostrato una definitiva maggiore affidabilit , in particolare nel paziente anziano [ 32 ]  . 
i dati in proposito sono in corso di raccolta e quando avranno raggiungo un congruo numero saranno oggetto di un successivo lavoro . per quanto riguarda i tempi tra il dosaggio della creatininemia e lespletamento dellesame con mdc , nel modello radiol med ( 2009 ) 114 : 496508 our population . 
on this subject , the esur guidelines [ 35 ] state that , even in areas with dietary iodine deficiency , as is ours , there is no need to evaluate thyroid function before icm administration in patients without clinical evidence of thyroid disease . 
moreover , because the bottles of contrast medium always contain amounts of free iodine ( much higher than the daily requirements ) , the esur considers patients with basedows disease and toxic nodular goitre as being at risk of developing thyrotoxicosis after icm administration , especially those living in areas with dietary iodine deficiency and / or the elderly . 
 finally , with regard to collaboration with the anaesthetistresuscitator , the ministerial circular of 17 / 09 / 97 [ 1 ] recommends only preliminary consultation with the anaesthesiologist and his / her presence in the hospital during the performance of examinations with icm on patients at risk for adverse reactions . 
however , in consideration of the distance between the radiology department and the operating theatre suite , we request that the anaesthesiologist is physically present in the radiology department during the examination . non si impone un tempo definito ( per esempio un massimo di un mese ) , ma si richiede lindicazione della data del dosaggio di laboratorio , per potersi regolare caso per caso , dal momento che nel paziente con buona funzionalit renale viene accettato anche un tempo di sei mesi [ 34 ] , mentre nel paziente con insufficienza renale pu essere necessario un dosaggio anche pi recente di una settimana . per quanto riguarda altri fattori di rischio alluso del mdc , ci sembra utile segnalare che , limitatamente al periodo sperimentale di 1 , 5 mesi di impiego del modello , i problemi riscontrati hanno riguardato anche la funzionalit tiroidea , con una transitoria esplosione di richieste di dosaggio di ft3 , ft4 e tsh , non giustificata dalla situazione clinica dei pazienti . 
al proposito le linee guida dellesur [ 35 ] chiariscono che , anche in aree geografiche con carenza di iodio come la nostra , non vi alcuna necessit di un dosaggio di laboratorio della funzione tiroidea prima di esami con mdc in pazienti clinicamente normali da questo punto di vista . 
inoltre , dal momento che i flaconi di mdc contengono sempre quantit di iodio libero ( di molto superiori al fabbisogno quotidiano ) , lesur cataloga i malati con morbo di basedow e gozzo multinodulare tossico come pazienti a rischio di sviluppare una tireotossicosi dopo la somministrazione di mdc , specie se residenti in aree geografiche a carenza iodica e / o anziani . 
the authors provide a simple yet exhaustive introduction to the concept of file format and describe the algorithms and main features of the most common formats ( bmp , jpeg , gif , dicom , tif , png ) and portable network graphics ( png )  . 
 the different formats are compared in terms of dimension , quality , portability and with reference to the following specific needs : electronic communications , publication on the world wide web , presentation of electronic posters , video presentations for teaching and manuscript publishing . 
we also illustrate how to handle the various formats with the programmes supplied with standard software installations . the large number of digital applications of image file formats calls for a simplification in daily radiological practice . 
we recommend the use of jpeg and png for electronic communications ; png and gif for publication on the worldwide web ; jpeg and png for electronic poster presentations ; dicom , png and jpeg for teaching presentations ; tif and png for printing on paper . riassunto evidenziare le differenze tra i pi comuni formati di salvataggio delle immagini radiologiche digitali . suggerire un uso appropriato e garantire la facilit di manipolazione nella gestione delle pi tipiche applicazioni pratiche nel lavoro quotidiano in radiologia . vengono presentati in modo semplice ma esaustivo il concetto di formato file , gli algoritmi dei formati pi comuni ( bmp , jpeg , gif , dicom , tif , png ) e le loro caratteristiche principali . vengono messi a confronto i differenti formati in base a dimensioni , qualit , portabilit ed in relazione alle seguenti situazioni specifiche : comunicazione elettronica , pubblicazione su pagine internet , presentazione di poster elettronici , comunicazioni didattiche , stampa di pubblicazioni . 
viene inoltre illustrato come gestire tali formati con i programmi che sono distribuiti assieme alle installazioni software standard . le numerose applicazioni digitali dei file immagine rendono dobbligo una semplificazione nella pratica radiologica quotidiana . 
in this context , it is very difficult to obtain that broad overview of the subject that is essential for selecting the most appropriate image file format for specific situations . 
 moreover , there is a widespread casualness in handling images , in part due to indifference in the choices made when sending e - mails , displaying images on screen or organising an institutional policy for image storage . 
such inappropriate decisions can result in minor or major mishaps that may be more or less strongly perceived ; for example , obliging a colleague to wait an additional 35 min at the monitor to download an attachment or , far worse , being obliged to continuously purchase supplementary hard disks because the storage server has reached full capacity . as it is not necessary to go into extreme detail to master the competences required to handle these tasks , we felt it might be useful to provide an overview of common resources and give a few simple recommendations , in plain language and using concrete examples . introduzione la gestione delle immagini digitali nella quotidiana pratica radiologica pu essere molto complicata . 
 assistiamo inoltre ad una diffusa leggerezza nella gestione delle immagini , in parte sostenuta da una certa indifferenza , nelle scelte che si operano quando si decide di inviare una email , di presentare a video delle immagini , o di organizzare una politica di archiviazione di istituto . 
si passa dallobbligare un collega ad attendere tre / cinque minuti in pi davanti ad un monitor per scaricare un allegato , a quello ben pi costoso di costringerci continuamente allacquisto di unit disco supplementari perch il nostro server di archiviazione gi pieno . dal momento che non necessario scendere nel dettaglio per impadronirsi delle competenze utili in tale direzione , ci parso appropriato stendere una panoramica delle risorse di uso comune e qualche semplice linea guida , senza mai sacrificare la semplicit del linguaggio , attraverso esempi concreti . image formats i formati immagine digital images are handled by computers as a grid of rows and columns of coloured dots , something like a battleship grid . 
each square corresponds to a dot on the screen a pixel which represents the elementary unit of every image . each pixel is characterised not only by its colour but by its coordinates that is , by its position within the image . 
otherwise , we could describe the content of each square in order , by announcing first row : water , water , water , ship , water second row : water , ship , ship and so on . 
in computing , these different techniques for describing the same image are known as formats . a format is a standardised method , that is , one that can be reproduced on any computer , for reading and arranging the le immagini digitali sono gestite da un computer come una griglia di righe e colonne di punti colorati , simili ad una tavola da battaglia navale . 
immaginiamo il seguente esempio : una griglia da battaglia navale di dieci righe per dieci colonne . essa contiene cento caselle , di cui la maggior parte sono azzurre ( lacqua appunto ) , ed una minore parte sono grigie , poich occupate dalle navi . 
oppure si potrebbe descrivere il contenuto di ogni casella ordinatamente , dichiarando prima riga : acqua , acqua , acqua , nave , acqua , seconda riga : acqua , nave , nave , e cos via . 
o ancora si potrebbe dire prima riga : tre caselle di acqua , una occupata da una nave , poi acqua fino a fine 486 radiol med ( 2009 ) 114 : 484495 fig . 
however , all formats can be classified according to three main features : the size of the image file , the maximum number of colours and possible loss of detail . 
 in particular , the size of the image file refers to the amount of physical memory ( in kilobytes or megabytes ) that a file takes up on a storage device . 
compression algorithms are extremely important , as the amount of memory needed to store an image can be reduced to the point that the image is several times smaller than the original . 
queste differenti tecniche di descrivere la stessa immagine sono note in informatica con il termine di formati . un formato un metodo standardizzato , ovvero riproducibile su qualsiasi pc , per leggere ed organizzare le informazioni contenute in un file . 
una volta selezionato un file immagine , il computer ne riconosce lestensione , abbina il formato corretto , e attua una precisa sequenza di operazioni per manipolare i dati e presentarli a schermo , chiamato algoritmo . 
ogni formato nasce per soddisfare particolari esigenze , ma tutti sono classificabili in base a tre caratteristiche principali : la dimensione del file immagine , il numero massimo di colori e leventuale perdita di dettaglio . 
 in particolare , con il termine dimensione del file immagine intendiamo la quantit di memoria fisica ( in unit kilobyte o megabyte ) che una immagine occupa su un supporto per memorizzarla . 
2 la stessa immagine , rappresentata con due profondit di grigi molto diverse . a destra , con una bassa profondit di colore , limmagine perde tutti i dettagli . whose size has been reduced by 90% will require only a tenth of time to be transferred from one peripheral device to another . 
some formats are very effective in compressing images ; others less so . the maximum number of colours refers to the colour depth , or the number of different colour nuances that the image can encode . 
this happens because each colour in the image will be specified much more accurately , with a larger series of digits . absence of loss of detail refers to the formats ability to preserve the individual details of the original image . 
as even minimal loss of data allows for very effective compression , some formats have been developed that expressly eliminate some barely perceivable details in favour of an excellent reduction in volume . 
alcuni formati sono eccellenti nel comprimere immagini , altri meno . con il termine numero massimo di colori , intendiamo la cosiddetta profondit del colore , ovvero il numero di differenti sfumature di colore che limmagine pu codificare . per fare un esempio pratico si pensi ad una proiezione pa di un torace . 
con una profondit del colore molto alta , ovvero con la possibilit di rappresentare milioni di tinte diverse , otteniamo una rappresentazione a video dellimmagine cos come siamo soliti pensarla , cio ricca di dettagli e di sottili differenze di sfumatura tra una struttura e laltra . allestremo opposto immaginiamo una profondit di colore di sole poche tinte . 
dal momento che anche piccole perdite di dati permettono una compressione molto efficace , si sono sviluppati alcuni formati che prevedono esplicitamente lo scarto di alcuni dettagli difficilmente percepibili in nome di una eccellente riduzione di volume . 
la conversione verso formati lossy accumula perdita di dati , che irreversibile . is thus a dot - by - dot description of the image , and for this reason , it is regarded as the standard of reference . 
the jpeg format has excellent colour depth , as it can have up to several million colours . the strength of this type of algorithm lies in its ability to reduce the size of images on the disk . 
essi sono i formati bitmap , jpeg , gif , dicom , tiff e png [ 18 ]  . formato bitmap un file immagine in formato bitmap costituito dalla serie di coordinate e colori di ogni singolo punto dellimmagine . si tratta quindi di una descrizione punto a punto dellimmagine , e per tale motivo limmagine bitmap considerata una misura di riferimento . 
il formato jpeg ha il grande pregio di permettere una compressione regolabile dallutente , che pu quindi scegliere quanto efficace essa debba essere . purtroppo ogni singolo programma di fotoritocco gestisce lefficacia della compressione jpeg in modo diverso . alcuni programmi , come ms paint , non danno affatto la possibilit di scegliere lefficacia della compressione , e ne utilizzano una pre - impostata , a basso rendimento . 
noi abbiamo usato come riferimento paint.net , poich si tratta di una alternativa gratuita a ms paint , semplice da usare e molto completa . va inoltre sottolineato come il formato jpeg sfrutti un algoritmo lossy , ovvero con una perdita di dati . 
il formato jpeg viene oggi impiegato soprattutto nel salvataggio e nella memorizzazione di immagini fotografiche , dove permette una minima perdita di dettaglio percepibile contro un grande vantaggio in termini di spazio di archiviazione . formato gif il formato gif un po obsoleto e molto sottodimensionato in quanto a caratteristiche . 
si tratta di un formato con forti limiti nella profondit del colore , e un algoritmo di compressione non particolarmente efficace su immagini fotografiche , che perdono notevolmente di dettaglio nella riduzione dei colori disponibili . 
sebbene infatti lalgoritmo gif sia teoricamente loss - less , nella pratica la conversione in questo formato di immagini di uso comune , come radiografie o fotografie , produce immagini assolutamente incomparabili alloriginale , a causa della sopracitata importante perdita di profondit di colore . 
the jpeg format is especially used for storing photographic images , where it allows a minimal loss of perceivable detail against major advantages in terms of storage space . gif format formato dicom the gif format is rather obsolete , and its features have been heavily reconsidered . 
the format has strong limitations in colour depth and employs a compression algorithm that is not very effective on photographic images , which lose considerable detail in the colour reduction process . 
in fact , although the gif algorithm is theoretically loss - less , in practice , the conversion of commonly il formato file dicom uno standard industriale [ 68 ] tuttora in sviluppo . 
ci vuol dire che un file dicom pu contenere una immagine a pieno dettaglio in formato bitmap , oppure compressa con algoritmo jpeg , 490 radiol med ( 2009 ) 114 : 484495 used images such as radiographs or photographs into gif produces images that are absolutely unlike the originals , owing to the substantial loss of colour depth . 
for this reason , the gif format is preferred for web pages , which tend to contain many of these elements . dicom format the dicom format is an industrial standard [ 68 ] that is still being developed . 
it is an anomalous format that does not introduce any new compression algorith instead , it merely encapsulates , or contains , an image in the format in which it was produced . 
however , the main difference between the two formats is that dicom is able to memorise a series of data not necessarily linked to the image , such as the patients demographic information , type of examination , date and time of the examination and so on . 
for this reason , dicom images are particularly suited for use in integrated reporting workstations or software - based reconstructions , but there is no difference in the quality of the image itself . also , as with the bmp format , dicom often generates very large images that are difficult to store . 
tipicamente le immagini dicom prodotte dalle apparecchiature radiologiche sono riproduzioni non compresse dellimmagine originale , e per questo motivo sono comparabili a delle immagini bitmap , di cui ereditano le caratteristiche . 
tuttavia la grande differenza tra questi due formati che il dicom in grado di memorizzare una serie di dati non necessariamente legati allimmagine visiva , come i dati anagrafici del soggetto , il tipo di esame , la data e lora di esecuzione , e cos via . 
per questo motivo esse sono molto pratiche nelle console di refertazione integrate o nelle ricostruzioni tramite software , ma non si distinguono dagli altri formati per nessuna vera qualit riferibile allimmagine stessa , anzi , parimenti al formato bitmap spesso producono immagini di grandi dimensioni , poco pratiche da archiviare . 
purtroppo i file tiff sono molto voluminosi , e per questo motivo non sono molto utilizzati , se non per scopi di archiviazione di immagini molto importanti , campo in cui si impongono come prima scelta . 
esso stato sviluppato appositamente per concentrare i punti di forza di molti formati in uno solo . le principali qualit delle immagini png risiedono in una buona compressione senza perdita di dati ( loss - less ) , nella capacit di supportare profondit di colore molto alte , e nella gestione delle trasparenze . 
sempre pi programmi supportano questo formato , e probabilmente il formato png si imporr a breve termine come unalternativa estremamente valida nei compiti di archiviazione e stampa [ 4 ]  . png format discussione png ( pronounced ping ) is the newest among the image file formats discussed here . 
it was specifically developed to combine the strengths of several formats in a single format . the main qualities of png images include efficient lossallo scopo di illustrare pi chiaramente le differenze tra i diversi formati che abbiamo discusso , e prefigurarne un utilizzo pratico , abbiamo allestito una semplice tavola sinottica che ne riassuma le caratteristiche essenziali radiol med ( 2009 ) 114 : 484495 less compression , very high colour depths and ability to handle transparencies . 
a growing number of programmes support this format , and it is likely that png will soon impose itself as an extremely valuable option for storage and print publishing [ 4 ]  . discussion the differences and practical uses of the various formats discussed in this paper are summarised in the synoptic table ( table 1 )  . 
per rendere lidea della capacit di compressione dei vari formati abbiamo ideato un semplice test . abbiamo convertito una immagine di riferimento bitmap di 466382 pixel raffigurante una proiezione pa di un torace , nei formati jpeg , gif , tiff e png . 
abbiamo quindi indicato nella colonna efficacia compressione torace la dimensione finale del file , dove a percentuali pi basse corrisponde una dimensione file minore ( e quindi una compressione pi alta ed una relativa perdita di dettaglio ) ( tabella 1 )  . 
 per quanto riguarda lutilizzo pratico delle immagini , nella routine radiologica le situazioni che ne richiedono un uso accorto sono essenzialmente : linvio tramite posta elettronica , la pubblicazione di immagini su pagine internet , la preparazione di poster elettronici illustrati , la presentazione a video di diapositive e limpaginazione di elaborati per la stampa cartacea . table 1 synoptic table of the main features of the various file formats . 
a questo punto nel menu a tendina salva come : possibile selezionare il formato di destinazione . of the compressed file and indicated the output file size in the column titled compression effectiveness chest , where low percentages correspond to smaller file sizes ( and to a higher compression ratio and relative loss of detail ) ( table 1 )  . 
in such situations , the png format can be used , as it offers good compression performance without sacrificing the information that the image must convey . web publishing when publishing images on the internet , special attention should be paid to the size of image files because in that context , it is more important to provide users with a smooth comunicazione elettronica ( e - mail ) nellinvio di immagini attraverso la rete internet , e in particolar modo quando si tratta di pi immagini , fondamentale considerare la dimensione dei file che vogliamo inviare . 
dal momento che il formato jpeg un formato lossy , in alcune occasioni consigliabile optare per una soluzione che preservi tutti i dettagli dellimmagine di partenza , a scapito dellefficacia di compressione . 
in tali situazioni pu essere consigliabile adoperare il formato png , che presenta una buona compressione senza sacrificare linformazione che deve veicolare limmagine . pubblicazione su internet quando si desidera pubblicare immagini su una pagina web bisogna prestare particolare attenzione alle dimensioni dei file immagine . 
per tali motivi le indicazioni che si pongono per le comunicazioni tramite email sono particolarmente adatte anche in questo caso . poich tuttavia la velocit di caricamento delle pagine dipende in larghissima parte dalle dimensioni delle immagini ( in rapporto inversamente proporzionale ) [ 9 ] , potrebbe essere consigliabile utilizzare rapporti di compressione pi spinti nelle immagini jpeg . 
however , because download speed is highly dependent on image size ( the larger the image , the slower the download ) [ 9 ] , it may be useful to use higher compression ratios in jpeg images . 
in addition , web pages are often rich in animations , arrows and graphs with few colours and diagrams , so one should also consider using a format , such as the gif format , capable of handling simple animations and characterised by excellent compression capabilities for simple graphics . preparation of electronic posters all images included in an electronic poster should , in our opinion , be of excellent quality , because individual slides often remain on screen for several seconds , giving viewers the time to notice even subtle details such as discolouration or border imperfection . 
even in this situation , the jpeg format ( possibly at low - compression ratio ) may be best for images in which some detail can be sacrificed , whereas the png format may be best for images that should be graphically perfect , as in the magnification of a detail . 
to better appreciate these points , it may be useful to view the many electronic posters posted at news / eposternews and presented at the sirm 2006 and 2008 congresses . slide shows the video presentation of a series of slides is largely similar to an electronic poster , and the same principles apply . 
this also provides the possibility of manipulating the images in real time for example , with multiplanar reconstructions or renderings which will enhance the interactiveness of the presentation . print publishing the most important aspects in printing images on paper are the quality of the image and its size in pixels , as these will directly affect the quality of the printed image . 
in fact , in the process of transforming a digital image into a printed image , one needs to consider the physical dimension of the internet sono molto ricche di animazioni , frecce , grafici con pochi colori e schemi , e quindi non va ignorata la possibilit di utilizzare un formato in grado di gestire semplici animazioni e caratterizzato da una ottima capacit di compressione nella grafica semplice come il formato gif . preparazione di poster elettronici liconografia di un poster elettronico dovrebbe , a nostro parere , essere particolarmente curata nei dettagli , anche nelle immagini meno importanti . 
ci giustificato dal fatto che spesso le singole diapositive rimangono a schermo a lungo , dando il tempo di notare anche sottili dettagli come le discromie o limperfezione dei bordi . 
ecco perch anche in questa situazione raccomandabile optare per il formato jpeg ( possibilmente a basso rapporto di compressione ) nelle immagini in cui si pu sacrificare un po di dettaglio , mentre il formato png in quelle che devono essere graficamente ineccepibili , come in un ingrandimento di particolare . 
a tale proposito risulta utile prendere visione dei numerosi poster elettronici pubblicati allindirizzo news , riguardanti il congresso sirm 2006 e 2008 . presentazione a video la presentazione a video di una serie di diapositive per molti aspetti una situazione simile a quella di un poster elettronico , ed infatti si applicano gli stessi principi . 
questo fornisce anche la possibilit di manipolare in tempo reale le immagini , per esempio con ricostruzioni multiplanari o rendering , che innalzano linterattivit della presentazione . stampa su carta per quanto riguarda la stampa su supporto cartaceo ci che maggiormente conta sono la qualit e le dimensioni in pixel dellimmagine , poich esse incideranno direttamente sulla bont dellimmagine nella pagina . 
per quanto riguarda le dimensioni delle immagini , la stampa su carta assume alcune caratteristiche singolari rispetto ad altre situazioni . infatti nel processo che porta dallimmagine digitale a quella stampata si introduce il concetto della dimensione fisica dellimmagine , ovvero della dimensione tangibile delloggetto ( carta , o altro supporto ) che contiene limmagine nella realt . 
per effettuare tale passaggio necessario specificare le dimensioni reali di un pixel , in modo che una stampante sappia , per usare un esempio limite , che un pixel 494 radiol med ( 2009 ) 114 : 484495 image , that is , the tangible dimension of the object ( paper or other medium ) containing the image . 
when transforming the image , one needs to specify the true dimensions of a pixel , so as to inform the printer that to use an extreme example a pixel on screen corresponds to a dot of 1 mm2 on paper . 
in practice , one specifies how many pixels should be contained in an inch ( 2.54 cm ) , the so - called dots per inch ( dpi )  . 
the smaller the pixels , the better the quality of the printed images , as more pixels will be printed per inch of paper , with a more natural - looking result . 
on the other hand , it should be noted that the value of the attribute dots per inch is an extrinsic value that bears no relation to the image displayed on screen . 
finally , although the tiff format is considered the reference standard , it is not necessarily superior to png for conventional printing purposes , and in some cases , it may be much easier to manipulate and send images at the more effective compression rates provided by the png format . conclusions each image file format was developed for a specific purpose , whether to minimise the size of the file or to preserve a faithful image . 
the tiff is the de facto standard when the maximum quality of the image data is needed . whenever possible , however , we recommend the use of the png format , which combines good compression effectiveness with preservation of image quality . sullo schermo corrisponde ad un punto di 1 mm2 sulla carta . nella pratica si preferisce specificare quanti pixel andranno contenuti in un pollice ( 2 , 54 cm ) , i cosiddetti punti per pollice , sintetizzati con lacronimo inglese dpi ( dots per inch )  . 
la qualit delle immagini su carta sar migliore se ci saranno pixel di minori dimensioni , poich in un pollice di carta ne verranno stampati un numero maggiore , dando allocchio una impressione pi naturale . 
per esempio , per stampare una immagine di 1010 pollici ad una risoluzione di 300 dpi ( la stessa risoluzione necessaria per la pubblicazione di immagini su la radiologia medica e su molte altre riviste ) necessaria una immagine di 30003000 pixel ( 300 dpi10 pollici )  . 
lo stesso risultato si pu ottenere stampando una immagine di 60006000 pixel a 600 dpi . daltro canto si vuole sottolineare come il valore dellattributo punti per pollice sia una caratteristica estrinseca dellimmagine , del tutto svincolata dalla sua rappresentazione a monitor . 
infatti possibile specificare tale valore a posteriori , e modificarlo a piacimento prima della stampa . a questo proposito si raccomanda lutilizzo di formati in grado di non perdere dettaglio e di poter gestire agevolmente tale attributo , come il formato tiff ed il formato png . 
a volte infatti pu essere di gran lunga pi agevole manipolare e spedire immagini alle compressioni pi efficaci garantite dal formato png . conclusioni ogni formato di file immagine nasce con uno scopo preciso , sia esso quello di minimizzare le dimensioni dei file , o quello di preservare una immagine fedele . 
levent1 1department of radiology , medical faculty , atatrk university , erzurum , turkey 2department of radiology , bilim university , florence nightingale hospital , istanbul , turkey 3department of radiology , numune hospital , erzurum , turkey 4department of pediatric cardiology , medical faculty , atatrk university , erzurum , turkey correspondence to : m . 
sok no 5 , dadaskent , erzurum , turkey , tel . : + 90 - 442 - 2361212 / 1521 , fax : + 90 - 442 - 2361301 , e - mail : akkanrad@hotmail.com received : 28 september 2008 / accepted : 31 october 2008 / published online : 14 april 2009 springer - verlag 2009 abstract purpose . 
these 18 patients were initially referred due to indications such as chest pain ( n = 11 ) , risk - factor assessment ( n = 3 ) , coronary artery anomaly ( n = 1 ) , suspected aberrant right subclavian artery due to dysphagia ( n = 1 ) and coronary artery bypass graft ( n = 2 )  . 
diciotto pazienti presentavano una tasca o una sacca a livello del setto interventricolare , verosimile espressione di chiusura spontanea del difetto interventricolare ( prevalenza 0 , 66% )  . i reperti della tcms di questi 18 pazienti sono stati correlati con i reperti ecocardiografici . 
il nostro studio dimostra che lincidenza di chiusura spontanea del difetto del setto interventricolare , radiol med ( 2009 ) 114 : 370375 patients initially diagnosed with ventricular diverticula with an apical and marginal septum location may actually have spontaneously closed muscular vsd . 
 keywords cardiac ct heart mdct angiography closed muscular ventricular septal defect introduction ventricular septal defects ( vsds ) are the second most common congenital heart defect after bicuspid aortic valves , but their true rate of incidence is , surprisingly , unknown [ 1 ]  . the incidence rate of vsds among live births is 1.53.5 per 1 , 000 term infants and 4.57.0 per 1 , 000 premature infants [ 2 ]  . the natural history of vsd , including incidence of spontaneous closure ( sc ) , is also uncerta however , some studies have reported the sc rate of vsd to be 48% by 6.9 years ( the mean age ) and 72% in patients without congestive heart failure ( chf ) [ 13 ]  . 
radiologists have begun to interpret coronary artery diseases , and in reporting the results of images obtained for coronary artery disease , they have begun to evaluate nonvascular cardiac structures as well . one of these is sc of muscular vsd observed in the interventricular septu in this study , we describe the experience of our institutions ( two centres ) in using cardiac multidetector ct angiography ( mdcta ) to diagnose sc of muscular vsd . materials and methods the study included 2 , 725 consecutive patients referred to atatrk university hospital and florence nightingale hospital for mdcta . 
in questo modo , alcuni pazienti , ai quali inizialmente era stata fatta diagnosi di diverticoli ventricolari a livello apicale e marginale del setto , in realt possono aver avuto una chiusura spontanea del difetto del setto interventricolare . 
questo risultato pu incidere sulle percentuali precedentemente riportate sia per quanto riguarda i diverticoli ventricolari sia per quanto riguarda la chiusura spontanea del difetto del setto interventricolare . parole chiave tc cardiaca cuore angiografia tcms chiusura del difetto del setto interventricolare disease , congenital malformation , atypical chest pain , screening for coronary artery disease and inconclusive conventional angiography . 
images were reviewed by a radiologist and a cardiologist in consensus , and the following data were recorded : gender , age , degree of coronary artery disease and presence of any other cardiac abnormality . 
similar records for images of the central muscular region to those of the earlier cases ( sc of muscular vsd ) were noted in the apical and marginal areas of the interventricular septuthese cases , with no history of surgery , were evaluated for sc of vsd . however , in the literature , ventricular diverticulum has been reported in all locations of the ventricle wall except 372 radiol med ( 2009 ) 114 : 370375 the interventricular septu in our study , patients with similar lesions in the basal inferoseptal , apical septum and midinferoseptal locations were not included because these lesions could not be differentiated from ventricular diverticula [ 5 , 6 ]  . 
 the procedures used were in accordance with the recommendations found in the declaration of helsinki , and approval of the local ethics committee was obtained . results retrospective electrocardiogram ( ecg ) - gated reconstructions were generated every 10% during the 50%90% of the r - r interval . 
 mdct scan protocol mdct was performed using two different 16 - detector - row ct scanners ( sensation16 , siemens medical systems , forchheim , germany , and aquillon , toshiba medical systems , tokyo , japan ) during one breath - hold ( 1624 s )  . with the first scanner , the following parameters were used : 160.75 - mm collimation , 1 - mm slice thickness and 0.6 - mm reconstruction interval . 
the indications for mdcta were suspected coronary artery disease ( n = 2 , 310 ) , coronary artery anomaly ( n = 22 ) , coronary artery stent patency ( n = 220 ) and coronary artery bypass graft assessment ( n = 173 )  . 
these 18 patients were referred due to indications such as chest pain ( n = 11 ) , risk factor assessment ( n = 3 ) , coronary artery anomaly ( n = 1 ) , suspected aberrant right subclavian artery ( n = 1 ) and coronary artery bypass graft ( n = 2 )  . 
1a - c a 46 - year - old man with spontaneous closure of muscular ventricular septal defect in the interventricular septu multiplanar reformatted multidetector computed tomography angiography ( mdcta ) images from 16 - mdct single - source scanner show long - axis ( a , c ) and short - axis ( b ) views of vsd ( ventricular septal defect ) ( arrows )  . 
le immagini angiografiche con tc a 16 strati mostrano lasse lungo ( a , c ) e lasse corto ( b ) del difetto del setto ventricolare ( frecce )  . 
of vsd location of vsd other abnormalities degree of coronary artery disease radiol med ( 2009 ) 114 : 370375 table 1 patient characteristics . tabella 1 caratteristiche dei pazienti . patient vsd , ventricular septal defect ; lad , left arterial dilatation central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular central muscular none moderate none mild none severe moderate none none none mild none mild severe none severe mild none myocardial bridging at lad middle segment aberrant right subclavian artery prior coronary artery bypass grafting aortic valve disease origin of the left circumflex coronary artery from the right sinus of valsalva myocardial bridging at lad middle segment prior percutaneous coronary intervention prior coronary artery bypass grafting ventricular function with no evidence of regional wallmotion abnormalities . 
vsds create a volume load on the left side of the heart secondary to the left - to - right shunt at the ventricular level , causing left atrial and left ventricular dilatation . 
the inlet defect makes up 5%8% of all vsds and is posterior and inferior to the perimembranous defect . muscular vsds make up 5%20% of all vsds [ 7 ]  . 
2a , b immagini assiale ( a ) e sagittale ( b ) del cuore di una donna di 39 anni con chiusura spontanea del difetto del setto interventricolare , che non si pu distinguere dai diverticoli settali a localizzazione apicale . laboratory tests for the diagnosis are not available . 
in the literature , ventricular diverticula have been reported to be located on all the ventricular walls ( apical and marginal septum ) except on the interventricular septum [ 5 ]  . 
nevertheless , similar appearances were observed in the apical and marginal septum as well . because they could not be differentiated from ventricular diverticula , these patients were excluded from the study . 
naturally , this finding may affect previously reported rates of both ventricular diverticula and the incidence of sc of muscular vsd . this will negatively affect the incidence rates of ventricular diverticula reported in earlier studies . 
it appears that there is a very high incidence of asymptomatic small muscular vsds that close spontaneously . isolated ventricular noncompaction is another entity that should be considered in the differential diagnosis . 
diagnosis of ventricular noncompaction usually requires the finding of more than three deep intertrabecular recesses [ 11 , 12 ]  . other pathologies that should be differentiated from sc muscular vsd are other causes of acquired ventricular aneurysms : those that occur after myocardial infarction , myocardial inflammatory disease such as sarcoidosis or myocarditis , infectious endocarditis or trauma [ 13 ]  . 
additional causes of ventricular aneurysm include connective tissue disease and ventricular dysplasia , as seen in patients with arrhythmogenic right ventricular cardiomyopathy . often , the distinction between fibrous ventricular diverticula and these entities can be made only with knowledge of cardiac history and visualisation of an associated abnormalitye.g. 
the true incidence of muscular vsd may have been underreported in the literature because of limitations inherent in the previously available imaging techniques and differences in the patient populations studied . 
because cardiac mdcta is frequently performed in patients with symptoms of chest discomfort , and because chest pain may be a signal of a cardiac abnormality , the incidence of sc muscular vsd is probably higher in this population than in the general asymptomatic population . however , in our study , a higher incidence of sc muscular vsd was shown in a large patient population . 
at our institutions , almost all of the cardiac mdcta studies are prospectively interpreted by two reviewers in consensus to generate an official report , and most reports are generated by two of the most senior reviewers . 
second , although a strict criterion consistent with the pathologic description of muscular vsd was chosen for the identification of this entity , pathologic proof of diagnosis was not obtained in any of our patients . 
however , given that the true prognostic implication of muscular vsd is unknown and that treatment of this entity is controversial , there is no indication to pursue an invasive procedure to confirm the diagnosis in these patients . in summary , this study shows that the incidence of sc muscular vsd with central septum location is probably higher than expected . 
3 immagine assiale del cuore di un uomo di 52 anni con chiusura spontanea del difetto del setto interventricolare , che non si pu distinguere dai diverticoli settali a localizzazione basale . this study has some limitations . 
guerci , radiologia padiglione barbieri , ospedale maggiore di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703660 , fax : + 39 - 052 - 1986352 , e - mail : leonardo.guerci@libero.it received : 12 august 2008 / accepted : 16 september 2008 / published online : 12 march 2009 springer - verlag 2009 abstract two women with profoundly different backgrounds were brought together in a destiny that saw their paths cross and join in the discovery of radioactivity : marie curie and blanche wittman . 
the discovery of radioactivity was the common denominator underlying the vicissitudes of their lives , the same radioactivity that was so acclaimed and of such incredible diagnostic and therapeutic potential while at the same time so underrated in the everyday life of the time that disregarded , almost disparagingly , the deleterious biologic effects it was capable of provoking . 
at the beginning of the twentieth century , those effects were in fact often underestimated or scarcely considered , and it was only after world war ii that there came an awareness of the ambiguous properties of ionising radiation . 
after numerous studies on radiation exposure , much of the current debate concerns the possible effects of exposure to small doses , such as those delivered in most radiological examinations . 
the theories proposed include the unorthodox theory of hormesis , which requires careful riassunto due donne , due storie profondamente diverse , unite da un destino che le incrocia e le unisce nella scoperta della radioattivit : marie curie e blanche wittman . 
la prima , una delle pi grandi donne e scienziate di tutti i tempi , unica nella storia ad aver vinto due premi nobel per la scienza , dotata di uno spirito umanitario fuori dal comune , dedic , nonostante lo scandalo sentimentale che la vide al centro della cronaca , la maggior parte della sua vita alla ricerca scientifica . 
la seconda , passata alla storia come la regina delle isteriche durante il suo ricovero nel famigerato manicomio della piti salpetrire di parigi , divenne alla sua guarigione una delle pi strette collaboratrici di m.me curie nellestrazione del radium dai fanghi della boemia , per ben 16 anni di duro lavoro , fino al momento della sua morte . 
ed proprio la scoperta della radioattivit il comun denominatore che sta alla base delle loro vicende umane , quella stessa radioattivit cos celebrata e dalle incredibili potenzialit diagnostiche e terapeutiche , ma allo stesso tempo cos svilita nella quotidianit della vita di quel tempo , che ignorava , talora quasi a sprezzo , gli effetti nocivi biologici in grado di provocare . 
nei primi anni del 900 tali effetti furono infatti spesso sottovalutati o scarsamente considerati , e fu solo dal secondo dopoguerra in poi che si manifest una forte presa di coscienza sulle ambigue propriet delle radiazioni ionizzanti . 
dopo numerosi studi condotti sullesposizione alle radiazioni ionizzanti , ci di cui molto si discute oggi riguarda principalmente i possibili effetti provocati dallesposizione a piccole dosi , come quelle erogate nella 348 radiol med ( 2009 ) 114 : 347357 reevaluation . 
much light has been shed on radiology since the time of blanche and marie , but there still remain many shadows to dispel , and this can only be done by serious and constant scientific commitment . keywords curie wittman ionizing radiation biological risk radiobiology maggior parte degli esami radiologici : tre le teorie proposte , una delle quali ( quella eretica della ormesi ) richiede di essere rivalutata con maggiore attenzione . molte luci si sono accese dai tempi della radiologia di blanche e marie , tuttavia al giorno doggi rimangono da chiarire ancora molte ombre , che solo un serio e costante impegno scientifico potr dissipare in futuro . parole chiave curie wittman radiazioni ionizzanti rischio biologico radiobiologia introduction introduzione a few years ago , the swedish writer p.o. 
enquist [ 1 ] wrote a charming book about two very different women brought together by the vagaries of life to work side by side and share hardships , danger and emotions linked with the early study of radioactivity : marie curie and blanche wittman . the clearly fictionalised vicissitudes narrated by enquist were the starting point for research that led us to analyse several aspects of the history of radiology . qualche anno fa , lo scrittore svedese p.o. 
enquist [ 1 ] ha dedicato un bel libro alla storia di due donne , molto diverse tra loro ma che i casi della vita hanno portato a lavorare fianco a fianco e a condividere fatiche , pericoli ed emozioni legate ai primi studi sulla radioattivit : marie curie e blanche wittman . 
a few days before she was awarded the prize in stockholm , a scandal over her affair with another famous physicist , paul langevin ( 18721946 ) broke out in paris . 
 this event was considered of such importance that the marie curie marie sklodowska , nata a varsavia , in polonia , nel 1867 , era figlia di un libero pensatore e di una cattolica praticante . 
pochi giorni prima della consegna del secondo nobel a stoccolma , a parigi scoppi lo scandalo per la relazione che la ancor giovane vedova aveva iniziato con un altro fisico famoso , paul langevin ( 18721946 )  . 
 radiol med ( 2009 ) 114 : 347357 questo evento ebbe una rilevanza tale che il fisico svante arrhenius , membro del comitato per il nobel , giunse a consigliare a marie di rifiutare il premio . 
lei stessa e la figlia irne ( allora diciassettenne ) , impararono a guidare questi automezzi , studiarono anatomia e , in compagnia di personale medico , prestarono a lungo la propria opera in zona di guerra . madre e figlia si sottoposero cos a forti dosi di raggi x senza alcuna protezione . 
negli stessi anni , marie fond un servizio di radioterapia militare , isolando personalmente il gas radioattivo ( radon ) in tubi di vetro che venivano spediti a diversi ospedali francesi . 
marie vers anche alla patria acquisita la maggior parte delle somme ricevute dalla fondazione nobel [ 3 ]  . dopo la fine della guerra , negli anni dal 1919 al 1934 , marie ormai una celebrit mondiale viaggi molto , recandosi anche pi volte negli stati uniti , dove incontr i presidenti harding e hoover , lanci raccolte di fondi per la ricerca e ottenne notevoli finanziamenti , nonostante la timidezza le impedisse di parlare in pubblico con facilit . 
during her stay in england , marie , deeply shocked by the parisian scandal , came into contact with the movement for womens suffrage , the leading member of which was emmeline pankhurst ( 18581928 ) , who was arrested on several occasions . back in paris after a break of 14 months , marie returned to her laboratory , as the scandal began to die down with the separation by mutual agreement of the langevins . 
marie and paul did not resume their affair , although their relationship remained friendly and fruitful on the professional level . at the outbreak of world war i , only two people remained on the premises of the radium institute , which was planned by marie and built in the latin quarter in the street renamed for the occasion in honour of pierre curie : marie , and a mechanic who was exempt from the draft due to a serious heart condition . although until then , maries main interest had been the radioactive phenomena , she realised the enormous diagnostic potential of artificial x - rays ( roentgen rays ) in saving the lives of wounded soldiers at the front . 
she set up 350 radiol med ( 2009 ) 114 : 347357 marie curie cominci a soffrire di disturbi fisici connessi alle radiazioni intorno al 1920 , con una doppia cataratta che richiese quattro dolorosi e , per lepoca , complicati interventi . 
negli ultimi anni , manifest una progressiva debolezza , dapprima attribuita erroneamente alla tubercolosi , finch uno specialista di ginevra cap che poteva trattarsi di una forma simil - tumorale di anemia aplastica , dovuta al danno midollare da radiazioni [ 4 ]  . quando mor , nel 1934 , 28 anni dopo il marito pierre , listituto da lei diretto era una delle massime realt scientifiche del tempo e molte applicazioni mediche e industriali delle scoperte dei curie testimoniavano gi delle vaste potenzialit applicative della radioattivit . 
negli anni compresi tra il 1919 ed il 1934 , listituto diretto da marie curie produsse 483 lavori scientifici o libri , 31 dei quali scritti da marie [ 3 ]  . marie venne sepolta due volte ; la prima a sceaux , con il marito pierre . 
il castello , in quegli anni , attirava la curiosit morbosa di frotte di visitatori , da sarah bernhardt ad axel munte , a numerosi giovani studiosi di neuropsichiatria , da broca a gilles de la tourette , al giovane freud . 
in sostanza , alla fine dell800 , non molto era cambiato nella vita degli internati da quando , un secolo prima , il castello era diretto dall illuminista dottor pinel , il quale aveva tentato con scarso successo , nel 1795 , loperazione insieme politica ed umanitaria di liberare i folli dalle catene . 
foucault ha scritto , a proposito del tentativo di pinel : le catene cadono , il folle si ritrova libero e in quel momento recupera la ragione la brutalit che appare nei dementi non che il riflesso della bestialit dei guardiani e ancora : a partire da pinel si vedr nella follia uno slancio venuto dal profondo , che oltrepassa i limiti dellindividuo e tende ad una apoteosi di se stesso [ 5 ]  . blanche , ricoverata dal 1878 al 1893 , divenne presto famosa come la regina delle isteriche , protagonista delle esibizioni organizzate e dirette settimanalmente dal dottor fig . 
marie and her daughter , irne ( aged 17 at the time ) , learned how to drive these vehicles , studied anatomy and , in the company of medical personnel , gave long - term service in the war zone . 
during the same period , marie established a military radiotherapy service and personally isolated the radioactive gas ( radon ) in glass tubes that were sent to various french hospitals . 
she also donated most of the money received from the nobel foundation to her adopted homeland [ 3 ]  . after the war , in the years between 1919 and 1934 , marie , who had become an international celebrity , travelled widely . 
the frail figure of this now elderly woman dressed constantly in black became legendary , and due to her austere appearance and moral force , marie was compared with a buddhist monk . launched very successful marie began to suffer from physical problems connected with radiation around 1920 , with the appearance of a double cataract that required four painful and for the times complicated operations . 
in her later years , she developed progressive weakness , which was at first erroneously attributed to tuberculosis until a specialist from geneva realised it could have been caused by aplastic anaemia , a tumour - like condition due to radiation - induced bone marrow damage [ 4 ]  . between 1919 and 1934 , the institute directed by marie produced 483 scientific papers or books , 31 of which were written by her [ 3 ]  . 
in those years , the piti salptrire attracted the morbid curiosity of a stream of visitors , from sarah bernhardt to axel munte and numerous neuropsychiatrists , from paul broca to georges gilles de la tourette and the young sigmund freud . 
in essence , at the end of the nineteenth century , little had changed in the lives of the patients from when a century earlier the hospital was directed by the enlightened physician philippe pinel , who , in 1795 , had attempted without success to perform the political and humanitarian task of freeing the inmates from their shackles . 
and at that moment they recovered their reasonthe brutality which appears in the demented is nought else than the reflection of the animality of the guardians and from pinel onwards , the classical mind recognised in madness an impulse from the depths which exceeded the juridical limits of the individual , ignoring fixed moral limits and tending towards an apotheosis of the self [ 5 ]  . blanche , who was hospitalised between 1879 and 1893 , soon became famous as the queen of hysterics , being the protagonist of the spectacular weekly lectures organised and directed by jean - martin charcot . 
the cures without support became real cures of false diseases , as in fact hysteria proved to be , which failed to outlive charcot . hysterical madness was a mixture of persuasion and mystification , even though , many years later , blanche stated that charcots weekly performances were not based on feigning . although charcot has been accused , and probably correctly , of misogyny [ 6 ] , in 1885 , he accepted into his group a brilliant young medical graduate , blanche edwards [ 7 ]  . after the death of charcot , blanche wittman , having been declared clinically cured , found temporary work as a technical assistant in the recently instituted radiology department of salptrire . 
indeed , roentgens discovery ( 1895 ) was made only 2 years after the death of charcot and was contemporary to freuds studies of hysteria . in 1898 , at the time of the dreyfus affair , blanche moved to the laboratory of the curies , with the thankless task of isolating radium from the pitchblende from sankt joachimsthal in bohemia and in which she remained for hours and hours each day immersed up to her knees in pitchblende . this was the beginning of the collaboration and cohabitation of blanche and marie , which lasted 16 years . 
after 4 years of work , the curies , with the help of several assistants , including blanche , managed to isolate 0.1 g of radium from tonnes of pitchblende . the lesions caused by the radioactive pitchblende caused blanche to have first her legs and then her left arm amputated . 
reduced virtually to a torso and forced to move about in a wooden cart , blanche had to stop working in the laboratory but remained until her death , in 1913 , within the curies family circle and their closest friends and collaborators , such as becquerel [ 8 ]  . ha potuto compiersi se non con la complicit del malato stesso . 
la follia isterica era un insieme di persuasione e di mistificazione anche se , parecchi anni dopo , blanche ebbe a dichiarare che gli spettacoli settimanali di charcot non erano basati sulla simulazione . 
nonostante charcot sia stato accusato , probabilmente con ragione , di misoginia [ 6 ] , nella sua quipe egli accett anche , nel 1885 , una giovane e brillante laureata in medicina , blanche edwards [ 7 ]  . 
 nel 1898 , allepoca dellaffare dreyfus , blanche si trasfer nel laboratorio dei coniugi curie , con lingrato compito di isolare il radium dai fanghi della pechblenda provenienti dalle cave di sankt joachimsthal in boemia e nei quali restava immersa fino alle ginocchia per ore ed ore , ogni giorno . 
da una tonnellata di fanghi e terriccio , dopo quattro anni di duro lavoro , i curie , con laiuto di alcuni aiutanti , tra cui blanche wittman , riuscirono ad isolare 0 , 1 grammi di radiu le lesioni provocate dai fanghi radioattivi portarono la povera blanche a subire progressivamente lamputazione delle gambe e del braccio sinistro . 
ridotta ad un torso e costretta a spostarsi su un carretto di legno , blanche cess ovviamente di lavorare nel laboratorio , ma rest fino alla morte , avvenuta nel 1913 , nella cerchia familiare dei curie e dei loro pi stretti amici e collaboratori , come il grande fisico henri becquerel [ 8 ]  . popularity and demonisation of ionising radiation at the beginning of the twentieth century , artificially produced x - rays and , to a lesser extent , the radiation emitted by newly discovered radioactive elements , had become quite fashionable . 
this popularity can be seen not only in the press of the time [ 9 ] but also in the numerous handmade articles and industrial products whose labels referred to the mysterious rays for publicity purposes , such as household products , detergents , postcards , razors , citrus squeezers , prophylactics , soap , spirits and a variety of other items [ 10 ]  . 
questa popolarit testimoniata , oltre che dalla stampa dellepoca [ 9 ] , anche da numerosi reperti , manufatti o prodotti industriali , che nelletichetta richiamavano i raggi misteriosi a scopo pubblicitario , come prodotti per la casa , detergenti , cartoline , rasoi , spremiagrumi , profilattici , sapone , alcolici ed apparecchi di ogni tipo [ 10 ]  . 
at circuses and trade fairs , as well as elegant salons , x - ray demonstrations were performed , mainly for the macabre fancy of observing the skeleton of friends and relatives in the penumbra of the fluoroscopic screen , illuminated by a weak green glow . 
to have her hand x - rayed , as roentgens wife berta had done several years earlier , the celebrated actress sarah bernhardt remained motionless on her knees for 5 min in a fashionable parisian salon [ 4 ]  . the new rays captured the imagination of the public , more so than the cinmotagraphe invented by the lumire brothers , auguste and louis , in the same year as roentgens discovery , for they embodied the guarantee of a better future , in a positivist vision of the world characterised by endless faith in progress . 
photographs of the time bear witness to the very slow growth in the awareness of the ambiguous properties of radiation , which can be a powerful weapon against disease in both diagnosis and treatment but also highly pathogenetic and therefore should be dominated and controlled , rather than used indiscriminately . 
nei circhi e nelle fiere di paese , come nei salotti eleganti , venivano eseguite dimostrazioni dei raggi x , principalmente per il gusto un po macabro di osservare lo scheletro di amici e parenti nella penombra dello schermo fluoroscopico , illuminata da una debole luminescenza verdastra . 
per farsi radiografare la mano , come aveva fatto pochi anni prima la moglie di roentgen , berta , la grande attrice sarah berhardt rimase immobile in ginocchio per 5 minuti in un salon parigino alla moda [ 4 ]  . i nuovi raggi catturavano limmaginazione del pubblico con grande intensit , pi dellinvenzione del cinematografo , che i fratelli lumire realizzarono nello stesso anno della scoperta di roentgen e rappresentavano la garanzia per un futuro migliore , in una visione del mondo ancora positivista , caratterizzata da grande fiducia nel progresso . liconografia del tempo testimonia di una presa di coscienza collettiva molto lenta delle ambigue propriet delle radiazioni , che possono costituire unarma potente contro le malattie nella diagnosi e nella terapia , ma anche risultare altamente patogene e dunque devono essere dominate e controllate , piuttosto che utilizzate indiscriminatamente . 
la invisibilit delle radiazioni portava ad una sottovalutazione degli effetti biologici . quando , un anno dopo la scoperta di roentgen , 354 radiol med ( 2009 ) 114 : 347357 could have ( unpredictable ) effects on the body . 
in 1903 , the first rudimentary forms of lead or leadrubber shields appeared , but they were seldom used , as their rigidity hampered free movement . the radiologists of the time performed hours of radioscopy every day without any protection whatsoever , and after several years of work , they developed paleness , weakening and severe asthenia . 
in 1925 , she was part of a commission of the french academy of medicine , which recommended the use of lead screens and periodic blood tests in subjects exposed to radiation in the workplace . 
hair and fingernails tended to fall out and not grow back . a list of radiation victims compiled in hamburg in 1936 and clearly incomplete bore the names of 220 physicians , physicists , chemists , technicians , nurses and religious workers . 
gendreau described the first case of occupational disease associated with radiation [ 4 ]  . workers in a watch factory established in 1914 ( radium corporation , newark , nj , usa ) used fine brushes to spread radioactive material ( known as glow in the dark ) on the watch faces to render them fluorescent in the dark . many of these watches were supplied to troops on the european fronts during world war i . 
the workers in the factory , who tended to moisten the brushes on their tongues , suffered severe ulcerations , jaw necrosis , tooth loss and various types of tumours . 
in 1929 , legal action was taken against the company , which defended itself by attributing the workers illnesses to symptoms of hysteria . the use of radiation for diagnostic and therapeutic purposes , particularly in the fight against cancer , was actively promoted as early as the latter phase of maries life after world war i . 
the biological effects of radiation became effectively controlled , and devices capable of delivering very low doses were developed without sacrificing diagnostic accuracy ( such as those quipped with image intensifiers and television chains )  . 
this growing sullamerican journal of the medical association , comparve il primo articolo sulle applicazioni mediche dei raggi x , il direttore della rivista ipotizz che la forma di energia appena scoperta potesse esercitare effetti ( imprevedibili ) sullorganismo ma , a parte il grande clinico inglese lister , nessuno raccolse queste osservazioni [ 4 ]  . 
nel 1903 comparvero le prime , rudimentali protezioni in piombo o in gomma piombifera ma pochi le utilizzarono , perch la loro rigidit ostacolava i movimenti . i radiologi praticavano ore di radioscopia ogni giorno , senza alcuna protezione e , dopo pochi anni di lavoro , accusavano pallore , deperimento e grave astenia . 
tiraboschi , da 15 anni in attivit come radiologo presso lospedale cittadino . lautopsia dimostr gravi lesioni a carico del midollo osseo e della milza ed il patologo ipotizz un ruolo eziologico delle radiazioni . 
nel 1925 marie fece parte di una commissione dellaccademia francese di medicina , che raccomand luso di schermi protettivi piombati e di test periodici del sangue in soggetti esposti professionalmente . 
i capelli e le unghie cadevano , per non ricrescere pi . una lista di vittime delle radiazioni , compilata ad amburgo nel 1936 e chiaramente incompleta , riporta 220 nomi di medici , fisici , chimici , tecnici , infermieri e religiosi . gendreau descrisse il primo caso di patologia lavorativa industriale legata alle radiazioni [ 4 ]  . 
 le operaie di una fabbrica di orologi fondata nel 1914 ( radium corporation , newark , new jersey ) utilizzavano sottili pennelli per spalmare materiale radioattivo ( detto : glow in the dark ) sui quadranti , allo scopo di renderli fluorescenti e consentire di leggere lora al buio . 
nel 29 venne istruito un processo e la ditta si difese attribuendo i disturbi delle operaie a sintomi isterici . limpiego delle radiazioni a scopo diagnostico e terapeutico , specie nella lotta contro i tumori , venne promosso attivamente gi nellultima fase della vita di marie curie , nel primo dopoguerra , ma solo nel secondo dopoguerra le conoscenze di radiobiologia raggiunsero un livello soddisfacente ; il controllo degli effetti biologici delle radiazioni divenne efficace e furono proposte apparecchiature in grado di erogare dosi molto basse , senza sacrificare radiol med ( 2009 ) 114 : 347357 awareness was certainly encouraged by the devastating effects of the atomic bombs dropped on hiroshima and nagasaki in japan in 1945 . 
it has been estimated that to obtain the same quantity of ( gamma ) radiation unleashed by the hiroshima bomb alone , millions of tonnes of the curies radium would be required . 
the nuclear proliferation in the cold war years and the chernobyl nuclear disaster in russia further contributed to the growing alarm that pervaded public opinion and the mass media in the second half of the twentieth century . the american philosopher john dewey wrote : the destructive use made of the fission of the nucleus of an atom has become the stock - in - trade of the assault upon science . what is so ignored as to be denied is that this destructive consequence occurred not only in a war but because of the existence of war , and that war as an institution antedates by unknown millennia the appearance on the human scene of anything remotely resembling scientific enquiry [ 11 ]  . today , the sustainability of medical imaging is being questioned [ 12 ]  . 
the so - called deterministic effects , which occur only in the presence of very high doses and coincide with cell death ( apoptosis ) , have a threshold effect and are not ( fortunately ) seen in individuals who undergo irradiation for diagnostic purposes or in personnel exposed to radiation in the workplace ( of course , radiotherapy is a case apart )  . the stochastic or random effects on the body are due to dna alterations produced by radiation , with consequent hereditary effects if these occur in germ cells or radioinduced tumours if they occur in somatic cells . 
particular concern regards computed tomography examinations , the number of which has increased 12 - fold over the last 20 years in europe and more than 20 - fold in the united states , with an increase of at least seven times the average dose per examination delivered to the population [ 15 ]  . laccuratezza diagnostica ( come gli impianti dotati di amplificatore di brillanza e di catene televisive )  . 
si pensi che , per ottenere la stessa quantit di radiazioni ( gamma ) prodotte dalla sola bomba di hiroshima , sarebbero stati necessari milioni di tonnellate del radium dei curie . 
la proliferazione nucleare negli anni della guerra fredda e la recente catastrofe nucleare di chernobyl hanno ulteriormente contribuito al crescente allarme , che ha pervaso lopinione pubblica ed i grandi media nella seconda met del novecento . 
si ignora che tale conseguenza distruttiva avvenuta non solo durante una guerra , ma a causa dellesperienza stessa della guerra , una istituzione nata parecchi millenni prima che comparisse sulla scena umana alcunch di lontanamente somigliante allindagine scientifica [ 11 ]  . oggi ci si interroga sulla sostenibilit dellimaging medico [ 12 ]  . 
per comprendere leffetto delle radiazioni bisogna tener conto del tipo di radiazioni coinvolte , della dose , cio della quantit di energia che esse trasferiscono nei tessuti e della variabile radiosensibilit dei tessuti stessi [ 13 ]  . 
i cosiddetti effetti deterministici , che si verificano solo per dosi molto elevate e coincidono con la morte delle cellule ( apoptosi ) , hanno un effetto - soglia e non si osservano ormai pi ( fortunatamente ) nelle persone sottoposte ad irradiazione per scopi diagnostici o in personale esposto lavorativamente ( diverso , ovviamente , il caso della radioterapia )  . 
 gli effetti stocastici o casuali sono dovuti ad alterazioni del dna prodotte dalle radiazioni , con conseguenti effetti ereditari se avvengono nelle cellule germinali o tumori radioindotti , se avvengono nelle cellule somatiche . 
le preoccupazioni riguardano soprattutto gli esami di tomografia computerizzata ( tc ) , il cui numero aumentato negli ultimi venti anni di 12 volte in europa e di oltre venti volte negli usa , con incremento di almeno 7 volte della dose media erogata per indagini radiologiche alla popolazione [ 15 ]  . state of the art and conclusions stato dellarte e conclusioni there are three theories with regard to the effects of low doses of ionising radiation . 
the best known and official doctrine , which has inspired international radiation protection laws , states that there is no threshold for stochastic effects and that even a single event or a very low dose can cause damage , the probability of which is linearly correlated with the dose ( linear nonthreshold [ lnt ] model )  . 
it has been estimated that one third of all computed tomography examinations could thus be avoided without sacrificing diagnostic accuracy . a second theory , which is not without biological and epidemiological evidence , suggests that the stochastic effects are in proportion to the dose , but in the case of low doses , there is a sort of practical threshold below which cell repair mechanisms manage to avoid damage . 
it may even be possible that the stochastic effects are not completely random , but at low doses only regard genetically predisposed individuals ( who may be identified with appropriate tests )  . the third theory , which goes contrary to accepted belief and is politically incorrect but supported by significant proof , some of which is experimental , is hormesis ( from the greek meaning to excite ) [ 16 ]  . 
moreover , life on earth evolved in conditions of environmental radioactivity much greater than the current average annual background level of around 3 msv , and the longevity of individuals exposed for professional or environmental reasons to small additional doses ( contemporary radiologists , aeroplane pilots or flight attendants , etc . ) is not lower but higher than the average , with a lower incidence of cancer . 
la lnt , estrapolata dagli effetti delle bombe atomiche sui sopravvissuti di hiroshima e nagasaki , considerata vera precauzionalmente , ma non vi sono prove certe che per dosi molto basse , come quelle coinvolte in quasi tutti gli esami di radiodiagnostica in et adulta , essa sia valida . 
la lnt ha ispirato il principio conosciuto con lacronimo alara ( as low as reasonably available ) , secondo il quale la dose erogata dovrebbe essere sempre la pi bassa ragionevolmente possibile in quelle condizioni cliniche [ 15 ]  . 
bisogna dunque mettere in atto ogni presidio tecnico per ridurre la dose erogata , senza che ci vada a discapito della accuratezza diagnostica e bisogna cercare di evitare esami inutili , di efficacia non dimostrata ( esempio : screening del tumore polmonare ) o sostituibili con altre metodiche di analoga efficacia diagnostica ( esempio : ecografia nella diagnosi della appendicite acuta )  . 
si calcola che almeno un terzo degli esami tc potrebbe cos essere evitato , senza pregiudizio per laccuratezza diagnostica . una seconda teoria , non priva di evidenze biologiche ed epidemiologiche , sostiene che gli effetti stocastici sono s proporzionali alla dose , ma che , quando si tratta di dosi piccole , esiste una sorta di soglia pratica , al di sotto della quale i meccanismi riparativi delle cellule e dei tessuti riescono ad evitare danni . 
anche possibile che gli effetti stocastici non siano poi del tutto casuali , ma che riguardino , per dosi basse , solo individui geneticamente predisposti ( ed individuabili con appositi test )  . la terza teoria , eretica e politicamente scorretta , ma sostenuta da notevoli elementi di prova anche sperimentali , lormesi ( dal termine greco che significa stimolazione ) [ 16 ]  . 
del resto , la vita sulla terra si evoluta in condizioni di radioattivit ambientale ben superiori allattuale fondo annuale medio di circa 3 millisievert e la longevit delle persone sottoposte professionalmente o per ragioni ambientali a piccole dosi aggiuntive ( i radiologi contemporanei , i piloti di aereo o le hostess ecc . ) non minore , ma maggiore della media , con minore incidenza di patologia neoplastica , il che sembra convalidare tale teoria . 
lormesi stata fortemente contrastata nei decenni scorsi , anche perch uno dei suoi ideatori ( arndt ) , oltre che psichiatra , era anche omeopata , ma le notevoli evidenze sembrano richiedere una pi seria valutazione di questa teoria , anche in campo radiologico [ 18 ]  . it is surprising that despite the widespread diffusion of clinical radiology and the advances in scientific knowledge that such an important question has still not received certain pu stupire che , nonostante la grande diffusione della radiologia medica e levoluzione delle conoscenze scientifiche , un problema di questa importanza non abbia ancora radiol med ( 2009 ) 114 : 347357 answers . 
di fisica sanitaria , irccs casa sollievo della sofferenza , san giovanni rotondo , italy 6facolt di medicina , universit di bari , bari , italy 7dipartimento di radiologia , universit novara , novara , italy 8dipartimento di scienze neurologiche e psichiatriche dellet evolutiva , universit la sapienza , roma , italy 9dipartimento di radiologia , azienda ospedaliera universitaria , umberto i , torrette , ancona , italy correspondence to : t . 
scarabino , via napoli 56 , 70031 andria , italy , tel . : + 39 - 088 - 3299140 , fax : + 39 - 088 - 3299220 , e - mail : tscarabino@hotmail.com received : 10 september 2008 / accepted : 6 october 2008 / published online : 10 march 2009 springer - verlag 2009 abstract purpose . 
this study evaluated the sensitivity of a 3.0 - tesla ( t ) magnetic resonance imaging ( mri ) in measuring cerebral phenylalanine using proton magnetic resonance spectroscopy and in assessing mr - documented whitematter changes by means of diffusion studies ( diffusionweighted imaging , apparent diffusion coefficient map ; diffusion tensor imaging ) in patients with phenylketonuria . 
lampiezza del segnale della fenilalanina relativo al rapporto creatina / fosfocreatina incrementa linearmente con la fenilalanina ematica ( r = 0 , 7067 ; p < 0 , 001 )  . 
lo studio di diffusione ha 462 radiol med ( 2009 ) 114 : 461474 exhibiting mri changes as well as decreased apparent diffusion coefficient values , but fractional anisotropy indices were normal . 
in particular , the multimodal approach with mri , proton magnetic resonance spectroscopy and diffusion magnetic resonance imaging can provide more information than previous studies performed with low - field systems . 
in particolare lapproccio multimodale con imaging rm di base , di spettroscopia e di diffusione pu fornire maggiori informazioni rispetto ai precedenti studi acquisiti con sistemi a pi basso campo . keywords phenylketonuria magnetic resonance imaging ( mri ) proton mr spectroscopic imaging diffusion mri parole chiave fenilchetonuria risonanza magnetica studio di spettroscopia protonica con risonanza magnetica studio di diffusione con risonanza magnetica introduction introduzione phenylketonuria ( pku ) is a disorder of amino acid metabolism caused by an inborn error in the phenylalanine hydroxylase gene ( pha ) , which strongly reduces hepatic hydroxylation of phenylalanine ( phe ) to tyrosine [ 1 ]  . 
previous morphological mri studies have documented focal symmetrical lesions in periventricular and , especially , parieto - occipital white matter ( wm ) in pku patients with phe blood levels exceeding 10 mg / dl . these lesions , the significance of which is as yet unclear , seem to be due to a reversible structural myelin alteration , as they regress when blood phe levels fall [ 2 ]  . proton magnetic resonance spectroscopy ( 1h - mrs ) measures noninvasively the concentration of several brain metabolites in vivo and can help to further elucidate the cerebral metabolic characteristics of pku . 
it allows evaluation of several aspects of brain biochemistry that could shed light on the nature of wm lesions , including measurement of n - acetyl - containing moieties [ mainly n - acetylaspartate ( naa ) ] , choline - containing compounds ( cho ) , creatine ( cr ) and phosphocreatine ( pcr ) , and myo - inositol ( mi ) [ 3 ]  . 
in particular , changes in naa ( a marker of neuronal integrity ) la fenilchetonuria ( pku ) un disordine del metabolismo degli amminoacidi causata da una alterazione congenita del gene della fenilalanina - idrossilasi che determina una significativa riduzione , a livello epatico , della idrossilazione della fenilalanina ( phe ) in tirosina [ 1 ]  . 
i pazienti non diagnosticati e quindi non trattati possono sviluppare diversi segni e sintomi : in particolare ritardo mentale e nella crescita , crisi epilettiche , manifestazioni cutanee ( eczemi e ipopigmentazioni )  . 
la diagnosi neonatale ha radicalmente cambiato la prognosi della pku anche se in realt possiamo riscontrare alcuni sintomi e alterazioni neuro - radiologiche anche in pazienti trattati precocemente . la pku stata studiata sotto diversi aspetti . 
essa documenta la presenza di focali e simmetriche lesioni a livello della sostanza bianca periventricolare , specie a livello parieto - occipitale , evidenti in tutti i pazienti in cui il livello ematico di phe supera il valore di 10 mg / dl . 
tali lesioni , il cui significato non ancora chiaro , sembra siano dovute a una alterazione strutturale e reversibile della mielina : infatti esse regrediscono nel momento in cui il livello di phe decresce verso valori normali [ 2 ]  . la spettroscopia protonica con rm ( 1h - mrs ) misura in maniera non invasiva e in vivo la concentrazione a livello cerebrale di alcuni metaboliti fornendo ulteriori informazioni sulle caratteristiche metaboliche cerebrali della pku e soprattutto permettendo una pi chiara analisi biochimica delle alterazioni della sostanza bianca tipiche di questa radiol med ( 2009 ) 114 : 461474 or in mi ( a potential astrocytic marker ) suggest a possible neurochemical dysfunction , whereas cho is one measure of the degree of tissue myelination [ 4 , 5 ]  . 
despite continuing progress in 1h - mrs acquisition methods and the development of increasingly sophisticated quantification routines , its determination is affected by the detection threshold at 1.5 t ( > 200 mmol / kg ) [ 3 ]  . 
furthermore , the very large volume of interest ( voi ) applied at 1.5 t ( > 30 cc ) makes phe signal detection unreliable due both to concurrent line - broadening effects on the resonance and the presence of macromolecular contributions at 7.3 ppm [ 36 ]  . in recent years , diffusion - weighted mri ( dwi - mri ) has been introduced in clinical practice . 
however , these studies have failed to clarify the significance of dwi changes in relation to clinical findings . the aim of this work was to analyse the potential and advantages of a 3.0 - t system in the multimodal study of brain alterations of patients with pku . 
they were 17 male and 15 female subjects aged from 7 to 34 ( mean 18.9 , standard deviation 6.0 ) years , 21 with early and 11 with late diagnosis . 
in particolare andiamo a misurare la concentrazione di molecole contenenti il gruppo n - acetile ( in prevalenza ln - acetil - aspartato , naa ) , le macro - molecole contenenti colina ( cho ) , la creatina ( cr ) , la fosfocreatina ( pcr ) e il mio - inositolo ( mi ) [ 3 ]  . 
le variazioni di naa ( marker di integrit neuronale ) e di mi ( potenziale marker astrocitario ) suggeriscono una possibile disfunzione neurochimica mentre mediante la quantificazione della cho abbiamo un indice del grado della mielinizzazione tissutale [ 4 , 5 ]  . 
lo studio di 1h - mrs con unapparecchiatura a 1 , 5 tesla ( t ) ha permesso di quantificare i livelli cerebrali di phe in pazienti con pku : tali misurazioni hanno fornito dati interessanti sulla biochimica delle alterazioni della sostanza bianca in tale patologia [ 35 ]  . 
la valutazione dei livelli di phe , ottenuta utilizzando sistemi a 1 , 5 t , per ancora soggetta a delle limitazioni : nonostante i miglioramenti dei protocolli di acquisizione 1h - mrs e di quantificazione dei metaboliti c un limite intrinseco dovuto alla soglia di detezione del metabolita ( > 200 mmol / kg ) legato direttamente alla intensit del campo magnetico ( 1 , 5 t ) [ 3 ]  . 
inoltre la notevole ampiezza del volume di interesse ( voi ) in sistemi a 1 , 5 t ( > 30 cc ) rende il valore di phe non attendibile e ci dovuto sia a effetti concomitanti di allargamento sulla risonanza che allinterferenza delle altri componenti macromolecolari presenti a 7 , 3 ppm [ 36 ]  . negli ultimi anni sono state introdotte di routine nella pratica clinica le sequenze rm pesate in diffusione ( dwmri )  . 
 [ 8 ] hanno dimostrato in pazienti con pku la presenza di alterazioni di segnale in dwi che si sovrappongono sostanzialmente alle alterazioni rilevate in condizioni rm di base e che sono caratterizzate da iperintensit in t2 . 
le mappe del coefficiente di diffusione apparente ( adc ) invece documentano valori compatibili con una diffusione ristretta dei protoni . tali studi comunque non hanno ancora chiarito lorigine di tali alterazioni e una chiara correlazione col quadro clinico . lo scopo del nostro lavoro di analizzare le possibilit e i vantaggi della rm 3 , 0 t nello studio multimodale delle alterazioni cerebrali di pazienti con pku ed in particolare di valutare la sensibilit di un sistema rm ad alto campo nel misurare la phe cerebrale con la 1h - mrs e nel documentare le alterazioni della sostanza bianca rilevate con lo studio rm di base utilizzando gli studi di dw - mri . magnetic resonance technique materiali e metodi mr studies were performed with a 3.0 - t scanner ( signa horizon lx , general electric medical system , milwaukee , wi , usa ) with a standard quadrature transmit / receive birdcage head coil . 
wm involvement was assessed by morphological mr with sagittal fast spoiled gradient recalled ( fspgr ) t1 - weighted [ repetition time ( tr ) / echo time sono stati inclusi nello studio 32 pazienti con un tipico quadro biochimico - clinico della pku : 17 maschi e 15 femmine , et compresa tra 7 e 34 anni ( media 18 , 9 , deviazione standard 6 , 0 ) : 21 con diagnosi precoce e 11 con diagnosi tardiva di malattia . 
in tutti i pazienti stato valutato il valore ematico di phe ed stata effettuata una 464 radiol med ( 2009 ) 114 : 461474 ( te ) / flip angle ( fa ) 225 / minimum / 75 ms , acquisition time 1 min 57 s ] sequences ; axial fluid - attenuated inversion recovery ( flair ) ( tr / te / ti , inversion time , 11 , 000 / 130 / 2 , 250 ms , acquisition time 2 min 26 s ) and spin echo ( se ) t1 - weighted ( tr / te 500 / 10 ms , acquisition time 2 min 21 s ) sequences , and coronal fast spin echo ( fse ) t2weighted ( tr / te 5 , 000 / 55 / 20 ms , acquisition time 1 min 05 s ) sequences . 
standard mr scans were acquired using 5mm - thick slices , 1 - mm gap , matrix size 256192 , and field of view ( fov ) 22 cm . single - voxel 1h - mrs was performed using a short te point - resolved spectroscopy ( press ) sequence ( tr / te 2 , 000 / 35 ms , total averages 128 , spectral width 2 , 500 hz , 1 , 024 complex data points , acquisition time 4 min 56 s )  . 
a voxel volume of just 8 cc was placed in the altered periventricular deep wm . the diffusion studies [ dwi , adc maps and diffusion tensor imaging ( dti ) ] were performed in the axial plane using a pulsed gradient se echo - planar sequence ( tr / te 8 , 000 / minimum ms ; dwi acquisition time 44 s and for dti 6 min 57 s ) without ( b - value = 0 ) and with ( b - value = 1 , 000 s / mm2 ) diffusion gradients applied along 25 different directions to cover the three - dimensional space uniformly . 
 additional dwis were acquired in the axial plane , with identical parameters except for the b - value , which was set at values from 500 to 2 , 500 s / mm2 ( 500 , 1 , 000 , 1 , 500 , 2 , 000 and 2 , 500 ) for five different acquisitions . data analysis all postprocessing was performed on a unix workstation . wm changes were analysed on mri both qualitatively , with reference to signal intensity in the different pulse sequences , and semiquantitatively , with reference to their anatomical location ( frontal , temporal , occipital , cerebellar and in brainstem ) and extension ( deep and / or subcortical wm )  . 
wm involvement was scored on t2 - weighted images by raters who were unaware of patients clinical history , as follows : 1 for deep wm involvement only ( limited involvement ) ; 2 for involvement of deep and subcortical wm ( intermediate involvement ) ; 3 for greater involvement of brainstem and / or cerebellum ( severe involvement )  . 
 brain phe was quantified by computing the amplitude of the phe signal at 7.36 ppm relative to the cr / pcr peak at 3.05 ppm , considered as an internal reference , using the sage / idl software . 
the other metabolites ( naa , cho , cr / pcr , mi ) were analysed by means of lcmodel routines . the diffusion images were analysed assuming a monoexponential relation between signal intensity and the product of the b - matrix ( a 33 matrix expressing the relationship between signal attenuation and elements of the diffusion tensor matrix )  . 
trenta soggetti sani ( 9 maschi e 21 femmine ; et compresa tra 12 e 58 anni ; media 32 , 9 ) sono stati arruolati nello studio come gruppo di controllo per confrontare i dati ottenuti dallimaging rm . 
il consenso informato stato firmato da tutti i pazienti o da loro parenti prossimi . tecnica rm lo studio rm stato effettuato con unapparecchiatura rm 3 , 0 t ( signa horizon lx , general electric medical system , milwaukee , wi , usa ) dotata di bobina della testa standard in quadratura trasmittente / ricevente . 
le alterazioni della sostanza bianca sono state valutate con la rm di base utilizzando le sequenze : fast spoiled gradient recalled ( fspgr ) t1 - pesata ( tr , tempo di ripetizione , / te , tempo di echo , / fa , flip angle , 225 / minimum / 75 ms , tempo di acquisizione 1 min 57 s ) acquisita in proiezione sagittale ; fluid - attenuated inversion recovery ( flair ) ( tr / te / ti , tempo di inversione , 11000 / 130 / 2250 ms , tempo di acquisizione 2 min 26 s ) e spin echo ( se ) t1 - pesata ( tr / te 500 / 10 ms , tempo di acquisizione 2 min 21 s ) in proiezione sagittale ; fast spin echo ( fse ) t2 - pesata ( tr / te 5000 / 55 / 20 ms , tempo di acquisizione 1 min 05 s ) in proiezione coronale . 
il volume di interesse di 8 cc stato posizionato nelle aree di alterazione della sostanza bianca periventricolare profonda . lo studio in diffusione ( dwi , mappe adc e diffusion tensor imaging , dti ) stato ottenuto sul piano assiale utilizzando sequenze pulsed - gradient se eco - planari ( tr / te 8000 / minimum ms , tempo di acquisizione dwi 44 s e 6 min 57 s per il dti ) senza ( b - value = 0 ) e con gradienti di diffusione ( b - value = 1000 s / mm2 ) applicati lungo 25 direzioni per coprire uniformemente e tridimensionalmente il volume di interesse . ulteriori immagini pesate in diffusione sono state acquisite sul piano assiale con gli stessi parametri fatta eccezione per il b - value che stato impostato in valori variabili compresi tra 500 e 2500 s / mm2 ( 500 , 1000 , 1500 , 2000 e 2500 ) per un totale di cinque diverse acquisizioni . analisi dei dati la successiva elaborazione dei dati stata effettuata utilizzando una workstation unix . 
le alterazioni della sostanza bianca sono state analizzate sia qualitativamente , con riferimento alle variazioni di intensit di segnale nelle varie sequenze , che semi - quantitativamente considerando la loro radiol med ( 2009 ) 114 : 461474 tensor diagonalisation , of the main eigenvalues min , med , and max , were generated and the fractional anisotropy index ( fai ) , was derived from the eigenvalues for each pixel . 
 the analysis was performed on parieto - occipital wm , as all patients exhibited dwi changes in this region ; a spherical region of interest ( roi ) of uniform size ( ~45 mm2 ) was placed on the dwis and adc maps , and eigenvalues and fai values were then calculated . 
these data were confirmed by dti quantitative analysis , as decreased adc values but normal fai indices were found in the rois located on the hyperintense parieto - occipital wm ( table 1 )  . 
qualitative analysis of anisotropy images acquired with b - values > 1 , 000 s / mm2 showed an increased contrast between normal tissue and t2 / flair / dwi - mri hyperintense areas . 
il punteggio utilizzato stato calcolato come segue : 1 punto per lesioni interessanti solo la sostanza bianca profonda ( coinvolgimento limitato ) , 2 punti per lesioni interessanti anche la sostanza bianca sottocorticale ( coinvolgimento intermedio ) , 3 punti per leventuale coinvolgimento del tronco e / o del cervelletto ( coinvolgimento severo )  . il valore di phe cerebrale stato quantificato valutando lampiezza del picco di phe a 7 , 36 ppm in relazione al picco di cr / pcr a 3 , 05 ppm ( considerato come un valore interno costante e quindi di riferimento , usando il software sage / idl )  . 
gli altri metaboliti ( naa , cho , cr / pcr e mi ) sono stati analizzati utilizzando lcmodel software . le immagini in diffusione sono state analizzate utilizzando una relazione mono - esponenziale tra lintensit di segnale e il segnale prodotto della matrice b ( matrice 33 che esprime la relazione tra lattenuazione di segnale e gli elementi della matrice del tensore di diffusione )  . 
 lanalisi stata effettuata sulla sostanza bianca parietooccipitale poich tutti i pazienti presentavano alterazioni di segnale in dwi in questa regione ; una regione di interesse ( roi ) sferica e di misura uniforme ( ~45 mm2 ) stata posizionata sulle immagini pesate in diffusione , quindi mappe di adc , autovalori e valori di fai sono stati calcolati . 
the advantages of a higher mr field , with respect to the low - field system used to date , is a larger diagnostic ability in the management of patients with this pathology . 
resolution quality tends to be privileged in clinical practice , with acquisition of a larger number of slices of reduced thickness , use of smaller fov and broader matrices , and acquisition times similar to those of 1.5 - t ai soggetti normali . 
questi dati sono stati confermati dalla analisi quantitativa del dti : nelle regioni di interesse localizzate nelle aree iperintense della sostanza bianca parieto - occipitale stato trovato un valore di adc ridotto ma un normale valore di fai ( tabella 1 )  . 
lanalisi qualitativa delle immagini dellanisotropia , acquisite con b - value pi elevato di 1000 s / mm2 , mostra un aumento del contrasto tra il tessuto normale e le aree di iperintensit in t2 / flair / dw - mri . 
2a - e proton magnetic resonance spectroscopy allows detection of an abnormal phenylalanine ( phe ) signal at 7.36 pp values of the main metabolites [ n - acetylaspartate ( naa ) , choline - containing compounds ( cho ) , creatine ( cr ) / phosphocreatine ( pcr ) ] were normal ( a , arrow )  . 
all patients exhibit variable white - matter hyperintensities on t2 ( c ) and fast low - angle inversion recovery ( flair ) ( d ) scans , mainly in temporal , occipital and periatrial regions . 
in our work , instead , we found the optimum acquisition time as a tradeoff between a time - consuming multimodal acquisition and the patients comfort during the exafurther technological advances are expected to overcome some minor limitations of this system , such as field discussione in tale studio nei pazienti con pku si confermano i dati dei precedenti studi circa la frequenza e le caratteristiche delle alterazioni della sostanza bianca e le correlazioni tra il radiol med ( 2009 ) 114 : 461474 fig . 
a questo valore il confronto dellintensit di segnale sullasse x ( a ) e y ( b ) permette di rilevare una sottile variazione di segnale nella sostanza bianca alterata in relazione ad una parziale conservata anisotropia ( freccia gialla )  . inhomogeneity , susceptibility and chemical - shift artefacts , high specific absorption rate ( sar ) and acoustic noise . in detail , the use of higher fields for spectroscopy allows reduced acquisition time ( higher s / r ) and improved spectral resolution [ 18 , 19 ]  . 
as a result of such improvements ( increased snr and greater spectral resolution compared with 1.5 - t studies ) , the phe signal was easily detected and was measurable despite the low phe concentrations . 
the relative amplitude of the phe signal increased linearly with blood phe up to 1 , 200 micromoles , where growing dispersion of brain phe values was noted , suggesting a more marked interindividual variability , probably due to saturation of the specific phe transport system at the level of the bloodbrain barrier ( bbb )  . a short te ( 35 ms ) was applied better to detect the phe signal as well as those of the principal metabolites . 
furthermore , spectroscopic studies with longer te are subject to greater snr loss at 3.0 t than at 1.5 t due to t2 reduction at higher field strengths and increased peak line width in relation to reduced t2 and microscopic and macroscopic body inhomogeneities . 
these features allow an increased b - value to enhance the anisotropic effect , thus improving the quality of more complex examinations such as fai , diffusion tensor and tractography , which are poorly displayed on 1.5 - t images , even with multiple grado di severit e parametri clinici e laboratoristici . 
per ottenere maggiori informazioni sulla patogenesi di tali alterazioni abbiamo condotto con apparecchiatura a 3 , 0 t uno studio rm multimodale che ha compreso nel protocollo uno studio di base , di spettroscopia e di diffusione al fine di migliorare , sfruttando i vantaggi derivanti dalluso dellalto campo rispetto a quello dei tradizionali sistemi a 1 , 5 t , la capacit diagnostica che pu risultare utile nel management di tali pazienti [ 1517 ]  . in generale lintroduzione di magneti ad alto campo ha infatti portato dei benefici in campo neuroradiologico . 
il confronto delle immagini acquisite con sistemi a 3 , 0 t rispetto a quelle ottenute con 1 , 5 t ha mostrato degli indubbi vantaggi quali : aumento della risoluzione spaziale , temporale e di contrasto , intensit di segnale pi elevato , ridotto tempo di acquisizione , maggiori e pi avanzate applicazioni , elevata sensibilit ed eccellente potere diagnostico nelle sequenze con mezzo di contrasto . 
 il neuroradiologo quindi , grazie allalto s / r dellalto campo , utilizzando lo stesso tempo di un esame con sistemi a 1 , 5 t , pu ottenere immagini di qualit superiore ( aumentando la matrice o riducendo lo spessore di strato o il fov ) oppure immagini della stessa qualit di un basso campo ma in un tempo ridotto : ci si traduce in un maggior confort per il paziente e in una riduzione degli artefatti da movimento . 
la qualit della risoluzione tende ad essere privilegiata nella pratica clinica , grazie allacquisizione di un maggior numero di slices con uno spessore di strato ridotto tramite lutilizzo di un fov pi piccolo , di matrici pi ampie con un tempo di acquisizione risultante simile a quello speso se si utilizzano scanner a 1 , 5 t . 
4a , b comparison of proton magnetic resonance spectroscopy brain phenylalanine ( phe ) detection at 1.5 t ( a ) and 3.0 t ( b ) at 7.36 ppdetection of phe signal in the 1.5 - t study requires a 32 - cc volume of interest ( voi )  . 
4a , b confronto della fenilalanina cerebrale rilevata con la spettroscopia protonica a 1 , 5 t ( a ) e 3 , 0 t ( b ) a 7 , 36 ppla documentazione del segnale della fenilalanina a 1 , 5 t necessita di un voi di 32 cc . 
luso di un pi piccolo voi ( 8 cc ) riduce gli effetti da sovrapposizione con altri metaboliti quali istidina , omocarnosina , macromolecole presenti a 7 , 3 ppm . radiol med ( 2009 ) 114 : 461474 quale compromesso tra il tempo necessario per uno studio multimodale e che garantisse un adeguato confort per il paziente durante lesame . nello specifico in spettroscopia luso dellalto campo permette di ridurre i tempi di acquisizione ( in virt del pi alto s / r ) ma anche migliora la risoluzione spettrale [ 18 , 19 ] la maggior ampiezza del chemical shift dei metaboliti in esame permette infatti di avere una migliore risoluzione spettrale che si traduce in una pi definita separazione dei picchi adiacenti che invece con un sistema a pi basso campo andrebbero a sovrapporsi . 
in virt di tali miglioramenti ( aumento del s / r e migliore risoluzione spettrale ) possibile individuare e misurare pi facilmente il picco della phe , persino a basse concentrazioni . 
lampiezza relativa del picco di phe aumenta linearmente con la concentrazione ematica della stessa sino a un valore di 1200 micromoli oltre il quale si osserva una dispersione dei valori cerebrali di phe dovuta probabilmente a una variabilit individuale derivante dalla saturazione dei sistemi di trasporto della phe localizzati a livello della barriera emato - encefalica ( bee )  . stato utilizzato un te ridotto ( 35 ms ) per avere una migliore individuazione del segnale ( picco ) della phe e degli altri principali metaboliti in esame . 
utilizzando un te pi lungo si avrebbe una riduzione del rapporto s / r pi marcata con lutilizzo di sistemi a 3 , 0 t che con quelli a 1 , 5 t , per effetto della riduzione del segnale in t2 che si ha ad alto campo , dellaumento dellampiezza della linewidth causata dalla riduzione del segnale sempre in t2 e per le disomogeneit a livello microa macro - scopico . anche limaging pesato in diffusione beneficia dellaumento del rapporto s / r , della risoluzione spaziale e della accuratezza delle immagini [ 1517 ]  . 
si verifica in tal modo un miglioramento della qualit di alcune misurazioni come la fractional anisotropy ( fai ) , il tensore di diffusione ( dti ) e di alcune tecniche di ricostruzione come la trattografia . questi valori non sono ben rappresentati a causa del basso s / r utilizzando un sistema a 1 , 5 t anche se si dovesse aumentare il numero delle eccitazioni . 
infatti le ricostruzioni dei tratti assonali riflettono con maggior accuratezza la realt anatomica , specialmente a livello delle biforcazioni dei fasci . radiol med ( 2009 ) 114 : 461474 excitations , owing to the low snr . 
in fact , the reconstructed dti trajectories reflect more accurately the underlying axonal fibres , particularly crossing or bifurcating bundles . for some years , it has been possible to reconstruct threedimensional pathways of wm tracts by combining anisotropy characteristics and directionality , applying the technique known as fibre tracking or tractography . 
the method allows reconstruction of continuous fibre trajectories by sequentially piecing together discrete and shortly spaced estimates of fibre orientation to form continuous fibre trajectories [ 2022 ]  . the colour map is an easy method to show dti values , as it displays the main direction of wm fibres in three fundamental colours : green , blue and red . 
in particular , ontogenetically older fibre systems , such as the optic radiation , had a normal appearance . wm changes depicted in pku patients do not therefore necessarily reflect an altered organisation of cerebral myelin pathways detectable on dti . 
some mr findings in pku appear to be more consistent with reversible dysmyelination associated with an increased myelin turnover than with a demyelination process [ 2 , 15 , 25 , 26 , 29 , 30 ]  . our latest report of decreased adc values with preserved anisotropic diffusivity on dwi - mri and abnormal elevation of brain phe levels on 1h - mrs [ 31 ] seems to be in line with the hypothesis of water accumulation in myelin sheaths [ 7 ] due to an abnormally increased myelin turnover with consequent preservation of anisotropy , which can occur only in structures whose microscopic barriers have not been either destroyed or partially vacuolated . however , a third hypothesis consistent with these findings is that of intracellular accumulation of a hydrophilic metabolite produced by the phe hydroxylase defect , leading da alcuni anni possibile effettuare una ricostruzione tridimensionale del decorso delle fibre mieliniche . 
utilizzando le caratteristiche di anisotropia e tecniche note come il fiber tracking o trattografia si ricostruisce la direzione delle fibre nervose interpolando in modo sequenziale , stime discrete e poco spaziate dellorientamento della fibra per ottenere la sua traiettoria continua [ 2022 ]  . 
 ne derivano mappe a colori che costituiscono un metodo semplice per mostrare i valori del tensore di diffusione attraverso la visualizzazione delle principali direzioni delle fibre nervose in tre diversi colori ( grigio , blu e rosso )  . lapplicazione di tale tecnica nei pazienti con pku ci consente di poter valutare lintegrit delle fibre nervose nelle aree caratterizzate da riduzione dei valori di adc . 
al momento attuale il principale problema nella tecnica del fiber tracking e nella rappresentazione delle mappe a colori dovuto alla difficolt di ottenere una buona delineazione delle fibre mieliniche , senza una parziale contaminazione da parte dei tratti nervosi adiacenti [ 24 ]  . lanalisi del dti ha mostrato una riduzione dei valori di adc nelle aree iperintense nellimaging di base , in linea con i precedenti lavori in letteratura [ 7 , 8 ]  . 
in particolare le fibre ontogeneticamente pi vecchie come i tratti ottici appaiono normali . le alterazioni della sostanza bianca , viste nella pku , non necessariamente riflettono una alterazione architetturale del decorso delle fibre mieliniche , valutato con dti . 
le alterazioni della sostanza bianca nei pazienti con pku sono state documentate in molti studi effettuati con sistemi rm a pi basso campo , ma il loro significato non ancora stato chiarito [ 315 , 2528 ]  . 
alcuni pattern rm sembrano essere correlati pi con un reversibile processo di dismielinizzazione che con uno di demielinizzazione [ 2 , 15 , 25 , 26 , 29 , 30 ]  . in un precedente nostro lavoro la riduzione dei valori di adc con una preservazione dei valori di fa in diffusione e lanormale incremento dei livelli di phe cerebrale in spettroscopia protonica [ 31 ] potrebbero suggerire un accumulo di acqua nelle guaine mieliniche [ 7 ] dovuto a un incremento anomalo del turn - over mielinico stesso che si ha in strutture in cui le barriere microscopiche non sono state ancora del tutto degradate o vacuolizzate . 
 una terza ipotesi in linea con le nostre valutazioni che laccumulo di una metabolita idrofilico intracelllulare prodotto dalla phe - idrossilasi porta a un aumento del contenuto di acqua intracellulare . 
5a - d imaging di diffusione : mappa di adc ( a ) con selezione di una roi , mappa di fai ( b ) e a colori ( c ) ; i valori delle roi di adc e fa ( d ) misurati nelle aree di ciascun paziente ( punti ) e in range normali ( barra : meansd )  . to increased intracellular water content [ 31 ]  . 
the latter data require further examination given that no other abnormalities were detected by in vivo mrs examination , apart from the phe increase . pattern di dwi sia le anormalit dei valori ottenuti con la spettroscopia ( accumulo di phe con valori normali degli altri metaboliti )  . 
questi ultimi dati richiedono ulteriori studi dato che nessuna altra anomalia stata rilevata nellesame di spettroscopia in vivo a parte lincremento della phe . conclusions conclusioni the higher snr of high - field mr systems is a resource that neuroradiologists must exploit in clinical practice , as the higher the snr , the more the imaging protocols can be adjusted . 
i sistemi a 3 , 0 t permettono infatti di effettuare oltre a un accurato studio di base , anche delle valutazioni di carattere fisiologico , metabolico e funzionale che consentono di aumentare la sensibilit e la specificit del potere diagnostico della rm . sono comunque necessari ulteriori progressi tecnologici che permettano di superare alcune piccole limitazioni di tali sistemi rm come la disomogeneit del campo magnetico , radiol med ( 2009 ) 114 : 461474 inhomogeneity , susceptibility and chemical - shift artefacts , high sar and acoustic noise . the growing diffusion of high - field mr systems over the next few years will help a clearer understanding of the pathogenic role of signal abnormalities of the cerebral parenchyma in patients having several kinds of neurological diseases , such as pku . 
in addition , measurement of brain phe levels with 1h - mrs and dwi - mr parameters could become the technique of choice to monitor the influx of blood phe into brain tissue , especially during therapy in follow - up studies . gli artefatti da suscettibilit magnetica e da chemical shift , lelevato sar ( specific absorption rate ) e lalto rumore acustico . la crescente diffusione di tali sistemi nei prossimi anni permetter una migliore comprensione delle cause di alterazione del segnale in pazienti con patologie come la pku . 
maria delle croci , v.le randi 5 , 48100 ravenna , italy 2scuola di specializzazione in radiodiagnostica , universit degli studi di ferrara , corso giovecca 203 , 44100 ferrara , italy 3servizio di anatomia patologica , ospedale civile s.maria delle croci , v.le randi 5 , 48100 ravenna , italy 4istituto di radiodiagnostica , universit degli studi di ferrara , corso giovecca 203 , 44100 , ferrara , italy correspondence to : g . 
cdus revealed an inflammatory process in 277 patients ( 34.58% ) , testicular trauma in 112 ( 13.9% ) , funicular torsion or torsion of the vestigial remnant in 44 ( 5.4% ) , findings suggestive of testicular neoplasm in 35 ( 4.3% ) and no abnormality in 41.5%. 
mri , used to further investigate the cdus findings in 46 cases , showed three cases of intraparenchymal haematoma , one of intrascrotal cavernous body rupture , one of testicular abscess with intrascrotal fistula , two of testicular infarction and 15 of neoplasmri allowed the exclusion of focal abnormalities in ten patients with testicular microlithiasis , in three with chronic orchitis and in four with atrophic involution . 
on the basis of our experience , cdus is irreplaceable as an initial approach to patients affected by scrotal disease , whereas mri is an ideal second - line investigation . 
lecd ha rilevato : in 277 pazienti ( 34 , 58% ) processo flogistico , in 112 ( 13 , 9% ) trauma del testicolo , in 44 ( 5 , 4% ) torsione del funicolo o di un residuo embrionario , in 35 ( 4 , 3% ) alterazioni riconducibili ad eteroplasia testicolare mentre nel 41 , 5% non erano presenti alterazioni patologiche . 
in 46 casi si ricorsi alla rm per chiarimento o miglior definizione diagnostica del reperto ecd rilevando : 3 casi di ematoma intraparenchimale , 1 caso di rottura intrascrotale del corpo cavernoso , 1 caso di ascesso testicolare con fistola intrascrotale , 2 casi di infarto , 15 casi di eteroplasia . 
la rm utile in casi selezionati , potendo rilevare situazioni complesse e precedentemente insospettabili , risultando in un miglioramento della gestione del paziente e in un contenimento globale dei costi . 
 radiol med ( 2009 ) 114 : 414424 keywords scrotum mri color doppler ultrasound scrotal disorders ultrasonography parole chiave scroto rm eco - color doppler patologia scrotale ultrasonografia introduction introduzione colour doppler ultrasonography ( cdus ) plays a key role as a first - line approach to scrotal disease , as it can help solve diagnostic dilemmas and establish a precise diagnosis , thus leading to appropriate clinical and therapeutic decisions . nevertheless , when the cdus findings are difficult to interpret in relation to the patients clinical data and medical history , or when the clinical and sonographic findings are unjustified , magnetic resonance imaging ( mri ) may be used to elucidate or reveal unusual features [ 1 ]  . the value of mri as a second - line technique after inconclusive sonography [ 2 , 3 ] has rarely been addressed in the literature , and the few existing studies are dated and involve small patient populations . 
the aim of this study was to review our experience of the past 7 years in an attempt to validate the usefulness of cdus in the study of scrotal disease and evaluate the role of mri in selected cases . materials and methods from 2000 to 2007 , 801 male subjects aged from 0 to 87 years were referred to our department to undergo cdus of the scrotuexaminations were carried out on a ge logic 7 sonographic unit with a 715 mhz linear - array probe and colour doppler , power doppler , and b - flow imaging . patients included urgent cases referred from the emergency department and high - priority outpatients referred by the urologist to investigate suspicion of acute or subacute scrotal disease . transverse planes panoramic grey - scale scans were obtained in the longituto compare size and dinal and echogenicity on the two sides . 
colour doppler imaging was then performed , with optimisation of the scanner to obtain the highest sensitivity to slow flow , with low pulse repetition frequency ( prf ) , low wall filter and appropriate colour ga in patients with suspected torsion or infarction , the asymptomatic side was evaluated first to ensure that the parameters for flow evaluation had been set appropriately . mri was performed in 46 patients to confirm or elucidate the cdus findings . 
the criteria adopted to define inconclusive sonographic evaluation were unclear nature of the lesion , inability to delineate the lesion spatially in terms of site and / or extension , conflicting clinical and sonographic diagnosis and marked structural heterogeneity associated with conditions predisposing to malignancy , such as testicular leco - color doppler ( ecd ) riveste un ruolo di primo approccio nella patologia dello scroto risolvendo nella maggior parte dei casi lenigma diagnostico oppure delineando in modo esaustivo il quadro patologico , permettendo cos corrette decisioni e idonei approcci clinico - terapeutici . 
pur tuttavia , in presenza di quadri ecd di dubbia interpretazione alla luce del reperto clinico - anamnestico o in presenza di reperti clinico - ecografici ingiustificabili , la risonanza magnetica ( rm ) pu trovare applicazione per risolvere , chiarire o svelare aspetti a volte inusuali [ 1 ]  . solo pochi autori hanno esaminato il ruolo della rm come metodica di secondo livello in caso di reperti ecografici non esaustivi [ 2 , 3 ]  . 
finalit del lavoro stata quella di effettuare una revisione della nostra casistica degli ultimi 7 anni allo scopo di riconfermare lutilit dellecd nellapproccio alle patologie dello scroto e far emergere il ruolo della rm in casi selezionati . materiali e metodi dal 2000 al 2007 sono stati inviati al nostro servizio 801 pazienti maschi di et compresa tra 0 e 87 anni , per essere sottoposti ad indagine ecd dello scroto con ecografo ge logic 7 con sonda lineare 715 mhz con modulo color doppler , power doppler e b flow . 
i pazienti erano giunti alla nostra osservazione in regime di urgenza , in quanto inviati dal pronto soccorso , oppure in regime prioritario ambulatoriale su consiglio dello specialista urologo , nel sospetto di una patologia acuta o subacuta . sono state eseguite scansioni in scala di grigi quanto pi possibile panoramiche , sui piani longitudinale e trasversale , per confrontare le dimensioni e lecogenicit dei due lati . 
lo studio color doppler stato condotto successivamente , ottimizzando lapparecchiatura per ottenere la massima sensibilit ai flussi lenti , con una bassa pulse repetition frequency ( prf ) , bassi filtri di parete e un appropriato guadagno di colore . 
nei casi di sospetta torsione o infarto , il lato asintomatico stato valutato per primo , per assicurarsi che i parametri di valutazione del flusso fossero settati in modo opportuno . in 46 pazienti si ritenuto di procedere ad indagine rm , per confermare o chiarire il dato ecd , rilevando in alcuni 416 radiol med ( 2009 ) 114 : 414424 microlithiasis , testicular retention and chronic orchitis . mri was performed on a 1.5 - tesla philips achieva unit with a 14 - cm circular surface coil . 
for studying the scrotum in the three orthogonal planes , a t2 - weighted fast spin - echo sequence with a 1012 - cm field of view and a 256256 matrix was used . 
axial t1 - weighted spoiled gradient - echo images were also obtained to detect haemorrhage . only selected cases were studied with mri following intravenous administration of gadolinium with diethylenetriamine penta - acetic acid ( gd - dtpa ) ; in these cases , axial and coronal t1 - weighted spoiled gradient - echo sequences with fat saturation were obtained after contrast injection . definitive diagnoses were confirmed at surgery in the cases of funicular torsion , morgagnis hydatid torsion and inguinoscrotal hernia . 
in the case of inflammatory processes , thrombophlebitis of the pampiniform plexus , complicated cysts and scrotal trauma with intact tunica vasculosa , the diagnosis was declared ex adjuvantibus after successful medical treatment , as confirmed by lesion regression at serial us follow - up and resolution of clinical symptoms . results among the 801 patients examined , medical history , clinical data and cdus findings led to a definite diagnosis of inflammatory process in 277 patients , traumatic lesion in 112 , funicular torsion in 33 ( three cases appearing at birth , with intrauterine torsion ) and torsion of the hydatid of morgagni [ 4 , 5 ] in 11 . 
i criteri utilizzati per definire la valutazione ecografia non esaustiva sono stati : incerta natura della lesione , incapacit dellecografia di definire spazialmente la lesione in termini di sede e / o di estensione della stessa , la discrepanza tra la clinica e la diagnosi ecografia , la presenza di una marcata disomogeneit strutturale in presenza di condizioni predisponesti linsorgenza di neoplasie quali microlitiasi testicolare ( mt ) , ritenzione testicolare , orchite cronica . abbiamo impiegato unapparecchiatura philips achieva 1 , 5 tesla con una bobina di superficie , circolare da 14 cm . per la patologia del canale inguinale si studiata la pelvi mediante scansioni assiali usando un campo di vista pi ampio . 
per lo studio dello scroto sui 3 piani ortogonali sono stati utilizzati : una sequenza fast spin - eco pesata in t2 , un campo di vista 1012 cm e una matrice 256256 . 
sono anche state acquisite immagini assiali spoiled - gradient - eco t1 pesate , molto utili per identificare lemorragia . lacido dietilen - triamino - penta - acetico chelato con gadolinio ( gd - dtpa ) , per via endovenosa , stato somministrato solo in casi selezionati ; sono state condotte acquisizioni assiali e coronali dopo somministrazione del mezzo di contrasto , sfruttando sequenze spoiled - gradient - eco con saturazione per il grasso t1 pesate . 
per le lesioni di sospetta origine neoplastica si proceduto con esame citologico estemporaneo intraoperatorio seguito in caso di reperto dubbio o positivo da orchiectomia e in caso di negativit da nodulectomia . 
nei processi flogistici , nelle tromboflebiti del plesso pampiniforme , nelle cisti complicate e nei traumi del testicolo con conservazione dellintegrit della tunica vasculosa , la diagnosi stata confermata ex adjuvantibus dal successo della terapia medica , confermato dalla regressione delle lesioni nel corso di controlli ecografici seriati e dalla regressione del quadro clinico . 
 risultati tra gli 801 pazienti esaminati lanamnesi , i dati clinici e i reperti ecd hanno permesso la diagnosi definitiva di : processo flogistico in 277 pazienti , lesione traumatica in 112 , torsione del funicolo in 33 casi ( in 3 con comparsa alla nascita e torsione intrauterina ) e torsione dellidatide del morgagni [ 4 , 5 ] in 11 pazienti . 
in 15 patients , mri confirmed the suspicion of neoplastic lesion by showing t1 isohyperintensity and clear t2 hypointensity relative to the surrounding parenchyma . the use of contrast material allowed us to evaluate lesion vascularity ( with findings virtually coincident with cdus and b - flow imaging )  . 
in ten patients with testicular microlithiasis on cdus , mri enabled us to rule out alterations in signal intensity or enhancement that might indicate ecografica , sottoposti a rm come indagine di secondo livello , sono stati 46 pari al 5 , 74% . 
in 15 pazienti la rm ha confermato il sospetto di lesione neoplastica in base allaspetto isoiperintenso in t1 e francamente ipointenso in t2 rispetto al parenchima circostante . lutilizzo del mdc ha permesso di valutare la vascolarizzazione delle lesioni ( con reperto sostanzialmente sovrapponibile al dato ecd e b flow )  . 
in 10 pazienti con reperto ecd di mt la rm ha permesso di escludere con sicurezza alterazioni di segnale o di contrast - enhancement ( c.e. ) riferibili a lesioni parenchimali ( in 1 caso ha consentito di rilevare accumulo focale di calcio - pirofosfatodiidratato )  . 
in 4 pazienti affetti da ritenzione testicolare grazie alla rm stato possibile identificare la sede del testicolo atrofico non visibile ecograficamente , differeziando tale condizione dallagenesia testicolare , ed escludere una patologia eteroproduttiva a cui tali soggetti sono predisposti . 
3a - c cisti intrascotale con contenuto infiammatorio : a aspetto ecd ; b rm : sequenza pesata in t1 ; c rm sequenza pesata in t2 . parenchymal lesions ( in one case , it allowed detection of a focal accumulation of calcium - pyrophosphate - dihydrate )  . mri was also used to confirm the sonographic diagnosis of inguinoscrotal hernia in three cases , in which it showed the presence of intestinal loops in the scrotal region . 
in four patients with cryptorchidism , mri helped to locate the undescended testis , which was not visible at us , to differentiate this condition from testicular agenesis and to exclude possible malignancy . 
likewise , it enabled us to exclude nella nostra casistica i casi ritenuti dubbi e sottoposti a rm come indagine di secondo livello sono stati 46 pari al 5 , 74% . 
 radiol med ( 2009 ) 114 : 414424 areas of signal alteration or increased contrast enhancement in three patients with chronic orchitis in whom cdus had shown marked echostructural inhomogeneity . 
mri was also used to follow - up conservative treatment in two patients with scrotal trauma and cdus findings of discontinuity of the tunica albuginea and intact capsular vascularity . discussion in our series , mri was performed as a second - line investigation in 46 patients ( 5.74% ) with inconclusive cdus findings . 
this pattern , which has been previously described in the literature [ 6 ] , is particularly useful for solving interpretation doubts : it should be noted that 10%15% of testicular neoplasms are detected as a consequence of traumas [ 79 ]  . in one patient with a large intrascrotal collection , mri enabled a diagnosis of epididymo - orchitis with abscess formation and intrascrotal fistula , which could not be detected by cdus . 
on the basis of the literature and patients clinical data , we interpreted the findings as complicated testicular cysts , an interpretation that was confirmed ex adjuvantibus after symptom resolution with appropriate medical treatment . 
si tratta di un reperto , gi descritto in letteratura [ 6 ] , utile laddove sussistano dubbi interpretativi : si tenga conto che il 10%15% delle lesioni eteroplasiche testicolari vengono scoperte in conseguenza di un trauma [ 79 ]  . in un pazienze con voluminosa raccolta intrascrotale la rm ha permesso di rilevare orchiepididimite ascessualizzata con tramite fistolizzato in sede intrascrotale , difficilmente rilevabile allindagine ecd . 
analogamente basandoci su tali osservazioni e sulla clinica abbiamo interpretato i nostri reperti come cisti del testicolo complicate , confermate poi ex juvantibus dalla risoluzione del quadro dopo adeguata terapia medica . 
contrast - enhanced t1 sequences demonstrated the characteristic rim of enhancement delimiting the lesion [ 12 , 13 ]  . in 15 patients with cdus findings suggestive of testicular neoplasm , mri confirmed the diagnosis ( definitive histology revealed 11 cases of germ - cell tumour and four benign neoplasms , two of which were adenomatoid tumours and two sertoli - cell tumours )  . 
in these patients , mri also enabled preoperative staging by depicting possible infiltration of the tunica albuginea , tunica vaginalis , epididymis and / or of the para - epididymal tissues . 
in questi pazienti la rm ha inoltre permesso la stadiazione pre - operatoria , potendo definire tunica albuginea , della tunica vaginale , dellepididimo e / o dei tessuti paraepididimari . 
in letteratura si trovano opinioni discordanti sul significato della mt , tuttavia prevalgono le tesi che attribuiscono alla mt il ruolo di condizione precancerosa [ 1418 ]  . in un paziente che presentava formazione dubbia del testicolo , del diametro di circa 1 cm , in sede parailare , iperecogena e senza significativo flusso intralesione all ecd , la rm ha evidenziato alta intensit del segnale nelle sequenze pesate in t1 e basso segnale in t2 . 
tale reperto risulta invariato da 3 anni e , alla luce di quanto riferito da alcuni aa [ 1921 ] , pu essere attribuito ad accumulo di calcio - pirofosfato - diidratato . la rm non in grado di identificare la mt [ 2224 ] : questo aspetto pu facilitare il rilievo di aree di alterato segnale nel parenchima testicolare in pazienti affetti da questa condizione . 
perci , ove la disomogeneit ecostrutturale del parenchima associata alla mt non ha permesso lassoluta esclusione con lecd di lesioni eteroproduttive , siamo ricorsi alla rm che ha escluso alterazioni di segnale radiol med ( 2009 ) 114 : 414424 fig . 
5a - d infarto testicolare ; a immagine ecd ; b immagine rm pesata in t1 ; c immagine rm pesata in t2 ; d immagine rm con mdc . low signal intensity on t2 . 
this finding has remained unchanged for 3 years and , based on previous reports [ 1921 ] , it may be due to an accumulation of calciumpyrophosphate - dihydrate . mri is unable to depict testicular microlithiasis [ 2224 ] , and this may facilitate the detection of parenchymal areas with pathological signal in affected patients . 
therefore , when the parenchymal echostructural inhomogeneity associated with testicular microlithiasis did not allow malignant lesions to be confidently excluded with cdus , the patient was further studied with mri , which revealed no signal alterations or areas of contrast enhancement in the testis . similarly , mri proved useful in three patients with marked parenchymal echostructural alteration due to chronic inflammation , in whom it confirmed the cdus findings and revealed no focal alteration . four patients with atrophic testicular involution secondary to cryptorchidism and / or funicular torsion and who presented diffuse parenchymal echostructural alterations on cdus were also studied with mri to exclude focal parenchymal lesions . 
cryptorchidism is a well - known risk factor for nel testicolo , ma soprattutto non ha rilevato aree di potenziamento dopo mezzo di contrasto . con analogo significato la rm risultata utile in 3 pazienti con marcata alterazione ecostrutturale del parenchima per flogosi cronica , nei quali ha confermato il reperto ecd non rilevando alterazioni focali . sempre per escludere lesioni focali parenchimali sono stati sottoposti a rm 4 casi di involuzione atrofica del testicolo , secondaria a ritenzione testicolare e / o a torsione del funicolo , che presentavano sovvertimento ecostrutturale diffuso del parenchima allecd . 
la ritenzione testicolare rappresenta un noto fattore di rischio per linsorgenza di neoplasie testicolari [ 2527 ] e in questi pazienti consigliato il monitoraggio ecografico : a volte la marcata alterazione ecostrutturale del parenchima e / o la scarsit del flusso parenchimale all ecd nel testicolo atrofico , possono creare dubbi allecografista . 
6a - c trauma dello scroto con rottura della tunica albuginea e integrit della tunica vascolosa : a quadro ecd ; b controllo ecd ; c quadro rm in esiti di rottura della tunica albuginea post - traumatica . testicular neoplasm [ 2527 ] , and sonographic surveillance is recommended in all patients with this condition . 
our experience confirms the usefulness of mri to exclude cancerous lesions . in three cases , mri confirmed the cdus suspicion of omental herniation within the inguinal canal , thus proving its extreme utility in the study of this structure [ 7 ]  . a ruptured tunica albuginea is an indication for exploratory surgery [ 2832 ]  . 
our relatively limited experience demonstrates that surgery is required only in patients with compromised capsular vascularity , that is , of the tunica vasculosa that runs below the tunica albuginea . as is known , on reaching the lower pole of the testis , the testicular artery divides into branches that pierce the tunica albuginea and run along the periphery of the testis in a layer known as the tunica vasculosa . 
dalla nostra seppur limitata esperienza si evince che i pazienti da sottoporre a revisione chirurgica , sarebbero solo quelli con compromissione della vascolarizzazione capsulare e cio della tunica vasculosa che decorre sotto la tunica albuginea  . 
come noto larteria testicolare giunta in prossimit del polo inferiore del testicolo si suddivide in diversi rami , che decorrono alla periferia del testicolo al di sotto della tunica albuginea , formando la cos detta tunica vascolosa . 
da queste arterie capsulari si sviluppano branche centripete che penetrano nel parenchima testicolare decorrendo verso il mediastinum testis ove si arborizzano in rami ricorrenti [ 10 , 33 ]  . 
si pu radiol med ( 2009 ) 114 : 414424 parenchyma and run towards the testicular mediastinum , where they arborise into recurrent rami [ 10 , 33 ]  . 
consequently , it appears reasonable to believe that discontinuity of the tunica albuginea with normal capsular vascularity is an indication for conservative treatment and close clinical and imaging follow - up . conclusions in our experience , cdus is irreplaceable as a first - line approach to patients with scrotal disease . 
we have proposed cdus evaluation of tunica vasculosa integrity in cases of testicular rupture to determine the feasibility of a conservative approach , even in the presence of discontinuity of the tunica albuginea . testicular infarction ; mri is highly valuable in the diagnosis of intratesticular haematoma ; cysts with atypical , presumably inflammatory content ; testicular abscess with intrascrotal fistula ; and in the diagnosis and preoperative staging of testicular neoplasms . 
mri proved to be an ideal second - line modality to be used in selected complex cases , as it improved patient management , leading to fewer unnecessary surgical operations and lower overall costs . quindi sostenere lipotesi che la soluzione di continuit della tunica albuginea con integrit della vascolarizzazione capsulare rappresenti indicazione alla terapia conservativa , con stretto monitoraggio clinico - strumentale . conclusioni dalla nostra esperienza lindagine ecd appare di insostituibile utilit nel primo approccio al paziente con patologia scrotale . 
abbiamo proposto la valutazione con ecd dellintegrit della tunica vasculosa , nei casi di rottura del testicolo , al fine di valutare lipotesi di un approccio terapeutico conservativo , anche in presenza di soluzione di continuit della tunica albuginea . la rm si offre come metodica di insostituibile utilit nella diagnosi di ematoma intratesticolare , di cisti a contenuto atipico verosimilmente infiammatorio , di infarto testicolare , di ascesso testicolare con fistolizzazione intrascrotale nonch nella diagnosi e stadiazione preoperatoria delle eteroplasie testicolari . 
simonetti department of imaging diagnostics , molecular imaging , interventional radiology and radiotherapy , policlinico universitario tor vergata , viale oxford 81 , 00133 rome , italy correspondence to : e . 
twenty - eight women , mean age 50 years , and with a diagnosis of pudendal neuralgia on the basis of clinical and electromyographic criteria were enrolled in the study . 
in pudendal nerve entrapment , ct - guided perineural injection in the anatomical sites of nerve impingement is a safe and reproducible treatment with a clinical efficacy of 92% at 12 months . 
nella valutazione a ventiquattrore post - trattamento stato riferito un miglioramento qualitativo significativo della sintomatologia dolorosa in 21 casi su 27 ; in 24 su 27 casi stato riportato un miglioramento 20% dellindice di qualit della vita ( qol index ) nel follow - up clinico a 3 , 6 , 9 e 12 mesi . 
nella sindrome da intrappolamento del nervo pudendo , liniezione perineurale tc guidata delle sedi anatomiche di conflitto nervoso risulta una procedura sicura e ripetibile con una efficacia clinica nel 92% dei pazienti trattati nel follow - up a 12 mesi . parole chiave nevralgia blocco del nervo pudendo intrappolamento nel canale di alcock tomografia computerizzata guidata 426 introduction chronic pelvic pain can be defined as noncyclic pain in the pelvis , anterior abdominal wall below the umbilical line and lumbosacral region and / or glutei that persists continuously for at least 6 months and is sufficiently severe to cause functional disability and / or require nonspecific pharmacotherapy . 
although the exact prevalence of chronic pelvic pain in the two genders is unknown , 15%20% of women aged 1850 years are estimated to be affected [ 1 ]  . 
chronic pelvic pain may occur in a variety of clinical syndromes [ 4 ]  . the diagnostic and therapeutic roles of interventional radiology have increasingly gained importance in three specific chronic pelvic pain syndromes : pudendal neuralgia , piriformis syndrome syndrome and border nerve ( ilioinguinal , iliohypogastric and genitofemoral nerve neuropathy )  . pudendal neuralgia is a clinical entity that was underrecognised and poorly understood for many years [ 3 , 4 ]  . the pudendal nerve is a mixed sensory and motor nerve that arises from the somatic component of sacral nerve roots s2 and s4 on the ventral aspect of the piriformis muscle in the pelvic cavity and crosses the gluteal region , passing through the greater ischiatic foramen into the infrapiriformis canal . it supplies the anus , the urethral sphincters , the pelvic floor and the perineum and is responsible for genital sensitivity . the nerve is accompanied by the internal pudendal artery and is surrounded by a venous plexus ( pudendal neurovascular bundle )  . 
if thickened , duplication of the obturator fascia may also contribute to the entrapment [ 6 , 7 ]  . radiol med ( 2009 ) 114 : 425436 introduzione il dolore pelvico cronico si pu definire come dolore nonciclico localizzato alla regione pelvica , alla parete addominale anteriore inferiormente alla linea ombelicale e alla regione lombo - sacrale e / o ai glutei , che persiste continuativamente per almeno 6 mesi , di entit sufficiente da causare disabilit funzionale e / o richiedere cure farmacologiche generiche . 
sebbene la prevalenza del dolore pelvico cronico nella popolazione generale in entrambe i sessi non sia ancora completamente definita , si stima che ne siano affette circa il 15%20% delle donne di et compresa tra i 18 e i 50 anni [ 1 ]  . 
 il ruolo diagnostico e terapeutico della radiologia interventistica appare di crescente importanza in tre quadri sindromici di dolore pelvico cronico : nevralgia del pudendo , sindrome del piriforme e sindrome border nerve ( neuropatia iliaco - inguinale , iliaco - ipogastrica e del nervo genito - femorale )  . 
 la nevralgia del nervo pudendo stata unentit clinica a lungo non riconosciuta o scarsamente identificata [ 3 , 4 ]  . il nervo pudendo un nervo misto sensitivo e motorio , derivante dalla componente somatica delle radici del sacro s2 ed s4 dalla parte ventrale del muscolo piriforme nella cavit pelvica , attraversa la regione glutea passando attraverso il pi grande forame ischiatico nel canale infrapiriforme . 
il nervo predisposto allintrappolamento a livello della spina ischiatica ed allinterno del canale pudendo . alla spina ischiatica , il nervo pu essere compresso di frequente tra i legamenti sacrospinoso e sacrotuberoso . 
a livello del canale di alcock , il nervo pu essere compresso radiol med ( 2009 ) 114 : 425436 pudendal nerve sacrospinosus legament sacrotuberosus legament ischiatic spine pudendal canal fig . 
enmg is indicated for determining pudendal motor innervation prior to surgical decompression but not for locating the site of compression or monitoring the surgical procedure [ 12 ]  . just as there are no definitive clinical or imaging criteria for diagnosing pudendal neuralgia , neither is there a standard therapeutic approach , with conservative treatment , nerve block , decompressive surgery and neuromodulation all having shown to be useful [ 13 ]  . 
se ispessita , la duplicazione della fascia otturatoria pu anche contribuire essa stessa allintrappolamento [ 6 , 7 ]  . boisson [ 8 ] sugger per primo , nel 1966 , che la causa del dolore anoperineale cronico potesse essere una neuropatia ; altri autori hanno successivamente confermato tale ipotesi , definendo la nevralgia del pudendo come una neuropatia da entrapment [ 6 , 9 , 10 ]  . 
tuttavia se lintrappolamento senza dubbio la causa pi frequente di nevralgia del pudendo , altre eziologie sono state descritte [ 11 ] : polineuropatia periferica , neuropatia post - erpetica , neuropatia post - attinica , compressione neoplastica . anche se gli studi neurofisiologici [ 12 ] hanno contribuito alla conoscenza della malattia , non possono essere riconosciuti come indagine diagnostica di prima istanza . gli studi elettroneuromiografici ( enmg ) presentano limitate sensibilit e specificit nella diagnosi differenziale tra lesione nervosa da conflitto e sindrome da dolore perineale cronico . 
lesame enmg indicato nella definizione della innervazione motoria del territorio di innervazione del pudendo prima della decompressione chirurgica ma non nella localizzazione della sede di compressione o nel monitoraggio intra - operatorio [ 12 ]  . se la diagnosi di nevralgia del pudendo non ha criteri diagnostici clinico - strumentali definitivi , altrettanto valido per il suo trattamento . 
la radiologia interventistica si propone in modo efficace come terapia infiltrativa percutanea del nervo pudendo sotto guida tc , ecografica o fluoroscopica . lo scopo del presente lavoro di descrivere i vantaggi della tecnica di blocco tc guidata del nervo pudendo e confrontarla con altre tecniche di radiologia interventistica imaging - guidate recentemente proposte in letteratura . 
end point primario dello studio la risoluzione persistente della sintomatologia algica nel periodo di follow - up individuale . materiali e metodi nel periodo compreso tra maggio 2006 e gennaio 2008 sono state incluse nel nostro studio prospettico 28 donne con et media 50 anni e diagnosi di nevralgia del pudendo , posta sulla base di criteri clinici ed elettromiografici , con algia significativa e invariata / persistente dopo 6 settimane di terapia conservativa ( tabella 1 )  . 
lintensit minima del dolore > 5 / 10 vas score ( visual analog pain scale livello di dolore riferito a intensit , distress muscolare , spasmo muscolare , interferenza con normali attivit quotidiane ) per tre giorni consecutivi e dolore posturale intermittente valutato durante test biomeccanico . 428 radiol med ( 2009 ) 114 : 425436 this paper describes the advantages of ct - guided pudendal nerve block and compares it with other imagingrecently guided proposed in the literature . 
the primary end - point of the study was persistent pain relief in the follow - up period . radiology procedures interventional materials and methods between may 2006 and january 2008 , we recruited 28 women ( mean age 50 years ) with a diagnosis of pudendal neuralgia based on clinical and electromyographic ( emg ) criteria and suffering from persistent significant pain after 6 weeks of conservative therapy ( table 1 )  . 
minimum pain intensity was a score of > 5 / 10 on the visual analogue scale ( vas ) : pain level related to intensity , muscular distress , muscular spasm and interference with normal daily activities for 3 consecutive days and intermittent postural pain assessed with a biomechanical test . i pazienti ( n = 28 ) hanno firmato un consenso informato allo studio precedentemente approvato dalla commissione etica del nostro policlinico . 
tutte le pazienti , con evidenza clinica di dolore cronico inabilitante gravativo non urente e non - ciclico della regione ano - rettale , labbra e perineo sono state sottoposte a rm del rachide lombo - sacrale per escludere la presenza di ernia discale e / o impingement radicolare . 
 tutte le pazienti erano maggiorenni , con un test di gravidanza negativo ( 6 in et riproduttiva ) , con un peso corporeo 50 kg ed erano stabili da un punto di vista medico sistemico . 
il protocollo di trattamento prevede che le inoculazioni siano eseguite in successione a distanza di 15 giorni una dallaltra per 3 volte ; in ogni seduta la prima sessione effettuata a livello della spina ischiatica e la seconda a livello del canale pudendo [ 14 ]  . 
patients with clinical evidence of chronic , disabling , nonburning , noncyclic aching pain in the anorectal , labial and perineal regions underwent magnetic resonance imaging ( mri ) of the lumbosacral spine to rule out intervertebral disk herniation and / or radicular impingement . 
the scans should allow clear la paziente posta in decubito prono ; il protocollo impiegato si avvale della acquisizione di scansioni da 2 , 5 mm , con pitch 1 , estese dal tetto dellacetabolo alla sinfisi pubica . 
il nervo pudendo sovrasta la spina ischiatica esattamente a livello della inserzione del legamento sacrospinoso , ed rivestito a questo livello dalla superficie interna del legamento sacrotuberoso , visibile come una linea iperdensa sovrapposta alla parte ventrale del muscolo grande gluteo . 
previa disinfezione della cute della regione glutea , viene inserito un ago spinale da 22 g per via trans - glutea , verso il fascio pudendo con direzione verticale in corrispondenza della parte caudale della spina ischiatica , evitando il nervo sciatico . 
the pudendal nerve crosses the ischial spine exactly at the point where the sacrospinous ligament attaches to the spine , and at this level , it is covered by the inner surface of the sacrotuberous ligament , which appears as a dense linear structure over the ventral portion of the gluteus maximus muscle . 
after the skin of the gluteal region has been disinfected , a 22 - gauge spinal needle is inserted transgluteally and advanced towards the pudendal bundle following a vertical direction at the caudal extremity of the ischial spine , with care being taken to avoid the sciatic nerve . 
once the needle tip is correctly placed in the interligamentous space ( between the sacrospinous and sacrotuberous ligaments , as close as possible to the caudal portion of the ischial spine ) , 0.75 ml of diluted contrast agent ( 5% iomeron 300 mg / ml , bracco , milan , italy ) is injected , which should appear to surround the pudendal bundle in the interligamentous space . this is followed by an injection of a mixture of methylprednisolone ( 1 ml depo - medrol 40 mg / ml solution , pfizer , new york , ny , usa ) and lidocaine ( 1 ml 2% 200 mg / 10 ml solution , bioindustria lim , novi ligure , italy )  . 
si inietta quindi una miscela di metilprednisolone acetato ( 1 ml di soluzione di depo - medrol 40 mg / ml , pfizer , new york , usa ) e di lidocaina cloridrato ( 1 ml di soluzione al 2% 200 mg / 10 ml , bioindustria lim , novi ligure , italia )  . la lidocaina , anestetico long - acting , produce unanestesia cutanea del territorio del nervo pudendo e fa da indicatore dellubicazione esatta del blocco del nervo . 
il cortisonico provvede alla risposta a lungo termine sia per gli effetti anti - infiammatori degli steroidi che per la necrosi adiposa indotta dagli steroidi con riduzione dellazione compressiva peri - neurale . 
dopo aver introdotto un ago da 22 - gauge con decorso verticale tramite un approccio transgluteo , si dispone lago a livello del tessuto adiposo posto subito lateralmente alla fascia otturatoria . 
una volta valutata la corretta posizione della punta dellago mediante iniezione di una soluzione di 0 , 75 ml di mezzo di contrasto diluito , che dimostra il nervo pudendo allingresso del canale di alcock , somministriamo localmente la miscela di anestetico e di steroide nelle stesse quantit e proporzioni della prima iniezione . 
 per una valutazione dellesito del trattamento dal punto di vista della valutazione soggettiva del paziente , a ciascuna delle donne inserite al protocollo di studio stato radiol med ( 2009 ) 114 : 425436 fig . 
 to obtain patients subjective evaluation of outcome , each woman was given a questionnaire ( including the vas ; pain score referred to intensity , muscular distress , muscular spasm , interference with normal daily activities ) to be filled in once a week at the same hour throughout the follow - up period ( from 3 to 12 months ) and handed in at the monthly hospital visits . 
patients were examined and interviewed every month to rate their perceived quality of life ( qol index ) after treatment on a five - point scale ( 1 = qol worsened ; 2 = qol unchanged ; 3 = qol improved with occasional symptom remission ; 4 = qol improved with persistent symptom remission ; 5 = qol optimal , with disappearance of pain )  . results a total of 82 procedures were completed over 164 sessions ( table 1 )  . 
in one case , the procedure had to be discontinued because the patient had respiratory insufficiency and could sottoposto un questionario relativo al vas score ( visual analog pain scale livello di dolore riferito a intensit , distress muscolare , spasmo muscolare , interferenza con normali attivit quotidiane ) da compilare settimanalmente a casa , allo stesso orario del giorno per la durata del followup ( variabile da 3 a 12 mesi ) e riconsegnato mensilmente in ospedale . 
con cadenza mensile i pazienti trattati sono stati visitati ed intervistati per ottenere un valore individuale di percezione della qualit della vita post - trattamento ( qol index ) in una scala variabile da 1 ( peggioramento della qualit della vita dopo il trattamento ) a 5 ( qualit della vita ottimale con scomparsa della sintomatologia dolorosa ) , con valori intermedi di 2 ( qualit della vita invariata rispetto al pre - trattamento ) 3 ( qualit della vita migliorata con remissione saltuaria dei sintomi ) e 4 ( qualit della vita migliorata con remissione persistente dei sintomi )  . risultati sono state completate 82 procedure per 164 sessioni ( tabella 1 )  . 
in un caso la procedura stata sospesa per impossibilit della paziente a mantenere la posizione prona in relazione ad una condizione di insufficienza respiratoria ; la paziente stata pertanto esclusa dalla successiva valutazione . 
nei restanti 27 casi sono state effettuate tutte le procedure ( 81 ) , nei tempi e nelle modalit sopradescritte . la procedura stata sempre eseguita senza complicanze in un periodo di tempo variabile da 20 a 30 minuti . 
in the remaining 27 patients , all procedures ( 81 ) were successfully completed within the timeframe and in the manner described above . all procedures were completed without complications in 2030 m infiltrations were unilateral on the symptomatic side in 26 / 27 cases and bilateral in one case . 
 minor treatment complications included a burning sensation at the injection site in 12 / 27 patients ( 44% ) , a temporary ( < 12 - h ) worsening of pain in 3 / 27 patients ( 11% ) and transient ( > 12 - h ) block of the sciatic nerve in 11 / 27 patients ( 40% )  . 
 evaluation of pain after treatment compared with perceived pain before treatment showed a significant improvement in 25 / 27 cases , with a vas ( meanstandard deviation ) of 2.120.41 , with a score of 5 in six patients ( 22% ) , a score of 4 in five ( 18% ) and a score of 3 in 14 ( 52% )  . 
 complicanze minori del trattamento sono state il bruciore a livello del sito di iniezione ( 12 / 27 pazienti , 44% ) , temporaneo ( < 12 ore ) peggioramento della sintomatologia algica ( 3 / 27 pazienti , 11% ) , blocco transitorio ( > 12 ore ) del nervo sciatico ( 11 / 27 pazienti , 40% )  . 
una dolenzia nelle sedi della infiltrazione , una volta scomparso leffetto dellanestetico , stata riscontrata in 26 casi su 27 ( 96% )  . il questionario a cui sono state sottoposte le pazienti ha fornito le seguenti valutazioni . 
a 24 ore dalla procedura in 21 su 27 casi ( 77% ) stata riferita una riduzione significativa del dolore rispetto alla baseline ( tabella 2 ) , mentre in 6 su 27 casi il dolore si ridotto in modo non significativo intensit 0 , 230 , 68 ; spasmo ( attivit 0 , 0590 , 49 ; 0 , 160 , 58 ; distress 1 , 680 , 58 )  . 
un miglioramento del 20% o pi del qol index stato riferito in 24 su 27 casi ( 88% ) rispetto al relativo follow - up ( 48% a 3 mesi ; 4% a 6 mesi ; 15% a 9 mesi ; 33% a 12 mesi ) mentre in 3 casi su 27 stato inferiore al 20% . 
 la valutazione del dolore al termine del trattamento rispetto alla percezione del dolore prima dellesecuzione del trattamento , ha riportato in 25 casi su 27 un miglioramento significativo con un vas ( mediadeviazione standard ) di 2 , 120 , 41 con score di 5 in 6 pazienti ( 22% ) , score 4 in 5 pazienti ( 18% ) e score 3 in 14 ( 52% )  . 
in 2 casi su 27 non stato riferito alcun beneficio a distanza dal trattamento eseguito ( vas 0 , 780 , 11 )  . discussione leziologia del dolore ano - perineale cronico in assenza di una identificabile causa urologica , ginecologica o proctologica frequente e di difficile individuazione . 
numerose sindromi sono state messe in causa per spiegare questo tipo di dolore , come ad esempio la coccigodinia , la proctalgia fugace o la sindrome del muscolo elevatore dellano . in assenza di imaging patognomonico , reperti laboratoristici ed elettrofisiologici , la diagnosi di nevralgia del pudendo rimane clinica . 
semplici recenti criteri utili alla identificazione clinica della nevralgia del pudendo dovuta ad intrappolamento del nervo sono i cinque criteri di nantes [ 9 ] : ( 1 ) dolore nel territorio del nervo pudendo : dallano verso il pene o il clitoride ; ( 2 ) dolore accentuato dalla posizione seduta ; ( 3 ) dolore che non risveglia il paziente di notte ; ( 4 ) sintomatologia algica in assenza di perdita di sensibilit ; ( 5 ) miglioramento del dolore dopo blocco anestetico del nervo . criteri di esclusione della neuropatia sono dolore puramente coccigeo , gluteo o ipogastrico , dolore esclusivamente parossistico , prurito , reperti di imaging che spiegano la sintomatologia . 
tuttavia la presenza di una sintomatologia radiol med ( 2009 ) 114 : 425436 discussion chronic anoperineal pain in the absence of any identifiable urological , gynaecologic or proctological cause is common and its aetiology difficult to ascertanumerous syndromes have been cited to explain this type of pain , such as coccygodynia , proctalgia fugax or levator ani syndrome . in the absence of pathognomonic imaging , laboratory and electrophysiological findings , the diagnosis of pudendal neuralgia remains clinical . 
simple criteria for the clinical demonstration of pudendal neuralgia due to nerve entrapment are the following ( nantes criteria ) [ 9 ] : ( 1 ) pain in the anatomical area supplied by the pudendal nerve ( from the anus to the penis or clitoris ) ; ( 2 ) pain worsens when patient is sitting ; ( 3 ) pain never causes the patient to wake in the night ; ( 4 ) no sensory loss is found on clinical examination ; ( 5 ) pain improves after anaesthetic nerve block . exclusion criteria for neuropathy are purely coccygeal , gluteal or hypogastric pain ; exclusively paroxysmal pain ; pruritus ; and imaging findings accounting for the symptoms . 
however , the presence of pain in the area supplied by the pudendal nerve should always arouse suspicion of pudendal neuralgia related to strain and compression . compression is more likely if the pain worsens upon sitting and is relieved upon standing or lying . 
long - term effectiveness is , however , undermined by late recurrence due to irreversible nerve damage ; incomplete release of the nerve , especially in the case of entrapment in the distal alcocks canal ; and the appearance of postsurgical perineural fibrosis . diagnostic imaging plays an important role in excluding other conditions that may simulate anoperineal pain and in providing guidance during nerve infiltration . 
 as in other entrapment syndromes , nerve infiltration at the site of compression has a dual role : diagnostic when performed with an anaesthetic , and therapeutic when performed with corticosteroids . 
treatment of pudendal neuropathy with corticosteroid and anaesthetic infiltration is not new , with pudendal nerve block via a transperineal approach having been first described by muelener in 1908 [ 14 ]  . 
pudendal nerve block with conventional fluoroscopic guidance has become popular in clinical practice owing to the easy identification of anatomical landmarks [ 18 , 19 ] , with placement of the needle tip near the apex of the iliac crest . 
nonetheless , the pudendal nerve courses in an anatomical plane formed by the sacrospinous and sacrotuberous ligament dolorosa nel territorio di innervazione del nervo pudendo deve sempre far considerare la presenza di una nevralgia dello stesso nervo , sia da allungamento sia da compressione ; la compressione pi probabile come causa del dolore quando questo peggiora con la posizione seduta mentre descresce in ortostatismo e nella posizione sdraiata . 
lefficacia a lungo termine risulta tuttavia inficiata dalla ricomparsa tardiva del dolore a causa di danneggiamento irreversibile del nervo , incompleto rilascio dello stesso soprattutto in caso entrapment a livello della parte distale del canale di alcock e dalla comparsa di fibrosi peri - neurale post - chirurgica . 
la diagnostica per immagini riveste un ruolo importante non nellaccertamento della patologia in se stessa quanto nella esclusione delle condizioni che possono simulare il dolore ano - perineale e come guida nellinfiltrazione del nervo . 
 come nelle altre sindromi da intrappolamento linfiltrazione del nervo nella sede della compressione ha un duplice effetto : diagnostico quando essa viene effettuata con anestetico e terapeutico quando vengono iniettati nella sede dei cortisonici . 
il trattamento della neuropatia del pudendo mediante infiltrazione con cortisonici ed anestetici non una terapia nuova ; il blocco del nervo pudendo con approccio transperineale stato descritto per la prima volta da muelener nel 1908 [ 14 ]  . 
 la terapia percutanea pu essere eseguita sotto guida tc [ 14 , 16 , 17 ] , fluoroscopica [ 18 ] oppure impiegando una guida elettromiografica [ 13 ]  . 
la tecnica di blocco del nervo pudendo con guida fluoroscopica convenzionale ha guadagnato popolarit nella pratica clinica per il facile riconoscimento dei reperi anatomici [ 18 , 19 ] , posizionando la punta dellago nella adiacenza dellapice della cresta iliaca . 
tuttavia il nervo pudendo decorre in un piano anatomico tra il legamento sacrospinoso e sacrotuberoso ( piano interligamentoso ) che non visualizzabile in fluoroscopia . la guida ecotomografica per il blocco percutaneo del nervo pudendo a livello della spina ischiatica una tecnica semplice e ripetibile [ 20 , 21 ]  . 
lecografia garantisce una diretta visualizzazione dei reperi anatomici in diretta contiguit con il nervo pudendo quali la spina ischiatica , larteria pudenda interna , ed i legamenti sacrospinoso e sacrotuberoso . 
us ensures direct visualisation of anatomical landmarks immediately contiguous to the pudendal nerve , such as the ischial spine , the internal pudendal artery and the sacrospinous and sacrotuberous ligaments . 
the disadvantages of us are related to the difficulty in visualising the pudendal nerve ( 12% in a recent series [ 22 ] ) , which measures 46 mm at the ischial spine [ 23 ] , the sacrotuberous ligament and the pudendal artery , which may be confused with the inferior gluteal artery , with consequent frequent sciatic nerve block . 
however , at the level of the ischial spine , in 30%40% of cases , the pudendal nerve shows anatomical variants , with two or three nerve trunks [ 7 ] covered by dense connective and / or fat tissue [ 22 ] , resulting in poor sonographic conspicuity and limited response to nerve stimulation . 
the depth of the ischial spine from the cutaneous plane is usually > 7 c this requires intraoperative fluoroscopy to confirm correct needle placement and solution delivery , with a us / fluoroscopy concordance of 82% . 
nerve stimulation ( graded electrical stimulation ) to confirm correct placement of the us - guided needle does not appear to be an absolute technique because of the size of the nerve at the level of the interligamentous space [ 24 , 25 ]  . 
 ct - guided infiltration is a problem - solving technique that ensures correct needle placement at the site of passage of the pudendal nerve close to the ischial spine and at the entrance to alcocks canal . 
 [ 19 ] reported on 200 infiltrations , with two or three injections of 5 ml of lidocaine and 1.5 ml of corticosteroids , but they failed to describe the final outcome in terms of pain relief . 
benson and griffis [ 14 ] obtained an improvement of symptoms in 31% of cases ( 12 / 38 ) by injecting 1 cc of triamcinolone and 9 cc of lidocaine and performing up to three injections 6 weeks apart . 
furthermore , they reported exacerbation of symptoms for 710 injection , which was , however , days following performed under emg guidance . the assessment of outcomes may prove difficult owing to the subjective nature of the evaluation of symptom improvement . the scale adopted in our study allows for a more systematic evaluation of the evolution of symptoms , as it distinguishes between the benefits deriving from the individual injections from the final overall benefits and includes an assessment dimensioni a livello della spina ischiatica sono di 46 mm [ 23 ] , del legamento sacrotuberoso , della arteria pudenda , facilmente confusa con la glutea inferiore con conseguente frequente blocco del nervo sciatico . 
sempre a livello della spina ischiatica , il nervo pudendo nel 30%40% dei casi presenta varianti anatomiche con 2 o 3 tronchi nervosi [ 7 ] , rivestiti da connettivo denso e / o da tessuto adiposo [ 22 ] , con conseguente ridotta visibilit ecografia del nervo nonch scarsa risposta alla stimolazione nervosa . 
la profondit della spina ischiatica dal piano cutaneo comunemente > 7 cm , con conseguente necessit intra - procedurale di ricorrere alla fluoroscopia per confermare il centraggio dellago e la somministrazione della soluzione , con una concordanza ecografia / fluoroscopia dell82% . 
la stimolazione nervosa ( stimolazione elettrica graduata ) per confermare il posizionamento dellago eco - guidato non appare una tecnica assoluta , a causa delle dimensioni del nervo a livello dello spazio interlegamentoso [ 24 , 25 ]  . liniezione perineurale pu determinare la comparsa di alterazioni enmg a breve termine , anche quando la sintomatologia dolorosa sia risolta . 
 linfiltrazione tc guidata una tecnica problem solving garantendo il corretto posizionamento dellago nella sede di passaggio del nervo pudendo in prossimit della spina ischiatica e a livello dellingresso nel canale di alcock . 
 [ 19 ] eseguendo 2 o 3 iniezioni di 5 ml di lidocaina e di 1 , 5 ml di cortisonico riporta una casistica di 200 infiltrazioni , ma non specifica il risultato finale delle stesse riguardo il sollievo dalla sintomatologia . 
 [ 16 ] riporta su di una casistica di 36 pazienti un miglioramento della sintomatologia nei 3 / 4 dei casi ; la sua tecnica consiste in 5 infiltrazioni ripetute a distanza di 30 giorni luna dallaltra . 
benson e griffis [ 14 ] riferisce un miglioramento dei sintomi nel 31% dei casi ( 12 / 38 ) iniettando 1 cc di triamcinolone e 9 cc di lidocaina ed eseguendo un massimo di 3 iniezioni a distanza di 6 settimane ; inoltre riporta unesacerbazione dei sintomi per i successivi 710 giorni a seguito delliniezione , eseguita per sotto guida emg e non mediante imaging . la valutazione dei risultati appare senza dubbio difficile , essendo molto soggettiva la valutazione del miglioramento sintomatologico . 
la scala da noi adottata permette una valutazione pi sistematica dellevoluzione dei sintomi , distinguendo il beneficio di ciascuna iniezione da quello finale complessivo e valutando anche la capacit del soggetto di svolgere normalmente la sua attivit quotidiana . in tutte le casistiche riportate non sono mai riferiti insuccessi tecnici della procedura ; nelliniezione in corrispondenza della spina ischiatica occorre tuttavia prestare attenzione a non spostare lago troppo lateralmente , pena una radiol med ( 2009 ) 114 : 425436 of the subjects ability to carry out daily activities . none of the previous series reported on any technical failures . 
however , with regard to injections at the ischial spine level , it is important to avoid moving the needle too laterally so as not to cause sciatic nerve block . 
secondary complications include haematoma at the injection site , pain worsening for a few days and transient nerve blocks lasting hours . as shown in our experience , perineural injection of the pudendal nerve is to be considered a safe procedure that is free of significant complications . 
in the case of suspected pudendal nerve entrapment syndromes , we believe that ctguided infiltration of impingement sites can and should be performed , partly in consideration of the fact that other approaches conservative therapy , decompressive surgery and neuromodulation [ 13 ] fail to provide consistent and long - lasting results . conseguente analgesia del nervo sciatico . 
le complicanze secondarie possono lematoma nella sede includere delliniezione , il peggioramento del dolore della durata di alcuni giorni ed il blocco transitorio del nervo per alcune ore . i risultati da noi presentati sono indicativi comunque della efficacia terapeutica e della mancanza di complicanze . 
giacomo , unit operativa di radiodiagnostica , monopoli , bari , italy 3universit degli studi di catania , cattedra di radiodiagnostica , azienda policlinico di catania gaspare rodolico , catania , italy correspondence to : p . 
chieffi 40 , 70051 barletta , italy , tel . : + - 39 - 340 - 0781993 , fax : + 39 - 088 - 1733866 , e - mail : paomi03@libero.it received : 11 october 2008 / accepted : 5 march 2009 / published online : 9 november 2009 springer - verlag 2009 abstract purpose . 
of these 31 patients , we included in the study 22 patients ( mean age 53 years ; range 4657 years ) who underwent liver transplantation within 1224 h after mr examination . 
dei 31 pazienti selezionati per il trapianto dorgano , sono stati inclusi nello studio 22 pazienti , di et media di 53 anni ( range 4657 anni ) , sottoposti a trapianto di fegato a distanza di circa 1224 ore dallesecuzione dellesame rm . i pazienti inclusi nello studio sono stati sottoposti ad esame rm con un apparecchio da 1 , 5 t . 
unenhanced baseline mr imaging correctly identified and characterised 20 lesions , equal to 33.90% of all lesions : 6 hcc , 12 dn and 2 dn with a subfocus of hcc . 
spio - enhanced mr imaging showed greater sensitivity detecting and characterising 45 lesions , equal to 76.27% of all lesions identified at histology : 14 hcc , 27 dn and 4 dn with subfocus of hcc . 
spio - enhanced mr imaging proved to be of value in detecting and characterising lesions in the cirrhotic liver , allowing differentiation of dn from hcc and providing an early diagnosis of neoplastic degeneration of dn . keywords spio dysplastic nodules hepatocellular carcinoma magnetic resonance imaging 14 hcc , 3 sono risultati ben differenziati , 8 moderatamente differenziati , 3 scarsamente differenziati . dei 39 nd , 28 erano a basso grado di malignit e 11 ad alto grado di malignit . 
con lesame rm di base abbiamo identificato e caratterizzato correttamente 20 lesioni , pari al 33 , 90% delle lesioni complessivamente individuate , di cui 6 hcc , 12 nd e 2 nd con foci di hcc . 
lesame rm , eseguito dopo somministrazione di mdc spio , ha mostrato una maggiore sensibilit identificando e caratterizzando complessivamente 45 lesioni , pari al 76 , 27% delle lesioni totali individuate con lesame istologico : 14 hcc , 27 nd e 4 nd con foci di hcc . 
i falsi negativi con la rm - spio sono stati 12 noduli displasici , pari al 31% , che allesame istologico sono risultati essere nd a basso grado di malignit e con diametro inferiore al c conclusioni . 
la rm con utilizzo di mdc spio , nella nostra esperienza risultata utile nella identificazione e caratterizzazione delle lesioni epatiche nel fegato cirrotico mostrandosi in grado di differenziare i noduli displasici dagli hcc e ha consentito una diagnosi precoce della trasformazione carcinomatosa dei noduli displasici . parole chiave spio noduli displasici carcinoma epatocellulare risonanza magnetica introduction introduzione cirrhosis is a progressive , diffuse disease of the liver characterised by hepatocyte necrosis , fibrosis , distortion of the normal hepatic architecture and a spectrum of nodular lesions that includes regenerative nodules ( rn ) , dysplastic nodules ( dn ) and hepatocellular carcinomas ( hcc ) [ 1 ]  . 
in italy , the likelihood of developing hcc secondary to cirrhosis ranges from 2% to 5% [ 3 ]  . in recent decades , the survival of hcc patients has been significantly increased by improvements and refinements in both nonsurgical treatments , such as percutaneous ethanol injection ( pei ) , thermoablation and lipiodol computed tomography ( ct ) ; and surgical treatments , such as liver resection and transplantation . 
the results of these treatments are , however , heavily dependent on accurate disease staging , so that the early diagnosis of hcc and its precursor , the dn , is mandatory [ 4 , 5 ]  . the screening protocol for high - risk cirrhotic patients entails ( ultrasonographic ) imaging and alpha - fetoprotein testing at 3to 6 - month intervals . 
unfortunately , an la cirrosi un progressivo e diffuso processo patologico del fegato caratterizzato da necrosi epatocitaria , fibrosi , sovvertimento della normale architettura epatica e dalla presenza di uno spettro di lesioni nodulari che include noduli di rigenerazione ( nr ) , noduli displasici ( nd ) ed epatocarcinomi ( hcc ) [ 1 ]  . 
in italia la probabilit annuale di sviluppare hcc su cirrosi epatica varia dal 2% al 5% [ 3 ]  . negli ultimi decenni si verificato un significativo incremento della sopravvivenza dei pazienti affetti da tale patologia per il miglioramento e laffinamento sia delle terapie che si basano sui trattamenti locali , come liniezione percutanea di etanolo ( pei ) , la termoablazione e la lipiodoltomografia computerizzata , sia di quelle che si basano invece su tecniche chirurgiche , quali la resezione o il trapianto . 
i risultati di queste terapie sono tuttavia fortemente condizionati dallo staging della malattia ed , quindi , estremamente importante effettuare una diagnosi precoce ed accurata dellhcc e del suo precursore , il nd [ 4 , 5 ]  . il protocollo di screening , nei pazienti cirrotici ad radiol med ( 2009 ) 114 : 12671282 1269 elevation of alpha - fetoprotein levels is neither sensitive nor specific enough to be used to screen for hcc . 
this test may , in fact , fail to detect small tumours ( < 2 cm ) , and high alpha - fetoprotein levels are seen in only 50% of patients with hcc and 26% of those with dn [ 6 , 7 ]  . imaging techniques therefore play a primary role in the diagnosis of focal lesions in the cirrhotic liver , even though there is no general agreement as to the most appropriate modality for the study of this disease . 
the literature reports conflicting data regarding not only the diagnostic capabilities of the different imaging modalities ultrasonographic ( us ) , ct and magnetic resonance ( mr ) imaging in the detection and characterisation of hcc and dn , but also the possibility of arriving at a differential diagnosis among the different lesions . 
histological analysis of the entire cirrhotic liver and a short interval between mr imaging and transplantation are factors that , if neglected , may lead to considerable variability among results . 
indeed , a long interval between mr examination and transplantation could mean the transformation of a dn into an hcc , whereas a histological examination limited to biopsies or specimens from partial liver resection could preclude identification of other nodular lesions in the liver parenchyma [ 812 ]  . in recent years , investigators have emphasised the value of hepatospecific superparamagnetic contrast agents based on iron oxide particles ( spio ) in the detection and characterisation of focal lesions with mr imaging , and their use has been advocated for staging patients scheduled for surgical or locoregional treatment of malignant focal hepatic lesions [ 13 , 14 ] and for monitoring patients with cirrhosis [ 1517 ]  . the rationale for using spio contrast agents to differentiate among the wide range of nodular lesions seen in cirrhosis is not based on vascular changes but on the cellular changes rn undergo as they develop into dn and then into hcc . 
in fact , during this process , the number and function of kupffer cells , the cells that accumulate spio , decrease [ 10 , 1820 ] , and some investigators have reported that hcc and dn show different enhancement patterns after spio administration . 
dn , on the other hand , have preserved cellular composition and function and hence greater spio accumulation , with the result that they appear markedly hypointense even relative to the surrounding liver . 
these different enhancement patterns led researchers to hypothesise that it was possible to differentiate between these two lesions and identify the transformation of a dn into an hcc at an early stage . the aim of this study was to evaluate the potential of spio - mr imaging in the detection and characterisation of elevato rischio , prevede lesecuzione di esame ecografico e dei dosaggi dellalfa - fetoproteina ( afp ) ad intervalli di 36 mesi . 
tale test , infatti , non sempre in grado di rilevare piccoli tumori ( < 2 cm ) ed elevati livelli di afp sono presenti solo nel 50% di pazienti con hcc e nel 26% di pazienti con nd [ 6 , 7 ]  . le tecniche dimaging svolgono pertanto un ruolo fondamentale nella diagnostica delle lesioni focali nella cirrosi epatica ; tuttavia non vi uniformit di vedute su quale sia la metodica pi idonea per lo studio di tale patologia . 
in letteratura sono piuttosto controversi i dati circa le reali potenzialit diagnostiche delle diverse tecniche dimaging ecografia ( us ) , tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) nella identificazione e nella caratterizzazione degli hcc e dei nd , nonch riguardo la possibilit di effettuare una diagnosi differenziale tra le diverse lesioni . questo si verifica per mancanza , in tutti i lavori finora pubblicati , di uniformit dei parametri di valutazione attendibili ; infatti , lanalisi istologica di tutto il fegato cirrotico ed il breve timing tra lesecuzione dellesame rm e il trapianto sono fattori che se non presi in considerazione possono portare una notevole variabilit nei risultati . 
infatti , un lungo tempo intercorso tra lesame rm e lesecuzione del trapianto potrebbe portare alla trasformazione di un nd in hcc , mentre uno studio anatomo - patologico limitato alle sole lesioni sottoposte a biopsia o a resezione parziale dellorgano potrebbe escludere lidentificazione di altre lesioni nodulari nel restante parenchima epatico [ 812 ]  . negli ultimi anni stata sottolineata lutilit dei mezzi di contrasto ( mdc ) superparamagnetici epatospecifici , a base di particelle di ossido di ferro ( spio ) , per lidentificazione e la caratterizzazione delle lesioni focali epatiche con rm ed il loro uso stato proposto per lo staging di pazienti da sottoporre a trattamenti chirurgici o loco - regionali per lesioni focali epatiche maligne [ 13 , 14 ] e nel follow - up dei pazienti portatori di cirrosi epatica [ 1517 ]  . il razionale di impiego dei mdc spio per la diagnosi differenziale tra il vasto spettro di lesioni nodulari presenti nella cirrosi epatica , si basa , pi che sulle modificazioni vascolari , sulle alterazioni cellulari che i nr subiscono nella loro trasformazione in nd prima e in hcc poi ; infatti , in rapporto a tale evoluzione , decrescono progressivamente il numero e la funzionalit delle cellule del kupffer , deputate alla captazione del mdc spio [ 10 , 1820 ]  . 
in relazione a tali riscontri , alcuni autori hanno rilevato un differente comportamento contrastografico con i mdc spio tra gli hcc e i nd , in quanto i primi , a causa delle alterazioni cellulari subite , non presenterebbero captazione di mdc spio , risultando marcatamente iperintensi rispetto al parenchima epatico contiguo ; i nd invece , preservando composizione e funzionalit cellulari , presenterebbero una maggiore captazione di mdc spio , apparendo francamente ipointensi anche rispetto al fegato sano limitrofo . 
tali comportamenti contrastografici hanno indotto a considerare 1270 radiol med ( 2009 ) 114 : 12671282 dn and hcc in the cirrhotic liver by correlating the findings on mr imaging performed 1224 h before liver transplantation with histopathology of the entire explanted liver . materials and methods in the setting of a screening programme for cirrhotic patients awaiting liver transplantation , we performed mr studies on 400 patients , 31 of whom had been selected for transplantation . 
prior to the mr examination , all patients received full explanation of the aims and design of the study and gave their informed consent . all patients were studied with a 1.5 - tesla unit ( magnetom 63p , siemens , germany ) using baseline proton density ( pd ) / t2 - weighted spin echo ( se ) sequences ( tr / te 2 , 0002 , 300 / 2080 ms ) , and t1 - weighted fast low - angle shot ( flash ) gradient echo ( ge ) sequences ( tr / flip angle / te 153 ms / 70 / 6 ms ) and t2 * - weighted fast imaging with steady - state precession ( fisp ) ge sequences ( tr / flip angle / te 130 ms / 40 / 10 ms )  . 
for the pd / t2weighted sequences obtained under free breathing , two acquisition and presaturation bands were positioned above and below the imaging volume so as to reduce flow artefacts . 
the t1weighted ge sequences provided a stack of 15 slices that was sufficient to study the entire liver in most patients . with the t2 * - weighted ge sequences , a stack of five slices was used so that three to four stacks were required to study the entire liver . 
in all sequences , we used a slice thickness of 8 mm with 1 - mm gap , 128256 matrix with 3 / 4 reconstruction algorithm , and 380to 450 - mm field of view . 
 following unenhanced baseline imaging , spio ( ferumoxide , endorem , guerbet , villepinte , france ) was administered by slow infusion ( 820 drops / min ) over 3045 min at a dose of 23.6 md iron per gram ( fe / g ) diluted in a 100cc flask of 5% glucose solution . 
approximately 30 - 60 min after the end of spio administration , t2 * - weighted ge sequences with the same parameters as used at baseline were obtained in all patients . the baseline and spio - enhanced images were evaluated singly and then in combination by observers blinded to the histopathological results who recorded the number and site of lesions and expressed their judgement as to the dysplastic , neoplastic or other nature of the lesions . 
for each nodule , the observers recorded signal intensity on t1and t2 - weighted images and enhancement pattern after spio administration and , based on these parameters , expressed a la possibilit di una diagnosi differenziale tra queste due lesioni , nonch di una precoce identificazione della trasformazione del nd in hcc . scopo del nostro lavoro stato quello di valutare le possibilit della rm con mdc spio nella identificazione , caratterizzazione di nd e hcc nel fegato cirrotico , confrontando i risultati della rm , eseguita nelle 1224 ore precedenti il trapianto di fegato , con lesame anatomopatologico dellintero fegato espiantato . materiali e metodi nellambito di un programma di screening di pazienti cirrotici in lista dattesa di trapianto epatico , abbiamo studiato con rm 400 pazienti , 31 dei quali sono stati selezionati in seguito al reperimento di un fegato da trapiantare e di questi solo 22 sono stati inclusi nello studio , in quanto sottoposti a trapianto di fegato a distanza di circa 1224 ore dallesecuzione dellesame rm . 
per le sequenze se dpt2w ottenute durante la respirazione libera del paziente , abbiamo utilizzato due acquisizioni e bande di pre - saturazione , al di sopra ed al di sotto del campo di studio , al fine di ridurre gli artefatti vascolari . le sequenze ge t1w e ge t2 w sono state eseguite durante lapnea respiratoria dei pazienti , con ununica acquisizione e senza bande di pre - saturazione . 
in tutte le sequenze stato utilizzato spessore di strato di 8 mm con un gap di 1 mm , matrice di 128256 con algoritmo di ricostruzione 3 / 4 , campo di vista ( fov ) di 380450 mm . dopo le sequenze di base stato somministrato mdc spio ( ferumoxide , endorem , guerbert , francia ) , in infusione lenta ( 820 gocce / min ) alla dose di 23 , 6 micromol fe / g , diluito in un flacone da 100 cc di soluzione glucosata al 5% , con un tempo di infusione di circa 3045 mdopo circa 3060 min dalla fine della somministrazione del mdc spio in tutti i pazienti sono state ripetute le sequenze ge t2 * w con gli stessi parametri utilizzati nelle sequenze di base , eseguite prima dellinfusione del mdc spio . le immagini di base e quelle dopo spio sono state valutate separatamente e comparativamente , alloscuro dei radiol med ( 2009 ) 114 : 12671282 1271 diagnostic hypothesis as to histological type . 
on baseline images , in agreement with the reported mr criteria ( table 1 ) , dn were defined as nodular lesions that appeared hyperintense on t1 - weighted images and hypointense on t2weighted images or isohyperintense on t1 - weighted images and isointense on t2 - weighted images . 
hcc were defined as lesions appearing isohyperintense on t1 - weighted images , hyperintense in t2 or hyperintense in t1 , and isointense in t2 or hypointense in t1 , and hyperintense in t2 . hcc subfoci in dn ( nodule - in - nodule ) were defined as nodular areas of heterogeneous signal intensity seen within a dn with typical signal intensity . on spio - enhanced images , the diagnosis was based on the pattern of spio uptake . 
dn were defined as nodules presenting variable uptake depending on the degree of dysplasia , appearing in some cases strongly hypointense , often even more hypointense than the surrounding liver . hcc were defined as nodules with no spio uptake and hence markedly hyperintense . 
hcc subfoci in dn were defined as nodular lesions with hyperintense appearance due to failure to accumulate spio in the context of a larger , hypointense dn due to spio uptake . 
the definitive diagnosis was reached with the histopathological examination performed within 1 week of surgery on the entire explanted liver . dn were classified according to the international working party terminology of hepatic lesions into : lowgrade dn , high - grade dn and dn containing a subfocus of hcc [ 21 ]  . 
hcc were classified based on histology into well differentiated , moderately differentiated and poorly risultati dellanatomia patologica , riportando il numero e la sede delle lesioni ed esprimendosi sulla natura displasica , neoplastica o di altro tipo delle lesioni stesse . 
per ogni nodulo stata indicata lintensit di segnale nelle sequenze di base pesate in t1 e in t2 , il comportamento dopo somministrazione di mdc spio e , in base a tali parametri , si avanzata una ipotesi diagnostica sul tipo istologico . 
nelle sequenze di base , in accordo con la semeiotica rm descritta in letteratura ( tabella 1 ) abbiamo considerato nd le lesioni nodulari che apparivano iperintense in t1w ed ipointense in t2w o iso - / iperintense in t1w e isointense in t2w ; hcc le lesioni che apparivano iso - / iperintense in t1w e iperintense in t2w o iperintense in t1w e isointense in t2w o ipointense in t1w ed iperintense in t2w ; foci di hcc in nd ( nodulonel - nodulo ) le aree nodulari di disomogenea intensit di segnale riscontrate allinterno di un nodulo displasico con le caratteristiche intensit di segnale descritte . dopo iniezione di mdc spio , la diagnosi si basata sul tipo di captazione dello stesso e sono stati considerati nd i noduli che presentavano una captazione di mdc variabile in relazione al grado di displasia , apparendo in alcuni casi fortemente ipointensi , spesso anche in maggior grado rispetto al parenchima epatico limitrofo . 
lidentificazione di foci di hcc in nd si invece basata sul riscontro , dopo mdc spio , di una lesione nodulare iperintensa per mancata captazione di mdc nel contesto di un nodulo displasico di maggiori dimensioni , ipointenso per lup - take di mdc . 
nine patients were excluded because of mr or clinicallaboratory evidence of abnormalities that constituted contraindications or indications to defer surgery , findings later confirmed by clinical - imaging follow - up and biopsy . 
three of these nine patients had suspicious focal liver lesions that were > 5 cm and involved both hepatic lobes ; another two patients had cancercirrhosis , with extensive involvement of the right lobe in one case and left lobe in the other . 
in one patient , mr imaging demonstrated a large confluent fibrosis that made it impossible to confidently rule out the presence of cancer - cirrhosis , which was later excluded by biopsy . 
 risultati i risultati del nostro studio sono riportati nella tabella 2 . dei 31 pazienti selezionati per il trapianto dorgano , sono stati inclusi nello studio 22 pazienti , sottoposti a trapianto fegato a distanza di 1224 ore dallesecuzione dellesame rm . 
nove pazienti sono stati eliminati dallo studio in quanto allesame rm e agli esami clinico - laboratoristici presentavano alterazioni che contravvenivano o consigliavano il posticipo dellesecuzione del trapianto , reperti poi supportati dal follow - up clinico - radiologico e dallesame bioptico . 
in 3 , di questi 9 casi , erano presenti lesioni focali epatiche sospette per hcc che avevano dimensioni complessivamente superiori a 5 cm ed interessavano entrambi i lobi epatici ; in altri 2 casi si trattava di cancro - cirrosi con esteso interessamento del lobo destro in un caso e del sinistro nellaltro ; in 1 caso il paziente era portatore di tips che si estendeva nellatrio destro e per il quale si preferito posticipare lintervento ai fini di una migliore pianificazione chirurgica ; in 1 caso la rm evidenziava una estesa fibrosi confluente che non consentiva di escludere con certezza una eventuale cancro - cirrosi , successivamente non confermata dallesame bioptico ; in 2 casi le scadenti condizioni cliniche dei pazienti hanno imposto di soprassedere al trapianto e di proseguire la terapia medica . 
sono stati quindi inclusi nel nostro studio 22 pazienti , di et media di 53 anni ( range 4657 anni ) , successivamente sottoposti a trapianto dorgano entro 1224 ore dallesecuzione dellesame rm . la cirrosi stata classificata utilizzando il child - pugh syste quindici erano pazienti con cirrosi child - pugh classe a , 7 con cirrosi child - pugh classe b . 
unidici avevano cirrosi correlata con il virus dellepatite b ( hbv ) , 7 cirrosi correlata con il virus dellepatite c ( hcv ) , 4 cirrosi alcool correlata . risultati anatomo - patologici lesame anatomo - patologico dei 22 fegati espiantati ha dimostrato in tutti i casi un aspetto di tipo nodulare : macronodulare in 9 casi , micronodulare in 3 casi e medio - macronodulare in 10 casi . 
sono state identificate , inoltre , 59 lesioni focali epatiche , di cui 14 hcc , 4 noduli displasici con allinterno foci di hcc , 39 noduli displasici e 2 radiol med ( 2009 ) 114 : 12671282 1273 seven were child - pugh class b . 
at baseline mr imaging , four of the 12 dn exhibited the typical pattern of t1 hyperintensity relative to liver and t2 hypointensity ; eight dn were isointense on t1and t2weighted images . 
the two hcc subfoci within dn showed the classic nodule - in - nodule appearance , with isohyperintense signal on t1 - weighted images and heterogeneous hyperintensity on t2 - weighted images , contained within a larger dn that appeared isointense on t1weighted images and isohypointense on t2 - weighted images . 
the signal characteristics of the remaining 39 undetected lesions were such that precise identification and characterisation was precluded . spio administration increased mri sensitivity by 42.37% relative to the baseline study . 
il diametro medio delle lesioni stato per gli hcc 1 , 7 cm ( range 12 , 5 cm ) , per noduli displasici 0 , 8 cm ( range 0 , 52 ) , per i noduli displasici con allinterno foci di hcc 2 , 1 cm ( range 0 , 82 , 8 ) e per i cistoadenomi 1 , 2 cm ( range 11 , 4 )  . risultati rm gli esami rm effettuati senza mdc ( rm di base ) e con ferumoxide hanno mostrato una differente sensibilit nellidentificazione delle lesioni focali epatiche . 
lesame rm di base ha consentito di diagnosticare correttamente 20 lesioni , pari al 33 , 90% di quelle identificate con lesame anatomopatologico , di cui , allesame anatomopatologico , 12 sono risultate nd e 8 hcc . 
nelle sequenze di base , dei 12 nd identificati , 4 hanno mostrato comportamento caratteristico con intensit di segnale aumentata rispetto al parenchima epatico circostante nelle immagini t1w e ridotta in quelle t2w ; 8 nd sono risultati isointensi in t1w e isointensi in t2w . 
per quanto riguarda gli hcc , allesame di base in 3 casi hanno mostrato iperintensit di segnale nelle sequenze t1w ; in 2 casi isointensit di segnale ed in 1 caso ipointensit di segnale . 
i due foci di hcc in nodulo displasico hanno presentato il classico aspetto rm di nodulo - nel - nodulo mostrando segnale iper - / isointenso nelle sequenze t1w , e disomogeneamente iperintenso nelle sequenze t2w allinterno di un nodulo displasico di pi grandi dimensioni isointenso nelle sequenze t1w ed iso / ipointenso nelle sequenze t2w . 
le rimanenti 39 lesioni non diagnosticate presentavano caratteristiche di segnale tali da non consentire una precisa identificazione ed una adeguata caratterizzazione . dopo somministrazione di mdc spio , la rm ha mostrato una maggiore sensibilit diagnosticando complessivamente 45 lesioni , pari al 76 , 27% delle lesioni totali individuate con lesame istologico , di cui , allesame anatomo - patologico , 27 sono risultate nd e 18 hcc , con un incremento del 42 , 37% rispetto alle sequenze rm di base . 
i falsi negativi con la rm - spio sono stati 12 noduli displasici , pari al 31% , che allesame istologico sono risultati essere nd a basso grado di malignit e con diametro inferiore al centimetro . 
due lesioni , caratterizzate istologicamente come cistoadenomi , non sono state identificate in prima istanza allesame rm di base n dopo mdc spio , ma solo valutando retrospettivamente le immagini , sulla scorta dei risultati dellesame istologico . 
baseline protondensity - weighted spin echo ( a ) , t2 - weighted spin echo ( b ) , fisp ( c ) and t1 - weighted flash ( d ) magnetic resonance ( mr ) sequences : the nodule seems slightly hyperintense in all baseline sequences ( a - d )  . 
il reperto anatomo - patologico corrispondente conferma la presenza di multipli e diffusi noduli di rigenerazione con nodulo di hcc bianco - verdastro ( f )  . radiol med ( 2009 ) 114 : 12671282 1275 fig . 
3a - c nodulo di hcc e nodulo displasico con focus di hcc allviii segmento epatico . rm di base , sequenza flash t1w ( a ) e fisp t2w ( b ) : sono ben evidenti due formazioni nodulari iperintense . 
il nodulo di minori dimensioni mostra , nella sequenza fisp t2w , disomogenea intensit di segnale con evidenza di piccolo nodulo centrale contestuale . tale reperto configura il tipico pattern di nodulo - nel - nodulo . 
il reperto anatomopatologico ( c ) dimostra il caratteristico aspetto di nodulo nel nodulo della lesione . in 12 dn , equal to 31% , which at histology proved to be low - grade dn < 1 cm in diameter . 
two lesions that were histologically characterised as cystoadenomas went unrecognised on initial viewing of the baseline and spio - enhanced mr images but were later identified on retrospective review after the results of the histological examination . 
in fact , according to several authors , the transition from a dn to an hcc occurs over a period of mancata identificazione stata probabilmente dovuta alle ridotte dimensioni , alla localizzazione in sede sottoglissoniana e allaspetto simil - cistico . 
infatti lo sviluppo di un hcc a partire da un nd avviene , secondo molti autori , in un tempo variabile di circa 46 mesi [ 12 , 23 ] e laspettativa di vita media in un paziente non trattato di soli 13 mesi , con una sopravvivenza a 2 anni inferiore al 33% [ 24 ]  . 
il reperto anatomo - patologico ( d ) ha dimostrato la presenza di area di fibrosi e lassenza di lesioni focali . approximately 46 months [ 12 , 23 ] , and mean life expectancy of untreated patients is only 13 months , with a 2 - year survival rate < 33% [ 24 ]  . 
this pathogenic theory is supported by other studies and confirmed by the international working party on terminology of hepatocellular lesions , which stated that carcinogenesis in the cirrhotic liver is a multistep process that involves a transition from large rn to lowand high - grade dn to dn with subfocus of hcc and eventually to hcc [ 21 ]  . identification of dn and hcc in the cirrhotic liver is difficult because of the marked architectural distortion of the parenchyma due to areas of fibrosis , steatosis , parenchymal necrosis and regenerative nodules [ 10 , 25 , 26 ]  . 
found that us had a sensitivity of 20.5% for the detection of hcc and of 1.6% for detection of dn , emphasising the difficulty in differentiating hcc and dn with us , as both manifest as hypoechoic nodular lesions [ 8 ]  . 
although the use of sonographic contrast agents has improved the techniques epatiche , in cui si affermato che la carcinogenesi nel fegato cirrotico avviene con un meccanismo multi - step che include la transizione da grossi noduli rigenerativi a noduli displasici a basso ed alto grado di malignit , quindi a noduli displasici con foci di hcc sino agli hcc [ 21 ]  . lidentificazione di nd e di hcc nel fegato cirrotico per difficoltosa per la notevole alterazione strutturale del parenchima epatico a causa della presenza di aree di fibrosi , steatosi , necrosi parenchimale e noduli di rigenerazione [ 10 , 25 , 26 ]  . 
 [ 8 ] , in uno studio su 200 pazienti con cirrosi , hanno rilevato una sensibilit dellecografia nella identificazione degli hcc del 20 , 5% e dei nd del 1 , 6% , sottolineando la difficolt di differenziare con lecografia gli hcc dai nd , poich entrambi apparivano come lesioni nodulari ipoecogene [ 8 ]  . 
lutilizzo dei mezzi di contrasto ecografici ha migliorato laccuratezza diagnostica nella identificazione di hcc e nd rispetto alla ecografia convenzionale ; tuttavia esistono ancora difficolt nella diagnosi differenziale tra le due lesioni con tale metodica [ 27 ]  . 1278 radiol med ( 2009 ) 114 : 12671282 accuracy in identifying hcc and dn , the difficulties in differentiating the two lesions with this modality remain [ 27 ]  . spiral ct is currently considered amongst the most reliable modalities for detecting hcc . 
reported a mean sensitivity of dynamic spiral ct in identifying hcc of 76% and mean sensitivity values of 39% in the detection of dn depending on lesion size [ 10 ]  . the lower sensitivity in dn detection is most likely due to the fact that some dn are hypoattenuating in the portal venous and delayed phases , and few dn show hyperattenuation in the hepatic arterial phase . 
in the early stages of carcinogenesis , this is similar to that of healthy liver parenchyma , whereas in the subsequent hcc stage , it is characterised by a predominance of abnormal arteries ( not accompanied by bile ducts and for this reason known as unpaired or nonportal arteries ) and arteriovenous shunts livers undergoing neoplastic degeneration [ 19 , 20 , 29 ]  . 
thus , the arterial and portal supply to lowand high - grade dn is variable and inconsistent , making difficult the detection and characterisation of dn on the basis of their vascular characteristics alone [ 10 ]  . 
 typical of cirrhotic unlike ct , mr imaging often proves capable of differentiating hcc from dn based on signal characteristics alone as a result of its multiparametric properties and highcontrast resolution [ 23 ]  . 
on unenhanced baseline mr imaging , dn normally have isohyperintense signal on t1weigthed images in relation to their glycoprotein content and degree of dysplasia ; the signal becomes hypointense to surrounding parenchyma on t2 - weighted images . 
unfortunately , however , the signal intensity of dn may be identical to that of well - differentiated hcc , especially of small hcc ( < 2cm )  . the signal intensity of hcc on unenhanced t1weighted mr images varies widely and hcc may appear as hypointense masses as a result of greater water content or fibrous tissue or poor cellular differentiation or alternatively as hyperintense due to steatosis , accumulation of glycoproteic material or areas of intralesional haemorrhage . in some cases , however , moderately and well - differentiated hcc may also appear isointense compared with the healthy hepatic parenchyma . 
conversely , on t2 - weighted images , hcc tend to appear as generally ill - defined and hyperintense lesions [ 12 , 30 ] with the exception of well - differentiated hcc , which are isointense relative to the healthy parenchyma . 
in letteratura riportato che la sensibilit della tc multifasica nella identificazione di hcc di diametro superiore a 2 cm del 93 , 6% , percentuale che si riduce al 61% nella valutazione di lesioni di minori dimensioni [ 28 ]  . 
 [ 10 ] hanno riportato una sensibilit media della tc spirale dinamica nellidentificazione dellhcc del 76% e valori medi di sensibilit del 39% nellidentificazione dei nd in relazione alle dimensioni delle lesioni [ 10 ]  . 
questi minori valori di sensibilit nella identificazione dei nd sono verosimilmente dovuti al fatto che solo alcuni nd sono ipodensi in fase venosa portale e in fase tardiva , cos come sono pochi i nd che mostrano iperdensit nella fase arteriosa epatica . 
questo fenomeno correlato al tipo di apporto ematico arterioso e venoso che , nelle prime fasi della carcinogenesi , simile a quello del tessuto epatico sano ; successivamente , nello stadio di hcc , prevalgono vasi arteriosi anomali , non accompagnati dai canalicoli biliari , e per tale motivo denominati unpaired o non portal arteries , e shunt artero - venosi tipici dei fegati cirrotici ed in degenerazione neoplastica [ 19 , 20 , 29 ]  . 
pertanto lapporto arterioso e portale ai nd a basso ed alto grado di malignit variabile ed incostante ; , dunque , difficile identificare e caratterizzare i noduli displasici soltanto sulla base delle caratteristiche vascolari [ 10 ]  . la rm , grazie alle sue intrinseche multiparametricit ed alta risoluzione di contrasto , rispetto alla tc si rivela spesso in grado , di differenziare gli hcc dai nd sulla base delle sole caratteristiche di segnale [ 23 ]  . 
nelle immagini rm di base , il nd presenta solitamente , nelle sequenze t1w , un segnale che , in relazione al contenuto glicoproteico ed al grado di displasia , pu essere iso - / iperintenso ; appare invece iso - / ipointenso rispetto al parenchima circostante nelle sequenze t2w . 
purtroppo per lintensit di segnale dei nd pu essere sovrapponibile a quella degli hcc ben differenziati , soprattutto se di piccole dimensioni ( hcc < 2 cm )  . le caratteristiche di segnale degli hcc nelle immagini rm di base t1w variano molto e possono apparire come formazioni ipointense , per il maggior contenuto di acqua o per la componente di tessuto fibroso e per la scarsa differenziazione cellulare ; o possono presentare elevata intensit di segnale per la presenza di steatosi , accumulo di materiale glicoproteico o aree di emorragia intratumorale . 
nelle immagini t2w , invece , gli hcc appaiono comunemente come lesioni non sempre ben definite , iperintense rispetto al parenchima circostante [ 12 , 30 ] ad eccezione degli hcc ben differenziati che mostrano isointensit di segnale rispetto al parenchima sano . la capacit di identificare e caratterizzare le lesioni nodulari nel fegato cirrotico aumenta con lausilio dei mdc siano essi paramagnetici o superparamagnetici . 
la rm con mdc paramagnetico sfrutta , come la tc , le caratteristiche vascolari delle lesioni focali epatiche sia per la loro radiol med ( 2009 ) 114 : 12671282 1279 imaging with paramagnetic contrast medium relies on the vascular characteristics of focal liver lesions for their detection and characterisation . 
gadolinium has shown a good level of accuracy , even in the study of small hcc ( < 1.52 cm ) and in cirrhotic livers , with a sensitivity of 84% [ 11 , 31 , 32 ]  . 
sensitivity in the detection of dn is instead only 15% , with low specificity values since the signal intensity of dn on mr imaging with paramagnetic contrast medium is very similar to that of many hcc [ 33 ]  . the introduction of spio contrast agents , which provide information about the composition and function of cells forming the nodular lesions and which overcome the limitations of relying on vascularisation changes , has made it possible to detect even small hcc , which in the early stage may preserve normal vascularity and thus be difficult to differentiate from other nodular lesions [ 34 , 35 ]  . 
 the mechanism of action of spio contrast agents is based on their uptake by kupffer cells or cells of the hepatic reticuloendothelial syste spio uptake is reflected in a marked reduction in signal intensity of the tissues containing kupffer cells . 
conversely , any malignant lesions , which do not contain reticuloendothelial cells , do not accumulate the contrast medium and therefore appear as areas of hyperintensity [ 36 , 37 ]  . 
the use of these contrast agents has in part solved the problem of false positive results seen with paramagnetic contrast agents injected as a bolus , a problem related to the presence of small arteriovenous shunts which , appearing as small areas of vascular enhancement during the arterial phase , may mimic the enhancement pattern of small hcc . 
these false positive results are similar to those seen during contrast - enhanced dynamic ct imaging . on this subject , the literature also contains studies on the combined use of gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa ) and spio , which , by fulfilling the criteria of vascularity as well as cellular composition and function [ 11 , 38 ] , reduces both the false positive results of paramagnetic contrast agents and the false negative results of spio agents the latter related to the presence , in moderately and well - differentiated hcc , of functioning kupffer cells that accumulate the contrast agent . 
as a result , the t2 - weighted signal intensity is higher in low - grade tumours , in which the number and function of kupffer cells is decreased [ 40 ]  . 
il gadolinio in molti studi ha mostrato una buona accuratezza anche nello studio dei piccoli hcc ( < 1 , 52 cm ) e nei fegati cirrotici mostrando una sensibilit dell84% [ 11 , 31 , 32 ]  . la sensibilit nellidentificazione dei nd invece , solo del 15% con bassi valori di specificit in quanto lintensit di segnale dei nd ottenuta dopo mdc paramagnetico paragonabile a quella di molti hcc [ 33 ]  . lintroduzione dei mdc spio fornendo informazioni sulla composizione e sulla funzione delle cellule che costituiscono le lesioni nodulari e , superando i limiti diagnostici legati alle alterazioni della vascolarizzazione , consente di identificare anche hcc di piccole dimensioni che nello stadio precoce possono in parte conservare una vascolarizzazione normale ed essere quindi difficilmente differenziabili dalle altre lesioni nodulari [ 34 , 35 ]  . 
il meccanismo dazione dei mdc spio si basa sulla loro captazione da parte delle cellule del sistema reticolo - endoteliale epatico , le cellule di kupffer , che si traduce in una marcata riduzione dellintensit di segnale dei tessuti in cui sono presenti tali cellule . pertanto , leffetto prodotto nelle immagini pesate in t2 fa s che alcune lesioni benigne captano il mezzo di contrasto come il parenchima epatico sano ; di contro , le lesioni focali maligne eventualmente presenti , sprovviste di cellule del sistema reticolo - endoteliale , non captano il mdc e appaiono come aree iperintense [ 36 , 37 ]  . 
lutilizzo di questi mdc ha risolto in parte il problema dei falsi positivi che si osservano con i mezzi di contrasto paramagnetici iniettati a bolo , legato alla presenza di piccoli shunt artero - venosi che , manifestandosi come piccole aree di enhancement vascolare in fase arteriosa , possono simulare il pattern contrastografico di piccoli hcc . 
 a tale proposito , in letteratura sono stati anche riportati studi sulluso combinato di gadolinio legato ad acido acetico dietilenetriaminepenta ( gd - dtpa ) e spio che , soddisfacendo sia i criteri di vascolarizzazione sia quelli di composizione e funzionalit cellulare [ 11 , 38 ] , riduce il problema dei falsi positivi dei mezzi di contrasto paramagnetici e dei falsi negativi con mdc spio , questi ultimi legati alla presenza , in hcc ben differenziati o moderatamente differenziati , di cellule di kupffer sane che di conseguenza captano il mdc . infatti , uno studio anatomo - patologico sulla carcinogenesi multi - step ha dimostrato che cellule del kupffer sono ancora presenti nei noduli epatici durante il processo di degenerazione ; ci che varia il numero di tali cellule che si riduce durante le fasi della malattia cirrotica e nellevoluzione dellhcc da uno stadio di alta differenziazione ad uno di moderata o scarsa differenziazione [ 35 , 39 ]  . 
lintensit di segnale nelle sequenze t2w , quindi , sar tanto pi elevato quanto meno differenziato sar il tumore , essendo inferiori il numero e la funzionalit delle cellule del kupffer presenti [ 40 ] ; questo offre la possibilit di effettuare una diagnosi differenziale tra hcc e noduli displasici . sebbene la rm con i mezzi di contrasto spio sia una 1280 radiol med ( 2009 ) 114 : 12671282 differentiating between hcc and dn . although spio - enhanced mr imaging is an accurate technique in the cirrhotic liver , the heterogeneous uptake of spio agents may affect the interpretation of findings . 
in liver cirrhosis , the marked subversion of hepatic structure and function , intrahepatic vascular changes , or the presence of inflammatory processes , thromboses , hepatitis or steatosis , may affect the intracellular uptake and distribution of spio agents in the liver , thereby reducing their effectiveness in the detection and characterisation of small focal lesions [ 43 , 44 ]  . 
such alterations , known as spio liver uptake and distribution alterations ( spio - luda ) lead to the formation of hyperintense areas due to reduced uptake or hypointense areas , which is due to increased uptake . although the incidence of such alterations is relatively low , in some cases , they give rise to diagnostic problems on mr imaging [ 26 ]  . we observed no significant spio uptake and distribution alterations ( table 1 ) , and the signal intensity of the nodular lesions seen in our study ( dn and hcc ) corresponded to the patterns reported in the literature . 
there were no cases of well - differentiated hcc showing spio uptake , as reported by other authors [ 45 ] , and hence no cases of false negative hcc diagnoses . 
 on the basis of our results and in agreement with the literature , spio - enhanced mr imaging proved to be a valuable tool for the detection and characterisation of focal lesions in the cirrhotic liver . 
in particular , spio - enhanced mr imaging is currently the only imaging modality capable of distinguishing between dn and hcc and thus providing the opportunity for an accurate and timely diagnosis of malignant change of dn , a crucial aspect for prognosis . tecnica dimaging accurata nello studio del fegato cirrotico , leterogeneo up - take degli spio pu compromettere linterpretazione dei reperti . 
nella cirrosi epaticail notevole sovvertimento della struttura e delle funzioni epatiche , le alterazioni vascolari intraepatiche o la presenza di processi flogistici , trombosi vascolari , di epatiti , steatosi , possono modificare la captazione intra - cellulare e la distribuzione dei mdc spio nel fegato riducendone lefficacia , con una minore utilit degli stessi nella identificazione e caratterizzazione di piccole lesioni focali [ 43 , 44 ]  . 
tali alterazioni , denominate alterazioni di captazione e distribuzione epatiche del mdc spio ( spio - acde ) , provocano la formazione di aree di iperintensit da ridotta captazione o di ipointensit da aumentata captazione . 
lincidenza di queste alterazioni relativamente bassa ma in alcuni casi determina difficolt diagnostiche allesame rm [ 26 ]  . in questa esperienza non si sono dimostrate significative alterazioni della captazione e della distribuzione dei mezzi di contrasto ( tabella 1 ) e lintensit di segnale delle lesioni nodulari epatiche considerate nel nostro studio ( nd e hcc ) stata corrispondente ai possibili pattern di segnale rm riportati in letteratura . 
non stato riscontrato nessun caso di hcc ben differenziato che captava mdc spio , come descritto da alcuni autori in letteratura [ 45 ] ; non sono stati pertanto riscontrati falsi negativi nella diagnosi di hcc . sono stati riscontrati , invece , falsi negativi per la diagnosi di nd . 
tali risultati sono probabilmente legati al fatto che il nostro campione di studio era relativamente limitato , quindi ridotta stata la possibilit di riscontro di hcc con comportamento contrastografico simile a quello dei nd . 
rossi , universit di verona , verona , italy 2istituto di radiologia , ospedale cafoncello , treviso , italy 3istituto di radiologia , ospedale san bassiano , bassano del grappa , vicenza , italy correspondence to : n . 
thirteen of 15 patients underwent mr examination for clinical suspicion of a lesion located in the periscapular region , whereas in 2 / 15 cases it was an incidental finding during mr examination performed for other diseases . 
mr imaging with its multiplanar capabilities and high - contrast resolution has a high level of accuracy in characterising elastofibroma dorsi and may avoid the need for biopsy or surgical operation . keywords elastofibroma dorsi magnetic resonance riassunto obiettivo . 
sono stati analizzati gli esami rm del distretto toracico presenti nellarchivio di tre istituti di radiologia , effettuati con magnete superconduttivo da 1 , 5 t su 1233 pazienti in un arco di nove anni , al fine di identificare retrospettivamente la presenza di elastofibromi del dorso . 
sono stati identificati 17 elastofibromi del dorso in 15 pazienti ( 12 femmine , 3 maschi ; et media 58 anni , range 2882 anni ) ; due pazienti presentavano lesioni bilaterali . 
la rm presenta elevata affidabilit nella caratterizzazione dellelastofibroma del dorso e consente di evitare il ricorso alla biopsia ed al trattamento chirurgico , qualora non indicati . parole chiave elastofibroma del dorso risonanza magnetica 1284 introduction elastofibroma dorsi is a pseudotumoral lesion of mesenchy mal origin , presumably of a reactive nature , which develops electively in the soft tissues of the periscapular region between the scapula and the chest wall . 
it is observed in elderly subjects , mostly women , with a marked correlation with manual work carried out over long periods of time [ 1 ]  . microscopically , elastofibromas are characterised by fibroelastic connective tissue with poorly organised , thick and elastic fibres and rare collagen fibres , with varying amounts of intermingled fatty strands [ 2 , 3 ]  . 
considering the dramatic intensification of computed tomography ( ct ) and magnetic resonance ( mr ) examinations , a progressive increase in the incidental detection of scapulohumeral elastofibromas is likely to occur . 
there is therefore a possibility that these lesions are misinterpreted as suspected neoplasms by radiologists unaware of the features of this disease . mr imaging allows characterisation of the site and morphostructural features of typical elastofibroma dorsi , in particular , with t2 - weighted sequences , thanks to the possibility of differentiating it from other soft tissue lesions of the infrascapular region [ 58 ]  . 
therefore , the aim of our study was to analyse the mr features of elastofibroma dorsi by correlating imaging and pathologic findings to help decrease the number of unjustified surgical biopsies and resections . radiol med ( 2009 ) 114 : 12831291 introduzione lelastofibroma del dorso una lesione pseudotumorale ad origine mesenchimale di verosimile natura reattiva che si sviluppa elettivamente nei tessuti molli della regione periscapolare , fra la scapola e la parete toracica . 
colpisce una popolazione di et media - avanzata , in prevalenza di sesso femminile , mostrando inoltre una correlazione positiva con lespletamento di lavori manuali per lunghi periodi di tempo [ 1 ]  . 
dato il vertiginoso aumento di indagini di tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) , verosimile che si andr incontro ad un aumento progressivo dei riscontri incidentali di elastofibromi scapolo - omerali . 
esiste pertanto la possibilit che tali lesioni vengano erroneamente considerate come sospette neoplasie dal radiologo non a conoscenza delle caratteristiche di queste entit nosologiche . la rm consente la caratterizzazione , in particolare mediante sequenze t2 pesate , degli elastofibromi del dorso tipici , per sede e caratteristiche morfo - strutturali , grazie alla possibilit di differenziare altre lesioni dei tessuti molli della regione infra - scapolare [ 58 ]  . 
lo scopo del nostro lavoro quindi quello di analizzare le caratteristiche rm degli elastofibromi del dorso , correlando i reperti imaging con quelli anatomo - patologici , allo scopo di promuovere la riduzione del numero di biopsie ed escissioni chirurgiche ingiustificate . materials and methods materiali e metodi we retrospectively evaluated chest mr imaging examinations performed on 1 , 233 patients in our institute ( n = 365 ) and at two other hospitals ( n = 444 and n = 424 ) from january 2000 to october 2008 to look for the presence of elastofibroma dorsi . 
sono state individuate 17 lesioni in 15 pazienti ( 12 femmine , 3 maschi , range det 2882 anni , media 58 anni ) , con due pazienti con lesioni bilaterali simmetriche . 
 in tutti i pazienti sono state ottenute sequenze multiplanari spin - echo pesate in t1 ( te 9 , tr 550 , flip angle 90 ) e fast spin echo t2 ( te 90 , tr 2000 , flip angle 90 ) , sequenze short tau inversion recovery ( stir ) ( te 70 , tr 4800 , flip radiol med ( 2009 ) 114 : 12831291 1285 90 ) and short - tau inversion recovery ( stir ) sequences ( te 70 , tr 4 , 800 , flip angle 90 ) with slice thickness 4 mlesion enhancement patterns were studied in 12 / 17 lesions . 
the contrast - enhanced examination was carried out with gadolinium chelates ( dotarem , guerbet , france ) injected at 0.2 mg / kg using an automatic power injector ( medrad , spectris ) to administer a single bolus at a rate of 1 ml / s , followed by acquisition of t1 - dependent sequences with and without fat saturation ( te 2 , tr 5 , flip angle 10 )  . 
we used high - resolution sequences with 256256 matrix and variable field of view ( fov )  . the mr images were retrospectively analysed to evaluate site ( infrascapular or subscapular ) ; shape ( elliptical or rounded ) ; size ; margins ( regular or irregular ) ; structure ( homogeneous or heterogeneous ) ; signal intensity on t1weighted , t1 with fat suppression and t2 - weighted sequences ; subjective evaluation of enhancement after contrast administration ( poor , fair , high ) ; and any associated finding ( bone erosion , thickening or infiltration of the surrounding tissues )  . 
in the six lesions without histological confirmation , we evaluated stability over time ( up to 18 months follow - up ) of size , margins and signal to confirm the benign nature of the lesion . all examinations were interpreted by radiologists with 5 , 10 and 12 years experience with mr imaging in each of the three hospitals participating in this study . 
in all cases , the presence of thick , disorganised elastic fibres confirmed by a positive verhoeff - van gieson test and of collagen fibres interspersed with more or less thick , fatty tissue septations confirmed the diagnosis of elastofibroma . results results are summarised in table 1 . 
thirteen of 17 lesions had infrascapular location , and only 4 / 17 were subscapular . all lesions had an elliptical shape , with the longest axis in the craniocaudal direction . 
the lesion margins were regular in 14 / 17 cases ; only three lesions had margins indistinguishable from the surrounding structures , in particular , from the adjacent muscles . all lesions were characterised by a heterogeneous structure . 
lesame con mezzo di contrasto ( mdc ) paramagnetico stato eseguito mediante iniezione di chelati del gadolinio ( dotarem , guerbet , francia ) , alla dose di 0 , 2 mg / kg . 
il mdc stato iniettato mediante pompa automatica ( medrad , spectris , usa ) , in un bolo unico con velocit di iniezione di 1 ml / s , e successiva acquisizione di sequenze t1 - dipendenti con e senza saturazione del grasso ( te 2 , tr 5 , flip angle 10 )  . 
sono state utilizzate sequenze ad elevata risoluzione con matrice di 256256 ed un campo di vista ( fov ) variabile . le indagini rm sono state analizzate retrospettivamente per valutare : sede ( infra - scapolare o sotto - scapolare ) , forma ( ellittica o rotondeggiante ) , dimensioni , margini ( regolari o irregolari ) , struttura ( omogenea o disomogenea ) , intensit di segnale nelle sequenze pesate in t1 , t1 con soppressione del grasso , t2 , valutazione soggettiva dellenhancement dopo somministrazione di contrasto ( scarsa , buona , intensa ) , ed eventuali reperti associati ( erosione ossea , ispessimento o infiltrazione tessuti circostanti )  . 
nel caso delle 6 lesioni di cui non stata ottenuta una conferma istologica si ricorso alla valutazione della stabilit dimensionale nel tempo ( follow - up fino a 18 mesi ) , dei margini e delle caratteristiche di segnale per confermare la benignit della lesione . tutti gli esami sono stati interpretati da medici radiologi con esperienza di 5 , 10 e 12 anni in risonanza magnetica in ognuna delle 3 sedi coinvolte in questo studio . 
in tutti i casi la presenza di spesse fibre elastiche disorganizzate , confermate dalla positivit al test di verhoeff - van gieson , e di fibre collagene , alternate a setti pi o meno spessi di tessuto adiposo , ha confermato la diagnosi di elastofibroma . risultati la tabella 1 mostra schematicamente i nostri risultati . tredici lesioni su 17 avevano sede infra - scapolare e solo 4 / 17 sede sotto - scapolare . 
on t1 - weighted sequences , 14 / 17 lesions showed intermediate signal intensity , mostly isointense to muscle , whereas three were predominantly hyperintense due to the presence of a moderate amount of fatty tissue . 
1a , b axial t1 - weighted spin - echo image ( a ) and t2 - weighted image ( b ) show an elastofibroma dorsi in its usual location in the periscapular region in a 62 - year - old woman with clinically evident mass . 
1a , b immagine assiale spin - echo t1 - dipendente ( a ) e t2 - dipendente ( b ) che mostra un elastofibroma del dorso nella sua tipica sede infrascapolare in una donna di 62 anni con tumefazione clinicamente evidente . 
2a - d axial t1 - weighted se ( a ) , t1weighted ( b ) and t1weighted se images acquired after intravenous administration of gadolinium chelates in the axial ( c ) and coronal ( d ) planes show an elliptical lesion located in the left infrascapular region in a 66 - year - old woman with clinically evident swelling of the periscapular region and limited shoulder motion . 
2a - d le immagini assiali spin - echo t1dipendente ( a ) , t1 - dipendenti fs ( b ) , e le immagini spin - echo t1 - dipendenti dopo somministrazione endovena di chelati del gadolinio acquisite sul piano assiale ( c ) e coronale ( d ) , mostrano una lesione della regione infrascapolare sinistra a morfologia ellittica , prevalentemente ipointensa in t1 ( a ) , isointensa al muscolo in t1 fs ( b ) , con discreto e disomogeneo rinforzo contrastografico ( c , d ) , in una donna di 66 anni con tumefazione periscapolare e limitazione funzionale . 
 conversely , the 3 / 17 lesions rich in lipids showed intermediate signal intensity , being mildly hyperintense to muscle due to the presence of large amounts of intralesional fat . 
on t1 - weighted sequences with selective fat suppression , all lesions were markedly hypointense , with loss of signal of grasso intra - lesionale rispetto al muscolo ; nelle sequenze pesate in t1 con soppressione selettiva del grasso tutte le lesioni si presentavano marcatamente ipointense , con caduta di segnale delle componenti adipose . 
3a - d axial ( a ) and coronal ( b ) t1 - weighted se , axial t2 - weighted stir ( c ) and t1 - weighted fat - suppressed ( d ) images show a bilateral symmetrical elliptical lesion in the infrascapular region in a 58 - year - old woman with clinically evident bilateral symmetrical swelling . 
3a - d le immagini assiali spin - echo t1 - dipendente sul piano assiale ( a ) e coronale ( b ) , e assiali t2 - dipendente stir ( c ) e spin - echo t1 - dipendenti con soppressione del grasso ( d ) mostrano due lesioni simmetriche della regione infrascapolare a morfologia ellittica , disomogeneamente iperintense in t1 per la presenza di spesse bande di tessuto adiposo ( a , b ) , tendenzialmente isointense al muscolo in t2 stir ( c ) e dopo soppressione del grasso ( d ) , mantenendo tuttavia un segnale pi intenso del grasso sottocutaneo , in una donna di 58 anni con tumefazione periscapolare bilaterale simmetrica . 
by contrast , 2 / 12 lesions showed less enhancement , in part due to the presence of abundant fat inside thein none of the cases did we note alterations in the surrounding bone and muscular structures , except for the mass effect produced by the larger masses on the belly of adjacent muscles . ma disomogenea in 10 / 12 lesioni , verosimilmente per il progressivo accumulo di chelati del gadolinio nel contesto del tessuto fibroso . 
in nessun caso sono state riscontrate alterazioni delle strutture ossee e muscolari circostanti , fatta eccezione per limpronta dovuta alleffetto massa sui ventri muscolari adiacenti ad opera delle masse di maggiori dimensioni . 
 discussion elastofibroma dorsi is a pseudotumoral lesion characteristically located in the periscapular soft tissues between the scapula and the chest wall or caudally to the lower pole of the scapula [ 1 , 4 , 9 , 10 ]  . 
in approximately 10% of cases , elastofibroma dorsi is bilateral and symmetrical , whereas other locations are extremely rare and include the extremities , ischial tuberosities , small intestine , colon and tracheodiscussione lelastofibroma del dorso una lesione pseudotumorale che si localizza elettivamente nei tessuti molli della regione peri - scapolare , tra la scapola e la parete toracica o caudalmente al polo inferiore della scapola stessa [ 1 , 4 , 9 , 10 ]  . 
in circa il 10% dei casi lelastofibroma del dorso bilaterale e simmetrico , mentre rarissime sono le altre sedi di riscontro come in corrispondenza delle estremit , delle tuberosit ischiatiche , del piccolo intestino , del colon , e dellalbero tracheobronchiale [ 1 , 912 ]  . 
come dimostrato da alcuni autori , queste lesioni non sono affatto rare ai controlli radiol med ( 2009 ) 114 : 12831291 1289 bronchial tree [ 1 , 9 , 1012 ]  . 
as shown by some authors , these lesions are not infrequent findings at autopsy , and they affect 24% of women and 11% of men older than 55 years of age [ 9 , 10 ]  . 
the snapping scapula sign , almost pathognomonic , calls for diagnostic confirmation with either ct or mr imaging [ 2 , 4 , 13 ]  . the imaging appearance of these lesions is closely related to their histopathological features : composed of elastic fibres , collagen and fat [ 3 , 57 , 14 , 15 ] , elastofibromas may grow slowly , possibly as a result of repeated microtrauma between the scapula and the chest wall during heavy physical work [ 1 , 16 ]  . 
considering the increase in chest ct and mr examinations , the number of elastofibroma dorsi diagnoses is likely to rise . hence , awareness of the imaging findings may help to reduce the number of unnecessary surgical biopsies and resections . 
the presence of an elliptical lesion with more or less thick , fatty septations in the subscapular region , even though not pathognomonic , should suggest a diagnosis of elastofibroma in all typical settings . 
mr imaging is the modality of choice for characterising expansile infrascapular lesions , leading in most cases to a definite diagnosis [ 4 , 68 , 11 , 14 ]  . 
the mr appearance of elastofibroma dorsi is of a solid , low - signal - intensity mass that may be moderately heterogeneous due to the presence of a fibroelastic component , almost isointense to skeletal muscle both on t1and on t2 - weighted sequences , with an internal fatty component arranged into septations of variable size and number . 
the internal fatty component arranged in linear or curvilinear streaks parallel to the longest axis of the lesion has high signal intensity on t1 - weighted sequences , intermediate on t2 - weighted sequences and shows the typical signal loss on sequences with fat suppression [ 7 , 8 , 14 ]  . lesion margins may be more or less defined , although infiltration into surrounding structures has never been documented . the enhancement pattern of elastofibroma varies , with mild to marked enhancement being described [ 5 ]  . 
in our experience , most lesions showed intense and heterogeneous enhancement after contrast administration . elastofibroma develops deep to the serratus anterior muscle , rhomboid muscle , and latissimus dorsi at the level of the lower scapular angle and over the ribcage from the autoptici , arrivando ad interessare il 24% dei soggetti di sesso femminile e l11% di sesso maschile sopra i 55 anni [ 9 , 10 ]  . 
il segno dello schiocco scapolare , pressoch patognomonico , necessita di conferma diagnostica mediante tc o rm [ 2 , 4 , 13 ]  . laspetto imaging di queste lesioni strettamente correlato alle loro caratteristiche anatomopatologhe : essendo costituiti da fibre elastiche , collagene e grasso [ 3 , 57 , 14 , 15 ] , gli elastofibromi possono crescere lentamente in verosimile rapporto a microtraumatismi fra la scapola e la parete toracica durante lespletamento di lavori manuali pesanti [ 1 , 16 ]  . 
dato il continuo aumento delle indagini tc ed rm del distretto toracico verosimile attendersi un progressivo incremento delle diagnosi di elastofibroma del dorso : la conoscenza dei reperti imaging da parte del radiologo pu pertanto contribuire a ridurre il numero delle biopsie e delle escissioni chirurgiche non necessarie . 
la presenza di una lesione a morfologia ellittica , contenente setti adiposi pi o meno spessi nella tipica sede sotto - scapolare , anche se non patognomonica , deve indirizzare alla diagnosi in tutti i casi tipici di elastofibroma . 
la rm la metodica di scelta per la caratterizzazione delle lesioni espansive del distretto infra - scapolare consentendo nella maggior parte dei casi di indirizzare ad una diagnosi definitiva [ 4 , 68 , 11 , 14 ]  . 
laspetto rm dellelastofibroma del dorso quello di una massa solida a bassa intensit di segnale , che pu essere moderatamente disomogenea , dovuta alla compresenza di una componente fibro - elastica , quasi isointensa al tessuto muscolare scheletrico sia nelle sequenze t1che t2 - dipendenti , nel cui contesto si pu identificare talvolta una componente adiposa distribuita a setti di entit e numero variabile . lipointensit nelle sequenze t2 - dipendenti ascrivibile alla scarsa cellularit del tessuto fibroso e delle fibre elastiche [ 6 ]  . 
la componente adiposa , frammista al tessuto fibroso in fasci lineari o curvilinei disposti parallelamente allasse maggiore della lesione , presenta unintensit di segnale elevata nelle sequenze t1 - pesate , intermedia nelle sequenze t2 - pesate , e presenta il tipico abbattimento del segnale nelle sequenze con soppressione selettiva di tipo spettrale del grasso [ 7 , 8 , 14 ]  . 
i margini lesionali possono essere pi o meno definiti , ma in nessun caso stata documentata linfiltrazione delle strutture vicine . il comportamento contrastografico dellelastofibroma variabile , essendo stati descritti casi da lieve a marcata impregnazione [ 5 ]  . 
 lelastofibroma si sviluppa profondamente al muscolo serrato anteriore , al romboide ed al latissimus dorsi a livello dellangolo scapolare inferiore ed a ridosso della 1290 radiol med ( 2009 ) 114 : 12831291 sixth to the eighth rib [ 1 , 2 , 4 , 7 ]  . 
the differential diagnosis , limited to atypical lesions ( intralesional haemorrhage , abundance or scarcity of fat , marked irregularity of margins ) must include desmoid tumour , neurofibroma , fibroma and malignant fibrous histiocytoma . 
all these lesions have poor cellularity and predominant fibrous tissue , and all appear hypointense on t2 - weighted sequences , although generally without hyperintense fatty septations on t1 [ 6 , 17 ]  . 
on the other hand , lipoma , well - differentiated liposarcoma , and haemangioma , which appear hyperintense on t1 - weighted sequences , do not show the typical hypoisointensity on t2 nor the streaked pattern typical of the fatty septations [ 5 ]  . the high frequency of bilateral findings ( 10% ) , in addition to reinforcing a possible diagnostic suspicion , must prompt investigation of the contralateral region , even when clinically asymptomatic [ 2 , 4 , 11 , 12 ]  . on the basis of our experience , biopsy should be limited to atypical cases when radiological examinations , especially mr imaging , do not allow for a confident diagnosis . surgical treatment is only necessary in symptomatic cases with functional limitations and / or pain , or for masses > 5 c alternatively , a large asymptomatic mass may be monitored over time , after biopsy , to rule out a malignant nature [ 2 ]  . analysis of the mr findings that we retrospectively evaluated proved that in 13 / 17 cases the diagnostic hypothesis was correct . 
the four noncharacterised lesions included two cases of incidental findings , subjected to biopsy , and two atypical lesions subsequently surgically resected . we believe that contrast administration is not necessary for characterising lesions with typical clinical and radiological findings and that its use could be limited to clarifying the nature of the lesion and its relation to neighbouring structures in atypical cases . 
among all symptomatic patients , only three , showing abundant fatty component arranged in thick and irregular septa , had an uncertain interpretation . gabbia toracica a livello delle coste , dalla sesta allottava [ 1 , 2 , 4 , 7 ]  . 
la diagnosi differenziale , limitata alle lesioni atipiche ( emorragia intra - lesionale , abbondanza o scarsit di adipe , marcata irregolarit dei margini ) deve includere il tumore desmoide , il neurofibroma , il fibroma e listiocitoma fibroso maligno , tutti caratterizzati da scarsa cellularit e prevalenza fibrosa e che quindi appaiono prevalente ipointensi nelle sequenze t2 - dipendenti , non mostrando di regola setti adiposi iperintensi in t1 [ 6 , 17 ] ; il lipoma , il liposarcoma ben differenziato e lemangioma , che appaiono invece iperintensi nelle sequenze t1 - dipendenti , non mostrano la tipica ipo - isointensit in t2 n il pattern a bande dei setti adiposi [ 5 ]  . 
lelevata frequenza di bilateralit ( 10% ) di queste formazioni espansive , oltre che rafforzare lipotesi diagnostica quando presente , deve indurre ad indagare il distretto controlaterale , anche se clinicamente silente [ 2 , 4 , 11 , 12 ]  . 
 secondo la nostra esperienza , la biopsia dovrebbe essere attualmente limitata ai casi atipici , qualora le indagini radiologiche , ed in particolare la rm , non consentano una diagnosi sicura ; il trattamento chirurgico si rende necessario solo nei casi sintomatici con limitazione funzionale e / o dolore , o per masse superiori ai 5 cm di maggior asse . in alternativa una massa di cospicue dimensioni , ma clinicamente silente , pu essere semplicemente monitorata nel tempo dopo averne escluso la malignit con prelievo bioptico [ 2 ]  . lanalisi dei referti delle indagini rm da noi retrospettivamente valutate ha mostrato che in 13 / 17 casi lipotesi diagnostica formulata era corretta . 
le 4 lesioni non caratterizzate comprendevano 2 casi di riscontro incidentale , sottoposte a biopsia , e 2 lesioni atipiche successivamente sottoposte ad escissione chirurgica . riteniamo che la somministrazione di mdc non sia indispensabile alla caratterizzazione delle lesioni con tipici reperti clinici e radiologici , e che potrebbe essere limitata ai casi atipici per meglio chiarire la natura della lesione ed i rapporti con le strutture circostanti . 
in realt non da escludere che questa nostra ipotesi sia stata condizionata dal fatto che la nostra serie comprendeva in prevalenza pazienti sintomatici con lesioni tipiche sia per caratteristiche morfo - strutturali che per sede . 
knauth springer - verlag berlin heidelberg , 2009 isbn 978 - 3 - 540 - 72784 - 5 published online : 20 november 2009 springer - verlag 2009 this is an easy to read and very informative book on the use of contrast media in daily diagnostic practice . 
going through its 29 chapters , plus the appendix containing the european society of urogenital radiology ( esur ) guidelines on contrast media ( version 7.0 ) and one page dedicated to the official publications from the same society , provides the reader with all possible information on the use of different contrast media . the second edition of the book is the result of in depth study and research by the academic members of the esur contrast medium safety committee updating in more than one chapter , information on the use of gadolinium - based contrast media and their possible complications , in particular those related to the alarming nefrogenic systemic fibrosis ( nsf )  . 
 nsf , whose real cause is yet unknown , has come slowly to the attention of the medical community in the past few years rendering what was thought ( gadolinium contrast agents ) to be a very safe diagnostic tool as a possible , harmful instrument in the radiologists hands . since in the daily practice there is not only gadoliniumbased contrast media in use , much discussion is devoted also to the other different types of contrast media and their use . 
one will find information on ionic and non - ionic as well as barium and ultrasound contrast media , detailed information on meta - analysis in research , and information on the rules that must be followed in contrast - media research , approval , manufacturing , and clinical application . great attention is given to the discussion of contrast - media related complications : this issue is thoroughly discussed in the relevant section of many chapters and thoroughly reviewed in the esur appendix guidelines . 
one should realize that each time a contrast medium is used , however safe it might be considered , it can given the different individual conditions of the patient create adverse reactions . 
scorrendo i 29 capitoli che lo compongono , pi lappendice che elenca le linee guida della european society of urogenital radiology ( esur ) sulluso dei mezzi di contrasto nella sua pi recente versione ( 7.0 ) e la pagina dedicata allelenco delle pubblicazioni ufficiali della stessa societ , il lettore trover tutte le informazioni possibili circa luso dei diversi mezzi di contrasto . la seconda edizione il risultato di una gran lavoro di ricerca e studio da parte dei membri accademici del comitato esur sulla sicurezza dei mezzi di contrasto , lavoro che aggiorna , in particolare in pi di un capitolo , le informazioni circa limpiego dei mezzi di contrasto a base di gadolinio e le loro possibili complicanze , in particolare quelle riferibili alla pi temuta e cio la fibrosi nefrogenica sistemica ( nsf )  . la nsf , le cui cause sono ancora sconosciute , stata riconosciuta con lentezza e ritardo dalla comunit medica negli ultimi anni , rendendo quelli che erano pensati come mezzi di contrasto sicuri ( cio a base di gadolinio ) , quali possibili strumento di danno nelle mani del radiologo . dal momento per che nella pratica quotidiana non esiste solo limpiego dei mezzi di contrasto a base di gadolinio , una parte consistente del volume e di discussione viene riservata a tutti i restanti tipi di mezzo di contrasto . 
il lettore trover informazioni sui mezzi di contrasto ionici e non ionici , su quelli baritati e per impiego in ecografia : il tutto correlato da informazioni precise sulla meta - analisi nella loro ricerca ed informazioni importanti circa le regole che debbono essere impiegate nella ricerca , approvazione , preparazione ed applicazione clinica dei mezzi di contrasto . 
 grande attenzione viene dedicata alla discussione delle complicanze provocate dallimpiego dei mezzi di contrasto : questo tema viene discusso con precisione nella parti relative di molti capitoli e ben riassunta nellappendice sulle linee guida dellesur . 
ci si deve rendere conto che tutte le volte che viene utilizzato un mezzo di contrasto , per quanto sicuro lo si possa ritenere , questi pu , in funzione anche della differenti condizioni cliniche di ciascun paziente in cui viene impiegato , provocare delle reazioni , reazioni che possono essere assai lievi ed a risoluzione rapida e spontanea ma anche , 1384 radiol med ( 2009 ) 114 : 13831384 resolving over a very short period to very severe and unexpected , requiring immediate and correct treatment . how many people know the correct doses of adrenaline or atropine to be used in an emergency situation ? are there any emergency procedure - charts in your diagnostic radiology suites ? in this respect some of the pages are unnerving and hair - raising . 
 in summary , this is a very useful book and a highly recommended resource text for every radiology department , it should be easily accessible not only for the old staff radiologists but most importantly for those who are in training . al contrario , essere piuttosto evidenti ed impreviste , necessitanti un intervento terapeutico immediato e corretto . quante persone conoscono la dose corretta di adrenalina o di atropina da utilizzare in situazioni di emergenza ? nelle sale di diagnostica radiologica vi sono cartelli riportanti le procedure da seguire nelleventuale emergenza ? da questo punto di vista alcune della pagine del volume sono piuttosto preoccupanti , tali da far venire i brividi . 
between april and august 2008 , we examined 65 patients with 64 - slice mdct - ca : 6 / 65 using the step - and - shoot dose - saving protocol , 45 / 65 the cardiac dose right protocol and 14 / 65 using a standard protocol . 
in the per - patient analysis , image quality was excellent in 100% of the step - and - shoot protocols , in 91.1% of the cardiac dose right protocols and in 85.8% of the standard protocols . 
langiografia coronarica con tomografia computerizzata multistrato ( ac - tcms ) comporta una dose elevata a causa di spessori submillimetrici e ridotti tempi di acquisizione ; le case costruttrici quindi hanno prodotto protocolli di risparmio di dose che per possono ridurre la qualit delle immagini e laccuratezza diagnostica . 
tra aprile e agosto 2008 , 65 pazienti sono stati sottoposti ad ac - tcms a 64 detettori ; 6 / 65 mediante protocollo step and shoot , 45 / 65 con protocollo cardiac dose right , 14 / 65 con protocollo standard . 
nelle analisi per paziente la qualit delle immagini risultata ottimale nel 100% dei casi per il protocollo step and shoot , nel 91 , 1% dei casi per il protocollo cardiac dose right e nell85 , 8% dei casi per il protocollo standard . 
il radiologo deve utilizzare il protocollo di scansione pi adatto a seconda dellindicazione clinica , del paziente e del tipo di informazioni necessarie per liter diagnostico . radiol med ( 2009 ) 114 : 11961213 1197 keywords mdct coronary angiography dosimetry dose saving parole chiave angiografia coronarica tcms dosimetria risparmio di dose introduction introduzione the rapid technological advancements of multidetector - row computed tomography ( mdct ) have increased the diagnostic accuracy of the noninvasive imaging of the coronary arteries . 
this has led to an increase in the number of diagnostic examinations being performed and has placed the technique within the diagnostic workup of the patient with coronary artery disease [ 15 ]  . 
the increasingly widespread use of the technique has emphasised the need to monitor and limit radiation exposure to the patient during these procedures . the use of mdct coronary angiography ( mdct - ca ) in the study of the heart does , in fact , involve high dose levels owing to the special operating conditions with which these examinations are performed ( submillimetre thickness of the elements being studied ; reduced acquisition times ) and the reconstruction methods used . 
the studies performed to date are in agreement on attributing a dose of 13 msv for calcium scoring and 1020 msv for mdct - ca [ 6 , 7 ]  . 
focusing on issues of dosimetry therefore becomes crucial . this is even more so with regard to mdct - ca when used as an elective noninvasive technique for diagnostic and not therapeutic purposes in patients with a low - medium risk of disease . 
the aim of this study was to evaluate diagnostic quality in assessing the coronary arteries with a number of dose - saving protocols . incrementato i rapidi avanzamenti tecnici della tomografia computerizzata multistrato ( tcms ) hanno laccuratezza diagnostica dellimaging non invasivo delle arterie coronarie portando conseguentemente ad un incremento delle indagini diagnostiche effettuate e ponendo la tecnica allinterno del workup diagnositco del paziente coronaropatico [ 15 ]  . 
 limpiego della angiografia coronarica mediante tcms ( ac - tcms ) nello studio del cuore comporta infatti una dose elevata in considerazione delle particolari condizioni operative con cui vengono eseguite queste indagini ( spessori submillimetrici degli elementi di rivelazione , ridotti tempi di acquisizione ) e delle modalit di ricostruzione . 
gli studi finora eseguiti concordano nellattribuire una dose di 13 msv al calcium score ( ca - score ) e di 1020 msv alla ac - tcms [ 6 , 7 ]  . 
 questo ancora pi vero in caso di ac - tcms che rappresenta una metodica non invasiva in elezione per pazienti con basso - medio rischio e che ha finalit diagnostica ma non terapeutica come la angiografia coronarica ( acc ) che in corso della stessa procedura effettua la diagnosi e la eventuale terapia con valori di esposizione relativamente bassi , mediamente pari a 57 msv se confrontati con lac - tcms [ 8 , 9 ]  . 
per fare fronte al problema dosimetrico le case costruttrici si sono mosse per la produzione di protocolli di risparmio di dose : tale risparmio di dose pu per comportare una riduzione della qualit delle immagini andando quindi a discapito quindi dellaccuratezza diagnostica [ 1015 ]  . 
an additional inclusion criterion was the presence of a heart beat with sinus rhyth patients with chronic atrial fibrillation with a mediumlow ventricular response ( inducible < 65 bpm ) were also admitted . exclusion criteria the following patients were excluded from the mdct - ca study : symptomatic patients with acute chest pain and an electrocardiogram ( ecg ) positive for ischaemia , patients with a heart rate 65 bpm , patients with a known allergy to iodinated contrast material , pregnant patients , patients with respiratory failure , patients with unstable clinical conditions and severe heart failure . 
patients unable to maintain breathhold for at least 810 s and with an unstable heart beat were also excluded . patient preparation the day before the examination , ecg monitoring was performed . 
at the time of the examination , the heart rate was monitored again , and when required , was lowered further with a 2.5 - mg intravenous dose of atenolol . the patient was positioned on the patient tray and connected to the electrodes monitoring a single ecg lead corresponding to either lead i or lead iii . 
the electrodes were positioned above the left and right clavicles with a ground electrode placed on the abdominal surface of the left tutti i pazienti sottoposti allindagine sono stati ammessi allo studio non invasivo delle coronarie se la loro frequenza cardiaca era < 65 bpm ( spontanea o indotta dalla somministrazione di - bloccanti ) e se avevano capacit di mantenere una apnea sufficiente per il periodo di acquisizione del volume di dati , in media pari a 1012 secondi . 
sono stati accettati allo studio anche i pazienti con fibrillazione atriale cronica con risposta ventricolare medio bassa , inducibile < 65 bp criteri di esclusione i pazienti sintomatici con dolore toracico acuto e elettrocardiogramma ( ecg ) positivo per ischemia , con frequenza cardiaca 65 bpm , allergia nota al mezzo di contrasto iodato , gravidanza , insufficienza respiratoria , stato clinico instabile e scompenso cardiaco di grado severo vengono esclusi dallo studio mediante ac - tcms . 
al momento dellesame stata controllata le frequenza cardiaca e se necessario ulteriormente abbassata per via endovenosa dal personale medico dedicato ( atenololo 2 , 5 mg )  . il paziente stato posizionato sul tavolo porta - paziente e collegato agli elettrodi dellecg monitorando una sola derivazione ecg corrispondente a di o diii . 
heart rate variability was observed , and a test was performed to assess whether the duration of the patients breath - hold was compatible with the scan time . the iodinated contrast material with an iodine concentration of 400 mgi / ml ( iomeron 400 , bracco , milan , italy ) was administered intravenously into an antecubital vein of the left arm with the use of an 18to 20 - gauge needle cannula and an injection rate of 5 ml / s . 
the standard dose of 80 ml was followed by a 20 - ml bolus of saline solution . acquisition synchronisation was achieved with the bolus tracking technique , which involves positioning a region of interest ( roi ) in the descending aorta . 
when the attenuation value within the roi reached the preset value of 120 hu , the scan was begun . protocols standard sono stati posizionati in sede sovraclaveare destra e sinistra con elettrodo terra sulla superficie addominale del fianco sinistro . 
 stata osservata la variabilit della frequenza cardiaca ed , inoltre , stato eseguito un test per valutare se la durata dellapnea del paziente era compatibile con il tempo di scansione . 
 il mezzo di contrasto iodato alla concentrazione iodica di 400 mgi / ml ( iomeron 400 , bracco , milano , italia ) stato somministrato per via endovenosa attraverso una vena antecubitale del braccio sinistro mediante unagocannula da 1820 gauge somministrato al flusso di 5 ml / s , alla dose standard di 80 ml seguito da un bolo di soluzione fisiologica di 20 ml . 
 la sincronizzazione dellacquisizione stata ottenuta mediante tecnica di bolus tracking che consiste nel posizionare una regione dinteresse ( roi ) nellaorta discendente ; quando il valore di attenuazione allinterno della roi ha raggiunto la soglia prestabilita , pari a 120 hu , stato dato il via alla scansione . all patients with a body mass index ( bmi ) > 27 , with early ectopic heart beats , extrasystoles , uncertain breath - hold or unstable heart rate , underwent a standard acquisition protocol . 
the protocol parameters included 120 kv , 800970 mas with a maximum intensity at 75% of the r - r interval and decreasing ( minimum 20% ) in the other phases of the cardiac cycle . 
in tutte le fasi del ciclo cardiaco viene somministrata dose piena , essendo quindi possibile una ricostruzione retrospettiva sia in fase telediastolica ( 75% ) che telesistolica ( 40% )  . 1200 step and shoot all patients with a stable heart rate < 65 bpm and bmi < 23 underwent the step - and - shoot dose - saving protocol . 
the protocol parameters included 120 kv and 210 mas , with the dose being delivered only at 75% of the r - r interval and nothing in the other phases of the cardiac cycle . 
the examination protocols are summarised in table 1 . a precontrast enhancement phase was obtained for all patients to evaluate the level of calciu the quantity of calcium in the coronary artery walls was evaluated with the calcium score technique following the agatston protocol . the ed was judged to be the best parameter for the evaluation and comparison of radiation exposure . 
tale protocollo prevede scansioni a 120 kv e 800970 mas con intensit massima al 75% del ciclo r - r , e decrescente ( min 20% ) nelle altre fasi del ciclo . 
only in the end - diastolic ( 75% ) phase is standard dose applied to the patient , and a lower dose is given in the rest of the cardiac cycle . 
the exposure is expressed as the dose length product ( dlp ) obtained in milligray per centimetre ( mgy / cm ) and was multiplied by a dose absorption conversion factor for the chest equivalent to 0.017. 
the patient characteristics subdivided by dose - saving protocol are summarised in table 2 . image analysis two expert observers , a radiologist and a cardiologist , performed a qualitative evaluation in consensus , which considered all segments of the coronary artery tree following the 17 - segment classification system of the american heart association [ 18 ]  . 
evaluation of the diagnostic quality of the images was performed by giving a score per segment and per examination of 0 in the event the examination or segment could not be evaluated and was therefore of insufficient quality , 1 for moderate quality and 2 for excellent quality . statistical analysis we used the spearman test to correlate image quality with the protocol used . 
tale dose , denominata anche dose length product ( dlp ) ed espressa in mgy / cm , stata moltiplicata per un fattore di conversione di assorbimento dose per il torace pari a 0 , 017 . 
le caratteristiche riassuntive dei pazienti suddivise per protocollo di modulazione di dose sono riassunte nella tabella 2 . analisi delle immagini due osservatori esperti specialisti in radiologia e cardiologia hanno effettuato in consenso una valutazione qualitativa considerando tutti i segmenti dellalbero coronarico , seguendo il sistema di classificazione della american heart association , diviso in 17 segmenti [ 18 ]  . 
al fine di giudicare la qualit diagnostica delle immagini stato conferito per segmento e per esame un punteggio pari a 0 in caso di esame o segmento non valutabile , di qualit insufficiente , 1 in caso di qualit discreta , 2 in caso di qualit ottimale . 
la distribuzione dei fattori di rischio risultata omogenea non mostrando significativa prevalenza di un fattore di rischio rispetto ad un altro nelle tre differenti categorie di protocolli di modulazione di dose . 
lanalisi delle caratteristiche dei pazienti suddivise per protocollo di modulazione di dose riassunta nella tabella 3 . radiol med ( 2009 ) 114 : 11961213 1203 mgy / cm for the cardiac dose right protocol and 290 mgy / cm for the step - and - shoot protocol . 
in total , 780 segments were identified ( mean 1314 per patient )  . with regard to the per - patient analysis , an image quality rating of 2 ( excellent ) was achieved in 6 / 6 ( 100% ) patients for the step - and - shoot protocol , 41 / 45 ( 91.1% ) patients for the cardiac dose right protocol and 12 / 14 ( 85.8% ) for the standard protocol . 
with regard to the per - segment analysis , an image quality rating of 2 was achieved in 31 / 31 ( 100% ) segments for the step - and - shoot protocol , 483 / 547 ( 82% ) segments for the cardiac dose right protocol and 165 / 202 ( 81.6% ) segments for the standard protocol . 
the results of the per - patient and per - segment analyses are summarised in table 4 . discussion mdct - ca has become a part of routine clinical practice only recently . 
its use in the past was mostly limited to validation studies in comparison with cca , with extensive use only in a few centres of applied clinical research [ 1921 ]  . the increasing use of the technique has focused attention on the need to maintain radiation exposure to the patient as low as possible to conform to the alara criteria for the optimisation of the examination [ 22 ]  . 
the term optimisation here suggests maintaining the dose at the lowest possible level achievable that is compatible with the image quality required for obtaining the sought - after diagnostic information [ 12 , 22 ]  . our findings show that the use of the appropriate acquisition technique makes possible a significant saving in radiation exposure of around 70% with the use of the cardiac dose right protocol and 30% with the step - and - shoot protocol when compared with the standard protocol . 
il bmi medio per i pazienti sottoposti a protocollo standard risultato essere pari a 26 , 6 , per il protocollo cardiac dose right di 22 , 6 e per il protocollo step and shoot di 21 , 3 . la dose registrata in termini di dlp comprensiva di acquisizione contrastografica e ca - score stata pari a 1205 , 58 mgy / cm in caso di protocollo standard , 872 , 07 mgy / cm in caso di protocollo care dose right e 390 mgy / cm in caso di protocollo step and shoot . 
la dose assorbita per ogni indagine di ca - score in termini di ctdivol era pari a 7 e , considerando che la lunghezza delle scansioni era mediamente pari a 13 cm ( range 1015 ) , ne risultata una dose assorbita in termini di dlp pari a 91 mgy / cm che , espresso in msv e rapportato al distretto anatomico in esame ha portato ad una dose effettiva per il solo ca - score pari a 1 , 547 . la dose effettiva al paziente dellintero esame comprendente scout , ca - score , premonitoring , monitoring e actcms in termini di msv risultata essere pari a 20 , 49 msv in caso di protocollo standard , 14 , 8 msv in caso di protocollo cardiac dose right e 6 , 63 msv in caso di protocollo step and shoot . 
sono stati analizzati in totale 780 segmenti ( media 1314 segmenti per paziente )  . nel contesto di una analisi per paziente la qualit delle immagini in caso di protocollo step and shoot risultata essere pari a 6 / 6 ( 100% ) pazienti valore 2 ( qualit ottimale ) , in caso di protocollo cardiac dose right risultata essere pari a 41 / 45 ( 91 , 1% ) pazienti valore 2 , in caso di protocollo standard risultata essere pari a 12 / 14 ( 85 , 8% ) pazienti valore 2 . 
nel contesto di una analisi per segmento la qualit delle immagini in caso di protocollo step and shoot risultata essere pari a 31 / 31 segmenti valore 2 ( 100 % ) , in caso di protocollo cardiac dose right risultata essere pari a 483 / 547 segmenti valore 2 ( 82% ) , in caso di protocollo standard risultata essere pari a 165 / 202 segmenti valore 2 ( 81 , 6% )  . 
i risultati delle analisi per paziente e per segmento sono riassunti in tabella 4 discussione lac - tcms una metodica entrata nella routine clinica solo molto recentemente , per lo pi utilizzata nel passato per validazione della metodica a paragone con lacc con un uso estensivo della metodica riservato solamente ad alcuni centri di ricerca clinica applicata [ 1921 ]  . 
volume - rendered and axial native scan obtained from retrospectively gated reconstructions at 40% ( a , b ) and 75% ( c , d ) of the r - r interval . 
la qualit delle immagini risulta pi scarsa nella finestra temporale al 40% con risparmio di dose . to perform a correct evaluation , the dose values must be correlated with the operating parameters used ( slice thickness , mas , kv , volume covered ) and the image quality parameters ( spatial resolution , noise , contrast ) [ 22 ]  . 
new ct scanners are equipped with dose - modulation systems that vary the tube current so as to achieve the highest possible image quality by optimising the use of x - rays and thus reducing radiation exposure to the patient . 
to obtain the same quantity of radiation and therefore the same level of noise , modulation of the tube current is crucial . ( as low as reasonably achievable ) di ottimizzazione dellindagine [ 22 ]  . 
con il temine ottimizzazione si intende il mantenimento della dose al livello pi basso ottenibile , compatibilmente con la qualit dellimmagine necessaria ad ottenere linformazione diagnostica ricercata [ 12 , 22 ]  . i nostri risultati dimostrano come con lutilizzo della tecnica di acquisizione appropriata si riesca ad ottenere un notevole risparmio di dose pari mediamente al 70% in caso di utilizzo di protocollo cardiac dose right e 30% in caso di protocollo step and shoot rispetto al protocollo standard . nonostante la riduzione di dose , la qualit complessiva dellesame rimasta soddisfacente , confermando che non 1208 radiol med ( 2009 ) 114 : 11961213 fig . 
volume - rendered and axial native scan obtained from retrospectively gated reconstructions at 40% ( a , b ) and 75% ( c , d ) of the rr interval . 
la qualit delle immagini risulta pi ottimale in tutte le finestre di acquisizione . scanner manufacturers adopt a variety of approaches to achieve this aim , ranging from the choice of the value of the current , the reference noise or the reference image . 
in addition to the normal dose - reduction techniques available on all scanners , techniques dedicated to the study of the heart have been implemented with two different modalities . the first ecg - gated dose modulation reduces the delivery of the radiation beam during the cardiac cycle ( e.g. systolic phase ) , which can be excluded a priori from the retrospective reconstruction phases [ 12 ]  . 
with this approach , the peak tube current ( mas ) is applied only during the diastolic phase of the cardiac cycle , necessario sempre utilizzare il protocollo standard di acquisizione . 
 per effettuare una corretta valutazione essenziale correlare i valori di dose ai parametri operativi utilizzati ( spessore di strato , mas , kv , volume coperto ) e ai parametri di qualit dellimmagine ( risoluzione spaziale , rumore , contrasto ) [ 22 ]  . 
i nuovi sistemi tc sono dotati di controllo della dose che agiscono variando il valore dei mas con lo scopo di raggiungere un migliore livello di qualit di immagine , ottimizzando limpiego di radiazione x e riducendo di conseguenza la dose radiante al paziente . 
where available , this technique can be used in patients without arrhythmias , with a constant heart rate and in whom the interval of the diastolic phase can be readily calculated , as the low level of radiation in the remainder of the cardiac cycle can compromise image quality [ 25 ]  . technique the second dose optimisation involves prospective triggering whereby the reconstruction window is preset by the radiologist before the contrast - enhanced study [ 15 ]  . 
the dose delivered to the patient is significantly reduced in that there is a sequential and nonspiral acquisition , which therefore reduces oversampling of the data acquired [ 13 ]  . 
because a rising bmi negatively influences image quality , which appear markedly affected by noise , this low - dose protocol can only be used for subjects who weigh < 70 kg and have a bmi < 20 . 
it should nonetheless be noted that mdct - ca is only rarely used to evaluate ventricular radiazione e quindi lo stesso livello di rumore , indispensabile agire sul valore dei mas . le ditte costruttrici utilizzano approcci diversi che variano tra la scelta di un valore di corrente , di rumore di riferimento o di immagine di riferimento . 
 la prima ( ecg - gated dose modulation ) riduce lerogazione del fascio di radiazione durante fasi come la sistole e che , a priori , si possono escludere dalle fasi di ricostruzione retrospettiva [ 12 ]  . 
tramite questo approccio loutput nominale massimo impostato ( mas ) viene applicato solo durante la fase diastolica del ciclo cardiaco , ovvero nella fase in cui i dati possono essere utilizzati per la ricostruzione . 
con questo metodo il valore della coronaro - tc pu dare valori di dose efficace dellordine di 57 msv , in funzione della frequenza cardiaca del paziente . dove disponibile questa tecnologia pu essere utilizzata per tutti i pazienti in assenza di aritmia , per pazienti con battito costante e in cui facilmente calcolabile lintervallo della fase diastolica su cui andare a ricostruire i dati , in quanto il 1210 radiol med ( 2009 ) 114 : 11961213 function , because echocardiography is in widespread use and because cardiac mr is the reference standard for this analysis . the data from our patient series show that the correct selection of the dose - saving protocol within subcategories of the patient population can provide a good compromise between the dose delivered and image quality and therefore overall diagnostic value . on the basis of the characteristics of the sample population , it is apparent that the most significant variable that determines the choice of one protocol over another is bmi . heart rate may play a significant role only in the choice between the step - and - shoot protocol and the other two protocols , whereas it has no significant effect on the choice between the standard protocol and the cardiac dose right protocol . at our centre , we make regular and widespread use of dose optimisation protocols with the following strategy . 
if the patient weighs < 70 kg , has a bmi < 20 and a stable heart rate < 65 bpm , then they undergo the mdct - ca study with the step - and - shoot protocol . 
if the patient weighs > 70 kg , has a bmi between 20 and 25 but a stable heart rate < 65 bpm , then they undergo mdct - ca with the cardiac dose right protocol . 
if , instead , the patient weighs > 70 kg , has a bmi > 25 and an unstable heart rate and we foresee the need for ecg editing or the evaluation of images reconstructed from different time windows , then we apply the standard protocol . 
in all cases where a functional evaluation is requested , we do not apply the step - and - shoot protocol but rather use the cardiac dose right protocol when possible . 
7 dose effettiva al paziente media nei differenti protocolli di modulazione di dose . basso livello di radiazioni del resto del ciclo cardiaco possono compromettere la qualit delle immagini [ 25 ]  . la seconda tecnica di ottimizzazione della dose prevede un triggering prospettico nel quale viene preimpostata dal radiologo prima dellesame contrastografico lunica finestra di ricostruzione [ 15 ]  . 
la dose al paziente decresce in modo importante in quanto vi una acquisizione sequenziale e non spirale che porta quindi a una riduzione del sovracampionamento dei dati acquisiti [ 13 ]  . 
per il fatto che lindice di massa corporea ( bmi ) influenza negativamente la qualit delle immagini che appaiono pi rumorose , tale protocollo a basso dosaggio pu essere utilizzato al fine di ottenere immagini diagnostiche solamente per soggetti con peso inferiore ai 70 kg e bmi inferiore a 20 . 
va detto per che la ac - tcms solo raramente viene utilizzata come metodica per la valutazione della funzione ventricolare essendo largamente in uso lecocardiografia ed essendo la risonanza magnetica cardiaca ( cardio - rm ) lo standard di riferimento per tale analisi . 
 dai dati ricavati dalla nostra casistica abbiamo dimostrato come una corretta selezione del protocollo di risparmio di dose in subpopolazioni campione da sottoporre allindagine porti a un buon rapporto tra la dose erogata , la qualit dellimmagine ottenuta e quindi il valore diagnostico complessivo . 
 sulla base dellanalisi delle caratteristiche della popolazione campione emerge come la variante pi significativa che determina la scelta di un protocollo rispetto ad un altro sia lindice di massa corporeo . 
la frequenza cardiaca poi varia in maniera pi significativa solo tra il protocollo step and shoot e gli altri 2 , mentre non varia significativamente tra il protocollo standard e cardiac dose right . nel nostro istituto utilizziamo regolarmente i protocolli di ottimizzazione della dose seguendo la seguente strategia di impostazione : se il paziente ha un peso inferiore ai 70 kg e bmi inferiore a 20 e mantiene una frequenza cardiaca stabilmente sotto i 65 bpm viene sottoposto ad indagine actcms mediante protocollo step and shoot . 
se il paziente ha un peso superiore ai 70 kg e bmi compreso tra 20 e 25 ma con frequenza cardiaca stabilmente sotto i 65 bpm viene sottoposto ad indagine ac - tcms mediante protocollo di modulazione della dose cardiac dose right . 
nel caso in cui il paziente sia sopra i 70 kg e con bmi superiore a 25 e con frequenza cardiaca instabile e prevediamo la necessit di un editing dellecg o la valutazione delle immagini secondo pi finestre temporali di ricostruzione applichiamo il protocollo standard . 
utilizziamo questa strategia di risparmio di dose in quanto lindagine , esponendo il paziente ad una dose considerevole , non pu andare incontro a un esame di qualit generalmente insoddisfacente e deve permettere una diagnosi nella stragrande maggioranza dei casi . 
 va infine ricordato come lac - tcms ormai nelluso clinico si proponga come metodica valida in grado spesso di modificare liter diagnostico del paziente cardiopatico evitando in molti casi lesecuzione di indagini invasive ed in alcuni casi inutili come lacc ( nel caso in cui non si dimostrino stenosi significative e quindi non si proceda a rivascolarizzazione ) oppure diagnostiche , ma con accuratezza 1212 radiol med ( 2009 ) 114 : 11961213 myocardial scintigraphy , which generally involves a dose to the patient per examination of around 2023 msv [ 2528 ]  . inferiore se paragonate allac - tcms come ad esempio la scintigrafia miocardica che generalmente prevede una dose al paziente per esame media di circa 2023 msv [ 2528 ]  . 
 conclusions conclusioni given that the latest generation of scanners has led to an increase in the dose delivered to patients , it is of crucial importance that dose - saving systems are adopted whenever possible . 
the radiologist must be aware of acquisition techniques with dose - saving protocols to avoid exposing the patient to an unnecessary and dangerous dose and must propose the most appropriate protocol in relation to the clinical indication , the type of patient and the information required for the diagnostic process . dato che con le ultime generazioni di scanner vi un incremento di dose al paziente di primaria importanza lutilizzo di sistemi di risparmio di dose , ove possibile . 
de filippo , scienze radiologiche , azienda ospedaliero - universitaria di parma , via gramsci 14 padiglione barbieri , 43100 parma , italy , tel . : + 39 - 052 - 1703660 , e - mail : massimo.defilippo@unipr.it received : 20 march 2008 / accepted : 13 october 2008 / published online : 19 november 2009 springer - verlag 2009 abstract purpose . 
through a search of the pathology databases of four italian hospitals , we identified six men ( mean age , 56 years ) with a histological diagnosis of ecd . histology was performed on retroperitoneal or pulmonary biopsy , depending on disease involvement on imaging . patients underwent plain radiography of the lower limbs and chest , total - body computed tomography ( ct ) and bone scintigraphy . 
magnetic resonance ( mr ) imaging was performed in two patients to evaluate the lower limbs and in one patient to study the brain , the chest and the abdomen . 
imaging studies revealed extraskeletal manifestations in all patients , including involvement of the retroperitoneal space ( n = 4 ) , the lung ( n = 4 ) and the heart ( n = 2 )  . 
sono stati identificati nel data base dellunit operativa di anatomia patologica di quattro ospedali italiani , sei pazienti con ecd , di sesso maschile , con et media di 56 anni . 
la diagnosi di natura dellecd istologica , 1320 radiol med ( 2009 ) 114 : 13191329 keywords erdheim - chester disease retroperitoneal fibrosis histiocytosis tuttavia il sospetto diagnostico pu essere agevolmente posto con limaging radiologico . parole chiave malattia di erdheim - chester fibrosi retroperitoneale istiocitosi introduction introduzione erdheim - chester disease ( ecd ) is a rare , systemic xanthogranulomatous infiltrative disease characterised by deposition of lipid - laden histiocytes in various organs , with the constant involvement of bone [ 16 ]  . 
ecd was first described by the american physician william chester and the viennese pathologist jacob erdheim in 1930 , who described two cases of a peculiar form of histiocytosis that they distinguished from other disorders such as handschller - christian disease and niemann - pick disease [ 7 ]  . the eponym erdheim - chester disease was coined by jaffe in 1972 [ 8 ]  . 
 the disease affects both genders , though with a slight predilection for men , and has a peak incidence between the fifth and sixth decade of life , although it may manifest at any age [ 4 ]  . 
skeletal involvement is most common in the long bones of the lower limbs . approximately 50% of patients present with extraskeletal manifestations , the most commonly involved sites being the heart , the lungs , the kidneys , the retroperitoneal space , the central nervous system and the skthe clinical course of ecd ranges from the absence of symptoms to a very poor outcome [ 9 ]  . 
 materials and methods we retrospectively searched the pathology databases of four italian hospitals for cases of ecd entered between january 2002 and january 2008 to identify organ involvement and clinical and radiological features . 
the diagnostic criteria for ecd are histopathological and based on the presence of lipid - laden histiocytes immunopositive for cd68 and immunonegative for s - 100 , cd1a and birbeck granules . 
 imaging studies included plain radiography of the lower limbs and chest , bone scintigraphy with technetium 99 ( 99mtc ) and chest and abdominal multidetector computed tomography ( mdct )  . 
patient 1 , who had a history of la malattia di erdheim - chester ( ecd ) una rara patologia sistemica di tipo infiltrativo xantogranulomatoso , caratterizzata dalla presenza di depositi di istiociti contenenti materiale lipoideo in vari organi , con coinvolgimento osseo pressoch costante [ 16 ]  . 
lecd fu descritta per la prima volta nel 1930 da un medico nordamericano , william chester e da un patologo viennese , jacob erdheim , che identificarono in due pazienti una particolare forma di istiocitosi , distinguendola da altri disordini , come la malattia di hand - schllerchristian e di niemann - pick [ 7 ]  . 
 la malattia presente in entrambi i sessi , con una lieve prevalenza nel sesso maschile ed un picco di incidenza tra la 5 e la 6 decade di vita , sebbene possa manifestarsi a qualsiasi et [ 4 ]  . 
linteressamento scheletrico dellecd riguarda prevalentemente le ossa lunghe degli arti inferiori ; circa la met dei pazienti presentano manifestazioni extra - scheletriche , le sedi maggiormente coinvolte sono : cuore , polmoni , reni , retroperitoneo , sistema nervoso centrale e cute . 
 materiali e metodi abbiano ricercato retrospettivamente nel database delle unit operative di anatomia patologica di quattro ospedali italiani la presenza di casi di malattia di erdheim - chester ( ecd ) , nel periodo compreso tra il gennaio 2002 e il gennaio 2008 , al fine di valutarne limpegno nei differenti organi e gli aspetti clinico - radiologici . 
i criteri diagnostici di ecd , sono istopatologici , basati sulla presenza di istiociti ricchi di lipidi , positivi allantigene per il cd68 e prive degli antigeni della proteina s - 100 , del cd1a e dei granuli di birbeck . 
il campionamento tissutale era stato ottenuto mediante biopsia retroperitoneale in tre casi e polmonare nei rimanenti tre casi . i pazienti erano stati sottoposti a radiografia del torace e degli arti inferiori , scintigrafia ossea con tecnezio 99 ( 99mtc ) , tomografia computerizzata multidetettore ( tcmd ) toracica e addominale . 
il paziente 1 , con anamnesi positiva per diabete insipido e microadenoma ipofisario , fu studiato radiol med ( 2009 ) 114 : 13191329 1321 diabetes insipidus and pituitary microadenoma , was studied with high - field magnetic resonance ( mr ) imaging to evaluate the brain , the chest , the abdomen and the lower limbs . patient 2 underwent mr imaging of the lower limbs to investigate diffuse bone changes identified on plain radiography . 
le indagini di imaging sono state valutate da due radiologi . results patients 1 and 2 had cardiac involvement , which in one patient manifested clinically as chest tightness and in the other as dyspnoea on exertion . 
in one case , the retroperitoneal solid tissue caused renal artery stenosis with resulting arterial hypertension , whereas in the other three cases , it surrounded the aorta and the iliac arteries , causing risultati nei pazienti 1 e 2 si evidenziava coinvolgimento cardiaco dellecd . 
lesordio clinico di ecd nei pazienti 3 e 4 era caratterizzato da alterazione degli indici di funzionalit renale , associato a ripetuti episodi di infezioni delle vie urinarie nel caso 3 . 
nei primi quattro pazienti la tc addome evidenziava infiltrazione retroperitoneale da parte di tessuto solido , prevalentemente perirenale e simmetrico , ipodenso e dotato di lieve contrast enhancement dopo somministrazione di mezzo di contrasto ( mdc )  . 
il tessuto solido retroperitoneale determinava nel caso 1 stenosi dellarteria renale con conseguente ipertensione arteriosa mentre negli altri tre casi circondava laorta e le arterie iliache , con fenomeni di incarceramento della fig . 
magnetic resonance image of the chest ( balanced sequence ) in the coronal plane ( a ) and contrast - enhanced computed tomography of the chest with four - chamber multiplanar reconstruction ( b )  . 
rm del torace ( balance w ) in sezione coronale ( a ) e tc con mdc del torace in sezione assiale obliqua four chambers mpr ( b )  . 
contrast - enhanced computed tomography of the upper abdomen ( a , b ) : the coated aorta , a specific finding in erdheim - chester disease , is well - depicted in the magnified image ( arrows in b )  . fig 2a , b ecd in fase avanzata . 
tc con mdc delladdome superiore ( a , b ) : aorta rivestita da tessuto solido , aspetto peculiare dellecd , ben evidente nellimmagine ingrandita ( frecce in b )  . 
renal pyelectasia , more evident on the left side , is due to compression by the fibrous tissue , which is also present at the level of the proximal periureteral spaces  . fig 3a , b ecd in fase iniziale . 
nel caso 5 lecd si manifestava con dolori al rachide in assenza di alterazioni allrx tradizionale , mentre la scintigrafia con 99mtc mostrava iperfissazione del radiol med ( 2009 ) 114 : 13191329 1323 fig . 
magnetic resonance images of the upper abdomen : axial t2 - weighted turbo spin - echo ( a ) and t1 - weighted fat - saturated fast - field echo sequence after the intravenous administration of paramagnetic contrast material . 
note the homogeneous enhancement of the fibrous tissue during the venous phase ( b ) and the sparing of the periaortic and pericaval regions ( a , b )  . fig 4a , b ecd in fase avanzata . 
il sottoslivellamento laterale sn della sella turcica ( freccia ) segno indiretto della presenza di un microadenoma ipofisario . scintigraphy showed increased tracer uptake at the level of a thoracic vertebra . four patients ( 2 , 3 , 5 and 6 ) had involvement of the pulmonary interstitiuchest radiography showed pleural and interstitial thickening ( kerley b lines )  . 
chest ct demonstrated a reticular interstitial pattern , smooth septal and fissural thickening , diffuse ground - glass opacities and centrilobular nodules with subpleural , peribronchovascular radiofarmaco in corrispondenza di una vertebrale dorsale . in quattro pazienti ( caso 2 , 3 , 5 e 6 ) vi era coinvolgimento dellinterstizio polmonare . 
i radiogrammi in proiezione antero - posteriore di gamba , mettono in evidenza bilateralmente , in corrispondenza della spongiosa tibiale e peroneale , diffuse e sfumate zone di radio - opacit , cui si associano ispessimenti focali delle corticali scheletriche , in assenza di reazioni periostali . radiol med ( 2009 ) 114 : 13191329 1325 fig . 
the clinical suspicion was confirmed by a biopsy of the retroperitoneal tissue in three patients ( 1 , 3 , and 4 ) and of pulmonary tissue in the remaining three patients ( 2 , 5 , 6 )  . 
il sospetto clinico stato confermato dallindagine bioptica su tessuto retroperitoneale in 3 pazienti ( casi 1 , 3 , 4 ) e polmonare nei rimanenti 3 casi ( 2 , 5 , 6 )  . 
 discussion discussione ecd is a rare form of non - langerhans histiocytosis , the reactive or neoplastic nature of which is still being debated [ 10 , 11 ]  . 
axial ( a ) and sagittal ct ( b ; multiplanar reconstruction ) demonstrates extensive erosion of t6 vertebral body with interruption of the posterior end - plate and initial involvement of the left vertebral pedicle . 
dimostrazione tc sul piano assiale ( a ) e sagittale ( b ; mpr ) di voluminosa erosione del soma di t6 con interruzione della limitante somatica posteriore ed inizile impegno del peduncolo vertebrale di sn . 
la rm ( c ) in se t1 w dimostra lindennit del canale vertebrale . in our experience , there was a frequent correlation between a histological diagnosis of ecd and skeletal involvement . 
bone involvement is an almost constant feature of ecd , there being only one report of a case without bone lesions [ 13 ]  . ecd generally affects the long bones of the lower limbs ( tibia and fibula )  . 
the related radiographic findings are diffuse or patchy opacities of the tibia and / or fibula , medullary sclerosis and cortical thickening of the metaphyseal and diaphyseal portions without epiphyseal changes . on 99mtc scintigraphy , intense , bilateral and symmetrical tracer uptake by the long - bone diaphyses and metaphyses is revealed , reflecting increased osteoblastic activity in those regions [ 1521 ]  . 
in our series , osteosclerotic changes were seen in the metaphyseal and diaphyseal portions of the tibia and fibula in three patients ( 1 , 3 and 4 )  . 
le lesioni ossee rappresentano un aspetto pressoch costante dellecd ; viene riportato in letteratura un solo caso di ecd in cui non erano state dimostrate lesioni ossee [ 13 ]  . lecd generalmente interessa le ossa lunghe degli arti inferiori ( in particolar modo tibia e perone ) e le alterazioni radiografiche si configurano come radio - opacit diffuse o a chiazze della tibia e / o del perone , la sclerosi midollare e lispessimento corticale delle regioni metafisarie e diafisaria ; scarse invece sono le alterazioni epifisiarie [ 13 ]  . 
la scintigrafia 99mtc evidenzia intensa iperfissazione , bilaterale , simmetrica a carico delle diafisi e metafisi delle ossa lunghe , conseguente ad aumento dellattivit osteoblastica in tali sedi [ 1521 ]  . 
nei casi 2 e 6 si osservano le caratteristiche radiol med ( 2009 ) 114 : 13191329 1327 the osteosclerotic changes were seen at the femoral level . bone involvement in these patients was asymptomatic , in contrast to previous reports where > 50% of patients have mild but persistent pain of the affected bone segment , most commonly the hips and knees [ 9 ]  . only patient 4 had symptomatic bone involvement , reporting with spinal pain despite the absence of significant abnormalities on plain radiography of the spine and lower limbs . 
are the only authors to have reported cases of lytic vertebral lesions ( two cases ) , and indeed , the spine is typically spared in ecd [ 22 ]  . 
otomastoiditis , spleen and bone marrow involvement are also more frequent in lch , whereas retroperitoneal involvement of the perirenal spaces and circumferential involvement of the aorta are typical features of ecd [ 23 ]  . 
in support of the latter hypothesis , cases of ecd coexisting with lch have been reported , suggesting the possibility that the two diseases are linked by a common precursor , cd34 + [ 24 , 25 ]  . 
il coinvolgimento osseo in questi pazienti era asintomatico , a differenza dei dati riportati in letteratura , secondo i quali oltre la met dei pazienti presentano dolore lieve ma persistente , localizzato al segmento osseo colpito , prevalentemente alle anche e alle ginocchia [ 9 ]  . solo il quarto paziente presentava sintomatologia dolorosa al rachide , in assenza di significative alterazioni allindagine radiografica del rachide e degli arti inferiori ; lesame scintigrafico evidenziava iperfissazione del radiofarmaco in corrispondenza di una vertebra dorsale ; la biopsia in tale sede non risultava diagnostica per campionamento inadeguato ; il prelievo bioptico a livello polmonare consentiva la diagnosi di ecd . 
 [ 22 ] sono gli unici autori ad avere riportato casi di lesioni osteolitiche vertebrali ( 2 pazienti ) ; infatti caratteristicamente nellecd si osserva risparmio del rachide . le lesioni osteolitiche dello scheletro assiale sono pi frequenti nellistiocitosi a cellule di langerhans ( lch ) , ma generalmente , queste tendono a risparmiare le ossa lunghe . inoltre i pazienti affetti da lch sono pi giovani rispetto a quelli con ecd ed hanno una prognosi migliore , con tassi di mortalit del 30% ( versus il 57% dellecd ) [ 9 ]  . 
a favore di tale ipotesi sono stati riportati alcuni casi in cui ecd ed lch coesistono , suggerendo la possibilit che le due patologie siano legate da un comune precursore cd34 + [ 24 , 25 ]  . 
in nessuno dei nostri pazienti stato osservato esoftalmo , sebbene rappresenti una frequente presentazione neurologica di ecd , conseguente ad una infiltrazione del tessuto adiposo retroconale e della guaina del nervo ottico . 
diabete insipido ed esoftalmo sono presenti in entrambe le forme di istiocitosi , in particolare nellistiocitosi a cellule del langerhans ( lch ) rappresentano in associazione ad osteolisi la classica triade di presentazione . 
tali reperti associati a diabete insipido sono rilevabili anche nello xantoma disseminato ( xd ) che pu simulare clinicamente lecd ; tuttavia nellxd il diabete insipido di grado lieve e transitorio ( nellecd persistente e progressivo ) , i pazienti hanno et inferiore a quelli con ecd , presentano diffuse lesioni cutanee e mucose e , raramente , possono presentare lesioni osteolitiche periarticolari [ 25 ]  . nei casi 1 e 2 stato riscontrato coinvolgimento cardiaco 1328 radiol med ( 2009 ) 114 : 13191329 among the typical manifestations of ecd [ 27 ]  . 
these same patients also exhibited thoracoabdominal periaortic infiltration , which is the most common cardiovascular manifestation of ecd [ 27 ] and is referred to as a coated aorta when the entire course of the vessel aorta is surrounded by fibrosis . 
at ct , care should be taken not to confuse periaortic infiltration with the aortic wall thickening seen in takayasu arteritis , a condition characterised by involvement of the full thickness of the aortic wall and sparing of the periaortic spaces . 
the use of contrast - enhanced ct is decisive for identifying this feature at the early stages of perirenal fibrosis . displacement of the aorta and ureters by the fibrous tissue may also be seen in forms secondary to malignant diseases , as in some histological types of non - hodgkins lymphomas . these , however , will rarely show the typical bilateral and symmetrical distribution of ecd [ 28 ]  . 
the differential diagnosis of pulmonary involvement by ecd prevalently includes cardiogenic interstitial oedema , where centrilobular nodules are absent , and carcinomatous lymphangitis and sarcoidosis , where septal thickening is typically nodular [ 29 , 30 ]  . our experience suggests that a clinical presentation of bilateral hydronephrosis , persistent bone pain , diabetes insipidus and exophthalmus should raise suspicion of ecd and prompt investigation with plain radiography of the lower limbs and ct of the chest and abdomen . 
if the examination reveals the characteristic diaphyseal and metaphyseal osteosclerosis , brain mr imaging should be used to search for any pituitary microadenomas ( at times hyposecreting )  . in conclusion , ecd is a rare multiorgan disease that has heterogeneous clinical presentations and a prevalence that appears to be underestimated . 
among the possible organs con riscontro di versamento pericardico , che recentemente stato incluso tra le manifestazioni tipiche dellecd [ 27 ]  . negli stessi pazienti stata anche evidenziata la presenza di infiltrato periaortico toraco - addominale ; tra le manifestazioni cardiovascolari questa la pi frequente in corso di ecd [ 27 ] e viene indicata anche con il termine di aorta rivestita , quando lintero decorso aortico circondato da fibrosi . 
allesame tc linfiltrato periaortico non deve essere confuso con lispessimento parietale aortico presente nellarterite di takayasu ; questultima condizione infatti si caratterizza per linteressamento a tutto spessore della parete aortica con risparmio degli spazi periaortici . 
la dislocazione dellaorta e degli ureteri da parte del tessuto fibrotico pu essere riscontrata anche nelle forme secondarie a patologie maligne , come nel caso di alcuni istotipi di linfomi nonhodgkin ; tuttavia rara la distribuzione bilaterale e simmetrica propria dellecd [ 28 ]  . 
la tc torace evidenziava un pattern interstiziale di tipo reticolare con ispessimento liscio dei setti e delle scissure , diffuse aree a densit ground glass e noduli centrolobulari con distribuzione subpleurica , peribroncovasale e interlobulare . 
la diagnosi differenziale in caso di coinvolgimento polmonare include principalmente ledema interstiziale cardiogenico in cui sono assenti i noduli centrolobulari , la linfangite carcinomatosa e la sarcoidosi ove lispessimento dei setti tipicamente nodulare [ 29 , 30 ]  . la nostra esperienza suggerisce che un quadro clinico caratterizzato da idronefrosi bilaterale , dolore osseo persistente , diabete insipido , esoftalmo , pu orientare il sospetto diagnostico di ecd e giustificare lesecuzione di un esame radiografico degli arti inferiori e di una tc toracica ed addominale . 
il riscontro occasionale in ecografia , tc o rm , di fibrosi perirenale giustificano un approfondimento con rx standard degli arti inferiori ; quando a tali livelli , si documenti la caratteristica osteosclerosi diafisaria e metafisaria dellecd , consigliabile ricercare la possibile presenza di microadenomi ipofisari ( talvolta iposecernenti ) con rm dellencefalo . in conclusione , lecd una patologia multiorgano rara , con manifestazioni cliniche estremamente eterogenee , la cui radiol med ( 2009 ) 114 : 13191329 1329 involved by the disease , skeletal tissue , the retroperitoneum and , in particular , perirenal spaces , were found to be constantly involved . 
hence they require a multidisciplinary and multispecialty approach , which must begin with an accurate medical examination , conducted in compliance with the lege artis principles and with respect for the victims dignity . 
this paper describes the radiologists key role in identifying physical injuries due to child abuse , in accordance with current regulations . keywords child abuse forensic radiology battered child syndrome riassunto labuso ed il maltrattamento sui minori una tematica di grande attualit con notevoli risvolti di carattere sociosanitario che interessano il medico sia come cittadino che in qualit di esercente una professione sanitaria . 
la molteplicit e la peculiarit di alcune lesivit di abuso , siano queste di tipo fisico , psichico o sessuale necessitano di un approccio multidisciplinare e polispecialistico che non pu prescindere tuttavia da una visita medica che , nel rispetto della dignit della presunta vittima , sia effettuata secondo i criteri propri della lege artis . 
il presente articolo descrive il ruolo del radiologo nella valutazione degli abusi fisici perpetrati a danno di minori alla luce della normativa vigente . parole chiave abuso sui minori radiologia forense sindrome del bambino battuto introduction introduzione in 1946 , radiologist john caffey following a . 
this was a concise , pragmatic definition of what is not so much a clinical syndrome as a sociocultural phenomenon that had strong repercussions on trauma medicine and on physicians themselves [ 1 ]  . 
tardieu del 1860 definiva in maniera concisa e pragmatica pi che una sindrome clinica un fenomeno socio - culturale che aveva pesanti riflessi sulla medicina traumatologica e notevoli ricadute sui medici [ 1 ]  . radiol med ( 2009 ) 114 : 13561366 1357 an accurate definition of child abuse is given in the world health report 2002 : child abuse or maltreatment constitutes all forms of physical and / or emotional illtreatment , sexual abuse , neglect or negligent treatment or commercial or other exploitation , resulting in actual or potential harm to the childs health , survival , development or dignity in the context of a relationship of responsibility , trust or power [ 2 ]  . 
therefore , child abuse includes the results not only of actions ( sexual or other kinds of violence ) but also of neglect or deprivation ( lack of care , attention , affection )  . 
in both cases , the physical examination alone , for legal purposes as well as for diagnosis and therapy , is unable to confirm or exclude suspected abuse ( at least from a medical point of view ) without the use of radiological tools . 
thus , radiology is an essential tool in medicolegal investigations of physical child abuse , which gives the specialist a proper understanding of type , extent and age of the injury , and the dynamics behind it ( aetiopathogenesis )  . extent of child abuse child abuse has become a very worrying issue with an impact on the whole of society . 
introna states : the abused child is the expression of multiple problems of a legal , cultural and economic nature involving his / her family at a given moment in time , and therefore he / she is the clue to pain that goes beyond his / her own person [ 3 , 4 ] as requested . child abuse is often rejected or negated , and it is always underreported . 
this is especially true in southern italy , where it often occurs within a complex family setting , which makes it difficult to evaluate the victim and type of abuse suffered . 
the child presents distinctive injuries , often inflicted with bare hands or by using various objects ( sticks , chains , strings , cigarettes or other sources of heat )  . 
this form of child abuse results from indeuna precisa e completa definizione pu essere tradotta dalla world health organization ( who ) che nel 2002 cos recitava : per abuso allinfanzia si intendono tutte le forme di cattiva salute fisica e / o emozionale , abuso sessuale , trascuratezza o negligenza o altro che comportino un pregiudizio reale o potenziale per la salute del bambino , per la sua sopravvivenza , per il suo sviluppo o per la sua dignit nellambito di una relazione caratterizzata da responsabilit , fiducia o potere [ 2 ]  . 
in relazione a tanto , labuso sui minori deve intendersi comprensivo sia degli atti ( violenze vere e proprie , non necessariamente sessuali ) che delle carenze e le deprivazioni ( sottrazione delle cure , dellattenzione , dellaffetto )  . 
in entrambe le ipotesi laccertamento medico , effettuato a fini giuridici lindagine oltrech diagnostico - terapeutici , utilizzer radiologica quale importantissimo strumento diagnostico per fondare ovvero escludere , quanto meno da un punto di vista medico , il sospetto di un abuso . 
lutilizzo di immagini digitali , utile ad una pi fine valutazione della lesione fisica osservata e correlato ad una specifica competenza del radiologo riguardo allepoca di mineralizzazione ossea trauma ed dei segmenti scheletrici allidoneit lesiva del trauma stesso ( eziopatogenesi ) , rende la valutazione radiologica strumento fondamentale nella valutazione medico - legale degli abusi fisici a carico di minori . interessati dal dimensioni del problema il maltrattamento dei bambini ha assunto dimensioni tali da costituire un serio motivo di preoccupazione da parte di tutta la societ civile . 
introna in un suo felicissimo intervento recita : il bambino maltrattato testimone di problemi multipli che investono il nucleo familiare in quel determinato momento storico , giuridico , culturale ed economico e quindi egli la spia di una sofferenza che va oltre la sua persona [ 3 , 4 ]  . 
questo vero soprattutto nelle regioni del sud dove la complessit dellambiente familiare , in cui , nella maggior parte dei casi , avviene tale tipologia di reati , rende estremamente difficile unesatta valutazione delle vittime e del tipo di abuso subito . 
these injuries are a sign of neglect by those responsible for the childs care because the injuries were not treated promptly and eventually became chronic . this paper focuses only on the battered child syndrome because this feature directly concern radiologists . radiological features of child abuse the radiologist is consulted during the investigation of battered child injuries , especially those related to cranial and musculoskeletal injuries , and he or she must be cognizant of the often critical features of such injuries . 
later , in 1962 , kempe coined the expression battered child syndrome [ 6 ] to group together the clinical and radiological signs of beaten children and to draw attention of the medical community to the problem , which , although steadily escalating , had been totally disregarded . incomplete or complete fractures are generally observed in the upper and lower limbs and in the ribs directly struck by blows , punches or kicks whilst the child is hunched up for self protection . 
it must be pointed out that the radiologist is always able to identify an injury but can never be absolutely sure of its mechanis nevertheless , some fractures are highly specific of the battered child syndrome , i.e. 
the knee ( proximal tibia ) , the wrist , the femur and the humerus are the most frequent sites of such fractures , which are rarely accompanied by a periosteal reaction and seldom cause growth disturbances or bending deformities [ 10 , 11 ]  . 
con questo termine si vogliono comprendere tutti quei maltrattamenti occulti costituiti da mancanza di protezione , di educazione , di amore e di accettazione che si estrinsecano con una serie di trascuratezze , rifiuti e sfruttamenti che sfociano nellabbandono psicologico ma , talvolta , possono determinare il decesso della vittima per inanizione . 
oltre alle sequele psicologiche , si possono riscontrare anche dermatosi comuni croniche da scarsa igiene , ripetute infezioni , ascessi e fistole che sono indicative della trascuratezza di chi si dovrebbe prendere cura del minore ed indicare affezioni perduranti nel tempo e non curate tempestivamente . in questo articolo tratteremo esclusivamente la valutazione specialistica degli abusi fisici sui minori ( battered child syndrome ) , i cui aspetti coinvolgono in maniera diretta e pressante lo specialista radiologo . aspetti radiologici degli abusi fisici sui minori lo specialista radiologo consultato in corso di accertamenti sul bambino battuto ( abusato da un punto di vista fisico ) , prevalentemente nei casi di violenza da trauma sullapparato cranico - muscolo - scheletrico e deve conoscerne gli aspetti , a volte del tutto peculiari , con cui questi possono palesarsi . 
 gi caffey nel 1957 aveva messo in evidenza ed illustrato alcuni nuovi e particolari tipi di frattura e di lesioni ossee che si possono riscontrare nei bambini battuti , specie nei pi piccoli [ 5 ]  . 
kempe successivamente , nel 1962 , allo scopo di puntare lattenzione del mondo scientifico su un problema sociale assolutamente trascurato , ma in fase di importante espansione , coni il termine di battered child radiol med ( 2009 ) 114 : 13561366 1359 fig . 
b frattura a manico di secchio . table 1 differential diagnosis between accidental and nonaccidental injuries abusive fractures metaphysis proximal tibia femur accidental fractures epiphysis distal tibia other sites with high energy mechanism tabella 1 diagnosi differenziale tra fratture accidentali e da abuso fratture da abuso sede metafisaria tibia prossimale femore fratture accidentali epifisi tibia distale altri siti con meccanismo elevata energia the lower limbs of children who are not ambulatory ( table 1 )  . 
 the so - called toddlers fracture , namely , the spiroidal fracture of the distal portion of the tibia , is a very common accidental injury in the paediatric age . 
on the other hand , if the same fracture is detected with identical radiological features in children not yet ambulatory , it should undeniably be considered as resulting from abuse [ 1214 ]  . 
multiple syndrome per indicare tutto il corteo di sintomi clinici e radiologici che caratterizzano gli aspetti traumatici del bambino battuto [ 6 ]  . come aspetto generale le fratture incomplete o complete interessano lo scheletro appendicolare , specie gli arti superiori ed inferiori e le coste che sono oggetto della violenza soprattutto a seguito di percosse , pugni e calci a bambini rannicchiati in atteggiamento di autoprotezione . 
raro che le lesioni scheletriche siano fatali e rare sono anche le lussazioni e le lesioni vertebrali , in ogni caso opportuno ricordare che il radiologo pu identificare la lesione , ma mai determinarne con certezza le modalit . 
tuttavia esistono alcune particolarit del tipo di fratture che possono indirizzare o far propendere il radiologo verso un trauma non accidentale e quindi da riferire a sindrome da bambino battuto . 
these are caused by traumatic anteroposterior compression of the rib cage , and the radiologist must bear in mind the fact that they cannot be caused even by the use of improper resuscitation procedures [ 1518 ]  . 
as they are extremely serious injuries , they may appear to indicate abuse , but , at the same time , they are very often associated with accidents such as tumbling out of bed , falling off the changing table or down the stairs . 
8a , b frattura lineare del parietale destro nella battered child syndrome . in the case of indirect head injuries , guthkelchi [ 24 ] made a further distinction by introducing shaken baby syndrome , in which lesions are secondary to the attendant axonal damage . when the infant is shaken violently and head movements are not synchronised with the rest of the body , in 90% of cases , this produces retinal haemorrhage , but it may also produce subdural haematoma ( related to vascular tears ) and osseous injuries ( detectable only by means of magnetic resonance imaging )  . 
 we must remember the possibility , even if remote , of finding damage to parenchymal organs , which is regularly accompanied by other types of lesions ( haematoma , pseudocyst , etc . ) that will be seen only through ultrasound or computed tomography [ 26 ]  . current regulations and forensic medicine considerations the entire medical profession , including radiologists , is bound by italian law to cooperate with police authorities to prevent and combat crime . 
evidenti le lesioni ipodense cerebrali , esiti di trauma da scuotimento . deontology code ( 2006 ) states that the doctor must protect children in cases of physical or psychological maltreatment or sexual abuse , and in the event of opposition from the legal guardians , the doctor must report to the appropriate legal authorities . 
361medici specialisti in radiodiagnostica , sono previsti , dalla legislazione attualmente vigente , obblighi giuridici finalizzati a forme di collaborazione con lautorit giudiziaria , al fine di prevenire e contrastare la criminalit . 
32 del codice di deontologia medica ( 2006 ) che prevede , oltrech una specifica tutela sui minori in casi di maltrattamenti fisici o psichici , violenze o abusi sessuali anche la possibilit in caso di opposizione dei legali rappresentanti alla necessaria cura dei minori di ricorrere alla competente autorit giudiziaria . 
 doveroso ricordare che la violazione del dovere o omissione di inoltrare il referto / rapporto costituisce un delitto contro lamministrazione della giustizia ; la mancata ottemperanza di tale dovere prevede automaticamente il reato di omissione datti dufficio qualora si accerti che il sanitario abbia , con coscienza e volont , voluto omettere o ritardare la presentazione del referto [ 28 ]  . 
failure to comply with this duty is malfeasance in office when it is ascertained that the health professional wilfully and knowingly failed to report or delayed reporting the crime [ 28 ]  . 
 conclusions too often do we hear about presumed physical , psychological or sexual child abuse based on psychological evaluations without any reference to the medical follow - up or specialistic investigations that could unequivocally confirm or exclude this suspicion . 
in fact , they have the knowledge to determine the time of mineralisation of skeletal segments , reconstruct the mechanisms of injuries to the osteoarticular system and interpret imaging findings . reporting child abuse is always a very delicate question , especially because it always involves the families . 
although a mere suspicion of abuse is sufficient for current regulations , the professional must be aware of the consequences of a misdiagnosis on the family and on the victitherefore , the radiologist is required to make both a cultural effort in understanding the problem and a methodological effort in evaluating the case in terms of collecting a complete clinical history and carefully interpreting the imaging findings . implementation of guidelines and protocols such as those proposed by the american college of radiology [ 29 ] , together with cooperation between several specialists , will help produce a methodologically flawless evaluation of the true extent of this serious problem , which has been neglected and underreported for too long . 
la particolare complessit della fenomenologia di abuso sui minori necessita , ai fini di un corretto inquadramento del fenomeno stesso , di un approccio multidisciplinare da parte di una equipe di specialisti , laddove di fondamentale importanza appare il contributo del radiologo pediatrico . 
linterpretazione delle lesioni eventualmente riscontrate con limaging non pu essere di pertinenza del pediatra ovvero dellortopedico ; solo il radiologo ha le competenze per discernere laddove possibile caratteristiche proprie di un trauma accidentale oppure di un abuso . 
infatti , la conoscenza della mineralizzazione ( epoca di ossificazione ) dei segmenti scheletrici , dei meccanismi traumatici che sottendono la genesi di lesivit soprattutto dellapparato osteo - articolare nonch la loro interpretazione diagnostica , di pertinenza del radiologo che ne certamente lunico e il migliore conoscitore . 
se da un lato la normativa vigente prevede che sia sufficiente il sospetto e non la certezza , per denunciare siffatto reato altres chiaro che una erronea diagnosi di abuso pu sconvolgere un nucleo familiare , ivi inclusa la vittima . 
allo specialista in radiodiagnostica richiesto pertanto uno sforzo culturale nei termini di comprensione / conoscenza del problema e metodologico nella valutazione di tale fenomeno che non potr prescindere dalla raccolta di un completo raccordo anamnestico , oltrech dalla successiva analisi dellimaging . 
bergamaschi1 1istituto di medicina del lavoro delluniversit cattolica del sacro cuore , largo gemelli 8 , 00168 roma , italy 2istituto nazionale di riposo e cura dellanziano ( inrca ) , u.o. 
le donne radiologo sono meno soddisfatte degli uomini per quanto riguarda i riconoscimenti per il lavoro ben fatto , la variet del lavoro , la distribuzione dei carichi di lavoro . 
appare realizzabile una indagine trasversale a campione multistratificato . parole chiave soddisfazione lavoro radiologo stress radiol med ( 2009 ) 114 : 13301344 introduction introduzione 1331 the scientific literature has reported increasing numbers of studies on job satisfaction among physicians [ 16 ] in that this measure it closely related to physical and psychological well - being , work - related choices and the quality of care delivered [ 7 , 8 ]  . 
 this pilot study aimed to investigate the professional satisfaction of italian radiologists and evaluate the feasibility of extending the investigation to the national level . materials and methods physicians attending two congresses of radiology and radiation oncology were invited to complete an anonymous questionnaire exploring the level of work stress , physical and psychological well - being and other factors potentially associated with medical error . 
in consideration of the findings of previous studies [ 11 , 12 ] , in the italian version , we included an additional item on equity of workload distribution , which was not present in the original version . 
surveys of physicians working in private practice have generally used a short form of the questionnaire , that is , excluding items concerning satisfaction with relationships with superiors or management . 
solo pochi studi hanno affrontato il tema della soddisfazione professionale dei radiologi . il presente studio - pilota il primo condotto nel nostro paese sulla soddisfazione professionale dei medici radiologi e mira , tra laltro , a valutare la fattibilit di una indagine estesa a tutto lambito nazionale . materiali e metodi i medici specialisti partecipanti a due congressi di radiologia e di radioterapia oncologica sono stati invitati a compilare un questionario anonimo , che indagava il livello di tensione lavorativa , il benessere psicofisico ed altri fattori potenzialmente associati allerrore medico . 
la scala di warr consta di 15 domande , a ciascuna delle quali si pu rispondere , secondo una scala likert in 7 punti , che va da estremamente insoddisfatto ( 1 punto ) a estremamente soddisfatto ( 7 punti )  . 
sulla base di studi precedenti [ 11 , 12 ] nella versione italiana stata aggiunta una domanda , relativa allequit nella ripartizione dei compiti di lavoro , che non figura nella versione originale . 
nelle ricerche condotte su medici liberi professionisti il questionario stato generalmente impiegato in forma breve , escludendo le domande riguardanti la 1332 radiol med ( 2009 ) 114 : 13301344 fig . 
job satisfaction scale ( jss ) [ 10 ] , italian version . what is your level of satisfaction with your job ? to complete the questionnaire , mark the number corresponding to one of the following levels of satisfaction in the box next to each question : 1 im extremely dissatisfied 2 im very dissatisfied 3 im moderately dissatisfied 4 im not sure 5 im moderately satisfied 6 im very satisfied 7 im extremely satisfied ( - ) satisfaction how satisfied are you with... w1 the physical work conditions w2 the freedom to choose your own method of working w3 your fellow workers w4 the recognition you get for good work w5 your immediate boss w6 the amount of responsibility you are given w7 your rate of pay w8 your opportunity to use your abilities w9 relations between management and workers w10 your chance of promotion w11 the way your company is managed w12 the attention paid to suggestions you make w13 your hours of work w14 the amount of variety in your job w15 your job security w16 distribution of workloads w17 now , taking everything into consideration , how do you feel about your job as a whole ? fig . 
1 questionario jss ( job satisfaction scale ) di warr et al [ 10 ] , versione italiana . quale il tuo livello di soddisfazione dal lavoro ? per rispondere al questionario , occorre segnare accanto a ciascuna domanda , nellapposita casella , il numero che corrisponde ad uno dei seguenti livelli di soddisfazione : 1 ono estremamente insoddisfatto 2 sono molto insoddisfatto 3 sono moderatamente insoddisfatto 4 sono incerto 5 sono moderatamente soddisfatto 6 sono molto soddisfatto 7 sono estremamente soddisfatto ( - ) soddisfazione quanto ti soddisfa... w1 lambiente di lavoro w3 i compagni di lavoro w5 il superiore w2 la libert di scegliere da s il proprio metodo di lavoro w4 i riconoscimenti che si ricevono per il lavoro ben fatto w6 linsieme delle responsabilit che ti vengono date w7 il guadagno economico w8 la possibilit di usare le proprie capacit professionali w9 le relazioni tra lamministrazione ed i lavoratori w10 le tue possibilit di promozione e carriera w11 il modo in cui lazienda in cui lavori diretta w12 lattenzione rivolta ai suggerimenti che fai w13 lorario di lavoro w14 la variet nel lavoro w15 la sicurezza dellimpiego w16 la ripartizione dei carichi di lavoro w17 ora , prendendo in considerazione tutte queste cose , quale il livello di soddisfazione che ricavi dal lavoro nel suo insieme ? radiol med ( 2009 ) 114 : 13301344 1333 a total of 314 physicians were interviewed , of whom 108 were radiotherapists and 206 radiologists . 
because the group of radiotherapists did not differ significantly from that of radiologists in terms of demographics ( sex , age ) or work - related variables ( experience , position , public or private sector ) , all data were pooled for the analysis . 
the subjects were predominantly men [ 251 men , ( 79.9% ) and 63 women ] , and nearly all of them worked in the public sector [ 289 physicians ( > 92% ) ]  . 
among those employed by the italian national health service ( nhs ) , 20% were heads of department ( n = 59 ) , > 19% were division heads ( n = 56 ) and the remainder were staff - grade consultants ( n = 174 ; 61% )  . 
as controls , we used a group of 34 specialists in infectious diseases , all of whom were hospital employees , who were invited to complete the same questionnaire on the occasion of their periodical medical check - up . 
the control group did not differ significantly from the group of radiologists in terms of age and sex . data were analysed using the statistical package for social science , version 11.5. 
this test measures the correlation between variables of single items in the scale , and the closer it is to a value of 1.0 , the higher the scales internal consistency . 
binomial logistic regression with backward stepwise selection was used to evaluate which of the many variables investigated were more directly correlated to physician satisfaction or dissatisfaction . results questionnaire validation the italian version of the satisfaction scale maintains the unitary nature of the original version by warr et al . 
this component correlated with all of the 17 items , with greater weight ( 0.810 ) attributed to the last item , which elicits a judgement on satisfaction derived from the job as a whole considering all the soddisfazione dei rapporti con i superiori o il management . la versione breve formata dalle domande 1 , 2 , 3 , 4 , 6 , 7 , 8 , 13 , 14 e dellultima , riassuntiva . 
nel nostro studio abbiamo preferito impiegare la versione estesa , in considerazione del fatto che gli intervistati operavano prevalentemente in condizioni di lavoro subordinato . sono stati intervistati 314 medici , di cui 108 specialisti in radioterapia e 206 specialisti in radiologia . 
il gruppo dei radioterapisti non presentava differenze significative rispetto a quello dei radiologi per nessuna delle variabili anagrafiche ( genere , et ) n per quelle legate al lavoro ( esperienza , ruolo , attivit nel settore pubblico o privato )  . 
i soggetti esaminati risultavano prevalentemente di sesso maschile ( 251 maschi , pari al 79 , 9% , 63 femmine ) , e quasi tutti operanti nel settore pubblico ( 289 , oltre il 92% )  . 
i medici dipendenti del sistema sanitario nazionale ( ssn ) erano nel 20% dei casi direttori di unit operativa ( 59 unit ) , in oltre il 19% dei casi responsabili di struttura semplice ( 56 unit ) , per il rimanente dirigenti medici ( 174 unit , 61% )  . 
la classe di et pi frequente risultata quella compresa tra 46 e 50 anni ( 27 , 7% ) , la categoria di esperienza lavorativa pi frequente quella superiore a 26 anni ( 22 , 6% )  . 
come controllo esterno stato impiegato un gruppo di 34 specialisti in malattie infettive , dipendenti ospedalieri , che sono stati invitati a compilare lo stesso questionario in occasione della visita medica periodica . 
il gruppo di controllo non differisce significativamente per et e sesso dai radiologi . i dati sono stati analizzati mediante il software statistico statistical package for social science ( spss ) , versione 11.5. 
convenzionalmente un valore di alfa pari a 0 , 60 ritenuto accettabile , un valore di 0 , 70 adeguato , un valore di 0 , 80 buono . lanalisi fattoriale stata impiegata per conoscere la struttura latente del set di variabili composto dalle domande del jss , riducendo linsieme delle variabili ad un ristretto gruppo di fattori omogenei e dotati di coerenza logica . 
le tabelle di contingenza sono state testate con il test del chi quadro di pearson , per verificare lipotesi zero di mancanza di associazione tra righe e colonne nei dati tabulati . 
per valutare quali , tra le numerose variabili indagate , risultassero pi direttamente legate alla soddisfazione o insoddisfazione dei medici , stata impiegata la regressione logistica binomiale , con selezione condizionale a ritroso ( backward stepwise )  . table 1 factor analysis : component matrix obtained using the extraction method . 
cronbachs coefficient is based on the correlation between the items in the scale and may be interpreted as the percentage of variance accounted for by the scale with respect to universal variance ; in other words , the correlation between the scale used and all possible other scales in the entire romain made up of the same number of items . 
the value found indicates that the jss is highly reliable for evaluating satisfaction . job satisfaction responses to the last item on the jss indicate that 49% of radiologists were satisfied to varying extents with their job . the proportion of satisfied radiotherapists was significantly higher ( 64% ) , as was that of infectious disease specialists ( 62% ) ( table 3 )  . 
analysis of responses to each item on the questionnaire better illustrates the differences among the groups of professionals ( table 4 )  . the differences between radiologists and radiotherapists in the mean scores for each item were statistically risultati validazione del questionario la scala di soddisfazione conserva , anche nella versione italiana , il carattere unitario della versione originale di warr et al . 
questa componente correlata a tutte le 17 domande , con il maggiore peso ( 0 , 810 ) attribuito allultima domanda , che appunto chiede di specificare la soddisfazione complessivamente tratta dal lavoro , tenendo conto di tutti i fattori indagati dalle domande precedenti . 
applicando nellanalisi fattoriale la rotazione obliqua varimax in modo da massimizzare la differenza tra le due componenti ( tabella 2 ) , si osserva che la prima componente riguarda soprattutto motivi di soddisfazione legati al soggetto e allambiente in cui lavora , mentre la seconda , correlata alle domande 9 , 10 , 11 , 12 e , in minor misura , 4 , 5 , 7 , 16 , si riferisce ai rapporti con la struttura in cui lavora . la consistenza interna del questionario jss , misurata mediante il coefficiente alfa di cronbach , molto elevata ( 0 , 9457 )  . 
il coefficiente di cronbach , basato sulla correlazione tra le domande , pu essere interpretato come la percentuale di varianza che la scala usata pu spiegare rispetto alla varianza universale , ovvero la correlazione tra la scala usata e tutte le possibili altre scale delluniverso composte da un analogo numero di domande . 
differences in satisfaction with physical working conditions , freedom to choose work method , lultima domanda del jss indica che il 49% dei radiologi soddisfatto , in misura maggiore o minore , del proprio lavoro ; tra i radioterapisti la percentuale di soddisfatti significativamente pi alta ( 64% ) e cos tra gli infettivologi ( 62% ) ( tabella 3 )  . 
se si analizzano le risposte fornite in corrispondenza di ciascuna delle domande del questionario , la differenza fra le categorie professionali viene meglio precisata ( tabella 4 )  . le differenze tra radiodiagnosti e radioterapisti nei punteggi medi riportati in ciascuna delle domande sono statisticamente significative ( p < 0 , 05 mediante il test t di student ) per quasi tutte le domande ; risultano sovrapponibili solo le risposte relative ai rapporti con colleghi e collaboratori , mentre approssimano la significativit senza raggiungerla le domande sulle possibilit di carriera e sulla variet del lavoro . 
risulta altamente significativa ( p < 0 , 01 ) la differenza di soddisfazione per le caratteristiche dellambiente di lavoro , per la discrezionalit nei metodi di lavoro , per le responsabilit affidate , per i rapporti con il direttore e con il management , per la stabilit del posto di lavoro . 
altamente significativa la differenza di punteggio per ( misurata dallultima domanda ) e per le scale di soddisfazione intrinseca , estrinseca e globale che si ottengono sommando i punteggi delle singole domande . 
 la soddisfazione globale nel confronto con gli infettivologi ospedalieri , i radiologi addetti alla diagnostica per immagini esprimono livelli sovrapponibili di soddisfazione ( o di insoddisfazione ) solo per quanto riguarda la libert di scegliere da s il metodo di lavoro , i riconoscimenti per il lavoro ben fatto , le possibilit di carriera . 
essi sono significativamente meno soddisfatti per tutte le altre variabili , e la differenza risulta altamente significativa ( p < 0 , 01 ) per lambiente di lavoro , le responsabilit , il guadagno economico , il modo in cui gestita lazienda , lattenzione rivolta ai propri suggerimenti , gli orari di lavoro , la variet dei compiti professionali e la stabilit del posto di lavoro , oltre che per la soddisfazione complessiva indicata dallultima domanda e per le scale combinate di soddisfazione intrinseca , estrinseca e totale . tra i medici radiologi e radioterapisti di genere femminile si osserva una maggiore prevalenza di insoddisfatti che tra i maschi ( tabella 5 ) , ma la differenza non raggiunge significativit statistica ( chi quadro = 0 , 073 )  . 
se per si effettua il confronto dei punteggi medi di ciascuna domanda si evidenziano alcune significative differenze , con le donne meno soddisfatte dei colleghi maschi per quanto riguarda i riconoscimenti per il lavoro compiuto ( p = 0 , 034 ) , la ripartizione dei carichi di lavoro ( p = 0 , 011 ) e la variet del lavoro ( p = 0 , 047 )  . 
likewise , the difference in scores for overall satisfaction ( measured by the last question ) and the scales of intrinsic , extrinsic and total satisfaction obtained by adding up the scores on the single items were also statistically significant . 
 compared with infectious disease specialists , diagnostic radiologists reported similar levels of satisfaction ( or dissatisfaction ) only as regards freedom to choose work method , recognition for good work and career prospects . 
 the prevalence of subjects satisfied with their job did not vary consistently across the various age groups ; the greatest frequency of dissatisfied professionals was recorded among pi basso che negli uomini ( p = 0 , 028 ) , anche se le risposte allultima domanda , sulla soddisfazione complessiva , non differiscono nei due sessi ( p = 0 , 110 )  . 
 la prevalenza di soggetti soddisfatti dal lavoro non varia nelle diverse classi di et con un andamento univoco ; la maggiore frequenza di soggetti insoddisfatti si registra nelle et di mezzo , tra 41 e 50 anni ( tabella 6 )  . 
appare invece chiara la maggiore soddisfazione del lavoro man mano che si procede dalle categorie di lavoro precario ai dirigenti medici , ai responsabili di struttura semplice , alla figure apicali ( tabella 7 )  . 
non si osserva alcuna differenza nei livelli medi di soddisfazione in funzione del tipo di struttura pubblica o privata in cui lattivit viene esercitata ( p = 0 , 427 )  . applicando il metodo della regressione logistica con selezione condizionale a ritroso ai dati relativi a tutti i medici intervistati ( tabella 8 ) si osserva che le variabili maggiormente associate con la soddisfazione sono : lambiente di lavoro , il superiore , lattenzione rivolta ai propri suggerimenti , la libert di scegliere da s il proprio metodo di lavoro , la variet del lavoro . 
il metodo di selezione stepwise finalizzato ad escludere le variabili meno significative , fino a determinare il set di variabili che pi efficacemente determinano leffetto finale , in questo caso la soddisfazione professionale . 
on the other hand , there was a clear trend towards greater satisfaction among physicians in the higher ranks of the hierarchy from temporary staff , to staff grade , to division heads and heads of department ( table 7 )  . 
numerosi studi hanno valutato i livelli di soddisfazione nei medici di medicina generale o di varie specialit e le relazioni con il contesto organizzativo , sociale e culturale della professione [ 16 ]  . 
the position held within the organisation was the last variable to be excluded by the statistical process and was thus the variable that correlated most closely among those excluded . risultati di tali studi non possono essere estrapolati direttamente alla radiologia , in quanto questa differisce sostanzialmente dalle altre specialit mediche , in primo luogo per le modalit di interazione con i pazienti , poi per il contesto organizzativo e relazionale , infine per la rapidit dellevoluzione tecnologica . 
 stata proprio lintroduzione di nuove tecnologie a motivare recentemente la pubblicazione di una serie di lavori , secondo i quali la modificazione dellambiente e dellorganizzazione di lavoro indurrebbero un aumento della soddisfazione professionale dei radiologi [ 1316 ]  . curiosamente , i livelli di soddisfazione dei radiologi non sono stati misurati a priori in nessuno di tali studi , ma sono stati indagati anamnesticamente solo dopo lintroduzione del miglioramento tecnologico . radiol med ( 2009 ) 114 : 13301344 1339 table 7 rate of professional satisfaction as a function of role ( excluding subject reporting uncertainty ) tabella 7 andamento della soddisfazione professionale in funzione del ruolo ( esclusi gli incerti )  . 
the results of these studies cannot be directly extrapolated to radiology , as the discipline differs sono pochi gli studi che affrontano specificamente il tema della soddisfazione professionale dei radiologi , e i risultati paiono talora contraddittori . 
nel regno unito unindagine trasversale condotta nei primi anni 90 su 214 radiologi e altri tre gruppi di consulenti ospedalieri , al fine di valutare lincidenza dello stress e dei disturbi ad esso correlato , ha stimato che il 27% dei consulenti presenta affezioni psichiatriche , senza significative differenze tra le varie specialit , ed ha dimostrato che la soddisfazione professionale ha un effetto protettivo sullo stress e 1340 radiol med ( 2009 ) 114 : 13301344 substantially from other medical specialties in terms of interaction with patients , organisational and relational context and the speed of technological evolution . 
 indeed , it was the introduction of new technologies that recently prompted the publication of a series of papers that maintained that the changes to the physical work setting and organisation would increase job satisfaction among radiologists [ 1316 ]  . 
oddly , the level of satisfaction of radiologists was not measured a priori in any of these studies , but only investigated historically after the introduction of the technological improvements . few studies have specifically addressed the issue of job satisfaction among radiologists , and the results appear somewhat conflicting . 
a cross - sectional survey conducted in the uk in the early 1990s to investigate stress and associated disturbances in 214 radiologists and three other groups of hospital consultants estimated that 27% of consultants had some psychiatric morbidity , without significant differences between the various specialist groups , and demonstrated that job satisfaction has some protective effect against stress and burnout [ 7 ]  . 
 the alarming tone of this study is apparently countered by the findings of a survey conducted in poland , where 80% of radiologists reported being satisfied with the clinical relevance of their specialty , meaningfulness of their job and appreciation shown by superiors and colleagues [ 18 ]  . however , the same 70 radiologists also reported suffering from work - related stress due to low salaries , haste , lack of clinical data about patients and fear of misdiagnoses , leading the authors to conclude that radiologists are at a high risk of burnout . 
the lack of homogeneity between the questionnaires , as well as methodology and objectives of the two studies , make it impossible to establish whether the inconsistent findings are the reflection of completely different situations or the result of different interpretations of a complex and multifaceted data set . 
 this difficulty in correctly interpreting results because of methodological differences is present in the series of north american papers by sunshines team [ 1923 ] who interpreted the data provided by the periodical stratified sample surveys conducted by the american college of radiology ( acr ) on a large number of specialists . 
these surveys , in fact , do not investigate professional satisfaction explicitly , so the authors have to estimate current satisfaction in two ways : ( a ) as a positive reply as to a question on whether sullesaurimento emozionale [ 7 ]  . 
il principale fattore di insoddisfazione per i radiologi risultato leccessivo carico di lavoro , seguito dalla carenza di personale e di fondi nel sistema sanitario , e dalle richieste incongrue poste dai clinici al radiologo . 
 al tono allarmante di questo studio si contrappone apparentemente il risultato dellindagine condotta in polonia , dove l80% dei radiologi si dichiara soddisfatto del lavoro , a causa del rilievo clinico della disciplina , della significativit del compito professionale , dellapprezzamento da parte di superiori e colleghi [ 18 ]  . 
da notare per che lo stesso gruppo di 70 radiologi polacchi segnala di subire stress professionale per le retribuzioni basse , i ritmi eccessivi , la mancanza di dati clinici relativi ai pazienti e la paura di denunce per gli errori diagnostici , per cui gli autori concludono che i radiologi sono ad elevato rischio di burn - out . 
la disomogeneit degli strumenti usati , della metodologia e delle finalit strategiche dei due lavori , rende impossibile stabilire se i quadri descritti corrispondano a situazioni diametralmente opposte o se derivino da differenti interpretazioni di un insieme complesso e variegato . 
 la difficolt di prescindere da vincoli metodologici che spesso limitano la possibilit di interpretare correttamente i risultati presente nella serie di pubblicazioni statunitensi del gruppo di sunshine [ 1923 ] che interpretano i dati forniti dalle periodiche indagini a campione multi - strato condotte dallamerican college of radiology ( acr ) su un consistente numero di specialisti . 
a prescindere da una valutazione del costrutto , che soprattutto per il secondo criterio questionabile ( si pu avere unottima opinione della disciplina e del lavoro in genere , pur avendo una pessima esperienza personale ) , si deve notare che entrambe le domande sono molto indirette , il che pone dubbi sulla loro sensibilit e specificit . 
di fatto , emerge dal confronto delle successive pubblicazioni che le percentuali di soggetti classificabili come soddisfatti professionalmente divergono sostanzialmente , a seconda che si adotti luno o laltro criterio . 
il primo criterio ha radiol med ( 2009 ) 114 : 13301344 1341 respondents would recommend a career in medicine to a college - age adult , combined with a positive reply as to whether they would recommend a specialisation in radiology ; ( b ) as a positive reply to the question bearing in mind all aspects of your work , what do you think of radiology as a profession ? apart from evaluating the validity of the construct , which is questionable especially with regard to the second criterion ( one may have an excellent opinion of the discipline and job in general but a very bad personal experience ) , it should be noted that both questions are extremely indirect , which raises doubts as to their sensitivity and specificity . 
using both criteria , the level of satisfaction of north american radiologists appears to be declining . a second measure was derived from the acr survey , called dynamic satisfaction and was based on a single question with five possible replies , which measured respondents level of satisfaction relative to the past ( compared to 5 years ago , what is your feeling about working as a radiologist ? )  . 
the studies conducted on the basis of the 1995 survey identified professional qualification and improved physical working conditions as causes of increased satisfaction , whereas the main source of decreased satisfaction , which mainly referred to men and the 4554 age group , was uncertainty due to reorganisation of the health system [ 21 , 22 ]  . 
the study based on the 2003 data , as well as confirming that satisfaction was increasing among women and young individuals and decreasing among men aged 4554 years , associated reduced satisfaction with excessive workloads [ 23 ]  . 
surprisingly , this last survey revealed no correlation between radiological subspecialty and level of satisfaction [ 23 ] , whereas previous surveys found satisfaction to be significantly higher among nuclear medicine physicians and radiation oncologists than among general diagnostic radiologists [ 20 ]  . as the authors admit , the question exploring dynamic satisfaction contains an evident recall bias , as it is imposto objectively evaluate ones current feelings sible compared to ones feelings five years ago . 
when reading the numerous studies published by north american authors one cannot but admire the expertise in statistical analysis , fornito tassi di soddisfazione che oscillano dal 42% della prima indagine del 1988 , al 65% del 1990 , al 51% del 1995 ; sulla base del secondo criterio sono stati descritti livelli di soddisfazione che vanno dal 97% dei primi sondaggi al 93% del 2003 [ 1923 ]  . 
 dallinchiesta dellacr stata ricavata una seconda grandezza , denominata soddisfazione dinamica , sulla base di una singola domanda con risposta prefissata in 5 punti , che pi propriamente misura il gradimento dellattivit di radiologo rispetto al passato ( compared to 5 years ago , what is your feeling about working as a radiologist ? )  . da questa variabile , ricavato il maggior numero di informazioni . 
gli studi condotti sulla base dellinchiesta del 95 identificano come cause di aumentata soddisfazione la qualificazione professionale e il miglioramento dellambiente di lavoro , mentre la ridotta soddisfazione , che riguarda soprattutto i maschi e la fascia di et tra 45 e 54 anni , sarebbe da ricondurre alle incertezze per la riorganizzazione del sistema sanitario [ 21 , 22 ]  . 
lo studio dei dati raccolti nel 2003 , oltre a confermare che la soddisfazione in aumento nelle donne e nei giovani , mentre in diminuzione per i maschi tra 45 e 54 anni , associa la riduzione della soddisfazione con leccessivo carico di lavoro [ 23 ]  . 
sorprendentemente , in questultima inchiesta non si rileva alcuna relazione tra la specialit radiologica praticata e il livello di soddisfazione [ 23 ] , mentre nelle analisi precedenti la soddisfazione negli specialisti in medicina nucleare e radioterapia era significativamente maggiore che nei radiodiagnosti generalisti [ 20 ]  . come riconoscono gli stessi ricercatori , la domanda su cui si basa la valutazione della soddisfazione dinamica negli studi statunitensi contiene un evidente recall bias , errore sistematico di richiamo , perch impossibile valutare oggettivamente le proprie sensazioni attuali a confronto con quelle che erano le proprie sensazioni cinque anni addietro . 
leggendo i numerosi studi pubblicati dagli autori statunitensi non si pu che rimanere ammirati dalla perizia di analisi statistica , mortificata purtroppo dallinconsistenza dei dati su cui poggia lanalisi . come riconoscono gli stessi autori , misurare il concetto di soddisfazione tratta dal lavoro intrinsecamente difficile , cos come lo cercare di stabilire un preciso nesso tra la soddisfazione da lavoro e levolversi del contesto professionale [ 22 ]  . 
le percezioni sono molto pi 1342 radiol med ( 2009 ) 114 : 13301344 which is , however , undermined by the quality of the data used for the analysis . as acknowledged by the authors , it is intrinsically difficult to measure the concept of job satisfaction , just as it is to try to establish a clear link between job satisfaction and a changing professional context [ 22 ]  . 
the fact that data are based on radiologists perceptions , memory of perceptions and willingness to report them is clearly a limitation . perceptions are far more variable than factual data , and they may change rapidly and be reported inconsistently by the same radiologist at two different times . 
the concept of satisfaction , derived from a single question , oversimplifies a very complex issue and excludes , in the north american surveys , other important factors such as pay , family environment and relationships with fellow workers [ 22 ]  . professional satisfaction has been investigated by clinical psychologists since the 1930 using different methods based on one question or an aggregate of questions . 
the many questionnaires proposed over the years tended to contain redundant and overlapping items , were often long and cumbersome and tended to confuse descriptive and evaluative judgements [ 10 ]  . 
 [ 10 ] designed the jss , which rapidly imposed itself as the most reliable instrument for measuring job satisfaction . our study demonstrates that a nonnegligible proportion of specialists in our sample was not satisfied with their job : one radiologist in four and one radiotherapist in five were professionally dissatisfied . 
less than half of those who worked in diagnostic imaging were satisfied with their job . this finding , which is important in itself , is even more striking if we consider that professional satisfaction has a strong negative correlation with occupational stress and a positive correlation with psychological well - being and healthy life style [ 8 ]  . the least satisfied professionals were the general diagnostic radiologists , especially if they were on the lower rungs of the hierarchical ladder , middle aged or women . even with the difficulties in comparing our data with the situation in north america because of methodological differences , italian radiologists appear to have lower levels of professional satisfaction compared with their north american colleagues . 
several factors relating to work organisation ; quality of interpersonal relations with peers , superiors and subordinates ; material and especially immaterial rewards for work done ; and fairness in workload distribution all affect the level of job satisfaction of italian radiologists significantly and in many cases negatively . 
if the differences in satisfaction among the various age groups and hierarchical levels can be ascribed to career progression and its consequences ; the differences between the sexes are explained by persisting discrimination towards female radiologists , who feel they receive less recognition for their variabili dei dati fattuali , possono cambiare rapidamente nel tempo ed essere riportate in modo molto diverso dallo stesso radiologo in due momenti diversi . 
il concetto di soddisfazione , ricavato da una sola domanda , semplifica eccessivamente un concetto molto complesso escludendo , nelle indagini americane , altri importanti concetti come la retribuzione , linterazione con il contesto familiare , le relazioni con i colleghi [ 22 ]  . la soddisfazione professionale stata indagata dagli psicologi clinici fin dagli anni 30 con diversi metodi , basati su una singola domanda , ma pi spesso su un aggregato di pi domande . 
i numerosi questionari proposti negli anni tendevano a contenere domande ridondanti e parzialmente sovrapponibili , erano spesso lunghi e complessi , tendevano a confondere giudizi descrittivi e valutativi [ 10 ] ; per ovviare a tali carenze il gruppo di warr et al . 
ha elaborato il jss , che si rapidamente imposto come lo strumento pi affidabile per misurare la soddisfazione da lavoro . la nostra indagine dimostra che una quota non trascurabile dei medici intervistati non soddisfatta del proprio lavoro : un radiodiagnosta su quattro e un radioterapista su cinque sono professionalmente insoddisfatti . 
questo risultato , di per s non trascurabile , assume maggiore rilievo se si considera che la soddisfazione professionale risulta significativamente associata , in senso inverso , con lo stress da lavoro , e si correla positivamente al livello di benessere psicologico e ad uno stile di vita sano [ 8 ]  . allinterno della categoria , i pi insoddisfatti risultano coloro che si dedicano alla diagnostica per immagini , soprattutto se occupano un livello basso nella scala gerarchica , sono di mezza et e di sesso femminile . 
pur considerando la difficolt di confrontare i dati da noi raccolti con la situazione statunitense , per le evidenti differenze metodologiche , sembra che i radiologi italiani presentino un livello di soddisfazione professionale inferiore rispetto ai colleghi doltre oceano . 
numerosi fattori legati allorganizzazione del lavoro , alla qualit dei rapporti interpersonali in senso orizzontale e verticale , alle ricompense materiali e soprattutto immateriali per il lavoro compiuto , allequit organizzativa del lavoro , influenzano significativamente , e spesso in senso negativo , il livello di soddisfazione professionale dei radiologi italiani . 
se le differenze nei livelli di soddisfazione tra le varie classi di et e tra diversi livelli gerarchici sembrano da attribuire in primo luogo allevoluzione della carriera e a tutte le sue conseguenze , le differenze tra i due generi sono spiegabili dal persistere di condizioni discriminatorie per le dottoresse , che sentono di ottenere meno riconoscimenti per il lavoro compiuto e di subire una ripartizione ingiusta dei carichi di lavoro , con una maggior quota di lavori ripetitivi . i fattori che maggiormente risultano capaci di determiradiol med ( 2009 ) 114 : 13301344 1343 work and suffer an unfair distribution of workloads , with a greater share of repetitive work . the factors that most affect the professional satisfaction of physicians are in part related to the physical working conditions and in part to human aspects , such as relationship with ones superior , freedom to choose ones work method , attention to ones suggestions and amount of job variety . our analysis , conducted with a sensitive instrument ( the jss ) , confirmed the role of organisational factors and work climate as the main determinants of professional satisfaction , along with improvements in physical working conditions , machines and diagnostic and care facilities . 
even with the difficulties in comparing our findings with the north american studies , it is interesting to note that environmental and organisational factors are closely related to professional satisfaction in the north american surveys , as well . our data inevitably suffer from a lack of sampling , which makes it impossible to extrapolate results to all italian radiologists . 
the interest of the findings of this initial analysis and the samples willingness to participate in the survey lead us to believe that extension of the study to the whole professional category would be well received and would provide highly relevant data for planning the development of the profession . 
increasing the data set of information would enable us to identify corrective actions capable of improving the professional satisfaction of radiologists . nare la soddisfazione professionale nei medici sono in parte collegati allambiente di lavoro fisico , in parte invece derivano da aspetti umani , come il rapporto con il superiore , la libert di scegliere da s il proprio metodo di lavoro , laccoglienza dei suggerimenti avanzati , la variet dei compiti . 
la nostra analisi , condotta con uno strumento sensibile come il jss , conferma il ruolo dei fattori organizzativi e del clima lavorativo come principali determinanti della soddisfazione professionale , accanto al miglioramento dellambiente fisico , delle macchine e delle strutture diagnostiche e terapeutiche . 
pur ribadendo la difficolt di effettuare confronti tra le nostre osservazioni e le ricerche statunitensi , interessante rilevare che una stretta relazione tra fattori ambientali e organizzativi e la soddisfazione professionale emerge anche dalle indagini americane . i dati da noi raccolti soffrono inevitabilmente della mancanza di un campionamento , il che impedisce di estrapolare i risultati alluniverso dei radiologi italiani . 
linteresse dei dati emersi da questa prima analisi e la disponibilit manifestata dai partecipanti allindagine ci inducono a ritenere che una estensione della ricerca a tutta la categoria sarebbe bene accetta e fornirebbe dati di sicuro interesse ai fini della programmazione dellevoluzione della professione . 
guglielmi2 , 3 1sezione dipartimentale di medicina legale , universit degli studi di foggia , ospedale colonnello davanzo , via degli aviatori 1 , 71100 foggia , italy 2dipartimento di diagnostica per immagini , universit degli studi di foggia , azienda ospedaliero - universitaria ospedali riuniti , viale luigi pinto 1 , 71100 foggia , italy 3dipartimento di radiologia , ospedale irccs casa sollievo della sofferenza , viale cappuccini 1 , san giovanni rotondo , 71013 foggia , italy correspondence to : g . 
mri , in addition , is also well suited to the examination of surviving victims of assault , especially choking , and helps visualise internal injuries sometimes not seen on external examination of the victivarious postprocessing techniques can provide strong forensic evidence for use in legal proceedings . 
the documentation and analysis of postmortem findings with msct and mri and postprocessing techniques ( virtopsy ) is investigator independent , objective and noninvasive and will lead to qualitative improvements in forensic pathologic investigation . 
apart from the accuracy and three dimensionality that conventional documentations lack , these techniques allow for the re - examination of the corpse and the crime scene even decades later , after burial of the corpse and liberation of the crime scene . 
 keywords virtopsy postmortem imaging multislice computed tomography ( msct ) magnetic resonance imaging ( mri ) noninvasive autopsy forensic radiology digital autopsy riassunto la tomografia computerizzata multistrato ( tcms ) e la risonanza magnetica ( rm ) sono metodiche dimaging sempre pi richieste in patologia forense . 
tali tecniche possono essere di grande ausilio alle classiche autopsie medico - legali . la visualizzazione degli organi interni del cadavere pu essere eseguita preventivamente utilizzando la tcms e / o la rm . 
la rm , in aggiunta , indicata anche per la valutazione delle vittime superstiti di azioni violente , in particolare lo strangolamento , in quanto aiuta ad individuare lesioni interne talvolta non apprezzabili neanche ad unattenta osservazione esterna della vittima . 
la documentazione e lanalisi dei reperti post - mortem individuati mediante tcms e rm come pure alcune tecniche di post - elaborazione ( virtopsy ) sono esecutore - indipendenti , oggettive , non invasive e porteranno nel tempo a miglioramenti qualitativi nelle indagini patologiche forensi . 
a parte laccuratezza e la tridimensionalit di cui mancano le documentazioni convenzionali , queste tecniche consentono di riesaminare sia il cadavere che il luogo del delitto anche decenni pi tardi , dopo la sepoltura della salma e lalterazione del luogo del reato . 
noi crediamo che questo approccio virtuale , noninvasivo o minimamente invasivo permetter di migliorare la medicina forense nel prossimo futuro . parole chiave virtopsy post - mortem imaging tomografia computerizzata multistrato ( tcms ) risonanza magnetica ( rm ) autopsia non - invasiva radiologia forense autopsia digitale 1368 introduction how relevant it is to deal with modern postmortem techniques in medicine is witnessed by the need for a modern and shared reflection about the contribution of radiologic science in necroscopic practice for forensic purposes . the progress and evolution of radiological sciences towards an increasingly improved definition of technical parameters enabling study of the details of the human body and its components , both in an anatomical - structural and a physiologicalpathophysiological sense , has brought closer two disciplines that only appear to be so different . 
in fact , both disciplines are based on the study and interpretation of anatomical findings , with radiology aiming to provide rapid responses with implications , forensic medicine to shed light on legal issues and both being carried out for research purposes . 
the methodological and operational approach between the two disciplines is recent , dating back to the early uses of conventional radiology in the study and detection of foreign bodies retained in the corpse . therapeutic - operational in the 1970s , the american college of pathologists reported on the importance of the correct use of preventive radiography in some cases of death and , at the time of its introduction , carried out studies on the use of ultrasoundguided techniques of anatomical sampling [ 1 ]  . 
in 1984 , di maio in italy published a paper instructing on the correct use of radiography in the study of firearm deaths , which immediately assumed the value of a protocol for the discipline . 
over the past 20 years , radiologic examinations have become increasingly available and accessible in both practical and economic terms , leading to a closer collaboration between the two disciplines , with a move from a needed sensitivity to performing radiographic examination in special cases to the almost routine and objective experience of the postmortem radiologic investigation , universally named virtopsy [ 36 ]  . the term virtopsy derives from the terms virtual and autopsy . 
merged the terms virtual and autopsy deleting autos to create the term virtopsy [ 7 ]  . virtopsy basically consists of documenting and analysing a body volume using multislice computed tomography ( msct ) , magnetic resonance imaging ( mri ) and 3d surface reconstructions by processing raw data sets radiol med ( 2009 ) 114 : 13671382 introduzione quanto attuale possa essere il discutere di moderne tecniche autoptiche allinterno del sistema medicina , testimoniato dalla necessit di unodierna , condivisa riflessione , sullapporto della scienza eidologica nella pratica autoptica a fini forensi . il progredire e levolversi delle scienze radiologiche , verso la sempre maggiore definizione di parametri tecnici atti allo studio dei dettagli del corpo umano e delle sue componenti , tanto in senso anatomo - strutturale , quanto in senso fisiologico / fisiopatologico hanno , forse come non mai , avvicinato due discipline solo apparentemente cos diverse . 
entrambe le discipline , infatti , a ben riflettere , basano il loro humus sullo studio e linterpretazione dei reperti anatomici , volti luna , la radiologia , allesigenza di una sempre pi rapida risposta dai risvolti terapeuticointerventistici , laltra , la medicina legale , allacclaramento dei fatti di giustizia , oltre che , naturalmente , per entrambe , ai fini di ricerca . 
laccostamento metodologico operativo tra le due discipline , invero , ha origini assai recenti , che risalgono ai primi impieghi della radiologia tradizionale per lo studio e la repertazione di corpi estranei ritenuti nellorganismo . gi negli anni 70 , negli stati uniti , lamerican college of pathologists segnalava limportanza del corretto utilizzo dellindagine radiografica preventiva in alcuni casi mortali , cos come , coeva alla sua introduzione , portava avanti studi sullutilizzo delle tecniche di prelievo anatomico eco - guidate [ 1 ]  . 
in italia , nel 1984 , di maio pubblicava un decalogo del corretto impiego della radiografia nello studio delle morti da armi da fuoco che , da subito , assumeva senso e valore protocollare per la disciplina . 
si riteneva cio indispensabile , per un corretto esperimento settorio nei casi di morti da armi da fuoco , la preventiva individuazione dei proiettili ritenuti integri o in frammenti cos come indispensabile era la loro consequenziale rimozione e repertazione [ 2 ]  . 
da allora passato oltre un ventennio , nel quale la sempre maggiore disponibilit degli esami eidologici , vieppi in termini di accessibilit , non solo di fruibilit pratica , ma anche economica , hanno , negli ultimi anni , posto in collaborazione le due discipline affinando metodiche e facendo crescere esperienze . 
si passati dallauspicata sensibilit alleffettuazione dellesame radiografico in particolari casi , alla pressoch routinaria ed oggettiva esperienza della sofiindagine eidologica pre - autoptica denominata sticata universalmente virtopsy [ 36 ]  . 
il termine autopsia una combinazione dei vocaboli classici greci autos ( auto , propri ) e opsomei ( io vedr )  . cos , autopsia significa vedere con i propri occhi . 
 la virtopsy consiste fondamentalmente nella documentazione ed analisi di un volume corporeo mediante tomografia radiol med ( 2009 ) 114 : 13671382 1369 with volume - rendering ( vr ) tools at a workstation in such a way that a virtual autopsy can be performed at any time or place . 
in deceased persons , the main goals are to determine the cause and manner of death , to evaluate the vitality of the sustained injuries and to develop a forensic reconstruction based on the findings ( table 1 )  . although autopsies are still recognised as important medical table 1 main objectives of virtopsy identification gender , age , body length , organ weight estimation , individual features ( dental , intracorporeal ) documentation foreign material ( bullets , metal fragments , inserted foreign bodies ) cause and manner of death as the result of different manners : accident , suicide , homicide , natural or iatrogenic causes possible causes : polytrauma , drowning , shooting , burn injuries , hanging , etc . vitality of sustained injuries forensic reconstruction education research tabella 1 principali obiettivi della virtopsy identificazione sesso , et , lunghezza corporea , stima del peso degli organi , caratteristiche individuali ( dentarie , intracorporee ) documentazione corpi estranei ( proiettili , frammenti metallici , corpi estranei impiantati ) causa e modalit di decesso quale esito di differenti modalit : incidente , suicidio , omicidio , cause naturali o iatrogene possibili cause : politrauma , annegamento , lesioni da arma da fuoco , ustioni , impiccamento , ecc . ricerca di segni vitali a carico delle strutture anatomiche lesionate ricostruzione forense istruzione ricerca computerizzata multistrato ( tcms ) , risonanza magnetica ( rm ) e ricostruzioni 3d di superficie , elaborando il set dei dati acquisiti con strumenti di volume rendering ( vr ) mediante una workstation dedicata , permettendo quindi di eseguire unautopsia virtuale in qualsiasi momento e in qualsiasi luogo , il tutto non alterando alcun reperto utile ai fini medico - legali a differenza di quanto avviene con le tecniche invasive utilizzate nelle autopsie tradizionali [ 8 ]  . 
 i principali obiettivi della medicina forense sono documentare , analizzare e chiarire le prove medico - scientifiche , sia che si tratti di soggetti viventi che di persone decedute , presentandole in un modo facilmente comprensibile in unaula giudiziaria . 
in persone decedute , gli obiettivi principali sono determinare la causa e le modalit di morte , valutare la presenza di segni vitali a carico delle strutture anatomiche lesionate e sviluppare una ricostruzione forense sulla base dei diversi reperti ( tabella 1 )  . 
tale fase comporta la scansione dellintero cadavere , al fine di acquisire mediante tcms o rm un insieme di dati da rielaborare poi con tecniche 3d volume - rendering [ 9 ]  . 
diversamente dalla genetica forense ( in cui viene utilizzato il dna ) e dalla tossicologia forense , la documentazione dei reperti patologici utili ai fini medico - legali ancora basata prevalentemente sulluso degli stessi protocolli e tecniche autoptiche utilizzate da secoli . 
lebraismo ortodosso , per esempio , vieta la manomissione dei corpi esanimi , tranne quando tali azioni possono salvare la vita ad altri o in situazioni di emergenza per la rimozione di organi ai fini di donazione . 
 pertanto da considerare che lautopsia convenzionale , al giorno doggi spesso respinta da parte di familiari o non tollerata per tali motivi religiosi nella nostra societ multietnica , potrebbe essere in parte sostituita da una documentazione non - invasiva di immagini e , se necessario , da tecniche di campionamento tissutale mini - invasive imagingguidate e dallangiografia per la valutazione delle alterazioni vascolari . 
i dati acquisiti in maniera digitale potrebbero invece essere consultati ogni qual volta emergono nuove problematiche medico - legali o essere inviati ad altri esperti esterni per un secondo parere . 
this involves cadaver scanning to acquire msct or mri data sets and the use of 3d direct volume - rendering techniques [ 9 ]  . autopsies are known for their importance in establishing the cause of death . 
other than in forensic genetics ( in which dna is used ) and forensic toxicology , the documentation of forensic pathologic findings is still predominantly based on the same autopsy techniques and protocols that have been used for centuries . 
religious prohibitions are one reason for this trend . orthodox judaism , for example , prohibits disturbing dead bodies except when such action may save others and urges avoidance of organ removal . 
followers of islam are opposed to any desecration or exposure of the body of a deceased believer . conventional autopsy , nowadays often refused by the family or not tolerated for religious reasons in our multiethnic societies , may thus be replaced by noninvasive imaging and , when required , by minimally invasive imaging - guided tissue sampling and by angiography to address vascular questions . 
in addition , autopsy specimens such as tissue sections are difficult to store indefinitely . digitally acquired data could instead be consulted whenever new issues arise , or they could be sent to other experts for a second opinion . 
several studies have shown that virtual autopsy holds great potential to aid forensic investigations [ 5 , 7 , 10 , 11 ]  . virtual autopsies have several other advantages over traditional methods of investigation . 
assessing the entire bone structure or searching for air , for example , is otherwise difficult and time - consuming . virtual autopsies also have a number of disadvantages . postmortem imaging with msct and mri provides no colour documentation of the body . 
mri , on the other hand , is better suited for the lautopsia virtuale ha la grande potenzialit di supportare le indagini forensi [ 5 , 7 , 10 , 11 ]  . 
infatti , la tcms ha dimostrato di essere molto utile nella repertazione di alterazioni ossee , dei corpi estranei , di embolia gassosa , e di grossolane alterazioni dei tessuti molli [ 7 , 12 ]  . 
la visualizzazione di strutture vascolari e la possibile emorragia allo stesso modo difficile da rilevare , ma risultati promettenti sono stati raggiunti dallangiografia post - mortem [ 13 , 14 ]  . 
 tecniche di imaging sia la tcms che la rm possono essere utilizzate per uno studio di imaging post - morte necessario illustrare agli specialisti del settore le principali applicazioni di ogni metodica come pure i loro limiti per trarre i maggiori vantaggi sfruttando le capacit insite in ciascuna tecnica . 
 gli strumenti a disposizione per facilitare la visualizzazione dei reperti dimaging post - mortem comprendono software che rendono pi facile e veloce la valutazione e linterpretazione di un grande volume di dati . 
msct has shown to be very useful in detecting bone lesions , foreign bodies , air embolisms and gross abnormalities of the soft tissue [ 7 , 12 ]  . 
visualising the circulation and possible bleeding is also difficult , but promising results have been achieved with postmortem angiography [ 13 , 14 ]  . postmortem information on imaging provides no histology and chemistry . 
this can be solved to a certain extent with msct - guided biopsies or mr spectroscopy . postmortal gas can be difficult to distinguish from bowel gas or gas in wound channels . 
it is thus important to perform postmortal imaging as soon as possible after death . imaging techniques both msct and mri can be used for postmortem imaging . practitioners need to appreciate the principal applications of each technique as well as its limitations to make the most of each modalitys capabilities . 
it is relatively easy to visualise bone , gas and metal with msct , for instance , but discrimination of soft tissue is limited . tools available to facilitate the visual presentation of postmortem imaging data include software packages that make it easier and quicker to view and interpret largevolume data sets . 
it is theoretically possible to reconstruct an infinite number of images from data acquired for a typical whole - body msct virtual autopsy , leading to data sets several gigabytes in size . 
this technique makes it possible to obtain not only tissue specimens but also samples of urine , bile or blood for toxicological or dna rielaborate dovrebbero fornire agli esaminatori una buona comprensione della anatomia 3d post - mortem in questione come pure orientare sulla probabile causa di morte . una peculiare caratteristica dellautopsia virtuale rappresentata dalla stragrande quantit di dati ottenuti . 
 teoricamente possibile ricostruire un infinito numero di immagini a partire dai dati acquisiti per una autopsia virtuale whole - body mediante tcms , comportando quindi pacchetti di dati delle dimensioni di diversi gigabyte . 
la tecnica di scansione della superficie corporea mediante scanner con ottica di superficie 3d fotogrammetrica pu documentare e confrontare gli oggetti e le ferite sul corpo . inoltre possibile utilizzare uno scanner di superficie dotato di un proiettore a fasci di luce e due fotocamere combinate che misurano la deformazione di tali fasci in relazione alla superficie corporea . 
successivamente il software in grado di elaborare un modello 3d basato sulla deformazione di tali strie luminose [ 1517 ]  . stata inoltre perfezionata per scopi forensi la tecnica mini - invasiva di biopsia imaging - guidata ( per esempio sotto guida tc ) su cadaveri per consentire il prelievo di campioni tissutali per lanalisi istologica . 
in tal modo possibile , in casi selezionati , eseguire una completa indagine autoptica in maniera mini - invasiva , specie ove sia impraticabile per qualsivoglia motivo la tradizionale autopsia . uno dei problemi cruciali in medicina - legale la valutazione del tempo trascorso dal momento del decesso . 
la spettroscopia mediante rm in grado di fornire una stima di tale tempo partendo da informazioni metaboliche ottenute dallanalisi di predefinite regioni encefaliche [ 18 ]  . la possibilit di ricavare multiple informazioni mediante tutte queste metodiche consente quindi lesecuzione in ultima analisi di una autopsia completa , minimamente invasiva , dalla cui fusione dei dati raggiunti possibile ottenere uno strumento importante da utilizzare nelle aule giudiziarie del futuro . principali applicazioni lautopsia virtuale in grado di fornire informazioni in merito alle possibili cause di morte . politrauma le fratture possono essere pi facilmente individuate utilizzando le ricostruzioni 3d . 
thus , a complete , minimally invasive autopsy examination is possible in selected cases in which traditional autopsy is impracticable for whatever reason . assessing the time since death is a fundamental problem . mr spectroscopy can provide an estimation of this time from metabolic information collected in a predefined region of the brain [ 18 ]  . 
data fusion may also be an important tool in the courtroom of tomorrow . main applications polytrauma virtual autopsy can provide information for many possible causes of death . fractures can be visualised using 3d reconstruction . 
the direction of the force causing bone fracture can be assessed by analysing the fracture systethus , the base of a wedge - shaped fracture piece indicates the direction of the force . 
in injuries to the head , determining whether the injury was caused by a fall to the ground or a blow to the head is an important forensic assessment when the deceased person was initially found lying injured on the ground . 
this determination can be made on the basis of typical skull fracture systems , the morphologic features of the crush wound and contrecoup lesions within the brain [ 20 ]  . as it does not use ionising radiation , and as it is well suited for the depiction of soft - tissue pathology , mri is also regularly utilised within the project in the assessment of surviving victims of blunt trauma , especially of manual strangulation [ 21 ]  . 
the problem in such cases is that the superficial findings may be innocuous , but the underlying soft tissuesespecially around the reflectogenic structures of the throatmay be severely traumatised , thus leading to a potentially life - threatening situation . identification prior to any postmortem investigation , the identity of the body must be clarified and proved ; otherwise , the postmortem investigation has as one of its goals the re - estabtura . 
in caso di lesioni alla testa , determinare se il danno stato causato da una caduta al suolo o da un colpo alla testa un importante elemento di valutazione forense specie quando la persona deceduta viene inizialmente ritrovata gi ferita per terra . 
questa valutazione pu essere effettuata sulla base del tipico aspetto di frattura delle ossa craniche , sulle caratteristiche morfologiche della ferita da impatto e in base alle lesioni da contraccolpo rinvenute allinterno del cranio [ 20 ]  . dal momento che non utilizza radiazioni ionizzanti e poich risulta essere particolarmente adatta alla valutazione della patologia dei tessuti molli , la rm regolarmente utilizzata anche nellambito del protocollo di valutazione delle vittime superstiti di traumi contusivi , in particolare di strangolamento manuale [ 21 ]  . 
il problema in questi casi che i reperti superficiali a volte possono anche essere di lieve entit e quindi non facilmente apprezzabili , mentre i tessuti molli sottostanti , specialmente quelli che circondano le strutture laringee , possono essere gravemente traumatizzati , determinando in tal modo una situazione di potenziale pericolo di vita . identificazione prima di qualsiasi tipo di indagine post - mortem , deve essere chiarita e dimostrata lidentit del cadavere ; se ci non possibile , uno dei principali obiettivi dellindagine post - mortem risulta essere la ricerca dellidentit del corpo non identificato . 
poich lesame del dna la tecnica pi costosa e che richiede maggior tempo , si utilizzano pi comunemente a tale scopo il rilevamento delle impronte digitali e lidentificazione e dello status dentario . 
i dati ottenuti dalla tcms di un cranio di un cadavere , possono essere utilizzati per ricostruire qualsivoglia proiezione radiografica utile al confronto con lo status ante - mortem [ 23 ]  . 
inoltre , il materiale utilizzato in trattamenti ortodontici pu essere accertato sulla base di dati tc postmortem e confrontato con i reperti dentari ante - mortem nel caso si sospetti di persone scomparse [ 25 ]  . 
in aggiunta a grossolani reperti morfologici come endoprotesi di spalla , anca , ginocchio o segni di percutaneo - vertebroplastica , reperti peraltro individuabili sulla base di un efficiente isperadiol med ( 2009 ) 114 : 13671382 1373 lishment of the identity of the unidentified body . 
the human or animal remains of past cultures can be investigated without disturbing them ( as would traditional autopsy ) , thereby providing information regarding the age and gender of , as well as any injuries or diseases suffered by , the deceased animal or person , as recently performed on the newly discovered egyptian mummies [ 2830 ]  . drowning traditional autopsies provide no unambiguous indications of drowning . 
drowning has especially been related to young adults who are under the influence of alcohol and other drugs whilst being near water [ 34 , 35 ]  . diagnosis relies primarily on the subjects individual characteristics and circumstances , macroand micropathological postmortem changes and studies of the lungs , zione esterna , una tcms whole - body di un cadavere rivela ulteriori reperti utilizzabili positivamente per lidentificazione , nonch per lesclusione di una presunta identit , conclusioni in alcuni casi non raggiungibili mediante lautopsia di routine come nel caso , ad esempio , di un cadavere completamente bruciato [ 26 , 27 ]  . unaltra disciplina in cui lodierno imaging di inestimabile valore paleoradiologia . 
i resti umani o animali , appartenenti ad epoche passate , possono essere studiati senza alterare minimamente il loro stato ( come avverrebbe invece con lautopsia tradizionale ) , mettendo cos a disposizione degli esperti informazioni riguardanti let e il sesso , cos come qualsiasi lesione o malattia subita dal defunto animale o persona , come ultimamente effettuato sulle mummie egiziane recentemente scoperte [ 2830 ]  . annegamento le autopsie tradizionali non forniscono indicazioni inequilorganizzazione vocabili di annegamento . 
attualmente lannegamento si riscontra soprattutto nei giovani adulti che abusano di alcol e altre droghe [ 34 , 35 ]  . la diagnosi si basa principalmente sulle caratteristiche individuali del soggetto e sulle circostanze , sulle alterazioni post - mortem macroe micro - patologiche , e sugli studi dei polmoni , tra cui il volume polmonare . 
gli specialisti del settore possono studiare il volume polmonare post - mortem , lattenuazione media , le differenze di attenuazione antero - posteriore , il profilo di densit polmonare , e lammontare di acqua presente nei polmoni . 
 [ 36 ] , analizzando i reperti tcms post - mortem preautoptici di dieci casi di annegamento e confrontandoli con 20 casi di non - annegamento sottoposti ugualmente ad autopsia e tcms post - mortem , avevano riscontrato la presenza di fluido nelle vie aeree in tutti i casi di annegamento . 
tutti questi reperti , tipici dellannegamento , ad eccezione degli spots di paltau ( depositi pleurici di emoglobina da emolisi ) , sono stati rilevati utilizzando la tcms post - mortem , ed stata trovata una buona correlazione tra la tcms e lautopsia tradizionale . 
 [ 36 ] , analysing the postmortem preautopsy msct findings of ten drowning cases in comparison with autopsy and postmortem msct of 20 nondrowning cases observed that fluid in the airways was present in all drowning cases . 
all the typical findings of drowning , except paltaus spots ( pleural haemoglobin deposits from haemolysis ) , were detected using postmortem msct , and a good correlation between msct and autopsy was found . 
knowing the bullets location before commencing physical autopsy will save the pathologist time , especially if the bullet has actually left the body . bullets frequently lodge far from their entry points , particularly if they are deflected by curved bones such as the ribs or skull . postmortem radiology serves to locate the projectile , entry and exit wounds , depict the bullet course and may help identify the ammunition and the weapon type utilised [ 37 ]  . 
to assess the direction from which gunshot wounds were created , different characteristics are visualizzazione diretta del broncospasmo , dellemodiluizione e dellacqua in tutti i seni paranasali , reperto piuttosto complicato o impossibile da rilevare con la classica autopsia . 
la conoscenza dellesatta posizione di un proiettile allinterno del corpo prima dellinizio di una autopsia tradizionale consentir al medico - legale di risparmiare il tempo necessario allindagine autoptica , specialmente se il proiettile ha in realt abbandonato il corpo . 
i proiettili infatti sono spesso rinvenuti anche in sedi distanti dai loro punti di ingresso , particolarmente se deviati da ossa curve come le coste o il cranio . la radiologia post - mortem utile quindi a individuare il proiettile , i fori dingresso e di uscita , indica il percorso compiuto dal proiettile , e pu aiutare a identificare le munizioni e il tipo di arma utilizzata [ 37 ]  . 
anche la precisa valutazione del percorso compiuto dal proiettile attraverso il corpo di estrema importanza , specie poich aiuta a ricostruire il luogo del delitto , la posizione della vittima e dellomicida [ 38 ]  . 
inoltre , la regola di puppe pu contribuire a valutare lordine cronologico in cui si sono formate le fratture , in quanto , secondo tale regola , le fratture pi recenti si interromperanno in corrispondenza di quelle precedentemente formate [ 39 ]  . 
 [ 40 ] dallanalisi forense di 57 casi mediante tecniche di neuroimaging , basate sulluso della tcms e della rm e dal confronto dei risultati ottenuti con i reperti autoptici , hanno osservato che abrasioni , contusioni e lacerazioni del cuoio capelluto sono state rilevate dalla rm piuttosto che dalla tc ; tuttavia , e non sorprendentemente , per quanto riguarda tutti i tipi di lesioni al cuoio capelluto , lautopsia era di gran lunga superiore alle tecniche di imaging . 
la tc e la rm sono state quasi equivalenti nella valutazione delle emorragie extra - assiali che , nel complesso , hanno trovato una soddisfacente correlazione con lautopsia . nei casi in cui la tc e la rm non hanno identificato radiol med ( 2009 ) 114 : 13671382 1375 fig . 
1 examination of a gunshot victim by msct : msct , 2d and 3d reconstructions of the body of a homicide victim . forensic radiology can be of great help in detecting entrance and exit wounds , bullet and bullet fragments within the body , bullet track and inflicted injuries , as well as in identifying the ammunition and the weapon type utilised . 
la radiologia forense pu essere di grande aiuto nellindividuazione del foro di ingresso e di uscita , del proiettile , dei suoi frammenti , del suo percorso e delle lesioni arrecate allinterno del corpo , oltre ad identificare il tipo di munizione e di arma utilizzata . 
 [ 40 ] , analysing 57 forensic cases by neuroimaging techniques such as msct and mri and comparing the results to the autopsy findings , observed that abrasions , contusions and lacerations of the scalp were detected by mri rather than ct . 
ct and mri were the evaluation of extra - axial almost equivalent emorragie subdurali , i reperti autoptici indicavano un sanguinamento con spessore inferiore a 3 mil 53% delle contusioni a carico della sostanza grigia sono state osservate mediante tc , di cui la rm ne ha rilevato circa il 41% ; le tecniche radiologiche sono state sufficienti per la valutazione di reperti definiti come lesioni da colpo o da contraccolpo allautopsia . 
la rm e la tcms si sono dimostrate superiori allautopsia in merito alla valutazione dellemorragia ventricolare , nonch dello pneumocefalo che non era stato osservato allindagine autoptica , anche se il cranio era stato parzialmente distrutto . 
la rm stata superiore alla tc nellindividuazione delle lesioni del parenchima cerebrale ( ad esempio nel mostrare chiaramente il percorso compiuto dal proiettile ) e a carico del troncoencefalo . lesioni da ustioni lautopsia virtuale pu apportare un contributo significativo in diversi casi che coinvolgono corpi gravemente bruciati , fornendo informazioni su eventuali fratture , distribuzione di gas , ed altri reperti . 
2 examination of a gunshot victim by msct : msct , 2d and 3d reconstructions of the skull of a gunshot victiknowing the bullets location in gunshot injuries before starting physical autopsy will save the pathologist time . 
in this case , postmortem radiology serves to locate the projectile and entry and exit wounds , depict the bullet course and may help in identifying the ammunition and the weapon type utilised . 
tcms e ricostruzioni 2d e 3d del cranio di una vittima darma da fuoco . la conoscenza preliminare dellesatta posizione della pallottola nelle lesioni da arma da fuoco ridurr al medico - legale il tempo necessario per lindagine autoptica . 
in questo caso la radiologia forense serve a individuare il proiettile , il foro di ingresso e di uscita , identificare il percorso compiuto dal proiettile agevolando lindividuazione del tipo di munizione e di arma adoperata . 
questo facilita il recupero del proiettile e di frammenti potenzialmente importanti nel rivelare informazioni circa langolazione e la direzione seguita dal proiettile stesso . hemorrhage that overall was found in a satisfactory correlation with the autopsy . 
mri and msct were superior to autopsy concerning evaluatius of ventricular hemorrhage , as well as pneumencephalus that had not been noted in the autopsy protocols , even if the head had been partially destroyed . 
quindi , il heat epidural , spesso riscontrato in cadaveri carbonizzati , non rappresenta una lesione antemortem e non dovrebbe essere erroneamente interpretata come tale [ 41 ]  . impiccamento per escludere un simulato suicidio in caso di impiccamento messo in atto per mascherare un qualche tipo di omicidio , i medici legali ricercano sulla vittima segni di reazioni vitali . le ricostruzioni 3d dei dati acquisiti con la tcms possono radiol med ( 2009 ) 114 : 13671382 burn injuries virtual autopsy can make a significant contribution to several cases involving severely burned bodies , providing information on fractures , gas distribution and other areas . 
thus , heat epidural is often seen in burned corpses but does not indicate an antemortem injury and should not be misinterpreted as such [ 41 ]  . hanging to exclude simulated suicidal hanging covering some kind of homicide , forensics experts search for vital reactions . three dimensional reconstruction of msct data can verify vital signs that are caused by the hanging procedure to exclude postmortem simulated hanging . 
bleeding into the insertions of the sternocleidomastoid muscle or softtissue structures of the neck prove that circulation was ongoing at the onset of strangulation , and strong breathing attempts against the occluded airways cause alveolar ruptures with subsequent pneumomediastinum and softtissue emphysema ascending into the neck [ 43 ]  . vitality of sustained injuries cutaneous vital reactions elucidate the sequence of injury and death in forensic pathologic investigations . 
the answer is provided by forensic findings that occur only with intact circulation ( e.g. fatal haemorrhage , air and fat embolism ) , respiration ( e.g. aspiration , emphysema ) , metabolism or consciousness . 
 cardiac applications the leading cause of natural death is cardiac insufficiency . postmortem imaging must be able to separate these natural deaths from unnatural deaths because the heart is often the target of injury in suicides as well as homicides . 
 1377 verificare la presenza di segni vitali causati dalla procedura di impiccamento per escludere che si tratti di una simulazione post - mortele immagini 3d possono inoltre visualizzare i segni della legatura aiutando a ricostruire il processo di strangolamento [ 19 , 21 , 42 ]  . 
il sanguinamento in corrispondenza delle inserzioni dei muscoli sternocleidomastoidei o a carico dei tessuti molli del collo dimostrano che la vittima era in vita al momento dello strangolamento , come pure i tentativi di respirazione forzata , per vincere locclusione delle vie aeree , possono causare rotture alveolari con conseguente pneumomediastino ed enfisema dei tessuti molli con carattere ascendente nel collo [ 43 ]  . 
la risposta fornita dal riscontro di reperti medico - legali identificabili solo quando la circolazione sanguigna ancora presente ( ad esempio , emorragia mortale , embolia adiposa e gassosa ) , in presenza di respirazione ( ad esempio , aspirazione , enfisema sottocutaneo ) , con metabolismo attivo e in stato di coscienza . 
la presenza di materiale aspirato , sia esso sangue , contenuto gastrico , o fuliggine , dimostra una ventilazione ancora in corso dopo il trauma , cos come un diffuso enfisema dei tessuti molli dopo un trauma contusivo . 
anche se lenfisema sottocutaneo apprezzabile alla palpazione dei tessuti molli , difficilmente tale reperto resta permanentemente tale allindagine autoptica in quanto laria tende a scomparire al momento dellincisione della cute sovrastante . 
limaging post - mortem deve essere in grado di discriminare questi decessi naturali dalle morti innaturale in quanto il cuore rappresenta il principale obiettivo da lesionare in suicidi e omicidi . 
acute bleeds tend to have higher hounsfield unit values than older bleeds on msct [ 4447 ]  . forensic outlook today we could translate virtopsy with digital autopsy so as to fit the expression to the method . 
indeed , a careful review of scientific papers published to date clearly shows that digital autopsy is particularly well suited to the basic objective of forensic medicine , that is , the investigation of scientific evidence . however , before moving towards the future , we should consider the present situation : the autopsy . 
judicial autopsy , far from exhausting the investigations on the corpse , is just one step in the process : not the first , much less the last [ 52 , 53 ]  . autopsy , as external inspection of the corpse and internal examination , is just one necessary step in the approach to the corpse . 
in the range of such ancillary examinations to the main investigation ( autopsy ) , the radiologic - forensic investigation rises to a new dimension and becomes rightfully placed among the instruments enabling the search for scientific ( validated and repeatable ) evidence . 
 awareness of the need for a guarantee of validity ( the best in a technical sense ) and reliance on increasingly objective technicalscientific aids has permeated the coroners causato da lesioni del miocardio o dei vasi epicardici pu essere documentato sia con la tcms che mediante rm . alla tcms le emorragie acute tendono a presentare pi alti valori densitometrici , in termini di unit hounsfield , rispetto ai sanguinamenti cronici [ 4447 ]  . 
invero , a ben scandagliare il contenuto della produzione scientifica sin qui prodotta , ben si comprende come , a fronte delleccezionale lavoro esperito , in realt lautopsia digitale ben si incardina su un concetto basilare della medicina legale quale quello della ricerca di evidenze scientifiche quale mezzi di prova . in realt , ancor prima di fare un passo verso il futuro , appare opportuno interrogarsi sul suo presente : the autopsy , do we still need it ? piace riportare il quesito in inglese poich esso parafrasa per intero il titolo di un editoriale edito nel 1970 sulla prestigiosa rivista chest [ 48 ]  . 
ed invero , ad una scorsa della letteratura nazionale ed internazionale pi recente , la ovvia risposta che lautopsia non solo necessaria ma da dire assolutamente irrinunciabile [ 4951 ]  . 
ed infatti , come abbiamo gi avuto modo di esprimere , lautopsia giudiziaria , lungi dallesaurire gli accertamenti sul cadavere , non che un momento di essi : non il primo , n tanto meno lultimo [ 52 , 53 ]  . lautopsia intesa come esame esterno cadaverico ed esperimento settorio , solo uno ( ineluttabile ) dei momenti di approccio al cadavere , forse neanche il pi importante , ma certamente propedeutico al corretto prelievo , campionamento e studio istologico di ogni singolo organo o frammento di esso . 
lindagine tossicologica , genetico - forense , e cos via , sino ad arrivare ai pi specialistici esami di metabolomica e / o proteonomica costituiscono oggi il corretto corollario ad una moderna indagine autoptica . 
nellambito di tali innesti ancillari alla indagine principe ( la autopsia ) , assurge a nuova dimensione lindagine eidologico - forense in grado di essere annoverata a pieno titolo tra i mezzi di ricerca di evidenze scientifiche ( come tali validate e ripetibili )  . 
 la consapevolezza della necessit di una forte garanzia di validit ( la migliore possibile in senso tecnico ) , della riferibilit a supporti tecnico - scientifici sempre pi oggettivi , ha permeato negli ultimi anni la sensibilit del medicolegale [ 54 ]  . 
ben si comprende , allora , come e perch alcuni autori siano giunti ad auspicare lo studio tc del cadavere nello specifico settore delle morti da arma da fuoco , alla stregua di una autopsia virtuale ( virtopsy ) da configurarsi come uno strumento observer - indipendent , che non altera la realt del corpo e poich digitalizzato ed archiviato , anche a distanza di tempo , sempre ripetibile ed oggettivabile [ 5 , 5557 ]  . indubbiamente , lo studio tridimensionale del corpo umano permette una esatta localizzazione dei corpi estranei di natura metallica eventualmente ritenuti ed offre un radiol med ( 2009 ) 114 : 13671382 1379 sensitivity in recent years [ 54 ]  . 
it is not surprising , then , that some authors advocated ct study of corpse in firearms deaths to be used as a virtual autopsy ( virtopsy ) and thus an observer - independent instrument that does not alter the corpse and that is repeatable and objectifiable , even over time [ 5 , 5557 ]  . undoubtedly , the 3d study of the human body allows correct localisation of any metallic foreign bodies and helps greatly in identifying the exact intracorporeal channels with a precision very similar to that of autopsy studies : very similar , but not replaceable , as findings without the physical detection and accurate description of gross features such as margins , rims and halos can be appreciated , even in intracorporeal parenchymas , and are indispensable for the correct description of the death event ( not merely the cause , but also with information regarding the manner and time )  . such a diagnostic aid is clearly of great benefit to the practice of forensic medicine : the possibility of new evaluations , subsequent verification and multidisciplinary consultation in complex investigations , even after the end of the classic postmortem procedures , is a positive opportunity . 
 digital autopsy can disclose findings that might escape even the most careful observation : while a minute bone splinter can easily escape an accurate direct inspection , it will not escape an aseptic database that will return this piece of information at a later evaluation allowing , for instance , confirmation of the differential diagnosis between the entry and the exit wounds . 
however , at this particular stage of the cultural debate , the above must lead to the correct interpretation and methodologicaloperational collocation of digital autopsy as an asset to two disciplines that depend on each other for the purposes of reaching specific diagnostic conclusions . 
 to conclude , it should be noted that although crucial to the autopsic investigation as a whole , these advanced studies will remain ancillary and supplemental to the classic postmortem investigation , without replacing it . 
hence the need to use semantic caution and steer the meaning of virtopsy toward the notion of digital autopsy that better reflects the nature of the technique and the intrinsic meaning of an ancillary method rather than a possible replacement , contributo eccellente nella esatta individuazione di tramiti intracorporei , con una precisione che raggiunge livelli di sovrapponibilit allosservazione settoria . 
sovrapponibile , ma non per questo sostituibile , poich reperti privi della materiale individuazione e dellesatta descrizione di caratteristiche macroscopiche , quali margini , orletti ed aloni , invero sono ben apprezzabili anche nei parenchimi intracorporei ed indispensabili per il corretto inquadramento dellevento morte ( inteso non solo come momento causativo ma corredato di informazioni preziose relative al modus ed al tempo della morte )  . evidente che lavere a disposizione un simile supporto diagnostico nella pratica di medicina forense in occasione delle ricognizioni autoptiche sia di straordinario vantaggio : la possibilit di procedere a nuove valutazioni , a riscontri successivi nel tempo , a consulti multidisciplinari per indagini complesse , anche dopo che si sono concluse le procedure autoptiche classiche , rappresenta una vantaggiosa opportunit . lautopsia digitale in grado di fornire rilievi che possono sfuggire anche alla pi attenta e sperimentata osservazione medico - legale : una minuscola scheggia ossea , ad esempio , pu assai facilmente sfuggire allosservazione diretta , pur accuratissima , ma non ad un asettico data - base che restituir questa informazione ad una valutazione successiva consentendo , ad esempio , di arricchire di ulteriori conferme la diagnosi differenziale tra fori di ingresso e fori di uscita . 
tutto questo , per , proprio in questa attuale fase del vivo dibattito culturale ci deve condurre alla corretta interpretazione e collocazione metodologico - operativa dellautopsia digitale quale patrimonio di due discipline non autonome luna dallaltra ai fini delle specifiche conclusioni diagnostiche , ma interdisciplinari . 
 peraltro ci sentiamo , in conclusione , di ammonire come tali indagini siano sovente di fondamentale importanza nellambito dellindagine autoptica intesa in maniera omnicomprensiva , ma con intendimento che tali sofisticate metodiche siano di accompagnamento ed approfondimento , ma non certo sostitutive , neppure parzialmente , dellindagine autoptica classicamente intesa . 
da qui la necessit di un pi prudente viraggio semantico dalla virtopsy al concetto di autopsia digitale pi rispondente tanto ad un corretto inquadramento della tecnica quanto allintrinseco significato di un affiancamento e non mai dellavvicendamento , che porti quindi non ad una virtopsy , ma semmai verso una virtuous autopsy o autopsia virtuosa . 1380 radiol med ( 2009 ) 114 : 13671382 leading not to a virtopsy but , if anything , to a virtuous autopsy . conclusioni conclusions in some countries , virtual autopsy is now used routinely for forensic work . 
findings identified during physical autopsy often raise additional questions that can be answered by virtual autopsy . the pathologist can also re - examine the cadaver at any point during the investigation and search for additional information . 
 the applications of msct technology in the forensic domain suggest that a mobile scanner could be used for postmortem data acquisition in cases of mass casualties such as airplane crashes or natural disasters . 
future applications of this approach include assessment of morbidity and mortality in the general population and , perhaps , routine screening of bodies prior to burial . several forces must work in unison if a new era of digital autopsies is to emerge . 
however , digital autopsy is and will remain merely an aid in the practice of forensic medicine and one that is not always available and that cannot be considered an alternative to conventional postmortem procedures . in alcuni paesi lautopsia virtuale attualmente utilizzata di routine per scopi forensi . 
i reperti identificati allindagine autoptica talvolta sollevano ulteriori problematiche cui lautopsia virtuale in alcuni casi in grado di rispondere . pertanto lo specialista del settore pu anche riesaminare virtualmente il cadavere in qualsiasi momento durante linchiesta giudiziaria alla ricerca di ulteriori utili informazioni . 
nuove scoperte emerse dalle indagini compiute sul luogo del reato possono comportare il riesame di altre ipotesi mediante imaging . lacquisizione delle immagini con gli attuali scanner tcms e la successiva sessione di elaborazione richiedono peraltro molto meno tempo rispetto a quello necessario per eseguire un esame autoptico completo . 
lindagine virtuale pu anche ridurre il tempo necessario per lautopsia tradizionale essendo il medico - legale preventivamente informato dei reperti pi significativi da valutare . le applicazioni della tecnologia tcms in ambito forense hanno suggerito luso di apparecchiature mobili per lacquisizione di informazioni nel post - mortem in caso di incidenti di massa , come incidenti aerei o calamit naturali . 
future applicazioni di questo approccio comprendono la valutazione della morbilit e della mortalit nella popolazione generale e , forse , lo screening di routine dei corpi prima della loro sepoltura . 
 diversi organi competenti devono lavorare allunisono , se una nuova era delle autopsie digitali dovr emergere . medici specializzati e autorit giudiziarie devono stabilire protocolli standard per la scansione e la memorizzazione dei dati . 
i radiologi avranno anche bisogno di una formazione specifica nel settore dellimaging post - mortem in quanto limaging del cadavere si presenta spesso in maniera molto diversa da quanto routinariamente osservato in pazienti viventi . 
non si pu , tuttavia , nascondere che quello dellautopsia virtuale , e rimane , soltanto un supporto alla pratica di medicina legale , non sempre disponibile e che , non pu certamente , costituirsi come alternativa alle procedure autoptiche usuali . acknowledgments the authors thank giampaolo grilli ( dipartimento di radiologia ospedaliera , azienda ospedalierouniversitaria di foggia ) for his contribute in the aquisition and post - elaboration of the images . ringraziamenti gli autori ringraziano il dott . 
the solution to this dilemma is particularly complex in an environment in which the tendency to sue physicians for civil liability or incriminate them for criminal liability appears to be particularly high . 
there does not appear to be any evidence to suggest disclosure modifies the probability of litigation against the physician . keywords ethics medical error disclosure malpractice apology riassunto nella pratica radiologica , come in qualsiasi attivit medica , lerrore inevitabile , anche se prevedibile e prevenibile . 
la soluzione di tale dilemma particolarmente complessa in un ambiente nel quale la tendenza a citare il medico per responsabilit civile o a incriminarlo penalmente appare oggettivamente elevata . la rivelazione dellerrore certamente utile ad aumentare la consapevolezza del paziente , ridurne le sofferenze , migliorare la qualit dellassistenza e limitare le conseguenze del danno . 
non vi evidenza che tale atto modifichi la probabilit che il medico sia sottoposto ad una azione giudiziaria . parole chiave etica errore medico rivelazione dellerrore mala pratica richiesta di scuse medical error lerrore medico a few years ago under the title to err is human , a book by the united states institute of medicine [ 1 ] dramatically drew attention to the issue of medical errors . 
figures published in the report that stated that between 44 , 000 and 98 , 000 patients die in us hospitals each year due to medical errors were greeted with alarm by the media : medical errors were said to be responsible for twice the number of deaths as the vietnam war or equivalent to a 9 / 11 every day . 
 pochi anni fa , sotto il titolo errare umano un saggio dellistituto di medicina statunitense ( iom ) [ 1 ] ha posto drammaticamente lattenzione sul tema degli errori medici . le cifre del rapporto , secondo il quale negli ospedali statunitensi morirebbero ogni anno da 44000 a 98000 pazienti a seguito di errori medici , sono state riprese con toni allarmanti dalla stampa : gli errori medici causerebbero ogni anno negli stati uniti il doppio di morti della guerra del 1346 radiol med ( 2009 ) 114 : 13451355 the tone was no different in the scientific press , according to which medical errors are the fifth cause of death in the us and cost some us $29 billion each year [ 2 ]  . 
it was rightly noted that if these statements were correct , the us healthcare system was a threat to public health of pandemic proportion [ 3 ]  . the estimate of errors and adverse events is generally based on the review of medical charts or analysis of litigation claims , error reporting systems or other methods of investigation , none of which is without limitations or pitfalls [ 4 ]  . 
a literature review taking into consideration this and seven other studies conducted in the united states , canada , the united kingdom , australia and new zealand estimated that adverse events during hospitalisation occur in one in every six patients [ 6 ]  . 
in italy there are no reliable statistics available , and estimates oscillate between 15 , 000 and 50 , 000 deaths per year as a result of intrahospital errors and adverse events . 
the figure of 30 , 00035 , 000 preventable deaths reported by many press agencies corresponds to 5.5% of total deaths , more than the number of deaths on the road or due to heart attack or many cancers . 
the associated costs are said to be in the order of 10 billion euro , or 1% of the gross domestic product . although the interpretation of the statistics by the media is undoubtedly distorted , the institute of medicine report gives voice to a real problethe deaths occur above all in the terminal phase of critical patients . 
the evaluation conducted a priori , which leads to the extrapolation of the number of preventable deaths , is fraught with limitations , is particularly influenced by the operator who performs it and is unable to make any inference regarding the possible survival that would have occurred had the error not been made [ 3 ]  . 
the phenomenon therefore tends to be overestimated , because the evaluation fails to take into consideration the risk of death in the absence of medical error [ 7 ]  . one study that considered the prognosis of patients who were the victims of medical error came to the conclusion that only 0.5% would have enjoyed at least 3 months of life if the care had been optimal [ 3 ]  . 
nonetheless , it is clear that there is a broad margin for the improvement of medical procedures . even irrespective of the drama of the preventible loss of human life , it should be borne in mind that a medical error can have significant psychological repercussions for both the family of the victim and the physician responsible for the error . 
il tono non diverso nei commenti della stampa scientifica , secondo la quale gli errori medici rappresentano per la popolazione degli usa la quinta causa di morte , e costano 29 miliardi di dollari lanno [ 2 ]  . 
 stato giustamente osservato che se queste affermazioni fossero corrette , il sistema sanitario rappresenterebbe una minaccia per la salute pubblica di proporzioni epidemiche [ 3 ]  . le stime degli errori e degli eventi avversi sono generalmente basate su metodi di revisione delle cartelle cliniche , o su analisi delle denunce , dei sistemi di segnalazione degli errori o su altri metodi di indagine , nessuno dei quali esente da limiti e punti deboli [ 4 ]  . 
una delle indagini pi accurate , lo harvard medical practice study , ha rilevato che eventi avversi occorrono nel 3 , 7% dei ricoveri ospedalieri , e che in pi di un quarto di questi casi ( quindi , nell1% di tutti i ricoveri ) rilevabile negligenza [ 5 ]  . 
una revisione della letteratura , che tiene conto di questo e di altri sette studi condotti in usa , canada , regno unito , australia e nuova zelanda , stima che gli eventi avversi durante lospedalizzazione riguardino quasi un paziente su dieci [ 6 ]  . 
la cifra di 3035 mila morti evitabili , che riportata da molte agenzie giornalistiche , corrisponde al 5 , 5% dei decessi totali , pi degli incidenti stradali , dellinfarto e di molti tumori . 
la valutazione che porta a determinare il numero di morti evitabili , condotta a posteriori presenta numerose limitazioni , risentendo spiccatamente delloperatore che la effettua , e non potendo inferire in alcun modo sulleventuale sopravvivenza che ci sarebbe stata se lerrore non si fosse verificato [ 3 ]  . 
uno studio che tiene conto della prognosi dei pazienti vittime di errori medici giunto alla conclusione che solo lo 0 , 5% di essi avrebbe goduto di almeno tre mesi di vita se le cure fossero state ottimali [ 3 ]  . tuttavia evidente che esiste un largo margine di miglioramento nelle procedure mediche . anche se si volesse prescindere dal dramma della perdita evitabile di una vita umana , occorre tenere presente che lerrore medico pu avere gravi conseguenze psicologiche sia per i familiari della vittima che per lo stesso medico che ne autore . indeed , once the patients family members have been victims of and witness to a fatal error , they may feel a real sense of guilt for not having safeguarded the health of their infatti , una volta che i familiari dei pazienti siano stati vittime e testimoni di un errore fatale , possono sentire un vivo senso di colpa per non avere vigilato sufficientemente radiol med ( 2009 ) 114 : 13451355 1347 loved one sufficiently well or for not having obtained the best available care or the most reliable physician . 
this conflict can increase the sense of isolation and abandonment prompted by the loss of their family member [ 8 ]  . at the same time , physicians , too , may feel a sense of guilt resulting from the error and the fear of suffering professional and economic consequences and of being isolated by their own colleagues and clients [ 8 ]  . 
added to this is the consideration that medical professionals who have committed a severe error are open to a reduction in quality of life and an increase in the frequency of burnout . 
perceived stress is associated with an increase in the number of errors committed in the subsequent period , thus creating a vicious circle whereby errors lead to stress and stress leads to new errors [ 9 ]  . in a pilot study conducted among a group of italian radiologists and radiation therapists , we observed that those who had been subject to litigation for presumed malpractice display a high rate ( > 60% of cases ) of reactions of anxiety and anger , and in one third of cases , even feelings of helplessness , disappointment , anguish and humiliation . 
one in 20 radiologists have reported physical disturbances following a malpractice suit , and almost 40% have admitted to having changed their own practice to adopt strategies of defensive radiology [ 10 ]  . error in radiology medical errors in radiology can be mainly classified in two categories : procedural errors , which arise from incorrectly performing radiological procedures such as the injection of iodinated contrast medium , the barium enema and , more generally , interventional radiology procedures ( biopsy , angioplasty , stenting , vascular embolisation , drainage , ablation , etc . ) , and diagnostic errors . 
procedural errors , which in italy are at the basis of 10%15% of malpractice suits against radiologists [ 11 ] , have the same clinical and medicolegal characteristics as those that occur in surgical specialisations and therefore have no specific features . 
in contrast , diagnostic errors , which are at the basis of 60% of claims against radiologists [ 11 ] , have a profoundly different nature in radiology from that in other medical and surgical specialisations . diagnostic imaging differs from clinical diagnostics in that in the latter there is direct contact between physician and patient . 
in radiology , instead , due to historical and practical reasons that are still prevalent in italy , the patient does not self - refer to the radiologist but is referred by a clinician . sulla salute del proprio caro e per non aver procurato le cure migliori o il medico pi affidabile . 
 di contro , anche i medici possono avvertire il senso di colpa per lerrore , la paura di subirne le conseguenze professionali ed economiche e di essere isolati dai propri colleghi e clienti [ 8 ]  . 
il distress percepito associato con laumento della commissione di errori nel periodo seguente : si crea cos un circolo vizioso , per cui gli errori portano a stress e questo a nuovi errori [ 9 ]  . in uno studio - pilota condotto su un gruppo di radiologi e radioterapisti italiani abbiamo osservato che coloro che hanno subito una denuncia per presunta malpractice manifestano con elevata frequenza ( oltre il 60% dei casi ) reazioni di ansia e rabbia e , in circa un terzo dei casi , anche sensazione di essere indifeso , e sensazioni di delusione , angoscia e umiliazione . 
un radiologo su venti ha riferito di avere riportato in seguito alla denuncia danni fisici obiettivabili , e quasi il 40% ha ammesso di avere cambiato la propria condotta professionale , per adottare strategie di radiologia difensiva [ 10 ]  . lerrore in radiologia gli errori medici in radiologia appartengono principalmente a due categorie : gli errori procedurali , che derivano dallo svolgimento non corretto di tecniche radiologiche , come liniezione di mezzo di contrasto iodato , il clisma opaco , e pi in generale tutte le tecniche proprie della radiologia interventistica ( biopsia , angioplastica , stenting , embolizzazione vascolare , drenaggio , ablazione ecc . ) , e gli errori diagnostici . 
gli errori procedurali , che danno origine nel nostro paese al 10%15% delle richieste di risarcimento contro i radiologi [ 11 ] , hanno le stesse caratteristiche cliniche e medico - legali di quelli che occorrono nelle specialit chirurgiche e non presentano quindi particolari specificit . 
al contrario gli errori diagnostici , che sono allorigine di oltre il 60% delle denunce contro i radiologi [ 11 ] , riconoscono in radiologia un profilo profondamente diverso da quello di altre discipline mediche e chirurgiche . la diagnostica per immagini differisce dalla diagnostica clinica per il fatto che in questultima c un contatto diretto tra medico e paziente , mentre in radiologia , per ragioni 1348 radiol med ( 2009 ) 114 : 13451355 communication with the referring clinician and the patient are two critical and distinguishing features of the radiologist that we will discuss below . the work of the radiologist consists of two distinct but integrated phases : the complete identification of all abnormalities in the radiological image and their correct interpretation . 
the inability to detect an abnormality in a radiological examination , are the leading cause of litigation against radiologists , particularly in the case of breast [ 12 ] or chest cancer [ 11 ]  . 
they appear to be significantly correlated with a number of psychophysiological factors , such as the level of alertness of the radiologists , which in turn depends on physical and mental fatigue and therefore on work - related stress , and on their state of visual tiredness , which depends on ergonomic conditions of the work environment , the duration of the visual task , and therefore on the pauses and workload . 
such a complex pattern explains why this type of error cannot be completely eliminated , even though specific techniques have been developed and taught that make up good radiological practices and are aimed at reducing the rate of perception errors [ 13 ]  . the reading of radiographs by a second radiologist would undoubtedly reduce ( although not completely eliminate ) the number of perception errors . 
however , this practice is possible only in some cases where a second radiologist is available , and it is in fact limited to cases of doubtful diagnosis and not adopted routinely for the reading of images except in some screening programmes . perception errors are committed even by expert radiologists operating in ideal conditions . 
the frequency and inevitability of perception errors and the availability to the patient of his or her radiological images explain why radiologists are more exposed to medicolegal risk than are other medical specialties . 
whereas in the traditional working model storiche e pratiche tuttora prevalenti nel nostro paese , il paziente non si presenta direttamente al radiologo , ma viene inviato da un clinico . 
la comunicazione con il clinico curante e quella con il paziente sono due aspetti critici peculiari della radiologia , dei quali ci occuperemo in seguito . il lavoro del radiologo consiste di due momenti separati , ancorch fra loro integrati : lidentificazione completa di tutte le anomalie dellimmagine radiologica e la loro corretta interpretazione . 
il secondo momento , lerrore di interpretazione , si pu ritenere analogo a quello di altre branche della medicina , nelle quali possibile interpretare in modo errato un rilievo obiettivo , ad esempio un soffio cardiaco o un altro segno clinico . lerrore percettivo , cio lincapacit a rilevare una anomalia in un esame radiografico , la principale causa di contenzioso contro i radiologi , soprattutto nel caso del tumore della mammella [ 12 ] o del torace [ 11 ]  . 
esso appare significativamente correlato con numerosi fattori psicofisiologici , come il livello di allerta del radiologo , che a sua volta dipende dalla fatica fisica e mentale e quindi dallo stress da lavoro , e il suo stato di affaticamento visivo , che dipende dalle condizioni ergonomiche dellambiente di lavoro , dalla durata dellimpegno visivo , e quindi dalle pause e dal carico di lavoro . 
un quadro cos complesso rende ragione del perch non sia possibile eliminare del tutto questo tipo di errore , nonostante siano state messe a punto ed insegnate tecniche specifiche , che rientrano nelle buone pratiche radiologiche , finalizzate proprio a ridurre il tasso di errori percettivi [ 13 ]  . la lettura dei radiogrammi da parte di un secondo radiologo potrebbe indubbiamente ridurre ( non eliminare in assoluto ) gli errori percettivi , ma tale pratica , possibile solo nei casi in cui vi sia la disponibilit di un secondo radiologo , di fatto limitata ai casi di dubbio diagnostico e non adottata routinariamente per la lettura delle immagini se non in alcuni programmi di screening . gli errori percettivi sono commessi anche da radiologi esperti , che operano in condizioni ideali . 
la frequenza e inevitabilit degli errori percettivi , e la disponibilit piena da parte del paziente della documentazione radiologica che lo riguarda , rendono ragione del fatto radiol med ( 2009 ) 114 : 13451355 1349 the presence of the prescribing physician is an implicit guarantee against the failure to transmit , or delayed transmission of , the report by the radiologist , this cannot be said to be the case in screening programmes . 
it therefore comes as no surprise that in the united states there has been a significant rise in the number of malpractice suits related to delayed or incomplete communication of diagnostic findings by the radiologist . 
in italy , communication problems are encountered in a part of criminal proceedings ( ex art . 589 or 590 of the penal code ) , which involve the radiologist and other specialists and account for > 12% of malpractice litigation against radiologists [ 11 ]  . in the united states , in cases where a communication deficit is dependent on a radiologist , the courts have established damages on average twice that awarded in cases where only a diagnostic error was found [ 16 ]  . 
it has in fact been noted that the marked development of radiological techniques has not been matched by a similar improvement in reporting and communication [ 17 ]  . it has therefore been suggested that perhaps radiologists should communicate the findings of examinations directly to patients to at least partially avoid errors in communication [ 18 ]  . in the united states it has been estimated that 40% of radiologists are sued for malpractice on average once every 5 years [ 19 ]  . 
in that country , litigation against radiologists accounts for 10%15% of total malpractice claims , even though radiologists in the united states are less exposed to the risk of litigation than are surgeons , but they are much more exposed than internists and other specialists [ 20 ]  . 
the average compensation payouts agreed by the courts have tripled over the last 15 years , and approximately one third of cases conclude with conviction of the radiologist [ 15 ]  . in the same period , italy has gone from a situation of low - level medicolegal conflict [ 21 , 22 ] to one similar to that in the united states . 
with regard to practising radiologists , approximately half have received or will receive a claim for compensation or a summons related to their professional practice over the last 10 years . 
with regard to young radiologists who are beginning their career in italy , it can be stated with statistical certainty that each and every one will receive a claim for compensation at some point during their working life [ 11 ]  . the contrast is even more striking when compared with countries with a particularly low level of judicial conflict , such as those in northern europe . 
in the united kingdom che i radiologi siano esposti ad un rischio medico - legale pi elevato rispetto ad altre specialit mediche . un altro aspetto peculiare dellerrore in radiologia la comunicazione . 
se nel modello di lavoro tradizionale la presenza di un medico prescrittore rappresenta una implicita garanzia contro la mancata o ritardata trasmissione del referto da parte del radiologo , ci non pu ritenersi valido nel caso dei programmi di screening , nel quale i pazienti presumono di essere sani , ed i loro medici curanti , che si attendono un risultato negativo , non hanno alcun motivo di sollecitare una risposta . 
 negli usa nei casi in cui sia stato riscontrato un difetto di comunicazione a carico del radiologo le corti hanno stabilito un risarcimento di entit mediamente doppia rispetto ai casi in cui fosse stato accertato solo un errore diagnostico [ 16 ]  . 
ci si interroga pertanto se non sia il caso che i radiologi comunichino direttamente ai pazienti i risultati degli esami , cos da evitare almeno in parte gli errori di comunicazione [ 18 ]  . negli stati uniti si stima che il 40% dei radiologi sia citato in giudizio mediamente una volta ogni 5 anni [ 19 ]  . sempre negli usa le denunce contro i radiologi rappresentano il 10%15% del totale delle denunce contro i medici per imperizia o negligenza anche se , in quel paese , i radiologi risultano nel complesso meno esposti al rischio di citazioni rispetto ai chirurghi , ma molto pi esposti dei medici internisti e specialisti [ 20 ]  . 
per i radiologi gi in attivit si pu dire che , mediamente , circa la met di essi ha ricevuto o ricever una richiesta di risarcimento o una citazione per la propria attivit professionale degli ultimi dieci anni . 
per i giovani radiologi che iniziano oggi la professione in italia , si pu dire che ciascuno di essi ha la certezza statistica di ricevere almeno una richiesta di risarcimento nel corso delle propria vita professionale [ 11 ]  . 1350 radiol med ( 2009 ) 114 : 13451355 over the past two centuries , from 1795 to today , only 85 physicians have been taken to court with the charge of manslaughter , and only 22 of those have been convicted ; none of them were radiologists [ 23 ]  . 
in italy , however , more than 100 radiologists have been charged with manslaughter in the last decade [ 11 ]  . in sweden , where the malpractice claims are dealt with through administrative channels and compensated by a national insurance system if an independent medical committee confirms the claim , litigation against physicians is decidedly low . 
this principle , which is included in the hippocratic oath , is older than radiology , but there is no doubt that it should also be applied to this branch of medicine . 
it places a number of specific obligations on both the physician who commits it and on their colleagues and the healthcare centre they work in . on an individual basis , the physician who commits an error has a responsibility towards the patient . 
if the error causes bodily harm , informing the patient of the error is a moral obligation , which in the united states is also a legal obligation [ 25 ]  . 
this act of conscience , this awareness of ones own error and the harm caused , leads to contrition and therefore repentance and the resolution not to repeat the error , together with satisfaction or reparation of the harm done . 
even though the expectation of the penitent is forgiveness , there is no guarantee that the mistreated patient is willing to forgive . the fact that the indications regarding disclosing medical error is based on religious values whereas we live in a secular society explains why they are only partially applied in medical practice . 
in gran bretagna negli ultimi due secoli , dal 1795 ad oggi , solo 85 medici hanno dovuto subire un processo per omicidio colposo , e soltanto 22 sono stati condannati ; nessuno di essi era radiologo [ 23 ]  . 
in italia , viceversa , oltre cento radiologi sono stati indiziati per omicidio colposo nellultima decade [ 11 ]  . in svezia , dove i reclami dei pazienti sono trattati per via amministrativa ed indennizzati da un sistema assicurativo nazionale se un collegio medico indipendente conferma la congruit della richiesta , la conflittualit legale per i medici decisamente ridotta . 
il tasso delle richieste di indennizzo per malpractice medica dopo un ricovero ospedaliero fermo da anni allo 0 , 2% dei ricoveri [ 24 ]  . responsabilit del medico e rivelazione degli errori i medici hanno sempre avuto il dovere di non causare alcun danno ai pazienti ( principio di non maleficenza )  . 
lerrore rappresenta una deviazione dallo standard della disciplina ; esso pone diversi e specifici obblighi sia al medico che lo commette , che ai suoi colleghi e allazienda sanitaria in cui operano . sul piano individuale il medico che ha commesso un errore responsabile verso il paziente . 
latto di coscienza , la consapevolezza del proprio errore e del danno causato determinano contrizione , pentimento , quindi il ravvedimento e il proponimento di non ripetere lerrore , uniti alla soddisfazione , riparazione del danno . 
anche se lattesa del penitente nel perdono , non vi alcuna garanzia che il paziente offeso sia disposto a perdonare . il fatto che le indicazioni sulla rivelazione degli errori medici siano basate sui valori religiosi , ma che la nostra sia una societ secolare , rende ragione del fatto che esse siano applicate solo parzialmente nella pratica medica . 
indagini condotte sui medici statunitensi indicano che il 95% di essi ha assistito ad almeno un errore ; oltre l80% ritiene che rivelare gli errori migliori la sicurezza dei futuri pazienti , ma la radiol med ( 2009 ) 114 : 13451355 1351 improves the safety of future patients , in 1991 , some 76% stated they failed to report a significant error . 
today , only one in 30 inform patients of serious errors , and one in five states that they have not reported errors they have committed [ 27 ]  . 
the opinions regarding appropriate behaviour in the event of error , the type of error that should be reported and the manner of doing so are radically different in patients and physicians [ 28 ]  . experience indicates that in some cases , the disclosure of an error by a physician can be used by the patient to launch litigation against the same physician [ 29 ]  . 
even though laws prompted by the intervention of senators hillary clinton in new york state and barack obama in illinois rule out the possibility of using as circumstantial evidence the apology of a physician to a patient , these laws do not rule out the possibility of the physicians being sentenced if they have admitted their own guilt . 
indeed , lawyers advise physicians never to apologise , or at least never to make a complete apology , but rather to display an attitude limited to expressing empathy and understanding without ever referring to ones own errors or those of other physicians and repeating the causal chain of events ( apologia or botched apology )  . 
an authentic apology requires recognition that a procedure has been violated , the consequent admission of blame for that violation , the expression of genuine remorse , regret for the harm caused , an explicit offer of reparation or the commitment to modify procedures such that the violation never occurs again [ 30 ]  . as can be easily imagined , patients have a rather different opinion from physicians and their legal representatives regarding the information that should be provided in the event of error . 
they expect complete admission of responsibility and are unwilling to accept partial admissions , even though in most cases they state that error disclosure by a physician would not deter them from seeking legal action [ 31 ]  . 
it has nonetheless been noted that the discovery of an error not disclosed by a radiologist or clinician tends to sharpen a patients determination to undertake legal proceedings and prompts the courts to set higher compensation than would be applied in the event the error was immediately disclosed [ 32 ]  . all the techniques of clinical risk management are based on the principle that the search for errors is made to identify the cause and not the perpetrator , and they guarantee that error reporting is anonymous . 
nonetheless , there is a fine line between analysis carried out for preventative purposes percentuale di quanti dichiarano di non avere riportato gli errori gravi commessi era del 76% nel 1991 . 
le opinioni sui comportamenti da tenere in caso di errore , su quali errori segnalare ed in che modo farlo , sono radicalmente diverse nei pazienti e nei medici [ 28 ]  . lesperienza indica che in alcuni casi lammissione di errore da parte del medico pu essere usata dal paziente per promuovere una azione giudiziaria contro il medico stesso [ 29 ]  . 
anche se , per intervento dei senatori hillary clinton nello stato di new york e barack obama nellillinois , sono state approvate leggi che escludono la possibilit di usare come prova indiziaria il fatto che il medico abbia offerto le proprie scuse al paziente , queste leggi non escludono che il medico possa essere condannato se nel farlo ha ammesso la propria colpa . 
di fatto , gli avvocati consigliano ai medici di non offrire mai le proprie scuse , o al massimo , di non fare una piena e completa offerta di scuse ( apology ) , ma una esposizione limitata ad esprimere empatia e comprensione , senza mai fare riferimento a errori propri o di altri medici e ribadendo la causalit degli accadimenti ( apology o botched apology )  . questa forma di comunicazione strategicamente diretta non a fornire informazioni , ma a giustificare la propria azione e neutralizzare potenziali effetti negativi [ 30 ]  . 
una autentica apology richiede invece un riconoscimento che una procedura stata violata , la conseguente ammissione di colpa per tale violazione , lespressione di un genuino rimorso , il dispiacere per il danno causato , una esplicita offerta di riparazione e limpegno a modificare le cose in modo che la violazione non debba pi accadere [ 30 ]  . i pazienti hanno , come facile prevedere , una opinione piuttosto diversa da quella dei medici e dei loro legali su quali debbano essere le informazioni fornite in caso di errore . 
essi pretendono una completa ammissione di responsabilit e non sono disposti ad accettare ammissioni parziali , anche se , nella maggioranza dei casi , dichiarano che la rivelazione di un errore da parte del medico non li distoglierebbe dallintraprendere una azione legale [ 31 ]  . 
 stato per osservato che la scoperta di errori non rivelati dal radiologo o dal medico rende i pazienti pi determinati a procedere giudizialmente e spinge le corti a fissare risarcimenti pi elevati di quelli che vengono determinati nei casi in cui vi sia stata una tempestiva rivelazione [ 32 ]  . anche se tutte le tecniche di clinical risk management partono dal principio che la ricerca degli errori si fa per identificare la causa e non il colpevole , e garantiscono lanonimato delle segnalazioni , la distinzione tra indagini a fini preventivi e a fini ispettivi molto sottile e pu essere 1352 radiol med ( 2009 ) 114 : 13451355 and investigative purposes , a line that can be easily overstepped . 
in the united states , consumer organisations demand that data regarding complications recorded in hospitals be available on line so that patients may make an informed decision [ 33 ]  . 
such a move would create the real possibility of triggering an uncontrollable spiral of alarm , with an increase in malpractice claims and therefore of insurance costs and defensive medical practices ( which already account for 8%10% of unjustified costs for various healthcare organisations )  . with regard to the issue of clinical risk , the attitude of healthcare organisations in italy and the english - speaking world is markedly different . 
in english - speaking countries , the principle has always been in force that the healthcare system is accountable in the event of errors committed by healthcare personnel when the latter are unable to demonstrate that they acted specifically to prevent the errors . roman law , in contrast , rules out criminal liability of the system ( societas delinquere non potest ) , and in this respect , art . 
this orientation has been a real hindrance to the principle of social accountability of the healthcare system and in the specific sense has led to an underestimation of the problem and a general omission of prevention measures , unjustly considered the exclusive responsibility of individuals . 
only recently has legislative decree 231 / 01 introduced into the italian judicial system the principle of institutional liability for administrative offences on the basis of failure to act and negligence in the management of the institutional body . 
the recent legislative decree 81 / 08 ( known as the consolidation act in matters of health and workplace safety ) extended this form of liability to offences in the workplace . these differences in legislative frameworks and traditions explain the difficulty in comparing the experiences and choices made in english - speaking countries with those in italy . 
in the united states , a number of healthcare organisations have managed to reduce expenses due to medical malpractice suits by applying a policy whereby the physicians and hospital managerial staff not only disclose errors but admit blame and offer compensation [ 29 ]  . 
some healthcare organisations have adopted a policy of absolute honesty , according to which the patient who has suffered the error is fully informed , receives care and is compensated . 
this system seems to have led to a reduction in medicolegal costs for healthcare organisations [ 34 ] , even though a reduction in the number of compensation claims has not been shown . 
negli stati uniti le organizzazioni dei consumatori chiedono che siano resi accessibili in rete i dati sulle complicazioni registrate negli ospedali , cos che sia possibile una scelta informata da parte dei pazienti [ 33 ]  . in italia , forse a solo scopo propagandistico , stato proposto di rendere disponibili on - line gli errori di ciascun medico . 
la possibilit di innescare in questo modo una spirale incontrollabile di allarme , con incremento delle denunce di malpractice e quindi dei costi assicurativi e delle pratiche di medicina difensiva ( che gi oggi rappresentano l8%10% di spese ingiustificate a carico dei diversi sistemi sanitari ) , concreta . riguardo al tema del rischio clinico latteggiamento delle aziende sanitarie anglosassoni e di quelle italiane estremamente diverso . 
nei paesi anglosassoni , difatti , stato sempre vigente il principio della responsabilit delle aziende sanitarie , che possono essere chiamate a rispondere degli eventuali errori dei propri dipendenti , qualora non siano in grado di dimostrare di avere attivamente operato per prevenire tali errori . 
il diritto romano , al contrario , escludeva la responsabilit penale delle aziende ( societas delinquere non potest ) e su questa linea la nostra costituzione ha stabilito , allart . 27 , che la responsabilit penale personale . 
tale orientamento ha costituito un reale ostacolo al principio della responsabilit sociale delle aziende e , nel campo specifico , ha indotto la sottovalutazione del problema e la generale omissione delle misure di prevenzione , a torto ritenute di esclusiva competenza dei singoli . 
solo di recente con il d . lgs 231 / 01 stato introdotto anche nel nostro sistema giudiziario il principio della responsabilit dellente per i delitti amministrativi , sulla base del comportamento omissivo e negligente nella gestione della propria struttura organizzativa . 
lgs 81 / 08 ( cosiddetto testo unico sulla salute e sicurezza sul lavoro ) ha esteso tale responsabilit anche ai delitti in campo lavorativo . le differenze del quadro normativo e delle tradizioni rendono ragione della difficolt di confrontare le esperienze e le scelte anglosassoni con quelle nostrane . 
negli usa alcune aziende sanitarie hanno ridotto le spese derivanti dal contenzioso medico - legale applicando una politica secondo la quale i medici e dirigenti dellospedale non solo rivelano gli errori , ma ammettono la colpa ed offrono un risarcimento [ 29 ]  . 
alcune organizzazioni sanitarie hanno adottato una politica di estrema onest secondo la quale il paziente che ha subito un errore viene informato in modo completo , ottiene assistenza e viene indennizzato . 
questo sistema sembra avere determinato una riduzione delle spese medico - legali da parte delle aziende sanitarie [ 34 ] , anche se non dimostrato che esso abbia ridotto il numero di richieste di risarcimento . 
 stato osservato infatti che il paziente o i suoi familiari hanno una risposta positiva verso radiol med ( 2009 ) 114 : 13451355 1353 lies respond positively towards the physician who openly and fully acknowledges having made a clinical error , thus maintaining their trust and satisfaction with the care provided , but it is unclear whether this dissuades them from taking legal action . 
in cases where the error causes damage of little count , an offer by the physician to compensate costs could have a negative effect [ 35 ]  . all this , however , is not to suggest that the disclosure of errors is a universal and painless practice in englishspeaking countries . 
many healthcare workers are loathe to reveal their own errors for fear of possible repercussions . nonetheless , there is strong cultural pressure in favour of such behaviour , right from the early stages of medical training . 
medical students are , in fact , instructed on how to behave in the event of errors committed by their tutor [ 36 , 37 ]  . the way to behave in the event of errors committed by colleagues in fact reveals the greatest distance between the ethical principles taught and applied in english - speaking countries and those of latin origin ( mind your own business )  . 
in the former , the physician is obliged to intervene should they note or receive an anonymous report of a colleague not adhering to standards : the failure to do so can lead to disciplinary action . 
the intervention should , of course , be graded according to the situation and may range from a simple discussion with the colleague to clarify matters and possibly involve advice to avoid the problem being repeated , to a report to a superior , right up to a report to professional bodies . il medico che riveli in modo aperto e completo di avere commesso un errore clinico , conservando la loro fiducia e la soddisfazione per loperato del medico , ma non chiaro se ci li distolga dallintraprendere una azione giudiziaria . nei casi in cui lerrore abbia prodotto danni poco rilevanti , il fatto che il medico si offra di rimborsare i costi potrebbe avere effetti negativi [ 35 ]  . non bisogna credere che la divulgazione degli errori sia una pratica universale e indolore nei paesi anglosassoni : molti sanitari sono riluttanti a rivelare i propri errori per il timore delle possibili ripercussioni . 
tuttavia presente una forte pressione culturale per favorire tale comportamento , sin dalla prime fasi delleducazione medica : gli studenti sono istruiti sul comportamento da tenere nel caso di errori compiuti dal loro tutore [ 36 , 37 ]  . 
 proprio sullatteggiamento da tenere nel caso di errori commessi dai colleghi che si rileva la maggiore distanza tra i principi etici insegnati e applicati nei paesi anglosassoni e la pratica popolare dei latini ( fatti i fatti tuoi )  . 
il medico obbligato ad intervenire nel caso che abbia notato , o abbia avuto segnalazione anche anonima , del fatto che un suo collega ha operato in modo difforme dagli standard ; nel caso che ometta di farlo , pu essere egli stesso sottoposto ad azione disciplinare . 
lintervento da compiere , naturalmente , graduato in funzione della necessit , e pu andare da un semplice colloquio con il collega , per chiarire i fatti ed eventualmente elargire consigli per evitare il ripetersi del problema , ad una segnalazione per via gerarchica , fino alla segnalazione agli organismi professionali . conclusions conclusioni as with all ethical problems , there are no simple and painless solutions that can be immediately applied . 
they may inform the patient that there has been a clinical problem , without accepting liability and possibly illustrating the factors that may cause undesirable effects or diagnostic difficulty in radiology . 
they may inform the patient that there has been a clinical problem , adding comforting statements such as : i am really sorry that this had to happen to you . 
they may inform the patient of the error , accept liability and offer compensation . in appears clear that in the setting of personal ethics , the correct choice can only be the latter . 
this is by no means an easy choice to make , and the physician should not expect that the patient sees things in the same light and offers come in ogni altro problema etico , non esistono ricette semplici e indolori da applicare automaticamente . 
il medico radiologo che si accorga di avere commesso un errore grave , che ha causato un danno ad un paziente , ha la possibilit di scegliere una delle cinque possibili alternative . 
pu comunicare al paziente che ci sia stato un problema clinico , ma senza assumersene la responsabilit , ed eventualmente illustrare i motivi che determinano effetti indesiderati o difficolt diagnostiche in radiologia . 
pu comunicare il fatto al paziente , dichiarando che si trattato di un errore ed assumendosene la responsabilit . infine , pu comunicare lerrore al paziente , assumersene la responsabilit ed offrire un risarcimento . appare evidente che , nellambito di unetica personalistica , la scelta corretta sar solo questultima . 
pozzi mucelli1 1department of radiology , 2department of biomedical and surgical science , university of verona , p.le scuro 10 , 37134 verona , italy 3erasmus university , medical center rotterdam , 3000 ca rotterdam , the netherlands correspondence to : v . 
the observers evaluated pancreatic parenchymal enlargement , signal intensity abnormalities , enhancement , vascular involvement , bile - duct diameter and main pancreatic duct ( mpd ) narrowing ( diffuse / focal / segmental )  . 
mr imaging showed diffuse pancreatic enlargement in 8 / 28 ( 29% ) cases , focal pancreatic enlargement in 16 / 28 ( 57% ) cases and no enlargement in 4 / 28 ( 14% ) cases . 
the alteration of pancreatic signal intensity was diffuse in 8 / 28 ( 29% ) cases ( 8 diffuse aip ) and focal in 20 / 28 ( 71% ) cases ( 20 focal aip )  . delayed pancreatic enhancement was present in all aip , with peripheral rim of enhancement in 8 / 28 ( 29% ) aip ( 1 / 8 diffuse , 7 / 20 focal ) ; vascular encasement was present in 7 / 28 ( 25% ) aip ( 1 / 8 diffuse , 6 / 20 focal ) ; distal common bile duct narrowing was present in 12 / 28 ( 43% ) aip ( 5 / 8 diffuse , 7 / 20 focal )  . 
scopo di questo lavoro stato valutare i rilievi di pancreatite autoimmune ( aip ) nella revisione retrospettiva delle immagini di risonanza magnetica ( rm ) , colangiopancreatografia - rm ( cprm ) e cprm con secretina . 
le immagini sono state analizzate considerando i seguenti parametri : volume del pancreas , alterazioni dellintensit di segnale del parenchima , impregnazione del pancreas , coinvolgimento vascolare , calibro delle vie biliari e restringimento ( diffuso / focale / segmentale ) del dotto pancreatico principale ( dpp )  . 
lesame rm ha evidenziato un incremento dimensionale diffuso del pancreas in 8 / 28 ( 29% ) casi , un ingrandimento di una parte del pancreas focale in 16 / 28 ( 57% ) casi e pancreas di regolare dimensione in 4 / 28 ( 14% ) casi . 
lalterazione dellintensit di segnale del pancreas era diffusa in 8 / 28 ( 29% ) casi ( 8 aip di tipo diffuso ) e focale in 20 / 28 ( 71% ) casi ( 20 aip di tipo focale )  . 
secretinenhanced mrcp is a problem - solving tool in the differential diagnosis between focal aip and ductal adenocarcinoma . keywords autoimmune pancreatitis mrcp secretin stimulation pancreas inflammatory diseases ( 5 / 8 aip di tipo diffuso , 7 / 20 aip di tipo focale )  . 
lesame cprm con secretina ha fatto rilevare il segno del dotto penetrante in 6 / 14 ( 43% ) aip ( 1 caso di aip diffusa con restringimento segmentale del dpp , 5 casi di aip focale con restringimento focale del dpp ) dimostrano lintegrit del dpp . 
 parole chiave pancreatite autoimmune cprm somministrazione di secretina pancreas malattie infiammatorie introduction introduzione autoimmune pancreatitis ( aip ) is defined as an autoimmune reaction around the pancreatic ducts resulting in inflammatory and fibrotic reaction with obliteration of the pancreatic ductal system [ 1 ]  . 
according to the different classification systems , the diagnosis of aip is based on the combination of four main criteria : imaging findings , laboratory data , histology and response to corticosteroid therapy , as assessed by both clinical and imaging findings [ 14 ]  . 
as a localised enlargement of the gland , which typically involves the head of the pancreas and the main pancreatic duct ( mpd ) upstream [ 5 , 6 ]  . 
differential diagnosis between focal aip and adenocarcinoma is extremely challenging but of paramount importance because of the different prognosis and because steroid therapy is effective in reversing clinical and morphological changes of aip [ 712 ]  . 
 most literature reports to date have concentrated on endoscopic retrograde cholangiopancreatography ( ercp ) and computed tomography ( ct ) features of aip [ 4 , 5 , 710 , 13 ]  . 
magnetic resonance ( mr ) imaging has a growing role in imaging the pancreas and biliary ducts , mainly related to visualisation of the ducts by means of mr cholangiopancreatography ( mrcp )  . 
few reports have evaluated the contribution of mr imaging in aip . furthermore , to our knowledge , the utility of secretin administration has not been evaluated , and only few studies la pancreatite autoimmune ( aip ) definita come una reazione autoimmunitaria attorno ai dotti pancreatici associata a reazione infiammatoria e fibrotica che risulta nella obliterazione del sistema duttale pancreatico [ 1 ]  . 
secondo i diversi sistemi di classificazione , la diagnosi di aip si basa sulla combinazione di 4 criteri principali : rilievi di imaging , dati di laboratorio , quadro istologico e risoluzione delle alterazioni cliniche e strumentali dopo terapia con corticosteroidi [ 14 ]  . 
 i reperti macroscopici di aip sono la diffusa ipertrofia del pancreas o pi raramente , la presenza di una alterazione espansiva formante massa , vale a dire un allargamento focale della ghiandola , che generalmente interessa la porzione della testa del pancreas e dilata il decorso del dotto pancreatico principiale ( dpp ) a monte [ 5 , 6 ]  . 
la diagnosi differenziale tra questultima , la forma focale di aip , e ladenocarcinoma pancreatico estremamente impegnativa , ma di fondamentale importanza , a causa della diversa prognosi e terapia ; il trattamento steroideo infatti efficace in caso di aip per risolvere le alterazioni cliniche e le modificazioni morfologiche [ 712 ]  . 
 fino ad oggi la maggior parte dei lavori riportati in letteratura si sono concentrati sugli aspetti delle aip rilevabili con colangio - pancreatografia retrograda endoscopica ( ercp ) e tomografia computerizzata ( tc ) [ 4 , 5 , 710 , 13 ]  . 
lindagine di risonanza magnetica ( rm ) ha un ruolo sempre pi importante nellimaging del pancreas e delle vie biliari , grazie alla capacit di visualizzazione dei dotti 1216 radiol med ( 2009 ) 114 : 12141231 have described mrcp features in aip [ 6 , 14 ]  . 
 the purpose of our study was to retrospectively review the imaging findings of mr imaging in general , and mrcp in particular , with and without administration of secretin , in patients with aip . materials and methods patients this study was approved by our investigator review board , and informed consent requirement was waived . 
a search of our institutions pathology , radiology and medical records from february 2001 to january 2006 revealed 55 patients with aip whose data were considered for inclusion in this retrospective study . 
patients were included if they fulfilled the histological criteria for aip ( fibrotic pancreatic change with lymphocyte and plasma - cell infiltration ) and had a complete mr and mrcp examination at the time of diagnosis . 
exclusion criteria were as follows : lack of histopathological diagnosis ( n = 16 ) , poor image quality ( n = 6 ) and lack of mr imaging before steroid treatment ( n = 5 )  . 
thus , the study population consisted of 28 patients ( 18 men , ten women ) , with a mean age of 45 ( range 2179 ) years at clinical presentation . 
 the frequency of symptoms at presentation was as follows : jaundice in 14 / 28 ( 50% ) , abdominal pain in 4 / 28 ( 14% ) , pancreatic - like abdominal pain ( with posterior irradiation ) in 8 / 28 ( 28% ) , weight loss in 2 / 28 ( 7% ) and diabetes in 2 / 28 ( 7% )  . 
eleven out of 28 ( 39% ) patients showed association with other autoimmune disorders : ulcerative colitis in 6 / 28 ( 21% ) , sjgren syndrome in 1 / 28 ( 3% ) , hashimotos thyroiditis in 1 / 28 ( 3% ) , sclerosing cholangitis in 2 / 28 ( 7% ) and retroperitoneal fibrosis in 1 / 28 ( 3% )  . 
the clinical and laboratory data are summarised in table 1 . the results of laboratory tests showed increased serum levels of bilirubin and cholestatic liver function tests in 10 / 28 ( 36% ) patients , increased serum amylase and lipase in 4 / 28 ( 12% ) , serum antibodies in 2 / 28 ( 6% ) patients , increased immunoglobulin ( ig ) g ( > 2.0 g / dl ) in 1 / 28 ( 3% ) patients and increased carbohydrate antigen ( ca ) 19 - 9 in 6 / 28 ( 18% ) patients ( table 1 )  . 
a history of habitual ( < 80 g / day ) alcohol consumption and cigarette smoking was present in 7 / 28 patients ; there were no patients with history of alcohol abuse ( > 80 g / day for at least 5 years )  . 
the pathological diagnosis was obtained by percutaneous ultrasonography ( us ) - guided biopsy in 23 / 28 ( 82% ) patients and by core biopsy during mediante colangiopancreatografia con rm ( cprm )  . 
un ridotto numero di studi ha valutato il contributo della rm nei casi di aip ; inoltre lutilit della somministrazione di secretina non stato ancora analizzata e solo pochi lavori descrivono le caratteristiche delle aip rilevabili allindagine cprm [ 6 , 14 ]  . 
 lo scopo del presente studio quello di valutare retrospettivamente i rilievi rm , cprm , in particolare , con e senza la somministrazione di secretina , nei pazienti con aip . 
 materiali e metodi pazienti lo studio stato approvato dal comitato etico della struttura e si soprasseduti al rilascio del consenso informato . dallanalisi degli archivi patologici , radiologici e clinici riguardanti il periodo compreso fra febbraio 2001 e gennaio 2006 sono stati evidenziati 55 pazienti con aip i cui dati sono stati presi in considerazione per linclusione in questo studio . 
i criteri di inclusione sono stati : presenza dei criteri istologici di aip ( fibrosi pancreatica con infiltrazione di linfociti e plasmacellule ) e di documentazione rm e cprm completa al momento della diagnosi . 
i criteri di esclusione sono stati i seguenti : mancanza di diagnosi istopatologica di aip ( n = 16 ) , cattiva qualit delle immagini ( n = 6 ) e mancato espletamento di indagine rm prima del trattamento steroideo ( n = 5 )  . 
la popolazione in studio , quindi , formata da 28 pazienti ( 18 uomini , 10 donne ) , con et media alla presentazione clinica di 45 anni ( range 2179 anni )  . 
 la frequenza dei sintomi di presentazione stata la seguente : ittero in 14 / 28 ( 50% ) , dolore addominale in 4 / 28 ( 14% ) , dolore addominale tipo pancreatite ( con irradiazione posteriore ) in 8 / 28 ( 28% ) , perdita di peso in 2 / 28 ( 7% ) e diabete di 2 / 28 ( 7% )  . 
altre malattie autoimmuni erano presenti in 11 / 28 ( 39% ) pazienti ; in particolare , colite ulcerosa in 6 / 28 ( 21% ) , sindrome di sjogren in 1 / 28 ( 3% ) , tiroidite di hashimoto in 1 / 28 ( 3% ) , colangite sclerosante in 2 / 28 ( 7% ) e fibrosi retroperitoneale in 1 / 28 ( 3% )  . 
 i risultati degli esami di laboratorio hanno dimostrato un aumento dei livelli sierici di bilirubina colestatica e dei test di funzionalit epatica in 10 / 28 ( 36% ) pazienti , aumento della lipasi e amilasi sierica in 4 / 28 ( 12% ) , innalzamento degli anticorpi in 2 / 28 ( 6% ) pazienti , aumento delle igg radiol med ( 2009 ) 114 : 12141231 1217 1218 radiol med ( 2009 ) 114 : 12141231 radiol med ( 2009 ) 114 : 12141231 1219 surgery in the remaining 5 / 28 ( 18% ) patients ( duodenocephalopancreasectomy : 3 / 5 patients ; bilioenteric anastomosis and cholecystectomy : 2 / 5 patients )  . 
in patients with jaundice associated with increased ca 19 - 9 ( n = 6 ) , pancreatic - like abdominal pain and jaundice ( n = 2 ) , diabetes ( n = 2 ) or those with suspected pancreatic tumour ( based on clinical signs and other imaging examinations such as ercp , us and ct performed before mr examination ) , dynamic mrcp after secretin administration was indicated . 
thus , secretin - enhanced mrcp was performed in 14 / 28 patients ( 50% ) : ten with symptoms suggestive of pancreatic disease and four with suspected diagnosis of pancreatic tumour . mr and mrcp protocols the conventional mr examination was performed with a 1.5 - t magnet ( symphony ; siemens , erlangen , germany )  . 
 the non - contrast - enhanced mr examination consisted of t1and t2 - weighted images acquired with gradient - echo ( ge ) fat - saturated ( fs ) and fast spin - echo ( fse ) sequences , with repetition time ( tr ) / echo time ( te ) ( ms / ms ) equal to 107 / 4.8 and 4950 / 102 , respectively . 
the additional delayed acquisition was performed in all cases at 5 min from the injection of the contrast mediu the mrcp examination was performed after oral administration of 100 ml superparamagnetic agent ( ferumoxsil , lumirem , guerbet , france ) with t2 - weighted rapid acquisition with relaxation enhancement turbo spin - echo ( raretse ) sequence in the paracoronal and axial planes . 
the imaging parameters were as follows : tr / te 4 , 500 / 991 ; turbo factor 410 ; field of view ( fov ) 350 mm ; matrix 410512 ; 64 - mm - thick slab . 
considering its higher spatial resolution , mrcp was also performed using a 3d t2weighted half - fourier single - shot turbo se ( haste ) sequence with respiratory triggering in the coronal oblique plane ( tr / te 4 , 450 / 585 )  . 
the imaging parameters were as follows : fov ( > 2 , 0 g / dl ) in 1 / 28 ( 3% ) pazienti , e incremento del marcatore tumorale ca - 19.9 in 6 / 28 ( 18% ) pazienti ( tabella 1 )  . una storia di consumo abituale di alcol ( < 80 g / giorno ) e fumo di sigaretta era presente in 7 / 28 pazienti ; nessuno riportava storia di abuso di alcool ( > 80 g / giorno per almeno 5 anni )  . 
la diagnosi patologica stata ottenuta con biopsia percutanea sotto guida ecografica in 23 / 28 ( 82% ) pazienti e con core - biopsy durante intervento chirurgico nei restanti 5 / 28 ( 18% ) pazienti ( duodeno - cefalopancreasectomia in 3 / 5 pazienti ; anastomosi bilio - enterica e colecistectomia negli altri 2 / 5 pazienti )  . 
nei pazienti con ittero associato ad aumento del ca - 19.9 ( 6 casi ) , con dolore addominale tipo pancreatite e ittero ( 2 casi ) , con diabete ( 2 casi ) o con sospetta diagnosi di tumore ( sulla base dei segni clinici e degli altri esami strumentali come ercp , ecografia e tc eseguita prima dellesame rm ) , stata espletata la valutazione cprm dopo secretina . 
quindi , lo studio cprm dopo secretina stato effettuato in 14 / 28 pazienti ( 50% ) , 10 pazienti con sintomi suggestivi di malattie del pancreas , 4 pazienti con sospetta diagnosi di tumore pancreatico . protocolli rm e cprm lesame rm stato eseguito con magnete 1 , 5 t ( symphonia , siemens , erlangen , germania ) in condizioni basali e con somministrazione di mezzo di contrasto in fase arteriosa , venosa e tardiva . 
gadoterate meglumina ( gd - dota , dotarem , guerbet , aulnay - sous - bois , francia ) stato iniettato per via endovenosa ad una dose di 0 , 2 mmol / kg . 
 nella fase pre - contrasto , sono state espletate sequenze t1 e t2 - dipendenti , acquisite con gradiente - echo ( gre ) fat saturation ( fs ) e fast spin - echo , e tr / te ( ms / ms ) , pari rispettivamente a 107 / 4 , 8 e 4950 / 102 . 
lo spessore di fetta stato 5 , 5 mm per le immagini t1 - dipendenti e 7 mm per quelle t2 - dipendenti , con slice - gap variabile ( 0 , 5 e 0 , 7 , rispettivamente )  . 
in fase arteriosa , come stabilito dalla tecnica timing run , stata utilizzata una sequenza t1 ( vibe ) dipendente volume ( tr / te : 107 / 4 , 8 ms ) ; in fase venosa le immagini , ottenute con la stessa sequenza , sono state acquisite con un ritardo di 65 secondi dallinizio delliniezione . 
 interpolated breath - hold lesame cprm stato condotto dopo somministrazione orale di 100 ml di agente superparamagnetico ( ferumoxsil , lumirem , guerbet , francia ) , con sequenze t2 - dipendenti rapid acquisition with relaxation enhancement - turbo spin echo ( rare - tse ) nei piani para - assiali e coronali con i seguenti parametri : tr / te : 4500 / 991 ; turbo factor : 410 ; campo di vista , 350 mm ; matrice , 410512 ; 64 mm di spessore di fetta . 
considerando la pi alta risoluzione spaziale , lo studio cprm stato effettuato utilizzando una sequenza 3d half - fourier acquisition single - shot turbo spin - echo 1220 radiol med ( 2009 ) 114 : 12141231 300 mm ; matrix 256256 interpolated ; 64 - mm - thick slab ; 0.95 - mm - thick partitions . a dynamic mrcp examination during secretin ( secrelux , goldham - bioglan , zusmarhausen , germany ) intravenous administration at 1 iu / kg was performed . 
after secretin stimulation , a 64 - mm t2 - weighted thick - slab rare sequence was repeated every 30 s for 5 min and every 60 s for other 5 min , reaching a total of 15 images . at the end of the dynamic phase , the same 3d t2 - weighted haste sequence with respiratory triggering , described above , was acquired in the paracoronal plane . image analysis two radiologists ( gc , rm ) skilled in abdominal imaging with 11 and 15 years of experience , respectively , in abdominal radiology , and blinded to the laboratory and histological data , independently reviewed all the examinations at the workstation in separate sessions . 
firstly , they evaluated the conventional mr images for parenchymal abnormalities , such as focal / diffuse enlargement of the pancreatic gland and / or signal intensity alterations of pancreatic parenchyma compared with those of the liver and spleen at the same level , peripancreatic oedema , early enhancement after contrast - medium administration and presence of delayed enhancement or peripheral rim and vascular involvement ( narrowingcompression of the vessels shown by decrease in signal intensity of perivascular fat )  . 
in particular , the imaging studies were analysed for the following features : dilation of common bile duct ( > 5 mm in normal fasting patients ; > 11 mm in patients with previous surgery ) focal , segmental or diffuse narrowing ( < 1 mm ) of the mpd , focal or diffuse dilation ( > 4 mm ) of the mpd and of the branch ducts . 
i parametri utilizzati sono stati i seguenti : campo di vista 300 mm ; matrice 256256 ; 64 mm di spessore di fetta , 0 , 95 mm di spessore partizioni . 
 lo studio cprm dinamico stato condotto prima e dopo somministrazione endovenosa di 1 ui / kg di secretina ( secrelux , goldham - bioglan , zusmarhausen , germania ) con sequenza thick slab rare t2 - dipendente ( 64 mm ) , ripetuta dopo iniezione di secretina ogni 30 secondi per i primi cinque minuti e ogni 60 secondi per i successivi cinque minuti , ottenendo un numero complessivo di 15 immagini . alla fine della fase dinamica stata ripetuta la stessa sequenza 3d haste t2w nel piano para - coronale descritta in precedenza . 
 analisi delle immagini due radiologi ( gc , rm ) , con rispettivamente 11 e 15 anni di esperienza in imaging addominale , alloscuro della documentazione clinica e istologica , hanno valutato indipendentemente e separatamente tutti gli esami alla work - station ; in caso di discrepanza si raggiunto il consenso . 
le immagini sono state analizzate considerando i seguenti rilievi : ingrandimento focale / diffuso del pancreas , alterazioni focali / diffuse dellintensit di segnale del pancreas rispetto allintensit del fegato e della milza rilevabili nella stessa scansione , edema peri - pancreatico , impregnazione parenchimale dopo somministrazione di mezzo di contrasto e comparsa di impregnazione periferica con aspetto di cercine iperintenso in fase tardiva , interessamento vascolare ( riduzione dellintensit di segnale del tessuto adiposo perivascolare suggestivo di restringimento o compressione esterna del vaso ) , e infine eventuali linfonodi peri - pancreatici ( tabella 2 )  . 
 lindagine cprm stata valutata analizzando le seguenti alterazioni duttali : dilatazione del dotto biliare comune ( > 5 mm in pazienti a digiuno ; > 11 mm in pazienti con precedente intervento chirurgico ) , assottigliamento ( < 1 mm ) del dpp , focale , segmentale o diffusa , dilatazione ( > 4 mm ) del dpp e dei dotti collaterali , focale , segmentale o diffusa . 
il restringimento del calibro del dpp stato definito focale quando lassotigliamento del dotto coinvolgeva un breve tratto del dpp , segmentale quando interessava il dotto per un tratto pi ampio rispetto a quello segmentale , corrispondente ad una regione del pancreas ( vale a dire la porzione nella testa o nel corpo , coda ) , ed infine diffuso quando lintero dpp appariva assotigliato [ 4 ]  . 
the cases in which secretin administration showed neither reduction of mpd stenosis nor the duct - penetrating sign were considered unresponsive to secretin cases in which secretin administration reduced mpd stenosis , the length and number of the decreased strictures were considered . 
other parameters assessed after secretin administration were visualisation of side branches , and impairment of the pancreatic function ( based on timing and degree of duodenal filling ) according to criteria reported in the literature ( table 4 ) [ 16 ]  . 
 histopathological diagnosis histopathologic evaluation was performed by one pathologist with > 10 years of experience in pancreatic pathology . the histopathologic criteria used to diagnose aip were as follows : infiltration around small pancreatic ducts , swirling fibrosis centred around ducts and veins , and obliterative phlebitis [ 10 ]  . lymphoplasmacytic statistical analysis interessava una regione del pancreas e diffusa quando coinvolgeva lintero decorso del dpp ( tabella 3 ) [ 4 ]  . 
 nei 14 casi in cui stata somministrata secretina , gli osservatori hanno analizzato leventuale miglioramento della visualizzazione del dpp in base alla presenza , al numero e alla estensione del restringimento del dpp e la positivit del segno del dotto penetrante [ 4 , 15 ]  . 
i casi in cui dopo secretina il tratto di dpp assotigliato e stenotico diventava meglio definito , irregolare ma non ostruito , riacquistando la continuit nel suo decorso che prima non era visualizzable , sono stati considerati positivi per la presenza del segno del dotto penetrante [ 15 ]  . 
i casi in cui dopo somministrazione di secretina non si rilevato n la riduzione della stenosi del dpp , n il segno del dotto penetrante sono stati considerati non responsivi alla secretina . 
gli altri parametri di valutazione dopo somministrazione di secretina sono stati : visualizzazione dei dotti collaterali , alterazioni della funzionalit esocrina pancreatica ( in base al tempo e grado di riempimento duodenale ) secondo i criteri riportati in letteratura ( tabella 4 ) [ 16 ]  . interobserver variability in determining the extent of parenchyma involvement as modification of normal signal intensity was assessed with - statistics . 
the strength of agreement was assessed as follows : values of 0.20 represented poor agreement ; 0.20.40 fair agreement ; 0.410.60 diagnosi patologica lesame patologico stato effettuato da un patologo con pi di 10 anni di esperienza in patologia pancreatica . 
axial t1 - weighted ge image ( a ) shows diffuse enlargement of the pancreas ; axial t2 - weighted image ( b ) shows increased signal intensity of peripancreatic fat tissue ( peripancreatic oedema ; arrows in b )  . 
immagine gre t1 - dipendente nel piano assiale ( a ) : diffuso allargamento del pancreas . immagine t2 - dipendente nel piano assiale ( b ) : aumentata intensit di segnale del tessuto adiposo peripancreatico ( edema peripancreatico : frecce in b )  . dopo somministrazione di mezzo di contrasto ( mdc ) , in fase tardiva , limmagine gre t1 - dipendente fs nel piano assiale ( c ) mostra impregnazione pancreatica periferica ( cercine iperintenso di impregnazione : frecce in c ) , reperto tipico nella pancreatite autoimmune . 
immagine gre t1 - dipendente fs nel piano assiale ( e ) , espletata 28 giorni dopo lassunzione di terapia steroidea , evidenzia una riduzione del volume pancreatico ; il dotto pancreatico principale visualizzabile lungo lintero decorso ( cprm , f )  . 1224 radiol med ( 2009 ) 114 : 12141231 fig . 
mrcp examination ( d ) shows stenosis of cbd in the intrapancreatic portion , with marked dilation of the bile duct upstream , and mpd narrowing at the head with irregular dilation at the body - tail associated with dilation of collateral branches . 
immagine gre t1 - dipendente fs nel piano assiale ( a ) : allargamento focale della ghiandola pancreatica localizzato alla testa ove lintensit del segnale diminuita rispetto a quella del parenchima epatico e splenico . 
dopo somministrazione di mdc , in fase tardiva , limmagine gre t1 - dipendente fs nel piano assiale ( c ) mostra un restringimento della confluenza portomesenterica ( freccia in c )  . 
lindagine cprm ( d ) , evidenzia una riduzione del calibro del dotto biliare comune nella porzione intrapancreatica con marcata dilatazione dei dotti biliari a monte e un restringimento del dpp nel tratto della testa con irregolare dilatazione al corpo - coda associata a estasia dei rami collaterali . 
la forza di accordo stata valutata come segue : scarso accordo per valori di minori o uguale a 0 , 20 ; accordo equo tra 0 , 200 , 40 ; accordo moderato tra radiol med ( 2009 ) 114 : 12141231 1225 fig . 
immagine gre t1 - dipendente fs nel piano assiale ( a ) : diminuzione dellintensit di segnale proveniente dal corpo - coda del pancreas con solo lieve allargamento del volume della ghiandola pancreatica . 
dopo somministrazione di mdc , immagine gre t1 - dipendente fs nel pianio assiale ( b ) : linfonodo globoso adiacente alla vena porta ( freccia in b )  . 
il calibro a livello della confluenza portomesenterica ridotto a causa dello stretto rapporto con la lesione pancreatica , meglio visualizzabile nella immagine coronale gre t1 - dipendente fs ( freccia in c )  . 
the features of the mpd are shown in table 3 . secretin - enhanced mrcp was performed in 4 / 8 patients with diffuse - type aip ( 50% ) ( table 4 )  . 
in the remaining 3 / 4 patients ( 75% ) , two with segmental irregular narrowing of the mpd and one with diffuse mpd dilation , secretin administration did not change the mpd calibre as depicted on presecretin mrcp ( table 4 )  . 
after contrast medium administration , enhancement of the pancreas was homogeneously reduced compared with the spleen and adjacent unaffected parenchyma in all patients ( 20 / 20 ; 100% )  . 
in 1 / 8 pazienti ( 12% ) era presente compressione della confluenza portomesenterica e in un altro paziente ( 1 / 8 , 12% ) linfonodi aumentati di volume ( tabella 2 )  . 
 lo studio cprm con secretina stato eseguito in 4 / 8 pazienti con aip di tipo diffuso ( 50% ) ( tabella 4 ) e ha rilevato le seguenti modificazioni . 
in un caso ( 1 / 4 , 25% ) , che aveva un irregolare assottigliamento di un segmento del dpp , dopo somministrazione di secretina era apprezzabile il segno del dotto penetrante . 
nei restanti 3 / 4 pazienti ( 75% ) , 2 dei quali con irregolare restringimento segmentale del dpp e laltro con diffusa dilatazione del dpp , la somministrazione di secretina non ha avuto alcun effetto sullaspetto morfologico del dpp ( tabella 4 )  . 
 aip di tipo focale nei casi di aip focale ( 20 / 28 casi : 71% ) nelle immagini t1dipendenti fs il parenchima pancreatico presentava una focale diminuzione dellintensit del segnale e appariva ipointenso rispetto alla milza e al parenchima pancreatico adiacente . 
lalterazione dellintensit del segnale era localizzata nella porzione testa in 14 / 20 pazienti ( 70% ) ( fig . 2a ) e nel corpo - coda in 6 / 20 pazienti ( 30% ) ( tabella 2 )  . nelle immagini t2 - dipendenti , un alone periferico iperintenso stata osservato in 4 / 20 pazienti ( 20% )  . 
dopo iniezione di mezzo di contrasto , limpregnazione della parte di pancreas coinvolta risultata diminuita rispetto al parenchima sano adiacente e alla milza in tutti i pazienti ( 20 / 20 , 100% )  . 
sia nei pazienti con dilatazione delle vie biliari che in quelli con stent biliare , la lesione era localizzata nella testa pancreatica ; nei pazienti con lesione localizzata al corpocoda le via biliare intra ed extra - epatica era normorappresentata ( tabella 3 )  . 
in un altro caso ( 10% ) con restringimento multifocale , in pi punti della porzione del corpo - coda , dopo somministrazione di secretina si rilevato la diminuzione del numero di stenosi . 
in 1 / 10 pazienti ( 10% ) con focale restringimento del dpp nella coda , la somministrazione di secretina non ha avuto alcun effetto sul calibro del dotto e la morfologia del dpp rimasta invariata . 
nei rimanenti 2 / 10 pazienti ( 20% ) che avevano un dpp dilatato rispettivamente nella porzione della testa e del corpo , dopo somministrazione di secretina si resa evidente la estasia dei dotti pancreatici collaterali ( tabella 4 )  . 
dopo iniezione di secretina ( b ) , il dotto pancreatico principale dimostrabile lungo tutto il suo decorso con visualizzazione del segmento della testa , non identificabile pre - secretina , grazie alla riduzione della stenosi ( frecce in b , segno del dotto penetrante )  . discussione the body , after secretin administration , there was a decrease in length of the stenosis . 
in 1 / 10 ( 10% ) patients who had mpd segmental irregular narrowing with multiple stenosis in the body - tail , secretin administration showed a reduction in number of the stenoses . 
in 1 / 10 patients ( 10% ) who had focal narrowing of mpd in the tail , administration of secretin did not change the mpd calibre as depicted on presecretin mrcp . 
in the remaining 2 / 10 patients ( 20% ) who had mpd dilation in the head ( n = 1 ) and in the body la pancreatite autoimmune una malattia infiammatoria del pancreas , non comune ( 4 , 6%6% delle pancreatiti croniche ) , con eziopatogenesi autoimmunitaria , di recente scoperta e in via di definizione [ 2 , 17 ]  . 
nella presente serie sono stati retrospettivamente analizzati i rilievi rm , cprm , e cprm con secretina in ragione del fatto che il comportamento delle pancreatiti autoimmuni allindagine cprm con secretina non stato ancora documentato e potrebbe fornire 1228 radiol med ( 2009 ) 114 : 12141231 ( n = 1 ) , dilation of collateral branches was appreciable after administration of secretin ( table 4 )  . in all patients , secretin administration showed preserved exocrine pancreatic function . 
as demonstrated by normal duodenal filling ( table 4 )  . discussion inflammatory involvement of the pancreas caused by autoimmune reaction is a recent pathological entity that is still incompletely understood [ 2 , 17 ]  . 
in this study , we performed a retrospective determination of mr , mrcp and secretin - mrcp findings . the use of mrcp after secretin administration for aip is a new method that has not been previously reported , and evaluation of aip by this method may provide important information . 
according to the literature , aip predominantly affects the elderly male population , with relatively mild symptoms compared with the acute abdominal pain accompanying forms of acute pancreatitis [ 3 , 4 ]  . 
the incidence of associated autoimmune diseases and the detection rate of autoantibodies show variable values ranging from 12% to 50% [ 24 ] and from 10% to 100% [ 1820 ] , respectively . 
we found associated autoimmune disease in 39% of cases and autoantibodies in 6% of cases only . in agreement with the literature [ 3 , 4 , 10 , 1922 ] , in our series we noted a male predominance ( 64% )  . 
although the diffuse form is the most frequently reported in the literature [ 6 , 10 , 11 , 21 , 23 ] , in our series the focal form of aip was more common . 
this may be due in part to the fact that we are a referral centre for pancreatic surgery , but it also reflects the fact that the focal form of aip still represents a major diagnostic challenge . 
 [ 11 ] : once again , we believe that being a referral centre for pancreatic surgery contributes to the selection of younger patients with suspected pancreatic tumour who could successfully undergo radical intervention . 
on the other hand , the younger age of the patients with focal aip is consistent with some reports of progression from segmental to diffuse disease observed on serial ercp without steroid importanti elementi diagnostici . 
in letteratura riportato che le pancreatiti autoimuni colpiscono prevalentemente le persone anziane di sesso maschile , con sintomi lievi in confronto agli attacchi di dolore addominale che si accompagnano alle forme di pancreatite acuta [ 3 , 4 ]  . 
la pancreatite autoimmune si associa ad altre malattie autoimmuni e allinnalzamento del tasso sierico di auto - anticorpi in un numero variabile di casi con incidenza rispettivamente del 12%50% [ 24 ] , e del 10%100% [ 1820 ]  . 
 in accordo con la letteratura [ 3 , 4 , 10 , 1922 ] , la popolazione colpita stata in prevalenza maschile ( 64% ) ; tuttavia , altri dati sono diversi da quanto rilevato nei precedenti lavori . 
let media era di 45 anni , quindi pi giovane rispetto a quella di 5568 anni riportata in altre esperienze [ 3 , 4 , 6 , 1922 ]  . 
inoltre , nonostante la forma diffusa di aip venga riportata come quella pi comune [ 6 , 10 , 11 , 21 , 23 ] , nella serie esaminata la forma focale di aip risultata pi numerosa . 
la preponderanza della forma focale di aip imputabile in parte al fatto che la casistica stata raccolta in centro di riferimento per la chirurgia del pancreas , ma dallaltra al fatto che le aip focali rappresentano ancora un importante problema diagnostico . 
 [ 11 ] probabilmente perch un centro specializzato in chirurgia pancreatica contribuisce alla selezione di giovani pazienti con sospetto tumore del pancreas , che potrebbero essere sottoposti con successo a intervento radicale . 
daltro canto , per , la giovane et dei pazienti con aip di tipo focale in linea con la teoria della progressione temporale della malattia , il cui esordio sarebbe localizzato e in assenza di trattamento medico diffonderebbe al resto del pancreas [ 4 , 22 , 2426 ] , suggerendo quindi che la forma focale e quella diffusa di aip siano spettro della stessa malattia piuttosto che di entit distinte [ 4 ]  . 
 nella presente serie , non tutti i pazienti con aip mostravano ipertrofia pancreatica ; in 4 casi vi era una modificazione dellintensit di segnale del parenchima non accompagnata da un aumento dimensionale della porzione di pancreas corrispondente . 
 dopo iniezione di mezzo di contrasto , limpregnazione radiol med ( 2009 ) 114 : 12141231 1229 treatment [ 4 , 22 , 2426 ] , suggesting than the different types are a spectrum of the same disease rather than separate entities [ 4 ]  . in our study , not all patients with aip had enlargement of the pancreas . 
these findings probably suggest earlier onset of signal intensity alteration compared with glandular enlargement in focal aip . after contrast medium administration , pancreatic enhancement was delayed in all cases , and a capsule - like smooth rim was seen in eight patients ( 28% )  . 
in our study , mr imaging identified the peripheral rim in a higher number of cases ( n = 8 ; 28% ) compared with other ct series [ 6 , 24 , 27 ] and more frequently in focal aip compared with diffuse aip ( seven focal aip vs one diffuse aip ) [ 13 ]  . 
moreover , the review of ercp features from the literature [ 22 ] of aip suggests that its typical appearance is not only diffuse irregular narrowing of the mpd but also segmental irregular narrowing that may advance to diffuse irregular narrowing . 
even if the role of mrcp may appear to be limited in diagnosing aip ( the entity being a narrow - duct disease ) [ 4 ] and mrcp cannot differentiate mpd irregular narrowing of aip from the stenosis of pancreatic carcinoma [ 22 ] , the administration of secretin opens new perspectives in the utilisation of mrcp as a diagnostic tool for the differential diagnosis of aip and inflammatory pancreatic disease versus pancreatic cancer [ 4 , 15 ]  . the focal type of aip is difficult to differentiate from pancreatic carcinoma on the basis of morphological features and early enhancement pattern , and due to these difficulties , most of these forms undergo surgery [ 28 ]  . 
the associated findings such as elevation of tumour markers , focal mass forming , dilatation of mpd and common bile duct upstream ( the double - duct sign ) , together with vascular encasement , can raise further concern for malignancy [ 12 , 29 , 30 ]  . 
also in our study , 56% of focal aip of the head had the diagnosis of pancreatic suspicious findings for del pancreas risultata ritardata in tutti i casi e il cercine periferico di enhancement stato osservato in 8 pazienti ( 28% )  . 
limpregnazione periferica tardiva un reperto distintivo della pancreatite autoimmune e utile nella diagnosi differenziale con il carcinoma ; in questa casistica studiata con indagine rm , il cercine di impregnazione periferica stato individuato in un numero pi elevato di casi ( 8 casi , 28% ) rispetto ad altre serie esaminate con indagine tc [ 6 , 24 , 27 ] , e pi frequentemente nelle aip focali rispetto alla forma diffusa ( in particolare in 7 casi di aip focale vs 1 caso di aip diffusa ) [ 13 ]  . 
il restringimento del tratto distale del dotto biliare comune una evenienza frequentemente descritta nelle pancreatiti autoimmuni [ 21 ]  . in modo analogo , la dilatazione delle vie biliari stata osservata in 5 pazienti con aip diffusa ( 63% ) e in 7 pazienti con aip focale della testa ( 50% ) mentre nessuna anomalia biliare stata rinvenuta nei casi di aip del corpo e della coda del pancreas . 
dalla disamina della letteratura [ 22 ] emerge che laspetto tipico del dpp nelle aip non solo quello di diffuso ed irregolare restringimento , ma anche quello di assottigliamento segmentale , cio pi breve e sfumato , che pu progredire fino alla stenosi diffusa . 
il contributo della indagine rm nellinquadramento delle malattie del pancreas deriva dalla possibilit di ottenere uno studio parenchimale e dei vasi sanguigni in modo simile alla tc e , con lo studio cprm , una rappresentazione dei dotti biliari e del pancreas . 
anche se lapporto dellindagine cprm pu apparire limitato nella diagnosi di aip essendo questa una patologia che si manifesta prevalentemente con un restringimento dei dotti [ 4 ] e non potendo differenziare il restringimento provocato da aip dalle stenosi neoplastiche [ 22 ] , luso dello stimolo secretinico apre nuove prospettive di utilizzo della cprm come strumento di diagnosi differenziale tra le aip e il carcinoma pancreatico [ 4 , 15 ]  . 
 la pancreatite autoimmune di tipo focale infatti difficile da distinguere dal carcinoma pancreatico sulla base dei reperti morfologici e del pattern di impregnazione in fase precoce , tanto che , a causa di queste difficolt , la maggior parte delle aip focali sottoposta a intervento chirurgico [ 28 ]  . 
la combinazione di rilievi quali aumento dei marcatori tumorali , alterazione espansiva del pancreas formante massa , dilatazione del dpp e del dotto biliare comune a monte del restringimento ( segno del doppio dotto ) , insieme con la compressione dei vasi peri - pancreatici possono destare il sospetto di malignit [ 12 , 29 , 30 ]  . anche nella presente casistica , il 56% delle aip focali della testa aveva caratteri macroscopici sospetti per carcinoma del pancreas ; in particolare , 2 pazienti con aip focale della testa ( 14% ) mostravano un innalzamento del ca - 19.9 e una 1230 radiol med ( 2009 ) 114 : 12141231 carcinoma . 
the other three patients with focal aip of the head ( 21% ) had increased ca 19 - 9 alone , and another three patients with focal aip of the head ( 21% ) had stenosis of peripancreatic vessels alone . the role of mrcp in the morphological evaluation of the pancreatic duct has been extensively demonstrated in the literature [ 14 , 30 , 3134 ]  . 
mr imaging with mrcp is superior to both mr imaging alone and ct in differentiating focal aip from carcinomas , considering that focal aip tends to have an irregular , but not obstructed , mpd , which tends to penetrate the mass after secretin administration , the socalled duct - penetrating sign [ 15 , 30 ]  . 
consequently , it increases fluid in the pancreatic duct and its delineation is improved at mrcp . the use of dynamic mrcp with secretin has already proven useful to visualise the pancreatic duct and evaluate the behaviour of the mpd [ 15 , 3134 ]  . 
in six cases in particular , in one case of diffuse aip and in five cases of focal aip of the head ( 43% of all aip and 50% of focal aip ) the mpd segmental or focal stenosis resolved during the dynamic study showing the duct - penetrating sign . 
in those cases , especially in the focal aip of the head with no typical sausage - like pancreatic enlargement , the administration of secretin was of paramount importance in excluding a ductal adenocarcinoma and avoiding unnecessary surgical intervention . 
moreover , considering the relatively small number of patients , it is difficult to assess the statistical significance of the imaging findings . in conclusion , in the right clinical scenario , conventional mr imaging with mrcp allows precise classification of the aip in most cases , thanks to the demonstration of the late rim enhancement and the behaviour of the stenotic biliary and pancreatic ducts , particularly after secretin stimulation . for these reason , we suggest mr imaging with mrcp in suspected aip , and especially in the presence of a focal pancreatic lesion mimicking a ductal adenocarcinoma . 
the administration of secretin represents a problem - solving tool capable of demonstrating the integrity of the mpd along with preserved pancreatic function , thus enabling a correct diagnosis . stenosi dei vasi peripancreatici , altri 3 pazienti con aip focale della testa ( 21% ) presentavano solo ca - 19.9 aumentato e gli altri 3 pazienti con aip focale della testa ( 21% ) avevano una stenosi dei vasi peripancreatici isolata . 
lo studio rm con cprm superiore allindagine rm e tc nella differenziazione delle forme di aip focale dai carcinomi visto che la aip focale si caratterizza per un dpp irregolare , assotigliato , ma non ostruita che tende a penetrare la massa , ridisegnandone la continuit dopo stimolo secretinico , il cosiddetto segno del dotto penetrante [ 15 , 30 ]  . 
lo stimolo secretinico aumenta la secrezione di fluidi nel sistema duttale e contemporaneamente aumenta il tono sfinteriale delloddi incrementando quindi la quantit di liquido nel dotto pancreatico e migliorandone la visualizzazione con cprm . 
lo studio cprm con secretina si gi dimostrato utile per la delineazione del dotto pancreatico e per la valutazione del comportamento dinamico del dpp [ 15 , 3134 ]  . 
in 6 casi , nel dettaglio , in 1 caso di aip diffusa e in 5 casi di aip focale della testa ( ovvero nel 43% della casistica globale e nel 50% delle aip focali ) , il restringimento segmentale focale del dpp si risolto dopo lo stimolo secretinico , indicando che il dotto era penetrante . 
in questi casi , soprattutto nelle aip focali della testa , la somministrazione di secretina stata di fondamentale importanza per escludere un adenocarcinoma duttale , e per eludere la necessit di intervento chirurgico . 
 tuttavia , questo studio presenta inevitabili limitazioni . in primo luogo , la popolazione esaminata comprende solo casi di aip e , in secondo luogo , essendo una valutazione retrospettiva , non tutti i pazienti sono stati sottoposti alla prova con secretina . 
 in conclusione , in presenza di un appropriato contesto clinico , le indagini rm e cprm consentono lesatta classificazione della pancreatite autoimmune nella maggior parte dei casi , grazie alla dimostrazione del cercine di impregnazione periferica e al pattern di restringimento duttale del sistema biliare e pancreatico e alle modificazioni indotte dalla stimolazione con secretina . 
i valori di attenuazione medi degli insulinomi e del pancreas normale nelle fasi precontrastografiche arteriosa e portale erano , rispettivamente , pari a 40 , 58 , 75 uh , 114 , 4827 , 30 uh , 112 , 1919 , 52 uh e 44 , 566 , 48 uh , 81 , 1615.22 uh , 90 , 5413 , 80 uh , con differenze statisticamente significative in tutti i casi ( p < 0 , 000 )  . 
lenhancement degli insulinomi nelle fasi arteriosa e portale era pari a 74 , 0329 , 51 uh e 70 , 9021 , 93 uh , rispettivamente , senza differenze statisticamente significative ( p = 0 , 499 )  . 
lacquisizione delle immagini nella fase arteriosa la pi utile nel riconoscimento di questi tumori . radiol med ( 2009 ) 114 : 12321238 1233 keywords pancreas pancreas neoplasms insulinomas computed x - ray tomography parole chiave pancreas tumori pancreatici insulinomi tomografia computerizzata introduction insulinoma is the most common syndromic pancreatic endocrine tumour . 
in addition , patients may report symptoms such as paroxysmal headache , tiredness , palpitations , sweating , fainting and morning unconsciousness [ 1 ]  . surgery is the preferred treatment , and patients may have a long survival without symptoms . 
some experts believe that because an insulinoma has been confirmed biochemically , preoperative imaging is not necessary , as nearly all insulinomas are located in the pancreas and can be detected with intraoperative inspection , palpation and sonography . 
for example , insulinomas located near the surface of the gland may undergo simple enucleation ; however , if tumours are located deep in the gland , partial pancreatectomy may be required . 
thus , if the sensitivity of noninvasive preoperative imaging improves , preoperative imaging evaluation is essential to insulinomas [ 3 ]  . along with the development of multidetector - row computed tomography ( ct ) and improvement and optimisation of scanning techniques , we are now able to rapidly image the pancreas during multiple phases of contrast enhancement . 
some experts have shown improved conspicuity of islet - cell tumours during the arterial phase of enhancement , whereas others have shown portal - venous - phase imaging to be more beneficial [ 35 ]  . 
 the aims of this study were to review our experience in the preoperative detection of insulinomas by using pancreatic thin - section dual - phase helical ct technology , quantitatively determine the enhancement characteristics and relative conspicuity of insulinomas in the different phases of pancreatic enhancement , establish the ability of multidetector - row ct to localise these tumours , and analyse the cause of false negative findings on multidetector helical ct . 
 materials and methods patients during the 6 - year period from 2002 to 2007 , 56 patients suspected of having insulinoma on the basis of clinical symptoms and laboratory data underwent surgery , and in 52 cases the insulinoma was proved by pathology . 
all patients in our study group presented with classic whipples triad , and most of them suffered from paroxysmal headache , weakness , palpitations , sweating , fainting , blurring of vision or morning unconsciousness . 
 ct acquisition all 46 patients underwent contrast - enhanced scanning with a 4or 16 - detector helical ct scanner ( light speed , ge healthcare ) ; ten patients ( group 1 ) only underwent portal - phase ct scanning , and the remaining 36 patients ( group 2 ) underwent dual - phase ct scanning . 
all patients were administered 500800 ml of water 30 min prior to the study and an additional 250300 ml of water immediately prior to the study to achieve adequate distension of the stomach and duodenum . the unenhanced ct acquisition was obtained with slice thickness and slice intervals of 7.5 mm ( 250 ma , 120 kv ) , and the enhanced ct acquisition was obtained with slice thickness and slice intervals of 3.755 mm ( 280300 ma , 120 kv ) covering the liver and pancreas . 
 all patients were given nonionic iodinated contrast material ( omnipaque 300 mg i / ml , ge healthcare ) administered with a power injector ( ulrich medical , germany ) at a rate of 34 ml / s through a 21 - gauge angiocatheter placed in an antecubital vethe volume of contrast material delivered was 90120 ml . dual - phase ct acquisition used a bolus - tracking 1234 radiol med ( 2009 ) 114 : 12321238 program ( smartprep , ge healthcare ) that monitored contrast enhancement after injection of contrast medium before initiation of the diagnostic scans . 
real - time lowdose ( 120 kvp , 50 ma ) serial monitoring scanning was initiated 1012 s after the start of the contrast injection , and the scanning threshold value was set at 80 hu . 
when the ct value of the aorta was > 80 hu , the arterial - phase acquisition was triggered , and the portal - phase acquisition was started 30 s after arterial phase acquisition . surgical and pathologic analysis we reviewed the surgical and pathology reports providing the diagnosis based on the gross , microscopic and immunohistochemical examination of surgical tissues . 
one roi was obtained from the lesion on corresponding unenhanced , arterial and portal - venous phases , and three rois that excluded lesions and edges of the organ , and vascular or ductal structures were obtained from homogeneous areas of the head , body and tail of the pancreas for a same section . 
then , the attenuation values were averaged , and lesion contrast enhancement was obtained by subtracting the average attenuation value on unenhanced images from the average attenuation value on contrast - enhanced images . 
students t test was used for qualitative analysis , and p0.05 were considered statistically significant . results surgical and pathology findings thirty - six patients were treated with pancreatic insulinoma enucleation or resection , two patients with pancreatic insulinoma enucleation under celioscopy , six patients with partial pancreatectomy and two patients with the child procedure . all patients were affected by insulinoma , as proved by the pathology reports describing the gross , microscopic and immunohistochemical examination of surgical tissues . imaging studies tumour detection sensitivities of ct for detecting insulinomas are listed in table 1 . 
dual - phase helical ct ( group 2 ) was significantly superior to single - phase helical ct ( group 1 ) ( 2 = 4.064 ; p = 0.044 ) with regard to sensitivity for depicting pancreatic insulinoma . 
1 caso di insulinomi multipli , due dei quali localizzati nella testa e uno nella coda del pancreas . radiol med ( 2009 ) 114 : 12321238 1235 pancreas : 15 ( 32.6% ) were located in the head of the pancreas , seven ( 15.2% ) in the neck , 13 ( 28.3% ) in the body and 11 ( 19.6% ) in the tail in 44 patients ; another two ( 4.3% ) tumours were ectopic in two patients and located near the left and right kidney , respectively . 
la massa della coda del pancreas appare isodensa nellesame senza mezzo di contrasto . essa presenta enhancement marcato nella fase arteriosa e lieve nella fase venosa portale . defined edges ( n = 31 / 86.1% ) and only five ( 13.9% ) had illdefined edges . 
contrast enhancement differences between the normal pancreas and the lesions were significantly higher during the arterial phase than the portal - venous phase ( p = 0.011 ) , resulting in greater tumour conspicuity . most insulinomas were hyperenhancing on at least one of the postcontrast phases ( n = 36 ) ; 28 ( 77.8% ) of them enhanced homogeneously , three ( 8.3% ) enhanced inhomogeneously and five ( 13.9% ) showed circular enhancement with filling in the portal venous phase . 
5 il grafico evidenzia l ' incremento medio di densit degli insulinomi e del pancreas normale e della differenza di contrasto tumore / pancreas nelle fasi precontrastografica , arteriosa e venosa portale . unenhanced phase portal investigated the enhancement characteristics of pancreatic insulinomas . 
 [ 5 ] reported that portal - venous - phase images were more helpful than arterial - phase images for detecting pancreatic islet - cell tumour on the basis of receiver operating curve analysis of qualitative data . 
 [ 8 ] reported that the sensitivity for detecting pancreatic adenocarcinoma was significantly greater during the pancreatic than the arterial phase and that the mean attenuation of the pancreas in all patients was greatest in the pancreatic phase at 107 hu versus 65 hu in the arterial phase . 
further studies will be necessary to assess this issue for detecting insulinomas . other investigators have shown good sensitivities with other modalities , such as magnetic resonance imaging ( mri ) and endoscopic sonography [ 5 , 6 , 1016 ]  . 
 [ 5 ] found that mri and biphasic ct had similar effectiveness in detecting islet - cell tumours . 1238 radiol med ( 2009 ) 114 : 12321238 gouya et al . 
 [ 6 ] found that the diagnostic sensitivity for dual - phase helical ct and endoscopic sonography was > 90% and for combined biphasic thin - section helical ct and endoscopic sonography was 100% . 
however , in our experience , pancreatic biphasic helical ct with thin sections is the preferred modality for suspected insulinomas . if there is a contraindication to ct or negative findings on ct , we will perform mri examination . 
in addition , the study may have had a selection bias , as some patients may not undergo ct examination if other modalities were performed , such as mri or endoscopic sonography as the initial modality and had positive results . 
therefore , our results cannot indicate the absolute sensitivity of ct in the prospective diagnosis of pancreatic islet - cell tumours . we can draw several conclusions from our evaluation of a biphasic multidetector - row ct protocol for detecting pancreatic insulinomas . 
first , dual - phase ct has a promising sensitivity in detecting pancreatic insulinomas . second , the acquisition of images in the arterial phase is helpful to detect insulinomas because tumour - to - gland attenuation differences are significantly conspicuous . finally , using a standard and uniform ct scanning technique and being aware of atypical appearances such as isoattenuating , extruded , pedunculated or ectopic insulinomas will help obtain the highest possible sensitivities . 
hence they require a multidisciplinary and multispecialty approach , which must begin with an accurate medical examination , conducted in compliance with the lege artis principles and with respect for the victims dignity . 
this paper describes the radiologists key role in identifying physical injuries due to child abuse , in accordance with current regulations . keywords child abuse forensic radiology battered child syndrome riassunto labuso ed il maltrattamento sui minori una tematica di grande attualit con notevoli risvolti di carattere sociosanitario che interessano il medico sia come cittadino che in qualit di esercente una professione sanitaria . 
la molteplicit e la peculiarit di alcune lesivit di abuso , siano queste di tipo fisico , psichico o sessuale necessitano di un approccio multidisciplinare e polispecialistico che non pu prescindere tuttavia da una visita medica che , nel rispetto della dignit della presunta vittima , sia effettuata secondo i criteri propri della lege artis . 
il presente articolo descrive il ruolo del radiologo nella valutazione degli abusi fisici perpetrati a danno di minori alla luce della normativa vigente . parole chiave abuso sui minori radiologia forense sindrome del bambino battuto introduction introduzione in 1946 , radiologist john caffey following a . 
this was a concise , pragmatic definition of what is not so much a clinical syndrome as a sociocultural phenomenon that had strong repercussions on trauma medicine and on physicians themselves [ 1 ]  . 
tardieu del 1860 definiva in maniera concisa e pragmatica pi che una sindrome clinica un fenomeno socio - culturale che aveva pesanti riflessi sulla medicina traumatologica e notevoli ricadute sui medici [ 1 ]  . radiol med ( 2009 ) 114 : 13561366 1357 an accurate definition of child abuse is given in the world health report 2002 : child abuse or maltreatment constitutes all forms of physical and / or emotional illtreatment , sexual abuse , neglect or negligent treatment or commercial or other exploitation , resulting in actual or potential harm to the childs health , survival , development or dignity in the context of a relationship of responsibility , trust or power [ 2 ]  . 
therefore , child abuse includes the results not only of actions ( sexual or other kinds of violence ) but also of neglect or deprivation ( lack of care , attention , affection )  . 
in both cases , the physical examination alone , for legal purposes as well as for diagnosis and therapy , is unable to confirm or exclude suspected abuse ( at least from a medical point of view ) without the use of radiological tools . 
thus , radiology is an essential tool in medicolegal investigations of physical child abuse , which gives the specialist a proper understanding of type , extent and age of the injury , and the dynamics behind it ( aetiopathogenesis )  . extent of child abuse child abuse has become a very worrying issue with an impact on the whole of society . 
introna states : the abused child is the expression of multiple problems of a legal , cultural and economic nature involving his / her family at a given moment in time , and therefore he / she is the clue to pain that goes beyond his / her own person [ 3 , 4 ] as requested . child abuse is often rejected or negated , and it is always underreported . 
this is especially true in southern italy , where it often occurs within a complex family setting , which makes it difficult to evaluate the victim and type of abuse suffered . 
the child presents distinctive injuries , often inflicted with bare hands or by using various objects ( sticks , chains , strings , cigarettes or other sources of heat )  . 
this form of child abuse results from indeuna precisa e completa definizione pu essere tradotta dalla world health organization ( who ) che nel 2002 cos recitava : per abuso allinfanzia si intendono tutte le forme di cattiva salute fisica e / o emozionale , abuso sessuale , trascuratezza o negligenza o altro che comportino un pregiudizio reale o potenziale per la salute del bambino , per la sua sopravvivenza , per il suo sviluppo o per la sua dignit nellambito di una relazione caratterizzata da responsabilit , fiducia o potere [ 2 ]  . 
in relazione a tanto , labuso sui minori deve intendersi comprensivo sia degli atti ( violenze vere e proprie , non necessariamente sessuali ) che delle carenze e le deprivazioni ( sottrazione delle cure , dellattenzione , dellaffetto )  . 
in entrambe le ipotesi laccertamento medico , effettuato a fini giuridici lindagine oltrech diagnostico - terapeutici , utilizzer radiologica quale importantissimo strumento diagnostico per fondare ovvero escludere , quanto meno da un punto di vista medico , il sospetto di un abuso . 
lutilizzo di immagini digitali , utile ad una pi fine valutazione della lesione fisica osservata e correlato ad una specifica competenza del radiologo riguardo allepoca di mineralizzazione ossea trauma ed dei segmenti scheletrici allidoneit lesiva del trauma stesso ( eziopatogenesi ) , rende la valutazione radiologica strumento fondamentale nella valutazione medico - legale degli abusi fisici a carico di minori . interessati dal dimensioni del problema il maltrattamento dei bambini ha assunto dimensioni tali da costituire un serio motivo di preoccupazione da parte di tutta la societ civile . 
introna in un suo felicissimo intervento recita : il bambino maltrattato testimone di problemi multipli che investono il nucleo familiare in quel determinato momento storico , giuridico , culturale ed economico e quindi egli la spia di una sofferenza che va oltre la sua persona [ 3 , 4 ]  . 
questo vero soprattutto nelle regioni del sud dove la complessit dellambiente familiare , in cui , nella maggior parte dei casi , avviene tale tipologia di reati , rende estremamente difficile unesatta valutazione delle vittime e del tipo di abuso subito . 
these injuries are a sign of neglect by those responsible for the childs care because the injuries were not treated promptly and eventually became chronic . this paper focuses only on the battered child syndrome because this feature directly concern radiologists . radiological features of child abuse the radiologist is consulted during the investigation of battered child injuries , especially those related to cranial and musculoskeletal injuries , and he or she must be cognizant of the often critical features of such injuries . 
later , in 1962 , kempe coined the expression battered child syndrome [ 6 ] to group together the clinical and radiological signs of beaten children and to draw attention of the medical community to the problem , which , although steadily escalating , had been totally disregarded . incomplete or complete fractures are generally observed in the upper and lower limbs and in the ribs directly struck by blows , punches or kicks whilst the child is hunched up for self protection . 
it must be pointed out that the radiologist is always able to identify an injury but can never be absolutely sure of its mechanis nevertheless , some fractures are highly specific of the battered child syndrome , i.e. 
the knee ( proximal tibia ) , the wrist , the femur and the humerus are the most frequent sites of such fractures , which are rarely accompanied by a periosteal reaction and seldom cause growth disturbances or bending deformities [ 10 , 11 ]  . 
con questo termine si vogliono comprendere tutti quei maltrattamenti occulti costituiti da mancanza di protezione , di educazione , di amore e di accettazione che si estrinsecano con una serie di trascuratezze , rifiuti e sfruttamenti che sfociano nellabbandono psicologico ma , talvolta , possono determinare il decesso della vittima per inanizione . 
oltre alle sequele psicologiche , si possono riscontrare anche dermatosi comuni croniche da scarsa igiene , ripetute infezioni , ascessi e fistole che sono indicative della trascuratezza di chi si dovrebbe prendere cura del minore ed indicare affezioni perduranti nel tempo e non curate tempestivamente . in questo articolo tratteremo esclusivamente la valutazione specialistica degli abusi fisici sui minori ( battered child syndrome ) , i cui aspetti coinvolgono in maniera diretta e pressante lo specialista radiologo . aspetti radiologici degli abusi fisici sui minori lo specialista radiologo consultato in corso di accertamenti sul bambino battuto ( abusato da un punto di vista fisico ) , prevalentemente nei casi di violenza da trauma sullapparato cranico - muscolo - scheletrico e deve conoscerne gli aspetti , a volte del tutto peculiari , con cui questi possono palesarsi . 
 gi caffey nel 1957 aveva messo in evidenza ed illustrato alcuni nuovi e particolari tipi di frattura e di lesioni ossee che si possono riscontrare nei bambini battuti , specie nei pi piccoli [ 5 ]  . 
kempe successivamente , nel 1962 , allo scopo di puntare lattenzione del mondo scientifico su un problema sociale assolutamente trascurato , ma in fase di importante espansione , coni il termine di battered child radiol med ( 2009 ) 114 : 13561366 1359 fig . 
b frattura a manico di secchio . table 1 differential diagnosis between accidental and nonaccidental injuries abusive fractures metaphysis proximal tibia femur accidental fractures epiphysis distal tibia other sites with high energy mechanism tabella 1 diagnosi differenziale tra fratture accidentali e da abuso fratture da abuso sede metafisaria tibia prossimale femore fratture accidentali epifisi tibia distale altri siti con meccanismo elevata energia the lower limbs of children who are not ambulatory ( table 1 )  . 
 the so - called toddlers fracture , namely , the spiroidal fracture of the distal portion of the tibia , is a very common accidental injury in the paediatric age . 
on the other hand , if the same fracture is detected with identical radiological features in children not yet ambulatory , it should undeniably be considered as resulting from abuse [ 1214 ]  . 
multiple syndrome per indicare tutto il corteo di sintomi clinici e radiologici che caratterizzano gli aspetti traumatici del bambino battuto [ 6 ]  . come aspetto generale le fratture incomplete o complete interessano lo scheletro appendicolare , specie gli arti superiori ed inferiori e le coste che sono oggetto della violenza soprattutto a seguito di percosse , pugni e calci a bambini rannicchiati in atteggiamento di autoprotezione . 
raro che le lesioni scheletriche siano fatali e rare sono anche le lussazioni e le lesioni vertebrali , in ogni caso opportuno ricordare che il radiologo pu identificare la lesione , ma mai determinarne con certezza le modalit . 
tuttavia esistono alcune particolarit del tipo di fratture che possono indirizzare o far propendere il radiologo verso un trauma non accidentale e quindi da riferire a sindrome da bambino battuto . 
these are caused by traumatic anteroposterior compression of the rib cage , and the radiologist must bear in mind the fact that they cannot be caused even by the use of improper resuscitation procedures [ 1518 ]  . 
as they are extremely serious injuries , they may appear to indicate abuse , but , at the same time , they are very often associated with accidents such as tumbling out of bed , falling off the changing table or down the stairs . 
8a , b frattura lineare del parietale destro nella battered child syndrome . in the case of indirect head injuries , guthkelchi [ 24 ] made a further distinction by introducing shaken baby syndrome , in which lesions are secondary to the attendant axonal damage . when the infant is shaken violently and head movements are not synchronised with the rest of the body , in 90% of cases , this produces retinal haemorrhage , but it may also produce subdural haematoma ( related to vascular tears ) and osseous injuries ( detectable only by means of magnetic resonance imaging )  . 
 we must remember the possibility , even if remote , of finding damage to parenchymal organs , which is regularly accompanied by other types of lesions ( haematoma , pseudocyst , etc . ) that will be seen only through ultrasound or computed tomography [ 26 ]  . current regulations and forensic medicine considerations the entire medical profession , including radiologists , is bound by italian law to cooperate with police authorities to prevent and combat crime . 
evidenti le lesioni ipodense cerebrali , esiti di trauma da scuotimento . deontology code ( 2006 ) states that the doctor must protect children in cases of physical or psychological maltreatment or sexual abuse , and in the event of opposition from the legal guardians , the doctor must report to the appropriate legal authorities . 
361medici specialisti in radiodiagnostica , sono previsti , dalla legislazione attualmente vigente , obblighi giuridici finalizzati a forme di collaborazione con lautorit giudiziaria , al fine di prevenire e contrastare la criminalit . 
32 del codice di deontologia medica ( 2006 ) che prevede , oltrech una specifica tutela sui minori in casi di maltrattamenti fisici o psichici , violenze o abusi sessuali anche la possibilit in caso di opposizione dei legali rappresentanti alla necessaria cura dei minori di ricorrere alla competente autorit giudiziaria . 
 doveroso ricordare che la violazione del dovere o omissione di inoltrare il referto / rapporto costituisce un delitto contro lamministrazione della giustizia ; la mancata ottemperanza di tale dovere prevede automaticamente il reato di omissione datti dufficio qualora si accerti che il sanitario abbia , con coscienza e volont , voluto omettere o ritardare la presentazione del referto [ 28 ]  . 
failure to comply with this duty is malfeasance in office when it is ascertained that the health professional wilfully and knowingly failed to report or delayed reporting the crime [ 28 ]  . 
 conclusions too often do we hear about presumed physical , psychological or sexual child abuse based on psychological evaluations without any reference to the medical follow - up or specialistic investigations that could unequivocally confirm or exclude this suspicion . 
in fact , they have the knowledge to determine the time of mineralisation of skeletal segments , reconstruct the mechanisms of injuries to the osteoarticular system and interpret imaging findings . reporting child abuse is always a very delicate question , especially because it always involves the families . 
although a mere suspicion of abuse is sufficient for current regulations , the professional must be aware of the consequences of a misdiagnosis on the family and on the victitherefore , the radiologist is required to make both a cultural effort in understanding the problem and a methodological effort in evaluating the case in terms of collecting a complete clinical history and carefully interpreting the imaging findings . implementation of guidelines and protocols such as those proposed by the american college of radiology [ 29 ] , together with cooperation between several specialists , will help produce a methodologically flawless evaluation of the true extent of this serious problem , which has been neglected and underreported for too long . 
la particolare complessit della fenomenologia di abuso sui minori necessita , ai fini di un corretto inquadramento del fenomeno stesso , di un approccio multidisciplinare da parte di una equipe di specialisti , laddove di fondamentale importanza appare il contributo del radiologo pediatrico . 
linterpretazione delle lesioni eventualmente riscontrate con limaging non pu essere di pertinenza del pediatra ovvero dellortopedico ; solo il radiologo ha le competenze per discernere laddove possibile caratteristiche proprie di un trauma accidentale oppure di un abuso . 
infatti , la conoscenza della mineralizzazione ( epoca di ossificazione ) dei segmenti scheletrici , dei meccanismi traumatici che sottendono la genesi di lesivit soprattutto dellapparato osteo - articolare nonch la loro interpretazione diagnostica , di pertinenza del radiologo che ne certamente lunico e il migliore conoscitore . 
se da un lato la normativa vigente prevede che sia sufficiente il sospetto e non la certezza , per denunciare siffatto reato altres chiaro che una erronea diagnosi di abuso pu sconvolgere un nucleo familiare , ivi inclusa la vittima . 
allo specialista in radiodiagnostica richiesto pertanto uno sforzo culturale nei termini di comprensione / conoscenza del problema e metodologico nella valutazione di tale fenomeno che non potr prescindere dalla raccolta di un completo raccordo anamnestico , oltrech dalla successiva analisi dellimaging . 
knauth springer - verlag berlin heidelberg , 2009 isbn 978 - 3 - 540 - 72784 - 5 published online : 20 november 2009 springer - verlag 2009 this is an easy to read and very informative book on the use of contrast media in daily diagnostic practice . 
going through its 29 chapters , plus the appendix containing the european society of urogenital radiology ( esur ) guidelines on contrast media ( version 7.0 ) and one page dedicated to the official publications from the same society , provides the reader with all possible information on the use of different contrast media . the second edition of the book is the result of in depth study and research by the academic members of the esur contrast medium safety committee updating in more than one chapter , information on the use of gadolinium - based contrast media and their possible complications , in particular those related to the alarming nefrogenic systemic fibrosis ( nsf )  . 
 nsf , whose real cause is yet unknown , has come slowly to the attention of the medical community in the past few years rendering what was thought ( gadolinium contrast agents ) to be a very safe diagnostic tool as a possible , harmful instrument in the radiologists hands . since in the daily practice there is not only gadoliniumbased contrast media in use , much discussion is devoted also to the other different types of contrast media and their use . 
one will find information on ionic and non - ionic as well as barium and ultrasound contrast media , detailed information on meta - analysis in research , and information on the rules that must be followed in contrast - media research , approval , manufacturing , and clinical application . great attention is given to the discussion of contrast - media related complications : this issue is thoroughly discussed in the relevant section of many chapters and thoroughly reviewed in the esur appendix guidelines . 
one should realize that each time a contrast medium is used , however safe it might be considered , it can given the different individual conditions of the patient create adverse reactions . 
scorrendo i 29 capitoli che lo compongono , pi lappendice che elenca le linee guida della european society of urogenital radiology ( esur ) sulluso dei mezzi di contrasto nella sua pi recente versione ( 7.0 ) e la pagina dedicata allelenco delle pubblicazioni ufficiali della stessa societ , il lettore trover tutte le informazioni possibili circa luso dei diversi mezzi di contrasto . la seconda edizione il risultato di una gran lavoro di ricerca e studio da parte dei membri accademici del comitato esur sulla sicurezza dei mezzi di contrasto , lavoro che aggiorna , in particolare in pi di un capitolo , le informazioni circa limpiego dei mezzi di contrasto a base di gadolinio e le loro possibili complicanze , in particolare quelle riferibili alla pi temuta e cio la fibrosi nefrogenica sistemica ( nsf )  . la nsf , le cui cause sono ancora sconosciute , stata riconosciuta con lentezza e ritardo dalla comunit medica negli ultimi anni , rendendo quelli che erano pensati come mezzi di contrasto sicuri ( cio a base di gadolinio ) , quali possibili strumento di danno nelle mani del radiologo . dal momento per che nella pratica quotidiana non esiste solo limpiego dei mezzi di contrasto a base di gadolinio , una parte consistente del volume e di discussione viene riservata a tutti i restanti tipi di mezzo di contrasto . 
il lettore trover informazioni sui mezzi di contrasto ionici e non ionici , su quelli baritati e per impiego in ecografia : il tutto correlato da informazioni precise sulla meta - analisi nella loro ricerca ed informazioni importanti circa le regole che debbono essere impiegate nella ricerca , approvazione , preparazione ed applicazione clinica dei mezzi di contrasto . 
 grande attenzione viene dedicata alla discussione delle complicanze provocate dallimpiego dei mezzi di contrasto : questo tema viene discusso con precisione nella parti relative di molti capitoli e ben riassunta nellappendice sulle linee guida dellesur . 
ci si deve rendere conto che tutte le volte che viene utilizzato un mezzo di contrasto , per quanto sicuro lo si possa ritenere , questi pu , in funzione anche della differenti condizioni cliniche di ciascun paziente in cui viene impiegato , provocare delle reazioni , reazioni che possono essere assai lievi ed a risoluzione rapida e spontanea ma anche , 1384 radiol med ( 2009 ) 114 : 13831384 resolving over a very short period to very severe and unexpected , requiring immediate and correct treatment . how many people know the correct doses of adrenaline or atropine to be used in an emergency situation ? are there any emergency procedure - charts in your diagnostic radiology suites ? in this respect some of the pages are unnerving and hair - raising . 
 in summary , this is a very useful book and a highly recommended resource text for every radiology department , it should be easily accessible not only for the old staff radiologists but most importantly for those who are in training . al contrario , essere piuttosto evidenti ed impreviste , necessitanti un intervento terapeutico immediato e corretto . quante persone conoscono la dose corretta di adrenalina o di atropina da utilizzare in situazioni di emergenza ? nelle sale di diagnostica radiologica vi sono cartelli riportanti le procedure da seguire nelleventuale emergenza ? da questo punto di vista alcune della pagine del volume sono piuttosto preoccupanti , tali da far venire i brividi . 
giacomo , unit operativa di radiodiagnostica , monopoli , bari , italy 3universit degli studi di catania , cattedra di radiodiagnostica , azienda policlinico di catania gaspare rodolico , catania , italy correspondence to : p . 
chieffi 40 , 70051 barletta , italy , tel . : + - 39 - 340 - 0781993 , fax : + 39 - 088 - 1733866 , e - mail : paomi03@libero.it received : 11 october 2008 / accepted : 5 march 2009 / published online : 9 november 2009 springer - verlag 2009 abstract purpose . 
of these 31 patients , we included in the study 22 patients ( mean age 53 years ; range 4657 years ) who underwent liver transplantation within 1224 h after mr examination . 
dei 31 pazienti selezionati per il trapianto dorgano , sono stati inclusi nello studio 22 pazienti , di et media di 53 anni ( range 4657 anni ) , sottoposti a trapianto di fegato a distanza di circa 1224 ore dallesecuzione dellesame rm . i pazienti inclusi nello studio sono stati sottoposti ad esame rm con un apparecchio da 1 , 5 t . 
unenhanced baseline mr imaging correctly identified and characterised 20 lesions , equal to 33.90% of all lesions : 6 hcc , 12 dn and 2 dn with a subfocus of hcc . 
spio - enhanced mr imaging showed greater sensitivity detecting and characterising 45 lesions , equal to 76.27% of all lesions identified at histology : 14 hcc , 27 dn and 4 dn with subfocus of hcc . 
spio - enhanced mr imaging proved to be of value in detecting and characterising lesions in the cirrhotic liver , allowing differentiation of dn from hcc and providing an early diagnosis of neoplastic degeneration of dn . keywords spio dysplastic nodules hepatocellular carcinoma magnetic resonance imaging 14 hcc , 3 sono risultati ben differenziati , 8 moderatamente differenziati , 3 scarsamente differenziati . dei 39 nd , 28 erano a basso grado di malignit e 11 ad alto grado di malignit . 
con lesame rm di base abbiamo identificato e caratterizzato correttamente 20 lesioni , pari al 33 , 90% delle lesioni complessivamente individuate , di cui 6 hcc , 12 nd e 2 nd con foci di hcc . 
lesame rm , eseguito dopo somministrazione di mdc spio , ha mostrato una maggiore sensibilit identificando e caratterizzando complessivamente 45 lesioni , pari al 76 , 27% delle lesioni totali individuate con lesame istologico : 14 hcc , 27 nd e 4 nd con foci di hcc . 
i falsi negativi con la rm - spio sono stati 12 noduli displasici , pari al 31% , che allesame istologico sono risultati essere nd a basso grado di malignit e con diametro inferiore al c conclusioni . 
la rm con utilizzo di mdc spio , nella nostra esperienza risultata utile nella identificazione e caratterizzazione delle lesioni epatiche nel fegato cirrotico mostrandosi in grado di differenziare i noduli displasici dagli hcc e ha consentito una diagnosi precoce della trasformazione carcinomatosa dei noduli displasici . parole chiave spio noduli displasici carcinoma epatocellulare risonanza magnetica introduction introduzione cirrhosis is a progressive , diffuse disease of the liver characterised by hepatocyte necrosis , fibrosis , distortion of the normal hepatic architecture and a spectrum of nodular lesions that includes regenerative nodules ( rn ) , dysplastic nodules ( dn ) and hepatocellular carcinomas ( hcc ) [ 1 ]  . 
in italy , the likelihood of developing hcc secondary to cirrhosis ranges from 2% to 5% [ 3 ]  . in recent decades , the survival of hcc patients has been significantly increased by improvements and refinements in both nonsurgical treatments , such as percutaneous ethanol injection ( pei ) , thermoablation and lipiodol computed tomography ( ct ) ; and surgical treatments , such as liver resection and transplantation . 
the results of these treatments are , however , heavily dependent on accurate disease staging , so that the early diagnosis of hcc and its precursor , the dn , is mandatory [ 4 , 5 ]  . the screening protocol for high - risk cirrhotic patients entails ( ultrasonographic ) imaging and alpha - fetoprotein testing at 3to 6 - month intervals . 
unfortunately , an la cirrosi un progressivo e diffuso processo patologico del fegato caratterizzato da necrosi epatocitaria , fibrosi , sovvertimento della normale architettura epatica e dalla presenza di uno spettro di lesioni nodulari che include noduli di rigenerazione ( nr ) , noduli displasici ( nd ) ed epatocarcinomi ( hcc ) [ 1 ]  . 
in italia la probabilit annuale di sviluppare hcc su cirrosi epatica varia dal 2% al 5% [ 3 ]  . negli ultimi decenni si verificato un significativo incremento della sopravvivenza dei pazienti affetti da tale patologia per il miglioramento e laffinamento sia delle terapie che si basano sui trattamenti locali , come liniezione percutanea di etanolo ( pei ) , la termoablazione e la lipiodoltomografia computerizzata , sia di quelle che si basano invece su tecniche chirurgiche , quali la resezione o il trapianto . 
i risultati di queste terapie sono tuttavia fortemente condizionati dallo staging della malattia ed , quindi , estremamente importante effettuare una diagnosi precoce ed accurata dellhcc e del suo precursore , il nd [ 4 , 5 ]  . il protocollo di screening , nei pazienti cirrotici ad radiol med ( 2009 ) 114 : 12671282 1269 elevation of alpha - fetoprotein levels is neither sensitive nor specific enough to be used to screen for hcc . 
this test may , in fact , fail to detect small tumours ( < 2 cm ) , and high alpha - fetoprotein levels are seen in only 50% of patients with hcc and 26% of those with dn [ 6 , 7 ]  . imaging techniques therefore play a primary role in the diagnosis of focal lesions in the cirrhotic liver , even though there is no general agreement as to the most appropriate modality for the study of this disease . 
the literature reports conflicting data regarding not only the diagnostic capabilities of the different imaging modalities ultrasonographic ( us ) , ct and magnetic resonance ( mr ) imaging in the detection and characterisation of hcc and dn , but also the possibility of arriving at a differential diagnosis among the different lesions . 
histological analysis of the entire cirrhotic liver and a short interval between mr imaging and transplantation are factors that , if neglected , may lead to considerable variability among results . 
indeed , a long interval between mr examination and transplantation could mean the transformation of a dn into an hcc , whereas a histological examination limited to biopsies or specimens from partial liver resection could preclude identification of other nodular lesions in the liver parenchyma [ 812 ]  . in recent years , investigators have emphasised the value of hepatospecific superparamagnetic contrast agents based on iron oxide particles ( spio ) in the detection and characterisation of focal lesions with mr imaging , and their use has been advocated for staging patients scheduled for surgical or locoregional treatment of malignant focal hepatic lesions [ 13 , 14 ] and for monitoring patients with cirrhosis [ 1517 ]  . the rationale for using spio contrast agents to differentiate among the wide range of nodular lesions seen in cirrhosis is not based on vascular changes but on the cellular changes rn undergo as they develop into dn and then into hcc . 
in fact , during this process , the number and function of kupffer cells , the cells that accumulate spio , decrease [ 10 , 1820 ] , and some investigators have reported that hcc and dn show different enhancement patterns after spio administration . 
dn , on the other hand , have preserved cellular composition and function and hence greater spio accumulation , with the result that they appear markedly hypointense even relative to the surrounding liver . 
these different enhancement patterns led researchers to hypothesise that it was possible to differentiate between these two lesions and identify the transformation of a dn into an hcc at an early stage . the aim of this study was to evaluate the potential of spio - mr imaging in the detection and characterisation of elevato rischio , prevede lesecuzione di esame ecografico e dei dosaggi dellalfa - fetoproteina ( afp ) ad intervalli di 36 mesi . 
tale test , infatti , non sempre in grado di rilevare piccoli tumori ( < 2 cm ) ed elevati livelli di afp sono presenti solo nel 50% di pazienti con hcc e nel 26% di pazienti con nd [ 6 , 7 ]  . le tecniche dimaging svolgono pertanto un ruolo fondamentale nella diagnostica delle lesioni focali nella cirrosi epatica ; tuttavia non vi uniformit di vedute su quale sia la metodica pi idonea per lo studio di tale patologia . 
in letteratura sono piuttosto controversi i dati circa le reali potenzialit diagnostiche delle diverse tecniche dimaging ecografia ( us ) , tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) nella identificazione e nella caratterizzazione degli hcc e dei nd , nonch riguardo la possibilit di effettuare una diagnosi differenziale tra le diverse lesioni . questo si verifica per mancanza , in tutti i lavori finora pubblicati , di uniformit dei parametri di valutazione attendibili ; infatti , lanalisi istologica di tutto il fegato cirrotico ed il breve timing tra lesecuzione dellesame rm e il trapianto sono fattori che se non presi in considerazione possono portare una notevole variabilit nei risultati . 
infatti , un lungo tempo intercorso tra lesame rm e lesecuzione del trapianto potrebbe portare alla trasformazione di un nd in hcc , mentre uno studio anatomo - patologico limitato alle sole lesioni sottoposte a biopsia o a resezione parziale dellorgano potrebbe escludere lidentificazione di altre lesioni nodulari nel restante parenchima epatico [ 812 ]  . negli ultimi anni stata sottolineata lutilit dei mezzi di contrasto ( mdc ) superparamagnetici epatospecifici , a base di particelle di ossido di ferro ( spio ) , per lidentificazione e la caratterizzazione delle lesioni focali epatiche con rm ed il loro uso stato proposto per lo staging di pazienti da sottoporre a trattamenti chirurgici o loco - regionali per lesioni focali epatiche maligne [ 13 , 14 ] e nel follow - up dei pazienti portatori di cirrosi epatica [ 1517 ]  . il razionale di impiego dei mdc spio per la diagnosi differenziale tra il vasto spettro di lesioni nodulari presenti nella cirrosi epatica , si basa , pi che sulle modificazioni vascolari , sulle alterazioni cellulari che i nr subiscono nella loro trasformazione in nd prima e in hcc poi ; infatti , in rapporto a tale evoluzione , decrescono progressivamente il numero e la funzionalit delle cellule del kupffer , deputate alla captazione del mdc spio [ 10 , 1820 ]  . 
in relazione a tali riscontri , alcuni autori hanno rilevato un differente comportamento contrastografico con i mdc spio tra gli hcc e i nd , in quanto i primi , a causa delle alterazioni cellulari subite , non presenterebbero captazione di mdc spio , risultando marcatamente iperintensi rispetto al parenchima epatico contiguo ; i nd invece , preservando composizione e funzionalit cellulari , presenterebbero una maggiore captazione di mdc spio , apparendo francamente ipointensi anche rispetto al fegato sano limitrofo . 
tali comportamenti contrastografici hanno indotto a considerare 1270 radiol med ( 2009 ) 114 : 12671282 dn and hcc in the cirrhotic liver by correlating the findings on mr imaging performed 1224 h before liver transplantation with histopathology of the entire explanted liver . materials and methods in the setting of a screening programme for cirrhotic patients awaiting liver transplantation , we performed mr studies on 400 patients , 31 of whom had been selected for transplantation . 
prior to the mr examination , all patients received full explanation of the aims and design of the study and gave their informed consent . all patients were studied with a 1.5 - tesla unit ( magnetom 63p , siemens , germany ) using baseline proton density ( pd ) / t2 - weighted spin echo ( se ) sequences ( tr / te 2 , 0002 , 300 / 2080 ms ) , and t1 - weighted fast low - angle shot ( flash ) gradient echo ( ge ) sequences ( tr / flip angle / te 153 ms / 70 / 6 ms ) and t2 * - weighted fast imaging with steady - state precession ( fisp ) ge sequences ( tr / flip angle / te 130 ms / 40 / 10 ms )  . 
for the pd / t2weighted sequences obtained under free breathing , two acquisition and presaturation bands were positioned above and below the imaging volume so as to reduce flow artefacts . 
the t1weighted ge sequences provided a stack of 15 slices that was sufficient to study the entire liver in most patients . with the t2 * - weighted ge sequences , a stack of five slices was used so that three to four stacks were required to study the entire liver . 
in all sequences , we used a slice thickness of 8 mm with 1 - mm gap , 128256 matrix with 3 / 4 reconstruction algorithm , and 380to 450 - mm field of view . 
 following unenhanced baseline imaging , spio ( ferumoxide , endorem , guerbet , villepinte , france ) was administered by slow infusion ( 820 drops / min ) over 3045 min at a dose of 23.6 md iron per gram ( fe / g ) diluted in a 100cc flask of 5% glucose solution . 
approximately 30 - 60 min after the end of spio administration , t2 * - weighted ge sequences with the same parameters as used at baseline were obtained in all patients . the baseline and spio - enhanced images were evaluated singly and then in combination by observers blinded to the histopathological results who recorded the number and site of lesions and expressed their judgement as to the dysplastic , neoplastic or other nature of the lesions . 
for each nodule , the observers recorded signal intensity on t1and t2 - weighted images and enhancement pattern after spio administration and , based on these parameters , expressed a la possibilit di una diagnosi differenziale tra queste due lesioni , nonch di una precoce identificazione della trasformazione del nd in hcc . scopo del nostro lavoro stato quello di valutare le possibilit della rm con mdc spio nella identificazione , caratterizzazione di nd e hcc nel fegato cirrotico , confrontando i risultati della rm , eseguita nelle 1224 ore precedenti il trapianto di fegato , con lesame anatomopatologico dellintero fegato espiantato . materiali e metodi nellambito di un programma di screening di pazienti cirrotici in lista dattesa di trapianto epatico , abbiamo studiato con rm 400 pazienti , 31 dei quali sono stati selezionati in seguito al reperimento di un fegato da trapiantare e di questi solo 22 sono stati inclusi nello studio , in quanto sottoposti a trapianto di fegato a distanza di circa 1224 ore dallesecuzione dellesame rm . 
per le sequenze se dpt2w ottenute durante la respirazione libera del paziente , abbiamo utilizzato due acquisizioni e bande di pre - saturazione , al di sopra ed al di sotto del campo di studio , al fine di ridurre gli artefatti vascolari . le sequenze ge t1w e ge t2 w sono state eseguite durante lapnea respiratoria dei pazienti , con ununica acquisizione e senza bande di pre - saturazione . 
in tutte le sequenze stato utilizzato spessore di strato di 8 mm con un gap di 1 mm , matrice di 128256 con algoritmo di ricostruzione 3 / 4 , campo di vista ( fov ) di 380450 mm . dopo le sequenze di base stato somministrato mdc spio ( ferumoxide , endorem , guerbert , francia ) , in infusione lenta ( 820 gocce / min ) alla dose di 23 , 6 micromol fe / g , diluito in un flacone da 100 cc di soluzione glucosata al 5% , con un tempo di infusione di circa 3045 mdopo circa 3060 min dalla fine della somministrazione del mdc spio in tutti i pazienti sono state ripetute le sequenze ge t2 * w con gli stessi parametri utilizzati nelle sequenze di base , eseguite prima dellinfusione del mdc spio . le immagini di base e quelle dopo spio sono state valutate separatamente e comparativamente , alloscuro dei radiol med ( 2009 ) 114 : 12671282 1271 diagnostic hypothesis as to histological type . 
on baseline images , in agreement with the reported mr criteria ( table 1 ) , dn were defined as nodular lesions that appeared hyperintense on t1 - weighted images and hypointense on t2weighted images or isohyperintense on t1 - weighted images and isointense on t2 - weighted images . 
hcc were defined as lesions appearing isohyperintense on t1 - weighted images , hyperintense in t2 or hyperintense in t1 , and isointense in t2 or hypointense in t1 , and hyperintense in t2 . hcc subfoci in dn ( nodule - in - nodule ) were defined as nodular areas of heterogeneous signal intensity seen within a dn with typical signal intensity . on spio - enhanced images , the diagnosis was based on the pattern of spio uptake . 
dn were defined as nodules presenting variable uptake depending on the degree of dysplasia , appearing in some cases strongly hypointense , often even more hypointense than the surrounding liver . hcc were defined as nodules with no spio uptake and hence markedly hyperintense . 
hcc subfoci in dn were defined as nodular lesions with hyperintense appearance due to failure to accumulate spio in the context of a larger , hypointense dn due to spio uptake . 
the definitive diagnosis was reached with the histopathological examination performed within 1 week of surgery on the entire explanted liver . dn were classified according to the international working party terminology of hepatic lesions into : lowgrade dn , high - grade dn and dn containing a subfocus of hcc [ 21 ]  . 
hcc were classified based on histology into well differentiated , moderately differentiated and poorly risultati dellanatomia patologica , riportando il numero e la sede delle lesioni ed esprimendosi sulla natura displasica , neoplastica o di altro tipo delle lesioni stesse . 
per ogni nodulo stata indicata lintensit di segnale nelle sequenze di base pesate in t1 e in t2 , il comportamento dopo somministrazione di mdc spio e , in base a tali parametri , si avanzata una ipotesi diagnostica sul tipo istologico . 
nelle sequenze di base , in accordo con la semeiotica rm descritta in letteratura ( tabella 1 ) abbiamo considerato nd le lesioni nodulari che apparivano iperintense in t1w ed ipointense in t2w o iso - / iperintense in t1w e isointense in t2w ; hcc le lesioni che apparivano iso - / iperintense in t1w e iperintense in t2w o iperintense in t1w e isointense in t2w o ipointense in t1w ed iperintense in t2w ; foci di hcc in nd ( nodulonel - nodulo ) le aree nodulari di disomogenea intensit di segnale riscontrate allinterno di un nodulo displasico con le caratteristiche intensit di segnale descritte . dopo iniezione di mdc spio , la diagnosi si basata sul tipo di captazione dello stesso e sono stati considerati nd i noduli che presentavano una captazione di mdc variabile in relazione al grado di displasia , apparendo in alcuni casi fortemente ipointensi , spesso anche in maggior grado rispetto al parenchima epatico limitrofo . 
lidentificazione di foci di hcc in nd si invece basata sul riscontro , dopo mdc spio , di una lesione nodulare iperintensa per mancata captazione di mdc nel contesto di un nodulo displasico di maggiori dimensioni , ipointenso per lup - take di mdc . 
nine patients were excluded because of mr or clinicallaboratory evidence of abnormalities that constituted contraindications or indications to defer surgery , findings later confirmed by clinical - imaging follow - up and biopsy . 
three of these nine patients had suspicious focal liver lesions that were > 5 cm and involved both hepatic lobes ; another two patients had cancercirrhosis , with extensive involvement of the right lobe in one case and left lobe in the other . 
in one patient , mr imaging demonstrated a large confluent fibrosis that made it impossible to confidently rule out the presence of cancer - cirrhosis , which was later excluded by biopsy . 
 risultati i risultati del nostro studio sono riportati nella tabella 2 . dei 31 pazienti selezionati per il trapianto dorgano , sono stati inclusi nello studio 22 pazienti , sottoposti a trapianto fegato a distanza di 1224 ore dallesecuzione dellesame rm . 
nove pazienti sono stati eliminati dallo studio in quanto allesame rm e agli esami clinico - laboratoristici presentavano alterazioni che contravvenivano o consigliavano il posticipo dellesecuzione del trapianto , reperti poi supportati dal follow - up clinico - radiologico e dallesame bioptico . 
in 3 , di questi 9 casi , erano presenti lesioni focali epatiche sospette per hcc che avevano dimensioni complessivamente superiori a 5 cm ed interessavano entrambi i lobi epatici ; in altri 2 casi si trattava di cancro - cirrosi con esteso interessamento del lobo destro in un caso e del sinistro nellaltro ; in 1 caso il paziente era portatore di tips che si estendeva nellatrio destro e per il quale si preferito posticipare lintervento ai fini di una migliore pianificazione chirurgica ; in 1 caso la rm evidenziava una estesa fibrosi confluente che non consentiva di escludere con certezza una eventuale cancro - cirrosi , successivamente non confermata dallesame bioptico ; in 2 casi le scadenti condizioni cliniche dei pazienti hanno imposto di soprassedere al trapianto e di proseguire la terapia medica . 
sono stati quindi inclusi nel nostro studio 22 pazienti , di et media di 53 anni ( range 4657 anni ) , successivamente sottoposti a trapianto dorgano entro 1224 ore dallesecuzione dellesame rm . la cirrosi stata classificata utilizzando il child - pugh syste quindici erano pazienti con cirrosi child - pugh classe a , 7 con cirrosi child - pugh classe b . 
unidici avevano cirrosi correlata con il virus dellepatite b ( hbv ) , 7 cirrosi correlata con il virus dellepatite c ( hcv ) , 4 cirrosi alcool correlata . risultati anatomo - patologici lesame anatomo - patologico dei 22 fegati espiantati ha dimostrato in tutti i casi un aspetto di tipo nodulare : macronodulare in 9 casi , micronodulare in 3 casi e medio - macronodulare in 10 casi . 
sono state identificate , inoltre , 59 lesioni focali epatiche , di cui 14 hcc , 4 noduli displasici con allinterno foci di hcc , 39 noduli displasici e 2 radiol med ( 2009 ) 114 : 12671282 1273 seven were child - pugh class b . 
at baseline mr imaging , four of the 12 dn exhibited the typical pattern of t1 hyperintensity relative to liver and t2 hypointensity ; eight dn were isointense on t1and t2weighted images . 
the two hcc subfoci within dn showed the classic nodule - in - nodule appearance , with isohyperintense signal on t1 - weighted images and heterogeneous hyperintensity on t2 - weighted images , contained within a larger dn that appeared isointense on t1weighted images and isohypointense on t2 - weighted images . 
the signal characteristics of the remaining 39 undetected lesions were such that precise identification and characterisation was precluded . spio administration increased mri sensitivity by 42.37% relative to the baseline study . 
il diametro medio delle lesioni stato per gli hcc 1 , 7 cm ( range 12 , 5 cm ) , per noduli displasici 0 , 8 cm ( range 0 , 52 ) , per i noduli displasici con allinterno foci di hcc 2 , 1 cm ( range 0 , 82 , 8 ) e per i cistoadenomi 1 , 2 cm ( range 11 , 4 )  . risultati rm gli esami rm effettuati senza mdc ( rm di base ) e con ferumoxide hanno mostrato una differente sensibilit nellidentificazione delle lesioni focali epatiche . 
lesame rm di base ha consentito di diagnosticare correttamente 20 lesioni , pari al 33 , 90% di quelle identificate con lesame anatomopatologico , di cui , allesame anatomopatologico , 12 sono risultate nd e 8 hcc . 
nelle sequenze di base , dei 12 nd identificati , 4 hanno mostrato comportamento caratteristico con intensit di segnale aumentata rispetto al parenchima epatico circostante nelle immagini t1w e ridotta in quelle t2w ; 8 nd sono risultati isointensi in t1w e isointensi in t2w . 
per quanto riguarda gli hcc , allesame di base in 3 casi hanno mostrato iperintensit di segnale nelle sequenze t1w ; in 2 casi isointensit di segnale ed in 1 caso ipointensit di segnale . 
i due foci di hcc in nodulo displasico hanno presentato il classico aspetto rm di nodulo - nel - nodulo mostrando segnale iper - / isointenso nelle sequenze t1w , e disomogeneamente iperintenso nelle sequenze t2w allinterno di un nodulo displasico di pi grandi dimensioni isointenso nelle sequenze t1w ed iso / ipointenso nelle sequenze t2w . 
le rimanenti 39 lesioni non diagnosticate presentavano caratteristiche di segnale tali da non consentire una precisa identificazione ed una adeguata caratterizzazione . dopo somministrazione di mdc spio , la rm ha mostrato una maggiore sensibilit diagnosticando complessivamente 45 lesioni , pari al 76 , 27% delle lesioni totali individuate con lesame istologico , di cui , allesame anatomo - patologico , 27 sono risultate nd e 18 hcc , con un incremento del 42 , 37% rispetto alle sequenze rm di base . 
i falsi negativi con la rm - spio sono stati 12 noduli displasici , pari al 31% , che allesame istologico sono risultati essere nd a basso grado di malignit e con diametro inferiore al centimetro . 
due lesioni , caratterizzate istologicamente come cistoadenomi , non sono state identificate in prima istanza allesame rm di base n dopo mdc spio , ma solo valutando retrospettivamente le immagini , sulla scorta dei risultati dellesame istologico . 
baseline protondensity - weighted spin echo ( a ) , t2 - weighted spin echo ( b ) , fisp ( c ) and t1 - weighted flash ( d ) magnetic resonance ( mr ) sequences : the nodule seems slightly hyperintense in all baseline sequences ( a - d )  . 
il reperto anatomo - patologico corrispondente conferma la presenza di multipli e diffusi noduli di rigenerazione con nodulo di hcc bianco - verdastro ( f )  . radiol med ( 2009 ) 114 : 12671282 1275 fig . 
3a - c nodulo di hcc e nodulo displasico con focus di hcc allviii segmento epatico . rm di base , sequenza flash t1w ( a ) e fisp t2w ( b ) : sono ben evidenti due formazioni nodulari iperintense . 
il nodulo di minori dimensioni mostra , nella sequenza fisp t2w , disomogenea intensit di segnale con evidenza di piccolo nodulo centrale contestuale . tale reperto configura il tipico pattern di nodulo - nel - nodulo . 
il reperto anatomopatologico ( c ) dimostra il caratteristico aspetto di nodulo nel nodulo della lesione . in 12 dn , equal to 31% , which at histology proved to be low - grade dn < 1 cm in diameter . 
two lesions that were histologically characterised as cystoadenomas went unrecognised on initial viewing of the baseline and spio - enhanced mr images but were later identified on retrospective review after the results of the histological examination . 
in fact , according to several authors , the transition from a dn to an hcc occurs over a period of mancata identificazione stata probabilmente dovuta alle ridotte dimensioni , alla localizzazione in sede sottoglissoniana e allaspetto simil - cistico . 
infatti lo sviluppo di un hcc a partire da un nd avviene , secondo molti autori , in un tempo variabile di circa 46 mesi [ 12 , 23 ] e laspettativa di vita media in un paziente non trattato di soli 13 mesi , con una sopravvivenza a 2 anni inferiore al 33% [ 24 ]  . 
il reperto anatomo - patologico ( d ) ha dimostrato la presenza di area di fibrosi e lassenza di lesioni focali . approximately 46 months [ 12 , 23 ] , and mean life expectancy of untreated patients is only 13 months , with a 2 - year survival rate < 33% [ 24 ]  . 
this pathogenic theory is supported by other studies and confirmed by the international working party on terminology of hepatocellular lesions , which stated that carcinogenesis in the cirrhotic liver is a multistep process that involves a transition from large rn to lowand high - grade dn to dn with subfocus of hcc and eventually to hcc [ 21 ]  . identification of dn and hcc in the cirrhotic liver is difficult because of the marked architectural distortion of the parenchyma due to areas of fibrosis , steatosis , parenchymal necrosis and regenerative nodules [ 10 , 25 , 26 ]  . 
found that us had a sensitivity of 20.5% for the detection of hcc and of 1.6% for detection of dn , emphasising the difficulty in differentiating hcc and dn with us , as both manifest as hypoechoic nodular lesions [ 8 ]  . 
although the use of sonographic contrast agents has improved the techniques epatiche , in cui si affermato che la carcinogenesi nel fegato cirrotico avviene con un meccanismo multi - step che include la transizione da grossi noduli rigenerativi a noduli displasici a basso ed alto grado di malignit , quindi a noduli displasici con foci di hcc sino agli hcc [ 21 ]  . lidentificazione di nd e di hcc nel fegato cirrotico per difficoltosa per la notevole alterazione strutturale del parenchima epatico a causa della presenza di aree di fibrosi , steatosi , necrosi parenchimale e noduli di rigenerazione [ 10 , 25 , 26 ]  . 
 [ 8 ] , in uno studio su 200 pazienti con cirrosi , hanno rilevato una sensibilit dellecografia nella identificazione degli hcc del 20 , 5% e dei nd del 1 , 6% , sottolineando la difficolt di differenziare con lecografia gli hcc dai nd , poich entrambi apparivano come lesioni nodulari ipoecogene [ 8 ]  . 
lutilizzo dei mezzi di contrasto ecografici ha migliorato laccuratezza diagnostica nella identificazione di hcc e nd rispetto alla ecografia convenzionale ; tuttavia esistono ancora difficolt nella diagnosi differenziale tra le due lesioni con tale metodica [ 27 ]  . 1278 radiol med ( 2009 ) 114 : 12671282 accuracy in identifying hcc and dn , the difficulties in differentiating the two lesions with this modality remain [ 27 ]  . spiral ct is currently considered amongst the most reliable modalities for detecting hcc . 
reported a mean sensitivity of dynamic spiral ct in identifying hcc of 76% and mean sensitivity values of 39% in the detection of dn depending on lesion size [ 10 ]  . the lower sensitivity in dn detection is most likely due to the fact that some dn are hypoattenuating in the portal venous and delayed phases , and few dn show hyperattenuation in the hepatic arterial phase . 
in the early stages of carcinogenesis , this is similar to that of healthy liver parenchyma , whereas in the subsequent hcc stage , it is characterised by a predominance of abnormal arteries ( not accompanied by bile ducts and for this reason known as unpaired or nonportal arteries ) and arteriovenous shunts livers undergoing neoplastic degeneration [ 19 , 20 , 29 ]  . 
thus , the arterial and portal supply to lowand high - grade dn is variable and inconsistent , making difficult the detection and characterisation of dn on the basis of their vascular characteristics alone [ 10 ]  . 
 typical of cirrhotic unlike ct , mr imaging often proves capable of differentiating hcc from dn based on signal characteristics alone as a result of its multiparametric properties and highcontrast resolution [ 23 ]  . 
on unenhanced baseline mr imaging , dn normally have isohyperintense signal on t1weigthed images in relation to their glycoprotein content and degree of dysplasia ; the signal becomes hypointense to surrounding parenchyma on t2 - weighted images . 
unfortunately , however , the signal intensity of dn may be identical to that of well - differentiated hcc , especially of small hcc ( < 2cm )  . the signal intensity of hcc on unenhanced t1weighted mr images varies widely and hcc may appear as hypointense masses as a result of greater water content or fibrous tissue or poor cellular differentiation or alternatively as hyperintense due to steatosis , accumulation of glycoproteic material or areas of intralesional haemorrhage . in some cases , however , moderately and well - differentiated hcc may also appear isointense compared with the healthy hepatic parenchyma . 
conversely , on t2 - weighted images , hcc tend to appear as generally ill - defined and hyperintense lesions [ 12 , 30 ] with the exception of well - differentiated hcc , which are isointense relative to the healthy parenchyma . 
in letteratura riportato che la sensibilit della tc multifasica nella identificazione di hcc di diametro superiore a 2 cm del 93 , 6% , percentuale che si riduce al 61% nella valutazione di lesioni di minori dimensioni [ 28 ]  . 
 [ 10 ] hanno riportato una sensibilit media della tc spirale dinamica nellidentificazione dellhcc del 76% e valori medi di sensibilit del 39% nellidentificazione dei nd in relazione alle dimensioni delle lesioni [ 10 ]  . 
questi minori valori di sensibilit nella identificazione dei nd sono verosimilmente dovuti al fatto che solo alcuni nd sono ipodensi in fase venosa portale e in fase tardiva , cos come sono pochi i nd che mostrano iperdensit nella fase arteriosa epatica . 
questo fenomeno correlato al tipo di apporto ematico arterioso e venoso che , nelle prime fasi della carcinogenesi , simile a quello del tessuto epatico sano ; successivamente , nello stadio di hcc , prevalgono vasi arteriosi anomali , non accompagnati dai canalicoli biliari , e per tale motivo denominati unpaired o non portal arteries , e shunt artero - venosi tipici dei fegati cirrotici ed in degenerazione neoplastica [ 19 , 20 , 29 ]  . 
pertanto lapporto arterioso e portale ai nd a basso ed alto grado di malignit variabile ed incostante ; , dunque , difficile identificare e caratterizzare i noduli displasici soltanto sulla base delle caratteristiche vascolari [ 10 ]  . la rm , grazie alle sue intrinseche multiparametricit ed alta risoluzione di contrasto , rispetto alla tc si rivela spesso in grado , di differenziare gli hcc dai nd sulla base delle sole caratteristiche di segnale [ 23 ]  . 
nelle immagini rm di base , il nd presenta solitamente , nelle sequenze t1w , un segnale che , in relazione al contenuto glicoproteico ed al grado di displasia , pu essere iso - / iperintenso ; appare invece iso - / ipointenso rispetto al parenchima circostante nelle sequenze t2w . 
purtroppo per lintensit di segnale dei nd pu essere sovrapponibile a quella degli hcc ben differenziati , soprattutto se di piccole dimensioni ( hcc < 2 cm )  . le caratteristiche di segnale degli hcc nelle immagini rm di base t1w variano molto e possono apparire come formazioni ipointense , per il maggior contenuto di acqua o per la componente di tessuto fibroso e per la scarsa differenziazione cellulare ; o possono presentare elevata intensit di segnale per la presenza di steatosi , accumulo di materiale glicoproteico o aree di emorragia intratumorale . 
nelle immagini t2w , invece , gli hcc appaiono comunemente come lesioni non sempre ben definite , iperintense rispetto al parenchima circostante [ 12 , 30 ] ad eccezione degli hcc ben differenziati che mostrano isointensit di segnale rispetto al parenchima sano . la capacit di identificare e caratterizzare le lesioni nodulari nel fegato cirrotico aumenta con lausilio dei mdc siano essi paramagnetici o superparamagnetici . 
la rm con mdc paramagnetico sfrutta , come la tc , le caratteristiche vascolari delle lesioni focali epatiche sia per la loro radiol med ( 2009 ) 114 : 12671282 1279 imaging with paramagnetic contrast medium relies on the vascular characteristics of focal liver lesions for their detection and characterisation . 
gadolinium has shown a good level of accuracy , even in the study of small hcc ( < 1.52 cm ) and in cirrhotic livers , with a sensitivity of 84% [ 11 , 31 , 32 ]  . 
sensitivity in the detection of dn is instead only 15% , with low specificity values since the signal intensity of dn on mr imaging with paramagnetic contrast medium is very similar to that of many hcc [ 33 ]  . the introduction of spio contrast agents , which provide information about the composition and function of cells forming the nodular lesions and which overcome the limitations of relying on vascularisation changes , has made it possible to detect even small hcc , which in the early stage may preserve normal vascularity and thus be difficult to differentiate from other nodular lesions [ 34 , 35 ]  . 
 the mechanism of action of spio contrast agents is based on their uptake by kupffer cells or cells of the hepatic reticuloendothelial syste spio uptake is reflected in a marked reduction in signal intensity of the tissues containing kupffer cells . 
conversely , any malignant lesions , which do not contain reticuloendothelial cells , do not accumulate the contrast medium and therefore appear as areas of hyperintensity [ 36 , 37 ]  . 
the use of these contrast agents has in part solved the problem of false positive results seen with paramagnetic contrast agents injected as a bolus , a problem related to the presence of small arteriovenous shunts which , appearing as small areas of vascular enhancement during the arterial phase , may mimic the enhancement pattern of small hcc . 
these false positive results are similar to those seen during contrast - enhanced dynamic ct imaging . on this subject , the literature also contains studies on the combined use of gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa ) and spio , which , by fulfilling the criteria of vascularity as well as cellular composition and function [ 11 , 38 ] , reduces both the false positive results of paramagnetic contrast agents and the false negative results of spio agents the latter related to the presence , in moderately and well - differentiated hcc , of functioning kupffer cells that accumulate the contrast agent . 
as a result , the t2 - weighted signal intensity is higher in low - grade tumours , in which the number and function of kupffer cells is decreased [ 40 ]  . 
il gadolinio in molti studi ha mostrato una buona accuratezza anche nello studio dei piccoli hcc ( < 1 , 52 cm ) e nei fegati cirrotici mostrando una sensibilit dell84% [ 11 , 31 , 32 ]  . la sensibilit nellidentificazione dei nd invece , solo del 15% con bassi valori di specificit in quanto lintensit di segnale dei nd ottenuta dopo mdc paramagnetico paragonabile a quella di molti hcc [ 33 ]  . lintroduzione dei mdc spio fornendo informazioni sulla composizione e sulla funzione delle cellule che costituiscono le lesioni nodulari e , superando i limiti diagnostici legati alle alterazioni della vascolarizzazione , consente di identificare anche hcc di piccole dimensioni che nello stadio precoce possono in parte conservare una vascolarizzazione normale ed essere quindi difficilmente differenziabili dalle altre lesioni nodulari [ 34 , 35 ]  . 
il meccanismo dazione dei mdc spio si basa sulla loro captazione da parte delle cellule del sistema reticolo - endoteliale epatico , le cellule di kupffer , che si traduce in una marcata riduzione dellintensit di segnale dei tessuti in cui sono presenti tali cellule . pertanto , leffetto prodotto nelle immagini pesate in t2 fa s che alcune lesioni benigne captano il mezzo di contrasto come il parenchima epatico sano ; di contro , le lesioni focali maligne eventualmente presenti , sprovviste di cellule del sistema reticolo - endoteliale , non captano il mdc e appaiono come aree iperintense [ 36 , 37 ]  . 
lutilizzo di questi mdc ha risolto in parte il problema dei falsi positivi che si osservano con i mezzi di contrasto paramagnetici iniettati a bolo , legato alla presenza di piccoli shunt artero - venosi che , manifestandosi come piccole aree di enhancement vascolare in fase arteriosa , possono simulare il pattern contrastografico di piccoli hcc . 
 a tale proposito , in letteratura sono stati anche riportati studi sulluso combinato di gadolinio legato ad acido acetico dietilenetriaminepenta ( gd - dtpa ) e spio che , soddisfacendo sia i criteri di vascolarizzazione sia quelli di composizione e funzionalit cellulare [ 11 , 38 ] , riduce il problema dei falsi positivi dei mezzi di contrasto paramagnetici e dei falsi negativi con mdc spio , questi ultimi legati alla presenza , in hcc ben differenziati o moderatamente differenziati , di cellule di kupffer sane che di conseguenza captano il mdc . infatti , uno studio anatomo - patologico sulla carcinogenesi multi - step ha dimostrato che cellule del kupffer sono ancora presenti nei noduli epatici durante il processo di degenerazione ; ci che varia il numero di tali cellule che si riduce durante le fasi della malattia cirrotica e nellevoluzione dellhcc da uno stadio di alta differenziazione ad uno di moderata o scarsa differenziazione [ 35 , 39 ]  . 
lintensit di segnale nelle sequenze t2w , quindi , sar tanto pi elevato quanto meno differenziato sar il tumore , essendo inferiori il numero e la funzionalit delle cellule del kupffer presenti [ 40 ] ; questo offre la possibilit di effettuare una diagnosi differenziale tra hcc e noduli displasici . sebbene la rm con i mezzi di contrasto spio sia una 1280 radiol med ( 2009 ) 114 : 12671282 differentiating between hcc and dn . although spio - enhanced mr imaging is an accurate technique in the cirrhotic liver , the heterogeneous uptake of spio agents may affect the interpretation of findings . 
in liver cirrhosis , the marked subversion of hepatic structure and function , intrahepatic vascular changes , or the presence of inflammatory processes , thromboses , hepatitis or steatosis , may affect the intracellular uptake and distribution of spio agents in the liver , thereby reducing their effectiveness in the detection and characterisation of small focal lesions [ 43 , 44 ]  . 
such alterations , known as spio liver uptake and distribution alterations ( spio - luda ) lead to the formation of hyperintense areas due to reduced uptake or hypointense areas , which is due to increased uptake . although the incidence of such alterations is relatively low , in some cases , they give rise to diagnostic problems on mr imaging [ 26 ]  . we observed no significant spio uptake and distribution alterations ( table 1 ) , and the signal intensity of the nodular lesions seen in our study ( dn and hcc ) corresponded to the patterns reported in the literature . 
there were no cases of well - differentiated hcc showing spio uptake , as reported by other authors [ 45 ] , and hence no cases of false negative hcc diagnoses . 
 on the basis of our results and in agreement with the literature , spio - enhanced mr imaging proved to be a valuable tool for the detection and characterisation of focal lesions in the cirrhotic liver . 
in particular , spio - enhanced mr imaging is currently the only imaging modality capable of distinguishing between dn and hcc and thus providing the opportunity for an accurate and timely diagnosis of malignant change of dn , a crucial aspect for prognosis . tecnica dimaging accurata nello studio del fegato cirrotico , leterogeneo up - take degli spio pu compromettere linterpretazione dei reperti . 
nella cirrosi epaticail notevole sovvertimento della struttura e delle funzioni epatiche , le alterazioni vascolari intraepatiche o la presenza di processi flogistici , trombosi vascolari , di epatiti , steatosi , possono modificare la captazione intra - cellulare e la distribuzione dei mdc spio nel fegato riducendone lefficacia , con una minore utilit degli stessi nella identificazione e caratterizzazione di piccole lesioni focali [ 43 , 44 ]  . 
tali alterazioni , denominate alterazioni di captazione e distribuzione epatiche del mdc spio ( spio - acde ) , provocano la formazione di aree di iperintensit da ridotta captazione o di ipointensit da aumentata captazione . 
lincidenza di queste alterazioni relativamente bassa ma in alcuni casi determina difficolt diagnostiche allesame rm [ 26 ]  . in questa esperienza non si sono dimostrate significative alterazioni della captazione e della distribuzione dei mezzi di contrasto ( tabella 1 ) e lintensit di segnale delle lesioni nodulari epatiche considerate nel nostro studio ( nd e hcc ) stata corrispondente ai possibili pattern di segnale rm riportati in letteratura . 
non stato riscontrato nessun caso di hcc ben differenziato che captava mdc spio , come descritto da alcuni autori in letteratura [ 45 ] ; non sono stati pertanto riscontrati falsi negativi nella diagnosi di hcc . sono stati riscontrati , invece , falsi negativi per la diagnosi di nd . 
tali risultati sono probabilmente legati al fatto che il nostro campione di studio era relativamente limitato , quindi ridotta stata la possibilit di riscontro di hcc con comportamento contrastografico simile a quello dei nd . 
de filippo , scienze radiologiche , azienda ospedaliero - universitaria di parma , via gramsci 14 padiglione barbieri , 43100 parma , italy , tel . : + 39 - 052 - 1703660 , e - mail : massimo.defilippo@unipr.it received : 20 march 2008 / accepted : 13 october 2008 / published online : 19 november 2009 springer - verlag 2009 abstract purpose . 
through a search of the pathology databases of four italian hospitals , we identified six men ( mean age , 56 years ) with a histological diagnosis of ecd . histology was performed on retroperitoneal or pulmonary biopsy , depending on disease involvement on imaging . patients underwent plain radiography of the lower limbs and chest , total - body computed tomography ( ct ) and bone scintigraphy . 
magnetic resonance ( mr ) imaging was performed in two patients to evaluate the lower limbs and in one patient to study the brain , the chest and the abdomen . 
imaging studies revealed extraskeletal manifestations in all patients , including involvement of the retroperitoneal space ( n = 4 ) , the lung ( n = 4 ) and the heart ( n = 2 )  . 
sono stati identificati nel data base dellunit operativa di anatomia patologica di quattro ospedali italiani , sei pazienti con ecd , di sesso maschile , con et media di 56 anni . 
la diagnosi di natura dellecd istologica , 1320 radiol med ( 2009 ) 114 : 13191329 keywords erdheim - chester disease retroperitoneal fibrosis histiocytosis tuttavia il sospetto diagnostico pu essere agevolmente posto con limaging radiologico . parole chiave malattia di erdheim - chester fibrosi retroperitoneale istiocitosi introduction introduzione erdheim - chester disease ( ecd ) is a rare , systemic xanthogranulomatous infiltrative disease characterised by deposition of lipid - laden histiocytes in various organs , with the constant involvement of bone [ 16 ]  . 
ecd was first described by the american physician william chester and the viennese pathologist jacob erdheim in 1930 , who described two cases of a peculiar form of histiocytosis that they distinguished from other disorders such as handschller - christian disease and niemann - pick disease [ 7 ]  . the eponym erdheim - chester disease was coined by jaffe in 1972 [ 8 ]  . 
 the disease affects both genders , though with a slight predilection for men , and has a peak incidence between the fifth and sixth decade of life , although it may manifest at any age [ 4 ]  . 
skeletal involvement is most common in the long bones of the lower limbs . approximately 50% of patients present with extraskeletal manifestations , the most commonly involved sites being the heart , the lungs , the kidneys , the retroperitoneal space , the central nervous system and the skthe clinical course of ecd ranges from the absence of symptoms to a very poor outcome [ 9 ]  . 
 materials and methods we retrospectively searched the pathology databases of four italian hospitals for cases of ecd entered between january 2002 and january 2008 to identify organ involvement and clinical and radiological features . 
the diagnostic criteria for ecd are histopathological and based on the presence of lipid - laden histiocytes immunopositive for cd68 and immunonegative for s - 100 , cd1a and birbeck granules . 
 imaging studies included plain radiography of the lower limbs and chest , bone scintigraphy with technetium 99 ( 99mtc ) and chest and abdominal multidetector computed tomography ( mdct )  . 
patient 1 , who had a history of la malattia di erdheim - chester ( ecd ) una rara patologia sistemica di tipo infiltrativo xantogranulomatoso , caratterizzata dalla presenza di depositi di istiociti contenenti materiale lipoideo in vari organi , con coinvolgimento osseo pressoch costante [ 16 ]  . 
lecd fu descritta per la prima volta nel 1930 da un medico nordamericano , william chester e da un patologo viennese , jacob erdheim , che identificarono in due pazienti una particolare forma di istiocitosi , distinguendola da altri disordini , come la malattia di hand - schllerchristian e di niemann - pick [ 7 ]  . 
 la malattia presente in entrambi i sessi , con una lieve prevalenza nel sesso maschile ed un picco di incidenza tra la 5 e la 6 decade di vita , sebbene possa manifestarsi a qualsiasi et [ 4 ]  . 
linteressamento scheletrico dellecd riguarda prevalentemente le ossa lunghe degli arti inferiori ; circa la met dei pazienti presentano manifestazioni extra - scheletriche , le sedi maggiormente coinvolte sono : cuore , polmoni , reni , retroperitoneo , sistema nervoso centrale e cute . 
 materiali e metodi abbiano ricercato retrospettivamente nel database delle unit operative di anatomia patologica di quattro ospedali italiani la presenza di casi di malattia di erdheim - chester ( ecd ) , nel periodo compreso tra il gennaio 2002 e il gennaio 2008 , al fine di valutarne limpegno nei differenti organi e gli aspetti clinico - radiologici . 
i criteri diagnostici di ecd , sono istopatologici , basati sulla presenza di istiociti ricchi di lipidi , positivi allantigene per il cd68 e prive degli antigeni della proteina s - 100 , del cd1a e dei granuli di birbeck . 
il campionamento tissutale era stato ottenuto mediante biopsia retroperitoneale in tre casi e polmonare nei rimanenti tre casi . i pazienti erano stati sottoposti a radiografia del torace e degli arti inferiori , scintigrafia ossea con tecnezio 99 ( 99mtc ) , tomografia computerizzata multidetettore ( tcmd ) toracica e addominale . 
il paziente 1 , con anamnesi positiva per diabete insipido e microadenoma ipofisario , fu studiato radiol med ( 2009 ) 114 : 13191329 1321 diabetes insipidus and pituitary microadenoma , was studied with high - field magnetic resonance ( mr ) imaging to evaluate the brain , the chest , the abdomen and the lower limbs . patient 2 underwent mr imaging of the lower limbs to investigate diffuse bone changes identified on plain radiography . 
le indagini di imaging sono state valutate da due radiologi . results patients 1 and 2 had cardiac involvement , which in one patient manifested clinically as chest tightness and in the other as dyspnoea on exertion . 
in one case , the retroperitoneal solid tissue caused renal artery stenosis with resulting arterial hypertension , whereas in the other three cases , it surrounded the aorta and the iliac arteries , causing risultati nei pazienti 1 e 2 si evidenziava coinvolgimento cardiaco dellecd . 
lesordio clinico di ecd nei pazienti 3 e 4 era caratterizzato da alterazione degli indici di funzionalit renale , associato a ripetuti episodi di infezioni delle vie urinarie nel caso 3 . 
nei primi quattro pazienti la tc addome evidenziava infiltrazione retroperitoneale da parte di tessuto solido , prevalentemente perirenale e simmetrico , ipodenso e dotato di lieve contrast enhancement dopo somministrazione di mezzo di contrasto ( mdc )  . 
il tessuto solido retroperitoneale determinava nel caso 1 stenosi dellarteria renale con conseguente ipertensione arteriosa mentre negli altri tre casi circondava laorta e le arterie iliache , con fenomeni di incarceramento della fig . 
magnetic resonance image of the chest ( balanced sequence ) in the coronal plane ( a ) and contrast - enhanced computed tomography of the chest with four - chamber multiplanar reconstruction ( b )  . 
rm del torace ( balance w ) in sezione coronale ( a ) e tc con mdc del torace in sezione assiale obliqua four chambers mpr ( b )  . 
contrast - enhanced computed tomography of the upper abdomen ( a , b ) : the coated aorta , a specific finding in erdheim - chester disease , is well - depicted in the magnified image ( arrows in b )  . fig 2a , b ecd in fase avanzata . 
tc con mdc delladdome superiore ( a , b ) : aorta rivestita da tessuto solido , aspetto peculiare dellecd , ben evidente nellimmagine ingrandita ( frecce in b )  . 
renal pyelectasia , more evident on the left side , is due to compression by the fibrous tissue , which is also present at the level of the proximal periureteral spaces  . fig 3a , b ecd in fase iniziale . 
nel caso 5 lecd si manifestava con dolori al rachide in assenza di alterazioni allrx tradizionale , mentre la scintigrafia con 99mtc mostrava iperfissazione del radiol med ( 2009 ) 114 : 13191329 1323 fig . 
magnetic resonance images of the upper abdomen : axial t2 - weighted turbo spin - echo ( a ) and t1 - weighted fat - saturated fast - field echo sequence after the intravenous administration of paramagnetic contrast material . 
note the homogeneous enhancement of the fibrous tissue during the venous phase ( b ) and the sparing of the periaortic and pericaval regions ( a , b )  . fig 4a , b ecd in fase avanzata . 
il sottoslivellamento laterale sn della sella turcica ( freccia ) segno indiretto della presenza di un microadenoma ipofisario . scintigraphy showed increased tracer uptake at the level of a thoracic vertebra . four patients ( 2 , 3 , 5 and 6 ) had involvement of the pulmonary interstitiuchest radiography showed pleural and interstitial thickening ( kerley b lines )  . 
chest ct demonstrated a reticular interstitial pattern , smooth septal and fissural thickening , diffuse ground - glass opacities and centrilobular nodules with subpleural , peribronchovascular radiofarmaco in corrispondenza di una vertebrale dorsale . in quattro pazienti ( caso 2 , 3 , 5 e 6 ) vi era coinvolgimento dellinterstizio polmonare . 
i radiogrammi in proiezione antero - posteriore di gamba , mettono in evidenza bilateralmente , in corrispondenza della spongiosa tibiale e peroneale , diffuse e sfumate zone di radio - opacit , cui si associano ispessimenti focali delle corticali scheletriche , in assenza di reazioni periostali . radiol med ( 2009 ) 114 : 13191329 1325 fig . 
the clinical suspicion was confirmed by a biopsy of the retroperitoneal tissue in three patients ( 1 , 3 , and 4 ) and of pulmonary tissue in the remaining three patients ( 2 , 5 , 6 )  . 
il sospetto clinico stato confermato dallindagine bioptica su tessuto retroperitoneale in 3 pazienti ( casi 1 , 3 , 4 ) e polmonare nei rimanenti 3 casi ( 2 , 5 , 6 )  . 
 discussion discussione ecd is a rare form of non - langerhans histiocytosis , the reactive or neoplastic nature of which is still being debated [ 10 , 11 ]  . 
axial ( a ) and sagittal ct ( b ; multiplanar reconstruction ) demonstrates extensive erosion of t6 vertebral body with interruption of the posterior end - plate and initial involvement of the left vertebral pedicle . 
dimostrazione tc sul piano assiale ( a ) e sagittale ( b ; mpr ) di voluminosa erosione del soma di t6 con interruzione della limitante somatica posteriore ed inizile impegno del peduncolo vertebrale di sn . 
la rm ( c ) in se t1 w dimostra lindennit del canale vertebrale . in our experience , there was a frequent correlation between a histological diagnosis of ecd and skeletal involvement . 
bone involvement is an almost constant feature of ecd , there being only one report of a case without bone lesions [ 13 ]  . ecd generally affects the long bones of the lower limbs ( tibia and fibula )  . 
the related radiographic findings are diffuse or patchy opacities of the tibia and / or fibula , medullary sclerosis and cortical thickening of the metaphyseal and diaphyseal portions without epiphyseal changes . on 99mtc scintigraphy , intense , bilateral and symmetrical tracer uptake by the long - bone diaphyses and metaphyses is revealed , reflecting increased osteoblastic activity in those regions [ 1521 ]  . 
in our series , osteosclerotic changes were seen in the metaphyseal and diaphyseal portions of the tibia and fibula in three patients ( 1 , 3 and 4 )  . 
le lesioni ossee rappresentano un aspetto pressoch costante dellecd ; viene riportato in letteratura un solo caso di ecd in cui non erano state dimostrate lesioni ossee [ 13 ]  . lecd generalmente interessa le ossa lunghe degli arti inferiori ( in particolar modo tibia e perone ) e le alterazioni radiografiche si configurano come radio - opacit diffuse o a chiazze della tibia e / o del perone , la sclerosi midollare e lispessimento corticale delle regioni metafisarie e diafisaria ; scarse invece sono le alterazioni epifisiarie [ 13 ]  . 
la scintigrafia 99mtc evidenzia intensa iperfissazione , bilaterale , simmetrica a carico delle diafisi e metafisi delle ossa lunghe , conseguente ad aumento dellattivit osteoblastica in tali sedi [ 1521 ]  . 
nei casi 2 e 6 si osservano le caratteristiche radiol med ( 2009 ) 114 : 13191329 1327 the osteosclerotic changes were seen at the femoral level . bone involvement in these patients was asymptomatic , in contrast to previous reports where > 50% of patients have mild but persistent pain of the affected bone segment , most commonly the hips and knees [ 9 ]  . only patient 4 had symptomatic bone involvement , reporting with spinal pain despite the absence of significant abnormalities on plain radiography of the spine and lower limbs . 
are the only authors to have reported cases of lytic vertebral lesions ( two cases ) , and indeed , the spine is typically spared in ecd [ 22 ]  . 
otomastoiditis , spleen and bone marrow involvement are also more frequent in lch , whereas retroperitoneal involvement of the perirenal spaces and circumferential involvement of the aorta are typical features of ecd [ 23 ]  . 
in support of the latter hypothesis , cases of ecd coexisting with lch have been reported , suggesting the possibility that the two diseases are linked by a common precursor , cd34 + [ 24 , 25 ]  . 
il coinvolgimento osseo in questi pazienti era asintomatico , a differenza dei dati riportati in letteratura , secondo i quali oltre la met dei pazienti presentano dolore lieve ma persistente , localizzato al segmento osseo colpito , prevalentemente alle anche e alle ginocchia [ 9 ]  . solo il quarto paziente presentava sintomatologia dolorosa al rachide , in assenza di significative alterazioni allindagine radiografica del rachide e degli arti inferiori ; lesame scintigrafico evidenziava iperfissazione del radiofarmaco in corrispondenza di una vertebra dorsale ; la biopsia in tale sede non risultava diagnostica per campionamento inadeguato ; il prelievo bioptico a livello polmonare consentiva la diagnosi di ecd . 
 [ 22 ] sono gli unici autori ad avere riportato casi di lesioni osteolitiche vertebrali ( 2 pazienti ) ; infatti caratteristicamente nellecd si osserva risparmio del rachide . le lesioni osteolitiche dello scheletro assiale sono pi frequenti nellistiocitosi a cellule di langerhans ( lch ) , ma generalmente , queste tendono a risparmiare le ossa lunghe . inoltre i pazienti affetti da lch sono pi giovani rispetto a quelli con ecd ed hanno una prognosi migliore , con tassi di mortalit del 30% ( versus il 57% dellecd ) [ 9 ]  . 
a favore di tale ipotesi sono stati riportati alcuni casi in cui ecd ed lch coesistono , suggerendo la possibilit che le due patologie siano legate da un comune precursore cd34 + [ 24 , 25 ]  . 
in nessuno dei nostri pazienti stato osservato esoftalmo , sebbene rappresenti una frequente presentazione neurologica di ecd , conseguente ad una infiltrazione del tessuto adiposo retroconale e della guaina del nervo ottico . 
diabete insipido ed esoftalmo sono presenti in entrambe le forme di istiocitosi , in particolare nellistiocitosi a cellule del langerhans ( lch ) rappresentano in associazione ad osteolisi la classica triade di presentazione . 
tali reperti associati a diabete insipido sono rilevabili anche nello xantoma disseminato ( xd ) che pu simulare clinicamente lecd ; tuttavia nellxd il diabete insipido di grado lieve e transitorio ( nellecd persistente e progressivo ) , i pazienti hanno et inferiore a quelli con ecd , presentano diffuse lesioni cutanee e mucose e , raramente , possono presentare lesioni osteolitiche periarticolari [ 25 ]  . nei casi 1 e 2 stato riscontrato coinvolgimento cardiaco 1328 radiol med ( 2009 ) 114 : 13191329 among the typical manifestations of ecd [ 27 ]  . 
these same patients also exhibited thoracoabdominal periaortic infiltration , which is the most common cardiovascular manifestation of ecd [ 27 ] and is referred to as a coated aorta when the entire course of the vessel aorta is surrounded by fibrosis . 
at ct , care should be taken not to confuse periaortic infiltration with the aortic wall thickening seen in takayasu arteritis , a condition characterised by involvement of the full thickness of the aortic wall and sparing of the periaortic spaces . 
the use of contrast - enhanced ct is decisive for identifying this feature at the early stages of perirenal fibrosis . displacement of the aorta and ureters by the fibrous tissue may also be seen in forms secondary to malignant diseases , as in some histological types of non - hodgkins lymphomas . these , however , will rarely show the typical bilateral and symmetrical distribution of ecd [ 28 ]  . 
the differential diagnosis of pulmonary involvement by ecd prevalently includes cardiogenic interstitial oedema , where centrilobular nodules are absent , and carcinomatous lymphangitis and sarcoidosis , where septal thickening is typically nodular [ 29 , 30 ]  . our experience suggests that a clinical presentation of bilateral hydronephrosis , persistent bone pain , diabetes insipidus and exophthalmus should raise suspicion of ecd and prompt investigation with plain radiography of the lower limbs and ct of the chest and abdomen . 
if the examination reveals the characteristic diaphyseal and metaphyseal osteosclerosis , brain mr imaging should be used to search for any pituitary microadenomas ( at times hyposecreting )  . in conclusion , ecd is a rare multiorgan disease that has heterogeneous clinical presentations and a prevalence that appears to be underestimated . 
among the possible organs con riscontro di versamento pericardico , che recentemente stato incluso tra le manifestazioni tipiche dellecd [ 27 ]  . negli stessi pazienti stata anche evidenziata la presenza di infiltrato periaortico toraco - addominale ; tra le manifestazioni cardiovascolari questa la pi frequente in corso di ecd [ 27 ] e viene indicata anche con il termine di aorta rivestita , quando lintero decorso aortico circondato da fibrosi . 
allesame tc linfiltrato periaortico non deve essere confuso con lispessimento parietale aortico presente nellarterite di takayasu ; questultima condizione infatti si caratterizza per linteressamento a tutto spessore della parete aortica con risparmio degli spazi periaortici . 
la dislocazione dellaorta e degli ureteri da parte del tessuto fibrotico pu essere riscontrata anche nelle forme secondarie a patologie maligne , come nel caso di alcuni istotipi di linfomi nonhodgkin ; tuttavia rara la distribuzione bilaterale e simmetrica propria dellecd [ 28 ]  . 
la tc torace evidenziava un pattern interstiziale di tipo reticolare con ispessimento liscio dei setti e delle scissure , diffuse aree a densit ground glass e noduli centrolobulari con distribuzione subpleurica , peribroncovasale e interlobulare . 
la diagnosi differenziale in caso di coinvolgimento polmonare include principalmente ledema interstiziale cardiogenico in cui sono assenti i noduli centrolobulari , la linfangite carcinomatosa e la sarcoidosi ove lispessimento dei setti tipicamente nodulare [ 29 , 30 ]  . la nostra esperienza suggerisce che un quadro clinico caratterizzato da idronefrosi bilaterale , dolore osseo persistente , diabete insipido , esoftalmo , pu orientare il sospetto diagnostico di ecd e giustificare lesecuzione di un esame radiografico degli arti inferiori e di una tc toracica ed addominale . 
il riscontro occasionale in ecografia , tc o rm , di fibrosi perirenale giustificano un approfondimento con rx standard degli arti inferiori ; quando a tali livelli , si documenti la caratteristica osteosclerosi diafisaria e metafisaria dellecd , consigliabile ricercare la possibile presenza di microadenomi ipofisari ( talvolta iposecernenti ) con rm dellencefalo . in conclusione , lecd una patologia multiorgano rara , con manifestazioni cliniche estremamente eterogenee , la cui radiol med ( 2009 ) 114 : 13191329 1329 involved by the disease , skeletal tissue , the retroperitoneum and , in particular , perirenal spaces , were found to be constantly involved . 
patients treated with these hearing devices are often children who require close follow - up with frequent functional and radiological examinations ; in particular , multislice computed tomography ( msct )  . 
dental volumetric cone - beam ct ( cbct ) has been reported as a reliable technique for acquiring images of the temporal bone while delivering low radiation doses and containing costs . 
one hundred patients ( mean age 26 years , range 743 ) with vibrant soundbridge implants on the round window underwent follow - up : 85 with cbct and 15 with msct . 
i pazienti trattati con questi tipi di ausili , spesso bambini , necessitano di un follow - up di esami sia funzionali che radiologici , in particolare mediante tomografia computerizzata multistrato ( mstc )  . la tc volumetrica dentale a fascio conico ( cbct ) una metodica utile allo studio dellosso temporale , con il vantaggio di erogare basse dosi di radiazioni ionizzanti e di avere costi di gestione contenuti . 
sono stati inclusi 100 pazienti ipoacusici ( et media 26 anni , range 743 ) , trattati mediante protesi vibrant soundbridge alla finestra rotonda , 15 studiati in follow - up mediante tc e 85 mediante cbct , calcolando le dosi medie assorbite per tessuto sia durante esame mstc che cbct : ogni studio era focalizzato sullosso temporale utilizzando il pi piccolo campo di vista ed il protocollo a bassa dose radiante . 
le immagini ottenute con la cbct sono di qualit inferiore rispetto alla mstc , ma sufficientemente diagnostiche , permettendo di valutare con sicurezza la radiol med ( 2009 ) 114 : 13081318 1309 technique for postoperative imaging and follow - up of patients with bionic ear implants . 
la cbct , grazie alla bassa dose impartita e alla sufficiente qualit delle immagini , pu essere considerata tecnica radiologica adeguata per i controlli postoperatori ed il follow - up dei pazienti con orecchio bionico . parole chiave orecchio bionico , impianti acustici tomografia computerizzata a fascio conico dose radiante introduction introduzione cone - beam computed tomography ( cbct ) is an evolution of conventional computed tomography ( ct ) from which it has inherited some physical features , such as the use of ionising radiation , the ability to provide high - quality images and the possibility of imaging anatomical structures with multiplanar and three - dimensional ( 3d ) reconstructions . 
the first applications of cbct were in the fields of dental and maxillofacial imaging , where it replaced in part orthopantomography and multislice ct ( mstc ) , which were limited by insufficient spatial information and high radiation doses , respectively . 
cbct has played a primary role in dental implantology owing to its ability to provide an estimate of the thickness and depth of residual alveolar bone and visualise anatomical structures at risk during surgery , such as the mandibular canal , the mental foramen , the nasopalatine duct and the maxillary sinus . 
cbct has also been employed to study the temporomandibular joints , bone neoplasms and single dental elements [ 57 ]  . the use of cbct is establishing itself in the otological field , where msct is the gold standard [ 8 , 9 ]  . 
the first clinical indications were middle - ear diseases causing conductive hearing impairment , in which it was used to identify the damaged conduction structure or to follow - up patients after ossiculoplasty [ 10 ]  . 
cbct was subsequently used for postoperative imaging and follow - up of patients with vibrant soundbridge ( vsb ) electromagnetic implants , both on the incus and on the round window [ 11 , 12 ]  . 
cbct may offer a valuable alternative to msct in vsb hearing implants , as the patients most of whom are children require periodic follow - up , and cbct delivers lower radiation doses . 
 the purpose of this study was to evaluate a cohort of hearing - impaired patients with middle ear implants to determine how much dose could be saved by studying the la cone beam computed tomography ( cbct ) o tomografia a fascio conico rappresenta una evoluzione della tomografia computerizzata convenzionale ( tc ) , condividendone caratteristiche di natura fisica , come lutilizzo di radiazioni ionizzanti , la capacit di ottenere immagini di elevata qualit , e la possibilit di studiare le varie strutture anatomiche con ricostruzioni multiplanari e tridimensionali ; si differenzia dalla progenitrice tc per le dimensioni ridotte , i costi contenuti , il limitato campo di vista e la minore dose radiante somministrata al paziente [ 14 ]  . 
le prime applicazioni della cbct sono state realizzate in campo odontoiatrico e maxillo - facciale , in parte sostituendo lortopantomografia e la tc multistrato ( mstc ) , per le quali linsufficiente informazione spaziale per la prima , e la dose radiante per la seconda rappresentavano dei limiti . 
la cbct ha rivestito un ruolo primario nellimplantologia dentale , per la capacit di fornire una stima dello spessore e della profondit dellosso alveolare residuo e nellevidenziare strutture anatomiche a rischio durante le procedure chirurgiche , come il canale mandibolare , il foro mentoniero , il dotto naso - palatino ed il seno mascellare ; inoltre , la cbct trova impiego anche nella valutazione delle articolazioni temporo - mandibolari , delle lesioni neoplastiche dellosso , e dei singoli elementi dentari [ 57 ]  . lutilizzo della cbct si sta imponendo in campo otologico , dove la mstc rappresenta il gold standard [ 8 , 9 ]  . 
le prime indicazioni cliniche hanno riguardato patologie dellorecchio medio che determinavano ipoacusia di tipo trasmissivo , al fine di comprendere quale struttura di conduzione fosse lesa , o per il follow - up dei pazienti sottoposti ad intervento di ossiculoplastica [ 10 ]  . 
successivamente la cbct stata impiegata per limaging postoperatorio ed il follow - up dei pazienti impiantati con protesi elettromagnetiche vibrant soundbridge ( vsb ) sia allincudine che alla finestra rotonda [ 11 , 12 ]  . 
la cbct pu rappresentare una valida alternativa allo studio mstc in questo tipo di 1310 radiol med ( 2009 ) 114 : 13081318 petrous bones with cbct rather than with mstc , as well as to evaluate image quality obtained with the two techniques . materials and methods patients the study was conducted on 100 hearing - impaired patients ( mean age 26 years , range 743 ) who , after initial clinical and aetiological assessment at our hospitals ear , nose and throat department , were treated with vsb implants on the round window . 
the time period considered spanned from may 2004 to november 2007 . postoperative follow - up included periodic functional tests to demonstrate restoration of hearing and radiological examinations to define the position of the implant and identify possible dislocations where clinically suspected . patients underwent conventional radiology ( anteroposterior and lateral skull radiography ) and / or computed tomography ( msct / cbct )  . equipment cbct images were obtained with maxiscan equipment ( qr - dvt 9000 , verona , italy ) , which generates a pulsed emission of a fixed 110 - kvp conical beam of x - rays rotating around the patients head and is capable of reconstructing a cylindrical volume with a diameter and height of 15 cthe 400 - cm2 - wide detector is made up of an image intensifier coupled with a ccd camera [ 1 , 2 , 13 , 14 ]  . 
raw data are processed with primary reconstruction to obtain sections in the axial plane or other planes specified by the operator of a nominal thickness of 1 mm ( in the protocol used )  . 
on the basis of the anteroposterior and lateral projection tomograms , cbct calculates the milliampere per second ( mas ) values for the axial scan ( generally between 100 and 150 mas )  . msct images of the petrous bones were obtained with a 120 - kvp , 60 - mas , low - exposure protocol in the transverse plane with electronic reconstruction in the coronal plane ( thickness 1 mm ; spiral technique ; pitch 0.4 ) using a brilliance ct 6 msct device ( philips , eindhoven , the netherlands )  . measurement of values of exposure to ionising radiation a comparison between the doses delivered to the patients and the associated radiological risk was performed with both devices . 
 lo scopo del presente lavoro quello di valutare una coorte di pazienti ipoacusici impiantati allorecchio medio per definire il risparmio di dose ottenibile eseguendo lo studio delle rocche petrose mediante cbct rispetto allesame mstc e di valutare la qualit delle immagini ottenute con le due diverse tecniche . materiali e metodi pazienti sono stati inclusi 100 pazienti ipoacusici ( et media 26 anni , range 743 ) , inizialmente inquadrati dal punto di vista clinico ed eziologico presso listituto di otorinolaringoiatria della nostra struttura e successivamente trattati mediante posizionamento di protesi vsb alla finestra rotonda . 
lintervallo di tempo considerato stato tra il maggio 2004 ed il novembre 2007 . il follow - up post - operatorio di questi pazienti includeva lesecuzione periodica di test funzionali , in grado di provare la ripresa della capacit uditiva , nonch di esami radiologici , per la valutazione della posizione della protesi e la sua eventuale dislocazione , qualora clinicamente sospettata . 
questi pazienti sono stati sottoposti ad indagini di radiologia convenzionale ( rx cranio in antero - posteriore e latero - laterale ) e / o tecniche tomografiche computerizzate ( mstc / cbct )  . apparecchiature le immagini cbct sono state ottenute utilizzando lapparecchiatura maxiscan ( qr - dvt 9000 , verona , italia ) che genera una emissione pulsata di un fascio conico di raggi x , con tensione di 110 kvp , non modificabile , che ruota attorno alla testa del paziente , ed in grado di ricostruire un volume cilindrico con diametro e altezza di 15 c il rivelatore , con estensione di 400 cm2 , costituito da un intensificatore di brillanza accoppiato ad una videocamera con schermo ccd [ 1 , 2 , 13 , 14 ]  . 
i dati grezzi ottenuti sono rielaborati mediante ricostruzione primaria , ottenendo sezioni assiali o su altri piani indicati dalloperatore , con spessore nominale di 1 mm ( nel protocollo da noi utilizzato )  . 
the tlds were wrapped in polyethylene and inserted into the holes in the phantom at the sites of interest ( crystalline lens , thyroid , cerebrum , hypophysis and marrow of the skull and of c1 , c2 and c7 vertebrae and nuchal skin ) and at other significant sites to determine the dose distribution . the tlds , gr200a lithium fluorides ( central research laboratory , beijing , china ) , were read with a pcl3 reader ( fimel , vlizy , france ) while the annealing process occurred inside an ett oven ( fimel , vlizy , france )  . 
the dosimeters were calibrated in terms of air kerma for doses between 5 mgy and 30 mgy using an x - ray tube with 80 kvp and 2.8 mm al filtration , through comparison with an ionisation chamber . 
the phantom was examined at different times with cbct and msct , following the manufacturers protocols for the specific examination ( table 1 )  . the tlds readings were used to derive the air kerma values . 
le misure sono state effettuate posizionando 46 dosimetri termoluminescenti ( tlds ) allinterno della testa di un fantoccio antropomorfo rando ( alderson research laboratories , stanford , cn , usa )  . 
i tlds sono stati avvolti nel polietilene e quindi inseriti negli appositi fori del fantoccio sia in siti di interesse ( cristallino , tiroide , cervello , ipofisi , midollo osseo delle ossa della teca e delle vertebre cervicali c1 , c2 e c7 , cute nucale ) che in altre posizioni significative per la determinazione della distribuzione di dose . i tlds , fluoruri di litio del tipo gr200a ( central research laboratory , pechino , cina ) , sono stati letti con lettore pcl3 ( fimel , vlizy , francia ) mentre il processo di annealing ( temperaggio ) stato eseguito con un forno ett ( fimel , vlizy , francia )  . 
i dosimetri sono tarati in termini di kerma in aria per dosi comprese tra 5 mgy e 30 mgy , utilizzando un tubo radiologico con 80 kvp e filtrazione di 2 , 8 mm al , mediante confronto con camera a ionizzazione . tre tlds non sono stati irradiati in modo da poter sottrarre il segnale di fondo . 
il fantoccio stato esaminato in momenti diversi alla cbct e alla msct seguendo i protocolli predisposti dalle rispettive ditte fornitrici per lesame in oggetto ( tabella 1 )  . dalla lettura dei tlds sono stati ricavati i valori di kerma in aria ; moltiplicando questi ultimi per il rapporto dei coefficienti di assorbimento di energia massici ariamuscolo [ 15 ] si ottenuta la dose in tessuto . 
le dosi equivalenti impartite ai diversi organi ( ht , misurato in msv ) sono state ricavate moltiplicando la dose ottenuta mediante tlds per la frazione del volume dellorgano irradiato ( dt , misurato in mgy ) e per il coefficiente di peso della radiazione ionizzante ( wr ) : il coefficiente di peso per la radiazione considerato uguale a 1 . il contributo di un singolo organo / tessuto nel determinare il rischio globale del paziente durante lesposizione radiante viene ottenuto moltiplicando la dose equivalente ( ht ) per il coefficiente di peso del tessuto ( wt )  . 
the image obtained with cbct measures 15 cm in diameter and therefore does not cover the whole phantom section . the slice thickness of the reconstructed image was determined by measuring its width at half the height of the profile of the lamellae fitted into the appropriate insert . 
when measuring uniformity , the value considered was the maximum ratio between the average pixel values in the regions of interest ( roi ) placed at the centre and in four peripheral locations of an image of the homogeneous insert of the phanto finally , we assessed whether it was possible to visualise the various anatomical components of the tympanic cavity and specifically of the vsb implants to determine the position of the distal end at the level of the round window or of the long apophysis of the incus . results all 100 patients underwent msct within 6 h of surgery , according to the protocol . 
per le scansioni con la cbct limmagine ottenuta ha diametro di 15 cm , quindi non comprende lintera sezione del fantoccio . lo spessore di strato dellimmagine ricostruita stato determinato misurando la larghezza a met altezza del profilo delle lamelle inserite nellapposito inserto ; per evitare lerrore dovuto al campionamento stata determinata la media delle dimensioni in diverse posizioni dellimmagine . per la determinazione della risoluzione spaziale ad alto contrasto , nel fantoccio in plexiglas sono presenti otto serie di cinque fori pieni daria a sezione circolare con diametro da 2 , 5 mm a 0 , 75 mm distanziati fra loro in modo tale che la distanza fra i centri sia doppia del diametro del foro . 
per valutare la visibilit dei particolari stata selezionata la scala di grigi con finestra ridotta al minimo scegliendo il livello che meglio permette di distinguerli ; questi vengono considerati visibili se risultano tutti distinti . nel fantoccio sono inseriti dei cilindri con diametro di un pollice ( 25 , 4 mm ) immersi in acqua con le seguenti densit : policarbonato = 1 , 20 g / cm3 , acrilico = 1 , 19 g / cm3 , nylon = 1 , 10 g / cm3 , polistirene = 1 , 05 g / cm3 , polietilene = 0 , 95 g / cm3 . questi inserti possono fornire una indicazione della risoluzione a basso contrasto . 
per la misura delluniformit viene considerato il massimo rapporto fra i valori medi dei pixel nelle regioni di interesse ( roi ) posizionate al centro ed in quattro posizioni alla periferia di una immagine acquisita in corrispondenza dellinserto omogeneo del fantoccio . 
 stata infine valutata la possibilit di evidenziare le diverse componenti anatomiche presenti allinterno del cavo timpanico , e nel caso specifico delle protesi vsb , in particolare per definire con certezza la posizione dellestremo distale a livello della finestra rotonda o allapofisi lunga dellincudine . risultati tutti i 100 pazienti sono stati sottoposti a esame mstc entro le 6 ore dallintervento , come da protocollo postchirurgico . 
successivamente , in corso di follow - up , i pazienti che hanno eseguito rx cranio nelle proiezioni ortogonali sono stati 2 / 100 ; i pazienti studiati mediante mstc delle rocche petrose sono stati 15 / 100 , e 85 / 100 mediante cbct . 
1a , b paziente portatore di impianto vibrant soundbridge alla finestra rotonda . sezione assiale msct ( a ) e corrispondente immagine cbct ( b ) che mostra il corretto posizionamento della massa vibrante . 85 / 100 were studied with cbct . 
with regard to the crystalline lens , the measured dose was 4.5 mgy for cbct and 15.5 mgy for msct , values that are substantially lower than those likely to cause deterministic effects , even after repeated exams . an overall analysis of the single results shows that the effective dose delivered to the individual patient during cbct of the ear was equal to 39.2% of the dose imparted during msct . 
per quanto riguarda il cristallino la dose risultata pari a 4 , 5 mgy per la cbct ed a 15 , 5 mgy per la mstc , valori decisamente inferiori a quelli che possono provocare effetti deterministici anche per esami ripetuti . 
 da una analisi globale dei singoli risultati si evince come la dose efficace somministrata ad un paziente durante esame cbct dellorecchio sia il 39 , 2% rispetto a quella di unindagine mstc : nello specifico la dose efficace della mstc stata di 0 , 28 msv , mentre quella della cbct stata di 0 , 11 msv . results of image quality are summarised in table 3 . 
con queste premesse , abbiamo considerato leventualit di sottoporre i pazienti operati ad un follow - up radiologico che sfruttasse tecniche alternative alla mstc : poich metodiche non ionizzanti non erano usufruibili , la radiografia standard del cranio e la cbct rappresentavano le uniche opzioni . 
 tutti i 100 pazienti della nostra casistica sono stati valutati nellimmediato post - operatorio come da protocollo ( entro le 6 ore ) mediante esame mstc al fine di escludere focolai emorragici in sede di intervento o un eventuale mal posizionamento della protesi . 
il follow - up standard includeva lesecuzione di una indagine mstc a 6 settimane , ossia allattivazione dellimpianto elettromagnetico , ed a 1 radiol med ( 2009 ) 114 : 13081318 1315 fig . 
4a , b low - contrast resolution on msct ( a ) and cbct ( b ) refers to the systems ability to distinguish small - sized objects against a low - contrast background . 
4a , b la risoluzione a basso contrasto per la mstc ( a ) e per la cbct ( b ) intesa come la capacit del sistema di distinguere oggetti di piccole dimensioni in un contesto di basso contrasto . 
 evidente la migliore capacit discriminativa della mstc rispetto alla cbct . discussion this study sought to identify the technique providing the best ratio between diagnostic quality and patient dose in the evaluation of the correct position of vsb ear implants . 
quindici / 100 pazienti hanno seguito liter tradizionale , e quindi sono stati studiati mediante mstc . il follow - up da noi proposto implicava lesecuzione di un rx cranio e / o di una cbct rispetto alla mstc : i primi 1316 radiol med ( 2009 ) 114 : 13081318 fig . 
5a , b uniformity is defined as the maximum ratio between the average values of pixels in different regions of interest , with one placed at the centre of the image and four in peripheral locations . 
5a , b luniformit definita come il massimo rapporto fra i valori medi dei pixel di regioni di interesse poste una al centro e quattro in periferia , con la mstc ( a ) e con cbct ( b )  . 
fifteen out of 100 patients were followed up with the standard protocol ( msct )  . the experimental follow - up protocol involved performing skull radiography and / or cbct instead of msct . 
finally , cbct was considered sufficient so that msct could be reserved for cases suspected to have more severe complications than implant dislocation ( no case in the period in question )  . analysis of dosimetric data , in agreement with the literature [ 1822 ] , showed that the use of cbct permits considerable dose saving compared with msct . 
in addition , although cbct provides lower - quality images , these are nonetheless adequate for evaluating the position of the hearing implant . in contrast to msct , cbct scans and reconstructions are not affected by artefacts related to the metallic components of the vibrating mass of the implant , which often limit visualisation of the structures being investigated . 
these two 2 / 100 pazienti hanno espletato indagine rx del cranio nelle proiezioni ortogonali , dalla quale non si riuscivano ad estrapolare sufficienti reperi , e quindi stata abbandonata e non riproposta nei successivi pazienti . 
si infine ritenuto sufficiente lesecuzione di questa sola metodica , riservando la mstc a quelle circostanze in cui il sospetto fosse di complicazioni pi gravi della semplice dislocazione della protesi ( nessun caso nella nostra casistica nel periodo in esame )  . lanalisi dei dati dosimetrici , in accordo con la letteratura [ 1822 ] , dimostra come lutilizzo della cbct comporti una considerevole riduzione di dose alla mstc , determinata in particolare dalla geometria del fascio , dal tipo di emissione ( pulsata , rispetto ad unemissione continua su tutto langolo di rotazione del tubo ) e da una maggiore efficienza di rilevazione . 
a differenza della mstc , la cbct non presenta nelle scansioni e nelle successive ricostruzioni artefatti derivanti dalle componenti metalliche della massa vibrante dellimpianto acustico , procuranti spesso limitazioni nella visualizzazione delle strutture dinteresse . 
la cbct conferma di avere una buona risoluzione ad alto contrasto ma a differenza della mstc risulta deficitaria nel basso contrasto : queste due caratteristiche conferiscono alla cbct la capacit di visualizzare con buona risoluzione di contrasto le strutture ossee , mentre con difficolt i tessuti molli . 
lorecchio medio una struttura anatomica , inserita in un contesto osseo , la rocca petrosa dellosso temporale , e riempita di aria attraverso la tuba di eustachio ; al suo interno la trasmissione del suono garantita dalla catena ossiculare , formata da singoli ossicini . 
la cbct riesce le diverse componenti a evidenziare correttamente radiol med ( 2009 ) 114 : 13081318 1317 characteristics mean that cbct visualises bone structures with good contrast resolution , whereas it is somewhat limited in depicting soft tissues . 
cbct correctly depicts the various anatomical components within the tympanic cavity and , in the case of vsb implants , allows accurate definition of the position of the distal end at the level of the round window or of the long apophysis of the incus . 
 because cbct has been reported to impart smaller radiation doses compared with msct , we attempted to determine the difference in dosimetric performance between the devices available at our department . 
data analysis showed that cbct delivers a patient dose equal to 39% of that imparted by msct with a low - dose protocol . according to the directive of the dimond iii european research group , when choosing between two techniques capable of solving a diagnostic problem , one needs to take into account both its usefulness in depicting the object being studied and the patient dose [ 23 ]  . 
in the case of vsb devices , it is important to consider that the majority of patients are children , and they have to undergo a intensive postoperative follow - up protocol involving repeated radiological examinations . 
such patients are those most likely to be affected by the cumulative effects of ionising radiation . cbct meets the european criteria for diagnostic capability , and its place in otology where msct is still the gold standard should be reassessed . 
 the limitations of this study , in which the comparison was based on the standard protocols in use at our hospital and on the best costbenefit ratio for each of the ct scanners available at the time of assessment , concern the unexpressed potential for reducing the msct dose by refining the protocol . 
however , there remains an objective difference between the doses delivered to individual patients , even after attempting to stress the protocols at a dosimetric level , which is due to the intrinsic characteristics of the two ct applications . 
we therefore believe that our study may encourage a more widespread use of cbct in other fields as well , given that while yielding the same diagnostic information , cbct allows lower patient doses and lower costs per examination . anatomiche presenti allinterno del cavo timpanico e , nel caso specifico delle protesi vsb , a definire con certezza la posizione dellestremo distale a livello della finestra rotonda o allapofisi lunga dellincudine . 
 dalla letteratura si conferma come la cbct somministri una quantit di radiazioni ionizzanti minore rispetto alla mstc ; si quindi voluto ottenere un riscontro oggettivo della differenza di prestazioni dosimetriche fra le apparecchiature a disposizione presso il nostro dipartimento . 
a conclusione dei rilievi e dellelaborazione dei dati si rileva come la cbct eroghi una dose radiante pari al 39% di quella della mstc con protocollo a bassa esposizione . secondo la raccomandazione del gruppo di ricerca europeo dimond iii nella scelta fra due tecniche bisogna considerare sia lutilit della stessa nel mettere in evidenza loggetto di studio , sia la dose radiante , se il quesito diagnostico viene soddisfatto [ 23 ]  . 
nel caso delle protesi vsb si deve tenere conto che spesso i pazienti sono in et pediatrica e che dal momento dellintervento entrano a far parte di un protocollo di follow - up radiologico intenso , composto da controlli ripetuti ; sono proprio questi pazienti che pi potrebbero risentire degli effetti cumulativi delle radiazioni ionizzanti . 
 i limiti di questo lavoro , nel quale il confronto stato compiuto secondo i protocolli di comune uso nella pratica clinica nella nostra struttura , e secondo il miglior rapporto costo - beneficio per ognuna delle macchine a tecnologia tc possedute al momento della valutazione dei pazienti , riguardano la potenzialit non espressa di diminuire la dose in msct , affinando il protocollo : resta comunque oggettivo il divario tra le dose impartite ai singoli pazienti , anche cercando di stressare dosimetricamente i protocolli , proprio per le caratteristiche intrinseche delle due diverse applicazioni di tecnologia tc , e per questo noi riteniamo che questo lavoro possa comunque essere di stimolo per cercare di diffondere luso della cbct anche in altre applicazioni , in modo da ridurre la dose al paziente , poich in caso di parit di informazione diagnostica si ha una minor dose al paziente e un minor costo per esame . conclusioni conclusions during cbct of the ear , the radiation dose delivered to the patient is lower than that of msct performed with a lowdose protocol . 
in comparison with msct , cbct provides an image quality that is lower in terms of low - contrast resolution and uniformity and slightly lower in terms of highdurante un esame cbct dellorecchio la dose radiante somministrata al paziente inferiore a quella erogata dalla tc con protocollo a bassa esposizione . 
la qualit dellimmagine ottenuta con cbct , rispetto alla mstc , minore in termini di risoluzione a basso contrasto e uniformit , leggermente inferiore per risoluzione ad alto contrasto , mentre equivalente per quanto riguarda lo 1318 radiol med ( 2009 ) 114 : 13081318 contrast resolution , whereas slice thickness is equal . 
the images are sufficiently diagnostic to identify the correct placement of vsb , both on the round window and on the incus , with the advantage of lower radiation exposure for the patient . 
sorrentino , via san lorenzo 291 / a , 90146 palermo , italy , tel . : + 39 - 091 - 6552335 , fax : + 39 - 091 - 6552337 , e - mail : drdiving@yahoo.it received : 05 junuary 2007 / accepted : 22 april 2008 / published online : 30 january 2009 springer - verlag 2009 abstract purpose . 
thirteen patients with a magnetic resonance imaging ( mri ) diagnosis of pcl lesions ( ten acute and three chronic ) and 20 healthy controls underwent conventional and compound hrus performed by the same radiologist who was blinded to the subjects case - control status . 
tredici pazienti con diagnosi rm di lesione del lcp , 10 acuta e 3 cronica , sono stati sottoposti ad hrus convenzionale e compound eseguita in cieco dallo stesso radiologo . 
in consenso ed in cieco altri due radiologi hanno misurato nelle immagini hrus lo spessore degli lcp , quindi i casi sono stati classificati in normali / patologici e questi ultimi in acuti / cronici . 
nelle immagini hrus convenzionali e compound lo spessore del lcp era rispettivamente nel normale 4 , 50 , 7 mm e 4 , 60 , 7 mm , nelle lesioni acute 9 , 11 , 5 mm e 9 , 21 , 7 mm e nelle croniche 70 , 9 mm e 70 , 8 mla riproducibilit intermetodo nella misurazione dello spessore del lcp nelle immagini convenzionali versus compound era del 98 , 6% . 
lhrus consente lo studio del lcp con riconoscimento incidentale delle alterazioni traumatiche . radiol med ( 2009 ) 114 : 312320 keywords posterior cruciate ligament knee sonography real - time spatial compound sonography magnetic resonance imaging parole chiave legamento crociato posteriore ginocchio ecografia real - time spatial compound risonanza magnetica introduction introduzione posterior cruciate ligament ( pcl ) lesions are a relatively uncommon consequence of traumatic knee injuries , and the reported incidence of pcl rupture ranges between 1% and 44% of all acute injuries of the knee ligaments [ 1 ]  . 
in addition , in acute settings , many of the manoeuvres used for diagnosis , among which the most important is the posterior drawer test , may give false - negative results [ 2 , 3 ]  . arthroscopy permits direct visualisation of pcl lesions and is considered the diagnostic standard . 
however , it is an invasive procedure characterised by postprocedural discomfort and a small but finite complication rate ( 1.4% of cases ) and should preferably be performed for therapeutic purposes [ 4 ]  . 
diagnostic imaging modalities such as computed tomography ( ct ) and magnetic resonance imaging ( mri ) allow noninvasive visualisation of the pcl and hence play a key role in detecting and evaluating traumatic pcl lesions . 
mri is a reliable noninvasive technique , but its use is limited by high costs though lower than those of arthroscopy and reduced availability , especially of high - field - strength units . in contrast , high - resolution ultrasonography ( hrus ) is a inexpensive , noninvasive and widely available technique . 
in studying the knee joint , hrus has proved to be highly reliable for evaluating extra - articular disease [ 6 ] but has yielded conflicting results in evaluating cruciate ligament and meniscal injuries [ 710 ]  . 
by reducing the negative effect of acoustic artefacts ( speckle and clutter ) and increasing the definition of tissue planes , real - time spatial compounding allows better spatial and contrast resolution . 
la diagnosi clinica allesame obiettivo , soprattutto in fase acuta , pu essere molto difficoltosa e / o pu sottostimare lentit della lesione . in queste condizioni molte delle manovre cliniche , e tra queste la pi rilevante il test del cassetto posteriore , possono risultare falsamente negative [ 2 , 3 ]  . 
 anche se lartroscopia rappresenta lo standard diagnostico , consentendo la visualizzazione diretta delle lesioni del lcp , una procedura invasiva eseguita preferibilmente a scopi terapeutici , caratterizzata da discomfort post - procedurale e con bassa , seppur presente , incidenza di complicanze ( 1 , 4% dei casi ) [ 4 ]  . 
la diagnostica per immagini , mediante la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm ) , consente la visualizzazione non invasiva del lcp e pertanto riveste un ruolo fondamentale nellidentificazione e valutazione delle alterazioni traumatiche del lcp . 
la rm una metodica affidabile e non invasiva , ma condizionata dallalto costo , comunque inferiore a quello dellartroscopia , e dalla ridotta diffusione sul territorio , specialmente se ci riferiamo alle apparecchiature ad alta intensit di campo . 
nello studio dellarticolazione del ginocchio lhrus si dimostrata molto affidabile nella valutazione delle alterazioni delle strutture extra - articolari [ 6 ] mostrando risultati controversi nella valutazione della alterazioni dei legamenti crociati e dei menischi [ 710 ]  . 
il real - time spatial compound riducendo linterferenza negativa degli artefatti acustici ( speckle and clutter ) consente una migliore risoluzione spaziale e di contrasto incrementando la tissue - plane definition . 
mri was performed with both low - field - strength ( artoscan c , esaote biomedica , genoa , italy ) and high - field - strength ( signa excite hd , ge medical systems , milwaukee , wi , usa ) units . 
the acute or chronic nature of lesions was established on the basis of previously published mri criteria [ 12 , 13 ]  . to assess the reliability of hrus with and without spatial compounding and determine the normal appearance of the pcl , a group of 20 healthy volunteers ( 12 men and eight women ; age range 2036 years ; mean age 24.6 ) with no history of traumatic or degenerative knee lesions and who had not undergone mri evaluation were enrolled as controls . 
in accordance with the declaration of helsinki [ 14 ] , approval by the ethics committee was not required . hrus technique conventional and real - time spatial compound hrus imaging was performed by the same radiologist , who was blinded to the subjects case - control status . 
patients underwent hrus of the affected knee only , and controls underwent hrus of one knee , which was chosen by tossing a co in consideration of the results obtained by miller in patients and controls , pcl thickness of the contralateral knee was not measured [ 7 ]  . 
hrus examinations were carried out on an hdi 5000 scanner ( atl - philips , bothell , wa , usa ) with a high - resolution multifrequency lineararray transducer ( 712 mhz )  . 
the proximal end of the probe was pushed down as much as possible with the heel - toe manoeuvre [ 8 ] and tilted slightly to achieve a plane parallel to the long pcl axis . 
hrus criteria used to define the presence of an acute pcl lesion were : ( 1 ) marked hypoechogenicity with nonvisualisation of the normal fibrillar pattern , ( 2 ) thickening , ( 3 ) ill - defined irregmateriali e metodi popolazione in un periodo di 15 mesi , 13 pazienti con diagnosi rm di lesione del lcp , 8 uomini e 5 donne ( et compresa tra 19 e 36 anni ; et media 24 , 5 anni ) , 10 ( 73 , 3% ) con lesione acuta e 3 ( 26 , 7% ) con lesione cronica , sono stati sottoposti ad hrus con tecnica convenzionale e con lapplicazione del real - time spatial compound . 
le indagini rm erano state eseguite sia con apparecchiature a basso campo ( artoscan c ; esaote biomedica , genova , italia ) che ad alto campo ( signa excite hd , ge medical systems , milwakee , wisconsin , usa )  . 
 per valutare laffidabilit dellhrus con entrambe le tecniche e dimostrare il normale aspetto del lcp stato reclutato un gruppo controllo non sottoposto a valutazione rm composto da 20 volontari sani , 12 uomini e 8 donne ( et compresa tra 20 e 36 anni ; et media 24 , 6 anni ) , con anamnesi negativa per patologia traumatica o degenerativa del ginocchio . 
i pazienti e i controlli informati degli scopi dello studio e delle modalit operative delle varie procedure hanno fornito in forma scritta il proprio consenso informato a partecipare allo studio . 
in considerazione del rispetto delle norme della dichiarazione di helsinki [ 14 ] non stato richiesto il parere del comitato etico . tecnica hrus le indagini hrus ( convenzionale e con real - time spatial compound imaging ) sono state eseguite in cieco dallo stesso radiologo non a conoscenza dei pazienti e dei controlli . 
nei pazienti il ginocchio sottoposto a valutazione hrus stato quello affetto dalla patologia del lcp ; nei volontari stato valutato un solo ginocchio ed il lato da valutare stato scelto in modo random con luso di una moneta prima dellindagine . 
per lesecuzione delle indagini hrus stata utilizzata unapparecchiatura hdi 5000 ( atl - philips , bothell , wa , usa ) utilizzando una sonda lineare multifrequenza ( 712 mhz ) ad alta risoluzione . 
each conventional and compound hrus image was rated for echostructure and margins using a fourpoint scale : ( 1 ) unacceptable , ( 2 ) poor quality but marginally acceptable , ( 3 ) good quality and ( 4 ) excellent quality . analysis of variance to quantify differences in pcl thickness measured with conventional and compound hrus was carried out by another author who pooled the results of the measurements obtained . 
measurements were reported as averagestandard deviation ( sd )  . results as no patient enrolled in the study was obese , the results of the hrus examinations were unaffected by this potential limitation . 
these patients underwent arthroscopy , which confirmed the pcl injury . the remaining three patients with pcl injury underwent physiotherapy , and the injury was confirmed by follow - up mri at 2 months . 
lanalisi della varianza dello spessore per quantizzare le differenze della misurazione legate alla metodica hrus ( convenzionale versus compound ) stata eseguita da un altro autore che ha combinato i risultati delle misurazioni ottenute . 
 risultati nessuno dei pazienti pervenuti alla nostra osservazione e reclutati nello studio era obeso ; pertanto il risultato delle indagini ecografiche non stato inficiato da questo 316 radiol med ( 2009 ) 114 : 312320 possibile limite . 
nei pazienti con lesione del lcp abbiamo evidenziato in tutti i casi nella classificazione della lesione come acuta o cronica una completa concordanza tra la classificazione rm e quelle hrus . 
 in 10 / 13 pazienti ( 76 , 92% ) , 8 con lesione acuta e 2 con lesione cronica del lcp , stata evidenziata alla rm unalterazione associata : al legamento crociato anteriore nel 70% e ai menischi nel 60% . 
lo spessore del lcp nelle lesioni acute era 9 , 11 , 5 mm nelle immagini hrus convenzionali e 9 , 21 , 7 mm in quelle con lapplicazione real - time spatial compound . 
mentre lo spessore del lcp nelle lesioni croniche era 70 , 9 mm nelle immagini hrus convenzionali e 70 , 8 mm in quelle con lapplicazione real - time spatial compound . 
confrontando lo spessore nelle immagini hrus convenzionali versus quello nelle compound stata rilevata una riproducibilit inter - metodo del 98 , 6% . le immagini hrus convenzionali e compound nella valutazione dellecostruttura degli lcp patologici hanno ricevuto un punteggio rispettivamente di 2 , 70 , 6 e 3 , 30 , 3 , in quella del margine superficiale un punteggio rispettivamente di 2 , 90 , 3 e 4 e in quella del margine profondo un punteggio rispettivamente di 2 , 40 , 7 e 3 , 50 , 5 . 
 le lesioni del lcp sono poco comuni essendo il risultato di traumi di notevole intensit e le cause di maggiore incidenza sono i traumi sportivi e della strada [ 15 ]  . 
in precedenza alcuni autori [ 79 ] hanno eseguito una valutazione ecografica non in cieco del lcp in volontari sani e in soggetti con lesioni acute o croniche ma nessuno ha mai effettuato valutazioni hrus in cieco . 
le scansioni hrus convenzionale ( a ) e real - time spatial compound ( b ) mostrano una formazione semilunare ipoecogena a struttura fibrillare , con margini regolari , ben distinguibile dal tessuto adiposo limitrofo iperecogeno . discussione results , with 100% sensitivity , specificity and positive predictive value . 
le scansioni hrus convenzionale ( a ) e real - time spatial compound ( b ) mostrano ispessimento e marcata ipoecogenicit del lcp con mancata identificazione del disegno fibrillare , irregolarit e sfumatura del margine superficiale , e scarsa identificazione del margine profondo . 
3a - c chronic injury of the posterior cruciate ligament ( pcl ) on conventional ( a ) and real - time spatial compound high - resolution ultrasonography ( hrus ) images ( b ) : thick and inhomogeneously hyperechoic structure with nonvisualisation of normal fibrillar pattern , irregular and smooth margins and inhomogeneity of the surrounding fat . 
le scansioni hrus convenzionale ( a ) e real - time spatial compound ( b ) mostrano aumentato di spessore e disomogenea iperecogenicit del lcp con mancata identificazione del disegno fibrillare , irregolarit e sfumatura dei margini , e disomogeneit del tessuto adiposo limitrofo . 
as reported by schulz et al . , knowledge of the biomechanics of the injury is crucial , as it can prompt the search for multiple ligament injuries or meniscal lesions [ 1 ]  . 
although there are previous reports [ 79 ] of unblinded sonographic evaluations of the pcl in healthy volunteers and in patients with acute or chronic injuries , ours is the first study to have performed blinded hrus evaluations . 
the evaluation of conventional and compound hrus images revealed that both techniques allow identification of diagnostic criteria , enabling detection of normal or injured pcls and acute or chronic injuries . 
the wider variability of the thickness values found in these studies may be explained by : ( 1 ) interindividual and interracial variations in the populations studied , for which no anthropometric correlation was determined in either our study or previous studies , ( 2 ) the level of measurement of pcl thickness differed between our study and previous studies ; in particular , cho et al . 
 [ 8 ] measured pcl thickness at the level of the tibial spine , whereas miller did not specify the level of measurement [ 7 ]  . pcl thickness in acute lesions was 9.11.6 mm on conventional hrus images and 9.21.7 mm on compound valutazione comparativa tra i due lcp normali nei volontari sani . 
la valutazione delle immagini hrus ottenute con la tecnica convenzionale e con quella compound ha messo in evidenza come con entrambe stata possibile lidentificazione dei criteri diagnostici per la classificazione degli lcp in normali / patologici e in questi ultimi in acuti e cronici . 
la nostra esperienza pertanto come confermato dalla variabilit intermetodo , con un valore del 98 , 6% , non ha mostrato differenze significative tra lhrus convenzionale e quella con lapplicazione compound nella capacit di caratterizzazione del lcp . 
pertanto entrambe hanno permesso in tutti i casi la corretta classificazione del lcp come normale o patologico con completa concordanza tra la classificazione sulle immagini rm e quella eseguita sulle immagini hrus ottenute con la tecnica convenzionale e con lapplicazione compound . nei volontari sani lo spessore del lcp misurato nelle immagini hrus eseguite senza e con compound risultato rispettivamente di 4 , 50 , 7 mm e 4 , 60 , 7 mnon stata evidenziata una differenza statisticamente significativa nello spessore del lcp misurato con entrambe le tecniche . 
 lo spessore del lcp nelle lesioni acute era 9 , 11 , 6 mm nelle immagini hrus convenzionali e 9 , 21 , 7 mm in quelle con lapplicazione compound . 
 [ 8 ] si rileva , come gi evidenziato in precedenza nella comparazione dello spessore dei lcp normali , una maggiore dispersione dei valori di spessore rispetto a quelli del nostro studio e le possibili giustificazioni sono le medesime prima menzionate per gli lcp normali . 
in our study , we classified pcl injuries as acute or chronic and separately evaluated the diagnostic role of the two hrus techniques in each injury . a comparison of our results with those of miller [ 7 ] and cho et al . 
although not an objective of this study , the use of pcl thickness alone as a diagnostic criterion proved unhelpful for classifying chronic injuries but relatively useful in acute injuries , as statistical analysis revealed a significant difference between the thickness of acutely injured and normal pcls . as with other muscles , tendons and ligaments , the pcl is mainly composed of specular reflectors . 
when these structures are insonated , the amplitude of the echo strongly depends on the angle of incidence the greatest amplitude being obtained when the ultrasound beam is perpendicular to the structure [ 11 ]  . 
averaging the images obtained from different angles of insonation results in suppression of artefacts , with improved image quality and a better signal - to - noise ratio [ 17 ]  . our comparison of conventional and compound hrus showed that the latter provides better visualisation of anatomical details , and in particular , improves fibrillar echostructure definition and pcl margins . 
in our experience , while not providing a diagnostic gain , compound imaging nevertheless improved depiction of the pcl and its pathological changes . one of the main limitations of spatial compounding is mostrato una certa utilit nella valutazione di quelli con lesioni acute mostrando rispetto ai normali una differenza statisticamente significativa . 
 llcp come altre strutture muscolo - tendineo - legamentoso costituito principalmente da reflettori speculari ; quando queste strutture vengono insonate lampiezza delleco di risposta dipende dallangolo di incidenza del fascio ultrasonoro e la maggiore ampiezza si ottiene quando questo perfettamente perpendicolare alla struttura in esame [ 11 ]  . 
le immagini hrus convenzionali sono spesso soggette allinterferenza degli artefatti a specchio e del rumore , i quali riducono la qualit dellimmagine non consentendone a volte una corretta valutazione [ 16 ]  . 
tutti gli artefatti si combinano riducendo la risoluzione di contrasto con degradazione dellecostruttura e riduzione della definizione dei dettagli , ed in particolare dei margini ; inoltre si assiste alla riduzione della cospicuit delle piccole strutture a basso contrasto e alla possibile illusione di discontinuit delle strutture continue . 
il real - time spatial compound imaging acquisisce diverse immagini sovrapposte delloggetto da vari punti di vista ; queste immagini sono quindi processate con una media digitale e combinate in una singola immagine in tempo reale . dalla media delle immagini acquisite dai differenti punti di vista si ottiene la soppressione degli artefatti con incremento della qualit dellimmagine e ne risulta un migliore rapporto segnale - rumore [ 17 ]  . 
 nel nostro studio confrontando lhrus convenzionale con quella con lapplicazione compound abbiamo osservato nel secondo caso una pi accurata visualizzazione dei dettagli anatomici , ed in particolare una migliore identificazione dellecostruttura fibrillare e della definizione dei margini del lcp . 
le immagini hrus convenzionali e compound nella valutazione dellecostruttura degli lcp patologici hanno ricevuto un punteggio rispettivamente di 2 , 70 , 6 e 3 , 30 , 3 , con migliore visualizzazione del disegno fibrillare nelle immagini hrus compound . 
nella valutazione dei margini superficiale e profondo degli lcp patologici le immagini hrus convenzionali e compound hanno ricevuto per il margine superficiale un punteggio rispettivamente di 2 , 90 , 3 e 4 e in quella del margine profondo un punteggio rispettivamente di 2 , 40 , 7 e 3 , 50 , 5 . 
nonostante i punteggi ottenuti sulle immagini hrus con lapplicazione del compound siano migliori rispetto a quelli ottenuti dalle immagini hrus convenzionale nel nostro studio non sono state rilevate differenze statisticamente significative tra i punteggi ottenuti . 
 una delle maggiori limitazioni del compound la riduzione del frame rate con riduzione della risoluzione temporale 320 radiol med ( 2009 ) 114 : 312320 the decreased frame rate that occurs with lower temporal resolution and a resulting persistence effect . 
the main limitations of our study were : ( 1 ) small case series , which precluded stringent statistical validation , and ( 2 ) body habitus , in that our series did not include obese patients , in whom spatial resolution is reduced by the greater distance between the transducer and the pcl resulting from increased thickness of popliteal fossa fat ( even though this shortcoming may generally be overcome by using multifrequency transducers )  . 
hrus is not recommended in the diagnostic workup of patients with knee trauma , as adequate information is obtained about superficial structures only ( such as collateral ligaments ) , whereas the information on inner structures ( menisci and anterior cruciate ligaments ) is partial and often incomplete and unreliable . traumatic knee injuries may result in multiple lesions affecting the menisci , ligaments and bones , as seen in our population . 
given the high level of accuracy of hrus in detecting pcl lesions , the technique could be used for the follow - up of isolated chronic lesions , making the use of mri unnecessary and thus providing considerable cost savings . che risulta in effetti di persistenza . 
lhrus non raccomandata nel corretto iter diagnostico dei pazienti con patologia traumatica del ginocchio consentendo di ottenere adeguate informazioni solo sulle strutture superficiali , come i legamenti collaterali , ma parziali e spesso incomplete e inaffidabili su quelle profonde , come i menischi e il legamento crociato anteriore . 
lhrus come evidenziato nel nostro studio consente con buona accuratezza il riconoscimento delle alterazioni del lcp e potrebbe essere impiegata nel follow - up delle lesioni croniche isolate non rendendo necessario lutilizzo della rm , con marcata riduzione dei costi . 
clinical , histological and atypical radiological patterns selected among our cases il tumore fibroso solitario della pleura ( tfsp ) : patologia dai mille volti . clinica , istologia e rappresentazione degli aspetti radiologici insoliti selezionati dalla nostra casistica l . 
fava1 1istituto di radiologia , universit degli studi di torino , ospedale san luigi gonzaga , regione gonzole 10 , 10143 orbassano , italy 2reparto di radiologia , ospedale degli infermi , biella , italy 3s.c.d.u. 
sftp usually presents as a peripheral mass abutting the pleural surface , to which it is attached by a broad base or , more frequently , by a pedicle that allows it to be mobile within the pleural cavity . 
a precise preoperative diagnosis can be arrived at with a cutting - needle biopsy , although most cases are diagnosed with postoperative histology and immunohistochemical analysis of the dissected sample . 
sftp , owing to its large size or unusual locations ( paraspinal , paramediastinal , intrafissural and intraparenchymal ) , can pose interpretation problems or , indeed , point towards a diagnosis of diseases of a totally different nature . 
we present some unusual radiographic and computed tomography ( ct ) images of large sftp or sftp located in atypical thoracic locations in patients who underwent surgical resection . keywords mesenchymal neoplasms pleura computed tomography riassunto il tumore fibroso solitario della pleura ( tfsp ) , descritto per la prima volta da klemperer e rabin nel 1931 , una neoplasia mesenchimale che solitamente coinvolge la pleura , ma che viene descritta anche in altre sedi sia toraciche , quali il mediastino , il pericardio ed il parenchima polmonare , sia extratoraciche , quali le meningi , lepiglottide , le ghiandole salivari , la tiroide , i reni e la mammella . 
di solito si presenta come massa periferica a contatto con la superficie pleurica alla quale unito da una larga base dimpianto o pi spesso da un peduncolo che lo pu rendere mobile allinterno del cavo pleurico . 
la diagnosi preoperatoria di certezza pu essere ottenuta mediante biopsia con ago tranciante , ma nella maggior parte dei casi post - chirurgica , frutto dellesame istologico e dellanalisi immuno - istochimica sul pezzo operatorio . 
il tumore fibroso solitario della pleura tuttavia , spesso a causa delle notevoli dimensioni o dello sviluppo in sedi inconsuete ( paraspinali , paramediastiniche , intrascissurali ed intraparenchimali ) pu creare numerose difficolt di interpretazione o addirittura orientare la diagnosi verso patologie di tuttaltra natura . 
in questo lavoro presentiamo gli aspetti radiologici inusuali di tfsp di grosse dimensioni o localizzati in sedi toraciche atipiche in pazienti sottoposti ad intervento chirurgico di exeresi . parole chiave tumori mesenchimali pleura tomografia computerizzata radiol med ( 2009 ) 114 : 204215 introduction solitary fibrous tumour of the pleura ( sftp ) is a mesenchymal tumour that tends to involve the pleura , although it has also been described in other thoracic areas ( mediastinum , pericardium and pulmonary parenchyma ) and in extrathoracic sites ( meninges , epiglottis , salivary glands , thyroid , kidneys and breast ) [ 12 ]  . 
sftp usually presents as a peripheral mass abutting the pleural surface , to which it is attached by a broad base or , more frequently , by a pedicle that allows it to be mobile within the pleural cavity [ 24 ]  . 
unlike mesothelioma , sftp is not asbestos - related and is usually a benign , rarely aggressive , tumour , although a small percentage of patients may develop locoregional recurrence [ 2 , 5 , 6 ]  . 
 the most accredited hypothesis is that these tumours originate from submesothelial stromal cells with fibroblastic or myofibroblastic phenotype , whose growth is promoted by an aberrant reaction to inflammatory or hormonal stimuli [ 7 ]  . 
most patients are asymptomatic at the time of the diagnosis , with the lesion being discovered during a chest x - ray performed for other reasons [ 4 , 8 ]  . 
in the remaining patients , particularly those with large and aggressive masses , the most common clinical manifestations are chest pain , cough and dyspnoea [ 4 , 6 , 9 ]  . 
the rate of incidental diagnoses is increasing , as demonstrated by our series in which symptomatic patients did not exceed 30% and confirmed by a comparison of studies published between 1942 and 1972 and between 1973 and 1980 in which symptomatic patients decreased from 72% to 54% [ 4 ]  . 
sftp , owing to its large size or unusual locations ( paraspinal , paramediastinal , intrafissural and intraparenchymal ) , can pose interpretation problems or , indeed , point towards a diagnosis of diseases of a totally different nature . 
 we present some unusual radiographic and computed tomographic ( ct ) images selected from our case history of sftp located in atypical thoracic locations differential diagnosis . histology and immunohistochemistry introduzione il tumore fibroso solitario della pleura ( tfsp ) una neoplasia mesenchimale che solitamente coinvolge la pleura , ma che viene descritta anche in altre sedi sia toraciche , quali il mediastino , il pericardio ed il parenchima polmonare , sia extratoraciche , quali le meningi , lepiglottide , le ghiandole salivari , la tiroide , i reni e la mammella [ 1 , 2 ]  . 
generalmente si presenta come massa periferica a contatto con la superficie pleurica alla quale unito da una larga base dimpianto o pi spesso da un peduncolo che lo pu rendere mobile allinterno del cavo pleurico [ 24 ]  . il tfsp , a differenza del mesotelioma , non una malattia asbesto - correlata e di solito non presenta un comportamento aggressivo , sebbene una ridotta percentuale di pazienti possa andare incontro a recidive loco - regionali [ 2 , 5 , 6 ]  . 
lipotesi pi accreditata sostiene che questi tumori possano originare delle cellule stromali sottomesoteliali con fenotipo fibroblastico o miofibroblastico , alla cui crescita contribuisce unaberrante reattivit a stimoli infiammatori od ormonali [ 7 ]  . 
la maggior parte dei pazienti asintomatico al momento della diagnosi essendo la lesione riscontrata in occasione di un radiogramma del torace eseguito per altri motivi [ 4 , 8 ] ; nei restanti casi , soprattutto in presenza di lesioni di grandi dimensioni e con comportamento aggressivo , le pi comuni manifestazioni cliniche sono dolore toracico , tosse e dispnea [ 4 , 6 , 9 ]  . 
la percentuale di casi riscontrati occasionalmente in continuo aumento , come testimoniato dalla nostra casistica in cui la percentuale di pazienti sintomatici non supera il 30% e dal confronto fra studi pubblicati nel periodo 1942 1972 e nella decade successiva , in cui la percentuale di pazienti sintomatici si ridotta dal 72% al 54% [ 4 ]  . 
questi dati sono da attribuire ad una sempre maggiore ( e talora inappropriata ) diffusione delle metodiche di imaging , con un incremento del numero di casi scoperti in fase iniziale ed in modo del tutto occasionale . tali lesioni tuttavia , spesso a causa delle cospicue dimensioni o dello sviluppo in sedi inusuali ( paraspinali , paramediastiniche , intrascissurali ed intraparenchimali ) possono creare numerose difficolt di interpretazione o addirittura orientare la diagnosi verso patologie di tuttaltra natura . in questo lavoro , abbiamo selezionato dalla nostra casistica alcuni dei casi pi interessanti caratterizzati da aspetti radiologici inconsueti sia per sede che per dimensioni per i quali si dovuto sensibilmente ampliare il ventaglio delle possibili diagnosi differenziali . 
 sftp is a rare mesenchymal neoplasm , previously defined as benign localised mesothelioma or fibrous benign mesothelioma , although the use of these terms is discouraged owing to the potential confusion with mesothelioma . as the name suggests , it is usually a single , occasionally large , pleural neoplasm , although multiple forms have been reported in the literature [ 4 , 8 , 10 ]  . 
macroscopically , it istologia ed immuno - istochimica il tfsp una rara neoplasia mesenchimale , in passato definita mesotelioma benigno localizzato o mesotelioma fibroso benigno , termini il cui uso deve essere scoraggiato per la potenziale confusione con il mesotelioma . 
come il termine suggerisce una neoplasia pleurica singola , 206 radiol med ( 2009 ) 114 : 204215 originates from the visceral pleura [ 6 ] , to which it is often connected by a short pedicle [ 2 , 3 , 11 ]  . 
microscopically , the typical finding is that of a patternless pattern consisting of spindle cells with round nuclei with scarce cytoplasm arranged in bundles or in a fishbone configuration , in close contiguity with small vessels , resulting in a haemangiopericytoma - like appearance . 
sftp is usually histologically benign , but the presence of cellular atypia and a high mitotic index [ defined as being in excess of 4 / 10 high power field ( hpf ) ] is strongly indicative of malignancy [ 10 ]  . 
the differential diagnosis of sftp includes sarcomatoid mesothelioma , primary pleural synovial sarcoma and haemangiopericytoma [ 1 , 1921 ]  . talvolta di grosse dimensioni , anche se in letteratura ne sono state descritte forme multiple [ 4 , 8 , 10 ]  . 
solitamente i tfsp sono istologicamente benigni , ma la presenza di atipie cellulari e di un alto indice mitotico ( definito come maggiore di 4 / 10 hpf ) fortemente indicativa di malignit [ 10 ]  . 
la diagnosi differenziale dei tfsp include il mesotelioma sarcomatoide , il sarcoma sinoviale pleurico primitivo e lemangiopericitoma [ 1 , 1921 ]  . radiological aspects chest film sftp usually appears on chest x - ray as a peripheral opacity with well - defined borders and homogeneous density [ 8 , 9 , 2224 ]  . 
il versamento pleurico di natura reattiva ( sieroso o siero - emorragico ) concomitante in una proporzione di casi che varia in letteratura fra il 6% e il 17% [ 3 , 4 , 12 , 27 , 28 ] , soprattutto in presenza di forme maligne [ 3 , 8 , 29 ]  . la valutazione dellangolo di raccordo con la parete toracica permette la distinzione fra masse di pertinenza pleurica e lesioni parenchimali , risultando ottuso nei piccoli tumori a genesi pleurica , acuto nelle neoplasie intrapolmonari e nei tfsp di maggior volume e / o peduncolati [ 30 , 31 ]  . la mobilit e le modificazioni di morfologia , imposte dalle diverse fasi della dinamica respiratoria e / o dai diversi decubiti del paziente , accertate fluoroscopicamente , costituiscono i segni patognomonici di una lesione peduncolata di pertinenza pleurica [ 3 , 9 , 32 , 33 ]  . radiol med ( 2009 ) 114 : 204215 fig . 
f immunoistochimica20 : bcl2 +  . pathognomonic signs of a pleural pedunculated lesion and can be verified with fluoroscopic examination [ 3 , 9 , 32 , 33 ]  . tomografia computerizzata ( tc ) computed tomography ( ct ) the size of the lesion will strongly affect its appearance on computed tomography ( ct )  . 
smaller fibromas usually appear as homogeneous , well - defined , rarely lobulated masses forming obtuse angles against the pleural surface [ 3 , 22 , 34 , 35 ]  . 
i fibromi di piccole dimensioni si presentano di solito come masse ben delimitate , omogenee , solo occasionalmente lobulate , a contatto con la superficie pleurica e con angolo di raccordo ottuso [ 3 , 22 , 34 , 35 ]  . quando di cospicue dimensioni sono invece piuttosto disomogenee e con angoli di raccordo acuti . 
il riscontro di un angolo di raccordo a detta degli autori anglosassoni , smooth tapering [ 22 , 34 ] un altro segno tc affidabile di neoplasia a partenza pleurica . 
nei tumori intrascissurali esso bilaterale e ne facilita la distinzione da una massa 208 radiol med ( 2009 ) 114 : 204215 junction of the mass with the pleural surface [ 22 , 34 ] is another reliable ct sign of a neoplasm of pleural origin intrafissural tumours , the finding is bilateral , facilitating differentiation from an intraparenchymal mass ( fig 3 c , d ) [ 22 ]  . 
intralesional calcifications ( punctate , linear or coarse ) constantly associated with areas of necrosis may be recognised in larger lesions [ 3 , 4 , 8 , 22 ]  . 
the presence of the pedicle is rarely identified on ct but can be inferred by evaluating lesion mobility [ 4 , 36 ]  . sftp exhibits medium to high attenuation on baseline scans owing to the high physical density of the collagen fibres and the abundant vascular network of the lesions ( fig . 4c ) [ 4 , 36 , 37 ]  . 
con laumentare delle dimensioni , dopo somministrazione di mezzo di contrasto costante il riscontro di lesioni piuttosto disomogenee caratterizzate da un pattern tomodensitometrico definito a carta geografica oppure da aree serpiginose iperdense , espressione della ricca rete vascolare , cui possono associarsi aree ipodense , riferibili a fenomeni di degenerazione cistica fig . 
3a - d a 35 - year - old man with incidental finding of intrafissural lung opacity on chest x - ray ( a , b ) confirmed on axial computed tomography ( c ) and parenchymal ( d ) windows . 
involvement of hilar - mediastinal lymph nodes enables a diagnosis of sftp to be definitely excluded . differential diagnosis of sftp in atypical locations the differential diagnosis of primary pleural tumours is relatively narrow and includes , in addition to pleural fibromas and malignant mesothelioma , the rarer lipomas , synovial sarcomas and epithelioid haemangioendothelioma [ 3941 ]  . 
linteressamento linfonodale ilo - mediastinico esclude con certezza la diagnosi di tfsp . diagnosi differenziale delle localizzazioni insolite il ventaglio diagnostico differenziale dei tumori primitivi della pleura relativamente contenuto , coinvolgendo oltre ai fibromi pleurici solitari ed al mesotelioma pleurico maligno anche i pi rari lipomi , sarcomi e lemangioendotelioma epitelioide [ 3941 ]  . 
il problema della diagnosi differenziale si rende ancora pi complesso quando queste lesioni si sviluppano in sedi inconsuete , rendendo ancora pi ampio il numero di patologie che entrano in diagnosi differenziale . 
in these cases , it is important to evaluate the ribs : chest wall involvement by sftp is rare [ 4 , 42 ] and usually manifests as sclerosis or cortical erosion at the costal level , a feature more typical of tumours of neurogenic origin [ 4 ]  . sftp that have a mediastinal pleural origin can mimic a thymic neoplasm or dysembryogenetic tumour . 
in questi casi , la valutazione della parete toracica importante ; infatti , in letteratura , la presenza di segni di estensione parietale riportata molto raramente [ 4 , 42 ] e si manifesta generalmente come sclerosi o erosione costale , un aspetto pi caratteristico delle neoplasie di origine neurogena [ 4 ]  . se invece si sviluppano dalla pleura mediastinica possono simulare una neoplasia timica oppure un tumore disembriogenetico . 
5a - d a 74 - year - old woman with a mediastinal mass discovered incidentally on chest x - ray ( a , b ) and confirmed at computed tomography ( ct ) ( c , d )  . 
5a - d donna di 74 anni con riscontro occasionale ( a , b ) di lesione a partenza mediastinica , sospetto confermato alla tc ( c , d )  . 
intraparenchymal and inverted sftp present as pulmonary nodules or rounded or oval masses with well - defined margins and enter the differential diagnosis with some benign diseases ( hamartochondromatosis ) or with less aggressive lesions such as carcinoids [ 44 ]  . two reports in the literature address ct imaging of intrapulmonary pleural fibromas [ 44 , 45 ] , and only one of them describes ct features of intense , predominantly peripheral , heterogeneous enhancement [ 45 ]  . 
attualmente la tc multidetettore con le ricostruzioni multiplanari ottenute da acquisizioni sottili permettono una migliore visualizzazione della scissura ed i suoi rapporti con il tumore . 212 radiol med ( 2009 ) 114 : 204215 fig . 
6a , b solitary fibrous tumour of the pleura ( sftp ) in a 63 - year - old patient with an incidental finding of left paraspinal opacity on chest x - ray ( a , b ) , which was confirmed at computed tomography ( ct ) ( c ) and initially diagnosed as a neurogenic tumour . 
7a - c a 44 - year - old man with atypical precordial pain who underwent chest x - ray in the lateral view ( a ) and computed tomography ( ct ) with sagittal maximum intensity projection ( mip ) reformations ( b ) and transverse lung windowing ( c )  . 
a radiogramma mirato in proiezione laterale , b tc con ricostruzione mip in sezione sagittale e c tc in sezione assiale con finestra per il parenchima dimostrano la presenza di una lesione nodulare localizzata nel lobo superiore sinistro che data la stretta contiguit con le strutture bronchiali e vascolari stata sospettata la diagnosi di carcinoide . 
8a - d a 47 - year - old man with incidental finding of a 3 - cm opacity on chest x - ray . computed tomography ( ct ) ( a , b ) confirmed the presence of a well - marginated parenchymal mass within the left lower lobe ( c , d )  . 
la tc prima e dopo somministrazione di mezzo di contrasto ( a , b ) mostra un nodulo intraparenchimale a margini ben definiti nel contesto del lobo inferiore sinistro ( c , d ) , in stretta contiguit con un vaso polmonare ( d )  . 
la diagnosi istopatologica definitiva stata di tfsp . conclusion conclusione in conclusion , sftp is a rare mesenchymal neoplasm that is relatively easy to diagnose when located in typical sites , as the diseases entering the differential diagnosis are few and rare . 
cova1 1unit clinica operativa di radiologia , 2unit clinica operativa di anatomia ed istologia patologica , ospedale di cattinara , universit di trieste , strada di fiume 447 , 34149 trieste , italy correspondence to : e . 
seven intratumoural tissue components can be identified both at ct and at pathology : ( 1 ) solid component , ( 2 ) haemorrhagic component , ( 3 ) coagulation necrosis , ( 4 ) liquefactive necrosis , ( 5 ) parenchymal consolidation , ( 6 ) diffuse peripheral component and ( 7 ) fibrotic component . 
necrotic and haemorrhagic components are typically observed in malignant lesions , whereas solid and fibrotic components may be seen both in solid lung malignancies and in benign lesions . keywords lung tumours ct radiological - pathological correlation riassunto lo scopo di questa presentazione descrivere le componenti tissutali intratumorali presenti nei tumori polmonari solidi che risultino evidenti allanalisi macroscopica e / o microscopica del campione patologico , autoptico oppure chirurgico , e che siano identificabili anche allindagine tomografia computerizzata ( tc ) eseguita mediante metodica diretta e dopo la somministrazione di mezzo di contrasto . 
le componenti a carattere necrotico ed emorragico vengono osservate tipicamente nelle neoplasie maligne , mentre le componenti solide ed a carattere fibrotico possono essere osservate sia nei processi polmonari solidi a carattere maligno sia nelle lesioni benigne . 
malignant tumours are the most common , with bronchogenic carcinoma being the leading cause of death from cancer in many countries i tumori solidi del polmone rappresentano un reperto frequente al radiogramma diretto del torace oppure alla tomografia computerizzata ( tc )  . 
although surgery has a high success rate in the initial stages of disease [ 2 , 3 ] , survival and general outcomes are closely related to the histological type of the tumour . 
in particular , histological typing of primary lung tumours is based on their most differentiated components , whereas grading is based on the cell features of their least differentiated components [ 13 ]  . 
four histological types account for more than 95% of primary lung cancers : squamous cell carcinoma , adenocarcinoma , undifferentiated large cell carcinoma and small cell carcinoma ( microcytoma )  . 
squamous cell carcinoma is characterised by the presence of intercellular bridging ( thin parallel strands connecting adjacent cells ) , abundant keratin production by the individual cells ( intense eosinophilia of the single cells ) and formation of keratin pearls in the well - differentiated forms . adenocarcinoma is the most common histological type of lung cancer and represents almost 50% of all bronchogenic carcinomas . 
the tumour cells are large , with abundant cytoplasm , large nuclei , prominent nucleoli and a growth pattern of cords of uniform cells . giant cell carcinomas are a subtype of undifferentiated large cell carcinomas and are characterised by giant pleomorphic cells with bizarre morphology . 
anche se la chirurgia raggiunge un elevato livello di successo negli stadi iniziali della patologia [ 2 , 3 ] , la sopravvivenza ed il risultato generale della terapia sono strettamente correlati allistotipo tumorale . 
in particolare , listotipo dei tumori polmonari primitivi viene classificato sulla base delle aree tumorali maggiormente differenziate mentre il grading tumorale basato sulle caratteristiche cellulari delle aree tumorali meno differenziate [ 13 ]  . 
quattro istotipi corrispondono ad oltre il 95% delle neoplasie primitive polmonari : tumore a cellule squamose , adenocarcinoma , carcinoma indifferenziato a grandi cellule , e tumore a piccole cellule ( microcitoma )  . 
il tumore a cellule squamose caratterizzato dalla presenza di ponti intercellulari ( sottili linee parallele tra i bordi di cellule contigue ) , abbondante produzione di cheratina da parte delle single cellule ( intensa eosinofilia delle singole cellule ) , e della formazione di perle di cheratina nelle forme ben differenziate . 
il carcinoma del polmone a cellule giganti rappresenta un sottotipo del carcinoma indifferenziato ed caratterizzato da cellule giganti pleomorfe ed a morfologia radiol med ( 2009 ) 114 : 173189 fig . 
adenocarcinoma del polmone con pattern bronchioloalveolare con massiva diffusione lobare ( frecce ) ( d )  . lung cancers show several macroscopic patterns in relation to the type of growth : 1 . 
peripheral single - nodule or multiple - nodule lung carcinoma : in this macroscopic pattern , single or multiple peripheral nodules are seen within the lung , resembling a secondary lesion . 
lung carcinoma with subpleural diffusion : this growth pattern is distinctive of adenocarcinoma . the aim of this paper is to describe the intratumoural tissue components of solid lung cancers evidenced by macroscopic and / or microscopic analysis of autopsic or surgical specimens and are also visible on nonenhanced and contrast - enhanced ct . 
the purpose is to illustrate some characteristic patterns of lung cancers that can facilitate their characterisation by ct on the basis of the morphological evaluation of the lesion . intratumoural tissue components seven distinct intratumoural tissue components may be described that have correlates on both nonenhanced and contrast - enhanced ct and gross and / or microscopic / histological examination of the pathology specimen : 1 . 
fibrotic component these tissue components may be encountered separately or in various combinations within the same tumour . carcinoma bronchiale in ordine di frequenza , ed tipico del carcinoma a cellule squamose e del tumore a piccole cellule . 
carcinoma del polmone con diffusione subpleurica . questo pattern di crescita caratteristico delladenocarcinoma . lo scopo di questa presentazione descrivere le componenti tissutali intratumorali presenti nei tumori polmonari solidi che risultino evidenti allanalisi macroscopica e / o microscopica del campione autoptico oppure chirurgico , e che siano anche identificabili allindagine tc diretta ed eseguita dopo la somministrazione di mezzo di contrasto . questo al fine di descrivere alcuni patterns caratteristici delle lesioni polmonari maligne che ne facilitino la caratterizzazione alla tc sulla base della valutazione morfologica della lesione . 
 radiol med ( 2009 ) 114 : 173189 solid component this tissue component consists of the simultaneous presence , though in varying proportions , of tumour cells and fibrovascular stroma . 
the solid component may have exclusive endobronchial growth , infiltrating growth within the bronchial wall and the mediastinal structures and peribronchial growth with progressive invasion or compression of the adjacent parenchyma , or again it may cause bronchial obstruction with atelectasis and postobstructive pneumonia . the peribronchial solid component may also manifest as multiple nodules in the lung parenchyma . 
bronchial solid component with invasion of adjacent structures ( bronchial wall and mediastinum ) : lung malignancies presenting with this type of solid component produce focal stenosis or complete occlusion of the affected bronchus . 
this pattern represents the evolution of early endobronchial solid lesions with subsequent invasion of the adjacent lung parenchyma or mediastinum . 3 peribronchial solid component : lung cancers with this type of solid component have solid density and welldefined margins or show infiltration or compression of the adjacent lung parenchyma . 
la componente solida pu presentare una crescita esclusivamente endobronchiale , una crescita infiltrante nei confronti della parete bronchiale e delle strutture mediastiniche , una crescita peribronchiale con progressiva infiltrazione ovvero compressione del parenchima polmonare adiacente , ovvero ancora pu causare ostruzione bronchiale con atelettasia e polmonite post - ostruttiva . 
 haemorrhagic component this intratumoural component may be observed at the level of the central or peripheral region of the solid component in squamous cell carcinomas in undifferentiated large cell carcinomas and in small cell tumours . 
at nonenhanced ct , this radiol med ( 2009 ) 114 : 173189 sostanzialmente , questo pattern rappresenta levoluzione di lesioni tumorali precoci endobronchiali con invasione successiva del parenchima polmonare adiacente oppure del mediastino . 
 componente emorragica questa componente intratumorale pu essere osservata a livello della regione centrale oppure periferica della componente solida nel carcinoma a cellule squamose , nel carcinoma indifferenziato a grandi cellule , e nel tumore a piccole cellule . 
the cut surface of the surgical specimen shows a bronchial lesion ( long arrow ) partially obstructing the lower bronchial lumen and infiltrating the adjacent lung parenchyma ( short arrow ) ( c )  . 
c la superficie di sezione del campione chirurgico del medesimo tumore dimostra un tumore bronchiale ( freccia lunga ) che ostruisce parzialmente il lume del bronco inferiore ed infiltra il parenchima polmonare adiacente ( freccia corta )  . 
lanalisi microscopica rivela il tipico aspetto istologico del carcinoma a cellule squamose con evidenza di ponti intercellulari , abbondante produzione di cheratina da parte delle single cellule con intensa eosinofilia delle singole cellule , e formazione di perle di cheratina . 
frequentemente , questa componente necrotica non chiaramente identificabile allanalisi delle immagini tc dato che risulta commista alla componente solida , nel qual caso determina radiol med ( 2009 ) 114 : 173189 fig . 
lanalisi microscopica rivela il tipico aspetto istologico del carcinoma a cellule squamose con evidenza di ponti intercellulari , abbondante produzione di cheratina da parte delle single cellule con intensa eosinofilia delle singole cellule , e formazione di perle di cheratina . 
the tumour appears heterogeneous , with an intratumoural area of low density that does not enhance after contrast material administration , whereas the solid viable peripheral component shows evident enhancement . 
the section surface of the specimen shows a mass with well - defined lobulated margins , with a brownish central component ( arrow ) that corresponds to the area of intratumoural low density identified at ct and reflecting central coagulation necrosis within the neoplasm ( c )  . 
b la superficie di sezione del campione macroscopico dimostra una massa a margini distinti e lobulati con una componente centrale brunastra ( freccia ) che corrisponde alla regione intratumorale ipodensa identificata alla tc e che riflette la necrosi centrale a carattere coagulativo nel contesto della neoplasia . 
questo pattern tipicamente osservato nel mesotelioma pleurico con coinvolgimento del parenchima polmonare e nelladenocarcinoma periferico con infiltrazione pleurica . parenchymal consolidation this component manifests as a process with massive lobar spread or parenchymal consolidation at gross pathology and exhibits air bronchogram at ct . 
 diffuse peripheral component on gross pathology , this solid component shows a subpleural growth pattern , and it partially or completely involves the peripheral lung region and the visceral and / or parietal pleura , with frequent simultaneous involvement of the lung fissures . 
this pattern is typically observed in pleural mesothelioma with parenchymal involvement and in peripheral adenocarcinoma with pleural infiltration . nente si presenta nella forma di noduli periferici , singoli oppure multipli , a volte coalescenti , oppure si pu manifestare come lesione localizzata a livello dellapice polmonare . 
on gross pathology , this component presents in the form of peripheral single or multiple at times coalescing nodules or as a lesion located at the level of the lung apices . 
extensive parenchymal consolidation at the level of the right lung . contrast - enhanced computed tomography ( b , c ) ( b mediastinal window ; c lung window )  . diffuse parenchymal consolidation involving the upper lobe of the right lung is visualised ( arrow )  . 
 discussion benign lung lesions must be differentiated from lung malignancies , in which infiltration of the adjacent parenchyma , invasion of mediastinal structures or bronchial obstruction are typically present [ 47 ]  . 
anche se lindagine tc standard ( non - dinamica ) eseguita con metodica diretta e con mezzo di contrasto non fornisce ovviamente la medesima risoluzione spaziale della microscopia ottica , alcune distinte componenti tissutali intratumorali possono essere riconosciute mediante una attenta analisi morfologica delle lesioni polmonari . 
in questa presentazione abbiamo descritto le componenti tissutali intratumorali presenti nei tumori polmonari solidi che risultano evidenti alla valutazione macroscopica e / o microscopica dei campioni patologici autoptici oppure chirurgici , e che risultano anche evidenti alla valutazione delle immagini tc dirette e con mezzo di contrasto ottenute 186 radiol med ( 2009 ) 114 : 173189 fig . 
d la microscopia ad alto ingrandimento ( 200 ; colorazione con ematossilina - eosina ) dimostra un adenocarcinoma ben differenziato con estesa reazione desmoplastica periferica e fibrosi ( frecce )  . 
 of contrast material clearly do not provide the same spatial resolution as optical microscopy , some distinct intratumoural tissue components may be recognised by a careful morphological analysis of the lung lesions . 
in this paper , we described the intratumoural tissue components seen in solid lung tumours at gross pathology and / or microscopic analysis of autopsic or surgical specimens , which are also appreciable on examination of nonenhanced and contrastenhanced ct images obtained with the standard nondynamic technique . the solid component related to the presence of proliferating neoplastic cells is common to all lung cancers . 
in particular , squamous cell carcinomas and small cell lung secondo la tecnica standard ( non - dinamica )  . la componente solida determinata dalla presenza di cellule neoplastiche in proliferazione comune a tutte le neoplasie polmonari maligne . 
in particolare , il carcinoma a cellule squamose ed il tumore polmonare a piccole cellule si manifestano tipicamente come lesioni centrali a livello del bronco principale , del bronco lobare , ovvero a livello dei bronchi segmentari in circa i due terzi dei casi e si possono quindi manifestare come masse polmonari ilari con invasione delle strutture mediastiniche adiacenti , oppure anche come lesioni bronchiali ostruttive con conseguente atelettasia ovvero polmonite post - ostruttiva . 
c la superficie di sezione del campione autoptico dimostra una lesione biancastra disomogenea ( frecce ) che rivela una prevalente componente fibrotica alla istologia ( d ) e caratteristiche tipiche della reazione tubercolare granulomatosa ( freccia )  . 
on gross pathology , these endobronchial tumours range from an irregular focal growth in the bronchial mucosa to a polypoid endobronchial mass with diffuse wall infiltration leading to stenosis and / or bronchial occlusion . 
circa un terzo dei carcinomi a cellule squamose presentano una localizzazione periferica a causa della prevalente crescita peribronchiale e si manifestano come noduli polmonari solitari periferici ( 3 cm in diametro ) ovvero come voluminose masse polmonari [ 5 ]  . 
 la componente emorragica e coagulativa pu essere riscontrata in tutti gli istotipi maligni mentre la componente necrotica colliquativa si riscontra tipicamente nel carcinoma a cellule squamose e nel carcinoma bronchioloalveolare [ 13 ]  . 
squamous cell carcinomas constitute the histological type that most commonly produces cavitation , owing to the presence of liquefactive central necrosis in approximately 10% of cases , leaving a cavity with a clear airfluid level with thick , irregular walls [ 5 , 6 ]  . 
the cystic or cavitated pattern , rarely seen in adenocarcinomas [ 11 , 12 ] , may be found in bronchioloalveolar carcinomas [ 13 , 14 ] , and it is generally suggestive of liquefactive intratumoural necrosis . intratumoural areas of coagulation or liquefactive necrosis are frequently observed in undifferentiated large cell lung carcinomas because of the large size of these tumours . 
they cause central hypoxia of the mass and appear as areas of brownish discolouration on examination of the cut surface of the specimen . parenchymal consolidation may be considered a solid tumoural component with diffuse alveolar involvement , similar to a pulmonary infection , and it is typically observed in bronchioloalveolar carcinoma . 
the diffuse peripheral component , which is found both in pleural mesothelioma and in lung adenocarcinoma , is related to the tumoural growth that involves the lung parenchyma starting from the pleural region , or to the neoplastic peribronchial growth with subsequent pleural infiltration . 
the fibrotic component is observed both in lung cancers , in particular adenocarcinomas , and in chronic lung infections . in fact , many benign lesions may mimic malignancies , and the most common of these are solid fibrotic areas , chronic pseudotumoural inflammatory processes [ 15 ] and tubercular lesions [ 16 ]  . 
in particular , active postprimary pulmonary tuberculosis may appear as a cavitation or bronchial wall thickening or in the form of miliary nodules , whereas chronic tuberculosis may appear in the form of calcified nodules , parenchymal consolidation or a spiculated peripheral lung mass [ 1517 ]  . conclusions several intratumoural tissue components may be identified in solid lung tumours , both on gross pathology and / or microscopic analysis of the specimen and on standard ct . 
the necrotic and haemorrhagic components are typically observed in malignant lung lesions , whereas the solid and fibrotic components may be observed in both malignant and benign solid lung lesions . listotipo che pi comunemente produce cavitazione per la presenza di necrosi centrale a carattere colliquativo in circa il 10% dei casi , residuando una cavit con netto livello idroaereo con pareti spesse ed irregolari [ 5 , 6 ]  . laspetto cistico ovvero cavitato , di raro riscontro nelladenocarcinoma [ 11 , 12 ] , pu invece essere riscontrato nel carcinoma bronchioloalveolare [ 13 , 14 ] ed generalmente suggestivo per necrosi intratumorale di tipo colliquativo . 
le aree intratumorali di necrosi coagulativa ovvero colliquativa sono frequentemente osservate nei carcinomi polmonari indifferenziati a grandi cellule a causa delle grandi dimensioni raggiunte spesso dal tumore con conseguente ipossia centrale della massa , ed appaiono come aree di discolorazione brunastra alla valutazione della superficie della sezione del reperto patologico . laddensamento parenchimale pu essere considerato come una componente tumorale solida con diffuso coinvolgimento alveolare , simile ad una infezione polmonare , e viene tipicamente riscontrato nel carcinoma bronchioloalveolare . la componente diffusa periferica , che viene osservata sia nel mesotelioma pleurico come anche nelladenocarcinoma polmonare , determinata dalla crescita tumorale che coinvolge il parenchima polmonare a partire dalla regione pleurica , oppure dalla crescita neoplastica peribronchiale con successiva infiltrazione della pleura . 
di fatto molte lesioni polmonari di tipo benigno possono mimare le neoplasie maligne , e tra queste le pi comuni sono le aree solide da esiti a carattere fibrotico , i processi infiammatori di tipo cronico a carattere pseudotumorale [ 15 ] e le lesioni tubercolari [ 16 ]  . 
in particolare , la tubercolosi polmonare attiva post - primaria si pu manifestare come cavitazione oppure come ispessimento della parete bronchiale ovvero anche come noduli miliari , mentre il processo tubercolare cronico pu manifestarsi come noduli calcifici ovvero anche come addensamento parenchimale oppure ancora come massa polmonare periferica a margini spiculati [ 1517 ]  . 
le componenti a carattere necrotico ed emorragico sono osservate tipicamente nelle neoplasie polmonari maligne , mentre le componenti solide ed a carattere fibrotico possono essere osservate nelle lesioni polmonari solide sia a carattere maligno che benigno . 
thirty - two chest radiographs and 32 chest us examinations were performed in 28 consecutive patients ( aged 4 months to 17 years ) with a clinical suspicion of pneumonia . 
chest us examinations were carried out with a convex - array broadband probe ( 25 mhz ) and a high - frequency linear - array broadband probe ( 512 mhz )  . 
for this reason , chest us may be a valuable aid and possible alternative to standard chest radiography in the evaluation and follow - up of children with suspected pneumonia . keywords thoracic sonography lung consolidation pleural effusion pneumonia riassunto obiettivo . 
in 28 pazienti consecutivi , con esame obiettivo sospetto per polmonite ( di et tra 4 mesi e 17 anni ) sono stati eseguiti , considerando sia gli esami allesordio che i controlli , 32 radiogrammi del torace ed altrettante ecografie della parete toracica . 
lecografia permette di identificare gli addensamenti parenchimali polmonari , qualora siano situati in sede subpleurica , quantomeno con la stessa sensibilit dellrx e come noto valuta molto bene il versamento pleurico . 
pertanto lecografia si pone come un valido supporto ed eventuale alternativa agli esami radiologici tradizionali nel monitoraggio dei pazienti pediatrici . parole chiave ecografia toracica addensamenti polmonari versamento pleurico polmonite 322 introduction chest radiography is considered the reference examination in the diagnosis of pneumonia in children , whereas chest ultrasound ( us ) is not typically used for this purpose [ 1 ]  . chest radiography presents , however , some important disadvantages , including exposure to ionising radiation and a high degree of interand intraobserver variability , not only in typical parenchymal consolidation but especially in consolidations affecting areas that are difficult to explore with radiography , such as retrocardiac locations or the lung bases [ 2 ]  . 
given the smaller volume of lung parenchyma in children , it is likely that the pleura becomes involved more rapidly and to a greater extent than in adults and that chest us may provide results at least comparable with those obtained in adults . 
in many cases , chest us may provide equally useful clinical information and be used as an alternative to standard chest radiography . the aim of this study was to evaluate the sensitivity of chest us compared with chest radiography in identifying parenchymal consolidation and pleural effusion in children with suspected pneumonia . the normal lung is poorly accessible to the us beam because the great difference in impedance between the pleura and the alveolar air causes us waves to be completely reflected . 
sometimes , when the bronchioles are traversed by the us beam , the air bronchogram may also appear as hyperechoic rounded images produced by the air trapped within the bronchial structures [ 5 , 6 ]  . 
us may also identify fluid bronchograms , which correspond to fluid - filled bronchial structures ( typically mucus and / or inflammatory exudate ) that assume a tubular , binary appearradiol med ( 2009 ) 114 : 321330 introduzione la radiografia del torace viene attualmente considerato lesame di riferimento per la diagnosi di polmonite nellet pediatrica , mentre lecografia della parete toracica , da alcuni definita anche ecografia polmonare , non risulta fra le diagnostiche per immagini utilizzate a tal fine [ 1 ]  . 
innanzitutto lesposizione alle radiazioni ionizzanti , secondariamente la variabilit dellinterpretazione intered intra - osservatore , non tanto in un classico quadro di consolidamento polmonare , quanto soprattutto in presenza di addensamenti polmonari in sedi mal esplorabili col radiogramma , ad esempio retrocardiaca o a livello delle basi [ 2 ]  . 
 ragionevole ipotizzare che nei bambini la polmonite possa estendersi alla pleura pi rapidamente ed in percentuali maggiori , in relazione al minor volume del parenchima polmonare , e quindi che con lecografia polmonare si possano ottenere risultati perlomeno sovrapponibili a quelli degli adulti . 
nei pazienti pediatrici , spesso affetti da flogosi delle vie respiratorie , a volte anche ripetutamente nel giro di pochi mesi , nei casi in cui non si sia un netto miglioramento allesame obiettivo nonostante la terapia ci si trova davanti alla necessit di eseguire un monitoraggio nel tempo con radiogramma del torace [ 1 ]  . 
scopo di questo lavoro valutare la sensibilit dellecografia della parete toracica , rispetto al radiogramma del torace nei pazienti pediatrici con sospetta polmonite , nellidentificazione degli addensamenti polmonari e del versamento pleurico . il polmone normale non raggiungibile , quindi non esplorabile con gli ultrasuoni , poich lelevata differenza dimpedenza acustica nel passaggio tra la pleura e laria contenuta allinterno degli alveoli polmonari determina una riflessione completa degli ultrasuoni . 
essi tuttavia possiedono ancora molta energia , per cui vengono riflessi pi volte tra la superficie impedente ed il trasduttore , generando artefatti costituiti da multipli echi trasversali , che vengono rappresentati sul monitor ad intervalli equidistanti tra loro e profondit via via crescenti ; essi sono definiti riverberi . quando invece gli alveoli in prossimit della pleura contengono materiale liquido , semiliquido o solido ( nel nostro caso essudato flogistico ) , gli ultrasuoni possono oltrepassare la pleura e raggiungere la zona di parenchima polmonare addensato [ 4 ]  . 
lecostruttura degli addensamenti spesso disomogenea in quanto possono coesistere zone con diversa radiol med ( 2009 ) 114 : 321330 ance , with hypoor anechoic fluid content and no doppler flow signals [ 7 ]  . 
anechoic tubular structures may also be seen that correspond to the vessels and are easily distinguished from a fluid bronchogram in that they show colour signals on colour doppler us [ 8 ]  . materials and methods between october 2006 and july 2007 , we performed a total of 32 chest us examinations and 32 chest radiographs ( including diagnostic and follow - up examinations ) on 28 consecutive children ( 17 boys , 11 girls ; mean age 4.5 years ; age range 4 months to 17 years ) admitted to the paediatric emergency ward for respiratory symptoms and a clinical suspicion of pulmonary disease . 
 before the us examination , the childrens parents or guardians were informed about the limitations inherent in the small series reported in the literature and thus the need for further investigation by chest radiography , even if the us examination provided an apparently diagnostic result . the parents and guardians were also informed that the data would be stored and used in accordance with the law in force , and their informed consent was obtained . patients were divided into three age groups : 024 months , 24 years and 4 years or older . 
patients from 0 to 24 months of age underwent ventrodorsal chest radiography in the supine position , 2to 4 - year - olds underwent only posteroanterior radiography in the standing position and patients aged 4 years or older underwent posteroanterior and laterolateral radiography in the standing position . 
pleural effusion was systematically looked for at the level of the anterior , lateral and posterior costophrenic angles . where pleural effusion was detected on us but not on chest radiography , the patient underwent serial us monitoring until complete reabsorption of the effusion . 
questo visibile come stria ecogena e riverberante , reperto simile ai rami biliari epatici in caso di aerobilia , e sarebbe presente in circa l80%90% dei casi di addensamenti polmonari secondo i dati presenti in letteratura . talvolta , quando i bronchioli vengono attraversati dagli ultrasuoni determinandone una sezione assiale , il broncogramma aereo pu apparire anche come immagini rotondeggianti iperecogene generate appunto dallaria intrappolata nelle strutture bronchiali [ 5 , 6 ] con lecografia si possono identificare anche i broncogrammi fluidi , cio strutture bronchiali a contenuto liquido ( generalmente muco e / o essudato flogistico ) che quindi assumono morfologia tubulare , a binario , con contenuto liquido ipo o anecogeno , prive di flusso al campionamento doppler [ 7 ]  . 
 materiali e metodi in un periodo di 9 mesi ( ottobre 2006luglio 2007 ) , considerando sia gli esami allesordio che i controlli seriati , sono state eseguite 32 ecografie della parete toracica ed altrettanti radiogrammi del torace in un totale di 28 pazienti consecutivi ( 17 maschi , 11 femmine ) afferiti al pronto soccorso pediatrico per sintomatologia respiratoria . tutti avevano un esame obiettivo sospetto per coinvolgimento polmonare , cio presenza di rantoli , ridotto murmure vescicolare , tachipnea , dispnea e / o tosse febbre > 37 , 5c . let media stata di 4 , 5 anni con un intervallo compreso tra 4 mesi e 17 anni . 
 i tutori legali dei pazienti , prima che questi ultimi fossero sottoposti allecografia , sono stati informati sui limiti derivanti dalle esigue casistiche a disposizione e pertanto della necessit di eseguire ulteriori approfondimenti ( in particolare il radiogramma del torace ) anche qualora lesame fosse apparentemente risultato diagnostico . 
ai tutori legali dei pazienti stato reso noto che i dati sarebbero stati conservati ed utilizzati in ottemperanza alle leggi ed alle norme vigenti ed stato ottenuto il loro consenso informato . 
ai pazienti nella fascia det 024 mesi stato eseguito il radiogramma del torace in proiezione ventro - dorsale in posizione supina , nella fascia 24 anni solo in proiezione postero - anteriore in stazione eretta ; infine nella fascia det superiore ai 4 anni sono strate eseguite le due proiezioni ortogonali postero - anteriore e latero - laterale in stazione eretta . 
si preso come standard di riferimento il solo radiogramma del torace . i pazienti sono stati sottoposti ad ecografia della parete 324 radiol med ( 2009 ) 114 : 321330 pendent radiologists who were blinded to each others findings . 
the data obtained were processed to calculate sensitivity , specificity and positive and negative predictive values of chest us in the identification of lung consolidation and pleural effusion . results the radiographic and us examinations were successfully performed in all patients . 
chest us depicted 22 cases of subpleural consolidation , none of which extending exclusively to the perihilar area ; pleural effusion was identified in 15 cases and air bronchogram in eight cases . 
the results are summarised in table 1 . among the examinations positive for consolidation , air bronchogram was seen on chest radiography in 29.1% ( 7 / 24 ) of cases and on us in 36.3% ( 8 / 22 ) of cases . 
pleural effusion was detected in 33.3% ( 8 / 24 ) of the cases that were positive for consolidation on chest radiography and in 68.1% ( 15 / 22 ) of those positive for consolidation on us . 
in our series , chest us compared with chest radiography had 91.67% sensitivity and 100% specificity for lung consolidation ; its negative predictive value was 84.6% and positive predictive value 100% . 
sono state eseguite scansioni longitudinali ed assiali ( intercostali ) lungo quelle che sono i tradizionali punti di repere : la linea emiclaveare , parasternale , ascellare in modo da coprire tutta la gabbia toracica . 
stato sistematicamente ricercato versamento pleurico a livello dei seni costofrenici anteriori , laterali e posteriori . nei casi di versamento pleurico con riscontro solo ecografico senza corrispettivo al radiogramma del torace si optato per un monitoraggio ecografico seriato nel tempo fino al completo riassorbimento dello stesso . 
con i dati ottenuti sono stati calcolati i valori di sensibilit , specificit , valore predittivo positivo e negativo dellecografia toracica nellidentificazione degli addensamenti polmonari e del versamento pleurico . risultati in tutti i pazienti stato possibile eseguire esami radiografici ed ecografici diagnostici . 
lecografia ha riscontrato in 22 casi addensamenti subpleurici , nessuno che si estendesse esclusivamente in sede perilare , in 15 casi stato segnalato il versamento pleurico ed in 8 casi il broncogramma . 
i dati sono riassunti anche nella tabella 1 . il broncogramma aereo , in rapporto ai soli esami positivi per addensamento , al radiogramma del torace stato riscontrato nel 29 , 1% ( 7 / 24 ) dei casi , mentre in ecografia nel 36 , 3% ( 8 / 22 ) dei casi . 
il versamento pleurico stato riscontrato nel 33 , 3% ( 8 / 24 ) dei casi nei quali i radiogrammi del torace avessero riscontrato un addensamento e nel 68 , 1% ( 15 / 22 ) delle ecografie positive per addensamento . 
nella nostra casistica lecografia della parete toracica , quando confrontata con il radiogramma del torace , ha riportato una sensibilit del 91 , 67% nellindividuare gli radiol med ( 2009 ) 114 : 321330 the statistical analysis because of the lack of a reference standard better than chest radiography . 
however , modalities employing ionising radiation must be used very sparingly in children for two reasons : their higher tissue sensitivity to ionising radiation ( as tissues are rich in proliferating cells ) , and their longer life expectancy , during which radiation - induced damage may emerge [ 9 ]  . 
once the clinical need for the examination has been ascertained , appropriate measures and technical parameters ( depending on the patients weight and / or age ) should always be implemented to achieve a significant reduction of exposure [ 11 ] while providing sufficient diagnostic quality ( following the principle of keeping radiation doses as low as reasonably achievable alara )  . 
the aim , it should be remembered , is not to produce a beautiful radiological image but to obtain an image allowing a diagnosis [ 9 , 12 ]  . 
chest radiography is thus only indicated in a restricted number of patients admitted to hospital for suspected pneumonia , that is , those who present severe symptoms and signs of pneumonia [ 1 ]  . 
in a small minority of patients with a suspicion of severe complications , with worsening signs and symptoms , discrepancy between imaging and clinical findings or with particularly severe and extensive lesions on radiography , computed tomography may also be used . although us has long been used to identify pleural effusion , only recently [ 13 , 14 ] has the evaluation of lung parenchyma become possible , partly as a result of technological advances and multifrequency transducers ( which have improved the techniques spatial resolution ) [ 15 ]  . 
 however , in the case of perihilar consolidation not extending to the subpleura and thus inaccessible to us , sonography is unable to visualise the diseased parenchyma addensamenti polmonari ed una specificit del 100% . 
in tutti i casi in cui era stato segnalato il versamento pleurico questo stato identificato anche con lecografia ; in pi sono stati identificati ulteriori 7 pazienti in cui il versamento era visibile solo ecograficamente ; in questi casi si monitorato il paziente fino al completo riassorbimento del versamento , eseguendo quindi in totale ulteriori 11 ecografie , i cui dati per , mancando uno standard di riferimento migliore del radiogramma del torace , non sono stati utilizzati al fine della valutazione statistica . 
per quanto concerne i versamenti pleurici , con i limiti sopra esposti , lecografia ha dimostrato dei valori di sensibilit e specificit nellordine del 100% . discussione il radiogramma del torace viene classicamente considerato la metodica di primo livello nella valutazione degli addensamenti polmonari . 
tuttavia in et pediatrica lutilizzo di metodiche che utilizzino radiazioni ionizzanti deve essere molto oculato , per due ragioni : la maggiore sensibilit dei tessuti agli effetti delle radiazioni ionizzanti ( perch pi ricchi di cellule in proliferazione ) e la maggiore aspettativa di vita durante la quale possono manifestarsi i danni radioindotti [ 9 ]  . 
la pi importante misura per ridurre la dose di radiazioni erogata alla popolazione per scopi medici si attua in primo luogo eseguendo lindagine ( sia essa un radiogramma , piuttosto che un esame di tomografia computerizzata ) solamente quando questa sia realmente giustificata . 
una volta assodata la correttezza dellindicazione allesame radiologico bisogna ricordare che tale tipo di indagini vanno sempre eseguite utilizzando adeguati accorgimenti e parametri tecnici ( variabili in funzione del peso e / o dellet del paziente ) che consentano di limitare al massimo lesposizione alle radiazioni ionizzanti [ 11 ] , pur ottenendo unindagine di sufficiente qualit diagnostica ( secondo il criterio del mantenere la dose il pi possibile bassa per quanto ragionevolmente fattibile alara , as low as reasonably achievable )  . 
pertanto lesecuzione del radiogramma del torace indicato solamente in una limitata parte dei pazienti che giungono allosservazione medica per sospetta polmonite , cio in caso di polmoniti con un quadro clinico severo [ 1 ]  . 
in casi ancora pi selezionati in cui si sospettino gravi complicanze , vi sia un importante peggioramento della sintomatologia , reperti 326 fig 1a axial image ( left ) showing pulmonary consolidation ( arrows ) with tiny hyperechoic spots ( air bronchogram , arrowhead )  . 
longitudinal image ( right ) with hypoechoic pneumonic lesion ( arrows ) above the left hemidiaphragm ( d , diaphragm , c , costal arch ) and small anechoic pleural effusion . 
1a a sinistra scansione assiale che dimostra laddensamento ( frecce ) ed alcuni minuti spot iperecogeni ( broncogramma aereo , testa di freccia )  . a destra scansione longitudinale ( d , diaframma , c , costa ) con addensamento ipoecogeno ( frecce ) in sede basale sinistra con sottile falda di versamento pleurico anecogeno . 
b allrx torace tenue e sfumato addensamento basale sinistro in sede paracardiaca , con velatura del seno costofrenico omolaterale . directly because of the interposition of the aerated lung . another reason for the failure of us to detect disease may be lesions located in areas difficult to reach with us , such as the posterior apical regions that are covered by the scapulae and supraclavicular fossa , and the axillary region . 
in such cases , however , us may depict indirect signs of radiol med ( 2009 ) 114 : 321330 strumentali discordanti con la clinica , o quadri particolarmente gravi ed estesi al radiogramma , pu essere utilizzata la tomografia computerizzata . da tempo nota la possibilit di valutare ecograficamente il versamento pleurico , ma solo recentemente [ 13 , 14 ] , grazie anche allevoluzione tecnologica degli ecografi e delle sonde multifrequenza ( che consentono di avere maggiore risoluzione spaziale ) si pensato di utilizzare questa metodica anche per la valutazione del parenchima polmonare [ 15 ]  . 
un ulteriore motivo di mancato riconoscimento delle lesioni pu essere rappresentato da sedi difficilmente esplorabili con lecografia quali le apicali posteriori , coperte dalle scapole e dalla fossa sovraclaveare , nonch la regione ascellare . lecografia in questi casi potrebbe tuttavia rilevare dei segni indiretti di coinvolgimento parenchimale , per esempio un versamento pleurico che , in base ai dati presenti in letteratura pu coesistere nei pazienti con polmonite , a seconda dellet e delle casistiche tra il 20% ed il 61% dei casi [ 16 ]  . nella nostra casistica il versamento stato riscontrato nel 33 , 3% dei casi nei quali i radiogrammi del torace riscontrassero un addensamento e nel 68 , 1% delle ecografie positive per addensamento . 
questi pazienti , come gi anticipato nei risultati , sono stati comunque sottoposti a controllo ecografico fino al completo riassorbimento del versamento , eseguendo quindi ulteriori 11 ecografie toraciche ottenendo dati concordanti con la letteratura , la quale riporta la migliore sensibilit dellecografia nella valutazione del versamento pleurico rispetto al radiogramma [ 17 ]  . 
 un aspetto peculiare dellecografia inoltre quello di poter anche caratterizzare , entro certi limiti , il tipo di versamento , quanto meno facendoci orientare verso un versamento non organizzato , con aspetto anecogeno o , viceversa , organizzato nel caso sia ad ecostruttura disomogenea , corpuscolata , con presenza di setti iperecogeni nel cui caso pu rendersi necessaria lesecuzione di toracentesi [ 18 , 19 ]  . in un caso il monitoraggio seriato nel tempo mediante ecografia , dimostrando la graduale riduzione e riassorbimento spontaneo del versamento pleurico ha permesso di evitare una toracentesi per il posizionamento del drenaggio pleurico . 
viceversa in un ulteriore caso , bench il contenuto del versamento non apparisse ecograficamente corpuscolato , al momento del drenaggio pleurico ( eseguito per la mancata risoluzione del quadro clinico ) stato evacuato materiale di aspetto lattescente , francamente purulento . 
in questo caso quindi lecografia avrebbe potuto fuorviare , portando ad un atteggiamento pi attendista ; naturalmente per il quadro radiologico , cos come quello laboratoristico , sono solamente degli aspetti di cui bisogna tenere conto alla luce della clinica nella gestione globale del paziente . i vantaggi del radiogramma rispetto allecografia della parete toracica , a fronte di unesposizione a radiazioni ionizzanti , sono quelli di permettere una maggiore panoramicit , facilit di esecuzione e refertazione , oltre a permettere una misurazione oggettiva del diametro della lesione . lecografia tra i suoi limiti ha limpossibilit ad esplorare alcune zone ( ad esempio la superficie pleurica al di sotto della scapola ) , lelevata operatore - dipendenza e tra laltro anche quando ripetuta sulla stessa apparecchiatura dallo stesso operatore non sempre pu essere facile valutare la riduzione dimensionale di un addensamento , specie se questo si estende molto in profondit rispetto alla superficie pleurica . 
bisogna inoltre ricordare che dovendo esplorare ecograficamente due emitoraci su tutta la loro estensione superficiale ( anteriore , posteriore , laterale ) , questo esame richiede sicuramente una quantit di tempo maggiore rispetto alla lettura di un radiogramma del torace , pertanto non facilmente applicabile nel contesto di un servizio di radiologia durgenza . daltro canto lecografia , soprattutto una volta che sia stata individuata la zona patologica , davvero molto rapida nelleffettuare una valutazione mirata relativa alla presenza o meno di un addensamento e / o di un versamento di precefig . 
on the left , an unevenly hypoechoic pulmonary consolidation ( arrows ) near the chondrocostal cartilage ( c ) , with tiny hyperechoic spots corresponding to an air bronchogram ( arrowhead )  . 
a sinistra addensamento disomogeneamente ipoecogeno ( frecce ) in sede paracardiaca subito posteriormente alle cartilagini condrocostali ( c ) , con evidenza di alcuni spot iperecogeni , tipo broncogramma aereo ( testa di freccia )  . 
nellimmagine a destra posteriormente alle cartilagini condrocostali ( c ) presente un addensamento parenchimale ( freccia ) ; nel suo contesto immagine lineare iperecogena ( testa di freccia ) tipo broncogramma aereo . 
b al radiogramma si apprezza uno sfumato addensamento in sede parailare inferiore - paracardiaca destra in corrispondenza del lobo medio . parenchymal involvement , such as pleural effusion that has been reported to coexist with pneumonia in 20%61% of cases , depending on age and patient series [ 16 ]  . 
the greater number of cases of pleural effusion detected with us may be explained by the fact that , especially in children , us is able to clearly depict even small effusions at the costophrenic angles , thanks to the 328 radiol med ( 2009 ) 114 : 321330 high spatial resolution afforded by high - frequency probes . additionally , it is always able to depict the region of interest directly without the interposition of other structures . in the case of very compact consolidations , colour doppler us also plays an important role , as it allows one to visualise vessels within the lung parenchyma . 
we thus performed 11 chest us scans achieving results comparable with those in the literature , which reports that us is more sensitive than chest radiography in the evaluation of pleural effusion [ 17 ]  . another peculiarity of us is its ability to give some indication of the type of effusion by indicating whether it is an unorganised anechoic effusion or , conversely , an organised effusion with an inhomogeneous corpuscular echostructure and hyperechoic septations , which might require a thoracentesis [ 18 , 19 ]  . 
in one case , serial us monitoring demonstrated the gradual reduction and spontaneous reabsorption of the pleural effusion , thus allowing thoracentesis to be avoided by placing a pleural drainage catheter . 
in another case , instead , despite the noncorpuscular appearance of the effusion on us , the pleural drainage catheter ( performed for persisting clinical signs and symptoms ) yielded milky , clearly purulent material . 
in this case , us could have misled us into adopting a more expectant approach , even though patient management is clearly guided not only by the radiological findings but also by the laboratory data and overall clinical condition . the advantages of radiography over chest us , despite the exposure to ionising radiation , include a more panoramic view , easier performance and reporting and objective determination of lesion diameter . 
in addition , because the entire surface of the two hemithoraces ( anterior , posterior , lateral ) need to be explored , us takes longer compared with chest radiography and is therefore poorly suited to emergency radiology settings . on the other hand , once the diseased area has been identified , us provides a very rapid and targeted evaluation of the presence of a previously detected consolidation and / or effusion , allowing serial monitoring over time , even in response to clinical changes indicating improvement or fig 3a on the left , axial intercostal image of a inhomogeneous consolidation with prevalently hypoechoic texture ( arrows ) and air bronchogram ( arrowheads )  . 
b al radiogramma si conferma una sfumata opacit a carico del campo polmonare superiore - medio di destra che si estende fino alla pleura . dente riscontro , potendo fare pi monitoraggi seriati nel tempo , anche in relazione a momenti in cui ci siano delle variazioni della sintomatologia clinica e quindi si sospetti un miglioramento o , viceversa , un peggioramento del quadro . lecografia permette inoltre una precisa e rapida valutazione anche dellevoluzione del versamento pleurico [ 20 ]  . nel caso di pazienti molto piccoli talvolta pu esser pi semplice eseguire lecografia , in cui si possono assecondare piccoli movimenti del paziente , esplorabile anche mentre dorme . 
in very young patients , it may at times be easier to perform us , as small movements can be followed and the patient can be studied even while asleep . 
paradoxically , a crying infant does not represent a major problem as occurs with ct or chest radiography , as crying enables the optimal evaluation of diaphragmatic motion with good visibility of the costophrenic angles during deep breathing . there are some limitations to our study . 
first , it included a small number of patients , and it is likely that we would have obtained lower sensitivity values if we had analysed a larger patient series with more cases of perihilar consolidation not extending to the pleura . 
likewise , had we used a more sensitive reference standard than chest radiography , our results with chest us would no doubt have been less encouraging . conclusions in consideration of the good sensitivity and positive and negative predictive values in identifying both parenchymal consolidation and pleural effusion , chest us proved to be a promising technique for the detection and follow - up of lung infections and associated pleural effusion . 
patients could be spared further radiological examinations that expose them to ionising radiation and which do not provide additional relevant clinical information . chest us also provides information about the need for further procedures , such as thoracentesis . 
us may also be used to guide thoracentesis to reduce the risks associated with the procedure , thereby decreasing morbidity and recovery time [ 19 ]  . the ease , speed and availability of us could also allow a higher frequency of follow - up examinations during treatment and an earlier detection of disease exacerbations , for example due to drug resistance . 
this would be beneficial in terms of both a more rational use of economic resources and a more appropriate management of the patient . del torace , in quanto ci permette di avere anche unottima valutazione dellescursione diaframmatica con una buona visibilit dei seni costofrenici durante i profondi respiri . il nostro studio presenta alcuni limiti . 
in primo luogo la bassa numerosit , per cui analizzando casistiche pi ampie , in cui siano compresi pi pazienti con addensamenti periilari senza estensione alla pleura , sarebbe plausibile ottenere valori di sensibilit peggiore . 
cova1 1unit clinica operativa di radiologia , ospedale di cattinara , universit degli studi , strada di fiume 447 , 34149 trieste , italy 2dipartimento di economia aziendale , universit degli studi , trieste , italy 3struttura complessa di cardiologia , ospedale di cattinara , trieste , italy correspondence to : f . 
sono stati calcolati i costi differenziali ( costo apparecchiature , costi variabili , costo del personale medico , tecnico e infermieristico ) , i costi comuni e i costi esterni . 
la coronaro - tc ha fatto registrare : costo differenziale 222 , 23 , costo comune 5 , 50 , costo esterno 2 , 30 , costo totale 230 , 03 . 
per la coronarografia si verificato : costo differenziale 366 , 18 , costo comune 0 , 50 , costo esterno 9 , 20 , costo degenza 1652 , costo totale 2027 , 88 . 
la coronaro - tc ha costi notevolmente inferiori alla coronarografia e un rapporto costo - efficacia migliore nella larga maggioranza dei pazienti . 240 radiol med ( 2009 ) 114 : 239252 keywords cost analysis multidetector computed tomography ct coronary angiography coronary angiography cost - effectiveness parole chiave analisi dei costi tomografia computerizzata multistrato coronaro - tc coronarografia costo efficacia coronaro - tc introduction introduzione coronary angiography with computed tomography ( ctca ) is rapidly establishing itself as an accurate technique for studying coronary arteries . 
in segmental analysis , the literature reports 72%95% sensitivity and 86%98% specificity for 16 - slice ct [ 1 , 2 ] and 95%99% sensitivity and 95%97% specificity , with a negative predictive value ( npv ) of 99%100% for 64 - slice ct [ 35 ]  . 
 the main strength of the technique lies in its high npv , which makes it a valuable diagnostic alternative for the noninvasive evaluation of the coronary circulation , allowing screening of patients with equivocal symptoms for significant coronary artery disease ( cad )  . 
the costs of ctca in particular have received sparse attention in the literature . the objective of our study was to analyse the costs of ctca performed at a department of radiology and compare them with those of conventional coronary angiography performed at the department of cardiology of the same hospital . 
a further aim was to compare the cost - effectiveness of the two modalities . materials and methods examination technique ctca la coronaro - tc si sta rapidamente imponendo come indagine accurata nella valutazione delle arterie coronarie . 
in letteratura , nellanalisi per segmento , vengono riportati valori di sensibilit tra il 72% e il 95% e di specificit del 86%98% mediante tc a 16 strati [ 1 , 2 ] , mentre gli studi relativi alla tecnologia a 64 strati riportano sensibilit pari al 95%99% e specificit pari al 95%97% , con un valore predittivo negativo del 99%100% [ 35 ]  . 
 il suo elevato valore predittivo negativo ne fa il reale punto di forza , proponendola come valido ed alternativo strumento diagnostico per la valutazione del circolo coronarico in modo non invasivo , al fine di gestire una porzione della popolazione con un corteo sintomatologico dubbio , in modo da evitare unindagine invasiva , e allo stesso tempo escludendo la presenza di una patologia ateromasica significativa . 
ulteriore obiettivo quello di confrontare ulteriormente le due metodiche con unanalisi di costo - efficacia . materiali e metodi tecnica desame coronaro - tc the ct scan was performed with an aquilion 64 multislice scanner ( toshiba medical systems , tokyo , japan ) with the following scanning parameters : slice thickness 640.5 mm , variable pitch and rotation time determined by the cardiac software on the basis of heart rate and adjusted to obtain maximum temporal resolution , 120 kv and variable ma . 
in particular , tube current was tailored to each patients weight and ranged from 300 ma ( for patients < 60 kg ) to 450 ma ( for those > 100 kg )  . ct scans were performed during the infusion of iomeprol , ( iomeron , a high - iodine - concentration contrast agent bracco , milan , 400 mgi / ml )  . 
a dose of 80 ml of contrast medium was la scansione tc stata eseguita con apparecchiatura multistrato aquilion 64 ( toshiba medical systems , tokyo ) con i seguenti parametri di scansione : spessore di strato 640 , 5 mm , pitch e tempo di rotazione variabili stabiliti dal software cardiologico dedicato in base alla frequenza cardiaca e regolati per ottenere la massima risoluzione temporale possibile , 120 kv e ma variabili . 
in particolare , la corrente del tubo radiogeno stata personalizzata in radiol med ( 2009 ) 114 : 239252 injected at a flow rate of 4 ml / s followed by a 40 - ml bolus of saline at the same flow rate . 
the contrast medium was injected through an 18 - gauge needle cannula placed in an antecubital vein of the right ara stellant dual - head automatic power injector ( medrad , indianola , ia , usa ) was used . 
the scan was synchronised with the contrast bolus by using the systems sure start triggering protocol , which involves placing a region of interest ( roi ) in the descending aorta and setting the enhancement threshold at 100 hu above baseline . the electrocardiographic trace was recorded throughout the scan for the retrospective reconstruction of isocardiophasic images . 
images were reconstructed by retrospective gating and unisegmental ( where possible ) or multisegmental technique , with initial placement of the temporal window in the end - diastolic phase at 75% of the r - r interval . 
where the end - diastolic phase proved inadequate , the dedicated software imagexact was used to identify the correct phase . axial images were processed on a dedicated workstation for 3d processing ( vitrea version 3.8.1 , vital images inc . minnetonka , mn , usa )  . 
reconstructions included 2d multiplanar reformations ( mpr ) , curved mpr ( cmpr ) along the course of the coronaries , maximum intensity projection ( mip ) and 3d volume rendering . 
whenever possible , we used vessel probe software to study the course of the coronaries and analyse any stenotic lesions in two orthogonal planes . conventional coronary angiography conventional coronary angiography was performed at the department of cardiology by selective catheterisation of the right and left coronary district . 
images were acquired with a dedicated c - arm innova 2100 ( general electric medical systems , chicago , il , usa ) and an additional ge innova 2000 c - arm equipped with high - definition flatpanel systems ( 1 , 0241 , 024 pixels12 bits )  . cost analysis we calculated the differential cost ( defined as the sum of the variable costs , equipment costs and personnel costs ) of the two procedures . 
we then calculated the common cost , which includes cost components that are the same for any type of procedure carried out at the departments of relazione al peso del paziente con un valore compreso fra 300 ma ( per pazienti di peso inferiore ai 60 kg ) e 450 ma ( per pazienti di peso superiore a 100 kg )  . lesame stato eseguito durante la somministrazione di iomeprolo , mezzo di contrasto ( mdc ) organoiodato ad alta concentrazione ( iomeron 400 mgi / ml )  . 
in pazienti portatori di bypass confezionati con arterie mammarie interne stato iniettato un volume di mdc di 100 ml a causa della maggior ampiezza del volume di acquisizione e quindi del maggior tempo di scansione . 
la scansione stata sincronizzata al bolo di contrasto mediante protocollo di triggering sure start fornito dalla apparecchiatura che prevede il posizionamento di una roi in aorta discendente ed un valore soglia regolato in 100 uh sopra il valore basale . durante la scansione stato acquisito il tracciato elettrocardiografico per la ricostruzione retrospettiva delle immagini isocardiofasiche . 
le immagini isocardiofasiche sono state ricostruite mediante gating retrospettivo e tecnica mono - segmentaria ( quando possibile ) o multisegmentaria con posizionamento iniziale della finestra temporale nella fase telediastolica al 75% dellintervallo rr . 
quando la qualit delle immagini lo ha reso possibile stato utilizzato il pacchetto software dedicato allo studio vascolare vessel probe per lo sviluppo del percorso coronarico e per lanalisi delle eventuali lesioni stenosanti effettuando lo studio del vaso su due piani ortogonali . coronarografia langiografia tradizionale stata eseguita presso la s.c. 
di cardiologia del nostro ospedale mediante cateterismo arterioso selettivo del distretto coronarico destro e sinistro . durante liniezione di iodixanolo ( visipaque 320 mgi / ml ) sono state ottenute serie di immagini ad elevato frame rate ( 15 immagini / s )  . 
solitamente vengono iniettati complessivamente 120140 ml di mdc per uno studio diagnostico . durante liniezione a bolo di mdc si acquisiscono le 242 radiol med ( 2009 ) 114 : 239252 radiology and cardiology . 
we then evaluated the variable costs , related to the type and amount of supplies used and the services connected to their use . physician , technologist and nursing personnel costs were also determined . 
examination duration was estimated on the basis of the time allocated by the hospitals computerised systein evaluating the differential costs , we only considered the technical act and consequently the costs incurred by the departments of radiology and cardiology , disregarding any relationship between these two departments and our hospitals other cost centres and the impact of the procedures on the patient - care process . every patient undergoing ctca and conventional coronary angiography requires a blood test to evaluate serum creatinine . 
patients undergoing coronary angiography are also screened for coagulation disorders [ platelets , international normalised ratio ( inr ) , thromboplastin time ]  . patients with prior allergic reactions to various substances approximately 1% require pharmacological preparation ( corticosteroids and anti - h1 and anti - h2 agents )  . 
although the costs for these procedures are not incurred by the department of radiology , they are considered , as they are essential for the performance of ctca and conventional coronary angiography and have a certain economic impact . 
 [ 9 , 10 ] to compare ctca and conventional coronary angiography . ctca cost = ne ( fe + rec ) + na ( fa + rac ) + nf ( rfc ) effectiveness = nex ( 1 - ndxe ) xpxsne + nexpxndxe . conventional coronary angiography cost = naxfa effectiveness = naxp test ; where ne = number of patients having na = number of patients having coronary angiography because of positive or nondiagnostic ctca = nex ( 1 - ndxe ) x [ pxsne + ( 1 - p ) x ( 1 - spe ) ] + nexndxe ; nf = number initial immagini in diverse proiezioni , usualmente quattro per la coronaria sinistra e due per la coronaria destra . 
sono stati poi valutati i costi variabili , relativi a tipologia e quantit dei materiali impiegati e ai servizi legati a tale impiego . successivamente sono stati valutati anche i costi del medico , del tecnico e del personale infermieristico . 
di cardiologia , ignorando i rapporti tra queste strutture e gli altri centri di costo dellazienda ospedaliero - universitaria e il ruolo che tali indagini hanno avuto sul processo di cura . va ricordato che ogni paziente che deve eseguire un esame di coronaro - tc e di coronarografia viene sottoposto a prelievo ematico per valutare i livelli sierici della creatinina . 
nell1% dei casi poi , essendoci unanamnesi positiva per allergia a diverse sostanze , si esegue anche una preparazione farmacologica ( basata sullimpiego di cortisonici associati ad anti - h1 ed anti - h2 )  . i costi legati a tali procedure non sono di pertinenza dellu.c.o. 
di radiologia ; tuttavia queste sono fondamentali ai fini dellesecuzione dellesame di coronaro - tc e della coronarografia ed avendo comunque un certo rilievo economico , verranno brevemente presi in considerazione . 
si ricorda ancora che i costi di materiali ed apparecchiature sono comprensivi di iva al 20% . stata inoltre effettuata unanalisi di costo - efficacia . radiol med ( 2009 ) 114 : 239252 of patients with false negative results who do not have coronary angiography = nex ( 1 - ndxe ) xpx ( 1 - sne ) ; fe = cost of ctca ; fa = cost of conventional coronary angiography ; re = rate of complications of ctca ; ra = rate of complications of coronary angiography ; rf = rate of complications over a 10year follow - up period in patients with cad and false negative tests ; c = mean cost of complications ; ndxe = number of nondiagnostic examinations at ctca ; sne = ctca sensitivity ; spe = ctca specificity ; p = pre - test likelihood the mathematical model adopted in our study evaluates a hypothetical cohort of patients with different pretest likelihoods who are studied with the two diagnostic tests . 
in particular , calculation of ctca costs included the rate and cost of complications as well as the equipment costs ; to this we added the cost of patients requiring coronary angiography ( because ctca is either nondiagnostic or positive for lesions eligible for percutaneous treatment ) and the cost of false negative patients who do not undergo coronary angiography . 
 [ 13 ] , who estimated an average overall cost for myocardial infarction of 11 , 742 ( hospitalisation , rehabilitation , nonproductive time ) , assuming this to be the most serious complication and considering the same cost for both procedures . 
by applying a complex mathematical model , this set of data can be used to compare the cost and cost - effectiveness of the two modalities based on the different pretest likelihoods . results ctca differential costs 1 . 
the lanalisi di costo - efficacia una forma di piena valutazione economica dove sia i costi che le conseguenze di un programma diagnostico o terapeutico vengono contemporaneamente esaminati [ 8 ]  . 
una riduzione dei costi con diagnosi corretta indica miglioramento del rapporto costo - efficacia . per la valutazione del rapporto costo - efficacia ci siamo basati sul modello decisionale sviluppato da patterson et al . 
 [ 9 , 10 ] per confrontare la coronaro - tc e la coronarografia . coronaro - tc costo = ne ( fe + rec ) + na ( fa + rac ) + nf ( rfc ) efficacia = ne ( 1nde ) psne + nepnde . coronarografia costo = nafa efficacia = nap ( ne = numero di pazienti con test iniziale ; na = numero di pazienti che eseguono la coronarografia perch la coronaro - tc positiva o non diagnostica = ne ( 1nde ) [ psne + ( 1 - p ) ( 1 - spe ) ] + nende ; nf = numero di pazienti falsi negativi che non eseguono coronarografia = ne ( 1nde ) p ( 1sne ) ; fe = costo coronaro - tc ; fa = costo coronarografia ; re = percentuale complicanze coronaro - tc ; ra = percentuale complicanze coronarografia ; rf = percentuale complicanze in un periodo di 10 anni di follow - up nei pazienti con cad e test falsi negativi ; c = costo medio complicanze ; nde = numero di esami non diagnostici alla coronaro - tc ; sne = sensibilit coronaro - tc ; spe = specificit coronaro - tc ; p = probabilit pre - test ) nel modello matematico che abbiamo adottato viene valutata una coorte ipotetica di pazienti con diverse probabilit pre - test che vengono sottoposti alle due indagini diagnostiche . 
in particolare , nel computo del costo della coronaro - tc si considera oltre al costo dellapparecchiatura , la percentuale delle complicanze e il loro costo ; a ci va sommato il costo dei pazienti che devono eseguire la coronarografia ( perch la coronaro - tc risulta positiva per lesioni da sottoporre a trattamento percutaneo o non diagnostica ) e il costo dei falsi negativi che non eseguono la coronarografia . 
nel 2006 , che dimostrano valori di sensibilit del 98 , 4% , di specificit del 90 , 7% ed una quota di esami non diagnostici del 3 , 6% . 
la coronarografia , che rappre244 radiol med ( 2009 ) 114 : 239252 maintenance and service costs were 91 , 800 annually . to this we added the cost of an electrocardiographic monitor ( hme lifepulse 10 tg ) compatible with the toshiba mdct scanner , which has a purchase price of 3 , 500 ( equal to 437 annually )  . 
the picture archiving and communication system ( pacs ) had a purchase price of 2 , 500 , 000 , corresponding to 312 , 500 yearly for 8 years of amortisation . 
additional materials include an 18 - gauge abbocath needle cannula ( 0.44 ) , a small amount of disinfectant , cotton wool and an adhesive plaster ( the cost of these is negligible )  . 
ctca protocols recommend the oral administration of 100 mg of - blocker ( metoprolol ) at least 1 h before the examination in subjects with a heart rate > 65 beats per minute . 
la quota di complicanze , ricavata dalla letteratura , risulta del 0 , 004% per la coronaro - tc e del 1 , 5% per la coronarografia [ 11 , 12 ]  . 
 [ 13 ] , che stima in circa 11742 il costo medio di un infarto miocardico ( ospedalizzazione , riabilitazione , non produttivit ) , valutando questa come la complicanza pi grave e considerando di utilizzare tale valore per entrambe le metodiche . 
dallinsieme di questi dati , attraverso un complesso modello matematico , si ottiene prima una comparazione dei costi e successivamente del rapporto costo - efficacia delle due apparecchiature in base alla diverse probabilit pre - test . risultati costi differenziali coronaro - tc 1 . 
a ci va ancora aggiunto il costo dellelettrocardiografo ecg monitor , hme lifepulse 10 tg compatibile con la mdtc toshiba che ha un costo dacquisto di 3500 ( pari a 437 annui )  . 
va ancora considerato il sistema pacs : il suo costo dacquisto stato pari a 2500000 , a cui corrispondono 312500 di costo annuo per 8 anni radiol med ( 2009 ) 114 : 239252 3 . 
we calculated the personnel costs ( radiologist , technologist and nurse ) by considering their yearly hours and subtracting time off for ordinary paid leave , extraordinary paid leave and sick leave ( 30% on average )  . 
radiologist costs were 120 / examination based on an annual cost of 101 , 040 , a daily cost of 577 , an hourly cost of 80 and an estimated commitment of 90 min ( preliminary evaluation of the patient , attendance during acquisition , image postprocessing , reporting )  . 
we considered the price of the dedicated haemodynamic unit ge innova 2000 ( general electric medical systems )  . the cost to be amortised ( purchase price ) is 1 , 004 , 611 , leading to a yearly cost of 125 , 576 for 8 years of amortisation . 
materials used during the procedure : sterile gauze ( 0.01 ) , four 10 - cc luerlock syringes ( 0.68 ) , four 20 - cc syringes ( 0.72 ) , arterial puncture needle ( 1.25 ) , two vials of lidocaine ( 0.11 ) , one 0.38 175 - cm , j - tip cordis emerald guidewire ( 6.78 ) , one 6 - fr st . 
lesecuzione di una coronaro - tc prevede lutilizzo di 80100 ml di mezzo di contrasto iomeprolo 400 ( iomeron , bracco , milano ) in flaconi da 250 ml ( 116 , 66 )  . 
viene inoltre utilizzato un ago cannula abbocath da 18 g ( 0 , 44 ) con una piccola quantit di disinfettante , un batuffolo di cotone ed un cerotto ( il costo di questo materiale trascurabile )  . 
nei protocolli di coronaro - tc prevista la somministrazione di 100 mg di - bloccante ( metoprololo ) per os almeno unora prima dellindagine nei soggetti che presentano una frequenza cardiaca superiore ai 65 battiti al minuto . 
si utilizza inoltre un cd rom ( costo unitario di 0 , 33 ) che viene fornito ai pazienti ambulatoriali , non provenienti dal reparto di cardiologia , che rappresentano il 28% delle coronaro - tc eseguite presso la nostra u.c.o. 
poich il costo dacquisto del tubo radiogeno di 91800 e la sua durata prevista pari a 300000 colpi , con un costo per ogni colpo di 0 , 30 emerge un costo per indagine di 6 , 12 . 
abbiamo calcolato il costo del personale ( medico , tecnico e infermieristico ) considerando il suo debito orario annuale , sottraendo da esso le assenze per congedo ordinario , straordinario e malattia ( in media 30% ) e stimando quindi in 35 settimane / anno il tempo lavorativo effettivo . 
ne consegue un costo medico di 120 / esame in base ad un costo annuo di 101040 , giornaliero di 577 e orario di 80 avendo stimato il suo impegno temporale per tale metodica in 90 minuti ( valutazione preliminare del paziente , presenza in fase di acquisizione dellesame , elaborazione delle immagini , stesura del referto )  . 
il costo del tecnico radiologo ( tsrm ) risulta di 15 , 5 in base ad un costo annuo di 39679 , giornaliero di 226 ed orario di 31 , stimando un suo impiego per 30 minuti . 
we calculated , using the same method as used for ctca , a cardiologist cost of 86.60 on the basis of a yearly cost of 101 , 040 , a daily cost of 577 and hourly cost of 80 and estimating a time commitment of approximately 65 min per examination . 
technologist cost was 31 based on a yearly cost of 39 , 679 , a daily cost of 226 and hourly cost of 31 , with a commitment of 60 min per examination . 
based on the data provided by our hospitals planning and control office , the cost of 1 day of hospitalisation at the department of cardiology is 1 , 652  . 
all patients undergoing conventional coronary angiography are hospitalised for at least 1 day , whether the puncture site is closed with a sealing device ( angioseal ) or by application of manual compression . 
the patient is discharged on the following day . common costs common costs are those related to support staff and support materials ( computers , printers , recording equipment , electrical and network materials , stationery , cleaning supplies )  . in calculating the cost of support staff , we considered all those professionals not discussed so far : one chief consultant radiologist , two chief technologists , three technologists , four auxiliary staff , four file clerks , six assistants and these professionals administrative assistants . 
materiale utilizzato dopo la procedura : dispositivo angio - seal ( 138 ) ; questo dispositivo stato utilizzato in 129 pazienti su 821 eseguiti nel periodo preso in considerazione per tale valutazione ovvero nel 15 , 71% dei casi . 
quindi , il materiale preparatorio ha un costo totale pari a 10 , 41 , il materiale utilizzato radiol med ( 2009 ) 114 : 239252 common cost of 5 per examination . 
the lack of support staff at the department of cardiology results in different common costs for the two procedures . external costs blood tests performed before the two procedures involve an external cost of 1.90 per examination for ctca and 8.80 for digital coronary angiography . 
this depends on the fact that a correct diagnosis is considered a positive factor in any cost - effectiveness analysis , and correct diagnoses will be all the more frequent the higher the pretest likelihood . 
in particular , the data demonstrate that ctca is more costeffective in patients with a pretest likelihood up to 86% , with a cost per correct diagnosis of cad ranging from 7 , 295.10 ( 10% pretest likelihood ) to 2 , 593.9 ( 86% pretest likelihood )  . 
by contrast , coronary angiography shows better cost - effectiveness for pretest likelihoods of 87%100% , with a cost per correct diagnosis of cad between 2 , 563.59 ( 87% pretest likelihood ) and 2 , 207.60 ( 100% pretest likelihood )  . 
new durante la procedura ha un costo totale pari a 112 , 9 e il materiale utilizzato dopo la procedura ha un costo di 21 , 68 , per un costo complessivo di 144 , 99 . 
abbiamo calcolato , con analoga modalit rispetto alla coronaro - tc , un costo medico di 86 , 6 in base ad un costo annuo di 101040 , giornaliero di 577 e orario di 80 stimando un impegno per tale metodica di circa 65 minuti . 
il costo del personale tecnico di 31 in base ad un costo annuo di 39679 , giornaliero di 226 e orario di 31 con un impegno di 60 minuti / esame . 
il costo del personale infermieristico di 29 in base ad un costo annuo di 39174 , giornaliero di 223 e orario di 29 con un impegno di 60 minuti / esame . 
viene effettuata nei pazienti sottoposti a coronarografia almeno una giornata di degenza , sia che venga posizionato il dispositivo di chiusura del foro dentrata ( angio - seal ) , sia che si applichi una compressione manuale . 
il paziente viene dimesso nella giornata successiva . costi comuni i costi comuni sono rappresentati dai costi relativi al personale di supporto e da quelli dei materiali di supporto ( computer , stampanti , registratori , materiale elettrico e di rete , materiale di cancelleria , materiale di pulizia )  . 
si tratta di 1 primario , 2 capotecnici , 3 tecnici , 4 ausiliari , 4 archivisti , 6 tra coadiutori e assistenti amministrativi . complessivamente questinsieme di unit lavora per il funzionamento di tutta lu.c.o. ; non riteniamo che il loro lavoro sia influenzato dalla tipologia di esami e quindi il loro costo complessivo stato ripartito proporzionalmente sullinsieme di tutte le indagini eseguite presso lu.c.o. 
nel 2006 il costo totale di tale pool di operatori risultato di 557646 ; il numero complessivo di esami stato di 111367 ; risulta un costo comune aggiuntivo per esame di 5 , 00 . 
the impact of new technology on health care expenditure depends exclusively on its appropriate use , even relative to other available diagnostic and therapeutic tools , to optimise resource utilisation . 
this is especially true in the field of diagnostic radiology , as technology has a major impact on overall hospital costs , and the clinical impact of the radiological process heavily affects how the patient is managed following diagnosis , with effects on treatment decisions and consequently on the overall cost of the disease . the main point to recall when dealing with an economic analysis is that the costs refer to the investment made when a resource is consumed during a therapeutic or diagnostic programme . 
one of the main aspects to be faced when costi esterni per il dosaggio dei diversi parametri ematochimici utili preliminarmente alleffettuazione delle due metodiche vi un costo esterno per esame che di 1 , 90 per la coronaro - tc e di 8 , 8 per la coronarografia digitale . 
inoltre nell1% dei pazienti si esegue una profilassi farmacologica ( basata sullimpiego di cortisonici associati ad anti - h1 ed anti - h2 ) , per un costo di 4 , in media 0 , 04 in pi per ogni esame . 
1 valutazione grafica dellanalisi di costo - efficacia delle due metodiche in relazione alle diverse probabilit pre - test di malattia coronarica . coronaro - tc : 222 , 23 + 5 , 50 + 2 , 3 = 230 , 03 coronarografia : 366 , 18 + 0 , 50 + 9 , 2 + 1652 = 2027 , 88 . le tabelle 2 e la fig . 
ci dipende dal fatto che una diagnosi corretta viene considerata un fattore positivo in unanalisi di costo - efficacia e una diagnosi corretta sar tanto pi frequente quanto pi elevata la probabilit pre - test . 
in particolare si dimostra come la coronaro - tc sia la metodica con il migliore rapporto di costo - efficacia nei pazienti con probabilit pre - test fino all86% con un costo per identificare correttamente la malattia coronaria che varia tra 7295 , 10 ( 10% probabilit pre - test ) e 2593 , 9 ( 86% probabilit pre - test )  . 
mentre dall87% al 100% di probabilit pre - test la metodica con il migliore rapporto costo - efficacia la coronarografia che presenta un costo per identificare correttamente la malattia coronarica che varia tra 2563 , 59 ( 87% probabilit pre - test ) e 2207 , 60 ( 100% probabilit pre - test )  . 
le nuove tecnologie , soprattutto al momento della loro introduzione nella pratica clinica , presentano costi elevati , che risultano giustificabili solo attraverso la dimostrazione di un reale impatto diagnostico - terapeutico . 
gli effetti sulla spesa sanitaria di un innovazione tecnologica dipendono esclusivamente da un suo appropriato utilizzo , anche in relazione ai mezzi diagnostici e terapeutici gi disponibili , in modo da ottimizzare luso delle risorse . 
in ambito radiologico queste considerazioni sono ancor pi valide in quanto le tecnologie utilizzate hanno un grosso peso sul totale dei costi aziendali , ed inoltre limpatto clinico fornito dal radiologo influenza notevolmente la storia del paziente successiva alla diagnosi , condizionando le scelte terapeutiche e di conseguenza i costi complessivi della patologia . il punto principale da ricordare quando si affronta unanalisi economica che i costi si riferiscono allinvestimento fatto quando una risorsa viene consumata in un programma di trattamento o di diagnosi . 
the only significant cost factor that is higher for ctca is medical personnel cost owing to the long postprocessing time , a factor that is likely to decrease with future software improvements . 
if , on the other hand , we correctly consider hospitalisation costs , the cost of coronary angiography exceeds that of ctca by a factor of 9 . this form of cost accounting employs a method that is frequently used in industrial organisations and that ensures a rigour that reduces the approximations of traditional costcalculation methods [ 14 ]  . 
our analysis illustrates the situation at the departments of radiology and cardiology at a given point in time , and as such cannot be extrapolated directly to other centres , where costs may differ considerably because of different equipment or materials used or different organisational strategies that affect , for example , personnel utilisation and cost . 
this analysis may thus serve as a methodological model to be applied to other settings . given that coronary angiography is performed on inpatients , any cost analysis should be compared against the reimbursement rates based on the diagnosis - related groups ( drg )  . 
in the friuli venezia giulia region , coronary angiography is listed under drg 124 ( cardiovascular disease except acute myocardial infarction , with cardiac catheterisation ) , which has a reimbursement rate of 4 , 876.00 , regardless of the actual number of days in hospital . ctca , instead , is normally performed on outpatients , so it is not allocated a reimbursement based on the drg . 
if the examination was to be performed on inpatients , drg 140 ( angina pectoris ) would probably apply , which has a reimbursement rate of 332.00 for up to 3 days in hospital and of 2 , 929.00 for hospitalisations exceeding 3 days . when considering cost - effectiveness , the least costly technique should ideally also be the most sensitive . although the sensitivity of ctca has been substantially improved by the advent of the new 64 - slice ct scanners , it nonetheless remains lower than that of coronary angiography ( the gold standard )  . 
in evaluating a patient at high risk of cad , the decision to perform ctca as a first - line study is not justified in either clinically or economically , as it is likely that the patient will subsequently have to undergo coronary angiography , at least for therapeutic purposes . 
this finding , affrontare per intraprendere questo tipo di analisi sono in primis il periodo di tempo nel quale valutare il costo poich una procedura bench pi conveniente pu richiedere nel tempo unulteriore procedura , per un risultato falsamente negativo o per linsorgenza di una complicanza , vanificando cos il vantaggio economico [ 8 ]  . lanalisi dei costi da noi effettuata , qualora non si consideri il costo della degenza , ha fatto rilevare un costo superiore del 38 , 8% della coronarografia rispetto alla coronaro - tc . 
lunico fattore di costo significativo in cui la coronaro - tc ha un valore superiore rappresentato dal costo del personale medico , dovuto al tempo di elaborazione tuttora elevato che questi esami richiedono , fattore che del tutto verosimilmente si ridimensioner negli anni a venire grazie ai miglioramenti dei software dedicati . qualora si prenda correttamente in considerazione anche il costo della degenza , il costo della coronarografia sopravanza quello della coronaro - tc di un fattore nove . questa analisi dei costi utilizza una tecnica cui si fa ricorso frequentemente in ambito industriale e che garantisce un rigore che riduce le approssimazioni dei metodi tradizionali di calcolo dei costi [ 14 ]  . 
di cardiologia , in un determinato momento storico , e i dati non possono essere esportati acriticamente , in quanto in altre strutture i costi possono essere estremamente diversi , vuoi per diverse apparecchiature e diversi materiali utilizzati , vuoi per diverse scelte organizzative che possono incidere ad esempio sullimpiego e quindi sui costi del personale . questa analisi assume quindi rilievo soprattutto quale modello metodologico utilizzabile in altre realt . dal momento che la coronarografia viene effettuata su pazienti ospedalizzati , unanalisi dei costi opportuno si raffronti con i rimborsi basati sul drg . 
nella nostra regione il drg 124 che richiama la coronarografia ( malattia cardiovascolare eccetto infarto miocardio acuto , con cateterismo cardiaco ) prevede un rimborso di 4876 , 00 , indipendentemente dalla durata della degenza . la coronaro - tc viene invece effettuata nella larghissima maggioranza dei casi in pazienti ambulatoriali e quindi ad essa non si applica il rimborso sulla base del drg . qualora venisse effettuata in paziente ospedalizzato , si applicherebbe verosimilmente il drg 140 ( angina pectoris ) che prevede un rimborso di 332 , 00 se la degenza inferiore ai 3 giorni e di 2929 , 00 se invece superiore ai 3 giorni . quando si consideri il rapporto costo - efficacia , va anzitutto rilevato come idealmente sia auspicabile che la metodica meno costosa sia anche la pi sensibile . 
however , because the pretest likelihood of disease is the decisive factor in establishing which of the two techniques ctca or coronary angiography is more cost effective , determining the pretest likelihood is an important step in selecting the most appropriate diagnostic strategy [ 15 , 16 ]  . it is also important to consider the impact of the different diagnostic approaches on patient survival and quality of life . this aspect could be addressed by further studies . our results can be compared with a recently published cost - effectiveness analysis carried out by dewey et al . 
 [ 13 ] , which sought to determine the cost - effectiveness of ctca and magnetic resonance imaging ( mri ) according to the pretest likelihood of cad compared with the gold standard digital coronary angiography . 
our findings differ from those reported by dewey et al . , in particular as regards their statement that ctca has good cost - effectiveness up to a pretest likelihood of 60%70% , whereas coronary angiography is more cost - effective in patients with higher pretest likelihoods . 
 [ 13 ] 230 , 03 2027 , 88 costo coronaro - tc costo coronarografia sensibilit della coronaro - tc 98 , 4% specificit della coronaro - tc 90% coronaro - tc : esami non diagnostici 3 , 6% 175 , 69 630 , 99 95 , 6% 78 , 8% 1 , 15% grafia ( considerata come gold standard ) e comunque bisogna ricordare come nella scelta della metodica diagnostica ci non sia sufficiente . 
infatti nella valutazione di un paziente ad alto rischio coronarico la scelta di effettuare come prima indagine la coronaro - tc non giustificata n dal punto di vista clinico n da quello economico poich verosimile che successivamente tale paziente dovr eseguire una coronarografia quantomeno ai fini terapeutici . 
 in base ai nostri dati , nella nostra realt operativa , abbiamo dimostrato come la coronaro - tc sia la metodica con il migliore rapporto costo - efficacia nella valutazione di pazienti che presentano una probabilit pre - test inferiore all87% . 
variazioni dei costi e variazioni dellaccuratezza diagnostica ( ad esempio ulteriore incremento della sensibilit con i progressi tecnologici delle apparecchiature tc ) potranno modificare il quadro anche in un prossimo futuro . 
va comunque sottolineato che la probabilit pre - test il fattore determinante nello stabilire quale tra la coronaro - tc e la coronarografia sia lindagine con il migliore rapporto di costo - efficacia , per cui stabilire il valore di probabilit pre - test un importante criterio nel selezionare la strategia diagnostica pi appropriata [ 15 , 16 ]  . 
ci potrebbe rappresentare loggetto di studi futuri . i nostri risultati possono essere confrontati con una valutazione di costo - efficacia comparsa recentemente in letteratura ed effettuata da dewey et al . 
 [ 13 ] che si proponeva di verificare il valore di costo - efficacia , in base alla probabilit pre - test di malattia coronarica di due indagini diagnostiche , la coronaro - tc e la risonanza magnetica , rispetto al gold standard rappresentato dalla coronarografia digitale . nella valutazione dei costi vi sono alcune differenze significative tra il lavoro di dewey et al . 
infatti per questa analisi noi ci siamo basati su costi ottenuti da una scrupolosa analisi dei costi differenziali , comuni ed esterni , mentre il lavoro di dewey utilizza dei dati di costo apparecchiature che derivano dai drg . 
questo deriva dal fatto che noi abbiamo eseguito unanalisi dei costi per ottenere il nostro dato , 252 radiol med ( 2009 ) 114 : 239252 besides , there was an important difference in the cost of coronary angiography , which was derived from the german equivalent of the drg system in dewey et al.s study but was actually computed by means of cost analysis in our study . consequently , dewey et al . 
found coronary angiography to be most cost effective for a pretest likelihood of at least 70% , with costs per correctly identified cad patient ranging from 1 , 153 ( 70% likelihood ) to 807 ( 100% likelihood ) , whereas we found coronary angiography to be most cost effective only for a pretest likelihood > 86% . 
 [ 13 ] riportano come la coronarografia sia la metodica con migliore rapporto costo - efficacia al di sopra del 70% di probabilit pre - test con un costo per identificare correttamente un paziente con malattia coronarica che varia tra 1153 ( 70% probabilit pre test ) e 807 ( 100% probabilit pre test ) , mentre dai nostri dati ci risulta vero solo con una probabilit pre - test di malattia superiore all86% . 
radiodiagnostica , fondazione irccs policlinico san matteo , v.le golgi 19 , 27100 pavia , italy 2specializzanda di radiologia , istituto di radiologia delluniversit di pavia , pavia , italy correspondence to : g . 
we retrospectively reviewed the radiographs taken during the past 26 years in children ( age 018 years ) undergoing imaging of the spine or of other body segments in which the spine was adequately depicted , to determine possible intervertebral disc calcifications . 
the following clinical evaluation was extrapolated from the patients charts : presence of spinal symptoms , history of trauma , suspected or clinically evident scoliosis , suspected or clinically evident syndromes , bone dysplasias , and preor postoperative chest or abdominal x - rays . 
five calcifications were asymptomatic ( one newborn baby with patau syndrome ; three patients studied to rule out scoliosis , hypochondroplasia and syndromic traits ; one for dyspnoea due to sunflower seeds inhalation )  . 
apart from the calcification in the patient with cervical pain , all calcifications were asymptomatic and constituted an incidental finding ( particularly those detected at the thoracic level in the patient studied for sunflower - seed inhalation )  . 
sono stati valutati retrospettivamente tutti i radiogrammi eseguiti nel corso di 26 anni in bambini ( di et compresa tra 0 e 18 anni ) sottoposti a studio del rachide o di altri distretti corporei in cui esso era compreso e ne era possibile la valutazione , alla ricerca di eventuali calcificazioni . 
abbiamo rilevato la presenza di calcificazioni dei dischi intervertebrali in 6 pazienti ; per 5 dei quali non vi era in anamnesi sintomatologia dolorosa ( un neonato affetto da sindrome di patau ; tre pazienti erano stati sottoposti ad esame radiologico per diagnosi clinica di scoliosi , ipocondroplasia e stato sindromico , rispettivamente ; uno perch aveva inalato semi di girasole ) , mentre uno solo era sintomatico , con anamnesi di dolore acuto al rachide cervicale . 
con la sola eccezione del paziente con algia cervicale , tutte le calcificazioni erano asintomatiche , il loro riscontro risultando del tutto fortuito ( in particolare quelle a livello toracico nel paziente sottoposto a radiografia del torace per la inalazione di semi di girasole ) , avevano di forma variabile , da lineari a rotondeggianti . 
la casistica esaminata conferma che il riscontro di calcificazioni dei dischi intervertebrali evento raro nellinfanzia e che non deve destare 332 radiol med ( 2009 ) 114 : 331341 only very few cases , such as those of medullary compression or severe dysphagia due to anterior herniation of cervical discs , may require surgical procedures . keywords spine childhood calcifications intervertebral disc calcifications preoccupazione , anche in presenza di sintomatologia dolorosa , dato che in questo caso la calcificazione tende a regredire spontaneamente ed in breve tempo ( contrariamente a quelle indolenti che possono perdurare per anni , per sparire entro i 20 ) , con o senza terapia antidolorifica ed immobilizzazione , richiedendo solo in rarissimi casi ( compressioni midollari o gravi fatti disfagici , in caso di erniazione anteriore nelle localizzazioni cervicali ) la necessit di interventi chirurgici . parole chiave rachide bambini calcificazioni calcificazioni dischi intervertebrali introduction introduzione intervertebral disc calcification is a chance finding in both childhood and the adult population . 
since the first case reported by bron [ 1 ] in 1924 of a 12 - year - old boy presenting with thoracic spine pain , fever and scoliosis , no more than 400 cases have been reported in the 0to 20 - year age group [ 225 ]  . 
the finding may be entirely serendipitous during x - ray studies performed for other clinical problems or may be detected in cases of a typical clinical syndrome characterised by acute pain , mostly affecting the cervical spine , accompanied by fever , raised erythrocyte sedimentation rate ( esr ) and sometimes leucocytosis [ 2 , 3 , 5 , 710 , 1619 , 2123 ]  . 
the time of appearance of calcifications is uncertain , although it certainly precedes by far the time of discovery , as shown by the many cases in which a careful re - evaluation of previous x - rays following the detection of calcifications showed that the lesions were indeed present even in childhood but had gone undetected and unreported [ 2 , 7 , 16 , 17 , 23 ]  . 
 we retrospectively reviewed x - rays taken during the past 26 years in children ( age 018 years ) undergoing imaging of the spine or other body segments in which the spine adequately visualised to discover possible intervertebral disc calcifications . 
the following clinical data were extrapolated from the patients charts : presence of spinal symptoms , history of trauma , suspected or clinically evident scoliosis , suspected or clinically evident syndromes , bone dysplasias and preor postoperative chest or abdominal x - rays . 
dalla prima segnalazione , nel lontano 1924 da parte di bron ( un ragazzo di 12 anni con dolori dorsali , febbre e scoliosi ) [ 1 ] , si sono avuti nel corso degli anni segnalazioni che hanno interessato non pi di 400 casi nel gruppo di et neonato fino a 20 anni [ 225 ]  . 
il reperto pu essere del tutto occasionale , nel corso di indagini radiologiche per altro motivo , o di riscontro in presenza di una sindrome clinica piuttosto tipica , caratterizzata da sintomatologia dolorosa acuta , con localizzazione quasi sempre a livello del rachide cervicale , accompagnata da rialzo febbrile , aumento della ves e saltuaria leucocitosi [ 2 , 3 , 5 , 710 , 1619 , 2123 ]  . 
incerta let in cui compaiono le calcificazioni : certo che essa deve essere situata a distanza anche di molti anni dalla loro effettiva scoperta , come dimostrato da casi in cui , dopo la scoperta di calcificazioni , lattenta rivalutazione , quando possibile , di indagini radiologiche eseguite in precedenza , ne ha dimostrato la presenza , allora per non segnalata , anche in bambini tenera et , e ci anche a distanza di anni dal successivo riscontro [ 2 , 7 , 16 , 17 , 23 ]  . 
dallesame delle richieste sono state registrate le seguenti informazioni : presenza di sintomatologia riferibile al rachide , anamnesi di trauma , sospetto o diagnosi clinica di scoliosi , di sindromi , di displasia ossea , richiesta di radiografia di addome e / o torace preo postoperatori . radiol med ( 2009 ) 114 : 331341 performed during her first day of life to evaluate bone changes related to the syndrome showed a differentiation defect at the thoracolumbar passage . 
eleven pairs of ribs were detected ( hypoplasia of the t11 right rib , no left rib ) and intervertebral disc calcifications at t10 - t11 and l1 - l2 levels . 
the first one was thin , oval in shape and slightly dense ; the second was round , large , fairly opaque and caused a small increase of the intervertebral space . 
this patient was a 121 / 2 - year - old girl who underwent x - ray study of the spine to rule out scoliosis in the absence of pa intervertebral disc calcifications were detected at t5 - t6 ( round and located in the posterior portion of the intervertebral space ) , t6 - t7 ( linear , central ) and possibly at t7 - t8 levels . 
lo studio radiologico dello scheletro per la determinazione di eventuali alterazioni ossee correlabili alla sindrome da cui affetta , eseguito nella prima giornata di vita , ha evidenziato vizio di differenziazione al passaggio dorso - lombare con presenza di 11 paia di coste ( ipoplasica la destra di d11 ed assente la sinistra ) , calcificazioni dei dischi corrispondenza di d10 - d11 e di l1 - l2 . 
i radiogrammi del torace evidenziano , oltre ad area di opacit disventilatoria in corrispondenza del lobo inferiore destro , calcificazioni dei dischi intervertebrali in corrispondenza di d2 - d3 e d5 - d8 , sotto forma di immagini radiopache di diversa densit , e di forma ovalare allungata . 
vizio di differenziazione al passaggio dorso - lombare con presenza di 11 paia di coste ( ipoplasica la destra di d11 ed assente la sinistra ) , calcificazioni dei dischi intervertebrali in corrispondenza di d10 - d11 e di l1 - l2 . 
a chest x - ray taken to determine the location of the foreign body showed right lower - lobe parenchymal opacity and intervertebral disc calcifications at t2t4 and t5t8 levels . 
according to the boys parents , the boy had never complained of spinal pa patient 4 caso 6 radiol med ( 2009 ) 114 : 331341 mai avvertito sintomatologia dolorosa in corrispondenza del rachide . 
vengono rilevate calcificazioni degli spazi intersomatici d4 - d5 , d9 - d10 , d12 - l1 , questultima di ampie dimensioni , anche se non omogenea , di forma ovalare , localizzata nei due terzi posteriori dello spazio intersomatico . 
3a il radiogramma del torace evidenzia opacit del lobo inferiore destro dovuta allaspirazione di semi di girasole nonch presenza di calcificazioni sottili , quasi lineari degli spazi intersomatici d2 - d4 e d5 - d8 , ben visibili anche b nella proiezione ll . radiol med ( 2009 ) 114 : 331341 fig . 
4a grossolana calcificazione dello spazio intersomatico posteriore d11 - d12 che impronta le limitanti somatiche , in particolare b la superiore di d11 . hospital to assess her dysmorphic features clinically unrelated to any syndrome . 
a very large , coarse , intervertebral disc calcification was detected in the posterior third of the t11 - t12 intersomatic space , with indentation of the vertebral margins , especially of t12 . 
this patient was an 11 - year - old boy examined to rule our hypochondroplasia in the absence of back paintervertebral disc calcifications were found at t4 - t5 , t9 - t10 , t12 - l1 levels . 
this patient was a 101 / 2 - year - old boy admitted to hospital due to sudden onset of progressively worsening neck pain unresponsive to analgesic therapy , with impairment of neck movement and severe neck , arm and back pa cervical spine x - ray showed a tiny wedge - shaped calcification posteriorly located at the c2 - c3 intervertebral mezzo , causa linsorgenza improvvisa di dolenzia in regione sterno - cleido - mastoidea che non recede con terapia antalgica , in aumento progressivo , con limitazione marcata della mobilit del collo associata ad estrema sensazione dolorosa al collo , braccio , schiena . 
a distanza di 6 mesi le calcificazioni erano ancora evidenti in assenza di altri episodi dolorosi . nessuno di questi soggetti stato sottoposto a studio tc od rm . quadro clinico , frequenza e sintomatologia le calcificazioni del disco intervertebrale nel bambino sono sempre osservate in corrispondenza del nucleo polposo , in particolare quello dei somi del tratto cervicale . hanno aspetto di solito ovalare , rotondeggiante , appiattito , raramente sono frammentate o puntiformi e sono localizzate quasi sempre in sede centrale [ 2 ]  . 
sono possibili minime alterazioni della morfologia dei somi adiacenti alla / e calcificazione / i , reperto presente nel 90% dei casi in pazienti sintomatici [ 2 , 6 , 9 , 10 , 1517 , 22 ] , sotto forma di riduzione in altezza , deformazione a cuneo anteriore o posteriore , irregolarit o sclerosi marginale , scomparsa del nucleo di ossificazione delle limitanti somatiche angolari anteriori [ 6 , 10 , 16 , 17 ] ed impronte da parte delle calcificazioni sulle limitanti somatiche adiacenti , reperti cui si pu associare riduzione od allargamento degli spazi intersomatici corrispondenti [ 3 , 6 , 8 , 10 , 18 , 19 ]  . 
 anche se le calcificazioni possono essere riscontrate in ogni tratto del rachide , quelle cervicali sono le pi frequenti ( con prevalente localizzazione in corrispondenza dello spazio intersomatico c5 - c6 e c6 - c7 , mentre molto rara la localizzazione in corrispondenza di c7 - d1 ) , con associata erniazione anteriore o posteriore nel 38% dei casi [ 4 , 6 , 10 , 12 , 1517 , 25 ] , seguite dalle toraciche , mentre le lombari sono di riscontro , molto raro [ 7 , 23 ]  . 
 possibile linteressamento multiplo nel 30%40% dei casi [ 2 , 16 , 19 ] , potendosi arrivare al numero di 8 osservate in un paziente asintomatico [ 2 ] e ad uno medio di 1 , 9 calcificazioni per paziente secondo girodias et al . 
il maggior riscontro nel gruppo di et 610 anni [ 7 , 8 , 16 , 19 , 20 , 22 , 23 , 25 ] con casi osservati anche nelle prime ore o giorni di vita [ 2 , 11 , 16 ] , con una certa maggior frequenza nei maschi delle calcificazioni a livello cervicale mentre nelle femmine la distribuzione variabile nei vari tratti ( 7 : 5 ) e con netta 336 radiol med ( 2009 ) 114 : 331341 fig . 
5a - d calcificazioni intersomatiche in corrispondenza di d4 - d5 , d9 - d10 , d - 12 - l1 di cui grossolana quella d12 - l1 , di forma quasi ovalare , al terzo medio dello spazio intersomatico . 
a distanza di un anno c , d , aspetto frammentato in due parti della calcificazione d12 - l1 ; meno densa e riconoscibile solo in parte quella tra d9 - d10 . space and a larger , inhomogeneous round calcification at the c5 - c6 central intervertebral space . 
six months later , the patient was free of symptoms , intervertebral disc calcifications were still the and detectable . none of the patients in this case series underwent computed tomography ( ct ) or magnetic resonance imaging ( mri )  . clinical findings , frequency and signs and symptoms intervertebral disc calcifications in children are always found in the nucleus pulposus , in particular those of the cervical spine . 
calcifications are usually oval or round , flat , rarely fragmented or punctiform , and located centrally , without reduction of the affected intervertebral disc space , which may be increased [ 2 ]  . 
slight changes may be detected in the adjacent vertebral bodies in nearly 90% of symptomatic cases [ 2 , 6 , 9 , 10 , 1517 , 22 ]  . 
these include flattening , anterior or posterior wedging , irregularities or marginal sclerosis , disappearance of anterior ring apophysis [ 6 , 10 , 16 , 17 ] and impression due to the calcification on the fig . 
noteworthy is the absence of swelling of the perivertebral soft tissue [ 17 ]  . even though calcifications may be found in any part of the spine , cervical calcifications are the most frequent ( especially at c5 - c6 and c6 - c7 intersomatic space , whereas the c7 - t1 localisation is rare ) , associated in 38% of cases with anterior or posterior herniation [ 4 , 6 , 10 , 12 , 1517 , 25 ]  . second most common are thoracic calcifications , whereas lumbar ones are very rare . 
multiple localisation is possible in 30%40% of cases [ 2 , 16 , 19 ] , with up to eight disc calcifications having been found in one asymptomatic patient [ 2 ] and a median of 1.9 calcifications according to girodias et al . 
there is a slight predominance among males ( 7 : 5 male - to - female ratio ) , in whom they more commonly affect the cervical spine , whereas distribution is uneven at the cervical and dorsal spine in females ; there is a clear - cut prevalence in caucasians patients [ 3 , 7 , 8 , 16 , 21 , 23 , 25 ]  . 
 radiological findings are completely different from those of spondylodiscitis , which is usually confined to a single disc lumbar spine involvement being more frequent followed by reduction of the intervertebral space , irregularities of vertebral - body plates , perivertebral soft tissue swelling , possible vertebral - body fusion and never disc calcification [ 6 , 7 , 16 , 17 , 22 ]  . in those cases in which neurological symptoms are present in addition to pain , mri will accurately demonstrate the possible compression of the medulla and nerve roots [ 6 , 17 , 2022 , 25 , 26 ] , diminished calcification signal intensity [ 12 , 23 ] and initial involvement of other discs , especially at the cervical level [ 26 ]  . 
mri may also show lower signal intensity of the vertebral body below the affected disc [ 12 ]  . ct will better define the site of calcified and probably herniated discs [ 16 , 25 ]  . for radiation protection reasons , mri should be the preferred imaging modality in paediatric patients , even though the procedure is longer and sometimes more poorly tolerated by children compared with the faster spiral ct , which has been advocated by some authors [ 16 , 25 ]  . 
mri also has the advantage of being able to adequately demonstrate spinal - cord compression in the case of disc herniation [ 6 , 17 , 2022 , 25 , 26 ] and revealing further calcifications undetectable on plain x - ray in cases of calcified discitis [ 26 ]  . 
 il quadro radiologico ben diverso da quello della spondilo - discite , di regola localizzata ad un solo disco spesso a livello lombare e che determina riduzione dello spazio intersomatico , irregolarit delle limitanti somatiche corrispondenti , manicotti perisomatici , possibile fusione tra i somi interessati ma mai calcificazione del disco [ 6 , 7 , 16 , 17 , 22 ]  . in casi in cui la sintomatologia oltre che dolorosa abbia anche una componente neurologica , lo studio con risonanza magnetica nucleare definir con precisione la eventuale compressione sul midollo spinale e le radici nervose [ 16 , 17 , 2022 , 25 , 26 ] , la ridotta intensit di segnale della calcificazione [ 12 , 23 ] , potendo evidenziare segni di iniziale interessamento anche di altri dischi , soprattutto a livello cervicale [ 26 ] ed una ridotta intensit del segnale del corpo vertebrale sottostante al disco interessato [ 12 ] mentre la tomografia computerizzata meglio evidenzier la posizione del nucleo calcificato ed eventualmente erniato [ 16 , 25 ]  . nei soggetti in et pediatrica , per motivi protezionistici dovrebbe essere preferito limpiego della rm , anche se lindagine pi lunga e spesso mal sopportata dai pazienti , a confronto della pi rapida tc spirale come suggerito in letteratura [ 16 , 25 ]  . 
la rm ha anche il vantaggio oltre al protezionistico di ben dimostrare non solo le compressioni sul midollo in caso di disco erniato [ 16 , 17 , 2022 , 25 , 26 ] , ma anche la possibile esistenza di ulteriori calcificazioni , non dimostrabili sui radiogrammi diretti , in caso di discite calcifica [ 26 ]  . clinicamente , le calcificazioni nel bambino possono essere divise in due gruppi , quelle sintomatiche , associate a un quadro clinico particolare , e quelle asintomatiche . 
le calcificazioni sintomatiche sono soprattutto localizzate a livello cervicale , in particolare in corrispondenza di c5 - c6 e c6 - c7 e sono pi frequenti nei maschi con et media di presentazione sui 7 , 1 anni [ 6 , 8 , 15 , 17 , 20 ]  . 
la comparsa dei sintomi improvvisa , nel giro di 12 / 24 ore , accompagnata da un quadro clinico tipico , caratterizzato da rialzo febbrile , torcicollo , aumento della ves , modica leucocitosi . 
il dolore quasi sempre il motivo causale dello studio del rachide e della conseguente scoperta delle calcificazioni , in particolare a livello cervicale , ove la loro presenza associata nell85%90% dei casi a spasmi muscolari peri - vertebrali , riduzione della mobilit e dolorabilit alla palpazione e da torcicollo nel 40% dei casi [ 4 , 7 , 13 , 16 , 17 , 19 , 20 , 25 ] , mal di schiena e talora a scoliosi [ 7 ] , mentre il dolore assai meno frequente , se non assente , nelle localizzazioni multiple , in particolare dorsali e lombari . 
la risoluzione della sintomatologia rapida ( 2 / 3 settimane ) [ 8 , 13 , 16 , 17 , 21 ] , salvo nei rari casi di pazienti con compressione midollare [ 8 ] , in cui a fronte di sofferenza radicolare resistente alla terapia 338 radiol med ( 2009 ) 114 : 331341 symptomatic calcifications are found at the cervical level , especially at c5 - c6 and c6 - c7 . 
presentation is usually abrupt over a 12to 24hour time span and usually found in connection with a typical clinical syndrome of low - grade fever , tenderness , neck pain , slight increase in esr and leucocytosis . 
pain is usually the reason for the radiological study and consequent discovery of calcifications , especially at the cervical level , where calcifications are associated with cervical pain , perivertebral muscle spasms , reduction in motility and tenderness in 85%90% of cases , torticollis in 40% of cases [ 4 , 7 , 13 , 16 , 17 , 19 , 20 , 25 ] , back pain and , sometimes , scoliosis [ 7 ]  . 
symptom resolution is fast ( 23 weeks ) [ 8 , 13 , 16 , 17 , 21 ] , except in rare cases of patients with medullary compression [ 8 ] in whom , due to compression radiculopathy resistant to conservative therapy , a surgical procedure is sometimes necessary [ 5 , 8 , 13 , 20 , 24 ]  . 
in the case of anterior herniation , there may be dysphagia due more to perioesophageal inflammatory swelling than to direct oesophageal compression by the displaced disc [ 4 , 8 , 1416 ]  . 
in cases of posterior herniation , neurological symptoms from simple paraesthesia to more severe radiculopathy due to cord compression by the extruded disc fragments [ 5 , 8 , 16 , 26 ] are rather infrequent and not the rule [ 17 , 23 , 24 ]  . 
they are followed in most cases by spontaneous resolution after noninvasive treatment , even in the case of severe and sometimes dramatic radiological findings [ 2 , 7 , 17 , 23 ]  . 
whereas it is uncertain whether trauma can trigger symptoms related to the presence of intervertebral disc calcifications , it is certainly true that a radiological survey of the spine will show the presence of calcifications or herniated disc fragments , but in only symptomatic patients [ 2 , 5 , 16 , 19 , 25 ]  . 
moreover , x - ray is unable to establish the time of appearance [ 1719 ]  . asymptomatic disc calcifications are more frequent in females , at an average presentation age of 4.1 years [ 8 , 17 ]  . they are usually found at the thoracic level and contrary to cervical calcifications that disappear in a relatively short time after discovery tend to persist for a long time before disappearing within the 20th year of life [ 2 , 8 , 16 , 17 , 23 ]  . the real frequency of disc calcifications in children is unknown . 
 [ 7 ] reported 15 cases of which 11 were symptomatic and four were studied for other reasons discovered over a 14 - year time span in the swedish town of ume ( 100 , 000 inhabitants but with no details on the paediatric population )  . 
in caso di erniazione anteriore possibile lassociazione con fenomeni disfagici , dovuti per pi a fatti infiammatori peri - esofagei che non a diretta compressione sullesofago da parte del nucleo erniato [ 4 , 8 , 1416 ]  . 
nelle erniazioni posteriori i sintomi neurologici , dalle semplici parestesie a quadri pi severi [ 5 , 8 , 16 , 26 ] di radicolopatia da compressione midollare per estrusione di frammenti del disco , con compressione sulle radici nervose , sono piuttosto infrequenti e non la regola [ 17 , 23 , 24 ] , avendo quasi sempre risoluzione spontanea con misure terapeutiche non invasive , anche a fronte di quadri radiologici talvolta drammatici [ 2 , 7 , 17 , 23 ]  . 
se non certo che fatti traumatici possano scatenare la sintomatologia legata alla presenza delle calcificazioni dei dischi intervertebrali certo invece che lo studio radiologico del rachide , in occasione di tali evenienze , evidenzier le calcificazioni eventualmente presenti , come certo il possibile riscontro di frammenti erniati nei soli pazienti sintomatici [ 2 , 5 , 16 , 19 , 25 ] non potendosi per stabilire da quanto essi siano presenti [ 1719 ]  . le calcificazioni asintomatiche sono invece localizzate quasi sempre a livello toracico , sono pi frequenti nelle femmine , con et mediana di presentazione sui 4 , 4 anni [ 8 , 17 ] e , a differenza delle cervicali , che tendono a scomparire in tempi relativamente brevi dopo la loro scoperta , persistono per lunghi periodi di tempo , prima di scomparire entro i 20 anni di vita [ 2 , 8 , 16 , 17 , 23 ]  . 
 [ 7 ] segnalano 15 pazienti , di cui 11 con sintomatologia dolorosa e 4 studiati per altri motivi , scoperti in un arco di tempo di 14 anni nella popolazione della citt di ume ( 100000 abitanti , senza precisazione per della componente pediatrica )  . 
nelladulto invece le calcificazioni intervertebrali , localizzate allannulus fibroso , sono di frequente riscontro dopo la quinta decade di vita , con un periodo libero in corrispondenza della terza e quarta e localizzazione in pi spazi intervertebrali nei vari segmenti del rachide , in particolare dorsale inferiore e lombare [ 27 ]  . 
queste calcificazioni , accompagnate da irregolarit delle limitanti , con riduzione degli spazi intersomatici , cui possono corrispondere associate fusioni intersomatiche , sono di solito asintomatiche , permanenti e di scoperta casuale nel corso di indagini radiologiche eseguite per altri motivi e da considerare un fisiologico fenomeno legato allinvecchiamento [ 23 , 27 , 28 ]  . 
 radiol med ( 2009 ) 114 : 331341 intervertebral calcifications at the annulus fibrosus are frequently discovered after the fifth decade of life , with a free period during the third and fourth decades , and are localised at several intervertebral spaces in different parts of the spine , especially at the lower thoracic and lumbar levels [ 27 ]  . 
these calcifications , usually accompanied by vertebral - plate irregularities and possible intervertebral body fusion , are usually asymptomatic , permanent and an incidental finding during radiological procedures : these are thought to represent a physiological consequence of aging [ 23 , 27 , 28 ]  . conclusions it is difficult to evaluate how long calcifications have been present before their incidental discovery or the appearance of pain , and for how long they will remain detectable after their discovery , given that follow - up over time shows their reduction and disappearance [ 2 , 13 , 16 , 17 , 23 ] without being able to demonstrate the time of disappearance . 
disc calcifications tend to disappear faster than the associated vertebral - body changes [ 10 , 17 ]  . acute cases of symptomatic , painful disc calcification , cervical in particular , are followed by disappearance within weeks or even days ( 9 days in one case ) [ 3 ] through a process of fragmentation and progressive reduction in opacity [ 2 , 5 , 6 , 13 , 16 ]  . 
at the thoracic and lumbar levels , calcifications tend to last unchanged for up to 10 years before they resolve spontaneously [ 2 , 7 , 16 ]  . in patients with disc calcifications , especially when symptomatic , it is possible to detect a reduction in intervertebral disc space and a slight flattening of the affected vertebral bodies a long time after their disappearance [ 17 ]  . 
metabolic causes , such as hypervitaminosis d , alcaptonuric hyperparathyroidism , haemochromatosis , ochronosis ( typical of adults , as a long time is necessary before calcified deposits appear ) , are not justified owing to the absence of analogous findings in other organs , whereas inflammatory , microtraumatic or vascular causes are more likely [ 2 , 7 , 21 , 22 ]  . 
 the large blood supply to the intervertebral disc in children and its more active metabolism which is increased in case of inflammation could explain the sudden appearance and disappearance or enlargement of the intervertebral disc calcification in comparison with that seen in adult patients [ 16 , 28 ]  . 
traumatic events may lead to the discovery conclusioni risulta difficile valutare da quanto tempo , prima della scoperta causale o della comparsa della sintomatologia dolorosa , siano gi presenti le calcificazioni e per quanto tempo rimangano poi visibili , in quanto controlli a distanza di tempo ne evidenziano la riduzione e la completa scomparsa [ 2 , 13 , 16 , 17 , 23 ] senza per poterne stabilire con esattezza il momento . 
da tenere ben presente che le calcificazioni scompaiono assai pi rapidamente delle alterazioni dei corpi vertebrali [ 10 , 17 ]  . certo che i casi acuti di calcificazione sintomatica dolorosa , in particolare cervicale , sono seguiti da scomparsa in tempi relativamente rapidi , di poche settimane se non di giorni ( 9 in un caso ) [ 3 ] , attraverso un processo di frammentazione e progressiva riduzione della loro radiopacit [ 2 , 5 , 6 , 13 , 16 ] , mentre a livello dorsale le calcificazioni tendono a permanere immodificate anche per lunghi periodi di tempo ( fino a 10 anni ) prima della scomparsa [ 2 , 7 , 16 ]  . nei soggetti in cui sono presenti le calcificazioni discali , in particolare quelle sintomatiche , sono osservabili a distanza di tempo dalla loro scomparsa fenomeni di riduzione dello spazio discale e relativo appiattimento dei corpi vertebrali interessati [ 17 ]  . 
cause metaboliche come lipervitaminosi d , liperparatiroidismo , la pseudogotta , lemocromatosi , locronosi alcaptonurica ( nelladulto in quanto richiede tempi molto lunghi prima che si giunga allosservazione dei depositi calcifici ) non sono giustificate per lassenza di analoghe localizzazioni in altre sedi , mentre fatti infiammatori , microtraumatici o vascolari sono stati chiamati in causa con forse maggior veridicit [ 2 , 7 , 21 , 22 ]  . sono state anche segnalate associazioni con anomalie congenite , in particolare cardiopatie , cataratte bilaterali , calasia [ 2 ] e sindrome di patau [ 11 ]  . la maggior vascolarizzazione dei dischi intervertebrali nel bambino e di conseguenza il suo pi attivo metabolismo , aumentato in caso di flogosi , potrebbe essere una giustificazione della rapida comparsa e successiva scomparsa od aumento nelle dimensioni delle calcificazioni del disco intervertebrale rispetto a quanto osservabile nelladulto [ 16 , 28 ]  . 
traumatismi sono stati chiamati in causa ( anche se assai difficili da valutare in et pediatrica ) non tanto come evento scatenante il meccanismo che sta alla base della formazione delle calcificazioni , quanto come elemento che permette la dimostrazione delle stesse . attualmente lipotesi della natura vascolare della lesione sembra essere la pi seguita , in particolare se in 340 radiol med ( 2009 ) 114 : 331341 of calcifications , but they are very difficult to evaluate in paediatric patients . 
 the most popular hypothesis is that the lesion has a vascular nature , particularly when in association with perinatal lesions , as shown by the rare cases of disc calcification found at birth [ 2 , 11 , 16 , 22 ]  . 
none of these hypotheses is in any case supported by real evidence . with the exception of the rare cases of anterior disc protrusion with associated dysphagia [ 8 , 13 , 1517 ] or posterior protrusion with slight [ 22 ] or evident spinal cord compression necessitating a surgical procedure [ 8 , 13 , 16 , 20 ] , intervertebral disc calcification is a benign and selflimiting disorder , which resolves with bed rest , analgesics , muscle - relaxing and anti - inflammatory medication without any need for invasive surgical procedures [ 2 , 16 , 17 , 2224 ]  . it is noteworthy that even in our small patient series ( three females and three males ) , there was only one case of symptomatic painful disc localised at the cervical level and that single or multiple , mostly thoracic , disc calcifications were detected during x - ray procedures performed for different reasons in asymptomatic patients . 
it is also interesting that calcifications were discovered in a newborn patient ( one of the few in the literature [ 2 , 11 ] ) affected by patau syndrome . we conclude with a citation from melnick that intervertebral disc calcification in children appears to be a selflimited disease and requires only symptomatic treatment and as stressed also by dias et al . 
seldom requires an operation [ 17 ]  . associazione con lesioni perinatali , come dimostrato dai rari casi di riscontro delle calcificazioni alla nascita [ 2 , 11 , 16 , 22 ]  . 
nessuna per di queste ipotesi corroborata da riscontri certi per la corretta spiegazione delle cause di questa affezione che rimane perci misteriosa riguardo ai suoi meccanismi scatenanti . salvo i rari casi di protrusione anteriore con associata disfagia [ 8 , 13 , 1517 ] o posteriore con compressione lieve [ 22 ] o significativa del midollo in cui stato necessario lintervento chirurgico [ 8 , 13 , 16 , 20 ] , la prognosi della affezione , che da considerarsi autolimitante , benigna con ritorno a condizioni di normalit con il riposo , farmaci miorilassanti ed antiflogistici senza che sia necessario il ricorso ad interventi pi cruenti [ 2 , 16 , 17 , 2224 ]  . significativa nella nostra casistica , anche se basata su soli 6 casi ( 3 femmine e 3 maschi ) , la presenza in un solo caso dei sintomi acuti tipici della localizzazione cervicale ed invece il riscontro di localizzazioni dorsali , singole od interessanti pi dischi intervertebrali , avvenuto in modo del tutto fortuito , in occasione di indagini radiologiche eseguite per altri motivi , in assenza di sintomatologia dolorosa . significativo invece il riscontro delle calcificazioni nel paziente in et neonatale , affetto da sindrome di patau , uno dei pochi casi segnalati in tale et [ 2 , 11 ]  . 
 possiamo concludere con laffermazione di melnick che nei bambini la calcificazione del disco intervertebrale pu essere considerata come una malattia autolimitantesi e che richiede solo terapia sintomatica e che , come sottolineato da dias et al . 
catalano , corso vittorio emanuele 89 bis , 80121 napoli , italy , tel . : + 39 - 081 - 7612417 , fax : + 39 - 081 - 5903689 , e - mail : orlandcat@tin.it received : 2 february 2008 / accepted : 6 march 2008 / published online : 12 december 2008 springer - verlag 2009 abstract purpose . 
il contenuto cistico appariva limpido in 6 papillomi e nelliperplasia duttale atipica e a fini echi in 2 papillomi ; nei carcinomi il contenuto era sotto forma di grossolani echi in 2 casi e di fini echi in 11 . 
calcificazioni intralesionali erano rilevabili 254 radiol med ( 2009 ) 114 : 253266 coarse echoes in two cases and fine echoes in 11 . intralesional calcifications were seen in three carcinomas . posterior enhancement was present in all carcinomas , whereas none showed posterior shadowing . 
leco - color doppler dimostrava assenza di flusso in 4 papillomi e segnali modesti in 4 papillomi e nelliperplasia duttale atipica ; i 13 carcinomi mostravano tutti segnali vascolari diffusi , con multipli vasi sparsi e da multipli poli vascolari . 
gli indici resistivi , misurabili in 4 / 8 papillomi , erano in media di 0 , 43 ; nei carcinomi lo studio flussimetrico era sempre possibile , con indice resistivo medio di 0 , 71 . 
i tumori mammari intracistici presentano aspetti ecostrutturali ed eco - color doppler peculiari , tali da consentire unefficace differenziazione rispetto alle cisti non tumorali ; spesso ipotizzabile una differenziazione tra papillomi e carcinomi . 
la presenza di vascolarizzazione pone invece lindicazione allescissione oppure alla biopsia dei gettoni solidi , anche quando lanalisi citologica risultata negativa . parole chiave mammella ecografia tumore intracistico carcinoma papillare introduction introduzione cystic lesions of the breast are a very common finding , especially in middle - aged women , being detected in one in four women aged 3550 years [ 1 ]  . 
a variety of breast disorders may exhibit a cystic appearance , at least in a number of cases , in a portion of the lesion and / or in a specific stage of their evolution : haematoma , abscess , plasma - cell mastitis , seroma , galactocele , lymphocele , fat necrosis ( lipid cyst ) , angioma , lymphangioma , aneurysm , arteriovenous malformation , fibroadenoma ( 3% of cases ) , phyllodes tumour , fibrocystic change , atypical ductal hyperplasia , papilloma ( with or without atypia ) and carcinoma [ 24 ]  . 
possible malignancies with cystic appearance include ductal carcinoma in situ and infiltrating ductal carcinoma , papillary carcinoma in situ and infiltrating papillary carcinoma , invasive lobular carcinoma , medullary carcinoma , squamous cell carcinoma and hypersecreting ductal adenocarcinoma [ 3 , 5 ]  . 
 on ultrasound ( us ) imaging , complicated or dirty cysts are defined as cystic masses characterised by mild posterior enhancement or multiple homogeneous internal low - level echoes but are otherwise identical to simple cysts . 
numerose lesioni possono avere , almeno in una parte dei casi , in maniera parziale e / o in una determinata fase della loro evoluzione , un aspetto similcistico , ematoma , ascesso , mastite plasmacellulare , sieroma , galattocele , linfocele , steatonecrosi ( cisti oleosa ) , angioma , linfangioma , aneurisma , malformazione artero - venosa , fibroadenoma ( 3% dei casi ) , tumore filloide , modifiche fibrocistiche , iperplasia duttale atipica , papilloma ( con o senza atipia ) , carcinoma [ 24 ]  . 
nellambito dei possibili carcinomi cistici , bisogna ricordare innanzitutto quello duttale in situ e infiltrante e quello papillare in situ e infiltrante , poi quelli lobulare infiltrante , midollare , squamoso nonch ladenocarcinoma duttale ipersecernente [ 3 , 5 ]  . 
 dal punto di vista ecografico , vengono definite complicate o sporche quelle formazioni cistiche , altrimenti semplici , ma caratterizzate da un rinforzo di parete posteriore poco evidente oppure da multipli e omogenei echi interni di basso livello , eventualmente mobili ( come dimostrabile anche con lm - mode , con leco - color doppler radiol med ( 2009 ) 114 : 253266 demonstrated by m - mode us , colour doppler us or vocal fremitus combined with doppler techniques )  . 
complex or partially solid cysts , in contrast , show some evidence of echostructural atypia , such as mural projections , thick septa ( > 0.4 mm ) or thick ( > 0.4 mm ) and irregular walls . 
 [ 2 ] distinguished among four types of complex cysts : cysts with thick walls ; cysts with one or more intracystic solid masses ; cysts with mixed solid and cystic components ( > 50% cystic ) ; cysts with mixed solid and cystic components ( > 50% solid with eccentric cystic foci )  . 
 [ 6 ] recently developed a broader classification covering all forms of cystic breast lesions , whihs was also based on sonographic morphostructural features : type i ( simple cyst ) , anechoic mass with imperceptible circumscribed border and posterior acoustic enhancement ; type ii ( clustered cysts ) , cluster of anechoic formations with no discrete solid component ; type iii ( septated cyst ) , cyst with thin septa ( < 0.5 - mm thick ) ; type iv ( complicated cyst ) , mass with homogeneous low - level echoes or floating debris or with fluid - debris levels ; type v ( complex fluid cyst ) , mass with thick walls or septa ( > 0.5 mm ) or nodules with > 50% fluid component ; type vi ( complex solid cyst ) , mass with < 50% fluid component , essentially solid , with eccentric cystic foci corresponding to dilated ducts , acini or necrosis . 
types v and vi are malignant in 26% and 62% of cases , respectively , being possibly related to fibroadenomas , phyllodes tumours or abscesses [ 6 ]  . although the classification systems of berg et al . 
in contrast , we believe angioarchitectural features to be an integral part of any sonographic assessment of breast masses and as such very useful for differentiating between true ( vascular ) intracystic solid projections and their avascular mimickers , and for distinguishing between intracystic papillomas and carcinomas . 
le cisti complesse , anche definite come parzialmente solide , sono invece quelle che mostrano qualche segno di atipia ecostrutturale , come gettoni murali , setti spessi ( > 0 , 4 mm ) o pareti spesse ( > 0 , 4 mm ) e irregolari ; queste cisti , che vanno inquadrate come bi - rads 4 , sono maligne nel 23%31% dei casi [ 2 , 3 ]  . 
 [ 2 ] hanno distinto le cisti complesse in quattro tipologie : cisti a parete spessa ; cisti con una o pi formazioni solide endocistiche ; cisti con quote solide e cistiche miste ( con queste ultime > 50% ) ; cisti con quote solide e cistiche miste ( con le prime > 50% e le seconde riconoscibili sottoforma di foci eccentrici )  . 
 [ 6 ] hanno recentemente pubblicato una pi ampia classificazione comprensiva di tutte le formazioni cistiche mammarie , sempre basata sui soli aspetti ecografici morfostrutturali : tipo i ( cisti semplice ) , formazione anecogena con bordo impercettibile e circoscritto e con rinforzo posteriore ; tipo ii ( cisti a grappolo ) , formazione anecogena a grappolo senza componenti solide ; tipo iii ( cisti settata ) , formazione con setti sottili ( < 0 , 5 mm di spessore ) ; tipo iv ( cisti complicata ) , formazione con echi omogenei di basso livello o con detriti galleggianti o con livello liquido - detriti ; tipo v ( cisti complessa liquida ) , formazione con pareti o setti spessi ( > 0 , 5 mm ) o con noduli ma comunque con componente liquida > 50% ; tipo vi ( cisti complessa solida ) , formazione con componente liquida < 50% , essenzialmente solida con foci cistici eccentrici , corrispondenti a dotti dilatati , acini o necrosi . 
i tipi da i a iv sono risultati sempre benigni , con il pattern iv spesso corrisponde ad ascessi ; i tipi v e vi sono maligni rispettivamente nel 26% e 62% dei casi , potendo anche essere espressione di fibroadenomi , tumori filloidi , ascessi [ 6 ]  . sebbene i sistemi classificativi di berg et al . 
nostro giudizio invece che i reperti angioarchitettonici , parte integrante di qualsiasi valutazione ecografica di una formazione mammaria , siano molto utili , sia per unimmediata distinzione tra i gettoni solidi endocistici , con segnali di flusso , ed i loro simulatori , avascolari , che per una distinzione , entro determinati limiti , tra papillomi e carcinomi intracistici . 
lo scopo del presente lavoro stato pertanto di valutare lapporto delle tecniche doppler nella diagnostica differenziale e nellinquadramento dei tumori intracistici della mammella . 256 radiol med ( 2009 ) 114 : 253266 cystic breast masses corresponding to type iv , v or vi cysts according to the chang classification [ 6 ] , with the exclusion of type vi predominantly solid cysts with eccentric cystic foci . 
selected patients were 45 women ( one case of male breast cancer was excluded ) aged 3187 years ( mean 59 ) , each with a single complicated / complex cyst . 
 us examinations were conducted on a technos mpx unit ( esaote , genoa , italy ) equipped with a broadband linear - array transducer ( 5.512.5 mhz , generally used at 10 mhz )  . 
a single focus was placed at the level of the deep aspect of the mass being examined . the gain curve was adjusted to the depth of the lesion , attempting to avoid intracystic artefactual images . 
during the scan , the cystic mass was compressed with the transducer and explored with partial changes in patient position . very superficial masses were scanned with the aid of a gel standoff pad . angioarchitecture was studied with colour doppler , in particular , power doppler ( with directional coding ) , with settings allowing maximal sensitivity to slow flows : pulse repetition frequency 750 hz ; low wall filter ( 50 hz ) ; colour gain just below the threshold for artefacts ; colour box restricted to the region of interest . 
emission frequency for colour and power doppler was adjusted to lesion depth : 7.1 mhz for superficial lesions ; 6.3 mhz for intermediate lesions ; 5.6 mhz for deep lesions . 
care was taken not to apply excessive compression with the transducer during the doppler study . evaluation of the us examinations was retrospective and based on video clips acquired with the us unit and transferred via a local network to a personal computer . maximum diameter and maximum diameter perpendicular to the first diameter of both the cystic lesion and any major intracystic projections were measured : the ratio of solid ( or pseudosolid ) to fluid component was defined as < 50% , 50% and > 50% . 
orientation of the mass relative to the cutaneous plane was classified as parallel ( if the long axis was parallel to the skin ) or antiparallel ( if the short axis was parallel to the skin )  . 
echogenicity of the fluid materiali e metodi tra gennaio e dicembre 2006 abbiamo selezionato prospetticamente le pazienti con riscontro ecografico di una o pi formazioni cistiche della mammella assimilabili ai tipi iv , v o vi secondo chang et al . 
i casi selezionati erano costituiti da 45 donne ( un caso di carcinoma maschile veniva escluso ) , di 3187 anni ( media 59 ) , ciascuna con una singola cisti complicata / complessa . 
 gli esami venivano condotti con ecografo technos mpx ( esaote , genova , italia ) equipaggiato con sonda lineare a larga banda ( escursione da 5 , 5 a 12 , 5 mhz , con impiego generalmente a 10 mhz )  . 
per formazioni particolarmente superficiali si ricorreva anche allimpiego di un cuscinetto distanziatore in gelatina . lo studio angio - architettonico veniva praticato con ecocolor doppler e soprattutto con power doppler ( in modalit con codifica direzionale ) , utilizzando dei parametri di studio tali da massimizzare la sensibilit ai flussi lenti : frequenza di ripetizione dellimpulso di 750 hz , filtro di parete al minimo ( low , pari a 50 hz ) , guadagno del colore subito al di sotto della soglia degli artefatti , box del colore ristretto sullarea di interesse . 
la frequenza di emissione per il color e power doppler veniva correlata alla profondit della lesione : 7 , 1 mhz per lesioni superficiali , 6 , 3 mhz per quelle a media profondit e 5 , 6 mhz per quelle pi profonde . 
quando possibile si campionava lo spettro flussimetrico doppler , ottenuto a livello del vaso intralesionale di calibro maggiore e con il flusso pi vivace allosservazione color doppler ; in caso di campionamenti su pi poli vascolari si prendeva in considerazione lo spettro pi pulito e che mostrasse i valori pi estremi , in senso benigno o maligno , dellindice resistivo . 
loperatore aveva cura di evitare una compressione eccessiva con la sonda durante lo studio doppler . la valutazione degli esami ecografici stata retrospettiva , basata sui filmati acquisiti sullecografo ed inviati via rete ad un personal computer . 
veniva misurato il diametro massimo ed il massimo diametro ad esso perpendicolare , sia della lesione cistica che delle eventuali proiezioni solide radiol med ( 2009 ) 114 : 253266 component was classified as homogenously anechoic , inhomogeneously anechoic with fine internal echoes , inhomogeneously anechoic with coarse internal echoes and hypoechoic . 
note was taken of the presence of thick walls ( > 0.5 mm ) , thick septa ( > 0.5 mm ) or solid papillary projections . solid projections were defined as single or multiple and hypoechoic or hyperechoic . 
finally , cysts were assessed for the presence of calcification in the solid component , posterior acoustic enhancement , posterior shadowing and solid satellite nodules . assessment parameters on colour doppler us were presence or absence of flow signal in the wall / septa or solid projections , number of vascular poles ( single or multiple ) , extent of flow ( few isolated signals , moderate diffuse vascularity or abundant diffuse vascularity )  . 
an on - site cytologist provided immediate evaluation , and only in equivocal cases was a core biopsy of the solid component obtained with an automated biopsy gun and 14 - gauge needles . results twenty - three nontumoural masses were treated conservatively , and the diagnosis was confirmed by follow - up ; three symptomatic large masses were aspirated for therapeutic purposes . 
lorientamento della formazione rispetto al piano cutaneo veniva catalogato come parallelo ( se il maggior asse lesionale parallelo alla cute ) o antiparallelo ( se il minior asse lesionale parallelo alla cute )  . 
la reflessivit della quota liquida veniva distinta in anecogena omogenea , anecogena disomogenea con echi interni fini , anecogena disomogenea con echi interni grossolani , presenza di pareti spesse ( > 0 , 5 mm ) , setti spessi ( > 0 , 5 mm ) o proiezioni papillari solide ; questi gettoni solidi venivano distinti in singoli e multipli ed in ipoecogeni e iperecogeni . veniva infine valutata la presenza di calcificazioni nelle quote solide , di rinforzo di parete posteriore e di attenuazione posteriore del fascio , nonch di noduli solidi satelliti . come parametri color - power doppler venivano definiti : presenza / assenza di segnali di flusso in pareti / setti o gettoni solidi , numero di poli vascolari ( singolo o multipli ) , entit ipoecogena . 
assenza di segnali di flusso sia a livello delle pareti che della quota ecogena luminale . 258 radiol med ( 2009 ) 114 : 253266 table 1 morphostructural , angioarchitectural and spectral findings in 45 patients with complicated / complex breast cyst findings features nontumoural lesions ( n = 23 ) papilloma ( n = 8 ) atypical ductal hyperplasia ( n = 1 ) carcinoma ( n = 13 ) maximum diameter ( mm ) 931 ( mean 18 ) 413 ( mean 8 ) 922 ( mean 13 ) orientation solid / fluid component shape margins fluid portion walls septa parallel antiparallel < 50% > 50% round oval oblong lobulated irregular welldefined illdefined homogeneously anechoic anechoic with fine echoes anechoic with coarse echoes hypoechoic thin ( 5 mm ) thick ( > 0.5 mm ) absent thin ( 5 mm ) thick ( > 0.5 mm ) absent present and hypoechoic present and hyperechoic papillary projections calcifications posterior enhancement absent present shadowing satellite solid nodules absent present absent present absent present septal or nodular signals absent present no . 
in the papillomas , del flusso ( qualche segnale isolato , discreta vascolarizzazione diffusa oppure cospicua vascolarizzazione diffusa )  . lanalisi spettrale , quando ottenibile , veniva utilizzata per calcolare lindice resistivo . 
 i prelievi citologici di conferma venivano effettuati con radiol med ( 2009 ) 114 : 253266 tabella 1 reperti morfo - strutturali , angio - architettonici e flussimetrici in 45 pazienti con cisti mammaria complicata / complessa reperti possibilit lesione non tumorale ( n = 23 ) papilloma ( n = 8 ) iperplasia duttale atipica ( n = 1 ) carcinoma ( n = 13 ) diametro massimo in mm 931 ( media 18 ) 413 ( media 8 ) 922 ( media 13 ) orientamento quota solida / liquida forma margini quota liquida pareti setti proiezioni papillari parallelo antiparallelo < 50% > 50% rotondeggiante ovalare allungata polilobulati irregolare netti e regolari mal definiti anecogena omogenea anecogena con echi fini anecogena con echi grossolani ipoecogena sottili ( 5 mm ) spesse ( > 0 , 5 mm ) assenti sottili ( 5 mm ) spessi ( > 0 , 5 mm ) assenti presenti e ipoecogene presenti e iperecogene calcificazioni rinforzo posteriore attenuazione del fascio noduli solidi satelliti assenti presenti assente presente assente presente assenti presenti segnali in setti o gettoni assenti presenti numero di poli vascolari singolo vascolarizzazione indice resistivo mmultipli qualche segnale isolato discreta e diffusa cospicua e diffusa 0 , 330 , 58 ( media 0 , 43 ) 0 , 550 , 77 ( media 0 , 71 ) colour doppler us detected no flow signals in four cases and moderate flow signals in the remaining four cases , as well as in the atypical ductal hyperplasia . 
il materiale aspirato veniva poi strisciato su vetrino , lasciato asciugare allaria e sottoposto a colorazione rapida secondo may - grnwald - giemsa 260 radiol med ( 2009 ) 114 : 253266 flow , with diffuse vascularity characterised by multiple scattered vessels or multiple vascular poles emerging from the base of the papillary projections . 
2 papilloma intracistico , immagine con power doppler direzionale ( modalit dual )  . piccola formazione ( freccia ) aggettante nel lume di una cisti uniloculata , per il resto a contenuto omogeneo . 
assenza di segnali di flusso sia nelle pareti cistiche che nellaggetto . risultati ventitre formazioni cistiche non tumorali venivano trattate conservativamente e la diagnosi veniva confermata dal follow - up ; 3 venivano aspirate a scopo soprattutto terapeutico , perch voluminose o sintomatiche . 
il contenuto cistico appariva limpido in 6 papillomi e nelliperplasia duttale atipica ed a fini echi sparsi in 2 papillomi ; nei carcinomi il contenuto era sotto forma di grossolani echi di basso livello in 2 casi e di fini echi sparsi nei restanti 11 casi . 
nei papillomi leco - color doppler dimostrava assenza di segnali di flusso in 4 casi e modesti segnali vascolari nei rimanenti 4 papillomi nonch nelliperplasia duttale atipica , sottoforma di un singolo peduncolo vascolare centrale o di qualche segnale sparso . 
tutti i 13 carcinomi mostravano invece segni di flusso intralesionale , con una vascolarizzazione diffusa , caratterizzata da multipli vasi sparsi e da multipli poli vascolari emergenti alla base delle proiezioni papillari . 
the smaller one is anterior and with a single flow signal internally ( single arrow in a ) , whereas the other is deeper and larger ( arrows in a )  . 
5a - c carcinoma papillare intracistico , immagini con power doppler direzionale ( a ) , con ago per biopsia ( b ) e dopo svuotamento ( c )  . 
al suo interno aggettano due formazioni solide , una pi piccola e anteriore con singolo segnale di flusso allinterno ( freccia singola in a ) ed una pi profonda e voluminosa ( frecce in a )  . 
in una serie di 1805 pazienti sottoposte ad esame ecografico , questa patologia veniva rilevata in 20 casi ( 1 , 1% ) tra cui solo 6 di tipo maligno [ 10 ]  . 
i carcinomi intracistici ( 0 , 3%2% dei cancri mammari nel sesso femminile ) sono generalmente del tipo papillare ed in questo caso insorgono in donne di et medio - avanzata ( media 65 anni ) , presentando una crescita lenta e una bassa frequenza di metastasi linfonodali alla presentazione , con buona prognosi ( in assenza di chiara diffusione extracistica ) [ 4 , 5 , 11 , 12 ]  . data lorigine duttale , i carcinomi papillari si localizzano soprattutto nelle regioni retroareolari ( almeno nel 50% dei casi ) : essi si formano infatti per dilatazione cistica di un assessment was possible in all carcinomas , where it yielded a mean resistive index of 0.71. 
owing to their ductal origin , papillary carcinomas tend to develop in the retroareolar regions ( in at least 50% of cases ) , where they form as a result of cystic dilatation of a duct around a solid vegetation that obstructs it . 
alternatively , they may present with bloody nipple discharge ( 22%34% of cases ) [ 14 ] or , in the case of internal haemorrhage , with rapid enlargement of the mass that may become tender . 
bleeding may be spontaneous and essentially related to torsion and infarction of the papillary projections or it may be induced by the diagnostic needle puncture itself [ 13 , 14 ]  . 
solid papillary tumours are rare ( four invasive papillary carcinomas in a series of 940 invasive breast carcinomas studied with mammography [ 15 ] ) and generally invasive and have an nonspecific sonographic pattern consisting of single or multiple lobular nodules with welldefined margins , relatively homogeneous hypoechoic echostructure and possible posterior enhancement [ 13 , 14 , 16 , 17 ]  . 
possible papillary projections tend radiol med ( 2009 ) 114 : 253266 dotto intorno ad una vegetazione solida che ne determina lostruzione ; in genere la vegetazione nasce come papilloma , per poi trasformarsi [ 4 , 13 ]  . quando voluminosi , i tumori intracistici possono manifestarsi come tumefazioni palpabili indolenti . 
in alternativa si pu avere una secrezione ematica dal capezzolo ( 22%34% dei casi [ 14 ] ) oppure , per unemorragia interna , un rapido ingrandimento della formazione che diviene anche dolente ; in un caso [ 5 ] la presentazione era sottoforma di cisti emorragiche multiple , insorte dopo un trauma , ma ricorrenti . 
il sanguinamento pu essere spontaneo , determinato essenzialmente dalla torsione e infarto dei gettoni papillari , o pu essere indotto dalla stessa puntura diagnostica [ 13 , 14 ]  . 
 lelemento istologico distintivo di tutti i tumori papillari dato dalla presenza di uno stroma fibrovascolare arborizzante , che supporta la componente epiteliale ; nelle forme carcinomatose si rileva una scarsit o una virtuale assenza dello strato mioepiteliale [ 13 , 14 ]  . 
quelli solidi , rari ( 4 carcinomi papillari invasivi su una casistica di 940 carcinomi mammari invasivi studiati con xeromammografia [ 15 ] ) e generalmente invasivi , hanno un aspetto ecografico aspecifico , sottoforma di noduli singoli o multipli , di forma lobulata , con margini definiti , a struttura ipoecogena relativamente omogenea , con eventuale rinforzo posteriore [ 13 , 14 , 16 , 17 ]  . 
i tumori papillari intraduttali e soprattutto intracistici sono di solito in situ , anche se la quota solida spesso cospicua al momento della diagnosi [ 6 ] ; la diffusione degli eventuali elementi invasivi viene in parte ostacolata dallo strato fibroso parietale [ 14 ]  . 
queste lesioni presentano un aspetto ecografico caratteristico , come formazioni cistiche ovalari , a margini netti , con rinforzo posteriore generalmente presente ( di solito da lieve a moderato )  . 
le cisti mostrano allinterno un contenuto liquido leggermente disomogeneo , con echi spesso di variabile diametro , e dei setti pi o meno polimorfi ; le eventuali proiezioni papillari hanno generalmente una morfologia semilunare , con possibili calcificazioni interne e con base di impianto sessile [ 14 , 18 , 19 ]  . 
in alcuni dei casi personali si osservavano una o pi piccole nodulazioni solide satelliti al carcinoma intracistico e ci conferma il dato della letteratura di un possibile riscontro di foci di carcinoma intraduttale adiacenti ai carcinomi papillari intracistici [ 14 ]  . i carcinomi intracistici vanno quindi distinti dai semplici papillomi , dai tumori solidi di alto grado con ampia necrosi , emorragia e colliquazione centrale , dai tumori maligni che abbiano infiltrato una cisti pre - esistente e dai coaguli ematici adesi alla parete delle cisti ( anche dopo cisticentesi ma in questultimo caso lanamnesi fondamentale ) [ 4 , 6 , 20 ]  . 
per dimostrare leffettiva natura della proiezione papillare , e distinguerla da semplice materiale ecogeno adeso alla parete cistica , possibile ricorrente alla radiol med ( 2009 ) 114 : 253266 to be crescent - shaped with internal calcifications and a sessile base [ 14 , 18 , 19 ]  . 
several cases in our series showed one or more small solid satellite nodules , which confirms previous reports on the possibility of identifying foci of intraductal carcinoma adjacent to intracystic papillary carcinomas [ 14 ]  . intracystic carcinomas thus need to be distinguished from simple papillomas ; from high - grade solid tumours with extensive central necrosis , haemorrhage and colliquation ; from malignant tumours invading a preexisting cyst and from blood clots adhering to the cyst walls ( even after cyst aspiration , although in this case , the patients history is fundamental ) [ 4 , 6 , 20 ]  . 
techniques that help to demonstrate the true nature of the papillary projection and distinguish it from echoic material adhering to the cyst wall include graded compression , changes in patient position , vocal fremitus on power doppler or flow signal detection with doppler techniques [ 3 , 7 ]  . 
detection of nonartefactual colour signals provides a simple and immediate means to demonstrate the solid nature of echoic luminal projections . however , even on the basis of our experience , whereas the presence of colour signals demonstrates the solid nature of the projecting structure , its absence does not exclude , it as it is impossible to adequately differentiate between adhering debris and solid projections [ 3 ]  . 
similarly , the presence of flow on doppler analysis is alone insufficient to discriminate papillomas from carcinomas , even though the signals are few or absent in papillomas and substantially more intense and diffuse in carcinomas . 
 [ 18 ] , power doppler demonstrated regular , nonanarchic vascularity with a single afferent vessel , suggesting a presumptive diagnosis of benignity , whereas histological examination subsequently revealed a papillary carcinoma . in early studies on intracystic tumours , us was reported to have had limited accuracy in diagnosing malignancy [ 10 ]  . in reality , even with modern sonographic equipment , the malignant nature of an intracystic projection cannot be definitely excluded or demonstrated . 
although the presence of vascular signals in an intracystic projection increases the level of suspicion of malignancy ( though benign intracystic projections may also demonstrate internal vessels , generally with low resistive index ) , in fact , all complex cysts should be aspirated and evaluated by cytology . 
it should also be noted that particularly large and / or fast - growing carcinomas may be massively necrotic and thus mimic a dirty cyst or an abscess : demonstration of flow signals at colour doppler us may be diagnostic in such cases [ 1 , 21 ]  . the classic elements for the differential diagnosis of breast nodules were not applicable in our series because all nontumoural lesions , papillomas and carcinomas constantly compressione dosata , alla variazione di decubito , al fremito vocale con power doppler oppure alla dimostrazione di segnali di flusso con tecniche doppler [ 3 , 7 ]  . 
quindi chiaro che , anche in base alla nostra esperienza , la presenza di segnali di colore dimostra la natura solida dellaggetto mentre la loro assenza non la esclude , non potendosi in questultimo caso porre un adeguata differenziazione tra detriti adesi e gettoni solidi [ 3 ]  . 
 inoltre chiaro che la sola presenza di flussi allanalisi doppler non sufficiente da sola per discriminare con certezza papilloma e carcinoma , anche se nel primo caso si osservano segnali scarsi , quando non assenti , mentre nel carcinoma la vascolarizzazione molto pi intensa e diffusa . 
 [ 18 ] il power doppler dimostrava una vascolarizzazione regolare , non anarchica , con singolo polo afferente , reperti tali da suggerire unipotesi di benignit , laddove poi lesame istologico avrebbe dimostrato un carcinoma papillare . nelle prime casistiche sui tumori intracistici lecografia presentava una limitata accuratezza nella diagnosi di malignit [ 10 ]  . 
sebbene la presenza di segnali vascolari in un gettone intracistico renda maggiore il sospetto di malignit ( quantunque anche le vegetazioni intracistiche benigne possono mostrare vasi interni , generalmente con spettro a basso indice resistivo ) , in realt tutte le cisti complesse andrebbero aspirate e sottoposte a valutazione citologica ; in caso di svuotamento incompleto dopo aspirazione poi spesso indicata una biopsia microistologica del residuo . 
bisogna anche ricordare come alcuni carcinomi , particolarmente voluminosi e / o a rapida crescita , possano essere massicciamente necrotici e simulare pertanto una cisti sporca o un ascesso : la dimostrazione di qualche segnale di flusso alleco - color doppler pu essere dirimente [ 1 , 21 ]  . gli elementi classici della diagnostica - differenziale del nodulo mammario sono poco applicabili , poich sia le lesioni non tumorali , che i papillomi che i carcinomi presentavano nella nostra casistica , in maniera costante o pressoch costante , la riconoscibilit di un rinforzo posteriore ( e lassenza di unattenuazione del fascio ) e la presenza di forma rotondeggiante - ovalare , di margini netti e regolari e di disposizione parallela rispetto al piano cutaneo . 
la natura invasiva del tumore intracistico pu essere sospettata soprattutto quando la base dei gettoni endocistici appare irregolare con strie ipoecogene penetranti nel parenchima adiacente , quando si osservano piccoli noduli solidi satelliti e , chiaramente , in presenza di localizzazioni linfonodali ascellari . 
a questo proposito , bisogna segnalare come la biopsia sia spesso limitata , 264 radiol med ( 2009 ) 114 : 253266 or almost constantly showed posterior enhancement ( and absent posterior shadowing ) , a rounded - oval shape , sharp regular margins and orientation parallel to the cutaneous plane . 
the invasive nature of an intracystic tumour may be suspected , particularly when the base of the intracystic projections appears irregular and with hypoechoic bands penetrating the adjacent parenchyma , when small satellite nodules are seen and , clearly , in the presence of axillary nodal metastases . 
on this subject , it should be noted that biopsy is often limited , as it is often performed on the largest portion of the intracystic solid component and not at the periphery where the invasive elements would be detected [ 5 , 13 ]  . 
in many cases , only evaluation of the entire surgical specimen enables a definitive distinction between benign and malignant papillary forms , as the foci of malignant degeneration are interspersed with benign papillary elements [ 18 ]  . high - resolution us , now also with harmonic imaging [ 22 ] and spatial compounding technology [ 20 ] , no doubt allows effective morphostructural assessment of breast cysts , enabling differentiation of the various types . 
the septa and solid projections of intracystic tumours show fairly large vessels at histological examination [ 14 ] , which explains the significant flow signals detected in the majority of lesions in our patients . 
if our experience is confirmed on larger series , diagnostic sampling of type iv and v cysts according to chang can be foregone and the lesion merely followed up whenever colour doppler us does not depict flow signals ( which is always the case in type iv cysts )  . 
in type vi cysts , however , where flow signals are constantly present , a pattern of diffuse hypervascularity on colour doppler us should constitute an indication for surgical excision or core biopsy ( also vacuum - assisted ) , even in the case of negative cytological examination . 
this finding does not , however , necessarily indicate malignancy , nor does a different appearance allow carcinoma to be ruled out : sonographic suspicion must lead to excision , even in the presence of negative cytological findings [ 5 , 11 ]  . 
aspiration of bloody fluid from a cyst dictates cytological evaluation of the aspirate [ 9 ] , which some authors reserve for cysts with haemorrhagic content only [ 2 ]  . 
further investigation may also be advisable for cysts , including those with simple appearance , which are not completely emptied with aspiration or which form again rapidly [ 5 ]  . 
in the case of complex cysts , however , cytological evaluation of the aspirate is considered to be poorly accurate : normally , it is recommended to perform a core biopsy , or vacuum - assisted biopsy , of the residual solid material , as only biopsy is considered capable of consistently excluding the risk of malignancy [ 3 , 4 , 6 ]  . poich viene condotta verso la parte pi ampia della quota solida endocistica e non verso la periferia ove si rileverebbe il carattere invasivo [ 5 , 13 ]  . 
in molti casi solo la valutazione dellintero pezzo operatorio asportato consente una distinzione finale tra forme papillari benigne e maligne , poich non di rado i foci degenerativi sono frammisti agli aspetti papillari benigni [ 18 ]  . lo studio ecografico ad alta risoluzione , anche grazie alle attuali possibilit tecnologiche derivanti dallimpiego dellarmonica tissutale [ 22 ] e dal compound spaziale [ 20 ] , consente sicuramente una valida valutazione morfo - strutturale delle cisti mammarie , distinguendone le diverse tipologie . 
i setti ed i gettoni solidi dei tumori intracistici presentano allesame istologico dei vasi di discreto calibro [ 14 ] , cosa che spiega i significativi segnali di flusso rilevati nella nostra casistica nella maggioranza delle lesioni . 
in base allesperienza personale , se confermata anche da casistiche pi ampie , si pu soprassedere dalla puntura diagnostica delle cisti tipo iv e v di chang et al . , limitandosi ad un controllo a distanza di tempo , se lo studio eco - color doppler non dimostra segnali di flusso ( cosa peraltro costante nelle cisti di tipo iv )  . 
nella tipologia vi secondo chang et al . , invece , ove peraltro i segnali di flusso sono risultati sempre presenti , un aspetto di ipervascolarizzazione diffusa allecocolor doppler deve porre unindicazione allescissione chirurgica oppure alla biopsia microistologica ( anche come vacuum - assisted ) , anche quando un eventuale esame citologico sia risultato negativo per cellule maligne . 
 il materiale aspirato dalle cisti complesse generalmente di aspetto ematico , pi o meno scuro , sebbene tale reperto non indichi necessariamente la natura maligna della cisti n , allopposto , un contenuto di aspetto differente permette di escludere il carcinoma : un sospetto ecografico deve condurre allescissione anche dinanzi ad un reperto citologico negativo [ 5 , 11 ]  . 
dinanzi allaspirazione di materiale ematico da una cisti si impone la valutazione citologica dello stesso [ 9 ] , da alcuni limitata proprio alle cisti che dimostrano un contenuto emorragico [ 2 ]  . 
una valutazione pi approfondita pu essere poi consigliabile nel caso di cisti , anche di aspetto semplice , che dopo una cisticentesi non si vuotano completamente o che si riformano rapidamente [ 5 ]  . nel caso delle cisti complesse la citologia su liquido aspirato considerata tuttavia poco accurata : generalmente viene invece consigliata la puntura delle quote solide residue dal prelievo del materiale liquido , con biopsia microistologica o anche con biopsia vacuum - assisted , poich si ritiene che solo la biopsia infatti ritenuta in grado di escludere consistentemente il rischio di malignit [ 3 , 4 , 6 ]  . 
riteniamo radiol med ( 2009 ) 114 : 253266 nonetheless , we prefer to carry out extemporaneous cytological analysis of the material obtained from the solid component and proceed to core biopsy only in doubtful cases . 
indeed , we believe that aspiration of the fluid component for cytological analysis causes decompression of the cyst and possibly extracystic leakage of the fluid component , which may make it more difficult to identify and sample the solid component [ 3 ]  . 
we thus prefer to sample the solid component directly with needle aspiration and only later to sample the fluid portion : if extemporaneous cytological analysis of the solid portion shows no signs of atypia or malignancy , we proceed with core biopsy of the remaining solid portion . 
because needle aspiration of the solid components has generally proved to be sufficient for the diagnosis in our experience , we prefer not to perform a core biopsy first , in contrast to what has been suggested in the literature [ 3 ]  . infatti che , se si esegue in prima istanza laspirazione della quota liquida ai fini dellanalisi citologica , si determina anche una decompressione della formazione cistica , con eventuale diffusione extracistica di liquido , e quindi vi possono essere maggiori difficolt ad identificare ed a campionare adeguatamente le porzioni solide [ 3 ]  . 
noi preferiamo quindi prelevare direttamente , mediante ago - aspirazione , la quota solida e solo in un secondo momento prelevare la parte liquida : qualora lanalisi citologica estemporanea della parte solida non dimostri segni di atipia o malignit , si proceder alla biopsia microistologica della parte solida residuata dalla cisticentesi . 
poich nellesperienza personale lago - aspirato dei gettoni solidi si generalmente dimostrato sufficiente per la diagnosi , preferiamo non eseguire la biopsia microistologica in prima istanza , a differenza di quanto consigliato in letteratura [ 3 ]  . conclusions intracystic breast tumours show distinctive echostructural and colour doppler us features that allow effective differentiation , not only from nontumoural complex cysts but also in many cases between intracystic papillomas and carcinomas . 
the main signs of malignancy detected in our series were elevated solid - to - cystic ratio , multiple solid projections , intralesional calcifications , intense vascularity of the papillary projections , multiple vascular poles and high resistive index of the intralesional vessels . 
the presence of neovascularity represents an indication for surgical excision of the lesion or biopsy of the solid projections , even in the case of negative cytological analysis . conclusioni i tumori mammari intracistici presentano aspetti eco - strutturali ed eco - color doppler peculiari , tali da consentire unefficace differenziazione non solo rispetto alle cisti complesse non tumorali , ma anche , in molti casi , tra papillomi e carcinomi intracistici . 
i maggiori indicatori di malignit sono risultati : elevato rapporto tra quota solida e cistica , multipli gettoni solidi , calcificazioni intralesionali , intensa vascolarizzazione delle proiezioni papillari , multipli poli vascolari , elevate resistenze al flusso in corrispondenza dei vasi intralesionali . 
sartor springer - verlag , berlin heidelberg , 2008 isbn 978 - 3 - 540 - 33004 - 2 this second edition of pediatric uroradiology , edited by fotter of gratz university with the help of a distinguished team , updates all 29 chapters for technical and theoretical changes in paediatric uroradiology that have occurred over the last few years . 
for instance , what was considered dogma in the management of urinary tract infections and vesicoureteral reflux is amply discussed and debated after presenting new sometimes contradictory knowledge and different opinions by leaders in the field . due to these new clinical findings , it will be necessary to re - evaluate procedures and conduct and implement the suggestions and recommendations found throughout the book . in particular , careful attention should be given to the chapter clinical management of common nephrourologic disorders ( guidelines and beyond )  . 
new insights are provided on how to manage prenatally diagnosed congenital uropathies , how to deal with the case of renal hypertension , how to use nuclear medicine and be spering in voiding cystourethrography , how to study renal tumours and how to say goodbye to intravenous urography . 
as in the first edition , emphasis is placed on voiding dysfunction due to either nonneurogenic or neurogenic bladder sphincter dysfunction . the number of pages has been increased from 431 in the first to 533 in the second edition and the number of chapters from 26 to 29 . 
fotter delluniversit di graz che ha coordinato un gruppo di esperti nella materia , porta alla luce nei suoi 29 capitoli tutti i cambiamenti , non solo tecnici , ma soprattutto teorici , avvenuti nel campo delluroradiologia pediatrica nel corso degli ultimi anni . 
quanto ritenuto per esempio un dogma nel trattamento delle infezioni delle vie urinarie e del reflusso vescico - ureterale viene ampiamente dibattuto alla luce delle recenti e talvolta contraddittorie acquisizioni , esponendo differenti opinioni e effettuando una discussione in merito , da parte di importanti cultori della materia . 
a causa di queste recenti acquisizioni dal punto di vista clinico sar necessario prendere in considerazione la rivalutazione di condotte e procedure ed adeguarsi ai suggerimenti presenti nel volume , soprattutto meditando con attenzione quanto scritto nel capitolo dal titolo : clinical management of common nephrourologic disorders ( guidelines and beyond )  . 
nuove indicazioni e suggerimenti vengono dati su come comportarsi in caso di uropatie riscontrate in utero ; come comportarsi in caso di ipertensione ; come utilizzare la medicina nucleare ed essere avari nellesecuzione di cistouretrografie ; come studiare i tumori renali ecc . 
viene data importanza , come nel volume della prima edizione alle disfunzioni della minzione sia non - neurogene che da disfunzioni neurogene dello sfintere vescicale . le pagine sono aumentate da 431 a 533 e con esse il numero delle figure , delle immagini e delle tabelle ed il numero dei capitoli da 26 a 29 . 
in alcuni capitoli mr urography oppure urinary tract trauma sono state effettuate modificazioni sostanziali mentre in altri solo delle aggiunte ( come langioplastica renale percutanea nel capitolo riguardante pediatric genitourinary intervention )  . 
 according to the new springer style , in this series , all boxes and relevant information sections of the book are highlighted in two shades of blue , which immediately catches the readers attention and makes them easier to understand . 
i do , however , regret the absence of contributions from italian colleagues , which were included in the first edition . in summary , this is an important and useful text . 
i believe this edition will become and important reference text for paediatric and adult radiologists , general paediatric practitioners , paediatric surgeons , urologists and paediatric nephrologists and will hopefully reach the largest possible circulation . apportata una modifica nella scaletta dei capitoli , ora pi consequenziali che non nella precedente edizione . secondo la nuova impostazione grafica della casa editrice , tutte le tabelle ed i quadri riassuntivi sono ben evidenziati in blu e blu pallido , cosa che richiama subito lattenzione rendendole pi facili da usare e memorizzare . 
purtroppo non si ha pi traccia dei contributi dei colleghi italiani presenti nella prima edizione . in conclusione , questo un libro di grande importanza ed utilit : solleva anche problematiche da risolvere , si spera , nel futuro con ulteriori studi dellargomento nellottica della miglior cura dei bambini . 
between 1 january 2006 and 30 june 2007 , 23 consecutive patients ( 21 men and 2 women ) presenting with electrocardiographic abnormalities mimicking acute myocardial infarction and a clinical suspicion of acute myocarditis ( fever , chest pain and elevated troponin levels ) underwent contrast - enhanced cardiac mri within a week of admission . 
dal 1 gennaio 2006 al 30 giugno 2007 , ventitre pazienti consecutivi ricoverati con alterazioni elettrocardiografiche di tipo simil - infartuale ( stemi ) e sospetto clinico di miocardite acuta ( febbre , dolore toracico , positivit dei valori di troponina ) sono stati sottoposti , entro 6 giorni dallesordio , a risonanza magnetica ( rm ) cardiaca con mdc . 
la rm cardiaca pu avere ruolo fondamentale nella diagnosi precoce di miocardite acuta , documentando un quadro di alterazioni di segnale del miocardio che esclude la genesi ischemica . 230 radiol med ( 2009 ) 114 : 229238 keywords magnetic resonance imaging myocarditis myocardial infarction parole chiave risonanza magnetica miocardite infarto del miocardio introduction introduzione myocarditis is an inflammation of the myocardium associated with myocyte necrosis and is usually of viral origin [ 1 , 2 ]  . 
persistence of viraemia associated with an autoimmune response can cause chronic inflammation that may progress to dilated cardiomyopathy [ 4 ]  . because noninvasive imaging modalities are unable to provide a definitive diagnosis , invasive procedures are used , such as endomyocardial biopsy , which is considered the reference standard for the diagnosis . 
in addition , there is some variability in the interpretation of specimens , and the standard histological criteria for inflammation and myocytolysis tend to underestimate the true incidence of myocarditis , requiring integration with immunohistochemical analysis [ 5 ]  . 
endomyocardial biopsy is indicated in patients with rapidly progressive cardiomyopathy not responding to conventional treatment or in cases of cardiomyopathy associated with severe arrhythmias . there is thus a need for imaging modalities able to assist in the early diagnosis and follow - up of myocarditis [ 6 ]  . magnetic resonance imaging ( mri ) has been shown to be effective not only for the diagnosis [ 7 ] , where evidence of late gadolinium enhancement reflects irreversible myocardial damage , but also for quantifying disease extent and thus allowing lesion monitoring [ 8 , 9 ]  . 
these findings have also been validated by histopathology , as reported in the literature [ 8 ]  . the late enhancement obtained with mri permits visualisation of small myocardial lesions that in patients with myocarditis tend to be located in the subepicardial or intramyocardial regions with sparing of the subendocardium , conversely to what occurs in ischemic necrosis where the damage is subendocardial or transmural [ 9 , 10 ]  . the aims of our study were to confirm the diagnostic reliability of mri in acute myocarditis in patients with infarction - like clinical findings and to evaluate the possibility of la miocardite una infiammazione del miocardio associata a necrosi , nella maggior parte dei casi di origine virale [ 1 , 2 ]  . 
il persistere della viremia associato alla risposta auto - immunitaria pu causare infiammazioni croniche che possono evolvere in cardiomiopatia dilatativa [ 4 ]  . allo stato attuale le metodiche non invasive non permettono di ottenere la diagnosi definitiva di miocardite cosicch necessario il ricorso a procedure diagnostiche invasive , come la biopsia endomiocardica , considerata la metodica di riferimento nella diagnosi di miocardite . 
in primo luogo la sensibilit della metodica strettamente correlata alla qualit dei frustoli ed inoltre si possono avere falsi - negativi quando il prelievo sia stato effettuato in unarea non coinvolta dal processo infiammatorio ; inoltre esiste variabilit nella interpretazione dei campioni ed i semplici criteri istologici di infiammazione e miocitolisi spesso sottostimano la reale incidenza di miocardite tant che debbono essere integrati con una analisi immunoistochimica [ 5 ]  . 
in secondo luogo la biopsia endomiocardica una procedura che comporta dei rischi per cui opinabile lutilizzo di questa metodica , specie nei casi in cui la patologia ha andamento benigno e regredisce spontaneamente in breve tempo . 
 stato dimostrato che la risonanza magnetica pu essere di aiuto non solo per la diagnosi [ 7 ] , identificando il late gadolinium enhacement ( le ) espressione di danno miocardico irreversibile ma in grado anche di quantificare lestensione della patologia , consentendone il monitoraggio [ 8 , 9 ]  . 
 il le ottenuto con rm permette di visualizzare piccoli danni miocardici che , in pazienti affetti da miocardite , sono localizzati usualmente nella porzione subepicardica o intramiocardica senza interessamento del subendocardio contrariamente a quanto avviene nella necrosi a genesi ischemica , radiol med ( 2009 ) 114 : 229238 monitoring disease evolution during the follow - up by correlating mri findings with cardiac function . materials and methods patient inclusion criteria patient inclusion criteria in our study were the following : 1 . 
absence of significant coronary artery stenosis on coronary angiography . twenty - three consecutive patients meeting the above criteria were enrolled in the study between 1 january 2006 and 30 june 2007 . 
two patients were excluded due to claustrophobia . magnetic resonance imaging mri examinations were performed on a superconductive 1.5 - t magnet ( intera , philips medical systems , best , the netherlands ) within 6 days of patient admission to hospital . 
all patients were imaged during a breath - hold . localisation was achieved with electrocardiograph ( ecg ) gated balanced fast - field echo ( ffe ) steady - state freeprecession sequences in planes corresponding to the cardiac axes . 
ecg - gated t1and t2 - weighted black - blood sequences were acquired in the short axis ( base , mid ventricle and apex ) , with tr dependent on the trigger ( t1 with tr 1 rr , te 25 ms , flip angle 90 , t2 with tr 2 rr , te 80 ms , flip angle 90 )  . 
due pazienti tuttavia sono stati esclusi in quanto non hanno potuto espletare lesame di rm per manifesta claustrofobia . risonanza magnetica gli esami di rm sono stati acquisiti utilizzando un magnete superconduttivo da 1.5 t ( intera , philips medical systems , best , olanda ) entro 6 giorni dallingresso in ospedale . 
le sequenze t1 e t2 pesate black blood sono state acquisite su asse corto ( basale , medio - ventricolare e apicale ) , cardiosincronizzate con tr dipendente dal trigger ( t1 con tr 1 rr , te 25 ms , flip angle 90 ; t2 con tr 2 rr , te 80 ms , flip angle 90 )  . 
 le immagini post - contrastografiche t1 pesate sono state acquisite con un ritardo di 1015 min dopo la 232 radiol med ( 2009 ) 114 : 229238 short - axis and twoand four - chamber long - axis views . 
areas of late enhancement were defined as those exhibiting a signal intensity 2 standard deviations ( sd ) above the mean signal intensity of the remote myocardiuthe portion of the heart exhibiting late enhancement was classified according to the segmentation established by the american heart association , which divides the left ventricle into 17 segments [ 11 ]  . 
standard coronary angiography using a philips integris allura unit was performed within 3 h of patient admission to exclude the presence of coronary vascular abnormalities . results the number of patients included in the study was 21 ( 20 men and one woman ; mean age 30 years ) ( table 1 )  . 
systolic function was preserved in most patients ( ef > 50% ) , with a mild dysfunction being encountered three patients only ( ef 45%48% ) ( table 1 )  . 
only mild segmental wall motion abnormalities were encountered , with no cases of akinesia . t2 - weighted sequences demonstrated increased signal intensity corresponding to the areas of late enhancement , a possible expression of oedema . 
la risoluzione spaziale stata sempre di 1 , 21 , 8 mla dose di contrasto utilizzata ( gadoteridol , magnevist , shering ag , berlin , germania ) stata di 0 , 1 mmol / kg . lestensione dellenhancement post - contrastografico stata misurata sulle immagini ad asse corto ed asse lungo due camere e quattro camere . 
sono state considerate come aree di le solo quelle con un livello di intensit 2 sd ( deviazioni standard ) rispetto alla media delle intensit di segnale di tutte le pareti del miocardio . 
la porzione di cuore interessata dal le stata classificata in accordo con la segmentazione dellamerican heart association , che suddivide il ventricolo sinistro in 17 segmenti [ 11 ]  . 
la coronarografia convenzionale stata effettuata con tecnica standard per escludere la presenza di alterazioni vascolari coronariche con apparecchio philips integris allura nellintervallo di tempo massimo di 3 ore dal momento dellarrivo del paziente nel nostro ospedale . risultati i pazienti inclusi nello studio sono stati 21 di cui 20 uomini e 1 donna . 
in questultimo paziente il test virologico ha rilevato una infezione da coxsackievirus . dal punto di vista clinico nel follow - up nessun paziente ha riportato eventi aritmici e / o ulteriori complicanze cardiologiche ; la frazione di eiezione risultata stabile o migliorata in tutti i pazienti . 
nel follow - up con le sequenze t2 non stata riscontrata presenza di edema ; anche paziente , che aveva presentato al controllo una nuova area di le , non si sono riscontrate aree edemigene . discussione il nostro studio , in accordo con quanto riportato in letteratura , conferma laffidabilit della rm nella diagnosi del coinvolgimento miocardico , definendo estensione e localizzazione del le durante la fase acuta di una miocardite attiva [ 13 , 14 ] , ed in grado di valutare la progressione o regressione dellaffezione cardiaca nel follow - up [ 9 ]  . 
inoltre non stata ancora chiarita la correlazione tra i pattern miocardici della rm e la riduzione della funzione sistolica . nel nostro studio stata analizzata la localizzazione del le e la sua correlazione con la severit della disfunzione miocardica in 21 pazienti con quadro clinico simil - infartuale , affetti da miocardite acuta , con arterie coronarie indenni . 
2 distribuzione delle aree di late enhancement della popolazione studiata in accordo con la segmentazione dellamerican heart association . discussion in agreement with previous reports , our study confirms the effectiveness of mri in diagnosing myocardial damage , as it is able to delineate the extent and location of late enhancement during the acute phase of active myocarditis [ 13 , 14 ] and evaluate disease progression or regression during the follow - up [ 9 ]  . 
nonetheless , mri is not regarded as the reference standard for diagnosing myocarditis , nor has the correlation between mri myocardial patterns and reduced systolic function been clarified to date . radiol med ( 2009 ) 114 : 229238 fig . 
piccola area di late enhancement intramiocardico in sede laterale medio - distale . our study analysed the location of the late enhancement and its correlation with myocardial dysfunction severity in 21 patients affected by acute myocarditis mimicking infarction and with healthy coronary arteries . 
we observed a peculiar distribution of the myocardial lesions , which involved the epicardial and / or intramyocardial region of the left ventricular wall , with prevalent involvement of the inferiore rispetto alla parete laterale . 
la distribuzione delle lesioni miocardiche da noi riscontrata , con il frequente coinvolgimento infiammatorio della parete laterale , ampiamente confermata da quanto riportato in letteratura , che inoltre , nei pi recenti contributi [ 15 ] ipotizza persino una stretta correlazione fra agente patogeno e sede della lesione miocardica [ 16 , 17 ]  . 
6a , b inversion - recovery gradient recalled echo ( ir - gre ) long - axis four - chamber view showing myocardial damage in the intermediate and distal segments of the lateral wall during acute myocarditis ( a )  . 
6a , b sequenze ir - gre post - contrastografiche : acquisizione in asse lungo 4 camere allesordio con aree di late enhancement localizzate a livello della parete laterale nei segmenti medi e distali ( a )  . 
the pattern of myocardial damage seen in our study with frequent involvement of the lateral wall has been widely reported in the literature , and recent contributions [ 15 ] have even suggested the possibility of a close relationship between the nature of the pathogen and the site of myocardial damage [ 16 , 17 ]  . durante il follow - up le aree di le si sono progressivamente ridotte nel tempo ad eccezione di un unico caso in cui sono comparse nuove aree di le . 
in tutti i pazienti non si mai rilevata impregnazione post - contrastografica tardiva ( le ) a partenza dal subendocardio , reperto tipico e , quadro rm ormai consolidato , di coinvolgimento miocardico su base ischemica [ 5 , 18 , 19 ]  . il meccanismo responsabile dellimpregnazione postcontrastografica tardiva non stato ancora completamente radiol med ( 2009 ) 114 : 229238 during the follow - up , the areas of late enhancement decreased progressively , with the exception of one patient who developed new areas of late enhancement . 
none of the patients exhibited late enhancement originating in the subendocardial portion , a typical and consolidated mri pattern of ischaemic myocardial damage [ 5 , 18 , 19 ]  . the mechanism responsible for late enhancement has not been elucidated , and various pathophysiological hypotheses have been put forward . 
during healing of the inflammatory process , contrast enhancement is progressively reduced , and in some cases , only a microscar can be identified , which reflects fibrous replacement of the necrotic myocytes . during the follow - up , in some of our patients , the late enhancement albeit less intense persisted in the same area for more than 4 months . 
this finding confirms the need to further investigate the long - term prognostic significance of late enhancement . finally , mri can provide information about the precise location of the myocardial damage induced by myocarditis and may serve as a guide for the execution of endomyocardial biopsy [ 20 ]  . left ventricular ef and the extent of late enhancement were not found to be closely correlated . 
a further explanation that may account for normal ef lies in the fact that the damage identified by contrast enhancement is overestimated during the acute phase , in part because not all the cells contained in the area of enhancement are totally damaged , as opposed to what happens in myocardial infarction . chiarito ed in merito sono state formulate varie ipotesi fisiopatologiche . 
fra queste quella che gode di maggior credito quella che identifica nella rottura della membrana dei miociti la causa della diffusione del mezzo di contrasto non solo nello spazio extracellulare ma anche in quello intracellulare [ 10 ]  . 
questa ipotesi supportata dai riscontri isto - patologici che identificano nelle fasi precoci della miocardite la presenza di edema interstiziale con infiltrato linfocitario e necrosi dei miociti ; il successivo danno cellulare si instaura nelle ore e / o giorni successivi al momento iniziale dellinfezione . 
peraltro il miocardio in condizioni di normalit non presenta impregnazione post - contrastografica perch i miociti , con membrane sarcolemmatiche integre , non permettono la diffusione del mezzo di contrasto al loro interno e quindi risulta impregnarsi solo lo spazio extra - cellulare , peraltro esiguo . 
quando il processo infiammatorio in fase di guarigione limpregnazione post - contrastografica si riduce progressivamente ed in alcuni casi pu essere identificata solamente una micro - cicatrice , espressione di sostituzione fibrotica delle aree di necrosi dei miociti . 
 nel follow - up della nostra serie si riscontrata , in alcuni casi , persistenza del le nella stessa sede , seppur ridotta in intensit , anche dopo 4 mesi . 
tale osservazione conferma quanto finora riportato in letteratura vale a dire che il significato del le , come valore prognostico clinico a lungo termine , deve essere ancora validato . infine da ricordare che la rm pu fornire informazioni sulla esatta localizzazione del danno miocardico causato dalla miocardite e pu pertanto essere utilizzata quale eventuale guida per la biopsia endomiocardica [ 20 ]  . la frazione di eiezione ventricolare sinistra ( lvef ) e lestensione del le non sono risultate strettamente correlate . 
una ulteriore spiegazione , a giustificazione del normale lvef , risiede nel fatto che il danno identificato dallimpregnazione post - contrastografica sovrastimato nella fase acuta , anche perch non tutte le cellule ubicate nellarea di enhancement sono totalmente danneggiate , contrariamente a ci che avviene nei casi di infarto del miocardio . 238 conclusions conclusioni radiol med ( 2009 ) 114 : 229238 late contrast enhancement at mri is a constant finding in the diagnosis of myocarditis and is directly correlated to myocardial damage . 
this late enhancement manifests with a characteristic pattern in that it originates from the epicardial and / or intramyocardial surface , and this distinguishes it from ischaemic necrosis that shows subendocardial and / or transmural involvement . 
finally , mri proved to be very useful in evaluating and monitoring the progression of inflammatory damage over time . limpregnazione post - contrastografica tardiva ( le ) ottenuta con rm un reperto costante nella diagnosi delle miocarditi ed direttamente correlata al danno miocardico . il pattern con cui si manifesta caratteristico originando dalla superficie epicardica e / o intramiocardica , il che lo distingue dalla necrosi di origine ischemica che ha una interessamento subendocardico e / o transmurale . 
trentatre pazienti ( 22 maschi , 11 femmine , di et media di 62 , 4 ) sono stati sottoposti a risonanza magnetica ( rm ) utilizzando un magnete da 1 , 5 tesla ( general electric , hd )  . 
a riposo sono state impiegate sequenze rm cine di tipo steady - state con imaging parallelo in 4 - camere , per il tratto di efflusso del ventricolo sinistro ed in asse corto . 
dobutamine stress cardiac mri is an accurate method for assessing myocardial ischaemia in patients with cad , and it could be useful as a noninvasive tool for excluding the disease . 
the increase in signal intensity and acquisition speed obtained by using steadystate free precession with parallel imaging proved useful in increasing test specificity with respect to previous similar studies . keywords magnetic resonance imaging dobutamine stress testing heart ischemia analizzato in totale 960 segmenti ed abbiamo osservato comparsa o peggioramento della cinesi in sette pazienti ed in 29 differenti segmenti . 
lincremento dellintensit del segnale e della velocit di acquisizione ottenuta utilizzando le sequenze steady - state free precession con imaging parallelo risultata utile nellincrementare la specificit del test rispetto a precedenti simili studi . parole chiave risonanza magnetica test da sforzo con dobutamina cuore ischemia introduction introduzione previous studies have demonstrated that cardiac magnetic resonance imaging ( mri ) with dobutamine stress has a clinically useful accuracy for detecting myocardial ischemia [ 16 ]  . 
 [ 6 ] demonstrated that stress cardiac mri provided better sensitivity ( 86% vs 74% ) and specificity ( 86% vs 70% ) than stress echocardiography for detecting new regional kinetic alterations in 172 patients compared with coronary angiography . 
 the fast - gradient - echo technique has been used to evaluate a group of patients referred for diagnosis of ischaemia . the technique provided useful data for diagnosing inducible ischaemia in patients unable to undergo stress echocardiography [ 6 , 7 ]  . 
acquisition time has been reduced to 67 s or less for each slice , with 30 phases per cardiac cycle , thus improving regional kinetic analysis and ventricular exploration during pharmacological stress studies [ 8 ]  . the purpose of this study was to assess the clinical utility of dobutamine stress mri in demonstrating inducible ischaemia in patients with atypical chest pain or equivocal studi precedenti hanno dimostrato che la risonanza magnetica cardiaca ( rmc ) da stress con dobutamina possiede unaccuratezza clinica utile alla rilevazione di ischemia miocardica [ 16 ]  . 
nonostante ci lecocardiografia ( eco ) da stress resta nella pratica clinica il metodo preferito per lanalisi della funzione regionale ventricolare in virt dellelevata accuratezza , versatilit , disponibilit e del costo relativamente contenuto . 
 [ 6 ] hanno dimostrato che la risonanza magnetica cardiaca da stress forniva una migliore sensibilit ( 86% vs 74% ) e specificit ( 86% vs 70% ) rispetto alleco - stress per la rilevazione di nuove alterazioni cinetiche regionali in 172 pazienti confrontati con angiografia coronarica . 
inoltre , la superiorit della rmc rispetto allecografia risultava pi evidente in pazienti che presentavano una qualit ecografica moderata . utilizzando la tecnica fast gradient echo , sono stati analizzati un gruppo di pazienti con sospetto di malattia ischemica ; questa tecnica ha fornito dati utili per la diagnosi di ischemia inducibile in pazienti non sottoponibili a eco - stress [ 6 , 7 ]  . 
il tempo di acquisizione stato ridotto a 67 secondi o meno per ogni sezione con 30 fasi acquisite nel singolo ciclo cardiaco , migliorando cos lanalisi cinetica regionale e 218 radiol med ( 2009 ) 114 : 216228 stress electrocardiography ( ecg ) not suitable for stress echocardiography using steady - state parallel imaging sequences . materials and methods the study population consisted of 33 patients ( 22 men and 11 women ; age range 5268 years , mean age 62.4 years ) with a suspicion of ischaemia due to atypical chest pain or equivocal stress ecg not suitable for stress echocardiography because of inadequate endocardial visualization despite the use of second harmonic imaging at the evaluation at rest . 
patients were excluded if they had known general contraindications to mri or dobutamine , a recent history of myocardial infarction , significant q waves and prior coronary surgery ( table 1 )  . 
 mri technique mri was performed using a 1.5 - tesla superconducting whole - body system ( general electric medical system , milwaukee , wi , usa ) equipped with 33 mt / m gradients ( slew rate 120 mt / m / s )  . 
in - plane resolution was 1.4 mm , with a slice thickness of 8 mm . first - pass perfusion was performed using t1 - weighted saturation recovery ( sr ) sequences repeated for 2530 s for each r - r or 2r - r interval , depending on heart rate , to obtain at least three slices for each acquisition at the apical , papillary and basal level . 
 study protocol intravenous access was gained through the right antecubital ve mri was performed with the patient in the supine position on the scanning table with an eight - channel phasedarray surface coil . 
a three - channel ecg monitor was lesplorazione del ventricolo durante lo stress farmacologico [ 8 ]  . lo scopo del presente studio stato di stabilire lutilit clinica della rmc da stress con dobutamina nella diagnosi di ischemia inducibile mediante lutilizzo di sequenze ssfp e di tecniche di imaging parallelo , in pazienti con dolore toracico atipico o ecg da sforzo dubbio non sottoponibili a eco - stress . materiali e metodi abbiamo studiato 33 pazienti ( 22 uomini e 11 donne di et compresa da 52 a 68 anni , et media 62 , 4 anni ) con il sospetto di ischemia cardiaca per la presenza dolore toracico atipico o ecg da sforzo dubbio , non idonei ad essere sottoposti a eco - stress a causa di inadeguata visualizzazione dei contorni endocardiaci , nonostante limpiego della seconda armonica , gi nella valutazione a riposo . lecocardiografia stata eseguita con un apparecchio recente ( philips 5000 ) da due diversi operatori con 9 e 7 anni di esperienza . 
i pazienti non erano arruolabili se presentavano controindicazioni generiche alla rm o alla dobutamina o se affetti da infarto miocardio di recente insorgenza , onde q significative e se precedentemente sottoposti a chirurgia coronaria ( tabella 1 )  . 
a tutti i partecipanti allo studio stato richiesto di sospendere lassunzione di - bloccanti e farmaci antiangina , rispettivamente 72 e 24 ore prima dellanalisi rmc . tecnica rm per limaging a risonanza magnetica stato usato uno scanner whole - body con magnete superconduttivo a 1 , 5 tesla ( general electric medical system , milwaukee usa ) con gradienti da 33 mt / m e tempo di risalita da 120 mt / m / s . 
 stato collegato un monitor ecg 3 canali e contemporaneamente misurati saturazione di o2 e pressione sanguigna brachiale . a riposo , abbiamo eseguito una valutazione funzionale standard che includeva una acquisizione in asse lungo verticale , acquisizioni multiple in asse corto al livello del ventricolo sinistro dallapice alla base senza alcun intervallo tra le sequenze ( 89 sequenze ) e acquisizione in 4 camere ( 46 sequenze senza intervallo ) e 34 sequenze nel tratto di deflusso del ventricolo sinistro ( lvot )  . 
lanalisi della perfusione al primo passaggio stata ottenuta in asse corto dopo iniezione di 0 , 1 m / kg di gadolinio alla velocit di infusione di 5 ml / s . 
lo stress test stato eseguito tramite lacquisizione di 6 sezioni ssfp dalla base allapice del ventricolo sinistro con un intervallo tra le sezioni di 46 msono state acquisite fino a 2 sequenze durante una singola apnea per una durata massima di 1315 secondi . 
le immagini sono state acquisite dopo 3 minuti dalliniezione di dosi crescenti di dobutamina endovena pari a 510203040 g / kg / min fino a raggiungere l85% della frequenza cardiaca massimale teorica calcolata dalla formula ( 220 et ) 0 , 85 per gli uomini e ( 200 et ) 0 , 85 per le donne . 
 stata monitorata costantemente la frequenza ed il ritmo cardiaco , ogni due minuti la pressione sistemica , sulle immagini acquisite la funzione regionale ; laumento della pressione sistolica oltre i 40 mmhg , la presenza di frequente extrasistolia o la comparsa di nuove alterazioni cinetiche parietali sono state considerate motivo di sospensione del test . analisi delle immagini la cinesi regionale stata analizzata da 2 osservatori non a conoscenza dei risultati degli altri esami . 
first - pass perfusion analysis was obtained on short - axis views after injection of 0.1 m / kg of gadolinium at a flow rate of 5 ml / s . 
stress evaluation was performed using six ssfp acquisitions obtained from the left - ventricle base to apex with an interslice gap of 46 mm . up to two acquisitions were acquired during a single breathhold lasting 1315 s . 
images were acquired starting 3 min after the intravenous injection of 5 , 10 , 20 , 30 or 40 g / kg / min dobutamine to reach 85% of the theoretical maximal heart rate predicted by the following formula : ( 220age ) 0.85 for men and ( 200age ) 0.85 for women [ 1 ]  . 
the test was discontinued in the event of an increase of systolic pressure > 40 mmhg or a drop in blood pressure , frequent arrhythmia or the appearance of new wall motion abnormalities . 
each of the six slices was divided into five segments : anteroseptal , anterior , lateral , posterior and posteroseptal from the basal level ( i ) to the apex ( vi )  . 
the test was considered positive for ischaemia if the score increased by at least 1 point during the infusion or indicative of viability if a hypokinetic segment became normal at low dobutamine dose and worsened at high dose . cases of disagreement were resolved by reviewing the images and reaching a consensus . 
coronary angiography was considered the standard of reference and was performed in 22 out of 32 patients included in the study within 3 months from the mri examination in the absence of cardiac events . at least two orthogonal planes were obtained , and standard analysis was used for each vessel . 
il test stato considerato positivo per ischemia se vi stato un aumento del punteggio di almeno un livello durante linfusione o indicativo di vitalit se un segmento diventava normale a basso dosaggio di dobutamine per poi peggiorare di nuovo allaumentare del dosaggio del farmaco . 
in caso di discordanza tra i due osservatori stato effettuato una rivalutazione per ottenere laccordo . lapporto arterioso coronarico stato definito secondo la nomenclatura e segmentazione della american heart association ( aha ) [ 9 ]  . 
la gravit della stenosi , durante lesame coronarografico , stata considerata significativa se superiore al 50% in coronarie 2 mm . analisi statistica tutti i parametri continui sono stati espressi come mediadeviazione standard ; stato considerato significativo un valore di p < 0 , 05 . 
sensibilit e specificit sono stati calcolati per stenosi superiori al 50% . risultati una paziente presentava a riposo grave ipertensione ed stata esclusa ; pertanto stata effettuata analisi cinetica e perfusionale a riposo e stress con dipiridamolo e non risultato evidente di difetto di perfusione o disfunzione cinetica dovuta a ischemia inducibile . 
i restanti presentavano cinesi normale in tutti i segmenti del ventricolo sinistro . tutti i pazienti sono stati in grado di raggiungere l85% della frequenza cardiaca massima teorica prevista dallet . per raggiungere tale valore , stata necessaria in 6 pazienti liniezione di atropina alla fine della somministrazione incrementale di dobutamina . 
in 4 pazienti stato sufficiente 1 mg di atropina , nei restanti due si dovuto ricorrere ad un dosaggio incrementale di rispettivamente 1 , 5 mg e 2 mg . radiol med ( 2009 ) 114 : 216228 rest 5 microg / kg / min 10 microg / kg / min 20 microg / kg / min 30 microg / kg / min 40 microg / kg / min fig . 
all patients were able to reach 85% of the theoretical maximum heart rate la frequenza cardiaca basale stata di 6918 battiti al minuto ( 5081 ) , la frequenza cardiaca massima di 145 battiti al minuto ( media 13411 )  . 
la pressione sanguigna di base stata tra 150 / 95 e 110 / 70 mmhg , con picco di pressionedurante il test tra 185 / 110 e 160 / 93 mmhg . 
 durante linfusione di dobutamina 12 pazienti hanno mostrato segni di ansia , ma solo in 4 casi questa stata responsabile di una cooperazione incompleta nellapnea e di conseguenza ha prodotto artefatti nelle immagini . 
atropine injection after incremental dobutamine administration was necessary in six patients to achieve at least 85% of the theoretical maximum heart rate . a dose of 1 mg of atropine was sufficient in four patients , whereas incremental doses of 1.5 and 2 mg were necessary in the remaining two patients . 
baseline blood pressure was between 150 / 95 mmhg and 110 / 70 mmhg , and peak blood pressure during the test was between 185 / 110 mmhg and 160 / 93 mmhg . during dobutamine infusion , 12 patients developed anxiety , but only in four of them did this result in incomplete cooperation in the breath - hold sequences , with consequent image artefacts . 
i dieci pazienti che non hanno eseguito la coronarografia e che non presentavano evidenza di ischemia inducibile alla rm da stress ( tre pazienti hanno rifiutato lesame coronarografico mentre nei restanti 7 casi , sulla scorta dei dati clinici e strumentali ottenuti abbiamo ritenuto inadeguato ed eccessivo il rischio di unangiografia coronarica ) sono stati ricontattati 912 mesi dopo ( media 10 , 2 mesi )  . 
parziale recupero funzionale stato osservato alla bassa dose di dobutamina nel segmento anterosettale ( c ) con peggioramento della cinesi alle alte dosi di dobutamina . examination and coronary angiography was between 1 week and 3 months ( mean 26 days )  . 
ten patients , who had no evidence of inducible ischaemia at mri , did not undergo coronary angiography ( three patients due to refusal and seven because review of the clinical and instrumental data indicated high risk )  . 
the reasons are sono presenti ad un esame basale cos come durante i test sotto sforzo e sono frequentemente correlate ad enfisema polmonare e conseguente bassa velocit di propagazione degli ultrasuoni . 
in definitiva , la penetrabilit acustica resta un aspetto determinante per la qualit dellimmagine [ 13 ]  . tutti i pazienti inclusi nel nostro studio presentavano una riduzione evidente della qualit ecocardiografica , responsabile di delineazione difficoltosa dei bordi endocardici . lapplicazione di imaging con seconda armonica non stata in grado di superare le difficolt nellanalisi cinetica . per questi pazienti leco - stress con dobutamina sarebbe rest 5 microg / kg / min 10 microg / kg / min radiol med ( 2009 ) 114 : 216228 69 hb / min 70 hb / min 73 hb / min 20 microg / kg / min 30 microg / kg / min 40 microg / kg / min 79 hb / min 112 hb / min 139 hb / min fig . 
4a - g acinesia del segmento postero - settale evidente allo stress massimale nelle immagini tele - sistoliche ( f ) , correlato alla presenza di stenosi significativa della coronaria destra ( g )  . related to the high accuracy achievable with this modality , its availability , versatility and relatively low costs . 
considerando tutti questi aspetti , la possibilit di valutare la cinesi del ventricolo sinistro tramite rm potrebbe rivelarsi unalternativa efficace sia per la valutazione basale sia durante il test da stress farmacologico [ 7 ]  . 
inoltre la risoluzione ad alto contrasto della rm molto utile per delineare in modo corretto non solo lendocardio ma anche i bordi epicardici in modo da ottenere una stima corretta dellispessimento della parete [ 14 , 15 ]  . 
lunica limitazione tecnica relativa alla rm dovuta alla sensibilit ad artefatti da movimento che possono essere presenti in modo particolare durante lo radiol med ( 2009 ) 114 : 216228 all the patients in our series had an evident reduction of echocardiographic quality that was considered responsible for difficulties in delineating the endocardial borders . 
in consideration of these aspects , the possibility of evaluating left ventricle kinesis by mri could be a useful alternative for evaluation both at baseline and during pharmacological stress test [ 7 ]  . 
moreover , the high - contrast resolution of mri is useful for correctly delineating not only the endocardium but also the epicardial borders and thus obtaining an accurate estimation of wall thickening [ 14 , 15 ]  . 
the only technical limitation of mri is related to its sensitivity to movement artefacts , which may be particularly present during stress imaging as a result of anxiety or pain affecting certain patients . previous studies have reported the feasibility of mri combined with pharmacological stress testing . 
the first investigation was performed in 1992 by pennel et al . , who used an intermediate dose of dobutamine ( up to 20 g / kg / min ) to examine 25 patients with exertional chest pa the study achieved a 90% agreement with dobutamine thallium - 201 single - photon - emission computed tomography [ 16 ]  . 
a few years later , two studies reported a good level of accuracy using a similar dose of dobutamine in a small group of patients [ 17 , 18 ]  . 
it was not until 1999 that nagel et al . reported the efficacy of mri with high doses of dobutamine ( up to 40 g / kg per minute ) followed by atropine as needed to reach the maximal theoretical heart rate for detecting inducible ischaemia . 
on the other hand , the quality of the images obtained with dobutamine stress echocardiography has been reported to be good or very good in 50% of cases with the standard modality and up to 70% using harmonic imaging [ 7 ]  . 
reported an 83% sensitivity and specificity of dobutamine mri in detecting noninducible ischaemia in patients not suitable for second harmonic imaging , particularly those with a large body , severe obstructive airway disease or prior cardiothoracic surgery [ 7 ]  . 
pennel , il quale nel 1992 ha esaminato 25 pazienti con dolore toracico da sforzo usando una dose intermedia di dobutamina ( fino a 20 g / kg / min )  . 
 [ 6 ] hanno riportato lefficacia del rm nellindividuare ischemia inducibile con alte dosi di dobutamina , fino a 40 g / kg / min , seguita , quando necessario , da atropina se per raggiungere la frequenza cardiaca massimale teorica ; loro hanno inoltre comparato i risultati con unampia popolazione sottoposta ad angiografia coronarica . 
gli autori hanno riscontrato una migliore attendibilit rispetto all eco - stress con dobutamina sia in termini di sensibilit ( 88 , 7% contro 74 , 3% ; p < 0 , 05 ) che di specificit per ischemia inducibile ( 85 , 7% contro 69 , 8% ; p < 0 , 05 ) comparata con angiografia coronarica [ 6 ]  . 
dallaltro lato , la qualit dellimmagine ottenibile tramite eco - stress con dobutamina stata considerata da buona a molto buona in solo il 50% dei casi con la modalit standard , e fino al 70% tramite imaging con armonica [ 7 ]  . 
 [ 7 ] hanno riferito lutilit della rm con dobutamina nel rilevare ischemia non inducibile in pazienti non sottoponibili ad imaging con seconda armonica , in particolare quelli sovrappeso , con gravi malattie ostruttive delle vie respiratorie o sottoposti a precedente chirurgia cardiotoracica , riportando una sensibilit e specificit dell83% [ 7 ]  . 
nel 2003 hanno riscontrato una sensibilit del 96% e una specificit del 95% usando un apparato rm a 1.0 tesla su 211 pazienti [ 19 ]  . tutti questi dati sperimentali sono stati ottenuti usando sequenze fast gradient - echo . 
solo nel 2004 patesch et al . [ 4 ] hanno riportato uno studio su stress con dobutamina combinata con adenosina condotto su 79 pazienti , fornendo rispettivamente una sensibilit dell89% e una specificit del 96% , usando sequenze ssfp [ 4 ]  . 
utilizzando queste sequenze essi sono stati in grado di ottenere un aumento nella risoluzione temporale fino a 25 fasi per ciclo cardiaco e una migliore delineazione dei bordi endocardici dovuta 226 radiol med ( 2009 ) 114 : 216228 reported a sensitivity of 96% and a specificity of 95% using a 1.0 - tesla mr apparatus on 211 consecutive patients [ 19 ]  . 
report on a study investigating combined adenosine and dobutamine stress in 79 consecutive patients , providing a sensitivity in comparison with coronary angiography of 89% and a specificity of 96% obtained using the steady - state free - precession sequences [ 4 ]  . 
use of these sequences enabled them to increase temporal resolution up to 25 phases per cardiac cycle and to achieve a better delineation of the endocardial borders due to an almost complete reduction of the signal void during the systolic phase that generally affects fast - gradient - echo sequences . 
nevertheless , the level of accuracy obtained was similar to that of the other previous experiences . in our study , we employed an ssfp sequence with parallel imaging that allowed us to obtain 2530 cardiac phases per cycle in half the time required for the previously reported sequences , making it possible to simultaneously acquire two different slices with a higher contrast - to - noise ratio compared with gradient - echo acquisition . 
a five - segment segmentation was performed in accordance with the american heart association [ 9 ]  . ventricular regional analysis was performed on a 30segment model , producing a definitely greater segmentation than reported by previous dobutamine stress mri studies . 
this could be related to the limited number of cases enrolled in our study or , alternatively , it could mean that increased regional segmentation does not offer an increase in sensitivity and specificity . 
the latter hypothesis , however , appears unrealistic if one considers that an increase in spatial coverage may increase the detection of inducible ischaemia , which may be evident only in small areas of the left ventricle due to stenosis of the distal coronary arteries [ 2023 ]  . 
the specificity obtained in our study was at the maximum level achievable , and this could , again , be due to the small number of patients examined or to the better border delineation obtained with the steady - state sequences and the multichannel phased - array coil [ 24 ]  . 
in agreement with other authors , we found the procedure to be safe , with no side effects being observed in our series [ 3 , 2729 ]  . the use of ssfp sequences is helpful for obtaining higher signal intensity and thus providing greater contrast alla riduzione quasi totale del vuoto di segnale durante la fase sistolica , che invece ostacolava le sequenze fast gradient - echo . 
 nel nostro studio abbiamo impiegato una sequenza ssfp con imaging parallelo con cui stato possibile ottenere 2530 fasi cardiache per ciclo in met del tempo richiesto per le sequenze precedentemente riportate rendendo possibile lacquisizione simultanea di due diverse sezioni con un rapporto contrasto / rumore superiore rispetto allacquisizione gradient - echo . 
lanalisi regionale ventricolare stata effettuata su un modello di 30 segmenti , producendo un segmentazione decisamente maggiore rispetto agli studi riportati finora . tuttavia , la sensibilit non risultata superiore rispetto ai dati precedentemente riportati . 
nel nostro studio abbiamo riportato una sensibilit dell85% , anche inferiore rispetto alla sensibilit riportata da kuijpers et al . [ 19 ] nel 2003 con limpiego di una rm ad 1 , 0 tesla e sequenze fast gradient - echo . 
questultima ipotesi sembra tuttavia poco realistica se si considera che lincremento della copertura spaziale pu incrementare la detezione di ischemia inducibile che pu essere evidente anche solo in piccoli territori del ventricolo sinistro a causa di stenosi di arterie coronarie distali [ 2023 ]  . 
dallaltro lato , la specificit da noi ottenuta stata pari al massimo livello raggiungibile e questo pu riflettere il limitato campione da noi studiato cosi come descritto per lanalisi dei dati sulla sensibilit , ma pu anche essere collegato alla migliore della delineazione dei bordi ottenuta usando le sequenze ssfp e la bobina multicanale phased array [ 24 ]  . 
la procedura si rivelata sicura anche nella nostra esperienza , cos come negli studi precedenti , infatti non sono stati riscontrati effetti collaterali nella nostra serie [ 3 , 2729 ]  . limpiego di sequenze ssfp utile per ottenere unintensit del segnale maggiore nelle immagini , fornendo un contrasto pi elevato tra sangue e miocardio , determinato principalmente dal loro differente rapporto t1 / t2 . 
lelevato rapporto segnale / rumore efficace anche per unacquisizione radiol med ( 2009 ) 114 : 216228 between blood and myocardium , which is principally determined by their different t1 / t2 ratios . 
these sequences are able to generate a significant increase in the delineation of endocardial borders , papillary muscles and trabeculations . the high signal - to - noise ratio is also useful for rapid acquisition , thanks to the possible use of very short tr values in the range of 35 ms [ 8 , 14 , 30 ]  . 
this is extremely useful when the heart rate increases during the dobutamine test , as it allows one to obtain a high frame rate even at maximal stress that is , when the r - r is reduced [ 3133 ]  . parallel imaging may represent a key factor in cardiac stress mri , as it reduces acquisition time by half . 
 the combination of the high signal intensity of ssfp sequences and parallel imaging , where signal intensity is inversely proportional to the square root of the acceleration factor , is ideal for dobutamine stress imaging [ 1 , 4 , 34 ]  . in conclusion , mri with ssfp and parallel imaging appears to be an advantageous technique for dobutamine stress mri , as it theoretically increases the high potential of the modality , which is considered the gold standard for evaluating inducible ischaemia . 
nevertheless , studies on larger populations are required to better evaluate the effects of technical improvements on the accuracy and especially the sensitivity of dobutamine stress testing . rapida con la possibilit di usare valori tr molto piccoli , di 35 ms [ 8 , 14 , 30 ]  . 
laumento nella risoluzione temporale rende possibile inoltre di aumentare i frames per ciclo cardiaco , cosa estremamente utile quando la frequenza cardiaca aumenta durante la somministrazione di dobutamina , cos da ottenere un alto rapporto frame / ciclo cardiaco anche a livello massimale di stress cio quando lr - r ridotto [ 3133 ]  . 
la combinazione tra lelevato segnale delle sequenze steady - state e limaging parallelo , nel quale lintensit del segnale inversamente proporzionale alla radice quadrata del fattore di accelerazione , si rivela ideale nel campo dellimaging da stress con dobutamina [ 1 , 4 , 34 ]  . in conclusione , limpiego di sequenze ssfp e imaging parallelo sembra una tecnica vantaggiosa per la rm da stress con dobutamina , aumentando teoricamente le potenzialit di questa metodica considerata la migliore per valutare lischemia inducibile . 
lagalla1 1dipartimento di biotecnologie e medicina legale , sezione di scienze radiologiche , 2dipartimento di medicina , pneumologia , fisiologia e nutrizione umana , sezione di pneumologia e medicina , 3dipartimento biomedico di medicina interna e specialistica , sezione di reumatologia , universit di palermo , palermo , italy correspondence to : m . 
bellia , via del vespro 127 , palermo , italy , tel . : + 39 - 091 - 6802652 , fax : + 39 - 091 - 6891857 , e - mail : maria.bellia@libero.it received : 10 december 2007 / accepted : 9 may 2008 / published online : 12 march 2009 springer - verlag 2009 abstract purpose . 
thirty - one patients with ssc ( 16 with the diffuse form and 15 with the limited form ) underwent functional and hrct evaluations of the lung . the semiquantitative evaluation of radiological involvement , as proposed by warrick , provides a score for each lesion based on the severity and the extent of the pulmonary damage . 
scopo del lavoro stato contribuire alla validazione del metodo del punteggio ( score ) radiologico di warrick nella valutazione del danno polmonare nella sclerosi sistemica ( scs ) e di correlare i risultati con le alterazioni della funzionalit respiratoria . 
trentuno pazienti affetti da scs , 16 da forma diffusa ( dscs ) , 15 da forma limitata ( lscs ) , sono stati sottoposti a valutazione respiratoria funzionale e radiologica tramite hrct . 
la valutazione semiquantitativa della compromissione radiologica stata effettuata mediante il metodo di warrick , che attribuisce un punteggio alle varie lesioni secondo un criterio di gravit ( score di severit del danno ) e di estensione delle stesse alterazioni allinterno del parenchima polmonare ( score di estensione del danno )  . 
i risultati del presente studio confermano il valore diagnostico dellhrct nel rappresentare il tipo e lestensione del danno polmonare determinato dalla scs . inoltre , la suddivisione in punteggi parziali ( alveolite e fibrosi ) apre una ulteriore prospettiva di valutazione dei rapporti tra interessamento polmonare e compromissione sistemica . parole chiave tomografia computerizzata ad alta risoluzione sclerosi sistemica alveolite fibrosi polmonare introduction introduzione systemic sclerosis ( ssc ) , or scleroderma , is a connectivetissue disease of unknown orig it is typically characterised by fibrosis of the skin , which may be diffuse or limited . 
the disease may also involve the blood vessels and internal organs , and the lung , the kidneys and the cardiovascular system are often affected simultaneously [ 1 ]  . 
clinical and radiological involvement of the lung is seen in 70%90% of cases , although autopsic studies have reported it to occur in 74% [ 3 ] to 100% of cases [ 4 ]  . 
the natural history of interstitial lung disease in ssc includes an initial phase of predominant alveolitis that is potentially reversible if treated immediately and adequately , and a progressive evolution with a prevalence of irreversible fibrosis leading to endstage lung disease . to substantially there is a growing interest in techniques capable of defining the stage of organ damage in its progression from inflammation irreversible structural damage . 
in this context , although chest radiography remains irreplaceable as a first - line imaging technique for detecting interstitial involvement , it is insufficient for discriminating between irreversible fibrosis and active alveolitis . 
considerable progress has been made with highresolution computed tomography ( hrct ) , which compared with conventional chest radiography offers high sensitivity even in the early phase of the disease , high la sclerosi sistemica ( scs ) o sclerodermia una malattia del tessuto connettivo ad eziologia sconosciuta , caratterizzata pi spesso da fibrosi della cute : questa pu essere colpita in forma diffusa o limitata . 
la malattia pu determinare inoltre un coinvolgimento dei vasi sanguigni e di organi interni : polmone , reni e apparato cardiovascolare tendono spesso ad essere interessati contemporaneamente [ 1 ]  . 
la patologia dellinterstizio polmonare costituisce limpegno viscerale pi frequente nella scs [ 2 ] e rappresenta una delle principali cause di morte in questi pazienti . linteressamento clinico - radiologico polmonare presente nel 70%90% dei casi , mentre studi basati sui rilievi autoptici hanno evidenziato dati di prevalenza del coinvolgimento polmonare posti tra il 74% [ 3 ] ed il 100% [ 4 ]  . 
la storia naturale dellinterstiziopatia da scs riconosce una fase iniziale con prevalenza di fenomeni alveolitici potenzialmente reversibili , se tempestivamente ed opportunamente trattati , ed una evoluzione progressiva con prevalenza di fenomeni fibrotici non suscettibili di intervento terapeutico fino alla condizione di end - stage lung . 
 un argomento di crescente interesse costituito dalle metodologie dirette a definire lo stadio evolutivo delle lesioni dorgano , lungo litinerario che dalla flogosi conduce al danno strutturale anatomico sostanzialmente irreversibile . 
a tal proposito , lesame radiologico del torace , pur conservando linsostituibile valore dellindagine di primo approccio che segnala il coinvolgimento dellinterstizio , non sufficiente per distinguere la fibrosi irreversibile 192 radiol med ( 2009 ) 114 : 190203 levels of accuracy in discriminating between idiopathic lung fibrosis and lung disease secondary to rheumatic disorders , and good capabilities in quantifying disease extent . 
for ssc in particular , warrick et al . [ 5 ] devised a semiquantitative method for evaluating radiological abnormalities whereby the different types of lesions are rated according to severity and extent of lung damage , leading to an overall hrct score . the goal of this study was to contribute to validating the warrick method by : ( 1 ) evaluating correlations with the main indices of lung function abnormalities in ssc with diffuse skin involvement ( dssc ) and ssc with limited skin involvement ( lssc ) ; ( 2 ) distinguishing between the fibrotic and alveolitic components of the warrick index to establish whether any of the radiological abnormalities reflect different stages of lung damage and correlate with specific lung - function abnormalities . materials and methods this study was conducted on 31 patients ( males : females 1 : 30 ; mean age 5410.4 years ) affected by ssc diagnosed on the basis of the criteria established in 1980 by the american college of rheumatology [ 6 ] and admitted to the department of rheumatology of the university of palermo . disease duration ranged from 5 months to 21 years . 
on the basis of the extent of skin involvement , 16 patients were classified as affected by dssc and the remaining 15 by lssc . all subjects tested positive for antinuclear antibody ( ana ) , 16 tested positive for anti - scl 70 , and 15 tested positive for anticentromere . 
patients with a history of allergy to organic or inorganic substances were excluded . functional evaluation each subject underwent respiratory function testing , which included spirometry , residual volume measurement with the helium dilution technique , and single - breath carbon monoxide ( co ) diffusion test . 
un significativo progresso stato realizzato con lintroduzione della tomografia computerizzata ad alta risoluzione ( hrct ) del torace che rispetto alla radiologia tradizionale si dimostrata tecnica dotata di alta sensibilit , sin dalle fasi precoci della malattia , elevata accuratezza nella discriminazione tra fibrosi idiopatica polmonare e patologia polmonare secondaria a malattie reumatiche nonch di elevata capacit nel quantificare lestensione della malattia . 
 [ 5 ] hanno elaborato un metodo di valutazione semiquantitativa delle alterazioni radiologiche che attribuisce un punteggio alle varie lesioni secondo criteri di gravit e di estensione del danno del parenchima polmonare , dalla cui somma si ottiene uno score hrct globale . 
la durata di malattia variava da 5 mesi a 21 anni . in base allestensione cutanea della malattia , 16 pazienti risultavano affetti dalla dscs e i restanti 15 dalla lscs . 
una storia di allergie a sostanze organiche o inorganiche costituiva un criterio di esclusione dallo studio . valutazione funzionale ciascun soggetto stato sottoposto ad una valutazione funzionale respiratoria comprendente la spirometria , la misura del volume residuo mediante tecnica di diluizione dellelio e test di diffusione del monossido di carbonio ( co ) radiol med ( 2009 ) 114 : 190203 hrct study all patients gave informed consent for the hrct study . scans were performed with a 4 - detector philips mx 8000 quad ( eindhoven , the netherlands ) ct scanner . 
scanning parameters were as follows : 120 kv , 170 mas , slice thickness 1 mm , interval 10 mm , acquisition time 0.8 s , smallest field of view ( fov ) providing coverage of both lungs and convolution filter for hard tissue . in the presence of mild ground - glass opacities in the posterior basal subpleural zone , a limited number of prone scans were added to exclude the possibility of gravitational effects causing increased parenchymal density . 
capacit polmonare totale ( tlc ) e la capacit di diffusione del co ( dlco ) sono state misurate ed espresse in percentuale del valore teorico di riferimento . valori inferiori all80% del teorico sono stati considerati anormali . 
per lo studio stato utilizzato uno spirometro a campana dotato di moduli per la diluizione dellelio e la misura del transfer gassoso per il co ( baires system ; biomedin , padova , italia )  . 
 studio hrct lesame hrct , previo consenso informato , stato eseguito con apparecchio tc multistrato a 4 detettori philips mx 8000 quad ( einthoven , olanda ) e lacquisizione stata realizzata con tecnica assiale , con scansioni dagli apici alle basi con paziente in posizione supina , in apnea inspiratoria , senza somministrazione di mezzo di contrasto . 
per la realizzazione dellindagine radiologica stato utilizzato un protocollo che prevede i seguenti parametri di scansione : 120 kv , 170 mas , spessore di strato 1 mm , intervallo di scansione 10 mm , tempo di scansione 0 , 8 s , campo di vista pi piccolo possibile ( fov ) che comprendesse entrambi i polmoni , filtro di convoluzione per tessuti duri . in presenza di opacit con aspetto a vetro smerigliato di lieve entit in sede mantellare basale posteriore , stato aggiunto un numero limitato di scansioni in decubito prono , allo scopo di escludere che laumentata densit parenchimale osservata non fosse dovuta a fenomeni di natura gravitazionale . 
le lesioni elementari considerate ai fini del calcolo del punteggio , cui viene attribuito uno valore crescente da 1 a 5 in relazione alla gravit del danno , sono le seguenti : 1 . 
1 areas of lung hyperintensity with ground - glass attenuation and prevalent distribution in the lower lobe ; a subpleural line is present on the right in the posterior subpleural zone . 
 [ 5 ] attribuisce inoltre un punteggio da 1 a 3 in relazione allaumentare del numero dei segmenti in cui diviso topograficamente il polmone , 194 radiol med ( 2009 ) 114 : 190203 interessati da ciascun tipo di alterazione parenchimale , ovvero punteggio 1 se la lesione in esame presente in un numero di segmenti compreso tra 1 e 3 , punteggio 2 se il numero di segmenti interessati compreso tra 4 e 9 e punteggio 3 se il numero di segmenti maggiore di 9 . 
tale metodo di valutazione semiquantitativa della malattia polmonare allhrct stato applicato anche nella valutazione delle alveoliti fibrosanti e in altre malattie interstiziali del polmone , dimostrando una bassa variabilit inter - osservatori [ 7 ]  . 
 oltre al punteggio hrct totale , abbiamo inoltre arbitrariamente distinto un indice di alveolite , che tenesse cio conto della presenza ed estensione delle opacit a vetro smerigliato , e un indice di fibrosi , che comprendesse invece alterazioni radiologiche quali gli ispessimenti settali , il polmone ad alveare e le cisti subpleuriche . 
il calcolo dellindice di alveolite stato ottenuto estrapolando il subtotale relativo alla presenza ( score di severit = 1 ) o assenza ( score di severit = 0 ) di ground glass e alla sua estensione , ovvero al numero di segmenti ove la lesione era riscontrabile ( valore di estensione da 1 a 3 ) ; ne deriva che il range di valori dellindice di alveolite compreso tra 0 e 4 . 
il calcolo dellindice di fibrosi stato ottenuto prendendo in esame le irregolarit dellinterfaccia tra pleura periferica e parenchima ( score di severit = 2 ) , le linee settali da ispessimento dei setti interlobulari e le linee subpleuriche ( score di severit = 3 ) , il polmone ad alveare ( score di severit = 4 ) e le cisti subpleuriche ( score di severit = 5 ) , e la loro estensione ( valore di estensione compreso tra 1 e 3 per ciascuna delle quattro alterazioni )  . 
 elaborazione statistica i dati sono espressi come medie e deviazione standard . lanalisi di regressione semplice stata eseguita per valutare la correlazione tra gli indici radiologici e i parametri respiratori funzionali . 
thin - walled subpleural cystic areas . furthermore , the warrick score [ 5 ] assigns a score from 1 to 3 according to the number of segments involved by each type of lesion : a score of 1 indicates that the lesion is present in from one to three segments , a score of 2 that it is present in from four to nine segments and a score of 3 that it is present in more than nine segments . 
this semiquantitative technique for hrct evaluation of lung disease has also been applied to the evaluation of fibrosing alveolitis and other interstitial lung diseases , showing a low interobserver variability [ 7 ]  . in addition to the total hrct score , we arbitrarily distinguished between an alveolitis index , based on the presence and extent of ground - glass opacities , and a fibrosis index , based on septal thickening , honeycombing and subpleural cysts . 
the alveolitis index was calculated by isolating the subtotal scores for the presence ( severity score = 1 ) or absence ( severity score = 0 ) of ground - glass attenuation and for its extent , that is , the number of lung segments exhibiting the lesion ( extent score = 13 ) ; hence , the alveolitis index score ranges from 0 to 4 . 
the fibrosis index was calculated based on irregularities in pleural margins ( severity score = 2 ) , septal lines due to thickening of the interlobular septa and subpleural lines ( severity score = 3 ) , honeycombing ( severity score = 4 ) , subpleural cysts ( severity radiol med ( 2009 ) 114 : 190203 table 1 criteria used in the warrick score tabella 1 criteri utilizzati per la valutazione del punteggio radiologico di warrick lesions and lung segments score lesions and lung segments score parenchymal abnormalities ground - glass opacities irregularities in the pleural margins septal / subpleural lines honeycomb lung subpleural cysts number of lung segments disease severity score disease extent score alterazioni parenchimali opacit a vetro smerigliato score di severit del danno ( ground glass ) irregolarit dei margini pleurici 2 linee settali / subpleuriche polmone a favo dapi cisti subpleuriche score di estensione del danno n di segmenti polmonari score = 5 ) and the extent of each of the four abnormalities ( extent score = 13 ) ; the fibrosis index score ranges from 0 to 26 . 
the alveolitis and fibrosis indices were applied to all patients , and correlations were assessed between the specific radiological abnormalities and the different forms of disease . statistical analysis senso restrittivo con alterazioni del transfer gassoso per il co in 23 soggetti ( 75% del campione ) ( tabella 2 )  . 
il confronto dei due gruppi clinici ( dssc vs lssc ) non ha mostrato differenze nei test funzionali polmonari n per quanto riguarda la tlc% del teorico ( dssc vs lssc : 89%16% vs 82%19% , p = 0 , 31 ) , n per quanto riguarda la dlco% del teorico ( dssc vs lssc : 70%21% vs 55%18% , p = 0 , 06 )  . 
 hrct results functional tests in all patients , lung - function testing showed a moderately restrictive pattern with abnormal gas transfer for co in 23 subjects ( 75% ) ( table 2 )  . 
seventeen patients lo score totale hrct secondo warrick risultato pari a 167 , 7 nel campione complessivo , senza differenze significative tra il gruppo di pazienti con forma diffusa e limitata di malattia ( dssc vs lssc : 168 vs 178 , p = 0 , 71 )  . 
 linee settali e linee subpleuriche erano lunica alterazione presente in tutti i pazienti ( 31 / 31 ) , mentre lopacit a vetro smerigliato era la seconda pi frequente alterazione riscontrata ( 18 / 31 )  . 
la correlazione tra le alterazioni radiologiche e il grado di compromissione della diffusione del co si confermata quando i punteggi hrct di estensione e di severit delle lesioni radiologiche sono stati valutati separatamente ( punteggio di estensione : r = 0 , 41 , p = 0 , 02 ; punteggio di severit : r = 0 , 39 , p = 0 , 03 )  . 
viceversa , il punteggio di estensione correlava con la tlc% del teorico 196 radiol med ( 2009 ) 114 : 190203 showed all of the abnormalities considered in the warrick index . 
septal and subpleural lines were the only abnormalities seen in all patients ( 31 / 31 ) , whereas ground - glass appearance was the second most common abnormality ( 18 / 31 )  . 
on the basis of these observations , we propose to extend the warrick method by analysing the indices separately in order to improve the characterisation of patients with scleroderma in clinical practice . hrct offers undisputed advantages in defining severity and extent of lesions in scleroderma [ 8 ]  . 
 al fine di valutare quale tipo di danno strutturale ( ground glass vs manifestazioni fibrotiche ) influenzasse specificamente le alterazioni funzionali respiratorie , sono stati utilizzati i punteggi radiologici relativi di alveolite e fibrosi . lindice di alveolite e lindice di fibrosi sono risultati rispettivamente pari a 1 , 91 , 1 e 14 , 27 , 4 . 
sulla base di queste osservazioni , lestensione del metodo di warrick attraverso lanalisi separata degli specifici indici da esso derivati pu essere proposta per una migliore caratterizzazione del paziente sclerodermico nella pratica clinica . lhrct offre vantaggi innegabili per quanto riguarda la definizione della qualit delle lesioni e della loro estensione nel paziente affetto da tale patologia [ 8 ]  . 
numerosi studi [ 9 , 10 ] hanno affrontato il tema delle correlazioni tra alterazioni morfologiche osservabili allhrct e modificazioni funzionali respiratorie nellintento di definire i rapporti patogenetici ed il valore clinico di tali alterazioni . 
come era lecito attendersi , i risultati del nostro studio confermano il rapporto tra entit del danno strutturale parenchimale , evidenziato alla hrct e alterazioni funzionali in senso restrittivo , caratterizzate da una riduzione dei volumi polmonari . 
as expected , the results of our study confirm the correlation between severity of structural parenchymal damage seen on hrct and restrictive functional abnormalities , characterised by reduced pulmonary volumes . 
this was thought to reflect the fact that evidence of fibrosis or ground - glass pattern corresponds to parenchymal lesions responsible for abnormalities in alveolocapillary diffusion , whereas other phenomena , not bili , per motivi diversi , delle alterazioni della diffusione alveolo - capillare , laddove alla base delle alterazioni della cvf si pongono altri fenomeni ( per esempio , fatica o debolezza muscolare o le alterazioni della cute del tronco ) non descritti dallhrct [ 5 ]  . 
 [ 11 ] , che hanno osservato come nei pazienti senza honeycomb lung la capacit di diffusione fosse pi bassa nei pazienti con ground glass rispetto a quelli che non presentavano tale segno , mentre una tale differenza non era riscontrabile per i volumi polmonari ; per contro tra quelli caratterizzati dal polmone ad alveare gli autori hanno osservato come valori spirometrici normali possano ancora essere rilevabili in soggetti con limitata diffusione dellhoneycomb ( < 15% ) , mentre tutti i pazienti con honeycomb diffuso ( in media 32% ) presentavano una sindrome restrittiva alla spirometria . 
 [ 11 ] , who observed that among patients without honeycomb lung , those with ground - glass opacities had lower dlco compared with those without , whereas no such difference was found for lung volumes . 
among patients with honeycomb lung , instead , the authors observed that normal spirometry values may still be detected in subjects with limited honeycombing ( < 15% ) , whereas all patients with diffuse honeycombing ( mean 32% ) showed a restrictive pattern at spirometry . thus , the available data confirm the role of the warrick index in the early stages of disease . 
 our proposal to subdivide the warrick score into two separate indices one for alveolitis and one for fibrosis dati disponibili confermano pertanto il ruolo dellindice di warrick nelle fasi precoci di malattia . 
 la nostra proposta di distinguere lo score di warrick rispettivamente in due indici , di alveolite e di fibrosi , nasce dal tentativo di introdurre degli indici parziali , che riflettano diverse fasi evolutive della malattia , in relazione alla prevalenza di peculiari alterazioni radiologiche . 
infatti , i punteggi relativi di alveolite e di fibrosi vengono ottenuti scorporando lindice di warrick , e mantenendo la divisione in estensione e gravit delle alterazioni : obiettivo quello di analizzare quali caratteristiche dellindice di warrick influenzino le alterazioni della diffusione alveolo - capillare e quali invece le alterazioni dei volumi polmonari . 
i punteggi subtotali hanno dimostrato che lindice di alveolite correla con il grado di compromissione della diffusione dei gas ma non con le alterazioni dei volumi polmonari ; al radiol med ( 2009 ) 114 : 190203 table 3 distribution of high - resolution computed tomography ( hrct ) abnormalities for each patient patients ground - glass attenuation irregularities in the pleural margins septal / subpleural lines honeycombing subpleural cysts stems from an attempt to introduce partial indices reflecting the prevalence of specific radiological abnormalities and thus the different stages of disease . 
in fact , the scores for alveolitis and fibrosis are obtained by isolating the components of the warrick index and maintaining the division into lesion severity and extent : the goal is to determine which items of the warrick index affect alveolocapillary diffusion and which affect pulmonary volumes . 
the subtotal scores showed that the alveolitis index correlates with the degree of impairment of gas diffusion but not with changes in lung volumes ; on the other hand , the fibrosis index correlates significantly with both of these functional abnormalities . 
da ci si pu dedurre che lindice di alveolite , espressione di un danno acuto e , verosimilmente , iniziale , contribuisce ad alterare la diffusione dei gas , mantenendo inalterati i volumi polmonari ; solo quando il danno si cronicizza e si estende ( aumento dellindice di fibrosi ) si assiste anche ad una compromissione dei volumi polmonari in senso restrittivo . 
tale pattern determinato da unopacit parenchimale tenue , una velatura della trasparenza che non cancella il sottostante disegno bronco - vasale . il segno del ground glass viene spesso considerato tra i reperti che si manifestano pi precocemente e rappresenta un indicatore di potenziale trattabilit e reversibilit del coinvolgimento polmonare , in quanto si assume che identifichi tabella 3 distribuzione delle alterazioni hrct per ciascun paziente pazienti aspetto a vetro smerigliato irregolarit dellinterfaccia linee settali e pleura / parenchima linee subpleuriche aspetto a favo dapi cisti subpleuriche radiol med ( 2009 ) 114 : 190203 the alveolitis index chiefly reflects changes affecting subpleural zones of the lower lobes , in which a pattern of interstitial thickening with ground - glass appearance may also be seen . 
the ground - glass pattern is often considered to be one of the earliest pulmonary manifestations and an indicator of potential treatability and reversibility of pulmonary involvement in that it is thought to represent areas of inflammation , where oedema and cells ( especially lymphocytes and / or neutrophils ) accumulate denoting the stage of active alveolitis . 
 however , a ground - glass pattern may also reflect other anatomical abnormalities : it may correspond to a thickening of the small airspaces and thus to fibrosis at a microscopic stage . 
finally , both inflammation le aree di flogosi , in cui edema e cellule ( in particolare linfociti e / o neutrofili ) si accumulano , connotando in tal modo la fase dellalveolite attiva . 
questa potenziale correlazione radiologico - funzionale potrebbe rivestire una grande importanza clinica in quanto nella scs lalveolite non trattata si accompagna ad una pi elevata mortalit [ 12 ]  . 
secondo uno studio su 15 pazienti con sclerodermia [ 14 ] , la correlazione anatomoradiologica del ground glass potrebbe essere diversa in relazione alla topografia delle lesioni : gli autori hanno correlato i risultati dellhrct con quelli della citologia del radiol med ( 2009 ) 114 : 190203 tlc % predicted dlco % predicted fig . 
4 correlazione tra lindice di alveolite e a la dlco% del teorico , b tlc% del teorico . dlco % predicted tlc % predicted and vascular abnormalities may lead to increased capillary blood volume , which contributes to forming the typical ground - glass opacity . 
according to a study performed on 15 patients with scleroderma [ 14 ] , the anatomicalradiological correlations of ground - glass opacities may differ depending on the location of the lesions : the authors correlated the findings of hrct and bronchoalveolar lavage ( bal ) repeated in two different sites either the lower lobe and lingual or the lower lobe and middle lobe . 
in the lower lobe , instead , bal ripetuto in due sedi diverse , rispettivamente nel lobo inferiore e , nei diversi casi , o nella lingula o nel lobo medio . i risultati dello studio segnalano uneccellente correlazione tra il rilievo di una alveolite e la presenza di ground glass a livello del medio o della lingula , ma non per quanto riguarda il lobo inferiore ; in questa ultima sede era invece riconoscibile una correlazione tra levidenza citologica di alveolite ed i segni hrct di franca fibrosi polmonare . 
 nellevoluzione della malattia la comparsa di un pattern reticolare o reticolo - nodulare segnala lispessimento del connettivo peribronchiale , dei setti interlobulari , dellinterstizio subpleurico oltre che dei setti intralobulari e della 202 radiol med ( 2009 ) 114 : 190203 fig . 
5 correlazione tra lindice di fibrosi e a la dlco% del teorico , b tlc% del teorico . dlco % predicted tlc % predicted there was a significant correlation between fibrosis on hrct and evidence of alveolitis on bal . 
 lung , which in the history of the disease , the appearance of a reticular or reticulonodular pattern indicates thickening of the peribronchial connective tissue , interlobular septa , subpleural airspaces and centrilobular bronchiolar walls changes that combine to create the fibrosis index . 
it is characterised by the presence of rounded cystic spaces ( 210 mm ) that are thick - walled ( 13 mm ) and arranged over several concentric layers at the subpleural level , with interposed fibrosis and consequent parenchymal architectural distortion . 
even though these lesions are typically found in peripheral locations [ 3 ] , they have also been reported in central lung regions in a non - negligible number of cases [ 15 ]  . 
as a result of the structural and functional derangements caused by the airspace disease and the traction and distortion effects on the airways , the lung pattern in ssc may be characterised by a high prevalence of bronchiectasis , as demonstrated by hrct . 
in a study of 21 patients with diffuse and limited disease , bronchiectasis was present in 59% of cases , apparently with no correlation with the diffuse or limited nature of disease or the ground - glass or fibrotic features of lesions [ 16 ]  . 
 in conclusion , the advent of new imaging modalities such as hrct has helped to expand our knowledge about this disease , allowing us to accurately define the severity and distribution of diffuse interstitial pulmonary disease and detect the presence of subclinical alveolitis . 
lapprodo del percorso evolutivo rappresentato dal polmone ad alveare , che costituisce evidenza patognomonica dellend - stage lung : esso si caratterizza per la presenza di lacune cistiche rotondeggianti ( 210 mm ) che condividono pareti spesse ( 13 mm di spessore ) e si dispongono su pi strati concentrici a livello subpleurico , con tessuto fibroso interposto e distorsione consequenziale della normale architettura parenchimale . 
anche se la disposizione periferica di queste lesioni caratteristica [ 3 ] , stato segnalato come esse possano non risparmiare le zone centrali del polmone in un numero non trascurabile di casi [ 15 ]  . 
in relazione al disordine strutturale e funzionale determinato dallinterstiziopatia e dagli effetti di trazione e di distorsione esercitati dal parenchima alterato sulle vie aeree , il quadro del polmone nella scs pu essere caratterizzato da una elevata prevalenza di bronchiectasie , come dimostrato dallhrct : in uno studio condotto su 21 pazienti con malattia estesa e limitata le bronchiectasie erano presenti nel 59% dei casi , senza apparente relazione col carattere esteso o limitato della malattia o con le caratteristiche di ground glass o fibrosi presentate dalle lesioni [ 16 ]  . 
 in conclusione , lavvento di nuove tecniche di diagnostica per immagini come lhrct ha contribuito negli anni ad ampliare le conoscenze su questo tema , consentendo di definire con accuratezza lentit e la distribuzione della pneumopatia interstiziale diffusa , evidenziando precocemente la presenza di alveolite subclinica . 
pertanto , la disponibilit di uno score per la valutazione semiquantitativa della radiol med ( 2009 ) 114 : 190203 radiological impairment has a major impact on clinical practice , as it allows the clinician to make appropriate treatment decisions and provides an adequate tool for the follow - up . however , the clinical significance of findings of early and ill - defined impairment remains to be investigated , and further studies that include patients with more severe structural pulmonary impairment are required to define the diagnostic and prognostic roles of the partial radiological indices . compromissione radiologica riveste una notevole importanza pratica , consentendo al clinico le opportune valutazioni ai fini terapeutici , e fornendo un mezzo adeguato per un accurato follow up . 
sardanelli1 1servizio di radiologia , dipartimento di scienze medico - chirurgiche , universit degli studi di milano , irccs policlinico san donato , via morandi 30 , 20097 san donato milanese , italy 2servizio di radiologia , irccs istituto ortopedico galeazzi , via r . 
galeazzi 4 , 20161 milano , italy 3unit di ortopedia , dipartimento di scienze medico - chirurgiche , universit degli studi di milano , irccs policlinico san donato , via morandi 30 , 20097 san donato milanese , italy correspondence to : a . 
for each sequence , we evaluated the visibility of the anatomical structures of the central pivot , lateral compartment , and anterior compartment using a semiquantitative score ( 0 = total masking ; 1 = insufficient visibility ; 2 = sufficient visibility ; 3 = optimal visibility )  . 
the visibility index ranged between 83% and 89% for the first four sequences without significant differences among them , 58% for stir and 11%36% for the last five sequences . significant differences were found between each of the four first sequences and the remaining sequences ( p < 0.004 ) and riassunto obiettivo . 
quattro pazienti portatori di protesi monocompartimentale mediale oxford iii sono stati sottoposti a rm a 1 , 5 t mediante scansioni coronali : spinecho ( se ) pesata in t1 ; turbo - se ( tse ) pesata in t1 ; tse pesata in densit protonica ( dp ) e t2 ; gradient - echo ( ge ) pesata in t1 ; short tau inversion recovery ( stir ) ; multi echo data image combination ( medic ) ; ge pesata in t2 * ; volumetric interpolated breath - hold examination ( vibe ) ; dual echo steady state ( dess )  . 
per ciascuna sequenza stata valutata la visibilit delle strutture anatomiche del pivot centrale , del compartimento laterale e del compartimento anteriore mediante un punteggio semiquantitativo ( 0 = totale mascheramento ; 1 = insufficiente riconoscibilit ; 2 = sufficiente riconoscibilit ; 3 = ottimale riconoscibilit )  . 
lindice di riconoscibilit risultato tra l83% e l89% per le prime quattro sequenze , senza differenze significative tra loro , 58% per la stir e tra l11% e il 36% per le ultime cinque sequenze . 
le sequenze se , tse e stir potrebbero essere utilmente incluse in un protocollo per lo studio del ginocchio con protesi monocompartimentale mediale . parole chiave ginocchio protesi monocompartimentali risonanza magnetica introduction introduzione medial unicompartmental knee replacement is considered a valid surgical option for patients affected by medial arthritis [ 14 ]  . 
long - term clinical results are optimal , with reported rates of implant survival equal to 97% at 10 years [ 6 ] and 94% at 15 years [ 7 ]  . middleand long - term evaluation of the remaining anatomical structures of the knee , in particular progression of arthritis of the untreated compartment [ 8 , 9 ] , should be performed with dedicated imaging techniques . 
whereas bone segments can be studied using radiographic examinations [ 8 , 10 , 11 ] , synovial and capsular structures and collateral ligaments can be investigated with ultrasound , an approach already proposed for evaluating soft tissues after total knee arthroplasty [ 12 ]  . 
no real solution , however , exists for evaluating the lateral and anterior compartments ( in particular , bone , cartilage and lateral meniscus ) or structures of the central pivot of knees treated with medial unicompartmental arthroplasty . magnetic resonance ( mr ) imaging is considered an optimal technique for imaging the knee and evaluating new therapeutic approaches [ 13 , 14 ]  . 
until now , mr imaging of the replaced knee has been practically considered to be contraindicated , even though pilot experiences of mr imaging of the knee after total arthroplasty have been reported [ 15 , 16 ]  . 
in fact , metallic objects inside the human body generate artefacts on mr images , and such artefacts vary in size and type according the radiofrequency sequence used and its technical parameters [ 17 ]  . 
gradient - echo ( ge ) sequences are more sensitive ( and thus produce larger artefacts ) when compared with spin - echo ( se ) sequences , and the size of the artefact increases as t2 * weighting increases [ 1820 ]  . 
therefore , orthopaedic metallic devices are generally considered a possible limitation for mr imaging , being a possible source of masking the anatomical districts to be studied [ 20 ]  . 
in particular , the current opinion is that in the limpianto di una protesi monocompartimentale mediale ( pmcm ) del ginocchio da tempo considerato una valida opzione chirurgica per il trattamento dellartrosi del compartimento mediale [ 14 ]  . 
la prognosi a lungo termine ottimale : sono state riportate sopravvivenze medie delle pmcm a 10 anni del 97% [ 6 ] , a 15 anni del 94% [ 7 ]  . la valutazione a medio e lungo termine delle strutture anatomiche residue , in particolare la progressione artrosica del compartimento laterale [ 8 , 9 ] , necessita di un utilizzo appropriato di tecniche di imaging . 
mentre lo studio delle strutture ossee agevolmente condotto mediante indagini radiografiche [ 8 , 10 , 11 ] , quello della sinovia , delle strutture capsulari e dei legamenti collaterali si giova dellapproccio ecografico , gi proposto per il follow - up delle protesi totali [ 12 ]  . 
resta aperto , nei pazienti con pmcm , il problema della valutazione dei compartimenti laterale e anteriore ( con particolare riferimento alle strutture osteocartilaginee e al menisco laterale ) , oltre che delle strutture del pivot centrale . la risonanza magnetica ( rm ) oggi considerata tecnica di imaging ottimale nello studio del ginocchio , anche relativamente alla valutazione di approcci terapeutici innovativi [ 13 , 14 ]  . 
fino ad oggi , nei pazienti con protesi del ginocchio la rm stata ritenuta sostanzialmente controindicata ai fini della valutazione del ginocchio operato , anche se sono state riportate alcune esperienze pilota nello studio rm di pazienti con protesi totali [ 15 , 16 ]  . 
infatti , la presenza di oggetti metallici intracorporei genera nelle immagini rm artefatti che variano a seconda del tipo di sequenza di impulsi a radiofrequenza e dei suoi parametri tecnici [ 17 ]  . 
in generale le sequenze gradient - echo ( ge ) sono pi sensibili ( e quindi producono artefatti di maggiori dimensioni ) rispetto a quelle spinradiol med ( 2009 ) 114 : 301311 presence of total arthroplasty of the knee , mr imaging does not allow a reliable evaluation of even superficial structures such as the quadriceps tendon , patellar tendon and collateral ligaments , which are better investigated with ultrasound [ 12 ]  . 
 the aim of our study was to test a series of mr sequences for evaluating the knee after medial unilateral arthroplasty in order to identify sequences that provide images affected by smaller artefacts and thus of potential use for assessing the anterior and lateral compartments and the central pivot . materials and methods patients between june and september 2005 , four symptomatic patients ( two women aged 60 and 65 years and two men aged 67 and 79 years ) who had undergone medial unicompartmental arthroplasty ( oxford iii , biomet , london , uk ) underwent mr imaging of the treated knee . 
this implant is composed of two metallic devices ( cobaltchromemolybdenum alloy ) implanted into the medial femoral condyle and into the corresponding portion of the tibial plate , which can be easily recognised at radiography , and of a radiolucent polymer meniscus [ 10 ]  . 
 mr protocol examinations were performed with a 1.5 - t superconductive magnet , 40 - mt / m gradient power and a 20 - cm flexible coil surrounding the knee ( sonata maestro class , siemens , erlangen , germany )  . 
in fact , whereas the sagittal scan plane would have prevented direct evaluation of mediolateral extent of artefacts , the axial scan plane would have allowed the direct evaluation of mediolateral and anteroposterior extent of artefacts ( though not the craniocaudal extent ) , but only with a far higher number of slices compared with coronal scanning and , as a consequence , longer scan time . 
 we tested seven sequences commonly used in musculoskeletal mr imaging : t1 - weighted se , t1 - weighted echo ( se ) e lentit dellartefatto aumenta col crescere della pesatura in t2 * [ 1820 ]  . 
per tale motivo , le protesi metalliche ortopediche sono in generale considerate condizioni potenzialmente limitanti lindagine rm in quanto potenziale fonte di mascheramento delle regioni anatomiche oggetto di studio [ 20 ]  . 
in particolare , in presenza di protesi totali del ginocchio , secondo lopinione corrente la rm non consente una valutazione affidabile neppure di strutture superficiali quali il tendine del quadricipite , i legamenti collaterali e il tendine rotuleo , per le quali appare nel complesso superiore il contributo diagnostico dellecografia [ 12 ]  . 
 scopo dello studio stato testare una serie di sequenze rm per lo studio del ginocchio trattato con pmcm al fine di identificare quelle che consentono di ottenere immagini gravate da minori artefatti , quindi potenzialmente utili per lo studio del pivot centrale e dei compartimenti anteriore e laterale . materiali e metodi pazienti tra giugno e settembre 2005 , 4 pazienti sintomatici ( 2 femmine di 60 e 65 anni e 2 maschi di 67 e 79 anni ) portatori di pmcm oxford iii ( biomet , london , uk ) sono stati sottoposti a rm del ginocchio protesizzato . 
tale protesi costituita da due componenti metalliche in lega al cobaltocromo - molibdeno impiantate sul condilo femorale mediale e sul corrispondente emipiatto tibiale , ben riconoscibili allesame radiografico , e da un menisco in polimero radiotrasparente [ 10 ]  . 
 protocollo rm le indagini sono state eseguite con apparecchiatura a magnete superconduttivo operante a 1 , 5 t , gradienti con potenza di 40 - mt / m ( sonata maestro class , siemens , erlangen , germania ) e bobina flessibile ( 20 cm ) posta a circondare larticolazione . 
infatti , mentre il piano sagittale non avrebbe permesso la valutazione diretta dellestensione medio - laterale degli artefatti , il piano assiale avrebbe s 304 radiol med ( 2009 ) 114 : 301311 turbo - se ( tse ) , proton - density ( pd ) and t2weighted tse , t1 - weighted spoiled ge ( fast low - angle shot ) , shorttau inversion recovery ( stir ) and multi - echo data image combination ( medic )  . 
moreover , to investigate artefact extent on images obtained with sequences highly sensitive to magnetic inhomogeneity , we tested a t2 * - weighted spoiled ge sequence and two three - dimensional sequences : the volumetric interpolated breath - hold examination ( vibe ) and the dual - echo steady - state ( dess ) sequences . 
each of the four patients remained in our department about 30 min after the examination and was asked if she or he had any discomfort during or after the exa image analysis for each of the ten sequences , two radiologists with about consentito la valutazione diretta dellestensione mediolaterale e antero - posteriore degli artefatti ( rinunciando a quella cranio - caudale ) ma con un numero di strati molto pi elevato rispetto al piano coronale e , quindi , tempi di scansione prolungati . 
 sono state testate sette sequenze tra quelle pi utilizzate in rm muscolo - scheletrica : se pesata in t1 ; turbo - se ( tse ) pesata in t1 ; tse pesata in densit protonica ( dp ) e t2 ; ge con spoiler ( fast low angle shot ) pesata in t1 ; short tau inversion recovery ( stir ) ; multi echo data image combination ( medic )  . 
allo scopo di verificare lestensione degli artefatti in sequenze ad alta sensibilit alla disomogeneit magnetica , sono state altres testate una sequenza ge con spoiler pesata in t2 * e due sequenze con acquisizione table 1 technical parameters of ten mr sequences used in four patients for the 1.5 - t study of the knee with unicompartmental oxford iii biomet arthroplasty sequences tr ( ms ) te ( ms ) flip angle thickness ( mm ) number of slices acquisition time ( min : sec ) tr , time of repetition ; te , time of echo ; pd , proton density ; tse , turbo spin - echo ; se , spin - echo ; stir , short tau inversion - recovery ; ge , gradient - echo ; dess , double echo in the steady state ; vibe , volumetric interpolated breath - hold examination ; medic , multi echo data image combination . 
for all sequences : matrix 256256 ; field of view 200200 mm ; number of excitations , nex = 1 , with the exception of t1and t2 * - weighted ge sequences ( nex = 2 )  . 
per tutte le sequenze : matrice 256256 ; campo di vista 200200 mm ; numero di eccitazioni , nex = 1 , ad eccezione delle sequenze ge t1e t2 * - pesate ( nex = 2 )  . 
 a tempo di interpulso = 130 ms radiol med ( 2009 ) 114 : 301311 10 and 4 years , respectively , of experience in musculoskeletal mr imaging rated in consensus the visibility of the anatomical structures of the central pivot ( cruciate ligaments ) , lateral compartment ( femoral and tibial bone and cartilages ; lateral meniscus ; capsule and lateral collateral ligament ) and anterior compartment ( femoral and tibial bone and cartilages ; hoffa fat pad , patellar tendon )  . we used a semiquantitative scoring system for the visibility of anatomical structures related either to the presence of image artefacts or to the contrast resolution for each sequence ( 0 = total masking ; 1 = insufficient visibility ; 2 = sufficient visibility ; 3 = optimal visibility )  . 
 statistical analysis differences among the visibility indexes of the ten sequences were globally evaluated with the friedman test . post hoc analysis for direct comparison between pairs of sequences was performed using the sign test . 
none of the four patients reported pain , heat or other local discomfort either during the examination or during the following 30 m visibility indexes of anatomical structures obtained with each of the ten sequences are reported in table 2 . 
nonsignificant differences ( p = 0.733 , friedman test ) were observed among the visibility indexes of the first four sequences ( pdand t2weighted tse , t1weighted se , and t1 - weighted tse )  . the visibility indexes of the first four sequences were significantly higher ( p < 0.004 , sign test ) than those of the remaining six sequences . 
visibility index of the stir sequence ( fifth , decreasing order ) was significantly higher ( p < 0.008 , sign test ) than that of the last five sequences ( t1and t2 * - weighted ge , dess , vibe , medic )  . 
the difference between the visibility index of the t1 - weighted ge tridimensionale , volumetric interpolated breath - hold sequence ( vibe ) e dual echo steady state ( dess )  . 
ciascuno dei quattro pazienti rimasto in reparto in osservazione per circa 30 minuti dopo lesecuzione dellindagine ed stato interrogato sulleventuale insorgenza di qualsiasi disturbo durante e dopo lindagine . analisi delle immagini due radiologi con circa 10 e 4 anni di esperienza in rm muscolo - scheletrica hanno valutato in consenso , per ciascuna sequenza , la visibilit delle strutture anatomiche del pivot centrale ( legamenti crociati ) , del compartimento laterale ( osso e cartilagine femorale e tibiale ; menisco laterale ; capsula e legamento collaterale laterale ) , del compartimento anteriore ( osso e cartilagine femorale e tibiale ; corpo di hoffa ; tendine rotuleo )  . 
 stato utilizzato un punteggio semiquantitativo di riconoscibilit delle strutture anatomiche in relazione alla presenza di artefatti e alla risoluzione di contrasto della sequenza ( 0 = totale mascheramento ; 1 = insufficiente riconoscibilit ; 2 = sufficiente riconoscibilit ; 3 = ottimale riconoscibilit )  . 
la somma dei punteggi riportati da ciascuna sequenza in ciascuno dei tre compartimenti e per tutti e quattro i pazienti stata divisa per il valore massimo ottenibile ( score = 3 per i tre compartimenti e per ognuno dei quattro pazienti , cio 334 = 36 ) , ottenendo per ciascuna sequenza un indice percentuale di riconoscibilit . 
 analisi statistica le differenze tra gli indici di riconoscibilit delle dieci sequenze sono stati globalmente valutati con il test di friedman ; lanalisi post - hoc per il confronto delle differenze tra gli indici di riconoscibilit di coppie di sequenze stata eseguita con il test dei segni . 
valori di p inferiori a 0 , 05 sono stati considerati significativi . risultati lindagine rm durata circa 3032 minuti , 24 dei quali per il tempo di acquisizione delle dieci sequenze , i rimanenti 68 minuti per il posizionamento del paziente , le sequenze di centratura e la discesa del paziente dal lettino . nessuno dei quattro pazienti ha lamentato dolore , riscaldamento o altre sensazioni locali durante lindagine o nei 30 minuti successivi . 
 arapporto percentuale tra la somma dei punteggi e il valore massimo ottenibile ( vedi testo ) and that of the t2 * - weighted ge was not significant ( p = 0.453 , sign test )  . 
this result was expected , given that orthopaedic implants are generally defined not as real contraindications to the study but as patient conditions possibly limiting the diagnostic effectiveness of the examination ; that is , as a possible source of image artefacts in the body region being investigated [ 22 ]  . secondly , comparison among sequences confirmed the in ordine decrescente in tabella 2 . 
non sono state osservate differenze significative ( p = 0 , 733 , test di friedman ) tra gli indici di riconoscibilit delle prime quattro sequenze ( tse dpe t2 - pesata , se t1 - pesata e tse t1 - pesata )  . 
lindice di riconoscibilit della sequenza stir ( quinta in ordine decrescente ) risultato significativamente maggiore ( p < 0 , 008 , test dei segni ) di quello delle ultime cinque sequenze ( ge t1e t2 * - pesata , dess , vibe , medic )  . 
1a - h comparison among magnetic resonance ( mr ) sequences used at 1.5 t for studying the knee after unicompartmental arthroplasty ( coronal plane , anterior compartment ) : a t1 - weighted turbo spin - echo ( tse ) ; b proton - density - weighted tse ; c t2 - weighted tse ; d short - tau inversion recovery ( stir ) ; e gradient - echo ( ge ) t2 * - weighted ; f dual - echo steady state ( dess ) ; g multi - echo data image combination ( medic ) ; h volumetric interpolated breath - hold examination ( vibe )  . 
note the visibility of the patellar tendon only in a , b , c , and d ( full arrow ) , whereas in the remaining images , the artefact entirely masks the image below the patellar apex . 
1a - h comparazione tra sequenze rm ( 1 , 5 t ) per lo studio del ginocchio con protesi monocompartimentale mediale ( piano coronale , compartimento anteriore ) : a turbo spin - echo ( tse ) pesata in t1 ; b tse pesata in densit protonica ; c tse pesata in t2 ; d short tau inversion - recovery ( stir ) ; e gradientecho ( ge ) pesata in t2 ; f dual echo steady - state ( dess ) ; g multi echo data image combination ( medic ) ; h volumetric interpolated breath - hold examination ( vibe )  . 
si osservi come il tendine rotuleo sia riconoscibile solo in a , b , c e d ( freccia piena ) mentre lartefatto metallico maschera completamente limmagine caudalmente allapice rotuleo . 
in b , c e d la sottile linea arcuata artefattuale non compromette la riconoscibilit del tendine rotuleo ( freccia vuota )  . higher sensitivity of the ge sequences to magnetic susceptibility artefacts when compared with se sequences [ 18 , 19 , 22 ]  . 
moreover , t1weighted ge sequences obtained a visibility index ( 36% ) that was slightly higher , though not significant ( p = 0.453 ) , than that of t2 * - weighted ge sequences ( 31% ) due to the effect of t2 * weighting , which emphasises image artefacts [ 18 , 19 ]  . 
however , neither of these sequences appeared to be diagnostic . in our study , the spatial relationship between the coronal scans and the course of the patellar tendon limited its evaluation . 
sagittal or axial scans allowed a better evaluation of due sequenze ge t1e t2 * - pesate risultata non significativa ( p = 0 , 453 , test dei segni )  . 
4. discussione i risultati del presente studio indicano in primo luogo che lindagine rm del ginocchio a 1 , 5 t in presenza di pmcm non comporta linsorgenza di eventi avversi durante o dopo lesecuzione della stessa . 
tale risultato era atteso in ragione della generale definizione delle protesi ortopediche non come controindicazioni ma come condizioni potenzialmente limitanti lindagine , ovvero fonte potenziale di artefatti nellambito della regione studiata [ 22 ]  . 308 radiol med ( 2009 ) 114 : 301311 fig . 
2a - h comparison among magnetic resonance ( mr ) sequences used at 1.5 t for studying the knee after unicompartmental arthroplasty ( coronal plane , central pivot ) : a t1 - weighted turbo spin - echo ( tse ) ; b proton - density - weighted tse ; c t2 - weighted tse ; d short - tau inversion recovery ( stir ) ; e gradient - echo ( ge ) t2 * - weighted ; f dual - echo steady state ( dess ) ; g multi - echo data image combination ( medic ) ; h volumetric interpolated breath - hold examination ( vibe )  . 
note that the anterior cruciate ligament is visualised only in a , b , c and d ( arrow ) , whereas in the remaining images , the artefact masks entirely the central pivot and partially the lateral condyle , allowing limited visibility of the lateral meniscus . 
2a - h comparazione tra sequenze rm ( 1 , 5 t ) per lo studio del ginocchio con protesi monocompartimentale mediale ( piano coronale per il pivot centrale ) : a turbo spin - echo ( tse ) pesata in t1 ; b tse pesata in densit protonica ; c tse pesata in t2 ; d short tau inversion - recovery ( stir ) ; e gradientecho ( ge ) pesata in t1 ; f ge pesata in t2 * ; g dual echo steady - state ( dess ) ; h multi echo data image combination ( medic )  . 
si osservi come il legamento crociato anteriore sia riconoscibile solo in a , b , c e d ( freccia ) mentre nelle restanti immagini lartefatto maschera interamente il pivot centrale e parzialmente il condilo laterale consentendo una limitata riconoscibilit del menisco laterale . 
 the stir sequence , even though limited by an overall visibility index ( 58% ) significantly lower than those of the first four se and tse sequences , must be regarded as a useful approach due to its high sensitivity for fluid collections and soft tissue and spongy bone oedema . 
the structure of the stir sequence used by us is that of an inversion pulse ( ti = 130 ms ) lowering the fat signal , in secondo luogo , il confronto tra sequenze ha confermato la maggiore sensibilit agli artefatti da suscettivit magnetica delle sequenze ge rispetto a quelle se [ 18 , 19 , 22 ]  . 
3a - h comparison among magnetic resonance ( mr ) sequences used at 1.5 t for studying the knee after unicompartmental arthroplasty ( coronal plane , lateral compartment ) : a t1 - weighted turbo spin - echo ( tse ) ; b proton - density - weighted tse ; c t2 - weighted tse ; d short - tau inversion recovery ( stir ) ; e gradient - echo ( ge ) t2 * weighted ; f dual - echo steady state ( dess ) ; g multi - echo data image combination ( medic ) ; h volumetric interpolated breath - hold examination ( vibe )  . 
in the area indicated by the oval in a , b , c and d , all anatomical structures can be recognised , in particular , the lateral portion of the capsule , lateral collateral ligament , external femorotibial joint space and lateral meniscus . 
3a - h comparazione tra sequenze rm ( 1 , 5 t ) per lo studio del ginocchio con protesi monocompartimentale mediale ( piano coronale per il compartimento laterale ) : a turbo spin - echo ( tse ) pesata in t1 ; b tse pesata in densit protonica ; c tse pesata in t2 ; d short tau inversion - recovery ( stir ) ; e gradient - echo ( ge ) pesata in t1 ; f ge pesata in t2 * ; g dual echo steady - state ( dess ) ; h volumetric interpolated breath - hold examination ( vibe )  . nellarea compresa dallovale in a , b , c e d si riconoscono tutte le strutture , in particolare il compartimento capsulare laterale , il legamento collaterale laterale , la rima articolare femoro - tibiale esterna e il menisco esterno . 
we did not perform sequences with spectral fat saturation due to their high sensitivity to the magnetic field distortion determined by the presence of ferromagnetic material [ 24 , 25 ] and to avoid a longer total examination time . 
on the basis of these results , an mr imaging protocol including sagittal t1weighted se , coronal pd - weighted tse , axial t2 - weighted tse and sagittal and coronal stir sequences could be used to study the knee with unicompartmental arthroplasty . our experience confirms the absence of contraindications to mr imaging for patients with joint replacement . 
in particular , for unicompartmental knee arthroplasty , mr imaging could be a diagnostic tool for evaluating the progression of arthritis of the lateral compartment and associated cartilage and meniscal changes and assessing the fini diagnostici : la pesatura in t2 * enfatizza gli artefatti [ 18 , 19 ]  . nelle sequenze coronali da noi utilizzate langolazione del piano di scansione rispetto al decorso del tendine rotuleo ne ha limitato la valutazione diagnostica che avrebbe potuto essere ottimizzata da piani di scansione sagittali o assiali . 
4 visibility index of the anatomical structures of the central pivot , anterior compartment , and lateral compartment of ten magnetic resonance ( mr ) sequences ( 1.5 t ) used to study the knee after medial unicompartmental arthroplasty . 
4 grafico a barre dellindice di riconoscibilit delle strutture anatomiche del pivot centrale , del compartimento anteriore del compartimento laterale per dieci diverse sequenze utilizzate per lo studio rm del ginocchio con protesi monocompartimentale a 1 , 5 t . 
the diagnostic value and clinical efficacy of this information require investigation with a specifically designed prospective study . radiol med ( 2009 ) 114 : 301311 prime quattro sequenze ( se e tse ) , rappresenta un approccio utile in virt dellelevata sensibilit alle raccolte liquide e alledema sia dei tessuti molli che , in particolare , dellosso spongioso . 
la struttura delle sequenza stir da noi utilizzata , del resto , quella di una sequenza tse t2pesata ( te = 54 ms ) preceduta da un impulso di inversione ( ti = 130 ms ) che abbatte il segnale del grasso . 
si deciso di non eseguire sequenze con saturazione spettrale del grasso in quanto marcatamente sensibili alla distorsione del campo magnetico determinata dalla presenza di materiale ferromagnetico [ 24 , 25 ] e per non prolungare la durata dellesame . 
in particolare , per le pmcm di ginocchio , indica nella rm una tecnica diagnostica che potrebbe fornire informazioni circa la progressione dellartrosi del compartimento laterale e delle associate degenerazioni cartilaginee e meniscali , nonch sullarticolazione femoro - rotulea e delle sue superfici cartilaginee , non valutabili con tecniche di imaging alternative . 
sardanelli2 1unit of breast imaging , university of genoa and san martino hospital , largo rosanna benzi 10 , 16132 genoa , italy 2department of medical and surgical sciences , university of milan school of medicine , unit of radiology , irccs policlinico san donato , via morandi 30 , 20097 san donato milanese , milan , italy 3unit of cytopathology , university of genoa and san martino hospital , largo rosanna benzi 10 , 16132 genoa , italy 4department of worldwide medical & regulatory affairs , bracco imaging spa , via e . 
a number of women who should undergo magnetic resonance ( mr ) imaging of the breast cannot use this diagnostic tool due to claustrophobia or excessive body size for the restricted confines of standard closed mr systems . 
the standard of reference was pathological examination for 16 lesions classified with a maximal breast imaging reporting and data system ( bi - rads ) score from 3 to 5 , fine - needle aspiration cytology and ( cid : 2 ) 2 - year follow - up for two lesions classified as bi - rads 3 , and ( cid : 2 ) 2 - years follow - up for five lesions classified as bi - rads 2 . 
le donne claustrofobiche o obese non possono eseguire la rm mammaria nei comuni magneti chiusi . nostro obiettivo stato valutare la performance diagnostica di un sistema aperto a basso campo per lo studio rm mammario dinamico in queste pazienti , utilizzando un mezzo di contrasto paramagnetico ad alta relassivit . 
stata eseguita sequenza gradient - echo dinamica 3d t1 - pesata ( risoluzione temporale = 94 secondi ) con gadobenato dimeglumina ( 0 , 1 mmol / kg )  . 
tre lesioni ( due tumori invasivi e una cisti ) non erano valutabili per la presenza di artefatti da movimento e sono state considerate come due falsi negativi e un falso positivo . performance diagnostica : sensibilit 86% ( 13 / 15 ; ic [ intervallo di confidenza ] 95% 70% , 100% ) ; specificit 87% ( 7 / 8 ; ic 95% 65% , 100% ) ; accuratezza 87% ( 20 / 23 ; 268 radiol med ( 2009 ) 114 : 267285 95% ci : 73%100% ) were obtained . 
in pazienti claustrofobiche o obese la rm mammaria a basso campo e magnete aperto con gadobenato dimeglumina consente una buona perfomance diagnostica . parole chiave mammella , tumori risonanza magnetica magneti aperti a basso campo gadobenato dimeglumina ( gd - bopta ) introduction introduzione magnetic resonance ( mr ) imaging of the breast is typically performed using 1.5 - t closed magnets [ 19 ]  . 
unfortunately , a number of women who should undergo mr imaging of the breast cannot use this diagnostic tool due to claustrophobia [ 10 ] or a body size that is too large for the restricted confines of closed systems [ 11 ]  . 
furthermore , the studies conducted at low field strength have been performed only with conventional contrast agents with standard r1 relaxivities of approximately 3.74.6 l mmol1 s1 ( as measured at 1.5 t ) [ 17 , 18 ]  . an inherent limitation of low - field magnets for diagnostic mr imaging of the breast is the reduced signal - tonoise ratio attainable compared with that attainable at higher field strengths . 
numerous studies have shown not only that gadobenate dimeglumine is effective for breast mr imaging [ 1922 ] but also that it offers improved diagnostic performance compared with gadopentetate dimeglumine administered at equivalent doses [ 23 ]  . our purpose was to evaluate the diagnostic performance of breast mr imaging on an open low - field magnet in la risonanza magnetica ( rm ) mammaria tipicamente eseguita con magneti chiusi a 1 , 5 t [ 19 ]  . 
un numero limitato di studi ha valutato la performance diagnostica delle indagini rm a contrasto dinamico a basso campo , per lo pi a fini interventistici ( biopsie e centraggi rm - guidati ) [ 1215 ] , e la stragrande maggioranza degli studi di rm mammaria allo stato dellarte sono realizzati con campi magnetici pi elevati che consentono migliori performance tecniche ( superiore risoluzione spaziale e temporale ) [ 1 , 16 ]  . 
occorre inoltre considerare che tutti gli studi a basso campo sono stati condotti con gli usuali mezzi di contrasto caratterizzati da relassivit r1 nellintervallo tra 3 , 7 e 4 , 6 l mmol1 s1 ( misurate a 1 , 5 t ) [ 17 , 18 ]  . unintrinseca limitazione allutilizzo di magneti a bassa intensit di campo per limaging mammario a rm il ridotto rapporto segnale / rumore rispetto a quello ottenibile con intensit di campo pi elevate . 
una possibilit di superare questa limitazione lutilizzo di mezzi di contrasto con relassivit r1 maggiore di quella dei mezzi di contrasto usuali . tale potenziale vantaggio offerto dal gadobenato dimeglumina ( multihance , gd - bopta ; bracco imaging spa , milano , italia ) la cui relassivit r1 nel plasma umano a 0 , 2 t ( 10 , 9 l mmol1 s1 ) circa doppia rispetto a quella del gadopentetato dimeglumina ( gd - dtpa ) ( 5 , 7 l mmol1 s1 ) [ 18 ]  . molteplici studi hanno dimostrato lefficacia del gadobenato dimeglumina per la rm mammaria [ 1922 ] , con migliore performance diagnostica rispetto al gadopentetato dimeglumina somministrato alla stessa dose [ 23 ]  . il nostro obiettivo stato valutare la performance diagnostica della rm mammaria a basso campo con magnete aperto in pazienti che non potevano essere sottoposte a indagine standard con magnete chiuso ad alto campo per ragioni psicologiche o fisiche , utilizzando come mezzo di contrasto il gadobenato dimeglumina . 
 radiol med ( 2009 ) 114 : 267285 patients who were precluded from undergoing standard mr imaging with a closed higher - field magnet for psychological or physical reasons using gadobenate dimeglumine as a contrast agent . materiali e metodi disegno dello studio e pazienti materials and methods study design and patient population from march 2002 to septemper 2004 , a total of 397 consecutive breast mr examinations were performed in genoa at the san martino university hospital . 
the low - field examinations were performed because of claustrophobia ( the patients refused the examination on the closed magnet , even with medication ) in 15 cases or large body size in three cases ( the patients were unable to enter the closed magnet ) ( table 1 )  . 
all 18 patients [ age 4816 years ; meanstandard deviation ( sd ) ] were specifically informed about the potential limitations of the mr exam performed at low field with a body coil , including the possibility of missing malignant lesions . 
the clinical indications for breast mr in these 18 patients were presurgical cancer staging ( n = 12 ) , high familial risk of breast cancer ( n = 4 ) and suspected local cancer recurrence ( n = 2 )  . 
 clinical breast examination and conventional imaging clinical breast examination ( cbe ) and mammography and / or ultrasound ( us ) were performed on the 18 patients as part of their clinical care ( table 1 )  . 
fourteen patients also underwent bilateral two - view screen - film mammography with additional projections as necessary ( mammomat 2000 , siemens medical solutions , erlangen , germany )  . 
because a dedicated breast coil tra marzo 2002 e settembre 2004 presso lazienda ospedale san martino e cliniche universitarie convenzionate ( genova ) sono state eseguite 397 indagini rm mammarie consecutive . 
di queste 397 indagini , 379 ( 95 , 5% ) sono state eseguite a 1 , 5 t ( vision , siemens , erlangen , germania ) con bobina dedicata bilaterale . 
si trattava di 15 pazienti claustrofobiche ( che avevano rifiutato di eseguire lindagine con magnete chiuso , anche con sedazione ) e di tre pazienti obese ( che non riuscivano ad entrare nel magnete chiuso ) ( tabella 1 )  . 
tutte le 18 pazienti ( et 4816 anni [ mediadeviazione standard ] ) sono state specificamente informate circa i potenziali limiti dellindagine rm eseguita a basso campo con bobina body , inclusa la possibilit di mancata diagnosi di lesioni maligne . 
le indicazioni allindagine erano : stadiazione prechirurgica ( n = 12 ) ; alto rischio familiare di tumore mammario ( n = 4 ) ; sospetta recidiva locale ( n = 2 )  . lo studio stato approvato dal comitato etico e tutte le 18 pazienti hanno fornito consenso informato scritto . 
 visita senologica , mammografia ed ecografia in tutte le 18 pazienti sono state eseguite visita senologica ( vs ) e mammografia e / o ecografia nel contesto dellusuale iter diagnostico ( tabella 1 )  . 
 risonanza magnetica stato utilizzato un sistema aperto operante a 0 , 2 t ( concerto , siemens medical solutions , erlangen , germania ) con gradienti da 20 mt / m e slew rate di 40 t / m / s . 
 le prime due pazienti della serie sono state studiate in posizione prona ( con le braccia posizionate in avanti , anteriormente alla testa ) utilizzando alcuni cuscini e supporti in 270 radiol med ( 2009 ) 114 : 267285 radiol med ( 2009 ) 114 : 267285 272 radiol med ( 2009 ) 114 : 267285 fig . 
1a - d benign breast lesions detected at gadobenate - dimeglumine - enhanced ( 0.1 mmol / kg ) dynamic breast magnetic resonance imaging with a 0.2 - t open magnet ( patients studied in the supine position ) : coronal first postcontrast subtracted images ( a , c ) and enhancement - to - time curves ( b , d )  . 
a small , round , homogenously enhancing mass ( arrow in a ) in a 28 - year - old woman and a large inhomogenously enhancing lobulated mass ( arrow in c ) in a 24year - old woman , both at the upper outer quadrant of the left breast . 
integrating morphology and dynamics , we obtained a breast imaging reporting and data system ( bi - rads ) 3 ( probably benign ) score , in agreement with the lesion features observed at ultrasound . 
1a - d lesioni benigne alla rm mammaria a basso campo ( 0 , 2 t ) con 0 , 1 mmol / kg di gadobenato dimeglumina ( pazienti in posizione supina ) : immagini coronali sottratte della prima fase dinamica ( a , c ) e curve dinamiche ( b , d )  . 
una piccola formazione rotondeggiante con enhancement omogeneo ( freccia in a ) in una donna di 28 anni e grande formazione lobulata con enhancement disomogeneo ( freccia in c ) in una donna di 24 anni , entrambe al quadrante supero - esterno della mammella sinistra . 
in b possiamo apprezzare il modesto enhancement precoce ( 49% ; valori assoluti da 286 , 2 a 425 , 3 unit arbitrarie ) e la dinamica incrementale ( curva di tipo 1 ) della lesione di piccole dimensioni , che depongono a favore della benignit , confermata dallassenza di modificazioni al follow - up . 
la curva dinamica della lesione maggiore ( d ) presenta invece un enhancement iniziale del 104% ( da 328 , 3 a 670 , 4 unit arbitrare ) con un andamento postiniziale con wash - out non significativo ( 17 , 1 unit arbitrare , pari al 5 , 0% dellenhancement iniziale ) , ovvero una curva a plateau ( tipo 2 )  . 
a causa delle difficolt incontrate durante queste indagini ( tempo di posizionamento prolungato e relativa instabilit della posizione della paziente ) , le rimanenti 16 pazienti sono stati studiate in posizione supina con mammelle libere ( senza uso di fasce o altri mezzi di contenzione ) e con le braccia distese lungo il corpo . 
2a , b breast cancer detected at gadobenate - dimeglumine - enhanced ( 0.1 mmol / kg ) dynamic breast magnetic resonance with a 0.2 - t open magnet in a 42 - year - old patient studied in the supine position : coronal first postcontrast subtracted images ( arrow in a ) and enhancement - to - time curve ( b )  . 
2a , b carcinoma mammario alla rm mammaria a basso campo ( 0 , 2 t ) con 0 , 1 mmol / kg di gadobenato dimeglumina in paziente di 42 anni studiata in posizione supina : immagini coronali sottratte della prima fase dinamica ( freccia in a ) e curva dinamica ( b )  . 
la curva dinamica ( b ) mostra un enhancement precoce del 74% ( da 206 , 6 a 359 , 1 unit arbitrarie ) e wash - out postiniziale ( curva di tipo 3 )  . 
3a , b breast cancer detected at gadobenate - dimeglumine - enhanced ( 0.1 mmol / kg ) dynamic breast magnetic resonance with a 0.2 - t open magnet in a 82 - year - old patient studied in the supine position : coronal first postcontrast subtracted image ( arrows in a ) and percent enhancement - to - time curve ( b )  . 
3a , b carcinoma mammario alla rm mammaria a basso campo ( 0 , 2 t ) con 0 , 1 mmol / kg di gadobenato dimeglumina in paziente di 82 anni studiata in posizione supina : immagini coronali sottratte della prima fase dinamica ( frecce in a ) e curva dinamica ( b )  . 
however , because of technical difficulties encountered during these examinations ( long positioning time and relative instability of the patients position ) , the remaining 16 patients were placed in the informate dellimportanza di evitare di muoversi durante lindagine , in particolare durante lacquisizione dinamica che avrebbe seguito le sequenze di centratura . 
stato altres richiesto alle pazienti di respirare con regolarit . 274 radiol med ( 2009 ) 114 : 267285 supine position with free breasts ( no use of bands or strips ) and with the arms placed along the body . 
all patients were carefully informed about the importance of avoiding any movement during the examination , in particular during the dynamic acquisition following the initial scout sequence . finally , the patients were instructed to breathe quietly . in order to reduce overall imaging time , the examination was limited to the dynamic study following the preliminary three - plane localising sequence . 
a three - dimensional axial ( eight patients ) or coronal ( ten patients ) gradient - echo ( fast low - angle shot ) sequence was used with the following common technical parameters : te 10.6 ms ; flip angle 30 ; one excitation ; partition thickness 3 mm without interslice gap ; acquisition time 94 s . 
 the dynamic study was acquired continuously without any time interval between the preand post - contrast phases . at the end of the first ( precontrast ) scan , the same operator manually injected a single 0.1 mmol / kg of body weight dose of gadobenate dimeglumine at a rate of approximately 2 ml / s , followed by a 20 - ml saline flush at a rate of approximately 1 ml / s . 
 mr postprocessing and image evaluation postprocessing involved image subtraction ( postcontrast minus precontrast ) of all dynamic phases , generation of maximum intensity projection ( mip ) reconstructions for bilateral axial and coronal views and right and left lateral views . 
moreover , we dotained enhancement - to - time curves for one or more regions of interest positioned within the lesion on the area subjectively recognised as showing maximal enhancement on the subtracted images of the dynamic phase judged as the best phase for lesion conspicuity [ 25 ]  . all mr examinations were prospectively evaluated in consensus by a senior radiologist and a resident in radiology with 12 and 2 years experience in breast mr , respectively . they were blinded to the results of cbe , mammography and us . 
 [ 4 ] , taking into account , for the levels of initial enhancement , the higher r1 relaxivity al fine di ridurre il tempo - esame , lindagine stata limitata allo studio dinamico dopo la preliminare sequenza triplanare di centratura . 
stata utilizzata una sequenza tridimensionale gradient - echo ( fast low angle shot ) assiale ( 8 pazienti ) o coronale ( 10 pazienti ) con i seguenti parametri tecnici comuni : te = 10 , 6 ms ; flip angle = 30 ; una eccitazione ; spessore di partizione = 3 mm , senza interspazio ; tempo di acquisizione per fase dinamica time = 94 secondi . 
la sequenza assiale stata acquisita con un tr di 29 ms , 44 partizioni , campo di vista rettangolare 380285 mm e matrice dimmagine 256192 ( pixel di 1 , 481 , 48 mm )  . 
la sequenza coronale stata acquisita con un tr 23 ms , 32 partizioni , campo di vista rettangolare 380309 mm e matrice dimmagine 256192 ( pixel di 1 , 481 , 61 mm )  . 
alla fine della prima scansione ( precontrasto ) , sempre il medesimo operatore ha somministrato manualmente 0 , 1 mmol / kg di gadobenato dimeglumina ( multihance ; bracco imaging spa , milano ) a circa 2 ml / s e 20 ml di soluzione fisiologica a circa 1 ml / s . 
 post - processing e valutazione delle immagini il post - processing stato effettuato mediante sottrazione dimmagine ( post - contrasto meno pre - contrasto ) per tutte le fasi dinamiche , ricostruzioni con algoritmo di massima intensit bilaterali ( assiali e coronali ) e laterali ( destra e sinistra ) e calcolo delle curve dinamiche dellenhancement in funzione del tempo per una o pi regioni di interesse posizionate nel contesto della lesione sullarea soggettivamente riconosciuta come maggiormente contrastata alle immagini sottratte della fase dinamica giudicata ottimale per la cospicuit della stessa lesione [ 25 ]  . tutte le indagini rm sono state valutate prospetticamente , in consenso , da un radiologo con 12 anni di esperienza in rm mammaria e da uno specializzando con due anni di esperienza in rm mammaria , in cieco rispetto ai risultati di vs , mammografia ed ecografia . 
le indagini sono state inizialmente valutate per il livello di qualit e la presenza di artefatti sulle immagini native ( da movimento ) e sottratte ( insufficiente coregistrazione )  . 
 [ 4 ] , tenendo conto , per il livello di enhancement iniziale , della pi elevata relassivit r1 del mezzo di contrasto utilizzato in questo studio , ovvero adottando le soglie modificate < 100% , 100% 240% e > 240% invece delle soglie classiche < 50% , 50% 100% e > 100% , come descritto in letteratura [ 27 ]  . 
ne conseguito il radiol med ( 2009 ) 114 : 267285 of the contrast agent used in this study , that is , adopting the modified thresholds of < 100% , 100% 240% and > 240% instead of the classic thresholds < 50% , 50% 100% and > 100% , as previously described [ 27 ]  . 
this score was translated into the 15 bi - rads score , as previously described [ 9 ] , as follows : no detectable enhancement = no enhancing focus = bi - rads 1 ; score 02 = benign = bi - rads 2 ; score 3 = probably benign = bi - rads 3 ; score 45 = suspicious = bi - rads 4 ; score 68 = highly suggestive of malignancy = bi - rads 5 . 
lesions with a maximal bi - rads score of 3 ( probably benign ) at one or more imaging modalities were also examined histopathologically after surgical excision ( n = 1 ) or by us - guided fine needle aspiration cytology ( n = 2 )  . 
the patients with lesions assigned a maximal bi - rads score of 2 ( benign ) underwent annual follow - up for 24 years , with cbe and us until 39 years of age , also with mammography for older women . 
annual follow - up was also performed for the two bi - rads 3 lesions evaluated with us - guided fine - needle aspiration cytology . all surgical samples were evaluated according to the guidelines of the association of directors of anatomic and surgical pathology [ 28 ]  . 
all tumours were classified according to the world health organization ( who ) system [ 29 ]  . statistical analysis sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and overall accuracy were calculated against a standard of reference comprising seguente sistema di valutazione di lesioni mammarie alla rm dinamica : forma ( rotondeggiante / ovale / lobulata = 0 ; lineare / dendritica / stellata = 1 ) ; margini ( definiti = 0 ; indefiniti = 1 ) ; pattern dellenhancement ( omogeneo = 0 ; disomogeneo = 1 ; anulare = 2 ) ; enhancement iniziale ( < 100% = 0 ; 100%240% = 1 ; > 240% = 2 ) ; enhancement postiniziale ( continuo = 0 ; plateau = 1 ; washout = 2 )  . 
questo punteggio stato tradotto in un punteggio bi - rads da 1 a 5 , come precedentemente descritto [ 9 ] , nel modo seguente : nessun enhancement identificabile = nessuna lesione con enhancement = bi - rads 1 ; punteggio 02 = lesione benigna = birads 2 ; punteggio 3 = lesione probabilmente benigna = birads 3 ; punteggio 45 = lesione sospetta per malignit = birads 4 ; punteggio 68 = lesione altamente sospetta per malignit = bi - rads 5 . 
 il diametro massimo di ciascuna lesione stato misurato elettronicamente dal primo autore sulle ricostruzioni mip ottenute dalle immagini sottratte assiali o coronali della fase dinamica considerata ottimale per la cospicuit della lesione . 
 correlazione radiologica - patologica tutte le lesioni sospette per malignit alla vs o classificate bi - rads 4 o 5 alla mammografia , allecografia o alla rm ( n = 13 ) sono state valutate istologicamente dopo asportazione chirurgica ( 4 lesioni non palpabili sono state centrate per mezzo di iniezione di sospensione di carbone sotto guida ecografica )  . 
lesioni con massimo punteggio birads 3 ( probabilmente benigno ) a una o pi delle modalit di imaging sono state valutate istologicamente dopo asportazione chirurgica ( n = 1 ) o mediante citologia su agoaspirato ecoguidato ( n = 2 )  . 
le pazienti che presentavano lesioni con massimo punteggio bi - rads 2 ( reperto benigno ) sono state sottoposte a follow - up da 2 a 4 anni con vs ed ecografia fino a 39 anni di et , anche con mammografia dopo i 39 anni di et . 
tutte le lesioni sono state valutate secondo la classificazione oms [ 29 ]  . analisi statistica sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) e accuratezza diagnostica sono stati calcolati rispetto allo standard di riferimento dato dalla combinazione tra esame istologico , citologia su agoaspirato e follow - up . 
sono state realizzate determinazioni separate per tutte e 23 le lesioni nelle 18 pazienti e 276 radiol med ( 2009 ) 114 : 267285 pathological examination , cytological examination and follow - up . 
 maximal diameters of the lesions measured on the mips were compared with those obtained on pathological specimens ; the comparison was presented using a bland - altman plot [ 30 ] , whereas the global agreement between the two measurements was calculated using the intraclass correlation coefficient [ 31 ]  . results diagnostic image quality was achieved for 15 / 18 ( 83% ) patients overall . 
images for the remaining 3 / 18 ( 17% ) patients ( all with claustrophobia ) were considered nondiagnostic due to patient movement and resulting misregistration artefacts during the dynamic phase of the mr examination . 
one of these was a 10 - mm invasive ductal carcinoma ( idc ) ( patient number 5 , lesion number 6 ) and another was a 20 - mm invasive tubular carcinoma ( patient 14 , lesion 19 )  . 
the third lesion ( patient 11 , lesion 16 ) was a 10 - mm cyst , as confirmed at us - guided fine - needle - aspiration cytology and negative follow - up . the final diagnosis of all lesions is listed in table 1 . 
one of these lesions ( patient 11 , lesion 16 ) was the 10 - mm cyst described above , whereas the others comprised a giant 45 - mm fibroadenoma ( patient 8 , lesion 11 ) that was surgically excised and a 20 - mm fibroadenoma ( patient 10 , lesion 15 ) characterised as benign on fineneedle - aspiration cytology and confirmed as benign at 2 - year follow - up with mammography and us . the morphologic and kinetic features of the lesions on low - field mr imaging are listed in table 2 . 
whereas all eight confirmed idcs showed morphological and kinetic parameters indicative of a malignant lesion , only three of five invasive lobular carcinomas ( ilcs ) , all in one patient ( patient 9 , lesions 12 , 13 and 14 ) showed morphological and kinetic parameters suspicious of malignancy . 
the other two ilcs demonstrated benign morphology but inhomogeneous enhancement with rapid wash - in followed by washout ( patient 2 , lesion 3 ) and suspicious morphology , together with inhomogeneous enhancement and intermediate washin followed by plateau ( patient 4 , lesion 5 )  . 
examples of dopo esclusione delle indagini di qualit non diagnostica . per gli indici di performance diagnostica sono stati calcolati gli intervalli di confidenza al 95% ( 95%ci ) secondo lapprossimazione della distribuzione binomiale alla distribuzione normale . il diametro massimale delle lesioni misurato alla rm sulle ricostruzioni mip stato comparato con quello istopatologico ( analisi di bland - altman [ 30 ] ) mentre laccordo globale tra le due misurazioni stato valutato mediante il coefficiente di correlazione intraclasse [ 31 ]  . risultati sul totale delle 18 indagini , 15 ( 83% ) sono state giudicate con qualit di immagine di livello diagnostico e vi sono state identificate 20 lesioni . 
la qualit di immagine ottenuta per le tre rimanenti 3 indagini ( 17% ) in 3 pazienti ( tutte claustrofobiche ) stata considerata non diagnostica a causa di artefatti da insufficiente coregistrazione dovuti a movimento della paziente durante lacquisizione dinamica . in queste tre pazienti mammografia e / o ecografia avevano identificato una lesione per ciascuna paziente ( tabella 1 ) : un carcinoma duttale invasivo ( cdi ) di 10 mm ( paziente numero 5 , lesione numero 6 ) ; un carcinoma tubulare invasivo di 20 mm ( paziente 14 , lesione 19 ) ; una cisti di 10 mm ( paziente 11 , lesione 16 ) confermata alla citologia su agoaspirato ecoguidato e follow - up negativo . la diagnosi conclusiva di tutte le lesioni elencata in tabella 1 . 
tre lesioni considerate bi - rads 3 sono state valutate mediante citologia su agoaspirato o istologia del pezzo operatorio : la cisti di 10 mm ( paziente 11 , lesione 16 ) descritta poco sopra , un fibroadenoma gigante di 45 mm ( paziente 8 , lesione 11 ) asportato chirurgicamente ; un fibroadenoma di 20 mm ( paziente 10 , lesione 15 ) risultato benigno alla citologia su agoaspirato e confermato come benigno al follow - up a due anni con mammografia ed ecografia . le caratteristiche morfologiche e dinamiche delle lesioni alla rm sono elencate in tabella 2 . 
mentre tutti gli otto cdi hanno mostrato caratteristiche morfologiche e dinamiche indicative di malignit , solo tre dei cinque carcinomi lobulari invasivi ( cli ) , tutti nella stessa paziente ( paziente 9 , lesioni 12 , 13 e 14 ) hanno mostrato caratteristiche morfologiche e dinamiche indicative di malignit . 
gli altri due cli hanno mostrato : uno morfologia di tipo benigno con enhancement disomogeneo , rapido wash - in seguito da wash - out ( paziente 2 , lesione 3 ) ; laltro morfologia sospetta con enhancement disomogeneo , wash - in intermedio seguito da plateau ( paziente 4 , lesione 5 )  . 
2 e 3 ( lesioni maligne )  . il confronto del diametro delle lesioni alla rm e allesame istologico ha mostrato un completo accordo per 9 / 14 lesioni asportate chirurgicamente ( 64% ) e una sottoradiol med ( 2009 ) 114 : 267285 mr diagnoses are shown in fig . 
2 and 3 ( malignant lesions )  . comparison between lesion diameter at mr imaging and that at pathological examination revealed full agreement for 9 / 14 ( 64% ) surgically excised lesions and an underestimation at mr imaging for 5 / 14 ( 36% ) lesions . 
for this latter determination , the two nonassessable malignant lesions on mr imaging ( one idc , one invasive tubular carcinoma ) were considered false negatives , whereas the nonassessable cyst was considered a false positive . 
however , many studies focused on the role of lowfield systems for preoperative localisation of breast lesions and for interventional procedures [ 1214 , 35 ] rather than for lesion detection and diagnosis . 
the long acquisition times ( primarily due to low - power gradient systems ) and low signal - to - noise ratios associated with these systems precluded their use for clinical dynamic imaging of the breast . more recently , pkk et al . 
investigated the potential clinical value of low - field breast mr imaging using a dynamic contrast - enhanced mr sequence in conjunction with an open 0.23 - t permanent magnet [ 15 ]  . 
in their study , they evaluated 16 malignant and 11 benign lesions with a mean lesion size of 2 cm and obtained sensitivity , specificity and accuracy values of 100% , 82% and 92% , respectively . 
interestingly , the corresponding specificity and accuracy values for the same patients examined using a 1.5t closed magnet were slightly worse ( 73% and 89% , respectively ) , even with an equal 100% sensitivity [ 15 ]  . however , a relatively high dose ( > 0.2 mmol / kg ) of a conventional contrast agent ( gadopentetate dimeglumine ) was considered necessary to achieve sufficient enhancement in this study . stima alla rm per le rimanenti 5 lesioni ( 36% )  . 
il diametro , misurato per 20 lesioni alla rm , risultato di 28 , 810 , 3 mm ( mediadeviazione standard ) con mediana di 20 m gli indici di performance diagnostica della rm mammaria a basso campo con gadobenato dimeglumina sono presentati in tabella 3 . 
se consideriamo solo le indagini di qualit diagnostica ( ovvero valutiamo 20 lesioni in 15 pazienti ) , sensibilit , specificit , vpp , vpn e accuratezza sono risultati tutti pari al 100% . 
se invece includiamo nellanalisi anche le tre indagini di qualit non diagnostica ( ovvero valutiamo 23 lesioni in 18 pazienti ) , gli indici di performance diagnostica sono risultati 86% , 87% , 93% , 78% e 87% , rispettivamente . 
in questultimo calcolo le due lesioni maligne non valutabili ( un cdi e un carcinoma tubulare invasivo ) sono considerate falsi negativi mentre la cisti non valutabile considerata come falso positivo . 
tuttavia , linteresse clinico si per lo pi focalizzato sul ruolo dei sistemi a basso campo per le biopsie e i centraggi prechirurgici rm - guidati [ 1214 , 35 ] piuttosto che sullidentificazione e caratterizzazione lesionale . 
i tempi di acquisizione prolungati ( dovuti innanzitutto alla scarsa potenza dei gradienti di campo ) e il ridotto rapporto segnale / rumore tipici di questi sistemi hanno precluso il loro utilizzo clinico per lo studio delle mammelle a contrasto dinamico . pi recentemente , pkk et al . 
 [ 15 ] hanno investigato il potenziale valore clinico della rm mammaria a contrasto dinamico a basso campo con un magnete aperto permanente operante a 0 , 23 t [ 15 ]  . 
 interessante notare come lo studio delle stesse pazienti con magnete chiuso operante a 1 , 5 t avesse dato una sensibilit egualmente elevata ( 100% ) ma livelli inferiori di specificit ( 73% ) e accuratezza ( 89% ) [ 15 ]  . 
tuttavia , in questo studio , gli autori hanno ritenuto necessaria una dose relativamente elevata ( maggiore di 0 , 2 mmol / kg ) di un mezzo di contrasto a bassa r1 relassivit ( gadopentetato dimeglumina )  . le potenzialit cliniche della rm mammaria a basso campo vanno correlate alle crescenti indicazioni , agli avanzamenti tecnologici dellhardware rm e , in particolare , alla rilevanza epidemiologica del numero di pazienti claustrofobiche o obese che necessiterebbero di unindagine da eseguirsi su sistemi a magnete chiuso . 
la claustrofobia da tempo un problema per alcuni dei pazienti che necessitano 278 radiol med ( 2009 ) 114 : 267285 radiol med ( 2009 ) 114 : 267285 280 radiol med ( 2009 ) 114 : 267285 fig . 
4 bland - altman comparison between magnetic resonance ( mr ) and pathological maximal diameters for 14 breast lesions . differences are obtained for each of the 14 lesions by subtracting the diameter measured at pathology from that measured at mr imaging . 
le differenze sono ottenute per ciascuna lesione sottraendo il diametro misurato allistopatologia a quello misurato alla rm . la visualizzazione di soli 11 punti dovuta alla perfetta sovrapposizione della differenza e dei valori medi per tre lesioni ( tabella 1 )  . mean ( mm ) table 3 diagnostic performance of breast magnetic resonance ( mr ) imaging performed at 0.2 t using a body coil and 0.1 mmol / kg of gadobenate dimeglumine in 18 claustrophobic or oversized patients tabella 3 performance diagnostica della rm mammaria eseguita a 0 , 2 t con bobina body e 0 , 1 mmol / kg di gadobenato dimeglumina in 18 pazienti claustrofobiche o obese index value 95% ci indice valore ic 95% sensitivity specificity positive predictive value negative predictive value overall accuracy 86% ( 13 / 15 ) 87% ( 7 / 8 ) 93% ( 13 / 14 ) 78% ( 7 / 9 ) 87% ( 20 / 23 ) 70%100% 65%100% 79%100% 51%100% 73%100% sensitibilit specificit valore predittivo positivo valore predittivo negativo accuratezza 86% ( 13 / 15 ) 87% ( 7 / 8 ) 93% ( 13 / 14 ) 78% ( 7 / 9 ) 87% ( 20 / 23 ) 70%100% 65%100% 79%100% 51%100% 73%100% numbers in parentheses were used to calculate the percentages . 
gli indici di performance diagnostica sono statti calcolati per tutte le 23 lesioni nelle 18 pazienti , considerando le tre indagini rm di qualit non diagnostica come due falsi negativi e un falso positivo ( tabella 1 : pazienti 5 , 11 e 14 ; lesioni numero 6 , 16 e 19 )  . ic , intervallo di confidenza the potential for low - field clinical mr imaging of the breast is related to the increasing indications for breast mr , to the technological advances in mr hardware and , importantly , to the number of claustrophobic or obese patients who require breast mr imaging . 
the increasing prevalence of obesity is an additional problem , not only given the practical problems associated with imaging oversized patients but also because obesity is an associated risk factor for breast cancer [ 36 ]  . 
in the usa , roughly 34% of the female population aged 2074 years were considered obese ( body mass index 30 ) in the period between 2001 and 2004 , whereas the prevalence of extreme obesity ( body mass index 40 ) among women in the same period was 6.9% [ 37 , 38 ]  . 
on this subject , it should be noted that our study was performed in italy , where the overwhelming majority of the population adopt a mediterranean lifestyle and diet and where the incidence of obesity is comparatively lower . 
lobesit un ulteriore problema , in notevole incremento , da valutare non solo in s ( per le difficolt tecniche che pu determinare per lesecuzione della rm mammaria su sistemi a magnete chiuso ) ma anche per il noto ruolo dellobesit quale fattore di rischio per il carcinoma mammario [ 36 ]  . 
negli usa , tra il 2001 e il 2004 , circa il 34% della popolazione femminile tra 20 e 74 anni era in condizioni di obesit ( body mass index maggiore o uguale a 30 ) e il 6.9% era in condizioni di estrema obesit ( body mass index maggiore o uguale a 40 ) [ 37 , 38 ]  . 
va notato che il nostro studio stato realizzato in italia , laddove la stragrande maggioranza della popolazione adotta stili di vita e dieta di tipo mediterraneo cui conseguono minori tassi di incidenza dellobesit . 
lincidenza di obesit grave cui consegue lesclusione dallaccesso alla rm su sistemi a magnete chiuso quindi verosimilmente maggiore negli usa laddove lobesit rappresenta un problema nazionale di dimensioni rilevanti [ 38 ]  . 
 radiol med ( 2009 ) 114 : 267285 closed magnets is likely to be much greater in the usa , where obesity is a national concern [ 38 ]  . 
 in terms of incidence , among the 397 consecutive patients evaluated over a 30 - month period at our institution , 18 patients ( approximately 5% ) of whom 15 ( 3.7% ) were claustrophobic and three ( 0.8% ) obese would otherwise have been excluded from evaluation with mr imaging had an open low - field mr system not been available . 
this percentage is not negligible ( it is equal to 1 in 20 ) , which may even be an underestimation given the likelihood of self - exclusion by claustrophobic or obese patients who know that breast mr is usually performed on closed magnets . 
although patient motion precluded the acquisition of diagnostic images in three women , overall diagnostic performance was good , with an overall accuracy of 87% for the 18 patients combined and an excellent correlation between the maximal lesion diameters measured on mr images and pathological specimens . 
 indications for breast mr imaging are rapidly expanding , even when filtered by critical analysis and consensus conferences among radiologists , surgeons , oncologists and other colleagues involved in breast diagnosis and care , as happened recently in italy [ 2 ]  . 
in addition to screening high - risk women [ 9 , 39 ] , breast mr is also used in clinical practice for presurgical staging [ 40 , 41 ] , for evaluating the effect of neoadjuvant chemotherapy on locally advanced cancers [ 42 , 43 ] , and for assessing equivocal breast findings on mammography and us [ 24 ] , even if this indication is under discussion and criticised [ 2 ]  . 
 our diagnostic performance values obtained using wellestablished morphological and kinetic assessment criteria are comparable with those determined elsewhere using conventional closed magnets and dedicated breast coils [ 4547 ]  . 
sebbene gli artefatti da movimento abbiano reso non diagnostica la qualit di immagine di tre indagini , la performance diagnostica complessiva stata buona , con unaccuratezza diagnostica globale dell87% su tutte e 18 le pazienti e uneccellente correlazione tra rm e istopatologia relativamente alle dimensioni lesionali . 
le recenti le indicazioni alla rm mammaria sono in rapida espansione , anche qualora sottoposte ad analisi critica e consensus conference tra radiologi , chirurghi , oncologi e altri specialisti del mondo senologico , com accaduto recentemente linee - guida dellamerican cancer society raccomandano la rm mammaria come modalit di screening per le donne con un rischio di tumore mammario nellarco di vita maggiore o uguale al 20%25% ( donne ad alto rischio genetico - familiare o esposte a radioterapia toracica tipicamente per il trattamento di linfomi tra 10 e 30 anni di et ) [ 39 ]  . 
oltre alla sorveglianza delle donne ad alto rischio [ 9 , 39 ] , la rm mammaria sempre pi utilizzata per la stadiazione prechirurgica [ 40 , 41 ] , per la valutazione delleffetto della chemioterapia neoadiuvante dei tumori localmente avanzati [ 42 , 43 ] e anche per la valutazione di reperti dubbi alla mammografia e allecografia [ 24 ] , anche se questultima indicazione oggetto di discussione e non esente da critiche [ 2 ]  . 
considerata la crescente importanza della rm mammaria e i limiti delle tecniche convenzionali in alcune situazioni ( per esempio lo studio mammografico delle mammelle ad elevata densit [ 8 , 44 ] ) , la rm mammaria dovrebbe essere accessibile a tutte le pazienti che non abbiano controindicazioni assolute allindagine . 
 i livelli di performance diagnostica da noi ottenuti utilizzando criteri standardizzati per la valutazione morfologica e dinamica sono comparabili a quelli altrimenti ottenuti con gli usuali magneti chiusi e bobine dedicate [ 4547 ]  . 
con leccezione delle tre indagini di qualit non diagnostica , tutte le lesioni maligne , inclusi cinque cli , sono stati correttamente diagnosticate utilizzando un mezzo di contrasto ad alta relassivit . 
the value of this agent lies in its increased r1 relaxivity in blood compared with other standard gadolinium agents [ 17 , 18 , 50 ] derived from weak and transient interaction of the gdbopta contrast - effective moiety of this agent with serum albumin [ 51 ]  . 
this results in markedly increased enhancement compared with that achievable with standard agents at an equivalent dose of 0.1 mmol / kg body weight and thus seems to improve breast lesion detection and visualisation [ 19 , 23 ]  . 
an association between one - sided increased breast vascularity and ipsilateral invasive cancer has been shown with gadobenate dimeglumine [ 20 , 52 ]  . the greater enhancement achievable with gadobenate dimeglumine could be important when using low - field magnets with inherently reduced signal - to - noise ratio [ 53 ]  . an alternative approach to achieving adequate enhancement would be to use a high dose of conventional gadolinium agent . 
this approach was recently adopted by pkk et al . , who administered 30 ml of gadopentetate dimeglumine ( corresponding to a dose of 0.21 mmol / kg body weight for a 70 - kg subject ) to women undergoing low - field breast mr imaging [ 15 ]  . 
however , the use of high doses is currently a matter of debate among the radiological community given the recently reported association between the administration of gd - chelates and the development of nephrogenic systemic fibrosis in patients with severe renal insufficiency [ 54 , 55 ]  . 
 our study suffered a series of important limitations concerning both the study design and the mr technique . these include the lack of a direct ( intraindividual ) comparison with data deriving from mr examinations conducted at higher field strength and the small number of patients and lesions evaluated . 
sebbene alcuni studi abbiano gi mostrato una superiore performance diagnostica della rm mammaria con gadobenato a 1 , 0 e 1 , 5 t [ 19 , 20 , 23 ] , per quanto a nostra conoscenza , questa la prima esperienza di rm mammaria con questo mezzo di contrasto a basso campo . 
il vantaggio fondamentale del gadobenato sta nella sua maggiore relassivit r1 nel sangue rispetto agli usuali mezzi di contrasto a base di gadolinio [ 17 , 18 , 50 ]  . 
ci determina un marcato aumento dellenhancement rispetto a quello ottenibile con gli usuali mezzi di contrasto a dosi equivalenti ( 0 , 1 mmol / kg ) cui sembra conseguire una superiore capacit di identificazione e visualizzazione delle lesioni mammarie [ 19 , 23 ]  . 
laumentata relassivit r1 consente altres un maggiore enhancement della vascolarizzazione mammaria ; lassociazione tra incremento asimmetrico della vascolarizzazione mammaria e tumore invasivo ipsilaterale stata infatti dimostrata con gadobenato [ 20 , 52 ]  . la possibilit di ottenere un maggiore enhancement con gadobenato potrebbe giocare un ruolo rilevante quando la rm mammaria realizzata con magneti a basso campo che producono immagini con rapporto segnale / rumore intrinsecamente ridotto [ 53 ]  . 
un approccio alternativo per ottenere un enhancement adeguato potrebbe essere luso di alte dosi di mezzi di contrasto paramagnetici a bassa relassivit . tale approccio stato recentemente utilizzato da pkk et al . 
 [ 15 ] che hanno somministrato 30 ml di gadopentetato dimeglumina ( corrispondenti a una dose di 0 , 21 mmol / kg per un peso corporeo di 70 kg ) a pazienti che eseguivano rm mammaria a basso campo [ 15 ]  . 
tuttavia , luso di alte dosi oggi molto discusso nella comunit radiologica in considerazione dellassociazione recentemente riportata tra la somministrazione di chelati del gadolinio e linsorgenza di fibrosi nefrogenica sistemica in pazienti con insufficienza renale grave [ 54 , 55 ]  . 
nonetheless , despite these limitations , our study shows that breast mr imaging on low - field open systems can be considered a possibility for claustrophobic or obese women who cannot undergo mr study at higher field strength on closed magnets . 
the availability of a dedicated breast coil should , however , be considered a requirement for future studies exploring the clinical use of lowfield open - unit breast mr imaging . given the potential for worldwide dissemination of lowfield magnets for breast mr screening programmes ( at least for high - risk women ) , further studies are needed to fully evaluate the potential of low - field open magnets with dedicated breast coils , possibly by means of direct ( intraindividual ) comparison with findings on higher field closed systems . 
moreover , low - field open breast mr imaging offers interesting possibilities for mr - guided breast biopsy and presurgical localisation [ 12 , 5659 ] as well as for reducing overall costs and possibly making breast mr imaging accessible to more women and more imaging centres . 
these include the recently available closed wide - bore or open high - field scanners [ 60 , 61 ] and mr examination under sedation or anaesthesia for claustrophobic women . 
 in conclusion , our preliminary experience showed that dynamic breast mr imaging of claustrophobic or oversized patients can be performed successfully on a low - field 0.2 - t open magnet using a single 0.1 mmol / kg body weight dose of gadobenate dimeglumine as a contrast agent . 
it is important to note that this technical combination can be used for claustrophobic or oversized patients only and not as a substitute for standard 1.5 - t breast mr imaging in normal subjects . 
further larger studies using dedicated breast coils are required to validate our general hypothesis regarding the value of breast mr imaging using open low - field magnets . insufficiente rappresentazione dello spettro di malattia . 
dal punto vista tecnico , il limite maggiore stato luso di una bobina body non dedicata ( la bobina dedicata per lo studio delle mammelle non era commercialmente disponibile per il nostro sistema aperto a basso campo )  . 
la risoluzione spaziale relativamente bassa ( dimensioni del pixel da 2 , 2 a 2 , 4 mm2 ) potrebbe avere limitato la valutazione della morfologia delle lesioni , limite che potrebbe essere superato disponendo di una bobina dedicata e utilizzando matrici dimmagine maggiori e spessori di partizione ridotti ( anche prolungando il tempo di acquisizione fino a 120 secondi )  . 
comunque , anche considerando questi limiti , il nostro studio mostra che la rm mammaria con magneti aperti a basso campo pu essere considerata una possibilit per le donne claustrofobiche o obese che non possono eseguire lindagine a pi alto campo con magneti chiusi . tuttavia , noi riteniamo che la disponibilit della bobina dedicata debba essere considerata necessaria per futuri studi sulluso clinico dei sistemi aperti a basso campo per la rm mammaria . date le potenzialit che i magneti a basso campo potrebbero offrire per la diffusione di programmi di screening mammario con rm ( almeno per le donne ad alto rischio ) , occorrono studi con disegno comparativo intraindividuale che mettano a confronto indagini a basso campo con indagini ad alto campo con magneti chiusi . 
inoltre , magneti aperti a basso campo offrono interessanti potenzialit per lesecuzione di biopsie e centraggi rm - guidati [ 12 , 5659 ] e per una sensibile riduzione dei costi economici che renderebbe la rm mammaria disponibile in un maggiore numero di centri e per un maggiore numero di donne . 
 infine opportuno tenere presente anche che possibili alternative per le donne claustrofobiche o obese possono essere date dalla recente disponibilit di sistemi chiusi con ampie dimensioni di accesso o sistemi aperti a campo relativamente alto [ 60 , 61 ]  . 
 in conclusione , la nostra esperienza preliminare ha mostrato che la rm mammaria in donne claustrofobiche o obese pu essere eseguita con successo utilizzando un sistema a magnete aperto a basso campo ( 0 , 2 t ) e 0 , 1 mmol / kg di gadobenato dimeglumina . 
importante sottolineare che questa combinazione tecnica pu essere utilizzata solo per pazienti claustrofobiche o obese e non pu in alcun modo essere proposta come alternativa allindagine standard a 1 , 5 t in soggetti normali . 
guglielmi2 , 5 1department of human physiology , university of rome tor vergata , via montpellier 1 , 00173 rome , italy . 2department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 3department of radiology , university of rome tor vergata , via montpellier 1 , 00173 rome , italy 4department of orthopaedics and traumatology , university hospital policlinico tor vergata rome , italy 5department of radiology , scientific institute hospital css , viale cappuccini 1 , san giovanni rotondo , 71013 foggia , italy correspondence to : g . 
this review discusses the application of dual - energy x - ray absorptiometry ( dxa ) on bc determination , given that dxa has the potential to provide overall and regional assessment of bc in terms of fat , lean mass and bone . 
dxa is widely used in many clinical settings primarily diagnosis osteoporosis . this article describes the use of whole - body dxa in assessing bc in patients with chronic diseases ( e.g. metabolic syndrome ) as well as in different sport activities to evaluate the effects of exercise . keywords total - body dxa body composition body fat lean body mass bone mineral density riassunto la valutazione della composizione corporea , da qui in avanti denominata con il termine anglosassone di body composition ( bc ) , un metodo essenziale per analizzare lo stato di salute in termini nutrizionali , sia a livello di popolazione sia a livello individuale , come pure per indagare lefficacia delle strategie nutrizionali preventive primarie e secondarie . 
questi tuttavia possono manifestarsi anche nel soggetto anziano , per il quale il trascorrere degli anni pu causare significativi cambiamenti nel rapporto tra grasso corporeo e muscolo . per misurare la composizione corporea esistono numerose tecniche ; alcune semplici , ma con margini di errore ancora elevati , altre invece costose e sofisticate ( come per esempio la valutazione a livello atomico e molecolare della bc ) ma pi affidabili nel rilevamento dei risultati a vari livelli . 
questa revisione della letteratura riguarda lapplicazione della tecnica dual - energy x - ray absorptiometry ( dxa ) per la determinazione della composizione corporea , in quanto tale metodica permette di misurare sia in maniera totale che segmentale , per singoli distretti , i vari componenti quali : massa grassa , massa magra e tessuto osseo . 
in questo articolo verranno descritte le altre possibili radiol med ( 2009 ) 114 : 286300 indicazioni , tra cui lo studio della bc nei pazienti con sindromi metaboliche croniche e lapplicazione in condizioni fisiologiche , quali per esempio nello sportivo , per valutare leffetto dellesercizio fisico sulla massa corporea . parole chiave dxa composizione corporea massa grassa massa magra densit minerale ossea introduction introduzione two parallel trends exist in the developed world in an increasing percentage of the population : ageing and obesity . debilitating illnesses such as cardiovascular disease and diabetes are common to both obesity and ageing , and osteoporosis , in particular , is the most common metabolic bone disease and indeed one of the most prevalent disorders associated with ageing [ 1 , 2 ]  . because obesity is becoming a worldwide epidemic , there is an increasing interest in the study of body composition ( bc ) both overall and regional to monitor the condition and delay the development of obesity - related diseases such as cardiovascular disease and type 2 diabetes [ 3 ]  . frailty and sarcopoenia may represent the advanced stages of age - related bc changes . 
it has been reported that loss of skeletal muscle mass occurs with advancing age in elderly men and women , even in independently living healthy subjects , and that men lose significantly more leg skeletal muscle mass than do women [ 4 ]  . furthermore , skeletal muscle mass loss in men is masked by weight stability resulting from a corresponding increase in total body fat mass ( fm )  . 
age - related changes in bc , including the increase and redistribution of fat tissue and the decrease in skeletal muscle and bone mass , begin as early as the fourth decade of life . 
preventive and therapeutic options for optimising bone mass and bc in old age is central to the care of patients in midlife and beyond . because of the high impact of osteoporotic fractures on morbidity and mortality and indirectly on health care costs , early and accurate diagnosis of these bc changes is of major importance [ 1 , 6 , 7 ]  . 
there is general agreement that lifestyle changes focused on improving dietary intake and increased daily physical activities are the cornerstones in both preventing and treating obesity and the metabolic syndrome [ 8 ]  . 
authors have shown a positive effect of exercise on bc , especially in reducing menopausal risk factors in women [ 9 ] and enhancing treatment efficacy in older nei paesi industrializzati si sta assistendo allo sviluppo di due tendenze che aumentano parallelamente nella popolazione , ossia obesit e invecchiamento . 
in particolare , losteoporosi risulta la patologia metabolica dellosso associata con maggiore prevalenza allavanzare dellet [ 1 , 2 ]  . per quanto riguarda lobesit , poich sta diventando una patologia a diffusione quasi epidemica , diventa necessario nei pazienti coinvolti effettuare una valutazione della composizione corporea ( bc ) anche distrettuale , per monitorare landamento dellaffezione e cercare di ritardare lespressione di patologie associate quali diabete e disturbi cardiovascolari [ 3 ]  . 
laffaticamento muscolare , il rischio di caduta , le limitazioni funzionali , limmobilit e di conseguenza le fratture da fragilit , sono tutte condizioni connesse alla perdita di massa muscolare . 
come noto , dalla letteratura si evince che la riduzione della massa muscolare scheletrica un processo fisiologico legato al progredire dellet che coinvolge entrambi i sessi indipendentemente dallo stato di salute . 
bisogna sottolineare inoltre che anche la bc soggetta a cambiamenti che iniziano allincirca dalla quarta decade di vita , nel senso di un incremento e ridistribuzione del tessuto adiposo e di una riduzione della massa muscolare e ossea . 
 necessario perci mettere in campo misure preventive e attuare trattamenti terapeutici mirati per fasce det . in considerazione dellalto impatto che le fratture da osteoporosi hanno sulla morbilit , sulla mortalit e di riflesso sui costi sanitari correlati , risulta necessario attuare una diagnosi precoce e attendibile dei suddetti 288 radiol med ( 2009 ) 114 : 286300 total 1 . , 0 - 2 , 5 fracture risk increased non increased high t - score vs . 
for this reason , and because bc is known to have a significant effect on athletic performance and because exercise has the potential to alter bc , there is considerable interest in the evaluation of bc in exercise and sport [ 11 , 12 ]  . 
nonetheless , fluctuations in body weight alone cannot be adequately understood unless they are interpreted as quantitative variations of the fat - free mass ( ffm ) , fm and total body water ( tbw ) components , as each component varies independently . 
most centres use axial dual - energy x - ray absorptiometry ( dxa ) of the spine , lumbar spine and nondominant proximal hip , as the hip is considered the most suitable site for predicting fracture risk [ 7 ] and the spine the most suitable for monitoring treatment effects [ 14 ] , as indicated by the world health organization , which also established that the results should be reported as a t - score for osteoporosis . 
esiste comunque un consenso comune sul fatto che un corretto stile di vita abbinato a una regolare attivit fisica e ad unalimentazione corretta e bilanciata , si configurano quali fattori fondamentali nella prevenzione delle sindromi metaboliche [ 8 ]  . 
alcuni autori hanno dimostrato leffetto benefico dellesercizio fisico svolto in modo regolare sulla bc soprattutto per quanto concerne la riduzione dei fattori di rischio legati alla menopausa nelle donne [ 9 ] cos come nei superobesi con diabete alimentare nellaumentare gli effetti terapeutici [ 10 ]  . 
per questo motivo , permane un considerevole interesse per la valutazione della bc associata allattivit fisica agonistica e non , in quanto noto che la bc ha un effetto significativo sulla prestazione atletica . 
non di meno , le fluttuazioni del peso corporeo non possono essere adeguatamente interpretate se non come variazioni quantitative delle seguenti componenti : massa magra ( fat free mass , ffm ) , massa grassa ( fat mass , fm ) e acqua corporea totale ( total body water , tbw )  . 
ci accade perch il femore risulta essere il migliore sito predittivo di rischio di frattura [ 7 ] mentre la colonna il miglior sito per esaminare landamento della terapia [ 14 ] , come da indicazione della who che si riferisce al valore espresso in t - score per effettuare la diagnosi di osteoporosi . 
nella scelta del metodo bisogna considerare , oltre ai costi legati allo strumento stesso e al personale deputato allutilizzo , leventuale esposizione del soggetto a radiazioni , il tempo necessario a ottenere linformazione richiesta e , non ultimo , laccuratezza dellinformazione ( tabella 1 )  . radiol med ( 2009 ) 114 : 286300 fig . 
il distretto addominale e le regioni prossimali degli arti inferiori possono essere definite manualmente , mentre altre sedi sono determinate automaticamente dal software , sebbene possano essere successivamente modificate . methods of assessing body composition depending on the information needed , several methods can be used to measure bc , each with some advantages and limitations [ 16 , 17 ]  . 
in selecting the method , one has to take into account cost ( equipment and personnel ) , possible radiation exposure , time required to obtain the information and accuracy of the information obtained ( table 1 )  . bc measurement is of interest to clinicians , nutritionists and physiologists . 
the most frequently used methods are based on a two - component model comprising fm and ffm , because the amount of fat in the body is of special nutritional interest . 
the three most common methods used to calculate bc based on the two - component model are underwater weighing ( uww ) , bioelectrical impedance le figure cliniche maggiormente interessate ai risultati della valutazione della bc sono linternista , il nutrizionista e il fisiologo . 
i metodi pi comunemente utilizzati si basano su modelli a due compartimenti che comprendono la massa grassa ( fat mass , fm ) e la massa magra ( fat free mass , ffm ) in quanto linteresse principale naturalmente la misurazione del grasso corporeo . 
i tre pi comuni metodi usati per calcolare la bc sul modello a due compartimenti sono la pesata idrostatica ( uww ) , lesame impedenziometrico ( bia ) e la plicometria ( sk )  . questo modello presuppone che nella ffm sia compresa una quantit fissa di acqua , proteine e minerali . 
tuttavia , bisogna tenere in considerazione il fatto che la massa ossea , lacqua e le proteine variano per ciascun individuo e sono influenzati dallet , dalletnia , dal sesso , dai fattori genetici , cos come da elementi modificabili quali la dieta e 290 radiol med ( 2009 ) 114 : 286300 analysis ( bia ) and skinfold thickness measurements . 
gli studi effettuati in passato sulla valutazione della bc si basavano per la maggior parte su misurazioni antropometriche indirette come lindice di massa corporea ( bmi ) e le circonferenze corporee . 
il bmi , la circonferenza vita e fianchi , con relativo rapporto ( whr ) , sono dati antropometrici indiretti , comunemente utilizzati come indice di obesit nelladulto . queste misure , essendo semplici da eseguire e standardizzate , si configurano come ideali per la compilazione di studi epidemiologici . 
 [ 19 ] hanno evidenziato che la dxa e due modelli di bia davano risultati simili di massa grassa in uomini e donne table 1 methods for assessing body composition techniques pros cons body mass index ( bmi ) free ; fast ; predictor of life expectancy skinfold thickness measurements convenient ; fast ; portable ; useful for detecting changes in percentage of body fat waist - hip ratio ( whr ) fast ; free with tape measure bioelectrical impedance analysis ( bia ) inexpensive ; portable ; fast ; accurate for estimating total body water in populations if height , weight and other variables are added underwater weighing ( uww ) relatively accurate ; very consistent ( good for measuring changes in percentage of body fat ) dual - energy x - ray absorptiometry ( dxa ) most precise ; most accurate ; fast ; gives information on total and regional percentage of fat does not give precise assessment of percentage of body fat for athletes . 
possible causes of error are posture ( height ) , hydration and bowel status ( weight ) requires precise and consistent technique ; not accurate for very thin or very fat people ; only measures fat under the skin ; not an accurate estimate of actual percentage of body fat . 
 possible sources of error are dehydration , bladder status , temperature , fat asymmetry , arm position , etc . uncomfortable ; wet ; bulky apparatus ; skimpy outfit required ; time consuming ; expensive ; hard to find ; bone density assumption causes error . 
possibile fonte di errore sono : deidratazione , stato di replezione vescicale , temperatura , asimmetria del tessuto adiposo , posizione degli arti , ecc . poco confortevole perch in acqua ; attrezzatura voluminosa ; tempi lunghi desame ; costosa ; difficile da trovare ; non calcola la densit dellosso . 
however , the differences depend on gender and body - weight status , indicating the importance of considering these factors when identifying people with excess fm [ 19 ]  . in addition to total body measurements , the interest of clinicians and researchers has also focused on regional assessment of bc . 
the application of techniques such as ct and mri to bc analysis over the last two decades has enabled the anatomical delineation and quantification of several types of adipose tissue depots [ 20 ]  . unfortunately , the routine use of ct and mri in bc con diverso grado di obesit e di attivit fisica . 
poich le differenze erano correlate al sesso e al peso corporeo , gli autori hanno sottolineato lincidenza di tali fattori nella valutazione di persone con eccesso di massa grassa [ 19 ]  . oltre alle valutazioni corporee totali , lattenzione del clinico particolarmente rivolta ai distretti corporei : i metodi di riferimento utilizzabili sono la risonanza magnetica ( rm ) e la tomografia computerizzata ( tc )  . 
sfortunatamente , lutilizzo di routine della tc e rm nella valutazione della bc ostacolato dai costi elevati , inoltre , la tc richiede una significativa esposizione a radiazioni 292 radiol med ( 2009 ) 114 : 286300 fig . 
results of the total - body scan are calculated automatically for bone mineral density ( bmd ) , fat tissue , and lean tissue for the total body and subregions . 
b evaluation of total bmd and bone mineral content ( bmc ) ( left ) , soft tissue ( middle ) and fat - mass distribution expressed as a percentage with a colour map ( right )  . 
b valutazione della bmd totale e del bmc ( sulla sinistra ) , dei tessuti molli ( al centro ) e della distribuzione del tessuto adiposo espressa in percentuale con una mappa a colori ( sulla destra )  . analysis is hampered by access and cost . 
 [ 23 ] compared abdominal adipose tissue measured by mri and dxa in nonobese men and defined dxa regions of interest ( rois ) in two different ways ( between the second and fourth lumbar vertebra or the iliac crest ) and found both of these regions comparable with mri total abdominal adiposity and mri - derived narrow abdominal slices . 
 [ 24 ] reported that dxa yielded accurate measurements of abdominal adipose tissue compared with ct in overweight / obese individuals weighing 66134 kg . dxa divides the body into three components : bone , fatfree and bone - free tissue , and fat [ 14 , 25 ]  . 
 [ 23 ] hanno misurato il tessuto adiposo addominale in uomini non obesi con la dxa e con la rm , definendo le regioni di interesse della dxa in due differenti modi ( tra la seconda e la quarta vertebra lombare e a livello delle creste iliache )  . 
quindi , per la dxa , che attualmente si configura come il metodo pi usato per misurare la densit minerale ossea , si prevede un utilizzo su larga scala anche per analisi distrettuali e totali della bc , in virt della sua accuratezza diagnostica ed economicit . 
la dxa ancora oggi una delle tecniche pi utilizzate per la valutazione della bc come risulta dallincremento della disponiradiol med ( 2009 ) 114 : 286300 result of the increasing worldwide availability of these scanners . 
inoltre , la metodica suscita interesse in quanto non invasiva , a basso rischio di radiazione e relativamente facile da eseguire sia per loperatore che per il soggetto che vi si sottopone . 
bene sottolineare che gli scanner di seconda generazione consentono una maggiore velocit di scansione e una minore esposizione alle radiazioni ionizzanti [ 15 , 19 , 26 ]  . principles of dxa , advantages and limitations principi della dxa , vantaggi e limitazioni the major commercial manufacturers of bone densitometers employ a subtly different technology ; however , our further discussion does not address the particulars of each technology and / or manufacturer . 
each system uses a source that generates x - rays at two energies : a detector , and an interface with a computer system for imaging the scanned areas of interest . 
dxa employs an x - ray tube and filtres to produce one low and one high pseudomonoenergetic beathe x - ray tube may be operated at constant potential or switched between two potentials . 
soft tissue , consisting largely of water and organic compounds , reduces photon flux to a much lesser extent than does bone mineral , and pixels containing bone are relatively easily distinguished from those with no bone present . 
however , hydration can vary from 67% to attualmente le principali ditte costruttrici di densitometri impiegano nella realizzazione degli scanner una tecnologia molto simile , in ogni caso la seguente discussione non riguarda nessuna delle diverse tecnologie in particolare . ciascun sistema utilizza una sorgente che genera raggi x a doppio livello energetico , un detettore , e uninterfaccia con un sistema computerizzato per la visualizzazione delle aree di interesse . 
viene effettuata una scansione rettilinea del corpo in posizione supina che divide il corpo in una serie di pixel , in cui ciascuno delle attenuazioni fotoniche misurata ai due livelli energetici . 
lapproccio della dxa per la misurazione della bc assume che il corpo consiste di tre componenti che sono distinguibili in base alle loro propriet di attenuazione : massa grassa , tessuto osseo e massa magra . 
allinterno di ciascun pixel le proporzioni di soli due componenti possono essere ottenute dal differente grado di assorbimento della doppia energia fotonica . i tessuti molli , composti principalmente da acqua e da componenti organici , riducono il flusso di fotoni molto meno del tessuto osseo , ed relativamente facile distinguere i pixel contenenti osso da quelli che non lo contengono . nelle zone dove losso non presente sono necessarie ulteriori calibrazioni per distinguere la componente grassa da quella magra appartenente ai tessuti molli . 
4 il software per lanalisi della composizione corporea ( body composition analysis , bca ) permette una valutazione totale e distrettuale della distribuzione della massa grassa , massa magra , massa totale e del bmc . 
 dxa software enables one to determine bone mineral and soft - tissue composition in different regions of the body . thus , bone mineral can be determined by scanning the spine , hip , forearm or whole body . 
these whole - body scans can then be analysed to measure the bc in defined regions of these scans , for example , in the arms , legs and trunk . 
thus , it is becoming increasingly clear that different skeletal regions , even those that have similar quantities of trabecular or cortical bone , may respond variably in different physiological situations [ 3135 ]  . the precision of a particular dxa device for assessing whole bc is generally good , with coefficients of variation of about 1% for bmc and 2%3% for total body fat [ 36 ]  . for this reason , dxa has been used to determine both longterm change in bc with ageing [ 4 ] and short - term change in bc as a result of intervention [ 3739 ]  . 
however , in regions such as the thorax , arm and head , the percentage of bone - free pixels is lidratazione tuttavia pu invece variare dal 67% al 85% . se un soggetto contiene pi della met della quantit di acqua , alcune scansioni dxa sovrastimeranno il contenuto di grasso [ 28 ]  . 
sebbene una variazione dellidratazione dal 68 , 2% al 78 , 2% non alteri significativamente la percentuale di grasso [ 29 ] una severa iperidratazione , cos come nellascite o edema , pu inficiare il risultato della percentuale di grasso [ 30 ]  . il software dellapparecchiatura dxa in grado di determinare la densit minerale ossea e la valutazione dei tessuti molli in differenti regioni del corpo umano . 
infatti , comincia ad essere evidente che , in differenti situazioni fisiologiche , si possono ottenere risposte non uguali nelle diverse regioni scheletriche comprese quelle che hanno la medesima distribuzione di trabecole [ 3135 ]  . la dxa possiede una precisione di scansione per la valutazione della bc con un coefficiente di variazione di circa 1% per il contenuto minerale osseo e del 2%3% per il contenuto totale di grasso corporeo [ 36 ]  . 
per questo motivo , la dxa stata usata per determinare cambiamenti a lungo termine della bc con let [ 4 ] e a breve termine come risposta al trattamento farmacologico [ 3739 ]  . in tutte le misure dxa si assume che la quantit di grasso sullosso lo stesso di quello intorno allosso . 
tuttavia , nelle regioni come il tronco , le braccia e la testa , la percentuale radiol med ( 2009 ) 114 : 286300 much lower and may be insufficient for accurate soft - tissue and hence bone determinations to be made [ 40 ]  . during whole - body scans , measurements are made over a very wide range of tissue depths . 
during the last few years , manufacturers have introduced major software upgrades as they have become aware of inaccuracies in their systems . physiological and clinical applications with ageing , changes in bc have an adverse impact on mortality and morbidity , as well as on quality of life . 
the study of the effects of ageing on bc measurements will enable a better understanding of the relative contribution of obesity and sarcopoenia morbidity and mortality in older adults [ 5 , 18 ]  . 
 several changes in bc may occur with ageing , including a reduction in fat - free tissue mass and an increase in fm , leading to a higher percentage of body fat at any given body weight in older adults . 
similarly , repositioning of fat to a more central distribution and loss of muscle bulk in the gluteal region will increase waist circumference and whr without an increase in fm . 
these and other age - related changes ( such as loss of skin elasticity , body cell mass and abdominal muscle bulk , and an increase in thoracic kyphosis ) may affect the validity of indirect anthropometric measures in determining bc [ 4 , 5 , 37 , 43 ]  . loss of skeletal muscle mass with ageing increases an individuals risk for sarcopoenia , which is characterised by low skeletal muscle mass , reduced muscle strength and increased risk for adverse health outcomes such as falls , fractures , impaired physical functioning , disability and frailty in older populations [ 22 ]  . 
 [ 18 ] studying 351 men ( mean age 63.5 years ) and 380 women ( mean age 62.1 years ) observed a trend towards sarcopoenia with dei pixel privi di osso sar molto bassa e quindi insufficiente per unaccurata analisi del tessuto molle [ 40 ]  . durante la scansione total body , le misure sono effettuate in un ampio spettro di spessore del tessuto . 
lo studio degli effetti dellet su ciascuna misura della composizione corporea sar capace di offrire in futuro una migliore conoscenza del contributo relativo dellobesit e sarcopenia sulla morbilit e mortalit dei soggetti in et adulta [ 5 , 18 ]  . tra i diversi cambiamenti che avvengono nella bc con lavanzare dellet sono inclusi una riduzione della massa magra ( ffm ) e un incremento della massa grassa che comporta una maggiore incidenza della percentuale di grasso corporeo sul peso totale delladulto . 
similmente , la ridistribuzione centrale del grasso e la riduzione della massa muscolare in regione glutea saranno responsabili dellaumento della circonferenza e whr senza un corrispondente incremento del tessuto adiposo . 
tutti i cambiamenti finora elencati ( quali la perdita di elasticit cutanea , della massa cellulare e della massa muscolare e unaccentuazione della cifosi dorsale ) possono alterare la validit di misure antropometriche indirette associate alla bc [ 4 , 5 , 37 , 43 ]  . la perdita di massa muscolare con lavanzare dellet incrementa il rischio di sarcopenia cui consegue la perdita della forza muscolare e di seguito il rischio di caduta , quindi di frattura , disabilit e fragilit nella popolazione anziana [ 22 ]  . 
 [ 18 ] hanno condotto uno studio su 351 uomini ( di et media 63 , 5 anni ) e 380 donne ( di et media 62 , 1 anni ) e hanno osservato , soprattutto negli uomini , un trend in ascesa della sarcopenia con let . 
such changes include agerelated loss of gluteal muscle bulk , kyphotic posture and loss of abdominal muscle tone , and shift of fm from a peripheral to a more central distribution . 
these changes may lead to an increase in whr in the absence of an increase in total body fat [ 4 , 18 ]  . it is well known that excess of intra - abdominal or visceral adipose tissue ( iaat or vat ) is related to the risk of developing coronary heart disease and type - 2 diabetes . researchers have suggested that iaat , independent of obesity severity , is a good predictor of the associated abnormalities of metabolic syndrome . 
their use could help in the early detection of abdominal / visceral obesity [ 23 , 44 , 45 ]  . most recent studies using new types of scanners and updated software [ 38 , 40 ] support the capability of dxa to measure small changes in bc . 
furthermore , a recent study in 76 postmenopausal women followed for 1 year showed that dxa was a more sensitive method for assessing small changes in bc compared with uww and a multicomponent model [ 38 , 47 ]  . 
they also provide the android / gynoid fat ratio and colour maps of the percentage of fat , thus helping to determine body fat distribution an important risk factor in a variety of serious diseases . in clinics it is important to know individuals bc , because in addition to the concept that bc naturally changes with age , physical activity and disease , fat is associated with health , and lean body mass is a better indicator of fitness and health than is weight , and increased fitness may reduce body fat but not reduce weight . a decrease in physical activity may lead to an increased loss of bone mineral and an increase in the incidence of osteoporotic fractures . 
questi cambiamenti possono portare ad un incremento di whr in assenza di un aumento del grasso corporeo totale [ 4 , 18 ]  . gi noto che leccesso di tessuto adiposo intra - addominale o tessuto viscerale ( iaat or vat ) correlato al rischio di sviluppare patologie cardiovascolari e diabete mellito di tipo 2 . 
alcuni studi hanno identificato per le scansioni dxa alcune regioni di interesse ( roi ) che possono essere validamente misurate usando siti anatomici specifici per la valutazione della distribuzione del tessuto adiposo . 
il loro utilizzo faciliterebbe la diagnosi precoce di obesit addominale / viscerale [ 23 , 44 , 45 ]  . studi recenti hanno evidenziato che limpiego di nuovi tipi di scanner e software aggiornati , supportano la capacit della dxa di misurare anche piccoli cambiamenti nella bc [ 38 , 40 ]  . 
inoltre , uno studio recente effettuato per un anno su 76 donne in stato post - menopausale , ha dimostrato che la dxa il metodo pi sensibile per valutare piccoli cambiamenti nella bc confrontato con la pesata idrostatica e con il modello multicompartimentale [ 38 , 47 ]  . 
 particolari dxa scanner sono inoltre in grado di esaminare soggetti gravemente obesi e di calcolare automaticamente i risultati raddoppiando i valori ottenuti da una semivalutazione total body , cos come la percentuale di grasso androide / ginoide e la mappa a colori della percentuale di grasso . 
ci pu aiutare a determinare con accuratezza la distribuzione di questultimo , acquisendo informazioni aggiuntive su quello che rimane un importante fattore di rischio per unampia variet di patologie . in clinica importante conoscere la composizione corporea perch , oltre al concetto che la bc si modifica con let , lattivit fisica e in condizioni patologiche , la quantit di grasso associata allo stato di salute e la distribuzione della massa magra un migliore indice predittivo rispetto al peso ; lincremento di massa magra pu infatti ridurre la quantit di grasso , ma non il peso corporeo totale . 
 una diminuzione dellattivit fisica pu condurre ad un aumento della perdita di massa ossea e un incremento radiol med ( 2009 ) 114 : 286300 athletes , especially those who are strength - trained , have greater bmd than do nonathletes and that strength , muscle mass and maximal oxygen uptake correlate with bone density [ 47 ]  . the factors associated with attaining optimal bmd and bmc have not been clearly identified . 
furthermore , physical activity has an effect on bc , especially skeletal muscle , which is the largest nonadipose tissue component and which plays an important role in physical activity and many biochemical processes . 
recent studies have confirmed that dxa can be used as a method for estimating total body muscle mass in healthy men and women of different age groups and that dxa can be used for estimating appendicular muscle mass ( amm ) [ 11 ]  . 
 [ 11 ] comparing three groups of athletes judo , karate and water polo with an ageand gendermatched control group , have shown that the athletes had significantly greater bmd and amm than the did nonathletes of similar age . 
in particular , weightbearing activities , such as walking , have a greater effect than nonweightbearing activities , such as cycling and swimming , whereas a reduction in mechanical loading , e.g. , bed rest or space flight , leads to bone loss . 
it has been previously suggested that the type of physical activity necessary to build and maintain bone density must be weightbearing , in part , because the loss of ambulation or weightlessness results in marked skeletal atrophy . 
within the athletic groups , however , water polo players had the highest amm but a lower total body bmd and an intermediate level of bmd for the arms , legs and trunk compared with the judo and karate groups , suggesting that the amm alone is not entirely responsible for the increased bmd in the athletic individuals . 
 [ 12 ] found significant regional tissue differences , measured by dxa , between soccer forwards and backs , which may be related to playing function , as well as differences between rugby players and controls . 
studi crosssectional mostrano che gli atleti , specialmente quelli che praticano allenamenti di tipo agonistico , hanno maggiore bmd rispetto ai sedentari ; la forza muscolare , la massa e il massimo consumo di ossigeno sono correlati alla bmd [ 47 ]  . i fattori associati al conseguimento di una bmd e bmc ottimale non sono stati chiaramente identificati . 
lattivit fisica ha un effetto sulla composizione corporea ( bc ) , specialmente sulla muscolatura scheletrica , che il pi vasto componente tissutale non - adiposo e riveste un importante ruolo nellattivit fisica e in alcuni processi biochimici . 
 [ 11 ] hanno valutato e messo a confronto tre gruppi di atleti praticanti judo , karate e water polo , con un gruppo controllo avente le medesime caratteristiche antropometriche . 
lo studio ha mostrato che gli atleti presentavano un valore maggiormente significativo di bmd e amm rispetto ai controlli di stessa et ; in particolare stato notato che le attivit svolte sotto carico , come per esempio camminare , hanno un maggiore effetto rispetto a quelle svolte fuori carico , come il ciclismo e il nuoto , mentre una riduzione nel carico meccanico , per esempio nellimmobilit a letto o nellattivit in assenza di gravit , conducono alla perdita di massa ossea . 
in precedenza stato suggerito che il tipo di attivit fisica relativo alla stimolazione della formazione ossea e al mantenimento dovrebbe essere svolta in condizione di carico , perch in condizioni opposte si arriva allatrofia scheletrica . 
considerando il gruppo di atleti , i praticanti water polo avevano un maggiore valore di amm ma un pi basso valore di bmd in total body , un livello intermedio di bmd per gli arti superiori , inferiori e al tronco comparato con i gruppi praticanti judo e karate , suggerendo che il valore di amm da solo non interamente responsabile dellincremento della bmd negli atleti . 
una variet di altri fattori pu essere responsabile delle differenze osservate , per esempio , variazioni nellintroito alimentare potrebbero determinare differenze nel valore energetico totale , del calcio e vitamina d [ 11 ]  . le informazioni fornite dallanalisi della bc su gruppi di atleti pu essere un importante indicatore dello stato nutrizionale e della prestazione fisica . 
 [ 12 ] hanno riscontrato differenze significative nella valutazione dei tessuti per distretti corporei , misurati con esame dxa , tra giocatori di calcio che ricoprivano in campo ruoli diversi . tali difformit possono essere correlate alla funzione di gioco cos come appare tra i giocatori di rugby e i controlli , 298 radiol med ( 2009 ) 114 : 286300 players , the correlation between age and fm was significant , whereas there was no correlation between fat and age in control subjects . 
in addition , soccer athletes who begin a season with a high level of fitness can maintain , and in some cases improve , bc and physical performance from before to after a competitive season . 
a correct combination of soccer - specific practices and strength and conditioning programmes can maintain and develop physical performance , allowing a soccer athlete to perform optimally throughout pre - , in - , and postseason play [ 51 ]  . 
data in the literature indicate that caution is necessary when dxa is used to compare patients with control subjects or to assess changes in bc in subjects whose relative weight changes significantly between measurements . 
it is often used in clinical settings , as well as to compare various bc methods for assessing body fat in overweight and obese children . in conclusion , bc assessments by dxa are readily available , less expensive and less invasive compared with other diagnostic imaging techniques , such as mri and ct . 
dxa is a simple , safe and precise technique that can measure bmd and soft - tissue composition not only in the whole body but also in specific regions of the body . this makes it an important tool not only for assessing and managing osteoporosis , but also for studying how softtissue composition changes in healthy and disease conditions . 
in aggiunta , i calciatori che cominciano una stagione con un alto livello di allenamento possono mantenere , e in alcuni casi migliorare , attraverso una valutazione della bc , la prestazione fisica prima e dopo la stagione calcistica . 
 necessaria una combinazione tra lattivit pratica calcistica specifica e un programma che mantenga e sviluppi la prestazione fisica [ 51 ]  . conclusioni la dxa stata designata per effettuare le misurazioni sulla massa ossea ed stato ampiamente dimostrato come questa sia una metodica accurata e precisa per tale utilizzo . inoltre , questa tecnica inizia ad essere utilizzata anche per la valutazione della bc . 
i dati presenti in letteratura suggeriscono una certa cautela nellimpiego di questa metodica nei confronti tra pazienti affetti da patologie e i controlli , come anche nella valutazione dei cambiamenti della bc in soggetti che presentano significative variazioni del peso tra le valutazioni . 
 la dxa offre facili e veloci informazioni circa il grasso corporeo , la massa magra e la massa ossea e , per la sua accuratezza , considerata un metodo di indagine superiore ad altri . 
non a caso utilizzata spesso nelle valutazioni cliniche , nella comparazione della bc con gli altri metodi per la misurazione del grasso corporeo , anche quello dei bambini obesi e sovrappeso . 
 per concludere , la valutazione della composizione corporea con metodica dxa prontamente disponibile , poco costosa e meno invasiva se confrontata con le altre metodiche diagnostiche come rm e tc . 
caudana1 1diagnostic imaging unit , 2vascular surgery unit , 3orthopaedics and traumatology unit , carlo poma hospital , viale albertoni 1 , 46100 , mantua , italy correspondence to : r . 
if diagnostic uncertainty persists , a bone biopsy is indicated . the inflammatory hyperaemia caused by the ulcer deteriorates the diagnostic quality of 40%50% of mr angiography studies in the infrapopliteal region . 
sedici pazienti diabetici sono stati sottoposti da gennaio 2006 a settembre 2007 a rm del piede per sospetta osteomielite monolaterale ; in 3 / 16 vi erano alterazioni radiografiche da osteo - artropatia neuropatica di charcot . 
la rm ha elevata sensibilit per losteomielite nel piede diabetico , ma pi bassa specificit dovuta soprattutto allosteo - artropatia neuropatica di charcot ; se permane dubbio diagnostico indicata la biopsia ossea . 
liperemia flogistica causata dallulcera deteriora il 40%50% degli studi angio - rm a livello sottopopliteo : in tali casi appropriata larteriografia selettiva per la possibilit di effettuare angioplastica nella stessa seduta . 122 radiol med ( 2009 ) 114 : 121132 keywords diabetic foot osteomyelitis foot mri peripheral vascular disease mr angiography parole chiave piede diabetico osteomielite rm piede vasculopatia periferica angio - rm introduction introduzione diabetic foot complications caused by neuropathy , ischaemia and resulting infection often lead to lower limb amputation , with severe disability and a significant impact on mortality . 
early recognition of osteomyelitis is essential for guiding medical and surgical treatment , which are usually implemented in an inpatient hospital setting [ 1 ]  . ( 89% ) the diagnosis of the clinical diagnosis of the infected foot is problematic in diabetic patients : up to two - thirds of patients may not present with the classic symptoms of deep infection owing to immunodeficiency related to diabetes mellitus . even laboratory examinations are often of little help , as inflammation indices may be absent [ 2 ]  . 
bone probing through skin ulceration is a clinical test with high positive predictive value foot osteomyelitis , although its low sensitivity ( 66% ) means that negative findings do not exclude bone infections [ 3 ]  . 
as a result , diabetic patients with suspected foot osteomyelitis require musculoskeletal imaging , both for the differential diagnosis particularly with neuropathic osteoarthropathy ( charcot foot ) and for an accurate evaluation of the extension of the infection , so as to plan surgery and avoid recurrences . 
moreover , diabetologists recommend that diabetic patients with foot ulcers should always undergo a vascular study to exclude the possibility that healing is prevented by peripheral arterial disease , which often has an insidious clinical onset due to the absence of neuropathic pain [ 4 ]  . our retrospective study presents the modern imaging approach to the infected diabetic foot , emphasizing the important role of magnetic resonance imaging ( mri ) in musculoskeletal and vascular assessment performed with the objective of selecting the most appropriate treatment . le complicanze del piede diabetico causate da neuropatia , ischemia e conseguente infezione portano spesso ad amputazione darto inferiore con grave disabilit e rilevante impatto anche sulla mortalit . 
lulcera del piede rappresenta in genere il primo segnale di allarme nel paziente diabetico e tende a progredire ( 15% dei casi ) verso losteomielite , in prevalenza con meccanismo di diffusione per contiguit . 
il riconoscimento precoce dellinsorgenza di osteomielite essenziale per indirizzare il trattamento sia medico che chirurgico , entrambi in genere attuati in ambiente ospedaliero [ 1 ]  . linquadramento clinico del piede infetto risulta difficile nel paziente diabetico : infatti fino a 2 / 3 dei pazienti possono non presentare i sintomi classici di infezione profonda a causa del deficit immunitario legato al diabete mellito ; anche gli esami di laboratorio spesso non sono di aiuto in quanto gli indici di flogosi possono essere assenti [ 2 ]  . 
il sondaggio osseo con specillo attraverso lulcera cutanea rappresenta un test clinico con elevato valore predittivo positivo ( 89% ) per la diagnosi di osteomielite del piede , ma la sua negativit non esclude linfezione ossea a causa della limitata sensibilit ( 66% ) [ 3 ]  . 
dunque nei pazienti diabetici con sospetta osteomielite del piede le metodiche di imaging muscolo - scheletrico sono necessarie sia per la diagnosi differenziale in particolare con losteo - artropatia neuropatica del piede di charcot sia per laccurato bilancio di estensione dellinfezione , cos da pianificare lintervento chirurgico ed evitare le recidive . 
inoltre , i diabetologi raccomandano di sottoporre sempre a studio vascolare il piede diabetico ulcerato , per escludere che larteriopatia periferica con esordio clinico spesso insidioso per lassenza di dolore dovuta alla neuropatia possa impedire la guarigione dellinfezione [ 4 ]  . lo scopo del nostro studio retrospettivo quello di presentare il moderno approccio imaging al piede diabetico infetto , sottolineando limportanza del ruolo che la risonanza magnetica ( rm ) ha avuto nella nostra esperienza nella valutazione muscolo - scheletrica e vascolare ai fini della scelta terapeutica ottimale . materials and methods materiali e metodi between january 2006 and september 2007 , 16 diabetic patients ( 11 men and five women , mean age 58 years , range 4278 ) with unilateral infected ulcer affecting the forefoot in ten cases , the midfoot in two and the hindfoot in four ( table 1 ) underwent mri of the foot . 
all patients underwent plain radiography of the foot , which was positive for osteomyelitis in 7 / 16 patients owing to the presence of corticoperiosteal thickening and / or of osteolytic foci in the cortical spongiosa close to the skin ulcer . 
tutti i pazienti sono stati sottoposti ad esame radiografico del piede , ritenuto positivo per osteomielite in 7 / 16 pazienti in base alla presenza di ispessimento cortico - periosteale e / o di focolai di osteolisi cortico - spongiosa in adiacenza allulcera cutanea . 
t1 - weighted spin - echo all musculoskeletal mri examinations were conducted with a 1.5 - tesla superconductive unit ( magnetom avanto : siemens ag medical solutions , erlangen , germany ) and an extremity coil . 
the mri protocol , selected on the basis of clinical suspicion and ulcer site , was different for studies of the forefoot compared with those of the midfoot and hindfoot and used a flex surface coil , a smaller field of view ( fov ) and predominantly coronal scans perpendicular to the metatarsal bones as recommended in the literature ( se : tr / te / fa 775 / 10 / 90 ) sequences and short - tau inversion - recovery sequences ( stir : tr / te / ti 5160 - 5760 / 53 / 150 ) were obtained in at least two planes , one of which was always sagittal , for selective fat suppression . 
in a few cases , a double t2and proton - density - weighted turbo - spin - echo sequence ( tse : tr / te / fa 3380 / 11103 / 150 ) was also obtained in the sagittal plane . 
parameters included 3 - mm slice thickness , 0.3 - mm interval for the t1 - weighted se sequences and 0.9 - mm interval for the stir sequences , and 16to 20 - cm fov . 
enhancement was assessed with a t1 - weighted tse sequence with selective ( tse - fs : tr / te / fa 791 / 10 / 150 ) with the same localization parameters as the stir sequences . fat suppression based on the suspicion of peripheral arteriopathy , 12 / 16 patients with infected diabetic foot also underwent mr angiography of the lower limbs with paramagnetic contrast agent ( table 1 ) 3 days to 6 weeks after mri of the foot , using the same scanner . 
this technique , through parallel imaging with dedicated phasedarray coils and high performing gradients , allows acquisithree peripheral arterial regions ( aortoiliac , tion of femoropopliteal , infrapopliteal ) within 42 s only ( excluding table motion )  . 
t1 - weighted 3d fast gradient - recalled - echo ( 3d fast - gre ) sequences were acquired in the coronal plane before and after administration of contrast material to allow subsequent subtraction . 
gadoliniumbenzyloxyproprionic - tetraacetic acid ( gd - bopta ) ( multihance , bracco , milan , italy ) at a dose of 0.15 mmol / kg , equivalent to 0.3 ( 3 / 9 oss . ) erano prevalenti le alterazioni dellosteo - artropatia neuropatica di charcot ( osteorarefazione , fratture , frammentazione ossea , lussazione , reazione osteoblastica riparativa )  . 
un paziente con ulcera del retropiede ed esame radiografico negativo stato sottoposto a biopsia ossea tcguidata del calcagno per interpretare il quadro rm dubbio . la diagnosi finale di osteomielite o la sua esclusione stata ottenuta integrando i rilievi clinico - laboratoristici con quelli imaging in tutti casi ; in 11 / 16 pazienti la diagnosi stata completata con esame batteriologico e / o istologico . tutti gli esami rm muscolo - scheletrici sono stati effettuati con apparecchiatura superconduttiva da 1 , 5 tesla ( magnetom avanto , siemens ag medical solutions , erlangen , germania ) e bobina da estremit . 
il protocollo rm , scelto sulla base del sospetto clinico e della sede dellulcera , stato diverso per lo studio dellavampiede rispetto a quello del medio e retropiede , impiegando bobina flex di superficie , fov pi piccolo e acquisizioni prevalenti sul piano coronale ovvero perpendicolare ai metatarsi come raccomandato in letteratura [ 5 ]  . 
sono state acquisite almeno in due piani , di cui uno sempre sagittale sequenze spin - echo t1 - pesate ( se : tr / te / fa 775 / 10 / 90 ) , sequenze short - inversion - time inversion - recovery per la selettiva soppressione del segnale adiposo ( stir : tr / te / ti 51605760 / 53 / 150 )  . 
in alcuni casi stata acquisita anche la sequenza turbo - spin - echo a doppia pesatura t2 e densit protonica ( tse : tr / te / fa 3380 / 11103 / 150 ) sul piano sagittale . 
sono stati impiegati spessore di fetta 3 mm , intervallo di 0 , 3 mm per le se t1 - pesate e di 0 , 9 mm per le stir , fov compreso tra i 16 cm ed i 20 cin tutti i pazienti lo studio rm stato completato con somministrazione di mezzo di contrasto ( mdc ) paramagnetico per via endovenosa ( dotarem , guerbet , aulnay - sous - bois , francia ) alla dose di 0 , 1 mmol / kg equivalente a 0 , 2 ml / kg ; lenhancement stato valutato con sequenza turbo - spin - echo t1 - pesata a selettiva soppressione del segnale adiposo ( tse - fs : tr / te / fa 791 / 10 / 150 ) con gli stessi parametri di centratura delle sequenze stir . nel sospetto di arteriopatia periferica 12 / 16 pazienti con piede diabetico infetto hanno effettuato anche lo studio angio - rm degli arti inferiori con mdc paramagnetico ( tabella 1 ) , a distanza di tempo variabile ( range : 3 giorni6 settimane ) dallesame rm del piede , utilizzando la stessa apparecchiatura rm . 
langio - rm degli arti inferiori stata effettuata con tecnica bolus - chase a tavolo mobile [ 6 ] : tale tecnica , grazie alla disponibilit dellimaging parallelo con bobine phased - array dedicate e di gradienti pi performanti , consente lacquisizione di 3 distretti arteriosi periferici ( aorto - iliaco , femoro - popliteo , infra - popliteo ) nellarco di soli 42 secondi ( escluso il movimento del tavolo )  . 
le sequenze fast - gradient - recalled - echo tridimensionali ( 3d fast - gre ) t1 - pesate sono state acquisite sul piano coronale prima e dopo somministrazione di mdc per consentire la successiva sottrazione . 
la somministrazione per via endovenosa di gadolinio - bopta ( multihance , bracco , milano , italia ) alla dose di 0 , 15 mmol / kg , equivalente a 0 , 3 ml / kg , radiol med ( 2009 ) 114 : 121132 ml / kg , was administered as an intravenous bolus ( 20 ml on average ) using a two - phase flow injector ( the first half at 1.2 ml / s , the second half at 0.6 ml / s ) , followed by the injection of 20 ml of saline at a flow rate of 1 ml / s . 
acquisition of the 3d gre sequences started when the care bolus technique detected the arrival of the contrast bolus in the aorta . during the postprocessing stage , after the subtraction process , panoramic coronal maximum intensity projection ( mip ) reconstructions were obtained from the aorta to the foot arteries by creating a composite image of the three regions . three radiologists retrospectively reviewed the mri images from the musculoskeletal study of the foot ( ur , ev , rc ) and the vascular study ( ur , at , rc )  . 
the most experienced radiologist ( rc > 15 years ) was considered the reference standard in the event of disagreement among less experienced radiologists ( ur , ev , at < 5 years )  . 
a primary sign of osteomyelitis on mri is evidence of low - signal - intensity areas in the bone marrow on t1 - weighted se images , with higher signal intensity on stir images and enhancement after contrast administration . 
secondary signs are identified close to the altered bone marrow signal and include oedema caused by septic inflammation ( cellulitis or phlegmon ) , soft - tissue abscess , skin ulcer and fistula , with possible interruption of the cortical bone . 
mr angiography of the lower limbs assessed the patency or stenosis - occlusion of the peripheral arteries and the presence of venous contamination artifacts superimposed enhancement of the venous circulation which is one of the main limitations of the technique , as it deteriorates the diagnostic quality of the images . 
with this assessment , the images of each of the three vascular regions were judged as either adequate or inadequate for peripheral revascularization . avvenuta in bolo ( in media 20 ml ) tramite iniettore con velocit di flusso bifasica ( la prima met a 1 , 2 ml / s , la seconda met a 0 , 6 ml / s ) , seguita dalla iniezione di 20 ml di soluzione salina con flusso di 1 ml / s . 
la diagnosi rm di osteomielite stata formulata sulla base della concordanza di segni primari e secondari [ 7 ] : la semeiotica rm della osteomielite considera come segno primario la presenza a livello del tessuto osteo - midollare di aree di ridotta intensit di segnale nelle immagini se t1pesate , con incremento dellintensit di segnale in quelle stir ed enhancement dopo somministrazione di mdc paramagnetico , mentre i segni secondari sono quelli rilevabili in adiacenza allalterazione del segnale osteo - midollare e comprendono ledema dovuto alla flogosi settica ( cellulite o flemmone ) , lascesso dei tessuti molli , lulcera cutanea e la fistola con leventuale interruzione della corticale ossea . nelle indagini angio - rm degli arti inferiori sono state valutate la perviet o la steno - occlusione delle arterie periferiche e la presenza di artefatti da contaminazione venosa ovvero lenhancement sovrapposto del circolo venoso uno dei principali limiti in quanto riduce la qualit diagnostica dellesame . 
i reperti angio - rm evidenziati sulle ricostruzioni mip sono stati analizzati per conferma anche nelle sequenze sottratte con software 3d ; cos valutate , le immagini di ciascuno dei tre distretti vascolari esaminati sono state giudicate sufficienti o insufficienti per la scelta del trattamento di rivascolarizzazione periferica . 
 results risultati in 13 / 16 patients with infected diabetic foot ulcers , the final diagnosis was osteomyelitis , whereas in 3 / 16 patients it was cellulitis ( table 1 )  . 
a the sagittal short - tau inversion - recovery sequence ( stir ) image shows a pathological fracture of the calcaneus and dislocation of the proximal fragment due to retraction of the achilles tendon . 
b magnetic resonance angiography ( mra ) of the right lower limb is hindered by venous contamination in the distal third , whereas the left infrapopliteal arteries are clearly visible up to the plantar arch . 
the mri diagnosis of exclusion of osteomyelitis proved correct in two patients with infected ulcer and cellulitis ( true negatives ) in whom conventional radiology had identified alterations due to neuropathic osteoarthropathy . 
overall , foot mri permitted correct identification or exclusion of osteomyelitis in 15 / 16 patients , with a high accuracy and sensitivity , even in the presence of radiographic evidence of neuropathic osteoarthropathy ( three cases )  . 
mri also proved useful for assessing the extent of osteomyelitis for surgical planning purposes ( four minor and one major amputation ) , for identifying soft - tissue abscesses requiring drainage ( three cases ) as well as other infectious complications including septic arthritis ( four cases ) , pathological fracture ( one case , fig . 1a ) and septic tenosynovitis ( one case )  . non da flogosi settica del tessuto osteo - midollare . 
2a - c reactive bone marrow oedema of the talus and calcaneus due to neuropathy in a diabetic patient with mal perforans and normal radiographic findings [ false - positive magnetic resonance imaging ( mri ) diagnosis of osteomyelitis ]  . 
a the coronal t1 - weighted turbo - spin - echo ( tse ) image with fat suppression after administration of paramagnetic contrast material reveals diffuse changes in signal intensity of bone marrow and soft tissues , as well as moderate contrast enhancement in the talus and in the subtalar portion of the calcaneus , wrongly interpreted as osteomyelitis associated with cellulitis . 
b in the axial short - tau inversion recovery ( stir ) image , the area of increased signal intensity in the calcaneus is identified to perform a bone biopsy . 
2a - c edema osteo - midollare reattivo talo - calcaneare da neuropatia in paziente diabetico con mal perforante e quadro radiografico normale ( errore rm di falsa positivit per la diagnosi di osteomielite )  . 
a nellimmagine coronale tse t1 - pesata con soppressione del segnale adiposo dopo somministrazione di mdc paramagnetico diffuse alterazioni del segnale osteo - midollare e dei tessuti molli in sede talare e nella porzione subtalare del calcagno caratterizzate da discreto enhancement , erroneamente interpretate come osteomielite associata a cellulite . 
c la biopsia ossea sotto guida tc ha escluso linfezione ossea . regions , the diagnostic patients with infected diabetic foot allowed evaluation of the diagnostic quality of the images obtained in the three vascular regions . 
these five patients later underwent selective arteriography of the ulcerated lower limb with an anterograde approach , owing to a suspicion of concomitant distal diabetic arterial disease ( table 1 )  . 
in 4 / 5 patients , arteriosclerotic occlusive lesions of the crural arteries were identified , and percutaneous transluminal angioplasty ( pta ) was performed during the same session . after the mr angiography , 9 / 12 patients underwent three of whom had a surgical vascular surgery , effettuati in 12 pazienti con piede diabetico infetto ha permesso di valutare la qualit diagnostica delle immagini ottenute in ciascuno dei tre distretti vascolari esaminati . 
questi 5 pazienti sono stati successivamente sottoposti ad arteriografia selettiva con approccio anterogrado dellarto inferiore affetto dallulcera , nel sospetto di concomitante arteriopatia diabetica distale ( tabella 1 )  . 
in 4 / 5 pazienti sono state riscontrate lesioni arteriosclerotiche steno - occlusive delle arterie crurali e si proceduto ad angioplastica ( pta ) nella stessa seduta . complessivamente 9 / 12 pazienti sono stati sottoposti dopo lo studio angio - rm a intervento vascolare , di cui 3 mediante by - pass chirurgico femoro - popliteo e 6 con tratta128 radiol med ( 2009 ) 114 : 121132 fig . 
3a - c severe charcot neuropathic osteoarthropathy , infected plantar ulcer and bone infarcts due to peripheral arterial disease [ osteomyelitis excluded by magnetic resonance imaging ( mri ) ]  . 
3a - c grave osteo - artropatia neuropatica di charcot , ulcera infetta plantare e infarti ossei da arteriopatia periferica ( rm negativa per osteomielite )  . a nel radiogramma in incidenza antero - posteriore frammentazione ossea del medio - piede in fase cronica con tipica frattura - dislocazione di lisfranc . 
liperintensit di segnale a livello del primo e secondo dito dovuta ad un artefatto ( insufficiente soppressione del segnale adiposo alla periferia della bobina da estremit )  . femoropopliteal bypass , and six underwent endovascular angioplasty ( three the femoropopliteal and infrapopliteal regions , three in the infrapopliteal region only ) with immediate technical success in 5 / 6 cases . in both mento endovascolare di angioplastica ( 3 a livello sia femoro - popliteo che infra - popliteo , 3 solo in sede infrapoplitea ) con successo tecnico immediato in 5 / 6 casi . discussion conventional radiology is still the first - line modality in the study of the diabetic foot owing to its rapidity , ease of use and inexpensiveness . 
it also allows the diagnosis of clinically overt osteomyelitis , reveals alterations due to charcots neuroarthropathy and is useful for the follow - up . known limits of conventional radiology , especially if performed in the early stage of bone infection , are its low sensitivity ( 60% ) and specificity ( 66% ) [ 8 ]  . 
the former is due to a need for 30%50% bone reabsorption , a process taking up to 23 weeks from the onset of infection , whereas the latter depends on the wide spectrum of diseases entering the differential diagnosis , first of all neuropathic discussione lindagine radiologica convenzionale rimane la metodica di primo livello per lo studio del piede diabetico per rapidit , facilit di esecuzione e bassi costi : oltre a permettere la diagnosi di osteomielite nella fase conclamata rileva le alterazioni da osteo - artropatia neuropatica di charcot ed utile per il follow - up . 
i limiti noti dellindagine radiologica , specie se espletata nelle prime fasi dellinfezione ossea , sono la bassa sensibilit ( 60% ) e specificit ( 66% ) [ 8 ] ; la prima dovuta alla necessit di un riassorbimento osseo pari al 30%50% , processo che impiega fino a 23 settimane dallinizio dellinfezione , mentre la seconda dipende dallampio spettro di patologie coinvolte nella diagnosi differenziale , prima fra tutte losteo - artropatia neuropatica che colpisce fino al 3% dei pazienti diabetici . 
the midfoot and hindfoot bones are the most commonly involved by this disease , which presents with demineralization , fractures , fragmentation , joint dislocation and collapse of the plantar arch , with the classic charcot deformity . 
the use of more sophisticated imaging modalities ( either mri or scintigraphy ) is indicated when radiography demonstrates alterations due to charcot neuroarthropathy or whenever the clinicallaboratory suspicion of osteomyelitis is high , or finally to demonstrate complications . 
bone biopsy , although not routinely performed because of its invasiveness , is considered the gold standard in the diagnosis of osteomyelitis and is still recommended to confirm an uncertain diagnosis and isolate the pathogen [ 9 ]  . mri has come to replace ct , as it is better able to identify bone marrow changes and evaluate septic involvement of the soft tissues , which allows surgery to be planned in such a way as to prevent recurrence of infection after amputation or abscess drainage [ 10 ]  . 
it is thus reserved for patients with contraindications to mri or with doubtful mri findings , or to assess response to antibiotic therapy during the follow - up [ 9 ]  . 
when there is topographic concordance between the primary and secondary mri signs , the mean reported sensitivity and mediopiede e del retropiede sono quelle pi spesso coinvolte da questa patologia che si manifesta con demineralizzazione , fratture , frammentazione , lussazione articolare fino al collasso dellarcata plantare , con la classica deformit del piede di charcot . 
il ricorso a metodiche di imaging pi sofisticate ( rm o scintigrafia ) indicato quando lesame radiologico riscontri alterazioni da osteo - artropatia neuropatica di charcot oppure qualora il sospetto di osteomielite sia elevato dal punto di vista clinico - laboratoristico o , infine , per evidenziare le complicanze dellinfezione . 
la biopsia ossea , bench non praticata di routine a causa dellinvasivit , tuttoggi considerata il gold standard per la diagnosi di osteomielite e viene dunque ancora raccomandata per confermare una diagnosi dubbia e per isolare lagente patogeno [ 9 ]  . la rm oggi ha sostituito la tc per la migliore capacit di identificare le alterazioni osteo - midollari e di valutare il coinvolgimento settico dei tessuti molli , ci che consente di pianificare gli interventi chirurgici al fine di evitare recidive infettive dopo amputazione o drenaggio di ascessi [ 10 ]  . la scintigrafia con granulociti tecneziati presenta accuratezza lievemente inferiore a quella della rm nella diagnosi di osteomielite [ 11 ] e risulta pi indaginosa e costosa ; viene attualmente pertanto riservata ai pazienti che hanno controindicazioni alla rm oppure in quelli con quadro rm dubbio o , infine , nel follow - up per valutare la risposta alla terapia antibiotica [ 9 ]  . 
la rm rappresenta pertanto lindagine preferenziale di secondo livello per la diagnosi di osteomielite : qualora vi sia concordanza topografica tra segni rm primari e secondari i valori medi di sensibilit e 130 radiol med ( 2009 ) 114 : 121132 specificity are 94% ( range 88%99% ) and 83% ( range 78%89% ) , respectively [ 2 , 7 ]  . 
on the other hand , a positive mri study is not always sufficient to establish a diagnosis of osteomyelitis , even when there is topographic concordance between primary and secondary signs . 
administration of paramagnetic contrast material increases specificity because enhancement of bone marrow , as assessed in the t1weighted sequences with selective fat suppression , is regarded as typical of osteomyelitis rather than of neuropathic osteoarthropathy [ 12 ]  . 
nonetheless , some authors have found that neuropathy - related reactive bone marrow oedema often associated with trabecular microfractures and joint effusion may also enhance , thus becoming indistinguishable from osteomyelitis [ 13 ]  . 
 the differential diagnosis between osteomyelitis and neuropathic osteoarthropathy is not a problem when the skin is intact but only when stress - related biomechanical alterations promote skin ulceration and the foot appears swollen , warm and erythematous . 
 in the chronic phase of neuropathic osteoarthropathy , subchondral cysts , osteoporosis and bone fragmentation may appear , with loss of articular relationships and subsequent endosteal and periosteal reparative bone proliferation , which are easily detected even on conventional radiology . in these cases , mri can usually be interpreted correctly if compared with the radiographic pattern [ 1214 ]  . 
the ankle - arm index ( aai ) may overestimate systolic pressure owing to calcified sclerosis of the tunica media hindering compression of the arteries , transcutaneous oximetry may be misleadingly low due to the presence of oedema and , finally , colour doppler ultrasound may not allow adequate evaluation of the infrapopliteal arterial region , the most commonly affected by diabetic arterial disease [ 4 ]  . 
 in genere la rm permette di escludere con affidabilit losteomielite se negativa o se lalterazione del segnale osteo - midollare lontana dallulcera , ma non sempre sufficiente a formulare diagnosi di osteomielite quando positiva , anche se vi concordanza topografica tra i segni rm primari e quelli secondari . 
la somministrazione di mdc paramagnetico risulta utile per aumentare la specificit dellesame dato che lenhancement del tessuto osteo - midollare , valutato nelle sequenze t1 - pesate con selettiva soppressione del segnale adiposo , considerato tipico dellosteomielite pi che delle alterazioni dovute a osteo - artropatia neuropatica [ 12 ]  . 
tuttavia , alcuni autori hanno riscontrato la possibilit che in alcuni casi ledema midollare reattivo da neuropatia spesso associato a micro - fratture trabecolari e versamento articolare possa presentare enhancement , risultando indistinguibile dallosteomielite [ 13 ]  . 
 il problema della diagnosi differenziale tra osteomielite e osteo - artropatia neuropatica non si pone quando la cute integra , ma solo quando le alterazioni bio - meccaniche dovute al carico favoriscono lulcerazione della cute ed il piede appare tumefatto , caldo , eritematoso ; in tale fase acuta la neuro - artropatia pu simulare losteomielite sia dal punto di vista clinico che radiologico . 
pertanto , in tutti i casi con rm positiva , ma discordante dai dati clinici , colturali , laboratoristici e radiologici , necessario ricorrere alla biopsia ossea per conferma , utilizzando la guida fluoroscopica o tc per raggiungere la sede della alterazione del segnale rm , scegliendo un tragitto che attraversi la cute integra , al fine di evitare la possibile contaminazione ossea [ 9 ]  . 
 nellosteo - artropatia neuropatica fase cronica possono comparire cisti subcondrali , osteoporosi e frammentazione ossea con perdita dei rapporti articolari e successiva proliferazione ossea riparativa endo e periosteale , facilmente rilevabili gi allesame radiologico convenzionale . 
 le indagini strumentali vascolari pi comunemente utilizzate per lo screening dellarteriopatia periferica presentano alcuni limiti nel paziente diabetico con osteomielite del piede : lindice caviglia - braccio ( abi ) pu sovrastimare la pressione sistolica per la sclerosi calcifica della tunica media che rende le arterie non comprimibili , lossimetria trans - cutanea pu essere falsamente bassa per la presenza di edema in corso di infezione e , infine , leco - color doppler radiol med ( 2009 ) 114 : 121132 quently , mr angiography plays a crucial role in these highrisk patients , allowing a noninvasive panoramic study of the lower - limb arteries [ 15 ]  . 
the advantages of mr angiography over ct angiography are the low nephrotoxicity of paramagnetic contrast agents , the absence of exposure to ionizing radiation and easier and more accurate postprocessing , especially in patients with diffuse wall calcifications [ 16 ]  . 
 until recently before the implementation of parallel imaging that significantly reduces acquisition times one of the major limits of lower - limb mr angiography was the filling of the venous circulation at the infrapopliteal level , which rendered up to 43% of mr angiography studies nondiagnostic [ 17 ]  . 
there is evidence that cellulitis and ulcers are the only two circumstances capable of significantly accelerating the transit time of contrast material through the peripheral arteries [ 18 ]  . 
in our experience , within the limits shown in the infrapopliteal region , mr angiography proved adequate for planning surgical or endovascular treatment , allowing healing of the ulcer and infection or identification of the level of amputation for critical limb ischaemia . conclusions pu non consentire una adeguata valutazione del distretto arterioso infra - popliteo , il pi frequentemente colpito dallarteriopatia diabetica [ 4 ]  . 
dunque , langio - rm ha assunto un ruolo cruciale in questi pazienti ad alto rischio , consentendo la valutazione panoramica arteriosa degli arti inferiori in maniera non invasiva [ 15 ]  . 
i vantaggi dellangiorm rispetto allangio - tc sono rappresentati dalla bassa nefrotossicit dei mdc paramagnetici , dallassenza di esposizione radiante e dal post - processing pi facile ed accurato , specie nei pazienti con estese calcificazioni parietali [ 16 ]  . 
 fino a pochi anni fa , prima dellapplicazione dellimaging parallelo che permette di ridurre sensibilmente i tempi di acquisizione , uno dei limiti maggiori dello studio angio - rm degli arti inferiori era rappresentato dal riempimento del circolo venoso a livello infra - popliteo : fino al 43% degli esami angio - rm risultavano non diagnostici [ 17 ]  . 
nella nostra esperienza langio - rm , pur con i limiti evidenziati a livello del distretto infrapopliteo , risultata idonea a pianificare la strategia di trattamento chirurgico o endovascolare per permettere la guarigione dellulcera e dellinfezione o comunque a individuare il livello di amputazione nellischemia critica di arto . mri of the diabetic foot is highly sensitive in the study of osteomyelitis and infectious complications . 
bolus - chase mr angiography of the lower limbs is the preferred vascular study in diabetic patients for planning peripheral revascularization . inflammatory hyperaemia of the diabetic foot , however , affects visualization of the infrapopliteal arteries in around 40%50% of limbs with infected ulcers . 
in these cases , in the presence of known patency of the femoropopliteal axis , the use of selective arteriography is justified by the opportunity to perform angioplasty during the same session . conclusioni la rm del piede diabetico ha elevata sensibilit per losteomielite e per le complicanze infettive . 
nei casi dubbi la biopsia ossea con guida imaging resta lunica indagine in grado di discriminare i casi di falsa positivit alla rm dovuti a osteo - artropatia neuropatica di charcot . 
we initiated a prospective , blinded investigation on 29 patients affected by oncological diseases ( n = 14 ) or lymphoma ( n = 15 ) , who underwent fluorodeoxyglucose ( fdg ) - based pet - ct and whole - body dwibs for restaging purposes . 
reader 1 had a sensitivity of 89.07% , a specificity of 98.5% , and an accuracy of 97.65% , with a positive predictive value ( ppv ) of 85.48% and a negative predictive value ( npv ) of 98.91%. 
abbiamo avviato uno studio prospettico , in cieco , su 29 pazienti oncologici ( 15 con linfoma e 14 con altre neoplasie ) , che si sono sottoposte nel loro normale percorso diagnostico a tac - pet con fluro - desossi - glucosio ( fdg ) e anche ad unindagine con wb - dwibs , per restaging di malattia . 
lagreement tra i due radiologi risultata quasi perfetta ( = 0 , 93 )  . rispettivamente i due radiologi hanno avuto una sensibilit del 89 , 07% e 87 , 39% , specificit del 98 , 5% e del 98 , 39% , accuratezza diagnostica del 97 , 65% e 97 , 8% per i due lettori , ppv del 85 , 48% e 88 , 13% e npv 98 , 91 e 98 , 75% . radiol med ( 2009 ) 114 : 117 conclusions . 
un difetto dello studio sicuramente larruolamento di pazienti con lesioni multiple disseminate , leterogeneit della casistica . keywords diffusion weighted imaging whole - body pet - ct parole chiave diffusion weighted imaging whole body tc - pet introduction introduzione in oncology , tumour therapy and follow - up are strongly based on reliable diagnostic imaging techniques enabling evaluation of the entire body for disease detection and staging . 
whole - body imaging is mainly applied to screening and staging , and the role of magnetic resonance imaging ( mri ) and positron emission tomography computed tomography ( pet - ct ) among whole - body imaging techniques has been well assessed in the literature [ 1 ]  . whole - body mri , intended as a conventional mri technique , has excellent tissue contrast and high spatial resolution and allows detailed morphological evaluation . 
these properties make it particularly suited to the study of bone marrow , very sensitive in detecting and locating skeletal metastasis and superior to ct in depicting bone and parenchymal infiltration [ 2 ] in almost all organs ( though not yet for lung parenchyma )  . since the introduction of pet - ct in 2001 , anatomicmetabolic studies have been found to be extremely sensitive in characterising lymph nodes and detecting metastasis . however , they also tend to be affected by false - positive results mainly related to brown fat , muscle tissue or inflammatory processes given that fluorodeoxyglucose ( fdg ) is not entirely a cancer - specific tracer . 
in addition , bowel muscular activity and urinary tract excretion hinder the interpretation of studies of the gastrointestinal and urinary system [ 3 ]  . the other whole - body technique , 99mtc - phosphonatebased skeletal scintigraphy ( or bone scan ) , is the standard nuclear - medicine method for the initial staging of primary or secondary bone tumours . 
however , it provides limited anatomical detail , has low sensitivity and specificity and only depicts bone metastasis at a relatively late stage when osteoblastic reaction to tumour deposits has already occurred [ 49 ]  . diffusion - weighted imaging ( dwi ) , a validated technique for mr evaluation of the brain , has recently been in oncologia , la terapia ed il controllo della risposta ad essa ( follow - up ) sono strettamente legati alla disponibilit di metodiche di imaging diagnostico , che permettano lanalisi di tutti i distretti corporei potenzialmente interessati dalla patologia e dalla sua diffusione ( whole - body ) , e che siano affidabili nel riconoscere e stadiare la patologia . 
per essere appropriato , lo screening di secondo e terzo livello deve disporre di una metodica caratterizzata da elevata specificit , applicata su una patologia ad elevata prevalenza nella popolazione . 
limaging whole - body ( whole body imaging , wbi ) orientato pertanto principalmente a scopi di screening e staging ; in letteratura [ 1 ] , ben assodato il ruolo dellimaging con risonanza magnetica ( whole body magnetic resonance imaging , wb - mri ) e della tomografia computerizzata abbinata alla tomografia ad emissione di positroni ( tc - pet )  . 
 per wb - mri , si intende lapplicazione total - body della tecnica rm convenzionale ; tale tecnica caratterizzata da eccellente risoluzione di contrasto ed alta risoluzione spaziale , permette una valutazione morfologica dettagliata ; queste caratteristiche rendono la metodica particolarmente idonea allo studio del midollo osseo , molto sensibile nella individuazione e localizzazione delle metastasi scheletriche , superiore alla tc nella definizione dellinfiltrazione ossea e parenchimatosa [ 2 ] , per quasi tutti gli organi ( allo stato attuale , non per il parenchima polmonare )  . dallintroduzione della tc - pet nel 2001 , lo studio anatomo - funzionale risultato particolarmente sensibile per la caratterizzazione dei linfonodi e delle metastasi , sebbene limitato da false positivit . 
queste ultime sono generate prevalentemente dal grasso bruno , da processi infiammatori o da tessuti muscolari metabolicamente attivi , dal momento che il marcatore metabolico il fluorodesossi - glucosio ( fdg ) , marker non specifico per lattivit cellulare neoplastica ; inoltre lattivit muscolare intestinale e lescrezione urinaria del metabolita rendono di difficile interpretazione questi due apparati [ 3 ]  . laltra principale metodica wb disponibile in medicina nucleare la scintigrafia ossea con tecnezio ( bone scan , bs ) , che rappresenta la metodica standard di staging dei radiol med ( 2009 ) 114 : 117 extended to extracranial districts [ 10 , 11 ] , although with several technical difficulties due to hardware limitations and the mobile nature of the organs to be studied . 
this is an echo planar imaging pulse sequence combined with short tau inversion recovery ( epi - stir ) suitable for evaluating extracranial districts and for whole - body imaging , partly owing to the excellent images obtained with postprocessing algorithms . apart from one congress abstract [ 13 ] , no papers have been published on the subject since takaharas report [ 12 ] , so the accuracy of whole - body dwibs in comparison with the pet - ct is as yet unknown . 
 the aim of this study was to assess the overall diagnostic accuracy of whole - body dwibs in comparison with petct , which is considered the standard of reference among whole - body imaging modalities . materials and methods patients from february 2007 to august 2007 , we enrolled 29 consecutive patients undergoing pet - ct for oncological and oncohaematological diseases ( table 1 ) and fulfilling the requisites for the study . inclusion criteria patients were eligible if they met the following criteria : 1 . 
they volunteered for the mr scan , were able to understand and sign an informed consent form informing them that : ( a ) the examination was not necessary but might tumori ossei primitivi o secondari . 
con lo sviluppo di sequenze pi veloci , insieme al potenziamento dei gradienti variabili e allintroduzione della tecnica del tavolo mobile , limaging rm pesato in diffusione , esteso allo studio di tutto il corpo diventato tecnicamente realizzabile . 
 [ 12 ] hanno messo a punto una sequenza per limaging rm pesato in diffusione , denominata diffusion weighted body imaging with background body signal suppression ( dwibs ) , una sequenza echo - planar abbinata alla soppressione del segnale del grasso con tecnica stir , ottimizzata per la valutazione dei distretti extracranici e particolarmente adatta ad un impiego whole - body , grazie anche agli ottimi risultati iconografici ottenuti con opportuni algoritmi di post - processing . 
pertanto , fino ad oggi , laccuratezza diagnostica della tecnica wb - dwibs in confronto con la tc - pet non nota . scopo del presente studio di valutare laccuratezza diagnostica della wb - dwibs in comparazione con il gold standard nellambito delle metodiche di imaging wholebody , la tc - pet . table 1 patient series grouped by type of neoplasm tabella 1 casistica raggruppata per tipologia di neoplasia primary tumour number of patients sedi del tumore primitivo numero di pazienti lymphoma lung breast kidney sarcoma primitive neuroectodermal tumour prostate linfoma polmone mammella intestino rene sarcoma pnet prostata radiol med ( 2009 ) 114 : 117 help to understand or stage their disease in the future , ( b ) the study required no contrast medium injection , ( c ) the study took 20 min , and ( d ) no ionising radiation would be used 2 . 
a q - body coil was used , with the patient positioned feet first on an extended anatomical coverage table , based on rolling - table technology ( mobitrak , philips )  . 
after a scout pulse sequence , we acquired a dwibs pulse sequence and an epi - stir single - shot pulse ( table 2 ) in the axial plane , repeated for up to four stacks to encompass all anatomical districts from the head to at least the distal thigh , similarly to the pet - ct acquisition protocol . 
we adopted two different b - factor values in the diffusion pulse sequence , b = 500 and b = 1000 s / mm2 , but only the latter was used for reading purposes , as suggested by takahara et al . 
the acquisition time for the protocol was 18 min which , summed to the scout sequence time , implied a total room occupation time of 20 min . nuclear medicine pet - ct scans were acquired on a hybrid siemens ( siemens , erlangen , germany ) system consisting of an lutetium oxyorthosilicate ( lso ) pet scanner ( hi - rez ) with pico - 3d electronics and a 16 - row ct device ( somatom sensation 16 )  . 
 image reformatting and analysis after acquisition and the choice of the higher b value , the materiali e metodi pazienti da febbraio 2007 fino ad agosto 2007 abbiamo arruolato 29 pazienti consecutivi , in previsione di eseguire una valutazione tc - pet , per patologie oncologiche , anche del distretto emolinfopoietico ( tabella 1 ) , che soddisfacevano i criteri di inclusione . criteri di inclusione i pazienti sono stati considerati reclutabili in relazione ai seguenti criteri : 1 . 
abbiamo utilizzato la bobina q - body , posizionando il paziente ( in modo che entrasse nel gantry caudocranialmente , feet first ) , su un tavolo porta - paziente a copertura anatomica estesa , basata sulla tecnologia del tavolo mobile ( mobitrak , philips )  . 
dopo una sequenza di centratura , abbiamo acquisito una sequenza dwibs ( stirecho planar , single shot ) ( tabella 2 ) sul piano assiale , ripetuta 4 volte per coprire tutti i distretti anatomici dalla testa alla coscia distale , in modo da replicare la copertura anatomica dellesame tc - pet . 
la sequenza stata pesata con un doppio valore di b ( b = 500 e b = 1000 s / mm2 ) , utilizzando solo il secondo per la refertazione , come suggerito da takahara et al . 
al termine , si provveduto a invertire la scala dei grigi , in modo che su sfondo bianco ( le aree prive di segnale ) si potesse riconoscere la patologia come immagini con diverse intensit di grigio ( le aree con segnale accentuato ) , con tutte le gradazioni intermedie . 
le immagini whole - body mip e mpr cos elaborate sono state poi salvate nel database dello scanner . anche le immagini native assiali sono state separate sulla base del parametro b , e quelle con b = 1000 s / mm2 , dopo aver preparato la finestra di visualizzazione in modo ottimale , sono state salvate nel database delle immagini . 
tutte le immagini , elaborate da un medico specializzando esperto , sono state private delle informazioni anagrafiche e salvate su una memoria di massa mobile ( cd ) , in formato dicom , registrando ogni supporto con il numero progressivo del paziente . 
le sessioni di refertazione sono state condotte , indipendentemente , da due radiologi esperti in rm ( a.s , lettore 1 e a.c. lettore 2 ) , rispettimente con 8 e 18 anni di pratica professionale in rm , reciprocamente inconsapevoli del risultato della refertazione dellaltro , e del risultato della lettura della tc - pet . i due radiologi hanno riempito una scheda di lettura predefinita , costituita da un foglio elettronico ( excel , microsoft , redmond , usa ) , nel quale sono state individuate 40 sedi anatomiche , scheletriche e viscerali , basandosi su unanaloga schematizzazione elaborata da lauenstein et al . radiol med ( 2009 ) 114 : 117 4 - mm - thick multiplanar reformations ( mpr ) in the coronal plane , and ( c ) multiple 4 - mm - thick mpr in the sagittal plane oriented to include the midline as well as the spine and paraspinal regions . 
all reformatted images were then fused by means of mobiview software ( philips ) with the smooth fusion algorithm to obtain whole - body mip and mpr images . the grey scale was subsequently inverted to allow visualisation of abnormalities ( increased signal ) as grey areas of varying intensity against a white background ( without signal )  . all of the whole - body mip and mpr images were saved in the scanners patient - image database . 
the native axial slices were separated on the basis of the b value , and those acquired with b = 1 , 000 s / mm2 were also saved in the image database after optimal window setting . 
all image sets , processed by an experienced trainee radiologist , were rendered anonymous and stored in digital imaging and communications in medicine ( dicom ) format on an optical disc marked with the patients progressive number for subsequent reading . 
images were read independently by two experienced mri radiologists ( reader 1 : as , with 8 years experience ; reader 2 : ac , with 18 years experience ) who were unaware of each others mri report and of the pet - ct results . the two readers noted their findings on a predefined reading grid consisting of a spreadsheet ( excel , microsoft , redmond , usa ) listing 40 skeletal and visceral sites and subsites , modified from the classification proposed by lauenstein et al . 
radiological reading time for each patient was also recorded . the pet - ct study was reported by the nuclear physician on a similar reading grid as that used by the radiologists . 
the nuclear physician first read the source axial pet images separately and then overlaid on axial ct images and next reviewed the coronal and sagittal images reconstructed with the mpr algorith image analysis included assessment of metabolic uptake of the tracer in terms of standardised uptake value ( suv )  . postprocessing and mean reading times were calculated . the cohen constant was calculated to determine the grade of interobserver agreement . 
for each reader , we calculated diagnostic accuracy , sensitivity and specificity of the wholebody dwibs readings together with negative and positive predictive values ( npv and ppv ) and compared the readings with those performed by the nuclear physician on the pet - ct studies . 
 lo specialista medico nucleare ha refertato lesame tcpet , su unanaloga scheda di lettura , valutando le immagini assiali pet , poi sovrapposte alle immagini tc e infine ricostruite nei piani coronale e sagittale tramite algoritmo mpr , utilizzando anche la valutazione dellintensit della captazione metabolica ( suv ) come criterio per definire patologico un reperto . statistica sono stati calcolati il tempo di post - processing e di refertazione . 
per ogni lettore , stata calcolata laccuratezza diagnostica , la sensibilit e la specificit delle letture wb - dwibs , insieme al valore predittivo negativo e positivo ( npv e ppv ) , comparando le letture dei radiologi con quella del medico nucleare eseguita sulle immagini tc - pet . risultati la tecnica wb - dwibs ha comportato un tempo di occupazione della sala rm di circa 20 minuti . 
il tempo di refertazione medio risultato di 20 minuti ( range 1525 minuti ) per il primo lettore e 18 minuti per il secondo ( range 1322 minuti )  . 
il tempo di refertazione ha avuto un trend decrescente per ognuno dei radiologi dal primo paziente fino al ventinovesimo . laccordo tra i due lettori stato quasi perfetto , con un valore di di 0 , 93 . 
i due radiologi , su 29 pazienti ( ognuno analizzato nelle 40 sedi anatomiche ) hanno considerato positive ( affette ) rispettivamente 124 e 128 sedi , delle quali 106 e 104 veri positivi ( vp ) , 18 e 14 falsi positivi ( fp ) , contro il rilievo ct - pet di positivit in 119 sedi . sono state considerate negative dai due radiologi 1196 e 1202 sedi , delle quali rispettivamente 1183 e 1187 veri negativi ( vn ) e 13 e 15 falsi negativi ( fn ) , rispetto alle 1121 sedi considerate negative dalla metodica di riferimento ( tabella 4 )  . 
quattordici dei 29 pazienti hanno avuto un responso esattamente speculare a quello della tc - pet . negli altri 15 pazienti si verificato un mismatch di lettura ( fp e fn ) da 1 a massimo 5 sedi . 
i due radiologi hanno avuto rispettivamente : il primo radiologo una sensibilit del 89 , 07% , specificit del 98 , 5% e accuratezza del 97 , 65% , con vpp e vpn di 85 , 48% e 98 , 91% ; il secondo radiologo una sensibilit del 87 , 39% , specificit del 98 , 39% e accuratezza diagnostica del 97 , 8% , con vpp del 88 , 13% e vpn del 98 , 75% . analizzando le discrepanze tra tc - pet e wb - dwibs , abbiamo rilevato rispettivamente per i due radiologi 18 e 14 falsi positivi , 13 e 15 falsi negativi , distribuiti come evidente nella tabella 5 , dove stata riportata la media tra i due radiol med ( 2009 ) 114 : 117 table 3 categorisation of skeletal and visceral sites used in the radiology report skeletal sites visceral sites skull , orbit and maxillary bones cervical spine thoracic spine lumbar spine sacrum coccyx sternum clavicle scapula humerus forearm ilium - ischium femur lower leg cranio , orbite e massiccio colonna cervicale colonna toracica colonna lombare sacro coccige sterno coste clavicola scapola omero avambraccio ilio - ischio femore arto inferiore neck neck nodes lung mediastinum pleura thoracic nodes breast axillary nodes liver adrenal glands kidneys pancreas spleen gallbladder bladder abdominal nodes retrocrural nodes female pelvis reproductive apparatus male pelvis reproductive apparatus omental / peritoneal pelvic nodes inguinal nodes soft tissues collo linfonodi del collo polmone mediastino pleura linfonodi toracici mammella linfonodi ascellari fegato surreni reni pancreas milza intestino colecisti vescica linfonodi addominali linfonodi retrocrurali pelvi femminile apparato riproduttivo pelvi maschile apparato riproduttivo omento peritoneo linfonodi pelvici linfonodi inguinali tessuti molli tabella 3 elenco delle sedi scheletriche e viscerali adottato per la scheda di lettura sedi scheletriche sedi parenchimali time of approximately 20 mpostprocessing had a mean duration of 15 min ( range 1017 min )  . 
of these sites , 106 and 104 were true positive ( tp ) and 18 and 14 were false positive ( fp ) compared with positive pet - ct findings in 119 sites . 
readers rated 1 , 196 and 1 , 202 sites , respectively , as negative , of which 1 , 183 and 1 , 187 were true negatives ( tn ) and 13 and 15 were false negatives ( fn ) compared with negative pet - ct findings in 1 , 121 sites ( table 4 )  . dallaltra parte , nelle sedi addominali e pelviche , appaiono pi concentrati i reperti di falsa positivit . 
un caso di non completa corrispondenza tra le tc - pet e wb - dwibs , quello di un paziente ( p.l. ) , affetto da sarcoma della coscia , trattato chirurgicamente e poi con chemioterapia . 
i numeri rappresntano la media tra i due lettori distribution of results distribuzione dei risultati false negative falsi negativi skull , orbit and maxillary bones sacrum sternum scapula ilium - ischium lung mediastinum thoracic nodes pancreas retrocrural nodes total thoracic spine scapula femur neck neck nodes breast axillary nodes liver adrenal glands kidneys omental / peritoneal pelvic nodes inguinal nodes soft tissues total cranio , orbite e massiccio sacro sterno scapola ileo - ischio polmone mediastino linfonodi toracici pancreas linfonodi retrocrurali totale colonna dorsale scapola femore collo linfonodi del collo mammella linfonodi ascellari fegato surreni reni omento / peritoneo linfonodi pelvici linfonodi inguinali tessuti molli totale false positive falsi positivi there was a perfect match with the pet - ct findings in 14 / 29 patients ; there was some mismatch , ranging from one site ( fp or fn ) to five sites in the same patient in the remaining 15 / 29 patients . 
 with regard to the sites of disagreement between petct and whole - body dwibs , the two readers provided 18 and 14 false - positive results and 13 and 15 false - negative results , distributed as seen in table 5 , which shows the mean between the two readers . 
table 5 shows that the spine was almost free of fp and fn results , whereas the lung - mediastinum and the skull - maxillary bones recorded more fn results than all the other areas taken as a whole . 
colour multiplanar reformation ( mpr ) fusion of pet and ct data ( a , b )  . single pet and ct axial images before coregistration and fusion ( c , d )  . 
1a - d paziente affetto da sarcoma alla coscia destra , trattato con chirurgia e chemioterapia , attualmente con riscontro di metastasi allilo sinistro e ai polmoni ( frecce ) , oltre a recidiva alla coscia controlaterale ( punta di freccia ) ; a , b fusione a colori mediante algoritmo mpr tra pet e tc ; c , d immagini assiali singole di pet e tc prima della co - registrazione e fusione . 
si notino le calcificazioni lesionali a livello dellilo polmonare ( c ) e del nodulo polmonare ( d )  . thigh sarcoma mismatch between pet - ct findings and dwibs refers to a previous treated with surgery and chemotherapy . 
nella stessa figura , si pu osservare un fp ( a livello renale ) con un mancato riconoscimento della lesione peri - cefalopancreatica , verosimilmente linfonodale ( falso negativo )  . discussione limaging rm a diffusione ( dwi ) , stato inizialmente introdotto nella pratica clinica in ambito neuroradiologico , principalmente per la valutazione dello stroke ischemico . solo recentemente il dwi stato esteso ad applicazioni rm in ambito body [ 11 ] anche per le problematiche tecniche intrinseche al distretto toraco - addominale : movimento , numerosit di interfacce tissutali , contenuto intestinale , contenuto gassoso . 
con il miglioramento tecnologico delle apparecchiature rm , con sequenze sempre pi veloci che hanno permesso lacquisizione delle immagini in respiro libero , la rm body e la diffusione a rm nello stesso ambito , sono divenute tecnicamente fattibili . 
alcuni autori [ 15 ] , inoltre , hanno dimostrato la possibilit di caratterizzare le radiol med ( 2009 ) 114 : 117 b = 500 b = 1000 fig . 
diffusion - weighted imaging with optimised background suppression pulse sequence ( dwibs ) coronal ( a ) , sagittal ( b ) and axial multiplanar reformation ( mpr ) images ( c ) at b = 1 , 000 did not confirm the pet - ct findings ( dotted circles )  . 
dwibs elaborata con mpr in coronale ( a ) , sagittale ( b ) e mpr ( c ) a b = 1000 , senza conferma dei reperti osservati in tac - pet ( circoli punteggiati )  . 
6. the same figure shows an fp result ( kidney ) and a missed , probably nodal , pericephalopancreatic lesion . discussion dwi was originally introduced into clinical practice for neuroimaging purposes and mainly for assessing stroke . lesioni maligne , in ambito body , mediante lo studio della diffusione e la misurazione quantitativa con roi posizionate su mappe adc . 
 [ 12 ] che hanno utilizzato una sequenza echo - planar single - shot accoppiata ad un impulso stir , denominata dwibs : questa sequenza ha permesso una maggiore e pi omogenea soppressione del segnale di fondo e lacquisizione con la tecnica del respiro libero , garantendo cos la possibilit di un tempo di acquisizione pi lungo e per questo con un numero maggiore di radiol med ( 2009 ) 114 : 117 fig . 
3 tac - pet : metastasi ossee diffuse ( frecce ) da primitivo ignoto . only recently has its use been extended to whole - body mr applications [ 11 ] owing to technical problems intrinsic to the thoracoabdominal area , including movement , number of tissue interfaces , bowel content and air content . 
dwi with quantitative measurement of apparent diffusion coefficient ( adc ) has been shown to be able to characterise malignant lesions in whole - body imaging [ 15 ]  . 
more recently , dwi has been improved by the introduction of dwibs , a diffusionweighted pulse sequence paired with a stir sequence [ 11 ]  . this sequence allowed greater homogeneous suppression of the background signal as well as acquisition during free breathing , thus permitting more time for the acquisition , a higher number of signal averages , a better signal - to - noise ratio ( snr ) and acquisition of thinner slices . 
the better fat suppression at the edges of the field of view ( fov ) provided by the stir sequence and the acquisition of thinner slices also allow for better mpr and mip reformamedie del campionamento del segnale , con conseguente incremento del snr e con la possibilit di acquisire sezioni pi sottili . 
in questo modo possibile ottenere migliori immagini mip e mpr , sia per le sezioni pi sottili , sia per la migliore soppressione del grasso ai margini del campo di vista indotta dallimpulso stir . 
in questi ultimi anni , la rm whole body diventata pi accessibile e tecnicamente realizzabile grazie allintroduzione commerciale della tecnologia del tavolo mobile , che insieme anche alla disponibilit del software di fusione di pi pacchetti di acquisizione in ununica immagine , ha permesso lacquisizione e la ricostruzione di immagini whole body . 
questi progressi tecnici sono stati preliminari allintroduzione della tecnica wb - dwibs , nel 2004 . ad oggi , nessuno ha comparato i risultati di questa tecnica con le metodiche di medicina nucleare come la tcpet e la scintigrafia ossea , in pazienti oncologici . 
abbiamo condotto questo studio per comparare la wb - dwibs con la tc - pet , attualmente considerata il gold standard nello staging tnm della patologia neoplastica maligna [ 16 ]  . alcune problematiche relative allimaging wb - dwi , radiol med ( 2009 ) 114 : 117 fig . 
in recent years , whole - body mri has become more accessible and easier to perform , thanks to the advent of rolling or moving table technology that , together with the availability of software allowing the fusion of multiple stacks , has made possible the acquisition and reconstruction of whole - body images . 
all these technical advances paved the way for the introduction of the whole - body dwibs technique in 2004 . to our knowledge , no published study has compared the results of whole - body dw - mri with whole - body nuclear imaging techniques ( pet - ct and bone scan ) in cancer patients . 
this study was thus conducted to compare wholebody dwibs and pet - ct , which is considered the standard of reference in the tumour - node - metastasis ( tnm ) staging system for malignancies [ 16 ]  . limitations of whole - body dwi are the huge amount of data to be postprocessed and interpreted . 
in this study , we had a mean postprocessing time of 15 min , mainly spent for window adjustments before completing image fusion and possono essere sicuramente considerate la notevole quantit di immagini da ri - elaborare nel post - processing e da interpretare . 
nel nostro studio , abbiamo riscontrato un tempo di ri - elaborazione delle immagini piuttosto lungo , circa 15 minuti , prevalentemente spesi nellottimizzazione delle finestre di visualizzazione , prima della fusione dei pacchetti e nella generazione delle ricostruzioni mip e mpr . 
il tempo di lettura medio risultato di 19 minuti , come media tra i due lettori ; le letture sono state molto concordanti e questo garantisce la riproducibilit del risultato , in quanto sembra che le immagini siano facilmente interpretate nello stesso modo da differenti lettori . i nostri risultati dimostrano che la wb - dwibs ha alta specificit ed accuratezza diagnostica ed un elevato valore predittivo negativo ( npv ) , tutti vicino al 98% , quando paragonata alla tc - pet . 
analizzando i falsi positivi e negativi della nostra casistica , si evidenziano tre macroaree critiche , che necessitano ulteriore approfondimento : la regione cranio - mascellare , la regione toracomediastinica e la regione addomino - pelvica . 
in addition , there was high interobserver agreement between the two readers . our results show that whole - body dwibs has high specificity , high accuracy and high npv ( all close to 98% ) when compared with pet - ct . 
analysing the fp and fn results of whole - body dwibs in our series , we observed three critical sites that require further investigation : the skull - maxillary bones , the lung - mediastinum and the abdominopelvic site . 
in particular , the thorax , one of the most investigated districts in cancer screening or staging , requires further investigation by means of dwi with dedicated multichannel coils and a specific pulse protocol . 
specifically , the spine was well assessed , with no fn findings , and only one fp result out of 18 tp results ( table 5 )  . sono responsabili della maggioranza dei fn e fp della nostra casistica . 
in particolare , il torace , che uno dei distretti pi esplorati per screening o staging oncologico , necessita un approfondimento ulteriore , con imaging di diffusione mediante bobine multicanale specifiche ed un protocollo con sequenza ottimizzata per la sua valutazione . invece la tecnica appare estremamente accurata nel riconoscimento di lesioni ossee del rachide e delle ossa lunghe , del cranio e del bacino , e per il rilievo di patologia linfonodale . 
nello specifico , la valutazione della colonna vertebrale appare beneficiare , senza falsi negativi e con un solo falso positivo ( tabella 5 ) su 18 rilievi patologici , delle potenzialit diagnostiche di questa nuova tecnica . 
in a e b si osservano multipli foci di alterazione del segnale a livello latero - cervicale bilaterale , a livello splenico , lomboaortico , pelvico e inguinale sinistro ( freccie nere )  . 
con le punte di freccia si osservano due foci segnalati da entrambi i radiologi a livello renale , dei quali ( a destra , punta di freccia rossa ) uno una localizzazione peri - cefalopancreatica ( errore di sede ) e uno ( a sinistra , punta di freccia verde ) un falso positivo non corrispondente a patologia . 
conferma nelle immagini tc - pet in assiale delle lesioni osservate sia in wb - dwibs che nella ricostruzione tc - pet con mpr in coronale , delle lesioni laterocervicali ( e - g , frecce tratteggiate ) , spleniche ( h - l , frecce intere ) , lombo - aortiche ( m - o , punte di freccia )  . radiol med ( 2009 ) 114 : 117 these preliminary data show that the two major clinical applications could be ( a ) bone lesion detection , and specifically screening or staging of the spine - bony pelvis , and ( b ) lymphoma staging , due to the accurate delineation of nodal disease . 
we will direct our future scientific efforts in these two directions . these data , to be confirmed on a larger number of patients , appear to point to a role for whole - body dwibs in cancer screening , staging , restaging and follow - up , given that the higher the specificity and npv , the better the technique as a screening tool . 
whole - body mri has been shown to be more accurate than pet - ct in evaluating the liver , bone and central nervous system [ 17 , 18 ]  . 
from this point of view , a comparison with pet - ct cannot substitute a comparison based on clinical and pathological follow - up or autopsic confirmation ( the true gold standard ) and , in this sense , our study is limited by a certain degree of bias . 
thus , in presenting our preliminary data , we refer to previous studies in which a direct comparison was made between mri and nuclear medicine . the main limitations of the present study inherent to its pilot nature are a heterogeneous case series , the presence of diffuse disease and the small sample size . 
even though wholebody dwibs is beginning to be used in clinical practice , the standard diagnostic workup of patients enrolled in the study was not modified on the basis of the findings of whole - body dwibs because of the lack of scientific validation . direzioni condurremo i nostri prossimi studi . 
 questi risultati , da confermare su una popolazione di pazienti pi ampia , sembrano indicare un ruolo della wbdwibs nello screening , stadiazione , ristadiazione e followup della malattia tumorale ; infatti , pi alta la specificit e il npv , migliore la tecnica per lo screening . 
osserviamo inoltre che la sensibilit non cos elevata ( < 90% ) come la specificit , sempre in riferimento alla tc - pet . la tc - pet ha comunque le sue limitazioni specifiche , in particolare riguardo ai falsi positivi [ 17 ] , che possono influenzare anche il calcolo dellaccuratezza diagnostica delle tecniche di imaging messe a confronto , e in particolare la sensibilit della wb - dwibs nel nostro studio . 
in molte forme tumorali , la tc - pet pi adatta nella individuazione del tumore ( parametro t ) e nello staging linfonodale ( parametro n ) , ma ci sono alcune forme neoplastiche che hanno scarsa captazione di fdg , come il carcinoma renale o i tumori con frequente diffusione alle ossa , al fegato e al cervello ( come il carcinoma della mammella ) , che sono pi idonei a essere studiati con metodiche whole body alternative : infatti gi stato dimostrato che la rm whole body convenzionale pi accurata della tc - pet nella valutazione del fegato , dellosso e del cervello [ 17 , 18 ]  . 
da questo punto di vista , un confronto con la tc - pet , non pu sostituire un confronto tra una metodica di imaging da validare e il follow - up clinico e patologico o autoptico , che rappresenta il vero gold standard ; pertanto i nostri risultati sono gravati da un certo margine di errore . 
gli autori fanno pertanto riferimento alla letteratura , dove il confronto tra rm e tecniche di medicina nucleare stato pi volte descritto , nel presentare questi dati preliminari . nel nostro studio , anche per le sue caratteristiche di studio pilota , principali bias possono essere considerati la casistica eterogenea , la presenza di patologia neoplastica diffusa e il campione di piccole dimensioni : attualmente stiamo estendendo lo studio ad un campione pi omogeneo , introducendo anche il follow - up clinico - patologico come standard di riferimento . 
parisi1 1department of radiation oncology , scientific institute hospital casa sollievo della sofferenza , san giovanni rotondo , 71013 foggia , italy 2university of bari , department of radiology , bari , italy 3university of foggia , department of radiology , scientific institute hospital casa sollievo della sofferenza , san giovanni rotondo , 71013 foggia , italy correspondence to : g . 
a systematic review of external radiation therapy studies in urinary cancers was performed . this synthesis of the literature is based on data from metaanalyses , randomised and prospective trials and retrospective studies . 
there are several reports on multimodality treatment in invasive bladder cancer : intravesical surgery and neoadjuvant chemotherapy to radiotherapy or concomitant radiochemotherapy with organ preservation . the conclusions reached for renal cancer are controversial , and data on cancers of the urethra and ureter are few and inconclusive . 
sufficient data now exist in the literature to demonstrate that conservative management with organ preservation is a valuable alternative to radical cystectomy , the traditional gold standard , in invasive bladder cancer , keywords urinary cancers treatment radiotherapy ( rt ) chemotherapy ( ct ) organ preservation overall survival ( os ) riassunto i tumori invasivi del tratto urinario sono relativamente rari ed il loro trattamento pu causare importanti cambiamenti nelle funzioni sessuali , sociali ed urinarie . 
ci sono pochi studi clinici controllati che hanno utilizzato la radioterapia adiuvante o radicalechemioterapia nei tumori del rene , degli ureteri e delluretra ; ci sono diversi studi sul trattamento multimodale del carcinoma invasivo della vescica : chirurgia intravescicale e chemioterapia neoadiuvante alla radioterapia o radio - chemioterapia concomitante con preservazione dellorgano . 
le conclusioni raggiunte sul carcinoma renale sono controverse ; i dati sul carcinoma degli ureteri e delluretra sono pochi e inconclusivi ; invece , vi sono ora in letteratura dati sufficienti che dimostrano come lapproccio con preservazione dellorgano , per il carcinoma vescicale invasivo rappresenta una valida alternativa alla cistectomia radicale , considerata per lungo tempo il gold standard . parole chiave tumore urinario trattamento radioterapia ( rt ) chemioterapia ( ct ) preservazione dellorgano sopravvivenza globale ( sg ) radiol med ( 2009 ) 114 : 7082 introduction surgery is the primary therapeutic option in the curative treatment of clinically localized urinary cancer . 
preoperative irradiation with doses of 2040 gy has been used to facilitate resection , to sterilise well - oxygenated peripheral extensions of the tumour that might be transected during nephrectomy , and to decrease the chance of dissemination at the time of nephrectomy . 
no advantage has been demonstrated in patients receiving preoperative irradiation with doses of 2040 gy with respect to overall survival ( os ) or survival free from distant metastases ( ffdm ) , although improvement in resectability has been noted [ 16 ]  . 
two studies [ 10 , 12 ] have reported excessive bowel and hepatic complications and an irradiation - related mortality rate of 13%19% , explained in part by the fractionation scheme . 
doses of 4550 gy can be given , with acceptable bowel and hepatic complications ; however , a dose of 50 gy is suggested as being the tolerance limit for the upper abdominal gastrointestinal tract [ 13 ]  . 
a recent study [ 15 ] has shown that 5year disease - free survival ( dfs ) is 66% in the radiotherapy introduzione la chirurgia la principale opzione terapeutica nella cura del tumore dellapparato urinario clinicamente localizzato . ad ogno modo , sebbene questappoccio sia associato ad un eccellente controllo locale , non scevro dal rischio di complicanze e , a volte , di una scarsa qualit di vita . 
nel trattamento del cancro invasivo della vescica come alternativa alla cistectomia radicale immediata si pu utilizzare la resezione la resezione transuretrale , la chemioterapia e la radioterapia con cistectomia di salvataggio . 
la maggior parte dei pazienti trattati con terapia trimodale conserva una buona funzione vescicale . rene la nefrectomia radicale resta la sola terapia efficace per il carcinoma renale ( cr ) clinicamente localizzato . 
la rt pre - operatoria con dosi da 20 a 40 gy stata utilizzata per facilitare la resezione , per sterilizzare i margini periferici ben ossigenati del tumore che potrebbero essere sezionati durante la nefrectomia , e per ridurre la possibilit di disseminazione al momento della nefrectomia . 
nessun vantaggio stato dimostrato nei pazienti sottoposti a rt pre - operatoria con dosi da 20 a 40 gy per ci che riguarda la sopravvivenza globale ( sg ) o sopravvivenza libera da metastasi a distanza ( slmd ) , sebbene sia stato notato un miglioramento della resecabilit [ 16 ]  . 
in studi datati , la radioterapia postoperatoria ha dimostrato un vantaggio di circa il 15% sul controllo locale ( cl ) rispetto alla nefrectomia da sola [ 711 ] , ma con risultati insoddisfacenti sulla sopravvivenza . 
due studi [ 10 , 12 ] hanno riportato eccessive complicanze intestinali ed epatiche , ed una percentuale del 13%19% di mortalit legata alla rt , spiegata in parte dallo schema di frazionamento . 
dosi di 4550 gy possono essere erogate con complicanze intestinali ed epatiche accettabili ; comunque suggerita una dose di 50 gy come limite di tolleranza per il tratto gastrointestinale superiore [ 13 ]  . 
 [ 11 ] lirradiazione post nefrectomia con dose mediana di 46 gy ha ridotto la percentuale di recidive locali nei pazienti con tumore in stadio pt3 dal 37% ( nei pazienti non irradiati ) al 10 % ( nei pazienti irradiati ) ( p = 0 , 05 ) ; ma , in un aggiornamento del radiol med ( 2009 ) 114 : 7082 group and 16% in the no - treatment group and has shown reduction of local recurrence , with a significant difference in both univariate and multivariate analyses , although no benefit was noted in patients with earlier - stage disease . another recent study [ 16 ] concluded that adjuvant rt is unlikely to improve treatment outcome . 
however , these series suggest a benefit in patients with a high risk of local recurrence ( incomplete resection t3 / t4 stage , nodal metastases ) , but there is no advantage for os . 
the authors achieved an overall partial / complete response ( cr ) of 90%98% . this new radiation technique is a big challenge , because the side effects are few , and local control is high due to easy dose escalation . 
complete resection is the only known cure for renal cancer , and the value of rt is controversial . results are awaited of multi - institutional prospective randomised trials using modern rt techniques to evaluate the role of rt and its effect on survival , especially in selected patients with a high risk of local or regional failure . ureter and urethra carcinomas of the ureter and urethra are unusual diseases with insufficient clinical experience , and the role of rt in situ not well defined . 
 [ 20 ] reviewed the records of 31 patients with locally advanced transitional cell carcinoma of the renal pelvis and ureter who underwent surgery followed by adjuvant rt with or without concurrent chemotherapy ( ct ) [ methotrexate , cisplatin ( cddp ) and vinblastine ( mcv ) ]  . five - year os and disease - specific survival ( dss ) with adjuvant concurrent chemoradiotherapy ( ccrt ) ( cddp ) improved in patients with resected , locally advanced uppertract urothelial malignancies . 
 the results of 34 women with primary urethral carcinoma were retrospectively reviewed at princess margaret hospital [ 23 ] .these patients were treated with rt with or lavoro , la rt post - operatoria non ha migliorato la sopravvivenza ed ha mostrato tossicit [ 14 ]  . 
un recente studio [ 15 ] ha mostrato che la sopravvivenza libera da malattia ( slm ) a 5 anni del 66% nel gruppo sottoposto a rt e del 16% nel gruppo non sottoposto a rt ed ha mostrato una riduzione della recidiva locale , con una differenza significativa sia allanalisi univariata che multivariata ; ma non stato notato nessun beneficio nei pazienti in stadio iniziale di malattia . 
comunque , tali lavori hanno suggerito un beneficio nei pazienti ad alto rischio di recidiva ( resezione incompleta negli stadi t3 / t4 , metastasi linfonodali ) , ma nessun vantaggio riguardo alla sg . 
 [ 18 ] riguardo lutilizzo della rt stereotassica extracranica nei tumori renali primitivi e metastatici : gli autori hanno riportato il 90%98% di risposte parziali / complete ; questa nuova tecnica di irradiazione una grande sfida perch gli effetti collaterali sono pochi ed il cl alto , dovuto alla facilit di aumentare la dose erogata . 
attendiamo i risultati di studi prospettici randomizzati multi - istituzionali che utilizzano tecniche moderne di rt per valutare il ruolo ed i suoi effetti sulla sopravvivenza , specialmente in pazienti selezionati con alto rischio di recidiva locale o regionale . 
la sg e la ssm a 5 anni con chemio - rt concomitante e adiuvante ( ccrt ) sono migliorate nei pazienti con neoplasie resecate e localmente avanzate del tratto urinario inferiore . 
i pazienti con malattia avanzata trattati con chirurgia da sola hanno avuto una slm pi breve ( 23 , 3 mesi ) rispetto quelli trattati con combinazione di rt - ct ( 45 , 2 mesi )  . grigsby [ 22 ] ha analizzato i dati di 44 donne con carcinoma delluretra . 
brachytherapy reduced the risk of local recurrence , and the beneficial effect was most prominently seen in patients with bulky primary disease . in the conservative management of these tumours , the combination of external beam brachytherapy with or without ct play a significant role , and the multimodality approach appears to be the optimal way to treat these patients , with surgery to be used for biopsy - proven persistent tumours or recurrence [ 24 ]  . radiotherapy bladder radical cystectomy with bilateral pelvic lymph node dissection followed by urinary diversion remains the gold standard for treating muscle - invading bladder cancer and is the single most successful modality , reporting long - term os in the range of 40%60% [ 2528 ]  . 
rt is utilised as single modality treatment , as neoadjuvant or adjuvant to surgery , or combined with ct with or without conservative local surgery . i risultati di 34 pazienti con carcinoma uretrale sono stati analizzati in modo retrospettivo al princess margaret hospital [ 23 ] , trattati con rtbrachiterapia . 
 nella strategia terapeutica conservativa di questi tumori , la combinazione di rt e brachiterapia con o senza ct , riveste un ruolo significativo e , lapproccio multimodale sembra essere il modo ottimale per trattare questi pazienti , riservando la chirurgia per laccertamento istologico della persistenza o recidiva tumorale [ 24 ]  . vescica la cistectomia radicale con linfadenectomia pelvica bilaterale seguita da diversione urinaria rimane il gold standard per il trattamento del carcinoma della vescica invasivo ed la singola modalit pi vantaggiosa che ha riportato una sg a lungo termine del 40%60% [ 2528 ]  . 
such comparisons were very difficult , because patients selected for radical cystectomy had less advanced tumours at diagnosis , were younger and in a better general condition than patients selected for definitive irradiation . 
results reported in the literature are not significant : the 5 - year survival rate for patients treated with rt alone ( dose of 6066 gy at a 1.8to 2 - gy daily fraction ) is 32% ( range 22%50% ) [ 29 , 30 ]  . 
a recent review of treatment outcomes in rt - treated patients showed the following 5 - year survival rates : t1 , 35%71% ; t2 , 10%59% ; t3 , 10%38% ; and t4 , 0%16% [ 31 ]  . 
tali confronti sono molto difficoltosi perch i pazienti selezionati per la cistectomia radicale avevano tumori in stadio meno avanzato alla diagnosi , erano pi giovani ed in migliori condizioni generali rispetto ai pazienti selezionati per la rt radicale . 
in letteratura i risultati non sono significativi : la sopravvivenza a 5 anni per i pazienti trattati con rt da sola ( dosi di 6066 gy , con 1 , 82 gy come frazione giornaliera ) del 32% ( 22%50% ) [ 29 , 30 ]  . 
una review recente riguardo i risultati della terapia nei pazienti sottoposti a rt , ha mostrato la seguente incidenza di sg a 5 anni : t1 , da 35% a 71% ; t2 , da 10% a 59% ; t3 , da 10% a 38% e t4 da 0% a 16% [ 31 ]  . radioterapia pre - operatoria la pi ampia esperienza ( 338 pazienti ) con rt pre - operatoria ha ottenuto una sotto - stadiazione patologica nel 65% dei pazienti ed una risposta patologica completa nel 42% dei casi . 
la sopravvivenza a 5 anni dei pazienti che hanno ricevuto la rt seguita da cistectomia stata 38% vs radiol med ( 2009 ) 114 : 7082 followed by cystectomy was 38% vs 29% for those treated with rt alone ( not statistically significant )  . 
 strong support for the use of preoperative irradiation in patients with t3b bladder cancer was reported by cole et al . [ 34 ] : the 5 - year local control in the preoperative group was 91% compared with 72% for those treated with radical cystectomy alone . 
however , a meta - analysis of five randomised trials showed no statistical difference in treatment outcomes between patients treated with preoperative rt and cystectomy alone [ 35 ]  . 
 preoperative ccrt showed better results than rt alone . in fact , in the nordic cystectomy trial [ 37 ] , the combination of ct ( adriamycin + cddp for two cycles ) plus rt ( 20 gy in four fractions ) followed by cystectomy showed a 5 - year os improvement of 15% only for t3 - t4 disease compared with rt or surgery alone ( p = 0.03 ) , whereas no survival benefit was found for early stages of disease ( t1t2 )  . 
in the canadian randomised study [ 38 ] , concurrent cisplatin improved pelvic disease control with preoperative 29% per quelli trattati con rt da sola ( non statisticamente significativo , nss )  . 
 [ 34 ] : il cl a 5 anni nel gruppo sottoposto a rt preoperatoria stato del 91% rispetto al 72% per quelli trattati con cistectomia radicale e c stato anche un beneficio in termini di sg e slm ( nss )  . 
comunque , una metanalisi di 5 studi randomizzati non ha mostrato differenze statisticamente significative tra i pazienti trattati con rt pre - operatoria e quelli trattati con cistectomia radicale [ 35 ]  . 
una conclusione simile stata raggiunta in uno studio di fase iii su 140 pazienti , che confronta la chirurgia da sola con chirurgia e rt preoperatoria [ 36 ]  . la ccrt pre - operatoria ha mostrato migliori risultati rispetto alla rt da sola . 
infatti , nello studio nordico sulla cistectomia [ 37 ] la combinazione di ct ( adriamicina + cisplatino per 2 cicli ) pi rt ( 20 gy in 4 frazioni ) seguita da cistectomia ha mostrato un incremento della sg a 5 anni del 15% solo per i t3 - t4 rispetto alla rt o chirurgia da sola ( p = 0 , 03 ) , mentre nessun beneficio di sopravvivenza stato trovato negli stadi iniziali di malattia ( t1t2 )  . 
only one randomised study of radical cystectomy alone vs cystectomy and postoperative rt [ 41 ] reported a 5 - year pelvic recurrence of 5% ( 50% in the cystectomy arm ) and an improvement in dfs in patients with schistosomiasis . 
the main disadvantage of postoperative rt is the high rate ( 20%40% ) of serious late gastrointestinal complications [ 39 , 40 , 4244 ] because of the larger volume of small bowel occupying the pelvis after cystectomy . 
patients at high risk of recurrence are probably better treated with ct , which may prevent local and distant relapse and is usually well tolerated . bladder - preservation therapy the relative negative impact on quality of life for urinary diversion and the trend towards organ preservation led many authors to explore the role of conservative management . 
neoadjuvant ct compared with rt or surgery was investigated in an attempt to improve the results of surgery alone or definitive rt maintaining a functioning bladder . in the european organisation for research and treatment of cancer ( eortc ) / medical research council [ 45 ] trial , 976 patients undergoing curative cystectomy or radical rt were randomised to receive three cycles of neoadjuvant ct ( mcv ) in 491 patients or no ct in 485 . 
a recent meta - analysis [ 46 ] confirmed that neoadjuvant platinum - based combination ct reduces mortality risk of 13% , with moderate improvement ( 5% , p = 0.016 ) of 5 - year os , irrespective of the type of local treatment ( surgery or rt alone or rt and cystectomy ) and without differences between subgroups of patients . 
there was no evidence to support the use of single - agent platinum . these studies showed that patients treated with rt ( conservative approach ) have preserved bladder function . over the past 1520 years , several prospective trials have investigated conservative therapy in which all patients were treated with transurethral resection of bladder tumours ( turbt ) with or without ct followed by ccrt . 
alcuni studi hanno riportato una riduzione del rischio di recidive pelviche dal 30% al 50% al 10% al 20% [ 3941 ] , ma alcuni pazienti hanno anche ricevuto rt pre - operatoria . 
solo uno studio randomizzato sulla cistectomia radicale da sola verso cistectomia e rt postoperatoria [ 41 ] , ha riportato recidive pelviche a 5 anni del 5% ( 50% nel braccio della cistectomia ) ed un incremento della slm nei pazienti con schistosomiasi . 
il principale svantaggio della rt post - operatoria lalta percentuale ( 20%40% ) di gravi complicanze gastrointestinali tardive [ 39 , 40 , 4244 ] , poich una gran parte di volume dellintestino tenue occupa la pelvi dopo cistectomia . 
i pazienti ad alto rischio di recidiva sono probabilmente trattati in modo migliore con la ct , che pu prevenire recidive locali e a distanza ed di solito ben tollerata . 
 terapia di preservazione della vescica il relativo impatto negativo sulla qualit della vita per la diversione urinaria e la tendenza verso la preservazione dellorgano , ha permesso a molti autori di esplorare il ruolo di un trattamento conservativo . 
 nello studio delleortc ( european organisation for research and treatment of cancer ) / medical research council [ 45 ] , 976 pazienti sottoposti a cistectomia curativa o rt radicale sono stati randomizzati a ricevere 3 cicli di ct neoadiuvante ( mcv , metotressato , cddp , vinblastina ) in 491 pazienti , oppure nessuna ct in 485 pazienti . 
la differenza assoluta tra i gruppi per quanto riguarda la sg a 3 anni del 5 , 5% ( 55 , 5% per ct vs 50% nessuna ct ) non risultata statisticamente significativa ( p = 0 , 075 ) : la ct neoadiuvante stata associata con una patologica completa pi alta , ma non c stato nessuna chiara evidenza sulla sopravvivenza . 
una recente metanalisi [ 46 ] ha confermato che la combinazione di ct neoadiuvante a base di platino riduce il rischio di mortalit del 13% , con un incremento moderato ( 5% , p = 0 , 016 ) della sg a 5 anni , indipendentemente dal tipo di trattamento locale ( chirurgia o rt da sola o rt e cistectomia ) , e senza differenze tra i sottogruppi di pazienti , non vi stata alcuna evidenza a favore di platino da solo . 
 negli ultimi 1520 anni , diversi studi prospettici hanno analizzato terapie conservative in tutti quei pazienti trattati radiol med ( 2009 ) 114 : 7082 patients with cr , a consolidation rt or ccrt regimen was administered . 
 since 1985 , radiation therapy oncology group ( rtog ) trials have used a trimodality conservative treatment ( turbt , rt , ct ) in patients with t2t4a muscleinvasive bladder cancer who were candidates for cystectomy . 
in three rtog trials [ 4749 ] , patients were treated with neoadjuvant turbt and ccrt ( conventional or altered fractionation ) , whereas in two trials [ 50 , 51 ] , patients were treated with induction by turbt with or without ct and ccrt . 
cystectomy was reserved for incompletely responders or relapse . in the rtog 89 - 03 phase iii study , the combination of neoadjuvant ct ( mcv2 cycles ) with ccrt with cddp failed to show significant benefits in terms of 5 - year local control ( 61% vs 49% ) , os ( 48% vs 49% ) and ffdm ( 33% vs 39% ) compared with ccrt alone , with more toxicity in the mcv arm [ 51 ]  . 
in fact , subsequent studies by the rtog emphasised the impact of adjuvant ct [ mcv or cddp + 5fluorouracil ( fu ) ] following rt ( hypoor hyperfractionated ) [ 49 ] , with good results at 3 years . 
from paris began a prospective trial of preoperative ct using 5 - fu and cddp with concomitant rt ( 3 gy b.i.d. , total dose 24 gy ) , followed by either cystectomy or additional ccrt . 
this treatment strategy resulted in a pathological cr of 77% and may be proposed as conservative treatment in patients with a cr to the initial course of chemoradiation [ 54 ]  . 
globally , os at 5 years was 51% . similar results were obtained in further series of combined modality treatment for bladder preservation with excellent cr ( ~70% ) , and 5 - year os ( ~50% ) , with bladder con resezione transuretrale della vescica ( turbt ) ct seguita da ccrt , e per i pazienti con risposta completa stata somministrata una rt di consolidamento o ccrt ; la cistectomia stata riservata per le risposte incomplete o per le recidive di malattia . 
 dal 1985 , gli studi dellrtog ( radiation therapy oncology group ) hanno utilizzato un trattamento conservativo trimodale ( turbt , rt , ct ) nei pazienti con carcinoma della vescica t2t4a , che erano candidati alla cistectomia . in tre studi dellrtog [ 4749 ] i pazienti sono stati trattati con turbt neoadiuvante e ccrt ( convenzionale o frazionamenti alterati ) ; mentre in 2 studi [ 50 , 51 ] i pazienti sono stati trattati con induzione mediante turbtct e ccrt ; la cistectomia stata riservata per le risposte incomplete o in caso di recidive . 
 nello studio di fase iii dellrtog 89 - 03 , la combinazione di ct neoadiuvante ( mcv2 cicli ) con ccrt mediante cddp non ha mostrato alcun beneficio significativo in termini di cl a 5 anni ( 61% vs 49% ) , sg ( 48% vs 49% ) e slm ( 33% vs 39% ) , rispetto alla ccrt da sola , con una maggiore tossicit nel braccio che ha usato lmcv [ 51 ]  . 
infatti gli studi successivi dellrtog hanno puntualizzato limpatto della ct adiuvante ( mcv o cddp + 5 - fu ) alla rt ( ipoo iper - frazionamenti ) [ 49 ] , con buoni risultati a 3 anni . 
 [ 54 ] di parigi , hanno iniziato uno studio prospettico di ct preoperatoria usando 5 - fu e cddp con rt concomitante ( 3 gy bid , dose totale di 24 gy ) , seguita sia da cistectomia o ccrt addizionale . 
questa strategia di trattamento ha determinato una risposta patologica completa nel 77% dei casi , e pu essere proposta come terapia conservativa nei pazienti con risposta completa al ciclo iniziale di ccrt [ 54 ]  . 
 [ 55 ] , nella quale 415 pazienti sono stati trattati dopo la turbt con rt da sola ( 126 pazienti ) o in concomitanza con cddp ( 240 pazienti ) o cddp + 5 - fu ( 49 pazienti ) , con percentuali di risposte complete migliori per rt + cddp - 5 - fu ( 87% ) rispetto al cddp ( 66% ) o rt da sola ( 61% ) ; globalmente , la sg a 5 anni risultata pare a 51% . risultati simili sono stati ottenuti in ulteriori studi con modalit di trattamento combinato per la conservazione della vescica , con eccellenti risposte complete ( ~70% ) , ed una sg a 5 anni ( ~50% ) , con conservazione dellorgano in radiol med ( 2009 ) 114 : 7082 table 1 series of combined modality treatment for bladder preservation series no . 
 [ 70 ] turbt 24 gy at 3 gy + cddp / fu 2 additional cycles of crt ( dose not given ) ( specific cancer ) ng ( overall rate of cystectomy : 25.6% ) danesi et al . 
table 1 summarises the results of these studies [ 5674 ]  . in a recent meta - analysis of fifteen radiation series with different fractionation schedules and total doses , pos et al . [ 75 ] found evidence for an overall doseresponse relationship with an increase in local control by a factor of 1.441.47 for an increment in dose of 10 gy . 
 [ 71 ] recently reported the long - term results of a phase i / ii trial of ct ( mcv ) followed by concomitant cddp + 5 - fu and hyperfractionated irradiation ( three 100cgy fractions / day , for a total dose of 69 gy )  . 
accelerated rt may overcome radioresistance due to tumour - cell repopulation , but a recent randomised trial [ 77 ] reported no improvement of local control or survival rates and increased acute bowel complications . 
there has been only one small phase iii study of curative rt in which survival was inferior in the hypofractionated arm [ 78 ]  . some trials , in an attempt to improve results , explore the use of new chemotherapeutic agents and accelerated or hyperfractionated rt to increase irradiation dose in combination with ct . 
new chemotherapeutic agents , in particular gemcitabine and taxanes , are effective in combination with cddp and rt ( paclitaxel and gemcitabine are good radiosensitisers ) [ 61 , 79 ]  . 
a recent italian study [ 68 ] reported the feasibility of a combined scheme with gemcitabine ( up to 400 mg / m2 ) plus cddp and rt , obtaining 100% cr . 
finally , the rtog 99 - 06 trial introduced concomitant paclitaxel + cddp plus bifractionated rt as induction treatment , followed by adjuvant ct ( gemcitabine and cddp ) in patients with cr ; no specific outcomes are yet available [ 80 ]  . 
in una meta - analisi recente su 15 studi di rt con differenti schemi di frazionamento e dose totale , pos et al . [ 75 ] , hanno evidenziato una relazione globale dose - risposta , con incremento del cl , di un fattore che va da 1 , 44 a 1 , 47 per un aumento di dose di 10 gy . 
una meta - analisi di stuschke e thames [ 76 ] ha indicato che i regimi iper - frazionati mostrano un aumento della sg ( odd ratio di mortalit 0 , 55 ; p = 0 , 002 ) ed una risposta completa ( odd ratio di fallimento di 0 , 44 ; p = 0 , 001 )  . 
 [ 71 ] , recentemente hanno riportato risultati a lungo termine di uno studio di fase ii / ii di ct ( mcv ) seguita da ct a base di cddp + 5 - fu concomitante e rt iper - frazionata ( 1 gy per 3 frazioni al giorno , per una dose totale di 69 gy )  . 
le percentuali a 5 anni di sg , conservazione della vescica , ssm , slm e sopravvivenza senza cistectomia per tutti e 77 i pazienti sono state 58 , 8% , 46 , 6% , 75% , 53 , 5% e 76 , 1% , rispettivamente . 
la rt accelerata pu superare la radioresistenza generata dal ripopolamento delle cellule tumorali , ma in uno studio recente randomizzato [ 77 ] , non riportato alcun incremento delle percentuali del lc o della sg ma sono aumentate le complicanze intestinali acute . 
 alcuni studi , nel tentativo di migliorare i risultati , hanno esplorato luso di nuovi agenti chemioterapici e rt accelerata o iper - frazionata per aumentare la dose di rt in associazione con la ct . 
nuovi agenti chemioterapici , in particolare gemcitabina e taxani , sono efficaci in combinazione con cddp e rt ( paclitaxel e gemcitabina sono buoni radiosensibilizzanti ) [ 61 , 79 ]  . 
un recente studio italiano [ 68 ] , ha riportato la fattibilit di uno schema combinato con gemcitabina ( fino 400 mg / m2 ) pi cddp e rt , ottenendo il 100% di risposta completa . 
infine , lrtog 99 - 06 ha introdotto ct concomitante a base di paclitaxel + cddp pi rt bifrazionata come trattamento di induzione , seguito da ct adiuvante ( gemcitabina e cddp ) nei pazienti con risposta completa ; risultati specifici non sono ancora disponibili [ 80 ]  . conclusions conclusioni radical nephrectomy is the only effective therapy for clinically localised renal cancer . 
la cistectomia di salvataggio usata in caso di risposta parziale dopo terapia di induzione ccrt ( rtog ) o recidiva radiol med ( 2009 ) 114 : 7082 response after induction ccrt treatment ( rtog ) or recurrent disease ( european trials ) : in both cases , surgery can be curative , reporting a 5 - year survival of approximately 50% [ 45 , 50 , 51 , 54 , 55 ]  . 
 trimodality treatment ( turbt , rt , ct ) of invasive bladder cancer may be offered as a valid alternative to radical cystectomy , with no decrease in survival related to the delay in cystectomy , which is currently the gold standard therapy . 
os is comparable with recent surgical data , reporting a 5 - year os of almost 50% , with bladder preservation in three fourths of these patients . di malattia ( studi europei ) : in entrambi i casi la chirurgia pu essere curativa , riportando una sopravvivenza a 5 anni del 50% approssimativamente [ 45 , 50 , 51 , 54 , 55 ]  . 
 il trattamento trimodale ( turbt , rt , ct ) del carcinoma invasivo della vescica pu offrire una valida alternativa alla cistectomia radicale con nessuna diminuzione della sopravvivenza correlata al ritardo della cistectomia , che rimane attualmente la terapia gold standard . 
complete tumour necrosis , confirmed by targeted biopsy , was observed in patients showing no intralesional flow signals and time - intensity curves with low peak of signal intensity and absence of plateau after treatment . 
dopo il trattamento , nei pazienti che presentavano assenza di segnali vascolari intralesionali , curve con basso picco di intensit e assenza di plateau , la biopsia mirata confermava la necrosi completa . 
in base ai risultati ottenuti , le curve con elevato picco di intensit e presenza di plateau , potrebbero rappresentare pattern del tessuto neoplastico intra o perilesionale e fornire quindi importanti informazioni sullefficacia del trattamento . radiol med ( 2009 ) 114 : 3241 keywords power doppler time - intensity curves contrast material focal hepatic lesions hepatocellular carcinoma metastasis parole chiave power doppler curve dintensit - tempo mezzi di contrasto lesioni focali epatiche carcinoma epatocellulare metastasi introduction introduzione in recent years , several nonoperative techniques have been used successfully in the locoregional treatment of hepatocellular carcinoma and metastases , including percutaneous ethanol transcatheter arterial chemoembolisation ( tace ) [ 35 ] , and radiofrequency ablation ( rfa ) [ 69 ]  . injection ( pei ) [ 1 , 2 ] , the follow - up of patients undergoing these treatments is generally based on imaging studies such as magnetic resonance imaging ( mri ) [ 10 , 11 ] or computed tomography ( ct ) [ 12 ] , with only few doubtful cases being studied by biopsy to assess whether complete necrosis of the neoplastic tissue has been achieved . contrast - enhanced colour doppler ultrasound ( cdus ) , thanks to its high sensitivity in detecting weak intratumoural flow signals , has been employed for several years in the differential diagnosis of focal hepatic lesions [ 1315 ]  . recently , it has also been used for the follow - up of intralesional therapy [ 1619 ] , to identify residual areas of intratumoural enhancement that could reflect incomplete necrosis or disease recurrence . 
a study of intralesional and perilesional vascularity with analysis of time - signal intensity curves performed immediately after treatment may help to ascertain whether certain flow signals reflect incomplete treatment . 
the use of contrast - enhanced power doppler us ( pdus ) with timeintensity curves in liver diseases [ 2023 ] , as in focal breast lesions [ 24 ] , may also provide valuable information on the persistence of neoplastic perilesional vascularity and consequently on incomplete necrosis . 
the purpose of this study was to assess the utility of pdus with analysis of time - intensity curves in monitoring focal hepatic lesions ( metastases , hepatocellular carcinoma ) treated with pei or rfa and to correlate the findings with the results of targeted biopsy . materials and methods twenty patients ( twelve men and six women ; age range 55 to 72 years ) with hepatocellular carcinoma and solitary metastases of the liver previously diagnosed by other methods ( ct , mri , biopsy ) underwent intralesional therapy with pei or rfa . 
all patients were studied negli ultimi anni sono state utilizzate diverse tecniche non chirurgiche per il trattamento loco - regionale dellepatocarcinoma e delle metastasi , alcune di queste , molto efficaci come lalcoolizzazione percutanea ( pei ) [ 1 , 2 ] , la chemioembolizzazione ( tace ) [ 35 ] e la radioipertermia ( rfta ) [ 69 ]  . il follow - up dei pazienti sottoposti a questi trattamenti generalmente affidato a metodiche di diagnostica per immagini come la rm [ 10 , 11 ] o la tc [ 12 ] ; solo in alcuni casi dubbi si ricorre alla biopsia per verificare leffettiva necrosi completa del tessuto neoplastico . 
 il color doppler con mdc , grazie allelevata sensibilit nel rilevare i deboli segnali vascolari intralesionali una metodica gi da qualche anno utilizzata per la diagnosi differenziale delle lesioni focali epatiche [ 1315 ] , ed stata gi utilizzata anche per il follow - up dopo la terapia intralesionale [ 1619 ]  . 
spesso subito dopo il trattamento il color doppler con mdc evidenzia una ricca vascolarizzazione perilesionale la cui natura non pu essere determinata se non con la biopsia ; quindi lo studio della vascolarizzazione intra e perilesionale con le curve intensit / tempo , subito dopo il trattamento , potrebbe essere utile poich alcuni segnali vascolari potrebbero essere indice di incompleto trattamento . 
lutilizzo del power doppler con mdc con la determinazione delle curve intensit / tempo nelle malattie del fegato [ 2023 ] o come nel caso delle lesioni focali della mammella [ 24 ] , potrebbe fornire , a nostro giudizio , informazioni preziose anche circa la persistenza di vascolarizzazione neoplastica perilesionale dopo il trattamento e quindi incompleta necrosi della lesione . 
obiettivo di questo lavoro quindi lutilizzo del power doppler con le curve intensit / tempo nel monitoraggio delle lesioni focali epatiche ( metastasi , epatocarcinoma ) sottoposte al trattamento intralesionale con pei e rfta confrontando i risultati con la biopsia mirata . materiali e metodi venti pazienti , dodici maschi e sei femmine , con et compresa tra 55 e 72 anni , affetti da epatocarcinoma e radiol med ( 2009 ) 114 : 3241 by pdus with analysis of time - intensity curves one day before and one day after treatment , followed by targeted biopsy two days later . 
subjects in the control group were imaged by pdus with analysis of time - intensity curves . the us studies were performed on an au cinque idea device ( esaote , genoa , italy ) with a 3.5 mhz convex - array probe . 
in patients the time - intensity curves were derived from a circular region of interest ( roi ) placed over the lesion and large enough to encompass both the intralesional and perilesional vessels . 
il giorno prima e il giorno dopo il trattamento , tutti i pazienti sono stati studiati con esame power doppler con determinazione delle curve intensit / tempo e successivamente , 2 giorni dopo il trattamento , sottoposti a biopsia mirata . 
i pazienti del gruppo di controllo sono stati sottoposti ad esame power doppler con curve intensit / tempo . per lindagine ecografica stato utilizzato un apparecchio au cinque idea ( esaote , genova ) con sonda convex da 3 , 5 mhz . 
nei pazienti patologici la curva intensit / tempo stata ottenuta utilizzando una roi circolare posizionata sulla lesione in modo da comprendere sia la vascolarizzazione intra che perilesionale a tale scopo stato fatto coincidere il diametro della roi con il diametro massimo ottenuto comprendendo la lesione e la vascolarizzazione perilesionale . 
nei pazienti del gruppo di controllo stata utilizzata su tutti i pazienti una roi circolare del diametro di un centimetro posizionata in unarea del parenchima del lobo destro del fegato . 
b the corresponding time - intensity curve shows an elevated peak of signal intensity ( arrowhead ) related to a high concentration of contrast agent and a plateau phase ( arrow ) due to the retention of contrast material within the lesion . 
b la curva intensit / tempo prima del trattamento mostra il raggiungimento di un elevato picco di intensit ( testa di freccia ) , che corrisponde ad unelevata concentrazione di mdc e la presenza di plateau ( freccia ) , dovuti ad una lunga permanenza del mdc nella lesione . 
b the corresponding time - intensity curve shows an elevated peak of intensity ( arrow ) due to high concentration of contrast material and plateaus ( arrow heads ) due to retention of the contrast material in the lesion . 
b la curva intensit / tempo prima del trattamento mostra il raggiungimento di un elevato picco di intensit ( freccia ) , che corrisponde ad unelevata concentrazione di mdc e la presenza di plateau ( teste di freccia ) , dovuti ad una prolungata permanenza del mdc nella lesione . 
b the corresponding time - intensity curve shows an elevated peak of intensity ( arrow ) related to the high concentration of contrast agent and plateaus ( arrowheads ) due to retention of the contrast material within the lesion . 
b la curva intensit / tempo eseguita subito dopo il trattamento mostra il raggiungimento di un elevato picco di intensit ( freccia ) che corrisponde ad unelevata concentrazione di mdc e la presenza di plateau ( teste di freccia ) , dovuto ad una prolungata permanenza del mdc nella lesione . 
b the corresponding time - intensity curve shows an elevated peak of signal intensity ( arrowhead ) related to the high concentration of contrast agent and a plateau phase ( arrow ) due to retention of the contrast in the lesion . 
b la curva intensit / tempo prima del trattamento mostra il raggiungimento di un elevato picco di intensit ( freccia ) , che corrisponde ad unelevata concentrazione di mdc e la presenza di un plateau ( testa di freccia ) , dovuto ad una lunga permanenza del mdc nella lesione . 
d la curva intensit / tempo eseguita subito dopo il trattamento mostra il raggiungimento di un elevato picco di intensit ( testa di freccia ) e la presenza di un plateau ( freccia ) , dovuto ad una prolungata permanenza del mdc nella lesione . in our study , contrast - enhanced pdus performed before treatment revealed intralesional or perilesional flow signals in all patients , so we were able to derive significant time - intensity curves . 
b gruppo di controllo ( paziente sano ) : la curva intensit / tempo eseguita in una porzione del lobo destro del fegato dimostra un basso picco di intensit ( bassa concentrazione di mdc ) ( freccia ) ed un profilo a cupola corrispondente ad un lento accumulo e lento , progressivo rilascio del mdc . performed one day after treatment revealed time - intensity curves without plateaus and with low peaks of signal intensity , confirming complete necrosis of the tumour and success of the treatment . 
this finding was confirmed by the biopsy . instead , in one patient without intralesional flow signals but with persisting perilesional flow signals and time - intensity curve characterised by plateau and high peak of signal intensity , the biopsy revealed residual neoplastic tissue . 
 non si sono verificate reazioni avverse alla somministrazione ev del mdc . discussione le curve intensit / tempo permettono lo studio del comportamento della vascolarizzazione intra e perilesionale dopo la somministrazione ev del mdc e in particolare monitorizzano landamento della concentrazione del mdc nella regione dinteresse in un tempo prestabilito . 
lesistenza di strutture vascolari intra e perilesionali di tipo neoplastico influenza il profilo delle curve in quanto la presenza di shunt artero - venosi e lassenza di sistemi sfinteriali fisiologici , tipiche dei vasi neoformati , si traduce in unintrappolamento del mdc allinterno degli stessi e quindi in una fase di wash - out caratterizzata dai plateau ( fasi stazionamento del mdc ) e presenza di elevati picchi di intensit . nel nostro studio lesame power doppler con mdc ha riscontrato la presenza di segnali vascolari intra o perilesionali in tutti i pazienti prima del trattamento intralesionale ; ci ha permesso lottenimento di curve intensit / tempo significative ; infatti la presenza di enhancement nellarea di interesse una condizione indispensabile e rappresenta quindi un limite della metodica . 
in 15 pazienti , al controllo dopo un giorno dal trattamento , sono state riscontrate curve intensit / tempo con assenza di plateau e basso picco di intensit a sostegno della necrosi completa del tumore e quindi del successo del trattamento ; ci stato confermato dalla biopsia di controllo , mentre , in un paziente che presentava assenza di segnali vascolari intralesionali e persistenza di segnali vascolari perilesionali , in cui la curva intensit / tempo mostrava profilo con plateau ed elevato picco di intensit , la biopsia confermava la persistenza di tessuto neoplastico . 
in questo ultimo caso la curva intensit / tempo ha evidenziato lincompleta necrosi tumorale anche in assenza di segnali vascolari intralesionali dopo il trattamento ; ci fa supporre che la presenza di tessuto neoplastico coinvolgeva la regione perilesionale . 
tale reperto assume notevole importanza , a nostro giudizio , poich il riscontro di una curva come la suddetta dopo il trattamento potrebbe fornire lindicazione per lesecuzione di unaltra seduta terapeutica per ottenere la completa necrosi del tumore . radiol med ( 2009 ) 114 : 3241 an indication for an additional treatment session to achieve complete necrosis of the tumour . 
 in the four patients exhibiting intralesional flow signals after treatment , the time - intensity curves were characterised by plateaus and high peaks of signal intensity , suggesting incomplete necrosis of the tumour , later confirmed by targeted biopsy . 
 the presence of plateaus and high peaks of signal intensity , which characterised all curves before treatment and those of lesions found to be positive at biopsy after treatment , might represent a pattern of neoplastic vascularity . the technique should be further evaluated on a larger number of patients . 
if our findings are confirmed , it could be proposed as an alternative to ct and mri in consideration of its numerous benefits , including limited invasiveness , rapidity , and lack of side - effects of contrast material . nei quattro pazienti che presentavano segnali vascolari intralesionali dopo il trattamento , le corrispondenti curve intensit / tempo mostravano profilo con plateau ed elevato picco di intensit a conferma dellincompleta necrosi del tumore , confermata dalla biopsia mirata . 
passariello1 1 sapienza universit di roma , dipartimento di scienze radiologiche , policlinico umberto i , viale regina elena 324 , 00161 roma , italy 2 sapienza universit di roma , dipartimento di urologia , policlinico umberto i , viale del policlinico 159 , 00161 roma , italy correspondence to : v . 
twenty - eight patients with suspected bladder cancer and ten patients who had undergone transurethral resection of the bladder were studied by ctc and vc in both the supine and prone positions after distending the bladder with air . 
valutare il ruolo della cistografia con tc ( ctc ) e della cistoscopia virtuale ( cv ) utilizzando una tc multidetettore a 64 strati ( tcmd - 64 ) nellidentificazione delle lesioni vescicali e confrontare i risultati ottenuti con la cistoscopia convenzionale . 
ventotto pazienti con sospetta neoplasia vescicale e 10 pazienti in follow - up dopo resezione trans - uretrale della vescica ( turb ) sono stati sottoposti ad esame ctc e cv . 
i valori di sensibilit e specificit delle singole metodiche ctc e cv sono stati costantemente inferiori rispetto a quelli riportati dalla valutazione combinata ( gruppo i : 93 , 10% / 92 , 31% ; gruppo ii : 100% / 100% ; gruppo iii : 100% / 100% )  . 
la cv e la ctc con tcmd - 64 sono tecniche proponibili nellidentificazione delle neoplasie vescicali di dimensioni comprese tra 1 e 5 multeriori studi necessitano di popolazioni pi ampie . 
 radiol med ( 2009 ) 113 : 5269 keywords bladder cancer ct cystography virtual cystoscopy parole chiave neoplasia vescicale cistografia tc cistoscopia virtuale introduction introduzione flexible cystoscopy is the gold standard for diagnosing bladder cancer , not only because of its high sensitivity and specificity in detecting lesions but also the possibility of performing resections or biopsies in real time [ 1 ]  . 
despite the development of new cystoscopes and examination techniques , flexible cystoscopy still remains an invasive investigation that is poorly tolerated by patients and is precluded in subjects with acute bleeding or urethral strictures [ 2 ]  . although noninvasive imaging modalities , such as intravenous urography and transabdominal ultrasound , have been used as first - line investigations in several studies [ 3 , 4 ] , the endoscopic approach , especially when implemented with the new fluorescence techniques that enable detection of flat or very small lesions ( < 5 mm ) [ 5 , 6 ] , remains the mainstay of all international diagnostic protocols . 
the first reports on the use of computed tomography cystography ( ctc ) and virtual cystoscopy ( vc ) for detecting bladder cancers were published in the late 1990s [ 79 ]  . 
with regard to lesion size , it has been shown that single - detector - row , fourdetector - row [ 13 ] and even 16 - detector - row ct performed with thin - slice reconstructions ( 1 mm ) [ 14 ] allow detection of lesions < 5 m incorporation of this modality in new study protocols is a critical decision that is being widely debated among clinicians and diagnostic specialists . 
this aspect does not seem to take into account the potential benefit , in terms of therapeutic timeliness , of early and noninvasive detection of minimal lesions , especially in the 30% of lesions that show rapidly progressive behaviour [ 15 ]  . 
in our opinion , the use of 64 - detector - row ct technology should improve z - axis resolution and increase spatial resolution , thanks to the acquisition of isotropic voxels , such that excellent sensitivity and specificity can be obtained for very small lesions . 
the aim of this study was to evaluate the diagnostic accuracy of ctc with vc in the early detection of bladder lesions 1 mm to 1 cm in size , using flexible cystoscopy as the standard of reference . 
 materials and methods study population between november 2006 and january 2008 , we selected 38 la cistoscopia convenzionale rappresenta attualmente il gold standard diagnostico di neoplasia vescicale non solo per i suoi elevati valori di sensibilit e specificit nellidentificazione di lesioni sospette , ma anche grazie alla possibilit di eseguire in tempo reale sia la resezione che un eventuale prelievo bioptico [ 1 ]  . 
nonostante lo sviluppo di nuovi cistoscopi e metodiche di esecuzione dellindagine , la cistoscopia convenzionale rimane , ancora oggi , un esame invasivo , generalmente poco tollerato dai pazienti e che non pu essere eseguito in tutti i casi come in soggetti che presentano un sanguinamento acuto o una stenosi uretrale [ 2 ]  . 
 le metodiche di imaging diagnostico non invasive , quali lurografia intravenosa , lecografia transaddominale sono state introdotte come primo approccio in diversi studi [ 3 , 4 ] , tuttavia lapproccio endoscopico , in considerazione anche delle nuove tecniche a fluorescenza , con cui stato implementato per lidentificazione delle lesioni piatte o molto piccole ( < 5 mm ) [ 5 , 6 ] , rimane un caposaldo in tutti i protocolli diagnostici internazionali . 
le prime cistografie con tc ( ctc ) e con cistoscopia virtuale ( cv ) per lo studio delle neoplasie vescicali sono state eseguite alla fine degli anni 90 [ 79 ] ; da allora la tecnica stata ampiamente sviluppata e recenti studi [ 1012 ] dimostrano alti potenziali di sensibilit nellidentificazione di neoplasie vescicali . per quanto riguarda le dimensioni delle lesioni vescicali , stato dimostrato che le tc a singolo detettore , a 4 detettori [ 13 ] e perfino a 16 detettori , utilizzando protocolli di studio con ricostruzioni a strato sottile ( 1 mm ) [ 14 ] , permettono lidentificazione di lesioni al di sotto dei 5 mm . linserimento di questa metodica di indagine in nuovi protocolli rimane attualmente una decisione critica dibattuta tra clinici e diagnosti specialisti . 
questo aspetto non sembra quindi rendere conto del vantaggio che lindividuazione precoce , con un metodo non invasivo , di lesioni minime potrebbe rappresentare in termini di tempestivit terapeutica : soprattutto in quel 30% dei casi in cui queste lesioni mostrano un comportamento rapidamente progressivo [ 15 ]  . 
lutilizzo delle apparecchiature tc con tecnologia multistrato a 64 detettori , dovrebbero migliorare la risoluzione lungo lasse z ed aumentare la risoluzione spaziale grazie alla isotropicit dei voxels , cos da offrire unottima sensibilit e specificit diagnostica per lesioni di dimensioni esigue . 
lo scopo di questo studio stato analizzare il grado di accuratezza diagnostica della cistrografia tc con cistoscopia virtuale nellidentificazione precoce di lesioni vescicali di dimensioni comprese tra 1 mm e 1 cm , utilizzando la cistoscopia convenzionale come metodica di riferimento . 
the population was initially divided into 28 patients ( 22 men and six women ) who had not undergone surgery and ten patients ( eight men and two women ) who were being followed up after transurethral resection of the bladder ( turb )  . 
all patients had a medical history suspicious for bladder cancer , including haematuria with negative urine culture , exposure to carcinogenic chemical agents , family history , recurrent or parasitic infections and positive cytology on urinalysis . 
approximately 1 week ( mean 83 ) after the ct scan , each patient was studied with conventional cystoscopy to determine the presence , location , morphology and size of any bladder lesions . 
 patient preparation before ct examination , a three - way 12 - f foley catheter was inserted into the bladder to achieve complete voiding . the bladder was then distended by insufflating 350500 cc of room air with 50 cc syringes , depending on patient tolerance . 
images obtained with these scans were then analysed by a third , independent , radiologist who materiali e metodi popolazione di studio in un periodo compreso fra novembre 2006 e gennaio 2008 , abbiamo selezionato complessivamente 38 pazienti ( 30 di sesso maschile e 8 di sesso femminile ) afferenti presso il centro per le neoplasie dellapparato urinario del dipartimento di urologia del nostro nosocomio . 
la popolazione di studio stata inizialmente suddivisa in 28 pazienti ( 22 uomini e 6 donne ) che non avevano subito interventi chirurgici e 10 ( 8 uomini e 2 donne ) pazienti in fase follow - up dopo resezione trans - uretrale della vescica ( turb )  . 
tutti i pazienti presentavano unanamnesi sospetta per neoplasia vescicale comprendente ematuria con urino - coltura negativa per processi infiammatori aspecifici , fattori di rischio con esposizione ad agenti chimici cancerogeni , familiarit , anamnesi di infezioni ricorrenti o malattia parassitaria della vescica e citologia positiva allesame delle urine . 
a circa una settimana ( media 83 ) dopo lesame tc ciascun paziente stato sottoposto ad esame di cistoscopia convenzionale in cui stata stabilita la presenza , la localizzazione , la morfologia e la dimensione di eventuali lesioni vescicali . 
 preparazione dei pazienti prima dellesecuzione dellesame tc nel lume vescicale stato posizionato un catetere di foley a tre vie ( calibro 12 f ) per il completo svuotamento della vescica ; successivamente stato disteso il lume vescicale insufflando circa 350500 cc di aria tramite siringhe da 50 cc , tenendo conto del grado di tolleranza del paziente . 
dopo lesame e la rimozione del catetere , a tutti i pazienti stata prescritta una terapia antibiotica a scopo profilattico per 3 giorni . apparecchiatura tc e protocolli di scansione tutti gli esami sono stati eseguiti con unapparecchiatura tc spirale multistrato a 64 detettori ( somatom sensation 64 , siemens , germania ) utilizzando i seguenti parametri : radiol med ( 2009 ) 113 : 5269 performed a contrast - enhanced scan ( at 60 s ) directly in the prone position to evaluate the possible extramural extension of any identified mural lesion . 
for each scan , we used multiplanar reconstructions ( mpr ) in the sagittal and coronal planes and volume rendering ( vr ) for endoluminal viewing ( virtual endoscopy )  . each examination was analysed in a double - blind fashion by two radiologists with 10 years experience in virtual endoscopy and who were unaware of patients clinical data . image analysis was performed over three reading sessions held approximately 1 week apart in which the order of the patients was changed each time . 
for each step , the radiologists expressed a diagnostic judgment on any lesion identified based on the following parameters : lesion site ( bladder dome , walls and trigone ) , size and morphology ( sessile where the base was larger than the height , otherwise pedunculated )  . 
bladder distension was evaluated on axial images using a reference score based on maximum anteroposterior diameter ( < 10 cm , poor distension = score 0 ; 1015 cm , satisfactory distension = score 1 ; > 15 cm , optimal distension = score 2 )  . 
bladder lumen and mucosa were studied with a pulmonary window level setting ( 1 , 500 / 700 hu ) ; bladder walls and extraluminal structures were studied with an abdominal - level setting ( 400 / 40 hu )  . 
for virtual cystoscopy , we used the 3d lit fly - through with direct lightshiny rendering and ct fatmusclebone colouring ( window the ct level 1500 / 200 ) supplied with colonoscopy software . 
 statistical analysis the study population was divided into three groups according to the size of bladder lesions identified at flexible cystoscopy : group 1 : lesions with maximum diameter from 1 mm to 5 mm group 2 : lesions between 5.1 mm and 9 mm 50 mas , 120 kv , spessore effettivo della fetta 1 millimetro , collimazione 0 , 6 millimetri , incremento di ricostruzione 0 , 75 millimetri , kernel b30 smooth , velocit di rotazione del tubo 0 , 5 s , risoluzione spaziale ( x ) 0 , 4 mm ( y ) 0 , 4 mm ( z ) 0 , 4 mil campo di vista ( fov ) stato ottimizzato individualmente per la valutazione completa della pelvi , in modo da ottenere contemporaneamente sia una visualizzazione della vescica sia delle strutture extra - vescicali ( media fov 304040 cm )  . 
successivamente sono state effettuate scansioni sia in posizione supina che prona per evitare che eventuali residui fluidi potessero occultare piccole lesioni parietali ; le immagini ottenute da queste scansioni sono state poi analizzate da un terzo radiologo non coinvolto nel presente studio il quale , nel caso in cui identificava lesioni vescicali , eseguiva una scansione supplementare della pelvi direttamente nella posizione prona , dopo somministrazione di mezzo di contrasto iodato non ionico ( a 60 s ) , al fine di evidenziare una possibile estensione extra - parietale della lesione . 
la dose length product ( dlp ) utilizzata stata di 354 mgy / cm , il computed tomography dose index / weight ( ctdiw ) stato di 29 , 06 mgra y e la dose efficace ( de ) stata di 6 , 726 msv . 
in caso di scnsione supplementare della pelvi , il valore dlp stato di 531 mgy / cm , il ctdiw stato di 43 , 59 mgray e il ed stato di 10 , 089 msv . post - processing ed analisi dei dati acquisiti i dati ottenuti con tale protocollo sono stati trasferiti in tempo reale ad una workstation del tipo hp kajak xu 800 double 2 , 8 ghz cpu , 3 , 37 gb di ram , con hard - disk da 140 gb e software dedicato , vitrea ( versione 3.7 , vital images , inc . , plymouth , minnesota , usa ) per lelaborazione e lanalisi dei dati . 
per ogni scansione eseguita sono stati utilizzati algoritmi di ricostruzione multiplanari ( mpr ) sui piani di scansione sagittale e coronale e di volume rendering per la visione endoluminale ( endoscopia virtuale )  . ogni singolo esame stato analizzato in doppio cieco da due radiologi , con 10 anni di esperienza in endoscopia virtuale , i quali non erano a conoscenza dei risultati clinici di preselezione dei pazienti . 
il protocollo di analisi delle immagini si basato su tre sessioni di lettura a distanza di circa una settimana luna dallaltra , nelle quali lordine dei pazienti analizzati stato cambiato ogni volta . 
durante i tre step i radiologi hanno quindi valutato dapprima le immagini assiali 2d nelle scansioni in posizione prona e supina , successivamente le immagini ricostruite con lalgoritmo multiplanare mpr ed infine le ricostruzioni con algoritmo vr ( visione endo - luminale )  . 
per ciascuna fase di analisi i radiologi hanno espresso un giudizio diagnostico sulle eventuali lesioni osservate stimando i seguenti parametri : sede ( cupola , pareti e fondo della vescica ) , dimensioni e morfologia ( sessile ove la base fosse maggiore dellaltezza , peduncolata nel caso contrario )  . 
furthermore , we conducted a detailed analysis of the first group using receiver operating characteristic ( roc ) curves to determine , for each technique taken alone and in combination , the lowest size threshold at which the method showed the best level of diagnostic accuracy . 
histopathology revealed the presence of neoplastic cells in 62 resected specimens , 52 of which were in 28 presurgical patients and ten in post - turb patients ( 48 lesions were transitional - cell carcinomas , ten were clear - cell adenocarcinomas and four were small - cell carcinomas )  . considering the subdivision of lesions into subgroups , 29 positive lesions were identified in 14 patients in group 1 , with lesions < 5 mm [ nine presurgical and five post - turb patients ; size range 1.35 mm ; mean 3.4 mm ; median 3.5 mm ; standard deviation ( sd ) 0.83 ] , 18 positive lesions were identified in 12 patients in group 2 , with lesions between 5.1 and 9 mm ( eight presurgical and four post - turb patients ; size range 5.29 mm ; mean 7.2 mm ; median 7.35 mm ; sd 1.196 ) , and 15 positive lesions were identified in 12 patients in group 3 , with lesions > 9.1 mm ( 11 presurgical patients and one post - turb patient ; size range 9.322 mm ; mean 12.42 mm ; median 11 mm ; sd 3.46 ) ( table 1 )  . 
mean examination time , excluding catheter insertion , was 82 m reconstruction of raw data produced approximately 800 images for each data set ( considering both supine and prone scans ) , with an additional 400 images in the case of contrast - enhanced imaging for staging purposes . 
per la valutazione del lume vescicale e della mucosa stato impostato un livello della finestra ottimale per il parenchima polmonare ( 1500 / 700 hu ) mentre il livello della finestra per laddome ( 400 / 40 hu ) stato utilizzato per la valutazione della parete e delle strutture extra - luminali . 
per la cistoscopia virtuale abbiamo utilizzato il preset fornito nel software dedicato per la colonscopia vituale 3d lit fly - trough con rendering direct light - shiny e colorazione tc fat - muscle - bone ( finestra utilizzata 1500 / 200 )  . 
in particolare sono stati stabiliti tre valori principali di cut - off dimensionale cos distribuiti : gruppo i : lesioni comprese fra 1 mm e 5 mm di diametro massimo ( dm ) ; gruppo ii : lesioni comprese fra 5 , 1 e 9 mm di dm ; gruppo iii : lesioni pi grandi di 9 , 1 mm di dm . lanalisi statistica dei dati raccolti stata realizzata calcolando sensibilit e specificit di ogni singola metodica ( ctc in posizione supina e prona , cv supina e prona , esame completo considerando entrambe ) per ogni sub gruppo di pazienti . 
abbiamo inoltre condotto un analisi accurata del primo gruppo di pazienti utilizzando il metodo delle receiver operating characteristic ( roc ) curve analysis per stabilire , per ciascuna metodica di scansione e per lanalisi combinata delle stesse , quale fosse il limite inferiore dimensionale in cui la metodica mostrava il miglior livello di accuratezza diagnostica . 
come ulteriore controllo abbiamo condotto un analisi incrociata dei risultati ottenuti dai due radiologi nellidentificazione delle lesioni nei tre gruppi , utilizzando il metodo di inter - rater agreement con statistica k per valutare la variabilit interoperatore . 
i seguenti valori di k sono stati utilizzati come cut - off analisi del livello di concordanza statistica : concordanza ; = 0 , 210 , 40 = modesta < 0 , 20 = scarsa = 0 , 410 , 60 = moderata concordanza ; concordanza ; = 0 , 610 , 80 = concordanza buona ; = 0 , 811 , 00 = concordanza completa . 
per tutti i test statistici utilizzati un livello di p < 0 , 05 stato considerato significativo . risultati cistoscopia convenzionale la cistoscopia convenzionale ha visualizzato correttamente un totale di 88 lesioni fra i 38 soggetti esaminati . 
prone vc had a sensitivity of 89.66% , a specificity of 92.31% , a ppv of 96.30% and an npv of 80% , whereas e 10 in pazienti post - turb ( 48 erano carcinomi a cellule transizionali , 10 adenocarcinomi a cellule chiare e 4 carcinomi a piccole cellule )  . 
la suddivisione in sub gruppi ha quindi identificato 29 lesioni positive in 14 pazienti nel i gruppo con neoplasie inferiori a 5 mm ( 9 pazienti preoperatori e 5 post - turb ; dimensioni minime 1 , 3 mm / massime 5 mm ; media 3 , 4 mm ; mediana 3 , 5 mm ; deviazione standard 0 , 83 ) , 18 lesioni positive in 12 pazienti nel ii gruppo con neoplasie comprese tra 5 , 1 e 9 mm ( 8 pazienti preoperatori e 4 post - turb ; dimensioni minime 5 , 2 mm / massime 9 mm ; media 7 , 2 mm ; mediana 7 , 35 mm ; deviazione standard 1 , 196 ) e 15 lesioni positive in 12 pazienti nel iii gruppo con neoplasie superiori a 9 , 1 mm ( 11 pazienti preoperatori e 1 post - turb ; dimensioni minime 9 , 3 mm / massime 22 mm ; media 12 , 42 mm ; mediana 11 mm ; deviazione standard 3 , 46 ) ( tabella 1 )  . 
 cistografia tc e cistoscopia virtuale gli esami tc sono stati generalmente ben tollerati dai pazienti , sebbene in 6 / 38 ( 4 / 10 pazienti dopo turb ) casi si sia verificato un certo disagio dovuto ad un diverso grado radiol med ( 2009 ) 113 : 5269 fig . 
1a - c sagittal multiplanar reproduction ( mpr ) images used for scoring bladder distension : optimal distension coincided with the insufflation of 450350 ml of air ( a ) , whereas satisfactory ( b ) and poor ( c ) distension levels were usually obtained with 350250 ml and < 250 ml . 
1a - c immagini mpr sagittali utilizzate per la valutazione del grado di distensione vescicale : una distensione ottimale coincide con linsufflazione di 350450 ml di aria ( a ) , mentre livelli di distensione soddisfacenti ( b ) e scarsi ( c ) vengono ottenuti di solito con 250350 ml e meno di 250 ml . 
in media il tempo per lesecuzione dellesame , escluso quello relativo al posizionamento del catetere , stato di 82 m la ricostruzione dei dati grezzi ha generato circa 800 immagini per ogni insieme di dati ( considerando entrambe le scansioni prona e supina ) , con un incremento di 400 immagini per l eventuale scansione di staging con mdc . 
il tempo medio della ricostruzione ctc / cv stato di 103 mcon un tempo medio di refertazione di 152 mla distensione della vescica risultata ottimale in 30 casi , soddisfacente in 5 e scarsa in 3 . 
la vc in posizione prona una sensibilit del 89 , 66% , specificit 92 , 31% , ppv 96 , 30% e npv del 80% ; mentre nella posizione supina sensibilit del 82 , 76% , specificit del 92 , 31% , ppv 96% e npv 70 , 59% . 
la valutazione combinata delle immagini ottenute con le diverse metodiche di valutazione nelle diverse posizioni ha riportato valori nettamente superiori con sensibilit del 93 , 10% , specificit 92 , 31% , ppv 96 , 43% e npv del 85 , 71% ( tabella 2 )  . la successiva analisi dei risultati con le curve roc ha evidenziato una tendenza simile alla statistica precedente riportando valori di area sottesa alla curva ( auc ) costantemente maggiori ( maggiore accuratezza diagnostica ) per la valutazione complessiva delle tecniche rispetto ad ogni singola metodica ( ctc prona = 0 , 844 ; ctc supina = 0 , 809 ; vc prona = 0 , 944 ; vc supina = 0 , 901 ; complessiva = 0 , 963 ) ( tabella 3 )  . 
dalle stessa analisi delle curve emerso che la valutazione complessiva abbassa sensibilmente anche il limite inferiore dimensionale per cui si mantiene il livello massimo di accuratezza diagnostica ( ctc prona = 2 , 4 mm ; ctc supina = 2 , 1 mm ; vc prona = 1 , 9 ; vc supina = 2 mm ; complessiva = 1 , 4 mm )  . 
the high - resolution scan protocol and optimal bladder distension allowed clear depiction of the lesion on both the sagittal multiplanar reproduction ( mpr ) ( arrow in a ) and native axial ( arrow in b ) images . 
il protocollo di scansione ad alta risoluzione e lottimale distensione vescicale hanno permesso una chiara visualizzazione della lesione in mpr sia sagittale ( a , freccia ) che assiale nativa ( b , freccia )  . 
nelle immagini vr ( c , testa di freccia ) , la lesione appare come un polipo regolarmente formato con una piccola base di impianto ; lesame istologico dopo resezione tramite cistoscopia convenzionale ( d ) ha dimostrato la presenza di cellule transizionali neoplastiche . 
comparando la scansione ctc supina con lacquisizione in posizione prona , non stata evidenziata una lesione peduncolata di circa 2 mm localizzata a livello del trigono e occultata verosimilmente da residui urinari . 
lanalisi statistica dei risultati riportati dalla valutazione delle immagini ottenute con la sola ctc in posizione prona ha riportato una sensibilit del 88 , 89% , specificit 88 , 89% , ppv 94 , 12% e npv del 80% ; mentre nella posizione supina sensibilit del 94 , 44% , specificit del 88 , 89% , ppv 94 , 44% e npv 88 , 89% . 
la vc in posizione prona una sensibilit del 100% , specificit 88 , 89% , ppv 94 , 74% e npv del 100% ; mentre nella posizione tabella 2 analisi statistica dei risultati ottenuti dalla valutazione singola e combinata di ciascuna metodica nelle differenti posizioni . 
questi risultati debbono comunque essere considerati come indicativi in base al numero di pazienti reclutati nel nostro studio preliminare ctc prona ctc supina vc prona vc supina ct combi confronto tra cistografia e cistoscopia virtuale gruppo 1 risultati gruppo 2 risultati gruppo 3 risultati sensibilit specificit sensibilit specificit sensibilit specificit 75 , 86% 84 , 62% 92 , 00% 61 , 11% 88 , 89% 88 , 89% 94 , 12% 80 , 00% 100% 100% 100% 100% 68 , 97% 76 , 92% 86 , 96% 52 , 63% 94 , 44% 88 , 89% 94 , 44% 88 , 89% 100% 100% 100% 100% 89 , 66% 92 , 31% 96 , 30% 80 , 00% 100% 88 , 89% 94 , 74% 100% 100% 100% 100% 100% 82 , 76% 92 , 31% 96 , 00% 70 , 59% 100% 88 , 89% 94 , 74% 100% 100% 100% 100% 100% 93 , 10% 92 , 31% 96 , 43% 85 , 71% 100% 100% 100% 100% 100% 100% 100% 100% ctc prona ctc supina vc prona vc supina ct combi ctc prona ctc supina vc prona vc supina ct combi ctc , cistografia con tc ; vc , cistografia virtuale ; ppv , valore predittivo positivo ; npv , valore predittivo negativo radiol med ( 2009 ) 113 : 5269 table 3 results of receiver operating characteristic ( roc ) curve analysis in group 1 . 
da notare come i valori di auc ( area under the roc curve ) , rispecchiando i valori di accuracy di ciascun approccio diagnostico ( valutazione singola di ctc e vc e combinata ) , dimostri una costante superiorit dellapproccio combinato . 
la valutazione combinata delle immagini ottenute con le diverse metodiche di valutazione nelle diverse posizioni ha riportato anche in questo gruppo valori nettamente superiori con sensibilit del 100% , specificit 100% , ppv 100% e npv del 100% ( tabella 2 )  . gruppo iii ( lesioni > 9 mm ) nei 12 pazienti nel iii gruppo ( 11 preoperatori e 1 postturb ) le lesioni identificate avevano una dimensione minima di 9 , 3 mm e massima di 22 mm ( media 12 , 42 mm ; mediana 11 mm ; deviazione standard 3 , 46 ) la morfologia delle lesioni identificate stata di tipo peduncolato in 11 fig . 
the area under the curve related to combined computed tomography cystography ( ctc ) and virtual cystoscopy ( vc ) ( ct overall ) is greater compared with those of ctc and vc alone , reflecting the superiority of the combined approach . 
la curva che si riferisce allapproccio combinato ( ct overall ) sottende un area ( auc : area under the roc curve ) maggiore rispetto alle altre curve , riflettendo la superiorit diagnostica dellapproccio combinato . radiol med ( 2009 ) 113 : 5269 fig . 
on sagittal multiplanar reconstruction ( mpr ) ( a ) and native axial ( b ) images , only two out of four lesions are visualised , and the hypertrophic mucosal folds do not allow clear depiction of the remaining polyps . 
in contrast , the volumerendered images ( c ) allow an intuitive discrimination between the long , curved mucosal folds ( arrowheads in c ) and the polyps ( arrows in c )  . 
nelle immagini mpr sagittali ( a ) e assiali ( b ) solo 2 su 4 lesioni totali possono essere visualizzate e le pliche ipertrofiche della mucosa non permettono una chiara individuazione dei rimanenti polipi . 
daltro canto , le immagini in vr ( c ) permettono una intuitiva discriminazione fra le lunghe pliche arrotondate delle pliche mucosa ( c , teste di frecce ) ed i polipi ( c , frecce )  . 
la sensibilit e specificit per lidentificazione delle lesioni stata del 100 % sia per la ctc ( scansione prona e supina ) che per la cv ( scansione prona e supina ) ( tabella 2 )  . 
nella tabella 4 troviamo anche i valori di concordanza parziale nei diversi gruppi ; un livello di concordanza inferiore viene dimostrato soprattutto tra il primo e il secondo gruppo di pazienti , dove le dimensioni delle lesioni hanno probabilmente reso pi diffifig . 
le ricostruzioni in vr ad alta risoluzione spaziale permettono uneccellente definizione delle immagini di cv , le quali sono fortemente confrontabili a quelle dellapproccio endoscopico convenzionale ( d )  . radiol med ( 2009 ) 113 : 5269 radiologist 2 interrater variability statistical analysis of the results of each radiologist revealed a k value of 0.868 ( table 4 ) , indicating complete agreement between the two radiologists . 
lower agreement levels were recorded in groups 1 and 2 in particular , where small lesion size probably hindered correct measurements , leading radiologist 2 to misclassify four group - 1 lesions ( based on measurements made with flexible cystoscopy ) as belonging to group 2 . 
7 , which compares the two radiologists performance in classifying lesions and shows the overall greater accuracy of radiologist 1 in assigning lesions to the groups established with flexible cystoscopy . discussion a number of imaging techniques have been proposed for detecting bladder lesions , but conventional cystoscopy remains the standard of reference in diagnosing bladder carcinoma [ 16 ]  . 
conventional cystoscopy allows not only the detection of lesions < 1 cm but also the opportunity to perform immediate resection ( curative or palliative ) and obtain a tissue sample for histopathological examination . on the other hand , conventional cystoscopy is , after colonoscopy , one of the most invasive and poorly tolerated examinations , often requiring local anaesthesia and sedatives to increase patient compliance . 
the technique is also limited by several intrinsic absolute contraindications that cannot be easily overcome , and it is precluded in patients with active haematuria or urethral strictures [ 2 ]  . 
additionally , even modern fibreoptic cystoscopes are often incapable of visualising correctly the bladder neck and luminal diverticula , especially in the anterior wall sites that are often prone to mucosal dysplasia with malignant degeneration [ 17 ]  . 
il grafico mette confronto visivamente ( nella tabella 4 numericamente ) i risultati ottenuti dal radiologo 1 con quelli del radiologo 2 inserendo nella prima colonna di ciascun gruppo i risultati in accordo e nella seconda quelli in disaccordo . 
 cile un corretta misurazione delle stesse , portando soprattutto per quanto riguarda il radiologo 2 , ad assegnare 4 pazienti del gruppo i ( sulla base della misurazione con cistoscopia convenzionale ) al gruppo ii . 
7 a colonne raggruppate che confronta lattribuzione a ciascun gruppo da parte dei due radiologi nel quale il primo ha dimostrato una accuratezza globale migliore nella misurazione delle lesioni osservate rispetto alla suddivisione in gruppi operata dalla cistoscopia convenzionale . discussione ad oggi sono state proposte diverse metodiche di imaging per lidentificazione delle lesioni vescicali anche se la cistoscopia convenzionale rimane la metodica di riferimento nella diagnosi di carcinoma della vescica [ 16 ]  . 
lapproccio endoscopico convenzionale garantisce oltre allidentificazione di lesioni subcentimetriche , la possibilit di realizzare un trattamento escissionale immediato ( curativo o palliativo ) e di poter ottenere un campione di tessuto per lesame bioptico . 
di contro , la cistoscopia tradizionale rappresenta , dopo la colonscopia , una delle procedure endoscopiche pi invasive e poco tollerate per il paziente al punto che lanestesia locale e leventuale somministrazione di sedativi sono spesso richiesti per aumentare il grado di compliance allesame del paziente . 
la cistoscopia convenzionale presenta inoltre alcune intrinseche intrinseche ed assolute controindicazioni allesecuzione che non possono essere facilmente superate : infatti i pazienti con ematuria in atto o radiol med ( 2009 ) 113 : 5269 involving turb and the size of bladder cancers at the time of initial diagnosis significantly affects treatment decisions . 
in fact , treatment protocols for lesions < 1 cm are essentially based on a conservative approach local chemotherapy ( bacillus of calmette - gurin , doxorubicin , mitomycin , gentamicin ) [ 15 , 19 ] , whereas those for involve neoadjuvant lesions advanced and chemotherapy and radiotherapy followed by surgical resection [ 20 ]  . 
moreover , it should be recalled that lesions < 10 mm carry a statistical risk , albeit low , of concurrent or preexisting invasion of the muscularis propria , which is in turn associated with metastatic spread [ 21 ]  . 
 larger our results suggest that ctc with vc represents a valuable and noninvasive diagnostic method for detecting recurrent or de novo bladder cancers ranging from 2 mm to 9 mm in size . 
furthermore , table 3 interestingly reveals an increase in specificity brought about by vc compared with ctc alone , probably as a result of better delineation of the mucosal surface . these statistical data may appear overly optimistic , and we need to acknowledge a probable bias related to the small number of patients in our series . 
 [ 22 ] identified only 70% of lesions < 1 cm by using a single - detector - row scanner with 3 - mm collimation , and kim et al . 
our analysis of interrater agreement seems in part to reflect the difficulties encountered by song et al . , showing a decreased ability to identify and measure lesions < 5 mhowever , this finding applies to < 30% of patients in group 1 and is , we believe , related to the degree of bladder distension , a crucial factor when evaluating very small lesions . 
in particular , in several cases with irregular appearance of the mucosal surface , bladder - wall evaluation was limited by poor bladder distension : in one of these cases , tumour identification proved impossible , whereas in the other case , it was only possible thanks to the large size of the mass ( 23 mm )  . 
the use of con stenosi uretrale non possono essere sottoposti a questo tipo di indagine [ 2 ] ; inoltre , anche i moderni cistoscopi a fibre ottiche difficilmente riescono a visualizzare correttamente il collo vescicale ed i diverticoli presenti nel lume vescicale , soprattutto della parete anteriore : siti frequentemente esposti a displasia della mucosa con degenerazione neoplastica [ 17 ]  . 
 per ovviare a tali limitazioni , vining ed altri autori hanno introdotto , per primi , nel 1996 la ctc con cv come metodica mini - invasiva per lo studio endoscopico della vescica e per la diagnosi delle lesioni vescicali [ 7 ]  . 
solo un anno pi tardi , hussain e altri autori [ 9 ] hanno proposto la cistoscopia virtuale , in alternativa alla cistoscopia convenzionale , come primo approccio diagnostico in pazienti con ematuria o nel follow - up dopo resezione della neoplasia . oggi , grazie allenorme diffusione delle apparecchiature tc multidettetore , la ctc con cv non rappresenta pi una raffinata evoluzione tecnica , ma sta lentamente cominciando a seguire la strada in passato intrapresa dalla colonscopia virtuale . 
tuttavia , la principale limitazione di questa metodica , rappresentata da unaccuratezza non ottimale nellidentificazione di piccole lesioni , ha continuato , sino ad oggi , a precludere limpiego nella diagnosi precoce delle lesioni vescicali [ 18 ]  . 
infatti , nel caso di lesioni subcentimetriche il protocollo terapeutico si basa essenzialmente su un approccio conservativo con resezione trans - uretrale ( turb ) e con la somministrazione locale di agenti chemioterapici ( bacillo di calmette - guerin , doxorubicina , mitomicina , gentamicina ) [ 15 , 19 ]  . 
al contrario per le neoplasie in stadio avanzato e con dimensioni maggiori i protocolli prevedono dapprima un trattamento neoadiuvante chemioterapico e radioterapico seguito dalla resezione chirurgica [ 20 ]  . 
inoltre bisogna tenere presente che lesioni inferiori a 10 millimetri presentano comunque un rischio statistico seppur basso di invasione concomitante o pre - esistente della muscularis propria che a sua volta si associa a diffusione metastatica della malattia [ 21 ]  . 
 i nostri risultati sembrerebbero dimostrare che la ctc insieme alla cv , rappresentano una metodica diagnostica valida e non invasiva per lidentificazione di lesioni della vescica ricorrenti o di nuova insorgenza con dimensioni comprese fra 29 millimetri . 
in particolare lanalisi dei dati compiuta nel gruppo di lesioni sotto i 5 mm ha dimostrato come un approccio combinato delle tecniche ctc e vc permette non solo di migliorare il grado di sensibilit e specificit statistica nellindividuazione della lesione sospetta ( sensibilit 93 , 10% e specificit 92 , 31% ) , ma soprattutto ridurre sensibilmente il limite dimensionale di identificazione ( 1 , 4 mm con sensibilit di 93 , 1% e specificit de 100% ) , come dimostrato dallanalisi roc ( tabella 3 )  . 
inoltre dalla stessa tabella 3 emerge il dato interessante dellaumento di specificit diagnostica apportato dalla cv rispetto ai valori riportati dalla sola ctc , probabilmente dovuto alla migliore delineazione della superficie total table 4 interrater agreement with kappa statistics . 
questi dati statistici potrebbero apparire oltremodo ottimistici e riconosciamo un probabile bias dovuto allesiguo numero di pazienti reclutato nello studio , tuttavia devono essere intesi come esperienza preliminare in vista di studi su larga scala che dovranno includere necessariamente popolazioni di studio pi ampie ed omogenee rispetto a quella selezionata nel presente studio . inoltre i nostri dati sono sostanzialmente concordi con i risultati di altri studi come quello effettuato da nerumi et al . 
 [ 22 ] il quale ha individuato solo il 70% delle lesioni < 1 cm servendosi di tc a singolo strato con collimazione a 3 mm , mentre kim et al . 
 [ 23 ] ha identificato l82% delle lesioni < 5 mm utilizzando uno scanner mdct a 4 strati ed una collimazione di 1 , 25 mm ; al contrario , song et al . 
 [ 18 ] utilizzando uno scanner mdct a 16 strati ed una collimazione di 3 millimetri , hanno definito inattendibile la metodica ctc insieme alla cv nellidentificazione di lesioni di dimensioni < 5 mm ( solo il 60% delle lesioni )  . 
la nostra analisi della variabilit inter - operatore sembra riflettere in parte le difficolt incontrate in questultimo studio riportando una diminuzione della capacit di individuazione e di misurazione di lesioni sospette inferiori ai 5 mtuttavia questo dato si riferisce a meno del 30% dei pazienti del primo gruppo ed a nostro avviso da correlare al grado di distensione della parete vescicale che assume necessariamente importanza critica in lesioni molto piccole . 
in particolare , in alcuni casi in cui la superficie mucosa si presentava irregolare , il risultato della valutazione della parete vescicale ha risentito dello scarso grado di distensione vescicale : infatti in uno di questi casi con scarsa distensione , lindividuazione del tumore non stata possibile , mentre nellaltro caso , solamente le grandi dimensioni della massa ( 22 mm ) ne hanno permesso lidentificazione . 
si dovrebbe considerare quindi lutilizzo di agenti farmacologici spasmolitici , introdotti con successo negli esami di colografia con tc di routine [ 24 ] in modo da facilitare il raggiungimento di una distensione vescicale adeguata nei pazienti con scarsa compliance e con disordini vescicali . 
altre modalit di distensione , come il riempimento da parte del mezzo di contrasto per via escretoria [ 22 ] o retrograda [ 25 ] , potrebbe rappresentare una valida alternativa ; tuttavia stato provato che linsufflazione di aria sia superiore allopacizzazione positiva per il pi alto gradiente di attenuazione raggiungibile con bassa corrente di tubo ( 100 mas ) , e con ricostruzioni virtuali meno soggette ad artefatti [ 26 ]  . 
una maggiore sensibilit , utilizzando entrambe le tecniche ( 2d e 3d ) , pu essere raggiunta in tutti i pazienti con una distensione ottimale o soddisfacente della vescica ; nel nostro studio , il livello ottimale di distensione ha coinciso con linsufflazione di circa 350450 cc di aria , il livello soddisfacente con 250350 cc e il livello scarso con meno di 250 cc ; ad ogni modo la validit di queste misurazioni soltanto indicativa , poich bisogna prendere atto di alcune considerazioni : unelevata distensione vescicale ( 350450 ml ) riduce lo spessore globale delle pareti vescicali ( nel nostro studio lo spessore medio di parete con distensione stato di 1 , 7 mm ) e pu radiol med ( 2009 ) 113 : 5269 to be superior to positive opacification due to the higher attenuation gradients achievable with low tube current ( 100 mas ) and fewer artefacts on virtual reconstructions [ 26 ]  . 
regardless , the validity of these measurements is only indicative , as several factors need to be considered : a high degree of bladder distension ( 350450 ml ) reduces the overall thickness of the bladder walls ( mean wall thickness of distended bladders was 1.7 mm ) and may enhance the accuracy in identifying focal thickening ( often related to tumour infiltration ) ; on the other hand , a poorly distended bladder ( < 250 ml ) coincides with poor delineation of the mucosal profile and a thickened bladder wall , thus hindering the detection of mural pathology . technical considerations include a short scanning time ( 3.5 s ) , which did not affect image quality with movement artefacts . 
the optimal attenuation gradient achieved between the air - dilated bladder lumen and the surrounding soft tissue allowed both tube current and radiation exposure to be significantly reduced in comparison with other studies [ 13 , 14 , 27 ]  . 
the use of a new - generation 64 - detector - row scanner combined with a high - resolution protocol with low values for slice thickness ( 1 mm ) , collimation ( 0.6 mm ) and reconstruction increment ( 0.4 mm ) enabled accurate , highresolution and fast exploration of the entire region of interest , offering reliable views for lesion detection . 
on the other hand , the high spatial resolution achieved with this thin - slice scanning protocol substantially increases the number of images and the amount of data acquired , requiring a dedicated workstation to efficiently handle data and reconstruct images . 
in contrast , ctc images were evaluated together with mpr reconstructions , as this allowed not only evaluation of axial images but also reliable multidimensional visualisation ( sagittal , coronal and oblique )  . among the various 3d techniques available , we chose vc because it is relatively familiar to radiologists specialising in virtual endoscopy , is widely accepted by clinicians and surgeons owing to its similarity to actual endoscopy and , most importantly , because of the better image quality reported in previous reports [ 2 , 28 ]  . the contribution of the 3d approach was fundamental . not only did it depict all lesions seen on 2d images , it also served as a diagnostic modality for lesions in subjects with suboptimal bladder distension and in two patients with irregular and hypertrophic mucosa . 
in these last two cases , ctc failed to discern between the folds of hypertrophic mucosa and pedunculated lesions , whereas vc allowed correct evaluation of the mucosal folds and a clear distinction between potenziare laccuratezza nellidentificazione dellispessimento focale ( spesso correlato allinfiltrazione tumorale ) ; daltra parte una vescica scarsamente distesa ( < 250 ml ) coincide con una scarsa delineazione del profilo mucoso e con una parete ispessita complicando lindividuazione di processi patologici in questa sede . alcune considerazioni di ordine tecnico riguardano la breve durata della scansione ( 3 , 5 s ) che non ha influenzato la qualit dellimmagine , con artefatti da movimento . 
il gradiente dattenuazione ottimale realizzato fra il lume vescicale dilatato dallaria ed il tessuto molle circostante ha permesso sia una riduzione significativa delle correnti del tubo sia dei valori desposizione alle radiazioni , specie se comparati ad altri studi [ 13 , 14 , 27 ]  . 
lutilizzo di un tomografo dultima generazione multistrato a 64 detettori ( 64mdct ) , in associazione con un protocollo ad alta risoluzione con bassi valori di spessore della fetta ( slice thickness 1 mm ) , di collimazione ( 0 , 6 mm ) ed incremento di ricostruzione ( 0 , 4 mm ) , ha permesso in pochi secondi unesplorazione diagnostica precisa e ad alta risoluzione dellintera regione dinteresse , offrendo una affidabile visione specifica per lidentificazione delle lesioni . 
daltra parte , lalta risoluzione spaziale ottenuta attraverso luso di questo protocollo a strato sottile ha determinato un aumento considerevole del numero di immagini e incrementato drammaticamente il numero di dati acquisiti ; si rende quindi necessario lutilizzo di una workstation dedicata per una gestione efficiente dei dati e per la ricostruzione delle immagini . 
le immagini della ctc , invece , sono state valutate insieme alle ricostruzioni mpr poich ci ha permesso non solo una valutazione delle immagini secondo un piano assiale ma anche una visualizzazione multidimensionale ed esatta ( sagittale , coronale ed obliqua )  . 
fra le diverse tecniche 3d disponibili , abbiamo scelto la cv per la relativa familiarit dutilizzo fra i radiologi che si occupano di endoscopia virtuale , per il largo consenso tra clinici e chirurghi dovuto ad immagini che offrono una visione endoscopica sostanzialmente sovrapponibile a quella in vivo , ma soprattutto , per la migliore qualit delle immagini segnalata in differenti studi [ 2 , 28 ]  . il contributo dellapproccio tridimensionale stato fondamentale poich non solo ha dimostrato tutte le lesioni evidenziate nelle immagini 2d , ma servita come modalit diagnostica in casi di lesioni in soggetti con vescica scarsamente distesa e in due pazienti con mucosa irregolare ed ipertrofica . 
in questi ultimi casi , la ctc non ha propriamente distinto pliche di una mucosa ipertrofica da lesioni peduncolate , mentre la cv ha permesso la corretta valutazione della superficie mucosa plicale e ha chiaramente distinto le lesioni dai tessuti circostanti . 
daltra parte , la cv ha reso possibile per lo studio del collo vescicale , la parete anteriore e , se presenti , i diverticoli vescicali , i quali sono siti scarsamente o per niente accessibili alla cistoscopia convenzionale [ 17 ]  . 
 la ctc e la cv , rispetto alla cistoscopia convenzionale , offrono una minore invasivit consentendo , oltre che la visualizzazione diretta della lesione , la possibilit di misuradiol med ( 2009 ) 113 : 5269 lesions and surrounding tissues . 
moreover , vc allowed detailed inspection of the bladder neck , anterior wall and vesical diverticula , all sites that are recognised as potential blind spots at conventional cystoscopy [ 17 ]  . 
 in comparison with conventional cystoscopy , ctc and vc are less invasive and , in addition to depicting lesions directly , allow precise measurement of lesion size and evaluation of wall thickness . 
the main disadvantages of vc include the inability to perform endoscopic resections or biopsies and acquire in vivo information about the colour and structure of the mucosa , as reported by others [ 2931 ] ; the latter limitation may affect detection rates in flat lesions [ 5 ] , although we were unable to verify this owing to the lack of flat lesions in our series . 
however , the advent of technologically advanced scanners has in part overcome this problem , as radiation doses can be reduced by using the dose - modulation software ( care dose ) supplied with the scanning equipment . 
ctc combined with vc can , however , be used in cases in which conventional cystoscopy is contraindicated or difficult to perform and in the follow - up of patients after surgery . 
in such cases , should vc prove negative , the technique could spare the patient further conventional cystoscopy studies or provide the clinician and endoscopist with basic indications regarding bladder - wall morphology . 
 conclusions ctc combined with vc , performed with 64 - detector - row ct , provides a high level of diagnostic accuracy in detecting both new and recurrent locoregional vesical lesions ranging from 2 mm to 9 mm in size . 
the two approaches ( 2d and 3d ) are complementary , and in some cases , 3d images are absolutely necessary for the diagnosis . evaluation of lesions < 5 mm requires meticulous patient preparation , especially with regard to bladder distension . 
 our study should , however , be considered a preliminary experience owing to the small number of patients examined . further studies with state - of - the - art multidetector equipment need to be conducted on larger and more homogeneous patient populations to achieve higher statistical power . rare esattamente le dimensioni della lesione e di valutare lo spessore della parete vescicale , senza trascurare che lutilizzo delle immagini 2d permette una valutazione dellestensione loco - regionale della malattia . 
ulteriori vantaggi sono rappresentati dalla possibilit di ottenere una visione corretta del lume vescicale in tutti i pazienti , anche in quelli con ostruzione uretrale severa o ematuria . gli svantaggi principali della cistoscopia virtuale sono rappresentati dallincapacit di effettuare resezioni per via endoscopica o biopsie , dallimpossibilit di ottenere informazioni in - vivo in relazione al colore e alla struttura del mucosa , come riportato in altri studi [ 2931 ] : questo limite pu sicuramente influenzare la percentuale dindividuazione di lesioni piatte [ 5 ] anche se nella nostra esperienza non abbiamo potuto constatarlo per lassenza di lesioni di questo tipo nella popolazione studiata . 
infine rimane il problema dellesposizione a radiazioni ionizzanti ; questultimo svantaggio stato parzialmente superato con lutilizzo di moderne apparecchiature , in cui si ha una minor dosaggio di radiazioni , grazie allutilizzo di protocolli con moderne tecniche di care - dose presenti nelle apparecchiature di tecnologia avanzata . 
 attualmente non possiamo offrire una sensibilit del 100% nellidentificazione delle neoplasie della vescica e di conseguenza non possiamo proporre lendoscopia virtuale in sostituzione del metodo endoscopico convenzionale ; tuttavia la metodica ctc , insieme alla cv , possono essere utilizzate a nostro avviso nei casi in cui la cistoscopia convenzionale risulti controindicata o difficile da eseguire e nel follow - up dei pazienti neoplasia post - chirurgici . 
 conclusioni in conclusione , la ctc in combinazione con la cv , con tc spirale multistrato a 64 detettori ( 64 - mdtc ) , rappresenta una metodica di imaging ad elevato livello di accuratezza diagnostica per lidentificazione sia di lesioni di nuova insorgenza che di recidive vescicali locoregionali di dimensioni comprese tra 2 mm e 9 m entrambi gli approcci ( 2d e 3d ) risultano complementari e , in alcuni casi , le immagini 3d sono assolutamente necessarie per la diagnosi . 
benzi 10 , 16132 genova , italy 2department of radiology , university of california san diego ( ucsd ) , san diego , ca , usa 3dipartimento di radiodiagnostica , az . 
it is thus important to recognise common abdominopelvic mr imaging artefacts and know how to choose protocols and modify scan parameters to eliminate or at least minimise themany mr artefacts , on the other hand , provide diagnostically useful information about the underlying tissue , and many powerful mr sequences , such as in - phase or out - of - phase gradient - recalled - echo ( gre ) sequences , may be thought of as imaging artefacts applied creatively . 
to distinguish friend from foe mr artefacts or to convert foes into friends , mr radiologists must recognise and understand the physical basis of such artefacts to take advantage of them for diagnostic purposes . riassunto gli artefatti rappresentano un problema comune a tutte le metodiche di imaging . 
molti artefatti , daltra parte , consentono di ottenere informazioni diagnostiche aggiuntive e alcune sequenze , come ad esempio le gradient - echo ( gre ) in fase e in opposizione di fase , possono essere pensate come artefatti applicati creativamente allimaging clinico . 
per poterli definire amici o nemici , o poterli convertire da svantaggiosi a utili , bisogna conoscerne le basi fisiche in modo da trarre dagli artefatti il potenziale vantaggio diagnostico aggiuntivo . keywords artifacts magnetic resonance body imaging parole chiave artefatti risonanza magnetica body imaging introduction introduzione imaging artefacts are common in magnetic resonance imaging ( mri ) studies of the abdomen and pelvis . 
there are many sources of artefacts in mri [ 14 ] , which can be summarised as follows : gli artefatti sono significativamente presenti negli studi rm di addome e pelvi . 
therefore , it is important to recognise common abdominopelvic mri artefacts and know how to eliminate or at least minimise theon the other hand , many mr artefacts yield diagnostically useful information , and some powerful mr sequences , such as in - phase and opposed - phased ( or out - of - phase ) gradient - recalled - echo ( gre ) imaging , may be thought of as imaging artefacts applied creatively . to distinguish friend from foe mr artefacts or to convert foes into friends , mr radiologists must recognise and understand the physical bases of artefacts to take advantage of them for diagnostic purposes . 
of these many mr artefacts , in this article , we focus on those that can be friends as well as foes in other words , those related to ( 1 ) chemical shift , ( 2 ) magnetic susceptibility , ( 3 ) motion , or ghosts and ( 4 ) flow . 
inoltre alcune sequenze , come ad esempio le gradient - echo ( gre ) in fase ( if ) e in opposizione di fase ( of ) , possono essere pensate come artefatti applicati creativamente allimaging clinico . per poterli definire amici o nemici , o poterli convertire da svantaggiosi a utili , bisogna conoscerne le basi fisiche per trarre dagli artefatti il potenziale vantaggio diagnostico aggiuntivo . 
altre condizioni particolari sono rappresentate dalluso di tecniche di imaging parallelo e dagli effetti di alcuni artefatti su esami di addome e pelvi effettuati con le pi recenti apparecchiature rm a 3 t . chemical shift chemical shift cs artefacts are due to the phenomenon whereby protons from different molecules precess at slightly different frequencies [ 14 ]  . 
in particular , the hydrogen protons in fat and h2o have slightly different precessional frequencies , and the protons in h2o precess faster than do those in fat . this difference in precessional frequency is directly proportional to the main magnetic field strength and has been measured as approximately 3.5 ppm , resulting in a difference of only 73 hz at 0.5 t , about 225 hz at 1.5 t and about 450 hz at 3 t [ 1 , 5 , 6 ]  . 
it is seen only in the frequency - encoding axis and occurs in all sequences spin echo ( se ) or in - phase or opposed - phase gre imaging . 
as the hydrogen protons in h2o precess faster than those in fat , anywhere gli artefatti da chemical shift ( cs ) si basano sul principio che i protoni di molecole differenti precessano a frequenze differenti [ 14 ]  . 
i protoni di idrogeno contenuti nellh2o e nelle molecole di grasso , in particolare , presentano frequenze di precessione lievemente diverse e , in realt , i protoni contenuti nellh2o sono pi veloci rispetto a quelli delle molecole di grasso . 
quello di 1 tipo dovuto a misregistrazione spaziale del segnale , si ha solamente nella direzione della codifica di frequenza , ed comune a tutte le sequenze sia ad echo di spin ( spin - echo , se ) che ad eco di gradiente ( gradient - echo , gre ) , queste ultime tanto con tempi di radiol med ( 2009 ) 114 : 1831 fig . 
this kind of artefact occurs at the interface of water and fat ( arrows ) , where a bright band towards the lower frequencies and a dark band towards the higher frequencies are visible . 
1a , b chemical - shift di 1 tipo . questo tipo di artefatto , alla interfaccia acqua / grasso ( frecce ) , si manifesta come banda di iperintensit alle frequenze pi basse e di ipontensit a quelle pi alte . 
 presente nella sola direzione della codifica di frequenza ed comune a tutte le sequenze , sia ad eco di gradiente ( a ) che ad eco di spin ( b )  . 
the first kind of cs artefact depends on several factors but mainly on magnetic field strength ( b0 ) , frequency range [ bandwidth ( bw ) ] and on pixel size ( matrix )  . 
it occurs in either phaseor frequency - encoding direction and only at specific tes in gre sequences , termed opposed phase or out of phase , when the fat and water spins will be 180 out of phase with consequent signal dropout . 
il cs di 1 tipo dipende da diversi fattori ma in particolare dal campo magnetico esterno ( b0 ) , dal range di frequenze ( bandwidth , bw ) e dalla dimensione del pixel ( matrice )  . 
questo tipo di artefatto , quindi , tanto maggiore quanto maggiore lintensit del campo magnetico ( 3 t > > 1 , 5 t > > 0 , 5 t ) , quanto pi basso il bw selezionato . 
si ha sia nella direzione della codifica di frequenza che di fase , soltanto alle sequenze gre con specifici te definite in opposizione di fase ( of ) ai quali gli spin di acqua e grasso si troveranno in opposizione di fase di 180 , con successiva cancellazione e caduta di segnale . 
the second kind of cs occurs in both the phaseor frequency - encoding direction ( arrows ) only at specific echo times in opposed - phase gradient - recalled echo ( gre ) sequences as a dark band of signal dropout around organs surrounded by fat ( india ink appearance )  . 
questo tipo di artefatto , comune alle sole sequenze gre in opposizione di fase ( of ) , apprezzabile sia nella direzione della codifica di fase che di frequenza ( frecce ) come banda scura intorno agli organi circondati da grasso ( india ink )  . 
potential solutions are , again , to use fat - suppression techniques ( if there is no signal from fat , there can be no cs ) , increase the bw [ with decreasing of signal - to - noise ratio ( snr ) ] and obviously to use a specific te for in - phase imaging . protoni di acqua e grasso sono if a 4 , 4 ms , 8 , 8 ms , e cos via , e sono in of a 2 , 2 ms , 6 , 6 ms , e cos via , e si trovano ciclicamente in fase e in opposizione di fase approssimativamente ogni 2 , 2 ms . 
quindi , ove acqua ( h2o ) e grasso ( tessuti contenenti gruppi - ch , - ch2 e - ch3 come colesterolo e precursori degli acidi grassi ) siano presenti radiol med ( 2009 ) 114 : 1831 fig . 
questo tipo di artefatto , visualizzabile alle sole sequenze gre in of come india ink artifact ( frecce , b ) , consente di diagnosticare con facilit condizioni di steatosi epatica ( si noti la omogenea caduta di segnale del parenchima epatico alle sequenze in of rispetto a quelle if )  . magnetic susceptibility the magnetic susceptibility ( ) of all substances is a measure of how magnetised they become when placed in a magnetic field [ 14 ]  . 
local heterogeneity of the magnetic field causes protons to precess at different frequencies than they normally would , and because of this , the protons are mapped to the incorrect location in the frequency - encoding direction . 
 there are three types of substances , each with different magnetic susceptibility , commonly dealt with in mri : ( 1 ) diamagnetic , ( 2 ) paramagnetic , ( 3 ) ferromagnetic . 
possibili rimedi al cs di 2 tipo sono rappresentati anche in questo caso dallutilizzo di sequenze fat suppression , dallincremento del bw ( con conseguente riduzione del snr ! ) e , ovviamente , dallutilizzo di appropriati te in cui acqua e grasso siano in fase . suscettibilit magnetica la suscettibilit magnetica ( ) di una sostanza la misura di quanto viene magnetizzata questa sostanza una volta posta allinterno di un campo magnetico [ 14 ]  . 
gli artefatti da suscettibilit si hanno qualora tessuti o materiali con differente siano adiacenti tra loro , causando in tal modo disomogeneit del campo magnetico locale . quindi questo fenomeno si ha alle interfacce tra tessuti e aria , tessuti e metalli oppure tessuti e sangue . 
allinterfaccia tra tessuti e aria presente nelle anse intestinali si ha distorsione dellanatomia con vuoto di segnale ( frecce , a e b ) e disomogenea soppressione del segnale del grasso ( freccia curva , b )  . strongly attracted by a magnetic field and have a large positive  . 
they can be seen only in the phase - encoding direction , mainly for a nellimaging a rm si ha a che fare con tre tipi di sostanze , ciascuna con una differente suscettibilit magnetica : diamagnetiche ; paramagnetiche ; ferromagnetiche . 
nonostante le sequenze se e tse siano meno sensibili di quelle gre , leffetto di suscettibilit magnetica comune comunque a tutte le sequenze [ 1 , 11 , 12 ]  . 
la maggior entit dellartefatto alle sequenze gre con te pi alto ( freccia , a ) , rispetto a quella con te pi basso ( b ) , prova la presenza di depositi di ferro ( emosiderinici ) nel parenchima splenico . significant asymmetry in the data space between frequency encoding ( on the order of milliseconds ) and a single phaseencoding step ( in order of seconds )  . 
ghosts are spaced equally , and this spacing depends only on repetition time tica , inoltre , aumenta allaumentare del te utilizzato e questa peculiarit pu rappresentare una fonte di preziose informazioni diagnostiche aggiuntive su particolari materiali o strutture che a volte sono difficili da identificare radiol med ( 2009 ) 114 : 1831 fig . 
for instance , ascites can appear to be peritoneal carcinomatosis , and in mr cholangiopancreatography ( mrcp ) , a flow void in the common bile duct can mimic a stone . 
si propagano solamente nella direzione della codifica di fase , soprattutto per lasimmetrica codifica spaziale dei dati tra la frequenza ( che nellordine di millisecondi ) e la fase ( nellordine invece di secondi )  . 
ad esempio lartefatto da pulsazione in un vaso indica la perviet del vaso stesso anche in assenza del signal void . possibili soluzioni sono rappresentate dal cambio di direzione di fase / frequenza ( lartefatto cambia solo direzione e la risoluzione peggiorata ) , dalluso di bande di presaturazione prossimali ai vasi o applicate sulla parete addominale , dalluso di tecniche di gating cardiaco e / o respiratorio , dalla somministrazione di gadolinio ev ( che accorcia il tempo di rilassamento t1 ) , o dalla sedazione del paziente ( uso pediatrico )  . 
lutilizzo di tecniche single - shot ( ssh ) ( b ) consente di eliminare gli artefatti da movimento respiratorio presenti alla sequenza tse t2 pesata ( a )  . 
the lack of a refocusing pulse in these gre sequences is a useful property that allows this artefact to be avoided . parallel imaging technique parallel imaging is a family of techniques developed shortly after the introduction of phased - array coils in order to reduce acquisition times by taking advantage of the spatial information inherent in multiple radiofrequency coils . 
in particolare nei pazienti non collaboranti consigliabile lutilizzo di sequenze gradient echo 2d con tempo di interpulso ( tipo turbo flash o turbo field echo ) per limaging t1 pree post - contrasto , meno sensibili a questo tipo di artefatti rispetto a quelle 3d . da flusso il flusso dei liquidi ( ascite , liquido amniotico , liquor cefalorachidiano , bile ) causa defasamento dei protoni che , alle sequenze ad eco di spin , si traduce in vuoti di segnale che possono anche mimare delle pseudomasse . 
nei pazienti con ascite , ad esempio , pu apparire come possibile carcinosi peritoneale , e negli studi di colangiopancreatografia a rm il vuoto di flusso nel coledoco pu mimare un calcolo . 
come possibile utilit clinica la perdita del flow void in un vaso , con conseguente iperintensit dello stesso alle immagini t1 pesate pre - contrasto , pu indicare la presenza di un trombo . 
 imaging parallelo limaging parallelo un insieme di tecniche che richiede luso di bobine multicanale ( phased array ) sviluppato relativamente di recente , e che comprende la tecnica smash ( simultaneous acquisition of spatial harmonics ) , asset ( array spatial sensitivity encoding technique ) e sense ( sensitivit encoding ) [ 1318 ]  . 
tale tecnica incrementa la velocit di acquisizione di un fattore ( di accelerazione ) da 1 , 5 a 3 ed oltre sulla maggior parte delle moderne apparecchiature disponibili in commercio [ 13 , 19 ]  . 
 particolarmente utile negli studi cardiaci e di addome - pelvi , dove lapnea frequentemente richiesta al paziente , e la stessa capacit di apnea critica in termini di qualit dellimmagine . 
liquid flow causes proton dephasing and signal loss on spin - echo ( se ) imaging [ such as half - fourier acquisition single - shot turbo spin echo ( haste ) ] ( a ) , which creates pseudomasses ( arrows )  . 
con sequenze ad eco di spin ( come le haste ) ( a ) il defasamento dei protoni allinterno del liquido ascitico crea vuoti di segnale che possono mimare delle pseudomasse ( frecce )  . 
le sequenze ultraveloci ad eco di gradiente , come le fisp ( b ) , non risentono invece di questo artefatto . simultaneous acquisition of spatial harmonics ( smash ) , sensitivity encoding ( sense ) and array spatial sensitivity encoding technique ( asset ) [ 1318 ]  . 
likewise , tse and single - shot fast se sequences can be improved by reducing echo train lengths [ etl , or turbo factor ( tf ) ] and thereby diminishing image blurring . 
if the calibration acquisition does not include a region that is subsequently imaged in the parallel acquisition , this region cannot be reconstructed , and a void will appear in the image . bile incrementare la risoluzione spaziale ; oppure , per le sequenze tse e single - shot fast se , possibile ridurre il blurring dellimmagine riducendo la lunghezza del treno di echi ( etl , o turbo factor [ tf ] )  . 
limaging parallelo altamente flessibile e virtualmente adattabile a qualsiasi sequenza [ 13 ]  . anche limaging parallelo risente di diversi artefatti . molti di essi possono essere eliminati grazie a una attenta cura della tecnica , mentre alcuni rimangono di fatto inevitabili [ 19 ]  . 
tuttavia le pi recenti tecniche di imaging parallelo , msense e grappa ( generalized autocalibrating partially parallel acquisition ) , effettuano una autocalibrazione durante ogni acquisizione per ridurre al minimo questo tipo di artefatti . 
spoiled - gradient - recalled - echo ( gre ) image through the liver with image - based parallel imaging algorithm ( acceleration factor of 2 ) is degraded by incomplete phase unwrapping ( left )  . 
immagine gre assiale del fegato ( a sinistra ) ottenuta con imaging parallelo ( fattore di accelerazione 2 ) che presenta artefatti da ribaltamento lungo lasse delle fasi ; notare sia la presenza di artefatti dovuti allaliasing anteriormente e posteriormente , che quella di una banda di basso rapporto segnale / rumore al centro dellimmagine . 
nellimmagine ripetuta dopo avere adeguatamente incrementato il campo di vista ( a destra ) , la decodifica spaziale lungo lasse delle fasi avviene correttamente e gli artefatti sono quindi eliminati . however , the most recent parallel imaging techniques , msense and generalised autocalibrating partially parallel acquisition ( grappa ) , perform an autocalibration during each acquisition in order to minimise this kind of artefact . artefacts may also appear when the field of view ( fov ) is too small in the parallel acquisition . 
unfortunately , although ultrahigh - field 3.0 - t systems have already been shown to be advantageous for brain and musculoskeletal imaging , only a few published reports have described the use of these systems in the abdomen and pelvis [ 5 , 2224 ]  . 
per diverse ragioni , per , il reale guadagno a 3 , 0 t , se confrontato con un sistema a 1 , 5 t , inferiore al fattore 2 teoricamente aspettato [ 5 , 22 ]  . 
nonostante i sistemi a 3 , 0 t abbiano dimostrato di essere vantaggiosi per limaging neurologico e muscoloscheletrico , sono ancora poche le esperienze riportate in letteratura riguardanti luso e i vantaggi di queste apparecchiature nello studio di addome e pelvi [ 5 , 2224 ]  . 
nellimaging addominale , le sequenze , la dimensione degli organi in esame e alcuni tipi di artefatto , sono significativamente diversi da quelli caratteristici dellimaging muscoloscheletrico o neurologico [ 523 ]  . il chemical shift ( cs ) di primo tipo a 3 , 0 t risulta ampio il doppio rispetto a 1 , 5 t ( tenuti costanti fov , bw , e risoluzione di base ) , ma in genere questo artefatto non rappresenta un problema clinicamente rilevante . 
immagini gre in fase e in opposizione di fase ottenute a 1 , 5 ( in alto ) e 3 t ( in basso ) in paziente portatore di clip metallica vicino allilo epatico . 
si noti anche la dipendenza dal te che in questo caso maggiore nellimmagine in fase a 1 , 5 t e in quella in opposizione di fase a 3 t . organ size and some artefacts differ significantly in abdominal imaging . 
questa maggior differenza in frequenza di risonanza tra acqua e grasso a 3 , 0 t permette una miglior separazione dei loro picchi durante esami di spettroscopia a rm , e consente una migliore e pi rapida tecnica di soppressione del segnale del grasso [ 5 ]  . gli artefatti da suscettibilit magnetica aumentano con il campo magnetico , e a 3 , 0 t presentano un volume circa il doppio rispetto a 1 , 5 t . 
la colografia a rm infatti di sicuro pi critica a 3 , 0 t . importante sottolineare che dispositivi metallici considerati sicuri a intensit di campo magnetico di 1 , 5 t non lo radiol med ( 2009 ) 114 : 1831 fig . 
coronal turbo - spin - echo ( tse ) ( left ) and gradient - recalledecho ( gre ) ( right ) images obtained at 3 t in a patient with a large ascites . 
i cosiddetti effetti dielettrici ( standing wave effect e conductivity artifact ) determinano forti variazioni di segnale in regioni corporee lontane dalla bobina di ricezione , con aree ipointense e buchi neri . 
the so - called standing - wave effect and conductivity artefact result in strong signal variations , especially brightening or dark holes in regions away from the receive coils , and in hypointense areas in the image where the radiofrequency field is partially attenuated [ 5 , 31 ]  . 
 conclusions imaging artefacts are common in mr and can cause image degradation , so it is important to recognise abdominopelvic mri artefacts and know how to eliminate or at least minimise the on the other hand , many mr artefacts provide a diagnostically useful tool and may be thought of as imaging artefacts applied creatively . 
mr radiologists must recognise and understand the physical bases of artefacts in order to be able to modify scan parameters to modulate the detrimental effect of artefacts and take advantage of them for diagnostic purposes . sono necessariamente a 3 , 0 t [ 5 ] , e tutti questi dispositivi necessitano di unattenta valutazione prima di sottoporre il paziente ad esame rm su alto campo [ 2530 ]  . alcuni artefatti , correlati alle pi alte frequenze trasmesse , e non presenti a 1 , 5 t , sono nuovi e peculiari a 3 , 0 t . 
i cosiddetti effetti dielettrici ( standing wave effect e conductivity artifact ) determinano infatti forti variazioni di segnale in regioni corporee particolarmente lontane dalla bobina di ricezione , con aree ipointense laddove il campo di rf risulti parzialmente attenuato [ 5 , 31 ]  . 
infatti per tali effetti degradanti sulle immagini , oltre che per concetti di tipo protezionistico , studi di rm fetale non dovrebbero essere eseguiti a 3 , 0 t [ 5 ]  . conclusioni i comuni artefatti presenti alle indagini di rm possono presentare un effetto degradante sulle immagini , quindi importante saperli riconoscere e possedere gli strumenti per eliminarli o ridurli al minimo . 
signal intensity values were significantly higher for splenic grafts , starting from 40 s after microbubble administration . starting from 90 s after injection , there was no overlapping between enhancement of splenic grafts and peritoneal metastases , and only splenic grafts showed a percent of enhancement higher than 60% of the maximum enhancement . 
sono stati valutati con ecocontrastografia 13 pazienti consecutivi con splenosi peritoneale e 13 con metastasi peritoneali iniettando 2 , 4 ml di sonovue ed osservando lenhancement delle lesioni in tempo reale per 240 s . 
a partire da 90 secondi dopo liniezione non vi era sovrapposizione tra i valori di enhancement degli impianti e delle metastasi , e solo i noduli splenici presentavano un enhancement maggiore del 60% del massimo enhancement . 
 radiol med ( 2009 ) 114 : 4251 considered a valuable alternative to scintigraphy for characterising peritoneal splenic grafts without radiation . keywords spleen us techniques splenosis ultrasound ( us ) contrast media conclusioni . 
lecocontrastografia dopo iniezione di sonovue consente la diagnosi differenziale tra isole di splenosi e metastasi peritoneali . parole chiave milza tecniche ecografiche splenosi ecocontrastografia mezzi di contrasto ecografici introduction introduzione contrary to other microbubble contrast agents , sonovue does not accumulate in the liver or in other organs but is characterised by exclusive spleen - specific uptake [ 1 ]  . 
this characteristic has been demonstrated for the native spleen in which spleen - specific enhancement has been observed for more than 5 min , a time longer than the blood - pool phase [ 1 , 2 ]  . 
spleen - specific uptake has been shown to be useful for characterising ectopic splenic tissue around the spleen [ 2 , 3 ] , in the pancreatic tail [ 4 , 5 ] and within the liver [ 6 ]  . splenosis represents the autotransplantation of splenic tissue after splenic trauma or surgery [ 7 ]  . 
the incidence of splenosis has recently risen following the increasing use of laparoscopic splenectomy [ 8 ] , and splenic autotransplantation in omental pouches is used during splenectomy by some surgeons in an attempt to increase the immune response to infection and prevent overwhelming postsplenectomy sepsis [ 911 ]  . whereas in most cases peritoneal splenosis causes no symptoms and is discovered incidentally during imaging studies performed for other reasons , in a small proportion of cases , it is symptomatic and should be considered in the differential diagnosis of previously splenectomised patients who present with unexplained abdominal masses [ 7 , 12 ] or occult bleeding [ 13 ]  . 
 the purpose of this study was to assess whether the differential diagnosis between peritoneal splenic implants and metastatic deposits can be obtained with contrastenhanced ultrasonography ( ceus ) after sonovue injection , based on the enhancement characteristics during the spleenspecific phase . materials and methods sonovue , contrariamente ad altri mezzi di contrasto ecografici , non si accumula nel fegato e in altri organi , ma presenta un accumulo specifico nel tessuto splenico [ 1 ]  . questo comportamento caratteristico stato dimostrato nella milza nativa nella quale laccumulo specifico delle microbolle consente di rilevarne il segnale per pi di 5 minuti , un tempo pi lungo della fase vascolare [ 1 , 2 ]  . 
 stato dimostrato che laccumulo spleno - specifico utile per la caratterizzazione di tessuto splenico ectopico intorno alla milza [ 2 , 3 ] , nella coda del pancreas [ 4 , 5 ] e nel contesto del parenchima epatico [ 6 ]  . la splenosi lautotrapianto di tessuto splenico che si verifica dopo traumi o chirurgia a carico della milza [ 7 ]  . 
lincidenza di splenosi recentemente aumentata in seguito al ricorso sempre pi frequente alla splenectomia laparoscopica [ 8 ] e per il fatto che alcuni chirurghi , durante lintervento di splenectomia , sono soliti trapiantare frammenti di tessuto splenico allinterno di tasche omentali nel tentativo di migliorare la risposta immunitaria alle infezioni e prevenire linsorgenza di sepsi post - splenectomia [ 911 ]  . nella maggior parte dei casi la splenosi peritoneale asintomatica , individuata accidentalmente durante procedure di imaging eseguite per altre ragioni ; in alcuni casi , tuttavia , pu essere sintomatica . 
opportuno , in particolare , considerare questa possibilit nella diagnosi differenziale dei pazienti precedentemente sottoposti a splenectomia che giungono allosservazione per la caratterizzazione di tumefazioni addominali [ 7 , 12 ] o sanguinamento occulto [ 13 ]  . 
 lo scopo di questo studio valutare se lecocontrastografia dopo iniezione di sonovue consente la diagnosi differenziale tra metastasi peritoneali e impianti peritoneali di tessuto splenico sulla base delle caratteristiche di enhancement in fase spleno - specifica . ceus was performed on 13 consecutive patients who had undergone splenectomy with spontaneous ( n = 2 ) or surgically implanted ( n = 11 ) peritoneal splenic grafts and 13 consecutive patients with peritoneal metastases that developed from different primary sites ( table 1 )  . 
scintigraphy materiali e metodi sono stati studiati con ecocontrastografia 13 pazienti consecutivi con pregressa splenectomia e impianti splenici radiol med ( 2009 ) 114 : 4251 table 1 primary malignancies of patients with peritoneal metastases malignancy no . 
of patients lung cancer pancreatic cancer gastric cancer colonic cancer ovary cancer gallbladder cancer hepatocellular carcinoma carcinoma del polmone carcinoma del pancreas carcinoma gastrico carcinoma del colon carcinoma ovarico carcinoma della colecisti epatocarcinoma tabella 1 neoplasie primitive dei pazienti con metastasi peritoneali neoplasia n di pazienti was performed to confirm the splenic nature of the peritoneal nodules identified in the patients with spontaneous and surgically implanted grafts . 
diagnosis of peritoneal metastases was confirmed with biopsy ( n = 3 ) or postmortem histological confirmation and by documenting disease progression during the follow - up . all examinations were carried out by the same sonologist ( mb ) on an hdi 5000 system ( atl , bothell , wa , usa )  . grey - scale ultrasound ( us ) and color doppler interrogation were performed with a 25 mhz convex probe and a 512 mhz linear probe , and ceus with a 25 mhz convex probe . 
to avoid bias in the retrospective evaluation of nodules , care was taken to avoid visualising ascites , which was present in 8 / 26 patients , within the images . 
digital cine clips were recorded during the entire contrast examinations and stored for offline retrospective analysis . a reader who did not perform the us examinations ( gc ) peritoneali spontanei ( n = 2 ) o chirurgici ( n = 11 ) e 13 pazienti consecutivi con metastasi peritoneali da tumori di diversi organi ( tabella 1 )  . 
la natura splenica dei noduli identificati nei pazienti con impianti splenici peritoneali spontanei o chirurgici stata confermata con la scintigrafia ottenuta eseguendo scansioni delladdome in proiezione anteriore , posteriore e laterale destra 20 minuti dopo liniezione endovenosa di 45 mci di tecnezio - 99m solfuro colloidale . 
la diagnosi di metastasi peritoneali stata confermata alla biopsia ( n = 3 ) o allautopsia e documentando durante il follow - up del paziente la progressione della malattia . tutti gli esami sono stati eseguiti dallo stesso operatore ( m.b. ) utilizzando un ecografo hdi 5000 ( atl , bothell , wa , usa )  . 
per lecografia in scala dei grigi e per lecocolor doppler sono stati utilizzati un trasduttore convex da 25 mhz ed un trasduttore lineare da 512 mhz ; per lecocontrastografia stato utilizzato un trasduttore da 25 mhz . 
lenhancement stato valutato utilizzando una tecnica contrastospecifica non distruttiva ( pulse inversion harmonic imaging , atl , bothell , usa ; indice meccanico 0 , 09 )  . lenhancement stato valutato in tempo reale dal tempo delliniezione del contrasto fino a oltre 4 minuti dopo liniezione . 
 i filmati digitali sono stati processati da un operatore differente da quello che aveva eseguito gli esami ecografici ( g.c. ) e che non era a conoscenza della natura dei noduli . sono state selezionate immagini a intervalli temporali compresi tra il momento delliniezione del contrasto e 4 minuti dopo liniezione ( 0 , 10 , 20 , 30 , 40 , 60 , 90 , 120 , 150 , 180 , 210 , 240 secondi dopo liniezione del contrasto )  . 
lintensit media del segnale stata valutata in tutte le immagini selezionate in unit di intensit video ( viu , range : 0255 ) misurando il livello di grigio medio nellistogramma in una regione dinteresse comprendente lintero nodulo . 
 la forma dei noduli stata valutata misurando sulla stessa immagine ecografica il massimo diametro longitudinale ( l ) e il minimo diametro trasverso ( t ) e calcolando il rapporto l / t [ 14 ]  . 
frames were selected at different time intervals ranging from the time of injection to 4 min after injection ( 0 , 10 , 20 , 30 , 40 , 60 , 90 , 120 , 150 , 180 , 210 , 240 s after microbubble injection )  . 
frames were saved as 8 - bit grey - scale images and stored in tiff format . average signal intensity was evaluated in all selected images in video intensity units ( viu , range : 0255 ) using commercially available software ( adobe photoshop cs2 version 9.0 ) by measuring the average grey level in the histogram in a region of interest encompassing the entire nodule . the shape of each nodule was assessed by measuring the largest longitudinal ( l ) and smallest transverse ( t ) diameters on the same us scan and by calculating the l / t ratio [ 14 ]  . 
to obtain a parameter independent of the variability of lesion enhancement deriving from the type and settings of the equipment used , patient characteristics and lesion depth , the percent rate between the signal intensity and the maximum signal intensity reached by the nodule was calculated using the formula ( sit / simax ) 100 , where sit is enhancement at time t , i.e signal intensity at time t after subtraction of signal intensity at time 0 , which was considered as background intensity , and simax is the maximum enhancement reached by the nodule from the time of injection to 4 min after injection . 
to assess interobserver variability , 45 images were randomly selected and enhancement evaluated by two independent readers ( gc and rz ) , as previously described . statistical analysis was performed with commercially available software ( graphpad prism version 4.00 for windows , graphpad software , san diego , ca , usa )  . differences between the l / t ratio , volume , and enhancement of the splenic nodules and of peritoneal metastases were evaluated using the mannwhitney test . 
probability p values of p < 0.05 were considered statistically significant . results at the time of the ceus examination 3 / 13 patients with peritoneal metastatic disease presented with liver metastases . 
after sonovue injection , splenic grafts were characterised by strong un parametro indipendente dalla variabilit dellenhancement derivante dal tipo e dalla regolazione dellapparecchiatura utilizzata , dalle caratteristiche del paziente , e dalla profondit della lesione stato calcolato il rapporto percentuale tra lintensit di segnale e la massima intensit del segnale raggiunta dal nodulo secondo formula : ( sit / simax ) 100 , dove sit lenhancement al tempo t , cio il valore che si ottiene sottraendo allintensit del segnale al tempo t lintensit del segnale al tempo 0 , considerata come background , e simax il massimo enhancement raggiunto dal nodulo nel tempo tra linizio delliniezione e 4 minuti dopo liniezione . 
 lanalisi statistica stata condotta utilizzando un software commerciale ( graphpad prism version 4.00 per windows , graphpad software , san diego , california , usa )  . il test di mann - whitney stato impiegato per valutare le differenze tra i rapporti l / t , i volumi e lenhancement dei noduli splenici e delle metastasi peritoneali . 
non sono state rilevate differenze statisticamente significative tra il rapporto l / t dei noduli splenici scelti come target ( 1 , 790 , 31 , mediana 1 , 78 , range 1 , 192 , 33 ) e delle metastasi peritoneali ( 1 , 710 , 31 , mediana 1 , 75 , range 1 , 292 , 20 ) : le due classi di noduli presentavano pertanto forma simile . 
non sono state rilevate differenze statisticamente significative tra il volume medio dei noduli splenici ( 32 , 2730 , 27 cm3 , mediana 27 , 88 cm3 , range 5 , 43102 , 96 cm3 ) e delle metastasi ( 29 , 9424 , 78 cm3 , mediana 31 , 10 cm3 , range 2 , 6775 , 73 cm3 )  . 
the average volume of splenic nodules ( 32.2730.27 cm3 , median 27.88 cm3 , range 5.43102.96 cm3 ) and peritoneal metastases ( 29.9424.78 cm3 , median 31.10 cm3 , range 2.6775.73 cm3 ) was not significantly different . 
the rates were significantly higher for splenic grafts starting from 60 s after microbubble injection dellintensit del segnale dei noduli di tessuto splenico e delle metastasi peritoneali nei differenti intervalli di tempo . nella nostra casistica a partire da 40 secondi dopo la somministrazione delle microbolle lintensit del segnale risultata significativamente maggiore per gli impianti splenici ( test di mann - whitney , p < 0 , 001 )  . 
the range of enhancement values is reported in parentheses bp values are by mann - whitney test cno overlapping between the range of enhancement of splenic grafts and of peritoneal metastases 10 s 20 s 30 s 40 s 60 s 90 s 120 sc 150 sc 180 sc 210 sc 240 sc 10 s 20 s 30 s 40 s 60 s 90 s 120 s 150 s 180 s 210 s 240 s 10 s 20 s 30 s 40 s 60 s 90 s 120 s 150 s 180 s 210 s 240 s tabella 2 enhancement allecocontrastografia degli impianti splenici e delle metastasi peritoneali tempo dopo liniezione delle microbolle ( secondi ) impianti splenici ( viu ) a metastasi peritoneali ( viu ) a valori di pb radiol med ( 2009 ) 114 : 4251 aviu , unit di intensit video . 
signal intensity in video intensity units ( viu ) at time t after subtraction of background si in viu at time 0 ] , and simax is the maximum enhancement reached by the nodule from the time of injection to 4 min after injection . 
the range of the percent rates is reported in parentheses bp values are by mann - whitney test tabella 3 rapporto percentuale tra lenhancement degli impianti splenici e delle metastasi peritoneali tempo dopo liniezione delle microbolle ( secondi ) impianti splenicia metastasi peritonealia valori di pb ail rapporto percentuale stato calcolato secondo la formula : ( sit / simax ) 100 , dove sit lenhancement al tempo t ( cio lintensit del segnale in viu al tempo t dopo la sottrazione dellintensit del segnale al tempo 0 , considerata come background ) e simax il massimo enhancement raggiunto dal nodulo dallistante delliniezione fino a 4 minuti dopo liniezione . 
il range e i rapporti percentuali sono riportati tra parentesi bvalori di p ottenuti con il test di mann - whitney radiol med ( 2009 ) 114 : 4251 signal intensity ( viu ) fig . 
in fact , although computed tomography ( ct ) and magnetic resonance imaging ( mri ) may , in splenic implants as in the native spleen , typically show inhomogeneous enhancement in the arterial phase and persistent , homogeneous enhancement during the following vascular phases [ 17 ] , differentiation between splenic implants and metastatic deposits can be problematic in clinical practice if based on radiological imaging alone [ 7 , 12 , 18 ] , when peritoneal nodules are identified accidentally in a patient without other obvious signs of metastatic disease . superparamagnetic iron oxide ( spio ) - enhanced mri allows a confident characterisation of splenic tissue ; this technique , however , is expensive [ 17 ]  . 
whereas ultrasonography allows differentiation between accessory spleens and splenic grafts based on their shape and vascular supply [ 14 ] , morphological and colour doppler appearance of peritoneal splenic nodules and metastases are often similar because both types of nodules are oval with peripheral feeding vessels at colour doppler interrogation . 
a variable amount of ascites is often present in patients with peritoneal metastases ( 7 / 13 patients in our series ) , whereas usually it is problema si presenta in particolare nei pazienti neoplastici quando lascite o altre lesioni secondarie non orientano nella diagnosi differenziale . 
bench la tc e la risonanza magnetica mostrino tipicamente , negli impianti splenici come nella milza nativa , enhancement disomogeneo in fase arteriosa ed enhancement omogeneo e persistente nelle successive fasi vascolari [ 17 ] , la diagnosi differenziale tra impianti splenici e metastasi peritoneali pu essere problematica nella pratica clinica sulla sola base dellimaging radiologico [ 7 , 12 , 18 ] quando i noduli peritoneali sono identificati accidentalmente in un paziente che non presenta altri chiari segni di diffusione metastatica . 
la risonanza magnetica con mezzi di contrasto superparamagnetici composti da nano - particelle di ossido di ferro ( spio ) permette una caratterizzazione accurata del tessuto splenico , questa tecnica , tuttavia , costosa [ 17 ]  . 
lecografia consente di differenziare gli impianti splenici dalle milze accessorie sulla base della morfologia e delle caratteristiche vascolari [ 14 ] , ma gli impianti splenici e le metastasi peritoneali si presentano spesso con morfologia e vascolarizzazione molto simile , cio come noduli di forma ovalare con vasi afferenti periferici . 
i pazienti con metastasi peritoneali si presentano spesso con ascite in quantit variabile ( 7 / 13 pazienti nella nostra casistica ) , mentre in genere , in assenza di complicanze , non si osserva liquido libero in addome nei pazienti con impianti di tessuto splenico . 
 il nostro studio documenta come gli impianti peritoneali di tessuto splenico , analogamente alla milza nativa [ 1 ] , mostrano un accumulo specifico di sonovue che si evidenzia come enhancement persistente per almeno 4 radiol med ( 2009 ) 114 : 4251 not recognised in patients with uncomplicated splenic peritoneal deposits . 
 as shown by our study , peritoneal splenic grafts show spleen - specific uptake after sonovue administration , as occurs for the native spleen [ 1 ] , resulting in contrast enhancement lasting at least 4 min after microbubble administration , a time longer than the blood - pool phase . 
as in our series peritoneal metastases did not present with late enhancement , irrespective of primary neoplasm , this enhancement characteristic should allow differential diagnosis between splenic nodules and metastatic deposits . 
 several limitations of our study should be mentioned . first , the ability of us to detect peritoneal lesions depends on both the skill of the operator and the characteristics of the patient . 
as signal intensity from microbubbles strongly depends on lesion depth and on the performance of the equipment used , our results cannot be generalised because a wider range of signal intensity values is expected using different us machines to image nodules at different depths . 
we believe that evaluating the percent rate between the signal intensity and the maximum signal intensity reached by the nodule could allow characterisation of peritoneal splenic nodules regardless of the equipment and lesion depth . 
bias could have affected the collection process . although the operators who retrospectively processed the digital cine clips and reviewed the images were blinded to the nature of the nodules during the evaluation process , absolute blinding was difficult to attain because the enhancement characteristics were essentially different . finally , the splenic nature of peritoneal nodules was confirmed by using 99mtc sulphur colloid scintigraphy . 
poich nella nostra casistica le metastasi peritoneali non hanno presentato enhancement tardivo , indipendentemente dal tipo di tumore primitivo , questa caratteristica sembra consentire la diagnosi differenziale tra noduli splenici e secondari . 
poich lintensit del segnale dipende fortemente dalla profondit della lesione e dalla performance dellapparecchiatura ecografica utilizzando ecografi diversi per studiare noduli posizionati a profondit differenti ci si aspetta un range pi ampio di valori di intensit di segnale . 
la valutazione del rapporto percentuale tra lintensit del segnale e la massima intensit raggiunta dal nodulo potrebbe pertanto consentire la caratterizzazione dei noduli di tessuto splenico in peritoneo indipendentemente dallapparecchiatura e dalla profondit della lesione . 
una terza limitazione del nostro studio che lenhancement delle lesioni stato valutato misurando il livello di grigio medio in unit video su immagini in scala dei grigi della profondit di 8 bit . 
misurazioni pi accurate possono essere ottenute utilizzando software dedicati progettati elettivamente per quantificare lintensit del segnale in scala lineare , prima della compressione logaritmica necessaria per la presentazione a video . 
bench gli operatori che hanno processato i filmati digitali retrospettivamente e quelli che hanno revisionato le immagini non fossero a conoscenza della natura dei noduli durante il processo di valutazione le caratteristiche di enhancement dei due tipi di noduli sono profondamente differenti ed ottenere unanalisi completamente in cieco difficile . 
questa indagine documenta la captazione del radiocolloide sia da parte del fegato che della milza , ma meno sensibile e specifica rispetto alla scintiradiol med ( 2009 ) 114 : 4251 splenic tissue but is less sensitive and specific compared with heat - damaged red - blood - cell scintigraphy , which allows imaging of the splenic tissue independently from liver [ 20 , 21 ]  . 
these preliminary data , however , need confirmation with a larger series of patients , with a variety of us equipment and contrast - specific modes . in conclusione , nella nostra casistica sonovue ha consentito la diagnosi differenziale tra impianti peritoneali di tessuto splenico e metastasi peritoneali . 
this article provides new evidence that the onset of toh related to pregnancy may occur not only in the third trimester , as described in most articles , but also early after delivery [ 2 ]  . 
to date , postpartum toh had been reported only anecdotally due to the lack of large series [ 2 ]  . most previous reports of pregnancy - related bilateral toh do not specify pain onset was synchronous for both hips or whether there was a side - to - side migration over a period of months . 
 [ 2 ] , who recently reported five patients with synchronous and bilateral pregnancy - related toh . these observations might corroborate the hypothesis that the simultaneous involvement of both hips might occur in some cases of pregnancy - related toh , but not in men , who would be more prone to develop a side - to - side migratory toh . 
lequesne [ 3 ] , in his classic description of toh in a population of ten men , found three cases of bilateral migrating involvement over a period of months , but none of them had a synchronous involvement . when it comes to the images shown in xyda et al.s article , we beg to add some comments . 
first , in the second and third case presented , the images in t1 - weighted sequences would seem to show a subtle subchondral hypointense band paralleling the articular surface . 
in toh , the detection of such subtle linear images may correspond to a epiphyseal fracture , and differentiation from an epiphyseal osteonecrosis may be challenging in some cases [ 4 ]  . 
tale articolo ha il merito di confermare che lesordio dellosteoporosi transitoria dellanca pu osservarsi non solo durante il terzo trimestre di gravidanza , come riportato classicamente in letteratura , ma anche durante il periodo post - parto [ 2 ]  . linsorgenza di unosteoporosi transitoria dellanca era stata documentata in letteratura solo a titolo aneddotico , a causa della mancanza di serie sufficientemente numerose di pazienti [ 2 ]  . 
inoltre , la maggior parte dei precedenti casi riportati di osteoporosi bilaterale dellanca , non specificano se linsorgenza della sintomatologia era sincrona per le due anche o se si trattava , piuttosto , di un quadro di dolore e di impotenza funzionale con migrazione allanca controlaterale realizzatosi nellarco di alcuni mesi . 
linsieme di queste osservazioni potrebbe corroborare lipotesi che il coinvolgimento simultaneo di entrambe le anche si osserva in alcuni casi di osteoporosi transitoria dellanca correlata alla gravidanza , mentre nella popolazione maschile , nelle forme bilaterali , si osserverebbe piuttosto un pattern di tipo migrante con interessamento successivo delle due anche . lequesne [ 3 ] , nella sua classica descrizione dellosteoporosi transitoria dellanca in una popolazione di 10 uomini , descrive 3 casi di coinvolgimento bilaterale migrante , ma nessun caso di coinvolgimento sincrono . dal punto di vista delle immagini fornite nellarticolo , ci permettiamo di aggiungere alcuni commenti . 
in primo luogo , nel caso 2 e 3 , le immagini in ponderazione t1 sembrano mostrare la presenza di una sottile immagine lineare ipointensa a topografia subcondrale , con andamento parallelo alla superficie articolare . 
la differenziazione di tali anomalie epifisarie nei confronti di unosteoneradiol med ( 2009 ) 114 : 168171 the experience of our group [ 4 ] and other authors [ 5 ] , such subchondral lines are frequently seen in toh . 
in our experience , fat suppression should be avoided because these technique obscures subchondral areas of hypointensity in t2 - weighted sequences that , if sufficiently large , are associated with a poor prognosis [ 4 ]  . in conclusion , we congratulate xyda and coworkers on their report of bilateral simultaneous toh in early postpartum , which had been only anecdotally described . 
nella nostra esperienza le sequenze ponderate in t2 senza saturazione rivestono unimportanza prognostica notevole poich la presenza di un territorio subcondrale ipointenso in t2 , di dimensioni sufficientemente estese associata ad una peggior prognosi [ 4 ]  . in conclusione , ci congratuliamo con il xyda et al . per la descrizione di tre casi di osteoporosi transitoria bilaterale dellanca la cui descrizione in letteratura era solo aneddotica . 
cardarelli , via antonio cardarelli 9 , 80138 napoli , italy 3neurological sciences department , second university of naples , piazza miraglia , 80138 naples , italy 4nuclear medicine , pet unit , policlinico s . 
orsola - malpighi , bologna university , italy 5dipartimento di scienze fisiche , universit federico ii , and infn , sezione di napoli , via cinthia , 80126 napoli , italy 6physics department , university of bologna and infn , bologna , italy correspondence to : r . 
the use of animal models in basic and preclinical sciences , for example , offers the possibility of testing diagnostic markers and drugs , which is becoming crucial in the success and timeliness of research and is allowing a more efficient approach in defining study objectives and providing many advantages for both clinical research and the pharmaceutical industry . 
the aim of this article is to review the characteristics of these systems and illustrate their main applications . in preclinical research , importance keywords molecular imaging micro - pet micro - ct optical imaging small - animal imaging riassunto negli ultimi anni si sono rese disponibili nuove apparecchiature per lo studio di piccoli animali . 
lutilizzo di modelli sperimentali nelle scienze di base e pre - cliniche consente di verificare test diagnostici e farmaci , divenendo essenziale per il successo e la tempestivit della ricerca , offrendo un approccio pi efficace nella definizione degli obiettivi da studiare e notevoli vantaggi sia per la ricerca clinica sia per le industrie farmaceutiche . 
lutilizzo di tali tecnologie consente di ottenere informazioni pi predittive riguardo alla distribuzione o allefficacia di una molecola . il topo , in particolare , un modello animale insostituibile per lo studio delle malattie umane . 
 parole chiave imaging molecolare micro - pet microtc imaging ottico imaging per piccoli animali radiol med ( 2009 ) 114 : 152167 introduction introduzione the availability of animal models in which to reproduce human diseases ( neurodegenerative diseases , tumour growth , genetic disorders ) has given rise to new diagnostic and therapeutic approaches . 
experimental models on small animals , and especially on genetically engineered mice , are receiving increasing recognition as a powerful means of analysis in oncological , cardiovascular and neurological research and in testing potential new drugs [ 3 , 4 ]  . imaging methods based on the introduction of very small concentrations of radiotracers have traditionally been used , together with organ dissection and tissue counts [ 5 ]  . 
alternatively , cryosection of the entire body followed by digital autoradiography [ 6 ] can provide anatomical images with very high spatial resolution ( about 50 m ) correlated with a quantitative analysis of the tracer concentration . 
the main limitation of these ex vivo techniques is that each laboratory animal can only be analysed once during the research study , thus rendering the research expensive , time consuming and relatively imprecise given the physiological variation between specimens . 
 the growing number of studies performed in animal models has attracted scientific interest to the point of awarding the inventor of this imaging technology [ 7 ] with the nobel prize for medicine and providing incentives for the development of new imaging systems adapted to the special conditions of an in vivo study . 
a variety of dedicated devices have been developed in this field , including optical imaging , computed tomography ( ct ) , positron emission tomography ( pet ) , single photon emission computed tomography ( spect ) , magnetic resonance imaging ( mri ) and ultrasonography ( us )  . 
today the provision of biomedical imaging techniques for small animals is one of the most important challenges and opportunities of the new millennium , with the possibility of longitudinal research studies repeatedly examining the same animal model before , during and after the experimental procedure . the aim of this paper is to describe the most common applications of these techniques and outline their relative advantages and disadvantages . 
the following techniques will be described in turn : optical imaging ( bioluminescence and fluorescence ) , micro - ct , micro - pet , micro - spect , micro - mri and micro - us . la disponibilit di modelli animali in grado di riprodurre le malattie umane ( malattie neurodegenerative , crescita tumorale , disordini genetici ) ha permesso nuovi approcci diagnostici e terapeutici . 
modelli sperimentali su piccoli animali , ed in particolare topi ingegnerizzati geneticamente , sono sempre pi riconosciuti come un mezzo potente di analisi nel campo della ricerca oncologica , cardiovascolare , neurologica , e nella sperimentazione di potenziali farmaci [ 3 , 4 ]  . 
 metodi di visualizzazione basati sullintroduzione in concentrazioni molto piccole di molecole radio - marcate sono gi tradizionalmente usati , in combinazione con la dissezione dorgano e la conta tissutale [ 5 ]  . 
in alternativa , la criosezione dellintero corpo seguita dallautoradiografia digitale [ 6 ] pu anche fornire immagini anatomiche con una altissima risoluzione spaziale ( circa 50 micron ) correlate ad unanalisi quantitativa della concentrazione di tracciante . 
il punto debole di queste metodiche ex vivo consiste nella possibilit , durante una ricerca , di poter analizzare una sola volta ogni cavia , rendendo cos la ricerca costosa , dispendiosa di tempo , e poco precisa considerata la variazione fisiologica interindividuale . 
 il numero crescente di studi effettuati su modelli animali ha attratto a tal punto linteresse scientifico da far insignire linventore di questa tecnologia [ 7 ] col premio nobel per la medicina e da incentivare lo sviluppo di nuovi sistemi di imaging adatti alle particolari condizioni di uno studio in vivo su di essi . 
oggi , la disponibilit di tecniche di imaging biomediche per piccoli animali rappresenta la pi importante sfida ed opportunit del nuovo millennio per la possibilit di ricerche longitudinali studiando ripetutamente lo stesso modello animale prima , durante , e dopo una procedura sperimentale . obiettivo di questo contributo descrivere le pi comuni applicazioni di queste metodiche , illustrandone limiti e vantaggi . 
saranno illustrate in sequenza limaging ottico ( bioluminescenza e fluorescenza ) , micro - tc , micro - pet , micro - spect , micro - rm e micro - us . strumenti imaging ottico instrumentation optical imaging progress in the field of optics has rekindled interest in i progressi nel campo dellottica hanno riacceso linteresse nellimaging ottico come potente mezzo di applicazione preclinica . 
the first uses a gene that encodes for an enzyme , such as luciferase [ 10 ] , which in the presence of oxygen and adenosine triphosphate ( atp ) generates bioluminescence with an emission peak of around 560 nthe second , in contrast , uses external dyes or fluorescent markers . 
the device for bioluminescence imaging can simply consist of a black box containing a highly sensitive charged coupled device ( ccd ) camera , which provides images of the distribution of light on the surface of the animal . 
fluorescence imaging , instead , requires the addition of an external light source , such as a laser , or a broad - band source , such as a mercury lamp , and multiple filters to obtain a spectrum of the light emitted . 
at these wavelengths there is also greater penetration and limited linear absorption of the animals internal organs . new optical imaging techniques have recently been developed based on infrared fluorescence that can provide not only planar data but also quantitative information and multiplexing studies : time - domain optical imaging [ 12 ] and tomographic optical imaging [ 13 ]  . 
in particular , because bioluminescence does not require stimulation of an external light source , the problem of the excitation beam penetrating the tissue does not exist , as with other techniques , and there is no background autofluorescence to disturb the signal . 
fluorescence imaging , on the other hand , has the advantage of the high signal produced by the fluorophores and the possibility that this is activated by specific biological processes , thus reducing background noise . the disadvantages derive from two fundamental sul mercato sono presenti diversi strumenti con un ampio intervallo di capacit . 
il primo utilizza come rilevatore un gene che codifica per un enzima , come la luciferasi [ 10 ] , che in presenza di ossigeno ed atp , genera la bioluminescenza con un picco in emissione di circa 560 n il secondo , invece , utilizza coloranti esterni o marcatori fluorescenti ; questi ultimi sono molecole che assorbono nella regione del vicino infrarosso ( nir ) oppure una nuova classe emergente , quantum dots [ 11 ]  . 
lo strumento per limaging in bioluminescenza pu essere semplicemente composto da un box nero contenente una camera ccd ad alta sensibilit , ottenendo cos immagini della distribuzione della luce sulla superficie dellanimale . 
limaging in fluorescenza , invece , richiede laggiunta di una sorgente di luce esterna , come un laser , o una sorgente a banda larga , ad esempio , una lampada a mercurio , e di filtri multipli al fine di ottenere uno spettro della luce emessa . 
 necessario utilizzare fluorofori che vengano eccitati nello spettro dellinfrarosso , dal momento che in questo intervallo di frequenze di eccitazione ed emissione si ottengono dei dati pi puliti dato il basso fondo generato . 
a queste frequenze si ha inoltre un maggior potere di penetrazione ed un assorbimento lineare limitato degli organi interni dellanimale . recentemente sono state sviluppate nuove tecnologie di imaging ottico basate sulla fluorescenza nellinfrarosso che consentono di ottenere non solo dati planari , ma anche di avere informazioni quantitative e di effettuare studi multiplexing , time domain optical imaging [ 12 ] ed imaging ottico tomografico [ 13 ]  . 
restano comunque sufficientemente efficaci i sistemi planari di imaging ottico in commercio e a basso costo , per effettuare studi di screening [ 16 ]  . i vantaggi dei metodi di imaging ottico sono luso di radiazioni a bassa energia non ionizzanti , unalta sensibilit con possibilit di rilevare segnali nellordine di micron o nellordine del sub - picomolare , la capacit di acquisizione continua di dati per il monitoraggio in tempo reale e lo sviluppo di accessori economici . 
in particolare , la bioluminescenza non necessita di una stimolazione esterna di luce : non vi quindi il problema della penetrazione del fascio di eccitazione nei tessuti , come nellaltra metodica , e non c un fondo di autofluorescenza a disturbare il segnale . 
limaging in fluorescenza , invece , si avvantaggia dellalto segnale dei fluorofori e dalla possibilit che questo venga attivato da specifici processi biologici , riducendo cos il rumore di fondo . radiol med ( 2009 ) 114 : 152167 properties of light in tissues , which depend on the wavelength and light diffusion and absorption , which influence image resolution and penetration depth of light into tissues , as well as the ability to obtain quantitative data . lastly , optical imaging has no equivalent in clinical practice , which renders correlation and application of the results difficult . 
this technique has been applied in studies monitoring expression of a transgene , progression of an infection , tumour growth and metastasis , transplant , toxicology , viral infection and gene therapy [ 1823 ]  . micro - ct micro - ct is the miniaturisation of ct , a technique widely used in clinical diagnostic imaging . 
small - animal micro - ct ( mice and rats ) is able to supply very high resolution anatomical images ( up to 9 m ) with three - dimensional views [ 24 ]  . 
in daily practice , researchers of some smallanimal - imaging facilities ( saifs ) tend to limit the study to short scans ( around 1 min ) , both to increase proceeds and reduce radiation exposure , which can jeopardise longitudinal studies , although the cost is a lower spatial resolution ( 150200 m )  . micro - ct systems can be found in many imaging facilities and can cover a variety of applications , both with regard to bone and soft tissue . 
in terms of the ct system specifications , particular attention should be paid to the field of view of the detector , which enables those levels of resolution to be achieved . 
a device of this kind is clearly very versatile , with a broad range of applications but with the drawback of delivering an elevated dose to the animal at high resolutions . 
most systems use a cone - beam x - ray source and a solid - state detector that rotates around the animal , allowing imaging of the entire animal in a single scan . 
 the principal drawbacks of first - generation micro - ct systems were poor contrast resolution for soft tissue , even gli svantaggi derivano da due fondamentali propriet della luce nei tessuti che dipendono dalla lunghezza donda , dalla diffusione della luce e dallassorbimento , che condizionano sia la risoluzione dellimmagine che la profondit di penetrazione della luce nei tessuti , oltre che la capacit di ottenere dati quantitativi . infine , limaging ottico non ha un corrispettivo nella pratica clinica , e questo rende difficile la correlazione e lapplicazione dei risultati . 
questa tecnologia stata applicata in studi di monitoraggio dellespressione di un transgene , per la progressione di uninfezione , crescita tumorale e metastasi , trapianto , tossicologia , infezioni virale e terapia genica [ 1823 ]  . micro - tc la micro - tc una miniaturizzazione della nota tc , ampiamente utilizzata nella diagnostica clinica . 
la microtc dedicata a piccoli animali ( topi e ratti ) in grado di fornire un imaging anatomico ad altissima risoluzione ( fino a 9 micron ) e con visualizzazione tridimensionale [ 24 ]  . nella quotidianit , sia per incrementare eventuali ricavi che per ridurre lesposizione a radiazioni ionizzanti che possono pregiudicare studi longitudinali , i ricercatori di alcune saifs tendono a ridurre lindagine a brevi scansioni ( circa 1 minuto ) , a prezzo di una minore risoluzione spaziale ( 150200 micron )  . 
 i sistemi micro - tc sono abbastanza diffusi presso molte facility di imaging e possono coprire diverse applicazioni sia per quanto riguarda studi su ossa che per tessuti molli . relativamente allo studio su reperti ossei , bisogna tenere in considerazione il limite di risoluzione di 15 micron se si vuole effettuare unanalisi a livello delle trabecole ed importante valutare tra le specifiche del sistema tc anche le dimensioni del campo di vista del rivelatore su cui possibile ottenere quelle determinate risoluzioni . 
per quanto riguarda sistemi dedicati a studi in vivo in genere la risoluzione ottimale si aggira intorno ai 50 o 100 micron , con la conseguente riduzione di dosi e la possibilit di effettuare studi longitudinali . 
second - generation micro - ct systems incorporated much of the technology used in clinical practice , including arrays with smaller detector elements and more powerful x - ray tubes , which enable not only faster scans 0.8 s for the entire animal but also the use of clinical contrast agents and the possibility of performing perfusion studies [ 27 ]  . 
in addition , the use of iodinated contrast agents has significantly improved image contrast , enabling visualisation of even small - diameter vessels ( 20 m ) [ 28 ]  . 
in questo caso necessario avere un dispositivo aggiuntivo di controllo respiratorio che minimizza gli artefatti nelle immagini causati dal movimento della cassa toracica dellanimale . la maggior parte dei sistemi utilizza una sorgente conica di raggi x e un detettore solido che ruota intorno la cavia e che permette lacquisizione dellintero animale in una singola scansione . 
gli svantaggi maggiori della prima generazione di micro - tc sono stati una povera risoluzione di contrasto per i tessuti molli , anche dopo luso di mezzi di contrasto , unalta dose di radiazioni , lunghi tempi di scansione , e artefatti nellimmagine , in particolare alle risoluzioni pi alte . 
la generazione successiva di micro - tc ha utilizzato molte delle tecnologie duso clinico , compresi rivelatori sottili e tubi radiogeni pi potenti , che permettono sia di effettuare scansioni pi veloci , 0 , 8 secondi per linterno animale , sia luso di agenti di contrasto clinici con maggiore traslazione degli studi sia la possibilit di effettuare studi di perfusione [ 27 ]  . 
inoltre , luso di mezzi di contrasto iodati , hanno significativamente migliorato il contrasto dellimmagine , visualizzando vasi anche di piccolo diametro ( 20 micron ) [ 28 ]  . 
i sistemi ad alta risoluzione micro - tc sono stati anche utilizzati in maniera soddisfacente nei tumori dei tessuti molli [ 33 ] e nella caratterizzazione fenotipica di malattia in animali transgenici [ 34 ]  . 
 micro - pet la pet , come la spect , consente di ottenere immagini di una funzione o di un processo biochimico del corpo , utilizzando un radiotracciante ad emissione di positroni . 
si supera cos il limite delle tecniche diagnostiche tradizionali , come le indagini radiologiche , tc o rm , che forniscono unimmagine di tipo anatomico sia il limite della variabilit interindividuale , spesso ritrovata negli studi di farmacologia , in quanto ogni animale pu rappresentare il proprio controllo . quasi tutti i sistemi micro - pet utilizzano piccoli la maggior parte bismuto germanato , cristalli , per germanio oxyorthosilicate , lutetium oxyorthosilicate , o cerio - doped lutetium yttrio ortosilicato di 12 mm , accoppiati a fotomoltiplicatori ( pmts ) convenzionali . 
ricostruzione con voxel 93 m . radiol med ( 2009 ) 114 : 152167 micro - pet as with spect , pet produces images of a biochemical function or process of the body with the use of a positronemitting radiotracer . 
the technique overcomes both the limitations of traditional morphological diagnostic techniques , such as ct or mri , and those of intraindividual variability , which is often found in pharmacological studies , in that each animal can serve as its own control . almost all micro - pet systems use small crystals ( 12 mm ) of bismuth germinate , germanium oxyorthosilicate ( gso ) , lutetium oxyorthosilicate or cerium - doped lutetiumyttrium orthosilicate ( lyso ) coupled with conventional photomultipliers ( pmts )  . 
one company has modified the pmt - based design and used solid - state detectors ( photodiodes ) coupled directly to the individual crystals . today , small - animal pet systems have a small gantry with an opening of 1222 cm and a shorter distance between detectors than do clinical pet devices . 
the overall spatial resolution can in general be improved during image reconstruction with the use of physical models to correct for detector blurring , positron - range blurring and other effects [ 37 ]  . the technology recently developed in the field of detectors used in micro - pet has led to significant improvements in terms of resolution uniformity over the field of view . 
the technology used in these systems is based on the presence of a dual ring of scintillation crystals ( gso and lyso ) , which enables greater depth of interaction of photons and therefore reduction in parallax . 
this produces increased and uniform resolution ( 1.4 mm ) throughout the field of view , enabling very effective quantitative analyses [ 38 ]  . another pet modality based on the same concept of coupling two scintillation crystals [ lyso and lutetium yttrium aluminate perovskite ( luyap ) ] is under development . 
this system uses a mobile gantry that is able to accommodate not only small but also medium - sized animals . the use of pet technology is experiencing tremendous expansion , although it is limited by the availability of a cyclotron in the vicinity and a radiopharmacy for production and synthesis of radiopharmaceuticals . 
fluorodeoxyglucose labelled with the isotope 18f is the most commonly used , although new isotopes with a longer half - life are being developed , such as gallium - 68 and copper - 64 for studying hypoxia . lastly , the advent of combined ct - pet systems will further optimise the pet examination by integrating animali si avvantaggiano di un gantry pi piccolo , 1222 cm di apertura , e di una minore distanza tra i rilevatori rispetto alla pet clinica . 
questo si traduce in una pi alta risoluzione spaziale sul volume di almeno 1 , 3 mm e nella capacit di determinare concentrazioni di traccianti nellordine del picomolare in vivo . 
la risoluzione spaziale complessiva pu essere generalmente migliorata durante il processo di ricostruzione dellimmagine attraverso modelli fisici per la correzione degli effetti di blurring del detettore , del range del positrone nellorganismo e di altri effetti [ 37 ]  . 
la tecnologia utilizzata in questi sistemi si basa sulla presenza di un doppio anello di cristalli scintillatori ( gso e lyso ) che consente una maggiore profondit di interazione dei fotoni e quindi una riduzione delleffetto di parallasse . 
in questo modo si possono ottenere elevate risoluzioni ( 1 , 4 mm ) e uniformi lungo il campo di vista , permettendo di fatto unanalisi quantitativa molto efficace [ 38 ]  . unaltra modalit pet in fase di sviluppo ed basato sullo stesso concetto di accoppiamento di 2 cristalli scintillatori ( lyso e luyap ) : questo sistema utilizza un gantry mobile in grado di accogliere non solo piccoli animali , ma anche animali di taglia maggiori . lutilizzo della tecnologia pet in grossa espansione anche se limitata dalla disponibilit di un ciclotrone nelle vicinanze e di una radiofarmacia per la produzione e la sintesi del radiofarmaco . 
attualmente il pi utilizzato il fdg abbinato allisotopo 18f , ma sono in fase di studio nuovi isotopi con emivita pi lunga , quali gallio 68 e rame 64 dedicato allo studio dellipossia . 
 infine , lavvento di sistemi integrati tc - pet consentir un ulteriore ottimizzazione dellindagine pet grazie allintegrazione dellimaging funzionale con quello anatomico della tc . i vantaggi della pet risiedono nella sua specificit , sensibilit , e nella possibilit di quantificare la concentrazione tissutale di un tracciante . 
la sensibilit , pari a 10100 volte la spect , tc e rm , deriva dalluso della coincidenza , dalla conta con collimatori elettronici , e dalla quantificazione conseguenti alla possibilit di correggere la perdita di segnale dovuta allattenuazione dei fotoni [ 39 ]  . 158 radiol med ( 2009 ) 114 : 152167 functional imaging with the morphological information provided by ct . the advantages of pet lie in its specificity , sensitivity and the ability to quantify the tissue concentration of a tracer . 
sensitivity of the technique between 10 and 100 times greater than spect , ct and mr resides in its use of electronic collimators to measure coincidence events and quantification made possible by correcting for signal loss due to photon attenuation [ 39 ]  . 
i pi utilizzati sono 133xe , il 99mtc e lo 123i che decadono emettendo raggi gamma e sono pi facilmente accessibili di quelli usati nella pet [ 46 ]  . 
limaging di piccoli animali , invece , richiede una pi alta risoluzione spaziale per oggetti molto pi piccoli e si ottiene mediante collimatori detti a pinhole , che permettono di raggiungere una risoluzione spaziale molto alta ( < 1 mm ) [ 47 ]  . 
questi sistemi utilizzano un gran numero di radiofarmaci gamma - emittenti , piccole molecole , peptidi e anticorpi , alcuni routinariamente usati nella clinica , altri ancora in fase di sviluppo . fra i limiti della micro - spect si comprendono : una perdita di segnale causata dallattenuazione da parte del collimatore di molti fotoni incidenti ; una elevata attivit del radiofarmaco necessaria per ottenere un segnale utile per la formazione dellimmagine ; la trasmissione di fotoni che decadono attraverso il tessuto . 
con i primi sistemi pinhole spect dedicati ( micro - spect ) , era possibile ottenere una risoluzione spaziale sub - millimetrica , ma il singolo pinhole ne limitava la sensibilit . 
 la prossima disponibilit di nuove tecnologie , in particolare lo sviluppo di nuovi rilevatori quali czt ( cadmio zinc telluride ) , consentir una sensibilit pari alla micropet , conservando una risoluzione sub - millimetrica . 
le fette sono coronali e la freccia rossa indica la assente o ridotta fissazione del radiofarmaco nella sede del danno . rays , are the most widely used and are more readily available than those used in pet [ 46 ]  . 
small - animal systems , in contrast , require much higher spatial resolution for imaging small objects . this is achieved with pinhole collimators capable of producing a spatial resolution < 1 mm [ 47 ]  . 
these systems use a large number of gamma - emitting radiopharmaceuticals , small molecules , peptides and antibodies , some of which are routinely used in clinical practice , and others are under development . the limitations of micro - spect include signal loss caused by collimator - induced attenuation of many incident photons , elevated activity of the radiopharmaceutical required to produce an adequate signal for image formation , and transmission of photons that decay throughout the tissues . 
with these models , the image can be reconstructed by superimposing data , the scan time has been reduced to several minutes and the dose of radiation per animal has been lowered . the upcoming technological developments , in particular , new detectors such as czt ( cadmium zinc telluride ) , will una tecnologia di sicuro interesse e di grosso potenziale applicativo per il futuro . 
la maggior parte dellimaging su piccoli animali con micro - rm effettuato su strumenti con carrello orizzontale , con campi di forza compresi tra i 4 , 7 t e i 9 , 4 t e con lettino di 2040 csono stati anche sperimentati sistemi con campi di forza pi alti come 11 , 7 t e 21 , 1 t [ 51 ]  . 
per esempio , quando si esaminano le differenze tra sostanza grigia e bianca nel cervello , i tempi di rilassamento rispondono in maniera pi stretta rispetto a quelli osservati nei pi bassi campi utilizzati nellimaging umano , e cos le differenze di contrasto grigio - bianco sono peggiori . 
 la risoluzione pari a 10100 micron e il contrasto 160 radiol med ( 2009 ) 114 : 152167 increase sensitivity to the level of micro - pet , all the while maintaining submillimetre resolution . 
the technique can be used to monitor physiological functions [ 49 ] , track metabolic processes and quantify receptor density [ 50 ]  . micro - mri micro - mri is a powerful and versatile imaging modality for studying small animals . 
t1 and t2 relaxation times are dependent on the magnetic field . for example , when the differences between grey and white matter in the brain are examined , relaxation times tend to be much longer and varied than in the lower fields used for human imaging , with a deterioration in greywhite contrast . the resolution of 10100 m and the spatial contrast of micro - mri systems are not the best among preclinical imaging systems . 
however , as with other modalities , hybrid systems are being developed , such as mri / pet , to obtain increasingly complete information from a single device [ 52 ]  . 
micro - mri systems can be used for functional and physiological studies of tissues [ 5355 ]  . micro - us based on the propagation of sound waves for imaging soft tissue , micro - us is in direct competition with the currently available optical systems in terms of reliability and field of application . 
most of these systems consist of clinical instrumentation adapted to preclinical use , and as yet , there are no ultrasound systems dedicated to the in vivo imaging of small animals , with the exception of one system developed around 5 years ago . 
this device uses very high frequencies , 2580 mhz , and produces a resolution below 30 m and a penetration of around 15 min addition , the use of microand nanobubbles with coatings and gas components as a sonographic contrast agent significantly improves sensitivity and enables measurement of flow in vessels 2030 m in diameter . 
tuttavia , come per altre modalit di imaging , si stanno sviluppando sistemi ibridi , come rm / pet , al fine di ottenere informazioni sempre pi complete con un singolo strumento [ 52 ]  . 
i sistemi microrm consentono indagini funzionali e fisiologiche a livello tissutale [ 5355 ]  . micro - us basata sulla propagazione delle onde sonore per limaging dei tessuti molli , la micro - us compete con i sistemi ottici in commercio in termini di affidabilit e campi dapplicazione . la maggior parte di queste apparecchiature consiste in strumenti clinici adattati alluso pre - clinico e non ci sono ancora sistemi ecografici dedicati per limaging in vivo su animale , ad eccezione di uno sviluppato circa 5 anni fa . questo strumento utilizza frequenze molto alte , 2580 mhz , e fornisce una risoluzione inferiore a 30 micron ed una penetrazione di circa 15 m inoltre , con lutilizzo di microe nano - bolle rivestite e riempite di gas come mezzo di contrasto ecografico , possibile migliorare significativamente la sensibilit dellimaging e misurare il flusso in vasi di 2030 micron di diametro . 
anche possibile attaccare ligandi o anticorpi al rivestimento , rendendo il mezzo di contrasto specifico e capace di legarsi selettivamente a citotipi o processi ( ad esempio , angiogenesi o infiammazione ) [ 56 , 57 ]  . lus una tecnica relativamente economica e accessibile , ma limitata alla profondit dei tessuti che possono essere raggiunti e quindi visualizzati . 
come conseguenza , luso degli ultrasuoni nellimaging animale non si diffuso come le altre modalit dimaging , ma si concentrato sullindagine di particolari strutture biologiche accessibili come la vescica [ 58 ] e i vasi sanguigni [ 59 ]  . 
inoltre una specifica potenzialit degli ultrasuoni lo studio dello sviluppo pre - natale [ 60 ] su animali transgenici . stabulazione degli animali un centro saif deve disporre sia di locali destinati ad accogliere le apparecchiature per la diagnostica che di ambienti annessi riservati alla stabulazione degli animali da sottoporre alle indagini . 
as a result , the use of us in smallanimal imaging is not as widespread as other imaging modalities , with efforts being concentrated on the study of accessible biological structures such as the urinary bladder [ 58 ] and the blood vessels [ 59 ]  . 
in addition , one specific potential application is in studying prenatal development of transgenic animals [ 60 ]  . animal housing saifs should have areas both for diagnostic equipment and housing animals to be studied . 
each area should guarantee appropriate air exchange ( every 1520 h ) , temperature regulation ( 222 c ) and control of relative humidity ( 55%10% ) , as well as the alternation of light and dark in the animal housing areas . the animal house should comprise a number of areas separated by filter barriers , including the animal housing area with feed storage and sawdust and other materials ( cages , grids , bottles ) , a procedure room , a cage - washing area , areas for waste disposal and a filter room / changing rooanimals should be housed in an area near to but separate from the procedure room so that animals waiting to undergo experiments are unable to hear the vocalisations of those undergoing procedures or smell blood in the event of surgical procedures . 
the procedure room should be equipped with the following : laminar - flow ventilation hood , housing for the dissecting microscope , airand oxygen - pressure monitoring , anaesthetic vaporiser , work bench , co2 euthanasia chamber , lockable cupboard for the storage of drugs and consumables , telephone and network connection with pc and a sink . lastly , the area for storing special waste and carcasses should be appropriately shielded and house a refrigeration system ( 20 c ) for their storage until their removal . preparation of animals for study all imaging techniques , except for some optical imaging devices , require the animals to be immobilised . 
some researchers inject barbiturates , but most prefer inhalation anaesthetics , such as isoflurane , because these are administered continuously and can be calibrated to ( 55%10% ) ed unalternanza luce / buio nei locali di stabulazione . 
 lo stabulario deve prevede diverse aree accessibili per mezzo di un filtro e comprendenti un locale di stabulazione con deposito mangime e segatura e / o altro materiale ( gabbie , griglie , bottiglie ) , un laboratorio , un locale lavagabbie , uno spazio per il deposito rifiuti , una stanza filtro / spogliatoio . 
gli animali in sosta devono essere allocati in un ambiente vicino , ma separato dal laboratorio per evitare che cavie che attendono di essere sottoposte ad indagini possano ascoltare le eventuali vocalizzazioni di animali sottoposti a manipolazioni o fiutare lodore del sangue in caso di procedure chirurgiche . 
il laboratorio deve disporre di una cappa a flusso laminare con alloggio per microscopio operatorio , flussimetri per aria ed ossigeno , vaporizzatore ed estrattore per gas anestetici , tavolo di lavoro , bocchetta per lerogazione della co2 al fine di poter procedere alleutanasia , armadietto con serratura per il deposito di farmaci e materiale di consumo , impianto telefonico e di rete con postazione pc , lavabo . 
infine , il locale deposito rifiuti speciali e stoccaggio carcasse deve essere opportunamente schermato e poter allocare un frigo 20c per il loro deposito , fino allallontanamento . preparazione degli animali per lindagine tutte le tecniche dimaging , eccetto per alcuni strumenti dimaging ottico , richiedono che i soggetti dello studio siano immobilizzati . 
alcuni ricercatori iniettano barbiturici , ma la maggior parte preferiscono gli anestetici inalatori , come lisofluorano , perch lanestesia inalatoria somministrata in maniera continua e pu essere calibrata sulle specifiche caratteristiche dellanimale e dellesperimento . 
il sistema dellanestesia gassosa , combinato con il sistema di riscaldamento per la prevenzione dellipotermia , stabilizza le funzioni corporee durante i protocolli sperimentali e riduce al minimo leventualit di perdere gli animali durante le diverse procedure . 
use of inhalation anaesthesia , coupled with active warming to prevent hypothermia , stabilises the vital functions during the experiment and reduces the risk of the animal dying during the various procedures . in addition to anaesthesia and the regulation of body temperature , the equipment must ensure the possibility of immobilising the animal during the study session [ 62 ]  . often , many saifs develop their own containers for specific applications , but most systems for small - animal imaging can hold both mice and rats . 
during the acquisition phase , some physiological parameters can and should be monitored , such as heart and respiratory function and internal temperature . facility organisation saifs should provide the six most utilised imaging modalities in scientific research laboratories . 
these modalities are optical imaging , ( bioluminescence and fluorescence ) , micro - pet , micro - ct , micro - spect , micro - mri and micro - us . 
a detailed list of the main saifs throughout the world and the manufacturers of small - animal imaging systems is available at in general , most saifs require the participation of at least a physicist , an engineer , a veterinarian and several technicians with skills in computer operating and programming , data and image acquisition and analysis and animal treatment . 
the use of animal models in basic and preclinical research and the possibility of performing longitudinal studies on the same animal are key factors for the success and timeliness of research . 
in response to this demand , saifs have been set up to perform a number of tasks : to assist researchers in inoltre , alcune tecniche dimaging richiedono una preparazione particolare : gli animali da sottoporre ad us , per esempio , devono essere tricotomizzati . 
nella fase di acquisizione , alcuni parametri fisiologici possono , e dovrebbero , essere monitorati , come la funzione cardiaca e respiratoria e la temperatura interna dellanimale . organizzazione del servizio il servizio di imaging per piccoli animali , saif , dovrebbe fornire un supporto che comprende le sei modalit pi utilizzate nei laboratori per la ricerca scientifica . 
le sei modalit comprendono : limaging ottico ( bioluminescenza e fluorescenza ) , la micro - pet , la micro - tc , la microspect , la micro - rm e la micro - us . 
una lista dettagliata delle principali saif nel mondo e delle ditte produttrici di strumenti per imaging su piccoli animali pu essere visualizzata nel sito generalmente , la maggior parte delle facilities richiedono la collaborazione di almeno un fisico , un ingegnere , un veterinario ed alcuni tecnici con competenza nelle operazioni e nella programmazione di computer , nellacquisizione e analisi dei dati e di immagine e nel trattamento degli animali . 
lutilizzo di modelli animali nelle scienze di base e pre - cliniche , la possibilit di studi longitudinali sullo stesso animale sono un fattore chiave per il successo e la tempestivit della ricerca . 
per soddisfare questa richiesta , sono nate alcuni servizi per limaging di piccoli animali al fine di : assistere i ricercatori nel progetto sperimentale ; sviluppare e fornire strumenti specifici e procedure innovative per limaging ; preparare gli animali per gli studi , inducendo e mantenendo unappropriata anestesia e immobilizzazione durante la sessione dimaging ; marcare in maniera appropriata i tessuti per la correlazione delle caratteristiche macroscopiche , microscopiche e di imaging del tessuto o organo ; processare , analizzare ed interpretare i dati per la pubblicazione . radiol med ( 2009 ) 114 : 152167 experimental projects ; to develop and supply specific instrumentation and innovative procedures for imaging ; to prepare animals for studies by inducing and maintaining appropriate anaesthesia and immobilisation during the imaging session ; to appropriately mark tissues for the correlation of macroscopic , microscopic and imaging characteristics of the tissues or organ ; to process , analyse and interpret data for publication . the facility should be designed to optimise work processes , access to the animals and exposure to radiation and the magnetic field . 
constant upgrading and renewal of the equipment , particularly with the development of new imaging devices and analysis and computational systems , should be a standard feature for improving the technical potential of the facility . 
lastly , a procedure room near the facility and the animal house will make new experimental protocols possible and facilitate analysis before , during or immediately after the surgical procedure [ 65 ]  . in this setting , the six imaging modalities take their place . these modalities are optical imaging , ( bioluminescence and fluorescence ) , micro - pet , micro - ct , micro - spect , micromri and micro - us . 
hybrid technologies , such as ct - pet and ct - spect , and in vivo coregistration of fluorescence imaging with morphological studies performed with ct or mri that compensates for the short path of the fluorescent signal , the limited penetration of the photons in the tissue and the low three - dimensional spatial resolution , provide complementary information [ 66 , 67 ] by correlating functional data with anatomical structures . of particular importance is that the saif should be selfcontained , so that significant and exhaustive results can be achieved with the same facility , the same personnel , the same animal and the same data analysis , thus saving time and money . each in vivo preclinical imaging modality has a specific application , which maximises the potential of each modality [ 68 ] ( table 1 )  . 
for example , us is an excellent instrument for analysing the vascularity of superficial neoplastic masses , micro - pet is extremely sensitive in measuring types of pathological metabolic activity of various processes , micro - mri can provide very high contrast images and optical imaging is the simplest technique for studying gene expression . 
this explains why saifs are becoming equipped with as many imaging modalities as possible , a tendency that is certain to continue increasing . in the setting of the saif , the radiologists and nuclear scientist technological knowledge , familiarity with the similar equipment in clinical practice and ability to correlate the various findings during diagnostic and therapeutic monitoring give him or her a frontline role . 
these skills cannot be substituted by the physicist or other specialist , both of lallocazione del servizio dovrebbe essere predisposta per ottimizzare il lavoro del personale , laccesso agli animali , il percorso e lesposizione alle radiazioni e al campo magnetico . 
un continuo aggiornamento e rinnovo delle apparecchiature , specie con lo sviluppo di nuovi strumenti per limaging e di sistemi di analisi e di calcolo , dovrebbe essere previsto al fine di migliorare le potenzialit tecniche del centro . 
infine , un area chirurgica , vicino alla facility e allo stabulario , permetter nuovi protocolli sperimentali e faciliter lanalisi prima , durante , o immediatamente dopo un intervento chirurgico [ 65 ]  . in questo articolato progetto vanno attentamente inserite le sei modalit dimaging che comprendono : limaging ottico ( bioluminescenza e fluorescenza ) , la micro - pet , la micro - tc , la micro - spect , la micro - rm e la micro - us . 
le tecnologie ibride , come la tc - pet e la tc - spect , e la coregistrazione in vivo dellimaging in fluorescenza con le modalit dimaging anatomico , quali la rm e la tc , che compensa il breve percorso del segnale fluorescente , la limitata penetrazione dei fotoni nel tessuto e la bassa risoluzione spaziale tridimensionale , forniscono informazioni complementari [ 66 , 67 ] correlando dati funzionali con le strutture anatomiche . in questo contesto dunque importante la completezza della saif , cos da ottenere dal medesimo servizio , personale , animale e dalla stessa analisi dei dati , risultati significativi ed esaustivi risparmiando tempo e denaro . 
 ognuna delle metodiche di imaging pre - clinico in vivo trova applicazioni specifiche in cui le potenzialit di ogni singola tecnica sono valorizzate al massimo ( tabella 1 ) [ 68 ]  . 
per esempio lultrasonografia un ottimo strumento per lanalisi della vascolarizzazione di masse neoplastiche superficiali , la micro - pet estremamente sensibile per la misura dellattivit metabolica di vari tipi di processi patologici , la micro - rm consente di ottenere immagini ad elevatissima contrasto , limaging ottico il mezzo pi semplice per lo studio dellespressione genica . 
questo rende ragione del perch le saifs si stiano attrezzando con il maggior numero possibile di metodiche , tendenza destinata sicuramente a crescere nel tempo . in queste saifs , le conoscenze tecnologiche del radiologo e del medico nucleare , la dimestichezza con apparecchiature simili nella pratica clinica e la capacit di correlare i vari reperti nel monitoraggio diagnostico e terapeutico , assegnano al radiologo un ruolo di primo piano . 
 purtroppo , molte apparecchiature sono state acquistate singolarmente ed allocate in dipartimenti estranei alla table 1 main features of commercial small - animal imaging systems technique resolution sensitivity depth of view acquisition time radiol med ( 2009 ) 114 : 152167 ct flat panel spect 10100 m 950 m 150 m < 50 m 12 mm < 1 mm 12 mm ct flat panel spect 10100 m 950 m 150 m < 50 m 12 mm < 1 mm 12 mm - mmol m - cmol m - cmol mmol p - nmol p - nmol p - nmol - mmol m - cmol m - cmol mmol p - nmol p - nmol p - nmol no limit no limit no limit 15 mm no limit no limit < 1 cm nessun limite nessun limite nessun limite 15 mm nessun limite nessun limite < 1 cm 1060 min 560 min 0.5 s3 min 1520 min 10 s20 min 0.5 s20 min 1060 min 560 min secondi 0 , 5 s3 min 1520 min 10 s20 min 0 , 5 s20 min mr , magnetic resonance ; ct , computed tomography ; us , ultrasound ; pet , positron emission tomography ; spect single photon emission computed tomography ; opt , optical imaging tabella 1 principali caratteristiche dei sistemi sul mercato per limaging di piccoli animali strumento risoluzione sensibilit profondit di campo tempo di acquisizione rm , risonanza magnetica ; tc , tomografia computerizzata ; us , ecografia ; pet , tomografia ad emissione di positroni ; spect , tomografia computerizzata a emissione di fotoni singoli ; opt , imaging ottico whom are part of the team but play different roles , optimising and developing the potential of the devices . unfortunately , many devices are acquired separately and allocated to departments outside the sphere of the radiologist . 
in contrast , radiologists and nuclear scientist should act to promote the creation of more complete and functional imaging centres in the mould of the true saif , where their role would come to the fore . 
i radiologi e medici nucleari , invece , devono farsi promotori dellistituzione di centri pi completi e funzionali tendendo alla realizzazione di vere e proprie saifs , dove il loro ruolo esaltato . 
inoltre opportuno che si applichino in queste nuove aree di ricerca , che saranno la linfa del nostra disciplina . infine , i radiologi e medici nucleari pi giovani devono essere allertati sulle potenzialit dimpiego anche in questo genere di strutture . 
questo settore di ricerca richiede la formazione di adeguate figure professionali che abbiamo competenze di tutte le metodiche di imaging ma anche di biologia molecolare , di gestione dei piccoli animali ( ogni specie ha caratteristiche differenti che la rendono pi o meno adatta a ciascun tipo di studio ) , di chimica organica e di fisica . 
 conclusioni conclusions the modalities of optical and nuclear imaging , micro - ct , micro - mri and micro - us are becoming key techniques for in vivo molecular imaging , thanks to their ability to identify molecular events with adequate sensitivity , specificity and temporal and spatial resolution . 
the availability of new le modalit di studio dell imaging ottico e nucleare , micro - tc , micro - rm , e micro - us stanno emergendo come tecniche chiave nellimaging molecolare in vivo grazie alla possibilit di individuare eventi molecolari con sufficiente sensibilit , specificit , risoluzione temporale e spaziale . 
la disponibilit di nuove sonde , hardware e software per limaging e lo sviluppo di differenti modelli transgenici di malattie ha dato un forte impulso a queste tecniche dindaradiol med ( 2009 ) 114 : 152167 imaging probes , hardware and software and the development of different transgenic models of disease have greatly stimulated these imaging modalities , which are complementary and which , despite responding to different needs and applications , require a multimodal approach to ensure coverage of the different applications . 
preclinical imaging will increasingly be used to study different stages of a pathological process and visualise certain tissues , cell types or receptors . the number of universities , pharmaceutical companies and research centres equipped with saifs will continue to grow . gine , che sono complementari tra di loro e che , sebbene rispondono ad esigenze ed applicazioni diverse , necessitano di un approccio multimodale in modo da coprire le diverse esigenze applicative . 
limaging pre - clinico sar sempre pi utilizzato per lo studio di differenti momenti di un processo patologico e per visualizzare un determinato tessuto , citotipo , o recettore di interesse . 
complete tumour necrosis , confirmed by targeted biopsy , was observed in patients showing no intralesional flow signals and time - intensity curves with low peak of signal intensity and absence of plateau after treatment . 
dopo il trattamento , nei pazienti che presentavano assenza di segnali vascolari intralesionali , curve con basso picco di intensit e assenza di plateau , la biopsia mirata confermava la necrosi completa . 
in base ai risultati ottenuti , le curve con elevato picco di intensit e presenza di plateau , potrebbero rappresentare pattern del tessuto neoplastico intra o perilesionale e fornire quindi importanti informazioni sullefficacia del trattamento . radiol med ( 2009 ) 114 : 3241 keywords power doppler time - intensity curves contrast material focal hepatic lesions hepatocellular carcinoma metastasis parole chiave power doppler curve dintensit - tempo mezzi di contrasto lesioni focali epatiche carcinoma epatocellulare metastasi introduction introduzione in recent years , several nonoperative techniques have been used successfully in the locoregional treatment of hepatocellular carcinoma and metastases , including percutaneous ethanol transcatheter arterial chemoembolisation ( tace ) [ 35 ] , and radiofrequency ablation ( rfa ) [ 69 ]  . injection ( pei ) [ 1 , 2 ] , the follow - up of patients undergoing these treatments is generally based on imaging studies such as magnetic resonance imaging ( mri ) [ 10 , 11 ] or computed tomography ( ct ) [ 12 ] , with only few doubtful cases being studied by biopsy to assess whether complete necrosis of the neoplastic tissue has been achieved . contrast - enhanced colour doppler ultrasound ( cdus ) , thanks to its high sensitivity in detecting weak intratumoural flow signals , has been employed for several years in the differential diagnosis of focal hepatic lesions [ 1315 ]  . recently , it has also been used for the follow - up of intralesional therapy [ 1619 ] , to identify residual areas of intratumoural enhancement that could reflect incomplete necrosis or disease recurrence . 
a study of intralesional and perilesional vascularity with analysis of time - signal intensity curves performed immediately after treatment may help to ascertain whether certain flow signals reflect incomplete treatment . 
the use of contrast - enhanced power doppler us ( pdus ) with timeintensity curves in liver diseases [ 2023 ] , as in focal breast lesions [ 24 ] , may also provide valuable information on the persistence of neoplastic perilesional vascularity and consequently on incomplete necrosis . 
the purpose of this study was to assess the utility of pdus with analysis of time - intensity curves in monitoring focal hepatic lesions ( metastases , hepatocellular carcinoma ) treated with pei or rfa and to correlate the findings with the results of targeted biopsy . materials and methods twenty patients ( twelve men and six women ; age range 55 to 72 years ) with hepatocellular carcinoma and solitary metastases of the liver previously diagnosed by other methods ( ct , mri , biopsy ) underwent intralesional therapy with pei or rfa . 
all patients were studied negli ultimi anni sono state utilizzate diverse tecniche non chirurgiche per il trattamento loco - regionale dellepatocarcinoma e delle metastasi , alcune di queste , molto efficaci come lalcoolizzazione percutanea ( pei ) [ 1 , 2 ] , la chemioembolizzazione ( tace ) [ 35 ] e la radioipertermia ( rfta ) [ 69 ]  . il follow - up dei pazienti sottoposti a questi trattamenti generalmente affidato a metodiche di diagnostica per immagini come la rm [ 10 , 11 ] o la tc [ 12 ] ; solo in alcuni casi dubbi si ricorre alla biopsia per verificare leffettiva necrosi completa del tessuto neoplastico . 
 il color doppler con mdc , grazie allelevata sensibilit nel rilevare i deboli segnali vascolari intralesionali una metodica gi da qualche anno utilizzata per la diagnosi differenziale delle lesioni focali epatiche [ 1315 ] , ed stata gi utilizzata anche per il follow - up dopo la terapia intralesionale [ 1619 ]  . 
spesso subito dopo il trattamento il color doppler con mdc evidenzia una ricca vascolarizzazione perilesionale la cui natura non pu essere determinata se non con la biopsia ; quindi lo studio della vascolarizzazione intra e perilesionale con le curve intensit / tempo , subito dopo il trattamento , potrebbe essere utile poich alcuni segnali vascolari potrebbero essere indice di incompleto trattamento . 
lutilizzo del power doppler con mdc con la determinazione delle curve intensit / tempo nelle malattie del fegato [ 2023 ] o come nel caso delle lesioni focali della mammella [ 24 ] , potrebbe fornire , a nostro giudizio , informazioni preziose anche circa la persistenza di vascolarizzazione neoplastica perilesionale dopo il trattamento e quindi incompleta necrosi della lesione . 
obiettivo di questo lavoro quindi lutilizzo del power doppler con le curve intensit / tempo nel monitoraggio delle lesioni focali epatiche ( metastasi , epatocarcinoma ) sottoposte al trattamento intralesionale con pei e rfta confrontando i risultati con la biopsia mirata . materiali e metodi venti pazienti , dodici maschi e sei femmine , con et compresa tra 55 e 72 anni , affetti da epatocarcinoma e radiol med ( 2009 ) 114 : 3241 by pdus with analysis of time - intensity curves one day before and one day after treatment , followed by targeted biopsy two days later . 
subjects in the control group were imaged by pdus with analysis of time - intensity curves . the us studies were performed on an au cinque idea device ( esaote , genoa , italy ) with a 3.5 mhz convex - array probe . 
in patients the time - intensity curves were derived from a circular region of interest ( roi ) placed over the lesion and large enough to encompass both the intralesional and perilesional vessels . 
il giorno prima e il giorno dopo il trattamento , tutti i pazienti sono stati studiati con esame power doppler con determinazione delle curve intensit / tempo e successivamente , 2 giorni dopo il trattamento , sottoposti a biopsia mirata . 
i pazienti del gruppo di controllo sono stati sottoposti ad esame power doppler con curve intensit / tempo . per lindagine ecografica stato utilizzato un apparecchio au cinque idea ( esaote , genova ) con sonda convex da 3 , 5 mhz . 
nei pazienti patologici la curva intensit / tempo stata ottenuta utilizzando una roi circolare posizionata sulla lesione in modo da comprendere sia la vascolarizzazione intra che perilesionale a tale scopo stato fatto coincidere il diametro della roi con il diametro massimo ottenuto comprendendo la lesione e la vascolarizzazione perilesionale . 
nei pazienti del gruppo di controllo stata utilizzata su tutti i pazienti una roi circolare del diametro di un centimetro posizionata in unarea del parenchima del lobo destro del fegato . 
b the corresponding time - intensity curve shows an elevated peak of signal intensity ( arrowhead ) related to a high concentration of contrast agent and a plateau phase ( arrow ) due to the retention of contrast material within the lesion . 
b la curva intensit / tempo prima del trattamento mostra il raggiungimento di un elevato picco di intensit ( testa di freccia ) , che corrisponde ad unelevata concentrazione di mdc e la presenza di plateau ( freccia ) , dovuti ad una lunga permanenza del mdc nella lesione . 
b the corresponding time - intensity curve shows an elevated peak of intensity ( arrow ) due to high concentration of contrast material and plateaus ( arrow heads ) due to retention of the contrast material in the lesion . 
b la curva intensit / tempo prima del trattamento mostra il raggiungimento di un elevato picco di intensit ( freccia ) , che corrisponde ad unelevata concentrazione di mdc e la presenza di plateau ( teste di freccia ) , dovuti ad una prolungata permanenza del mdc nella lesione . 
b the corresponding time - intensity curve shows an elevated peak of intensity ( arrow ) related to the high concentration of contrast agent and plateaus ( arrowheads ) due to retention of the contrast material within the lesion . 
b la curva intensit / tempo eseguita subito dopo il trattamento mostra il raggiungimento di un elevato picco di intensit ( freccia ) che corrisponde ad unelevata concentrazione di mdc e la presenza di plateau ( teste di freccia ) , dovuto ad una prolungata permanenza del mdc nella lesione . 
b the corresponding time - intensity curve shows an elevated peak of signal intensity ( arrowhead ) related to the high concentration of contrast agent and a plateau phase ( arrow ) due to retention of the contrast in the lesion . 
b la curva intensit / tempo prima del trattamento mostra il raggiungimento di un elevato picco di intensit ( freccia ) , che corrisponde ad unelevata concentrazione di mdc e la presenza di un plateau ( testa di freccia ) , dovuto ad una lunga permanenza del mdc nella lesione . 
d la curva intensit / tempo eseguita subito dopo il trattamento mostra il raggiungimento di un elevato picco di intensit ( testa di freccia ) e la presenza di un plateau ( freccia ) , dovuto ad una prolungata permanenza del mdc nella lesione . in our study , contrast - enhanced pdus performed before treatment revealed intralesional or perilesional flow signals in all patients , so we were able to derive significant time - intensity curves . 
b gruppo di controllo ( paziente sano ) : la curva intensit / tempo eseguita in una porzione del lobo destro del fegato dimostra un basso picco di intensit ( bassa concentrazione di mdc ) ( freccia ) ed un profilo a cupola corrispondente ad un lento accumulo e lento , progressivo rilascio del mdc . performed one day after treatment revealed time - intensity curves without plateaus and with low peaks of signal intensity , confirming complete necrosis of the tumour and success of the treatment . 
this finding was confirmed by the biopsy . instead , in one patient without intralesional flow signals but with persisting perilesional flow signals and time - intensity curve characterised by plateau and high peak of signal intensity , the biopsy revealed residual neoplastic tissue . 
 non si sono verificate reazioni avverse alla somministrazione ev del mdc . discussione le curve intensit / tempo permettono lo studio del comportamento della vascolarizzazione intra e perilesionale dopo la somministrazione ev del mdc e in particolare monitorizzano landamento della concentrazione del mdc nella regione dinteresse in un tempo prestabilito . 
lesistenza di strutture vascolari intra e perilesionali di tipo neoplastico influenza il profilo delle curve in quanto la presenza di shunt artero - venosi e lassenza di sistemi sfinteriali fisiologici , tipiche dei vasi neoformati , si traduce in unintrappolamento del mdc allinterno degli stessi e quindi in una fase di wash - out caratterizzata dai plateau ( fasi stazionamento del mdc ) e presenza di elevati picchi di intensit . nel nostro studio lesame power doppler con mdc ha riscontrato la presenza di segnali vascolari intra o perilesionali in tutti i pazienti prima del trattamento intralesionale ; ci ha permesso lottenimento di curve intensit / tempo significative ; infatti la presenza di enhancement nellarea di interesse una condizione indispensabile e rappresenta quindi un limite della metodica . 
in 15 pazienti , al controllo dopo un giorno dal trattamento , sono state riscontrate curve intensit / tempo con assenza di plateau e basso picco di intensit a sostegno della necrosi completa del tumore e quindi del successo del trattamento ; ci stato confermato dalla biopsia di controllo , mentre , in un paziente che presentava assenza di segnali vascolari intralesionali e persistenza di segnali vascolari perilesionali , in cui la curva intensit / tempo mostrava profilo con plateau ed elevato picco di intensit , la biopsia confermava la persistenza di tessuto neoplastico . 
in questo ultimo caso la curva intensit / tempo ha evidenziato lincompleta necrosi tumorale anche in assenza di segnali vascolari intralesionali dopo il trattamento ; ci fa supporre che la presenza di tessuto neoplastico coinvolgeva la regione perilesionale . 
tale reperto assume notevole importanza , a nostro giudizio , poich il riscontro di una curva come la suddetta dopo il trattamento potrebbe fornire lindicazione per lesecuzione di unaltra seduta terapeutica per ottenere la completa necrosi del tumore . radiol med ( 2009 ) 114 : 3241 an indication for an additional treatment session to achieve complete necrosis of the tumour . 
 in the four patients exhibiting intralesional flow signals after treatment , the time - intensity curves were characterised by plateaus and high peaks of signal intensity , suggesting incomplete necrosis of the tumour , later confirmed by targeted biopsy . 
 the presence of plateaus and high peaks of signal intensity , which characterised all curves before treatment and those of lesions found to be positive at biopsy after treatment , might represent a pattern of neoplastic vascularity . the technique should be further evaluated on a larger number of patients . 
if our findings are confirmed , it could be proposed as an alternative to ct and mri in consideration of its numerous benefits , including limited invasiveness , rapidity , and lack of side - effects of contrast material . nei quattro pazienti che presentavano segnali vascolari intralesionali dopo il trattamento , le corrispondenti curve intensit / tempo mostravano profilo con plateau ed elevato picco di intensit a conferma dellincompleta necrosi del tumore , confermata dalla biopsia mirata . 
we initiated a prospective , blinded investigation on 29 patients affected by oncological diseases ( n = 14 ) or lymphoma ( n = 15 ) , who underwent fluorodeoxyglucose ( fdg ) - based pet - ct and whole - body dwibs for restaging purposes . 
reader 1 had a sensitivity of 89.07% , a specificity of 98.5% , and an accuracy of 97.65% , with a positive predictive value ( ppv ) of 85.48% and a negative predictive value ( npv ) of 98.91%. 
abbiamo avviato uno studio prospettico , in cieco , su 29 pazienti oncologici ( 15 con linfoma e 14 con altre neoplasie ) , che si sono sottoposte nel loro normale percorso diagnostico a tac - pet con fluro - desossi - glucosio ( fdg ) e anche ad unindagine con wb - dwibs , per restaging di malattia . 
lagreement tra i due radiologi risultata quasi perfetta ( = 0 , 93 )  . rispettivamente i due radiologi hanno avuto una sensibilit del 89 , 07% e 87 , 39% , specificit del 98 , 5% e del 98 , 39% , accuratezza diagnostica del 97 , 65% e 97 , 8% per i due lettori , ppv del 85 , 48% e 88 , 13% e npv 98 , 91 e 98 , 75% . radiol med ( 2009 ) 114 : 117 conclusions . 
un difetto dello studio sicuramente larruolamento di pazienti con lesioni multiple disseminate , leterogeneit della casistica . keywords diffusion weighted imaging whole - body pet - ct parole chiave diffusion weighted imaging whole body tc - pet introduction introduzione in oncology , tumour therapy and follow - up are strongly based on reliable diagnostic imaging techniques enabling evaluation of the entire body for disease detection and staging . 
whole - body imaging is mainly applied to screening and staging , and the role of magnetic resonance imaging ( mri ) and positron emission tomography computed tomography ( pet - ct ) among whole - body imaging techniques has been well assessed in the literature [ 1 ]  . whole - body mri , intended as a conventional mri technique , has excellent tissue contrast and high spatial resolution and allows detailed morphological evaluation . 
these properties make it particularly suited to the study of bone marrow , very sensitive in detecting and locating skeletal metastasis and superior to ct in depicting bone and parenchymal infiltration [ 2 ] in almost all organs ( though not yet for lung parenchyma )  . since the introduction of pet - ct in 2001 , anatomicmetabolic studies have been found to be extremely sensitive in characterising lymph nodes and detecting metastasis . however , they also tend to be affected by false - positive results mainly related to brown fat , muscle tissue or inflammatory processes given that fluorodeoxyglucose ( fdg ) is not entirely a cancer - specific tracer . 
in addition , bowel muscular activity and urinary tract excretion hinder the interpretation of studies of the gastrointestinal and urinary system [ 3 ]  . the other whole - body technique , 99mtc - phosphonatebased skeletal scintigraphy ( or bone scan ) , is the standard nuclear - medicine method for the initial staging of primary or secondary bone tumours . 
however , it provides limited anatomical detail , has low sensitivity and specificity and only depicts bone metastasis at a relatively late stage when osteoblastic reaction to tumour deposits has already occurred [ 49 ]  . diffusion - weighted imaging ( dwi ) , a validated technique for mr evaluation of the brain , has recently been in oncologia , la terapia ed il controllo della risposta ad essa ( follow - up ) sono strettamente legati alla disponibilit di metodiche di imaging diagnostico , che permettano lanalisi di tutti i distretti corporei potenzialmente interessati dalla patologia e dalla sua diffusione ( whole - body ) , e che siano affidabili nel riconoscere e stadiare la patologia . 
per essere appropriato , lo screening di secondo e terzo livello deve disporre di una metodica caratterizzata da elevata specificit , applicata su una patologia ad elevata prevalenza nella popolazione . 
limaging whole - body ( whole body imaging , wbi ) orientato pertanto principalmente a scopi di screening e staging ; in letteratura [ 1 ] , ben assodato il ruolo dellimaging con risonanza magnetica ( whole body magnetic resonance imaging , wb - mri ) e della tomografia computerizzata abbinata alla tomografia ad emissione di positroni ( tc - pet )  . 
 per wb - mri , si intende lapplicazione total - body della tecnica rm convenzionale ; tale tecnica caratterizzata da eccellente risoluzione di contrasto ed alta risoluzione spaziale , permette una valutazione morfologica dettagliata ; queste caratteristiche rendono la metodica particolarmente idonea allo studio del midollo osseo , molto sensibile nella individuazione e localizzazione delle metastasi scheletriche , superiore alla tc nella definizione dellinfiltrazione ossea e parenchimatosa [ 2 ] , per quasi tutti gli organi ( allo stato attuale , non per il parenchima polmonare )  . dallintroduzione della tc - pet nel 2001 , lo studio anatomo - funzionale risultato particolarmente sensibile per la caratterizzazione dei linfonodi e delle metastasi , sebbene limitato da false positivit . 
queste ultime sono generate prevalentemente dal grasso bruno , da processi infiammatori o da tessuti muscolari metabolicamente attivi , dal momento che il marcatore metabolico il fluorodesossi - glucosio ( fdg ) , marker non specifico per lattivit cellulare neoplastica ; inoltre lattivit muscolare intestinale e lescrezione urinaria del metabolita rendono di difficile interpretazione questi due apparati [ 3 ]  . laltra principale metodica wb disponibile in medicina nucleare la scintigrafia ossea con tecnezio ( bone scan , bs ) , che rappresenta la metodica standard di staging dei radiol med ( 2009 ) 114 : 117 extended to extracranial districts [ 10 , 11 ] , although with several technical difficulties due to hardware limitations and the mobile nature of the organs to be studied . 
this is an echo planar imaging pulse sequence combined with short tau inversion recovery ( epi - stir ) suitable for evaluating extracranial districts and for whole - body imaging , partly owing to the excellent images obtained with postprocessing algorithms . apart from one congress abstract [ 13 ] , no papers have been published on the subject since takaharas report [ 12 ] , so the accuracy of whole - body dwibs in comparison with the pet - ct is as yet unknown . 
 the aim of this study was to assess the overall diagnostic accuracy of whole - body dwibs in comparison with petct , which is considered the standard of reference among whole - body imaging modalities . materials and methods patients from february 2007 to august 2007 , we enrolled 29 consecutive patients undergoing pet - ct for oncological and oncohaematological diseases ( table 1 ) and fulfilling the requisites for the study . inclusion criteria patients were eligible if they met the following criteria : 1 . 
they volunteered for the mr scan , were able to understand and sign an informed consent form informing them that : ( a ) the examination was not necessary but might tumori ossei primitivi o secondari . 
con lo sviluppo di sequenze pi veloci , insieme al potenziamento dei gradienti variabili e allintroduzione della tecnica del tavolo mobile , limaging rm pesato in diffusione , esteso allo studio di tutto il corpo diventato tecnicamente realizzabile . 
 [ 12 ] hanno messo a punto una sequenza per limaging rm pesato in diffusione , denominata diffusion weighted body imaging with background body signal suppression ( dwibs ) , una sequenza echo - planar abbinata alla soppressione del segnale del grasso con tecnica stir , ottimizzata per la valutazione dei distretti extracranici e particolarmente adatta ad un impiego whole - body , grazie anche agli ottimi risultati iconografici ottenuti con opportuni algoritmi di post - processing . 
pertanto , fino ad oggi , laccuratezza diagnostica della tecnica wb - dwibs in confronto con la tc - pet non nota . scopo del presente studio di valutare laccuratezza diagnostica della wb - dwibs in comparazione con il gold standard nellambito delle metodiche di imaging wholebody , la tc - pet . table 1 patient series grouped by type of neoplasm tabella 1 casistica raggruppata per tipologia di neoplasia primary tumour number of patients sedi del tumore primitivo numero di pazienti lymphoma lung breast kidney sarcoma primitive neuroectodermal tumour prostate linfoma polmone mammella intestino rene sarcoma pnet prostata radiol med ( 2009 ) 114 : 117 help to understand or stage their disease in the future , ( b ) the study required no contrast medium injection , ( c ) the study took 20 min , and ( d ) no ionising radiation would be used 2 . 
a q - body coil was used , with the patient positioned feet first on an extended anatomical coverage table , based on rolling - table technology ( mobitrak , philips )  . 
after a scout pulse sequence , we acquired a dwibs pulse sequence and an epi - stir single - shot pulse ( table 2 ) in the axial plane , repeated for up to four stacks to encompass all anatomical districts from the head to at least the distal thigh , similarly to the pet - ct acquisition protocol . 
we adopted two different b - factor values in the diffusion pulse sequence , b = 500 and b = 1000 s / mm2 , but only the latter was used for reading purposes , as suggested by takahara et al . 
the acquisition time for the protocol was 18 min which , summed to the scout sequence time , implied a total room occupation time of 20 min . nuclear medicine pet - ct scans were acquired on a hybrid siemens ( siemens , erlangen , germany ) system consisting of an lutetium oxyorthosilicate ( lso ) pet scanner ( hi - rez ) with pico - 3d electronics and a 16 - row ct device ( somatom sensation 16 )  . 
 image reformatting and analysis after acquisition and the choice of the higher b value , the materiali e metodi pazienti da febbraio 2007 fino ad agosto 2007 abbiamo arruolato 29 pazienti consecutivi , in previsione di eseguire una valutazione tc - pet , per patologie oncologiche , anche del distretto emolinfopoietico ( tabella 1 ) , che soddisfacevano i criteri di inclusione . criteri di inclusione i pazienti sono stati considerati reclutabili in relazione ai seguenti criteri : 1 . 
abbiamo utilizzato la bobina q - body , posizionando il paziente ( in modo che entrasse nel gantry caudocranialmente , feet first ) , su un tavolo porta - paziente a copertura anatomica estesa , basata sulla tecnologia del tavolo mobile ( mobitrak , philips )  . 
dopo una sequenza di centratura , abbiamo acquisito una sequenza dwibs ( stirecho planar , single shot ) ( tabella 2 ) sul piano assiale , ripetuta 4 volte per coprire tutti i distretti anatomici dalla testa alla coscia distale , in modo da replicare la copertura anatomica dellesame tc - pet . 
la sequenza stata pesata con un doppio valore di b ( b = 500 e b = 1000 s / mm2 ) , utilizzando solo il secondo per la refertazione , come suggerito da takahara et al . 
al termine , si provveduto a invertire la scala dei grigi , in modo che su sfondo bianco ( le aree prive di segnale ) si potesse riconoscere la patologia come immagini con diverse intensit di grigio ( le aree con segnale accentuato ) , con tutte le gradazioni intermedie . 
le immagini whole - body mip e mpr cos elaborate sono state poi salvate nel database dello scanner . anche le immagini native assiali sono state separate sulla base del parametro b , e quelle con b = 1000 s / mm2 , dopo aver preparato la finestra di visualizzazione in modo ottimale , sono state salvate nel database delle immagini . 
tutte le immagini , elaborate da un medico specializzando esperto , sono state private delle informazioni anagrafiche e salvate su una memoria di massa mobile ( cd ) , in formato dicom , registrando ogni supporto con il numero progressivo del paziente . 
le sessioni di refertazione sono state condotte , indipendentemente , da due radiologi esperti in rm ( a.s , lettore 1 e a.c. lettore 2 ) , rispettimente con 8 e 18 anni di pratica professionale in rm , reciprocamente inconsapevoli del risultato della refertazione dellaltro , e del risultato della lettura della tc - pet . i due radiologi hanno riempito una scheda di lettura predefinita , costituita da un foglio elettronico ( excel , microsoft , redmond , usa ) , nel quale sono state individuate 40 sedi anatomiche , scheletriche e viscerali , basandosi su unanaloga schematizzazione elaborata da lauenstein et al . radiol med ( 2009 ) 114 : 117 4 - mm - thick multiplanar reformations ( mpr ) in the coronal plane , and ( c ) multiple 4 - mm - thick mpr in the sagittal plane oriented to include the midline as well as the spine and paraspinal regions . 
all reformatted images were then fused by means of mobiview software ( philips ) with the smooth fusion algorithm to obtain whole - body mip and mpr images . the grey scale was subsequently inverted to allow visualisation of abnormalities ( increased signal ) as grey areas of varying intensity against a white background ( without signal )  . all of the whole - body mip and mpr images were saved in the scanners patient - image database . 
the native axial slices were separated on the basis of the b value , and those acquired with b = 1 , 000 s / mm2 were also saved in the image database after optimal window setting . 
all image sets , processed by an experienced trainee radiologist , were rendered anonymous and stored in digital imaging and communications in medicine ( dicom ) format on an optical disc marked with the patients progressive number for subsequent reading . 
images were read independently by two experienced mri radiologists ( reader 1 : as , with 8 years experience ; reader 2 : ac , with 18 years experience ) who were unaware of each others mri report and of the pet - ct results . the two readers noted their findings on a predefined reading grid consisting of a spreadsheet ( excel , microsoft , redmond , usa ) listing 40 skeletal and visceral sites and subsites , modified from the classification proposed by lauenstein et al . 
radiological reading time for each patient was also recorded . the pet - ct study was reported by the nuclear physician on a similar reading grid as that used by the radiologists . 
the nuclear physician first read the source axial pet images separately and then overlaid on axial ct images and next reviewed the coronal and sagittal images reconstructed with the mpr algorith image analysis included assessment of metabolic uptake of the tracer in terms of standardised uptake value ( suv )  . postprocessing and mean reading times were calculated . the cohen constant was calculated to determine the grade of interobserver agreement . 
for each reader , we calculated diagnostic accuracy , sensitivity and specificity of the wholebody dwibs readings together with negative and positive predictive values ( npv and ppv ) and compared the readings with those performed by the nuclear physician on the pet - ct studies . 
 lo specialista medico nucleare ha refertato lesame tcpet , su unanaloga scheda di lettura , valutando le immagini assiali pet , poi sovrapposte alle immagini tc e infine ricostruite nei piani coronale e sagittale tramite algoritmo mpr , utilizzando anche la valutazione dellintensit della captazione metabolica ( suv ) come criterio per definire patologico un reperto . statistica sono stati calcolati il tempo di post - processing e di refertazione . 
per ogni lettore , stata calcolata laccuratezza diagnostica , la sensibilit e la specificit delle letture wb - dwibs , insieme al valore predittivo negativo e positivo ( npv e ppv ) , comparando le letture dei radiologi con quella del medico nucleare eseguita sulle immagini tc - pet . risultati la tecnica wb - dwibs ha comportato un tempo di occupazione della sala rm di circa 20 minuti . 
il tempo di refertazione medio risultato di 20 minuti ( range 1525 minuti ) per il primo lettore e 18 minuti per il secondo ( range 1322 minuti )  . 
il tempo di refertazione ha avuto un trend decrescente per ognuno dei radiologi dal primo paziente fino al ventinovesimo . laccordo tra i due lettori stato quasi perfetto , con un valore di di 0 , 93 . 
i due radiologi , su 29 pazienti ( ognuno analizzato nelle 40 sedi anatomiche ) hanno considerato positive ( affette ) rispettivamente 124 e 128 sedi , delle quali 106 e 104 veri positivi ( vp ) , 18 e 14 falsi positivi ( fp ) , contro il rilievo ct - pet di positivit in 119 sedi . sono state considerate negative dai due radiologi 1196 e 1202 sedi , delle quali rispettivamente 1183 e 1187 veri negativi ( vn ) e 13 e 15 falsi negativi ( fn ) , rispetto alle 1121 sedi considerate negative dalla metodica di riferimento ( tabella 4 )  . 
quattordici dei 29 pazienti hanno avuto un responso esattamente speculare a quello della tc - pet . negli altri 15 pazienti si verificato un mismatch di lettura ( fp e fn ) da 1 a massimo 5 sedi . 
i due radiologi hanno avuto rispettivamente : il primo radiologo una sensibilit del 89 , 07% , specificit del 98 , 5% e accuratezza del 97 , 65% , con vpp e vpn di 85 , 48% e 98 , 91% ; il secondo radiologo una sensibilit del 87 , 39% , specificit del 98 , 39% e accuratezza diagnostica del 97 , 8% , con vpp del 88 , 13% e vpn del 98 , 75% . analizzando le discrepanze tra tc - pet e wb - dwibs , abbiamo rilevato rispettivamente per i due radiologi 18 e 14 falsi positivi , 13 e 15 falsi negativi , distribuiti come evidente nella tabella 5 , dove stata riportata la media tra i due radiol med ( 2009 ) 114 : 117 table 3 categorisation of skeletal and visceral sites used in the radiology report skeletal sites visceral sites skull , orbit and maxillary bones cervical spine thoracic spine lumbar spine sacrum coccyx sternum clavicle scapula humerus forearm ilium - ischium femur lower leg cranio , orbite e massiccio colonna cervicale colonna toracica colonna lombare sacro coccige sterno coste clavicola scapola omero avambraccio ilio - ischio femore arto inferiore neck neck nodes lung mediastinum pleura thoracic nodes breast axillary nodes liver adrenal glands kidneys pancreas spleen gallbladder bladder abdominal nodes retrocrural nodes female pelvis reproductive apparatus male pelvis reproductive apparatus omental / peritoneal pelvic nodes inguinal nodes soft tissues collo linfonodi del collo polmone mediastino pleura linfonodi toracici mammella linfonodi ascellari fegato surreni reni pancreas milza intestino colecisti vescica linfonodi addominali linfonodi retrocrurali pelvi femminile apparato riproduttivo pelvi maschile apparato riproduttivo omento peritoneo linfonodi pelvici linfonodi inguinali tessuti molli tabella 3 elenco delle sedi scheletriche e viscerali adottato per la scheda di lettura sedi scheletriche sedi parenchimali time of approximately 20 mpostprocessing had a mean duration of 15 min ( range 1017 min )  . 
of these sites , 106 and 104 were true positive ( tp ) and 18 and 14 were false positive ( fp ) compared with positive pet - ct findings in 119 sites . 
readers rated 1 , 196 and 1 , 202 sites , respectively , as negative , of which 1 , 183 and 1 , 187 were true negatives ( tn ) and 13 and 15 were false negatives ( fn ) compared with negative pet - ct findings in 1 , 121 sites ( table 4 )  . dallaltra parte , nelle sedi addominali e pelviche , appaiono pi concentrati i reperti di falsa positivit . 
un caso di non completa corrispondenza tra le tc - pet e wb - dwibs , quello di un paziente ( p.l. ) , affetto da sarcoma della coscia , trattato chirurgicamente e poi con chemioterapia . 
i numeri rappresntano la media tra i due lettori distribution of results distribuzione dei risultati false negative falsi negativi skull , orbit and maxillary bones sacrum sternum scapula ilium - ischium lung mediastinum thoracic nodes pancreas retrocrural nodes total thoracic spine scapula femur neck neck nodes breast axillary nodes liver adrenal glands kidneys omental / peritoneal pelvic nodes inguinal nodes soft tissues total cranio , orbite e massiccio sacro sterno scapola ileo - ischio polmone mediastino linfonodi toracici pancreas linfonodi retrocrurali totale colonna dorsale scapola femore collo linfonodi del collo mammella linfonodi ascellari fegato surreni reni omento / peritoneo linfonodi pelvici linfonodi inguinali tessuti molli totale false positive falsi positivi there was a perfect match with the pet - ct findings in 14 / 29 patients ; there was some mismatch , ranging from one site ( fp or fn ) to five sites in the same patient in the remaining 15 / 29 patients . 
 with regard to the sites of disagreement between petct and whole - body dwibs , the two readers provided 18 and 14 false - positive results and 13 and 15 false - negative results , distributed as seen in table 5 , which shows the mean between the two readers . 
table 5 shows that the spine was almost free of fp and fn results , whereas the lung - mediastinum and the skull - maxillary bones recorded more fn results than all the other areas taken as a whole . 
colour multiplanar reformation ( mpr ) fusion of pet and ct data ( a , b )  . single pet and ct axial images before coregistration and fusion ( c , d )  . 
1a - d paziente affetto da sarcoma alla coscia destra , trattato con chirurgia e chemioterapia , attualmente con riscontro di metastasi allilo sinistro e ai polmoni ( frecce ) , oltre a recidiva alla coscia controlaterale ( punta di freccia ) ; a , b fusione a colori mediante algoritmo mpr tra pet e tc ; c , d immagini assiali singole di pet e tc prima della co - registrazione e fusione . 
si notino le calcificazioni lesionali a livello dellilo polmonare ( c ) e del nodulo polmonare ( d )  . thigh sarcoma mismatch between pet - ct findings and dwibs refers to a previous treated with surgery and chemotherapy . 
nella stessa figura , si pu osservare un fp ( a livello renale ) con un mancato riconoscimento della lesione peri - cefalopancreatica , verosimilmente linfonodale ( falso negativo )  . discussione limaging rm a diffusione ( dwi ) , stato inizialmente introdotto nella pratica clinica in ambito neuroradiologico , principalmente per la valutazione dello stroke ischemico . solo recentemente il dwi stato esteso ad applicazioni rm in ambito body [ 11 ] anche per le problematiche tecniche intrinseche al distretto toraco - addominale : movimento , numerosit di interfacce tissutali , contenuto intestinale , contenuto gassoso . 
con il miglioramento tecnologico delle apparecchiature rm , con sequenze sempre pi veloci che hanno permesso lacquisizione delle immagini in respiro libero , la rm body e la diffusione a rm nello stesso ambito , sono divenute tecnicamente fattibili . 
alcuni autori [ 15 ] , inoltre , hanno dimostrato la possibilit di caratterizzare le radiol med ( 2009 ) 114 : 117 b = 500 b = 1000 fig . 
diffusion - weighted imaging with optimised background suppression pulse sequence ( dwibs ) coronal ( a ) , sagittal ( b ) and axial multiplanar reformation ( mpr ) images ( c ) at b = 1 , 000 did not confirm the pet - ct findings ( dotted circles )  . 
dwibs elaborata con mpr in coronale ( a ) , sagittale ( b ) e mpr ( c ) a b = 1000 , senza conferma dei reperti osservati in tac - pet ( circoli punteggiati )  . 
6. the same figure shows an fp result ( kidney ) and a missed , probably nodal , pericephalopancreatic lesion . discussion dwi was originally introduced into clinical practice for neuroimaging purposes and mainly for assessing stroke . lesioni maligne , in ambito body , mediante lo studio della diffusione e la misurazione quantitativa con roi posizionate su mappe adc . 
 [ 12 ] che hanno utilizzato una sequenza echo - planar single - shot accoppiata ad un impulso stir , denominata dwibs : questa sequenza ha permesso una maggiore e pi omogenea soppressione del segnale di fondo e lacquisizione con la tecnica del respiro libero , garantendo cos la possibilit di un tempo di acquisizione pi lungo e per questo con un numero maggiore di radiol med ( 2009 ) 114 : 117 fig . 
3 tac - pet : metastasi ossee diffuse ( frecce ) da primitivo ignoto . only recently has its use been extended to whole - body mr applications [ 11 ] owing to technical problems intrinsic to the thoracoabdominal area , including movement , number of tissue interfaces , bowel content and air content . 
dwi with quantitative measurement of apparent diffusion coefficient ( adc ) has been shown to be able to characterise malignant lesions in whole - body imaging [ 15 ]  . 
more recently , dwi has been improved by the introduction of dwibs , a diffusionweighted pulse sequence paired with a stir sequence [ 11 ]  . this sequence allowed greater homogeneous suppression of the background signal as well as acquisition during free breathing , thus permitting more time for the acquisition , a higher number of signal averages , a better signal - to - noise ratio ( snr ) and acquisition of thinner slices . 
the better fat suppression at the edges of the field of view ( fov ) provided by the stir sequence and the acquisition of thinner slices also allow for better mpr and mip reformamedie del campionamento del segnale , con conseguente incremento del snr e con la possibilit di acquisire sezioni pi sottili . 
in questo modo possibile ottenere migliori immagini mip e mpr , sia per le sezioni pi sottili , sia per la migliore soppressione del grasso ai margini del campo di vista indotta dallimpulso stir . 
in questi ultimi anni , la rm whole body diventata pi accessibile e tecnicamente realizzabile grazie allintroduzione commerciale della tecnologia del tavolo mobile , che insieme anche alla disponibilit del software di fusione di pi pacchetti di acquisizione in ununica immagine , ha permesso lacquisizione e la ricostruzione di immagini whole body . 
questi progressi tecnici sono stati preliminari allintroduzione della tecnica wb - dwibs , nel 2004 . ad oggi , nessuno ha comparato i risultati di questa tecnica con le metodiche di medicina nucleare come la tcpet e la scintigrafia ossea , in pazienti oncologici . 
abbiamo condotto questo studio per comparare la wb - dwibs con la tc - pet , attualmente considerata il gold standard nello staging tnm della patologia neoplastica maligna [ 16 ]  . alcune problematiche relative allimaging wb - dwi , radiol med ( 2009 ) 114 : 117 fig . 
in recent years , whole - body mri has become more accessible and easier to perform , thanks to the advent of rolling or moving table technology that , together with the availability of software allowing the fusion of multiple stacks , has made possible the acquisition and reconstruction of whole - body images . 
all these technical advances paved the way for the introduction of the whole - body dwibs technique in 2004 . to our knowledge , no published study has compared the results of whole - body dw - mri with whole - body nuclear imaging techniques ( pet - ct and bone scan ) in cancer patients . 
this study was thus conducted to compare wholebody dwibs and pet - ct , which is considered the standard of reference in the tumour - node - metastasis ( tnm ) staging system for malignancies [ 16 ]  . limitations of whole - body dwi are the huge amount of data to be postprocessed and interpreted . 
in this study , we had a mean postprocessing time of 15 min , mainly spent for window adjustments before completing image fusion and possono essere sicuramente considerate la notevole quantit di immagini da ri - elaborare nel post - processing e da interpretare . 
nel nostro studio , abbiamo riscontrato un tempo di ri - elaborazione delle immagini piuttosto lungo , circa 15 minuti , prevalentemente spesi nellottimizzazione delle finestre di visualizzazione , prima della fusione dei pacchetti e nella generazione delle ricostruzioni mip e mpr . 
il tempo di lettura medio risultato di 19 minuti , come media tra i due lettori ; le letture sono state molto concordanti e questo garantisce la riproducibilit del risultato , in quanto sembra che le immagini siano facilmente interpretate nello stesso modo da differenti lettori . i nostri risultati dimostrano che la wb - dwibs ha alta specificit ed accuratezza diagnostica ed un elevato valore predittivo negativo ( npv ) , tutti vicino al 98% , quando paragonata alla tc - pet . 
analizzando i falsi positivi e negativi della nostra casistica , si evidenziano tre macroaree critiche , che necessitano ulteriore approfondimento : la regione cranio - mascellare , la regione toracomediastinica e la regione addomino - pelvica . 
in addition , there was high interobserver agreement between the two readers . our results show that whole - body dwibs has high specificity , high accuracy and high npv ( all close to 98% ) when compared with pet - ct . 
analysing the fp and fn results of whole - body dwibs in our series , we observed three critical sites that require further investigation : the skull - maxillary bones , the lung - mediastinum and the abdominopelvic site . 
in particular , the thorax , one of the most investigated districts in cancer screening or staging , requires further investigation by means of dwi with dedicated multichannel coils and a specific pulse protocol . 
specifically , the spine was well assessed , with no fn findings , and only one fp result out of 18 tp results ( table 5 )  . sono responsabili della maggioranza dei fn e fp della nostra casistica . 
in particolare , il torace , che uno dei distretti pi esplorati per screening o staging oncologico , necessita un approfondimento ulteriore , con imaging di diffusione mediante bobine multicanale specifiche ed un protocollo con sequenza ottimizzata per la sua valutazione . invece la tecnica appare estremamente accurata nel riconoscimento di lesioni ossee del rachide e delle ossa lunghe , del cranio e del bacino , e per il rilievo di patologia linfonodale . 
nello specifico , la valutazione della colonna vertebrale appare beneficiare , senza falsi negativi e con un solo falso positivo ( tabella 5 ) su 18 rilievi patologici , delle potenzialit diagnostiche di questa nuova tecnica . 
in a e b si osservano multipli foci di alterazione del segnale a livello latero - cervicale bilaterale , a livello splenico , lomboaortico , pelvico e inguinale sinistro ( freccie nere )  . 
con le punte di freccia si osservano due foci segnalati da entrambi i radiologi a livello renale , dei quali ( a destra , punta di freccia rossa ) uno una localizzazione peri - cefalopancreatica ( errore di sede ) e uno ( a sinistra , punta di freccia verde ) un falso positivo non corrispondente a patologia . 
conferma nelle immagini tc - pet in assiale delle lesioni osservate sia in wb - dwibs che nella ricostruzione tc - pet con mpr in coronale , delle lesioni laterocervicali ( e - g , frecce tratteggiate ) , spleniche ( h - l , frecce intere ) , lombo - aortiche ( m - o , punte di freccia )  . radiol med ( 2009 ) 114 : 117 these preliminary data show that the two major clinical applications could be ( a ) bone lesion detection , and specifically screening or staging of the spine - bony pelvis , and ( b ) lymphoma staging , due to the accurate delineation of nodal disease . 
we will direct our future scientific efforts in these two directions . these data , to be confirmed on a larger number of patients , appear to point to a role for whole - body dwibs in cancer screening , staging , restaging and follow - up , given that the higher the specificity and npv , the better the technique as a screening tool . 
whole - body mri has been shown to be more accurate than pet - ct in evaluating the liver , bone and central nervous system [ 17 , 18 ]  . 
from this point of view , a comparison with pet - ct cannot substitute a comparison based on clinical and pathological follow - up or autopsic confirmation ( the true gold standard ) and , in this sense , our study is limited by a certain degree of bias . 
thus , in presenting our preliminary data , we refer to previous studies in which a direct comparison was made between mri and nuclear medicine . the main limitations of the present study inherent to its pilot nature are a heterogeneous case series , the presence of diffuse disease and the small sample size . 
even though wholebody dwibs is beginning to be used in clinical practice , the standard diagnostic workup of patients enrolled in the study was not modified on the basis of the findings of whole - body dwibs because of the lack of scientific validation . direzioni condurremo i nostri prossimi studi . 
 questi risultati , da confermare su una popolazione di pazienti pi ampia , sembrano indicare un ruolo della wbdwibs nello screening , stadiazione , ristadiazione e followup della malattia tumorale ; infatti , pi alta la specificit e il npv , migliore la tecnica per lo screening . 
osserviamo inoltre che la sensibilit non cos elevata ( < 90% ) come la specificit , sempre in riferimento alla tc - pet . la tc - pet ha comunque le sue limitazioni specifiche , in particolare riguardo ai falsi positivi [ 17 ] , che possono influenzare anche il calcolo dellaccuratezza diagnostica delle tecniche di imaging messe a confronto , e in particolare la sensibilit della wb - dwibs nel nostro studio . 
in molte forme tumorali , la tc - pet pi adatta nella individuazione del tumore ( parametro t ) e nello staging linfonodale ( parametro n ) , ma ci sono alcune forme neoplastiche che hanno scarsa captazione di fdg , come il carcinoma renale o i tumori con frequente diffusione alle ossa , al fegato e al cervello ( come il carcinoma della mammella ) , che sono pi idonei a essere studiati con metodiche whole body alternative : infatti gi stato dimostrato che la rm whole body convenzionale pi accurata della tc - pet nella valutazione del fegato , dellosso e del cervello [ 17 , 18 ]  . 
da questo punto di vista , un confronto con la tc - pet , non pu sostituire un confronto tra una metodica di imaging da validare e il follow - up clinico e patologico o autoptico , che rappresenta il vero gold standard ; pertanto i nostri risultati sono gravati da un certo margine di errore . 
gli autori fanno pertanto riferimento alla letteratura , dove il confronto tra rm e tecniche di medicina nucleare stato pi volte descritto , nel presentare questi dati preliminari . nel nostro studio , anche per le sue caratteristiche di studio pilota , principali bias possono essere considerati la casistica eterogenea , la presenza di patologia neoplastica diffusa e il campione di piccole dimensioni : attualmente stiamo estendendo lo studio ad un campione pi omogeneo , introducendo anche il follow - up clinico - patologico come standard di riferimento . 
caudana1 1diagnostic imaging unit , 2vascular surgery unit , 3orthopaedics and traumatology unit , carlo poma hospital , viale albertoni 1 , 46100 , mantua , italy correspondence to : r . 
if diagnostic uncertainty persists , a bone biopsy is indicated . the inflammatory hyperaemia caused by the ulcer deteriorates the diagnostic quality of 40%50% of mr angiography studies in the infrapopliteal region . 
sedici pazienti diabetici sono stati sottoposti da gennaio 2006 a settembre 2007 a rm del piede per sospetta osteomielite monolaterale ; in 3 / 16 vi erano alterazioni radiografiche da osteo - artropatia neuropatica di charcot . 
la rm ha elevata sensibilit per losteomielite nel piede diabetico , ma pi bassa specificit dovuta soprattutto allosteo - artropatia neuropatica di charcot ; se permane dubbio diagnostico indicata la biopsia ossea . 
liperemia flogistica causata dallulcera deteriora il 40%50% degli studi angio - rm a livello sottopopliteo : in tali casi appropriata larteriografia selettiva per la possibilit di effettuare angioplastica nella stessa seduta . 122 radiol med ( 2009 ) 114 : 121132 keywords diabetic foot osteomyelitis foot mri peripheral vascular disease mr angiography parole chiave piede diabetico osteomielite rm piede vasculopatia periferica angio - rm introduction introduzione diabetic foot complications caused by neuropathy , ischaemia and resulting infection often lead to lower limb amputation , with severe disability and a significant impact on mortality . 
early recognition of osteomyelitis is essential for guiding medical and surgical treatment , which are usually implemented in an inpatient hospital setting [ 1 ]  . ( 89% ) the diagnosis of the clinical diagnosis of the infected foot is problematic in diabetic patients : up to two - thirds of patients may not present with the classic symptoms of deep infection owing to immunodeficiency related to diabetes mellitus . even laboratory examinations are often of little help , as inflammation indices may be absent [ 2 ]  . 
bone probing through skin ulceration is a clinical test with high positive predictive value foot osteomyelitis , although its low sensitivity ( 66% ) means that negative findings do not exclude bone infections [ 3 ]  . 
as a result , diabetic patients with suspected foot osteomyelitis require musculoskeletal imaging , both for the differential diagnosis particularly with neuropathic osteoarthropathy ( charcot foot ) and for an accurate evaluation of the extension of the infection , so as to plan surgery and avoid recurrences . 
moreover , diabetologists recommend that diabetic patients with foot ulcers should always undergo a vascular study to exclude the possibility that healing is prevented by peripheral arterial disease , which often has an insidious clinical onset due to the absence of neuropathic pain [ 4 ]  . our retrospective study presents the modern imaging approach to the infected diabetic foot , emphasizing the important role of magnetic resonance imaging ( mri ) in musculoskeletal and vascular assessment performed with the objective of selecting the most appropriate treatment . le complicanze del piede diabetico causate da neuropatia , ischemia e conseguente infezione portano spesso ad amputazione darto inferiore con grave disabilit e rilevante impatto anche sulla mortalit . 
lulcera del piede rappresenta in genere il primo segnale di allarme nel paziente diabetico e tende a progredire ( 15% dei casi ) verso losteomielite , in prevalenza con meccanismo di diffusione per contiguit . 
il riconoscimento precoce dellinsorgenza di osteomielite essenziale per indirizzare il trattamento sia medico che chirurgico , entrambi in genere attuati in ambiente ospedaliero [ 1 ]  . linquadramento clinico del piede infetto risulta difficile nel paziente diabetico : infatti fino a 2 / 3 dei pazienti possono non presentare i sintomi classici di infezione profonda a causa del deficit immunitario legato al diabete mellito ; anche gli esami di laboratorio spesso non sono di aiuto in quanto gli indici di flogosi possono essere assenti [ 2 ]  . 
il sondaggio osseo con specillo attraverso lulcera cutanea rappresenta un test clinico con elevato valore predittivo positivo ( 89% ) per la diagnosi di osteomielite del piede , ma la sua negativit non esclude linfezione ossea a causa della limitata sensibilit ( 66% ) [ 3 ]  . 
dunque nei pazienti diabetici con sospetta osteomielite del piede le metodiche di imaging muscolo - scheletrico sono necessarie sia per la diagnosi differenziale in particolare con losteo - artropatia neuropatica del piede di charcot sia per laccurato bilancio di estensione dellinfezione , cos da pianificare lintervento chirurgico ed evitare le recidive . 
inoltre , i diabetologi raccomandano di sottoporre sempre a studio vascolare il piede diabetico ulcerato , per escludere che larteriopatia periferica con esordio clinico spesso insidioso per lassenza di dolore dovuta alla neuropatia possa impedire la guarigione dellinfezione [ 4 ]  . lo scopo del nostro studio retrospettivo quello di presentare il moderno approccio imaging al piede diabetico infetto , sottolineando limportanza del ruolo che la risonanza magnetica ( rm ) ha avuto nella nostra esperienza nella valutazione muscolo - scheletrica e vascolare ai fini della scelta terapeutica ottimale . materials and methods materiali e metodi between january 2006 and september 2007 , 16 diabetic patients ( 11 men and five women , mean age 58 years , range 4278 ) with unilateral infected ulcer affecting the forefoot in ten cases , the midfoot in two and the hindfoot in four ( table 1 ) underwent mri of the foot . 
all patients underwent plain radiography of the foot , which was positive for osteomyelitis in 7 / 16 patients owing to the presence of corticoperiosteal thickening and / or of osteolytic foci in the cortical spongiosa close to the skin ulcer . 
tutti i pazienti sono stati sottoposti ad esame radiografico del piede , ritenuto positivo per osteomielite in 7 / 16 pazienti in base alla presenza di ispessimento cortico - periosteale e / o di focolai di osteolisi cortico - spongiosa in adiacenza allulcera cutanea . 
t1 - weighted spin - echo all musculoskeletal mri examinations were conducted with a 1.5 - tesla superconductive unit ( magnetom avanto : siemens ag medical solutions , erlangen , germany ) and an extremity coil . 
the mri protocol , selected on the basis of clinical suspicion and ulcer site , was different for studies of the forefoot compared with those of the midfoot and hindfoot and used a flex surface coil , a smaller field of view ( fov ) and predominantly coronal scans perpendicular to the metatarsal bones as recommended in the literature ( se : tr / te / fa 775 / 10 / 90 ) sequences and short - tau inversion - recovery sequences ( stir : tr / te / ti 5160 - 5760 / 53 / 150 ) were obtained in at least two planes , one of which was always sagittal , for selective fat suppression . 
in a few cases , a double t2and proton - density - weighted turbo - spin - echo sequence ( tse : tr / te / fa 3380 / 11103 / 150 ) was also obtained in the sagittal plane . 
parameters included 3 - mm slice thickness , 0.3 - mm interval for the t1 - weighted se sequences and 0.9 - mm interval for the stir sequences , and 16to 20 - cm fov . 
enhancement was assessed with a t1 - weighted tse sequence with selective ( tse - fs : tr / te / fa 791 / 10 / 150 ) with the same localization parameters as the stir sequences . fat suppression based on the suspicion of peripheral arteriopathy , 12 / 16 patients with infected diabetic foot also underwent mr angiography of the lower limbs with paramagnetic contrast agent ( table 1 ) 3 days to 6 weeks after mri of the foot , using the same scanner . 
this technique , through parallel imaging with dedicated phasedarray coils and high performing gradients , allows acquisithree peripheral arterial regions ( aortoiliac , tion of femoropopliteal , infrapopliteal ) within 42 s only ( excluding table motion )  . 
t1 - weighted 3d fast gradient - recalled - echo ( 3d fast - gre ) sequences were acquired in the coronal plane before and after administration of contrast material to allow subsequent subtraction . 
gadoliniumbenzyloxyproprionic - tetraacetic acid ( gd - bopta ) ( multihance , bracco , milan , italy ) at a dose of 0.15 mmol / kg , equivalent to 0.3 ( 3 / 9 oss . ) erano prevalenti le alterazioni dellosteo - artropatia neuropatica di charcot ( osteorarefazione , fratture , frammentazione ossea , lussazione , reazione osteoblastica riparativa )  . 
un paziente con ulcera del retropiede ed esame radiografico negativo stato sottoposto a biopsia ossea tcguidata del calcagno per interpretare il quadro rm dubbio . la diagnosi finale di osteomielite o la sua esclusione stata ottenuta integrando i rilievi clinico - laboratoristici con quelli imaging in tutti casi ; in 11 / 16 pazienti la diagnosi stata completata con esame batteriologico e / o istologico . tutti gli esami rm muscolo - scheletrici sono stati effettuati con apparecchiatura superconduttiva da 1 , 5 tesla ( magnetom avanto , siemens ag medical solutions , erlangen , germania ) e bobina da estremit . 
il protocollo rm , scelto sulla base del sospetto clinico e della sede dellulcera , stato diverso per lo studio dellavampiede rispetto a quello del medio e retropiede , impiegando bobina flex di superficie , fov pi piccolo e acquisizioni prevalenti sul piano coronale ovvero perpendicolare ai metatarsi come raccomandato in letteratura [ 5 ]  . 
sono state acquisite almeno in due piani , di cui uno sempre sagittale sequenze spin - echo t1 - pesate ( se : tr / te / fa 775 / 10 / 90 ) , sequenze short - inversion - time inversion - recovery per la selettiva soppressione del segnale adiposo ( stir : tr / te / ti 51605760 / 53 / 150 )  . 
in alcuni casi stata acquisita anche la sequenza turbo - spin - echo a doppia pesatura t2 e densit protonica ( tse : tr / te / fa 3380 / 11103 / 150 ) sul piano sagittale . 
sono stati impiegati spessore di fetta 3 mm , intervallo di 0 , 3 mm per le se t1 - pesate e di 0 , 9 mm per le stir , fov compreso tra i 16 cm ed i 20 cin tutti i pazienti lo studio rm stato completato con somministrazione di mezzo di contrasto ( mdc ) paramagnetico per via endovenosa ( dotarem , guerbet , aulnay - sous - bois , francia ) alla dose di 0 , 1 mmol / kg equivalente a 0 , 2 ml / kg ; lenhancement stato valutato con sequenza turbo - spin - echo t1 - pesata a selettiva soppressione del segnale adiposo ( tse - fs : tr / te / fa 791 / 10 / 150 ) con gli stessi parametri di centratura delle sequenze stir . nel sospetto di arteriopatia periferica 12 / 16 pazienti con piede diabetico infetto hanno effettuato anche lo studio angio - rm degli arti inferiori con mdc paramagnetico ( tabella 1 ) , a distanza di tempo variabile ( range : 3 giorni6 settimane ) dallesame rm del piede , utilizzando la stessa apparecchiatura rm . 
langio - rm degli arti inferiori stata effettuata con tecnica bolus - chase a tavolo mobile [ 6 ] : tale tecnica , grazie alla disponibilit dellimaging parallelo con bobine phased - array dedicate e di gradienti pi performanti , consente lacquisizione di 3 distretti arteriosi periferici ( aorto - iliaco , femoro - popliteo , infra - popliteo ) nellarco di soli 42 secondi ( escluso il movimento del tavolo )  . 
le sequenze fast - gradient - recalled - echo tridimensionali ( 3d fast - gre ) t1 - pesate sono state acquisite sul piano coronale prima e dopo somministrazione di mdc per consentire la successiva sottrazione . 
la somministrazione per via endovenosa di gadolinio - bopta ( multihance , bracco , milano , italia ) alla dose di 0 , 15 mmol / kg , equivalente a 0 , 3 ml / kg , radiol med ( 2009 ) 114 : 121132 ml / kg , was administered as an intravenous bolus ( 20 ml on average ) using a two - phase flow injector ( the first half at 1.2 ml / s , the second half at 0.6 ml / s ) , followed by the injection of 20 ml of saline at a flow rate of 1 ml / s . 
acquisition of the 3d gre sequences started when the care bolus technique detected the arrival of the contrast bolus in the aorta . during the postprocessing stage , after the subtraction process , panoramic coronal maximum intensity projection ( mip ) reconstructions were obtained from the aorta to the foot arteries by creating a composite image of the three regions . three radiologists retrospectively reviewed the mri images from the musculoskeletal study of the foot ( ur , ev , rc ) and the vascular study ( ur , at , rc )  . 
the most experienced radiologist ( rc > 15 years ) was considered the reference standard in the event of disagreement among less experienced radiologists ( ur , ev , at < 5 years )  . 
a primary sign of osteomyelitis on mri is evidence of low - signal - intensity areas in the bone marrow on t1 - weighted se images , with higher signal intensity on stir images and enhancement after contrast administration . 
secondary signs are identified close to the altered bone marrow signal and include oedema caused by septic inflammation ( cellulitis or phlegmon ) , soft - tissue abscess , skin ulcer and fistula , with possible interruption of the cortical bone . 
mr angiography of the lower limbs assessed the patency or stenosis - occlusion of the peripheral arteries and the presence of venous contamination artifacts superimposed enhancement of the venous circulation which is one of the main limitations of the technique , as it deteriorates the diagnostic quality of the images . 
with this assessment , the images of each of the three vascular regions were judged as either adequate or inadequate for peripheral revascularization . avvenuta in bolo ( in media 20 ml ) tramite iniettore con velocit di flusso bifasica ( la prima met a 1 , 2 ml / s , la seconda met a 0 , 6 ml / s ) , seguita dalla iniezione di 20 ml di soluzione salina con flusso di 1 ml / s . 
la diagnosi rm di osteomielite stata formulata sulla base della concordanza di segni primari e secondari [ 7 ] : la semeiotica rm della osteomielite considera come segno primario la presenza a livello del tessuto osteo - midollare di aree di ridotta intensit di segnale nelle immagini se t1pesate , con incremento dellintensit di segnale in quelle stir ed enhancement dopo somministrazione di mdc paramagnetico , mentre i segni secondari sono quelli rilevabili in adiacenza allalterazione del segnale osteo - midollare e comprendono ledema dovuto alla flogosi settica ( cellulite o flemmone ) , lascesso dei tessuti molli , lulcera cutanea e la fistola con leventuale interruzione della corticale ossea . nelle indagini angio - rm degli arti inferiori sono state valutate la perviet o la steno - occlusione delle arterie periferiche e la presenza di artefatti da contaminazione venosa ovvero lenhancement sovrapposto del circolo venoso uno dei principali limiti in quanto riduce la qualit diagnostica dellesame . 
i reperti angio - rm evidenziati sulle ricostruzioni mip sono stati analizzati per conferma anche nelle sequenze sottratte con software 3d ; cos valutate , le immagini di ciascuno dei tre distretti vascolari esaminati sono state giudicate sufficienti o insufficienti per la scelta del trattamento di rivascolarizzazione periferica . 
 results risultati in 13 / 16 patients with infected diabetic foot ulcers , the final diagnosis was osteomyelitis , whereas in 3 / 16 patients it was cellulitis ( table 1 )  . 
a the sagittal short - tau inversion - recovery sequence ( stir ) image shows a pathological fracture of the calcaneus and dislocation of the proximal fragment due to retraction of the achilles tendon . 
b magnetic resonance angiography ( mra ) of the right lower limb is hindered by venous contamination in the distal third , whereas the left infrapopliteal arteries are clearly visible up to the plantar arch . 
the mri diagnosis of exclusion of osteomyelitis proved correct in two patients with infected ulcer and cellulitis ( true negatives ) in whom conventional radiology had identified alterations due to neuropathic osteoarthropathy . 
overall , foot mri permitted correct identification or exclusion of osteomyelitis in 15 / 16 patients , with a high accuracy and sensitivity , even in the presence of radiographic evidence of neuropathic osteoarthropathy ( three cases )  . 
mri also proved useful for assessing the extent of osteomyelitis for surgical planning purposes ( four minor and one major amputation ) , for identifying soft - tissue abscesses requiring drainage ( three cases ) as well as other infectious complications including septic arthritis ( four cases ) , pathological fracture ( one case , fig . 1a ) and septic tenosynovitis ( one case )  . non da flogosi settica del tessuto osteo - midollare . 
2a - c reactive bone marrow oedema of the talus and calcaneus due to neuropathy in a diabetic patient with mal perforans and normal radiographic findings [ false - positive magnetic resonance imaging ( mri ) diagnosis of osteomyelitis ]  . 
a the coronal t1 - weighted turbo - spin - echo ( tse ) image with fat suppression after administration of paramagnetic contrast material reveals diffuse changes in signal intensity of bone marrow and soft tissues , as well as moderate contrast enhancement in the talus and in the subtalar portion of the calcaneus , wrongly interpreted as osteomyelitis associated with cellulitis . 
b in the axial short - tau inversion recovery ( stir ) image , the area of increased signal intensity in the calcaneus is identified to perform a bone biopsy . 
2a - c edema osteo - midollare reattivo talo - calcaneare da neuropatia in paziente diabetico con mal perforante e quadro radiografico normale ( errore rm di falsa positivit per la diagnosi di osteomielite )  . 
a nellimmagine coronale tse t1 - pesata con soppressione del segnale adiposo dopo somministrazione di mdc paramagnetico diffuse alterazioni del segnale osteo - midollare e dei tessuti molli in sede talare e nella porzione subtalare del calcagno caratterizzate da discreto enhancement , erroneamente interpretate come osteomielite associata a cellulite . 
c la biopsia ossea sotto guida tc ha escluso linfezione ossea . regions , the diagnostic patients with infected diabetic foot allowed evaluation of the diagnostic quality of the images obtained in the three vascular regions . 
these five patients later underwent selective arteriography of the ulcerated lower limb with an anterograde approach , owing to a suspicion of concomitant distal diabetic arterial disease ( table 1 )  . 
in 4 / 5 patients , arteriosclerotic occlusive lesions of the crural arteries were identified , and percutaneous transluminal angioplasty ( pta ) was performed during the same session . after the mr angiography , 9 / 12 patients underwent three of whom had a surgical vascular surgery , effettuati in 12 pazienti con piede diabetico infetto ha permesso di valutare la qualit diagnostica delle immagini ottenute in ciascuno dei tre distretti vascolari esaminati . 
questi 5 pazienti sono stati successivamente sottoposti ad arteriografia selettiva con approccio anterogrado dellarto inferiore affetto dallulcera , nel sospetto di concomitante arteriopatia diabetica distale ( tabella 1 )  . 
in 4 / 5 pazienti sono state riscontrate lesioni arteriosclerotiche steno - occlusive delle arterie crurali e si proceduto ad angioplastica ( pta ) nella stessa seduta . complessivamente 9 / 12 pazienti sono stati sottoposti dopo lo studio angio - rm a intervento vascolare , di cui 3 mediante by - pass chirurgico femoro - popliteo e 6 con tratta128 radiol med ( 2009 ) 114 : 121132 fig . 
3a - c severe charcot neuropathic osteoarthropathy , infected plantar ulcer and bone infarcts due to peripheral arterial disease [ osteomyelitis excluded by magnetic resonance imaging ( mri ) ]  . 
3a - c grave osteo - artropatia neuropatica di charcot , ulcera infetta plantare e infarti ossei da arteriopatia periferica ( rm negativa per osteomielite )  . a nel radiogramma in incidenza antero - posteriore frammentazione ossea del medio - piede in fase cronica con tipica frattura - dislocazione di lisfranc . 
liperintensit di segnale a livello del primo e secondo dito dovuta ad un artefatto ( insufficiente soppressione del segnale adiposo alla periferia della bobina da estremit )  . femoropopliteal bypass , and six underwent endovascular angioplasty ( three the femoropopliteal and infrapopliteal regions , three in the infrapopliteal region only ) with immediate technical success in 5 / 6 cases . in both mento endovascolare di angioplastica ( 3 a livello sia femoro - popliteo che infra - popliteo , 3 solo in sede infrapoplitea ) con successo tecnico immediato in 5 / 6 casi . discussion conventional radiology is still the first - line modality in the study of the diabetic foot owing to its rapidity , ease of use and inexpensiveness . 
it also allows the diagnosis of clinically overt osteomyelitis , reveals alterations due to charcots neuroarthropathy and is useful for the follow - up . known limits of conventional radiology , especially if performed in the early stage of bone infection , are its low sensitivity ( 60% ) and specificity ( 66% ) [ 8 ]  . 
the former is due to a need for 30%50% bone reabsorption , a process taking up to 23 weeks from the onset of infection , whereas the latter depends on the wide spectrum of diseases entering the differential diagnosis , first of all neuropathic discussione lindagine radiologica convenzionale rimane la metodica di primo livello per lo studio del piede diabetico per rapidit , facilit di esecuzione e bassi costi : oltre a permettere la diagnosi di osteomielite nella fase conclamata rileva le alterazioni da osteo - artropatia neuropatica di charcot ed utile per il follow - up . 
i limiti noti dellindagine radiologica , specie se espletata nelle prime fasi dellinfezione ossea , sono la bassa sensibilit ( 60% ) e specificit ( 66% ) [ 8 ] ; la prima dovuta alla necessit di un riassorbimento osseo pari al 30%50% , processo che impiega fino a 23 settimane dallinizio dellinfezione , mentre la seconda dipende dallampio spettro di patologie coinvolte nella diagnosi differenziale , prima fra tutte losteo - artropatia neuropatica che colpisce fino al 3% dei pazienti diabetici . 
the midfoot and hindfoot bones are the most commonly involved by this disease , which presents with demineralization , fractures , fragmentation , joint dislocation and collapse of the plantar arch , with the classic charcot deformity . 
the use of more sophisticated imaging modalities ( either mri or scintigraphy ) is indicated when radiography demonstrates alterations due to charcot neuroarthropathy or whenever the clinicallaboratory suspicion of osteomyelitis is high , or finally to demonstrate complications . 
bone biopsy , although not routinely performed because of its invasiveness , is considered the gold standard in the diagnosis of osteomyelitis and is still recommended to confirm an uncertain diagnosis and isolate the pathogen [ 9 ]  . mri has come to replace ct , as it is better able to identify bone marrow changes and evaluate septic involvement of the soft tissues , which allows surgery to be planned in such a way as to prevent recurrence of infection after amputation or abscess drainage [ 10 ]  . 
it is thus reserved for patients with contraindications to mri or with doubtful mri findings , or to assess response to antibiotic therapy during the follow - up [ 9 ]  . 
when there is topographic concordance between the primary and secondary mri signs , the mean reported sensitivity and mediopiede e del retropiede sono quelle pi spesso coinvolte da questa patologia che si manifesta con demineralizzazione , fratture , frammentazione , lussazione articolare fino al collasso dellarcata plantare , con la classica deformit del piede di charcot . 
il ricorso a metodiche di imaging pi sofisticate ( rm o scintigrafia ) indicato quando lesame radiologico riscontri alterazioni da osteo - artropatia neuropatica di charcot oppure qualora il sospetto di osteomielite sia elevato dal punto di vista clinico - laboratoristico o , infine , per evidenziare le complicanze dellinfezione . 
la biopsia ossea , bench non praticata di routine a causa dellinvasivit , tuttoggi considerata il gold standard per la diagnosi di osteomielite e viene dunque ancora raccomandata per confermare una diagnosi dubbia e per isolare lagente patogeno [ 9 ]  . la rm oggi ha sostituito la tc per la migliore capacit di identificare le alterazioni osteo - midollari e di valutare il coinvolgimento settico dei tessuti molli , ci che consente di pianificare gli interventi chirurgici al fine di evitare recidive infettive dopo amputazione o drenaggio di ascessi [ 10 ]  . la scintigrafia con granulociti tecneziati presenta accuratezza lievemente inferiore a quella della rm nella diagnosi di osteomielite [ 11 ] e risulta pi indaginosa e costosa ; viene attualmente pertanto riservata ai pazienti che hanno controindicazioni alla rm oppure in quelli con quadro rm dubbio o , infine , nel follow - up per valutare la risposta alla terapia antibiotica [ 9 ]  . 
la rm rappresenta pertanto lindagine preferenziale di secondo livello per la diagnosi di osteomielite : qualora vi sia concordanza topografica tra segni rm primari e secondari i valori medi di sensibilit e 130 radiol med ( 2009 ) 114 : 121132 specificity are 94% ( range 88%99% ) and 83% ( range 78%89% ) , respectively [ 2 , 7 ]  . 
on the other hand , a positive mri study is not always sufficient to establish a diagnosis of osteomyelitis , even when there is topographic concordance between primary and secondary signs . 
administration of paramagnetic contrast material increases specificity because enhancement of bone marrow , as assessed in the t1weighted sequences with selective fat suppression , is regarded as typical of osteomyelitis rather than of neuropathic osteoarthropathy [ 12 ]  . 
nonetheless , some authors have found that neuropathy - related reactive bone marrow oedema often associated with trabecular microfractures and joint effusion may also enhance , thus becoming indistinguishable from osteomyelitis [ 13 ]  . 
 the differential diagnosis between osteomyelitis and neuropathic osteoarthropathy is not a problem when the skin is intact but only when stress - related biomechanical alterations promote skin ulceration and the foot appears swollen , warm and erythematous . 
 in the chronic phase of neuropathic osteoarthropathy , subchondral cysts , osteoporosis and bone fragmentation may appear , with loss of articular relationships and subsequent endosteal and periosteal reparative bone proliferation , which are easily detected even on conventional radiology . in these cases , mri can usually be interpreted correctly if compared with the radiographic pattern [ 1214 ]  . 
the ankle - arm index ( aai ) may overestimate systolic pressure owing to calcified sclerosis of the tunica media hindering compression of the arteries , transcutaneous oximetry may be misleadingly low due to the presence of oedema and , finally , colour doppler ultrasound may not allow adequate evaluation of the infrapopliteal arterial region , the most commonly affected by diabetic arterial disease [ 4 ]  . 
 in genere la rm permette di escludere con affidabilit losteomielite se negativa o se lalterazione del segnale osteo - midollare lontana dallulcera , ma non sempre sufficiente a formulare diagnosi di osteomielite quando positiva , anche se vi concordanza topografica tra i segni rm primari e quelli secondari . 
la somministrazione di mdc paramagnetico risulta utile per aumentare la specificit dellesame dato che lenhancement del tessuto osteo - midollare , valutato nelle sequenze t1 - pesate con selettiva soppressione del segnale adiposo , considerato tipico dellosteomielite pi che delle alterazioni dovute a osteo - artropatia neuropatica [ 12 ]  . 
tuttavia , alcuni autori hanno riscontrato la possibilit che in alcuni casi ledema midollare reattivo da neuropatia spesso associato a micro - fratture trabecolari e versamento articolare possa presentare enhancement , risultando indistinguibile dallosteomielite [ 13 ]  . 
 il problema della diagnosi differenziale tra osteomielite e osteo - artropatia neuropatica non si pone quando la cute integra , ma solo quando le alterazioni bio - meccaniche dovute al carico favoriscono lulcerazione della cute ed il piede appare tumefatto , caldo , eritematoso ; in tale fase acuta la neuro - artropatia pu simulare losteomielite sia dal punto di vista clinico che radiologico . 
pertanto , in tutti i casi con rm positiva , ma discordante dai dati clinici , colturali , laboratoristici e radiologici , necessario ricorrere alla biopsia ossea per conferma , utilizzando la guida fluoroscopica o tc per raggiungere la sede della alterazione del segnale rm , scegliendo un tragitto che attraversi la cute integra , al fine di evitare la possibile contaminazione ossea [ 9 ]  . 
 nellosteo - artropatia neuropatica fase cronica possono comparire cisti subcondrali , osteoporosi e frammentazione ossea con perdita dei rapporti articolari e successiva proliferazione ossea riparativa endo e periosteale , facilmente rilevabili gi allesame radiologico convenzionale . 
 le indagini strumentali vascolari pi comunemente utilizzate per lo screening dellarteriopatia periferica presentano alcuni limiti nel paziente diabetico con osteomielite del piede : lindice caviglia - braccio ( abi ) pu sovrastimare la pressione sistolica per la sclerosi calcifica della tunica media che rende le arterie non comprimibili , lossimetria trans - cutanea pu essere falsamente bassa per la presenza di edema in corso di infezione e , infine , leco - color doppler radiol med ( 2009 ) 114 : 121132 quently , mr angiography plays a crucial role in these highrisk patients , allowing a noninvasive panoramic study of the lower - limb arteries [ 15 ]  . 
the advantages of mr angiography over ct angiography are the low nephrotoxicity of paramagnetic contrast agents , the absence of exposure to ionizing radiation and easier and more accurate postprocessing , especially in patients with diffuse wall calcifications [ 16 ]  . 
 until recently before the implementation of parallel imaging that significantly reduces acquisition times one of the major limits of lower - limb mr angiography was the filling of the venous circulation at the infrapopliteal level , which rendered up to 43% of mr angiography studies nondiagnostic [ 17 ]  . 
there is evidence that cellulitis and ulcers are the only two circumstances capable of significantly accelerating the transit time of contrast material through the peripheral arteries [ 18 ]  . 
in our experience , within the limits shown in the infrapopliteal region , mr angiography proved adequate for planning surgical or endovascular treatment , allowing healing of the ulcer and infection or identification of the level of amputation for critical limb ischaemia . conclusions pu non consentire una adeguata valutazione del distretto arterioso infra - popliteo , il pi frequentemente colpito dallarteriopatia diabetica [ 4 ]  . 
dunque , langio - rm ha assunto un ruolo cruciale in questi pazienti ad alto rischio , consentendo la valutazione panoramica arteriosa degli arti inferiori in maniera non invasiva [ 15 ]  . 
i vantaggi dellangiorm rispetto allangio - tc sono rappresentati dalla bassa nefrotossicit dei mdc paramagnetici , dallassenza di esposizione radiante e dal post - processing pi facile ed accurato , specie nei pazienti con estese calcificazioni parietali [ 16 ]  . 
 fino a pochi anni fa , prima dellapplicazione dellimaging parallelo che permette di ridurre sensibilmente i tempi di acquisizione , uno dei limiti maggiori dello studio angio - rm degli arti inferiori era rappresentato dal riempimento del circolo venoso a livello infra - popliteo : fino al 43% degli esami angio - rm risultavano non diagnostici [ 17 ]  . 
nella nostra esperienza langio - rm , pur con i limiti evidenziati a livello del distretto infrapopliteo , risultata idonea a pianificare la strategia di trattamento chirurgico o endovascolare per permettere la guarigione dellulcera e dellinfezione o comunque a individuare il livello di amputazione nellischemia critica di arto . mri of the diabetic foot is highly sensitive in the study of osteomyelitis and infectious complications . 
bolus - chase mr angiography of the lower limbs is the preferred vascular study in diabetic patients for planning peripheral revascularization . inflammatory hyperaemia of the diabetic foot , however , affects visualization of the infrapopliteal arteries in around 40%50% of limbs with infected ulcers . 
in these cases , in the presence of known patency of the femoropopliteal axis , the use of selective arteriography is justified by the opportunity to perform angioplasty during the same session . conclusioni la rm del piede diabetico ha elevata sensibilit per losteomielite e per le complicanze infettive . 
nei casi dubbi la biopsia ossea con guida imaging resta lunica indagine in grado di discriminare i casi di falsa positivit alla rm dovuti a osteo - artropatia neuropatica di charcot . 
parisi1 1department of radiation oncology , scientific institute hospital casa sollievo della sofferenza , san giovanni rotondo , 71013 foggia , italy 2university of bari , department of radiology , bari , italy 3university of foggia , department of radiology , scientific institute hospital casa sollievo della sofferenza , san giovanni rotondo , 71013 foggia , italy correspondence to : g . 
a systematic review of external radiation therapy studies in urinary cancers was performed . this synthesis of the literature is based on data from metaanalyses , randomised and prospective trials and retrospective studies . 
there are several reports on multimodality treatment in invasive bladder cancer : intravesical surgery and neoadjuvant chemotherapy to radiotherapy or concomitant radiochemotherapy with organ preservation . the conclusions reached for renal cancer are controversial , and data on cancers of the urethra and ureter are few and inconclusive . 
sufficient data now exist in the literature to demonstrate that conservative management with organ preservation is a valuable alternative to radical cystectomy , the traditional gold standard , in invasive bladder cancer , keywords urinary cancers treatment radiotherapy ( rt ) chemotherapy ( ct ) organ preservation overall survival ( os ) riassunto i tumori invasivi del tratto urinario sono relativamente rari ed il loro trattamento pu causare importanti cambiamenti nelle funzioni sessuali , sociali ed urinarie . 
ci sono pochi studi clinici controllati che hanno utilizzato la radioterapia adiuvante o radicalechemioterapia nei tumori del rene , degli ureteri e delluretra ; ci sono diversi studi sul trattamento multimodale del carcinoma invasivo della vescica : chirurgia intravescicale e chemioterapia neoadiuvante alla radioterapia o radio - chemioterapia concomitante con preservazione dellorgano . 
le conclusioni raggiunte sul carcinoma renale sono controverse ; i dati sul carcinoma degli ureteri e delluretra sono pochi e inconclusivi ; invece , vi sono ora in letteratura dati sufficienti che dimostrano come lapproccio con preservazione dellorgano , per il carcinoma vescicale invasivo rappresenta una valida alternativa alla cistectomia radicale , considerata per lungo tempo il gold standard . parole chiave tumore urinario trattamento radioterapia ( rt ) chemioterapia ( ct ) preservazione dellorgano sopravvivenza globale ( sg ) radiol med ( 2009 ) 114 : 7082 introduction surgery is the primary therapeutic option in the curative treatment of clinically localized urinary cancer . 
preoperative irradiation with doses of 2040 gy has been used to facilitate resection , to sterilise well - oxygenated peripheral extensions of the tumour that might be transected during nephrectomy , and to decrease the chance of dissemination at the time of nephrectomy . 
no advantage has been demonstrated in patients receiving preoperative irradiation with doses of 2040 gy with respect to overall survival ( os ) or survival free from distant metastases ( ffdm ) , although improvement in resectability has been noted [ 16 ]  . 
two studies [ 10 , 12 ] have reported excessive bowel and hepatic complications and an irradiation - related mortality rate of 13%19% , explained in part by the fractionation scheme . 
doses of 4550 gy can be given , with acceptable bowel and hepatic complications ; however , a dose of 50 gy is suggested as being the tolerance limit for the upper abdominal gastrointestinal tract [ 13 ]  . 
a recent study [ 15 ] has shown that 5year disease - free survival ( dfs ) is 66% in the radiotherapy introduzione la chirurgia la principale opzione terapeutica nella cura del tumore dellapparato urinario clinicamente localizzato . ad ogno modo , sebbene questappoccio sia associato ad un eccellente controllo locale , non scevro dal rischio di complicanze e , a volte , di una scarsa qualit di vita . 
nel trattamento del cancro invasivo della vescica come alternativa alla cistectomia radicale immediata si pu utilizzare la resezione la resezione transuretrale , la chemioterapia e la radioterapia con cistectomia di salvataggio . 
la maggior parte dei pazienti trattati con terapia trimodale conserva una buona funzione vescicale . rene la nefrectomia radicale resta la sola terapia efficace per il carcinoma renale ( cr ) clinicamente localizzato . 
la rt pre - operatoria con dosi da 20 a 40 gy stata utilizzata per facilitare la resezione , per sterilizzare i margini periferici ben ossigenati del tumore che potrebbero essere sezionati durante la nefrectomia , e per ridurre la possibilit di disseminazione al momento della nefrectomia . 
nessun vantaggio stato dimostrato nei pazienti sottoposti a rt pre - operatoria con dosi da 20 a 40 gy per ci che riguarda la sopravvivenza globale ( sg ) o sopravvivenza libera da metastasi a distanza ( slmd ) , sebbene sia stato notato un miglioramento della resecabilit [ 16 ]  . 
in studi datati , la radioterapia postoperatoria ha dimostrato un vantaggio di circa il 15% sul controllo locale ( cl ) rispetto alla nefrectomia da sola [ 711 ] , ma con risultati insoddisfacenti sulla sopravvivenza . 
due studi [ 10 , 12 ] hanno riportato eccessive complicanze intestinali ed epatiche , ed una percentuale del 13%19% di mortalit legata alla rt , spiegata in parte dallo schema di frazionamento . 
dosi di 4550 gy possono essere erogate con complicanze intestinali ed epatiche accettabili ; comunque suggerita una dose di 50 gy come limite di tolleranza per il tratto gastrointestinale superiore [ 13 ]  . 
 [ 11 ] lirradiazione post nefrectomia con dose mediana di 46 gy ha ridotto la percentuale di recidive locali nei pazienti con tumore in stadio pt3 dal 37% ( nei pazienti non irradiati ) al 10 % ( nei pazienti irradiati ) ( p = 0 , 05 ) ; ma , in un aggiornamento del radiol med ( 2009 ) 114 : 7082 group and 16% in the no - treatment group and has shown reduction of local recurrence , with a significant difference in both univariate and multivariate analyses , although no benefit was noted in patients with earlier - stage disease . another recent study [ 16 ] concluded that adjuvant rt is unlikely to improve treatment outcome . 
however , these series suggest a benefit in patients with a high risk of local recurrence ( incomplete resection t3 / t4 stage , nodal metastases ) , but there is no advantage for os . 
the authors achieved an overall partial / complete response ( cr ) of 90%98% . this new radiation technique is a big challenge , because the side effects are few , and local control is high due to easy dose escalation . 
complete resection is the only known cure for renal cancer , and the value of rt is controversial . results are awaited of multi - institutional prospective randomised trials using modern rt techniques to evaluate the role of rt and its effect on survival , especially in selected patients with a high risk of local or regional failure . ureter and urethra carcinomas of the ureter and urethra are unusual diseases with insufficient clinical experience , and the role of rt in situ not well defined . 
 [ 20 ] reviewed the records of 31 patients with locally advanced transitional cell carcinoma of the renal pelvis and ureter who underwent surgery followed by adjuvant rt with or without concurrent chemotherapy ( ct ) [ methotrexate , cisplatin ( cddp ) and vinblastine ( mcv ) ]  . five - year os and disease - specific survival ( dss ) with adjuvant concurrent chemoradiotherapy ( ccrt ) ( cddp ) improved in patients with resected , locally advanced uppertract urothelial malignancies . 
 the results of 34 women with primary urethral carcinoma were retrospectively reviewed at princess margaret hospital [ 23 ] .these patients were treated with rt with or lavoro , la rt post - operatoria non ha migliorato la sopravvivenza ed ha mostrato tossicit [ 14 ]  . 
un recente studio [ 15 ] ha mostrato che la sopravvivenza libera da malattia ( slm ) a 5 anni del 66% nel gruppo sottoposto a rt e del 16% nel gruppo non sottoposto a rt ed ha mostrato una riduzione della recidiva locale , con una differenza significativa sia allanalisi univariata che multivariata ; ma non stato notato nessun beneficio nei pazienti in stadio iniziale di malattia . 
comunque , tali lavori hanno suggerito un beneficio nei pazienti ad alto rischio di recidiva ( resezione incompleta negli stadi t3 / t4 , metastasi linfonodali ) , ma nessun vantaggio riguardo alla sg . 
 [ 18 ] riguardo lutilizzo della rt stereotassica extracranica nei tumori renali primitivi e metastatici : gli autori hanno riportato il 90%98% di risposte parziali / complete ; questa nuova tecnica di irradiazione una grande sfida perch gli effetti collaterali sono pochi ed il cl alto , dovuto alla facilit di aumentare la dose erogata . 
attendiamo i risultati di studi prospettici randomizzati multi - istituzionali che utilizzano tecniche moderne di rt per valutare il ruolo ed i suoi effetti sulla sopravvivenza , specialmente in pazienti selezionati con alto rischio di recidiva locale o regionale . 
la sg e la ssm a 5 anni con chemio - rt concomitante e adiuvante ( ccrt ) sono migliorate nei pazienti con neoplasie resecate e localmente avanzate del tratto urinario inferiore . 
i pazienti con malattia avanzata trattati con chirurgia da sola hanno avuto una slm pi breve ( 23 , 3 mesi ) rispetto quelli trattati con combinazione di rt - ct ( 45 , 2 mesi )  . grigsby [ 22 ] ha analizzato i dati di 44 donne con carcinoma delluretra . 
brachytherapy reduced the risk of local recurrence , and the beneficial effect was most prominently seen in patients with bulky primary disease . in the conservative management of these tumours , the combination of external beam brachytherapy with or without ct play a significant role , and the multimodality approach appears to be the optimal way to treat these patients , with surgery to be used for biopsy - proven persistent tumours or recurrence [ 24 ]  . radiotherapy bladder radical cystectomy with bilateral pelvic lymph node dissection followed by urinary diversion remains the gold standard for treating muscle - invading bladder cancer and is the single most successful modality , reporting long - term os in the range of 40%60% [ 2528 ]  . 
rt is utilised as single modality treatment , as neoadjuvant or adjuvant to surgery , or combined with ct with or without conservative local surgery . i risultati di 34 pazienti con carcinoma uretrale sono stati analizzati in modo retrospettivo al princess margaret hospital [ 23 ] , trattati con rtbrachiterapia . 
 nella strategia terapeutica conservativa di questi tumori , la combinazione di rt e brachiterapia con o senza ct , riveste un ruolo significativo e , lapproccio multimodale sembra essere il modo ottimale per trattare questi pazienti , riservando la chirurgia per laccertamento istologico della persistenza o recidiva tumorale [ 24 ]  . vescica la cistectomia radicale con linfadenectomia pelvica bilaterale seguita da diversione urinaria rimane il gold standard per il trattamento del carcinoma della vescica invasivo ed la singola modalit pi vantaggiosa che ha riportato una sg a lungo termine del 40%60% [ 2528 ]  . 
such comparisons were very difficult , because patients selected for radical cystectomy had less advanced tumours at diagnosis , were younger and in a better general condition than patients selected for definitive irradiation . 
results reported in the literature are not significant : the 5 - year survival rate for patients treated with rt alone ( dose of 6066 gy at a 1.8to 2 - gy daily fraction ) is 32% ( range 22%50% ) [ 29 , 30 ]  . 
a recent review of treatment outcomes in rt - treated patients showed the following 5 - year survival rates : t1 , 35%71% ; t2 , 10%59% ; t3 , 10%38% ; and t4 , 0%16% [ 31 ]  . 
tali confronti sono molto difficoltosi perch i pazienti selezionati per la cistectomia radicale avevano tumori in stadio meno avanzato alla diagnosi , erano pi giovani ed in migliori condizioni generali rispetto ai pazienti selezionati per la rt radicale . 
in letteratura i risultati non sono significativi : la sopravvivenza a 5 anni per i pazienti trattati con rt da sola ( dosi di 6066 gy , con 1 , 82 gy come frazione giornaliera ) del 32% ( 22%50% ) [ 29 , 30 ]  . 
una review recente riguardo i risultati della terapia nei pazienti sottoposti a rt , ha mostrato la seguente incidenza di sg a 5 anni : t1 , da 35% a 71% ; t2 , da 10% a 59% ; t3 , da 10% a 38% e t4 da 0% a 16% [ 31 ]  . radioterapia pre - operatoria la pi ampia esperienza ( 338 pazienti ) con rt pre - operatoria ha ottenuto una sotto - stadiazione patologica nel 65% dei pazienti ed una risposta patologica completa nel 42% dei casi . 
la sopravvivenza a 5 anni dei pazienti che hanno ricevuto la rt seguita da cistectomia stata 38% vs radiol med ( 2009 ) 114 : 7082 followed by cystectomy was 38% vs 29% for those treated with rt alone ( not statistically significant )  . 
 strong support for the use of preoperative irradiation in patients with t3b bladder cancer was reported by cole et al . [ 34 ] : the 5 - year local control in the preoperative group was 91% compared with 72% for those treated with radical cystectomy alone . 
however , a meta - analysis of five randomised trials showed no statistical difference in treatment outcomes between patients treated with preoperative rt and cystectomy alone [ 35 ]  . 
 preoperative ccrt showed better results than rt alone . in fact , in the nordic cystectomy trial [ 37 ] , the combination of ct ( adriamycin + cddp for two cycles ) plus rt ( 20 gy in four fractions ) followed by cystectomy showed a 5 - year os improvement of 15% only for t3 - t4 disease compared with rt or surgery alone ( p = 0.03 ) , whereas no survival benefit was found for early stages of disease ( t1t2 )  . 
in the canadian randomised study [ 38 ] , concurrent cisplatin improved pelvic disease control with preoperative 29% per quelli trattati con rt da sola ( non statisticamente significativo , nss )  . 
 [ 34 ] : il cl a 5 anni nel gruppo sottoposto a rt preoperatoria stato del 91% rispetto al 72% per quelli trattati con cistectomia radicale e c stato anche un beneficio in termini di sg e slm ( nss )  . 
comunque , una metanalisi di 5 studi randomizzati non ha mostrato differenze statisticamente significative tra i pazienti trattati con rt pre - operatoria e quelli trattati con cistectomia radicale [ 35 ]  . 
una conclusione simile stata raggiunta in uno studio di fase iii su 140 pazienti , che confronta la chirurgia da sola con chirurgia e rt preoperatoria [ 36 ]  . la ccrt pre - operatoria ha mostrato migliori risultati rispetto alla rt da sola . 
infatti , nello studio nordico sulla cistectomia [ 37 ] la combinazione di ct ( adriamicina + cisplatino per 2 cicli ) pi rt ( 20 gy in 4 frazioni ) seguita da cistectomia ha mostrato un incremento della sg a 5 anni del 15% solo per i t3 - t4 rispetto alla rt o chirurgia da sola ( p = 0 , 03 ) , mentre nessun beneficio di sopravvivenza stato trovato negli stadi iniziali di malattia ( t1t2 )  . 
only one randomised study of radical cystectomy alone vs cystectomy and postoperative rt [ 41 ] reported a 5 - year pelvic recurrence of 5% ( 50% in the cystectomy arm ) and an improvement in dfs in patients with schistosomiasis . 
the main disadvantage of postoperative rt is the high rate ( 20%40% ) of serious late gastrointestinal complications [ 39 , 40 , 4244 ] because of the larger volume of small bowel occupying the pelvis after cystectomy . 
patients at high risk of recurrence are probably better treated with ct , which may prevent local and distant relapse and is usually well tolerated . bladder - preservation therapy the relative negative impact on quality of life for urinary diversion and the trend towards organ preservation led many authors to explore the role of conservative management . 
neoadjuvant ct compared with rt or surgery was investigated in an attempt to improve the results of surgery alone or definitive rt maintaining a functioning bladder . in the european organisation for research and treatment of cancer ( eortc ) / medical research council [ 45 ] trial , 976 patients undergoing curative cystectomy or radical rt were randomised to receive three cycles of neoadjuvant ct ( mcv ) in 491 patients or no ct in 485 . 
a recent meta - analysis [ 46 ] confirmed that neoadjuvant platinum - based combination ct reduces mortality risk of 13% , with moderate improvement ( 5% , p = 0.016 ) of 5 - year os , irrespective of the type of local treatment ( surgery or rt alone or rt and cystectomy ) and without differences between subgroups of patients . 
there was no evidence to support the use of single - agent platinum . these studies showed that patients treated with rt ( conservative approach ) have preserved bladder function . over the past 1520 years , several prospective trials have investigated conservative therapy in which all patients were treated with transurethral resection of bladder tumours ( turbt ) with or without ct followed by ccrt . 
alcuni studi hanno riportato una riduzione del rischio di recidive pelviche dal 30% al 50% al 10% al 20% [ 3941 ] , ma alcuni pazienti hanno anche ricevuto rt pre - operatoria . 
solo uno studio randomizzato sulla cistectomia radicale da sola verso cistectomia e rt postoperatoria [ 41 ] , ha riportato recidive pelviche a 5 anni del 5% ( 50% nel braccio della cistectomia ) ed un incremento della slm nei pazienti con schistosomiasi . 
il principale svantaggio della rt post - operatoria lalta percentuale ( 20%40% ) di gravi complicanze gastrointestinali tardive [ 39 , 40 , 4244 ] , poich una gran parte di volume dellintestino tenue occupa la pelvi dopo cistectomia . 
i pazienti ad alto rischio di recidiva sono probabilmente trattati in modo migliore con la ct , che pu prevenire recidive locali e a distanza ed di solito ben tollerata . 
 terapia di preservazione della vescica il relativo impatto negativo sulla qualit della vita per la diversione urinaria e la tendenza verso la preservazione dellorgano , ha permesso a molti autori di esplorare il ruolo di un trattamento conservativo . 
 nello studio delleortc ( european organisation for research and treatment of cancer ) / medical research council [ 45 ] , 976 pazienti sottoposti a cistectomia curativa o rt radicale sono stati randomizzati a ricevere 3 cicli di ct neoadiuvante ( mcv , metotressato , cddp , vinblastina ) in 491 pazienti , oppure nessuna ct in 485 pazienti . 
la differenza assoluta tra i gruppi per quanto riguarda la sg a 3 anni del 5 , 5% ( 55 , 5% per ct vs 50% nessuna ct ) non risultata statisticamente significativa ( p = 0 , 075 ) : la ct neoadiuvante stata associata con una patologica completa pi alta , ma non c stato nessuna chiara evidenza sulla sopravvivenza . 
una recente metanalisi [ 46 ] ha confermato che la combinazione di ct neoadiuvante a base di platino riduce il rischio di mortalit del 13% , con un incremento moderato ( 5% , p = 0 , 016 ) della sg a 5 anni , indipendentemente dal tipo di trattamento locale ( chirurgia o rt da sola o rt e cistectomia ) , e senza differenze tra i sottogruppi di pazienti , non vi stata alcuna evidenza a favore di platino da solo . 
 negli ultimi 1520 anni , diversi studi prospettici hanno analizzato terapie conservative in tutti quei pazienti trattati radiol med ( 2009 ) 114 : 7082 patients with cr , a consolidation rt or ccrt regimen was administered . 
 since 1985 , radiation therapy oncology group ( rtog ) trials have used a trimodality conservative treatment ( turbt , rt , ct ) in patients with t2t4a muscleinvasive bladder cancer who were candidates for cystectomy . 
in three rtog trials [ 4749 ] , patients were treated with neoadjuvant turbt and ccrt ( conventional or altered fractionation ) , whereas in two trials [ 50 , 51 ] , patients were treated with induction by turbt with or without ct and ccrt . 
cystectomy was reserved for incompletely responders or relapse . in the rtog 89 - 03 phase iii study , the combination of neoadjuvant ct ( mcv2 cycles ) with ccrt with cddp failed to show significant benefits in terms of 5 - year local control ( 61% vs 49% ) , os ( 48% vs 49% ) and ffdm ( 33% vs 39% ) compared with ccrt alone , with more toxicity in the mcv arm [ 51 ]  . 
in fact , subsequent studies by the rtog emphasised the impact of adjuvant ct [ mcv or cddp + 5fluorouracil ( fu ) ] following rt ( hypoor hyperfractionated ) [ 49 ] , with good results at 3 years . 
from paris began a prospective trial of preoperative ct using 5 - fu and cddp with concomitant rt ( 3 gy b.i.d. , total dose 24 gy ) , followed by either cystectomy or additional ccrt . 
this treatment strategy resulted in a pathological cr of 77% and may be proposed as conservative treatment in patients with a cr to the initial course of chemoradiation [ 54 ]  . 
globally , os at 5 years was 51% . similar results were obtained in further series of combined modality treatment for bladder preservation with excellent cr ( ~70% ) , and 5 - year os ( ~50% ) , with bladder con resezione transuretrale della vescica ( turbt ) ct seguita da ccrt , e per i pazienti con risposta completa stata somministrata una rt di consolidamento o ccrt ; la cistectomia stata riservata per le risposte incomplete o per le recidive di malattia . 
 dal 1985 , gli studi dellrtog ( radiation therapy oncology group ) hanno utilizzato un trattamento conservativo trimodale ( turbt , rt , ct ) nei pazienti con carcinoma della vescica t2t4a , che erano candidati alla cistectomia . in tre studi dellrtog [ 4749 ] i pazienti sono stati trattati con turbt neoadiuvante e ccrt ( convenzionale o frazionamenti alterati ) ; mentre in 2 studi [ 50 , 51 ] i pazienti sono stati trattati con induzione mediante turbtct e ccrt ; la cistectomia stata riservata per le risposte incomplete o in caso di recidive . 
 nello studio di fase iii dellrtog 89 - 03 , la combinazione di ct neoadiuvante ( mcv2 cicli ) con ccrt mediante cddp non ha mostrato alcun beneficio significativo in termini di cl a 5 anni ( 61% vs 49% ) , sg ( 48% vs 49% ) e slm ( 33% vs 39% ) , rispetto alla ccrt da sola , con una maggiore tossicit nel braccio che ha usato lmcv [ 51 ]  . 
infatti gli studi successivi dellrtog hanno puntualizzato limpatto della ct adiuvante ( mcv o cddp + 5 - fu ) alla rt ( ipoo iper - frazionamenti ) [ 49 ] , con buoni risultati a 3 anni . 
 [ 54 ] di parigi , hanno iniziato uno studio prospettico di ct preoperatoria usando 5 - fu e cddp con rt concomitante ( 3 gy bid , dose totale di 24 gy ) , seguita sia da cistectomia o ccrt addizionale . 
questa strategia di trattamento ha determinato una risposta patologica completa nel 77% dei casi , e pu essere proposta come terapia conservativa nei pazienti con risposta completa al ciclo iniziale di ccrt [ 54 ]  . 
 [ 55 ] , nella quale 415 pazienti sono stati trattati dopo la turbt con rt da sola ( 126 pazienti ) o in concomitanza con cddp ( 240 pazienti ) o cddp + 5 - fu ( 49 pazienti ) , con percentuali di risposte complete migliori per rt + cddp - 5 - fu ( 87% ) rispetto al cddp ( 66% ) o rt da sola ( 61% ) ; globalmente , la sg a 5 anni risultata pare a 51% . risultati simili sono stati ottenuti in ulteriori studi con modalit di trattamento combinato per la conservazione della vescica , con eccellenti risposte complete ( ~70% ) , ed una sg a 5 anni ( ~50% ) , con conservazione dellorgano in radiol med ( 2009 ) 114 : 7082 table 1 series of combined modality treatment for bladder preservation series no . 
 [ 70 ] turbt 24 gy at 3 gy + cddp / fu 2 additional cycles of crt ( dose not given ) ( specific cancer ) ng ( overall rate of cystectomy : 25.6% ) danesi et al . 
table 1 summarises the results of these studies [ 5674 ]  . in a recent meta - analysis of fifteen radiation series with different fractionation schedules and total doses , pos et al . [ 75 ] found evidence for an overall doseresponse relationship with an increase in local control by a factor of 1.441.47 for an increment in dose of 10 gy . 
 [ 71 ] recently reported the long - term results of a phase i / ii trial of ct ( mcv ) followed by concomitant cddp + 5 - fu and hyperfractionated irradiation ( three 100cgy fractions / day , for a total dose of 69 gy )  . 
accelerated rt may overcome radioresistance due to tumour - cell repopulation , but a recent randomised trial [ 77 ] reported no improvement of local control or survival rates and increased acute bowel complications . 
there has been only one small phase iii study of curative rt in which survival was inferior in the hypofractionated arm [ 78 ]  . some trials , in an attempt to improve results , explore the use of new chemotherapeutic agents and accelerated or hyperfractionated rt to increase irradiation dose in combination with ct . 
new chemotherapeutic agents , in particular gemcitabine and taxanes , are effective in combination with cddp and rt ( paclitaxel and gemcitabine are good radiosensitisers ) [ 61 , 79 ]  . 
a recent italian study [ 68 ] reported the feasibility of a combined scheme with gemcitabine ( up to 400 mg / m2 ) plus cddp and rt , obtaining 100% cr . 
finally , the rtog 99 - 06 trial introduced concomitant paclitaxel + cddp plus bifractionated rt as induction treatment , followed by adjuvant ct ( gemcitabine and cddp ) in patients with cr ; no specific outcomes are yet available [ 80 ]  . 
in una meta - analisi recente su 15 studi di rt con differenti schemi di frazionamento e dose totale , pos et al . [ 75 ] , hanno evidenziato una relazione globale dose - risposta , con incremento del cl , di un fattore che va da 1 , 44 a 1 , 47 per un aumento di dose di 10 gy . 
una meta - analisi di stuschke e thames [ 76 ] ha indicato che i regimi iper - frazionati mostrano un aumento della sg ( odd ratio di mortalit 0 , 55 ; p = 0 , 002 ) ed una risposta completa ( odd ratio di fallimento di 0 , 44 ; p = 0 , 001 )  . 
 [ 71 ] , recentemente hanno riportato risultati a lungo termine di uno studio di fase ii / ii di ct ( mcv ) seguita da ct a base di cddp + 5 - fu concomitante e rt iper - frazionata ( 1 gy per 3 frazioni al giorno , per una dose totale di 69 gy )  . 
le percentuali a 5 anni di sg , conservazione della vescica , ssm , slm e sopravvivenza senza cistectomia per tutti e 77 i pazienti sono state 58 , 8% , 46 , 6% , 75% , 53 , 5% e 76 , 1% , rispettivamente . 
la rt accelerata pu superare la radioresistenza generata dal ripopolamento delle cellule tumorali , ma in uno studio recente randomizzato [ 77 ] , non riportato alcun incremento delle percentuali del lc o della sg ma sono aumentate le complicanze intestinali acute . 
 alcuni studi , nel tentativo di migliorare i risultati , hanno esplorato luso di nuovi agenti chemioterapici e rt accelerata o iper - frazionata per aumentare la dose di rt in associazione con la ct . 
nuovi agenti chemioterapici , in particolare gemcitabina e taxani , sono efficaci in combinazione con cddp e rt ( paclitaxel e gemcitabina sono buoni radiosensibilizzanti ) [ 61 , 79 ]  . 
un recente studio italiano [ 68 ] , ha riportato la fattibilit di uno schema combinato con gemcitabina ( fino 400 mg / m2 ) pi cddp e rt , ottenendo il 100% di risposta completa . 
infine , lrtog 99 - 06 ha introdotto ct concomitante a base di paclitaxel + cddp pi rt bifrazionata come trattamento di induzione , seguito da ct adiuvante ( gemcitabina e cddp ) nei pazienti con risposta completa ; risultati specifici non sono ancora disponibili [ 80 ]  . conclusions conclusioni radical nephrectomy is the only effective therapy for clinically localised renal cancer . 
la cistectomia di salvataggio usata in caso di risposta parziale dopo terapia di induzione ccrt ( rtog ) o recidiva radiol med ( 2009 ) 114 : 7082 response after induction ccrt treatment ( rtog ) or recurrent disease ( european trials ) : in both cases , surgery can be curative , reporting a 5 - year survival of approximately 50% [ 45 , 50 , 51 , 54 , 55 ]  . 
 trimodality treatment ( turbt , rt , ct ) of invasive bladder cancer may be offered as a valid alternative to radical cystectomy , with no decrease in survival related to the delay in cystectomy , which is currently the gold standard therapy . 
os is comparable with recent surgical data , reporting a 5 - year os of almost 50% , with bladder preservation in three fourths of these patients . di malattia ( studi europei ) : in entrambi i casi la chirurgia pu essere curativa , riportando una sopravvivenza a 5 anni del 50% approssimativamente [ 45 , 50 , 51 , 54 , 55 ]  . 
 il trattamento trimodale ( turbt , rt , ct ) del carcinoma invasivo della vescica pu offrire una valida alternativa alla cistectomia radicale con nessuna diminuzione della sopravvivenza correlata al ritardo della cistectomia , che rimane attualmente la terapia gold standard . 
san giovanni battista , c.so bramante 88 , 10126 turin , italy 3radiology service , ospedale santa croce e carle , via coppino 26 , 12100 cuneo , italy correspondence to : c . 
le indicazioni alla procedura erano : sanguinamento digestivo ( 52 , 8% ) , ascite refrattaria ( 35 , 3% ) , tutela della perviet portale pre - trapianto epatico ( 3 , 0% ) , trombosi delle vene sovraepatiche ( 2 , 3% )  . 
durante un follow - up di 1500 giorni , lincidenza cumulativa di reintervento sugli stent stata del 25 , 7% ( nitinol ) , 32 , 9% ( wallstent ) e 1 , 8% ( palmaz ) ; la mortalit stata rispettivamente 31 , 1% , 38 , 5% e 56 , 4% . 
tips placement is safe and effective and may act as a bridge to liver transplantation . ultrasonography plays a fundamental role in the preliminary assessment , in portal vein puncture and during the follow - up . 
 parole chiave tips radiologia interventistica insufficienza epatica ipertensione portale keywords tips interventional radiology liver failure portal hypertension introduction introduzione transjugular intrahepatic portosystemic shunt ( tips ) insertion was introduced into clinical practice more than 20 years ago for the treatment of portal hypertension and its complications . 
a number of controlled trials have compared the efficacy of tips versus medical and endoscopic treatment in preventing variceal bleeding and treating refractory ascites , to date the universally accepted indications for tips [ 17 ]  . 
these include portal thrombosis , budd - chiari syndrome , pleural ascites [ 810 ] , hepatopulmonary syndrome ( hps ) [ 11 ] , hepatorenal syndrome ( hrs ) [ 3 , 1217 ] , prophylaxis of intraoperative bleeding in cirrhotic patients with portal hypertension who are candidates for major abdominal surgery [ 8 , 18 , 19 ] and maintenance of portal vein patency prior to orthotopic liver transplantation ( olt ) [ 20 , 21 ]  . we retrospectively reviewed a large series of patients who underwent tips over a 15 - year period at a referral centre and compared the data with the literature with the aim of providing useful radiological and clinical information for multidisciplinary management of cirrhotic patients with complicated portal hypertension . da oltre 20 anni lo shunt intraepatico porto - sistemico ( tips ) stato introdotto nella pratica clinica per il trattamento dellipertensione portale e delle sue complicanze . numerosi trials controllati hanno comparato lefficacia della tips con la terapia medica ed endoscopica nella profilassi del sanguinamento da varici e nel trattamento dellascite refrattaria , che rimangono le principali indicazioni , univocamente condivise [ 17 ] ; le linee guida alla procedura sono state tracciate sulla base di aspetti tecnici angiografici , fattori prognostici clinico - laboratoristici ed incidenza di complicanze . 
indicazioni pi rare ed oggetto di studi non controllati condotti su piccoli gruppi di pazienti , alcune delle quali non uniformemente accettate sono : la trombosi portale , la sindrome di budd - chiari , lascite pleurica [ 810 ] , la sindrome epato - polmonare ( hps ) [ 11 ] , la sindrome epato - renale ( hrs ) [ 3 , 1217 ] , la profilassi del sanguinamento intraoperatorio in pazienti cirrotici con ipertensione portale candidati ad interventi di chirurgia addominale maggiore [ 8 , 18 , 19 ] e la tutela della perviet portale pre - trapianto epatico ( olt ) [ 20 , 21 ]  . scopo di questo lavoro analizzare retrospettivamente , confrontandoli con una revisione della letteratura , i dati di unampia casistica di pazienti sottoposti a tips nellarco di quindici anni presso un centro di riferimento al fine di fornire informazioni tecniche radiologiche e cliniche utili nella gestione multidisciplinare del paziente cirrotico con ipertensione portale complicata . 
 materials and methods between march 1992 and december 2006 , 658 patients ( 432 males and 226 females , age range 485 years , mean age 56.2 years ) with cirrhosis and portal hypertension of varying aetiology ( table 1 ) were referred to our centre for tips placement . 
fourteen patients had previously undergone liver transplantation and were being treated for materiali e metodi dal marzo 1992 al dicembre 2006 sono giunti al nostro istituto per essere sottoposti a tips 658 pazienti , 432 maschi e 226 femmine , det compresa tra 4 e 85 anni , con et media di 56 , 2 anni . 
le indicazioni alla tips sono riassunte in tabella 2 . radiol med ( 2009 ) 114 : 8394 table 1 aetiology of cirrhosis infectious , viral ( hcv , hbv ) alcoholic cryptogenic budd - chiari syndrome biliary cirrhosis number hcv , hepatitis c virus ; hbv , hepatitis b virus tabella 1 eziologia della cirrosi infettiva virale ( hcv , hbv ) alcolica criptogenica sindrome di budd - chiari cirrosi biliare hcv , virus dellepatite c ; hbv , virus dellepatite b refractory ascites ( n = 6 ) , pleural ascites ( n = 4 ) , bleeding ( n = 2 ) and recurrent budd - chiari syndrome ( n = 2 )  . all patients referred electively to our centre had already undergone clinical assessment with echocardiography and portal ultrasonography ( us )  . 
tips procedures were performed in the angiography suite with the following x - ray systems : angio diagnost 3 dvi , multi diagnost 3 and allura xper fd20 ( all philips medical systems , best , the netherlands )  . 
in the case of elective procedures , patients signed the informed consent form and were acute bleeding recurrent bleeding refractory ascites budd - chiari syndrome pleural ascites hepatorenal syndrome hepatopulmonary syndrome pre - olt pre - surgery partial thrombosis of the portal quattordici pazienti erano gi stati sottoposti a trapianto epatico e sono stati trattati per : ascite refrattaria ( 6 casi ) , ascite pleurica ( 4 casi ) , sanguinamento ( 2 casi ) e recidiva di sindrome di budd - chiari ( 2 casi )  . 
per le procedure eseguite in regime di elezione il giorno antecedente lesame il paziente ha firmato un consenso informato ed stato visitato dallanestesista ; sono stati valutati lemocromo e lo screening emocoagulativo completo ed stata intrapresa una profilassi antibiotica ad ampio spettro . 
attraverso un introduttore vascolare posizionato in vena giugulare interna di 10 f di calibro e 35 cm di lunghezza , con lausilio di un catetere angiografico di 4 f e 65 cm di lunghezza ( terumo corporation , tokyo , giappone ) ed una guida idrofila con punta j di 0 , 035 pollici e 180 cm di lunghezza ( terumo corporation , tokyo , giappone ) stata incannulata la vena sovraepatica destra ( 521 pazienti ) o mediana ( 128 pazienti )  . 
all patients underwent complete blood count and coagulation screening tests and received broad - spectrum antibiotics . patients vital signs were monitored continuously throughout the procedure , and an anaesthetistresuscitator was present during all angiographic manoeuvres . 
after placing a 35 - cm - long , 10 - f vascular introducer in the internal jugular vein , the right ( 521 patients ) or middle ( 128 patients ) hepatic vein was cannulated with the aid of a 65cm - long , 4 - f angiographic catheter ( terumo corporation , tokyo , japan ) and a 180 - cm - long , 0.035 - j - tip hydrophilic guidewire ( terumo corporation , tokyo , japan )  . 
us , performed with a 3.5 - mhz convex - array probe and intercostal scans enabled us to withdraw the needle tip in the hepatic vein until a portal branch of adequate size and with favourable anatomical relationships could be identified , and subsequently to guide advancement of the obturator in real time . 
in 520 cases , the portal system was accessed via the right portal vein , in 85 cases via the left portal vein and in 46 cases via the bifurcation . after removing the needle obturator under us and fluoroscopic guidance , the hydrophilic guidewire was advanced to the portal trunk and a 110 - cm - long , 4 - f pigtail catheter was introduced into the guidewire . 
portal ( with the catheter tip in the trunk ) and systemic ( from the side of the vascular introducer sheath with the catheter tip in the hepatic vein ) pressure measurements were then obtained , and subsequently portography was performed after injecting 25 ml of contrast material ( ultravist 370 , shering ag , berlin , germany ) into the splenic vein at a flow rate of 8 ml / s with an automatic injector . 
the parenchymal tract was then dilated until complete distension by using an 8 - mm angioplasty balloon catheter of varying length ( 48 cm ) ( wanda , boston scientific , natick , ma , usa ; smash , boston scientific ; xxl , boston scientific )  . 
subsequently , the palmaz ( mechanically expandable ) , memotherm and luminexx ( nitinol ) , wallstent and wallgraft ( self - expandable ) stents ( table 3 ) were deployed and dilated to approximately 10 mm , except in patients scheduled for olt . 
lecografia , effettuata con sonda convex di 3 , 5 mhz in scansioni intercostali , ha permesso di arretrare in vena sovraepatica la punta dellago sino a visualizzare un ramo portale di calibro adeguato e con rapporti anatomici favorevoli , e successivamente di guidare in tempo reale lavanzamento del mandrino . 
si effettuata la manometria portale ( con apice del catetere posto a livello del tronco ) e sistemica ( dalla via laterale dellintroduttore vascolare con apice in vena sovraepatica ) ; la successiva portografia stata ottenuta infondendo in vena splenica , con lausilio di iniettore automatico , 25 ml di mdc ( ultravist 370 , shering ag , berlin , germania ) , con un flusso di 8 ml / s . 
utilizzando un catetere a palloncino da angioplastica ( wanda , boston scientific corporation , natick , ma , usa ; smash , boston scientific corporation , natick , ma , usa ; xxl boston scientific corporation , natick , ma , usa ) da 8 mm e lunghezza variabile ( 48 cm ) si proceduto quindi alla dilatazione del tramite parenchimale fino alla sua completa distensione . 
sia la puntura portale che la dilatazione del tragitto sono state eseguite con adeguata sedazione ( remifentanyl 0 , 05 - 0 , 1 kg / min e propofol 1 mg / kg / ora )  . 
successivamente si proceduto al rilascio ed alla dilatazione degli stent palmaz ( espandibili meccanicamente ) , memotherm e luminexx ( nitinol stent ) , wallstent e wallgraft ( autoespandibili ) ( tabella 3 )  . 
le trombosi portali sono state trattate con angioplastiche ripetute , utilizzando palloni di diametro variabile tra 8 mm e 14 mm ; tentativi di fibrinolisi con urochinasi ( 200000 ui a bolo seguite da 1 milione di ui nelle successive 24 ore ) sono stati inefficaci . 
 si sono eseguiti infine un controllo flebografico , con i flussi gi descritti , ed una rilevazione delle nuove pressioni portale e sistemica : lopacizzazione esclusiva dei rami portali intraepatici principali e la devascolarizzazione delle varici in corso di portografia insieme ad un gradiente porto - sistemico minore od uguale a 10 mmhg sono stati considerati deponenti per il buon successo emodinamico della procedura . in 45 pazienti ( 6 , 8% ) , di cui 15 sottoposti a tips in regime durgenza , si deciso di eseguire lembolizzazione selettiva di varici gastro - esofagee persistenti con spirali radiol med ( 2009 ) 114 : 8394 repeated angioplasty procedures using 8to 14 - mm balloons . 
attempts at fibrinolysis with urokinase ( 200 , 000 iu as a bolus followed by 1 million iu over 24 h ) were ineffective . finally , postprocedural phlebography was performed with the flow rates described above , and the new portal and systemic pressures were measured : exclusive opacification of the main intrahepatic portal branches and variceal devascularisation at portography along with a portosystemic gradient 10 mmhg were considered evidence of haemodynamic success . in 45 patients ( 6.8% ) , 15 of whom were emergency referrals , we decided to perform selective embolisation of persistent gastro - oesophageal varices with metal coils ( balt , montmorency , france ; cook europe ) measuring 10 mm and 16 mm in diameter . metalliche ( balt , montmorency , francia ; cook , bjaeverskov , danimarca ) di 10 mm e 16 mm di diametro . stato considerato successo tecnico il corretto posizionamento e la regolare perviet dello stent , con rapida opacizzazione dellatrio destro in corso di flebografia . 
in 7 pazienti non si potuto portare a termine la tips per occlusione inveterata delle vene sovraepatiche , per progressione intraepatica della trombosi portale o per rapporti anatomici sfavorevoli tra i rami portali e le vene sovraepatiche . 
in 1 caso di precoce occlusione della tips pluri - recidivata si ottenuta la perviet dello shunt posizionando coassialmente agli stent gi in sede un ulteriore protesi ricoperta ( wallgraft , boston scientific corporation , natick , ma , usa ) di 12 mm di calibro . 
in seven patients , tips placement could not be completed owing to chronic occlusion of the hepatic veins due to intrahepatic progression of portal thrombosis or because of unfavourable anatomical relationships between the portal and hepatic veins . within 48 h of the angiographic procedure , abdominal us was carried out to exclude any possible complications . in one case of recurrent early occlusion of tips , stent patency was achieved by inserting an additional 12 - mmcalibre covered stent coaxially to the previously deployed stents ( wallgraft , boston scientific )  . patients subsequently underwent us every 6 months , or more frequently if clinically indicated . 
in patients treated for hepatic vein thrombosis or hepatopulmonary syndrome , the stent had to be revised within the first year after insertion in 40% and 66.7% of cases , respectively . 
1 si evince inoltre come la mortalit sia stata elevata e precoce ( 56 , 4% , 43 , 9%68 , 7% con ci del 95% ) per i pazienti trattati con stent di palmaz , mentre inferiore , distribuita nel tempo e similare per le tips eseguite con protesi termoespandibili ( 31 , 1% , 24 , 2%37 , 8% con ci del 95% ) ed autoespandibili ( 38 , 5% , 20 , 8%56% con ci del 95% )  . 
 il successo clinico , considerando che 51 pazienti sono andati allolt dopo un periodo medio dalla tips di 6 mesi , stato ottenuto nel 100% dei pazienti con trombosi portale ( regressione dellascite e detensione delle varici ) o candidati alla gastrectomia ( assenza di cospicua emorragia intraoperatoria ) , nel 91% dei sanguinamenti ( stabilit emodinamica ) considerando che 19 / 76 ( 25% ) dei pazienti trattati in urgenza sono deceduti entro 30 giorni dalla tips , nel 60% delle asciti refrattarie ( ascite minima o assente , blanda terapia diuretica ed assenza di paracentesi ) , nel 70% dei pazienti con hrs ( sospensione emodialisi e miglioramento della creatininemia ) , nel 65% delle asciti pleuriche ( incremento dei volumi polmonari e migliore ventilazione ) , nel 47% delle s . 
1 analisi statistica della perviet degli stent e della mortalit dei pazienti . achieved in 100% of patients with portal thrombosis ( ascites regression and variceal devascularisation ) or candidates for gastrectomy ( no substantial intraoperative haemorrhage ) ; 91% of cases of bleeding ( haemodynamic stability ) , considering that 19 / 76 ( 25% ) emergency referrals died within 30 days of tips , 60% of patients with refractory ascites ( minimal or absent ascites , mild diuretic therapy and no paracentesis ) , 70% of patients with hrs ( discontinuation of haemodialysis and improved serum creatinine ) , 65% of cases of pleural ascites ( increased respiratory volumes and improved ventilation ) , 47% of cases of budd - chiari syndrome ( regression of ascites with significant reduction of liver volume ) and 20% of patients with hps ( significant increase in oxygen saturation )  . none of the procedure - related complications proved fatal or required surgical repair . 
si sono verificati : 6 insufficienze cardiache da sovraccarico destro , 6 emobilie , 3 migrazioni accidentali in arteria polmonare di stent palmaz , 2 ematomi intraepatici , 1 emoperitoneo . 
gli ematomi intraparenchimali , verificatisi in pazienti assai scoagulati forse per puntura accidentale di rami arteriosi , non hanno indotto particolare sintomatologia e / o anemizzazione , sono stati diagnosticati dallecografia addominale precoce post - procedura e si sono risolti spontaneamente . 
lemoperitoneo si verificato nelle ore successive alla tips durgenza per stravaso di una varice gastrica persistente non embolizzata in radiol med ( 2009 ) 114 : 8394 haematoma ( n = 2 ) and haemoperitoneum ( n = 1 )  . 
intraparenchymal haematomas , occurring in heavily anticoagulated patients perhaps due to accidental puncture of arterial branches gave rise to no specific symptoms or anaemia , were diagnosed on early postprocedural abdominal us and resolved spontaneously . 
the six cases of haematobilia were caused by accidental puncture of the gall bladder or highorder bile duct branches and were diagnosed on us within 24 h of the procedure ; 3 / 6 patients received blood transfusion . 
in 43 / 651 patients ( 6.6% ) treated for bleeding or refractory ascites , pse resolved following the tips procedure . discussion clinical aspects in our experience , oesophageal , gastric and intestinal bleeding is the most frequent indication for tips placement . 
a number of studies have shown that tips improves the survival rates of patients with massive and / or recurrent haemorrhage against a rebleeding rate at 2 years of 23%40% [ 24 ] , which is mostly promoted by venous systemic pressure exceeding 15 mmhg , stent malfunction and continuing alcohol consumption [ 25 ]  . 
there is no consensus regarding the treatment of varices during tips placement , which can be achieved by several means : sclerosing agents , acrylic glues , coils and the amplatzer vascular plug [ 26 ]  . 
whereas several authors advocate the systematic occlusion of portosystemic collateral vessels [ 27 ] , others report a 65% rate of rebleeding in patients with correctly embolised varices [ 28 ]  . 
our policy of embolising in patients with previous only persistent varices haematemesis after adequate reduction of the portosystemic gradient ( 10 mmhg ) allowed the rate of rebleeding to be maintained < 10% . 
our data confirm the high rate of presenza di sonda emostatica endoscopica ; la complicanza stata sospettata clinicamente , confermata da una tc e trattata con embolizzazione endovascolare selettiva mediante spirali metalliche . 
i 6 casi di emobilia si sono verificati per puntura accidentale della colecisti o di dotti biliari di maggior ordine e sono stati diagnosticati dallecografia a 24 ore dalla procedura ; 3 / 6 pazienti sono stati emotrasfusi . lencefalopatia porto - sistemica ( pse ) comparsa dopo la tips in 77 / 651 pazienti ( 11 , 8% ) ; lincidenza della complicanza stata particolarmente elevata nei casi di ascite pleurica ( 4 / 12 pazienti , 33 , 3% )  . 
non vi unanime consenso circa il trattamento delle varici in corso di tips , attuabile con differenti presidi : sclerosanti , colle acriliche , spirali ed amplatzer vascular plug [ 26 ] ; alcuni autori sostengono lefficacia dellocclusione sistematica dei collaterali porto - sistemici [ 27 ] , mentre altri lavori riportano un 65% di recidiva di sanguinamento in pazienti con varici correttamente embolizzate [ 28 ]  . 
il nostro atteggiamento di embolizzare , in presenza di adeguata riduzione del gradiente porto - sistemico ( 10 mmhg ) , soltanto le varici persistenti di pazienti con pregressi episodi di ematemesi ha consentito di contenere la recidiva di emorragia al di sotto del 10% . 
i nostri dati confermano lelevata mortalit precoce dei pazienti trattati in urgenza , che giungerebbero comunque allexitus in oltre l80% dei casi di sanguinamento non controllato [ 29 ]  . 
 lascite refrattaria , correlata a prognosi sfavorevole oltre che ad incrementato rischio di infezioni ed insufficienza renale [ 30 ] , rappresenta nella nostra casistica la seconda principale indicazione alla tips . 
il risultato clinico della tips , nella nostra ed altrui esperienza [ 31 ] , non influenzato dalla funzionalit epatica basale del paziente e non sono stati dimostrati fattori prognostici positivi certi . 
 riguardo allimpiego della tips nel trattamento radiol med ( 2009 ) 114 : 8394 early deaths among emergency referrals , 80% of whom , however , would have died in any case due to uncontrolled bleeding [ 29 ]  . refractory ascites , correlated to poor outcome and increased risk of infection and kidney failure [ 30 ] , was the second leading indication for tips in our series . 
the clinical outcome of tips , in our experience and that of other authors [ 31 ] , is unrelated to liver function at baseline , and no certain positive prognostic factors have been identified to date . with regard to the use of tips in the treatment of hepatic hydrothorax , our results were similar in terms of clinical outcome [ 32 , 33 ] and pse incidence with those of other nonrandomised , uncontrolled studies [ 34 ]  . 
because the waiting list for olt is relatively short at our hospital ( 6 months on average ) , it was jointly decided to dilate the stent to 8 mm only in order to reduce the risk of liver failure . 
there is evidence that tips may reduce the mortality and morbidity associated with olt [ 21 ]  . no randomised controlled trials exist that establish a protocol for the treatment of budd - chiari syndrome . 
in patients unresponsive to anticoagulation therapy , tips can reduce portal hypertension , improve liver function and control ascites [ 3 ]  . the only established treatment for hps is liver transplantation , which may , however , be risky or contraindicated in cases of severe hypoxaemia [ 11 ]  . 
the therapeutic efficacy of the intrahepatic shunt is still controversial , with some authors suggesting that the extent of arteriovenous pulmonary fistulas before treatment and the portosystemic gradient after tips are the main determinants of outcome . the unsatisfactory clinical impact observed in out series may be explained by the comorbidities affecting some of our patients ( two cases of emphysema , one of a previous specific process ) , whereas we are unable to account for the high incidence of stent revisions . in our patients who received lactulose to regulate bowel function , the pse induced by tips was mostly transient and mild to moderate and rarely required an angiographic reduction procedure . 
pse regression following tips in patients treated for bleeding or intractable ascites may be explained dellidrotorace epatico il nostro studio si allinea per risultato clinico [ 32 , 33 ] ed incidenza di pse con i dati di altri lavori non randomizzati e non controllati [ 34 ] ; in molti casi lo shunt intraepatico rappresenta una soluzione ponte allolt , senza il quale questi pazienti giungono allexitus per lo pi per complicanze correlabili alla progressione dellinsufficienza epatica [ 35 ]  . 
 nei pazienti in lista olt il confezionamento della tips ha garantito la perviet portale ; in considerazione del fatto che presso il nostro centro i pazienti giungono allolt in tempi brevi ( mediamente 6 mesi ) stato deciso collegialmente di dilatare lo stent a soli 8 mm , per ridurre il rischio di insufficienza epatica . 
lefficacia terapeutica dello shunt intraepatico tuttora dibattuta ; alcuni autori suggeriscono come lentit delle fistole artero - venose polmonari prima del trattamento ed il gradiente porto - sistemico post - tips siano i fattori prognostici pi rilevanti . linsoddisfacente impatto clinico emerso nella nostra esperienza potrebbe essere spiegabile con le comorbilit di cui alcuni dei nostri pazienti erano affetti ( 2 casi di enfisema , 1 caso di pregresso processo specifico )  . 
 nei pazienti da noi trattati , con alvo regolato da lattulosio , la pse indotta dalla tips , nella gran parte dei casi temporanea e di grado lieve o moderato , ha reso di rado necessario lintervento angiografico di riduzione . 
la regressione della pse dopo la tips in pazienti trattati per sanguinamento o ascite intrattabile spiegabile rispettivamente con il cessato assorbimento intestinale delle proteine ematiche e con il sensibile decremento della terapia diuretica . 
 i casi di scompenso cardiaco destro da sovraccarico provocati dalla tips ci hanno indotto a sottoporre ad ecocardiogramma tutti i pazienti candidati alla procedura . radiol med ( 2009 ) 114 : 8394 by discontinued intestinal absorption of blood proteins and by a significant reduction of diuretic treatment , respectively . the cases of right - sided cardiac failure following tips induced us to perform echocardiography on all candidates for the procedure . aspetti tecnici technical aspects us enabled correct patient selection , was effective in guiding the portal puncture and helped to avoid major periprocedural complications [ 36 ]  . 
the cases of intraparenchymal haematoma and haematobilia occurred at the end of particularly complex procedures , and their onset was promoted by the blood dyscrasia typical of cirrhosis . pre - tips radiological assessment , in some cases supplemented by a ct study , provides essential information about the nature , extent and age of the portal thrombus and on the haemodynamics of the splenomesenteric system . our experience confirms previously reported findings [ 37 ] regarding the greater technical difficulty of angiographic procedures , sometimes requiring transcaval puncture , and the high incidence of occlusions at 1 year when patients with budd - chiari syndrome are treated with bare stents . 
this finding suggests that us should be performed more frequently every 34 months . the case of haemoperitoneum emphasises the need for accurate phlebography following tips , with injection of contrast material into the proximal splenic vein in order to demonstrate any persistent varices . in our experience , the patency of self - expandable and thermosensitive bare stents was satisfactory but lower than that of modern polytetrafluoroethylene ( ptfe ) - covered stents [ 38 ]  . 
this type of stent - graft , which has inherent technical limitations , was used in the early years of our experience and was characterised by less accurate patient selection , less technical skill of the interventional radiologists and organisational problems in referring patients for olt . conclusions tips placement is a safe and effective first - line procedure to treat complications of portal hypertension that are refractory to medical and endoscopic therapy . 
 la valutazione radiologica pre - tips , talvolta completata da approfondimento tc , fornisce indispensabili informazioni circa la natura , lestensione e let del trombo portale e sullemodinamica del sistema spleno - mesenterico . 
 la nostra esperienza conferma i riscontri della letteratura [ 37 ] circa la maggior difficolt tecnica delle procedure angiografiche , con necessit talvolta di puntura transcavale , e circa lelevata incidenza di occlusione entro 1 anno degli stent nudi nel trattamento di pazienti con sindrome di budd - chiari . 
 il caso di emoperitoneo rimarca la necessit di eseguire un attento studio flebografico post tips con iniezione di mdc in vena splenica prossimale , al fine di dimostrare eventuali varici persistenti . 
la performance dei nitinol stent e degli stent autoespandibili risulta sovrapponibile , a fronte di una mortalit simile . lincidenza cumulativa di reinterventi degli stent palmaz risultata bassa solo perch la mortalit ad essi associata stata molto elevata ; questi tipi di protesi , che presentavano limiti tecnici intrinseci , sono state impiegate nei primi anni del nostro studio caratterizzati da una meno precisa valutazione dei criteri di elezione alla procedura , da una minor abilit tecnica degli radiologi interventisti e dalla difficolt organizzativa di avviare il paziente allolt . 
the literature indicates that modern covered stents ensure better primary patency than do bare stents and that their higher cost is offset by the fewer angiographic revisions required during the follow - up . although there is consensus regarding the effectiveness of tips in treating variceal bleeding , refractory ascites and hydrothorax despite the increased incidence of pse there is still controversy about the use of tips to treat rarer and more complex conditions , such as budd - chiari syndrome , hrs and hps . finally , in some patients , tips can serve as an effective bridge to olt . 
dalla letteratura emerge come i moderni stent ricoperti garantiscano una maggiore perviet primaria rispetto alle protesi nude , a fronte di un costo maggiore , compensato tuttavia dal minor numero di revisioni angiografiche in corso di follow - up . vi unanime consenso circa lefficacia della tips nel trattamento del sanguinamento da varici , dellascite refrattaria e dellidrotorace , a fronte di unincrementata incidenza di encefalopatia porto - sistemica . 
ancora incerti e dibattuti rimangono i risultati del trattamento mediante tips di quadri clinici pi rari e complessi come la sindrome di budd - chiari , la hrs e la hps . in alcuni pazienti infine la tips pu essere considerata unefficace soluzione temporanea in attesa dellolt ; i tempi di attesa di ogni singolo centro trapianti condizionano indicazioni ed aspetti tecnici della procedura . 
fava1 1istituto di radiologia universit di torino sede san luigi , orbassano , italy 2sc radiodiagnostica i e ii ospedale san giovanni battista , torino , italy 3sc radiodiagnostica ospedale s . 
ninety - eight patients with cerebral tumours , 46 of which were primary ( seven grade 0 - i , nine low - grade gliomas , two gliomatosis cerebri , nine lymphomas and 19 high - grade gliomas ) and 52 secondary , underwent conventional magnetic resonance ( mr ) imaging completed with dwi and dynamic contrast susceptibility pwi . 
seventeen of 98 tumours were cystic or necrotic ( 12 / 17 hypointense and 5 / 17 hyperintense on dwi ) ; the adc value of hyperintense cystic areas was 0.970.2310 - 3 mm2 / s . 
novantotto pazienti con tumore cerebrale , 46 con tumore primitivo ( 7 di grado 0 - i , 9 gliomi a basso grado , 2 gliomatosi cerebri , 9 linfomi , 19 gliomi ad alto grado ) e 52 con metastasi sono stati sottoposti ad esame rm convenzionale completato da acquisizione dwi e da studio perfusionale ottenuto durante la somministrazione di un bolo di gadolinio . 
diciassette tumori erano costituiti da una componente centrale cistica che in 5 casi era iperintensa in dwi ( valore medio adc 0 , 970 , 2310 - 3 mm2 / s )  . ladc della parte solida dei tumori aveva valori compresi tra 0 , 64 e 3 , 510 - 3 mm2 / s . 
la pwi fornisce elementi utili nella diagnosi differenziale tra gliomi a basso ed alto grado e tra gliomi ad alto grado e linfomi . parole chiave risonanza magnetica diffusione perfusione tumori cerebrali introduction introduzione the role of conventional magnetic resonance ( mr ) imaging , with or without contrast agent administration , in the diagnosis of brain tumours is widely accepted . 
mr imaging not only has high sensitivity in detecting and locating lesions , it also gives information about phenomena such as mass effect , haemorrhage , oedema or necrosis , thus helping to differentiate brain tumours from other pathological processes and providing indications about the type of tumour [ 1 , 2 ]  . the importance of characterising tumours ( typing and grading ) to plan appropriate treatment and monitor response to treatment early on in the disease has stimulated research in this area , with numerous studies investigating , over the past decade , the application of new techniques such as diffusion - weighted imaging ( dwi ) , perfusion - weighted imaging ( pwi ) and in vivo mr spectroscopy ( mrs ) [ 14 ]  . the term diffusion refers to the random ( brownian ) movement of water molecules in tissues ; the diffusion capacity of water molecules is tissue - specific and may be altered in given pathological conditions . 
dwi enables assessment of this tissue - related parameter , and calculation of the apparent diffusion coefficient ( adc ) provides major diagnostic clues for evaluating intracranial masses [ 2 , 5 ]  . perfusion reflects the delivery of nutrients to tissue and is defined as flow per unit of time . 
the grey matter of a healthy individual is perfused at a rate of 5060 ml / 100 g / min and the flow maintained in a restricted range by cerebral self - regulation mechanisms . 
low - perfusion states may thus lead to cellular ischaemia , whereas high - perfusion states may be related to hypervascular lesions such as certain tumours [ 6 ]  . the most commonly measured perfusion parameters are cerebral blood volume ( cbv ) , which reflects the amount of blood present in a given amount of tissue at a given time ; cerebral blood flow ( cbf ) , which indicates the quantity of blood transiting through a given amount of tissue in a unit of time ; and mean transit time ( mtt )  . 
these parameters are closely linked to one another , with cbf being equal to the il ruolo della risonanza magnetica ( rm ) convenzionale , con e senza mezzo di contrasto ( mdc ) , nella diagnosi dei tumori dellencefalo saldamente consolidato ; la rm non solo possiede unelevata sensibilit nel riconoscimento e nella localizzazione delle lesioni , ma fornisce informazioni su fenomeni quali leffetto massa , lemorragia , ledema o la necrosi dei tessuti che aiutano nella diagnosi differenziale con altri tipi di processi patologici dando anche indicazioni sul tipo di tumore [ 1 , 2 ]  . limportanza della caratterizzazione ( tipo e grading ) dei tumori , al fine della corretta impostazione terapeutica , nonch lutilit di fornire precoci informazioni sulla risposta alla terapia ha stimolato in questi ultimi anni la ricerca e , nellultima decade , sono stati pubblicati numerosi studi riguardanti limpiego delle nuove tecniche quali la diffusione ( dwi ) , la perfusione ( pwi ) e la spettroscopia in vivo ( mrs ) nella caratterizzazione dei tumori cerebrali [ 14 ]  . con il termine diffusione si indica il movimento random ( browniano ) delle molecole di acqua nei tessuti ; la diffusibilit delle molecole dellacqua caratteristica per ogni tessuto e si pu modificare in determinate condizioni patologiche . 
le sequenze pesate in diffusione permettono di valutare questo parametro tessutale ed il calcolo del coefficiente di diffusione apparente ( adc ) fornisce elementi diagnostici importanti nella valutazione delle masse intracraniche [ 2 , 5 ]  . la perfusione rappresenta lapporto nutritivo ematico ai tessuti e viene definita come il flusso per unit di tempo . solitamente viene misurata in ml / 100 g di tessuto / min , o unit di cbf . 
la sostanza grigia delluomo sano viene perfusa ad un ritmo di 5060 ml / 100 g / min e viene mantenuta in un range ristretto dai meccanismi di autoregolazione cerebrale . 
perci stati di bassa perfusione possono sfociare nellischemia cellulare , mentre stati di elevata perfusione possono essere correlati a lesioni ipervascolari , come alcuni tumori [ 6 ]  . i parametri che pi frequentemente vengono misurati sono : il cbv ( cerebral blood volume ) che equivale alla radiol med ( 2009 ) 114 : 645659 ratio between volume and transit time [ 7 ]  . 
the most frequently used parameter in brain tumour imaging is the relative regional cerebral blood volume ( rrcbv ) , which is increased in tumours as a result of neoangiogenesis [ 8 , 9 ]  . this study correlated the adc and rrcbv values obtained by applying echoplanar ( epi ) and gradient - echo ( gre ) sequences in a large series of brain tumours with histological findings to evaluate the usefulness of this technique in characterising brain tumours . materials and methods in this prospective study conducted between january 2003 and august 2006 , patients with brain tumours were studied with conventional mr imaging complemented by dwi and pwi . 
from among these , 98 patients ( 53 men and 45 women ) were selected on the basis of the following exclusion criteria : lack of histological diagnosis , nonneoplastic lesions , previous treatments on the tumours ( surgery , chemotherapy , radiotherapy ) , incorrect examination technique . all lesions were characterised histologically . 
tumours were subdivided into primary and secondary ; the former were grouped by histological type and grade according to the world health organization ( who ) classification , whereas the latter were classified according to the tumour of origin . study protocol mr imaging was performed during a single session in all patients by using a superconducting 1 - tesla scanner ( signa horizon , ge ) with a maximum gradient strength of 23 mt / m and a slew rate of 77 mt / m / s . 
we used 1 m gadobutrol ( gadovist ) injected intravenously with the aid quantit di sangue presente in una data quantit di tessuto in un dato momento ; il cbf ( cerebral blood flow ) che indica la quantit di sangue che attraversa una data quantit di tessuto nellunit di tempo e lmtt ( mean transit time ) o tempo di transito medio . 
il parametro pi utilizzato nello studio dei tumori cerebrali il volume ematico regionale relativo ( rrcbv ) che aumenta nei tumori in rapporto ai fenomeni di neoangiogenesi [ 8 , 9 ]  . in questo lavoro vengono correlati i valori di adc e di rrcbv , ottenuti su unampia serie di tumori cerebrali utilizzando sequenze echo planari ( epi ) gradient echo ( gre ) , con il relativo dato isto - patologico , per valutare lapporto di questa tecnica nella caratterizzazione dei tumori cerebrali . materiali e metodi nel periodo compreso tra gennaio 2003 e agosto 2006 stato effettuato uno studio prospettico che prevedeva di completare lesame rm convenzionale con acquisizioni dwi e pwi nei pazienti con tumore cerebrale . 
tra questi sono stati selezionati 98 pazienti ( 53 maschi e 45 femmine ) utilizzando i seguenti criteri di esclusione : assenza della diagnosi istologica , lesioni non neoplastiche , pregressi trattamenti sul tumore ( chirurgia , chemioterapia , radioterapia ) , non corretta esecuzione dellesame . tutte le lesioni sono state caratterizzate istologicamente ; i tumori sono stati suddivisi in primitivi e secondari ; i primi sono stati raggruppati per istotipo e grado secondo la classificazione della who , mentre i secondi sono stati classificati sulla base del tumore dorigine . protocollo di studio la rm stata eseguita in tutti i pazienti in ununica seduta utilizzando un magnete superconduttivo operante a 1 tesla ( signa horizon , ge ) con potenza massima dei gradienti di 23 mt / m e slew - rate di 77 mt / m / s . 
 stata impiegata la bobina head di ricezione e trasmissione in quadratura . in tutti i pazienti stato eseguito un esame standard con impiego di sequenze se t1 ( tr / te 500 / 12 ms ) , fse pesate in t2 ( tr / te 4000 / 85 ms etl 13 ) e flair ( tr / te 8000 / 90 ms ti 2000 ms )  . 
sono state ottenute immagini sui tre piani dello spazio con sezioni di 45 mm e gap 0 , 51 mm . prima della somministrazione del mdc stata eseguita in tutti i casi una sequenza pesata in diffusione , sul piano 648 radiol med ( 2009 ) 114 : 645659 of a dual - syringe automatic injector ( medrad ) via an 18gauge needle cannula at a flow rate of 5 ml / s . 
in all cases , a few minutes before the dynamic phase , patients were administered 0.05 mmol / kg of gd as a prebolus to attenuate the t1 effects of bloodbrain barrier ( bbb ) disruption . to study the entire area of the lesion , we acquired a set of 12 slices repeated sequentially 40 times , thus obtaining 480 images in 1 min 12 s . 
all axial images were acquired with the same geometry ( fov , slice thickness , gap , angle ) to enable fusion of the dw and pw images with the corresponding flair and / or contrastenhanced t1 - weighted images . 
adc maps inclusive of the adc calculation were generated by positioning 25to 30 - mm2 regions of interest ( roi ) over the tumour areas . the mean adc values of solid and fluid components were obtained separately for each lesion . pw images were processed by applying a formula to calculate , starting from the baseline t2 value of tissues , the drop in signal during the passage of the bolus ( r2 ) and its subsequent return to the baseline level : r2 * = - 1n [ s ( t ) / s ( 0 ) / te ] where s ( t ) corresponds to the signal intensity at time ( t ) , s ( 0 ) represents the mean mr signal before the arrival of the contrast and te to echo time . 
mathematical integration of the area under r2 * curve ( negative enhancement integral ) corresponds to the cbv . to obtain cbv maps , a number of rois 2530 mm2 in diameter were placed over the tumour in such a way as to cover the entire lesion , and the enhancing and nonenhancing areas of tumour were evaluated separately . 
for each lesion , we calculated the mean rcbv of pathological tissue ( rcbvp ) and normal tissue ( rcbvn ) and the ratio between the two means , thus obtaining a value that we called rrcbv [ 10 ]  . 
stato utilizzato il gadobutrolo 1 m ( gadovist ) , iniettato endovena tramite lausilio di un iniettore automatico a doppia siringa ( medrad ) utilizzando unagocannula 18 g con velocit di flusso 5 ml / s . 
la dose somministrata stata per ogni paziente di 0 , 15 mmol / kg , seguita da 20 ml di soluzione fisiologica ; la fase dinamica stata sempre preceduta di pochi minuti dalla somministrazione di un prebolo di 0 , 05 mmol / kg di gadolinio per attenuare gli effetti t1 di alterazione della barriera ematoencefalica ( bee )  . sono state impostate 12 slices in modo da studiare interamente larea lesionale ripetute in maniera sequenziale per 40 volte ottenendo cos 480 immagini in un 112 . 
le prime 4 sequenze ( 48 slices ) , acquisite prima dellinizio della somministrazione del mdc per raggiungere lo stato di steady - state , sono state escluse dalle successive rielaborazioni . 
tutte le immagini assiali sono state acquisite con la stessa geometria : fov , spessore di strato , gap , inclinazione , per permettere la fusione delle immagini acquisite in dwi e pwi con le relative immagini flair e / o t1 post contrasto . 
dopo linfusione del mdc , sono state effettuate scansioni sui tre piani dello spazio ( coronale , sagittale ed assiale ) con sequenze se t1 - pesate . elaborazione delle immagini sono state successivamente rielaborate sia le immagini dwi sia quelle pwi utilizzando , sulla consolle operativa o sulla workstation ( adw 4.0 ) , un software fornito dalla ge ( functool 2 )  . 
per ogni lesione stata ottenuta separatamente la media delladc relativa alle componenti solide e a quelle fluide . le immagini pwi sono state elaborate applicando una formula che , partendo dal valore t2 di base dei tessuti , calcola la caduta di segnale durante il passaggio del bolo ( r2 ) e il successivo ritorno alla stato di partenza . r2 * = - 1n [ s ( t ) / s ( 0 ) / te ] dove s ( t ) corrisponde al segnale al tempo ( t ) ed s ( 0 ) rappresenta la media del segnale rm prima dellarrivo del contrasto e te il tempo di echo . 
the students t test for unpaired data was applied to the mean values obtained ; values of p < 0.0001 were considered to be statistically significant . results of the 98 patients , 46 had primary brain tumours and 52 had one or more secondary lesions ( table 1 )  . 
 of all tumours examined , 17 were morphologically composed of a necroticcystic central component surrounded by a strongly enhancing solid peripheral rim . the necroticcystic component was hypointense on dwi in 12 tumours and hyperintense in five . 
per ogni lesione stata calcolata la media del rcbv del tessuto patologico ( rcbvp ) e del tessuto sano ( rcbvn ) ed stato calcolato il rapporto tra le due medie ottenendo un valore che chiameremo rrcbv [ 10 ]  . 
ai valori delle medie cos ottenute stato applicato il test t di student per dati non appaiati ; sono stati considerati significativi valori di p < 0 , 0001 . risultati dei 98 pazienti 46 erano portatori di un tumore cerebrale primitivo e 52 di una o pi localizzazioni secondarie ( tabella 1 )  . tra tutti i tumori esaminati 17 erano costituiti morfologicamente da una componente centrale necrotico - cistica con spesso cercine periferico solido dotato di intenso contrast enhancement . 
the rrcbv values of the low - grade ( ii ) and high - grade ( iii - iv ) gliomas , as well as the values of highgrade gliomas and lymphomas , were analysed with students t test for unpaired data . 
the results are shown in tables 2 and 3 . twenty - nine of the brain metastases were from lung cancer , whereas the others were distributed as follows : seven from cancers of the uropoietic system ( six renal carcinomas and one bladder carcinoma ) , seven from breast cancer , four from gastrointestinal cancers , one from melanoma and three from lymphoma . 
a scansione assiale t1 pesata dopo somministrazione del mdc : lesione cistica con orletto iperintenso e cospicuo edema digitato della sostanza bianca perilesionale ; b analoga scansione in dwi : la lesione appare iperintensa ; c mappa adc : il valore di adc allinterno della componente cistica della lesione di 0 , 910 - 3 mm2 / s . 10 13 16 19 22 25 28 31 34 37 40 43 46 49 n pazienti metastasi tumori primari fig . 
2 rappresentazione grafica della distribuzione dei valori di adc nei vari tipi di tumori , distinti tra tumori cerebrali primitivi e metastasi . 652 radiol med ( 2009 ) 114 : 645659 fig . 
a contrast - enhanced t1 - weighted image ; b curves of signal decrease in the regions of interest ; c relative regional cerebral blood volume ( rrcbv ) maps . 
5 confronto dellrrcbv tra gliomi grado iii e grado iv . glioma di iv grado glioma di iii grado linfomi cerebrali gliomi ad alto grado 2 3 4 9 10 10 12 13 14 15 16 17 18 19 pazienti fig . 
i valori di rrcbv relativi ai gliomi a basso grado ( ii ) e quelli ad alto grado ( iii - iv ) , cos come i valori dei gliomi ad alto grado e quelli dei linfomi sono stati sottoposti a test statistici utilizzando la t di student per dati non appaiati ed i risultati ottenuti vengono riportati nelle tabelle 2 e 3 . ventinove delle metastasi encefaliche erano da carcinoma polmonare , mentre le altre erano cos ripartite : 7 da tumori dellapparato uropoietico ( 6 carcinomi renali e 1 carcinoma della vescica ) , 7 da carcinoma mammario , 4 da neoplasie dellapparato digerente , 1 da melanoma e 3 da linfoma . 
in the majority of cases , morphological imaging is able to differentiate low - grade from diffusely invasive or frankly malignant lesions , which tend to show significant perilesional oedema and intense contrast enhancement . radiol med ( 2009 ) 114 : 645659 i tumori neuroepiteliali , in particolare i glomi , rappresentano una causa frequente di tumori dellencefalo . 
gli esami radiologici morfologici sono in grado di differenziare nella maggior parte dei casi le lesioni di basso grado da quelle diffusamente infiltranti o chiaramente maligne che presentano generalmente un significativo edema perilesionale ed unelevata impregnazione contrastografica . 
ci nonostante , non tutte le neoplasie gliali ad alto grado presentano necrosi o effetto massa e circa il 40 % non presenta impregnazione contrastografica [ 2 , 11 ]  . il problema si complica se teniamo conto di altri due elementi : in primo luogo dellelevata frequenza delle metastasi cerebrali che si sviluppano in circa il 15%25% di tutti i pazienti con neoplasie maligne [ 12 ] e in secondo luogo dellaumentata incidenza dei linfomi cerebrali primitivi verificatasi nelle ultime due decadi per aumento della popolazione immucompromessa in relazione allincremento del numero di soggetti sottoposti a trapianto dorgano e di quelli con aids [ 13 , 14 ]  . la rm convenzionale dimostra molti limiti nella differenziazione tra i diversi gradi di tumori primari neuroepiteliali , le metastasi e i linfomi . 
nevertheless , not all high - grade glial tumours exhibit necrosis or mass effect , and approximately 40% of them are nonenhancing [ 2 , 11 ]  . the issue becomes more complex if we consider two other factors : first , the high frequency of cerebral metastases occurring in around 15%25% of all patients with malignancies [ 12 ] , and second , the rising incidence over the past two decades of primary cerebral lymphomas as a result of the increasing number of immunocompromised subjects due to organ transplantations and aids [ 13 , 14 ]  . conventional mr imaging has many limitations in distinguishing among the different grades of primary neuroepithelial tumours , metastases and lymphomas . 
for this reason , it is important to have access to a diagnostic imaging technique capable of enabling the rapid and noninvasive diagnosis and tumour monitoring [ 13 , 15 ]  . diffusion imaging by evaluating the mobility of water molecules in tissue , diffusion imaging can provide diagnostic information in several pathological conditions . 
in cerebral masses , the role of dwi and adc mapping in differentiating cystic tumours from abscesses and epidermoid from arachnoid cysts is known and well established [ 1618 ]  . the five cystic tumours with hyperintense fluid component on dwi resembled abscesses in appearance , although the adc values were slightly higher [ 18 , 19 ]  . 
the high mucinous content explains the adc restriction [ 1820 ]  . the adc of the solid component of the tumours showed wide variations without significant differences among the various types of tumour . 
in our series , the mean adc for lymphomas did not exceed 1.410 - 3 mm2 / s , a finding in agreement with previous reports [ 2 , 4 , 16 , 21 ]  . 
in fact , the extent of oedema strongly affects adc values , and it is likely that steroid treatment , frequently initiated at presentation in patients with brain tumours , influences the dwi parameters [ 22 ]  . perfusion imaging brain tumours may stimulate the formation of new vascular networks , and neoangiogenesis is fundamental for tumour growth . 
the increased metabolic demands of the growing tumour and the resulting hypoxia in large tumours stimulate fornire informazioni diagnostiche in svariate condizioni patologiche nel caso di masse cerebrali noto e consolidato il ruolo delle sequenze dwi e delle mappe delladc nel differenziare i tumori cistici dagli ascessi e le cisti epidermoidi dalle cisti aracnoidee [ 1618 ]  . i 5 tumori cistici con componente fluida iperintensa in dwi avevano un aspetto simile a quello degli ascessi , ma con valori di adc lievemente superiori [ 18 , 19 ]  . 
erano tutte metastasi da carcinoma polmonare ; allesame istologico larea cistica di questi tumori era costituita da tessuto mucinoso nel quale galleggiavano cellule neoplastiche , mentre non era evidenziabile contenuto ematico ; lelevata componente mucinosa spiega la restrizione del coefficiente di diffusione apparente [ 1820 ]  . per quanto concerne ladc delle componenti solide dei tumori i dati ottenuti dimostrano unampia variabilit di valori senza significativa differenza tra i vari tipi di neoplasie ; nella maggior parte dei casi tuttavia i valori di adc erano superiori rispetto a quelli del tessuto sano normale . 
dalla osservazione dei dati emerge che tra tutti i tipi tumorali i linfomi sono quelli che mostrano i valori complessivamente inferiori ; in questa casistica la media di adc per i linfomi non supera mai il valore di 1 , 410 - 3 mm2 / s ; questo concorda con i dati della letteratura [ 2 , 4 , 16 , 21 ]  . 
in realt lentit delledema condiziona molto i valori di adc ed probabile che il trattamento con farmaci corticosteroidei , frequentemente adottato gi allesordio della clinica nei pazienti con tumori cerebrali , influisca sui parametri ottenuti in dwi [ 22 ]  . imaging di perfusione i tumori cerebrali possono indurre la formazione di nuovi vasi ; la neoangiogenesi fondamentale per la crescita dei tumori . 
la prima tecnica , detta spin label , ancora in fase di studio e prevede di marcare i globuli rossi durante il passaggio nei vasi epiaortici e successivamente di valutarne il primo passaggio nel tessuto cerebrale [ 23 ]  . 
i mdc esogeni impiegati sono i chelati del gadolinio che non superano normalmente la bee e quindi si comportano come 656 radiol med ( 2009 ) 114 : 645659 the formation of cytokines responsible for angiogenesis [ 1 ]  . this process is closely related to biological aggressiveness and is one of the main parameters considered in the histopathological grading of glial tumours [ 1 ]  . 
the first technique , known as spin labelling , is still under development and involves tagging red blood cells during their passage in the epiaortic vessels and subsequently evaluating their first pass within cerebral tissue [ 23 ]  . 
the contrast agent compartmentalised inside vessels causes , on first pass when concentration is high , a drop in the t2 signal , which is best appreciated in t * gradient - echo sequences that are most heavily affected by magnetic susceptibility effects . 
studies comparing different gd concentrations have demonstrated that at the same dose levels , the use of 1 m gd increases the first - pass magnetic susceptibility effect , leading to curves with higher peaks [ 2426 ]  . one of the problems arising when evaluating concentration curves with dsci is leakage of contrast material into the extravascular space , which occurs in pathological conditions accompanied by bbb abnormalities . 
this problem can be overcome by administering a small dose of contrast material ( 0.05 mmol / kg ) approximately 5 min before initiating perfusion imaging [ 6 , 8 , 27 ]  . because the rcbv values obtained by applying the negative enhancement integral are not absolute , a standard reference is required to enable comparisons among different patients . 
this could be the rcbv obtained at the level of the contralateral white matter , or ipsilateral normal white matter in the case of lesions affecting both cerebral hemispheres . this provides the rrcbv value , which is calculated with the formula rrcbv = rcbvp / rcbvn [ 10 ]  . the results obtained in our series allow us to make a few concluding remarks . 
if we consider glial tumours , there are statistically significant differences ( p < 0.0001 ) between the rrcbv value of lowand high - grade gliomas ( table 2 )  . 
il mdc compartimentalizzato allinterno dei vasi determina , al primo passaggio , quando la concentrazione elevata , un abbattimento del segnale t2 , meglio valutabile utilizzando sequenze gradient - echo t2 * , che maggiormente risentono degli effetti di suscettibilit magnetica ; questa tecnica denominata con lacronimo dsci ( dynamic contrast susceptibility imaging ) [ 6 , 23 ]  . vengono abitualmente utilizzate sequenze epi che permettono di studiare un esteso volume cerebrale ed offrono il vantaggio di unelevata risoluzione temporale . 
in questo studio stato utilizzato gadolinio ( gd ) alla concentrazione 1 m somministrato a 5 ml / s con una dose pari 0 , 15 mmol / kg ; diversi studi condotti comparando concentrazioni diverse di gadolinio , hanno dimostrato che limpiego di gd 1 m , a parit di dose iniettata , aumenta leffetto di suscettibilit magnetica al primo passaggio per cui si ottengono curve con picco pi elevato [ 2426 ]  . uno dei problemi che insorge nella valutazione delle curve di concentrazione con effetto dsci rappresentato dallo stravaso di mdc nello spazio extravascolare che si verifica in quelle condizioni patologiche che si accompagnano ad alterazione della bee . 
un artificio per ovviare a questo problema quello di somministrare una piccola dose di mdc ( 0 , 05 mmol / kg ) circa 5 minuti prima dellacquisizione perfusionale [ 6 , 8 , 27 ]  . i valori di rcbv , ottenuti applicando lintegrale di enhancement negativo , non sono assoluti ; pertanto , per poter effettuare il confronto tra pazienti diversi , necessario utilizzare un riferimento standard che pu essere rappresentato dal valore di rcbv ottenuto a livello della sostanza bianca controlaterale alla lesione o della sostanza bianca sana omolaterale in caso di lesioni che interessano entrambi gli emisferi cerebrali . 
si ottiene in tal modo lrrcbv che si calcola con formula rrcbv = rcbvp / rcbvn [ 10 ]  . la seguente dai risultati ottenuti in questa casistica si possono trarre alcune considerazioni . 
se si considerano i tumori della serie gliale emergono delle differenze statisticamente significative ( p < 0 , 0001 ) del valore di rrcbv tra gliomi a basso grado e gliomi ad alto grado ( tabella 2 )  . 
pertanto se si fa la media del rcbv posizionando roi allinterno di tutto il tumore , ne deriva una riduzione complessiva dei valori di rrcbv nei tumori pi necroradiol med ( 2009 ) 114 : 645659 neoangiogenesis [ 28 ]  . 
all lymphomas were characterised by a low rrcbv value , constantly lower than 2 ( the maximum value observed was 1.53 ) , whereas the majority of high - grade gliomas had high rrcbv values . 
the differential diagnosis between lymphomas and gliomatoses is , however , straightforward at conventional mr imaging and based on morphology and tumour extension [ 30 , 31 ]  . lowest rrcbv values seen with regard to metastases , no statistically significant differences were seen in the perfusion values of the various types of metastases . 
the high rrcbv values seen in meningiomas , however , are in line with previous reports [ 15 , 26 ]  . conclusions diffusionand perfusion - weighted mr imaging in patients with brain tumours provide additional information that tici . 
per questo motivo stato ipotizzato di utilizzare oltre allimaging convenzionale anche le mappe di rrcbv come guida per effettuare le biopsie stereotassiche [ 29 ]  . se si confrontano i gliomi ad alto grado con i linfomi , per i quali la diagnosi differenziale con lrm convenzionale pu talvolta essere problematica , possiamo vedere come in questo studio i valori di perfusione diano risultati statisticamente significativi ( p < 0 , 0001 )  . 
tutti i linfomi erano caratterizzati da un valore di rrcbv basso , sempre inferiore a 2 ( il valore massimo riscontrato stato di 1 , 53 ) , mentre la maggior parte dei gliomi ad alto grado aveva valori di rrcbv elevati . 
la possibilit di discriminare tra tumori gliali ad alto grado e linfomi concorda con quanto gi riportato da altri studi [ 15 , 20 ]  . un discorso a parte va fatto per le gliomatosi cerebri . 
in questo studio sono compresi solo due casi , ed entrambi hanno bassi valori di rrcbv , simili a quelli dei linfomi e dei tumori low - grade ; questo dato correla con la ridotta microvascolarizzazione di questi tumori il cui grading elevato dato dalla elevata estensione . 
la diagnosi differenziale tra linfomi e gliomatosi tuttavia agevole allo studio rm convenzionale sulla base della morfologia e dellestensione del tumore [ 30 , 31 ]  . per quanto concerne le metastasi non sono invece state riscontrate differenze statisticamente significative dei valori di perfusione tra i vari tipi di metastasi . 
i dati ottenuti oscillano su un ampio range ; i valori di rrcbv risultano pi bassi nelle localizzazioni da linfoma ed in alcuni casi di metastasi da carcinoma del polmone o della mammella ; questultimo dato potrebbe essere correlato , almeno in parte , alle terapie a cui tali soggetti erano sottoposti per il tumore dorigine . 
i valori elevati di rrcbv riscontati nei meningiomi sono in linea con quanto riportato in letteratura [ 15 , 26 ]  . conclusioni le tecniche di diffusione e di perfusione con rm se utilizzate nei pazienti con tumore cerebrale forniscono informazioni non ottenibili con lesame convenzionale , possono essere eseguite a completamento dellesame convenzionale utilizzando lo stesso contrasto e con un minimo aumento del tempo di esecuzione . 658 radiol med ( 2009 ) 114 : 645659 cannot be obtained with conventional mr . 
should dwi and pwi prove superior to conventional imaging , they could be used to monitor patients undergoing treatment to obtain an earlier evaluation of response to chemoor radiotherapy and guide the clinicians treatment choices . le immagini dwi hanno rilevante importanza nella diagnosi delle masse cistiche , mentre non sembrano avere un ruolo nella caratterizzazione dei tumori . 
dwi e pwi inoltre si propongono come tecniche promettenti nel management dei tumori cerebrali : il dato relativo alla microvascolarizzazione offerto dalla pwi potrebbe servire come guida al prelievo bioptico , indicando le aree maggiormente aggressive . 
sardanelli servizio di radiologia , dipartimento di scienze medico - chirurgiche , universit degli studi di milano , irccs policlinico san donato , via morandi 30 , 20097 san donato milanese , italy a . 
the mr protocol applied at our institution for both diagnosis and follow - up after surgical or endovascular treatment consists of four steps : morphologic study , cine mr study , flow analysis , and mr angiography ( mra )  . the first three sequences are acquired during breath - hold and with electrocardiographic gating . 
cine true - fast imaging with steady - state precession ( true - fisp ) sequences show not only morphologic features but also blood - flow changes inside the aorta . 
gradient - echo sequences for phase - velocity mapping allow flow analysis . application of bernoullis equation here briefly presented and discussed allows for calculation of the pressure gradient caused by the coarctation . 
mra , acquired with a breath - hold three - dimensional t1weighted gradient - echo sequence and intravenous administration of paramagnetic contrast material , allows for optimal depiction of the aortic lumen , with a panoramic view of the whole aorta , its main branches and possible collateral circulation . 
 keywords aorta aortic coarctation bernoullis equation magnetic resonance ( mr ) imaging mr flow analysis ( phase - velocity mapping ) riassunto la coartazione aortica rappresenta il 5%10% di tutte le patologie congenite del cuore e dei grandi vasi e il 7% dei casi di piccoli cardiopatici in condizioni critiche . 
la risonanza magnetica ( rm ) permette lo studio di questa patologia con una serie di vantaggi rispetto a tecniche alternative quali langiografia convenzionale , lecografia transesofagea e la tomografia computerizzata . 
il nostro protocollo rm , utilizzato sia per la diagnosi , sia per il follow - up dopo trattamento chirurgico o endovascolare , consiste di quattro fasi : studio morfologico , cinetico , flussimetria e angio - rm . 
le sequenze a sangue chiaro true - fast imaging with steady - state precession ( true - fisp ) , oltre a dare informazioni di tipo morfologico , mostrano le alterazioni del flusso ematico allinterno del vaso . 
le sequenze gradient - echo con mappaggio fase - velocit consentono la quantificazione del flusso ; lapplicazione dellequazione di bernoulli ( qui brevemente presentata e discussa ) , consente infatti il calcolo del gradiente pressorio determinato dalla coartazione . 
lo studio angiorm , ottenuto in apnea mediante sequenze gradient - echo tridimensionali t1 - pesate con somministrazione endovenosa di mezzo di contrasto paramagnetico , mostra una visione volumetrica panoramica del lume dellaorta , delle sue principali ramificazioni e , quando presenti , dei circoli collaterali . 
 parole chiave aorta coartazione aortica equazione di bernoulli flussimetria rm risonanza magnetica ( rm ) radiol med ( 2009 ) 114 : 524537 introduction introduzione over recent years , several magnetic resonance ( mr ) techniques have been successfully applied for evaluating congenital heart diseases . 
we summarize here the currently available knowledge about coa , including epidemiology , aetiopathogenesis , topographic classification , and the different mr imaging techniques . negli ultimi anni numerose tecniche di risonanza magnetica ( rm ) sono state applicate con successo alla valutazione delle cardiopatie congenite . 
la coartazione aortica ( coa ) rappresenta un reperto non infrequente nella pratica clinica , pari a circa il 5%10% di tutte le malformazioni congenite del cuore e dei grandi vasi [ 1 ]  . 
sono qui rivisitate le attuali conoscenze sulla malattia relativamente a epidemiologia , eziopatogenesi , classificazione topografica e studio con differenti tecniche rm . definition coarctation is a term derived from the latin coarctatio , meaning narrowing or stricture . 
similar congenital malformations are aortic atresia and the true aortic interruption , mostly located at the arch ( interrupted aortic arch )  . coa , also known as congenital aortic stenosis , was originally noted during autopsy by j.f. 
he collected 200 previously documented cases , but coa was not regularly diagnosed until after 1933 [ 6 ]  . epidemiology and aetiology coa accounts for 5%10% of all congenital heart diseases and represents 7% of critically ill infants with heart disease . it is seven times more common in caucasian than in asian population . 
in atlanta ( usa ) from 1970 to 1983 , the prevalence per 1 , 000 live births was as follows : interruption of the aortic arch , 0.05 ; coarctation , 0.36 ; hypoplasia of the aorta , 0.06 [ 7 ] , giving a total prevalence of 0.47 per 1 , 000 live births . 
in bohemia in 1980 , a prevalence of 6.67 congenital heart malformations per 1 , 000 live births was reported , and 5.77% of these malformations consisted of coa cases [ 9 ] , giving a coa prevalence of 3.84 per 1 , 000 live births . the aetiology of coa is still unclear . 
up to 60% [ 10 ] or 85% [ 1 ] of coa cases are associated with bicuspid aortic valve , supporting the hypothesis of a common cause for the two congenital malformations [ 11 ] or an influence of the bicuspid aortic valve on the development of coa [ 1 ]  . 
pathologic examination of the ascending aorta of patients with definizione il termine coartazione deriva dal latino coarctatio , letteralmente restringimento ovvero , nel caso di una struttura vascolare , riduzione di calibro cui consegue ostruzione al flusso ematico . 
paris [ 4 ] ne forn la prima descrizione accurata nel 1791 mentre j . abbott pubblic una serie autoptica retrospettiva di 200 casi nel 1928 [ 5 ] , ma la malattia non stata diagnosticata con regolarit fino a dopo il 1933 [ 6 ]  . epidemiologia ed eziologia la coa rappresenta il 5%10% di tutte le patologie congenite del cuore e dei grandi vasi e il 7% dei casi di piccoli cardiopatici in condizioni critiche . 
 si osserva una prevalenza maschile con rapporto maschi / femmine tra 1 , 3 e 2 , 1 nella maggior parte delle serie [ 1 ]  . nellarea metropolitana di atlanta ( usa ) stata osservata tra il 1970 e il 1983 una prevalenza su 1000 nati vivi pari a 0 , 05 per linterruzione dellarco , 0 , 36 per la coartazione e 0 , 06 per lipoplasia [ 7 ] , con una prevalenza totale pari al 0 , 47 per 1000 nati vivi . 
una prevalenza pari a 0 , 32 per 1000 nati vivi stata riportata per lislanda dal 1980 al 1994 [ 8 ]  . in boemia nel 1980 stata riportata una prevalenza di 6 , 67 malformazioni congenite cardiache per 1000 nati vivi ; il 5 , 77% di queste era costituito da casi di coa [ 9 ] , per una prevalenza di coa pari a 3 , 84 per 1000 nati vivi . leziologia della coa non ancora stabilita con certezza . 
si associa a bicuspidia valvolare aortica fino al 526 radiol med ( 2009 ) 114 : 524537 bicuspid aortic valve frequently shows loss of smoothmuscle cells and severe degeneration of the medial elastic fibers ( so - called cystic medial necrosis ) [ 11 ]  . 
associated cardiac defects are observed in approximately 50% of patients with coa , mostly being left - sided hypoplastic or obstructive defects and ventricular septal defects [ 1 ]  . 
moreover , the higher coa prevalence in males and a relatively high prevalence in patients with turners syndrome suggest a link between x - chromosome defects and anomalous development of the aorta and valve [ 11 ]  . 
however , this classification is now considered too simplistic because many patients lack symptoms , and coa diagnosis is delayed until adulthood [ 14 ]  . only malformations determining a total obstruction or a severe degree of stenosis ( severe tubular hypoplasia , severe coarctation , vessel atresia or interruption ) or associated with cardiac defects are diagnosed during childhood [ 13 ]  . 
thus , the prevalence in adulthood , including the nonsevere form of coa , should be higher than the incidence in live births . a commonly accepted classification is based on stenosis location : preisthmic , isthmic and postisthmic . 
 a physiopathologic approach is given by the subdivision 60% [ 10 ] o all85% dei casi [ 1 ] , supportando lipotesi di una causa comune alle due malformazioni [ 11 ] o di uninfluenza della bicuspidia valvolare aortica sullo sviluppo della coa [ 1 ]  . 
indagini istologiche dellaorta ascendente di soggetti con bicuspidia valvolare hanno mostrato un ridotto numero di cellule muscolari lisce e severa degenerazione delle fibre elastiche della tonaca media ( cosiddetta necrosi medio - cistica ) [ 11 ]  . 
malformazioni cardiache congenite si associano a coa in circa il 50% dei casi , per lo pi rappresentate da sindromi ipoplasiche o ostruttive delle cavit sinistre o da difetti del setto interventricolare [ 1 ]  . 
dal 3%5% [ 1 ] al 10% [ 12 ] dei pazienti con coa presentano altres aneurismi intracranici , in accordo con lipotesi che la coa sia parte di una patologia arteriosa diffusa , secondaria ad anomalie dello sviluppo della cresta neurale [ 12 ]  . 
inoltre , la maggiore prevalenza di coa nei maschi e nei pazienti con sindrome di turner induce a ipotizzare un legame tra difetti del cromosoma x ed alterazioni dello sviluppo dellaorta e della valvola aortica [ 11 ]  . 
solo le malformazioni che comportano stenosi di grado elevato o ostruzione totale del flusso ematico ( ipoplasia tubulare serrata , coartazione serrata , atresia o interruzione del vaso ) o che si associano a malformazioni cardiache sono diagnosticate in et infantile [ 13 ]  . ne deriva che la prevalenza in et adulta , includendo le forme non severe di coa , dovrebbe essere sensibilmente pi elevata di quella calcolata in base alla diagnosi sui nati vivi . radiol med ( 2009 ) 114 : 524537 fig . 
1a - c angio - rm ( ricostruzioni volumetriche ) di casi di : ipoplasia tubulare dellarco aortico ( freccia in a ) , coartazione istmica ( freccia in b ) e interruzione dellaorta discendente ( freccia in c )  . into preductal , ductal and postductal coa , referring to the location of the botallo ductus arteriosus . 
this kind of coa , observed in approximately 5% of infants with turner syndrome , typically results from a cardiac anomaly during fetal life decreasing blood flow through the left ventricle , leading to hypoplastic development of the aorta . 
in postductal coa , the narrowing is distal to the insertion of the ductus arteriosus . as a consequence , blood flow to the lower body is impaired . it is thought to be the consequence of muscular cells extending from ductus arteriosus into the aorta during fetal life [ 15 ]  . clinical features and treatment the age of clinical presentation is mainly related to the degree of stenosis and to the presence of associated abnormalities . 
nella forma preduttale la coa prossimale allinserzione del dotto ; se severa , il flusso a valle dipende dalla perviet del dotto la cui chiusura , quindi , pu risultare fatale . 
questo tipo di coa , osservato in circa il 5% dei nati affetti da sindrome di turner , tipicamente il risultato di anomalie cardiache fetali con ridotto efflusso dal ventricolo sinistro , cui consegue unipoplasia dellaorta . 
nella forma post - duttale la coa a valle dellinserzione del dotto e ne risulta un ridotto flusso alla porzione inferiore del corpo ; ritenuta essere la conseguenza della migrazione di miocellule dal dotto arterioso allaorta durante la fase fetale [ 15 ]  . 
si dovrebbe sempre considerare lipotesi di coa in soggetti adolescenti o giovani di sesso maschile con 528 radiol med ( 2009 ) 114 : 524537 coa becomes clinically relevant , it can lead to systemic hypertension and secondary left ventricular hypertrophy with heart failure . 
if it is not treated , the patients mean age of death is about 34 years [ 16 ]  . invasive treatment should always be considered in patients with pressure gradients > 30 mmhg on cardiac catheterization [ 17 ]  . 
successful surgical correction of coa by resection of the stenotic tract with end - to - end anastomosis was first described by crafoord and nylin in 1945 [ 18 ]  . 
 perioperative mortality rates are determined largely by age and concomitant congenital heart disease rather than by the choice of operative technique for correcting coa [ 23 ] and are less than 3% for older children and adults [ 24 ]  . several postsurgical complications such as cerebrovascular , cardiac and aortic events may occur . 
the most common complications are cerebrovascular accidents , cerebral haemorrhage , recurrent hypertension , heart failure , endocarditis , endarteritis , coronary artery disease , recoarctation , poststenotic aneurysm , and aortic rupture [ 10 ]  . 
due to successful surgical or endovascular treatments , follow - up of treated adult patients is often required . imaging of coa a posteroanterior chest x - ray examination can show a dilated ascending aorta , low prominence of the first left arch , a notch sign corresponding with the location of coa and small notches on the inferior posterior margin of ribs , mainly from fourth to eighth , due to the osteolytic effect of the collateral hypertrophic intercostal arteries . 
 similarly to aortic dissection [ 26 ] , coa can be diagnosed using transesophageal echocardiography ( tee ) , digital subtraction angiography ( dsa ) , computed tomography ( ct ) , and mr imaging . 
due to the use of ionising radiation and iodinated contrast agents , ct and dsa are not regarded as first - line techniques for diagnosing coa , particularly in children . 
 over recent years , mr imaging has become a well - established diagnostic tool for studying congenital heart diseases and coa [ 27 , 28 ] , offering many advantages over other ipertensione agli arti superiori e ipotensione e polsi deboli agli arti inferiori . 
se non trattata , porta al decesso mediamente a 34 anni di et [ 16 ]  . il trattamento invasivo dovrebbe essere sempre considerato nei pazienti che presentano un gradiente pressorio maggiore di 30 mmhg al cateterismo cardiaco [ 17 ]  . crafoord e nylin [ 16 ] descrissero per primi , nel 1945 , lintervento correttivo che prevede la resezione del tratto stenotico con successiva anastomosi termino - terminale . successivi miglioramenti delle tecniche chirurgiche [ 18 , 20 ] , tra i quali lintroduzione dellaortoplastica con flap dellarteria succlavia , hanno permesso la correzione in caso di varianti anatomiche complesse . 
 i tassi di mortalit peri - operatoria , determinati soprattutto dallet del paziente e da eventuali anomalie associate piuttosto che dalla tecnica utilizzata per la correzione della coa [ 23 ] , sono inferiori al 3% sia nei bambini che negli adulti [ 24 ]  . 
sono riportate complicanze post - chirurgiche quali lesioni cerebrovascolari , emorragie cerebrali , ipertensione recidivante , scompenso cardiaco , endocardite , endoarterite , patologie coronariche , ricoartazione , aneurismi post - stenotici e rottura dellaorta [ 10 ]  . 
il successo del trattamento chirurgico o endovascolare della coa pone oggi lesigenza del follow - up in et adulta dei pazienti trattati . imaging della coa il radiogramma toracico postero - anteriore pu mostrare ectasia dellaorta ascendente , scarsa prominenza del primo arco di sinistra , incisura in corrispondenza della sede di coartazione e piccole incisure sul margine inferiore dellarco posteriore delle coste , per lo pi dalla quarta allottava , dovute alleffetto osteolitico delle arterie intercostali collaterali ipertrofiche . 
 come per la dissezione aortica [ 26 ] , la diagnosi di coa pu essere posta mediante ecocardiografia transesofagea ( ete ) , angiografia digitale con sottrazione dimmagine ( ads ) , tomografia computerizzata ( tc ) e rm . 
the mr examination takes about 30 min ; the postprocessing requires about 30 min . setting up the patient a good electrocardiographic ( ecg ) line resulting from correct placement of four leads over the anterior or posterior left side of the chest is crucial to obtain a good cardiac synchronization ( ecg gating ) [ 35 ]  . 
la tc e lads non sono considerate tecniche di prima scelta per la diagnosi di coa , soprattutto in et pediatrica , a causa dellutilizzo di radiazioni ionizzanti e mezzi di contrasto ( mdc ) iodati . 
essa offre molteplici vantaggi rispetto alle altre tecniche di imaging cardiovascolare tra i quali la possibilit di ottenere immagini native multiplanari senza luso di radiazioni ionizzanti , lelevata risoluzione temporale ( fino allimaging in tempo reale ) e la possibilit di studio flussimetrico [ 2931 ]  . 
 nello studio dei grandi vasi , la rm vede il suo esordio oltre ventanni or sono con semplici sequenze spin - echo ( se ) e gradient - echo ( ge ) con rifocalizzazione degli spin in flusso laminare . 
successivamente sono state introdotte le sequenze turbo - se ( tse ) , ge cine - rm , ge segmentate , half - fourier acquisition single shot turbo spin - echo ( haste ) e true - fast with steady - state precession ( truefisp )  . 
sequenze ge con mappaggio fase - velocit permettono , inoltre , di ottenere dati flussimetrici [ 33 ] mentre sequenze ge tridimensionali con somministrazione endovenosa di mdc paramagnetico permettono di ottenere immagini simil - angiografiche ad ampio campo di vista , sulle quali si possono effettuare misure accurate del lume aortico [ 34 ]  . protocollo rm faremo qui riferimento alla nostra esperienza ( 20032007 ) con apparecchiatura operante a 1 , 5 t ( magnetom sonata maestro class , siemens , erlangen , germania ) presso lirccs policlinico san donato ( san donato milanese , milano , italia ) su pazienti con coa prima del trattamento e nel loro follow - up a breve e lungo termine . 
thus , we prefer the use of breath - hold ecg - gating : dark - blood t2 - weighted haste [ 37 ] , with high il corretto posizionamento di quattro elettrodi sullemilato sinistro del torace , anteriormente o posteriormente , cruciale per una buona sincronizzazione con lelettrocardiogramma ( ecg - gating ) [ 35 ]  . 
the acquisition of an image passing through the ascending and descending aorta ( three parallel oblique lines ) is planned on a scout axial true fast imaging with steady - state precession ( true fisp ) image ( a )  . 
2a , b definizione del piano obliquo anteriore sinistro ( oas ) per lo studio dellaorta toracica . sullimmagine assiale true - fast imaging with steady - state precession ( true - fisp ) di centratura ( a ) rappresentata la pianificazione di una scansione oas passante per laorta ascendente e discendente ( tre linee oblique parallele )  . 
3a , b bright - blood image ( true - fast imaging with steady - state precession ) ( a ) and dark - blood image ( half - fourier acquisition single - shot turbo spin - echo ) ( b ) , along the same left anterior oblique plane passing through an isthmic coarctation ( arrow )  . 
3a , b immagini a sangue chiaro ( true - fast imaging with steady - state precession ) ( a ) e a sangue scuro ( half - fourier acquisition single - shot turbo spin - echo ) ( b ) lungo il piano obliquo anteriore sinistro passante per una coartazione istmica dellaorta ( freccia )  . 
breath - hold , ecg - gated cine true - fisp sequences ( bright blood , hybrid t2 / t1 - weighted ) are acquired for multiple frames along the cardiac cycle . 
la nostra preferenza va a sequenze in apnea e con sincronizzazione ecg : haste a sangue scuro , pesate in t2 [ 37 ] , con elevato radiol med ( 2009 ) 114 : 524537 fig . 
4 immagine cine true - fast imaging with steady - state precession lungo il piano obliquo anteriore sinistro : coartazione istmica dellaorta ( freccia nera ) ; marcato jet anterogrado ( frecce bianche ) da accelerazione di flusso post coartazione . flow study this part of the mr protocol involves the use of ge phasevelocity mapping sequences on planes orthogonal to the longitudinal axis of the vessel ( through - the - plane acquisition )  . 
phase - velocity sequences provide two different set of images : ( 1 ) magnitude images that give anatomical information , and ( 2 ) phase images that give data about flow direction and velocity . 
si utilizzano sequenze true - fisp ( a sangue chiaro , pesatura ibrida t2 / t1 , con sincronizzazione ecg ) acquisite in apnea per molteplici frame lungo le fasi del ciclo cardiaco . 
per studiare il flusso aortico post - coartazione necessario impostare unelevata codifica di velocit ( velocity encoding , venc ) , generalmente tra 350 e 500 ms , onde evitare artefatti ( aliasing ) nel lume aortico . 
lacquisizione fornisce due serie di immagini : una serie con significato anatomico ( immagini di magnitudo o modulo ) e una serie con significato funzionale ( immagini di fase ) , contenente informazioni su direzione e velocit del flusso . 
lacquisizione lungo il piano obliquo anteriore sinistro ( a ) evidenzia minimo restringimento residuo ( freccia ) ; lacquisizione lungo il piano valvolare aortico ( b ) evidenzia la coesistente bicuspidia ( frecce )  . 
since the kinetic energy of the blood is proportional to the square of its velocity , the right side of bernoullis equation represents the difference between the kinetic energy of blood after coa and that before coa . 
siccome lenergia cinetica del sangue proporzionale al quadrato della sua velocit , il membro destro dellequazione di bernoulli rappresenta la differenza tra lenergia cinetica del sangue a valle della coa e quella a monte della coa . 
 al fine di esprimere p in mmhg anzich in pascal ( pa ) , lunit di misura della pressione nel sistema internazionale , occorre introdurre il seguente coefficiente di conversione : 1 pa = 0 , 0075 mmhg infine , ricordando che la densit del sangue d pari a circa 1067 g / l , otteniamo : i.e. 
if v1 and v2 are given in m / s , the coefficient 4 adjusts the measurement units so to allow the pressure gradient p to be expressed as mmhg . 
se le velocit v1 e v2 sono espresse in m / s , il coefradiol med ( 2009 ) 114 : 524537 that the peak velocity before coa ( v1 ) is generally negligible if compared with the peak velocity after coa ( v2 )  . 
first , it works only if the patient is in the supine position , as the nonperfect horizontal position introduces the gravity - force effect ( this limitation is not relevant for mr applications )  . 
in such a context , a p > 20 mmhg is highly suggestive of significant coa [ 41 , 42 ]  . mr angiography ( mra ) contrast - enhanced mra is a reliable technique for evaluating great vessels . 
for a long time , gadolinium chelates have been considered safe contrast agents and have been used in patients allergic to drugs or iodinated contrast agents and in nephropathic or cardiopathic patients [ 43 ]  . 
patients with severe renal failure [ glomerular filtration rate ( gfr ) < 30 ml / min1.73 m2 ] are considered to be at risk [ 44 , 46 ]  . 
in patients with gfr30 ml / min1.73 m2 , a single dose of 0.1 mmol / kg of gadolinium - based contrast agent can be safely administered intravenously [ 46 ]  . 
for diagnosis or follow - up of coa , we used a power injector with an injection rate of 2 ml / s for both the contrast material and the following 20 - ml saline flush . 
we used a three - dimensional breath - hold , not ecg - gated , t1 - weighted ge sequence with a short acquisition time ( nearly 20 s )  . 
in patients with gfr < 30 ml / min1.73 m2 , time - of - flight and phase - contrast sequences can be used , even though image quality is lower and veins are also visualized [ 47 ]  . 
sulla ricostruzione volumetrica posteriore obliqua ( a ) sono riportate le sedi del calcolo dellarea delle sezioni del vaso a monte della coartazione , al livello della coartazione e a valle della coartazione . 
a sinistra sono riportati i valori di tali aree come normal a , minimum e area 01 , rispettivamente ; inoltre riportato come ratio 01 il rapporto percentuale tra larea a monte della coartazione e larea al livello della coartazione ( grado di stenosi )  . 
la linea centrale endoluminale ( frecce in a ) , generata automaticamente , permette la ricostruzione lungo il piano curvo ( b )  . ficiente 4 consente di esprimere il gradiente p in mmhg . unulteriore semplificazione possibile considerando che la velocit di picco a monte della stenosi ( v1 ) in genere trascurabile rispetto alla velocit a valle della stenosi ( v2 ) e , quindi , pu essere ignorata . 
in primo luogo , la formula di bernoulli valida solo se il paziente supino , in quanto la posizione ortostatica introdurrebbe nella formula un termine aggiuntivo che tiene conto della forza di gravit ( tale limitazione non rilevante per usuali applicazioni rm )  . 
i chelati del gadolinio sono stati considerati a lungo mdc privi di effetti collaterali e si riteneva potessero essere impiegati anche in presenza di allergie a farmaci o ai mdc iodati cos come in caso di pazienti nefropatici o cardiopatici [ 43 ]  . 
sono considerati a rischio pazienti con insufficienza renale grave ( gfr , rateo di filtrazione glomerulare < 30 ml / min1 , 73 m2 ) [ 44 , 46 ]  . 
in pazienti con gfr 30 ml / min1 , 73 m2 si pu utilizzare la singola dose endovena ( 0 , 1 mmol / kg ) di un chelato del gadolinio senza rischi per il paziente [ 46 ]  . 
per la diagnosi e il follow - up della coa , noi utilizziamo un flusso di 2 ml / s sia per il mdc , sia per il bolo di 20 ml di soluzione fisiologica , entrambi somministrati con iniettore automatico . 
in caso di gfr < 30 ml / min1 , 73 m2 possibile impiegare sequenze angiografiche senza mdc ( time of flight e phase contrast ) ottenendo per immagini di qualit inferiore comprendenti anche i vasi venosi [ 47 ]  . 
maximum intensity projections allow aortic demonstration in the angiographic - like view . surface shading display and volume - rendering techniques , obtained with standardised reconstruction algorithms , allow reliable measurements . 
in order to correctly measure aorta diameters and assess the degree of stenosis , measurements should be performed both in lao and in planes orthogonal to the longitudinal axis of the vessel . 
the distance of the coa from the left subclavian artery origin is an important variable for surgical or endovascular therapy planning . le rielaborazioni di volume ( volume rendering technique ) e di superficie ( surface shading display ) , con algoritmi di ricostruzione standardizzati , permettono misurazioni accurate . 
la distanza della coa dallorigine dellarteria succlavia sinistra o dai vasi epiaortici un dato importante nel planning della procedura chirurgica o endovascolare . conclusioni conclusions to correctly diagnose coa , establish disease severity and evaluate treatment options , as well as for follow - up during adulthood , a complete mr protocol is required , including morphological , functional , and flow study as well as contrast - enhanced mra and accurate postprocessing . per diagnosticare correttamente i casi di coa , valutare lentit della stenosi e le possibilit terapeutiche , cos come nel follow - up in et adulta , necessario un protocollo rm che comprenda acquisizioni morfologiche , cinetiche , flussimetriche e angiografiche , completato da accurato postprocessing . 
among the various therapies , local radiotherapy is the gold standard for pain palliation from single metastasis , even though the maximum benefit is obtained between 12 and 20 weeks from initiation . 
from november 2003 to may 2008 , ten ablation treatments were performed in ten patients with acute pain from metastatic bone lesions . patient selection and choice of the most appropriate ablation treatment was made based on lesion characteristics . 
three patients were treated with radiofrequency , one with plasma - mediated radiofrequency , two with plasma - mediated radiofrequency and cementoplasty , three with radiofrequency and cementoplasty and one with microwave . 
in both cases , 3 - month follow - up showed a statistically significant reduction of pain no case did local complications occur either during or after treatment . only one patient treated with radiofrequency ( 1 / 9 , 11% ) developed low - grade fever and general malaise during the 6 days following the procedure , compatible with a postradiofrequency syndrome , which was treated with riassunto obiettivo . 
tra le varie terapie , la radioterapia locale il gold - standard nella palliazione del dolore da metastasi singola , anche se il massimo beneficio si ottiene tra le 12 e le 20 settimane dallinizio della terapia . 
la valutazione stata effettuata non solo con imaging , ma anche con una vas score ( visual analoge scale ) per la determinazione del dolore e con la variazione delle dose equivalenti di morfina . 
solamente in un paziente trattato con radiofrequenza ( 1 / 9 , 11% ) abbiamo riscontrato nei 6 giorni successivi al trattamento insorgenza di febbricola e malessere generale compatibile con la sindrome postradiol med ( 2009 ) 114 : 608625 acetaminophen ( paracetamol ) only and resolved on day 7 . 
percutaneous ablation therapies represent a safe and valuable alternative for treating localised pain from single bone metastasis , providing rapid ( 4 - week ) relief of symptoms and a significant reduction in morphine doses . 
le tecniche ablative percutanee rappresentano una sicura e valida alternativa al trattamento del dolore localizzato da metastasi ossee singole , apportando in breve tempo ( 4 settimane ) un miglioramento della sintomatologia e una sensibile riduzione delle dosi di morfina . 
ci concorre a migliorare la qualit della vita in pazienti affetti da malattia metastatica . parole chiave metastasi osso palliazione ablazione introduction introduzione bone metastases are a common problem in cancer patients , affecting up to 30% of patients with epithelial cancers . 
in 70% of cases , the metastases originate from cancers of the prostate or breast , in 20%30% from cancers of the lung or kidney and in 10% from cancers of the rectum , colon , ovary and pancreas [ 1 ]  . the causes of pain in patients with bone metastases are not fully understood but appear to be unrelated to the type of tumour , location , number or size of the metastatic lesions . possible mechanisms of pain include stretching of the periosteum secondary to tumour growth , fractures ( both micro and macro ) , cytokine - mediated osteoclastic bony destruction that results in stimulation of the nerve endings in the endosteum and tumour growth into surrounding nerves and tissues [ 2 ]  . several types of treatment , including chemotherapy , hormonal therapy , surgery , radiotherapy and radiometabolic therapy , are used for palliation purposes . 
however , a number of patients fail to benefit from these conventional treatments , and pain relief , when achieved , does not occur until 412 weeks after treatment [ 3 ]  . 
a variety of alternative strategies have been proposed for treating painful bone metastases , all of which are based on image - guided percutaneous procedures for ablating focal bone lesions [ 1 , 4 , 5 ] , in some cases associated with cementoplasty [ 68 ]  . the aim of this study was to evaluate the technical success , effectiveness and possible complications of percutaneous ablation treatment in patients with painful bone metastases . 
esse nel 70% dei casi insorgono dal tumore della prostata o della mammella , nel 20%30% dal tumore del polmone o del rene , nel 10% dalle neoplasie del retto , colon , ovaio e pancreas [ 1 ]  . le cause di dolore in soggetti affetti da metastasi ossee non sono ancora completamente note , ma non sembrano correlate al tipo di tumore primitivo , alla localizzazione della lesione , al numero e alle dimensioni delle lesioni . 
possibili meccanismi nella genesi del dolore comprendono : stretching del periostio secondario alla crescita del tumore ; fratture ( sia micro - fratture che macro - fratture ) ; distruzione ossea di tipo osteoclastico citochino - mediata che determina una stimolazione delle fibre nervose terminali endostali ; crescita tumorale nelle strutture nervose e nei tessuti adiacenti [ 2 ]  . 
alcuni pazienti non riescono a trarre benefici da questi trattamenti convenzionali e il sollievo dal dolore , quando si verifica , non avviene mai prima di 412 settimane [ 3 ]  . 
sono state proposte varie strategie alternative per il trattamento delle metastasi ossee dolorose , che richiedono metodiche percutanee imaging - guidate finalizzate allablazione delle lesioni focali ossee [ 1 , 4 , 5 ] , in alcuni casi associando la cementoplastica [ 68 ]  . scopo del lavoro stato quello di valutare il successo tecnico , lefficacia e le eventuali complicanze in pazienti affetti da metastasi ossee sintomatiche e sottoposti a terapia ablativa percutanea . 
 610 radiol med ( 2009 ) 114 : 608625 materials and methods materiali e metodi between november 2003 and may 2008 , we performed ten ablation treatments in ten patients ( five men and five women ; mean age 62 years ; range 2882 ) with acute pain from bone metastases of different origin , site ( table 1 ) and size ( mean volume 63.25 cm3 ; range 218.93.3 cm3 ) ( table 2 )  . 
in all of these patients , the pain had proved refractory to conventional approaches . owing to the poor expected response , one patient received no treatment before the ablation procedure ( table 1 )  . 
three patients were treated with radiofrequency ( rf ) alone , one with plasma - mediated rf , two with plasma - mediated rf combined with cementoda novembre 2003 a maggio 2008 sono stati effettuati , nel servizio di radiologia del nostro ospedale 10 trattamenti in 10 pazienti , 5 uomini e 5 donne ( et media 62 anni , range da 28 a 82 anni ) con dolore acuto da lesioni metastatiche ossee di varia origine , sede ( tabella 1 ) e volume ( volume medio 63 , 25 cm3 , range da 218 , 9 a 3 , 3 cm3 ) ( tabella 2 )  . tutte le lesioni trattate erano osteolitiche . 
 quattro pazienti erano stati precedentemente sottoposti a radioterapia e chemioterapia , 1 paziente solo a radioterapia , 4 pazienti solo a chemioterapia : in questi casi si sono dimostrati refrattari alle terapie convenzionali . 
nessun paziente era suscettibile di trattamento chirurgico , per lassenza di rischio di frattura patologica . tre pazienti sono stati trattati solo con radiofrequenza ( rf ) , table 1 personal series patient no . / age / gender primary tumour histology site of metastasis radiotherapy chemotherapy bladder liver liver liver breast lung lung colon - rectum transverse colon uterine cervix carcinoma right 8th rib left 9th rib left ischiopubic ramus right 8th rib infiltrating lobular vertebra l4 carcinoma adenocarcinoma adenocarcinoma adenocarcinoma adenocarcinoma squamous cell carcinoma vertebra l1 left sacroiliac joint left acetabolum left ischiatic spine left iliac wing not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive n / et / sesso tumore primitivo istologia sede metastasi radioterapia chemioterapia vescica fegato fegato fegato mammella polmone polmone carcinoma carcinoma lobulare vertebra l4 infiltrante adenocarcinoma adenocarcinoma viii arcata costale destra ix arcata costale sinistra branca ischio - pubica sinistra viii arcata costale destra non responsivo non responsivo non responsivo non responsivo non responsivo vertebra l1 articolazione sacroilaca sinistra acetabolo sinistra spina ischiatica sinistra ala iliaca sinistra non responsivo non responsivo non responsivo non responsivo non responsivo non responsivo non responsivo non responsivo colon - retto colon trasverso portio uterina adenocarcinoma adenocarcinoma carcinoma squamocellulare hcc , carcinoma epatocellulare hcc , hepatocellular carcinoma tabella 1 serie personale 1 / 70 / m 2 / 69 / m 3 / 45 / m 4 / 40 / m 5 / 60 / f 6 / 73 / f 7 / 73 / f 8 / 82 / f 9 / 81 / m 10 / 38 / f 1 / 70 / m 2 / 69 / m 3 / 45 / m 4 / 40 / m 5 / 60 / f 6 / 73 / f 7 / 73 / f 8 / 82 / f 9 / 81 / m 10 / 38 / f radiol med ( 2009 ) 114 : 608625 table 2 descriptions of lesions and procedures per patient patient procedure lesion no . 
stato eseguito il calcolo del volume per ciascuna lesione attraverso la formula 4 / 3ab2 , dove a il semiasse maggiore e b il semiasse minore plasty , three with rf combined with cementoplasty and one with microwave ablation . 
 1 con radiofrequenza plasma - mediata , 2 con radiofrequenza plasma - mediata associata a cementoplastica , 3 con radiofrequenza associata a cementoplastica , 1 con microonde . tutti hanno completato il follow - up a 12 settimane . 
 pretreatment assessment before undergoing ablation treatment , patients were evaluated by means of a validated visual analogue scale ( vas ) for pain assessment and by recording any use of analgesics . inclusion criteria were moderate or severe pain rated 4 or more on the 10 - point vas ; patients with lower scores were treated with analgesics . 
pain was localised to the site corresponding to the lesion detected by computed tomography ( ct ) ( aquilon 64 , toshiba , tokyo , japan ) or magnetic resonance valutazione prima del trattamento prima dei trattamenti ablativi i pazienti sono stati valutati usando una codificata visual analogue scale ( vas ) per la determinazione del dolore , ed stato registrato leventuale utilizzo di analgesici . 
criteri di inclusione nello studio sono stati : dolore moderato o severo con valore uguale o superiore a 4 nella scala vas di 10 punti ; i pazienti con punteggio inferiore sono stati trattati con analgesici . 
prima del trattamento , tutti i pazienti inclusi nel nostro studio 612 radiol med ( 2009 ) 114 : 608625 table 3 morphine - equivalent doses for several opioids according to route of administration tabella 3 dosi equivalenti di morfina per diversi oppioidi a seconda della via di somministrazione administration route via di somministrazione parenteral dose equivalents oral dose equivalents parenterale dose equivalenti orale dose equivalenti morphine methadone codeine buprenorphine tramadol fentanyl 10 mg 10 mg 120 mg 0.3 mg 100 mg 25 mcg / hc 30 mga 20 mg 200 mg 0.4 mgb 120 mg morfina metadone codeina buprenorfina tramadolo fentanile 10 mg 10 mg 120 mg 0 , 3 mg 100 mg 25 g / h c 30 mga 20 mg 200 mg 0 , 4 mgb 120 mg achronic use ; bsublingual ; ctransdermal auso cronico ; bsublinguale ; ctransdermica ( mr ) imaging ( 1.5 tesla avanto , siemens , munich , germany )  . 
specifically , nine patients were imaged by contrast - enhanced ct ( iopamiro , bracco , milan , italy ) and one by contrast - enhanced mr imaging ( magnevist , schering , berlin , germany )  . 
exclusion criteria were the presence of more than two symptomatic lesions and safety margins less than 1 cm from the spinal cord , major motor nerve , brain , adamkiewicz artery , bowel and bladder [ 9 ]  . before the ablation treatment , patients were on analgesic therapy ( opioids or nsaids ) , which was translated into morphine - equivalent doses to render the data homogeneous ( table 3 )  . 
analgesic use was monitored before treatment and at 1 , 4 , 8 and 12 weeks thereafter . treatment selection depending on whether the lesion is osteoblastic or osteolytic , the most beneficial ablation method , that is , the one best suited to the individual metastasis , must be selected . both rf and microwave ablation are based on the use of heat , although heat production occurs in two different manners : rf generates heat by delivering electrical current to tissues and causing ion agitation and friction ; electromagnetic microwave generates heat by agitating water molecules in tissue and producing friction [ 10 ]  . 
plasma - mediated rf ( coblation ) consists of using electrical energy to create a field of ionised particles that break the organic bonds within soft tissue ( ablation )  . 
il dolore era localizzato alla sede corrispondente alla lesione evidenziata con indagini eseguite con tomografia computerizzata ( tc ) ( aquilon 64 , toshiba , tokio , giappone ) o risonanza magnetica ( rm ) ( 1 , 5 tesla avanto , siemens , munich , germania ) ; in particolare 9 pazienti sono stati sottoposti a tc con mdc ( iopamino , bracco , milano , italia ) e 1 paziente a rm con mdc paramagnetico ( magnevist , schering , berlin , germania )  . 
criteri di esclusione al trattamento ablativo sono stati : la presenza di pi di due lesioni sintomatiche ; margini di sicurezza inferiori a 1 cm dal midollo spinale , dal nervo motorio maggiore , dallencefalo , dallarteria di adamkiewicz , dallintestino e dalla vescica [ 9 ]  . 
prima del trattamento i pazienti erano in terapia con analgesici ( oppioidi o farmaci anti - infiammatori non steroidei ) , convertiti poi , ai fini di rendere omogenei i dati , in dosi - equivalenti di morfina ( tabella 3 )  . 
tutti i pazienti assumevano dagli 80 ai 100 equivalenti di morfina . lutilizzo di analgesici stato monitorato prima della procedura , alla prima , alla quarta , allottava e alla dodicesima settimana susseguenti la stessa . selezione della tipologia di trattamento in questa fase occorre valutare , a seconda che la lesione sia osteoblastica o osteolitica , quale sia il trattamento ablativo di cui pu giovare il paziente , ovvero il pi adatto a quella specifica metastasi . 
sia lablazione con radiofrequenza che quella con microonde caratterizzata dallimpiego di calore , che avviene con due modalit differenti : la rf genera calore tramite lattrito causato dallagitazione ionica che si ha al passaggio di corrente elettrica , le microonde invece generano calore per le oscillazioni delle molecole dacqua tissutali provocate dallinterazione tra le radiazioni elettromagnetiche e le stesse molecole dacqua [ 10 ]  . 
in particolare la radiofrequenza utilizzabile solo in lesioni osteolitiche o miste , ma non pu essere usata nelle radiol med ( 2009 ) 114 : 608625 there is a need for greater precision and control during the procedure and for treating osteoblastic lesions . 
it may be performed provided that the cortical bone is intact . procedure procedures were carried out with the patient under deep sedation achieved with the cyclic administration of alfentanil ( 0.51 mg ) and midazolam ( 13 mg ) and continuous infusion of propfol ( 50120 mg )  . 
blood pressure was checked every 4 m local anaesthesia ( 1% carbocaine ) was applied to the skin at the access site . different types of imaging were used to guide the procedure : ultrasound ( iu22 , philips , best , the netherlands ) in four cases , ultrasound and fluoroscopy ( allura xper fd , philips ) in one case , ct ( aquilon 64 , toshiba , tokyo , japan ) in three cases , ct fluorography in one case and carm cone - beam ct in one case ( xper ct , allura , philips ) ( table 2 )  . 
1 ago da rf posizionato allinterno di una lesione iliaca . lesioni osteoblastiche , dato che in questo caso non avviene conduzione di calore ; non pu essere impiegata neanche se la lesione si trova in prossimit di organi come il midollo spinale ( esempio metastasi vertebrale ) per il rischio di lesioni da calore [ 11 ] ; lablazione con microonde indicata se la lesione voluminosa e non in prossimit di organi termosensibili . 
la radiofrequenza plasma - mediata ( coblazione ) consiste nellutilizzo dellenergia elettrica atta a creare un campo di particelle ionizzate che spezzano i legami organici allinterno dei tessuti molli ( ablazione )  . 
infine il trattamento combinato con cementoplastica consiste nelliniezione di cemento preceduto da un qualsiasi trattamento ablativo e si pu effettuare a patto che sia integra la corticale ossea . procedura la procedura stata eseguita in sedazione profonda con somministrazione ciclica di alfentanyl ( 0 , 51 mg ) e mydazolam ( 13 mg ) e infusione continua di propofol ( 50120 mg ) ; stata somministrata una ultra short term profilaxis ( 1 g di cefazolina )  . 
 stata effettuata anestesia locale con 1% di carbocaina nella zona cutanea di introduzione dellago . sono state impiegate differenti tipologie di imaging per la guida : in 4 casi stata impiegata guida ecografica ( iu22 , philips , best , olanda ) , in 1 caso guida ecografica e fluoroscopica ( allura xper fd , philips , best , olanda ) , in 3 casi guida tc ( aquilon 64 , toshiba , tokio , giappone ) , in 1 caso guida fluoro - tc e in 1 caso la c - arm cone - beam tc ( xper ct , allura , philips , best , olanda ) ( tabella 2 )  . 
in tutti i casi trattati con radiofrequenza stato utilizzato un ago da 17 gauge con diametro di apertura degli uncini allestremit di 4 cm ; il generatore di rf , durante il passaggio di energia , rileva limpedenza elettrica del tessuto . 
la procedura stata condotta in accordo ai protocolli forniti dalle 614 radiol med ( 2009 ) 114 : 608625 17 - gauge needle with a maximum hook - deployment diameter of 4 cthe rf generator measures electrical impedance of tissue during the passage of energy . 
plasma - mediated rf procedures ( coblation ) were performed with a cavity spinewand kit ( arthrocare corp , sunnyvale , ca , usa )  . the device was directed anteriorly through the tissue to be ablated . 
in the cases undergoing combined treatment with cementoplasty ( fig . 5a , b ) , the rf electrode was introduced through an 11 - gauge simko needle ( simko special vertebroplasty needle , optimed )  . 
after withdrawal of the rf electrode , the simko needle was connected to a system ( cement - king application system , optimed ) for the injection of cement ( osteopal v , biomet , merck )  . 
per la procedura di radiofrequenza plasma - mediata ( coblazione ) , stato usato un kit cavity spinewand ( arthrocare corp , sunnyvale , ca , usa ) ; il dispositivo stato diretto anteriormente attarverso il tessuto da ablare . 
 la fattibilit della procedura combinata con cementoplastica stata sancita dalla possibilit di effettuare un corretto posizionamento dellago allinterno della lesione , mentre il successo tecnico stato inteso come la possibilit sia di effettuare lablazione allinterfaccia tra tessuto molle e osso sia di iniettare cemento nel caso del trattamento combinato . 
2 schema che mostra la modalit di ablazione con movimento rotatorio del dispositivo di radiofrequenza plasma - mediata allinterno della lesione in direzione dei diversi orientamenti orari a ore 3 , 6 , 9 e 12 . radiol med ( 2009 ) 114 : 608625 fig . 
evidente la presenza di cemento nella lesione ablata ( freccia )  . the possibility of achieving correct needle placement inside the lesion , whereas technical success was defined as the ability to achieve ablation at the interface between soft tissue and bone and then to inject cement in the case of combined treatments . 
 risultati il successo tecnico , inteso come la possibilit di effettuare lablazione allinterfaccia tra tessuto molle e osso e di iniettare cemento nel caso del trattamento combinato , stato raggiunto nel 100% dei casi . 
la termoablazione con rf ha raggiunto in tutti i casi dimensioni di necrosi di circa 4 cm , mentre la termoablazione con microonde ha creato unarea di necrosi superiore ai 6 cm in 10 minuti . 
il tempo totale delle procedure ( intese come la sola ablazione o lablazione associata a cementoplastica ) variava da un massimo di 25 minuti a un minimo di 15 minuti . 
solamente in un paziente trattato con radiofrequenza ( 1 / 9 , 11% ) abbiamo riscontrato nei 6 giorni successivi al trattamento insorgenza di febbricola e malessere generale compatibile con la sindrome post - radiofrequenza , risoltisi poi al settimo giorno e trattati solo con acetaminofene ( paracetamolo ) [ 12 ]  . riguardo alla valutazione con scala vas , la risposta di tutti i pazienti nella valutazione del dolore prima della procedura era di 8 punti ( in una scala da 0 a 10 )  . 
attraverso una valutazione a 1 , 4 , 8 e 12 settimane , emerso che il valore medio nella scala vas stato rispettivamente di 4 , 1 la prima settimana e 2 nei radiol med ( 2009 ) 114 : 608625 table 4 results of the follow - up in terms of reduction of pain and morphine - equivalent dose . 
 pain reduction ( vas ) morphine - equivalent dose before 24 h 1 week 4 week 8 week 12 week before 1 week 4 week 8 week 12 week tabella 4 risultati nel follow - up in termini di riduzione del dolore e dose in equivalenti di morfina . 
in due casi ( pazienti n 7 e n 9 ) essa aumentata di 10 equivalenti di morfina tra lottava e la dodicesima settimana dal trattamento ( vedasi testo ) riduzione del dolore ( vas ) dose in equivalenti di morfina prima 24 h sett 1 sett 4 sett 8 sett 12 prima sett 1 sett 4 sett 8 sett 12 complications ( cement leakage )  . 
pain regression was considered statistically significant at a p value of < 0.001. the wilcoxon test for paired data was used to evaluate when this difference was already statistically significant . 
 results technical success , defined as the ability to achieve ablation at the interface between soft tissue and bone and to inject controlli a 4 , 8 e 12 settimane ( tabella 4 )  . 
rf ablation produced an area of necrosis of approximately 4 cm in all cases , whereas microwave ablation produced an area of necrosis > 6 cm in 10 mprocedure times were also shorter with the plasma - mediated rf technique ( 20 min )  . 
total procedure time ( referring to ablation alone or combined ablation and cementoplasty ) ranged regressione lineare logaritmica con p < 0 , 001 statisticamente significativa ; in particolare la differenza tra prima del trattamento e a una settimana dal trattamento significativamente aumentata ( dolore post - procedurale ) , per i motivi precedentemente esposti , mentre vi una significativa diminuzione della dose di morfina tra prima del trattamento e la quarta settimana successiva allo stesso . radiol med ( 2009 ) 114 : 608625 from 25 min to 15 m in no cases did local complications occur either during or after treatment . 
in only one case of rf ablation ( 1 / 9 , 11% ) did the patient develop low - grade fever and general malaise during the 6 days after treatment , compatible with a postradiofrequency syndrome . 
this was treated with acetaminophen only ( paracetamol ) and resolved on day 7 [ 12 ]  . with regard to vas score , all patients had a pain score of 8 ( on a scale from 0 to 10 ) before the procedure . 
after day 1 , the score decreased by 1 point in 9 / 10 patients and by 2 points in the patient treated with microwave ablation . evaluation at 1 , 4 , 8 , and 12 weeks showed that the mean vas score was 4.1 at week 1 , and 2 at 4 , 8 and 12 weeks ( table 4 )  . 
 analgesic dose increased during week 1 ( from 10 to 20 morphine equivalents ) , probably owing to postprocedural pain , but then decreased substantially after 1 month in all patients ( from 50 to 30 morphine equivalents ) ( table 4 )  . 
in two cases ( patients 7 and 9 ) , it increased by ten morphine equivalents between 8 and 12 weeks , most likely because of the appearance of a new bone metastasis at another site from the one previously treated ( table 4 )  . 
in particular , the difference between pretreatment and 1 - week posttreatment increased significantly ( postprocedural pain ) for the reasons described above , whereas there was a significant reduction in the morphineequivalent dose between pretreatment levels and week 4 after treatment . discussion several therapies are used for the palliation of bone metastases , including chemotherapy [ 13 ] , hormonal therapy [ 14 , 15 ] , surgery [ 1618 ] and radiotherapy ( local transcutaneous radiotherapy , hemibody irradiation , radionuclide therapy ) [ 3 , 19 , 20 ]  . 
a number of patients fail to benefit from these conventional treatments , however , and pain relief , when it does occur , is never achieved before 412 weeks [ 3 ]  . 
if , on the one hand , chemotherapy reduces the primary mass and secondary lesions in 20%80% of patients , on the other hand , it leads to drug resistance and recurrence of bone pain . in addition , myelodepression is common due to the toxicity of many drugs used in current treatment protocols . hormonal therapy is only effective in breast and prostate tumours , where it relieves pain from bone metastases in discussione attualmente nel trattamento palliativo delle metastasi ossee vengono utilizzate varie terapie , tra cui la chemioterapia [ 13 ] , la terapia ormonale [ 14 , 15 ] , la chirurgia [ 1618 ] e la radioterapia ( radioterapia transcutanea locale , irradiazione emicorporea , radioisotopoterapia con radionuclidi ) [ 3 , 19 , 20 ]  . 
alcuni pazienti non riescono a trarre benefici da questi trattamenti convenzionali e il sollievo dal dolore , quando si verifica , non avviene mai prima di 412 settimane [ 3 ]  . 
se da un lato la chemioterapia riduce la massa primitiva e le lesioni secondarie nel 20%80% dei pazienti , dallaltro induce farmacoresistenza e ripresa del dolore osseo ; inoltre frequente linsorgenza di mielodepressione data la tossicit di molti farmaci utilizzati negli attuali protocolli terapeutici . 
la terapia ormonale efficace solamente nei tumori della mammella e della prostata , dove tuttavia induce sollievo dal dolore delle metastasi ossee in pi del 70% dei casi [ 14 ]  . 
infine la radioterapia locale gravata nel 60% dei casi da effetti tossici ( nausea , vomito e diarrea ) e la radioisotopoterapia da una parte dimostra efficacia nei soggetti con metastasi ossee multiple , dallaltra non considerata trattamento standard per le metastasi singole . sulla base di queste considerazioni i farmaci analgesici ( oppioidi e fans ) spesso rimangono lunica alternativa nel dolore metastatico e in alcuni casi rimangono lunica alternativa per la palliazione della sintomatologia . 
 noto che gli effetti collaterali , soprattutto nei trattamenti prolungati , sono costipazione , grave limitazione dello stato fisico e mentale , nonch cirrosi e coma epatico . diversi autori hanno studiato varie strategie alternative per il trattamento del dolore da metastasi ossea che comportano lutilizzo di metodiche percutanee imagingguidate con lo scopo di ablare le lesioni focali ossee : etanolo , termoterapia interstiziale laser - indotta , ablazione con radiofrequenza ( rfa ) percutanea e , pi recentemente , crioablazione [ 2 , 4 , 11 ]  . 
la nostra esperienza si riferisce alla risposta di 10 pazienti al trattamento della sintomatologia dolorosa con diverse tecniche di radiologia interventistica che includono tecniche ablative ( termoablazione con rf , termoablazione con radiofrequenza plasma - mediata , termoablazione con microonde ) associate o meno alla 620 radiol med ( 2009 ) 114 : 608625 > 70% of cases [ 14 ]  . 
finally , local radiotherapy produces toxic effects ( nausea , vomiting and diarrhoea ) in 60% of cases , and radionuclide therapy is effective in patients with multiple bone metastases but is not considered standard treatment for a single metastasis . on the basis of these considerations , analgesics ( opioids and nsaids ) are often the only option for metastatic pain , and in some cases for palliation of symptoms . 
the world health organization ( who ) [ 21 ] recommends a three - step approach : ( 1 ) initial treatment with nsaids such as aspirin , ibuprofen , naproxen , ( 2 ) if pain persists , use of mild opioids such as codeine and hydrocodone , ( 3 ) for persisting moderate or severe pain , high doses of opioids such as morphine , hydromorphone , or fentanyl as an intermittent or continuous infusion . 
known side - effects , above all in long - term treatments , are constipation , severe physical and mental impairment , cirrhosis and hepatic coma . several authors have investigated alternative approaches to painful bone metastases , all of which involve using percutaneous image - guided methods to ablate focal bone lesions : ethanol , laser interstitial thermal therapy , percutaneous rf ablation and , more recently , cryoablation [ 2 , 4 , 11 ]  . 
this study reports on the response of ten patients treated with different interventional radiology techniques , namely , ablation techniques ( rf ablation , plasma - mediated rf ablation , microwave ablation ) used alone or in combination with cementoplasty . 
in agreement with the literature [ 11 ] , we treated patients with up to two bone metastases ( lytic or mixed , but not osteoblastic ) causing acute disabling pain . pain was poorly controlled with conventional treatments . ablation techniques are successful in relieving pain only if the needle is placed at the interface between soft tissue and bone . 
the advantage of rf ablation lies in the use of electrodes that have a smaller diameter compared with the microwave antennas , an aspect that should theoretically reduce complications related to electrode deployment . 
microwave treatment has the advantage of shorter procedure times and the ability to ablate larger lesions than those usually treated with rf , thanks to the possibility of placing two antennas simultaneously indeed , in one of our patients , its use was cementoplastica . 
in accordo con le indicazioni della letteratura [ 11 ] , sono stati trattati pazienti che non avessero pi di due metastasi ossee , che queste fossero litiche o miste , ma non blastiche , e che , soprattutto , fossero causa di dolore acuto e invalidante . 
in questi pazienti , il followup non si ferma solo al dato di diagnostica per immagini , ma si concentra sulla efficacia clinica del trattamento , ossia sulla riduzione del dolore . in questo studio sono state trattate tre lesioni solo con radiofrequenza e una solo con microonde . 
gli svantaggi invece rispetto allimpiego di microonde sono dati da tempi lunghi di procedura ( circa 30 minuti ) e dalla necessit di effettuare pi posizionamenti in caso di ampio volume da ablare . 
il trattamento con microonde ha invece il vantaggio di giovare di una procedura pi breve e di poter ablare lesioni di dimensioni maggiori rispetto a quelle usualmente trattate con radiofrequenza , ci per la possibilit di posizionare due antenne contemporaneamente . 
infatti , in una nostra paziente , lampia superficie di contatto softtissue - osso ha giustificato il suo utilizzo : lablazione ha garantito in un tempo inferiore rispetto alla rf un volume di necrosi superiore . 
inoltre , dal punto di vista della qualit dellablazione , studi sperimentali e clinici [ 10 , 22 , 23 ] hanno evidenziato che il trattamento con microonde garantisce il raggiungimento di temperature intra - lesionali pi elevate , una minore dispersione di calore e quindi unefficacia superiore rispetto alla termoablazione con rf nelle lesioni in prossimit dei vasi sanguigni . 
infine con la metodica delle microonde la diminuzione del dolore stata pi sensibile ( 2 punti bpi ) dopo 24 ore dal trattamento rispetto alle altre metodiche utilizzate ( 1 punto bpi ) , per poi allinearsi con i dati ottenuti dalle altre tecniche nelle fasi successive . 
 le metodiche di termoablazione con radiofrequenza e con microonde hanno comunque linconveniente di non poter essere utilizzate nelle metastasi osteoddensanti , dato che il tessuto osseo non favorisce la conduzione di calore ( radiofrequenza ) n lagitazione di molecole dacqua ( microonde )  . nelle metastasi osteoddensanti possibile utilizzare la crioablazione che ha per lo svantaggio di impiegare aghi di grosse dimensioni e di avere tempi lunghi di procedura [ 2 ]  . inoltre sia la radiofrequenza che le microonde possono provocare lesioni termiche ad organi adiacenti . 
per ovviare radiol med ( 2009 ) 114 : 608625 justified by the extensive contact area between soft tissue and bone , and the ablation procedure produced a larger necrosis volume in a shorter time compared with rf . 
in addition , from the viewpoint of the quality of ablation , experimental and clinical studies [ 10 , 22 , 23 ] have shown that microwave treatment provides higher intralesional temperatures and less heat dispersion and consequently better effectiveness compared with rf ablation in lesions located in proximity to blood vessels . 
finally , microwave ablation provided greater pain relief [ 2 points on the brief pain inventory ( bpi ) ] than did the other methods ( 1 point bpi ) 24 h after treatment before becoming aligned with the other methods at subsequent follow - up assessments . 
 rf and microwave ablation methods both suffer the same limitation of not being applicable to osteoblastic lesions , as bone tissue does not allow the conduction of heat ( radiofrequency ) or the agitation of water molecules ( microwaves )  . 
to avoid this complication , several possibilities exist : to create an air ( in microwave ) interface or water ( in rf ablation ) interface to limit the ablation area ; to place thermocouples close to the structures at risk of thermal injury , as these can guide the operator in continuing or discontinuing the procedure by providing feedback on temperature ; to use bipolar rf , which through an electrode thermally shielded by another opposing electrode ensures well - delimited ablations [ 24 ] ; to use plasma - mediated rf ablation [ 25 ]  . a distinctive feature of plasma - mediated rf ablation ( coblation ) is the ability to release , in an extremely precise manner , a minimal amount of heat ( unlike conventional electrosurgery ) , a crucial factor in treating vertebral lesions . the low rf energy ( 100 khz ) is thus used to excite the electrolytes in a conductive medium ( plasma ) , such as saline solution or the aqueous intracellular environment , creating an area of highly ionised particles immediately adjacent to the electrode tip . 
this molecular dissociation process converts the ablated tissue into gas , creating a cavity at the treatment site [ 25 ] , which accounts for its suitability for osteolytic lesions . coblation in this study was used for a metastasis to a rib in a patient who had undergone right liver resection for hepatocarcinoma and had shown , on preprocedural ct , a bowel loop adjacent to the inner aspect of the affected rib . coblation was used to avoid damaging the bowel wall , and indeed , it allowed for extreme precision in delimiting the ablation margins . with regard to our results , in all cases pain , reduction a tale complicanza , si hanno diverse possibilit : creare uninterfaccia o con aria ( nelle microonde ) o con acqua ( nellablazione con rf ) per limitare il territorio di ablazione . 
possibile inoltre posizionare termocoppie a ridosso delle strutture a rischio di danno termico , che misurando la temperatura durante la procedura , sono utili alloperatore nel decidere se interrompere o meno lablazione ; utilizzare la radiofrequenza bipolare , che attraverso un elettrodo schermato termicamente da un secondo elettrodo opposto al primo , garantisce ablazioni ben definite [ 24 ] ; utilizzare la radiofrequenza plasma - mediata [ 25 ]  . nella tecnica di termoablazione con radiofrequenza plasma - mediata ( coblazione ) caratteristica identificativa la capacit di cedere , in maniera molto precisa , una quantit minima di calore ( contrariamente allelettrochirurgia convenzionale ) , fattore importante per esempio nel trattamento di lesioni vertebrali . 
la bassa energia di radiofrequenza ( 100 khz ) viene quindi utilizza per eccitare gli elettroliti in un mezzo conduttivo ( plasma ) , come una soluzione fisiologica o lambiente acquoso intracellulare , in modo da formare unarea di particelle altamente ionizzate nellarea immediatamente adiacente alla punta del dispositivo . 
questo processo di dissociazione molecolare converte il tessuto ablato in gas e in questo modo si viene a creare una cavit nella zona del trattamento [ 25 ] , trovando dunque particolare indicazione nelle lesioni osteolitiche . la coblazione stata utilizzata in questo studio per la lesione costale di un paziente che , in seguito ad epatectomia destra per exeresi di una neoplasia epatica , evidenziava allesame tc , eseguito prima del trattamento , unansa intestinale adiacente alla faccia interna della costa interessata dalla lesione . 
per evitare di danneggiare la parete dellansa , stata impiegata la coblazione che , in effetti , ha dimostrato notevole precisione nella definizione dei limiti dellablazione e ne ha quindi giustificato limpiego . in merito ai risultati , in tutti i casi abbiamo ottenuto un decremento del dolore tale da dimezzare , allottava settimana dal trattamento , la dose di equivalenti di morfina necessari per controllare il dolore . 
qualunque sia la tecnica ablativa utilizzata , il meccanismo di riduzione del dolore non ancora chiaro , ma vi sono alcune ipotesi : distruzione delle fibre sensoriali del periostio e della corticale ; decompressione meccanica del volume tumorale ; distruzione delle cellule tumorali che producono citochine come tnf ( fattore di necrosi tumorale alfa ) e interleuchine che promuovono la trasmissione del dolore ; inibizione dellattivit degli osteoclasti [ 26 , 27 ]  . 
regardless of the ablation technique used , the mechanism by which pain is reduced is not understood , although several hypotheses have been proposed : destruction of the periosteal and cortical sensory nerve fibres , mechanical decompression of the tumour volume , destruction of tumours cells that produce cytokines such as tumour necrosis factor alfa ( tnf - ) and interleukins that promote pain transmission , and inhibition of osteoclast activity [ 26 , 27 ]  . 
 [ 28 ] , in a study of 12 patients , demonstrated that rf is a safe and effective treatment that improves quality of life and reduces analgesic use in patients with bone metastases . 
 [ 29 ] reported major complications in three patients : one second - degree burn at the grounding - pad site , one case of transient bladder and bowel incontinence and one case of fracture of the acetabulum 6 weeks after rf treatment of an acetabular lesion . 
studies of coblation on bone lesions [ 25 ] investigated the use of rf ablation to treat vertebral lesions only ( for which no complications were reported ) , so we are unable to compare the results with our experience , as we used rf treatment in a costal lesion . 
 [ 9 ] presented the first experimental and clinical results of the use of microwave ablation in bone metastases , reporting excellent technical results in terms of volume of necrosis , speed of the procedure and absence of complications . 
 [ 29 ] , there may be a new rise in morphine - dose requirements long after treatment , indicative of the development of pain at other sites of metastases . 
 [ 28 ] , studiando 12 pazienti , hanno dimostrato la sicurezza e lefficacia della rf per la riduzione del dolore , il miglioramento della qualit della vita e la riduzione delluso di analgesici nei pazienti con metastasi che coinvolgevano losso . 
 [ 29 ] che ha considerato 43 pazienti , stato segnalato un incremento della dose di oppiodi al primo giorno dal trattamento e un successivo decremento di pi del 50% . sulla base di unattenta selezione dei pazienti , nella nostra casistica non si sono verificate complicanze probabilmente anche per lesiguo numero di pazienti ( 6 ) trattati con rf . 
 [ 29 ] si sono invece verificate complicanze maggiori in 3 pazienti : uno ha subito unustione di secondo grado nellarea cutanea della messa a terra , un altro ha accusato incontinenza vescicale e intestinale e infine in un paziente si verificata una frattura acetabolare della zona trattata a 6 settimane dal trattamento con rf . 
gli studi effettuati con la coblazione su lesioni ossee [ 25 ] hanno preso in esame solo il trattamento di lesioni vertebrali ( per le quali per altro non sono riportate complicanze ) e quindi non possibile fare un confronto dato che nel nostro studio la metodica stata utilizzata in una lesione costale . 
 [ 9 ] hanno redatto i primi studi sperimentali e clinici sullutilizzo della termoablazione con microonde nelle metastasi ossee , riportando un ottimo risultato tecnico sia in termini di volume di necrosi , sia di rapidit della procedura , sia di assenza complicanze . 
 [ 29 ] , possibile che vi sia , a distanza dalla procedura , un nuovo aumento della dose di morfina , compatibile con linsorgenza di nuove localizzazioni ossee in siti diversi da quello trattato . 
 [ 6 ] , pazienti sottoposti a rfa associata a cementoplastica per voluminose metastasi ossee coinvolgenti anche la regione extra - ossea hanno ottenuto una riduzione della dose di analgesici solo nel 41% dei casi ; le voluminose dimensioni delle lesioni trattate giustificano il divario tra questo risultato e quello ottenuto dallo studio di callstrom et al . 
 [ 28 ] ( trattamento solo con rf )  . nel nostro studio sono state trattate con cementoplastica le lesioni che , in relazione alla sede , necessitavano di una stabilizzazione . 
in all cases , in agreement with the literature , the results achieved were excellent , not only as concerns stabilisation and thus prevention of pathological fractures , but also as concerns pain relief , achieved in 100% of cases . 
 [ 6 ] emphasised that the technique is easy to perform , inexpensive and minimally invasive , even though the effects of combining rf ablation and cementoplasty with radiotherapy are not well known . 
 [ 34 ] believe that the coagulation necrosis induced by rf facilitates even cement distribution within the ablated lesion and that cementoplasty enhances the analgesic effect by stabilising the bone . 
 the results obtained have been excellent , with pain relief being achieved in 100% of cases , both in case reports [ 30 , 31 , 34 ] and in larger series [ 6 , 28 , 32 , 33 ] , as well as in our small patient series . 
it should be emphasised that , whereas studies performed with rf or cementoplasty alone achieved 100% technical success and 80%100% pain relief [ 35 , 36 ] , combined rf and cementoplasty ensured pain relief in all cases but a slightly lower rate of technical success . conclusions there is no agreement as to the best treatment for bone metastases . 
it is clear that the rationale for the use of these treatments is that , when indicated , they ensure considerably faster pain relief compared with conventional treatments , providing a substantial improvement in quality of life in a short time . 
however , further investigations on larger patient populations , as well as randomised controlled studies , are required to validate the effectiveness of these treatments . con cementoplastica dopo rfa e 2 con vertebroplastica dopo radiofrequenza plasma - mediata . 
in tutti i casi , in accordo con i dati della letteratura , sono stati ottenuti ottimi risultati non solo nellambito della stabilizzazione e quindi nella prevenzione della possibile frattura patologica , ma soprattutto in quello della riduzione della sintomatologia dolorosa , che si avuta nel 100% dei casi . 
 [ 34 ] ritengono che la necrosi coagulativa indotta dalla rf faciliti lomogenea distribuzione del cemento allinterno della lesione ablata e che la cementoplastica , per effetto della stabilizzazione ossea , migliori leffetto antalgico . 
 i risultati ottenuti sono stati ottimi , sia nei case report [ 30 , 31 , 34 ] che nelle casistiche [ 6 , 28 , 32 , 33 ] dove la riduzione del dolore si verificata nel 100% dei casi analogamente a quanto emerso nellesperienza personale , peraltro numericamente esigua . 
va sottolineato che , se da un lato negli studi effettuati solo con radiofrequenza o solo con cementoplastica si ottenuto un successo tecnico del 100% a fronte di un risultato in termini di riduzione del dolore compreso tra l80% e il 100% [ 35 , 36 ] , dallaltro la tecnica combinata di radiofrequenza e cementoplastica ha assicurato la riduzione del dolore in tutti i casi trattati , ma un successo tecnico in una percentuale leggermente inferiore . conclusioni attualmente non esistono ancora pareri concordi sulla metodica migliore nel trattamento delle metastasi ossee . 
appare evidente che ci che giustifica il ricorso a queste terapie il fatto che , laddove vi sia lindicazione , esse garantiscono una riduzione della sintomatologia dolorosa notevolmente pi rapida rispetto alle terapie convenzionali apportando , in breve tempo , un sensibile miglioramento della qualit della vita . 
midiri3 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria di parma , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dibimel , sezione di scienze radiologiche , universit di palermo , palermo , italy 4dipartimento di ostetricia e ginecologia e scienze radiologiche delluniversit di catania , catania , italy 5dipartimento di radiologia , universit degli studi di trieste , trieste , italy 6dipartimento di radiologia , universit degli studi di verona , verona , italy correspondence to : f . 
cademartiri , dipartimento di radiologia , c / o piastra tecnica piano 0 , azienda ospedaliero - universitaria di parma , via gramsci 14 , parma , italy , tel . : + 39 - 0521 - 703516 / 3756 , fax : + 39 - 0521 - 703630 , e - mail : filippocademartiri@hotmail.com received : 11 february 2008 / accepted : 15 september 2008 / published online : 15 april 2009 springer - verlag 2009 abstract purpose . 
msct - ca was performed in 43 patients ( 31 men , 12 women , mean age 58.87.7 years ) with stable angina after a routine diagnostic workup involving stress ecg and conventional ca . 
lac - tcms stata eseguita in 43 pazienti ( 31 uomini , 12 donne , et media 58 , 87 , 7 anni ) con angina stabile sottoposti ad iter diagnostico comprendente la prova da sforzo con ecg e langiografia coronarica convenzionale . 
lac - tcms ha migliorato la probabilit post - test di una rilevante ca dal 50% fino all86% dopo una prova da sforzo negativa , e 514 radiol med ( 2009 ) 114 : 513523 conclusions . 
lac - tcms uno strumento non invasivo potenzialmente utile nelliter diagnostico dei pazienti con angina stabile in grado di rendere nota od escludere una significativa ca . parole chiave imaging coronaropatia aterosclerotica tomografia computerizzata angiografia coronarica prova da sforzo introduction introduzione stress testing has shown to be of prognostic value in patients with stable angina , as it is useful for selecting patients to be studied with coronary angiography ( ca ) and consequently orienting subsequent revascularisation strategies . 
current guidelines recommend stress testing in the diagnostic workup of patients with stable angina , and exercise electrocardiography ( ecg ) is the first test most patients undergo [ 14 ]  . 
however , the usefulness of msct - ca as an alternative or an adjunct to stress testing in the diagnostic workup of patients with stable angina in clinical practice has not been established . this study aimed to assess the diagnostic value of stress testing and msct - ca , both jointly and independently , in identifying or excluding significant coronary artery disease ( cad ) in a consecutive cohort of patients with stable angina . materials and methods population we evaluated 43 patients ( 31 men , 12 women , mean age 58.87.7 years ) selected according to the following inclusion criteria : stable angina , sinus rhythm and ability to hold breath for at least 12 s ( table 1 )  . 
exclusion criteria were a history of allergic reactions , serum creatinine > 120 mol / l , thyroid disease , ecg abnormalities at rest ( st - segment depression 1 mm at rest , left bundle branch block ) precluding reliable evaluation and inability to perform msct - ca before conventional coronary angiography ( cca ) owing to logistic reasons . 
the study was approved by our institutions ethics committee , and all patients gave their informed consent . la prova da sforzo si dimostrata di valore prognostico nei pazienti con angina stabile poich utile nella selezione dei pazienti da indirizzare verso la coronarografia e conseguentemente in grado di guidare le successive strategie di rivascolarizzazione . 
le attuali linee - guida raccomandano la prova da sforzo nelliter diagnostico dei pazienti con angina stabile ; il test ergometrico con ecg il primo esame effettuato nella maggior parte dei pazienti [ 14 ]  . 
langiografia coronarica mediante tomografia computerizzata multistrato ( ac - tcms ) una tecnica non invasiva che pu valutare con efficacia le stenosi coronariche significative in popolazioni selezionate di pazienti [ 514 ]  . 
tuttavia non ancora noto il valore dellactcms in alternativa o come aggiunta alla prova da sforzo nelliter diagnostico dei pazienti con angina stabile nella routine clinica . con questo studio intendiamo stabilire il valore diagnostico della prova da sforzo e dellac - tcms , insieme ed indipendentemente , in una coorte consecutiva di pazienti con angina stabile , allo scopo di rivelare o escludere una significativa coronaropatia aterosclerotica ( ca )  . materiali e metodi popolazione sono stati valutati 43 pazienti ( 31 uomini , 12 donne , et media 58 , 87 , 7 anni ) nel rispetto dei seguenti criteri dinclusione : angina stabile , ritmo cardiaco sinusale e capacit di mantenere lapnea inspiratoria per almeno 12 secondi ( tabella 1 )  . 
altri criteri di esclusione erano : diatesi allergica , creatinina sierica > 120 mol / l , tireopatie , anomalie ecg a riposo ( sotto - slivellamento 1 mm del tratto st a riposo , blocco di branca sinistro ) precludenti unaffidabile interpretazione , ed impossibilit di eseguire unac - tcms prima dellangiografia coronarica radiol med ( 2009 ) 114 : 513523 table 1 patient characteristics tabella 1 caratteristiche dei pazienti risk factors ( % ) number of patients ( % ) fattori di rischio ( % ) numero pazienti ( % ) hypercholesterolaemia systemic hypertension smoking family history of early onset cad obesity ( bmi 30 ) diabetes mellitus treatment aspirin - blockers ace inhibitors / at - 2 antagonists calcium antagonists nitrates ( systemic ) statins 30 ( 70 ) 29 ( 67 ) 18 ( 42 ) 16 ( 37 ) 11 ( 26 ) 6 ( 14 ) 41 ( 95 ) 36 ( 84 ) 14 ( 33 ) 14 ( 33 ) 13 ( 30 ) 30 ( 70 ) ipercolesterolemia ipertensione sistemica fumo storia familiare di ca precoce obesit ( bmi30 ) diabete mellito trattamento aspirina - bloccanti ace inibitori / at - ii antagonisti calcio - antagonisti nitrati ( per via sistemica ) statine 30 ( 70 ) 29 ( 67 ) 18 ( 42 ) 16 ( 37 ) 11 ( 26 ) 6 ( 14 ) 41 ( 95 ) 36 ( 84 ) 14 ( 33 ) 14 ( 33 ) 13 ( 30 ) 30 ( 70 ) cad , coronary artery disease ; bmi , body mass index ca , coronopatia aterosclerotica ; bmi , body mass index patient preparation patients with sinus rhythm > 70 beats per minute ( bpm ) received 100 mg of metoprolol orally 45 min before the scan unless contraindicated ( severe heart failure or chronic obstructive pulmonary disease )  . scanning parameters , reconstruction and image analysis all patients underwent msct ( sensation 64 , siemens , forchheim , germany ) according to a previously described protocol [ 15 ]  . 
only coronary branches 2 mm in diameter were considered clinically relevant , as smaller ones are not amenable to percutaneous or surgical revascularisation . conventional coronary angiography all ct scans were performed within 4 weeks from cca . 
a single observer blinded to the msct - ca findings determined the diameter of all coronary branches using a quantitative technique ( caas , pie medical , maastricht , the netherlands )  . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito consenso informato scritto . preparazione dei pazienti i pazienti con un ritmo superiore ai 70 bpm hanno ricevuto per os una dose di 100 mg di metoprololo 45 min prima della scansione , a meno di eventuali controindicazioni ( grave scompenso cardiaco o broncopatia cronica ostruttiva )  . parametri di scansione , ricostruzione e analisi delle immagini tutti i pazienti sono stati sottoposti a tc multistrato ( sensation 64 , siemens , forchheim , germania ) secondo protocollo gi descritto [ 15 ]  . 
tutti i rami coronarici 2 mm sono stati indipendentemente analizzati mediante le convenzionali tecniche di post processing da due osservatori , non a conoscenza dei risultati dellacc ( vedi metodologia e postprocessing gi descritti [ 15 ] )  . 
sono stati valutati solo i rami coronarici di diametro superiore a 2 mm in quanto clinicamente rilevanti , ossia gli unici passibili di eventuale rivascolarizzazione percutanea o chirurgica . angiografia coronarica convenzionale tutte le scansioni tc sono state eseguite entro 4 settimane dallacc . 
un solo osservatore , alloscuro dei risultati 516 exercise stress testing the protocol for the bicycle exercise test involved an initial workload of 25 w followed by a 25 - w increment every 2 mheart rhythm and blood pressure were recorded at rest and at the end of each phase of the test . 
the results of the stress test were classified as positive when the st segment appeared horizontal or had a depression 1 mm for at least 6080 ms after the end of the qrs complex [ 3 ]  . 
cca revealed no significant stenoses in 26% ( 11 / 43 ) , singlevessel disease in 32% ( 14 / 43 ) and multivessel disease in 42% ( 18 / 43 ) of patients . 
in the remaining 37 patients , stress testing to identify significant cad had 79% sensitivity ( 95% ci 6292 ) , 67% specificity ( 95% ci 3490 ) , 88% positive predictive value ( 95% ci 7393 ) and 50% negative predictive value ( 95% ci 2272 )  . only one msct - ca was considered inconclusive as a result of motion artefacts related to high heart rate ( 84 bpm )  . in 42 patients , msct - ca to identify significant cad showed 100% sensitivity ( 95% ci 91100 ) , 90% specificity ( 95% ci 6199 ) , 97% positive predictive value ( 95% ci 8799 ) and 100% negative predictive value ( 95% ci 71100 )  . 
la ca stata ritenuta rilevante quando era presente almeno una stenosi significativa . prova da sforzo il protocollo del ciclo ergometro ha utilizzato un carico iniziale di 25 w , seguito da un incremento di 25 w ogni 2 minuti . 
il ritmo cardiaco e la pressione arteriosa sono stati registrati a riposo e alla fine di ogni fase del test da sforzo . un ecg a 12 derivazioni stato acquisito ogni minuto ; un ecg di monitoraggio del ritmo cardiaco a 3 derivate stato acquisito continuativamente . 
i risultati della prova da sforzo sono stati classificati come positivi quando il tratto st appariva orizzontale o sotto - slivellato 1 mm per almeno 6080 ms dopo la fine del complesso qrs [ 3 ]  . le prove da sforzo negative dei pazienti che non avevano raggiunto gli standard di riferimento stabiliti per et , sesso e peso sono state invece classificate come non conclusive . analisi statistica per valutare il valore diagnostico della prova da sforzo e dellac - tcms allo scopo di individuare o escludere i pazienti con una rilevante ca sono stati calcolati i seguenti parametri : sensibilit , specificit , valore predittivo positivo , valore predittivo negativo , rapporto di verosimiglianza positivo ( sensibilit / [ 1 - specificit ] ) e rapporto di verosimiglianza negativo ( [ 1 - sensibilit ] / specificit ] )  . risultati il 51% ( 22 / 43 ) dei pazienti ha ricevuto b - bloccanti prima della scansione ( frequenza cardiaca media 59 , 38 , 3 bpm )  . lacc ha rivelato lassenza di stenosi significative nel 26% ( 11 / 43 ) , malattia mono - vasale nel 32% ( 14 / 43 ) , e malattia multi - vasale nel 42% ( 18 / 43 ) dei pazienti . 
pertanto , la probabilit pre - test di una ca significativa era del 74% . valore diagnostico del test da sforzo e dellac - tcms sei prove da sforzo sono state classificate come non conclusive . 
patients without significant cad were correctly identified at msct - ca in nine out of 11 cases owing to the presence of one false positive and of one inconclusive scan . diagnostic value of msct - ca in addition to stress testing msct - ca performed after the exercise stress test considerably improved posttest probability . 
in 42 pazienti lac - tcms volta allidentificazione di una ca significativa ha evidenziato : sensibilit 100% ( 95% ic : 91100 ) , specificit 90% ( 95% ic : 6199 ) , valore predittivo positivo 97% ( 95% ic : 8799 ) e valore predittivo negativo 100% ( 95% ic : 71100 )  . 
i pazienti senza ca significativa sono stati correttamente identificati dallac - tcms in 9 degli 11 casi per la presenza di un falso positivo e di una scansione non conclusiva . valore diagnostico dellac - tcms addizionale alla prova da sforzo limpiego dellac - tcms eseguita dopo la prova da sforzo ha prodotto degli apprezzabili miglioramenti nella probabilit post - test . 
limmagine mip mostra una stenosi significativa a livello dellacd prossimale ( testa di freccia ) , confermata dallangiografia coronarica convenzionale ( acc )  . with major cardiovascular risk factors , should undergo stress testing [ 16 , 17 ]  . 
some noninvasive tests have the advantage of providing additional information on ventricular dysfunction , blood pressure and heart rate response to stress , as well as on the degree of ischaemia . 
the choice of the most appropriate noninvasive diagnostic test in patients with known or suspected cad must take into account the patients ability to exercise , the presence of ecg abnormalities at rest and the sensitivity , specificity and costs of the technique . in clinical practice , patients with a positive stress test are subsequently studied with cca to direct patients to coronary angioplasty , surgical bypass or pharmacological treatment . 
conversely , patients with typical chest pain and negative stress test require further noninvasive diagnostic investigations in the context of a periodic clinical follow - up in a day - hospital setting , according to the level of clinical suspicion of cad based on case history , physical examination and ecg at rest . 
in a proportion of cases , when symptoms persist or worsen without other causes accounting for this , cca becomes necessary . recent guidelines / recommendations and publications consider appropriate the use of msct - ca in intermediaterisk patients [ 1922 ]  . 
tutti i pazienti con dolore toracico tipico o atipico , specialmente in presenza dei fattori maggiori di rischio cardiovascolare , dovrebbero essere sottoposti alla prova da sforzo [ 16 , 17 ]  . 
i test non invasivi potrebbero , peraltro , rendere pi accurata la valutazione dei pazienti asintomatici a rischio intermedio [ 18 ]  . tuttavia , lacc spesso necessaria per dirimere la diagnosi quando il test da sforzo non conclusivo . 
alcuni test non invasivi hanno inoltre il vantaggio di fornire informazioni addizionali sulla disfunzione ventricolare , sulla risposta della pressione arteriosa e della frequenza allo stress e sul grado di ischemia . 
la scelta del pi appropriato test diagnostico non invasivo nei pazienti con ca nota o sospetta deve tenere conto della capacit di sostenere uno sforzo fisico , della presenza di anomalie elettrocardiografiche a riposo , della sensibilit , della specificit e dei costi . 
 radiol med ( 2009 ) 114 : 513523 nella routine clinica i pazienti con prova da sforzo positiva sono ulteriormente valutati mediante acc per indirizzare il paziente allangioplastica coronarica , al bypass chirurgico , o al trattamento farmacologico . 
i pazienti con dolore toracico tipico e prova da sforzo negativa , invece , richiedono ulteriori test diagnostici non invasivi nel contesto di un periodico follow - up clinico in regime di day hospital , secondo il livello di sospetto clinico di ca basato sullanamnesi , sullesame obiettivo , e sullecg a riposo . 
in un certo numero di casi , quando la sintomatologia permane o peggiora senza che altre cause possano giustificarla diventa necessaria lesecuzione dellacc . recenti linee guida / raccomandazioni e pubblicazioni riportano come appropriata lapplicazione della ac - tcms in pazienti con rischio intermedio [ 1922 ]  . 
in questa classe di pazienti la distribuzione pressoch dicotomica della malattia rende opportuno un test caratterizzato da alta sensibilit ed ancor pi con elevato valore predittivo negativo . nel nostro studio abbiamo valutato il valore diagnostico della prova da sforzo e dellac - tcms indipendentemente , e in particolare il valore addizionale dellac - tcms dopo prova da sforzo in 43 pazienti consecutivi con angina stabile e una probabilit pre - test medio - alta ( 74% ) di ca significativa . 
i nostri risultati mostrano che la prova da sforzo rivela correttamente la presenza o lassenza di una ca significativa nel 65% ( 28 / 43 ) dei pazienti , mentre lactcms valuta correttamente tutti i pazienti con ca significativa ( 32 )  . 
lac - tcms ha evidenziato valori di sensibilit ( 100% ) , specificit ( 90% ) , valore predittivo positivo ( 97% ) e valore predittivo negativo ( 100% ) in linea con quelli di altri lavori presenti in letteratura [ 7 , 11 , 13 , 14 ]  . 
 [ 10 ] che riporta un valore predittivo negativo moderato ( 75% ) nella valutazione per paziente , tale da suggerire un limitato impatto diagnostico dellac - tcms nelliter diagnostico delle popolazioni ad alto rischio . 
 lac - tcms risulta particolarmente efficace nel migliorare la probabilit post - test di significativa ca dopo prova da sforzo negativa del 50% , un valore che implica unincertezza diagnostica tale da giustificare il proseguimento delliter diagnostico , fino all86% nel caso di ac - tcms positiva e fino allo 0% nel caso di ac - tcms negativa . 
pertanto , le informazioni aggiuntive fornite dallac - tcms hanno la capacit di influenzare il successivo management dei pazienti con angina stabile , ma con test da sforzo negativo ovvero con probabilit pre - test intermedia . nei pazienti con angina stabile e test da sforzo positivo , ovvero ad alta probabilit di significativa ca , lac - tcms risultata capace di migliorare ulteriormente la probabilit post - test fino al 100% nel caso di ac - tcms positiva e fino fig . 
le immagini mip e cmpr indicano la presenza di una stenosi significativa a livello dellarteria circonflessa prossimale , che stata confermata dallangiografia coronarica convenzionale ( acc )  . particular , the additional value of msct - ca after the stress test in 43 consecutive patients with stable angina and a medium - to - high ( 74% ) pretest probability of significant cad . 
our results showed that the stress test correctly identified the presence or absence of significant cad in 65% ( 28 / 43 ) of patients , whereas msct - ca correctly identified all patients with significant cad ( 32 )  . 
msct - ca had sensitivity ( 100% ) , specificity ( 90% ) , positive predictive ( 97% ) and negative predictive ( 100% ) values in line with those reported by previous studies [ 7 , 11 , 13 , 14 ]  . 
conflicts with these data , as they found a moderate negative predictive value ( 75% ) in the evaluation per patient , suggesting a limited diagnostic impact of msct - ca on the diagnostic workup of high - risk patient populations [ 10 ]  . 520 radiol med ( 2009 ) 114 : 513523 msct - ca was particularly effective in improving the posttest probability of significant cad after a negative stress test by 50% , a value that implies a diagnostic uncertainty that calls for further investigation , reaching 86% in the case of positive msct - ca and 0% in the case of negative msct - ca . 
hence , the additional information provided by msct - ca is able to influence the management of patients with stable angina but only in the case of a negative stress test , i.e. 
the current guidelines on stable angina recommend that patients with a high pretest probability should undergo noninvasive investigations followed by diagnostic cca to direct them to the most appropriate treatment . 
however , a targeted approach whereby diagnostic cca is performed in anticipation of an interventional procedure presents several disadvantages compared with a step - wise approach that allows the necessary time to inform the patient about the risks , benefits and therapeutic alternatives while permitting optimal hydration and pretreatment with oral antiaggregants prior performing angioplasty [ 4 ]  . the proposal to introduce msct - ca in the diagnostic algorithm of patients with typical chest pain raises some important questions . 
the cost of performing msct - ca may only be estimated in that it has not yet been assigned a procedure code in the national italian tariff nomenclator identifying it as a specialist service . 
this percentage can be reasonably expected to increase when the population is at high cardiovascular risk and decrease with a decreasing prevalence of the disease ( bayes theorem )  . 
furthermore , when symptoms persist in patients with a negative exercise test , further diagnostic investigations are normally used , such as myocardial perfusional scintigraphy or stress allo 0% nel caso di ac - tcms negativa . 
le attuali lineeguida dellangina stabile suggeriscono che i pazienti con alta probabilit pre - test dovrebbero essere sottoposti ad esami non invasivi e in seguito ad acc diagnostica per indirizzare questi pazienti verso il pi appropriato trattamento . 
un approccio mirato verso lacc diagnostica in previsione di una procedura interventistica presenta tuttavia diversi svantaggi , se confrontato ad un approccio a stadi , che garantisce il tempo necessario ad informare il paziente dei rischi , dei benefici e delle alternative terapeutiche e parimenti consente unidratazione ottimale e il pretrattamento con anti - aggreganti orali prima dellangioplastica [ 4 ]  . 
inoltre , tale sproporzione potrebbe aumentare se come atteso ci sar un necessario adeguamento del rimborso della ac - tcms . tuttavia , come dimostrato dal presente studio , il test ergometrico non ha unelevata predittivit specialmente quando negativo . 
questo determina un ritardo diagnostico in una significativa percentuale di pazienti ad alto rischio . ragionevole attendersi che tale percentuale aumenti quando la popolazione sia ad un rischio cardiovascolare decrescente per la minore prevalenza di malattia ( teorema di bayes )  . 
inoltre , quando tali pazienti con test ergometrico negativo continuano a lamentare sintomi , di regola passano ad ulteriori stadi diagnostici che possono essere costituiti dalla scintigrafia miocardica perfusionale o dallecocardiografia da stress . 
these two techniques , despite a higher diagnostic accuracy than exercise testing , nonetheless have sensitivity and specificity values no higher than 90% . it should be remembered that the correct performance of a stress test remains a basic requirement of clinical medicine . 
furthermore , pharmacological treatment with drugs such as digitalis , nitroderivatives , beta - blockers and some antidepressants needs to be suspended before the test so as not to affect the result . 
in the case of recent myocardial infarction , unstable angina , arrhythmias , severe aortic stenosis , severe heart failure , recent infarction , acute myocarditis / pericarditis and aortic aneurysm , conventional exercise stress testing is contraindicated . thromboembolism / pulmonary a second problem concerns the dose of ionising radiation . 
further studies are needed to better assess the cost - benefit ratio compared with other techniques . inoltre , essere ricordato che la terapia farmacologica con farmaci quali la digitale , i nitroderivati , i betabloccanti ed alcuni antidepressivi dovrebbe essere sospesa prima dellesecuzione del test al fine di non condizionarne il risultato . 
in caso di infarto miocardico recente , angina instabile , aritmie , stenosi aortica severa , scompenso cardiaco severo , trombo - embolia / infarto polmonare recenti , miocardite / pericardite in fase acuta , aneurisma dellaorta , il test da sforzo tradizionale controindicato . una seconda problematica riguarda la dose di radiazioni ionizzanti . 
se vero che la dose riportata pari a 1521 msv superiore a quella di unacc , bisogna sottolineare che questultima comporta un rischio di complicanze maggiori pari al 2% [ 23 ]  . 
se poi effettuiamo il paragone con la scintigrafia miocardica bisogna ricordare che questultima espone il paziente ad una dose di radiazioni ionizzanti analoga [ 24 ]  . studi prospettici pi ampi sono necessari per meglio giudicare il valore diagnostico dellac - tcms addizionale al test da sforzo nei pazienti a bassa probabilit pre - test di ca significativa ( pazienti con angina atipica o dolore toracico non cardiaco ) che teoricamente potrebbero trarre maggior beneficio da una metodica non invasiva . le recenti tecnologie a doppia sorgente hanno introdotto ulteriori miglioramenti dal punto di vista della compliance della metodica ac - tcms nei confronti di frequenze cardiache pi elevate ( ad esempio > 6570 bpm ) e rispetto alle strategie di limitazione della dose di radiazioni ionizzanti . 
questi miglioramenti renderanno progressivamente pi accettabile il compromesso tra rischio necessario della procedura e beneficio dellinformazione diagnostica . conclusioni la prova da sforzo fornisce informazioni aggiuntive che agevolano liter diagnostico dei pazienti con angina stabile , ma appare di limitato valore diagnostico nellindividuazione di una ca significativa , specialmente nella popolazione che ricade nella fascia di rischio intermedio . 
lesecuzione di unac - tcms dopo la prova da sforzo migliora marcatamente la probabilit post - test della presenza di una significativa ca specialmente quando il test ergometrico sia negativo o inconclusivo . 
twenty - six consecutive patients , 14 with liver metastases ( ten from colorectal cancer ; four from carcinoid tumours ) and 12 with biliary cancers ( ten klatskin tumours ; one gallbladder tumour ; one intrahepatic cholangiocarcinoma ) with insufficient predicted future remnant liver ( frl ) underwent right pve to induce hypertrophy of the contralateral hemiliver prior to surgical resection . 
the frl volume increased by 5%25% ( 15% on average ) after right pve in patients with liver metastases and by 9%19% ( 14% on average ) in patients with biliary cancers . 
in all patients , the ratio of frl to functional liver volume was 30% after right pve . no postoperative deaths due to severe liver failure occurred in the 20 patients who underwent extended hepatectomy . 
lo scopo del nostro studio retrospettivo stato di valutare lefficacia dellembolizzazione del ramo portale destro ( rpve ) come trattamento pre - chirurgico per indurre lipertrofia del fegato sinistro in pazienti candidati a resezione epatica . 
ventisei pazienti consecutivi , 14 portatori di metastasi epatiche ( colon - retto , 10 pazienti ; carcinoide , 4 pazienti ) e 12 portatori di neoplasia delle vie biliari ( neoplasia di klatskin , 10 pazienti ; neoplasia della colecisti , 1 paziente ; colangiocarcinoma intraepatico , 1 paziente ) con potenziale riserva funzionale epatica ( frl ) insufficiente sotto stati sottoposti a rpve come trattamento pre - chirurgico . 
il volume del frl ha dimostrato un incremento volumetrico compreso tra il 5%25% ( 15% in media ) dopo rpve nei pazienti con metastasi epatiche e tra il 9%19% ( 14% in media ) in pazienti con neoplasie biliari . 
lembolizzazione portale allarga le indicazioni alla chirurgia resettiva epatica in pazienti con metastasi epatiche e neoplasie delle vie biliari con potenziale riserva funzionale insufficiente . 554 radiol med ( 2009 ) 114 : 553570 keywords right portal vein embolisation hepatic functional reserve ct hepatic volumetry parole chiave embolizzazione del ramo portale destro riserva funzionale epatica tc volumetria epatica introduction introduzione the curative treatment of primary and secondary liver cancers that ensures long - term survival is surgery . 
more than 45% of liver tumours , both primary and secondary , require extended liver resection with disease - free margins . postoperative death after extended hepatectomy , which ranges from 3.2%7% in patients with a normal hepatic functional reserve to 32% in patients with cirrhosis , is most often caused by an insufficient future remnant liver ( frl )  . postoperative liver failure has been shown to be directly related to frl volume , and preoperative procedures to induce liver regeneration have been proposed [ 13 ]  . 
on the basis of experimental studies in 1920 that showed that ligation of a portal branch led to atrophy of the ipsilateral liver parenchyma and hypertrophy of parenchyma with preserved portal flow , makuuchi et al . 
 [ 4 ] in 1990 used portal occlusion as a preoperative treatment to extend the indication for curative liver resection to patients with biliary cancers . embolisation of a portal branch is currently indicated when the volume of the predicted frl is insufficient to ensure an adequate postoperative hepatic functional reserve . 
separate determinations of liver volume and tumour volume makes it possible for hepatic functional reserve to be estimated with computed tomography ( ct ) and magnetic resonance ( mr ) imaging by subtracting tumour volume from total liver volume , i.e. 
the potential functional reserve of frl as a ratio between the frl and the total functional liver mass . the purpose of this retrospective study was to assess the effectiveness of right portal vein embolisation ( pve ) as a preoperative treatment in noncirrhotic patients in whom the predicted functional reserve of the frl , calculated with ct , was insufficient for radical liver resection . 
in pi del 45% dei tumori del fegato , sia primitivi che secondari , necessaria unampia chirurgia resettiva epatica che assicuri margini di resezione liberi da malattia . la principale causa di morte post - chirurgica dopo epatectomie estese , che oscilla tra il 3 , 2% e 7% nei pazienti con normale riserva funzionale epatica e fino al 32% nei pazienti con cirrosi , spesso un insufficiente future remnant liver ( frl )  . 
stato dimostrato che linsufficienza epatica post - chirurgica direttamente correlata al volume del frl e sono state proposte procedure pre - chirurgiche che inducono la rigenerazione epatica [ 13 ]  . 
sulla base di studi sperimentali che nel 1920 avevano dimostrato che la legatura di un ramo portale determinava latrofia del parenchima epatico tributario e lipertrofia del parenchima epatico con flusso portale conservato , makuuchi et al . 
 [ 4 ] gi nel 1990 hanno usato per primi locclusione portale come trattamento pre - chirugico per ampliare lindicazione a chirurgia resettiva epatica curativa in pazienti portatori di neoplasie delle vie biliari . 
lembolizzazione di un ramo portale attualmente indicata quando il volume del potenziale frl inadeguato ad assicurare unadeguata riserva funzionale epatica postchirurgica e quindi il calcolo della volumetria epatica necessario per selezionare i pazienti da sottoporre a trattamento pre - chirurgico . 
il calcolo separato del volume epatico e del volume tumore permette oggi alla tomografia computerizzata ( tc ) ed alla risonanza magnetica ( rm ) di valutare la riserva funzionale epatica sottraendo al volume totale epatico il volume tumore e quindi la potenziale riserva funzionale del frl come rapporto del frl sulla massa epatica totale funzionante . scopo primario di questo studio retrospettivo di valutare lefficacia dellembolizzazione del ramo portale destro ( rpve ) come trattamento pre - chirurgico in pazienti non cirrotici nei quali la potenziale riserva funzionale del frl , calcolata mediante tc , era insufficiente per una chirurgia resettiva epatica oncologicamente radicale . 
 materials and methods materiali e metodi between november 1996 and september 2007 , 26 noncirrhotic patients ( 12 men and 14 women , aged 3581 years ; mean age 58 years ) underwent pve procedures . 
dodici pazienti erano portatori di neoplasie delle vie biliari [ 5 ] : neoplasia di klatskin ( 10 pazienti ) classificati secondo bismuth come tipo ii ( interruzione convergenza biliare principale , 6 pazienti ) , tipo iiia ( interruzione radiol med ( 2009 ) 114 : 553570 confluence , n = 6 ) , type iiia ( obstructed main confluence extending to the right secondary confluence , n = 2 ) , type iv ( obstructed primary and secondary confluence bilaterally , n = 2 ) , gallbladder cancer ( n = 1 ) and intrahepatic cholangiocarcinoma ( n = 1 )  . 
in particular , the lesions were located in the right liver lobe and in segment iv in three patients ( two with colorectal metastases and one with carcinoid metastases ) and in the right liver lobe in segments iv and ii in two patients ( one with colorectal metastases one with carcinoid metastases )  . 
all patients with hepatic metastases from colorectal cancer underwent chemotherapy ( three to six cycles , four cycles on average ) , with partial response ( no less than 30% ) according to the response evaluation criteria in solid tumours ( recist ) criteria [ 6 ] or with stable disease . 
in the patient with bilobar colorectal metastases in segments ii and iv of the left liver , right pve was preceded by excision of the left lobar metastases , a procedure known as two - stage hepatectomy . 
all patients with klatskin tumours underwent percutaneous biliary drainage bilaterally ( n = 6 ) or on the left side only ( n = 4 ) ; a prerequisite for right pve was biliary drainage of the frl with reduction of bilirubin ( < 3 mg / dl )  . 
in particolare le lesioni erano localizzate nel fegato destro e nel iv segmento epatico in 3 pazienti ( 2 da neoplasia colo - rettale e 1 da carcinoide ) ; nel fegato destro , nel iv e nel ii segmento in 2 pazienti ( 1 da neoplasia colo - rettale e 1 da carcinoide )  . tutti i pazienti portatori di metastasi epatiche da neoplasie colo - rettali hanno effettuato chemioterapia ( 36 cicli con una media di 4 cicli ) con una risposta parziale ( non inferiore al 30% ) secondo i criteri recist ( response evaluation criteria in solid tumours ) [ 6 ] o con malattia stabile , che ha preceduto lembolizzazione portale con un intervallo di tempo di almeno 28 giorni . 
nel paziente portatore di metastasi bilobari da neoplasia colo - rettale , localizzate nel fegato sinistro , in corrispondenza del ii oltre che nel iv segmento , la rpve stata preceduta dalla metastesectomia delle metastasi del fegato sinistro , two stage hepatectomy . 
i pazienti con metastasi da carcinoide non sono stati sottoposti a terapia neo - adiuvante : quando possibile , la resezione epatica rappresenta in questi pazienti il miglior trattamento in termini di sopravvivenza a lungo termine [ 7 ]  . tutti i pazienti portatori di neoplasie di klatskin sono stati sottoposti a drenaggio biliare per via transcutanea dei due emisistemi biliari ( 6 pazienti ) o dellemisistema di sinistra ( 4 pazienti ) ; presupposto indispensabile alla rpve stato il drenaggio biliare del frl con riduzione dei valori ematici di bilirubina ( non superiore a 3 mg / dl )  . 
 nel periodo compreso tra il 1996 ed il 2003 gli esami tc sono stati eseguiti in 11 pazienti con tc spirale singolo strato prospeed advantage ( ge medical systems , milwaukee , wis , usa ) come precedentemente descritto [ 8 ]  . nel periodo compreso tra il 2003 ed il 2007 gli esami tc sono stati eseguiti in 15 pazienti mediante tc spirale multistrato lightspeed pro 16 ( ge medical system ) , utilizzando i seguenti parametri : ma automatico ( noise index 14 ) , 120 kvp , collimazione dei detettori 1 , 25 , velocit del tavolo 18 , 75 mm per rotazione , velocit di rotazione del gantry 0 , 6 secondi a rotazione . 
sono stati utilizzati uno spessore di ricostruzione di 2 , 5 mm ed un intervallo di ricostruzione di 2 , 5 mil mezzo di contrasto ( 2 ml / kg di peso corporeo con una concentrazione di 350 mgi / ml ) stato somministrato per via ev attraverso lutilizzo di un iniettore automatico , ad una velocit di 45 ml / s attraverso un ago - cannula di 18 gauge posta in una vena del braccio . 
la scelta dei tempi di ritardo per lacquisizione delle immagini stata ottenuta mediante lutilizzo di un sistema automatico di bolus tracking che prevedeva un singolo sistema di monitoraggio a bassa dose posto a livello di un vaso dinteresse ( aorta addominale ) dopo circa 10 secondi dallinizio delliniezione del mezzo di contrasto ; raggiunto un picco di enhancement di circa 80 uh nella regione dinteresse , circa 10 secondi dopo iniziava lacquisizione della fase arteriosa . 
le fasi portali e tardive venivano calcolate a 70 e 180 secondi dalliniezione del mezzo di contrasto . 556 radiol med ( 2009 ) 114 : 553570 number , location and volume of the liver metastases as well as the resectability criteria based on the evaluation of vascular relationships ensuring adequate perfusion , and venous and biliary drainage of the frl . 
in no patient did the ct scan provide a ratio of hepatic to splenic parenchyma density ratio 1.1 , an indication of moderate - to - severe ( 30% ) steatosis [ 9 , 10 ]  . all patients with klatskin tumours underwent mr cholangiography ( 1.5 - tesla , horizon advantage system , ge medical systems ) to stage the biliary disease . 
volumetric data were obtained from the portal - venous - phase scans , and all examinations were processed by two radiologists on a workstation ( ge medical system 4.1 ) that automatically calculated the volume by multiplying the area by the thickness and also generated 3d reconstructions . the liver parenchyma was isolated from surrounding tissues by using the cursor , and the total liver volume was calculated . 
frl was jointly determined by surgeons and radiologists on the basis of disease extent on imaging ( number , site , vascular relationships of metastases and vascular relationships of biliary cancers ) and according to the surgical plan defined by the surgeons . 
in the volumetric assessment the suprahepatic veins , the teres ligament , the umbilical portion of the left portal branch , the gallbladder and the inferior vena cava were used as anatomical landmarks to delineate the liver segments and separate the liver to be resected from the frl . 
tumour volume was not calculated in patients with biliary cancers , as small size and predominantly biliary involvement made it irrelevant to the evaluation of the ratio of frl volume to total volume of nontumourous liver parenchyma . 
the catheter was advanced to the portal trunk and , after the injection of contrast material , portography was performed to identify the intrahepatic portal branches and any anatomical variants . 
all patients underwent a ct scan 1 week before right pve and , after right pve , within a week before surgery . selection criteria for pve was an frl / total functional liver parenchyma ratio 30% . 
where waiting times exceeded 1 month , this was related to one patient with liver metastases refusing surgery for 2 months , and to our deferring surgery to after having solved the lesame tc prima e dopo rpve ha fornito il numero , la sede , il volume delle metastasi epatiche ed i criteri di resecabilit , basata sulla valutazione dei rapporti vascolari che assicurassero adeguata perfusione , drenaggio venoso e biliare del frl . 
in nessun paziente lesame tc ha rilevato il rapporto della densit parenchima epatico - parenchima splenico 1 , 1 , indice di steatosi moderata - grave ( superiore al 30% ) [ 9 , 10 ]  . tutti i pazienti portatori di neoplasie di klatskin hanno eseguito la colangio - rm per stadiare la malattia sul versante biliare ( stata utilizzata apparecchiatura a 1 , 5 tesla , horizon advantage ge medical systems , milwaukee , wis )  . 
i dati volumetrici sono stati elaborati dalle scansioni eseguite durante la fase portale dellenhancement vascolare e tutti gli esami sono stati elaborati da due radiologi dedicati ad una workstation ( ge medical system 4.1 ) che ci ha fornito il volume mediante il calcolo automatico dellarea x lo spessore , fornendoci anche ricostruzioni 3d . mediante un cursore stato isolato il parenchima epatico dai tessuti circostanti ed stato calcolato il volume epatico totale . 
le vene sovraepatiche , il legamento rotondo , la porzione ombelicale del ramo portale sinistro , la colecisti e la vena cava inferiore sono stati utilizzati come reperi anatomici per delineare i vari segmenti epatici e per separare nella valutazione volumetrica il fegato da resecare dal frl . 
il volume tumore non stato calcolato nei pazienti con neoplasie delle vie biliari per le piccole dimensioni e per il prevalente coinvolgimento biliare , quindi non stato considerato rilevante nella valutazione del rapporto tra volume del frl e volume del parenchima epatico totale funzionante . 
 lembolizzazione del ramo portale destro stata effettuata dopo puntura sotto guida ecografica del ramo portale di sinistra a livello del recesso di rex ; il catetere ha raggiunto quindi il tronco portale e con liniezione del mdc si ottenuto una portografia per individuare i rami portali intra - epatici ed eventuali varianti anatomiche ; successivamente si occluso il ramo portale destro con le sue diramazioni con materiale embolizzante costituito da cianoacrilato e lipiodol . 
tutti i pazienti sono stati sottoposti ad esame tc entro una settimana prima della rpve e dopo rpve entro una settimana prima della chirurgia . il criterio di selezione dei pazienti da sottoporre ad rapporto embolizzazione prechirurgica frl / parenchima epatico totale funzionante inferiore al 30% . 
any volume changes in frl before and after right pve were assessed with the t test , with significance set at p < 0.001. results the injection of cyanoacrylate and lipiodol achieved complete embolisation of the right portal tree in 24 patients . in two patients , preliminary embolisation of the portal branch of segment iv to be resected according to the surgical plan was achieved . 
 the increase a significant change ( p < 0.001 ) in frl volume after right pve was obtained both in patients with liver metastases and in those with biliary cancers . 
in nine patients with hepatic colorectal metastases , in frl volume ( 18571.16 cm3 ) after 2548 days ( 33.8 days on average ) associated with atrophy of the functional liver parenchyma to be resected ( 186.196.62 cm3 ) changed the frl / total functional liver - volume ratio from 18%29% ( 25% on average ) before right pve to 30%51% ( 39% on average ) after right pve . 
after right pve , the volume of the metastases from colorectal cancer in the embolised liver increased by 6%155.5% , whereas in the patient who waited 60 days , the tumour increased in volume by 562.7% ( table 1 )  . 
patients with metastases from carcinoid tumours showed no increase in volume of metastases after right pve in either the embolised or unembolised liver , whereas frl hypertrophy ( 283.7570.1 cm3 ) significantly changed liver parenchyma ratio from 20%27% to 42%52% ( table 1 ) after a period of 3034 days ( 31 days on average )  . 
after a period of 3180 days ( 45.9 days on average ) after right pve , frl hypertrophy ( 187.1671.5 cm3 ) and atrophy of the parenchyma to be resected ( 305.7182.5 cm3 ) changed 30%45% ( table 2 )  . 
le variazioni volumetriche del frl prima e dopo rpve sono state valutate mediante il test t di student ( un valore di p < 0 , 001 stato considerato significativo )  . risultati mediante liniezione di cianoacrilato e lipiodol si ottenuta lembolizzazione completa dellalbero portale di destra in 24 pazienti . 
in 2 pazienti si ottenuta lembolizzazione del ramo portale segmentario del iv segmento da resecare nel programma chirurgico , in uno dei quali la successiva embolizzazione a destra non stata completa ed ha interessato solo il settore anteromediale . 
un paziente stato sottoposto ad una seconda seduta di embolizzazione che ha seguito di 22 giorni la precedente con la quale non si era ottenuta lembolizzazione completa dellalbero portale di destra . 
 la variazione volumetrica dopo rpve del frl stata significativa nei pazienti con metastasi epatiche ( p < 0 , 001 ) e nei pazienti con neoplasie delle vie biliari ( p < 0 , 001 )  . 
in 9 pazienti portatori di metastasi da colon - retto lincremento volumetrico del frl ( 18571 , 16 cm3 ) dopo un periodo compreso tra i 25 ed i 48 giorni ( in media 33 , 8 giorni ) associato allatrofia del parenchima epatico funzionante da resecare ( 186 , 196 , 62 cm3 ) ha modificato il rapporto frl / volume epatico totale funzionante dal 18%29% ( in media 25% ) prima della rpve al 30%51% ( in media 39% )  . 
dopo rpve si riscontrato un incremento volumetrico delle metastasi da colon - retto nel fegato embolizzato compreso tra il 6% e il 155 , 5% , mentre nella paziente che ha atteso 60 giorni lincremento del volume tumore stato del 562 , 7% ( tabella 1 )  . 
nei pazienti portatori di metastasi da carcinoide dopo rpve non si verificato incremento volumetrico delle metastasi sia nel fegato embolizzato che nel fegato non embolizzato , mentre lipertrofia del frl ( 283 , 7570 , 1 cm3 ) ha significativamente cambiato il rapporto frl / parenchima epatico funzionante dal 20%27% al 42%52% ( tabella 1 ) dopo un periodo compreso tra i 30 ed i 34 giorni ( in media 31 giorni )  . 
nei pazienti portatori di neoplasie delle vie biliari lfrl costituiva il 18%28 , 6% del parenchima epatico funzionante , dopo un periodo compreso tra i 31 e gli 80 giorni ( in media 45 , 9 giorni ) dopo rpve lipertrofia del frl ( 187 , 1671 , 5 cm3 ) e latrofia del parenchima da resecare ( 305 , 7182 , 5 cm3 ) ha modificato questo rapporto compreso 30%45% ( tabella 2 )  . 
non progressione di malattia rispetto allesame pre - rpve stata documentata dalla tc nelle neoplasie di klatskin , nella neoplasia della colecisti e 558 radiol med ( 2009 ) 114 : 553570 radiol med ( 2009 ) 114 : 553570 560 radiol med ( 2009 ) 114 : 553570 radiol med ( 2009 ) 114 : 553570 562 radiol med ( 2009 ) 114 : 553570 patient who had undergone metastasectomy during previous surgery . 
eight patients with biliary cancers underwent right hepatectomy extended to segment i ( n = 3 ) and to segments i and iv ( n = 5 )  . preoperative imaging understaged four patients , and radical surgery could not be performed owing to the finding , on exploratory laparotomy , of peritoneal carcinosis ( one patient with metastasis from colon cancer ) , positive lymph nodes at the hepatic hilum ( one patient with type ii klatskin tumour ) , neoplastic lymphangitis along the hepatic pedicle ( one patient with type ii klatskin tumour ) and hepatic artery invasion ( one patient with type iv klatskin tumour )  . 
two patients did not undergo surgical exploration : one with a klatskin tumour because of the onset of ascites after the second embolisation session , and the other with colorectal cancer because of the onset of lung metastases . 
 discussion surgery of biliary cancers is a difficult procedure requiring hepatectomy extended to the caudate lobe , a site of possible recurrence ; resection of the main bile duct with creation of biliodigestive anastomoses ; and possible vascular reconstructions in patients with obstructive jaundice . 
five - year survival in patients with klatskin tumours treated with surgical resection with disease - free margins is between 43% and 46% , but it involves ablation of up to 80% of the liver parenchyma [ 13 ]  . 
in our experience , five patients with biliary cancers who underwent surgical resection after right pve required a right hepatectomy extended to segment iv associated with caudectomy ( necessary for all patients with biliary cancer )  . 
reported that in 132 patients with cholangiocarcinoma who underwent surgical resection after right pve due to insufficient frl volume , the 5 - year survival rate was comparable to that of a control group who underwent surgery without preoperative right pve owing to adequate frl [ 12 ]  . patients with unresected liver metastases from colorectal cancer had a mean survival of 421 months , with a 3 - year survival rate less than 3% . systemic chemotherapy improves quality of life but has limited impact on survival . 
dodici pazienti portatori di metastasi epatiche sono stati sottoposti ad epatectomia destra ( 4 pazienti ) , epatectomia destra allargata a i e iv segmento ( 2 pazienti ) , epatectomia destra allargata al iv ( 6 pazienti ) , uno dei quali con metastesectomia in un precedente tempo chirurgico . 
in tutti i pazienti stata eseguita lecografia intraoperatoria che ha confermato il numero e la sede delle lesioni individuate allesame tc . otto pazienti portatori di neoplasie biliari sono stati sottoposti ad epatectomia destra allargata al i segmento ( 3 pazienti ) e ad epatectomia destra allargata a i e iv segmento ( 5 pazienti )  . quattro pazienti sono stati sottostadiati allimaging preoperatorio e non stato possibile effettuare una chirurgia oncologicamente radicale per la presenza alla laparotomia esplorativa di carcinosi peritoneale ( 1 pazienti portatore di metastasi da neoplasia del colon ) , di linfonodi positivi allilo epatico ( 1 pazienti con tumore di klatskin tipo ii ) , per linfangite neoplastica lungo il peduncolo epatico ( 1 pazienti con tumore di klatskin tipo ii ) , per infiltrazione dellarteria epatica ( 1 pazienti con tumore di klatskin tipo iv )  . 
2 pazienti non sono stati esplorati chirurgicamente , un pazienti portatore di neoplasia di klatskin per la comparsa di ascite dopo la seconda seduta di embolizzazione e laltro pazienti con neoplasia colon - rettale per la comparsa di metastasi polmonari . 
nellimmediato postoperatorio , nella nostra casistica , nessun paziente deceduto per insufficienza epatica grave post - chirurgica ; solo in quattro pazienti si avuta una transitoria lieve insufficienza epatica ( bilirubina > 2 , 9 mg / dl e riduzione del tempo di protrombina < 50% [ 11 ] )  . 
 discussione la chirurgia delle neoplasie delle vie biliari una procedura difficile che richiede estese epatectomie che comprendono sempre il lobo caudato , sede di possibile recidiva , la resezione della via biliare con la ricostruzione di anastomosi biliodigestive , possibili ricostruzioni vascolari , in pazienti con ittero ostruttivo e , quindi , la riduzione dei rischi chirurgici e postchirurgici un sfida per il chirurgo epatobiliare [ 12 ]  . 
la sopravvivenza a 5 anni nei pazienti portatori di neoplasie di klatskin sottoposti ad exeresi chirurgica con margini di resezione libera da malattia compresa tra 43%46% ma prevede lasportazione fino all80% del parenchima epatico [ 13 ]  . 
 [ 12 ] hanno verificato in 132 pazienti con colangiocarcinoma , sottoposti ad exeresi chirurgica dopo rpve per insufficiente frl , che la sopravvivenza a 5 anni sovrapponibile ad un gruppo di controllo sottoposto a chirurgia senza rpve per adeguato frl [ 12 ]  . 
nei pazienti con metastasi epatiche da neoplasie del colon - retto non trattate chirurgicamente , la sopravvivenza media varia dai 4 ai 21 mesi con una sopravvivenza a 3 anni inferiore al 3% . radiol med ( 2009 ) 114 : 553570 fig . 
1a - h computed tomography ( ct ) images obtained before and after right portal vein embolisation ( rpve ) in a 71 - year - old man with gallbladder cancer . 
a - d axial and oblique reformatted ct images obtained before ( a , b ) and after ( c , d ) rpve show the gallbladder cancer invading liver segments iv ( arrows in a and c ) and v ( arrows in b and d ) without hilar invasion . 
e - h twoand three - dimensional maximum intensity projection ( mip ) reformations obtained before ( e , f ) and after rpve ( g , h ) clearly show a proportional twofold atrophy - hypertrophy effect ( decrease in volume of the right liver and increase in volume of the left liver )  . 
a - d le immagini tc assiali e le ricostruzioni oblique ottenute prima ( a , b ) e dopo ( c , d ) rpve documentano la neoplasia delle colecisti che invade iv ( frecce in a e c ) e v segmento epatico ( frecce in b e d ) , senza infiltrazione dellilo . 
e - h le ricostruzioni 2d e 3d mip ottenute prima ( e , f ) e dopo rpve ( g , h ) dimostrano chiaramente un proporzionale duplice effetto atrofia - ipertrofia ( riduzione di volume del fegato destro ed incremento volumetrico del fegato sinistro )  . 
a , b maximum intensity projection ( mip ) reformation in the portal phase ( a ) and axial computed tomography ( ct ) in the delayed phase ( b ) demonstrate an enhancing irregular nodular mass ( arrows in a and b ) adjacent to the right portal vein and invading segment iv with involvement of the right secondary biliary confluence and dilatation of the right intrahepatic bile duct . 
after rpve , left hepatic hypertrophy is evident on 3d mip reconstructions , on anterior view ( c ) and at surgery ( d ) , with evident delimitation caused by the different perfusion of the two hemilivers . 
a , b la ricostruzione mip 2d in fase portale ( a ) e limmagine assiale in fase tardiva ( b ) documentano una formazione nodulare , irregolare e con enhancement ( frecce in a e b ) adiacente al ramo portale di destra che invade il iv segmento con interruzione della convergenza biliare secondaria di destra e dilatazione a monte delle vie biliari intraepatiche dellemisistema di destra . 
lipertrofia del fegato sinistro dopo rpve evidente nelle ricostruzioni mip 3d , visione anteriore ( c ) e allintervento chirurgico ( d ) con evidente demarcazione per la diversa perfusione dei due emifegati . 
the nonresectability of potential candidates for resection may be related to an insufficient frl ( 8% in 746 hepatectomies in elias et al.s experience ) [ 16 ]  . the liver has the ability to regenerate rapidly , a property that provides the rationale for new and innovative surgical techniques for liver resection and organ transplantation . 
one strategy employed by many hepatobiliary surgeons to reduce the risk of complications after extended hepatectomy is pve . occlusion of a portal branch causes the redistribution of the portal flow with a double effect : atrophy of the embolised parenchyma and hypertrophy of the unembolised parenchyma . 
lunico trattamento che migliora la sopravvivenza quello chirurgico : dopo la resezione a 5 anni stimata essere tra il 25% ed il 40% , a 10 anni tra il 22% e il 26% [ 14 , 15 ]  . 
tuttavia lintervento chirurgico possibile solo nel 15%25% dei pazienti con metastasi da colon - retto in relazione allo stadio della malattia , alla localizzazione delle lesioni ripetitive epatiche ed a problemi tecnici ma in pazienti potenzialmente resecabili la non resecabilit pu essere legata ad un insufficiente frl ( 8% in 746 epatectomie nellesperienza di elias ) [ 16 ]  . il fegato possiede la capacit di rigenerare velocemente e su questo principio si basano le pi moderne ed innovative tecniche chirurgiche di resezioni epatiche e di trapianto dorgano . 
locclusione di un ramo portale determina la ridistribuzione del radiol med ( 2009 ) 114 : 553570 to be resected and hypertrophy of the frl is to the advantage of the potential postoperative hepatic functional reserve . immediately after embolisation , the portal flow increases in the unembolised portal territory , as demonstrated by doppler ultrasonography [ 17 ] , leading to parenchymal hypertrophy that correlates with the magnitude of the increase in portal flow [ 8 , 18 , 19 ]  . 
 [ 21 ] , however , showed that not only the amount but also the quality of portal blood affects liver regeneration , and it is indeed the blood flowing back from the pancreatic bed that contains hepatotrophic factors . 
 [ 22 ] reported that the regeneration process of a normal liver after resections occurs in three phases : rapid increase during the first month , decrease during the second month and , finally , extremely slow increase . 
 [ 23 ] recently demonstrated that noncirrhotic livers require a minimum of 3 weeks after right pve owing to hypertrophy of the frl , followed by a plateau lasting between 22 and 56 days . 
noncirrhotic livers have the greatest regenerative capacity ( approximately 1221 cm3 / day 2 weeks after pve , approximately 11 cm3 / day at 4 weeks and 6 cm3 / day at 32 weeks ) [ 2 , 24 , 25 ]  . 
in noncirrhotic patients , a period of 34 weeks is required to assess the efficacy of pve in increasing frl volume . longer waiting periods , related to inflammatory biliary complications in patients with biliary cancers or to the patients refusal , showed that the atrophy of the embolised parenchyma progresses over time , whereas the hypertrophy of the frl is not significantly different . 
 at the beginning of our experience , when surgical planning envisaged a right hepatectomy extended to segment iv , we combined embolisation of the portal branch of segment iv with subsequent right pve . 
 [ 26 ] , we no longer believe this approach to be necessary , in part in consideration of the increased risk of accidental reflux of embolising material into the left portal branch . 
the potential hepatic functional reserve is calculated by using ct determinations of frl volume and total volume of functional liver parenchyma , obtained by subtracting tumour volume from total liver volume , and thus by the frl / total functional liver - volume ratio . 
the method allows for separate determinations of tumour volume and healthy parenchyma , thereby providing an flusso portale con un duplice effetto : latrofia del parenchima epatico embolizzato e lipertrofia del parenchima epatico non embolizzato . 
questo duplice effetto antagonista con atrofia del parenchima epatico da resecare ed ipertrofia del frl a vantaggio della potenziale riserva funzionale epatica post - chirurgica . immediatamente dopo lembolizzazione il flusso portale aumenta , come dimostrato mediante eco - doppler [ 17 ] , nel territorio portale non embolizzato determinando ipertrofia del parenchima epatico che correla con lentit dellincremento del flusso portale [ 8 , 18 , 19 ]  . 
 [ 21 ] hanno dimostrato che non solo la quantit , ma anche la qualit del sangue portale influenza la rigenerazione epatica , infatti il sangue refluo dal letto pancreatico che contiene fattori epatotrofici . 
 [ 22 ] hanno dimostrato che il quadro rigenerativo di un fegato normale dopo resezioni epatiche consiste in tre fasi : un rapido incremento durante il primo mese , un decremento nel secondo e alla fine un lentissimo incremento . 
 [ 23 ] hanno recentemente dimostrato che in fegati non cirrotici un minimo di 3 settimane richiesto dopo rpve per lipertrofia dellfrl seguito da un plateau compreso tra 22 e 56 giorni . 
fegati non cirrotici dimostrano la pi alta capacit rigenerativa ( circa 1221 cm3 / d a 2 settimane dopo lembolizzazione portale , circa 11 cm3 / d a 4 settimane e 6 cm3 / d a 32 settimane ) [ 2 , 24 , 25 ]  . 
fegati cirrotici o pazienti diabetici mostrano il pi basso grado di ricrescita approssimativamente ( 9 cm3 / d a 2 settimane dopo pve ) [ 2 , 25 ]  . 
il periodo di attesa pi lungo , in relazione a complicanze flogistiche biliari nei pazienti portatori di neoplasie delle vie biliari o al rifiuto di una paziente , ha dimostrato che latrofia del parenchima epatico embolizzato progressiva nel tempo mentre non significativamente diversa lipertrofia del frl . 
 allinizio della nostra esperienza , quando il programma chirurgico prevedeva lepatectomia destra allargata al quarto segmento , abbiamo associato lembolizzazione del ramo portale segmentario del iv che precedeva lembolizzazione del ramo portale di destra , ma in accordo con capussotti et al . 
la potenziale riserva funzionale epatica calcolata mediante la volumetria tc del frl e del volume totale del parenchima epatico funzionante , ottenuto sottraendo al volume epatico totale il volume tumore e quindi dal loro rapporto ( frl / volume totale epatico funzionante )  . 
la metodologia da noi usata permette di ottenere la volumetria separata del volume 566 radiol med ( 2009 ) 114 : 553570 accurate estimation of functional parenchyma , particularly in those cases where the liver parenchyma to be resected is extensively involved . 
 [ 27 ] demonstrated that the evaluation of tumour volume in patients with liver metastases significantly affects the evaluation of the hepatic functional reserve . the evaluation of tumour volume before and after right pve also provided us with information on the oncogenic effect of right pve on liver disease . 
in biliary cancers , no local disease progression was detected . our results coincide with previous experiences [ 8 , 28 ] that reported an increase in volume of hypovascular metastases from colorectal cancers after right pve in embolised and unembolised livers and no change in the volume of hypervascular metastases from carcinoid tumours in either tumore e del parenchima sano e quindi fornisce la valutazione reale del parenchima funzionante , in particolare nei casi in cui il parenchima epatico da resecare in gran parte sostituito . 
 [ 27 ] hanno infatti dimostrato che nei pazienti portatori di metastasi epatiche la valutazione del volume tumore incide in maniera significativa nella valutazione della riserva funzionale epatica . la valutazione del volume tumore prima e dopo rpve ci ha inoltre fornito dati sulleffetto oncogenetico della metodica sulla patologia epatica . 
dopo rpve nella patologia secondaria epatica aumentato il volume delle metastasi da colon - retto mentre rimasto immodificato il volume tumore nelle metastasi da carcinoide ; nelle neoplasie delle vie biliari non abbiamo riscontrato progressione locale di malattia . 
i nostri risultati concordano con esperienze precedenti [ 8 , 28 ] che avevano documentato laumento volumetrico delle metastasi , ipovascolari , da colon - retto dopo rpve nel fegato embolizzato e non embolizzato , mentre il volume delle metastasi ipervascolarizzate da carcinoide rimaneva invariato sia nel radiol med ( 2009 ) 114 : 553570 fig . 
a - f axial computed tomography ( ct ) scans obtained in a 54 - year - old man show multiple synchronous liver metastases from colon cancer in the left ( 1 , 2 , 5 ) and right ( 3 , 4 , 6 ) liver , with partial response after six cycles of chemotherapy . 
surgical plan : ablation with free resection margins of the liver lesion located in segment viii ( lesion 3 ) requires right hepatectomy combined with resection of the middle supra hepatic vethe potential frl consists of segments i , ii and iii . 
i - p axial ct scans obtained 29 days after rpve document left hepatic hypertrophy , especially of the caudate lobe , the outcome of previous left metastasectomy ( 1 , 2 , 5 ) and enlarged liver metastases in the right liver lobe ( tumour volume increased from 45 to 115 cm3 ) ( 3 , 4 , 6 )  . 
a - f in un paziente di 54 anni , le immagini assiali dellesame tc documentano multiple metastasi epatiche sincrone da cancro del colon localizzate nel fegato sinistro ( 1 , 2 , 5 ) e nel fegato destro ( 3 , 4 , 6 ) , con risposta parziale dopo 6 cicli di chemioterapia . 
programma chirurgico : lasportazione con margini di resezione liberi della lesione epatica dellviii segmento ( lesione 3 ) necessita di epatectomia destra , associata a resezione della vena sovraepatica media . 
i - p le immagini assiali della tc eseguita 29 giorni dopo lembolizzazione documentano lipertrofia del fegato sinistro , in particolare del lobo caudato , gli esiti della pregressa metastasectomia a sinistra ( 1 , 2 , 5 ) e le metastasi epatiche del fegato destro ( 3 , 4 , 6 ) aumentate di dimensioni ( volume tumore 115 vs 45 cm3 )  . 
 [ 29 ] hypothesised that a cytokine regulating the hepatocyte growth factor ( hgf ) which is altered in patients with colorectal cancer and distant metastases is responsible for the growth of liver metastases in these patients . 
in contrast , preoperative right pve does not affect 5 - year survival rates compared with control groups undergoing resection of liver metastases from colon cancer without right pve [ 16 ]  . new strategies are being proposed for patients with multiple liver metastases from colorectal cancer , which combine the intra - arterial [ 30 , 31 ] or systemic [ 3235 ] infusion of chemotherapeutic agents with selective pve , with the aim of simultaneously obtaining tumour shrinkage and fegato embolizzato che non embolizzato . 
 [ 29 ] hanno ipotizzato che una citochina che regola il fattore di crescita degli epatociti ( hgf ) , alterata nei pazienti con neoplasia colon - rettale e metastasi a distanza , sia responsabile della crescita delle metastasi epatiche in questi pazienti . 
lembolizzazione portale prechirurgica non modifica , invece , la sopravvivenza a 5 anni rispetto a gruppi di controllo sottoposti a chirurgia per metastasi epatiche da neoplasia del colon senza rpve [ 16 ]  . attualmente nuove strategie vengono proposte in pazienti portatori di multiple metastasi epatiche da colon - retto che associano alla selettiva embolizzazione portale infusione intraarteriosa [ 30 , 31 ] o sistemica [ 3235 ] di chemoterapici con lo scopo di ottenere contemporaneamente la 568 radiol med ( 2009 ) 114 : 553570 frl hypertrophy . 
 the second factor that affects the indication for right pve in candidates for liver resection is the possible coexistence of chronic liver disease , as this influences the amount of hepatic functional reserve needed to reduce postoperative morbidity and mortality . 
in patients with klatskin tumours , preventive drainage of the potential frl to resolve the cholestasis ( bilirubin < 2.9 mgdl ) is the essential precondition for pve to obtain an adequate regenerative response of the frl . 
 [ 27 ] , depending on the severity of cirrhosis and on residual liver function assessed with the indocyanine test . the presence of systemic disease , such as diabetes , in which the regenerative capacity of the liver is reduced by the hepatotrophic effect of insulin , and the complexity of surgery are , respectively , the third and fourth factors to be considered when selecting candidates for preoperative right pve . 
the use of lipiodol mixed with cyanoacrylate achieved right pve embolisation without complications and without recanalisation , with the added benefit of radiopacity allowing monitoring of the procedure by fluoroscopy [ 41 , 42 ]  . a potential functional reserve of frl < 30% constitutes an indication for right pve in patients previously exposed to chemotherapy or with previous cholestasis . 
 il secondo fattore che regola lindicazione alla rpve nei candidati a resezione epatiche leventuale concomitanza di epatopatia perch su questo si basa lentit della riserva funzionale epatica necessaria per ridurre la morbilit e mortalit post - chirurgica . 
lasportazione di pi del 75% del parenchima epatico ben sopportata nel paziente giovane ( 40 anni ) , ma la chirurgia resettiva epatica deve essere pi conservativa in relazione allet , alla patologia epatica e sistemica [ 36 ]  . 
 il minimo volume residuo del frl consigliato in pazienti con normale funzionalit epatica tra il 25%30% della massa epatica totale funzionante [ 9 , 19 , 35 , 36 ] anche se sono state effettuate resezioni epatiche con un volume di frl non inferiore al 20% senza complicanze post - chirurgiche [ 22 ]  . 
nei pazienti con neoplasie di klatskin , il preventivo drenaggio del potenziale frl che risolva la colestasi ( livello di bilirubina inferiore a 2 , 9 mgdecilitro ) il presupposto indispensabile allembolizzazione portale perch si ottenga unadeguata risposta rigenerativa del frl . 
la capacit rigenerativa del fegato cirrotico ridotta sia in relazione alla riduzione del flusso portale che alla fibrosi e quindi in questi pazienti il volume minimo del frl necessario pu raggiungere il 50% come dimostrato da kubota ed al . 
 [ 27 ] in relazione alla gravit della cirrosi e quindi alla funzionalit epatica residua valutata mediante il test dellindocianina . la presenza di una malattia sistemica come il diabete che riduce la capacit rigenerativa del fegato in relazione alleffetto epato - trofico dellinsulina e la complessit dellintervento chirurgico sono il terzo ed il quarto fattore da considerare nella selezione dei pazienti da candidare a rpve prechirurgica . 
 in conclusione , il nostro studio retrospettivo ha verificato che lembolizzazione portale pre - chirurgica una procedura sicura ; luso di lipiodol misto a cianoacrilato ha ottenuto lembolizzazione dellalbero portale destro senza complicanze e senza ricanalizzazione con il vantaggio legato alla sua radiopacit di monitorare lembolizzazione mediante fluoroscopia [ 41 , 42 ]  . la potenziale riserva funzionale del frl inferiore al 30% unindicazione alla rpve in pazienti precedentemente sottoposti a terapie chemioterapiche o con precedente colestasi ed allarga le indicazioni alla chirurgia radiol med ( 2009 ) 114 : 553570 extends the indications for liver resection in primary and secondary liver cancers , making radical surgery possible without severe postoperative complications . 
the addition of two - stage hepatectomy appears to be a promising innovation for patients with bilobar liver metastases from colorectal cancer . resettiva epatica in patologie primitive e secondarie epatiche rendendo possibile una chirurgia oncologicamente radicale senza gravi complicanze postchirurgiche . 
although combined ct and fluoroscopic guidance is normally preferred for difficult areas such as the cervical and upper thoracic vertebrae , to ensure operator radiation protection , the technique should also be considered for areas normally treated under fluoroscopic guidance alone . 
however , a larger patient series is needed to correctly evaluate the real contribution of low - dose ct to patient exposure . keywords vertebroplasty dose interventional radiology vertebral compression fracture riassunto obiettivo . 
in base a questo studio si osserva come la dose alloperatore sia in media circa 0 , 8 microsv in corso di vertebroplastica eseguita con guida combinata tc e radioscopica , mentre si attesti attorno a 5 , 8 microsv se eseguita con guida esclusivamente radioscopica ; per quanto riguarda i pazienti la dose di circa 6 msv per la guida combinata e circa 8 msv nel caso di guida esclusivamente radioscopica ; tale differenza non risulta statisticamente significativa . 
se la guida combinata tc e radioscopica risulta preferibile per sedi complesse come il trattamento a livello del rachide cervicale e dorsale alto essa da prendersi in considerazione qualora si privilegi la protezionistica delloperatore anche per quei metameri vertebrali solitamente trattati con esclusiva guida radioscopica , tuttavia serve una pi ampia casistica per poter valutare il reale contributo della tc a basso dosaggio nellesposizione del paziente . parole chiave vertebroplastica dose radiologia interventistica fratture vertebrali da compressione 596 introduction although most operators perform percutaneous vertebroplasty ( pvp ) using fluoroscopic guidance alone , there continues to be controversy as to whether the procedure should be performed under fluoroscopic guidance alone or with a combination of computed tomography ( ct ) and fluoroscopic guidance . 
however , when pvp is performed by experienced operators , fluoroscopy time is reduced to 10 min on average [ 2 ]  . the aim of this study was to evaluate the effective radiation dose to operators and patients during pvp performed under combined ct and fluoroscopic guidance and to compare it with corresponding dose measurements obtained during pvp carried out under fluoroscopic guidance alone . materials and methods dose measurements in previous studies were obtained both by using electronic and thermoluminescent dosimeters ( tld ) [ 1 ] and by recording the dose - area product ( dap ) and the entrance skin dose [ 3 , 4 ]  . 
in our study , operator dose was measured with an electronic dosimeter , whereas patient dose was determined by measuring the dap both with gafchromic films and with an ionisation chamber , from which we derived the effective dose . 
dap is defined as the integral of the absorbed dose to air across the area a of the beam : dap = ( cid : 2 ) adair ( a ) da dap has the useful property of being invariant with distance from the x - ray tube focus . 
this means it can be measured at any plane between the tube and the patient , as long as care is taken to avoid points of measurement with nonnegligible backscattered radiation from the patient and to ensure that the beam is focused on the detector . 
in the case of a uniform beam , as is assumed as a first approximation in diagnostic imaging , the equation becomes : dap dairxa other fundamental concepts are the absorbed dose and , radiol med ( 2009 ) 114 : 595607 introduzione la maggioranza degli operatori esegue la vertebroplastica percutanea ( pvp ) con guida esclusivamente radioscopica tuttavia continuano ad esserci due scuole contrapposte sulla tecnica : esclusiva guida radioscopica , combinata radioscopica e tc guidata , con fautori e detrattori delluna e dellaltra . 
una delle critiche pi frequenti nei confronti di coloro che preferiscono la guida tc che cos facendo la procedura molto pi lenta e che il rischio espositivo del paziente notevolmente superiore . 
in tali lavori si sono evidenziati tempi radioscopici molto variabili fra i 10 ed i 60 minuti ed una elevata esposizione per quanto riguarda loperatore , soprattutto alle estremit [ 1 ]  . tuttavia in mani esperte nei pi recenti lavori il tempo di scopia pu ridursi fino ad una media di 10 minuti [ 2 ]  . scopo del lavoro valutare leffettiva dose radiante a cui sono sottoposti operatore e paziente in corso di pvp con guida combinata radioscopica e tc e confrontarla con misurazioni analoghe eseguite in corso di pvp sotto esclusivo controllo radioscopico . materiali e metodi le misurazioni nei vari studi in letteratura sono state eseguite sia usando dosimetri termoluminescenti ( tld ) ed elettronici [ 1 ] sia registrando la dap ( dose per area ) e la dose in ingresso alla cute [ 3 , 4 ]  . 
per quanto riguarda il nostro studio la dose alloperatore stata misurata mediante dosimetro elettronico , mentre per quanto riguarda la dose al paziente stata misurata la dap sia mediante pellicole gaf - cromic sia con camera a ionizzazione trasmissiva da cui si ricavata la dose efficace ; tale valore stato sommato alla dose efficace in tc nei casi di guida combinata . 
per dap si intende il prodotto dose - area che definito come lintegrale della dose assorbita in aria sullarea a del fascio : dap = ( cid : 2 ) adair ( a ) da essa una grandezza particolarmente utile per la sua invarianza rispetto alla distanza dal fuoco che consente la sua misurazione in qualsiasi piano fra il tubo radiogeno e la posizione del paziente , con lunica avvertenza di evitare punti di misura in cui sia non trascurabile la radiazione retrodiffusa dal paziente e di assicurarsi che il fascio sia compreso nel rilevatore . 
tale grandezza include , oltre a quella di dose , una misura dellarea del fascio e quindi della collimazione impiegata , introducendo informazioni su di un importante fattore di protezione . 
nel caso di fascio uniforme , come in prima approssimazione si ha per la radiol med ( 2009 ) 114 : 595607 directly related to it , the effective dose . 
all the above were during hs [ 6 ] scans , that is , with a pitch of 6 equal to a pitch of 1.5 on single - detector - row machines . 
one limitation to dose reduction was the build of some patients , which obliged us to increase the kilovolts to allow for readable ct scans . the patient was placed prone on the ct table . 
un limite alla riduzione della dose stato lhabitus costituzionale di alcuni pazienti che ci ha costretto ad aumentare i kv per rendere leggibili le scansioni tc . il paziente stato posizionato prono sul lettino della tc . a seguire stato sistemato lateralmente al paziente lintensificatore di brillanza , utile per verificare il posizionamento ed indispensabile per controllare liniezione del cemento allo scopo di identificare la eventuale comparsa di leak extra - somatico vertebrale e / o vascolare e / o epi - durale . 
una volta posizionato il paziente si proceduto ad una prima scansione tc per individuare il / i metameri da trattare e si eseguita una scansione con un repere cutaneo per verificare la via di accesso . 
successivamente si proceduto allanestesia locale con lausilio di un agocannula spinale di 22 g di calibro iniettando lidocaina o , nel caso di vertebre toraciche , una miscela di lidocaina e cortisone ( kenacort ) , cos da ridurre al minimo leventuale disagio relativo allinfiammazione del plesso radicolare in caso di accesso parapeduncolare / intercostotrasversario . 
sono stati quindi inseriti gli aghicannula di calibro compreso fra 10 e 598 radiol med ( 2009 ) 114 : 595607 15 g allinterno del corpo vertebrale con accesso transpeduncolare o intercostotrasversario , aiutandosi nella progressione mediante un piccolo martello ortopedico . 
a questo punto , sotto guida radioscopica , stato infuso il cemento allinterno dei corpi vertebrali . in sala angiografica il paziente stato collocato in decubito prono sul lettino angiografico lasciando le impostazioni automatiche della macchina . 
il posizionamento e la progressione degli aghi da vertebroplastica nel soma , con accesso preferibilmente transpeduncolare , avvenuto sotto controllo radioscopico in antero - posteriore ( ap ) e in latero - laterale ( ll ) in modo da verificare la corretta progressione e il posizionamento dellago attraverso il peduncolo . 
in ap lago non deve uscire dal peduncolo , mentre la ll serve a verificare di quanto progredisce . la strumentazione impiegata nella valutazione di dose stata : camera a ionizzazione trasmissiva a doppio canale diamentor m4 - kdk ; pellicola di tipo gaf - chromic xr tipo t ; dosimetro unfors edd - 30 . 
tale camera radiotrasparente , ha unarea sensibile di 1515 cper la misura del dap il range compreso da 0 , 1 cgycm2 a 106 cgycm2 , la linearit la precisione e la riproducibilit della misura sono comprese entro l1% . 
per la misura del kerma in aria il range compreso fra 0 , 010 mgy e 10 gy ; la linearit e la precisione sono inferiori al 2 , 5% e la riproducibilit entro l1% . 
le caratteristiche principali risposta sono : bassa dipendenza della dallenergia ( < 3% per 80120 kv ) ; bassa dipendenza della risposta dal rateo medio di dose ; elevata risoluzione spaziale ; adeguata equivalenza con lacqua . le pellicole ( di dimensione 1515 cm ) sono state poste sulla finestra di uscita del tubo radiologico , essendo il valore della dap invariante rispetto alla distanza dal fuoco ; ponendo infatti la pellicola sulla finestra di uscita del tubo , piuttosto che sulla cute del paziente , la misura non influenzata dal contributo di radiazione retrodiffusa dal paziente stesso , non di intralcio alla procedura ed inoltre nella guida combinata la pellicola sarebbe stata anche impressionata dal fascio della tc . 
2 vertebroplastica di t12 eseguita con 80 kv e 40 ma , 5 mm di spessore , 30 mm / s lavanzamento del lettino in hs [ 6 ] e rotazione del tubo in 0 , 8 secondi . positioning and monitor the cement injection for possible extravertebral , and / or vascular and / or epidural leakages . 
an initial ct scan was performed to identify the vertebra or vertebrae to be treated , followed by a scan with radiopaque marker on the skin to locate the access route . 
local anaesthesia was achieved by injecting lidocaine or , in the case of thoracic vertebrae , a mixture of lidocaine and cortisone ( kenacort ) with the aid of a 22 - gauge spinal needle to minimise discomfort due to inflammation of the radicular plexus in the case of parapedicular / intercostal transverse approach . 
needle cannulas with 10to 15 - gauge calibre were subsequently inserted into the vertebral body with a transpedicular or intercoastal transverse approach and advanced with the aid of a small orthopaedic hammer . 
at this point , the cement was injected into the vertebral bodies under fluoroscopic guidance . in the angiography room , the patient was placed prone on the angiographic table and the procedure was carried out leaving the machines automatic settings . 
placement and advancement of the vertebroplasty needles , preferably inserted with a transpedicular approach , occurred under anteroposterior ( ap ) and laterolateral ( ll ) fluoroscopic guidance to check correct progression of the needle through the pedicle . 
on ap views , the needle must not be seen to exit from the pedicle , whereas the ll views serve to monitor its progression . the equipment used for dose measurements was as follows : diamentor m4 - kdk dual - channel transmission ion chamber ; type t gafchromic xr films ; unfors edd - 30 dosimeter . 
the chamber radiol med ( 2009 ) 114 : 595607 is radiolucent and has a sensitive area of 1515 cfor dap measurements , the range is between 0.1 cgyxcm2 and 106 cgyxcm2 , and the linearity , precision and reproducibility of measurements are in the range of 1% . 
their main features are low dependence of response on energy ( < 3% for 80120 kv ) , low dependence of response on average dose rate , high spatial resolution and adequate water equivalence . 
 the films ( 1515 cm ) were placed over the output window of the x - ray tube , since the dap value does not vary in relation to distance from the focus . 
in fact , with the film placed over the output window rather than over the patients skin , the measurement is not affected by the backscatter contribution , the film does not interfere with the procedure and , furthermore during procedures using combined ct and fluoroscopic guidance , the film would have been penetrated by the ct beathe irradiated films are read by a scanner at least 24 h following irradiation . from the calibration curve , one can derive the dap and point dose values based on film blackening . 
the values measured with the films and with the transmission ion chamber are comparable . to evaluate effective patient dose when using the image intensifier and the angiographic unit , we utilised the pcxmc15 software programme ( stuk , radiation and nuclear safety authority , helsinki , finland ) , which is based on the monte carlo method ( simulation of the process of energy deposition on a virtual phantom for a large number of incident photons ) and provides a value in terms of deep dose ( hp10 )  . 
the data required are voltage , current , fluoroscopy time , field size , projection , focus - to - skin distance and dap ( obtained from the ion chamber or film measurement )  . to evaluate effective patient dose when using ct , we utilised the ct - expo v1.5 programme , which is also based on the monte carlo method and provides a value of effective fig . 
i dati impiegati sono : tensione di utilizzo , ma , tempo di scopia , dimensione del campo , proiezione , distanza fra il fuoco del tubo radiogeno e la cute del paziente , dap ( ricavato dalla misura della camera a trasmissione o dalla pellicola )  . per la valutazione della dose efficace al paziente nellimpiego della tc si utilizzato il programma ct - expo v . 
i dati impiegati sono : tensione , ma , tempo di rotazione totale , pitch , spessore della slice e numero di slice , numero di serie acquisite e collimazione . 
di fisica sanitaria durante i controlli di qualit annuali sullapparecchiatura . le misurazioni sulla dose alloperatore sono state eseguite mediante un dosimetro unfors edd - 30 indossato dal radiologo interventista inizialmente sotto il camice piombato , poi si deciso che sarebbe stato meglio posizionarlo sopra ed eseguire le dovute correzioni per lo spessore del camice in quanto molto spesso il rateo di dose era inferiore alla minima soglia misurata dallo strumento , che quindi segnava zero ( tabella 1 )  . 
loperatore , essendo sottoposto a sorveglianza fisica per la radioprotezione , munito di dosimetro a film - badge a corpo intero , posizionato sotto il camice piombato , e dosimetro a bracciale a tld , poich tali dosimetri sono indossati dalloperatore non solo durante le procedure di vertebroplastica ma durante tutta lattivit lavorativa e pertanto la misura da essi fornita non impiegabile nella valutazione 600 radiol med ( 2009 ) 114 : 595607 dose in terms of deep dose . 
the data required are voltage , current , total rotation time , pitch , slice thickness and number of slices , number of serial scans and collimation . the ctdi value provided by the equipment is comparable with that measured experimentally with a pencil type ion chamber by the medical physics staff during the annual quality control procedures . measurements of operator dose were carried out with a unfors edd - 30 dosimeter . 
this was initially positioned under the interventional radiologists lead apron and subsequently , because the dose rate was very often lower than the minimum threshold measured by the instrument which showed zero it was decided to place it over the apron and to make the required adjustments for apron thickness ( table 1 )  . 
the dosimeter was placed on the chest to the le owing to continuous physical monitoring for radiation protection purposes , the operator wears a film - badge full - body dosimeter under the lead apron and a tld wrist dosimeter . however , because these dosimeters are worn throughout the working day and not only during vertebroplasty procedures , their measurements could not be used in our evaluation . 
nelle procedure che prevedono solo la guida radioscopica angiografica il paziente in posizione prona sul lettino , il tubo e posto in basso ad una distanza media fra il fuoco del tubo e il ricettore di immagini mediamente 120 cm : il paziente viene quindi investito dal fascio in proiezione antero - posteriore durante il posizionamento dellago e in latero - laterale nelliniezione del cemento ; il tubo e alla destra del paziente mentre loperatore alla sinistra . 
nelle procedure che invece impiegano luso combinato di tc ed intensificatore di brillanza , questultimo posizionato ortogonalmente al lettino tc ( e quindi allasse testa - piedi del paziente ) , il tubo in questo caso alla sinistra del paziente e loperatore a destra . 
the tube is on the patients right and the operator is on the lein procedures performed under combined ct and fluoroscopic guidance , the image intensifier is placed perpendicularly to the ct table ( hence to the headfoot axis of the patient ) , the tube is on the patients left and the operator on the right . 
the distance between the focus and the image intensifier is 100 c during the procedures , the operators wear 0.5 - mm pb - equivalent lead aprons . the unfors edd - 30 dosimeter consists of a 61122 mm sensor placed on a cable connected to a display unit . the sensor has a spherical response that can measure dose independently of the incident angle of radiation . 
 lo strumento ha dimensioni 829821 mm e pesa 200 g , non risulta quindi di minimo intralcio alloperatore . lintervallo di dose accumulata compreso fra 10 nsv e 9999 sv , il minimo valore di soglia del rateo di dose per far partire la misura 0 , 054 msv / h . 
 risultati per ogni paziente abbiamo preso nota delle impostazioni dellapparecchiatura tc come kv , ma , pitch , tempo di rotazione , spessore e numero di slice , collimazione ed il numero delle scansioni eseguite , mentre il contributo dellintensificatore di brillanza ( ib ) stato calcolato considerando i minuti di scopia , i kv , i ma , il fuoco del tubo radiogeno , la distanza fra la cute ed il tubo e calcolando la dose efficace tenendo conto delle misurazioni delle pellicole ( tabella 2 )  . in sala angiografica le misurazioni tenevano conto solo della dose prodotta dallangiografo , in questo caso per tabella 1 dose alloperatore s.c.d.u. 
neuroradiologia , guida radioscopica ds , deviazione standard ; adose alloperatore adattata allo spessore del camice ; t1 , durata dellirraggiamento ( min ) ; t2 , durata delle misurazioni ( min ) ; n.non misurabile 602 results for each patient , we took note of the ct settings , including kv , ma , pitch , rotation time , slice thickness and number , collimation and number of scans , whereas the contribution of the image intensifier was derived from fluoroscopy time , kv , ma , x - ray tube focus , focus - to - skin distance and by calculating the effective dose from the film measurements ( table 2 )  . radiol med ( 2009 ) 114 : 595607 oltre ai valori presi in considerazione per lib le misurazioni sono state calcolate separatamente in base alla proiezione , se ap o ll , e quindi i risultati sono stati sommati ( tabella 3 )  . data lampiezza del campione preso in esame finora abbiamo analizzato i dati applicando il test t di student che ha dimostrato come non ci sia una differenza statisticamente significativa per quanto riguarda la dose al paziente in corso di vertebroplastica quando eseguita sotto table 2 patient dose during vertebroplasty with combined computed tomography ( ct ) and fluoroscopic guidance vertebra / e kv t tot ctdi no . 
bcorrisponde al paziente 2 della tabella 3 trattato per crolli successivi con entrambe le metodiche radiol med ( 2009 ) 114 : 595607 measurements in the angiographic room took into account only the dose produced by the angiographic unit . 
in this case , however , in addition to the values considered for the image intensifier , determinations were made separately for the ap and ll projections , and the results were summed ( table 3 )  . given the size of the sample studied to date , we analysed the data with students t test , which showed that patient dose did not differ significantly between vertebroplasty performed with fluoroscopic guidance alone and with combined ct and fluoroscopic guidance [ t = 0.9726 ; p = 0.3436 with 95% confidence interval ( ci ) ] , whereas operator dose was substantially lower during vertebroplasty performed under combined ct and fluoroscopic guidance ( t = 3.5674 , p = 0.0022 with 95% ci )  . 
this change did not , however , affect the substantial difference in operator dose in favour of combined ct and fluoroscopic guidance ( t = 3.5341 , p = 0.0024 with 95% ci )  . because the ct settings were modified during the procedures , we reanalysed the data with students t test after creating two groups with a cutoff value of 120 kv for ct voltage . 
however , no statistically significant difference emerged between highand low - voltage settings ( t = 2.0956 , p = 0.0656 with 95% ci )  . for each series of values , we then calculated the ratio of dap to effective dose ( and effective dose to dap ) , the mean values and related standard deviations . 
it was particularly interesting to find that the linear coefficient of the straight line was comparable with the mean value of ratio of effective test t di student i dati creando due gruppi e ponendo come cut - off i 120 kv di tensione della tc . 
sono stati quindi posti su grafico i valori di dap ( ascisse ) e di dose efficace ( ordinate ) , interpolando i dati con una correlazione di tipo lineare . 
neuroradiologia , guida radioscopica paziente note dose sv rateo sv / h i valori adattati sono sottolineati ds , deviazione standard ; adose alloperatore adattata allo spessore del camice ; t1 , durata dellirraggiamento ( min ) ; t2 , durata delle misurazioni ( min ) ; n.m. , non misurabile dose to dap . 
 discussione discussion in our series , fluoroscopy time has less variability than that reported in the literature [ 1 ] ( 2.110.53 min for combined guidance and 4.228.4 for fluoroscopic guidance ) , whereas mean fluoroscopy time during procedures with fluoroscopic guidance alone was 10.22 min and thus in line with previous reports [ 2 ]  . 
 our study shows that ct guidance is a valuable alternative for vertebroplasty procedures , as patient dose , generally believed to be too high , can by taking appropriate measures be lowered to similar levels to those imparted in the angiognella casistica presentata il tempo della scopia ha una variabilit molto inferiore rispetto a quanto riportato in letteratura [ 1 ] ( fra 2 , 1 e 10 , 53 minuti per la guida combinata e fra 4 , 2 e 28 , 4 per lesclusiva guida radioscopica ) , mentre il tempo medio di scopia sotto esclusiva guida radioscopica , di 10 , 22 minuti , assolutamente in linea con quanto riportato in letteratura [ 2 ]  . 
 da questo studio si evince come la guida tc sia una valida alternativa per lesecuzione della vertebroplastica in quanto la dose al paziente , ritenuta per lo pi troppo alta , in realt , con gli opportuni accorgimenti , analoga a quella cui il paziente esposto durante una seduta in sala angiografica . 
per quanto riguarda loperatore risultato che la dose , nel caso di procedura eseguita in sala tc , inferiore a quella eseguita in sala angiografica con una differenza statisticamente significativa ( t = 3 , 5674 p = 0 , 0022 con i.c. al 95% ) ; si deve comunque segnalare lesiguit del 606 radiol med ( 2009 ) 114 : 595607 y = 0 , 119x r2 = 0 , 5043 effective dose / dap linear ( effective dose / dap ) y = 0 , 1873x r2 = 0 , 954 relationship dap / effective dose linear ( relationship dap / effective dose ) 10 , 0 15 , 0 20 , 0 25 , 0 30 , 0 35 , 0 dap ( mgyxcm2 ) fig . 
however , it is important to note that the patient sample was small and that in some cases , the operator dose was lower than the minimum threshold detectable by the equipment . 
 further campione ed il fatto che in alcuni casi la dose alloperatore era inferiore al minimo rilevabile dallapparecchiatura . ulteriori studi con un campione di maggiori dimensioni sono pertanto indispensabili per poter individuare leventuale vantaggio della guida tc con bassa tensione ed intensit nel ridurre la dose al paziente . analogamente necessario effettuare un campione pi radiol med ( 2009 ) 114 : 595607 studies on larger patient series are therefore needed to determine the possible benefit of low - voltage , low - current ct guidance in reducing patient doses . likewise , more measurements of operator exposure by placing the dosimeter over the lead apron and correcting the results for apron thickness are required to validate the reduction in dose during pvp under combined ct and fluoroscopic guidance . 
 in view of the quadratic dispersion of the beam , another factor to be considered is the possibility of using devices that allow cement injection without requiring the operator to be in direct contact with the patient or in close proximity to the direct bea numeroso di misurazioni dellirraggiamento alloperatore ponendo il dosimetro sopra il camice ed eseguendo le dovute correzioni per lo spessore del camice stesso al fine di poter confermare o meno la reale riduzione di dose nellesecuzione di pvp sotto guida combinata tc e radioscopica . 
da questo punto di vista anche importante valutare il diverso contributo del tipo di apparecchiature utilizzate ( intensificatori di brillanza , angiografi portatili , applicazione di laser mobili ) , oltre a quello delle possibili modifiche sulle impostazioni delle apparecchiature stesse ; ad esempio : preferire una radioscopia che tendenzialmente usa ma minori di unaltra ( per esempio fluoro1 o fluoro3 negli angiografi philips ) , utilizzare la scopia pulsata al posto della continua durante linfissione degli aghi . 
this study was performed to validate a highresolution whole - body magnetic resonance angiography ( mra ) protocol with parallel imaging and biphasic administration of a single bolus of contrast agent in the preliminary assessment of systemic atherosclerotic burden in patients referred for endovascular procedures . 
forty patients referred for endovascular treatment of atherosclerotic disease of the carotid arteries ( n = 23 ) , peripheral vessels ( n = 14 ) or aorta ( n = 3 ) on the basis of previous clinical and diagnostic examinations underwent high - resolution whole - body mra at 1.5 t with 3d spoiled gradient recalled echo ( gre ) sequences , featuring parallel imaging acquisition technique with 2 acceleration factor . 
ottimizzare un protocollo angio - rm whole - body ( wb ) ad alta risoluzione con tecnica di imaging parallelo e somministrazione bifasica di un singolo bolo di mezzo di contrasto ( mdc ) nello studio della patologia aterosclerotica sistemica ed effettuare una valutazione preliminare del potenziale diagnostico in pazienti candidati a trattamento endovascolare di lesioni arteriose steno - occlusive . 
il mdc stato somministrato con un protocollo di iniezione bifasica a singolo bolo : 10 ml ad una velocit di iniezione di 1 ml / s seguiti da 10 ml alla velocit di 0 , 5 ml / s di gd - bopta . 
la presenza o lassenza di patologia aterosclerotica stata valutata da radiol med ( 2009 ) 114 : 538552 consensus ; segments were classified as having clinically significant disease ( 50% stenosis or an aneurysmal dilatation ) or no significant disease ( < 50% stenosis )  . 
the presence of stenoocclusive disease , determined at all segments , was compared with findings on digital subtraction angiography ( dsa ) , which were interpreted by a third independent reader . 
sensitivity , specificity and concordance of whole - body mra findings with dsa were calculated , and receiver operating characteristic ( roc ) analysis was performed for all vascular territories . 
a total of 1 , 680 arterial segments was evaluated ; 138 ( 8.3% ) were affected by atherosclerotic alterations . carotid lesions were confirmed in 23 patients ( 34 segments ) , involvement of peripheral vessels in 14 ( 57 segments ) and abdominal aneurysms in three . 
subclinical atherosclerotic lesions were evidenced in 25 patients , involving carotid arteries ( 12 segments ) , peripheral vessels ( 21 segments ) and abdominal aorta ( one segment )  . 
the subclinical detection of the total atherosclerotic burden has potential implications for secondary care in this population . due osservatori in consenso ; i segmenti sono stati classificati come patologici ( stenosi 50% o dilatazioni aneurismatiche ) o non patologici ( < 50% )  . 
la capacit di individuare lesioni asintomatiche ha un potenziale nellapproccio di prevenzione secondaria . keywords atherosclerosis mr angiography wholebody imaging systemic vessels parole chiave aterosclerosi angio - rm imaging wholebody vasi sistemici introduction introduzione atherosclerosis is a ubiquitous , multiterritorial arterial disease involving the large vessels and the peripheral circulation whose clinical manifestations lead to adverse social and personal health outcomes in a significant portion of the western population [ 1 , 2 ]  . 
imaging plays a key role in staging the disease and planning appropriate treatment . however , despite the multiterritorial distribution of atherosclerosis , the diagnostic approach relying on conventional modalities such as colour doppler ultrasound ( us ) , computed tomography angiography ( cta ) and conventional angiography has always been limited to investigating symptomatic vascular territories only . 
more recently , magnetic resonance angiography ( mra ) has been successfully proposed for the safe and comprehensive evaluation la malattia aterosclerotica ( ma ) una patologia polidistrettuale con distribuzione ubiquitaria che coinvolge i grossi vasi e la circolazione periferica , con manifestazioni cliniche correlate ad evoluzioni socio - sanitarie sfavorevoli in una quota significativa della popolazione occidentale [ 1 , 2 ]  . 
tuttavia , nonostante la distribuzione polidistrettuale della ma , lapproccio diagnostico , attraverso lutilizzo dei tradizionali metodi quali leco - colordoppler , langio - tc e langiografia convenzionale , stato lungamente confinato ai soli distretti vascolari sintomatici . 
pi di recente langio - rm stata proposta con successo per una sicura e completa valutazione del danno da ma a livello dei 540 radiol med ( 2009 ) 114 : 538552 imaging techniques [ 68 ] and of atherosclerotic burden of all arteries in the body ( wholebody technique ) [ 35 ]  . 
the aim of our study was to validate a high - resolution , whole - body mra study protocol with parallel imaging technique and sequence acquisition during the biphasic administration of a single bolus of a highrelaxivity interstitial contrast agent by performing a preliminary evaluation of its diagnostic accuracy in patients referred for endovascular procedures for atherosclerotic disease . vasi arteriosi di tutto il corpo ( tecnica whole - body ) [ 35 ]  . gran parte di questo successo dovuto soprattutto ai progressi tecnologici nellutilizzo dei sistemi integrati di bobine , delle tecniche di imaging parallelo [ 68 ] ed in parte dei mdc intravascolari [ 911 ]  . 
lobiettivo del nostro studio stato quello di validare un protocollo desame angio - rm whole - body ad alta risoluzione con tecnologia di imaging parallelo e sequenze acquisite durante la somministrazione bifasica di un unico bolo di mdc interstiziale ad alta relassivit , effettuando una valutazione preliminare dellaccuratezza diagnostica in pazienti candidati a trattamento endovascolare per ma . materials and methods population materiali e metodi popolazione between november 2006 and november 2007 , we recruited 40 subjects ( 25 men and 15 women ; mean age 675 years , age range 3284 years ) referred to our hospitals department of vascular surgery for endovascular treatment under angiographic guidance . 
twenty - three patients ( 13 men and 10 women ) had one or more carotid artery lesions , with colour doppler us evidence of a haemodynamically significant and symptomatic stenosis ( 12 drop attacks , 11 minor transient ischaemic attacks )  . 
fourteen patients ( 10 men and 4 women ) had one or more lesions of the peripheral circulation of the lower limbs , so the indication for treatment had been provided by the clinical findings ( ankle - brachial pressure index < 0.90 , refractory claudication or critical ischaemia ) and colour doppler us evidence of haemodynamically significant stenoses . exclusion criteria were general contraindications for mr imaging ( pacemaker or implantable medical devices , metallic fragments , claustrophobia ) , angiography ( congestive heart failure ) and administration of iodineor gadolinium - based contrast agents ( allergy , serum creatinine levels > 1.5 mg / dl )  . 
the study was granted the approval of our institutions ethics committee . dal novembre 2006 al novembre 2007 sono stati reclutati 40 soggetti ( 25 uomini e 15 donne con et media di 675 anni , range det 3284 anni ) ricoverati presso il reparto di chirurgia vascolare del nostro istituto e candidati al trattamento endovascolare sotto guida angiografica per ma . ventitre pazienti ( 13 uomini e 10 donne ) presentavano una o pi lesioni carotidee per cui lindicazione al trattamento era stata posta in seguito alla documentazione con eco - colordoppler di stenosi emodinamicamente significativa e sintomatica ( 12 drop - attack , 11 tia minori )  . 
tre pazienti ( 2 uomini e 1 donna ) presentavano una dilatazione aneurismatica dellaorta addominale per cui lindicazione al trattamento era stata posta in seguito alla diagnosi effettuata con esami tc delladdome eseguiti per altra motivazione ( controllo oncologico )  . 
quattoridici pazienti ( 10 uomini e 4 donne ) presentavano una o pi lesioni a livello del circolo periferico degli arti inferiori per cui lindicazione al trattamento era stata posta sulla base di dati clinici ( indice pressorio sistolico braccio - caviglia inferiore a 0 , 90 , claudicatio non responsiva al trattamento o ischemia critica ) e con esame eco - colordoppler positivo per stenosi emodinamicamente significative . sono stati esclusi dallo studio tutti i pazienti con controindicazioni generali allesame rm ( pace maker o dispositivi medici impiantabili , frammenti metallici , claustrofobia ) , allangiografia ( scompenso cardiaco congestizio ) ed alla somministrazione di mdc iodato o a base di gadolinio ( allergia , livelli di creatinina sierica > 1 , 5 mg / dl )  . 
lo studio ha ricevuto lapprovazione da parte del comitato etico del nostro istituto . all mra studies were conducted on a high - performance 1.5 - t scanner ( magnetom avanto , siemens medical system , erlangen , germany ) with gradient strength of 45 mt / m2 and slew rate of 200 t / m / s . 
the scanning protocol involved the use of the integrated moving - table system and evaluation of four anatomical stations : head / neck , thorax / abdomen , pelvis / thigh , calf / foot . 
the optimal delay between contrast injection and sequence acquisition was calculated by using the bolus - tracking technique , with the start of image acquisition synchronised with the arrival of contrast material in the left cardiac cavities . 
the precontrast images were automatically subtracted from the postcontrast images to increase the contrast between the vasculature and the background . digital subtraction angiography all patients underwent the scheduled angiographic endovascular procedure to treat the previously known vascular lesions . 
all examinations were conducted on a digital subtraction angiography ( dsa ) unit ( integris v5000 , philips medical systems , best , the netherlands )  . in patients undergoing treatment of epiaortic vessels , a transfemoral approach with a 5 - f catheter was used . 
the first injection of contrast agent was given at the aortic arch level , and images were obtained in the two projections ( left antero - oblique and right antero - oblique ) to identify the common carotid , vertebral and subclavian arteries . 
after selective catheterisation of the common carotid arteries , images were obtained in the anteroposterior , lateral and oblique directions ( 45 and + 45 ) , and the intracranial lassetto angio - whole - body ( tecnologia avanto , siemens medical system , erlangen , germania ) con intensit dei gradienti di 45 mt / m2 e tempo di risalita di 200 t / m / s . 
il protocollo di scansione stato impostato utilizzando il sistema integrato di scorrimento continuo del lettino porta - paziente ed ha previsto la valutazione di 4 segmenti anatomici : testa - collo , toraceaddome , pelvi - coscia , gamba - piede . 
le immagini sequenziali pre - contrastografiche sono state ottenute in senso caudo - craniale con scorrimento continuo del lettino porta - paziente , utilizzando sequenze 3d flash ( fast low angle shot ) con integrated parallel acquisition technique ( ipat ) ottimizzate per unelevata risoluzione spaziale e per breve tempo di acquisizione ( tr 3 , 5 ms , te 1 , 18 ms , fa 30 , voxel size 1 , 3 mm0 , 9 mm0 , 9 mm , matrice 256512 , ta 16 s , fattore ipat2 ) secondo sezioni coronali . 
il protocollo stato ripetuto in senso cranio - caudale dopo una singola somministrazione bifasica di mdc tramite iniettore a doppia testata : 0 , 2 mmol / kg di gd - bopta sono stati somministrati in singolo bolo con protocollo di iniezione bifascio ( prima fase di iniezione ad 1 ml / s e seconda fase a 0 , 5 ml / s ) con bolus - chaser di 25 ml di soluzione fisiologica alla velocit di 0 , 5 ml / s . 
il ritardo ottimale tra liniezione del contrasto e lacquisizione stato calcolato con la tecnica del bolus - tracking , con avvio sincronizzato allarrivo del mdc in corrispondenza delle cavit cardiache di sinistra . 
le immagini pre - contrastografiche sono state automaticamente sottratte da quelle contrastografiche , incrementando il contrasto tra il vaso e il background . angiografia con sottrazione digitale in tutti i pazienti stato eseguito il trattamento programmato delle lesioni vascolari note in anamnesi attraverso procedura endovascolare sotto guida angiografica . 
la prima iniezione di contrasto stata condotta a livello dellarco aortico e le 542 radiol med ( 2009 ) 114 : 538552 circulation was visualised in the anteroposterior and lateral projections . 
in all patients , we used a nonionic iodinated contrast agent ( iomeron 300 , bracco , milan , italy ) administered at a dose of 20 ml and flow rate of 20 ml / s for images at the level of the aortic arch and 610 ml at a flow rate of 6 ml / s for selective catheterisation at the level of the common carotids . 
all examinations were performed with a field of view ( fov ) of 33 cm , a matrix of 1.0241.024 , with a spatial resolution of 0.320.32 min patients undergoing treatment of peripheral vessels , we used a transfemoral approach with a 4or 5 - f catheter , depending on the patients characteristics . 
contrast material was administered at a dose of 15 ml and flow rate of 10 ml / s for images at the femoral level and 810 ml at a rate of 6 ml / s for selective catheterisation , for a total of 70 ml ( range 6080 ml ) per patient . examinations were carried out with a fov of 33 cm , a matrix of 1.0241.024 , with a spatial resolution of 0.320.32 mfinally , in patients undergoing treatment of an abdominal aortic aneurysm , we used a transfemoral approach with a 5 - f catheter and administration 30 ml of contrast medium at a flow rate of 25 ml / s , obtaining anteroposterior and laterolateral projections with a fov of 33 cm , and matrix of 1.0241.024 and a spatial resolution of 0.320.32 m postprocessing the mra images were evaluated in real time on an independent workstation ( aquarius , terarecon inc . , san mateo , ca , usa ) dedicated to the 3d reconstruction of vascular data sets . 
to evaluate the anatomy and degree of vascular stenosis and to study the aneurysms , the following reconstruction algorithms were used : maximum intensity projection ( mip ) to gain an overview of the various vascular territories , multiplanar reformation ( mpr ) and curved mpr to measure the degree of stenosis . image assessment and statistical analysis the mra studies were reviewed first , followed by the dsa studies after a 1 - week interval . 
mra results were evaluated in consensus by two radiologists with 8 and 15 years of experience , respectively , in vascular diagnostics ; both observers were unaware of the diagnostic indication for the mra study . 
all dsa examinations were evaluated by an successive immagini , secondo le due proiezioni ( sinistra antero - obliqua e destra antero - obliqua ) , per individuare le carotidi comuni , le arterie vertebrali e le arterie succlavie . dopo una cateterizzazione selettiva delle carotidi comuni sono state ottenute immagini in antero - posteriore , laterale e nelle direzioni oblique ( 45 e + 45 ) e il circolo intracranico stato visualizzato in antero - posteriore e nelle proiezioni laterali . 
in tutti i pazienti stato utilizzato un mdc iodato non ionico ( iomeron 300 , bracco , milano , italia ) al dosaggio di 20 ml con velocit di 20 ml / s per le immagini a livello dellarco aortico e 610 ml sono stati utilizzati , con un flusso di 6 ml / s , per la cateterizzazione selettiva a livello delle carotidi comuni . 
ogni esame stato condotto con un fov di 33 cm , una matrice di 1 , 0241 , 024 , con una risoluzione spaziale di 0 , 320 , 32 m nei pazienti candidati a trattamento di ma dei vasi del circolo periferico stato usato un approccio transfemorale con un catetere da 4 f o 5 f , in base alle caratteristiche del paziente . 
il mdc stato somministrato al dosaggio di 15 ml con velocit di 10 ml / s per le immagini a livello femorale e di 810 ml con velocit di 6 ml / s per la cateterizzazione selettiva , per totale di 70 ml ( range 6080 ml ) di mezzo di contrasto per ciascun paziente . 
per lesame si usato un fov di 33 cm , una matrice di 1 , 0241 , 024 , con una risoluzione spaziale di 0 , 320 , 32 minfine nei pazienti candidati a trattamento per patologia aneurismatica dellaorta addominale stato usato un approccio transfemorale con un catetere da 5 f e somministrazione di mdc al dosaggio di 30 ml con velocit di 25 ml / s , ottenendo proiezioni antero - posteriori e laterolaterali con un fov di 33 cm e matrice di 1 , 0241 , 024 , ad una risoluzione spaziale di 0 , 320 , 32 m post - processing le immagini angio - rm sono state valutate in tempo reale durante la refertazione utilizzando una workstation indipendente ( aquarius , terarecon inc . , san mateo , ca , usa ) dedicata per la ricostruzione volumetrica di datasets di esami vascolari . 
per valutare lanatomia ed il grado di stenosi vascolare ed effettuare lo studio degli aneurismi sono stati impiegati i segeuenti algoritmi di ricostruzione : il mip ( maximum intensity projection ) per la valutazione panoramica dei vari distretti vascolari , lmpr ( multiplanar reformatted projection ) e il curve - mpr per la misurazione del grado di stenosi . radiol med ( 2009 ) 114 : 538552 independent reader unaware of the results of mra at the time of reporting . 
image and diagnostic quality was judged according to a five - point scale : 0 = nondiagnostic ; 1 = suspected diagnosis but insufficient data ; 2 = adequate for diagnosis ; 3 = good - quality images for diagnosis ; 4 = excellent images with definitive diagnosis . segments were considered pathological if they showed a wall dilatation with aneurysmal features or a > 50% reduction in diameter and nonpathological if the stenosis was < 50% . 
in addition , receiver operating characteristic ( roc ) curve analysis was carried out to validate the sensitivity and specificity of mra relative to dsa in all four vascular territories . 
with regard to the segments studied with mra alone , we evaluated the number , severity and prevalence of atherosclerotic lesions . analisi delle immagini e statistica la revisione stata effettuata partendo dallangio - rm e procedendo dopo un intervallo di una settimana con gli esami angiografici . 
i risultati dellangio - rm sono stati valutati in consenso da due radiologi con 8 e 15 anni desperienza nella diagnostica vascolare ; entrambi gli osservatori non erano a conoscienza dellindicazione diagnostica allesame angio - rm . 
la qualit iconografica e diagnostica stata giudicata utilizzando una scala con cinque livelli : 0 = non diagnostico ; 1 = diagnosi sospetta , ma con dati insufficienti a stabilirla ; 2 = sufficiente per la diagnosi ; 3 = immagini di buona qualit per fare diagnosi ; 4 = immagini di qualit eccellente con diagnosi definitiva . 
sono stati considerati patologici tutti quei segmenti che presentavano una dilatazione della parete con caratteristiche aneurismatiche o una riduzione di calibro > 50% e non patologici quelli che avevano stenosi < 50% . 
all mra examinations and angiographic procedures were well - tolerated ; during the days following the examinations , there were no changes in blood chemistry attributable to the administration of contrast material . 
room time for mra studies was 257 min , including patient preparation and positioning ; effective machine time was 135 m room time for the angiographic procedures limited to the diagnostic phase alone without considering stent deployment or angioplasty procedures was 526 min including patient preparation . 
 quantitative assessment of vascular damage for the thorax / abdomen , 3.15 a total of 1 , 680 arterial segments were evaluated , 138 ( 8.3% ) of which were considered pathological ( table 2 )  . the mean quality rating of mra images was 3.48 for the head / neck , 3.56 pelvis / thigh and 2.85 for calf / foot . 
in six patients , image quality was marred by motion artefacts ( n = 4 , carotid ) , incorrect timing ( n = 1 , carotid ) or early venous filling due to the presence of trophic lesions ( n = 2 , tibial )  . 
the total number of images with suboptimal image quality was 49 ( 2% : 27 leg segments , 12 thigh segments , 8 abdominalsplanchnic segments , 2 carotids ) , of which five had a quality rating of 0 , 15 of 1 and 29 of 2 . 
la concordanza statistica tra le due modalit nella valutazione della stenosi stata quantificata utilizzando il test t di student : un valore di p < 0 , 05 stato considerato statisticamente significativo . 
lanalisi statistica stata effettuata con il software statistico spss 13.0 statistical package ( chicago , ill , usa )  . risultati lintervallo medio tra lesecuzione degli studi angio - rm e le procedure angiografiche stato di 42 giorni . 
tutti gli esami angio - rm e le procedure angiografiche sono state ben tollerate ; nei giorni successivi agli esami non si sono evidenziate alterazioni degli esami ematochimici riconducibili alla somministrazione di mdc . 
il room - time per gli esami angiorm stato di circa 257 minuti , inclusa la preparazione ed il posizionamento del paziente ; il tempo - macchina effettivo stato di circa 135 minuti . 
il room - time per le procedure angiografiche , limitatamente allaspetto diagnostico ( non considerando quindi il posizionamento di stent o gli interventi di angioplastica ) , stato di 526 minuti inclusa la preparazione del paziente . 
il tempo impiegato in media per il post - processing degli esami angio - rm stato di 72 minuti . il tempo impiegato in media per la valutazione delle immagini stato di 155 minuti per gli esami angio - rm e di 83 min per quelli angiografici . 
 valutazione quantitativa del danno vascolare sono stati valutati un totale di 1680 segmenti arteriosi , con un totale di segmenti considerati patologici pari a 138 ( 8 , 3% ) ( tabella 2 )  . 
la qualit media delle immagini angiorm stata di 3 , 48 nel distretto testa - collo , 3 , 56 nel distretto torace - addome , 3 , 15 nel distretto pelvi - coscia e 2 , 85 nel distretto gamba - piede . 
in 6 pazienti si verificata una degradazione della qualit delle immgini dovuta ad artefatti da movimento ( n = 4 , carotidi ) , errata valutazione del timing ( n = 1 , carotidi ) , precoce riempimento venoso per presenza di lesioni trofiche ( n = 2 , tibiali ) ; il totale di segmenti in cui la qualit delle immagini risultata sub - ottimale stato di 49 ( 2% , nellordine 27 segmenti di gamba , 12 segmenti di coscia , 8 segmenti addominali - splancnici , 2 carotidi ) , di cui 5 con livello di qualit pari a 0 , 15 con livello di qualit pari a 1 e 29 con livello di qualit pari a 2 . 
in another two cases ( six segments ) , angiography and mra were discordant in their evaluation of lesions affecting the peripheral vasculature ( > 50% stenoses of calf vessels missed at mra )  . 
unanalisi basata su curve roc ( tabella 3 ) stata utilizzata per calcolare sensibilit e specificit dellangio - rm nella valutazione delle lesioni con stenosi superiore al 50% , i valori ottenuti sono stati rispettivamente di 95% e 97% nel distretto testa - collo ( auc = 0 , 948 ) , 100% e 100% nel distretto torace - addome ( auc = 1 ) , 98% e 97% nel distretto pelvi - coscia ( auc = 0 , 973 ) e 84% e 88% nel distretto gamba - piede ( auc = 0 , 856 )  . 
in 2 casi ( 2 segmenti ) vi stata una sottostima di lesioni carotidee da parte dellangio - rm ( stenosi > 85% valutate come 70% ) , uno di questi con qualit delle 546 fig . 
1a - d a 67 - year - old man with high blood pressure and hypercholesterolaemia referred for endovascular procedure on peripheral vessels for leriche - fontaine stage ii intermittent claudication ( fatigue and stress pain of the proximal legs , walking autonomy < 200 m )  . 
whole - body magnetic resonance angiography ( mra ) ( a ) showed a parietal ulcer of the aortic bifurcation ( asterisk ) with severe stenosis of the left common iliac artery ( c )  . 
1a - d uomo di 67 anni , iperteso , dislipidemico , candidato procedure endovascolare a livello del circolo periferico per trattamento di claudicatio intermittens al ii stadio di leriche - fontaine ( dolore sotto sforzo , autonomia inferiore ai 200 metri )  . 
ten of these patients ( six with carotid lesions , two with iliac artery lesions , one with femoral lesions and one with calf - vessel lesions ) were scheduled for additional short - term endovascular treatments to prevent the lesions identified on mra from becoming clinically manifest . 
because the lesions requiring treatment on the basis of mra evidence had not been previously studied in this subgroup of patients , the radiol med ( 2009 ) 114 : 538552 immagini sub - ottimale . 
in altri 2 casi ( 6 segmenti ) vi stata una valutazione non concorde tra angiografia ed angio - rm per quanto riguarda lesioni del distretto periferico ( stenosi > 50% dei vasi di gamba non rilevate allangio - rm )  . 
per quanto riguarda i segmenti studiati unicamente con langio - rm sono state evidenziate lesioni da ma ( stenosi vascolari > 50% o dilatazioni patologiche della parete vascolare ) in 25 pazienti su 40 ( 62 , 5% )  . 
in particolare sono state evidenziate lesioni carotidee misconosciute in 10 casi ( 40% del totale , range di stenosi 60%90% , valore medio 72% , totale segmenti = 12 ) , stenosi significative delle arterie iliache in 7 casi ( 28 % , totale segmenti = 12 ) , stenosi dei vasi femorali in 3 casi ( 12% , totale segmenti = 8 ) , stenosi dei vasi di gamba in 4 casi ( 16% , totale segmenti = 11 ) ed 1 caso di aneurisma dellaorta addominale ( 4% , totale segmenti = 1 ) di dimensioni < 5 cm . in 10 di questi pazienti ( 6 con lesioni delle carotidi , 2 con lesioni delle arterie iliache , 1 con lesioni dei vasi femorali ed 1 con lesioni dei vasi di gamba ) stato programmato unulteriore trattamento endovascolare a breve termine allo scopo di prevenire le manifestazioni cliniche delle lesioni individuate allangio - rm . 
in questo sottogruppo dei pazienti , non essendo state precedentemente studiate le lesioni per cui veniva richiesto il trattamento sulla base dei dati angio - rm , stato effettuato un completamento diagnostico con angio - tc e con ecocolor - doppler ( questultimo nelle carotidi , nei vasi femorali e di gamba ) per fornire unulteriore validazione dei reperti e consentire un planning pre - trattamento pi approfondito . discussione il nostro studio ha permesso di evidenziare come una tecnica angio - rm whole - body allo stato dellarte renda possibile lidentificazione di lesioni misconosciute in pazienti candidati a trattamento endovascolare per ma . 
la recente introduzione delle tecniche di imaging parallelo , supportata dallimpiego di magneti ad alto campo con gradienti altamente performanti e dallavvento delle varie tecniche di bolus - tracking , pu esser considerata un punto di svolta nellevoluzione clinica dellangio - rm : oggi di fatto possibile eseguire un studio whole - body in pochi minuti e con unelevata accuratezza diagnostica . 
tuttavia alcuni distretti vascolari , fra cui gamba e piede dove strutture arteriose di calibro ridotto decorrono in stretta vicinanza di vasi venosi che possono contaminare e degradare lintensit di segnale , presentano ancora delle difficolt nellimaging con angio - rm . 
severe stenosis of the right internal carotid was demonstrated at both digital subtraction angiography ( dsa ) and magnetic resonance angiography ( mra ) ( b , c , arrows )  . 
whole - body mra ( a ) also showed multiple and ulcerated subclinical lesions at the level of the infrarenal aorta and the origin of left common iliac artery ( d , e , arrowheads ) fig . 
oltre la severa riduzione di calibro dellarteria carotide interna destra dimostrata sia allesame angiografico ( b , c , frecce ) che allangiorm , lo studio wb ( a ) ha inoltre evidenziato la presenza di lesioni aterosclerotiche sconosciute ed in gran parte ulcerate a livello dellaorta sottorenale e dellarteria iliaca comune sinistra in sede ostiale ( d , e , punte di freccia )  . 
nella nostra esperienza un fattore di accelerazione ( ipat ) pari a 2 stato sufficiente a ridurre drasticamente il tempo di acquisizione a livello di tutti i segmenti , con maggior beneficio in corrispondenza dei distretti periferici , senza tuttavia limitare la la configurazione utilizzata ha risoluzione spaziale : permesso limpiego di valori di matrice maggiori rispetto a quelli proposti sia negli iniziali studi di angio - rm wholebody [ 4 ] che in lavori pi recenti [ 12 ]  . 
i parametri alla base della fattibilit di questo approccio sono rappresentati pricipalmente dallutilizzo di elementi di bobina con elevat sensibilit e multipli canali indipendenti per la ricezione del segnale associato allelevata performance dei gradienti . inoltre la tecnologia autocalibrante delle bobine evita eventuali interferenze tra lutilizzo dellimaging parallelo e lo spostamento del tavolo durante le varie fasi dellacquisizione . 
rispetto alle sequenze di un protocollo convenzionale , lutilizzo dellipat pu condurre a discreti fenomeni di riduzione del rapporto segnale / rumore , maggiormente evidente in corrispondenza dl circolo periferico ; nella nostra esperienza tuttavia questo inconveniente stato diagnostic workup was completed with cta and colour doppler us ( the latter for the carotids , femoral and calf vessels ) to confirm the findings and permit more in - depth preprocedural planning . discussion our study allowed us to demonstrate that a state - of - the - art whole - body mra technique is able to detect unknown lesions in patients referred for endovascular treatment of atherosclerotic lesions . 
the recent introduction of parallel imaging techniques , supported by the use of high - field magnets with high - performance gradients and the advent of bolus - tracking techniques , may be considered a breakthrough in the clinical evolution of mra . 
some vascular territories , however , including the calf and foot where small arteries run in close proximity to veins that may contaminate and degrade signal intensity , still represent a challenge for mra imaging . 
in these cases , the use of sequences with high spatial resolution , optimal scan timing and high - relaxivity contrast media may greatly improve 548 radiol med ( 2009 ) 114 : 538552 fig . 
whole - body magnetic resonance angiography ( mra ) ( a ) demonstrates severe stenosis of both internal carotid arteries confirmed on digital subtraction angiography ( dsa ) images obtained during the interventional procedure ( b - e , arrows )  . 
in our experience , an acceleration factor ( ipat ) of 2 was sufficient to dramatically reduce acquisition time in all segments with more pronounced benefits in the peripheral vessels without limiting spatial resolution . 
the configuration allowed the use of higher matrix values compared with those proposed by early studies on whole - body mra [ 4 ] and more recent studies [ 12 ]  . 
compared with the sequences of a conventional protocol , the use of ipat may lead to lower signal - to - noise ratio , which is more evident in the peripheral circulation . 
in our experience , this trascurabile dal punto di vista degli effetti sullaccuratezza diagnostica , soprattutto grazie allutilizzo del gd - bopta , un mdc con caratteristiche di relassivit ideali [ 13 ] per gli studi vascolari di primo passaggio ( legame debole con lalbumina plasmatica ) gi impiegato con successo [ 6 ] nei protocolli whole - body . 
nel nostro studio stato utilizzato un approccio con singola iniezione bifasica del mdc , boluschaser e timing calcolato con tecnica di bolus - tracking : nei lavori precedenti [ 47 ] stata generalmente impiegata uniniezione bifasica , pre - miscelazione tra mdc e soluzione fisiologica e timing calcolato con tecnica di test - bolus , oppure stato proposto un approccio con due iniezioni separate di mdc [ 8 ]  . 
 [ 12 ] con risultati sostanzialmente sovrapponibili in termini di qualit ed immagini.unulteriore accuratezza diagnostica delle radiol med ( 2009 ) 114 : 538552 table 3 receiver operating characteristic ( roc ) curve analysis . 
excellent results were also recorded for the head / neck and thigh territories , with sensitivity and specificity levels of 95% and 97% for head / neck and 98% and 97% for thigh . 
results in the remaining segment were slightly worse and less concordant with dsa , with sensitivity and specificity of 84% and 88% , respectively 1specificity 1specificity 1specificity 1specificity problem had little or no effect on diagnostic accuracy , above all thanks to the use of gd - bopta , a contrast agent with ideal relaxivity characteristics [ 13 ] for first - pass vascular studies ( weak affinity for serum albumin ) that has already been successfully used [ 6 ] in whole - body protocols . 
previous studies [ 47 ] generally used either a biphasic injection with premixing of contrast material and saline and timing calculated with the test - bolus technique , or two separate injections of contrast material [ 8 ]  . 
further validation of our contrast administration protocol derives from the evidence that the few cases of suboptimal image quality were related to motion artefacts validazione del protocollo di somministrazione del mdc utilizzato deriva dallevidenza del fatto che i pochi casi in cui ladeguatezza diagnostica delle immagini risultata sub - ottimale sono stati riferibili ad artefatti da movimento o alla presenza di lesioni trofiche dei tessuti molli con conseguente precoce riempimento venoso : in nessun caso abbiamo riscontrato un insufficiente enhancement vascolare per scarso riempimento o unestesa sovrapposizione venosa . 
la rilevanza clinica dei reperti evidenziati nel nostro studio non nuova : gi in precedenza [ 1418 ] stato documentato come la prevalenza di lesioni aterosclerotiche sincrone possa essere accertata virtualmente in qualunque distretto vascolare , indipendentemente dal segmento inizialmente sintomatico . 
la tabella mostra le curve roc calcolate rispettivamente per i distretti : testa - collo , torace - addome , coscia e gamba . lanalisi dimostra come nel distretto toraco - addominale langiorm abbia sensibilit e specificit pari ad 1 , fornendo risultati completamente sovrapponibili alla dsa . 
nel distretto testa - collo e nel distretto coscia il risultato stato leggermente inferiore a quanto ottenuto nel distretto toraco - addominale , ma comunque molto significativo , sensibilit e specificit infatti si sono attestate rispettivamente su valori di 95% e 97% per testa - collo e 98% e 97% per coscia . 
nel rimanente segmento invece langiorm ha mostrato minore concordanza con la dsa con valori di sensibilit e specificit pari 84% ed 88% 1specificit 1specificit 1specificit 1specificit or the presence of trophic lesions with consequent early venous filling . 
in no case was vascular enhancement inadequate because of poor filling or extensive venous overlap . the clinical relevance of our findings is not new ; previous reports [ 1418 ] have already demonstrated that the prevalence of synchronous atherosclerotic lesions may be ascertained in virtually any vascular territory , regardless of the initially symptomatic segment . 
a further important finding concerns treatment planning : in ten patients ( 25% of the study population ) , a subsequent therapeutic intervention was planned in addition to that for which the patient had been referred . these data reflect the true multiterritorial and systemic nature of atherosclerotic disease . 
from the point of view of diagnostic accuracy , the comparison with the reference standard , albeit only available for symptomatic districts interventi terapeutici : in 10 pazienti , ovvero il 25% della popolazione , stato pianificato un ulteriore trattamento successivamente a quello che in un primo tempo ne aveva determinato il ricovero . 
da un punto di vista strettamente pertinente laccuratezza diagnostica della metodica possibile notare come nella nostra popolazione il confronto con la tecnica di riferimento , sia pur limitatamente ai soli territori sintomatici programmati per il trattamento , sia risultato eccellente : in tutti i distretti sono stati raggiunti livelli di sensibilit e specificit superiori al 90% , con la sola eccezione del circolo di gamba che , tuttavia , stato valutato in maniera pienamente soddisfacente , tenendo conto che le cause di degradazione delle immagini sono state quasi esclusivamente riconducibili ad artefatti da movimento o ritorno venoso precoce . 
 oltre ai potenziali , evidenti benefici che una metodica come langio - rm whole - body introduce , devono tuttavia radiol med ( 2009 ) 114 : 538552 scheduled for treatment , showed the technique to have excellent diagnostic accuracy in our study population . 
the levels of sensitivity and specificity achieved were greater than 90% in all districts with the sole exception of the calf , for which assessment was nevertheless fully satisfactory considering that the causes of image degradation were related to motion artefacts or early venous return . beyond the clear potential benefits of a modality such as whole - body mra , a few important remarks are in order . first , the definition of whole - body mra traditionally excludes evaluation of the coronary arteries , a frequent site of synchronous atherosclerotic lesions [ 15 ]  . 
thus , for a comprehensive evaluation of the arterial vasculature with a single examination , the only technologically feasible option is cta , thanks to the high temporal resolution afforded by latest - generation scanners ( with 64 detector rows )  . 
in addition , as concerns treatment of carotid stenoses [ 19 , 20 ] and abdominal aortic aneurysms [ 2124 ] , many conflicting views exist in the literature , and no univocal criteria have been established as to the possible benefits of screening asymptomatic patients . 
first the lack of a reference standard for all segments analysed : as obvious dose concerns preclude conventional angiography of the entire arterial system , and because our protocol did not include any comparison with whole - body cta , we must limit our analysis to the prevalence of atherosclerotic disease in asymptomatic territories without any estimation of the true capability of mra to discriminate between significant and nonsignificant lesions . 
another limitation is related to the fact that our study did not comprise asymptomatic patients : this may have produced an observer bias in that observers were aware that the studies were conducted to confirm a known and / or symptomatic disease in a population with a high pretest likelihood . 
these limitations do not , however , affect the technical aspects that our study emphasises : state - of - the - art equipment , optimised imaging protocols and the currently available contrast media allow for a high - resolution , rapid and relatively safe ( after evaluation of renal function ) study of the entire arterial vasculature , which can help identify a range of asymptomatic abnormalities that may pose a real risk to the patient . 
the technical goal has been achieved , and future research will need to further investigate , on larger patient populations , the possible clinical benefits that mra protocols can provide , even in asymptomatic patients at high risk of cardiovascular events . 
in primo luogo la definizione di whole - body in angio - rm classicamente esclude la valutazione delle arterie coronarie , altra sede in cui si evidenziano frequentemente lesioni da ma sincrone [ 15 ] ; dunque per una integrale valutazione del circolo arterioso nello stesso esame lunica opzione tecnologicamente esplorabile langio - tc , grazie allelevata risoluzione temporale che si ottiene con gli apparecchi di ultima generazione ( con configurazione dei detettori 64 )  . 
inoltre , per quanto concerne il trattamento delle stenosi carotidee [ 19 , 20 ] e degli aneurismi dellaorta addominale [ 2124 ] esistono molte opinioni discordanti in letteratura e non sono stati ancora stabiliti dei criteri univoci per leventuale beneficio apportato da un esame di screening in pazienti asintomatici ; in questi casi potrebbero essere giustificati dei dubbi sulla eventuale selezione dei pazienti . 
 il nostro studio presenta inoltre alcune limitazioni intrinseche , prima fra tutte la mancata disponibilit di un parametro di riferimento su tutti i segmenti analizzati : non essendo possibile effettuare unangiografia convenzionale dellintero sistema arterioso per ovvie motivazioni dosimetriche e non avendo incluso nel protocollo di studio uneventuale comparazione con un protocollo angio - tc whole - body , possiamo limitare la nostra analisi solamente a quella che risulta la prevalenza della ma nei distretti asintomatici , senza alcuna stima della vera capacit dellangio - rm di discriminare tra lesioni significative e non . 
unaltra limitazione deriva dal fatto che non sono stati inclusi nella nostra popolazione dei pazienti asintomatici : pu quindi essersi prodotto negli osservatori un bias dovuto alla conoscienza relativa del fatto che gli esami erano stati condotti per confermare una patologia nota e / o sintomatica , in una popolazione con alta probabilit pre - test . queste limitazioni tuttavia non influenzano quello che laspetto tecnico che il nostro lavoro vorrebbe sottolineare : con apparecchiature allo stato dellarte , protocolli di imaging ottimizzati e mezzi di contrasto attualmente disponibili possibile eseguire uno studio ad elevata risoluzione dei vasi arteriosi dellintero corpo , che allo stesso tempo rapido e relativamente sicuro ( previa valutazione della funzionalit renale ) , evidenziando una gamma di alterazioni asintomatiche che possono costituire un rischio reale per il paziente . 
il limite tecnico praticamente raggiunto ed in futuro dovranno senzaltro essere approfonditi maggiormente e su larga scala gli eventuali benefici clinici che i protocolli angio - rm possono apportare , eventualmente anche in pazienti asintomatici ma ad alto rischio per eventi cardiovascolari . 
bartolozzi1 1radiologia diagnostica e interventistica , dipartimento di oncologia , trapianti e nuove tecnologie in medicina , universit di pisa , via roma 67 , 56100 pisa , italy 2unit operativa di chirurgia iv , azienda ospedaliera universitaria pisana , pisa , italy 3divisione di gastroenterologia , dipartimento di medicina interna , universit di pisa , pisa , italy correspondence to : e . 
in the framework of the 3 - year project of the italian legatumori ( 2003 - 2006 ) , we evaluated the diagnostic accuracy of computed tomography ( ct ) colonography in detecting colorectal lesions in a screening population with positive faecal occult blood test ( fobt )  . 
patients were referred for conventional colonoscopy in the following situations : detection of three or more suspected lesions with maximum diameter 6 mm ; evidence of one or more lesions with maximum diameter > 6 mm ; presence of colonic masses ( maximum diameter > 3 cm )  . 
it generated 93 false positives and 19 false negatives in the identification of diminutive lesions ( 6 mm ) , and 70 false positives and six false negatives in lesions > 6 msensitivity was 83% in smaller lesions and 93% in lesions > 6 mm ; specificity was 45% and 59% , respectively . 
nellambito di un progetto triennale finanziato dalla legatumori ( 20032006 ) stata valutata laccuratezza diagnostica della cv nel rilievo di lesioni colorettali in una popolazione di screening risultata positiva al test per il sof . 
lesame di cc veniva indicato in presenza di : almeno 3 lesioni sospette per polipi con diametro inferiore o uguale a 6 mm , almeno 1 lesione con diametro superiore a 6 mm , o masse coliche ( diametro massimo > 3 cm )  . 
la cv ha consentito la diagnosi di masse coliche in 12 / 135 ( 8% ) pazienti ; ha generato 93 falsi positivi e 19 falsi negativi per polipi di dimensioni minori o uguali a 6 mm , e 70 falsi positivi e 6 falsi negativi per polipi di dimensioni maggiori . 
in una popolazione di screening con sof + , la cv senza fecal tagging e senza ladozione di un cut off dimensionale nella indicazione alla colonscopia tradizionale , ha evidenziato una bassa specificit , a fronte radiol med ( 2009 ) 114 : 586594 very low specificity but high sensitivity in the detection of all colorectal lesions . 
 di una elevata sensibilit nel rilievo di tutte le lesioni . keywords ct colonography colorectal cancer screening parole chiave colonscopia virtuale cancro colorettale screening introduction introduzione screening programmes for the prevention of colorectal cancer ( crc ) envisage the use of faecal occult blood testing ( fobt ) as the first - line investigation , and there is clinical evidence that this test is able to reduce mortality from crc in populations at average risk . 
on four randomised controlled trials and two nonrandomised trials showed that fobt offered to 10 , 000 subjects older than 40 years of age yielded a 16% reduction in mortality from crc [ 1 ]  . 
an italian study , score2 working group , found that in a sample of 28 , 319 asymptomatic subjects ( aged 5564 years ) with average risk of developing crc , adherence to screening by sigmoidoscopy or fobt was similar ( 28% and 30% , respectively ) , whereas the sensitivity of sigmoidoscopy for colorectal lesions was three times higher [ 2 ]  . 
data for the period 20002001 showed an adhesion rate of 41% among 192 , 583 asymptomatic subjects aged 5070 years ; of these , 5.8% were positive and 75.3% agreed to undergo conventional colonoscopy . 
ct colonography ( ctc ) has been proposed as an alternative to conventional colonoscopy in that it has similar sensitivity in detecting significant lesions ( that is , advanced adenomas , with maximum diameter > 1 cm ) but is less invasive and better tolerated . 
a comparison of the three trials shows that the best results , achieved by picki programmi di screening per la prevenzione del carcinoma colorettale ( ccr ) prevedono lutilizzo in prima istanza del test del sangue occulto fecale ( sof ) ed unevidenza clinica che tale test sia in grado di ridurre la mortalit per neoplasia nella popolazione a rischio medio . 
 [ 1 ] , su 4 studi randomizzati e 2 non randomizzati , ha evidenziato che il test del sof offerto a 10000 soggetti di et superiore a 40 anni ha consentito di ridurre la mortalit per carcinoma colorettale del 16% [ 1 ]  . 
uno studio italiano , score2 working group , ha evidenziato che su un campione di 28319 soggetti asintomatici ( et compresa tra 55 e 64 anni ) , con rischio medio di sviluppare un ccr , le percentuali di adesione allo screening mediante sigmoidoscopia o test del sof erano paragonabili , rispettivamente del 28% e 30% ; per contro la sensibilit della sigmoidoscopia nel rilievo di lesioni colorettali era 3 volte superiore [ 2 ]  . 
questi dati sono a favore quindi del test pi invasivo che , a fronte di una simile percentuale di adesione rispetto al sof , presenta una netta superiorit in termini di accuratezza diagnostica . 
la bassa percentuale di adesione confermata da ulteriori programmi di screening , come ad esempio quello effettuato dalla regione toscana ; i dati relativi al periodo 20002001 hanno evidenziato , su 192583 soggetti asintomatici di et compresa tra 50 e 70 anni , una percentuale di adesione del 41% ; di questi il 5 , 8% risultato positivo e il 75 , 3% ha accettato di sottoporsi ad una colonscopia tradizionale di controllo . 
 pertanto gli attuali test di screening del ccr , a fronte di una non invasivit da una parte e elevata accuratezza diagnostica dallaltra , non consentono ancora una significativa adesione al programma di prevenzione da parte della popolazione a rischio . 
la ricerca di un metodo alternativo quindi giustificata allo scopo di identificare un test che ad unaccuratezza diagnostica accettabile , compara588 radiol med ( 2009 ) 114 : 586594 hardt et al . , are accounted for by greater radiologist experience , use of faecal tagging techniques and primary 3d visualisation , which increase the techniques sensitivity [ 57 ]  . 
 because ctc has only recently been introduced into clinical practice , it does not yet feature in crc screening protocols , whereas the use of the double - contrast barium enema is consolidated in cases of incomplete conventional colonoscopy . 
within the framework of a 3 - year project funded by legatumori ( 20032006 ) , we evaluated the diagnostic accuracy of ctc in the detection of colorectal lesions in a screening population with positive fobt . 
 materials and methods patients the study considered 230 asymptomatic subjects ( aged 4580 years ) with positive fobt performed on their physicians advice or in response to the invitation of the tuscany region in the context of a regional crc screening programme [ 3 ]  . 
the patients had been informed about the need for further investigation with conventional colonoscopy but refused to undergo the test and were therefore told about alternative diagnostic tests and referred to the department of diagnostic and interventional radiology to complete screening with ctc . 
 examination protocol and image analysis technique intestinal cleansing was achieved with a low - residue diet during the 2 days before the examination and oral administration of a polyethylene glycol solution ( 3 l ) ( selg 1000 ; promefarm srl , milan , italy ) the day before the examination . 
to reduce bowel peristalsis , promote colonic distension and improve patient tolerance , patients received 20 mg of hyoscine butylbromide ( buscopan , boehringer ingelheim , florence , italy )  . 
subsequently , the colon was insufflated with room air by using a rectal tube and enema bag . the volume of air insufflated , 2 l on average , was adjusted according to patient tolerance . 
the volumetric acquisition was obtained with a multislice scanner ( lightspeedplus ; ge medical systems , usa ) without contrast administration and with low radiation dose with the patient in supine and prone position . 
scanning parameters were as follows : slice thickness 1.25 mm , reconstruction interval 1.25 mm , pitch 6 ( gantry rotation 0.5 s ) , 120 kv , 50 bile a quella della colonscopia convenzionale , unisca un maggior gradimento da parte del paziente . 
la colonscopia virtuale ( cv ) viene proposta come alternativa alla cc per la sua paragonabile sensibilit nel rilievo di lesioni significative ( cio gli adenomi avanzati , con diametro massimo > 1 cm ) , ma meglio tollerata dal paziente perch meno invasiva . 
i pi recenti trials clinici di rockey , cotton e pickhardt , su soggetti asintomatici hanno evidenziato dati discordanti di accuratezza diagnostica della metodica [ 4 ]  . confrontando i 3 studi , emerge che i migliori risultati , relativi allo studio di pichkardt , sono giustificati da una maggior esperienza dei radiologi , dalluso di tecniche di marcatura fecale e dalla tecnica di visualizzazione primaria 3d che consente un incremento della sensibilit [ 57 ]  . 
 data la sua recente introduzione nella pratica clinica , la cv non ancora inserita nei protocolli di screening del ccr ; risulta invece consolidato luso del clisma a doppio contrasto , indicato nei casi di cc incompleta . 
nellambito di un progetto triennale finanziato dalla legatumori ( 20032006 ) stata valutata laccuratezza diagnostica della cv nel rilievo di lesioni colorettali in una popolazione di screening risultata positiva al test per il sof . 
 materiali e metodi pazienti sono stati inclusi nello studio 230 soggetti asintomatici ( di et compresa tra 45 e 80 anni ) , risultati positivi al test del sof , eseguito su consiglio del proprio medico curante o su invito della regione toscana nellambito del protocollo di screening regionale per la prevenzione dei tumori del colon [ 3 ]  . 
i pazienti , informati dal medico curante della necessit di eseguire un approfondimento diagnostico con cc , hanno rifiutato lindagine ; sono stati quindi informati sui possibili test diagnostici alternativi e inviati presso la divisione di radiologia diagnostica e interventistica per completare lo screening con cv . 
 protocollo desame e metodo di analisi delle immagini la pulizia intestinale stata ottenuta mediante dieta priva di fibre nei due giorni antecedenti lesame e , assunzione radiol med ( 2009 ) 114 : 586594 mas ( calculated dose 4.5 mgy per acquisition )  . 
whenever a colonic mass was detected , patients received 120 ml intravenous iodinated contrast material ( visipaque 320 , ge / healthcare ) at a flow rate of 3ml / s . 
all examinations were reviewed with primary 2d analysis , using endoscopic 3d visualisation for equivocal findings ; 2d analysis was carried out with a bone window ( width 1 , 500 , level 150 )  . 
images were reviewed with double reading by two radiologists who , before the start of the study , had interpreted more than 500 ctc examinations , more than 500 of which were with endoscopic control . according to the european society of gastrointestinal and abdominal radiology ( esgar ) consensus statement , the two observers could be considered experts [ 8 ]  . 
 conventional colonoscopy was indicated in the presence of at least three suspected polyps up to 6 mm in diameter , at least one lesion > 6 mm in diameter or colonic masses ( maximum diameter > 3 cm )  . 
the endoscopist was aware of the ctc results , and in all cases , the radiologist or trainee radiologist who had performed ctc attended the conventional colonoscopy examination and indicated the site of the lesion whenever this had not been identified during the first passage of the endoscope . 
 ctc sensitivity and specificity for polyps were calculated using results of conventional colonoscopy as the reference standard both in patients with complete conventional colonoscopy and in those with incomplete examinations , in which case only the examined segments were considered . 
in the case of positive fobt and negative ctc , the patient was offered a 5 - year follow - up visit with repetition of fobt or ctc ( to be chosen by the referring physician and the patient )  . 
ctc examinations were complete in all cases , allowing exploration of the entire colon up to the caecuin 16 / 230 cases , exploration of the sigmoid colon orale di una soluzione acquosa ( 3 l ) di polietilenglicole ( selg 1000 , promefarm srl , milano , italia ) il giorno precedente . 
per ridurre la peristalsi intestinale , favorire la distensione colica e migliorare la tolleranza del paziente sono stati somministrati 20 mg di bromuro di joscina ( buscopan , boehringer ingelheim , firenze , italia ) ; successivamente stato effettuato pneumocolon con aria ambiente , mediante sonda rettale e sacca per clisma . 
lacquisizione volumetrica era ottenuta con appa ( lightspeedplus , ge / medical recchiatura multistrato systems , usa ) , in condizioni basali e bassa dose radiante , nei decubiti supino e prono , utilizzando i seguenti parametri : spessore di strato 1 , 25 mm , intervallo di ricostruzione 1 , 25 mm , pitch 6 ( rotazione del tubo 0 , 5 s ) , 120 kv , 50 mas ( dose calcolata 4 , 5 mgy per acquisizione )  . 
 le immagini relative alla prima acquisizione , condotta in posizione supina , venivano immediatamente analizzate per escludere la presenza di masse coliche ( diametro massimo > 3 cm )  . 
in caso positivo si procedeva alla somministrazione di mezzo di contrasto iodato ev ( visipaque 320 , ge / healthcare ) , per un totale di 120 ml con flusso 3 ml / s . 
gli esami erano valutati con doppia lettura in consenso da due radiologi che , allinizio dello studio , avevano gi letto oltre 500 colonscopie virtuali di cui oltre 150 controllate endoscopicamente . 
 lesame di cc veniva indicato in presenza di : almeno 3 lesioni sospette per polipi con diametro inferiore o uguale a 6 mm , almeno 1 lesione con diametro superiore a 6 mm , o masse coliche ( diametro massimo > 3 cm )  . 
at conventional colonoscopy , the colon could not be explored up to the caecum in 16 / 135 ( 11.9% ) cases owing to patient intolerance ( n = 11 ) , luminal stenosis due to sigmoid diverticulosis ( n = 2 ) and tortuous elongated sigmoid ( n = 2 )  . 
lendoscopista era a conoscenza dei reperti della cv e in tutti i casi il medico radiologo o lo specializzando in radiologia che avevano effettuato lesame di cv erano presenti durante la colonscopia , indicando allendoscopista la sede di lesione nel caso non fosse stata identificata durante il primo passaggio dellendoscopio . 
 la sensibilit e specificit venivano calcolate per polipi , utilizzando i risultati della cc come standard di riferimento , sia nei pazienti in cui la cc era completa , sia in quelli in cui la cc risultava incompleta , limitatamente ai segmenti colici esaminati . 
nei casi di sof positivo e cv negativa veniva prospettato al paziente un follow - up a 5 anni , con ripetizione del sof o dellesame di cv ( a scelta del medico curante e del paziente )  . 
1a - c adenocarcinoma of the ascending colon in a 57 - year - old woman with positive faecal occult blood test ( fobt ) and high familial risk for colorectal cancer . 
in the supine acquisition , the abundant residual fluid in the ascending colon does not allow clear identification of endoluminal lesions . however , a focal thickening of a haustral fold ( arrow ) , partially covered by fluid , can be appreciated in the distal third of the colonic segment ( a )  . 
nel decubito prono ( b ) lo spostamento dei residui fluidi dal colon destro verso i segmenti distali consente il rilievo di una massa ( diametro massimo 3 , 5 cm ) , a sviluppo sessile ( freccia )  . 
a sessile mass ( maximum diameter 4 cm ) located in the distal third of the ascending colon can be appreciated in both the supine ( a ) and prone ( b ) decubitus . 
repositioning of the patient ( from supine to prone ) causes the small amount of fluid evident in the ascending colon to move to the contralateral , more distal , colonic wall ( arrowheads )  . 
nei decubiti supino ( a ) e prono ( b ) apprezzabile una massa ( diametro massimo di 4 cm ) a sviluppo sessile , localizzata nel 1 / 3 medio del colon ascendente . 
si pu notare come nel variare il decubito , la minima quantit di residuo fluido presente nel colon ascendente in supino sia migrata per gravit verso la parete controlaterale e pi distale dello stesso segmento colico ( testa di freccia )  . 
although several semeiotic criteria may be used , including the stato possibile condurre lesplorazione colica fino al cieco per intolleranza del paziente ( n = 11 ) , stenosi del lume in diverticolosi del sigma ( n = 2 ) , angolature in dolicosigma ( n = 2 )  . 
in base al solo decubito supino non possibile identificare la morfologia del polipo che risulta invece chiara nel decubito prono ( b ) , dove sono apprezzabili il peduncolo ( testa di freccia ) e la porzione cefalica ( freccia ) , che presenta diametro massimo di 3 cm . heterogeneous density of residue or the fact that the residue moves as the patient is repositioned , inadequate bowel cleansing will invariably lead to diagnostic doubts . 
 escludendo i polipi inferiori a 6 mm , clinicamente non significativi ( cio con rischio prossimo allo zero nella probabilit di presentare foci di degenerazione neoplastica e quindi non meritevoli di segnalazione alla colonscopia virtuale ) , sono stati rilevati polipi significativi in 57 / 230 ( 19% ) pazienti . 
 discussione il primo dato che emerge dai nostri risultati relativo alla bassa specificit del test per tutti i tipi di polipi considerati . il dato , era a nostro avviso prevedibile e da riferire in primo luogo al mancato utilizzo della marcatura fecale . 
sebbene si possano utilizzare alcuni criteri di semeiotica , come la disomogenea densit dei residui o il fatto che cambiano generalmente posizione al variare del decubito , la scarsa preparazione intestinale genera sempre e comunque un dubbio diagnostico . 
recentemente sia linternational working group on virtual colonoscopy , sia lesgar , hanno riunito i maggiori esperti in materia e raggiunto un consenso , indicando che i polipi con dimensioni inferiori a 6 mm non dovrebbero essere segnalati nel referto onde evitare la generazione di molti falsi positivi [ 7 , 10 ]  . 
in questo studio infatti lelevato numero di falsi positivi da attribuire proprio alla decisione di segnalare le formazioni endoluminali di dimensioni non significative ; situazione che si pu verificare molto spesso in cv senza marcatura fecale e laddove coesiste una scarsa toelette intestiradiol med ( 2009 ) 114 : 586594 fig . 
4a , b false positive result at computed tomographic ( ct ) colonography in a 61 - year - old woman with marked diverticulosis of the sigmoid colon and positive faecal occult blood test ( fobt )  . 
in the supine decubitus ( a ) , a pedunculated lesion with homogeneous density is interpreted as a polyp ( arrows ) ; a coronal multiplanar reconstruction ( b ) further demonstrates the pedunculated morphology of the finding ( arrows ) , which is not , however , confirmed by conventional colonoscopy performed 10 days later . 
nel decubito supino ( a ) si rileva una sospetta lesione parietale a densit omogenea e sviluppo peduncolato ; la ricostruzione multi planare coronale ( b ) evidenzia ulteriormente la morfologia peduncolata del reperto ( frecce ) , che non viene per confermato dalla cc eseguita a distanza di circa 10 giorni . 
 indeed , in this study , the high number of false positive results is to be ascribed primarily to the decision to report endoluminal lesions of nonsignificant size , a situation that may occur very frequently at ctc without faecal tagging and in the presence of poor bowel cleansing . 
even the poor specificity for polyps > 6 mm can be accounted for by the criteria adopted in the study , which had been initially designed in this manner and subsequently not modified to avoid nonuniform interpretation and reporting . 
 [ 11 ] showed that reporting ctc studies with the exclusion of diminutive lesions that is , those < 6 mm would lead to a 77.6% reduction of endoscopic screening procedures and a proportional reduction of related complications . 
this conventional method colonoscopy , which may benefit from a previous ctc , especially in the case of intolerant patients , as the targeted search for a lesion shortens examination times . accuracy of increased the nale . 
anche la scarsa specificit per polipi di dimensioni superiori a 6 mm da attribuire agli stessi criteri dello studio , disegnato inizialmente secondo queste modalit e quindi non modificato per evitare una disomogenea metodologia di interpretazione e refertazione . 
 [ 11 ] , ha evidenziato che la refertazione di esami di cv con esclusione delle lesioni diminutive , cio inferiori a 6 mm , consentirebbe una riduzione del 77 , 6% delle procedure endoscopiche di screening e una proporzionale riduzione delle complicanze ad esse correlate . 
nel presente studio prospettico la cc veniva eseguita in presenza del medico radiologo che aveva interpretato la cv e , che quindi suggeriva di ispezionare il segmento colico in cui aveva indicato la lesione . 
questo metodo consentiva una maggiore accuratezza della cc , che pu pertanto beneficiare di una cv precedente , soprattutto , nei pazienti con scarsa tolleranza allesame , dove la ricerca mirata di una lesione riduce i tempi desame . 594 radiol med ( 2009 ) 114 : 586594 one limitation of this study was the lack of endoscopic control in patients with negative ctc results ( 95 / 230 ; 42% )  . we are therefore unable to provide diagnostic accuracy data on a per - patient basis . 
these limitations may be overcome by larger patient series that are emerging from multicentre trials , among which is the american college of radiology imaging network ( acrin ) 6664 trial ( just completed , with the enrolment of more than 2 , 000 asymptomatic patients ) and the italian society of radiology ( sirm ) - impact study ( completed , with the recruitment of more than 1 , 000 asymptomatic patients ) [ 12 , 13 ]  . 
questi limiti , potranno essere superati da pi ampie casistiche che stanno emergendo da studi multicentrici , di cui lo studio americano acrin 6664 ( appena concluso con il reclutamento di oltre 2000 pazienti asintomatici ) e lo studio italiano sirm - impact ( concluso con il reclutamento di oltre 1000 pazienti asintomatici ) [ 12 , 13 ]  . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , 2dipartimento di sanit pubblica , cattedra di igiene , policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy correspondence to : a . 
a total of 467 patients underwent a pet / ct scan using an iodinated contrast mediuwe compared images obtained by the single pet scan , the single ct scan and by the fusion of the two procedures ( pet / ct )  . 
la tecnica pet risultata avere una sensibilit pari al 94 , 05% , una specificit pari al 91 , 60% ed unaccuratezza del 93 , 36% ; la tecnica tc una sensibilit pari al 91 , 07% , una specificit pari al 95 , 42% ed unaccuratezza del 92 , 29% . 
essa risultata particolarmente efficace quando , pur in presenza di un innalzamento progressivo dei marcatori , non era visualizzabile clinicamente o strumentalmente ripresa di malattia , 572 radiol med ( 2009 ) 114 : 571585 specificity , enabling modification of patient treatment , but it is also a unique , high - profile procedure that can produce cost savings . keywords fdg - pet / ct colorectal cancer staging liver metastases recurrence garantendo cos unanticipazione diagnostica . 
la pet / tc non solo offre una performance diagnostica ottimale in termini di sensibilit e specificit , permettendo peraltro di modificare liter terapeutico del paziente , ma riveste anche caratteri di indagine unica di elezione , con conseguenti risparmi economici . parole chiave fdg - pet / tc carcinoma colon - rettale stadiazione metastasi epatiche recidiva introduction introduzione colorectal cancer has an elevated incidence in western countries and is the second most frequent cause of death from cancer in both genders in europe and the united states [ 1 ]  . 
liver metastases are a common occurrence in the history of patients affected by colorectal cancer , with an incidence of 20% at the time of diagnosis and > 50% during the course of the disease [ 3 ]  . 
in 15%30% of cases , the metastases manifest exclusively in the liver at the same time or months or years after diagnosis of the primary tumour of the colon or rectuthe natural history of the disease shows that once they have been identified , liver metastases are destined to increase in size and number . hepatic resection of metastatic lesions is considered the most effective treatment option in terms of increased survival [ 4 , 5 ] , although few patients are able to undergo radical surgery at the time of diagnosis ( owing to lesion site , multifocal involvement and / or insufficient residual liver function ) , and the 5 - year survival rate after surgery is only 20%50% [ 6 ]  . 
to date , the imaging modalities used for this purpose have been ultrasonography , contrast - enhanced computed tomography ( ct ) and magnetic resonance imaging ( mri )  . 
however , given the poor long - term results obtained , these modalities are evidently unable to guarantee an accurate preoperative assessment [ 7 ]  . the impact of positron emission tomography ( pet ) on the quality of pretreatment diagnostic staging has been demonstrated in many tumours , including colorectal carcinoma . 
retrospective studies have shown that pet provides a better preoperative selection of patients with colorectal cancer and secondary lesions , which after resection of liver il cancro del colon - retto presenta unelevata incidenza nel mondo occidentale ed la seconda causa di mortalit per neoplasia in ambedue i sessi sia in europa che negli stati uniti [ 1 ]  . 
in italia , in particolare , i nuovi casi sono ogni anno circa 46000 con sopravvivenza a 5 anni del 58% [ 2 ]  . nella storia dei pazienti affetti da neoplasia del colon - retto , le metastasi epatiche rappresentano unevenienza comune , presentandosi nel 20% dei casi al momento della diagnosi ed in oltre il 50% nel corso della malattia [ 3 ]  . 
nel 15%30% dei casi le metastasi si manifestano esclusivamente al fegato contestualmente o a distanza di mesi o di anni dal momento della diagnosi del tumore primitivo del colon o del retto . 
 la resezione epatica delle lesioni metastatiche lapproccio terapeutico finora ritenuto pi efficace in termini di aumento della sopravvivenza [ 4 , 5 ] , ma solo pochi pazienti sono radicalmente operabili al momento della diagnosi ( in relazione alla localizzazione , al coinvolgimento multifocale e / o in ragione di una insufficiente funzionalit epatica residua ) e la sopravvivenza a 5 anni dopo la chirurgia solo del 20%50% [ 6 ]  . 
finora le tecniche diagnostiche utilizzate a questo scopo sono state lecotomografia , la tomografia computerizzata ( tc ) con mezzo di contrasto ( mdc ) , la risonanza magnetica ( rm ) ma , in considerazione degli scarsi risultati ottenuti a lungo termine , evidentemente esse da sole risultano insufficienti non riuscendo a garantire unaccurata valutazione pre - chirurgica [ 7 ]  . 
 limpatto della pet ( tomografia a emissione di positroni ) sulla qualit dello staging diagnostico pre - terapeutico radiol med ( 2009 ) 114 : 571585 metastases translates into longer survival [ 8 ]  . 
this occurs because the tracer used usually 2 ( 18f - fdg ) , a [ fluorine - 18 ] fluoro - 2 - deoxy - d - glucose glucose analogue labelled with fluorine is avidly taken up by the neoplastic cells , which have a more active glucose metabolism than normal cells [ 9 ]  . 
the metabolic information provided by fdg - pet can therefore be used to obtain a more accurate definition of the areas of malignancy and possible lymph - node involvement , as well as identifying distant metastases , as the examination provides a full - body scan [ 10 ]  . 
furthermore , functional / metabolic alterations can be demonstrated and located earlier than the information provided by other imaging modalities , which are based purely on anatomical dimensional criteria or vascular abnormalities . 
the introduction of new hybrid pet / ct scanners is in this sense a great leap forward [ 1113 ]  . the aim of this study was to compare the diagnostic accuracy of 18f - fdg - pet , ct and pet / ct in the detection of liver metastases during staging and follow - up of patients with colorectal cancer . materials and methods the study involved patients referred to our department between april 2005 and december 2007 with a diagnosis of colorectal cancer and suspected liver metastases . 
the definitive diagnosis was provided by histology and / or clinical / radiological follow - up in all patients , even those who did not undergo biopsy or surgical procedures . pet / ct examination technique all examinations were performed with an integrated pet / ct scanner , discovery st ( ge , general electric medical systems , milwaukee , wi , usa )  . 
before injection of the radiotracer , patients blood glucose levels were evaluated , and 18f - fdg was injected only in conditions of normal glycaemia to avoid reducing the diagnostic potential of pet as a result of the competitive effect created by high blood glucose levels . 
studi retrospettivi hanno dimostrato che la pet permette una migliore selezione pre - operatoria dei pazienti con tumore del colon - retto con localizzazioni secondarie , che si traduce , dopo la resezione di metastasi epatiche , con una pi lunga sopravvivenza [ 8 ]  . 
le informazioni metaboliche che fornisce la fdg - pet permettono dunque una pi accurata definizione delle aree di malignit , delleventuale coinvolgimento linfonodale oltre allidentificazione di lesioni ripetitive a distanza in quanto lindagine consente una scansione di tutto il corpo [ 10 ]  . 
inoltre le alterazioni funzionali / metaboliche possono essere dimostrate e segnalate pi precocemente rispetto a quelle fornite da altre tecniche di imaging che si basano su criteri puramente anatomici dimensionali o su anomalie di vascolarizzazione . le limitate informazioni morfologiche fornite dalla pet , rendono per necessaria lintegrazione con la tc convenzionale . 
lintroduzione di nuovi scanner ibridi pet / tc rappresenta a tal fine un grande passo avanti [ 1113 ]  . lo scopo di questo studio comparare laccuratezza diagnostica della 18f - fdg - pet , della tc e quella della pet / tc nel rilievo di metastasi epatiche in pazienti affetti da neoplasie del colon - retto in fase di stadiazione e nel follow - up . 
 materiali e metodi lo studio ha riguardato i pazienti , giunti presso il nostro dipartimento nel periodo compreso tra aprile 2005 e dicembre 2007 , con diagnosi di neoplasia del colon e del retto con sospetto di metastasi epatiche valutate mediante pet , tc e pet / tc con mdc organo - iodato . 
la diagnosi definitiva stata ottenuta mediante conferma istologica e / o attraverso il follow - up clinico - radiologico di tutti i pazienti , anche di quelli non sottoposti a procedure bioptiche o ad intervento chirurgico . tecnica di esecuzione dellesame pet / tc ms tutti gli esami sono stati eseguiti con uno scanner integrato pet / tc ms discovery st ( ge , general electric , medical systems , milwaukee , wi , usa )  . 
tale sistema combina uno scanner tc modello high speed ultra con 16 file di detettori con un tomografo pet con 10080 cristalli di germinato di bismuto ( bgo ) disposti in 24 anelli . 
during this phase , the patient was kept in a quiet environment to limit muscle activity and thereby reduce radiotracer accumulation in skeletal muscle . the patient was also adequately hydrated with intravenous saline solution ( 250500 ml ) to reduce pooling of the radiotracer in the renal collecting syste at the same time , a single dose of approximately 900 cc of a solution containing contrast material ( gastrografin - 370 mgi / ml , schering ag , berlin , germany ) was administered orally to adequately opacify the bowel loops according to a protocol implemented in the department . the examination was performed with the patient lying supine inside the gantry with arms above the head and began with a scout scan . 
the following scan parameters were used : 140 kv to obtain good quality images at the level of the shoulder and pelvic girdles ; 80 ma ; fov 420500 mm ; ct slice thickness 3.75 mm ( retrospectively reconstructed to 1.25 mm ) to approximate the width of the pet section ; slice interval 3.27 mm , to coincide with the spacing between the pet sections ; scan speed < 1 s per revolution . 
once the ct scan was completed , the pet scan was performed with a 2d technique in the caudocranial direction from the proximal third of the femurs to the head ; five to six bed positions were acquired , with a duration of 4 min per bed . images were reconstructed using a standard iterative algorithm [ ordered subsets expectation maximisation ( osem ) ] , with a mean duration for the pet examination of 2024 mpet acquisition was immediately followed by ct examination performed with the intravenous administration of 100120 ml of nonionic iodinated contrast medium with an injection rate of 23 ml / s ( iomeron - 350 mgi / ml , bracco , milan , italy )  . 
two data sets were acquired : the first included the upper abdomen with a delay of 30 s from the beginning of the contrast injection , and the second extended from the neck to the pubic symphysis with a delay of 6080 s . 
the overall duration of the entire pet / ct acquisition was on average 40 min . image analysis images were processed on an advantage - windows 4.2 workstation ( ge , general electric medical systems ) individually for the pet and ct examinations and with iniettando il 18f - fdg solo in condizioni di normoglicemia per evitare di ridurre il potenziale diagnostico della pet per leffetto competitivo dovuto ad elevati livelli glicemici . nel caso di iperglicemia si invitato il paziente ad incrementare temporaneamente lattivit muscolare , per riportare la glicemia al di sotto di 150 mg / dl . 
durante questa fase il paziente stato tenuto in un ambiente tranquillo per limitare lattivit muscolare onde ridurre , dopo liniezione , laccumulo del radiofarmaco nella muscolatura scheletrica ; si inoltre provveduto ad una adeguata idratazione mediante infusione endovena di soluzione fisiologica ( 250500 ml ) per ridurre il ristagno di tracciante nellemuntorio renale . 
contemporaneamente sono stati somministrati per via orale circa 900 cc di una soluzione contenente mdc ( gastrografin , 370 mgi / ml , schering ag , berlino , germania ) in ununica somministrazione , per unadeguata opacizzazione delle anse intestinali secondo il protocollo praticato nel nostro dipartimento . per lesecuzione dellesame , il paziente viene posizionato allinterno del gantry in decubito supino , con le braccia al di sopra della testa e lindagine inizia con uno scanogramma . viene quindi acquisita una tc in condizioni basali a basso amperaggio ( 80 ma ) necessaria per la correzione dellattenuazione per lo studio pet , utilizzando i seguenti parametri : 140 kv per ottenere immagini di buona qualit a livello del cingolo scapolo - omerale e pelvico ; 80 ma ; fov : 420500 mm ; spessore della sezione tc pari a 3 , 75 mm ( retroricostruibile a 1 , 25 mm ) per approssimare la larghezza della sezione pet ; intervallo tra le sezioni ricostruito pari a 3 , 27 mm , per la coincidenza con la spaziatura tra le sezioni pet ; velocit di scansione inferiore a 1 secondo per rivoluzione . terminata la tc , stato effettuato lesame pet con tecnica 2d in direzione caudo - craniale a partire dal iii prossimale dei femori fino a comprendere il cranio ; sono stati acquisiti 56 lettini con durata di 4 minuti ognuno . 
 le immagini sono state ricostruite utilizzando un algoritmo iterativo standard ( osem , ordered subsets expectation maximization ) , per una durata in media dellindagine pet pari a 2024 minuti circa . 
subito dopo lacquisizione pet viene effettuato lesame tc dopo somministrazione endovena di 100120 ml di mdc organo - iodato non ionico a 23 ml / s ( iomeron - 350 mgi / ml , bracco , milano , italia ) predisponendo due pacchetti susseguenti di scansioni : il primo comprendente laddome superiore con un ritardo di 30 secondi dallinizio delliniezione del mdc , il secondo esteso dal collo fino alla sinfisi pubica con un ritardo di 6080 secondi . 
unulteriore scansione viene effettuata in fase tardiva per una corretta caratterizzazione delle lesioni . infine , dopo avere fatto addurre lungo il tronco gli arti superiori , si acquisiscono scansioni assiali sul cranio . la tecnica di acquisizione stata : 120140 kv , amperaggio automatico ( limite 330350 ma ) , spessore di 3 , 750 mm ( retroricostruibile a 1 , 25 mm ) , modalit di acquisizione radiol med ( 2009 ) 114 : 571585 pet / ct fusion software . 
acquisition data of all ct examinations were processed and retrospectively reconstructed with the following parameters : slice thickness 1.25 mm and interval 3.27 mm to coincide with the spacing between the pet sections . 
attenuation changes of the lesions were then quantified in both baseline conditions and after contrast enhancement . images obtained with ct and pet were independently reviewed by a radiologist and nuclear physician in a doubleblind fashion . 
la durata complessiva dellintera acquisizione pet / tc risultata in media di circa 40 minuti . analisi delle immagini le immagini sono state rielaborate su una workstation advantage - windows 4.2 ( ge , general electric , medical systems ) , singolarmente per lesame pet e tc e mediante ricostruzioni con software di fusione pet / tc . 
i dati di acquisizione di tutti gli esami tc da noi valutati sono stati rielaborati e retroricostruiti con le seguenti indicazioni : spessore delle sezioni pari a 1 , 25 mm ed intervallo tra le sezioni di 3 , 27 mm per la coincidenza con la spaziatura tra le sezioni pet . 
1a - d focal increase of 2 - [ fluorine - 18 ] fluoro - 2 - deoxy - d - glucose ( 18f - fdg ) uptake by two hepatic metastases in the right lobe in a 63 - year - old man with colorectal cancer . 
on coronal maximum intensity projection ( mip ) ( a ) , fdg positron emission tomography ( fdg - pet ) and ( b ) fused pet contrastenhanced computed tomography ( ct ) images show both lesions , although they are located in different planes . 
1a - d iperfissazione del tracciante in corrispondenza di due metastasi epatiche a livello del lobo di destra in un uomo di 63 anni con carcinoma del colon - retto . 
presenza di due lesioni nodulari epatiche localizzate a livello dellviii ( c ) e del v ( d ) segmento . 576 radiol med ( 2009 ) 114 : 571585 fig . 
the axial ( a ) 2 - [ fluorine - 18 ] fluoro - 2 - deoxy - d - glucose positron emission tomography ( 18f - fdg - pet ) image and ( b ) the fusion pet contrast - enhanced computed tomography ( ct ) images show the lesion as a focal increase of fdg uptake that corresponds to a focal hypoattenuating lesion on contrast - enhanced ct in the portal phase ( c )  . 
nellimmagine assiale fdg - pet ( a ) ed in quella di fusione pet / tc ( b ) la lesione riconoscibile come area di aumentato metabolismo in corrispondenza di una formazione ipodensa alla tc ( c ) in fase portale . 
d nella scansione assiale tc basale senza mdc la lesione focale scarsamente riconoscibile . statistical analysis data analysis was performed on the basis of the positive findings in the individual patient . 
for each imaging modality , we evaluated sensitivity , specificity and diagnostic accuracy with 95% confidence intervals ( 95% ci )  . the difference between the individual modalities ( pet and ct ) and the combined technique ( pet / ct ) , with a statistically significant value of p < 0.05 , was estimated with the z lesioni , evidenziate in condizioni basali e nella fase postcontrastografica . 
 le immagini ottenute con la tc e con la pet sono state visionate e valutate indipendentemente , in doppio cieco da uno specialista radiologo e da uno specialista in medicina nucleare . 
abbiamo valutato , per le tecniche in esame , la sensibilit , la specificit e laccuratezza diagnostica con i relativi intervalli di confidenza al 95% ( ic 95% ) ; la differenza tra le singole metodiche ( pet , tc ) e la combinata ( pet / tc ) , con un valore statisticamente significativo di p < 0 , 05 , stata stimata con il test z . 
la diagnosi definitiva stata ottenuta mediante conferma istologica e / o attraverso il follow - up di tutti i pazienti , anche di quelli non sottoposti a procedure bioptiche o ad intervento chirurgico . 
3a - c liver metastases depicted only by 2 - [ fluorine - 18 ] fluoro - 2 - deoxy - dglucose positron emission tomography ( 18f - fdg - pet )  . 
the axial pet scan ( a ) and the fdg - pet / computed tomography ( ct ) fusion image ( b ) show multiple foci of increased fdg uptake in the liver of 59 - year - old woman with colorectal carcinoma . 
la scansione pet assiale ( a ) e limmagine fdg - pet / tc ( b ) con mdc di fusione , documentano aumento focale della captazione di fdg in corrispondenza di multiple metastasi epatiche in una donna di 59 anni con carcinoma del colon - retto . 
the ppv of pet was calculated to be 96.64% ( 95% ci : 94.6998.59 ) , and the npv was 85.71% ( 95% ci : 79.9291.51 ) ( table 2 )  . 
for the combined technique , the ppv was 99.10% ( 95% ci : 98.08100 ) and the npv was 94.81% ( 95% ci : 91.0798.56 ) ( table 4 )  . 
per la tecnica pet / tc combinata il vpp pari al 99 , 10% ( ic 95% : 98 , 08100 ) , il vpn pari al 94 , 81% ( ic 95% : 91 , 0798 , 56 ) ( tabella 4 )  . lindividuazione di una differenza statisticamente significativa per sensibilit , specificit e accuratezza stata ottenuta mediante il test z relativamente alla tecnica combinata ( pet / tc ) vs pet . 
non stata evidenziata alcuna differenza statisticamente significativa di sensibilit , specificit e accuratezza tra le singole tecniche ( pet vs tc ) ( tabella 5 )  . radiol med ( 2009 ) 114 : 571585 fig . 
coronal maximum intensity projection 2 [ fluorine - 18 ] fluoro - 2 - deoxy - d - glucose positron emission tomography ( mip 18f - fdg - pet ) scan ( b ) does not reveal focal uptake of fdg in the liver . 
a la scansione tc , acquisita in fase portale , documenta la presenza di una lesione focale di natura secondaria di 7 mm di diametro localizzata a livello dellviii segmento epatico . 
there was no statistically significant difference in sensitivity , specificity or accuracy between the individual techniques ( pet vs ct ) ( table 5 )  . discussione discussion colorectal cancer is one of the most common cancers in western countries , and liver metastases from the tumour are an enormous challenge for clinical oncology . 
a third of il tumore del colon - retto una delle neoplasie pi frequenti nei paesi occidentali e le metastasi epatiche di tale neoplasia rappresentano un grande problema nelloncologia clinica . 
the high level of clinical transferability of the information provided by pet nello studio delle neoplasie del colon - retto , la pet stata di solito impiegata allo scopo di chiarire la natura di lesioni dubbie gi evidenziate da esami di i livello come la tc oppure quando , soprattutto in corso di follow - up , si osservava un incremento di un marcatore oncologico , in assenza di localizzazioni documentate dai pi convenzionali esami diagnostici [ 14 ]  . 
the z test failed to demonstrate statistically significant differences between the two individual modalities and showed that pet and ct were very much alike in their detection of liver metastases . 
in contrast , combined pet / ct proved superior to pet and ct used individually , with statistically significant differences in all the parameters studied except ct specificity . in our study there was greater concordance among imaging modalities in terms of sensitivity , specificity and diagnostic accuracy than reported in the literature , as most studies to date have used ct without contrast enhancement , which does not enable visualisation of many liver metastases [ 1719 ]  . 
in our study , contrast - enhanced ct improved diagnostic reliability above all for the purposes of correct preoperative staging without negatively influencing the qualitative and quantitative data obtained at pet . although pet and ct are shown by the data to be equivalent in their ability to identify secondary hepatic lesions , the two modalities are evidently complementary . 
in agreement with the literature , the integration of pet with ct makes possible the combination of metabolic data and morphological imaging , thus enabling an accurate definition of the extension of disease at the time of diagnosis [ 20 , 21 ]  . 
the combined technique in fact offers improved localisation of the foci of radiotracer uptake , differentiating the increases in metabolic activity due to physiological or inflammatory processes from those of neoplastic origin [ 22 , 23 ]  . 
in addition , it improves the localisation and characterisation of lesions [ 24 ] , thus reducing the number of lesions of uncertain or indefinite origin . the evaluation of treatment response is also improved by not relying solely on size criteria . 
sebbene tale tracciante non sia specifico della cellula tumorale , la 18f - fdg - pet risulta largamente utilizzata nello studio di molte patologie neoplastiche [ 16 , 17 ] , in quanto considerata migliore dellimaging convenzionale nellidentificazione della patologia tumorale primitiva o secondaria . 
 nel nostro studio abbiamo voluto comparare le informazioni funzionali e morfologiche ottenute rispettivamente mediante la 18f - fdg - pet e la tc , con quelle fornite dalla lesioni secondarie pet / tc , nella valutazione delle epatiche . 
i risultati da noi ottenuti hanno evidenziato valori sovrapponibili di sensibilit , specificit e accuratezza diagnostica tra le due metodiche poste a confronto ed un miglioramento , se considerate le due tecniche associate . 
il test z non ha identificato differenze statisticamente significative tra le due singole tecniche in esame dimostrando una sostanziale equivalenza della pet e della tc nella identificazione delle localizzazioni secondarie epatiche . 
diversamente la tecnica combinata pet / tc risultata superiore alle tecniche diagnostiche pet e tc applicate singolarmente , con valori di significativit statistica in tutti i parametri studiati tranne che per la specificit tc . nel nostro studio , le metodiche mostrano una concordanza con valori di sensibilit , specificit ed accuratezza superiori ai dati della letteratura poich , la maggior parte degli studi finora effettuati utilizzano la tc senza la somministrazione di mdc organo - iodato , che non permette la visualizzazione di molte metastasi epatiche [ 1719 ]  . 
anche se le localizzazioni secondarie epatiche mostrano una evidente ipercaptazione di 18f - fdg alle immagini pet , spesso le lesioni non vengono evidenziate alla tc basale . nel nostro studio lesame tc effettuato con la somministrazione endovenosa di mdc organo - iodato , ha migliorato lattendibilit diagnostica , ai fini soprattutto di un corretto staging pre - operatorio senza inficiare le informazioni qualitative e quantitative ottenute alla pet . sebbene la pet e la tc risultano , dai dati di questo lavoro , equivalenti nella capacit di identificare localizzazioni secondarie epatiche , appare chiaro che le due metodiche sono tra loro complementari . 
in accordo con i dati della letteratura , la possibilit di integrare la pet con la tc consente di combinare linformazione metabolica con il dato anatomico permettendo , al momento della diagnosi , unaccurata definizione della estensione di malattia [ 20 , 21 ]  . 
la tecnica combinata permette infatti una migliore localizzazione dei foci di uptake , differenziando gli aumenti di attivit metabolica di natura fisiologica o flogistica da quelli di natura neoplastica [ 22 , 23 ]  . 
infatti , noto che la riduzione del numero delle radiol med ( 2009 ) 114 : 571585 may not lead to a significant reduction in lesion size , as the neoplastic tissue may be replaced by necrotic tissue or fibrosis , which cannot be differentiated from malignant tissue with conventional diagnostic modalities . 
in addition , treatment planning may be oriented and / or modified by fusion of the metabolic data provided by pet , which is fundamental for identifying secondary lesions located in the peritoneum , mesentery and lymph nodes [ 25 ] where ct shows its major limitations with the morphological data provided by ct which makes possible the examination of fundamental anatomical structures such as the portal vein , the vena cava or the bile ducts [ 26 ]  . accurate preoperative staging is crucial for determining the optimal therapeutic approach in each patient [ 27 ]  . 
the combined technique , which is able to perform precise tumour staging , can orient or rule out the need for further procedures , thus changing the treatment plan [ 18 , 2830 ]  . pet / ct has proven particularly effective even when clinical or imaging techniques fail to demonstrate disease recurrence in the presence of a progressive increase in tumour markers , thus leading to an earlier diagnosis with a positive impact on patient survival . 
the change in the uptake of 18ffdg in fact correlates with serum carcinoembryonic antigen levels , the increase in which is a common finding in these patients [ 25 ]  . the combined modality also minimises the intrinsic limitations of the two techniques responsible for fn findings . 
moreover , the use of pet / ct leads to an overall reduction in costs with respect to the separate use of the two imaging modalities [ 33 ] and improved utilisation of the diagnostic devices [ 34 ]  . 
lastly , by optimising study protocols , the combined pet / ct examination is also able to reduce the overall dose of radiation delivered to the patient [ 33 ] and the overall examination time , thus minimising patient discomfort . cellule neoplastiche pu non comportare una significativa riduzione delle dimensioni della lesione in quanto il tessuto tumorale pu essere sostituito da tessuto necrotico o fibroso , che risulta indistinguibile alla diagnostica convenzionale dal tessuto maligno . 
inoltre la fusione del dato metabolico , fornito dalla pet , fondamentale per evidenziare le localizzazioni secondarie a livello peritoneale , mesenteriale e linfonodale [ 25 ] in cui la tc mostra il suo maggior limite , con il dato morfologico , fornito dalla tc , che permette di esaminare strutture anatomiche fondamentali quali la vena porta , la vena cava o le vie biliari , guida e / o modifica il planning terapeutico [ 26 ]  . 
e la tecnica combinata , in grado di effettuare una precisa stadiazione tumorale , pu guidare o escludere la necessit di ulteriori procedure , cambiando la modalit di trattamento [ 18 , 2830 ]  . 
la pet / tc si dimostrata particolarmente efficace anche quando , in presenza di un innalzamento progressivo dei marcatori tumorali , non era visualizzabile clinicamente o strumentalmente alcuna ripresa di malattia , rendendo possibile unanticipazione diagnostica , con un aumento potenziale dellindice di sopravvivenza . 
il cambiamento nelluptake 18f - fdg correla infatti con i livelli di cea sierico , la cui elevazione sine materia di frequente riscontro in questi pazienti [ 25 ]  . 
infine , ottimizzando i protocolli di studio , con lesame combinato pet / tc si riduce anche la dose complessiva di radiazioni ionizzanti assorbita [ 33 ] , i tempi globali di esecuzione delle indagini , apportando un minore disagio al paziente . conclusions conclusioni pet / ct is able to provide a synergy of functional , anatomical and structural information with considerable optimisation con la pet / tc si ottiene un sinergismo informativo funzionale - anatomico - strutturale con una notevole ottimizzazione 584 radiol med ( 2009 ) 114 : 571585 of the data obtained with the two modalities taken individually . 
the use of pet / ct may be instrumental in reaching an earlier diagnosis , which influences patient management by prompting the performance of procedures of proven effectiveness or the nonperformance of procedures that may prove ineffective or even harmful . 
lastly , the technique has the characteristic of an all - in - one examination if performed with contrast medium , thus leading to significant economic savings . delle informazioni derivanti dalle due modalit pet e tc prese singolarmente . 
la pet / tc pu consentire tra laltro unanticipazione diagnostica che incide sulla gestione del paziente attraverso lesecuzione di interventi di documentata efficacia o la non esecuzione di interventi che potrebbero risultare inefficaci o addirittura dannosi . 
new york , 2009 isbn 978 - 88 - 470 - 1343 - 8 published online : 15 june 2009 springer - verlag 2009 this work presents the entire urogenital system in a methodical and thorough fashion . 
until a few years ago , this technique was considered the reference examination for many renal and urinary tract diseases , whereas today it has largely been replaced by ultrasonography , computed tomography ( ct ) urography and magnetic resonance ( mr ) urography . 
it is clear , however , that the ct and mr studies are able to provide in a single examination information regarding the renal parenchyma and the collecting system , the adjacent organs and structures , and functional and vascular characteristics , all of which cannot be captured in a simple urographic examination . 
 this change has come about not only in intravenous urography , but also in other forms of imaging of the urinary tract , such as antegrade and retrograde pyelography , which today is limited to only a few and principally interventional or intraoperative applications . 
however , the most important change in the imaging of the urogenital system , as with other organs and systems , is the broadening of the diagnostic imaging spectrutoday , the radiologist is involved on a number of fronts , from diagnosis intended as the identification of a lesion , its characterisation and , in the case of oncologic disease , its staging to prognosis and follow - up . added to these are functional evaluations such as can be obtained with doppler ultrasonography , spectroscopy and dynamic studies with contrast media . 
 in this work , olivetti and grazioli manage to provide thorough and updated information on all of these aspects , with a highly topical and modern interpretation of contemporary radiology of the urogenital syste the book is divided into nine sections , beginning with il testo si propone con unimpostazione molto accurata in tutte le sue parti e affronta in modo organico e completo tutto lapparato uro - genitale . 
si tratta di un libro molto attuale perch il progresso che la diagnostica per immagini ha compiuto in questo distretto stato notevole e ha cambiato profondamente il nostro modo di operare e di esaminare la patologia genito - urinaria . lesempio pi evidente di questo cambiamento nella diagnostica per immagini rappresentato dellurografia endovenosa , fino a pochi anni fa considerata lindagine di riferimento per molte patologie renali e della via escretrice , oggi sostituita dallecografia , dallurografia tc o dallurografia rm . 
per evidente che le indagini tc e rm possono dare , in un unico esame , informazioni sul parenchima , sulla via escretrice , su aspetti funzionali , vascolari , nonch sugli organi e le strutture vicine , aspetti che non possono essere colti dalla semplice indagine urografica . questo cambiamento non ha riguardato solo lurografia endovenosa , ma altre forme di visualizzazione della via escretrice , quali le pielografie ascendenti e discendenti , oggi limitate a poche applicazioni , per lo pi interventistiche o intraoperatorie . 
il cambiamento pi importante nel distretto genito - urinario , al pari di quello di altri distretti e altri organi , per lallargamento dellorizzonte della diagnostica per immagini che vede impegnato il radiologo su pi fronti che vanno dalla diagnosi , intesa come riconoscimento di lesione , alla caratterizzazione , alla stadiazione nel caso della patologia oncologica , alla prognosi e al follow - up . a queste si aggiungono oggi valutazioni funzionali come ad esempio quelle ottenibili con il doppler , la spettroscopia , le valutazioni dinamiche con mezzi di contrasto . il testo di olivetti e grazioli riesce a dare una informazione completa e attuale di tutti questi aspetti interpretando radiol med ( 2009 ) 114 : 664665 the anatomy of the urinary tract , and is accompanied by excellent illustrations , some of which can be found in the later chapters . 
the presentation of normal anatomy is followed by radiologic anatomy , which includes urography , angiography , standard ultrasonography , color doppler and contrast - enhanced ultrasonography , ct complete with ct urography and mr with mr angiography and mr urography . 
this is followed by chapters on the normal human anatomy and radiologic anatomy of the male and female reproductive systems , which are organised in the same way as the previous chapters . 
the last section deals with interventional radiology in its various forms and includes chapters on biopsies , the treatment of varicocele , drainage and embolization . my sincere congratulations go to olivetti and grazioli for this fine book which clearly reflects not only their professionalism , but also their passion and enthusiasm for our discipline . in modo molto attuale e moderno la radiologia dellapparato genito - urinario dei nostri giorni . il testo si articola in nove sezioni , iniziando con lanatomia dellapparato urinario , corredata da ottimi disegni che troviamo anche in alcuni capitoli successivi . 
allanatomia classica fa seguito lanatomia radiologica comprendente lurografia , langiografia , lecografia di base , lecografia color doppler e con mezzo di contrasto , la tomografia computerizzata completa di urografia , la risonanza magnetica con langiografia rm e lurografia rm . 
seguono i capitoli di anatomia umana classica e quindi di anatomia radiologica dellapparato genitale maschile e femminile che seguono la stessa impostazione dei capitoli precedenti . le sezioni successive sono dedicate alla clinica e allimaging dei vari organi e apparati . 
guglielmi an issue of the radiologic clinics of north america volume 46 , issue 4 july 2008 elsevier - saunders , 2009 isbn 0033 - 8389 / 08 published online : 15 june 2009 springer - verlag 2009 the ageing of the population worldwide , a result of heavily declining birth rates and the steady increase in the number of elderly individuals , is creating a series of social , economic and health care problems . 
in response to the question : who is the typical geriatric patient ? hazzard some time ago answered : think of the oldest , sickest , most complicated and frail of your patients one normally affected by multiple diseases , often with atypical presentation , and by functional disabilities . 
his or her health problems are chronic , progressive , and only in part reversible . with increasing frequency , health care professionals are confronted with complex clinical scenarios arising in the same patient , which make management difficult and require special competences . 
in the elderly , and especially in geriatric patients , the coexistence of several diseases , the prevalence of involutional and degenerative aspects and a rapidly changing clinical situation together with physical and cognitive problems frequently makes it difficult for the radiologist to provide clinicians with the answers they require . in addition to being typical , all the above disturbances may also be the norm for the elderly . 
however , if we unaware of the specific normality of the elderly , we run the risk of overdiagnosis and overtreatment that is , of putting in place totally inadequate and generally excessive diagnostic and therapeutic measures that may be considered overzealous . 
 it is thus important for the radiologist to be familiar with the most common clinical scenarios in geriatric patients , which often differ from those seen in younger adults , and for the geriatrician to be aware of the potential and limits of linvecchiamento della popolazione mondiale , determinato dalla notevole riduzione del numero delle nascite e dal costante incremento del numero degli anziani , sta progressivamente determinando una serie di problemi sociali , economici e sanitari . 
alla domanda : chi il tipico paziente geriatrico ? qualche tempo fa hazzard rispose : pensa al pi anziano , al pi malato , al pi complicato ed al pi fragile dei tuoi pazienti affetto di solito da multiple malattie , la cui presentazione spesso atipica , e portatore di deficit funzionali . 
 con crescente frequenza gli operatori sanitari al giorno doggi si confrontano con complessi scenari clinici presenti nello stesso paziente , il che comporta una difficile gestione e richiede speciali competenze . 
nellanziano ed in particolare nei pazienti geriatrici , la coesistenza di pi patologie , la prevalenza di aspetti involutivo - degenerativi , una situazione clinica rapidamente mutevole assieme a problemi fisici e cognitivi frequentemente rendono difficile al radiologo fornire ai clinici le risposte che talvolta si aspettano . tutti questi disturbi , oltre ad essere tipici sono nella norma per lanziano ; quindi nellambito della radiologia geriatrica importante sapere distinguere lanziano sano da quello bisognevole di cure , poich quasi tutti si lamentano di qualche disturbo , ma talvolta non conoscendo la normalit specifica dellanziano si corre il rischio di sconfinare nellover diagnosis e nellover treatment , cio di mettere in atto interventi diagnostici e terapeutici del tutto inadeguati , il pi delle volte eccessivi e tali da configurare il cosiddetto accanimento . 
 importante per i radiologi conoscere le situazioni cliniche di pi comune riscontro nel paziente geriatrico , che sono spesso differenti da quelle osservabili negli adulti pi giovani , e per i geriatri essere a conoscenza delle potenzialit e dei limiti della moderna radiologia e delle sue appliradiol med ( 2009 ) 114 : 662663 modern radiology and its applications in geriatric patients . edited by giuseppe guglielmi , this issue of radiologic clinics of north america consists of 11 chapters that , supported by up - to - date references , review all aspects of imaging elderly patients , including the most common cardiovascular , gastrointestinal , neurological , oncohaematological , genitourinary and metabolic disorders . 
questo volume della collana radiologic clinics of north america , coordinato da giuseppe guglielmi , comprende 11 capitoli supportati da una aggiornata bibliografia che focalizzano lattenzione su tutti gli aspetti dellimaging nel paziente anziano , passando in rassegna le pi comuni problematiche cardiovascolari , respiratorie , gastrointestinali , neurologiche , onco - ematologiche , genito - urinarie e metaboliche . 
nieder springer - verlag berlin heidelberg , 2008 isbn 978 - 3 - 540 - 77384 - 9 e - isbn 978 - 3 - 540 - 77385 - 6 in this 650 - pages book written by experts in the field and edited by well - known and respected profs . 
lu and brady the reader will find forty - six chapters divided into 12 sections . the aim of the book is to present to the reader namely radiotherapy experts or radiotherapists in training as well as clinicians an evidence - based approach to the subject . the concept of evidence - based medicine and radiotherapy is explained well in the 16 - page introduction written by the two editors and described throughout the book in the framework of each chapter , according to the type of evidence level and grade of recommendations as found and described in the literature according to tumour type . 
both concepts are delineated well and relevant information for the reader is presented throughout the text . each chapter opens with a summary of important information on introduction and objectives ( clearly indicated in a blue box ) : then different colours are used to highlight the text headings ( blue for diagnosis , staging and prognosis ; red for treatment radiation , surgery , chemotherapy ; green for follow - up and surveillance ) and are summarised in a large algorithm . relevant tables for imaging , laboratory work - ups for diagnosis , tumour typing and tumour tables according to the ajcc and / or who classifications are also listed . an unusually large reference list closes each chapter , some references are as recent as to 2008 . 
 the subject index and two appendixes , one for performance status scales , the other for estimated normal tissue tolerance dose are at the end of the text . throughout the text acronyms are extensively used and this is a source of disappointment since sometimes ( yet not always ! ) their explanation is found later in the text . 
a list of abbreviations would have been useful and is recommended quarantasei capitoli suddivisi in 12 sezioni costituiscono le 650 pagine di questo libro scritto da una serie di esperti nel campo sotto la direzione dei ben noti professori lu e brady . 
 scopo del volume di presentare al lettore soprattutto radioterapisti esperti ed in via di specializzazione e tirocinio , come anche ai clinici un approccio basato sullevidenza riguardo alla materia in studio . il concetto di medicina e radioterapia basate sullevidenza ben spiegato nelle 16 pagine di introduzione a firma dei curatori del volume ed di continuo riscontro nella struttura e nel testo di ciascun capitolo , in funzione del tipo di livello di evidenza e del grado di raccomandazione trovato e descritto nella letteratura e nella pratica clinica per ciascun tipo di tumore . 
entrambi sono ben evidenziati e di importante informazione per il lettore in tutto il testo . ogni capitolo aperto da un riquadro dallo sfondo blu , contenente importanti informazioni circa lintroduzione e gli obiettivi dello stesso . 
poi colori differenti caratterizzano i titoli dei sottocapitoli ( blu per la diagnosi , stadiazione e prognosi ; rosso per la terapia radiante , chirurgica , chemioterapica ; verde per i controlli e la sorveglianza nel tempo ) e sono ripresi nella ampie figure degli algoritmi . vi sono poi tabelle circa le modalit degli studi per immagine , degli esami di laboratorio da eseguire a seconda del tipo di tumore in studio nonch le tabelle con gli elenchi dei sistemi di stadiazione degli stessi secondo le classificazioni della ajcc e / o del who . un elenco di voci bibliografiche sempre piuttosto lungo e talvolta aggiornato fino al 2008 chiude ciascun capitolo . 
il volume termina con lindice analitico e due appendici , una riguardo allo stato di rendimento del paziente , laltro al livello stimato di dose di tolleranza dei tessuti normali . in tutto il testo luso degli acronimi frequente e diffuso ed causa di insoddisfazione dato che la spiegazione degli stessi spesso ( ma talvolta neppure ) rintracciabile a distanza dalla prima citazione . 
pescarini3 1istituto nazionale di riposo e cura dellanziano ( inrca ) sede di roma , via cassia 117 , 00189 roma , italy 2istituto di medicina del lavoro delluniversit cattolica del sacro cuore roma , italy 3istituto oncologico veneto irccs dipartimento di scienze oncologiche e chirurgiche delluniversit degli studi di padova , padova , italy correspondence to : a . 
fileni , via cassia 1167 , 00189 roma , italy , tel . : + 39 - 06 - 30342519 , fax : + 39 - 06 - 30363596 , e - mail : a.fileni@inrca.it received : 12 june 2008 / accepted : 16 september 2008 / published online : 14 may 2009 springer - verlag 2009 abstract purpose . 
the study considered insurance claims filed by radiologists of the italian society of medical radiology ( sirm ) over a 12.5 - year period between 1 january1993 and 30 june 2005 . 
the analysis uncovered a complex problem : although radiologists save many lives through the radiographic diagnosis of breast cancer and consequently contribute to the welfare of society , in practice , they can face real or alleged errors , with serious judicial consequences . 
lo studio riguarda le denunce assicurative dei radiologi iscritti alla sirm dal 01 / 01 / 1993 al 30 / 06 / 2005 per un periodo di 12 , 5 anni . 
nellipotesi che la tendenza a denunciare i radiologi sia costante , si prevede che per il periodo dosservazione giungano ancora 637 nuovi casi , per un totale complessivo di 1725 . per lo studio radiografico della mammella sono attese altre 178 denunce . 
bench il radiologo con la diagnosi mammografica dei tumori della mammella salvi molte vite , contribuendo al bene della societ , nella pratica pu incorrere in errori veri o presunti , con conseguenze giudiziarie sempre pi incombenti . 
 parole chiave mammella denunce mammografia radiologi introduction introduzione from a study of a cohort of radiologists comprising more than half those enrolled in the italian society of medical radiology ( sirm ) , it emerges that failure to diagnose breast cancer is the most frequent cause of medicolegal litigation , which has considerably increased over the past 12 years [ 1 ]  . starting from an analysis of epidemiological data concerning malpractice liability claims against radiologists , we sought to examine error as an adverse event in breast cancer diagnostics with a view to uncovering critical areas and identifying possible strategies to control the malpractice risk connected to the performance of mammography . materials and methods the claims filed by italian radiologists insured through the sirm professional liability insurance scheme were anonymously reviewed . 
the number of insured radiologists increased steadily from 1 , 400 at the beginning of the study period to 4 , 490 in 2005 , for a total of 35 , 081.5 persons / year ( radiologists insured over an entire calendar year )  . 
the incidence and prevalence of claims relating to breast cancer were calculated for the period being examined . to account for the fact that claims for presumed diagnostic errors are lodged after a variable time interval , at times close to the expiry of the prescriptive period for compensation ( 10 years from the event ) , we estimated the number of insurance claims expected to be filed until the end of the prescriptive period by using a method described in a previous paper [ 1 ]  . 
first , starting from the assumption that the tendency to sue physicians is constant over time , we assumed that the trend of claims between 1993 and 1995 , once the effect of late claims was eliminated , expressed the constant trend of claims in the cohort . we then calculated the cumulative percentage of claims filed after 1 , 2 , 3 or more years in the period prior to 1995 . those cumulative percentages were applied as coefficients to the current observations . 
 dallo studio di una coorte di radiologi italiani pari ad oltre la met dei radiologi iscritti alla societ scientifica ( societ italiana di radiologia medica ) risulta evidente che la denuncia per mancata diagnosi di tumore della mammella la causa di contenzioso medico - legale che ha registrato il maggiore incremento negli ultimi dodici anni [ 1 ]  . 
muovendo dallanalisi dei dati epidemiologici relativi alle denunce di responsabilit civile contro i radiologi , ci si proposti di esaminare lerrore quale evento avverso nella diagnostica del tumore della mammella , al fine di riconoscere le problematiche relative e di identificare le possibili strategie per il controllo del rischio di malpractice connesso allesecuzione degli esami mammografici . materiali e metodi sono state analizzate in forma anonima le denunce assicurative sporte dai radiologi italiani che hanno sottoscritto lassicurazione professionale con la sirm . 
gli assicurati , in numero di 1400 allinizio del periodo dosservazione , sono progressivamente aumentati fino a 4490 nel 2005 ; complessivamente quindi le persone / anno ( radiologi assicurati per un intero anno solare ) sono 35081 , 5 . 
si proceduto al calcolo del tasso dincidenza e del tasso di prevalenza nel periodo delle denunce per neoplasia mammaria . per ovviare al fatto che le denunce per i presunti errori diagnostici sono presentate a distanza di tempo variabile dallevento , talvolta anche ai limiti della prescrizione della risarcibilit ( dieci anni ) , si proceduto a stimare il numero delle denunce che perverranno entro i termini di prescrizione con un metodo gi applicato in passato [ 1 ]  . 
in primo luogo , partendo dallipotesi che la propensione a denunciare i medici radiologi sia costante nel tempo , stato assunto che landamento delle denunce nei primi anni dosservazione , tra il 1993 ed il 1995 , una volta esaurito leffetto delle denunce landamento costante delle denunce nella coorte . 
 stata quindi la percentuale cumulativa delle denunce calcolata tardive , esprima 638 results in the study period , 1 , 088 malpractice claims were filed against radiologists ( table 1 ) , 302 of which originated from alleged failure to diagnose cancer . 
of these , 189 ( 62% ) were in regard to breast cancer and mammographic examinations ( table 2 ) , and two to mammography but not breast cancer . comparison with all other cancer sites demonstrated the criticality of mammographic diagnostics ( table 2 )  . 
clearly , in view of the time required for cases to go through three levels of courts in italy , one cannot know whether the event was a consequence of the doctors actions . 
 risultati nel periodo in esame ( 01 / 01 / 199330 / 06 / 2005 ) sono state sporte 1088 denunce contro i radiologi ( tabella 1 ) , di cui 302 originate da presunti errori diagnostici per neoplasie . centottantanove di tali denunce ( 62% ) riguardano la patologia tumorale della mammella e la relativa indagine mammografica ( tabella 2 )  . 
ai fini assicurativi , comunque , questo aspetto irrilevante , in quanto lentit dei premi richiesti al singolo assicurato non commisurata tanto alle somme effettivamente erogate dallente assicuratore , quanto alle richieste di risarcimento della controparte . tenuta ferma lipotesi che la propensione a denunciare i radiologi sia rimasta costante nel periodo dosservazione , stato esaminato separatamente landamento delle denunce degli anni per i quali si concluso il periodo per la prescrizione ( 10 anni )  . 
 stato cos possibile rilevare che solo il 19% delle denunce si riferisce ad eventi occorsi nello stesso anno , mentre nella maggior parte dei casi levento avvenuto in epoche precedenti , fino a 10 anni prima ( tabella 3 )  . landamento storico stato pertanto utilizzato per stimare il numero di denunce che ci si attende pervenga per il periodo di osservazione . 
si ottiene cos la previsione che il numero totale possa raggiungere le 1725 unit , per ulteriori 637 denunce per tutte le cause in aggiunta a quelle finora pervenute ( tabella 4 )  . 
 stata valutata la frequenza di ciascuna categoria delle cause di denuncia , ad uno e pi anni dal sinistro , in modo da stimare a quale gruppo apparterranno le denunce previste in futuro . 
the results indicated that only 19% of claims were related to events that occurred during the same year , whereas the majority of claims were related to events occurring during previous years , up to 10 years earlier ( table 3 )  . 
the total number of claims may reach 1 , 725 , as a further 637 claims for all causes are expected in addition to those already lodged ( table 4 )  . 
the percentage of claims regarding breast cancer filed more than 1 year after the first was 28% of the total ; thus , a further 178 claims relating to breast cancer are expected . 
the mean amount requested for each professional liability claim was 405 , 000 euro , an amount that rose over the last years of the study period . pari al 28% del totale ; si attendono quindi ulteriori 178 denunce per neoplasia mammaria . 
la prevalenza delle denunce gi pervenute , originate da neoplasie mammarie nel periodo in esame , pari al 5 , 4 per mille ( 189 casi per 35081 , 5 persone / anno )  . 
se sar confermata la previsione circa le denunce che saranno ricevute nei prossimi anni , sempre riferite al periodo in esame , si raggiunge un tasso del 10 , 5 per mille . 
limporto medio delle richieste per ciascun procedimento di responsabilit civile stato di 405000 euro ; tale importo in aumento negli ultimi anni dosservazione . discussione i dati esposti corrispondono al rischio malpractice relativo allindagine mammografica e conseguente ad una mancata diagnosi di neoplasia della mammella . 
il notevole incremento di denunce negli anni considerati indica una criticit assoluta che riguarda i radiologi rappresentati nel campione dai numerosi soci della societ scientifica italiana sirm , che scelgono la copertura della polizza assicurativa collegata alliscrizione annuale . lo studio , attendibile quindi per numero e omogeneit , in linea con lindagine di farria [ 2 ] negli usa , tenuto conto di alcune diversit note quali la mentalit , il sistema sanitario e il tasso di litigiosit pi elevato oltreoceano . 
the marked rise in claims over the study period indicates an absolute criticality regarding the radiologists in our sample , that is , members of the sirm who have chosen to subscribe to the professional liability insurance policy attached to the yearly sirm membership . the study , which is robust in terms of sample number and uniformity , is in line with the survey conducted by farria et al . 
if the likelihood of being subject to litigation in italy is equal to one case every 10 years per radiologist , the situation in the usa is even more dramatic : no less than legale in italia di un evento ogni 10 anni per radiologo , negli usa la situazione ancora pi drammatica : ben il 55% dei radiologi occupati in senologia ha ricevuto una denuncia con richiesta dindennizzo negli ultimi 5 anni . inoltre , in un sistema sorretto da strutture private , pi di un terzo delle aziende sanitarie che eseguono mammografie ha chiuso in passivo lultimo esercizio finanziario tanto da sospendere o ridurre il servizio , con un riflesso immediato sul prolungamento delle liste dattesa . 
ancora , unindagine condotta sulla formazione dei radiologi [ 3 ] indica che una delle ragioni principali per non impegnarsi nellattivit mammografica rappresentata dallo stress che si verifica nella visione e interpretazione dei radiogrammi per il timore di denunce . 
additionally , in a system supported by private facilities , more than one third of breast - imaging practices incurred financial losses over the last year to the point that the service was discontinued or reduced , with the immediate effect of longer waiting lists . another survey conducted on radiologist training [ 3 ] indicates that one of the main reasons for not entering the field of breast imaging is the stress related to viewing and interpreting mammograms for the fear of malpractice lawsuits . all this has a negative influence on the practice of radiology , leading to forms of defensive medicine with requests for further investigations or at times with organised aspects such as the publication of databases of the most litigious patients . 
the phenomenon is of great concern in italy owing to the unnecessary costs incurred by the healthcare system as a result of defensive medicine practices [ 46 ]  . the results also show that although the majority of claims related to mammography concerns public facilities , aspetti talora organizzati , quali la pubblicazione di database dei pazienti pi litigiosi . 
il fenomeno di enorme interesse anche nel nostro paese per i costi sostenuti inutilmente dal sistema sanitario a causa della medicina difensiva [ 46 ]  . dai risultati emerge ancora che per quanto riguarda le denunce per la mammografia , bench il maggior numero delle denunce riguardi le strutture pubbliche , vi una litigiosit per esami condotti presso strutture private che appare relativamente elevata in funzione dei minori volumi di attivit : ci potrebbe indicare una maggior propensione al contenzioso da parte delle donne che hanno scelto il professionista e pagato direttamente la prestazione . il riscontro del 69% di casi con decesso indica la gravit della malattia tumorale nei casi che danno origine a denuncia . 
poich la nostra indagine circoscritta alle richieste di assistenza avanzate dai radiologi in risposta alle citazioni , e corrisponde quindi solo allinizio del contenzioso , non possibile sapere se nella realt vi sia 642 radiol med ( 2009 ) 114 : 636644 there is also some degree of litigiousness for examinations performed at private facilities , which appears relatively high in proportion to their small work volumes . 
this could indicate a greater tendency to litigate on the part of women who have chosen their specialist and paid for the service themselves . the finding of 69% of claims in relation to deceased patients reflects the severity of the cancer in the cases producing the claims . 
because our survey is confined to requests for assistance by radiologists who have received summons and thus corresponds only to the early stages of the litigation proceedings , we cannot know whether there indeed was a failure to diagnose the cancer and whether this caused harm to the patient . 
 it should be recalled that apart from possible human error [ 7 ] , the possibility of a false negative ( fn ) result should always be considered in mammography . 
in the self - assessment test of the 2002 sirm national congress [ 10 ] , which may be considered as a test on the mammographic performance of the average italian radiologist , the rate of fn was 31% . 
 [ 11 ] used a test investigating lesion detection and number of recalls , reporting than only 32.7% of radiologists passed at the first attempt . the absolute prevalence of fn cases in mammography also defines the type of error for which the radiologist is sued . 
italian radiologists , like their us counterparts , are sued for not having detected and / or interpreted a mammographic lesion that subsequently turned out to be malignant [ 12 ]  . 
over the past few decades , they are prevalently related to omissive behaviour . in other words , whereas in the past radiologists were sued for having done something wrong , today , they are sued for not having done something appropriate [ 13 ]  . 
 given the considerable possibilities of an increasingly technological medicine , the failure to make use of further investigation methods by those performing and reporting dubious mammographic examinations is the source of claims due to omission . 
on this topic , neither economic nor procedural justifications are normally accepted in court , even when supported by community health interventions that have been validated by an evident reduction in mortality , as occurs in classic screening programmes [ 14 ]  . integrated diagnostics an application that has always resisted in its cultural perspective of maximal clinical effectiveness [ 15 ] with the recent proposal for customised stata una mancata diagnosi e se questa ha determinato un danno alla paziente . 
fanno testo le autorevoli dichiarazioni di kopans [ 8 ] la mammografia non sempre porta a diagnosticare i tumori mammari e di mavroforou [ 9 ] anche ai radiologi pi esperti possono sfuggire lesioni maligne . gli studi in materia sui radiologi italiani mettono evidenza anche lentit delle mancate diagnosi . 
nel test di autovalutazione del congresso nazionale della sirm dellanno 2002 [ 10 ] , che pu essere inteso come verifica della prestazione in mammografia del radiologo medio italiano la quota di fn del 31% . 
 [ 11 ] , con un test tarato sia sul rilevamento delle lesioni che sul numero degli eventuali richiami , segnalano che solo il 32 , 7% dei radiologi in grado di superare la prova al primo approccio . lassoluta prevalenza de casi fn in mammografia definisce in generale anche la tipologia dellerrore per il quale il radiologo chiamato in causa . 
i radiologi italiani , analogamente a quanto avviene negli usa , sono chiamati in giudizio per non aver saputo riconoscere e / o interpretare una lesione mammografica poi rivelatasi maligna [ 12 ]  . 
in sostanza mentre un tempo il radiologo subiva un procedimento per aver fatto qualcosa di sbagliato , oggi lo per non aver fatto qualcosa di appropriato [ 13 ]  . 
 a fronte delle ampie possibilit di una medicina sempre pi tecnologica , il mancato ricorso ad ulteriori metodiche dindagine da parte di chi ha eseguito e refertato lesame mammografico dubbio origina la denuncia di comportamenti omissivi . 
a riguardo , in sede di giudizio , non sono di regola accolte giustificazioni n economiche n procedurali , anche se sostenute da logiche di intervento sanitario di tipo collettivo gi validate da evidente riduzione della mortalit , come avviene nei programmi di screening classico [ 14 ]  . la diagnostica integrata , aspetto applicativo che resiste fin dai primordi nella sua prospettiva culturale di massima efficacia clinica [ 15 ] e con la recente proposta di modelli organizzativi personalizzati [ 16 ] , rappresenta la modalit dapproccio personale pi consona ad evitare censure supportate da omissioni . 
in un recente studio policentrico , lincremento del numero di neoplasie diagnosticate con radiol med ( 2009 ) 114 : 636644 organisation models [ 16 ] constitutes the most suitable personal approach for avoiding litigation caused by omission . 
in a recent multicentre study , the increase in the number of cancers diagnosed through the systematic use of ultrasound combined with mammography in women at high risk was not considered sufficient to compensate for the increased expenditure , the use of highly qualified personnel and the inevitable increase in false positive results [ 17 ]  . the long latency between the diagnostic service and the possible claim indicates a need to seek prospective insurance coverage . 
claims - made policies , for example , while less costly , offer coverage only for claims relating to events that occurred during the policy year and up to a short time thereafter and are therefore unsuitable for protecting against civil liability claims lodged several years after the service was rendered , at times even after retirement . 
another type of policy ( known as loss occurrence ) covers for all claims filed in relation to events that occurred within the policy year and up to the expiry of the 10 - year prescriptive period . it should also be noted that some types of malpractice claims are not covered by the insurance policy . 
 the mean amount of damages , 405 , 000 euro , which appears fairly high , is rising , and this will lead to an increase in insurance premiums unless drastic reforms are made to the healthcare compensation syste to this end , both medical councils and professional medical associations are urging the government to review the judicial and institutional aspects of medical liability in italy . 
in the field of mammography , a recent document of the italian ministry of health [ 18 ] draws attention to all the issues regarding alleged interpretation errors in the reading of mammograms and the finding of interval cancers . 
the document notes that the indications provided for predicting and minimising errors in a context of clinical risk management are inadequate to avert the risk of litigation , in which the review process is usually influenced by the retrospective method of judicial evaluation . limpiego sistematico dellecografia associata alla mammografia in donne a rischio , non stato ritenuto sufficiente a compensare lesborso economico , limpiego di personale altamente qualificato , e linevitabile aumento dei falsi positivi [ 17 ]  . lelevato intervallo di tempo tra la prestazione e leventuale denuncia indica la necessit di provvedere ad una copertura assicurativa valida in termini prospettici . 
le polizze claims made ad esempio , economicamente meno onerose , coprono solo le denunce pervenute nellanno assicurato , o in un breve periodo successivo , e si rivelano quindi inadatte a tutelare dalle denunce di responsabilit civile sporte a distanza di numerosi anni dallesecuzione della prestazione , eventualmente anche dopo la cessazione dellattivit professionale . 
 limporto medio di richiesta dindennizzo di 405000 euro , che gi appare piuttosto elevato , tende a crescere e , con esso , cresceranno i premi richiesti dalla compagnie assicurative , a meno di drastiche riforme del sistema risarcitorio medico - sanitario . 
in campo mammografico un recente documento del ministero della sanit [ 18 ] mette in evidenza tutte le problematiche riguardanti gli errori interpretativi supposti nella lettura della mammografia e il riscontro dei cancri dintervallo . 
si osserva nel documento che le indicazioni a prevedere e a contenere lerrore nellambito della gestione del rischio clinico non appaiono sufficienti a scongiurare il pericolo di un procedimento , nel quale le modalit di revisione risentono di solito di una metodologia di valutazione giudiziaria influenzata dal senno del poi . conclusioni conclusions analysis of professional liability claims filed against italian radiologists in relation to mammography indicates the presence of an extensive and complex problem : on the one hand , the radiologists personal commitment to a field where many lives can be saved and , on the other , the risk of facing the legal consequences of real or alleged errors . 
twenty - six consecutive patients , 14 with liver metastases ( ten from colorectal cancer ; four from carcinoid tumours ) and 12 with biliary cancers ( ten klatskin tumours ; one gallbladder tumour ; one intrahepatic cholangiocarcinoma ) with insufficient predicted future remnant liver ( frl ) underwent right pve to induce hypertrophy of the contralateral hemiliver prior to surgical resection . 
the frl volume increased by 5%25% ( 15% on average ) after right pve in patients with liver metastases and by 9%19% ( 14% on average ) in patients with biliary cancers . 
in all patients , the ratio of frl to functional liver volume was 30% after right pve . no postoperative deaths due to severe liver failure occurred in the 20 patients who underwent extended hepatectomy . 
lo scopo del nostro studio retrospettivo stato di valutare lefficacia dellembolizzazione del ramo portale destro ( rpve ) come trattamento pre - chirurgico per indurre lipertrofia del fegato sinistro in pazienti candidati a resezione epatica . 
ventisei pazienti consecutivi , 14 portatori di metastasi epatiche ( colon - retto , 10 pazienti ; carcinoide , 4 pazienti ) e 12 portatori di neoplasia delle vie biliari ( neoplasia di klatskin , 10 pazienti ; neoplasia della colecisti , 1 paziente ; colangiocarcinoma intraepatico , 1 paziente ) con potenziale riserva funzionale epatica ( frl ) insufficiente sotto stati sottoposti a rpve come trattamento pre - chirurgico . 
il volume del frl ha dimostrato un incremento volumetrico compreso tra il 5%25% ( 15% in media ) dopo rpve nei pazienti con metastasi epatiche e tra il 9%19% ( 14% in media ) in pazienti con neoplasie biliari . 
lembolizzazione portale allarga le indicazioni alla chirurgia resettiva epatica in pazienti con metastasi epatiche e neoplasie delle vie biliari con potenziale riserva funzionale insufficiente . 554 radiol med ( 2009 ) 114 : 553570 keywords right portal vein embolisation hepatic functional reserve ct hepatic volumetry parole chiave embolizzazione del ramo portale destro riserva funzionale epatica tc volumetria epatica introduction introduzione the curative treatment of primary and secondary liver cancers that ensures long - term survival is surgery . 
more than 45% of liver tumours , both primary and secondary , require extended liver resection with disease - free margins . postoperative death after extended hepatectomy , which ranges from 3.2%7% in patients with a normal hepatic functional reserve to 32% in patients with cirrhosis , is most often caused by an insufficient future remnant liver ( frl )  . postoperative liver failure has been shown to be directly related to frl volume , and preoperative procedures to induce liver regeneration have been proposed [ 13 ]  . 
on the basis of experimental studies in 1920 that showed that ligation of a portal branch led to atrophy of the ipsilateral liver parenchyma and hypertrophy of parenchyma with preserved portal flow , makuuchi et al . 
 [ 4 ] in 1990 used portal occlusion as a preoperative treatment to extend the indication for curative liver resection to patients with biliary cancers . embolisation of a portal branch is currently indicated when the volume of the predicted frl is insufficient to ensure an adequate postoperative hepatic functional reserve . 
separate determinations of liver volume and tumour volume makes it possible for hepatic functional reserve to be estimated with computed tomography ( ct ) and magnetic resonance ( mr ) imaging by subtracting tumour volume from total liver volume , i.e. 
the potential functional reserve of frl as a ratio between the frl and the total functional liver mass . the purpose of this retrospective study was to assess the effectiveness of right portal vein embolisation ( pve ) as a preoperative treatment in noncirrhotic patients in whom the predicted functional reserve of the frl , calculated with ct , was insufficient for radical liver resection . 
in pi del 45% dei tumori del fegato , sia primitivi che secondari , necessaria unampia chirurgia resettiva epatica che assicuri margini di resezione liberi da malattia . la principale causa di morte post - chirurgica dopo epatectomie estese , che oscilla tra il 3 , 2% e 7% nei pazienti con normale riserva funzionale epatica e fino al 32% nei pazienti con cirrosi , spesso un insufficiente future remnant liver ( frl )  . 
stato dimostrato che linsufficienza epatica post - chirurgica direttamente correlata al volume del frl e sono state proposte procedure pre - chirurgiche che inducono la rigenerazione epatica [ 13 ]  . 
sulla base di studi sperimentali che nel 1920 avevano dimostrato che la legatura di un ramo portale determinava latrofia del parenchima epatico tributario e lipertrofia del parenchima epatico con flusso portale conservato , makuuchi et al . 
 [ 4 ] gi nel 1990 hanno usato per primi locclusione portale come trattamento pre - chirugico per ampliare lindicazione a chirurgia resettiva epatica curativa in pazienti portatori di neoplasie delle vie biliari . 
lembolizzazione di un ramo portale attualmente indicata quando il volume del potenziale frl inadeguato ad assicurare unadeguata riserva funzionale epatica postchirurgica e quindi il calcolo della volumetria epatica necessario per selezionare i pazienti da sottoporre a trattamento pre - chirurgico . 
il calcolo separato del volume epatico e del volume tumore permette oggi alla tomografia computerizzata ( tc ) ed alla risonanza magnetica ( rm ) di valutare la riserva funzionale epatica sottraendo al volume totale epatico il volume tumore e quindi la potenziale riserva funzionale del frl come rapporto del frl sulla massa epatica totale funzionante . scopo primario di questo studio retrospettivo di valutare lefficacia dellembolizzazione del ramo portale destro ( rpve ) come trattamento pre - chirurgico in pazienti non cirrotici nei quali la potenziale riserva funzionale del frl , calcolata mediante tc , era insufficiente per una chirurgia resettiva epatica oncologicamente radicale . 
 materials and methods materiali e metodi between november 1996 and september 2007 , 26 noncirrhotic patients ( 12 men and 14 women , aged 3581 years ; mean age 58 years ) underwent pve procedures . 
dodici pazienti erano portatori di neoplasie delle vie biliari [ 5 ] : neoplasia di klatskin ( 10 pazienti ) classificati secondo bismuth come tipo ii ( interruzione convergenza biliare principale , 6 pazienti ) , tipo iiia ( interruzione radiol med ( 2009 ) 114 : 553570 confluence , n = 6 ) , type iiia ( obstructed main confluence extending to the right secondary confluence , n = 2 ) , type iv ( obstructed primary and secondary confluence bilaterally , n = 2 ) , gallbladder cancer ( n = 1 ) and intrahepatic cholangiocarcinoma ( n = 1 )  . 
in particular , the lesions were located in the right liver lobe and in segment iv in three patients ( two with colorectal metastases and one with carcinoid metastases ) and in the right liver lobe in segments iv and ii in two patients ( one with colorectal metastases one with carcinoid metastases )  . 
all patients with hepatic metastases from colorectal cancer underwent chemotherapy ( three to six cycles , four cycles on average ) , with partial response ( no less than 30% ) according to the response evaluation criteria in solid tumours ( recist ) criteria [ 6 ] or with stable disease . 
in the patient with bilobar colorectal metastases in segments ii and iv of the left liver , right pve was preceded by excision of the left lobar metastases , a procedure known as two - stage hepatectomy . 
all patients with klatskin tumours underwent percutaneous biliary drainage bilaterally ( n = 6 ) or on the left side only ( n = 4 ) ; a prerequisite for right pve was biliary drainage of the frl with reduction of bilirubin ( < 3 mg / dl )  . 
in particolare le lesioni erano localizzate nel fegato destro e nel iv segmento epatico in 3 pazienti ( 2 da neoplasia colo - rettale e 1 da carcinoide ) ; nel fegato destro , nel iv e nel ii segmento in 2 pazienti ( 1 da neoplasia colo - rettale e 1 da carcinoide )  . tutti i pazienti portatori di metastasi epatiche da neoplasie colo - rettali hanno effettuato chemioterapia ( 36 cicli con una media di 4 cicli ) con una risposta parziale ( non inferiore al 30% ) secondo i criteri recist ( response evaluation criteria in solid tumours ) [ 6 ] o con malattia stabile , che ha preceduto lembolizzazione portale con un intervallo di tempo di almeno 28 giorni . 
nel paziente portatore di metastasi bilobari da neoplasia colo - rettale , localizzate nel fegato sinistro , in corrispondenza del ii oltre che nel iv segmento , la rpve stata preceduta dalla metastesectomia delle metastasi del fegato sinistro , two stage hepatectomy . 
i pazienti con metastasi da carcinoide non sono stati sottoposti a terapia neo - adiuvante : quando possibile , la resezione epatica rappresenta in questi pazienti il miglior trattamento in termini di sopravvivenza a lungo termine [ 7 ]  . tutti i pazienti portatori di neoplasie di klatskin sono stati sottoposti a drenaggio biliare per via transcutanea dei due emisistemi biliari ( 6 pazienti ) o dellemisistema di sinistra ( 4 pazienti ) ; presupposto indispensabile alla rpve stato il drenaggio biliare del frl con riduzione dei valori ematici di bilirubina ( non superiore a 3 mg / dl )  . 
 nel periodo compreso tra il 1996 ed il 2003 gli esami tc sono stati eseguiti in 11 pazienti con tc spirale singolo strato prospeed advantage ( ge medical systems , milwaukee , wis , usa ) come precedentemente descritto [ 8 ]  . nel periodo compreso tra il 2003 ed il 2007 gli esami tc sono stati eseguiti in 15 pazienti mediante tc spirale multistrato lightspeed pro 16 ( ge medical system ) , utilizzando i seguenti parametri : ma automatico ( noise index 14 ) , 120 kvp , collimazione dei detettori 1 , 25 , velocit del tavolo 18 , 75 mm per rotazione , velocit di rotazione del gantry 0 , 6 secondi a rotazione . 
sono stati utilizzati uno spessore di ricostruzione di 2 , 5 mm ed un intervallo di ricostruzione di 2 , 5 mil mezzo di contrasto ( 2 ml / kg di peso corporeo con una concentrazione di 350 mgi / ml ) stato somministrato per via ev attraverso lutilizzo di un iniettore automatico , ad una velocit di 45 ml / s attraverso un ago - cannula di 18 gauge posta in una vena del braccio . 
la scelta dei tempi di ritardo per lacquisizione delle immagini stata ottenuta mediante lutilizzo di un sistema automatico di bolus tracking che prevedeva un singolo sistema di monitoraggio a bassa dose posto a livello di un vaso dinteresse ( aorta addominale ) dopo circa 10 secondi dallinizio delliniezione del mezzo di contrasto ; raggiunto un picco di enhancement di circa 80 uh nella regione dinteresse , circa 10 secondi dopo iniziava lacquisizione della fase arteriosa . 
le fasi portali e tardive venivano calcolate a 70 e 180 secondi dalliniezione del mezzo di contrasto . 556 radiol med ( 2009 ) 114 : 553570 number , location and volume of the liver metastases as well as the resectability criteria based on the evaluation of vascular relationships ensuring adequate perfusion , and venous and biliary drainage of the frl . 
in no patient did the ct scan provide a ratio of hepatic to splenic parenchyma density ratio 1.1 , an indication of moderate - to - severe ( 30% ) steatosis [ 9 , 10 ]  . all patients with klatskin tumours underwent mr cholangiography ( 1.5 - tesla , horizon advantage system , ge medical systems ) to stage the biliary disease . 
volumetric data were obtained from the portal - venous - phase scans , and all examinations were processed by two radiologists on a workstation ( ge medical system 4.1 ) that automatically calculated the volume by multiplying the area by the thickness and also generated 3d reconstructions . the liver parenchyma was isolated from surrounding tissues by using the cursor , and the total liver volume was calculated . 
frl was jointly determined by surgeons and radiologists on the basis of disease extent on imaging ( number , site , vascular relationships of metastases and vascular relationships of biliary cancers ) and according to the surgical plan defined by the surgeons . 
in the volumetric assessment the suprahepatic veins , the teres ligament , the umbilical portion of the left portal branch , the gallbladder and the inferior vena cava were used as anatomical landmarks to delineate the liver segments and separate the liver to be resected from the frl . 
tumour volume was not calculated in patients with biliary cancers , as small size and predominantly biliary involvement made it irrelevant to the evaluation of the ratio of frl volume to total volume of nontumourous liver parenchyma . 
the catheter was advanced to the portal trunk and , after the injection of contrast material , portography was performed to identify the intrahepatic portal branches and any anatomical variants . 
all patients underwent a ct scan 1 week before right pve and , after right pve , within a week before surgery . selection criteria for pve was an frl / total functional liver parenchyma ratio 30% . 
where waiting times exceeded 1 month , this was related to one patient with liver metastases refusing surgery for 2 months , and to our deferring surgery to after having solved the lesame tc prima e dopo rpve ha fornito il numero , la sede , il volume delle metastasi epatiche ed i criteri di resecabilit , basata sulla valutazione dei rapporti vascolari che assicurassero adeguata perfusione , drenaggio venoso e biliare del frl . 
in nessun paziente lesame tc ha rilevato il rapporto della densit parenchima epatico - parenchima splenico 1 , 1 , indice di steatosi moderata - grave ( superiore al 30% ) [ 9 , 10 ]  . tutti i pazienti portatori di neoplasie di klatskin hanno eseguito la colangio - rm per stadiare la malattia sul versante biliare ( stata utilizzata apparecchiatura a 1 , 5 tesla , horizon advantage ge medical systems , milwaukee , wis )  . 
i dati volumetrici sono stati elaborati dalle scansioni eseguite durante la fase portale dellenhancement vascolare e tutti gli esami sono stati elaborati da due radiologi dedicati ad una workstation ( ge medical system 4.1 ) che ci ha fornito il volume mediante il calcolo automatico dellarea x lo spessore , fornendoci anche ricostruzioni 3d . mediante un cursore stato isolato il parenchima epatico dai tessuti circostanti ed stato calcolato il volume epatico totale . 
le vene sovraepatiche , il legamento rotondo , la porzione ombelicale del ramo portale sinistro , la colecisti e la vena cava inferiore sono stati utilizzati come reperi anatomici per delineare i vari segmenti epatici e per separare nella valutazione volumetrica il fegato da resecare dal frl . 
il volume tumore non stato calcolato nei pazienti con neoplasie delle vie biliari per le piccole dimensioni e per il prevalente coinvolgimento biliare , quindi non stato considerato rilevante nella valutazione del rapporto tra volume del frl e volume del parenchima epatico totale funzionante . 
 lembolizzazione del ramo portale destro stata effettuata dopo puntura sotto guida ecografica del ramo portale di sinistra a livello del recesso di rex ; il catetere ha raggiunto quindi il tronco portale e con liniezione del mdc si ottenuto una portografia per individuare i rami portali intra - epatici ed eventuali varianti anatomiche ; successivamente si occluso il ramo portale destro con le sue diramazioni con materiale embolizzante costituito da cianoacrilato e lipiodol . 
tutti i pazienti sono stati sottoposti ad esame tc entro una settimana prima della rpve e dopo rpve entro una settimana prima della chirurgia . il criterio di selezione dei pazienti da sottoporre ad rapporto embolizzazione prechirurgica frl / parenchima epatico totale funzionante inferiore al 30% . 
any volume changes in frl before and after right pve were assessed with the t test , with significance set at p < 0.001. results the injection of cyanoacrylate and lipiodol achieved complete embolisation of the right portal tree in 24 patients . in two patients , preliminary embolisation of the portal branch of segment iv to be resected according to the surgical plan was achieved . 
 the increase a significant change ( p < 0.001 ) in frl volume after right pve was obtained both in patients with liver metastases and in those with biliary cancers . 
in nine patients with hepatic colorectal metastases , in frl volume ( 18571.16 cm3 ) after 2548 days ( 33.8 days on average ) associated with atrophy of the functional liver parenchyma to be resected ( 186.196.62 cm3 ) changed the frl / total functional liver - volume ratio from 18%29% ( 25% on average ) before right pve to 30%51% ( 39% on average ) after right pve . 
after right pve , the volume of the metastases from colorectal cancer in the embolised liver increased by 6%155.5% , whereas in the patient who waited 60 days , the tumour increased in volume by 562.7% ( table 1 )  . 
patients with metastases from carcinoid tumours showed no increase in volume of metastases after right pve in either the embolised or unembolised liver , whereas frl hypertrophy ( 283.7570.1 cm3 ) significantly changed liver parenchyma ratio from 20%27% to 42%52% ( table 1 ) after a period of 3034 days ( 31 days on average )  . 
after a period of 3180 days ( 45.9 days on average ) after right pve , frl hypertrophy ( 187.1671.5 cm3 ) and atrophy of the parenchyma to be resected ( 305.7182.5 cm3 ) changed 30%45% ( table 2 )  . 
le variazioni volumetriche del frl prima e dopo rpve sono state valutate mediante il test t di student ( un valore di p < 0 , 001 stato considerato significativo )  . risultati mediante liniezione di cianoacrilato e lipiodol si ottenuta lembolizzazione completa dellalbero portale di destra in 24 pazienti . 
in 2 pazienti si ottenuta lembolizzazione del ramo portale segmentario del iv segmento da resecare nel programma chirurgico , in uno dei quali la successiva embolizzazione a destra non stata completa ed ha interessato solo il settore anteromediale . 
un paziente stato sottoposto ad una seconda seduta di embolizzazione che ha seguito di 22 giorni la precedente con la quale non si era ottenuta lembolizzazione completa dellalbero portale di destra . 
 la variazione volumetrica dopo rpve del frl stata significativa nei pazienti con metastasi epatiche ( p < 0 , 001 ) e nei pazienti con neoplasie delle vie biliari ( p < 0 , 001 )  . 
in 9 pazienti portatori di metastasi da colon - retto lincremento volumetrico del frl ( 18571 , 16 cm3 ) dopo un periodo compreso tra i 25 ed i 48 giorni ( in media 33 , 8 giorni ) associato allatrofia del parenchima epatico funzionante da resecare ( 186 , 196 , 62 cm3 ) ha modificato il rapporto frl / volume epatico totale funzionante dal 18%29% ( in media 25% ) prima della rpve al 30%51% ( in media 39% )  . 
dopo rpve si riscontrato un incremento volumetrico delle metastasi da colon - retto nel fegato embolizzato compreso tra il 6% e il 155 , 5% , mentre nella paziente che ha atteso 60 giorni lincremento del volume tumore stato del 562 , 7% ( tabella 1 )  . 
nei pazienti portatori di metastasi da carcinoide dopo rpve non si verificato incremento volumetrico delle metastasi sia nel fegato embolizzato che nel fegato non embolizzato , mentre lipertrofia del frl ( 283 , 7570 , 1 cm3 ) ha significativamente cambiato il rapporto frl / parenchima epatico funzionante dal 20%27% al 42%52% ( tabella 1 ) dopo un periodo compreso tra i 30 ed i 34 giorni ( in media 31 giorni )  . 
nei pazienti portatori di neoplasie delle vie biliari lfrl costituiva il 18%28 , 6% del parenchima epatico funzionante , dopo un periodo compreso tra i 31 e gli 80 giorni ( in media 45 , 9 giorni ) dopo rpve lipertrofia del frl ( 187 , 1671 , 5 cm3 ) e latrofia del parenchima da resecare ( 305 , 7182 , 5 cm3 ) ha modificato questo rapporto compreso 30%45% ( tabella 2 )  . 
non progressione di malattia rispetto allesame pre - rpve stata documentata dalla tc nelle neoplasie di klatskin , nella neoplasia della colecisti e 558 radiol med ( 2009 ) 114 : 553570 radiol med ( 2009 ) 114 : 553570 560 radiol med ( 2009 ) 114 : 553570 radiol med ( 2009 ) 114 : 553570 562 radiol med ( 2009 ) 114 : 553570 patient who had undergone metastasectomy during previous surgery . 
eight patients with biliary cancers underwent right hepatectomy extended to segment i ( n = 3 ) and to segments i and iv ( n = 5 )  . preoperative imaging understaged four patients , and radical surgery could not be performed owing to the finding , on exploratory laparotomy , of peritoneal carcinosis ( one patient with metastasis from colon cancer ) , positive lymph nodes at the hepatic hilum ( one patient with type ii klatskin tumour ) , neoplastic lymphangitis along the hepatic pedicle ( one patient with type ii klatskin tumour ) and hepatic artery invasion ( one patient with type iv klatskin tumour )  . 
two patients did not undergo surgical exploration : one with a klatskin tumour because of the onset of ascites after the second embolisation session , and the other with colorectal cancer because of the onset of lung metastases . 
 discussion surgery of biliary cancers is a difficult procedure requiring hepatectomy extended to the caudate lobe , a site of possible recurrence ; resection of the main bile duct with creation of biliodigestive anastomoses ; and possible vascular reconstructions in patients with obstructive jaundice . 
five - year survival in patients with klatskin tumours treated with surgical resection with disease - free margins is between 43% and 46% , but it involves ablation of up to 80% of the liver parenchyma [ 13 ]  . 
in our experience , five patients with biliary cancers who underwent surgical resection after right pve required a right hepatectomy extended to segment iv associated with caudectomy ( necessary for all patients with biliary cancer )  . 
reported that in 132 patients with cholangiocarcinoma who underwent surgical resection after right pve due to insufficient frl volume , the 5 - year survival rate was comparable to that of a control group who underwent surgery without preoperative right pve owing to adequate frl [ 12 ]  . patients with unresected liver metastases from colorectal cancer had a mean survival of 421 months , with a 3 - year survival rate less than 3% . systemic chemotherapy improves quality of life but has limited impact on survival . 
dodici pazienti portatori di metastasi epatiche sono stati sottoposti ad epatectomia destra ( 4 pazienti ) , epatectomia destra allargata a i e iv segmento ( 2 pazienti ) , epatectomia destra allargata al iv ( 6 pazienti ) , uno dei quali con metastesectomia in un precedente tempo chirurgico . 
in tutti i pazienti stata eseguita lecografia intraoperatoria che ha confermato il numero e la sede delle lesioni individuate allesame tc . otto pazienti portatori di neoplasie biliari sono stati sottoposti ad epatectomia destra allargata al i segmento ( 3 pazienti ) e ad epatectomia destra allargata a i e iv segmento ( 5 pazienti )  . quattro pazienti sono stati sottostadiati allimaging preoperatorio e non stato possibile effettuare una chirurgia oncologicamente radicale per la presenza alla laparotomia esplorativa di carcinosi peritoneale ( 1 pazienti portatore di metastasi da neoplasia del colon ) , di linfonodi positivi allilo epatico ( 1 pazienti con tumore di klatskin tipo ii ) , per linfangite neoplastica lungo il peduncolo epatico ( 1 pazienti con tumore di klatskin tipo ii ) , per infiltrazione dellarteria epatica ( 1 pazienti con tumore di klatskin tipo iv )  . 
2 pazienti non sono stati esplorati chirurgicamente , un pazienti portatore di neoplasia di klatskin per la comparsa di ascite dopo la seconda seduta di embolizzazione e laltro pazienti con neoplasia colon - rettale per la comparsa di metastasi polmonari . 
nellimmediato postoperatorio , nella nostra casistica , nessun paziente deceduto per insufficienza epatica grave post - chirurgica ; solo in quattro pazienti si avuta una transitoria lieve insufficienza epatica ( bilirubina > 2 , 9 mg / dl e riduzione del tempo di protrombina < 50% [ 11 ] )  . 
 discussione la chirurgia delle neoplasie delle vie biliari una procedura difficile che richiede estese epatectomie che comprendono sempre il lobo caudato , sede di possibile recidiva , la resezione della via biliare con la ricostruzione di anastomosi biliodigestive , possibili ricostruzioni vascolari , in pazienti con ittero ostruttivo e , quindi , la riduzione dei rischi chirurgici e postchirurgici un sfida per il chirurgo epatobiliare [ 12 ]  . 
la sopravvivenza a 5 anni nei pazienti portatori di neoplasie di klatskin sottoposti ad exeresi chirurgica con margini di resezione libera da malattia compresa tra 43%46% ma prevede lasportazione fino all80% del parenchima epatico [ 13 ]  . 
 [ 12 ] hanno verificato in 132 pazienti con colangiocarcinoma , sottoposti ad exeresi chirurgica dopo rpve per insufficiente frl , che la sopravvivenza a 5 anni sovrapponibile ad un gruppo di controllo sottoposto a chirurgia senza rpve per adeguato frl [ 12 ]  . 
nei pazienti con metastasi epatiche da neoplasie del colon - retto non trattate chirurgicamente , la sopravvivenza media varia dai 4 ai 21 mesi con una sopravvivenza a 3 anni inferiore al 3% . radiol med ( 2009 ) 114 : 553570 fig . 
1a - h computed tomography ( ct ) images obtained before and after right portal vein embolisation ( rpve ) in a 71 - year - old man with gallbladder cancer . 
a - d axial and oblique reformatted ct images obtained before ( a , b ) and after ( c , d ) rpve show the gallbladder cancer invading liver segments iv ( arrows in a and c ) and v ( arrows in b and d ) without hilar invasion . 
e - h twoand three - dimensional maximum intensity projection ( mip ) reformations obtained before ( e , f ) and after rpve ( g , h ) clearly show a proportional twofold atrophy - hypertrophy effect ( decrease in volume of the right liver and increase in volume of the left liver )  . 
a - d le immagini tc assiali e le ricostruzioni oblique ottenute prima ( a , b ) e dopo ( c , d ) rpve documentano la neoplasia delle colecisti che invade iv ( frecce in a e c ) e v segmento epatico ( frecce in b e d ) , senza infiltrazione dellilo . 
e - h le ricostruzioni 2d e 3d mip ottenute prima ( e , f ) e dopo rpve ( g , h ) dimostrano chiaramente un proporzionale duplice effetto atrofia - ipertrofia ( riduzione di volume del fegato destro ed incremento volumetrico del fegato sinistro )  . 
a , b maximum intensity projection ( mip ) reformation in the portal phase ( a ) and axial computed tomography ( ct ) in the delayed phase ( b ) demonstrate an enhancing irregular nodular mass ( arrows in a and b ) adjacent to the right portal vein and invading segment iv with involvement of the right secondary biliary confluence and dilatation of the right intrahepatic bile duct . 
after rpve , left hepatic hypertrophy is evident on 3d mip reconstructions , on anterior view ( c ) and at surgery ( d ) , with evident delimitation caused by the different perfusion of the two hemilivers . 
a , b la ricostruzione mip 2d in fase portale ( a ) e limmagine assiale in fase tardiva ( b ) documentano una formazione nodulare , irregolare e con enhancement ( frecce in a e b ) adiacente al ramo portale di destra che invade il iv segmento con interruzione della convergenza biliare secondaria di destra e dilatazione a monte delle vie biliari intraepatiche dellemisistema di destra . 
lipertrofia del fegato sinistro dopo rpve evidente nelle ricostruzioni mip 3d , visione anteriore ( c ) e allintervento chirurgico ( d ) con evidente demarcazione per la diversa perfusione dei due emifegati . 
the nonresectability of potential candidates for resection may be related to an insufficient frl ( 8% in 746 hepatectomies in elias et al.s experience ) [ 16 ]  . the liver has the ability to regenerate rapidly , a property that provides the rationale for new and innovative surgical techniques for liver resection and organ transplantation . 
one strategy employed by many hepatobiliary surgeons to reduce the risk of complications after extended hepatectomy is pve . occlusion of a portal branch causes the redistribution of the portal flow with a double effect : atrophy of the embolised parenchyma and hypertrophy of the unembolised parenchyma . 
lunico trattamento che migliora la sopravvivenza quello chirurgico : dopo la resezione a 5 anni stimata essere tra il 25% ed il 40% , a 10 anni tra il 22% e il 26% [ 14 , 15 ]  . 
tuttavia lintervento chirurgico possibile solo nel 15%25% dei pazienti con metastasi da colon - retto in relazione allo stadio della malattia , alla localizzazione delle lesioni ripetitive epatiche ed a problemi tecnici ma in pazienti potenzialmente resecabili la non resecabilit pu essere legata ad un insufficiente frl ( 8% in 746 epatectomie nellesperienza di elias ) [ 16 ]  . il fegato possiede la capacit di rigenerare velocemente e su questo principio si basano le pi moderne ed innovative tecniche chirurgiche di resezioni epatiche e di trapianto dorgano . 
locclusione di un ramo portale determina la ridistribuzione del radiol med ( 2009 ) 114 : 553570 to be resected and hypertrophy of the frl is to the advantage of the potential postoperative hepatic functional reserve . immediately after embolisation , the portal flow increases in the unembolised portal territory , as demonstrated by doppler ultrasonography [ 17 ] , leading to parenchymal hypertrophy that correlates with the magnitude of the increase in portal flow [ 8 , 18 , 19 ]  . 
 [ 21 ] , however , showed that not only the amount but also the quality of portal blood affects liver regeneration , and it is indeed the blood flowing back from the pancreatic bed that contains hepatotrophic factors . 
 [ 22 ] reported that the regeneration process of a normal liver after resections occurs in three phases : rapid increase during the first month , decrease during the second month and , finally , extremely slow increase . 
 [ 23 ] recently demonstrated that noncirrhotic livers require a minimum of 3 weeks after right pve owing to hypertrophy of the frl , followed by a plateau lasting between 22 and 56 days . 
noncirrhotic livers have the greatest regenerative capacity ( approximately 1221 cm3 / day 2 weeks after pve , approximately 11 cm3 / day at 4 weeks and 6 cm3 / day at 32 weeks ) [ 2 , 24 , 25 ]  . 
in noncirrhotic patients , a period of 34 weeks is required to assess the efficacy of pve in increasing frl volume . longer waiting periods , related to inflammatory biliary complications in patients with biliary cancers or to the patients refusal , showed that the atrophy of the embolised parenchyma progresses over time , whereas the hypertrophy of the frl is not significantly different . 
 at the beginning of our experience , when surgical planning envisaged a right hepatectomy extended to segment iv , we combined embolisation of the portal branch of segment iv with subsequent right pve . 
 [ 26 ] , we no longer believe this approach to be necessary , in part in consideration of the increased risk of accidental reflux of embolising material into the left portal branch . 
the potential hepatic functional reserve is calculated by using ct determinations of frl volume and total volume of functional liver parenchyma , obtained by subtracting tumour volume from total liver volume , and thus by the frl / total functional liver - volume ratio . 
the method allows for separate determinations of tumour volume and healthy parenchyma , thereby providing an flusso portale con un duplice effetto : latrofia del parenchima epatico embolizzato e lipertrofia del parenchima epatico non embolizzato . 
questo duplice effetto antagonista con atrofia del parenchima epatico da resecare ed ipertrofia del frl a vantaggio della potenziale riserva funzionale epatica post - chirurgica . immediatamente dopo lembolizzazione il flusso portale aumenta , come dimostrato mediante eco - doppler [ 17 ] , nel territorio portale non embolizzato determinando ipertrofia del parenchima epatico che correla con lentit dellincremento del flusso portale [ 8 , 18 , 19 ]  . 
 [ 21 ] hanno dimostrato che non solo la quantit , ma anche la qualit del sangue portale influenza la rigenerazione epatica , infatti il sangue refluo dal letto pancreatico che contiene fattori epatotrofici . 
 [ 22 ] hanno dimostrato che il quadro rigenerativo di un fegato normale dopo resezioni epatiche consiste in tre fasi : un rapido incremento durante il primo mese , un decremento nel secondo e alla fine un lentissimo incremento . 
 [ 23 ] hanno recentemente dimostrato che in fegati non cirrotici un minimo di 3 settimane richiesto dopo rpve per lipertrofia dellfrl seguito da un plateau compreso tra 22 e 56 giorni . 
fegati non cirrotici dimostrano la pi alta capacit rigenerativa ( circa 1221 cm3 / d a 2 settimane dopo lembolizzazione portale , circa 11 cm3 / d a 4 settimane e 6 cm3 / d a 32 settimane ) [ 2 , 24 , 25 ]  . 
fegati cirrotici o pazienti diabetici mostrano il pi basso grado di ricrescita approssimativamente ( 9 cm3 / d a 2 settimane dopo pve ) [ 2 , 25 ]  . 
il periodo di attesa pi lungo , in relazione a complicanze flogistiche biliari nei pazienti portatori di neoplasie delle vie biliari o al rifiuto di una paziente , ha dimostrato che latrofia del parenchima epatico embolizzato progressiva nel tempo mentre non significativamente diversa lipertrofia del frl . 
 allinizio della nostra esperienza , quando il programma chirurgico prevedeva lepatectomia destra allargata al quarto segmento , abbiamo associato lembolizzazione del ramo portale segmentario del iv che precedeva lembolizzazione del ramo portale di destra , ma in accordo con capussotti et al . 
la potenziale riserva funzionale epatica calcolata mediante la volumetria tc del frl e del volume totale del parenchima epatico funzionante , ottenuto sottraendo al volume epatico totale il volume tumore e quindi dal loro rapporto ( frl / volume totale epatico funzionante )  . 
la metodologia da noi usata permette di ottenere la volumetria separata del volume 566 radiol med ( 2009 ) 114 : 553570 accurate estimation of functional parenchyma , particularly in those cases where the liver parenchyma to be resected is extensively involved . 
 [ 27 ] demonstrated that the evaluation of tumour volume in patients with liver metastases significantly affects the evaluation of the hepatic functional reserve . the evaluation of tumour volume before and after right pve also provided us with information on the oncogenic effect of right pve on liver disease . 
in biliary cancers , no local disease progression was detected . our results coincide with previous experiences [ 8 , 28 ] that reported an increase in volume of hypovascular metastases from colorectal cancers after right pve in embolised and unembolised livers and no change in the volume of hypervascular metastases from carcinoid tumours in either tumore e del parenchima sano e quindi fornisce la valutazione reale del parenchima funzionante , in particolare nei casi in cui il parenchima epatico da resecare in gran parte sostituito . 
 [ 27 ] hanno infatti dimostrato che nei pazienti portatori di metastasi epatiche la valutazione del volume tumore incide in maniera significativa nella valutazione della riserva funzionale epatica . la valutazione del volume tumore prima e dopo rpve ci ha inoltre fornito dati sulleffetto oncogenetico della metodica sulla patologia epatica . 
dopo rpve nella patologia secondaria epatica aumentato il volume delle metastasi da colon - retto mentre rimasto immodificato il volume tumore nelle metastasi da carcinoide ; nelle neoplasie delle vie biliari non abbiamo riscontrato progressione locale di malattia . 
i nostri risultati concordano con esperienze precedenti [ 8 , 28 ] che avevano documentato laumento volumetrico delle metastasi , ipovascolari , da colon - retto dopo rpve nel fegato embolizzato e non embolizzato , mentre il volume delle metastasi ipervascolarizzate da carcinoide rimaneva invariato sia nel radiol med ( 2009 ) 114 : 553570 fig . 
a - f axial computed tomography ( ct ) scans obtained in a 54 - year - old man show multiple synchronous liver metastases from colon cancer in the left ( 1 , 2 , 5 ) and right ( 3 , 4 , 6 ) liver , with partial response after six cycles of chemotherapy . 
surgical plan : ablation with free resection margins of the liver lesion located in segment viii ( lesion 3 ) requires right hepatectomy combined with resection of the middle supra hepatic vethe potential frl consists of segments i , ii and iii . 
i - p axial ct scans obtained 29 days after rpve document left hepatic hypertrophy , especially of the caudate lobe , the outcome of previous left metastasectomy ( 1 , 2 , 5 ) and enlarged liver metastases in the right liver lobe ( tumour volume increased from 45 to 115 cm3 ) ( 3 , 4 , 6 )  . 
a - f in un paziente di 54 anni , le immagini assiali dellesame tc documentano multiple metastasi epatiche sincrone da cancro del colon localizzate nel fegato sinistro ( 1 , 2 , 5 ) e nel fegato destro ( 3 , 4 , 6 ) , con risposta parziale dopo 6 cicli di chemioterapia . 
programma chirurgico : lasportazione con margini di resezione liberi della lesione epatica dellviii segmento ( lesione 3 ) necessita di epatectomia destra , associata a resezione della vena sovraepatica media . 
i - p le immagini assiali della tc eseguita 29 giorni dopo lembolizzazione documentano lipertrofia del fegato sinistro , in particolare del lobo caudato , gli esiti della pregressa metastasectomia a sinistra ( 1 , 2 , 5 ) e le metastasi epatiche del fegato destro ( 3 , 4 , 6 ) aumentate di dimensioni ( volume tumore 115 vs 45 cm3 )  . 
 [ 29 ] hypothesised that a cytokine regulating the hepatocyte growth factor ( hgf ) which is altered in patients with colorectal cancer and distant metastases is responsible for the growth of liver metastases in these patients . 
in contrast , preoperative right pve does not affect 5 - year survival rates compared with control groups undergoing resection of liver metastases from colon cancer without right pve [ 16 ]  . new strategies are being proposed for patients with multiple liver metastases from colorectal cancer , which combine the intra - arterial [ 30 , 31 ] or systemic [ 3235 ] infusion of chemotherapeutic agents with selective pve , with the aim of simultaneously obtaining tumour shrinkage and fegato embolizzato che non embolizzato . 
 [ 29 ] hanno ipotizzato che una citochina che regola il fattore di crescita degli epatociti ( hgf ) , alterata nei pazienti con neoplasia colon - rettale e metastasi a distanza , sia responsabile della crescita delle metastasi epatiche in questi pazienti . 
lembolizzazione portale prechirurgica non modifica , invece , la sopravvivenza a 5 anni rispetto a gruppi di controllo sottoposti a chirurgia per metastasi epatiche da neoplasia del colon senza rpve [ 16 ]  . attualmente nuove strategie vengono proposte in pazienti portatori di multiple metastasi epatiche da colon - retto che associano alla selettiva embolizzazione portale infusione intraarteriosa [ 30 , 31 ] o sistemica [ 3235 ] di chemoterapici con lo scopo di ottenere contemporaneamente la 568 radiol med ( 2009 ) 114 : 553570 frl hypertrophy . 
 the second factor that affects the indication for right pve in candidates for liver resection is the possible coexistence of chronic liver disease , as this influences the amount of hepatic functional reserve needed to reduce postoperative morbidity and mortality . 
in patients with klatskin tumours , preventive drainage of the potential frl to resolve the cholestasis ( bilirubin < 2.9 mgdl ) is the essential precondition for pve to obtain an adequate regenerative response of the frl . 
 [ 27 ] , depending on the severity of cirrhosis and on residual liver function assessed with the indocyanine test . the presence of systemic disease , such as diabetes , in which the regenerative capacity of the liver is reduced by the hepatotrophic effect of insulin , and the complexity of surgery are , respectively , the third and fourth factors to be considered when selecting candidates for preoperative right pve . 
the use of lipiodol mixed with cyanoacrylate achieved right pve embolisation without complications and without recanalisation , with the added benefit of radiopacity allowing monitoring of the procedure by fluoroscopy [ 41 , 42 ]  . a potential functional reserve of frl < 30% constitutes an indication for right pve in patients previously exposed to chemotherapy or with previous cholestasis . 
 il secondo fattore che regola lindicazione alla rpve nei candidati a resezione epatiche leventuale concomitanza di epatopatia perch su questo si basa lentit della riserva funzionale epatica necessaria per ridurre la morbilit e mortalit post - chirurgica . 
lasportazione di pi del 75% del parenchima epatico ben sopportata nel paziente giovane ( 40 anni ) , ma la chirurgia resettiva epatica deve essere pi conservativa in relazione allet , alla patologia epatica e sistemica [ 36 ]  . 
 il minimo volume residuo del frl consigliato in pazienti con normale funzionalit epatica tra il 25%30% della massa epatica totale funzionante [ 9 , 19 , 35 , 36 ] anche se sono state effettuate resezioni epatiche con un volume di frl non inferiore al 20% senza complicanze post - chirurgiche [ 22 ]  . 
nei pazienti con neoplasie di klatskin , il preventivo drenaggio del potenziale frl che risolva la colestasi ( livello di bilirubina inferiore a 2 , 9 mgdecilitro ) il presupposto indispensabile allembolizzazione portale perch si ottenga unadeguata risposta rigenerativa del frl . 
la capacit rigenerativa del fegato cirrotico ridotta sia in relazione alla riduzione del flusso portale che alla fibrosi e quindi in questi pazienti il volume minimo del frl necessario pu raggiungere il 50% come dimostrato da kubota ed al . 
 [ 27 ] in relazione alla gravit della cirrosi e quindi alla funzionalit epatica residua valutata mediante il test dellindocianina . la presenza di una malattia sistemica come il diabete che riduce la capacit rigenerativa del fegato in relazione alleffetto epato - trofico dellinsulina e la complessit dellintervento chirurgico sono il terzo ed il quarto fattore da considerare nella selezione dei pazienti da candidare a rpve prechirurgica . 
 in conclusione , il nostro studio retrospettivo ha verificato che lembolizzazione portale pre - chirurgica una procedura sicura ; luso di lipiodol misto a cianoacrilato ha ottenuto lembolizzazione dellalbero portale destro senza complicanze e senza ricanalizzazione con il vantaggio legato alla sua radiopacit di monitorare lembolizzazione mediante fluoroscopia [ 41 , 42 ]  . la potenziale riserva funzionale del frl inferiore al 30% unindicazione alla rpve in pazienti precedentemente sottoposti a terapie chemioterapiche o con precedente colestasi ed allarga le indicazioni alla chirurgia radiol med ( 2009 ) 114 : 553570 extends the indications for liver resection in primary and secondary liver cancers , making radical surgery possible without severe postoperative complications . 
the addition of two - stage hepatectomy appears to be a promising innovation for patients with bilobar liver metastases from colorectal cancer . resettiva epatica in patologie primitive e secondarie epatiche rendendo possibile una chirurgia oncologicamente radicale senza gravi complicanze postchirurgiche . 
sardanelli servizio di radiologia , dipartimento di scienze medico - chirurgiche , universit degli studi di milano , irccs policlinico san donato , via morandi 30 , 20097 san donato milanese , italy a . 
the mr protocol applied at our institution for both diagnosis and follow - up after surgical or endovascular treatment consists of four steps : morphologic study , cine mr study , flow analysis , and mr angiography ( mra )  . the first three sequences are acquired during breath - hold and with electrocardiographic gating . 
cine true - fast imaging with steady - state precession ( true - fisp ) sequences show not only morphologic features but also blood - flow changes inside the aorta . 
gradient - echo sequences for phase - velocity mapping allow flow analysis . application of bernoullis equation here briefly presented and discussed allows for calculation of the pressure gradient caused by the coarctation . 
mra , acquired with a breath - hold three - dimensional t1weighted gradient - echo sequence and intravenous administration of paramagnetic contrast material , allows for optimal depiction of the aortic lumen , with a panoramic view of the whole aorta , its main branches and possible collateral circulation . 
 keywords aorta aortic coarctation bernoullis equation magnetic resonance ( mr ) imaging mr flow analysis ( phase - velocity mapping ) riassunto la coartazione aortica rappresenta il 5%10% di tutte le patologie congenite del cuore e dei grandi vasi e il 7% dei casi di piccoli cardiopatici in condizioni critiche . 
la risonanza magnetica ( rm ) permette lo studio di questa patologia con una serie di vantaggi rispetto a tecniche alternative quali langiografia convenzionale , lecografia transesofagea e la tomografia computerizzata . 
il nostro protocollo rm , utilizzato sia per la diagnosi , sia per il follow - up dopo trattamento chirurgico o endovascolare , consiste di quattro fasi : studio morfologico , cinetico , flussimetria e angio - rm . 
le sequenze a sangue chiaro true - fast imaging with steady - state precession ( true - fisp ) , oltre a dare informazioni di tipo morfologico , mostrano le alterazioni del flusso ematico allinterno del vaso . 
le sequenze gradient - echo con mappaggio fase - velocit consentono la quantificazione del flusso ; lapplicazione dellequazione di bernoulli ( qui brevemente presentata e discussa ) , consente infatti il calcolo del gradiente pressorio determinato dalla coartazione . 
lo studio angiorm , ottenuto in apnea mediante sequenze gradient - echo tridimensionali t1 - pesate con somministrazione endovenosa di mezzo di contrasto paramagnetico , mostra una visione volumetrica panoramica del lume dellaorta , delle sue principali ramificazioni e , quando presenti , dei circoli collaterali . 
 parole chiave aorta coartazione aortica equazione di bernoulli flussimetria rm risonanza magnetica ( rm ) radiol med ( 2009 ) 114 : 524537 introduction introduzione over recent years , several magnetic resonance ( mr ) techniques have been successfully applied for evaluating congenital heart diseases . 
we summarize here the currently available knowledge about coa , including epidemiology , aetiopathogenesis , topographic classification , and the different mr imaging techniques . negli ultimi anni numerose tecniche di risonanza magnetica ( rm ) sono state applicate con successo alla valutazione delle cardiopatie congenite . 
la coartazione aortica ( coa ) rappresenta un reperto non infrequente nella pratica clinica , pari a circa il 5%10% di tutte le malformazioni congenite del cuore e dei grandi vasi [ 1 ]  . 
sono qui rivisitate le attuali conoscenze sulla malattia relativamente a epidemiologia , eziopatogenesi , classificazione topografica e studio con differenti tecniche rm . definition coarctation is a term derived from the latin coarctatio , meaning narrowing or stricture . 
similar congenital malformations are aortic atresia and the true aortic interruption , mostly located at the arch ( interrupted aortic arch )  . coa , also known as congenital aortic stenosis , was originally noted during autopsy by j.f. 
he collected 200 previously documented cases , but coa was not regularly diagnosed until after 1933 [ 6 ]  . epidemiology and aetiology coa accounts for 5%10% of all congenital heart diseases and represents 7% of critically ill infants with heart disease . it is seven times more common in caucasian than in asian population . 
in atlanta ( usa ) from 1970 to 1983 , the prevalence per 1 , 000 live births was as follows : interruption of the aortic arch , 0.05 ; coarctation , 0.36 ; hypoplasia of the aorta , 0.06 [ 7 ] , giving a total prevalence of 0.47 per 1 , 000 live births . 
in bohemia in 1980 , a prevalence of 6.67 congenital heart malformations per 1 , 000 live births was reported , and 5.77% of these malformations consisted of coa cases [ 9 ] , giving a coa prevalence of 3.84 per 1 , 000 live births . the aetiology of coa is still unclear . 
up to 60% [ 10 ] or 85% [ 1 ] of coa cases are associated with bicuspid aortic valve , supporting the hypothesis of a common cause for the two congenital malformations [ 11 ] or an influence of the bicuspid aortic valve on the development of coa [ 1 ]  . 
pathologic examination of the ascending aorta of patients with definizione il termine coartazione deriva dal latino coarctatio , letteralmente restringimento ovvero , nel caso di una struttura vascolare , riduzione di calibro cui consegue ostruzione al flusso ematico . 
paris [ 4 ] ne forn la prima descrizione accurata nel 1791 mentre j . abbott pubblic una serie autoptica retrospettiva di 200 casi nel 1928 [ 5 ] , ma la malattia non stata diagnosticata con regolarit fino a dopo il 1933 [ 6 ]  . epidemiologia ed eziologia la coa rappresenta il 5%10% di tutte le patologie congenite del cuore e dei grandi vasi e il 7% dei casi di piccoli cardiopatici in condizioni critiche . 
 si osserva una prevalenza maschile con rapporto maschi / femmine tra 1 , 3 e 2 , 1 nella maggior parte delle serie [ 1 ]  . nellarea metropolitana di atlanta ( usa ) stata osservata tra il 1970 e il 1983 una prevalenza su 1000 nati vivi pari a 0 , 05 per linterruzione dellarco , 0 , 36 per la coartazione e 0 , 06 per lipoplasia [ 7 ] , con una prevalenza totale pari al 0 , 47 per 1000 nati vivi . 
una prevalenza pari a 0 , 32 per 1000 nati vivi stata riportata per lislanda dal 1980 al 1994 [ 8 ]  . in boemia nel 1980 stata riportata una prevalenza di 6 , 67 malformazioni congenite cardiache per 1000 nati vivi ; il 5 , 77% di queste era costituito da casi di coa [ 9 ] , per una prevalenza di coa pari a 3 , 84 per 1000 nati vivi . leziologia della coa non ancora stabilita con certezza . 
si associa a bicuspidia valvolare aortica fino al 526 radiol med ( 2009 ) 114 : 524537 bicuspid aortic valve frequently shows loss of smoothmuscle cells and severe degeneration of the medial elastic fibers ( so - called cystic medial necrosis ) [ 11 ]  . 
associated cardiac defects are observed in approximately 50% of patients with coa , mostly being left - sided hypoplastic or obstructive defects and ventricular septal defects [ 1 ]  . 
moreover , the higher coa prevalence in males and a relatively high prevalence in patients with turners syndrome suggest a link between x - chromosome defects and anomalous development of the aorta and valve [ 11 ]  . 
however , this classification is now considered too simplistic because many patients lack symptoms , and coa diagnosis is delayed until adulthood [ 14 ]  . only malformations determining a total obstruction or a severe degree of stenosis ( severe tubular hypoplasia , severe coarctation , vessel atresia or interruption ) or associated with cardiac defects are diagnosed during childhood [ 13 ]  . 
thus , the prevalence in adulthood , including the nonsevere form of coa , should be higher than the incidence in live births . a commonly accepted classification is based on stenosis location : preisthmic , isthmic and postisthmic . 
 a physiopathologic approach is given by the subdivision 60% [ 10 ] o all85% dei casi [ 1 ] , supportando lipotesi di una causa comune alle due malformazioni [ 11 ] o di uninfluenza della bicuspidia valvolare aortica sullo sviluppo della coa [ 1 ]  . 
indagini istologiche dellaorta ascendente di soggetti con bicuspidia valvolare hanno mostrato un ridotto numero di cellule muscolari lisce e severa degenerazione delle fibre elastiche della tonaca media ( cosiddetta necrosi medio - cistica ) [ 11 ]  . 
malformazioni cardiache congenite si associano a coa in circa il 50% dei casi , per lo pi rappresentate da sindromi ipoplasiche o ostruttive delle cavit sinistre o da difetti del setto interventricolare [ 1 ]  . 
dal 3%5% [ 1 ] al 10% [ 12 ] dei pazienti con coa presentano altres aneurismi intracranici , in accordo con lipotesi che la coa sia parte di una patologia arteriosa diffusa , secondaria ad anomalie dello sviluppo della cresta neurale [ 12 ]  . 
inoltre , la maggiore prevalenza di coa nei maschi e nei pazienti con sindrome di turner induce a ipotizzare un legame tra difetti del cromosoma x ed alterazioni dello sviluppo dellaorta e della valvola aortica [ 11 ]  . 
solo le malformazioni che comportano stenosi di grado elevato o ostruzione totale del flusso ematico ( ipoplasia tubulare serrata , coartazione serrata , atresia o interruzione del vaso ) o che si associano a malformazioni cardiache sono diagnosticate in et infantile [ 13 ]  . ne deriva che la prevalenza in et adulta , includendo le forme non severe di coa , dovrebbe essere sensibilmente pi elevata di quella calcolata in base alla diagnosi sui nati vivi . radiol med ( 2009 ) 114 : 524537 fig . 
1a - c angio - rm ( ricostruzioni volumetriche ) di casi di : ipoplasia tubulare dellarco aortico ( freccia in a ) , coartazione istmica ( freccia in b ) e interruzione dellaorta discendente ( freccia in c )  . into preductal , ductal and postductal coa , referring to the location of the botallo ductus arteriosus . 
this kind of coa , observed in approximately 5% of infants with turner syndrome , typically results from a cardiac anomaly during fetal life decreasing blood flow through the left ventricle , leading to hypoplastic development of the aorta . 
in postductal coa , the narrowing is distal to the insertion of the ductus arteriosus . as a consequence , blood flow to the lower body is impaired . it is thought to be the consequence of muscular cells extending from ductus arteriosus into the aorta during fetal life [ 15 ]  . clinical features and treatment the age of clinical presentation is mainly related to the degree of stenosis and to the presence of associated abnormalities . 
nella forma preduttale la coa prossimale allinserzione del dotto ; se severa , il flusso a valle dipende dalla perviet del dotto la cui chiusura , quindi , pu risultare fatale . 
questo tipo di coa , osservato in circa il 5% dei nati affetti da sindrome di turner , tipicamente il risultato di anomalie cardiache fetali con ridotto efflusso dal ventricolo sinistro , cui consegue unipoplasia dellaorta . 
nella forma post - duttale la coa a valle dellinserzione del dotto e ne risulta un ridotto flusso alla porzione inferiore del corpo ; ritenuta essere la conseguenza della migrazione di miocellule dal dotto arterioso allaorta durante la fase fetale [ 15 ]  . 
si dovrebbe sempre considerare lipotesi di coa in soggetti adolescenti o giovani di sesso maschile con 528 radiol med ( 2009 ) 114 : 524537 coa becomes clinically relevant , it can lead to systemic hypertension and secondary left ventricular hypertrophy with heart failure . 
if it is not treated , the patients mean age of death is about 34 years [ 16 ]  . invasive treatment should always be considered in patients with pressure gradients > 30 mmhg on cardiac catheterization [ 17 ]  . 
successful surgical correction of coa by resection of the stenotic tract with end - to - end anastomosis was first described by crafoord and nylin in 1945 [ 18 ]  . 
 perioperative mortality rates are determined largely by age and concomitant congenital heart disease rather than by the choice of operative technique for correcting coa [ 23 ] and are less than 3% for older children and adults [ 24 ]  . several postsurgical complications such as cerebrovascular , cardiac and aortic events may occur . 
the most common complications are cerebrovascular accidents , cerebral haemorrhage , recurrent hypertension , heart failure , endocarditis , endarteritis , coronary artery disease , recoarctation , poststenotic aneurysm , and aortic rupture [ 10 ]  . 
due to successful surgical or endovascular treatments , follow - up of treated adult patients is often required . imaging of coa a posteroanterior chest x - ray examination can show a dilated ascending aorta , low prominence of the first left arch , a notch sign corresponding with the location of coa and small notches on the inferior posterior margin of ribs , mainly from fourth to eighth , due to the osteolytic effect of the collateral hypertrophic intercostal arteries . 
 similarly to aortic dissection [ 26 ] , coa can be diagnosed using transesophageal echocardiography ( tee ) , digital subtraction angiography ( dsa ) , computed tomography ( ct ) , and mr imaging . 
due to the use of ionising radiation and iodinated contrast agents , ct and dsa are not regarded as first - line techniques for diagnosing coa , particularly in children . 
 over recent years , mr imaging has become a well - established diagnostic tool for studying congenital heart diseases and coa [ 27 , 28 ] , offering many advantages over other ipertensione agli arti superiori e ipotensione e polsi deboli agli arti inferiori . 
se non trattata , porta al decesso mediamente a 34 anni di et [ 16 ]  . il trattamento invasivo dovrebbe essere sempre considerato nei pazienti che presentano un gradiente pressorio maggiore di 30 mmhg al cateterismo cardiaco [ 17 ]  . crafoord e nylin [ 16 ] descrissero per primi , nel 1945 , lintervento correttivo che prevede la resezione del tratto stenotico con successiva anastomosi termino - terminale . successivi miglioramenti delle tecniche chirurgiche [ 18 , 20 ] , tra i quali lintroduzione dellaortoplastica con flap dellarteria succlavia , hanno permesso la correzione in caso di varianti anatomiche complesse . 
 i tassi di mortalit peri - operatoria , determinati soprattutto dallet del paziente e da eventuali anomalie associate piuttosto che dalla tecnica utilizzata per la correzione della coa [ 23 ] , sono inferiori al 3% sia nei bambini che negli adulti [ 24 ]  . 
sono riportate complicanze post - chirurgiche quali lesioni cerebrovascolari , emorragie cerebrali , ipertensione recidivante , scompenso cardiaco , endocardite , endoarterite , patologie coronariche , ricoartazione , aneurismi post - stenotici e rottura dellaorta [ 10 ]  . 
il successo del trattamento chirurgico o endovascolare della coa pone oggi lesigenza del follow - up in et adulta dei pazienti trattati . imaging della coa il radiogramma toracico postero - anteriore pu mostrare ectasia dellaorta ascendente , scarsa prominenza del primo arco di sinistra , incisura in corrispondenza della sede di coartazione e piccole incisure sul margine inferiore dellarco posteriore delle coste , per lo pi dalla quarta allottava , dovute alleffetto osteolitico delle arterie intercostali collaterali ipertrofiche . 
 come per la dissezione aortica [ 26 ] , la diagnosi di coa pu essere posta mediante ecocardiografia transesofagea ( ete ) , angiografia digitale con sottrazione dimmagine ( ads ) , tomografia computerizzata ( tc ) e rm . 
the mr examination takes about 30 min ; the postprocessing requires about 30 min . setting up the patient a good electrocardiographic ( ecg ) line resulting from correct placement of four leads over the anterior or posterior left side of the chest is crucial to obtain a good cardiac synchronization ( ecg gating ) [ 35 ]  . 
la tc e lads non sono considerate tecniche di prima scelta per la diagnosi di coa , soprattutto in et pediatrica , a causa dellutilizzo di radiazioni ionizzanti e mezzi di contrasto ( mdc ) iodati . 
essa offre molteplici vantaggi rispetto alle altre tecniche di imaging cardiovascolare tra i quali la possibilit di ottenere immagini native multiplanari senza luso di radiazioni ionizzanti , lelevata risoluzione temporale ( fino allimaging in tempo reale ) e la possibilit di studio flussimetrico [ 2931 ]  . 
 nello studio dei grandi vasi , la rm vede il suo esordio oltre ventanni or sono con semplici sequenze spin - echo ( se ) e gradient - echo ( ge ) con rifocalizzazione degli spin in flusso laminare . 
successivamente sono state introdotte le sequenze turbo - se ( tse ) , ge cine - rm , ge segmentate , half - fourier acquisition single shot turbo spin - echo ( haste ) e true - fast with steady - state precession ( truefisp )  . 
sequenze ge con mappaggio fase - velocit permettono , inoltre , di ottenere dati flussimetrici [ 33 ] mentre sequenze ge tridimensionali con somministrazione endovenosa di mdc paramagnetico permettono di ottenere immagini simil - angiografiche ad ampio campo di vista , sulle quali si possono effettuare misure accurate del lume aortico [ 34 ]  . protocollo rm faremo qui riferimento alla nostra esperienza ( 20032007 ) con apparecchiatura operante a 1 , 5 t ( magnetom sonata maestro class , siemens , erlangen , germania ) presso lirccs policlinico san donato ( san donato milanese , milano , italia ) su pazienti con coa prima del trattamento e nel loro follow - up a breve e lungo termine . 
thus , we prefer the use of breath - hold ecg - gating : dark - blood t2 - weighted haste [ 37 ] , with high il corretto posizionamento di quattro elettrodi sullemilato sinistro del torace , anteriormente o posteriormente , cruciale per una buona sincronizzazione con lelettrocardiogramma ( ecg - gating ) [ 35 ]  . 
the acquisition of an image passing through the ascending and descending aorta ( three parallel oblique lines ) is planned on a scout axial true fast imaging with steady - state precession ( true fisp ) image ( a )  . 
2a , b definizione del piano obliquo anteriore sinistro ( oas ) per lo studio dellaorta toracica . sullimmagine assiale true - fast imaging with steady - state precession ( true - fisp ) di centratura ( a ) rappresentata la pianificazione di una scansione oas passante per laorta ascendente e discendente ( tre linee oblique parallele )  . 
3a , b bright - blood image ( true - fast imaging with steady - state precession ) ( a ) and dark - blood image ( half - fourier acquisition single - shot turbo spin - echo ) ( b ) , along the same left anterior oblique plane passing through an isthmic coarctation ( arrow )  . 
3a , b immagini a sangue chiaro ( true - fast imaging with steady - state precession ) ( a ) e a sangue scuro ( half - fourier acquisition single - shot turbo spin - echo ) ( b ) lungo il piano obliquo anteriore sinistro passante per una coartazione istmica dellaorta ( freccia )  . 
breath - hold , ecg - gated cine true - fisp sequences ( bright blood , hybrid t2 / t1 - weighted ) are acquired for multiple frames along the cardiac cycle . 
la nostra preferenza va a sequenze in apnea e con sincronizzazione ecg : haste a sangue scuro , pesate in t2 [ 37 ] , con elevato radiol med ( 2009 ) 114 : 524537 fig . 
4 immagine cine true - fast imaging with steady - state precession lungo il piano obliquo anteriore sinistro : coartazione istmica dellaorta ( freccia nera ) ; marcato jet anterogrado ( frecce bianche ) da accelerazione di flusso post coartazione . flow study this part of the mr protocol involves the use of ge phasevelocity mapping sequences on planes orthogonal to the longitudinal axis of the vessel ( through - the - plane acquisition )  . 
phase - velocity sequences provide two different set of images : ( 1 ) magnitude images that give anatomical information , and ( 2 ) phase images that give data about flow direction and velocity . 
si utilizzano sequenze true - fisp ( a sangue chiaro , pesatura ibrida t2 / t1 , con sincronizzazione ecg ) acquisite in apnea per molteplici frame lungo le fasi del ciclo cardiaco . 
per studiare il flusso aortico post - coartazione necessario impostare unelevata codifica di velocit ( velocity encoding , venc ) , generalmente tra 350 e 500 ms , onde evitare artefatti ( aliasing ) nel lume aortico . 
lacquisizione fornisce due serie di immagini : una serie con significato anatomico ( immagini di magnitudo o modulo ) e una serie con significato funzionale ( immagini di fase ) , contenente informazioni su direzione e velocit del flusso . 
lacquisizione lungo il piano obliquo anteriore sinistro ( a ) evidenzia minimo restringimento residuo ( freccia ) ; lacquisizione lungo il piano valvolare aortico ( b ) evidenzia la coesistente bicuspidia ( frecce )  . 
since the kinetic energy of the blood is proportional to the square of its velocity , the right side of bernoullis equation represents the difference between the kinetic energy of blood after coa and that before coa . 
siccome lenergia cinetica del sangue proporzionale al quadrato della sua velocit , il membro destro dellequazione di bernoulli rappresenta la differenza tra lenergia cinetica del sangue a valle della coa e quella a monte della coa . 
 al fine di esprimere p in mmhg anzich in pascal ( pa ) , lunit di misura della pressione nel sistema internazionale , occorre introdurre il seguente coefficiente di conversione : 1 pa = 0 , 0075 mmhg infine , ricordando che la densit del sangue d pari a circa 1067 g / l , otteniamo : i.e. 
if v1 and v2 are given in m / s , the coefficient 4 adjusts the measurement units so to allow the pressure gradient p to be expressed as mmhg . 
se le velocit v1 e v2 sono espresse in m / s , il coefradiol med ( 2009 ) 114 : 524537 that the peak velocity before coa ( v1 ) is generally negligible if compared with the peak velocity after coa ( v2 )  . 
first , it works only if the patient is in the supine position , as the nonperfect horizontal position introduces the gravity - force effect ( this limitation is not relevant for mr applications )  . 
in such a context , a p > 20 mmhg is highly suggestive of significant coa [ 41 , 42 ]  . mr angiography ( mra ) contrast - enhanced mra is a reliable technique for evaluating great vessels . 
for a long time , gadolinium chelates have been considered safe contrast agents and have been used in patients allergic to drugs or iodinated contrast agents and in nephropathic or cardiopathic patients [ 43 ]  . 
patients with severe renal failure [ glomerular filtration rate ( gfr ) < 30 ml / min1.73 m2 ] are considered to be at risk [ 44 , 46 ]  . 
in patients with gfr30 ml / min1.73 m2 , a single dose of 0.1 mmol / kg of gadolinium - based contrast agent can be safely administered intravenously [ 46 ]  . 
for diagnosis or follow - up of coa , we used a power injector with an injection rate of 2 ml / s for both the contrast material and the following 20 - ml saline flush . 
we used a three - dimensional breath - hold , not ecg - gated , t1 - weighted ge sequence with a short acquisition time ( nearly 20 s )  . 
in patients with gfr < 30 ml / min1.73 m2 , time - of - flight and phase - contrast sequences can be used , even though image quality is lower and veins are also visualized [ 47 ]  . 
sulla ricostruzione volumetrica posteriore obliqua ( a ) sono riportate le sedi del calcolo dellarea delle sezioni del vaso a monte della coartazione , al livello della coartazione e a valle della coartazione . 
a sinistra sono riportati i valori di tali aree come normal a , minimum e area 01 , rispettivamente ; inoltre riportato come ratio 01 il rapporto percentuale tra larea a monte della coartazione e larea al livello della coartazione ( grado di stenosi )  . 
la linea centrale endoluminale ( frecce in a ) , generata automaticamente , permette la ricostruzione lungo il piano curvo ( b )  . ficiente 4 consente di esprimere il gradiente p in mmhg . unulteriore semplificazione possibile considerando che la velocit di picco a monte della stenosi ( v1 ) in genere trascurabile rispetto alla velocit a valle della stenosi ( v2 ) e , quindi , pu essere ignorata . 
in primo luogo , la formula di bernoulli valida solo se il paziente supino , in quanto la posizione ortostatica introdurrebbe nella formula un termine aggiuntivo che tiene conto della forza di gravit ( tale limitazione non rilevante per usuali applicazioni rm )  . 
i chelati del gadolinio sono stati considerati a lungo mdc privi di effetti collaterali e si riteneva potessero essere impiegati anche in presenza di allergie a farmaci o ai mdc iodati cos come in caso di pazienti nefropatici o cardiopatici [ 43 ]  . 
sono considerati a rischio pazienti con insufficienza renale grave ( gfr , rateo di filtrazione glomerulare < 30 ml / min1 , 73 m2 ) [ 44 , 46 ]  . 
in pazienti con gfr 30 ml / min1 , 73 m2 si pu utilizzare la singola dose endovena ( 0 , 1 mmol / kg ) di un chelato del gadolinio senza rischi per il paziente [ 46 ]  . 
per la diagnosi e il follow - up della coa , noi utilizziamo un flusso di 2 ml / s sia per il mdc , sia per il bolo di 20 ml di soluzione fisiologica , entrambi somministrati con iniettore automatico . 
in caso di gfr < 30 ml / min1 , 73 m2 possibile impiegare sequenze angiografiche senza mdc ( time of flight e phase contrast ) ottenendo per immagini di qualit inferiore comprendenti anche i vasi venosi [ 47 ]  . 
maximum intensity projections allow aortic demonstration in the angiographic - like view . surface shading display and volume - rendering techniques , obtained with standardised reconstruction algorithms , allow reliable measurements . 
in order to correctly measure aorta diameters and assess the degree of stenosis , measurements should be performed both in lao and in planes orthogonal to the longitudinal axis of the vessel . 
the distance of the coa from the left subclavian artery origin is an important variable for surgical or endovascular therapy planning . le rielaborazioni di volume ( volume rendering technique ) e di superficie ( surface shading display ) , con algoritmi di ricostruzione standardizzati , permettono misurazioni accurate . 
la distanza della coa dallorigine dellarteria succlavia sinistra o dai vasi epiaortici un dato importante nel planning della procedura chirurgica o endovascolare . conclusioni conclusions to correctly diagnose coa , establish disease severity and evaluate treatment options , as well as for follow - up during adulthood , a complete mr protocol is required , including morphological , functional , and flow study as well as contrast - enhanced mra and accurate postprocessing . per diagnosticare correttamente i casi di coa , valutare lentit della stenosi e le possibilit terapeutiche , cos come nel follow - up in et adulta , necessario un protocollo rm che comprenda acquisizioni morfologiche , cinetiche , flussimetriche e angiografiche , completato da accurato postprocessing . 
fava1 1istituto di radiologia universit di torino sede san luigi , orbassano , italy 2sc radiodiagnostica i e ii ospedale san giovanni battista , torino , italy 3sc radiodiagnostica ospedale s . 
ninety - eight patients with cerebral tumours , 46 of which were primary ( seven grade 0 - i , nine low - grade gliomas , two gliomatosis cerebri , nine lymphomas and 19 high - grade gliomas ) and 52 secondary , underwent conventional magnetic resonance ( mr ) imaging completed with dwi and dynamic contrast susceptibility pwi . 
seventeen of 98 tumours were cystic or necrotic ( 12 / 17 hypointense and 5 / 17 hyperintense on dwi ) ; the adc value of hyperintense cystic areas was 0.970.2310 - 3 mm2 / s . 
novantotto pazienti con tumore cerebrale , 46 con tumore primitivo ( 7 di grado 0 - i , 9 gliomi a basso grado , 2 gliomatosi cerebri , 9 linfomi , 19 gliomi ad alto grado ) e 52 con metastasi sono stati sottoposti ad esame rm convenzionale completato da acquisizione dwi e da studio perfusionale ottenuto durante la somministrazione di un bolo di gadolinio . 
diciassette tumori erano costituiti da una componente centrale cistica che in 5 casi era iperintensa in dwi ( valore medio adc 0 , 970 , 2310 - 3 mm2 / s )  . ladc della parte solida dei tumori aveva valori compresi tra 0 , 64 e 3 , 510 - 3 mm2 / s . 
la pwi fornisce elementi utili nella diagnosi differenziale tra gliomi a basso ed alto grado e tra gliomi ad alto grado e linfomi . parole chiave risonanza magnetica diffusione perfusione tumori cerebrali introduction introduzione the role of conventional magnetic resonance ( mr ) imaging , with or without contrast agent administration , in the diagnosis of brain tumours is widely accepted . 
mr imaging not only has high sensitivity in detecting and locating lesions , it also gives information about phenomena such as mass effect , haemorrhage , oedema or necrosis , thus helping to differentiate brain tumours from other pathological processes and providing indications about the type of tumour [ 1 , 2 ]  . the importance of characterising tumours ( typing and grading ) to plan appropriate treatment and monitor response to treatment early on in the disease has stimulated research in this area , with numerous studies investigating , over the past decade , the application of new techniques such as diffusion - weighted imaging ( dwi ) , perfusion - weighted imaging ( pwi ) and in vivo mr spectroscopy ( mrs ) [ 14 ]  . the term diffusion refers to the random ( brownian ) movement of water molecules in tissues ; the diffusion capacity of water molecules is tissue - specific and may be altered in given pathological conditions . 
dwi enables assessment of this tissue - related parameter , and calculation of the apparent diffusion coefficient ( adc ) provides major diagnostic clues for evaluating intracranial masses [ 2 , 5 ]  . perfusion reflects the delivery of nutrients to tissue and is defined as flow per unit of time . 
the grey matter of a healthy individual is perfused at a rate of 5060 ml / 100 g / min and the flow maintained in a restricted range by cerebral self - regulation mechanisms . 
low - perfusion states may thus lead to cellular ischaemia , whereas high - perfusion states may be related to hypervascular lesions such as certain tumours [ 6 ]  . the most commonly measured perfusion parameters are cerebral blood volume ( cbv ) , which reflects the amount of blood present in a given amount of tissue at a given time ; cerebral blood flow ( cbf ) , which indicates the quantity of blood transiting through a given amount of tissue in a unit of time ; and mean transit time ( mtt )  . 
these parameters are closely linked to one another , with cbf being equal to the il ruolo della risonanza magnetica ( rm ) convenzionale , con e senza mezzo di contrasto ( mdc ) , nella diagnosi dei tumori dellencefalo saldamente consolidato ; la rm non solo possiede unelevata sensibilit nel riconoscimento e nella localizzazione delle lesioni , ma fornisce informazioni su fenomeni quali leffetto massa , lemorragia , ledema o la necrosi dei tessuti che aiutano nella diagnosi differenziale con altri tipi di processi patologici dando anche indicazioni sul tipo di tumore [ 1 , 2 ]  . limportanza della caratterizzazione ( tipo e grading ) dei tumori , al fine della corretta impostazione terapeutica , nonch lutilit di fornire precoci informazioni sulla risposta alla terapia ha stimolato in questi ultimi anni la ricerca e , nellultima decade , sono stati pubblicati numerosi studi riguardanti limpiego delle nuove tecniche quali la diffusione ( dwi ) , la perfusione ( pwi ) e la spettroscopia in vivo ( mrs ) nella caratterizzazione dei tumori cerebrali [ 14 ]  . con il termine diffusione si indica il movimento random ( browniano ) delle molecole di acqua nei tessuti ; la diffusibilit delle molecole dellacqua caratteristica per ogni tessuto e si pu modificare in determinate condizioni patologiche . 
le sequenze pesate in diffusione permettono di valutare questo parametro tessutale ed il calcolo del coefficiente di diffusione apparente ( adc ) fornisce elementi diagnostici importanti nella valutazione delle masse intracraniche [ 2 , 5 ]  . la perfusione rappresenta lapporto nutritivo ematico ai tessuti e viene definita come il flusso per unit di tempo . solitamente viene misurata in ml / 100 g di tessuto / min , o unit di cbf . 
la sostanza grigia delluomo sano viene perfusa ad un ritmo di 5060 ml / 100 g / min e viene mantenuta in un range ristretto dai meccanismi di autoregolazione cerebrale . 
perci stati di bassa perfusione possono sfociare nellischemia cellulare , mentre stati di elevata perfusione possono essere correlati a lesioni ipervascolari , come alcuni tumori [ 6 ]  . i parametri che pi frequentemente vengono misurati sono : il cbv ( cerebral blood volume ) che equivale alla radiol med ( 2009 ) 114 : 645659 ratio between volume and transit time [ 7 ]  . 
the most frequently used parameter in brain tumour imaging is the relative regional cerebral blood volume ( rrcbv ) , which is increased in tumours as a result of neoangiogenesis [ 8 , 9 ]  . this study correlated the adc and rrcbv values obtained by applying echoplanar ( epi ) and gradient - echo ( gre ) sequences in a large series of brain tumours with histological findings to evaluate the usefulness of this technique in characterising brain tumours . materials and methods in this prospective study conducted between january 2003 and august 2006 , patients with brain tumours were studied with conventional mr imaging complemented by dwi and pwi . 
from among these , 98 patients ( 53 men and 45 women ) were selected on the basis of the following exclusion criteria : lack of histological diagnosis , nonneoplastic lesions , previous treatments on the tumours ( surgery , chemotherapy , radiotherapy ) , incorrect examination technique . all lesions were characterised histologically . 
tumours were subdivided into primary and secondary ; the former were grouped by histological type and grade according to the world health organization ( who ) classification , whereas the latter were classified according to the tumour of origin . study protocol mr imaging was performed during a single session in all patients by using a superconducting 1 - tesla scanner ( signa horizon , ge ) with a maximum gradient strength of 23 mt / m and a slew rate of 77 mt / m / s . 
we used 1 m gadobutrol ( gadovist ) injected intravenously with the aid quantit di sangue presente in una data quantit di tessuto in un dato momento ; il cbf ( cerebral blood flow ) che indica la quantit di sangue che attraversa una data quantit di tessuto nellunit di tempo e lmtt ( mean transit time ) o tempo di transito medio . 
il parametro pi utilizzato nello studio dei tumori cerebrali il volume ematico regionale relativo ( rrcbv ) che aumenta nei tumori in rapporto ai fenomeni di neoangiogenesi [ 8 , 9 ]  . in questo lavoro vengono correlati i valori di adc e di rrcbv , ottenuti su unampia serie di tumori cerebrali utilizzando sequenze echo planari ( epi ) gradient echo ( gre ) , con il relativo dato isto - patologico , per valutare lapporto di questa tecnica nella caratterizzazione dei tumori cerebrali . materiali e metodi nel periodo compreso tra gennaio 2003 e agosto 2006 stato effettuato uno studio prospettico che prevedeva di completare lesame rm convenzionale con acquisizioni dwi e pwi nei pazienti con tumore cerebrale . 
tra questi sono stati selezionati 98 pazienti ( 53 maschi e 45 femmine ) utilizzando i seguenti criteri di esclusione : assenza della diagnosi istologica , lesioni non neoplastiche , pregressi trattamenti sul tumore ( chirurgia , chemioterapia , radioterapia ) , non corretta esecuzione dellesame . tutte le lesioni sono state caratterizzate istologicamente ; i tumori sono stati suddivisi in primitivi e secondari ; i primi sono stati raggruppati per istotipo e grado secondo la classificazione della who , mentre i secondi sono stati classificati sulla base del tumore dorigine . protocollo di studio la rm stata eseguita in tutti i pazienti in ununica seduta utilizzando un magnete superconduttivo operante a 1 tesla ( signa horizon , ge ) con potenza massima dei gradienti di 23 mt / m e slew - rate di 77 mt / m / s . 
 stata impiegata la bobina head di ricezione e trasmissione in quadratura . in tutti i pazienti stato eseguito un esame standard con impiego di sequenze se t1 ( tr / te 500 / 12 ms ) , fse pesate in t2 ( tr / te 4000 / 85 ms etl 13 ) e flair ( tr / te 8000 / 90 ms ti 2000 ms )  . 
sono state ottenute immagini sui tre piani dello spazio con sezioni di 45 mm e gap 0 , 51 mm . prima della somministrazione del mdc stata eseguita in tutti i casi una sequenza pesata in diffusione , sul piano 648 radiol med ( 2009 ) 114 : 645659 of a dual - syringe automatic injector ( medrad ) via an 18gauge needle cannula at a flow rate of 5 ml / s . 
in all cases , a few minutes before the dynamic phase , patients were administered 0.05 mmol / kg of gd as a prebolus to attenuate the t1 effects of bloodbrain barrier ( bbb ) disruption . to study the entire area of the lesion , we acquired a set of 12 slices repeated sequentially 40 times , thus obtaining 480 images in 1 min 12 s . 
all axial images were acquired with the same geometry ( fov , slice thickness , gap , angle ) to enable fusion of the dw and pw images with the corresponding flair and / or contrastenhanced t1 - weighted images . 
adc maps inclusive of the adc calculation were generated by positioning 25to 30 - mm2 regions of interest ( roi ) over the tumour areas . the mean adc values of solid and fluid components were obtained separately for each lesion . pw images were processed by applying a formula to calculate , starting from the baseline t2 value of tissues , the drop in signal during the passage of the bolus ( r2 ) and its subsequent return to the baseline level : r2 * = - 1n [ s ( t ) / s ( 0 ) / te ] where s ( t ) corresponds to the signal intensity at time ( t ) , s ( 0 ) represents the mean mr signal before the arrival of the contrast and te to echo time . 
mathematical integration of the area under r2 * curve ( negative enhancement integral ) corresponds to the cbv . to obtain cbv maps , a number of rois 2530 mm2 in diameter were placed over the tumour in such a way as to cover the entire lesion , and the enhancing and nonenhancing areas of tumour were evaluated separately . 
for each lesion , we calculated the mean rcbv of pathological tissue ( rcbvp ) and normal tissue ( rcbvn ) and the ratio between the two means , thus obtaining a value that we called rrcbv [ 10 ]  . 
stato utilizzato il gadobutrolo 1 m ( gadovist ) , iniettato endovena tramite lausilio di un iniettore automatico a doppia siringa ( medrad ) utilizzando unagocannula 18 g con velocit di flusso 5 ml / s . 
la dose somministrata stata per ogni paziente di 0 , 15 mmol / kg , seguita da 20 ml di soluzione fisiologica ; la fase dinamica stata sempre preceduta di pochi minuti dalla somministrazione di un prebolo di 0 , 05 mmol / kg di gadolinio per attenuare gli effetti t1 di alterazione della barriera ematoencefalica ( bee )  . sono state impostate 12 slices in modo da studiare interamente larea lesionale ripetute in maniera sequenziale per 40 volte ottenendo cos 480 immagini in un 112 . 
le prime 4 sequenze ( 48 slices ) , acquisite prima dellinizio della somministrazione del mdc per raggiungere lo stato di steady - state , sono state escluse dalle successive rielaborazioni . 
tutte le immagini assiali sono state acquisite con la stessa geometria : fov , spessore di strato , gap , inclinazione , per permettere la fusione delle immagini acquisite in dwi e pwi con le relative immagini flair e / o t1 post contrasto . 
dopo linfusione del mdc , sono state effettuate scansioni sui tre piani dello spazio ( coronale , sagittale ed assiale ) con sequenze se t1 - pesate . elaborazione delle immagini sono state successivamente rielaborate sia le immagini dwi sia quelle pwi utilizzando , sulla consolle operativa o sulla workstation ( adw 4.0 ) , un software fornito dalla ge ( functool 2 )  . 
per ogni lesione stata ottenuta separatamente la media delladc relativa alle componenti solide e a quelle fluide . le immagini pwi sono state elaborate applicando una formula che , partendo dal valore t2 di base dei tessuti , calcola la caduta di segnale durante il passaggio del bolo ( r2 ) e il successivo ritorno alla stato di partenza . r2 * = - 1n [ s ( t ) / s ( 0 ) / te ] dove s ( t ) corrisponde al segnale al tempo ( t ) ed s ( 0 ) rappresenta la media del segnale rm prima dellarrivo del contrasto e te il tempo di echo . 
the students t test for unpaired data was applied to the mean values obtained ; values of p < 0.0001 were considered to be statistically significant . results of the 98 patients , 46 had primary brain tumours and 52 had one or more secondary lesions ( table 1 )  . 
 of all tumours examined , 17 were morphologically composed of a necroticcystic central component surrounded by a strongly enhancing solid peripheral rim . the necroticcystic component was hypointense on dwi in 12 tumours and hyperintense in five . 
per ogni lesione stata calcolata la media del rcbv del tessuto patologico ( rcbvp ) e del tessuto sano ( rcbvn ) ed stato calcolato il rapporto tra le due medie ottenendo un valore che chiameremo rrcbv [ 10 ]  . 
ai valori delle medie cos ottenute stato applicato il test t di student per dati non appaiati ; sono stati considerati significativi valori di p < 0 , 0001 . risultati dei 98 pazienti 46 erano portatori di un tumore cerebrale primitivo e 52 di una o pi localizzazioni secondarie ( tabella 1 )  . tra tutti i tumori esaminati 17 erano costituiti morfologicamente da una componente centrale necrotico - cistica con spesso cercine periferico solido dotato di intenso contrast enhancement . 
the rrcbv values of the low - grade ( ii ) and high - grade ( iii - iv ) gliomas , as well as the values of highgrade gliomas and lymphomas , were analysed with students t test for unpaired data . 
the results are shown in tables 2 and 3 . twenty - nine of the brain metastases were from lung cancer , whereas the others were distributed as follows : seven from cancers of the uropoietic system ( six renal carcinomas and one bladder carcinoma ) , seven from breast cancer , four from gastrointestinal cancers , one from melanoma and three from lymphoma . 
a scansione assiale t1 pesata dopo somministrazione del mdc : lesione cistica con orletto iperintenso e cospicuo edema digitato della sostanza bianca perilesionale ; b analoga scansione in dwi : la lesione appare iperintensa ; c mappa adc : il valore di adc allinterno della componente cistica della lesione di 0 , 910 - 3 mm2 / s . 10 13 16 19 22 25 28 31 34 37 40 43 46 49 n pazienti metastasi tumori primari fig . 
2 rappresentazione grafica della distribuzione dei valori di adc nei vari tipi di tumori , distinti tra tumori cerebrali primitivi e metastasi . 652 radiol med ( 2009 ) 114 : 645659 fig . 
a contrast - enhanced t1 - weighted image ; b curves of signal decrease in the regions of interest ; c relative regional cerebral blood volume ( rrcbv ) maps . 
5 confronto dellrrcbv tra gliomi grado iii e grado iv . glioma di iv grado glioma di iii grado linfomi cerebrali gliomi ad alto grado 2 3 4 9 10 10 12 13 14 15 16 17 18 19 pazienti fig . 
i valori di rrcbv relativi ai gliomi a basso grado ( ii ) e quelli ad alto grado ( iii - iv ) , cos come i valori dei gliomi ad alto grado e quelli dei linfomi sono stati sottoposti a test statistici utilizzando la t di student per dati non appaiati ed i risultati ottenuti vengono riportati nelle tabelle 2 e 3 . ventinove delle metastasi encefaliche erano da carcinoma polmonare , mentre le altre erano cos ripartite : 7 da tumori dellapparato uropoietico ( 6 carcinomi renali e 1 carcinoma della vescica ) , 7 da carcinoma mammario , 4 da neoplasie dellapparato digerente , 1 da melanoma e 3 da linfoma . 
in the majority of cases , morphological imaging is able to differentiate low - grade from diffusely invasive or frankly malignant lesions , which tend to show significant perilesional oedema and intense contrast enhancement . radiol med ( 2009 ) 114 : 645659 i tumori neuroepiteliali , in particolare i glomi , rappresentano una causa frequente di tumori dellencefalo . 
gli esami radiologici morfologici sono in grado di differenziare nella maggior parte dei casi le lesioni di basso grado da quelle diffusamente infiltranti o chiaramente maligne che presentano generalmente un significativo edema perilesionale ed unelevata impregnazione contrastografica . 
ci nonostante , non tutte le neoplasie gliali ad alto grado presentano necrosi o effetto massa e circa il 40 % non presenta impregnazione contrastografica [ 2 , 11 ]  . il problema si complica se teniamo conto di altri due elementi : in primo luogo dellelevata frequenza delle metastasi cerebrali che si sviluppano in circa il 15%25% di tutti i pazienti con neoplasie maligne [ 12 ] e in secondo luogo dellaumentata incidenza dei linfomi cerebrali primitivi verificatasi nelle ultime due decadi per aumento della popolazione immucompromessa in relazione allincremento del numero di soggetti sottoposti a trapianto dorgano e di quelli con aids [ 13 , 14 ]  . la rm convenzionale dimostra molti limiti nella differenziazione tra i diversi gradi di tumori primari neuroepiteliali , le metastasi e i linfomi . 
nevertheless , not all high - grade glial tumours exhibit necrosis or mass effect , and approximately 40% of them are nonenhancing [ 2 , 11 ]  . the issue becomes more complex if we consider two other factors : first , the high frequency of cerebral metastases occurring in around 15%25% of all patients with malignancies [ 12 ] , and second , the rising incidence over the past two decades of primary cerebral lymphomas as a result of the increasing number of immunocompromised subjects due to organ transplantations and aids [ 13 , 14 ]  . conventional mr imaging has many limitations in distinguishing among the different grades of primary neuroepithelial tumours , metastases and lymphomas . 
for this reason , it is important to have access to a diagnostic imaging technique capable of enabling the rapid and noninvasive diagnosis and tumour monitoring [ 13 , 15 ]  . diffusion imaging by evaluating the mobility of water molecules in tissue , diffusion imaging can provide diagnostic information in several pathological conditions . 
in cerebral masses , the role of dwi and adc mapping in differentiating cystic tumours from abscesses and epidermoid from arachnoid cysts is known and well established [ 1618 ]  . the five cystic tumours with hyperintense fluid component on dwi resembled abscesses in appearance , although the adc values were slightly higher [ 18 , 19 ]  . 
the high mucinous content explains the adc restriction [ 1820 ]  . the adc of the solid component of the tumours showed wide variations without significant differences among the various types of tumour . 
in our series , the mean adc for lymphomas did not exceed 1.410 - 3 mm2 / s , a finding in agreement with previous reports [ 2 , 4 , 16 , 21 ]  . 
in fact , the extent of oedema strongly affects adc values , and it is likely that steroid treatment , frequently initiated at presentation in patients with brain tumours , influences the dwi parameters [ 22 ]  . perfusion imaging brain tumours may stimulate the formation of new vascular networks , and neoangiogenesis is fundamental for tumour growth . 
the increased metabolic demands of the growing tumour and the resulting hypoxia in large tumours stimulate fornire informazioni diagnostiche in svariate condizioni patologiche nel caso di masse cerebrali noto e consolidato il ruolo delle sequenze dwi e delle mappe delladc nel differenziare i tumori cistici dagli ascessi e le cisti epidermoidi dalle cisti aracnoidee [ 1618 ]  . i 5 tumori cistici con componente fluida iperintensa in dwi avevano un aspetto simile a quello degli ascessi , ma con valori di adc lievemente superiori [ 18 , 19 ]  . 
erano tutte metastasi da carcinoma polmonare ; allesame istologico larea cistica di questi tumori era costituita da tessuto mucinoso nel quale galleggiavano cellule neoplastiche , mentre non era evidenziabile contenuto ematico ; lelevata componente mucinosa spiega la restrizione del coefficiente di diffusione apparente [ 1820 ]  . per quanto concerne ladc delle componenti solide dei tumori i dati ottenuti dimostrano unampia variabilit di valori senza significativa differenza tra i vari tipi di neoplasie ; nella maggior parte dei casi tuttavia i valori di adc erano superiori rispetto a quelli del tessuto sano normale . 
dalla osservazione dei dati emerge che tra tutti i tipi tumorali i linfomi sono quelli che mostrano i valori complessivamente inferiori ; in questa casistica la media di adc per i linfomi non supera mai il valore di 1 , 410 - 3 mm2 / s ; questo concorda con i dati della letteratura [ 2 , 4 , 16 , 21 ]  . 
in realt lentit delledema condiziona molto i valori di adc ed probabile che il trattamento con farmaci corticosteroidei , frequentemente adottato gi allesordio della clinica nei pazienti con tumori cerebrali , influisca sui parametri ottenuti in dwi [ 22 ]  . imaging di perfusione i tumori cerebrali possono indurre la formazione di nuovi vasi ; la neoangiogenesi fondamentale per la crescita dei tumori . 
la prima tecnica , detta spin label , ancora in fase di studio e prevede di marcare i globuli rossi durante il passaggio nei vasi epiaortici e successivamente di valutarne il primo passaggio nel tessuto cerebrale [ 23 ]  . 
i mdc esogeni impiegati sono i chelati del gadolinio che non superano normalmente la bee e quindi si comportano come 656 radiol med ( 2009 ) 114 : 645659 the formation of cytokines responsible for angiogenesis [ 1 ]  . this process is closely related to biological aggressiveness and is one of the main parameters considered in the histopathological grading of glial tumours [ 1 ]  . 
the first technique , known as spin labelling , is still under development and involves tagging red blood cells during their passage in the epiaortic vessels and subsequently evaluating their first pass within cerebral tissue [ 23 ]  . 
the contrast agent compartmentalised inside vessels causes , on first pass when concentration is high , a drop in the t2 signal , which is best appreciated in t * gradient - echo sequences that are most heavily affected by magnetic susceptibility effects . 
studies comparing different gd concentrations have demonstrated that at the same dose levels , the use of 1 m gd increases the first - pass magnetic susceptibility effect , leading to curves with higher peaks [ 2426 ]  . one of the problems arising when evaluating concentration curves with dsci is leakage of contrast material into the extravascular space , which occurs in pathological conditions accompanied by bbb abnormalities . 
this problem can be overcome by administering a small dose of contrast material ( 0.05 mmol / kg ) approximately 5 min before initiating perfusion imaging [ 6 , 8 , 27 ]  . because the rcbv values obtained by applying the negative enhancement integral are not absolute , a standard reference is required to enable comparisons among different patients . 
this could be the rcbv obtained at the level of the contralateral white matter , or ipsilateral normal white matter in the case of lesions affecting both cerebral hemispheres . this provides the rrcbv value , which is calculated with the formula rrcbv = rcbvp / rcbvn [ 10 ]  . the results obtained in our series allow us to make a few concluding remarks . 
if we consider glial tumours , there are statistically significant differences ( p < 0.0001 ) between the rrcbv value of lowand high - grade gliomas ( table 2 )  . 
il mdc compartimentalizzato allinterno dei vasi determina , al primo passaggio , quando la concentrazione elevata , un abbattimento del segnale t2 , meglio valutabile utilizzando sequenze gradient - echo t2 * , che maggiormente risentono degli effetti di suscettibilit magnetica ; questa tecnica denominata con lacronimo dsci ( dynamic contrast susceptibility imaging ) [ 6 , 23 ]  . vengono abitualmente utilizzate sequenze epi che permettono di studiare un esteso volume cerebrale ed offrono il vantaggio di unelevata risoluzione temporale . 
in questo studio stato utilizzato gadolinio ( gd ) alla concentrazione 1 m somministrato a 5 ml / s con una dose pari 0 , 15 mmol / kg ; diversi studi condotti comparando concentrazioni diverse di gadolinio , hanno dimostrato che limpiego di gd 1 m , a parit di dose iniettata , aumenta leffetto di suscettibilit magnetica al primo passaggio per cui si ottengono curve con picco pi elevato [ 2426 ]  . uno dei problemi che insorge nella valutazione delle curve di concentrazione con effetto dsci rappresentato dallo stravaso di mdc nello spazio extravascolare che si verifica in quelle condizioni patologiche che si accompagnano ad alterazione della bee . 
un artificio per ovviare a questo problema quello di somministrare una piccola dose di mdc ( 0 , 05 mmol / kg ) circa 5 minuti prima dellacquisizione perfusionale [ 6 , 8 , 27 ]  . i valori di rcbv , ottenuti applicando lintegrale di enhancement negativo , non sono assoluti ; pertanto , per poter effettuare il confronto tra pazienti diversi , necessario utilizzare un riferimento standard che pu essere rappresentato dal valore di rcbv ottenuto a livello della sostanza bianca controlaterale alla lesione o della sostanza bianca sana omolaterale in caso di lesioni che interessano entrambi gli emisferi cerebrali . 
si ottiene in tal modo lrrcbv che si calcola con formula rrcbv = rcbvp / rcbvn [ 10 ]  . la seguente dai risultati ottenuti in questa casistica si possono trarre alcune considerazioni . 
se si considerano i tumori della serie gliale emergono delle differenze statisticamente significative ( p < 0 , 0001 ) del valore di rrcbv tra gliomi a basso grado e gliomi ad alto grado ( tabella 2 )  . 
pertanto se si fa la media del rcbv posizionando roi allinterno di tutto il tumore , ne deriva una riduzione complessiva dei valori di rrcbv nei tumori pi necroradiol med ( 2009 ) 114 : 645659 neoangiogenesis [ 28 ]  . 
all lymphomas were characterised by a low rrcbv value , constantly lower than 2 ( the maximum value observed was 1.53 ) , whereas the majority of high - grade gliomas had high rrcbv values . 
the differential diagnosis between lymphomas and gliomatoses is , however , straightforward at conventional mr imaging and based on morphology and tumour extension [ 30 , 31 ]  . lowest rrcbv values seen with regard to metastases , no statistically significant differences were seen in the perfusion values of the various types of metastases . 
the high rrcbv values seen in meningiomas , however , are in line with previous reports [ 15 , 26 ]  . conclusions diffusionand perfusion - weighted mr imaging in patients with brain tumours provide additional information that tici . 
per questo motivo stato ipotizzato di utilizzare oltre allimaging convenzionale anche le mappe di rrcbv come guida per effettuare le biopsie stereotassiche [ 29 ]  . se si confrontano i gliomi ad alto grado con i linfomi , per i quali la diagnosi differenziale con lrm convenzionale pu talvolta essere problematica , possiamo vedere come in questo studio i valori di perfusione diano risultati statisticamente significativi ( p < 0 , 0001 )  . 
tutti i linfomi erano caratterizzati da un valore di rrcbv basso , sempre inferiore a 2 ( il valore massimo riscontrato stato di 1 , 53 ) , mentre la maggior parte dei gliomi ad alto grado aveva valori di rrcbv elevati . 
la possibilit di discriminare tra tumori gliali ad alto grado e linfomi concorda con quanto gi riportato da altri studi [ 15 , 20 ]  . un discorso a parte va fatto per le gliomatosi cerebri . 
in questo studio sono compresi solo due casi , ed entrambi hanno bassi valori di rrcbv , simili a quelli dei linfomi e dei tumori low - grade ; questo dato correla con la ridotta microvascolarizzazione di questi tumori il cui grading elevato dato dalla elevata estensione . 
la diagnosi differenziale tra linfomi e gliomatosi tuttavia agevole allo studio rm convenzionale sulla base della morfologia e dellestensione del tumore [ 30 , 31 ]  . per quanto concerne le metastasi non sono invece state riscontrate differenze statisticamente significative dei valori di perfusione tra i vari tipi di metastasi . 
i dati ottenuti oscillano su un ampio range ; i valori di rrcbv risultano pi bassi nelle localizzazioni da linfoma ed in alcuni casi di metastasi da carcinoma del polmone o della mammella ; questultimo dato potrebbe essere correlato , almeno in parte , alle terapie a cui tali soggetti erano sottoposti per il tumore dorigine . 
i valori elevati di rrcbv riscontati nei meningiomi sono in linea con quanto riportato in letteratura [ 15 , 26 ]  . conclusioni le tecniche di diffusione e di perfusione con rm se utilizzate nei pazienti con tumore cerebrale forniscono informazioni non ottenibili con lesame convenzionale , possono essere eseguite a completamento dellesame convenzionale utilizzando lo stesso contrasto e con un minimo aumento del tempo di esecuzione . 658 radiol med ( 2009 ) 114 : 645659 cannot be obtained with conventional mr . 
should dwi and pwi prove superior to conventional imaging , they could be used to monitor patients undergoing treatment to obtain an earlier evaluation of response to chemoor radiotherapy and guide the clinicians treatment choices . le immagini dwi hanno rilevante importanza nella diagnosi delle masse cistiche , mentre non sembrano avere un ruolo nella caratterizzazione dei tumori . 
dwi e pwi inoltre si propongono come tecniche promettenti nel management dei tumori cerebrali : il dato relativo alla microvascolarizzazione offerto dalla pwi potrebbe servire come guida al prelievo bioptico , indicando le aree maggiormente aggressive . 
among the various therapies , local radiotherapy is the gold standard for pain palliation from single metastasis , even though the maximum benefit is obtained between 12 and 20 weeks from initiation . 
from november 2003 to may 2008 , ten ablation treatments were performed in ten patients with acute pain from metastatic bone lesions . patient selection and choice of the most appropriate ablation treatment was made based on lesion characteristics . 
three patients were treated with radiofrequency , one with plasma - mediated radiofrequency , two with plasma - mediated radiofrequency and cementoplasty , three with radiofrequency and cementoplasty and one with microwave . 
in both cases , 3 - month follow - up showed a statistically significant reduction of pain no case did local complications occur either during or after treatment . only one patient treated with radiofrequency ( 1 / 9 , 11% ) developed low - grade fever and general malaise during the 6 days following the procedure , compatible with a postradiofrequency syndrome , which was treated with riassunto obiettivo . 
tra le varie terapie , la radioterapia locale il gold - standard nella palliazione del dolore da metastasi singola , anche se il massimo beneficio si ottiene tra le 12 e le 20 settimane dallinizio della terapia . 
la valutazione stata effettuata non solo con imaging , ma anche con una vas score ( visual analoge scale ) per la determinazione del dolore e con la variazione delle dose equivalenti di morfina . 
solamente in un paziente trattato con radiofrequenza ( 1 / 9 , 11% ) abbiamo riscontrato nei 6 giorni successivi al trattamento insorgenza di febbricola e malessere generale compatibile con la sindrome postradiol med ( 2009 ) 114 : 608625 acetaminophen ( paracetamol ) only and resolved on day 7 . 
percutaneous ablation therapies represent a safe and valuable alternative for treating localised pain from single bone metastasis , providing rapid ( 4 - week ) relief of symptoms and a significant reduction in morphine doses . 
le tecniche ablative percutanee rappresentano una sicura e valida alternativa al trattamento del dolore localizzato da metastasi ossee singole , apportando in breve tempo ( 4 settimane ) un miglioramento della sintomatologia e una sensibile riduzione delle dosi di morfina . 
ci concorre a migliorare la qualit della vita in pazienti affetti da malattia metastatica . parole chiave metastasi osso palliazione ablazione introduction introduzione bone metastases are a common problem in cancer patients , affecting up to 30% of patients with epithelial cancers . 
in 70% of cases , the metastases originate from cancers of the prostate or breast , in 20%30% from cancers of the lung or kidney and in 10% from cancers of the rectum , colon , ovary and pancreas [ 1 ]  . the causes of pain in patients with bone metastases are not fully understood but appear to be unrelated to the type of tumour , location , number or size of the metastatic lesions . possible mechanisms of pain include stretching of the periosteum secondary to tumour growth , fractures ( both micro and macro ) , cytokine - mediated osteoclastic bony destruction that results in stimulation of the nerve endings in the endosteum and tumour growth into surrounding nerves and tissues [ 2 ]  . several types of treatment , including chemotherapy , hormonal therapy , surgery , radiotherapy and radiometabolic therapy , are used for palliation purposes . 
however , a number of patients fail to benefit from these conventional treatments , and pain relief , when achieved , does not occur until 412 weeks after treatment [ 3 ]  . 
a variety of alternative strategies have been proposed for treating painful bone metastases , all of which are based on image - guided percutaneous procedures for ablating focal bone lesions [ 1 , 4 , 5 ] , in some cases associated with cementoplasty [ 68 ]  . the aim of this study was to evaluate the technical success , effectiveness and possible complications of percutaneous ablation treatment in patients with painful bone metastases . 
esse nel 70% dei casi insorgono dal tumore della prostata o della mammella , nel 20%30% dal tumore del polmone o del rene , nel 10% dalle neoplasie del retto , colon , ovaio e pancreas [ 1 ]  . le cause di dolore in soggetti affetti da metastasi ossee non sono ancora completamente note , ma non sembrano correlate al tipo di tumore primitivo , alla localizzazione della lesione , al numero e alle dimensioni delle lesioni . 
possibili meccanismi nella genesi del dolore comprendono : stretching del periostio secondario alla crescita del tumore ; fratture ( sia micro - fratture che macro - fratture ) ; distruzione ossea di tipo osteoclastico citochino - mediata che determina una stimolazione delle fibre nervose terminali endostali ; crescita tumorale nelle strutture nervose e nei tessuti adiacenti [ 2 ]  . 
alcuni pazienti non riescono a trarre benefici da questi trattamenti convenzionali e il sollievo dal dolore , quando si verifica , non avviene mai prima di 412 settimane [ 3 ]  . 
sono state proposte varie strategie alternative per il trattamento delle metastasi ossee dolorose , che richiedono metodiche percutanee imaging - guidate finalizzate allablazione delle lesioni focali ossee [ 1 , 4 , 5 ] , in alcuni casi associando la cementoplastica [ 68 ]  . scopo del lavoro stato quello di valutare il successo tecnico , lefficacia e le eventuali complicanze in pazienti affetti da metastasi ossee sintomatiche e sottoposti a terapia ablativa percutanea . 
 610 radiol med ( 2009 ) 114 : 608625 materials and methods materiali e metodi between november 2003 and may 2008 , we performed ten ablation treatments in ten patients ( five men and five women ; mean age 62 years ; range 2882 ) with acute pain from bone metastases of different origin , site ( table 1 ) and size ( mean volume 63.25 cm3 ; range 218.93.3 cm3 ) ( table 2 )  . 
in all of these patients , the pain had proved refractory to conventional approaches . owing to the poor expected response , one patient received no treatment before the ablation procedure ( table 1 )  . 
three patients were treated with radiofrequency ( rf ) alone , one with plasma - mediated rf , two with plasma - mediated rf combined with cementoda novembre 2003 a maggio 2008 sono stati effettuati , nel servizio di radiologia del nostro ospedale 10 trattamenti in 10 pazienti , 5 uomini e 5 donne ( et media 62 anni , range da 28 a 82 anni ) con dolore acuto da lesioni metastatiche ossee di varia origine , sede ( tabella 1 ) e volume ( volume medio 63 , 25 cm3 , range da 218 , 9 a 3 , 3 cm3 ) ( tabella 2 )  . tutte le lesioni trattate erano osteolitiche . 
 quattro pazienti erano stati precedentemente sottoposti a radioterapia e chemioterapia , 1 paziente solo a radioterapia , 4 pazienti solo a chemioterapia : in questi casi si sono dimostrati refrattari alle terapie convenzionali . 
nessun paziente era suscettibile di trattamento chirurgico , per lassenza di rischio di frattura patologica . tre pazienti sono stati trattati solo con radiofrequenza ( rf ) , table 1 personal series patient no . / age / gender primary tumour histology site of metastasis radiotherapy chemotherapy bladder liver liver liver breast lung lung colon - rectum transverse colon uterine cervix carcinoma right 8th rib left 9th rib left ischiopubic ramus right 8th rib infiltrating lobular vertebra l4 carcinoma adenocarcinoma adenocarcinoma adenocarcinoma adenocarcinoma squamous cell carcinoma vertebra l1 left sacroiliac joint left acetabolum left ischiatic spine left iliac wing not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive not responsive n / et / sesso tumore primitivo istologia sede metastasi radioterapia chemioterapia vescica fegato fegato fegato mammella polmone polmone carcinoma carcinoma lobulare vertebra l4 infiltrante adenocarcinoma adenocarcinoma viii arcata costale destra ix arcata costale sinistra branca ischio - pubica sinistra viii arcata costale destra non responsivo non responsivo non responsivo non responsivo non responsivo vertebra l1 articolazione sacroilaca sinistra acetabolo sinistra spina ischiatica sinistra ala iliaca sinistra non responsivo non responsivo non responsivo non responsivo non responsivo non responsivo non responsivo non responsivo colon - retto colon trasverso portio uterina adenocarcinoma adenocarcinoma carcinoma squamocellulare hcc , carcinoma epatocellulare hcc , hepatocellular carcinoma tabella 1 serie personale 1 / 70 / m 2 / 69 / m 3 / 45 / m 4 / 40 / m 5 / 60 / f 6 / 73 / f 7 / 73 / f 8 / 82 / f 9 / 81 / m 10 / 38 / f 1 / 70 / m 2 / 69 / m 3 / 45 / m 4 / 40 / m 5 / 60 / f 6 / 73 / f 7 / 73 / f 8 / 82 / f 9 / 81 / m 10 / 38 / f radiol med ( 2009 ) 114 : 608625 table 2 descriptions of lesions and procedures per patient patient procedure lesion no . 
stato eseguito il calcolo del volume per ciascuna lesione attraverso la formula 4 / 3ab2 , dove a il semiasse maggiore e b il semiasse minore plasty , three with rf combined with cementoplasty and one with microwave ablation . 
 1 con radiofrequenza plasma - mediata , 2 con radiofrequenza plasma - mediata associata a cementoplastica , 3 con radiofrequenza associata a cementoplastica , 1 con microonde . tutti hanno completato il follow - up a 12 settimane . 
 pretreatment assessment before undergoing ablation treatment , patients were evaluated by means of a validated visual analogue scale ( vas ) for pain assessment and by recording any use of analgesics . inclusion criteria were moderate or severe pain rated 4 or more on the 10 - point vas ; patients with lower scores were treated with analgesics . 
pain was localised to the site corresponding to the lesion detected by computed tomography ( ct ) ( aquilon 64 , toshiba , tokyo , japan ) or magnetic resonance valutazione prima del trattamento prima dei trattamenti ablativi i pazienti sono stati valutati usando una codificata visual analogue scale ( vas ) per la determinazione del dolore , ed stato registrato leventuale utilizzo di analgesici . 
criteri di inclusione nello studio sono stati : dolore moderato o severo con valore uguale o superiore a 4 nella scala vas di 10 punti ; i pazienti con punteggio inferiore sono stati trattati con analgesici . 
prima del trattamento , tutti i pazienti inclusi nel nostro studio 612 radiol med ( 2009 ) 114 : 608625 table 3 morphine - equivalent doses for several opioids according to route of administration tabella 3 dosi equivalenti di morfina per diversi oppioidi a seconda della via di somministrazione administration route via di somministrazione parenteral dose equivalents oral dose equivalents parenterale dose equivalenti orale dose equivalenti morphine methadone codeine buprenorphine tramadol fentanyl 10 mg 10 mg 120 mg 0.3 mg 100 mg 25 mcg / hc 30 mga 20 mg 200 mg 0.4 mgb 120 mg morfina metadone codeina buprenorfina tramadolo fentanile 10 mg 10 mg 120 mg 0 , 3 mg 100 mg 25 g / h c 30 mga 20 mg 200 mg 0 , 4 mgb 120 mg achronic use ; bsublingual ; ctransdermal auso cronico ; bsublinguale ; ctransdermica ( mr ) imaging ( 1.5 tesla avanto , siemens , munich , germany )  . 
specifically , nine patients were imaged by contrast - enhanced ct ( iopamiro , bracco , milan , italy ) and one by contrast - enhanced mr imaging ( magnevist , schering , berlin , germany )  . 
exclusion criteria were the presence of more than two symptomatic lesions and safety margins less than 1 cm from the spinal cord , major motor nerve , brain , adamkiewicz artery , bowel and bladder [ 9 ]  . before the ablation treatment , patients were on analgesic therapy ( opioids or nsaids ) , which was translated into morphine - equivalent doses to render the data homogeneous ( table 3 )  . 
analgesic use was monitored before treatment and at 1 , 4 , 8 and 12 weeks thereafter . treatment selection depending on whether the lesion is osteoblastic or osteolytic , the most beneficial ablation method , that is , the one best suited to the individual metastasis , must be selected . both rf and microwave ablation are based on the use of heat , although heat production occurs in two different manners : rf generates heat by delivering electrical current to tissues and causing ion agitation and friction ; electromagnetic microwave generates heat by agitating water molecules in tissue and producing friction [ 10 ]  . 
plasma - mediated rf ( coblation ) consists of using electrical energy to create a field of ionised particles that break the organic bonds within soft tissue ( ablation )  . 
il dolore era localizzato alla sede corrispondente alla lesione evidenziata con indagini eseguite con tomografia computerizzata ( tc ) ( aquilon 64 , toshiba , tokio , giappone ) o risonanza magnetica ( rm ) ( 1 , 5 tesla avanto , siemens , munich , germania ) ; in particolare 9 pazienti sono stati sottoposti a tc con mdc ( iopamino , bracco , milano , italia ) e 1 paziente a rm con mdc paramagnetico ( magnevist , schering , berlin , germania )  . 
criteri di esclusione al trattamento ablativo sono stati : la presenza di pi di due lesioni sintomatiche ; margini di sicurezza inferiori a 1 cm dal midollo spinale , dal nervo motorio maggiore , dallencefalo , dallarteria di adamkiewicz , dallintestino e dalla vescica [ 9 ]  . 
prima del trattamento i pazienti erano in terapia con analgesici ( oppioidi o farmaci anti - infiammatori non steroidei ) , convertiti poi , ai fini di rendere omogenei i dati , in dosi - equivalenti di morfina ( tabella 3 )  . 
tutti i pazienti assumevano dagli 80 ai 100 equivalenti di morfina . lutilizzo di analgesici stato monitorato prima della procedura , alla prima , alla quarta , allottava e alla dodicesima settimana susseguenti la stessa . selezione della tipologia di trattamento in questa fase occorre valutare , a seconda che la lesione sia osteoblastica o osteolitica , quale sia il trattamento ablativo di cui pu giovare il paziente , ovvero il pi adatto a quella specifica metastasi . 
sia lablazione con radiofrequenza che quella con microonde caratterizzata dallimpiego di calore , che avviene con due modalit differenti : la rf genera calore tramite lattrito causato dallagitazione ionica che si ha al passaggio di corrente elettrica , le microonde invece generano calore per le oscillazioni delle molecole dacqua tissutali provocate dallinterazione tra le radiazioni elettromagnetiche e le stesse molecole dacqua [ 10 ]  . 
in particolare la radiofrequenza utilizzabile solo in lesioni osteolitiche o miste , ma non pu essere usata nelle radiol med ( 2009 ) 114 : 608625 there is a need for greater precision and control during the procedure and for treating osteoblastic lesions . 
it may be performed provided that the cortical bone is intact . procedure procedures were carried out with the patient under deep sedation achieved with the cyclic administration of alfentanil ( 0.51 mg ) and midazolam ( 13 mg ) and continuous infusion of propfol ( 50120 mg )  . 
blood pressure was checked every 4 m local anaesthesia ( 1% carbocaine ) was applied to the skin at the access site . different types of imaging were used to guide the procedure : ultrasound ( iu22 , philips , best , the netherlands ) in four cases , ultrasound and fluoroscopy ( allura xper fd , philips ) in one case , ct ( aquilon 64 , toshiba , tokyo , japan ) in three cases , ct fluorography in one case and carm cone - beam ct in one case ( xper ct , allura , philips ) ( table 2 )  . 
1 ago da rf posizionato allinterno di una lesione iliaca . lesioni osteoblastiche , dato che in questo caso non avviene conduzione di calore ; non pu essere impiegata neanche se la lesione si trova in prossimit di organi come il midollo spinale ( esempio metastasi vertebrale ) per il rischio di lesioni da calore [ 11 ] ; lablazione con microonde indicata se la lesione voluminosa e non in prossimit di organi termosensibili . 
la radiofrequenza plasma - mediata ( coblazione ) consiste nellutilizzo dellenergia elettrica atta a creare un campo di particelle ionizzate che spezzano i legami organici allinterno dei tessuti molli ( ablazione )  . 
infine il trattamento combinato con cementoplastica consiste nelliniezione di cemento preceduto da un qualsiasi trattamento ablativo e si pu effettuare a patto che sia integra la corticale ossea . procedura la procedura stata eseguita in sedazione profonda con somministrazione ciclica di alfentanyl ( 0 , 51 mg ) e mydazolam ( 13 mg ) e infusione continua di propofol ( 50120 mg ) ; stata somministrata una ultra short term profilaxis ( 1 g di cefazolina )  . 
 stata effettuata anestesia locale con 1% di carbocaina nella zona cutanea di introduzione dellago . sono state impiegate differenti tipologie di imaging per la guida : in 4 casi stata impiegata guida ecografica ( iu22 , philips , best , olanda ) , in 1 caso guida ecografica e fluoroscopica ( allura xper fd , philips , best , olanda ) , in 3 casi guida tc ( aquilon 64 , toshiba , tokio , giappone ) , in 1 caso guida fluoro - tc e in 1 caso la c - arm cone - beam tc ( xper ct , allura , philips , best , olanda ) ( tabella 2 )  . 
in tutti i casi trattati con radiofrequenza stato utilizzato un ago da 17 gauge con diametro di apertura degli uncini allestremit di 4 cm ; il generatore di rf , durante il passaggio di energia , rileva limpedenza elettrica del tessuto . 
la procedura stata condotta in accordo ai protocolli forniti dalle 614 radiol med ( 2009 ) 114 : 608625 17 - gauge needle with a maximum hook - deployment diameter of 4 cthe rf generator measures electrical impedance of tissue during the passage of energy . 
plasma - mediated rf procedures ( coblation ) were performed with a cavity spinewand kit ( arthrocare corp , sunnyvale , ca , usa )  . the device was directed anteriorly through the tissue to be ablated . 
in the cases undergoing combined treatment with cementoplasty ( fig . 5a , b ) , the rf electrode was introduced through an 11 - gauge simko needle ( simko special vertebroplasty needle , optimed )  . 
after withdrawal of the rf electrode , the simko needle was connected to a system ( cement - king application system , optimed ) for the injection of cement ( osteopal v , biomet , merck )  . 
per la procedura di radiofrequenza plasma - mediata ( coblazione ) , stato usato un kit cavity spinewand ( arthrocare corp , sunnyvale , ca , usa ) ; il dispositivo stato diretto anteriormente attarverso il tessuto da ablare . 
 la fattibilit della procedura combinata con cementoplastica stata sancita dalla possibilit di effettuare un corretto posizionamento dellago allinterno della lesione , mentre il successo tecnico stato inteso come la possibilit sia di effettuare lablazione allinterfaccia tra tessuto molle e osso sia di iniettare cemento nel caso del trattamento combinato . 
2 schema che mostra la modalit di ablazione con movimento rotatorio del dispositivo di radiofrequenza plasma - mediata allinterno della lesione in direzione dei diversi orientamenti orari a ore 3 , 6 , 9 e 12 . radiol med ( 2009 ) 114 : 608625 fig . 
evidente la presenza di cemento nella lesione ablata ( freccia )  . the possibility of achieving correct needle placement inside the lesion , whereas technical success was defined as the ability to achieve ablation at the interface between soft tissue and bone and then to inject cement in the case of combined treatments . 
 risultati il successo tecnico , inteso come la possibilit di effettuare lablazione allinterfaccia tra tessuto molle e osso e di iniettare cemento nel caso del trattamento combinato , stato raggiunto nel 100% dei casi . 
la termoablazione con rf ha raggiunto in tutti i casi dimensioni di necrosi di circa 4 cm , mentre la termoablazione con microonde ha creato unarea di necrosi superiore ai 6 cm in 10 minuti . 
il tempo totale delle procedure ( intese come la sola ablazione o lablazione associata a cementoplastica ) variava da un massimo di 25 minuti a un minimo di 15 minuti . 
solamente in un paziente trattato con radiofrequenza ( 1 / 9 , 11% ) abbiamo riscontrato nei 6 giorni successivi al trattamento insorgenza di febbricola e malessere generale compatibile con la sindrome post - radiofrequenza , risoltisi poi al settimo giorno e trattati solo con acetaminofene ( paracetamolo ) [ 12 ]  . riguardo alla valutazione con scala vas , la risposta di tutti i pazienti nella valutazione del dolore prima della procedura era di 8 punti ( in una scala da 0 a 10 )  . 
attraverso una valutazione a 1 , 4 , 8 e 12 settimane , emerso che il valore medio nella scala vas stato rispettivamente di 4 , 1 la prima settimana e 2 nei radiol med ( 2009 ) 114 : 608625 table 4 results of the follow - up in terms of reduction of pain and morphine - equivalent dose . 
 pain reduction ( vas ) morphine - equivalent dose before 24 h 1 week 4 week 8 week 12 week before 1 week 4 week 8 week 12 week tabella 4 risultati nel follow - up in termini di riduzione del dolore e dose in equivalenti di morfina . 
in due casi ( pazienti n 7 e n 9 ) essa aumentata di 10 equivalenti di morfina tra lottava e la dodicesima settimana dal trattamento ( vedasi testo ) riduzione del dolore ( vas ) dose in equivalenti di morfina prima 24 h sett 1 sett 4 sett 8 sett 12 prima sett 1 sett 4 sett 8 sett 12 complications ( cement leakage )  . 
pain regression was considered statistically significant at a p value of < 0.001. the wilcoxon test for paired data was used to evaluate when this difference was already statistically significant . 
 results technical success , defined as the ability to achieve ablation at the interface between soft tissue and bone and to inject controlli a 4 , 8 e 12 settimane ( tabella 4 )  . 
rf ablation produced an area of necrosis of approximately 4 cm in all cases , whereas microwave ablation produced an area of necrosis > 6 cm in 10 mprocedure times were also shorter with the plasma - mediated rf technique ( 20 min )  . 
total procedure time ( referring to ablation alone or combined ablation and cementoplasty ) ranged regressione lineare logaritmica con p < 0 , 001 statisticamente significativa ; in particolare la differenza tra prima del trattamento e a una settimana dal trattamento significativamente aumentata ( dolore post - procedurale ) , per i motivi precedentemente esposti , mentre vi una significativa diminuzione della dose di morfina tra prima del trattamento e la quarta settimana successiva allo stesso . radiol med ( 2009 ) 114 : 608625 from 25 min to 15 m in no cases did local complications occur either during or after treatment . 
in only one case of rf ablation ( 1 / 9 , 11% ) did the patient develop low - grade fever and general malaise during the 6 days after treatment , compatible with a postradiofrequency syndrome . 
this was treated with acetaminophen only ( paracetamol ) and resolved on day 7 [ 12 ]  . with regard to vas score , all patients had a pain score of 8 ( on a scale from 0 to 10 ) before the procedure . 
after day 1 , the score decreased by 1 point in 9 / 10 patients and by 2 points in the patient treated with microwave ablation . evaluation at 1 , 4 , 8 , and 12 weeks showed that the mean vas score was 4.1 at week 1 , and 2 at 4 , 8 and 12 weeks ( table 4 )  . 
 analgesic dose increased during week 1 ( from 10 to 20 morphine equivalents ) , probably owing to postprocedural pain , but then decreased substantially after 1 month in all patients ( from 50 to 30 morphine equivalents ) ( table 4 )  . 
in two cases ( patients 7 and 9 ) , it increased by ten morphine equivalents between 8 and 12 weeks , most likely because of the appearance of a new bone metastasis at another site from the one previously treated ( table 4 )  . 
in particular , the difference between pretreatment and 1 - week posttreatment increased significantly ( postprocedural pain ) for the reasons described above , whereas there was a significant reduction in the morphineequivalent dose between pretreatment levels and week 4 after treatment . discussion several therapies are used for the palliation of bone metastases , including chemotherapy [ 13 ] , hormonal therapy [ 14 , 15 ] , surgery [ 1618 ] and radiotherapy ( local transcutaneous radiotherapy , hemibody irradiation , radionuclide therapy ) [ 3 , 19 , 20 ]  . 
a number of patients fail to benefit from these conventional treatments , however , and pain relief , when it does occur , is never achieved before 412 weeks [ 3 ]  . 
if , on the one hand , chemotherapy reduces the primary mass and secondary lesions in 20%80% of patients , on the other hand , it leads to drug resistance and recurrence of bone pain . in addition , myelodepression is common due to the toxicity of many drugs used in current treatment protocols . hormonal therapy is only effective in breast and prostate tumours , where it relieves pain from bone metastases in discussione attualmente nel trattamento palliativo delle metastasi ossee vengono utilizzate varie terapie , tra cui la chemioterapia [ 13 ] , la terapia ormonale [ 14 , 15 ] , la chirurgia [ 1618 ] e la radioterapia ( radioterapia transcutanea locale , irradiazione emicorporea , radioisotopoterapia con radionuclidi ) [ 3 , 19 , 20 ]  . 
alcuni pazienti non riescono a trarre benefici da questi trattamenti convenzionali e il sollievo dal dolore , quando si verifica , non avviene mai prima di 412 settimane [ 3 ]  . 
se da un lato la chemioterapia riduce la massa primitiva e le lesioni secondarie nel 20%80% dei pazienti , dallaltro induce farmacoresistenza e ripresa del dolore osseo ; inoltre frequente linsorgenza di mielodepressione data la tossicit di molti farmaci utilizzati negli attuali protocolli terapeutici . 
la terapia ormonale efficace solamente nei tumori della mammella e della prostata , dove tuttavia induce sollievo dal dolore delle metastasi ossee in pi del 70% dei casi [ 14 ]  . 
infine la radioterapia locale gravata nel 60% dei casi da effetti tossici ( nausea , vomito e diarrea ) e la radioisotopoterapia da una parte dimostra efficacia nei soggetti con metastasi ossee multiple , dallaltra non considerata trattamento standard per le metastasi singole . sulla base di queste considerazioni i farmaci analgesici ( oppioidi e fans ) spesso rimangono lunica alternativa nel dolore metastatico e in alcuni casi rimangono lunica alternativa per la palliazione della sintomatologia . 
 noto che gli effetti collaterali , soprattutto nei trattamenti prolungati , sono costipazione , grave limitazione dello stato fisico e mentale , nonch cirrosi e coma epatico . diversi autori hanno studiato varie strategie alternative per il trattamento del dolore da metastasi ossea che comportano lutilizzo di metodiche percutanee imagingguidate con lo scopo di ablare le lesioni focali ossee : etanolo , termoterapia interstiziale laser - indotta , ablazione con radiofrequenza ( rfa ) percutanea e , pi recentemente , crioablazione [ 2 , 4 , 11 ]  . 
la nostra esperienza si riferisce alla risposta di 10 pazienti al trattamento della sintomatologia dolorosa con diverse tecniche di radiologia interventistica che includono tecniche ablative ( termoablazione con rf , termoablazione con radiofrequenza plasma - mediata , termoablazione con microonde ) associate o meno alla 620 radiol med ( 2009 ) 114 : 608625 > 70% of cases [ 14 ]  . 
finally , local radiotherapy produces toxic effects ( nausea , vomiting and diarrhoea ) in 60% of cases , and radionuclide therapy is effective in patients with multiple bone metastases but is not considered standard treatment for a single metastasis . on the basis of these considerations , analgesics ( opioids and nsaids ) are often the only option for metastatic pain , and in some cases for palliation of symptoms . 
the world health organization ( who ) [ 21 ] recommends a three - step approach : ( 1 ) initial treatment with nsaids such as aspirin , ibuprofen , naproxen , ( 2 ) if pain persists , use of mild opioids such as codeine and hydrocodone , ( 3 ) for persisting moderate or severe pain , high doses of opioids such as morphine , hydromorphone , or fentanyl as an intermittent or continuous infusion . 
known side - effects , above all in long - term treatments , are constipation , severe physical and mental impairment , cirrhosis and hepatic coma . several authors have investigated alternative approaches to painful bone metastases , all of which involve using percutaneous image - guided methods to ablate focal bone lesions : ethanol , laser interstitial thermal therapy , percutaneous rf ablation and , more recently , cryoablation [ 2 , 4 , 11 ]  . 
this study reports on the response of ten patients treated with different interventional radiology techniques , namely , ablation techniques ( rf ablation , plasma - mediated rf ablation , microwave ablation ) used alone or in combination with cementoplasty . 
in agreement with the literature [ 11 ] , we treated patients with up to two bone metastases ( lytic or mixed , but not osteoblastic ) causing acute disabling pain . pain was poorly controlled with conventional treatments . ablation techniques are successful in relieving pain only if the needle is placed at the interface between soft tissue and bone . 
the advantage of rf ablation lies in the use of electrodes that have a smaller diameter compared with the microwave antennas , an aspect that should theoretically reduce complications related to electrode deployment . 
microwave treatment has the advantage of shorter procedure times and the ability to ablate larger lesions than those usually treated with rf , thanks to the possibility of placing two antennas simultaneously indeed , in one of our patients , its use was cementoplastica . 
in accordo con le indicazioni della letteratura [ 11 ] , sono stati trattati pazienti che non avessero pi di due metastasi ossee , che queste fossero litiche o miste , ma non blastiche , e che , soprattutto , fossero causa di dolore acuto e invalidante . 
in questi pazienti , il followup non si ferma solo al dato di diagnostica per immagini , ma si concentra sulla efficacia clinica del trattamento , ossia sulla riduzione del dolore . in questo studio sono state trattate tre lesioni solo con radiofrequenza e una solo con microonde . 
gli svantaggi invece rispetto allimpiego di microonde sono dati da tempi lunghi di procedura ( circa 30 minuti ) e dalla necessit di effettuare pi posizionamenti in caso di ampio volume da ablare . 
il trattamento con microonde ha invece il vantaggio di giovare di una procedura pi breve e di poter ablare lesioni di dimensioni maggiori rispetto a quelle usualmente trattate con radiofrequenza , ci per la possibilit di posizionare due antenne contemporaneamente . 
infatti , in una nostra paziente , lampia superficie di contatto softtissue - osso ha giustificato il suo utilizzo : lablazione ha garantito in un tempo inferiore rispetto alla rf un volume di necrosi superiore . 
inoltre , dal punto di vista della qualit dellablazione , studi sperimentali e clinici [ 10 , 22 , 23 ] hanno evidenziato che il trattamento con microonde garantisce il raggiungimento di temperature intra - lesionali pi elevate , una minore dispersione di calore e quindi unefficacia superiore rispetto alla termoablazione con rf nelle lesioni in prossimit dei vasi sanguigni . 
infine con la metodica delle microonde la diminuzione del dolore stata pi sensibile ( 2 punti bpi ) dopo 24 ore dal trattamento rispetto alle altre metodiche utilizzate ( 1 punto bpi ) , per poi allinearsi con i dati ottenuti dalle altre tecniche nelle fasi successive . 
 le metodiche di termoablazione con radiofrequenza e con microonde hanno comunque linconveniente di non poter essere utilizzate nelle metastasi osteoddensanti , dato che il tessuto osseo non favorisce la conduzione di calore ( radiofrequenza ) n lagitazione di molecole dacqua ( microonde )  . nelle metastasi osteoddensanti possibile utilizzare la crioablazione che ha per lo svantaggio di impiegare aghi di grosse dimensioni e di avere tempi lunghi di procedura [ 2 ]  . inoltre sia la radiofrequenza che le microonde possono provocare lesioni termiche ad organi adiacenti . 
per ovviare radiol med ( 2009 ) 114 : 608625 justified by the extensive contact area between soft tissue and bone , and the ablation procedure produced a larger necrosis volume in a shorter time compared with rf . 
in addition , from the viewpoint of the quality of ablation , experimental and clinical studies [ 10 , 22 , 23 ] have shown that microwave treatment provides higher intralesional temperatures and less heat dispersion and consequently better effectiveness compared with rf ablation in lesions located in proximity to blood vessels . 
finally , microwave ablation provided greater pain relief [ 2 points on the brief pain inventory ( bpi ) ] than did the other methods ( 1 point bpi ) 24 h after treatment before becoming aligned with the other methods at subsequent follow - up assessments . 
 rf and microwave ablation methods both suffer the same limitation of not being applicable to osteoblastic lesions , as bone tissue does not allow the conduction of heat ( radiofrequency ) or the agitation of water molecules ( microwaves )  . 
to avoid this complication , several possibilities exist : to create an air ( in microwave ) interface or water ( in rf ablation ) interface to limit the ablation area ; to place thermocouples close to the structures at risk of thermal injury , as these can guide the operator in continuing or discontinuing the procedure by providing feedback on temperature ; to use bipolar rf , which through an electrode thermally shielded by another opposing electrode ensures well - delimited ablations [ 24 ] ; to use plasma - mediated rf ablation [ 25 ]  . a distinctive feature of plasma - mediated rf ablation ( coblation ) is the ability to release , in an extremely precise manner , a minimal amount of heat ( unlike conventional electrosurgery ) , a crucial factor in treating vertebral lesions . the low rf energy ( 100 khz ) is thus used to excite the electrolytes in a conductive medium ( plasma ) , such as saline solution or the aqueous intracellular environment , creating an area of highly ionised particles immediately adjacent to the electrode tip . 
this molecular dissociation process converts the ablated tissue into gas , creating a cavity at the treatment site [ 25 ] , which accounts for its suitability for osteolytic lesions . coblation in this study was used for a metastasis to a rib in a patient who had undergone right liver resection for hepatocarcinoma and had shown , on preprocedural ct , a bowel loop adjacent to the inner aspect of the affected rib . coblation was used to avoid damaging the bowel wall , and indeed , it allowed for extreme precision in delimiting the ablation margins . with regard to our results , in all cases pain , reduction a tale complicanza , si hanno diverse possibilit : creare uninterfaccia o con aria ( nelle microonde ) o con acqua ( nellablazione con rf ) per limitare il territorio di ablazione . 
possibile inoltre posizionare termocoppie a ridosso delle strutture a rischio di danno termico , che misurando la temperatura durante la procedura , sono utili alloperatore nel decidere se interrompere o meno lablazione ; utilizzare la radiofrequenza bipolare , che attraverso un elettrodo schermato termicamente da un secondo elettrodo opposto al primo , garantisce ablazioni ben definite [ 24 ] ; utilizzare la radiofrequenza plasma - mediata [ 25 ]  . nella tecnica di termoablazione con radiofrequenza plasma - mediata ( coblazione ) caratteristica identificativa la capacit di cedere , in maniera molto precisa , una quantit minima di calore ( contrariamente allelettrochirurgia convenzionale ) , fattore importante per esempio nel trattamento di lesioni vertebrali . 
la bassa energia di radiofrequenza ( 100 khz ) viene quindi utilizza per eccitare gli elettroliti in un mezzo conduttivo ( plasma ) , come una soluzione fisiologica o lambiente acquoso intracellulare , in modo da formare unarea di particelle altamente ionizzate nellarea immediatamente adiacente alla punta del dispositivo . 
questo processo di dissociazione molecolare converte il tessuto ablato in gas e in questo modo si viene a creare una cavit nella zona del trattamento [ 25 ] , trovando dunque particolare indicazione nelle lesioni osteolitiche . la coblazione stata utilizzata in questo studio per la lesione costale di un paziente che , in seguito ad epatectomia destra per exeresi di una neoplasia epatica , evidenziava allesame tc , eseguito prima del trattamento , unansa intestinale adiacente alla faccia interna della costa interessata dalla lesione . 
per evitare di danneggiare la parete dellansa , stata impiegata la coblazione che , in effetti , ha dimostrato notevole precisione nella definizione dei limiti dellablazione e ne ha quindi giustificato limpiego . in merito ai risultati , in tutti i casi abbiamo ottenuto un decremento del dolore tale da dimezzare , allottava settimana dal trattamento , la dose di equivalenti di morfina necessari per controllare il dolore . 
qualunque sia la tecnica ablativa utilizzata , il meccanismo di riduzione del dolore non ancora chiaro , ma vi sono alcune ipotesi : distruzione delle fibre sensoriali del periostio e della corticale ; decompressione meccanica del volume tumorale ; distruzione delle cellule tumorali che producono citochine come tnf ( fattore di necrosi tumorale alfa ) e interleuchine che promuovono la trasmissione del dolore ; inibizione dellattivit degli osteoclasti [ 26 , 27 ]  . 
regardless of the ablation technique used , the mechanism by which pain is reduced is not understood , although several hypotheses have been proposed : destruction of the periosteal and cortical sensory nerve fibres , mechanical decompression of the tumour volume , destruction of tumours cells that produce cytokines such as tumour necrosis factor alfa ( tnf - ) and interleukins that promote pain transmission , and inhibition of osteoclast activity [ 26 , 27 ]  . 
 [ 28 ] , in a study of 12 patients , demonstrated that rf is a safe and effective treatment that improves quality of life and reduces analgesic use in patients with bone metastases . 
 [ 29 ] reported major complications in three patients : one second - degree burn at the grounding - pad site , one case of transient bladder and bowel incontinence and one case of fracture of the acetabulum 6 weeks after rf treatment of an acetabular lesion . 
studies of coblation on bone lesions [ 25 ] investigated the use of rf ablation to treat vertebral lesions only ( for which no complications were reported ) , so we are unable to compare the results with our experience , as we used rf treatment in a costal lesion . 
 [ 9 ] presented the first experimental and clinical results of the use of microwave ablation in bone metastases , reporting excellent technical results in terms of volume of necrosis , speed of the procedure and absence of complications . 
 [ 29 ] , there may be a new rise in morphine - dose requirements long after treatment , indicative of the development of pain at other sites of metastases . 
 [ 28 ] , studiando 12 pazienti , hanno dimostrato la sicurezza e lefficacia della rf per la riduzione del dolore , il miglioramento della qualit della vita e la riduzione delluso di analgesici nei pazienti con metastasi che coinvolgevano losso . 
 [ 29 ] che ha considerato 43 pazienti , stato segnalato un incremento della dose di oppiodi al primo giorno dal trattamento e un successivo decremento di pi del 50% . sulla base di unattenta selezione dei pazienti , nella nostra casistica non si sono verificate complicanze probabilmente anche per lesiguo numero di pazienti ( 6 ) trattati con rf . 
 [ 29 ] si sono invece verificate complicanze maggiori in 3 pazienti : uno ha subito unustione di secondo grado nellarea cutanea della messa a terra , un altro ha accusato incontinenza vescicale e intestinale e infine in un paziente si verificata una frattura acetabolare della zona trattata a 6 settimane dal trattamento con rf . 
gli studi effettuati con la coblazione su lesioni ossee [ 25 ] hanno preso in esame solo il trattamento di lesioni vertebrali ( per le quali per altro non sono riportate complicanze ) e quindi non possibile fare un confronto dato che nel nostro studio la metodica stata utilizzata in una lesione costale . 
 [ 9 ] hanno redatto i primi studi sperimentali e clinici sullutilizzo della termoablazione con microonde nelle metastasi ossee , riportando un ottimo risultato tecnico sia in termini di volume di necrosi , sia di rapidit della procedura , sia di assenza complicanze . 
 [ 29 ] , possibile che vi sia , a distanza dalla procedura , un nuovo aumento della dose di morfina , compatibile con linsorgenza di nuove localizzazioni ossee in siti diversi da quello trattato . 
 [ 6 ] , pazienti sottoposti a rfa associata a cementoplastica per voluminose metastasi ossee coinvolgenti anche la regione extra - ossea hanno ottenuto una riduzione della dose di analgesici solo nel 41% dei casi ; le voluminose dimensioni delle lesioni trattate giustificano il divario tra questo risultato e quello ottenuto dallo studio di callstrom et al . 
 [ 28 ] ( trattamento solo con rf )  . nel nostro studio sono state trattate con cementoplastica le lesioni che , in relazione alla sede , necessitavano di una stabilizzazione . 
in all cases , in agreement with the literature , the results achieved were excellent , not only as concerns stabilisation and thus prevention of pathological fractures , but also as concerns pain relief , achieved in 100% of cases . 
 [ 6 ] emphasised that the technique is easy to perform , inexpensive and minimally invasive , even though the effects of combining rf ablation and cementoplasty with radiotherapy are not well known . 
 [ 34 ] believe that the coagulation necrosis induced by rf facilitates even cement distribution within the ablated lesion and that cementoplasty enhances the analgesic effect by stabilising the bone . 
 the results obtained have been excellent , with pain relief being achieved in 100% of cases , both in case reports [ 30 , 31 , 34 ] and in larger series [ 6 , 28 , 32 , 33 ] , as well as in our small patient series . 
it should be emphasised that , whereas studies performed with rf or cementoplasty alone achieved 100% technical success and 80%100% pain relief [ 35 , 36 ] , combined rf and cementoplasty ensured pain relief in all cases but a slightly lower rate of technical success . conclusions there is no agreement as to the best treatment for bone metastases . 
it is clear that the rationale for the use of these treatments is that , when indicated , they ensure considerably faster pain relief compared with conventional treatments , providing a substantial improvement in quality of life in a short time . 
however , further investigations on larger patient populations , as well as randomised controlled studies , are required to validate the effectiveness of these treatments . con cementoplastica dopo rfa e 2 con vertebroplastica dopo radiofrequenza plasma - mediata . 
in tutti i casi , in accordo con i dati della letteratura , sono stati ottenuti ottimi risultati non solo nellambito della stabilizzazione e quindi nella prevenzione della possibile frattura patologica , ma soprattutto in quello della riduzione della sintomatologia dolorosa , che si avuta nel 100% dei casi . 
 [ 34 ] ritengono che la necrosi coagulativa indotta dalla rf faciliti lomogenea distribuzione del cemento allinterno della lesione ablata e che la cementoplastica , per effetto della stabilizzazione ossea , migliori leffetto antalgico . 
 i risultati ottenuti sono stati ottimi , sia nei case report [ 30 , 31 , 34 ] che nelle casistiche [ 6 , 28 , 32 , 33 ] dove la riduzione del dolore si verificata nel 100% dei casi analogamente a quanto emerso nellesperienza personale , peraltro numericamente esigua . 
va sottolineato che , se da un lato negli studi effettuati solo con radiofrequenza o solo con cementoplastica si ottenuto un successo tecnico del 100% a fronte di un risultato in termini di riduzione del dolore compreso tra l80% e il 100% [ 35 , 36 ] , dallaltro la tecnica combinata di radiofrequenza e cementoplastica ha assicurato la riduzione del dolore in tutti i casi trattati , ma un successo tecnico in una percentuale leggermente inferiore . conclusioni attualmente non esistono ancora pareri concordi sulla metodica migliore nel trattamento delle metastasi ossee . 
appare evidente che ci che giustifica il ricorso a queste terapie il fatto che , laddove vi sia lindicazione , esse garantiscono una riduzione della sintomatologia dolorosa notevolmente pi rapida rispetto alle terapie convenzionali apportando , in breve tempo , un sensibile miglioramento della qualit della vita . 
volta 171 , 50133 firenze , italy 2dipartimento di fisica e tecnologie relative , universit di palermo , palermo , italy 3istituto di radiologia , policlinico , palermo , italy 4medicad s.r.l. , palermo , italy correspondence to : s . 
il set contiene 31 mammografie di screening refertate come negative , precedenti la comparsa di carcinomi di intervallo classificati alla revisione come errori di screening o minimal sign , e 89 controlli negativi verificati , scelti a random dalla stessa casistica di screening . 
rispetto ai due sistemi cad a confronto cyclopus risulta pi sensibile ( r2 p = 0 , 14 ; cadx p = 0 , 02 ) , e meno specifico ( r2 p = 0 , 02 ; cadx p = 0 , 64 )  . parole chiave carcinoma mammario diagnosi computer assistita mammografia introduction introduzione false negatives on mammography screening may be due to misperception of radiological abnormalities , and perception could be possibly improved by computer analysis of digitised images identifying mammography sites for review . computer - assisted diagnosis ( cad ) could be particularly useful in screening where the mammograms to be read are many and the abnormalities to be perceived are few , thus easily causing loss of attention or fatigue . 
cad has been the object of several studies demonstrating that it allows a moderate increase in specificity associated with an accettable decrease in specificity [ 17 ]  . different cad systems have been developed , but few have been tested in comparison . 
no doubt , radiologists are mostly interested in the impact of cad on final diagnosis , and studies of cad efficacy are mainly based on comparison of a single reading with or without cad . 
nevertheless the impact of cad depends on its absolute accuracy , that is , the power of marking cancer areas while keeping the rate of marked benign areas as low as possible . 
the aim of this study was to assess the systems diagnostic accuracy by testing it on a training set and to compare its performance with that of two other commercial systems , namely , cadx ( former cadx , now commercialised by icad , inc . , nashua , nh , usa ) and r2 ( r2 technology , inc . , santa clara , ca , usa ) already tested on the same set [ 8 ]  . materials and methods cyclopus was tested on a mammography set developed at i falsi negativi dello screening mammografico possono essere dovuti alla mancata percezione di anormalit radiologiche e la percezione potrebbe essere migliorata con lanalisi computerizzata di immagini mammografiche digitali o digitalizzate , capaci di selezionare aree meritevoli di revisione . 
la diagnosi aiutata dallanalisi computerizzata ( cad ) stata oggetto di numerosi studi che dimostrano come il cad consenta un moderato aumento della sensibilit a fronte di unaccettabile riduzione della specificit [ 17 ]  . 
luso del cad , pertanto , potrebbe essere particolarmente utile nello screening , dove il numero di mammografie da interpretare molto elevato , le anormalit da percepire sono poche e la caduta di attenzione o laffaticamento del lettore pi facile . diversi sistemi cad sono stati sviluppati , ma pochi sono stati testati a confronto . 
indubbiamente quello che interessa al radiologo leffetto di cad sulla diagnosi finale , e per questo gli studi dellefficacia di cad in genere si basano su un confronto tra la lettura singola e quella aiutata da cad . 
peraltro limpatto di cad sulla diagnosi finale dipende dalla sua accuratezza assoluta , dalla capacit cio di segnalare alterazioni mammografiche dovute a cancro e di mantenere al minimo la segnalazione di alterazioni che poi si rivelano non neoplastiche . 
scopo del presente studio stato quello di testare laccuratezza diagnostica di cyclopus applicandolo a una casistica campione , e di confrontare la sua prestazione con due altri sistemi commerciali : cadx ( ora commercializzato da icad , inc . , nashua , nh , usa ) e r2 ( r2 technology , inc . , santa clara , ca , usa ) , gi testati sulla stessa casistica [ 8 ]  . 628 radiol med ( 2009 ) 114 : 626635 the scientific institute for cancer prevention ( ispo ) and used in the past to evaluate the accuracy of other cad systems [ 8 ]  . 
the set consists of 120 one - view ( mediolateral oblique , n = 82 ) or two - view ( mediolateral oblique + craniocaudal , n = 38 ) conventional mammograms and includes previous screening mammograms ( originally reported as negative ) preceding 31 interval cancers ( ic ) and 89 negative controls ( randomly selected from the same screening database and assumed to be negative on the basis of at least one further negative biennial screen )  . 
ic are periodically identified by linkage of florence screening programme archives with the tuscany cancer registry [ 9 ] and are routinely classified by expert radiologists according to the european guidelines [ 10 ] , namely , occult , minimal sign ( ms ) and screening error ( se )  . 
the 31 ic in the set account for all consecutive ic observed in a 5 - year period in the florence screening programme after excluding occult cases : 20 had been classified as ms and 11 as se . all films in the set were digitised at medicad in a blind fashion ( operators were not aware of which cases were ic or controls ) by means of a ccd digitiser operating at 80 m per pixel , 12 - bit greyscale . 
the general architecture of cyclopus includes several steps : pre - processing : the digital image is processed to delimit the mammographic area to be submitted to further analysis segmentation : the cleaned image is segmented to select regions of interest ( roi ) mapping out its contour features extraction : characteristic information extracted from each roi classification : a probability of pathology is assigned to each roi . in cyclopus , in particular , image segmentation is based on the region - growing method in a process of multilevel analysis . 
the region - growing method consists of determining a set of points or initial regions ( seeds ) , which are expanded by incorporating the neighbouring pixels having met a test of similarity with the region . 
for the classification step , artificial neural networks ( ann ) are used , organised on an architecture of neurons and connections . the number of input neurons corresponds to the number of features extracted . 
the ann operation involves a learning materiali e metodi cyclopus stato testato su un set di mammografie sviluppato allistituto scientifico per la prevenzione oncologica ( ispo ) di firenze e in precedenza usato nella valutazione di accuratezza di altri due sistemi cad . 
il set utilizzato per testare il sistema consta di 120 mammografie convenzionali in proiezione singola ( mediolaterale obliqua n = 82 ) o doppia ( mediolaterale obliqua + craniocaudale n = 38 ) , e comprende le mammografie refertate come negative precedenti a 31 casi di carcinoma di intervallo ( ci ) e 89 controlli negativi ( tratti in maniera random dalla stessa casistica di screening , e verificati tali in base ad almeno un controllo successivo biennale negativo )  . 
i 31 casi di ci nel set in studio costituiscono una casistica consecutiva relativa circa 5 anni di attivit del programma di screening di firenze , dopo esclusione dei i casi occulti : 20 erano stati classificati come sm e 11 come es . 
 tutte le mammografie del set sono state digitalizzate da medicad con metodica cieca ( gli operatori non erano al corrente di quali casi fossero ci o controlli ) mediante un digitalizzatore a ccd operante a 80 micron per pixel , 12 bit di scala di grigi . 
il metodo utilizzato da cyclopus comprende varie fasi : pre - processing : inizialmente limmagine viene preprocessata al fine di delimitare la mammella ; segmentazione : la zona delimitata in precedenza viene scomposta in sub - regioni otticamente omogenee e fra queste vengono selezionate quelle interessanti , potenziali sedi di lesioni , region of interest ( roi ) ; estrazione di caratteristiche : ad ogni roi vengono associate alcune grandezze analitiche , che ne descrivono le propriet ; classificazione : ogni roi viene classificata in base al grado di similitudine con patologie tumorali analoghe accertate . in particolare , in cyclopus , la segmentazione delle immagini basata sul metodo di region growing allinterno di un processo di analisi di tipo multi - livello . tale metodo consiste nel determinare un set di punti o regioni iniziali ( seeds ) i quali sono poi espansi incorporando in essi i pixel confinanti che soddisfano ad un test di similarit con la regione . 
per la classificazione delle roi sono utilizzate reti neurali radiol med ( 2009 ) 114 : 626635 phase consisting of iterative training in order to establish the connection parameters between neurons . the system allows a choice among four different working presets ( as to sensitivity / specificity ) , namely , very high sensitivity , high sensitivity , high specificity , and very high specificity . 
on that basis , we assessed the absolute accuracy ( sensitivity , specificity , positive predictive value , number of markings per view among negative controls ) of cyclopus . comparison of performance with the two other commercial systems was performed on the basis of data published in a previous report [ 8 ]  . 
statistical significance of observed differences was calculated with the mcnemar test for paired data and set at p < 0.05. results table 1 shows the results of the case - based diagnostic accuracy of cyclopus . 
data are summarised in table 2 . table 3 shows the diagnostic performance of cyclopus compared with cadx and r2 , as determined in 2004 on the same test set [ 8 ]  . 
il funzionamento di tali reti presuppone una fase di apprendimento , costituita da un addestramento iterativo per la determinazione dei parametri interni di connessione fra i neuroni . il sistema permette di scegliere il punto di lavoro ( in termini di sensibilit / specificit ) tra i quattro possibili : sensibilit molto elevata , sensibilit elevata , specificit elevata , specificit molto elevata , identificati utilizzando un database di propriet della medicad . 
nel presente articolo vengono riportati in dettaglio i risultati ottenuti con il punto sensibilit elevata che risultato quello maggiormente proponibile per luso clinico ; i risultati ottenibili con gli altri punti di lavoro sono riportati in modo riassuntivo . le immagini digitalizzate sono state processate mediante computer , usando applicazioni iterative di cyclopus , al fine di identificare aree di interesse meritevoli di una revisione . i risultati dellanalisi del sistema , in termini di mammografie con marcatura delle roi , sono stati riportati su carta ( calcificazioni e opacit di massa sono contrassegnate con simboli diversi )  . 
 le stampe sono state confrontate con le mammografie originali da uno di noi ( sc ) , per definire quali roi corrispondessero a ci ( veri positivi ) o a aree di benignit ( falsi positivi )  . 
su tale base abbiamo definito laccuratezza diagnostica assoluta di cyclopus ( sensibilit , specificit , valore predittivo positivo , numero di roi per proiezione tra i controlli negativi )  . 
la significativit statistica ( posta a p < 0 , 05 ) delle differenze osservate tra i diversi sistemi a confronto stata calcolata in base al test di mcnemar per dati appaiati . risultati la tabella 1 mostra i risultati di accuratezza diagnostica di cyclopus , basata sui casi , non sulle singole proiezioni . 
la sensibilit stata del 74 , 2% , ed risultata pi elevata per i ci classificati come es ( 90 , 9% ) che per quelli classificati come sm ( 65 , 0% )  . 
i dati sono riassunti nella tabella 2 . la tabella 3 mostra le prestazioni diagnostiche di cyclopus rispetto a r2 e cadx , le prestazioni di questi due 630 radiol med ( 2009 ) 114 : 626635 microcalcifications ( 90 markings for masses , 213 for microcalcifications )  . 
cyclopus had a higher overall sensitivity compared with r2 ( p = 0.14 ) or cadx ( p = 0.02 ) , although the difference with r2 was not significant owing to the limited sample size . 
cyclopus mostra una maggiore sensibilit per le opacit di massa rispetto alle calcificazioni ( 208 roi rispetto a 62 , tra i controlli negativi ) , in maniera pi marcata di cadx ( 192 vs 130 ) , mentre r2 privilegia lidentificazione delle microcalcificazioni ( 90 roi per masse , 213 per calcificazioni )  . 
cyclopus mostra una sensibilit globale superiore a r2 ( p = 0 , 14 ) o cadx ( p = 0 , 02 ) , anche se la differenza con r2 non statisticamente significativa per il limitato campione in esame . 
sample size is no doubt limited compared with screening practice , the prevalence of cancers being substantially higher ( 20% ) compared with the average frequency of ic ( 0.8 [ 10 ] )  . 
such a condition is likely to influence the reader to adopt a lower threshold for suspicion ( aimed at maximising sensitivity ) and is a common bias of studies investigating the impact of cad but is necessary to obtain a set size compatible with a feasible review process . moreover , this study tested the algorithm , which cannot be emotionally influenced by the prevalence of positive cases in the set . 
this applies particularly to controls and to differences in specificity , which nevertheless should not be of major concern , as by definition , cad has a very low specificity that requires the reader to apply a major discount filter to an roi excess . the number of ic in the study set may be apparently low , but this is due to the rarity of ic . 
this study considers all ic reviewed as se or ms observed in a 5 - year period in a screening unit with a workload of 30 , 000 tests per year , among the largest in italy and europe , and thus represents a large realistic sample . 
the proportion of ic reviewed as se or ms is not artificial but real , as this is a consecutive sample , although these values are far from being universal given that attribution to se or ms categories is to some extent subjective [ 12 ]  . 
the choice of excluding ic reviewed as occult from the set was adopted , as the reader is expected to discount the large majority of rois , and this is much more likely to occur with cases that have been reviewed as having no radiological abnormalities . 
cad is unlikely to improve cancer detection rate of ic reviewed as occult . studies of cad impact on conventional reading show an incremental detection rate ranging between 1% and 19 % and a corresponding incremental recall rate ranging between 6% and 35% [ 1222 ]  . 
one particular advantage of cad would be to adopt it as an alternative to double reading , which is recommended by the european guidelines [ 10 ] and causes major radiol med ( 2009 ) 114 : 626635 cyclopus ( 1 , 13 ) , rispetto a r2 ( 0 , 93 ) o cadx ( 0 , 99 )  . la tabella 4 riporta i risultati ottenibili con cyclopus operando con i quattro diversi punti di lavoro . 
la conseguente variazione della sensibilit ( da 45 , 2% a 84 , 9% , p = 0 , 007 ) e delle roi per proiezione ( da 0 , 24 a 1 , 37 , p = 106 ) decisamente importante e significativo . 
le dimensioni del campione in esame sono certamente esigue rispetto alla pratica di screening , con una concentrazione di carcinomi decisamente pi elevata ( 20% ) di quella mediamente riscontrata per i ci ( 0 , 8 [ 10 ] )  . 
tale condizione , che pu certamente influenzare il lettore verso una minore soglia di sospetto ( per aumentare la sensibilit ) , comune alla gran parte degli studi che valutano limpatto di cad sulla lettura umana , per lovvia necessit di mantenere le dimensioni del set entro un margine che renda la valutazione fattibile : peraltro in questo caso ad essere testato il computer , che certamente non influenzato emotivamente dalla frequenza di casi positivi . 
 altres vero che la limitatezza di casi e controlli ha comportato una minore potenza dello studio , che certamente non capace di dimostrare la significativit statistica per differente di modesta entit . 
questo vale soprattutto per la numerosit dei controlli , e quindi per le differenze in specificit , che peraltro non dovrebbero troppo preoccupare dal momento che cad , per definizione , ha una specificit molto modesta , che comunque necessita di un filtro importante da parte del lettore . 
la numerosit dei ci in esame pu sembrare esigua , ma legata alla rarit intrinseca dei ci : in questo caso i ci nel set sono quelli rivalutati come es o sm corrispondenti a circa 5 anni di attivit di una unit di screening di 30000 test annui , tra le pi grandi in italia e in europa , e quindi costituiscono certamente un campione realistico . 
la composizione in es e sm della casistica non artificiale ma reale , in quanto si tratta di un campione di ci consecutivo , anche se non ha un valore universale considerando la soggettivit del revisore nellattribuire queste categorie [ 12 ]  . 
la scelta di escludere dal campione i ci classificati come occulti alla revisione deriva del fatto che , poich nelluso clinico il lettore deve trascurare la gran parte delle roi , molto verosimile che questo avvenga per le regioni che alla revisione sono risultate completamente negative , e che quindi cad non possa aumentare il tasso diagnostico attraverso la identificazione di ci rivalutati come occulti . gli studi sullimpatto di cad in ausilio alla lettura convenzionale mostrano un aumento del tasso diagnostico di carcinoma che varia dal 1% al 19% [ 1222 ] e al radiol med ( 2009 ) 114 : 626635 difficulties due to the lack of trained radiologists , although the existing evidence is not fully encouraging [ 2 ]  . 
such a comparison is not possible on the basis of existing studies of single cad systems because the mammography sets on which algorithms are tested are different in structure and difficulty , thus influencing performance . 
several retrospective studies are biased as cad is tested on screen - detected cancers ( that is , detected without the need for cad ) rather than on ic ( the detection of which is the real goal of cad )  . 
overall , a reliable comparison of different cad systems is still to be done , as very few studies have performed a proper comparison of algorithms on the same training set [ 8 ]  . cad impact on reading diagnostic accuracy is strictly dependent on the absolute accuracy of the systedifferent algorithms could be simply tested on the same training set , comparing them for sensitivity and specificity , independently from the impact of cad marking on the radiologists interpretation . 
a training set made up of negative controls seeded with ic cases , as in this study , is ideal for the purpose . this study evaluates the absolute diagnostic accuracy of cyclopus , a new algorithm , and compares it with two other cad commercial systems , which had been tested on the same training set . 
no doubt , the training set is imperfect , as it is based on screen - film mammograms ( and the future use of cad is likely to be mostly with digital mammography ) and includes a large proportion of singleview mammograms ( single view is suppose to reduce cad performance compared with double view )  . 
however , because the same training set was used to test the three algorithms , its imperfection should equally affect their performance . cyclopus proved to be more sensitive for masses compared with microcalcifications , as was cadx , and this is supposed to be an advantage , at least in theory , as ic are known to be mostly depicted as masses [ 23 ]  . 
setting the high sensitivity working point , cyclopus was substantially more sensitive compared with the two other systems . contempo un aumento del tasso di richiamo che varia dal 6% al 35% [ 1222 ]  . 
un particolare vantaggio offerta dal cad sarebbe quello di impiegarlo in alternativa alla doppia lettura , raccomandata dalle linee guida ue [ 10 ] e fonte di problemi organizzativi per la carenza di radiologi esperti , anche se levidenza finora esistente non del tutto incoraggiante [ 2 ]  . 
certamente la diffusione della mammografia digitale faciliter limpiego del cad , per la possibilit di visionare le marcature cad direttamente sul monitor , decisamente competitiva rispetto alla complessit dellanalisi cad di immagini analogiche . ipotizzando una sempre maggiore diffusione del cad , verosimile che gli acquirenti si interessino , oltre che ai costi , a un confronto tra le performance dei diversi sistemi in commercio . 
il confronto tra diversi algoritmi non pu essere fatto in base ai numerosi studi che impiegano i singoli sistemi cad , perch le casistiche di riferimento , dalla cui composizione e difficolt dipendono le prestazioni del cad , non sono confrontabili . 
molti studi retrospettivi risultano problematici per il fatto che il cad viene testato su carcinomi diagnosticati dallo screening ( per i quali non serviva laiuto di cad ) invece che su carcinomi di intervallo ( che il cad dovrebbe contribuire a ridurre )  . gli studi prospettici di lettura assistita dal cad , impiegando diversi algoritmi , sono pi complessi da realizzare e richiedono tempo per dare risultati validi . 
in sostanza il confronto tra algoritmi sostanzialmente ancora da fare , in quanto sono molto pochi gli studi che confrontano diversi algoritmi sulla stessa casistica campione [ 8 ]  . poich limpatto del cad sullaccuratezza diagnostica deriva in prima istanza dallaccuratezza diagnostica assoluta del sistema , il confronto tra algoritmi potrebbe limitarsi alla analisi di una stessa casistica campione con diversi algoritmi , confrontando la sensibilit e la specificit di questi ultimi a prescindere dallimpatto che le marcature cad possano avere sulla lettura . 
una casistica costruita insemenzando casi normali con carcinomi di intervallo , come in questo studio , costituisce il supporto ideale per tale confronto . il presente studio valuta la performance diagnostica di cyclopus , un nuovo cad commerciale , e la confronta con altri due sistemi commerciali , che in passato erano stati testati sulla stessa casistica . 
indubbiamente la casistica non quella ideale , sia perch analogica ( e luso del cad sar in futuro prevalentemente su sistemi di mammografia digitale ) , sia perch costituita in parte da esami con proiezione singola , che , come noto , pu in qualche modo ridurre la performance del cad . 
il fatto peraltro che la casistica sia la stessa per i tre sistemi suggerisce che i suoi eventuali limiti influenzino in modo paritetico la performance dei sistemi a confronto . cyclopus risulta maggiormente sensibile per la presenza di anomalie caratterizzate da opacit di massa che non da calcificazioni , in analogia a cadx , e questo teoricamente un vantaggio perch noto che la stragrande maggioranza dei ci si associa a opacit di massa e non a calcificazioni 634 radiol med ( 2009 ) 114 : 626635 cyclopus was less specific than the two other systems , as shown by the higher false positive rate and the higher average number of markings per view . 
overall , the balance may look acceptable : the additional cancers marked by cyclopus compared with cadx or r2 were six and ten , and the additional false positive control cases were 12 and two , respectively . 
the aim of our study , however , was to provide a first evaluation of cyclopus , and a comparison with two commercial systems seemed to us appropriate , also considering the difficulty in comparing different cad algorithms ( comparison studies are anecdotal in the literature )  . 
a higher sensitivity ( absolute value ) observed for cyclopus compared with the other two systems is promising , but because of its marginal statistical significance , confirmation by studies with greater power is needed . 
il bilancio pu apparire conveniente : il numero di carcinomi aggiuntivi identificati da cyclopus rispetto a cadx o r2 rispettivamente di 6 e di 10 a fronte di un numero aggiuntivo di controlli falsi positivi rispettivamente di 12 e 2 . 
il tentativo di aumentare la specificit di cyclopus adottando il livello di lavoro specificit elevata consente un notevole miglioramento delle roi per proiezione ( 0 , 48 ) , decisamente migliore di quanto ottenuto con gli altri due sistemi ( r2 = 0 , 93 ; cadx = 0 , 99 ) , ma con una notevole perdita in sensibilit ( 58 , 1% vs 74 , 1% ) , che non riteniamo clinicamente accettabile , anche se la sensibilit risultante paragonabile a quelle degli altri sistemi a confronto ( r2 = 54 , 8% ; cadx = 41 , 9% )  . il campione in esame ha certamente limiti di potenza , ma era in qualche modo obbligato dalla sua disponibilit relativa a uno studio precedente [ 8 ] , effettivamente non disegnato per un puro confronto tra algoritmi , ma per un confronto delleffetto di cad sulla lettura umana . 
scopo dello studio , peraltro , era una prima valutazione del sistema cyclopus , e un confronto con dati gi esistenti per due algoritmi di commercio ci parso opportuno , data la difficolt di poter testare tra loro diversi sistemi ( gli studi tra sistemi sono aneddotici in letteratura )  . 
il confronto tra algoritmi cad dovrebbe avvenire soprattutto in base alla sensibilit , dato che la specificit attesa per definizione molto bassa , e luso clinico di cad prevede che il lettore operi comunque un grossolano sconto sulle roi . 
la maggiore sensibilit ( stima puntuale ) osservata per cyclopus promettente ma con significativit statistica marginale e necessita di conferme con studi di maggiore potenza . auspicabile che altri studi come questo siano condotti in futuro , e che i loro risultati costituiscano una valida base per un giudizio comparativo tra i diversi algoritmi , attualmente pressoch impossibile . conflict of interest statement : gli autori donato cascio , francesco fauci , rosario magro , giuseppe raso e raffaele ienzi sono consulenti tecnico - scientifici e soci della medicad s.r.l. 
twenty - four consecutive patients ( 16 women , eight men ; mean age , 56.5 years ) with a diagnosis of fuo based on routine investigations were retrospectively studied . 
a nal diagnosis was reached in 17 of 24 patients ( vasculitis , n = 5 ; autoimmune disorder , n = 2 ; neoplasm , n = 3 ; infectious disease , n = 6 ; biliary microlithiasis , n = 1 )  . 
if prospective trials on this topic con rm the present ndings , pet / ct should be incorporated in the routine diagnostic work - up of patients with classical fuo . keywords fever of unknown origin pet / ct clinical management diagnosis riassunto obiettivo . 
abbiamo incluso , retrospettivamente , ventiquattro pazienti consecutivi ( 16 femmine e 8 maschi ) di et media 56 , 5 anni , nei quali , dopo gli esami di routine , era stata posta diagnosi di fuo classica . 
in 17 pazienti si raggiunta una diagnosi nale : vasculite ( 5 ) , malattia auto - immune ( 2 ) , neoplasia ( 3 ) , malattia infettiva ( 6 ) , micro - litiasi biliare ( 1 )  . 
se ulteriori studi prospettici su questo argomento confermeranno gli attuali risultati , lesame pet / tc dovrebbe essere incluso nella routine diagnostica di questi pazienti . parole chiave febbre di origine sconosciuta pet / tc gestione clinica diagnosi 810 introduction fever of unknown origin ( fuo ) constitutes a diagnostic challenge owing to both the wide range of possible causes and the frequently inconclusive or misleading ndings of clinical investigations . 
in 1961 , petersdorf and beeson de ned fuo as a fever lasting > 3 weeks with a temperature > 38.3c , measured on several occasions and with no diagnosis after 1 week of inpatient investigation [ 1 ]  . 
nearly 30 years later , in 1992 , petersdorf modi ed the latter criterion into a failure to reach a diagnosis after appropriate examinations in outor inpatients [ 2 ]  . 
in the 1990s , a new four - tiered fuo classi cation was proposed [ 3 ] : ( 1 ) classical fuo ( fuo in nonimmunocompromised patients ) ; ( 2 ) nosocomial fuo ; ( 3 ) fuo in neutropenic patients ; ( 4 ) hiv - associated fuo . causes of classical fuo can be grouped into four major subcategories : infections ; malignancies ; autoimmune noninfectious diseases and miscellaneous [ 4 ]  . 
the healthcare costs related to fuo are very high as a result of the prevalence of the condition and the extent of resources used for its management ( especially in the diagnostic phase )  . 
in addition , 1235% of these patients die of fuo - related problems [ 5 ] , whereas the prognosis is often positive when the cause of the fever is not established after clinical and imaging investigations . 
it is therefore essential to distinguish between patients in whom aggressive treatment is mandatory and patients in whom a wait - and - see approach is more appropriate [ 6 ]  . 
 combined positron emission tomography and computed tomography with [ 18f ] uorodeoxyglucose ( [ 18f ] - fdgpet / ct ) is a noninvasive diagnostic procedure widely used in managing patients with cancer . 
furthermore , glucose and [ 18f ] - fdg are trapped by white blood cells , especially neutrophils and monocytes / macrophages , in response to in ammatory stimuli , as shown by in vitro and in vivo studies [ 7 , 8 ]  . 
several authors have reported the ability of pet to localise periodontal , abdominal or pelvic abscesses , vascular in ammations , tuberculosis and infection of bone , joint , soft tissue and prostheses [ 9 , 10 ]  . 
therefore , [ 18f ] - fdg - pet may represent a highly useful examination not only for identifying the causes of classical fuo radiol med ( 2011 ) 116 : 809820 introduzione la febbre di origine sconosciuta ( fuo ) rappresenta una vera e propria s da in ambito diagnostico sia per lelevato numero dei possibili fattori eziologici coinvolti , sia per i risultati spesso inconcludenti o fuorvianti ottenuti dagli esami clinici eseguiti . 
nel 1961 , petersdorf e beeson de nirono la fuo come febbre di durata maggiore di tre settimane con temperatura superiore ai 38 , 3c misurata in occasioni differenti e senza una diagnosi eziologica dopo una settimana di indagini eseguite in regime di ricovero [ 1 ]  . 
circa 30 anni dopo , nel 1992 , sempre petersdorf ha modi cato lultimo criterio di questa de nizione con : mancata diagnosi dopo appropriati esami in regime di ricovero o ambulatoriale [ 2 ]  . 
negli anni 90 , stata proposta per la fuo una classi cazione su base eziologica con identi cazione di quattro gruppi [ 3 ] : ( 1 ) fuo classica ( fuo in pazienti immunocompetenti ) ; ( 2 ) fuo nosocomiale ; ( 3 ) fuo in pazienti neutropenici ; e ( 4 ) fuo associata ad virus dellimmunodecienza umana ( hiv )  . a loro volta , le cause della fuo classica si possono raggruppare in quattro sottogruppi maggiori : infezioni , neoplasie , malattie autoimmuni e miscellanea [ 4 ]  . 
i costi sanitari legati alla fuo risultano estremamente elevati in considerazione della sua prevalenza e dellentit di risorse impiegate per la sua gestione ( soprattutto nella fase diagnostica )  . 
inoltre , dal 12% al 35% di questi pazienti muoiono per problemi ad essa correlati [ 5 ] , mentre spesso la prognosi risulta positiva se leziologia della fuo non viene identi cata dopo gli esami clinicostrumentali . 
di conseguenza , durante la fase diagnostica risulterebbe estremamente utile poter distinguere i pazienti che necessitano di un trattamento aggressivo da quelli nei quali un approccio wait and see pi appropriato [ 6 ]  . 
 lesame integrato tomogra a ad emissione di positroni / tomogra a computerizzata ( pet / tc ) con ( 18f ) uorodeossiglucosio [ ( 18f ) fdg ] un esame diagnostico non invasivo utilizzato ampiamente nei pazienti oncologici . 
peraltro , glucosio e il ( 18f ) fdg sono utilizzati / intrappolati anche dai leucociti , specialmenradiol med ( 2011 ) 116 : 809820 but also for monitoring treatment response . 
this study was therefore undertaken to compare our results with those reported in the literature , which was extensively analysed and discussed , with a view to de ning the utility of pet / ct in patients with classical fuo . 
fuo was de ned as fever ( > 38c ) for more than 3 weeks without a nal diagnosis after chest x - ray or ct scan , abdominal ultrasonography ( us ) or ct , routine blood chemistry , urinalysis and in - depth examination of any abnormalities detected . 
 pet / ct study pet / ct studies were acquired using the same combined pet / ct scanner ( discovery st , general electric medical system , waukesha , wi , usa )  . 
 the acquisition protocol started with a scout view ( a bidimensional ct projection ) that was used to de ne the body axial extension ( beginning and end position ) over which ct and pet data would be acquired . 
once the scan range was de ned , ct was performed ( voltage , 140 kv ; tube current , 60 mas ) from the proximal femur to the base of the skull . 
pet data on tracer distribute i neutro li e i monociti / macrofagi , quando questi vengono attivati da stimoli ogistici , come stato dimostrato da studi in vitro ed in vivo [ 7 , 8 ]  . 
diversi autori hanno mostrato la capacit dellesame pet di localizzare ascessi periodontali , addominali o pelvici , in ammazioni vascolari , lesioni tubercolari nonch infezioni di protesi , tessuti molli , ossa ed articolazioni [ 9 , 10 ]  . 
queste considerazioni suggeriscono che lesame pet con ( 18f ) fdg possa rappresentare uno strumento estremamente adatto per identi care e chiarire le cause eziologiche della fuo classica ; inoltre lo stesso esame potrebbe essere utilizzato anche per monitorare la risposta al trattamento . 
in questi ultimi anni , il ruolo dellesame pet nei pazienti con fuo classica stato largamente indagato ; tuttavia le conclusioni dei lavori pubblicati non sempre sono concordanti ed dif cile avere un quadro chiaro [ 1114 ]  . 
per questo motivo lo scopo del nostro studio stato prima di tutto di confrontare i nostri dati con quelli riportati in letteratura ( che stata ampiamente analizzata e discussa ) , dopo di che cercare di de nire il ruolo della pet / ct nei pazienti con fuo classica . materiali e metodi selezione dei pazienti in questo studio retrospettivo abbiamo incluso 24 pazienti consecutivi ( 16 femmine e 8 maschi ; et media 56 , 5 anni , deviazione standard 19 , 1 anni ) inviati al nostro centro pet con diagnosi di fuo classica tra marzo 2007 e luglio 2009 ( tabella 1 )  . 
la de nizione di fuo presa in considerazione prevede febbre ( > 38c ) per pi di tre settimane senza una diagnosi nale dopo radiogra a o tc del torace , ecogra a o tc addominale , emocromo , esame delle urine , ed approfondimento delle anomalie riscontrate . 
il follow - up stato realizzato per tutti i pazienti contattando i medici curanti ed stato ottenuto per tutti ; il periodo minimo di follow - up stato di 6 mesi . esame pet / tc lo studio pet stato acquisito con un tomografo pet / tc discovery st ( general electric medical system , waukesha , wisconsin , usa )  . 
i dati emissivi della pet sono stati acquisiti 60 812 table 1 patient characteristics radiol med ( 2011 ) 116 : 809820 sex diagnosis final diagnosis [ 18f ] - fdg - pet / ct pt . 
pet was considered true positive if the nal diagnosis was consistent with the pet ndings and false positive if the pet ndings were not con rmed as the cause of fuo on further investigations . 
a nal diagnosis was reached in 17 cases ( vasculitis , n = 5 ; autoimmune disorder , n = 2 ; neoplasm , n = 3 ; infectious disease , n = 6 ; biliary microlithiasis , n = 1 )  . 
in four cases with [ 18f ] - fdg uptake in lymph node stations and / or the oropharyngeal region , pet scan was interpreted as suggestive of infection and , after further clinical studies , the patients were treated with antimycotics ( n = 1 ) or antibiotics ( n = 3 ) ; all underwent fuo remission after treatment . 
in two patients , an autoimmune disease was diagnosed ; in one patient , the nal diagnosis was haemophagocytosis ( and the fever persisted after 1 year of follow - up )  . 
one patient had biliary microlithiasis that was held responsible for fuo ( in this patient , focal uptake of [ 18f ] - fdg was seen around the biliary prosthesis , but it was considered reactive to the prosthesis itself )  . 
il protocollo di acquisizione inizia con una scout view ( proiezione tc bidimensionale del paziente ) , utilizzata per de nire lestensione assiale del corpo ( posizione di inizio e ne ) sulla quale acquisire i dati tc e pet . 
una volta de nito lintervallo di scansione viene acquisito lesame tc , dalla base cranica alla porzione prossimale del femore ( voltaggio di 140 kv e intensit di corrente di 60 mas )  . 
i dati emissivi della distribuzione del tracciante sono stati acquisiti in modalit 3d ( 89 eld of view [ fov ] di 3 , 5 minuti ciascuno ) , dalla porzione prossimale del femore alla base cranica . 
lesame pet stato considerato : vero positivo se la diagnosi nale era in accordo con lesito pet ; falso positivo se il reperto identi cato come patologico dalla pet non stato confermato come causa della fuo nelle indagini diagnostiche successive . 
2 [ 18f ] uorodeoxyglucose positron emission tomography computed tomography ( [ 18f ] - fdg - pet / ct ) maximum intensity projection ( mip ) of a 31 - year - old women referred for fever of unknown origin ( fuo )  . 
 la febbre scomparsa dopo lintervento chirurgico . presenza di un processo infettivo in atto e , dopo ulteriori approfondimenti clinici , i pazienti sono stati trattati con antimicotici ( un caso ) o antibiotici ( 3 casi )  . 
nei restanti 6 casi ( 6 dei 17 con diagnosi nale ) lesame pet risultato negativo o inutile ai ni della diagnosi : a 2 pazienti stato diagnosticata una malattia auto - immune ; in un caso la diagnosi nale stata di emofagocitosi ed il paziente continua a presentare febbre dopo un anno di terapia ; 1 paziente presentava vasculite degli arti inferiori e bronchiolite obliterante con polmonite ( boop ) ; 1 paziente presentava microlitiasi biliare e questa stata giudicata come la responsabile della fuo ( in questo paziente alla pet si evidenziava un focale accumulo di ( 18f ) fdg intorno alla protesi biliare , ma il reperto stato giudicato come reazione ogistica dovuta alla presenza della stessa )  . 
 di questi pazienti : 3 continuano a presentare febbre dopo due anni di follow - up ( ipotesi diagnostiche : febbre ereditaria , malattia auto - immune ) ; in 3 casi la febbre scomparsa spontaneamente ; 1 paziente morto per cachessia quattro mesi dopo aver eseguito lesame pet . nel nostro studio il valore della pet nellindirizzare la diagnosi stato del 46% ( 11 / 24 )  . 
in due casi lesame pet stato falsamente radiol med ( 2011 ) 116 : 809820 2 years of follow - up ( diagnostic hypotheses of hereditary fever , autoimmune disease ) ; three underwent spontaneous fever remission ; one died of cachexia 4 months after the pet scan . 
in two cases , pet was falsely positive ( one case was the abovementioned patient with biliary microlithiasis and another patient presented a misleading [ 18f ] - fdg uptake in abdominal lymph nodes that was not con rmed by the biopsy )  . 
therefore , of 11 negative pet studies , only one ( 9% ) was followed by a worsening of the clinical condition . discussion in the diagnostic de nition of patients with fuo , the optimal examination is one that has the highest sensitivity to allow identi cation of the aetiology and consequently appropriate treatment planning , enables monitoring of the response to treatment and subsequent follow - up , is also useful in negative cases by identifying patients with a good prognosis for whom the best approach is to wait and see . 
in identifying fuo aetiology , the possible advantages of pet and pet / ct over other diagnostic procedures were largely understood several years ago , and in the last decade , its use in this eld has been extensively evaluated ( table 2 ) [ 1122 ]  . 
pet was helpful in 55% of patients , showing a high positive predictive value ( ppv ) ; furthermore , the authors reported on the usefulness of pet in negative cases also . 
 [ 12 ] , compared the utility of [ 18f ] - fdg - pet and 67ga - citrate scintigraphy to obtain a diagnosis in 58 consecutive cases of fuo . 
pet was used as a second step technique when the cause was not identi ed after medical history and clinical examination , routine laboratory tests , chest radiography and abdominal us . 
 [ 14 ] , in a prospective study of 19 patients with classical fuo recruited from the department of infectious diseases , compared inpositivo ( un primo caso era il paziente sopracitato con la micro - litiasi biliare , un secondo paziente ha presentato un anomalo accumulo in linfonodi addominali reperto che la successiva biopsia non ha confermato come responsabile della febbre )  . 
in de nitiva , di 11 pazienti con esame pet negativo solo 1 ( 9% ) ha mostrato una prognosi negativa . discussione per una gestione clinica ottimale dei pazienti con fuo classica , lesame ideale dovrebbe : avere la massima sensibilit possibile , cos da permettere lidenti cazione delleziologia e di conseguenza la piani cazione del trattamento migliore ; consentire la possibilit di monitorare la risposta al trattamento ed il successivo follow - up ; risultare utile anche in caso di negativit , identi cando quei pazienti con prognosi migliore e dunque nei quali lapproccio migliore quello del wait and see . 
ma i teorici vantaggi dellesame pet e pet / tc rispetto agli altri esami nellidenti care le cause della fuo , sono stati intuiti da diversi autori e nellultima decade il ruolo della pet stato estesamente indagato e discusso ( tabella 2 ) [ 1122 ]  . 
lesame pet era infatti utile a ni diagnostici nel 55% dei casi , con un valore predittivo positivo ( ppv ) elevato ; inoltre , gi in questo lavoro , gli autori sottolineavano lutilit dellesame pet anche nei casi negativi . 
 [ 12 ] hanno confrontato il ruolo della ( 18f ) fdg - pet con quello della scintigra a con 67ga citrato nellidenti cazione delle cause di fuo in un gruppo di 58 pazienti . 
in quello studio , lesame pet stato usato come second step technique , vale a dire in quei casi in cui la causa non era stata identi cata dopo anamnesi , esame obiettivo , esami laboratoristici di routine , radiograa del torace ed ecogra a addominale . 
la pet risultata utile per raggiungere la diagnosi nale nel 69% dei casi , mentre nei pazienti con pet negativa , nessuno studio successivo riuscito ad identi care la causa di fuo . 
 [ 14 ] , nel 2004 , in un studio prospettico hanno confrontato la scintigra a con granulociti marcati e la ( 18f ) fdg - pet , in 19 pazienti con fuo classica ricoverati nel reparto di malattie infettive . 
 [ 15 ] reported a large retrospective study of 74 patients in which pet was performed only if the history , clinical examination , blood chemistry , urinalysis , chest xray and abdominal us failed to provide clear diagnostic indications . 
 [ 15 ] hanno pubblicato un grosso studio retrospettivo su 74 pazienti , nei quali lesame pet era stato effettuato solo dopo che lanamnesi , lesame obiettivo , lemocromo , lesame urine , la radiogra a del torace e lecogra a addominale non avevano portato una chiara indicazione diagnostica . 
lo studio pet risultato pi utile nei pazienti con febbre continua piuttosto che in quelli con febbre intermittente , e nei casi con pcr e ves elevati piuttosto che in quelli con valori normali . 
jaruskova radiol med ( 2011 ) 116 : 809820 in patients with continuous rather than intermittent fever and was found useful in 39% of cases with elevated crp and esr but not in those with normal values . 
 [ 17 ] , in a study in 118 patients with prolonged febrile status ( 76% fuo , 24% suspected postsurgical infections ) , reported that pet or pet / ct was helpful for diagnoses in 36% of the entire population . 
 [ 18 ] evaluated the role of [ 18f ] - fdg - pet / ct in 48 patients , in 46% of which pet identi ed the underlying cause of fuo , with a ppv and a negative predictive value for focal disease of 81% and 100% , respectively . 
a negative [ 18f ] - fdg - pet / ct performed after the initial workup was highly indicative for establishing a wait - and - see strategy and obviated the need for further investigations . 
in this study , the [ 18f ] - fdg - pet / diagnostic contrast - enhanced ct ( cect ) was reported in conference by a radiologist and a nuclear medicine physician . 
 [ 21 ] , performing a similar study in 68 patients , reported a pet / cect diagnostic yield of 56% ( particularly in patients with high levels of crp and esr )  . 
 [ 22 ] , in a study of the role of pet or pet / ct in 44 children with fuo , reported similar results to the studies on adults : 19 scans ( 43% ) were useful for the nal diagnosis . 
patient age did not in uence the accuracy of the technique , whereas crp levels were signi cantly higher in patients with a positive pet scan than in those with a normal scan . 
furthermore , there are some dif culties that limit the use of this examination : rstly , the need for an in vitro labelling process of the white blood cells with its associated risks ( in particular blood contamination ) ; secondly , the special equipment and quali ed staff required ; thirdly , the time required to complete the exam [ 23 ]  . 
on the other hand , the examination is not helpful in the case of malignancies or vasculitis [ 24 , 25 ] , and this limitation is now more important considering the fact that et al . 
 [ 17 ] , in un lavoro su 118 pazienti con prolungato stato febbrile ( 76% fuo e 24% sospette infezioni post - chirurgiche ) hanno riportato che pet o pet / tc erano di aiuto per la diagnosi nel 36% della loro popolazione . 
nel 46% di questi , lesame ha identi cato la causa della fuo ; il ppv e il valore predittivo negativo per lidenti cazione di malattia focale sono risultati rispettivamente del 81% e 100% . 
 [ 20 ] hanno valutato il ruolo dellesame ( 18f ) fdg - pet combinato con tc diagnostica ( cetc ) , refertato in collaborazione tra medico nucleare e radiologo , in 48 pazienti con fuo . 
 [ 21 ] , effettuando un studio molto simile , hanno riportato valori di sensibilit interessanti ma signi cativamente minori , pari al 56% ( in questo studio , la massima sensibilit era nei pazienti con pcr e ves elevati )  . 
non ci sono chiare spiegazioni per giusti care la differenza tra questi due studi , per questo altri lavori sarebbero estremamente utili al ne di stabilire il reale potenziale dellesame pet / tc con tc diagnostica . 
 [ 22 ] studiando il ruolo dellesame pet o pet / tc in 44 bambini con fuo , hanno trovato risultati simili agli studi effettuati negli adulti : 19 esami ( 43% ) sono risultati utili per raggiungere una diagnosi nale . 
let del paziente non in uenzava laccuratezza della tecnica mentre i valori di pcr erano signi cativamente pi elevati nel gruppo dei pazienti con pet positiva rispetto a quelli con pet negativa . come dimostrato da altri autori , lo studio pet non lunico esame di medicina nucleare disponibile per pazienti con fuo . 
peraltro varie dif colt limitano luso di questo esame : primo , la necessit di una marcatura in vitro delle cellule ematiche con tutti i rischi associati ; secondo , sono necessarie una speciale attrezzatura e personale quali cato ; terzo , il tempo necessario per completare lacquisizione dellesame [ 23 ]  . 
 inoltre , in caso di neoplasia o vasculite , questo esame non utile [ 24 , 25 ] e tale limite oggi ancora pi rilevante considerando il fatto che lo spettro delle malattie che causano fuo si sta modi cando con riduzione della prevalenza delle infezioni [ 24 ]  . 
lunico studio che ha confrontato lutilit della ( 18f ) 818 radiol med ( 2011 ) 116 : 809820 the spectrum of diseases causing fuo is changing with a decrease in the proportion of infections [ 24 ]  . 
the only study that compared the utility of [ 18f ] - fdg - pet and white blood cell scans [ 14 ] reported that the latter demonstrated signi cantly greater speci city . 
however , this study had many limitations : the number of patients was very small , the study was performed with pet alone and the ndings were not subsequently con rmed . our study lends support to previous results , con rming and stressing the crucial role of pet / ct in the clinical setting of classical fuo . 
first of all , we can stress the fact that the use of the hybrid scanner adds crucial advantages to pet alone , as the integration of anatomical and morphological images allows improved interpretation of both abnormal [ 18f ] - fdg uptake and suspicious morphological ndings . 
pet / ct was of help in the diagnostic de nition of 11 out of the 24 selected cases ( pet / ct positive in focal in ammations , malignancies and vasculitis ) , but it was also useful in negative cases . 
it should be pointed out that with high probability , a negative scan excludes malignancies , vasculitis and focal infections , and this is helpful both for the referring clinician and for the patient . 
finally , pet / ct is a totalbody , noninvasive , practical and well - tolerated examination , which allows the conclusion of the diagnostic workup in the case of both positive and negative results . 
therefore , during the diagnostic workup , if a ct scan is required , the pet / ct study is equally useful , if not more so . study limitations fdg - pet con quella della scintigra a con globuli bianchi marcati [ 14 ] ha riportato una maggiore speci cit di questultima . 
tuttavia questo studio presentava diversi limiti : il gruppo dei pazienti incluso era estremamente piccolo , lo studio stato effettuato con tomografo pet in assenza di co - registrazione tc , questi dati non sono stati convalidati da altri studi in letteratura . per quello che riguarda la pet / tc , i risultati del nostro studio rafforzano e confermano quelli delle precedenti pubblicazioni , evidenziando il ruolo cruciale di questo esame nella gestione clinica dei pazienti con fuo classica . 
possiamo evidenziare che lesame pet eseguito con tecnica ibrida ( pet / tc ) aggiunge vantaggi cruciali al semplice esame pet grazie al fatto che luso combinato delle immagini anatomiche e di quelle morfologiche consente di migliorare linterpretazione degli accumuli patologici di ( 18f ) fdg e dei reperti anatomici sospetti . 
in questi pazienti , infatti , sia il radiologo che il medico nucleare sono alla ricerca di un indizio e qualsiasi anomalia ( anatomica o funzionale che sia ) potrebbe essere lespressione della causa eziologica . 
dunque , il fatto di poter acquisire simultaneamente e co - registrare entrambi i tipi di immagine porta alla riduzione dei tempi necessari alliter diagnostico e , soprattutto , migliora il risultato nale . 
il valore aggiunto dellesame pet / tc la sua utilit sia nei casi positivi che in quelli negativi ; questa aspetto rinforzato nel nostro studio dal lungo periodo di follow - up . 
lesame pet / tc ha contribuito nellidenti cazione della causa di fuo in 11 dei 24 pazienti ( pet / tc positiva in pazienti con in ammazione focale , neoplasia e vasculite ) ; tuttavia va sottolineato il fatto che lesame risultato utile anche nei casi negativi . 
importante sottolineare che un esame negativo esclude , con alta probabilit , la presenza di neoplasia , vasculite o infezioni focali e questo di aiuto sia per il medico che per il paziente . 
in ne , la pet / tc un esame total body , non invasivo , facile da eseguire e ben tollerato , che consente di giungere alla conclusione delliter diagnostico sia nei casi positivi che in quelli negativi . 
il numero dei pazienti incluso limitato e c una certa eterogeneit tra i radiol med ( 2011 ) 116 : 809820 low , and there was a certain heterogeneity in our population , which was further increased by the fact that the study was undertaken in a diagnostic centre related to different community hospitals . 
questi aspetti potrebbero aver in uenzato la nostra sensibilit complessiva ; tuttavia anche vero che quella presentata nel nostro studio attualmente la situazione pi tipica nella quale si trova ad operare il medico nucleare . 
if larger studies on this topic con rm our ndings , pet / ct , or better , pet / cect , should be included in the routine diagnostic workup of patients with classical fuo . nellultima decade , pi di una dozzina di studi hanno valutato il ruolo dellesame pet e pet / tc nei pazienti con fuo classica . 
 lesame pet / tc risulta utile sia nel caso risulti positivo sia nel caso risulti negativo ; inoltre , nei casi positivi , consente anche di monitorare la risposta al trattamento e di eseguire leventuale follow - up . 
 after the histopathological diagnosis had been obtained , the lesions were retrospectively divided into ve groups : adenocarcinomas ( n = 16 ) , squamous cell carcinomas ( n = 12 ) , chronic pneumonias ( n = 2 ) , malignant mediastinal tumours ( n = 2 ) and typical carcinoids ( n = 2 )  . 
using an adc value of 1.2510 - 3 mm2 / s as a threshold , we were able to differentiate malignant from benign lesions with 91% diagnostic accuracy , 90% sensitivity , 100% speci city , 100% positive predictive value and 57% negative predictive value . 
lobiettivo del nostro lavoro stato valutare retrospettivamente il ruolo delle sequenze pesate in diffusione con soppressione del segnale del grasso e del background nella diagnostica differenziale di lesioni benigne e maligne del distretto toraco - mediastinico , attraverso il calcolo dei valori medi del coef ciente di diffusione apparente ( adc )  . 
trentaquattro pazienti portatori di noduli polmonari / masse mediastiniche , gi sottoposti a tomogra a computerizzata ( tc ) del torace sono stati sottoposti a risonanza magnetica ( rm ) del torace con sequenze pesate in diffusione . 
retrospettivamente , dopo aver ottenuto la diagnosi istopatologica , le lesioni sono state suddivise in cinque gruppi : adenocarcinomi ( n = 16 ) , carcinomi squamocellulari ( n = 12 ) , polmoniti croniche ( n = 2 ) , tumori maligni mediastinici ( n = 2 ) , carcinoidi tipici ( n = 2 )  . 
le sequenze short tau inversion recoveryradiol med ( 2011 ) 116 : 720733 mediastinum provided potentially useful images for the differential diagnosis of benign and malignant lesions . keywords diffusion - weighted imaging ( dwi ) thoracopulmonary mri chest lesions echo - planar imaging ( stir - epi ) applicate al distretto toraco - mediastinico forniscono immagini potenzialmente utili per la diagnosi differenziale di lesioni benigne e maligne . parole chiave imaging pesato in diffusione rm toracopolmonare lesioni toraciche introduction introduzione carr and purcell rst reported that the magnetic resonance ( mr ) signal could be in uenced by the diffusion of water molecules in 1954 . 
the date of this discovery is not surprising , as the magnet they used created such a heterogeneous magnetic eld that it generated a constant eld gradient of around 1 gauss / cm [ 1 ] , resulting in an artefactual signal related to proton motion . 
the rst studies on the application of dw - mri to extracranial sites were disappointing , as image quality was poor , the possibility of adc quanti cation was limited and adc values had low reproducibility . 
in recent years , several investigators have demonstrated the diagnostic potential of dwi in extracranial pathology , and in particular in oncology [ 2 , 3 , 5 , 6 , 810 ]  . 
 in the study of the chest , computed tomography ( ct ) is the modality of choice for evaluating morphology , dimensions , location and structure of pulmonary nodules , as well as the most commonly used noninvasive modality for studying mediastinal masses . 
in recent years , short - tau inversion - recovery echo - planar imaging ( stir - epi ) sequences have been optimised for wb - dw - mri [ 10 , 11 ]  . 
stir - epi sequences allow fat suppression ( with a presaturation inversion pulse ) and suppression of the background body signal , including vessels , muscles and connective tissue ( characterised by high isotropic diffusivity ) by diffusion weighting . 
 these sequences can be applied to the chestmediastinum nel 1954 carr e purcell [ 1 ] notarono per la prima volta che il segnale nella risonanza magnetica ( rm ) poteva essere in uenzato dalla diffusione delle molecole di acqua ; la data di questa scoperta non deve sorprendere in quanto il magnete da loro utilizzato creava un campo magnetico cos disomogeneo da generare un gradiente di campo costante di circa 1 gauss / cm [ 1 ]  . 
nelle sequenze pesate in diffusione il contrasto tissutale dipende infatti dal grado di restrizione del movimento protonico ; tali sequenze permettono inoltre di quanti care il grado di restrizione attraverso il calcolo del coef ciente di diffusione apparente ( adc )  . limaging pesato in diffusione da diversi anni affermato , in campo neuroradiologico ; gli ottimi risultati ottenuti in tale ambito hanno suggerito unestensione dellimpiego di tale tecnica in altri distretti sino alle recentissime applicazioni allintero corpo whole body diffusion magnetic resonance imaging ( wb - dwmri ) [ 211 ]  . 
i primi studi sullapplicazione dellimaging pesato in diffusione ( dwi ) con rm in ambito extracranico hanno avuto risultati poco incoraggianti ; la qualit delle immagini ottenute era scarsa , la possibilit di quanti care ladc molto limitata , i valori calcolati poco riproducibili . 
negli ultimi anni diversi autori hanno documentato le potenzialit diagnostiche del dwi in ambito extracranico , soprattutto nella patologia oncologica [ 2 , 3 , 5 , 6 , 810 ]  . 
 in ambito toracico la tomogra a computerizzata ( tc ) rappresenta la metodica delezione per la valutazione morfologica , dimensionale , topogra ca e strutturale dei noduli polmonari ; la tc inoltre la metodica non invasiva maggiormente utilizzata per lo studio delle masse mediastiniche . 
 materials and methods patients over a period of 30 months ( november 2006 to april 2009 ) , we selected 34 patients ( 25 men and nine women , age range 4773 years , mean age 59 years ) who underwent dw - mri of the chest without administration of contrast material . 
patients were enrolled in the study after undergoing unenhanced and contrast - enhanced ct of the chest , according to the following inclusion criteria : ct evidence of a solitary pulmonary nodule or mediastinal mass requiring characterisation by ct - guided biopsy or mediastinoscopy ; axial dimensions of the pathological nding absence of clear ct features of benignity or malignancy ( in particular , absence of calci cation and necrotic foci , and absence of low - density areas with fat attenuation inside the lesions )  . after mri , 32 patients underwent transthoracic ctguided biopsy and two underwent mediastinoscopy . 
the histopathological diagnosis was considered the standard of reference in all patients . 1 cm , examination technique and image analysis ct examinations were carried out with a light speed 4 system ( ge medical systems , milwaukee , wi , usa )  . 
 scans were acquired during a single breath - hold before and after administration of nonionic iodinated contrast material ( 80100 ml , ow rate 34 ml / s , scan delay 2530 s from the beginning of the injection ) after obtaining the patients informed consent . 
scan parameters were as follows : slice thickness 5 mm ( with retroreconstruction up to 2.5 mm ) ; feed 15 mm / rotation ; rotation speed 0.8 s ; overall acquisition time 1215 s ; 120140 kv ; 180240 ma . 
the mr studies were performed with a 1.5 - t imager ( achieva , philips medical systems , best , the netherlands , release 2.1 ) with a 33 mt / m gradient strength and 160 mt / m / s slew rate by using phased - array sensitivityencoding ( sense ) body coils . 
le sequenze stir - epi sopprimono il segnale del tessuto adiposo ( mediante il pre - impulso di inversione ) e dei tessuti di fondo ( background - suppression ) rappresentati da vasi , muscoli , connettivo ( tessuti caratterizzati da diffusivit isotropica ) mediante la pesatura in diffusione . 
 materiali e metodi pazienti in un periodo di 30 mesi ( da novembre 2006 ad aprile 2009 ) , abbiamo selezionato 34 pazienti ( 25 uomini e 9 donne di et 4773 anni , con et media di 59 anni ) che sono stati sottoposti ad esame diffusion - rm del distretto toracico , senza somministrazione di mezzo di contrasto ( mdc )  . 
i pazienti sono stati arruolati , dopo essere stati sottoposti ad esame tc del torace , con e senza mdc , secondo i seguenti criteri dinclusione : riscontro allesame tc di un nodulo polmonare solitario o di una massa mediastinica da caratterizzare mediante biopsia tc - guidata o mediastinoscopia ; dimensioni assiali del tessuto patologico non inferiori ad 1 cm ; assenza di caratteristiche tomodensitometriche altamente probanti per benignit o malignit ( in particolare : assenza di calci cazioni e di foci necrotici intralesionali , assenza di aree ipodense , con valori densitometrici di tipo adiposo , allinterno delle lesioni )  . dopo lesame rm 32 pazienti sono stati sottoposti a biopsia transtoracica tc - guidata , 2 pazienti a mediastinoscopia . 
adc maps were automatically generated by the software on the basis of the images obtained with a b factor of 1 , 000 s / mm2 and 0 s / mm2 . 
adc values were calculated by a radiologist ( reader 1 , as , with 8 years of experience in mr imaging )  . dwis acquired with b values of 0 , 500 and 1 , 000 s / mm2 were also subjected to qualitative evaluation . 
two radiologists ( reader 2 , as , with 14 years of experience in mri ; reader 3 , ac , with 27 years of experience ) assessed lesion signal intensity , which were displayed by inverting the grey scale to visualise pathological tissue ( increased signal ) as a hypointense area ( grey - black ) in a background devoid of signal . 
the two readers were then asked to independently rate the signal intensity of the pathological areas , according to the following scale : 0 : no signal , equal to signal of the pulmonary parenchyma ; 1 : nearly no signal , slightly higher than that of the pulmonary parenchyma ( lesions just detectable in the dw sequences ) ; 2 : intermediate signal , between 1 and 3 ; 3 : high signal ( areas of de nite hypointensity appearing black on dwi and with similar signal intensity to that of the spinal cord )  . statistical analysis mean adc value was calculated for each lesion by placing an roi on the pathological areas . 
following qualitative evaluation of dwi , the degree of agreement between the two radiologists was assessed by calculating the cohen kappa coefcient . 5 mm ( retroricostruibile no a 2 , 5 mm ) , velocit di avanzamento 15 mm / rotazione , tempo di rotazione di 0 , 8 s , tempo complessivo di acquisizione pari a 1215 s , 120140 kv , 180240 ma . 
gli esami rm sono stati condotti con apparecchiatura da 1 , 5 t ( achieva , philips medical systems , best , olanda , release 2.1 ) , con potenza dei gradienti di 33 mt / m e slew - rate dei gradienti di 160 mt / m / s utilizzando bobine phased - array sense ( sensitivity encoding ) - body per la ricezione del segnale . 
dalle immagini ottenute con pesatura del parametro b di 1000 s / mm2 e 0 s / mm2 sono state generate automaticamente , dal software della rm , le mappe adc . 
il calcolo delladc stato effettuato da un radiologo ( lettore 1 : as , con 8 anni di esperienza in rm )  . le immagini pesate in diffusione acquisite con valori del parametro b di 0 , 500 e 1000 s / mm2 sono state inoltre valutate qualitativamente . 
due radiologi ( lettore 2 : as , con 14 anni di esperienza in rm , lettore 3 : ac con 27 anni di esperienza in rm ) hanno valutato lintensit del segnale delle lesioni , visualizzate invertendo la scala dei grigi in maniera tale da ottenere la visualizzazione del tessuto patologico ( segnale incrementato ) come area ipointensa ( grigio - nera ) su uno sfondo privo di segnale ( rappresentato dal background )  . 
dopo la valutazione delle immagini ai due lettori stato chiesto , indipendentemente , in cieco , di giudicare lintensit di segnale delle aree patologiche , secondo la seguente scala : 0 : intensit di segnale nulla , pari al segnale del parenchima polmonare ; 1 : intensit di segnale quasi nulla , di poco superiore al segnale del parenchima polmonare ( lesioni appena riconoscibili nelle sequenze pesate in diffusione ) ; 2 : intensit di segnale intermedia , tra 1 e 3 ; 3 : elevata intensit di segnale ( aree nettamente ipointense , nere nelle immagini pesate in diffusione , con la stessa intensit di segnale del midollo spinale )  . analisi statistica su ognuna delle lesioni esaminate stato calcolato il 724 results histopathological analysis overall , 30 malignant and four benign lesions were diagnosed . 
there were 16 adenocarcinomas , including undifferentiated ( g4 , n = 1 ) , poorly differentiated ( g3 , n = 7 ) and moderately differentiated ( g2 , n = 8 ) carcinomas ; 12 squamous cell carcinomas , including undifferentiated ( g4 , n = 1 ) , poorly differentiated ( g3 , n = 5 ) , moderately differentiated ( g2 , n = 2 ) , and well - differentiated ( g1 , n = 4 ) carcinomas ; two chronic in ammatory lesions , including one lipoid pneumonia and one eosinophilic pneumonia ; two malignant mediastinal tumours , including one mediastinal teratoma and one thymic carcinoma ; and two typical carcinoids . 
 lesion histopathological diagnosis , location , preoperative staging and grading are reported in table 1 . radiol med ( 2011 ) 116 : 720733 valore medio di adc attraverso il posizionamento di roi sulle aree patologiche . 
stato determinato un valore soglia di adc per discriminare con la massima accuratezza diagnostica le lesioni benigne dalle maligne . lanalisi statistica dei dati stata effettuata utilizzando la versione 13.0 del software spss ( spss , chicago , illinois )  . 
figures 1 and 2 show ct scans , dw images and adc maps ( with rois for adc quanti cation ) of two patients affected by an adenocarcinoma and a squamous cell carcinoma , respectively . 
sono stati diagnosticati 16 adenocarcinomi di cui : carcinomi indifferenziati ( g4 ) n = 1 , carcinomi scarsamente differenziati ( g3 ) n = 7 , moderatamente differenziati ( g2 ) n = 8 ; 12 carcinomi squamocellulari di cui carcinomi indifferenziati ( g4 ) n = 1 , carcinomi scarsamente differenziati ( g3 ) n = 5 , moderatamente differenziati ( g2 ) n = 2 , ben differenziati ( g1 ) n = 4 ; 2 alterazioni ogistiche croniche di cui una polmonite lipoidea , una polmonite eosino la ; 2 tumori maligni mediastinici di cui un teratoma mediastinico , un carcinoma timico ; 2 carcinoidi tipici . 
non sono state riscontrate differenze statisticamente signi cative tra il valore medio di adc calcolato nel gruppo degli adenocarcinomi ( 1 , 36410 - 3 mm2 / s ) ed il valore medio di adc calcolato nel gruppo delle lesioni maligne mediastiniche ( 1 , 05110 - 3 mm2 / s ) ( p > 0 , 05 )  . 
by using a threshold adc value of 1.25103 mm2 / s , we were able to differentiate benign from malignant lesions with the highest diagnostic accuracy ( 91% ) , with 90% sensitivity , 100% speci city , 100% positive predictive value , and 57% negative predictive value ( table 3 )  . qualitative analysis of signal intensity all lesions examined were detectable on dwi , with signal intensity values of 2 to 3 according to the scale adopted . 
no dio di adc calcolato nel gruppo degli adenocarcinomi ( 1 , 36410 - 3 mm2 / s ) si dimostrato signi cativamente inferiore rispetto al valore medio di adc calcolato nel gruppo delle ogosi croniche ( 1 , 85410 - 3 mm2 / s ) ( p < 0 , 05 )  . 
nella figura 4 riportiamo le immagini pesate in diffusione e la relativa mappa adc ( con il posizionamento dellarea roi per la quanti cazione del coef ciente di diffusione apparente ) di un paziente portatore di polmonite lipoidea . adenocarcinomi versus carcinoidi tipici : il valore medio di adc calcolato nel gruppo degli adenocarcinomi ( 1 , 36410 - 3 mm2 / s ) risultato signi cativamente inferiore rispetto al valore medio di adc calcolato nel gruppo dei carcinoidi tipici ( 2 , 20010 - 3 mm2 / s ) ( p < 0 , 05 )  . 
nella figura 5 riportiamo laspetto tc , limaging in diffusione con relativa mappa adc di un paziente portatore di carcinoide tipico . carcinomi squamocellulari versus ogosi croniche : il radiol med ( 2011 ) 116 : 720733 table 2 mean apparent diffusion coef cient ( adc ) values calculated by placing a region of interest ( roi ) over the single lesions examined patient no . 
cohens kappa coef cient for b factor equal to 0 was 0.51 ( poor interrater agreement ) ; for b factor equal to 500 , 0.76 ( indicating substantial agreement ) ; for b factor equal to 1 , 000 , 0.87 ( indicating almost perfect agreement )  . 
previous studies conducted on other body regions have reported statistically signi cant differences in adc values of benign valore medio di adc calcolato nel gruppo delle ogosi croniche ( 1 , 85410 - 3 mm2 / s ) risultato signi cativamente superiore rispetto al valore medio di adc calcolato nel gruppo dei carcinomi squamocellulari ( 1 , 23110 - 3 mm2 / s ) ( p < 0 , 05 )  . 
 carcinomi squamocellulari versus carcinoidi tipici : i valori medi di adc calcolati nel gruppo dei carcinomi squamo cellulari ( 1 , 23110 - 3 mm2 / s ) risultano signi cativamente inferiori rispetto ai valore medi di adc calcolati nel gruppo dei carcinoidi tipici ( 2 , 20010 - 3 mm2 / s ) ( p < 0 , 05 )  . 
 lesioni maligne mediastiniche versus ogosi croniche : il valore medio di adc calcolato nel gruppo delle lesioni maligne mediastiniche ( 1 , 05110 - 3 mm2 / s ) si dimostrato signi cativamente inferiore rispetto al valore medio di adc calcolato nel gruppo delle ogosi croniche ( 1 , 85410 - 3 mm2 / s ) ( p < 0 , 05 )  . 
 lesioni maligne mediastiniche versus carcinoidi tipici : il valore medio di adc calcolato nel gruppo delle lesioni maligne mediastiniche ( 1 , 05110 - 3 mm2 / s ) risulta signicativamente inferiore rispetto al valore medio di adc calcolato nel gruppo dei carcinoidi tipici ( 2 , 20010 - 3 mm2 / s ) ( p < 0 , 05 )  . 
 confronto tra lesioni benigne flogosi croniche versus carcinoidi tipici : non sono state riscontrate differenze statisticamente signi cative tra i valori medi di adc calcolati nel gruppo delle ogosi croniche ( 1 , 85410 - 3 mm2 / s ) e il valore medio di adc calcolato nel gruppo dei carcinoidi tipici ( 2 , 20010 - 3 mm2 / s ; deviazione standard [ ds ] 0 , 338 ) ( p > 0 , 05 )  . 
utilizzando un valore soglia di adc di 1 , 25103 mm2 / s stato possibile differenziare lesioni benigne dalle maligne con la pi alta accuratezza diagnostica ( 91% ) , con valori di sensibilit del 90% , speci cit del 100% , valore predittivo positivo del 100% e valore predittivo negativo del 57% ( tabella 3 )  . 
per un valore di b factor uguale a 0 , la costante di cohen calcolata stata di circa 0 , 51 ( scarso grado di agreement tra i due osservatori )  . 
per valori tabella 2 valori medi di coef ciente di diffusione apparente ( adc ) calcolati mediante il posizionamento delle roi a livello delle singole lesioni esaminate di b factor uguale a 1000 , la costante di cohen risultava pari a 0 , 87 ( grado di agreement tra i due radiologi molto buono )  . 
 radiol med ( 2011 ) 116 : 720733 paziente ( numero ) diagnosi istopatologica ( 103 mm2 / s ) discussione 728 adenocarcinoma adenocarcinoma carcinoma squamocellulare carcinoma squamocellulare polmonite lipoidea adenocarcinoma adenocarcinoma adenocarcinoma carcinoma squamocellulare carcinoma squamocellulare carcinoma squamocellulare carcinoma squamocellulare carcinoma squamocellulare carcinoma squamocellulare adenocarcinoma carcinoma squamocellulare carcinoma timico carcinoma squamocellulare adenocarcinoma adenocarcinoma polonite eosino la adenocarcinoma carcinoma squamocellulare carcinoma squamocellulare adenocarcinoma adenocarcinoma adenocarcinoma teratoma maturo adenocarcinoma carcinoide tipico carcinoide tipico adenocarcinoma adenocarcinoma adenocarcinoma 1 , 360 , 36 1 , 240 , 23 1 , 240 , 81 1 , 530 , 21 1 , 880 , 30 1 , 230 , 02 1 , 450 , 26 1 , 300 , 15 1 , 220 , 18 1 , 230 , 19 1 , 130 , 22 0 , 770 , 12 1 , 270 , 14 1 , 330 , 15 1 , 390 , 17 1 , 280 , 18 1 , 130 , 19 1 , 230 , 24 1 , 40 , 17 1 , 740 , 26 1 , 940 , 34 1 , 280 , 25 1 , 270 , 20 1 , 310 , 15 1 , 450 , 69 1 , 370 , 23 1 , 290 , 26 1 , 040 , 14 1 , 290 , 14 2 , 20 , 33 2 , 10 , 24 1 , 320 , 16 1 , 350 , 18 1 , 280 , 19 and malignant lesions . 
in agreement with previous reports [ 29 ] , our study demonstrated that diffusion is signi cantly restricted in cases of pathological hypercellularity in which extracellular spaces , where proton diffusion is relatively unrestricted , are extremely reduced . 
cell density increases in tumours in comparison with healthy tissue , and the adc consequently decreases , as seen in the patients affected by malignancies with different degrees of cell differentiation . in the thoracopulmonary region , dwi with adc quanti cation proved to be useful in the differential diagnosis between malignant and benign lesions . 
only a limited number of studies have investigated the possible use of dwi in chest imaging [ 1214 ] , and all of them used dw - epi sequences without presaturation pulses . 
le informazioni fornite ri ettono la struttura dei tessuti a livello cellulare ; in particolare lintensit del segnale fortemente in uenzata dalla densit cellulare , dalla presenza di giunzioni strette intercellulari , di membrane cellulari , di bre , di macromolecole , di organuli intracellulari . 
il nostro studio , in accordo con precedenti lavori [ 29 ] , dimostra che la diffusivit signi cativamente ristretta nei casi di patologica ipercellularit tissutale , in cui gli spazi interstiziali extracellulari , ove la diffusivit protonica scarsamente vincolata , risultano estremamente ridotti . 
nei tumori la densit cellulare aumenta rispetto ai tessuti normali , e ladc di conseguenza diminuisce come abbiamo osservato in questo lavoro nei pazienti affetti da neoplasie maligne a vario grado di differenziazione . 
in base alle nostre conoscenze questo studio rappresenta il primo lavoro in cui stato valutato il ruolo di sequenze pesate in diffusione con soppressione del grasso e del background nellimaging del distretto toracico . 
i precedenti studi hanno infatti utilizzato sequenze epi pesate in diffusione , senza pre - impulsi di saturazione . nella nostra esperienza le sequenze stir - epi hanno fornito immagini diagnostiche ed stato sempre possibile quanti care agevolmente il coef ciente di diffusione apparente . 
in tutti i pazienti esaminati , lidenti cazione del tessuto patologico stata semplice e facilitata dallinversione della nestra di visualizzazione . i risultati del nostro lavoro evidenziano una sovrapposizione dei valori di adc di adenocarcinomi e carcinomi squamocellulari , a vario grado di differenziazione ; questi dati differiscono dai risultati precedentemente ottenuti da altri autori [ 12 ]  . 
the lesion results in pathological restriction to tissue diffusivity and appears hyperintense on diffusion - weighted images acquired with a b factor equal to 1 , 000 ( b )  . 
la lesione determina patologica restrizione della diffusivit tissutale e presenta elevato segnale nelle sequenze dwi , acquisite con b factor pari a 1000 ( b ) , nestra di visualizzazione invertita . 
 the lesion results in pathological restriction to tissue diffusivity and is hyperintense in the diffusion - weighted sequences acquired with b factor equal to 1 , 000 ( b )  . 
il posizionamento della roi documenta valori medi di adc relativamente bassi ( 1 , 1710 - 3 mm2 / se ) ( c )  . 730 radiol med ( 2011 ) 116 : 720733 fig . 
3 patient with a mediastinal teratoma : the lesion causes pathological restriction to tissue diffusivity and is hyperintense in the diffusion - weighted sequences acquired with a b factor equal to 1 , 000 ( left panel , inverted display )  . 
la lesione determina patologica restrizione della diffusivit tissutale e risulta iperintensa nelle sequenze dwi , acquisite con b factor pari a 1000 ( immagine a sinistra , nestra di visualizzazione invertita )  . 
4 patient with chronic lipoid pneumonia : the lesion causes mild restriction to tissue diffusivity and has intermediate signal intensity in the diffusionweighted sequences acquired with a b factor equal to 1 , 000 ( left panel )  . 
il posizionamento della roi documenta valori medi di adc relativamente alti ( 1 , 8810 - 3 mm2 / s ) ( immagine a destra )  . quanti cation proved straightforward in all cases . 
the pathological tissue was readily detected in all patients , and detection was facilitated by inversion of the grey - scale display . the results of our study show an overlap of adc values of adenocarcinomas and squamous cell carcinomas with different degrees of cell differentiation . 
 [ 12 ] found signi cantly higher mean adc values among adenocarcinomas compared with squamous sizione dei valori medi di adc dei tumori maligni esaminati ( adenocarcinomi , carcinomi squamocellulari , lesioni maligne mediastiniche )  . 
listotipo ed il grado di differenziazione delle lesioni maligne non vengono determinati in base alla densit cellulare ; tale parametro biologico in uenza invece fortemente il grado di restrizione della diffusivit tissutale e quindi ladc . 
the lesion causes restriction to tissue diffusivity and appears moderately hyperintense in the diffusion - weighted sequences acquired with a b factor equal to 1 , 000 ( b )  . 
this may be explained by the fact that , although the degree of restriction to tissue diffusivity and therefore adc are strongly affected by cellular density , this biological parameter is not used to determined the histological type and grade of malignant lesions , and in histopathological classi cation , tumour grade is mostly established based on other factors , such as come la cheratinizzazione , la strati cazione e le atipie delle cellule , mentre la densit cellulare non un parametro particolarmente considerato , ci pu spiegare il nostro risultato . 
by applying an adc threshold value of 1.25103 mm2 / s , we were able to discriminate malignant from benign lesions with a very high level of diagnostic accuracy ( 91% )  . 
moreover , benign lesions have a reduced mitotic index compared with malignant lesions , and cell lysis and membrane fragmentation are much more limited . our results also demonstrate the poor speci city of the quantitative analysis of signal intensity in differentiating benign from malignant lesions , both of which present high signal intensity in stir - epi sequences ( between 2 and 3 according to the scale adopted )  . 
signal intensity in dw sequences is , in fact , in uenced by the t2 relaxation time of pathological tissues , unlike the adc , which is , instead , a reliable indicator of the degree of restriction to tissue diffusivity . the main limitation to our study is the small number of benign lesions included , so that our ndings require validation by larger series ; in addition , owing to the small size of the overall sample , the groups were compared with a nonparsoglia di adc pari a 1 , 25103 mm2 / s stato possibile discriminare lesioni maligne dalle benigne con la massima accuratezza diagnostica ( 91% )  . 
supponiamo che questo risultato sia legato alla ridotta densit cellulare e al ridotto rapporto nucleo / citoplasma delle lesioni benigne rispetto alle maligne ; inoltre le lesioni benigne hanno un indice mitotico ridotto rispetto alle lesioni maligne ed i fenomeni di lisi cellulare con frammentazione della membrana sono molto pi limitati . i risultati del nostro lavoro evidenziano inoltre la scarsa speci cit dellanalisi qualitativa del segnale nella differenziazione di lesioni benigne e maligne , che presentano indistintamente segnale elevato nelle sequenze stir - epi ( compreso tra 2 e 3 secondo la scala utilizzata )  . 
lintensit di segnale nelle sequenze pesate in diffusione risente infatti del tempo di rilassamento t2 dei tessuti patologici , a differenza del coef ciente di diffusione apparente , che invece un indice fedele del grado di restrizione della diffusivit tissutale . 
 il principale limite del nostro studio la scarsa numerosit campionaria del gruppo delle lesioni benigne , per cui i nostri risultati dovranno essere avvalorati da casistiche pi ampie ; a causa del campione numericamente ridotto i gruppi sono stati confrontati con un test non parametrico per variabili indipendenti ( test u di mann - whitney )  . 
furthermore , the small size of the sample did not allow statistical analysis of malignant lesions subdivided by grade of cell differentiation . zione di pazienti ( lesioni con istotipo , sede e grado di differenziazioni differenti )  . 
la ridotta numerosit del campione non ha inoltre permesso di effettuare unanalisi statistica per sottogruppi delle lesioni maligne a diverso grado di differenziazione . conclusioni conclusions the results of this study conducted on a limited number of patients demonstrate that stir - epi sequences applied to the chestmediastinum provides diagnostic images that are potentially useful for the differential diagnosis between benign and malignant lesions . 
further studies on more numerous and less heterogeneous patient series are required to validate these preliminary results . in conclusione i risultati di questo lavoro , su un ridotto numero di pazienti , dimostrano che le sequenze stirepi applicate al distretto toraco - mediastinico forniscono immagini diagnostiche , potenzialmente utili per la diagnosi differenziale di lesioni benigne e maligne . 
cademartiri1 , 2 1department of radiology and cardiology , c / o piastra tecnica , piano 0 , azienda ospedaliero - universitaria , via gramsci 14 , 43100 parma , italy 2department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands 3department of emergency medicine , azienda ospedaliero - universitaria , parma , italy 4department of cardiology , ospedale san gennaro , asl napoli 1 , naples , italy 5department of cardiology , azienda ospedaliero - universitaria , foggia , italy 6sdn foundation , ircss , naples , italy correspondence to : f . 
a total of 145 consecutive patients ( 75 men ; 6412 years ) with acp were referred from the emergency department for ctca , which was performed with a standard protocol using a 64 - slice scanner . 
patients were strati ed according to the morise clinical score ( low , intermediate , high ) and to the ctca ndings [ absence of coronary artery disease ( cad ) , nonobstructive cad , obstructive cad ]  . 
obstructive cad ( > 50% luminal narrowing ) was detected in 35 ( 24% ) patients ; nonobstructive cad ( 50% luminal narrowing ) in 62 ( 43% ) and absence of cad in 48 ( 33% ) patients . 
sixteen events ( three hard events ) occurred in patients without a history of cad , and four events ( one hard event ) occurred in patients with a history of cad . 
i pazienti sono stati strati cati secondo lo score di morise ( basso , intermedio , alto ) e la ctca ( assenza di coronary artery disease [ cad ] , cad non ostruttiva , cad ostruttiva )  . 
stata rilevata cad ostruttiva ( riduzione del lume > 50% ) in 35 ( 24% ) pazienti ; cad non ostruttiva ( riduzione del lume 50% ) in 62 ( 43% ) pazienti e assenza di cad in 48 ( 33% ) pazienti . 
sedici eventi ( 3 eventi hard ) si sono veri cati in pazienti senza storia di cad e 4 eventi ( 1 evento hard ) si veri cato nei pazienti con storia di cad . 
ctca shows the potential for optimal strati cation of patients with acp . keywords computed tomography coronary angiography prognostic value prognosis acute chest pain con assenza di cad secondo la ctca la frequenza di eventi stata pari allo 0% . 
la ctca ha il potenziale per una ottimale strati cazione del rischio nei pazienti con acp . parole chiave angiogra a coronarica mediante tomogra a computerizzata valore prognostico prognosi dolore toracico acuto introduction introduzione computed tomography coronary angiography ( ctca ) is an emerging technique for noninvasive evaluation of coronary atherosclerosis in patients with suspected and known coronary artery disease ( cad ) [ 16 ]  . 
current - generation ct scanners have a high diagnostic accuracy for detecting and excluding obstructive cad compared with conventional coronary angiography ( cag ) in selected patients [ 16 ]  . 
however , few data are available on the prognostic value of ctca [ 3 , 816 ]  . preliminary reports suggest that ctca has a very high negative predictive value ( npv ) for future cardiovascular events [ 3 , 816 ]  . 
ctca has been proposed for the immediate strati cation of patients presenting at the emergency room ( er ) with acute chest pain ( acp ) [ 1724 ]  . 
of these , 7080% are classi ed as nonanginal pain , 78% as acute coronary syndrome and up to 78% as non - st elevation myocardial infarction ( nstemi ) and / or unstable angina ( ua )  . 
la generazione corrente di apparecchiature di tomogra a computerizzata ( tc ) ha una elevata accuratezza diagnostica nella rilevazione ed esclusione della cad ostruttiva quando confrontata con la coronarogra a convenzionale ( cag ) in popolazioni selezionate di pazienti [ 16 ]  . 
al contrario , pochi dati sono disponibili riguardo il valore prognostico della ctca [ 3 , 816 ]  . studi preliminari mostrano un elevato valore predittivo negativo della ctca per eventi cardiovascolari a distanza [ 3 , 816 ]  . 
la ctca stata proposta per la strati cazione precoce dei pazienti che si presentano nel dipartimento di emergenza ( er ) con dolore toracico acuto ( acp ) [ 1724 ]  . 
lacp rappresenta il 5%10% dei pazienti che si presentano aller ; di questi il 70%80% viene classi cato come dolore toracico non anginoso , il 7%8% viene classi cato come sindrome coronarica acuta , e no al 7%8% viene classi cato come infarti miocardici senza sopra - elevazione del tratto st ( non - st elevation myocardial infarction , nstemi ) e / o angina instabile ( unstable angina , ua )  . 
patients with previous coronary artery bypass surgery ( cabg ) , known previous reaction to iodinated contrast medium and / or renal failure ( creatinine clearance < 60 ml / min ) were excluded . 
the morise risk score was calculated to stratify pretest risk [ 25 , 26 ]  . ctca data acquisition all examinations were performed with a single - source 64 - slice ct system ( somatom sensation 64 cardiac , siemens , forchheim , germany ) [ 4 ]  . 
first , a prospectively triggered coronary calcium ct data set was obtained using standardised ct parameters comprising 201.2 - mm collimation , 330 ms gantry rotation time , 120 kv tube voltage , 150 mas tube current . 
thereafter , ctca was performed after intravenous administration of 100 ml bolus of nonionic contrast material ( iomeron 400mgi / ml , bracco , milan , italy ) at a ow rate of 46 ml / s depending on patient status . 
ctca was performed with 640.6 mm collimation , 330 ms gantry rotation time , 120 kv tube voltage , 900 mas tube current , pitch 0.20 , temporal resolution 165 ms , spatial resolution 0.4 mm3 , reconstruction slice thickness 0.75 mm and reconstruction increment 0.5 m beta - blocker ( atenolol 510 mg ) was administered iv to all patients with a heart rate > 65 beats / min and without contraindications ( asthma or bronchospasm , systolic blood pressure < 100 mmhg )  . 
to obtain optimal image quality , data sets were reconstructed at no less than two points of the cardiac cycle using a retromateriali e metodi pazienti abbiamo arruolato retrospettivamente 145 pazienti consecutivi ( 75 maschi ; 6412 anni ) che si sono presentati al er della nostra istituzione con acp e sono stati inviati a ctca . 
 i pazienti con coronaropatia nota ( per esempio , pregresso infarto miocardico , pregressa rivascolarizzazione mediante angioplastica ) o con cardiopatia nota ( per esempio , scompenso cardiaco ) sono stati inclusi nello studio . 
i pazienti con pregresso bypass aorto - coronarico ( cabg ) , pregressa reazione al mezzo di contrasto iodato e / o insuf cienza renale ( clearance creatinina < 60 ml / min ) sono stati esclusi . 
sono stati considerati i seguenti fattori di rischio : ( 1 ) ipertensione ( de nita come pressione arteriosa [ pa ] 140 / 80 mmhg o necessit di terapia antiipertensiva ) ; ( 2 ) ipercolesterolemia ( colesterolo low density lipoprotein [ ldl ] > 130 mg / dl ) ; ( 3 ) diabete mellito ; ( 4 ) fumo ; ( 5 ) obesit ( body mass index [ bmi ] > 30 ) ; ( 6 ) familiarit per cardiopatia ischemica . 
 per la strati cazione del rischio pre - test stato utilizzato lo score di morise [ 25 , 26 ]  . scansione ctca tutti gli esami ctca sono stati effettuati con un apparecchiatura tc a singola sorgente a 64 strati ( somatom sensation 64 cardiac , siemens , forchheim , germania ) [ 4 ]  . 
 inizialmente , stata effettuata una scansione con triggering elettrocardiogra co ( ecg ) prospettico per la valutazione del calcio coronarico utilizzando parametri tc standard : collimazione 201 , 2 mm , tempo di rotazione del gantry 330 ms , voltaggio del tubo 120 kv , corrente del tubo 150 mas . 
 quindi , la ctca stata effettuata dopo la somministrazione di un bolo endovenoso di 100 ml di mezzo di contrasto non ionico ( iomeron 400 mgi / ml , bracco , milano , italia ) ad un usso di 46 ml / s a seconda delle condizioni del paziente . 
axial data sets were transferred to a remote workstation ( mmwp / leonardo , siemens medical solutions , forchheim , germany ) for postprocessing and subsequent evaluation . ct data analysis coronary artery calcium score the coronary artery calcium score ( cacs ) was assessed with the application of dedicated software ( cascore , siemens medical solutions )  . 
for multivariate analysis , patients were divided into ve groups based on cacs score : group 1 , cacs 010 ; group 2 , 11100 ; group 3 , cacs 101400 ; group 4 , cacs 4011000 ; group 5 , cacs > 1 , 000 . 
patients were nally classi ed as being in one of three groups based on the ctca ndings : ( 1 ) normal coronary arteries , ( 2 ) nonobstructive cad , and ( 3 ) obstructive cad . 
inoltre , in tutti i pazienti senza contro - indicazioni ( stenosi aortica severa , pressione arteriosa sistolica < 100 mmhg ) sono stati somministrati 0 , 3 mg di nitro - glicerina sub - linguale [ 27 ]  . 
per ottenere una qualit di immagine ottimale , i dataset sono stati ricostruiti in almeno due punti del ciclo cardiaco utilizzando un algoritmo ecg retrospettivo ( solitamente una fase tele - diastolica a 350 ms dallonda r ed una fase tele - sistolica a + 275 ms ) , quindi la modulazione prospettica dellamperaggio non stata utilizzata nel nostro studio . 
i dataset assiali sono stati trasferiti ad una workstation ( mmwp / leonardo , siemens medical solutions , forchheim , germania ) per il post - processing . analisi dei dati calcium score coronarico lo score del calcio coronarico ( cacs ) stato valutato con un software dedicato ( cascore , siemens medical solutions , forchheim , germania )  . 
il calcio coronarico stato identi cato automaticamente mediante lapplicazione software come aree di elevata densit lungo il decorso delle arterie coronarie la cui attenuazione risultava 130 unit houns eld ( hu )  . 
per lanalisi multi - variata i pazienti sono stati suddivisi in cinque gruppi a seconda del cacs score : pazienti con cacs 010 ( gruppo 1 ) , pazienti con cacs 11100 ( gruppo 2 ) , pazienti con cacs 101400 ( gruppo 3 ) , pazienti con cacs 4011000 ( gruppo 4 ) , e pazienti con cacs > 1000 ( gruppo 5 )  . 
le placche ostruttive sono state de nite come quelle che determinavano una riduzione del lume > 50% ; le placche non ostruttive sono state de nite tali quando determinavano una riduzione del lume coronarico50% . 
 694 radiol med ( 2011 ) 116 : 690705 in ogni paziente abbiamo valutato il numero di segmenti coronarici con ateromasia , il numero di segmenti con malattia ostruttiva , ed il numero di ogni tipo di placca . 
 in ne , i pazienti sono stati classi cati in 3 gruppi basandosi sulle caratteristiche della ctca : ( 1 ) pazienti con coronarie normali , ( 2 ) pazienti con malattia non ostruttiva , e ( 3 ) pazienti con malattia ostruttiva . 
gli end - point clinici utilizzati erano : ( 1 ) morte cardiaca , ( 2 ) infarto miocardico non fatale , ( 3 ) angina instabile , ( 4 ) rivascolarizzazione miocardica ( pci / cabg )  . 
lanalisi di sopravvivenza stata effettuata per gli eventi totali ( end - point 14 ; major adverse cardiac events [ mace ] e per gli eventi 13 de niti come eventi hard )  . 
le variabili continue , espresse come medie e deviazioni standard ( sd ) , sono state confrontate utilizzando il test t di student a due code e lanalisi della varianza se normalmente distribuite , o mediante il test del chi quadrato ed il kruskal - wallis se non normalmente distribuite . 
le curve degli eventi per lend - point composito ( mace ) e per gli eventi hard ( morte cardiaca , infarto miocardico non fatale ed angina instabile ) sono state confrontate il logrank test . 
gli hazard ratios ( ossia il tasso di eventi / paziente nel tempo ) sono stati calcolati con intervalli di con denza del 95% come una stima del rischio associate con particolari variabili . 
the clinical endpoints were : ( 1 ) cardiac death , ( 2 ) nonfatal myocardial infarction , ( 3 ) ua , and ( 4 ) myocardial revascularisations ( pci ) / cabg ]  . 
 survival analysis was performed for total cardiac events [ endpoints 14 ; major adverse cardiac events ( mace ) ] and for clustered endpoints 13 de ned as hard events . 
 continuous variables , expressed as mean and standard deviation ( sd ) , were compared using the two - tailed t test and analysis of variance ( anova ) if normally distributed or by means of the chi - square and kruskalwallis method if not normally distributed . 
event curves of the composite endpoint ( cardiac death , nonfatal infarction , angina requiring hospitalisation , myocardial revascularisation ; mace ) and hard cardiac events ( cardiac death , nonfatal infarction , ua ) were compared using the log - rank test . 
there were no signi cant differences in terms of mean age ( 63.611.9 years ) , prevalence of men ( n = 75 ; 52% ) , mean bmi ( 26.44.5 ) and heart rate ( 61.19.8 beats / min ) during the ctca scan between the population with and without a history of cad . 
non abbiamo riscontrato differenze signicative in termini di et media ( 63 , 611 , 9 anni ) , prevalenza di maschi ( 75 ; 52% ) , bmi ( 26 , 44 , 5 ) , e frequenza cardiaca ( 61 , 19 , 8 bpm ) durante la scansione ctca , tra la popolazione con e senza storia di malattia coronarica . 
la grande maggioranza dei pazienti si presentava con dolore toracico atipico ( 52 ; 36% ) o altri sintomi come dispnea ( 67 ; 46% ) , mentre solo 26 ( 18% ) pazienti si presentavano con dolore tipico . 
per quanto riguarda la strati cazione del rischio preliminare alla ctca , la maggioranza dei pazienti era a rischio intermedio ( n = 83 ; 57% ) nella popolazione complessiva . 
nel sottogruppo dei pazienti senza storia di cad i pazienti a rischio intermedio erano il 65% ( n = 83 ) ed i pazienti a rischio basso erano il 13% ( n = 16 )  . 
 tutti i pazienti con cad nota sono stati considerati ad alto rischio . table 1 baseline characteristics of overall population , patients without a history of cad and patients with a previous history of cad patients w / o history of cad ( n = 127 ) patients with history of cad ( n = 18 ) clinical characteristics age [ years ; mean ( sd ) ] male gender ( % ) bmi [ kg / m ; mean ( sd ) ] mean heart rate [ bpm ; mean ( sd ) ] follow - up [ months ; mean ( sd ) ] risk factors no . 
in the subgroup without a history of cad , 65% ( n = 83 ) of patients were at intermediate risk , and 13% ( n = 16 ) of patients were at low risk . 
all patients with a history of cad were considered high risk by default . ctca strati cation a total of 127 ( 87.6% ) patients were without a history of cad , and 18 ( 12.4% ) patients had a history of cad . 
signi cant cad ( > 50% luminal narrowing ) was detected in 35 ( 24% ) patients ; nonsigni cant cad ( 50% luminal narrowing ) was detected in 62 ( 43% ) and absence of cad in 48 ( 33% ) patients ( tables 2 and 3 )  . 
the prevalence of obstructive disease , as expected , strati cazione mediante ctca in totale 127 ( 87 , 6% ) pazienti non avevano storia di cad e 18 ( 12 , 4% ) pazienti avevano storia di cad . 
la cad signi cativa ( riduzione del lume > 50% ) stata rilevata in 35 ( 24% ) pazienti ; cad non signi cativa ( riduzione del lume50% ) stata rilevata in 62 ( 43% ) pazienti ed assenza di cad in 48 ( 33% ) pazienti ( tabelle 2 e 3 )  . 
la malattia ostruttiva multi - vasale era presente nell8% ( 12 ) della popolazione totale e prevalentemente distribuita nel sotto - gruppo con storia di cad ( 4 ; 22% )  . follow - up e prognosi abbiamo riscontrato 20 eventi durante un follow - up medio di 203 mesi ; di questi , 4 erano eventi hard e , di questi , 3 morti cardiache ed un infarto miocardico ; gli eventi rimaradiol med ( 2011 ) 116 : 690705 table 2 ctca characteristics of overall population , patients without a history of cad and patients with a previous history of cad patients w / o history of cad ( n = 127 ) patients with history of cad ( n = 18 ) patients absence of cad ( % ) nonobstructive cad ( % ) obstructive cad ( % ) single - vessel disease ( % ) multivessel disease ( % ) obstructive cad in lm / lad ( % ) rca ( % ) lcx ( % ) total agatston cs [ mean ( sd ) ] segments no . 
la maggioranza degli eventi totali erano rivascolarizzazioni ( 16 / 20 ; 80% ) di cui 14 percutanee ( pci ) con stent e 2 bypass aorto - coronarici ( cabg )  . 
sedici eventi ( di cui 3 eventi hard ) si sono veri cati in pazienti senza storia di cad e 4 eventi ( di cui 1 evento hard ) si sono veri cati in pazienti con storia di cad . 
 698 radiol med ( 2011 ) 116 : 690705 table 3 ctca characteristics of overall population , patients without a history of cad and patients with a previous history of cad who experienced a mace during follow - up patients w / o history of cad ( n = 16 ) patients with history of cad ( n = 4 ) patients absence of cad ( % ) nonobstructive cad ( % ) obstructive cad ( % ) single - vessel disease ( % ) multivessel disease ( % ) obstructive cad in lm / lad coronary artery ( % ) rca ( % ) lcx ( % ) agatston score [ mean ( sd ) ] segments no . 
sixteen events ( three hard events ) occurred in patients without a i pazienti sono stati strati cati dalla ctca in coronarie normali ( 48 ; 0 eventi ) , cad non ostruttiva ( 62 ; 6 eventi ) , e cad ostruttiva ( 35 ; 14 eventi ) ; la differenza di prognosi nei tre gruppi risultata sempre signi cativa ( p < 0 , 05 )  . 
un infarto miocardico si veri cato in un paziente con cad ostruttiva . nella popolazione con storia di cad ( n = 127 ) , abbiamo osservato un totale di 16 eventi ( 13 rivascolarizzazioni e 3 eventi hard )  . 
i pazienti sono stati strati cati dalla ctca in coronarie normali ( n = 46 ; 0 eventi ) , cad non ostruttiva ( n = 56 ; 5 eventi ) e cad ostruttiva ( n = 25 ; 11 eventi ) ; la differenza di prognosi nei tre gruppi risultata sempre signi cativa ( p < 0 , 05 )  . 
an acute myocardial infarction occurred in one patient with obstructive cad . in the population without a history of cad ( n = 127 ) , we observed 16 events ( 13 revascularisations and three hard events )  . 
an acute myocardial infarction occurred in a patient with obstructive cad . in the population with a history of cad ( n = 18 ) , we observed four events ( three revascularisations and one hard event )  . 
in multivariate analysis , after adjustment for cardiovascular risk factors , hypercholesterolaemia and obstructive cad were signi cant predictors of events ( p < 0.05 ; table 4 )  . veri cate in pazienti con cad non ostruttiva e 7 in pazienti con cad ostruttiva . 
un infarto miocardico si veri cato in un paziente con cad ostruttiva . nella popolazione con storia di cad ( n = 18 ) , abbiamo osservato un totale di 4 eventi ( 3 rivascolarizzazioni e un evento hard )  . 
i pazienti sono stati strati cati dalla ctca in coronarie normali ( n = 2 ; 0 eventi ) , cad non ostruttiva ( 6 ; 1 eventi ) e cad ostruttiva ( n = 10 ; 3 eventi ) ; la differenza di prognosi nei 3 gruppi non risultata signi cativa a causa del basso numero di pazienti ( p > 0 , 05 )  . 
 nellanalisi multi - variata , dopo correzione per i fattori di rischio cardiovascolari factors , liper - colesterolemia e la cad ostruttiva sono risultati predittore signi cativi di eventi ( p < 0 , 05 ; tabella 4 )  . discussione il nostro studio dimostra che la ctca in grado di strati care in modo af dabile il rischio di eventi cardiovascolari in un follow - up a medio termine in pazienti con acp . 
 la frequenza di eventi cardiaci era signi cativamente pi elevata nei pazienti con cad ostruttiva quando confrontata con i pazienti con cad non ostruttiva , sia per quanto riguarda le rivascolarizzazioni sia per quanto riguarda gli eventi hard . 
the rate of events was signi cantly higher in patients with a known lanalisi multi - variata ha mostrato come gli unici predittori indipendenti di mace erano la presenza di ipercolesterolemia e di cad ostruttiva . 
altri predittori come il calcium score , il diabete mellito , e cos via , non sono emersi probabilmente a causa dei numeri relativamente bassi e del follow - up relativamente breve . 
acute chest pain represented 510% of patients accessing the er ; of those 7080% were classi ed as having nonanginal pain , 78% as having acute coronary syndrome and up to 78% as having nstemi and / or ua [ 21 , 22 ]  . 
the clinical classication between nonanginal chest pain and nstemi / ua is not always easy and sharp , and in such patients , ruling - out strategies may be more effective . 
decision making for patients in this cohort has important consequences at two levels : inappropriate hospital admission resulting in increased costs , and inappropriate discharge resulting in increased risk of cardiac events . 
the requirements for further testing are : simple and fast , reliable and able to detect / exclude signi cant cad and other major cardiothoracic sources of chest paa test with these features may allow us to reduce costs and mistakes / liability and may increase patient satisfaction [ 2124 ]  . it is known from previous studies based on cag that cad severity is an independent prognostic predictor [ 3 , 816 ]  . 
 [ 8 ] con rmed these ndings in a larger patient group ( n = 187 ) without known cad with a longer follow - up ( 20 months )  . 
in that study , the presence of signi cant cad and the extent of cad , de ned by a modi ed duke coronary artery score , were predictors of all - cause mortality [ 14 ]  . 
 [ 12 ] analysed 517 patients with suspected cad who underwent both myocardial perfusion scintigraphy ( mpi ) and ctca and reported an annualised event rate of 4.8% in patients 5%10% dei pazienti che accedono al pronto soccorso ; di questi il 70%80% vengono classi cati come dolore non anginoso , il 7%8% sono classi cati come sindrome coronarica acuta e no al 7%8% vengono classi cati come nstemi e / o ua [ 21 , 22 ]  . 
la distinzione clinica tra dolore toracico non anginoso e nstemi / ua non sempre facile e nitida , e questa una popolazione nella quale le strategie di esclusione ( rule - out ) possono risultare pi ef caci . 
lalgoritmo decisionale in questa coorte ha delle importanti ricadute a due livelli : ricoveri inappropriati che generano aumento dei costi , e dimissioni inappropriate che determinano un aumento del rischio di eventi cardiovascolari . 
i requisiti per ulteriori test sono : semplice e veloce , af dabile , capacit di rilevare e / o escludere cad signi cativa e altre cause cardio - toraciche maggiori di dolore toracico . 
un test con queste propriet potrebbe consentire una riduzione dei costi , degli errori / responsabilit , e potrebbe anche incrementare la soddisfazione dei pazienti [ 2124 ]  . noto da studi precedenti basati sulla cag che la severit della cad un predittore prognostico indipendente [ 3 , 816 ]  . 
 [ 11 ] hanno riportato , in una casistica di 100 pazienti con e senza cad nota , il valore prognostico della ctca ad un anno [ 11 ]  . 
 [ 8 ] hanno confermato queste osservazioni in una popolazione pi ampia ( n = 187 ) senza storia di cad e con un follow - up pi lungo ( 20 mesi )  . 
in questo studio , la presenza di cad ostruttiva e lestensione della cad , de nite mediante uno score coronarico modi cato di duke sono risultati predittore indipendenti per tutte le cause di morte [ 14 ]  . 
 [ 12 ] hanno analizzato 517 pazienti sottoposti a scintigra a miocardica da stress ( mpi ) e ctca con sospetta cad e hanno rilevato frequenza di eventi per anno di 4 , 8% nei pazienti con cad ostruttiva alla ctca e di 1 , 8% nei pazienti con cad moderata o assente . 
 [ 30 ] assessed the prognostic value of 64 - slice ctca in 220 patients with known or suspected cad during a mean follow - up of 144 months [ 30 ]  . 
at 1 year , patients with cad had a 34% event rate , whereas patients with normal coronary arteries had a cardiac event rate of 0% [ 30 ]  . 
in our study , we considered mace and hard events separately , because the rate of cardiac revascularisations during follow - up could be signi cantly in uenced by ctca results . 
short - term ( 30 days ) follow - up in patients with nonsigni cant cad ( as detected by ctca ) was extremely favourable . prognostic studies are important to determine whether patients in whom ctca rules out obstructive cad can be reassured and invasive coronary angiography can be safely avoided . 
in our study , patients without coronary atherosclerosis had an excellent prognosis ( 0% cardiac event rate at 20 months ) , thus con rming the high npv of ctca at follow - up . 
 study limitations the main limitation of our study is that the number of clinical events at follow - up is relatively low ( in particular , for the subgroup with a history of cad ) due to the population characteristics ( population at low to intermediate cardiovascular risk ) and to the relatively short follow - up . 
we included patients with both suspected and known cad , as usually encountered in clinical practice ; however , the proportion of patients with previous acute myocardial infarction or pci was limited ( 12% )  . 
nevertheless , at multivariate analysis , a history of cad was not an independent predictor . high radiation exposure in ctca with retrospective gating is still a matter a concern [ 3137 ]  . 
therefore , ad un anno , i pazienti con presenza di cad avevano una frequenza di eventi del 34% , mentre i pazienti con coronarie normali hanno mostrato 0 eventi [ 30 ]  . 
nel nostro studio abbiamo considerato i mace e gli eventi hard separatamente , poich la frequenza di rivascolarizzazioni coronariche durante il follow - up pu essere signi cativamente in uenzata dai risultati della ctca . 
il follow - up a breve termine ( 30 giorni ) nei pazienti con cad non signi cativa ( alla ctca ) risultato estremamente favorevole . gli studi prognostici sono importanti per determinare se i pazienti nei quali la ctca esclude la cad ostruttiva possono essere rassicurati ed possibile evitare una coronarogra a invasiva . 
nel nostro studio , i pazienti senza aterosclerosi coronarica hanno dimostrato una prognosi eccellente ( frequenza di eventi a 20 mesi pari a 0% ) , confermando lelevato valore predittivo negativo della ctca anche al follow - up . 
 limitazioni dello studio la principale limitazione dello studio consiste nel numero relativamente basso di eventi clinici al follow - up ( in particolare nel gruppo con storia di cad ) , causato dalle caratteristiche della popolazione ( popolazione a rischio bassointermedio ) , e follow - up relativamente breve . 
abbiamo incluso pazienti con cad nota e sospetta nel nostro studio , come accade di osservare nella pratica clinica , tuttavia la proporzione di pazienti con precedente ami o pci era ridotta ( 12% )  . 
in ragione delleterogeneit della popolazione e del numero relativamente basso di eventi , non abbiamo effettuato analisi sullassociazione tra la sede e le caratteristiche delle placche coronariche e la frequenza di eventi . 
tuttavia , allanalisi multi - variata la storia di cad allanalisi multi - variata non risultato un predittore indipendente . la dose di radiazioni elevate della ctca con gating ecg retrospettivo rimane un problema della metodica [ 3137 ]  . 
pertanto il bene cio dellutilizzo della ctca nel 704 radiol med ( 2011 ) 116 : 690705 the bene t of using ctca in the diagnostic workup must be counterbalanced by the possible risks related to radiation exposure . 
recently , a dose - modulation algorithm that reduces tube current by 80% during the systolic phase , and prospective ecg - triggering protocols , have been developed that allow a signi cant reduction of radiation exposure , down to 15 msv , with preserved diagnostic accuracy [ 3137 ]  . 
recentemente , sono stati sviluppati degli algoritmi di modulazione della dose di radiazioni che riducono la corrente del tubo dell80% durante la fase sistolica e dei protocolli di scansione prospettica basati sullecg che consentono una riduzione della dose no a 15 msv con accuratezza diagnostica preservata [ 3137 ]  . 
 conclusions conclusioni this study shows that ctca is able to reliably identify coronary atherosclerotic burden and to stratify cardiovascular risk at follow - up in patients with acp and suspected or known cad . 
bchler published online : 17 june 2011 springer - verlag 2011 dear editor : prognostic value of loss of wall enhancement for bowel infarction school of medicine , ponti cia universidad catlica , lira 44 , santiago , chile correspondence to : p . 
the study stated that loss of bowel wall enhancement was predictive of good outcome in patients with bowel infarction . i believe that a methodological mistake could have led moschetta and colleagues to wrong conclusions . 
a general rule of thumb is to use the fisher test when either the sample size is less than 30 or the expected number of observations in any cell of a 22 contingency table is less than ve [ 2 ]  . i performed the fisher exact test with the data published in table 3 and found a signi cant association with the patient outcome ( dead or alive ) in three out of ten signs evaluated ( wall thickening , intramural pneumatosis and pneumoperitoneum ) , instead of nine reported by the authors . 
the chi - square test showed an approximate p - value of 0.3 ( p = 0.260 ) rather than a p - value of 0.03 , as it is reported in the article . 
1 , east jian she road , zhengzhou , 450052 henan province , pr china correspondence to : x - w han , tel . : + 86 - 0371 - 65165352 , fax : + 86 - 0371 - 66971086 , e - mail : hanxinwei@tom.com. received : 28 april 2010 / accepted : 14 june 2010 / published online : 19 march 2011 springer - verlag 2011 abstract purpose . 
sono stati trattati consecutivamente con sems integrati a y otto pazienti con ostruzioni anastomotiche complesse che coinvolgevano lansa afferente ed efferente dopo gastro - digiuno - anastomosi ( billroth ii )  . 
in base al sistema di punteggio dellostruzione delloutlet gastrico ( gooss ) , il miglioramento in seguito allintervento stato statisticamente signi cativo ( p = 0 , 01 )  . 
durante il followup di 3 , 131 , 81 mesi , tutte le stenosi si sono risolte senza complicanze correlate allo stent e si osservato un miglioramento clinico in tutti gli otto pazienti . 
la media e la mediana dei periodi di sopravvivenza 760 radiol med ( 2011 ) 116 : 759765 proved to be an expedient , simple , safe and minimally invasive procedure for treating complex anastomotic stenoses after gastrojejunostomy ( billroth ii )  . keywords billroth ii stent anastomosis obstruction introduction over the last decade , self - expandable metallic stents ( sems ) have been utilised with increasing frequency in patients with gastric outlet obstruction ( goo ) , providing simple , safe and effective palliation [ 14 ]  . 
the use of an integrated y - sems , which is inserted under uoroscopic or endoscopic monitoring , has not been reported in the literature , with the exception of reports of a y - shaped stent that utilised two sems [ 513 ]  . 
during 2009 , we designed an integrated y - shaped sems ( microtech , nanjing , china ) specialised for patients with multiple anastomotic strictures after gastrojejunostomy ( billroth ii )  . 
 therefore , the purpose of this study was to report our initial experience with an integrated y - sems for patients with complex strictures after billroth ii . materials and methods patients this study was approved by the university committee on human investigation , and informed consent was obtained from each patient . 
from april 2009 to december 2009 , eight patients ( 3876 years , mean age 58.7511.17 years , six men , two women ) who suffered from complex stenoses involving both the afferent and efferent loops were treated with an integrated y - shaped sems ( micro - tech )  . 
il posizionamento di un sems a y integrato si dimostrato semplice , sicuro , minimamente invasivo ed adeguato al trattamento di stenosi anastomotiche complesse dopo gastro - digiuno - anastomosi ( billroth ii )  . parole chiave billroth ii stent anastomosi ostruzione by the interventional radiologist according to the multidetector ct or barium study . stent and delivery system the integrated , self - expandable , y - shaped , metallic stent was woven from threads of 0.24 - mm - diameter highly elastic nitinol ( nickel titanium , naval ordnance laboratory ) wire and consisted of three parts : body , afferent limb and efferent limb , as shown in figure 1 . 
the two limbs were also in a tubular con guration ( 22 mm in diameter , 2080 mm in length , respectively , depending on the patients afferent and efferent size )  . 
indication for use of the inverted y - stent included multiple stenoses or stula near the anastomosis and afferent and the efferent loops . the delivery system was a three - tier - structure y - stent delivery system , and the details of the delivery system have been previously described [ 14 , 15 ]  . 
the longer tubes are long at the proximal end and short at the distal end , whereas the shorter tubes are short at the proximal and long at the distal end . 
the body of the two shorter guiding tubes is also located in the pusher catheter , and the tails extend out of the back of the pusher catheter by about 5 cthe two bronchial stents are bound by two binding threads and xed at the proximal end of the two longer guiding tubes . 
finally , the outer tier is a 27 f ( 9 mm ) - diameter introducer sheath with a radiopaque marker ring at its proximal end and a lateral tube for ventilation at the distal end . 
the patient was placed in a right anterior oblique or supine position with the neck extended , and stenosis was identi ed by an injection of 2050 ml of 30% diluted nonionic contrast medium ( ultravist 300 ; schering , guangzhou , china )  . 
two guide wires ( radiofocus m ; terumo , tokyo , japan ) were inserted into the afferent and efferent loops and were exchanged using catheters ( torcon nb ; cook , bloomington , in , usa ) for two 0.035 - superstiff guidewires ( thsf ; cook , bloomington , in , usa )  . 
c withdrawal of the sheath over the pusher catheter and deployment of the stent while pushing the inverted y - stent to the anastomotic area and the two limbs of the stent into the afferent and efferent loops . 
contrast medium was injected through the catheter into the tracheal stent to assess correct sten placement and expansion . follow - up and evaluation of postoperative outcome a follow - up contrast swallow ( ultravist ) was obtained to evaluate stent patency and migration or expansion 37 days following placement . 
the follow - up protocols were performed at 1 , 3 , 6 and 12 months and annually after by one of the two authors and included a clinical and barium study . 
if follow - up at the outpatient clinic was not practical , patients or their families were contacted by telephone by one of the two authors every 1 or 2 months until the patient died . 
 technical success was de ned as successful stent insertion in the targeted position and the con rmation of patency using a combination of endoscopy and uoroscopy with oral contrast mediuclinical success was de ned as improvement in the obstructive symptoms and oral intake without vomiting 17 days after stent placement . 
the degree of dysphagia was assessed before and after stent placement using an adaptation of the goo scoring system ( gooss ) proposed by adler and baron [ 16 ] , with swallowing ability divided into four categories : 0 no oral intake ; 1 liquids only ; 2 soft solids ; 3 low - residue or full diet . statistical analysis data are presented as mean standard deviation . 
statistical analyses were performed using spss statistical software ( version 10.0 for windows , spss inc . , chicago , il , usa ) ; p < 0.05 was considered statistically signi cant . results technical and initial clinical results stent placement in the anastomotic areas was technically successful and well tolerated in all patients , with no procedure - related complications . 
five patients continued with follow - up health care after the procedures ; the remaining three died of the following causes unrelated to stent insertion : multiple organ failure ( n = 2 ) , diffuse metastasis ( n = 1 )  . 
to date , this is the rst report to describe treatment of multiple anastomotic obstructions after gastrojejunostomy with the use of an integrated y - shaped sems . local recurrence that causes obstruction occurs in approximately 20% of patients after gastrectomy for gastric carcinoma , with or without distant metastasis [ 17 , 18 ]  . 
most of these recurrent tumours are unsuitable for further resective or palliative surgery because of advanced malignancy , poor patient performance status or malnutrition and a high risk of signi cant morbidity and mortality rates [ 19 , 20 ]  . 
when the stenoses exist in the anastomotic area involving the afferent and efferent loops after gastrojejunostomy , a y - stent is often required for 764 radiol med ( 2011 ) 116 : 759765 successful palliation . 
the insertion of a y - stent created by two straight stents , on the one hand , did not t the characteristic of the anastomosis and , on the other hand , could not provide long - term patency of anastomosis due to interference of the stent threads , which resulted in early reobstructions [ 5 , 13 ]  . 
except for our previously designed integrated y - shaped sems and delivery system for treating complex stenoses or stulas in the carinal region , no other report was found in the literature regarding deployment techniques of the integrated y - shaped sems . 
 due to the different structure between the carinal area and the anastomosis after gastrojejunostomy , we devised another integrated yshaped sems specialised for patients with multiple anastomotic strictures after gastrojejunostomy . 
all patients in our study were successfully implanted with the integrated y - shaped sems . compared with the y - stent created by two straight stents , the integrated y - shaped sems has several distinct advantages : it is more suitable for the anatomy of the anastomosis , which provides long - term anastomosis patency and has less in uence on the function of the small bowel ; it is not prone to migration due to the interconnection of the body and the two limbs ; the procedure is relatively simple and rapid due to deployment of one integrated y - shaped sems with one procedure ; the stent can be retrieved easily . this study has the following limitations . 
second , application of the integrated y - shaped sems was not possible in some cases , when in anastomosis , the afferent and efferent loops were completely obstructed and dif cult to recanalise with the guidewire and the catheter . 
fundamentals and technical aspects springer - verlag , new york dordrecht heidelberg london , 2010 isbn 978 - 1 - 4419 - 6520 - 2 ( soft cover ) isbn 978 - 0 - 387 - 73506 - 1 ( hard cover ) e - isbn 978 - 1 - 4419 - 6521 - 9 doi 10.1007 / 978 - 1 - 4419 - 6521 - 9 published online : 8 march 2011 springer - verlag 2011 in this pocket - size , soft cover 241 page book ( hard cover edition published in 2008 ) prof . 
hendrick shares all his experience and knowledge he has gathered over the years as a researcher and teacher in the eld of breast magnetic resonance imaging ( mri )  . the topic is not so simple , yet the way it is addressed ( one - on - one teacher - student approach ) offers a continuous exchange of knowledge between the teacher and pupil driving to the expected mastering of the subject matter . starting from the fundamentals of magnetic resonance breast imaging one is taken through all its different modalities and sequences , learning how to use these and how mri works . 
 the author refers to the mathematically inclined reader in order to help him properly understand some of the presented sometimes at large formulas ; i would also include the physics inclined reader since without this sort of inclination and knowledge one would sometimes get lost . the book will be greatly appreciated by all those who are dealing with breast mri due to its more and more widespread use and its importance in the clinical and diagnostic setting . 
the less than 10 minute procedure time , due to the use of updated , and even dedicated , scanners and proposed protocols , makes breast mri competitive and offers more information ( just to quote the perfusion curves ) than mammography . in questo volumetto in brossura di 241 pagine dalle dimensioni tascabili ( ledizione con copertina rigida stata pubblicata nel 2008 ) , il prof . 
hendrick mette a disposizione del lettore tutta la sua esperienza e conoscenza accumulata nel corso degli anni come ricercatore ed insegnante nel campo della risonanza magnetica ( rm ) della mammella . largomento non dei pi semplici eppure limpostazione della sua esposizione , con un approccio viso a viso insegnante - studente , offre un continuo scambio di conoscenze tra il maestro e lallievo in modo tale da far raggiungere la padronanza voluta dellargomento . 
 iniziando dalle basi dello studio per immagini con risonanza magnetica della mammella , il lettore viene guidato attraverso le sue varie modalit e sequenze , imparando come usarle e , soprattutto , come funziona la rm . 
 lautore fa riferimento a quello che de nisce lettore incline alla matematica per aiutarlo a comprendere in modo adeguato alcune delle formule utilizzate ( talvolta in modo eccessivo ) ; da parte mia aggiungerei anche al lettore incline alla sica poich senza questa inclinazione e conoscenza lo stesso si troverebbe talvolta perso . questo libro sar di sicuro apprezzato da tutti coloro che hanno a che fare con la rm della mammella , visto il sempre pi ampio uso della stessa e la sua importanza nel campo clinico e diagnostico . 
il tempo di indagine inferiore ai 10 minuti , in funzione delluso di attrezzature sempre pi aggiornate , se non propriamente dedicate , nonch i protocolli proposti , rendono la rm della mammella competitiva , offrendo anche maggiori informazioni ( basti pensare alle curve di perfusione ) rispetto alla mammogra a . 824 radiol med ( 2011 ) 116 : 823824 a practical drawback : the way the book is bound makes reading it dif cult ( unless one wants to split open its spine )  . un unico inconveniente : la rilegatura del libro ne rende la lettura dif cile ( salvo il volerne rompere il dorso per facilitarla )  . 
mandale springer , new york heidelberg dordrecht london , 2010 isbn : 978 - 1 - 4419 - 1727 - 0 e - isbn : 978 - 1 - 4419 - 1728 - 7 doi 10.1007 / 978 - 1 - 4419 - 1728 - 7 published online : 8 march 2011 springer - verlag 2011 this book is a review crib and targets the radiologists - intraining preparing for their oral board exam in the usa . 
it encompasses a variety of cases simple as well as dif cult or unusual ones which should and could be of practical use not only to the student but also to the radiologist in the mammographic daily diagnostic work ow . there are 240 pages divided into two parts : the rst and largest reviews 79 mammography and ultrasound cases ; the second 13 magnetic resonance imaging ( mri ) cases . 
an appendix on interventional procedures and high yield facts and a very tight index closes the book . a few pages , at the beginning of each section , deal with mammographic and mri artefacts . each case is presented following a xed framework which presents on one page the patient history , radiology ndings , assessment ( breast imaging reporting and data system [ birads ] whenever possible ) , diagnosis , discussion and references ( no more than ve , usually two , to help the reader widen is the basic knowledge , just in case he / she wants to )  . 
 on the facing page , or sometimes the following page / s , well chosen and carefully reproduced x - ray images , ( coupled with ultrasonography [ us ] , mri and sometimes kinetic curves ) are displayed so making easy to simplify the comparison of clinical data and reported radiological ndings . since the book was supposed to be an aid for the board examination preparation , cases are organized in a random way , as the candidate would nd during his / her oral examination . 
in the same way , case reports and discussions are presented as a report would be written , presenting clinical data , differential diagnoses , possible outcome for the patient etc . 
in this way bi - rads assessment is important and one will nd its categories explained in the appendix . questo volume da considerasi un bigino di revisione rivolto agli specializzandi in radiologia in vista della loro preparazione per gli esami di abilitazione ( board ) negli stati uniti . 
esso comprende una variat di casi , dai semplici ai dif cili ai non comuni , che potrebbero essere di utilit non solo allo studente ma anche al radiologo nello svolgimento del lavoro mammogra co giornaliero . il volume consiste di 240 pagine ed diviso in due parti : la prima e pi consistente rivede 79 casi di mammogra e ed eco - mammogra e ; la seconda 13 casi studiati con risonanza magnetica ( rm )  . 
a chiusura del volume si trova unappendice sulle procedure interventistiche , su dati diagnostici importanti ed un indice analitico coinciso . allinizio di ciascuna parte alcune pagine sono dedicate agli artefatti sia mammogra ci che rm . 
ciascun caso presentato secondo uno schema sso e cio su di una pagina la storia del paziente , i riscontri radiologici , la valutazione ( breast imaging reporting and data system [ bi - rads ] quando possibile ) , la diagnosi , la discussione ed i riferimenti bibliogra ci ( non pi di cinque , di solito due , concepiti come un aiuto ad ampliare le conoscenze di base del lettore , sempre che lui / lei lo voglia )  . sulla pagina a fronte , talvolta sulla / e successiva / e vengono presentate immagini radiologiche ben scelte e riprodotte con cura , corredate da immagini ecogra che , rm e talvolta da curve cinetiche , in modo tale da rendere facile il confronto tra i dati clinici ed i reperti radiologici descritti . 
 dal momento che il volume stato concepito come un aiuto nella preparazione dellesame di abilitazione , i casi sono stati organizzati in modo casuale , tale e quale a quello che il candidato / a troverebbe nel suo esame orale . 
nello stesso modo i reperti e le discussioni sono presentati in maniera analoga a quella in cui un referto dovrebbe essere scritto , descrivendo i dati clinici , le diagnosi differenziali , le possibilit prognostiche per il paziente ecc . 
da questo punto di vista la valutazione bi - rads importante e la descrizione dei vari punti di tale classi cazione riportata nellappendice . in conclusione , questo libro raccomandato agli specia828 radiol med ( 2011 ) 116 : 827828 in conclusion , this book is recommended for trainees in radiology who will approach the dif culties of mammography , not only in view of an examination , but also on practical diagnostic grounds . 
as well it will be useful for grownups and experts and it should be kept on hand in every mammography diagnostic unit . lizzandi in radiologia che dovranno affrontare le dif colt insite nella mammogra a , non solo in funzione di un esame ma , soprattutto , in campo diagnostico pratico . 
simonetti department of diagnostic imaging , molecular imaging , interventional radiology and radiation therapy , policlinico tor vergata , viale oxford 81 , 00133 roma , italy correspondence to : g . 
sixty - four - slice ct coronary angiography provides accurate three - dimensional evaluation of the coronary artery tree with correct visualisation of any coronary anomalies , a relatively common nding that had a prevalence of 5.7% in our study population . 
la tc volumetrica consente unaccurata valutazione tridimensionale del circolo coronarico con visualizzazione delle anomalie coronariche che rappresentano un reperto relativamente comune nella popolazione con prevalenza del 5 , 7% . keywords coronary anomalies ct anatomical variants congenital anomalies parole chiave anomalie coronariche tc coronarica varianti anatomiche anomalie congenite 676 introduction visualisation of the coronary arteries has always constituted a challenge for diagnostic imaging because of their rapid movement during the cardiac cycle and the small size , tortuous course and intrinsic anatomical variability of the cardiac vessels . 
since the early 1990s , increasingly sophisticated technologies have been introduced in coronary diagnostics in an attempt to replace conventional coronary angiography ( ca ) , with the result that cardiac imaging has become a daily problem in routine clinical practice . 
over the past 10 years , multislice ct ( msct ) , especially after the advent of 64 - slice equipment , has rapidly gained credibility for the quality of results and reproducibility in the morphological evaluation of the coronary arteries [ 912 ]  . 
one of the strengths of ctca lies in its ability to provide a three - dimensional visualisation of the epicardial vessels [ 13 ]  . coronary artery anomalies are present at birth , but only a minority of them become manifest during the early years of life . 
nonetheless , some coronary anomalies may manifest with angina pectoris , infarction , syncope , more - or - less severe myocardial arrhythmias or even cardiac arrest and sudden death . 
the indications for the examination were several and included screening for coronary disease in asymptomatic and symptomatic patients , follow - up of patients previously treated with coronary stent or bypass , further investigation following ca or myocardial scintigraphy , electrocardiogram ( ecg ) abnormalities and follow - up of patients after ascending aorta or valve - replacement surgery . 
patients unable to radiol med ( 2011 ) 116 : 675689 introduzione la visualizzazione delle arterie coronarie ha sempre rappresentato una s da per la diagnostica non solo per il loro rapido movimento durante il ciclo cardiaco , ma anche per il calibro ridotto , il decorso tortuoso e lintrinseca variabilit anatomica nella vascolarizzazione cardiaca . 
dallinizio degli anni novanta , diverse tecnologie sempre pi avanzate e alternative alla coronarogra a , si sono affacciate sulla scena della diagnostica delle patologie coronariche , rendendo limaging cardiaco un problema quotidiano nella normale pratica clinica . 
nel corso dellultimo decennio la tomogra a computerizzata multistrato ( tcms ) , soprattutto dopo lintroduzione delle apparecchiature a 64 strati , ha rapidamente guadagnato credibilit per la qualit dei risultati ottenuti e per la riproducibilit nella valutazione morfologica delle arterie coronarie [ 912 ]  . 
uno dei punti di forza dellangio - tc delle coronarie consiste nella capacit di visualizzare in modo tridimensionale lanatomia dei vasi epicardici [ 13 ]  . le anomalie coronariche sono presenti dalla nascita , ma solo una piccola percentuale di esse si rende manifesta nei primi anni di vita . 
tuttavia alcune di esse possono presentarsi con angina pectoris , infarto miocardico , sincope , aritmie pi o meno severe o addirittura arresto cardiaco con gurando il quadro di morte improvvisa . 
in letteratura esistono prevalentemente descrizioni di anomalie coronariche basate sullangiogra a coronarica mentre sono poche quelle basate sulla tcms che presentano peraltro casistiche ridotte o popolazioni di studio gi molto selezionate [ 1417 ]  . 
lo scopo di questo lavoro quello di fornire la prevalenza di varianti e anomalie coronariche in unampia popolazione di pazienti sottoposti ad angiogra a coronarica con tcms a 64 strati . 
 materiali e metodi popolazione in esame da marzo 2005 ad agosto 2009 sono state eseguite 3236 angio - tc diagnostiche delle coronarie su 2133 maschi e 1103 femmine con et compresa tra 1884 anni ( et media 57 , 48 , 3 )  . 
la popolazione in studio eseguiva lesame secondo indicazioni estremamente varie : screening di malattia coronarica in pazienti asintomatici e sintomatici , follow - up in pazienti precedentemente trattati con stent coronarico o bypass , controllo indirizzato dallangiogra a coronarica o dalla scintigra a miocardica , anomalie in pazienti allelettrocardiogramma ( ecg ) , follow - up radiol med ( 2011 ) 116 : 675689 hold their breath for at least 1012 s were also excluded . 
our departments ethics committee gave its approval for the study protocol , and all patients underwent ct imaging after providing their signed informed consent . patient preparation patients with a heart rate > 70 bpm received premedication with oral beta - blockers 45 days before the ct examination . 
patients who continued to have a heart rate between 70 and 80 bpm were given beta - blockers ( 100 mg metoprolol tartrate orally 4550 min prior to the study or 550 mg metoprolol tartrate 1015 min before the study ) under close cardiological monitoring of heart rate and arterial blood pressure , together with benzodiazepines if necessary ( diazepam 12 mg per os 15 min before the examination )  . 
 premedication was only administered to patients who did not have speci c contraindications to the premedication drugs . scan protocol and image reconstruction the msct study was performed using a 64 - slice scanner ( lightspeed 64 ct , ge medical systems , milwaukee , wi , usa )  . 
scan parameters were as follows : axial thickness 2.5 mm ; eight images per rotation ; rotation time 0.35 s ; tube voltage 120 kv ; tube current 300 ma ; dedicated convolution kernel for the calcium score . 
the scan parameters of the postcontrast phase were slice thickness 0.625 mm ; interval 0.625 mm ; rotation time 0.35 s ; tube voltage 120 kv ; tube current 700900 ma for scans with retrospective gating and 400600 ma for those with prospective gating . 
a dose of 100 ml of iodinated contrast material ( 400 mgi / ml , iomeprol , iomeron 400 , bracco , milan , italy ) was administered as a rapid bolus at 5 ml / s , followed by 30 ml of saline solution at the same ow rate . 
contrast material was administered through an automatic injector ( stellant , medrad , pittsburgh , pa , usa ) connected to a 20 - gauge cannula previously placed in an antecubital vein of the right arto optimise opaci cation of the coronary vessels , the smart prep function was used . 
retrospective reconstructions were obtained , as needed , in different phases of the cardiac cycle ( 3090% , 510% increments )  . precedentemente operati allaorta ascendente o di sostituzione valvolare . 
non sono stati inclusi nello studio pazienti con controindicazioni assolute allesecuzione dellesame come : insuf cienza renale , distiroidismi , allergia documentata al mezzo di contrasto organo - iodato , gravidanza . 
il comitato etico del nostro dipartimento ha approvato il protocollo di studio e tutti i pazienti si sono sottoposti allesame dopo aver rmato un consenso informato . preparazione del paziente i pazienti con frequenza cardiaca superiore ai 70 bpm sono stati premedicati con beta - bloccanti per os 45 giorni prima dellesame . 
nei pazienti che continuavano ad avere una frequenza cardiaca compresa tra 7080 bpm si provveduto , sotto videat cardiologico con stretto monitoraggio di frequenza cardiaca e pressione arteriosa , alla somministrazione di beta - bloccanti ( 100 mg di metaprololo tartrato per os 4550 minuti prima dellesame ovvero 550 mg di metoprololo tartrato 1015 minuti prima dellesecuzione dellesame ) e alloccorrenza con benzodiazepine ( diazepam , 12 mg per os 15 minuti prima dellesecuzione dellesame )  . 
sono stati sottoposti a premedicazione solo i soggetti che non presentavano controindicazioni speci che alla somministrazione dei farmaci sopradescritti . protocollo di scansione e ricostruzione delle immagini lo studio tcms stato eseguito con scanner a 64 strati ( lightspeed 64 ct ; ge medical systems , milwaukee , wi , usa )  . 
i parametri utilizzati per la prima scansione sono stati i seguenti : spessore assiale 2 , 5 mm , 8 immagini per rotazione , tempo di rotazione 0 , 35 secondi , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 300 ma , ltro di convoluzione dedicato per il calcium score . 
 lacquisizione con somministrazione di mezzo di contrasto stata effettuata in 2475 pazienti con gating restrospettivo , mentre nei restanti pazienti che presentavano una frequenza cardiaca stabilmente al di sotto dei 60 battiti al minuto stato utilizzato un gating prospettico per ridurre la dose di radiazioni ionizzanti somministrata . 
i parametri di scansione della fase contrastogra ca sono stati : spessore elicoidale 0 , 625 mm , intervallo 0 , 625 mm , tempo di rotazione 0 , 35 secondi , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 700900 ma per le acquisizioni con gating retrospettivo , 400600 ma per quelle con gating prospettico . 
sono stati somministrati 100 678 data collection and statistical analysis three observers with 7 years experience with cardiac ct interpreted the examinations and compared their results to reach a diagnostic consensus . 
the 3 , 236 examinations were analysed on a dedicated workstation ( general electric advantage workstation 4.4 , healthcare , waukesha , wi , usa ) using a variety of postprocessing algorithms . 
for each examination , the following reconstructions were obtained : maximum intensity projections ( mip ) , multiplanar reconstructions ( mpr ) , curved mpr , volume rendering ( vr ) and , when needed , advanced vascular analysis ( ava ) and cardiac transparency images to facilitate viewing the coronary anatomy and identify all segments of the coronary tree . 
 the images were assessed for the following parameters : coronary dominance ( right , left , balanced ) ; anatomical variants : presence of intermediate branch , presence and number of diagonal and marginal branches ; coronary anomalies , subdivided anatomically into anomalies of origin and course , intrinsic coronary anomalies and termination anomalies . results are expressed as prevalence in absolute number and percentage of all anomalies identi ed and all ndings reported . results of the 3 , 236 patients , 2 , 851 ( 88.1% ) had right dominance , 275 ( 8.5% ) had left dominance and 110 ( 3.4% ) had balanced , codominant distribution ( table 1 )  . 
marginal branches had a very similar distribution : 51% of patients ( n = 1650 ) had at least one , 41.1% ( n = 1329 ) had two , 6% ( n = 194 ) had more than two and 1.9% ( n = 63 ) had none ( table 1 )  . the number of coronary anomalies amounted to 224 in 186 patients , given that 37 patients had more than one anomaly ( 36 had two ; one had three )  . 
the 89 anomalies of origin and course included : 24 anomalous origins of the right coronary artery ( rca ) , of which eight arose from the ascending aorta , eight radiol med ( 2011 ) 116 : 675689 ml di mezzo di contrasto iodato ( 400 mgi / ml , iomeprol , iomeron 400 , bracco , milano ) in bolo rapido a 5 ml / s , seguiti da un bolo di 30 ml di soluzione siologica alla stessa velocit . 
la somministrazione avvenuta tramite iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 20 gauge preventivamente posizionata in una vena antecubitale del braccio destro . 
sono state effettuate alloccorrenza ricostruzioni retrospettive in diverse fasi del ciclo cardiaco ( 30%90% , incremento di 5%10% )  . raccolta dati e analisi statistica tre osservatori con unesperienza quotidiana in cardio - tc di 7 anni hanno visualizzato gli esami ottenuti e i singoli risultati sono stati confrontati per ottenere una concordanza diagnostica . 
sono state eseguite per ogni esame ricostruzioni maximun intensity projection ( mip ) , ricostruzioni multiplanari ( mpr ) , mpr - curved , volume rendering ( vr ) e alloccorrenza , advanced vascular analysis ( ava ) e immagini di trasparenza cardiaca , al ne di facilitare la visualizzazione dellanatomia coronarica e identi care la totalit dei segmenti dellalbero coronarico . 
sono stati quindi valutati i seguenti parametri : il bilanciamento della vascolarizzazione ( dominanza coronaria destra , sinistra , bilanciata ) ; le varianti anatomiche : presenza di ramo intermedio , presenza e numero dei rami diagonali e marginali ; le anomalie coronariche , suddividendole sulla base della classi cazione anatomica in : anomalie di origine e decorso , intrinseche della coronaria stessa e di terminazione . i risultati sono stati espressi come prevalenza in numero assoluto , percentuale sul totale delle anomalie riscontrate e sul totale dei reperti descritti . risultati dei 3236 pazienti studiati in 2851 , pari all88 , 1% , la dominanza della vascolarizzazione risultata destra , in 275 sinistra ( 8 , 5% ) ed in 110 bilanciata ( 3 , 4% ) ( tabella 1 )  . 
i dati riguardanti i principali rami marginali sono estremamente simili ai precedenti : il 51% dei soggetti ( n = 1650 ) ne presenta almeno uno , il 41 , 1% ( n = 1329 ) due , il 6% ( n = 194 ) pi di due e nell1 , 9% della popolazione in esame ( n = 63 ) non stato possibile visualizzarne neanche uno ( tabella 1 )  . le anomalie coronariche riscontrate nel nostro studio sono risultate 224 in 186 soggetti , in quanto 37 pazienti erano portatori di pi di unanomalia ( 36 pazienti ne presentavano due , 1 ne presentava tre )  . 
sono state evidenziate : 89 anomalie di origine e decorso ( 2 , 8% ) , 129 anomalie intrinseche della coronaria stessa ( 4% ) e 6 anomalie di terminazione ( 0 , 2% )  . 
i 24 aneurismi , di verosimile origine congenita e non aterosclerotica , erano cos suddivisi sullalbero coronarico : 13 a carico della coronaria destra , 1 sul tronco comune ( tc ) , 5 sulla da , 3 sulla cx e 2 su un ramo marginale . 
 680 radiol med ( 2011 ) 116 : 675689 table 2 prevalence of coronary anomalies expressed in absolute values , as a percentage of all anomalies and of the study population . 
prevalence in number and percentage of principal subtypes observed coronary anomalies number % anomalies % population number % population rca , right coronary artery ; lca , left coronary artery ; lad , left anterior descending artery tabella 2 prevalenza delle anomalie coronariche riscontrate , espresse in : numero assoluto sulla popolazione studiata , percentuale sulla totalit delle anomalie e sulla popolazione in esame . 
the 24 aneurysms , most likely congenital rather than atherosclerotic , were distributed as follows : 13 involved the rca , one the left main stem , ve the lad , three the cx and two a marginal branch . 
nonostante le anomalie coronariche siano spesso soltanto un reperto occasionale , una parte di esse si pu manifestare con una coorte di sintomi estremamente varia : angina pectoris , infarto miocardico , sincope , aritmie e morte improvvisa . 
il quadro di arresto cardiaco con morte improvvisa rappresenta la manifestazione clinica pi drammatica e si stima che il 19% delle morti improvvise in giovani atleti sia correlata con anomalie coronariche [ 18 ]  . radiol med ( 2011 ) 116 : 675689 fig . 
1a - c volume - rendered images of anomalies of origin and course : origin of left main coronary from the ascending aorta ( a , b ) ; origin of both coronary arteries from the ascending aorta ( c ) , the right coronary artery arises more laterally , on the left near the anterior commissure , with angulation and interarterial course ( the pulmonary artery is not visualised )  . 
origine del tronco comune ( tc ) dallaorta ascendente ( a , b ) ; origine di entrambe le coronarie dallaorta ascendente , la coronaria destra ( cdx ) origina in una posizione pi laterale a sinistra , con angolazione e decorso interposto tra aorta e arteria polmonare non visualizzata nellimmagine ( c )  . 
2a - d anomalies of origin and course : maximum intensity projection ( mip ) ( a ) and volume rendering ( vr ) ( b ) images of a circum ex artery arising from the right coronary with a retroaortic course . 
 aorta ( ao ) , arteria polmonare ( ap ) , atrio destro ( adx ) , atrio sinistro ( asn ) , ventricolo destro ( vdx ) , tronco comune ( tc )  . 682 radiol med ( 2011 ) 116 : 675689 fig . 
3a , b anomaly of origin : absence of left main coronary artery : maximum intensity projection ( a ) and volume rendering ( b ) images show a separate origin of the anterior descending artery and circum ex artery from the left sinus of valsalva . 
5a - d anomaly of volume rendering ( a , b ) and multiplanar projection images ( c , d ) demonstrate a thin right coronary artery ( cdx ) arising from the rst segment of a single left anterior descending artery ( da ) ; the left coronary terminates with a 2 - cm ( * ) aneurysm draining directly into the right ventricle . 
5a - d anomalia di immagini vr ( a , b ) e mpr ( c , d ) in un caso di monocoronaria sinistra con origine della coronaria destra ( cdx ) dal primo tratto della discendente anteriore ( da ) che presenta una formazione aneurismatica di 2 cm ( * ) a livello della super cie diaframmatica del cuore stolizzata con il ventricolo destro . 
 although coronary anomalies are often no more than an incidental nding , some may exhibit an extremely varied constellation of symptoms , including angina pectoris , myocardial infarction , syncope , arrhythmias and sudden death . 
cardiac arrest with sudden death is the most dramatic clinical manifestation , and it has been estimated that 19% of sudden deaths among young athletes are related to coronary anomalies [ 18 ]  . 
 criteria for de ning coronary normality / abnormality are as follows : normal , any morphological feature present in > 1% of an unselected population ; normal variant , an alternative , relatively uncommon , morphological feature seen in > 1% of the population ; anomaly , a rare morphological feature seen in < 1% of the population [ 19 ]  . per de nizione si considera : normale ogni condizione presente in pi del 1% di una popolazione non selezionata ; variante normale , unalternativa morfologica relativamente inusuale osservata in pi del 1% della popolazione ; anomalia , quadro morfologico raro osservato in meno del 1% della popolazione [ 19 ]  . la coronarogra a viene attualmente ancora considerata il gold standard per la diagnosi di anomalie coronariche e lincidenza riportata del 1 , 3% [ 15 ]  . 
inoltre la coronarogra a sottostima lincidenza reale dei ponti miocardici , potendo evidenziare solo quelli profondi ed in cui si veri ca una riduzione del lume in sistole [ 20 , 21 ]  . 
altre metodiche quali lecogra a ( sia transtoracica sia transesofagea ) e la risonanza magnetica ( rm ) presentano enormi limiti nella valutazione dellalbero coronarico potendo valutare generalmente solo lorigine o il tratto iniziale . 
any dif culty in catheterising the coronaries or interpreting coronary angiograms should always lead to a suspicion of some anomaly of orig evaluation of the course of the artery is often incorrect , as ca provides only a two - dimensional silhouette of the vessel lumen rather than panoramic , threedimensional images . 
moreover , ca underestimates the true incidence of myocardial bridges , as it is only able to detect deep myocardial bridges in which the lumen is reduced during systole [ 20 , 21 ]  . 
other modalities , such as ultrasonography ( both transthoracic and transoesophageal ) and magnetic resonance ( mr ) imaging are limited in evaluating the coronary tree , as they are generally able to assess only the origin or initial segment of the artery . 
electron - beam tomography has high diagnostic accuracy in the study of the coronary arteries , but its limited availability and high cost have considerably reduced clinical implementation [ 7 , 8 ]  . 
the use of multidetector - row equipment , the possibility of acquiring images synchronised with the electrocardiogram and the availability of several postprocessing protocols ( mip , mpr , curved mpr , vr , ava ) have made it possible for msct to depict the complex and tortuous coronary anatomy , its variants and major diseases [ 16 , 17 ]  . 
coronary dominance was right - sided in 88.1% , left - sided in 8.5% and balanced in 3.4% , in agreement with the main studies reported in the literature ( table 1 ) [ 14 , 15 , 19 ]  . 
moreover , at least two intermediate branches were detected in 0.8% of patients as a result of quadrifurcation of the left main ste our results regarding the number of diagonal and marginal branches of the lca were in part at variance with those reported by cademartiri et al . 
the presence of one or two branches either diagonal or marginal was seen in > 90% of patients in our study , with almost identical prevalence ( 47% ) of one or two branches among the diagonals , in contrast to the greater incidence of two or more diagonal branches reported by cademartiri et al . 
luso infatti di apparecchiature multidetettore , la possibilit di acquisire le immagini con sincronizzazione ecg e la disponibilit di poter usufruire di diversi protocolli di post - processing ( mip , mpr , mpr - curved , vr , ava ) hanno permesso alla tcms di dimostrare agevolmente la complessa e tortuosa anatomia coronarica , le sue varianti e le principali patologie [ 16 , 17 ]  . 
in circa quattro anni e mezzo sono state eseguite 3236 angiotc diagnostiche delle coronarie con tcms a 64 strati , tra queste stata dimostrata una dominanza destra nel 88 , 1% , sinistra nel 8 , 5% e dominanza bilanciata nel 3 , 4% , in accordo con i principali dati riportati in letteratura ( tabella 1 ) [ 14 , 15 , 19 ]  . 
nella nostra casistica la presenza di uno o due rami , sia diagonali che marginali , coinvolge pi del 90% degli individui , con una pressoch totale uguaglianza di prevalenza ( 47% ) tra le due condizioni per quanto riguarda i diagonali , al contrario della maggior incidenza di due o pi rami diagonali riportata dallo studio sopramenzionato . 
tuttavia in tale studio la popolazione era pi selezionata poich 67 soggetti , pari al 12 , 3% della popolazione studiata , eseguivano langio - tc delle coronarie con diagnosi o forte sospetto di anomalia coronarica alla coronarogra a . 
la prevalenza dei ponti miocardici ancora sconosciuta , compresa tra un range dello 0 , 5%4 , 9% negli studi angiogra ci al 15%85% delle autopsie [ 22 ]  . 
 however , their patient population was more selective , as 67 ( 12.3% ) patients underwent ctca due to a diagnosis or strong suspicion of coronary anomaly at conventional ca . 
the actual prevalence of myocardial bridges is probably overestimated by autoptic studies owing to the preparation and selection of the hearts undergoing autopsy , but underestimated by ca , which identi es only indirect signs of bridging such as reduced vessel lumen during systole , a feature present in only a portion of the deeper myocardial bridges . 
along its course within the myocardium , the epicardial vessel may undergo varying degrees of systolic compression , which may manifest as angina , myocardial infarction , left ventricular dysfunction , paroxysmal atrioventricular block and sudden death . 
myocardial bridges are considered to be responsible for infarction in approximately 6% of patients without evidence of atherosclerotic disease ; however , they cannot currently be considered a major additional risk factor for coronary atherosclerosis over and above the classical risk factors . 
an ectopic origin of the coronary arteries from the ascending aorta involving the rca in eight patients , the lca in six and the acute marginal branches in two does not generally give rise to clinical manifestations . 
however , this type of anomaly may cause dif culties in selective catheterisation during ca as a result of the inability to identify the coronary con tcms in pazienti con dolore toracico la prevalenza dei ponti miocardici si distribuisce in un range tra il 3 , 5% e il 30 , 5% . 
gli studi anatomo - patologici verosimilmente sovrastimano la reale prevalenza dei bridge miocardici per motivi di preparazione e di selezione dei cuori sottoposti ad autopsia , mentre la coronarogra a li sottostima , potendo basarsi solo su segni indiretti quale la riduzione del lume vasale in fase sistolica che presente solo in una parte dei ponti miocardici pi profondi . 
il vaso epicardico , nel passaggio allinterno del miocardio che si veri ca in questo tipo di anomalia , pu andare incontro a compressione sistolica di vario grado con possibilit di manifestarsi attraverso angina , infarto del miocardio , disfunzione del ventricolo sinistro , blocco atrio - ventricolare parossistico e morte improvvisa . 
i ponti miocardici sono ritenuti causa di infarto in circa il 6% dei pazienti che non presentano evidenza di malattia aterosclerotica , tuttavia allo stato attuale non possono essere considerati un fattore di rischio rilevante e addizionale per lo sviluppo dellaterosclerosi coronarica rispetto ai fattori di rischio classici della popolazione . 
tra queste sono stati evidenziati 24 casi di origine anomala della coronaria destra , 27 origini anomale della coronaria sinistra , associate in vario modo a 36 anomalie di decorso coronarico . 
le origini ectopiche delle coronarie dallaorta ascendente , riscontrate in 8 soggetti per quanto riguarda la coronaria destra , in 6 per la sinistra ed in 2 per i rami marginali acuti non comportano generalmente disturbi clinici . 
condizioni di questo tipo possono per indurre dif colt nella cateterizzazione selettiva durante coronarogra a , per impossibilit di individuare lostio coronarico nella normale sede bulbare e possono rischiare di essere recise durante interventi sullaorta ascendente o di sostituzione valvolare qualora non si conoscesse il loro decorso anomalo . 
 also associated with a high risk of sudden death , especially in young individuals undergoing intense physical exertion , are some types of ectopic origin of the coronaries from the contralateral sinus of valsalva . 
the ectopic origin of the lca from the right sinus of valsalva is generally associated with a septal course , which is less dangerous than an interarterial course [ 1 ]  . 
in our study , we found 12 cases of ectopic origin of the rca from the left side ( eight from the left sinus of valsalva and four from the lca ) and three cases of ectopic origin of the lca from the right sinus of valsalva . 
speci cally , we found drainage of the rca into the left atrium in one case and into a bronchial vessel in another , two cases of stula between the lad and left ventricle and one of stula between the lad and the pulmonary artery out ow tract , and one case of drainage between the left main stem and the pulmonary artery . coronary stula is an anomaly capable of causing or predisposing to myocardial ischaemia and congestive heart failure in that by draining into the right heart , it may lead to a leftright shunt with volume overload . 
demonstrated that 80% of patients younger than 20 years with coronary stula are asymptomatic on presentation [ 25 ]  . anchessa tuttavia pu essere soggetta a danno iatrogeno in corso di sostituzione valvolare per effetto compressivo . 
nel nostro studio abbiamo riscontrato 12 origini ectopiche della coronaria destra da sinistra ( 8 dal seno di valsalva sinistro e 4 dalla coronaria sinistra ) e 3 origini ectopiche della coronaria sinistra dal seno di valsalva destro . 
 in particolare abbiamo evidenziato : 1 caso di drenaggio della coronaria destra in atrio destro ed 1 caso in un vaso bronchiale ; 2 casi di stola tra da e ventricolo destro ed 1 tra da e tronco di ef usso della polmonare ; 1 caso di drenaggio tra tc e arteria polmonare . 
 la stola coronarica unanomalia in grado di determinare o predisporre ad un evento ischemico miocardico ed a scompenso cardiaco congestizio , in quanto , drenando nelle sezioni cardiache di destra , pu comportare uno shunt sinistro - destro con sovraccarico di volume . 
in primo luogo seppur la nostra popolazione in esame comprendesse individui di diverse razze ed etnie , almeno il 90% dei soggetti studiati era di razza caucasica ( 2133 maschi e 1103 femmine con et compresa tra 1884 anni , et media 57 , 48 , 3 )  . 
moreover , our study focused exclusively on the prevalence of coronary anomalies in the population without discussing their clinical relevance in relation to the literature [ 19 , 28 , 29 ]  . 
the cost - effectiveness of msct in relation to the hanno identi cato nel 52% dei casi valutati unorigine separata dellarteria coronaria discendente e dellarteria circon essa nel seno coronarico sinistro , mentre velican et al . 
 questo studio inoltre valuta esclusivamente la prevalenza nella popolazione delle anomalie coronariche senza valutare la rilevanza clinica delle stesse riferita a quanto noto in letteratura [ 19 , 28 , 29 ]  . 
per quanto riguarda i ponti miocardici sappiamo ad esempio che la rilevanza clinica diversa tra quelli super ciali e quelli profondi e in base alla loro lunghezza [ 20 ]  . 
lesposizione alle radiazioni in corso di un esame di questo tipo generalmente di 1520 msv a discapito dellesame coronarogra co che si pone a valori di esposizione inferiori che dif cilmente superano i 7 msv . 
unindagine di questo tipo pu essere effettuata anche nellinfanzia in pazienti con elevato rischio di malformazioni coronariche con unesposizione estremamente bassa compresa tra 0 , 17 e 0 , 65 msv con modulazione estrema di dose e trigger prospettico come riportato da goo et al . 
 conclusioni i miglioramenti nella risoluzione spaziale e temporale , nelle tecniche di gating ecg - correlate , negli algoritmi e nei software di post - processing hanno reso langio - tc coronarica una metodica accurata e af dabile nella diagnostica vascolare cardiaca con risultati anche superiori rispetto alle tradizionali tecniche diagnostiche invasive e non invasive . 
however , the indication for noninvasive coronary imaging to investigate suspected coronary anomalies or exclude their presence should be carefully considered together with the clinician to avoid exposing young patients to excessive doses of ionising radiation . 
with the availability of extreme dose modulation systems and prospective gating , this problem no longer exists owing to the possibility of obtaining a greater amount of diagnostic information compared with conventional ca , noninvasively , and with an equal or lower dose of ionising radiation . one group of patients who could bene t considerably from a noninvasive imaging modality such as ctca is that of young patients with exertional angina , syncope and ventricular tachyarrhythmias who have a low pretest likelihood of signi cant atherosclerotic disease on the basis of the medical history and clinical and laboratory data . finally , in light of the above considerations , we conclude that msct - ca should become the examination of choice in patients with suspected coronary anomaly . le anomalie coronariche sono un reperto relativamente frequente nel contesto dellimaging non invasivo coronarico . 
tuttavia , lindicazione allesecuzione di unindagine non invasiva coronarogra ca per sospetta anomalia coronarica o per escluderne la presenza deve essere ben ponderata in cooperazione con il clinico , al ne di evitare ad un paziente di giovane et uneccessiva esposizione a radiazioni ionizzanti . 
con gli attuali presidi di modulazione estrema dellesposizione e acquisizioni con trigger prospettico , tale problema non si pone per la possibilit di ottenere maggiori informazioni diagnostiche rispetto alla coronarogra a , in modo non invasivo e con una dose di radiazioni ionizzanti uguale o inferiore . un gruppo particolare di pazienti che potrebbe bene ciare notevolmente di una metodica di imaging non invasiva quale langio - tc coronarica rappresentato da pazienti giovani con angina da sforzo , sincope e tachiaritmie ventricolari e dai quali non ci si aspetta una patologia aterosclerotica signi cativa sulla base dei dati anamnestici e clinico - laboratoristici . alla luce di queste considerazioni possiamo in ne concludere che nel sospetto di anomalia coronarica lesame con tcms dovrebbe essere lindagine di prima scelta . conflict of interest none pediatric surgical diseases . 
 the topic is divided into 8 chapters ( head and neck ; thorax ; abdomen ; genitourinary disorders ; cardiovascular disorders ; musculoskeletal disorders ; emergency and trauma ; oncology ) each of which is headed by ( apart from the emergency and trauma section ) a more or less long introduction . the collection of cases ( 94 from italian hospitals , most from naples , the rest from abroad , even a clavicle fracture ! ) is relevant . each case is presented in one page ( radiological and clinical images ; brief history and salient laboratory data ; questions on how to deal with the problem and in this case further examinations in order to obtain a proper diagnosis ) , the discussion , further images and nal diagnosis are on the following page . this lay - out often requires that the reader must shuf e forward and backward , especially where more than one radiological image is presented . 
shouldnt these chapters have been merged ? is a bone fracture an emergency or a musculoskeletal disorder ? due editori , cinque editori associati , novantasei collaboratori hanno riunito le forze per preparare questo volume che in 530 pagine discute 249 casi clinici . la materia divisa in 8 capitoli ( capo e collo ; torace ; addome ; malattie dellapparato genito - urinario ; malattie cardiovascolari ; malattie muscolo - scheletriche ; urgenze e trauma ; oncologia ) ciascuno preceduto ( eccezion fatta per quello dedicato alle urgenze e trauma ) da una introduzione pi o meno lunga . la raccolta dei casi ( 94 da ospedali italiani , per lo pi da napoli , il resto dallestero , compresa una frattura di clavicola ! ) pertinente . ciascun caso presentato su di una pagina ( immagini radiologiche e cliniche ; breve storia e dati salienti di laboratorio ; quesiti su come comportarsi per risolvere il problema ed in tal caso quali ulteriori indagini richiedere per ottenere una diagnosi corretta ) , mentre la discussione , altre immagini e la diagnosi nale sono sulla pagina successiva . questa impostazione richiede spesso al lettore uno sfogliare avanti ed indietro di pagina , soprattutto nei casi in cui vi sia pi di una immagine radiologica . 
 vi inoltre un ulteriore inconveniente nella presentazione : i casi riguardanti alcune condizioni ( per esempio la stenosi ipertro ca del piloro , linvaginazione o lappendicite ) non sono presentati uno di seguito allaltro in modo tale da fornire al lettore lintero spettro delle loro possibili manifestazioni cliniche e radiologiche . 
questo fatto si ri ette anche nellindice ove la stessa condizione citata pi di una volta ed in modi differenti . motivo di perplessit poi il vedere come le stesse condizioni ( lappendicite per esempio ) siano state trattate nel capitolo dedicato alladdome e poi ancora in quello dedicato allurgenza e trauma . 
non sarebbe stato meglio uni carli ? una frattura unurgenza o una malattia muscoloscheletrica ? 826 radiol med ( 2011 ) 116 : 825826 going through the histories of the presented cases one will often read : the paediatrician , the surgeon or the doctor performed the examination ( a radiological examination )  . 
the paediatrician or the paediatric surgeon request and the radiologist performs the requested examination and makes a diagnosis ! at this point one realizes that only 26 of the presented cases are associated with a radiologists name . most of the images , clinical , surgical , radiological are of good quality , cleverly mixed and organized . 
 furthermore , just to quote some examples , one will nd incorrect image labelling ; images that are described and not to be found ; left for right side re uxing megaureter ; urethral duplication for ureteral duplication ; complete ureteric duplication on the right ( q / a 147 ) when one can only see a grade iii vesico - ureteric re ux etc . i also have some doubts regarding the roviraltas syndrome case ( q / a 92 ) : if one over lls the stomach with contrast medium and there is a tight hypertrophic stenosis as figure 2 shows , it is a rule of thumb that a gastro - oesophageal re ux will follow ( as in figure 1 )  . 
il pediatra o il chirurgo pediatra richiedono ed il radiologo esegue lindagine richiesta fornendo poi la diagnosi ! a questo punto ci si rende conto che solo 26 dei casi presentati sono associati al nome di un radiologo . la maggior parte delle immagini , cliniche , chirurgiche , radiologiche sono di buona qualit , disposte ed organizzate con intelligenza . 
tuttavia , si trovano alcuni brutti esempi di immagini radiologiche : non accuratamente ritagliate ; senza protezione gonadica ; estese a torace e addome in casi di urogra a . inoltre , solo per citare alcuni esempi , si potranno trovare errori nelle didascalie ; immagini che sono descritte e non sono presenti ; sinistro per megauretere re uente destro ; duplicit uretrale per duplicit ureterale ; duplicit ureterale destra completa ( q / a 147 ) , mentre osservabile solo un re usso vescico - ureterale di iii grado ecc . ho poi alcuni dubbi riguardanti il caso di sindrome di roviralta ( q / a 92 ) : se lo stomaco viene riempito in eccesso dal mezzo di contrasto ed presente una stenosi ipertro ca serrata come dimostrato dalla figura 2 , evidente che ne seguir un re usso gastro - esofageo ( come nella figura 1 )  . 
 un reperto conseguente al primo e non vice - versa . la presentazione delle voci bibliogra che discordante : si trovereanno molte e differenti modalit di presentazione , anche nello stesso elenco . 
in group a , the ct scan was performed with conventional bowel preparation ( a full cathartic dose and oral contrast medium to tag any residue in the 3 days preceding the study )  . 
in the second group , ct colonography was performed after a reduced bowel preparation , with the oral contrast medium for residue tagging being administered only on the day of the investigation . 
due gruppi di 40 pazienti asintomatici consecutivi , di et fra i 48 ed i 72 anni , sono stati sottoposti a colon - tc : nel gruppo a lesame tc stato eseguito con preparazione intestinale convenzionale ( catartico a piena dose e mezzo di contrasto orale per la marcatura dei residui nei 3 giorni precedenti lindagine ) ; il secondo gruppo ha eseguito la colon - tc dopo preparazione intestinale ridotta con somministrazione orale di contrasto per la marcatura dei residui solo il giorno dellindagine . 
in pazienti asintomatici , lutilizzo di un software per la sottrazione di liquidi in concomitanza ad 750 radiol med ( 2011 ) 116 : 749758 images in conjunction with reduced bowel preparation does not reduce examination quality or diagnostic performance when compared with the conventional ct colonography technique and is more acceptable to and better tolerated by the patient . una ridotta preparazione intestinale , non comporta una riduzione di qualit e performance diagnostica rispetto alla tecnica colon - tc tradizionale , mentre risulta pi accettabile e meglio tollerato da parte del paziente . parole chiave colon - tc tecnica di esame accettabilit keywords virtual colonoscopy ct colonography imaging technique acceptability introduction introduzione colorectal cancer is the second leading cause of death for cancer in the usa [ 1 ]  . 
the target of screening for colorectal cancer is intermediate - grade adenoma , characterised by a mean size of about 1 cm at diagnosis and the presence of a villous structure equal to at least 25% of the lesion [ 4 ]  . 
computed tomography ( ct ) colonography is able to con rm or exclude the presence of such lesions with levels of accuracy comparable with conventional colonoscopy and is therefore ideal for colorectal cancer screening [ 510 ]  . 
ct colonography performed with conventional bowel preparation , similar to that used for colonoscopy , involves some discomfort for the patient in the days before the examination as well as a risk of side effects , which makes this type of preparation neither suitable nor acceptable for a screening investigation [ 11 , 12 ]  . 
the introduction of oral contrast media for tagging residual stools and uid has led to a signi cant reduction in the level of required intestinal catharsis [ 1115 ] and the development of various combinations regarding the choice of contrast media ( ionic / nonionic ) and timing of contrast administration ( in the days preceding the examination or on the same day ) [ 14 , 19 , 20 , 22 , 23 ]  . 
however , few data are available with regard to the quality , acceptability and the diagnostic performance of ct colonography carried out with conventional preparation compared with simpli ed preparation and administration of oral contrast medium on the day of the ct scan [ 23 ]  . the aim of our study was therefore to compare examination quality , diagnostic performance and acceptability in two groups of patients who were recruited prospectively and studied with ct colonography following simplied bowel preparation and software for electronic residue subtraction , compared with patients receiving conventional bowel preparation . il carcinoma del colon - retto rappresenta la seconda causa di morte per patologie neoplastiche negli stati uniti [ 1 ]  . 
il target dello screening per neoplasia del colon - retto rappresentato dalladenoma di grado medio , caratterizzato da dimensioni medie alla diagnosi di circa 1 cm e dalla presenza di una struttura villosa pari ad almeno il 25% della lesione [ 4 ]  . 
la colon - tomogra a computerizzata ( colon - tc ) capace di confermare o escludere con accuratezza sovrapponibile alla colonscopia tradizionale la presenza di lesioni con tali caratteristiche , e pertanto si candida come indagine ideale per lo screening del carcinoma del colon - retto [ 510 ]  . 
la colon - tc effettuata con preparazione intestinale tradizionale , simile a quella utilizzata per la colonscopia , comporta un disagio per il pazienti nei giorni antecedenti lesame , nonch il rischio di effetti collaterali , rendendo tale preparazione non adatta n accettabile per gli studi di screening [ 11 , 12 ]  . 
recenti lavori hanno pertanto puntato lattenzione sullaumento della accettabilit dellesame da parte del paziente , ottenuto mediante una riduzione della complessit della preparazione intestinale o della restrizione dietetica richiesta [ 1123 ]  . 
lintroduzione dei mezzi di contrasto orali per la marcatura dei residui fecali e uidi ha reso possibile una signi cativa riduzione della catarsi intestinale normalmente richiesta [ 1115 ] e lo svilupparsi di varie combinazioni riguardanti la scelta del mezzo di contrasto da impiegare ( ionico / non ionico ) e le tempistiche di somministrazione degli stessi ( nei giorni precedenti lesame o il giorno stesso ) [ 14 , 19 , 20 , 22 , 23 ]  . 
tuttavia , sono disponibili pochi dati in letteratura riguardo la qualit , laccettabilit e la performance diagnostica della colon - tc effettuata con preparazione intestinale tradizionale standard e mediante preparazione intestinale sempli cata e somministrazione di contrasto orale il giorno stesso dellindagine tc [ 23 ]  . 
 lo scopo del nostro lavoro pertanto quello di confrontare qualit desame , performance diagnostica ed accettabilit dellindagine da parte di due gruppi di pazienti prospetticamente reclutati e sottoposti a colon - tc con proradiol med ( 2011 ) 116 : 749758 materials and methods patients and inclusion and exclusion criteria over a period of 15 months , 150 consecutive patients were considered for inclusion in the study . 
patients with intestinal polyposis ( n = 2 ) , acute abdomen either ongoing or over the previous month ( obstruction , perforation , acute diverticulitis ) ( n = 5 ) and patients with prior colorectal surgery ( n = 63 ) were excluded from the study . 
therefore , 80 patients were prospectively enrolled ( 48 men and 32 women , mean age 59 years , range 4872 years ) who underwent ct colonography for polyp detection . 
the patients underwent ct colonography due to the presence of faecal occult blood ( n = 37 ) , a family history of colorectal cancer ( n = 27 ) or for screening purposes ( n = 16 )  . diet , bowel preparation , residue removal in the 3 days preceding the survey , patients in both groups followed a low - residue diet , avoiding the intake of any bre - containing foods . 
in addition , they were instructed to consume only soup on the day before the ct scan and to fast from any solid food on the day of the scan . 
the rst group ( group a , n = 40 ) performed a conventional cathartic bowel preparation , the goal of which is to make the bowel lumen as free as possible from uid and faecal residue . 
in addition to the dietary restrictions described above , all patients in group a took intestinal cathartics ( isocolan , polyethylene glycol 4 , 000 , giuliani s.p.a , milan , italy ) , one packet of 34.8 g for each of the three main meals of the day , diluted in 500 ml of water in the 2 days preceding the scan ; at each meal , the cathartic was combined with meglumine amidotrizoate ( gastrogra n , bayer schering pharma , milan , italy ; with an iodine concentration of 370 mg / ml ) at a concentration of 10 ml diluted in 100 ml of water . 
in addition , on the day of the scan , all patients in group a received a glycerine enema and a nal dose of gastrogra n ( 25 ml ) during the 3 h preceding the study . the second group ( group b , n = 40 ) followed a simplied or partial bowel preparation with 13.8 g of the oral cathartic polyethylene glycol ( peg macrogol 3 , 350 , movicol , norgine s.r.l , italy ) diluted in 750 ml of water taken with each of the six main meals in the 2 days preceding the study . 
on the day of the examination , an oral contrast medium was administered ( meglumine amidotrizoate , gastrogra n , bayer schering ; iodine concentration of 370 mg / ml ) at a total dose of 50 ml diluted in 1 , 000 ml of water , starting 3 h before the scan . 
patients were also asked to drink the solution in a slow and continuous fashion in tocollo di preparazione intestinale sempli cata ed utilizzo di un software di sottrazione dei liquidi , a confronto con un protocollo di preparazione tradizionale . materiali e metodi pazienti , criteri di inclusione e di esclusione in un arco temporale di 15 mesi , sono stati considerati 150 pazienti consecutivi per linclusione nel nostro studio . 
sono stati esclusi dallo studio i pazienti affetti da sindromi polipose intestinali ( n = 2 ) , qualsiasi forma di addome acuto in atto o nel corso dellultimo mese ( occlusione , perforazione , diverticolite acuta ; n = 5 ) , ed i pazienti con pregressi interventi di chirurgia colo - rettale ( n = 63 )  . 
sono stati pertanto prospetticamente arruolati 80 pazienti ( 48 maschi , 32 femmine ; et media 59 anni , range 4872 anni ) sottoposti a colon - tc per la ricerca di formazioni polipoidi . 
i pazienti arruolati hanno effettuato la colon - tc per la presenza di sangue occulto nelle feci ( n = 37 ) , familiarit per carcinoma del colon - retto ( n = 27 ) , a scopo di screening ( n = 16 )  . 
 dieta , preparazione intestinale , rimozione dei residui nei tre giorni precedenti lindagine , i pazienti di entrambi i gruppi hanno seguito una dieta povera di scorie , evitando lassunzione di qualsiasi prodotto contenente bre . 
in maniera casuale , i pazienti arruolati sono stati suddivisi in due gruppi , in base alla preparazione intestinale effettuata : il primo gruppo ( gruppo a ; n = 40 soggetti ) ha eseguito una preparazione intestinale convenzionale , di tipo catartico , il cui scopo rendere il lume del colon il pi possibile libero da residui uidi e fecali : oltre alle restrizioni dietetiche sopra descritte , tutti i pazienti del gruppo a hanno assunto dei catartici intestinali ( isocolan , polietilenglicole 4000 , giuliani spa , milano , italia ) , 1 bustina da 34 , 8 g per ognuno dei 3 pasti principali della giornata , diluiti in 500 ml dacqua , nei due giorni antecedenti lesame ; ad ogni pasto , il catartico stato associato alla meglumina amidotrizoato ( gastrogra n , bayer schering pharma , milano , italia ; concentrazione di iodio pari a 370 mg / ml ) nella concentrazione di 10 ml , diluito in circa 100 ml dacqua . 
 il giorno dellindagine inoltre tutti i pazienti sono stati sottoposti a clistere di glicerina e somministrazione orale dellultima dose di gastrogra n ( 25 ml ) , in regime ambulatoriale il giorno dellesame , durante le 3 ore antecedenti lindagine . il secondo gruppo ( gruppo b ; n = 40 soggetti ) ha invece eseguito una preparazione intestinale sempli cata o parziale , con assunzione per via orale di un agente catartico 752 radiol med ( 2011 ) 116 : 749758 order to avoid excessive gastric distension and promote a constant intestinal peristalsis , thus ensuring homogeneous distribution of the contrast medium within the intestinal lumen . 
the topogram acquired at the beginning of the study was used to assess the proper progression of the contrast medium and decide on the best timing for the examination . examination protocol all ct colonography studies were performed with a multidetector ct unit ( brilliance 64 , philips , eindhoven , the netherlands ) and two acquisitions with the patient in the prone and supine positions , respectively . 
data were then reconstructed to a slice thickness of 2 mall patients were administered the spasmolytic agent hyoscine butylbromide ( buscopan , boehringer ingelheim , germany ) intramuscularly 10 min before the examination to reduce intestinal peristalsis and improve the quality of the examination . 
with the patient in a left lateral decubitus position , the colon was distended by insuf ating room air manually through a pump connected to a soft rectal tube equipped with a self - retaining balloon . 
 the extent of colonic distension was assessed on a caseby - case basis : colonic insuf ation was interrupted when the patient expressed discomfort , and in all cases , distension was assessed on the scout view before starting the scan and corrected , if necessary , to obtain appropriate distension . image analysis all images were evaluated by two experienced radiologists ( 15 and 16 years of experience in colorectal disease , respectively ) on a dedicated workstation , allowing the simultaneous twoand three - dimensional analysis of the images acquired . 
using bone window settings ( width 3 , 000 hu , centre 300 hu ) , the analysis was performed for each patient taking into account the six colonic segments : caecum , ascending colon , transverse colon , descending colon , sigmoid colon and rectuall studies were also evaluated with and without the use of software for residue subtraction . 
any doubtful ndings were discussed in consensus . examination quality for the two patient groups was evaluated on the basis of a qualitative analysis performed by the two readers , who assessed the following parameters : number of segments free of faecal residue ; residue volume in relation to the total segment volume in segments partially occupied by faecal residue , rated according to three subclasses : ( 1 ) < 10% ; ( 2 ) 1025% ; ( 3 ) > 25% . 
diagnostic performance in the detection of polyps 6 mm in diameter , based on identi cation of true - positive ( tp ) ndings and exclusion of false - positives ( fp ) was evaluated for both ( peg macrogol 3350 , movicol , norgine italia srl , italia ) nella dose di 13 , 8 g in 750 ml di acqua per pasto , nei sei principali pasti delle 2 giornate precedenti lindagine . 
il giorno stesso dellesame stato somministrato un mezzo di contrasto orale ( meglumina amidotrizoato , gastrogra n , bayer schering pharma , milano , italia ; concentrazione di iodio pari a 370 mg / ml ) , in una dose totale di 50 ml , diluito in 1000 ml di acqua , a partire da 3 ore prima dellesame . 
 i pazienti sono stati inoltre invitati ad assumere in maniera lenta e continua la soluzione sopra descritta allo scopo di evitare uneccessiva distensione gastrica e favorire invece una costante peristalsi intestinale che garantisse una distribuzione omogenea del contrasto nel lume intestinale . 
 il topogramma acquisito nelle fasi iniziali dellindagine stato utile a valutare la corretta progressione del liquido di contrasto ed a scegliere il tempismo migliore per lesecuzione dellindagine stessa . protocollo desame tutti gli esami colon - tc sono stati eseguiti con un apparecchio tc multistrato ( brilliance 64 , philips , eindhoven , olanda ) , con 2 acquisizioni rispettivamente con paziente in decubito prono e supino , con i seguenti parametri di scansione : spessore di fetta 1 mm , z = 1 , 120 kvp e 60 mas . 
i dati sono stati poi ricostruiti con uno spessore pari a 2 min tutti i pazienti stato utilizzato un agente spasmolitico ( buscopan , boehringer , ingelheim , germania ) intramuscolo 10 minuti prima dellesame per ridurre la peristalsi intestinale ed aumentare la qualit desame . 
con il paziente in decubito laterale sinistro , il colon stato disteso utilizzando aria ambiente , progressivamente pompata manualmente tramite pompetta collegata ad un tubo rettale morbido dotato di pallone di contenzione . 
lentit della distensione colica stata valutata di caso in caso : linsuf azione colica veniva interrotta nel caso in cui il paziente lamentasse dolore , in tutti i casi era valutata sul topogramma prima dellesecuzione dellindagine ed eventualmente veniva poi corretta no ad ottenere una distensione idonea . 
 analisi delle immagini tutte le immagini sono state valutate da 2 radiologi esperti in patologia colo - rettale ( 15 e 6 anni di esperienza rispettivamente ) , su una workstation dedicata che permetteva lanalisi simultanea bie tridimensionale delle immagini acquisite . 
utilizzando una nestra di visualizzazione per i tessuti ossei ( ampiezza 3000 hu , centro 300 hu ) , lanalisi stata eseguita considerando , per ogni paziente , 6 segmenti colici : cieco , colon ascendente , colon trasverso , colon discendente , colon sigma e retto . 
tutti i rilievi dubbi sono stati discussi in consenso . la qualit desame , per i due gruppi di indagini eseguite con differente protocollo , stata valutata in base ad radiol med ( 2011 ) 116 : 749758 techniques using as a reference - standard breoptic colonoscopy performed only in patients with suspected colorectal polyps on ct colonography . the acceptability of the bowel preparation protocol was assessed with the aid of a self - completed questionnaire and scored on a scale from 1 ( nearly total unacceptability of the protocol ) to 10 ( no discomfort associated with the protocol )  . statistical analysis interobserver variability in determining the presence or absence of polyps and assessing examination quality was evaluated using the statistic . 
a p value < 0.05 was considered statistically signi cant . distribution of faecal residue ( stool and uids ) within the six colonic segments in the two groups of patients is outlined in table 1 . 
in group a , 180 / 240 segments were free una analisi qualitativa espletata dai 2 radiologi coinvolti , i quali hanno valutato i seguenti parametri : numero di segmenti liberi da residui ; nei segmenti parzialmente occupati da residui , volume degli stessi in relazione al volume totale del segmento preso in esame , considerando 3 sottoclassi : ( 1 ) inferiore al 10 % , ( 2 ) dal 10% al 25% , ( 3 ) superiore al 25% . 
la performance diagnostica nellevidenziare polipi con dimensioni uguali o superiori a 6 mm , basata sullidenti cazione di rilievi veri positivi ( vp ) e sullesclusione dei falsi positivi ( fp ) , stata valutata per entrambe le tecniche desame , utilizzando come standard di riferimento la colonscopia ottica , eseguita solo nei pazienti con sospetto di polipi alla colon - tc . 
 laccettabilit della preparazione effettuata stata valutata mediante questionario auto - compilativo da parte dei pazienti coinvolti , considerando una scala di valori di accettabilit compresa fra 1 ( pressoch totale inaccettabilit della preparazione ) e 10 ( nessun fastidio connesso con la preparazione )  . 
 la concordanza inter - osservatore stata considerata scarsa per valori di inferiore o uguale a 0 , 20 , discreta per compresa tra 0 , 21 e 0 , 40 , moderata per tra 0 , 41 e 0 , 60 , table 1 qualitative evaluation of the amount of faecal or uid residue not subtracted or insuf ciently removed by the software in the two study populations undergoing conventional full - dose ( group a ) and reduced - dose ( group b ) bowel preparation residue absent < 10% 10%25% > 25% group a group b group a group b group a group b group a group b tabella 1 stima qualitativa della quantit di residui non sottratti o insuf cientemente rimossi dal software , nelle due popolazioni di studio sottoposte a preparazione intestinale convenzionale ( gruppo a ) e parziale ( gruppo b ) residui assenti < 10% 10%25% > 25% gruppo a gruppo b gruppo a gruppo b gruppo a gruppo b gruppo a gruppo b 180 180 165 165 results caecum ascending transverse descending sigmoid rectum total cieco ascendente trasverso discendente sigma retto totale 754 radiol med ( 2011 ) 116 : 749758 fig . 
1a - d a 56 - year - old woman with a family history of colon cancer undergoing conventional bowel preparation with oral administration of gastrogra n in the 3 days prior to the examination , together with a full dose of the cathartic drug ( group a )  . 
1a - d donna di 56 anni con familiarit per carcinoma del colon sottoposta a preparazione intestinale convenzionale con somministrazione di gastrogra n per os nei tre giorni antecedenti allindagine unitamente allingestione orale dellagente catartico ( gruppo a )  . 
 le immagini di partizione ottenute sui piani assiale e coronale prima ( a , b ) e dopo utilizzo del software di sottrazione ( c , d ) dimostrano una pressoch completa replezione del colon con il mezzo di contrasto orale , correttamente rimosso per azione del software stesso , garantendo una elevata qualit desame . 
in group a , 16 / 17 polyps were identied ( with six fp ) , whereas in group b , 12 / 13 polyps were detected ( with ve fp ) compared with conventional colonoscopy performed on patients with positive or doubtful ndings on ct colonography ( table 2 )  . 
inter - observer agreement was excellent both for identifying polyps ( = 0.94 ) buona per tra 0 , 61e 0 , 80 , ed eccellente per tra 0 , 81 e 1 . 
2a - d a 68 - year - old woman with positive faecal occult blood test undergoing reduced intestinal preparation with oral administration of the contrast material on the day of examination ( group b )  . 
2a - d donna di 68 anni con sangue occulto nelle feci , sottoposta a preparazione intestinale sempli cata con somministrazione di contrasto orale il giorno stesso dellindagine ( gruppo b )  . 
 the self - completed questionnaires revealed greater acceptance patients undergoing the partial bowel preparation protocol compared with patients undergoing conventional preparation ( p = 0.01 ) : the mean score for patients in group a ( conventional preparation ) was 6 ( range 48 ) , whereas that for patients in group b ( partial preparation ) was 9 ( range 610 )  . discussion the technological advances of ct scanners , the relative speed and accessibility of the examination and its good overall accuracy in identifying colorectal polyps make ct colonography a potential candidate for colorectal cancer screening [ 59 ]  . 
conventional bowel preparation , similar to that required for breoptic colonoscopy , ensures a good quality examination but is often associated with marked patient discomfort in the days before the test , leading to poor patient acceptance . 
the presence of faecal residue ( stool or uid ) within the colonic lumen is a major cause of poor examination quality , leading to an increased risk of qualit desame ( p > 0 , 05 )  . 
anche in questo gruppo i residui sono stati mediamente pi abbondanti nel sigma , nel discendente e nel retto . abbiamo riscontrato una differenza non signi cativa per quanto riguarda i settori del colon liberi da residui ( p = 0 , 09 ) , e quelli con maggior quantit di residui ( p = 0 , 124 )  . 
nel gruppo a sono stati identi cati 16 / 17 polipi ( con 6 fp ) , mentre nel gruppo b sono stati identi cati 12 / 13 polipi ( con 5 fp ) a confronto con la colonscopia tradizionale , espletata solo nei pazienti con rilievi positivi o dubbi alla colon - tc ( tabella 2 )  . 
la concordanza inter - osservatore stata eccellente sia per quanto riguarda la identi cazioni di lesioni polipoidi ( = 0 , 94 ) , che per quanto concerne la valutazione della qualit dindagine ( = 0 , 92 )  . 
dai questionari auto - compilativi emersa una maggiore accettabilit da parte dei pazienti sottoposti a preparazione intestinale parziale rispetto a quella convenzionale ( p = 0 , 01 ) : la valutazione media dei pazienti del gruppo a , sottoposti alla preparazione convenzionale , stata di 6 ( range 48 ) , mentre quella del gruppo b , sottoposti a preparazione parziale , stata di 9 ( range 610 )  . 
 756 radiol med ( 2011 ) 116 : 749758 table 2 trueand false - positive ndings in the two subgroups of patients undergoing different intestinal preparations , using as the reference standard breoptic colonoscopy , performed only in the subset of patients presenting positive or doubtful ndings at computed tomography colonography discussione patients true positives , n ( % ) false positives , n group a group b 16 / 17 ( 94.1 ) 12 / 13 ( 92.3 ) tabella 2 rilievi veri positivi e falsi positivi delle due popolazioni di studio , sottoposte a diversa preparazione intestinale , a confronto con i risultati della coloscopia ottica , eseguita nei soli pazienti con rilievi alla colon - tc pazienti veri positivi , n ( % ) falsi positivi , n gruppo a gruppo b 16 / 17 ( 94 , 1 ) 12 / 13 ( 92 , 3 ) error [ both false negatives ( fn ) and fp ] and longer image interpretation times [ 15 , 22 ]  . the introduction of new and less demanding bowel preparation protocols with limited dietary restriction and / or a lower doses of intestinal cathartics in the days preceding the study along with the possibility of administering oral contrast material for faecal tagging on the day of the examination and the development of residue - removal software has made possible a real increase in the acceptability of ct colonography by patients [ 15 , 18 , 23 ]  . 
in agreement with the literature , our results show that there is no signi cant difference in the quality of ct colonography examinations performed after a reducedor full - dose bowel catharsis , thanks to the use of uid - subtraction software . 
although not demonstrated in our study , the success of the simpli ed bowel preparation protocol can be attributed to a greater adherence to the simpli ed preparation on the part of patients , compared with the conventional protocol . 
a further increase in patient acceptance of the various preparation protocols could result from not imposing any dietary restrictions on the study population , as demonstrated by a recent study by liedenbaum et al . 
although those authors concluded that there was no loss of examination quality in the patient group with unrestricted diet compared with the group prescribed a lowbre diet [ 15 ] , we did not introduce this parameter in our analysis because we are convinced that dietary restriction is one of the smaller inconveniences of bowel preparation , with the extent of catharsis being more upsetting in direct proportion to the development of diarrhoea and abdominal pain . nonetheless , despite the absolute quality of investigations obtained following partial preparation being slightly lower grazie alla innovazione tecnologica delle apparecchiature tc , alla relativa rapidit ed accessibilit allindagine , ed alla buona accuratezza globale nellidenti cazione dei polipi colo - rettali , la colon - tc si candida come potenziale indagine per lo screening del carcinoma del colon - retto [ 59 ]  . 
la preparazione intestinale convenzionale , simile a quella richiesta per la colonscopia ottica , garantisce attualmente una buona qualit desame , ma spesso associata ad un marcato disagio da parte dei pazienti nei giorni antecedenti lesame , rendendo laccettabilit dellindagine ancora scarsa . 
la presenza di residui allinterno del lume colico , sia di natura liquida sia di natura fecale , rappresenta unimportante causa di riduzione della qualit desame , condizionando un relativo aumento del rischio di errore sia in negativo ( falsi negativi ) , che in positivo ( falsi positivi ) , e pu portare ad un aumento dei tempi di lettura [ 15 , 22 ]  . 
 lintroduzione di nuovi e meno impegnativi protocolli per la preparazione intestinale , con limitata restrizione dietetica e / o riduzione della dose di catartico intestinale nei giorni antecedenti lindagine , insieme alla possibilit di somministrare il mezzo di contrasto orale per la marcatura fecale il giorno stesso dellesame ed al perfezionamento dei software di rimozione dei residui , ha reso possibile un aumento concreto dellaccettabilit da parte dei pazienti dellindagine colon - tc [ 15 , 18 , 23 ]  . 
in accordo con i dati della letteratura , i nostri risultati dimostrano come non ci sia una differenza signi cativa nella qualit desame colon - tc eseguita previa catarsi intestinale parziale o a piena dose , anche grazie allutilizzo del software di sottrazione liquidi . 
 anche se non dimostrato dal nostro studio , il successo della preparazione intestinale sempli cata da ricercarsi nella maggiore adesione al protocollo di preparazione da parte dei pazienti , rispetto alladesione al protocollo tradizionale . 
nonostante questi autori concludano come non vi sia stata perdita di qualit nel gruppo di pazienti senza restrizioni dietetiche rispetto al gruppo sottoposto a dieta povera di bre [ 15 ] noi non abbiamo introdotto questo parametro nella nostra analisi perch convinti che la restrizione dietetica rappresenti uno dei minori fastidi connessi alla preparazione , essendo fastidio maggiore lentit della catarsi direttamente proporzionale allo sviluppo di diarrea ed addominalgia . 
 in ogni caso , nonostante la qualit assoluta delle indagini acquisite nei pazienti sottoposti a preparazione parziale sia stata lievemente inferiore a quella del gruppo di pazienti sottoposti a preparazione catartica tradizionale , la differenza qualitativa fra le due popolazioni non stata signi catiradiol med ( 2011 ) 116 : 749758 than that obtained after conventional cathartic preparation , the qualitative difference between the two groups was not signi cant . 
speci cally , the sigmoid and descending colon , with the right colon , were the segments with most residue in both groups of patients , with no statistically signi cant difference between groups . 
as expected , and in agreement with the results of other recent reports [ 15 , 22 , 23 ] , our study con rmed greater acceptance of the investigation by the patients in group b when compared with those in group a . although the small sample size renders the statistical validity of our preliminary results rather modest , the overall diagnostic accuracy was comparable between the two groups of patients despite the small qualitative difference encountered between the two protocols being tested . 
an additional advantage of the partial bowel preparation with administration of oral contrast medium on the day of the examination is the possibility of preventing , monitoring and promptly treating any side effects arising as a result of the partial absorption of the oral contrast medium by the intestinal wall [ 24 ]  . this study has its limitations . 
this said , however , the excellent results obtained lay the foundation for re ning the simpli ed intestinal preparation protocol and undertaking further studies involving a larger number of patients . 
 secondly , conventional colonoscopy was performed only in patients with positive ndings at ct colonography , and therefore , the real impact of fn ndings may have been underestimated , giving less reliable estimates of overall accuracy . 
nello speci co , il sigma ed il colon discendente , insieme al colon destro , sono risultati i settori con maggior quantit di residui nei due gruppi di pazienti , senza alcuna differenza statisticamente signi cativa fra i due sottogruppi sottoposti a differente preparazione . 
come atteso , ed in accordo con i risultati di altri lavori recentemente pubblicati [ 15 , 22 , 23 ] , il nostro studio ha confermato un aumento dellaccettabilit dellindagine da parte dei pazienti del gruppo b rispetto al gruppo a . 
 in ne , anche se lesiguit del campione analizzato rende modesta la validit statistica dei risultati preliminari nora ottenuti , laccuratezza diagnostica globale stata sovrapponibile nei due gruppi di pazienti nonostante la modesta differenza qualitativa ottenuta con le due preparazioni testate . 
tra gli altri vantaggi della preparazione intestinale parziale con somministrazione di mezzo di contrasto orale il giorno dellesame vanno annoverati la possibilit di prevenire , monitorare e curare tempestivamente eventuali effetti collaterali che possano insorgere durante lassunzione di contrasto per via orale , in relazione al parziale assorbimento dello stesso dalle pareti intestinali [ 24 ]  . questo studio presenta dei limiti . 
in primo luogo abbiamo arruolato un numero relativamente limitato di pazienti ; tuttavia , gli ottimi risultati ottenuti pongono le basi per il perfezionamento del protocollo di preparazione intestinale sempli cata , e per lesecuzione di ulteriori studi che arruolino un numero pi ampio di pazienti . 
secondo , la colonscopia tradizionale stata eseguita solo nei pazienti con rilievi positivi alla colon - tc e di conseguenza il reale impatto dei rilievi falsi negativi pu essere stato sottostimato , rendendo poco attendibili le stime di accuratezza globale . 
orsi1 1interventional radiology unit of european institute of oncology , via ripamonti 435 , 20141 milan , italy 2clinical center for tumor therapy of 2nd hospital of chongqing university of medical sciences , chongqing 400010 , china 3division of senology of european institute of oncology , via ripamonti 435 , 20141 milan , italy 4school of medicine , university of milan , milan , italy correspondence to : g . 
 from september 2008 to april 2009 , 22 patients with 29 lesions were treated : nine patients with liver and / or softtissue metastases from colorectal carcinoma ( crc ) , six with pancreatic solid lesions , three with liver and / or bone metastases from breast cancer , one with osteosarcoma , one with muscle metastasis from lung cancer , one with iliac metastasis from multiple myeloma and one with abdominal liposarcoma . 
the mean diameter of tumours was 4.2 call patients were evaluated 1 day , 1 month and 3 months after hifu treatment by multidetector computed tomography ( mdct ) , positron - emission tomography ( pet ) - ct and clinical evaluation . 
da settembre 2008 ad aprile 2009 sono stati trattati 22 pazienti con 29 lesioni : 9 pazienti con metastasi epatiche e / o dei tessuti molli da carcinoma del colon retto ( crc ) , sei pazienti con lesioni solide del pancreas , tre con metastasi epatiche e / o ossee da tumore mammario , uno con osteosarcoma , uno con metastasi muscolare da tumore del polmone , uno con lesione iliaca da mieloma multiplo ed uno con liposarcoma addominale . 
il diametro medio era di 4 , 2 ctutti i pazienti sono stati valutati ad 1 giorno , 1 mese e a 3 mesi di distanza dal trattamento hifu con tomogra a computerizzata multidetettore ( mdct ) , tomogra a computerizzata con tomogra a ad emissione di positroni ( pet - ct ) e valutazione clinica . 
pet - ct e / o mdct hanno mostrato risposta completa in 11 / 13 metastasi epatiche ; tutte le lesioni ossee , dei tessuti molli e radiol med ( 2011 ) 116 : 734748 ablated at mri . 
according to our preliminary experience in a small number of patients , we conclude that hifu ablation is a safe and feasible technique for locoregional treatment and is effective in pain control . keywords high - intensity focused ultrasound ( hifu ) solid tumours ablation le lesioni pancreatiche sono state palliate nei sintomi , con risposta completa allesame pet - ct , mdct o risonanza magnetica ( rm ) ; il liposarcoma ha mostrato una ablazione quasi completa allesame rm . 
secondo la nostra esperienza preliminare da un limitato numero di pazienti , lablazione usghifu pu essere considerata una metodica sicura e fattibile in assenza di alternative terapeutiche locoregionali e valida per il controllo del dolore . parole chiave ultrasuoni focalizzati ad elevata intensit ( hifu ) tumori solidi ablazione introduction introduzione high - intensity focused ultrasound ( hifu ) is a highly precise medical procedure that burns and destroys tumour tissue selectively and without harming overlying and adjacent structures within the path of the beathe possibility that fu therapy might be developed as a result of controlling local heating phenomena was introduced by lynn et al . 
the advent of more sophisticated imaging has led to a resurgence of interest in hifu . currently , both b - mode ultrasonography ( us ) and magnetic resonance imaging ( mri ) have been incorporated into hifu devices . 
in the past few years , several clinical hifu projects have been conducted by various research groups , and signi cant results showed that hifu treatment would be safe , effective and feasible in clinical application [ 36 ]  . 
experience from chinese authors with us - imaging - guided hifu ( usghifu ) for treating solid malignant tumours includes primary and metastatic liver cancer , malignant bone tumour , breast cancer , soft - tissue sarcoma , kidney cancer , pancreatic cancer and bone metastatic tumours [ 717 ]  . 
the group from chongqing , china , reported the largest series of hifu clinical applications to date , in which 1 , 038 patients were treated with usghifu in ten centres with both curative and palliative purposes [ 6 ] , showing promising results . 
using either radiological gli ultrasuoni focalizzati ad alta intensit ( hifu ) rappresentano una tecnica altamente precisa che consiste nellutilizzo di ultrasuoni focalizzati per bruciare e distruggere il tessuto tumorale situato in profondit nel corpo , in modo selettivo e senza danneggiare le strutture interposte nel percorso del fascio . 
negli anni passati sono stati condotti diversi progetti clinici hifu da vari gruppi di ricerca e i risultati pi signi cativi hanno dimostrato che il trattamento hifu sarebbe stato sicuro , ef cace e realizzabile nellapplicazione clinica [ 36 ]  . 
lesperienza degli autori cinesi con lhifu che utilizza la guida ecogra ca ( usghifu ) nel trattamento dei tumori solidi maligni include il tumore epatico primitivo e metastatico , il tumore osseo maligno , il cancro della mammella , il sarcoma dei tessuti molli , il tumore renale , il tumore del pancreas e i tumori ossei metastatici [ 717 ]  . 
il gruppo di chongqing no ad oggi ha riportato il maggior numero di applicazioni cliniche per hifu , nelle quali 1038 pazienti sono stati tratti con hifu sotto guida ecogra ca sia con nalit curative che palliative [ 6 ] , mostrando risultati promettenti . 
i risultati hanno mostrato che lablazione 736 radiol med ( 2011 ) 116 : 734748 images , such as mri and contrast - enhanced ultrasound ( ceus ) , 20 of 22 were assessed . 
the results revealed that the adverse event pro le was favourable when compared with open or minimally invasive techniques [ 5 ]  . however , at the present time , there is no report on hifu treatment for solid malignant tumours from a european cancer referral centre for de ning the clinical and technical indications for this technique . 
the aim of our study was to de ne the safety and feasibility of usghifu for treating different type of solid malignant tumours . materials and methods patients this study was de ned as part of the institutional guideline on the minimally invasive management of solid tumours at the european institute of oncology , milan , italy . 
a speci c written informed consent was signed by every patient before selection and treatment . from september 2008 to april 2009 , 22 patients ( eight men and 14 women , age range 1675 years , mean age 61.3 years ) were enrolled . 
all patients were deemed not to be candidates for surgery because of comorbidities ( cardiac and / or renal failure ) and / or local advanced disease , nor suitable radiofrequency ablation ( rfa ) owing to the presence of major blood vessels close to the tumour , tumour location adjacent to viscera ( such as the bowel or gallbladder ) or because of patient refusal to undergo any of those treatments . 
there were ve patients with liver metastases from colorectal cancer ( crc ) , two with chest wall metastasis from crc , one with liver and lung metastases from crc , one with soft - tissue metastasis from crc , one with liver metastasis from breast cancer , one with liver and sternum metastases from breast cancer , one with rib metastasis from breast cancer , one with osteosarcoma , one with leg metastasis from lung cancer , one with iliac metastasis from multiple myeloma , one with abdominal liposarcoma and six with pancreatic lesions . 
with the aim of palliation , we performed hifu on three patients with pancreatic adenocarcinoma and three with pancreatic neuroendocrine tumour ( net ) ; ve of those patients were at the advanced stage with no con ultrasuoni focalizzati con guida rm per lablazione dei bromi uterini fattibile e sicura [ 10 , 11 ]  . 
 attualmente tuttavia , non esiste alcun report sul trattamento hifu dei tumori solidi maligni prodotto da un centro oncologico di riferimento europeo nalizzato alla de nizione delle indicazioni cliniche e tecniche per questa tecnologia . 
 lo scopo del nostro studio stato quello di de nire sicurezza e fattibilit del usghifu nel trattamento di diversi tipi di tumori solidi maligni . materiali e metodi pazienti lo studio stato incluso nelle linee guida istituzionali per il trattamento mininvasivo dei tumori solidi allistituto europeo di oncologia ( milano , italia )  . 
da settembre 2008 ad aprile 2009 stato incluso in questo studio un totale di 22 pazienti ( 8 maschi e 14 femmine , range det 1675 anni , et media 61 , 3 anni )  . 
tutti i pazienti inclusi nello studio non erano n candidabili a chirurgia a causa di comorbilit ( insuf cienza cardiaca e / o renale ) o malattia in stato avanzato , n a radiofrequenza per la vicinanza di grossi vasi alle lesioni da trattare , di visceri cavi come intestino o colecisti o erano stati esclusi per tali trattamenti . tutti i pazienti avevano un punteggio sulla scala di performance di karnofsky di almeno il 70% , in assenza di controindicazioni a sottoporsi ad anestesia generale . 
 tra i 22 pazienti , si segnalano 5 metastasi epatiche da cancro del colon - retto ( crc ) , due metastasi alla parete toracica da crc , un paziente con metastasi epatiche e polmonari da crc , uno con metastasi ai tessuti molli da crc , uno con metastasi epatiche da carcinoma della mammella , uno con metastasi epatiche e sternali da carcinoma mammario , uno con secondarismo costale da carcinoma mammario , uno con osteosarcoma , un paziente con metastasi agli arti inferiori da tumore polmonare , uno con localizzazioni iliache da mieloma multiplo , uno con liposarcoma addominale e sei radiol med ( 2011 ) 116 : 734748 indication for surgical resection , and one had local relapse after surgery . all the lesions scheduled to be treated were detectable at us , and the diagnoses were con rmed with ct / us - guided histology . 
these patients suffered from recurrent episodes of severe nightly hypoglycaemia leading to unconsciousness , episodes that conservative medical therapy with diazoxide ( 300 mg daily ) failed to control . all pancreatic cancer patients had chemotherapy and radiotherapy with advanced local disease at the time of hifu treatment . 
one patient only , admitted with a poor performance status , received supportive care with nonsteroidal anti - in ammatory drugs and narcotic analgesics because she was not a candidate for either chemotherapy for renal failure or surgical resection because of the encasement of main vessels by the tumour . 
 table 1 characteristics of the 22 patients treated with high - intensity focused ultrasound ( hifu ) table 1 caratteristiche dei 22 pazienti trattati con ultrasuoni focalizzati ad elevata intensit ( hifu ) characteristics no . 
di pazienti m / f et ( anni ) valore mediosd dimensione delle lesioni ds , deviazione standard 8 / 14 61.312.5 120 cm 8 / 14 61.312.5 120 cm pazienti con lesioni pancreatiche . 
con nalit palliativa abbiamo eseguito hifu su tre pazienti con adenocarcinoma pancreatico e su tre pazienti con tumore neuro - endocrino ( net ) pancreatico , cinque dei quali in stadio avanzato senza alcuna indicazione alla chirurgia ; un paziente ha mostrato recidiva locale dopo la chirurgia . 
 tutte le lesioni in programma di trattamento erano riconoscibili in ecogra a e la diagnosi stata confermata con esame istologico eseguito sotto guida ecogra ca o della tomogra a computerizzata ( tc )  . 
questi pazienti soffrivamo di episodi ricorrenti di grave ipoglicemia notturna con perdita di coscienza e la terapia medica conservativa con diazoxide ( 300 mg al giorno ) non era in grado di controllare gli episodi notturni di ipoglicemia . 
solo un paziente , incluso nello studio con un basso perfomance status , ha ricevuto terapie di supporto con farmaci antinammatori non steroidei e analgesici narcotici dal momento che non era candidato n alla chemioterapia per insuf cienza renale , n alla resezione chirurgica dal momento che il tumore in ltrava i vasi principali . 
in tutti i pazienti con tumore pancreatico e con metastasi ossee e ai tessuti molli non si era veri cato alcun miglioramento del dolore correlato al cancro nei precedenti trattamenti . 
le caratteristiche dei tumori sono mostrate nella tabelle 1 e 2 . preparazione pre - trattamento esami di routine e preparazioni pre - trattamento sono stati condotti in accordo ai principi della chirurgia . 
prima del trattamento sono stati eseguiti i convenzionali test biochimici epatici , tempo di protrombina , emocromo completo , radiogra a del torace , ecogra a addominale , elettrocardiogramma ( ecg ) ; la funzionalit polmonare stata valutata prima del trattamento . 
stato necessario eseguire una adeguata preparazione intestinale table 2 characteristics of the 22 patients with 29 tumours treated with high - intensity focused ultrasound ( hifu ) site number of tumours patients per i pazienti con tumore pancreatico e per i pazienti con tumori addominali in adiacenza alle anse intestinali . 
ai pazienti stato richiesto il digiuno notturno il giorno prima del trattamento hifu . radiol med ( 2011 ) 116 : 734748 738 liver bone soft tissue pancreas lung total fegato osso tessuti molli pancreas polmone totale table 2 caratteristiche dei 22 pazienti con 29 neoplasie trattati con ultrasuoni focalizzati ad elevata intensit ( hifu ) sede numero delle lesioni pazienti conventional liver biochemical tests , prothrombin time and complete blood cell counts , chest radiography , abdominal us , electrocardiogram ( ecg ) and lung function were evaluated before treatment . 
a mylab70 us imaging device ( esaote , genoa , italy ) coupled with the hifu machine was used as the real - time imaging unit of the systethis 1.08.0 - mhz imaging probe is situated in the centre of the hifu transducer and may allow for realtime us image monitoring during treatment . skin surface overlying the lesion was shaved in every patient to avoid the presence of hairs within the acoustic pathway ; the same skin surface was also degassed by using a vacuum cup aspiration device and degreased with 95 alcohol . 
lenergia terapeutica focalizzata degli ultrasuoni stata prodotta da un trasduttore di 20 cm di diametro con lunghezza focale di 15 cm , prodotti ad una frequenza di 0 , 8 mhz . 
un dispositivo di imaging ad ultrasuoni mylab 70 ( esaote , genova , italia ) , accoppiato con la macchina hifu , stato utilizzato per ottenere immagini in tempo reale . 
questa sonda da 1 , 08 , 0 collocata nel centro del trasduttore di ultrasuoni focalizzati ad alta intensit e permette il monitoraggio del trattamento in tempo reale con limmagine ecogra ca . 
 la super cie corporea che ricopre la lesione stata rasata in ogni paziente , allo scopo di evitare la presenza di peli lungo il percorso acustico ; la stessa super cie stata degassi cata utilizzando un dispositivo di aspirazione a coppa e successivamente sgrassata con alcol a 95 . 
lanestesia generale con intubazione endotracheale e ventilazione meccanica ha svolto anche il ruolo supplementare di permettere la sospensione provvisoria del respiro con il con controllo polmonare dellinspirio , necessario nellablazione di lesioni epatiche poste posteriormente , rispetto alla gabbia toracica , nello spazio intercostale . 
dopo lanestesia , i pazienti sono stati posizionati con cura sopra il letto di trattamento , con particolare attenzione al corretto posizionamento della supercie corporea in corrispondenza della lesione da trattare , a contatto con lacqua degassi cata . 
per tutti i pazienti durante la procedura stato effettuato il monitoraggio respiratorio e della frequenza cardiaca , della pressione sanguigna , della saturazione dellossigeno e dellanidride carbonica . sia per la piani cazione pre - trattamento che per la sonazione stata selezionata la modalit di scansione ad ultrasuoni su di un piano sagittale ; il trattamento stato eseguito con rilascio di energia sia con modalit puntiforme che lineare . 
a ultrasound ( us ) image obtained before high - intensity focused us ( hifu ) treatment shows a small lesion ( bold arrow ) close to the inferior vena cava ( ivc )  . 
b immagine ecogra ca ottenuta immediatamente al termine dellablazione hifu mostra una iperecogenicit a livello dellarea trattata ( freccia )  . anaesthesia to prevent the patient from experiencing pain or discomfort and ensure immobility . 
general anaesthesia with endotracheal intubation and mechanical ventilation also has the supplementary bene t of permitting provisional suspension of breath with controlled pulmonary in ation , as is required for ablating liver lesions behind the rib cage through the intercostal space . 
treatment powers of 60400 w were used for the different tumour types and sites . evaluation of therapeutic ef cacy patients were evaluated by pet - ct , mri , or / and mdct and clinical evaluation . 
in three patients with liver lesions and one with pancreatic cancer , contrast - enhanced ultrasound ( ceus ) was performed at the end of the procedure to assess the vascular feeding after hifu ablation . 
to exclude major complications and evaluate treatment ef cacy , patients underwent mdct within the rst 24 h after hifu treatzate potenze di trattamento da 60 a 400 w in relazione alle diverse tipologie e posizioni dei tumori . valutazione dellef cacia terapeutica i pazienti sono stati valutati con pet - tc , rm e / o tcmd e con la valutazione clinica . 
tutti i pazienti sono stati sottoposti a [ 18f ] uorodesossiglucosio ( fdg ) - pet - tc e / o a tcmd o rm addominale dopo 3 o 4 settimane e a 3 mesi dopo la procedura hifu . 
 interpretazione delle indagini pet - tc e tcmd le [ 18f ] - fdg - pet - tc eseguite in condizioni di base e nei controlli successivi sono state interpretate da un medico specialista in medicina nucleare , alloscuro delle condizioni cliniche e dellesame obiettivo del paziente , degli altri reperti di imaging e dei risultati istopatologici . 
la tcmd stata considerata positiva ogni volta venisse riconosciuta iperdensit irregolare attorno al sito della lesione trattata con hifu e / o 740 radiol med ( 2011 ) 116 : 734748 ment . 
all patients then underwent [ 18f ] uorodeoxyglucose ( fdg ) pet / ct and / or abdominal mdct or mri at 34 weeks and 3 months after the hifu procedure . pet / ct and mdct scan interpretation baseline and follow - up [ 18f ] - fdg - pet / ct scans were read by one experienced nuclear medicine physician blinded to the patients clinical status and physical examination , other imaging ndings and histopathological results . 
detection of hypodensity at hifu ablation site without contrast enhancement on the edges was considered as the sign of lesion treatment , and the mdct scan was therefore interpreted as negative . 
we also calculated sonication time , de ned as exposure time , which was related to tumour size , site and blood supply , which ranged from 1 min 38 s to 166 min ( meansd , 37.442.7 min ) ( table 3 )  . 
the fraction of sonication time over treatment time for liver lesions was 14.3%. grey - scale value changes massive grey - scale changes during treatment , interpreted as tissue necrosis by sonication , were observed in 27 of incremento dimensionale dellarea sottoposta a trattamento . 
 il riconoscimento di ipodensit nel sito di ablazione hifu senza incremento di contrasto nei bordi stato considerato come il segno del trattamento e quindi la tcmd stata interpretata come negativa . 
nei quattro pazienti valutati alla ne della procedura con mezzo di contrasto eco ampli catore ( ceus ) , le caratteristiche di vascolarizzazione della lesione sono risultate in accordo con i reperti tcmd ottenuti il giorno successivo . risultati timing i dettagli riguardo alla durata della procedura sono i seguenti . 
il tempo di sala , che include il tempo di preparazione e il tempo di trattamento , de nito dal momento in cui il paziente giunge nella unit hifu no alluscita del paziente dalla sala hifu , compreso tra 2 ore e 30 minuti e 7 ore e 5 minuti . 
il tempo complessivo di trattamento , de nito dal tempo di inizio della localizzazione no allultima sonicazione , variabile tra 59 minuti e 318 minuti ( mediadeviazione standard [ ds ] , 162 , 783 , 0 min )  . 
abbiamo inoltre calcolato il tempo di sonicazione , inteso come tempo di esposizione , correlato alle dimensioni del tumore , sede del tumore e suo apporto vascolare , variabile da 1 minuto e 38 secondi a 166 minuti ( mediads , 37 , 442 , 7 minuti ) ( tabella 3 )  . 
per 11 pazienti con 13 lesioni epatiche : la media del trattamento complessivo stata di 107 , 2 minuti ( range : 59170 ) ; il tempo medio di sonazione stato di 15 , 3 minuti ( range : 1 , 640 , 7 )  . 
il rapporto tra il tempo di sonazione e il tempo di trattamento stato del 14 , 3% . modi che dei valori nella scala di grigi in 27 delle 29 lesioni ( 93 , 1% ) si veri cata unimportante modi ca dei valori della scala di grigi durante il trattamento , interpretata come necrosi tissutale causata dalla sonazione . 
 radiol med ( 2011 ) 116 : 734748 table 3 data on high - intensity focused ultrasound ( hifu ) procedure performed on 22 patients with solid tumours ( mean valuestandard deviation ) tumour site no . 
grey - scale changes were not observed in two liver metastases . postprocedure evaluation and short - term follow - up mdct or mri performed 1 day after hifu showed complete response in 20 / 22 patients without any injury of the surrounding organs ; as a precautionary measure , all patients were observed in hospital for 2 nights . 
mdct / mri at 24 h after treatment detected no injury of the surrounding organs , and all patients were observed in hospital for 3 days as a precautionary measure . 
amylase levels showed no signi cant elevation over baseline during the 3 days after treatment . the huge retroperitoneal before hifu , all 14 patients with pancreatic tumour and valutazione post - procedura e follow - up a breve tempo la tcmd o la rm eseguite un giorno dopo hifu hanno mostrato completa risposta in venti dei ventidue pazienti senza alcun danno agli organi adiacenti ; tutti i pazienti in via precauzionale sono stati trattenuti in ospedale per due notti . 
la tcmd / rm a 24 ore non ha identi cato alcun danno degli organi adiacenti e tutti i pazienti sono stati trattenuti in via precauzionale in ospedale per 3 giorni dopo il trattamento . prima degli ultrasuoni focalizzati ad alta intensit , tutti i 14 pazienti con tumore pancreatico , lesioni ossee e dei tessuti molli lamentavano dolore cronico per cui era necessaria la somministrazione per via orale di farmaci antidolori ci . 
in tutti i pazienti si osservata riduzione del dolore con remissione completa ( senza necessit di farmaci antidolori ci oppioidi ) entro 2448 ore dalla singola sessione di ultrasuoni focalizzati . 
b lesame tc con mezzo di contrasto eseguito 24 ore dopo trattamento hifu mostra unarea ipodensa priva di contrast enhancement , in corrispondenza della pregressa lesione , in assenza di tessuto patologico residuo . 
b il controllo pet - tc ad un mese mostra la scomparsa di attivit metabolica a livello della lesione ( freccia )  . bone and soft tissues lesions complained of chronic pain that necessitated management with oral analgesic drugs . 
a follow - up postinterventional fasting test was not performed because remission was determined clinically of the basis of the disappearance of the hypoglycaemic episodes and reduction of tumour vascularity at follow - up mdct . stata stabilita dai dati clinici in assenza di ulteriori episodi di ipoglicemia e dalla riduzione nei controlli successivi della vascolarizzazione dei tumori valutata con tcmd . eventi avversi tutti i pazienti sono stati dimessi dopo un intervallo da 1 a 3 giorni di osservazione . 
ledema locale nel sito di esposizione della cute stato lunico effetto collaterale osservato , identi cato in 3 pazienti ( due con metastasi della parete toracica e uno con liposarcoma retro peritoneale )  . 
b controllo pet - tc ad 1 mese con evidente scomparsa dellattivit metabolica in corrispondenza della lesione ( freccia )  . adverse events all patients were discharged after 13 days of observation . 
local oedema at the level of exposed skin surface was the only side effect observed , and it was detected in three patients ( two with chest wall metastases and one with retroperitoneal liposarcoma )  . 
no other postprocedural side effects were observed . one 61 - year - old woman with a liver metastasis located at segment ii showed after 2 months an extrahepatic and subcutaneous sterile in ltration . 
the patient continued to receive chemotherapy , and after 5 weeks , she experienced local pain without high fever , and us and mdct showed a subcutaneous in ltration from liver necrosis . 
no other hifu - related adverse effects were observed after 3 months of follow - up in the responders . discussion minimally invasive therapies , such as radiofrequency locale senza febbre alta e lecogra a e la tcmd hanno mostrato in ltrazione sottocutanea da necrosi epatica . 
nessun altro evento avverso correlato allhifu stato osservato dopo tre mesi di follow - up in questi pazienti che hanno risposto alla terapia . discussione le terapie mininvasive , come la radiofrequenza , la chemioembolizzazione , la crioablazione , lablazione a microonde , la termoterapia interstiziale laser e lhifu , sono state usate per lablazione dei tumori solidi . 
la chirurgia lo standard terapeutico attuale per i pazienti con metastasi epatiche da tumori colorettali , offrendo la possibilit di una radicalit completa con la resezione [ 12 ]  . 
7a , b immagine tc della paziente con metastasi epatica al iv segmento da tumore mammario 1 mese dopo trattamento hifu ( a ) che mostra in ltrato sottocutaneo da necrosi epatica e 3 mesi ( b ) dopo con riassorbimento quasi completo . 
 ablation ( rfa ) , transcatheter arterial chemoembolisation ( tace ) , cryoablation , microwave coagulation , laserinduced interstitial thermotherapy and hifu , have all been used to ablate solid tumours . 
surgery is the current standard of care in patients with colorectal liver metastasis , as resection offers the chance of a complete cure [ 12 ]  . local ablative techniques , such as rfa , cryoablation , microwave coagulation and laser - induced interstitial thermotherapy , also offer potential local tumour control and occasionally achieve long - term disease - free survival [ 1315 ]  . 
a study with a small number of patients has shown that hifu is safe and feasible for treating pancreatic cancer [ 4 ]  . our results show that hifu is safe and could be used to treat solid malignancies . 
local oedema was the most le tecniche di ablazione locale come la radiofrequenza , la crioablazione , lablazione a microonde e la termoterapia interstiziale laser permettono un controllo locale di malattia ed occasionalmente portano a lunghi intervalli di sopravvivenza senza malattia [ 1315 ]  . 
uno studio con un numero limitato di pazienti ha dimostrato che hifu fattibile e privo di complicanze nel trattamento di tumori pancreatici [ 4 ]  . i nostri risultati hanno dimostrato che lablazione con tecnica hifu sicura e pu essere impiegata per il trattamento dei tumori solidi . 
earlier studies reported mild discomfort or local pain was seen in 5480% of treated patients [ 5 , 19 ] , but in our study , no patients reported discomfort or local pain 1 day after hifu treatment . 
a low - grade fever was another common adverse effect in earlier studies [ 5 ] , but we did not observe low - grade fever in any of our patients . 
this event was probably related to the chemotherapy with antiantigenetic drugs that the patient received after hifu . as this was a feasibility study , we enrolled patients who were treated for different purposes and did not focus on the long - term effects of treatment but only evaluated the patients at 1 day and 34 weeks after treatment . 
we treated a total of 13 liver lesions in eight patients ; pet - ct or / and mdct showed that 11 of 13 ( 87.5% ) were completely ablated . 
higher power and more energy are needed for ablating tumours close to the major blood vessels because of the cooling effects from great vessels [ 17 , 20 ]  . our results show that us grey - scale values are reliable to de ne coagulation necrosis . 
studi precedenti al nostro hanno descritto moderato fastidio o dolore locale in 54%80% del pazienti trattati [ 5 , 19 ] , ma nella nostra esperienza non abbiamo avuto pazienti con fastidio o dolore locale il giorno dopo il trattamento . 
tale evento probabilmente da relazionare al trattamento chemioterapico con farmaci antiangiogenetici che la paziente ha ricevuto dopo hifu . nellottica di uno studio di fattibilit abbiamo arruolato pazienti trattati con differenti intenti non concentrandoci sui risultati a lungo termine e rivalutando unicamente i pazienti il giorno dopo e 34 settimane dopo il trattamento . 
abbiamo trattato un totale di 13 lesioni epatiche in otto pazienti e la pet - tc e / o la tcmd hanno dimostrato lablazione completa di 11 / 13 ( 87 , 5% )  . 
sono infatti necessarie unenergia ed una potenza maggiori per i trattamenti di lesioni adiacenti grossi vasi per leffetto di raffreddamento indotto dagli stessi [ 17 , 20 ]  . i nostri risultati dimostrano che i valori di scala di grigio corrispondono alla necrosi coagulativa . 
abbiamo calcolato il tempo di allestimento della sala e del trattamento vero e proprio rilevando che il 51% del tempo di allestimento della sala stato utilizzato per la preparazione del paziente . 
il tempo medio complessivo per lablazione di una lesione con diametro medio di 4 , 2 cm ( range , 1 , 020 , 0 ) variato da 59 a radiol med ( 2011 ) 116 : 734748 treatment time for ablating a mass with a mean diameter of 4.2 cm ( range 1.020.0 ) ranged from 59 min to 318 min ( meansd , 162.783.0 min ) , which is still longer than desirable ( table 3 )  . 
even improving us lesion targeting may result in a shorter treatment time . this study was limited to a small number of patients and short - term follow - up because its aim was to assess the feasibility of this new technique . 
additional studies to compare hifu with other available techniques , such as transcatheter arterial embolization ( tae ) and rfa , are important to allow selection of the most appropriate therapy for individual patients . conclusions the results of this study demonstrate that usghifu can achieve locoregional tumour ablation without signi cant side effects and in fact appears to be feasible and safe for the ablation of solid lesions . 
even though the relative risks and bene ts of hifu ablation must be rigorously measured to better de ne its role in clinical practice in the treatment of solid tumours , we believe it can be used as a cytoreductive measure in an adjuvant setting ( debulking effect ) with the aim of achieving better palliation , especially in locally advanced pancreatic malignancies and bone and soft - tissues lesions . 
however , further studies , such as randomised controlled trials , are needed to select a patient group that would be the best candidate for this noninvasive treatment . 318 minuti ( mediads , 162 , 783 , 0 minuti ) che sempre pi di quanto sia desiderabile ( tabella 3 )  . 
anche il miglioramento nella ricerca della lesione target con gli ultrasuoni pu ridurre ulteriormente i tempi . lo studio attuale limitato ad un numero di pazienti ridotto con un follow - up breve poich nato come valutazione di fattibilit di una nuova tecnica . 
la sopravvivenza ed il tasso di recidiva non sono stati i nostri obiettivi principali ma ulteriori studi in futuro sono necessari per de nire il reale bene cio di questa tecnica . 
paragonandola tuttavia con altre tecniche ablative come lembolizzazione arteriosa e la radiofrequenza ulteriori studi potranno de nire in maniera mirata il trattamento pi adeguato per ogni singolo paziente . conclusioni i risultati di questo studio dimostrano che il trattamento ad ultrasuoni focalizzati eco guidato permette di ottenere un trattamento di tipo loco - regionale senza signi cativi effetti collaterali . 
 anche se il rapporto tra rischi ed i bene ci dellablazione con tecnica hifu devono essere ancora testati per meglio de nire il suo ruolo nella pratica clinica nel trattamento dei tumori solidi , pensiamo che possa essere impiegato con intento citoriduttivo in un contesto adiuvante ( debulking effect ) con lo scopo di una migliore palliazione , in particolare nelle neoplasie pancreatiche localmente avanzate , nelle lesioni ossee e dei tessuti molli . 
lanzara , sezione di radiodiagnostica , seconda universit degli studi di napoli , piazza miraglia 4 , 80100 napoli , italy 3dipartimento di scienze biomorfologiche e funzionali , universit degli studi federico ii di napoli , via pansini 5 , 80134 napoli , italy correspondence to : a . 
our study population comprised 167 ( 91 male , 76 female patients , age range 11 months to 82 years ; mean age 29 years ) out of 1 , 896 patients with throat swab positive for h1n1 and clinical and laboratory ndings indicative of viral in uenza . 
all 167 patients were studied by chest x - ray ( cxr ) , and 20 patients with positive cxr and worsening clinical condition also underwent computed tomography ( ct )  . 
 abnormalities identi ed on cxr , variously combined and distributed , were as follows : 53 ir , 5 n , 13 ggo , 50 cons ; the predominant combination was represented by six ggo with cons . 
 the abnormalities identi ed on ct , variously combined and distributed , were as follows : 14 ir , 2 n , 5 ggo ; the predominant combination was 10 ggo with cons . 
centosessantasette su 1896 casi risultati positivi al tampone faringeo per h1n1 ( 91 m , 76 f , range et 11 mesi82 anni , et media 29 anni ) , con alterazioni clinico - laboratoristiche di in uenza virale , hanno costituito la popolazione del nostro studio . 
tutti i 167 pazienti hanno eseguito radiogra a ( rx ) del torace ; per le pi gravi condizioni cliniche , 20 casi positivi alla rx del torace hanno effettuato tomogra a computerizzata ( tc ) del torace . 
le lesioni polmonari identi cate alla rx , variamente associate e distribuite , sono state : 53 ri , 5 n , 13 ogg , 50 cm ; 6 ogg con cm rappresentavano lassociazione predominante . 
le lesioni polmonari identi cate alla tc , variamente associate e distribuite , sono state : 14 ri , 2 n , 5 ogg ; 10 ogg con cm rappresentavano lassociazione predominante . 
sebbene differentemente identi cati in rx e tc , i segni di sovrainfezione batterica pi frequenti sono stati tree - in - bud , cm con radiol med ( 2011 ) 116 : 706719 bronchogram , and pleural and pericardial effusion . 
la rx e la tc del torace hanno identi cato sede ed estensione delle lesioni polmonari , documentando i segni di sovrainfezione batterica e le complicanze polmonari . keywords in uenza a virus h1n1 subtype computed tomography x - ray pneumonia viral parole chiave virus dellin uenza a sottotipo h1n1 tomogra a computerizzata rx polmonite virale introduction introduzione swine - origin in uenza or swine in uenza ; swine u is an acute respiratory infection caused by the novel in uenza a , subtype h1n1 , which was transmitted to humans from pigs in mexico and the united states in march and april 2009 and rapidly spread worldwide [ 1 , 2 ]  . 
h1n1 virus is a subtype of the in uenza a virus that belongs to the orthomyxoviridae family , of which numerous variants exist that cause u pandemics among animals , such as bird u and swine u . 
genetic analyses suggest that the emergence of the novel h1n1 strain of swine u in humans is the direct consequence of a reassortment of the viral genomes of swine u , bird u and human u in north america and eurasia [ 36 ]  . 
in june 2009 , following the report of the rst human - to - human transmission in two countries in one world health organization ( who ) region and the rapid spread of the virus , the who declared a level - 6 pandemic alert [ 6 , 7 ]  . 
high fever , sore throat , cough , fatigue , joint pain , nausea , vomiting and / or diarrhoea are the principal symptoms of h1n1 in uenza ; more complex cases present with respiratory failure [ 1 , 6 , 8 ]  . 
the speci c tropism of the virus for the respiratory tract has led to the use of imaging to better characterise the location , distribution and type of the primary pulmonary lesions [ 9 ]  . 
chest x - ray ( cxr ) and chest computed tomography ( ct ) have been the investigations of choice for identifying and quantifying , respectively , pulmonary damage in patients affected by in uenza a [ 1012 ]  . 
the aim of this paper is to describe the radiological and clinical ndings in patients hospitalised for a diagnosis of suspected h1n1 swine - origin in uenza . lin uenza virale a di origine suina ( s - oiv , swine - origin in uenza o swine in uenza o swine u ) rappresenta una patologia respiratoria acuta causata dal nuovo sottotipo di virus in uenzale h1n1 , trasmesso alluomo da alcuni allevamenti di maiali del messico e degli stati uniti nei mesi di marzo ed aprile 2009 e diffusosi rapidamente nellintero globo [ 1 , 2 ]  . 
il virus in uenzale h1n1 un sottotipo di in uenzavirus a appartenente alla famiglia delle orthomyxoviridae , di cui sono note numerose varianti che , negli animali , causano forme in uenzali pandemiche , come lin uenza aviaria e la febbre suina . 
analisi genetiche suggeriscono che la comparsa della nuova linea h1n1 dellin uenza suina nelluomo sia diretta conseguenza di un riassortimento dei genomi virali dellin uenza suina , aviaria ed umana del nord america e delleurasia [ 36 ]  . 
 nel mese di giugno 2009 , in seguito alla documentazione pubblicata da parte della organizzazione mondiale della sanit ( oms ) del primo contagio interumano in due stati e alla rapida diffusione del virus , stato dichiarato lo stato di emergenza mondiale di scala 6 ( pandemia in uenzale ) [ 6 , 7 ]  . 
febbre elevata , faringodinia , tosse , astenia , artromialgie , nausea , vomito e / o diarrea hanno costituito i principali sintomi desordio clinico dellin uenza h1n1 ; nei casi pi complessi insorta insuf cienza respiratoria acuta [ 1 , 6 , 8 ]  . 
il peculiare tropismo virale per lapparato respiratorio ha determinato il ricorso alle tecniche di imaging per meglio caratterizzare sede , distribuzione e tipologia delle lesioni elementari polmonari [ 9 ]  . 
 lesame radiogra co del torace ( rx ) e la tomogra a computerizzata ( tc ) del torace hanno rappresentato le indagini 708 materials and methods between may and mid - november 2009 , 3 , 649 patients with suspected swine - origin in uenza a virus infection presented to our hospital . 
the diagnosis of h1n1 viral in uenza was con rmed in 1 , 896 / 3 , 649 ( 51.9% ) cases by reverse transcriptase polymerase chain reaction ( rt - pcr ) for detection of viral rna in pharyngeal swabs . 
 cxr was performed on all 167 patients , 20 of whom ( 11.9% ) were also studied by ct to assess equivocal ndings on cxr or discrepancies between the cxr and clinical ndings . 
cxr was performed using the standard technique ( posteroanterior projection : 10 mas , 70 kv ; lateral projection : 60 mas , 80 kv ; lm - focus distance 180 cm ) with the patient in standing position in 150 cases ( 89.9% ) ; only 17 patients ( 10.1% ) were imaged in a sitting or lying position and with anteroposterior projection due to an inability to maintain a standing position and / or inspiration . 
 ct study was performed with a 64 - detector - row ct scanner immediately after the cxr in 11 / 20 cases and 24 h after cxr in the remaining 9 / 20 cases . 
on clinical request , 18 / 20 patients 12 / 20 large and 6 / 20 poorly cooperative patients underwent unenhanced chest and abdominal ct with the spiral technique : breath - hold volumetric scans , slice thickness 1 mm , kv 120 , ma 180 , pitch 1 . 
only 2 / 18 patients with suspected pulmonary embolism were subsequently imaged after intravenous administration of nonionic iodinated contrast material with the sure start technique at a ow rate of 3 ml / s and dose of 100 ml . 
the resulting ct images were viewed with a lung window ( width 1 , 500 hu , level 700 hu ) and mediastinal window ( width 350 hu , level 40 hu )  . 
the remaining 2 / 20 patients were studied with high - resolution ct of the chest for clinical suspicion of concurrent interstitial pulmonary disease using a standard protocol : collimation 1 mm , interval 10 mm , acquisition time 12 s , high - spatial - frequency reconstruction algorithm , matrix 512 512 , 120 kv , 200 ma , fov encompassing both lungs , window level 600 hu ( range 500 / 900 hu ) , window width 1 , 500 hu ( range 1 , 100 / 2 , 000 hu ) , expiratory scans and patient in prone position when needed . 
two radiologists independently examined and interpreted the cxr and ct images stored in the picture archiving and communications system ( pacs )  . the primary lesions assessed at cxr and chest ct were radiol med ( 2011 ) 116 : 706719 di riferimento ai ni rispettivamente dellindividuazione e quanti cazione del danno polmonare nei pazienti affetti da in uenza virale a [ 1012 ]  . 
scopo del nostro studio de nire il quadro radiologico e clinico dei pazienti ospedalizzati per diagnosi di in uenza virale h1n1 di origine suina . materiali e metodi dal mese di maggio alla met di novembre 2009 , 3649 pazienti con sospetta in uenza virale a di origine suina si sono presentati presso il nostro presidio ospedaliero . 
la diagnosi di in uenza virale h1n1 stata confermata in 1896 / 3649 ( 51 , 9 % ) casi con tecnica reverse transcription - polymerase chain reaction ( rt - pcr ) , mediante ricerca dellrna virale nel materiale prelevato con tampone faringeo . 
di essi , 167 / 261 ( 63 , 9% ) pazienti sono stati sottoposti ad indagini diagnostiche strumentali a causa del persistere e / o dellaggravarsi della sintomatologia respiratoria dopo terapia medica da almeno 3 giorni . 
 hanno eseguito lesame radiogra co del torace 167 pazienti e , di essi , 20 ( 11 , 9% ) sono stati sottoposti ad esame tc , al ne di valutare reperti dubbi o discordanti fra rx del torace e manifestazioni cliniche . 
lesame radiogra co del torace stato effettuato mediante tecnica standard ( proiezione postero - anteriore [ pa ] : 10 mas , 70 kv ; proiezione latero - laterale [ ll ] : 60 mas , 80 kv ; distanza tubo - paziente 180 cm ) ed in posizione ortostatica in 150 casi ( 89 , 9% ) ; solo in 17 casi ( 10 , 1% ) sono stati effettuati radiogrammi in posizione seduta o sdraiata ed in proiezione antero - posteriore ( ap ) per incapacit da parte dei pazienti a mantenere la posizione ortostatica e / o linspirio . 
 lindagine tc stata eseguita mediante apparecchiatura tc multidetettore ( tcmd ) a 64 le di detettori subito dopo la rx del torace in 11 / 20 casi , dopo 24 ore dallesame radiogra co in 9 / 20 casi . 
su richiesta clinica , 18 / 20 pazienti , di cui 12 / 20 di elevata taglia corporea e 6 non collaboranti , sono stati sottoposti ad esame tc torace ed addome senza somministrazione di mezzo di contrasto endovena mediante tecnica spirale : scansioni volumetriche in inspirio , spessore di strato di 1 mm , kv 120 , ma 180 , pitch 1 . 
solo in 2 / 18 pazienti , per sospetto di embolia polmonare , stato successivamente somministrato mezzo di contrasto iodato non ionico endovena mediante tecnica sure start , velocit di usso 3 ml / s , volume di contrasto 100 ml . 
le immagini tc cos acquisite sono state visualizzate mediante nestra radiol med ( 2011 ) 116 : 706719 de ned according to the fleischner society glossary [ 13 ] and recent publications [ 10 , 11 ] describing the main radiological pulmonary manifestations of a / h1n1 in uenza : interstitial reticulation ( ri ; linear opacities of the central and peripheral interstitium appearing as radio - opaque lines on cxr and hyperdensities on ct ) , nodules ( n ; wellor illde ned , rounded opacities / hyperdensities , with maximum diameter of 3 cm . ) , ground - glass opacities ( ggo ; heterogeneous increase in parenchymal opacity with preservation of bronchial and vascular margins ) , consolidation ( cons ; homogenously increased parenchymal attenuation that obscures the margins of the bronchial and vessels walls )  . 
 images were also assessed for signs of bacterial suprainfection : consolidation with air bronchogram ( area of radiolucency at cxr and low attenuation at ct , re ecting the airlled bronchi on a background of opaque or high - attenuation airless lung ) , cavitations ( gaslled spaces , seen as lucencies or low - attenuation areas within a parenchymal consolidation ) , tree - in - bud pattern ( branching centrilobular structures ) , pleural and / or pericardial effusion ( uid in the pleural / pericardial cavity ) , lymphadenopathy ( short - axis diameter > 1 cm for mediastinal nodes and > 3 mm for hilar nodes )  . 
extent of pulmonary damage was de ned univocally at cxr and chest ct : unilateral or bilateral ; symmetrical or asymmetrical ; focal , multifocal or diffuse ; with predominant distribution in the upper , middle or lower lobes . 
all patients had abnormal blood chemistry results : 157 ( 94% ) elevated erythrocyte sedimentation rate ( esr ) , 150 ( 89.8% ) elevated c - reactive protein ( crp ) , 144 ( 86.2% ) elevated lactate dehydrogenase ( ldh ) , 83 ( 49.7% ) polmonare ( ampiezza di nestra 1500 hu , livello di nestra - 700 hu ) e mediastinica ( ampiezza di nestra 350 hu , livello di nestra 40 hu )  . 
i restanti 2 / 20 pazienti sono stati studiati con tomogra a computerizzata ad alta risoluzione ( hrct ) del torace per sospetto clinico di concomitante interstiziopatia polmonare , mediante protocollo standard di acquisizione : collimazione 1 mm , intervallo di acquisizione 10 mm , tempo di scansione 12 s , algoritmo di ricostruzione ad alta frequenza spaziale , matrice 512512 , 120 kv , 200 ma , eld of view ( fov ) contenente ambedue i polmoni , livello di nestra - 600 hu ( range - 500 / 900 hu ) , ampiezza nestra 1500 hu ( range 1100 / 2000 hu ) , scansioni in espirio ed a paziente prono alloccorrenza . 
due radiologi hanno esaminato ed interpretato indipendentemente le immagini radiogra che e tc del torace custodite nellarchivio picture archiving and communications system ( pacs )  . le lesioni elementari individuate alla rx ed alla tc del torace sono state da noi de nite secondo il glossario della fleischner society [ 13 ] e recenti pubblicazioni [ 10 , 11 ] che hanno descritto le principali manifestazioni radiologiche polmonari dellin uenza a / h1n1 : reticolazione dellinterstizio ( ri : opacit a decorso lineare dellinterstizio centrale e periferico che appaiono come strie radiopache sul radiogramma standard e come iperdensit all indagine tc ) , noduli ( n : opacit / iperdensit rotondeggianti , bene o scarsamente de nite , del diametro massimo di 3 cm ) , opacit ground glass ( ogg : aumento disomogeneo della densit parenchimale con conservazione del pro lo dei bronchi e delle strutture vascolari contestuali ) , consolidamenti ( cm : omogeneo incremento dellattenuazione parenchimale polmonare con mancata de nizione delle pareti bronchiali e vascolari contestuali )  . 
 sono stati individuati , inoltre , i segni di sovra - infezione batterica : consolidamento con broncogramma aereo ( area di radiotrasparenza , al radiogramma standard del torace , e di bassa densit , allesame tc , rappresentata dal contenuto aereo dei bronchi nel contesto di unarea di radiopacit / elevata densit del parenchima polmonare , priva daria ) , cavitazioni ( spazi contenenti aria , visibili come aree di trasparenza o bassa attenuazione nellambito di una consolidazione parenchimale ) , albero in ore o tree - in - bud ( strutture rami cate centro - lobulari ) , versamento pleurico e / o pericardico ( lm uido nel cavo pleurico / pericardico ) , linfoadenopatie ( incremento del diametro corto dei linfonodi mediastinici , se esso > 1 cm , dei linfonodi ilari se esso > 3 mm )  . 
l estensione del danno stata de nita univocamente alla rx ed alla tc del torace : unilaterale o bilaterale ; simmetrica o asimmetrica ; focale , multifocale o diffusa ; a predominante distribuzione nei lobi superiori , 710 radiol med ( 2011 ) 116 : 706719 fig . 
a chest x - ray , posteroanterior projection : diffuse and bilateral thickening of the interstitium , particularly visible in the right lower lung eld , where there is an area of ggo . 
a radiogramma del torace in proiezione pa : ispessimento diffuso e bilaterale dellinterstizio polmonare pi evidente nel campo polmonare inferiore di destra in cui si osserva un addensamento parenchimale del tipo vetro smerigliato . 
none of the patients showed isolated pulmonary consolidation , and none of those studied with contrast - enhanced multidetector - row ct ( mdct ) showed direct and / or indirect signs of pulmonary embolis on cxr , ndings suggestive of bacterial suprainfection were seen in various combinations in 14 / 90 patients ( 15.5% ) ( table 1 ) : pleural effusion in 9 / 14 ( 64.2% ) , consolidation with air bronchogram in 4 ( 28.5% ) , lymphadenopathy in 2 ( 14.2% ) , cavitation in 1 ( 7.1% ) , hydropneumothorax in 1 medi o inferiori . 
ricostruzioni multiplanari ( mpr ) e maximum intensity projection ( mip ) sono state eseguite nel post - processing in tutti i pazienti studiati con scansioni tc volumetriche . risultati dei 167 pazienti studiati 161 ( 96 , 4% ) presentavano febbre , 153 ( 91 , 6% ) cefalea , 143 ( 85 , 6% ) tosse , 58 ( 34 , 7% ) faringodinia , 69 ( 41 , 3% ) diarrea , 57 ( 34 , 1% ) vomito . 
113 / 167 ( 67 , 6% ) pazienti presentavano almeno una condizione clinica patologica pregressa : 76 ( 45 , 5% ) erano affetti da asma , 25 ( 14 , 9% ) erano diabetici , 13 ( 7 , 7% ) presentavano broncopneumopatia cronica ostruttiva ( bpco ) , 23 ( 13 , 7% ) immunosoppressione , 65 ( 38 , 9% ) cardiopatie , 17 ( 10 , 1% ) insuf cienza renale cronica , 11 ( 6 , 5% ) disordini congnitivi , 5 ( 2 , 9% ) patologie neuro - muscolari , 3 ( 1 , 7% ) malformazioni scheletriche , 2 ( 1 , 1% ) gravidanza , 1 ( 0 , 5% ) uso di droghe . 
ct con rmed the cxr ndings of bacterial suprainfection in 9 cases ( 9 / 14 , 64.2% ) and identied as false positive ve cases of suspected pleural effusion detected on cxr . 
a chest x - ray performed at the bedside with anteroposterior projection : multiple ggo and small consolidations ( cons ) bilaterally , distributed peripherally and in the middlebasal lung elds . 
a radiogramma del torace , eseguito a letto in proiezione ap : multipli addensamenti con aspetto a ogg e parcellari consolidamenti ( cm ) bilaterali , pi evidenti in sede medio - basale . 
b sezione assiale di mdct del torace : multiple areole di ogg e parcellari cm bilaterali , a prevalente distribuzione mantellare ed in sede lobare inferiore . chogram , which had gone undetected on cxr . 
finally , in 3 / 9 patients in whom ct con rmed the cxr signs of bacterial suprainfection , it also identi ed the presence of pericardial effusion , which had been missed at cxr in all cases owing to very small size . blood and bronchoaspirate culture identi ed staphylococcus aureus in 3 / 9 patients and a mixed bacterial ora in 6 / 9 cases . 
 discussion human in uenza pandemics are caused by in uenza viruses from nonhuman reservoirs : among the in uenza pandemics sede ed estensione ( tabella 2 ) : 14 ( 82 , 3% ) ri , 2 n ( 11 , 7% ) , 5 ( 29 , 4% ) ogg . 
 quattordici / 90 pazienti ( 15 , 5% ) presentavano reperti radiogra ci sospetti per sovrainfezione batterica ( tabella 1 ) , variamente combinati tra di loro : 9 / 14 ( 64 , 2% ) segni di versamento pleurico , 4 ( 28 , 5% ) consolidamenti con broncogramma aereo , 2 ( 14 , 2% ) linfonodi , 1 ( 7 , 1% ) cavitazione , 1 ( 7 , 1% ) idropneumotorace . 
nove / 17 ( 52 , 9% ) casi mostravano segni di sovrainfezione batterica , variamente combinati , allindagine tc ( tabella 2 ) : 9 / 9 ( 100% ) albero in ore , 6 ( 66 , 6% ) consolidamenti con broncogramma aereo , 4 ( 44 , 4% ) versamento pleurico e 3 ( 33 , 3% ) pericardico , 2 ( 22 , 2% ) linfonodi > 1 cm , 1 ( 11 , 1% ) cavitazione , 1 ( 11 , 1% ) idropneumotorace . 
lindagine tc ha confermato in 9 casi i reperti di sovrainfezione batterica identi cati alla rx del torace ( 9 / 14 , 64 , 2% ) ed ha indicato come falsi positivi 5 casi di sospetto versamento pleurico rilevati alla rx del torace . 
inoltre , in due dei 9 casi in cui la tc ha confermato i segni radiogra ci di sovra infezione batterica , essa ha individuato consolidamenti con broncogramma aereo misconosciuti alla rx del torace . 
the infection is due to pigto - human transmission of a viral pathogen produced by the triple genetic reassortment of human , swine and avian viral strains in north america and eurasia ; human - to - human transmission occurs through respiratory droplets or contact with infected surfaces [ 9 , 14 , 16 ]  . 
 according to the who , from the beginning of the pandemic to 15 november 2009 , > 78 , 000 cases of in uenza a h1n1 were noti ed in europe and 190 , 765 in the americas , with a death toll of at least 350 and 4 , 806 , respectively [ 17 ]  . 
from 19 october , when in unet monitoring began in italy [ 18 ] , to 8 november , there were an estimated 1 , 521 , 000 cases of in uenza a / h1n1 in italy sola proiezione ap . 
in ne , in 3 dei 9 pazienti in cui la tc ha confermato i reperti radiogra ci di sovrainfezione batterica , essa ha anche rilevato la presenza di versamento pericardico . 
in tutti i 3 casi esso era stato misconosciuto alla rx del torace a causa della sua modestissima entit . allemocoltura e nel broncoaspirato , in 3 / 9 pazienti stato identi cato il batterio staphylococcus aureus , in 6 / 9 casi una ora batterica mista . 
quindici / 167 pazienti ( 8 , 98% ) hanno necessitato di intubazione oro - tracheale e ventilazione assistita , previo ricovero in unit di terapia intensiva , per il peggioramento delle condizioni clinico - radiologiche . 
 tutti presentavano condizioni patologiche concomitanti rappresentate da ipertensione arteriosa complicata da placenta previa ed atonia uterina post - partum ( 1 / 15 ; 6 , 6% ) , cardiopatia ipertensiva ( 3 / 15 ; 20% ) , en sema ( 3 / 15 ; 20% ) , distro a bollosa ( 1 / 15 ; 6 , 6% ) , malformazioni scheletriche della gabbia toracica ( 2 / 15 ; 13 , 3% ) , obesit ( 4 / 15 ; 26 , 6% ) , diabete ( 2 / 15 ; 13 , 3% ) , uso di droghe ( 1 / 15 ; 6 , 6% )  . 
b sezione assiale di mdct del torace : consolidamenti polmonari bilaterali con associate diffuse alterazioni ground glass sono prevalentemente distribuiti in sede mantellare e posteriore e nel segmento apicale del lobo inferiore . 
sei / 15 ( 40% ) pazienti morirono per linsorgere in 4 casi di acute respiratory distress syndrome ( ards ) , in 2 di multi - organ failure ( mof )  . 
 discussione le pandemie in uenzali umane derivano da virus in uenzali provenienti da reservoir non umani : delle tre pandemie in uenzali del ventesimo secolo , quella del 1918 stata causata da un virus in uenzale di origine aviaria [ 14 ] e le altre due , nel 1957 e nel 1968 , sono state provocate da nuove linee virali risultanti dalla combinazione di virus aviari e umani attraverso un processo di riassortimento [ 15 , 16 ]  . 
 lin uenza virale a rappresenta unepidemia su scala mondiale causata da un nuovo virus in uenzale a / h1n1 che si diffuso nel marzo 2009 dal messico in tutto il mondo . 
linfezione dovuta alla trasmissione , da parte di alcuni allevamenti suini alluomo , di un patogeno virale prodotto dal triplo riassorimento genetico delle tipologie virali umana , suina ed aviaria nel nord america e nei paesi eurasiatici ; il contagio interuomo si realizzerebbe mediante la trasmissione di goccioline di saliva o il contatto delle mani con super ci infette [ 9 , 14 , 16 ]  . 
 secondo loms , dallinizio della pandemia al 15 novembre 2009 , oltre 78000 casi di in uenza a h1n1 sono stati noti cati in europa e 190765 nelle americhe , con un numero di decessi rispettivamente di almeno 350 e 4806 [ 17 ]  . 
dal 19 ottobre , giorno di avvio della sorveglianza in unet in italia [ 18 ] , all8 novembre , sono stimati 1521 mila i casi di in uenza a h1n1 nel nostro paese , con un numero di decessi pari a 53 secondo leuropean centre for disease prevention and control ( ecdc ) [ 19 ]  . 
in italia le regioni dove si registrata la pi ampia diffusione del virus sono state le marche con un incidenza del 2 , 9% seguite da emilia romagna ( 1 , 8% ) , lazio ( 1 , 7% ) , abruzzo ( 1 , 6% ) e campania ( 1 , 6% )  . 
in data 15 novembre 2009 , in cui si registrato il picco di contagio , le vittime correlate alla in uenza a sono salite a 53 di cui 23 in campania , 7 in emilia romagna , 5 in lombardia . 
in un recente lavoro [ 8 ] stato confermato che il virus h1n1 si trasmette caratteristicamente tra bambini e giovani adulti , colpendo nel 45% dei casi giovani di et < 18 anni e solo nel 5% dei casi individui di et > 65 anni . 
sebbene nella nostra personale esperienza la gravit dellimpatto epidemiologico dellin uenza h1n1 sia stato ampiamente ridimensionato rispetto alle aspettative globali , anche la nostra popolazione di studio ha presentato un prevalente interessamento delle fasce di et pi giovanili radiol med ( 2011 ) 116 : 706719 fig . 
the most affected age groups were children and teenagers from birth to 14 years of age ( incidence 3.6% ) , and , to a lesser extent , individuals aged 1564 years ( 0.7% ) and > 65 years ( 0.1 % ) [ 19 ]  . 
a recent paper [ 8 ] con rmed that the h1n1 virus is typically transmitted among children and young adults , affecting individuals < 18 years in 45% of cases and those > 65 years in 5% of cases only . 
la pi alta incidenza nelle fasce di et inferiori ai 18 anni potrebbe essere legata , invece , in particolar modo nei bambini , a meccanismi di immunode cienza e / o di immaturit immunologica [ 21 , 22 ]  . 
 le principali manifestazioni cliniche dellin uenza virale h1n1 descritte in letteratura [ 8 ] sono rappresentate da : febbre ( 95% ) , tosse ( 88% ) , cefalea ( 34% ) , faringodinia ( 31% ) , vomito ( 29% ) , diarrea ( 25% )  . 
in accordo con i dati della letteratura [ 8 ] abbiamo osservato un elevazione degli indici di funzionalit epatica ( 44 , 9% ) , dei leucociti ( 17 , 9% ) e trombocitopenia ( 2 , 9% )  . 
le principali patologie concomitanti sono state bronchite asmatica 716 radiol med ( 2011 ) 116 : 706719 cially as regards children to mechanisms of immunode ciency and / or immunological immaturity [ 21 , 22 ]  . 
 the most important reported [ 8 ] clinical manifestations of h1n1 virus in uenza are : fever ( 95% ) , cough ( 88% ) , headache ( 34% ) , sore throat ( 31% ) , vomiting ( 29% ) and diarrhoea ( 25% )  . 
 to date , few studies addressing chest imaging in patients affected by in uenza a / h1n1 have been published [ 1012 ] , and the presentation of h1n1 virus pneumonia on both cxr and chest ct seems to re ect the general features of viral pneumonia [ 23 ]  . 
one study [ 11 ] reported on the main cxr and chest ct ndings in seven patients affected by in uenza a / h1n1 : bilateral ggo , more frequently associated with focal or multifocal areas of consolidation . 
of the 15 / 66 ( 22.7% ) patients who underwent ct , 9 / 15 ( 60% ) had ggo combined with consolidation , with diffuse or lobar extension in 70% of cases . 
it is likely that the alarmism regarding in uenza infection prompted many patients to seek early medical attention , thus allowing detection of interstitial reticulation , an early nding in viral disease . 
only 5% of patients had allo stato attuale sono stati realizzati pochi studi di imaging del torace nei pazienti affetti da in uenza virale a / h1n1 [ 1012 ]  . 
alcuni autori [ 11 ] hanno descritto le principali alterazioni radiogra che e tc in 7 pazienti affetti da inuenza a / h1n1 : opacit ground - glass bilaterali , pi di frequente associate ad aree di consolidamento a distribuzione multifocale , talora anche focali . 
dei 66 ( 30% ) pazienti che avevano effettuato rx del torace , 28 / 66 ( 42% ) presentavano consolidamenti ( 50% ) , maggiormente distribuiti ai lobi inferiori ; dei 15 / 66 ( 22.7% ) pazienti sottoposti ad esame tc , 9 / 15 ( 60% ) presentavano lassociazione di ground glass e consolidamenti , ad estensione diffusa ed a sede lobare inferiore nel 70% dei pazienti . 
queste ultime presentavano , tuttavia , unestensione prevalentemente monolaterale e focale ( 61 , 5% ) e distribuzione pi evidente in sede medio - basale ( 46 , 1% )  . 
verosimile che lallarmismo per il contagio in uenzale abbia indotto numerosi pazienti a recarsi prontamente allattenzione medica , rendendo precoce losservazione radiogra ca delle ri , reperto iniziale di danno in corso di malattia virale . 
in accordo con i dati della letteratura [ 10 , 11 ] le lesioni elementari evidenziate in tc ( tabella 2 ) sono state ogg associate a cm ( 58 , 8% ) , ambedue ad estensione bilaterale , radiol med ( 2011 ) 116 : 706719 nodules , which showed unilateral and focal extension and basal distribution in 60% of cases . 
the distribution of ggo combined with consolidation was predominant in the lower lobes ( 60% ) and subpleural regions and was associated in 60% of cases with similar peribronchovascular lesions . 
additionally , there were no cases of isolated consolidation without ggo , probably owing to the relatively early observation of the primary pulmonary lesions : in the initial phase of infection , ggos earlier lesions in which bronchial and vessel margins are still discernible manifest alongside consolidations compared with the later phases of disease ( not necessarily evolving to ards ) in which they increase in attenuation and coalesce into consolidations . 
only two cases showed parenchymal nodules , which were focal and unilateral and distributed in the lower lobe ; these nodules had already been identi ed at cxr and were referable to an underlying infectious disease . 
at variance with previous reports [ 10 ] , in the contrast - enhanced examinations requested for suspected pulmonary embolism , we found no thromboembolic phenomena involving the pulmonary arteries or their branches . 
 recent literature [ 2426 ] has extensively described the principal pulmonary abnormalities seen in bacterial infections : consolidations with air bronchogram , tree - in - bud pattern , cavitation , pleural and / or pericardial effusion and lymphadenopathy . 
in agreement with these data [ 2426 ] , although differently identi ed by the two imaging modalities ( tables 1 and 2 ) , the most common signs of bacterial suprainfection in our series were tree - in - bud pattern , consolidation with air bronchogram and pleural and pericardial effusion . 
la distribuzione delle ogg associate ai cm stata predominante ai lobi inferiori ( 60% ) ed in sede subpleurica , associata nel 60% dei casi ad omologhe lesioni in sede peribroncovascolare . 
inoltre non sono stati evidenziati cm isolati in assenza di ogg verosimilmente per la relativa precocit di osservazione delle lesioni elementari polmonari : nella fase iniziale di infezione le ogg , lesioni pi precoci in cui sono ancora distinguibili bronchi e vasi , si manifestano insieme ai cm , rispetto a fasi pi tardive della patologia , non necessariamente evolventi in ards , in cui esse aumentano la loro densitometria e con uiscono interamente in consolidamenti . 
solo in 2 casi sono state identi cate nodulazioni parenchimali , focali e monolaterali , a distribuzione lobare inferiore , peraltro gi identi cate allesame rx del torace , inquadrabili nellambito della patologia infettiva di base . 
contrariamente ad alcuni autori [ 10 ] , negli esami eseguiti con mezzo di contrasto endovena per quesito clinico di embolia polmonare , non abbiamo evidenziato fenomeni di natura tromboembolica a carico delle arterie polmonari e dei suoi rami . 
 la letteratura moderna [ 2426 ] ha ampiamente descritto le principali alterazioni polmonari identi cabili in caso di infezione batterica : consolidazioni con broncogramma aereo , tree - in - bud , cavitazioni , versamento pleurico e / o pericardico , linfoadenomegalie . 
in accordo con i dati della letteratura [ 2426 ] , sebbene differentemente identi cati nelle due metodiche di studio ( tabelle 1 e 2 ) , i segni di sovrainfezione batterica pi frequenti nel nostro gruppo di studio sono stati tree - in - bud , cm con broncogramma aereo , versamento pleurico e pericardico . 
dei 15 / 167 casi ( 8 , 98% ) sottoposti a ventilazione meccanica per peggioramento del quadro clinico - radiologico , tutti presentavano patologie concomitanti , in particolare bpco ( 33 , 3% )  . 
standard cxr and chest ct are the reference investigations in identifying the location and extension of primary pulmonary lesions and documenting the signs of bacterial suprainfection and pulmonary complications of h1n1 in uenza , thus allowing correct diagnostic , prognostic and therapeutic management . 
 radiol med ( 2011 ) 116 : 706719 caratteristiche radiologiche e cliniche di unampia popolazione di pazienti ospedalizzati in un centro di riferimento per le malattie infettive con diagnosi accertata , mediante tampone faringeo , di in uenza virale h1n1 . 
lesame radiogra co standard e la tomogra a computerizzata del torace hanno rappresentato le indagini di riferimento nellindividuazione della sede ed estensione delle lesioni elementari polmonari , documentando i segni di sovrainfezione batterica e le complicanze polmonari dellin uenza h1n1 , ai ni di un corretto inquadramento diagnostico , prognostico e terapeutico . 
mercuri2 1department of interventional angiographic radiology , istituto ortopedico rizzoli , via di barbiano 1 / 10 , 40136 bologna , italy 2department of orthopaedics , istituto ortopedico rizzoli , university of bologna , bologna , italy 3department of radiology , istituto ortopedico rizzoli , bologna , italy 4department of radiology , ospedale sant orsola , bologna , italy 5department of nuclear medicine , maggiore hospital , bologna , italy 6unita operativa di oncologia , ospedale sant orsola , bologna , italy 7istituto toscano tumori , nuovo ospedale san giuseppe , empoli , italy 8poliambulatorio di radiologia zappi , bartalena , imola , italy correspondence to : p . 
 indications for repeat embolisation included pain or imaging evidence of progressive disease : 105 patients had repeat embolisation at the same location at an interval of 13 months ; 260 patients had one embolisation , 78 had two and 29 had three or more . 
in 35 cases , embolisation was not feasible because of poor lesion vascularisation ( 21 patients with bone metastases and two with aneurysmal bone cysts ) , origin of the adamkiewicz artery in the embolisation eld ( four patients with bone metastases and one with aneurysmal bone cyst ) , atheromatosis and arteriosclerosis ( ve patients with bone metastases ) and riassunto obiettivo . 
lembolizzazione stata usata come trattamento primario per pseudo - tumori e tumori benigni , con signi cato adiuvante nel trattamento dei tumori maligni e nelle forme benigne e con signi cato palliativo nel trattamento dei sarcomi dellosso e delle lesioni metastatiche . 
il dolore e levidenza allimaging di una progressione di malattia era lindicazione per la ripetizione dellembolizzazione ; 105 hanno ripetuto lembolizzazione nella stessa sede , ad intervallo di 13 mesi ; 260 pazienti sono stati sottoposti ad una sola embolizzazione , 78 pazienti a due embolizzazioni e 29 pazienti a tre o pi embolizzazioni . 
si ottenuta risposta clinica in 406 procedure ( 97% ) e nessuna risposta in 13 procedure in pazienti con tumori del bacino 794 radiol med ( 2011 ) 116 : 793808 anatomical and technical problems such as small - calibre vessels , many branches and acute vessel angles ( two patients with bone metastases )  . 
in 35 pazienti non stata eseguita alcuna embolizzazione : in 21 pazienti con metastasi e in 2 con cisti aneurismatiche per scarsa vascolarizzazione ; in 4 con metastasi ossea ed in 1 con cisti aneurismatica per la presenza di arteria di adamkiewicz nella vascolarizzazione della lesione ; in 5 pazienti con metastasi ossee per problemi steno - ostruttivi su base ateromasica ; in 2 pazienti con metastasi per problemi tecnici legati al calibro dei vasi . 
lnbca , a nostro avviso , lagente embolizzante pi adatto per locclusione di piccoli vasi in assenza di complicanze maggiori , ma richiede buona esperienza da parte degli operatori . parole chiave embolizzazione arteriosa selettiva nbca tumori ossei introduction introduzione embolisation was rst reported by frieda feldman in 1975 as a useful adjunct for managing selected bone tumours [ 1 ]  . 
ever since , many authors have reported on selective and superselective intra - arterial embolisation for primary bone and soft - tissue tumours and bone metastases from different primary neoplasms [ 217 ]  . 
these reports indicate that embolisation is generally an effective treatment for selected primary tumours and bone metastases and associated with a rapid reduction in pain and tumour volume lasting from 1 to 9 months [ 5 , 7 , 9 , 11 , 18 ]  . embolisation can be palliative or adjunctive , primary or serial . 
reduced bleeding is particularly il primo lavoro sullutilit dellembolizzazione arteriosa come supporto aggiuntivo nel management dei pazienti con tumori ossei , fu prodotto dal dottor frieda feldman nel 1975 [ 1 ]  . 
da allora , molti autori si sono espressi sullapplicazione di questa metodica sia per i tumori primitivi ossei e dei tessuti molli , che per le metastasi ossee da differente neoplasia primitiva [ 217 ]  . 
questi report hanno evidenziato che lembolizzazione in genere uno strumento ef cace per selezionate neoplasie primitive e secondarie , che si associa ad una riduzione del volume tumorale e della sintomatologia dolorosa , con una durata da uno a nove mesi [ 5 , 7 , 9 , 11 , 18 ]  . lembolizzazione pu essere palliativa o adiuvante , primaria o seriale . 
in questo modo si determina una riduzione del volume tumorale , una diminuzione del sanguinamento ed una maggior de nizione del con ne tumore - tessuto circostante , cos da rendere pi agevole la resezione chirurgica . 
il ridotto sanguinamento inoltre radiol med ( 2011 ) 116 : 793808 advantageous for patients with rare blood groups or those prone to transfusion reactions [ 7 , 14 , 19 ]  . 
in this paper , we present our experience with 454 selective transarterial superselective embolisations using n - 2 - butyl cyanoacrylate ( nbca ) for primary , adjuvant or palliative treatment of bone tumours and discuss the clinical and imaging results . materials and methods particolarmente vantaggioso per quei pazienti con gruppi sanguigni rari o per quelli con maggior predisposizione a reazioni avverse trasfusionali [ 7 , 14 , 19 ]  . in questo studio , presenteremo la nostra esperienza di 454 embolizzazioni arteriose selettive e superselettive utilizzando ln - 2 - butil - cianoacrilato ( nbca ) per il trattamento primario , adiuvante o palliativo dei tumori ossei , discutendone i risultati e le implicazioni dal punto di vista clinico e diagnostico . we present 365 patients with primary and metastatic musculoskeletal bone tumours treated with selective transfemoral embolisation using nbca during an 8 - year period from december 2002 to april 2010 . 
primary tumour histology and location varied ( tables 1 and 2 ) ; 105 materiali e metodi durante un periodo di 8 anni , da dicembre 2002 ad aprile 2010 , 365 pazienti , 206 uomini e 159 donne con et media pari a 53 anni ( range da 3 , 3 a 87 anni ) , sono stati sottoposti ad embolizzazione selettiva trans - femorale con nbca per neoplasie primitive o secondarie dellapparato table 1 tumour histology and number of embolisations of the 365 patients in this study primary tumour patients embolisation one embolisation two embolisations three or more embolisations bone metastases aneurysmal bone cyst osteosarcoma giantcell tumour vertebral haemangiomas chordoma haemangioendothelioma of bone osteoblastoma haemangiopericytoma paraganglioma ependymoma malignant schwannoma plasmacytoma metastasi ossee cisti ossee aneurismatiche osteosarcoma tumore a cellule giganti emangioma vertebrale cordoma emangioendotelioma osseo osteoblastoma emangiopericitoma paraganglioma ependimoma schwannoma maligno plasmocitoma 243 243 187 187 tabella 1 istologia tumorale e numero di embolizzazione nei 365 pazienti inclusi in questo studio tumore primitivo pazienti embolizzazione una due tre o pi table 2 site of the 454 embolisations embolisations tabella 2 sito delle 454 embolizzazioni sito embolizzazioni 796 site pelvis and sacrum spine lower limb upper limb thoracic cage pelvi e sacro rachide arto inferiore arto superiore gabbia toracica patients had repeat embolisation at the same location at an interval of 13 months ; 260 patients had one , 78 had two and 29 had three or more . 
the study was approved by the institutional review board / ethics committee of the authors institution . embolisation was indicated in all tumours with favourable vascularity as judged by pre - embolisation angiography . 
patients with bone metastases were the most numerous in the series ; all patients had intense pain , and one patient had a pathological fracture . technique diagnostic digital subtraction angiography ( dsa ) ( contrast medium : iomeprol 300 mg / ml , iomeron , bracco , milan , italy , and iohexol 350 mg / ml , omnipaque , ge healthcare , milan , italy ) was performed before embolisation to identify the feeding vessels . 
angiographic apparatus used were the philips integris v3000 cesar - scp - visub angiographic system ( philips medical systems , eindhoven , the netherlands ) and the siemens angiostar plus / plus or ( siemens ag , medicals engineering , forchheim , germany )  . 
in patients with metastases in the pelvis or lower extremities , the contralateral transfemoral radiol med ( 2011 ) 116 : 793808 muscolo - scheletrico , con lesecuzione , complessivamente , di 454 embolizzazioni . 
listotipo tumorale , cos come la sede , stato variabile ( tabelle 1 e 2 ) : in particolare , 105 pazienti hanno ripetuto la procedura nella stessa sede a distanza di 13 mesi ; 260 pazienti sono stati sottoposti ad una sola embolizzazione , 78 pazienti hanno eseguito 2 embolizzazioni ed in ne 29 pazienti tre o pi embolizzazioni . 
 inoltre , questo studio stato approvato dalla commissione etica del nostro istituto . lembolizzazione stata eseguita in tutti i tumori con una vascolarizzazione giudicata favorevole in base allangiogra a pre - procedura . 
tale procedura stata effettuata come trattamento primario per i tumori ossei benigni , come trattamento adiuvante lintervento chirurgico per tumori ossei sia benigni che maligni , ed in ne a scopo palliativo per i sarcomi ossei e per le metastasi . 
 i pazienti con metastasi ossee sono stati i pi numerosi pazienti arruolati ; in tutti i casi era presente unintensa sintomatologia dolorosa e un paziente presentava una frattura patologica . tecnica al ne di identi care i vasi rifornenti la neoplasia , unangiogra a digitale a sottrazione ( mezzo di contrasto : iomeprol 300 mg / ml [ iomeron , bracco , milano , italia ] e iohexol 350 mg / ml [ omnipaque , ge healthcare , milano , italia ] ) stata eseguita prima della procedura di embolizzazione . 
 lapparecchio angiogra co utilizzato stato il philips integris v3000 cesar - scp - visub angiographic system ( philips medical systems , eindhoven , olanda ) e il siemens angiostar plus / plus o.r. 
in tutti i pazienti adulti , langiogra a e lembolizzazione arteriosa selettiva sono state effettuate sotto anestesia locale , utilizzando la tecnica seldinger attraverso il cateterismo arterioso dellarteria femorale ; in tutti i pazienti pediatrici , langiogra a e lembolizzazione arteriosa selettiva sono state effettuate sotto anestesia generale . 
larteria femorale stata cateterizzata con un introduttore 4 french ( cordis corporation , miami , fl , usa ) o con un introduttore 5 french ( terumo corporation , tokyo , giappone )  . 
a questo punto , nei pazienti con lesioni spinali o pelviche , stata eseguita unaortogra a panoramica con catetere 4 french pigtail ( cordis corporation ) , seguita da una arteriogra a selettiva e superselettiva mediante cateteri cobra , e simmons ( terumo corporation ) e microcateteri di 130 cm , 2 , 7 - 2 , 9 french pre - modellati mc - pp27131 ( coaxial catheters system , terumo corporation )  . 
the femoral artery was catheterised with a 4 - french ( cordis corporation , miami , fl , usa ) or 5 - french ( terumo corporation , tokyo , japan ) introducer . 
from the mixture , 1 ml was aspirated in an insulin ( 1 ml ) syringe ; depending on the pathological vasculature , 0.10.2 ml of the aspirate mixture was injected , sandwiched with 2 + 2 ml of 5% glucosate solution under uoroscopic control . 
the bolus administration in low doses ( 0.10.2 ml ) of the sandwiched embolic agent under uoroscopic control , followed by arteriography and new embolisation if incomplete occlusion or more feeding vessels were observed , provided for the ef cacy and safety of the embolisation procedures . the technical success of embolisation was evaluated by additional angiography after completion of the procedure . 
embolisation was considered technically complete when there was stasis of intravascular contrast material and either complete elimination of the tumours hypervascular staining or 80% elimination of the tumours pathological vasculature compared with the initial diagnostic angiogram [ 7 , 19 ]  . clinical and imaging effects of treatment were evaluated at routine follow - up examinations . 
nei pazienti con lesioni localizzate agli arti , invece , laortogra a non stata eseguita ; in pazienti con lesioni dellarto superiore , lembolizzazione stata eseguita con utilizzo di catetere vertebral ( terumo corporation ) e microcateteri , e in pazienti con lesioni dellarto inferiore con catetere vertebral , cobra e microcateteri . 
in tutti i pazienti , lagente embolizzante impiegato stato lnbca ( glubran 2 , gem , viareggio , italia ) , diluito con lipiodol al 33% ( 1 acone [ 10 ml ] , lipiodol ultra uido , guerber spa , francia ) ed iniettato tra soluzione glucosate al 5% , al ne di prevenire la polimerizzazione . 
di tale miscela , 1 ml stato aspirato in una siringa da insulina ( 1 ml ) e , a seconda della vascolarizzazione patologica , 0 , 10 , 2 ml della miscela aspirata , sono state iniettate , racchiuse in una 2 + 2 ml di soluzione glucosata al 5% , sotto controllo uoroscopico . 
se a causa dellipervascolarizzazione della lesione fosse necessario pi di un acone di nbca ( 1 ml ) , si pu procedere alla preparazione di una nuova miscela con le medesime modalit ; complessivamente , nella nostra casistica , sono stati impiegati in media tra gli 0 , 5 e i 2 ml di nbca con lipiodol per ogni singola embolizzazione . 
il bolo cos composto , somministrato a bassa dose ( 0 , 10 , 2 ml ) sotto controllo uoroscopico , garantisce lef cacia e la sicurezza della procedura . il successo tecnico dellembolizzazione stato valutato da unangiogra a panoramica , eseguita al termine della procedura . 
lembolizzazione stata considerata tecnicamente ben riuscita , laddove era presente stasi intravascolare di mezzo di contrasto , oppure una completa eliminazione dello stesso , o uneliminazione superiore all80% rispetto a quella dellangiogramma iniziale [ 7 , 19 ]  . il risultato dal punto di vista clinico e di imaging stato quindi valutato durante le indagini di routine durante follow - up . 
si de nisce come risposta clinica , una riduzione della sintomatologia dolorosa e dellimpiego di analgesici maggiore o uguale al 50% , come assenza di risposta , una riduzione inferiore al 50% . 
 la risposta dal punto di vista diagnostico stata invece studiata mediante indagini di tomogra a computerizzata 798 radiol med ( 2011 ) 116 : 793808 pain and analgesics use , and no response as < 50% decrease . 
 imaging tumour response was evaluated on computed tomography ( ct ) scans obtained at 3 , 6 and 12 month or at the latest follow - up by hypoattenuating areas within the tumour that resembled necrosis , tumour size and ossi cation . risultati a 3 , 6 , 12 mesi o no allultimo follow - up ed stata de nita dalla valutazione del volume tumorale , dellossi cazione e della comparsa di aree di ipoattenuazione a livello dellarea tumorale , indicanti la comparsa di necrosi . results total of 419 procedures ( 93% ) were technically successful ; selective catheterisation and embolisation of the feeding vessels was achieved in all cases . 
1 pre - embolisation angiography of a 67 - year - old man with a metastatic renal - cell carcinoma of the l3 vertebra shows the adamkiewicz artery originating from the second left lumbar artery ( arrows )  . 
1 langiogra a pre - embolizzazione di un uomo di 67 anni con carcinoma renale metastatico a livello di l3 mostra lorigine dellarteria di adamkiewicz dalla seconda arteria lombare sinistra ( frecce )  . 
 quattrocentodiciannove embolizzazioni ( 93% ) , sono state portate a termine con successo ; la cateterizzazione selettiva e lembolizzazione dei vasi rifornenti la lesione stata raggiunta in tutti i casi . 
inoltre , in tutti i casi , langiogra a post - procedura ha evidenziato , a livello lesionale , una completa interruzione dellapporto vascolare o una riduzione della vascolarizzazione superiore all80% . 
nei pazienti con intensa sintomatologia dolorosa , in particolare nei pazienti con lesioni agli arti dimostratisi essere quelli con una sintomatologia pi intensa prima dellembolizzazione , si raggiunta una risoluzione del dolore pressoch completa . 
 nei pazienti con lesioni spinali , il miglioramento del dolore stato invece di media entit . per quel che riguarda i pazienti con metastasi ossee , si raggiunta una risoluzione della sintomatologia di durata media pari a mesi 8 , 1 ( range da 1 a 12 mesi ) ; la ricomparsa del dolore non ha comunque mai raggiunto i livelli di intensit pre - procedura . 
il massimo diametro tumorale dopo embolizzazione stato in media pari a 5 , 5 cm ( range da 2 a 20 cm ) , contro i 7 , 8 cm ( range da 5 a 30 cm ) prima dellembolizzazione stessa . 
in 65 pazienti ( di cui , 35 con carcinoma renale , figure 1 e 2 , 15 con carcinoma tiroideo , 8 con tumore al seno e 7 con tumore polmonare , figura 3 ) stata documentata la presenza di un variabile grado di ossi cazione : in particolare , si osservata unabbondante ossi cazione in sei pazienti , mentre i restanti hanno evidenziato una iniziale rima periferica di formazione ossea . 
in 12 pazienti radiol med ( 2011 ) 116 : 793808 a clinical response was achieved in 406 procedures ( 97% ) , and no response in 13 procedures in patients with pelvis and sacrum skeletal metastases . 
medium pain relief was observed in patients with spinal lesions . in patients with bone metastases , the mean duration of pain relief was 8.1 ( range 112 ) months ; recurrent pain was never as intense as pre - embolisation pa mean maximal tumour diameter after embolisation was 5.5 cm ( range 220 cm ) compared with 7.8 cm ( range 530 that cm ) before embolisation . 
in 12 patients with bone metastases , surgical treatment was performed after embolisation ; in none of these patients was surgery feasible before embolisation . embolisation was effective in 32 patients with aneurysmal bone cysts ( 94% )  . 
recurrence and / or persistence of the lesion occurred in 14 patients ; nine patients had one recurrence and / or persistence , and ve patients had two recurrences each . 
ten of the 19 recurrences occurred in patients with lesions > 5 c three patients had complications , including skin necrosis ( two patients ) and transient paresis of the sciatic nerve ( one patient )  . 
eighty - one patients ( 22% ) exhibited clinical signs of postembolisation syndrome as diagnosed by fever or chills , nausea and vomiting and increased ischaemic pain at the site of embolcon metastasi ossee , si proceduto allintervento chirurgico dopo lembolizzazione ; in nessuno di essi tale intervento risultava eseguibile prima dellembolizzazione stessa . per quel che riguarda i pazienti con cisti ossee aneurismatiche , lembolizzazione stata ef cace in 32 casi ( 94% )  . 
 la recidiva e / o la persistenza della lesione si veri cata in 14 pazienti , di cui nove hanno presentato una recidiva e / o una persistenza della lesione stessa , e cinque due recidive . 
dieci delle 19 recidive si sono osservate in pazienti con lesioni con diametro maggiore a 5 c tre pazienti hanno presentato complicanze caratterizzate da necrosi cutanea ( due pazienti ) e paresi transitorie del nervo sciatico ( un paziente )  . 
una povert vascolare stata osservata soprattutto in alcuni tumori in ltratanti a derivazione neurogenica , quali schwannomi maligni . nellimmediato periodo post - embolizzazione , si sono registrate 122 complicanze minori e 6 complicanze maggiori . 
ottantuno pazienti ( 22% , di cui 49 con metastasi ossee e 32 con altri tumori ) hanno evidenziato segni clinici della sindrome post - embolizzazione quali febbre , brividi , nausea , vomito e un aumento del dolore , ischemico , a livello del sito dellembolizzazione . 
parestesie transitorie sono state osservate in 41 pazienti ( 11% , di cui 37 con metastasi ossee sacroiliache , 2 con cisti aneurismatiche e 2 con tumori del sacro a cellule giganti ) con lesioni del bacino e del sacro . 
 si segnalano inoltre transitoria paresi del nervo sciatico , veri catasi in un solo paziente ( 0 , 3% ) dopo embolizzazione per cisti ossea aneurismatica della pelvi , e necrosi cutanea e sottocutanea in 5 pazienti ( 1 , 4% ) , di cui due con cisti ossee aneurismatiche della spalla e della pelvi , uno con emangioma dellomero , uno con tumore a cellule giganti del bacino e uno con paraganglioma metastatico a localizzazione pelvica dopo due procedure di embolizzazione . 
2a axial ( left ) and sagittal ( right ) computed tomography of a 32 - year - old man with giant - cell tumour of the sacrub preoperative selective angiography and embolisation of the feeding vessels originating from the internal iliac arteries ( left ) and middle sacral artery ( centre )  . 
3a computed tomography ( left ) and coronal t2 - weighted magnetic resonance imaging ( right ) of the pelvis of a 16 - year - old girl with a large osteosarcoma . 
3a tomogra a computerizzata ( sinistra ) a sezioni coronali t2 - pesate di risonanza magnetica ( destra ) , di un ampio osteosarcoma del bacino , in donna di anni 16 . 
d a due anni dalla diagnosi e dalla chemioterapia , la risonanza magnetica assiale ( sinistra ) e coronale ( destra ) evidenzia una signi cativa riduzione del volume tumorale . radiol med ( 2011 ) 116 : 793808 802 fig . 
transient paraesthesias were observed in 41 patients ( 11% ) with pelvic and sacrum lesions ; there were 37 patients with sacroiliac metastatic bone tumours , two with aneurysmal bone cysts and two with giant - cell tumours of the sacruin all patients , symptoms resolved completely with symptomatic treatment within less than a week . 
skin breakdown and subcutaneous necrosis occurred in ve patients ( 1.4% ) ; there were two patients with aneurysmal bone cysts of the shoulder and pelvis , one with haemangioma of the humerus , one with giant - cell tumour of the pelvis and one with a metastatic paraganglioma of the pelvis after two embolisations . 
the patient with aneurysmal bone cyst complicated by skin necrosis of the shoulder underwent ap reconstruction ; this was considered a major complication . discussione in questo studio , abbiamo esaminato il ruolo dellembolizzazione arteriosa selettiva nei tumori ossei in una grande casistica di pazienti . 
sappiamo , comunque , che un trial prospettico e randomizzato sarebbe pi vantaggioso per de nire lesatto ruolo dellembolizzazione a scopo primario , palliativo o adiuvante per le metastasi ossee , le cisti ossee aneurismatiche e i tumori a cellule giganti , poich noto che in questi pazienti possono essere eseguiti altri approcci terapeutici . 
in 12 pazienti con metastasi ossee , radiol med ( 2011 ) 116 : 793808 discussion in this study , we explored the role of selective transarterial embolisation for bone tumours in a large series of patients . 
we acknowledge that a prospective randomised trial would be more bene cial for de ning the exact value of primary , palliative or adjuvant embolisation for metastatic bone disease , aneurysmal bone cysts and giant - cell tumours , as in these patients , other treatments were also performed . 
preoperative or serial embolisation techniques using different embolic agents can be used as primary or adjuvant treatment to surgery or radiation therapy for patients with metastatic bone disease [ 6 ]  . 
by superselective catheterisation and embolisation of the pathological feeding arteries to the lesion with the most appropriate embolic agent , embolisation can be expected to be successful in up to 90% of cases . 
 patients with renal or thyroid bone metastases have a good chance of undergoing successful treatment with selective vascular occlusion , in contrast to patients with lung metastases to bone [ 7 ]  . 
imaging showed evidence of tumour necrosis in all cases and variable ossialla procedura di embolizzazione seguito il trattamento chirurgico : si precisi che in nessuno di essi la resezione chirurgica era eseguibile prima dellesecuzione dellembolizzazione stessa . le opzioni terapeutiche nei casi di malattia ossea metastatica hanno in genere una nalit palliativa . 
si ricordi inoltre che tutte le lesioni secondarie causano progressivamente una perdita ossea e che molte , se non tutte , si caratterizzano per unipervascolarizzazione , specie in caso di carcinoma primitivo renale e tiroideo [ 5 , 20 ]  . 
le tecniche di embolizzazione pre - operatoria e di embolizzazione seriale , che impiegano differenti agenti embolici , possono essere impiegate nel trattamento primario o adiuvante la chirurgia o la radioterapia proprio per i pazienti con malattia ossea metastatica [ 6 ]  . 
poich tutte le metastasi ossee si caratterizzano per unipervascolarizzazione , tutti i pazienti dovrebbero essere considerati come appropriati canditati per lesecuzione di tale procedura [ 5 , 20 ] , che , tramite il cateterismo superselettivo e lembolizzazione delle arterie tributarie della lesione con un appropriato agente embolico , pu essere espletata con successo in pi del 90% dei casi . 
il periodo di tempo libero dalla sintomatologia dolorosa pu durare da 1 a 9 mesi ; dopo tale intervallo , una ripetizione dellembolizzazione sicura e si pu rendere necessaria [ 21 ]  . 
il successo della procedura dipende , comunque , anche dal tipo e dal comportamento del tumore primitivo ; nei pazienti con metastasi ossee da tumore renale o tiroideo , ci sono buone probabilit che il trattamento attraverso locclusione vascolare selettiva sia portato a termine con successo , a differenza dei pazienti con metastasi da tumore polmonare [ 7 ]  . 
 i nostri dati evidenziano , comunque , che questo effetto palliativo risulta essere solo transitorio ; i sintomi si sono infatti ripresentati a distanza di circa 8 mesi ( range da 1 a 12 mesi )  . 
pu essere oggetto di discussione se la presenza di addizionali terapie possa aver contribuito al successo dellembolizzazione , o se il successo dellembolizzazione combinato ad altri trattamenti possa dipen804 radiol med ( 2011 ) 116 : 793808 cation in 65 patients . 
however , it can be questioned whether the presence of additional therapies may have contributed to the success of embolisation or even that the success of embolisation combined with other therapies may be entirely attributed to these additional therapies . 
as we did not perform the additional treatments in a randomised fashion , we cannot conclude whether they were associated with improved or longer - lasting clinical and imaging results . 
nevertheless , all embolisations were technically successful and were accompanied by an acute improvement in symptoms that cannot be explained by the additional therapies . given the high vascularity and morbidity associated with surgical resection and / or radiation therapy , embolisation has been reported to be a useful primary treatment modality for sacral giant - cell tumours . 
in our series of patients with giant - cell tumour of the sacrum , overall survival to local recurrence was 90% at 60 and 120 months , and local recurrence rate was 10% . 
embolisation has been used for aneurysmal bone cysts in combination with surgery to reduce operative blood loss [ 2830 ] or as primary treatment of sites with dif cult surgical access and in patients at high risk of extensive intraoperative bleeding [ 3139 ]  . 
fourteen patients with recurrent and / or persistent lesions underwent repeat embolisation . long - term series reporting on embolisation for primary treatment of vertebral haemangiomas are lacking [ 4042 ]  . 
poich tali trattamenti aggiuntivi non sono stati studiati in maniera randomizzata , non possiamo concludere se questi possano essere correlati ad una risposta clinica e imaging migliore o pi duratura . 
tuttavia , tutte le embolizzazioni sono state correttamente eseguite dal punto di vista tecnico e si sono associate ad un rapido miglioramento della sintomatologia , che non pu essere spiegato dalle terapie aggiuntive . nei tumori sacrali a cellule giganti , a causa dellalta vascolarizzazione e della morbilit correlata alla resezione chirurgica e / o alla radioterapia , la letteratura riporta che lembolizzazione pu essere unutile opzione terapeutica primaria ; la sopravvivenza no alla recidiva locale a seguito di resezione , terapia radiante ed embolizzazione stata riportata essere tra il 57% e l80% [ 8 , 2326 ]  . 
nei nostri pazienti con tumori sacrali a cellule giganti , la sopravvivenza no alla recidiva locale stata globalmente del 90% a 60 e 120 mesi , ed il tasso di recidive locali stato del 10% . 
nella nostra pratica clinica , il fenolo e lazoto liquido sono impiegati come emostatici nel corso di resezione chirurgica per ridurre il sanguinamento e migliorare il curretage , tranne che nei casi in cui si identi ca una vicinanza con la radice del nervo sacrale [ 27 ]  . 
lembolizzazione stata anche impiegata per il trattamento di cisti ossee aneurismatiche , sia in combinazione con la chirurgia per ridurre le perdita ematiche intra - operatorie [ 2830 ] , che come trattamento primario in siti a dif coltoso accesso chirurgico ed in pazienti ad alto rischio di massivo sanguinamento in corso di intervento [ 3139 ]  . 
quattordici pazienti hanno sviluppato delle recidive e / o evidenziato la persistenza di malattia e sono stati sottoposti a ripetizione del trattamento . mancano invece studi a lungo termine sullapplicazione dellembolizzazione come trattamento primario per gli emangiomi vertebrali [ 4042 ]  . 
in other malignant tumour histologies , embolisation was performed effectively without complications . vascular mapping and the haemodynamic status of the tumour , as well as the tumours anatomical region , must be determined using selective angiography before embolisation . 
arteries feeding the tumour must be catheterised superselectively using microcatheters , and the procedure must be undertaken with the most suitable embolising agent to protect the haemodynamics of normal bone tissues as much as possible . 
when the procedure is followed by surgery , it is recommended that the surgery be performed within 3 days to avoid revascularisation [ 7 , 19 ]  . currently available embolic agents include gelfoam , polyvinyl alcohol ( pva ) particles , liquid ( absolute alcohol ) , coils , tissue adhesives , ethanol , micro brillar collagen and autologous blood clot [ 19 ]  . 
in addition , the use of coils in managing hypervascular bone tumours has been reported to be ineffective because the rich vascularisation of these lesions can open collateral channels within hours [ 17 , 21 , 22 ]  . 
moreover , if particles are used , their size has to be adjusted to the diameter of potential collateral vessels and shunts because these entities are often present in hypervascular malignant bone tumours [ 5 , 10 , 21 , 22 ]  . 
liquid embolic agents offer the advantages of low viscosity for easy injection through small catheters or il mappaggio vascolare e lo stato emodinamico , cos come lanatomia regionale , devono essere determinati attraverso unangiogra a selettiva , prima di procedere allembolizzazione . 
in particolare , devono essere valutati accuratamente le arterie tributarie , le collaterali , i rapporti del tumore con gli adiacenti distretti vascolari e la possibile presenza di stole artero - venose intratumorali . 
 le arterie tributarie della lesione devono essere cateterizzate in maniera superselettiva utilizzando microcateteri e la procedura deve essere eseguita con il pi idoneo agente embolizzante , allo scopo di proteggere il pi possibile lemodinamica del normale tessuto osseo . 
langiogra a post - embolizzazione in ne necessaria per valutare leffetto della procedura : se il vaso tributario occluso , pu essere comunque osservato un vaso adiacente e questo deve essere embolizzato [ 7 , 14 ]  . 
 gli agenti embolici attualmente disponibili includono gelfoam , particelle di alcool polivinile ( pva ) , microsfere , liquidi ( alcool puro e etanolo ) , spirali , adesivi tissutali e micro brille di collagene [ 19 ]  . 
le spirali sono ideali per determinare locclusione di vasi singoli e di grosso calibro ; nel management dei tumori ossei ipervascolarizzati sono inef caci poich determinano una occlusione solo prossimale favorendo le formazione di circoli collaterali nel giro di ore [ 17 , 21 , 22 ]  . 
 tuttavia , la somministrazione di particelle non precisa e il trasporto attraverso i piccoli microcateteri o attraverso distretti vascolari tortuosi pu risultare dif coltoso [ 11 , 14 , 49 , 50 ]  . 
in ne , se si utilizzano le particelle , le loro dimensioni devono essere corrette in base al diametro dei potenziali shunt e vasi collaterali , spesso presenti nei tumori ossei maligni ipervascolari [ 5 , 10 , 21 , 22 ]  . 
gli agenti embolici liquidi offrono invece il vantaggio di una bassa viscosit e quindi di una agevole somministrazione attraverso cateteri piccoli o attraverso cateteri con molte angolazioni per la tortuosit del distretto vascolare . 
lnbca , o colla liquida , 806 radiol med ( 2011 ) 116 : 793808 catheters with many bends through tortuous blood vessels . nbca , or liquid glue , is a liquid embolic agent with distinct advantages as an embolic material . 
 although nbca can pass through bent catheters , thus navigating tortuous blood vessels , it does not permeate all the way to the capillary level , and therefore does not cause tissue death . 
in our practice and in this study , nbca was the preferred embolic agent because we consider it to be the most for controlled embolisation of the pathological tumour vasculature , for permanent occlusion of the target vessels and for complete lesion devascularisation . when embolisation is planned carefully and the vessel is occluded selectively via a securely positioned catheter , complications rarely occur . 
bolus administration of small doses ( 0.10.2 ml ) of sandwiched nbca under uoroscopic control , followed by arteriography , provides for the ef cacy and safety of the procedure . 
postembolisation syndrome , with symptoms such as fever , pain due to ischaemic necrosis of the tumour and malaise , has been reported in 1886% of cases [ 7 , 21 ]  . 
embolisation of adjacent or distant nontargeted vessels can result in a large zone of tissue loss and may be associated with risk of nerve palsy , skin breakdown and subcutaneous or muscle necrosis ; tissue ischaemia may lead to infection . 
care should be taken to the location and vascular supply of at - risk vital structures , such as the femoral region , to avoid embolising supply to the sciatic nerve , the humeral area to avoid circum ex femoral nerve and the lateral cutaneous nerve of the thigh [ 5 , 10 , 16 , 21 , 51 ]  . the occurrence of the adamkiewicz artery that originates between the t5 and l2 vertebra in the embolisation eld should be recognised on the pre - embolisation angiogra in our practice , we encountered the adamkiewicz artery in the embolisation eld during four embolisations for bone metastases and one for aneurysmal bone cyst of the spine . 
in line with the literature , life expectancy is not in uenced by embolisation therapy , and embolisation therapy does not appear to improve the survival of patients with malignant bone tumours [ 3 , 5255 ]  . 
inoltre , sebbene lnbca sia in grado di passare attraverso cateteri curvi utilizzati in distretti vascolari tortuosi , non va incontro a diffusione no al distretto capillare e pertanto non causa morte tissutale . 
 nella nostra pratica clinica e nel presente studio , riteniamo che lnbca sia il miglior agente embolico per il controllo dellembolizzazione nel distretto tumorale , per unocclusione permanente a livello del bersaglio vascolare e per una completa devascolarizzazione della lesione . quando lembolizzazione piani cata con accuratezza e locclusione vascolare selettiva , mediante un sicuro posizionamento del catetere , le complicanze sono rare . 
 la somministrazione di un piccolo bolo di nbca ( 0 , 10 , 2 ml ) sotto controllo uoroscopico , seguito da arteriogra a , effettuato per garantire ef cacia e sicurezza alla procedura . 
lembolizzazione di un distretto vascolare non bersaglio , adiacente o distante , pu determinare una grossa perdita tissutale e pu associarsi al rischio di paralisi , necrosi cutanea , sottocutanea e muscolare ; lischemia tissutale pu inoltre facilitare le infezioni . 
lattenzione dovrebbe quindi essere rivolta alla localizzazione dellapporto vascolare delle strutture vitali a rischio , quali la regione femorale per evitare di embolizzare lapporto ematico al nervo sciatico , al nervo femorale circon esso e al nervo laterale cutaneo della coscia [ 5 , 10 , 16 , 21 , 51 ]  . 
 nella nostra esperienza , abbiamo identi cato tale arteria durante quattro procedure eseguite per metastasi ossee e una procedura eseguita per cisti ossea aneurismatica del rachide ; in questi casi si optato per una sospensione della procedura stessa per evitare il rischio di paraplegia derivante dallocclusione dellarteria di adamkiewicz . in questo studio , a causa delleterogeneit del gruppo dei pazienti e dellistologia tumorale , non abbiamo fatto unanalisi sulla sopravvivenza . 
in linea con la letteratura , laspettativa di vita non in uenzata dallembolizzazione e , daltra parte , lembolizzazione stessa non sembra migliorare la sopravvivenza dei pazienti con tumori ossei maligni [ 3 , 5255 ]  . 
questo dato non deve sorprendere perch , nella maggior parte dei casi , lembolizzazione ha come bersaglio solo una parte della problematica tumoradiol med ( 2011 ) 116 : 793808 most part , embolisation only targets a portion of the tumour burden . 
le terapie locali per il controllo tumorale , quali lembolizzazione , rimangono comunque risorse preziose per preservare la qualit di vita . conclusions conclusioni we recommend embolisation for highly vascular tumours of variable histology as primary or palliative treatment or as an adjunct to surgery to reduce intraoperative blood loss and facilitate resection . 
the low number of complications in this study and the fact that they were minor suggest that strict adherence to the principles of transcatheter embolisation and mini - bolus administration of nbca is important . 
nbca is considered the most appropriate embolic agent for small - vessel occlusion without major causing complications . raccomandiamo lembolizzazione per tumori ipervascolarizzati , di diverso istotipo , come trattamento primario , palliativo o adiuvante la chirurgia , per ridurre il sanguinamento intra - operatorio e facilitare la resezione . 
il basso numero di complicanze , ed il fatto che esse fossero prevalentemente minori , suggerisce che fondamentale una rigorosa adesione ai principi delle tecniche di embolizzazione e della somministrazione del millibolo di nbca . 
bellomi1 , 3 1department of radiology , european institute of oncology , via ripamonti 435 , 20141 milan , italy 2division of epidemiology and biostatistics , european institute of oncology , via ripamonti 435 , 20141 milan , italy 3school of medicine , university of milan , via a . 
 there was no signi cant difference in adc values between responders and nonresponders at the staging mr examination ( p = 0.09 ) and no signi cant correlation between pretreatment adc values and percentage of tumour reduction . 
diciassette pazienti consecutive sono state prospetticamente sottoposte ad esami di risonanza magnetica ( rm ) della pelvi , comprendenti sequenze pesate in diffusione ( dwi ) , prima e dopo terapie non chirurgiche per tumore della cervice uterina . 
le differenze dei valori delle mappe adc tra i due gruppi alla baseline , e nel gruppo di studio prima e dopo terapia sono state valutate con test non parametrici . 
diametro e volume dei tumori cervicali si sono ridotti dopo le terapie in 14 / 17 lesioni ( rispondenti ) , sono invece aumentati in 3 / 17 lesioni ( non rispondenti )  . 
non si sono riscontrate differenze signi cative nei valori di adc alla rm basale tra rispondenti e non rispondenti ( p = 0 , 09 ) , n tra valori adc basali e percentuale di riduzione del tumore . 
i tumori con pi alto incremento percentuale di valori di adc hanno mostrato pi elevata riduzione del volume tumorale , ma questo non risultato signi cativo ( p = 0 , 12 )  . 
i valori di adc del tumore della cervice uterina hanno mostrato signi cativo incremento dopo terapia rispetto ai valori pre - terapia , particolarmente per i tumori rispondenti . parole chiave rm diffusion - weighted imaging cervice tumore risposta introduction introduzione when the radiologist faces uterine cervical cancer treatment options , important but dif cult issues that must be dealt with are evaluation of tumour response to therapy and discrimination between postradiation changes and viable tumour . 
 tumour response to therapy is conventionally addressed by changes in tumour size according to the response evaluation criteria in solid tumours ( recist ) , but changes in size are not always adequate to determine whether or not the tumour is responding to the therapies , and alternative imaging modalities to substitute for the anatomical assessment described in recist are currently under evaluation [ 1 ]  . 
on the other hand , differentiation between residual tumour and radiation changes cannot be made with conventional magnetic resonance ( mr ) images , especially in the rst 3 months after therapy [ 2 , 3 ]  . 
given these dif culties , an early and reliable response marker would have great clinical value for cervical cancer patients to cease ineffective treatment , frequently associated with increased toxicity and development of drug resistance , and to avoid delays in starting alternative , potentially more effective , treatments [ 4 ]  . as changes in tumour size occur as a consequence of biological and molecular changes , functional imaging techniques are under consideration as an adjunctive tool in evaluating many tumour features , including tumour response . 
in oncological imaging , dwi has been linked to lesion aggressiveness and tumour response , with apparent diffusion coefcient ( adc ) measurements being inversely correlated to cellularity and cell membrane integrity [ 7 ]  . 
previous studies evaluated the potential role of dwi in monitoring tumour response to therapy [ 4 , 710 ] and in differentiating normal from cancerous tissue in the uterine cervix [ 11 ]  . 
adc maps usually re ect the complexity of a tumour mass , and during follow - up to therapies , a decreased adc value caused by a decrease of perfusion may be followed by increased adc values caused by necrosis [ 12 ]  . 
therefore , the diffusion characteristics of a tumour would be better evaluated by assessing the adc values of the entire tumour volume rather than on a single most representative slice . quando il radiologo valuta il tumore della cervice uterina dopo terapia , un aspetto importante ma dif cile da valutare rappresentato dalla valutazione della risposta tumorale alla terapia e la distinzione tra le modi cazioni dovute alla radioterapia e il tumore residuo . 
la risposta del tumore alla terapia convenzionalmente indicata da modi cazioni delle dimensioni , in accordo con i criteri response evaluation criteria in solid tumors ( recist ) , ma i cambiamenti dimensionali non sono sempre indicativi di risposta alle terapie , per cui sono in fase di studio modalit alternative di imaging per sostituire i criteri anatomici recist [ 1 ]  . 
 inoltre , la distinzione tra modi cazioni post - radioterapia e tumore residuo , in particolare nei primi 3 mesi dopo terapia , non sempre possibile utilizzando le immagini di risonanza magnetica convenzionale [ 2 , 3 ]  . in considerazione di tali dif colt , individuare un marker di risposta , precoce ed af dabile , avrebbe un enorme valore clinico per le pazienti affette da tumore della cervice , sia per sospendere i trattamenti inef caci , frequentemente associati con un incremento della tossicit e con lo sviluppo di farmaco - resistenza , sia per evitare ritardi nellinizio di trattamenti alternativi e potenzialmente pi ef caci [ 4 ]  . poich i cambiamenti nelle dimensioni del tumore avvengono come conseguenza di modi cazioni biologiche e molecolari , tecniche di imaging funzionale vengono attualmente prese in considerazione come uno strumento aggiuntivo nella valutazione di molti aspetti del tumore , inclusa la risposta tumorale alla terapia . 
nella diagnostica per immagini oncologica , limaging pesato in diffusione , connesso con laggressivit e la risposta del tumore , essendo il valore della mappa del coef ciente di diffusione apparente ( adc ) inversamente proporzionale alla cellularit e allintegrit delle membrane cellulari [ 7 ]  . 
studi precedenti hanno valutato il ruolo potenziale della dwi nel monitoraggio della risposta alle terapie [ 4 , 710 ] , e nella distinzione tra tessuto normale e tumorale nella cervice uterina [ 11 ]  . 
la mappa adc di solito ri ette la complessit della massa tumorale , anche negli esami di follow - up effettuati durante la terapia , nei quali una diminuzione dei valori della mappa adc , causata da una riduzione della perfusione , possono essere seguiti da un aumento nel valore adc dovuto alla 768 radiol med ( 2011 ) 116 : 766780 the purpose of this study was to prospectively assess whether differences of adc values within the entire cervical cancer tumour volume before and after therapy may be considered as a quantitative method to monitor treatment response after nonsurgical therapy . patients and methods patients patients undergoing a rst mr examination for cervical cancer staging and a second examination for end of therapy followup during a 12 - month period between may 2008 and april 2009 were prospectively enrolled . 
written informed consent to undergo the procedure and to the use of anonymised clinical and imaging data for scienti c and / or educational purposes was obtained from all patients . 
for each patient , the following data were recorded on an excel spreadsheet le ( microsoft of ce excel 2003 , richmond , va , usa ) to be further evaluated : mr examination date , age , histological diagnosis obtained from pretherapy biopsy , therapy intent ( neoadjuvant or curative ) and type ( chemotherapy and / or radiotherapy ) , beginning and end therapy dates . 
for the control group , age , adc mean values standard deviations ( sd ) were recorded . mr technique all mr examinations were performed on a 1.5 - t scanner ( avanto , siemens , erlangen , germany )  . 
perci , le caratteristiche di diffusione di un tumore potrebbero essere meglio valutate stimando i valori adc dellintero volume tumorale , piuttosto che unicamente nellimmagine pi rappresentativa del tumore stesso . lo scopo di questo studio stato quello di valutare prospetticamente se le differenze nei valori di adc , considerando lintero volume tumorale della cervice uterina , prima e dopo terapia , possono essere considerate come un metodo quantitativo ef cace nel monitoraggio della risposta alle terapie non chirurgiche . pazienti e metodi pazienti in un periodo di 12 mesi , tra maggio 2008 e aprile 2009 , sono state arruolate pazienti che si sono sottoposte ad una risonanza magnetica basale per la stadiazione del tumore della cervice e ad una seconda valutazione alla ne della terapia . 
tutte le pazienti hanno rmato un consenso informato con il quale acconsentivano alla procedura e allutilizzo dei dati clinici e di imaging , resi anonimi , per scopi scienti ci e / o formativi . 
per ciascuna paziente , i seguenti dati sono stati raccolti in un foglio elettronico in formato excel ( microsoft of ce excel 2003 , richmond , usa ) , per essere successivamente esaminati : data dellesame di risonanza magnetica , et della paziente , diagnosi istologica ottenuta dalla biopsia eseguita prima di iniziare la terapia , data di inizio e ne del trattamento . 
stato riportato lo stadio clinico secondo linternational federation of gynecology and obstetrics ( figo ) alla diagnosi , successivamente modi cato retrospettivamente in accordo alla stadiazione figo modi cata [ 13 ]  . 
in base allo stadio figo le pazienti sono state in seguito anche divise in due sottogruppi comprendenti : tumori in stadio precoce ( tutti gli stadi compresi tra ib1 e iia2 ) , e tumori in stadio avanzato ( tra iib - ivb )  . stato anche memorizzato il diametro assiale massimo ed il volume della lesione cervicale prima e dopo la terapia insieme con il valore medio di adc ( come descritto nel paragrafo sulla misurazione dei valori adc ) ; per il gruppo di controllo sono stati memorizzati et delle pazienti e deviazione standard del valore medio di adc della cervice . tecnica rm tutti gli esami di risonanza magnetica sono stati eseguiti utilizzando una macchina da 1 , 5 t ( avanto , siemens , erlangen , germania )  . 
lesame standard della pelvi ha incluso : sequenze assiali t2 - pesate a respiro libero ( tempo radiol med ( 2011 ) 116 : 766780 mm ; ipat factor = 2 ) ; coronal t2 - weighted sequences ( tr / te 5 , 120 / 174 ms ; 260 - mm fov ; slice thickness 5 mm ; voxel size 1.00.75.0 mm ; ipat factor = 2 ) and para - axial t2 - weighted images , perpendicular to the longitudinal axis of the endocervical canal ( tr / te 5 , 060 / 174 ms ; 220 - mm fov ; slice thickness 3 mm ; voxel size 1.00.93.0 mm ; ipat factor = 2 )  . 
axial dwi sequences were acquired with the following imaging parameters : 40 slices ; voxel 3.02.75.0 mm ; transversal orientation ; fov read 340 mm ; slice thickness 5 mm ; tr / te 6 , 000 / 68 ms ; averages 4 ; ipat factor = 2 ; bandwidth 1 , 446 hz / px ; epi factor 69 ; 5 diffusion weightings ( b - values 0 ; 50 ; 250 ; 500 ; 900 s / mm2 )  . 
the adc value was measured over multiple slices on a four - view screen by uploading the t2 images as morphological images , the b = 0 dwi that most closely re ect the t2 images , thus allowing evaluation of the entire tumour diffusion , and the adc maps . 
following completion of therapy , if there was no residual tumour , the roi was traced on what was considered to be the normal residual cervix , as much as possible in the same area used in the pretherapy mr examination . 
 if there was a remnant of the tumour ( partial response ) or larger tumour ( no response ) , the rois were again traced on each slice to cover the entire tumour volume . 
le sequenze assiali dwi sono state acquisite con i seguenti parametri : 40 immagini ; voxel 3 , 02 , 75 , 0 mm ; orientamento trasversale ; campo di vista ( fov ) 340 mm ; spessore dello strato 5 mm ; tr 6000 ms ; te 68 ms ; averages 4 ; fattore ipat = 2 ; larghezza di banda 1446 hz / px ; fattore echo planar imaging ( epi ) 69 ; 5 pesature in diffusione ( valore - b 0 ; 50 ; 250 ; 500 ; 900 s / mm2 )  . 
le mappe adc sono state automaticamente generate dal software usando tutti i valori di b . se non controindicato , stato somministrato un mezzo di contrasto paramagnetico ( gadobenato dimeglumina [ gd - dtpa ] , 0 , 2 mmol / kg ; velocit di usso = 2 ml / s ) per via endovenosa ed stata acquisita una sequenza gradientecho 3d isotropica , assiale t1 fat - sat post - contrasto ( tr / te 7 , 0 / 2 , 1 ms ; ip angle 12 ; campo di vista di 340 mm ; spessore / intervallo5 / 1 ; dimensioni del voxel 0 , 90 , 90 , 9 mm ; nessun ipat )  . misurazione dei valori adc le caratteristiche di diffusione dellintero volume tumorale cervicale prima e dopo terapia , sono state valutate da un radiologo esperto ( 5 anni di esperienza in radiologia ginecologica ) due volte , per valutare la variabilit intra - osservatore , e da un radiologo non esperto , per valutare la variabilit inter - osservatore . 
il valore adc stato misurato su pi immagini su uno schermo con quattro riquadri , in cui venivano caricate le immagini t2 da usare come immagini morfologiche , le immagini pesate in diffusione con b = 0 , che meglio corrispondono alle immagini t2 e permettono una valutazione della diffusione dellintero volume tumorale e , in ne la mappa adc . 
finally , wilcoxons two - sample test was also performed to evaluate differences in adc values at the staging mr examination between cases and controls , responder and nonresponder tumours and tumours divided according to low and high stage . 
 results patients among 63 women who underwent a pelvic mr imaging for cervical cancer staging during the 1 - year period considered , 15 were excluded because they did not undergo the posttherapy mr examination at our institution , and 31 were excluded because they underwent surgical radical hysterectomy as rst - line therapy . 
therefore , our study cohort comprised 17 women ( median age 50 years ; range 3575 ) with cervical cancer who underwent two routine pelvic mr examinations at our institution , one for staging and one for evaluation after nonsurgical therapy ( chemotherapy and / or radiotherapy )  . 
 the control group comprised 17 women ( median age 46 years ; range 2373 ) who underwent mr imaging for the following indications : intestinal cancer ( n = 10 ) , uterine bromas ( n = 3 ) , retroperitoneal sarcoma ( n = 1 ) , retroperitoneal bromatosis ( n = 1 ) , vaginal cancer ( n = 1 ) , abdominal pain ( n = 1 )  . median interval between beginning of therapy and posttherapy mr evaluation of the study group was 80 ( range 61174 ) days ; median interval between the beginning of therapy and posttherapy mr evaluation was 32 ( range 1684 ) days . 
gadolinium - based contrast medium was administered to all cervical cancer patients : postgadolinium images did not in uence lesion conspicuity , but they helped attain a more precise evaluation of anatomical details in radiol med ( 2011 ) 116 : 766780 termine della terapia , non cera pi tumore residuo , la roi veniva tracciata su ci che era considerato residuo normale della cervice uterina , il pi possibile nella stessa area valutata nella risonanza magnetica pre - terapia . 
se , al termine della terapia , cera tumore residuo ( risposta parziale ) o una lesione tumorale di maggiori dimensioni ( nessuna risposta ) le roi venivano nuovamente tracciate su ciascuna immagine per coprire lintero volume tumorale . 
nel gruppo di controllo , la roi stata tracciata in unarea comprendente tessuto cervicale normale , escludendo lo stroma che normalmente ha un basso segnale sulle immagini t2 - pesate . analisi statistica i valori appaiati di adc prima e dopo terapia sono stati confrontati utilizzando il test non parametrico di wilcoxon . 
in ne , il test di wilcoxon stato anche utilizzato per valutare le differenze nei valori di adc tra i casi e i controlli , tra i tumori rispondenti e non rispondenti alle terapie , e tra i tumori divisi in stadio precoce ed avanzato ; tali valutazioni sono state effettuate solo alla risonanza magnetica di stadiazione . 
le analisi sono state effettuate usando un software standard ( sas versione 8.2 , sas insitute inc . , cary , usa )  . risultati pazienti delle 63 pazienti che sono state sottoposte ad una risonanza magnetica per stadiazione di un tumore della cervice durante il periodo in esame , 15 sono state escluse perch non hanno effettuato la risonanza magnetica post - terapia presso il nostro istituto , e 31 sono state escluse perch sono state sottoposte ad intervento chirurgico di isterectomia radicale come prima linea di trattamento . 
pertanto il nostro studio comprende una popolazione di 17 pazienti ( et media = 50 anni , range 3575 ) con tumore della cervice che hanno effettuato due risonanze magnetiche della pelvi di routine presso il nostro istituto , una per la stadiazione e una per la valutazione della risposta dopo terapie non chirurgiche ( chemioterapia e / o radioterapia )  . 
within the control group , gadolinium was not administered to one patient because of personal history of allergy to gadoliniu median time between the two mr examinations of the study group was 123 ( range 32185 ) days . 
among responders , 9 / 14 had no residual tumour after completion of therapies ( complete response ) and 5 / 14 still had residual tumour ( partial response )  . 
il mezzo di contrasto a base di gadolinio stato somministrato a tutte le pazienti : le immagini post - contrasto non hanno in uenzato la valutazione della lesione , ma hanno permesso una valutazione pi precisa dei dettagli anatomici nelle pazienti candidate ad intervento chirurgico . 
in all patients , the presence or absence of response to therapy was con rmed by clinical examination by the gynaecologist within 1 week after mr examination . interand intraobserver agreement interobserver agreement was assessed by comparing the two sets of measurements made by readers a and b using the bland and altman plot . 
intraobserver agreement was evaluated from the le due indagini di risonanza stato in media di 123 giorni ( range 32185 giorni )  . il diametro assiale massimo delle lesioni tumorali della cervice si ridotto in 14 / 17 lesioni ( rispondenti ) , con un diametro medio prima e dopo la terapia di 43 , 7 mm e 12 , 7 mm , rispettivamente . 
tra le pazienti che hanno mostrato una risposta al trattamento , 9 / 14 non avevano tumore residuo al termine della terapia ( risposta completa ) e 5 / 14 avevano un residuo di malattia ( risposta parziale )  . 
in tutte le pazienti la presenza o assenza di risposta alla terapia stata confermata dallesame clinico ginecologico eseguito entro una settimana dallindagine rm . variabilit intere intra - osservatore adc value measurements the mean number of pixels within the rois , used to average the single adc values over the number of slices , was 2 , 802.8 ( range 6711 , 015 ) for pretherapy mr examinations and 771.4 ( range 874 , 206 ) for posttherapy mr evaluation . 
among responder patients , mean adc values increased on average by 39.4% and tumour la variabilit inter - osservatore stata valutata confrontando i due set di valori ottenuti dai due radiologi a ( esperto ) e b ( non esperto ) usando il metodo di bland e altman . 
il valore medio di adc della cervice uterina nel gruppo di controllo era 1 , 4510 - 3 mm2 / s ( 1 , 241 , 70 ) , valore signi cativamente diverso da quello ottenuto nella popolazione in studio prima della terapia ( p < 0 , 0001 )  . 
4a - c a 58 - year - old woman with international federation of gynecology and obstetrics stage i b2 squamous - cell carcinoma who underwent neoadjuvant chemotherapy : axial t2 - weighted image of the cervix at staging magnetic resonance ( mr ) imaging shows the pretherapy cervical cancer ( a )  . 
diffusion - weighted imaging at b = 0 matched with the t2 - weighted image was used to trace the region if interest ( b ) , which was then applied to the corresponding image of the apparent diffusion coef cient map ( c )  . 
limmagine pesata in dwi a b = 0 , accoppiata allimmagine t2 stata usata per tracciare la roi ( b ) , che stata poi copiata sulla immagine corrispondente nella mappa adc ( c )  . 
 non si evidenziata una differenza statisticamente signicativa dividendo la popolazione in due ulteriori sottogruppi in base alla risposta completa o parziale , con una media dei valori di 1 , 0210 - 3 mm2 / s ( range 0 , 741 , 145 ) e 1 , 0210 - 3 mm2 / s ( range 0 , 971 , 3 ) rispettivamente per le pazienti con risposta completa e parziale ( p = 0 , 29 )  . 
tra le pazienti che hanno mostrato una risposta alla terapia , il valore medio di adc ha mostrato un incremento del 39 , 4% mentre il volume tumorale diminuito dell85 , 8% . 
non c una correlazione statisticamente signi cativa tra i valori di adc pre - terapia e la risposta tumorale post - terapia espressa come percentuale di riduzione del volume tumorale ( coef ciente di spearman 0 , 30 ; p = 0 , 23 )  . 
tumori con un maggiore incremento percentuale dei valori adc hanno mostrato una riduzione percentuale del volume tumorale maggiore , ma questo non stato statisticamente signi caradiol med ( 2011 ) 116 : 766780 fig . 
region of interest traced on the diffusion - weighted image at b = 0 ( b ) was applied to the corresponding apparent diffusion coef cient ( adc ) image ( c )  . 
our data show a signi cant difference in adc values both between normal and cancerous tissue in the cervix and between cervical tumours before and after nonsurgical therapy for all patients ( p = 0.003 ) , with a signi cant increase of adc values for responder tumours ( p = 0.0009 ) and a relative decrease of adc values for nonresponder tumours . 
 [ 11 ] , who demonstrated a signi cant difference in adc values between healthy and cancerous cervix , as well as an increase of adc values in response to therapy in a subgroup of nine cancer patients followed up after therapy , even though they evaluated the adc values only on a single slice rather than on the entire tumour volume . 
in addition to naganawa et al . , other studies showed a signi cant difference in adc values of normal cervix compared with cervical carcinoma [ 16 , 17 ] , but evaluation of the diffusion characteristics of normal and cancerous tissue was made using relatively low ( 600 s / mm2 ) maximum b - values [ 4 , 16 , 17 ] or only one high b - value ( 1 , 000 s / mm2 ) [ 18 , 19 ]  . 
 the information provided by dwi and adc values has been related to cellular density , diffusion of protons within a tissue , tumour structure and intralesional components [ 79 , 20 ]  . 
an inverse correlation between cellular density and adc values has been well described for brain [ 21 ] , prostate [ 22 ] , renal [ 23 ] , breast [ 24 ] and gynaecological [ 16 , 25 ] tumours . 
the choice of b - values in uences the adc measurements , as the adc value is in uenced at low b - values by perfusion from local vasculature [ 7 , 26 , 27 ] and at moderate to high b - values by compartmentalisation in intraand extracellular spaces [ 28 ]  . 
 [ 7 ] , dwi acquisition should be performed with a high maximum b - value ( such as 900 s / mm2 ) and several lower b - values ( 0 ; 50 ; 250 ; 500 s / mm2 ) and , given the heterogeneous cellularity within a tumour , a composite of rois over multiple slices should be delineated if a tumour is being followed over time to better re ect the heterogeneity of the entire + 41 , 8% e - 2 , 5% ( p = 0 , 04 )  . 
non ci sono state differenze statisticamente signi cative nei valori di adc alla rm basale tra i tumori rispondenti e quelli non - rispondenti ( p = 0 , 09 )  . 
non ci sono state differenze statisticamente signi cative nei valori di adc tra i tumori suddivisi in stadio precoce ( n = 9 ) e avanzato ( n = 8 ) ( p = 0 , 96 ) , anche dopo aver escluso i tre tumori non - rispondenti ( p = 0 , 56 )  . discussione le immagini pesate in diffusione sono attualmente utilizzate nella pratica dellimaging oncologico come un possibile strumento per la caratterizzazione tissutale , monitoraggio della risposta alle terapie ed identi cazione di recidive tumorali , senza il bisogno di mezzo di contrasto [ 7 ]  . 
i nostri dati dimostrano una differenza signi cativa dei valori di adc sia tra tessuto normale e tessuto neoplastico nella cervice , sia nel tessuto tumorale prima e dopo terapia non chirurgica per tutte le pazienti ( p = 0 , 003 ) , con un pi signi cativo incremento dei valori di adc per i tumori rispondenti ( p = 0 , 0009 ) , e un relativo decremento dei valori di adc per i tumori non - rispondenti . 
inoltre , i cambiamenti percentuali dei valori di adc prima e dopo terapia erano pi alti nei rispondenti rispetto ai non rispondenti ( p = 0 , 04 )  . 
 [ 11 ] , che hanno dimostrato una differenza signi cativa nei valori di adc tra la cervice sana e quella neoplastica con un incremento dei valori di adc in risposta alla terapia in un sottogruppo di 9 pazienti neoplastiche seguite dopo terapia , sebbene loro avessero valutato il valore di adc solo su una singola immagine invece che sullintero volume tumorale . 
 anche altri studi hanno dimostrato una signi cativa differenza dei valori di adc della cervice normale rispetto alla cervice neoplastica [ 16 , 17 ] , ma la valutazione delle caratteristiche di diffusione del tessuto normale e neoplastico stata fatta utilizzando un valore di b massimo relativamente basso ( 600 s / mm2 ) [ 4 , 16 , 17 ] , oppure utilizzando solo un alto valore di b ( 1000 s / mm2 ) [ 18 , 19 ]  . le informazioni ottenute dalla immagini pesate in diffusione e dai valori della mappa adc sono correlate alla densit cellulare , alla diffusione dei protoni presenti nel tessuto , alla struttura tumorale , ed a componenti intralesionali [ 79 , 20 ]  . 
una correlazione inversa tra la densit cellulare e i valori di adc stata ben descritta per i tumori dellencefalo [ 21 ] , della prostata [ 22 ] , del rene [ 23 ] , della mammella [ 24 ] e per quelli ginecologici [ 16 , 25 ]  . 
la scelta del valore di b in uenza le misurazioni di adc , poich il valore di adc in uenzato : a valori di b bassi dalla perfusione delle strutture vascolari locali [ 7 , 26 , 27 ] , e a valori di radiol med ( 2011 ) 116 : 766780 tumour volume over time [ 7 ]  . 
 [ 4 ] have shown that cellular death and vascular changes caused by therapy could be detected by dwi before a reduction of lesion diameter becomes apparent at morphological imaging . 
according to our results , dwi based on many b - values and adc measurements applied to the entire tumour volume may be used as an adjunctive , but not substitutive , tool to the standard mr imaging examination to assess the response of cervical cancer to nonsurgical therapies . 
nevertheless , the usual morphological images ( t2and t1 - weighted images , with or without administration of contrast medium ) were still necessary to address speci c questions , such as involvement of parametria , endocervix , vaginal fornices and lymph nodes [ 29 ] , as well as to give information about tumour volume and anatomical details of in ltration of adjacent structures in patients for whom surgery or radiotherapy is planned [ 30 ]  . 
thus , the usual management of cervical cancer patients undergoing nonsurgical therapy , based on one mr examination before therapies and one after the end of therapies , was not altered so as not to give additional discomfort to the patients . 
based on our results , further studies , including an earlier mr evaluation , should be performed to assess whether changes in dwi occur earlier than changes in size and , as a consequence , whether the use of dwi may be considered as an early biomarker of tumour response to therapies . 
the possibility of predicting responder from nonresponder uterine cervical tumours , as well as early identi cation of nonresponder tumours , would help in addressing cervical cancer patients to stop ineffective treatments and to avoid delays in starting alternative , potentially more effective , treatments . 
 [ 7 ] le acquisizioni dwi dovrebbero essere eseguite con un elevato valore massimo di b ( come 900 s / mm2 ) e pi valori bassi ( 0 , 50 , 250 , 500 s / mm2 ) e , in considerazione della eterogeneit cellulare presente nel tumore , dovrebbe essere tracciata una serie di roi su multiple sezioni se il tumore viene seguito nel tempo , per meglio ri etterne leterogeneit dellintero volume [ 7 ]  . le sequenze dwi utilizzate in questo studio , come la valutazione delle mappe adc , sono state eseguite in accordo a queste raccomandazioni . 
 [ 4 ] hanno dimostrato che la morte cellulare ed i cambiamenti vascolari indotti dalla terapia possono essere identi cati dalla dwi prima che diventi evidente una riduzione del diametro della lesione alle immagini morfologiche . secondo i nostri risultati , la sequenza dwi basata su pi valori di b e le misurazioni di adc eseguite sullintero volume tumorale possono essere usate in aggiunta , ma non come strumento sostitutivo allo studio rm standard , nel valutare la risposta a terapie non chirurgiche del tumore della cervice uterina . infatti , nella lettura dellesame rm , le sequenze dwi servono ad identi care la presenza e la sede delle lesioni cervicali . 
nonostante ci , le immagini morfologiche standard ( immagini pesate in t1 e t2 , con o senza la somministrazione di mezzo di contrasto ) sono ancora necessarie per rispondere a speci che domande , come il coinvolgimento dei parametri , dellendocervice , dei fornici vaginali e dei linfonodi [ 29 ] , come anche nel dare informazioni sul volume tumorale e sui dettagli anatomici dellin ltrazione di strutture adiacenti , soprattutto in pazienti candidate alla chirurgia e alla radioterapia [ 30 ]  . quando questo studio stato iniziato , non cerano evidenze de nitive sullutilit delle dwi nella valutazione della risposta alla terapia nel tumore della cervice . 
di conseguenza , la gestione normale delle pazienti con questa patologia , candidate a terapia non chirurgica , attualmente basata su uno studio rm eseguito prima delle terapie e uno studio eseguito dopo la ne delle terapie , non stata modicata per non arrecare ulteriori disagi alle pazienti . 
sulla base dei nostri risultati , ulteriori studi , includenti una pi precoce valutazione rm , dovrebbero essere eseguiti per stabilire se le modi cazioni in dwi sono pi precoci rispetto ai cambiamenti di dimensione e , di conseguenza , se lutilizzo delle dwi pu essere considerato come un marcatore precoce della risposta tumorale alle terapie . dzik - jurasz et al . 
 [ 31 ] hanno suggerito che elevati valori di adc prima del trattamento possono rappresentare un indicatore di necrosi che potrebbe essere predittivo di una scarsa 778 radiol med ( 2011 ) 116 : 766780 mcveigh et al . 
 [ 16 ] , we observed no signi cant difference in the median of grouped adc values of responder and nonresponder tumours at the staging mri ( p = 0.09 ) , either in the two readings by the same reader ( intraobserver agreement ) or between readings of the two readers ( interobserver agreement )  . 
median adc values of responders were , in fact , lower ( 1.0210 - 3 mm2 / s ) than those of nonresponders ( 1.1210 - 3 mm2 / s ) , but this difference did not reach signi cance . 
thus , in this study , a cutoff value of adc to distinguish the nonresponder tumours based on the sole dwi information from pretherapy mr examination was not identi ed . 
 the lack of correlation between percent increase in adc values and percent reduction of tumour volumes found in this series may be due to the high number of completeresponder tumours . 
indeed , 9 / 14 tumours showed a 100% reduction , independently of percent increase of adc values , whereas 5 / 14 showed a partial response ( tumour volume reduction lower than 100% ) ; therefore , a statistical analysis in this subgroup of patients would have been underpowered . 
this difference may be due to the different evaluation of the adc maps made over multiple slices to cover the entire volume of the tumour in this study and , in contrast , on the single most representative slice in the study by mcveigh . 
undertaking a more powerful study in a reasonably short time in order to minimise variations in treatment and in mr technique would likely require a multicentric study , which would introduce intersite variability . 
 la possibilit di distinguere i tumori della cervice uterina rispondenti dai non rispondenti , e la conseguente identi cazione precoce dei tumori non rispondenti , potrebbe aiutare ad indirizzare le pazienti con questa patologia ad interrompere trattamenti inef caci e ad evitare ritardi nelliniziare trattamenti alternativi potenzialmente pi ef caci . 
 [ 16 ] , noi non abbiamo osservato nessuna differenza nella mediana dei valori di adc dei tumori rispondenti e di quelli non rispondenti alla rm di stadiazione ( p = 0 , 09 ) , sia nelle due letture dello stesso osservatore ( accordo intra - osservatore ) sia nelle letture dei due osservatori ( accordo inter - osservatore )  . 
la media dei valori di adc dei rispondenti stata infatti pi bassa ( 1 , 0210 - 3 mm2 / s ) rispetto a quella dei non rispondenti ( 1 , 1210 - 3 mm2 / s ) , ma questa differenza non ha raggiunto la signi cativit . 
pertanto , in questo studio non stato identi cato un valore di adc per distinguere i tumori non rispondenti sulla base della sola informazione della dwi dello studio rm preterapia . 
questa mancanza di signi cativit e di speci cit potrebbe essere correlata alla distribuzione dei valori ed al piccolo numero di pazienti non rispondenti ( n = 3 )  . 
 lassenza di correlazione tra lincremento percentuale dei valori di adc e la riduzione percentuale del volume tumorale riscontrato in questo studio , potrebbe essere dovuto allelevato numero di tumori che hanno risposto completamente . 
 infatti , 9 / 14 tumori hanno mostrato una riduzione del 100% , indipendentemente dallincremento percentuale del valore di adc , mentre 5 / 14 hanno mostrato una risposta parziale ( riduzione del volume tumorale < 100% ) ; pertanto unanalisi statistica in questo sottogruppo di pazienti potrebbe essere non adeguata . in contrasto con mcveigh et al . 
 [ 16 ] , i nostri valori di adc non hanno mostrato differenze signi cative tra i tumori raggruppati in stadi precoci ed avanzati ( p = 0 , 96 )  . 
questa discordanza potrebbe essere dovuta alla diversa valutazione delle mappe adc , effettuate su multiple sezioni a coprire lintero volume del tumore in questo studio , e sulla sola sezione pi rappresentativa nello studio di mc veigh et al . 
precedenti studi non hanno dimostrato signi cative differenze nel valore di adc tra i tumori squamocellulari e gli adenocarcinomi [ 4 , 11 , 16 ] , mentre liu et al . 
per il basso numero di adenocarcinomi inclusi in questo gruppo di studio ( 3 / 17 ) , in accordo con la distribuzione di questo tipo istologico , riportata dallistituto nazionale dei tumori degli usa come 25 , 2% contro il 68 , 7% dei tumori squamocellulari [ 32 ] , questa valutazione non stata eseguita e non sono state fatte analisi statistiche . un limite di questo studio il basso numero di pazienti inclusi . 
purtroppo , per intraprendere uno studio pi ampio in tempi ragionevolmente pi brevi , per minimizzare le variazioni nel trattamento e nella tecnica rm , sarebbe stato radiol med ( 2011 ) 116 : 766780 parameters and the same mr machine . 
furthermore , the same method of tracing rois over the slices was applied to all examinations in the three sets of data , acquired twice by the same reader and once by the second reader , thus ensuring optimal intrapatient comparison and consistency of dwi comparison within the cohort . 
however , the aim of this study was demonstrating changes in adc values in cervical cancers before and after therapy and correlating these changes with variations in tumour size rather than assessing whether a negative mr examination matched the absence of residual tumour at surgery . 
 in conclusion , this study showed signi cant differences in adc values of normal and cancerous cervical tissue and of cervical tumours before and after nonsurgical therapies , with a signi cantly higher percent increase of adc values in responders than in nonresponders . 
in the future , dwi may be considered as an additional tool to the standard mr examination of the pelvis in cervical cancer patients to assess response to nonsurgical therapy , with neither exposure to ionising radiation nor additional discomfort for the patient , and no additional need for contrast medium injection . necessario uno studio multicentrico , che avrebbe introdotto una variabilit inter - sede . 
 inoltre , stato applicato a tutti gli esami lo stesso metodo per tracciare le roi con la valutazione di tre serie di dati , valutati due volte dallo stesso lettore e una volta dal secondo lettore , assicurando una ottima comparazione intra - paziente ed anche allinterno della popolazione . 
tuttavia , lo scopo dello studio era dimostrare cambiamenti dei valori di adc nei tumori della cervice prima e dopo terapia , e correlare questi cambiamenti con la variazione dimensionale del tumore , piuttosto che stabilire se una rm negativa corrisponda alla assenza di tumore residuo alla chirurgia . 
 in conclusione , questo studio mostra differenze signicative dei valori di adc tra tessuto cervicale normale e tumorale , e nei tumori della cervice prima e dopo terapie non chirurgiche , con un incremento percentuale del valore di adc signi cativamente pi alto nei rispondenti rispetto ai non rispondenti . 
in futuro , le immagini pesate in diffusione potrebbero essere considerate come strumento aggiuntivo allesame rm standard della pelvi in pazienti con tumore della cervice , per valutare la risposta alle terapie non chirurgiche , senza esposizione a radiazioni ionizzanti , senza disagi aggiuntivi per le pazienti e senza aggiunta di mezzo di contrasto . 
martinoli4 1department of radiology , national institute for cancer research , largo rosanna benzi 10 , 16138 genova , italy 2department of endocrinological & medical sciences ( disem ) and center of excellence for biomedical research , university of genova , genova , italy 3instituto de investigacin biomdica ( iib ) - sant pau , endocrinology / medicine department and centro de investigacin biomdica en red de enfermedades raras ( ciber - er , unidad 747 ) , isciii ; universitat autonoma de barcelona , barcelona , spain 4depatment of radiology dicmi , universit di genova , genova , italy correspondence to : a . 
in the early stage of disease , peripheral nerve enlargement associated with carpal tunnel syndrome or cubital tunnel syndrome and thickening of retinacula , such as a1 pulley in trigger nger , represent the features that may be seen by radiologists and are worthy of an endocrinological evaluation . 
few and nonspeci c symptoms characterise the initial phases of the disease , and therefore , most patients will have generally consulted many specialists ( most frequently musculoskeletal radiologists ) before an adequate endocrinological assessment is performed . 
the rst and most important therapeutic approach to acromegaly is early diagnosis , whereas the therapeutic goals are to eliminate morbidity and reduce mortality to the expected ageand sex - adjusted rates and prevent the development of systemic complications . 
when both radiological and clinical abnormalities are present , an endocrinological workup is useful to diagnose the disease in an early phase . riassunto lobiettivo del lavoro di riassumere le complicanze precoci dellacromegalia . 
nelle fasi precoci della malattia lingrandimento dei nervi periferici associato alla sindrome del tunnel carpale o del tunnel cubitale e lispessimento dei retinacoli come la puleggia a1 nel dito a scatto rappresentano i segni che possono essere notati dal radiologo e che meriterebbero una valutazione specialistica endocrinologica . 
nelle fasi iniziali i sintomi possono essere pochi e aspeci ci , pertanto i pazienti consultano molti specialisti , tra cui il radiologo muscolo - scheletrico , prima di effettuare una visita specialistica endocrinologica . 
 dato che gli obiettivi terapeutici sono la riduzione della morbilit e della mortalit , la diagnosi precoce rimane il miglior approccio terapeutico possibile per prevenire le complicanze sistemiche . parole chiave tunnel carpale tunnel cubitale dito a scatto acromegalia ecogra a complicazioni osteoarticolare 782 radiol med ( 2011 ) 116 : 781792 keywords carpal tunnel cubital tunnel trigger nger acromegaly ultrasound complications musculoskeletal introduction introduzione acromegaly is a rare syndrome that usually develops over many years due to long - term exposure to elevated levels of growth hormone ( gh ) and peripheral insulin - like growth factor 1 ( igf - 1 ) [ 1 ]  . 
however , clinical signs such as somatic dis gurements , voice alterations and extremity enlargement are considered pathognomonic and can suggest the diagnosis during the rst clinical evaluation [ 3 , 4 ] and are as important as symptoms for an early diagnosis . 
nevertheless , the disease still goes undetected because of limited knowledge of the syndrome [ 4 ]  . radiologists are among those specialists who may evaluate a patient affected by acromegaly before the nal diagnosis is achieved , especially for the radiological symptoms . 
in this case , initial recognition of the clinical signs , together with a radiological evaluation of symptoms , could suggest to radiologists the diagnosis of acromegaly and the need to refer the patient for endocrinological evaluation . 
 musculoskeletal manifestations of this syndrome are frequent , and virtually all patients develop symptoms or signs related to arthropathy , but these signs have been poorly studied [ 46 ]  . 
 the aim this review is to highlight the early musculoskeletal complications of acromegaly in order to enable the radiologist to suspect a possible diagnosis in an early phase of the disease and refer the patient for endocrinological assessment . 
 lacromegalia una sindrome rara che si sviluppa lentamente nel corso degli anni in seguito a una prolungata esposizione ad elevati livelli di ormone della crescita ( gh ) e fattore di crescita insulino - simile di tipo i ( igf - 1 ) [ 1 ]  . 
al momento della diagnosi i pazienti generalmente presentano alterazioni somatiche del volto , ingrandimento delle mani e dei piedi , e ipertro a dei tessuti molli [ 2 ]  . 
queste caratteristiche vennero chiamate acromegalia , dal greco acros ( ) , estremit , e megalos ( ) , ingrandite [ 3 ]  . la diagnosi di acromegalia signi cativamente ritardata a causa della natura insidiosa della malattia . 
comunque i segni clinici come le alterazioni somatiche , le alterazioni della voce , lingrandimento di mani e piedi sono considerati patognomonici e possono suggerire la diagnosi durate un primo esame clinico [ 3 , 4 ] e questi segni sono importanti come i sintomi nelleffettuare una diagnosi precoce . 
 le manifestazioni osteoarticolari di questa sindrome sono frequenti e virtualmente tutti i pazienti sviluppano sintomi e segni correlati allartropatia acromegalica , tuttavia queste manifestazioni sono state relativamente poco studiate [ 46 ]  . 
lartropatia acromegalica tipicamente assomiglia allosteoartrosi e colpisce prima che la diagnosi nale sia raggiunta [ 57 ]  . lo scopo di questo articolo di enfatizzare le complicanze muscolo - scheletriche precoci dellacromegalia per rendere il radiologo capace di sospettare la presenza della malattia nelle fasi pi precoci . 
in questo modo verrebbe garantita una pi rapida valutazione endocrinologica . radiol med ( 2011 ) 116 : 781792 radiographic features of acromegaly aspetti radiogra ci dellacromegalia radiographic changes in the peripheral joints are typically widespread . 
 il paziente acromegalico tipicamente presenta : crescita delle ossa acrali con bozze frontali prominenti , aumento della taglia delle mani e dei piedi , slargamento della mandibola e prognatismo , aumento dello spazio tra i denti incisivi [ 8 ]  . 
tra le differenti e non speci che manifestazioni osteoarticolari dellacromegalia , alcune possono suggerire la diagnosi se associate a sintomi e segni clinici tipici ( tabelle 1 e 2 ) [ 10 , 11 ]  . sindrome del tunnel carpale fig . 
note the advanced arthropathy at the level of the rst metatarsophalangeal joint , which is more evident on the left side ( asterisks ) , with hallux valgus , bone erosions and osteophytes . 
a livello della prima articolazione metatarso - falangea si notano i segni di unartropatia avanzata , pi evidente a sinistra ( asterisco ) con alluce valgo , erosioni osse e osteo ti . 
da notare anche laumento di dimensioni dei sesamoidi , tipico dellacromegalia ( teste di freccia )  . i pazienti acromegalici possono soffrire di disturbi sensitivi alle mani come parestesie , bruciore , intorpidimento . 
lassociazione tra acromegalia e sindrome del tunnel carpale stata riconosciuta come una frequente complicanza della malattia con una prevalenza che pu raggiungere il 64% al momento della diagnosi [ 2 , 3 , 8 , 10 ]  . 
alcuni autori hanno riferito che la sindrome del tunnel carpale potrebbe essere causata da un aumento delledema allinterno del nervo mediano 784 radiol med ( 2011 ) 116 : 781792 fig . 
2 sagittal t2 - weighted fat - suppressed magnetic resonance ( mr ) image of the lumbar spine in a 41 - year - old acromegalic patient ( estimated disease duration : 4 years ) showing an increase of intervertebral disc spaces at the level of l3 - l4 and l4 - l5 . 
5 axial t2 - weighted turbo spin - echo magnetic resonance image of a 55 - year - old acromegalic woman demonstrates hypertrophy of the facet joints ( arrow ) , with associated fatty in ltration of the paraspinal muscles ( asterisks )  . 
5 immagine in risonanza magnetica ( rm ) assiale t2 pesata di un paziente di 55 anni con ipertro a delle faccette articolari ( freccia ) e in ltrazione adiposa dei muscoli paraspinali ( asterischi )  . radiol med ( 2011 ) 116 : 781792 table 1 most frequent signs and symptoms present at diagnosis in acromegalic patients sign / symptom percentage hand / foot enlargement facial feature changes hyperhidrosis headache joint pain gonadal dysfunction fatigue macroglossia increased spacing between teeth ingrandimento di mani e piedi cambio della morfologia somatica iperidrosi cefalea dolore articolare disfunzione gonadica astenia macroglossia aumento dello spazio tra i denti tabella 1 sintomi e segni pi frequento nei pazienti con acromegalia al momento della diagnosi segni / sintomi percentuale acromegalic patients typically present with acral bony overgrowth that results in frontal bossing , increased hand and foot size , mandibular enlargement with prognathism and widened space between the lower incisor teeth [ 8 ]  . 
among the different nonspeci c osteoarticular features of acromegaly , some may suggest the diagnosis if related with the clinical signs and symptoms of the disease ( tables 1 and 2 ) [ 10 , 11 ]  . 
association with acromegaly and median neuropathy or carpal tunnel syndrome is recognised as a common condition of this disease , with a prevalence up to 64% of patients at presentation [ 2 , 3 , 8 , 10 ] , and nerve conduction studies reported subclinical abnormalities in the vast majority of patients [ 916 ]  . 
moreover , some authors have reported that the development of a carpal tunnel syndrome is probably due to oedema of the median nerve within the carpal tunnel rather than extrinsic compression from increased volume of the carpal tunnel piuttosto che da una compressione estrinseca allinterno del tunnel [ 13 ]  . 
 stato recentemente dimostrato , utilizzando lecogra a ad alta risoluzione , che nei pazienti con acromegalia , un ingrandimento diffuso dei nervi pu essere responsabile della sindrome del tunnel carpale [ 10 ]  . 
nelle neuropatie da intrappolamento laspetto eco strutturale del nervo diventa uniformemente ipoecogeno con perdita del normale pattern fascicolare a livello della sede di compressione e prossimalmente ad esso [ 10 ]  . 
a livello del tunnel carpale , nei pazienti con acromegalia , larea misurata risultata di 16 , 54 , 4 mm2 , mentre nella popolazione normale larea risulta inferiore ai 10 mm2 . 
 lingrandimento dei nervi periferici nellacromegalia una caratteristica intrinseca della malattia ed correlata alla durata di malattia , al controllo clinico della malattia e ai valori plasmatici di igf - 1 . 
le principali diagnosi differenziali radiologiche includono la lebbra e il diabete mellito in quanto in queste condizioni patologiche pu essere presente un diffuso ingrandimento dei nervi periferici associato alla sindrome del tunnel carpale [ 1720 ]  . 
anche nei pazienti con malattia controllata le dimensioni dei nervi sono pi grandi che nei soggetti normali [ 21 ] , per questo motivo solo una diagnosi precoce e un rapido controllo della malattia pu permettere una normalizzazione dei nervi [ 21 ]  . 
nella nostra casistica il 60% dei pazienti con sindrome del tunnel carpale al 786 radiol med ( 2011 ) 116 : 781792 table 2 radiological ndings of musculoskeletal features of acromegaly radiological ndings site advanced musculoskeletal manifestations decreased bone mineral density vertebral fractures increased sesamoid volume increased heel fat - pad thickness osteoarthritis proliferative enthesopathy baastrups disease bone overgrowth increased thickness of a1 pulley enlargement of distal phalanx diffuse idiopathic skeletal hyperostosis ( dish ) early musculoskeletal manifestations widening of articular spaces increase of intervertebral disc spaces lumbar spine dorsal and lumbar spine foot ( hallux ) plantar foot mcp , mtp , ipj of hand and foot ; spine enthesis especially of the foot lumbar spine acral bones . 
tendon insertions hands fingers thoracic spine mcp , mtp , ipj of hand and foot ; spine spine early musculoskeletal manifestations suggesting an early diagnosis if other clinical features are present trigger nger carpal tunnel syndrome cubital tunnel syndrome diffuse nerve enlargement hands median nerve ulnar nerve ulnar and median nerve mc , metacarpophalangeal ; mtp , metatarsophalangeal ; ipj , interphalangeal joint tabella 2 reperti radiologici delle complicanze muscoloscheletriche dellacromegalia . 
articolazione reperti radiologici sede manifestazioni tardive diminuzione densit ossea fratture vertebrali aumento di volume dei sesamoidi aumento di spessore del grasso della pianta del piede artrosi entesopatia proliferativa malattia di baastrup crescita ossea inserzioni tendinee ispessimento puleggia a1 ingrandimento falangi distali dish manifestazioni precoci ampliamento spazi articolari aumento di spessore dei dischi colonna lombare colonna dorsale e lombare piede ( alluce ) pianta del piede mcp , mtp , ipj di mani e piedi ; colonna entesi del piede colonna lombare ossa acrali mani dita colonna toracia mcp , mtp , ipj mani e piedi ; colonna colonna manifestazioni precoci che suggeriscono ulteriori accertamenti se sono presenti le caratteristiche siche dellacromegalia dito a scatto sindrome del tunnel carpale sindorme del tunnel cubitale diffuso ingrandimento dei nervi mcp , metacarpofalangea ; mtp , metatarsofalange ; ipj , interfalangea mani nervo mediano nervo ulnare nervi mediano e ulnare radiol med ( 2011 ) 116 : 781792 contents [ 13 ]  . 
other studies , on the contrary , have reported that carpal tunnel syndrome in acromegaly is due either to oedematous synovial tissues that compresses the median nerve or to irreversible narrowing of the carpal tunnel [ 12 , 1416 ]  . 
 it has been demonstrated , by using high - resolution ultrasound , that in acromegalic patients , carpal tunnel syndrome may be induced by the diffuse nerve swelling that affects acromegalic limbs , [ 10 ]  . 
in entrapment neuropathies , the nerve echotexture may become uniformly hypoechoic , with loss of the fascicular pattern at the level of the compression and proximal to it [ 10 ]  . 
at the level of the carpal tunnel , the median nerve csa was measured as 16.54.4 mm2 in acromegalic patients , whereas in the normal population , the mean area of the median nerve at the carpal tunnel was < 10 mm2 . 
 main radiological differential diagnoses include leprosy and diabetes , because in these diseases , diffuse enlargement of peripheral nerves associated with carpal tunnel syndrome may be found [ 1720 ]  . 
for this reason , only an early diagnosis and prompt disease control might enable nerve normalisation [ 21 ]  . acromegalic patients often have a history of previous , unsuccessful , surgery for carpal tunnel syndrome . 
a transverse 17 - 5 mhz ultrasound image obtained at the level of the carpal tunnel demonstrates an enlarged median nerve ( cross - sectional area : 14.5 mm2 , normal value < 10 mm2 ) in an asymptomatic patient . 
b the median nerve ( mn ) enlargement persisted ( crosssectional area : 8.2 mm2 , normal value < 5 mm2 ) also at the level of the midforearm between the exor digitorum super cialis and profundus muscles ( ft )  . 
 ecogra a assiale a 17 , 5 mhz a livello del tunnel carpale che dimostra un ingrandimento del nervo mediano ( area 14 , 5 mm2 , normale < 10 mm2 ) in assenza di sintomi in a . 
il nervo mediano ( mn ) risulta ingrandito ( area : 8 , 2 mm2 , normale < 5 mm2 ) anche a livello dellavambraccio tra i tendini essori delle dita ( ft ) in b . 
 un radiologo muscolo scheletrico dovrebbe cercare le tipiche caratteristiche dellacromegalia quando diagnostica un tunnel carpale bilaterale e un diffuso ingrandimento dei nervi , con o senza pregressa chirurgia per sindrome del tunnel carpale . 
se questi indizi coincidono , il paziente dovrebbe essere inviato ad una visita specialistica endocrinologica . sindrome del tunnel cubitale la sindrome del tunnel cubitale , cio lintrappolamento del 788 radiol med ( 2011 ) 116 : 781792 fig . 
transverse 17 - 5 mhz ultrasound image obtained at the level of the carpal tunnel demonstrates a bilaterally enlarged median nerve ( cross - sectional area : 21.5 mm2 and 22 mm2 , normal value < 10 mm2 ) with loss of the normal fascicular echotexture and hypoechoic appearance in a symptomatic patient . 
lecogra a assiale a 17 , 5 mhz a livello del tunnel carpale dimostra un ingrandimento bilaterale del nervo mediano con perdita della normale struttura fascicolare ( area : 21 , 5 mm2 e 22 mm2 , normale < 10 mm2 )  . 
 a musculoskeletal radiologist should look for the typical features of acromegaly when nding a patient with bilateral carpal tunnel and diffuse nerve enlargement , with or without previous surgery for carpal tunnel syndrome : for example , information regarding changes in the size of rings or shoes should be elicited . 
 cubital tunnel syndrome ulnar nerve entrapment at the elbow ( cubital tunnel syndrome ) is the second most common peripheral nerve entrapment syndrome following carpal tunnel syndrome in the normal population . 
moreover it has been found that cubital tunnel syndrome in acromegalic patients has a prevalence of 21% , similar to that for carpal tunnel syndrome , and can be improved with clinical control of the disease . 
inoltre , stato dimostrato che la prevalenza della sindrome del tunnel cubitale nei pazienti affetti da acromegalia raggiunge il 21% , dato simile alla prevalenza del tunnel carpale , e che pu migliorare solo con il controllo clinico della malattia . 
in primo luogo deve differenziare la sindrome del tunnel carpale dalla sindrome del tunnel cubitale , in secondo luogo deve escludere le caratteristiche compatibili con acromegalia nei pazienti con tunnel cubitale . 
in generale , la sindrome del tunnel carpale correlata ad un ingrandimento del nervo mediano prossimale rispetto al tunnel carpale , mentre la sindrome del tunnel cubitale ad un ingrandimento del nervo prossimale rispetto al gomito . 
di fatto la chirurgia pu essere considerata il trattamento di scelta nella sindrome del tunnel carpale , mentre nella sindrome del tunnel cubitale pu essere proposta la terapia conservativa [ 22 ]  . 
a short - axis ultrasound image of the ulnar nerve ( un ) at the cubital tunnel shows a markedly enlarged ulnar nerve in a symptomatic de novo acromegalic patient . 
firstly , carpal tunnel syndrome must be differentiated from cubital tunnel syndrome ; secondly it is necessary to look for typical features of acromegaly in a patient with cubital tunnel syndrome . 
in general , carpal tunnel syndrome is related to an enlarged median nerve proximally to the carpal tunnel , whereas cubital tunnel syndrome is related to an enlarged ulnar nerve proximally to the elbow . 
thus , nerve swelling is one of the predisposing factors to nerve entrapment in both carpal and cubital tunnel syndromes . differentiating between the two entrapment neuropathies is crucial due to the different therapeutic approaches . 
 in fact , in carpal tunnel syndrome , surgery is considered the treatment of choice , whereas in cubital tunnel , conservative therapy including patient education to avoid activities that produce symptoms , such as repetitive elbow exion or direct pressure to the medial epicondyle , splinting and work environment modi cation [ 22 , 23 ]  . 
 tuttavia la patogenesi di questa sindrome sembra simile a quella del tunnel carpale in cui la cronica e abbondante esposizione a gh e igf - 1 determina un diffuso ingrandimento dei nervi . 
nellacromegalia i valori normali dellarea del nervo ulnare sono 9 , 5 mm2 a livello dellavambraccio e 13 , 1 mm2 a livello del braccio , mentre a nella popolazione normale sono 5 , 3 mm2 e 6 , 6 mm2 rispettivamente . 
quindi un consulto specialistico endocrinologico pu essere suggerito in presenza di nervi ingranditi fuori dai canali osteo brosi . 790 radiol med ( 2011 ) 116 : 781792 cubital tunnel syndrome has only recently been recognised as being associated with acromegaly [ 22 ] , and therefore , the literature about this syndrome in relation to acromegaly is poorly represented . 
however , the pathogenesis of this entrapment syndrome seems similar to that of carpal tunnel syndrome , in which the chronic and exaggerated stimulation of gh and igf - 1 determines a diffuse enlargement of the nerves . 
 trigger nger trigger nger , a transient locking of the ngers in exion , is a common condition in which there is thickening and constriction of the proximal part of the exor tendon sheath at the base of the nger or thumb [ 24 ]  . 
this pulley is highly important for pathology : it is not only a stabiliser of the exor tendons during nger exion but it is a target area for trigger nger in different pathological conditions , such as acromegaly and scleroderma [ 24 ]  . 
it is known that the bone and hyaline cartilage are typical targets of gh and igf - 1 excess , and normalisation of gh and igf - 1 levels is only partly effective in reversing advanced arthropathy of acromegaly [ 3 ]  . 
however , the role of gh and igf - 1 on the brous tissue of retinacula , such as the a1 pulley , has only recently been investigated [ 26 ]  . 
measuring the thickdito a scatto il dito a scatto , cio un transitorio blocco del dito in posizione essa , una condizione comune in cui c un ispessimento e una costrizione della parte prossimale dei tendini essori e della loro guaina alla base delle dita o del pollice [ 24 ]  . 
il dito a scatto stato associato anche al diabete mellito , allartrite reumatoide , alla gotta , allinsuf cienza renale con o senza amiloidosi e alla polineuropatia familiare amiloidosica [ 25 ]  . 
la cartilagine ialina e losso sono tipici bersagli di gh e igf - 1 e la normalizzazione di questi valori ormonali non suf ciente a rendere reversibili i segni avanzati dellartropatia acromegalia [ 3 ]  . 
 ecogra a assiale a 12 , 5 mhz a livello della puleggia a1 del terzo dito , ispessita ( frecce )  . radiol med ( 2011 ) 116 : 781792 fig . 
il dito a scatto unaltra frequente e precoce complicanza muscolo - scheletrica dellacromegalia . conclusions conclusioni diffuse peripheral nerve enlargement , carpal tunnel syndrome , cubital tunnel syndrome and trigger nger are the early musculoskeletal complications of acromegaly and represent the features that may be noted by radiologists . 
 lingrandimento diffuso dei nervi periferici , la sindrome del tunnel carpale , la sindrome del tunnel cubitale e il dito a scatto sono le complicanze precoci dellacromegalia che possono essere riconosciute dal radiologo muscolo - scheletrico . 
over the last 4 years , 22 patients ( 14 men and 8 women ; mean age 62.6 years ) affected by 5 acute ( < 14 days ) thrombotic occlusions of the native arteries ( 4 plaque thromboses in the common iliac artery and one on a dissection intimal flap of the external iliac artery ) , 17 subacute and chronic thromboses affecting 4 femoro - popliteal by - pass grafts , 10 stents ( 7 in the common iliac artery and 3 in the superficial femoral artery ) and 3 stents - grafts were studied . 
in the subacute and chronic occlusions , the procedure was completed with percutaneous transluminal angioplasty ( pta ) ( 8 / 22 ) , cutting balloon ( 6 / 22 ) and stenting ( 5 / 22 )  . 
arterial recanalisation with rt is the treatment of choice for acute thrombosis of healthy native arteries ( 47 mm ) ; the treatment of thrombosis complicating calcified plaques or dissection intimal flaps riassunto obiettivo . 
negli ultimi 4 anni sono stati selezionati 22 pazienti ( 14 maschi e 8 femmine ; et media 62 , 6 anni ) portatori di 5 occlusioni trombotiche acute ( < a 14 giorni ) in arteria nativa ( 4 trombosi su placca dellarteria iliaca comune , 1 trombosi su flap di dissezione dellarteria iliaca esterna ) , 17 occlusioni trombotiche subacute e croniche in 4 by - pass femoro - poplitei , 10 stents ( 7 in arteria iliaca comune e 3 in arteria femorale superficiale ) e 3 stents - grafts . 
nelle occlusioni sub - acute e croniche stata associata langioplastica ( pta ) ( 8 / 22 casi ) , cutting ballon ( 6 / 22 ) e stenting ( 5 / 22 )  . 
la ricanalizzazione mediante tr il trattamento di scelta nelle occlusioni trombotiche acute su arteria sana ( 47 mm ) ; il trattamento della trombosi su placca calcifica e su flap di dissezione pu comportare la radiol med ( 2011 ) 116 : 932944 may cause rupture of the arterial wall . 
in subacute and chronic occlusions of by - pass grafts , stents and stent grafts , additional procedures are necessary to achieve complete recanalisation . keywords mechanical thrombectomy rotational thrombectomy thrombotic arterial occlusions rottura della parete arteriosa . 
 parole chiave trombectomia meccanica trombectomia rotazionale occlusioni trombotiche arteriose introduction introduzione acute and subacute thromboembolic occlusions are still a major cause of peripheral ischaemia and limb amputation . conventional treatment includes thrombo - embolectomy with a fogarty thrombectomy catheter and surgical by - pass [ 18 ]  . 
recent years have seen the development of rotational thrombectomy ( rt ) , and many types of devices are available with which to exploit either the vortex principle to fragment the thrombus ( amplatz thrombectomy catheter , angiojet ; arrow - trerotola thrombolysis system ) or the venturi effect to aspirate it ( hydrolyser , thrombektomat ) [ 913 ]  . 
the literature contains reports of experimental studies [ 35 , 14 ] and a few clinical studies [ 6 , 7 , 10 , 11 , 15 ] , all of which have shown promising results . 
la trombectomia rotazionale ( tr ) si sviluppata negli ultimi anni , grazie alla commercializzazione di diversi tipi di device che permettono la frammentazione del trombo sfruttando il vortex principle ( amplatz thrombectomy catheter , angiojet , arrow - trerotola thrombolysis system ) o la sua aspirazione mediante effetto venturi ( hydrolyser , thrombektomat ) [ 913 ]  . 
in letteratura sono attualmente riportati studi sperimentali [ 35 , 14 ] e limitate esperienze cliniche [ 6 , 7 , 10 , 11 , 15 ] che hanno dimostrato promettenti risultati . scopo del nostro lavoro presentare la nostra esperienza nellutilizzo di tale device nel trattamento di occlusioni acute , sub - acute e croniche in vari distretti . 
 materials and methods materiali e metodi between november 2004 and april 2008 , we selected 22 patients ( 14 men and 8 women ; mean age 62.6 years ) affected by 5 acute thrombotic occlusions ( < 14 days ) in native arteries ( 4 thromboses of the common iliac artery , 1 thrombosis of the external iliac artery ) and 17 subacute or chronic occlusions ( > 14 days ) in 4 femoro - popliteal by - pass grafts , 10 stents [ 7 in the common iliac artery and 3 in the superficial femoral artery ( sfa ) ] , 2 femoro - popliteal stentsgrafts and 1 stent - graft in the common iliac artery ( placed to treat aneurysms ) ( table 1 )  . 
the clinical diagnosis was ( us ) and confirmed by colour - doppler ultrasound nel periodo compreso tra novembre 2004 e aprile 2008 sono stati selezionati 22 pazienti ( 14 maschi e 8 femmine ; et media 62 , 6 anni ) portatori di 5 occlusioni trombotiche acute ( < 14 giorni ) in arteria nativa ( 4 trombosi dellarteria iliaca comune , 1 trombosi dellarteria iliaca esterna ) , 17 occlusioni sub - acute o croniche ( > 14 giorni ) in 4 by - pass femoropoplitei , 10 stent ( 7 in arteria iliaca comune e 3 in arteria femorale superficiale ) , 2 stent - graft femoro - poplitei e 1 stentgraft in arteria iliaca comune ( posizionato per aneurisma ) ( tabella 1 )  . 
indications for rt included acute thrombosis in a medium - calibre native artery and subacute or chronic occlusion of by - pass grafts , stents or stent - grafts along the iliac - femoropopliteal arterial axis . 
because the 6 - fr or 8 - fr thrombectomy catheters cannot be used in arteries < 4 mm in calibre , distal trattamento mediante tr nei casi di trombosi acuta su arteria nativa di medio calibro e di occlusione sub - acuta o cronica di bypass , stent o stent - graft lungo lasse arterioso iliacofemoro - politeo . 
il catetere da trombectomia in relazione al calibro ( 6 o 8 fr ) non pu essere utilizzato in arterie di piccolo calibro < a 4 mm , quindi sono state escluse dal trattable 1 rotational thrombectomy with rotarex pt . 
in order to obtain an optimal calibre of the recanalised vessel , in 17 / 22 cases , the procedure was completed by percutaneous transluminal angioplasty ( pta ) , tamento le embolie distali della gamba , con interessamento delle arterie della triforcazione . 
nella nostra esperienza in tutti i casi locclusione stata valicata con filo guida da 0 , 035 idrofilo ( terumo , tokyo , giappone )  . successivamente stato inserito un introduttore vascolare da 8 fr in cross - over , 6 fr o 8 fr in accesso antero - grado ( cordis , johnson & johnson , miami lakes , fl , usa ) mediante catetere da cambio retto da 4 fr ( cordis , johnson & johnson , miami lakes , fl , usa ) con posizionamento , a valle dellocclusione , di una guida da 0 , 018 lunga 260 cm ( terumo , tokyo , giappone )  . 
su tale guida stato fatto scorrere il catetere da tr con un movimento di to - and - fro ( vai e vieni ) lungo locclusione realizzando un lume di ricanalizzazione , mediante spirale metallica rotante ad una velocit di rotazione di 50000 rpm ( rotazioni al minuto )  . 
lazione di tale device ha prodotto la frammentazione del trombo in particelle di circa 100500 m che mediante un vacuum continuo ( > 5 , 8 kpa , 43 mmhg ) sono state aspirate ed eliminate allinterno di una sacca posizionata allestremo prossimale del catetere , con minima perdita di sangue ( < 100 ml / procedura )  . 
a occlusione ( freccia ) ; b trombectomia ; c ricanalizzazione con persistenza delle stenosi alle anastomosi ( frecce ) ; d ricanalizzazione completa delle anastomosi prossimale e distale dopo cutting balloon pta ( frecce )  . 
the recanalisation of occluded stents along the superficial femoral artery ( sfa ) and common iliac artery , in addition to revealing reductions in calibre and stent wall irregularities due to myointimal hyperplasia , showed disease progression in all cases , with stenosis due to an atheromatous plaque both proximal and completata con angioplastica ( pta ) , cutting balloon o stenting . 
la ricanalizzazione degli stents occlusi lungo larteria femorale superficiale e in arteria iliaca comune , oltre ad evidenziare delle riduzioni in calibro con irregolarit delle pareti dello stent da iperplasia miointimale , ha mostrato in tutti i casi una progressione di malattia con stenosi da placca ateromasica a radiol med ( 2011 ) 116 : 932944 fig . 
a langiografia documenta occlusione dello stent - graft ; b trombectomia ( freccia ) ; c ricanalizzazione dello stent - graft con riperfusione della sacca aneurismatica ( frecce ) ; d sotto guida ecografia viene infisso ago ( frecce ) nel contesto della sacca aneurismatica rifornita con iniezione di trombina ; e il controllo documenta ricanalizzazione dello stent - graft e completa esclusione dellaneurisma . 
one of them involved the external iliac artery in a patient in whom a 5 fr vascular introducer had been left in place for several days to monitor intracranial circulation with angiography . 
 sono inoltre state trattate 5 trombosi acute di cui una dellarteria iliaca esterna in una paziente in cui stato lasciato in sede per diversi giorni un introduttore vascolare da 5 fr per controlli angiografici del circolo intra - cranico . rimosso lintroduttore nel sospetto clinico di trombosi acuta 938 radiol med ( 2011 ) 116 : 932944 fig . 
a occlusione dello stent in aic di destra e steno - occlusione dellaic di sinistra in esiti di kissing stenting ; b trombectomia ; c parziale ricanalizzazione , con lume insufficiente ; d kissing balloon pta ; e completa ricanalizzazione degli stents . 
 the follow - up of patients treated with rt for acute thrombosis involved clinical assessment and colour - doppler us at 1 and 3 months and only clinical monitoring thereafter . 
 il follow - up dei pazienti sottoposti a trattamento con tr per trombosi acute stato effettuato inizialmente con valutazione clinica ed eco - color - doppler a 1 e 3 mesi . 
a eco - color doppler ; b dimostrazione angiografica delloccluisone dellaie ; c trombectomia ; d lacerazione dellaie ; e , f trattamento mediante stent - graft ; g tc post - procedura . 
nel caso di occlusioni sub - acute e croniche il follow - up stato eseguito mediante esame clinico ed eco - color doppler a 1 , 3 , 6 e 12 mesi e successivamente annualmente . 
 results in acute occlusions of medium - calibre native arteries ( 4 / 22 cases ) , immediate technical success was achieved with rt and no additional procedures were required . 
in 1 case of acute thrombosis of the external iliac artery , rt produced a vascular lesion that was immediately repaired with a stent grain subacute occlusions of by - pass grafts ( 4 / 17 cases ) , rt was combined with cutting - balloon angioplasty of the anastomotic stenoses . 
in chronic occlusions ( 13 / 17 cases ) of stents and stent - grafts , additional procedures were needed to achieve an optimal lumen size ( 8 / 10 pta ; 2 / 10 cutting balloon ; 3 / 10 stent - in - stent )  . 
in 1 case , rt was not performed because the catheter was unable to cross a thrombotic sfa occlusion in a case of unrecognised fracture of a preexisting stent ; in this case , recanalisation was achieved using cutting - balloon angioplasty and stent - in - stent . risultati nelle occlusioni acute in arteria nativa di medio calibro ( 4 / 22 casi ) stato ottenuto mediante tr un successo tecnico immediato senza procedure aggiuntive . 
in un caso di trombosi acuta in corrispondenzadellarteria iliaca esterna si verificata una lesione vascolare da tr , immediatamente trattata mediante stent - gra nelle occlusioni sub - acute in by - pass ( 4 / 17 casi ) stata la tr stata associata allangioplastica delle stenosi anastomotiche mediante cutting balloon . 
nelle occlusioni croniche ( 13 / 17 casi ) in stents e stent - grafts , per ottenere un lume ottimale , sono state necessarie procedure aggiuntive ( 8 / 10 pta ; 2 / 10 cutting balloon ; 3 / 10 stent in stent )  . 
in the remaining 17 cases of subacute and chronic thrombosis , radiological examinations revealed two stent reocclusions in the sfa at 3 and 12 months , respectively , which were surgically converted into femoro - popliteal by - pass grafts . discussion in recent years , three large prospective randomised studies ( rochester trial , stile trial , and topas trial ) compared intra - arterial fibrinolytic therapy and surgery in the treatment of thrombotic arterial occlusions [ 1618 ]  . 
although comparison of these studies is in part limited by the different protocols and inclusion criteria used ( acute / subacute / chronic ischaemia , thrombotic occlusion / thromboembolic occlusion , proximal / distal occlusions , thromboses of native vessels / bypass grafts , etc . ) , no evidence has emerged indicating the superiority of fibrinolytic therapy over surgery . 
surgical revascularisation is definitely indicated in severe limb ischaemia ( stages iia and iib in the fontaine classification ) , whereas intra - arterial fibrinolysis is a valuable alternative in acute thrombosis ( < 14 days ) with mild to moderate limb ischaemia . 
nei rimanenti 17 casi di trombosi sub - acute e croniche ai controlli radiologici si sono verificate due riocclusioni di stent in afs , rispettivamente a 3 e 12 mesi , convertiti chirurgicamente in by - pass femoropopliteo . 
 discussione negli ultimi anni tre grandi studi prospettici randomizzati ( rochester trial , stile trial e topas trial ) hanno confrontato il trattamento fibrinolitico intrarterioso e la chirurgia nel trattamento delle occlusioni arteriose trombotiche [ 1618 ]  . 
sebbene il confronto tra gli studi citati sia in parte limitato da differenti protocolli e criteri di inclusione nella selezione dei pazienti ( ischemia acuta / subacuta / cronica , occlusione trombotica / occlusione trombo - embolica , occlusioni prossimali / occlusioni distali , trombosi di vasi nativi / trombosi di bypass , ecc . ) , non esiste evidenza di superiorit del trattamento fibrinolitico rispetto a quello chirurgico . 
la rivascolarizzazione chirurgica sicuramente indicata nei casi di severa ischemia dellarto ( classe iia e iib secondo fontaine ) ; al contrario il trattamento fibrinolitico intrarterioso una valida alternativa nei casi di trombosi acuta ( < 14 giorni ) , in presenza di ischemia dellarto di grado lieve - moderato . 
utilizzando questultimo approccio inoltre possibile , mediante langiografia definire con maggiore accuratezza eventuali lesioni stenosanti , possibili responsabili dellevento trombotico acuto , da sottoporre ad un successivo intervento di rivascolarizzazione percutanea o chirurgica [ 1618 ]  . 
 tuttavia la fibrinolisi gravata da un basso ma non trascurabile tasso di complicanze emorragiche ( 1%2% emorragia intracranica ) , che risultano comunque bilanciate come dimostra lo studio rochester da percentuali di mortalit peri - procedurali simili allintervento chirurgico ( 14% fibrinolisi vs 18% chirurgia ) , che al follow - up a 12 mesi tendono a diventare statisticamente significative ( 16% fibrinolisi vs 42% chirurgia ) , poich gravate da un pi alto tasso di complicanze cardio - polmonari ( 16% fibrinolisi vs 49% chirurgia ) [ 16 ]  . 
la tr pu essere considerata una potenziale alternativa alla fibrinolisi loco - regionale ed alla chirurgia per il trattamento delle occlusioni arteriose trombotiche su vasi nativi e su bypass chirurgici . 
in an ischaemic limb , the distal embolisation impairs the microcirculation with persistent or progressive ischaemia , so it is essential that the rt devices cause as little endothelial damage as possible , with rapid thrombus fragmentation and aspiration . 
 compared with fibrinolysis , rt has the advantage of allowing treatment of patients with contraindications to anticoagulation therapy and achieving immediate recanalisation of the occluded segment with prompt resolution of the clinical picture . 
another significant advantage of the new rt catheters ( rotarex ) is the ability to reduce the risk of distal migration of thrombi during the percutaneous procedure , thus significantly lowering the duration of limb ischaemia . on the other hand , rt procedures have the disadvantage of being relatively long and laborious . 
in our experience , the rotarex procedure took 6216 min , its duration being influenced by the extent of thrombosis , device preparation and difficulties in reaching the target site , especially when using a contralateral approach and cross - over technique . 
the rt procedure is complementary to other recanalisation techniques in the case of impassable stenosis or insufficient lumen and in fact cannot be used in arteries < 4 mm in diameter due to catheter calibre ( 6 fr or 8 fr )  . 
the first large series was reported by zeller [ 10 ] , who treated 33 occlusions in native arteries , 58 subacute and chronic utilizzato off - label alcuni di tali device per il trattamento delle occlusioni trombotiche del sistema arterioso periferico . nonostante il differente meccanismo di funzionamento di questi device ( angiojet , amplatz , hydrolyser , oasis ) ed i differenti tassi di perviet primaria ( rispettivamente 61% vs 75% vs 83% vs 11 , 8% ) [ 1922 ] lembolizzazione distale e le lesioni vascolari costituiscono sicuramente le principali complicanze della tr . 
 la tr rispetto alla fibrinolisi ha il vantaggio di poter trattare pazienti con controindicazioni alla terapia anticoagulante e di realizzare unimmediata ricanalizzazione del tratto occluso con pronta risoluzione del quadro clinico . 
altro importante vantaggio dei nuovi cateteri da tr ( rotarex ) la capacit di ridurre il rischio di migrazione distale del trombo durante il trattamento percutaneo , abbassando in modo significativo la durata dellischemia dellarto . 
la durata complessiva della procedura nella nostra esperienza , mediante rotarex di 6216 minuti , appare condizionata dallestensione della trombosi , dai tempi di preparazione del device e dalla difficolt di portare in sede il catetere , specie nel caso di approccio controlaterale in cross - over . 
la procedura di tr complementare ad altre tecniche di ricanalizzazione nei casi di stenosi non valicabili o di lume insufficiente ; infatti non pu essere utilizzata correttamente in arterie con diametro < a 4 mm , in relazione al calibro del catetere ( 6 o 8 fr )  . 
altro importante limite al suo impiego lutilizzo di costosi cateteri monouso da 6 o 8 fr [ circa 2750 euro per catetere rotarex vs 56 , 4 euro per un trattamento fibrinolitico ( 2000000 u / die ) protratto per 72 ore vs 924 , 81002 , 8 euro per terapia fibrinolitica di 72 ore associata a stenting del vaso ] , nonostante la consolle e il motore da tr siano forniti gratuitamente dalla straub . 
 il primo studio clinico che descrive il funzionamento del catetere rotarex quello di schmitt e collaboratori [ 3 ] che hanno dimostrato in fase preliminare , come la tr possa essere tecnica fattibile ed efficace nelle occlusioni trombotiche acute e sub - acute dellarteria femoro - poplitea . 
 [ 6 ] mediante il trattamento di 19 942 radiol med ( 2011 ) 116 : 932944 occlusions in native arteries and 9 by - pass grafts in 98 patients , achieving an immediate technical success rate of 94% , 93% and 78% , respectively , and 18 complications including 1 death ; the other complications were 8 perforations , 7 distal embolisations and 2 amputations . 
the complications reported were 2 reocclusions on day 1 and day 7 , respectively ; 1 haematoma at the access site ; 1 arterio - venous fistula and ten distal embolisations 6 of them significant treated with thromboaspiration . 
 our series was small because we excluded , in agreement with the literature [ 6 , 10 , 12 ] , patients with occlusions on subacute and chronic atheromatous plaques along the iliacfemoral axis and especially along the sfa , as we believe that these occlusions require other recanalisation techniques [ 16 , 17 ]  . 
in these cases , the thrombectomy catheter has a higher risk of perforation , particularly if the plaque is calcified ; in addition , the unrecognised subintimal passage of the angiography wire may cause the thrombectomy catheter to rupture the artery with a risk of arteriovenous fistula and an increased probability inversely proportional to the occluded segment of producing distal embolisation . 
in contrast to previous reports , during the 22 treatments with rt with the rotarex catheter , we had only one case of perforation , which involved a case of acute thrombosis of the external iliac artery in an unrecognised iatrogenic dissection flap caused by an indwelling 5 fr vascular introducer . 
in the case of chronic thrombotic occlusions , an essential precondition for rt is that the guidewire crosses the arterial occlusion , which explains why it is preferable to negotiate long occlusions subintimally and achieve recanalisation with subintimal pta [ 2325 ]  . 
in these cases complete recanalisation was achieved without additional procedures ( pta or stenting ) , which are not , however , unanimously recommended [ 26 ]  . indeed , the technical principle behind angioplasty is to squash the thrombus and spread it along the healthy arterial walls , creating a recanalisation lumen and possible distal migration of the thrombus [ 27 ]  . 
la prima ampia casistica di 98 pazienti quella di zeller [ 10 ] che ha trattato 33 occlusioni in arteria nativa , 58 occlusioni sub - acute e croniche in arterie native e 9 by - pass con un tasso di successo tecnico immediato rispettivamente del 94% , 93% e 78% e 18 complicanze tra cui un decesso ; le altre complicanze riscontrate sono state 8 perforazioni , 7 embolie distali e 2 amputazioni . 
successivamente duc [ 12 ] ha trattato 38 pazienti con trombosi acuta , sub - acuta e cronica dellarteria femorale superficiale con solo 5 procedure aggiuntive , 2 pta e 5 stents , ottenendo un successo tecnico immediato del 100% . 
in questa casistica emergono quali complicanze 2 riocclusioni rispettivamente a 1 e 7 giorni dopo la procedura , 1 ematoma del sito daccesso , 1 fistolaartero venosa ed embolie distali in 10 pazienti di cui 6 rilevanti , trattate con trombo - aspirazione . 
 la nostra casistica esigua in quanto non sono stati selezionati pazienti con occlusioni su placca ateromasica subacuta e cronica lungo lasse iliaco - femorale specie lungo larteria femorale superficiale , come riportato in letteratura , [ 6 , 10 , 12 ] in quanto ormai convinti che questo tipo di occlusioni necessitano di altre tecniche di ricanalizzazione [ 16 , 17 ]  . 
in questi casi il catetere da trombectomia ha un maggior rischio di perforazioni specie su placche calcifiche ; peraltro il passaggio sub - intimale misconosciuto della guida angiografica , pu determinare la fissurazione dellarteria da parte del catetere da trombectomia con il rischio di formazione di fistole artero - venose , nonch la maggiore probabilit , inversamente proporzionale al tratto occluso , di realizzare unembolia distale . 
infatti a differenza dei dati di letteratura durante i 22 trattamenti mediante tr con rotarex nella nostra casistica si verificata una sola perforazione , su trombosi acuta dellarteria iliaca esterna su flap di dissezione iatrogeno misconosciuto , determinato da permanenza in situ di introduttore vascolare da 5 fr . 
nel caso di occlusioni trombotiche croniche , presupposto indispensabile per eseguire la tr che il filo guida valichi locclusione arteriosa ; per tale motivo nei casi di occlusione lunga preferibile valicare locclusione in sede sotto - intimale e realizzare una ricanalizazione mediante pta sub - intimale [ 2325 ]  . 
 i migliori risultati nella nostra serie si sono avuti nel trattamento della tromboembolia su arteria nativa di medio calibro , anche se tale patologia unevenienza abbastanza rara ; in questi casi la ricanalizzazione completa non necessita di procedure aggiuntive ( pta o stenting ) , che peraltro non trovano una indicazione unanime [ 26 ]  . 
infatti il principio tecnico dellangioplastica di schiacciare e spalmare il trombo lungo le pareti arteriose , in questo caso sane , realizzando un lume di ricanalizzazione ed una possibile dislocazione distale del trombo [ 27 ]  . 
this procedure , which is also feasible in patients who have recently undergone surgery or who have contraindications to fibrinolytic therapy , was free of major complications such as vessel perforations and allowed for immediate recanalisation . 
the failure of ultrasound thrombolysis was related to one reocclusion that appeared within only 2 h of the procedure and was subsequently treated with surgery . our series included recanalisation of subacute and chronic occlusions of stents and stent - grafts , an approach that has not been previously reported . 
 conclusions nei casi di ricanalizzazione di by - pass femoro - popliteo , la tr ha immediatamente evidenziato la causa delle stenosi anastomotiche serrate , che viste le caratteristiche morfologiche ( brevi - sub - occludenti da iperplasia miointimale ) abbiamo preferito trattare con cutting balloon ( boston scientific , natick , ma , usa )  . 
tale procedura attuabile anche in pazienti operati di recente o con controindicazioni alla terapia fibrinolitica , risultata priva di complicanze maggiori come la perforazione del vaso , consentendo unimmediata ricanalizzazione vascolare . 
 [ 26 ] hanno trattato 20 pazienti con occlusione acuta di by - pass femoro - popliteo comparando il successo tecnico tra 10 casi di trombectomia mediante catetere rotarex ( tempo medio di 64 , 5 minuti ) e la trombolisi mediante ultrasuoni nei rimanenti 10 casi , con un tempo medio di 904 minuti ; il successo tecnico privo di complicanze peri - procedurali stato del 100% per la tr e del 90% per la lisi ad ultrasuoni . 
 nella nostra casistica abbiamo incluso la ricanalizzazione delle occlusioni sub - acute e croniche di stents e stent - graft ; questo tipo di approccio non viene menzionato in letteratura . 
la ricanalizzazione di stents e stent - graft mediante tr permette unimmediata ricanalizzazione del lume vasale ; in questo caso le maglie stesse dello stent evitano la perforazione della parete arteriosa . 
 technical and clinical success and recanalisation with rt proved to be a valuable alternative to surgery in the treatment of acute thrombotic occlusions in medium - sized native arteries and in sub - acute and chronic occlusions of by - pass grafts , stents and stentgrafts , as the technique is able to restore patency with immediate morbidity rates , thanks to its minimal invasiveness . 
the treatment of subacute and chronic thrombosis in mediumsized native arteries , especially those affected by calcified atheromatous plaques , may lead to rupture of the arterial wall due to the possible subintimal passage of the guidewire . 
because arterial rupture may also occur in acute thromboses secondary to traumatic or iatrogenic conditions due to occluding flaps , rt should not be regarded as the treatment of choice in these cases . rt could become a complementary technique to surgery in the near future . 
on the basis of correct preprocedural planning , the vascular radiologist will be able to choose the most suitable technique according to the location , length and type of thrombosis to be treated , thus minimising complication rates . 
 conclusioni la ricanalizzazione mediante tr si rivelata una valida alternativa terapeutica alla chirurgia nel trattamento delle occlusioni trombotiche acute su arteria nativa di medio calibro e nelle occlusioni sub - acute e croniche di by - pass , stent e stentgraft , in quanto realizza il ripristino della perviet con successo tecnico - clinico immediato e bassi tassi di morbilit legati ad un approccio mininvasivo . 
il trattamento delle trombosi sub - acute e croniche su arteria nativa di medio calibro specie su placca ateromasica calcifica pu comportare la rottura della parete arteriosa per il possibile passaggio sottointimale del filo guida . 
mediante un corretto planning pre - procedurale il radiologo vascolare potr scegliere la tecnica interventistica pi adeguata in relazione alla localizzazione , lunghezza e tipo di trombosi da trattare , riducendo al minimo il tasso di complicanze . 
cardarelli , naples , italy 3department of pathology , maresca hospital , naples , italy 4cytopathology service , section of pathology , department of surgery , national cancer centre , fondazione g . 
although computed tomography ( ct ) is still the gold standard for acute intestinal disorders , over the last few years , magnetic resonance imaging ( mri ) has become a useful alternative tool . 
sebbene attualmente la tomogra a computerizzata ( tc ) rimane la metodica di scelta nelle patologie intestinali acute , negli ultimi anni la risonanza magnetica ( rm ) si proposta come valida alternativa . 
il modello documenta la corretta sequenza degli eventi dellischemia mesenterica arteriosa acuta 830 radiol med ( 2011 ) 116 : 829841 keywords experimental model acute bowel ischaemia micro - mri pathology ( imaa ) e dimostra che la rm pu essere proposta per la sua diagnosi precoce . 
this condition is characterised by sudden occlusion of the superior mesenteric artery ( sma ) and / or inferior mesenteric artery ( ima ) , followed impaired vascular supply to the bowel region [ 1 , 2 ]  . 
this goal , however , is still far from achieved , due to the nonspeci c clinical / laboratory ndings and to the absence of speci c and early radiological ndings typical of ami [ 810 ]  . 
magnetic resonance imaging ( mri ) , on the contrary , is less frequently employed in these patients because of its limited availability , high costs and motion artefacts , which have prevented its use in the diagnostic workup of acute intestinal diseases for several years [ 11 ]  . 
 based on these considerations , a novel animal model of acute intestinal ischaemia was developed with the aim of assessing the effectiveness of 7 - t micro - mri in early diagnosis and to document the correct temporal evolution of these lesions . materials and methods animals the study was conducted on 30 sprague dawley rats weighing 400 g on average , which were randomly assigned to two experimental groups ( 1 and 2 )  . 
questa condizione caratterizzata da unimprovvisa occlusione dellarteria mesenterica superiore ( ams ) e / o inferiore ( ami ) seguita da una compromissione dellapporto vascolare nel distretto intestinale [ 1 , 2 ]  . 
nonostante i progressi raggiunti nelle ultime decadi nellambito della chirurgia e della terapia intensiva , il tasso di mortalit correlato a questa patologia rimane elevato , no a s orare l80% [ 36 ]  . 
questo risultato rimane tuttavia lontano per la presentazione clinica e laboratoristica aspeci ca e per lassenza di reperti radiologici speci ci e precoci di ima [ 8 10 ]  . 
la risonanza magnetica ( rm ) , al contrario , meno utilizzata nella gestione del paziente con patologia addominale acuta , per la sua limitata disponibilit , per i costi elevati e per artefatti da movimento che ne hanno precluso per anni limpiego nelliter diagnostico della patologia intestinale acuta [ 11 ]  . 
 le pi recenti apparecchiature di rm presentano incrementata velocit di acquisizione delle immagini , unaumentata capacit di contrasto per i tessuti molli e maggiore diffusione sul territorio [ 12 ]  . 
sulla base di queste considerazioni stato utilizzato un innovativo modello animale di ischemia intestinale acuta con lo scopo di valutare sia lef cacia della micro - rm a 7 t nella diagnosi precoce sia di documentare la corretta cronologia delle lesioni . materiali e metodi animali lo studio stato condotto su 30 ratti sprague dawley del peso medio di 400 g , assegnati casualmente a due gruppi sperimentali ( gruppo 1 , gruppo 2 )  . 
their body temperatures were tracked using rectal probes and kept at 370.5c. surgical model each rat was studied to analyse lesions secondary to acute arterial mesenteric ischaemia ( arterial ami ) after occlusion of the sma . 
in group 1 ( n = 15 ) , the sma was occluded by laparotomy in a single surgical session and the macroscopic lesions were documented photographically ( nikon coolpix s210 , 8.0 megapixel , iso 2000 ) during the following hours . 
 at time zero ( immediately before sma ligation ) , a rst photograph was taken of the exposed abdominal organs ( jejunum to colon ) to conduct a preliminary morphological evaluation of the bowel loops that would later serve as a control image for the same animal . 
in particular , in three animals , observation was limited to the rst 4 h , and at the end of the test , the intestinal packet was removed for histopathological characterisation of the injury . 
in three other animals , observation lasted 6 h , whereas in the remaining nine , observation was extended to 8 h , followed by resection of the intestinal packet for histological analysis . 
in group 2 ( n = 15 ) , arterial ami was induced over two surgical session approximately 3 days apart , and the lesions were evaluated using 7 - t micro - mr imaging . 
a 3 / 0 silk thread was placed around the origin of the vessel to obtain a loop whose ends were inserted into a silicone tube and later tunnelled subcutaneously from the abdominal cavity to the dorsal cervical region , where the thread ends were secured . 
three days after the rst surgical session , the rats were anaesthetised again with the same protocol , and arterial ami was reproduced by pulling the ends of the thread protruding from the silicone tube . 
the interval of approximately 3 days between the two surgical sessions was suf cient to suppress artefacts due to abdominal free air and manipulation of intestinal loops immediately prior to the operation . 
 7 - t micro - mri each rat in group 2 underwent mri of the abdomen using a 7 - t micro - mri scanner ( biospec 70 / 16us , bruker medical systems , ettlingen , germany )  . 
la temperatura corporea stata monitorata tramite sonda rettale e mantenuta a 370 , 5c . modello chirurgico ciascun ratto stato studiato per analizzare le lesioni conseguenti ad ischemia mesenterica arteriosa acuta ( imaa ) dopo occlusione della ams . 
nei ratti del gruppo 1 ( n = 15 ) lams stata occlusa per via laparotomica in ununica seduta operatoria e nelle successive ore le lesioni macroscopiche sono state documentate con immagini fotogra che ottenute mediante apparecchio nikon coolpix s210 , 8.0 megapixels , iso 2000 . 
al tempo zero ( subito prima della legatura dellams ) , stata acquisita per ciascun ratto una prima immagine fotogra ca degli organi esposti allesterno della cavit addominale ( tratto compreso tra digiuno e colon ) con la nalit di effettuare una valutazione preliminare morfologica delle anse intestinali , da utilizzare poi come immagine di controllo per lo stesso animale . 
in altri 3 animali losservazione stata protratta sino a 6 ore , mentre nei restanti 9 animali losservazione stata estesa no ad 8 ore , con successiva resezione del pacchetto intestinale per lanalisi istologica . 
nel gruppo 2 ( n = 15 ) limaa stata indotta facendo ricorso a due sedute operatorie ad una distanza di tempo di circa 3 giorni luna dallaltra e le lesioni sono state valutate con limaging micro - rm a 7 t . 
un lo di seta 3 / 0 stato posizionato attorno allorigine del vaso in modo da confezionare un cappio le cui estremit sono state inserite in un tubicino di silicone , successivamente tunnelizzato dalla cavit addominale alla regione cervicale dorsale per via sottocutanea . 
dopo 3 giorni dalla prima seduta operatoria , i ratti sono stati nuovamente anestetizzati , seguendo lo stesso protocollo anestesiologico del precedente intervento , e limaa stata riprodotta ponendo in trazione le estremit del lo che fuoriuscivano dal tubicino di sili832 radiol med ( 2011 ) 116 : 829841 characterise any signs of intestinal ischaemia and compare ndings with histological evaluation . 
immediately before inducing infarction , the animals underwent a 7 - t micromri scan for preliminary morphological and functional evaluation of the intestinal loops , which would later serve as a control image for the animal . 
in particular , after a scout view in the three orthogonal planes ( tr 200.0 ms , te 5.0 ms ) , images of the entire abdomen were acquired using an axial t2 - weighted rapid acquisition relation enhancement ( rare ) sequence ( tr 6 , 030.3 ms , te 36 ms 180 ip angle ; 52 slices ; slice thickness 1 mm , interslice distance 1 mm , eld of view 6 cm ; acquisition matrix 256256 )  . 
the same sequence was then used to evaluate the damage in the immediate postischaemic period , 5 min after ligation , and at intervals of 30 min until the end of the observation period . 
 under baseline conditions and 5 min after the sma occlusion , an additional 2d fast low - angle shot time of ight ( flash - tof ) sequence ( tr 12 ms , te 3.5 ms ; 90 ip angle ; 180 slices ; slice thickness 0.4 mm , interslice distance 0.25 mm , eld of view 6 cm ; acquisition matrix 256256 ) was obtained rst to visualise the vascular anatomy then to con rm complete vessel occlusion after a maximum intensity projection ( mip ) reconstruction . 
for group 2 ( n = 15 ) , the scans were repeated up to 4 h after vascular occlusion in three animals , after 6 h in other three and after 8 h in the remaining nine . 
special care was taken in evaluating the mean diameter of the lumen of bowel loops , wall thickness , air uid levels in the affected loops and free uid in the abdomen . at the end of the session , the intestinal packet was removed for histopathological characterisation of the injury and the animal was euthanised as described above ( 0.5 ml tanex administered via the lung )  . histological evaluation pathological characterisation of damage was conducted on all animals in both groups at prede ned time points ( 4 , 6 and 8 h )  . 
for all specimens , the intestinal tract between jejunum and ascending colon was resected before euthanasia and , after being xed in a solution of 10% formalin - acetate for at least 5 days , it was processed for histopathological evaluation . 
conventionally , specimens taken are divided into four portions , each including : ( 1 ) jejunum and the rst 10 cm of the ileum ( rst segment 1s ) ; ( 2 ) central ileal ( second segment 2s ) ; ( 3 ) last 10 cm of ileum ( third segment 3s ) ; ( 4 ) caecum and ascending colon ( fourth segment 4s )  . 
il rispetto di un intervallo di tempo di circa 3 giorni tra le due sedute operatorie risultato suf ciente per abolire gli artefatti dovuti alla presenza di aria libera in addome ed alla manipolazione delle anse nellimmediato periodo postoperatorio . 
 micro - rm a 7 t ciascun ratto appartenente al gruppo2 stato sottoposto a rm delladdome utilizzando un apparecchio micro rm a 7 t ( biospec 70 / 16us , bruker medical systems , ettlingen , germania )  . 
tale metodica veniva utilizzata al ne di confermare lassenza di usso attraverso lams , di identi care e caratterizzare i segni di ischemia intestinale e di comparare questi reperti con lanalisi istologica . 
subito prima di indurre linfarto , gli animali sono stati sottoposti ad una prima scansione micro - rm a 7 t con la nalit di effettuare una valutazione preliminare morfologica e funzionale delle anse intestinali da utilizzare poi come immagine di controllo per lo stesso animale . 
in particolare , dopo una scout view nei tre piani ortogonali ( tempo di ripetizione [ tr ] = 200 , 0 ms , tempo di eco [ te ] = 5 , 0 ms ) , le immagini dellintero addome venivano acquisite mediante una sequenza rapid acquisition with relaxation enhancement ( rare ) t2 in sezione assiale ( tr = 6030 , 3 ms , te = 36 ms ; ip angle 180 ; 52 slices ; slice thickness 1 mm , interslice distance 1 mm , eld of view 6 cm ; acquisition matrix 256256 )  . 
la stessa sequenza veniva poi utilizzata per la valutazione del danno nellimmediato post - ischemico , 5 minuti dopo la legatura , e ad intervalli di 30 minuti no alla ne del periodo di studio . 
in condizioni basali e a 5 minuti dallocclusione dellams una sequenza aggiuntiva fast low angle shot ( flash ) - 2d - time - ofight ( tof ) ( tr = 12 ms , te = 3 , 5 ms ; ip angle 90 ; 180 slices ; slice thickness 0 , 4 mm , interslice distance 0 , 25 mm , eld of view 6 cm ; acquisition matrix 256256 ) veniva effettuata al ne di visualizzare lanatomia vascolare prima e di confermare successivamente locclusione completa del vaso , dopo ricostruzione in maximum intensity projection ( mip )  . 
 anche per questo secondo gruppo sperimentale ( n = 15 ) , le scansioni venivano ripetute sino a 4 ore dalleffettiva occlusione vascolare in 3 animali , 6 ore in altri 3 ratti , ed 8 ore nei restanti 9 animali . 
particolare attenzione veniva posta nella valutazione del diametro medio del lume delle anse intestinali , dello spessore parietale , nellidenti cazione di livelli idro - aerei nelle anse colpite e di versamento libero in addome . al termine della seduta , il pacchetto intestinale veniva rimosso per la caratterizzazione istopatologica del danno e lanimale sottoposto ad eutanasia come precedentemente indicato ( tanex 0 , 5 ml per via intrapolmonare )  . radiol med ( 2011 ) 116 : 829841 from each paraf n block and stained with hematoxilin and eoxin ( h&e )  . 
histopathological evaluation was conducted using a zeiss axioskop 2 light microscope ( zeiss ) equipped with a high - resolution digital microcamera ( c4742 - 95 , hamamatsu photonics , milan , italy )  . 
the ileal loops underwent the same pathological evolution , but the spasm was observed about 1 h after arterial occlusion , with transition to de nite analisi istologica la caratterizzazione anatomopatologica del danno stata effettuata su tutti gli animali del gruppo 1 e del gruppo 2 ai time - point stabiliti ( 4 , 6 e 8 ore )  . 
per tutti i campioni il tratto di intestino compreso tra digiuno e colon ascendente stato resecato prima di procedere alleutanasia e , dopo ssazione per almeno 5 giorni in una soluzione di acetato di formalina al 10% , stato processato per lanalisi istopatologica . 
convenzionalmente , i campioni prelevati sono stati suddivisi in quattro porzioni , ciascuna includendo rispettivamente : ( 1 ) digiuno e i primi 10 cm di ileo ( primo segmento 1s ) ; ( 2 ) segmento centrale di ileo ( secondo segmento 2s ) ; ( 3 ) ultimi 10 cm di ileo ( terzo segmento 3s ) ; ( 4 ) intestino cieco e colon ascendente ( quarto segmento 4s )  . 
per ciascuna di queste regioni di intestino sono state realizzate ed incluse in paraf na delle sezioni trasversali di 3 mm di spessore , a distanza di 10 mm luna dallaltra . 
grazie allausilio di un microtomo , fettine dello spessore di 3 micron sono state effettuate su ciascun blocco di paraf na e successivamente sottoposte a colorazione con ematossilina eosina ( e&e )  . 
spasmo delle anse digiunali a 30 minuti ( freccia in b ) che si protraeva no a 3 ore , per transitare da questo momento in poi in ipotono ( c )  . 
in b aspetto dopo 8 ore di osservazione : mesentere pallido con assottigliamento dei vasi mesenterici ( che esordiva gi a 5 minuti dalla legatura ) ; viraggio cromatico verso il rosso vinaccia della parete intestinale digiuno - ileale . ; ileo ri esso ipotonico diffuso a tutto il tratto di intestino mesenteriale . hypotonia after about 4 h . 
immediately before inducing radiol med ( 2011 ) 116 : 829841 skope 2 light ( zeiss ) , dotato di fotomicrocamera digitale ad alta risoluzione ( c4742 - 95 , hamamatsu photonics , milano , italia )  . 
le anse dellileo hanno presentato la stessa evoluzione patologica , ma lo spasmo stato osservato a circa 1 ora dallocclusione arteriosa con il passaggio a circa 4 ore in ipotono franco . 
subito prima dellinduzione di imaa , 3 giorni dopo lintervento chirurgico in laparotomia , non stata evidenziata la presenza di gas libero nella cavit addominale n segni di irritazione viscerale o mesenterica . 
3a , b maximum intensity projection reconstruction of the vascular tree with identi cation of the superior mesenteric vein ( smv ) and artery ( sma ) a before occlusion ( 2d - fast low - angle shot time of ight )  . 
3a , b ricostruzione mip dellalbero vascolare con identi cazione della vena mesenterica superiore ( smv ) e dellarteria mesenterica superiore ( sma ) prima dellocclusione ( flash 2d - tof ) ( a )  . 
a baseline t2 ; b 2 h after ligation : dilatation of some loops with thinned bowel walls ( region of interest ) ( re ex hypotonic ileus )  . 
in a aspetto basale in t2 ; in b aspetto a 2 ore dalla legatura , dove appare una dilatazione di alcune anse intestinali con assottigliamento della parete delle stesse ( ileo ri esso ipotonico )  . 
alla dilatazione hanno fatto seguito i livelli idro - arei , ben evidenti a 4 ore dalla legatura dellams e uniperintensit della parete delle anse coinvolte ( c )  . 
b increasing free intraperitoneal uid : a small amount of free uid between the loops appeared only 30 min after superior mesenteric vein ( sma ) ligation ( arrows )  . 
il liquido andava crescendo , divenendo meglio apprezzabile dopo 4 ore ( c ) e diffuso in tutto laddome dopo 8 ore ( d )  . arterial ami , 3 days after laparotomic surgery , no free gas within the abdominal cavity nor signs of visceral or mesentery irritation were found . 
 wall damage was more eivdent in the last ileal segment ( 3s ) , where the initial formation of a grunhagen subepithelial space was reported ( chiu 2 )  . the three specimens removed 6 h after sma ligation showed a clear re ex hypotonic ileus , with signi cant dilatation of some loops . 
the mucosa showed discontinuous alterations , with apparently healthy areas alternating with areas undergoing necrobiotic phenomena and regenerative compensatory hyperplasia at the bases of the glandular crypts ( skip lesions )  . 
these ndings were almost identical in the specimens obtained from the two test groups and at different time points . discussion imaging ndings of ami are nonspeci c and heterogeneous , as are aetiology and clinical and laboratory signs [ 14 ]  . 
the diagnostic hypothesis is not considered at all or is considered late for two reasons : first , ami in humans is not always either complete or at the emergence of the vascular axis ; therefore , the pain appears after different time periods in every patient . 
second , every patient presents to the emergency department at different time lines , depending on accessibility of the facility . the radiological approach to diagnosing ami relies on contrast - enhanced ct , which detects morphological changes suggestive of the condition . 
the advantages of mri over ct include higher contrast resolution in soft tissues and no risks from ionising radiation or of nephropathy induced by iodinated infartuali era evidenziata dal viraggio cromatico della sierosa intestinale , variabile dal rosso vinaccia al nero antracite . 
la stessa mostrava alterazioni discontinue , alternando zone di mucosa apparentemente orida con zone in preda a fenomeni necrobiotici ed iperplasia compensatoria rigenerativa della base delle criptae ghiandolari ( skip lesions )  . 
nella regione 3s , in ne , la mucosa appariva francamente sempli cata , oltre a presentare reperti sovrapponibili a quelli gi descritti per la regione 2s ( grado chiu 4 - 5 )  . 
i reperti erano pressoch sovrapponili fra i campioni appartenenti ai due gruppi sperimentali e ai diversi time point . discussione i reperti allimaging di ima sono aspeci ci ed eterogenei , cos come leziologia , i segni clinici e laboratoristici [ 14 ]  . 
il primo perch lima nelluomo non sempre n completa , n allemergenza dellasse vascolare , e per questo la sintomatologia dolorosa si rende manifesta con un intervallo di tempo diverso in ogni paziente . 
 il secondo perch ogni paziente si reca al pronto soccorso dopo che trascorso un intervallo di tempo diverso , condizionato dalla accessibilit della struttura . lapproccio radiologico attuale per la diagnosi di ima basato sul riscontro tc dopo somministrazione di mezzo di contrasto ( mdc ) endovena ( ev ) delle modi cazioni morfologiche suggestive di tale patologia . 
i vantaggi della rm rispetto alla tc includono una maggiore risoluzione di contrasto per i tessuti molli e lassenza di rischio da radiazioni ionizzanti o di nefropatie indotte da mezzi di contrasto iodati . 
lindagine tc mantiene una risoluzione spaziale superiore , ma questa differenza si va riducendo grazie allintroduzione di nuove sequenze per la rm addominale con voxel dellordine di 2 mm per apparecchiature da 1 , 5 t e di 1 mm per apparecchiature da 3 t [ 12 , 15 ]  . 
the ct scan still has a higher spatial resolution , but the difference is becoming less evident with the introduction of new abdominal mri sequences with voxels in the order of 2 mm for 1.5 - t scanners and of 1 mm for 3 - t scanners [ 12 , 15 ]  . 
 our experience is the rst in which 7 - t micro - mri sequences in rats with arterial ami due to sma occlusion were evaluated to establish the typical ndings of the condition and their evolution . 
the micro - mri study method and other diagnostic imaging techniques for small animals are emerging as key techniques in in vivo molecular imaging , given their ability to identify events with suf cient sensitivity , speci city and temporal and spatial resolution . 
in our study , we observed that wall thickening was absent from arterial ami and that the small - bowel loops appeared , on the contrary , extremely thin , resembling sheets of paper , an appearance that has an incidence of 5% in the literature [ 18 ]  . 
its low incidence rate , as well as the reported wide variability of wall thickening in literature reports , are conditioned by the different number of cases with arterial or venous infarctions in their mixed series . 
wall thickening is caused by intramural oedema and / or haemorrhage and / or by superinfection of the ischaemic bowel wall events that are not found in arterial ami [ 25 , 26 ]  . 
 seven - tesla micro - mr imaging never detected oedema of the mesentery , even though neither thinning vascular structures , nor gradual exsanguination of the mesentery could be observed . 
the authors argue that the ct nding described in the literature only applies to infarctions of venous orig the third most frequent nding reported in the literature ( 65% of cases ) is dilatation of bowel loops with air uid levels [ 1924 ]  . 
the la nostra esperienza la prima nella quale sequenze micro - rm a 7 t in ratti con imaa da occlusione dellams sono state analizzate per stabilire quali siano i reperti distintivi della patologia e la loro cronologia . 
la modalit di studio micro - rm , insieme ad altre metodiche di diagnostica per immagini per piccoli animali , stanno emergendo come tecniche chiave nellimaging molecolare in vivo grazie alla possibilit di individuare eventi con suf ciente sensibilit , speci cit , risoluzione temporale e spaziale . 
nel nostro studio abbiamo osservato che lispessimento parietale assente nellimaa e le anse del piccolo intestino si presentano viceversa estremamente assottigliate con aspetto a foglio di carta , che in letteratura descritto con incidenza pari a 5% [ 18 ]  . 
la sua bassa percentuale di incidenza , cos come lampia variabilit riportata per lispessimento parietale , nei contributi presenti in letteratura , sono condizionate dal diverso numero di casi di pazienti con infarto arterioso o venoso nelle loro casistiche miste . 
lispessimento parietale dovuto alledema intramurale e / o allemorragia e / o alla superinfezione della parete intestinale ischemica , che sono assenti in caso di imaa [ 25 , 26 ]  . 
alla micro - rm a 7 t non veniva mai riscontrato edema del mesentere , pur non essendo stato possibile evidenziare lassottigliamento delle strutture vascolari n il progressivo dissanguamento del mesentere . 
 840 radiol med ( 2011 ) 116 : 829841 ileal loops followed the same pattern , but the spasm was observed at around 1 h and hypotonia at 4 h . 
some authors report ascitis in 4988% of cases [ 22 , 23 ] ; others view it as a late nding emerging only after 12 h [ 28 ]  . 
in our experience , using 7 - t micro - mri , we observed a thin amount of uid between the bowel loops after just 30 min , which grew gradually and became more evident after 4 h , extending to the entire abdomen after 8 h . seven - tesla micro - mri without intravenously administered contrast medium revealed hyperintensity of the loops affected by the ischaemic insult after 3 h . 
these observations are in line with reports by other authors [ 29 ] , who believe that unenhanced t2 - weighted mri sequences , conducted ex vivo , are useful in identifying wall hyperintensity of acute intestinal ischaemia , differentiating it from subacute forms . 
our experience con rms the late presentation of this nding , because we observed it in only one rat after 8 h . finally , in arterial ami due to sma occlusion , the earliest ndings are blanching of the mesentery and re ex spastic ileus , which appear at 5 and 15 min , respectively , from onset of the ischaemic insult . 
mri is the most sensitive modality for early diagnosis of arterial ami due to sma occlusion , as it is capable of detecting the ischaemic loop after only 4 h . con ict of interest none lo spasmo una reazione precoce e transitoria allinsulto ischemico delle pliche semilunari che , in anse sottili a foglio di carta , determinano il collasso del lume . 
la micro - rm a 7 t consentiva di documentare lileo ri esso ipotonico , la dilatazione del lume e , dopo 4 ore , i crescenti livelli idro - aerei . 
nella nostra esperienza abbiamo osservato alla micro - rm a 7 t un reperto di sottile falda di liquido tra le anse dopo appena 30 minuti , che andava crescendo divenendo meglio apprezzabile dopo 4 ore e diffuso in tutto laddome dopo 8 ore . 
queste osservazioni sono in accordo con la segnalazione di altri autori [ 29 ] secondo i quali le sequenze rm t2 - pesate senza mdc ev , condotte ex vivo , sono utili per identi care liperintensit parietale dellischemia intestinale acuta distinguendola dalle forme subacute . 
la nostra esperienza conferma la presentazione tardiva di tale reperto essendo stata riscontrata in un solo ratto ad 8 ore . in conclusione , nellimaa da occlusione dellams i reperti pi precoci sono limpallidimento del mesentere e lileo ri esso spastico che esordiscono rispettivamente a 5 e 15 minuti dallinstaurarsi dellinsulto ischemico . 
scaglione3 1dipartimento di diagnostica per immagini , universit degli studi di foggia , azienda ospedaliero - universitaria ospedali riuniti , viale luigi pinto 1 , 71100 foggia , italy 2u.o. 
radiologia muscoloscheletrica , irccs ospedale casa sollievo della sofferenza , viale cappuccini 1 , 71013 san giovanni rotondo ( fg ) , italy 3dipartimento di diagnostica per immagini , presidio ospedaliero pineta grande , via domiziana k30 , 81030 castel volturno ( ce ) , italy 4sezione dipartimentale di medicina legale , universit degli sudi di foggia , ospedale colonnello davanzo , via degli aviatori 1 , 71100 foggia , italy correspondence to : g . 
the aim of this study was to evaluate the impact of conventional radiology on the assessment of causes of death of human beings after a building collapse and to establish whether the radiographic approach is useful and justi able . 
scopo del lavoro stato quello di valutare limpatto della radiologia tradizionale nellaccertamento delle cause del decesso di persone a seguito di un crollo di un edi cio abitativo e stabilire in che termini lapproccio radiogra co stato utile e giusti cabile . 
 nei 3 pazienti del gruppo ii la morte sopraggiunta a causa di as ssia meccanica associata a lesioni cerebrali in tutti i casi , a lesioni addominali in 2 casi e a lesioni cardiache in un caso . 
in questo gruppo di pazienti , i reperti radiogra ci hanno consentito di apprezzare segni di frattura a carico della teca cranica in un caso , aria nelle camere cardiache in un altro e lesione del diaframma in un terzo . 
nei 2 pazienti del gruppo iii sono state evidenziate al tavolo autoptico lesioni incompatibili con la vita a livello cardiaco e addominale in entrambi i casi ed 970 radiol med ( 2011 ) 116 : 969981 victims . 
conventional radiography should be considered inadequate , especially if the potential of the modern software tools available on current computed tomography and magnetic resonance images is considered . keywords plain x - ray radiographs building collapse autopsy ndings noninvasive autopsy forensic pathology postmortem imaging encefalico in uno . 
lapproccio radiogra co tradizionale per laccertamento delle morti di tali pazienti da considerarsi insuf ciente , specie alla luce delle potenzialit dei moderni software collegati alle attuali apparecchiature di tomogra a computerizzata ( tc ) e risonanza magnetica ( rm )  . 
 parole chiave radiologia tradizionale crollo edi cio reperti autoptici autopsia non - invasiva patologia forense post - mortem imaging introduction introduzione collapse of a residential building is an uncommon event resulting from numerous causes ( earthquakes , hurricanes , oods , snow slides , explosions , terrorist attacks , structural failures , design errors , inadequate materials or soil ) [ 1 , 2 ]  . 
buildings such as this , which in part extend below street level and are locally known as the caves , were originally meant for warehousing food and later used as dwellings despite the unsatisfactory hygienic , lighting and ventilation conditions . 
its potential improved markedly as a result of the technological advances of the past 20 years [ ultrasound ( us ) , computed tomography ( ct ) and magnetic resonance ( mr ) technology ] , whereas the objectives remained essentially unchanged : identifying the victim , recording and ascertaining the cause il crollo di un edi cio abitativo un evento raro e riconosce molteplici cause ( terremoti , uragani , allagamenti , slavine , esplosioni , attentati terroristici , insuf cienze strutturali , errori progettuali , inadeguatezza dei materiali o del suolo ) [ 1 , 2 ]  . 
abitazioni come questa , che si sviluppano in parte al di sotto del livello stradale e per questo chiamate cave , erano , in origine , adibite al semplice deposito per la conservazione di alimenti e poi , successivamente , destinate a scopo abitativo nonostante le precarie condizioni igieniche , di esposizione alla luce e alla ventilazione . 
le sue possibilit sono migliorate notevolmente in relazione radiol med ( 2011 ) 116 : 969981 allevoluzione tecnologica che la radiologia ha subito nellultimo ventennio ( tecniche ecogra che , di tomogra a computerizzata e di risonanza magnetica ) , pur restando gli obiettivi principali essenzialmente gli stessi : identi cazione , documentazione e accertamento della causa di morte dei soggetti , ricostruzione dellevento , in formazione e ricerca [ 4 ]  . 
the purpose of this paper was to illustrate the type and frequency of injuries compatible with life , to assess the impact of conventional radiology in ascertaining the cause of death in these victims and to evaluate whether radiography was useful and justi able as a procedure for forensic ascertainment of the causes of death . materials and methods at the time of the catastrophe , the cave was occupied by 14 persons . 
le indagini radiogra che sono state effettuate con apparecchio digitale telecomandato ( opera t90 e , general medical merate spa , seriate , bergamo , italia ) su tutti i distretti corporei e in almeno due proiezioni . 
laddove le lesioni scheletriche erano gi deducibili dallesame obiettivo ( presenza di escoriazioni , ecchimosi o deformit corporee ) e / o nelle proiezioni radiogra che ortogonali si provveduto ad integrare le stesse con ulteriori dettagli , se necessario , per laccertamento della causa di morte . 
radiographs were obtained of all body regions and in at least two projections using remotecontrolled digital equipment ( opera t90 and general medical merate spa , seriate , bg , italy )  . 
when skeletal lesions were noted on physical examination ( presence of excoriations , bruises or physical deformities ) and / or on the radiographic orthogonal views , more detailed information was sought whenever needed for identifying the cause of death . 
the niss is an evolution of the iss and provides a value deriving from the sum of the squares of the three highest scores of the lesions detected , regardless of the anatomical region involved . 
these values were completed classi cati e codi cati utilizzando il punteggio in riferimento allabbreviated injury scale ( ais ) ed il valore del suo derivato new injury severity score ( niss ) [ 68 ]  . 
il niss rappresenta levoluzione delliss e fornisce un numero che deriva della somma dei quadrati dei tre punteggi pi elevati delle lesioni rilevate , indipendentemente dalla regione anatomica di interesse . 
autopsy ndings were compared with radiographic ndings . results to moderate twentyve percent of victims sustained brain , thoracic and abdominal lesions not compatible with life ( niss = 76 ) , whereas 37.5% suffered mild lesions ( niss < 25 )  . 
the chest was the most frequently involved anatomical region ( 32% ) , followed by the head and neck ( 28% ) , the skin ( 22% ) and the abdomen ( 21% )  . 
lesions of the appendicular skeleton were detected in 7% of cases , with a prevalence of femoral - shaft fractures ( 62.5% ) followed by pelvic , humeral and radial lesions . 
il torace stata la regione implicata nel danno ( 32% ) , corporea maggiormente seguita dai distretti testa - collo ( 28% ) , dalla cute ( 22% ) e dalladdome ( 21% )  . 
le lesioni allo scheletro appendicolare sono state rinvenute nel 7% dei casi , con prevalenza delle lesioni della dia si femorale ( 62 , 5% ) seguite dalle lesioni del bacino , dellomero e del radio . 
 i reperti radiogra ci hanno mostrato fratture costali , pneu976 radiol med ( 2011 ) 116 : 969981 classi ed according to the corresponding niss values are reported in table 1 . 
group 3 , which consisted of two cadavers , had the most severe lesions , with an niss score of 76 , a value associated with lesions not compatible with survival , such as myocardial infarction and laceration associated with large multiorgan lacerations of the intraand retroperitoneal organs and massive haemoperitoneuthese lesions were associated with brain lesions , diffuse intra - alveolar haemorrhage and a left hemidiaphragmatic lesion in one case . 
assessing the number , type and severity of lesions observed on the cadavers , revealed by direct necroscopic examination and / or radiography and toxicological analysis , is instrumental for establishing the causes of the event , preventing and reducing risks deriving from such accidents and understanding the death of the victims . 
il gruppo ii , composto da 3 cadaveri , ha mostrato lesioni di grado moderato - grave ( niss compreso tra 26 e 50 ) variamente distribuite nel distretto cranio - facciale , al torace e alladdome . 
in questo gruppo di pazienti la causa di morte stata attribuita ad as ssia meccanica associata a lesioni cerebrali in tutti i casi e a lacerazione dei visceri addominali con emoperitoneo in due casi , di cui uno associato a lesione dellemidiaframma sinistro con erniazione dello stomaco e della essura splenica del colon e laltro associato a lesione del miocardio ventricolare sinistro . 
il gruppo iii , composto da 2 cadaveri , ha presentato il pi alto score di niss ( 76 ) cio un valore relativo a lesioni incompatibili con la sopravvivenza , quali infarto e lacerazioni del miocardio associati a vaste lacerazioni multi - organo dei visceri intrae retro - peritoneali e cospicuo emoperitoneo . 
 discussione i meccanismi , la distribuzione e la tipologia delle lesioni traumatiche a seguito di un crollo di un edi cio abitativo sono molteplici e complessi e vanno principalmente , ma non esclusivamente , posti in relazione alla causa del crollo [ 915 ]  . 
la valutazione del numero , della tipologia e della gravit delle lesioni riscontrate sui cadaveri , evidenziate attraverso lesame necroscopico diretto e / o le indagini radiogra che e tossicologiche , rappresentano un elemento determinante per la comprensione delle cause dellevento , per la prevenzione e la riduzione dei rischi derivanti da tali incidenti ed , in ne , per la comprensione della morte delle vittime . 
infatti noto che a seguito di un crollo di un edi cio abitativo , indipendentemente dalle cause che lo determinano , le caratteristiche tecniche delledi cio e la modalit del danno siano intimamente legati al pattern del danno radiol med ( 2011 ) 116 : 969981 fig . 
b il reperto autoptico mostra la presenza di due ampie lacerazioni sulla super cie esterna del ventricolo cardiaco sinistro ( frecce )  . known that in the event of a building collapse , regardless of its causes , the technical characteristics of the building and the circumstances of the damage are more closely related to the pattern of injury and to the mechanism of the victims deaths rather than to a general increase in the risk of injury [ 810 ]  . 
 nel caso in oggetto , lesplosione di una bombola di gas ha rappresentato levento scatenante , ma non causa esclusiva della tragedia : i rilievi successivi al disastro hanno , infatti , dimostrato notevoli carenze strutturali ed irrego978 radiol med ( 2011 ) 116 : 969981 explosion of a gas cylinder triggered the event , it was not the only cause of the tragedy : in fact , surveys conducted after the catastrophe revealed signi cant structural inadequacies and irregularities in the planning , construction and maintenance of the building [ 4 ]  . 
the frequency and type of the lesions observed were closely related to the factors and cofactors that caused the event and are therefore comparable with events of the same type . 
lesion distribution revealed by autopsy indicated that the chest is the most frequently affected anatomical region and that asphyxia , probably due to dust inhalation following masonry collapse , was the main cause of death among the victims . 
 the paralytic ileus , observed at abdominal autopsy in all cases , should not be considered signi cant and related to the lesions detected at autopsy , as it is more reasonably connected with the death of the victims rather than with the signs of peritoneal irritation secondary to haemoperitoneu conversely , conventional radiology proved to be useful in supporting the evidence of some concurrent causes of death , such as hemidiaphragmatic lesions with visceral herniation , systemic bone disintegration and multiple rib fractures . 
in light of the results obtained from the radiographic assessment of the cause of death of these victims of a building collapse , we can state that radiography is no longer justi ed in that , although it provides complete and exhaustive information about skeletal lesions , it can only reveal the concurrent causes of death . 
 therefore , the use of modern software tools associated with current multislice ct and mr virtopsy techniques would appear more useful , as they provide an important contribution to identifying the victims and establishing causes , force vectors and concurrent causes of death [ 1618 ]  . 
 although it cannot supplant conventional autopsy , and taking into account the panoramic capabilities and shorter examination times of ct , the systematic use of these technologies is helpful in forensic practice , as it prevents or at least markedly reduces the number and duration of conventional autopsies while not altering the state of the cadavers [ 1921 ]  . 
consequently , radiologists with experience in postmortem imaging are needed to guide and support forensic specialists in de nitely establishing causes of death without necessarily having to perform conventional autopsy . 
la frequenza e la tipologia delle lesioni riscontrate risultano intimamente legate a fattori e cofattori che hanno determinato levento stesso ; pertanto , esse sono confrontabili e comparabili con evenienze delle medesima tipologia . 
la distribuzione delle lesioni autoptiche dimostra come il torace sia la regione anatomica maggiormente colpita e come las ssia , legata probabilmente allinalazione delle polveri a seguito del crollo delle opere murarie , sia stata la causa principale della morte delle vittime . 
lileo paralitico , evidenziato allesame diretto delladdome in tutti i casi , non da considerarsi signi cativo e correlabile alle lesioni autoptiche in quanto pi ragionevolmente connesso con lexitus delle vittime piuttosto che ai segni di irritazione peritoneale secondari allemoperitoneo . 
di converso , la radiologia tradizionale si dimostrata utile a supporto dellevidenza di alcune concause di morte quale la lesione dellemidiaframma con radiol med ( 2011 ) 116 : 969981 fig . 
6a skull radiograph : multiple displaced fractures with vertical direction on the front - parietal region of the skull ( arrow ) extending to the skull base and mandible ( arrow )  . 
multiple fratture scomposte a decorso verticale evidenti a livello del tavolato cranico fronto - parietale ( freccia ) con interessamento della base cranica e della mandibola ( freccia )  . 
alla luce dei risultati ottenuti dalla valutazione radiologica tradizionale nellaccertamento delle cause di morte nel decesso di persone coinvolte nel crollo di un edi cio abitativo , possiamo affermare che tale indagine risulta non pi giusti cabile in quanto , mentre per le lesioni scheletriche osteoarticolari fornisce informazioni complete ed esaustive , nellaccertamento dellevento fatale lindagine radiologica tradizionale pu svelare solo le concause di morte delle vittime . 
pertanto auspicabile che si utilizzino i moderni software legati allattuale tecnologia di tomogra a computerizzata ( tc ) multistrato e risonanza magnetica ( rm ) applicata alla virtopsy che offrono attualmente un contributo essenziale nellidenti cazione dei soggetti , nella de nizione degli agenti causali , dei vettori di forza e delle concause di morte delle vittime [ 1618 ]  . 
pur non sostituendosi allautopsia tradizionale e con le opportune differenze in termini di panoramicit e durata di esecuzione delle indagini a favore della tc , lutilizzo sistematico di tali apparecchiature risulta ef cace nella pratica clinica medico - legale perch consente di evitare o ridurre notevolmente il numero ed i tempi di esecuzione delle necroscopie tradizionali , rispettando totalmente lo stato di rilevamento dei corpi delle vittime [ 1921 ]  . 
corrispondentemente , divengono indispensabili radiologi esperti nellimaging post - mortem , al ne di potere indirizzare e sostenere i periti nellaccertamento de nitivo delle cause di decesso , senza dover necessariamente ricorrere al riscontro diretto . 
therefore , conventional radiography in these circumstances must be considered obsolete and inadequate , particularly in light of the potential of modern software tools provided with ct and mr technology . la radiologia tradizionale offre un contributo limitato nellaccertamento delle lesioni letali secondarie al crollo di edi ci abitativi . 
pertanto , lapproccio radiogra co tradizionale per laccertamento delle morti di tali pazienti da considerarsi obsoleto ed insuf ciente , specie alla luce delle potenzialit dei moderni software collegati alle attuali apparecchiature tc e rm . 
cova unit clinico operativa di radiologia , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , 34149 trieste , italy correspondence to : f . 
pozzi - mucelli , tel . : + 39 - 040 - 3994372 , fax : + 39 - 040 - 3994500 , e - mail : fabio.pozzimucelli@alice.it received : 26 may 2010 / accepted : 30 august 2010 / published online : 21 april 2011 springer - verlag 2011 abstract purpose . 
different embolisation agents were used : coils ( 17 cases ) , embolisation particles ( 14 cases ) , glue ( one case ) , coated stent ( two cases ) and mechanical occlusion devices ( two cases )  . 
technical success was achieved in 26 / 27 patients ( 96.3% ) ; in one case , embolisation of a polar artery arising from the aneurysmal sac was not possible . 
le indicazioni sono state : macroematuria sintomatica in 9 pazienti ( 33 , 3% ) ( tumorale in 7 casi e iatrogena in 2 ) , tumore renale sintomatico inoperabile in 5 pazienti ( 18 , 5% ) , voluminoso ematoma sottocapsulare o perirenale in 3 casi ( 11 , 1% ) ed aneurisma dellarteria renale principale in 2 casi ( 7 , 4% )  . 
in 8 pazienti ( 29 , 6% ) candidati a posizionamento di endoprotesi aortica addominale ( evar ) si proceduto alla preventiva embolizzazione del ramo renale polare originantesi dalla sacca aneurismatica o dal colletto sottorenale aortico per prevenire la possibile rivascolarizzazione della sacca . 
sono stati utilizzati diversi agenti embolizzanti : spirali ( 17 casi ) , particelle embolizzanti ( 14 casi ) , colla ( 1 caso ) , stent ricoperto ( 2 casi ) , occlusore meccanico ( 2 casi )  . 
one possible new indication is the prophylactic exclusion of the polar artery arising from the neck or the sac of an abdominal aortic aneurysm in patients who are candidates for evar . 
this procedure requires the availability of various materials for performing embolisation and experience in their use . keywords renal arteries kidney angiography embolisation invasiva nel trattamento della macroematuria sintomatica neoplastica / iatrogena e nella palliazione di tumori renali inoperabili . 
questa procedura richiede la disponibilit di diversi materiali per effettuare lembolizzazione ed esperienza nel loro utilizzo . parole chiave arterie renali rene angiogra a embolizzazione introduction introduzione one of the areas in which interventional radiology has demonstrated its ability to offer enormous therapeutic potential with minimal invasiveness regards arterial embolisation procedures . 
although there are many indications for endovascular embolisation or exclusion of the renal arteries and their distal and / or polar branches [ renal artery embolisation ( rae ) ] , these procedures are mainly done for therapeutic or palliative purposes in patients with renal trauma or tumour . 
nonetheless , in recent years , new indications have advanced , including preoperative embolisation of the renal polar arteries in patients who are candidates for endoprosthesis deployment to exclude abdominal aortic aneurysms ( aaa )  . 
different embolisation agents may be used to achieve the desired therapeutic result . the aim of this study was to review our experience with this procedure over the past 10 years to identify the current and emerging indications , the materials used and the results obtained . materials and methods a retrospective review of the interventional radiology procedures performed at our centre between june 1999 and july 2009 revealed 27 patients ( 19 men and eight women ; mean age 74 years ; age range 3793 years ) who had undergone rae . 
tali interventi vengono eseguiti in diversi distretti arteriosi ; a livello addominale tra le varie strutture arteriose che possono essere sottoposte ad embolizzazione vi sono le arterie renali e i suoi rami distali e / o polari . 
le indicazioni allembolizzazione o allesclusione endovascolare delle arterie renali e dei suoi rami distali e / o polari ( ear ) sono molteplici , ma queste procedure vengono effettuate principalmente a scopo terapeutico o palliativo in pazienti con traumi o tumori renali , anche se negli ultimi anni stanno emergendo ulteriori indicazioni quali lembolizzazione preoperatoria delle arterie renali polari nei pazienti candidati al posizionamento di endoprotesi per lesclusione di aneurismi dellaorta addominale . 
diversi sono i materiali embolizzanti che possono venire impiegati per ottenere un risultato terapeutico adeguato . scopo di questo lavoro rivalutare la nostra esperienza di circa 10 anni di attivit in questo tipo di procedure al ne di identi care le indicazioni attuali ed emergenti , i materiali utilizzati ed i risultati ottenuti . materiali e metodi ad una valutazione retrospettiva dellattivit di radiologia interventistica effettuata presso la nostra struttura nel periodo compreso tra giugno 1999 e luglio 2009 , 27 pazienti ( 19 maschi e 8 femmine ; et media : 74 anni ; range : 3793 anni ) sono stati sottoposti ad ear . 
tale procedura stata eseguita con la nalit di prevenire una possibile rivascolarizzazione della sacca aneurismatica dopo il posizionamento dellendoprotesi . la maggior parte delle procedure stata eseguita utilizzando un sistema per angiogra a e radiologia interventistica philips integris allura ( philips medical systems netherlands bv , best , olanda )  . 
 dopo preliminare aortogra a si proceduto a cateterismo selettivo o superselettivo dei rami arteriosi renali interessati e successivo rilascio di agenti embolizzanti quali spirali metalliche a rilascio non controllato ( cook , bloomington , in , usa ; boston scienti c corporation , natick , mass . , usa ; balt , montmorency , francia ) o dispositivi occlusori tipo plug ( amplatzer vascular plug , aga medical , golden valley , usa ) o stent ricoperti ( atrium , atrium medical corporation , hudson , usa ; jostent peripheral graft , jomed , rangendingen , germania ) o particelle embolizzanti non riassorbibili in alcol polivinilico ( pva ) o similare ( contour emboli , boston scienti c corporation , natick , usa ; bead block , terumo medical corp . , somerset , usa ; embosphere , biosphere medical , rockland , usa ) o riassorbibibili ( spon948 radiol med ( 2011 ) 116 : 945959 usa ) or absorbable particles ( spongostan standard ; j&j medical limited , gargrave , skipton , england ; curaspon , curamedical , assendelft , the netherlands ) or liquid embolisation agents , such as glues ( glubran 2 gem srl , viareggio , italy )  . 
in 11 patients ( 40.7% ) , two or three different embolisation agents were used . in all cases , a nal angiogram was obtained to evaluate the effective exclusion of the vascular region subjected to embolisation and the possible embolisation of nontarget segments , with technical success being de ned as the cessation of bleeding or vascular exclusion of the lesion after rae . results the results are reported in table 1 . 
in addition , in the latter case of highow arteriovenous stula , embolisation was initially attempted using multiple coils and , due to the persistence of reduced ow , completed with several coarse fragments of absorbable particles , which completely stopped the ow . 
 in tutti i casi stata eseguita unangiogra a nale di controllo per la valutazione delleffettiva esclusione del territorio vascolare sottoposto ad embolizzazione e di eventuali embolizzazioni di segmenti non bersaglio , de nendo come successo tecnico la cessazione del sanguinamento o lesclusione vascolare della lesione dopo ear . risultati i risultati sono riportati nella tabella 1 . 
in this case , the exclusion of a segmental branch , in addition to the aneurysm , did not produce ischaemic - like symptoms , and a contrast - enhanced colour doppler ultrasound performed 30 days after the procedure showed no areas of renal injury . in the patient in whom selective catheterisation was not possible , the inferior polar artery arose directly from the aneurysmal sac that , at preliminary ct angiography , appeared occupied by a large ulcerated thrombus . 
 in questo caso , lesclusione di un ramo segmentario , oltre allaneurisma , non ha comportato linsorgenza di alcuna sintomatologia di tipo ischemico ed un esame eco - color doppler con mezzo di contrasto , effettuato 30 giorni dopo , non ha evidenziato aree di sofferenza renale . 
 nel paziente in cui non stato possibile cateterizzare selettivamente larteria polare inferiore tale vaso originava direttamente dalla sacca aneurismatica che al preliminare controllo angio - tomogra a computerizzata ( tc ) appariva occupata da una vasta apposizione trombotica ulcerata . 
 solo in un caso ( 3 , 7% ) di paziente affetto da neoplasia renale inoperabile con macroematuria vi stata una recidiva della macroematuria a distanza di 13 mesi ed stato ritrattato con successo . 
polare pre - evar macroematuria in neoplasia renale macroematuria in neoplasia renale fav renale sintomatica neoplasia renale inoperabile sintomatica aneurisma dellarteria renale polare macroematuria in neoplasia renale neoplasia renale inoperabile sintomatica embolizzazione a . 
in another case , during the placement of a coil in a renal polar artery , the slightly oversized coil caused the distal end of the catheter to come out of the vessel . 
in un altro caso durante la fase di posizionamento di una spirale in unarteria polare renale , la spirale lievemente sovradimensionata ha causato la fuoriuscita dellestremit distale del catetere dal vaso . 
a distanza di tempo si osservato un incremento dellemoglobina in 9 / 11 ( 81 , 8% ) dei pazienti con macroematuria o ematoma sottocapsulare , mentre un decremento della creatininemia stato osservato in 9 / 27 ( 33 , 3% ) casi . discussion the indications for embolisation of the renal artery and its intraparenchymal branches are substantially codied and consist of the embolisation of inoperable renal tumours responsible for symptomatic haematuria or signi cant symptoms [ 15 ]  . 
it has in fact been suggested that the embolisation of renal lesions can slow down the le indicazioni allembolizzazione dellarteria renale e dei suoi rami intraparenchimali sono sostanzialmente codi cate e costituite dallembolizzazione di tumori renali inoperabili responsabili di ematurie sintomatiche o di sintomatologie importanti [ 15 ] in quanto stato suggerito che il trattadiscussione radiol med ( 2011 ) 116 : 945959 fig . 
1a - d donna di 69 anni operata 3 giorni prima di nefrectomia parziale al rene destro con anemizzazione e macroematuria , la ricostruzione tridimensionale volume rendering ( a ) mette in evidenza un singolo blush pseudoaneurismatico di mezzo di contrasto di circa 15 mm di diametro nei settori mediosuperiori del rene . 
d post - procedurale , dopo embolizzazione mediante tre spirali metalliche : completa esclusione dei foci pseudoaneurismatici e preservazione dei rami intraparenchimali . progression of metastatic disease [ 6 ]  . 
in agreement with other authors [ 7 ] , we do not perform preoperative embolisation in renal carcinoma patients who are candidates for nephrectomy , as there are no data in the literature to support this practice . 
 occasionally , those lesions can cause substantial bleeding with signi cant haematuria and large subcapsular or perirenal haematomas and produce dramatic , life - threatening mento di embolizzazione delle lesioni renali pu determinare un rallentamento nella progressione della malattia metastatica [ 6 ]  . 
in accordo con quanto sostenuto da altri autori [ 7 ] , non eseguiamo lembolizzazione preoperatoria nei pazienti candidati a nefrectomia per carcinoma renale in quanto non ci sono dati in letteratura che supportino tale pratica . 
on these occasions , the endovascular procedure needs to be extremely rapid [ 12 ] , whereas on other occasions , the symptoms may be absent or vague , with the patient clinically stable such that the endovascular procedure may be done electively [ 7 ]  . the overall results reported in the literature vary broadly according to the characteristics of the various patient popumaturie importanti ed ematomi sottocapsulari o perirenali voluminosi e sono causa di sintomatologie drammatiche che mettono a rischio la vita del paziente e lintervento endovascolare deve essere estremamente tempestivo [ 12 ] , mentre altre volte la sintomatologia pu essere assente o sfumata e il paziente clinicamente stabile , per cui la procedura endovascolare pu essere eseguita in elezione [ 7 ]  . 
c controllo angiogra co dopo embolizzazione mediante particelle riassorbibili e dispositivo occlusore . lations , with the best results in terms of technical success which , when referring to palliation of renal tumours , varies from 90% to 100% , with recurrence and therefore the need for a second embolisation procedure at 218 months from the initial procedure in 510% of cases [ 15 ]  . 
with regard to technical success in cases of acute haemorrhage ( traumatic / iatrogenic or secondary to expansile renal lesions ) , the literature reports values between 85% and 92% , with the need for a second embolisation procedure at 26 days in 1719% of cases [ 815 ]  . the literature [ 1 ] , but also our own experience , suggests that coils are the most frequently used embolisation agent in the treatment of traumatic lesions in that they are technically easier to use , whereas in palliative treatment , the i risultati complessivi riportati in letteratura variano ampiamente a seconda delle caratteristiche della casistica considerata con risultati migliori in termini di successo tecnico che , quando riferito alla palliazione di neoplasie renali , varia dal 90% al 100% con recidive , e quindi necessit di un secondo intervento di embolizzazione , nel 5%10% dei casi a 218 mesi dalla prima procedura [ 15 ]  . 
 per quanto riguarda il successo tecnico in caso di emorragie acute ( traumatiche / iatrogene o secondarie a lesioni espansive renali ) in letteratura sono riportati valori di successo tecnico compresi tra l85% e il 92% con necessit di un secondo intervento di embolizzazione a 26 giorni nel 17%19% dei casi [ 815 ]  . 
4a - c a 65 - year - old man with a history of hypertension , incidental aneurysm of the right renal aneurysa magnetic resonance angiography showing a 2 - cm aneurysm of the main trunk of the right kidney and a polar artery . 
c controllo angiograco dopo posizionamento di stent ricoperto con completa esclusione della lesione aneurismatica . use of embolisation particles is more frequent , as they produce a more distal embolisation [ 2 ]  . 
the literature also suggests greater effectiveness of embolisation treatment when trisacryl microspheres are used rather than pva particles due to their more distal penetration ( for the same diameter ) within the vascular nidus of the lesion [ 1 , 2 ]  . 
it should also be recalled that the literature reports the use of other embolisation agents , the so - called liquids , such as absolute alcohol [ 2 , 16 ] and glues [ 1719 ]  . 
various studies reported on their experience with embolisation at the renal level using an acrylic glue known as n - butyl - 2cyanoacrylate ( nbca ) [ 18 , 19 ]  . 
towards the end of the 1990s , however , it turned out that this use was not of cially authorised for endovascular treatment and was banned [ 20 ]  . 
in later years , however , a new glue derived from the former was introduced , the use of which is permitted emerge che le spirali rappresentano lagente embolizzante pi utilizzato nel trattamento delle lesioni traumatiche in quanto tecnicamente pi facili e maneggevoli da usare , mentre nelle embolizzazioni palliative pi frequente il ricorso alle particelle embolizzanti in quanto consentono unembolizzazione pi distale [ 2 ]  . 
sempre dalla letteratura sembra inoltre emergere una migliore ef cacia del trattamento embolizzante quando impiegate le microsfere trisacriliche piuttosto che le particelle in pva , in virt di una capacit di penetrazione pi distale ( a parit di diametro ) allinterno del nidus vascolare della lesione [ 1 , 2 ]  . 
va ricordato , inoltre , che in letteratura riportata la possibilit di utilizzo di altri agenti embolizzanti , cos detti liquidi , quali lalcol assoluto [ 2 , 16 ] e le colle [ 1719 ]  . 
in passato sono state riportate varie esperienze di embolizzazione a livello renale in cui veniva utilizzata una colla acrilica nota come radiol med ( 2011 ) 116 : 945959 for endovascular treatment . 
the glue is a comonomer consisting of two monomers : nbca and the monomer denominated ms by the manufacturer of the comonomer itself ( gem italy , viareggio , italy )  . 
with respect to nbca , the comonomer has the not insigni cant advantage of polymerising within the vessel in relatively longer times , thus allowing a more controlled embolisation procedure . 
 although this embolisation agent is very effective and enables a lasting and very distal embolisation , its use at the renal level has only been sporadically reported , probably due to the lack of ease in its use and the associated risk of embolising nontarget structures . 
also in our limited experience , we had the feeling of incomplete control of the release of the glue within the artery and , unlike the other patients treated with embolisation particles or mechanical agents , the patient suffered mild pain , which disappeared after a short time . further indications for embolisation of renal arteries are renal artery vascular diseases , such as arteriovenous stulas and acquired or congenital pseudoaneurysms [ 21 , 22 ] and aneurysms . 
encouraging short - term and long - term results have been presented both in case reports and more extensive studies [ 2326 ]  . a less frequently reported indication is the exclusion of an aneurysm of the renal artery . 
in truth , the inclusion of these cases in this series is debatable in that the coated stent guarantees the patency of a vessel , but at the same time , the exclusion of a pathological vascular segment is achieved and the exclusion of splanchnic or renal artery aneurysms with the use of coated stents has been reported as embolisation [ 2729 ]  . 
an alternative to the coated stent is , as mentioned above , the lling of the aneurysmal sac with coils or microcoils , preferably with controlled release , in similar fashion to the treatment of cerebral aneurysms [ 25 ]  . 
nonetheless , this embolisation technique cannot always be used , as in the case of wideneck aneurysms , because the coils may become unstable and protrude into the lumen of the vessel from which the aneurysm arises . 
the rst involves deploying a bare metal stent across the neck of the aneurysm and then lling the sac by passing the microcoils through the stent interstices with a microcatheter [ 30 , 31 ]  . n - butil - 2 - cianoacrilato ( nbca ) [ 18 , 19 ]  . 
si tratta di un comonomero costituito da 2 monomeri : ln - butil - 2 - cianoacrilato e il monomero denominato ms di propriet della ditta produttrice del comonomero stesso ( gemitaly , viareggio , italia ) , che rispetto allnbca ha anche il non trascurabile vantaggio di polimerizzare allinterno del vaso in tempi relativamente pi lunghi , consentendo una manovra di embolizzazione pi controllata . 
sebbene tale agente embolizzante sia molto ef cace e consenta unembolizzazione duratura e molto distale , il suo impiego a livello renale solo sporadicamente riportato e questo verosimilmente a causa del non suo facile impiego e al rischio di causare embolizzazione di strutture non bersaglio . 
anche nella nostra limitata esperienza si avuta la sensazione di un non sicuro controllo del rilascio della colla nellarteria e , a differenza degli altri casi in cui si sono utilizzate particelle embolizzanti o agenti meccanici , il paziente ha comunque avvertito una discreta sintomatologia dolorosa regredita in breve tempo . ulteriori indicazioni allembolizzazione delle arterie renali sono le patologie vascolari dellarteria renale , quali le stole artero - venose , i pseudoaneurismi acquisiti o congeniti [ 21 , 22 ] e gli aneurismi , e risultati incoraggianti a breve e lungo termine sono stati presentati sia in case report che in lavori con casistiche pi consistenti [ 2326 ]  . 
 meno frequente , ma comunque riportata , la procedura di esclusione di un aneurisma dellarteria renale : esistono varie opzioni , quali limpiego delle spirali o microspirali [ 2325 ] o lutilizzo di stent ricoperti [ 26 ]  . 
in realt pu essere discutibile considerare tali casi in questa casistica in quanto lo stent ricoperto garantisce la perviet di un vaso , ma allo stesso tempo si ottiene lesclusione di un segmento vasale patologico ed in letteratura lesclusione di aneurismi splancnici o renali mediante limpiego di stent ricoperti stata riportata come embolizzazione [ 2729 ]  . 
unalternativa allo stent ricoperto , come sopra accennato , il riempimento della sacca aneurismatica con spirali o microspirali , preferibilmente a rilascio controllato , analogamente a quanto viene fatto per gli aneurismi cerebrali [ 25 ]  . 
tuttavia tale tecnica di embolizzazione non sempre pu essere usata , come nel caso di aneurismi a colletto largo , poich le microspirali possono risultare instabili e protrudere nel lume del vaso da cui origina laneurisma . 
due possibili alternative in questi casi , in mancanza di stent ricoperti adeguati o nellimpossibilit di un loro posizionamento , sono il posizionamento di uno 956 radiol med ( 2011 ) 116 : 945959 an alternative method , although data available are still extremely preliminary , sees the use of a new type of multilayer stent composed of several layers of very ne nitinol wires , which preliminary studies show is able to maintain the ow in the vessel within the stent , whereas ow progressively lessens in the aneurysm until its complete thrombosis is achieved [ 32 ]  . a rare indication for rae , seen in our experience and also reported in the literature , is the treatment of haematuria and / or spontaneous haematoma in patients with autosomal - dominant polycystic kidney disease [ 33 ]  . 
a further indication that has appeared in recent years is embolisation of the renal polar branches originating from the aneurysmal sac or infrarenal neck in patients with an aaa who are candidates for evar . 
diffusion of this type of procedure has progressively led to the indication of embolisation of collateral branches , such as the lumbar arteries and the inferior mesenteric artery , to prevent reperfusion of the aneurysmal sac , with results that nonetheless fail to be completely convincing [ 34 , 35 ]  . 
it is instead unclear what attitude should be taken in relation to renal polar branches arising from the aneurysmal sac or the infrarenal neck of the aorta with the aim of preventing possible sac revascularisation . 
a review of the literature shows that some centres , prior to deploying the abdominal aortic endoprosthesis , embolise the renal polar arteries arising from the neck [ 36 , 37 ] , whereas other authors [ 38 , 39 ] who have not performed a preliminary embolisation of the renal polar artery and have evaluated the effect of the coverage by the endoprosthesis of those branches , have not observed consequences such as endoleak due to reperfusion or signi cant damage to the parenchyma and renal function resulting from a segmental infarction of the renal parenchyma . 
in our experience , we have observed that the nonembolisation of a polar branch arising from the aneurysmal sac tends to favour the development of a type 2 endoleak , not so much through the renal polar artery in which ow always remains normally directed , but through a lumbar artery or the inferior mesenteric artery in which the ow changes direction . 
 the procedure is justi ed only in cases of the polar artery arising from the sac , in that polar arteries arising from the neck are adequately closed simply by the deployment of the prosthesis . in our experience the procedure was carried out prior to stent non ricoperto in corrispondenza del colletto dellaneurisma e quindi , dopo essere passati tra le maglie dello stent con un microcatetere , il rilascio in sicurezza delle microspirali no ad ottenere il riempimento della sacca [ 30 , 31 ]  . una nuova alternativa , ma i dati sono ancora estremamente preliminari , data dalla possibilit di impiego di un nuovo tipo di stent , denominato multistrato , costituito da pi strati di li di nitinol molto sottili che , dalle esperienze preliminari , in grado di mantenere il usso nel vaso allinterno dello stent , mentre questo progressivamente si riduce nellaneurisma no alla completa trombosi di questultimo [ 32 ]  . unindicazione pi rara allesecuzione di una ear , osservata anche nella nostra esperienza e riportata anche in letteratura , rappresentata dal trattamento dellematuria e / o dellematoma spontaneo in pazienti con malattia policistica renale autosomica dominante [ 33 ]  . 
unulteriore possibile indicazione , emersa negli ultimi anni , lembolizzazione di rami polari renali originanti dalla sacca aneurismatica o dal colletto sottorenale in pazienti portatori di aneurismi dellaorta addominale candidati a trattamento di esclusione dellaneurisma mediante endoprotesi aortica ( evar )  . 
con la diffusione di tale tipo di intervento si progressivamente posta lindicazione alla procedura di embolizzazione di rami collaterali originantesi dalla sacca aneurismatica , quali le arterie lombari e larteria mesenterica inferiore per prevenire la riperfusione della sacca aneurismatica , con risultati che tuttavia non appaiono ancora del tutto convincenti [ 34 , 35 ]  . 
non invece chiaro latteggiamento da assumere nei confronti dei rami polari renali originantesi dalla sacca aneurismatica o dal colletto sottorenale dellaorta con lo scopo di prevenire possibili rivascolarizzazioni della sacca . 
 dalla revisione della letteratura abbiamo trovato che alcuni centri embolizzano , preventivamente al posizionamento di unendoprotesi aortica addominale , le arterie renali polari originantesi dal colletto [ 36 , 37 ] , mentre altri autori [ 38 , 39 ] , che non hanno eseguito lembolizzazione preliminare dellarteria polare renale e hanno valutato leffetto della copertura da parte dellendoprotesi di tali rami , non hanno osservato conseguenze quali lendoleak da riperfusione o danni signi cativi sul parenchima e la funzione renale quale conseguenza di un infarto segmentario del parenchima renale . 
nella nostra esperienza abbiamo osservato che la mancata embolizzazione di un ramo polare originante dalla sacca aneurismatica costituisce una causa favorente lo sviluppo di un endoleak di tipo 2 , non tanto attraverso larteria polare renale nella quale il usso rimane sempre normo - diretto , ma attraverso unarteria lombare o larteria mesenterica inferiore nelle quali il usso inverte la sua direzione . 
verosimilmente tale procedura giusti cata solo nei casi di arterie polari che originano dalla sacca , in quanto quelle che originano dal colletto vengono chiuse in modo radiol med ( 2011 ) 116 : 945959 fig . 
a langio - tc preprocedurale ( ricostruzione mip ) dimostra la presenza di unarteria polare inferiore accessoria destra in paziente portatore di rene a ferro di cavallo ; b arteriogra a selettiva dellarteria polare inferiore destra . 
c embolizzazione dello stesso vaso mediante 3 spirali metalliche con completa esclusione del usso ematico . the deployment of the endoprosthesis , on the same day or 1 or 2 days before the intervention . 
we preferred to perform the embolisation in the angiography suite rather than in the operating room where the aortic endoprosthesis placement is carried out because the c - arm available to us does not guarantee optimal image quality for precise execution of the procedure . adeguato semplicemente con il posizionamento della protesi . 
si preferito eseguire lembolizzazione nella sala angiogra ca piuttosto che in sala operatoria , dove si esegue il posizionamento dellendoprotesi aortica , in quanto larco a c a nostra disposizione non garantisce la qualit dimmagine ottimale per una precisa esecuzione della manovra . conclusions rae is an effective and minimally invasive procedure with low morbidity rates and short hospital stay . 
it should be considered the treatment of choice in neoplastic / iatrolear rappresenta una terapia ef cace e minimamente invasiva e deve essere considerata il trattamento di scelta conclusioni 958 radiol med ( 2011 ) 116 : 945959 genic symptomatic gross haematuria , in the palliation of inoperable renal tumours , aneurysms and arteriovenous malformations of the main renal artery or its branches and in the prophylactic exclusion of the inferior polar artery in candidates for evar . 
we believe that as tumours require a more distal and less focused embolisation , particles or glues are preferable , whereas coils or microcoils are more suited to vascular lesions ( active bleeding , pseudoaneurysms or stulas ) where a more targeted embolisation is required . 
nonetheless , the use of several agents together may occasionally be necessary . della macroematuria sintomatica neoplastica / iatrogena , nella palliazione di tumori renali inoperabili , di aneurismi e malformazioni arterovenose a carico dellarteria renale principale o dei suoi rami e nellesclusione preventiva dellarteria polare inferiore in pazienti candidati ad evar , con scarsa morbilit e breve degenza intraospedaliera . 
diversi sono gli agenti embolizzanti a disposizione : nella loro scelta sicuramente gioca un ruolo lesperienza delloperatore con il materiale da impiegare : riteniamo che per le lesioni tumorali , dove necessaria unembolizzazione pi distale e meno focalizzata , le particelle o le colle siano da preferirsi , mentre per le lesioni vascolari ( sanguinamenti attivi , pseudoaneurismi o stole ) le spirali o le microspirali , che consentono unembolizzazione pi mirata , siano pi adatte . 
in questo lavoro vengono descritte le caratteristiche in tomogra a computerizzata ( tc ) del sarcoma sinoviale primitivo del polmone ( ppss ) in 3 casi arrivati alla nostra osservazione e sottoposti ad intervento chirurgico , in associazione alla revisione della letteratura relativa a questo raro tumore toracico . 
nei 2 pazienti sottoposti anche a pet - tc , lesame dimostrava patologico accumulo del tracciante solo nella sede della lesione , senza altre localizzazioni toraco - addominali o muscolo - scheletriche . 
il terzo paziente ha avuto la conferma diagnostica di sarcoma sinoviale monofasico radiol med ( 2011 ) 116 : 868875 of monophasic synovial sarcoma in the third patient was con rmed using thoracoscopic biopsy discussion . 
both in the cases described and in those identi ed in the literature review , standard chest x - rays mainly showed a parenchymal mass of pleural origin with either irregular or well - de ned margins . 
ct characteristics are more de nite , with evidence of a mass with regular and sharply de ned margins , occasionally polycyclic , with inhomogeneous density due to the presence of colliquative areas within the tumour . 
sia nei casi descritti che nella revisione della letteratura la radiogra a standard del torace dimostra principalmente una massa parenchimale a margini sia irregolari che netti , a base pleurica . 
sebbene il ppss sia un tumore raro , la presenza di una massa polmonare a densit disomogenea , associata spesso a versamento pleurico ma senza adenopatie , in un paziente asintomatico o paucisintomatico deve indurre a considerare anche questa neoplasia nel range delle diagnosi differenziali dei tumori polmonari , escludendo la presenza di metastasi a partenza dai pi frequenti sarcomi sinoviali a carico dellapparato muscolo - scheletrico . keywords synovial sarcoma lung ct parole chiave sarcoma sinoviale polmone tc introduction introduzione synovial sarcoma is a cancer usually originating in the para - articular soft tissues of the limbs in young adults [ 1 ]  . 
the rise of sophisticated diagnostic techniques in immunohistochemistry , electron microscopy and cytogenetic analysis has led to a more frequent recognition of pssl as a well - de ned histological subtype of sarcoma of the lung [ 4 ]  . 
 we also present a review of the literature regarding this rare thoracic tumour . il sarcoma sinoviale una neoplasia che normalmente origina nei tessuti molli para - articolari delle estremit in giovani adulti [ 1 ]  . 
 [ 3 ] nel 2002 hanno descritto il ppss come una distinta entit anatomica con caratteristiche anatomopatologiche simili a quelle del tumore delle parti molli e la diagnosi deve essere confermata dopo aver escluso altre neoplasie primitive sarcomatose ( per esempio il carcinoma sarcomatoide ) e le metastasi da sarcomi di altri organi . 
 laumento delle tecniche di diagnosi so sticata in immunoistochimica , in microscopia elettronica e nelle analisi citogenetiche , ha portato ad un pi frequente riconoscimento del ppss come un ben de nito sottotipo istologico di sarcoma del polmone [ 4 ]  . 
in questo lavoro vengono descritte le caratteristiche in tomogra a computerizzata ( tc ) del ppss di 3 casi arrivati alla nostra osservazione e sottoposti ad intervento chirurgico , in associazione alla revisione della letteratura relativa a questo raro tumore toracico . 
 materials and methods clinical and radiological ndings of three patients with a diagnosis of pssl were obtained through a review of the le informazioni cliniche e radiologiche di 3 pazienti con materiali e metodi 870 radiol med ( 2011 ) 116 : 868875 clinical records of the department of thoracic surgery and the ct [ and possible positron emission tomography pet - ct ] examinations in the radiology archives , either on the picture archiving and communication system ( pacs ) or on x - ray lall patients were men and aged between 51 and 65 ( mean 58 ) years . 
another patient had undergone thoracoscopic resection of a lesion of the left lower lobe 18 months previously ; the lesion was at rst diagnosed as a brous pleural tumour and then as a monophasic synovial sarcoma . 
the other two patients had symptoms characterised by pain in the hemithorax and shoulder corresponding to the tumour , with fever in one patient only . all patients had undergone both chest x - rays and ct scans , and two were also studied with pet - ct ( siemens biograph - 16 - usa )  . 
the thoracoabdominal ct scans ( all using intravenously administered contrast medium omnipaque 350 , ge healthcare , usa ) were performed with a range of equipment including conventional , single - slice or 16 - slice multidetector ct ( siemens somaton emotion , siemens , germany )  . 
two patients underwent tumour removal , whereas the third was rst operated on ( due to a diagnosis at variance with the nal one ) and then underwent thoracoscopy with a biopsy of the pleural lesions . results in all cases , chest x - ray revealed the presence of lung masses measuring , respectively , 7 , 6 and 4.5 cm ( mean 5.8 cm ) in diameter , two of which were located in the right upper lobe and one in the left lower lobe . 
mediastinal adenopathy , which was diagnosi di ppss sono state ottenute dalla revisione delle cartelle cliniche della chirurgia toracica e degli esami tc e , eventualmente , di tomogra a a emissione di positroni pet - tc , presenti negli archivi radiologici , sia su sistemi picture archiving and communications system ( pacs ) che su pellicola radiogra ca . 
un paziente era gi stato sottoposto a bilobectomia destra 13 anni prima e a resezione di recidiva 10 prima dellattuale neoplasia per blastoma polmonare e un altro paziente era stato sottoposto18 mesi prima a resezione per via toracoscopia di una lesione del lobo inferiore sinistro diagnosticata in prima istanza come tumore broso della pleura e in secondo tempo come sarcoma sinoviale monofasico . 
negli altri 2 pazienti era presente sintomatologia caratterizzata da dolore allemitorace e alla spalla corrispondenti alla neoplasia e a febbre in un solo paziente . tutti avevano eseguito sia la radiogra a del torace che la tc e due anche la pet - tc ( biograph 16 , siemens , usa )  . 
 gli esami tc toraco - addominali ( sempre anche con mezzo di contrasto [ mdc ] endovena [ ev ] ; omnipaque 350 , ge healthcare , usa ) sono stati effettuati con differenti apparecchiature ( tradizionale , singolo strato o multidetettore a 16 strati ; somaton siemens , emotion siemens , germania )  . 
due pazienti sono stati operati con asportazione della neoplasia e 1 stato prima operato ( con diagnosi diversa da quella de nitiva ) e poi sottoposto a toracoscopia con biopsia delle lesioni pleuriche . risultati in tutti i casi la radiogra a del torace era risultata positiva dimostrando la presenza di masse polmonari , rispettivamente di 7 , 6 e 4 , 5 cm ( media 5 , 8 cm ) , localizzate 2 nel lobo superiore destro e una nel lobo inferiore sinistro . 
adenopatie mediastiniche , peraltro non signi cative , erano presenti in un solo paziente e ancora in un unico paziente era presente un nodulo inderadiol med ( 2011 ) 116 : 868875 fig . 
contrast - enhanced ct of the chest ( b ) : bulky , partly colliquated , paramediastinal mass in the upper right lobe without cleavage plane with the posterior tracheal wall and compressing the superior vena cava . 
tc torace con mdc ( b ) : voluminosa massa paramediastinica superiore destra , in parte colliquata , senza piano di clivaggio con la parete postero - laterale della trachea e con compressione sulla vena cava superiore . 
 linfonodi con aspetto reattivo in regione paratracheale inferiore destra . not signi cant , was present in one patient only ; also in one patient , there was an indeterminate nodule 5 mm in diameter close to the main lesion . 
in the two patients who also underwent pet - ct , the examination showed pathological tracer uptake con ned to the lesion site , without other thoracoabdominal or musculoskeletal localisations . ct - guided biopsy , performed in only one patient , proved positive for a mesenchymal tumour . 
in the third patient , who had undergone resection of a pulmonary nodule 18 months previously , the diagnosis of monophasic synovial sarcoma was con rmed by thoracoscopic biopsy ; this patient could not proceed to surgery owing both to lesion extent and to the fact that the lesion was considered a recurrence of pssl arising a short time after initial surgery . 
nei due pazienti sottoposti anche a pet - tc , lesame dimostrava patologico accumulo del tracciante solo nella sede della lesione , senza altre localizzazioni toraco - addominali o muscolo - scheletriche . 
il terzo paziente , quello operato 18 mesi prima per resezione di nodulo polmonare , ha avuto la conferma diagnostica di sarcoma sinoviale monofasico dalle biopsie toracoscopiche , senza poter procedere ad intervento chirurgico sia per lestensione della lesione sia perch la stessa stata considerata come recidiva di ppss a breve distanza dal primo intervento . 
2a , b tc torace con mdc : versamento pleurico sinistro con nodi solidi ( frecce ) e atelettasia da compressione del lobo inferiore per recidiva di sspp asportato 18 mesi prima . 
normally , patients with pssl report chest pain , cough and / or shortness of breath , but in 24% of cases , the tumour is discovered during chest x - rays performed for other reasons , as occurred in one of our patients [ 6 ]  . 
 [ 9 ] reviewed the imaging features of 12 cases of pssl . in our study , standard chest x - rays mostly show a parenchymal mass of pleural origin with margins that are either irregular or sharp . 
ct features are better de ned : the mass always displays sharp margins and a regular , at times polycyclic , outline , with inhomogeneous density due to colliquative areas within the tumour . 
 normalmente i pazienti con ppss riferiscono comparsa di dolore toracico , tosse e / o dispnea , ma nel 24% dei casi la neoplasia viene scoperta casualmente in seguito ad esame radiologico del torace eseguito per altri motivi , come successo in uno dei nostri pazienti [ 6 ]  . 
le caratteristiche tc sono pi de nite : sempre presente una massa a margini netti e contorni regolari , a volte policiclici , con densit disomogenea per presenza di aree di colliquazione allinterno . 
3a - d preoperative contrast - enhanced chest computed tomography ( ct ) ( a , b ) : homogeneously dense mass close to the anterior junction line on the right . 
tc torace eseguita dopo 5 anni dallasportazione della lesione precedente : comparsa nuova massa paramediastinica nella stessa sede ( c ) con adenopatie in parte colliquate sempre in sede precarenale ( d )  . eral pleural effusion is often present , but calci cations and adenopathy are rare . 
 more rarely , pssl can present as a solitary pulmonary nodule , an endobronchial tumour or a mass within the pulmonary arteries . the differential diagnosis must take into account the common primary tumours of the lung as well as metastases arising from tumours elsewhere in the body ( especially musculoskeletal tumours ) , as well as pleural broma , mesothelioma and the rare lung sarcomas ( brosarcoma , sarcomatous carcinoma , leiomyosarcoma or haemangiopericytoma )  . 
 la diagnosi differenziale radiologica deve prendere in considerazione i comuni tumori primitivi del polmone , ma anche le metastasi da neoplasie in altre sedi ( con particolare riguardo a quelle dellapparato muscolo - scheletrico ) , il broma pleurico . 
sicuramente la conoscenza di precedente esposizione ad asbesto indice di insorgenza di mesotelioma e la presenza di adenopatie mediastiniche nettamente pi frequente nel carcinoma broncogeno rispetto al ppss dove , come stato 874 table 1 characteristics at computed tomography size lobe 1 upper right 76 cm 2 lower left 64 cm colliquative colliquative 3 upper right 44.5 cm solid homogeneous tabella 1 caratteristiche tc radiol med ( 2011 ) 116 : 868875 densitometric characteristics other nodules pleural effusion mediastinal adenopathy signs of in ltration prior surgery yes same lobe , 5 mm yes chest wall yes , with solid pleural nodules subcarinal resection of nodule lower left lobe mediastinal median and lower right fat bilobectomy lobo grandezza caratteristiche densitometriche altri noduli versamento pleurico adenopatie mediastiniche segni di in ltrazione pregresso intervento 1 superiore destro 2 inferiore sinistro 76 cm 64 cm 3 superiore destro 44 , 5 cm colliquata colliquata solida omogenea s , stesso lobo , 5 mm si parete toracica s , con noduli pleurici solidi sottocarenale no resezione nodulo lobo inferiore sinistro bilobectomia grasso mediastinico medio - inferiore destra opathy is signi cantly more frequent in bronchogenic carcinoma when compared with pssl where , as already noted , enlarged lymph nodes are rare . in radiological terms , our three patients exhibited the most common form of the cancer , presenting with lung masses and pleural effusion , even though the small lesion excised in one of the patients and diagnosed as a brous tumour was actually a pssl in nodular for perhaps an incorrect diagnosis can also explain the patient with a previous diagnosis of blastoma , the lack of targeted immunohistochemical examinations leading to an evident initial error in lesion interpretation . 
treatment is surgical , sometimes combined with chemotherapy and radiotherapy , which , however , do not provide favourable prognostic outcomes . reported survival is between 6 and 58 months following diagnosis , even though 80% of patients display tumour recurrence in the same hemithorax but without abdominal lesions [ 10 ]  . 
nonehave died , and one is still alive more than 6 years after surgery . given that lung metastases from soft - tissue sarcoma are more common than pssl [ 11 ] , the diagnosis should also be supported by medical history , clinical examination and radiological search for tumours in other sites in the body . 
 i nostri tre pazienti rientrano radiologicamente nella forma pi comune della neoplasia , presentandosi con masse polmonari e con versamento pleurico , anche se la piccola lesione operata in uno dei pazienti e diagnosticata come tumore broso era in realt un ppss in forma nodulare . 
 forse una errata diagnosi si pu ipotizzare anche per il paziente con precedente diagnosi di blastoma : la mancanza di esami immunoistochimici mirati ha portato ad un evidente primo errore interpretativo della lesione . 
 la sopravvivenza riportata in letteratura compresa tra i 6 e i 58 mesi dalla diagnosi , anche se l80% dei pazienti ha mostrano ripresa di malattia nello stesso emitorace di partenza , senza lesioni addominali [ 10 ]  . 
la lunga sopravvivenza , pur in caso di recidiva , documentata anche nei nostri pazienti : nessuno deceduto e uno di loro ancora vivo dopo pi di 6 anni dallintervento . 
 poich la presenza di metastasi polmonari da sarcoma delle parti molli pi comune rispetto al ppss [ 11 ] , la diagnosi deve essere supportata anche dalla storia del paziente , dallesame clinico e dalla ricerca radiologica di neoplasie in altre sedi . 
a questo scopo indicata la pet che mostra un importane aumento dello standard uptake value radiol med ( 2011 ) 116 : 868875 pet - ct is excellent for this purpose , displaying a notable increase in standard uptake value in regions affected by neoplasms . 
a diagnosis of pssl is dif cult to reach with the use of ultrasoundor ct - guided biopsy alone , as the only result obtained is often that of an unspeci ed malignancy of mesenchymal origin , as indeed happened in our patient who underwent this procedure . in conclusion , although pssl is a rare tumour , the presence of a lung mass with inhomogeneous density , often associated with pleural effusion but without adenopathy , in an asymptomatic or poorly symptomatic patient should lead to this tumour being considered in the differential diagnosis after excluding the presence of metastases from the more frequent synovial sarcomas affecting soft tissues . ( suv ) nelle regioni interessate da neoplasia . 
cattaneo labanof , laboratorio di antropologia e odontologia forense , sezione di medicina legale , dmu dipartimento di morfologia umana e scienze biomediche , universit degli studi di milano , via mangiagalli 37 , milano , italy correspondence to : c . 
the increasing applications of forensic radiology and the wide use of conventional radiography and computed tomography ( ct ) in routine clinical practice demonstrate the potential of these technologies as tools for verifying the correspondence between an unidenti ed body and an identity suspect . 
despite the increasing importance of the comparison between radiographic and ct ndings , numerous limitations still need to be overcome , including the fact that few forensic centres have access to sophisticated x - ray technologies and that the reliability of those technologies for detecting speci c morphological traits and bone lesions is a matter of intense debate . 
 in addition , as with other morphological methods for identi cation , comparisons between antemortem and postmortem data require standardisation and statistical analysis , especially in europe where there are very few indications concerning the admission in court of evidence obtained by anthropological and radiological methods . 
in the future , with developments in radiographic technologies and increasing numbers of studies on their application to the forensic setting , radiology will become one of the most useful tools in the eld of personal identi cation . riassunto lidenti cazione personale dei cadaveri senza identit cruciale per motivi etici , giuridici e civilistici , e viene eseguita tramite un confronto fra i dati del pro lo biologico ottenuti dal cadavere e il materiale ante mortem di uno o pi sospetti didentit o persone scomparse . 
le crescenti applicazioni della radiologia forense e lampio uso della radiogra a tradizionale e della tomogra a assiale computerizzata ( tac ) nella comune pratica clinica mostrano la potenziale importanza di tali tecnologie come strumento di veri ca della corrispondenza fra un corpo senza identit ed un sospetto didentit . 
questo studio vuole esporre una revisione della letteratura riguardante lapplicazione della radiologia forense al complesso ambito dellidenti cazione personale ; nonostante la crescente importanza del confronto fra radiogra e ed immagini tac , numerosi limiti aspettano ancora di essere superati ; al momento infatti pochi istituti di medicina legale hanno accesso agli strumenti radiogra ci pi so sticati , e sta sorgendo un ampio dibattito sulla reale af dabilit di tali tecniche nellidenti cazione di speci ci tratti morfologici e lesioni su osso . 
inoltre , cos come altri metodi identi cativi basati sul confronto morfologico , anche il confronto fra dati radiogra ci ante e post mortem richiede una standardizzazione ed un approfondimento statistico , specialmente in europa ove esistono pochissime indicazioni sulla modalit di ammissione di una prova scienti ca ottenuta tramite metodi antropologici e radiologici in un processo . 
in futuro , con lo sviluppo delle tecnologie radiogra che e laumento del numero di studi riguardanti la loro applicazione a contesti forensi , la radiologia diverr uno degli strumenti pi utili nel campo dellidenti cazione personale . radiol med ( 2011 ) 116 : 960968 keywords forensic anthropology forensic radiology biological pro le personal identi cation parole chiave antropologia forense radiologia forense pro lo biologico identi cazione personale introduction introduzione forensic pathologists and anthropologists are often called in to help identify an unknown cadaver . 
the identi cation of an unidenti ed body is crucial both from a juridical point of view in particular for criminal , civil , insurance and administrative reasons and for ethical reasons for the reconciliation of the family with the lost relative . 
 whenever the unknown body is well preserved , bodily features such as height , eye colour , hair colour and marks such as tattoos or scars are usually useful to assist in identity . 
conversely , when the body is badly preserved , mummi ed , skeletonised or even charred , the application of techniques provided by forensic anthropology is mandatory . when the cadaver has a presumed identity and personal identi cation is requested , several disciplines can be applied , such as odontology , genetics and dactyloscopy . 
although plain radiography is widely used by experts [ 28 ] , today , more advanced radiographic techniques such as computed tomography ( ct ) and multidetector ct ( mdct ) are also applied in forensics [ 911 ]  . 
the odontological procedures for personal identi cation are the easiest and fastest to use and can be performed with dental charts , casts and various types of x - ray examinations [ 15 , 16 ]  . 
lidenti cazione di un cadavere senza identit cruciale sia da un punto di vista giuridico , poich coinvolge motivazioni di ordine penale , civile , assicurativo ed amministrativo , sia per esigenze etiche , nalizzate a restituire il corpo del defunto ai propri parenti . 
in caso di cadaveri sconosciuti con un sospetto didentit , tre fattori devono essere attentamente valutati : lo stato di decomposizione del corpo , il materiale ante mortem ( am ) raccolto dal sospetto didentit , e le tecniche disponibili per lidenti cazione , congiuntamente alle indicazioni riguardanti la loro accuratezza . 
 quando un cadavere sconosciuto ben conservato , le caratteristiche corporee come laltezza , il colore degli occhi e dei capelli , contrassegni come cicatrici , tatuaggi , ecc . , sono in genere utili allidenti cazione . 
tuttavia , quando queste ultime non possono essere utilizzate ( ad esempio , la documentazione am non disponibile ) , la radiologia forense diviene lunico strumento per ottenere unidenti cazione positiva [ 1 ]  . 
limmagine radiogra ca ampiamente e comunemente utilizzata in ambito identi cativo [ 28 ] , sebbene attualmente anche le pi avanzate tecniche radiogra che come a tomogra a assiale computerizzata ( tac ) e la multi - detector computed tomography ( mdct ) trovano unutile applicazione in ambito forense [ 911 ]  . 
 nel processo identi cativo i dati radiogra ci am e post mortem ( pm ) sono messi a confronto e la corrispondenza fra le due immagini deve essere ottenuta tramite una meticolosa comparazione dei dettagli [ 1214 ]  . 
questo approccio viene ampiamente utilizzato nel campo dellodontologia forense , ove le caratteristiche anatomiche , patologiche e iatrogene degli elementi dentari contribuiscono a rendere unico il pro lo dentario ; da questo punto di vista , le procedure di identi cazione personale basate su metodi odontologici sono le pi facili e veloci da effettuarsi , e possono essere eseguite tramite schemi dentali , sovrapposizioni dentarie e indagini radiogra che [ 15 , 16 ]  . 
laccuratezza e laf dabilit di tale approccio ampiamente riconosciuto ; nondimeno , tale confronto pu essere eseguito su ogni distretto osseo , anche 962 radiol med ( 2011 ) 116 : 960968 general , it is essential to detect and focus on the distinctive and unchangeable individual features . 
unfortunately , such unique and unchangeable features have not yet been de ned in forensic medicine , nor has any speci c number of concordant traits been established to ascertain an identity [ 18 ]  . 
for example , fischman states that one to four concordant features and no discrepancies are usually considered to claim an identity [ 14 ] ; brogdon [ 17 ] states that a minimum number should not be pursued , as a bunch of common and nonspeci c features is sometimes enough to claim an identity ; kuehn et al . 
in general , the identi cation process is quite easy and straightforward when dealing with bone prosthesis , bone calluses , osteoarthritis and other exceptional traits ; indeed , mann and brogdon state that one feature is enough when it is unique and unmistakable [ 4 , 17 ] , but ascertainment of identity is more dif cult when no particular feature is involved . 
moreover , research carried out on the frequencies of morphological characteristics of the skeleton , such as fractures , pathological conditions and surgical hardware , suggests that some features previously supposed to be suf ciently unique may in fact be quite common [ 20 ]  . 
in fact , the direct comparison of antemortem and postmortem x - rays is widely applied by international experts dealing with personal identi cation [ 2 , 5 , 22 , 23 ]  . 
judges subject forensic science techniques to strict evaluation of scienti c bases , and whenever a method fails to prove reliable , the expert examination may be rejected in court . 
anthropological and radiological methods in fact often deal with morphological assessment of skeletal features , which are based on the personal experience of the single expert witness and the error rate and standard deviation of which are not easily quanti able . 
this means that such methods cannot provide a reliable rate of probability of positive matching , which is requested by the daubert criteria on the admissibility of scienti c evidence in trial [ 24 ]  . 
only in recent years has forensic anthropology found a base for its admission in court , thanks to the kumho sentence , which stated that the daubert criteria are exible and that scienti c evidence se alcuni distretti sembrano pi af dabili di altri ( ad esempio , il torace , il capo , laddome ) [ 17 ]  . 
sfortunatamente , in ambito forense non si ancora raggiunta una de nizione di tali caratteri unici ed immutabili , n un numero speci co di tratti concordanti necessari per stabilire lidentit [ 18 ]  . 
ogni autore suggerisce un diverso numero di caratteristiche necessarie : fischman [ 14 ] sostiene che da uno a quattro tratti in comune e nessuna discrepanza emersa sono comunemente considerati suf cienti per raggiungere unidenti cazione positiva , mentre brogdon [ 17 ] dichiara che un numero minimo di caratteristiche non pu essere stabilito in quanto un insieme di caratteristiche anche solo comuni e non speci che talvolta suf cienti per effettuare unidenti cazione . 
in generale , il processo di identi cazione abbastanza facile e lineare quando riguarda protesi ossee , calli ossei , particolari forme di osteoartrosi ed altri tratti eccezionali ; infatti mann [ 4 ] e brogdon [ 17 ] sostengono che un solo tratto suf ciente se unico e inconfondibile , ma lidenticazione diviene molto pi dif cile quando non coinvolta nessuna caratteristica particolare . 
inoltre , una ricerca effettuata sulla frequenza delle caratteristiche morfologiche dello scheletro , come fratture , condizioni patologiche ed impianti chirurgici , suggerisce che alcuni tratti precedentemente considerati , suf cientemente unici , possono essere piuttosto comuni [ 20 ]  . 
alcuni autori sostengono che la quanti cazione e la standardizzazione delle caratteristiche utili allidenti cazione personale non necessaria e che lopinione del consulente in tali casi valido e suf ciente [ 21 ] ; infatti , la diretta comparazione del materiale radiogra co am e pm ampiamente applicata in ambito internazionale per lidenti cazione personale [ 2 , 5 , 22 , 23 ]  . 
 tuttavia , sfortunatamente questo approccio qualitativo pu mostrare alcuni limiti cruciali nel corso del processo ; infatti i giudici sottopongono le tecniche di indagine forensi ad una stretta valutazione delle basi scienti che e qualora un metodo fallisca nel dimostrarsi af dabile , quella speci ca indagine pu essere rigettata dalla corte ; i metodi antropologici e radiologici infatti spesso riguardano la valutazione morfologica di caratteristiche scheletriche , basata sullesperienza personale del singolo consulente , e il cui margine di errore e deviazione standard non sono facilmente determinabili : questo signi ca che tali metodi non possono fornire una af dabile probabilit riguardante lidenti cazione positiva , che tuttavia richiesta dai criteri stabiliti dalla sentenza daubert riguardati lammissibilit di una prova scienti ca nel processo [ 24 ]  . 
solo negli ultimi anni lantropologia forense ha trovato una base per la sua ammissibilit in aula , grazie alla sentenza kumho , che stabilisce che i criteri della radiol med ( 2011 ) 116 : 960968 may be based on the scienti c experience of the single expert witness [ 25 ]  . 
as a result , there is a strong need to quantify the error rate of the techniques used in forensic anthropology and radiology , and several forensic anthropologists are working to this effect . 
standardisation of the anthropological identi cation methods is particularly needed if one considers that speci c guidelines such as the daubert criteria or kumho sentence are still missing in europe , and that there is therefore no precise indication regarding the admission of scienti c evidence in court . 
 in forensic radiology , research for identi cation is conducted on the skeletal features of several body districts : head ( suture pattern , frontal sinuses ) [ 21 , 26 ] , thorax ( vertebrae , ribs , clavicles ) [ 17 , 19 , 27 ] , abdomen and pelvis ( vertebrae , scoliosis , etc . ) [ 17 , 23 ] , arms and legs [ 2 , 3 ]  . 
this paper presents a review of the classical and more recent applications of forensic radiology in the broad eld of identi cation subdivided into the issues of biological identity and personal identi cation . biological pro le : sex , age , stature at times it is necessary to build a biological pro le when no presumed identity exists . 
ct and mdct are widely explored and applied by several authors to a biological pro le [ 31 ] , also in mass disaster fatalities [ 9 , 11 ]  . 
several authors have demonstrated that information on sex , age and height can be obtained by obtaining ct scans of a dead body [ 9 , 32 ]  . positive or personal identi cation daubert sono essibili e che la prova scienti ca pu essere basata sullesperienza scienti ca del singolo consulente [ 25 ]  . 
per tale ragione , esiste attualmente una forte necessit di quanti care lerrore delle tecniche usate in antropologia e radiologia forense , e diversi autori sono impegnati per trovare una soluzione a tale necessit . 
gli antropologi forensi infatti stanno tentando di dare una quanti cazione ai risultati delle tecniche di identi cazione osteologica , e tale tentativo ancora pi necessario se si pensa che in europa speci che linee guida per lammissibilit della prova scienti ca come i criteri di daubert o la sentenza kumho sono ancora del tutto assenti , e pertanto non esiste ancora alcuna indicazione precisa riguardante tale argomento . 
 in radiologia forense , lapprofondimento dellidenti cazione avviene su criteri scheletrici provenienti da diversi settori corporei : capo ( suture craniche , seni frontali ) [ 21 , 26 ] , torace ( vertebre , coste , clavicole ) [ 17 , 19 . 
questo articolo ha come scopo la presentazione di una revisione della letteratura riguardante le applicazioni classiche e pi recenti della radiologia forense nel campo dellidenti cazione , suddivise nei due ambiti riguardati la de nizione dei caratteri biologici e lidenti cazione personale speci ca . 
la ricostruzione del pro lo biologico include la diagnosi di sesso , stima di et , statura e appartenenza etnica ; lesame radiologico dei distretti scheletrico e dentario sono imprescindibili per determinare let del soggetto se si trova nella fascia di et dellinfanzia e delladolescenza [ 28 ]  . 
la radiologia pu inoltre fornire importanti informazioni riguardanti il sesso ; diverse misure infatti possono essere utilizzate per una valutazione del genere del soggetto [ 29 , 30 ]  . 
la tac e la mdct sono attualmente ampiamente utilizzate ed applicate da diversi autori per la ricostruzione del pro lo biologico [ 31 ] , anche nel caso di disastri di massa [ 9 , 11 ]  . 
diversi autori hanno dimostrato che possibile ottenere informazioni su sesso , et ed altezza usando le scansioni tac su cadaveri [ 9 , 32 ]  . head identi cazione personale positiva capo there is a presumed identity , forensic radiwhen ology is essential for personal identi cation . 
different authors have reported cases of positive identi cation based on x - rays of the head through a pure visual comparison of quando presente un sospetto didentit , la radiologia forense ha unimportanza cruciale per lidenti cazione personale . 
in particolare i seni frontali sono ampiamente utilizzati e studiati , sia nellambito classico che in quello pi innovativo della radiologia : diversi autori 964 radiol med ( 2011 ) 116 : 960968 skeletal features [ 8 ]  . 
other authors focused on the application of advanced techniques to the frontal sinuses , with the aim of de ning an objective and quantitative method of analysis to replace simple visual comparison , with encouraging results [ 26 ]  . 
a similar quantitative approach , applied to cranial suture patterns , was adopted by rogers and allard [ 21 ] , who undertook an extensive statistical study of the number , position , length and direction of the lines , concluding that four consecutive corresponding lines ( for length , position and direction ) are enough to claim a positive identity [ 21 ]  . 
 recent clinical approaches involve the use of ct and magnetic resonance imaging ( mri ) instead of plain radiography , but this tendency makes it even more dif cult to obtain adequate antemortem data . 
solved an identi cation case by comparing the ct images of the bone structures of the skull , and in particular , the details of the frontal and sphenoid sinus , mastoid and ethmoid air cells , torcular and sagittal cranial suture [ 33 ]  . 
 they studied both morphological and metric features , concluding that the morphological feature ( presence or absence of the sinuses , presence , absence or incompleteness of intrasinus septum , etc . ) differed signi cantly in the population . 
altri autori si sono focalizzati sullapplicazione di tecniche pi avanzate ai seni frontali , con lo scopo di raggiungere un obiettivo metodo di analisi quantitativa , che potesse rimpiazzare la semplice comparazione a occhio dei pro li dei seni , con risultati incoraggianti [ 26 ]  . 
un simile approccio quantitativo , applicato al disegno delle suture craniche , fu seguito da rogers e allard [ 21 ] , che intrapresero un ampio studio statistico su numero , posizione , lunghezza e direzione delle linee , concludendo che 4 linee consecutive corrispondenti ( per lunghezza , posizione e direzione ) sono suf cienti per effettuare unidenti cazione positiva . i recenti approcci clinici riguardano luso della tomogra a elettronica a scansione e della risonanza magnetica nucleare ( rmn ) invece delle classiche proiezioni radiogra che , ma questa tendenza rende ancora pi dif cile la ricerca di adeguata documentazione am . 
 [ 33 ] hanno concluso un caso identi cativo tramite comparazione di immagini tac della struttura ossea del cranio , analizzando nel confronto i seni frontali e sferoidale , le celle mastoidee ed etmoidali e la sutura sagittale . 
 [ 10 ] cercarono di sviluppare un metodo facile ed af dabile per lidenti cazione personale sulla base dei seni frontali , analizzando sia gli aspetti morfologici che metrici , e concludendo che le caratteristiche morfologiche ( presenza od assenza dei seni , presenza , assenza od incompletezza del setto , ecc . ) erano signi cativamente differenti nella popolazione . 
 the thorax has proved very useful in several forensic cases because of the remarkable number of features offered by this area and the wide availability of chest x - rays in the population [ 17 ]  . 
 [ 19 ] , in a study using thoracic x - rays , measured the reliability of the visual comparison , established useful features for identi cation process and evaluated possible sources of error . 
the most important source of error proved to be torace il torace un distretto importante per lidenti cazione personale , per la presenza di un elevato numero di caratteristiche morfologiche utilizzabili , nonch per lampia disponibilit di radiogra e toraciche come materiale am nella popolazione generale [ 17 ]  . 
 [ 19 ] condussero uno studio simile su radiogra e del torace , con lo scopo di quanti care laf dabilit del confronto visuale e mettere in evidenza le caratteristiche utili nel processo identi cativo , veri cando anche le possibili fonti di errori . 
 [ 27 ] , and the skeletal features considered to be most useful were the same in both studies . abdomen and pelvis the abdomen and pelvis maintain their anatomical position in the case of an accident , and the complex morphology of vertebrae is useful for identi cation purposes . 
in 1997 , valenzuela reported on a case of identi cation conducted through comparison of lumbar x - rays , emphasising the usefulness of vertebral osteophytes , of the unique shape of transverse and spinous processes , of vertebral - body trabecular patterns , scoliosis and other features [ 23 ]  . 
however , until now , no quantitative study has been conducted on these districts . arms and legs identi cation from a single bone is based on the observation of anomalous development , degenerative disease , tumours , prostheses , trabecular patterns and so on . 
an example of morphological analysis of bone features in the identi cation process is given by dean et al . , who by simulating a comparison between ctitious antemortem and postmortem material using preand postsurgical radiographs of the ankle succeeded in achieving a positive identi cation [ 34 ]  . 
 the features reported to be useful in this research study compare well with those reported in other studies ( bone shape , trabecular bone pattern , shape of radio - opaque and translucent features and degenerative changes ) [ 4 , 36 ]  . 
la pi importante fonte di errore riguardava la qualit dellimmagine radiogra ca : brogdon [ 6 ] consider anche la posizione del cadavere nelle immagini radiogra che pm come unimportante fonte di errore . 
nel 1997 , valenzuela [ 23 ] riport un caso di identi cazione personale effettuata tramite il confronto di radiogra e del distretto lombare , tramite de nizione del pro lo degli osteo ti vertebrali , e la comparazione delle forme uniche dei processi trasversi e spinosi , del disegno trasecolare del corpo vertebrale , delle curve scoliotiche ed altre caratteristiche [ 23 ]  . 
 arti superiori ed inferiori lidenti cazione da un solo osso basata sullosservazione di caratteristiche morfologiche riguardanti un anomalo sviluppo , malattie degenerative , tumori , protesi , disegno trabecolare , ecc . 
 [ 34 ] , che simularono un confronto fra materiale am e pm ttizio utilizzando lastre radiogra che pree post - chirurgiche di anca , con un risultati positivi [ 34 ]  . 
 [ 3 ] pubblicarono un articolo riguardante il confronto visivo di radiogra e della mano ed osservarono che gli operatori con minima esperienza erano meno abili nel processo identi cativo degli operatori pi esperti in tale ambito . 
le caratteristiche registrate come utili allidenti cazione in tale studio coincidono con quanto riportato da altri autori ( forma dellosso , disegno trabecolare osseo , forma delle caratteristiche radiopache e radiotrasparenti e modicazioni degenerative ) [ 4 , 36 ]  . 
laccuratezza del metodo 966 discussion the discovery and development of x - ray technology has given a great contribution to the improvement of medicine and forensic sciences , with x - ray examinations being admitted in court very early after the discovery of x - rays [ 6 ]  . 
the importance of x - ray examination in forensic practice is also supported by developments in the eld of virtopsy and the application of increasingly advanced techniques to forensic cases [ 37 ]  . 
virtopsy involves the use of imaging techniques such as ct and mri to visualise the morphology and lesions of inner viscera and bones and obtain large amounts of information without invasive procedures . 
in addition , the importance of the radiological approach in forensics is demonstrated by its widespread use in cases of child physical abuse , where ascertaining the presence of signs of recent and past trauma is mandatory [ 38 , 39 ]  . the use of radiology in personal identi cation leads to several advantages . 
firstly , x - ray examination is the most common diagnostic test in clinical practice and therefore usually the most frequent antemortem source of information when there is a presumed identity . 
in addition , the same radiograph with the same characteristics of an antemortem x - ray examination can be performed on the unidenti ed corpse , and this means a more reliable comparison between antemortem and postmortem data . 
at the present time , few forensic centres own x - ray and ct equipment , even though odonnell and woodford [ 40 ] suggest that in the next 510 years , most centres will either gain access to ct facilities or install the equipment in their own laboratories . 
the most important limitation , however , consists in the reliability of x - ray imaging , which is widely debated by different authors , especially in the eld of the analysis and description of lesions . 
different authors have in fact remarked that ct and x - ray examinations can detect only a limited percentage of skeletal traits or lesions if compared with the evidence gained from autopsy or after maceration of bones [ 4143 ] , especially in speci c skeletal districts such as the vertebrae [ 44 ]  . 
the issue of precision and accuracy of x - ray technologies is a relevant point of debate and should be analysed in depth to ascertain whether such technologies are reliable in personal identi cation . although reliable , every identi cation procedure based on x - ray technologies similar to other morphological radiol med ( 2011 ) 116 : 960968 presenta una elevata dipendenza dalloperatore , ma lo studio propone una valutazione numerica di tale confronto . 
 discussione la scoperta e lo sviluppo della tecnologia dei raggi x ha dato un grande contributo allo sviluppo della medicina e delle scienze forensi ; infatti molto presto dopo la scoperta dei raggi x gli esami radiogra ci furono ammessi in tribunale [ 6 ]  . 
limportanza dellindagine radiogra ca nella pratica forense provata anche dallo sviluppo crescente registrato nel campo della virtopsy e dallapplicazione di tecnologie sempre pi avanzate ai casi forensi [ 37 ]  . 
la virtopsy nel dettaglio riguarda luso delle tecniche di diagnostica per immagine come la tac e la rmn per la visualizzazione della morfologia e di eventuali lesioni degli organi interni e delle ossa , allo scopo di raggiungere un maggiore numero di informazioni senza utilizzare procedure cruente . 
inoltre , limportanza dellapproccio radiologico provata anche dalla sua diffusione come fondamentale test diagnostico nel caso di abusi sici su bambini , ove laccertamento della presenza di segni di traumatismi recenti e pregressi di fondamentale importanza [ 38 , 39 ]  . luso della radiologia nel campo dellidenti cazione personale comporta numerosi vantaggi ; prima di tutto , gli esami radiogra ci costituiscono il test diagnostico pi comune nella pratica clinica , e pertanto costituiscono la pi frequente forma di informazioni am qualora sia presente un sospetto didentit . 
inoltre , le stesse proiezioni radiogra che del materiale am possono essere ottenute anche sul cadavere da identi care , con una conseguente elevata af dabilit del confronto fra i dati am e pm . 
al momento , gli istituti di medicina legale in possesso di macchine radiogra che o addirittura di strumenti tac sono pochi , anche se odonnell e woodford [ 40 ] suggeriscono che nei prossimi 510 anni la maggior parte degli istituti di medicina legale potr installare tali macchinari nei propri laboratori . 
diversi autori infatti osservano che le tac e le radiogra e classiche possono identi care solo una percentuale limitata di tratti e lesioni scheletriche , se comparate con le stesse percentuali evidenziate durante lautopsia o dopo macerazione delle ossa [ 4143 ] , specialmente in speci ci distretti vertebrali quali le vertebre [ 44 ]  . 
al momento il tema della precisione ed accuratezza dellindagine radiogra ca un punto cruciale di dibattito e dovrebbe essere approfondito per veri care la sua reale af dabilit nel campo dellidenticazione personale . ogni procedura radiogra ca basata su tecnologia radioradiol med ( 2011 ) 116 : 960968 methods for comparing antemortem and postmortem data suffers from a lack of literature data on mean error and the threshold for distinguishing between a correct and an incorrect match . 
in other words , although all skeletons are different , nothing can be said as to how different two skeletons are and how many common radiological features between two bones are needed to con rm a positive identi cation . 
if these limitations are overcome , the easy readability and widespread use of x - rays technology will lead to a heightened role of forensic radiology in the dif cult and crucial issue of personal identi cation . 
 gra ca , cos come per altri metodi morfologici di confronto fra i dati am e pm , sebbene af dabile , soffre della mancanza di dati disponibili in letteratura riguardanti lerrore medio e il livello soglia utile per distinguere unidenti cazione positiva . 
in altre parole , sebbene ogni scheletro sia diverso da qualsiasi altro , nulla pu essere stabilito su quanto due scheletri siano differenti , e quante caratteristiche radiologiche in comune fra due ossa siano suf cienti per confermare unidenti cazione positiva . 
un aiuto in tal senso pu derivare da studi sperimentali condotti su un ampio numero di radiogra e , allo scopo di trovare unindicazione numerica utile a distinguere i confronti con esito positivo ed i confronti con esito negativo . 
 se tali limiti saranno superati , la facile leggibilit e lampia diffusione della tecnologia dei raggi x determiner una crescente importanza della radiologia forense nel dif cile , eppure importante , campo dellidenti cazione personale . 
knauth springer - verlag , berlin heidelberg , 2010 isbn 978 - 3 - 540 - 79879 - 8 e - isbn 978 - 3 - 540 - 79886 - 6 doi 10.1007 / 978 - 3 - 540 - 79886 - 6 published online : 7 march 2011 springer - verlag 2011 this second edition of a well known book is intended to provide the reader with all the most updated information in the rapidly evolving eld of virtual colonoscopy . there are 17 chapters dealing with all the problems and important items the radiologist or more speci cally the colonographer needs when confronting this peculiar and important diagnostic tool . an in depth discussion is devoted to performing , properly evaluating and nally correctly reporting the ndings of a virtual colonoscopy examination . 
in this respect , importance is given to patient preparation ( cathartic drugs are not easily accepted ) , fecal tagging , use of contrast medium , proper computed tomography ( ct ) parameters and dose reduction , plus data interpretation . all of the above are important points , considering that virtual colonoscopy as a screening tool for colonic cancer is strongly advocated by the authors and important international cancer , radiologic and endoscopic societies . in order to avoid pitfalls or devastating consequences for the patient in case of missed lesions all throughout the book the importance of training in virtual colonoscopy image review and evaluation is emphasized . a standard reporting system is advocated to describe the exact location of a suspected or detected lesion , including its appearance , shape , dimension and extension in order to serve as a reference - point for the endoscopist in case of concurrent examination or in view of future check - ups . 2d and 3d images , three transparency views and comquesta seconda edizione di un ben noto volume ha lo scopo precipuo di fornire al lettore le pi aggiornate informazioni in merito al settore in rapida evoluzione della colonscopia virtuale . i diciassette capitoli sono dedicati a tutti i problemi e gli importanti aspetti che il radiologo o meglio il colonradiologo ha bisogno di conoscere quando si confronti con questo importante e peculiare strumento diagnostico . una disamina approfondita dedicata allesecuzione , alla valutazione appropriata ed in ne alla corretta refertazione di quanto riscontrato durante lesecuzione di una colonscopia virtuale . 
sotto questo punto di vista molta importanza deve essere posta nella preparazione del paziente ( le sostanze purganti non sono molto gradite ed accettate ) , alla marcatura delle feci ( fecal tagging ) , alluso del mezzi di contrasto , ai corretti parametri di tomogra a computerizzata ( tc ) per riduzione della dose nonch allinterpretazione dei dati . tutti i punti sopra indicati sono importanti , tenuto anche conto che la colongra a virtuale fortemente indicata quale strumento di screening del cancro del colon sia dagli autori che da importanti societ internazionali di radiologia , endoscopia e per lo studio dei tumori . 
 lungo tutto il volume viene enfatizzata limportanza della preparazione e della pratica necessarie nella revisione e valutazione delle immagini ottenute con la colonscopia virtuale allo scopo di evitare errori o conseguenze devastanti per il paziente nelleventuale mancato riconoscimento di lesioni . viene dunque perorata la creazione di un sistema standard di refertazione per la descrizione dellesatta localizzazione di una lesione sospetta o riconosciuta , completata dalla descrizione del suo aspetto , forma , dimensione ed estensione , tale da servire da punto di riferimento certo per lendoscopista in caso di concomitante indagine endoscopica o in vista di successivi controlli . 988 radiol med ( 2011 ) 116 : 987988 puter aided detection ( cad ) are the bread and butter of virtual colonoscopy . 
in fact virtual colonoscopy reading is time - consuming due to the attention and effort required and one should evaluate no more than six examinations in a session , in order to avoid mistakes and when there are doubts , review by more than one expert radiologist is mandatory . the references are up todate in all chapters ( up to 2008 ) and one 2009 reference is included in chapter 16 . 
 this is an important and impressive book , enriched by an enormous amount of perfectly reproduced images , a must have book for radiologists , endoscopists and surgeons who understand , as stated above , that virtual colonoscopy is a very important diagnostic and screening tool when in the proper hands , or a mouse - trap and source of devastating errors in the hands of others . immagini 2d e 3d , immagini tridimensionali in trasparenza e la diagnosi assistita dal computer ( computer aided detection , cad ) sono il pane quotidiano della colonscopia virtuale . 
in effetti la lettura di un esame di colonscopia virtuale implica una notevole quantit di tempo a causa dellattenzione richiesta e chi referta non dovrebbe superare la soglia di sei esami per seduta , allo scopo di evitare errori : in ogni caso , quando esistano dubbi , si rende necessaria la revisione da parte di pi di un esperto radiologo . le voci bibliogra che sono aggiornate in tutti i capitoli no al 2008 ed una riferita al 2009 inclusa nel capitolo 16 ; tuttavia la loro presentazione discordante : in ordine alfabetico nella maggior parte dei capitoli ; di citazione in altri . 
ciatto published online : 28 july 2011 springer - verlag 2011 b3 core biopsies should be assumed as positive ndings for accuracy purposes le biopsie percutanee b3 dovrebbero essere assunte come reperti positivi nella valutazione di accuratezza corte c brus 1g , 37067 valeggio sul mincio ( vr ) , italy , tel . : + 39 - 348 - 6540748 , e - mail : stefano.ciatto@gmail.com sir , gentile direttore , the paper by luparia et al . 
apart from uncommon pathological gures , such as b3 high prevalence ( 23.6% as compared to 9 - 10% average literature gures ) and a subsequent low positive predictive value ( ppv , 4.2% as compared to 25 - 30% average literature gures ) , or a null ppv for a few b4 cases , i would like to comment on the criteria adopted to assess vab accuracy . 
in particular , assuming b3 ndings as negative is uncommon , as they are currently assumed as positive in the literature [ 2 , 3 ] and usually referred for surgical con rmation [ 3 ]  . 
however , since they still referred to surgery 83% of b3 cases , it seems conrmed that b3 were dealt with as suspicious cases , that means positive for accuracy assessment purposes . 
a parte alcune caratteristiche isto - patologiche non usuali della casistica , come una elevata prevalenza di lesioni b3 ( 23 , 6% rispetto al 9 - 10% mediamente riportato in letteratura ) , un conseguente basso valore predittivo positivo ( ppv ) dei casi b3 ( 4 , 2% rispetto al 25 - 30% mediamente riportato in letteraura ) , e un ppv nullo per un numero limitato di lesioni b4 , mi lascia dubbioso il criterio adottato per la valutazione della accuratezza di vab . 
laver assunto le diagnosi b3 come negative non comune , dal momento che i b3 sono generalmente considerati positivi in letteratura [ 2 , 3 ] e avviati alla conferma chirurgica [ 3 ]  . 
ammetto che sussiste un dibattito sulla possibilit di individuare un sottogruppo di b3 che possano essere solo controllati nel tempo , come certi sottotipi istologici speciali ( lesioni papillari e radial scar ) e / o i b3 senza atipie , e comprendo anche che gli autori , visto il basso vpp dei loro casi b3 , abbiano scelto di discutere collegialmente la necessit di chirurgia in questi casi , ma il fatto che abbiano poi concluso per linvio al chirurgo nell83% dei casi conferma che hanno gestito i casi b3 come sospetti , e positivi per quanto riguarda laccuratezza diagnostica . 
questo soprattutto se gli autori vogliono confrontare i loro risultati con quelli di altri studi ( cosa che riportano in una tabella ad hoc ) che hanno considerato i b3 come positivi . 
ovviamente gli autori possono discutere uno scenario ipotetico nel quale i b3 non vengono mai avviati al chirurgo , consistente con una sensibilit del 94 , 9% e una speci cit del 98 , 3% . 
houssami n , ciatto s , bilous m et al ( 2007 ) borderline breast core needle histology : predictive values for malignancy in lesions of uncertain maligmnat potential ( b3 )  . 
ciatto s , houssami n , ambrogetti d et al ( 2007 ) accuracy and understimation of malignancy of breast core needle biopsy : the florence experience of over 400 consecutive biopsies . 
knauth springer - verlag , berlin heidelberg , 2010 isbn : 978 - 3 - 540 - 78449 - 4 e - isbn : 978 - 3 - 540 - 78450 - 0 doi 10.1007 / 978 - 3 - 540 - 78450 - 0 published online : 7 march 2011 springer - verlag 2011 the aim of this 209 page / 13 chapter book is to introduce all the technical details , opportunities and problems related to the use of digital mammography ( dm ) to the reader . 
 since its introduction about a decade ago , dm has represented a real breakthrough in the diagnostic eld of mammography due to its capabilities in daily work ow , image viewing and storage and ease of communicating these parameters . 
 hints on problems in image processing and in diagnosis when comparing images taken with different digital mammography equipments over time , conventional lm mammography or images taken in different locations with different equipments are presented and discussed . 
 results of clinical trials performed in the usa and europe are taken into account and discussed at length , as well as the impact of visibility and appearance of mammographic signs of malignancy . further improvements in dm , inherent to contrast - enhanced dm , digital breast tomosynthesis and breast computed tomography ( ct ) are discussed in the last two chapters . 
 a long yet incomplete two plus page list of abbreviations intendimento di questo volume , nei suoi 13 capitoli e 209 pagine , di presentare al lettore tutti i dettagli tecnici , le possibilit ed i problemi legati allimpiego della mammogra a digitale ( md )  . dalla sua introduzione , circa una diecina di anni fa , la md ha rappresentato un vero passo in avanti nel campo della diagnostica mammogra ca date le sue potenzialit nella attivit di lavoro giornaliera , le possibilit di valutare ed archiviare le immagini e la facilit di comunicazione di questi parametri . 
 vengono presentati e discussi suggerimenti sui problemi correlati con il trattamento delle immagini e con la diagnosi , quando se ne confrontino serie riprese nel tempo con differenti tipi di attrezzature mammogra che , con pellicole convenzionali oppure immagini ottenute in altre sedi con attrezzature diverse . chi si occupa di md dovrebbe essere preparato a studiare sia la sica che le tecniche proprie della metodica in modo tale da ottenere immagini corrette e che rispettino dei ben precisi criteri di qualit . 
una discussione approfondita dedicata a questi argomenti come anche a problemi pratici come lorganizzazione della sala referti e la sua illuminazione . vengono presi in considerazione e discussi a fondo i risultati di ricerche cliniche svoltesi negli stati uniti ed in europa come pure limpatto rappresentato dalla visibilit ed aspetto dei segni mammogra ci di malignit . 
 negli ultimi due capitoli vengono discussi ulteriori miglioramenti della md insiti nella stessa con aumento di contrasto , la tomosintesi digitale e la mammo - tomogra a computerizzata ( tc )  . 
as advocated in a previous book review it would be advisable to have this list of abbreviations on some loose or hard bound pages to have on hand , to be used ( very often ) in translation of abbreviations . the authors , all well known in their eld of research and daily work , have produced a book which will be of help to all those who are using or will be using dm in the future , to provide the best diagnostic results in the endless ght against breast cancer . una lunga , eppure non completa lista di abbreviazioni ( due pagine e linizio di una terza ) , apre il volume . 
come gi segnalato in una precedente recensione sarebbe consigliabile il poter avere disponibili su pagine separate e mobili , rigide o non , tali elenchi di abbreviazioni da poter utilizzare ( molto spesso ! ) nella traduzione delle stesse . 
 gli autori , tutti ben conosciuti nel loro campo di ricerca e lavoro quotidiano , hanno prodotto un libro che sar di aiuto a tutti coloro che gi usano o useranno in futuro la md , in modo tale da offrire i migliori risultati diagnostici nella lotta senza ne contro il cancro della mammella . 
gourtsoyiannis department of radiology , university hospital of heraklion , medical school of crete , 71110 stavrakia , heraklion , crete , greece department of rheumatology , university hospital of heraklion , medical school of crete , heraklion , crete , greece 3department of preschool education , university of crete , greece correspondence to : e . 
le immagini sono state valutate per la presenza e lestensione di intrappolamento daria , per il coinvolgimento delle vie aeree ( bronchi / bronchioli ) ed il modello hrct dominante . 
la differenza di attenuazione tra le regioni dintrappolamento daria in espirazione e le stesse regioni in inspirazione aveva un range compreso tra 32 e 89 unit di houns eld ( hu )  . 
the nonsigni cant correlation between at extent and inspiratory ndings may suggest at as an additional hrct nding in patients with wg . keywords wegeners granulomatosis bronchiolectasis air trapping risoluzione era patologica in 19 pazienti ( 90 , 4% ) e rappresentata dai seguenti modelli polmonari principali : nodulare , cavitario / non cavitario ( n = 7 , 38 , 9% ) , opacit a vetro smerigliato ( ggo ) ( n = 5 , 26 , 3% ) , masse ( n = 3 , 15 , 8% ) , modello brotico ( n = 3 , 15 , 8% ) e consolidativo con broncogramma aereo ( n = 1 , 5 , 3% )  . 
le regioni dintrappolamento daria nella granulomatosi di wegener , rappresentano un nuovo reperto , indiretto e probabilmente , in rari casi , lunico reperto di coinvolgimento polmonare rilevato in tc ad alta risoluzione . 
la correlazione non statisticamente signi cativa tra lestensione dellintrappolamento daria ed i reperti in fase inspiratoria possono suggerire lintrappolamento daria come un ulteriore reperto nella tc ad alta risoluzione in pazienti con granulomatosi di wegener . 
 parole chiave granulomatosi di wegener bronchiolettasia intrappolamento daria introduction first described by friedrich wegener in the late 1930s , wegeners granulomatosis ( wg ) is a rare systemic autoimmune disorder characterised histologically by a necrotising granulomatous vasculitis that most commonly involves the lungs , nasal pathways , paranasal sinuses and kidneys , but may affect any organ system [ 13 ]  . 
the disease traditionally belongs to the group of diffuse interstitial lung diseases that , according to a recent classi cation , has been renamed diffuse parenchymal lung diseases [ 4 ]  . 
it follows a chronic relapsing course , and the respiratory tract is the most commonly involved syste upper respiratory tract disease is reported in up to 90% and lung involvement in 7090% of patients [ 5 ]  . 
the disease involves the subglottic part of the airways , mainly the trachea and the main bronchi , causing bronchial wall thickening and airway lumen stenosis [ 1 , 2 ]  . 
 the primary aim of this study was to document the inspiratory high - resolution computed tomography ( hrct ) patterns and airway involvement as well as expiratory ndings in patients with known wg . 
disease assessment consisted of documenting the presence and extent of air trapping ( at ) on expiratory hrct scans and correlating it with the inspiratory hrct patterns and with the extent of bronchial and bronchiolar involvement , as studied on deep inspiratory and deep expiratory chest hrct images . materials and methods patients between april 1999 and january 2009 , 23 consecutive patients , 14 women and 9 men with an age range between 18 and 72 ( mean 45 ) years were retrospectively studied . 
twenty - one of these patients were newly diagnosed with wg , whereas two had been diagnosed 7 and 8 years , respectively , before the hrct scans were performed . 
two of these patients were active smokers ( mean 20 pack - years ) and 860 radiol med ( 2011 ) 116 : 858867 were excluded from the study , whereas among the remaining 21 patients , two were former smokers having ceased smoking 7 and 10 years , respectively , before the study began . 
at the time of examination , all 21 patients presented with a positive serum titre for anticytoplasmic antibodies ( canca ) , whereas 12 of them were positive for anti - pr3 antibodies . the clinical diagnosis of wg was established in accordance with the 1990 american college of rheumatology criteria [ 6 ] and the chapel hill criteria [ 7 ]  . 
transbronchial biopsy was performed in four patients , video - assisted thoracoscopy ( vat ) in two , open lung biopsy in one , renal biopsy in seven , nasal mucosa biopsy in four and skin and subcutaneous tissue biopsy in three . 
in each patient , sequential inspiratory scanning sequences were acquired at 10 - mm intervals from the level of the lung apices to below the costophrenic angles , and expiratory hrct scans were acquired with a 20 - mm interval . 
all images were reconstructed using a high - spatial frequency reconstruction algorithm . two experienced chest radiologists independently examined the hrct images in random order and recorded the presence and extent of ndings by visual assessment . 
expiratory scans were studied rst in order to avoid any bias in the interpretation of areas of at documented on expiration from the identi cation of inspiratory ndings , such as nodules and airway involvement . 
 on inspiration , the scans were visualised at two different window settings : one appropriate for lung parenchyma ( width 1 , 400 / level ; 700 hu ) and one ( width 1 , 000 / level ; 600 hu ) for scoring slight attenuation differences in the lung parenchyma . 
 the predominant parenchymal pattern nodules and masses ( cavitated or not ) , ground - glass opacities , consolidation areas and honeycombing as a sign of lung brosis was evaluated on inspiratory hrct scan . 
the presence or absence of bronchial and bronchiolar wall thickening was assessed considering that the wall thickness of conducting bronchi and bronchioles of < 5 mm in calibre should normally measure one sixth to one tenth of their diameter [ 8 ]  . 
hence , in every patient with suspected airway wall thickening , we calculated the ratio between the bronchial wall thickness ( t ) and total diameter of the bronchus ( d ) , which in normal individuals is 0.2 , or 20% , on average [ 9 ]  . 
 to assess possible airway dilation , a comparison was made between the internal diameter of the bronchus and the diameter of the adjacent pulmonary artery branch measured at sea level [ 10 ]  . 
to this end , we calculated the bronchoarterial ratio , de ned as the ratio between the bronchial luminal diameter ( l ) and the diameter ( d ) of its accompanying artery . 
a bronchoarterial ratio > 1 was considered typical of bronchiectasis , as was visualisation of a bronchus within < 2 cm of the costal pleura or abutting the mediastinal pleura . 
according to the nomenclature committee of the fleischner society , at is a pathophysiological term that indicates the retention of excess air in all or part of the lung at any stage of expiration [ 11 ]  . 
to assess the presence or absence of at , small regions of interest ( rois ) 12 cm in diameter including at least 95 pixels each were drawn freehand to measure the attenuation difference in houns eld units between areas of low attenuation on expiration and corresponding areas on inspiration . 
b hrct eseguita in espirazione allo stesso livello presenta delle zone dintrappolamento daria distribuita a carta geogra ca in ambedue le basi polmonari . at extent was classi ed as lobular when composed of hypoattenuation areas corresponding to fewer than three adjacent secondary pulmonary lobules in one or two regions per lung level , as segmental when corresponding to a pulmonary segment or three or more adjacent secondary pulmonary lobules , and as lobar when the hypoattenuation area was more extended than a pulmonary segment . 
in patients showing multiple at patterns , the most extensive one ( lobar rather than segmental ; segmental rather than lobular ) was taken in consideration [ 12 , 13 ]  . subsequently , the extent of at areas was evaluated by visual assessment using a semiquantitative scoring system estimating the percentage of lung that appeared abnormal on each scan [ 14 ]  . 
 [ 16 ] , was used to estimate at on expiratory scans in three different lung elds for each lung to a total of six lung elds for both lungs : upper lungs elds , from the lung apices to just above the level of the carina ; middle lung elds between the level of the carina and the pulmonary veins ; inferior lung elds from the pulmonary vein level to the level of the diaphragat each level and for each lung , a 5 - point scale was used to estimate the percentage of at extent visible to each radiologist : 0 for no at ; 1 for at between 1% and 25% of the cross - sectional area of the affected lung ; 2 for at between 26% and 50% ; 3 for at from 51% to 75% ; 4 for at between 76% and 100% [ 1416 ]  . 
more speci cally , the mann whitney and kruskalwallis tests were used to examine statistically signi cant differences between two mean values or among three or more mean values , respectively . 
the aim of the analyses was to correlate the extent of at on expiration with the predominant inspiratory hrct pattern and its total extent on inspiration as well as with airway involvement . 
 according to the 5 - point scale used for at extent , two patients ( 9.5% ) scored 0 , 16 ( 84.2% ) scored 1 , three ( 14.3% ) scored 2 and none scored 3 or 4 . 
at areas were observed in all six lung elds ( three for each lung ) and were distributed : bilaterally in the lower lung elds in all seven patients ( 100% ) , in the upper lung elds in four ( 51.7% ) and in the middle lung elds in three ( 42.9% ) ; in two , the radiol med ( 2011 ) 116 : 858867 fig . 
in our study group , the attenuation difference between inspiration and expiration ranged from 32 to 89 hu ( mean 6023.5 hu ) , whereas the attenuation measurements in the adjacent normal parenchyma ranged between 710 hu and 885 hu ( mean 795.461.7 hu ) on inspiratory scans and from 640 hu to 775 hu ( mean 69558.9 hu ) on expiratory scans , with a difference between inspiration and expiration that ranged from 100 hu to 250 hu . 
it is important to mention that none of the patients exhibited wall thickening of the trachea or the main bronchi , as commonly mentioned in literature [ 13 , 9 ]  . 
spearmans correlation coef cient between right and left lung at scores was statistically highly signi cant ( r = 0.97 , p < 0.01 ) , indicating that at was diffusely distributed . 
4 inspiratory chest high - resolution computed tomography ( hrct ) scan at the level of the right main bronchus shows thickening of the bronchial wall of the right upper lobar bronchus and its posterior and apical branches . 
4 hrct del torace in inspirio al livello del bronco principale di destra evidenzia ispessimento della parete bronchiale del bronco lobare superiore di destra e dei suoi rami posteriori e apicali . 
b nella nestra per parenchima polmonare la massa circoscritta da opacit a vetro smerigliato ( tc halo sign , che indica emorragia polmonare ) 864 radiol med ( 2011 ) 116 : 858867 fig . 
the disease affects about 3 : 100 , 000 people men and women equally and can occur at any age ( mean 41 years ) and , in comparison with other vasculitides , the lung is the most commonly affected organ , with a very aggressive airway pathology and chronic relapsing course [ 17 , 18 ]  . 
 in contrast to the well - described pulmonary parenchymal involvement in wg , the lower airway disease manifestations are less well recognised by clinicians , and little is known from the literature [ 2123 ]  . 
in the study by travis et al . , open lung biopsy was performed in 67 patients with wg , and a variety of bronchial / bronchiolar lesions were noted , including acute and chronic bronchiolitis ( 51% and 64% , respectively ) , follicular bronchiolitis ( 28% ) and bronchiolitis obliterans ( 31% )  . 
in other studies , small airway abnormalities in wg were characterised as unusual manifestations , including bronchiectasis and peribronchial thickening [ 2528 ]  . interestingly , no patient in our study had tracheal or main bronchial involvement . 
it is worth mentioning that all patients who presented with mild dyspnoea , dry cough , haemoptysis and inspiratory or expiratory wheezing had bronchial and bronchiolar involvement on inspiratory scans . 
based on these results , hrct appears to be capable of demonstrating segmental , subsegmental , bronchial and bronchiolar involvement in patients with wg , and the small airways may also be affected . 
 in normal individuals who are nonsmokers and have no history of exposure to organic or inorganic substances , the attenuation difference increases on expiratory hrct by about 150 hu compared with inspiratory scans [ 15 , 29 ]  . 
it is well known that areas of at show signi cantly less attenuation increase on expiration than in 866 radiol med ( 2011 ) 116 : 858867 normal lung , combined with a lack of volume reduction in these areas [ 30 ]  . 
usually , an attenuation increase of < 80 hu between inspiration and expiration may be indicative of at , so that comparison between inspiratory and expiratory ct scans may be helpful when at is subtle or diffuse [ 30 , 31 ]  . 
the most frequent at distribution pattern was segmental ( n = 4 , 19% ) , which together with the lobar pattern ( n = 1 , 4.7% ) are reported to be pathological and highly suggestive of small - airway disease [ 12 , 13 ]  . 
the probability of these at areas being pathological is higher if we consider that none of these patients was a smoker or suffered from asthma or chronic obstructive pulmonary disease . 
this con rms the diffuse involvement of lung parenchyma due to vasculitis , which is a systemic in ammatory disease , and this explains the geographical distribution of at areas . 
and include : ( a ) parenchymal necrosis , ( b ) vasculitis and ( c ) granulomatous in ammation accompanied by an in ammatory in ltrate composed of a mixture of neutrophils , lymphocytes , plasma cells , histiocytes and eosinophils [ 22 ]  . 
our hypothesis concerning the at nding is that it may be related to endoluminal formation of granulomas as well as to abnormal thickening of the bronchial and bronchiolar walls , causing bronchiectasis and bronchiolectasis and consequently at . 
 this hypothesis clearly needs to be veri ed . finally , the mean values of the total extent of at areas showed no statistically signi cant difference ( p > 0.005 ) between the predominant patterns on inspiratory hrct scans , such as pulmonary nodules , masses , ground - glass opacities , honeycombing and consolidation areas and the extent of airway involvement , including bronchial and bronchiolar wall thickening and the bronchiectasis and bronchiolectasis recorded in these patients . conclusions hrct in wg patients on deep inspiration may present various ndings , such as nodules , ground - glass opacities , consolidation areas and honeycombing . 
especially in the absence of inspiratory ndings , the presence of at may unveil pulmonary involvement in wg , playing an important role in the therapeutic approach to these patients . 
passariello1 1department of radiological sciences , university of rome sapienza , v.le regina elena 324 , 00161 rome , italy 2department of thoracic surgery , university of rome sapienza , rome , italy 3department of nuclear medicine , university of rome sapienza , rome , italy correspondence to : f . 
sono stai determinati i valori di accuratezza , sensibilit , speci cit , valore predittivo positivo ( ppv ) e valore predittivo negativo ( npv ) della tc - ds in confronto alla scintigra a perfusionale : 0 , 88 , 0 , 84 , 0 , 90 , 0 , 93 e 0 , 88 , rispettivamente . 
la tc - ds si presenta accurata e promettente , radiol med ( 2011 ) 116 : 842857 keywords lung cancer perfusion scintigraphy dualsource computed tomography lung perfusion fornendo importanti informazioni di natura funzionale sul polmone . parole chiave tumore del polmone scintigra a perfusionale tc a doppia sorgente radiogena perfusione del polmone introduction introduzione the indication for surgical intervention in patients with from lung cancer is based on both the cancer stage and patients clinical condition . 
when planning the surgical procedure , in particular if this is to be heavily destructive ( pneumonectomy , segmentectomy or lobectomy ) , preliminary pulmonary function tests are needed to obtain a predictive evaluation of the patients haemodynamic and ventilation tolerance [ 1 ]  . 
lung cancer patients candidate for surgical intervention are therefore evaluated in terms of two closely related aspects : morphology and function . computed tomography ( ct ) represents the gold standard in morphological characterisation , localisation and staging of lung cancer , and it is often supported by pulmonary function tests ( pft ) and ventilation / perfusion scintigraphy to measure parenchymal function . 
furthermore , it allows no direct comparison with morphological changes , and it exposes patients to an additional dose of radiation . the new dual - source ct ( dsct ) scanners , equipped with a dual x - ray source , exploit the different attenuation of iodine detectable at different energies and can consequently provide functional information based on the distribution of contrast material during its rst passage through the pulmonary capillary network . 
commercially available software provides both qualitative and quantitative information about iodine distribution and hence about regional perfusion by generating false - colour maps in which areas of the lung parenchyma with different degrees of perfusion appear in different colours ranging from white - yellow ( high degree of perfusion ) to blue - purple ( low degree of perfusion ) [ 57 ]  . 
in addition , integration with the automated study of the distribution of air volumes inside the lung parenchyma and areas of emphysematous change provides information regarding the extent of functional lindicazione allintervento chirurgico nei pazienti affetti da cancro del polmone viene valutata sia in base allo stadio della neoplasia , sia in base alle condizioni cliniche del soggetto . 
nella piani cazione di un intervento chirurgico , in particolare se ampiamente demolitivo , ( pneumonectomia , segmentectomia o lobectomia ) , necessario uno studio funzionale preliminare del parenchima polmonare al ne di effettuare una valutazione predittiva della tolleranza emodinamica e ventilatoria del paziente [ 1 ]  . 
 la tomogra a computerizzata ( tc ) rappresenta il gold standard nel processo di caratterizzazione morfologica , localizzazione e stadiazione del tumore polmonare ; essa viene af ancata dalle prove di funzionalit respiratoria e dalla scintigra a perfusionale polmonare per la valutazione dello stato funzionale del parenchima . 
attualmente , nella maggior parte dei centri di riferimento per la chirurgia del polmone , alle normali prove spirometriche viene infatti associata la valutazione scintigra ca nei pazienti che devono essere sottoposti ad interventi di pneumonectomia o resezioni polmonari ampie . 
il limite principale della tecnica scintigra ca rappresentato , tuttavia , da una limitata risoluzione spaziale e da una conseguente ridotta accuratezza nellindividuazione topogra ca di aree fotopeniche a distribuzione regionale . 
non inoltre possibile effettuare un confronto diretto con le alterazioni morfologiche e sottopone il paziente ad una ulteriore dose di radiazioni . le nuove apparecchiature tc denominate dual - source ( tc - ds ) , dotate di una doppia sorgente radiogena , sono in grado di sfruttare il differente potere di attenuazione dello iodio rilevabile a diverso voltaggio ; questo permette , quindi , di ottenere informazioni funzionali derivate dalla distribuzione del mezzo di contrasto ( mdc ) iodato in corrispondenza della fase di primo passaggio nella rete capillare polmonare . 
 la diffusione commerciale di software dedicati consente di ottenere informazioni sia qualitative che quantitative sulla distribuzione dello iodio e quindi sul grado di perfusione regionale con lelaborazione di mappe di falsi colori , in 844 radiol med ( 2011 ) 116 : 842857 ventilatory impairment [ 810 ]  . the purpose of our study was to determine the diagnostic potential of dsct in assessing pulmonary function in lung cancer patients who are candidates for surgical intervention . 
 data obtained with dsct were then compared with results of perfusion scintigraphy and pft . materials and methods patient selection and study design over a period of 6 months , we recruited 12 patients ( eight men and four women ; mean age 58.37 years ) with biopsyproven lung cancer ( maximum mean transverse diameter of the main lesion 64 cm ) who were candidates for possible surgical intervention . 
after approval from the local ethics committee and patients written consent informed had been obtained , patients were studied by dsct and lung perfusion scintigtable 1 disease stage for patients included in the study patient no . 
 stadio cui le zone di parenchima polmonare con differente grado di perfusione assumono tonalit cromatiche differenti in un range che va dal bianco - giallo ( elevato grado di perfusione ) no al blu - viola ( basso grado di perfusione ) [ 57 ]  . 
lintegrazione con lo studio automatizzato della distribuzione dei volumi aerei allinterno del parenchima polmonare e delle aree con compromissione en sematosa , consente , inoltre , di fornire informazioni per una valutazione del grado di danno funzionale ventilatorio [ 810 ]  . lo scopo del nostro studio stato quello di determinare le potenzialit diagnostiche della tc - ds nella valutazione funzionale del polmone nei pazienti affetti da patologia neoplastica polmonare candidati ad intervento chirurgico ; i dati ottenuti con la tc - ds sono stati confrontati con i risultati della scintigra a perfusionale e con le prove di funzionalit respiratoria . materiali e metodi selezione dei pazienti e progetto di studio durante un periodo di 6 mesi sono stati reclutati 12 pazienti ( 8 uomini , 4 donne ; et media : 58 , 37 ) con una neoplasia polmonare confermata mediante esame bioptico ( diametro trasverso massimo medio della lesione principale : 64 cm )  . 
dopo approvazione del comitato etico locale e sottoscrizione di un consenso informato , i pazienti sono stati sottoposti ad uno studio tc - ds e ad una indagine di scintigra a perfusionale polmonare ad una distanza temporale massima di 5 giorni . 
tutti i pazienti hanno inoltre eseguito le prove di funzionalit respiratoria con spirometria . protocollo tc lesame tc stato eseguito utilizzando una apparecchiatura dual source ( siemens somatom de nition , enlargen , germania )  . 
lacquisizione , condotta secondo un protocollo denominato dual energy , viene effettuata attraverso lutilizzo simultaneo di due tubi radiogeni a differente voltaggio , uno ad 80 kv ( in grado di ricoprire un campo di vista [ fov ] di 26 , 5 cm ) ed uno a 140 kv ( fov di 50 cm ) , con i seguenti parametri tecnici per entrambi : tempo di rotazione 0 , 33 secondi ; collimazione 0 , 6 mm ; spessore di strato 1 , 53 mlamperaggio viene variato utilizzando un protocollo care dose con quality reference impostato a 8 mas per il tubo a 140 kv e 340 mas per il secondo tubo . 
lapplicazione del protocollo care dose permette di ridurre i valori di mas somministrati senza perdita nella qualit dellimmagine : la corrente del tubo viene automaticamente ridotta in quelle posizioni angolari dove il radiol med ( 2011 ) 116 : 842857 raphy over a maximum period of 5 days . 
all patients also underwent pft with spirometry . diametro del paziente , e quindi i valori di attenuazione , sono minori [ 11 ]  . ct protocol ct exams were performed with a dual - source scanner ( siemens somatom de nition , erlangen , germany )  . 
scans were acquired with a dual - energy protocol , which relies on the simultaneous use of two x - ray tubes operated at different voltages : one at 80 kv ( fov 26.5 cm ) and one at 140 kv ( fov , 50 cm )  . 
the technical parameters were as follows : rotation time 0.33 s ; collimation 0.6 mm ; slice thickness 1.53 mmilliamperage was varied by using the care dose protocol with quality reference milliampere set at 8 mas for the 140 - kv tube and 340 mas for the 80 - kv tube . 
application of the care dose protocol reduces milliampere with loss of image quality : tube current is automatically reduced in the angular positions where the diameter of the patient and consequently the attenuation values are smaller [ 11 ]  . a dose of 70 cc of iodinated contrast material was administered at a high ow rate ( 5 cc / s ) , followed by 40 cc of saline solution at the same ow rate . 
synchronisation of ct acquisitions with the passage of contrast agent through the pulmonary circulation was achieved with the bolus - tracking technique ( care bolus ) : a circular region of interest ( roi ) was placed over the pulmonary artery to measure changes in attenuation values from the time of contrast administration ; the scan ( which lasted 56 s approximately ) was started when the contrast agent reached the vessel and the threshold attenuation value of 100 hu was achieved , with an additional 6 - s delay . 
to determine the stage of disease , a second , singleenergy scan was acquired of the chest , abdomen , pelvis and skull during the venous phase after administration of a second bolus of contrast material ( 60 cc at 3 cc / s ) with an additional 40 - s delay . 
 starting from the data set acquired with the dual - energy technique , two groups of images were produced : one with high - resolution reconstruction kernel ( b60 for the study of the lung parenchyma and one with a lower resolution kernel , b30 , for the study of soft tissues such as mediastinum and vascular structures )  . 
all studies were transferred to a workstation and processed using dedicated software . scintigraphy protocol all examinations were obtained with an in nia dual - head sono stati somministrati ad alta velocit di usso ( 5 cc / s ) 70 cc di mdc organo - iodato per ogni paziente , seguiti da un bolo di soluzione siologica di 40 cc alla stessa velocit di usso . 
la sincronizzazione temporale dellacquisizione tc con il passaggio del mdc a livello del circolo polmonare stata effettuata con tecnica di bolus tracking ( care bolus ) : una regione di interesse ( roi ) circolare viene posizionata da un operatore sullarteria polmonare per misurare le variazioni dei valori di hu dal momento della somministrazione del mdc ; la scansione ( della durata di circa 56 secondi ) inizia quando il mdc giunge nel vaso e viene raggiunto un valore soglia di 100 hu , con un ritardo ulteriore di 6 secondi . 
in tal modo lacquisizione viene effettuata in una fase di primo passaggio del mdc nel circolo polmonare : in tale fase vascolare si assiste alla opacizzazione esclusiva del circolo arterioso polmonare . 
ai ni del completamento della stadiazione tumorale , stata effettuata una seconda scansione ( a singola energia ) di torace , addome , pelvi e cranio in fase venosa , dopo somministrazione di un secondo bolo di mdc ( 60 cc a 3 cc / s ) con un ritardo aggiuntivo di 40 secondi . 
 a partire dai dataset acquisiti in doppia energia , sono stati prodotti due gruppi di immagini : uno con ricostruzione ad alta risoluzione per lo studio del parenchima polmonare ( denominato b60 ) ed uno a pi bassa risoluzione per lo studio dei tessuti molli ( mediastino e strutture vascolari , b30 )  . 
gli studi sono stati quindi trasferiti su work station dedicate ed elaborate mediante software ai ni del presente studio . protocollo della scintigra a lesame stato eseguito con apparecchiatura in nia a doppia testa ( ge ) , con collimatore low energy - high resolution dopo somministrazione di un valore dose - attivit di circa 185 mbq ( corrispondenti a circa 5 mc ) di microaggregati di albumina ( maa ) marcati con 99mtc . 
sono state eseguite sei proiezioni standard ( anteriore , posteriore , obliqua destra e sinistra , laterale destra e sinistra ) in un tempo complessivo per paziente variabile fra 10 e 12 minuti . 
 lacquisizione di tutte le proiezioni ha richiesto circa 800 kcounts ( 800.000 colpi ) , utilizzando una energia pari a 140 kev ( con nestra del 20% : range tra 126 e 154 )  . protocollo della spirometria tutti i pazienti hanno eseguito al momento del ricovero una spirometria di base con valutazione dei volumi dinamici : volume espiratorio massimo ( fev1 ) , forced vital capacity 846 radiol med ( 2011 ) 116 : 842857 camera ( ge ) , with low - energy , high - resolution collimator after administration of an activity value of approximately 185 mbq ( equivalent to 5 mc approximately ) of 99mtclabelled macroaggregated albumin ( maa )  . 
acquisition of all projections required approximately 800 kcounts using a 140 kev energy ( with 20% window ; range 126154 )  . ( fvc ) , forced expiratory ow ( fef ) 25%75% . i pazienti che assumevano terapia broncodilatatoria domiciliare hanno eseguito lindagine dopo la somministrazione dei farmaci al ne di effettuare le prove nelle migliori condizioni del paziente e riprodurne le condizioni cliniche di base allingresso in reparto ( dipendenti dalla somministrazione domiciliare dei farmaci broncodilatatori ) [ 12 , 13 ]  . elaborazione degli studi tc con software dedicati spirometry protocol analisi degli studi tc - ds perfusionali all patients underwent initial spirometry with measurement of dynamic volumes [ forced expiratory volume in 1 s ( fev1 ) , forced vital capacity ( fvc ) , forced expiratory ow rate ( fef2575% ) on admission to hospital . 
patients receiving home bronchodilator therapy underwent spirometry after drug administration so they could do the test in the best possible condition and reproduce their condition on admission , which depended on home bronchodilator use [ 12 , 13 ]  . ct postprocessing with dedicated software analysis of dsct perfusion studies evaluation of lung parenchyma perfusion was done on the basis of the dual - energy chest scans reconstructed with the b30 kernel ; data sets were transferred and processed using commercially available software ( siemens dual energy , syngo 2006g , siemens medical solutions )  . 
this scoring system was applied on both the dsct and scintigraphic studies . images were evaluated by two experienced chest radiologists ( ff , 11 years of experience , and cc , 15 years ) in a blinded fashion in order to measure interobserver variability . 
four weeks later , the images were re - evaluated with the same scoring system and the same software by one of the radiologists to measure intraobserver variability . la valutazione perfusionale del parenchima polmonare stata effettuata a partire dagli studi del torace acquisiti in doppia energia e ricostruiti con algoritmo di ricostruzione b30 ; i dataset sono stati trasferiti ed elaborati con un software commercialmente disponibile fornito dalla casa produttrice ( siemens dual energy , syngo 2006g ; siemens medical solutions )  . 
 gli studi sono stati valutati da due esperti radiologi toracici in cieco ( ff , 11 anni di esperienza , cc , 15 anni ) al ne di valutare il livello di variabilit inter - osservatore . 
un radiologo a distanza di 4 settimane ha rivalutato le immagini con lo stesso sistema di scoring , applicando nuovamente lanalisi del software di perfusione al ne di valutare il livello di variabilit intra - osservatore . analisi degli studi tc per la valutazione dei volumi polmonari e del grado di en sema i dataset acquisiti in singola energia ( 140 kv ) e ricostruiti con algoritmo ad alta risoluzione per il parenchima polmonare ( b60 ) sono stati trasferiti su una apposita consolle ed elaborati con un applicativo del programma syngo ( siemens , inspace 4d , lung parenchymal analysis ) , in grado di fornire radiol med ( 2011 ) 116 : 842857 fig . 
1a - c studio perfusionale del parenchima polmonare con tc dual - source : lindagine dimostra multipli difetti di perfusione su un piano sagittale ( a ) , coronale ( b ) e assiale ( c ) , riferibili al quadro bronco - en sematoso del paziente in studio . 
 analysis of ct studies in evaluating lung volumes and extent of emphysema the data sets acquired with the single - energy technique ( 140 kv ) and reconstructed with high - resolution kernel for lung parenchyma ( b60 ) were transferred to a dedicated workstation and processed using a syngo application ( siemens , inspace 4d , lung parenchyma evaluation ) , which automatically calculates values of lung volume and extent of emphysema ; this process does not require a dual - energy study . 
due medici nucleari in consensus hanno valutato le immagini scintigra che identi cando e registrando su una tabella i lobi ipoperfusi secondo il sistema di scoring utilizzato per immagini tc - ds . radiol med ( 2011 ) 116 : 842857 software . 
the scintigrams were evaluated in consensus by nuclear medicine physicians who identi ed and entered on a table the hypoperfused lobes using the scoring system used for the dsct images . analisi statistica statistical analysis statistical analysis was performed with a statistical software package ( spss 13 for macintosh ; spss , chicago , il , usa )  . 
agreement was considered poor for kappa values of 0.210.40 , fair for values of 0.410.60 , good for values of 0.610.80 and excellent for values of 0.811.00. results the mean duration of ct scans was 73 min , including patient preparation and positioning . 
the radiation dose delivered to the patient , calculated as dose - length product ( dlp ) in milligray per centimetre and displayed on the ct console for each patient , had a mean value of 305.429.6 , which is similar to values reported in the literature [ 14 , 15 ]  . 
in particular , as shown in table 2 , of a total of 60 lobes studied , the dsct evaluation reported the absence of perfusion defects in four lobes assessed as hypoperfused at scintigraphy . 
the values of regional lung air content derived from the automatic calculation provided by the ct software and lanalisi statistica stata interamente condotta con un software statistico dedicato ( spss 13 per macintosh ; spss , chicago , ill )  . 
i valori di accuratezza diagnostica , sensibilit , speci cit , valore predittivo positivo ( ppv ) e valore predittivo negativo ( npv ) sono stati calcolati utilizzando come reference standard la scintigra a perfusionale . 
 inoltre , la presenza o assenza di difetti perfusionali rilevati allesame di tc - ds stata confrontata con la presenza o assenza del medesimo reperto alla scintigra a perfusionale tramite il test di mcnemar . 
linter - reader agreement tra i due lettori e lintra - reader agreement tra le due letture di tc - ds , effettuate dal radiologo con maggiore esperienza , sono stati studiati tramite la di cohen . 
lagreement stato giudicato scarso per valori di = 0 , 210 , 40 , moderato per valori di = 0 , 410 , 60 , buono per valori di = 0 , 610 , 80 ed eccellente per valori di = 0 , 811 , 00 . risultati la durata media degli esami tc stata di circa 73 minuti , comprensivi di preparazione e posizionamento del paziente . 
la dose di radiazioni somministrata al paziente , calcolata come dose length product ( dlp ) in mgy per centimetro e riportata dalla tc per ogni paziente , ha presentato un valore medio di 305 , 429 , 6 , sovrapponibile a quelli riportati in letteratura [ 14 , 15 ]  . in tabella 2 sono riportati i dati delle valutazioni qualitative della scintigra a perfusionale e della tc - ds . 
i valori di accuratezza diagnostica , sensibilit , speci cit , ppv e npv della tc - ds nella valutazione qualitativa dei livelli di perfusione sono stati di 0 , 88 , 0 , 84 , 0 , 90 , 0 , 93 e 0 , 88 , rispettivamente . 
in particolare , come mostrato in tabella 2 , su un totale di 60 lobi studiati , la valutazione tc - ds ha riportato lassenza di difetti di perfusione in quattro lobi valutati invece come ipoperfusi alla scintigra a . 
the curves have a reverse trend : the higher the extent of emphysema , the lower the level of fev1 and vice versa . the mcnemar test showed no statistically signi cant difference ( p = 0.09 ) in the identi cation of patients with emphysema . 
 complete agreement was obtained between the rst and second reading by the same radiologist both in the evaluation of perfusion defects and of areas of emphysematous change . discussion spirometrici sono riportati nelle tabelle 3 e 4 . 
il gra co in figura 4 mostra la correlazione tra il grado di en sema e i valori spirometrici ( fev1 ) ; landamento delle curve risulta inverso : maggiore il grado di compromissione en sematica minore il livello di fev1 riportato e viceversa . 
il test di mcnemar non ha evidenziato differenze statisticamente signi cative ( p = 0 , 09 ) nellindividuazione dei pazienti con compromissione en sematosa . linter - reader agreement tra i due lettori nella valutazione della presenza di un difetto di perfusione allesame di tc - ds risultata eccellente ( = 0 , 92 ) ; un risultato analogo stato evidenziato per la valutazione della presenza di compromissione en sematosa ( = 0 , 94 )  . 
una completa concordanza stata ottenuta tra la prima e seconda lettura da parte dello stesso radiologo sia per la valutazione dei difetti di perfusione che per la valutazione delle aree con compromissione en sematosa . ct represents the modality of choice for the morphological evaluation and staging of lung cancer patients . 
these systems provide images of excellent technical and diagnostic quality within a few seconds , allowing imaging of most patients including discussione la tc rappresenta lesame di elezione nella valutazione morfologica e nella stadiazione del paziente con patologia tumorale del polmone . 
tuttavia , alcune informazioni de nite funzionali , rimangono appannaggio di valutazioni clinico - strumentali e della medicina nucleare , in particolare per ci che riguarda la valutazione della perfusione polmonare [ 24 ]  . 
the introduction of dedicated software in clinical practice has allowed us to obtain automatic reconstructions of lung perfusion on which a visual and qualitative analysis of possible hypoperfused areas may be carried out . the results of our study , con rmed by previous reports , millimetriche , in tempi di acquisizione pi rapidi rispetto alle macchine di precedente generazione . 
ci consente di ottenere studi con immagini di eccellente qualit tecnica e diagnostica in un tempo di acquisizione di pochi secondi , quindi effettuabili nella maggior parte dei pazienti , compresi quelli con severa patologia en sematosa o che necessitino di somministrazione di ossigeno permanente [ 16 , 17 ]  . lapplicazione di una doppia sorgente radiogena a differente voltaggio , con due sistemi di acquisizione disposti a 90 rispetto allasse di rotazione del gantry , consente di effettuare una discriminazione sica del tessuto in studio ed in particolare , nella nostra valutazione dello iodio presente durante la fase di primo passaggio del mezzo di 852 radiol med ( 2011 ) 116 : 842857 fig . 
3a - d evaluation of lung perfusion by dual - source computed tomography ( dsct ) and scintigraphy in a patient with lung cancer : both methods show a segmental perfusion defect surrounding the neoplasm ( localised in the basalposterior segment of the right lower lobe ) in a coronal and sagittal plane ( a , c ) in the dsct study and on a posteroanterior projection in the scintigraphic evaluation ( d )  . 
3a - d confronto tra lo studio perfusionale con tc dual - source e scintigra a in un paziente con adenocarcinoma del polmone : entrambe le indagini evidenziano un difetto di perfusione segmentale nella zona periferica della lesione localizzata nel segmento basale - posteriore del lobo inferiore di destra , apprezzabile su un piano coronale e sagittale in tc - ds ( a , c ) ed in proiezione postero - anteriore nello studio scintigra co ( d )  . 
in b si evidenzia un difetto ventilatorio in sede perilesionale . demonstrate that dual - energy ct is an accurate and reproducible technique that can easily be applied in all patients [ 16 , 17 ]  . 
as a result , the contrast agent must be administered at a high ow rate ( > 4.5 cc / s ) to enable detection of a large quantity of iodine inside the pulmonary circulation during the short acquisition time and at a high concentration to obtain more intense and homogeneous enhancement with a small quantity ( 6070 cc approximately per study )  . indeed , a major problem in software - mediated perfusion studies is related to the presence of beam - hardening artefacts at the level of the superior vena cava or of the subclavian and brachiocephalic veins . 
lintroduzione nella pratica clinica di software dedicati consente di ottenere ricostruzioni perfusionali automatizzate del parenchima polmonare su cui effettuare una valutazione visivo / qualitativa di eventuali aree ipoperfuse . i risultati del nostro studio , confermati anche in precedenti valutazioni , hanno dimostrato che lutilizzo della tecnica a doppia energia rappresenta una metodica accurata , riproducibile e di facile applicazione in ogni paziente [ 16 , 17 ] ; tuttavia necessario sottolineare alcuni rilevanti accorgimenti tecnici . 
la perfusione polmonare con tc - ds infatti basata sulla visualizzazione , con ricostruzioni basate su mappe di falsi colori , del passaggio del mdc attraverso la rete capillare polmonare . 
in primo luogo , pertanto necessario che il mdc iniettato sia : somministrato ad alta velocit di usso ( > 4 , 5 cc / s ) , cos da consentire nel breve tempo dacquisizione dellesame il rilevamento di radiol med ( 2011 ) 116 : 842857 table 4 top : mean values derived from the automatic analysis performed by the software in the computed tomography ( ct ) evaluation of emphysema in a topographic approach for the 12 patients . 
the defect una elevata quantit di iodio allinterno del circolo polmonare ; il mdc deve essere ad alta concentrazione , per ottenere un grado di enhancement maggiore ed omogeneo ed in quantit limitata ( circa 6070 cc per studio )  . una delle problematiche pi rilevanti nel processo di 854 radiol med ( 2011 ) 116 : 842857 pft / dsct emphysema fev1 ct - emphysema fig . 
4 il gra co mostra landamento dei valori di fev1 rispetto a quelli riportati automaticamente dal software per il grado di compromissione en sematosa ( valori medi ) per ogni paziente ; landamento delle due curve inverso : laddove il valore di fev1 maggiore , minore il grado di compromissione en sematosa riportato e viceversa ( r = 0 , 657 ; p < 0 , 0001 )  . elaborazione degli studi perfusionali mediato dal software pu derivare , infatti , dalla presenza di artefatti da indurimento del fascio a livello della vena cava superiore o della vena succlavia e brachiocefalica . 
i pazienti affetti da bronco - pneumopatia cronica ostruttiva ( bpco ) , in particolare , possono presentare un tempo di circolo sanguigno signi cativamente rallentato , ed necessario , pertanto , somministrare il mezzo di contrasto in un volume ridotto per evitare che esso sia ancora presente in sede cavale superiore durante il tempo di acquisizione . 
nel nostro studio la tecnica a doppia energia ha erogato al paziente una dose sovrapponibile a quella per un normale studio angio - tc del torace a singola energia ( computed tomography dose index [ ctdi ] : 7 , 14 mgy / cm )  . 
nel nostro studio stato inoltre applicato , per ogni paziente , un protocollo care dose , mantenendo , comunque , un elevato livello di qualit diagnostica . in ne , necessario ricorrere allutilizzo di software di elaborazione dedicati , oggi commercialmente disponibili ed integrabili in consolle af ancate alle apparecchiature tc , per ottenere in maniera rapida elaborazioni delle immagini fig . 
5a , b artefatto da indurimento del fascio nella valutazione perfusionale tc : la presenza del mezzo di contrasto a livello della vena succlavia destra e della vena cava superiore ha reso mal valutabile il parenchima polmonare in sede apicale e paracavale . 
subsequent administration of a saline bolus compacts the contrast bolus and ushes any residual contrast responsible for the artefact . a second factor to be taken into account in performing dual - energy ct imaging concerns the radiation dose delivered to the patient . 
in our study , dual - energy ct delivered a dose almost equivalent to that of normal , single - energy chest ct angiography ( ct dose index 7.14 mgy / cm )  . 
 furthermore , in our study , we used a care dose protocol for all patients while maintaining a high diagnostic quality . lastly , dedicated processing software programmes , which are commercially available and can be integrated into ct workstations , are needed to obtain rapid , reproducible and easy - to - interpret postprocessed images . 
in our study , use of a dsct scanner allowed us to obtain images that were qualitatively very similar to the scintigrams , with the advantage of a higher spatial resolution and topographic de nition of perfusion defects at the level of the pulmonary parenchyma . the selection criteria for choosing candidates for pneumonectomy and lobectomy require an evaluation of respiratory function and consequently of possible defects due to the often associated chronic obstructive pulmonary disease . 
 our preliminary experience reveals a good correlation between data obtained from the automatic evaluation of the extent of emphysema and the functional tests , in line with previous reports [ 1820 ]  . 
this quantitative approach has been investigated in previous studies [ 2123 ] and is particularly useful for : collecting information on the treatment plan by indicating even small changes in parenchymal density undetectable at routine ct ; identifying areas with the most pronounced emphysematous changes that require treatment [ 8 ]  . the combination of morphological and functional both perfusional and ventilatory information afforded by dsct allows the technique to be indicated as the method of choice for managing lung cancer patients scheduled for surgery . 
nel nostro studio , lapplicazione di una apparecchiatura tc dual - source ha consentito di ottenere immagini qualitativamente sovrapponibili a quelle scintigra che , con il vantaggio di una maggiore risoluzione spaziale e di de nizione topogra ca dei difetti di perfusione a livello del parenchima polmonare . la valutazione dei criteri di selezione dei pazienti candidati ad intervento di pneumonectomia e di lobectomia necessita di una valutazione della funzionalit respiratoria e pertanto di eventuali de cit legati alla condizione di bpco spesso associata . 
la nostra esperienza preliminare evidenzia una buona correlazione tra i dati ottenuti dalla valutazione automatizzata del grado di en sema e le prove funzionali , rispecchiando quelle che sono le esperienze note nella letteratura [ 1820 ]  . 
 nel nostro studio abbiamo utilizzato un software in grado di effettuare automaticamente una analisi topograca e quantitativa dei volumi aerei polmonari e del grado di compromissione en sematosa del parenchima . 
in particolare , per la selezione delle aree en sematose , stato scelto come cut - off un range di valori densitometrici compreso tra - 951 e - 1024 uh . 
questo approccio di tipo quantitativo gi stato valutato in studi precedenti [ 2123 ] e si dimostrato particolarmente utile per : ottenere informazioni sullandamento del programma terapeutico evidenziando alterazioni densitometriche parenchimali anche lievi e non valutabili allesame tc di routine ; consentire lindividuazione delle aree con maggior grado di compromissione en sematosa distrettuale su cui praticare un eventuale trattamento [ 8 ]  . la combinazione delle informazioni morfologiche e di quelle funzionali perfusionali e ventilatorie ottenute con la tc dual - source , consente di indicare tale tecnica quale metodica unica nella gestione dei pazienti affetti da patologia neoplastica del polmone candidati alla chirurgia . 
non abbiamo trovato riscontro , inoltre , di nessuno studio precedentemente pubblicato che riportasse una valutazione comparativa tra le informazioni funzionali ventilatorie integrate con i dati di perfusione tc - ds , associata al calcolo automatico del grado di en sema e dei volumi polmonari regionali in pazienti affetti da tumore del polmone . 
 [ 22 ] , in una valutazione simile effettuata su pazienti fumatori affetti da en sema , hanno riportato una correlazione fra il grado di en sema misurato automaticamente ed i difetti di perfusione riscontrati a livello parenchimale ( p = 0 , 0355 ; r = - 0 , 54 ) [ 22 ]  . 
no previous published study has reported a comparative evaluation of ventilatory function data integrated with dsct perfusion data associated with the automatic determination of extent of emphysema and regional lung volumes in lung cancer patients . 
data derived from our preliminary experience are very encouraging and suggest that further studies should be conducted on a larger number of patients . a second limitation is that our study did not include any quantitative assessment of lung perfusion levels in a comparison between scintigraphy and dsct . 
this analysis was not possible owing to the limited fov ( 26.5 cm ) of the low - voltage tube , which caused exclusion from the analysis of a small portion of peripheral pulmonary parenchyma ( in particular at the basallateral level ) in a group of large - build patients ( 8 / 12 )  . 
that way , the overall diagnostic accuracy proved to be adequate , as patients with small perfusion defects at the level of the basal segments ( undetectable because of small fov ) had additional defects in other areas of the same lobe that were depicted by dsct . 
as discussed in previous studies [ 14 , 24 ] , there is as yet no solution to this proble the improvement and evolution of dsct scanners will help to overcome this limitation in the near future . a third limitation is that the scintigraphic studies included a standard acquisition of six projections rather than a single photon emission ct ( spect ) acquisition . 
one example is given by possible areas of atelectasis : in dsct perfusion studies , these appear as nonperfused during the rst passage of the contrast agent owing to peripheral vascular bundles , whereas they appear as regularly perfused on scintigraphy owing to delayed blood lling of the collapsed region . 
hence , for correct interpretation , perfusion studies must always be combined with evaluation of the morphological images . dati derivati dalla nostra valutazione preliminare appaiono molto incoraggianti per un proseguimento dello studio su un numero pi ampio di pazienti selezionati . in secondo luogo nel nostro studio non stata effettuata una valutazione di natura quantitativa dei livelli di perfusione polmonare in un confronto tra scintigra a e tc dualsource . 
questa analisi non stata possibile a causa del limitato campo di vista ( 26 , 5 cm ) del tubo a basso voltaggio , che ha determinato lesclusione dalla elaborazione di una piccola parte della regione periferica del parenchima polmonare ( in particolare a livello della regione basalelaterale dei polmoni ) in un gruppo di pazienti ( 8 / 12 ) di grossa corporatura . 
stato possibile superare questo limite tecnico attraverso una analisi di tipo visivo / qualitativo : in tal modo i livelli complessivi di accuratezza diagnostica sono risultati adeguati in quanto i pazienti che mostravano piccoli difetti perfusionali a livello dei segmenti basali ( non evidenziabili a causa del fov ridotto ) , riportavano difetti addizionali localizzati in altre sedi dello stesso lobo dimostrabili nello studio tc - ds . 
il miglioramento e levoluzione delle apparecchiature tc dual - source consentir , in un prossimo futuro , di superare questo ostacolo . terzo , gli studi scintigra ci effettuati comprendevano una acquisizione standard di 6 proiezioni piuttosto che una acquisizione tomogra a computerizzata a emissione di fotoni singoli ( spect )  . 
 nonostante questa possa essere riferibile alla effettiva perfusione polmonare nei soggetti sani , un ruolo diverso deve esserle af dato nella valutazione della perfusione dei soggetti con patologia distruttiva parenchimale . 
un esempio pu essere dato da una eventuale area di atelectasia : nello studio perfusionale con tc - ds essa si presenta non perfusa durante il primo passaggio del mezzo di contrasto a causa dellaffastellamento dei vasi periferici , mentre apparir regolarmente perfusa allesame scintigra co per via di un riempimento sanguigno pi tardivo della regione collassata . 
per una corretta interpretazione lo studio perfusionale deve , pertanto , essere sempre associato alla valutazione delle immagini morfologiche . nuove apparecchiature dual - source sono in fase di studio e saranno presto disponibili con un incremento dellamradiol med ( 2011 ) 116 : 842857 new dsct scanners are under investigation and will soon be available with increased width of the second integration with high - concentration contrast detector ; agents ( 500 mg / i ) will lead to a signi cant improvement in the diagnostic quality of the technique . in conclusion , dsct is an accurate and promising technique that provides important information on lung function . 
 piezza del secondo detettore ; lintegrazione con mdc ad elevata concentrazione ( 500 mg / i ) consentir un ulteriore miglioramento della qualit diagnostica della metodica . in conclusione , la tecnica tc con doppia energia si presenta accurata e promettente , fornendo importanti informazioni di natura funzionale sul polmone . 
guarise1 1struttura complessa di radiologia , ospedale san bassiano , bassano del grappa , italy 2struttura complessa di chirurgia vascolare , ospedale san bassiano , bassano del grappa , italy correspondence to : g . 
multihole microcatheters allow the thrombolytic agent to be distributed more evenly into the clot and may help to reduce reactive arterial spasm . keywords intra - arterial thrombolysis acute hand ischaemia urokinase microcatheter riassunto obiettivo . 
il microcatetere multiforato un utile supporto che permette una pi omogenea distribuzione dellagente trombolitico allinterno del coagulo e pu ridurre lo spasmo arterioso reattivo . parole chiave trombolisi intra - arteriosa ischemia acuta della mano urochinasi microcatetere 920 introduction acute hand ischaemia is an infrequent occurrence , and the clinical and therapeutic approach is still controversial [ 13 ]  . 
although a few case series of acute ischaemic lesions have been described in the literature , the series are small and do not allow for guidelines regarding the most appropriate therapeutic approach [ 4 , 5 ]  . 
furthermore , no study has as yet compared the results of surgical thrombectomy ( the gold standard in the treatment of thrombotic ischaemia ) [ 5 ] and intra - arterial thrombolysis ( an emerging , minimally invasive method with few local or systemic complications and with good results in other body regions ) [ 13 , 6 ] , nor has the use of multihole microcatheters been described in this particular region of the body . the purpose of this paper is to describe our initial experience in the treatment of acute ischaemic hand lesions with percutaneous intra - arterial thrombolysis with or without multihole microcatheters and compare the results with those available in the literature . materials and methods between march 2005 and may 2009 , three men ( mean age 39 years ; range 2648 years ) presented to the emergency department for acute hand ischaemia following an accidental intra - arterial injection of cocaine ( n = 1 ) or a traumatic event ( n = 2 )  . 
on clinical presentation , all three patients exhibited the typical clinical signs of acute ischaemia : nger pain , pallor , nail cyanosis , coldness , dysfunction , paraesthesia / dysaesthesia . 
preliminary doppler ultrasound ( us ) examination ( iu22 philips , philips healthcare , amsterdam , the netherlands ) con rmed the patency of the radial and ulnar arteries down to the wrist , with no ow signal in the affected digital arteries . all three patients subsequently underwent selective catheterisation of the humeral artery after antegrade access through the humeral artery ( n = 1 ) or retrograde access through the common femoral artery ( n = 2 ) using seldingers technique ( with a 18 - gauge needle cannula ; arterial introducer , radifocus introducer ii , 4 or 5 f , 10 cm , terumo corporation , tokyo , japan ) with placement of a diagnostic catheter ( bern imager ii , 4 or 5 f , 65 or 100 cm , boston scienti c , natick , ma , usa ) into the ipsilateral humeral artery . 
sono stati descritti in letteratura alcuni casi di lesioni ischemiche acute , ma le casistiche riportate sono limitate e non permettono una standardizzazione di linee guida riguardanti lapproccio terapeutico [ 4 , 5 ]  . 
inoltre a tuttoggi non stato compiuto alcuno studio comparativo riguardo i risultati della trombectomia chirurgica ( consolidata come gold standard di trattamento delle ischemie trombotiche ) [ 5 ] con la trombolisi endoarteriosa ( metodica emergente , poco invasiva , con ridotte complicanze sia locali che sistemiche e con buoni risultati gi documentati in altri distretti corporei ) [ 13 , 6 ] , n stato riportato luso di microcatetere multiforato in questo particolare distretto corporeo . scopo di questo lavoro riportare la nostra esperienza iniziale nel trattamento delle lesioni ischemiche acute della mano con trombolisi endoarteriosa percutanea senza o con microcatetere multiforato e confrontare i risultati con quelli della letteratura . materiali e metodi nel periodo compreso fra marzo 2005 e maggio 2009 tre pazienti maschi ( et media 39 anni , intervallo di et 2648 anni ) si sono presentati al pronto soccorso per lesione ischemica acuta della mano secondaria a iniezione accidentale endoarteriosa di cocaina ( 1 caso ) oppure post - traumatica ( 2 casi ) in un intervallo di tempo medio di circa 2 ore dallinsorgenza della sintomatologia acuta . 
alla presentazione clinica tutti e 3 i pazienti manifestavano i tipici segni clinici di ischemia acuta : dolore , pallore , cianosi ungueale , dita fredde , impotenza funzionale , parestesie / disestesie delle dita . 
allesame eco - color doppler preliminare ( iu22 philips , philips healthcare , amsterdam , olanda ) si confermava la perviet delle arterie radiale e ulnare no al polso , con assenza di segnali di usso arterioso a livello delle arterie delle dita interessate . tutti e 3 i pazienti sono stati quindi sottoposti a cateterismo selettivo dellarteria omerale , previo accesso arterioso omerale anterogrado ( 1 caso ) oppure arterioso femorale comune retrogrado ( 2 casi ) con tecnica di seldinger ( agocannula da 18 g ; introduttore arterioso radifocus introducer ii , 4 o 5 f , 10 cm , terumo corporation , tokio , giappone ) e posizionamento di un catetere diagnostico ( bern imager ii , 4 o 5 f , 65 o 100 cm , boston scienti c , natick , ma , usa ) in arteria omerale omolaterale . 
intra - arterial thrombolysis was performed by administering a bolus of urokinase ( crinos , milan , italy , 200 , 000300 , 000 iu ) , combined with a vasodilator ( verapamil , isoptin , knoll , 0.40.8 cc ) in all three cases . 
in the rst case , the procedure was completed with the administration of an intra - arterial bolus of 12 , 500 iu of heparin sodium ( epsoclar , hospira )  . results results are summarised in table 1 . 
in all of them , the arterial occlusion was distal ( ulnar artery , carpal arch ) or ultradistal ( metacarpal arteries , proper digital arteries )  . in all cases , urokinase thrombolysis without ( n = 1 ) or with ( n = 2 ) the microcatheter was completed with the administration of an intra - arterial vasodilator to prevent or treat a reactive spasm , with good angiographic and clinical results . the only local complication ( patient 1 ) , occurring 67 h later , was a haematoma at the site of arterial access resulting from the accidental puncture ( no us guidance ) of an ulnar artery originating from the brachial artery above the elbow joint ( anatomical variant )  . discussion acute hand ischaemia is an infrequent condition , and the few reports in the literature generally regard small case series of posttraumatic ischaemia [ 79 ] or larger series of patients with chronic kidney disease undergoing haemodialysis and with brescia - cimino arteriovenous stulas [ 4 , 10 , 11 ]  . 
nel 1 caso la procedura stata completata con somministrazione di eparina sodica ( epsoclar , hospira ) in bolo endoarterioso ( 12500 ui )  . risultati i risultati sono riassunti in tabella 1 . 
tutti e 3 i pazienti trattati erano maschi , giovani o relativamente giovani , con fattori di rischio traumatici o legati a tossicodipendenza ; nessuno di essi soffriva di insuf cienza renale cronica . 
in tutti e 3 i casi locclusione arteriosa era distale ( arteria ulnare , arcata arteriosa del polso ) o ultra - distale ( arterie metacarpali , arterie digitali proprie )  . il trattamento trombolitico con urochinasi senza ( 1 caso ) o con ( 2 casi ) microcatetere stato completato in tutti e 3 i casi con vasodilatatore intra - arterioso per prevenire / trattare uno spasmo arterioso reattivo , con buoni risultati angiogra ci e clinici . 
si veri cata come unica complicanza locale ( 1 caso ) dopo circa 67 ore un ematoma nel sito di accesso arterioso al braccio per puntura accidentale ( senza guida ecogra ca ) dellarteria ulnare che originava dallarteria brachiale al di sopra dellarticolazione del gomito ( variante anatomica )  . discussione lischemia acuta della mano condizione poco frequente con limitate esperienze riportate in letteratura , riguardanti casistiche generalmente piuttosto esigue ad eziologia posttraumatica [ 79 ] oppure casistiche pi ampie di pazienti in insuf cienza renale cronica in trattamento emodialitico portatori di stola artero - venosa ( a - v ) di brescia - cimino [ 4 , 10 , 11 ]  . 
le cause pi frequenti di ischemia acuta delle estremit distali della mano comprendono stenosi ed occlusioni arteriose distali ( trombotiche o emboliche ) su base aterosclerotica , post - traumatica ( attivit sportive o lavorative con microtraumatismi ripetuti ) [ 79 ] , embolica ( brillazione atriale , valvulopatia cardiaca ed endocardite , 922 radiol med ( 2011 ) 116 : 919931 radiol med ( 2011 ) 116 : 919931 924 radiol med ( 2011 ) 116 : 919931 lation , heart - valve disease and endocarditis , patent ductus arteriosus ) [ 112 ] , accidental intra - arterial introduction of chemical irritants ( drugs ) [ 1317 ] , anatomical abnormalities ( nerve - entrapment syndrome ) causing extrinsic compression [ 7 , 8 ] or arterial steal syndrome . the clinical presentation of acute hand ischaemia includes the typical symptoms and signs of acute ischaemia : nger pain , pallor , nail cyanosis , coldness , sensory and / or motor impairment of the ngers and , in dialysis patients , ischaemic ulcers . 
the differential diagnosis of acute hand ischaemia includes other similar clinical conditions unrelated to impaired arterial supply , such as venous hypertension , neuropathy ( diabetic , uraemic ) or carpal tunnel syndrome , and it is based on an appropriate and detailed history ( including occupational and sports activities ) , accurate physical examination , instrumental investigations such as pulse oximetry , doppler us , computed tomography ( ct ) or magnetic resonance ( mr ) angiography [ 18 ] and , possibly , digital subtraction angiography ( dsa )  . 
 in some reports , percutaneous intra - arterial thrombolysis [ 14 ] is or is not combined with percutaneous transluminal angioplasty ( pta ) [ 10 , 11 ] in cases of acute hand ischaemia ( table 2 ) , with associated vascular stenosis as the risk factor for decreased distal arterial blood ow , which increases the likelihood of thrombotic vessel occlusion . 
the patient populations described in the literature are generally small and heterogeneous , with the inclusion of patients with and without chronic kidney failure and different pharmacological or surgical treatments . 
among reports involving patients without chronic kidney failure treated with intra - arterial brinolysis , patient series ( 612 patients ) comprise various causes of arterial occlusion and , as in the report by widlus et al . 
 however , none of these reports have described the use of microcatheters for superselective catheterisation of the affected arteries . in our admittedly very small patients series , all three patients were relatively young and had no anatomical or familial risk factors for the condition ( there were no cases of chronic kidney failure or arteriovenous stula ) , and no subclinical stenoses requiring dilation ( table 2 )  . 
la diagnosi differenziale di una sindrome ischemica acuta della mano deve essere posta con altre condizioni cliniche simili , ma non associate a de cit dellapporto arterioso , quali ipertensione venosa , neuropatia ( diabetica , uremica ) o sindrome del tunnel carpale , e comprende una corretta e dettagliata anamnesi ( anche lavorativa e sportiva ) , un esame obiettivo accurato e , poi , indagini strumentali quali pulsossimetria , eco - color doppler , angio - tomogra a computerizzata ( tc ) o angiorisonanza magnetica ( rm ) [ 18 ] ed eventuale angiogra a digitale a sottrazione dimmagine ( dsa )  . 
 nel caso di eco - color doppler non diagnostico o dubbio , utile , per decidere la tipologia di trattamento , approfondimento diagnostico con studio angio - tc o angio - rm . 
 in alcuni lavori in letteratura la trombolisi percutanea endoarteriosa [ 14 ] viene associata o meno ad angioplastica transluminale ( pta ) [ 10 , 11 ] per il trattamento di lesioni ischemiche acute della mano ( tabella 2 ) con associata stenosi vascolare , che rappresenta la condizione predisponente ad una riduzione del usso sanguigno arterioso a valle , e , quindi , contribuisce ad aumentare la probabilit di occlusione trombotica del vaso stesso . 
tra quelle riguardanti pazienti senza insuf cienza renale cronica , trattati con terapia brinolitica intra - arteriosa , le serie riportate ( comprendenti da 6 a 12 pazienti ) contemplano cause differenti di occlusione arteriosa e , nel caso del lavoro di widlus et al . 
 [ 12 ] , luso di farmaci brinolitici differenti ( streptochinasi e urochinasi ) ; tuttavia , in nessuna di esse riportato luso di microcatetere per il cateterismo superselettivo delle arterie bersaglio . nella nostra casistica , numericamente molto limitata , tutti e 3 i pazienti erano relativamente giovani e non vi erano fattori anatomici o anamnestici favorenti ( nessuno dei pazienti era affetto da insuf cienza renale cronica , n portatore di stola a - v ) , n stenosi subcliniche meritevoli di eventuale trattamento dilatante associato ( tabella 2 )  . 
le cause identi cabili nella nostra casistica erano la microembolizzazione associata a radiol med ( 2011 ) 116 : 919931 926 radiol med ( 2011 ) 116 : 919931 radiol med ( 2011 ) 116 : 919931 fig . 
b angiography after intraarterial thrombolysis ( urokinase ) , vasodilator ( verapamil ) and heparthe angiogram shows partial restoration of patency of the proper digital arteries to the rst and second digits ( long arrow ) and a reactive spasm of the distal radial artery ( short arrows )  . 
langiogra a mostra parziale recupero della perviet delle arterie digitali proprie del 1 e 2 dito ( freccia lunga ) , e uno spasmo reattivo dellarteria radiale distale ( frecce corte )  . 
c langiogra a mostra lorigine prossimale dellarteria ulnare ( u ) e dellarteria radiale ( r ) dallarteria brachiale ( freccia )  . repeated microtraumas with consequent endothelial damage and superimposed acute thrombosis in the remaining two patients . the peculiarity of the upper limb arteries , which are medium to small in size and course fairly super cially , lies in their sensitivity to mechanical and chemical stimuli to which they respond sharply and immediately with spasms that may be very intense . 
therefore , brinolytic therapy for acute occlusions should involve the combination of the thrombolytic agent with a vasodilator in consideration of the spastic component always associated with such lesions in this anatomic region , in contrast to , for example , the lower limbs , where the reactive spasm is not constant . the type of arterial puncture is another crucial aspect for the outcome of treatment . 
whereas we initially ( patient 1 ) opted for direct antegrade puncture of the humeral artery , which is technically dif cult and not free of complications danno endoteliale da irritazione chimica , nel 1 caso , ed il microtraumatismo ripetuto con conseguente lesione endoteliale e trombosi acuta sovrapposta , nei rimanenti 2 casi . peculiarit delle arterie dellarto superiore ( di medio e piccolo calibro , piuttosto super ciali ) la particolare sensibilit agli stimoli sia meccanici che chimici , ai quali reagiscono vivacemente e subitamente con spasmi reattivi anche molto intensi . 
pertanto il trattamento brinolitico in caso di occlusione acuta , tenendo conto della componente spastica sempre associata in questo tipo di lesioni , dovrebbe contemplare lassociazione del trombolitico con il vasodilatatore , a differenza di altri distretti ( per esempio arti inferiori ) ove , invece , lo spasmo reattivo non sempre costante . il tipo di puntura arteriosa un altro punto cruciale ai ni del risultato del trattamento . 
a preliminary angiography shows occlusion of the palmar arch at the level of the fourth metacarpus ( long arrow ) and occlusion of the ulnar artery at the level of the carpus ( short arrow )  . 
 a langiogra a preliminare mostra occlusione dellarco palmare a livello del 4 metacarpo ( freccia lunga ) e occlusione dellarteria ulnare a livello del carpo ( freccia corta )  . 
d langiogra a nale mostra recupero della perviet dellarco palmare e recupero della perviet dellarteria ulnare distale ectasica ( freccia )  . ( leakage , haematoma , pseudoaneurysm , antegrade dissection , arteriovenous stula ) , in the two following cases , we performed conventional retrograde puncture of the common femoral artery at the groin using seldingers technique and selective catheterisation of the brachial artery . 
this latter technique is easier and better established , although it has the disadvantage of requiring very long catheters ( at least 150 cm ) to arrive as close as possible to the acute thrombotic lesion ( usually very distal )  . 
for this reason , in the last two cases , we used special multihole microcatheters for neuroradiological use ( micromewi , micro therapeutics , risma , dissezione anterograda , stola a - v ) , negli ultimi 2 casi , invece , siamo ricorsi alla puntura tradizionale retrograda dellarteria femorale comune allinguine secondo la tecnica di seldinger e cateterismo selettivo dellarteria brachiale interessata , tecnicamente pi facile e consolidata rispetto alla prima , ma con lo svantaggio di richiedere cateteri molto lunghi ( almeno 150 cm ) per poter arrivare il pi vicino possibile alla lesione trombotica acuta da trattare ( di solito molto distale )  . 
a preliminary angiography shows occlusion of the palmar arch at the level of the fourth and fth ngers ( long white arrow ) , occlusion of the distal ulnar artery ( short white arrow ) and occlusion of the digital arteries to the fourth nger and to the stump of the fth nger ( short black arrows ) b final angiography after intraarterial thrombolysis ( urokinase ) and vasodilator ( verapamil ) using a microcatheter . 
a langiogra a preliminare mostra occlusione dellarco palmare a livello del 4 - 5 dito ( freccia lunga bianca ) , occlusione dellarteria ulnare distale ( freccia corta bianca ) e occlusione delle arterie digitali del 4 dito e del moncone del 5 dito ( frecce corte nere )  . 
these are very thin ( 2.9 f ) and long ( 150180 cm ) , with multiple side holes and two radiopaque markers at the distal end , which can be used coaxially with a standard vertebral or multipurpose diagnostic angiography catheter ( 5 f )  . 
the microcatheters can be placed very distally into small - calibre arteries without causing reactive spasms that would risk invalidating or negatively in uencing the results of the intravascular thrombolysis procedure . 
in addition , they allow better distribution of the brinolytic agent over a larger area of the clot , thus reducing procedure time , patient and operator radiation exposure and brinolytic and vasodilator dose . the most widely used brinolytic drug in this type of procedure is urokinase , usually injected as an intra - arterial bolus at a dose of 100 , 000300 , 000 ui . 
to this we always added a ca2 + antagonist vasodilator ( verapamil , isoptin , knoll , 0.40.8 cc ) in a 1 : 10 dilution in order to prevent or treat the often associated reactive arterial spasms . 
in the two cases treated with a multihole microcatheter , the lower incidence of reactive arterial spasm in response to the passage of guidewires and catheters led to a signi cant reduction in the vasodilator dose . 
 the decision to combine an anticoagulant ( heparin ) as an intra - arterial bolus ( patient 1 ) derived from the hypothesis of a possible synergic effect with the thrombolytic agent , given the underlying chemicalembolic aetiopathogenesis . 
negli ultimi 2 casi con microcatetere multiforato si osservata minore incidenza di spasmo arterioso reattivo al passaggio di li guida e cateteri , conseguentemente una riduzione signi cativa della dose di farmaco vasodilatatore impiegato . 
 la scelta di associare un anticoagulante ( eparina ) in bolo endoarterioso ( 1 caso ) stata suggerita nellipotesi di un possibile effetto sinergico con lagente trombolitico , dato il particolare meccanismo eziopatogenetico chimico - embolico sottostante . 
leventualit di un successivo trattamento trombolitico endoarterioso in infusione lenta continua 930 radiol med ( 2011 ) 116 : 919931 tory , and the patient could be spared the risks of prolonged thrombolysis . in assessing the results , the radiological and clinical pictures need to be distinguished . 
in contrast to the lower limbs , where a good radiological outcome corresponds to a good clinical outcome and vice versa , in the upper limbs , there may be some discrepancy between the ndings , especially in extremely distal occlusions . 
even when the result of postprocedure angiography appeared suboptimal , we refrained from pursuing a better result because we realised that any improvement , even though suboptimal , of the arterial blood supply to the affected region was suf cient to guarantee a partial increase in perfusion with rapid and marked clinical improvements , immediate disappearance of the acute ischaemic symptoms and subsequent functional recovery . 
on the other hand , the appearance of reactive spasms in response to the mere passage of a guidewire or catheter is suf cient to cause occlusion or tight stenosis of a very small artery with the risk of jeopardising the entire procedure , as such spasms often are extremely resistant to vasodilator therapy . in our small case series , there were no systemic complications related to the thrombolytic drug ( such as haemorrhage ) or local complications ( such as dissections , vesselwall rupture , haemorrhage , haematoma )  . 
the only local complication was observed during an antegrade access to the humeral artery ( patient 1 ) and consisted of a haematoma in the access site due to accidental puncture of the ulnar artery , which had a high origin from the humeral artery in the middle third of the arm ( an anatomical abnormality also seen in patient 2 ) [ 20 ] , which required surgical repair . 
this complication could probably be prevented by performing the antegrade puncture under us guidance or , as was done in the two subsequent cases , retrograde catheterisation via the common femoral artery , provided that suf ciently long catheters are available ( 150 cm )  . one limitation of this study is the small number of cases , partially justi ed by the low frequency of the condition . 
anche quando il risultato angiogra co post - procedurale sembrava non ottimale , ci siamo astenuti dal perseguire un risultato migliore perch abbiamo constatato che un miglioramento , seppur non ottimale , della vascolarizzazione arteriosa nel distretto interessato era suf ciente a garantire un parziale aumento dellapporto arterioso con rapido e consistente miglioramento clinico , immediata scomparsa della sintomatologia ischemica acuta e successiva ripresa funzionale . 
come unica complicanza locale abbiamo , tuttavia , riportato , durante laccesso anterogrado allarteria omerale ( 1 caso ) , un ematoma nel sito di accesso arterioso percutaneo in seguito alla puntura accidentale dellarteria ulnare , che presentava unorigine alta dallarteria omerale al tratto medio del braccio ( anomalia presente anche nel caso 2 ) [ 20 ] , che ha richiesto raf a chirurgica . 
tale complicanza si poteva , probabilmente , evitare eseguendo la puntura anterograda sotto guida ecogra ca , oppure , come abbiamo poi fatto nei 2 casi successivi , eseguendo il cateterismo per via retrograda trans - femorale comune , purch siano disponibili cateteri suf cientemente lunghi ( 150 cm )  . tra i limiti di questo lavoro vi in primis lesiguit della casistica , in parte motivata dalla bassa frequenza della patologia considerata . 
it averts or at least reduces the need for surgical thrombectomy or more complex procedures for microvascular reconstruction , which have no doubt proved highly effective in numerous series , especially in posttraumatic or haemodialysis patients [ 5 , 19 , 21 , 22 ]  . the simplest approach with the lowest incidence of complications is retrograde access via the common femoral artery , with particularly long and thin catheters or , better , multihole microcatheters , given the very distal location of the ischaemic lesions . 
these provide the additional bene t of permitting better distribution of the thrombolytic agent and reducing the frequently associated reactive spasms , which can be prevented or treated by combining the brinolytic agent ( urokinase ) with the intra - arterial vasodilator . 
the clinical outcome is generally good , with rapid disappearance of the symptoms of acute ischaemia , even though the immediate radiological results are not always optimal . dellischemia acuta della mano , in quanto migliora il usso arterioso loco - regionale ed il run - off distale , evitando o comunque riducendo la necessit di ricorrere alla trombectomia chirurgica o a procedure pi complesse di ricostruzione microvascolare , che si sono dimostrate certamente valide in numerose casistiche , specie in pazienti post - traumatici o emodializzati [ 5 , 19 , 21 , 22 ]  . lapproccio pi semplice e meno gravato da complicanze quello transfemorale comune per via retrograda , con luso di cateteri o , meglio , di microcateteri multiforati particolarmente lunghi e sottili , in quanto le lesioni ischemiche sono spesso molto distali , con lulteriore vantaggio , da parte di questi ultimi , di consentire una migliore distribuzione dellagente trombolitico e ridurre lo spasmo arterioso reattivo molto spesso associato e prevenibile o trattabile associando al farmaco brinolitico ( urochinasi ) il vasodilatatore intra - arterioso . 
rotondo dipartimento di internistica clinica e sperimentale magrassi - lanzara , sezione di radiodiagnostica e radioterapia , seconda universit degli studi di napoli , p.zza miraglia 2 , 80138 napoli , italy correspondence to : g . 
la sostanziale sovrapposizione tra i parametri mammogra ci e ultrasonogra ci dei broadenomi e dei tumori lloidi e lassenza di caratteristiche patognomoniche non consentono di fare diagnosi differenziale tra i due istotipi . 
la cnb ecoguidata rappresenta un valido strumento nella diagnosi differenziale tra broadenoma e tumore lloide . parole chiave fibroadenoma ecogra a tumore lloide 906 introduction fibroadenoma is the most common benign breast disease in the female population aged 2050 years . 
the aetiopathogenetic factors underlying development of the mass remain unclear , even though the role of oestrogen and progesterone status is undeniable [ 1 ]  . when a broadenoma exceeds 5 cm in diameter , 500 g in weight or occupies more than four fths of the entire mammary gland , it is de ned as being a giant broadenoma . 
giant broadenomas , in particular in the juvenile variant , are perhaps the least common form , with an incidence < 4% of all broadenomas [ 2 , 3 ]  . 
despite the low incidence , however , these lesions are the most common cause of unilateral breast enlargement among teenagers . intralobular stroma also gives rise to phyllodes tumour , a neoplasm with a low incidence ( 0.31.0% of all breast neoplasms ; 23% of broepithelial neoplasms ) , which arises 1020 years later than broadenoma and is generally distinguished into benign or malignant according to its histopathological features . 
the aim of our study was to analyse the mammographic and ultrasonographic ( us ) features of broadenoma and phyllodes tumour and evaluate the diagnostic accuracy of mammography , us and us - guided core needle biopsy ( cnb ) in the differential diagnosis between broadenoma and phyllodes tumour . radiol med ( 2011 ) 116 : 905918 introduzione il broadenoma rappresenta la patologia mammaria benigna di pi comune riscontro nella popolazione femminile di et compresa tra i 20 ed i 50 anni di et ; considerate tutte le patologie della mammella , poi , seconda per incidenza in tutte le fasce det solo alladenocarcinoma . 
 quando un broadenoma supera i 5 centimetri di diametro , i 500 grammi di peso o occupa un volume superiore ai 4 / 5 dellintera ghiandola mammaria , si de nisce gigante . 
il broadenoma gigante , particolarmente nella sua variante giovanile , rappresenta forse la variante di pi rara osservazione , con unincidenza che non supera complessivamente il 4% di tutti i broadenomi [ 2 , 3 ] ; nonostante la bassa incidenza nella popolazione , per , tale lesione costituisce la pi comune causa di aumento volumetrico monolaterale della mammella in et adolescenziale . 
 dallo stroma intralobulare specializzato nasce anche il tumore lloide , neoplasia a bassa incidenza ( 0 , 3%1 , 0% di tutte le neoplasie della mammella , 2%3% delle neoplasie broepiteliali ) , che insorge 1020 anni pi tardi rispetto al broadenoma e che viene generalmente distinto in benigno e maligno in relazione alle caratteristiche anatomopatologiche . 
il tumore lloide presenta un elevato tasso di recidiva locale , nonch una percentuale non trascurabile di degenerazione maligna , motivi per i quali il trattamento di scelta della neoplasia rappresentato dallescissione chirurgica . pertanto , ai ni di un corretto approccio terapeutico , risulta indispensabile la diagnosi differenziale tra le suddette lesioni . 
each patient underwent breast examination , mammography , us , us - guided cnb and excision biopsy , all done by an experienced breast radiologist , which con rmed the presence of 67 broadenomas ( ten giant ) , and 16 phyllodes tumours ( 14 benign ; two malignant )  . 
 images were acquired in the two standard projections ( craniocaudal and mediolateral oblique ) , and spot - compresnel periodo compreso tra il 2001 e il 2008 sono state analizzate 83 lesioni di 83 donne dellet media di 45 , 4 anni ( range 1875 anni , deviazione standard 20 , 3 anni )  . 
ogni paziente stata sottoposta a visita senologica , a mammogra a , a esame ecogra co , a core needle biopsy ecoguidata e a biopsia escissionale che ha confermato la presenza di 67 broadenomi ( 10 dei quali giganti ) e 16 tumori lloidi , ( 14 benigni , 2 maligni )  . 
us was performed using a logiq s6 scanner ( ge healthcare , waukesha , wi , usa ) with a multifrequency matrix - array linear transducer ( 7 - 14 mhz )  . 
sonograms were assessed for the following parameters : diameter ( < 2 , 24 or > 4 cm ) , shape ( oval , rounded , lobular or multilobular ) , contours ( smooth or irregular ) , echogenicity ( hyper - , iso - , hypoechoic ) , echostructure ( homogeneous or heterogeneous ) and posterior acoustic changes ( none ; posterior shadowing ; posterior enhancement ) [ 5 ]  . 
 lesions were considered doubtful ( not broadenomas ) if they had a maximum diameter > 4 cm ( at mammography and us ) , high density ( at mammography ) , multilobulated and / or irregular contours ( at mammography and us ) , rounded shape ( at mammography and us ) and heterogeneous echogenicity with intralesional cystic areas ( at us ) [ 4 , 5 ]  . 
histological examination was performed by an experienced pathologist . statistical analysis we calculated the statistical signi cance of the frequency of the mammographic and us ndings in the differential diagnosis between broadenoma and phyllodes tumour . 
in order to assess the association between the mammographic and us ndings with phyllodes tumour and broadenoma , fishers exact test was performed on 22 tables and the fisherfreemanhalton test on rc tables ( statxact - 7 cytel studio version 7.0.0 21 oct 2005 )  . 
nellanalisi mammogra ca sono stati analizzati i seguenti parametri : forma , dimensioni , contorni , densit , presenza o assenza di calci cazioni o di halo sign [ 4 ]  . 
nellanalisi ecogra ca delle lesioni sono stati analizzati i seguenti parametri : diametro ( < 2 , compreso tra 2 e 4 o > 4 cm ) , forma ( ovale , rotonda , lobulata o plurilobulata ) , margini ( lisci o irregolari ) , ecogenicit ( iper - iso - ipoecogeno ) , ecostruttura ( omogenea o disomogenea ) e alterazioni della trasmissione del fascio ( assenza di alterazioni , attenuazione , accentuazione ) [ 5 ]  . 
sono state considerate dubbie ( non broadenoma ) le lesioni che presentavano : dimensioni massime > 4 cm ( alla mammogra a e allecogra a ) , alta densit ( alla mammogra a ) , pro li lesionali plurilobulati e / o irregolari ( alla mammogra a e allecogra a ) , morfologia rotondeggiante ( alla mammogra a e allecogra a ) ed ecogenicit disomogenea con areole cistiche intralesionali ( allecogra a ) [ 4 , 5 ]  . 
lanalisi istologica stata effettuata da un anatomopatologo dedicato . analisi statistica stata calcolata la signi cativit statistica della frequenza dei reperti mammogra ci ed ecogra ci nella diagnosi differenziale tra broadenoma e tumore lloide . 
per valutare lassociazione dei reperti mammogra ci ed ecogra ci con il tumore lloide e il broadenoma stato effettuato il test esatto di fisher per le tabelle 22 e il test esatto di fisherfreeman - halton nelle tabelle rc , statxact - 7 cytel studio version 7.0.0 ( 21 ottobre , 2005 )  . 
la signi cativit statistica stata calcolata con test di mc nemar . results risultati of the 83 lesions studied , 73 were palpable and ten nonpalpable ; of the 67 broadenomas , 61 were palpable and six nonpalpable ; of the 16 phyllodes tumours , 14 were palpable and two nonpalpable . 
at mammography , 89% of broadenomas appeared as low - density lesions relative to the surrounding parenchyma ( p = 0.0001 ) and only 11% as high - density lesions ; in contrast , 62% of phyllodes delle 83 lesioni analizzate , 73 erano palpabili , 10 non palpabili . 
alla mammogra a , l89% dei broadenomi si presentava come una lesione radiopaca a bassa densit rispetto al parenchima circostante ( p = 0 , 0001 ) e radiol med ( 2011 ) 116 : 905918 908 fig . 
in addition , 94% of broadenomas showed a halo sign ( p = 0.0001 ) , a nding that was seen in only 25% of phyllodes tumours ( table 1 )  . 
inoltre , il 94% dei broadenomi presentava halo sign ( p = 0 , 0001 ) , segno riscontrato soltanto nel 25% dei tumori lloidi ( tabella 1 )  . 
il 56% dei tumori lloidi aveva un diametro traverso massimo compreso tra 2 e 4 cm , il 44% ha un diametro > 4 cm , nessun tumore lloide aveva un diametro traverso massimo < 2 cm ( tabella 2 )  . 
on colour doppler us , no pattern of the spatial distribution of vessels could be identi ed that might help distinguish broadenomas from phyllodes tumours . calculation of the diagnostic accuracy of mammography , us and cnb compared with nal histology in the differential diagnosis between broadenoma and phyllodes tumour yielded the following results : sensitivity 45% for mammography ( range 3456% ) , 50% for us ( range 3961% ) and 81% for cnb ( range 7189% ) ; speci city 50% for mammography ( range 3961% ) , 69% for us ( range 5778% ) and 97% for cnb ( range 9099% ) ; posi49% isoecogeno , il 30% ipoecogeno , il 16% marcatamente ipoecogeno . 
lecostruttura del broadenoma era omogenea nel 44% ( p = 0 , 0001 ) , disomogenea nel 52% , lecostruttura del tumore lloide era omogenea nel 38% dei casi , disomogenea nel 62% e con aree cistiche contestuali nel 44% dei casi . 
 allintegrazione eco - color doppler , non era stato identi cato alcun pattern di distribuzione spaziale dei vasi in grado di differenziare il broadenoma dal tumore lloide . abbiamo , inoltre , calcolato laccuratezza diagnostica della mammogra a , dellecogra a e della core needle biopsy confrontata con listologia de nitiva nella diagnosi differenziale tra broadenoma e tumore lloide . 
a , b ultrasonography performed with multifrequency probe : large hypoechoic mass ( maximum diameter approximately 9 cm ) with homogenous internal echopattern and mass effect on adjacent breast tissue . 
a , b esame ecotomogra co eseguito con sonda multifrequenza : voluminosa lacuna ipoecogena ( diametro trasversale massimo 9 cm circa ) con tappeto di echi endolesionale omogeneo e netto effetto massa sul parenchima mammario adiacente . 
all values were statistically signi cant ( p = 0.001 ) ( table 3 )  . speci cit delle tre indagini era rispettivamente del 50% ( range 39%61% ) , 69% ( range 57%78% ) , 97% ( range 90%99% ) ; il valore predittivo positivo era del 79% per la mammogra a ( range 68%87% ) , dell82% per lecogra a 912 radiol med ( 2011 ) 116 : 905918 table 3 diagnostic accuracy of mammography , ultrasound and core needle biopsy compared with nal histology in the differential diagnosis between broadenoma and phyllodes tumour percent 95% con dence interval p value * lower limit upper limit tabella 3 accuratezza diagnostica della mammogra a , ecogra a e needle biopsy rispetto allistologia de nitiva nella diagnosi differenziale tra broadenoma e tumore lloide ic 95% limite inferiore limite superiore mammography vs nal histology sensitivity speci city positive predictive value ultrasound vs . 
at mammography , broadenomas may appear as low - density or , less commonly , high - density lesions with regular or irregular contours , with or without calci cations and with or without halo sign ( table 1 ) [ 4 , 15 ]  . 
i valori ottenuti sono statisticamente signi cativi ( p = 0 , 001 ) ( tabella 3 )  . discussione il ruolo della diagnostica per immagini nella diagnosi differenziale tra broadenoma e tumore lloide , nonch tra tumore lloide benigno e maligno da sempre controverso [ 424 ]  . 
alla mammogra a il broadenoma si pu presentare come una lesione radiopaca a bassa densit o , pi raramente ad elevata densit , con contorni regolari o irregolari , con o senza calci cazioni contestuali e con o senza halo sign ( tabella 1 ) [ 4 , 15 ] ; la dif colt maggiore radiol med ( 2011 ) 116 : 905918 fig . 
a esame ecogra co di voluminosa massa palpabile tradotta come lacuna ipoecogena ad echo pattern interno disomogeneo , a margini netti ma lobulati che allingrandimento elettronico mostra piccolo incluso similcistico ( freccia nera )  . 
c lesame ecogra co mostrava una lacuna ipoecogena a contorni marcatamente lobulati , ma netti , con tappeto dechi endolesionale omogeneo senza alterazioni del fascio acustico posteriore , priva di chiari elementi di sospetto ( probabile broadenoma )  . 
however , the presence or absence of intralesional calci cations in our study ( table 1 ) or in yilmatz et al.s study [ 4 ] had no statistical signi cance . 
 [ 4 ] affermano che il broadenoma si presenta alla mammogra a come una lesione radiopaca a bassa densit , mentre il tumore lloide come una massa radiopaca a densit maggiore ( p < 0 , 038 ) [ 4 ]  . 
nel nostro studio , nonostante il risultato non sia statisticamente signi cativo , abbiamo riscontrato che il 62% ( 10 / 16 ) dei tumori lloidi si presenta come una massa radiopaca ad elevata densit . 
tuttavia , nel nostro radiol med ( 2011 ) 116 : 905918 a halo sign in 2 / 19 broadenomas and 3 / 12 phyllodes tumours ( p = 0.349 ) [ 4 ]  . in most cases , us can discriminate between broadenomas and cystic or mixed lesions that may have identical clinical and mammographic features . 
however , if we exclude cases of small intralesional cysts , only a limited proportion of masses with similar mammographic appearance ( mostly phyllodes tumours and lymphomas , in particular in immunocompromised patients ) can be clari ed with us [ 5 , 6 , 11 ]  . in our study , broadenomas had a maximum diameter not exceeding 2 cm ( p = 0.0001 ) , consistent with the literature . 
in our study , 83% of broadenomas ( 56 / 67 ) had an oval shape ( p = 0.0001 ) and smooth contours ( p = 0.01 ) , in line with the ndings reported by yilmaz et al . 
the presence of intralesional cystic areas is pathognomonic for phyllodes tumour and improves the limited diagnostic accuracy of us ( 34% sensitivity and 69% speci city in our series , in agreement with the literature ) [ 4 , 5 , 20 , 25 ]  . 
al contrario , il 94% ( 63 / 67 ) dei broadenomi e il 25% ( 4 / 16 ) dei tumori lloidi da noi analizzati presentano halo sign ( p = 0 , 0001 ) ; il dato non in accordo con quello riportato da yilmaz et al . 
 [ 4 ] , che riscontrano questo segno in 2 / 19 broadenomi e in 3 / 12 tumori lloidi ( p = 0 , 349 ) [ 4 ]  . allecogra a possibile , nella maggior parte dei casi , distinguere i broadenomi da lesioni a contenuto cistico o misto che possono assumere aspetti ad essi del tutto sovrapponibili dal punto di vista clinico e mammogra co . 
lecogra a , tuttavia , se si esclude la presenza di piccole formazioni cistiche intralesionali , risolve solo in una limitata percentuale dei casi la diagnosi differenziale con masse con aspetto mammogra co simile ( soprattutto tumori lloidi e linfomi , specie nei pazienti immunocompromessi ) [ 5 , 6 , 11 ]  . 
 nel nostro studio , i broadenomi avevano un diametro massimo non superiore ai 2 cm ( p = 0 , 0001 ) , dato in accordo con la letteratura internazionale . 
 [ 20 ] affermano che i broadenomi si presentano per lo pi come lesioni dal diametro trasverso < 2 cm , i tumori lloidi come lesioni con diametro massimo 2 cm , mentre liberman et al . 
la presenza di aree cistiche contestuali patognomonica per tumore lloide e consente di incrementare la scarsa accuratezza diagnostica dellecogra a ( sensibilit 34% , speci cit 69% nel nostro studio , in accordo con la letteratura ) [ 4 , 5 , 20 , 25 ]  . 
in letteratura descritta la correlazione tra la distribuzione spaziale dei vasi ( capsulari , segmentari ) e la diagnosi anatomopatologica di broadenoma [ 26 ] ; al contrario , non si evidenzia alcuna caratteristica peculiare alleco - color doppler che consenta di porre il sospetto di tumore lloide [ 2729 ]  . 
moreover , from a clinical and imaging point of view , differentiation between giant broadenoma and other conditions associated with breast asymmetry is highly complex : in fact , giant broadenoma is virtually identical to phyllodes tumour in its benign ( high incidence of local recurrence ) and malignant forms ( high recurrence and metastatic rates ) [ 2 ]  . 
in these cases , histopathological examination is mandatory : whereas broadenomas are characterised by low mitotic activity , low stromal cellularity , absence of cellular atypia ( normal diploidy ) and expansile growth with sharp and well - visible contours , phyllodes tumours show an intracanalicular , frond - like growth pattern , moderate stromal hypercellularity at times with necrosis , sclerosis and various types of metaplasia , low mitotic activity and considerable increase in lesion size [ 1 , 8 , 11 ]  . 
contrary to the traditional view that considered phyllodes tumour to be an evolution of broadenoma , the two lesions are now regarded as two distinct disease entities [ 3 ]  . 
therefore , a lesion that shows low density , regular contours and a halo sign on mammography and an oval or lobular shape , smooth contours , hypoechoic echogenicity and a homogeneous echostructure on us may be considered a probable broadenoma . 
conversely , a high - density opacity , with no calci cations or halo sign at mammography , and with rounded or multilobular shape , irregular contours , marked hypoechogenicity ( relative to the surrounding fat ) , with a heterogeneous echostructure and containing cystic areas at us is likely to be a benign lesion ( other than broadenoma )  . despite the presence of features suggestive of the two histological types , the limited diagnostic accuracy of mammography and us ( table 3 ) , the overlap between mammographic and us ndings and the absence of pathognomonic signs do not permit discrimination between broadenoma and phyllodes tumour [ 4 , 5 ]  . 
especially in the case of phyllodes tumours , the results may in fact prove false negative if sampling was performed in an area of hypocellular stroma [ 17 , 18 ]  . 
although only a few studies have investigated the role of cnb in the differential diagnosis between broadenoma and phyllodes tumour [ 19 , 20 ] , they have all reported high ppv and negative predictive values ( npv ) [ 17 , 2123 ]  . 
it is reasonable to believe that immunohistochemical techniques and cell proliferation noma gigante e tumore lloide ( segnale intralesionale nel sequenze t1 e t2 ponderate e cinetica di enhancement post - contrastogra co assolutamente aspeci co ) [ 3 , 11 , 12 , 16 ]  . 
va detto , inoltre , che la diagnosi differenziale sul piano clinico e strumentale del broadenoma nella sua variante gigante nei confronti di altre condizioni associate ad asimmetria mammaria notevolmente complessa : esso infatti frequentemente del tutto indistinguibile dal tumore lloide nelle sue varianti benigna ( alto incide di recidive locali ) e maligna ( elevata capacit di recidiva e metastatica ) [ 2 ]  . 
 in questi casi necessario ricorrere allesame anatomopatologico : mentre il broadenoma si caratterizza per una bassa attivit mitotica cellulare , una bassa cellularit stromale , assenza di atipie cellulari ( corredo nucleare normalmente diploide ) , crescita per espansione con bordi netti e ben visibili , il tumore lloide mostra una crescita intracanalicolare con una estensione frond - like , una ipercellularit stromale modesta , talora con necrosi , sclerosi e vari tipi di metaplasia , bassa attivit mitotica e notevole aumento volumetrico espansivo [ 1 , 8 , 11 ]  . 
quindi , una lesione radiopaca a bassa densit , margini regolari e halo sign alla mammogra a e di forma ovale o lobulata , con margini lisci , ipoecogena e ad ecostruttura omogenea allecogra a , pu essere considerata come un probabile broadenoma . 
 al contrario , unopacit ad elevata densit , senza calci cazioni n halo sign alla mammogra a , che si presenta di forma rotondeggiante o plurilobulata , a margini irregolari , marcatamente ipoecogena ( in relazione al tessuto adiposo circostante ) , ad ecostruttura disomogenea e aree cistiche contestuali allecogra a , pu essere considerata come una probabile lesione benigna ( ma non broadenoma )  . 
 nonostante la presenza di caratteristiche suggestive per i due istotipi , la scarsa accuratezza diagnostica della mammogra a e dellecogra a ( tabella 3 ) , la sovrapposizione tra i parametri mammogra ci ed ecogra ci e lassenza di caratteri patognomonici non consentono di differenziare il broadenoma dal tumore lloide [ 4 , 5 ]  . 
soprattutto in caso di tumore lloide , infatti , il risultato pu essere falsamente negativo se il prelievo viene effettuato in unarea di stroma ipocellulare [ 17 , 18 ]  . 
pochi sono gli studi in letteratura che analizzano il ruolo della cnb nella diagnosi differenziale tra broadenoma e tumore lloide [ 19 , 20 ] , ma tutti riportano un elevato valore predittivo positivo e negativo [ 17 , 2123 ]  . 
 realistico pensare che in futuro tecniche immunoistochimiche e marcatori della proliferazione cellulare , quali p53 e ki 67 , ne renderanno radiol med ( 2011 ) 116 : 905918 markers such as p53 and ki - 67 will facilitate the differential diagnosis and prognostic evaluation in the future [ 17 ]  . in our experience , the diagnostic accuracy of mammography , us and cnb compared with nal histology shows that only cnb is able to differentiate between broadenoma and phyllodes tumour ( 81% sensitivity , 97% speci city and 87% ppv ) , as reported in the literature [ 19 , 20 , 30 , 31 ]  . pi agevole la diagnosi differenziale e la conseguente implicazione prognostica [ 17 ]  . nel nostro contributo i valori di accuratezza diagnostica della mammogra a , dellecogra a e della core needle biopsy , confrontati con listologia de nitiva , dimostrano che soltanto la core needle biopsy in grado di fare diagnosi differenziale tra broadenoma e tumore lloide ( sensibilit 81% , speci cit 97% e valore predittivo positivo 87% ) , cos come dimostrato in letteratura [ 19 , 20 , 30 , 31 ]  . conclusions conclusioni on mammography , broadenomas mostly appear as lowdensity opacities with regular contours and a halo sign ; phyllodes tumours appear as high - density opacities with neither calci cations nor halo sign . 
if a lesion appears on us as an oval or lobular mass with smooth contours , hyperechogenicity relative to the surrounding glandular tissue and homogeneous echostructure , it is likely to be a broadenoma . 
if a lesion appears rounded or multilobular , with irregular contours , marked hypoechogenicity ( relative to the surrounding fat ) , heterogeneous echostructure and cystic areas , it is likely to be a benign lesion ( but not broadenoma )  . 
there is nonetheless a substantial overlap between the mammographic and us parameters of broadenomas and phyllodes tumours , and no pathognomonic signs exist that allow discrimination between the two histological types . 
us - guided cnb represents a valuable tool in the differential diagnosis between broadenoma and phyllodes tumour . in conclusione , alla mammogra a , il broadenoma si presenta prevalentemente come unopacit a bassa densit , a margini regolari e halo sign ; il tumore lloide come unopacit ad elevata densit senza calci cazioni , n halo sign . 
se allesame ecogra co una lesione si presenta di forma ovale o lobulata , margini lisci , ipoecogenicit rispetto al tessuto ghiandolare circostante ed ecostruttura omogenea , pu essere considerata come un probabile broadenoma ; se in presenza di queste caratteristiche , ha un diametro > 5 cm , come un probabile broadenoma gigante ; se di forma rotondeggiante o plurilobulata , a margini irregolari , marcatamente ipoecogena ( in relazione al tessuto adiposo circostante ) , ad ecostruttura disomogenea e aree cistiche contestuali , pu essere considerata come una probabile lesione benigna ( ma non broadenoma )  . 
tuttavia , esiste una sostanziale sovrapposizione tra i parametri mammogra ci e ultrasonogra ci dei broadenomi e dei tumori lloidi e non ci sono caratteristiche patognomoniche che consentano di fare diagnosi differenziale tra i due istotipi . al contrario , la core needle biopsy ecoguidata rappresenta un valido strumento nella diagnosi differenziale tra broadenoma e tumore lloide . 
mr - guided vab was attempted in 29 / 106 lesions ( 27% ) ; in 2 / 29 patients , the procedure could not be performed owing to failure to visualise the lesion . 
lesions with clearly malignant features and borderline lesions ( atypical ductal hyperplasias ) were identi ed in 12 cases ( 44% ) and benign entities in 15 ( 56% )  . 
seven of 12 ( 58% ) malignant lesions were < 10 mamong the 27 successful mr - vab procedures , vab yielded one false - negative diagnosis ( 4% ) and underestimation ( 4% )  . 
sono state avviate al vab , con lutilizzo di un ago da 10 gauge , le pazienti con alterazioni sospette alla rm , non riconoscibili con ecogra a n mammogra a , non palpabili , in cui la tipizzazione non poteva essere ottenuta con metodiche alternative . 
il riscontro di patologia francamente maligna o di lesioni border - line si veri cato in 12 casi ( 44% ) , nei restanti 15 casi ( 56% ) si rilevata patologia benigna . 
sette / 12 ( 58% ) lesioni maligne avevano diametro inferiore o uguale a 10 muno / 27 casi ( 4% ) risultato falso negativo al vab ; 1 / 27 casi ( 4% ) stato sottostimato dal vab . 
complessivamente , il prelievo vab sotto guida rm ha mostrato valori di sensibilit e speci cit rispettivamente del 92% e 100% con valore predittivo positivo del 100% e valore predittivo negativo del 93% . radiol med ( 2011 ) 116 : 876885 keywords breast cancer diagnosis breast mri biopsy vacuum - assisted biopsy ( vab ) conclusioni . 
le dimensioni della lesione inferiori a 1 cm non sono un limite per la metodica . parole chiave carcinoma mammario diagnosi rm della mammella vab biopsia introduction introduzione as its high diagnostic sensitivity , magnetic resonance ( mr ) imaging of the breast provides added value compared with mammography and ultrasonography [ 1 ]  . 
although the clinical impact of breast mr imaging in the workup of breast disease is still controversial [ 26 ] , the growing diffusion of the technique leads to the increasingly frequent nding of incidentally discovered breast lesions without a correlate on conventional breast imaging . 
the wide availability of aspiration cytology with ne ferromagnetic needles and coaxial nonmagnetic needles allows lesions to be characterised noninvasively but is limited by the inadequacy of the samples collected , especially in the case of non - mass - like lesions [ 79 ]  . 
the advent of large calibre needles and mr - compatible materials has made it possible to collect more material with improved precision , at the price , however , of a considerable increase in costs [ 10 ]  . 
 the introduction of a microhistological sampling technique with cutting needles and a vacuum aspiration device vacuum assisted biopsy ( vab ) has marked a new step forward in the direction of more sophisticated sampling technology [ 11 ] , even though the costs have increased further [ 12 ] and no reimbursement by the italian national health system is as yet envisaged . 
 the aim of this study was to evaluate the impact on clinical practice of mr - guided vab as the nal step in the diagnostic workup of breast lesions incidentally detected on mr imaging and to validate the techniques diagnostic accuracy by correlating the microhistological results with the histopathological ndings on the surgical specimen . material and methods in ragione dellelevata sensibilit diagnostica , lindagine di risonanza magnetica ( rm ) della mammella rappresenta una metodica imaging dal valore aggiuntivo rispetto alla mammogra a e allecogra a [ 1 ]  . 
sebbene limpatto clinico dellintroduzione della rm mammaria nelliter diagnostico della patologia mammaria sia ancora controverso [ 26 ] , la crescente diffusione dellindagine rm comporta il sempre pi frequente riscontro di lesioni mammarie incidentalmente identi cate nellindagine rm , prive di corrispettivo allesame senologico tradizionale . 
lampia disponibilit dellesame citologico per aspirazione con ago sottile ferromagnetico e ago coassiale amagnetico rende possibile la diagnosi di natura in maniera incruenta , ma penalizzato da prelievi inadeguati , soprattutto in caso di lesioni non massa [ 79 ]  . 
lavvento di aghi di grosso calibro e di materiali rm compatibili , ha permesso di ottenere materiale pi abbondante e precisione superiore , sebbene con incremento considerevole dei costi [ 10 ]  . 
 lattuale disponibilit di una tecnologia di prelievo microistologico con aghi trincianti e con dispositivo di aspirazione sottovuoto ( vacuum assisted biopsy , vab ) ha rappresentato un nuovo passo avanti verso una tecnologia di prelievo pi so sticata [ 11 ] , sebbene con ulteriore lievitazione dei costi [ 12 ] per la quale in italia non ancora previsto il rimborso da parte del sistema sanitario nazionale ( ssn )  . 
 scopo di questo lavoro valutare lincidenza nella pratica clinica dei prelievi vab sotto guida rm come tappa nale delliter diagnostico nella gestione delle lesioni incidentalmente identi cate allindagine rm e di validarne laccuratezza diagnostica comparando i risultati microistologici con quelli istologici derivanti dal pezzo operatorio . we retrospectively analysed 98 patients ( 97 women and one man ; mean age 49 years ; range 2279 years ) with 106 breast lesions identi ed on mr imaging from september 2007 to march 2009 . 
indications for mr examination included preoperative assessment of patients scheduled for materiali e metodi sono stati retrospettivamente analizzati 98 pazienti ( 97 donne e 1 uomo ; et media 49 anni ; range 2279 anni ) porta878 radiol med ( 2011 ) 116 : 876885 surgery due to malignant disease detected on mammography and ultrasound ( us ) in 53 cases ( 45% ) , evaluation of the surgical scar in 27 ( 27% ) patients and screening of women at high risk of breast cancer in 18 cases ( 18% )  . we included in the analysis cases in which mr imaging identi ed suspicious or highly suspicious lesions , according to classi cation of the american college of radiology breast imaging reporting and data system ( bi - rads ) 4 and 5 , that were nonpalpable and occult on conventional breast imaging and for which we had complete data regarding subsequent diagnostic procedures or follow - up for at least 12 months . 
 the lesions sampled under mr guidance were grouped by mr appearance ( mass - like enhancement , non - masslike enhancement , focus ) [ 1 ] and size ( long axis ) and distributed on the basis of level of suspicion of malignancy ( bi - rads classi cation ) [ 13 ]  . 
patients with a histopathological diagnosis of benign lesion were followed up by mr imaging at 6 months and subsequently referred for standard screening follow - up for at least 12 months . 
the microhistological diagnosis of vab was then correlated with histological diagnosis of the surgical specimen , considered the gold standard . mr - guided biopsy all biopsies were performed after obtaining the patients informed consent and discontinuing any anticoagulation therapy in accordance with the protocol standardised by the current guidelines [ 14 ]  . 
lesion localisation was performed with the patient in the prone position and using an mr - compatible stereotactic system ( siemens , erlangen , germany ) consisting of a support to accommodate the breast and two plates with parallel perforated holes for mediolateral compression of the breast . 
signal reception is guaranteed by a soft , circular surface coil placed between the two bars so as to completely surround the breast . lesion localisation was achieved with t1 - weighted axial sequences before and after administration of contrast material . 
the spatial coordinates were calculated with the breast tori di 106 lesioni identi cate dallesame rm nel periodo compreso tra settembre 2007 e marzo 2009 . lindagine rm stata effettuata per la valutazione preoperatoria in pazienti candidate a intervento per patologia maligna accertata allindagine mammo - ecogra ca in 53 casi ( 45% ) ; per studio di cicatrice in 27 ( 27% ) pazienti sottoposte a precedente intervento ; per sorveglianza di donne ad alto rischio di carcinoma mammario in 18 casi ( 18% )  . sono stati inclusi nellanalisi i casi in cui la rm ha identi cato lesioni sospette o altamente sospette ( breast imaging reporting and data system [ bi - rads ] 4 e 5 ) non palpabili e non visibili allindagine senologica convenzionale , in cui erano disponibili tutte le notizie riguardo al successivo iter diagnostico o al follow - up per almeno 12 mesi . 
 le lesioni sottoposte a prelievo rm - guidato sono state raggruppate per aspetto rm ( enhancement tipo mass , non mass , focus ) [ 1 ] , dimensione ( considerata come maggior asse della lesione ) e distribuite in rapporto al giudizio di sospetto ( secondo la classi cazione bi - rads - american college of radiology ) [ 13 ]  . 
il gold standard stato lesame patologico proveniente dallescissione chirurgica . prelievo sotto guida rm la procedura di prelievo rm guidato stata eseguita con il consenso informato da parte della paziente e dopo sospensione di eventuali terapie anticoagulanti , secondo modalit standardizzate dalle attuali linee guida [ 14 ]  . 
la centratura della lesione avvenuta con paziente in decubito prono e sistema stereotassico rm compatibile ( siemens , erlangen , germania ) costituito da un supporto per il posizionamento della mammella interessata e da due piatti dotati di fessure parallele per la compressione del seno in direzione mediolaterale . 
la ricezione del radiol med ( 2011 ) 116 : 876885 biopsy tool software available on the systeafter establishing the entry hole , a coaxial introducer consisting of a plastic cannula and a titanium stylet was xed to the support syste after removing the stylet , the site was anaesthetised ( 10 cc 2% lidocaine hydrochloride ) and incised with a scalpel , and the biopsy probe was inserted . 
postprocedural mr with an axial t1 - weighted sequence was used to verify clip position and the success of the procedure ( correct targeting ; bleeding )  . results targeted us of the site of the incidental mr lesion identi ed 77 of 106 ( 73% ) lesions identi ed on mr imaging . 
after conventional mr imaging without compression and with a dedicated breast coil , which con rmed nonvisualisation of the lesion presumably re ecting an area of enhancement of functional gland tissue patients were referred for follow - up at 6 months . a total of 27 / 29 ( 93% ) procedures were successfully completed . 
comparing bi - rads assessment with the microhistological diagnosis , in 5 / 12 ( 42% ) malignant lesions , the mr evaluation was highly suspicious ( bi - rads 5 ) and in 7 / 12 ( 58% ) suspicious ( bi - rads 4 )  . 
with regard to the result of pathology segnale garantita da una bobina di super cie , di forma circolare e consistenza morbida , interposta fra le barre in modo da circondare completamente la mammella . per la localizzazione spaziale della lesione sono state acquisite sequenze assiali t1 - dipendenti prima e dopo somministrazione di mezzo di contrasto . 
dopo aver rimosso il mandrino previa anestesia cutanea ( lidocaina cloridrato diluita al 2% , 10 cc ) e incisione con bisturi , stata inserita la sonda per i prelievi . 
la procedura si terminata con il posizionamento di clip in titanio ( micromark ii ; biomarc , ultraclip ) per centratura della sede del prelievo e mediante acquisizione di sequenza t1 assiale stato effettuato il controllo rm post - prelievo del posizionamento della clip e della validit della procedura ( centratura del bersaglio , eventuale comparsa di ematomi )  . risultati nella serie complessiva di 106 lesioni identi cate dallindagine rm , lecogra a mirata nella sede della lesione incidentalmente evidenziata dalla rm ha identi cato 77 su 106 ( 73% )  . 
dopo espletamento dindagine rm convenzionale , senza compressione e con bobina dedicata , che ha confermato la non riconoscibilit della lesione presumibilmente con signi cato di area dimpregnazione ghiandolare funzionale , si optato per il controllo rm dopo 6 mesi . 
il numero dei frustoli prelevati stato variabile 880 radiol med ( 2011 ) 116 : 876885 table 1 distribution of mr pattern , size , level of suspicion in 27 mrguided vab cases study variable variable categories no . 
compared with the previous cancer , the site of the malignant lesion was subcicatricial in one case , ipsilateral but in a different da 9 a 25 cores per ciascuna procedura ( valore medio di 18 frustoli / procedura ) ( tabella 2 )  . 
la comparsa di complicanze si veri cata in una sola paziente , portatrice di una lesione profonda , adesa al pettorale in cui lematoma risultato assai esteso ed ha richiesto terapia antibiotica . 
comparando il giudizio bi - rads con la diagnosi microistologica , in 5 / 12 ( 42% ) delle lesioni maligne stato formulato un giudizio rm di altamente sospetto ( birads 5 ) e in 7 / 12 ( 58% ) giudizio rm di sospetto ( bi - rads 4 )  . 
per quanto riguarda il risultato patologico in rapporto alle dimensioni della lesione , 7 / 12 ( 58% ) lesioni maligne avevano diametro inferiore o uguale a 10 mm e 5 / 12 ( 42% ) lesioni maligne erano estese pi di 10 mm . le 12 pazienti con diagnosi vab di malignit sono state avviate allintervento chirurgico ; 14 / 15 lesioni con diagnosi vab di benignit sono state avviate al follow - up che ne ha confermato la stabilit nel tempo ( periodo minimo di 12 mesi ) ; una paziente con diagnosi vab di benignit stata avviata allintervento chirurgico a causa del persistere del sospetto radiologico . 
rispetto alla neoplasia antecedente , la sede della lesione maligna stata rispettivamente sottocicatriziale in 1 caso , omolaterale alla pregressa neoplasia ma in quadranti diversi in 3 casi e controlaterale in 1 caso . 
of cores per procedure microhistological vab ndings 1 ( 4 ) < 11 21 ( 78 ) 1120 > 20 5 ( 18 ) in ltrating carcinoma 8 ( 30 ) 3 ( 10 ) in situ carcinoma 1 ( 4 ) borderline lesion 15 ( 56 ) benign lesion numero di frustoli < 11 prelevati / procedura 1120 diagnosi microistologica vab lesioni in situ > 20 lesioni in ltranti lesioni borderline lesioni benigne 1 ( 4 ) 21 ( 78 ) 5 ( 18 ) 8 ( 30 ) 3 ( 10 ) 1 ( 4 ) 15 ( 56 ) radiol med ( 2011 ) 116 : 876885 fig . 
axial t1 - weighted contrast - enhanced magnetic resonance ( mr ) image obtained in a screening setting shows a small , irregular , spiculated , enhancing mass spanning 7 mm [ mr diagnostic image ( a ) ]  . 
allesame rm dopo somministrazione di mezzo di contrasto ( mdc ) , espletato per screening , si evidenzia una piccola formazione espansiva di 7 mm , con impregnazione di tipo massa e pro li sfumati ( a immagine durante lesame rm diagnostico )  . 
lesame microistologico ( b5 ) stato confermato dallesame patologico del pezzo operatorio con diagnosi di carcinoma duttale in ltrante ( diametro massimo di in ltrazione 6 mm )  . quadrant in three cases and contralateral in one . 
the mr examination modi ed the surgical operation , and the women underwent bilateral quadrantectomy right upper outer and left lower outer quadrant in a single surgical procedure . correlation between vab results and results of histology of the surgical specimen revealed discordance in four cases : 1 / 27 cases ( 4% ) was false negative at vab ( brocystic disease at vab vs ductal carcinoma in situ at surgery carcinoma duttale in situ [ dcis ] allintervento ; si trattava di lesione di 9 mm nella quale il sospetto radiologico era elevato ) , 1 / 27 casi ( 4% ) stato sottostimato dal vab ( carcinoma duttale in situ al vab vs carcinoma duttale in ltrante allintervento ) ; nei rimanenti 2 casi ( 8% ) risultati dcis al vab lallargamento chirurgico ha rilevato solo proliferazione atipica residua ( trattavasi di 2 lesioni con diametro inferiore al centimetro e con campionamento superiore a 20 frustoli )  . 
complessivamente , il prelievo vab sotto guida rm ha mostrato valori di sensibilit e speci cit rispettivamente del 92% e 100% con valore predittivo positivo del 100% 882 radiol med ( 2011 ) 116 : 876885 fig . 
sagittal t1 - weighted contrast - enhanced magnetic resonance ( mr ) image obtained for preoperative evaluation shows clumped linear and ductal enhancement in the left lower quadrant ( residual disease ) ( f )  . 
 axial t1 - weighted contrast - enhanced mr image of the left breast shows a separate , irregularly shaped , 13 mm , enhancing , non - mass - lesion in the left breast at 12 : 00 oclock position ( g )  . 
allesame mammogra co ( a - e ) , a destra nel versante inferiore del piano sagittale mediano , multiple calci cazioni pleomorfe in area di 2 cle calci cazioni vengono sottoposte a prelievo microistologico sotto guida stereotassica ( b5 )  . 
allesame rm dopo somministrazione di mdc eseguito per valutazione pre - operatoria , nel versante inferiore della mammella destra , sede del prelievo si rileva estesa area di impregnazione a piccoli noduli riferibile a lesione residua ( f )  . 
overall , mr - guided vab had a sensitivity and speci city of 92% and 100% , respectively , with a positive predictive value ( ppv ) of 100% and a negative predictive value ( npv ) of 93% . 
in our series , second - look us resolved the management of a large majority ( 73% ) of mr - visible lesions , a percentage higher than reported in other studies [ 17 , 18 ]  . 
 in our series , in the only case of false - negative result at vab , surgery was dictated by the discrepancy between the benign diagnosis and the high level of radiological suspicion . 
the vab diagnoses of malignant disease proved to be accurate and timely , considering that 58% of the malignant lesions had a diameter < 1 c this nding is in agreement with previous larger series and demonstrates that small lesion size does not constitute a limitation to the procedure [ 16 ]  . 
that atypical proliferative lesions and ductal carcinoma in situ are the most common causes of error is well known and has already been demonstrated for biopsy under stereotactic guidance [ 22 , 23 ]  . 
come evidenziato da precedenti esperienze [ 1720 ] , il second - look ecogra co si conferma essere il primo ragionevole approccio per la identi cazione e tipizzazione delle lesioni incidentalmente evidenziate allindagine rm . 
una possibile spiegazione della discrepanza riguardo al tasso di detection rate del secondlook ecogra co risiede nella diversa diffusione dellimaging ecogra co e nella diversa esperienza degli operatori che lo svolgono . 
in questo studio , il prelievo vab sotto guida rm ha mostrato valori di sensibilit e speci cit rispettivamente del 92% e 100% con valore predittivo positivo del 100% e valore predittivo negativo del 93% . 
 la diagnosi vab di malignit risultata accurata e precoce considerando che il 58% delle lesioni maligne evidenziate avevano diametro inferiore a 1 c tale dato , in accordo con quanto osservato in pi ampie casistiche , dimostra che le dimensioni contenute della lesione non costituiscono un limite della procedura [ 16 ]  . 
in letteratura , come peraltro gi dimostrato per i prelievi sotto guida stereotassica , ben noto che le cause pi frequenti di errore sono rappresentate dalle lesioni proliferative atipiche e dal carcinoma duttale in situ [ 22 , 23 ]  . 
questo risultato conferma lutilit dellesteso campionamento al ne di fornire una 884 radiol med ( 2011 ) 116 : 876885 8% of cases , vab allowed complete removal of the lesion in situ , with only residual foci of a borderline lesion being identi ed at surgery [ 24 ]  . 
this result con rms the usefulness of extended sampling to provide a precise diagnosis and correct possible localisation defects that could affect the adequacy of the sample . in conclusion , mr - guided vab proved to be a welltolerated , simple and reliable method for characterising suspicious nonpalpable breast lesions detected on breast mr imaging and occult on mammography and us . 
this approach allows identi cation of new disease foci , containment of the number of false positive results and planning of de nitive surgery in the case of a microhistological diagnosis of malignancy , all in a single session . 
with regard to costs : economic costs of mr - guided biopsies and the economicsocial costs of biopsies / surgical excisions generated by false - positive mr ndings make it desirable to concentrate all mr - guided procedures in referral centres to which all facilities offering breast mr imaging can direct their patients . 
only by optimising the sampling technique and results can new , possibly less expensive , solutions be proposed . diagnosi precisa e di correggere eventuali vizi di centratura che potrebbero compromettere ladeguatezza del prelievo . in conclusione , il prelievo vab sotto guida rm risultato essere metodica af dabile nella tipizzazione delle lesioni mammarie rm sospette , non palpabili , ecogra camente e mammogra camente occulte , ben tollerato dalle pazienti e di facile procedura . 
il prelievo vab pu pertanto essere proposto in casi selezionati , dopo attenta rivalutazione dellesame senologico convenzionale , per la tipizzazione delle lesioni rm - visibili , rendendo possibile la programmazione del trattamento chirurgico de nitivo in unico tempo . 
tale approccio permette di ottenere lidenti cazione di nuovi foci di malattia , contenimento del numero dei falsi positivi e intervento chirurgico programmato in caso di diagnosi microistologica di malignit . 
in considerazione dei costi , economici per quanto concerne i prelievi rm guidati ed economici - sociali in caso di biopsie / allargamenti chirurgici generati dai reperti rm falsi positivi , si auspica daltra parte laccentramento delle metodiche rm guidate in centri di riferimento a cui possano afferire tutte le strutture ove vengono espletate indagini di rm della mammella . 
between 2004 and 2007 , 182 patients with malignant breast lesions detected on us and / or x - ray mammography and con rmed by cytology / histology underwent preoperative breast contrast - enhanced ( ce ) - mri . 
tra il 2004 ed il 2007 , 182 pazienti con lesioni maligne allecogra a e / o mammogra a e confermate dallesame citologico / istologico sono state sottoposte a rm della mammella con mezzo di contrasto ( mdc ) per stadiazione preoperatoria . 
sensibilit , speci cit , accuratezza , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) per identi cazione e diagnosi sono risultati del 100% , 88 , 9% , 94 , 6% , 90 , 3% and 100% per la rm e del 64 , 3% , 70 , 4% , 67 , 3% , 69 , 2% e 65 , 5% per il second - look ecogra co . 
il second - look ecogra co un valido metodo radiol med ( 2011 ) 116 : 886904 keywords breast mri second - look ultrasound breast cancer incidental ndings per le lesioni occasionali alla rm della mammella , in particolar modo per i potenziamenti di tipo nodulare . 
 parole chiave rm della mammella second - look ecograco carcinoma della mammella lesioni incidentali introduction introduzione magnetic resonance imaging ( mri ) is well established as the most sensitive diagnostic technique for detecting and staging malignant breast lesions and has recently been recommended by the american cancer society ( acs ) as a breast cancer screening procedure for women with a 2025% or greater lifetime risk of breast cancer , including women with a strong family history of breast or ovarian cancer and women treated for hodgkins disease [ 1 ]  . 
its value as a routine clinical procedure extends beyond the depiction of breast cancer to monitoring the effects of neoadjuvant chemotherapy , presurgical planning and detecting cancer recurrence [ 24 ]  . 
apart from its superiority over whole - breast ultrasound ( us ) and x - ray mammography for evaluating known breast lesions , breast mri has proved particularly valuable for detecting unsuspected multifocal disease and mammographically occult malignant disease [ 57 ] .unfortunately , detecting abnormal enhancing lesions not seen on previous mammography and whole - breast us is potentially problematic for subsequent patient - management decisions in that it is sometimes unclear whether these lesions should be ignored , followed up or referred for biopsy . 
the purpose of this prospective study was to assess the utility of second - look us for evaluating incidental enhancing lesions identi ed on preoperative breast mri performed for staging malignant lesions diagnosed by conventional breast imaging methods ( mammography and / or us ) and con rmed by cytology or core biopsy . materials and methods patients between november 2004 and march 2007 , 182 consecutive patients with suspected breast malignancy on conventional x - ray mammography and / or whole - breast us , and invasive carcinoma subsequently con rmed by cytology or core biopsy , underwent preoperative breast mri for accurate breast cancer staging . 
no patient was undergoing or had undergone chemotherapy or had received any other contrast material in the week prior to stato ampiamente dimostrato come la risonanza magnetica ( rm ) sia la tecnica diagnostica pi sensibile nellidenti cazione e stadiazione delle lesioni mammarie maligne . 
recentemente lamerican cancer society ( acs ) ha raccomandato il suo impiego per lo screening del carcinoma mammario in donne con rischio di carcinoma della mammella pari o superiore al 20%25% , includendo donne con forte familiarit per carcinoma mammario o ovarico e donne sottoposte a terapia per morbo di hodgkin [ 1 ]  . 
nella routine diagnostica il suo ruolo si estende dallindividuazione del carcinoma mammario al monitoraggio della risposta alla chemioterapia neoadiuvante , alla stadiazione preoperatoria ed allidenti cazione di recidiva di malattia [ 24 ]  . 
oltre alla sua superiorit rispetto ad ecogra a e mammogra a nella valutazione delle lesioni mammarie note , la rm si dimostrata particolarmente utile nellindividuazione di patologie multifocali o lesioni maligne non evidenziate mediante le tecniche diagnostiche convenzionali [ 57 ]  . 
sfortunatamente , lidenti cazione di lesioni con impregnazione post - contrastogra ca abnormale e non osservate alla mammogra a e / o ecogra a mammaria , potenzialmente problematica per la scelta della successiva strategia terapeutica da adottare , poich a volte non ben chiaro se tali lesioni debbano essere ignorate , sottoposte a follow - up o a biopsia . 
lobiettivo di questo studio prospettico stato quello di dimostrare lutilit del second - look ecogra co nella valutazione di lesioni con impregnazione post - contrastogra ca evidenziate alla risonanza magnetica preoperatoria della mammella , eseguita per la stadiazione di lesioni mammarie maligne diagnosticate mediante le tecniche diagnostiche convenzionali per la mammella ( mammogra a e / o ecogra a ) e confermate dallesame citologico o dalla biopsia percutanea . materiali e metodi pazienti nel periodo compreso tra novembre 2004 e marzo 2007 , 182 pazienti con sospetto di neoplasia della mammella alla mammogra a e / o ecogra a e successiva diagnosi di carcinoma invasivo allesame citologico o alla biopsia percutanea , sono state sottoposte a rm preoperatoria della mammella per unaccurata stadiazione . 
 likewise , patients with incidental lesions considered de nitely benign on breast mri [ category 2 according to the breast imaging reporting and data system ( bi - rads ) lexicon ] [ 8 ] were not included . 
 mr imaging breast mri was performed on a 1.5 - t imager ( avanto , siemens , erlangen , germany ) using a bilateral breast surface coil with the patient in the prone position . 
transverse threedimensional dynamic t1 - weighted gradient - echo ( gre ) images were acquired before contrast agent administration ( unenhanced images ) and then ve times after contrast agent administration ( contrast - enhanced images )  . 
the imaging parameters for the t1 - weighted gre sequence were identical for all patients , with repetition time 8.1 ms , echo time 4 ms , ip angle 30 ; one signal acquired ; rectangular eld of view < 36 cm and matrix 496 512 . 
contrast agent administration was in all cases performed by power injector ( spectris , medrad , indianola , pa , usa ) via an antecubital venous access at a standard ow rate of 2 ml / s ( bolus ) , followed by a 10 - ml saline ush at the same rate . 
the contrast agent used in all patients was gadobenate dimeglumine ( multihance , bracco imaging spa , milan , italy ) at a nal dose of 0.1 mmol / kg bodyweight , as this agent has previously been shown to have preferential properties for breast imaging [ 912 ]  . 
data acquisition began immediately after contrast agent injection , at the end of the saline ush . second - look ultrasound ultrasound examinations were performed by one of two experienced radiologists using a high - resolution unit ( ssa700a , toshiba , japan ) with a linear array probe centred at rale , le pazienti di et maggiore ai 40 anni anche a mammogra a . 
nessuna di tali pazienti era in corso di chemioterapia neoadiuvante n alcuna di loro aveva ricevuto alcun tipo di mezzo di contrasto nelle due settimane precedenti allo studio con rm . 
le pazienti con lesioni con impregnazione postcontrastogra ca , riscontrate occasionalmente alla rm , sono state sottoposte successivamente a second - look ecogra co mirato allo studio del reperto osservato incidentalmente alla rm . 
allo stesso modo le lesioni occasionali considerate benigne alla rm ( categoria 2 secondo il breast imaging reporting and data system [ bi - rads ] lexicon ) [ 8 ] non sono state incluse in questo studio studio . 
 imaging rm la rm della mammella stata eseguita su un magnete a 1 , 5 t ( avanto , siemens , erlangen , germania ) usando bobine bilaterali dedicate per lo studio della mammella , con la paziente in posizione prona . 
sono state acquisite sequenze assiali 3d dinamiche , t1 pesate ( gradient echo [ gre ] ) prima ( immagini senza impregnazione ) e 5 volte dopo la somministrazione di mezzo di contrasto ( immagini con impregnazione )  . 
in tutti le pazienti per le sequenze t1 ( gre ) pesate sono stati usati gli stessi parametri comprensivi di : un tempo di ripetizione di 8 , 1 ms , tempo di eco di 4 ms , ip angle di 30 , singola acquisizione di segnale , campo di vista rettangolare 36 cm e matrice di 496512 . 
non sono state impiegate sequenze di soppressione del segnale del grasso , per eliminare il segnale proveniente dal grasso stata effettuata una sottrazione delle immagini ( immagini con impregnazione post - contrastogra ca immagini senza impregnazione postcontrastogra ca )  . 
il mezzo di contrasto stato somministrato attraverso un accesso venoso antecubitale , mediante lausilio di un iniettore automatico ( spectris ; medrad , indianola , pa ) al usso standard di 2 ml / s ( bolo ) , seguito dalla somministrazione di 10 ml di soluzione siologica alla stessa velocit . 
come mezzo di contrasto in tutti i pazienti stato impiegato il gadobenate dimeglumine ( multihance , bracco imaging spa , milano , italia ) alla dose di 0 , 1 mmol / kg di peso corporeo , essendo stati gi dimostrati i vantaggi relativi al suo uso nella diagnostica rm della mammella [ 912 ]  . 
the patient was placed in the supine position for lesions detected in the medial parts of the breast and in a contralateral posterior oblique position with the arms raised for lesions detected in lateral parts of the breast . 
 given differences in positioning between prone mri and supine us , targeting for the second - look us exam was in all cases performed by breast quadrant . image interpretation all mr and us images were evaluated prospectively by two radiologists in consensus ( xy , 7 years experience in breast mri and 9 years experience in breast us ; xx , 5 years experience in breast mri and 7 years experience in breast us ) with full knowledge of the patients clinical history and with previous conventional imaging ndings available . 
all images were reviewed electronically using a picture archiving and communication system ( pacs ) ( lifeweb ; ferrania technologies , london , england ) that allowed manual windowing and optimisation of parameters . 
in all cases , source images , subtracted images ( postcontrast minus precontrast unenhanced images ) and maximum intensity projection ( mip ) reconstructions were evaluated , as were signal intensity / time ( si / t ) curves determined at regions of interest ( roi ) placed on enhancing regions within the lesion . 
 type i curves demonstrated persistent enhancement with either a straight si / t line ( ia ) or curve ( ib ) and were more frequently considered indicative of a benign lesion ; type ii curves demonstrated a rapid early increase of si followed by an si plateau and were considered borderline ; type iii curves demonstrated a rapid early increase of si followed by rapid washout of contrast material and were considered indicative of malignancy [ 1315 ]  . 
based on the bi - rads classi cation a spiculated lesion with rim enhancement , nonsmooth borders and rapid washout would typically be considered a bi - rads 5 lesion . 
the size of all detected lesions was recorded for subsequent comparison . lesion biopsy all incidental enhancing lesions detected on breast mri subito dopo linoculazione del mezzo di contrasto , alla ne del usso di soluzione siologica . second - look ecogra co gli esami ecogra ci sono stati eseguiti da uno dei due esperti radiologi , impiegando apparecchi ad alta risoluzione ( ssa700a , toshiba , giappone ) , con sonde lineari con frequenza di 14 mhz . 
per lo studio dei quadranti interni le pazienti sono state sistemate in posizione prona mentre i quadranti esterni sono stati esaminati con la paziente adagiata sul anco controlaterale e con le braccia sollevate . 
 in ogni caso vista la differenza di posizionamento tra risonanza magnetica ed ecogra a , larea studiata attraverso lecogra a mirata sempre coincisa con lintero quadrante della mammella . interpretazione delle immagini tutte le immagini di risonanza magnetica ed ecogra a sono state analizzate da due radiologi in consensus ( xy , sette anni di esperienza nel campo della rm ; xx cinque anni di esperienza nel campo della rm ; xy , nove anni di esperienza in ecogra a mammaria ; xx , sette anni di esperienza in ecogra a mammaria ) con piena conoscenza della storia clinica delle pazienti e con i precedenti esami diagnostici convenzionali a disposizione per confronti . 
tutte le immagini sono state riesaminate elettronicamente attraverso un sistema di archiviazione e trasmissione di immagini ( lifeweb , ferrania technologies , londra , inghilterra ) che ha consentito di modi care manualmente la nestra ed ottimizzare i parametri . 
la valutazione delle immagini di rm avvenuta in base alla morfologia delle lesioni ed alle caratteristiche di potenziamento post - contrastogra co secondo la classi cazione bi - rads [ 8 ]  . 
secondo tale classi cazione le lesioni individuate sono state de nite come lesioni nodulari ( mass - like ) , non nodulari ( non mass - like ) o foci di potenziamento post - contrastogra co . 
in tutti i casi sono stati prese in esame sia le immagini base sia quelle sottratte ( immagini dopo somministrazione di mezzo di contrasto meno le immagini precontrasto ) sia le ricostruzioni di massima intensit di proiezione ( mip ) come anche le curve intensit segnale / tempo ( is / t ) , ottenute attraverso il posizionamento di una regione di interesse ( roi ) in un punto di potenziamento post - contrastogra co allinterno della lesione . 
 le curve di tipo i con un potenziamento di tipo continuo e corrispondenti ad una linea dritta ( ia ) o ad una curva ( ib ) 890 radiol med ( 2011 ) 116 : 886904 that were considered category 3 , 4 or 5 according to the bi - rads lexicon [ 8 ] and that subsequently had a suspicious correlate on second - look us ( bi - rads 45 ) were evaluated histologically immediately after the second - look us examination . 
lesions with a de nite us correlate were evaluated by means of core needle biopsy ( cnb ) under us guidance or by excisional biopsy following us - guided wire localisation . 
incidental enhancing lesions that were considered bi - rads 3 on breast mri that had a correlate lesion on second - look us that was considered benign or probably benign ( bi - rads 23 ) were managed conservatively with initial follow - up breast mri and us at 6 months , followed by repeat follow - up at 12 and 24 months . 
 for suspicious lesions at mri ( bi - rads 45 ) without a us correlate , cnb was performed under mri guidance , whereas lesions considered bi - rads 3 on breast mri were managed conservatively , with initial follow - up breast mri at 6 months followed by repeat follow - up at 12 and 24 months . 
repeat mri was avoided for patients with lesions with similar size and morphology at mri and us that was con rmed as broadenoma on histology after us - guided biopsy . 
 thereafter , the relative abilities of breast mri and secondlook us to accurately characterise incidental enhancing lesions was determined for all histologically proven lesions and all lesions referred for follow - up . 
for this latter assessment , lesions considered bi - rads 4 or 5 on breast mri were considered true positive ( tp ) for malignancy if histology subsequently revealed a malignant lesion but false positive ( fp ) if histology revealed a benign lesion . 
 conversely , lesions classi ed as bi - rads 3 on mri were considered true negative ( tn ) if histology or follow - up subsequently revealed a benign lesion but false negative ( fn ) if histology or follow - up revealed a malignant lesion . 
 likewise , a tp malignant lesion on second - look us was a lesion demonstrating malignant features ( bi - rads 45 ) that was con rmed as malignant on histology ; an fp lesion was one that demonstrated malignant features con rmed as benign at histology . 
finally , a tn lesion on second - look us was one that demonstrated benign features ( bi - rads 23 ) and was con rmed as benign at histology or followup ; an fn lesion was one that demonstrated benign features but was con rmed as malignant at histology . 
sensitivity , sono state associate pi frequentemente a lesioni benigne ; le curve di tipo ii caratterizzate da un rapido e precoce incremento dellintensit del segnale seguito dal raggiungimento di un plateau dellintensit del segnale sono state considerate borderline ; le curve di tipo iii comprendenti curve con rapido e precoce incremento dellintensit di segnale seguito da un rapido washout del mezzo di contrasto sono state invece considerate come indicative di malignit [ 1315 ]  . 
in relazione alla classi cazione bi - rads quindi una lesione con morfologia spiculata , orletto periferico di impregnazione post - contrastogra ca , bordi sfumati e rapido washout , tipicamente dovrebbe essere giudicata come bi - rads 5 . 
di tutte le lesioni sono state documentate le dimensioni in modo da rendere possibile i successivi confronti . biopsia delle lesioni tutte le lesioni riscontrate occasionalmente alla risonanza magnetica , considerate come categorie 3 , 4 o 5 secondo la classi cazione bi - rads [ 8 ] e con caratteristiche di sospetto al second - look ecogra co ( birads 4 - 5 ) , immediatamente dopo il controllo ecogra co mirato sono state sottoposte ad esame istologico . 
le lesioni incidentali , de nite bi - rads 3 alla risonanza magnetica della mammella e con un corrispettivo ecogra co benigno o probabilmente benigno ( bi - rads 2 - 3 ) , sono state indirizzate ad una strategia terapeutica conservativa , comprensiva di un follow - up iniziale con risonanza magnetica ed ecogra a bilaterale delle mammelle a 6 mesi e con la ripetizione di tali esami a 12 e 24 mesi . 
per le lesioni de nite sospette alla risonanza magnetica ( birads 4 - 5 ) , per le quali tuttavia non era stato possibile individuare un corrispettivo ecogra co la biopsia percutanea stata effettuata sotto guida rm , mentre le lesioni classi cate come bi - rads 3 alla risonanza magnetica della mammella sono state trattate in maniera conservativa con uniniziale risonanza magnetica della mammella eseguita a 6 mesi e successivamente a 12 e 24 mesi . 
le pazienti , con reperti benigni aspeci ci alla biopsia percutanea sotto guida ecogra ca , sono state sottoposte nuovamente a rm della mammella dopo un mese , per confermare che fosse stata bioptizzata la lesione corretta . 
in caso di pazienti con lesioni con morfologia e dimensioni simili sia alla rm che allesame ecogra co e confermate broadenomi allesame istologico dopo biopsia percutanea sotto guida ecogra ca , la ripetizione della risonanza magnetica stata evitata . analisi statistica stata valutata lindividuazione delle lesioni al secondradiol med ( 2011 ) 116 : 886904 speci city , accuracy and positive ( ppv ) and negative ( npv ) predictive values of breast mri and second - look us for the characterisation of incidental enhancing lesions was then determined for all incidental lesions detected on mri . 
analysis was performed using a general linear mixed model ( glimmix ; sas version 9.2 ) , adapted to t a model having sensitivity , speci city , accuracy , ppv or npv as the dependent variable ( distributed as a binary and introduced in the model by means of a logit link function ) ; and techniques ( xed effect ) , patients and lesions ( random effects ) as independent variables . 
analyses were also performed to compare detection and characterisation of mass - like and non - mass - like lesions on mri and secondlook us , the relative difference in size of incidental lesions detected on both mri and second - look us and detection of lesions on second - look compared with rst - look us . 
finally , comparison of lesion detection on second - look compared with rst - look us was performed using mcnemars test at a signi cance level of p < 0.05. 
of these 58 patients , 46 ( mean age 50.711.5 years ; range 2175 years ) underwent second - look high - resolution us directed at the site of the incidental nding and had either pathology results or full 24 - month follow - up information available . 
three patients were excluded because second - look us information was not available ( patients changed hospital ) , whereas nine patients were excluded because complete 24 - month follow - up information was missing . 
 quindi attraverso lanalisi di tutte le lesioni sottoposte ad esame istologico , pi tutte quelle sottoposte a follow - up , sia per la rm mammaria che per il second - look ecograco mirato , stata calcolata la capacit di caratterizzare in maniera accurata le lesioni occasionali . 
a tale scopo le lesioni classi cate come bi - rads 4 o 5 alla rm mammaria , sono state considerate come veri positivi ( vp ) per la malignit , se confermate maligne allesame istologico mentre sono state considerate falsi positivi ( fp ) , nel caso in cui lesame istologico abbia mostrato la presenza di una lesione benigna . 
cos al contrario , le lesioni classi cate bi - rads 3 alla rm della mammella , sono state reputate vp , quando lesame istologico o il follow - up abbiano rivelato la loro natura benigna e fp quando abbiano rivelato la loro natura maligna . 
quindi una lesione maligna , vp al second - look ecogra co , stata considerata una lesione con caratteristiche di malignit ( bi - rads 4 o 5 ) , confermata tale allesame istologico , mentre una lesione fp stata considerata una lesione con caratteristiche maligne , ma giudicata benigna allesame istologico . 
in ne stato de nito vn al second - look ecogra co , una lesione con caratteristiche benigne ( bi - rads 2 o 3 ) confermate tali allesame istologico , mentre una lesione fn stata considerata una lesione con caratteristiche di benignit , ma maligna allistologia . 
 per tutte le lesioni riscontrate occasionalmente alla rm della mammella sono stati calcolati sensibilit , speci cit , accuratezza ed i valori predittivo positivo ( vpp ) e negativo ( vpn ) rispettivamente sia della rm mammaria che del second - look ecogra co relativi alla caratterizzazione di tali reperti . 
lanalisi statistica stata condotta mediante limpiego di un modello misto lineare generalizzato ( glimmix , sas version 9.2 ) , adattato ad un modello avente sensibilit , speci cit , accuratezza , vpp o vpn come variabili dipendenti ( distribuite attraverso un sistema binario ed introdotte nel sistema mediante una funzione link logit ) e tecniche ( effetto sso ) e pazienti , lesioni ( effetto casuale ) come variabili indipendenti . 
la sensibilit stata stimata in base al tipo di lesione ( lesione di tipo nodulare o non nodulare ) e confrontata tra i diversi tipi attraverso il test esatto di fisher . 
lanalisi statistica stata compiuta anche per confrontare lindividuazione e caratterizzazione delle lesioni alla rm ed al second - look ecograco , la relativa differenza nelle dimensioni delle lesioni occasionali osservate alla rm ed al second - look ecogra co e per confrontare lindividuazione delle lesioni al secondlook ecogra co rispetto al rst look ecogra co . 
quarantasei di queste 58 pazienti ( et media : 50 , 711 , 5 anni ; intervallo di et 2175 anni ) , con a disposizione i risultati dellesame istologico o del follow - up completo a 24 mesi , sono state sottoposte anche a second - look ecogra co , mirato alla valutazione dellarea , sede del reperto riscontrato occasionalmente . 
tre pazienti sono state escluse per la non disponibilit di informazioni relative al second - look ecogra co ( le pazienti avevano cambiato ospedale ) mentre altre 9 sono state escluse per la mancanza delle informazioni relative al follow - up completo a 24 mesi . 
complessivamente sono state individuate 55 lesioni incidentali con impregnazione postcontrastogra ca , delle quali 24 classi cate come bi - rads 3 , 22 come bi - rads 4 e 9 come bi - rads 5 alla rm . 
queste 55 lesioni sono state identi cate nella stessa mammella in 25 / 46 pazienti ( 26 lesioni ) e nella mammella controlaterale in 21 / 46 pazienti ( 29 lesioni , comprendenti 2 pazienti con patologia multifocale di riscontro occasionale per un totale di 9 lesioni ) ; 39 lesioni erano inoltre di tipo nodulare ( mass - like ) mentre 16 di tipo non nodulare ( non mass - like )  . 
 le dimensioni di tutte lesioni occasionali alla rm della mammella , sono risultate comprese tra 3 e 13 mm ( dimensione media : 72 , 2 mm ) eccetto 5 di dimensioni 1 c il second - look ecogra co stato eseguito su tutte le regioni corrispondenti alle 55 lesioni individuate in maniera occasionale alla rm mammaria . istologia delle lesioni la biopsia percutanea o escissionale stata effettuata su 34 ( 61 , 8% ) delle 55 lesioni incidentali in 31 / 46 pazienti . 
1 diagramma di usso che mostra i criteri di selezione e valutazione dei pazienti . were detected in the ipsilateral breast in 25 / 46 patients ( 26 lesions ) and the contralateral breast in 21 / 46 patients ( 29 lesions , including two patients with incidental multifocal disease , for a total of nine lesions ) and included 39 lesions that were mass - like and 16 that were non - mass - like . 
the size of the incidental lesions detected on breast mri ranged from 313 mm ( mean size 72.2 mm ) , with all but ve lesions 1 cm in diameter . 
second - look us was performed at the sites of all 55 incidental enhancing lesions detected at breast mri . lesion histology core needle or excisional biopsy was performed for 34 ( 61.8% ) of the 55 incidental enhancing lesions in 31 / 46 patients . 
2a - c a 68 - year - old woman with a parenchymal distortion in the upper outer quadrant of the left breast , con rmed to be an invasive lobular carcinoma ( ilc ) at pathology after core biopsy , at mammography and negative ultrasound ( us )  . 
the transverse contrast enhanced t1 - weighted subtracted magnetic resonance image ( mri ) ( tr / te / fa = 8.1ms / 4 ms / 30 ) reveals an enhancing mass ( arrow ) with spiculated margins in the lower outer quadrant of the left breast ( a )  . 
2a - c donna di 68 anni con distorsione parenchimale ( carcinoma lobulare invasivo allesame istologico dopo biopsia percutanea ) nel quadrante superiore esterno ( qse ) della mammella di sinistra alla mammogra a ed ecogra a negativa . 
limmagine di rm ( sequenza t1 pesata , sottratta , dopo somministrazione di mezzo di contrasto ; tr / te / fa = 8 , 1 ms / 4 ms / 30 ) mostra una massa con impregnazione postcontrastogra ca ( freccia ) a margini spiculati nel quadrante inferiore esterno ( qie ) della mammella di sinistra ( a )  . 
la lesione stata sottoposta a resezione dopo posizionamento di repere sotto guida ecogra ca e confermata maligna ( carcinoma lobulare invasivo ) dallesame istologico . performed under us guidance for 31 / 34 lesions in 28 / 31 patients and under mri guidance for the remaining 3 / 34 lesions in 3 / 31 patients . 
however , the positive diagnosis of invasive ductal carcinoma ( idc ) and ductal carcinoma in situ ( dcis ) for the ve biopsied lesions led to both patients undergoing quadrantectomy . 
 mri - guided biopsy was performed in two patients because no lesions were detected on second - look us , whereas in the third patient , mri - guided biopsy was performed for one of two lesions not detected on second - look us despite depiction of two correlate lesions with benign features on second - look us . 
la biopsia stata eseguita sotto guida ecogra ca per 31 / 34 lesioni in 28 / 31 pazienti e sotto guida rm per le rimanenti 3 / 34 lesioni in 3 / 31 pazienti . 
in ogni caso la diagnosi positiva di carcinoma duttale in ltrante ( cdi ) e di carcinoma duttale in situ ( cdis ) per le 5 lesioni sottoposte a biopsia ha fatto s che entrambe le pazienti andassero incontro a quadrantectomia . 
la biopsia rm - guidata stata svolta in 2 pazienti per lassenza di lesioni al second - look ecogra co , mentre nella terza paziente la biopsia sotto guida rm stata eseguita su una delle 2 lesioni non evidenziabile al second - look ecograco , nonostante lindividuazione di 2 lesioni correlate , con caratteristiche benigne , al second - look ecogra co . 
3a - c a 63 - year - old woman with a suspicious lesion in the upper outer quadrant of the left breast [ invasive ductal carcinoma ( idc ) at cytology ] at mammography and ultrasound ( us ) and negative examination in the contralateral breast . 
the transverse contrast - enhanced t1 - weighted gradient - echo subtracted magnetic resonance image ( mri ) ( tr / te / fa = 8.1m / 4 ms / 30 ) reveals an enhancing lesion ( arrow ) in the lower outer quadrant of the right breast ( a )  . 
the lesion has smooth and irregular margins , and the signal intensity / time ( si / t ) curve was considered to be type i [ breast imaging reporting and data system ( bi - rads ) 3 at mri ] ( b )  . 
3a - c donna di 63 anni , recentemente sottoposta a mastoplastica additiva , con lesione sospetta nel qse della mammella di sinistra ( carcinoma duttale invasivo allesame citologico ) alla mammogra a ed ecogra a della mammella controlaterale negativa . 
limmagine di rm ( sequenza gre t1 pesata , sottratta , dopo somministrazione di mezzo di contrasto ; tr / te / fa = 8 , 1 ms / 4 ms / 30 ) rivela una lesione con impregnazione post - contrastogra ca ( freccia ) nel qie della mammella destra ( a )  . 
lesame istologico de nitivo ha rivelato uniperplasia lobulare atipica . hyperplasia , and one ( 3.0% ) each lobular carcinoma in situ ( lcis ) , brocystic dysplasia , atypical lobular hyperplasia , broadenoma , papillomatosis , radial scar , intramammary lymph node ]  . 
three lesions classi ed as bi - rads 4 at mri were subsequently con rmed as benign at histology ( one broadenoma , one intramammary lymph node and one radial scar ) and were considered fp for subsequent analyses . 
tre lesioni classi cate bi - rads 4 alla rm sono state successivamente de nite benigne allesame istologico ( 1 broadenoma , 1 linfonodo intramammario , 1 radial scar ) e quindi considerate fp per le successive valutazioni . 
lesions detected on second - look us included 36 ( 92.3% ) of the 39 su tutte le informazioni radiologiche e cliniche raccolte nei 24 mesi successivi , ha confermato la benignit di tutte e 17 le lesioni . second - look ecogra co il second - look ecogra co ha identi cato 42 delle 55 lesioni aggiuntive in 38 ( 82 , 6% ) delle 46 pazienti . 
considerando che le lesioni evidenti al rst look ecogra co erano apprezzabili anche al second - look ecogra co , lindividuazione delle lesioni al second - look ecogra co , in confronto al primo esame ecogra co , stata estremamente signi cativa tabella 1 confronto tra lindividuazione delle lesioni occasionali , con impregnazione post - contrastogra ca al second - look ecogra co ed alla risonanza magnetica della mammella , per lesioni con conferma allesame istologico lesioni occasionali alla rm della mammella confermate istologicamente reperti al second - look ecogra co paziente no . 
tra le lesioni osservate al secondlook ecogra co vi sono state 36 ( 92 , 3% ) delle 39 lesioni di tipo nodulare evidenziate alla rm , ma solamente 6 ( 37 , 5% ) delle 16 lesioni di tipo non nodulare . 
4a - d a 55 - year - old woman with a cluster of suspicious microcalci cations in the lower outer quadrant of the left breast [ con rmed to be an invasive ductal carcinoma ( idc ) at pathology after core biopsy ] at mammography . 
the transverse contrast - enhanced t1 - weighted gradient - echo ( gre ) subtracted magnetic resonance image ( mri ) ( tr / te / fa = 8.1ms / 4 ms / 30 ) reveals four enhancing nodules with irregular margins in the upper inner quadrant of the right breast ( arrows ) ( a )  . 
despite the si / t curve , the lesions were classi ed as breast imaging reporting and data system ( bi - rads ) 4 on mri because of the morphology . 
4a - d donna di 55 anni con un cluster di microcalci cazioni sospette nel qie della mammella di sinistra ( carcinoma duttale invasivo allesame istologico dopo biopsia percutanea ) alla mammogra a . 
limmagine di rm ( sequenza gre t1 pesata , sottratta , dopo somministrazione di mezzo di contrasto ; tr / te / fa = 8 , 1 ms / 4 ms / 30 ) rivela quattro noduli con impregnazione post - contrastogra ca nel qsi della mammella di destra ( frecce ) ( a )  . 
 le 42 lesioni osservate al second - look ecogra co hanno incluso 21 ( 75 , 0% ) delle 28 ( 24 lesioni sottoposte a biopsia pi 4 lesioni nelle pazienti con patologia multifocale ) lesioni confermate maligne alla rm mammaria e 21 ( 77 , 8% ) delle 27 lesioni che sono state successivamente confermate ( 10 lesioni alla biopsia ) o diagnosticate ( 17 lesioni dopo il follow - up ) come benigne . 
in tutte queste pazienti le lesioni non evidenziabili al second - look ecogra898 radiol med ( 2011 ) 116 : 886904 lesions ( three idc , two dcis ) detected on breast mri and classi ed as bi - rads 4 were present in two patients with incidental multifocal disease who subsequently underwent quadrantectomy . 
at nal diagnosis after follow - up mri , three of these lesions were considered benign , whereas two lesions , which occurred in two premenopausal patients of 32 and 42 years , could not be seen on follow - up mri or us and were considered transient areas of enhancement arising due to the hormonal status of the women at the time of the initial mri examination . 
considering lesions not seen on second - look us as either tn or fn , if the corresponding lesion on mri was tn or tp , respectively , there were 18 tp , eight fp , 19 tn and ten fn lesions on second - look us . 
although evaluation of differences in sensitivity and npv was not possible because of the absence of fn ndings with mri , a signi cant ( p = 0.0021 ) bene t for mri over secondlook us was noted for overall accuracy for depicting lesions . 
differences in the characterisation of mass - like and non - mass - like lesions on second - look us are shown co avevano dimensioni 5 mcomplessivamente il grado di con denza diagnostica del second - look ecogra co per le lesioni presenti sia alla rm che al second - look ecogra co stato pari al 73 , 5% ( 95% intervallo di con denza [ ci ] : 63%86 , 8% ) ma del 92 , 3% ( 95% ci : 79 , 1%98 , 4% ) solo per le lesioni di tipo nodulare . 
tra le 13 lesioni non riscontrabili al second - look vi stato 1 cli di 5 mm classi cato come bi - rads 5 alla rm e 2 casi confermati di cdis di 7 mm precedentemente classi cati come bi - rads 4 ( tabella 1 )  . 
5 ulteriori lesioni ( 3 cdi , 2 cdis ) identi cate alla rm della mammella e classi cate come bi - rads 4 sono state apprezzate nelle due pazienti con patologia multifocale , diagnosticata in via occasionale , che successivamente sono state sottoposte a quadrantectomia . 
second - look us sensitivity ( % ) speci city ( % ) accuracy ( % ) ppv ( % ) npv ( % ) 100 ( 28 / 28 ) 88.9 ( 24 / 27 ) 94.6 ( 52 / 55 ) 90.3 ( 28 / 31 ) 100 ( 24 / 24 ) 64.3 ( 18 / 28 ) 70.4 ( 19 / 27 ) 67.3 ( 37 / 55 ) 69.2 ( 18 / 26 ) 65.5 ( 19 / 29 ) analysis performed using general linear mixed model nc , not calculable ; ppv , positive predictive value ; npv , negative predictive value tabella 2 performance diagnostica del second - look ecogra co confrontata con la rm della mammella per la caratterizzazione di 55 lesioni incidentali alla rm parametri di performance diagnostica second - look ecogra co rm vs . 
the three mass - like lesions among the 13 unseen lesions were 6 , 6 and 7 m the slightly larger size of lesions detected at second - look us compared with mri was con rmed by bland - altman analysis . 
given the increasingly widespread use of breast mri and its acknowledged high sensitivity for detecting lesions [ 1628 ] , a potential dilemma arises when incidental abnormal foci of enhancevp , 3 fp , 24 lesioni vn e nessun fn . 
attribuendo il valore di vn o fn alle lesioni non viste al second - look ecogra co , a seconda che le corrispettive lesioni alla rm fossero vn o vp , rispettivamente , al second - look ecogra co si sono osservate 18 lesioni vp , 8 lesioni fp , 19 lesioni vn e 10 fn . 
sebbene una stima delle differenze nella sensibilit e nel vpn non sia stata possibile a causa del mancato riscontro di reperti fn alla rm , complessivamente stato registrato un vantaggio signi cativo ( p = 0 , 0021 ) nellaccuratezza diagnostica della rm rispetto al second - look ecograco . 
per la caratterizzazione delle lesioni di tipo nodulare rispetto a quelle di tipo non nodulare stata osservata una signi cativa , maggiore performance in termini di sensibilit ( p = 0 , 026 ) ed accuratezza ( p = 0 , 0428 )  . dimensioni delle lesioni la dimensione media delle 42 lesioni evidenziate al secondlook ecogra co stata di 7 , 952 , 56 malla rm le stesse lesioni avevano dimensioni pari a 7 , 382 , 28 mla differenza tra second - look ecogra co e rm ( 0 , 570 , 94 mm ) , nelle dimensioni medie , stata signi cativa ( p = 0 , 0003 )  . 
tra le 13 lesioni non osservate , 3 misuravano 6 , 6 e 7 mil fatto che le dimensioni delle lesioni al second - look ecogra co fossero lievemente maggiori rispetto alla rm stato confermato con il test di bland - altman . discussione il ruolo della rm mammaria ampiamente riconosciuto per numerose situazioni cliniche [ 14 ]  . 
visto il ricorso , sempre pi frequente , alla rm della mammella e vista la sua ben nota , elevata sensibilit , nellidenti cazione delle lesioni [ 1628 ] , il riscontro occasionale di foci di impregnazione post - contrastogra ca , precedentemente non evidenziati agli esami convenzionali di mammogra a ed ecogra a , pu costituire un potenziale dilemma . 
per tale motivo il second - look ecogra co mirato viene considerato sempre di pi un passaggio necessario nella gestione delle pazienti con lesioni individuate incidentalmente alla rm mammaria e non evidenziate mammogra camente ed ecogra camente [ 2633 ]  . 
questo fenomeno legato anche ai recenti risultati che mostrano come le lesioni occasionali alla rm , con un corrispettivo ecogra co , abbiano una maggiore probabilit di essere maligne [ 2629 ] ed in parte al fatto che la biopsia sotto guida ecogra ca sia meno costosa e pi facilmente reperibile rispetto alla biopsia sotto guida rm [ 27 , 3436 ]  . 
in questo senso se una lesione evidenziata alla rm pu essere individuata anche ecogra 900 radiol med ( 2011 ) 116 : 886904 ment are revealed that had previously gone undetected on conventional mammography or us . 
for this reason , second - look - directed us is increasingly considered an integral step in managing patients with mammographically and sonographically occult breast lesions incidentally detected on breast mri [ 2633 ]  . 
in part , this re ects recent ndings that show that incidental enhancing lesions on mri that have a de nite us correlate are more likely to be malignant [ 2629 ] and in part the fact that biopsy under us guidance is less expensive and more readily available than biopsy under mri guidance [ 27 , 3436 ]  . 
in this setting , if a lesion detected at breast mri can be depicted with directed us , it may be amenable to us - guided percutaneous biopsy , which may spare the patient mri - guided biopsy . 
in our study , 55 incidental enhancing lesions , considered bi - rads 3 , 4 or 5 at mri , were detected in 46 ( 25.3% ) of 182 patients referred for preoperative breast mri for histologically con rmed breast cancer depicted on x - ray mammography and / or rst - look wholebreast us . 
 [ 27 ] , who identied a us correlate for 21 ( 23% ) of 93 lesions detected on breast mri , it should be noted that the authors also included patients with lesions classi ed as bi - rads 2 and that those patients comprised the majority of patients who would not have a second - look us correlate . in our study , patients with incidental lesions classi ed as bi - rads 2 were not included . 
 [ 28 ] , who found a de nite correlate on second - look us for 142 ( 82% ) of 173 lesions initially detected only on breast mri ; and those of destounis et al . 
 [ 26 ] , who retrospectively found 31 ( 57% ) of 54 mri - detected and histologically con rmed malignant lesions upon re - evaluation of previous mammograms and sonograms ; and wiratkapun et al . 
 [ 30 ] , who identi ed 46 ( 47% ) of 97 mri - detected lesions on targeted us in 55 women . given that precise topographic evaluation of the site of the incidental lesion is achievable with mri before the second - look us examination , it is perhaps not surprising that directed second - look us should prove effective at depicting even small lesions . 
notably , the mean size of the corresponding lesions on mri was smaller ( 7.382.28 ; p = 0.0003 ) , possibly re ecting the better resolution of camente , possibile pensare di effettuare la biopsia percutanea sotto guida ecogra ca risparmiando alla paziente la biopsia rm - guidata . 
inoltre lesecuzione della biopsia percutanea sotto guida ecogra ca pu accelerare la pianicazione preoperatoria della strategia terapeutica , nel caso in cui siano ottenuti dei risultati maligni [ 2 , 4 ]  . 
nel nostro studio in 46 ( 25 , 3% ) delle 182 pazienti , sottoposte a rm mammaria preoperatoria per la presenza di carcinoma mammario , confermato istologicamente e diagnosticato mammogra camente e / o attraverso lecogra a mammaria bilaterale , stato riscontrato occasionalmente un numero totale di 55 lesioni con potenziamento postcontrastogra co , classi cate come bi - rads 3 , 4 o 5 . 
 [ 27 ] , che hanno identi cato un corrispettivo ecogra co per 21 ( 23% ) delle 93 lesioni evidenziate alla rm , doveroso sottolineare che la trenta et al . 
 [ 27 ] hanno incluso anche pazienti con lesioni de nite bi - rads 2 , che costituiscono la maggior parte delle lesioni prive di un corrispettivo ecogra co al second - look . 
 [ 28 ] che hanno trovato un sicuro corrispettivo ecogra co al second - look per 142 ( 82% ) delle 173 lesioni inizialmente osservate solo alla rm e con quelli di destounis et al . 
 [ 26 ] che retrospettivamente , attraverso la rivalutazione dei precedenti esami mammogra ci ed ecogra ci hanno individuato 31 ( 57% ) delle 54 lesioni evidenti alla rm e confermate maligne allesame istologico e con quelli di wiratkapun et al . 
dal momento che con la rm possibile ottenere una precisa valutazione topogra ca della sede della lesione incidentale prima del second - look ecogra co forse non sorprende lef cacia del second - look ecogra co nellindividuazione anche di lesioni di piccole dimensioni . 
in particolare , la dimensione media delle lesioni corrispondenti alla rm era inferiore ( 7 , 382 , 28 ; p = 0 , 0003 ) , questo forse per la migliore risoluzione della rm . 
 [ 27 ] per le lesioni identi cate sia allesame di rm che ecogra co hanno riportato una dimensione media pari a 9 mm contro gli 8 mm registrati per le lesioni non evidenziabili allesame ecogra co . 
nel nostro studio 24 ( 57 , 1% ) delle 42 lesioni , con un corrispettivo ecogra co , sono state successivamente confermate maligne contro le 7 ( 53 , 4% ) delle 13 , per le quali non era stato possibile apprezzare un corrispettivo ecogra co . 
in our study , 24 ( 57.1% ) of the 42 lesions with a us correlate were subsequently con rmed as malignant compared with seven ( 53.4% ) of 13 lesions that did not have a us correlate . 
although this ratio does not re ect the ndings of previous studies that demonstrated a signi cantly higher likelihood of carcinoma among lesions with a us correlate than among lesions without a us correlate [ 27 , 29 , 33 ] , it can possibly be explained by the fact that the number of lesions without a us correlate was relatively small , and that four of the seven carcinomas that did not have a us correlate were very small ( 5 mm ) and occurred in two patients with incidental enhancing multifocal disease . 
although our ndings suggest that lesion detection on second - look us does not increase the likelihood that a lesion detected on mri is malignant , further work in a larger patient cohort should certainly be performed to clarify these ndings [ 37 ]  . 
discrepancies between us and breast mri among histologically con rmed malignant lesions were noted for two dcis lesions , which were considered to have benign features on second - look us . 
conversely , a broadenoma and an intramammary lymph node , which were misdiagnosed as malignant on breast mri , were both determined to have benign features on second - look us . 
more notable discrepancies between second - look us and breast mri occurred for con rmed benign lesions that were considered to have malignant or , more frequently , doubtful features on second - look us . 
this might have been due to the fact that only women with breast carcinoma were evaluated , which may have negatively in uenced the interpretation of second - look us images . 
a prospective study with randomised mr and second - look us images evaluated separately might have negated a possible bias towards more pessimistic interpretations . possible limitations of our study are : ( i ) evaluation was performed on a lesion - by - lesion basis without focusing i risultati degli studi precedenti , che hanno mostrato una signi cativa maggiore probabilit di malignit tra le lesioni prive di di un corrispettivo ecogra co [ 27 , 29 , 33 ] , in realt pu essere spiegato dal fatto che , il numero delle lesioni non riscontrate al second - look ecogra co stato relativamente basso e che 4 dei 7 carcinomi , che non avevano un corrispettivo ecogra co in realt avevano dimensioni molto piccole ( 5 mm ) e si erano presentati in due pazienti con malattia multifocale incidentale . 
sebbene i risultati del nostro studio suggeriscano che lindividuazione delle lesioni al controllo ecogra co mirato non si associ alla maggiore probabilit di malignit della lesione evidenziata alla rm , per chiarire questo punto sono necessari ulteriori studi condotti su una maggiore coorte di pazienti [ 37 ]  . 
questo per riconducibile al fatto che la nostra valutazione stata condotta solamente su pazienti con carcinoma mammario gi noto , nelle quali il rischio di carcinomi sincroni o omolaterali alla neoplasia nota , maggiore . 
 per quanto riguarda la performance diagnostica , la sensibilit , la speci cit , laccuratezza , il vpp e vpn della risonanza magnetica della mammella con gadobenatedimeglumine nel diagnosticare le lesioni con impregnazione post - contrastogra ca come maligne o benigne , i valori ottenuti sono stati rispettivamente 100% , 88 , 9% , 94 , 5% , 90 , 3% and 100% . 
in confronto per il second - look ecogra co sono stati ottenuti dei valori lievemente inferiori e pari a 90 , 5% , 61 , 9% , 76 , 2% , 70 , 4% ed 86 , 7% . 
tra le lesioni confermate come maligne allesame istologico , si sono riscontrate delle discrepanze tra esame ecogra co e rm mammaria , per due casi di cdis , ai quali al second - look ecogra co erano state attribuite caratteristiche di benignit . 
ulteriori importanti discrepanze tra second - look ecogra co e rm si sono veri cate per lesioni benigne , considerate maligne o comunque con caratteristiche di dubbia interpretazione al second - look ecogra co . 
 possibili limiti del nostro studio sono ( i ) che la valutazione stata condotta lesione per lesione senza mettere a fuoco limpatto esercitato dal rilevamento di lesioni occasionali sulla gestione del paziente , ( ii ) non abbiamo realizzato un sottogruppo per le pazienti con mammella densa , ( iii ) non abbiamo valutato in maniera speci ca pazienti con aumentato rischio di carcinoma mammario o pazienti 902 radiol med ( 2011 ) 116 : 886904 on the impact of the detected incidental enhancing lesions on patient management . 
as regards the latter issues , it is well established that detection of lesions on mammography is less reliable in women with very dense breast parenchyma [ 38 , 39 ] whereas studies have shown that it is not infrequent that benign - appearing lesions on mri may , in fact , be malignant in high - risk women with proven or pro le - like germ - line mutations [ 40 ]  . 
in our study , 24 - month follow - up was considered suf cient to diagnose benign lesions in women with benign - appearing lesions on mri with or without second - look us corroboration . 
nevertheless , future prospective work should be performed to evaluate the role of second - look us speci cally in women with proven or pro le - like germ - line mutations . 
likewise , further work should speci cally address the issue of incidental lesions classi ed as bi - rads 2 on mri . in conclusion , results of our analysis con rm that directed second - look us is a valuable technique for depicting and diagnosing incidental enhancing lesions detected on preoperative mri . 
if a lesion can be depicted with us , it may be amenable to us - guided percutaneous biopsy , which is less expensive and a more straightforward procedure than mri - guided biopsy . 
on the other hand , due to the similar rate of malignancy regardless of whether a de nite correlate is found on secondlook us , the absence of us correlate lesions should not preclude mri - guided biopsy of suspicious ( bi - rads 4 and 5 ) lesions detected on mri . 
per quanto riguarda le ultime questioni ben dimostrato che lidenticazione delle lesioni alla mammogra a , nelle pazienti con mammella densa , meno attendibile [ 38 , 39 ] mentre studi hanno dimostrato come nelle pazienti con elevato rischio di carcinoma mammario , con mutazione provata o pro lo simile a mutazioni della linea germinale , lesioni con caratteristiche di benignit alla rm possano essere invece essere maligne [ 40 ]  . 
nel nostro studio un periodo di follow - up a 24 mesi stato ritenuto suf ciente per considerare benigne lesioni con caratteristiche di benignit alla rm , indipendentemente dalla conferma del second - look ecogra co . 
in ogni caso necessario che nel futuro vengano condotti degli studi per valutare in maniera speci ca il ruolo del second - look ecogra co nella valutazione di donne con mutazione genetica accertata o aventi pro lo simile a mutazioni della linea germinale . 
 in conclusione i risultati del nostro studio confermano che , il second - look ecogra co mirato , costituisce una tecnica attendibile per lidenti cazione e diagnosi di lesioni riscontrate occasionalmente alla risonanza magnetica preoperatoria della mammella . 
marini1 1istituto di scienze radiologiche , policlinico umberto i , universit degli studi sapienza roma , viale regina elena 324 , 00161 roma , italy 2dipartimento di scienze radiologiche , ospedale pediatrico meyer , viale pieraccini 24 , careggi , italy 3chirurgia maxillo - facciale , policlinico umberto i , universit degli studi sapienza roma , viale regina elena 324 , 00161 roma , italy correspondence to : a . 
we enrolled 24 pregnant women ( 27 fetuses ) ( mean gestational age 23.7 weeks ) with a level - two us diagnosis of cleft lip ( cl ) or clp with or without associated central nervous system ( cns ) or facialbone anomalies . 
mri con rmed the diagnosis in 16 / 25 fetuses and added information about the extent of the cleft and the degree of involvement of the anterior and posterior palate in 8 / 25 fetuses . 
in the study of clp fetal , mri is able to de ne the degree of involvement of the posterior palate and the lateral extent of the cleft with higher diagnostic accuracy than us . 
abbiamo prospettivamente arruolato 24 donne in gravidanza ( 27 feti ; et gestazionale media 23 , 7 settimane ) con diagnosi ecogra ca di ii livello di lbs o lps , associata o meno ad anomalie cranio - encefaliche o del massiccio facciale ; le pazienti sono state sottoposte a rm fetale per lo studio del massiccio facciale , oltre che del sistema nervoso centrale ( snc ) e del body fetale . 
la rm ha confermato la diagnosi ecogra ca in 16 / 25 feti ed ha aggiunto informazioni riguardo lestensione della schisi ed il coinvolgimento del palato in 8 / 25 feti ; ha smentito la diagnosi in 1 / 25 feti . 
lo studio rm fetale del massiccio facciale radiol med ( 2011 ) 116 : 11341148 1135 study of the fetal head and biometric development of the facial bones , thus enabling early detection of potential syndromic conditions . keywords fetal mri facial cleft cleft lip and palate prenatal diagnosis nelle lbs - lps de nisce con maggiore accuratezza il grado di coinvolgimento del palato posteriore e la lateralit ; consente , inoltre , una valutazione del distretto cranioencefalico e dello sviluppo biometrico del massiccio facciale al ne di identi care precocemente eventuali condizioni sindromiche . parole chiave rm fetale labioschisi labio - palatoschisi diagnosi prenatale introduction introduzione cleft lip and palate ( clp ) is the most common facial malformation , having an incidence of around 1 / 700 live births [ 1 ]  . 
this malformation may be isolated or associated with genetic syndromes ; in fact , around 11% of patients with cleft lip ( cl ) also have one of more than 170 monogenic syndromes reported in the london dysmorphology database . 
therefore , the presence of an orofacial cleft associated with changes to the main biometric parameters of the fetal face should be considered a warning sign and prompt a fetal chromosome analysis in the search for possible syndromes and multiple anomaly conditions . in this setting , the ultrasound ( us ) examination plays a key role in the early prenatal diagnosis of cl , and especially in the identi cation of clp . 
accurate evaluation of the extension of the cleft underpins a correct diagnosis , parent counselling and treatment planning [ 5 ]  . study of the fetal face has in recent years relied not only on the traditional 2d us examination but also on new 3d and 4d techniques . 
these have made it possible to visualise all of the critical structures of the face ( forehead , eyes , nasal bones and nares , lips , chin ) with single - volume acquisitions , thus markedly increasing the accuracy in the diagnosis of secondary palate anomalies with the possibility of multiplanar reconstructions [ 68 ]  . 
these include surface rendering , which is able to produce images of the facial skin and soft tissues ; and transparency mode , which offers speci c images of the facial bones [ 9 ]  . fetal magnetic resonance imaging ( mri ) is progressively becoming a robust level - three technique in the diagnosis of facial anomalies , thanks to the advent of ultrafast sequences that suffer few motion artefacts and offer excellent spatial resolution . 
the aim of our study was to evaluate the role of fetal mri as a complement to us in diagnosing clp , whether isolated or associated with syndromes and multiple anomaly conditions . la labiopalatoschisi ( lps ) rappresenta lanomalia congenita del massiccio facciale di pi frequente riscontro ; la sua incidenza di circa 1 / 700 nati vivi [ 1 ]  . 
tale malformazione pu essere isolata o rientrare nel contesto di sindromi genetiche ; circa l11% dei pazienti affetti da schisi labiale ( lbs ) , infatti , pu essere inquadrato nel contesto di una delle oltre 170 sindromi monogeniche riportate nel london dysmorphology database . 
di conseguenza , in epoca prenatale , la presenza di schisi facciale associata ad alterazioni dei principali diametri del massiccio deve essere considerata un segnale dallarme ed indurre ad eseguire unanalisi cromosomica fetale e a ricercare eventuali condizioni polimalformative sindromiche e non . in tal senso lesame ecogra co riveste un ruolo chiave per la diagnosi prenatale precoce delle lbs , e soprattutto per lidenti cazione del coinvolgimento palatale ( lps ) ; laccurata de nizione dellestensione del cleft alla base di un corretto inquadramento diagnostico , del counseling con i genitori e della piani cazione terapeutica [ 5 ]  . lo studio del massiccio facciale si avvalso negli ultimi anni , oltre che del tradizionale esame ultrasonograco 2d , delle nuove tecniche 3d e 4d , le quali consentono di visualizzare tutte le strutture critiche della faccia ( fronte , occhi , ossa nasali e narici , labbra , mento ) con singole acquisizioni volumetriche , incrementando notevolmente laccuratezza diagnostica nei difetti del palato secondario con la possibilit di ricostruzioni multiplanari [ 68 ]  . 
inoltre , ad oggi sono disponibili ulteriori tecniche di ricostruzione ecogra che 3d e 4d , quali il surface rendering , che consente di ottenere immagini dei tessuti molli e del piano cutaneo del viso , e il trasparency mode , che permette di ottenere immagini speci che delle strutture ossee facciali [ 9 ]  . la risonanza magnetica ( rm ) fetale , grazie allavvento di sequenze ultraveloci , scarsamente artefattate dal movimento e dotate di ottima risoluzione spaziale , si sta progressivamente affermando , come esame di iii livello , anche 1136 materials and methods between may 2007 and april 2010 , we prospectively enrolled 24 pregnant women ( three twin pregnancies , n = 27 fetuses ) with a level - two us diagnosis of cl or clp with or without associated anomalies of the head , brain or face . 
only 14 / 24 women had undergone amniocentesis , which in all cases de ned a normal karyotype ( 5xy fetuses , 9 xx fetuses ) [ ce1 ]  . imaging technique the fetal mri study was performed with a 1.5 - t system ( siemens somatom avanto ) with 32 - channel phased - array coils used in combination with a spinal coil . 
 lo scopo del nostro studio valutare il ruolo complementare , rispetto allesame ecogra co , della rm fetale nellinquadramento delle labiopalatoschisi isolate e associate a quadri sindromici o polimalformativi . materiali e metodi tra maggio 2007 e aprile 2010 abbiamo prospettivamente arruolato 24 donne in gravidanza ( 3 gravidanze bi - gemellari , 27 feti totali ) con diagnosi ecogra ca di ii livello di lbs o lps , associata o meno ad altre anomalie cranioencefaliche o del massiccio facciale . 
tutte le pazienti sono state sottoposte ad esame di rm fetale per lo studio del massiccio facciale , oltre che del sistema nervoso centrale ( snc ) e del body fetale . 
solamente 14 / 24 pazienti avevano effettuato lamniocentesi de nendo un cariotipo normale in tutti i casi ( 5 feti xy , 9 feti xx )  . tecnica di imaging lesame di rm fetale stato effettuato con ununit a 1 , 5 t ( siemens somatom avanto ) , con bobine di super cie phased - array a 32 canali associate a una bobina spine integrata . 
 tutte le donne sono state sottoposte allesame senza alcun tipo di sedazione , n sulle donne stesse n sul feto , e senza somministrazione di mezzo di contrasto ; preventivamente le pazienti , attraverso la compilazione di un questionario relativo alla gravidanza e allanamnesi personale e familiare , hanno sottoscritto il proprio consenso informato . 
1a - h scanning planes to evaluate the main structures of the splanchnocranium : a - e axial plane ( white arrows : b orbits and eyes , c septum and nasal cavity , d upper jaw with dental roots , e lower jaw with dental roots ) ; f - h sagittal plane ( white arrows : g corpus callosum and palate , h upper lip ) fig . 
1a - h piani di scansione rm per lo studio del massiccio facciale : a - e piano assiale ( frecce bianche : b cavit orbitarie e globi oculari , c fosse nasali e setto nasale , d mascellare superiore con processi alveolari , e mascellare inferiore con processi alveolari ) ; f - h piano sagittale ( frecce bianche : g corpo calloso e palato , h labbro superiore )  . 1138 radiol med ( 2011 ) 116 : 11341148 maxilla and mandible with their tooth buds . 
the sagittal plane is the reference plane for the study of the facial pro le ( particularly useful for evaluating the forehead and its relationship with the nasal structures and the chin ) and the primary and secondary palate , which can best be visualised with a median plane normally used in the brain for studying the corpus callosu this scan is also used to evaluate the tongue and upper airways from the nasal cavities to the pharyngolaryngeal structures . 
the coronal plane is useful for evaluating the entire face and is especially suitable for studying the orbits , nose and nostrils , upper lip and mouth and the ch lastly , the paracoronal plane ( nosemouth scan ) is the reference plane in the evaluation of cl , given its usefulness in the study of the integrity of the upper lip and the normal morphology of the nostrils . 
sul piano assiale abbiamo valutato la posizione e la morfologia delle orbite e dei globi oculari , il setto e le fosse nasali , il mascellare superiore e la mandibola con le relative gemme dentarie . 
 il piano sagittale il piano di riferimento per lo studio del pro lo facciale ( particolarmente utile per la valutazione della fronte , anche in rapporto con le strutture nasali , e del mento ) e del palato anteriore e posteriore attraverso lacquisizione di un piano mediano normalmente utilizzato nellencefalo per lo studio del corpo calloso . 
il piano coronale utile per la valutazione del viso nel suo complesso , in particolare consente lo studio delle orbite , del naso e delle narici , del labbro superiore , della bocca e del mento . 
2a - c scanning planes to evaluate the main structures of the splanchnocranium : a , b coronal plane ( white arrows : b orbits and eyes ) ; c paracoronal plane ( black arrows : nostrils ; white arrow : upper lip ) fig . 
2a - c piani di scansione rm per lo studio del massiccio facciale : a , b piano coronale ( freccia bianca : b cavit orbitarie e globi oculari ) ; c piano paracoronale ( frecce nere : narici ; freccia bianca : labbro superiore )  . radiol med ( 2011 ) 116 : 11341148 1139 with the calculation of the jaw index , de ned as the ratio between apd and bpd ; inferior facial angle ( ifa ) , measured in the midsagittal plane of the head , between a line passing through the frontonasal junction , perpendicular to the forehead , and passing through the anterior border of the upper lip and the chin ; frontomaxillary angle ( fma ) , measured in the midsagittal plane and given by a line passing through the forehead and chin and another passing through the upper border of the palate ; biorbital ( bod ) and intraorbital ( iod ) diameter by tracing a line between the external and internal margins of the two orbits , respectively . results a total of 25 / 27 fetuses had a us diagnosis of cl - clp . 
in 6 / 24 fetuses with cl - clp , the mr study revealed abnormalities in the following parameters with respect to normal development of the fetal face : ifa , fma , iod . 
we considered normal the fetuses with these parameters in the normal range , as de ned by the 2d / 3d us study and reported in the literature [ 12 , 19 , 20 ]  . we found an abnormal ifa in three fetuses with clp riferimento nella valutazione dei cleft labiali , consentendo lo studio dellintegrit del labbro superiore e della normale morfologia delle narici . 
in sede di refertazione , abbiamo inoltre analizzato 7 parametri di riferimento [ 1214 ] per la valutazione biometrica del massiccio facciale : diametro fronto - occipitale osseo ( dfoo ) , misurato su un piano sagittale mediano dellestremo cefalico ; diametro antero - posteriore della mandibola ( dapm ) e diametro biparietale della mandibola ( dbpm ) , misurati su un piano assiale dellestremo cefalico , determinando il jaw index , de nito dal rapporto tra il dapm ed il dbpm ; angolo facciale inferiore ( ifa ) , misurato su un piano sagittale mediano del cranio , tra una linea passante per la giunzione fronto - nasale , perpendicolare alla fronte , e una passante per il bordo anteriore del labbro superiore e il mento ; angolo fronto - mascellare ( fma ) , misurato su un piano sagittale mediano dellestremo cefalico , dato da una linea passante per la fronte e il mento e unaltra passante per il margine superiore del palato ; diametro bisorbitario ( dbo ) ed interorbitario ( dio ) , misurati sul piano coronale , tracciando rispettivamente una linea tra i margini esterni ed interni delle due orbite . risultati venticinque / 27 feti avevano diagnosi ecogra ca di lbs - lps . 
 la rm ha confermato la diagnosi ecogra ca , determinando una concordanza completa tra le due metodiche , in 16 / 25 feti ; ha evidenziato una concordanza parziale in 8 / 25 feti ; ha smentito la diagnosi in 1 / 25 feti . 
labiopalatoschisi completa bilaterale con ampio cleft labiale e del palato anteriore e posteriore ( frecce bianche )  . with associated micrognathia , and an abnormal iod and above normal fma in the fetus with unilateral clp and associated holoprosencephaly , cyclopia and arachnoid cyst of the posterior cranial fossa . 
in addition , the fma was above normal in the fetus with unilateral clp , associated interventricular cardiac defect and borderline ventriculomegaly ; and in the fetus with unilateral cl , involvement of the primary palate , associated lateral shift of the nasal septum and mild bilateral ventriculomegaly . 
mr ndings were con rmed by the postnatal physical examination or autopsy ndings , which were considered the reference standard . discussion the facial skeleton is derived almost entirely from the mesenchyme of the rst three branchial arches , which consist of mesoderm , which develop lateroventrally in the deviazione del setto nasale e ventricolomegalia bilaterale lieve . 
lesame rm ha evidenziato in 6 / 24 feti , positivi per lbs - lps , unalterazione dei seguenti parametri riguardanti il normale sviluppo del massiccio facciale : ifa , fma , dio . 
abbiamo considerato come normali i feti che presentavano tali parametri nellambito dei range di normalit , de niti allesame ecogra co 2d / 3d , della letteratura [ 12 , 19 , 20 ]  . in particolare , abbiamo riscontrato unalterazione dellifa nei tre feti affetti da lps associata a micrognazia , del dio e dellfma , che risultava aumentato , nel feto affetto da lps unilaterale con oloprosencefalia alobare , ciclopia e cisti aracnoidea della fossa cranica posteriore ; inoltre lfma risultava aumentato nel feto affetto da lps unilaterale associata a difetto interventricolare cardiaco e ventricolomegalia bordeline , e nel feto affetto da labioschisi unilaterale con coinvolgimento del palato anteriore associata a laterodeviazione del setto nasale e ventricolomegalia bilaterale lieve . 
5a feto a 27 settimane + 2 giorni affetto da oloprosencefalia alobare con ipotelorismo ( b , riduzione diametro bisorbitario ) , nel quale lo studio rm ha smentito il rilievo ecogra co di labioschisi e dimostrato lintegrit del labbro superiore ( c , d , freccia bianca )  . 
between the 4th and the 10th week of gestation , ve main buds of tissue fuse together : a single median frontonasal process and two paired buds , the maxillary and the mandibular prominences . 
at around the 7th week , the central portion of the nose and the lateral nasal prominences develop into the nostrils , whereas at the 8th week , the structures responsible for the formation of the eyes have developed . 
it is the result of the failure of one or both of the medial nasal prominences to fuse with the maxillary prominences , generally between the 4th and 7th week discussione lo splancnocranio deriva quasi completamente dal mesenchima dei primi tre archi branchiali , costituiti da mesoderma ( blocchi di mesoderma accoppiati e verticali ) , che si sviluppano latero - ventralmente nella regione della testa e del collo , adiacenti allo stomodeo e allorofaringe primitivo . 
tra la 4a e la 10a settimana di gestazione si fondono 5 protuberanze di cui una impari , il processo fronto - nasale , e due pari , le protuberanze mascellari e mandibolari . 
alla 5a settimana si ultima la formazione del processo nasale mediano e laterale , intorno alla 7a settimana la parte centrale del naso e dai processi laterali si sviluppano le narici e all8a settimana si sviluppano le strutture deputate alla formazione degli occhi . 
la schisi di qualsiasi elemento del palato primario , con e senza interessamento del palato secondario , viene de nita come labioschisi o labiopalatoradiol med ( 2011 ) 116 : 11341148 1143 fig . 
cleft secondary palate ( cp ) is the result of a developmental abnormality or failure to fuse of the lateral palatine prominences between the 8th and 12th weeks of gestation [ 1 , 21 ]  . in contrast to cp , which often occurs in isolation , cl alone is a rare event . 
unlike clp , cp ( incidence of 1 / 2000 live births ) shows no remarkable variation among races , whereas the female - to - male ratio is 2 : 1 . 
it has also been noted that males tend to be more frequently affected by the more severe defects and complete forms and are more likely to have bilateral rather than unilateral forms . when analysing factors involved in the aetiology of clp , schisi ed avviene per mancata fusione di uno o pi processi nasali mediani con il processo mascellare generalmente tra la 4a e la 7a settimana di gestazione . 
le schisi del palato secondario avvengono invece per un alterato sviluppo o la mancata fusione dei processi palatini laterali tra l8a e la 12a settimana di gestazione [ 1 , 21 ]  . al contrario delle palatoschisi , che spesso si riscontrano in maniera isolata , le labioschisi isolate sono rare ; infatti circa il 70% di schisi labiali presenta anche schisi palatali . 
rispetto alle labiopalatoschisi , nelle palatoschisi ( incidenza di 1 / 2000 nati vivi ) non vi una contaminazione razziale ed i soggetti nati malformati sono pi femmine che maschi per un rapporto di 2 : 1 . 
per quanto riguarda le lps , quindi , vi una differenza di incidenza delle malformazioni a seconda delle razze ; in particolare lincidenza risulta pi alta nei bambini giapponesi ed ancora maggiore tra gli indigeni americani rispetto alla razza caucasica . 
stato notato anche che tra i maschi sono pi frequenti i difetti pi gravi e le forme complete e 1144 radiol med ( 2011 ) 116 : 11341148 the concept of aetiological heterogeneity is paramount , i.e. 
these factors include : multifactorial inheritance : this is the most important , most common but also the least known type of inheritance pattern underlying many disorders that have a genetic predisposition . inheritance factors : only appropriate genetic counselling is able to establish the in uence exerted by inheritance factors and their role in terms of the risk of recurrence . teratogenic factors : medicinal products and infections are the main factors responsible for congenital defects caused by the environment . 
 lastly , anticonvulsants and alcohol during pregnancy increase the risk of clp in the setting of syndromic conditions ; clefts can be associated with chromosomal defects or syndromes of unknown aetiology : chromosomal defects include down syndrome and trisomy 13 and 18 ; syndromes of unknown aetiology include the pierre robin sequence characterised by micrognathia , glossoptosis and soft - palate cleft . craniomaxillofacial abnormalities can have direct consequences on the survival of the newborn resulting from compromised swallowing and impaired respiratory function . 
at the same time , the fetal brain should be evaluated to identify the presence or otherwise of a syndromic condition . us is the rst - choice examination in the prenatal diagnosis of cl thanks to its low cost and ease of use . 
 additional 3d and 4d us reconstruction techniques , tra queste quelle bilaterali rispetto a quelle monolaterali . nellanalisi dei fattori implicati nelleziologia delle labiopalatoschisi pi che mai da tenere in considerazione il concetto delleterogenicit eziologica , ovvero dellesistenza di molteplici cause per un unico fenomeno . 
i fattori in causa possono essere : lereditariet multifattoriale , che rappresenta il pi importante , il pi comune , ma anche il meno conosciuto tipo di pattern ereditario alla base di molti disordini che riconoscono una predisposzione genetica ; i fattori ereditari : solo una consulenza genetica adeguata in grado di stabilire leffettiva entit dei fattori ereditari e quanto questi incidano in termini di rischio di ricorrenza ; fattori teratogeni : i farmaci e le infezioni sono i principali responsabili di difetti congeniti causati dallambiente . 
 secondo i dati della letteratura le benzodiazepine e gli steroidi possono determinare un modesto aumento del rischio di schisi labiopalatina senza altre anomalie associate ; il diabete materno e lassunzione di anfetamine aumentano il rischio in associazione ad altre anomalie ( ad esempio , cardiopatie congenite ) ; in ne gli antiepilettici e lalcool in gravidanza aumentano il rischio d labiopalatoschisi nellambito di altre sindromi ; in ne le schisi possono anche essere associate a difetti cromosomici , come la sindrome di down , la trisomia 13 e 18 , oppure a sindromi ad eziologia sconosciuta come la sequenza di pierre robin caratterizzata da micrognazia , glossoptosi e schisi del palato molle . 
ai ni della correzione chirurgica risulta necessario un corretto inquadramento della patologia : la monolateralit o la bilateralit , il grado di coinvolgimento del palato duro e le eventuali alterazioni biometriche del massiccio facciale , ottenute mediante la valutazione dei principali parametri . 
risulta inoltre necessaria la contemporanea valutazione dellencefalo per de nire la presenza o meno di una condizione sindromica . lecogra a rappresenta lindagine di prima scelta nella diagnosi prenatale delle labioschisi grazie ai suoi bassi costi e alla facilit di esecuzione . 
tuttavia la sua accuratezza pu essere limitata da condizioni patologiche fetali , quali anidramnios , oligoidramnios , sindromi malformative complesse e condizioni di pertinenza materna , come lobesit , oltre ad essere una metodica operatore - dipendente [ 22 , 23 ]  . 
lesame ecogra co , inoltre , non consente di de nire lesatto coinvolgimento del palato duro in relazione al radiol med ( 2011 ) 116 : 11341148 1145 such as surface rendering and transparency mode , provide improved visualisation of the fetal face and the presence of clefts , particularly in the presence of hard - palate involvement [ 9 ]  . 
 in t2 - weighted sequences , the signal intensity of the amniotic uid swallowed by the fetus provides excellent visualisation of the oropharynx , thus showing involvement of the secondary palate in cases where the volume of the oropharyngeal cavity is reduced by the encumbrance of the tongue . 
 moreover , mri is able to identify the direct communication between the buccal and the nasal cavities [ 21 ]  . in characterising cases of cl - clp , the diagnostic accuracy of mri proved to be higher in eight cases , particularly with regard to de ning the two essential parameters for surgical planning : the laterality and anteroposterior extent of the cleft , which determines the degree of palatal involvement . 
these data are directly correlated with the severity of complications and surgical dif culty in the intraoperative and postoperative period [ 24 ] we also obtained useful information regarding measurement of the fetal face in 6 / 24 fetuses . 
in the cases of associated micoragnathia , multiplanar mri with high anatomical detail played a key role in determining whether intervening immediately in the rst days of life or planning a series of interventions to be performed over time was more appropriate . 
measurements of the fetal face , therefore , may be considered a valid support in the diagnosis of conditions associated with cl - clp , and abnormal measurements should raise the suspicion of a syndromic fetus . results obtained from our population show a diagnostic accuracy of mri equal to 100% in the evaluation of both cl and clp . 
the technique proved able to correctly distinguish unilateral and midline from bilateral defects , as well as involvement of the anterior palate and alveolar processes from involvement of the secondary palate [ 2527 ]  . the main limitation to our study is the small size of the population . 
ulteriori tecniche di ricostruzione ecogra che 3d e 4d , quali il surface rendering ed il trasparency mode , permettono una migliore visualizzazione del viso fetale e di eventuali schisi , soprattutto in presenza di coinvolgimento del piano osseo [ 9 ]  . tuttavia , spesso si rende necessario il ricorso a metodiche di imaging di iii livello : la rm consente la visualizzazione diretta della schisi e la de nizione dellinteressamento del palato primitivo e / o secondario . 
liperintensit di segnale del liquido amniotico ingerito dal feto , nelle sequenze t2 pesate , permette unottima visualizzazione dellorofaringe , de nendo un interessamento del palato secondario nei casi in cui la cavit orofaringea presenta volume ridotto per ingombro della lingua ; inoltre , la rm permette lindividuazione della comunicazione diretta tra la cavit buccale e le cavit nasali [ 21 ]  . nella caratterizzazione dei casi di lbs - lps la rm ha dimostrato una maggiore accuratezza diagnostica in 8 casi , in particolare nella de nizione di due parametri essenziali nella piani cazione chirurgica : la lateralit ed il grado di estensione in senso antero - posteriore della schisi determinando in tal senso il grado di coinvolgimento palatale ; tali dati sono direttamente proporzionali al grado di complicanze e dif colt chirurgiche nellimmediato e nel postoperatorio [ 24 ]  . 
nei casi di associata micrognatia la rm , mediante immagini multiplanari ad alto dettaglio anatomico , permette agli operatori di decidere quando sia preferibile un trattamento immediato nei primi giorni di vita , o quando invece sia pi indicata la piani cazione di una serie di interventi da effettuare nel tempo . 
nei tre feti sindromici , invece , abbiamo riscontrato , unalterazione del dio e dellfma ; la diagnosi prenatale o autoptica hanno confermato la sindromicit di tali feti ; in particolare stato diagnosticato un feto affetto da trisomia 13 , deceduto alla nascita , uno affetto da trisomia 18 ed uno da trisomia 21 ( tabella 2 )  . 
la biometria del massiccio facciale , quindi , pu essere considerata un valido supporto nella diagnosi di patologie associate alla lbs - lps ed una sua alterazione deve porre il sospetto diagnostico di uneventuale condizione sindromica . dai risultati ottenuti dalla nostra casistica emerge come laccuratezza diagnostica dellesame rm risultata essere del 100% sia nella valutazione dei difetti labiali che nella de nizione dellinteressamento palatale , discriminando correttamente i difetti unilaterali e mediani da quelli bilaterali , cos come il coinvolgimento del palato anteriore e dei processi alveolari da quello del palato posteriore o secondario [ 2527 ]  . 
 il limite principale del nostro studio rappresentato dalla casistica ancora limitata ; per quanto concerne la metodica , i limiti sono legati alla dif colt di visualizzazione delle componenti scheletriche e al movimento fetale . 
per lo studio 1146 radiol med ( 2011 ) 116 : 11341148 table 2 magnetic resonance imaging ( mri ) and postnatal diagnosis in syndromic fetuses fetuses , n mri characteristics unilateral clp associated with an interventricular cardiac defect and borderline ventriculomegaly unilateral cl with involvement of the anterior palate associated with a lateral shift of the nasal septum and mild bilateral ventriculomegaly unilateral clp associated with alobar holoprosencephaly , cyclopia and arachnoid cyst of the posterior cranial fossa trisomy 13 ( postmortem diagnosis ) postnatal diagnosis trisomy 18 trisomy 21 cl , cleft lip ; clp , cleft lip and palate tabella 2 rm e diagnosi post - natale in feti sindromici feti , n caratteristiche rm diagnosi post - natale lps unilaterale associata a difetto interventricolare cardiaco e ventricolomegalia bordeline labioschisi unilaterale con coinvolgimento del palato anteriore associata a latero deviazione del setto nasale e ventricolomegalia bilaterale lieve lps unilaterale con oloprosencefalia alobare , ciclopia e cisti aracnoidea della fossa cranica posteriore trisomia 18 trisomia 21 trisomia 13 ( esame autoptico ) rm , risonanza magnetica ; lps , labio - palatoschisi tion . 
the sequences that proved to be diagnostic in terms of facial measurements and identi cation of the malformation were the t2 - weighted haste and the true - fisp sequences . 
both these sequences enabled us to reach the correct diagnosis , although the greater contrast resolution of the t2 - weighted haste sequences better visualised the defects of the palate and soft tissues . 
on the other hand , the true - fisp sequences with their intrinsic characteristics proved particularly useful in the study of particularly mobile fetuses . the images with the highest diagnostic quality , which therefore provided a better and simpler characterisation of the abnormalities found , were acquired on fetuses with advanced gestational age ( after the 27th week of gestation )  . 
 this is largely due to the greater anatomical detail obtained in larger structures and the reduced fetal motion . in conclusion , thanks to an excellent depiction of fetal face anatomy , high - contrast resolution , multiplanar capabilities and large eld of view , mri offers a complete evaluation of abnormalities of the fetal face and bra these advantages therefore enable better treatment planning in the setting of multidisciplinary patient management [ 2830 ]  . del distretto scheletrico , ultimamente , sono state proposte le sequenze epi , le quali per nel nostro lavoro non hanno aggiunto ulteriori informazioni . 
entrambe le sequenze ci hanno permesso di porre diagnosi anche se la maggiore risoluzione di contrasto insita nelle sequenze haste t2 pesate meglio documenta la risoluzione di continuit del palato e delle parti molli . 
daltro canto le sequenze true - fisp sono state particolarmente utili , per le loro caratteristiche intrinseche , nei feti con spiccata motilit . le immagini di maggiore qualit diagnostica , che hanno pertanto permesso una migliore e pi facile caratterizzazione delle alterazioni riscontrate , sono state acquisite su feti con et gestazionale avanzata ( dopo le 27 settimane di gestazione ) ; tale dato da mettere in relazione al miglior dettaglio anatomico derivante da strutture di maggiori dimensioni e alla ridotta mobilit del feto . 
 in conclusione , grazie allottima visualizzazione dellanatomia del massiccio facciale fetale , allelevata risoluzione di contrasto , alla multiplanariet della metodica e allampio campo di vista , la rm consente un completo inquadramento della patologia del massiccio facciale e del distretto encefalico , consentendo una piani cazione del management terapeutico nellottica di una gestione multidisciplinare del paziente [ 2830 ]  . conclusions the mr study of the fetal face is indicated as a level - three study to be performed after level - two us has identi ed an lo studio rm fetale del massiccio facciale trova un ruolo conclusioni radiol med ( 2011 ) 116 : 11341148 1147 abnormality of the fetal lip or palate . 
the aim of this study was to better de ne the laterality and anteroposterior extent of the cleft and thus provide an accurate diagnosis at an early gestational age [ 10 ]  . in addition , mri is able to analyse the entire fetal head , measure the biometric development of the fetal face and identify dif cult - to - characterise associated pathological conditions ( especially involving the cns ) at an early stage , thus prompting suspicion of syndromic conditions . come esame di iii livello dopo un esame ecogra co di ii livello che abbia identi cato il difetto labiale e / o palatale , al ne di meglio de nire il grado di coinvolgimento del palato posteriore ed il grado di lateralit , consentendo una diagnosi accurata gi in et gestazionale precoce [ 10 ]  . inoltre , la rm consente di analizzare in toto il distretto cranio - encefalico , di effettuare una valutazione dello sviluppo biometrico del massiccio facciale e di identi care precocemente eventuali patologie associate di dif cile caratterizzazione ( soprattutto a carico del snc ) , permettendo di sospettare condizioni sindromiche . 
in 19 patients ( 2.6 % ) ultrasound ( us ) showed enlarged lymph nodes in the upper abdomen , and abdominal computed tomography ( ct ) was performed results . 
detecting enlarged lymph nodes in the upper abdomen after liver transplantation is and infrequent occurrence ; however , thorough imaging is required to detect and characterise a wide variety of disorders . 
gli esami istologici hanno rivelato un disturbo linfoproliferativo post - trapianto ( ptld ) in 6 pazienti ( 31 , 5% ) , una neoplasia epatica in 6 pazienti ( 31 , 5% ) , una tubercolosi sistemica disseminata in un caso ( 5 , 2% ) ed una sarcoidosi in un altro caso ( 5 , 2% )  . 
nella maggior parte dei casi le linfoadenomegalie si riveleranno correlate ad un disordine linfoproliferativo post - trapianto o ad una recidiva di malattia . keywords liver hepatic transplantation ct lymph nodes parole chiave fegato trapianto di fegato tc linfonodi 1068 introduction orthotopic liver transplantation ( olt ) is a well - established treatment for a variety of irreversible acute and chronic endstage liver diseases , for which no other satisfactory therapy is available . 
 in cases of inconclusive results , con rmation of anomalies depicted at us or clinical suspicion of a complication despite normal us , helical computed tomography ( ct ) should be performed . 
we review our experience in a single centre on pathologic conditions associated with enlarged lymph nodes after liver transplantation and imaging features that may allow narrowing the differential diagnosis . materials and methods patients between january 1997 and september 2008 , 715 olts were performed at our institution in 585 patients , 488 men and 227 women , between 15 and 73 ( mean 54 ) years of age . 
the main causes for liver transplantation were alcoholic cirrhosis ( n = 149 ) , posthepatitis c cirrhosis ( n = 130 ) , hepatocellular carcinoma ( n = 219 ) , retransplantation ( n = 77 ) , familial amyloidal polyneuropathy ( n = 26 ) , posthepatitis b cirrhosis ( n = 23 ) , primary biliary cirrhosis ( n = 17 ) and others . follow - up after liver transplantation at our institution is basically done with us on the rst and seventh days after the procedure , 1 month after liver transplantation and then every 6 months , and also in the event of clinical symptoms or impaired hepatic biology . 
additionally , an abdominal ct is performed when suspicious ndings are found on us examination . inclusion criterion was the detection of an abnormality on us suggesting lymphadenopathy and re ected in the us report of the hepatic transplantation database . 
in 19 patients ( 2.6% ) , us showed enlarged lymph nodes in the hepatic hilum , celiac region or lesser omentum , in which cases abdominal ct was performed . 
there were 15 men and four women , with ages ranging from 42 to 66 ( mean 55 ) years . patients with a nal diagnosis of posttransplantation lymphoproliferative disorder ( ptld ) , tumoral disease , tuberculosis or sarcoidosis had clinical and / or biological abnormalities ( 76% )  . 
indications for liver transplantation in this group included hepatic cirrhosis of different origin in eight patients ( origin was related to hepatitis c virus in ve patients and to alcohol in three ) , hepatic cirrhosis and hepatocellular carcinoma ( hcc ) in seven patients , cholangiocarcinoma in two patients , liver metastasis of a gastric carcinoid tumour in one patient and familial amyloidal polyneuropathy ( fap ) in one patient . 
in patients in whom hcc was the indication for liver transplantation , the origin of hepatic cirrhosis was related to hepatitis c virus in three , alcohol in three and hepatitis b virus in one . ct technique abdominal ct examinations were performed with two different helical ct units ( nxi , yocogawa , japan , and ct brightspeed , ge healthcare milwaukee , wi , usa ) with 250400 mas and 120 kvp . 
 the incidence of ptld in our series was 0.83% ( 6 / 715 ) , radiol med ( 2011 ) 116 : 10671075 1069 accounting for 31.5% ( 6 / 19 ) of patients with olt and enlarged lymph nodes . 
epstein - barr virus ( ebv ) was positive in three histological specimens ( in two patients with b cell lymphoma and in the patient with plasmacytic hyperplasia )  . 
 axial computed tomography images in arterial ( a ) , portal ( b ) and equilibrium ( c ) phases show a hypovascular , ill - de ned mass encasing hilum structures ( note intrahepatic bile duct dilatation )  . 
le immagini tc assiali in fase arteriosa ( a ) , portale ( b ) e di equilibrio ( c ) mostrano una massa ipovascolarizzata , mal de nita ed in ltrante le strutture ilari ( da notare la dilatazione delle vie biliari intra - epatiche )  . 
il campione istologico risultato positivo per ebv . tumoral disease sarcoidosis four patients with tumoral hepatic disease ( 31.5% ) developed recurrence , which was the indication for liver transplantation ( two hcc , one cholangiocarcinoma and one hepatic metastases of a gastric neuroendocrine tumour )  . 
two patients developed de novo malignancies corresponding to a disseminated squamous - cell carcinoma of the oesophagus and a disseminated mucinous adenocarcinoma of the rectutime from liver transplantation to diagnoses ranged from 3 to 41 months . 
in this group , pathologic lymph nodes were located in more than one region , basically gastrohepatic ligament , celiac region and hepatic hila , but also in the retroperitoneuin all cases except recurrent cholangiocarcinoma , associated hepatic lesions were detected . 
axial computed tomography images in arterial ( a ) and portal ( b ) phases show hypervascular hepatic lesions and hypervascular enlarged lymph nodes located at the porta hepatis and celiac trunk due to massive recurrence of hepatocellular carcinoma . 
le immagini tc assiali in fase arteriosa ( a ) e portale ( b ) mostrano lesioni epatiche ipervascolarizzate associate a linfoadenomegalie ipervascolarizzate localizzate nella porta hepatis e lungo il tronco celiaco dovute ad una massiva recidiva di hcc . 
nine months after the procedure and during re - evaluation for new liver transplantation due to ischaemic cholangitis , a markedly hypodense retroperitoneal enlarged lymph node of 2.5 cm with thin peripheral enhancement and associated bilateral pulmonary pseudonodular lesions were discovered . 
rapid evolution to sepsis caused death 11 months after liver transplantation , and cultures of different specimens at necropsy ( lungs , retroperitoneal lymphadenopathy and spleen ) demonstrated caseating granulomas due to disseminated systemic tuberculosis . 
no signs of hcc progression were demonstrated at necropsy . hyperplasic lymph nodes in a group of ve patients ( 26% ) , cytological study of enlarged lymph nodes located at porta hepatis revealed changes of nonspeci c reactive lymphadenitis without malignant cells . 
mean time of diagnosis ranged from 8 to 12 months in patients with previous medical history of hepatitis c cirrhosis and 36 months in patient undergoing liver transplantation due to familial amyloidal polyneuropathy . 
 in this group , ct images showed isolated , well - de ned , enlarged lymph nodes in porta hepatis ranging from 2 to 3.3 cthey were all homogeneous , but in two cases , they were isodense to the hepatic parenchyma during the portal phase ; in two cases , they were slightly hypodense during the portal phase ; and in one case , the lymph node was hypervascular during the arterial phase . 
3a , b follow - up ultrasound in an asymptomatic 54 year - old woman 2 years after liver transplantation due to hepatitis - c - induced cirrhosis showed enlarged lymph nodes . 
axial ct image in portal phase ( a ) show an ill - de ned hypovascular mass in porta hepatis and celiac trunk without encasement of vascular or biliary structures . 
3a , b follow - up con us di una donna di 54 anni , asintomatica , 2 anni dopo trapianto di fegato per cirrosi epatica c - correlata con comparsa di linfoadenomegalie . 
limmagine tc assiale in fase portale ( a ) mostra una massa ipovascolarizzata , mal de nita , nella porta hepatis ed in adiacenza del tronco celiaco , senza in ltrazione delle strutture vascolari o biliari . 
lo studio del materiale ottenuto con biopsia chirurgica ha evidenziato la presenza di granulomi non - caseosi . lesions were detected , and only in one case were coexisting signs of chronic liver disease detected . 
 ptld is a well - known complication after solid - organ transplantation , with a reported incidence of 210% [ 2 ] , ranging from 23% in adults and > 10% in the paediatric population . 
ebv and immunosuppressive therapy are considered the two major risks factors due to the capability of the virus to stimulate b lymphocyte proliferation without the inhibitory effect of t lymphocytes , which are pharmacologically suppressed [ 3 ]  . 
 these entities are divided into four main histological types according to the latest world health organisation ( who ) reactive plasmacytic hyperplasia classi cation : early and infectious - mononucleosis - like disease , polymorphic ptld , monomorphic ptld and hodgkins and hodgkinlike lymphomas . 
radiologically , ptld can virtually affect any organ , leading to a wide spectrum of ndings , with lymph nodes , liver and gastrointestinal tract being the most frequent sites when considering abdominal disease . 
 [ 6 ] , different patterns of involvement are considered : an in ltrative pattern with heterogeneous ill - de ned low attenuation regions with or without associated hepatomegaly , a tumoral pattern with diffuse hypodense nodular lesions and a porta hepatis mass with frequent encasement of vascular and biliary structures . radiol med ( 2011 ) 116 : 10671075 1073 fig . 
4a ultrasound ( us ) at the level of the porta hepatis in a 39 - year - old patient in whom liver transplantation was performed due to a familial amyloidal polyneuropathy shows isoechogenic lymph node . 
axial ct scan ( b ) at the same level shows well - de ned , hypodense , enlarged lymph nodes close to the main portal veus - guided ne - needle aspiration biopsy showed nonspeci c reactive lymphadenopathy . 
c il follow - up tc 2 anni pi tardi dimostra una stabilit di malattia . in our study , we found no allograft disease , as frequently as reported by pickhardt et al . 
 [ 6 ] the discrepancy may be due to the patterns of allograft disease considered by different authors ; whereas hilar mass is considered as a form of presentation of graft disease by pickhardt et al . 
this histological result probably represents a very initial stage of the disease , considered a nonneoplastic reactive response to ebv infection , which may often disappear spontaneously or with reduced immunosuppression . 
 hepatic tumoral involvement after liver transplantation can be secondary to recurrence of the tumour considered for the indication to the procedure , or less frequently to development of de novo neoplasia ( metastasis of a previously unknown primary tumour )  . 
due to high rates of recurrence , cholangiocarcinoma is no longer considered an indication for liver transplantation by most groups , although some selected cases have been transplanted in our institution . 
 tumoral recurrence of hcc may affect any organ , but most common sites of recurrence in order of frequency are lungs , liver graft and regional lymph nodes , followed by adrenal glands and bone . 
in our series , tumoral recur1074 radiol med ( 2011 ) 116 : 10671075 rence of hcc presented as lung metastasis with multifocal liver involvement and enlarged locoregional lymph nodes . 
 in one patient who was diagnosed 13 months after the procedure , hepatic lesions and lymphadenopathy showed a hyperenhancing pattern , whereas the patient detected 3 months after the procedure presented with hypovascular lesions related to a recurrent poorly differentiated hcc . 
 despite advances in surgical techniques and immunosuppressive treatments leading to a survival increase , patients undergoing organ transplantation are at risk of developing a wide variety of infections , including tuberculosis . 
on the other hand , although mechanisms of transmission may vary among patients , reactivation of a pre - existing latent infection seems to be more frequent than primo - infection or liver - graft transmission radiologically , pulmonary disease is the most frequent pattern seen in transplant recipients , followed by disseminated forms and extrapulmonary disease . 
whereas affected lymph nodes in tuberculosis tend to show a hypodense centre due to necrosis , with peripheral enhancement , pathological lymph nodes in nontreated lymphoma most commonly show homogeneous enhancement after contrast administration [ 12 ]  . 
 some of the proposed causes include in ammatory mediators , in particular , inf [ 12 , 13 ] , a drug widely used as treatment for some neoplasm and for viral infections , especially hepatitis c . 
unfortunately , the patient died approximately 1 year late due to complications of acute hepatitis c recurrence . it is not infrequent to identify enlarged lymph nodes at the hepatic hilum in patients with hepatitis - c - induced cirrhosis , which is the most frequent indication for liver transplantation in europe and the usa . 
these changes are similar to those seen previous to liver transplantation , such as nodularity of liver surface due to regenerating nodules , brous scarring with nonuniform segmental atrophy or hypertrophy of the liver , extrahepatic changes due to portal hypertension and unspeci c lymph nodes at the porta hepatis , more frequently seen in cases of hepatitis c viral infection . 
follow - up usually shows stability or even regression of these nonspeci cally enlarged lymph nodes . in conclusion , detecting enlarged lymph nodes in the upper abdomen after liver transplantation is infrequent , and thorough imaging is required to detect and characterise a wide variety of disorders . 
if liver transplantation is performed due to malignant disease , such as hcc or metastases of neuroendocrine tumours , detection of enlarged lymph nodes associated with liver lesions suggests tumoral recurrence . 
midiri dipartimento di biotecnologie mediche e medicina legale , sezione di diagnostica per immagini , policlinico universitario , via del vespro 127 , 90127 palermo , italy correspondence to : t . 
eighty - four focal breast lesions , 64 benign and 20 malignant ( mean diameter , 15.1 mm ) , detected but not characterised on b - mode us in 72 women , breast imaging reporting and data system ( bi - rads ) us category 3 ( n = 56 ) or category 4 ( n = 28 ) , were studied with us elastography and classi ed in consensus by two radiologists according to a ve - point colour scale . 
a total of 65 / 84 ( 77.4% ) lesions were correctly classi ed as benign or malignant using us elastography , whereas the remaining 19 / 84 ( 22.6% ) were incorrectly assessed . 
the high npv of us elastography may help reduce the use of biopsy in bi - rads 3 lesions , but its low ppv in bi - rads 4 lesions does not allow avoidance of riassunto obiettivo . 
ottantaquattro lesioni focali mammarie , 64 benigne e 20 maligne ( diametro medio : 15 , 1 mm ) , rilevate ma non caratterizzate allecogra a di base in 72 donne punteggio ecogra co breast imaging reporting and data system ( bi - rads ) 3 ( n = 56 ) o bi - rads 4 ( n = 28 ) , sono state sottoposte ad elastosonogra a e classi cate in consenso da due radiologi secondo una scala colorimetrica in cinque punti . 
sessantacinque / 84 ( 77 , 4% ) lesioni sono state correttamente classi cate come benigne o maligne allelastosonogra a , mentre le rimanenti 19 / 84 ( 22 , 6% ) sono state erroneamente valutate . 
lelevato vpn dellelastosonogra a pu essere utile per evitare lestensivo ricorso alla biopsia nelle lesioni mammarie in classe bi - rads 3 , ma il basso 1028 radiol med ( 2011 ) 116 : 10271038 biopsy on the basis of the us elastographic score alone in this group of lesions . vpp in quelle bi - rads 4 non consente di escludere il ricorso alla biopsia sulla scorta del solo punteggio elastosonogra co . keywords breast ultrasound elastography breast neoplasms parole chiave mammella elastosonogra a neoplasie mammarie introduction introduzione the role of grey - scale ultrasound ( us ) has considerably expanded in characterising focal breast lesions . 
 in particular , the development of a categorisation system based on sonographic semiological criteria , such as the breast imaging reporting and data system ( bi - rads ) , has proved useful for describing and classifying both benign and malignant breast lesions [ 2 ]  . 
however , the limited reproducibility of the system in determining the exact likelihood of malignancy of suspicious breast lesions ( category 4 ) , with variability ranging from 3% to 94% , leaves the problem of recourse to more invasive and costly diagnostic procedures , such as biopsy , essentially unchanged [ 3 ]  . 
 furthermore , even though the risk of malignancy in lesions classi ed as bi - rads category 3 should be < 2% , the large number of biopsies performed on benign lesions continues to represent a real problem , especially in the light of the cost - effectiveness of screening programmes [ 2 ]  . the introduction of us elastography into clinical breast imaging in 1997 made it possible to evaluate a mechanical property completely different from echogenicity : that is , tissue elasticity [ 4 ]  . 
tissue elasticity , de ned mathematically by the elastic or young modulus , can be obtained from the pressure required to deform a given tissue or structure [ 5 ]  . 
the recent availability of us units equipped with an elastography module enabling real - time , free - hand imaging has prompted several authors to assess the contribution of us elastography to the characterisation of breast lesions , with encouraging results [ 610 ]  . 
the purpose of this study was to evaluate the usefulness of us elastography in characterising breast lesions classi ed as indeterminate at b - mode materials and methods patients lecogra a in scala di grigi , grazie ai continui progressi tecnologici , che ne hanno notevolmente migliorato sia la risoluzione spaziale sia quella di contrasto , ha notevolmente ampliato il suo ruolo nella caratterizzazione delle lesioni focali mammarie [ 1 ]  . 
in particolare , lelaborazione di un sistema di categorizzazione basato su criteri semeiologici ecogra ci , quale il breast imaging reporting and data system ( bi - rads ) , si dimostrato uno strumento utile ai ni di descrivere e sistematizzare le lesioni mammarie sia benigne che maligne [ 2 ]  . 
tuttavia , la limitata riproducibilit di tale sistema nel de nire lesatta probabilit di malignit di una lesione mammaria sospetta ( categoria 4 ) , con una variabilit che va dal 3% al 94% , lascia sostanzialmente inalterata la problematica relativa al ricorso , in tale ambito , a procedure diagnostiche pi invasive e costose , quali la biopsia [ 3 ]  . 
inoltre , sebbene il rischio di malignit delle lesioni classi cate in categoria bi - rads 3 dovrebbe essere inferiore al 2% , il gran numero di biopsie tuttoggi effettuate su lesioni benigne continua a costituire un reale problema , soprattutto nellottica costo / bene cio dei programmi di screening [ 2 ]  . lintroduzione in ambito clinico - senologico dellelastosonogra a , avvenuta nel 1997 , ha reso possibile valutare una propriet meccanica completamente differente dallecogenicit : lelasticit tissutale [ 4 ]  . 
del tutto recentemente , la disponibilit commerciale di unit ecogra che dotate di modulo elastosonogra co capace di consentire un esame in tempo reale ed a mano libera , ha consentito a diversi autori di cominciare a valutare lapporto dellelastosonogra a nella caratterizzazione delle lesioni mammarie con incoraggianti risultati [ 610 ]  . 
scopo del presente lavoro stato quello di valutare lutilit dellimpiego dellelastosonogra a nella caratterizzazione delle lesioni mammarie indeterminate allecogra a di base . between june 2008 and june 2009 , 72 women ( age range 2284 years ; mean age , 47.512.33 years ) with 84 focal breast lesions ( diameter , 444 mm ; mean , 15.1 mm ) were prospectively evaluated following approval by the ethics ottenuta lapprovazione da parte del comitato etico istituzionale , sono state prospetticamente valutate , nel periodo materiali e metodi pazienti radiol med ( 2011 ) 116 : 10271038 1029 committee . 
thirty - seven were also clinically palpable ( diameter , 844 mm ; mean , 20.9 mm ) , whereas 47 lesions ( diameter 415 mm ; mean , 8 mm ) were nonpalpable and were detected during routine examinations . 
in order to assess the impact of elastography on the diagnostic workup , all lesions with a clear cystic appearance and / or classi ed as bi - rads 2 ( and therefore not requiring biopsy ) were excluded from the analysis . 
the lesions classi ed as bi - rads 5 were also excluded , as they were almost certainly malignant and requiring appropriate treatment . examination technique all investigations were performed using logos hi vision gold us equipment ( esaote / hitachi medical corporation , tokyo , japan ) equipped with a multifrequency linear - array transducer ( 13 - 5 mhz ) and a dedicated us elastography module . 
before the us elastography examination itself , the breast parenchyma was always imaged with grey - scale and colour power doppler us to locate the lesion and select the most appropriate scan plane . 
in particular , the us elastography investigation was conducted in real time using a split - screen display with simultaneous viewing of the b - mode image on the right and the us elastogram superimposed on the same b - mode image on the le the equipment uses a special autocorrelation system ( the extended combined autocorrelation method ) that can be applied in real time to take into account not only changes along the axis of propagation of the us beam but also movements along the lateral axis , thereby reducing artefacts due to lateral displacement of the tissues [ 8 ]  . the signal from the structures being examined and relative to a speci c sampling box placed on the region of interest and extending also to healthy breast tissue is processed in real time and the resulting elastogram is immediately superimposed over the b - mode image and displayed on a colour scale from red ( soft or highly elastic tissue ) to blue ( hard or inelastic tissue )  . 
at the same time , a special indicator light provides real - time feedback on the quality of the examination by scoring it from 1 to 6 and displaying the score alongside the us elastogra scores of 3 or higher indicate a suf cient or good reliability of the elastogra compreso tra giugno 2008 e giugno 2009 , 72 donne di et compresa tra 22 e 84 anni ( et media : 47 , 512 , 33 anni ) con 84 lesioni mammarie focali ( diametro : 444 mm ; media : 15 , 1 mm ) , tutte ecogra camente rilevabili . 
trentasette lesioni erano anche clinicamente palpabili ( diametro : 844 mm ; media : 20 , 9 mm ) , mentre 47 lesioni ( diametro 415 mm ; media : 8 mm ) non erano palpabili e sono state individuate durante controlli di routine . 
tutte le pazienti , quindi , sono state sottoposte a indagine ecogra ca , condotta da due radiologi esperti in ecogra a senologica ( almeno dieci anni ) , i quali hanno classi cato ciascuna lesione , sulla base dei reperti b - mode , in accordo con lo schema bi - rads ecogra co [ 11 ]  . 
al ne di valutare limpatto dellelastosonogra a nel modi care liter diagnostico , sono state escluse dalla presente valutazione tutte le lesioni classi cate con aspetto chiaramente cistico e / o classi cate come bi - rads 2 e , pertanto , non necessitanti di campionamento bioptico . 
anche le lesioni classi cate come bi - rads 5 allindagine ecogra ca di base sono state escluse dal presente studio , in quanto quasi certamente maligne e gi di per s necessitanti di adeguato trattamento . tecnica desame tutte le indagini ecogra che sono state effettuate con apparecchiatura logos hivision gold ( esaote / hitachi medical corporation , tokio , giappone ) dotata di trasduttore lineare multifrequenza ( 135 mhz ) nonch di modulo elastosonogra co dedicato . 
prima dellesame elastosonogra co vero e proprio , stato sempre effettuato uno studio ecogra co del parenchima mammario , sia in scala di grigi che con modulo color e power doppler , al ne di individuare la lesione stessa e selezionare un adeguato piano di scansione . 
in particolare , lindagine elastosonogra ca stata condotta in tempo reale , mediante suddivisione dello schermo ecogra co in due parti e visualizzando contemporaneamente nella parte destra dello schermo la consueta immagine b - mode e , nella parte sinistra , lelastogramma superimposto alla stessa immagine b - mode . 
lapparecchiatura impiegata implementa un particolare sistema di autocorrelazione ( metodo di autocorrelazione estesa combinata ) che pu essere applicato in tempo reale permettendo di tenere conto non solo delle alterazioni lungo lasse di propagazione del fascio ultrasonoro , ma anche dei movimenti lungo lasse laterale , riducendo gli artefatti dovuti , appunto , alla dislocazione laterale dei tessuti [ 8 ]  . 
 1030 radiol med ( 2011 ) 116 : 10271038 in our study , us elastograms were considered acceptable only if they were found to be adequately and continuously superimposed over the b - mode image , with light indicator scores between 4 and 6 . 
two radiologists with at least 10 years experience in breast us and who were not involved in performing the examinations and were unaware of patients clinical history and nal diagnosis , consensually evaluated the images of ine . 
to avoid any recall bias , four image evaluation sessions were scheduled , each 1 week apart . the us elastograms were classi ed using a score ranging from 1 to 5 , according to the scheme proposed by the italian study group ( elasticity score ) based on the classi cation previously proposed by itoh et al . 
 [ 7 ] : score 1 , presence of a three - layered colour pattern of blue , green and red ; score 2 , diffuse green , possibly with a few small inconsistent blue spots ; score 3 , diffuse green with some blue spots ; score 4 , almost completely blue with maybe a few small green spots , especially peripherally ; score 5 , completely blue and with a blue rim surrounding the lesion . 
a score of 1 is considered predominant in liquid lesions ; scores 2 and 3 correspond to lesions that are predominantly elastic and therefore more frequently benign , whereas scores 4 and 5 indicate lesions that are predominantly hard and more frequently malignant [ 7 , 12 ]  . standards of reference the nal diagnosis was obtained through a microhistological biopsy in 67 cases and cytological examination in the remaining 17 . 
all samples were collected under us guidance using 21to 23 - gauge needles for cytological sampling and 14to 18 - gauge needles for microhistological sampling . statistical analysis in order to evaluate the usefulness of us elastography in characterising suspicious breast lesions and therefore to verify its sensitivity , speci city and positive and negative predictive values ( ppv and npv ) , we calculated the true positive ( tp ) , true negative ( tn ) , false positive ( fp ) and false negative ( fn ) results . 
in agreement with the literature , lesions were considered positive ( p ) for malignancy if they had us elastography scores of 4 or 5 and negative ( n ) if they had scores of 1 , 2 or 3 . il segnale proveniente dalle strutture esaminate e relativo ad un apposito box di campionamento posto dalloperatore sulla regione di interesse comprendente anche il tessuto mammario sano viene elaborato in tempo reale e , immediatamente , lelastogramma ottenuto viene sovrapposto allimmagine in b - mode e visualizzato secondo una scala cromatica che va dal rosso ( sof ce ) al blu ( anelastico )  . 
al contempo , un apposito indicatore luminoso indica , in tempo reale , la corretta conduzione dellesame attraverso una scala di valori da 1 a 6 , che viene visualizzata lateralmente allimmagine elastosonogra ca . 
questultima , nel nostro studio , stata considerata accettabile solo nel caso in cui fosse risultata sovrapposta in maniera congrua e continua allimmagine b - mode , con valori assegnato dallapposito indicatore luminoso compresi tra 4 e 6 ; sono state considerate , invece , inesatte le informazioni provenienti da elastogrammi con una sovraimposizione fugace e con valori di scala inferiori a 4 . 
la durata di ogni singola valutazione elastosonogra ca stata , in media , pari a circa 3 minuti ( intervallo : 25 minuti )  . analisi delle immagini tutti gli esami sono stati archiviati come dati grezzi in forma digitale . 
due radiologi esperti in ecogra a senologica ( almeno dieci anni ) , non coinvolti nellesecuzione degli esami e non a conoscenza della storia clinica dei pazienti n della diagnosi nale , hanno valutato in consenso off - line le immagini ottenute . 
per evitare il recall bias sono state previste quattro sessioni di valutazione distanziate da una settimana . le immagini elastogra che sono state classi cate con un punteggio variabile da 1 a 5 , secondo lo schema proposto dal gruppo di studio italiano ( elasticity score ) sulla base della classi cazione precedentemente proposta da itoh et al . 
 [ 7 ] : ( 1 ) presenza di tri - strati cazione cromatica : blu / verde / rossa ; ( 2 ) prevalenza di verde , con eventualmente qualche incostante punto blu ; ( 3 ) prevalenza di verde , con qualche punto blu ; ( 4 ) quasi completamente blu , con eventualmente qualche punto verde , soprattutto perifericamente ; ( 5 ) completamente blu , anche con alone blu perilesionale . 
il punteggio 1 considerato predominante nelle lesioni liquide , i punteggi 2 e 3 corrispondono a lesioni in prevalenza elastiche e , dunque , pi frequentemente benigne , mentre i punteggi 4 e 5 corrispondono a lesioni prevalentemente rigide e pi frequentemente maligne [ 7 , 12 ]  . 
tutti i prelievi sono stati eseguiti sotto guida ecogra a radiol med ( 2011 ) 116 : 10271038 results mediante aghi da 2123 g per lesame citologico e con aghi da 1418 g per lesame microistologico . 1031 the cytohistological examinations of the 84 lesions studied provided a diagnosis of benignity in 64 cases ( 76.2% ) and malignancy in the remaining 20 cases ( 23.8% ) ( table 1 )  . 
 analisi statistica table 1 final diagnosis and ultrasound ( us ) elastography score of the 84 breast lesions examined us elastography score 5 total benign lesions fibroadenoma corpuscular cyst angioma cicatricial brosis adenosis granuloma fat necrosis pseudoangiomatous hyperplasia cold abscess malignant lesions invasive ductal carcinoma ductal carcinoma in situ abscessed ductal carcinoma tubular carcinoma lobular carcinoma mucinous carcinoma sarcoma total 21 2 37 8 tabella 1 diagnosi nale e punteggio elastosonogra co delle 84 lesioni mammarie prese in esame punteggio elastosonogra co 5 totale lesioni benigne fibroadenoma cisti corpuscolata angioma fibrosi cicatriziale adenosi granuloma steatonecrosi iperplasia pseudoangiomatosa ascesso freddo lesioni maligne carcinoma duttale in ltrante carcinoma duttale in situ carcinoma duttale ascessualizzato carcinoma tubulare carcinoma lobulare carcinoma mucinoso sarcoma totale 21 2 37 8 allo scopo di valutare lutilit dellimpiego dellelastosonogra a nella caratterizzazione delle lesioni mammarie sospette e quindi di veri carne la sensibilit , la speci cit ed il valore predittivo positivo ( vpp ) e negativo ( vpn ) abbiamo calcolato : i veri positivi ( vp ) , i veri negativi ( vn ) , i falsi positivi ( fp ) ed i falsi negativi ( fn )  . 
abbiamo considerato , in accordo con i dati della letteratura , positive ( p ) per malignit le lesioni con punteggio elastosonogra co pari a 4 o 5 ; e negative ( n ) le lesioni con un punteggio elastosonogra co pari a 1 , 2 o 3 . risultati lesame cito - istologico delle 84 lesioni oggetto di studio del nostro lavoro ha fornito una diagnosi di benignit in 64 casi ( 76 , 2% ) e di malignit nei rimanenti 20 casi ( 23 , 8% ) ( tabella 1 )  . 
allindagine ecogra ca di base , 56 / 84 lesioni ( 66 , 7% ) sono state classi cate come appartenenti alla classe bi - rads 3 e le rimanenti 28 ( 33 , 3% ) a quella bi - rads 4 . 
complessivamente , 65 / 84 ( 77 , 4% ) lesioni sono state correttamente classi cate come benigne o maligne allelastosonogra a , mentre le rimanenti 19 / 84 ( 22 , 6% ) sono state erroneamente valutate . 
nella serie presa in esame ne derivano , per quanto attiene lelastosonogra a , tassi di sensibilit , speci cit , vpp e vpn pari rispettivamente a 70% , 79 , 6% , 51 , 8% e 89% ( tabella 4 )  . 
parallelamente , considerando come benigne le lesioni in classe ecogra ca bi - rads 3 e maligne quelle in classe bi - rads 4 , la valutazione della sola ecogra a convenzionale ha portato al riscontro di 14 falsi positivi e 6 falsi negativi , con valori di sensibilit , speci cit , vpp e vpn pari rispettivamente a 68 , 4% , 78 , 5% , 48 , 1% e 89 , 5% . 1032 radiol med ( 2011 ) 116 : 10271038 table 2 ultrasound ( us ) elastography scores for the 56 breast imaging reporting and data system 3 lesions us elastography score total cold abscess ( 1 ) corpuscular cysts ( 6 ) granuloma ( 1 ) mucinous carcinoma ( 1 ) fibroadenoma ( 2 ) fibroadenoma ( 19 ) fat necrosis ( 1 ) angioma ( 8 ) fibrosis ( 1 ) corpuscular cysts ( 2 ) fibroadenoma ( 2 ) tubular carcinoma ( 1 ) ductal carcinoma ( 1 ) idc ( 3 ) fat necrosis ( 2 ) fibroadenoma ( 4 ) corpuscular cyst ( 1 ) the number of lesions is shown in brackets idc , invasive ductal carcinoma punteggio elastosonogra co tabella 2 punteggio elastosonogra co delle 56 lesioni mammarie in classe birads 3 totale ascesso freddo ( 1 ) cisti corpuscolata ( 6 ) granuloma ( 1 ) carcinoma mucinoso ( 1 ) fibroadenoma ( 2 ) fibroadenoma ( 19 ) liponecrosi ( 1 ) angioma ( 8 ) fibrosi ( 1 ) cisti corpuscolata ( 2 ) fibroadenoma ( 2 ) carcinoma tubulare ( 1 ) carcinoma duttale ( 1 ) cdi ( 3 ) liponecrosi ( 2 ) fibroadenoma ( 4 ) cisti corpuscolata ( 1 ) tra parentesi indicato il numero di lesioni cdi , carcinoma duttale in ltrante on b - mode us , 56 / 84 lesions ( 66.7% ) were classi ed as bi - rads 3 and the remaining 28 ( 33.3% ) as bi - rads 4 . 
overall , 65 / 84 ( 77.4% ) lesions were correctly classi ed as benign or malignant at us elastography , whereas the remaining 19 / 84 ( 22.6% ) were incorrectly assessed . 
in particolare , sette lesioni benigne ( 2 granulomi su cicatrice , 2 broadenomi , 1 adenosi , 1 iperplasia pseudoangiomatosa , 1 cisti corpuscolata ) classi cate in classe bi - rads 4 sono state correttamente valutate come benigne alla valutazione elastosonogra ca , mentre 3 lesioni maligne ( tutti carcinomi duttali in ltranti ) , classi cate in classe bi - rads 3 , sono state correttamente valutate come maligne allindagine elastosonogra ca . 
di contro , sei lesioni correttamente valutate in classe bi - rads 3 ( 4 broadenomi e 2 aree di steatonecrosi ) sono state erroneamente valutate come maligne alla valutazione elastosonogra ca . 
in ne , tre lesioni maligne ( 1 carcinoma tubulare , 1 carcinoma duttale ascessualizzato e 1 sarcoma ) classi cate come bi - rads 4 sono state invece erroneamente considerate benigne alla valutazione elastosonogra ca . classe ecogra ca bi - rads 3 nella tabella 2 sono riportati i punteggi relativi alla valutazione elastosonogra ca delle 56 lesioni mammarie in classe radiol med ( 2011 ) 116 : 10271038 1033 table 3 ultrasound ( us ) elastography scores for the 28 breast imaging reporting and data system category 4 breast lesions us elastography score total ductal carcinoma ( 1 ) granuloma ( 2 ) sarcoma ( 1 ) fibroadenoma ( 2 ) adenosis ( 1 ) adenosis ( 1 ) tubular carcinoma ( 1 ) pseudoangiomatous hyperplasia ( 1 ) corpuscular cyst ( 1 ) adenosis ( 2 ) fibrosis ( 3 ) corpuscular cyst ( 1 ) idc ( 5 ) ductal carcinomain situ ( 1 ) lobular carcinoma ( 2 ) idc ( 3 ) the number of lesions is shown in brackets idc , invasive ductal carcinoma punteggio elastosonogra co tabella 3 punteggio elastosonogra co delle 28 lesioni mammarie in classe birads 4 carcinoma duttale ( 1 ) granuloma ( 2 ) adenosi ( 1 ) cdi ( 5 ) cdi ( 3 ) sarcoma ( 1 ) fibroadenoma ( 2 ) adenosi ( 1 ) carcinoma tubulare ( 1 ) iperplasia pseudoangiomatosa ( 1 ) cisti corpuscolata ( 1 ) carcinoma duttale in situ ( 1 ) carcinoma lobulare ( 2 ) adenosi ( 2 ) fibrosi ( 3 ) cisti corpuscolata ( 1 ) tra parentesi indicato il numero di lesioni cdi , carcinoma duttale in ltrante totale fig . 
b - mode ultrasound ( us ) ( right ) depicts a heterogeneous hypoechoic lesion with irregular margins and a diameter of 6 mm ( breast imaging reporting and data system us category 4 )  . 
allecogra a di base ( destra ) si apprezza una lesione ipoecogena a margini irregolari del diametro di 6 mm ( classe bi - rads ecogra ca 4 )  . 
a sinistra , la valutazione elastosonogra ca dimostra una marcata rigidit tissutale di tutta la lesione ( punteggio 5 )  . us elastography led to a different judgement from that obtained using b - mode us in 19 / 84 ( 22.6% ) cases , changing the initial b - mode us ndings from benign to malignant in ten cases and from malignant to benign in the remaining nine . 
nessuna di queste ha presentato un punteggio elastosonogra co pari a 5 , tuttavia 10 / 56 ( 17 , 9% ) di queste ultime hanno presentato un punteggio elastosonogra co pari a 4 , deponente quindi per malignit . 
tale giudizio stato confermato dallesame istologico in tre casi di carcinoma duttale in ltrante , ma sconfessato nei rimanenti sette casi ( 4 broadenomi , 2 aree di steatonecrosi , 1 cisti corpuscolata )  . 
 b - mode ultrasound ( us ) ( right ) shows a heterogeneous hypoechoic lesion with a diameter of 6 mm ( breast imaging reporting and data system us category 4 )  . 
 b - mode ultrasound ( us ) ( right ) depicts a homogeneously hypoechoic lesion without posterior acoustic enhancement showing regular margins , 5 mm in diameter ( breast imaging reporting and data system us category 3 )  . 
b - mode ultrasound ( us ) ( right ) depicts an isohypoechoic lesion with ill - de ned margins and a diameter of 15 mm ( breast imaging reporting and data system us category 4 )  . 
allecogra a di base ( destra ) si apprezza una lesione iso - ipoecogena a margini mal de niti del diametro di 15 mm ( classe bi - rads ecogra ca 4 )  . 
in contrast , six lesions correctly assessed as bi - rads 3 ( four broadenomas and two areas of fat necrosis ) were incorrectly assessed as malignant at us elastography . 
finally , three malignancies ( one tubular carcinoma , one abscessed ductal carcinoma and one sarcoma ) classi ed as bi - rads 4 were instead erroneously considered benign at us elastography . classe bi - rads 3 e con punteggio elastosonogra co di benignit ( da 1 a 3 ) , tre carcinomi ( 1 mucinoso , 1 tubulare e 1 duttale in ltrante ) hanno presentato un punteggio elastosonogra co di benignit , pari rispettivamente a 1 per il primo e 3 per i rimanenti due . 
applicando , dunque , il relativo sistema di punteggio alla classe bi - rads 3 lelastosonogra a ha presentato valori di sensibilit , speci cit , vpp e vpn pari rispettivamente a 50% , 86% , 30% e 93 , 5% ( tabella 4 )  . classe ecogra ca bi - rads 4 nella tabella 3 sono riportati i punteggi relativi alla valuradiol med ( 2011 ) 116 : 10271038 1035 table 4 sensitivity , speci city and positive and negative predictive values of ultrasound ( us ) elastography , overall and relative to the breast imaging reporting and data system ( bi - rads ) us classi cation . 
this assessment was con rmed by histology in three cases of invasive ductal carcinoma but refuted in the remaining seven cases ( four broadenomas , two areas of fat necrosis and one case of corpuscular cyst )  . 
 among the remaining 46 bi - rads 3 lesions with benign us elastography scores ( 13 ) , there were three carcinomas : one mucinous ( score 1 ) , one tubular ( score 3 ) and one invasive ductal carcinoma ( score 3 )  . 
therefore , applying the relevant scoring system to bi - rads 3 lesions , us elastography had sensitivity , speci city , ppv and npv of 50% , 86% , 30% and 93.5% , respectively ( table 4 )  . tazione elastosonogra ca delle 28 lesioni mammarie in classe ecogra ca bi - rads 4 . 
in particolare , 17 / 28 ( 60 , 7% ) di queste hanno presentato un punteggio elastosonogra co di malignit ( 4 o 5 ) , confermata in 11 casi allistologia , ma smentita nei rimanenti sei casi ( 3 brosi , 1 adenosi , 1 neoformazione intracistica e 1 iperplasia duttale semplice )  . 
di contro , tra le 11 lesioni in classe bi - rads 4 con punteggio elastosonogra co di benignit ( 13 ) lesame istologico ha confermato la presenza di 1 carcinoma ascessualizzato , 1 sarcoma e 1 carcinoma tubulare , rispettivamente presentanti allindagine elastosonogra ca un punteggio di 1 , 2 e 3 . 
this was con rmed by histology in 11 cases but refuted in the remaining six ( three cases of brosis , one adenosis , one intracystic mass and one simple ductal hyperplasia )  . 
in contrast , among the 11 bi - rads 4 lesions with benign us elastography scores ( 13 ) , histology revealed in accordo con quanto riportato da alcuni autori , nel nostro studio , mirato alla valutazione del ruolo dellelastosonogra a nelle lesione focali mammarie indeterminate allecogra a di base , non abbiamo riscontrato differenze statisticamente signi cative tra le due metodiche in termini di sensibilit , speci cit e valori predittivi , positivo e negativo [ 12 , 13 ]  . 
complessivamente , nella nostra esperienza , lelastosonogra a ha dimostrato una sensibilit del 70% , infe1036 radiol med ( 2011 ) 116 : 10271038 the presence of one abscessed carcinoma , one sarcoma and one tubular carcinoma , with us elastography scores of 1 , 2 and 3 , respectively . 
overall , in our experience , us elastography had a sensitivity of 70% , lower than reported by other authors ( 7996.9% ) and a speci city of 79.6% , within the range reported in the literature ( 7689% ) [ 8 , 12 , 14 , 15 ]  . 
one study only , with a 33.2% prevalence of malignant lesions , reported a sensitivity of 96.9% , but this was obtained using a different us elastography scoring system that is not directly comparable with the one adopted by us [ 15 ]  . 
in the case of indeterminate bi - rads 3 breast lesions , our ndings , in agreement with the literature , support the use of us elastography for its high npv and therefore its ability to con rm the benign nature of the lesion and thus avoid the need for biopsy [ 8 , 16 , 17 ]  . 
in particular , in our experience , us elastography proved particularly useful in corpuscular cysts , which passed from a score of bi - rads 3 ( probably benign ) to a us elastography score of 1 ( highly suggestive of benignity )  . 
in this regard , it should also be noted that riore ai valori riportati da altri autori variabili tra il 79% ed il 96 , 9% e una speci cit del 79 , 6% , compresa nellambito dei valori riportati in letteratura ( 76%89% ) [ 8 , 12 , 14 , 15 ]  . 
 infatti , avendo escluso dalla nostra analisi la classe ecograca bi - rads 5 , per la quale il campionamento bioptico gi indicato , la prevalenza di lesioni maligne risultata , nella nostra casistica , pari al 33 , 8% , dunque nettamente inferiore a quella di altri studi , che presentavano punte anche del 76% [ 6 , 8 , 12 ]  . 
solo in uno studio , con prevalenza di lesioni maligne pari al 33 , 2% , si riscontrata una sensibilit pari al 96 , 9% , ma impiegando un punteggio elastosonogra co diverso e quindi non direttamente comparabile a quello usato nel presente lavoro [ 15 ]  . 
nel caso , dunque , di lesione mammaria indeterminata in classe ecogra ca bi - rads 3 , la valutazione statistica dei nostri dati , in accordo a quanto riportato in letteratura , supporta limpiego dellelastosonogra a per il suo elevato vpn e , quindi , per confermare la natura benigna di una lesione , evitando il ricorso alla biopsia [ 8 , 16 , 17 ]  . 
nella nostra esperienza , in particolare , il contributo della valutazione elastosonogra ca risultato particolarmente utile nel caso delle cisti corpuscolate , passate nella quasi totalit dei casi da un punteggio bi - rads 3 , pur indicativo di probabile benignit , ad uno elastosonogra co 1 , altamente suggestivo di benignit . 
 a tale proposito , appare opportuno ricordare come anche lanalisi color doppler possa fornire utili indicazione al ne di distinguere le cisti non tumorali dai tumori mammari intracistici [ 18 ]  . 
tuttavia , tre carcinomi classi cati come bi - rads 3 ( 1 mucinoso , 1 tubulare e 1 duttale in ltrante ) hanno presentato , nella nostra serie , un punteggio elastosonogra co di benignit , almeno in parte da mettere in relazione alle caratteristiche istologiche , quali lelevato contenuto di mucina , o alle dimensioni superiori a 2 centimetri , situazione questultima che pu condizionare la disoradiol med ( 2011 ) 116 : 10271038 1037 colour doppler can help to distinguish nontumoural cysts from intracystic breast carcinomas [ 18 ]  . 
however , three carcinomas classi ed as bi - rads 3 ( one mucinous , one tubular and one invasive ductal ) had a benign us elastography score , at least in part as a result of histological features such as high mucin content , or a size > 2 cm that can lead to lesion heterogeneity due the presence of necroticcolliquative areas , as demonstrated by giuseppetti et al . 
in this regard , it would seem appropriate to periodically follow - up bi - rads 3 lesions not subjected to biopsy in order to assess their stability over time and thus lower the risk of missing the opportunity of early diagnosis of a possible malignancy [ 19 ]  . 
in contrast , the ppv of us elastography in bi - rads 4 focal breast lesions 64.7% in our experience is not suf ciently high to the need for biopsy on the basis of the us elastography score alone , as suggested by a previous report on nonpalpable breast lesions [ 12 ]  . 
in addition , although all bi - rads 4 lesions with a us elastography score of 5 proved to be ductal carcinomas at histological examination , six of the 14 bi - rads 4 lesions with a us elastography score of 4 turned out to be benign . 
this is con rmed by the fact that an abundant brotic component accounted for a malignant us elastography score in four broadenomas in our series , whereas the majority of broadenomas ( 25 / 29 , 86% ) had a high level of elasticity and consequently a benign us elastography score . there are several limitations to our study . 
first , the reference standard was not histological examination of the surgical specimen in all cases , but the semiological criteria used in cyto - microhistological evaluation , known in the literature and commonly used in clinical practice . 
in addition , as all us elastography examinations were performed by a single operator , it was not possible to assess the interoperator variability of this relatively new us technique . 
further research is needed to evaluate these aspects . in conclusion , by providing additional diagnostic information regarding the elasticity of breast lesions , us elastography completes but does not in any way replace the mogeneit della lesione per la presenza di aree necroticocolliquative , come gi dimostrato da giuseppetti et al . 
 a tale proposito , appare opportuno controllare periodicamente le lesioni classi cate come bi - rads 3 , ancorch non sottoposte a biopsia , al ne valutarne la stabilit nel tempo e , quindi , di ridurre la possibilit di non diagnosticare tempestivamente una eventuale lesione maligna [ 19 ]  . 
di contro , il vpp riportato dallelastosonogra a nellanalisi delle lesioni focali mammarie bi - rads 4 , pari nella nostra esperienza al 64 , 7% , non risulta abbastanza soddisfacente da consentire di escludere il ricorso alla biopsia sulla scorta del solo punteggio elastosonogra co , in accordo con quanto suggerito da un precedente studio condotto su lesioni mammarie non palpabili [ 12 ]  . 
inoltre , sebbene tutte le lesioni in classe bi - rads 4 con punteggio elastosonograco pari a 5 si siano rivelate dei carcinomi duttali allindagine istologica , sei delle 14 lesioni focali in classe bi - rads 4 con punteggio elastosonogra co pari a 4 si sono rivelate in realt benigne . 
a conferma di quanto appena esposto , proprio la presenza di abbondante componente brotica stata alla base del riscontro di un punteggio elastosonogra co di malignit in quattro broadenomi della nostra serie . 
questi ultimi , di contro , hanno presentato nella maggior parte dei casi ( 25 / 29 , 86% ) unelavata elasticit e , di conseguenza , un punteggio elastosonogra co di benignit . 
in primo luogo lo standard di riferimento non stato , in tutti i casi , la valutazione istologica del resecato operatorio , bens i criteri semeiologici alla valutazione cito - microistologia , ancorch noti in letteratura e comunemente impiegati nella pratica clinica . 
inoltre , un solo operatore ha effettuato tutti gli esami elastosonogra ci e , pertanto , non stato possibile valutare la variabilit interoperatore di una metodica di impiego relativamente recente come lelastosonogra a . 
ulteriori studi sono auspicabili per valutare tali aspetti . in conclusione , nella nostra esperienza , lelastosonogra a , fornendo ulteriori informazioni diagnostiche circa lelasticit delle lesioni mammarie , completa ma non sostituisce in alcun modo la valutazione morfologica dellesame ecogra co in b - mode . 
gemelli , largo francesco vito 1 , 00168 roma , italy 2unit operativa di radiodiagnostica , ospedale civile del ceppo , pistoia , italy 3unit di biostatistica , dipartimento di farmacologia clinica ed epidemiologia , consorzio mario negri sud , santa maria imbaro ( ch ) , italy 4unit operativa di ortopedia e traumatologia , ospedale g . 
forty - eight patients ( 40 men , eight women ; mean age , 31 years ) underwent arthroscopic reconstruction of the acl using double - strand semitendinosus and gracilis tendons . 
all patients underwent mr imaging 12 months after surgery and clinical evaluation at 6 and 12 months using the international knee documentation committee ( ikdc ) scoring systemr imaging and clinical features were correlated using the mannwhitney u test for continuous variables and fishers exact test for categorical variables . 
quarantotto pazienti ( 40 uomini e 8 donne , et media : 31 anni ) sono stati sottoposti a ricostruzione artroscopica del lca , utilizzando i tendini semitendinoso e gracile ( dgst )  . 
tutti i pazienti sono stati sottoposti ad esame rm , sono stati valutati 12 mesi dopo lintervento chirurgico e valutati clinicamente a 6 e 12 mesi , in accordo con linternational knee documentation commitee scoring ( ikcd test )  . 
misalignment of the ligament - screw system and the tibial tunnel and the presence of uid in the tibial tunnel appear to be directly correlated with clinical instability . keywords knee mr imaging anterior cruciate ligament tibial tunnel clinicamente instabili vs . 
 72 , 55 , 5 per langolo calcolato sullimmagine coronale del nuovo lca ( p = 0 , 3248 ) ; era presente uido nel tunnel tibiale rispettivamente nel 42 , 9% e nel 9 , 8% ( p = 0 , 2104 )  . 
 parole chiave ginocchio rm legamento crociato anteriore tunnel tibiale introduction introduzione arthroscopic reconstruction of the anterior cruciate ligament ( acl ) is performed by graft xation in tunnels drilled into the tibia and femur . 
 [ 2 ] reported that the direct contact between the graft and the bone inside the tunnel is crucial for integration within 912 weeks . in our study , we refer to the xation system that , following the indications of weil et al . 
the graft is prepared and secured at the proximal extremity using two poly - l - lactic acid screws , whereas a device consisting of a sheath and a conical screw made of 70% poly - l - lactic acid ( plla ) and 30% tricalcium phosphate ( tcp ) is inserted into the tibia [ 37 ]  . 
fixation with bioabsorbable material assists the radiologist in that it avoids interference caused by metal structures that distort magnetic resonance ( mr ) imaging and limit its use in the study of graft healing [ 9 ]  . 
 [ 11 ] observed that central xation of the new ligament is more effective , as it produces a stronger biological stimulus for osteointegration . la ricostruzione artroscopica del legamento crociato anteriore ( lca ) viene attualmente eseguita mediante la ssazione di graft in tunnel costruiti nella tibia e nel femore . 
 il neo - legamento viene preparato e ssato allestremit prossimale con 2 chiodini in acido polilattico , mentre nella tibia si ricorre ad un device costituito da una guaina ed una vite conica composte per il 70% di acido poli - l - lattico ( plla ) e dal 30% di fosfato tricalcico ( tcp ) [ 37 ]  . 
la ssazione con mezzi riassorbili di ausilio al lavoro del radiologo perch si eliminano le interferenze che le strutture metalliche hanno con gli esami strumentali e che modi cano le immagini in risonanza magnetica ( rm ) , limitandone luso nello studio della guarigione dellinnesto [ 9 ]  . 
i mezzi di ssazione in acido polilattico subiscono la degradazione , ma la ssazione primaria permane per il periodo neces1126 radiol med ( 2011 ) 116 : 11241133 mr imaging , with its high speci city ( 85100% ) and sensitivity ( 82100% ) due to the ability to identify direct and indirect signs , is considered the method of choice for characterising acl injuries and is routinely used in clinical practice [ 12 , 13 ]  . 
the site of the tibial tunnel is of crucial importance in acl reconstruction , and in particular , it has been shown that impingement with the anterior condylar roof is one of the leading causes of failure of the procedure [ 1418 ]  . 
the purpose of our study was to evaluate the following with mr imaging : position of the tibial tunnel in relation to blumensaats line in sagittal images and the angle between the ligament - screw system and the tibial surface as measured in coronal images ; presence of uid inside the tunnel and correlation with clinical instability ; alignment between the ligament - screw system and the tibial tunnel ; clinical signs of knee stability in patients treated with arthroscopic acl reconstruction . materials and methods the study was approved by the ethics committee , and all patients gave signed informed consent . 
 from july 2004 to october 2005 , we recruited 48 patients ( 40 men and eight women ; mean age 31 years ; range 1847 years ) who underwent arthroscopic acl reconstruction using the semitendinosus and gracilis tendons as a gra in 16 patients , the orthopaedic surgeon found a traumatic lesion of the internal meniscal brocartilage . graft xation was obtained with a bioabsorbable version of the intra x device , known as bio - intra x ( mitek ) and consisting of 70% poly - l - lactic acid ( plla ) and 30% tricalcium phosphate ( tcp )  . 
assessments were performed by an orthopaedic surgeon with extensive experience in knee disorders and based on the international knee documentation committee ( ikdc ) scoring syste according to the results , the patients were subdivided into three groups ( a , b and c )  . 
the study protocol consisted of the following sequences : proton - density fat - saturated turbo spin - echo ( pd - fs - tse ) with fat suppression in the axial and sagittal sario allosteointegrazione dellimpianto [ 10 ]  . 
 [ 11 ] hanno osservato che la ssazione concentrica del neolegamento pi ef cace poich produce uno stimolo biologico maggiore allosteointegrazione . la rm , presentando unalta speci cit ( 85%100% ) e sensibilit ( 82%100% ) , grazie alla sua capacit di evidenziare segni diretti ed indiretti , considerata metodica delezione per laccertamento delle lesioni del lca e di utilizzo quotidiano nella pratica clinica [ 12 , 13 ]  . 
lalloggiamento del tunnel tibiale risulta di particolare importanza per la ricostruzione del lca , in particolare si rilevato che limpingement con il tetto condilare anteriore tra le pi rilevanti cause di fallimento di questintervento [ 1418 ]  . 
 lobiettivo del nostro studio stato valutare con le immagini rm quanto segue : la posizione del tunnel tibiale rispetto alla linea di blumensaat nelle immagini sagittali e langolo formato dal sistema vite - camicia - ligamento con la super cie tibiale misurato nelle immagini coronali ; la presenza di liquido nel tunnel e la correlazione con lallineamento del sistema vite - camicia - ligamento ed il linstabilit clinica ; tunnel tibiale ; i segni clinici di stabilit del ginocchio in pazienti sottoposti a ricostruzione artroscopica del lca . materiali e metodi per questo studio , stato ottenuto il permesso del comitato etico e tutti i pazienti hanno rmato il consenso informato . 
sono stati reclutati quarantotto pazienti ( 40 uomini e 8 donne , et media 31 anni ; range tra 18 e 47 anni ) , tra luglio 2004 ed ottobre 2005 , e sottoposti ad intervento di ricostruzione artroscopia del lca , utilizzando i tendini semitendinoso e gracile come gra in 16 pazienti il chirurgo ortopedico ha riscontrato lesione traumatica della brocartilagine meniscale interna . la ssazione del graft stata ottenuta con una versione riassorbibile del device , detto intra x , il bio - intra x ( mitek ) , costituito dal 70% di plla e per il 30% da tcp . 
 tutti i pazienti sono stati sottoposti a controllo clinico per valutare il grado di stabilit del ginocchio da chirurgo ortopedico con elevata esperienza in patologia di ginocchio , utilizzando il ikdc test a 6 ( t1 ) e 12 ( t2 ) mesi dopo lintervento . 
we used 3 - mm slice thickness , 0.30.5 interval , 512512 matrix , 14 - cm eld of view ( fov )  . images were analysed by two trainee radiologists , and one consultant radiologist with 18 years of experience in musculoskeletal radiology . 
images were assessed for the position of the tibial tunnel in relation to blumensaats line , the coronal angle between the acl and tibial articular surface , sagittal alignment of the long axis of the ligamentscrew system with the tibial tunnel and the presence of uid inside the tunnel . 
under normal conditions , if a line is drawn tangential to the anterior acl margin , the two lines intersect at the level of the condylar insertion of the acl forming an angle anteriorly [ 19 ]  . 
all those who analysed the mr images were blinded to the results of the clinical assessment . statistical associations between mr parameters and clinical stability were analysed using the mannwhitney u test for continuous variables and fishers exact test for categorical variables . 
il protocollo di studio prevedeva le seguenti sequenze : proton density - turbo spin echo con soppressione del segnale adiposo ( pd - tse ) sui piani assiale e sagittale ( tempo di ripetizione [ tr ] = 4740 , tempo di eco [ te ] = 33 ) , pd - tse sul piano sagittale ( tr = 2000 , te = 32 ) , fat saturated ( fs ) - t1 sul piano coronale ( tr = 1150 , te = 16 )  . 
 stato utilizzato uno spessore di strato di 3 mm , 0 , 30 , 5 di intervallo , matrice di acquisizione 512512 , campo di vista ( fov ) di 14 cm . le immagini sono state studiate da due specializzandi e da uno specialista radiologo con elevata esperienza ( 18 anni ) in radiologia muscolo - scheletrica . 
stata valutata la posizione del tunnel tibiale rispetto alla linea di blumensaat , langolo coronale del lca rispetto alla super cie articolare tibiale , lallineamento dellasse maggiore del sistema vite - camicia - legamento e del tunnel sul piano sagittale , ed in ne la presenza di uido allinterno del tunnel . 
se si traccia una linea tangente al margine anteriore del lca , in condizioni di normalit , le due linee si incrociano normalmente a livello dellinserzione condiloidea del lca , formando un angolo che si apre anteriormente [ 19 ]  . 
1 posizione del tunnel tibiale secondo la classi cazione del metodo di muneta , rispetto alla linea di blumensaat . using sas software ( statistical package release 9.1 sas institute , cary , nc , usa )  . hanno analizzato le immagini non erano a conoscenza della valutazione clinica . radiol med ( 2011 ) 116 : 11241133 1128 results on the basis of the clinical assessment with the ikdc scoring system at 12 months ( table 1 ) , 28 patients were assigned to group a . 
the examiner stands on the side of the injured knee and pulls the tibia anteriorly ; a sensation of giving way or a nonrigid endpoint is a sign of acl injury . 
 mr imaging is the method of choice for the follow - up of acl reconstruction and to assess graft complications [ 14 , sono state analizzate le associazioni statistiche tra i parametri rm e la stabilit clinica del paziente con il mann - whitney u test per le variabili continue ed il fisher exact test per le variabili categoriche . 
tutte le analisi sono state fatte da un esperto in materia , utilizzando il statistical package software ( sas , release 9 , 1 , sas institute , cary , nc , usa )  . risultati sulla base della valutazione clinica con lo schema ikdc a 12 mesi ( tabella 1 ) , ventotto pazienti sono stati inseriti nel gruppo a . 
il test di lachman il pi sensibile e viene eseguito per fare diagnosi clinica di lesione del legamento crociato anteriore con il paziente in posizione supina con il ginocchio a 20 di essione , lesaminatore si pone dal lato del ginocchio leso e tira la tibia in avanti ; una sensazione di cedimento o un punto di blocco non rigido sono indici della lesione del lca . 
2 proton - density fat - saturated turbo spin - echo in the sagittal plane : misalignment between the screw and tibial tunnel ( arrow ) ; oedema is seen inside and on the anterior wall of the tunnel . 
2 scansione pd - tse - fs sul piano sagittale : si noti lanomalo decorso della vite rispetto al tunnel osseo ( freccia ) ; si segnala la presenza di edema nel tunnel e nella parete anteriore . 
3 proton - density fat - saturated turbo spin - echo in the sagittal plane : evident misalignment of the screw , which is enveloped by its expansion sheath ( arrow )  . 
la giusta posizione del tunnel tibiale ha un ruolo importante nelloutcome della ricostruzione , per evitare impingement con il tetto condilare anteriore ed il conseguente fallimento del lca [ 14 , 15 ]  . 
questo valore cut - off in buona correlazione con i nostri risultati 77 , 311 , 3 nel gruppo c e 72 , 55 , 5 nei gruppi a e b . 
 i nostri risultati sulla posizione del tunnel tibiale rispetto alla linea di blumensaat e langolo coronale del graft , comunque , non sono stati statisticamente signi cativi , con una grande deviazione standard rispetto ai valori medi . 
 probabilmente , sarebbe stata necessaria una popolazione pi ampia di pazienti instabili e questo senzaltro il principale limite del nostro studio . abbiamo osservato nel 42 , 9% dei pazienti instabili e nel 9 , 8% dei pazienti stabili una reazione edematosa nella porzione anteriore del tunnel tibiale con in ltrazione di liquido nello spazio tra losso e il graft , probabilmente dovuta ad una perdita della compressione concentrica sul gratale condizione necessita di uno stretto follow - up per fig . 
5 proton - density fat - saturated turbo spin - echo in the axial plane : misalignment between the central portion of the screw and the ligaments displaced to the medial wall of the tunnel ( arrow )  . 
5 scansione pd - tse - fs sul piano assiale : si nota come la porzione centrale della vite sia mal posizionata rispetto ai legamenti disposti tutti sul versante mediale del tunnel ( freccia )  . 
correct placement of the tibial tunnel is crucial for the outcome of the procedure , and in particular for avoiding impingement against the condylar roof anteriorly and subsequent failure of the reconstruction [ 14 , 15 ]  . 
 however , our ndings regarding tibial tunnel position in relation to blumensaats line and the coronal acl angle failed to reach statistical signi cance , showing a high standard deviation of the mean values . 
6a proton - density turbo spin - echo ( pd - tse ) in the sagittal plane : different layers interposed between the bone tunnel and tibial screw are evident . 
6a scansione pd - tse sul piano sagittale : sono ben evidenti le differenti strutture interposte tra il tunnel osseo e la vite tibiale ; procedendo in senso antero - posteriore possiamo documentare la linea ipointensa del tunnel , la stria ipointensa dei legamenti e della camicia , le spire della vite , la parete ed in ne la porzione centrale , cava , della vite ( freccia )  . 
b scansione pd - tse - fs sul piano sagittale : sono ben evidenti le stesse strutture documentate nella scansione in a ; la porzione cava della vite appare iperintensa ( freccia )  . 
 some authors [ 22 , 24 ] report high mr signal intensity in correspondence with the screwbone and ligamentbone interfaces in t2 - weighted images and persistence of uid inside the tibial tunnel , probably due to failed osteointegration , leading to knee instability . 
furthermore , in some cases , it was dif cult to identify the systems expansion valutare se lo slargamento del tunnel pu essere responsabile dellinstabilit del gra alcuni autori [ 22 , 24 ] hanno riscontrato iperintensit del segnale rm in corrispondenza delle interfacce vite - osso e legamento - osso nelle immagini t2 - pesate e persistenza del liquido nel tunnel tibiale , probabilmente dovuti alla mancata osteointegrazione del neo - legamento , causando linstabilit del ginocchio . 
il nostro studio ha mostrato disallineamento del sistema vite - camicia - legamento e tunnel tibiale nel 57 , 1% dei pazienti clinicamente instabili ( gruppo c ) e nel 12 , 2% dei pazienti clinicamente stabili ( gruppi a e b )  . 
in the future , we intend to expand the case series to reach a statistically signi cant correlation between clinical instability and tibial tunnel position in relation to blumensaats line and the coronal angle in unstable patients , and to strengthen our ndings with a 2 - year follow - up of the patients enrolled . 
 osteo - induzione del sistema stesso . in conclusione , il disallineamento del sistema vitecamicia - legamento rispetto al tunnel tibiale e la presenza di liquido nel tunnel sembrano essere direttamente correlati con linstabilit clinica . 
i nostri obiettivi futuri saranno ampliare la casistica per raggiungere una correlazione , statisticamente signi cativa , tra linstabilit clinica con la posizione del tunnel tibiale rispetto alla linea di blumensaat e langolo coronale nei pazienti instabili ed incrementare i risultati con un follow - up a due anni dei pazienti arruolati . 
as it happens in fortunate research elds , three dimensional echocardiography , at rst aiming to add spatial information for better anatomic study , has recently been shown to provide ne physiologic information on myocardial wall motion when coupled with the very new technique of speckle tracking - derived velocity information . 
as such , the medical community is eager to receive solid information on whether the effort and investments have been worthwhile and possibly on how to handle this complex subject . 
the scheme of presentation helps the reader to appreciate the history of the technical evolution , to recognize how limitations in sampling rate have been arranged both for imaging and doppler velocimetry . 
since the learning curve may be strongly in uenced by the capability of physicians to cope with it , the authors devoted a special effort to explain the different modalities and commented on a large number of gures and video - clips . 
the role of 3d - echocardiography emerging in cardiac dyssynchrony is addressed in detail and with caution , especially following the disappointments with the 2d - echo - derived indexes in recent years . 
 the need for an adequate learning curve is correctly stressed , although small studies suggest its usefulness to predict bene t from resynchronization therapy . lecocardiogra a tridimensionale ( ecocardio - 3d ) giunta a maturit per lapplicazione clinica dopo un lungo periodo di progressi tecnici e gli scienziati che hanno iniziato da pionieri questo campo di ricerca possono godere ora del successo dei loro sforzi . 
come si veri ca in campi di ricerca fortunati , lecocardio - 3d che si pre ggeva , alle sue origini , di fornire ulteriori informazioni spaziali per una miglior valutazione anatomica , ha dimostrato ultimamente la capacit di poter fornire ni informazioni siologiche sulla motilit della parete miocardica , se associata con la assai nuova tecnica dellinformazione della velocit derivata dallo speckle tracking . 
appunto perch tale , la comunit medica desiderosa di ricevere informazioni ben precise per riconoscere se gli sforzi e gli investimenti fatti siano stati utili e pro cui e , se possibile , su come utilizzare questa complessa materia . il volume dal titolo three - dimensional echocardiography merita una menzione particolare sia per la capacit che per lottimo e comprensibile modo in cui presenta sinteticamente largomento . la scaletta della presentazione aiuta il lettore ad apprezzare la storia dellevoluzione tecnica ed a riconoscere come le limitazioni delle esempli cazioni siano state ben ordinate sia per le immagini che per la velocimetria doppler . 
dal momento che la curva di apprendimento pu essere in uenzata dalla capacit di adattamento dei medici , gli autori hanno dedicato uno sforzo speciale alla spiegazione delle differenti modalit , dedicando molta attenzione e commenti ad un grande numero di gure e video - clips . 
 viene poi illustrato , sia nel dettaglio che con precauzione , il ruolo emergente dellecocardio - 3d nella valutazione della dissincronia cardiaca , soprattutto a seguito delle disillusioni avute negli ultimi anni relativamente agli indici derivati dallecocardio - 2d . viene evidenziata correttamente la necessit di una adeguata curva di apprendimento della metodica , anche se studi di limitate dimensioni suggeriscono la sua utilit nel predire 1150 radiol med ( 2011 ) 116 : 11491150 the two chapters devoted to the investigation of valve diseases are particularly well written . 
the large number of examples is remarkable and all together constitute a guide to clinical investigation planning , since 3d - echocardiography is far less intuitive than 2d - echo . 
 the fact that 3d - echo may add information in the clinical arena but at the expense of a careful learning curve is well demonstrated with gures and video in the last four chapters on congenital heart diseases , cardiac tumours and sources of embolism and monitoring guiding cardiac interventions and surgery . 
 in summary , this text provides the reader with consistent information in a concise manner that could be useful both to beginners and veterans . bene cio dalla terapia di risincronizzazione . i due capitoli dedicati alla valutazione delle valvulopatie sono particolarmente ben scritti . 
straordinario il gran numero di esempi che nel loro insieme costituiscono una guida nella piani cazione della valutazione clinica , dal momento che lecocardio - 3d assai meno intuitiva dellecocardio - 2d . il fatto che lecocardio - 3d possa aggiungere informazioni nellambito clinico , ma a spese di una appropriata ed accurata curva di apprendimento , ben dimostrato negli ultimi quattro capitoli sulle cardiopatie congenite , i tumori del cuore , le cause dei fenomeni di embolizzazione e nel monitoraggio - guida alle procedure cardiovascolari e agli interventi chirurgici . in conclusione , questo volume fornisce al lettore , in modo succinto , informazioni coerenti , utili sia per il principiante che per lesperto . franco recusani divisione di cardiologia , fondazione irccs policlinico s . 
three hundred and ninety - two patients with liver or / and spleen trauma ( 179 liver and 217 spleen injuries ) , who underwent ceus examinations following contrast - enhanced computed tomography ( ct ) , were enrolled in this retrospective study over a period of > 4 years . 
ceus detected contrast medium extravasation or pooling in 16% ( 63 / 396 ) of liver or spleen lesions in 61 patients , which was con rmed by contrast - enhanced ct . 
of 63 lesions in 61 patients , ceus showed that 74.6% ( 47 / 63 ) ( 21 liver lesions and 26 spleen lesions ) presented contrast medium extravasation or pooling , both in the organ and out the capsule , in 14.3% ( 9 / 63 ) and only outside the capsule in 11.1% ( 7 / 63 )  . 
trecentonovantadue pazienti con trauma epatico e / o splenico ( 179 traumi epatici e 217 splenici ) , sottoposti ad esame ceus seguito da tomogra a computerizzata ( ct ) con mezzo di contrasto , sono stati arruolati in questo studio retrospettivo per un periodo di pi di 4 anni . 
la ceus ha rilevato lo stravaso o laccumulo di mdc nel 16% ( 63 / 396 ) delle lesioni epatiche o spleniche in 61 pazienti , confermato poi dalla tc con mezzo di contrasto . 
le informazioni ottenute dalla chirurgia , sia dal trattamento minimamente invasivo sia da quello conservativo , presi come riferimento standard , e la sensibilit delle due tecniche non si sono dimostrate differenti ( p = 0 , 122 )  . 
 nelle 63 lesioni in 61 pazienti , la ceus ha mostrato che il 74 , 6% ( 47 / 63 ) delle lesioni ( 21 lesioni epatiche e 26 spleniche ) ha presentato stravaso o accumulo di mdc , entrambi allinterno dellorgano o fuori dalla capsula nel 14 , 3% ( 9 / 63 ) e solo fuori dalla capsula nell11 , 1% ( 7 / 63 )  . 
 limaging ceus del sanguinamento attivo da traumi epatici e splenici presenta differenti caratteristiche , e le dimensioni e le forme del sanguinamento attivo dovuto allo stravaso o allaccumulo del mezzo di contrasto sono variabili . 
la ceus pu mostrare il sanguinamento attivo associato a trauma epatico e splenico con diverse caratteristiche di imaging , rendendo quindi possibile diagnosticare il sanguinamento attivo . parole chiave fegato milza trauma sanguinamento attivo mezzo di contrasto ecogra a microbolle introduction active bleeding from hepatic and splenic trauma is a major cause of death and disability . 
digital subtraction angiography ( dsa ) cannot only be used to identify active bleeding but also to arrest bleeding after penetrating trauma to the abdomen [ 5 , 6 ]  . 
additional drawbacks include : ( a ) high expense , ( b ) need for highly trained staff and ( c ) need for patient transfer from the emergency department . 
 with the development of contrast media , contrast - enhanced ultrasound ( ceus ) has improved the sensitivity of conventional us for detecting and characterising focal liver lesions [ 10 ]  . 
performed ceus examinations in 83 traumatic emergencies , and their clinical study showed for the rst time how us can detect contrast medium extravasation , a signi cant indicator of active haemorrhage . 
thus , the purpose of our study was to observe the ceus imaging features of active bleeding from hepatic and splenic trauma . materials and methods the study was approved by the ethics committee of the chinese peoples liberation army general hospital and was designed according to the health insurance portability and accountability act . 
informed consent for both ceus and the use of related data for future research was obtained from each patient before and after the procedure . patients a total of 392 patients with liver and / or spleen trauma ( 179 liver and 217 spleen injuries ) were enrolled in this retrospective study covering a period of > 4 years ( september 2004 to december 2008 )  . 
 ultrasound imaging us contrast agent used in this study was sonovue ( bracco , milan , italy ) , a second - generation contrast medium for diagnostic imaging approved in china in 2003 , which consists of stabilised microbubbles containing an inert gas ( sulfur hexa uoride , 8 l / ml of solution ) and covered by a phospholipid membrane [ 15 ]  . 
sonovue , a dose of 0.025 ml / kg , was administered as a quick bolus through an antecubital ve 1078 ultrasound image interpretation two us specialists , each with 5 years experience in diagnosing abdominal parenchymal organ trauma , performed the examinations . 
for patients not undergoing further diagnostic procedures or surgery , follow - up information was obtained from either the patients chart or the trauma surgeon in charge of the patient . 
differences between group means were determined by analysis of variance ( anova ) ( systat ver 13.0 , spss , inc , chicago , il , usa ) , with the chi - square test for 22 tables , where applicable . 
the 63 liver or spleen lesions with contrast - medium extravasation or pooling indicating active bleeding consisted of 29 liver and 34 spleen lesions . imaging of 63 lesions in 61 patients , ceus identi ed contrast medium extravasation or pooling in 74.6% ( 47 / 63 ) lesions ( 21 liver and 26 spleen ) , both in the lesion and out of the capsule in 14.3% ( 9 / 63 ) and only outside of the capsule in 11.1% ( 7 / 63 )  . 
i siti di emorragia attiva appaiono come spot a banda isolati , iperecogeni ed isoecogeni con dimensioni e forma variabili ( frecce ) b limmagine tc mostra la lesione epatica come unarea di bassa attenuazione ( frecce lunghe ) e dimostra il sanguinamento attivo come area di elevata attenuazione ( frecce corte ) a causa dello stravaso di mezzo di contrasto . brooklet or in a serpentine pattern . 
b within the lesion , there were enhanced perfusion regions , including the remaining normal parenchyma ( ne arrow ) and contrast medium extravasation and pooling ( thick arrow )  . 
a scansione ecogra ca trasversale obliqua della milza che mostra larea lesionata con aspetto anecogeno ed ipoecogeno con difetto di perfusione con margini irregolari nella regione medio - inferiore della milza . 
b allinterno della lesione ci sono regioni che presentano enhancement perfusionale e rappresentano parenchima residuo normale ( freccia sottile ) e stravaso e accumulo di mezzo di contrasto ( frecce spesse in a and b )  . 
the active bleeding disappeared in both patients 20 and 40 min , respectively , after ceus . discussion sonovue , the second - generation contrast medium used in this study , allows boosting of the lesion - to - parenchyma conspicuity , which increases us sensitivity . 
ceus has been largely employed in the evaluation of focal lesions [ 17 , 18 ] but also to improve us accuracy in detecting parenchymal organ injury after blunt abdominal trauma [ 1923 ]  . 
however , active bleeding not only presented as a hyperechoic area but also as a hyperechoic or isoechoic area , in contrast to the ndings of some recent studies [ 11 , 22 ]  . 
in addition , the active bleeding sites presented various shapes depending on the different locations , velocities and quantities . radiol med ( 2011 ) 116 : 10761082 1081 this study showed that the sensitivity of ceus was 72.4%. 
in the diagnosis of active haemorrhage from hepatic or splenic trauma , contrast - enhanced ct has several advantages over ceus , such as screening the entire abdomen and no limitations due to obesity , meteorism or subcutaneous emphysema . 
 in the diagnosis of active bleeding , ceus has several advantages : ( 1 ) it can detect active bleeding from hepatic and splenic trauma with excellent imaging characteristics ; ( 2 ) real - time imaging allows ceus to accurately evaluate active bleeding because active bleeding is characterised by activity . 
 ( 3 ) the examination is rapid , with a room time < 10 mthe use of ceus saves time and is safe . our study has several limitations : ( 1 ) ceus shares with conventional us several limitations , such as patient obesity , meteorism , subcutaneous emphysema etc . 
 ( 2 ) ceus requires rapid and skilful diagnosis because the duration of a single ceus examination is only 68 m ( 3 ) in theory , ceus can show active haemorrhage with any velocity . 
 ( 4 ) the real correlation between bleeding velocity and ceus imaging whether active bleeding from an artery , vein or capillary can be accurately detected or not needs to be investigated by further studies . 
it should not be intended as a substitute for ct but as a selective possibility to boost the role of us in the initial screening of patients with abdominal trauma . in conclusion , our study has shown that active haemorrhage from liver and spleen trauma appeared with various imaging features on ceus , according to which the diagnosis can be established . 
cademartiri1 , 2 1dipartimento di radiologia e del cardio - polmonare , azienda ospedaliero - universitaria di parma , c / o piastra tecnica piano 0 , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia e cardiologia , ospedale san gennaro , napoli , italy 4cpc centro prevenzione cardiovascolare , ospedale san raffaele , milano , italy 5dipartimento di radiologia e cardiologia , azienda asl , carrara , italy 6dipartimento di radiologia , universit di messina , messina , italy 7dipartimento di cardiologia , universit di foggia , foggia , italy 8dipartimento di radiologia , azienda ospedaliero - universitaria san martino , genova , italy correspondence to : f . 
we selected from a population of 1 , 500 patients in a multicentre registry with nstemi - acs who had undergone ctca and cag , ( n = 237 ; 187 men , mean age 6310 years )  . 
scopo del nostro lavoro stato valutare laccuratezza diagnostica dellangiogra a coronarica non invasiva con tomogra a computerizzata ( ctca ) nellindividuazione delle stenosi coronariche signi cative ( riduzione del lume coronarico 50% ) confrontata con la coronarogra a convenzionale ( cag ) nella sindrome coronarica acuta senza elevazione del tratto st ( acs - nstemi ) e nelle sue sottopopolazioni per genere e numero di fattori di rischio ( fdr )  . 
da una popolazione di 1500 pazienti appartenenti ad un registro multicentrico sono stati selezionati i pazienti con acs - nstemi ( 237 , 187 maschi , et media 6310 anni ) sottoposti a ctca e cag . 
ctca is a reliable diagnostic modality with high sensitivity and npv in nstemi - acs patients who are not candidates for early revascularisation , regardless of gender and number of risk factors . keywords ct coronary angiography conventional coronary angiography acute coronary syndrome nstemi risk factors diagnostic accuracy registry popolazione era del 53% . 
nellanalisi per paziente la sensibilit , speci cit , valore predittivo positivo e negativo della ctca sono risultati 100% ( maschi 100% ; femmine 100% ; 0rf 100% ; 1 - 2rf 100% ; > 2rf 100% ) , 95% ( maschi 98% ; femmine 50% ; 0rf nv% ( nv , non valutabile ) ; 12rf 96% ; > 2rf 96% ) , 95% ( maschi 98% ; femmine 91% ; 0rf 91% ; 1 - 2rf 96% ; > 2rf 96% ) , 100% ( maschi 100% ; femmine 100% ; 0rf nv% ; 1 - 2rf 100% ; > 2rf 100% ) , rispettivamente . 
la ctca una metodica diagnostica af dabile sia per lelevata sensibilit che per lelevato valore predittivo negativo nei pazienti con acs - nstemi non candidati ad immediata rivascolarizzazione , indipendentemente dal genere e dal numero di fattori di rischio . parole chiave angiogra a coronarica tc angiogra a coronarica convenzionale sindrome coronarica acuta nstemi fattori di rischio accuratezza diagnostica registro introduction introduzione computed tomography coronary angiography ( ctca ) is an accurate and robust modality for diagnosing and excluding coronary artery disease ( cad ) [ 18 ]  . 
given the limited information and absence of proper guidelines , the creation and sharing of multicentre registries with large patient populations guarantees an adequate response to the emerging questions surrounding the technique [ 2 , 16 ]  . 
 acute coronary syndrome ( acs ) is a clinical situation in which the short times of performing conventional coronary angiography ( cag ) and immediate revascularisation can be crucial [ 2 , 1733 ]  . 
however , acs is characterised by at least two major clinical presentations : acs with elevated st segment ( stemi ) and acs without elevated st segment ( nstemi ) [ 34 , 35 ]  . 
the latter includes unstable angina , which consists of the onset or worsening of typical chest pain , with no increase in markers of myocardial damage or st - segment elevation [ 34 ]  . 
for this category , a reliable diagnostic modality is desirable , and ctca has demonlangiogra a coronarica con tomogra a computerizzata ( ctca ) una metodica accurata e robusta per la diagnosi e lesclusione della malattia coronarica [ 18 ]  . 
la creazione e condivisione di registri multicentrici garantisce la possibilit di rispondere adeguatamente ai quesiti emergenti sulla metodica con ampie popolazioni di pazienti in presenza di scarse informazioni ed in mancanza di vere e proprie linee guida [ 2 , 16 ]  . 
 la sindrome coronarica acuta ( acs ) una situazione clinica nella quale i tempi brevi di esecuzione di una coronarogra a convenzionale e di una rivascolarizzazione immediata possono essere essenziali [ 2 , 1733 ]  . 
tuttavia , la acs costituita da almeno due grandi entit cliniche : la acs con elevazione del tratto st ( stemi ) e la acs senza elevazione del tratto st ( nstemi ) [ 34 , 35 ]  . 
questultima include langina instabile che consiste , in sintesi , nellesordio o nellaggravamento di una sintomatologia dolorosa toracica tipica senza lincremento dei markers di danno miocardico e lelevazione del tratto st [ 34 ]  . 
in questo caso il con ne tra acs e dolore toracico non coro1016 radiol med ( 2011 ) 116 : 10141026 strated signi cant potential in this group of patients [ 2 , 1733 ]  . in this study , we compared the diagnostic accuracy of ctca with cag in a population of patients with nstemiacs who were drawn from a multicentre registry [ 2 ]  . 
we selected patients with nstemi - acs from among the general population of the registry ( n = 237 ; 187 men , 50 women ; mean age 6310 years ; tables 1 and 2 ) [ 34 ]  . 
cdx , coronaria destra ; csx , coronaria sinistra ; tcs , tronco comune sinistro ; acx , arteria coronaria circon essa ; ada , arteria coronaria discendente anteriore . narico pu essere meno de nito ed in questa categoria che una metodica diagnostica af dabile sarebbe auspicabile . 
la ctca ha mostrato di avere un potenziale notevole in questa categoria di pazienti [ 2 , 1733 ]  . in questo lavoro presentiamo laccuratezza diagnostica della ctca a confronto con la coronarogra a convenzionale ( cag ) in una popolazione di pazienti con acsnstemi derivante da un registro multicentrico [ 2 ]  . 
 da maggio 2004 a giugno 2010 , sono stati studiati mediante ctca 1500 pazienti consecutivi ( 882 maschi , 490 femmine , et media 5812 anni ) , candidati allesecuzione di unangiogra a coronarica convenzionale ( cag ) allo scopo di determinare la presenza , la severit e lestensione della malattia coronarica [ 2 ]  . 
dalla popolazione generale del registro sono stati selezionati i pazienti con acs - nstemi ( 237 , 187 maschi , 50 femmine , et media 6310 anni ) ( tabelle 1 e 2 ) [ 34 ]  . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . analisi statistica i dati sono presentati come prevalenze , medie e deviazioni standard . 
la performance diagnostica dellangiogra a coronarica mediante ctca nellindividuazione delle lesioni aterosclerotiche coronariche signi cative , utilizzando la cag come tecnica di riferimento di seguito riportata come sensibilit , speci cit , valore predittivo positivo e negativo con intervalli di con denza ( ic ) al 95% calcolati con espansione binomiale . 
tutte le statistiche sono state eseguite per la popolazione totale , per la popolazione maschile e per quella femminile e nelle sotto - popolazioni strati cate per numero di fattori di rischio : 0rf = assenza di fattori di rischio ; 1 - 2rf = presenza di 1 o 2 fattori di rischio ; > 2rf = presenza di pi di 2 fattori di rischio . 
all statistics were calculated for total population , male and female populations and the subpopulations strati ed by number of risk factors ( rf ) ( 0 rf = no risk factors present ; 12 rf = one to two risk factors present ; > 2 rf = more than two risk factors present )  . 
mean heart rate during the examination was 595 bpthe prevalence of obstructive disease was 53% ( 126 / 237 ) , with a marked prevalence among women [ men 45% vs . 
nei sottogruppi suddivisi in base al numero di fattori di rischio si osserva un progressivo aumento dellet media ed un passaggio da una maggiore prevalenza di femmine con 0rf and una netta prevalenza di maschi con 1 - 2rf e > 2rf ( tabella 2 )  . 
subgroups subdivided on the basis of the number of rf showed a progressive increase in age and a shift from a higher prevalence of women with 0 rf and a marked prevalence of men with 12 rf and > 2 rf ( table 2 )  . 
per - patient positive likelihood ratios were optimal in all populations ( lr + between 18 and 27 ) , whereas negative likelihood ratios were excellent ( lr = 0.0 in all cases )  . 
no signi cant differences in diagnostic accuracy between the different subpopulations were observed . discussion acs is a clinical condition in which the short times of performing cag and immediate revascularisation can be crucial [ 2 , 1733 ]  . 
when possible , patients with typical chest pain , positivity for biomarkers of myocardial damage and stemi should be immediately sent to the catheterisation laboratory for prompt revascularisation . ctca has been proposed for early strati cation of patients with acute chest pain [ 16 , 29 , 31 , 33 , 3740 ] , which is present in 5%10% of patients presenting at the casualty ward . 
of these , 70%80% are classi ed as having non - angina - like pain , 7%8% as having acs and up to 7%8% as having nstemi and / or unstable angina . 
ctca may accurately and rapidly rule out signi cant cad in the setting of acute chest pain [ 16 , 31 , 33 , 37 , 38 ]  . acs consists of at least two major clinical entities : acs with stemi and acs with nstemi [ 34 , 35 ]  . 
i quozienti di probabilit positivi per segmento sono risultati ottimali in tutte le popolazioni ( lr + compresi tra 11 e 25 ) , mentre i quozienti di probabilit negativi sono risultati eccellenti ( lrcompresi tra 0 , 0 e 0 , 028 )  . 
i quozienti di probabilit positivi per paziente sono risultati ottimali in tutte le popolazioni ( lr + compresi tra 18 e 27 ) , mentre i quozienti di probabilit negativi sono risultati eccellenti ( lr - = 0 , 0 in tutti i casi )  . 
non sono state osservate differenze signi cative differenze di accuratezza diagnostica tra le sottopopolazioni . discussione la sindrome coronarica acuta ( acs ) una situazione clinica nella quale i tempi di esecuzione di una coronarogra a convenzionale e di una rivascolarizzazione immediata possono essere essenziali [ 2 , 1733 ]  . 
i pazienti con dolore toracico tipico , curva enzimatica di danno miocardico e elevazione del tratto st , quando possibile , dovrebbero essere inviati immediatamente al laboratorio di emodinamica per effettuare una rivascolarizzazione precoce . 
il dolore toracico acuto rappresenta il 5%10% dei pazienti che si presentano al pronto soccorso ; di questi il 70%80% vengono classi cati come dolore non anginoso , il 7%8% vengono classi cati come acs , e no al 7%8% vengono classi cati come nstemi e / o angina instabile . 
 la ctca potrebbe consentire un accurato e veloce ruleout della malattia coronarica signi cativa nel contesto del dolore toracico acuto [ 16 , 31 , 33 , 37 , 38 ]  . la acs costituita da almeno due grandi entit clinica : la acs - stemi e la acs - nstemi [ 34 , 35 ]  . 
questultima include anche lentit clinica denominata angina instabile che consiste , in sintesi , nellesordio di una sintomatologia dolorosa toracica tipica senza lincremento dei markers di danno miocardico e lelevazione del tratto st , oppure nellaggravamento di sintomatologia anginosa in una breve arco temporale [ 34 ]  . 
in questo caso il con ne tra acs e dolore toracico non coronarico pu essere meno de nito ed in questa categoria di pazienti che una metodica diagnostica af dabile sarebbe auspicabile . 
la ctca ha mostrato di avere un potenziale notevole in questa categoria di pazienti [ 2 , 1733 ]  . radiol med ( 2011 ) 116 : 10141026 1021 1022 radiol med ( 2011 ) 116 : 10141026 diagnostic accuracy per segment diagnostic accuracy per patient fig . 
per - patient accuracy shows high sensitivity and negative predictive values in all subgroups , whereas speci city and positive predictive value are lower in the female and 0 rf populations . 
gra co a barre dellaccuratezza diagnostica e dei quozienti di probabilit ( lr ) per segmento e per paziente della angiogra a coronarica con tomogra a computerizzata ( ctca ) nella popolazione totale e nei sottogruppi . 
laccuratezza diagnostica per paziente mostra valori elevati si sensibilit e valore predittivo negativo elevati in tutti i sottogruppi , mentre la speci cit ed il valore predittivo positivo sono inferiori nella popolazione femminile e nella popolazione 0rf . 
for this category of patients , a reliable diagnostic modality is desirable , and ctca has i dati del registro mostrano valori di accuratezza diagnostica ottimali ed in linea con le principali casistiche di validazione in pazienti stabili [ 4144 ]  . 
in particolare la sensibilit ed il valore predittivo per paziente sono risultati del 100% e 100% , rispettivamente , con valori di speci cit e radiol med ( 2011 ) 116 : 10141026 1023 demonstrated signi cant potential in this group of patients [ 2 , 1733 ]  . registry data show optimal accuracy values in line with the major validation series [ 4144 ]  . 
the second is the rule out myocardial infarction using computer assisted tomography ( romicat ) trial [ 29 ] , in which sensitivity and npv of ctca in acs were 100% and 100% , respectively , in 363 patients . 
the authors also suggest that the use of ctca in this category of patients could signi cantly reduce costs [ 25 ]  . evidence in the literature and data from our registry show that in cases of chest pain with suspected coronary origin ( nstemi - acs ) , ctca is able to provide adequate diagnostic accuracy , particularly for ruling out disease . 
 the costbene t ratio must take into account numerous factors , including biological cost ( dose of ionising radiation compared with tests that do not use ionising radiation ) , economic cost ( with respect to less expensive tests ) , geographic distribution of the technique ( compared with more commonly available modalities ) and expertise ( which is still limited in some centres )  . study limitations our series reports data recorded in the period when the most modern dose - reduction systems were not widely available . 
 however , the introduction of new hardware and software able to provide adequate image quality using prospective triggering based on the electrocardiographic signal has brought dose values to < 5 msv [ 912 ]  . 
in questo trial randomizzato controllato la ctca stata confrontata con lo standard of care ( soc , vale a dire stress tomogra a computerizzata a emissione di fotoni singoli [ spect ] )  . 
 [ 24 ] effettuato su 104 pazienti con nstemi gli autori hanno rilevato unottima accuratezza diagnostica della ctca per la rilevazione ed esclusione delle stenosi coronariche critiche ( vale a dire , sensibilit e valore predittivo negativo pari al 100% )  . 
gli autori suggeriscono inoltre che lutilizzo della ctca in questa categoria di pazienti potrebbe portare ad una signi cativa riduzione dei costi [ 25 ]  . le evidenze della letteratura ed i dati del nostro registro evidenziano pertanto che in caso di dolore toracico di sospetta origine coronarica ( acs - nstemi ) la ctca in grado fornire adeguata performance diagnostica soprattutto per lesclusione della malattia . 
il rapporto costo / bene cio deve tenere conto di molti fattori tra cui il costo biologico ( dose di radiazioni rispetto a test che non necessitano di radiazioni ) , il costo economico ( rispetto a test con costi inferiori ) , la disponibilit territoriale della metodica ( rispetto a metodiche diagnostiche molto pi diffuse ) , lexpertise ( ancora limitato ad alcuni centri )  . limiti dello studio la nostra casistica riporta dati provenienti dal periodo nel quale le soluzioni pi moderne per la riduzione della dose non erano largamente disponibili . 
tuttavia , lintroduzione di nuovi hardware e software in grado di fornire adeguata qualit di immagine utilizzando il triggering prospettico basato sul segnale ecg consentono di portare i valori di dose al di sotto dei 5 msv [ 912 ]  . 
una limitazione dello studio deriva dal design del registro che non offre le stesse caratte1024 radiol med ( 2011 ) 116 : 10141026 the study can be found in the registry design , which does not offer the same characteristics of a trial or a prospective study . 
tuttavia , questa anche la forza delle informazioni presentate in quanto pi realistiche rispetto agli studi convenzionali in condizioni ottimali ( per esempio , pazienti ben selezionati , possibilit di valutazione delle immagini estesa nel tempo , ecc )  . conclusioni conclusions data in our registry demonstrate that ctca is a robust and reliable morphological modality for evaluating obstructive cad in patients with acs and without stemi . 
the intrinsic registry design tends to better re ect clinical practice and its characteristic variability and heterogeneity . i dati del nostro registro dimostrano che la ctca una metodica morfologica per la valutazione dellaterosclerosi coronarica ostruttiva nel contesto della sindrome coronarica acuta senza sopra - elevazione del tratto st robusta ed af dabile . 
grassi1 1sezione di radiologia , dipartimento magrassi - lanzara , seconda universit di napoli , naples , italy 2ii clinica neurologica , seconda universit di napoli , naples , italy 3dipartimento di gerontologia , geriatria e malattie del metabolismo , seconda universit di napoli , naples , italy correspondence to : a . 
in 37 patients , contrast agent transport was preserved and safe ; in 19 , we observed penetration of the contrast agent into the laryngeal inlet without aspiration ; in 24 , there was aspiration ( four preswallowing , eight intraswallowing , nine postswallowing , three mixed ) , whereas in one patient no transit was seen . 
penetration without aspiration was resolved by coughing or throat clearing ; aspiration was resolved in 13 patients by assuming the chin - tuck posture and in six by rotating the head ; in ve patients , it was not resolved . 
in caso di transito alterato , penetrazione o aspirazione del mezzo di contrasto ( mdc ) nelle vie aeree , sono state ipotizzate e veri cate durante lesame vfm posture di compenso per la correzione del disturbo deglutitorio . 
in 37 pazienti il transito del mdc era conservato e sicuro , in 19 abbiamo osservato penetrazione del mdc in aditus laringeo senza aspirazione , in 24 aspirazione ( 4 pre - deglutitoria , 8 intra - deglutitoria , 9 post - deglutitoria , 3 mista ) , in 1 non era presente transito . 
la penetrazione senza aspirazione stata risolta con un colpo di tosse o col raclage sostenuto ; laspirazione stata risolta in 13 pazienti con la postura a capo esso , in 6 col capo ruotato , in 5 non stata risolta . 
la vfm , correlando il dato morfologico a quello funzionale , permette di caratterizzare con precisione il disturbo disfagico ed ipotizzare le posture di compenso pi idonee al singolo caso e veri carne lef cacia . 1084 radiol med ( 2011 ) 116 : 10831094 parole chiave video uoromanometria disfagia posture di compenso sclerosi laterale amiotro ca the dysphagic disorder but also to identify the most appropriate compensation posture for each patient and verify its effectiveness . keywords video uoromanometry dysphagia compensatory postures amyotrophic lateral sclerosis introduction introduzione amyotrophic lateral sclerosis ( als ) , or lou gehrigs disease , is a neurodegenerative disease characterised by progressive muscular paralysis re ecting degeneration of motor neurons in the primary motor cortex , brainstem and spinal cord [ 1 ]  . 
in patients with als , dysphagia is caused by degeneration of bulbar motor neurons and leads to an increased risk of aspiration , weight loss , malnutrition and dehydration the latter being also favoured by upper - limb weakness and greater dif culties in meal preparation [ 3 ]  . the rst clinical manifestations of the disease appear when progressive motor neuron loss exceeds the ability of surviving motor neurons to compensate , thus leading to progressive paralysis , with preservation of the cognitive , sensory , sexual and sphincter functions . 
the prognosis is poor for both forms , leading to death by respiratory failure , aspiration pneumonia or malnourishment and dehydration within 23 years for bulbar and 35 years for spinal als [ 4 ]  . early recognition of dysphagia and , in particular , of the different forms of aspiration into the airways , makes it possible to identify and assume compensation postures to improve swallowing and to make appropriate dietary changes to preserve oral feeding and postpone percutaneous endoscopic gastrostomy ( peg ) as long as possible [ 5 , 6 ]  . 
correct diagnostic assessment of dysphagia in patients with als requires a multidisciplinary approach with close collaboration of the neurologist , the speech therapist , the gastroenterologist and the radiologist [ 7 , 8 ]  . evaluation of swallowing by video uoroscopy ( vfs ) represents the gold standard in patients with neurological disorders and enables accurate analysis of the mechanisms involved in the oral and pharyngeal phases of deglutition [ 911 ]  . 
thanks to the simultaneous acquisition of video uoroscopic and manometric data , video uoromanomla sclerosi laterale amiotro ca ( sla ) o malattia di lou gehrig una malattia neurodegenerativa caratterizzata dalla progressiva paralisi muscolare che ri ette la degenerazione dei neuroni motori della corteccia motoria primaria , del tronco encefalico e del midollo spinale [ 1 ]  . 
let media di insorgenza della sla di circa 60 anni con una leggera prevalenza nel sesso maschile ( maschi : femmine1 , 5 : 1 ) [ 2 ]  . 
 la disfagia , nei pazienti con sla , causata dalla degenerazione dei neuroni motori bulbari e determina un aumento del rischio di aspirazione , perdita di peso , malnutrizione e disidratazione , queste ultime favorite anche dalla severa debolezza degli arti superiori e le conseguenti dif colt nella preparazione dei pasti [ 3 ]  . le prime manifestazioni cliniche della malattia compaiono quando la perdita progressiva dei motoneuroni supera la capacit di compenso dei motoneuroni superstiti no ad arrivare ad una progressiva paralisi , con risparmio delle funzioni cognitive , sensoriali , sessuali e s nteriali . 
in entrambe le forme la prognosi infausta conducendo a morte per insuf cienza respiratoria , polmonite ab ingestis o per un grave stato di denutrizione e disidratazione entro 23 anni per i casi di sla bulbare e 35 anni per i casi di sla spinale [ 4 ]  . riconoscere precocemente il disturbo disfagico e , soprattutto , le diverse tipologie di aspirazione nelle vie aeree , consente di ricercare ed adottare posture di compenso della deglutizione e modi care adeguatamente la dieta al ne di mantenere il pi a lungo possibile lalimentazione orale e ritardare il ricorso alla gastrostomia endoscopica percutanea ( peg ) [ 5 , 6 ]  . 
il corretto inquadramento diagnostico della disfagia nei pazienti con sla necessita di un approccio multidisciplinare con stretta sinergia tra neurologo , logopedista , gastroenterologo e radiologo [ 7 , 8 ]  . lo studio della deglutizione mediante video uoroscopia ( vfs ) rappresenta il gold standard nei pazienti affetti da malattie neurologiche e permette unaccurata analisi dei meccanismi della fase orale e faringea della deglutizione [ 911 ]  . 
limpiego della video uromanometria ( vfm ) , grazie allacquisizione contemporanea dei dati video uoradiol med ( 2011 ) 116 : 10831094 1085 etry ( vfm ) allows for a more precise determination of the causes and effects of the pharyngeal dysfunction [ 12 , 13 ] , which cannot be evaluated by using the two techniques separately [ 12 , 14 ] , and it is particularly useful for treatment planning [ 15 , 16 ]  . in the literature , several compensation postures have been described that facilitate food transit and prevent aspiration . 
the purpose of our study was to verify the effectiveness of compensation postures , suggested on the basis of the type of dysphagia identi ed at vfm examination , in ensuring safe oropharyngeal transit . roscopici e manometrici , consente una pi precisa determinazione delle cause e degli effetti della disfunzione faringea [ 12 , 13 ] , non altrimenti valutabili con le singole indagini di cui si compone [ 12 , 14 ] , ed utile soprattutto per la successiva piani cazione terapeutica [ 15 , 16 ]  . in letteratura sono state descritte posture di compenso atte a favorire il transito alimentare e prevenire laspirazione ; scopo del nostro lavoro veri care lef cacia di tali posture di compenso ipotizzate in base alle caratteristiche del disturbo disfagico individuato con vfm , per garantire il transito orofaringeo in sicurezza . materials and methods materiali e metodi eighty - one consecutive patients with als admitted to the department of neurology from january to december 2008 were included in the study . 
all patients underwent speech therapy evaluation according to the most recent guidelines [ 17 , 18 ] , with assessment of clinical history , feeding status , behavioural features , symptoms and problems reported by patients , morphological and functional evaluation and diagnostic summary . 
for this combined study , the dyno compact system ( men s biomedica s.r.l. , bologna , italy ) was used equipped with : ( 1 ) graphics card for to manage ultrasound or radiographic images ; ( 2 ) avius dedicated software package , which enables digital - quality recording ( pal / ntsc , composite video or s - video ) of the vfs study in avi format with 320 240 resolution and 25 hz acquisition frequency ; the delay introduced by the process of image digitalisation is in the order of 200 ms , so for the purposes of analysis , images can be considered synchronised with the manometric recordings . manometry was performed after positioning a manometry probe with ve - channel endoluminal solid - state microtransducers 2 cm apart and with an angle of 120 90 . 
then , a pull - through was performed by retracting the probe until the last transducer was positioned at the level of the upper esophageal sphincter ( ues ) , three inside the pharynx and the rst at the level of passavants ridge . during data acquisition , video images and manometric traces are visualised in real time , with a sliding cursor showing the exact correspondence between theat the end of the examination , video images are analysed either in real time , at increased or reduced speed or frame by frame . 
tutti i pazienti sono stati sottoposti ad un protocollo di valutazione logopedica in sintonia con le pi recenti linee guida [ 17 , 18 ] , corredato cio da anamnesi , stato alimentare , caratteristiche comportamentali , sintomatologia e dif colt riferite dal paziente , valutazione morfofunzionale e sintesi diagnostica . la vfm prevede lesecuzione contemporanea della vfs con la simultanea registrazione di un tracciato manometrico . 
software dedicato , che registra in qualit digitale ( pal / ntsc , video composito o s - video ) la vfs , in lmati avi con risoluzione 320240 e con frequenza di acquisizione di 25 hz ; il ritardo introdotto dal processo di digitalizzazione dellimmagine dellordine dei 200 ms , quindi , ai ni dellanalisi , limmagine si pu considerare sincronizzata con i tracciati pressori . 
 la manometria stata effettuata dopo il posizionamento di un sondino manometrico con microtrasduttori endoluminali allo stato solido a 5 canali , distanziati 2 cm luno dallaltro e con un angolo di 12090 . 
 successivamente stato eseguito un pull - trough ritirando il sondino no a posizionare lultimo trasduttore a livello dello s ntere esofageo superiore ( ses ) , tre in faringe , il primo a livello del cuscinetto del passavant . durante la fase di acquisizione dei dati i lmati e le tracce manometriche sono visualizzate sullo schermo in tempo - reale : un cursore che scorre su di essi mostra lesatta corrispondenza tra il lmato ed i tracciati . 
gli esami sono stati acquisiti con paziente in ortostatismo , salvo i casi in cui la compromissione della funzione statica dei pazienti ha reso necessaria lacquisizione dellesame in posizione assisa . 
lesame 1086 radiol med ( 2011 ) 116 : 10831094 vfm study began with a baseline , unenhanced acquisition to study vocal cord motility and soft palate ; baseline acquisition was followed by a contrast - enhanced scan to evaluate the entire swallowing act , with special attention being paid to aspiration . 
we administered a single bolus of barium ( a pronto bario hd suspension , bracco spa , milan , italy , 250% w / v ) at a dose ranging from 5 to 15 ml optimised for patient status . 
 in the event of altered bolus transit or of bolus penetration or aspiration into the airways , some manoeuvres to correct the swallowing disorder were hypothesised and tested at vfm . 
although indicated to improve bolus transport in the presence of pharyngeal dysfunction [ 19 ] , praxic alterations in als patients of the oral structures involved in bolus retention and swallowing , in particular the tongue [ 20 ] , preclude the application of this manoeuvre . 
it consists of voluntary manual prolongation of laryngeal excursion during swallowing , which is intended to increase the extent of laryngeal elevation and duration of ues opening , thus favouring a safer transit of the food bolus . 
although its use is recommended in cases of ues dysfunction [ 21 ] , the frequent strength de cit associated with atrophy of the distal upper extremities or severe cramps and muscular damage to the upper limbs prevent its use [ 22 ]  . the supraglottic and super - supraglottic swallows are also not applicable to als patients : the former consists of breath - holding during the entire swallowing act and in producing a cough at the end of the swallowing act before starting the next inspiration ; the latter is a variation of the supraglottic swallow in which full closure of the glottis is achieved by contracting the diaphragm muscles [ 23 ]  . 
thus the corrective techniques used in this study to favour adequate and safe bolus transit were the following : chin - down , or chin - tuck , posture , suggested in patients with dif cult bolus management with possible fall below the tongue base or delayed pharyngeal re ex or with pooling of contrast material inside the pharynx [ 24 ] because of the airway protection provided by changes in pharyngeal dimensions [ 25 ] ; head - rotation posture in the presence of failed / reduced vfm iniziava con una valutazione senza mezzo di contrasto ( mdc ) per lo studio della motilit delle corde vocali e la motilit del palato molle ; poi si procedeva con la fase contrastogra ca che valuta tutto latto deglutitorio con particolare attenzione allaspirazione . 
abbiamo somministrato una dose singola di mdc baritato ( una sospensione di prontobario hd , bracco spa , milano ; 250% p / v ) , la cui quantit compresa tra 5 e 15 ml stata ottimizzata in base al paziente . 
 in caso di transito alterato del mdc , di penetrazione o di aspirazione dello stesso nelle vie aeree , sono state ipotizzate e veri cate durante lesame vfm metodiche rimediative per la correzione del disturbo deglutitorio . 
tra le manovre di compenso descritte in letteratura alcune non sono direttamente utilizzabili in caso di sla : la manovra di deglutizione forzata , che consiste nella spinta forzata e prolungata della lingua contro il palato durante latto deglutitorio , indicata per migliorare il trasporto del bolo , in presenza di disfunzioni faringee [ 19 ] , ma non applicabile in questi pazienti perch le alterazioni prassiche delle strutture orali preposte al contenimento e alla deglutizione del bolo , in maggioranza riferibili al distretto linguale [ 20 ] , non consentono di mettere in atto tale manovra . 
anche la manovra di mendelsohn non utilizzabile dai soggetti affetti da sla : consiste nel volontario prolungamento manuale dellelevazione laringea durante la deglutizione che porta ad aumento dellestensione dellelevazione laringea e della durata dellapertura del ses , favorendo un pi sicuro transito del bolo alimentare ; consigliata nei casi di disfunzione dello ses [ 21 ] , ma i frequenti de cit di forza associata ad atro a delle estremit distali superiori , o crampi e danni muscolari severi degli arti superiori ne impediscono lutilizzo [ 22 ]  . non trovano applicazione nei pazienti con sla anche le manovre di deglutizione sopraglottica e supersopraglottica : la prima consiste nel mantenere lapnea durante tutta la deglutizione ed effettuare un colpo di tosse a conclusione dellatto deglutitorio , prima della successiva inspirazione ; la seconda una variante della prima , nella quale si richiede una piena chiusura s nterica della glottide attraverso la contrazione dei muscoli diaframmatici [ 23 ] ; entrambe richiedono un breve training per la loro precisa messa in atto e vengono impiegate nei casi di disfagia secondaria a chirurgia del distretto laringeo . 
in questo studio , pertanto , le ipotesi rimediative impiegate per favorire un transito adeguato del mdc ed in sicurezza sono state : la postura del capo esso , o chin down o chin tuck , suggerita nei casi di dif colt nella gestione del bolo con possibile caduta al basi - lingua o di ritardo nellelicitazione del ri esso faringeo di deglutizione , o di ristagni di mdc in faringe [ 24 ] , per leffetto di protezione fornito alle vie aeree in relazione ai cambiamenti delle dimensioni faringee [ 25 ] ; radiol med ( 2011 ) 116 : 10831094 1087 ues opening , as this produces a fall in ues pressure and delays its closure during the swallowing act [ 26 ] ; hyperextended head posture , which facilitates bolus transit by exploiting gravity ; it is indicated in cases of reduced pharyngeal peristalsis [ 5 ]  . 
 la postura del capo ruotato in presenza di mancata / ridotta apertura del ses , poich produce la caduta pressoria del ses e ne ritarda la chiusura durante latto deglutitorio [ 26 ] ; la postura del capo in iperestensione che facilita il passaggio del bolo sfruttando la forza di gravit ed indicata nei casi di ridotta peristalsi faringea [ 5 ]  . 
 results clinical history and morphological and functional speech therapy assessment risultati of the 81 patients undergoing clinical history speech therapy assessment , 14 ( 17.5% ) reported no swallowing disorders and 67 ( 82% ) reported dysphagia . 
of the six patients with dysphagia for solid food , one showed alterations only during the oral phase of swallowing and ve only during the pharyngeal phase ; the 11 patients with dysphagia for liquids only reported a sensation of liquid bolus going down the wrong way . risultati dellanamnesi e della valutazione morfofunzionale logopedica degli 81 pazienti sottoposti allanamnesi logopedia , 14 ( 17 , 5% ) non riferivano disturbi della deglutizione e 67 ( 82% ) disfagia . 
tra questi ultimi , 6 ( 9% ) presentavano disfagia per solidi , 11 ( 15% ) disfagia per liquidi , e 50 ( 75 , 7% ) riferivano disturbi nella deglutizione di entrambe le consistenze . 
tra i 6 casi di disfagia per solo bolo solido , 1 caso presentava alterazione della sola fase buccale e 5 della sola fase faringea ; gli 11 pazienti che presentavano disfagia per i soli liquidi lamentavano la sensazione del bolo liquido che va di traverso . vfm examination risultati dellesame vfm in 37 of the 81 patients studied , contrast agent transit was preserved and safe . 
in 19 cases ( 23% ) , we observed bolus penetration into the laryngeal lumen only , without aspiration below the glottic level , whereas in 24 ( 34% ) , aspiration was observed . 
of the 39 patients with suspected aspiration at speech therapy assessment , 18 were con rmed at vfm , 13 presented with penetration without aspiration and eight were false positives . 
 vfm showed that in the 24 patients with aspiration , this occurred in the preswallowing phase in four ( 17% ) cases , in the intraswallowing phase in eight ( 30% ) and in the postswallowing phase in nine ( 39% ) ; multiple swallowing disorders were seen in three ( 13% ) , with the concurrent presence of several types of aspiration , which we de ned as mixed aspiration . 
 intraswallowing aspiration was related to pharyngeal hypertonicity in 7 / 8 cases ( 87% ) , accompanied by reduced laryngeal elevation and / or closure in three patients and in four cases by ues dysfunction ; the latter was observed degli 81 pazienti in esame , in 37 il transito del mdc era conservato e sicuro . 
in 19 casi ( 23% ) si osservata la sola penetrazione del mdc nel lume laringeo senza aspirazione dello stesso al di sotto del piano glottico ed in 24 ( 34% ) aspirazione ; tra questi , 6 ( 25% ) non presentavano ri esso tussigeno spontaneo . 
dei 39 soggetti con sospetto di aspirazione alla valutazione logopedica , in 18 stata confermata alla vfm , 13 presentavano penetrazione senza aspirazione e 8 sono risultati dei falsi positivi . alla vfm , nei 24 pazienti con aspirazione , in 4 ( 17% ) si evidenziata aspirazione pre - deglutitoria , in 8 ( 30% ) intradeglutitoria , in 9 ( 39% ) post - deglutitoria ed in 3 ( 13% ) erano evidenti disturbi multipli della deglutizione associati alla presenza contemporanea di diverse tipologie di aspirazione , che per comodit di esposizione abbiamo de nito aspirazione mista . 
laspirazione intra - deglutitoria in 7 casi su 8 ( 87% ) avvenuta in relazione ad ipertono faringeo , accompagnato in 3 soggetti , da ridotta elevazione e / o chiusura laringea e , in 4 casi , da disturbi dello ses ; questi ultimi si sono manifestati in 1 caso con chiusure anticipate e nei restanti 3 con rilasciamenti incompleti . 
study population : january - december 2008 ( 81 patients ) chin tuck compensation postures no compensation head rotation head hyperextension preserved and safe transit penetration without aspiration preswallowing aspiration intraswallowing aspiration postswallowing aspiration mixed aspiration no transit total transito conservato e sicuro penetrazione senza aspirazione aspirazione pre - deglutitoria aspirazione intra - deglutitoria aspirazione post - deglutitoria mista assenza di transito totale 81 tabella 1 correlazione tra disturbo disfagico valutato alla vfm ed ef cacia delle posture di compenso . 
casistica personale : gennaio - dicembre 2008 ( 81 pazienti ) capo esso posture di compenso non compenso capo ruotato capo iperesteso in one case with premature closure and in the remaining three cases with incomplete release . 
in the nine cases of postswallowing aspiration , the bolus was inhaled following contrast - agent pooling inside the pharynx : in two cases , this occurred at the level of the pyriform sinuses , in two at the level of the epiglottic valleculae and in ve at both levels . 
in one patient , the problem was not solved . mixed aspiration was seen in one bedridden patient with hyperextended head and unable to change posture and in two with multiple dysfunctions of the different swallowing phases associated with severe oropharyngeal incoordination . 
nei 9 casi di aspirazione post - deglutitoria il bolo stato inalato in seguito a ristagno di mdc in faringe : in 2 casi si apprezzava a livello dei seni piriformi , in 2 a livello delle vallecole glosso - epiglottiche e in 5 a livello di entrambe le sedi . 
dal punto di vista manometrico in 1 paziente era presente rilasciamento incompleto e in 2 ipotono dello ses , in 2 pazienti era presente ipertono dello ses , negli altri 4 non erano presenti alterazioni . 
 there are 5 endoluminal microtransducers , 2 cm apart from each other , the rst is located at the level of passavants ridge , three inside the pharynx , the last at the level of the upper esophageal sphincter ( ues )  . 
sono presenti 5 microtrasduttori endoluminali , distanziati 2 cm luno dallaltro , il primo posizionato a livello del cuscinetto del passavant , tre in faringe , lultimo a livello dello s ntere esofageo superiore ( ses )  . 
 the second part of the vfm examination , in which the compensatory postures were applied , led to several considerations : in the case of preswallowing aspiration , generally resulting from abnormalities of the oral and propulsive phases , we agree with previous reports that suggest that i risultati dimostrano che i de cit deglutitori in pazienti affetti da sla sono diversi per meccanismo compromesso , in relazione alle caratteristiche della patologia e del decorso . 
la seconda parte dellesame vfm , dove si resa necessaria lapplicazione delle posture di compenso , ha prodotto levidenza di varie considerazioni : nei casi di aspirazione pre - deglutitoria , in genere provocate da alterazioni delle fasi buccali e propulsive , concordiamo con la letteratura per lopportunit di impiegare la postura di compenso del capo esso , che ha radiol med ( 2011 ) 116 : 10831094 1090 fig . 
la base della lingua copre laditus laringeo prevenendo la penetrazione del mdc in laringe . the chin - tuck posture is appropriate , as this resolved the problem in 100% of cases ; in cases of intraswallowing aspiration , the chin - tuck position was effective in patients with reduced laryngeal elevation / closure only , in whom it eliminated aspiration in all cases . 
conversely , head rotation can be more rationally suggested in case of intraswallowing aspiration secondary to cricopharyngeal dysfunction , as it reduces ues tone and delays closure [ 26 ]  . 
in the last case , no satisfactory result was obtained , possibly due to massive intraswallowing aspiration ; postswallowing aspiration occurred in nine patients as a result of penetration into the laryngeal vestibule and pooling inside the epiglottic valleculae and / or the pyriform sinuses . 
five patients bene ted from the chintuck posture [ 24 ] , two of whom had hypotonic ues ; in consentito la risoluzione del disturbo nel 100% dei casi ; nei casi di aspirazione intra - deglutitoria la postura del capo esso si dimostrata ef cace solo in quei soggetti che presentavano ridotta elevazione / chiusura laringea ; ci ha consentito di risolvere laspirazione in tutti i casi che presentavano questo disturbo . 
il suggerimento di rotazione del capo trova , viceversa , unapplicazione pi razionale nei casi di aspirazione intradeglutitoria secondaria a disfunzioni cricofaringee , consigliata per ridurre il tono dello ses e ritardarne la chiusura [ 26 ]  . 
nellultimo caso non si sono ottenuti risultati soddisfacenti presumibilmente per la massiccia aspirazione intradeglutitoria presentata dal paziente ; laspirazione post - deglutitoria nei 9 pazienti si vericata in correlazione a penetrazione nel vestibolo laringeo e stasi nelle vallecole glosso epiglottiche e / o nei seni piriformi . 
il transito avviene senza aspirazione nonostante il passaggio del bolo in faringe non innescchi la peristalsi . contrast , the patient with incomplete release and the two patients with hypertonic ues bene ted from head rotation [ 26 ]  . 
there was no improvement in one case only as a result of massive inhalation of contrast material into the airways ; patients with mixed aspiration were at an advanced stage of disease , with swallowing incoordination and poor cooperation ; in one case only was aspiration reduced with the chin - tuck posture . 
for these patients , compensation postures are known to be of limited bene t [ 27 ] ; in cases of severe swallowing alterations owing to absent lingual pump , the hyperextended head position restored bolus transport [ 5 ] , and vfm validated its safety : although bolus passage failed to trigger the swallowing re ex and pharyngeal peristalsis was uncoordinated with bolus passage , the patient showed no aspiration . postura a capo esso [ 24 ] , tra questi i 2 con ipotono dello ses ; il paziente con rilasciamento incompleto ed i 2 pazienti con ipertono dello ses hanno invece bene ciato del capo ruotato [ 26 ]  . 
non abbiamo ottenuto alcun miglioramento in 1 solo caso in relazione ad inalazione massiva del mdc nelle vie aeree ; i pazienti con aspirazione mista presentavano uno stadio avanzato di patologia con incoordinazione deglutitoria e scarsa collaborazione ; solo in 1 abbiamo ottenuto una riduzione dellaspirazione con capo esso . 
per questi soggetti il bene cio delle metodiche rimediative noto essere molto ridotto [ 27 ] ; nel caso di grave alterazione dellatto deglutitorio per assenza della pompa linguale , la postura del capo in iperestensione ha consentito di ripristinare il transito del mdc [ 5 ] e la vfm ha permesso di veri carne la sicurezza : nonostante il passaggio del bolo non inneschi il ri esso deglutitorio e la peristalsi faringea fosse incoordinata rispetto al passaggio del bolo il soggetto non 1092 radiol med ( 2011 ) 116 : 10831094 separate mention must be made of silent aspiration and penetration without aspiration . 
silent aspiration refers to the passage of ingested material below the vocal cords in the absence of protective cough , and it is estimated to occur in about half of the patients with aspiration [ 28 ]  . 
 in our patient population , it occurred in six cases , that is , in 25% of patients with aspiration three of them with intraand three with postswallowing aspiration with no apparent correlation explaining the absence of protective cough . 
this phenomenon should not be underestimated [ 29 ] owing to the possible associated complications : aspiration pneumonia is three times more frequent in dysphagic than in nondysphagic individuals [ 30 ] and represents the most common cause of death in patients with neurological diseases associated with dysphagia [ 31 ]  . in our series , penetration of contrast material into the laryngeal vestibule occurred in 19 patients ( 23% ) , whereas in the healthy population aged > 50 years , bolus passage into the larynx occurs in 16.8% of swallows [ 32 ]  . 
in patients with als , the need to move the material away from the laryngeal vestibule arises from the consideration that the material may be directly inhaled into the airways at the end of the swallowing act , in particular in the case of deep penetration . 
 conclusions the variety of dysphagic disorders observed in our population of patients with als con rms the need for a complete and individual evaluation allowing identi cation of compensation strategies . 
this type of workup , which involves the collaboration of several different healthcare professionals ( neurologist , speech and language therapist , gastroenterologist , radiologist ) , facilitates the diagnosis and promotes appropriate management according to the needs of the individual patient , taking into consideration that the main feature of als rehabilitation is represented by remediation rather than rehabilitation programmes . in our population of als patients , the alterations observed required only three possible compensation postures : chin tuck , head rotation , and hyperextended head . 
the chin - tuck posture proved useful in the majority of cases , given that it offers a valuable protection mechanism for the airways by opening the valleculae and preventing penetration into the larynx ; above all , with this posture , the tongue base narrows and covers the laryngeal inlet . 
head rotation is indicated in the case of hypertonicity , incomplete release or premature ues closure , as it reduces the resting pressure of the sphincter and presentava aspirazione . due menzioni a parte meritano i fenomeni dellaspirazione silente e della penetrazione senza aspirazione . 
per aspirazione silente si intende il passaggio degli ingesti al di sotto delle corde vocali in assenza di tosse protettiva e si stima intorno alla met dei pazienti con aspirazione [ 28 ] ; nella nostra casistica esso riguarda 6 casi , ossia il 25% dei pazienti che presentavano aspirazione , 3 con aspirazione intrae 3 post - deglutitoria , senza alcuna apparente correlazione che giusti casse lassenza del ri esso tussigeno . 
 questo fenomeno un evento da non sottovalutare [ 29 ] per le possibili complicanze ad esso associate : la polmonite ab ingestis tre volte pi frequente nei soggetti disfagici rispetto ai non disfagici [ 30 ] e rappresenta la pi comune causa di morte nei pazienti con patologie neurologiche associate a disfagia [ 31 ]  . la sola penetrazione del mdc nel vestibolo laringeo nella nostra casistica si veri cata in 19 soggetti ( 23% ) mentre nella popolazione sana con pi di 50 anni , il passaggio del bolo in laringe avviene nel 16 , 8% delle deglutizioni [ 32 ]  . 
 nei pazienti con sla , la necessit di allontanare il materiale dal vestibolo laringeo nasce dalla considerazione che questultimo potr essere aspirato direttamente nelle vie aeree a conclusione dellatto deglutitorio , soprattutto se la penetrazione stata profonda . 
 conclusioni la variet di disturbi disfagici rilevati nella nostra casistica , nei pazienti con sla , ci induce a confermare la necessit di una valutazione individuale e completa , che risponda a requisiti di studio e suggerimenti rimediativi . 
 un percorso cos codi cato , integrato da pi professionalit ( neurologo , logopedista , gastrenterologo , radiologo ) , consente di promuovere una diagnosi e una gestione opportuna in base alle speci cit rilevate , tenendo conto che la principale caratteristica dellassetto riabilitativo nella sla rappresentata dalla metodologia strettamente rimediativa e non riabilitativa . nella sla le alterazioni riscontrate nella nostra casistica hanno condotto a sole 3 le posture di compenso possibili : il capo esso , il capo ruotato e il capo in iperestensione . 
la postura del capo esso si dimostrata utile nella maggior parte dei casi in quanto rappresenta un valido meccanismo di protezione delle vie aeree determinando lampliamento delle vallecole e prevenendo la penetrazione in laringe , ma soprattutto restringe e copre con la base della lingua laditus laringeo . 
la postura del capo ruotato indicata nei casi di ipertonia , rilasciamenti incompleti o chiusure anticipate del ses poich riduce la pressione a riposo dello radiol med ( 2011 ) 116 : 10831094 1093 increases its opening time by moving the cricoid cartilage away from the posterior pharyngeal wall . 
lastly , in the case of penetration without contrast agent aspiration into the laryngeal inlet , we suggest throat clearing every three to four swallowing acts to prevent possible postswallowing inhalation . in conclusion , because vfm enables identi cation and interpretation of alterations underlying swallowing disorders through correlation of morphological and functional data , it can help characterise dysphagic disorders , suggest the most suitable compensation posture for each patient and validate the effectiveness of such postures . s ntere e ne aumenta il tempo di apertura grazie allallontanamento della cartilagine cricoide dalla parete faringea posteriore ; la postura del capo in iperestensione indicata nei casi di assenza della pompa linguale solo se si dimostra che il transito avviene in modo sicuro . 
in ne , nei casi di penetrazione senza aspirazione del mdc in aditus laringeo riteniamo necessario suggerire un raclage sostenuto ogni 34 atti deglutitori , per evitare la possibilit di inalazione post - deglutitoria . 
guglielmi6 , 7 1human nutrition and physiology unit , university of rome tor vergata , via montpellier 1 , 00173 rome , italy 2imaging division , clinical department of radiological and histocytopathological sciences , university of bologna , santorsolamalpighi hospital , via massarenti 9 , 40138 bologna , italy 3department of orthopaedics and traumatology , university hospital policlinico tor vergata , viale oxford 81 , 00133 rome , italy 4endocrinology department , university hospital policlinico tor vergata , viale oxford 81 , 00133 rome , italy 5institute of medical informatics and biometry , university tor vergata , rome , italy 6department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 7department of radiology , hospital san giovanni rotondo , 71013 san giovanni rotondo , italy correspondence to : a . 
the knowledge of factors modulating the behaviour of bone mass is crucial for preventing and treating osteoporotic disease ; among these factors , body weight ( bw ) has been shown to be of primary importance in postmenopausal women . 
 our aim was to analyze the relationship between body mass index ( bmi ) , fat and lean mass and bone mineral density ( bmd ) in a large population of women . 
between 2005 and 2008 , weight and height of 6 , 249 italian women ( aged 3080 years ) were measured and bmi was calculated ; furthermore bmd , bone mineral content , fat and lean mass were measured by dual - energy x - ray absorptiometry . 
la conoscenza dei fattori che modulano il comportamento della massa ossea cruciale nella prevenzione e nel trattamento della malattia osteoporotica ; tra questi fattori , il peso corporeo ( bw ) ha dimostrato di essere di primaria importanza nelle donne in postmenopausa . 
il nostro obiettivo stato quello di analizzare la relazione tra lindice di massa corporea ( bmi ) , la massa grassa , la massa magra e la densit minerale ossea ( bmd ) in una vasta popolazione di donne . 
nel periodo compreso tra il 2005 e il 2008 sono stati rilevati peso e altezza di 6249 donne italiane ( et 4080 anni ) , ed stato calcolato il bmi ; inoltre sono stati misurati bmd , contenuto minerale osseo , massa grassa e massa magra attraverso assorbimetria a raggi x a doppia energia . 
an overall examination of our results suggests that both fat and lean body mass can in uence bone mass and that their relative effect on bone could be modulated by their absolute amount and ratio to total bw . 
unanalisi generale dei nostri risultati suggerisce quindi che sia la massa grassa sia la massa magra possono in uenzare la massa ossea e che gli effetti relativi sullosso possono essere modulati dalla loro quantit assoluta e dal rapporto sul peso corporeo complessivo . parole chiave osteoporosi composizione corporea indice di massa corporea densit minerale ossea densitometria ossea a raggi x a doppia energia fotone introduction introduzione osteoporosis is becoming increasingly prevalent with the aging of the world population . 
bmi is inversely related with the risk of osteoporotic hip fracture [ 3 ] , although its relationship with other limb fragility fractures is still debated [ 5 ]  . 
recently suggested that there are no bmi categories that protect against these fragility fractures compared with that of normal bw after adjusting for bone mineral density ( bmd ) and age [ 6 ]  . 
showed that traumatic forces increase with bw , but fracture rates at the hip and central body were less frequent with increasing a causa del progressivo invecchiamento della popolazione mondiale , losteoporosi sta diventando una patologia sempre pi diffusa e rappresenta un grave problema di sanit pubblica associata ad un incremento della mortalit e della morbilit [ 1 ]  . 
 lo studio epidemiologico sulla prevalenza dellosteoporosi in italia ha mostrato che la prevalenza allet di 60 anni al di sopra del 22 , 8% e del 14 , 5% , rispettivamente nelle donne e negli uomini ed responsabile di circa 80.000 nuove fratture ogni anno [ 2 ]  . 
 stata , inoltre , riscontrata una relazione tra le fratture osteoporotiche e lindice di massa corporea ( bmi ) , parametro biometrico espresso come rapporto tra peso ( body weight , bw ) e altezza [ 3 , 4 ]  . 
lindice di massa corporea risultato inversamente proporzionale al rischio di frattura osteoporotica del collo del femore [ 3 ] , anche se ancora oggetto di dibattito leventuale correlazione con altre fratture da fragilit degli arti [ 5 ]  . 
 [ 6 ] hanno recentemente suggerito che , dopo correzione per et e densit minerale ossea ( bone mineral density , bmd ) , non radiol med ( 2011 ) 116 : 11151123 1117 bmi , possibly due to greater soft - tissue padding . 
upper - extremity fractures showed no variation with bmi , and lower - extremity fracture rates were higher only in the overweight population ( bmi 2529.9 kg / m2 ) [ 7 ]  . several changes in body composition may occur with ageing , including reduced fat - free tissue mass and increased fat mass , leading to a higher percentage of body fat at any given bw in older adults . 
however , predictive methods have a relatively large error at an individual level , and thus , if individuals must be classi ed into categories , misclassi cation can occur . 
this study also represents a rst important report on reference standard values for body composition in italian women . materials and methods study participants in a cross - section study , we retrospectively analyzed data of 6 , 249 italian women ranging in age from 30 to 80 years who participated in ongoing studies on body composition and / or energy metabolism at our university from 2005 to mid - 2008 . 
participants were categorised in bmi groups according to world health organisation ( who ) criteria : normal weight , bmi < 24.9 kg / m2 ; overweight , bmi > 25 < 29.9 kg / m2 ; obesity , bmi > 30 kg / m2 . 
in addition , they were classi ed into categories according to body fat percentage ( bf% ) : normal bf% , < 35% in women ; high bf > 35% in women ; very high bf% , > 40% in women . 
 [ 7 ] hanno dimostrato che le forze traumatiche incrementano con laumentare del peso corporeo , ma la percentuale di fratture del rachide e del collo femorale risulta inferiore , probabilmente a causa dellaumento del tessuto adiposo . 
 le fratture alle estremit superiori non hanno evidenziato variazioni rispetto al bmi , mentre le percentuali di fratture alle estremit inferiori sono risultate maggiori solo nei soggetti in sovrappeso ( bmi 2529 , 9 kg / m2 ) [ 7 ]  . linvecchiamento pu comportare molteplici cambiamenti nella composizione corporea ( body composition , bc ) , in particolare pu veri carsi una riduzione della quota di massa magra e un incremento di quella grassa . 
comunque , i metodi predittivi hanno un errore relativamente ampio a livello individuale perci , se i soggetti devono essere inseriti in categorie , pu veri carsi unerrata classi cazione . lo scopo di questo studio stato sia quello di valutare la relazione tra bmi , bc e bmd sia quello di determinare la prevalenza dellosteopenia e dellosteoporosi nella popolazione femminile italiana . 
questo studio rappresenta anche il primo importante contributo scienti co relativo ai valori standard di riferimento per la composizione corporea delle donne italiane . materiali e metodi soggetti in questo studio trasversale abbiamo analizzato retrospettivamente i dati di 6249 donne italiane di et compresa tra 30 e 80 anni . 
the scanner was calibrated daily against the standard calibration block supplied by the manufacturer to control for possible baseline dri dxa measured total bmd and bmc with a precision ( coef cient of variation ) of 0.7%. 
 the diagnosis of osteoporosis was done according to t - score values and diagnosis by who as showed in table 1 . statistical analysis all data analysis was performed using the statistical package for the social sciences windows , version 15.0 ( spss , chicago , il , usa )  . 
i soggetti sono stati inseriti in gruppi di bmi , secondo i criteri dellorganizzazione mondiale della sanit ( who ) : peso normale , bmi < 24 , 9 kg / m2 ; sovrappeso , 25 < bmi < 29 , 9 kg / m2 ; obesit , bmi > 30 kg / m2 . 
inoltre sono stati classi cati in categorie secondo la percentuale di grasso corporeo ( body fat , bf ) nel sesso femminile ( normale bf% , < 35% ; elevata bf% , > 35% ; molto elevata bf% , > 40% )  . 
secondo i criteri who lobesit nei soggetti giovani e di mezza et corrisponde a valori percentuali di bf superiori al 35% nelle donne [ 8 ]  . bmd , contenuto minerale osseo e misurazioni della composizione corporea le misurazioni del bmd , del contenuto minerale osseo ( bmc ) , della massa grassa e di quella magra sono state effettuate in tutte le sedi corporee , utilizzando la tecnica assorbimetrica a raggi x a doppia energia ( dxa , hologic qdr 4500a , hologic inc . , waltham , ma , usa )  . 
la diagnosi di osteoporosi stata effettuata secondo i criteri ed i valori di t - score della who espressi in tabella 1 . analisi statistica lanalisi di tutti i dati stata ottenuta utilizzando il programma statistico social science windows versione 15.0 ( spss , chicago , il , usa )  . 
 le differenze tra le decadi di et per tutte le variabili sono state calcolate usando unanalisi della varianza ( anova ) a una variabile ( one - way ) e la comparazione multipla del test bonferroni . 
vi stato un incremento del bmi in relazione allet , in particolare stato osservato un signi cativo aumento dellobesit ( p < 0 , 001 ) dalla classe 3 di et ( 5059 anni ) alla classe 5 ( 7080 anni )  . 
hence , it clearly appears to be important to determine standard references for body composition values , especially with techniques that will play a prominent role in the next clinical generation . 
the collection and analysis of references for body composition in men and women will be dif cult , as differences in fat mass and lean mass may be marked between countries and populaquanto sia cruciale acquisire dei dati normali di riferimento sulla bmd considerando le varie tecniche utilizzate nella diagnosi della malattia . 
infatti , sono stati raccolti valori standard di riferimento per la dxa , ma anche per la quantitative computed tomography ( qct ) e per la peripheralqct ( pqct ) [ 911 ] ; risaputo quanto questi valori siano essenziali per lapplicazione dei metodi di imaging nella diagnosi delle malattie del metabolismo osseo . 
di conseguenza appare importante determinare gli standard di riferimento per i valori di bc , specialmente per le tecniche che acquisiranno un ruolo prominente nella pratica clinica in un prossimo futuro . 
la raccolta e lanalisi dei dati di riferimento per la bc nei maschi e nelle femmine sar un compito dif cile a causa delle differenze nella massa grassa e muscolare riscontrabili tra paesi e popolazioni differenti tra loro . 
therefore , a national normative database is de nitely necessary on a country basis to provide the speci c phenotype of the population in whole - body dxa analysis of body composition . 
 some authors have performed research on the relationships between bone mass and bw or bmi [ 13 , 14 ] and between bone mass and nonbone mass [ 1517 ]  . 
 the social problem of obesity is becoming better understood , but the endocrine function and the role of adipose tissue is still one of the main subjects of study and debate . 
 hence , body composition analysis may provide an important contribution to understanding how fat is fat and the function and physiopathology of adipose tissue [ 18 , 19 ]  . 
an overall examination of our results therefore suggests that both fat and lean body mass can in uence bone mass and that their relative effect on bone could be modulated by their absolute amount and ratio to total body mass weight . 
an important building block in the reference values of body composition by dxa in italian women has now been laid . per fornire il fenotipo speci co della popolazione in base allanalisi whole - body della bc ottenuta con dxa . al giorno doggi , alcuni autori hanno pubblicato ricerche sulle relazioni tra tessuto osseo e bw o bmi [ 13 , 14 ] , e tra tessuto osseo e parti molli [ 1517 ]  . 
sar una s da prevedere correlazioni signi cative tra i valori di bc e i rischi o i fattori prognostici per un ampio spettro di malattie . il problema sociale dellobesit sta diventando man mano sempre pi conosciuto , ma la funzione endocrina e il ruolo del tessuto adiposo sono ancora oggetto di studio e di dibattito . 
quindi , la bc pu fornire un contributo importante per capire la percentuale di massa grassa , la funzione e la siopatologia del tessuto adiposo [ 18 , 19 ]  . 
una valutazione complessiva dei nostri risultati suggerisce , pertanto , che sia la massa grassa che quella muscolare possono in uenzare il tessuto osseo , e che il loro effetto sul tessuto osseo potrebbe essere modulato dalla loro somma e dalla percentuale rispetto al peso della massa corporea . 
improperly taken x - rays do not help at all in providing clues for a proper diagnosis . this said , a misdiagnosis today could have serious consequences in the short term ; the same child could be referred not long after with more severe lesions , even fatal ones . the book is divided into two sections : section a ( image reproduction , display and interpretation in child abuse ) addresses in one chapter what is de ned as evidence - based radiology in child abuse ; section b ( skeletal injuries in child abuse ) is divided into ve sub - sections addressing axial skeleton ( 3 chapters ) , appendicular skeleton and viscera ( 3 chapters ) , differential diagnoses ( 2 chapters ) , dating fractures ( 1 chapter ) , examples ( 1 chapter ) and ends with the reference list . in section a , evidence - based radiology in child abuse , the reader will nd a great deal of information on : background ; imaging ; skeletal survey ; bone scans and the pitfalls of radionuclide bone scans ; computed tomography ( ct ) scans ; ultrasound ( us ) / magnetic resonance imaging ( mri ) ; post - mortem investigations ; computed / digital vs . 
 il volume ora in discussione , concepito come un atlante di immagini radiologiche raccolte in un ampio arco di tempo , aggiunge ulteriori informazioni ed aiuta nellinterpretazione di tale tipo di immagini . 
le autrici pongono laccento sullimportanza e sulla qualit delle immagini stesse per poter porre una diagnosi adeguata : radiogrammi ripresi in modo improprio non aiutano affatto nelloffrire elementi signi cativi per una diagnosi corretta . detto questo , una diagnosi non corretta oggi , potrebbe avere serie conseguenze nel breve periodo : lo stesso bambino potrebbe infatti essere rivisto dopo non molto tempo con lesioni ancora pi importanti , anche mortali . il volume diviso in due parti : la parte a ( riproduzione delle immagini , presentazione ed interpretazione nellabuso del bambino ) tratta in un solo capitolo quella che de nita radiologia basata sulle prove nellabuso del bambino ; la parte b ( lesioni scheletriche nellabuso ) divisa in cinque sottosezioni che trattano rispettivamente : lo scheletro assiale ( 3 capitoli ) , lo scheletro delle appendici ed i visceri ( 3 capitoli ) , diagnosi differenziali ( 2 capitoli ) , et delle fratture ( 1 capitolo ) , esempi ( 1 capitolo ) e termina con i riferimenti bibliogra ci . nella parte a , radiologia basata sullevidenza nellabuso del bambino , il lettore trover un numero cospicuo di informazioni sul problema di base , il ruolo delle immagini , lo studio dello scheletro , le immagini con scintigra a ossea ed i possibili errori della stessa , la tomogra a computerizzata ( tc ) , lecogra a e la risonanza magnetica ( rm ) , le indagini post - mortem , le immagini della radiologia computerizzata / digitale a fronte di quelle della analogica , le lesioni caratteristiche ( lesioni delle parti molli , fratture meta sarie , dia sarie , del cranio e delle coste , neo - formazione di osso subperiostale , fratture poco comuni e di alta speci cit per abuso ) , la datazione radiologica delle fratture , la diagnosi differenziale e un sommario . 
 1152 radiol med ( 2011 ) 116 : 11511152 in section b , each chapter opens with a few pages of detailed description of fractures affecting the addressed body part ; how and what sort of force is needed to account for the fracture in discussion , its pattern , healing , dating , effects and differential diagnosis . each table exemplifying a fracture presents a key box detailing , according to the type of fracture : age of fracture , degree of force , mechanism , height of fall , general prevalence , prevalence in child abuse and speci city in child abuse , plus a few lines of comment on important clinical or technical rule - of - thumb points . 
this is a pure x - ray lm atlas : where you will encounter the diagnostic dif culties and dilemmas linked to some images , most of all in rib fracture identi cation . 
 going through the chapters , the reader will learn quite a lot , looking at the images , taking into account the very important chapter on the normal variants and pathological conditions as well as the suggestion to repeat the examination at a 14 day interval looking for bone callus to properly assert the presence of a doubtful or suspected fracture improperly x - rayed the rst time . 
 the same can be said about the case examples chapter , a review of some of the cases sent to the authors for their expert opinion : here you can and will realise how poor quality or improper x - ray lm positioning can be the source of dilemma or incorrect diagnoses . 
here the reader will face some questions : what do you think about the images ? how would you report them ? this review can be closed by a few words written by the authors in their preface to the book : which is the lesser error to make a wrongful diagnosis of physical abuse thus removing one infant from loving carers , or to miss the diagnosis and return a baby to an environment in which episodes of abuse may escalate , culminating in that babys death ? both scenarios are distinct possibilities ; the dif culty with making the diagnosis of abuse ( particularly in non - lethal cases ) is that no external gold - standard exists . this book is to be praised and strongly recommended to radiologists ( a copy should be available in all emergency departments ) , orthopaedics , paediatricians and legal medicine physicians . 
 nella parte b , ciascun capitolo si apre con alcune pagine di descrizione dettagliata delle fratture che interessano la regione del corpo di riferimento , come e che tipo di forza sia necessaria per determinare la frattura in discussione , il suo aspetto , la sua guarigione , la sua datazione , le sue conseguenze , per terminare con la diagnosi differenziale . ciascuna presentazione di un esempio di frattura preceduta da una tabella che riporta nei dettagli , a seconda del tipo della frattura , i seguenti dati : et della frattura , entit della forza , meccanismo , altezza della caduta , prevalenza generale della frattura e sua prevalenza e speci cit nellabuso ; dati accompagnati da alcune brevi righe di commento su importanti aspetti clinici o concetti tecnici da non dimenticare . il lettore deve considerare che solo alcune immagini tc e nessuna rm o ecogra a sono presenti o descritte : il volume in questione un puro atlante di immagini radiologiche tradizionali in cui trover le dif colt ed i dilemmi sollevati da alcune immagini , in particolare nellidenti cazione delle fratture costali . nellesaminare i vari capitoli il lettore avr molto da imparare , valutando le immagini , prendendo nella giusta considerazione lassai importante capitolo sulle varianti del normale e su varie condizioni patologiche , nonch tenendo in giusto conto il suggerimento di ripetere le immagini a distanza di 14 giorni alla ricerca della presenza del callo osseo , per sostenere correttamente la presenza di una frattura dubbia o sospetta , riprodotta incorrettamente alla prima indagine . analogo discorso riguarda il capitolo sugli esempi tratti dalla casistisca , una carrellata di alcuni dei casi inviati alle autrici per consulenza specialistica esperta : in queste pagine il lettore pu e si render conto di quanto la scarsa qualit o la non corretta posizione nella ripresa dei radiogrammi possa essere alla base di dilemmi o di diagnosi non corrette . 
in alcuni casi ci si trover di fronte anche ad alcune domande : cosa si pensa delle immagini presentate ? come le si referterebbero ? questa recensione pu essere chiusa con alcune delle parole scritte dalle autrici nella prefazione al volume : quale lerrore di minor importanza : porre una diagnosi errata di abuso sico con la conseguenza di allontanare un infante da amorevoli genitori o sbagliare la diagnosi e riconsegnare un beb ad un ambiente in cui gli episodi di abuso possono aggravarsi per culminare nella morte ? entrambi gli scenari sono possibilit reali : la dif colt nel porre la diagnosi di abuso ( soprattutto nei casi non letali ) sta proprio nel fatto che non esiste una speci ca regola aurea . 
cattaneo1 , 2 1labanof , laboratorio di antropologia e odontologia forense , sezione di medicina legale , universit degli studi di milano , via mangiagalli 37 , milano , italy 2dmu dipartimento di morfologia umana e scienze biomediche , universit degli studi di milano , via mangiagalli 37 , milano , italy 3laboratory of biological and molecular anthropology , institute of experimental biology , faculty of science , masaryk university , 60200 brno , czech republic 4department of radiology , sesto s . 
this study aimed at testing the applicability of the greulich and pyle atlas , the demirjian and the mincer methods on a mixed population to compare skeletal and dental methods of age estimation . 
one hundred and nine orthopantomographs ( opg ) of children aged between 4 and 15.5 years were evaluated by demirjians method ; whenever the highest demirjian score was reached ( 31 cases ) , the mincer method was applied . 
tuttavia , non sempre il gruppo etnico di appartenenza pu essere accertato , per esempio nei casi di cadaveri in avanzato stato di decomposizione : in tali casi la stima dellet deve essere eseguita senza le correzioni fornite dalla letteratura per i diversi gruppi etnici . 
centonove ortopantomogra e di bambini di et compresa fra i 4 ed i 15 , 5 anni sono state valutate con metodo demirjian ; nei casi in cui stato raggiunto il massimo punteggio demirjian , si applicato il metodo mincer . 
la maturazione scheletrica di 54 soggetti di et compresa fra i 7 ed i 19 anni stata quindi determinata con il metodo di greulich e pyle . 1106 radiol med ( 2011 ) 116 : 11051114 results . 
mean variances from the different methods do not signi cantly differ from data reported in the literature and demonstrate that the reliability of demirjian , and greulich and pyle as they stand may be applied satisfactorily to remains or individuals of unknown ethnic orig keywords forensic radiology age estimation greulich and pyle atlas demirjian mincer risultati . 
le differenze medie fra i diversi metodi non differiscono signi cativamente dai dati riportati in letteratura e dimostrano che i metodi demirjian e greulich e pyle possono essere applicati con successo a resti o individui di origine etnica sconosciuta . parole chiave radiologia forense stima dellet atlante di greulich e pyle metodo demirjian metodo mincer introduction introduzione age estimation is one of the most relevant issues for juridical consequences and at the same time a dif cult issue in forensic radiology , both in cases of unknown corpses and in the living ( although with different aims ) from imputability of individuals who do not have legal documents to adoption . 
some reviews of these methods have been made in the last few years , and with time , the rst guidelines have begun to appear in the forensic scenario [ 13 ]  . 
ethnic variability is undoubtedly a relevant issue in age estimation , which is shown also by the increase in the number of population studies , leading in some cases to the development of speci c sections within scienti c although it seems recommendable to apply population - speci c methods , sometimes , ethnicity is not known . 
 in the case of unknown deceased , for example , the speci c ethnic group the subject belongs to can only be hypothesised , and if the corpse is badly preserved , even the main race can be de ned only with dif culty . 
the few studies concerning the epidemiology of unknown deceased individuals state that , on average , one third of all cases concern charred bodies or corpses in advanced decomposition , with clear limits in racial assessment [ 4 ]  . 
but how safely different skeletal and odontological radiological methods can be applied to subjects of unknown ethnicity is not clear . the few guidelines existing in the literature suggest three methods as gold standards for use with the living : the greulich and pyle atlas , the demirjian and the mincer methods . 
 the reference atlas of greulich and pyle is the most widely used method for bone - age determination from hand and wrist la stima dellet uno degli argomenti pi rilevanti in ambito antropologico per le conseguenze giuridiche , e nello stesso tempo una delle applicazioni pi complesse della radiologia forense , sia nellambito del riconoscimento dei cadaveri sconosciuti che nel caso di viventi , seppur con ni differenti . 
diversi metodi di stima dellet , sia scheletrici che dentari , sono stati sviluppati dalla letteratura , e negli ultimi anni sono iniziate a comparire le prime revisioni sui diversi metodi formulati e le prime linee - guida da applicare allo scenario forense [ 13 ]  . 
la variabilit etnica indubbiamente un fattore importante nellambito della stima dellet , come dimostrato anche dal crescente numero di studi di popolazione che hanno portato in alcuni casi allo sviluppo di speci che sezioni nellambito dei giornali scienti ci ; anche se raccomandabile applicare i necessari fattori di correzione derivanti da tali studi , a volte la razza del soggetto di cui necessario eseguire la stima dellet non conosciuta . 
 nel caso di cadaveri sconosciuti ad esempio lo speci co gruppo etnico di appartenenza pu essere solo ipotizzato , e se il cadavere in avanzato stato di decomposizione , persino il gruppo razziale principale pu essere solo de nito con estrema dif colt . 
i pochi studi riguardanti la casistica di cadaveri sconosciuti evidenziano che in media un terzo di tutti i casi riguarda cadaveri carbonizzati o corpi in avanzato stato di decomposizione , con evidenti limiti per la diagnosi di razza [ 4 ]  . 
questo signi ca che la stima dellet in tali casi risulta mancante dellinformazione riguardante lef cienza e laf dabilit degli speci ci metodi scheletrici e dentari in relazione alle variabili etniche . 
tuttavia non ancora chiaro quanto pu essere sicura una stima dellet effettuata tramite metodi scheletrici e dentari basati su immagini radiogra che nel caso di soggetti privi di indicazioni sul gruppo razziale di appartenenza . 
ethnic variability has been considered by the literature : the greulich and pyle method , for example , has shown the widest limits in black female subjects , and some authors suggest that the atlas in these cases should not be applied [ 10 ]  . 
different authors in fact state that other skeletal tests , such as tannerwhitehouse ii , should be the method of choice , thanks to the higher precision shown in different experimental studies [ 11 , 12 ]  . 
however , the literature does not provide a univocal indication , as in some cases , the difference of errors between the two methods does not seem signi cant [ 13 ]  . 
in any case , the greulich and pyle atlas is currently one of the most common methods used for assessing skeletal age not only in forensic , but also in clinical , practice , especially among radiologists since it is easy and fast to use [ 13 , 14 ]  . the demirjian method for assessing dental maturity was rst described in 1973 , applied on a french canadian population , and is widely used and accepted thanks to an easy and user - friendly maturity scoring system , even though the procedure does not consider racial differences . 
a score is given to the dental elements , according to root development , from a to h : a indicates the rst stage of dental development , with the mineralisation of tooth cusps ; h shows that the root growth is complete . 
each stage has an assigned number score ; the sum of scores from the seven permanent teeth ( two incisors , one canine , two premolars and two molars ) gives the age estimation [ 15 ]  . 
different authors have so far applied the method on several populations , and most ascertained that the maturity curves elaborated for the demirjian population did not t [ 1618 ] and that the dental maturity in their respective populations was advanced [ 17 , 1932 ]  . 
 [ 38 ] rst attempted to standardise the demirjian method for a belgian population , although the authors state that the revised version may be not applicable to other geographical contexts . 
other authors pointed out that the demirjian method , although with a general overestimation , shows similar results in different populations , limiting the importance of the racial factor [ 39 , 40 ]  . from demirjian charts for evaluating dental growth , another method was developed based on the study of third molar ( m3 ) development , described by mincer et al . 
their study provides age thresholds for amerletteratura indicano tre metodi come il gold standard per la stima dellet : latlante di greulich e pyle , il metodo demirjian ed il metodo mincer . 
la variabilit etnica stata infatti considerata dalla letteratura : il metodo di greulich e pyle , ad esempio , ha mostrato limiti consistenti quando stato utilizzato per stimare let di femmine negroidi , tanto che diversi autori suggeriscono che latlante in questi casi non dovrebbe essere utilizzato [ 10 ]  . 
 diverse fonti infatti sottolineano che in questi casi altri test come il tanner - whitehouse ii dovrebbero essere la metodiche di scelta , come mostrato dalla maggiore precisione evidenziata dallapplicazione di tale metodo in diversi studi sperimentali [ 11 , 12 ] ; tuttavia attualmente non esiste unindicazione univoca in tal senso , poich in alcuni casi la differenza degli errori mostrata dai due metodi non sembra signi cativa [ 13 ]  . 
in ogni caso , latlante di greulich e pyle attualmente uno dei metodi pi comuni di stima dellet non solo in ambito forense , ma anche nella pratica clinica , specialmente fra i radiologi , poich facile e rapido da usare [ 13 , 14 ]  . il metodo demirjian per la stima dellet dentaria stato descritto per la prima volta nel 1973 , ed stato tarato su una popolazione franco - canadese ; oggi ampiamente accettato ed utilizzato , grazie anche alla facilit di utilizzo del suo metodo a punteggio , sebbene il metodo non prenda in considerazione le differenze etniche . 
un punteggio viene assegnato ad ogni elemento dentario in base al grado di sviluppo della radice , dallo stadio a allh ; a indica il primo stadio di sviluppo dentario , con la mineralizzazione delle cuspidi dentarie , mentre lo stadio h indica che laccrescimento radicolare completo . 
ogni stadio ha un determinato punteggio , variabile per ogni elemento dentario : la somma dei punteggi degli elementi dentari di una emiarcata tranne il terzo molare ( i due incisivi , il canino , i due premolari e i primi due molari ) fornisce la stima dellet [ 15 ]  . 
diversi autori hanno applicato nora il metodo a differenti contesti geogra ci : molti di loro hanno veri cato che le curve di maturit elaborate da demirjian non concordavano con i dati relativi a singoli gruppi etnici [ 1618 ] , e che la maturazione dentaria delle rispettive popolazioni era pi avanzata [ 17 , 1932 ] o , meno frequentemente , veri cavano una sottostima dellet derivante dallapplicazione del metodo [ 3133 ] , sebbene in tali casi i fattori socio - economici potrebbero avere un ruolo non trascurabile . 
in the majority of cases , the method is applicable [ 43 , 44 , 46 , 48 , 50 ] , although some differences in timing of third molar development were observed between populations [ 42 , 49 , 51 , 5254 ] , in part because the m3 is the most variable tooth in the dentition . 
nevertheless , very few studies have been performed to verify their reliability if the race is unknown , as commonly occurs in the case of unknown deceased or the living without documents . 
this study aimed to ascertain the applicability of the three most commonly used methods of age estimation ( greulich and pyle , demirjian , mincer in their original versions ) to a population of unknown ethnic origin in order to verify their reliability . materials and methods one hundred and sixty - seven subjects ( 78 males , 89 females ) of various ethnic origin ( egypt , morocco , senegal , argentina , brazil , colombia , ecuador , peru , albania , bulgaria , moldavia , romania , greece ) aged between 4 and 31 years ( table 1 ) who underwent hand and wrist radiography and an orthopantomography ( opg ) between 1999 and 2008 in the department of radiology of the hospital of sesto s . 
 skeletal maturation of hand and wrist from 54 subjects ( 25 males , 29 females ) aged between 7 and 19 years of age was determined by the greulich and pyle method . 
 [ 38 ] per primi tentarono di standardizzare il metodo demirjian alla popolazione belga , sebbene gli autori stessi osservino che il metodo revisionato potrebbe non essere applicabile ad altri contesti geogra ci [ 38 ]  . 
daltra parte , altri autori sottolineano che il metodo demirjian , sebbene con una generale e costante sovrastima , produce risultati equiparabili in diverse popolazioni , il che limiterebbe limportanza del fattore etnico nellapplicazione di tale metodo [ 39 , 40 ]  . dagli schemi di demirjian per la valutazione dellaccrescimento dentario , un altro metodo stato sviluppato , basato sullo studio del terzo molare ( m3 ) descritto da mincer et al . 
gli stessi stadi ( da a ad h ) creati da demirjian sono stati applicati al terzo molare , allo scopo di ottenere informazioni sullet di soggetti sopra i 16 anni , limite del metodo demirjian . 
gli studi di mincer consentirono di estrapolare i valori di riferimento per la popolazione bianca americana ( dai 14 ai 24 anni ) e per gli afroamericani ( standardizzati solo dallo stadio f allo stadio h )  . 
diversi autori hanno applicato il metodo anche ad alcune popolazioni asiatiche ed europee [ 4251 ] ; nella maggior parte dei casi il metodo applicabile [ 43 , 44 , 46 , 48 , 50 ] , sebbene alcune differenze fra le diverse popolazioni nello sviluppo del terzo molare siano state descritte nelle diverse popolazioni [ 42 , 49 , 51 , 5254 ] , anche a causa delle variabilit di sviluppo di tale elemento dentario . 
 quelli sopra elencati sono comunemente considerati dai diversi autori come i metodi di elezione per la stima dellet e sono attualmente i pi utilizzati in ambito forense ; tuttavia , pochissimi studi sono stati condotti per veri care la loro af dabilit nei casi in cui letnia del soggetto non sia conosciuta , come spesso accade per i cadaveri sconosciuti o per i viventi privi di documenti . 
questo studio mira a veri care lapplicabilit dei tre metodi di stima dellet pi utilizzati in ambito forense ( greulich e pyle , demirjian , mincer nelle loro versioni originali ) , applicati su una popolazione di origine etnica ignota , allo scopo di veri care in tale delicata situazione la loro af dabilit . table 1 details of hand and wrist radiographs and orthopantomographs hand - wrist radiographs , n orthopantomographs , n male female total materiali e metodi tabella 1 dettagli delle radiogra e di mano e polso ed ortopantomogra a ( opt ) selezionati per lo studio maschi femmine totale radiogra e di mano e polso , n 25 opt , n sono stati inclusi nello studio 167 soggetti ( 78 maschi , 89 femmine ) di origine etnica differente ( egitto , marocco , senegal , argentina , brasile , colombia , ecuador , per , albania , bulgaria , moldavia , romania , grecia ) di et compresa fra i 4 ed i 31 anni ( tabella 1 ) che si sottoposero a radiogra a di mano e polso ed ortopantologra a ( opt ) fra il 1999 ed il 2008 presso il dipartimento di radiologia dellospedale di sesto s . 
 results the greulich and pyle method ( table 2 ) showed that age was overall more frequently underestimated ( in 46% of cases ) than overestimated ( in 37% ) ; the agreement of estimated age ( ea ) and chronological age ( ca ) within 1 year was observed in 17% of cases . 
 zione scheletrica di mano e polso stata valutata in 54 soggetti ( 25 maschi , 29 femmine ) di et compresa fra i 7 ed i 19 anni , tramite confronto con atlante di greulich e pyle . 
 le differenze fra et stimata ed et cronologica sono state calcolate per ogni metodo , cos come la differenza media , massima e minima per i maschi e le femmine . 
 risultati lutilizzo dellatlante di greulich e pyle ha mostrato pi frequentemente una sottostima dellet ( 46% ) che una sovrastima ( 37% ) ( tabella 2 ) ; la corrispondenza dellet stimata con let cronologica ( entro lanno ) fu osservata nel 17% dei casi , e fu osservata pi frequentemente nei maschi ( 28% ) che nelle femmine ( 7% )  . 
la differenza media fra et stimata ed et cronologica stata di 0 , 755 anni0 , 522 deviazione standard ( ds ) , nei maschi di 0 , 819 anni0 , 995 ds e nelle femmine di 0 , 7010 , 522 ds ; la differenza massima fra et stimata ed et cronologica fu 3 , 5 anni , la differenza minima di 0 anni . 
 la differenza media fra et stimata ed et cronologica fu di 0 , 824 anni0 , 76 ds , nei maschi 0 , 861 anni0 , 765 ds e nelle femmine 0 , 79 anni0 , 753 ds , la differenza massima fu di 3 , 26 anni e la minima di 0 , 01 anni . 
 tutti i soggetti di et superiore ai 23 anni furono correttamente diagnosticati dal metodo mincer ; la differenza rispetto allet cronologica fu in media di 2 , 95 anni2 , 496 ds . 
la differenza media pi bassa rispetto allet cronologica fu ottenuta dallapplicazione dellatlante di greulich e pyle ( 0 , 755 anni0 , 522 ds ) , seguito dal metodo demirjian con una differenza media di 0 , 824 anni0 , 76 ds . 
il metodo mincer ha mostrato la differenza media pi elevata ( 2 , 95 anni2 , 496 ds )  . negli ultimi anni gli studi sulle metodologie di stima dellet si sono concentrate in particolar modo sulla variabilit etnica . 
in the case of living individuals with no valid documents and with uncertain age and area of provenance , as in cases of unknown deceased or of the living with no identi cation documents , age estimation is important and frequently of radiological relevance , particularly for juveniles and young adults . 
in this scenario , the literature needs to provide not only indications concerning the applicability of single methods to different populations but also to verify whether the results from the same methods are dependent on the ethnic factor . 
this study was performed to verify whether the standards of greulich and pyle , demirjian and mincer methods in their original version are applicable to young adults when their ethnic origin is unknown , in comparison with data from studies performed on populations of known origin . the rst information derives from comparison of the three methods : the greulich and pyle atlas proved to be the most accurate , as con rmed by the literature [ 55 , 56 ] , followed by demirjian and then mincer . 
for example , the literature has shown that the greulich and pyle atlas is less reliable in black females , whereas the error range is more limited in white females and black males [ 8 , 10 ]  . 
the study substantially con rms the indications provided by the literature : the atlas is more prone to yield the best results in female populations , as reported by several authors [ 10 , 57 ]  . 
in 17% of cases , estimated and chronological ages were concordant within 1 year , which shows the fairly good reliability of the atlas as a preliminary method in age assessment , regardless of ethnic origin , in comparison with dental methods . 
this result may be explained by the limited number of x - ray images included in the atlas , whereas the demirjian method , based on the sum of seven different scores , has a wider range of possible results . 
nevertheless , this is a preliminary indication concerning the higher reliability of the greulich and pyle atlas in comparison with dental methods . the demirjian method showed a very similar error range to data provided by the literature in different geographical contexts . 
in tale scenario risulta di notevole importanza ottenere informazioni sullapplicabilit dei singoli metodi su diverse popolazioni , e veri care se i risultati derivanti dagli stessi metodi dipendano dalla variabilit etnica . 
lo studio attuale stato effettuato allo scopo di veri care se i metodi greulich e pyle , demirjian e mincer nella loro versione originale sono applicabili ai giovani adulti nel caso in cui lorigine etnica degli stessi sia sconosciuta . la prima informazione ottenuta deriva dal confronto dei tre metodi : latlante di greulich e pyle risultato il pi af dabile , come peraltro confermato dalla letteratura [ 55 , 56 ] , seguito dal metodo demirjian e mincer . 
per esempio , la letteratura ha mostrato che latlante di greulich e pyle meno af dabile nel caso di femmine negroidi , mentre lerrore medio pi limitato nel caso di femmine caucasoidi e maschi negroidi [ 8 , 10 ]  . 
lo studio attuale ha sostanzialmente confermato le indicazioni fornite dalla letteratura : latlante tende a fornire i risultati migliori nella popolazione femminile , come confermato da diversi autori [ 10 , 57 ]  . 
nel 17% dei casi let stimata corrispondeva allet cronologica con un errore inferiore allanno ; lo studio ha evidenziato una buona af dabilit dellatlante di greulich e pyle come metodo preliminare di stima dellet indipendentemente dal fattore etnico , in paragone ai metodi dentari ; tale risultato potrebbe essere spiegato dal limitato numero di immagini radiogra che incluse nellatlante , mentre il metodo demirjian , basato sulla somma di sette differenti punteggi , ha una pi ampia gamma di possibili risultati : nondimeno , i risultati emersi da questo studio sono ancora preliminari , e richiedono una conferma su una popolazione pi ampia . 
 il metodo demirjian ha mostrato un margine di errore sovrapponibile con le informazioni fornite dalla letteratura sullapplicazione del metodo nei diversi contesti geogra ci , che evidenzia una generale tendenza alla sovrastima . 
lo stesso fenomeno stato osservato infatti nel caso dellapplicazione del metodo su popolazioni saudite [ 23 ] , ungheresi [ 27 ] , nord - est brasiliane [ 26 ] , norvegesi [ 28 ] , nlandesi [ 29 ] , polacche [ 30 ] , cinesi [ 55 ] , olandesi [ 25 ] , iraniane [ 31 ] , australiane [ 19 ] e brasiliane [ 20 ]  . 
i risultati del presente articolo sembrano confermare che il metodo quantitativo sviluppato da demirjian lievemente in uenzato dalla variabilit etnica , come mostrato da diversi autori ( tabella 5 ) [ 39 , 40 ]  . 
unaltra informazione emersa nel corso dello studio riguarda lelevata af dabilit del metodo nella diagnosi dei soggetti di et superiore 1112 radiol med ( 2011 ) 116 : 11051114 table 5 comparison of results of the demirjian method with data provided by the literature on different populations this study farah et al . 
differences shown by different sources seem to con rm the quantitative method developed by demirjian is in uenced slightly by ethnic variation , as stated by different authors [ 39 , 40 ] ( table 5 )  . 
another nding provided by the study concerns the success of the demirjian method in recognising subjects > 16 years , which were all correctly assessed with the highest maturation score . 
the demirjian method can be therefore considered as a good screening method , regardless of ethnic origin , in distinguishing subjects > 16 years , who will then be examined by age estimation methods tested on the late adolescent population , such as the mincer method . 
nevertheless , this procedure should follow an initial age assessment based on skeletal maturation performed by the greulich and pyle method in order to reduce the number of false positive results ( subjects wrongly assessed as being > 16 and 23 years )  . concerning the mincer method , the mean variance was distinctively higher than in the demirjian and greulich and pyle methods . 
 our study therefore con rmed data from the literature ai 16 anni , che sono stati tutti correttamente valutati con il punteggio massimo di maturazione dentaria ; il metodo demirjian pu essere pertanto considerato come un buon metodo di screening indipendentemente dal fattore etnico per distinguere i soggetti di et superiore di 16 anni , che poi saranno ulteriormente esaminati da metodi di stima testati su soggetti tardo - adolescenti e giovani adulti , come il metodo mincer . il metodo di mincer stato in grado di diagnosticare con suf ciente precisione tutti i soggetti di et superiore ai 23 anni . 
nondimeno , tale metodo dovrebbe essere applicato dopo una prima stima dellet basata sul grado di maturazione scheletrica tramite lutilizzo dellatlante di greulich e pyle , allo scopo di ridurre il numero di falsi positivi ( soggetti erroneamente valutati sopra i 16 ed i 23 anni )  . per quanto riguarda il metodo di mincer , la differenza media rispetto allet cronologica fu pi elevata rispetto al metodo demirjian ed allutilizzo dellatlante di greulich e pyle . 
 this information , if con rmed by further studies on wider populations , will assist in de ning a common procedure for age estimation based on the potential of the single methods in order to reduce the estimated age range , even in cases of blind age assessment where individualisation is dif cult to achieve . 
even if it remains true that the smallest error will be achieved when using population - speci c adaptations to methods , blind use of such radiological methods , regardless of the results , may be acceptable , as long as the larger error is taken into consideration with respect to populationspeci c approaches . 
 del soggetto non siano disponibili ; inoltre , i risultati forniti dai singoli metodi evidenziarono unelevata precisione nella diagnosi dei soggetti di et superiore ai 16 anni per il metodo demirjian , e sopra i 23 anni per il metodo mincer ; tale informazione , se confermata da ulteriori studi eseguiti su popolazioni pi ampie , potrebbe fornire un aiuto nella de nizione di una procedura standardizzata per la stima dellet , basata sulla potenzialit di ogni singolo metodo per ridurre lintervallo di stima dellet , anche nei casi in cui la stima dellet sia cieca delle indicazioni sulletnia di appartenenza , ove laderenza del risultato nale al singolo individuo dif cilmente realizzabile . 
anche se rimane scontato che il minor margine di errore viene raggiunto utilizzando applicando i fattori di correzione speci ci per le singole popolazioni etniche , un utilizzo cieco dei metodi radiologici di stima pu essere accettabile . 
avogadro , novara , italy 2universit degli studi di roma campus biomedico , roma , italy 3universit degli studi di roma cattolica , roma , italy 4universit degli studi di sassari , sassari , italy 5universit degli studi di chieti , chieti , italy 6universit degli studi di trieste , trieste , italy 7universit degli studi di catania , catania , italy 8universit degli studi di varese , varese , italy 9universit degli studi di genova , genova , italy 10universit degli studi di foggia , foggia , italy 11universit degli studi di verona , verona , italy 12universit degli studi di milano bicocca , milano , italy 13universit degli studi di modena , modena , italy 14universit degli studi di firenze , firenze italy 15universit degli studi di udine , udine , italy correspondence to : a . 
once a common educational programme and time slot had been identi ed and planned , the programme was delivered via internet - based video conferencing once a week for 2 - h lectures . 
the universities involved were trieste , udine , verona , milano bicocca , novara , varese , genova , sassari , rome campus , rome cattolica , chieti , foggia , catania , modena and firenze . 
scopo del nostro lavoro stato progettare , realizzare e valutare un percorso didattico di e - learning per la formazione degli specializzandi in radiodiagnostica , coinvolgendo pi scuole di specializzazione distribuite su tutto il territorio nazionale , nellottica della condivisione culturale . 
previa identi cazione e piani cazione di un programma didattico temporale condiviso , la modalit tecnica di e - learning in teleconferenza ha previsto un collegamento via internet il mercoled pomeriggio e due ore di lezione , alla lezione seguita una interazione didattica delle singole sedi con il discente . 
le universit che hanno aderito sono state : trieste , udine , verona , milano bicocca , novara , varese , genova , sassari , roma campus , roma cattolica , chieti , foggia , catania , modena , firenze . 
based on our experience , whereas e - learning in radiology has become established and compulsory , there is the need for legislation that on the one hand protects online teaching activity and on the other allows study and continuing medical education ( cme ) credits to be recognised . keywords e - learning video conferencing radiology lezioni , per un totale di 36 ore di lezione effettive . 
relativamente al giudizio sulla qualit del video e , in particolare , sul dettaglio delle immagini radiologiche proposte in diapositiva e / o in lmati il 71% dei discenti ha espresso un giudizio ottimo , il 24% un giudizio buono , il 4 , 5% un giudizio suf ciente non vi stato alcun giudizio insuf ciente . 
da quanto esposto e dallesperienza vissuta se la via delle - learnig in radiologia , a nostro parere , ormai segnata ed obbligatoria , si impone la necessit legislativa di normative che , da una parte , tutelino lattivit didattica in rete e , dallaltra , consentano il riconoscimento di crediti formativi e di educazione continua in medicina ( ecm )  . parole chiave educazione via internet teleconferenza radiologia introduction introduzione the days are long gone when socrates taught with the peripatetic method , whereby each step , or thereabouts , corresponded to a notion that his students were required to appropriate . 
throughout history , teaching has kept pace with the changing times according to patterns , projects and options dictated , for the most part , by technological development [ 1 , 2 ]  . 
with the dawning of the new millennium information , technology ( it ) has become for education and teaching a pillar supporting new teaching strategies , and with it , the term e - learning has been coined [ 1 , 3 ]  . e - learning is short for electronic learning and refers to the possibility of offering teaching and / or education via the internet or world wide web [ 4 , 5 ]  . 
the extent of the role of e - learning soon became evident , such that at the end of 1999 , the european commission launched the eeurope programme , which aimed to accelerate the learning of digital technology in european countries [ 6 ]  . 
in this programme , e - learning is placed at the heart of the european unions cultural policy . as always occurs , the far - reaching spread of new technologies is a slow and gradual process , and the creation of an information technology ( it ) culture took some time [ 7 ]  . 
 technological familiarisation was required , and the results speak for themselves : in 1997 , only 16.7% of italian housesono ormai lontani gli anni in cui socrate educava ed insegnava con il metodo peripatetico , l dove ad ogni passo , o quasi , corrispondeva una nozione che gli allievi , podisti per de nizione , dovevano incamerare . 
nella evoluzione storica anche la didattica stata al passo con i tempi secondo schemi , progetti ed opzioni dettati , soprattutto , dalla evoluzione tecnologica [ 1 , 2 ]  . 
a partire dal nuovo millennio anche leducazione e linsegnamento hanno trovato nellofferta elettronica un pilastro su cui costruire nuove strategie didattiche ed stato coniato il termine e - learning [ 1 , 3 ]  . e - learning lacronimo di electronic learning cio la possibilit di mettere a punto unofferta didattica e / o di educazione tramite internet o world wide web [ 4 , 5 ]  . 
la convinzione che lelectronic learning potesse cambiare le regole del gioco stata immediata , tanto che la commissione europea alla ne dellanno 1999 ha dato vita al programma eeurope , che ha avuto come scopo laccelerazione dellapprendimento della tecnologia digitale nei paesi europei [ 6 ] ; in questo programma viene posto proprio le - learning al centro della politica culturale dellunione . come sempre avviene , il processo di diffusione capillare di nuove tecnologie lento e graduale ed anche la cultura informatica ha necessitato dei suoi tempi [ 7 ] , si parlato di interventi di familiarizzazione tecnologica ed i risultati sono stati tangibili : basti pensare che se nel 1997 solo il 16 , 7% delle famiglie italiane possedeva un personal computer radiol med ( 2011 ) 116 : 989999 holds owned a personal computer , whereas the gure today is said to be around 90% . in 2003 , under the advocacy of the tertiary education and research sectors , the italian society of e - learning ( sie - l ) was founded with the aim of promoting teaching courses at the school , university and postuniversity levels . 
in fact , only 2 short years later , in 2005 , around 80% of italian universities were able to offer either pure or blended e - learning courses [ 1 ]  . in the european setting , italy was quick to realise the prospects of e - learning . 
also in 2003 , a study carried out by assintel ( national association of enterprises operating in the information and communication technology sector ) showed that the e - learning market in italy has grown faster than in other european countries [ 7 ]  . 
 indeed , thanks to the internet , a teacher / trainer may simultaneously reach a greater number of students / trainees in different locations [ 8 , 9 ]  . the advent of teaching over the internet has also enabled the low - cost enhancement of a new concept of cultural sharing . 
this sees the involvement of numerous teachers / trainers representing different working groups who make their contribution and share their own experiences with other colleagues and / or working groups in different locations [ 1012 ]  . 
the aim of our work was to plan , implement and evaluate an e - learning teaching course for the training of radiology residents at numerous specialty schools located throughout italy in the setting of cultural sharing . materials and methods the initial planning phase of the project involved the presentation of the project and aggregation of the participants . 
 an e - mail was sent on 11 may 2009 informing all directors of the italian specialty schools of radiology of the desire to establish an e - learning project for the 2009 / 2010 academic year in the form of single - topic teaching seminars . 
once participation in the project had been acquired , a lesson calendar was drawn up , with seminars attualmente si parla di percentuali vicine al 90% . nel 2003 , sotto la spinta del mondo accademico e della ricerca , stata costituita in italia la societ italiana di e - learning ( sie - l ) , che ha come scopo il favorire percorsi didattici a livello scolastico , universitario e post - universitario ; questo messaggio , di innovazione culturale , stato recepito soprattutto dal mondo accademico tanto che , dopo appena due anni , nel 2005 , circa l80% delle universit italiane erano in grado di offrire percorsi didattici e - learning , puro o blended [ 1 ]  . 
98 del 29 / 04 / 2003 con la legge moratti - stanca si sono costruite le basi per le procedure di accreditamento dei corsi di studio a distanza delle universit statali e non statali e sempre nel 2003 , da uno studio condotto dallassociazione nazionale delle imprese che operano nel settore dellinformatica & communication technology ( assintel ) si evince che il mercato italiano delle - learnig ha presentato il tasso di crescita pi alto rispetto a quello degli altri paesi europei [ 7 ]  . 
internet funge da collante e da veicolo tecnico e culturale ; infatti tramite , e grazie , ad esso possibile per un docente raggiungere , simultaneamente , pi discenti allocati in diverse sedi [ 8 , 9 ]  . lavvento della diffusione didattica , tramite internet , consente , inoltre , di potenziare con costi contenuti , un nuovo concetto di condivisone culturale ; tale concetto vede coinvolti ed impegnati pi docenti , espressione di diversi gruppi di lavoro , che apportano il loro contributo , condividendo la propria esperienza con altri colleghi e / o gruppi di lavoro di diverse sedi [ 1012 ]  . 
scopo del nostro lavoro stato progettare , realizzare e valutare un percorso didattico di e - learning per la formazione degli specializzandi in radiodiagnostica , coinvolgendo pi scuole di specializzazione distribuite su tutto il territorio nazionale , nellottica della condivisione culturale . materiali e metodi la piani cazione del progetto ha previsto una prima fase di presentazione ed aggregazione telematica degli attori . 
 tramite e - mail , in data 11.05.2009 tutti i direttori delle scuole di specializzazione in radiodiagnostica italiane sono stati informati della volont di istituire , per lanno accademico 2009 / 2010 , un progetto di e - learning sotto forma di seminari didattici monotematici . 
acquisite le adesioni al progetto stato piani cato , in base ad esse , un calendario delle lezioni che ha previsto lattivit seminariale a partire dal 21 ottobre 2009 per concludersi a luglio 2010 . 
luigia macarini , luca colosimo , cesare ettorre gian , carlo beomonte zobel , bruno torricelli , pietro cova , maria cova , maria zuiani , chiara mascalchi , mario pozzi - mucelli , roberto sironi , sandro fugazzola , carlo garlaschi , giacomo meloni , gianni carriero , alessandro bonomo lorenzo beomonte zobel bruno storto m . 
per ogni scuola di specializzazione stato , inoltre , richiesto un referente che potesse fungere da tutor di rete per la realizzazione dellintero progetto [ 13 ] , per coinvolgere gli specializzandi stato deciso che il tutor di rete dovesse essere un iscritto alla scuola di specializzazione e radiol med ( 2011 ) 116 : 989999 tutor should be enrolled at the school . 
coordination of the entire network was entrusted to the novara network tutor resident . from the technical point of view , the entire e - learning process was managed by a system administrator with expertise in this sector ( exit srl ) , and the online meeting space microsoft live meeting was chosen for presenting the lessons . 
it requires installation of a software application on all participants computers and provides real - time interaction with participants who may make presentations , launch projects , brainstorm , modify les or collaborate through the use of a virtual whiteboard . 
the programme was chosen for its speed , the excellent audio / video quality and the voice compression characteristics , which guarantee easy listening even in the presence of microinterruptions in the connection . 
in terms of hardware , the minimum requirements for connection and participation in the lessons were the following : personal computer with a 500 - mhz processor or above ( 1 ghz recommended ) operating system windows xp sp2 or sp3 or above ( vista or windows 7 ) at least 256 mb ( 512 mb recommended ) dedicated directx video card compatible with 64 mb of random access memory ( ram ) webcam audio card , microphone , speakers / headphones video projector or other peripheral device for video reproduction , e.g. 
plasma or liquid crystal display ( lcd ) screen , with super video graphics array ( vga ) resolution of at least 800600 ( super vga 1 , 024768 recommended ) fast subscriber line ( adsl ) in order to receive the content , the computers used in the various locations required the following programmes in addition to microsoft live meeting : internet browser ( interned explorer ( ie ) 6 or above , mozilla firefox 3.x , apple safari 3.x ) sun java 1.6.0_11 or above microsoft of ce power point 2002 or above adobe flash player 9 or above . with regard to the server , a hosted service external to the organisation was used , i.e. 
in addition to the part of the server ( hosted ) , the programme was completed with a software client to be installed on all computers participating in the meeting and which could be automatically installed at the rst invitation to participate . 
the client was extremely lightweight , free and constantly updated thanks to the internet connection , e.g. , asymmetric digital la coordinazione tutoriale dellintera rete stata af data allo specializzando tutor di rete di novara . dal punto di vista tecnico tutto il processo di e - learnig stato af dato ad un amministratore di sistema esperto in tale attivit ( exit srl ) e per le lezioni stato valutato e scelto il programma di videoconferenza , microsoft live meeting . 
microsoft live meeting consente di accedere , tramite internet , ad unarea per riunioni in linea ; esso necessita linstallazione di un software su tutti i computer dei partecipanti e consente una reale interazione con i partecipanti che possono effettuare presentazioni , avviare progetti , mettere insieme idee , modi care le , collaborare attraverso una lavagna virtuale . 
 il programma stato selezionato per la sua velocit , lottima resa audio - video e le caratteristiche di compressione della voce che garantiscono uidit nellascolto anche in presenza di microinterruzioni di banda . 
oltre alla parte del server ( hosted ) , il programma si completa con un software client da installare sui computer che partecipano alla riunione , e che pu essere , automaticamente , installato sin dal primo invito di partecipazione . 
una lezione tipo eseguita durante il ciclo seminariale on line ha previsto , in primis , da parte dellamministratore del sistema , la creazione di una conference room alla quale vengono assegnati i partecipanti e generate le relative credenziali di accesso al processo di e - learnig . 
 in data 20 settembre 2009 , presso listituto di radiologia delluniversit del piemonte orientale di novara , si svolta una riunione preliminare , in cui erano presenti i tutor 994 radiol med ( 2011 ) 116 : 989999 windows update facility . 
a typical lesson delivered during the online series of seminars rst involved creation by the system administrator of a virtual conference roo the participants were assigned to the conference room and the relative access credentials for the e - learning process were generated . on 20 september 2009 , a preliminary meeting was held at the universit del piemonte orientale di novara attended by all network tutors of the participating specialty schools . 
for the purposes of assessing the effectiveness of the project , a common multiple - choice questionnaire was devised and approved , to be completed at the end of every lecture at each of the locations . 
the questionnaire sought information regarding number of participants in the classroom , overall assessment of the teaching content , interruptions without reconnection of the internet service , transient interruptions of the internet service and audio and video quality . 
at the end of the series of lessons random suggestions on how to improve the project on the whole were requested from some of the residents . results after identifying and planning a joint teaching programme ( table 1 ) , the technical approach to e - learning in the online meeting space involved an internet connection on wednesday afternoons and a 2 - h lesson , followed by more traditional interaction with the trainee radiologists at the individual locations . 
the following universities participated in the project : trieste , udine , verona , milan bicocca , novara , varese , genoa , sassari , rome campus , rome cattolica , chieti , foggia , catania , modena and florence . 
the university of rome cattolica participated in the project with two locations : rome gemelli university hospital and rome cattolica campobasso campus . overall 18 lessons were held for a total of 36 h of teaching . 
with regard to the overall attendance of the specialty schools to the entire teaching programme , there were absences by the schools in 9% of lessons : three were absent for one lesson , one for seven lessons , one for four lessons and one for six lessons . 
la riunione ha consentito di sviscerare ed affrontare , sia dal punto di vista tecnico che didattico , le varie problematiche ; durante questa , unica , riunione stata quindi costituita la rete organizzativa progettuale . 
 ai ni della valutazione dellef cacia del progetto , stata condivisa ed approvata una scheda comune di valutazione a scelta multipla obbligata , che ogni sede ha compilato alla ne di ogni lezione . 
la scheda ha richiesto delle informazioni relativamente a : numero dei partecipanti in aula , giudizio complessivo sui contenuti didattici , interruzioni senza ripristino della linea internet , interruzione momentanea della linea internet , qualit audio , qualit video . 
alla ne del ciclo didattico sono stati richiesti suggerimenti random ad alcuni discenti , al ne di migliorare il progetto nel suo complesso . risultati previa identi cazione e piani cazione di un programma didattico temporale condiviso ( tabella 1 ) , la modalit tecnica di e - learning in teleconferenza ha previsto un collegamento via internet il mercoled pomeriggio e due ore di lezione , alla lezione seguita una interazione didattica delle singole sedi con il discente . 
le universit che hanno aderito sono state : trieste , udine , verona , milano bicocca , novara , varese , genova , sassari , roma campus , roma cattolica , chieti , foggia , catania , modena , firenze . 
relativamente alla partecipazione complessiva delle scuole di specializzazione allintero programma didattico , nel 9% delle lezioni si sono veri cate assenze da parte delle scuole : tre scuole sono state assenti per una lezione , una scuola per sette lezioni , una scuola per quattro lezioni , una scuola per sei lezioni . 
relativamente al giudizio complessivo dei discenti sui contenuti didattici , l83% ha espresso un giudizio ottimo , il 15% un giudizio buono e lo 0 , 3% un giudizio suf ciente , non vi stato alcun giudizio insuf ciente . relativamente alla interruzione senza ripristino della linea internet , solo in una lezione si veri cata , in una singola sede , una interruzione del collegamento a causa radiol med ( 2011 ) 116 : 989999 pendent of the e - learning process . 
with regard to residents overall opinion of the course content , 83% found the course excellent , 15% good and 0.3% satisfactory ; no trainee expressed an unsatisfactory opinion . an interruption to the internet service without reconnection occurred only on one occasion at one location due to a storm , whereas 1.5% of connections experienced transient interruptions limited to a few minutes and did not signi cantly disrupt learning . 
there were 13 transient interruptions to the internet service for a total of 33 min out of an overall total of 2 , 160 min of internet connection . with regard to residents opinion of video quality , and especially of the detail of the radiological images presented in slides and moving pictures , 71% gave an excellent assessment , 24% good and 4.5% satisfactory ; no trainee expressed an unsatisfactory opinion . 
in this case , the lesson was nonetheless delivered by another location ( novara ) , which at the beginning of the project was nominated as active reserve , ready to intervene and compensate for any technical problems at the location of the scheduled lesson . the overall ( and entirely funded ) costs of the entire series of seminars included the services of a company specialised in webcasting and were equal to 5 , 000 euro . 
the additional cost is dif cult to estimate given the variety of prices and possible con gurations , but it seems reasonable to suggest a minimum amount of 700800 euro . in order to improve the project , 20 random suggestions were requested from the residents who participated in the course . 
 the cases could be presented by the residents at the teaching location for that lesson . provide a nal test on the topic covered . cover a complete topic each year with special emphasis on imaging characteristics ; here emergency medicine was the most proposed topic for a possible future series of seminars . di un temporale , mentre nell1 , 5% dei collegamenti si sono veri cate interruzioni momentanee , contenute nellarco massimo di pochi minuti , che non hanno in ciato la continuit didattica . 
 su un totale di 2160 minuti complessivi di collegamento le interruzioni momentanee della linea internet sono state 13 per un totale di 33 minuti . relativamente al giudizio sulla qualit del video e , in particolare , sul dettaglio delle immagini radiologiche proposte in diapositiva e / o in lmati , il 71% dei discenti ha espresso un giudizio ottimo , il 24% un giudizio buono , il 4 , 5% un giudizio suf ciente , non vi stato alcun giudizio insuf ciente . 
relativamente alla qualit audio , il 72% dei discenti ha espresso un giudizio ottimo , il 25% un giudizio buono , il 3% un giudizio suf ciente , non vi stato alcun giudizio insuf ciente . 
relativamente alla sede di lezione , solo in un caso si veri cato un problema di connessione e caricamento del le con impossibilit a trasmettere la lezione ; in questo caso la lezione stata comunque svolta da unaltra sede didattica ( novara ) che , allinizio del programma di e - learning , era stata prevista come riserva / attiva , pronta ad intervenire per supplire ad eventuali problemi tecnici della sede di lezione programmata in calendario . 
 i costi complessivi , tra laltro nanziati , dellintero ciclo seminariale hanno previsto lassistenza da parte di una ditta specializzata in teletrasmissione , e sono stati pari a 5000 euro . 
tale costo aggiuntivo dif cilmente stimabile , data la variet di prezzi e di possibili con gurazioni , ma ragionevolmente ipotizzabile in un minimo di 700800 euro . al ne di migliorare il progetto sono stati richiesti , in maniera random , 20 suggerimenti da parte dei discenti che hanno partecipato al corso , da questi si evincono i seguenti principali suggerimenti : contenere ad unora il tempo di lezione , al ne di evitare il crollo dellattenzione ; presentare dei casi clinici alla ne di ogni singola lezione , relativi al tema trattato , casi che potrebbero essere presentati dagli specializzandi delle sede didattica di lezione ; predisporre un test nale di apprendimento sullargomento trattato ; trattare ogni anno un argomento completo con particolare attenzione alla semeiotica e , a tal proposito , la maggior esigenza didattica , per il prossimo eventuale ciclo , stata suggerita in tema di patologia dellurgenza . discussione la lezione frontale / ex cattedra , malgrado la sempre maggiore 996 discussion despite the continuing trend towards direct tutorial teaching , traditional lecturing is still an important point of reference [ 14 ]  . 
to keep pace with the times , there is an increasing need to combine a variety of teaching methods to optimise physical space , time and human resources and to maximise cultural gain [ 1 , 9 ]  . 
recently , thanks to the support of new technologies , this need has received an important contribution in the setting of shared culture at low cost [ 15 ]  . 
the sharing of culture makes it possible for opinion leaders of the sector to share professional experience and enrich their own cultural assets through contact with the expertise that is particularly dedicated to the topic . on the other hand , economic dif culties that often arise could seriously jeopardise or at any rate limit direct participation in courses and / or congresses that demand substantial expenses [ 16 ]  . 
this emphasises the concept of safeguarding the need for cultural sharing , enriching and updating with limited costs , by exploiting technological developments and e - learning [ 12 , 1618 ]  . 
in nancial terms , the overall cost of a connection with four centres amounted to 12 , 000 euro , with the setup and management of the point - to - point connection accounting for 8 , 000 euro . 
our preliminary analysis of a satellite conferencing service revealed that , considering booking the satellite and transmitting the signal from the mobile broadcasting station , each 2 - h lesson cost around 3 , 000 euro . recently , the advent of streaming has revolutionised the process of e - learning by making it much more attainable [ 1 , 12 ]  . 
the term streaming indicates the ability to broadcast audio / video data from a single source to one or more reception points , with the signal being conveyed via the internet . 
on - demand streaming indicates that the audio / radiol med ( 2011 ) 116 : 989999 indicazione verso levoluzione tutoriale diretta , rimane , pur sempre , un importante riferimento [ 14 ]  . 
al passo con i tempi , si sente , sempre pi , lesigenza di unire pi forze didattiche al ne di ottimizzare spazi , tempi e risorse umane con il massimo apporto culturale [ 1 , 9 ]  . 
la condivisone culturale consente la possibilit di condividere , con opinion leaders del settore , esperienze professionali , arricchendo il proprio bagaglio culturale grazie al contatto didattico con expertise , che si sono particolarmente dedicati allargomento . daltra parte le dif colt economiche , con cui spesso ci si scontra , potrebbero mandare in crisi , o comunque limitare , la partecipazione diretta a corsi di aggiornamento e / o attivit congressuali che presuppongono costi enormi [ 16 ]  . 
 da qui il concetto di salvaguardare la necessit di condivisione , di arricchimento e di aggiornamento culturale con costi contenuti , sfruttando levoluzione tecnologica , grazie alle - learning [ 12 , 1618 ]  . 
i tentativi di superare le frontiere didattiche , grazie allinsegnamento a distanza , sono stati pi volte descritti dalla letteratura : si passati dai tentativi di collegamento con linea telefonica ai complessi e costosi collegamenti tramite satellite [ 19 , 20 ]  . 
se i collegamenti via satellite sono da sempre stati proibitivi per i costi vivi di esercizio , i collegamenti per via telefonica , nel passato , hanno creato speranze ed illusioni . nellambito delle pregresse esperienze delle scuole di specializzazione in radiodiagnostica in italia , nel 2003 stato tentata unattivit didattica congiunta tra le scuole di specializzazione delluniversit degli studi di novara e di modena . 
a tal ne fu utilizzato un sistema di teletrasmissione per via telefonica tipo polispan fx4 , realizzato con connessione punto - punto ; tale esperienza , malgrado limpegno da parte delle due scuole di specializzazione , non ebbe i risultati attesi , infatti le cadute frequenti della linea telefonica in ciavano pesantemente la qualit didattica ed i costi erano elevati . 
in termini economici basti pensare che una connessione con quattro centri aveva un costo globale di 12000 euro , mentre una connessione punto - punto aveva un costo impianto e gestione pari a 8000 euro . 
la video conferenza tramite satellite ha dei costi poco sostenibili [ 18 , 20 ] sia per la prenotazione del satellite che per la tecnologia di trasmissione ; in una nostra preliminare analisi dei costi , relativa ad un processo di teleconferenza via satellite , abbiamo calcolato che per ogni singola lezione di due ore , tra la prenotazione satellitare e la diffusione con cabina di regia unica su camper mobile , il costo medio si aggira intorno a 3000 euro . 
per streaming si intende la possibilit di veicolare un usso di dati audio / video trasmessi da una sorgente a uno o pi punti di recezione ; il tutto utilizza quale veicolo di diffusione la linea internet . 
lo streaming on demand radiol med ( 2011 ) 116 : 989999 video content is compressed and stored on a server in the form of les , and a user who is connected can request the audio / video content from the server . 
to facilitate distribution of material , the size of video sequences in terms of frames per second needs to be reduced while searching for the appropriate compromise in terms of image and video quality [ 1 , 12 ]  . 
windows media encoder is a highly used encoding application in the windows environment , whereas in linux the most widespread application is mencoder . our pilot e - learning project focused on two priorities ; on the one hand was the need to organise a correct , linear and coherent series of seminars of use to the trainee radiologists and on the other the need for a high - quality product at a reasonable cost . 
in strict teaching terms , the main idea to create a single - theme course on the imaging characteristics of oncological disease proved to be a winning strategy and was particularly appreciated by the residents : 83% found the course excellent , 15% good and 0.3% satisfactory , whereas no participant judged the course to be unsatisfactory . 
this tested single - theme aspect of the course is also fundamental for the purposes of continuing the project , which could develop into a variety of topics over the years . however , in terms of teaching , suggestions from trainee radiologists regarded lesson length . 
in this sense , reducing the length of the lecture to 45 min , to be followed by a session on clinical cases presented by residents at the location of the lecture , could be an alternative solution worth trying out . 
some 7071% of participants judged the overall audiovideo quality to be excellent , which is particularly encouraging considering that small technical modi cations within the individual location could , in the future , have a positive impact at a minimum cost ( optimisation of acoustics in small sound - proofed latest - generation webcams , appropriate video rooms , projectors )  . 
 the entire e - learning process , which also created a minimal sense of cultural belonging , is characterised by presuppone che i contenuti audio / video siano compressi e memorizzati su un server sotto forma di le ed un utente , connesso , possa chiedere al server di ricevere i contenuti audio / video . 
relativamente allattivit didattica in diagnostica per immagini , lencoding costituisce un momento fondamentale ; infatti nelle presentazioni didattiche di diagnostica per immagini la maggiore criticit rappresentata dal peso delle immagini e dai lmati ed necessario disporre di un adeguato programma di encoder . 
per consentire una facile distribuzione del materiale , infatti , necessario ridurre le dimensioni dei lmati , il numero di frame per secondo , trovando un giusto compromesso tra qualit dellimmagine e qualit dei video [ 1 , 12 ]  . 
tutti questi elementi devono essere , necessariamente , ottimizzati , tramite un corretto processo di encoding , in quanto in uenzano , in maniera sensibile , la banda necessaria per poterlo vedere : tra i software dedicati allencoding in ambiente windows , molto diffuso il windows media encoder , mentre in ambito linux il pi diffuso il mencoder . la nostra esperienza pilota di e - learnig ha tenuto conto di due esigenze prioritarie : da una parte la necessit di organizzare una corretta e lineare attivit seminariale organica ed utile ai discenti , dallaltra la necessit di avere un prodotto di elevata qualit a costi contenuti . 
relativamente allaspetto puramente didattico , linput principale di creare un percorso didattico monotematico in tema di semeiotica nella patologia oncologica risultato vincente e particolarmente gradito ai discenti , che nel l83% hanno espresso un giudizio ottimo , nel 15% un giudizio buono e nello 0 , 3% un giudizio suf ciente , senza alcun giudizio insuf ciente . 
 questo aspetto monotematico pilotato , inoltre , fondamentale ai ni del proseguo del progetto che negli anni potrebbe sviluppare diversi argomenti . sempre dal punto di vista didattico , i suggerimenti dei discenti , hanno posto lattenzione sul tempo / lezione ; infatti due ore di lezione sono risultate particolarmente pesanti con calo dellattenzione ; a tal proposito la riduzione del tempo lezione a 45 minuti con unappendice di casi clinici , presentati dai discenti della sede di lezione , potrebbe essere una nuova via didattica suggerita , sicuramente da sperimentare . 
 dal punto di vista tecnico il primo annoso problema delle teleconferenze , cio linterruzione della linea , risultato inin uente ai ni didattici , in particolare le microinterruzioni che si sono veri cate nell1 , 5% dei casi non hanno creato problemi didattici nel complessivo processo di apprendimento . 
il giudizio di qualit complessiva audio - video che , nel 70%71% , stato valutato ottimo , particolarmente incoraggiante , considerato anche il fatto che piccoli accorgimenti tecnici interni alle singole sedi potranno , nel futuro , fare la differenza con un minimo costo ( ottimizzazione dellacustica in sale piccole ed insonorizzate , webcam di ultima generazione , videoproiettori adeguati )  . 998 radiol med ( 2011 ) 116 : 989999 moderate costs . 
in addition , to extend the life of the teaching material , a cd is being prepared that consists of all the lessons , with an associated cost of 2 , 150 euro for 1 , 000 copies . 
this represents a crowning achievement for the entire e - learning process and is particularly important for guaranteeing the continued bene t of this cultural investment . a possible future development of the project is to allow each participant to record the video conferencing lesson , thus creating a le on their own computer containing both the video and audio material . 
in this context , the choice for the moment of not making the lessons available online , despite the possibility of providing password access , is dictated by legislation that fails to protect the concept of copyleft [ 1 , 21 ]  . conclusions the e - learning process has by now become a common feature on the educational scene . 
the innovative nature of e - learning is a useful complement to the traditional educational and training activity ( theoretical and practical ) of each school , which is irreplaceable . 
 the possibility of having the various faculty boards recognise study credits [ creditit formazione universitaria ( cfu ) ] associated with an e - learning project in the setting of specialty - school teaching is a further teaching / institutional goal that could prove to be a valid aid for the teaching body . based on our experience , whereas e - learning in radiology has in our opinion become established and compulsory , there is the need for legislation that on the one hand protects online teaching and on the other allows study and continuing medical education ( cme ) credits to be recognised . lintero processo di e - learnig , che ha anche creato un minimo senso di appartenenza culturale , ha costi contenuti , basti pensare che per ogni lezione avrebbe inciso , su ogni scuola , per un totale di circa 18 euro . 
a latere , al ne di non disperdere il materiale didattico , si sta cercando di creare un cd che possa raccogliere tutte le lezioni , a tal proposito limpatto economico dei costi per costruire il database su cd pari a 2150 euro per 1000 copie ; tale aspetto , a coronamento dellintero processo di e - learnig , particolarmente importante al ne di non disperdere limpegno culturale profuso . in fase di ride nizione del progetto si sta valutando la possibilit , per ogni partecipante , di poter registrare la lezione in videoconferenza , creando un le sul proprio computer che possa contenere sia il materiale video che audio . 
a tal proposito la scelta , al momento , di non mettere in rete le lezioni , malgrado la possibilit di accessi criptati da password , dettata dalla attuale normativa che non tutela il concetto di copyleft [ 1 , 21 ]  . conclusioni il processo di e - learnig fa , ormai , parte integrante della didattica ; esso permette di superare le barriere di diffusione culturale e , con costi particolarmente bassi , permette scambi culturali e condivisioni culturali . 
questa prima esperienza italiana si svolta nello spirito della collaborazione e della sperimentazione , da essa emersa una grande soddisfazione da parte dei docenti e soddisfazione ed entusiasmo da parte dei discenti . 
la didattica in teleconferenza , analogamente a quella dei corsi di aggiornamento post - universitari , migliora complessivamente la qualit della formazione degli specializzandi , che , peraltro , in ciascuna sede deve raggiungere adeguati standard , di cui si deve far carico il direttore con il suo gruppo di docenti . 
cademartiri1 , 2 1dipartimento di radiologia e del cardio - polmonare , azienda ospedaliero - universitaria di parma , c / o piastra tecnica piano 0 , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia e cardiologia , ospedale san gennaro , napoli , italy 4cpc centro prevenzione cardiovascolare , ospedale san raffaele , milano , italy 5dipartimento di radiologia e cardiologia , azienda asl , carrara , italy 6dipartimento di radiologia , universit di messina , messina , italy 7dipartimento di cardiologia , universit di foggia , foggia , italy 8dipartimento di radiologia , azienda ospedaliero - universitaria san martino , genova , italy correspondence to : f . 
a total of 1 , 500 patients ( 928 men , mean age 58.212.5 years ) in sinus rhythm who underwent ctca ( 64 - slice technology ) and cag were enrolled . 
 in the per - patient analysis , sensitivity , speci city , positive predictive value ( ppv ) and negative predictive value ( npv ) of ctca were 99% , 92% , 94% and 99% , respectively . 
obiettivo del nostro lavoro stato valutare laccuratezza diagnostica dellangiogra a coronarica non invasiva con tomogra a computerizzata ( ctca ) nellindividuazione delle stenosi coronariche signi cative ( riduzione del lume coronarico 50% ) confrontata con la coronarogra a convenzionale ( cag ) in base al valore di calcium score ( cacs )  . 
la prevalenza di malattia ostruttiva nella popolazione era del 51% ( 23 , 5% malattia mono - vasale ; 27 , 5% multi - vasale ; con aumento progressivo dal 17 , 9% al 94% nelle diverse classi di cacs )  . 
ctca is a reliable diagnostic modality , with high sensitivity and npv regardless of cacs . keywords ct coronary angiography conventional coronary angiography diagnostic accuracy coronary artery calcium score registry ha mostrato un valore predittivo positivo peggiore ( 76% 77% ) nelle classi di cacs basso ( 110 / 11100 )  . 
la ctca una metodica diagnostica af dabile con elevata sensibilit e valore predittivo negativo indipendentemente dal valore di cacs . parole chiave angiogra a coronarica tc angiogra a coronarica convenzionale accuratezza diagnostica calcio coronarico registro introduction introduzione in the diagnosis and exclusion of coronary artery disease tomography coronary angiography ( cad ) , computed ( ctca ) is an accurate and robust modality that can be performed with low doses of radiation [ 115 ]  . 
 one limitation in evaluating and interpreting coronary artery stenosis with ctca is linked to the presence and quantity of coronary calcium as measured with the coronary artery calcium score ( cacs ) [ 5 , 7 , 1722 ]  . 
however , some studies have shown that a progressively higher cacs tends to reduce the speci city and positive predictive value ( ppv ) rather than cause an overall deterioration in diagnostic performance [ 5 , 7 , 1722 ]  . this report presents a patient population drawn from a multicentre ctca registry and focuses on diagnostic accuracy with conventional coronary angiography ( cag ) as reference . 
 materials and methods registry langiogra a coronarica con tomogra a computerizzata ( ctca ) una indagine accurata e robusta per la diagnosi e lesclusione della malattia coronarica ( cad ) che pu essere effettuata con basse dosi di radiazioni ionizzanti [ 115 ]  . 
 uno dei limiti nella valutazione e nella interpretazione delle stenosi coronariche mediante ctca legato alla presenza ed alla quantit di calcio coronarico ( cacs ) [ 5 , 7 , 1722 ]  . 
parte della letteratura ha cercato di de nire dei valori di cacs al di sopra dei quali non sarebbe opportuno effettuare lo studio angiogra co coronarico mediante tomogra a computerizzata ( tc ) , tuttavia , in alcune casistiche emerge come in realt un cacs progressivamente pi elevato determina una riduzione della speci cit e del valore predittivo positivo pi che un deterioramento globale della performance diagnostica [ 5 , 7 , 1722 ]  . in questo lavoro presentiamo una casistica derivante da un registro multicentrico di ctca focalizzato sullaccuratezza diagnostica della ctca messa a confronto con la coronarogra a convenzionale ( cag ) con particolare attenzione allanalisi della performance diagnostica a seconda del valore di cacs . 
 the participating centres are characterised by : > 300 ctca examinations performed per year ; on - site or directly accessible catheterisation laboratory ; experience of the operators materiali e metodi registro i dati presentati derivano da un registro multicentrico [ 2 ]  . 
i 1002 radiol med ( 2011 ) 116 : 10001013 > 5 years ; ability to maintain a detailed longitudinal prospective database of all the characteristics of patients undergoing ctca ; homogeneous scan protocols and image analysis ( pharmacological preparation of the patient , scan / reconstruction parameters and contrast agent administration ) ; systematic evaluation of the examinations by at least two expert operators in 90% of cases ( double reading )  . study population from may 2004 to june 2010 , 1 , 500 consecutive patients ( 928 men , 572 women ; mean age 58.212.5 years ; median age 59 years ; range 2186 years ; table 1 ) who were candidates for cag were studied with ctca to verify the presence and extension of cad [ 2 ]  . 
with regard to the use of dedicated convolution software , standard lters ( mediumsmooth ) were generally used with cacs < 100 , whereas higher convolution lters ( mediumsharp / sharp ) were used with cacs 100 . 
the ethics committee approved the study , and all patients provided informed consent . statistical analysis data are reported as prevalence , mean and standard deviacentri partecipanti sono caratterizzati da : volume di esami ctca > 300 / anno ; presenza di laboratorio di emodinamica in loco o direttamente afferente ; esperienza degli operatori > 5 anni ; capacit di mantenere un database dettagliato longitudinale prospettico di tutte le caratteristiche dei pazienti che effettuano ctca ; impostazione omogenea dei protocolli di scansione ed analisi delle immagini ( preparazione farmacologica del paziente , parametri scansione / ricostruzione e somministrazione del mezzo di contrasto ) ; valutazione sistematica delle indagini da parte di almeno due operatori esperti nel 90% dei casi ( doppia lettura )  . popolazione studiata da maggio 2004 a giugno 2010 , sono stati studiati mediante ctca 1500 pazienti consecutivi ( 928 di sesso maschile , 572 di sesso femminile , et media 58 , 212 , 5 anni ; mediana 59 anni ; range 2186 anni ) ( tabella 1 ) gi candidati allesecuzione di una cag allo scopo di determinare la presenza e lestensione della malattia coronarica [ 2 ]  . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . analisi statistica i dati sono presentati come prevalenze , medie e deviazioni standard . 
la performance diagnostica dellangiogra a coronarica mediante ctca nellindividuazione delle lesioni aterosclerotiche coronariche signi cative , utilizzando la cag come tecnica di riferimento , di seguito riportata come sensibilit , speci cit , valore predittivo positivo ( vpp ) e negativo ( vpn ) con intervalli di con denza ( ic ) al 95% calcolati con espansione binomiale . 
tutte le statistiche sono state eseguite per la popolazione totale e per i sottogruppi con differente cacs ( secondo agatston ) classi cati come segue [ 22 ] : cacs 0 ; cacs 110 ; cacs 11100 ; cacs 101400 ; cacs 401 1000 ; cacs > 1000 . 
the diagnostic performance of ctca in identifying signi cant coronary artery atherosclerotic lesions , with cag used as the reference technique , is reported in terms of sensitivity , speci city , ppv and negative predic1004 radiol med ( 2011 ) 116 : 10001013 tive value ( npv ) , with 95% con dence intervals ( ci ) calculated with binomial expansion . 
all statistics were calculated for the total population and for the classes with different cacs ( agatston score ) , which were classi ed as follows [ 22 ] : 0 ; 110 ; 11100 ; 101400 ; 4011 , 000 ; > 1 , 000 . 
nel gruppo con cacs > 1000 la prevalenza di cad ostruttiva si riduce al 64% come verosimile esito del bias di selezione dei pazienti ( ossia vengono inviati a ctca maggiormente i pazienti nei quali esistono dubbi sulla effettiva presenza di cad ostruttiva )  . 
la speci cit ha mostrato valori meno elevati nei gruppi con cacs > 1000 ( speci cit = 87% ) , ed il valore predittivo positivo ha mostrato valori meno elevati nei gruppi con cacs > 1000 ( vpp = 53% )  . 
la speci cit ha mostrato valori meno elevati nei gruppi con cacs 4011000 ( 77% ) , mentre il valore predittivo positivo ha mostrato valori meno elevati nei gruppi con cacs 0 ( 76% ) e cacs 110 ( 78% )  . 
the literature published to date provides indications that are partly in con ict regarding the use of the total calcium score ( agatston ) for de ning the threshold above which angiographic scans would be inadvisable [ 5 , 7 , 1722 , 2831 ]  . 
on the one hand , to limit the number of false positives , there is an attempt to provide a threshold above which ctca is not recommended [ 5 , 7 , 1722 , 2831 ] , whereas on the other hand , ctca is generally performed to rule out disease following an inconclusive stress test [ 16 , 32 ]  . 
le coronarie sono , infatti , vasi di piccole dimensioni ed il blooming delle calci cazioni ha un impatto maggiore rispetto ad altri vasi di maggiori dimensioni ( per esempio , arterie carotidi interne )  . il ruolo clinico del cacs consiste nella strati cazione del rischio di cad ostruttiva e di eventi coronarici in maniera incrementale , caratteristica non sempre rispettata dai metodi convenzionali come lo score di framigham [ 2427 ]  . 
 la letteratura pubblicata no ad oggi fornisce indicazioni in parte contrastanti sullutilizzo del valore di calcio totale secondo agatston per de nire la soglia oltre la quale non sarebbe opportuno procedere alla scansione angiogra ca [ 5 , 7 , 1722 , 2831 ]  . 
da un lato si vorrebbe fornire una soglia oltre la quale la ctca non andrebbe fatta per limitare il numero di falsi positivi [ 5 , 7 , 1722 , 2831 ] , dallaltro bisogna considerare che la ctca viene generalmente effettuata come test per esclusione di malattia che segue un test provocativo dubbio [ 16 , 32 ]  . 
bisogna considerare , tuttavia , che laumento di cacs si associa allaumento della prevalenza di malattia coronarica ostruttiva e ad un aumento della severit ed estensione della coronaropatia ( vale a dire , una maggiore prevalenza di coronaropatia ostruttiva multi - vasale )  . 
with regard to obstructive disease , a higher prevalence of three - vessel disease can be seen in the extreme cacs classes , which re ects , on the one hand , the selection bias of the patients sent for computed tomography coronary angiography ( cacs < 10 ) and , on the other hand , the natural history of the disease ( cacs > 400 )  . 
focalizzando la valutazione sulla malattia ostruttiva , si osserva una prevalenza di malattia tri - vasale pi elevata nelle classi estreme di cacs che ri ette da un lato il bias di selezione dei pazienti inviati a ctca ( cacs < 10 ) e dallaltro la storia naturale della malattia ( cacs > 400 )  . 
this effect partially attenuates the overestimation of obstructive cad by ctca when shifting from a per - segment to a per - patient analysis . the results of our study based on a large population con rm these observations . 
the prevalence of obstructive cad is undoubtedly higher in patients with a high cacs , but ctca nonetheless is not an appropriate technique for establishing the presence and extent of ischaemia . 
even though the diquesto effetto , in parte , attenua la sovrastima della malattia coronarica ostruttiva da parte della ctca nel passaggio dallanalisi per segmento allanalisi per paziente . i risultati del nostro studio basati su una popolazione ampia confermano queste osservazioni . 
3 per - segment and per - patient diagnostic accuracy of coronary artery computed tomography ( ctca ) in the total population and in the coronary artery calcium score ( cacs ) classes . 
note the low positive predictive value ( ppv ) of the technique in the per - segment evaluation ( upper panel ) , which appears normalised in the per - patient evaluation ( lower panel )  . 
gra co a barre dellaccuratezza diagnostica per segmento e per paziente della angiogra a coronarica con tomogra a computerizzata ( ctca ) nella popolazione totale , e nelle classi di calcium score coronarico ( cacs )  . 
da notare il basso valore predittivo positivo della metodica nella valutazione per segmento ( pannello in alto ) che si normalizza nella valutazione per paziente ( pannello in basso )  . 
 nellanalisi per paziente il valore pi sfavorevole di valore predittivo positivo ( vpp ) si osserva nelle classi a basso cacs ( per esempio , cacs 110 / 11 100 )  . 
on the other hand , in line with the current recommendations , the patient who undergoes ctca will also have been evaluated with at least one other imaging test , and the examination would aim to rule out disease given its npv [ 16 ]  . 
 mance diagnostica della ctca viene in parte deteriorata nelle classi ad elevato cacs , in particolare in termini di speci cit e valore predittivo positivo , i valori rimangono in un range accettabile ( speci cit > 77% e vpp > 76% ) per lapplicabilit clinica della metodica in una popolazione adeguatamente selezionata . i valori quozienti di probabilit ( lr + e lr - ) sono ottimali nei gruppi con cacs basso ed questo un ulteriore punto di forza della metodica che pu essere sfruttato nellambito degli algoritmi diagnostici decisionali clinici . 
daltra parte , seguendo le attuali raccomandazioni , il paziente che arriva a ctca dovrebbe essere stato valutato con almeno un altro test strumentale e lindagine si porrebbe come strumento di esclusione per il suo valore predittivo negativo [ 16 ]  . 
4 likelihood ratios ( lr ) show how weighting of the diagnostic accuracy by disease prevalence produces a reduction in the lr + and lr when going from a per - segment analysis to a per - patient analysis . 
il gra co a barre dei quozienti di probabilit ( lr ) dimostra come la pesatura dellaccuratezza diagnostica per la prevalenza di malattia determini una riduzione del lr + e del lrnel passaggio dalla valutazione per - segmento a quella per - paziente . 
i valori migliori di lr + si ottengono nella popolazione con calcium score coronarico ( cacs ) 0 sia nella valutazione per segmento che in quella per paziente . limitations to the study limiti allo studio our case series reports data recorded in the period when the most modern dose - reduction systems were not available [ 912 ]  . 
tuttavia , questa anche la forza delle informazioni presentate in quanto molto pi realistiche rispetto agli studi convenzionali in condizioni ottimali ( per esempio , pazienti ben selezionati , possibilit di valutazione delle immagini estesa nel tempo , ecc )  . conclusions conclusioni data in our registry demonstrate that ctca is a robust and reliable morphological modality for evaluating obstructive cad in the population , regardless of cacs . 
our data therefore suggest that the introduction of cacs thresholds i dati del nostro registro dimostrano che la ctca una metodica morfologica per la valutazione dellaterosclerosi coronarica ostruttiva robusta ed af dabile nella popolazione indipendentemente dalla quantit di cacs . 
computed tomography coronary angiography ( ctca ) is positive , the probability that a patient effectively has coronary stenosis 50% increases signi cantly , even if the pretest probability is low or very low ( range 020% )  . 
il gra co mostra le probabilit condizionali nella popolazione totale e nelle varie classi di calcium score coronarico ( cacs ) , utilizzando i valori di accuratezza diagnostica e la prevalenza di malattia per paziente . 
 per un test positivo aumenta signicativamente la probabilit che un paziente sia effettivamente portatore di una stenosi coronarica 50% anche con probabilit pre - test bassa o molto bassa ( range 0%20% )  . 
the intrinsic design of the registry tends to better re ect clinical practice and it characteristic variability . non sembra quindi opportuno introdurre soglie di cacs oltre le quali non effettuare la scansione angiogra ca . 
stolzmann p , leschka s , scheffel h et al ( 2008 ) dual - source ct in step - andshoot mode : noninvasive coronary angiography with low radiation dose . 
scheffel h , alkadhi h , leschka s et al ( 2008 ) low - dose ct coronary angiography in the step - and - shoot mode : diagnostic performance . 
achenbach s , marwan m , ropers d et al ( 2010 ) coronary computed tomography angiography with a consistent dose below 1 msv using prospectively electrocardiogramtriggered high - pitch spiral acquisition . 
maffei e , martini c , de crescenzo s et al ( 2010 ) low dose ct of the heart : a quantum leap into a new era of cardiovascular imaging . 
hendel rc , patel mr , kramer cm et al ( 2006 ) accf / acr / scct / scmr / asnc / nasci / scai / sir 2006 appropriateness criteria for cardiac computed tomography and cardiac magnetic resonance imaging : a report of the american college of cardiology foundation quality strategic directions committee appropriateness criteria working group , american college of radiology , society of cardiovascular computed tomography , society for cardiovascular magnetic resonance , american society of nuclear cardiology , north american society for cardiac imaging , society for cardiovascular angiography and interventions , and society of interventional radiology . 
cademartiri f , mollet nr , lemos pa et al ( 2005 ) impact of coronary calcium score on diagnostic accuracy for the detection of signi cant coronary stenosis with multislice computed tomography angiography . 
cornalba1 1dipartimento di radiologia diagnostica ed interventistica , universit degli studi di milano , ospedale san paolo , via di rudin 8 , 20142 milano , italy 2unit di radiologia , irccs policlinico san donato , piazza e . 
malan , san donato milanese , milano , italy 3dipartimento di scienze medico - chirurgiche , universit degli studi di milano , via festa del perdono 7 , milano , italy correspondence to : s . 
forty - nine patients ( 30 men , 19 women ; age range 3082 years ) underwent abdominal contrast - enhanced msct and 3d - us performed with a 3.5 - mhz 3d / 4d convex - array probe . 
analysis of variability per patient between msct and 3d - us showed a bias of 19 ml , a cor of 47 ml and an accuracy of 78% , with an average 3d - us underestimation of 19 ml ( 9% )  . 
three - dimensional us is a valuable technique for monitoring renal volume , whereas msct may be reserved for assessing renal anatomy and relationships with neighbouring organs . keywords ultrasound 3dmsct renal volume riassunto obiettivo . 
quarantanove pazienti ( 30 maschi ; 19 donne ; et 3082 ) , sono stati sottoposti a tcms delladdome con somministrazione di mezzo di contrasto ( mdc ) ed a ecogra a con sonda convex volumetrica 3d / 4d con tecnologia elettromeccanica . 
la volumetria 3d rappresenta una valida metodica nel monitoraggio del volume renale nel tempo , mentre la tcms pu essere riservata ai casi in cui occorra una valutazione panoramica dellanatomia renale e dei rapporti con gli organi circostanti . parole chiave ecotomogra a 3d volumetria renale tcms 1096 introduction determining renal volume is important in numerous clinical situations : during treatment for renal failure , in the followup after renal transplant [ 1 , 2 ] , in the evaluation of renal artery stenoses [ 3 ] , in renovascular hypertension [ 4 ] , in recurrent urinary tract infections [ 5 ] , in the follow - up after unilateral nephrectomy [ 5 ] , in young patients with vesicoureteral re ux [ 6 , 7 ]  . 
given that some treatment decisions are based on serial measurements of renal volume , which provide information about disease progression , stability or regression or about the onset of complications , an accurate and noninvasive method is needed that preferably does not use ionising radiation or contrast material [ 8 ]  . ever since ultrasound ( us ) was described as a useful modality for calculating renal volume [ 4 , 5 , 9 , 10 ] , two techniques have been suggested : measurement of the largest renal diameter [ 10 , 11 ] , and estimation of renal volume based on the ellipsoid formula [ 4 , 5 ]  . 
however , it has been reported that these techniques tend to underestimate renal volume , as measurement of the largest diameter is poorly reproducible and does not correlate with true kidney size [ 4 , 5 ] , whereas the ellipsoid formula fails to take into account the variability of the shape of the kidney [ 5 , 10 ]  . 
in addition , these methods are highly operator dependent , as they involve manually performing the measurements needed to determine renal volume [ 8 ]  . multislice computed tomography ( msct ) [ 12 ] and magnetic resonance imaging ( mri ) , with their ability to analyse volumetric data , are more accurate in determining the volume of abdominal organs [ 8 , 1317 ]  . 
the introduction of 3d - us imaging with dedicated probes allowing direct and automatic breath - hold acquisition of kidney sections reconstructed in the axial , sagittal and coronal planes [ 8 , 1320 ] has opened up new possibilities , in part thanks to limited costs , noninvasiveness , absence of ionising radiation and consequently contraindications . 
 the purpose of our study was to assess the accuracy of 3d - us with a dedicated volumetric probe for determining renal volume in comparison with msct , which is considered the standard of reference . materials and methods population radiol med ( 2011 ) 116 : 10951104 introduzione la determinazione del volume renale assume un ruolo importante in numerose situazioni cliniche : in corso di trattamento dei pazienti con insuf cienza renale , nel follow - up dei pazienti con trapianto renale [ 1 , 2 ] , nella valutazione delle stenosi delle arterie renali [ 3 ] , nellipertensione renovascolare [ 4 ] , nelle infezioni urinarie ricorrenti [ 5 ] , nella valutazione dei pazienti dopo nefrectomia monolaterale [ 5 ] e nei giovani pazienti con re usso vescico - ureterale [ 6 , 7 ]  . 
 dal momento che alcune decisioni terapeutiche possono derivare da misurazioni seriali del volume renale , le quali forniscono informazioni sulla progressione , stabilit o regressione della patologia esistente o sulla insorgenza di eventuali complicanze , si rende utile una metodica che sia accurata , non invasiva e che preferibilmente non utilizzi radiazione ionizzanti o mezzo di contrasto [ 8 ]  . 
 da quando lecogra a stata descritta come metodica utilizzabile per la valutazione del volume renale [ 4 , 5 , 9 , 10 ] sono state proposte due tecniche : la misura del diametro massimo renale [ 10 , 11 ] e la stima del volume renale mediante la formula dellellissoide [ 4 , 5 ]  . 
da quanto riportato in letteratura , con queste differenti tecniche il volume renale appare sottostimato poich la misura del diametro massimo poco riproducibile e non correlata con le reali dimensioni renali [ 4 , 5 ] , mentre la formula ellissoidale non tiene conto della variabilit della forma del rene [ 5 , 10 ]  . 
inoltre , queste tecniche con acquisizione manuale delle varie misure necessarie alla determinazione del volume sono molto operatore dipendenti [ 8 ]  . attualmente la possibilit da parte della tomogra a computerizzata multistrato ( tcms ) [ 12 ] e della risonanza magnetica ( rm ) di analizzare dati volumetrici rende queste tecniche pi accurate nella valutazione dei volumi dei vari organi addominali [ 8 , 1317 ]  . 
la comparsa nella pratica clinica della ecotomogra a tridimensionale ( eco 3d ) con sonda dedicata che permette , durante una singola apnea , lacquisizione diretta ed automatica di sezioni del rene ricostruite nei piani assiali , sagittali e coronali [ 8 , 1320 ] ha aperto una nuova possibilit anche in ragione dei costi contenuti , della non invasivit , dellassenza di radiazioni ionizzanti e , quindi , della mancanza sostanziale di controindicazioni . 
 lo scopo di questo studio stato valutare laccuratezza dellecotomogra a 3d nella misurazione del volume renale utilizzando una sonda volumetrica dedicata e considerando la tcms come standard di riferimento . our study was conducted on 49 consecutive patients ( 30 men and 19 women , age range 3082 years ; mean age 68 years ) who underwent abdominal msct for different clinical indications . 
all patients enrolled in the study were contacted after the ct examination , and informed consent for the 3d - us study was obtained in all cases . acquisition protocol and image analysis all patients had undergone abdominal ct , with scans extending from the upper pole of the kidney to the bladder base ( 120 kvp , automatic mas modulation , 5 - mm slice thickness )  . 
all examinations were performed with a 64 - slice lightspeed vct scanner ( general electric medical system , milwaukee , wi , usa ) following automatic administration of 90110 ml of iomeprol ( iomeron ) at 370 mg / ml iodine concentration . 
 the probe had 192 elements on a single matrix , 40.5 mm radius of curvature , 68 eld of view , 8580 acquisition volume , upper frame rate 35 f / s . 
to understand the cor , consider the following scenario : let us suppose that a patient undergoes ct with renal volume determination and that 6 months later , the determination is repeated with us instead of ct . 
abbiamo deciso di reclutare nello studio solo pazienti con anamnesi negativa per patologia renale allo scopo di testare la metodica su una popolazione priva di alterazioni patologiche che potessero essere considerate un fattore condizionante la misurazione . 
tutti i pazienti arruolati nello studio sono stati contattati al termine della loro indagine tc ed stato acquisito consenso informato allesecuzione dellindagine ecogra ca . protocollo di acquisizione ed analisi di immagine tutti i pazienti avevano effettuato lindagine tc delladdome con scansioni estese dal polo renale superiore al pavimento vescicale ( 120 kvp , modulazione automatica dei mas , spessore di strato 5 mm )  . 
tutte le indagini sono state effettuate con tomografo lightspeed vct 64 strati ( general electric medical system , milwaukee , wi , usa ) e con somministrazione automatica da 90 a 110 ml di iomeron 370 mg / ml . 
tutte le indagini sono state eseguite con un ecotomografo logic q9 ( general electric medical system , milwaukee , wi , usa ) mediante utilizzo di sonda convex volumetrica 3d / 4d con tecnologia elettromeccanica per le acquisizioni volumetriche dotata di banda da 1 , 55 mhz . 
la sonda presenta 192 elementi su singola matrice di elementi , raggio di curvatura 40 , 5 mm , apertura campo di vista 68 , volume di acquisizioni 8580 , frame rate superiore a 35 f / s . 
furthermore , we measured the ratio between this coef cient and the mean renal volume and its complement to 1 ; considering ct as the standard of reference , the value obtained represents the accuracy of 3d - us . 
la variabilit tra le due metodiche di misura stata stimata col metodo bland - altman ed stata riportata in termini di bias e coef ciente di ripetibilit ( cor )  . 
supponiamo che un paziente esegua una tomogra a computerizzata con misura del volume renale e che , dopo un intervallo di sei mesi , ripeta tale misura con ecogra a anzich con tomogra a computerizzata . 
inoltre , abbiamo calcolato il rapporto tra tale coef ciente e il volume renale medio e il suo complemento a 1 : considerando la tc come standard di riferimento , il valore cos ottenuto rappresenta radiol med ( 2011 ) 116 : 10951104 1099 fig . 
analysis of variability per kidney yielded the following results : bias 9 ml , cor 34 ml and accuracy 80% for the right kidney ( n = 48 ) ; 29 ml , 50 ml and 80% , respectively , for the radiol med ( 2011 ) 116 : 10951104 laccuratezza della ecotomogra a 3d . 
inoltre , stata valutata la correlazione bivariata tra lindice di massa corporea ( imc ) , et del paziente , peso e volume medio bilaterale mediante il coef ciente di correlazione di spearman . 
 tutti i calcoli sono stati eseguiti con spss v.17 ( spss inc , chicago , il , usa ) e valori di p < 0 , 05 sono stati considerati come signi cativi . risultati popolazione i dati demogra ci del campione analizzato sono indicati in tabella 1 . 
i dati di 5 reni ( 2 reni di destra e 3 reni di sinistra ) di 5 pazienti diversi sono stati esclusi perch presentano misure estreme , palesemente outlier , distribuite in modo casuale e , pertanto , non costituenti un possibile bias . 
non si osservata alcuna correlazione signi cativa tra limc , et del paziente , peso e volume renale . discussione la stima del volume renale rappresenta un parametro clinico importante nella valutazione della riserva funzionale renale , ed generalmente alla base di alcune decisioni terapeutiche . 
misurazioni seriate del volume renale possono fornire informazioni sulla funzione di ltrazione dellorgano ed assumono particolare importanza nel corso del follow - up per stabilire leventuale stabilit o la progressione della malattia [ 8 ]  . 
 dallanalisi dei dati presenti in letteratura mediante valutazione ecogra ca con la tecnica dellellissoide il volume renale nel maschio compreso tra 110 e 190 ml e nella donna tra 90 e 150 ml [ 21 ]  . 
no signi cant correlation was observed between bmi , age , weight and renal volume . discussion determining renal volume is an important clinical parameter in assessing renal functional reserve and is generally the basis for several treatment decisions . 
serial measurements of renal volume can provide information on renal metodica adeguata per la misurazione del volume renale utilizzando la formula dellellissoide , nonostante sia emerso dal confronto con altre tecniche che tale metodica determina una sottostima del volume compreso tra il 3% ed il 44% [ 9 , 11 , 18 ]  . 
possibili spiegazioni per la scarsa accuratezza della volumetria renale possono essere le seguenti : linadeguata visualizzazione dellorgano dovuta alla presenza di interposto gas intestinale o strutture ossee ( coste ) che limitano la nestra acustica , la non corretta misurazione manuale dei diametri renali , la presenza fig . 
4 gra co di bland - altman per il confronto tra tomogra a computerizzata ed ecotomogra a 3d . 1102 radiol med ( 2011 ) 116 : 10951104 ltration and are especially important during patient followup to assess disease stability or progression [ 8 ]  . the literature regarding sonographic determination of renal volume with the ellipsoid formula indicates renal volumes of 110190 ml in men and 90150 ml in women [ 21 ]  . 
on ct , the mean volume is 193 ml for men and 157 ml for women [ 8 ] , whereas on mri , it ranges from 132 to 276 ml in men and from 87 to 223 ml in women [ 8 ]  . several published studies indicate that us is an adequate technique for determining renal volume using the ellipsoid formula , even though comparison with other modalities has revealed an underestimation of 344% [ 9 , 11 , 18 ]  . 
the reasons for the low us accuracy in renal volume determination may include inadequate visualisation of the organ due to interposed bowel gas or bony structures ( ribs ) limiting the acoustic window , incorrect manual measurements of renal diameters , presence of respiratory artefacts and patient body habitus [ 20 ]  . 
despite this known underestimation , us has been considered adequate for clinical needs given that absolute renal volume is not as important as its variations over time . according to the literature , the 3d technique appears to produce an underestimation of renal volume [ 19 ] , even though this underestimation is lower than that of the ellipsoid formula [ 19 ]  . 
in our study conducted on 49 patients and a total of 98 kidneys , 3d - us revealed higher values compared with msct in 11 cases only ( 11% ) , with a mean difference of 17 ml ; in the remaining 87 cases ( 89% ) , msct yielded higher values ( mean difference 24 ml )  . 
this resulted in 78% accuracy and an average underestimation of 19 ml , which , in relation to the mean values of msct ( 210 ml ) , corresponds to a mean underestimation of 9% , which is consistent with previous ndings [ 9 , 1118 ]  . 
these data are also con rmed by direct comparison between mean values of renal volume measured at msct ( 210 ml ) and those measured at 3d - us ( 192 ml ) : the wilcoxon test yielded a p value < 0.001. the underestimation observed in our study must be understood as a mean value : in clinical practice , this underestimation may be compensated for by adding 9% to the renal volume obtained at 3d - us . 
our study showed cor values of 47 ml , which implies that a difference < 47 ml between the volumes measured with the two techniques ( rst examination and follow - up ) in the individual patient cannot be necessarily interpreted as progression of the clinical condition . the analysis per kidney did not reveal any signi cant difference in accuracy with regard to determining right and left renal volumes : in fact , although the mean underestimation was 9 ml and 29 ml , respectively , in terms of accuracy , we obtained values of 80% in both kidneys . 
tuttavia , nonostante il riconoscimento di questa sottostima , la metodica ecogra ca stata considerata comunque adeguata alle necessit cliniche in quanto non risulta fondamentale il valore assoluto del volume renale ma la sua variazione nel tempo . da quanto noto in letteratura , anche la tecnica 3d appare caratterizzata da una sottostima del valore del volume renale [ 19 ] , ma tale sottostima risulta inferiore a quella che si veri ca con la tecnica dellellisoide [ 19 ]  . 
 ne risultata unaccuratezza del 78% ed una sottostima media di 19 ml che , relativamente al valore medio misurato alla tcms ( 210 ml ) , corrisponde ad una sottostima media del 9% , compatibile con quanto riportato in letteratura [ 9 , 1118 ]  . 
questo dato , inoltre , confermato dal confronto diretto tra la media del volume renale misurato alla tcms ( 210 ml ) e quello misurato alla ecotomogra a 3d ( 192 ml ) : il test di wilcoxon ha fornito un valore di p < 0 , 001 . la sottostima osservata nel nostro studio deve essere intesa come un valore medio : nella pratica clinica , questa sottostima pu essere compensata sommando al volume renale ottenuto alla ecotomogra a 3d il 9% del suo valore . 
dal nostro studio risultato cor = 47 ml , ovvero , nel singolo paziente , differenze tra il volume misurato con le due metodiche ( prima indagine e follow - up ) inferiori a 47 ml non possono essere interpretate necessariamente come progressione dello status clinico del paziente . allanalisi per singolo rene , non emersa una sostanziale differenza di accuratezza nella valutazione del rene destro e del rene sinistro : infatti , sebbene la sottostima media sia risultata di 9 ml e 29 ml , rispettivamente , in termini di accuratezza abbiamo ottenuto un valore pari all80% in entrambi i reni . 
tuttavia , la differenza tra il volume del rene destro misurato alla tcms ( 174 ml ) e quello misurato alla ecotomogra a 3d ( 165 ml ) altamente signi cativa ( p < 0 , 001 ) ; analogamente per il rene sinistro ( 250 ml versus 220 ml , p < 0 , 001 )  . 
lastly , with both techniques , we observed a signi cant difference between mean right and left renal volume ( p < 0.001 , table 2 )  . even assuming that msct [ 22 , 23 ] and mri [ 24 , 25 ] provide an accurate and reproducible estimation of renal volume that is not in uenced by geometric factors [ 8 ] , it should nonetheless be considered that these modalities have some limitations , such as limited availability of equipment , cost of the single examination , long imaging times or use restrictions for mri and use of ionising radiation for ct . 
as a result , us represents a valuable alternative due to the absence of contraindications , its fast examination times and its limited cost per examination , which contribute to making it an ideal , frequently repeatable , examination . 
furthermore , the possibility of using a dedicated probe to obtain the scans needed for volumetric measurement during a single breathhold reduces the incidence of respiratory artefacts [ 8 , 1317 ]  . 
finally , the possibility of obtaining automatic volumetric scans reduces operator dependence , thus improving the potential for reproducibility of the technique . accurata e riproducibile del volume renale non in uenzata da fattori geometrici [ 8 ] , bisogna tuttavia considerare che queste metodiche presentano alcune limitazioni , a partire dalla limitata disponibilit delle apparecchiature ai costi del singolo esame , dalla durata dellesame per la rm alla impossibilit di eseguirla in certe condizioni , dallutilizzo delle radiazioni ionizzanti per la tc . 
tali limitazioni risultano ulteriormente accentuate in quanto lindagine deve essere necessariamente ripetuta pi volte nel tempo nel corso dei vari follow - up per ottenere un monitoraggio della patologia adeguato alle necessit . 
la tecnica ecogra ca conseguentemente rappresenta una valida alternativa per lassenza di controindicazioni , per la velocit di esecuzione e per i costi contenuti per singolo esame , che la rendono ottimale come indagine da ripetere frequentemente nel corso del tempo nello stesso soggetto . 
la possibilit di utilizzare una sonda dedicata che effettui in ununica apnea le scansioni necessarie alla misurazione volumetrica consente inoltre di ridurre gli artefatti respiratori [ 8 , 1317 ]  . 
la possibilit di ottenere la scansione volumetrica in modo automatico permette in ne di ridurre la componente di dipendenza dalloperatore migliorando le potenzialit di riproducibilit della metodica . conclusioni conclusions bearing in mind the almost systematic underestimation 9% , 3d volumetry represents a valuable technique for renal volume determination . 
renal volume determination with msct or mri can be reserved for cases requiring a more precise and accurate assessment and a panoramic overview of the anatomy of the kidney and its relationships with neighbouring organs . tenendo conto della sottostima pressoch sistematica del 9% del volume renale , la volumetria 3d rappresenta una valida metodica nella stima del volume renale . 
fugazzola1 1universit dellinsubria , dipartimento di diagnostica per immagini , ospedale di circolo fondazione macchi , viale borri 57 , 21100 varese , italy 2cattedra di radiologia , dipartimento di scienze per la salute , universit del molise , campobasso , italy correspondence to : g . 
la rfa con effetto citoriduttivo , in pazienti con tumore della mammella rappresenta unef cace metodica di trattamento , in aggiunta alla chemioterapia sistemica e allormonoterapia , delle metastasi epatiche . 
 rfa rappresenta una valida alternativa alla chirurgia nel trattamento loco - regionale delle metastasi da tumore mammario . keywords radiofrequency thermal ablation ( rfa ) breast cancer metastasis parole chiave termoablazione con radiofrequenza ( rfa ) tumore della mammella metastatico 1060 introduction liver metastases have been identi ed at autopsy in as many as 5575% of patients with breast cancer [ 1 ]  . 
 a small group of patients with metastasis con ned to the liver ( 512% ) appear to have an improved prognosis after hepatic resection , and association with hormonal or chemotherapy can be a more effective treatment option [ 36 ]  . in the last 10 years , radiofrequency thermal ablation ( rfa ) has gained wide acceptance for treating patients with nonresectable primary and metastatic liver tumours . 
 rfa has been demonstrated to be an effective cytoreductive strategy for a variety of metastatic liver malignancies , with few side effects and little disruption of patients life [ 711 ]  . 
 the aim of this study was to evaluate the effectiveness of rfa in patients with liver metastasis from breast cancer and its impact on survival . materials and methods between november 2003 and october 2007 , 13 female patients ( age range 3682 years ; median 54.5 years ) underwent rfa at our institution to treat 21 liver metastases from breast cancer . 
inclusion criteria were : ( 1 ) up to three metastases with diameter 7 cm ; ( 2 ) no evidence of extrahepatic disease or stable extrahepatic disease for at least 3 months ; ( 3 ) platelet count > 35 103 / l ; ( 4 ) international normalised ratio ( inr ) < 1.5. 
patient characteristics are listed in tables 1 and 2 . diagnostic workup included contrast - enhanced abdominal computed tomography ( ct ) scan and a biopsy under ultrasound ( us ) guidance . 
all patients were treated with prophylactic antibiotic therapy consisting of cefazolin 1 g iv every 8 h starting 3 days before the procedure and continuing up to 2 days after it . radiol med ( 2011 ) 116 : 10591066 introduzione il 55%75% delle pazienti affette da tumore mammario presenta allesame autoptico metastasi epatiche [ 1 ]  . 
la chemioterapia rimane lopzione terapeutica di scelta per le pazienti con malattia metastatica diffusa , mentre nelle pazienti ( 5%12% ) [ 2 ] con localizzazione metastatica limitata al fegato , si osservata una prognosi migliore dopo resezione epatica in associazione a chemioterapia e ormonoterapia [ 36 ]  . nellultimo decennio , termoablazione mediante radiofrequenza ( rfa ) si dimostrata una terapia diffusamente accettata per il trattamento dei tumori e utilizzata sui tumori epatici metastatici : ha un ef cace potere citoriduttivo con pochi effetti collaterali ed un impatto positivo sulla qualit di vita delle pazienti [ 711 ]  . 
lobiettivo del nostro studio quello di valutare lef cacia della rfa epatica in pazienti affette da metastasi epatiche da carcinoma mammario in chemioterapia o ormonoterapia e il suo impatto sulla sopravvivenza . materiali e metodi tra novembre 2003 e ottobre 2007 , presso il nostro centro , 13 pazienti ( et 3682 anni , mediana 54 , 5 anni ) sono state sottoposte a terapia ablativa tramite radiofrequenza per il trattamento di 21 metastasi epatiche secondarie a tumore mammario . 
i criteri di inclusione nello studio sono stati : limite di 3 metastasi con diametro massimo inferiore o uguale a 7 cm ; nessuna evidenza di malattia extraepatica o malattia extraepatica stabile da almeno 3 mesi ; conta piastrinica > 35103 / l ; international normalized ratio ( inr ) < 1 , 5 . 
prima del trattamento con rfa , 6 / 13 pazienti sono state sottoposte a terapia chemioterapica , 6 / 13 a terapia ormonale e 1 / 13 sia a terapia sia chemioterapica che ormonale . 
le caratteristiche delle pazienti sono elencate nelle tabelle 1 e 2 . le indagini diagnostiche comprendono una tomogra a computerizzata ( tc ) addominale ( aquilion 64 , toshiba ) con mezzo di contrasto e una biopsia sotto guida ecogra ca ( iu22 , philips )  . 
ablations were performed using la procedura ablativa stata condotta in sedazione profonda , in accordo con le linee guida della monitored anaesthesia care : alle pazienti sono stati somministrati propofol ( 50120 mg ) , fentanyl ( 13 mg ) e midazolam ( 13 mg ) ; nella sede dingresso dellago stata effettuata unanestesia locale con lidocaina 1% . 
the choice of electrode size was determined in relation to tumour dimensions , and the safety margin was 5 mlesions with a diameter 3 cm were treated with two or more overlapping ablation treatments , up to a maximum of four for the largest lesion . 
technique effectiveness was evaluated by contrast - enhanced ct at 1 month : complete ablation was considered when no enhancement was observed in the ablated tumour ; irregular or nodular peripheral contrast enhancement was considered as residual tumour [ 12 ]  . 
la dimensione degli elettrodi stata stabilita in relazione alla dimensione della lesione ed al margine di sicurezza di 5 mle lesioni con diametro superiore a 3 cm sono state trattate con 2 o pi trattamenti ablativi sovrapposti , no ad un massimo di 4 per la lesione con diametro maggiore . 
il follow - up stato effettuato mediante tc a 1 , 3 , 6 e 12 mesi . il successo tecnico stato de nito come il corretto posizionamento dellelettrodo durante la procedura . 
lef cacia tecnica stata valutata tramite tc con mezzo di contrasto effettuata ad un mese dallintervento : la mancanza di enhancement nellarea interessata della lesione ablata stata considerata segno di completa ablazione ; enhancement irregolare o periferico stato considerato come tumore residuo [ 12 ]  . 
il metodo di kaplan - meier stato usato per valutare il tasso di insorgenza della prima metaradiol med ( 2011 ) 116 : 10591066 1063 medcalc version 9.4.2.0 ( medcalc software , mariakerke , belgium ) was used for the analyses . results technical success was 100% , and no major or minor complications occurred at the end of the procedure . 
mean follow - up was 12.9 ( range 435 ) months ; at the last follow - up at 12 months , three patients had died for extrahepatic spread of disease , whereas ten were still alive . 
la durata media del follow - up stata di 12 , 9 mesi ( range 435 mesi ) ; allultimo follow - up a 12 mesi , 3 pazienti erano morte per diffusione extraepatica della malattia , mentre 10 erano ancora in vita . 
nella nostra casistica 7 / 21 lesioni in 7 / 13 pazienti sono aumentate dimensionalmente 7 , 18 , 19 e 38 mesi in ordine cronologico ; lintervallo libero da progressione di malattia stato in media di 16 , 6 mesi . 
il 50% della frequenza di comparsa si rileva a 18 mesi , e la curva scende a zero a 38 mesi . 1064 radiol med ( 2011 ) 116 : 10591066 fig . 
most patients are not suitable for surgery because of their poor general condition or the stage of disease . medical therapy for metastatic breast cancer consists of chemotherapy or endocrine therapy because even in the case of isolated metastases in one organ , diffuse tumour - cell dissemination exists . 
in determining technique effectiveness , size of the index tumour and proximity to larger branches of the hepatic and portal veins are also believed to be factors of donne affette da tumore della mammella svilupper metastasi epatiche . 
la resezione chirurgica talvolta associata alla chemioterapia rappresenta lopzione terapeutica di scelta in pazienti selezionate , con singola metastasi epatica e basso rischio chirurgico ; tuttavia solo nel 4%5% delle pazienti si evidenzia una sola metastasi epatica da tumore mammario . 
 la maggior parte delle pazienti non possono essere candidate ad un intervento chirurgico a causa delle loro condizioni generali e dello stato avanzato della malattia . la terapia farmacologia per il tumore della mammella metastatico consiste nella chemioterapia e nelle endocrinoterapia perch anche nel caso di singola lesione metastatica localizzata in un organo , il rischio di disseminazione delle cellule tumorali esiste ; in questo caso la sopravvivenza varia dai 3 ai 6 mesi , e raramente supera i 2 anni [ 17 , 18 ]  . 
attualmente la rfa rappresenta un trattamento alternativo nella gestione delle pazienti ad elevato rischio chirurgico e in quelli con patologia extra epatica stabile , che non sono candidati alla resezione chirurgica . 
la rfa il trattamento complementare di scelta ( in alternativa alla chirurgia ) alla terapia sistemica nelle metastasi epatiche e nei pazienti che hanno sviluppato malattia epatica dopo chemioterapia [ 15 ]  . 
 negli studi esaminati lef cacia tecnica varia dal 79% al radiol med ( 2011 ) 116 : 10591066 1065 greater importance than the site of origin of metastases [ 13 , 14 , 19 , 20 , 2326 ]  . 
 our high rate of technique effectiveness is most probably due to multiple overlapping ablation treatments in lesions with diameter 3 caccording to the literature , the best results in terms of local tumour control have been noted in patients with lesions < 4 cm in diameter . 
 [ 15 ] , rfa is used to reduce tumour bulk in conjunction with systemic therapy and is a relatively simple percutaneous technique demonstrated to be an effective cytoreductive strategy . 
 [ 21 ] recently reported that overall 1 - , 3and 5 - year survival rates after the rst rf ablation were 68% , 43% and 27% , respectively , and that overall 1 - , 3and 5 - year survival rates after diagnosis of the rst liver metastasis were 92% , 60% and 32% , respectively . 
more recently , in a series of 31 patients with isolated breast cancer and liver metastases treated with major liver resections and minor resections with or without rfa , vlastos et al . 
 [ 28 ] demonstrated a median survival of 63 months , overall 2and 5 - year survival rates of 86% and 61% , respectively , and 2and 5 - year diseasefree survival rates of 39% and 31% , respectively . 
nella determinazione dellef cacia tecnica concorrono diversi fattori tra cui le dimensioni del tumore e la vicinanza ai rami di maggior calibro delle vene epatiche e della vena porta [ 13 , 14 , 19 , 20 , 2326 ]  . lelevata ef cacia tecnica da noi ottenuta probabilmente legata ai multipli trattamenti termoablativi nelle pazienti con lesioni di dimensioni superiori ai 4 cm di diametro . 
va comunque sottolineato che i migliori risultati in termine di migliore controllo locale della malattia sono stati evidenziati , in accordo anche ai dati della letteratura , in pazienti con lesioni pi piccole di 4 cm di diametro . 
 [ 13 ] riportano in un follow - up di 444 mesi , un totale di 63% pazienti libere da malattia , tuttavia , in tale studio non sono presenti dati di sopravvivenza totale per cui una discussione e un confronto pi preciso con i nostri dati non realizzabile [ 13 ]  . 
 [ 21 ] hanno presentato una sopravvivenza a 1 , 3 , 5 anni dalla diagnosi di tumore della mammella del 68% , 43% e 27% , mentre una sopravvivenza a 1 , 3 , 5 anni dalla diagnosi di metastasi epatica del 92% , 60% e 32% rispettivamente [ 21 ]  . 
la rfa confrontata con la chirurgia , offre il vantaggio di essere meno costosa e meno invasiva [ 23 , 24 ] ; i nostri dati sono sovrapponibili a quanto ottenuto dal trattamento chirurgico nel lavoro di pocard et al . 
 [ 28 ] in una serie di 31 pazienti con singola lesione epatica da tumore mammario , trattata con resezione chirurgica maggiore o minore , con o senza rfa presenta una sopravvivenza media di 63 mesi e totale a 2 e 5 anni del 86% e 61% rispettivamente . la rfa , ragionevolmente , pu essere utilizzata in alternativa alla chirurgia come terapia locale di prima scelta , in quanto la storia naturale della malattia , ha dimostrato la scarsa ef cacia delle terapie locali ( chirurgia , ablazione del tumore in situ )  . 
luso della rfa non controindica il simultaneo o susseguente espletamento di altri trattamenti complementari . conclusions conclusioni in our experience and according to the literature , rfa appears to be a useful adjunct to systemic chemotherapy and / or hormone therapy in the locoregional treatment of hepatic metastases from breast cancer . 
rfa may also be a less invasive alternative to surgery in the locoregional treatnella nostra esperienza e in accordo con la letteratura , la rfa pu essere associata alla chemioterapia e / o ormonoterapia nel trattamento loco regionale delle metastasi epatiche da tumore della mammella . 
a prospective randomised trial comparing systemic treatment alone and systemic treatment with rfa for selected breast cancer liver metastases is needed to show any advantage of rfa in local and overall disease control when compared with systemic treatment alone . delle metastasi epatiche da umore della mammella . 
risulta quindi necessario uno studio prospettico randomizzato che compari la sola chemioterapia e la chemioterapia in associazione alla rfa atto a dimostrare i vantaggi della rfa nel controllo locale della malattia rispetto al solo trattamento sistemico . 
the aim of this study was to investigate the ef cacy of a dedicated software tool for automated volume measurement of breast lesions in contrast - enhanced ( ce ) magnetic resonance mammography ( mrm )  . 
the volume of all lesions was measured automatically ( avm ) from ce 3d mrm examinations by means of a computer - aided detection ( cad ) system and compared with the size estimates based on maximum diameter measurement ( mdm ) on mrm , ultrasonography ( us ) , mammography and histopathology . 
 this result was similar to mdm ( 3% understimation , not signi cantly different ) but signi cantly better than us and mammographic lesion measurements ( 24% and 33% size underestimation , respectively )  . 
 entrambi i metodi ottengono nella stima della dimensione per lesioni alla mammella valori pi vicini allo standard costituito dalla misura su pezzo operatorio rispetto ad ecogra a e mammogra a . parole chiave risonanza magnetica mammogra ca cad mezzo di contrasto paramagnetico 1040 introduction contrast - enhanced ( ce ) magnetic resonance mammography ( mrm ) is a promising complementary technique to mammography because of its inherent three - dimensionality [ 1 , 2 ]  . 
furthermore , tumourinduced microvessels show structural abnormalities that give rise to leakage of contrast mediuthis is the origin of the characteristic different patterns for malignant and benign lesions [ 15 ]  . image analysis of dynamic series can be manually performed : the radiologist draws regions of interest ( roi ) on areas exhibiting suspicious contrast agent uptake and evaluates the pixel intensity curve as a function of time . 
 however , in recent years , computer - aided detection ( cad ) systems have been developed to help to manage the large number of images produced during the dynamic acquisition [ 6 ]  . 
this is a notable feature , as mr imaging has shown superior potential for quanti cation of tumour size and follow - up after chemotherapy [ 712 ] , in addition to possible improvements in diagnostic accuracy . 
 objective tumour shrinkage has been adopted as a standard end - point for selecting anticancer agents , and size is one of the standard prognostic and therapeutic factors in common use today . 
oltre allinformazione sulla morfologia della lesione , la risonanza magnetica ( rm ) pu evidenziare caratteristiche funzionali dei tessuti , come la perfusione e la cinetica del mezzo di contrasto . 
la cinetica dellimpregnazione del mezzo di contrasto studiata tramite acquisizioni dinamiche : dopo liniezione di un bolo , sono effettuate svariate acquisizioni sul volume delle mammelle e viene considerata la curva temporale pixel per pixel . 
unaumentata densit dei microvasi incrementer il usso sanguigno , che porter ad una evidenziazione del contrasto ; inoltre , i microvasi indotti dal tumore mostrano anomalie strutturali che danno origine a una alterata permeabilit al mezzo di contrasto . 
questa lorigine delle diverse caratteristiche delle lesioni maligne e benigne [ 15 ]  . lanalisi sulle immagini delle serie dinamiche pu essere effettuata manualmente : i medici radiologi sono soliti tracciare regioni di interesse ( roi ) su aree con sospetta impregnazione contrastogra ca e valutare la curva dellintensit del pixel in funzione del tempo . 
tuttavia , negli ultimi anni , sono comparsi sistemi di rilevazione supportata dal computer ( computer aided diagnosis , cad ) , per aiutare i medici radiologi nella gestione dellelevato numero di immagini prodotte durante le acquisizioni dinamiche [ 6 ]  . 
 questi sistemi automatizzano e velocizzano il processo di analisi , in particolare evidenziano le regioni con sospetta impregnazione contrastogra ca e forniscono informazioni addizionali , come ad esempio la dimensione della lesione . 
 questultima una caratteristica rilevante , poich la rm ha dimostrato un potenziale superiore nella quanti cazione della dimensione del tumore e nel follow - up dopo chemioterapia [ 712 ] , oltre a un possibile miglioramento dellaccuratezza diagnostica . 
lesion volume was evaluated according to different methods : automated segmentation on mr imaging , manual volume estimation based on diameter measurement on mr imaging , us and mammography , and volume estimation based on measurement of the diameter on the histopathological specimen . 
of 52 lesions , 44 ( 33 invasive ductal carcinomas , 11 invasive lobular carcinomas ) were malignant , ve were low - grade lesions ( two ductal carcinomas in situ ; three lobular carcinomas in situ ) and three were benign ( one brocistic disease , two sclerosing adenosis )  . 
all remaining 149 patients had lesions classi ed as below category 4 of the breast imaging reporting and data system ( bi - rads ) and hence did not require further workup . 
volume measurements based on mrm , us and mammography were carried out for all 52 histopathologically proven lesions . magnetic resonance imaging examinations were performed on a 1.0 - t scanner ( intera , philips medical systems , pc best , the nederlands )  . 
 the breasts were imaged before and ve times after the intravenous injection ( injection rate 2 cc / s , followed by 15 ml of saline ush ) of 0.2 mmol / kg body weight gadopentate dimeglumine ( magnevist , schering , berlin , germany )  . 
la dimensione della lesione stata valutata secondo diversi metodi : segmentazione automatica in rm , stima manuale del volume basata sulla misura del diametro in rm , ecogra a ( us ) e mammogra a , stima del volume basata sulla misura del diametro sul reperto operatorio . 
delle 52 lesioni , 44 ( 33 carcinomi duttali invasivi e 11 carcinomi lobulari invasivi ) si sono dimostrate maligne , 5 si sono rivelate di basso grado ( 2 carcinomi duttali in situ e 3 carcinomi lobulari in situ ) e 3 benigne ( 1 malattia brocistica e 2 adenosi sclerosanti )  . 
le altre 149 pazienti sono state classi cate al di sotto del grado 4 del breast imaging reporting and data system ( bi - rads ) e perci non hanno necessitato di ulteriore follow - up . 
la misura del volume basata su mrm , ecogra a , mammogra a stata effettuata su tutte le 52 lesioni confermate istologicamente . immagini di risonanza magnetica gli esami sono stati effettuati su unapparecchiatura da 1 , 0 t ( intera , philips , medical systems , pc best , paesi bassi )  . 
le mammelle sono state acquisite prima delliniezione intravenosa e 5 volte dopo la somministrazione di 0 , 2 mmol / kg peso corporeo ( velocit di iniezione 2 cc / s , seguita da 15 ml di lavaggio di soluzione salina ) di gadopentato dimeglumina ( magnevist , schering , berlino , germania )  . 
la scelta del piano coronale , per questo modello di apparecchiatura , stata raccomandata dalla ditta produttrice in fase di impostazione del protocollo di acquisizione , per limitare gli artefatti da movimento . 
 gli esami ecogra ci sono stati effettuati con unapparecchiatura dotata di trasduttore 7 , 55 , 5 mhz ( envisor , philips medical system , pc best , paesi bassi )  . 
i mammogrammi sono stati interpretati secondo il metodo bi - rads e con conoscenza degli esiti clinici . massimo diametro del tumore come stima della dimensione la stima della dimensione della lesione stata valutata misurando il diametro massimo in tutte le modalit di imaging : nelle immagini mammogra che la dimensione della lesione stata misurata direttamente sulla pellicola radiogra ca con un righello . 
 stato poi considerato come dimensione della lesione il valore medio delle misure nelle proiezioni cranio - caudale e medio - laterale obliqua ; negli esami ecogra ci il medico ha direzionato la sonda per visualizzare la lesione sul piano in cui la sua dimensione appariva massima . 
quindi la dimensione stata misurata per mezzo dello strumento di misura delle lunghezze del software dellunit di acquisizione ; le immagini mrm sono state reperite sul sistema picture archiving and communications system ( pacs ) dellospedale ( carestream health , rochester , ny , usa ) e visualizzate su un monitor di refertazione . 
il medico ha quindi misurato la dimensione della lesione sul piano su cui essa appariva massima utilizzando lo strumento per la lunghezza delle distanze nel software del pacs ; le valutazioni con il cad sono state effettuate secondo quanto descritto nella sezione successiva . radiol med ( 2011 ) 116 : 10391049 1043 on mammographic images , lesion size was measured directly on the lm with a ruler . 
the mean value of the measurements in the craniocaudal and oblique mediolateral projections was considered as lesion dimension . on us , the radiologist oriented the transducer to display the lesion in the plane displaying its maximum size . 
 mrm images were retrieved from the hospital picture archiving ( pacs ) and communication system ( carestream health , rochester , ny , usa ) and displayed on a reporting monitor . 
the radiologist measured the lesion size along the plane in which it appeared to be the greatest using the ruler tool of the pacs software . cad evaluations were performed as described in following section . measurements were carried out by three of the authors ( gl , cam and rv ) , with 5 , 28 and 15 years , respectively , of experience in mammographic and us breast imaging , and 5 years of experience in mr breast imaging . volume analysis : automated software programme all mri examinations were processed by a dedicated cad for mrm ( cadstream , merge , hartland , wi , usa )  . 
this software is designed to automate the image processing and analysis functions that are typically performed manually by the mr technologist and radiologist , as previously described [ 15 ]  . 
for breast mr examinations , the software incorporates three mr series into the calculations : an unenhanced series , an early contrast - enhanced series and a delayed contrast - enhanced series . 
in the protocol used in this study , the early contrast - enhanced series was centred over roughly 2 min ( images obtained within 4 min ) and the delayed contrastenhanced series was centred over 47 min ( images obtained within 8 min )  . 
in addition , the software le misure sono state effettuate da 3 degli autori , gl , cam , rv , con rispettivamente 5 , 28 e 15 anni di esperienza in mammogra a ed ecogra a della mammella e tutti e 3 con 5 anni di esperienza nellimaging mr alla mammella . analisi del volume : software automatico tutti gli esami rm sono stati elaborati con un cad dedicato per risonanza magnetica alla mammella , cadstream ( merge , hartland , wi , usa )  . 
il software progettato per elaborare in modo automatico le immagini e le funzioni di analisi che sono tipicamente effettuate manualmente dal medico radiologo o da un tecnico , come precedentemente descritto da levrini et al . 
per esami mrm , il software considera 3 serie dinamiche per il calcolo : una serie pesata in t1 pre - contrasto , una delle prime serie post - contrasto , una serie post - contrasto tardiva . 
nel protocollo utilizzato in questo studio la prima serie post - contrasto utilizzata nel calcolo centrata circa a 2 minuti dalliniezione ( immagini ottenute entro 4 minuti ) e la serie tardiva centrata attorno a 47 minuti ( immagini ottenute entro 8 minuti )  . 
se il valore del pixel cresce oltre una soglia prestabilita , il pixel mostrato colorato sul monitor ( la soglia stata ssata al 100% del valore del pixel nellimmagine pre - contrasto )  . 
inoltre , il programma assegna un colore speci co ai pixel che raggiungono la soglia di impregnazione signicativa ; il colore assegnato al pixel dipende dal cambiamento intercorso tra la prima serie post - contrasto e quella tardiva : se il valore del pixel sulla serie tardiva decresce pi del 10% rispetto alla prima serie post - contrasto , il pixel colorato in rosso , indicando una curva con dismissione rapida ( wash - out ) del contrasto ; se il valore del pixel aumenta pi del 10% , colorato in blu , indicando una curva con impregnazione persistente ; se il valore del pixel non aumenta o diminuisce pi del 10% , colorato in giallo , indicando un andamento a plateau . 1044 radiol med ( 2011 ) 116 : 10391049 assigned a speci c colour to each pixel that reached the threshold for signi cant enhancement . 
the colour assigned depended on the change in pixel values between the initial contrast - enhanced series and the delayed contrast - enhanced series : value on the delayed series decreased by if the pixel > 10% of its initial contrast - enhanced value , that pixel was colour - coded red on the monitor , indicating washout of contrast material . 
 finally , the radiologist may select a speci c area of signi cant enhancement and the software will automatically generate a synopsis of the full volume of that lesion , including the percentage of the lesion that shows washout , plateau and persistent enhancement . 
il risultato nale una mappa colore sovrapposta a ogni strato rm , che indica le regioni di signi cativa impregnazione e fornisce dettagli sulla tipologia dellimpregnazione e sullestensione della stessa . in ne , il radiologo pu selezionare unarea di impregnazione signi cativa e il programma genera automaticamente una sinossi del volume della lesione , che include la percentuale della lesione che mostra wash out , plateau o impregnazione persistente . 
tutte le serie dellesame possono essere visualizzate con o senza mappa colore sovrapposta . analisi statistica lanalisi statistica stata effettuata con il software statistical package for the social sciences ( spss inc . , chicago , il , usa )  . 
i test statistici sono riportati nelle sezioni risultati e discussione . risultati let media delle 43 pazienti con lesioni confermate istologicamente di 50 , 1 anni ( da 33 a 78 anni , range interquartile 43 , 556 anni )  . 
su 52 lesioni , 23 ( 44% ) erano invisibili alla mammogra a , 4 ( 8% ) occulte allecogra a , 1 ( 2% ) stata giudicata non sospetta dallanalisi cad , poich laumento dellintensit del pixel era al di sotto della soglia prestabilita . 
un test di mcnemar stato effettuato per valutare la signi cativit di queste differenze : lanalisi cad signi cativamente pi accurata nella rivelazione di lesioni rispetto alla mammogra a ( p < 0 , 001 ) , mentre la differenza tra cad ed ecogra a non signi cativa ( p = 0 , 37 )  . le misure sul reperto istopatologico sono state considerate come gold standard : il valore mediano stato di 20 mm ( range 370 mm , range interquantile 1033 , 5 mm )  . 
stimata dalla formula : dim x dim h dim h dove a laccuratezza nella misura della dimensione della lesione , dim x la dimensione della lesione misurata nella modalit diagnostica x , dim h la dimensione della lesione valutata sul reperto istopatologico . 
nelle figure 2 e 3 sono riportati esempi di valutaradiol med ( 2011 ) 116 : 10391049 1045 examination can be displayed by the software with or without the colour overlay . table 2 accuracy of the different techniques in evaluating maximum tumour diameter statistical analysis modality accuracy ( mean values ) visible lesions ( n ) statistical analysis was performed with spss software ( spss , chicago , il , usa )  . 
of 52 lesions , 23 ( 44% ) were mammographically occult , four ( 8% ) were sonographically occult and one ( 2% ) was judged as nonsuspicious by cad analysis because pixel intensity enhancement was below the xed threshold . 
accuracy is assessed according to the formula : dim x dim h dim h where a is accuracy in the measurement , dim x is lesion size measured with the diagnostic modality x , dim h is lesion size evaluated on the histopathologic specimen . 
figure 4 shows the cad result that reports lesion size and position . discussion in recent years , mrm has gained increasing importance in diagnosing , staging and surgical planning of breast cancer [ 2 ]  . 
mr examinations offer unique advantages : the study of tumour morphology bene ts from the high spatial resolution and inherent three - dimensional imaging ; differential diagnosis can take advantage of multiparametric information based on t1 and t2 relaxation times . 
moreover , mrm can provide functional information on perfusion and capillary contrast agent leakage : contrast agent washin and washout patterns have shown a high sensitivity in the differmammography ultrasonography magnetic resonance mammography cad analysis 33% 24% 3% 4% cad , computer - aided detection mammogra a ecogra a risonanza magnetica mammogra ca analisi cad 33% 24% 3% 4% cad , computer - aided detection tabella 2 accuratezza delle diverse tecniche nel valutare il diametro massimo del tumore modalit accuratezza ( valori medi ) lesioni visibili ( n ) zione delle dimensioni di una lesione maligna con misura manuale in mrm e con il cad . 
la figura 4 riporta il risultato del cad che indica le dimensioni e la posizione della lesione . discussione negli ultimi anni la risonanza magnetica mammogra ca ha guadagnato unimportanza crescente nella diagnosi dei tumori alla mammella , nella stadiazione e nella piani cazione chirurgica [ 2 ]  . 
gli esami di risonanza magnetica hanno vantaggi peculiari : lo studio della morfologia del tumore trae bene cio dalla elevata risoluzione spaziale e dallintrinseca tridimensionalit dellimaging , la diagnosi differenziale si avvantaggia dellinformazione multiparametrica basata sui tempi di rilassamento t1 e t2 . 
inoltre , mrm pu fornire informazioni funzionali sulla perfusione e la perdita di mezzo di contrasto dai capillari : le curve di accumulo e dismissione del mezzo di contrasto hanno mostrato elevata sensibilit nella diagnosi differenziale tra lesioni benigne e maligne [ 1 ]  . un tipico esame mrm comprende almeno una sequenza pesata in t2 ( con o senza soppressione del grasso ) , unacquisizione dinamica dopo somministrazione di mezzo di contrasto ( inclusa unacquisizione pre - contrasto per sottrarre il grasso e il tessuto stazionario ) ed una sequenza pesata in t1 ad alta risoluzione con soppressione del 1046 radiol med ( 2011 ) 116 : 10391049 fig . 
lacquisizione dinamica fornisce uninformazione funzionale sullangiogenesi del tumore e sulla vascolarizzazione . i sistemi cad possono ottimizzare il usso di lavoro , aiutando il medico nella gestione dellelevata mole di immagini prodotte dalle serie dinamiche . 
sebbene luso di questi sistemi non sia ancora considerato obbligatorio rispetto ad un approccio manuale e il loro valore aggiunto tuttora dibattuto [ 1820 ] , essi si stanno diffondendo in maniera crescente . 
la possibilit di utilizzarli per la determinazione in automatico delle dimensioni della lesione una caratteristica da studiare in dettaglio , in particolare per la valutazione della risposta a trattamenti di chemioterapia neoadiuvante , come indicato da sardanelli et al . 
questa sottostima non statisticamente signi cativa ( test t di student per dati appaiati a due code , p = 0 , 24 ) ed sostanzialmente sovrapponibile a quanto misurato manualmente dal medico direttamente sulle immagini mrm . 
tale valutazione manuale sottostima il diametro massimo in media del 3% e la differenza tra la stima del cad e mrm non signi cativa ( test t di student per dati appaiati a due code , p = 0 , 62 )  . 
la stima nella dimensione della lesione offerta dal cad tanto accurata quanto quella effettuata direttamente su immagini rm , ma lanalisi automatica garantisce una maggiore standardizzazione nella valutazione del volume del tumore e consente un risparmio di tempo . 
la stima del cad della dimensione 33 mm . ential diagnosis of benign and malignant lesions [ 1 ]  . a typical mrm examination comprises at least a t2 - weighted sequence ( with or without fat suppression ) , a dynamic acquisition after contrast agent administration ( including a precontrast acquisition to subtract stationary tissues and fat ) and a high - resolution t1 - weighted sequence with fat suppression to evaluate late enhancement [ 16 , 17 ]  . 
even though the use of cad systems is still not considered mandatory with respect to a manual radiol med ( 2011 ) 116 : 10391049 1047 approach , and its added value is still debated [ 1820 ] , these tools are becoming increasingly wide spread . 
this underestimation was not statistically signi cant ( two - tailed students t test , p = 0.24 ) and it was basically equal to the measurement performed by the radiologist directly on the mrm images . 
in our study , us and mr con rmed their greater accuracy in lesion detection ( even though we did not distinguish among the different lesion types , as our sample was smaller ) , but our results show that mr is suporior to us in the evaluation of tumour size . 
on the contrary , this level of accuracy was accomplished in only 33% of lesions on us examinations and 31% on mammography , which show a general understimation of lesion dimensions . era al di sotto della soglia prestabilita . 
confrontato con le altre modalit lanalisi del cad pi accurata nella valutazione volumetrica . quattro lesioni su 52 sono risultate occulte allesame ecogra co , ma la differenza con le prestazioni del cad non signi cativa . 
tuttavia la valutazione ecogra ca meno accurata nella stima della dimensione del tumore e sottostima questa del 24% in media ( differenza altamente signicativa con il cad , test t di student per dati appaiati a due code , p < 0 , 001 )  . confrontato con gli esami mammogra ci , il sistema cad sia pi accurato nella stima della dimensione del tumore , che pi sensibile nella rivelazione di lesioni : solo 29 lesioni su 52 erano visibili in mammogra a ( la differenza con lanalisi del cad altamente signi cativa , test di mcnemar , p < 0 , 001 ) e per quelle visibili in mammogra a la sottostima nella dimensione della lesione del 33% ( differenza altamente signi cativa con cad e mrm , test t di student per dati appaiati a due code , p < 0 , 001 )  . laccuratezza nella valutazione preoperatoria di tumori alla mammella stata studiata da berg et al . 
 [ 21 ] : gli autori concludono che lecogra a e la risonanza magnetica sono pi accurate della mammogra a nella rivelazione di tumori invasivi , ma rischiano di sovrastimare lestensione della malattia . 
nel nostro studio , lecogra a e la risonanza magnetica confermano di essere pi accurate nella rivelazione delle lesioni ( pur non avendo noi distinto le varie tipologie di tumore essendo il nostro campione pi piccolo ) , ma i nostri risultati mostrano che gli esami di risonanza magnetica sono pi accurati rispetto allecogra a nello stimare le dimensioni della lesione . 
 al contrario questo livello di accuratezza ottenuto solo nel 33% delle lesioni osservate allecogra a e al 31% in mammogra a , che mostrano una generale sottostima delle dimensioni della lesione . poich lobiettivo principale nel trattamento di tumori alla mammella resecabili precocemente sono la conservazione della mammella e la prevenzione di recidive , importante identi care lestensione del tumore prima della chirurgia . 
il volume della massa tumorale pu essere sottostimato , ma questo fatto spesso ben evidenziabile allatto operatorio o al pi tardi determina il riscontro di margini in ltrati da malattia allesame istologico del pezzo . 
 [ 21 ] si attendono lesistenza di una massa tumorale residua approssimativamente nel 19% dei pazienti con carcinoma invasivo se la programmazione dellintervento derivasse unicamente dai riscontri di mammogra a e esame clinico ( ad esempio , allargamento della resezione o mastectomia in caso di margini positivi )  . 
presumibile , ma a sostegno 1048 radiol med ( 2011 ) 116 : 10391049 as breast conservation and prevention of recurrent disease are the main treatment goals in early resectable breast cancer , it is important to reliably determine tumour extent prior to surgery . 
decreasing the theoretical risk of local recurrence comes at the price of an increased risk of unnecessary wider excisions or mastectomy or , in most cases , additional imaging follow - up because of incidental ndings at mr imaging . 
recently , the relation between preoperative mrm and outcome after breast - conserving treatment for early - stage ( t1 or t2 ) and in situ breast carcinoma was determined in a large , nonrandomised cohort study : it was concluded that the use of mrm was not associated with improved outcome after breast - conserving treatment [ 22 ]  . our study has some limitations that need to be addressed . 
it is generally believed that the sensitivity of mrm imaging is lower at 1.0 t than at 1.5 t despite reports that sensitivity at the two eld strengths is equivalent [ 23 ]  . 
 thirdly , the number of patients is relatively small , which makes rm statistical conclusion dif cult ; larger patient samples should be considered in order to strengthen our deductions . 
la riduzione teorica del rischio di recidiva locale ottenuta al costo di un virtuale incremento di resezioni ampie o mastectomie non necessarie o , nella maggioranza dei casi , di indagini di diagnostica per immagini di controllo necessarie per valutare levoluzione di reperti rm incidentali . 
recentemente la relazione tra rm pre - operatoria e lesito del trattamento chirurgico conservativo per il tumore mammario in stadio iniziale ( t1 o t2 ) ed il carcinoma in situ stata descritta in un esteso studio di coorte non randomizzato : le conclusioni sono state che lutilizzo della mrm non associato ad un migliore risultato dopo il trattamento chirurgico conservativo [ 22 ]  . necessario precisare alcune limitazioni di questo studio . 
 opinione diffusa che la sensibilit della mrm inferiore quando viene utilizzata una apparecchiatura a 1 , 0 t rispetto alla abituale da 1 , 5 t , malgrado i dati disponibili [ 23 ] abbiano documentato sovrapponibili sensibilit alle due intensit di campo confrontate . 
terza limitazione costituita dal numero di pazienti relativamente esiguo , fatto che rende dif coltoso ottenere conclusioni statistiche solide ; sarebbe auspicabile valutare un numero di pazienti superiore per rafforzare le nostre deduzioni . 
in ne , tutti gli studi ecograci sono stati effettuati da un radiologo al corrente dei reperti clinici e mammogra ci ; cos le indagini rm sono state valutate alla luce dei reperti mammogra ci , clinici ed ecogra ci . 
 conclusioni in questo studio stato utilizzato un sistema cad per risonanza magnetica mammogra ca , basato sulla dinamica dellimpregnazione contrastogra ca , per stimare le dimensioni di lesioni alla mammella . 
il sistema cad si rivelato accurato e ha fornito misure consistenti con la stima sul reperto istopatologico . un sistema cad pu velocizzare lanalisi di unelevata quantit di immagini che provengono da esami mrm e fornisce informazioni aggiuntive sulla morfologia e funzionalit delle lesioni , come ad esempio la loro dimensione . 
further studies with larger patient samples are required to establish whether cad systems should be used extensively for mrm . tuisce uninformazione rilevante , come ad esempio per valutare la risposta a chemioterapia neoadiuvante . 
biti1 1radiotherapy unit , university of florence , viale morgagni 85 , 50134 florence , italy 2molecular and nutritional epidemiology unit , cancer research and prevention center , scienti c institute of tuscany , florence , italy 3department of medical physics , university of florence , florence , italy 4diagnostic senology unit , university of florence , florence , italy 5department of surgery , university of florence , florence , italy 6department of pathology , university of florence , florence , italy correspondence to : i . 
concerning cardiac assessment , six of the 56 evaluable patients ( 10.7% ) developed an asymptomatic decline of left ventricular ejection fraction > 10% and < 20% of the baseline value . 
per quanto riguarda la tolleranza cardiologica , sei dei 56 pazienti valutabili ( 10 , 7% ) hanno sviluppato un decremento asintomatico della frazione di eiezione ventricolare sinistra compreso tra il 10% e il 20% ( dallinizio del trattamento )  . 
in termini di tossicit non si sono inoltre veri cati effetti collaterali cardiaci severi . parole chiave carcinoma mammario iniziale chemioradioterapia concomitante antracicline tossicit cardiaca radioterapia adiuvante introduction introduzione breast - conserving surgery has been accepted as a validated surgical approach for early breast cancer ( bc )  . 
moreover , a recent meta - analysis of 13 randomised studies involving 22 , 903 patients demonstrated that the addition of taxanes to an ac - based regimen improved disease - free ( dfs ) and overall ( os ) survival in high - risk patients with early bc [ 46 ]  . it seems that the prognosis of bc is associated with the presence or absence of occult distant metastasis but not to the extension of the surgery . 
however , a meta - analysis showed a signi cant risk reduction of death due to bc after breast - conserving surgery and radiotherapy ( rt ) [ 7 ]  . 
the importance of rt timing following surgery to reduce the risk of local recurrence is well known [ 811 ]  . the optimal sequence of ct and rt after breastconserving surgery still remains controversial , although both adjuvant ct and rt can reduce the risk of bc recurrence . 
concurrent administration of ct and rt seems to be an ideal treatment after breast - conserving surgery , but the reported increase in toxicity [ 1012 ] resulted in the infrequent use of this therapeutic approach in clinical practice . we evaluated the feasibility of the concurrent rt and ac - based ct treatment , with particular emphasis on the side of breast disease occurrence . 
we also investigated the impact of treatment on adverse events and , in particular , on cardiac toxicity . la chirurgia conservativa della mammella ( bcs ) comunemente accettata come un valido approccio chirurgico nei tumori in fase iniziale . 
la somministrazione precoce di chemioterapia ( ct ) adiuvante pu ridurre il rischio di recidiva di malattia e la mortalit assoluta , indipendentemente dallet del paziente e dal regime chemioterapico utilizzato [ 1 , 2 ]  . 
i regimi chemioterapici basati sulle antracicline hanno mostrato una superiorit signi cativa quando confrontati con la chemioterapia secondo schema ciclofosfamide , methotrexate e 5uoro uracile ( cmf ) [ 3 ]  . 
inoltre , una recente metanalisi comprendente 13 studi randomizzati che includevano 22.903 pazienti , ha dimostrato che laggiunta dei taxani ad un regime chemioterapico basato sulle antracicline , aumenta la sopravvivenza libera da malattia ( dfs ) e la sopravvivenza globale ( os ) nei pazienti con tumore della mammella in fase iniziale ad alto rischio [ 46 ]  . sembra che la prognosi dei tumori della mammella sia associata alla presenza o meno di metastasi occulte a distanza , ma non allestensione della chirurgia effettuata . 
 daltra parte , una metanalisi ha mostrato una signi cativa riduzione del rischio di morte per tumore della mammella dopo chirurgia conservativa e radioterapia ( rt ) [ 7 ]  . 
 ben nota limportanza della tempestivit della radioterapia dopo chirurgia per ridurre la recidivit locale di malattia [ 811 ]  . la sequenza ottimale con cui eseguire la chemioterapia e la radioterapia dopo la bcs rimane ancora oggi una problematica controversa , sebbene sia noto come la chemioterapia e la radioterapia adiuvanti siano in grado di ridurre il rischio di ricaduta del tumore della mammella . 
la somministrazione concomitante di chemioe radioterapia sembra essere un trattamento ideale dopo la chirurgia conservativa , ma laumento della tossicit riportato in letteratura ha fatto 1052 materials and methods from september 2002 to december 2007 , 60 patients with early bc underwent concurrent adjuvant ac - based ct regimen and rt at our institute . 
according to the protocol , all patients received rt to the entire breast , supraclavicular fossa and axilla with external - beam rt using 6 - mv photon half - beam tangential elds for the breast and lower part of axilla ( mean delivered dose 50 gy ; range 4652 gy ) in 2 - gy daily fractions . 
the supraclavicular fossa and axilla apex were treated with a half - beam direct eld ( 6 - mv photons ) with posterior compensation ( 25 - mv photons )  . 
in all patients , the boost was delivered in 2 - gy daily fractions . ac - based regimens consisted of four cycles of intravenously administered ac ( doxorubicin 60 mg / m2 , cyclophosphamide 600 mg / m2 ) on day 1 , repeated every 21 days , or four cycles of intravenously administered epirubicin ( epi ) 100 mg / m2 on day 1 , repeated every 21 days , followed by four courses of intravenously administered cmf ( cyclophosphamide 600 mg / m2 , methotrexate 40 mg / m2 , and 5uorouracil 600 mg / m2 ) on days 1 and 8 , repeated every 28 days . all patients were required to have normal bone marrow reserve ( granulocytes > 1 , 500 / mm3 , platelets > 100 , 000 / mm3 , haemoglobin > 10 g / dl ) , renal function ( creatinine clearance > 50 ml / min ) , liver function ( bilirubin < 2 mg / dl ) and a left ventricular ejection fraction ( lvef ) > 50% at the baseline evaluation . 
baseline assessments included echocardiography with lvef measurement ; periradiol med ( 2011 ) 116 : 10501058 s che questo approccio terapeutico risulti di non comune utilizzo nella pratica clinica [ 1012 ]  . abbiamo pertanto valutato la fattibilit del trattamento radioterapico concomitante alla chemioterapia contenente antracicline , con particolare enfasi riservata al lato della mammella affetto dalla neoplasia . 
abbiamo inoltre ponderato limpatto del trattamento in termini di effetti collaterali e , in particolare , di tossicit cardiaca . materiali e metodi in un periodo compreso tra settembre 2002 e dicembre 2007 , 60 pazienti con un tumore della mammella in fase iniziale sono state sottoposte presso il nostro istituto a terapia adiuvante concomitante radioe chemioterapica contenente antracicline . 
in questa analisi abbiamo incluso solo le pazienti senza segni radiologici o clinici di recidiva locale o a distanza di malattia , nel momento in cui sono state visitate presso lunit di radioterapia , dopo aver effettuato il trattamento chirurgico conservativo . 
tutte le pazienti sono state trattate con radioterapia a fasci esterni sulla mammella e sulla regione inferiore dellascella utilizzando fotoni da 6 - mv con due campi tangenti ed un frazionamento di 2 gy giornalieri ( dose media 50 gy , range 4652 gy )  . 
la fossa sovraclaveare e lapice dellascella sono stati trattati con un campo diretto half - beam ( fotoni da 6 - mv ) con un compenso posteriore ( fotoni da 25 - mv )  . 
patients main characteristics are summarised in table 1 . acute radiation - related skin toxicity was assessed weekly during rt according to the radiation therapy oncology group scale [ 13 , 14 ]  . 
to record late toxicity , we used the late effects in normal tissues subjective , objective , management and analytic scale ( lent - soma ) [ 15 , 16 ]  . 
 for statistical analysis , we used a logistic model with stepwise selection considering rt interruption as the dependent variable , investigating several parameters ( bc side , age , ct regimen , baseline lvef value ) as independent predictive factors of rt discontinuation . results data regarding acute skin toxicity are shown in table 2 . 
 concomitant ct - rt caused acute skin toxicity g3 in 8.9% of patients ( ve of 56 ) and acute skin toxicity g4 in one normale riserva midollare ( neutro li > 1500 / mm3 , piastrine > 100.000 / mm3 , emoglobina > 10 g / dl ) , una funzione renale ed epatica nella norma ( clearance della creatinina > 50 ml / minuto , bilirubina < 2 mg / dl ) ed una frazione di eiezione ventricolare sinistra ( lvef ) superiore al 50% . 
la valutazione basale consisteva di unecocardiogra a con misurazione del lvef ; indagini ultrasonogra che cardiache sono state eseguite alla ne del trattamento chemioterapico , ogni quattro / sei mesi per i primi due anni dal termine della chemioterapia ed in seguito annualmente . 
le caratteristiche principali dei pazienti sono riassunte nella tabella 1 . la tossicit cutanea acuta da radiazioni stata valutata settimanalmente durante la radioterapia seguendo la scala radiation therapy oncology group ( rtog ) [ 13 , 14 ]  . 
per registrare la tossicit tardiva stata utilizzata la scala late effects in normal tissues subjective , objective , management and analytic ( lent - soma ) [ 15 , 16 ]  . 
rt was stopped in 21.3% of patients ( 12 of 56 ) ; in all cases , the interruption was 7 ( mean 5 ) days and the treatment was subsequently concluded reaching the prescribed total dose . 
in the logistic model with stepwise analysis using rt interruption as dependent variable , none of the evaluated parameters ( age , bc side , baseline lvef value , ct regimen ) emerged as an independent predictive factor of rt discontinuation ( data not shown )  . 
all ct was restarted after the interruption and was subsequently completed . concerning left - side bc patients , four of the 30 ( 13.3% ) developed a decline of lvef > 10% and < 20% of baseline value . 
one year after the end of ct , three of these patients ( including the symptomatic patient ) had unchanged lvef , and one had an increase of 5% of lvef . 
il trattamento concomitante radio - chemioterapico ha causato una tossicit cutanea acuta g3 nell8 , 9% dei pazienti ( 5 su 56 ) e tossicit cutanea acuta g4 in un solo paziente ( 1 , 7% )  . 
la radioterapia stata sospesa nel 21 , 3% dei casi ( 12 su 56 ) ; in tutti i pazienti la sospensione stata 7 giorni ( media 5 giorni ) ed il trattamento stato successivamente concluso , raggiungendo la dose totale prescritta . 
 considerando linterruzione della radioterapia come una variabile dipendente nel modello logistico statistico , nessuno dei parametri esaminati ( et , localizzazione del tumore , lvef basale , chemioterapia effettuata ) si dimostrato un fattore predittivo indipendente di interruzione della radioterapia ( dati non mostrati )  . 
la chemioterapia stata rimandata nel 57 , 1% dei pazienti ( 32 su 56 ) ; in tutti i casi la sospensione stata correlata a tossicit ematologica ed stata 7 giorni . 
tutte le chemioterapie interrotte o rimandate sono state successivamente riprese e poi completate . per quanto riguarda le pazienti con un tumore della mammella localizzato a sinistra , 4 su 30 pazienti ( 13 , 3% ) hanno mostrato un decremento della lvef > 10% e < 20% rispetto ai valori basali . 
ad un anno dal termine della chemioterapia , tre di queste pazienti ( incluso la paziente sintomatica ) hanno mostrato una lvef immutata , mentre una paziente ha mostrato un incremento del 5% della lvef . 
una paziente ha mostrato una riduzione asintomatica della funzionalit cardiaca sinistra , mentre unaltra paziente ha avuto sintomi cardiaci ( brillazione atriale ) , che hanno richiesto una speci ca terapia cardiologica . 
dopo due anni dal termine della chemioterapia questi pazienti hanno mostrato una lvef immutata . prendendo in considerazione le pazienti con tumore della mammella destra , 2 su 26 pazienti ( 7 , 6% ) hanno sviluppato una diminuzione asintomatica della lvef > 10% e < 20% rispetto ai valori basali . 
 dopo due anni dal termine della chemioterapia la paziente mostra una lvef immutata . ad un follow - up medio di 4 , 1 anni ( range 26 anni ) , una paziente ( 1 , 7% ) ha mostrato una recidiva di malattia locoregionale nella fossa sovraclaveare e tre pazienti ( 5 , 4% ) radiol med ( 2011 ) 116 : 10501058 1055 concerning the right - side bc patients , two of the 26 ( 7.6% ) developed an asymptomatic decline of lvef > 10% and < 20% of the baseline value . 
two years after ct , the patient had unchanged lvef . at a median follow up of 4.1 ( range 26 ) years , one patient ( 1.7% ) developed locoregional recurrence in supraclavicular fossa , and three patients ( 5.4% ) developed distant metastases ( two liver and one lung )  . discussion the optimal sequencing of rt and ct in early bc remains controversial [ 17 ]  . 
several authors reported a negative effect of rt on the ability to deliver optimal doses of ct and suggested that this may affect treatment outcome [ 10 , 18 , 19 ]  . 
 [ 26 ] , in a prospective nonrandomised study , reported the acute toxicity of rt alone and rt concurrent with ac ( ac / rt ) and rt concurrent with cmf ( cmf / rt )  . 
this experience was not positive in the concomitant arms : in fact , it was observed that patients treated with ac / rt and cmf / rt had a signi cantly higher incidence of high - grade skin toxicity , oesophagitis , dyspnoea , anorexia , nausea and hospitalisation when compared with those treated exclusively with rt . 
the dose of ct was reduced to < 85% of the planned dose in 11% of patients ; 17% of patients treated with concurrent ct and rt needed admission to hospital . in our experience , all patients received ac - based regimens and rt to the breast and local drains . 
 [ 27 ] ; hanno sviluppato metastasi a distanza ( due localizzazioni epatiche ed una localizzazione polmonare )  . discussione la sequenza ottimale della rt e della ct nei tumori della mammella in fase iniziale continua a rimanere controversa [ 17 ]  . 
diversi autori hanno riportato un effetto negativo della rt sulla possibilit di somministrare dosi ottimali di ct , suggerendo che questo potrebbe in uenzare loutcome del trattamento [ 10 , 18 , 19 ] ; un aumento dei livelli di tossicit potrebbe quindi compromettere la dose ottimale somministrata , sia per quanto riguarda la rt che la ct [ 20 ]  . 
 [ 26 ] , in uno studio prospettico non randomizzato , hanno riportato i dati riguardanti la tossicit acuta della rt da sola o concomitante a doxorubicina - ciclofosfamide ( ac / rt ) o somministrata in regime concomitante con ciclofosfamide , metotrexate e 5uorouracile ( cmf / rt )  . 
questa esperienza non si rilevata positiva nei bracci concomitanti : infatti stato osservato che i pazienti trattati con ac / rt e cmf / rt avevano una incidenza signi cativamente pi elevata di tossicit cutanea di alto grado , esofagite , dispnea , anoressia , nausea e ospedalizzazione , quando confrontati con i pazienti trattati con rt esclusiva . 
la dose della ct era stata ridotta a meno dell85% della dose prestabilita nell11% dei pazienti , il 17% dei pazienti trattati con rt e ct concomitanti hanno richiesto ospedalizzazione . nella nostra esperienza tutti i pazienti hanno ricevuti ct a base di antracicline e rt sulla mammella e sui drenaggi linfatici locali . 
nonostante lampio volume trattato e lutilizzo di antracicline , abbiamo registrato solo il 21 , 4% di interruzioni della rt a causa di tossicit cutanea acuta e inferiore a 7 giorni in tutti i casi ; tossicit cutanea g3 e g4 stata osservata rispettivamente nell8 , 9% e 1 , 7% dei pazienti . 
 ad un follow - up mediano di 76 , 4 mesi ( media 65 , 3 mesi ) , solo una paziente trattata con antracicline ha presentato 1056 radiol med ( 2011 ) 116 : 10501058 the authors compared two adjuvant treatments associating concomitant ct and rt . 
 this preliminary analysis showed the feasibility of this uncommon approach in terms of acute skin toxicity and cardiac safety but does not allow conclusions concerning local bc recurrence and distant failure . we had more ct interruptions compared with ct alone or other ct - rt associations [ 29 , 30 ]  . 
in fact , this group of patients was enrolled in a phase ii study that required rt to the breast and lymph node drain our clinical routine practice , it is not usual to give rt to the lymph node drain independently of the number of positive axillary lymph nodes [ 31 , 32 ]  . a relevant result was represented by the absence of severe cardiac effects . 
these patients were enrolled in a pilot study that investigated the ef cacy and feasibility of sequential and combined doxorubicin / docetaxel / cmf regimens ; their median age was 48 ( range 2965 ) years . 
nelle pazienti trattate con antracicline , la dfs dopo 5 anni era dell80% rispetto al 76 , 4% delle pazienti trattate con cmf ( log - rank test : p = 0 , 136 )  . 
la os dopo 5 anni era rispettivamente dell82 , 5% e dell81 , 1% nelle pazienti trattate con antracicline e cmf ( log - rank test : p = 0 , 428 )  . la sopravvivenza libera da malattia loco - regionale a 5 anni era del 98 , 6% nel gruppo a e del 94% nel gruppo b ( log - rank test : p = 0 , 033 )  . 
le percentuali di anemia di grado 2 e grado 3 erano rispettivamente del 13 , 9% nel gruppo dei pazienti trattati con antracicline e del 6 , 7% nel gruppo cmf ( p = 0 , 009 )  . 
questi risultati non si discostano molto da quelli ottenuti in un nostro precedente studio , in cui avevamo confrontato la rt esclusiva rispetto al trattamento concomitante rt - cmf [ 28 ]  . siamo consapevoli del maggior limite del nostro studio , rappresentato dal breve periodo di follow - up ( 4 , 1 anni )  . 
 questanalisi preliminare dimostra comunque la fattibilit di questo non comune approccio terapeutico , in termini di tossicit cutanea acuta e tossicit cardiaca , ma non permette al momento di formulare nessuna asserzione de nitiva per quanto riguarda il controllo loco - regionale e a distanza della malattia . nella nostra casistica si sono veri cate maggiormente interruzioni della chemioterapia rispetto a regimi chemioterapici esclusivi o ad altre associazioni radio - chemioterapiche [ 29 , 30 ]  . 
infatti i pazienti valutati in questanalisi erano stati arruolati in uno studio di fase ii che prevedeva la rt della mammella e dei drenaggi linfatici locali : nella nostra pratica clinica giornaliera non per comune irradiare i drenaggi linfatici , indipendentemente dal numero di linfonodi ascellari positivi [ 31 , 32 ]  . un importante risultato stato rappresentato dallassenza di importanti effetti collaterali cardiaci . 
per quanto riguarda le pazienti con tumore della mammella localizzato a sinistra , abbiamo osservato un decremento asintomatico del lvef compreso fra il 10%20% rispetto ai valori basali nel 13 , 3% dei casi . 
 queste pazienti sono state incluse in uno studio pilota che valutava lef cacia e la fattibilit di regimi concomitanti e sequenziali con doxorubicina / docetaxel / cmf in pazienti con unet mediana di 48 anni ( range 2965 anni )  . 
 the authors concluded that sequential and combined doxorubicin / docetaxel / cmf regimens plus conventional rt in selected non - high - risk cardiac patients are relatively safe without cardiac toxicity at mid - term follow - up [ 34 ]  . 
 it is possible that this nding is related to the modern rt techniques that offer the opportunity to decrease the risk of cardiac toxicity [ 35 , 36 ] compared with classical techniques [ 37 , 38 ]  . 
probably , partial breast irradiation could be a valid option for selected patients who need concomitant ct - rt , but new randomised clinical trials are necessary . lit cardiaca e sono tornate al loro valore iniziale di lvef durante il follow - up . 
 gli autori hanno quindi concluso che i regimi sequenziali e combinati doxorubicina / docetaxel / cmf con la rt convenzionale in pazienti selezionati non ad alto rischio cardiaco sono relativamente sicuri dopo un follow - up a medio termine [ 34 ]  . 
possibile che questi risultati siano correlati allimplementazione delle moderne tecniche radioterapiche , che offrono lopportunit di diminuire il rischio di tossicit cardiaca [ 35 , 36 ] rispetto alle tecniche classiche [ 37 , 38 ]  . 
probabilmente lirradiazione parziale della mammella potrebbe rappresentare una valida opzione per pazienti selezionati che necessitano di trattamenti concomitanti ct - rt , ma nuovi studi clinici randomizzati sono necessari . conclusions in our experience , concomitant ct - rt did not emerge as a signi cant predictor on rt interruption . 
skin toxicity due to concomitant ac - based regimens and rt was acceptable , and no severe cardiac events were recorded . conclusioni nella nostra esperienza il trattamento concomitante ct - rt non risultato essere un fattore prognostico signi cativo di interruzione della radioterapia . 
la tossicit cutanea dovuta alla somministrazione concomitante di regimi a base di antracicline assieme alla rt risultata essere accettabile e , in particolare , non si sono veri cati eventi cardiaci di grado severo . con ict of interest none radiol med ( 2011 ) 116 : 503 doi 10.1007 / s11547 - 011 - 0646 - 0 erratum the ultrasonographic correlates of carpal tunnel syndrome in patients with normal electrodiagnostic tests correlazioni ecogra che nella sindrome del tunnel carpale nei pazienti con test elettrodiagnostici negativi m . 
kahnouji2 1advanced diagnostic and interventional radiology research center ( adir ) , imaging medical center , imam hospital , tehran university of medical sciences , tehran 14155 - 7146 , iran 2department of neurology , imam hospital , tehran university of medical sciences , p.o. 
bellomi1 , 2 1divisione di radiologia , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy 2facolt di medicina e chirurgia , universit degli studi di milano , 20100 milano , italy 3divisione di epidemiologia and biostatistica , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy 4divisione di oncologia medica , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy 5divisione di anatomia patologica e medicina di laboratorio , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy 6dipartimento di medicina del lavoro clinica del lavoro luigi devoto , sezione di statistica medica e biometria ga maccacaro , universit degli studi di milano , milano , italy correspondence to : g . 
twenty - eight patients with solid breast lesions > 10 mm underwent conventional contrastenhanced magnetic resonance imaging ( mri ) and diffusion - weighted mri ( dw - mri )  . 
two observers ( expert and trainee ) segmented the lesion from the surrounding breast tissue on dw images with high b - value ( 1 , 000 s / mm2 )  . 
the mean of the differences was 0.012 10 - 3 mm2 / s , corresponding to an intraobserver variability of 1.1% ( limits of agreement : - 5% / + 8% )  . 
 the mean interobserver difference was 0.022 10 - 3 mm2 / s , corresponding to an interobserver variability of 2% ( limits of agreement : 9% / + 14% )  . 
ventotto pazienti con lesioni mammarie solide > 10 mm sono state sottoposte a risonanza magnetica ( rm ) convenzionale con mezzo di contrasto e a rm pesata in diffusione ( rm - dw )  . 
due osservatori hanno isolato la lesione dal tessuto mammario circostante nelle sequenze con elevata pesatura in diffusione ( b - value = 1000 s / mm2 ) ; tale analisi stata ripetuta da un osservatore dopo 6 mesi . 
stata calcolata una media delle differenze di 0 , 01210 - 3 mm2 / s , corrispondente ad una variabilit intra - osservatore di 1 , 1% ( limiti di accordo - 5% / + 8% )  . 
stata calcolata una media delle differenze di 0 , 02210 - 3 mm2 / s , corrispondente ad una variabilit inter - osservatore di 2% ( limiti di accordo di - 9% / + 14% )  . 
 radiol med ( 2011 ) 116 : 466476 which supports its potential use in routine clinical practice . keywords breast carcinoma diffusion - weighted magnetic resonance imaging intraobserver variability interobserver variability conclusioni . 
in breast cancer , timesignal intensity curves of a region of interest ( roi ) placed over the lesion typically show a high early peak , followed by a plateau or washout phase . 
this feature is due to the presence of highly permeable capillaries , which facilitate the rapid passage of a large amount of contrast material into the interstitial space and its rapid return into the vascular compartment by passive diffusion [ 3 ]  . 
breast mri also assesses the qualitative features of contrast enhancement , which may be homogeneous , heterogeneous or located predominantly at the periphery of the lesions ( rim enhancement )  . 
on the basis of the presence or absence of each of the above features , the breast lesion is given a score , which expresses the likelihood of malignancy according to the categories of the breast imaging reporting and data system ( bi - rads ) for mri [ 4 ]  . although the use of diffusion - weighted ( dw ) mri sequences for studying breast lesions is a relatively recent development , numerous studies have reported on the potential of dw - mri in the workup of breast abnormalities . 
these encouraging results have prompted many radiologists to incorporate dw sequences into conventional mri examinations , given that dw sequences are relatively fast ( generally 56 min ) and do la risonanza magnetica ( rm ) con mezzo di contrasto della mammella entrata a far parte della routine clinica , con performance elevate se eseguita per le corrette indicazioni ( ad esempio , sorveglianza delle donne ad alto rischio , stadiazione locale pre - trattamento chirurgico , valutazione delleffetto della chemioterapia neoadiuvante , studio della cicatrice nella mammella operata per carcinoma , carcinoma occulto della mammella , mammella secernente ) [ 1 , 2 ]  . 
le curve intensit - tempo relative a una regione di interesse ( roi ) posizionata sulla lesione mammaria indagata presentano tipicamente un picco precoce ed elevato , seguito da una fase di plateau o di wash - out nel carcinoma mammario ( cm )  . 
tale caratteristica dovuta alla presenza di capillari molto permeabili nel cm , che favoriscono un veloce ed abbondante passaggio di mezzo di contrasto nellinterstizio e un suo veloce ritorno nel compartimento vascolare per diffusione passiva [ 3 ]  . 
in relazione alla presenza o meno di ciascuna delle caratteristiche semeiotiche descritte attribuito un punteggio alla lesione mammaria , che ne de nisce la probabile malignit secondo le categorie breast imaging reporting and data system ( bi - rads ) rm [ 4 ]  . relativamente recente lutilizzo di sequenze pesate in diffusione ( dw ) per lo studio delle lesioni mammarie . 
one study compared the published experiences of 12 different centres , all of which used a 1.5 - tesla ( t ) mri system but with different parameters for dw sequences [ 11 ]  . 
the aim of our work was therefore to determine the intraand interobserver variability in calculating adc value of breast carcinomas . materials and methods patients the study was approved by the local ethics committee . 
 between may 2008 and july 2009 , a prospective study was conducted in which dw sequences were incorporated into the conventional mri examinations of women with solid breast lesions > 10 mm and a radiological and / or cytological diagnosis of malignancy who were candidates for surgery . 
all patients were enrolled after giving written informed consent . mri technique all mri examinations were performed with a 1.5 - t imager ( avanto , siemens , erlangen , germany )  . 
all patients were imaged lying prone , with both breasts positioned in a dedicated 8 - channel breast coil ( invivo breast array coil , invivo , orlando , fl , usa )  . 
all sequences were acquired with the use of parallel imaging , with the generalized autocalibrating partially parallel acquisitions ( grappa ) algorithm and an acceleration factor of 2 to decrease acquisition time and increase spatial resolution . 
 the dynamic sequence was repeated eight times : one baseline acquisition and seven continuous acquisitions starting after a 10 - s interval , during which gadopentetate dimeglumine ( magnevist , bayer schering , germany ) was administered intravenously with an automatic injector . 
the dose of contrast material was determined based on the patients te stato osservato un valore di adc pi basso nei cm che esprimono recettori per gli estrogeni [ 8 ]  . 
questi incoraggianti risultati hanno spinto molti radiologi ad integrare le sequenze dw allinterno dellesame rm convenzionale , favoriti dal fatto che le sequenze dw hanno una durata relativamente breve ( generalmente , entro i 56 minuti ) e non interferiscono con lesecuzione dellesame rm convenzionale con mezzo di contrasto . 
 uno studio ha confrontato le esperienze pubblicate in letteratura da 12 centri diversi , che hanno utilizzato tutti un apparecchio rm da 1 , 5 t , ma parametri delle sequenze dw non omogenei [ 11 ]  . 
 lo scopo di questo lavoro di determinare la variabilit intra - osservatore e inter - osservatore nel calcolo del valore di adc nei carcinomi mammari . materiali e metodi pazienti lo studio stato approvato dal comitato etico del nostro istituto . 
nel periodo compreso tra maggio 2008 e luglio 2009 stato eseguito uno studio prospettico , che prevedeva di includere sequenze dw allinterno dellesame rm convenzionale effettuato in donne con lesioni solide mammarie superiori ai 10 mm e diagnosi radiologica e / o citologica di malignit , candidate a chirurgia . 
tutte le pazienti sono state arruolate dopo avere ottenuto un consenso informato scritto . tecnica rm gli esami rm sono stati eseguiti con un apparecchio rm da 1 , 5 t ( avanto , siemens , erlangen , germania )  . 
tutte le pazienti sono state esaminate in posizione prona , con entrambe le mammelle adagiate allinterno di una bobina dedicata a 8 canali ( invivo breast array coil , invivo , orlando , florida , usa )  . 
dopo lacquisizione di una survey , sono state acquisite immagini rm nel piano assiale con il seguente ordine : short - tau inversion recovery ( stir ) pesate in t2 ( tempo di ripetizione [ tr ] / tempo di eco [ te ] / tempo di inversione [ ti ] = 3510 / 72 / 170 ms ; spessore , 3 mm ; gap 0 , 3 mm ; matrice 320320 , tempo di acquisizione 3 min 38 s ) ; sequenze dw ( tr / te = 4800 / 71 ms ; spessore , 5 mm ; gap 1 mm ; matrice 15090 , tempo di acquisizione 5 min 04 s ) con 4 b - value ( 0 , 250 , 500 , 1000 s / mm2 ) e soppressione del segnale lipidico mediante tecnica radiol med ( 2011 ) 116 : 466476 weight ( 0.1 mmol / kg ) and administered at a ow rate of 2 ml / s , followed by a standard bolus of saline solution ( 20 ml ) injected at the same rate of 2 ml / s . image analysis included digital subtraction of from the image processing dynamic precontrast sequence the postcontrast sequences ( subtracted images ) ; maximum intensity projection ( mip ) reconstructions in the axial , coronal and sagittal planes ; and adc mapping ( in grey scale , with light shades for high adc values and dark shades for low values ) ; and was done automatically by the mri systems software . 
all examinations were rendered anonymous and analysed by a radiologist experienced in the interpretation of breast mr images ( expert observer ) and a trainee radiologist ( nonexpert observer )  . 
the solid breast lesion was identi ed by using all available images ( stir , subtracted images , mip , dw images and adc maps )  . to calculate adc value ( quantitative analysis ) , dw sequences and adc maps were sent to a pc in digital imaging and communications in medicine ( dicom ) format [ 13 ]  . 
in all cases , the image was manually thresholded to ensure that certain pixels covered the entire area of the lesion ; any pixels outside of the lesion were removed digitally . 
six months after initial evaluation , the expert observer recalculated the adc values after separating the solid lesion from the surrounding breast tissue and selecting the volume of interest , following the same procedure as used for the rst reading . statistical analysis results of quantitative analysis were compared to evaluate intraobserver variability in the expert observer and interobserver variability between the expert and nonexpert observer . 
for each analysis , we calculated the differences between the two measurements with limits of agreespectral selection attenuated inversion recovery ( spair ) ; gradient echo 3d - fast low angle shot ( flash ) ( tr / te 7 , 4 / 4 , 7 ms ; ip angle 25 , matrice 38496 ; spessore 1 , 3 mm , gap 0 , 25 mm , tempo di acquisizione 1 min 02 s )  . 
tutte le sequenze prevedevano lutilizzo dellimaging parallelo , con algoritmo generalized autocalibrating partially parallel acquisitions ( grappa ) e fattore di accelerazione 2 , per diminuire il tempo di acquisizione e incrementare la risoluzione spaziale . 
la sequenza dinamica stata ripetuta per 8 volte : unacquisizione basale e sette acquisizioni continue aventi inizio dopo una pausa di 10 secondi , durante la quale avviene somministrazione endovenosa di gadopentetato dimeglumina ( magnevist , bayer schering , germania ) con un iniettore automatico . 
la dose stata decisa in base al peso della paziente ( 0 , 1 mmol / kg ) e somministrata ad un usso di 2 ml / s , seguita da un bolo standard di soluzione siologica ( 20 ml ) , anchessa ad un usso di 2 ml / s . analisi delle immagini le elaborazioni delle immagini con la sottrazione digitale della sequenza dinamica pre - contrasto dalle sequenze dinamiche post - contrasto ( immagini sottratte ) , le ricostruzioni maximum intensity projection ( mip ) nei piani assiale , coronale e sagittale , e le mappe adc ( in scala di grigi , con colore chiaro per valori elevati e con colore scuro per valori bassi di adc ) sono create in maniera automatica dal software dellapparecchio rm . 
 tutti gli esami sono stati resi anonimi e analizzati da un radiologo esperto nellinterpretazione di esami rm della mammella ( osservatore esperto ) e da un radiologo in formazione ( osservatore inesperto ) ; la lesione solida mammaria stata identi cata utilizzando tutte le immagini disponibili ( stir , sottratte , mip , dw e mappe adc )  . per il calcolo del valore di adc ( analisi quantitativa ) , le sequenze dw e le mappe adc sono state inviate a un pc in formato digital imaging and communications in medicine ( dicom ) [ 13 ]  . 
 stata sempre eseguita una modi ca manuale del threshold dellimmagine , in modo che dei pixel coprissero per intero larea della lesione ; eventuali pixel al di fuori della lesione sono stati rimossi digitalmente . 
i volumi cos ottenuti da entrambi gli osservatori , corrispondenti alle lesioni solide , sono stati salvati ed elaborati con un codice sviluppato nel nostro dipartimento basato su un software disponibile allinterno della functional mri of 470 radiol med ( 2011 ) 116 : 466476 fig . 
1 diffusion - weighted magnetic resonance imaging acquisition produces a series of images with different diffusion weightings according to the b value applied during imaging ( upper row )  . 
signal intensity decay with increasing b values ( lower row , far left ) can be modelled as an exponential equation , and on tting the equation to the data , the adc value is determined for each voxel to produce an adc map ( lower row , centre )  . 
rois were de ned by thresholding the highest b value image ( middle row , far right and centre right ) and then including only the cluster of suprathreshold voxels ( red ) that were part of the lesion ( middle row , centre left ) , as judged by comparison with the postcontrast images . 
to illustrate the stereotypical pattern of hyperintensity on the high b - value image and hypointensity on the adc map , the roi boundary only is overlaid on the corresponding images ( dashed arrows ) , allowing the reader to see the underlying tumour . 
la riduzione dellintensit del segnale allaumento del b - value ( riga inferiore a sinistra ) pu essere modellata come una equazione esponenziale ed integrando i dati allequazione , il valore adc calcolato per ogni voxel per produrre una mappa adc ( riga inferiore , al centro )  . 
le roi sono state disegnate utilizzando un threshold dellimmagine con il b - value maggiore ( riga in mezzo , a destra e centro - destra ) e poi includendo il cluster dei voxel oltre il threshold ( in rosso ) che includevano la lesione . 
per illustrare il pattern tipico di iperintensit sulle immagini con b - value elevato e ipointensit sulle mappe adc , il margine della roi stato sovrapposto sulle rispettive immagini ( freccia tratteggiata ) permettendo allosservatore di identi care il tumore sottostante . 
i valori di adc da ciascun voxel compreso nel volume di interesse sono ottenuti dalle mappe adc e sono stati usati per calcolare la media , la mediana e la deviazione standard per il tumore ( riga inferiore , destra )  . ment , with values expressed in the unit of measurement used , and the ratio between the two measurements with the corresponding limits of agreement to estimate the percentage variation of the two measurements . 
for the latter analysis , logarithmic transformation was applied to adc values , and the analysis was conducted on the differences between logarithms , as suggested by bland and altman [ 16 ]  . 
all patients tolerated the mr examination well , with no cases of adverse reaction to the contrast mediu mean lesion size was 21 ( range 1050 ) mall patients underwent surgery ( 16 mastectomy , 12 quadrantectomy )  . 
 il calcolo del valore di adc delle lesioni mammarie stato ripetuto a una distanza di 6 mesi dalla prima valutazione dallosservatore esperto ; lisolamento della lesione solida dal resto del tessuto mammario e la selezione del volume di interesse sono stati effettuati dallosservatore esperto , seguendo la medesima procedura eseguita per la prima lettura . analisi statistica i risultati dellanalisi quantitativa sono stati paragonati allo scopo di valutare la variabilit intra - osservatore nellosservatore esperto e la variabilit inter - osservatore radiol med ( 2011 ) 116 : 466476 table 1 histology : histological type and tumour node metastasis ( tnm ) staging patient histological typea tra osservatore esperto e non - esperto . 
per entrambe le analisi sono stati calcolati : le differenze tra le due misurazioni con i rispettivi intervalli di accordo , con i valori espressi nellunit di misura utilizzata e il rapporto tra le due misurazioni con i rispettivi intervalli di accordo , per ottenere una stima della variazione percentuale delle due misurazioni effettuate . 
per questultima analisi , i valori di adc sono stati sottoposti a trasformazione logaritmica e lanalisi stata cos condotta sulle differenze tra i logaritmi , come suggerito da bland e altman [ 16 ]  . 
2b. stata calcolata una media delle differenze di 0 , 012103 mm2 / s ( limiti di accordo : - 0 , 059 ; + 0 , 08310 - 3 mm2 / s ) , corrispondente ad una variabilit intra - osservatore pari a 1 , 1% ( limiti di accordo di - 5% / + 8% )  . 
these sequences were optimised to achieve a compromise between image quality requirements for quantitative analysis ( with adequate b value and signal - to - noise ratio ) and the short acquisition time needed for acceptable incorporation into a conventional contrastenhanced mri examination . mean adc value calculated in breast carcinomas in our study ( 1.0710 - 3 mm2 / s ) was comparable with the mean value calculated for seven different centres ( 0.9910 - 3 mm2 / s ) , which used similar mri equipment ( 1.5 t ) and dw sequences ( maximum b value of 1 , 000 or 1 , 074 s / mm2 ) to those used by us [ 11 ]  . 
this similarity in adc value further supports the possibility of comparing the adc value calculated for breast carcinomas in different centres and with different equipment , provided that the same dw sequence parameters are used . 
 queste sono state ottimizzate in modo da trovare un equilibrio tra i requisiti di qualit dellimmagine necessari per unadeguata analisi quantitativa ( con un numero suf ciente di b - value e un adeguato rapporto segnale / rumore ) e i requisiti necessari di brevit , fondamentali per renderne accettabile lintegrazione allinterno di un esame rm convenzionale con mezzo di contrasto . il valore medio di adc che abbiamo calcolato nei cm del nostro studio ( 1 , 0710 - 3 mm2 / s ) paragonabile al valore medio calcolato fra 7 centri diversi ( 0 , 9910 - 3 mm2 / s ) che hanno utilizzato unapparecchiatura rm ( 1 , 5 t ) e una sequenza dw ( b - value massimo di 1000 o 1074 s / mm2 ) simili alle nostre [ 11 ]  . 
questa sovrapponibilit del valore di adc avvalora ulteriormente la possibilit di confrontare il valore di adc calcolato per i cm in centri diversi e con apparecchiature rm diverse , se i parametri delle sequenze dw sono simili . 
tali fonti di variabilit potrebbero rendere elevata la variabilit nel calcolo del valore di adc eseguito da operatori diversi o dallo stesso operatore in momenti diversi , limitando di fatto lutilizzo del valore di adc nella routine clinica . 
 gli autori hanno descritto una buona riproducibilit del parametro misurato ( il valore di adc ) e hanno rappresentato i dati su gra co , senza speci care il dato tuttavia , posnumerico . 
 [ 12 ] , gli autori hanno incluso tutte le lesioni mammarie con dimensioni superiori ai 7 mm , delle quali 22 ( 25% ) erano benigne e 9 carcinoma in situ ( duttale o lobulare )  . 
2a , b both the interrater ( a ) intrarater ( b ) comparisons and showed low mean differences , 0.02210 - 3 mm2 / s and 0.01210 - 3 mm2 / s , respectively . 
2a , b il confronto inter - osservatore ( a ) e intra - osservatore ( b ) ha mostrato piccole differenze nei valori medi ; rispettivamente di 0 , 02210 - 3 mm2 / s e 0 , 01210 - 3 mm2 / s . 
il range dei limiti di accordo del confronto interosservatore quasi il doppio di quello intraosservatore ( - 0 , 10010 - 3 mm2 / s : 0 , 14310 - 3 mm2 / s vs - 0 , 5910 - 3 mm2 / s : 0 , 08310 - 3 mm2 / s )  . random or systematic errors in the use of the image - analysis software could lead to major errors in adc calculation . 
 these sources of variability could lead to high variability in adc determinations done by different operators or by the same operator at different times , thereby limiting the use of adc values in routine clinical practice . 
la natura solida e le dimensioni superiori ai 10 mm delle lesioni mammarie incluse nel nostro studio hanno probabilmente reso pi semplice per gli osservatori la de nizione dei margini della lesione . 
le dimensioni superiori al 10 mm , inoltre , hanno probabilmente limitato gli errori di calcolo dovuti alleffetto di volume parziale che potrebbero veri carsi per il calcolo delladc nelle lesioni mammarie di pochi millimetri , in cui gran parte dei voxel apparentemente relativi alla lesione mammaria sarebbe in effetti condivisa con 474 radiol med ( 2011 ) 116 : 466476 ( interobserver )  . 
 [ 12 ] , all breast lesions > 7 mm where included , of which 22 ( 25% ) were benign and nine were carcinoma in situ ( ductal or lobular )  . 
by contrast , our study considered only solid breast lesions > 10 mm , which were all subsequently found to be in ltrating breast carcinomas ( ductal or lobular )  . 
in addition , the larger size most likely limited calculation errors resulting from possible partial volume effects when determining the adc of lesions measuring a few millimetres only , where many of the voxels apparently belonging to the lesion are in fact shared with the surrounding breast tissue . 
in our study , although all available images ( stir , subtracted images , mip , dw images and adc maps ) were used to identify the lesion , only those with high diffusion weighting ( b value 1 , 000 s / mm2 ) were used to separate the solid lesion from the surrounding breast tissue . 
the differences between the two studies demonstrate the strength of the impact of operator technique in selecting the volume of interest for adc determination in the context of the quantitative analysis of dw - mri of breast carcinomas . 
the breast is less subject to artefacts compared with other body regions , such as the neck and face region ( movement artefacts due to deglutition and carotid pulsatility ) , the upper abdomen ( movement artefacts due to diaphragmatic excursion ) and the pelvis ( movement artefacts due to intestinal peristalsis and magnetic susceptibility due to the interface between bowel gas and surrounding tissues )  . 
in addition , the higher fat content of breast tissue , the signal of which is completely suppressed on dw images , and the use of images with high b value to de ne the roi , which allows il tessuto mammario circostante . 
nel nostro studio , invece , ci siamo serviti di tutte le immagini disponibili ( stir , sottratte , mip , dw e mappe adc ) per lidenti cazione della lesione mammaria , ma abbiamo utilizzato solo le immagini con elevata pesatura in diffusione ( b - value di 1000 s / mm2 ) per isolare la lesione solida dal resto del tessuto mammario . 
le differenze riscontrate tra i due studi mostrano quanto possa essere grande limpatto della tecnica con cui loperatore seleziona il volume di tumore da analizzare ai ni del calcolo del valore di adc , nellambito dellanalisi quantitativa della dw - mr dei cm . 
in ne , un insieme di condizioni che generalmente si veri cano per la rm - dw della mammella pu aver favorito una bassa variabilit nel calcolo del valore di adc nelle lesioni mammarie del nostro studio . 
la mammella meno soggetta ad artefatti rispetto ad altri distretti corporei , come ad esempio il distretto cervicofacciale ( artefatti da movimento per la deglutizione e da pulsatilit carotidea ) , lalto addome ( artefatti da movimento per lescursione del diaframma ) e la pelvi ( artefatti da movimento per la peristalsi intestinale e da suscettibilit magnetica dovuti alle interfacce tra il gas intestinale e i tessuti circostanti )  . 
inoltre , la elevata rappresentazione del tessuto adiposo nella mammella rispetto ad altre regioni anatomiche , il quale del tutto soppresso nelle immagini dw , e lutilizzo nel nostro studio di immagini con elevata pesatura in diffusione per la de nizione delle roi , che consentono un ef cace abbattimento del segnale originato dal tessuto ghiandolare sano , hanno probabilmente favorito lidenti cazione del cm e la delimitazione dei suoi margini con la roi . 
in particolare , la bassa variabilit intra - osservatore mette in evidenza la stabilit nel calcolo del valore di adc nei cm e suggerisce la possibilit da parte dello stesso operadiol med ( 2011 ) 116 : 466476 effective suppression of the signal from the healthy glandular tissue , probably helped our observers to identify the breast carcinoma and delineate its margins with the roi . 
 in particular , the low intraobserver variability re ects the stability of the adc determinations in breast cancers and suggests that the same operator can reliably repeat the measurements at different times , as could be the case in clinical practice for example , in breast cancer patients treated with neoadjuvant chemotherapy . 
the relatively low interobserver variability suggests that , provided image analysis is rigorously standardised , different operators could obtain comparable adc values in breast cancers , as could be the case in routine practice for breast cancer patients whose dw - mr images are analysed by different operators . there are a few limitations to our study . 
 this approach requires collaboration of a specialist in image analysis ( physicist , bioengineer , etc . ) , who is , however , needed for verifying image quality and results in any study involving a quantitative analysis of mr images . 
another limitation could be that a small fraction of the training in radiological mri of the nonexpert observer took place together with the expert observer during routine practice , and this may have contributed to limiting interobserver variability . 
 ratore di ripetere in maniera af dabile tali misure in momenti diversi , come , ad esempio , potrebbe veri carsi nella routine clinica per le pazienti con cm sottoposte a chemioterapia neoadiuvante . 
la variabilit inter - osservatore relativamente bassa suggerisce la possibilit da parte di operatori diversi di ottenere misurazioni sostanzialmente paragonabili del valore di adc sui cm , se lanalisi delle immagini standardizzata in maniera rigorosa , come , ad esempio , potrebbe veri carsi nella routine clinica per le pazienti con cm la cui rm - dw analizzata da radiologi diversi . il nostro studio ha dei limiti . 
questo approccio rende necessario il contributo di uno specialista ( sico , bio - ingegnere , ecc . ) in analisi dimmagini , il quale tuttavia necessario per il controllo della qualit delle immagini e dei risultati negli studi che prevedono lanalisi quantitativa delle immagini rm . 
un altro limite potrebbe essere costituito dal fatto che una piccola parte della formazione radiologica in rm dellosservatore inesperto sia avvenuta con losservatore esperto durante la routine clinica ; questo potrebbe aver contribuito a limitare la variabilit interosservatore . 
 in conclusione , abbiamo dimostrato che il nostro metodo di analisi quantitativa delle immagini dw ha consentito di ottenere basse variabilit intra - osservatore e variabilit inter - osservatore , le quali supportano lutilizzo del valore di adc nella routine clinica per i cm , qualora studi futuri ne validino in maniera de nitiva lutilit clinica . 
torricelli1 1department of radiology , azienda ospedaliera universitaria , policlinico , modena , italy 2department of surgery , azienda ospedaliera universitaria , policlinico , modena , italy 3department of pathology , azienda ospedaliera universitaria , policlinico , modena , italy correspondence to : f . 
thirty patients with histologically proven rectal cancer underwent surface - coil 3t mr imaging with sagittal , paracoronal and para - axial t2 - weighted turbo spin echo ( tse ) sequences . 
in the patients who underwent mr imaging before and after radiotherapy ( group 1 ) , the diagnostic accuracy of 3t mr imaging was 88% for t2 , 94% for t3 and 88% for t4 cancers . 
the high signal - to - noise ratio coupled with a large eld of view enables surface - coil 3t mr imaging to achieve high levels of diagnostic accuracy in the local staging of rectal cancer , and in particular in assessing in ltration of mesorectum and mesorectal fascia . 
sono state eseguite sequenze turbo spin echo ( tse ) t2 sagittali , para - coronali e para - assiali , spessore immagine 3 mm senza gap , eld of view ( fov ) 24 cm , matrice acquisizione 400512 . 
nei pazienti esaminati prima e dopo terapia neoadiuvante ( gruppo 1 ) i valori di accuratezza diagnostica della rm 3 t sono stati 88% per t2 , 94% per t3 , 88% per t4 , valore medio 92% , nei pazienti sottoposti a intervento chirurgico senza terapia neoadiuvante ( gruppo 2 ) laccuratezza diagnostica stata 93% per t2 , 79% per t3 , 86% per t4 , valore medio 86% ; laccuratezza globale stata 90% per t2 , 87% per t3 , 87% per t4 , valore medio 89% . 
 376 radiol med ( 2011 ) 116 : 375388 parole chiave rm 3 t stadiazione loco - regionale carcinoma rettale introduction introduzione colon carcinoma is one of the most common malignancies in industrialised countries , and location in the rectum sigmoid is seen in 60%70% of cases [ 13 ]  . 
once a histological diagnosis of rectal carcinoma has been established , a series of parameters need to be de ned , which are essential for planning treatment and which include depth of wall in ltration , mesorectal in ltration , circumferential resection margin ( crm ) , invasion of surrounding structures and presence of distance metastasis . 
in fact , whereas tumours con ned to the rectal wall can be treated radically by local excision alone , those that in ltrate the mesorectal fat require more extensive surgery , such as total mesorectal excision ( tme ) or abdominoperineal resection [ 39 ]  . 
additionally , stages t3 and t4 cancers [ 1 , 2 ] and those that in ltrate the upper portion of the anal canal are also subjected to neoadjuvant chemoradiotherapy with the aim of downstaging the tumour , a practice that has proved effective in improving outcome and permitting a more conservative surgical treatment [ 2 ]  . accurate preoperative assessment is therefore fundamental for directing management decisions [ 1016 ] , and in this context , imaging plays an increasingly important role . 
 among the imaging modalities used for disease staging , endorectal ultrasound is considered the reference standard for evaluating the depth of wall in ltration ; however , it suffers signi cant diagnostic limitations in evaluating extraparietal disease extent ( mesorectum and adjacent organs ) and regional lymph nodes [ 3 , 17 , 18 ] , as well as being dif cult to perform in severely stenosing tumours . multidetector computed tomography ( mdct ) , despite the signi cant recent improvement in staging effectiveness , still has limitations in contrast resolution that preclude adequate local staging of tumours of the middle and lower rectum , where correct assessment of parietal and perirectal in ltration is problematic [ 1 , 3 ]  . 
better results have been reported for cancers of the upper third of the rectum , where the greater abundance of perirectal fat heightens the natural contrast and therefore makes mdct staging more accurate [ 19 ]  . 
 numerous studies have demonstrated the ability of magnetic resonance ( mr ) imaging with phased - array coil to evaluate in ltration of the rectal layers , extension to the mesorectum and possible involvement of adjacent organs , reporting levels of accuracy that have made it the most accurate imaging technique for staging rectal cancer [ 1 , 3 , 2022 ]  . 
nearly all such studies were , however , conducted with 1.5 - t magnets and very few with systems operating il carcinoma del colon costituisce una delle pi frequenti neoplasie nei paesi industrializzati e la localizzazione al retto - sigma riscontrabile nel 60%70% di tutti i carcinomi del colon [ 13 ]  . 
dal momento in cui viene posta la diagnosi istologica di carcinoma del retto fondamentale de nire una serie di parametri che risultano indispensabili per la programmazione delle strategie terapeutiche e che sono rappresentati dalla profondit di in ltrazione parietale , dallin ltrazione del mesoretto , dal margine di resezione circonferenziale ( crm ) e dallin ltrazione di organi adiacenti oltre che , ovviamente , dalla presenza di metastasi a distanza . 
infatti , mentre i tumori con nati alla parete rettale possono essere trattati in modo radicale con la sola escissione locale , quelli in ltranti il tessuto adiposo mesorettale necessitano di approcci chirurgici pi estesi quali lasportazione totale del mesoretto ( tme ) o la resezione addominoperineale [ 39 ]  . 
inoltre , i tumori agli stadi t3 e t4 [ 1 , 2 ] e quelli che in ltrano la porzione superiore del canale anale , vengono sottoposti anche a chemio - radioterapia neoadiuvante con lo scopo di ridurre lo stadio della neoplasia , prassi che ha dimostrato di poter migliorare la prognosi e rendere possibili trattamenti chirurgici pi conservativi [ 2 ]  . unaccurata valutazione preoperatoria pertanto fondamentale per guidare le decisioni terapeutiche [ 1016 ] ed in tale ambito limaging riveste un ruolo sempre pi determinante . 
tra le metodiche di imaging utilizzabili per la stadiazione , lecogra a endorettale considerata il gold standard nel valutare la profondit di in ltrazione parietale , ma ha signi cativi limiti diagnostici nella valutazione dellestensione extraparietale ( al mesoretto ed organi adiacenti ) e dei linfonodi regionali [ 3 , 17 , 18 ] , oltre ad essere di dif cile esecuzione nelle forme fortemente stenosanti . la tomogra a computerizzata multidetettore ( tcmd ) , pur avendo negli ultimi anni migliorato in modo signile proprie performances stadiative , presenta cativo tuttora limiti di risoluzione di contrasto che non consentono unadeguata stadiazione locale delle neoplasie del retto medio - basso , dove risulta problematica la corretta valutazione dellin ltrazione parietale e perirettale [ 1 , 3 ]  . 
 migliori risultano invece i suoi risultati nelle neoplasie del terzo rettale superiore dove la maggiore presenza di adipe perirettale migliora il contrasto naturale e rende pi adeguate le possibilit stadiative della tcmd [ 19 ]  . 
 numerosi contributi della letteratura hanno dimostrato la capacit della risonanza magnetica ( rm ) con bobina phased array di valutare lin ltrazione tumorale delle radiol med ( 2011 ) 116 : 375388 at higher eld intensities . 
finally , a limited number of investigations conducted with both 1.5 - t and 3 - t magnets have evaluated patients with rectal carcinoma after neoadjuvant therapy [ 27 , 28 ]  . 
 the study population consisted of 30 patients ( 20 men , 10 women ; mean age 63 10 years ) with a diagnosis of rectal carcinoma proved by ultrasound - guided or endoscopic rectal biopsy and who were evaluated between april 2005 and december 2008 . 
twelve tumours were located in the upper third of the rectum , 11 in the middle third and seven in the distal third . mr imaging in all cases , mr imaging was conducted with a 3 - t system ( philips intera 3 - t , philips medical systems , best , the netherlands ) with the use of a pelvic phased - array surface coil . 
approximately 2 h before the mr study , the patients were given a water enema to cleanse the rectum and , at the beginning of the examination , they were administered antispasmodic iv ( buscopan , boheringer ) to reduce artefacts due to bowel peristalsis . 
examinations were performed without the administration of endorectal contrast medium in all but four patients who were affected by cancer of the rectal ampulla that was poorly depicted in the initial sequences and in whom the rectal lumen was distended with warm water delivered through an endorectal tube . 
the following sequences were acquired : axial t2 - weighted turbo spin echo ( tse ) ( time of repetition [ tr ] / time to echo [ te ] 3 , 200 / 100 ms , echo train length 16 ) encompassing the entire pelvis , eld of view 24 cm ; slice thickness 5 mm ; interval 1 mm ; matrix 312400 ; 2 signals acquired ; sensitivity encoding factor 1.5 ; sagittal t2 - weighted tse ( tr / te 3 , 200 / 100 ms , echo train length 18 ) ; eld of view 2224 cm ; slice thickness 3 mm ; no interslice gap ; matrix 400512 ; 2 signals acquired ; tonache rettali , lestensione al tessuto mesorettale e leventuale coinvolgimento degli organi adiacenti , con risultati in termini di accuratezza tali da rendere tale metodica la pi accurata tecnica di imaging per la stadiazione del carcinoma rettale [ 1 , 3 , 2022 ]  . 
la quasi totalit degli studi sovracitati stata condotta con magneti operanti a 1 , 5 t , mentre poco numerosi sono gli studi eseguiti con apparecchiature ad intensit di campo superiore ; in particolare , alcuni studi eseguiti con magnete operante a 3 t [ 2326 ] hanno riportato ottima accuratezza diagnostica , sovente superiore a quella ottenibile con magnete operante a 1 , 5 t . 
pochi studi , in ne , condotti sia con magneti a 1 , 5 t , che a 3 t , hanno valutato pazienti affetti da carcinoma del retto dopo terapia neoadiuvante [ 27 , 28 ]  . 
 lo scopo primario del presente studio valutare laccuratezza della rm a 3 t ( 3t rm ) nella stadiazione del carcinoma del retto ; scopo secondario quello di confrontare laccuratezza ottenibile con 3t rm in pazienti sottoposti a chirurgia dopo terapia neoadiuvante con quella di pazienti sottoposti ad intervento chirurgico senza terapia adiuvante . 
la popolazione dello studio consiste di 30 pazienti ( 20 maschi , 10 femmine ; et media 6310 ) con carcinoma del retto comprovato da biopsia rettale sotto guida ecogra ca o endoscopica , valutati da aprile 2005 a dicembre 2008 . 
dodici tumori erano localizzati nel terzo superiore del retto , 11 nel terzo medio del retto e 7 nel terzo distale . imaging rm la rm stata eseguita in tutti i pazienti impiegando un magnete operante a 3 t ( philips intera 3t , philips medical systems , best , olanda ) , con posizionamento di bobina di super cie phased array pelvica . 
circa 2 ore prima dellesame rm stato eseguito clistere idrico di pulizia dellampolla rettale e , allinizio dellesame , stata somministrato spasmolitico per via endovenosa ( buscopan , boheringer ) per ridurre gli artefatti da peristalsi intestinale . 
tutti gli esami sono stati eseguiti senza limpiego di contrasti endorettali , ad eccezione di 4 pazienti , affetti da carcinoma della porzione ampollare che era risultato mal visualizzabile nelle sequenze iniziali , ed in cui si provveduto a distendere il lume rettale con acqua tiepida , tramite sonda endorettale . 
in the event of very low rectal cancers with possible involvement of the anal canal , we obtained a similar paracoronal sequence parallel to the long axis of the anal canal ; axial t1 - weighted spin echo ( se ) ( tr / te 550 / 10 ms ) before and after administration of paramagnetic contrast medium ( gadolinium dota , dotarem , guerbet , arnoix sous bois , france ) ; eld of view 24 cm ; slice thickness 3 mm ; no interslice gap ; matrix 336512 ; sensitivity encoding factor 1.7 ; 2 signals acquired . 
 overall examination time was 3045 min . image analysis mr images were jointly reviewed prior to surgery by two observers ( fs and pt , radiologists with 5 and 10 years of experience in rectal mr imaging , respectively ) who were aware of the results of endorectal ultrasound and diagnostic biopsy . 
mr staging of local tumour extent was obtained on the basis of all t2 - weighted sequences and , in seven cases , also considering the t1 - weighted sequences with and without intravenous gadolinium administration . 
all tumours showed intermediate signal intensity in the t2 - weighted sequences ( higher relative to muscle and lower relative to submucosa ) in comparison with the rectal wall and mesorectal fat . 
 the observers used the tnm classi cation for tumour staging : stage t1 , if the tumour is con ned to the submucosa ; stage t2 , if the tumour signal intensity extends to the muscular layer without involving the perirectal fat ; stage t3 , if the tumour has intermediate signal and invades the mesorectal fat ; stage t4 , if the tumour extends to surrounding organs ( seminal vesicles , prostate , vaginauterus )  . 
 analisi delle immagini le immagini di rm sono state valutate congiuntamente da 2 osservatori ( fs e pt , medici radiologi , rispettivamente con 5 e 10 anni di esperienza in rm rettale ) prima dellintervento chirurgico . 
 la stadiazione rm dellestensione locale della neoplasia stata ottenuta sulla base dellanalisi di tutte le sequenze t2 pesate e , in 7 casi , anche tramite le sequenze t1 pesate con e senza somministrazione ev di gadolinio . 
le neoplasie hanno dimostrato in tutti casi intensit di segnale intermedia nelle sequenze t2 pesate ( pi alto del muscolo pi basso della sottomucosa ) al confronto con la parete rettale ed il tessuto adiposo mesorettale . 
 gli osservatori hanno utilizzato , a ni stadiativi , la classi cazione tumore - nodulimetastasi ( tnm ) : radiol med ( 2011 ) 116 : 375388 surgery and histopathology all patients underwent surgery consisting of local excision ( n = 11 ) , total mesorectal excision ( n = 16 ) and abdominoperineal resection ( n = 3 )  . 
preoperative neoadjuvant therapy consisted of the application of 45 gy to the pelvis in 1.8 gy fractions ; chemotherapy involved one cycle of 5uorouracil administered by continuous iv infusion at a daily dose of 250 mg / m2 . 
surgery was performed 56 weeks after the end of neoadjuvant therapy . in all 30 patients , histological examination and pathological staging was performed on the surgical specimen through the anatomical study of macrosections and conventional histopathological examination . 
the following two parameters were considered : in ltration of the mesorectal fat , to differentiate stage t2 from t3 ; in ltration of adjacent organs and the mesorectal fascia , which , if present , de ned stage t4 . 
the statistical signi cance of any difference in results between groups 1 and 2 was evaluated using the pearson test . results the mr study was well tolerated by all patients . 
 among patients in group 1 ( table 2 ) , two showed no signs of tumour , eight were staged as t2 , ve as t3 and one as t4 . 
in this group , histological examination established a diagnosis of stage t1 cancer in one case , t2 in stadio t1 , se il tumore non si estende oltre la sottomucosa ; stadio t2 , se il tumore , di segnale maggiore della tonaca muscolare , si estende no alla tonaca muscolare , ma non nel tessuto adiposo perirettale ; stadio t3 , se la neoplasia , di segnale intermedio , in ltra il tessuto adiposo mesorettale ; stadio t4 , se la neoplasia si estende ad organi circostanti : vescichette seminali , prostata , vagina - utero . lidenti cazione di linfonodi a distanza o di metastasi extrapelviche non rientrata tra gli scopi di questo studio . 
 la brosi perirettale stata identi cata come tessuto a margini spiculati ad intensit di segnale bassa nelle sequenze t2 pesate . chirurgia e anatomia patologica tutti i pazienti sono stati sottoposti a intervento chirurgico tramite escissione locale ( 11 ) , escissione totale del mesoretto ( 16 ) e resezione addominoperineale ( 3 )  . 
sedici pazienti sono stati sottoposti a terapia neoadiuvante preoperatoria : radioe chemioterapia ( gruppo 1 ) ed in questo gruppo la rm stata eseguita prima e dopo almeno 1015 giorni il termine della terapia ed entro 10 giorni dallintervento chirurgico . 
la radioterapia preoperatoria neoadiuvante consistita nellapplicazione di 45 gy , applicate alla pelvi in frazioni di 1 , 8 gy ; la chemioterapia stata basata su un ciclo di 5 fu , somministrato per infusione endovenosa continua alla dose giornaliera di 250 mg / m2 . 
lintervento chirurgico stato eseguito 56 settimane dopo il completamento della terapia neoadiuvante . in tutti i 30 pazienti la valutazione istologica e la stadiazione anatomo - patologica stata eseguita sul pezzo operatorio attraverso lo studio anatomico di macrosezioni ed il tradizionale studio istopatologico . 
lanatomo - patologo ha esaminato i campioni senza essere a conoscenza della stadiazione preoperatoria radiologica . analisi dei dati i risultati radiologici sono stati correlati a quelli istopatologici , assunti come standard di riferimento . 
sono stati considerati i 2 parametri seguenti : in ltrazione del tessuto adiposo mesorettale , per differenziare lo stadio t2 dal t3 ; in ltrazione di organi contigui e della fascia mesorettale , che se presenti , hanno de nito lo stadio t4 . 
 la signi cativit statistica della differenza dei risultati tra il gruppo 1 e il gruppo 2 stata valutata statisticamente tramite il test di pearson . table 1 tumour in ltration : comparison between magnetic resonance imaging ( mri ) and histopathological staging ; overall ( group 1 and group 2 ) sensitivity , speci city and accuracy of mr according to the different t stages of the tumour histology no tumour ( n = 2 ) t1 ( n = 1 ) t2 ( n = 12 ) t3 ( n = 11 ) t4 ( n = 4 ) total ( n = 30 ) radiol med ( 2011 ) 116 : 375388 380 mri no tumour stage no tumour mean value mri no tumore stadio no tumore valore medio sensitivity 100% 92% 82% 50% sensibilit 100% 92% 82% 50% speci city 100% 89% 89% 92% speci cit 100% 89% 89% 92% accuracy 100% 90% 87% 87% 89% accuratezza 100% 90% 87% 87% 89% risultati tabella 1 in ltrazione tumorale confronto tra stadiazione tramite rm e quella anatomopatologica ; valori complessivi ( gruppo 1 + gruppo 2 ) di sensibilit , speci cit ed accuratezza della rm in base agli stadi t della neoplasia rettale istologia no tumore ( n = 2 ) t1 ( n = 1 ) t2 ( n = 12 ) t3 ( n = 11 ) t4 ( n = 4 ) totale ( n = 30 ) six , t3 in four and t4 in three ; no residual tumour was detected in two cases . 
six of eight tumours staged as t2 on mr imaging were con rmed by pathology , one case was overstaged ( histological stage t1 ) and one was understaged ( histological stage t4 )  . 
four of ve tumours staged as t3 on mr imaging were con rmed by pathology , one case was overstaged ( histological stage t1 ) and one case was understaged ( histological stage t4 )  . 
mr imaging had a sensitivity , speci city and accuracy of 100% , 80% and 88% , respectively , for stage t2 ; 100% , 92% and 94% for stage t3 ; and 33% , 100% and 88% for stage t4 . 
mean overall accuracy of mr imaging in patients in group 1 was 92% . in the 14 patients in group 2 ( table 3 ) who underwent surgery without prior neoadjuvant therapy , mr imaging lo studio stato ben tollerato da tutti i pazienti . 
 nei pazienti del gruppo 1 ( tabella 2 ) non si sono identi cati segni di localizzazione neoplastica in 2 pazienti , 8 casi sono stati stadiati t2 , 5 casi t3 , 1 caso t4 . 
in questo gruppo lesame istologico ha posto diagnosi di stadio t1 in 1 caso , t2 in 6 casi , t3 in 4 casi , t4 in 3 casi ; in 2 casi non radiol med ( 2011 ) 116 : 375388 table 2 group 1 : comparison between the results of magnetic resonance imaging ( mri ) and histopathology staging after neoadjuvant therapy ; sensitivity , speci city , accuracy and mean value according to the different t stages of the tumour tabella 2 gruppo 1 : confronto tra risultati di rm dopo terapia neoadiuvante con quelli stadiativi dellanatomia patologica ; valori di sensibilit , speci cit , accuratezza e valore medio secondo i vari stadi t della neoplasia rettale patient no . 
 mri postneoadjuvant therapy histological results numero pazienti rm post terapia neoadiuvante risultati istologici stage no tumour t4 mean value fibrosis no tumour sensitivity 100% 100% 100% 33% fibrosis no tumour stadio fibrosi no tumore sensibilit fibrosi no tumore speci city accuracy speci cit accuratezza 100% 80% 92% 100% 100% no neoplasia valore medio 100% 100% 100% 33% 100% 80% 92% 100% 100% staged ve cases as t2 , six as t3 and three as t4 . 
mr imaging had a sensitivity , speci city and accuracy of 83% , 100% and 93% , respectively , for stage t2 ; 71% , 86% and 79% for stage t3 ; and 100% , 85% and 86% for stage t4 . 
sei su 8 tumori stadiati come t2 dalla rm sono stati confermati dallesame anatomopatologico , 1 caso stato sovrastadiato ( stadio istologico : t1 ) ed 1 sottostadiato ( stadio istologico : t4 )  . 
quattro su 5 tumori stadiati come t3 dalla rm sono stati confermati dallesame anatomo - patologico , 1 caso stato sovrastadiato ( stadio istologico : t1 ) ed 1 caso sottostadiato ( stadio istologico : t4 )  . 
la rm ha mostrato sensibilit , speci cit e accuratezza rispettivamente del 100% , 80% , e 88% per lo stadio t2 ; 100% , 92% e 94% per lo stadio t3 ; 33% , 100% , e 88% per lo stadio t4 . 
laccuratezza media complessiva della rm nei pazienti del gruppo 1 stata del 92% . nei 14 pazienti del gruppo 2 ( tabella 3 ) , sottoposti a intervento chirurgico senza terapia neoadiuvante , la rm ha stadiato 5 casi come t2 , 6 come t3 e 3 come t4 . 
quattro su 6 tumori 382 radiol med ( 2011 ) 116 : 375388 table 3 group 2 : comparison between results of magnetic resonance imaging ( mri ) and histopathology staging ; sensitivity , speci city , accuracy and mean value according to the different t stages of the tumour tabella 3 gruppo 2 : confronto tra risultati stadiativi della rm con quelli anatomopatologici ; valori di sensibilit , speci cit , accuratezza e valore medio secondo i vari stadi t della neoplasia rettale patient no . 
 mri staging histological results numero pazienti stadiazione rm risultati istologici stage mean value t3 , 5 mm from fascia t4 , seminal vesicles t4 , seminal vesicles t4 , seminal vesicles sensitivity 83% 71% 100% stadio t3 , 5 mm dalla fascia t4 , vescichette seminali t3 t4 , vescichette seminali t4 t4 , vescichette seminali t3 sensibilit speci cit speci city accuracy accuratezza 100% 86% 85% valore medio 83% 71% 100% 100% 86% 85% the development of high - resolution phased - array coils , have signi cantly improved the performance of mr imaging in the study of pelvic malignancies , making this modality especially suited to the study of rectal tumours where it allows analysis not only of the parietal component of the tumour but also of the surrounding anatomical structures and mesorectal fascia [ 1 ]  . although many authors have reported excellent results with the use of 1.5 - t systems [ 14 , 29 , 30 ] , it became immediately clear that the greater signal - to - noise ratio of 3 - t systems could be exploited to increase spatial resolution and allow acquisition of thin slices , with no interval gap and with high matrices and large elds of view , without impairing image quality [ 1 , 24 ]  . 
however , considering the entire patient cohort , the diagnostic accustadiati alla rm come t3 sono stati confermati dallesame anatomo - patologico , 2 casi sono stati sottostadiati ( stadio istologico t4 )  . 
la rm ha mostrato sensibilit , speci cit , accuratezza rispettivamente del 83% , 100% e 93% per lo stadio t2 ; 71% , 86% e 79% per lo stadio t3 ; 100% , 85% e 86% per lo stadio t4 . 
il valore del test di pearson stato di 0 , 855 , quindi non si dimostrata alcuna signi cativit statistica nella differenza tra i risultati conseguiti nei due gruppi di pazienti . 
 discussione i signi cativi progressi tecnologici delle apparecchiature rm , in particolare i miglioramenti nel campo della tecnologia dei gradienti e lo sviluppo di bobine phased array ad alta risoluzione , hanno signi cativamente migliorato le prestazioni della rm nellambito delle patologie neoplastiche del distretto pelvico , rendendo questa metodica particolarmente indicata per lo studio delle neoplasie rettali dove , oltre alla valutazione della componente tumorale parietale , possibile anche unaccurata analisi delle strutture anatomiche circostanti e della fascia mesorettale [ 1 ]  . sebbene molti autori abbiano riportato ottimi risultati con limpiego di apparecchiature rm operanti a 1 , 5 radiol med ( 2011 ) 116 : 375388 fig . 
1a para - axial t2 - weighted fast spin echo ( fse ) sequence : the image shows diffuse thickening of the rectal wall without precise delineation of the tumour . 
b limmagine assiale t2 pesata ottenuta dopo distensione del lume rettale con acqua mostra una precisa identi cazione del tumore in stadio t2 a livello della parete posterolaterale di destra . t [ 14 , 29 , 30 ] apparso subito evidente come il maggiore rapporto segnale - rumore garantito dalle rm operanti a 3 t avrebbe potuto essere utilmente impiegato per incrementare la risoluzione spaziale e permettere lacquisizione di sezioni sottili , senza intervallo di acquisizione , con matrici elevate ed ampi fov , senza degradazione qualitative delle immagini [ 1 , 24 ] , creando in tal modo le condizioni per unottimale valutazione delle neoplasie pelviche , con particolare riguardo al carcinoma rettale dove lelevata risoluzione spaziale costituisce il presupposto per lottimale valutazione sia dellin ltrazione parietale , che del mesoretto e degli organi endopelvici . in letteratura pochi autori hanno sino ad ora valutato laccuratezza della 3t rm nella stadiazione dei tumore rettale [ 2326 ] , sottolineandone in particolare laccuratezza nella determinazione della resecabilit dello s ntere [ 26 ]  . 
nel nostro studio , nei pazienti gruppo 2 , sottoposto a stadiazione prechirurgica , si avuto una accuratezza diagnostica per lo stadio t2 sovrapponibile ai risultati di kim et al . 
 [ 23 ] , in particolare vi completa sovrapposizione di risultati per lo stadio t2 , mentre per lo stadio t3 i risultati sono molto vicini ( 87% rispetto al 90% ) , mentre nel gruppo di kim et al . 
2 limmagine para - assiale t2 pesata fse mostra un tumore in stadio t3 in ltrante la parete posteriore - destra del retto ed il tessuto adiposo mesorettale ; stata misurata la distanza della neoplasia dalla fascia mesorettale ( freccia )  . racy obtained in our study appears similar to that reported by kim et al . 
a paraaxial t2 - weighted fse image showing , in the mesorectal fat , the presence of low - signal - intensity spiculated tissue ( arrow ) , without signi cant enhancement after intravenous infusion of contrast medium ( b , c before and after contrast administration ) and interpreted as brosis . 
a para - assiale t2 pesata fse mostra la presenza , nel contesto del tessuto adiposo perirettale , di tessuto spiculato ( freccia ) di basso segnale , senza signi cativo incremento del segnale dopo somministrazione e.v. 
 in our opinion , this may depend on the small number of t4 cancers and on the location of the cancers in the two cases of understaging , both of which were anterior supraampullary carcinomas with peritoneal in ltration , locations that are known to be dif cult to evaluate with mr imaging [ 29 ]  . 
in comparison with previous reports , our results are consistent with those obtained with 3 - t systems [ 2326 ] and on average better than those obtained with 1.5 - t equipment [ 1 , 3 , 14 , 15 , 20 , 21 , 31 ]  . 
a nostro parere questo pu dipendere dal basso numero di casi in stadio t4 e dalla particolare localizzazione nei 2 casi sottostadiati , entrambi carcinomi sovrampollari anteriori con in ltrazione neoplastica del peritoneo , sedi riconosciute di dif cile valutazione rm [ 29 ]  . 
inoltre la sovrastadiazione in 2 casi nel gruppo 2 verosimilmente legata alla reazione desmoplastica e alledema reattivo post - attinico , reperti ampiamente descritti nella letteratura corrente [ 24 , 29 ] , e documentati alla valutazione anatomopatologica in entrambi i casi . 
 al confronto con i dati riportati letteratura i nostri risultati sono in linea con quelli ottenuti con apparecchiature a 3 t [ 2326 ] e mediamente superiori ai risultati ottenuti con apparecchiature a 1 , 5 t [ 1 , 3 , 14 , 15 , 20 , 21 , 31 ]  . 
il maggiore limite emerso dalla letteratura scienti ca attuale , negli altri studi con la rm a 1 , 5 t , riguarda la dif colt a differenziare lo stadio t2 dai casi in stadio t3 dove presente solo minima in ltrazione extraviscerale [ 1 , 3 ]  . 
4a para - axial t2 - weighted fast spin echo ( fse ) image of a tumour of the right posterolateral wall of the rectum with invasion of the mesorectal fat and mesorectal fascia . 
however , this staging dif culty with mr imaging has limited clinical impact , as both stage t2 cancer and stage t3 cancer with minimal mesorectal in ltration ( 05 mm ) are treated with the same approach : anterior rectal resection without adjuvant therapy , owing to the good prognosis of both stages [ 32 , 33 ]  . 
in our study , this limitation appeared to have less relevance , as we had only stadiativa della rm ha una ridotta rilevanza clinica , poich sia lo stadio t2 , che quello t3 con minima in ltrazione del mesoretto ( da 0 a 5 mm ) hanno lo stesso approccio terapeutico : resezione anteriore del retto senza terapia adiuvante a seguito della buona prognosi di entrambi questi stadi [ 32 , 33 ]  . 
nel nostro studio questo limite sembrato essere meno rilevante , perch abbiamo avuto solo 2 casi in cui la stadiazione si rilevata errata : un caso nel gruppo 1 dove una neoplasia in stadio t4 per in ltrazione del peritoneo stata sottostadiata a t2 , ed un caso nel gruppo 2 , dove una 386 radiol med ( 2011 ) 116 : 375388 two cases of incorrect mr staging : one in group 1 , where a t4 cancer with peritoneal in ltration was understaged as t2 , and one in group 2 , where a t2 cancer was overstaged as t3 . 
 [ 28 ] found good ppv ( 84% ) and a fair overall diagnostic accuracy ( 79.2% ) in patients with stages t3 and t4 tumours treated with neoadjuvant therapy . 
moreover , in our study , there was no statistically signi cant difference ( p = 0.855 ) between the results achieved in group 1 and group 2 , a nding that appears to con rm the limited impact of the local changes induced by neoadjuvant therapy on the diagnostic accuracy of mr imaging . 
firstly , the number of patients included was small , and their distribution in the two groups was not homogeneous ( there were no patients with stage t1 tumours ) , a fact that might lead to an overestimation of diagnostic accuracy . 
in fact , mr imaging is usually limited in differentiating stage t1 from stage t2 tumours , and the literature demonstrates that endorectal ultrasound is still the modality of choice in these early - stage tumours [ 1 , 5 , 15 , 16 , 23 ]  . 
many reports have demonstrated the importance of describing the relationship between the tumour and the mesorectal fascia , which represents the plane through which tme is usually performed and is an important predictor of survival , the probability of local recurrence and the negativity of excision margins [ 20 , 21 , 29 , 30 , 34 , 35 ]  . 
 dalle nostre ricerche nella letteratura corrente non sono emersi studi che confrontassero laccuratezza della rm tra gruppi di pazienti sottoposti o non a terapia neoadiuvante , mentre solo pochi studi hanno valutato laccuratezza diagnostica della rm a 1 , 5 t dopo terapia neoadiuvante , documentandone una minore ef cacia stadiativa . 
 [ 27 ] hanno mostrato un elevato valore predittivo positivo ( 88%91% ) della rm a 1 , 5 t e buona accuratezza ( 78% ) nella identi cazione dei pazienti sottoposti a terapia neoadiuvante in stadio istologico t0 - t2 , mentre bonomo et al . 
 [ 28 ] in pazienti in stadio t3 e t4 , sottoposti a terapia neoadiuvante hanno riscontrato buoni valori predittivi positivi ( 84% ) e discreta accuratezza complessiva ( 79 , 2% )  . 
nel nostro studio laccuratezza stadiativa della 3t rm dopo terapia neoadiuvante stata complessivamente del 92% con variazioni dal 100% nello stadio t0 all88% nello stadio t2 , risultati che contrastano con quelli di torkzadt et al . 
nel nostro studio , inoltre , non c stata una signi cativa differenza statistica ( p = 0 , 855 ) tra i risultati ottenuti nel gruppo 1 e nel gruppo 2 , dato che conferma la scarsa rilevanza delle alterazioni locali indotte dalla terapia neoadiuvante sulla accuratezza diagnostica della rm , anche se tale riscontro deve essere supportato e confermato da un pi ampio gruppo di pazienti . 
per prima cosa , il numero di pazienti coinvolti nello studio ridotto e la distribuzione dei pazienti nei diversi gruppi non omogenea ( non sono presenti pazienti con tumore in stadio t1 ) , dato che potrebbe portare ad una sovrastima nel calcolo dellaccuratezza . 
di solito infatti in rm dif cile differenziare lo stadio t1 dallo stadio t2 e la letteratura dimostra che lecogra a endorettale ancora la metodica di elezione per questi stadi tumorali iniziali [ 1 , 5 , 15 , 16 , 23 ]  . 
molti lavori hanno dimostrato limportanza di descrivere le relazioni tra neoplasia e fascia mesorettale , rappresentante il piano di resezione principale della tme e importante fattore prognostico di sopravvivenza e di probabilit di recidiva locale e di integrit dei margini di resezione chirurgica dalla neoplasia [ 20 , 21 , 29 , 30 , 34 , 35 ]  . 
knauth springer - verlag , berlin heidelberg , 2010 isbn 978 - 3 - 540 - 97716 - 6 e - isbn 978 - 3 - 540 - 79717 - 3 doi 10.1007 / 978 - 3 - 540 - 79717 - 3 published online : 7 march 2011 springer - verlag 2011 the aim of this 168 page / 13 chapter book is to introduce the latest information and updated ( 2009 ) references in the eld of magnetic resonance angiography ( mra ) to the reader . the content is divided into three main sections : image acquisition techniques and sequences ( 5 chapters ) ; clinical applications ( 6 chapters ) ; special topics : transplants ( 2 chapters ) , plus the subject index . going through the book one realises how important mra and contrast enhanced mra sequences have become , gaining more and more momentum in the clinical diagnostic setting . robust strengths of the book include sequence speci cations ; use of contrast media in different procedures according to body organ and different anatomical districts ; evaluation of images both correct or presenting artefacts . 
the absence of ionizing radiation related to the use of mra is stressed and surely this advantage will increase the demand for mra , as this sort of equipment is made more available , with improved examination speed and reduction in patient time in the gantry . numerous images are presented and are of high quality , perfectly reproduced all throughout the book . 
to properly indicate the addressed problem ? i am also personally proud that this is one of the few books in this important series edited and entirely written by italian crme de la crme radiologists . intendimento di questo volume , nei suoi 13 capitoli e 168 pagine , di fornire al lettore le pi recenti ed aggiornate conoscenze ( voci bibliogra che no al 2009 ) nel campo della angiogra a con risonanza magnetica ( angio - rm )  . 
 il contenuto del volume diviso in tre grandi argomenti : tecniche di acquisizione de lle immagini e loro sequenze ( 5 capitoli ) ; applicazioni cliniche ( 6 capitoli ) ; argomenti speciali : i trapianti ( 2 capitoli ) per terminare con lindice analitico . nello scorrere il volume il lettore si rende conto di quanto siano divenute importanti sia la angio - rm che le sequenze con mezzo di contrasto , che si sono dimostrate di sempre maggior peso nel campo diagnostico clinico . tra i numerosi punti di forza del volume sono da ricordare la descrizione precisa delle sequenze da usare ; luso dei mezzi di contrasto nelle diverse modalit di indagine in funzione dellorgano in studio e dei vari distretti anatomici ; la interpretazione delle immagini sia corrette che in caso di artefatti . 
 viene poi segnalata e messa in evidenza lassenza delle radiazioni conseguente alluso dellangio - rm , cosa che di sicuro incrementer limpiego della stessa man mano che le apparecchiature dedicate saranno pi diffuse , tenuto anche conto dellaumento nella velocit di esecuzione delle indagini e della riduzione del tempo del paziente nellapparecchiatura . vengono presentate numerose immagini , di elevata qualit , perfettamente riprodotte in tutto il volume . 
it is frequently observed on multidetector ct ( mdct ) scans performed during daily clinical practice and may be caused by various pathological conditions , including oedema , inflammation , haemorrhage , neoplastic infiltration or sclerosing mesenteritis . 
otherwise , it may represent an incidental finding on mdct performed for other reasons . this article describes the mdct features of misty mesentery in different diseases in order to provide a rational approach to the differential diagnosis . riassunto il termine mesentere nebuloso indica un incremento patologico della densit del tessuto adiposo mesenterico alla tomografia computerizzata ( tc )  . 
 keywords disease abdomen multidetector ct mesentery parole chiave patologia addome tc multidetettore mesentere introduction introduzione the introduction of multidetector - row technology has greatly enhanced the role of computed tomography ( ct ) in evaluating patients suspected of having abdominal disease . 
furthermore , misty mesentery may represent an incidental finding on multidetector - row ct ( mdct ) performed for other reasons . as a matter of fact , misty mesentery is not an uncommon lavvento della tecnologia multidetettore ha ampliato notevolmente le potenzialit diagnostiche della tomografia computerizzata ( tc ) nella valutazione di pazienti con sospetta patologia addominale ; in tali pazienti il mesentere nebuloso rappresenta frequentemente il segno chiave , espressione della malattia sottostante . 
il mesentere nebuloso pu essere , daltro canto , un riscontro incidentale nel corso di esami tc multidetettore ( tcmd ) 352 radiol med ( 2011 ) 116 : 351365 finding at abdominal mdct , and radiologists must become familiar with this sign in order to understand its diagnostic value . 
we present a review of diseases that can result in misty mesentery , in order to provide a rational approach to the differential diagnosis on the basis of the associated findings . mesentery : normal anatomy mesenteries ( small - bowel mesentery , transverse mesocolon and sigmoid mesentery ) represent the reflection of the peritoneum on the bowel surface and suspend the loops of the small and large intestine from the posterior abdominal wall . they are composed of two layers within which vessels , lymphatics , lymph nodes , nerves and variable amounts of fat and connective tissue are housed . 
un dato di fatto , pertanto , che il mesentere nebuloso un reperto frequente alla tcmd delladdome e che i radiologi devono familiarizzare con tale segno e comprenderne il valore diagnostico . 
con questo lavoro offriamo una revisione delle patologie che possono manifestarsi con il segno del mesentere nebuloso , al fine di fornire un approccio razionale alla diagnosi differenziale , identificando reperti associati e possibili peculiari pattern di presentazione che orientano la diagnosi . mesentere : anatomia normale i mesi ( mesentere , mesocolon trasverso e mesosigma ) sono riflessioni del peritoneo sulla superficie intestinale e sospendono le anse del tenue e del colon ; essi sono formati da due foglietti peritoneali che contengono vasi arteriosi e venosi , linfatici , linfonodi , nervi e una quota variabile di tessuto adiposo e tessuto connettivo . 
 mesentere nebuloso : definizione il termine misty mesentery o mesentere nebuloso , introdotto da mindelzun nel 1996 [ 1 ] , indica un aumento della densit del tessuto adiposo mesenterico alla tc . 
1a , b immagini tc multidetettore assiali che illustrano i normali valori di attenuazione del mesentere ( a ) ed il tipico reperto del mesentere nebuloso , ossia un aumento della densit del tessuto adiposo mesenterico ( b )  . radiol med ( 2011 ) 116 : 351365 mesentere nebuloso : cause e reperti dellimaging il mesentere nebuloso pu essere conseguenza di diverse condizioni , quali ledema , il linfedema , la flogosi , lemorragia , la panniculite o le neoplasie [ 2 ]  . 
ledema mesenterico diffuso si riscontra frequentemente in pazienti con cirrosi epatica : in questi casi il meccanismo eziopatogenetico pi comune delledema lipertensione portale , che causa un aumento della pressione idrostatica allinterno delle vene mesenteriche , con conseguente stravaso di liquidi nel mesentere . 
la caratteristica del mesentere nebuloso nei pazienti cirrotici rappresentata dalla progressione dal solo edema mesenterico , verso una combinazione di edema mesenterico ed omentale , fino alla comparsa contemporanea di edema mesenterico , omentale e retroperitoneale . 
analogamente , la presenza di abbondante ascite senza aspetto nebuloso del mesentere molto rara nei pazienti cirrotici ed in tal caso dovrebbero essere considerate altre ipotesi diagnostiche , quali il carcinoma epatocellulare , locclusione dei rami portali e delle vene sovraepatiche o la peritonite batterica . 
nei pazienti con edema mesenterico sostenuto da patologia sistemica o da cirrosi epatica liperdensit del meso tende ad essere diffusa e si estende dalla superficie sierosa intestinale sino alla radice del mesentere . 
diffuse mesenteric oedema occurs frequently in patients with cirrhosis : in these cases , the most common pathogenic mechanism of oedema is portal hypertension , which causes increased hydrostatic pressure within the mesenteric veins , and consequently , fluid to seep out into the mesentery . 
the ct hallmark of misty mesentery in patients with cirrhosis is represented by a progression from mesenteric oedema alone , through a combination of mesenteric and omental oedema to a combination of mesenteric , omental , and retroperitoneal oedema . 
moreover , as mesenteric oedema in cirrhosis is due to portal hypertension , the presence of severe ascites in a patient with radiol med ( 2011 ) 116 : 351365 fig . 
3a , b arterial contrast - enhanced multidetector - row computed tomography images in a 57 - year - old patient with cirrhosis and a hepatocellular carcinoma nodule treated with transcatheter arterial chemoembolisation ( arrowhead in a )  . 
mild omental oedema ( curved arrow in a ) and ascites ( asterisks in a and b ) are associated with florid , widespread mesenteric oedema ( arrow in b )  . 
3a , b immagini tc multidetettore acquisite in fase arteriosa in un paziente di 57 anni con cirrosi ed un nodulo di epatocarcinoma ( hcc ) trattato con chemioembolizzazione ( testa di freccia in a )  . 
si documenta un modico edema omentale ( freccia curva in a ) con ascite ( asterischi in a e b ) e concomitante diffuso edema mesenterico ( freccia in b )  . 
4a , b portal - venous - enhanced multidetector - row computed tomography images of a 50 - year - old patient with cirrhosis and hepatocellular carcinoma ( arrowhead in a )  . 
ascites and omental soft - tissue nodules ( arrows in a ) cannot be related to oedema from portal hypertension , being associated with normal density of mesenteric fat ( asterisk in b )  . 
lascite e i noduli omentali ( frecce in a ) non sono causati dalledema secondario allipertensione portale , poich la densit del tessuto adiposo mesenterico normale ( asterisco in b ) ; tali reperti possono indicare un coinvolgimento neoplastico del peritoneo , confermato dallanalisi citologica del versamento ascitico . cirrhosis without the ct feature of misty mesentery is so uncommon that additional causes of ascites should be considered ( hepatocellular carcinoma , portal or hepatic venous occlusion , bacterial peritonitis )  . 
in patients with mesenteric oedema due to systemic diseases or cirrhosis , the mesenteric haziness appears to be diffuse and , therefore , extends from the serosal surface of the intestine to the root of the small bowel mesentery at the origin of mesenteric linfedema mesenterico il linfedema mesenterico pu essere primitivo o secondario a varie patologie . 
il reperto caratteristico di tale affezione rappresentato dal diffuso ispessimento radiol med ( 2011 ) 116 : 351365 nodulare della parete delle anse tenuali , conseguente alla dilatazione dei linfatici allinterno dei villi . 
lispessimento parietale dellansa intestinale pu assumere un aspetto stratificato a causa delledema della mucosa o della sottomucosa ; sono generalmente presenti ascite e linfedema mesenterico [ 5 , 6 ]  . 
le linfoadenopatie paraortiche e mesenteriche sono rare e la loro assenza utile per escludere altre patologie , quali ad esempio il linfoma , la malattia di whipple , la malattia celiaca e la tubercolosi , che possono comunque causare diffuso ispessimento parietale del piccolo intestino [ 7 ]  . il linfedema mesenterico secondario dovuto ad ostruzione linfatica conseguente a pericardite costrittiva , anomalie post - attiniche , malattia di crohn , tubercolosi intestinale o linfoma intestinale . flogosi mesenterica la maggior parte delle flogosi acute del tratto gastroenterico , quali colecistite , pancreatite , appendicite , diverticolite , malattie infiammatorie e tubercolosi , coinvolge il meso adiacente , causandone un aspetto nebuloso . 
il mesentere , poich parte integrante del peritoneo , coinvolto nella maggior parte dei pazienti con peritonite tubercolare : i seguenti segni tc sono altamente suggestivi di peritonite tubercolare [ 8 ] : 1 . 
 [ 4 ] , called small intestinal lymphangiectasia and characterised by a congenital abnormality of the lymphatic systethe ct appearance of primary intestinal lymphangiectasia is represented by diffuse nodular thickening of the smallbowel wall , which is the result of the dilated lymphatic channels within the villi . 
small - bowel thickening may assume a typical stratified appearance due to mucosa or submucosa oedema ; ascites and mesenteric lymphoedema are usually present [ 5 , 6 ]  . 
para - aortic and mesenteric lymph nodes are not usually identified , and the absence of such adenopathy was considered to be helpful in excluding other conditions , such as lymphoma , whipples disease , coeliac disease and tuberculosis , which can also produce diffuse small - intestinal - wall thickening [ 7 ]  . 
le frecce indicano anse del tenue distese , con ispessimento stratificato delle pareti . mesenteric inflammation most acute inflammatory diseases of the gastrointestinal tract , such as cholecystitis , pancreatitis , appendicitis , diverticulitis , inflammatory bowel disease and tuberculous peritonitis , involve the adjacent mesentery , causing misty mesentery . 
8 immagine tc multidetettore che documenta il mesentere nebuloso ( asterisco ) in un paziente con pancreatite acuta . rica , caratterizzata da una infiammazione cronica del tessuto adiposo mesenterico , che infiltrato da linfociti e macrofagi ripieni di grasso . 
la causa di tale patologia non chiara ed correlata ad un ampio spettro di affezioni quali vasculite , malattie granulomatose , disordini autoimmuni , radiol med ( 2011 ) 116 : 351365 ischemia , infezioni , traumi , precedenti interventi chirurgici o sindrome paraneoplastica [ 9 , 10 ]  . 
9 immagine tc multidetettore che documenta il mesentere nebuloso localizzato ( asterisco ) in un paziente con appendicite acuta ( freccia )  . mesenteric haemorrhage acute haemorrhage is characterised by high ct attenuation values ( 4060 hu )  . 
12 immagine tc multidetettore di un paziente con tubercolosi addominale che documenta iperdensit del tessuto adiposo mesenterico ( teste di freccia ) , con linfoadenopatie retroperitoneali caratterizzate da necrosi caseosa centrale ( frecce )  . 
the cause of this disease is unclear and has been related to a wide spectrum of conditions such as vasculitis , granulomatous disease , autoimmune disorders , ischaemia , infections , trauma , prior abdominal surgery or paraneoplastic response [ 9 , 10 ]  . 
nella maggior parte dei casi i tumori mesenterici primitivi sono benigni , come i desmoidi , che derivano da una proliferazione benigna di tessuto fibroso e possono manifestarsi in associazione con la sindrome di gardner , nel post - partum o a seguito di interventi chirurgici ; alla tc i desmoidi generalmente si presentano come masse con densit dei tessuti molli , con margini ben demarcati o scarradiol med ( 2011 ) 116 : 351365 fig . 
la tc dimostra sfumata infiltrazione del tessuto adiposo mesenterico o multiple masse solide rotondeggianti che di solito inglobano i vasi mesenterici e producono il caratteristico segno del sandwich , con dislocazione delle anse tenuali . 
15 multidetector - row computed tomography image showing mesenteric panniculitis as a well - circumscribed , inhomogeneous , fatty mass ( arrowheads ) , with higher attenuation values than normal retroperitoneal fat . 
15 immagine tc multidetettore che documenta la presenza di panniculite mesenterica , con una massa a densit adiposa , ben circoscritta , disomogenea ( teste di freccia ) , che mostra densit superiore a quella del normale tessuto adiposo retroperitoneale . 
because it extends along the root of the jejunal mesentery , panniculitis typically has a leftward 360 radiol med ( 2011 ) 116 : 351365 orientation ; there are scattered , well - defined small nodes . the fat - ring sign and a pseudocapsule are present . 
in the retractile form , the fibrosis predominates , and the disease manifests itself as large masses of soft - tissue attenuation that may involve vessels and may contain calcifications . 
when segmental misty mesentery shows the above - described ct features and no underlying disease is detected , mesenteric panniculitis has to be considered . nevertheless , mesenteric panniculitis may be a nonspecific response to an abdominal malignancy [ 11 , 12 ] and , therefore , close clinical follow - up to search for hidden malignancy is warranted in these patients . 
in most cases , primary mesenteric tumours are histologically benign , including desmoid tumours , which result from a benign proliferation of fibrous tissue and may occur in association with gardners syndrome , postpartum or postsurgery . 
direct spread : gastrointestinal carcinoid tumours : desmoplastic reaction from carcinoid tumours of the small bowel is common and occurs as a fixed solid mass with a stellate pattern of linear strands . 
ct features include an ill - defined infiltration of the rounded , mildly mesenteric enhancing masses that usually encase the mesenteric vessels and produce the sandwich sign , a mass loops . 
18 multidetector - row computed tomography image showing an enhancing mass with a coarse calcification in the mesentery ( arrow ) and focal wall thickening of an adjacent bowel loop ( arrowhead )  . 
19 immagine tc multidetettore di un paziente con linfangioma mesenterico . diagnosi differenziale e conclusioni poich il mesentere nebuloso pu essere espressione di patologie benigne e maligne , per la diagnosi differenziale necessario un approccio razionale . 
considerando i reperti precedentemente descritti , si pu dedurre che il coinvolgimento mesenterico , diffuso o focale , a limiti scarsamente definiti e tenuemente iperdenso frequente nelle patologie 362 radiol med ( 2011 ) 116 : 351365 fig . 
21 immagine tc multidetettore di un paziente con mesotelioma peritoneale maligno che documenta abbondante ascite ( asterisco ) e irregolare infiltrazione tumorale lungo i vasi mesenterici ( freccia )  . table 1 misty mesentery and corresponding diagnosis computed tomography features diagnosis diffuse or segmental increase of mesenteric fat attenuation without mass effect mass with increased attenuation showing the fatty - halo sign and a tumour pseudocapsule enhancing mass of soft tissue attenuation with vessel displacement non - neoplastic diseases neoplastic diseases stellate appearance of the mesentery associated with peritoneal nodules tabella 1 caratteristiche tc del mesentere nebuloso e diagnosi corrispondente computed tomography features diagnosis iperdensit diffusa o focale del grasso mesenterico senza effetto massa patologie massa con densit dei tessuti molli , con il segno dellalone adiposo e pseudocapsula massa con densit dei tessuti molli che disloca i vasi patologie non neoplastiche patologie neoplastiche aspetto stellato del mesentere , associato a noduli peritoneali diagnosis . 
according to the aforementioned ct features , diffuse or segmental involvement with ill - defined edges and stranding of mesentery is frequently observed in benign diseases , whereas mass - like , well - defined involvement is observed in neoplastic diseases , with the exception of mesenteric panniculitis ( table 1 )  . 
moreover , the radiologist must keep in mind that the clinical history and associated findings benigne , mentre la presenza di masse a margini ben definiti indica generalmente una patologia neoplastica , con leccezione della panniculite mesenterica nella forma retrattile ( tabella 1 )  . 
il radiologo , inoltre , deve sempre considerare la storia clinica del paziente ed i reperti associati , al fine di ottenere una migliore comprensione delle cause del mesentere nebuloso . 
table 2 provides a rational approach for differential diagnosis : the algorithm aims at reaching the final diagnosis by combining the morphological pattern of mesenteric involvement with specific associated findings . 
this approach could help the radiologist to correctly interpret the sign of misty mesentery , mostly in pathological processes that are characteristically centred in the mesentery adjacent to the bowel wall rather than in the bowel wall itself [ 14 ]  . correct noninvasive diagnosis is important because treatment strategies for these conditions range from monitoring to surgery . 
tale approccio aiuta il radiologo ad interpretare correttamente il segno del mesentere nebuloso , soprattutto nel caso di processi patologici che originano dal mesentere piuttosto che dalle anse intestinali [ 14 ]  . 
gandini istituto di radiologia diagnostica ed interventistica , universit di torino , aso san giovanni battista di torino , sede molinette , via genova 3 , 10126 torino , italy correspondence to : a . 
from january 2004 to december 2008 , we conducted 602 stereotactic , 11 - gauge , vacb procedures on 243 nonpalpable breast lesions categorised as bi - rads r3 , 346 categorised as bi - rads r4 and 13 categorised as bi - rads r5 . 
lesions of uncertain malignant potential ( b3 ) ( 23.6% ) were debated at multidisciplinary meetings , and diagnostic surgical biopsy was recommended for 83.1% of theall malignant lesions ( b4 and b5 ) underwent surgical excision . 
tra gennaio 2004 e dicembre 2008 , sono state eseguite 602 vacb con ago da 11 g , sotto guida stereotassica , su 243 lesioni classi cate come bi - rads r3 , 346 come bi - rads r4 e 13 come bi - rads r5 . 
le lesioni b3 ( 23 , 6% ) sono state discusse in sessioni multidisciplinari ; di queste l83 , 1% stato sottoposto a veri ca chirurgica , come tutte le lesioni risultate b4 e b5 . 
la vacb risultata metodica accurata nella caratterizzazione di lesioni a basso e medio rischio , evitando lintervento chirurgico in oltre la met dei casi con un effettivo risparmio economico . 478 radiol med ( 2011 ) 116 : 477488 keywords breast stereotactic vacuum - assisted core biopsy cost - effectiveness non palpable breast lesions mammotome parole chiave mammella biopsia mammaria stereotassica vacuum - assistita costo - ef cacia lesioni mammarie non palpabili mammotome introduction introduzione percutaneous vacuum - assisted core biopsy ( vacb ) has proven to be an effective and accurate method for histopathological characterisation of nonpalpable breast lesions , showing virtually identical results to diagnostic surgical biopsy , which is considered the reference standard for histological diagnosis of preclinical lesions [ 17 ]  . 
in particular , to quantify the actual cost savings , we evaluated the correlation between abnormalities considered at low ( bi - rads r3 ) and intermediate ( bi - rads r4 ) risk of malignancy and the histopathological diagnosis of benign disease . la biopsia percutanea vacuum assistita ( vacb ) si rivelata una metodica ef cace ed accurata per la caratterizzazione istopatologica di lesioni non palpabili della mammella , con risultati sovrapponibili alla biopsia chirurgica diagnostica , correntemente considerata la procedura gold standard per la diagnosi istologica delle lesioni pre - cliniche [ 17 ]  . 
lesions consisted of microcalci cations as the only suspicious radiological nding in 95.8% of cases ( 577 / 602 ) and microcalci cations associated with other mammographic signs ( structural distortion , asimmetric density , opacities ) in 3% ( 18 / 602 ) ; in 7 / 602 ( 1.2% ) cases only did we obtain biopsies of structural distortions , opacities or thickening for which both core needle biopsy ( cnb ) and ne - needle aspiration cytology ( fnac ) provided inconclusive results ( c1 and b1 )  . 
 mammographic ndings were classi ed according to the breast imaging reporting and data system ( bi - rads ) , 4th edition classi cation of the american college of radiology ( arc ) [ 12 ]  . 
vacb was performed using the mammotome device ( ethicon endo - surgery , cincinnati , oh , usa ) with 11 - gauge needles applied to the prone fischer mammotest stereotactic table ( fischer imaging , denver , co , usa )  . 
biopsy samples were nel periodo compreso tra gennaio 2004 e dicembre 2008 sono state eseguite 602 vacb in pazienti di et compresa tra 35 e 73 anni ( et media : 56 , 3 anni )  . 
le lesioni erano rappresentate nel 95 , 8% dei casi ( 577 / 602 ) da microcalci cazioni come unico sospetto radiogra co , nel 3% ( 18 / 602 ) da microcalci cazioni associate ad altri segni mammogra ci ( distorsione strutturale , addensamenti asimmetrici , opacit ) e in soli 7 / 602 ( 1 , 2% ) casi sono state biopsiate distorsioni , opacit o addensamenti , nelle quali sia la core needle biopsy ( cnb ) che la ne needle aspiration citology ( fnac ) non avevano fornito unadeguata risposta diagnostica ( c1 e b1 )  . 
in 534 / 602 ( 88 , 7% ) lestensione delle lesioni era 10 mm , mentre solo in 68 casi ( 11 , 3% ) le dimensioni erano > 10 mi reperti mammogra ci sono stati classi cati secondo il sistema bi - rads , dellamerican college of radiology [ 12 ]  . 
la vacb stata effettuata utilizzando il dispositivo mammotome ( ethicon endosurgery , cincinnati , oh , usa ) con ago da 11 gauge , applicato al tavolo stereotassico digitale prono fischer mammotest ( fischer imaging , denver , co , usa )  . 
tutti i prelievi radiol med ( 2011 ) 116 : 477488 arranged on absorbent paper according to sampling order , taking care to separate the samples with even numbers from those with odd numbers . 
approximately 2 weeks after the procedure , unilateral two - view mammograms were obtained in all patients to evaluate the correct position of the nonmagnetic metal clip and the presence of any residual microcalci cations . 
all procedures were performed as day cases , and mean procedure time was around 60 mthe results of the microhistological examination were classi ed into ve categories in accordance with the european guidelines [ 13 ] : b1 = normal , b2 = benign , b3 = lesion of uncertain clinical signi cance , b4 = suspicious for malignancy , b5 = positive . 
benign cases ( b2 ) underwent successive follow - up mammograms over the years , all of which have proved negative . cost analysis the second phase of the study involved comparison between the effective and overall costs incurred for the two biopsy methods ( vacb vs diagnostic surgical biopsy ) , taking into account the minimum reimbursement fees ( not including complications and / or comorbidities ) established for the single procedures performed in the departments of radiodiagnostics and general surgery . 
we considered a mean duration of the surgical procedure of around 90 min , with the presence in the operating room of two surgeons , one anaesthetist , one general care nurse , one room nurse and one auxiliary nurse . 
the reimbursement rate for a vacb procedure ( ministerial decree 22 / 7 / 96 : 85.11.3 ) includes the cost of the technology used ( complete vacb kit and operating costs for the stereotactic table ) , consumables ( anaesthesia , gauze swabs , plasters , etc ) and hourly cost of operators based on the salary scale ( one radiologist , one radiographer and one nurse )  . 
sono stati effettuati radiogrammi con ingrandimento dei campioni prelevati , allo scopo di veri care la presenza di microcalci cazioni , e sono stati chinati solo i frustoli contenenti le microcalci cazioni . 
a circa due settimane dallesecuzione della procedura , tutte le pazienti sono state sottoposte a controllo mammograco monolaterale in due proiezioni per valutare il corretto posizionamento della clip metallica amagnetica precedentemente posizionata e leventuale presenza di microcalcicazioni residue . 
lesame microistologico stato classi cato in 5 categorie in accordo con le linee guida europee [ 13 ] : b1 = normale , b2 = benigno , b3 = lesione di incerto signi cato , b4 = sospetto di malignit , b5 = positivo . 
lesame istologico de nitivo stato considerato il gold standard in tutti i casi di lesioni maligne o atipiche sottoposte ad intervento chirurgico ; nei casi in cui allistologia de nitiva non fosse pi presente la lesione maligna , stato rivisto il prelievo da vacb a conferma della diagnosi precedentemente posta . 
i casi benigni ( b2 ) sono stati sottoposti nel corso degli anni a successivi follow - up mammogra ci , risultati in tutti i casi a tuttoggi negativi . valutazione dei costi la seconda fase dello studio ha previsto il confronto tra i costi effettivi e complessivi affrontati per eseguire le due metodiche bioptiche diagnostiche ( vacb vs biopsia chirurgica diagnostica ) , prendendo in considerazione le tariffe di rimborso minime ( non gravate da complicanze e / o comorbilit ) previste per le singole procedure della radiodiagnostica e della chirurgia generale . 
le tariffe di rimborso relative alla biopsia chirurgica sono state derivate dal nomenclatore tariffario regionale delle prestazioni specialistiche ambulatoriali ( drg n262 approvato con deliberazione giunta regione piemonte n50 - 1062 del 10 / 10 / 2005 ) e comprendono il costo della sala operatoria , del ricovero in regime di day - hospital e del reperaggio sotto guida radiologica della lesione da sottoporre a biopsia , il costo dei materiali ( anestesia , materiale per le suture , farmaci vari etc . ) e la retribuzione oraria degli operatori , da stipendio tabellare ( in base alla loro quali ca ed al loro numero )  . 
 stata considerata una durata media della procedura chirurgica di circa 90 minuti , con la presenza in sala operatoria di due chirurghi , un anestesista , un infermiere professionale , uno strumentista e un infermiere generico . 
the correlation between radiological suspicion and microhistological diagnostic category is summarised in table 2 , whereas the correlation between radiological suspicion and nal histology on the surgical specimen is shown in table 3 . vacb proved to be inadequate ( b1 ) in 0.5% of cases because of failure to complete the procedure due to either excessive bleeding ( n = 2 ) or patient anxiety ( n = 1 )  . 
in accordance with the protocol , the patients were scheduled for yearly follow - up if the calci cations were completely removed or 6 - month follow - up if removal were incomplete . 
il 16 , 9% delle b3 non operate stato inviato a follow up annuale ( periodo di osservazione medio 2 , 95 anni / persona intervallo da 1 a 5 anni )  . 
la correlazione tra rischio radiologico e categoria diagnostica istologica riassunta nella tabella 2 , mentre nella tabella 3 riportata la correlazione tra rischio radiologico e diagnosi de nitiva su exeresi chirurgica . 
 la vacb risultata non idonea ( b1 ) nello 0 , 5% dei casi , poich la procedura non stata completata o per eccessivo sanguinamento ( 2 casi ) o per crisi ansiosa della paziente ( 1 caso )  . 
in 2 / 337 casi ( 0 , 6% ) con esito di benignit , in considerazione del rischio radiologico r4 , dellincompleta asportazione delle microcalci cazioni e a seguito della discussione multidisciplinare , stata comunque consigliata veri ca chirurgica . 
delle 150 lesioni proliferative a rischio ( lpr ) , indicate anche come borderline in letteratura [ 1416 ] , 142 sono state classi cate istologicamente come b3 e 8 come b4 . 
tra i 142 casi risultati b3 , 118 ( 83 , 1% ) sono stati sottoposti a veri ca chirurgica : in 112 / 118 casi ( 94 , 9% ) lesame istologico de nitivo ha confermato lesito della vacb di lesioni proliferative non neoplastiche , mentre in 6 casi ( 5 , 1% ) lesame de nitivo stato di carcinoma duttale in situ ( cdis )  . 
tutti questi 6 casi presentavano nei campioni prelevati con la vacb neoplasia lobulare intraepiteliale ( lin ) pura o associata ( 3 casi ) ad altre lesioni proliferative a rischio . 
of the 150 proliferative lesions of uncertain malignant potential , also known as borderline lesions [ 1416 ] , 142 were histologically classi ed as b3 and 8 as b4 . 
among the 142 cases of b3 lesion , 118 ( 83.1% ) were subjected to diagnostic surgical excision : nal histology con rmed the vacb diagnosis of benign proliferative lesion in 112 / 118 cases ( 94.9% ) , whereas in 6 cases ( 5.1% ) , it resulted in a diagnosis of ductal carcinoma in situ ( dcis )  . 
all vacb specimens retrieved in these six cases showed evidence of lobular intraepithelial neoplasm ( lin ) in its pure form or associated with other indeterminate 8 / 602 casi ( 1 , 3% ) di lesioni b4 , tutti appartenenti alla categoria radiologica r4 , stata consigliata la veri ca chirurgica e lesame istopatologico de nitivo stato di lesione benigna . 
in tutti i casi stata confermata la malignit della lesione , tuttavia in 8 ( 10 , 1% ) pazienti la diagnosi su biopsia chirurgica stata di carcinoma invasivo , mentre alla vacb era stata fatta diagnosi di cdis ( tabelle 1 , 4 )  . 
in the other 8 / 602 cases ( 1.3% ) of b4 lesion ( all radiologically classi ed as r4 ) , surgical excision was recommended , and nal histology revealed benign disease . 
the 112 patients with b5 lesions underwent surgical excision , and malignancy was con rmed in all cases ; however , the nal diagnosis in 8 ( 10.1% ) patients was invasive carcinoma , in contrast with vacb that had provided a diagnosis if dcis ( tables 1 , 4 )  . 
given that the regional government reimbursement rate in piedmont is 750.00 euro for each vacb procedure ( ministerial decree 22 / 7 / 96 : 85.11.3 ) , there is substantial parity between the cost of the procedure and the reimbursement . 
la sensibilit della vacb rispetto allesame istologico de nitivo risultata del 94 , 9% ( 112 / 118 ) ( con un intervallo di con denza al 95% compreso tra 94% e 95 , 8% ) , la speci cit del 98 , 3% ( 476 / 484 ) ( con un intervallo di con denza al 95% compreso tra 97 , 8% e 98 , 8% ) , il valore predittivo positivo del 93 , 3% ( 112 / 120 ) , il valore predittivo negativo del 98 , 8% ( 476 / 482 ) , mentre laccuratezza del 97 , 7% ( 588 / 602 )  . 
negli ultimi 5 anni presso il nostro centro sono state complessivamente evitate 335 biopsie chirurgiche su lesioni con rischio radiologico r3 - r4 ; il risparmio complessivo risultato pari a 155440 , 00 euro , corrispondente ad un risparmio annuo di 31088 , 00 euro . discussione le microcalci cazioni rappresentano una buona parte dei segni mammogra ci legati a lesioni del parenchima radiol med ( 2011 ) 116 : 477488 fig . 
1a , b cluster of heterogeneous calci cations , some rounded , with a maximal extension of 6 mm ( bi - rads r3 ) : craniocaudal ( a ) and mediolateral oblique ( b ) magni cation views . 
1a , b gruppo di microcalci cazioni eterogenee , alcune delle quali rotonde , con estensione di 6 mm ( bi - rads r3 ) : ingrandimento mirato nella proiezione cranio - caudale ( a ) e medio - laterale obliqua ( b )  . 
up to 80 morphological descriptors have , in fact , been reported in the literature , with the result that the standardisation of mammographic diagnosis is dif cult [ 12 , 17 , 18 ]  . 
the advent of cnb with manual or semiautomatic devices has substantially improved diagnostic accuracy in microcalci cation clusters , even though a considerable proportion of biopsies still prove to be nondiagnostic or discordant with the radiological classi cation [ 8 , 19 , 20 ]  . although fnac and cnb may represent a good alternative to diagnostic surgical biopsy , neither of them provides conclusive results in all cases . 
con lintroduzione della core needle biopsy mediante dispositivi manuali o semiautomatici , laccuratezza nella diagnosi di natura dei clusters di microcalci cazioni sensibilmente migliorata , pur rimanendo consistente le quota di prelievi non diagnostici o in disaccordo con lipotesi radiologica [ 8 , 19 , 20 ]  . entrambe le metodiche , fnac e cnb , pur rappresentando una buona alternativa alla biopsia chirurgica diagnostica , non sono sempre risolutive . 
 stato dibattuto in letteratura il ricorso ad agobiopsia percutanea come primo approccio a lesioni classi cate bi - rads r3 ( per le quali lacr raccomanda un monitoraggio di almeno 6 mesi )  . 
tuttavia , nel caso delle microcalci cazioni r3 sottoposte a vacb stata osservata in letteratura una malignit variabile tra 0% e 19% , mentre nella nostra casistica stata del 7 , 4% , percentuale bassa ma non trascurabile , che ci pare giusti chi il prelievo ago bioptico [ 1 , 6 , 2123 ]  . 
nei casi classi cati come bi - rads r4 , la malignit riscontrata allesame istologico de nitivo stata del 25 , 1% , similmente ad altre casistiche ( intervallo dal 15 , 3% al 36 , 6% ) radiol med ( 2011 ) 116 : 477488 484 fig . 
2a - c cluster of pleomorphic calci cations , some granular , with a maximal extension of 15 mm ( bi - rads r4 ) , close to the surgical scar in a patient who previously underwent surgical excision for cribriform ductal carcinoma in situ ( dcis ) : craniocaudal ( a ) and mediolateral oblique ( b ) magni cation views . 
stereotactic 11 - gauge vacb result [ magni cation view of specimens with calci cations ( c ) ] : breast parenchyma with intraductal calci cations ( b2 ) [ 13 ]  . 
2a - c gruppo di microcalci cazioni pleomorfe , alcune delle quali granulari , con estensione di 15 mm , localizzate in prossimit della cicatrice chirurgica , in paziente precedentemente sottoposta ad escissione ampia per cdis cribriforme ( bi - rads r4 ) : ingrandimento mirato nella proiezione cranio - caudale ( a ) e medio - laterale obliqua ( b )  . 
 stata eseguita vacb ( radiogramma di alcuni dei frustoli prelevati , comprendenti le microcalci cazioni [ c ] ) con esito microistologico di : frustoli di parenchima mammario con calci cazioni intraduttali ( b2 ) [ 13 ]  . 
however , in the case of r3 microcalci cations sampled with vacb , the literature reports a rate of malignancy ranging from 0% to 19% as against 7.4% in our series , a low but not negligible rate , which we believe justi es a needle biopsy [ 1 , 6 , 2123 ]  . 
in cases classi ed as bi - rads r4 , the rate of malignant disease at nal histology was 25.1% , consistent with previous reports ( range 15.3%36.6% ) [ 6 , 21 , 22 ]  . 
 the bi - rads r5 lesions ( 2.2% ) studied by vacb were characterised by casting microcalci cations not associated with opacities for which fnac and cnb had proven insuf cient ( c1 and b1 )  . 
as reported by previous studies in which casting microcalci cations accounted for 19% of the entire series [ 1 , 6 , 2123 ] , these lesions do not constitute an elective indication for the use of vacb . 
data indicate that microcalci cations classi ed as probably benign were con rmed as such in the majority of cases , whereas the concordance in suspicious cases tended to be lower , [ 6 , 21 , 22 ]  . 
i casi classi cati bi - rads r5 ( 2 , 2% ) sottoposti a vacb seguivano a microcalci cazioni a stampo , non associate ad opacit , per le quali la fnac e la cnb non avevano fornito unadeguata risposta diagnostica ( c1 e b1 ) ; questo tipo di lesioni , similmente a quanto riportato in altri studi , in cui costituivano generalmente dall1% al 9% di tutta la casistica [ 1 , 6 , 2123 ] , non trovano indicazione elettiva allutilizzo della vacb . 
da questi dati si rileva che le microcalci cazioni verosimilmente benigne nella maggior parte dei casi sono state confermate come tali , mentre nei casi sospetti la corrispondenza risultata minore , poich stato comunque trovato un numero considerevole di lesioni benigne . 
il dato morfologico nella categoria bi - rads r4 non trova , infatti , una correlazione con leffettivo risultato istologico : le lesioni maligne corrispondevano prevalentemente a microcalci cazioni con morfologia granulare o nemente pleomorfa , ma anche una buona parte di lesioni benigne presentava tale tipo di morfologia . 
3a , b cluster of pleomorphic calci cations with a maximal extension of 8 mm ( bi - rads r4 ) in a 35 - year - old patient at rst mammography : craniocaudal ( a ) and mediolateral oblique ( b ) magni cation views . 
3a , b gruppo di microcalci cazioni pleomorfe , con estensione di 8 mm ( bi - rads r4 ) riscontrato alla prima mammogra a in paziente di 35 anni con familiarit : ingrandimento mirato nella proiezione cranio - caudale ( a ) e medio - laterale obliqua ( b )  . 
stata eseguita vacb con esito microistologico di cdis di tipo cribriforme micropapillare ( b5a ) [ 13 ] , confermato allesame istologico de nitivo . with many lesions proving to be benign . 
the morphological appearance of bi - rads r4 lesions does not correlate with the histological result : malignant lesions mainly corresponded to granular or ne pleomorphic calci cations , features that were also present in a large number of benign lesions . 
of particular signi cance are the 337 cases in which vacb with the mammotome device demonstrated the benign nature of the microcalci cations , allowing them to be classi ed as b2 . 
avoidance of surgical biopsies thanks to vacb demonstration of the benign nature of the microcalci cations led to considerable economic savings ( 31 , 088.00 euro / year )  . 
even if cost savings are of limited signi cance in themselves , one cannot neglect the savings in terms of time and occupation of the operating rooms and the lower psychological impact of a minimally invasive needle biopsy . 
in our experience , a microhistological diagnosis of borderline lesion was established in 24.9% of cases ( 150 / 602 ) , a higher percentage than reported in other studies ( range 8.1%12% ) [ 1 , 6 ]  . 
 laccuratezza della vacb nella nostra casistica risultata elevata : sensibilit e speci cit sono state rispettivamente del 94 , 9% e 98 , 3% , in linea con i valori riportati in letteratura ( sensibilit 87 , 5%99% , speci cit 86 , 9% 100% ) ( tabella 5 ) [ 2 , 6 , 19 , 24 , 25 ]  . 
le biopsie chirurgiche evitate in seguito a dimostrazione della natura benigna delle microcalci cazioni mediante vacb hanno determinato un discreto risparmio economico ( 31088 , 00 euro / anno )  . 
se il dato economico appare di per s poco signi cativo , non di meno deve essere considerato il risparmio in termini di tempo ed impegno delle sale operatorie e limpatto psicologico sulla paziente , sicuramente inferiore per unagobiopsia mini - invasiva . 
meritevoli di considerazione sono le lesioni classi cate istologicamente come b3 ( lesioni proliferative di incerto signi cato ) : nella nostra esperienza il riscontro microistologico di lpr risultato pari al 24 , 9% dei casi ( 150 / 602 ) , percentuale superiore a quella di altri studi ( valori compresi tra 8 , 1% ed 12% ) [ 1 , 6 ]  . 
 la discussione multidisciplinare che prende in considerazione aspetti clinici , anamnestici , il quadro radiologico e le caratteristiche istologiche di questi casi fondamentale 486 radiol med ( 2011 ) 116 : 477488 table 5 sensitivity and speci city of vacuum - assisted core biopsy ( vacb ) : comparison with the literature study author ( year ) sensitivity ( 95% ci ) speci city ( 95% ci ) no . 
this may have been due to the selection of lesions to be sampled by vacb , as > 95% of them had microcalci cations as the only mammographic sign , in contrast to other studies that included a greater proportion of opacities , distortions and asimmetric densities either alone or associated with microcalci cations [ 46 ]  . 
it should be noted , however , that the sensitivity of mr imaging for in situ lesions , especially if low grade , is not as high as that reported for invasive lesions . the limitations of vacb in our experience were similar to those reported by other studies [ 3134 ] and consist of the possibility of underestimating proliferative lesions of uncertain malignant potential ( b3 ) and malignant lesions in situ . per la corretta gestione della paziente [ 16 , 2628 ]  . 
nella nostra casistica abbiano riscontrato un basso tasso di malignit nelle diagnosi di b3 ( 4% ) rispetto ad altri studi ( 9%15% dei casi ) ; questo dato potrebbe essere dovuto alla selezione delle lesioni da sottoporre a vacb , costituite nella nostra serie in oltre il 95% dei casi da microcalci cazioni come unico segno mammogra co , a differenza di altri studi in cui sono state incluse una maggior quota di lesioni rappresentate da opacit , distorsioni ed addensamenti come uniche lesioni , oppure associate a microcalci cazioni [ 46 ]  . 
nella maggior parte di b3 , abbiamo riscontrato un quadro microistologico di lesioni miste ; la variabile malignit associata e leterogeneit microistologica hanno comportato nella maggior parte dei casi unindicazione alla veri ca chirurgica e solo nei casi con completa escissione delle microcalci cazioni ( radiologicamente confermata ) ( 16% ) al follow - up clinico - radiologico [ 29 ]  . in tal senso , studi preliminari sembrano suggerire che anche limpiego della risonanza magnetica nella valutazione delle lpr diagnosticate microistologicamente possa essere molto utile nellescludere la presenza di patologia maligna associata , con un valore predittivo negativo del 98 , 2% [ 30 ] ( tenendo conto tuttavia che la sensibilit della risonanza per le lesioni in situ , soprattutto se di basso grado , non cos elevata come per le lesioni invasive )  . come emerge da altri studi in letteratura [ 3134 ] , anche nella nostra esperienza i limiti della procedura vacb sono stati costituiti dalla possibilit di sottostima nelle lesioni proliferative a rischio ( b3 ) e nelle lesioni maligne in situ . radiol med ( 2011 ) 116 : 477488 conclusions conclusioni vacb with the mammotome device is an accurate method for characterising microcalci cations at low and intermediate risk of malignancy at radiology , obviating the need for surgery in more than half of the cases with benign results at vacb . 
the effective economic and logistic savings of the operating theatres justi es the use of vacb , even though it is more expensive that conventional core biopsy with semiautomatic devices . la vacb con sistema mammotome risultata una metodica accurata nella caratterizzazione di microcalci cazioni a basso e medio rischio radiologico , evitando lintervento chirurgico in oltre la met dei casi risultati benigni alla vacb . 
di radiologia , dipartimento di scienze mediche , tecnologiche e traslazionali , azienda ospedaliero - universitaria di trieste , strada di fiume 447 , 34149 trieste , italy correspondence to : p . 
image quality was analysed in terms of spatial and contrast resolution on several scans of a phantom performed with automatic dose modulation and different reconstruction kernels and accepted noise level . 
ctu cannot be considered a standard examination : the scan parameters need to be adapted to the image quality required for the speci c clinical problem . keywords multislice computed tomography urography radiation dose reconstruction kernel riassunto obiettivo . 
stata analizzata la qualit di immagine in termini di risoluzione spaziale e di contrasto di diverse scansioni su fantoccio , ripetute con modulazione automatica di dose , variando il ltro di ricostruzione e il livello di rumore accettato ; sono stati valutati i valori di esposizione e confrontato lesito con quanto osservato in 52 pazienti sottoposti ad esame uro - tc . 
la dose di esposizione e la qualit dimmagine variano notevolmente modi cando i parametri di ricostruzione , sebbene non sempre laumento di dose comporti un reale vantaggio in termini di de nizione dimmagine . 
luro - tc non pu essere considerato un esame standardizzato : i parametri di scansione devono essere sempre valutati e modulati in base alla qualit di immagine richiesta dallo speci co problema clinico . parole chiave tomogra a computerizzata multistrato uro - tc dosimetria filtri di ricostruzione introduction introduzione computed tomography urography ( ctu ) is a diagnostic examination optimized for imaging the kidneys , ureters and luro - tomogra a computerizzata ( tc ) un esame diagnostico ottimizzato per limaging dei reni , degli ureteri e della 418 radiol med ( 2011 ) 116 : 417431 bladder . 
the examination involves the use of multidetector ct with thin - slice imaging , intravenous administration of a contrast medium , and imaging in the excretory phase [ 1 ]  . 
 the high resolution provided by the modern multidetector ct ( mdct ) systems allows for the depiction of ndings < 5 mm [ 2 ] and consequently the assessment not only of anatomical variants of the urinary system but also of very early stage in ammatory or neoplastic diseases . 
according to the published data on radiation dose , a ctu protocol involving four acquisition phases ( unenhanced , arterial , parenchymal and excretory ) exposes the patient to a dose of 2535 msv , as against a mean dose for conventional urography of about 5 msv , a dose that varies widely , however , depending on the indication and the operators experience [ 1 , 36 ]  . 
ctu optimisation entails the use of protocols with fewer scans , allowing the dose to be reduced to values of around 10 msv for two - phase protocols ( unenhanced and combined nephrographic and excretory phase ) or even lower values when the study is limited to the combined nephrographic and excretory phase or corticomedullary , nephrographic and excretory phase [ 7 ]  . 
 in 1995 it was calculated that , although accounting for < 5% of all imaging studies , ct examinations contributed 40% of the collective dose to the population from medical x - rays [ 8 ]  . 
therefore , when planning a ct examination , attention should be given as far as possible to reducing radiation dose in accordance with the as low as reasonably acceptable ( alara ) principle established by the international commission on radiological protection ( icrp ) [ 9 ]  . 
to monitor the radiation dose delivered to the patient during a ct examination , two radiation dose indices can be used : the computed tomography dose index ( ctdi ) and the dose - length product ( dlp )  . 
ctdi evaluation can be obtained with a pencil chamber placed inside a standard ct dosimetry phanto weighted ctdi ( ctdiw ) takes into account the different exposure at the periphery and centre of the anatomical region being studied , whereas dlp corresponds to ctdi multiplied by scan length . 
it should be noted that the ctdiw and dlp values are dose estimates that refer to standard - sized dosimetry phantoms rather than to the real size of the patient , so that the dose may be underestimated in thin patients and overestimated in larger patients . 
an estimate of these two values for each examination setup should be displayed on the operators console in accordance with the safety requirements for vescica , che necessita luso di unapparecchiatura tc multidetettore , con acquisizione di immagini a strato sottile , somministrazione endovenosa di mezzo di contrasto ed una scansione ottenuta in fase escretoria [ 1 ]  . 
lelevata risoluzione spaziale offerta dagli attuali sistemi tc multidetettore permette il riconoscimento di reperti di dimensioni inferiori ai 5 mm [ 2 ] e , quindi , lo studio non solo di varianti anatomiche dellapparato urinario , ma anche di condizioni in ammatorie o neoplastiche in fase iniziale . 
luro - tc , in particolare quando eseguita con tecnica multifasica , un esame ad elevata dose di radiazioni ed attualmente questo il vero problema che ne pu limitare lutilizzo . 
in base ai dati di dosimetria desunti dalla letteratura , un protocollo uro - tc che prevede quattro fasi ( diretta , arteriosa , parenchimale ed escretrice ) espone il paziente ad una dose stimabile di 2535 msv , a fronte di una dose media in urogra a tradizionale , pur estremamente variabile in base ai reperti valutati ed allesperienza delloperatore , di circa 5 msv [ 1 , 36 ]  . 
lottimizzazione delluro - tc prevede lutilizzo di protocolli a minor numero di scansioni con diminuzione della dose no a valori di circa 10 msv , per protocolli a due fasi ( diretta e combinata nefro - escretoria ) , o anche inferiori qualora si possa limitare lesame alla sola fase combinata nefro - escretoria o corticomidollare - nefro - escretoria [ 7 ]  . 
 gi nel 1995 si era calcolato che gli esami tc , pur rappresentando meno del 5% di tutti gli esami radiologici , erano responsabili del 40% della dose di esposizione della popolazione alle radiazioni ionizzanti per scopo medico [ 8 ]  . 
negli ultimi decenni la diffusione degli esami tc aumentata esponenzialmente e , di conseguenza , anche il suo impatto sullesposizione , pertanto in fase di piani cazione dellesame necessario focalizzare lattenzione , per quanto possibile , sul risparmio di dose , in linea con il principio di ottimizzazione sancito dallinternational commission on radiological protection ( icrp ) [ 9 ]  . 
per monitorare la dose di radiazioni cui viene sottoposto un paziente durante lesecuzione di un esame tc si possono usare due indicatori di dose il computed tomography dose index ( ctdi ) e il dose lenght product ( dlp )  . 
il ctdi pesato ( ctdiw ) considera la diversa esposizione in periferia e al centro della regione anatomica in corso di studio , mentre il dlp corrisponde al prodotto del ctdi e dellestensione della scansione . 
 da notare come i valori di ctdiw e di dlp siano stime di dose che si riferiscono a fantocci di dimensione ssa , che non tengono in considerazione le reali dimensioni del paziente , con una conseguente sottostima di dose nei pazienti magri ed una sovrastima in quelli con maggiore massa corporea . 
la stima di questi due valori per radiol med ( 2011 ) 116 : 417431 ct systems issued by the international electrotechnical commission ( iec ) [ 10 ]  . in multislice ct , radiation exposure depends on image acquisition and reconstruction parameters . 
on current ct systems the user needs only to select the image quality , which is determined by the reconstruction lter or kernel , slice thickness and accepted noise level . 
once image quality has been selected , the system automatically delivers the optimal tube current for the type of image , calculated on the basis of the density and thickness values obtained with the scout images according to preset maximum threshold values , which cannot be exceeded . 
modulation may be activated along the z axis or in the x - y plane , depending on the how advanced the system is . the aim of this study was to evaluate the possibilities of optimising the ctu examination by modulating reconstruction parameters on the basis of acquisitions performed on a phantom and data from our clinical practice . materials and methods phantom study to evaluate dose and image quality , we imaged a catphan 600 phantom ( phantom laboratory , greenwich , ny , usa ) with repeated scans using a 64 - slice ct system ( aquilion 64 , toshiba medical systems , tokyo , japan )  . 
acquisition parameters were : collimation 640.5 mm , pitch 0.828 , 120 kv , automatic z - axis tube - current modulation based on the scout image using sure exposure software . 
moreover , a scan was acquired with the low - dose protocol suggested by the ciascuna impostazione desame deve essere indicata sulla consolle del tecnico operatore , secondo le speci che per la sicurezza delle apparecchiature tc della international electrotechnical commission ( iec ) [ 10 ]  . in tc multistrato lesposizione a radiazioni del paziente dipende dai parametri di acquisizione e dai parametri di ricostruzione . 
le attuali apparecchiature tc vengono fornite di alcuni software ef caci nella riduzione della dose , come la modulazione automatica dellerogazione della corrente al tubo e i ltri anti - rumore . 
la modulazione automatica della corrente una metodica che consente di adattare la corrente in modo continuo in base alle caratteristiche della regione bersaglio durante la rotazione del tubo [ 11 , 12 ]  . 
nei sistemi tc attuali , sulla consolle deve essere solamente selezionata la qualit di immagine , dipendente dal tipo di ltro o kernel di ricostruzione , dallo spessore di strato e dal livello di rumore che si disposti ad accettare , ed automaticamente viene erogata una corrente al tubo ottimale per quel tipo di immagine , calcolata sulla base delle informazioni di densit e spessore ottenibili dalle immagini scout , secondo valori di soglia massima preimpostati , che comunque non devono essere superati . 
la modulazione pu essere attivata solo lungo lasse z o anche sul piano xy , secondo levoluzione dellapparecchiatura . il nostro studio si propone di valutare le possibilit di ottimizzazione dellesame uro - tc modulando i parametri di ricostruzione mediante acquisizioni su fantoccio e sulla base dei dati registrati nella nostra casistica quotidiana . materiali e metodi studio su fantoccio per la valutazione dosimetrica e di qualit di immagine stato eseguito uno studio su fantoccio tipo catphan 600 ( the phantom laboratory incorporated , greenwich , ny , usa ) sottoposto a scansioni ripetute con apparecchiatura tc a 64 strati ( aquilion 64 , toshiba medical systems , tokyo )  . 
sono stati utilizzati i seguenti parametri di acquisizione : collimazione 640 , 5 mm , pitch 0 , 828 , 120 kv , corrente modulata automaticamente in base allimmagine scout dal software di modulazione automatica ( sure exposure ) sullasse z . 
le immagini assiali sono state ricostruite a spessore di 5 mm , il volume di immagini per le ricostruzioni multiplanari ( mpr ) e volumetriche stato ricostruito a 0 , 5 mm con intervallo di ricostruzione di 0 , 3 mla variazione dei parametri ha interessato unicamente i ltri di ricostruzione e la deviazione standard ( rumore ) accettata . 
sono stati utilizzati rispettivamente il ltro di ricostruzione 11 , corri420 radiol med ( 2011 ) 116 : 417431 manufacturer for studying renal colic , which corresponds to a kernel fc11 with an accepted sd of 15 , to which q01 ( smooth ) noise ltration was applied . 
the ctdiw * is a derived parameter that represents the ctdiw product , the number of detector rows and slice thickness divided by the table feed per rotation . data analysis image volumes were sent to a vitrea version 4.1.2.0 workstation ( vital images inc . , minnetonka , mn , usa ) and evaluated at a slice thickness of 3 mm in the same viewing conditions by two operators with different levels of experience ( 4 and 7 years )  . 
stata inoltre eseguita una scansione con il protocollo low - dose , suggerito dalla ditta costruttrice per lo studio della colica renale , che corrisponde ad un ltro 11 con deviazione standard accettata 15 , a cui applicato il ltro anti - rumore tipo q01 ( smooth )  . 
il ctdiw * un parametro derivato che rappresenta il prodotto del ctdiw , del numero di righe di detettori e dello spessore di strato impostato rapportato al movimento del lettino per rotazione . analisi dei dati i volumi di immagini ottenuti sono stati inviati alla consolle di ricostruzione vitrea versione 4.1.2.0 ( vital images inc . , minnetonka , minnesota , usa ) e valutati ad uno spessore di strato di 3 mm da due operatori con diversa esperienza fig . 
nearly all patients underwent a preliminary low - dose scan at 120 kv with automatic tube - current modulation , extending from the upper pole of the kidney to the base of the bladder . 
for the contrast - enhanced scan , patients received a diuretic injection and were subsequently imaged with the split - bolus technique consisting of a rst injection of 400 mgi kg contrast medium at a rate of 2 ml / s , followed by an interval of 7 min and a second bolus of 200 mgi kg at 2 ml / s . 
assuming as a reasonable approximation that the ctdiw * and dlp values correlate linearly with the bsa , we normalised the values obtained for the bsa and calculated the ctdiw * and dlp derived from these mean values for a theoretical patient with a bsa of 1.8181 , corresponding to the standard patient ( 170 cm tall and 70 kg )  . 
using the conversion factor obtained with the monte carlo method indicated in the european guidelines on quality criteria for computed tomography ( eur 16262 ) [ 13 ] , the effective dose for each scan was calculated in this standard patient . results ctdiw * values recorded on the phantom in the different scans ( table 1 ) demonstrated that , the reconstruction kernel being equal , the tube current selected by the autoradiologica ( 4 e 7 anni ) alle medesime condizioni di visualizzazione . 
in quasi tutti i pazienti stata acquisita una preliminare scansione diretta low - dose , a 120 kv e con modulazione automatica della corrente , estesa dal polo superiore dei reni alla base vescicale . 
 per la scansione contrastogra ca stato utilizzato il metodo split - bolus dopo iniezione di diuretico , con una prima iniezione di mezzo di contrasto di 400 mgi pro kg a 2 ml / s seguita da una pausa di 7 minuti e quindi un secondo bolo di 200 mgi pro kg a 2 ml / s . 
le immagini assiali sono state ricostruite a spessore di 5 mm , il volume di immagini per le ricostruzioni mpr e volumetriche stato ricostruito a 0 , 5 mm con intervallo di ricostruzione di 0 , 3 mm . per ciascun gruppo di pazienti stato calcolato il valore medio di dlp , di ctdiw * e di body surface area ( bsa ) , utilizzando la formula di mosteller [ ( cm * kg ) / 3600 ]  . 
assumendo come approssimazione accettabile che i valori di ctdiw * e di dlp siano correlati in modo lineare con il bsa , i valori ottenuti sono stati normalizzati per il bsa e sono stati calcolati il ctdiw * e il dlp derivabili da questi dati medi per un teorico paziente con bsa pari a 1 , 8181 , corrispondente al paziente tipo di 170 cm e 70 kg . 
2a - d ricostruzione mip ( a , c ) e cmpr lungo il decorso delluretere destro ( b , d ) di due esami uro - tc normali eseguiti con ltro di ricostruzione 11 ( a , b ) e 13 ( c , d )  . matic modulation system increased with decreasing sd . 
 the corresponding ctdiw * values were then compared with one another using as a standard the scan performed with kernel fc13 and sd 12.5 , which represents the scan setting most commonly used for ctu at our institution ( table 2 )  . 
assessment of image quality by the two readers was concordant as regards the detectability of both the highand low - contrast objects ( table 3 )  . in the 52 patients undergoing ctu for whom the recorded dlp and ctdiw * values were displayed on the operator console , the calculated mean dpl and ctdiw * were 306.27 mgy * cm and 10.21 mgy , respectively , for the unenhanced low - dose scan . 
the nephrographicexcretory scan performed with a reconstruction kernel fc11 involved a mean dlp of 313.76 mgy * cm and ctdiw * of il metodo monte carlo tratto da european guidelines of quality criteria for computer tomography ( eur 16262 ) [ 13 ] , sono stati calcolati i valori di dose ef cace in questo paziente tipo derivante per ciascuna scansione . risultati i valori di ctdiw * registrati sul fantoccio nelle diverse scansioni eseguite , riassunti nella tabella 1 , dimostrano , a parit di ltro di ricostruzione , un aumento della corrente al tubo radiogeno selezionata dal modulatore automatico al diminuire della deviazione standard accettata . 
i valori di ctdiw * corrispondenti sono stati poi confrontati fra loro usando come standard la scansione con ltro 13 e deviaradiol med ( 2011 ) 116 : 417431 fig . 
 the mean bsa value of all patients was 1.8654 , whereas that of patients imaged with kernel fc11 was 1.7747 and that of patients imaged with kernel fc13 was 1.8849. 
la valutazione della qualit di immagine stata concorde per i due osservatori sia per la distinzione degli elementi ad alto contrasto sia per la riconoscibilit delle sfere a basso contrasto ( tabella 3 )  . nei 52 pazienti sottoposti ad esame uro - tc di cui possediamo la registrazione dei valori di dlp e di ctdiw * presentati sulla consolle delloperatore stato calcolato per la scansione diretta low - dose un dlp medio pari a 306 , 27 mgy * cm e un valore di ctdiw * pari a 10 , 21 mgy . 
 la scansione nefro - escretoria eseguita con ltro di ricostruzione 11 ha comportato per il paziente in media un dlp di 313 , 76 mgy * cm e un ctdiw * di 10 , 08 mgy , mentre la scansione nefro - escretoria eseguita con ltro di ricostruzione 13 ha comportato in media un dlp di 733 , 61 mgy * cm e un ctdiw * di 22 , 16 mgy . 
il valore di bsa medio di tutti i pazienti corrisponde a 1 , 8654 , quello dei pazienti in cui stato usato il ltro 11 a 1 , 7747 e quello dei pazienti in cui stato usato il ltro 13 a 1 , 8849 . 
 i valori di dlp e di ctdiw * della scansione low - dose nei pazienti in cui stata poi eseguita la scansione nefro - escretoria con ltro 11 corrispondono a 234 , 74 mgy * cm e 8 , 22 mgy rispettivamente . 
in base ai valori di dlp e di ctdiw * medi sono stati calcolati i valori di dlp e di ctdiw * medi normalizzati per il bsa dei singoli gruppi , corrispondenti a 164 , 18 mgy * cm , 176 , 79 mgy * cm e 389 , 20 mgy * cm e 5 , 47 mgy , 5 , 67 mgy e 11 , 75 mgy rispettivamente per le scansioni low - dose , contrastogra che con ltro 11 e con ltro 13 . 
sono stati , quindi , calcolati i valori di dlp e ctdiw * per il paziente tipo , partendo dai valori medi , corrispondenti a 298 , 50 mgy * cm , 321 , 43 mgy * cm e 707 , 61 mgy * cm e 9 , 94 mgy , 10 , 32 mgy e 21 , 37 mgy rispettivamente , come riassunto in tabella 4 ed illustrato nelle figure 4 e 5 . nella nostra casistica si presentato un paziente con perfetta corrispondenza al paziente tipo ( 170 cm e 70 kg )  . 
in un lavoro del 2004 si dimostrato come la maggior parte dei radiologi non sia in grado di fornire una stima della dose di esposizione derivante da un esame tc [ 20 ]  . 
using a published conversion factor [ 13 ] , we estimated the effective dose for each scan in this patient , obtaining a value of 4.8 msv for the low - dose scan , 6.2 msv for the nephrographicexcretory phase with kernel fc11 and a value of 12.7 msv for the nephrographicexcretory scan with kernel fc13 . discussion although the radiology literature has always paid attention to the issue of dosimetry [ 1419 ] , there appears to be little collective awareness of the risks connected to radiation among the medical and radiological community . 
while awaiting the results of a study investigating the real risk of cancer resulting from ct [ 21 ] , it should be recalled that this modality iniziato sul reale rischio di cancro connesso alla tc [ 21 ] , questo va considerato un esame ad alta dose di radiazioni e con potenziale rischio di carcinogenesi , molto pi elevato di quello derivante dalle altre pratiche radiologiche , ed in quanto tale da utilizzare solo quando realmente necessario e nel modo pi appropriato , ricordando di ridurre la dose di esposizione , per quanto possibile . 
in tc multistrato lesposizione a radiazioni del paziente dipende dai parametri di acquisizione e dai parametri di ricostruzione . la maggior parte dei sistemi tc viene preimpostata nello studio delladdome con un voltaggio del tubo radiogeno , per un paziente di media corporatura , pari a 120 kv . 
 [ 19 ] hanno pubblicato uno studio su fantoccio in cui hanno dimostrato una riduzione di dose del 60% impostando il tubo a 80 kv , ma tale protocollo risultato utilizzabile solo quando si studiano elementi ad elevato contrasto , mentre il rumore risulta eccessivo per poter avere una buona sensibilit nellindividuazione delle piccole neoplasie intrarenali o intraureterali . 
la selezione dei valori di corrente erogata al tubo varia molto in letteratura a seconda dei diversi gruppi di studio e dipende fortemente dal numero di strati dellapparecchiatura tc e dallo spessore di strato impostato [ 1 , 3 , radiol med ( 2011 ) 116 : 417431 delivers a high radiation dose with a potential risk of carcinogenesis , which far exceeds that deriving from other radiological procedures . 
as a consequence , ct should be used only when truly necessary and in the most appropriate manner , taking care to minimise the radiation dose as far as possible . in mdct radiation dose depends on acquisition and reconstruction parameters . 
 [ 19 ] published a phantom study in which they demonstrated a 60% dose reduction by setting the tube voltage at 80 kv , but this protocol was found to be utilisable only for studying highcontrast elements , the noise level being too high to achieve good sensitivity for detecting small renal or ureteral neoplasms . 
tube current settings vary widely in the literature and are heavily dependent on the number of detector rows and slice thickness used [ 1 , 3 , 6 ]  . 
spatial resolution in the x - y plane is in uenced by the size of the eld of view and kernel and corresponds to approximately 0.70.8 mm per standardor medium - smooth kernel in the abdomen , but it is also dependent on slice thickness due to presence of partial volume effect [ 8 , 18 ]  . 
clearly , to obtain higher contrast resolution along with improved spatial resolution , a greater amount of current needs to be delivered to reduce quantum noise by increasing the number of incident photons on the detector [ 8 ]  . in addition to modulating the scan parameters , the radiologist can limit the number of scans to be obtained , for example , by using the split - bolus or triple - bolus technique to obtain both angionephrographic and excretory information simultaneously [ 3 , 7 ]  . 
in our practice , ctu is not considered a standard examination , and the number of phases and scan parameters are always adapted to the patients age and to the clinical question being asked . 
 whenever possible , we omit the unenhanced scan and use the split - bolus technique to study both the parenchyma and urinary tract with a single scan ; only if clearly needed do we perform an additional scan , the extension of which is always limited to the equivocal nding . 
il pitch pu essere abbassato no a 0 , 50 , 7 , ottenendo cos maggiori informazioni sullasse z [ 18 ] , anche in questo caso , per , a costo di aumento di dose . 
la risoluzione spaziale sul piano xy in uenzata dalle dimensioni del eld of view ( fov ) e dal kernel e corrisponde a circa 0 , 70 , 8 mm per kernel di tipo standard o mediumsmooth nelladdome , ma dipende anche dallo spessore di strato , per la presenza delleffetto di volume parziale [ 8 , 18 ]  . 
 naturalmente per ottenere una risoluzione di contrasto pi elevata , con miglioramento anche della risoluzione spaziale , necessario erogare maggior corrente al tubo , per ridurre il disturbo del rumore quantico aumentando il numero di fotoni incidenti sul detettore [ 8 ]  . oltre ai parametri tecnici della singola scansione il medico pu agire limitando il numero di scansioni eseguite , ad esempio con lutilizzo della tecnica a doppio o triplo bolo di mezzo di contrasto , per ottenere simultaneamente sia informazioni angio - nefrogra che che escretorie [ 3 , 7 ]  . 
 nella nostra pratica clinica luro - tc non considerato un esame standardizzato , ma viene sempre modulato in base al quesito clinico e allet del paziente sia per quanto riguarda il numero di fasi che i parametri di scansione . 
quando possibile evitiamo di eseguire la scansione diretta e utilizzando la tecnica del doppio bolo otteniamo informazioni sia sul parenchima renale che sulla via escretrice con ununica scansione , riservando solo ai casi realmente necessari lesecuzione di un ulteriore scansione , comunque limitata per estensione allo studio del solo reperto dubbio . 
la scansione senza contrasto impostata sempre a bassa dose , secondo i parametri suggeriti dalla letteratura e dalla ditta costruttrice per lo studio della colica renale , cui corrisponde un valore di dlp nel reale paziente tipo di 170 cm e 70 kg di 284 mgy * cm e di dose ef cace di 4 , 8 msv . 
la scansione nefro - escretoria impostata con parametri differenziati in base al quesito clinico : quando si studiano anomalie anatomiche o patologie benigne caratterizzate da reperti non troppo minuti , viene impostata con ltro di ricostruzione 11 e deviazione standard accettata di 12 , 5 . 
il valore di dlp per il reale paziente tipo di 170 cm e 70 kg di 369 mgy * cm cui corrisponde una dose ef cace di 6 , 2 msv . 
per lo studio della patologia neoplastica e della papilla , il protocollo usato prevede 428 radiol med ( 2011 ) 116 : 417431 eters suggested by the literature and the system manufacturers for studying renal colic . 
the nephrographic - excretory phase is carried out with parameters that are differentiated according to the clinical question : for anatomical abnormalities or benign conditions characterised by ndings that are not excessively small , we use a scan setting with a reconstruction kernel fc11 and an accepted sd of 12.5. 
for studying neoplastic and papillary disease , the protocol involves the use of a kernel fc13 , again with an sd of 12.5 , which allows for less noise and better contrast , thus enabling the detection of small ndings as well . 
as can be noted , the scan done with reconstruction kernel fc13 delivers twice the dose of the scan with kernel fc11 and should thus only be used when absolutely necessary , at least in young patients . 
 when observing data on mean dose in patients undergoing ctu , we noticed that the patients forming the two subgroups were heterogeneous in size : mean bsa of patients studied with kernel fc11 was 1.7587 , whereas that of patients studied with kernel fc13 was 1.8849 , with an overall mean value of 1.8654. 
 to coherently compare the two settings of the contrastenhanced scan , we decided to normalise the dose values to the patients bsa , assuming as a reasonable approximation an undemonstrated linear correlation between bsa variation and dose variation effected by the automatic modulation syste dlp and ctdiw * for the standard patient ( 170 cm and 70 kg ) were derived from the values obtained . in the dosimetric evaluation , it should be noted that the scan range was not uniform in the different techniques : in fact , the unenhanced scan and the contrast - enhanced scan performed with kernel fc11 extended from the upper pole of the kidney to the bladder base , whereas the contrastenhanced scan extended from the hepatic dome to the pubic symphysis in almost all cases . 
 lutilizzo del ltro 13 , sempre con deviazione standard 12 , 5 , che fornisce immagini meno rumorose e , quindi , con miglior de nizione di contrasto , tale da consentire il riconoscimento anche di piccoli reperti . 
ovviamente , per ottenere questa qualit diagnostica la corrente erogata al tubo maggiore e il valore di dlp per il reale paziente tipo di 170 cm e 70 kg di 747 mgy * cm con dose ef cace di 12 , 7 msv . 
come si pu notare la scansione eseguita con ltro 13 comporta per il paziente pi che un raddoppio della dose rispetto alla scansione con ltro 11 , quindi va usata , almeno nei pazienti giovani , solo in caso di reale necessit . 
 osservando i dati di dose media nei pazienti sottoposti ad esame uro - tc abbiamo notato come i pazienti appartenenti ai due sottogruppi non fossero omogenei quanto a dimensioni , infatti il bsa medio dei pazienti studiati con ltro 11 pari a 1 , 7587 e il bsa medio dei pazienti studiati mediante scansione con ltro 13 risulta pari a 1 , 8849 , con media complessiva di 1 , 8654 . 
 per una valutazione di confronto coerente fra le due impostazioni della scansione contrastogra ca si deciso di normalizzare i valori di dose al bsa dei pazienti , assumendo come stima accettabile una correlazione lineare , non dimostrata , fra variazione di bsa e variazione di dose attuata dal modulatore automatico . 
dai valori cos ottenuti stato calcolato il dlp e il ctdiw * per il teorico paziente di 170 cm e 70 kg . nella valutazione dosimetrica da notare come nelle diverse modalit il range di scansione non fosse uniforme , infatti nei pazienti la scansione diretta e la scansione contrastogra ca con ltro 11 sono state limitate dal polo renale superiore alla base vescicale , mentre la scansione contrastogra ca stata , quasi sempre , estesa dalla cupola epatica alla sin si pubica . 
le variazioni di ctdiw * e di dlp sul paziente tipo reale e sulla media dei pazienti appaiono comunque coerenti . dati gli elevati valori degli indicatori di dose nelle indagini in esame , abbiamo valutato la possibilit di cambiare le impostazioni di scansione , per veri care no a che punto la scelta di eseguire esami ad alta dose sia giusti cata dalla qualit diagnostica delle immagini . 
abbiamo veri cato che il rapporto di ctdiw * fra la modalit in ltro 11 e la modalit in ltro 13 risulta rispettivamente 0 , 46 su fantoccio , 0 , 48 sui dati medi normalizzati dei pazienti in esame e 0 , 5 sul paziente tipo reale . 
i valori si presentano , quindi , coerenti fra loro e pertanto in base alle valutazioni sui valori di ctdiw * ottenuti su fantoccio , possiamo ottenere una stima suf cientemente accurata della percentuale di risparmio o aumento di dose connesso alle varie modalit . 
nella scanradiol med ( 2011 ) 116 : 417431 given the high values of the dose indices , we assessed the possibility of changing the scan settings to verify to what extent the decision to perform high - dose examinations is justi ed by the diagnostic quality of the images . 
 we found that the ctdiw * between the technique using kernel fc11 and the technique using kernel fc13 was 0.46 on the phantom , 0.48 on the normalised mean data of the patients and 0.5 on the real standard patient . 
the values are therefore coherent with one another , so that the ctdiw * values obtained on the phantom provide a suf ciently correct estimate of the percentage of dose reduction or increase associated with the different techniques . 
in the low - dose scan ( kernel fc11 and sd 15 ) , application of the smooth denoising lter renders the images visually less noisy and more pleasing but reduces the perception of both highand low - contrast details and is therefore counterproductive , at least in the phantodetectability of highcontrast elements is very similar for all scans performed with a medium denoising lter , whether with reconstruction kernel fc11 ( corresponding to a smooth lter without correction for beam hardening ) or kernel fc13 ( corresponding to a standard medium - smooth lter without beam - hardening correction )  . 
clinical use of the contrastenhanced scan with kernel fc11 when studying ureteral morphology and lithiasis conditions requiring the evaluation of high - contrast structures therefore appears justied and in line with the alara principle , with estimated dose reductions of , respectively , 59% and 54% for techniques using accepted sd of 15 or 12.5 , compared with the standard setting kernel fc13 . all dosimetry studies performed on ctu to date have regarded the opaci ed ureter as a high - contrast structure [ 24 ]  . 
conversely , in view of the dilution of the contrast agent due to the diuretic administered to distend the ureter and distribute the contrast uniformly inside it , our study paid special attention to the evaluation of low - contrast objects . 
depiction of detail does not improve when the accepted noise level is lowered , whereas the dose increases by 10% compared with that associated with the use of the standard kernel fc13 . 
between the scans with an sd of 12.5 and 10 , there is no signi cant improvement in object detectability , even though the estimated increase in dose is around 27% in the less noisy scan . 
to see any improvement in image quality , the sd needs to be further decreased to values of 7.5 , which provide better de nition of edges without , however , improving detectasione a bassa dose ( ltro 11 e deviazione standard 15 ) lapplicazione del ltro antirumore di tipo smooth rende le immagini visivamente meno rumorose e quindi pi gradevoli , ma riduce la percezione sia dei dettagli ad elevato che a basso contrasto , risultando perci controproducente , almeno su fantoccio . 
la riconoscibilit degli elementi ad elevato contrasto sovrapponibile per tutte le scansioni eseguite con un ltro anti - rumore di tipo intermedio , sia con ltro di ricostruzione di tipo 11 , corrispondente ad un ltro smooth senza correzione per lindurimento del fascio radiante , che di tipo 13 , ltro intermedio standard - smooth , senza correzione per lindurimento del fascio radiante . 
luso clinico della scansione contrastogra ca con ltro 11 nello studio della morfologia ureterale e nella malattia litiasica , condizioni in cui si devono valutare strutture ad elevato contrasto , appare pertanto giusti cata e in linea con i principi di ottimizzazione , con un risparmio di dose stimabile , nei confronti dellimpostazione standard a ltro 13 , del 59% e 54% , nelle modalit con deviazione standard accettata rispettivamente di 15 o 12 , 5 . gli studi dosimetrici nora effettuati per la valutazione delluro - tc hanno sempre considerato luretere opacizzato come una struttura ad elevato contrasto [ 24 ]  . 
tenendo conto della diluizione del mezzo di contrasto apportata dalluso del diuretico , utile per ottenere unottimale distensione della via escretrice ed una distribuzione uniforme del contrasto in essa , nel nostro studio abbiamo , invece , posto particolare attenzione alla valutazione del visibilit degli oggetti a basso contrasto . 
la ricostruzione a ltro 11 consente una buona riconoscibilit dei dettagli nellimpostazione con ds 12 , 5 , che non migliora quando viene ridotto il rumore accettato , a fronte di un aumento di dose del 10% rispetto a quello richiesto per luso del ltro 13 standard , pertanto limpostazione di una deviazione standard cos ridotta non appare giusti cata . nelle scansioni eseguite con ltro 13 si osserva un miglioramento nella riconoscibilit degli oggetti a basso contrasto , che sono distinguibili no ad un diametro di 4 mm nelle scansioni con deviazione standard accettata uguale o inferiore a 12 , 5 . 
fra la scansione con deviazione standard di 12 , 5 e di 10 , a fronte di un aumento di dose di esposizione stimabile attorno al 27% nella scansione meno rumorosa , non si osserva un signi cativo miglioramento nella riconoscibilit degli oggetti . 
per osservare un miglioramento nella qualit delle immagini bisogna scendere ulteriormente con la deviazione standard , no a valori di 7 , 5 , ottenendo immagini che si presentano a contorni pi de niti ma che comunque non consentono di riconoscere un numero maggiore di elementi , pur con un aumento di dose che appare davvero considerevole , stimabile attorno al 118% . 
 da questi dati luso dellimpostazione a ltro 11 e ds 15 , con ltro antirumore di tipo intermedio appare un buon compromesso fra dose di esposizione e qualit dellimma430 radiol med ( 2011 ) 116 : 417431 bility ; the increase in dose is indeed very high around 118% . 
 on the basis of these data , using the setting with kernel fc11 with sd 15 and medium denoising lter appears to provide a good trade - off between dose and image quality on the phantom , in contrast with the settings used until now for the unenhanced scan . 
for the contrast - enhanced scan , the decision to use a reconstruction kernel fc11 or fc13 and intermediate accepted noise level ( sd 12.5 ) depending on the clinical question , appears adequate , whereas a further noise reduction provides no diagnostic advantage . conclusions any investigation involving exposure to ionising radiation should be performed after careful evaluation of the clinical indication to ensure that the investigation is justi ed and to select the most appropriate technique in accordance with the alara principle . 
conversely , application of an additional smooth denoising lter for the unenhanced low - dose scan does not appear bene cial , as more information can be gained with the scan performed with the same dose parameters but with the application of a medium lter . optimisation of the ctu study in clinical practice will need to start from the unenhanced scan : an effective dose of 4.8 msv for a scan that provides secondary information compared with the contrast - enhanced scan is not justi ed . 
 a possible immediate solution is to couple the detectors during acquisition , a setup that can also be used for the nephrographicexcretory scan , with a collimation of 321 mm instead of the current 640.5 mthe reconstruction index should never be lower than the spatial resolution in the x - y plane , as the voxels will be shorter in the z axis , and , since noise potentially increases with effective voxel size , the system is forced to deliver higher tube current to maintain the desired signal - to - noise ratio , leading to a 16 - fold increase in dose [ 25 ]  . subsequently , it will be necessary to evaluate image quality obtained with a lower voltage setting , as proposed by coppenrath et al . 
per la scansione contrastogra ca , la scelta nora attuata di un ltro di ricostruzione di tipo 11 o 13 e livello di rumore accettato intermedio ( deviazione standard 12 , 5 ) in base al quesito clinico , appare adeguata , mentre unulteriore riduzione del rumore non comporta un guadagno diagnostico . conclusioni ogni indagine che richiede unesposizione a radiazioni ionizzanti deve essere eseguita dopo attenta valutazione del caso clinico , per accertare la giusti cazione dellesame stesso e valutare la migliore tecnica nel rispetto del principio dellottimizzazione . 
ci tanto pi vero per luro - tc , il cui limite principale la dose di radiazioni relativamente elevata cui il paziente sottoposto , che comporta valori di dose ef cace no a 17 , 5 msv . in base alla valutazione della qualit delle immagini eseguita mediante studio su fantoccio possiamo affermare che le scansioni eseguite con ltro di ricostruzione 11 e 13 , corrispondenti ad un ltro smooth ed intermedio standard - smooth , senza correzione per lindurimento del fascio radiante , con deviazione standard accettata di 12 , 5 , rappresentano un buon compromesso fra dose di esposizione e qualit dimmagine per i differenti quesiti clinici . 
appare , invece , non conveniente lapplicazione di un ulteriore ltro antirumore di tipo smooth per la scansione diretta a bassa dose , potendosi ottenere maggiori informazioni nella scansione eseguita con gli stessi parametri di dose ma con applicazione di un ltro intermedio . lottimizzazione dellesame di uro - tc nella nostra pratica clinica dovr innanzitutto concentrarsi sulla scansione diretta : una dose ef cace pari a 4 , 8 msv per una scansione che fornisce informazioni secondarie rispetto a quella contrastogra ca , non appare giusti cata . 
laccorgimento immediato da adottare potr essere laccoppiamento dei detettori in fase di acquisizione , eventualmente utilizzabile anche nella scansione nefro - escretoria , con una collimazione di 321 mm invece dellattuale 640 , 5 mlindice di ricostruzione non dovrebbe mai essere inferiore alla risoluzione spaziale sul piano xy , perch si ottengono voxel pi corti sullasse z e , dal momento che il rumore aumenta potenzialmente con il volume del voxel effettivo , per mantenere il desiderato rapporto segnale - rumore lapparecchiatura costretta ad erogare una maggiore corrente al tubo , con un aumento di dose al paziente anche di 16 volte [ 25 ]  . in un secondo tempo sar necessario valutare la qualit delle immagini ottenibili impostando una minor tensione al tubo radiogeno , analogamente a quanto proposto da coppenrath et al . 
 [ 19 ] , essendo la scansione diretta necessaria principalmente per studiare elementi ad elevato radiol med ( 2011 ) 116 : 417431 serving mainly to study high - contrast structures such as stones . 
optimisation can then be re ned through more in - depth studies of image quality obtained by modulating the remaining parameters , even with the use of different phantoms having speci c characteristics for ctu . contrasto , quali i calcoli . 
kahnouji2 1advanced diagnostic and interventional radiology research center ( adir ) , imaging medical center , imam hospital , tehran university of medical sciences , tehran 14155 - 7146 , iran 2department of neurology , imam hospital , tehran university of medical sciences , p.o. 
ghasemi esfe , tel : + 98 - 216 - 1192670 , fax : + 98 - 216 - 6910201 , e - mail : areza.ghasemi@gmail.com received : 30 may 2010 / accepted : 9 july 2010 / published online : 4 february 2011 springer - verlag 2011 abstract purpose . 
 nonetheless , in a portion of patients complaining of the typical signs and symptoms of cts , the edt is negative , and yet no paraclinical tool has been acknowledged for con rming the diagnosis . 
 ci nonostante , pur in presenza di sintomi tipici di stc non sempre i ted risultano positivi ed ancora non sono state de nite ed accettate indagini alternative che consentano di confermare la diagnosi . 
larea del nervo mediano calcolata in sezione trasversale a livello del polso ed il rapporto tra questa e larea stimata a livello dellavambraccio sono risultati signi cativamente superiori nel gruppo dei pazienti rispetto ai controlli sani . 
i coef cienti di ipoecogenicit [ odds ratio ( or ) 4 , 317 ; intervallo di con denza ( ic ) del 95% ] e di ipervascolarizzazione [ or 5 , 0004 ; 95% ic 1 , 02 - 21 , 15 ] del nervo mediano sono risultati signi cativamente pi elevati nel gruppo dei pazienti rispetto ai controlli . 
ultrasound imaging is a useful technique in diagnosing cts patients when edt results are not con rmatory and the patient is suspected of having neuropathy . keywords carpal tunnel syndrome electrodiagnostic tests ultrasonography electromyography nel predire la stc mediante sola indagine ecogra ca . 
limaging ecogra co utile nella diagnosi di stc in pazienti con sospetta neuropatia e ted non conclusivi . parole chiave sindrome del tunnel carpale test elettrodiagnostici ecogra a elettromiogra a introduction material and methods carpal tunnel syndrome ( cts ) is the most common form of entrapment neuropathy . 
it is estimated that the prevalence of cts in the adult general population is about 5.8% in women and 0.6% in men , but in a considerable portion of patients the condition remains undetected [ 5 ]  . 
 traditionally , cts is suspected on the basis of its characteristic signs and symptoms , and diagnosis is established by an electrodiagnostic test ( edt ) [ 6 ]  . 
although edt has high speci city in diagnosing cts [ 7 ] , its accuracy is not de nite , and false - negative results have been reported to be about 1020% [ 1 , 811 ]  . 
since that time , ongoing advances in us technology have made it a useful tool with which to obtain better spatial resolution and depict peripheral nerves with higher imaging quality [ 6 ]  . 
nonetheless , as edt does not have de nite accuracy , in a portion of patients complaining of the typical signs and symptoms of cts , edt results are negative , and yet no paraclinical tool has been acknowledged for con rming cts diagnosis in this subgroup of patients . 
considering that us has recently emerged as a practical and noninvasive method with reasonable accuracy in cts diagnosis [ 6 , 1319 ] , it would be interesting to evaluate its value when edt is not helpful , i.e. 
 thirty - four patients with clinical evidence of cts who had normal edt were enrolled in a cross - sectional study that was conducted from january 2008 to july 2009 in the advanced diagnostic and interventional radiology research center , imaging medical center , af liated with tehran university of medical sciences , tehran , iran . 
clinical evidence of cts , evaluated by an experienced neurologist , was de ned as pain , paraesthesia or prickling sensation in at least two of the digits iiii along , with any of the following sign or symptoms : sensory loss in the territory of median nerve , positive tinel or phalen sign , atrophy of the thenar muscles , or weakness of grip . 
patients with a history of surgical treatment for cts , wrist trauma or fracture or other conditions associated with neuropathy ( such as diabetes mellitus , hypothyroidism , chronic renal failure , pregnancy ) or with clinical ndings of any other neuropathy ( such as cervical radiculopathy and polyneuropathy ) were not included . 
electromyography ( emg ) was performed with a 10 - channel medelec synergy t - ep systepatients without evidence of cts on emg according to padua et al.s criteria [ 21 ] were included . 
 healthy individuals ( n = 41 ) were selected from volunteer hospital staff without symptoms and signs of peripheral neuropathy ( such as history of upper - limb pain , paraesthesia , weakness or any abnormality found in a brief neurological examination ) or evidence of any underlying disease associated with peripheral neuropathy . 
emg was performed in all of these volunteers , and those with normal emg ndings were enrolled as the control group . the study was approved by the local ethics review committee at the university . 
1a , b sezione trasversale ecogra ca del tunnel carpale a livello dellosso pisiforme ; caratteristico aspetto punteggiato del nervo mediano in un soggetto sano ( a ) ; marcata ipoecogenicit del nervo in un paziente affetto da sindrome del tunnel carpale ( stc ) ( b )  . in detail to patients and controls , written informed consent was obtained from all participants . 
 ultrasonography an experienced musculoskeletal radiologist blinded to the patient and control groups performed high - resolution us using a 9 - 13 mhz linear - array probe ( sonoline antares , siemens )  . 
peripheral nerves are seen as multiple speckled hypoechoic areas ( groups of fascicles ) surrounded by echogenic perineurium and / or epineuriu nerve oedema increases the hypoechoic signal of the nerve . 
using the ellipsoid area formula ( d1 d2 3.14 / 4 ) , two perpendicular diameters ( maximum anteroposterior and mediolateral diameters ) of the nerve at the level of the pisiform bone were calculated and , presuming the oval shape of the nerve , the area was calculated . 
we performed a double - level measurement of the median nerve at the level of forearm as well as the pisiform bone , as previously proposed by hobson - webb et al . 
the transducer was directly placed on the skin of most patients , but in thin patients with a very super cial nerve , if there was poor image quality to measure the nerve csa , we used a gel pad on the wrists . 
because of the deeper position of the nerve , there was no need to apply gel pads to the forear colour doppler us ( cdus ) was performed with settings suitable for detecting lowow vessels and imaged in power doppler mode . 
pulse repetition frequency was placed at 488 hz , doppler gain was then adjusted to the maximum level , creating no clutter or 492 radiol med ( 2011 ) 116 : 489496 fig . 
2a - c longitudinal view of three median nerves : nerve of a healthy individual without increased intraneural vascularity ( a ) ; intraneural hypervascularity in a patient complaining of clinical signs and symptoms of carpal tunnel syndrome ( cts ) ( b ) ; perineural increased vascularity in a healthy individual ( c )  . 
2a - c sezione longitudinale del nervo mediano in tre differenti casi : nervo di un soggetto sano in assenza di incremento della vascolarizzazione intraneurale ( a ) ; ipervascolarizzazione intraneurale in un paziente con tipici segni e sintomi di sindrome del tunnel carpale ( stc ) ( b ) ; incremento della vascolarizzazione perineurale in un soggetto sano ( c )  . 
if there was perineural vascularity or any prominent vessel near the nerve , we considered it as a normal variant , and it was not considered as intraneural hypervascularity of the median nerve . 
all participants were examined by us within 1 week of emg , and all measurements were performed twice and the average taken as the value . the level of association between continuous variables was measured using pearsons correlation coef cients . 
 the probability of having clinical evidence of cts in an individual with one or a combination of us signs of cts was calculated using the following formula : exp ( logit ) / [ 1 + exp ( logit ) ] , where logit , derived from the logistic regression modelling , is equal to the natural log of the odds of having clinical evidence of cts . 
 comparison of variables between case and control groups was made using chi - square analysis for categorical variables , students sample t test for normally distributed continuous variables , and the mannwhitney u test for continuous variables that deviated from normal distribution . 
the probability of having clinical evidence of cts in a person with one us signs of cts was approximately 35% , approximately 70% in a person with two , and approximately 90% in a person with all three signs . od or the ellipsoid formula . 
csa of the median nerve in the wrist and the wfr were measured either by the tracing method or ellipsoid formula and were signi cantly higher in patients compared with controls . 
in patients but not in controls , d1 / d2 of the median nerve in both forearm and wrist were signi cantly lower in those with hypoechogenicity pattern in the median nerve . 
 with respect to laplaces law , it is believed that the principal sensory bres injured in compressive neuropathies are small and cannot be reliably evaluated with edt [ 27 ]  . 
in fact , edt is more a diagnostic tool to evaluate large myelinated nerve bres rather than small nonmyelinated ones [ 28 , 29 ]  . clinicians usually encounter dilemma when facing patients with the clinical characteristics of cts but with nor494 radiol med ( 2011 ) 116 : 489496 mal edt ndings . 
us is the usually the most commonly recommended alternative to edt for detecting clinically suspicious patients , as it has lower cost and more comfort compared with other imaging techniques , such as computed tomography and magnetic resonance imaging [ 17 , 30 ]  . 
 there are several studies available reporting different us criteria for diagnosing cts in patients with clinical and electrophysiological ndings [ 3 , 6 , 13 , 14 , 16 , 3134 ]  . 
the csa of the median nerve at the level of the pisiform bone is the most commonly discussed criterion for diagnosing cts in suspicious patients [ 6 , 10 , 17 , 18 , 31 , 35 ]  . 
whereas some authors argue that csa of the median nerve has higher sensitivity and speci city in comparison to edt , others do not [ 17 , 35 ]  . 
 in this study , we calculated the csa of the median nerve using either the ellipsoid formula or the tracing method at two levels : wrist and forearwe found that the mean csa of the median nerve at wrist level , calculated with both techniques , was signi cantly higher in patients compared with controls . 
in a study by klauser et al . , the mean csa of the median nerve in 93 wrists of healthy volunteers ( 9.0 mm2 ) was signi cantly smaller than that of 100 cts wrists ( 16.8 mm2 ) [ 22 ]  . 
 normal peripheral nerve is visualised on us as a bundle containing multiple stippled hypoechoic areas surrounded by hyperechoic perineuriuas the nerve becomes oedematous , the hypoechoic signals become intensi ed [ 32 ]  . 
our results may highlight the role of cdus as an emerging tool for cts diagnosis . although , as described above , several studies have evaluated the role of us imaging in cts diagnosis , there is insuf cient evidence as regards the actual implementation of us in clinical practice ( for example , when cts is clinically suspected and edt results have not been clarifying , and the physician has to choose another diagnostic paraclinical tool to con rm the clinical diagnosis )  . 
to the best of our knowledge , the only study that has measured the value of us in detecting cts in patients with negative edt was performed by koyuncuoglu et al . 
they enrolled patients with positive clinical ndings but negative edt results for cts and used csa of the median nerve > 10.5 mm at wrist level as the diagnostic criterion . 
regression models , compared with crude analysis modelling , bene t from the capability of adjustment for the intercorrelation of the determinant factors and can help with readily approximating the probability of the outcome variable when there is more than one positive determinant factor . 
it is notable that the positive us signs were present in a portion of healthy individuals , and it would be important for a physician encountering the same clinical situation to have an approximation of the clinical value for each or a combination of positive us signs . 
among the three determinant factors hypervascularity , hypoechogenicity or high wrist csa of the median nerve we found that the presence of any one of these signs would predict clinical evidence of cts with a probability of approximately 35% . 
in the presence of two phenomena , this probability increases to as high as 70% ; when all the three sings are present , the probability is approximately 90% . our study has some limitations : firstly , us is an operator - dependent imaging tool . 
in this study , to evaluate us imaging in clinically suspected cts without con rmatory edt ndings , we included patients based on the presence of clinical evidence of cts . 
thirdly , to rule out tiny artefactual or noisy pixels produced by lowow settings , one can use spectral doppler recording or rely on visualising the pulsatile ow during systole and diastole within the nerve . 
however , spectral radiol med ( 2011 ) 116 : 489496 doppler is another option for detecting intraneural hypervascularisation . in summary , we showed that us imaging is a useful technique in diagnosing cts patients when edt results are not con rmatory and the patient is suspected of having neuropathy . 
knauth springer - verlag , berlin heidelberg , 2010 isbn 978 - 3 - 540 - 78570 - 0 e - isbn 978 - 3 - 540 - 78576 - 7 doi 10.1007 / 978 - 3 - 540 - 78576 - 7 published online : 7 march 2011 springer - verlag 2011 diffusion - weighted magnetic resonance imaging ( dwmri ) is a well established technique , routinely used in the study and evaluation of intracranial diseases . 
on the contrary , only a few years have passed since it has shown potential in the study of body conditions , gaining increasing momentum in the clinical setting . as stated by the editors in their preface , dw - mri has important advantages over other radiological procedures : short performance times ; no need for contrast medium ; it offers qualitative and quantitative information thus providing unique information on micro - structural and functional alterations in body tissues . the text is presented in 16 chapters , divided into four sections : principles and background ( 3 chapters ) ; non - oncologic application in the body ( 3 chapters ) ; oncological applications in the body ( 8 chapters ) ; future developments ( 2 chapters )  . the reader will note that the bulk of the text deals with dw - mri in oncology , highlighting the pros and cons of the technique in this eld , sometimes dif cult and with convoluted meaning ; yet applications outside this eld of research are also discussed . 
the last two interesting chapters in which multifunctional mri imaging assessment is discussed also look into the future as well as the potential of dw - mri as an imaging biomarker in clinical trials . the gures are impressive ; table lay - out is appropriate and rich in detail on imaging parameters or results of previous data collected from the literature ( references are updated to 2009 )  . in case one is not aware of the how and why of the technique it may be dif cult to properly process the amount of information found throughout the text . 
 la tecnica di risonanza magnetica per diffusione ( dw - mri ) ben riconosciuta ed affermata , di impiego routinario nello studio e valutazione delle cerebropatie ; al contrario , invece , solo pochi anni sono passati da quando ha dimostrato le sue potenzialit nello studio delle affezioni del corpo , guadagnando progressivo impulso nellambito clinico . come ben speci cato dai curatori del volume nella loro prefazione , la dw - mri presenta signi cativi vantaggi rispetto ad altre metodiche radiologiche : breve tempo di esecuzione ; assenza di mezzo di contrasto ; possibilit di offrire informazioni uniche , sia qualitative che quantitative , sulle alterazioni micro - strutturali e funzionali dei tessuti del corpo . il testo organizzato in 16 capitoli , divisi in quattro sezioni : principi e basi ( 3 capitoli ) ; applicazioni non oncologiche nel corpo ( 3 capitoli ) ; applicazioni oncologiche nel corpo ( 8 capitoli ) ; sviluppi futuri ( 2 capitoli )  . il lettore si render conto che il grosso del testo riguarda luso della risonanza magnetica per diffusione in campo oncologico , mettendo in evidenza i pro ed i contro della tecnica in questo campo , talvolta dif cile e con signi cati complicati ; tuttavia sono anche discusse le possibili applicazioni al di fuori di questo campo di ricerca . gli ultimi due interessanti capitoli , in cui vengono discusse le valutazioni dellimaging multifunzionale in risonanza magnetica ( rm ) , si rivolgono al futuro ed anche alla potenzialit della dw - mri utilizzata come biomarcatore per immagine nei trial clinici . le gure sono di grande effetto ; le tavole sono accurate nella loro presentazione e ricche di dettagli sui parametri per ottenere le immagini o sui risultati di dati precedenti raccolti dalla letteratura ( le voci bibliogra che sono aggiornate al 2009 )  . qualora il lettore non sia a conoscenza dei come e dei perch della tecnica , avr dif colt nella valutazione della massa di informazioni contenute nel testo . 
personalmente ho trovato dif cile la digestione dei capitoli riguardanti i principi e le basi della tecnica , lottando anche con gli acronimi usati in abbondanza . 500 radiol med ( 2011 ) 116 : 499500 apart from my personal problems , the book represents a breakthrough in this domain of radiology and will help the reader to better understand and focus on all sorts of problems one might encounter using this technique which is fully open to future development and should become a very important adjuvant in patients care . 
buzzi , via castelvetro 32 , milan , italy 2dipartimento di scienze radiologiche , oncologiche e anatomo - patologiche , sapienza universit di roma , rome , italy 4unit dipartimentale medicina fetale , asl bari , bari , italy correspondence to : f . 
this paper is the result of the work of the fetal magnetic resonance ( fmr ) study group of the italian society of medical radiology ( sirm ) in cooperation with the study group of the italian society of ultrasound in obstetrics and gynaecology ( sieog )  . 
as fmri is undergoing continuous development , and its indications and role are also likely to change over time , the fetal magnetic resonance study group is in agreement with the other scienti c bodies involved in the drafting of this document to propose subsequent modi cations to it when new clinical and scienti c evidence suggest the need . keywords fetal mri brain development fetal ultrasound fetal development riassunto lobiettivo di questo lavoro quello di dare delle risposte , sulla base delle evidenze clinico - scienti che , a quali siano ad oggi le reali indicazioni allo studio con risonanza magnetica fetale ( rmf ) e dove questo debba collocarsi nei protocolli diagnostici prenatali . 
questo lavoro il risultato della attivit del gruppo di studio di risonanza magnetica fetale della societ italiana di radiologia medica ( sirm ) svolto in collaborazione con gruppo di studio della societ italiana di ecogra a ostetrico - ginecologico ( sieog ) e rivisto ed approvato anche dal direttivo della associazione italiana di neuroradiologia ( ainr )  . 
in quanto tecnica in continua evoluzione , anche indicazioni e ruolo della rmf sono destinati verosimilmente a cambiare nel tempo : il gruppo di studio in rmf si propone , in accordo con le altre societ coinvolte , di indicare successive modi che a questo documento quando nuove evidenze clinico - scienti che lo renderanno necessario . parole chiave rm fetale sviluppo cerebrale ecogra a fetale sviluppo fetale introduction introduzione this paper is the nal document drafted by the fetal magnetic resonance ( fmr ) study group of the italian society of medical radiology ( sirm ) in cooperation with the study group of the italian society of ultrasound lavoro rappresenta il documento conclusivo questo elaborato dal gruppo di studio in risonanza magnetica fetale ( rmf ) della societ italiana di radiologia medica ( sirm ) , articolato in collaborazione col gruppo di studio 338 radiol med ( 2011 ) 116 : 337350 in obstetrics and gynaecology ( sieog )  . 
the aim of the document is to provide answers , on the basis of clinical and scienti c evidence , regarding the real indications for fmri today and where it ts in prenatal diagnostic protocols . 
as cooperation between radiologists , neuroradiologists and gynaecologists is the mandatory premise for identifying the correct collocation of fmri in modern fetal imaging , this document was jointly drafted and approved by the executive boards of sirm and sieog and the executive board of the italian association of neuroradiology ( ainr )  . as the technique is undergoing continuous development and the indications and the role of fmri are also likely to change over time , the fmr study group is in agreement with the other scienti c bodies involved in the drafting of this document to revise it when new clinical and scienti c evidence suggests the need . the document is divided into three parts : indications for fmri , study techniques with the various study protocols and safety issues . 
in the rst part , as a premise to the indications for the study , the viewpoint of the three associations involved is emphasised , that is , that fmri is a targeted examination possibly performed following a level ii ultrasound ( us ) assessment . 
instead , it should be considered a study performed with the precise aim of clarifying a diagnostic doubt or query on the basis of the consolidated indications in the literature . 
for the most part , these regard the study of the central nervous system ( cns ) , although with increasing knowledge , other organs and systems can currently be effectively studied with fmri , at all times based on speci c indications . in the section dealing with the study techniques and the various study protocols , the active role of the radiologist is emphasised . 
this role begins with the clinical history of the patient ; includes correctly positioning the patient ; performing the study itself , which must be adapted to each individual and each particular diagnostic query ; and is completed with the reporting phase . 
this latter phase requires not only a qualitative evaluation but also accurate quantitative morphometric measurements , with particular regard to studying the fetal head , which may be compared with morphometric data from the us assessment . the third section presents the most recent evidence regarding the issue of safety . 
to date , however , there are no data available that suggest potential deleterious effects to the fetus or the embryo caused by radiofrequency magnetic elds at the intensity used for clinical purposes . 
lobiettivo del documento quello di dare delle risposte , sulla base delle evidenze clinico - scienti che , a quali siano ad oggi le reali indicazioni allo studio rmf e dove questo debba collocarsi nei protocolli diagnostici prenatali . 
poich la collaborazione fra radiologi , neuroradiologi e ginecologi la premessa necessaria alla identi cazione di una corretta collocazione della rmf nel moderno imaging fetale questo lavoro stato condiviso e approvato oltre che dal direttivo della sirm e della sieog anche dal direttivo della associazione italiana di neuroradiologia ( ainr )  . in quanto tecnica in continua evoluzione , anche indicazioni e ruolo della rmf sono destinati verosimilmente a cambiare nel tempo : il gruppo di studio in rmf si propone , in accordo con le altre societ coinvolte , di indicare successive modi che a questo documento quando nuove evidenze clinico - scienti che lo renderanno necessario . il documento diviso in tre parti : le indicazioni allo studio rmf , le modalit di esecuzione con i diversi protocolli di studio e un capitolo nale sul tema della sicurezza . 
 nella prima parte , come premessa alle indicazioni allo studio , si ribadito il punto di vista delle tre associazioni coinvolte che considera la rmf un esame mirato a seguito di una valutazione ecogra ca possibilmente di 2 livello . 
 non attualmente pensabile , se non in casi selezionati , considerare lo studio del feto come un esame total - body o tanto meno di screening , quanto piuttosto uno studio svolto con il preciso scopo di approfondire un dubbio o un quesito diagnostico sulla base delle indicazioni consolidate dalla letteratura . 
queste sono di gran lunga prevalenti nello studio del sistema nervoso centrale , tuttavia con laumentare delle conoscenze anche altri organi e apparati possono oggi essere utilmente valutati con rmf sempre sulla base di indicazioni speci che . 
 nella parte relativa alla modalit di esecuzione dellesame e ai relativi protocolli di studio , si voluto sottolineare il ruolo attivo del medico radiologo dalla fase di anamnesi a quella del posizionamento della paziente , alla esecuzione stessa dello studio che , a partire dalle sequenze di base , deve essere adattato ad ogni singola paziente e ad ogni particolare quesito , per arrivare alla fase di refertazione che necessita non solo di una valutazione qualitativa , ma anche di una accurata valutazione morfometrica quantitativa , in particolare per il distretto cranio - encefalico , che possa essere di confronto ai dati morfometrici dello studio ecogra co . in ne nellultima parte si riporta la documentazione pi recente in tema di sicurezza . 
non esistono tuttavia ad oggi dati che suggeriscano potenziali effetti dannosi di campi magnetici e radiofrequenze alle intensit utilizzate a scopo clinico sia sul feto che sullemradiol med ( 2011 ) 116 : 337350 basis of this consideration , the american college of radiology ( acr ) recently eliminated all distinctions between the rst and subsequent trimesters . 
sulla base di questa considerazione lamerican college of radiology ( acr ) ha recentemente eliminato ogni differenza fra il primo trimestre ed i successivi , vengono tuttavia mantenute delle misure di prudenza e cautela riassumibili nella valutazione attenta dei costi / bene ci dellesame sul feto e della sua necessit ed inderogabilit . indications for the fmri study when to perform fmri performing the examination is recommended from 19 weeks of gestation ( wg ) onwards with the best technology currently available , obtaining suf cient spatial and contrast resolution to provide diagnostic or at any rate additional information with respect to state - of - the - art us is not considered possible before 19 wg . 
for example , at 19 wg , the hemispheres of the brain have an anteriorposterior diameter of around 50 mtherefore , with a eld of view ( fov ) that on average is between 280 and 340 mm , the effect of the poor spatial resolution becomes extremely critical , and some structures , such as the corpus callosum , may be dif cult to evaluate . 
a titolo esempli cativo , a 19 settimane gli emisferi cerebrali hanno un diametro ant - post di circa 50 mm ; pertanto , con un campo di vista che si colloca mediamente fra i 280 ed i 340 mm leffetto della scarsa risoluzione spaziale diventa assai critico ed alcune strutture , come ad esempio il corpo calloso , rischiano di essere dif cilmente valutabili . 
inoltre va considerato che le tabelle di normalit oggi disponibili in letteratura partono solo dalla 20a sg [ 1 , 2 ] e lesperienza clinica al di sotto di questa et ad oggi molto ridotta . 
non indicato eseguire una rmf per veri care dubbi insorti sulla sola ecogra a di screening effettuata a 1921 settimane di gestazione ( linee guida sieog ) [ 3 ]  . 
la rmf dovrebbe quindi essere considerata una tecnica di iii livello il cui quesito clinico deve essere giusti cato da un approfondimento ecogra co di ii livello eseguito quindi da operatori esperti ( possibilmente in centri di riferimento ) [ 49 ]  . cosa valutare in un esame rmf the fmri study must be targeted , and in general should not be a total - body assessment , except in a minority of speci c cases and only when formulated and agreed upon by the diagnostic team . on the basis of its collocation in the diagnostic pathway , fmri should be targeted at a certain region , which should also be identi ed in the radiological report . 
based on current knowledge , studies on anatomical organs - systemsareas for which there is suf cient agreement in the literature regarding the diagnostic utility of fmri appear to be justied . 
in this setting , two regions can be identi ed : the head and neck , obviously including the brain [ 1013 ] ; and the lo studio rmf deve essere mirato ed in generale non pu assumere carattere di valutazione total - body , tranne che in una minoranza di casi speci ci e preventivamente impostati e concordati con lquipe diagnostica . 
in base alle attuali conoscenze appaiono giusti cati studi su organi - apparati - aree anatomiche per le quali esiste suf ciente accordo in letteratura riguardo lutilit diagnostica della rmf . 
in tale ottica possiamo oggi identi care 2 distretti : quello dellarea testa - collo compreso ovviamente lencefalo [ 1013 ] , e quello toraco340 radiol med ( 2011 ) 116 : 337350 chest and abdomen [ 1417 ]  . 
given the limited evidence in the literature and the dif culty in performing the examination , it is currently not possible to include musculoskeletal structures and in particular the developing limbs and osteocartilaginous components of the vertebral column among the anatomical areas that can be studied with fmri . as fmri examination is by de nition targeted at a certain region , the general rule applying to all radiological examinations clearly holds : if a clear pathological nding belonging to another anatomical region falls within the fov as an incidental nding of the targeted study , it cannot be overlooked . 
this is , of course , provided that the moreor - less evident and unequivocal nature of the incidental nding can be reasonably evaluated on the basis of the quality of the images that were not speci cally targeted and the region of the nding . 
this consideration is also valid for the placenta and the amniotic sac when clear abnormalities not noted on the us scans are identi ed . where to perform a fmri study the fmri study should be performed in centres speci cally equipped for that purpose . the discussion so far suggests that it is dif cult to imagine placing the fmri study on the same level as any other mri examination performed as an outpatient procedure . 
on the one hand , there needs to be direct contact and ongoing cooperation with the referring clinicians / obstetricians , particularly with the team of experts dedicated to studying fetal abnormalities . 
per le scarse evidenze in letteratura e per la dif colt di esecuzione , non sembra oggi possibile includere nei distretti anatomici studiabili anche le strutture muscolo - scheletriche in particolare gli arti e la componente osteo - cartilaginea del rachide in formazione . posto che lesame rmf quindi per de nizione mirato ad un distretto , vale ovviamente la regola generale attuata su qualsiasi esame radiologico : se un chiaro reperto patologico , appartenente ad un altro distretto , ricade nel campo di vista , come evento collaterale dello studio mirato , esso non pu essere trascurato . 
fermo restando che il carattere pi o meno eclatante ed inequivocabile del reperto collaterale possa essere ragionevolmente valutato in base alla qualit delle immagini ( non speci catamente mirate ) ed al distretto sede del reperto . 
collo le patologie di pi frequente riscontro in epoca prenatale sono il linfangioma cistico ed il teratoma [ 40 , 41 ]  . la rmf pu : valutare leventuale estensione allo stretto toracico superiore ; identi care , quando presente , la compressione e / o dislocazione delle vie aeree , ben identi cabili per il loro contenuto uido che le rende iperintense nelle immagini pesate in t2 ; studiare i rapporti della massa con il fascio vascolonervoso del collo . tali informazioni risultano , infatti , dirimenti per decidere la procedura terapeutica pi idonea ( ex utero intrapartum treatment , exit ; resezione della massa )  . 
torace la rmf pu aiutare nella identi cazione di : masse intratoraciche : malattia adenomatoide cistica congenita ( ccam ) , sequestro broncopolmonare , cisti broncogene , sindromi da ostruzione delle vie respiratorie superiori con imaging positivo per segni indiretti ( chaos )  . 
lostruzione in assenza di questi reperti pu non essere direttamente riscontrabile [ 4244 ] ; ernia diaframmatica ( cdh ) [ 45 ] ; 342 radiol med ( 2011 ) 116 : 337350 whatever the intrathoracic disease , fmri provides information not only regarding location , size and morphology of the mass but also regarding the secondary effects it produces , such as developmental abnormalities of the residual and contralateral lung , mediastinal shift , nonimmune hydrops fetalis due to compression of the inferior vena cava and the heart [ 47 , 48 ] and polyhydramnios due to compression of the oesophagus and reduced swallowing of amniotic uid , as well as any associated extrapulmonary conditions . with regard to cdh , fmri should provide the following information : location ( right , left ) ; herniated organs ( bowel ; particularly de ne liver - up and liver - down ) ; lung volume measurements of the residual and contralateral lung and the indices of fetal lung maturity ; signal intensity analysis as a possible expression of lung maturity ( this still requires further validation ) ; possible mediastinal shift ; polyhydramnios and hydrops fetalis ; associated conditions . fmri may be indicated when , after a us study and counselling , the parent ( s ) decides to consider the option of an in - utero procedure . 
abdomen fmri can : identify the position of the visceral organs within the abdomen to verify the cardiacvisceral situs ( situs solitus or situs inversus )  . identify defects of the abdominal wall with herniation of the abdominal organs , lined or otherwise by the peritoneal folds . 
in these cases fmri is able to identify herniated organs , differentiate omphalocele from gastroschisis , measure the abdominal hernia and measure the ratio between the herniated mass and the abdomen ( to date , there is no evidence of greater accuracy than us , and the indication for fmri may be for surgical planning and de ning the manner of birth rather than for diagnostic purposes per se ) [ 4951 ]  . visualise intra - abdominal masses . 
 per quanto concerne la cdh , la rmf deve fornire le seguenti informazioni : localizzazione ( destra , sinistra ) ; organi erniati ( intestino e particolarmente de nire liverup e liver down ) ; volumetria polmonare del polmone residuo e del controlaterale e indici di maturazione polmonare ; analisi dellintensit di segnale possibile espressione della maturazione polmonare ( tale dato necessita ancora di ulteriore validazione ) ; eventuale shift mediastinico ; polidramnios e idrope ; patologie associate . si ritiene che vi sia indicazione allesecuzione della rmf , qualora la coppia , dopo valutazione ecogra ca e counselling , decida di prendere in considerazione la opzione di intervento in utero . 
for example , in differential diagnosis queries for treatment planning purposes , signal hyperintensity in t1 may orient the diagnosis towards a meconium cyst or an enterogenic cyst [ 5255 ]  . evaluate size and signal intensity of parenchymal organs , such as the liver and spleen , which in the event of metabolic or haematologic disorders may be abnormal ( iron overload , haematological diseases with an increase in haematopoiesis )  . when studying the gastrointestinal tract , indications for fmri do not include : identifying the oesophageal atresia . 
the presence of a stomach distended by uid does not rule out the presence of oesophageal atresia given the possibility of tracheooesophageal stulas distal to the obstruction . atresia of the duodenal tract . 
urogenital system the information provided by fmri is important for studying urogenital malformations associated with oligohydramnios or anhydramnios conditions that make the us study technically dif cult [ 5664 ]  . 
 fmri offers a good depiction of : autosomal recessive polycystic kidneys ; multicystic kidneys , renal agenesis , pelvicalyceal dilatations and renal masses ; hydroureteronephrosis ( evaluation of the degree and segments involved ; study of the renal parenchyma possibly with functional index ) ; posterior urethral valves ( puv ) ( evaluation of the degree of hydroureteronephrosis and the renal parenchyma ; renal dysplasia is often associated with puvs ) ; neurogenic bladder with associated conditions ( myelomeningocele ) ; enlarged bladder ( prune - belly syndrome , with study of the abdominal wall , microcolon ) ; renal and adrenal masses ; pathological conditions of the adnexa ; renal pelvic masses . indications for studying the placenta fmri provides a good evaluation of placental insertion ; la visualizzazione delle masse endoaddominali : in tali condizioni la rmf aiuta a determinarne la corretta origine , estensione e volumetria , la tipologia ( cistica o solida ) , lo spessore delle pareti , la presenza di setti o vegetazioni , oltre a caratterizzarne il contenuto distinguendo grazie alla sua multiparametricit il uido sieroso , la componente sebacea , emorragica o proteinacea ( diagnosi differenziale cisti enterogene , linfangioma )  . 
anche se lanalisi della parete , il ne dettaglio dei setti migliore con lecogra a per la sua migliore risoluzione spaziale , importante pu essere lanalisi del segnale sia t2 che t1 . 
per esempio uniperintensit di segnale in t1 pu indirizzare verso lipotesi di cisti da meconio o cisti enterogene in quesiti di diagnosi differenziale ai ni del planning terapeutico [ 5255 ] ; la valutazione delle dimensioni e dellintensit di segnale degli organi parenchimali come il fegato e la milza che nel caso di patologie metaboliche o ematologiche possono risultare alterate ( emocromatosi , malattie ematologiche con incremento dellematopoiesi )  . non costituiscono indicazioni alla rmf : lindividuazione delle atresie esofagee . 
la presenza di uno stomaco disteso da uido non pu escludere la presenza di atresia esofagea per la possibilit di stole tracheo - esofagee a valle dellostruzione ; le atresie del tratto duodenale . 
apparato genitourinario i dati forniti dalla rmf sono importanti per lo studio delle malformazioni del tratto urinario associate ad oligoo anidramnios , condizioni queste che rendono tecnicamente dif cile lo studio ecogra co [ 5664 ]  . sono ben visualizzabili mediante rmf : reni policistici da patologia autosomica recessiva ; reni multicistici , agenesie renali , dilatazioni pelvicaliceali e masse renali ; valutazione delle idroureteronefrosi ( entit , segmenti interessati , studio del parenchima renale con possibile indice funzionale ) ; valvole uretrali posteriori ( vup ; valutazione del grado di idroureteronefrosi , del parenchima renale : spesso nelle vup i reni risultano displasici ) ; vescica neurologica con patologie associate ( mielomeningocele ) ; megavescica ( sindrome di prune belly con studio della parete addominale , microcolon ) ; valutazione masse renali e surrenaliche ; patologia di pertinenza annessiale ; patologia espansiva pelvica . 344 radiol med ( 2011 ) 116 : 337350 extension ; relations with the myometrium ; relations with the internal ori ce of the uterus ; structure , which appears homogeneous between the 20th and 30th wg and becomes relatively inhomogeneous in the third trimester due to the presence of brous bands ; placental infarcts ; and pseudocystic spaces . 
in this sense , it should be noted that as with transvaginal or transanal us , fmri is unable to provide conclusive data , only high suspicion [ 6568 ]  . examination technique and study protocols indicazioni allo studio della placenta la rmf ben valuta linserzione , lestensione , il rapporto con il miometrio , il rapporto con lori zio uterino interno ( oui ) , la struttura , che risulta omogenea tra la 20a e la 30a settimana , diventando relativamente disomogenea nellultimo trimestre per la presenza di strie brotiche , aree infartuali e di lacune pseudocistiche . 
a questo proposito , si sottolinea che anche la rmf , cosi come lecogra a transvaginale ( tv ) o transaddominale ( ta ) , non permette di raggiungere dati conclusivi al riguardo ma solo di elevato sospetto [ 6568 ]  . magnet modalit di esecuzione , protocolli di studio the recommended magnetic eld for obtaining a suf cient signal - to - noise ratio ( snr ) is 1.5 t achieved with traditional superconducting magnets . 
a suf cient snr in terms of vertical geometry can also be obtained with a 1 - t magnet , whereas the use of lower - intensity magnetic elds is not recommended . 
the use of magnetic elds with intensity higher than 1.5 t is currently not considered a routine approach , as this still needs to be validated by speci c research protocols . coils various types of coils can be used in relation to gestational age , size of the amniotic sac and the uterus . 
the highest performing coils are undoubtedly multichannel phasedarray or cardiac surface coils , which enable greater signal in the longitudinal direction , although still limited to around 5060 calternatively , spine coils can be used to study the fetal body , which allow a greater fov for later gestational ages . 
 the following is required before performing an fmri examination : signed informed consent from the expectant mother after consultation with the physician aimed at verifying the absence of the usual contraindications ( pacemaker , metal clips ) , as well as explaining the role of mri in evaluating malformations and informing the patient of speci c contraindications ( safety )  . recording clinical data / history and reviewing the us images that prompted the suspicion of disease . 
the consultation is also aimed at acquiring the active cooperation from the patient in the sequences that require speci c breathing instructions , and the manner in which the fmri examination will be performed is explained ( duration , safety , diagnostic value )  . when possible , the examination is ideally performed magnete bobine il campo magnetico consigliato per ottenere un suf ciente rapporto segnale / rumore quello di 1 , 5 t ottenuto con magneti tradizionali superconduttori . 
un suf ciente rapporto segnale / rumore in ragione della geometria verticale pu essere anche ottenuto con magnete aperto a 1 t , mentre si sconsiglia luso di intensit di campo inferiori . 
 luso di intensit di campo maggiori di 1 , 5 t non oggi considerabile come approccio di routine poich deve essere ancora validato in speci ci protocolli di ricerca . possono essere utilizzate diverse tipologie di bobine anche in relazione allepoca gestazionale , alle dimensioni del sacco gestazionale e dellutero : le pi performanti sono certamente le bobine di super cie multicanale di tipo phasedarray o cardio che permettono di avere maggior segnale per unestensione longitudinale tuttavia limitata intorno ai 5060 cm ; si possono inoltre utilizzare bobine di tipo spine per lo studio del corpo che permettono un maggiore campo di vista per le epoche gestazionali pi tardive . prima di eseguire lesame rmf necessaria : la raccolta del consenso informato dalla gestante da parte del medico dopo un colloquio esplicativo volto allaccertamento dellassenza delle usuali controindicazioni alla rm ( pacemaker cardiaco , clips metalliche ) , del ruolo della rm nella valutazione della patologie malformative , eventuali controindicazioni speci che ( safety ) ; la raccolta dei dati clinico - anamnestici con presa visione della documentazione ecogra ca da cui stato generato il sospetto patologico ; durante tale colloquio viene inoltre stabilito un primo approccio con la paziente volto a conquistarne la collaborazione attiva nelle sequenze con necessit di respirazione e vengono spiegate le modalit di esecuzione della rmf ( durata , safety , valore diagnostico )  . 
alternatively , if a us study is possible immediately prior to the fmri examination to determine the fetal sleepwake phase , it may be bene cial to wait for the sleep phase , as the fetal sleepwake cycles are 30 min in length . the patient is placed in a comfortable position on the table , usually in the supine position , or in cases where this position is not tolerated ( vena cava compression , polyhydramnios , multiple pregnancies ) , then in the left lateral position is preferred . 
in general , no sedatives are used for mother or fetus , and no contrast agent is administered ( see safety issues below )  . the study protocol involves the acquisition of various sequences , some of which are indispensable , whereas others are optionally added according to the clinical query . 
the main fmri sequences are ultrafast t2 - weighted sequences , which enable excellent evaluation of the fetal anatomy thanks to high - contrast resolution and are therefore a good compromise between contrast and spatial resolution . 
the examination technique includes : localiser sequence : fast sequence ( generally a t2 - weighted single - shot fast turbo spin echo ) in the maternal coronal plane to identify fetal position with respect to the mother ( presentation ) and determine the relative position of the fetal head , spine and stomach , and to localise the placenta ( anterior / posterior )  . the standard sequence for an fmri examination is a t2 - weighted fast or turbo spin - echo sequence that in a single tr ( single shot ) acquires a single slice . 
commercially , this sequence is known as half - fourier acquisition single - shot turbo spin echo ( haste ) or single - shot fast spin echo ( ssfse ) or single - shot turbo spin echo ( sstse )  . 
the slice needs to be suf ciently thin ( 34 mm ) , with axial , sagittal and coronal orientation orthogonal to the organ / area of interest to provide detailed evaluation of the fetal anatomy . the optimal compromise between spatial resolution , contrast resolution and snr of these sequences provides excellent visualisation of the fetal anatomy during all stages of pregnancy , and in particular , displays the static uids and structures composed prevalently of uid as hyperintense structures . 
this therefore enables the study of the fetal brain , uid - containing cavities ( nasal and oral cavities , pharynx , trachea , stomach and proximal intestine , urinary tract , gall bladder ) , lungs , placenta and amniotic uid . 
 quando possibile sarebbe preferibile eseguire lesame al mattino dopo un digiuno di almeno 4 ore , poich stato dimostrato che lipoglicemia riduce i movimenti fetali ; alternativamente se possibile eseguire un esame ecograco prima dellesecuzione della rmf , volto a veri care la fase sonno o veglia del feto , si pu aspettare la fase del sonno considerando che il regolare ciclo sonno - veglia fetale prevede unalternanza di tali fasi ogni 30 minuti . la donna viene posta in una posizione confortevole sul lettino , generalmente in decubito supino o , nei casi in cui tale posizione non venga tollerata ( compressione cavale , polidramnios , gravidanze multiple ) , in decubito laterale sinistro e viene fatta riposare alcuni istanti in tale posizione per ridurre il movimento spontaneo fetale . 
 le principali sequenze utilizzate in rmf sono sequenze t2 pesate di tipo veloce - ultraveloce che consentono unottima valutazione dellanatomia fetale grazie allelevata risoluzione di contrasto , rappresentano quindi un buon compromesso tra risoluzione di contrasto e spaziale . 
lo strato deve essere suf cientemente sottile ( 34 mm ) con orientamento multiplanare assiale , sagittale e coronale ortogonale allorgano / distretto di interesse per la valutazione di dettaglio dellanatomia fetale . lottimo compromesso tra la risoluzione spaziale , di contrasto e il rapporto segnale - rumore ( snr ) di queste sequenze oltre alla loro rapidit di esecuzione permettono infatti di visualizzare lanatomia fetale in maniera eccellente durante tutte le fasi della gravidanza ed in particolare di evidenziare i uidi statici e le strutture a prevalente composizione uida come strutture iperintense consentendo 346 radiol med ( 2011 ) 116 : 337350 additional sequences include : gradient echo ( gre ) with steady - state free precession ( ssfp ) for evaluating the cardiac region and great vessels . 
these sequences in fact present intermediate contrast between t1 and t2 , use a very short tr ( < 3 ms ) and are thus not in uenced by motion , and they are able to visualise uid in motion as high - signal - intensity structures ; ssfp cine with both radial and cartesian [ 2d fourier transformation ( ft ) ] k - space sampling . 
these sequences are able to identify the heart and great vessels and can be used as real - time sequences to evaluate certain fetal movements . thick - slab cholangiography ( 4080 mm slice thickness ) heavily weighted in t2 to highlight uidlled structures by freezing an image of all uidlled structures in the entire fetus . t1 - weighted fast spoiled gre single - shot 2d or 3d with and without fat signal saturation , acquired during breathholding . diffusion - weighted ( dw ) echo - planar imaging ( epi ) , with the application of gradients oriented in the three planes in space ( b0 , b200 and b700 s / mm2 ) , for studying the kidneys , lungs , brain and placenta . 
these sequences , which have an acquisition time of around 20 s , provide information on the microscopic motion of the free and bonded water molecules in the biological tissues and enable the study of cerebral , pulmonary and renal maturity . duration of an fmr study depends on a number of factors : number of fetuses , complexity of the malformations present , repositioning of the coils and the amount of fetal motion that may require reacquisition of some sequences in the correct anatomical plane . 
the study usually takes between 20 and 45 min , with a minimum of 15 mit is nonetheless recommended to limit the examination time to avoid maternal heat stress and speci c absorption rate ( sar ) deposition in the fetus . 
using more than one sequence for the study and always including a t1 - weighted sequence in the protocol , even if of limited diagnostic quality , is recommended . reporting the fmri report should include : maternal data ; gestational age as determined from clinical data and us ndings ; type of system , sequences and scan planes used ; clinical indication and region ( s ) targeted by the study ; possibly , measurements of the anatomical structures for each region studied . 
the following measurements are lo studio quindi dellencefalo fetale , delle cavit contenenti uidi ( cavit nasali ed orale , faringe , trachea , stomaco e intestino prossimale , sistema urinario , colecisti ) , dei polmoni , della placenta e del liquido amniotico ( la )  . 
 ulteriori sequenze possono essere : sequenze gradient echo ( gre ) con tecnica steady state free precession ( ssfp ) per la valutazione del distretto cardiaco e dei grossi vasi . 
queste sequenze , infatti , presentano un contrasto intermedio t1 e t2 , utilizzano un tr ultrabreve ( < 3 ms ) non risultando in uenzate dal movimento e permettono di evidenziare come strutture ad elevata intensit di segnale i uidi in movimento ; sequenze cine - rm di tipo ssfp con tecnica di campionamento del k - spazio sia radiale che cartesiana ( 2dft )  . 
 tali sequenze permettono di individuare il cuore e i grossi vasi : possono essere utilizzate come sequenze real time per valutare alcuni movimenti fetali ; sequenze colangiogra che thick slab ( spessore di strato 4080 mm ) altamente pesate in t2 , per mettere in evidenza strutture ripiene di liquido congelando unimmagine delle strutture uide in tutto il feto ; sequenze fast spoiled gre single shot 2d o 3d t1 pesate , con e senza saturazione del segnale del tessuto adiposo , acquisite in apnea respiratoria ; sequenze echo planar imaging ( epi ) pesate in diffusione ( dwi ) , con applicazione di gradienti orientati secondo i 3 piani dello spazio ( b0 , b200 e b700 s / mm2 ) per lo studio dei distretti renale , polmonare , encefalico e della placenta . 
tali sequenze , con tempi di acquisizione di circa 20 secondi , forniscono informazioni sul movimento microscopico delle molecole dacqua , libera e legata , nei tessuti biologici e permettono lo studio della maturazione cerebrale , polmonare e renale . 
 la durata di uno studio di rmf dipende da vari fattori : numero di feti , complessit delle malformazioni eventualmente presenti , riposizionamento della bobina ed entit dei movimenti fetali che possono richiedere la riacquisizione di alcune sequenze sul giusto piano anatomico . 
abitualmente uno studio di rmf richiede dai 20 ai 45 minuti , con un minimo di 15 minuti ; risulta necessario comunque cercare di contenere i tempi dellesame per evitare leccessivo riscaldamento della gestante ed il potenziale trasferimento di energia al feto ( sar )  . 
 consigliabile utilizzare pi di una sequenza per lo studio rmf e includere sempre nel protocollo rmf una sequenza t1 pesata anche se di scarsa qualit diagnostica . refertazione la compilazione del referto prevede : indicazione dei dati materni ; indicazione dellet gestazionale come si evince dai dati anamnestici ed ecogra ci ; tipologia di apparecchiatura utilizzata , sequenze e piani di scansione impiegati ; radiol med ( 2011 ) 116 : 337350 recommended : bone and cerebral biparietal diameter , occipitofrontal diameter , transverse cerebellar diameter , anteroposterior and longitudinal diameter of the vermiform process of the cerebellum , longitudinal diameter of the corpus callosum , atrial diameter of the cerebral ventricles . 
 in addition , an evaluation of the main cerebral ssures is recommended , which is an important parameter for information on brain development and for verifying that the development matches gestational age . 
 in the fetal total - body study , lung - volume measurements are recommended in space - occupying thoracic masses and cdh , whereas kidney measurements are advisable especially in urinary tract disease . 
 is also advised : ( a ) detailed description of the disease in question , with an analysis of the malformation or the expansile lesion being studied ( location , volume , signal analysis , relations with adjacent structures , inability to nd anatomical structures , associated signs ) ; ( b ) conclusions ; where possible these should indicate possible diagnoses in order of probability and follow - up where required . safety limitations the most recent and important documents published on safety available today are the italian national institute for occupational safety and prevention ( ispesl ) document posted on the institutes web site on 6 february 2009 and published in radiologo in april , 2008 , with regard to italy ; and the acr guidance for safe mr practices : 2007 document published in the american journal of roentgenology ( ajr 2007 , 188 : 1 - 27 ) with regard to the united states . 
 02 / 09 / 1991 , which reads : although there is no evidence to suggest the embryo is sensitive to magnetic elds and radiofrequency elds at the strength used in current mr systems for diagnostic purposes ( 1991 ) , caution is warranted in exposing women in the rst trimester of pregnancy , except in cases of real and pressing need assessed by the physician and ordered under her / his direct responsibility . 
the patient shall be informed about the possible risks of the examination beforehand . whereas the need for informed consent has been established , there remains the practical problem of informing the patient of the hypothetical risks of the examination , which to date have neither been con rmed by the literature nor precisely de ned . 
in the chapter titled patient pregnancies , the acr document states : present data have not indicazione clinica e a quale distretto / i rivolto lesame ; per ogni distretto interessato consigliabile la misurazione delle strutture anatomiche . 
si consiglia di misurare il diametro biparietale ( dbp ) osseo e cerebrale , il diametro fronto - occipitale ( dfo ) , il diametro trasverso cerebellare , il diametro antero - posteriore e longitudinale del verme cerebellare , il diametro longitudinale del corpo calloso , il diametro atriale dei ventricoli cerebrali . 
 nello studio del body fetale si raccomanda di misurare la volumetria polmonare nelle patologie toraciche occupanti spazio e nelle cdh ; la biometria renale consigliabile , in particolare in tutte le patologie del tratto urogenitale . 
si consiglia anche di inserire nel referto : ( a ) la descrizione dettagliata della patologia in questione con lanalisi della malformazione o della patologia espansiva in esame ( localizzazione , volumetria , analisi del segnale , rapporti con le strutture contigue , mancato reperimento di strutture anatomiche , segni associati ) ; ( b ) le conclusioni : ove sia possibile indicare le ipotesi diagnostiche in ordine di probabilit ed eventuali controlli . sicurezza limitazioni allesecuzione dellesame i principali e pi recenti documenti sulla sicurezza oggi disponibili sono , per quanto riguarda litalia , il documento dellispesl pubblicato sul sito il 6 / 2 / 09 e ripreso nel numero 4 / 2008 del radiologo e , per quanto riguarda gli stati uniti , la acr guidance for safe mr practices : 2007 pubblicata su ajr 2007 ; 188 : 1 - 27 . 
02.09.1991 : sebbene non esistano evidenze che dimostrino una sensibilit dellembrione ai campi magnetici e ai campi a radiofrequenza di intensit e potenze utilizzate nella attuale strumentazione rm ad uso diagnostico ( 1991 ) , prudente escludere dallesposizione le donne nel primo trimestre di gravidanza , tranne nei casi di effettiva e improrogabile necessit , valutati dal medico , sotto la sua responsabilit . 
stabilita la necessit di un consenso informato , permane il problema pratico di informare su ipotetici rischi che ad oggi non sono n confermati dalla letteratura n de niti con precisione . 
il documento acr riporta invece al capitolo patient pregnancies : 348 radiol med ( 2011 ) 116 : 337350 conclusively documented any deleterious effects of mr imaging exposure on the developing fetus . 
all distinctions between the rst and later trimesters have therefore been eliminated , although caution has been maintained that may be summarised in terms of careful assessment of the costs and bene ts of fetal examination and the substantiated need and pressing nature [ 6976 ]  . present data have not conclusively documented any deleterious effects of mr imaging exposure on the developing fetus . 
 viene quindi abolita ogni differenza fra il primo trimestre ed i successivi , vengono tuttavia mantenute delle misure di prudenza e cautela riassumibili nella valutazione attenta dei costi / bene ci dellesame sul feto e della sua necessit ed inderogabilit [ 6976 ]  . limitations to the use of contrast agents limitazioni alluso del mezzo di contrasto animal studies conducted to date have shown no teratogenic effects of gadolinium - based contrast agents . 
however , there is no evidence of its harmlessness in humans , so its use is not recommended except in cases of absolute necessity , which as a rule are implicitly correlated with maternal health . 
the acr document takes a rather permissive line : mr contrast agents should not be routinely provided to pregnant patients , although thereafter it recalls the concept of riskbene t ratio for the patient . 
when contrast agent use is sporadically found in the literature or reported anecdotally in specialist referral centres , it is generally with reference to cases that nonetheless would have nished with a terminated pregnancy . 
in conclusion , the use of contrast agents should not currently be considered an additional tool for fmri , but rather , solely a special exception in select cases of established clinical need . acknowledgements the authors thank the entire executive board of the italian society of medical radiology , with special thanks to the president , alfredo siani , and francesco sardanelli , for the ongoing support provided to the study group . 
lastly , we thank the sieog study group in fetal imaging , especially vincenzo daddario and dario paladini . gli studi ad oggi compiuti in animali non hanno dimostrato effetti teratogeni dei mdc contenenti gadolinio . 
il documento dellacr di tono pi permissivo : mr contrast agents should not ruotinely provided to pregnant patients , ma nella sostanza richiama di seguito il concetto dei costi / bene ci per la paziente . 
quanto di sporadico e occasionale pu essere rintracciato in letteratura o nellaneddotica dei centri di riferimento di norma riferito a casi che comunque sarebbero andati incontro alla interruzione di gravidanza . 
in conclusione luso dei mezzi di contrasto non pu essere considerato oggi uno strumento aggiuntivo dellimaging rm del feto , ma unicamente una particolare eccezione in casi selezionati dalla necessit clinica . ringraziamenti gli autori desiderano ringraziare tutto il direttivo della societ italiana di radiologia medica ed in particolare il presidente dott . 
nieder springer - verlag , berlin heidelberg , 2010 isbn 978 - 3 - 540 - 92809 - 6 e - isbn 978 - 3 - 540 - 92810 - 2 published online : 7 march 2011 springer - verlag 2011 this book addresses tumour biology and how its role may in uence cancer treatment and related clinical strategies . 
 robust research and clinical results are presented by a team of professionals who , for many years , have been dedicated to the ght against cancer . the topic is fascinating yet very dif cult to follow if one doesnt have sound and up - to - date knowledge of the genetic , biological , and laboratory issues which are the bread and butter of the text and related discussions . my point is that often the reader may get lost among all the acronyms , shortened names , protein names , biological markers , genetic tricks , new terms such as genomic , epigenomics , etc . 
considering the enormous mass of information poured into the text the reader when necessary ( and this happens very often ) will have to struggle with a very concise and poor subject index . 
in another a medley of one lo scopo che si sono pre ssi gli autori di questo volume di studiare la biologia tumorale e come il suo ruolo possa in uenzare le strategie cliniche e terapeutiche nella lotta contro il cancro . 
in questa ottica il gruppo di esperti che da lunghi anni ha dedicato la propria attivit a questo scopo , presenta i risultati di una ricerca di laboratorio e sperimentale continua oltre che dal punto di vista clinico . largomento affascinante , anche se molto dif cile da seguire per un profano ed in assenza di una conoscenza approfondita ed aggiornata dei vari argomenti di genetica , biologia , laboratorio che sono alla base di tutti gli argomenti del testo e delle relative discussioni . dico questo perch spesso il lettore potrebbe avere la sensazione di perdersi tra tutti gli acronimi , termini abbreviati , nomi di proteine e di marcatori biologici , trucchi della genetica , nuovi termini come genomica , epigenomica , ecc . : tenuto poi conto dellenorme massa di informazioni presenti nel testo , in caso di necessit ( e capita spesso ) si scontrer con un indice analitico conciso , povero . se si riescono a superare tutti gli scogli di cui sopra o se si a conoscenza della materia , sar possibile trovare una notevole quantit di informazioni sulla biologia dei tumori e la tumorogenesi , langiogenesi , il ruolo giocato dal sistema immunitario , la proliferazione , la siologia e la ripopolazione cellulare , la diffusione delle metastasi e la capacit delle cellule di sfuggire a tutti i possibili strumenti terapeutici , anche se questi sono sotto forma di armi molecolari . sono ben descritti e discussi lo studio per immagini , la chemioterapia , la terapia molecolare mirata e le possibili strategie radioterapiche , presentandone i pro e contro , alla luce delle ricerche pi avanzate e dei conseguenti risultati clinici . al termine di ogni capitolo presente una bibliogra a ampia ed aggiornata ; la sua impostazione non omogenea : in un capitolo si trover la citazione dei nomi di tutti gli autori ; in un altro un solo nome seguito da et al . ; in un terzo tre nomi e poi et al . ; in un altro ancora un miscuglio 498 radiol med ( 2011 ) 116 : 497498 or more names plus et al.. 
dif cult to understand as well is the fact that each chapters author / s is / are keen to show how much research he / she / they have performed on the relevant matter . 
yet , arent 41 self - citations ( as in chapter 4 ) a bit redundant ? arriving at the end of the book one realizes that much has been achieved in the eld of cancer research and therapy , yet a lot more needs to be done : with every new discovery more problems arise , these need to be addressed , before victory in the eld may be achieved . di uno o pi nomi seguiti da et al.. 
cosa dif cile da capire anche il fatto che in ciascun capitolo lautore / i sia / siano desideroso / i di far conoscere quanto lavoro e ricerca egli / loro abbia / abbiano svolto sullargomento in questione . 
rossi1 1department of clinic sciences , section of radiological sciences , 2department of pathology and laboratory medicine , section of pathology , university of parma , via gramsci 14 , 43100 parma , italy 3department of radiology , santorsola - malpighi hospital , university of bologna , via massarenti 9 , 40138 bologna , italy correspondence to : m . 
de filippo , e - mail : massimo.defilippo@unipr.it received : 22 january 2010 / accepted : 4 april 2010 / published online : 10 february 2011 springer - verlag 2010 abstract purpose . 
lutilizzo di immagini tridimensionali mpr ha permesso in tutti i casi il prelievo di materiale biologico ( 10 di tipo citologico e 4 di tipo istologico ) e in 11 su 14 casi ( 78 , 5% ) il prelievo risultato adeguato per un giudizio diagnostico . 
le immagini mpr ottenute con tcmd hanno permesso di raggiungere lesioni retroperitoneali considerate un tempo difficilmente accessibili o inaccessibili con la guida delle immagini tcmd assiali . limpiego delle immagini mpr , inoltre , non incrementa il tempo di esecuzione del prelievo . 408 radiol med ( 2011 ) 116 : 407416 parole chiave tomografia coomputerizzata biopsia retroperitoneo tumori introduction introduzione radiologically guided percutaneous fine - needle aspiration biopsy ( fnab ) and core biopsy are safe , accurate and minimally invasive procedures allowing cytohistological diagnosis of retroperitoneal lesions for which imaging has failed to provide a definitive diagnosis [ 1 , 2 ]  . 
cytohistological investigation plays an important role in the primary diagnosis of neoplasms but also in staging , selecting tumour - specific therapy and follow - up [ 3 , 4 ]  . 
anatomical and histological complexity makes the retroperitoneum the centre of different primary neoplasms ( many malignant ) arising in the epithelium , soft tissues , nervous tissues and haemolymphopoietic system ; there is also frequent tumour infiltration from adjacent structures ( vertebral column , abdominal wall , chest ) and metastasis [ 57 ]  . 
nowadays , percutaneous fnab biopsy and core biopsy provide minimally invasive options that allow unnecessary surgical resection to be avoided ( as in the case of lymphoma and unresectable masses ) and the planning of alternative strategies , such as neoadjuvant chemotherapy and radiotherapy [ 3 , 9 ]  . 
 the imaging procedures commonly used to guide retroperitoneal biopsy are ultrasound ( us ) and multidetector - row spiral computed tomography ( mdct ) [ 10 , 11 ]  . selecting the more appropriate guidance technique is based on lesion site and size ( lymphadenopathy , free masses , masses or nodules in parenchymatous organs )  . 
these include the lack of ionising radiation , portability , decreased procedure time , real - time visualisation of the needle throughout the procedure and relatively low costs [ 12 , 13 ]  . 
mdct - guided biopsy offers some advantages , especially in small , low - density lesions and lesions located deep in the retroperitoneum that are difficult to reach with us guidance alone [ 3 ]  . 
nevertheless , it is not infrequent for some lesions to be obscured by skeletal segments , abdominal organs , vessels and nervous structures so that mdct - guided biopsy may also prove difficult , if not impossible . 
the introduction of mdct has , however , allowed multiplanar reconstructions ( mpr ) to be obtained that have been shown particularly useful in guiding percutaneous pulmonary biopsies [ 1417 ] the purpose of this paper is to illustrate the utility and advantages of mdct with mpr in guiding fnab and core lagoaspirazione con ago sottile ( fnab ) e lagobiopsia , eseguite con approccio percutaneo , sono procedure scarsamente invasive e di provata sicurezza ed efficacia , spesso impiegate nella definizione cito - istologica di lesioni retroperitoneali nelle quali limaging non stato in grado di fornire una diagnosi di certezza [ 1 , 2 ]  . 
lesame cito - istologico di fondamentale importanza nella diagnosi di natura , ma anche nella fase di stadiazione della neoplasia , nellimpostazione della strategia terapeutica e nel successivo follow - up [ 3 , 4 ]  . il retroperitoneo , per la sua complessit anatomica ed istologica , sede di svariate neoplasie primitive ( molte delle quali maligne ) epiteliali , delle parti molli , neuroectodermiche e del sistema emolinfopoietico ; frequenti sono anche le infiltrazioni tumorali da strutture adiacenti ( ad esempio , colonna vertebrale , pareti addominali , torace ) e le metastasi [ 57 ]  . 
le attuali metodiche agoaspirative e agobioptiche , oltre a ridurre a livelli minimi linvasivit della manovra di prelievo tissutale , consentono di evitare la resezione chirurgica quando non necessaria ( ad esempio , linfomi e masse non resecabili ) e dare cos spazio a strategie terapeutiche alternative tra cui la chemioterapia neoadiuvante e la radioterapia [ 3 , 9 ]  . 
 le tecniche radiologiche di guida allesecuzione dellagobiopsia retroperitoneale sono lecografia ( us ) e la tomografia computerizzata ( tc ) multidettore ( tcmd ) [ 10 , 11 ]  . 
la scelta della guida pi appropriata si basa su fattori strettamente legati alla sede e alle dimensioni della lesione in esame ( ad esempio , linfonodi , masse libere , masse e noduli nel contesto di organi parenchimatosi )  . 
i vantaggi in ambito interventistico dellus , rispetto alla tcmd , sono ben noti ; uno tra tutti la possibilit dellus di guidare in tempo reale la traiettoria dellago [ 12 , 13 ]  . 
la tcmd permette di visualizzare sia lesioni di piccole dimensioni e bassa densit che lesioni situate in zone difficili e profonde nel retroperitoneo , mal visualizzabili con lus [ 3 ]  . 
tuttavia , non di rado , alcune lesioni vengono coperte da segmenti scheletrici , organi addominali , vasi e strutture nervose , e pertanto anche con la guida tcmd , la procedura agobioptica pu risultare difficile e , talvolta , non eseguibile . 
lintroduzione della tcmd ha per consentito di ottenere ricostruzioni di immagini multiplanari ( mpr ) che si sono dimostrate particolarmente vantaggiose nella guida dellagobiopsia percutanea di lesioni polmonari [ 1417 ]  . 
 lo scopo del lavoro stato quello di indagare la possibile utilit dellimpiego delle immagini mpr nelle agobiopsie percutanee tcmd - guidate di lesioni retroperitoneali difficilmente raggiungibili con la sola osservazione delle immagini assiali . 
 radiol med ( 2011 ) 116 : 407416 biopsy of retroperitoneal lesions difficult to reach using axial mdct guidance alone . materiali e metodi pazienti materials and methods patients the study included inpatients and outpatients with us or ct evidence of small retroperitoneal lesions suspicious for malignancy . 
in these lesions , us guidance was of limited use in selecting the optimal path of the biopsy needle owing to the interposition of abdominal organs and vessels between the skin and the target lesion . 
also included in the study were patients in whom axial mdct failed to provide a safe needle trajectory because of the interposition of skeletal structures , vessels and abdominal organs between the skin and the target lesion . patients with small or large retroperitoneal lesions amenable to us or axial mdct guidance , patients with blood coagulation disorders and paediatric patients were excluded . 
 methods a six - slice helical mdct scanner ( somatom emotion 6 , siemens , erlangen , germany ) was used , with the simultaneous acquisition of six slices per rotation and the following technical parameters : 90 mas , 130 kv , 2 - mm collimation , 2.5 - mm slice thickness , 1 - mm reconstruction increment . 
all patients gave written informed consent after receiving verbal and written information regarding the benefits and risks of the procedure . patients were placed on the mdct table in the supine , prone or lateral position depending on the site of the target lesion and its distance from the abdominal wall . 
on the basis of these 3d images , a 2022 gauge chiba needle or an 18gauge microhistological needle ( biomol , hospital service , italy ) was inserted , taking care to select the shortest needle path without the interposition of large vessels , nerves , abdominal organs or bony structures . 
for microhistological biopsies , tissue samples were fixed in formalin . sono stati inclusi tutti i pazienti con lesioni retroperitoneali di piccole dimensioni sospette per malignit allo studio ecografico o mediante tc . 
in tali lesioni la guida ecografica alla biopsia non consentiva unottimale pianificazione della traiettoria dellago , per il sovrapporsi , tra la cute e la lesione bersaglio , di visceri e strutture vascolari . 
sono stati inclusi inoltre tutti i pazienti in cui le immagini tc assiali non consentivano una programmazione sicura della traiettoria dellago per il sovrapporsi , tra la cute e la lesione bersaglio , di strutture scheletriche , visceri e vasi . 
con tali criteri sono stati prospetticamente studiati 14 pazienti det compresa da 26 a 77 anni ( et media 51 , 5 anni ) , dei quali 9 maschi e 5 femmine . 
 tecnica tc stata utilizzata unapparecchiatura a 6 strati tcmd ( somatom emotion 6 , siemens , erlangen , germania ) a scansione elicoidale , con acquisizione simultanea di sei strati per ogni rotazione completa . 
i parametri tecnici utilizzati sono stati i seguenti : 90 mas , 130 kv , collimazione 2 mm , spessore di strato 2 , 5 mm e intervallo di ricostruzione di 1 mlelaborazione delle immagini stata ottenuta con una workstation dedicata ( leonardo , siemens )  . 
ciascun paziente , in regime di ricovero ordinario o di day hospital , ha fornito il proprio consenso firmato previa informazione verbale e scritta sui vantaggi e le possibili complicanze correlate alla procedura . i pazienti sono stati posizionati sul lettino della tcmd in decubito supino , prono , o laterale a seconda della sede della lesione da sottoporre ad agobiopsia e della sua distanza dalla parete addominale . 
sulla base di tali immagini tridimensionali , stato introdotto , un ago chiba point centimetrato di 22 / 20 g ( per prelievo del materiale idoneo allo studio citologico ) o un ago tranciante da 18 g ( biomol , hospital service , italia ) , scegliendo il tragitto pi breve in cui non ci fosse linterposizione , tra la cute e la lesione bersaglio , di grossi vasi , nervi , strutture viscerali o scheletriche , nonch lingresso nello spazio retroperitoneale . con una scansione tcmd successiva stata ottenuta la conferma , che la punta dellago fosse stata correttamente posizionata . 
finally , all patients were followed up until the cytological or histological confirmation of the diagnosis was obtained . biopsie microistologiche , i frustoli di tessuto sono stati fissati in formalina . 
non stata effettuata alcuna restrizione dietetica o idrica aggiuntiva o diversa da quella clinicamente indicata . infine , i pazienti , sono stati seguiti fino a conferma cito / istologica della diagnosi . results risultati anatomical and radiological characteristics of the 14 patients are summarised in table 1 . 
lutilizzo di immagini tridimensionali mpr ha permesso in tutti i casi il prelievo di materiale biologico ( 10 di tipo citologico e 4 di tipo istologico ) e in 11 su 14 casi ( 78 , 5% ) il prelievo risultato adeguato per un giudizio diagnostico . 
i prelievi istologici sono risultati adeguati per la diagnosi in tutti casi , quelli citologici in 7 su 10 casi ( 70% ) ( tabella 1 )  . in 6 casi ( pazienti 3 , 4 , 7 , 1113 ) , le lesioni sottoposte ad agobiopsia erano noduli solidi nel contesto di organi parenchimatosi o strutture muscolari , linfoadenomegalie in 6 casi ( pazienti 1 , 2 , 5 , 6 , 7 , 8 , 9 )  . 
in due casi ( pazienti 10 , 14 ) la biopsia stata eseguita in un surrene lievemente aumentato di volume , in cui era stata documentata una captazione del tracciante radioattivo allesame tc - tomografia ad emissione di positroni ( pet )  . 
in un solo caso si osservata una complicanza rappresentata da una sottile falda di pneumotorace , del tutto asintomatica , a seguito di una biopsia di un linfonodo peripancreatico ( paziente 5 )  . 
 us and mdct are the most commonly used imaging techniques for guiding percutaneous needle biopsy of suspected or known retroperitoneal malignancies [ 10 , 11 ]  . us is considered the technique of choice because it allows real - time visualisation of the needle throughout the procedure , it does not expose the patient to radiobiological risk and it has relatively low costs [ 1214 ]  . 
mdct , with its ability to visualise fine anatomical detail , is preferred for lesions that are difficult to reach with the us beanevertheless , in some cases , the target lesion may prove hard or impossible to reach , even with mdct guidance , because it is obscured by bony structures , vessels and / or abdominal organs . 
in these cases , surgical biopsy or surgical resection is recommended [ 3 ]  . the anatomical obstacles between the skin and the target lesion in our study included abdominal organs in discussione le tecniche radiologiche di guida allesecuzione di agobiopsie percutanee di lesioni retroperitoneali di incerta natura solitamente utilizzate sono lus e la tcmd [ 10 , 11 ]  . 
lus la guida strumentale di prima scelta nelle biopsie percutanee , in quanto permette la guida in tempo reale della traiettoria dellago , non espone il paziente a rischio radiobiologico , ed ha relativi bassi costi [ 1214 ]  . 
tuttavia , in alcuni casi , anche con la guida tcmd , pu essere difficile o non possibile raggiungere il tessuto da sottoporre a biopsia , in quanto mascherato da strutture vascolari , scheletriche e / o viscerali ; in tali situazioni viene suggerita la biopsia escissionale ( open biopsy ) o la resezione chirurgica della lesione [ 3 ]  . radiol med ( 2011 ) 116 : 407416 radiol med ( 2011 ) 116 : 407416 radiol med ( 2011 ) 116 : 407416 fig . 
dimostrazione sul piano assiale nativo della punta dellago ( freccia ) allinterno del surrene sinistro . b , c limmagine mpr assiale obliqua ( b ) e parasagittale sinistra ( c ) rendono possibile la scelta del percorso dellago che eviti la sovrapposizione del rene sinistro e del seno costo - frenico sinistro , suggerendo una doppia inclinazione ( caudo - craniale e medio - laterale )  . 
note how the adrenal lesion is hidden by the proximal end of the left 12th rib ( short arrow ) and in close contact with the abdominal aorta and the upper pole of the left kidney . 
si noti come la lesione surrenalica sia coperta dallestremo prossimale dellultima costa di sinistra ( freccia corta ) e sia a stretto contatto con laorta addominale ed il polo superiore del rene sinistro . 
b limmagine mpr parasagittale rende possibile la scelta del percorso dellago che eviti la penetrazione dellaorta addominale e del rene sinistro , suggerendo una doppia inclinazione ( cranio - caudale e medio laterale )  . 414 radiol med ( 2011 ) 116 : 407416 fig . 
la scansione assiale nativa documenta la punta dellago ( freccia ) allinterno del linfonodo . il linfonodo neoplastico completamente coperto dal processo traverso sinistro della i vertebra lombare ( testa di freccia ) ed a stretto contatto con lilo renale destro . 
a unenhanced axial multidetector computed tomography of the upper abdomen ( patient lying prone ) shows the needle tip ( arrow ) inside the metastatic lymph node ( arrowheads ) , which is hidden by a vertebral transverse process . 
a , b contrast - enhanced axial multidetector computed tomography of the upper abdomen ( patient lying prone ) shows a 10 - mm enhancing node in the left psoas muscle ( arrowheads in a ) , which is more evident in a higher contrast window ( b )  . 
impregnazione nodulare del mdc di 10 mm ( punte di freccia in a ) , nel contesto del muscolo psoas di sinistra , meglio evidente nella finestra ad elevato contrasto ( b ) ; si noti come la lesione sia coperta dal processo traverso della ii vertebra lombare ( freccia in b )  . 
in such cases , double oblique mpr views ( craniocaudal and mediolateral ) enables selection of a needle path that avoids bony structures , vessels and organs . us - guidance of biopsy of the right adrenal gland is particularly straightforward , thanks to the presence of the hepatic acoustic window . 
on the basis of our results , guidance of mdct with mpr enables the selection of alternative routes , thereby increasing the likelihood of reaching sites that would otherwise be difficult to access . riore ai 2 cm , era coperta nelle scansioni assiali tc dallaorta addominale , dal polo renale superiore sinistro e dallarticolazione costo - vertebrale sinistra . 
in questi casi la scelta della migliore traiettoria dellago che potesse evitare strutture scheletriche , vasi o visceri stata ottenuta con una doppia obliquit ( medio - laterale e cranio - caudale ) grazie alla guida delle immagini mpr . 
la guida bioptica tcmd con immagini mpr da tempo entrata nelluso delle unit di radiodiagnostica tuttavia lutilizzo ed i vantaggi sono stati descritti solo per lesioni polmonari [ 1619 ]  . 
sulla base dei nostri risultati , analogamente a quanto gi dimostrato per le lesioni polmonari , la guida tcmd , con lausilio delle ricostruzioni mpr , pu consentire la scelta di piani di accesso alternativi aumentando le possibilit di raggiungere sedi di difficile acceso . 
 416 conclusions conclusioni radiol med ( 2011 ) 116 : 407416 mdct is the imaging examination of choice in the biopsy of retroperitoneal lesions that are difficult to see on us scans . 
in our experience , images did not the use of mpr increase the rate of complications or the procedure time . la tcmd lindagine strumentale di scelta nella guida bioptica delle lesioni retroperitoneali difficilmente documentabili in us . 
rotondo1 1dipartimento di internistica clinica e sperimentale magrassi - lanzara , sezione di radiodiagnostica e radioterapia , seconda universit degli studi di napoli , p.zza miraglia 2 , 80138 napoli , italy 2servizio di radiologia , ospedale san massimo , penne , pescara , italy correspondence to : g . 
the aim of this study was to compare magnetic resonance ( mr ) enteroclysis with mr enterography to verify whether nasoenteric intubation in patients affected by crohns disease can provide supplementary information to that afforded by mr study of the small bowel . 
distension of the small - bowel loops was obtained by administering polyethylene glycol : 15 patients were given the mixture by mouth ( mr enterography ) , whereas the remaining 25 received it via nasoenteric intubation ( mr enteroclysis )  . our study protocol included morphological sequences taken before and after intravenous injection of contrast medium and real - time functional sequences . 
complete distension of the small - bowel loops was obtained in the 25 patients who underwent mr enteroclysis , with the additional advantage of a suitable assessment of those segments involved in the pathological process . 
in un periodo di 12 mesi , 40 pazienti con morbo di crohn ( 28 femmine e 12 maschi ; et media 35 anni ) sono stati sottoposti ad esame rm . 
la distensione delle anse dellintestino tenue stata ottenuta con polietilen glicole ( peg ) : 15 pazienti hanno assunto per os la miscela ( mr - os ) , mentre a 25 pazienti stata iniettata tramite sondino naso - enterico ( mr - e )  . 
nei 25 pazienti sottoposti ad mr - e si ottenuta una completa distensione di tutte le anse dellintestino tenue con unadeguata valutazione dei tratti interessati dal processo patologico , cos non stato nei 15 sottoposti ad mr - os poich le anse del digiuno e del tenue prossimale sono risultate parzialmente collabite . 
la mr - e la tecnica pi efficace nello studio dellintestino tenue nei pazienti affetti da morbo di crohn , fornendo unadeguata valutazione morfologica , ma anche informazioni funzionali . 390 radiol med ( 2011 ) 116 : 389406 keywords crohns disease mr enteroclysis mr enterography bowel distension wall lesions stenosis fistulas parole chiave morbo di crohn enteroclisi rm enterografia rm distensione intestinale lesioni di parete stenosi e fistole introduction introduzione crohns disease is a chronic inflammatory disease of the gastrointestinal tract , which can involve almost any segment from the mouth to the anus . 
the sites most frequently involved are the terminal ileum and the proximal colon [ 1 ]  . although endoscopy with biopsy is considered the reference standard for diagnosing inflammatory bowel diseases such as crohns disease [ 2 , 3 ] , the small bowel is still defined the black box of the gastrointestinal tract due to the difficult access for endoscopic techniques [ 4 ]  . 
various imaging techniques have been proposed for the panoramic study of the small bowel , such as scintigraphy with labelled leukocytes , and computed tomography ( ct ) [ 6 ]  . 
limitations of these techniques include the low contrast resolution of the former and exposure to ionising radiation for both , which in patients with crohns disease given the need for life - long follow - up is biologically significant and limits the repetition of the techniques [ 6 , 7 ]  . magnetic resonance ( mr ) imaging overcomes these limitations . 
the elevated soft - tissue contrast , the lack of ionising radiation and the functional information it can provide make mr imaging an ideal candidate for diagnosis and follow - up of patients with crohns disease [ 8 ]  . however , the study protocol has not yet been standardised , and some controversy remains regarding the value of nasoenteric intubation [ 9 , 10 ]  . the aim of our study was to compare mr enteroclysis ( contrast material administered after the placement of a nasoenteric tube ) with mr enterography ( contrast material administered by mouth ) to evaluate which is more effective in patients with crohns disease . materials and methods in a 12 - month period ( october 2008october 2009 ) , 40 consecutive patients ( 28 women and 12 men , mean age 35 years , range 1860 years ) were referred to our department with a histological diagnosis of crohns disease ( table 1 )  . all 40 patients had undergone conventional enteroclysis ( table 2 ) and underwent mr examination to complete the diagnostic work - up . 
clinically , the patients presented with different levels of disease activity according to the harveybradshaw index ( hbi ) ( table 3 ) and on the basis of laboratory test findings [ white blood count ( wbc ) , haematocrit il morbo di crohn una malattia infiammatoria cronica del tratto gastroenterico , che pu colpire qualsiasi segmento dalla bocca allano . 
sebbene lendoscopia con biopsia sia considerata il gold standard per la diagnosi delle patologie infiammatorie intestinali ( ibd ) , come il morbo di crohn [ 2 , 3 ] , lintestino tenue tuttora definito the black box dellapparato gastroenterico proprio per il difficile accesso alle metodiche endoscopiche [ 4 ]  . 
sono state proposte diverse metodiche di imaging per lo studio panoramico dellintestino tenue , come la scintigrafia con i leucociti marcati e la tomografia computerizzata ( tc ) [ 6 ]  . 
limiti di queste metodiche sono , per la prima , la bassa risoluzione di contrasto e per entrambe , unesposizione a radiazioni ionizzanti , che nei pazienti con morbo di crohn , data la necessit di un follow - up a vita , assumono un significato biologico importante e ne limitano la ripetizione [ 6 , 7 ]  . la risonanza magnetica ( rm ) supera tali limiti . 
lelevata risoluzione di contrasto per i tessuti molli , il non utilizzo di radiazioni ionizzanti e la disponibilit di sequenze funzionali candidano la rm come esame ideale per la diagnosi ed il follow - up dei pazienti con morbo di crohn [ 8 ]  . 
tuttavia il protocollo di studio non ancora standardizzato e rimane soprattutto controverso il valore dellintubazione naso - digiunale [ 9 , 10 ]  . il nostro studio si pone lobiettivo di confrontare lenteroclisi rm con somministrazione di mezzo di contrasto ( mdc ) dopo posizionamento di sondino naso - enterico ( mre ) con lenterografia rm con somministrazione di mdc per os ( mr - os ) , per valutare quale sia pi efficace nei pazienti con il morbo di crohn . materiali e metodi in un periodo di 12 mesi ( ottobre 2008ottobre 2009 ) , 40 pazienti consecutivi ( 28 femmine e 12 maschi ; et media 35 anni ; range 1860 anni ) sono giunti alla nostra attenzione con diagnosi istologica di morbo di crohn ( tabella 1 )  . 
allesame clinico , i pazienti presentavano differente attivit di malattia , secondo lharvey - bradshaw index radiol med ( 2011 ) 116 : 389406 table 1 location and number of lesions detected with endoscopy vs . 
enteroclisi digiuno ileo prossimale ileo terminale ( ultimi 20 cm ) ileo terminale ( ultimi 20 cm ) colon prossimale colon distale - sigma non accessibile non accessibile 1 o > 1 sede pazienti numero di lesioni pazienti numero di lesioni endoscopico enteroclisi 1 or > 1 1 o > 1 table 2 signs and symptoms used to calculate the harvey - bradshaw index ( hbi ) tabella 2 segni e sintomi per calcolare lharvey - bradshaw index ( hbi ) signs and symptoms segni e sintomi general state of health condizioni generali good intermediate poor very bad abdominal pain absent mild moderate serious abdominal mass none not sure sure present and painful good intermediate bad very bad worst absent mild moderate serious dolore addominale massa addominale none not sure sure present and painful bouts of diarrhoea complications ( fistulas , abscesses ) number of stools complications ( fistulas , abscesses ) 1 point for each bout each complication 1 point each stool 1 score each complication 1 score ( ht ) , erythrocyte sedimentation rate ( esr ) and c - reactive protein ( crp ) ] ( table 4 ) [ 11 ]  . 
 two days prior to the examination , all patients took a 2 , 000 cc solution of polyethylene glycol ( peg ) in water ( selg 2000 , milan , italy ) to cleanse the bowel and were invited to follow a semiliquid diet and on the day of the examination to have nothing by mouth . 
distension of the small bowel was obtained with the administra ( hbi ) ( tabella 3 ) e sulla base dei valori di alcuni test di laboratorio ( conta dei globuli bianchi , ematocrito , velocit di eritrosedimentaione [ ves ] e proteina c reattiva ) ( tabella 4 ) [ 11 ]  . 
 due giorni prima dellesame , tutti i pazienti hanno assunto una soluzione acquosa di circa 2000 cc di polietilenglicole ( peg ; selg 2000 , milano , italia ) , allo scopo di ottenere unadeguata pulizia intestinale ed invitati ad una dieta semiliquida , mentre il giorno dellesame al digiuno completo . 
per i pazienti allergici si provveduto alla 392 table 3 disease activity of the sample examined with reference to the harveybradshaw index and laboratory tests patients disease activity tabella 3 attivit di malattia del campione in esame secondo lhbi ed i test di laboratorio pazienti attivit di malattia remission moderate serious remissione moderata severa tion of an 1 , 800 - cc solution of peg in water ( selg 2000 )  . small - bowel distension was achieved in 15 patients with the ingestion of the solution 3040 min prior to entering the scanner ( mr enterography ) , whereas in 25 patients , the solution was injected via the nasoenteric tube after they had entered the scanner ( mr enteroclysis )  . all patients were premedicated with 20 - mg i.v. 
of hyoscine - n - butylbromide to reduce intestinal peristalsis and segmentation of the bowel loops during the examination . this was injected in the patients who underwent mr enterography immediately prior to positioning in the scanner , whereas the patients who underwent mr enteroclysis were injected after the dynamic scan confirmed that the entire small bowel had been enhanced , after around 1 , 000 cc of solution . 
quindici pazienti hanno assunto per os la miscela in un intervallo variabile tra 3040 min prima del posizionamento nello scanner ( mr - os ) , mentre a 25 pazienti la soluzione stata iniettata dopo il loro posizionamento nello scanner , tramite sondino naso - enterico ( mr - e )  . tutti i pazienti sono stati premedicati con 20 mg ev di nbutilbromuro di joscina , per ridurre la peristalsi intestinale e la segmentazione delle anse durante lesecuzione dellesame ; nei pazienti sottoposti a mr - os stato iniettato subito prima del posizionamento nello scanner , mentre ai pazienti sottoposti ad mr - e stato iniettato dopo che , al controllo dinamico , tutto il piccolo intestino risultato opacizzato , dopo circa 1000 cc di soluzione . 
le immagini di mr - e e di mr - os sono state visualizzate ed analizzate in maniera random , indipendentemente , da due differenti radiologi , di cui uno con esperienza di 20 anni sulle patologie intestinali e sulla rm delladdome , laltro con unesperienza di 4 anni . 
i criteri di correttezza dellesecuzione degli esami si sono basati sulla valutazione di 11 parametri : radiol med ( 2011 ) 116 : 389406 table 4 criteria adopted in the 40 patients who underwent magnetic resonance imaging . 
the aim was to verify examination accuracy criteria result score fied at endoscopy and conventional enteroclysis ; fibrofatty proliferation went mr enteroclysis , t2 - weighted dynamic single - shot turbo spin echo ( tse ) functional sequences with fs were acquired in the coronal plane ( matrix 512512 , slice thickness 100 mm ; tr / te 4 , 000 / 299 , flip angle150 ) to monitor distension of the small - bowel loops . the post - contrast acquisitions were processed , and the time - intensity ( t / i ) curves were evaluated . 
mr enteroclysis and mr enterography images were visualised and analysed in a random fashion and independently by two radiologists : one with 20 years of experience in bowel disease and abdominal mr , and the other with 4 years of experience . the accuracy criteria for performing the examinations were based on the evaluation of 11 parameters : 1 . 
degree of distension of the loops ( evaluating both the mean diameter calculated between the two most distended loops and the two least distended loops of the entire length of the small bowel , and distension of all of the small - bowel loops ) ; 2 . 
presence of complications ( fistulas , abscesses ) ; all of these parameters were given a score ( table 4 )  . statistical analysis the accuracy of mr enterography and mr enteroclysis was calculated and compared with endoscopy and conventional enteroclysis . 
of identified lesions stenosis distension wall thickness contrast enhancement time / intensity curve comb sign lymph nodes complications stenosi dilatazione spessore di parete contrast enhancement curva i / t comb sign linfonodi fibro - fatty proliferation complicanze i , intensit ; t , tempo suboptimal optimal 1 or > 1 absent present absent present < 3 mm > 3 mm absent present inconsistent consistent absent present absent present absent present absent present subottimale ottimale 1 o > 1 assente presente assente presente < 3 mm > 3 mm assente presente non significativa 0 significativa assente presente assenti presenti assente presente assenti presenti tabella 4 criteri valutati nei 40 pazienti sottoposti ad esame rm per la valutazione della correttezza della tecnica di esame parametri giudizio score grado di distensione numero delle lesioni identificate results are reported in table 5 for patients who underwent mr enterography and table 6 for patients who underwent mr enteroclysis . 
il grado di distensione delle anse ( valutando sia il diametro medio calcolato fra le due anse pi distese e le due meno distese di tutti i tratti intestinali in esame , sia la distensione di tutte le anse dellintestino tenue ) ; table 5 accuracy criteria in patients who underwent magnetic resonance enterography no . 
la presenza di stenosi ( intesa come la riduzione del calibro dellansa > 80% rispetto al calibro delle anse contigue ) ; radiol med ( 2011 ) 116 : 389406 table 6 accuracy criteria in patients who underwent magnetic resonance enteroclysis no . 
of patients result score criteria distension quality number of identified lesions stenosis distension wall thickness contrast enhancement time - intensity curve comb sign lymph nodes fibrofatty proliferation complications grado di distensione numero delle lesioni identificate stenosi dilatazione spessore di parete contrast enhancement curva i / t comb sign linfonodi fibro - fatty proliferation complicanze i , intensit ; t , tempo suboptimal optimal 1 or > 1 absent present absent present < 3 mm > 3 mm absent present inconsistent consistent absent present absent present absent present absent present subottimale ottimale 1 o > 1 assente presente assente presente < 3 mm > 3 mm assente presente non significativa significativa assente presente assenti presenti assente presente assenti presenti tabella 6 criteri di correttezza nei pazienti sottoposti ad mr - e parametri numero pazienti giudizio score detected by mr enterography and mr enteroclysis . 
la dilatazione delle anse poste a monte rispetto alla stenosi ( incremento del calibro delle anse a monte > 2 / 3 rispetto al calibro delle anse non patologiche ) ; 5 . 
la presenza di complicanze ( fistole , ascessi )  . tabella 7 distensione delle anse intestinali nei pazienti sottoposti ad mros ; valori medi a tutti questi parametri stato assegnato uno score sede distensione digiuno ileo prossimale ileo distale 2 , 5 cm 2 , 2 cm 2 , 15 cm ( tabella 5 )  . analisi statistica stata calcolata laccuratezza diagnostica della mr - os e della mr - e , confrontandola con lendoscopia e con lenteroclisi convenzionale . 
la significativit statistica stata calcolata attraverso il test del 2 con correzione di yates . risultati i risultati ottenuti sono riportati in tabella 6 per i pazienti sottoposti ad mr - os ed in tabella 7 per i pazienti sottoposti ad mr - e . 
 gli esami rm ( mr - os , mr - e ) sono stati confrontati con lendoscopia e con lenteroclisi ; abbiamo costruito le tabelle di contingenza 22 e calcolato laccuratezza diagnostica . 
in particolare , nella tabella 11 sono stati confrontati i risultati dellmr - os con i risultati dellendoscopia e abbiamo ottenuto una sensibilit pari all89% , una specificit pari al 67% , un valore predittivo positivo pari al 94% , un valore predittivo negativo pari al 50% e una prevalenza dell86% . 
nella tabella 12 sono stati confrontati i risultati dellmr - e con i risultati dellendoscopia e abbiamo ottenuto una sensibilit pari al 90% , una specificit pari al 100% , un valore predittivo positivo pari al 100% , un valore predittivo negativo pari al 40% e una prevalenza dell94% . 
nella tabella 13 sono stati confrontati i risultati dellmr - os con i risultati dellenteroclisi e abbiamo ottenuto una sensibilit pari al 89% , una specificit pari al 33% , un valore predittivo positivo pari al 80% , un valore predittivo negativo pari al 50% e una prevalenza dell75% . 
2a - c curva a dispersione , in blu mr - os , in rosso mr - e ; in a rappresentazione della distensione per il digiuno ; in b rappresentazione della distensione per l ileo prossimale ed in c rappresentazione della distensione per l ileo distale . sensitivity , 33% specificity , 80% ppv , 50% npv and 75% prevalence . 
table 13 compares mr enteroclysis with conventional enteroclysis , and the following values were calculated : 91% sensitivity , 100% specificity , 100% ppv , 40% npv and 94% prevalence . 
the chi - squared value was 6.386 with one degree of freedom , and the p value was 0.0115. mr enteroclysis proved to be more effective than mr enterography in evaluating stenosis and its significance and also in evaluating bowel - wall thickness . 
nella tabella 14 sono stati confrontati i risultati dellmr - e con i risultati dellenteroclisi e abbiamo ottenuto una sensibilit pari al 91% , una specificit pari al 100% , un valore predittivo positivo pari al 100% , un valore predittivo negativo pari al 40% e una prevalenza dell94% . 
in addition , mr imaging has the advantage over traditional techniques of visualising the entire thickness of the bowel wall and the perivisceral loose connective tissue [ 16 , 17 ]  . 
bowel distension is the most important technical requirement for all imaging modalities , because a collapsed bowel loop can mask or lalta risoluzione di contrasto per i tessuti molli , lacquisizione multiplanare delle immagini e la possibilit di ottenere informazioni funzionali sono le condizioni che rendono la rm lindagine pi idonea per la valutazione delle malattie infiammatorie dellintestino tenue [ 15 ]  . 
la distensione intestinale il requisito tecnico pi importante da conseguire per tutte le metodiche di imaging , perch unansa collassata pu portare a misconoscere un processo patologico o mimarlo [ 19 ]  . 
bench unansa con pareti marcatamente ispessite si possa considerare patologica anche in assenza di adeguata distensione , nei pazienti con morbo di crohn , per le caratteristiche proprie di questa malattia , devono essere riconosciuti tutti i tratti coinvolti dal processo . 
ne consegue che lottimizzazione della metodica permette lidentificazione del maggior numero di lesioni individuabili con la rm , e pertanto un incremento della sensibilit . alcuni autori [ 20 ] sostengono che sebbene la distensione intestinale sia superiore nei pazienti sottoposti a mr - e rispetto a pazienti sottoposti a mr - os , tuttavia essa non comporta significative differenze gestionali tra i due gruppi . 
although a bowel loop with markedly thickened walls can be considered pathological even in the absence of adequate distension , in patients with crohns disease , due to the particular characteristics of this disease , all of segments involved in the process need to be identified . 
therefore , optimisation of the technique enables identification of the highest number of lesions identifiable with mr , and therefore increases sensitivity . some authors [ 20 ] suggest that although bowel distension is greater in patients undergoing mr enteroclysis than in patients undergoing mr enterography , this produces no significant difference between the two groups . 
in our study , some of the bowel loops , including jejunal and proximal loops , of patients who underwent mr enterography were partially collapsed , and therefore , an evaluation of bowel - wall thickness as an indicator of the presence or absence of disease was not adequate [ 22 , 23 ]  . 
 nel campione in esame la non significativit numerica dei pazienti con localizzazione al digiuno e allileo prossimale , non consente di ottenere dati statisticamente rilevanti , sebbene sia da sottolineare come nel solo paziente in cui era presente un focolaio digiunale e sottoposto ad mr - os la lesione sia stata misconosciuta allesame di rm , cos come sono state misconosciute alla mr - os le due lesioni poste allileo prossimale e note allenteroclisi , mentre stata confermata la lesione ileale prossimale , riscontrata allenteroclisi , nel paziente sottoposto ad mr - e . 
 [ 23 ] , in accordo con la clinica e gli indici di laboratorio , hanno proposto una classificazione della malattia che tenga conto degli aspetti iconografici , identificando quattro sottovarianti , infiammatoria attiva , fistolizzante , fibrostenotica e riparativa - rigenerativa . 
le lesioni ulcerative , aftoidi e penetranti , vengono facilmente identificate con la rm , come delle irregolarit nel profilo della mucosa , rispettivamente come un nidus ad elevata intensit ( cratere ulcerativo ) circondato da un anello ad intensit medio - alta ( edema perilesionale ) , e come una linea ad elevata intensit di segnale che si approfondisce nello spessore parietale , mentre la mucosa sana tra le lesioni pu assumere aspetto pseudopolipoide [ 24 ]  . 
 sia la mr - os che la mr - e nel nostro studio , confrontate con lendoscopia , hanno presentato una sensibilit ed una specificit elevata nellidentificazione delle lesioni di parete poste allileo terminale ( tabelle 11 e 12 ) , con alto valore predittivo positivo e basso valore predittivo negativo , sebbene la mr - e presenti una sensibilit e una specificit superiore rispetto alla mr - os ( p = 0 , 0115 vs 0 , 143 )  . 
diversamente , dai nostri dati , emerge che nella valutazione delle lesioni poste a sede prossimale , e quindi al digiuno ed allileo prossimale , la mr - e abbia una sensibilit , una specificit ed un valore predittivo positivo superiore e un valore predittivo negativo inferiore rispetto alla mr - os ( tabelle 13 e 14 ) , come effetto di uninadeguata distensione delle anse ottenuta con questa ultima tecnica ( p = 0 , 5271 vs 0 , 0115 )  . 
la rm correla bene con la clinica , infatti i pazienti con sintomatologia lieve o moderata ( tabella 3 ) presentano un quadro iconografico e funzionale caratterizzato da stenosi non significative ed assenza di complicanze , diversamente nei pazienti con attivit severa secondo hbi ( tabella 3 ) , i reperti riscontrati , quali ascessi , fistole , occlusione , comb sign hanno presentato una maggiore frequenza rispetto al gruppo moderato ( tabelle 6 e 7 )  . 
a nostro avviso proprio la minor distensione del lume conduce ad una sovrastima del reperto , mentre solo una adeguata valutazione della stenosi indirizza al trattamento pi idoneo , e quindi alla corretta gestione del paziente [ 20 , 21 ]  . 
esame mr - e , sequenza trufi in coronale ; si noti l adeguato grado di distensione digiunale . in our patient population , the nonsignificant number of patients with disease involving the jejunum and the proximal ileum did not allow statistically significant data to be obtained . 
also unrecognised at mr enterography were the two lesions located in the proximal ileum and identified at conventional enteroclysis , whereas the proximal ileal lesion identified at conventional enteroclysis in the patient who underwent mr enteroclysis was confirmed . 
 [ 24 ] , in accordance with clinical and laboratory findings , proposed a classification that takes into account imaging appearance and identifies four subtypes : active inflammatory , fistulizing / perforating , fibrostenotic and reparative or regenerative . 
ulcerating , aphthoid and penetrating lesions are easily identified with mr as irregularities of the mucosa profile , respectively as a nidus of elevated intensity ( ulcerating crater ) surrounded by a ring of mediumhigh intensity ( perilesional oedema ) and as a line of elevated signal intensity that deepens in the wall , whereas the healthy mucosa between the lesions has a pseudopoly402 radiol med ( 2011 ) 116 : 389406 poid appearance [ 25 ]  . 
 some authors have compared mr imaging with the hbi when evaluating disease activity in crohns disease [ 11 ]  . we analysed the same parameters ( table 4 ) and obtained the same results ( tables 5 and 6 )  . 
instead , in patients with severe disease activity according to the hbi ( table 2 ) , findings such as abscesses , fistulas , occlusion and the comb sign are much more frequent than in the moderate group ( tables 5 and 6 )  . 
we suggest that the lesser distension of the lumen leads to an overestimation of the finding , whereas only an adequate evaluation of the stenosis can ideally orient treatment and thus prompt correct patient management [ 20 , 21 ]  . 
once an adequate degree of distension has been achieved , the real degree of stenosis can be quantified by evaluating proximal dilatation and comparing it with the information provided by t2 - weighted and contrastenhanced images ; then , from an analysis of the t / i curves , a fibrous stenosis can be differentiated from an inflammatory stenosis . 
raggiunto un adeguato grado di distensione e valutando la dilatazione a monte possibile quantificare il reale grado di stenosi e confrontando tale dato con le informazioni fornite dalle immagini t2 - w e postcontrasto e quindi dallanalisi delle curve i / t , differenziare una stenosi fibrotica da una infiammatoria . 
nelle immagini t2 - w la sottomucosa di un tratto stenotico tendenzialmente ipointensa , mentre nella stenosi infiammatoria presenta una elevata intensit di segnale , espressione di edema ed infiltrato cellulare . 
le sequenze single shot , attuabili solo in corso di mr - e , radiol med ( 2011 ) 116 : 389406 consentono , quindi una valutazione di ordine dinamicofunzionale , rappresentando un valore aggiunto alla tecnica . unadeguata distensione determina una corretta definizione dello spessore parietale e di conseguenza nella valutazione delle curve di i / t pi semplice lapposizione della regione di interesse ( roi ) , riducendo il rischio di errore nel postprocessing . unulcera transmurale quando supera la tonaca muscolare determina uninfiammazione nel tessuto mesenteriale adiacente , che pu evolvere in un piccolo ascesso peri - intestinale . 
un tramite fistoloso di piccola entit difficilmente identificabile sulle immagini ed apparire come delle irregolarit nodulari o spiculature della superficie sierosa dellansa ; diversamente per fistole di maggiori entit , nelle sequenze t2 - w la penetrazione del mdc nelle stesse che ne consente lidentificazione come delle immagini lineari ad elevata intensit di segnale , perpendicolari alla parete intestinale , mentre nelle sequenze acquisite dopo somministrazione di mdc ev , quando associate a reazioni desmoplastiche del grasso mesenteriale assumono aspetto stellato . 
gli svantaggi della metodica sono legati allintubazione naso - enterica , sia per il costo del sondino sia per lesposizione a radiazioni ionizzanti , necessaria per il controllo del suo posizionamento , sia per il maggior tempo richiesto , sebbene quando condotta da operatore esperto richieda al massimo 5 minuti . 
il nostro studio ha escluso pazienti pediatrici , ove la scarsa collaborazione e compliance dei pazienti giustifica lutilizzo dellmr - os . conclusioni la risonanza magnetica divenuta negli ultimi anni la metodica di imaging che meglio affianca lendoscopia nella prima diagnosi e nel follow - up dei pazienti con morbo di crohn consentendo una valutazione sia di dettaglio che panoramica [ 22 ]  . 
5 paziente donna 30 anni con diagnosi di morbo di crohn ( localizzazione ileo terminale ) , sottoposta ad mr - e : sequenza funzionale single shot idrografica . inflammatory stenosis , signal intensity is increased due to oedema and cellular infiltrate . 
adequate distension makes possible accurate definition of wall thickness and as a result facilitates placing a region of interest ( roi ) when evaluating t / i curves , thus reducing the risk of postprocessing error . a transmural ulcer , when it exceeds the muscular coat , causes inflammation of the adjacent mesentery , which can develop into a small peri - intestinal abscess . 
a small fistula is difficult to identify on the images and appears as a nodular irregularity or spiculation of the serous surface of the loop . with larger fistulas , penetration of the contrast material into the fistula itself makes its identification possible in t2weighted sequences , in which it appears as a linear hyperintensity running perpendicular to the intestinal wall . 
contrast material , when associated with desmoplastic reactions of the mesentery fat , the fistula has a stellate appearance . 404 radiol med ( 2011 ) 116 : 389406 abscesses or inflammatory masses are less common than fistulas , and adequate bowel distension is the most important requirement for identifying enteroenteric fistulas . 
the disadvantages of the technique are related to nasoenteric intubation , not only in terms of tube cost and exposure to ionising radiation needed to monitor tube placement , but also with regard to the longer time required , even though this does not exceed 5 min when performed by an expert operator . 
our study did not include paediatric patients , in whom poor cooperation and compliance justifies the use of mr enterography . conclusions in recent years , mr has become the imaging modality that best supports endoscopy in the initial diagnosis and followup of patients with crohns disease , as it makes possible a detailed and panoramic evaluation [ 22 ]  . 
7 a a 26 - year - old male patient affected by crohns disease located in the terminal ileumagnetic resonance ( mr ) enterography , coronal true fast induction steady - state potential sequence : distinct involvement of the last ileal loop , limited distension of the jejunum folds . 
b enteroclysis : jejunal lesions not identified by mr - os . radiol med ( 2011 ) 116 : 389406 clysis ; the possibility of extraluminal evaluation ; and the absence of ionising radiation justify the growing interest in the technique [ 16 ]  . mr enteroclysis , thanks to the adequate distension it provides of all bowel loops , including the jejunum and the proximal small - bowel loops , is the technique that best enables accurate assessment of crohns disease . 
mr enteroclysis enables identification of a stenotic segment , evaluation of significance or insignificance , definition of characteristics whether inflammatory or fibrous and therefore guidance towards the most appropriate treatment . 
the possibility of obtaining dynamicfunctional information , which can only be achieved with mr enteroclysis , makes it a unique imaging modality . bile a quella fornita dallenteroclisi baritata , la possibilit di una valutazione extraluminale ed il non utilizzo delle radiazioni ionizzanti giustificano il crescente interesse rivolto a tale metodica [ 16 ]  . la mr - e , fornendo unadeguata distensione di tutte le anse del tenue , anche del digiuno e del tenue prossimale , la tecnica che meglio consente una corretta definizione del morbo di crohn . 
con lmr - e possibile individuare un tratto stenotico , ma anche valutarne la significativit o non significativit , definirne le caratteristiche , infiammatoria o fibrotica , e quindi indirizzare il paziente al trattamento pi idoneo . 
6 peoples hospital af liated to shanghai jiaotong university , 600 yishan road , shanghai , 200233 china 2 department of radiology , ruijin hospital af liated to shanghai jiaotong university , school of medicne , 197 ruijin er road , 200025 china 3shanghai jiaotong university , school of medicine , 227 chong qin nan road , shanghai , 200025 china correspondence to : z . 
all ndings were analysed prospectively and correlated with tumour / node / metastasis ( tnm ) staging , dukes staging , histological grading , presence of lymph node metastasis , serosal involvement and mvd . 
a livello del tessuto tumorale e della parete rettale indenne sono stati calcolati i seguenti parametri : costante di transito ( ktrans ) , la percentuale dello spazio di distribuzione extravascolare extracellulare leakage space ( ve ) e la rate constant ( kep )  . la densit microvascolare stata stimata mediante analisi immunoistochimica su sezioni del pezzo operatorio . 
 il valore della costante di transito ( ktrans ) risultato signi cativamente diverso in caso di presenza o meno di coinvolgimento linfonodale di malattia ( p = 0 , 000 ) e nei diversi stadi sia secondo la classi cazione di dukes ( p = 0.04 ) che secondo il ptnm ( p = 0 , 03 )  . 
lo studio dinamico mediante risonanza magnetica 3d rappresenta un valido strumento diagnostico per la valutazione della vascolarizzazione tumorale . parole chiave carcinoma del retto risonanza magnetica studio dinamico post - contrasto angiogenesi prognosi introduction with 655 , 000 deaths worldwide per year , colorectal cancer is the fth most common form of cancer in the united states and the third leading cause of cancer - related death in the western world [ 1 , 2 ]  . 
generally , it is measured by microvessel density ( mvd ) , which depends on the availability of postoperative tissue or adequate biopsy materials and is somewhat invasive [ 6 ]  . 
however , as yet , there is no satisfactory imaging modality to predict prognosis and to assist in the selection of the right patients for extended surgical procedures and trials of adjuvant chemotherapy . 
the microcirculation can be assessed by semiquantitative evaluation of the signal intensity curve or by quanti cation of the change of contrast - agent concentration with kinetic modelling techniques [ 14 ]  . 
semiquantitative evaluation has the advantage of a good intrinsic signal - to - noise ratio ( snr ) , but it does not re ect the rate at which contrast medium passes from the intravascular space to the extravascular extracellular space ( ees ) and then back to the intravascular space over time after bolus injection . 
concentration - time curves ( ctc ) are then mathematically tted using [ 15 ] modelling parameters that include the volume transfer constant ( ktrans ) of the contrast agent , leakage space as a percentage of unit volume of tissue ( ve ) and the rate constant ( kep also called k21 )  . 
as far as we know , the correlation between dce - mr imaging and angiogenesis is controversial , and few studies have investigated the relationship between 3d - dce - mr parameters and angiogenesis [ 6 , 21 , 22 ]  . 
 the primary aim of this prospective study was to evaluate the relationship between 3d - dce - mr parameters and clinicopathological features of rectal cancer and assess their potential as new radiological prognostic predictors . material and methods 368 patients after adequate bowel preparation , 26 patients ( ten men , 16 women ; age range 2875years ; mean 58.310.5 ) with pathologically proved rectal cancer ( from may 2009 to february 2010 ) were prospectively included in this study . 
 magnetic resonance imaging and analysis mr studies were undertaken on a 1.5 - tesla supermagnetic mr scanner ( ge - signa hdx1.5t , ge medical systems , milwaukee , wi , usa ) using a phased - array body coil . 
 after plain scan ( t1 mapping ) , multiphase t1 - weighted dce - mr images were obtained using a spoiled gradientecho sequence ( lava ) in the axial plane . 
the following quantitative kinetic parameters were calculated automatically : volume transfer constant of the contrast agent ( ktrans ) , rate constant ( kep ) and volume as a percentage of the extravascular extracellular leakage space ( ve )  . 
 on the basis of the precontrast images , a region of interest ( roi ) covering the whole lesion and normal rectal wall with exclusion of peripheral fat , artefact and blood vessels was drawn over the tumour by a radiologist with 8 years of experience in gastrointestinal radiology . 
histograms of pixel data were obtained from all acquired tumour slices , and mean values were recorded for further study . microvessel staining and evaluation all patients were evaluated pathologically for the histological diagnosis and mvd counting . 
for surgically resected specimens , tissue blocks were obtained by sectioning each tumour with reference to the plane of imaging of the radiol med ( 2011 ) 116 : 366374 corresponding preoperative mr image as far as possible . 
 tissue blocks were dehydrated in graded alcohols , and microvessel density ( mvd ) was estimated by immunohistochemical staining of surgical specimens with anti - cd34 monoclonal antibody ( dako , denmark ) [ 23 ]  . 
 [ 24 ] : any single brown - staining endothelial cell or small clusters of brown - staining endothelial cells , with or without a lumen , and clearly separated from adjacent microvessels , tumour cells and other connective tissue elements were considered as individual vessels . 
 after screening the areas with intense neovascularised spots in a low power eld ( 40 ) , microvessels in the area with the highest number of discrete microvessels were counted in a 200 eld . 
differences of ktrans , kep and mvd between different histological grading , presence of lymph node metastasis , serosal involvement and dukes staging were compared with the analysis of variance ( anova ) test . 
spearman rank correlation tests were used to determine the strength of the relations between the dce - mr parameters , mvd , ptnm [ tumour / node / metastasis system from the american joint committee on cancer ( ajcc ) ] , dukes staging and histological grade . 
 results following the total mesorectal excision ( tme ) principle , 24 / 26 patients underwent standard rectal cancer resection , including miles and dixons operation , and the remaining two were treated with palliative surgery . 
tumour : transfer constant ( ktrans ) 11.971 / min , leakage space ( ve ) 12.2% and rate constant ( kep ) 98.331 / md detection of endothelial cells by anti - cd34 antibody in poorly differentiated gastric cancer : numerous microvessels are seen ( 200 )  . 
tumore : k trans 11 , 971 / min , leakage space ( ve ) 12 , 2 % e rate constant ( kep ) 98 , 331 / md marcatura delle cellule endoteliali mediante anticorpo anti - cd34 in un carcinoma gastrico scarsamente differenziato : notare la notevole densit microvascolare ( mvd 32 in un campo a 200 )  . 
tumour : transfer constant ( ktrans ) 2.559 / min , leakage space ( ve ) 19.5% and rate constant ( kep ) 13.11 / md detection of endothelial cells by anti - cd34 antibody in moderately differentiated gastric cancer : numerous microvessels are seen ( 200 )  . 
marcatura delle cellule endoteliali mediante anticorpo anti - cd34 in un carcinoma gastrico moderatamente differenziato : notare la notevole densit microvascolare ( mvd 34 in un campo a 200 )  . 
 discussion in previous reports , investigators have suggested that gadolinium - enhanced or dynamic mr imaging may be useful for evaluating ktrans in colorectal [ 26 ] and prostate cancer in selected patients [ 17 , 27 ]  . 
this nding might also be due to the larger tumour size in the late stage , with necrosis in the tumour centre , re ecting the heterogeneity of the tumour in the late stage . 
tumour : transfer constant ( ktrans ) 3.680 / min , leakage space ( ve ) 20.4% and rate constant ( kep ) 18.07 / md detection of endothelial cells by anti - cd34 antibody in well - differentiated gastric cancer : few microvessels are seen ( 200 )  . 
the heterogeneity of tumour predominates the biology in the late stage , and a mixed situation occurs most commonly when neither ow nor permeability surface area product predominates [ 14 ]  . 
another reason could be the case of signet - ring cell carcinoma , a rare form of adenocarcinoma of the large intestine , in which mean mvd was signi cantly lower than mean mvd in adenocarcinoma [ 22 , 28 ]  . 
another case of mucinous cell carcinoma might also have contributed to the decrease of ktrans , as there is excess mucin production and rather lower vessel distribution [ 13 , 22 , 28 ]  . 
 ve re ects the situation in extravascular extracellular space , as the extravascular extracellular space and the vascular space are balanced in size and shape to ensure adequate supply of nutrients and oxygen to the tissue , and this balance could be disturbed in malignant tissues . 
this might be because of tumour angiogenesis , characterised structurally by abnormal blood vessels lacking the usual vessel hierarchy and having a chaotic , heterogeneous distribution , and the extravascular extracellular space could be variable . 
much attention has been paid to the change of ve before and after treatment , and nowadays , ve is regarded as a prognostic parameter for the outcome of cancer treatment , especially chemotherapy or radiotherapy , which was not included in our study [ 29 , 30 ]  . 
 the main impetus of this study was to nd the indicator of prognosis preoperatively and nontraumatically , and the prognosis is determined by tumour in ltration , extension and stage , especially the tnm syste compared with kep , which proved to have a moderate relationship with tnm , ktrans revealed a medium - to - large positive correlation with all of these prognostic indicators . 
 radiol med ( 2011 ) 116 : 366374 microvessel density has also been correlated with colorectal tumour grade and stage in some reports [ 3336 ] , whereas other studies show no relation between microvessel density and patient outcome [ 3739 ]  . 
it might be that tumour vessels are structurally and functionally abnormal , with uneven diameters , increased length and tortuosity , multiple arteriovenous shunts and loss of physiological regulation of blood ow . 
unlike organs such as the uterus and prostate gland , where little change in organ morphology occurs on formalin xation , rectal cancer is more challenging to evaluate because of changes in tumour shape and shrinkage during tissue processing [ 21 ]  . 
in fact , distribution of gd - dtpa is determined not only by mvd but also by vessel permeability and size of the extravascular extracellular space [ 41 , 42 ]  . 
 in this study , the 3d - dce - mr technique enabled greater coverage of tumour volume , with thinner slice thickness ( 4 mm ) and multiple data sets acquired every 8 s rather than 1215 s or 30 s , as in previous reports [ 6 , 19 , 20 ]  . 
 one of the limitations in our study is that the sample size was small , and no estimation of demarcation point of ktrans value could be provided for tnm staging or dukes staging in clinical practice . 
as there are only two patients with signet ring or mucinous cell carcinoma in our study , it is impossible to analyse the changes of ktrans value in the different histological types . 
franco , e - mail : fabiofranco.email@gmail.com received : 17 march 2010 / accepted : 2 june 2010 / published online : 12 january 2011 springer - verlag 2011 abstract purpose . 
during this period , 46 patients were admitted for splenic trauma , of whom 17 were treated surgically , 15 conservatively and 14 with percutaneous embolisation ( 13 men , mean age 44.8 , mean injury severity score 18.5 , six with grade iv and eight with contrast blush )  . 
patients in shock were referred for laparotomy and splenectomy , whereas those who were haemodynamically stable or responsive to uid resuscitation were further evaluated with computed tomography ( ct )  . 
in the presence of imaging evidence of splenic injury ranging from grade i to grade iii ( n = 15 ) a conservative approach was adopted , whereas haemodynamically unstable patients with grade v injury ( n = 17 ) were treated with splenectomy . 
in questo periodo sono stati ammessi 46 pazienti con lesione splenica posttraumatica , di cui 17 sono stati trattati chirurgicamente , 15 con trattamento conservativo e 14 con embolizzazione percutanea ( 13 maschi , et media 44 , 8 , injury severity score [ iss ] 18 , 5 circa , 6 con grado iv e 8 con stravaso di mezzo di contrasto )  . 
i pazienti in stato di shock sono stati immediatamente sottoposti a laparotomia e splenectomia , mentre quelli emodinamicamente stabili o responsivi alla somministrazione di uidi sono stati valutati con tc . 
in base al dato strumentale , in 15 pazienti , con lesioni spleniche di grado i , ii e iii stato considerato il trattamento conservativo , mentre 17 pazienti emodinamicamente instabili , con lesioni di v grado , sono stati sottoposti a splenectomia . 
in 13 casi sono state posizionate spirali rm compatibili con diametro variabile tra 4 e 6 mm ; in un solo paziente sono state iniettate solo radiol med ( 2011 ) 116 : 454465 to reach a quick decision on the most appropriate treatment for patients presenting with blunt abdominal trauma , and splenic artery embolization seems to offer a reliable option in those with high - grade splenic injury or active bleeding . keywords blunt splenic injury , splenic artery embolization nonoperative management spleen splenic salvage particelle riassorbibili . 
in 13 / 14 casi ( 92 , 9% ) non sono state osservate complicanze post - procedurali , mentre in un solo paziente , trattato con particelle riassorbibili , si resa necessaria la splenectomia per recidiva di sanguinamento a 24 ore dallembolizzazione . 
sulla base del nostro algoritmo , possibile una veloce decisione sul trattamento pi opportuno delle lesioni spleniche post - traumatiche e lembolizzazione percutanea sembra offrire unaf dabile opzione in pazienti con lesioni dorgano di grado elevato o con sanguinamento attivo . parole chiave trauma splenico embolizzazione dellarteria splenica management conservativo milza salvataggio di milza introduction introduzione blunt abdominal trauma frequently causes splenic injury , and splenectomy has long been considered the treatment of choice . 
the spleen has important immune functions : it lters the blood , removing particulate antigens , bacteria and damaged red cells ; it produces immunoglobulin , tuftsin , opsonin and properdin and stores white blood cells [ 2 ]  . 
in both children and adults , the asplenic condition is an important risk factor for postsplenectomy infections , such as pneumonia , subphrenic abscess , pancreatitis , meningitis and sepsis , as has emerged from several large series [ 2 , 3 ]  . 
it consists of bed rest associated with close haemodynamic , clinical and imaging evaluation in the attempt to obtain a natural haemostasis noninvasively , reserving the surgical approach for those manifesting a recurrence of bleeding . 
rebleeding itself represents the most frequent cause of failure of this approach [ 511 ]  . splenic artery embolization ( sae ) in blunt abdominal trauma was rst proposed by sclafani et al . 
the aim of this study , which focuses on the periprocedural 30 - day period , was to evaluate the results of our experience with transarterial embolization in patients with blunt splenic injury . i traumi addominali provocano spesso lesioni spleniche e la splenectomia stata considerata per lungo tempo il trattamento di scelta . 
la milza , infatti , ha importanti funzioni , in particolare per limmunit : un ltro per il sangue , rimuove particolari antigeni , batteri e globuli danneggiati , produce immunoglobuline , tuftsina , opsonine , properdina ed un deposito di globuli bianchi [ 2 ]  . 
sia nei bambini che negli adulti , lasplenia un importante fattore di rischio per le infezioni post - splenectomia , come polmoniti , ascessi subfrenici , pancreatiti , meningiti e sepsi , come emerso da diversi studi [ 2 , 3 ]  . 
il management non - operativo ( nom ) si sta affermando , con crescente successo , per preservare le funzioni della milza ed ora considerato unopzione ef ciente nei pazienti emodinamicamente stabili con trauma splenico . 
 esso consiste nel riposo a letto associato a controlli seriati emodinamici , clinici e strumentali , nel tentativo di ottenere unemostasi naturale in modo non invasivo , riservando lapproccio chirurgico solo per coloro che manifestano una recidiva di sanguinamento . 
lobiettivo di questo lavoro , concentrato sul periodo periprocedurale di 30 giorni , quello di valutare i risultati della nostra esperienza di embolizzazione percutanea in pazienti con lesioni spleniche sanguinanti . 
the purpose of the protocol was to accelerate decisions on the proper therapeutic approach on the basis of haemodynamic status , the suspicion of abdominal trauma involving the spleen and the grade of splenic injury . 
according to the algorithm , patients presenting with shock [ blood pressure 90 mmhg ; shock index ( ratio of heart rate to systolic blood pressure ) 1.0 ] were treated with uid resuscitation following the recommendations of advanced trauma life support [ 23 ]  . 
in the presence of splenic damage , treatment was chosen on the basis of injury severity as graded by ct following the american association for the surgery of trauma organ injury scale ( table 1 ) [ 24 ]  . 
scopo del protocollo stato quello di accelerare la scelta di un corretto approccio terapeutico sulla base dello stato emodinamico , il sospetto di trauma addominale con coinvolgimento della milza e il grado di lesione della milza . 
secondo lalgoritmo , i pazienti che presentano shock ( pressione sanguigna 90 mmhg ; indice di shock rapporto tra frequenza cardiaca e pressione sistolica 1 , 0 ) vengono trattati con somministrazione di uidi e secondo le raccomandazioni di advanced trauma life support [ 23 ] , nei casi in cui non si sia ottenuta una risposta pressoria , i pazienti con forte sospetto di lesioni negli organi addominali , sono sottoposti a laparotomia durgenza ed eventuale splenectomia , con la sola valutazione clinica ed ecogra ca . 
in presenza di lesione splenica la terapia stata scelta in base al danno , classi cato alla tc secondo lamerican association for the surgery of trauma splenic injury scale ( tabella 1 ) [ 24 ]  . 
surgery was considered for splenic lesions associated with coexisting abdominal injuries needing laparotomy or for grade v splenic injury or in the case of conservative treatment failure , with bleeding recurrence . mico , riposo a letto , emoglobina sequenziale , ematocrito e monitoraggio ecogra co . 
la chirurgia stata considerata , solo , per lesioni spleniche associate a coesistenti lesioni addominali che necessitavano di laparotomia o per danni splenici di grado v o in caso di fallimento del trattamento conservativo , con recidiva di sanguinamento . 
ct examinations were evaluated by the attending radiologist on a dedicated workstation ( leonardo , siemens ) and integrated by multiplanar and sono state effettuate scansioni con tc spirale a 64 strati ( sensation 64 , siemens , forcheim , germania ) dopo la somministrazione di mezzo di contrasto endovenoso ( 300 mg / ml iomeprolo , iomeron 300 , bracco , milano , italia ) alla dose di 2 , 5 ml / kg peso , per un massimo di 120 ml , a un tasso di 22 , 5 ml / s ; il bolus - tracking stato utilizzato per ottimizzare la scansione per le fasi arteriose e venose . 
gli esami tc sono stati valutati dal medico radiologo su una stazione di lavoro dedicata ( leonardo , siemens , germania ) integrata da rico458 radiol med ( 2011 ) 116 : 454465 volume - rendered reconstructions and assessed for grade of splenic injury . struzioni multiplanari e volume - rendering . 
 transarterial embolization embolizzazione arteriosa percutaneous embolization was performed in 14 patients ( 13 men , mean age 44.8 ) , of whom six had grade iv splenic injuries , and eight ( with grade iiii injuries ) had ct evidence of contrast blush . 
arteriography and subsequent splenic embolization , planned on ct ndings , was achieved in the angiography suite ( integris bn 3000 , philips healthcare , eindhoven , the netherlands ) by an experienced interventional radiologist who was always present or available on call . 
embolisation was achieved through a 45 f cobra or simmons catheter ( glidecath , terumo , tokyo , japan ) or by a coaxial microcatheter ( progreat , terumo , tokyo , japan ) , whereas vessel occlusion was carried out mainly by coil ( 46 mm ) delivery ( mreye , william cook europe , bjaeverskov , denmark ) to exclude the damaged area from blood in ow , as proved by periprocedural angiography . 
in one case only was the artery occluded by injection of gelfoam pledgets ( spongel , yamanouchi , tokyo , japan ) , whereas in another case , occlusion was obtained by the combination of coil implantation and injection of gel - foam pledgets . right in the case of parenchymal injury involving completely the spleen or a large part of the organ , the main splenic artery was occluded ( proximal embolisation )  . 
 in patients treated by embolization , we evaluated the following : immediate technical success , de ned as capacity to reach the damaged vessel or feeding artery until exclusion of direct blood ow to the spleen was proved by angiography ; procedural success , de ned as a permanent haemostasis with no recurrent bleeding needing further interventions ; lembolizzazione percutanea , stata eseguita in 14 pazienti ( 13 maschi , et media 44 , 8 ) , di cui 6 casi con lesioni spleniche di grado iv e in 8 casi ( grading da i a iii ) , la tc ha dimostrato un blush di mdc . 
larteriogra a e la successiva embolizzazione splenica , piani cata in base ai risultati tc , stata realizzata in sala angiogra ca ( integris bn 3000 , philips sanit , eindhoven , olanda ) da un radiologo interventista esperto , sempre reperibile . 
lembolizzazione stata ottenuta attraverso un catetere 45 f cobra o simmons ( glidecath , terumo , tokyo , giappone ) , o da un microcatetere coassiale ( progreat , terumo , tokyo , giappone ) , mentre locclusione di vasi stata effettuata principalmente mediante posizionamento di spirali metalliche rm compatibili con diametro variabile tra 4 e 6 mm ( mreye , william cook europe , bjverskov , danimarca ) , escludendo la zona danneggiata dallaf usso di sangue , come dimostrato da un controllo angiograco periprocedurale . 
in un solo caso , per occludere i vasi sanguinanti , sono state usate particelle riassorbibili ( spongel , yamanouchi , tokyo , giappone ) ed in un altro particelle riassorbibili in combinazione con spirali metalliche . in caso di lesioni parenchimali che coinvolgevano completamente la milza o grande parte dellorgano , stata occlusa larteria splenica principale ( embolizzazione prossimale )  . 
con la punta del catetere allinterno dellarteria splenica , ma distalmente allostio dei maggiori vasi collaterali ( come larteria dorsale del pancreas ) , stata effettuata lembolizzazione no a fermare il usso di sangue attraverso larteria . 
nei pazienti trattati con lembolizzazione , abbiamo valutato : il successo tecnico immediato , de nito come la capacit di ricercare il vaso danneggiato o larteria afferente la lesione , bloccando il usso sanguigno diretto alla milza e comprovarlo al controllo angiogra co periprocedurale ; il successo procedurale , de nito come una emostasi permanente senza risanguinamenti che necessiterebbero ulteriori interventi ; la preservazione della milza , de nito come il mantenimento della vitalit dellorgano no alla dimissione o su 30 giorni di follow - up ; radiol med ( 2011 ) 116 : 454465 table 2 summary of main clinical data and embolization results patient no . 
proximal embolization was chosen in eight cases : six procedures were done with coil implantation , one with injection of gel - foam pledgets and another by a combination of coil implantation and injection of gelfoam pledgets . 
selective embolisation was preferred in six la morbilit - mortalit o complicazioni inerenti alle procedure , de nite come qualsiasi evento avverso rilevante correlato alla procedura ; lintervallo di tempo tra larrivo allospedale e la procedura terapeutica . 
 risultati di 46 pazienti , 17 ( con stato emodinamico instabile ) sono stati trattati chirurgicamente , 15 in modo conservativo ( di cui per 2 stato necessario lintervento chirurgico per risanguinamento ) e 14 sono stati sottoposti ad embolizzazione percutanea . 
lembolizzazione prossimale stata scelta in 8 casi : 6 procedure di posizionamento di spirali , in 1 caso si sono iniettate solo particelle riassorbibili e in un altro caso locclusione stata ottenuta con la combinazione di posizionamento di spirali ed liniezione di particelle riassorbibili ( tabella 2 )  . 
in 13 / 14 cases ( 92.9% ) , no bleeding recurrence was observed ; in one case , the only patient treated with gel - foam particles , urgent splenectomy was required for bleeding recurrence within 24 h of embolization . 
the mean time from hospital arrival to percutaneous embolisation was 171 min ( 120300 min ) ( table 2 )  . ottenuto in tutti i casi , con esclusione completa della lesione dal usso sanguigno ( tabella 2 )  . 
il tempo medio dallarrivo in ospedale allesecuzione dellembolizzazione percutanea stato di 171 minuti ( 120300 min ) ( tabella 2 )  . discussion discussione treatment of blunt splenic injury has evolved in recent decades . 
il management non - operativo ( nom ) stato valutato in diversi studi che indicano globalradiol med ( 2011 ) 116 : 454465 reports , which indicate overall spleen salvage of 57%91% [ 510 , 14 ] , becoming the standard of care in patients presenting with stable haemodynamic values on admission . 
in particular , ct provides rapid and reliable detection of splenic injury and real - time evaluation of its degree , directing the patient to a suitable therapeutic option , namely , nonoperative treatment or percutaneous embolization or surgery . 
in addition , ct is useful for identifying possible associated lesions [ 25 , 26 ]  . with a view to reducing unnecessary surgical interventions , a modi ed algorithm has been adopted to accelerate decisions on proper treatment in patients with blunt abdominal trauma involving the spleen . 
subsequently , on the basis of the ct ndings , patients underwent embolisation in the presence of grade iv splenic injury or , regardless of injury grade , evidence of intraparenchymal contrast blush or posttraumatic pseudoaneurys emergency surgery was reserved for grade v injury or haemodynamically unstable patients . in our experience , the algorithm allows for quick decisions and the opportunity to carry out splenic embolisation in posttraumatic injuries : mean embolisation time from hospital admission to procedure was 171 min ( 120300 min )  . 
embolization of the main splenic artery ( proximal embolisation ) was carried out in the event of diffuse organ damage , and segmentary artery occlusion ( distal embolisation ) was performed on those with localised injury . 
natural repair and splenic vitality is guaranteed through a collateral circulation arising from the greater pancreatic , dorsal pancreatic and short gastric arteries , avoiding direct blood in ow and pressure on the damaged spleen . 
no collateral ow is possible , and the mente un risparmio della milza tra 57%91% [ 510 , 14 ] , diventando , cos , lo standard di cura nei pazienti che presentano valori di emodinamica stabile al momento del ricovero . 
 su queste basi , lintegrazione di embolizzazione percutanea ( sae ) e del nom ha raggiunto un tasso di salvataggio splenico tra 73%96% , come riportato da altre esperienze [ 1321 ]  . 
in particolare , la tc fornisce una detection rapida e af dabile delle lesioni della milza e la valutazione in tempo reale del grado delle lesioni , fornendo al paziente una scelta terapeutica adeguata , vale a dire il nom o sae o la chirurgia . 
 abbiamo , quindi , adottato un algoritmo modi cato con lintento di ridurre inutili interventi chirurgici e decidere pi velocemente il corretto trattamento nei pazienti con traumi addominali che coinvolgono la milza . 
pertanto , sulla base dellesame tc , i pazienti sono stati sottoposti ad embolizzazione in presenza di lesioni spleniche di iv grado o , a prescindere dal grado di lesione , quando cera la presenza di blush vascolare intraparenchimale o uno pseudo - aneurisma post - traumatico . 
 nella nostra esperienza , lalgoritmo ha permesso una rapida decisione sulla possibilit di effettuare lembolizzazione splenica nelle lesioni post - traumatiche : tempo medio dellembolizzazione dal accesso ospedaliero alla procedura stato 171 minuti ( 120300 min )  . 
lembolizzazione dellarteria splenica principale ( embolizzazione prossimale ) stata effettuata in caso di danneggiamento diffuso dellorgano , mentre locclusione delle arterie segmentarie ( embolizzazione distale o selettiva ) in quei pazienti con presenza di una lesione localizzata . 
la riparazione e la vitalit della milza garantita da circoli collaterali derivanti dallarteria grande pancreatica , dalla dorsale del pancreas e dallarterie gastriche brevi , evitando cos lafusso di sangue diretto ed un elevata pressione sanguigna sulla milza danneggiata . 
e controllo angiogra co nale : si osserva vascolarizzazione della milza attraverso vasi collaterali derivanti dallarteria splenica distalmente al sito di occlusione ( freccia )  . treated area is destined to infarction . 
several materials have been proposed for this use : pitressin , autologous clots and , in more recent papers , gel - foam pledgets and metallic coils [ 1222 ]  . 
gel - foam pledgets have a diameter up to 1 , 000 once injected from the catheter , they follow the arterial blood stream and occlude the peripheral vessels , thus stopping the bleeding . 
come contropartita , molti studi segnalano un alto tasso di ri - sanguinamento quando le particelle riassorbibili vengono usate da sole come agente embolizzante [ 17 , 21 ] ; questo si veri cato , nella nostra esperienza , in un solo caso in cui stato embolizzata larteria splenica semplicemente con materiale riassorbibile . 
il paziente , un maschio di 41 anni , ha avuto una lesione splenica di iv grado causata da un incidente dauto che stata trattata con embolizzaradiol med ( 2011 ) 116 : 454465 fig . 
rebleeding may have been due to blood - stream pressure that pushed the gel - foam pledgets located in the main splenic artery distally to the most peripheral vessels , leaving , a large part of the spleen still vascularised . 
questo potrebbe essere dovuto alla pressione sanguigna , che spinge distalmente le particelle riassorbibili , dallarteria principale splenica ai vasi pi periferici , lasciando quindi gran parte della milza ancora vascolarizzata . 
from then on , vessel occlusion was achieved by coil embolization only , which in our opinion , is the technique of choice . an advantage of percutaneous intervention is the possibility of extending the procedure to coexisting lesions [ 17 , 19 ]  . 
among our patients , a 56 - year - old man involved in a car crash was rst embolized for an actively bleeding grade iii splenic lesion and , immediately after , treated for posttraumatic thoracoabdominal aortic dissection by endoprosthesis implantation . 
in our experience , with the exception of one case of post - embolisation re - bleeding , we observed no complications related to the procedure , in agreement with the low morbidity rate described in other reports [ 1215 , 1721 ]  . 
in particular , it was not possible to compare the results of patients who underwent sae with those treated with nom , as these approaches are addressed to substantially different types of splenic injury grade and / or active bleeding . 
additionally , we did not consider the role of contrast - enhanced sonography during admission , monitoring or follow - up , which , according to recent studies [ 27 ] , has proved very effective in identifying and staging abdominal solid - organ injuries . in conclusion , the modi ed algorithm allows rapid direction of patients with blunt abdominal trauma to the most appropriate treatment . 
considering the percutaneous procedure , the mean time from hospital arrival to embolisation was 171 msae can be considered a rapid , effective and safe procedure within the 30 - day period ( our follow - up period after treatment ) and a feasible method of integrating nom . 
more accurate and larger studies are needed to evaluate indications , timing , safety and the role of contrast - enhanced sonography and long - term results of sae . sivamente con spirali che , a nostro avviso , rappresentano il dispositivo di scelta . 
 tra i nostri pazienti , un uomo di 56 anni , coinvolto in un incidente dauto , stato prima embolizzato per una lesione sanguinante della milza di iii grado e , subito dopo , trattato per dissezione post - traumatica dellaorta toraco - addominale mediante impianto endoprotesi . 
nella nostra esperienza , con leccezione di un solo caso di ri - sanguinamento post - embolizzazione , non abbiamo rilevato complicanze connesse alla procedura , in accordo al basso tasso di morbilit descritti in altri studi [ 1215 , 1721 ]  . 
in particolare , non stato possibile confrontare i risultati dei pazienti sottoposti a sae rispetto al nom , dal momento che questi approcci sono rivolti a pazienti sostanzialmente diversi in termini di grado di lesioni spleniche e / o sanguinamento attivo . 
il presente studio si concentrato sui risultati nel periodo peri - procedurale e non abbiamo valutato i pazienti con follow - up a lungo termine per valutare la funzionalit splenica . 
 ulteriore limite del nostro studio di non aver considerato il ruolo dellecogra a con mdc ( ceus ) , che , in base a recenti studi [ 27 ] , si dimostrata molto ef cace nel riconoscimento e nella stadiazione delle lesioni traumatiche degli organi solidi addominali , allammissione , nel monitoraggio e nel follow - up dei pazienti da noi trattati . in conclusione , seguendo il nostro algoritmo modi cato , stato possibile fornire rapidamente il trattamento pi appropriato ai pazienti con traumi addominali . 
lembolizzazione dellarteria splenica pu essere considerata un trattamento rapido , ef cace , sicuro ( secondo i follow - up da noi effettuati nei 30 giorni successivi al trattamento ) ed un metodo pratico per integrare la gestione non operativa . 
selli2 1radiologia diagnostica e interventistica , universit di pisa , pisa , italy 2urologia , universit di pisa , pisa , italy 3scuola superiore santanna , pisa , italy correspondence to : g . 
donatelli , via pesenti 25 , 56124 pisa , italy , tel . : + 39 - 349 - 1581130 , e - mail : graziella_donatelli@hotmail.com received : 23 february 2009 / accepted : 17 september 2009 / published online : 12 february 2011 springer - verlag 2011 abstract purpose . 
the introduction of pharmacological therapy , based on clinical and functional evaluation of the lower urinary tract , is correlated with satisfactory morphofunctional outcomes , reducing moderate - to - severe postvoid residual ( pvr ; p < 0.1 ) and compliance ( p < 0.05 ) at the price of reduced bladder sensation . 
our study con rmed a relationship between detrusor overactivity and hypertonic bladder , bladder diverticula , vesicoureteral re ux , between detrusor underactivity and pvr and between dsd and bladder diverticula . 
questo studio stato condotto con un triplice obiettivo : analizzare i reperti morfo - funzionali vescicos nterici pi frequentemente rilevati con lesame video - urodinamico in pazienti con vescica neurologica secondaria a sclerosi multipla , studiare il ruolo di questo esame nella loro gestione clinica e dimostrare lesistenza di un rapporto di dipendenza tra variabili funzionali e morfologiche . 
lintroduzione della terapia farmacologica basata sulla valutazione clinica e funzionale dellunit vescico - s nterica consente di ottenere risultati morfofunzionali buoni , con il miglioramento del residuo postminzionale ( rpm ) moderato - severo ( p < 0 , 1 ) e della compliance ( p < 0 , 05 ) , a scapito della sensibilit vescicale ( p < 0 , 1 )  . 
la gestione clinica dei pazienti basata anche su valutazioni morfologiche del basso tratto urinario consente di ottenere risultati statisticamente migliori , con la riduzione dei casi di dissinergia detrusore - s ntere esterno ( desd ) e iperattivit detrusoriale con fuga di urina nellesame di controllo . 
i dati ottenuti da questo studio consentono di dimostrare lesistenza di un rapporto di causalit tra iperattivit detrusoriale e ipertono parietale , diverticoli vescicali e re usso vescico - ureterale ( rvu ) , tra ipoattivit detrusoriale e rpm , e tra desd e diverticoli vescicali ; permettono inoltre di avvalorare lutilit dellesame videourodinamico nella valutazione e nel management urologico di questi pazienti . radiol med ( 2011 ) 116 : 432443 keywords videourodynamics neurogenic bladder multiple sclerosis parole chiave video - urodinamica vescica neurologica sclerosi multipla introduction introduzione multiple sclerosis is a demyelinating disease of the central nervous system ( cns ) with multifactorial aetiology , progressive course characterised by periods of remission and relapse and dominated by clinical polymorphism attributed to lesion dissemination in space and time . 
the disease prevalently affects women , with a female - to - male ratio of approximately 3 : 1 , and it appears to be markedly in uenced by environmental factors as well as genetic and immunological factors . 
in fact , different populations have different incidence rates the frequency of the disease rises with increasing distance from the equator , and the relative risk ( rr ) for the individual is linked to the environment in which they spend the rst 15 years of life [ 1 , 4 ]  . 
in 50%90% of patients [ 5 , 6 ] , in different periods of the natural history of the disease but prevalently during the rst 10 years after diagnosis [ 6 , 7 ] , morphofunctional alterations occur to the lower urinary tract . 
 careful management of lower urinary tract dysfunction contributes to improving quality of life in these patients . materials and methods the study was conducted on 75 patients with neurogenic bladder secondary to multiple sclerosis who were observed between july 1998 and may 2008 at the diagnostic and interventional radiology department and the urology department of the santa chiara hospital in pisa . 
the only exclusion criterion applied was the presence of other disease , whether neurogenic or otherwise , that could have been responsible for morphofunctional abnormalities of the lower urinary tract . patients were subdivided into groups on the basis of the number of examinations performed , whether they were undergoing pharmacological treatment at the time of the rst examination or whether treatment was introduced at a later date . 
in this way , ve groups were created : 55 patients la sclerosi multipla una malattia demielinizzante del sistema nervoso centrale ad eziologia multifattoriale , con un decorso progressivo caratterizzato dalla presenza di remissioni e ricadute , dominata da un polimor smo clinico attribuibile al carattere disseminato delle lesioni nello spazio e nel tempo . 
in italia ha una prevalenza di 4070 casi per 100000 individui e unincidenza in costante aumento che nel 1999 ha raggiunto i 4 , 2 casi per 100000 individui [ 3 ]  . 
 infatti popolazioni diverse presentano tassi dincidenza diversi , la frequenza della malattia aumenta con la distanza dallequatore e il rischio relativo assunto dallindividuo relativo allambiente in cui il soggetto trascorre i primi quindici anni di vita [ 1 , 4 ]  . 
nel 50%90% dei pazienti [ 5 , 6 ] , in momenti diversi della storia naturale della malattia ma prevalentemente durante i primi dieci anni dalla diagnosi [ 6 , 7 ] , compaiono alterazioni morfo - funzionali vescico - s nteriche ; esse richiedono uno studio adeguato per poterne de nire le caratteristiche ed intraprendere , se necessario , una terapia appropriata . 
un accurato management delle disfunzioni delle basse vie urinarie contribuisce a migliorare la qualit di vita di tali pazienti . materiali e metodi lo studio stato condotto su 75 pazienti con vescica neurologica secondaria a sclerosi multipla , osservati tra luglio 1998 e maggio 2008 presso lunit operativa ( uo ) di radiologia diagnostica e interventistica e luo di urologia universitaria dellospedale s . 
di essi 47 sono donne , di et compresa fra 39 e 78 anni ( et media 57 anni , = 11 anni ) , e 28 uomini , di et compresa fra 32 e 83 anni ( et media 50 anni , = 11 anni ) ; 21 di essi hanno eseguito due esami video - urodinamici , per un totale di 96 esami valutati . 
lunico criterio di esclusione applicato stato la presenza di altra patologia , neurologica o meno , potenzialmente responsabile di alterazioni morfo - funzionali vescico - s nteriche . i pazienti sono stati suddivisi in pi gruppi in base al numero di esami eseguiti , allassunzione di terapia farmacotable 1 allocation of patients by sex and treatment radiol med ( 2011 ) 116 : 432443 434 men women total patients at rst examination without treatment patients at rst examination with treatment patients who underwent a second examination patients at second examination after introduction of treatment patients second examination after implantation of baclofen pump tabella 1 ripartizione dei pazienti per sesso e percorso terapeutico maschi femmine totale pazienti pazienti al 1 esame senza terapia pazienti al 1 esame con terapia pazienti che hanno eseguito 2 esami pazienti al 2 esame dopo introduzione di terapia pazienti al 2 esame dopo impianto di pompa al baclofene ( 73% ) without treatment at the time of the rst examination ; 20 ( 27% ) undergoing treatment at the time of the rst examination ; 21 ( 28% ) who underwent two examinations in six cases , pharmacological treatment was initiated after the rst examination , and in ve of these ( 83% ) , treatment involved implantation of a baclofen pump ( table 1 )  . videourodynamic study was done in accordance with the international continence society standards [ 8 ]  . 
 flowmetry was judged nonassessable for voided volumes < 50 ml and was not performed in patients with an indwelling catheter or in those who reported an absent bladder sensation at the beginning of the examination . 
videourodynamic study was conducted with a medtronic duet system ; for the cystomanometry and the pressure ow study , 9and 6 - fr double - lumen bladder catheters were used for recording the intravesical pressure , and a 12 - fr rectal balloon catheter was used for measuring abdominal pressure . 
sono stati cos delineati 5 gruppi : 55 pazienti ( 73% ) senza terapia al momento del primo esame ; 20 pazienti ( 27% ) con terapia al primo esame ; 21 pazienti ( 28% ) che hanno eseguito due esami : in 6 casi dopo il primo esame stata introdotta una terapia farmacologica , e in 5 di questi ( 83% ) si trattato dellimpianto di pompa al baclofene ( tabella 1 )  . 
la ussometria risultata non valutabile per volumi minzionali inferiori a 50 ml e non stata eseguita in pazienti portatori di catetere vescicale a permanenza e in coloro che riferivano lassenza di stimolo minzionale allinizio dellesame . 
lesame urodinamico stato eseguito con apparecchio duet medtronic ; per la cistomanometria e lo studio pressioneussso , sono stati utilizzati cateteri vescicali a doppio lume di calibro 9 e 6 fr per la registrazione della pressione endovescicale e cateteri rettali a palloncino del diametro di 12 fr per la misurazione della pressione addominale . 
in particular , one acquisition was obtained at baseline , after urinary owmetry and prior to bladder lling ; two at complete lling with the patient in a lying position , with and without valsalva manoeuvre ; two with the patient in the upright position , with one during the valsalva manoeuvre and one during voiding ; and one after voiding . 
in the case of urine leakage or vesicoureteral re ux ( vur ) , bladder volume and detrusor pressure at the time of the event were recorded with serial morphofunctional acquisitions up to its maximum level of expression . we analysed 18 variables : urgency , frequency , urinary incontinence ( ui ) , recurrent urinary tract infections ( uti ) , urinary retention ( ur ) , bladder sensation , bladder compliance , detrusor overactivity with and without incontinence , detrusor underactivity , acontractile detrusor , vur , hypertonic bladder wall , bladder diverticula , hypertonic bladder neck , hypertonic external urethral sphincter , detrusor sphincter dyssynergy ( dsd ) and postvoid residual ( pvr ) , the latter being subdivided into four subgroups on the basis of volume ( 50150 ml , 151250 ml , 251400 ml , > 400 ml ; pvr < 50 ml was considered nonsigni cant )  . data were analysed with microsoft of ce excel and r 2.5.1. 
i mezzi di contrasto impiegati sono stati visipaque ( iodixanolo , amersham health ; concentrazione di iodio 320 mg / dl ) e ultravist ( iopromide , bayer schering pharma ; concentrazione di iodio 370 mg / dl )  . 
 gli esami sono stati seguiti mediante la registrazione dei tracciati urodinamici e acquisizioni in uoroscopia ottenute periodicamente , in presenza di una sintomatologia riferita dal paziente o alterazioni dei tracciati . 
le immagini acquisite durante gli esami sono quelle ritenute utili dalloperatore a documentare la situazione delle basse vie urinarie ; in particolare sono state fatte una acquisizione in basale , dopo la ussometria e prima del riempimento vescicale ; due a pieno riempimento in clinostatismo , con e senza manovra di valsalva ; due in ortostatismo , di cui una durante manovra di valsalva e una minzionale ; una post - minzionale . 
il riempimento vescicale , le caratteristiche morfologiche delle basse vie urinarie e leventuale fuga di urina iodata durante le contrazioni detrusoriali disinibite o la manovra di valsalva sono state monitorate con la uoroscopia . 
in caso di fuga di urina sono stati registrati il volume di riempimento vescicale e la pressione detrusoriale concomitanti allevento , cos come in presenza di un episodio di re usso vescico - ureterale ( rvu ) , con acquisizione di una documentazione seriale morfo - funzionale no al suo massimo grado di espressione . 
 sono state analizzate 18 variabili : urgenza minzionale ( um ) , frequenza minzionale ( fm ) , incontinenza urinaria ( iu ) , infezioni urinarie ricorrenti ( ivu ) , ritenzione urinaria ( ru ) , sensibilit vescicale , compliance vescicale , iperattivit detrusoriale con e senza fuga di urina ; ipoattivit detrusoriale , acontrattilit detrusoriale , re usso vescicoureterale , ipertono parietale , diverticoli vescicali , ipertono del collo vescicale , ipertono dello s ntere uretrale esterno , dissinergia detrusore - s ntere esterno ( desd ) e residuo post - minzionale ( rpm ) , questultimo suddiviso in quattro sottogruppi in base alla sua entit ( 50150 ml , 151250 ml , 251400 ml , > 400 ml ; lrpm considerato non signi cativo se inferiore a 50 ml )  . i dati sono stati analizzati con microsoft of ce excel 2003 ed r 2.5.1. 
le analisi statistiche sono state condotte utilizzando : il test z per campioni indipendenti nella valutazione delle differenze nelle variabili di interesse tra i pazienti al primo esame video - urodinamico con e senza terapia ( essendo i campioni suf cientemente numerosi , si considerano valide le assunzioni di normalit asintotica degli stimatori ) ; il test di mcnemar per campioni appaiati nel confronto delle variabili di interesse tra campioni appaiati ( in due esami consecutivi , prima e dopo lintroduzione della terapia , prima e dopo limpianto della pompa al baclofene ) ; 436 radiol med ( 2011 ) 116 : 432443 radiol med ( 2011 ) 116 : 432443 438 radiol med ( 2011 ) 116 : 432443 il test chi - quadro nellanalisi della dipendenza tra variabili funzionali e morfologiche . 
 risultati sono state analizzate le frequenze di presentazione delle variabili in studio separatamente nei pazienti che al momento del primo esame video - urodinamico assumevano o meno terapia farmacologica , allo scopo di studiare i reperti pi frequentemente rilevati in questi due gruppi di pazienti e le eventuali differenze tra gli stessi . 
sono invece risultate statisticamente signi cative ( p < 0 , 1 ) le frequenze di presentazione di rpm 251400 ml e normale sensibilit vescicale , pi frequenti nei pazienti non in terapia , e quella delliposensibilit , pi frequente nei pazienti in terapia farmacologica e verosimilmente legata ad essa . 
ancora pi signi cativa la differenza di frequenza della ridotta compliance ( p < 0 , 05 ) , pi rappresentata nei pazienti non in terapia . confrontando i risultati ottenuti nei pazienti studiati prima e dopo lintroduzione della terapia farmacologica ( tabella 2 ) , si evidenzia una signi cativa riduzione della fig . 
statistical signi cance was found ( p < 0.1 ) for pvr 251400 ml and normal bladder sensation , which were more frequent in patients not undergoing treatment ; and reduced bladder sensation , which was more frequent in fig . 
il tracciato cistomanometrico evidenzia repentine uttuazioni della pressione detrusoriale durante la fase di riempimento vescicale , con valori massimi di 78 cmh2o . radiol med ( 2011 ) 116 : 432443 patients undergoing pharmacological treatment and probably linked to it . 
le restanti variabili risultano sostanzialmente stabili in entrambi i casi . confrontando i risultati ottenuti nella valutazione dei pazienti sottoposti a due esami indipendentemente dalle decisioni terapeutiche prese nel frattempo ( tabella 2 ) si osserva una signi cativa riduzione della frequenza di riscontro delliperattivit detrusoriale associata a fuga di urina ( p < 0 , 05 )  . per quanto riguarda lanalisi dei sintomi riferiti dai pazienti al momento dellesame , si nota una frequenza signicativamente minore di urgenza minzionale nei pazienti in terapia al momento del primo esame rispetto a quelli non in terapia , nei pazienti al secondo esame video - urodinamico indipendentemente dal planning terapeutico intrapreso , dopo introduzione di terapia e impianto di pompa al baclofene ( tabella 2 )  . 
allo stesso modo si evidenzia una riduzione dei casi di incontinenza urinaria e infezioni delle vie urinarie dopo introduzione di terapia farmacologica ( tabella 2 )  . come mostrato nella tabella 3 , i dati relativi ai primi esami sostenuti da pazienti non in terapia farmacologica hanno permesso di evidenziare rapporti di dipendenza tra diverse variabili in studio ; in particolare , il rapporto di causa - effetto tra iperattivit detrusoriale e ipertono parietale , diverticoli fig . 
3a , b contrazione detrusoriale disinibita con pressione detrusoriale massima di 44 cmh2o che determina fuga di urina in paziente con diverticoli vescicali . 440 radiol med ( 2011 ) 116 : 432443 vescicali e rvu , tra ipoattivit detrusoriale e rpm , e tra desd e diverticoli vescicali , con vario livello di signi cativit . 
a signi cantly lower frequency of urgency was reported by patients undergoing treatment at the time of the rst examination than by those not undergoing treatment and by patients at the second videourodynamic examination regardless of treatment strategy after the introduction of treatment and implantation of the baclofen pump ( table 2 )  . 
reduction was also observed in patients with ui and uti after the introduction of pharmacological treatment ( table 2 )  . as table 3 shows , data regarding the rst examinations in patients not undergoing pharmacological treatment highlights the dependent relationships between different study variables , particularly the causeeffect relationship between detrusor overactivity and hypertonic bladder wall , between bladder diverticula and vur , between detrusor underactivity and pvr and between dsd and bladder diverticula , with varying levels of signi cance . 
presentation frequency of study variables in patients who at rst videourodynamic examination where not undergoing pharmacological treatment were not in total agreement with data presented in the literature [ 913 ] , which are more heterogeneous . 
 this disagreement could be due to the different degrees of disease severity and different duration of urological symptoms in patients enrolled in the various studies . comparison between patients who at rst videourodynamic evaluation were or were not undergoing pharmacological treatment revealed a more favourable morphofunctional picture in the former group . 
le frequenze di presentazione delle variabili in studio nei pazienti che al momento della prima valutazione video - urodinamica non assumevano terapia farmacologica non sono sempre in accordo con i dati presenti in letteratura [ 913 ] , peraltro non omogenei tra loro ; tale discordanza potrebbe essere imputata al diverso grado di malattia presente nei pazienti reclutati per i vari studi e alla diversa durata dei sintomi urologici negli stessi . 
valutando i risultati ottenuti dal confronto tra pazienti che al momento del primo esame video - urodinamico assumevano o meno terapia farmacologica si evidenzia un quadro morfo - funzionale globalmente migliore per i primi . confrontando i risultati ottenuti nelle analisi con campioni appaiati , in pazienti che al momento del primo esame non assumevano terapia , si evidenzia sempre un miglioramento del quadro morfo - funzionale vescico - s nterico : in particolare la riduzione della frequenza dei casi di desd e di iperattivit detrusoriale associata a fuga di urina al momento del secondo esame . 
sulla base dei risultati riportati in tabella 2 , si pu concludere che il management clinico del paziente con vescica neurologica secondaria a sclerosi multipla integrato dallesame video - urodinamico permette una gestione pi adeguata dellunit vescico - s nterica , consentendo di ottenere miglioramenti morfo - funzionali pi marcati . i pazienti da noi studiati non sono stati strati cati per 442 radiol med ( 2011 ) 116 : 432443 ported in table 2 , we conclude that clinical management combined with videourodynamic examination of the patient with neurogenic bladder secondary to multiple sclerosis improves the management of the lower urinary tract and produces more notable morphofunctional improvements . although the patients we studied were not strati ed according to disease severity or duration of lower urinary tract involvement , the ndings were nonetheless interesting . 
in fact , on the basis of the assumption that the disease can either remain clinically and pathologically stable for a moreor - less lengthy period or worsen but certainly not regress , improvements in one or more functional , morphological or mixed variables can only be the result of the treatment undertaken , whereas stability can also be attributed to remission . 
a more accurate evaluation of this issue requires prospective studies and strati cation of patients according to disease severity and duration of lower urinary tract involvement , with the exclusion of other diseases that could in uence morphology and / or function of the lower urinary tract . 
another limitation of our study was the unavailability of suf cient clinical data ( analytical evaluation of symptoms reported by patients and their correlation with morphofunctional data ) and the lack of adequate diagnostic follow - up of the entire urinary tract . although videourodynamic examination generally includes an emg , which is indicated in patients with neurogenic bladder secondary to multiple sclerosis , this part of the examination was omitted for several reasons : ( a ) the invasiveness of the procedure ( given their greater reliability , needle electrodes tend to be used rather than surface electrodes ) ; ( b ) the need for cooperation of a neurologist both for electrode placement and trace interpretation ( therefore , a larger team is required ) ; ( c ) the nonnegligible frequency of artefacts and risk of electrode displacement during the examination . 
we therefore feel that the experience of operators in the eld of videourodynamics and the correlation of pressure traces with uoroscopic and radiological imaging can compensate for the absence of emg traces . indications for videourodynamic study in patients with neurogenic bladder are still a matter of debate in the absence of guidelines that meet with the consensus of urologists and neurologists [ 14 ]  . 
guidelines of the international consultation on incontinence advise an invasive instrumental approach as a second - line examination after noninvasive clinical and instrumental evaluation and treatment failure [ 2 , 7 , 15 , 16 ] in light of treatment effectiveness in most patients and the low complication rate involving the upper urinary tract ( 0.34% ) [ 7 , 15 , 17 ]  . 
if grado di malattia n per durata dellimpegno delle basse vie urinarie , ma i risultati ottenuti sono ugualmente interessanti ; infatti , partendo dal presupposto che la malattia pu mantenersi clinicamente e anatomo - patologicamente stabile pi o meno a lungo nel tempo o aggravarsi ma certamente non regredire , il miglioramento di una o pi variabili funzionali , morfologiche o miste dovuto unicamente al trattamento instaurato , mentre la loro stabilit pu essere imputabile anche alla fase di remissione della malattia . 
una valutazione pi accurata di questa problematica dovrebbe essere condotta mediante studi prospettici con strati cazione dei pazienti in studio per grado di malattia e durata dellimpegno vescico - s nterico , utilizzando come criterio di esclusione qualunque altra patologia che potrebbe in uenzare la morfologia e / o la funzione delle basse vie urinarie . 
un limite dello studio peraltro rappresentato dalla indisponibilit di suf cienti notizie cliniche ( rilevazione analitica dei sintomi riferiti dai pazienti e della loro correlazione con i dati morfo - funzionali ) e dalla mancanza di un adeguato follow - up diagnostico dellintero apparato escretore urinario . 
 nonostante lesame video - urodinamico includa lesecuzione dellelettromiogra a ed essa sia indicata nei pazienti con vescica neurologica secondaria a sclerosi multipla , questa parte dellesame stata omessa in ragione della sua invasivit ( dovrebbero essere utilizzati elettrodi ad ago anzich a placca perch pi af dabili ) , per la necessit della collaborazione con neurologi sia per il posizionamento degli elettrodi che per linterpretazione dei tracciati ( sarebbe quindi richiesto un team pi numeroso ) , per la frequenza non trascurabile degli artefatti e del rischio di dislocazione degli elettrodi durante lesame . 
riteniamo pertanto che lesperienza degli operatori in campo di video - urodinamica e la correlazione dei tracciati pressori con limaging uoroscopio e radiogra co possano supplire alla mancanza dei tracciati elettromiogra ci . le indicazioni dello studio video - urodinamico nei pazienti con vescica neurologica costituiscono ancora materia di dibattito , in assenza di linee guida che trovino il consenso di urologi e neurologi [ 14 ]  . 
le linee guida dellinternational consultation on incontinence consigliano un approccio strumentale invasivo come indagine di secondo livello dopo una valutazione clinica e strumentale non invasiva e il fallimento della terapia [ 2 , 7 , 15 , 16 ] , in ragione dellef cacia della stessa nella maggior parte dei pazienti e della bassa percentuale di complicanze a carico delle alte vie urinarie ( 0 , 34% ) [ 7 , 15 , 17 ]  . 
eccezioni a questo approccio pratico sono la presenza di un importante rpm o di ivu [ 14 ] , queste ultime spesso indicative di rvu , evidenziabile solo mediante cistogra a minzionale o in corso di iperattivit detrusoriale . 
nel caso in cui si debba ricorrere allo studio radiol med ( 2011 ) 116 : 432443 a more invasive examination is required , the guidelines indicate videourodynamic study as the reference standard [ 6 ]  . invasivo , le linee guida indicano lesame video - urodinamico come il gold standard [ 6 ]  . 
 they support the utility of the morphofunctional evaluation of the lower urinary tract as a second - line study after the noninvasive study of lower urinary tract dysfunction in setting a more complete and adequate clinical management of patients with neurogenic bladder . 
fugazzola 1department of radiology , university of insubria , v.le borri 57 , varese , italy 2department of vascular surgery , university of insubria , v.le borri 57 , varese , italy correspondence to : d . 
fifty - two consecutive patients ( 36 men and 16 women ; mean age 73.6 years ; range 5885 ) with chronic complete sfa occlusion and good distal run - off ( two or three patent vessels ) underwent endovascular recanalisation by direct stenting . 
during the follow - up , 12 reocclusions were observed : eight were treated with mechanical thrombectomy and in - stent angioplasty , and four were converted into femoropopliteal bypasses . 
cinquantadue pazienti consecutivi ( 36 uomini e 16 donne ; et media 76 , 3 anni ; range 5885 ) con occlusione completa dellafs e buon run - off distale ( 2 o 3 vasi pervi ) sono stati sottoposti a ricanalizzazione endovascolare mediante direct stenting . 
il trattamento percutaneo delle occlusioni croniche complete dellafs , nella nostra serie , mostra buoni tassi di perviet primaria e secondaria a breveradiol med ( 2011 ) 116 : 444453 secondary patency rates in the short and medium term , with few periprocedural complications . 
le riocclusioni possono essere trattate con tecnica percutanea , che garantisce un buon tasso di perviet secondaria . keywords super cial femoral artery chronic occlusion percutaneous treatment direct stenting parole chiave arteria femorale super ciale occlusioni croniche trattamento percutaneo direct stenting introduction introduzione treatment of occlusive lesions of the super cial femoral artery ( sfa ) is highly controversial . 
the tasc guidelines generally advise against the use of endovascular angioplasty ( pta ) techniques , sometimes associated with stenting , but they admit that stents may play a limited role in limb salvage in the event of pta failure or complications . 
indications for using stents are therefore restricted to suboptimal results of angioplasty , such as elastic recoil with residual stenosis > 30% , dissection with a ow - limiting ap and failure to maintain initial patency [ 16 ]  . more recently , improvements in techniques and devices have offered new options for percutaneous treatment of sfa occlusions . 
in particular , the use of nitinol stents may provide an effective alternative to surgical revascularisation in patients with severe cardiovascular comorbidities who are not candidates for surgery [ 4 ]  . 
all patients presented with severe claudication ( rutherford stage iii ) , chronic limb ischaemia with pain at rest ( rutherford stage iv ) or ischaemic ulcers ( rutherford stage v )  . 
a fairly good peripheral run - off ( de ned as at least two patent tibioperoneal arteries ) was present il trattamento delle lesioni ostruttive dellarteria femorale super ciale ( afs ) una questione molto controversa . 
le linee guida tasc generalmente scoraggiano luso delle tecniche endovascolari di angioplastica ( pta ) eventualmente associata a stenting , ma ha ammesso che gli stents possono avere un ruolo limitato nel salvataggio darto nei casi di insuccesso o nelle complicanze della pta ; quindi le indicazioni per lutilizzo degli stents sono limitate ai risultati sub - ottimali dellangioplastica come nel caso di ritorno elastico di parete condizionante stenosi residua > 30% , dissezione con ap stenosante o occludente , nonch il mancato mantenimento della perviet iniziale [ 16 ]  . pi recentemente , il miglioramento delle tecniche e dei dispositivi ha fornito nuove opzioni per il trattamento percutaneo delle occlusioni dellafs : in particolare , lutilizzo di stents in nitinol pu rappresentare unef cace alternativa alla rivascolarizzazione chirurgica in pazienti con grave comorbilit cardiovascolare , pertanto non candidati allintervento chirurgico [ 4 ]  . 
1a - f preprocedural angiography : total occlusion of the super cial femoral artery ( sfa ) with recanalisation at the level of the popliteal artery ( a - c )  . 
direct stenting ( d - f ) : posizionamento di stents in nitinol ( edwards lifestent ) con completa ricanalizzazione dellafs . radiol med ( 2011 ) 116 : 444453 fig . 
i - l al termine della procedura si documenta ricanalizzazione completa dellarteria femorale super ciale ( afs ) con perviet delle arterie della triforcazione della gamba . 448 radiol med ( 2011 ) 116 : 444453 in all cases . 
exclusion criteria were acute limb ischaemia , major tissue loss ( rutherford stage vi ) , previous by - pass surgery or sfa stenting , involvement of the iliac arterial axis ( stenoses > 50% or occlusions ) and absolute contraindications to the injection of iodinated contrast material . 
 the contralateral approach was used more frequently to reduce the risk of retroperitoneal haematoma and to avoid compression at the puncture site at the end of the procedure to reduce the risk of acute sfa reocclusion . 
 after a standard transfemoral puncture , a 5f valved introducer sheath ( terumo , tokyo , japan ) was inserted , and the lumen of the contralateral external iliac artery was reached with a 5f hook simmons 1 catheter ( cordis , warren , nj , usa ) and a 0.035hydrophilic guidewire ( terumo , tokyo , japan )  . 
the guidewire was subsequently replaced with a super - stiff guidewire ( amplatz , boston scienti c , natick , ma , usa ) and , after removal of the catheter and introducer sheath , a 45 cm long 6f introducer sheath was inserted ( cordis , warren , nj , usa )  . 
the occlusion was traversed using a stiff , straight or angled hydrophilic guidewire ( glidewire terumo , tokyo , japan ) and with a 4f or 5f straight or vertebral catheter ( cordis , miami , fl , usa )  . in 18 / 52 patients ( 34.6% ) , the occlusion could be easily crossed with the stents , whereas 22 / 52 patients ( 42.3% ) required a catheter with a 2 mm thick and 4 cm long balloon ( cordis , miami , fl , usa )  . 
in the remaining 12 patients ( 23.1% ) , severe atheromatous calci cations did not allow the occlusion to be crossed inside the lumen , so the guidewire and the catheter were advanced through the subintimal space and the lumen was re - entered at the femoro - popliteal junction or above the knee joint at the level of the patent vessel . 
self - expandable nitinol stents 6 or 7 mm in diameter , 10 or 12 cm in length and with a 1 to 2 cm overlap with the next stent were used in 40 cases . 
a total of 152 nitinol stents were employed : 80 luminexx ( bard , nj , usa ) , 48 smart ( cordis , johnson & johnson , miami lakes , fl , iii della classi cazione di rutheford ) , ischemia cronica degli arti con dolore a riposo ( stadio iv della classi cazione di rutheford ) o ulcere ischemiche ( stadio v della classi cazione di rutheford )  . 
i criteri di esclusione sono stati : ischemia acuta degli arti , importanti perdite di tessuto ( stadio vi della classi cazione di rutheford ) , precedente intervento chirurgico di by - pass o stenting dellafs , coinvolgimento dellasse arterioso iliaco ( > 50% stenosi o occlusioni ) ed in ne controindicazioni assolute alliniezione di mezzo di contrasto iodato . 
la ricanalizzazione stato eseguita previa puntura percutanea trans - femorale con approccio retrogrado controlaterale in 44 / 52 casi ( 84 , 6% ) ; nei restanti 8 pazienti ( 15 , 4% ) stato preferito laccesso trans - femorale anterogrado omolaterale . 
abbiamo utilizzato pi di frequente laccesso controlaterale per diminuire il rischio di ematoma retroperitoneale ed evitare , al termine della procedura , la compressione a livello del sito di puntura in modo da ridurre il rischio di riocclusione acuta dellafs . 
dopo puntura trans - femorale comune stato posizionato introduttore valvolato da 5f ( terumo , tokyo , giappone ) e , mediante lutilizzo di catetere tipo hook o simmons1 da 5 f ( cordis , warren , nj , usa ) , stato guadagnato il lume dellarteria iliaca esterna controlaterale con guida idro lica 0 , 035 ( terumo , tokyo , giappone ) ; stata sostituita , quindi , la guida stessa con guida super - stiff ( amplatz , boston scienti c , natick , ma , usa ) e , rimossi il catetere e lintroduttore , con posizionamento di introduttore lungo 45 cm da 6 f ( cordis , warren , nj , usa )  . 
locclusione stata valicata tramite supporto di guida idro lica rigida retta od angolata ( glidewire terumo , tokyo , giappone ) e catetere retto o vertebrale da 4 o 5f ( cordis , miami , fl , usa )  . 
 in 18 / 52 ( 34 , 6% ) pazienti locclusione stata valicata agevolmente dagli stents , in 22 / 52 pazienti ( 42 , 3% ) stato necessario lausilio di un catetere fornito di pallone dilatatore del calibro di 2 mm e della lunghezza di 4 cm ( cordis , miami , fl , usa )  . 
nei restanti 12 casi ( 23 , 1% ) le severe calci cazioni ateromasiche non hanno permesso di valicare locclusione allinterno del lume vasale , quindi stata fatta avanzare guida e catetere in sede subintimale effettuando il rientro al passaggio femoro - popliteo o in sede poplitea sovra - articolare in corrispondenza del vaso pervio . 
 in 40 casi sono stati utilizzati stents autoespandibili in nitinol del calibro di 6 o 7 mm e 10 o 12 cm di lunghezza con overlap di 1 o 2 cm con altro stent . 
la post - dilatazione stata eseguita utilizzando un catetere a palloncino del calibro di 6 mm e lunghezza 10 cm ( cordis , warren , nj , usa )  . 
in the latter eight cases , a genesis balloon - expandable steel stent was used ( cordis , johnson & johnson ) in order to increase precision when delivering it at the femoral bifurcation . all patients received 3 , 000 iu heparin intra - arterially during the procedure and 5 , 000 iu heparin i.v. 
in 250 ml saline solution for 48 h after the procedure , as well as fraxiparine at an anticoagulant dose for 30 days , followed by a double antiaggregant regimen of aspirin ( 100 mg / day ) and clopidogrel ( 75 mg / day ) for 3 months . 
follow - up was performed with clinical evaluation ( classi cation of symptoms and evaluation of peripheral pulses ) and colour doppler ultrasound at 6 , 12 , 18 and 24 months for 36 patients , up to 18 months in four patients and up to 12 months in 12 patients . 
no patient underwent limb amputation in the course of the follow - up . mente sono stati impiegati 152 stents in nitinol : 80 luminexx ( bard , nj , usa ) , 48 smart ( cordis , johnson & johnson , miami lakes , fl , usa ) e 24 edwards lifestent ( edwards lifesciences , irvine , ca , usa )  . 
in questi ultimi ( 8 casi ) stato utilizzato uno stent in acciaio medicale espandibile su pallone genesis ( cordis , johnson & johnson , miami lakes , fl , usa ) per essere molto pi precisi nel rilascio in corrispondenza della biforcazione femorale . durante la procedura , tutti i pazienti hanno ricevuto 3000 ui di eparina per via intra - arteriosa . 
dopo lintervento , tutti i pazienti hanno ricevuto 5000 ui ev di eparina in 250 ml di soluzione siologica per 48 ore , fraxiparina a dose scoagulante per 30 giorni , poi doppio antiaggregante ( aspirina , 100 mg / die e clopidogrel , 75 mg / die per tre mesi )  . 
il followup stato effettuato mediante valutazione clinica ( classi cazione dei sintomi ed esame dei polsi periferici ) ed eco - color doppler a 6 , 12 , 18 e 24 mesi per 36 pazienti , in 4 pazienti no a 18 mesi ed in 12 pazienti no a 12 mesi . 
si sono veri cati 4 casi di embolia distale , trattati mediante trombo - aspirazione con catetere da 6 f lungo 110 cm ( cordis , warren , nj , usa ) in due casi di insuccesso stato lasciato in sede catetere retto da 5 f multiforo ( cordis , johnson & johnson , miami lakes , fl , usa ) per trombolisi loco - regionale intraarteriosa ( uk 500000 ui in 500 ml di soluzione siologica a 60 ml / h ; eparina per via endovenosa 5000 ui in 250 ml di soluzione siologica a 20 ml / h ) per circa 24 ore . nessun paziente stato perso durante il follow - up ( tabella 1 )  . 
la perviet primaria stata del 92 , 3% a 6 mesi ( 4 embolie distali ) e del 76 , 9% a 12 mesi ( 8 occlusioni , trattate con successo con trombectomia meccanica tipo rotarex e angioplastica intra - stent , pertanto , il tasso di perviet secondaria stata del 100% a 6 e 12 mesi )  . 
al follow - up a 24 mesi , il tasso di perviet primaria e secondaria sono risultati non modi cati ( 69 , 2% e 92 , 3% )  . 
several studies have been conducted on the endovascular treatment of sfa occlusions > 10 cm in length ( 16 cm on average ) , and in some cases , only pta was used , achieving a mean primary patency rate of 46% at 12 months [ 79 ]  . 
other studies have reported the results obtained in combination with stenting after angioplasty failure ( secondary stenting ) , with a mean primary patency rate of 55% at 12 months [ 1013 ]  . 
 [ 14 ] found that , in femoral axis stenosis , there is no substantial difference between pta and stenting in terms of long - term patency rate , whereas in the treatment of occlusions especially long ones stenting is superior to angioplasty in term of patency outcomes . the use of stents in the femoro - popliteal region has lowered the rate of early restenoses ( due to elastic recoil , residual stenosis and ow - limiting ap ) , allowing long , complex lesions to be treated even in calci ed arteries [ 4 ]  . 
 despite these encouraging results , however , indications for stenting remain controversial : in fact , the main limitation is myointimal hyperplasia a cause of in - stent restenosis which typically occurs in long stenoses or occlusions or when multiple stents are deployed [ 15 ]  . 
 intimal hyperplasia occurs more frequently after stenting compared with pta alone and is probably due to the constant pressure of the stent on the arterial wall [ 16 ] : ve randomised controlled studies failed to show any bene cial effect of sfa stenting with steel stents compared with pta [ 1721 ]  . 
diversi studi riguardano il trattamento endovascolare delle occlusioni dellafs > 10 cm di lunghezza ( in media 16 cm ) : in alcuni casi stato utilizzata solo la pta , con un tasso di perviet primaria del 46% in media a 12 mesi [ 79 ]  . 
altri studi riportano i risultati ottenuti in associazione allo stenting dopo il fallimento dellangioplastica ( secondary stenting ) con un tasso di perviet primaria del 55% in media a 12 mesi [ 1013 ]  . 
 [ 14 ] ha documentato che , nella patologia stenotica dellasse femorale , non esiste differenza sostanziale tra pta e stent riguardo al tasso di perviet a distanza , mentre nel trattamento delle occlusioni specie lunghe i risultati dello stenting in termini di perviet sono superiori a quelli dellangioplastica [ 14 ]  . limpiego degli stents nel distretto femoro - popliteo ha ridotto la percentuale di restenosi precoci ( dovute al ritorno elastico di parete , a stenosi residua ed a limitazione del usso in caso di ap stenosante ) consentendo il trattamento delle lesioni lunghe e complesse , anche in arterie calci che [ 4 ]  . 
nonostante i risultati incoraggianti , per , le indicazioni alluso degli stents restano incerte : in effetti la principale limitazione rappresentata dalliperplasia miointimale , causa di restenosi intra - stent , che si veri ca in particolare in presenza di stenosi o occlusioni lunghe , o nel caso vengano posizionati pi stents [ 15 ]  . 
liperplasia intimale pi frequente dopo posizionamento di stent rispetto alla sola pta , ed probabile che sia dovuta alla costante pressione dello stent sulla parete arteriosa [ 16 ] : cinque studi randomizzati e controllati non hanno dimostrato un effettivo benecio dello stenting dellafs con stents in acciaio , rispetto alla pta [ 1721 ]  . 
tuttavia , questi studi valutano i risultati radiol med ( 2011 ) 116 : 444453 obtained with the two techniques in patients with short occlusions , in which case excellent results can be obtained with pta alone [ 4 ]  . 
 the recent introduction of nitinol stents appears to have improved the duration of percutaneous treatment in peripheral occlusive arterial diseases of the lower limbs : stent implantation prevents contraction of the elastic bres at the level of the atheromatous plaque , allowing the vessel calibre to remain constant . 
furthermore , thanks to the improvement of stent delivery systems and the smaller calibre of these devices , the most complex lesions , including very long occlusions , can be traversed without predilatation or by using undersized dilatation only if the occlusion cannot be crossed by the stent directly . 
this may reduce the incidence of in - stent restenoses , which are seen on secondary stenting , as well as the risk of embolisation , as reported by mewissen et al . 
in a recent randomised study , the use of nitinol stents proved superior to pta with subsequent stent implantation : at 12 months , restenosis rate was 37% in the rst group ( direct stenting ) and 63% in the second group ( pta ) [ 25 ]  . 
the use of multiple stents in the sfa seems to reduce the number of reocclusions due to the proximal and distal progression of the disease [ 27 , 28 ]  . 
in our experience , it is advisable to use as few stents as possible to cover the length of the occlusion , because their overlapping increases the risk of stent fracture [ 28 ] and consequent thrombotic occlusion . 
in this series , two edwards lifestents ( for each long lesion ) were placed in 12 patients , resulting in regular vascular patency and no complications at 12 months . the main limitation of this study was the small number ottenuti con le due tecniche in pazienti con occlusioni brevi : in questi casi , eccellenti risultati possono essere raggiunti con la sola pta [ 4 ]  . 
 recentemente , tuttavia , lintroduzione di stents in nitinol sembra migliorare la durata del trattamento percutaneo nellarteriopatia obliterante periferica degli arti inferiori : limpianto dello stent previene la contrazione delle bre elastiche in corrispondenza della placca ateromasica per cui il vaso mantiene un calibro costante . 
inoltre , con il miglioramento dei sistemi di rilascio degli stents nonch la riduzione in calibro dei devices , la maggior parte delle lesioni complesse , comprese le occlusioni molto lunghe , pu essere attraversata senza ricorrere alla pre - dilatazione o ricorrere ad una dilatazione sottostimando il vaso solo nei casi in cui non possibile attraversare locclusione direttamente con lo stent . 
la tecnica del direct stenting permette di evitare il trauma della pre - dilatazione ; possibile che questo riduca lincidenza di restenosi intra - stent , osservate con il secondary stenting , riducendo anche la percentuale di rischio embolico , come riportato da mewissen [ 22 , 23 ]  . 
in un recente studio randomizzato , lutilizzo di stents in nitinol ha dato risultati superiori a quelli ottenuti con pta ed impianto successivo di stents : a 12 mesi , i tassi di restenosi erano del 37% nel primo gruppo ( direct stenting ) e del 63% nel secondo gruppo ( pta ) [ 25 ]  . 
 [ 26 ] hanno evidenziato un miglioramento del tasso di perviet primaria a due anni , con limpiego del direct stenting per il trattamento delle occlusioni dellafs confrontato con la pta e secondary stenting ( con tasso di restenosi rispettivamente del 45 , 7% e del 69 , 2% ) , in particolare nei pazienti con ischemia critica degli arti . 
i tassi di perviet primari e secondari sono sostanzialmente sovrapponibili al secondary stenting [ 27 ] con il vantaggio a favore del direct stenting di tempi procedurali pi brevi e di una parziale riduzione delle complicanze emboliche distali peraltro non statisticamente signi cativa ( 7 , 7% vs 9 , 5% )  . 
nella nostra esperienza inoltre meglio utilizzare il minor numero possibile di stents , in relazione alla lunghezza dellocclusione , perch la loro sovrapposizione aumenta il rischio di frattura degli stents [ 28 ] , con conseguente occlusione trombotica degli stessi . 
in questa serie sono stati collocati due edwards lifestents ( per ciascuna lesione lunga ) in 12 pazienti con dimostrazione di regolare perviet vascolare ed assenza di complicanze al follow - up a 12 mesi . la limitazione pi importante relativa a questo studio 452 radiol med ( 2011 ) 116 : 444453 of patients enrolled . 
inoltre , non sono disponibili indagini radiologiche per la valutazione di eventuali fratture di stents , tuttavia , nei pazienti con riocclusioni non si sono evidenziate fratture dei devices impiantati . conclusions conclusioni the optimal treatment of total sfa occlusions is open to debate . 
this said , however , further studies with larger patient populations and longer follow - up periods are needed to validate the method as a primary approach in patients with chronic ischaemia due to total sfa occlusion . il trattamento ottimale delle occlusioni complete dellafs questione di dibattito . 
in questo studio dimostriamo la fattibilit e lef cacia della ricostruzione endoluminale dellafs mediante direct stenting , con un accettabile tasso di complicanze acute e di restenosi a medio - lungo termine . 
policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy 2dipartimento di medicina nucleare e imaging molecolare , irccs neuromed , via atinense 18 , pozzilli , isernia , italy correspondence to : f . 
the objective of this preliminary study was to examine the effects of combined magnetic resonance / positron emission tomography ( mr - pet ) evaluation in the morphofunctional characterisation of ovarian lesions . 
from june 2008 to september 2010 , we evaluated 24 patients ( mean age 4410 years ; range 2474 ) with ovarian lesions incidentally detected on ultrasonography ( us ) and / or multislice computed tomography ( ct )  . 
the added value of this fusion imaging modality lies in combining the benefits of the morphological evaluation provided by mr imaging and the metabolic assessment provided by pet . keywords mr - pet metabolic evaluation postprocessing ovarian lesions ct - pet fusion imaging riassunto obiettivo . 
scopo di questo studio preliminare stato esaminare gli effetti della valutazione combinata risonanza magnetica ( rm ) / tomografia ad emissione di positroni ( pet ) nella caratterizzazione morfo - funzionale delle lesioni ovariche . 
da giugno 2008 a settembre 2010 sono state valutate 24 pazienti ( et media di 4410 anni ; range 2474 anni ) con riscontro casuale di lesione annessiale mediante esame ecotomografico e / o tramite tomografia computerizzata ( tc ) multistrato . 
 radiol med ( 2011 ) 116 : 12881302 1289 parole chiave rm / pet studio metabolico postprocessing lesioni ovariche tc / pet fusione di immagini introduction introduzione ovarian cancer is the second most common gynaecological malignancy and has the highest mortality rate , with a 5 - year survival rate of 46% [ 1 ]  . 
other risk factors are nulliparity , caucasian race , early menarche , late menopause , gonadal dysgenesis and repeated hormone stimulation in patients undergoing artificial insemination , whereas protective factors include multiparity , the use of combined oral contraceptives and prolonged breastfeeding [ 5 ]  . the international federation of gynecology and obstetrics ( figo ) and the tumour node metastasis ( tnm ) classifications of ovarian cancer are based on intraoperative findings that include both cytological and histological assessment [ 6 ]  . transabdominal or transvaginal colour doppler ultrasound ( us ) is , together with the clinical evaluation , the first - line modality for reaching a diagnosis . 
magnetic resonance ( mr ) imaging , thanks to sequences characterised by high spatial and temporal resolution and dynamic contrastenhanced sequences , is a level - two examination for studying the female pelvis that provides a detailed anatomical depiction of the pelvic organs and permits distinction of the liquid , serous or haemorrhagic content of adnexal masses , thus guiding towards a diagnosis of benignity or malignancy . 
however , given the diverse presentations of ovarian cancers , the definite diagnosis is sometimes only established after exploratory laparotomy [ 8 ]  . computed tomography combined with positron emission tomography ( ct - pet ) with [ 18 ] f - fluorodeoxyglucose ( [ 18 ] f - fdg ) may be a valuable tool in assessing ovarian cancers , as it allows metabolic characterisation of lesions based on the increased glucose metabolism observed in tumour cells [ 9 ]  . 
in this context , even if us remains the method of choice for diagnosing ovarian cancer , mr and ct - pet imaging appear to be the two most promising modalities in this area , although with different features and results . 
ct - pet plays a fundamental role in disease staging , monitoring treatment response and identifying residual disease and recurrence , even though it has low sensitivity for identifying the primary lesion [ 10 ]  . 
this il carcinoma ovarico la seconda pi comune neoplasia maligna ginecologica con il pi elevato tasso di mortalit , presentando una sopravvivenza a 5 anni del 46% [ 1 ] ; ci dovuto anche al fatto che al momento della diagnosi circa il 75 % delle pazienti presenta una patologia in fase avanzata [ 2 ]  . 
fattori di rischio sono rappresentati da nulliparit , razza caucasica , menarca precoce , menopausa tardiva , disgenesia gonadica e ripetute stimolazioni ormonali in pazienti sottoposte a fecondazione assistita , mentre fattori protettivi risultano essere la pluriparit , lutilizzo di anticoncezionali estro - progestinici ed un prolungato periodo di allattamento al seno [ 5 ]  . 
 la classificazione del tumore ovarico da parte della federazione internazionale dei ginecologi e ostetrici ( figo ) e la classificazione tumore - noduli - metastasi ( tnm ) sono basate su reperti intra - operatori che includono sia la valutazione citologica che quella istologica [ 6 ]  . 
la risonanza magnetica ( rm ) , grazie allutilizzo di sequenze ad alta risoluzione spaziale e temporale , alluso di sequenze dinamiche dopo somministrazione di mezzo di contrasto , unindagine di seconda istanza valida nello studio della pelvi femminile , in quanto consente una dettagliata rappresentazione anatomica degli organi dello scavo pelvico e permette di distinguere il contenuto delle masse annessiali determinandone la natura liquida , sierosa o emorragica , indirizzando verso una diagnosi di benignit o di malignit . 
lo sviluppo di tecniche pi recenti ( rm spettroscopia e imaging di diffusione ) pu favorire la caratterizzazione corretta delle lesioni [ 7 ] tuttavia , a causa della eterogeneit di presentazione delle neoplasie ovariche , a volte si perviene alla diagnosi definitiva solo con la laparotomia esplorativa [ 8 ]  . 
 la tomografia computerizzata ( tc ) / tomografia ad emissione di positroni ( pet ) con 18f - fluoro - desossi - glucosio ( 18f - fdg ) pu fornire un valido contributo nella valutazione delle neoplasie ovariche , con la caratterizzazione metabolica delle lesioni in virt dellincremento del metabolismo glucidico nelle cellule tumorali [ 9 ]  . 
considerato quanto sopra detto , se lultrasonografia rimane la metodica di base nella diagnosi delle neoplasie ovariche , la rm e la tc / pet sembrano essere le due pi promettenti metodiche in tale ambito , sebbene con caratteristiche e risultati dif1290 radiol med ( 2011 ) 116 : 12881302 latter role could be played by mr imaging [ 8 ]  . to define malignancy of an adnexal lesion on mr imaging , published studies indicate a series of major criteria ( diameter > 4 cm , solid or predominantly solid lesion , intralesional necrosis , wall thickness > 3 mm , presence of internal vegetation or nodules , septations > 3 mm thick , necrosis ) , and minor criteria ( infiltration of other anatomical structures , presence of ascites , peritoneal involvement and satellite lymphadenopathies ) [ 11 , 12 ]  . the recent development of software that fuses data obtained with mr with the metabolic information provided by pet may have a positive effect on the diagnosis of adnexal lesions , facilitating appropriate surgical and therapeutic planning . 
the purpose of our study was to evaluate the diagnostic accuracy of mr , ct - pet and mr - pet fusion imaging in diagnosing ovarian lesions and the differential diagnosis between benign and malignant lesions . 
 materials and methods from june 2008 to september 2010 , we selected 29 patients ( mean age 4410 years ; range 2474 ) with an adnexal lesion incidentally diagnosed at us and / or multislice ct and no evident clinical symptoms . 
of the 29 selected patients , five were excluded from the study : one with breast cancer and a suspicious serous cystadenoma who underwent neoadjuvant chemotherapy for the breast cancer ; two who could not be studied by ct - pet owing to severe diabetes and two with a diagnosis of benign disease who underwent follow - up imaging . 
the patients finally included in the study underwent blood chemistry analysis with measurement of the specific tumour marker carbohydrate antigen ( ca ) 125 , pelvic mr and ct - pet imaging . 
 magnetic resonance imaging a few minutes before the mr examination , patients received an antispasmodic agent ( buscopan , one vial i.v. , boehringer ingelheim ) to reduce artefacts related to bowel peristalsis . 
 mr imaging was performed using a 3 - t permanent magnet ( achieva , philips medical system , best , the netherlands ) equipped with a slew rate of 150 mt m1 ms and a gradient field strength of 30 mt / m , with multichannel ( 6 channels ) phased - array coil . 
la tc / pet ha un ruolo fondamentale soprattutto nella stadiazione della malattia e nel monitoraggio della risposta alla terapia , ovvero nellindividuare la malattia residua e la presenza di recidive , pur essendo dotata di bassa sensibilit nellindividuazione della lesione primitiva [ 10 ] , ruolo che peraltro potrebbe svolgere la rm [ 8 ]  . 
 in relazione a quanto documentato in letteratura esistono , per definire la malignit di una lesione annessiale in rm , criteri maggiori ( diametro superiore a 4 cm , lesione solida o prevalentemente solida , necrosi intralesionale , spessore della parete maggiore di 3 mm , presenza di vegetazioni o nodularit interne , setti con spessore maggiore di 3 mm , necrosi ) e criteri minori ( infiltrazione di altre strutture anatomiche , presenza di ascite , interessamento peritoneale e linfoadenopatie satelliti ) [ 11 , 12 ]  . il recente sviluppo di un software che consente di fondere i dati ottenuti con la rm e le informazioni metaboliche della pet pu sortire un effetto positivo nella diagnosi delle lesioni annessiali , favorendo un appropriato planning chirurgico - terapeutico . 
scopo del nostro studio stato pertanto quello di valutare laccuratezza diagnostica dellimaging mediante rm , tc / pet e fusione rm / pet nella diagnosi delle lesioni ovariche e nella diagnosi differenziale tra formazioni benigne e maligne . 
 materiali e metodi da giugno 2008 a settembre 2010 sono state selezionate 29 pazienti ( et media : 4410 anni ; range 2474 anni ) con diagnosi di lesione annessiale mediante esame ecotomografico e / o tc multistrato di riscontro casuale , in assenza di sintomatologia clinica evidente . 
delle 29 pazienti selezionate , 5 sono state escluse dal nostro studio : una paziente gi affetta da carcinoma mammario con sospetto cistoadenoma sieroso stata sottoposta a chemioterapia neoadiuvante per la neoplasia della mammella ; due pazienti non sono state sottoposte allesame tc / pet per diabete severo e due pazienti con diagnosi di patologia benigna sono state inviate a follow - up strumentale a distanza . 
le pazienti incluse nello studio hanno eseguito esami ematochimici con dosaggio del marker tumorale specifico carbohydrate antigen 125 ( ca125 ) , esame rm della pelvi ed esame tc / pet . 
the dynamic study was performed with axial 3d t1 - weighted fast - field echo ( ffe ) with fat suppression [ t1 - weighted high - resolution isotropic volume examination ( thrive ) ] , with the possibility of obtaining multiplanar reconstructions ( mpr ) , after intravenous administration of a 0.1 mmol / kg bolus of paramagnetic contrast material [ gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa ) , magnevist , schering , berlin , germany ] at a rate of 2 ml / s . mr images were examined by a radiologist experienced in pelvic mr and then compared with the postoperative histological findings . 
the lesions were considered malignant when they showed at least two of the major criteria described above ; they were considered benign when they showed none or only one of these criteria . 
this system provides 47 images with a 3.75 - mm interval covering a 157 - mm axial field of view ( fov )  . patients received a mean dose of 370 mbq of [ 18 ] f - fdg administered i.v. 
the interval between radiotracer administration and ct - pet imaging was approximately 50 m serum glucose levels were < 150 mg / dl ( mean 98 ; range 77124 ) in all cases . 
for image acquisition , a standard ct - pet protocol was used , from the top to the proximal third of the femur with the patient in the supine position . 
lesame rm stato eseguito con magnete permanente 3 , 0 t ( achieva , philips medical system , best , paesi bassi ) dotato di gradienti rapidi a 150 mt m1 / ms e ripidi di 30 mt / m con bobina phased - array multicanale ( 6 canali )  . 
 stata effettuata una valutazione morfologica della pelvi utilizzando le seguenti sequenze : scout ( gradient echo [ ge ] ) , ref scan per lapplicazione dellimaging parallelo , turbo spin echo ( tse ) - t1 sul piano assiale , tse - t2 sui piani assiale e coronale , tse - t2 - spectral attenuated inversion recovery ( spair ) con soppressione selettiva del segnale del tessuto adiposo sul piano assiale . 
lo studio dinamico stato eseguito con sequenze 3d fast field echo ( ffe ) - t1 con soppressione del grasso ( t1 high - resolution isotropic volume excitation , thrive ) sul piano assiale , con possibilit di ricostruzioni multiplanari , dopo somministrazione endovenosa a bolo di mezzo di contrasto paramagnetico gadobenato dimeglumina ( gd - dtpa ) alla velocit di 2 ml / s e con dosi di 0 , 1 mmol / kg ( magnevist , schering , berlin , germania )  . 
le lesioni sono state considerate maligne quando presentavano almeno due dei criteri maggiori di malignit descritti mentre sono state considerate benigne quando non presentavano alcuno o solo uno di tali criteri . 
lacquisizione delle immagini stata effettuata con tomografo ibrido tc / pet discovery 16st ( ge medical system milwakee , wi , usa ) , che combina uno scanner tc a 16 strati con un tomografo pet che consta di 10080 cristalli di bismuto - germanato ( bgo ) disposti su 24 anelli , con workstation dedicata windows advantage 4.4. 
le dimensioni dei cristalli sono di 6 , 36 , 330 mm3 e sono organizzati in blocchi di 66 cristalli , accoppiati con un singolo tubo fotomoltiplicatore con quattro anodi . 
questo sistema permette di ottenere 47 immagini con un intervallo di 3 , 75 mm , coprendo un campo di vista ( fov ) assiale di 157 m la dose media di 18f - fdg somministrata stata 370 mbq per via endovenosa , a digiuno , successivamente seguita da idratazione parenterale con 500 ml di soluzione fisiologica per ridurre la presenza di radiofarmaco nei reni . 
after pet , total - body ct was ( 120140 ma , automatic milliamperage , performed 3.75 - mm slice thickness with 1.25 - mm reconstruction increment , 0.5 - s rotation time , 512512 matrix ) after opacification of the bowel loops with orally administered contrast material and i.v. 
on the pet images , when sites of abnormal radiotracer uptake were identified , regions of interest ( roi ) were drawn to quantify the increased metabolism by calculating the standardised uptake value ( suvmax )  . 
the comparative analysis of images was therefore achieved by using the software advantage mr - pet fusion ( ge medical systems ) , which is available on the systems workstation ( advantage windows 4.4 , ge medical systems ) and allows simultaneous analysis of images after these have been saved in digital imaging and communication in medicine ( dicom ) format . 
in particular , ct ( obtained by coregistration with pet ) and mr images were first aligned by identifying three or more pairs of corresponding landmarks to align the anatomical images . 
subsequently , once the mr examination was sampled and adequately aligned with ct data , unnecessary ct data were discarded and , using the fusion software , were replaced by pet images . 
lacquisizione tc per lattenuazione , stata effettuata a basso dosaggio , con 80 ma e 120140 kv ad uno spessore di 3 , 75 mla correzione per attenuazione delle immagini pet stata ottenuta adattando le hounsfield units ( hu ) della tc al coefficiente lineare di attenuazione per fotoni di 511 kev . 
alla fine dellacquisizione pet si proceduto allesecuzione di un esame tc total body ( 120140 ma , amperaggio automatico , spessore di strato di 3 , 75 mm ricostruibile fino a 1 , 25 mm , tempo di rotazione di 0 , 5 secondi , matrice 512512 ) previa opacizzazione per os delle anse intestinali con mezzo di contrasto orale e somministrazione endovenosa di contrasto organo - iodato eseguendo una acquisizione in fase precoce delladdomepelvi ed unacquisizione pi tardiva del torace - addomepelvi . 
nelle immagini pet , quando documentati siti di uptake anomalo del radiofarmaco , sono state posizionate delle regions of interest ( roi ) per misurare lincremento del dato metabolico con il calcolo dello standardized uptake value massimo ( suvmax )  . 
tale valore la misura parametrica quantitativa massima della radioattivit misurata nel contesto della lesione in relazione alla dose totale di radiofarmaco somministrata e al peso corporeo , ottenuta con la seguente formula [ 13 ] : [ radioattivit ( kbq ) / volume del tessuto ( ml ) ] / [ dose somministrata ( kbq ) / peso corporeo ( gr ) ] il valore suvmax utilizzato come cut - off per distinguere le formazioni benigne dalle lesioni maligne stato 2 , 5 [ 14 ]  . 
 inoltre , sono state considerate come maligne le neoformazioni pelviche dotate di iperfissazione del radiofarmaco associate a linfonodi loco - regionali anchessi dotati di patologico uptake del 18f - fdg . 
 fusione e valutazione delle immagini rm / pet un tomografo che sia in grado di acquisire in coregistrazione e di fondere automaticamente le scansioni pet ed rm non al momento disponibile , pertanto lanalisi comparativa delle immagini stata possibile mediante softwareadvantage mr - pet fusion ( ge medical systems ) disponibile su consolle di ricostruzione , ( advantage windows 4.4 ; ge medical systems ) in grado di analizzare comparativamente le immagini una volta trasferite in digital imaging and communication in medicine ( dicom )  . 
in particolare si proceduto in prima istanza allallineamento delle immagini tc ( ottenute in coregistrazione con la pet ) radiol med ( 2011 ) 116 : 12881302 1293 final mr - pet diagnosis was obtained in consensus between the two physicians . 
sensitivity , specificity , positive ( ppv ) and negative ( npv ) predictive values were measured for ct - pet , mr and mr - pet fusion imaging using histology as the gold standard . 
suvmax values for malignant lesions were high except in patient numbers 7 , 11 , 12 , 16 and 18 , who were considered false negatives on ct - pet . 
successivamente , una volta campionato e allineato adeguatamente lesame rm con i dati tc , sono stati scartati i dati di tomografia computerizzata non pi necessari e , tramite il software di fusione , sono stati sostituiti dalle immagini pet . 
 nellanalisi delle immagini sono stati impegnati un medico nucleare ed un medico radiologo che hanno prima analizzato separatamente i due esami e poi hanno valutato insieme le due metodiche fuse cercando comparativamente alterazioni morfologiche o aree di alterato enhancement allesame rm cui corrispondessero aree di patologico incremento dellattivit metabolica in pet . 
sono stati calcolati i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) dellesame tc / pet , dellesame rm e della fusione delle immagini rm / pet , usando il referto istologico come esame gold standard.i dati del suvmax e del diametro delle lesioni ovariche sono stati confrontati tra i pazienti con lesioni benigne e con lesioni maligne usando il test u di mann - whitney . 
 risultati tutte le pazienti ( n = 24 ) incluse nello studio sono state sottoposte ad intervento chirurgico ( 11 per via laparotomica e 13 per via laparoscopica )  . 
le dimensioni medie delle lesioni maligne sono state di 43 , 629 mm ( range 9140 mm ) , il valore medio di suvmax 42 , 5 ( range 0 , 912 )  . 
 ct - pet detected 14 / 19 malignant lesions ( 74% ) , of which ten were serous cystadenocarcinomas , two were endometrial cystadenocarcinomas and two were mucinous cystadenocarcinomas at histology . 
with regard to the benign masses , ct - pet correctly identified four true negatives ( mean suvmax , 1 ) and one false positive result ( endometriotic cyst ) owing to a high suvmax . 
 mr - pet detected 18 / 19 malignant lesions ( 94% ) , of which 12 were serous cystadenocarcinomas , three were endometrial cystadenocarcinomas and three were mucinous radiol med ( 2011 ) 116 : 12881302 delle lesioni ( p = 0 , 62 ) , mente le lesioni maligne presentavano un suvmax nettamente pi alto rispetto a quello delle formazioni benigne ( p = 0 , 02 )  . tali risultati sono elencati nella tabella 1 per le lesioni maligne , insieme alle dimensioni riscontrate in rm , al valore di captazione semiquantitativo registrato in pet ( suvmax ) e ai risultati dellanalisi integrata rm / pet . 
i valori di suvmax per le lesioni maligne sono risultati elevati ad eccezione delle pazienti 7 , 11 , 12 , 16 e 18 , risultate in tc / pet come falsi negativi . 
per quanto riguarda le formazioni benigne la rm ha presentato 3 veri negativi ( dimensioni medie 28 mm ) e due falsi positivi , in entrambi i casi si trattava di cistoadenoma mucinoso . 
 lo studio tc / pet ha diagnosticato 14 / 19 lesioni maligne ( 74% ) , risultate allesame istologico 10 cistoadenocarcinomi sierosi , 2 cistoadenocarcinomi endometrioidi , 2 cistoadenocarcinoma mucinosi . 
per quanto riguarda le formazioni benigne la tc / pet ha correttamente individuato 4 veri negativi ( suvmax medio 1 ) e un falso positivo ( cisti endometriosica ) , a causa dellelevato suvmax . 
 lo studio rm / pet ha diagnosticato 18 / 19 lesioni maligne ( 94% ) , risultate allesame istologico 12 cistoadenocarcinomi sierosi , 3 cistoadenocarcinomi endometrioidi e 3 cistoadenocarcinomi mucinosi . 
solo un caso ( cistoadenocarcinoma mucinoso ) risultato in rm / pet come falso negativo , perch era negativo alla valutazione pet e presentava dubbie caratteristiche di malignit alla rm . 
 tutte le formazioni risultate allesame istologico come benigne sono state correttamente valutate in rm / pet come veri negativi ( 5 / 5 )  . i valori di sensibilit per rm e tc / pet sono risultati rispettivamente 84% e 74% mentre il valore di sensibilit della rm / pet risultato maggiore ( 94% )  . 
2a - c axial pet image showing pathological uptake of the tracer in the right pelvic region ( a ) , corresponding to an ovarian lesion with mixed fluid and solid component on axial t2 - weighted mr images ( b )  . 
2a - c immagine assiale pet mostra patologica captazione del radiofarmaco in sede pelvica destra ( a ) in corrispondenza di lesione annessiale a componente mista solida e fluida nelle sequenze rm assiali t2 pesate ( b )  . 
listologico ha documentato un cistoadenocarcinoma mucinoso ( paziente 10 in tabella 1 )  . stati rispettivamente del 93% e 44% per la tc / pet , 89% e 50% per la rm e 100% ed 83% per la rm / pet . discussione le pazienti con tumore ovarico vengono spesso sottoposte , in fase di stadiazione , sia ad esame rm della pelvi che ad esame tc / pet . 
considerato questo presupposto interessante valutare se esiste un meccanismo che possa comparare direttamente i rilievi ottenuti con le due metodiche e la sua utilit clinica e diagnostica [ 15 ]  . 
lecografia lesame di prima istanza nella valutazione delle lesioni annessiali , in quanto fornisce informazioni sulla presenza di neoformazioni ovariche , presentando il limite di una non corretta diagnosi differenziale in alcuni casi . 
eventuali alterazioni morfologiche possono inoltre essere valutate anche dopo somministrazione di mezzo di contrasto . per la valutazione morfologica delle lesioni e dellenhancement post - contrastografico fondamentale lesame dei segni diretti e indiretti di neoplasia [ 11 , 12 ]  . 
one case alone ( mucinous cystadenocarcinoma ) proved to be a false negative on mr - pet , as it was negative on pet and showed doubtful signs of malignancy on mr imaging . 
all lesions diagnosed as benign at histology were correctly indicated as true negatives ( 5 / 5 ) on mr - pet . sensitivity values for mr and ct - pet were 84% and 74% , respectively , whereas those of mr - pet were higher ( 94% )  . 
ppv and npv were 93% and 44% for ct - pet , 89% and 50% for mr imaging and 100% and 83% for mr - pet , respectively . discussion during staging , patients with ovarian cancer often undergo both pelvic mr imaging and ct - pet . 
us is the level - one modality for studying adnexal lesions in that it provides information about the presence of ovarian masses , even though with the limitation of an imprecise differential diagnosis in some cases . 
attualmente la rm rappresenta comunque unindagine deccellenza nella diagnosi delle neoplasie ovariche , in quanto ci indirizza ad un adeguato planning terapeutico , risultando utile come metodica problem - solving rispetto al solo esame ecotomografico ed al dosaggio dei markers tumorali [ 16 ]  . 
in addition , any morphological abnormality may also be evaluated after administration of contrast material . in the morphological evaluation of lesions and contrast enhancement , the study of direct and indirect signs of neoplasm is fundamental [ 11 , 12 ]  . 
mr imaging is nonetheless an excellent examination tool in diagnosing ovarian cancer , as it guides towards adequate treatment planning and is a useful problem - solving technique compared with us alone and tumour marker measurement [ 16 ]  . 
 at ct - pet , the increased glucose metabolism of tumour cells is reflected in [ 18 ] f - fdg uptake by neoplastic lesions [ 17 ] where , once in the cytoplasm , it is phosphorylated but , unlike glucose , can no longer represent a substrate for further reactions and remains trapped inside the cell membrane [ 9 ]  . 
for these reasons , and in consideration of its co 18f - fdg allinterno delle lesioni discariocinetiche [ 17 ] ove , una volta trasportato allinterno del citoplasma , viene fosforilato ma , a differenza del glucosio , non pu pi costituire un substrato per ulteriori reazioni e rimane intrappolato allinterno della membrana cellulare [ 9 ]  . 
le applicazioni cliniche dello studio tc / pet nel tumore dellovaio riguardano inoltre non solo la caratterizzazione della lesione primitiva ma anche la stadiazione locoregionale dei linfonodi e la valutazione di metastasi a distanza . 
per queste ragioni e in considerazione dellelevato costo la tc / pet non viene comunemente utilizzata nella diagnosi della lesione primaria , pu tuttavia rappresentare un valido ausilio in pazienti selezionate , in virt del suo elevato potere predittivo positivo . 
la tc / pet risulta inoltre particolarmente utile nella valutazione della recidiva locale e nella diagnosi differenziale tra malattia attiva versus fibrosi ( ad esempio in fase post - attinica ) laddove limaging tradizionale risulta scarsamente dirimente [ 18 ]  . 
questo ruolo appare oggi indiscusso in considerazione della possibilit di sfruttare sia le capacit diagnostiche della tc total body , associata alla somministrazione di mezzi di contrasto orale ed endovenoso , sia il 1298 radiol med ( 2011 ) 116 : 12881302 fig . 
3a - d axial t2 - weighted mr image ( a ) , t2 spectral selection attenuated inversion recovery ( spair ) image ( b ) , t1 - weighted image ( c ) and thrive image after gadolinium administration ( d ) show bulky septated mass in the pelvis . 
3a - d lesame rm con sequenze assiali t2 pesate ( a ) , sequenze assiali t2 spair ( b ) , sequenze assiali t1 pesate ( c ) e sequenze assiali thrive dopo somministrazione di gadolinio ( d ) documenta voluminosa neoformazione in regione annessiale con setti nel contesto . 
listologico ha documentato un cistoadenocarcinoma sieroso ( paziente 3 in tabella 1 )  . high costs , ct - pet is not commonly used for diagnosing the primary lesion ; nonetheless , its high ppv makes it a valuable aid in the study of selected patients . 
furthermore , it has been shown that ct - pet studies can frequently modify the staging obtained with conventional imaging , thus influencing treatment plans and patient prognosis [ 19 ]  . 
 stato inoltre dimostrato che lo studio tc / pet in grado di cambiare frequentemente la stadiazione ottenuta con limaging tradizionale con effetto sullapproccio terapeutico e la prognosi [ 19 ]  . 
in epoca pre - pet il gold standard per stabilire lefficacia di una terapia antiblastica era la valutazione del cambiamento morfologico e dimensionale delle lesioni ; poich tuttavia i cambiamenti metabolici molecolari precedono le variazioni anatomiche , la valutazione quantitativa con suvmax dei diversi valori di captazione del glucosio , prima e dopo trattamento , pu dare una risposta precoce sullefficacia del trattamento iniziato con la possibilit di cambiarlo o correggerlo in itinere [ 18 ]  . 
 altri autori hanno dimostrato una correlazione tra il cambiamento quantitativo della captazione , la risposta clinica e la variazione dei livelli di alcuni markers ( ca125 ) [ 20 ]  . 
 radiol med ( 2011 ) 116 : 12881302 1299 advent of pet imaging , the gold standard for establishing the effectiveness of antineoplastic therapy was the study of morphological and dimensional changes of the lesions ; however , as molecular metabolic changes precede anatomical variations , a quantitative assessment based on suvmax of glucose uptake values before and after treatment may provide an early assessment of treatment effectiveness so that it can be changed or adjusted [ 18 ]  . 
 therefore , in view of the role of mr imaging in diagnosing ovarian lesions , with an accuracy similar to that of postoperative staging [ 21 ] , and the performance of ct - pet in providing a metabolic characterisation of these lesions and evaluating distant metastases , the potential role of combined mr - pet in studying adnexal masses appears clear , even though further studies involving larger patient populations are required . 
with regard to the ppv ( 100% ) and npv ( 83% ) shown by fusion imaging , we can state that a positive result on mr - pet invariably corresponds to a positive histological finding , whereas a negative result cannot rule out a positive histological result , although keeping in mind the limited population in our series . 
 in table 1 , among the histologically proven malignant lesions are two lesions that , due to their small size and predominantly fluid component , were incorrectly considered negative on ct - pet ( patients 7 and 18 ) : in these two cases , the suvmax value was negligible , and the correct diagnosis was obtained with mr imaging , which consequently also affected the mr - pet study . 
pet imaging has limited resolution in diagnosing small neoplasms , having a cutoff of approximately 8 mas a consequence , the difficulty in clinical practice lies in obtaining a metabolic characterisation of lesions < 8 mm that , despite being visible at ct - pet , cannot be studied from a metabolic point of view . 
among benign lesions , ct - pet imaging yielded one false positive result , which turned out to be an endometriconsiderato pertanto il ruolo della rm nella diagnosi delle lesioni ovariche , che presenta accuratezza simile a quella effettiva della stadiazione post - chirurgica [ 21 ] , e in relazione a quanto espresso sulla performance della tc / pet nella caratterizzazione metabolica di tali lesioni e nella valutazione delle metastasi a distanza , appare evidente il ruolo potenziale della valutazione integrata rm / pet nello studio delle neoformazioni annessiali , tuttavia sono necessari ulteriori studi sullargomento su casistiche pi ampie . 
secondo i nostri risultati la rm ha presentato valori di sensibilit superiori a quelli della tc / pet ( 84% rispetto a 74% ) mentre la specificit di questultima metodica si rivelata maggiore ( 80% rispetto a 60% )  . 
si pu affermare che la rm sia pi indicata nella diagnosi delle lesioni maligne e che la tc / pet invece consenta di definire meglio la benignit delle neoformazioni ovariche . 
in relazione al vpp ( 100% ) e al vpn ( 83% ) dimostrati dalla fusione delle due metodiche si pu affermare che lesito positivo della rm / pet sia associato invariabilmente alla positivit del reperto istologico mentre lesito negativo non possa tuttavia escludere la positivit allesame istologico , tenendo presente tuttavia la ridotta popolazione in esame . 
 nella tabella 1 , tra le lesioni maligne allesame istologico , sono presenti due lesioni che , per le loro esigue dimensioni o per la prevalente componente fluida , erano risultate falsamente negative allesame tc / pet ( pazienti 7 e 18 ) : in questi due casi il valore di suvmax documentato era trascurabile e la diagnosi corretta stata ottenuta con la valutazione rm , che di conseguenza ha avuto il suo effetto anche nella valutazione integrata rm / pet . 
il potere di risoluzione della pet nella diagnosi di neoplasie di piccole dimensioni limitato con un cut - off di circa 8 mdi conseguenza la difficolt nella pratica clinica si traduce nel caratterizzare metabolicamente lesioni inferiori a tale diametro che , pur essendo visibili nella tc associata alla pet , non possono essere valutate dal punto di vista metabolico . 
in tal caso ipotizzabile che lelevata captazione del radiofarmaco nel contesto della formazione ( suvmax 3 , 6 ; paziente 1 ; tabella 2 ) potesse esser dovuta allelevato metabolismo espresso dalle cellule infiammatorie [ 22 ]  . in relazione ai falsi negativi della rm tuttavia la caratterizzazione metabolica della tc / pet ha permesso di identificare come maligne due lesioni , identificate come negative radiol med ( 2011 ) 116 : 12881302 1300 fig . 
4a - c axial t2 - weighted mr image ( a ) showing cystic lesion with a wall thickness > 3 mon the axial t2 spair image ( b ) , an internal nodule is evident ( arrow )  . 
4a - c lesame rm con sequenza assiale t2 pesata ( a ) mostra lesione a contenuto fluido con ispessimento della parete maggiore di 3 mm ; nella sequenza t2 assiale spair ( b ) visibile gettone solido ( freccia )  . 
in this case , the strong uptake of contrast material inside the lesion ( suvmax 3.6 ; patient 1 , table 2 ) was probably caused by the accelerated metabolism of inflammatory cells [ 22 ]  . with regard to mr false negative results , the metabolic characterisation of ct - pet allowed detection of two malignant lesions that had strong [ 18 ] f - fdg uptake and that were shown to be two endometrial carcinomas at histology ( patients 8 and 9 ; table 1 )  . 
only combined mr - pet assessment indicated these two cases as true negatives , so it may be stated that the added value of mr - pet was mainly observed in the correct identification of benign masses , with a high specificity ( 100% )  . 
in tc / pet tuttavia risultata falsamente positiva una cisti endometriosica , verosimilmente a causa dellaumentato turn - over cellulare indotto dallinfiammazione : solo la valutazione integrata rm / pet ha permesso di identificare come veri negativi questi ultimi due casi presentati , per cui si pu affermare che il valore aggiunto della rm / pet si osservato in particolare nella identificazione corretta delle formazioni benigne , con specificit elevata ( 100% )  . 
per quanto riguarda i linfonodi il limite della rm rappresentato dal ristretto fov di acquisizione nella valutazione della pelvi , potendo valutare le sole stazioni pelviche e risultando perradiol med ( 2011 ) 116 : 12881302 1301 whole - body ct - pet imaging provided superior longterm staging . 
with regard to lymph nodes , the limitation of mr imaging is its reduced fov , as it can only study the pelvic nodal stations and is thus inferior to ct - pet . 
therefore , ct - pet also plays a key role in studying extrapelvic lymph nodes and evaluating distant metastases , in particular , in lesions > 1 cmr imaging proved to be superior in locoregional staging . 
in consideration of the above , the use of ct - pet is reasonable in all cases with doubtful characterisation on mr and when there is a high suspicion of distant metastases . 
this may also occur on ct - pet , although the time needed for the examination to be reliable is a few weeks only , that is , less than that needed for mr . 
future studies by our department on larger series will ascertain the usefulness of combined pelvic mr fusion imaging and whole - body ct - pet for characterising pelvic masses and in prognostic stratification . 
the major goal is to avoid unnecessary invasive surgical procedures in the case of false positive lesions on mr or ct - pet that turn out to be true negatives on combined mr - pet assessment . 
pertanto la tc / pet ha un ruolo importante anche nello studio delle stazioni linfonodali di drenaggio extra - pelviche e nella valutazione delle localizzazioni a distanza , soprattutto nelle lesioni superiori al centimetro . 
quanto sopra espresso rende ragionevole ricorrere alla tc / pet in tutti quei casi in cui sia dubbia la caratterizzazione delle lesioni in rm e quando il sospetto di metastasi a distanza sia elevato . 
anche in tc / pet la reazione infiammatoria indotta dalla terapia attinica pu creare dei risultati falsamente positivi ; tuttavia il tempo necessario affinch lindagine sia attendibile solo di alcune settimane e comunque inferiore rispetto alla rm . 
futuri studi in programma nel nostro dipartimento su pi ampie casistiche potranno effettivamente chiarire lutilit della valutazione integrata con fusione delle immagini rm della pelvi e tc / pet whole body nella caratterizzazione delle neoformazioni pelviche e nella stratificazione prognostica . 
 in relazione ai nostri risultati la valutazione combinata rm / pet sarebbe auspicabile al fine di implementare i valori di sensibilit e di specificit delle due metodiche in ununica sessione . 
il fine pi importante potrebbe essere quello di evitare interventi chirurgici invasivi non necessari , in riferimento alle lesioni falsamente positive documentate in rm o tc / pet che si sono dimostrate come veri negativi alla valutazione integrata rm / pet . 
cademartiri1 , 2 1department of radiology and cardiology , azienda ospedaliero - universitaria , parma , italy 2department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands 3department of radiology , policlinico g.b. 
giaccone , university of palermo , palermo , italy 5department of radiology , ospedale san gennaro , napoli , italy 6department of radiology , sdn - irccs foundation , napoli , italy correspondence to : f . 
tel. : + 39 - 0521 - 703516 , fax : + 39 - 0521 - 703630 , e - mail : filippocademartiri@gmail.com received : 23 july 2009 / accepted : 24 september 2009 / published online : 4 september 2011 springer - verlag 2011 abstract purpose . 
a total of 722 patients ( 480 men ; 62.710.9 years ) who were referred for further cardiac evaluation underwent cacs and contrast - enhanced ctca to evaluate the presence and severity of cad . 
 patients were stratified according to the morise clinical score ( low , intermediate , high ) , to cacs ( 010 , 11100 , 101400 , 4011 , 000 , > 1 , 000 ) and to ctca ( absence of cad , nonsignificant cad , obstructive cad )  . 
significant cad ( > 50% luminal narrowing ) was detected in 260 ( 36% ) patients ; nonsignificant cad ( < 50% luminal narrowing ) in 250 ( 35% ) and absence of cad in 212 ( 29% )  . 
settecentoventidue pazienti ( 480 maschi ; et media 62 , 710 , 9 anni ) con indicazione ad approfondimento cardiologico sono stati sottoposti a cacs e ct - ca per la valutazione della presenza e severit di cad . 
i pazienti sono stati stratificati secondo lo score di morise ( basso , intermedio , alto ) , secondo il cacs ( 010 , 11100 , 101400 , 4011000 , > 1000 ) e secondo la ct - ca ( assenza di cad , cad non significativa , cad ostruttiva )  . 
cad ostruttiva ( riduzione del lume > 50% ) stata rilevata in 260 ( 36% ) pazienti ; cad non significativa ( riduzione del lume < 50% ) in 250 ( 35% ) e assenza di cad in 212 ( 29% ) pazienti . 
three hard events ( 14% ) occurred in patients with cacs100 and two ( 9.5% ) in patients with intermediate morise score ; one revascularisation was observed in a patient with low morise score . 
cacs 100 and lowintermediate morise score did not exclude the possibility of events at follow - up . keywords computed tomography coronary angiography prognostic value prognosis calcium score morise score nei pazienti con assenza di cad alla ct - ca gli eventi sono stati lo 0% contro l1 , 7% ed il 7 , 3% dei pazienti con cad non ostruttiva e cad ostruttiva , rispettivamente ( p < 0 , 0001 )  . 
due eventi hard ( 9 , 5% , 2 / 21 ) sono stati osservati in pazienti con morise score intermedio ed una rivascolarizzazione in paziente con morise score basso . 
cacs100 ed uno score di morise basso - intermedio non escludono la possibilit di eventi al follow - up . parole chiave angiografia coronarica con tomografia computerizzata valore prognostico prognosi calcium score score di morise introduction introduzione computed tomography coronary angiography ( ctca ) is an emerging technique for the noninvasive evaluation of coronary atherosclerosis in patients with suspected and known coronary artery disease ( cad )  . 
current - generation ct scanners have a high diagnostic accuracy to detect and exclude obstructive cad compared with conventional coronary angiography ( cag ) in selected patients [ 14 ]  . 
however , few data are available on the prognostic value of ctca [ 917 ]  . preliminary reports suggest that ctca has a very high negative predictive value ( npv ) for future cardiovascular events [ 916 ]  . 
the coronary artery calcium score ( cacs ) has also been widely used in north america and asia for stratifying cardiovascular risk in usually asymptomatic patients [ 18 , 19 ]  . very few reports have compared the prognostic value of ctca with other risk stratification strategies [ 1113 , 20 , 21 ]  . 
the aim of this study was therefore to assess the proglangiografia coronarica mediante tomografia computerizzata ( ct - ca ) una metodica diagnostica emergente per la valutazione non invasiva dellaterosclerosi coronarica in pazienti con malattia coronarica ( cad ) sospetta o nota [ 14 ]  . 
lattuale generazione di apparecchiature per la tomografia computerizzata ( tc ) ( 64 strati ) ha una elevata accuratezza diagnostica nella rilevazione della cad ostruttiva se comparata con la coronarografia percutanea ( cag ) in popolazioni selezionate di pazienti [ 14 ]  . 
al contrario , esistono pochi dati sul valore prognostico della ct - ca [ 917 ]  . studi preliminari suggeriscono che la ct - ca abbia un elevato valore predittivo negativo per eventi cardiovascolari [ 916 ]  . 
il calcium score coronarico ( cacs ) stato utilizzato ampiamente in nord america 1190 radiol med ( 2011 ) 116 : 11881202 nostic value of ctca in patients with suspected or known cad and compare it with cacs and a clinical score [ 19 , 22 , 23 ]  . materials and methods patients the study population included 788 consecutive patients ( between april 2006 and december 2007 ) who underwent ctca for suspected or known cad . 
at follow - up , we lost 66 ( 8% ) patients ; therefore , the final study population consisted of 722 patients ( 480 men , 242 women ; mean age 63 11 years )  . 
the following risk factors were considered : ( 1 ) hypertension ( defined as arterial pressure 140 / 80 mmhg or need for antihypertensive therapy ) ; ( 2 ) hypercholesterolemia [ low - density lipoprotein ( ldl ) cholesterol > 130 mg / dl ] ; ( 3 ) diabetes mellitus ; ( 4 ) smoking habit ; ( 5 ) obesity [ body mass index ( bmi ) > 30 ] ; ( 6 ) family history of cardiac disease . 
patients with a history of cad were directly classified with a score > 15 . ctca data acquisition all examinations were performed with a single - source 64 - slice ct system ( somatom sensation 64 cardiac , siemens , forchheim , germany ) [ 24 ]  . 
first , a prospectively ed in asia per la stratificazione del rischio cardiovascolare in pazienti prevalentemente asintomatici [ 18 , 19 ]  . pochi sono gli studi di paragone tra il valore prognostico della ct - ca ed altre strategie di stratificazione del rischio [ 1113 , 20 , 21 ]  . 
lo scopo dello studio quello di valutare il valore prognostico della ct - ca in pazienti con cad sospetta o nota e paragonarlo con il cacs ed uno score clinico [ 19 , 22 , 23 ]  . materiali e metodi pazienti la popolazione studiata consiste di 788 pazienti consecutivi ( periodo aprile 2006 e dicembre 2007 ) sottoposti a ctca per cad sospetta o nota . 
i pazienti sono stati sottoposti a ct - ca a causa di sintomi ( dolore toracico , dispnea ) , test provocativi anormali e / o elevato profilo di rischio cardiovascolare . 
al followup 66 ( 8% ) pazienti sono stati persi , quindi la popolazione finale dello studio consiste di 722 pazienti ( 480 maschi , 242 femmine , et media 6311 anni )  . 
sono stati considerati i seguenti fattori di rischio : ( 1 ) ipertensione ( definita come pressione arteiosa 140 / 80 mmhg o necessit di terapia anti - ipertensiva ) ; ( 2 ) iper - colesterolemia ( colesterolo ldl > 130 mg / dl ) ; ( 3 ) diabete mellito ; ( 4 ) fumo ; ( 5 ) obesit ( indice di massa corporea [ bmi ] > 30 ) ; ( 6 ) familiarit per malattie cardiovascolari . 
 lo score di morise stato calcolato per stratificare il rischio pre - test risk dei pazienti [ 22 , 23 ]  . score di morise lo score di morise [ 23 ] basato sullet , lo stato estrogenico , la storia di angina secondo il metodo di diamond [ 22 ] ed i principali fattori di rischio cardiovascolare ( diabete , dislipidemia , ipertensione , fumo , familiarit )  . 
ad ogni parametro viene assegnato un punteggio ed un punteggio totale pari a 08 rappresenta un rischio basso , un punteggio pari a 915 rappresenta un rischio intermedio , mentre un punteggio > 15 rappresenta un rischio elevato . 
i pazienradiol med ( 2011 ) 116 : 11881202 1191 triggered coronary calcium ct data set was obtained using standard ct parameters comprising 201.2 - mm collimation , 330 ms gantry rotation time , 120 kv tube voltage and 150 mas tube current . 
thereafter , ct coronary angiography was performed after administration of 100 ml nonionic contrast material ( iomeron 400 mgi / ml , bracco , milan , italy ) at a flow rate of 46 ml / s depending on patient status . 
ctca was performed with 640.6 - mm collimation , 330 ms gantry rotation time , 120 kv tube voltage , 900 mas tube current , pitch 0.20 , temporal resolution 165 ms , spatial resolution 0.4mm3 , reconstruction slice thickness 0.75 mm and reconstruction increment 0.5 mintravenously administered beta - blocker ( atenolol 510 mg ) was administered to all patients with a heart rate > 65 bpm and without contraindications ( asthma or bronchospasm , systolic blood pressure < 100 mmhg )  . 
to obtain optimal image quality , data sets were reconstructed at least at two points of the cardiac cycle using a retrospective ecg - gating algorithm ( one diastolic cardiac phase usually at 350 ms from the r waves and one end - systolic phase at + 275 ms ) ; tube current modulation was not used . 
axial data sets were transferred to a remote workstation ( leonardo , siemens medical solutions , forchheim , germany ) for postprocessing and subsequent evaluation . ct data analysis coronary artery calcium score cacs was assessed with dedicated software ( cascore , siemens medical solutions , forchheim , germany )  . 
for multivariate analysis , patients were divided into five groups based on cacs score : group 1 , 010 ; group 2 , 11100 ; group 3 , 101400 ; group 4 , 4011 , 000 ; group 5 , > 1 , 000 . 
 ti con cad nota vengono direttamente classificati con un punteggio > 15 . scansione ct - ca tutte le ct - ca sono state effettuate mediante unapparecchiatura tc a singola sorgente 64 - strati ( somatom sensation 64 cardiac , siemens , forchheim , germania ) [ 24 ]  . 
inizialmente , abbiamo eseguito una scansione con triggering ecg prospettico senza mezzo di contrasto per la quantificazione del calcio coronarico utilizzando parametri standard ( collimazione 201 , 2 mm , tempo di rotazione del gantry 330 ms , 120 kv , corrente del tubo 150 mas )  . 
quindi , abbiamo eseguito la ct - ca dopo la somministrazione endovenosa di 100 ml di mezzo di contrasto non ionico ( iomeron 400 mgi / ml , bracco , milano , italia ) con un flusso di 46 ml / s a seconda delle caratteristiche del paziente . 
la scansione ct - ca stata effettuata con collimazione 64 ( 322 ) 0 , 6 mm , tempo di rotazione del gantry 330 ms , 120 kv , corrente del tubo 900 mas , pitch 0 , 20 , risoluzione temporale 165 ms , e risoluzione spaziale 0 , 4 mm3 , spessore ricostruito degli strati 0 , 75 mm e incremento di ricostruzione 0 , 5 min tutti i pazienti con frequenza cardiaca > 65 bpm ed in assenza di contro - indicazioni ( asma bronchiale o broncospasmo documentati , pressione sistolica < 100 mmhg ) sono stati somministrati beta - bloccanti per via endovenosa ( atenololo 510 mg )  . 
inoltre , in tutti i pazienti senza contro - indicazioni ( stenosi aortica severa , pressione sistolica < 100 mmhg ) sono stati somministrati 0 , 3 mg di nitroglicerina per via sub - linguale [ 25 ]  . 
i dataset sono stati ricostruiti in almeno due punti del ciclo cardiaco utilizzando la tecnica ecg retrospettiva ( una fase diastolica di solito a - 350 msec dallonda r ed una fase sistolica di solito a + 275 msec dallonda r ) al fine di ottenere una migliore qualit di immagine . 
i dataset assiali sono stati trasferiti ad una workstation ( leonardo , siemens medical solutions , forchheim , germania ) per il post - processing e le successive analisi . coronary artery lesion assessment analisi dei dati tc all ctca were evaluated by two experienced observers who were unaware of the patients clinical history . 
patients were finally classified as belonging to one of three groups based on ctca findings : ( 1 ) normal coronary arteries , ( 2 ) nonobstructive cad and ( 3 ) obstructive cad . 
clinical end - points were : ( 1 ) cardiac deathdefined as death caused by acute myocardial infarction , ventricular arrhythmias or refractory heart failure ; ( 2 ) nonfatal myocardial infarction - defined based on criteria of typical chest pain , elevated cardiac enzyme levels and / or typical changes on the ecg ; ( 3 ) unstable angina ; ( 4 ) myocardial revascularisation ( percutaneous coronary intervention / coronary artery bypass grafting )  . survival analysis was performed for total cardiac events [ endpoints 14 ; major adverse cardiac events ( mace ) ] and for clustered endpoints 13 , defined as hard events . 
rca , coronaria destra ; lca , coronaria sinistra ; lm , tronco comune ; cx , coronaria circonflessa ; lad , coronaria discendente anteriore calcio coronarico stato identificato sulle immagini assiali come unarea densa sul tragitto delle arterie coronarie caratterizzata da unattenuazione 130 unit hounsfield ( hu )  . 
per lanalisi multi - variata i pazienti sono stati suddivisi in 5 gruppi a seconda del punteggio cacs : gruppo 1 con cacs 010 , gruppo 2 con cacs 11100 , gruppo 3 con cacs 101400 , gruppo 4 con cacs 4011000 , e gruppo 5 con cacs > 1000 . 
utilizzando i dati precedenti i pazienti sono stati classificati sulla ct - ca in tre gruppi : ( 1 ) pazienti con coronarie normali , ( 2 ) pazienti con cad non ostruttiva , ( 3 ) pazienti con cad ostruttiva . 
gli end - point clinici utilizzati erano : ( 1 ) morte cardiaca , ( 2 ) infarto miocardico non - fatale , ( 3 ) angina instabile , ( 4 ) rivascolarizzazione miocardica ( percutanea / chirurgica , pci / cabg )  . 
lanalisi di sopravvivenza stata effettuata per gli eventi totali ( endpoints 14 ; major adverse cardiac events , mace ) e per gli eventi hard ( endpoints 13 )  . 
 radiol med ( 2011 ) 116 : 11881202 1193 statistical analysis analisi statistica categorical baseline characteristics , expressed as numbers and percentages , were compared using the chi - square test . 
 continuous variables , expressed as mean and standard deviation ( sd ) , were compared using the two - tailed t test and analysis of variance ( anova ) if normally distributed or by means of the chi - square and kruskalwallis method if not normally distributed . 
event curves of the composite endpoint ( cardiac death , nonfatal infarction , angina requiring hospitalisation , myocardial revascularisation ; mace ) and hard events ( cardiac death , nonfatal infarction , unstable angina ) were compared using the log - rank test . 
la variabili continue , espresse come medie e deviazioni standard ( sd ) , sono state confrontate mediante il test t di student a due code e lanalisi della varianza quando caratterizzate da distribuzione normale , e con il test del chi - quadrato e di kruskal - wallis se non normalmente distribuite . 
per la prognosi abbiamo utilizzato un end - point composito caratterizzato da morte cardiaca , infarto miocardico non - fatale , angina instabile , e rivascolarizzazione ( mace )  . 
prevalence of significant cad was 10% ( 43 / 413 ) in the minimal / mild cacs ( 100 ) , 47% ( 48 / 103 ) in the moderate cacs ( 101400 ) and 82% ( 169 / 205 ) in the severe cacs ( > 400 )  . settecento - ventidue pazienti sono stati inclusi nellanalisi finale . 
of risk factors ( meansd ) history of cad , n ( % ) absent present ami revascularisation ami + revascularisation symptoms , n ( % ) asymptomatic typical chest pain atypical chest pain other dyspnoea 62.510.9 480 ( 66 ) 274 6110 bpm 92 ( 12.7 ) 451 ( 62 ) 367 ( 51 ) 256 ( 35 ) 384 ( 53 ) 156 ( 22 ) 2.41.2 511 ( 71 ) 211 ( 29 ) 39 ( 6 ) 68 ( 9 ) 104 ( 14 ) 207 ( 28 ) 143 ( 20 ) 229 ( 32 ) 143 ( 20 ) et ( anni ; mediads ) genere maschile bmi ( kg / m ; mediads ) frequenza cardiaca ( mediads ) fattori di rischio cardiovascolari , n ( % ) 62 , 510 , 9 480 ( 66% ) 274 6110 bpm 92 ( 12 , 7 ) diabete 451 ( 62 ) ipertensione 367 ( 51 ) dislipidemia 256 ( 35 ) fumo 384 ( 53 ) familiarit per cad obesit ( bmi > 30 ) 156 ( 22 ) numero di fattori di rischio ( mediads ) 2 , 41 , 2 storia di cad , n ( % ) assente presente ima rivascolarizzazione ima + rivascolarizzazione simtomi , n ( % ) asintomatici dolore tipico dolore atipico altro dispnea 511 ( 71 ) 211 ( 29 ) 39 ( 6 ) 68 ( 9 ) 104 ( 14 ) 207 ( 28 ) 143 ( 20 ) 229 ( 32 ) 143 ( 20 ) sd , standard deviation ; cad , coronary artery disease ; n , number of patients ; ami , acute myocardial infarction ; bmi , body mass index ds , deviazione standard ; cad , malattia coronarica ; ima , infarto miocardico acuto ; bmi , body mass index ctca stratification a total of 10 , 918 coronary segments were assessed ( 137 ; 1% of nondiagnostic quality )  . 
for the morise score , it is possible to observe that in the two most represented groups ( intermediate and high risk ; 92% of patients ) , ctca can substratify a substantial number of patients without any cad ( 35% in the intermediate risk and 16% in the high risk )  . 
the prevalence of nonobstructive cad remains somewhat stable throughout the three groups , whereas the prevalence of significantly obstructive disease is 3% in the low - risk group , 18% in the intermediate - risk group and 56% in the high - risk group . 
la prevalenza di cad ostruttiva era del 10% ( 43 / 413 ) nei gruppi con cacs100 , del 47% ( 48 / 103 ) nel gruppo con cacs 101400 e del 82% ( 169 / 205 ) nei gruppi con cacs > 400 . stratificazione di malattia secondo la ct - ca sono stati valutati un totale di 10918 segmenti coronarici ( 137 ; 1% di qualit non diagnostica )  . 
riguardo lo score di morise si pu osservare che nei due gruppi pi rappresentati ( rischio intermedio e alto ; corrispondenti al 92% dei pazienti ) , la ct - ca ri - stratifica una consistente quota di pazienti senza alcuna cad ( 35% nel gruppo a rischio intermedio e 16% nel gruppo ad alto rischio )  . 
in particular , the low fraction of patients at low risk using the morise clinical score ( 8% ; a ) compared with cacs ( 40% ; b ) and ctca ( 29% ; c )  . 
in particolare , possiamo osservare la bassa frazione di pazienti a basso rischio del morise score ( 8% ; a ) , a paragone del cacs ( 40% ; b ) e della ct - ca ( 29% ; c )  . 
cad , malattia coronarica ; cacs , calcium score coronarico ; ctca , angiografia coronarica con tomografia computerizzata . 1196 radiol med ( 2011 ) 116 : 11881202 represents 5% in the group with cacs 010 and 85% in the group with cacs > 1 , 000 . 
nonobstructive disease has a prevalence of 22% in the group with cacs 010 and 15% in the group with cacs > 1 , 000 ; however , it represents > 50% of patients in the groups with cacs 11100 and cacs 101400 . 
ami , infarto miocardico acuto ; ua , angina instabile ; ca , arresto cardiaco ; vt , tachicardia ventricolare ; vf , fibrillazione ventricolare ; pci , angioplastica coronarica ; cabg , bypass aortocoronarico . mentre la prevalenza di cad ostruttiva il 3% nel gruppo a basso rischio , del 18% nel gruppo a rischio intermedio e del 56% nel gruppo ad alto rischio . 
la cad non ostruttiva ha una prevalenza del 22% nel gruppo con cacs 010 e del 15% nel gruppo con cacs > 1000 , tuttavia rappresenta > 50% dei pazienti nei gruppi con cacs 11100 e con cacs 101 400 . 
nei pazienti con coro narie normali alla ct - ca la frequenza di mace stata pari 0% versus l1 , 7% nei pazienti con cad non ostruttiva , e il 7 , 3% nei pazienti con cad ostruttiva ( p < 0 , 0001 )  . 
nellanalisi multivariata ( dopo la correzione per i fattori di rischio cardiovascolari ) , il diabete , la cad ostruttiva , ed il cacs > 1000 sono risultati predittori significativi di eventi maggiori ( p < 0 , 05 )  . discussione lo score clinico di morise ha il vantaggio , se confrontato con lo score di rischio di framingham , che richiede pochi parametri , meno dipendente dallet e , cosa pi importante , tiene conto dei sintomi [ 22 , 23 ]  . 
we also observed one revascularisation in the low morise score group ( left panel ) and 26 events ( 24 revascularisations and two hard events ; 9.5% , 2 / 21 ) in the intermediate morise score group ( left and right panels )  . 
abbiamo anche osservato 1 rivascolarizzazione nel gruppo a basso rischio ( pannello di sinistra ) e 26 eventi ( 24 rivascolarizzazioni e 2 eventi hard ; 9 , 5% , 2 / 21 ) nel gruppo a rischio intermedio ( pannelli di sinistra e destra )  . 
we also observed three hard events in the groups with cacs < 100 ( 14% ; 3 / 21 ) : one ami in a patient with cacs 0 ; one ami in a patients with cacs 15 ; one ua in a patient with cacs 56 . 
in particolare , 1 infarto miocardico acuto ( ima ) in un paziente con cacs 0 , 1 ima in un paziente con cacs 15 , ed una angina instabile ( ua ) in un paziente con cacs 56 . 
cardiac event rate pendenti per mace sono la presenza di cad ostruttiva , un cacs > 1000 , ed il diabete . noto da studi precedenti effettuati con cag che la severit della cad un predittore prognostico nei pazienti con malattia ostruttiva . 
in particolare , i pazienti con cad ostruttiva del tronco comune , con cad ostruttiva tri - vasale oppure con cad ostruttiva bi - vasale con un stenosi sulla 1198 radiol med ( 2011 ) 116 : 11881202 survival fig . 
i pazienti con assenza di malattia coronarica ( cad ) alla ct - ca hanno mostrato sopravvivenza priva di eventi al 100% ( sia per gli eventi avversi cardiovascolari maggiori [ mace ] che per gli eventi hard )  . 
multivariate analysis showed that the only independent predictors for mace were the presence of obstructive coronary disease , a cacs > 1 , 000 and diabetes . it is known from previous studies using cag that cad severity is a prognosis predictor in patients with significant cad . 
in particular , patients with significant left main stenosis , three - vessel disease or two - vessel disease with a left anterior descending artery stenosis > 90% are at higher risk of events [ 27 ]  . 
it is known from previous studies using myocardial perfusion scintigraphy or echocardiography stress testing that patients with type - 2 diabetes mellitus have a worse outcome compared with patients without diabetes for any degree of inducible ischaemia [ 28 ]  . 
noto da studi precedenti effettuati con scintigrafia miocardica o ecocardiografia da stress che i pazienti con diabete tipo 2 hanno un outcome peggiore rispetto ai pazienti senza diabete per qualsiasi grado di ischemia inducibile [ 28 ]  . 
i pazienti con infarto miocardico pregresso sono considerati ad alto rischio per la ricorrenza di eventi cardiaci , tuttavia plausibile che il carico aterosclerotico , radiol med ( 2011 ) 116 : 11881202 1199 burden and by a more accelerated progression of the atherosclerotic lesions in diabetics , as observed in an autopsy study [ 29 ]  . 
patients with previous myocardial infarction are considered at high risk for recurrence of a cardiac event ; however , it is plausible that the atherosclerotic burden , which is usually high in these patients , may be the most important prognostic factor . 
in that study , presence , and extent of significant cad defined by a modified duke coronary artery score , were predictors of all - cause mortality [ 10 ]  . 
analysed 517 patients with suspected cad who underwent both myocardial perfusion imaging and ctca and reported an annualised event rate of 4.8% in patients with significant cad at ctca and 1.8% in patients with none or mild cad [ 12 ]  . 
 at 1 year , patients with cad had a 34% event rate , whereas patients with normal coronary arteries had a cardiac event rate of 0% [ 13 ]  . 
in our study , patients without coronary atherosclerosis had an excellent prognosis ( 0% cardiac event rate at 20 months ) , thus confirming the high npv of ctca at follow - up . 
 study limitations the main limitation of our study is that the number of clinical events at follow - up is relatively low due to the population characteristics , which was a population at intermediate cardiovascular risk , and to the relatively limited followup . 
we included patients with both suspected and known cad , as usually encountered in clinical practice ; however , che di solito elevato in questi pazienti , possa essere il pi importante fattore prognostico . 
in questo studio la presenza di cad ostruttiva e lestensione della cad , definite mediante uno score coronarico di duke modificato sono risultati predittori per tutte le cause di mortalit [ 10 ]  . 
 [ 12 ] hanno studiato 517 pazienti con sospetta cad sottoposti a spect e ct - ca ed hanno riportato una frequenza di eventi per anno del 4 , 8% nei pazienti con cad ostruttiva versus l1 , 8% nei pazienti con cad non ostruttiva o senza cad alla ct - ca 1 , 8% . 
ad un anno , i pazienti con cad avevano una frequenza di eventi pari al 34% , mentre i pazienti senza cad avevano una frequenza di eventi pari a allo 0% [ 13 ]  . 
nel nostro studio abbiamo considerato i mace e gli eventi hard anche separatamente , a causa del fatto che la frequenza di rivascolarizzazione durante il follow - up pu essere significativamente condizionata dai risultati della ct - ca . 
 gli studi prognostici sono importanti per determinare se i pazienti , nei quali la ct - ca esclude la presenza di cad ostruttiva , possano essere rassicurati evitando la cag . 
nel nostro studio , i pazienti senza cad ( coronarie normali ) hanno mostrato una prognosi eccellente ( frequenza di eventi a 20 mesi pari allo 0% ) , confermando lelevato valore predittivo negativo della ct - ca anche al follow - up . 
nel nostro studio abbiamo incluso pazienti con cad sospetta o nota , cosa che riflette la pratica clinica , tuttavia la proporzione di pazienti con pregresso infarto miocardico e / o rivascolarizzazione limitata ( 29% )  . 
a causa delle eterogeneit delle popolazione e del numero relativamente basso di eventi , non abbiamo 1200 radiol med ( 2011 ) 116 : 11881202 the proportion of patients with previous acute myocardial infarction or revascularisation was limited ( 29% )  . 
due to the heterogeneous population and the relatively low number of events , we did not perform an association analysis between localisation or characteristics of coronary plaques and event rate . 
nevertheless , at multivariate analysis , cad history was not an independent predictor . high radiation exposure in ctca with retrospective gating is still a matter of concern [ 30 , 31 ]  . 
 recently , a dose modulation algorithm that reduces tube current by 80% during the systolic phase and prospective ecg - triggering protocols were developed that allow significant reduction of radiation exposure up to 34 msv ( or even below ) with preserved diagnostic accuracy [ 3235 ]  . 
 however , so far , the diagnostic accuracy of this new and promising technique is slightly lower compared with coronary angiography and retrospective - gating ct because of motion artefacts and is thus limited to highly selective patient populations . eseguito alcuna analisi per lassociazione tra sede e caratteristiche delle placche aterosclerotiche e la frequenza di eventi . 
tuttavia , nellanalisi multi - variata , la storia di cad non risultato un predittore indipendente . la dose di radiazioni elevata della ct - ca effettuata con tecnica di gating ecg retrospettivo rimane un problema della metodica [ 30 , 31 ]  . 
recentemente sono stati sviluppati protocolli per la modulazione della dose durante la fase sistolica che n consentono una riduzione dell80% e tecniche di triggering prospettico che consentono di effettuare la ct - ca con una dose effettiva di 34 msv ( o meno ) senza condizionare significativamente laccuratezza diagnostica [ 3235 ]  . 
tuttavia , al momento laccuratezza diagnostica ottenuta con queste tecniche leggermente inferiore alla ct - ca con tecnica di gating ecg retrospettivo a causa della limitata capacit di compensazione degli artefatti da movimento e devono essere utilizzate in popolazioni molto selezionate di pazienti . conclusions conclusioni this study shows that ctca reliably identifies coronary atherosclerotic burden and stratifies cardiovascular risk at follow - up in patients with suspected or known cad . 
a morise clinical score with lowintermediate risk and a cacs < 100 or < 10 do not exclude the possibility of future events . il nostro studio dimostra che la ct - ca capace di studiare il carico aterosclerotico coronarico e di stratificare il rischio cardiovascolare al follow - up in pazienti con cad sospetta o nota . 
cademartiri1 , 2 1department of radiology and cardiology , c / o piastra tecnica , piano 0 , azienda ospedaliero - universitaria , via gramsci 14 , 43100 parma , italy 2department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands 3department of radiology and cardiology , ospedale san gennaro , napoli , italy 4department of radiology , universit di messina , messina , italy 5department of radiology , universit di palermo , palermo , italy 6department of radiology , universit di verona , verona , italy 7department of radiology , sdn - irccs foundation , napoli , italy correspondence to : f . 
a total of 183 consecutive asymptomatic individuals ( 92 men ; mean age 5411 years ) with more than one major risk factor ( obesity , hypertension , diabetes , hypercholesterolaemia , family history , smoking ) and an inconclusive or nonfeasible noninvasive stress test result ( stress electrocardiography , stress echocardiography , nuclear stress scintigraphy ) underwent ct - ca in an outpatient setting . 
mean calcium score was 177432 , mean heart rate during the ct - ca scan was 588 bpm and the prevalence ( per - patient ) of obstructive cad was 19% . 
per - patient sensitivity , specificity , positive predictive value and negative predictive value of ct - ca were 100% ( 90100 ) , 98% ( 9699 ) , 97% ( 8599 ) , 100% ( 97100 ) , respectively . 
obiettivo di questo lavoro stato valutare laccuratezza diagnostica dellangiografia coronarica con tomografia computerizzata ( ct - ca ) nellindividuazione delle stenosi coronariche significative ( riduzione del lume coronarico 50% ) confrontata con la coronarografia convenzionale ( cag ) in una popolazione di soggetti asintomatici a rischio intermedio / alto . 
centottantatre soggetti consecutivi asintomatici ( 92 maschi e 91 femmine ; et media 5411 anni ) con pi di un fattore di rischio ( obesit , ipertensione arteriosa , diabete mellito , dislipidemia , familiarit , fumo di sigaretta ) e stress test inconclusivo o non eseguibile ( stress elettrocardiogramma [ ecg ] , stress ecocardiografia , o stress tomografia computerizzata a emissione di fotoni singoli [ spect ] ) sono stati sottoposti a ct - ca . 
il calcium score medio , la frequenza cardiaca media e la prevalenza di malattia per paziente sono risultati 177432 , 588 battiti per minuto ( bpm ) , e 19% , rispettivamente . 
la ct - ca ha mostrato malattia significativa mono - vasale nell9% dei casi , bi - vasale nel 9% dei casi , e tri - vasale in nessun paziente . 
la sensibilit , specificit , valore predittivo positivo della 1162 radiol med ( 2011 ) 116 : 11611173 modality for excluding significant cad in intermediate / high - risk asymptomatic patients with inconclusive or nonfeasible noninvasive stress test . keywords computed tomography coronary angiography conventional coronary angiography asymptomatic primary prevention coronary artery disease ct - ca per paziente sono risultati 100% ( 90%100% ) , 99% ( 96%99% ) , 97% ( 85%99% ) , 100% ( 97%100% ) , rispettivamente . 
la ct - ca un ottimo strumento per lesclusione di malattia coronarica significativa nel asintomatico ad intermedio / alto rischio con stress test in conclusivo o non eseguibile . parole chiave coronarografia con tomografia computerizzata coronarografia convenzionale pazienti asintomatici prevenzione primaria malattia coronarica introduction introduzione computed tomography coronary angiography ( ct - ca ) is a consolidated examination technique for studying the coronary arteries and significant stenoses . 
 the 64 - slice scanner is the current diagnostic standard for ct - ca and is able to explore the entire epicardial coronary tree [ 4 , 5 ]  . 
the main characteristic of ct - ca is its high sensitivity and negative predictive value ( npv ) , enabling exclusion of coronary artery disease ( cad )  . recently , several multicentre trials strengthened data regarding ct - ca and in particular its use in symptomatic patients at intermediate cardiovascular risk [ 69 ]  . 
the population for whom ct - ca is indicated consists of symptomatic patients at intermediate risk after appropriate stratification , including patients with inconclusive or nonfeasible stress test [ stress electrocardiography ( ecg ) , stress echocardiography , stress scintigraphy ] [ 10 ]  . 
 these studies reported good diagnostic performance of ct - ca , even in the presence of low or very low prevalence of significant obstructive disease ( 026% ) [ 1116 ]  . the aim of this study was to evaluate the diagnostic accuracy of ct - ca in asymptomatic patients at intermediate / high cardiovascular risk with inconclusive or nonfeasible stress test compared with conventional coronary angiography ( cag )  . langiografia coronarica con tomografia computerizzata ( ct - ca ) una metodica di indagine consolidata che consente lo studio delle arterie coronarie e delle stenosi significative [ 15 ]  . 
 di recente , alcuni trials multicentrici hanno ulteriormente rafforzato queste informazioni riguardo la ct - ca ed in particolare lutilizzo in pazienti sintomatici a rischio cardiovascolare intermedio [ 69 ]  . 
la popolazione elettiva per la ct - ca consiste dei pazienti sintomatici a rischio intermedio dopo adeguata stratificazione inclusi quelli con test provocativo inconclusivo / non eseguibile ( stress elettrocardiogramma [ ecg ] , ecocardiografia da stress , scintigrafia da stress ) [ 10 ]  . 
in questi studi si evidenzia una buona performance diagnostica della ct - ca anche in presenza di prevalenza di malattia ostruttiva significativa bassa o molto bassa ( 0%26% ) [ 1116 ]  . lo scopo di questo studio valutare laccuratezza diagnostica della ct - ca in pazienti asintomatici a rischio intermedio - alto con test provocativo in conclusivo o non eseguibile confrontata con coronarografia convenzionale ( cag )  . materials and methods patients materiali e metodi over a 36 - month period , 183 consecutive asymptomatic patients [ 92 men , 91 women ; mean agestandard deviation ( sd ) 5411 ] with more than one cardiovascular risk soggetti in un periodo di 36 mesi sono stati arruolati 183 individui radiol med ( 2011 ) 116 : 11611173 1163 factor ( obesity , hypertension , diabetes , dyslipidaemia , family history , smoking ) were enrolled ( table 1 )  . 
i pazienti erano in ritmo sinusale , erano in grado di mantenere una apnea inspiratoria di 12 s e non avevano contro - indicazioni alla somministrazione endovenosa di mezzo di contrasto iodato ( creatinina plasmatica < 120 mg / l , assenza di precedenti reazioni avverse )  . 
lo studio stato approvato da comitato etico ed i pazienti hanno fornito consenso informato . preparazione i pazienti con una frequenza cardiaca allarrivo superiore a 65 battiti per minuto ( bpm ) hanno ricevuto una singola dose endovenosa di atenololo ( 5 mg ) 10 minuti prima dellindagine sotto monitoraggio ecg e pressorio . 
immediatamente prima dellindagine stata somministrata a tutti i pazienti una tavoletta sub - linguale di isosorbide dinitrato ( 0 , 3 mg )  . tutti i pazienti sono stati studiati con ct - ca mediante apparecchiatura a 64 strati ( sensation 64 cardiac , siemens , forchheim , germania )  . 
il calcium score coronarico ( cacs ) stato ottenuto mediante software dedicato ( cascore , siemens , germania ) [ 18 ]  . durante la scansione angiografica stato somministrato per via endovenosa un bolo di 100 ml mezzo di contrasto iodato ( iomeprol , iomeron 400 , bracco , milano , italia ) seguito da 50 ml di soluzione salina attraverso una vena antecubitale del braccio ( velocit 5 ml / s ) e linizio della scansione stata innescata mediante tecnica di bolus tracking [ 19 , 20 ]  . 
 ricostruzione delle immagini le immagini sono state ricostruite con tecnica di gating ecg retrospettivo ( spirale ) con dati provenienti da una singola apnea inspiratoria ed algoritmo di ricostruzione a singolo segmento ( 180 )  . 
i dataset sono stati ricostruiti nelle fasi tele - diastolica ( - 300 / - 450 ms prima della successiva onda r oppure 60% / 70% dellintervallo r - r )  . 
the study was approved by the ethics committee , and all patients provided informed consent . preparation ct protocol patients with a heart rate ( hr ) > 65 bpm received a single intravenous dose of atenolol ( 5 mg ) 10 min prior to the examination under constant ecg and pressure monitoring . 
during the angiography scan , an intravenous bolus of 100 ml of iodinated contrast material ( iomeprol , iomeron 400 , bracco , milan , italy ) followed by 50 ml of saline solution was injected into an antecubital vein at a speed of 5 ml / s , and the scan was triggered automatically with the bolus - tracking technique [ 19 , 20 ]  . image reconstruction images were reconstructed with the ( spiral ) retrospective ecg gating technique , with data being derived from a single breath - hold and with the use of a single - segment reconstruction algorithm ( 180 )  . 
the data sets were reconstructed in the end - diastolic phase ( 300 / 450 ms prior to the subsequent r - wave or 60 / 70% of the r - r interval )  . 
 in the event of inadequate image quality , additional reconstructions were obtained in the end - systolic phase ( + 225 / + 325 ms from the previous r - wave and 25 / 35% of the r - r interval )  . 
le immagini assiali sono state ricostruite con uno spessore individuale di 0 , 75 mm ed un incremento di ricostruzione di 0 , 4 mtutti i dataset sono stati ricostruiti con un filtro di convoluzione intermedio . valutazione immagini tc tutte le scansioni sono state analizzate indipendentemente da due osservatori in consenso e non a conoscenza dei risultati della cag . 
i segmenti sono stati classificati come normali / non significativamente malati ( indenni o con irregolarit del lume o con riduzione del diametro < 50% ) o significativamente malati ( stenosi del lume 50% )  . angiografia coronarica convenzionale la cag stata eseguita entro 4 settimane dalla ct - ca . 
un singolo osservatore , non a conoscenza dei risultati della ct - ca , ha identificato i segmenti coronarici utilizzando la medesima classificazione in 17 segmenti [ 21 ]  . 
i segmenti sono stati classificati come normali ( con pareti e lume regolari ) , non significativamente malati ( con irregolarit del lume o con riduzione del diametro < 50% ) o significativamente malati ( stenosi del lume 50% )  . 
le stenosi coronariche sono state quantificate in due proiezioni ortogonali utilizzando un algoritmo di misurazione validato per langiografia coronarica ( caas , pie medical , maastricht , olanda ) , e classificate come significative se la riduzione del diametro del lume era 50% . 
la performance diagnostica dellangiografia coronarica mediante ct - ca nellindividuazione delle lesioni aterosclerotiche coronariche significative , utilizzando la cag come tecnica di riferimento di seguito riportata come sensibilit , specificit , valore predittivo positivo radiol med ( 2011 ) 116 : 11611173 1165 e negativo con intervalli di confidenza ( ic ) al 95% calcolati con espansione binomiale . 
sono stati calcolati i likelihood ratio positivo e negativo ( lr + e lr - , rispettivamente ) e i valori di probabilit post - test positiva e negativa ( ptp + e ptpcome curve di probabilit condizionale )  . 
 la cag ha dimostrato assenza di malattia significativa in 151 ( 83% ) pazienti e la presenza di almeno una stenosi significativa in 32 ( 19% ) pazienti . individui con stenosi significative e calcio coronarico nella popolazione con almeno una stenosi significativa ( n = 32 ) , un paziente aveva un valore di cacs pari a zero ed il valore medio complessivo era di 697674 ( agatston score )  . 
la dose di radiazioni stimata associate al protocollo stata di calcolata con un software dedicato ( windose , institute of medical physics , erlangen , germania ) ed i valori sono risultati pari a 15 / 21 ( maschi / femmine ) msv . 
la sensibilit , specificit , valore predittivo positive e negative nellanalisi per segmento sono risultati 98% , 97% , 38% , 100% ( lr + 29 ; lr0 , 019 ) , rispettivamente . 
la sensibilit , specificit , valore predittivo positivo e negativo nellanalisi per vaso sono risultati 100% , 95% , 58% , 100% ( lr + 20 ; lr0 , 0 ) , rispettivamente . 
la sensibilit , specificit , valore predittivo positivo e negativo nellanalisi per paziente sono risultati 100% , 99% , 97% , 100% ( lr + 151 ; lr0 , 0 ) , rispettivamente ( tabella 2 )  . 
cdx , coronaria destra ; csx , coronaria sinistra ; tc , tronco comune sinistro ; cx , coronaria circonflessa ; ada , coronaria discendente anteriore . in consensus who were unaware of the cag findings . 
segments were classified as normal / not significantly diseased ( healthy or with lumen irregularities or reduction < 50% ) or significantly diseased ( > 50% lumen reduction )  . conventional coronary angiography cag was performed within 4 weeks of ct - ca . 
the segments were classified as normal ( with regular walls and lumen ) , not significantly diseased ( with lumen irregularities or reduction < 50% ) or significantly diseased ( 50% lumen reduction )  . 
coronary artery stenoses were quantified in two orthogonal views using a measurement algorithm validated for coronary angiography ( caas , pie medical , maastricht , the netherlands ) and classified as significant if lumen reduction was 50% . 1166 statistical analysis data are presented as prevalence , mean and sd . 
the diagnostic performance of ct - ca in identifying significant cad , with cag as the reference standard , is reported in terms of sensitivity , specificity , positive predictive value ( ppv ) and npv , with 95% confidence intervals ( ci ) calculated with binomial expansion . 
the positive ( lr + ) and negative ( lr - ) likelihood ratios were calculated , as were positive and negative posttest probability ( ptp + and ptpas conditional probability curves )  . 
 individuals with significant stenosis and coronary artery calcium in the patient population with at least one significant stenosis ( n = 32 ) , one patient had a cacs value of zero , and the overall mean was 697674 ( agatston score )  . 
estimated radiation dose associated with the protocol was calculated with a dedicated software package ( windose , institute of medical physics , erlangen , germany ) and the values were 15 / 21 ( males / females ) msv . 
a total of 2 , 604 coronary segments were radiol med ( 2011 ) 116 : 11611173 significative , la ct - ca ha correttamente come positivi classificato 53 segmenti . 
i valori di accuratezza diagnostica della ct - ca ( sensibilit 100% e specificit 99% ) in questa popolazione sono risultati al pari o migliori rispetto alle maggiori casistiche riguardanti pazienti sintomatici [ 69 , 2224 ]  . 
 la frequenza di falsi positivi stata dello 0 , 55% ( 1 / 183 ) nellanalisi per paziente , dello 0 , 5% ( 35 / 732 ) nellanalisi per vaso e del 3 , 3% ( 87 / 2604 ) nellanalisi per segmen to . 
tutta via , per qualche motivo questi pazienti erano a rischio intermedio / alto ed avevano effettuato un test provoca tivo oppure non potevano eseguirlo essendo comunque stato indicato dallo specialista . 
il calcio coronarico non sarebbe stato sufficiente ad includere / escludere i pazienti dato che la distribuzione nei pazienti con almeno una stenosi significativa era 13% ( 4 / 32 ) con cacs < 100 , 53% ( 17 / 32 ) con cacs tra 100 e 1000 , e 34% ( 11 / 32 ) con cacs > 1000 ( cacs medio in questo gruppo 668605 , agatston score )  . 
 esistono in letteratura differenti studi che hanno valutato la performance diagnostica della ct - ca in individui radiol med ( 2011 ) 116 : 11611173 1167 1168 radiol med ( 2011 ) 116 : 11611173 cacs in patients with obstructive cad available for evaluation . 
the diagnostic accuracy values of ct - ca ( sensitivity 100% and specificity 99% ) in this population are similar to or better than those in most series regarding symptomatic patients [ 69 , 2224 ]  . the frequency of false positives was 0.55% ( 1 / 183 ) in the per - patient analysis , 0.5% ( 35 / 732 ) in the per - vessel analysis and 3.3% ( 87 / 2 , 604 ) in the per - segment analysis . 
nonetheless , for one reason or another , these patients were at intermediate / high cardiovascular risk and had been referred for a stress test that proved either inconclusive or unfeasible . 
coronary calcium alone would not have been sufficient for including / excluding these patients , given that the distribution in patients with at least one significant stenosis was 13% ( 4 / 32 ) with cacs < 100 , 53% ( 17 / 32 ) with cacs between 100 and 1 , 000 and 34% ( 11 / 32 ) with cacs > 1 , 000 ( mean cacs in this group 668 605 ; agatston score )  . various studies have evaluated the diagnostic performance of ct - ca in intermediate / high cardiovascular risk patients . 
studied the diagnostic accuracy of ct - ca in a cohort of asymptomatic patients at high risk [ 15 ] and reported a disease prevalence of 26% and a sensitivity and specificity of ct - ca of 100% [ 15 ]  . 
tuttavia , una quota non indifferente ( 13% ) di individui aveva un cacs basso ( agatston 1100 ; 10% ) o assente ( agaiston 0 ; 3% )  . 
 in questo studio , senza una validazione con cag , vie ne riportata una prevalenza di malattia ostruttiva del 7% [ 11 ]  . esiste un notevole interesse circa la possibilit di studiare gli individui asintomatici mediante ct - ca . 
la metodica , infatti , consente per la prima volta di valutare non solo la presenza di malattia ostruttiva ma anche il carico di placca coronario in questo gruppo di pazienti [ 26 ]  . 
sensitivity ( sens ) , specificity ( spec ) , positive predictive value ( ppv ) and negative predictive value ( npv ) ( upper panel ) ; positive likelihood ratio ( lr + ; lower left panel ) and negative likelihood ratio ( lr - ; lower right panel ) of the total population that underwent computed tomography coronary angiography ( ct - ca )  . 
il grafico a barre mostra i valori di sensibilit , specificit , valore predittivo positivo e negativo ( pannello superiore ) , e i likelihood ratio ( lr + e lr - ; panelli inferiori ) della popolazione totale sottoposta a ct - ca . 
in that study , done without cag validation , the reported prevalence of obstructive disease was 7% [ 11 ]  . there is significant interest regarding the possibility of using ct - ca to study asymptomatic individuals . 
indeed , for the first time , the modality makes it possible to evaluate not only the presence of obstructive disease but also the coronary plaque burden in this group of patients [ 26 ]  . 
the primary question for which given current knowledge there is no response is : what is the point of evaluating subclinical obstructive atherosclerosis in asymptomatic subjects ? for years , cacs has been used to directly visualise coronary artery atherosclerosis [ 17 ]  . 
la domanda principale , per la quale non esiste allo stato attuale delle conoscenze una risposta , a che cosa serve valutare laterosclerosi sub - clinica ostruttiva o meno nei soggetti asintomatici . 
tuttavia , il rapido e recente sviluppo della tecnologia ct - ca ha portato allattenzione il fatto che la malattia coronaria ostruttiva pu esistere anche in assenza di calcio coronarico [ 25 , 27 ]  . 
 oltre a questo sappiamo dalla letteratura che i test funzionali ( stress ecg , ecocardiografia da stress , stress spect ) non sono in grado di rilevare laterosclerosi sub - clinica e che soffrono di una consistente riduzione dellaccuratezza diagnostica in condizioni di bassa probabilit pretest e / o con individui asintomatici . 
si dimostra come la strategia pi efficace dal punto di vista dei costi sia quella basata sulla ct - ca come primo o secondo esame nella popolazione di 1170 radiol med ( 2011 ) 116 : 11611173 fig . 
ct - ca markedly increases the posttest probability of disease when positive ( light grey line positive test ) and similarly reduces it when negative ( dark grey line negative test ) both in per - patient and per - segment analyses . 
il grafico mostra la relazione tra la probabilit pre - test e post - test di malattia coronarica ostruttiva utilizzando i dati d accuratezza diagnostica ( ct - ca per - patient ; ct - ca per - segment ) e di prevalenza di malattia ( per - patient 19% ; per - vessel 7% ; per - segment 2 , 0% )  . 
la ct - ca aumenta significativamente la probabilit post - test di malattia quando positiva ( linea grigio chiaro ; test positive ) e analogamente la diminuisce quando negativa ( linea grigio scuro ; test negative ) sia nellanalisi per paziente che per segmento . 
shows that the most cost - effective strategy is based on ct - ca as a firstor second - line examination in a patient population with pr - test probability / disease prevalence of 10% [ 22 ]  . 
attualmente la dose di radiazioni media per una ct - ca di circa 12 msv con ampie variazioni legate ai protocolli utilizzati , allesperienza degli operatori , alle apparecchiature [ 28 ]  . 
the mean radiation dose for a ct - ca scan is around 12 msv , with significant variations in relation to the protocols used , operator experience and the system used [ 28 ]  . 
in particular , the implementation of prospective triggering based on the ecg ( instead of spiral retrospective ecg gating ) allows the examination to be performed with a dose of 15 msv depending on the system used [ 2932 ]  . limitations the cad population studied is relatively small , with a relatively low prevalence ( 19% )  . 
radiation dose remains a problem , even though the most recent software and hardware developments suggest the feasibility of ct - ca with doses < 5 msv without significantly compromising accuracy [ 2932 ]  . 
secondly , the ability of ct - ca to accurately evaluate the degree of stenosis is limited , and using a 70% threshold would increase specificity and ppv at the expense of reduced sensitivity and npv . 
la dose di radiazioni rimane un problema della metodica anche se i pi recenti sviluppi tecnologici ( software / hardware ) , suggeriscono la fattibilit della ct - ca con dosi < 5 msv senza significativa compromissione dellaccuratezza diagnostica [ 2932 ]  . 
la discrepanza tra le due metodiche in termini di soglia utilizzata deriva principalmente da due considerazioni : la prima che la ct - ca non una metodica che viene utilizzata per decidere se il paziente deve essere rivascolarizzato a meno ; la seconda che comunque la capacit della ct - ca di valutare accuratamente il grado di stenosi limitata ed utilizzare una soglia del 70% porterebbe ad un aumento della specificit e valore predittivo positivo a prezzo di una riduzione della sensibilit del valore predittivo negativo . 
 inoltre , anche la cag , che costituisce lo standard di riferimento per la quantificazione del grado di stenosi , rimane limitata ed il test provocativo di ischemia associato alla valutazione clinica devono completare comunque la valutazione morfologica . conclusioni conclusions ct - ca has a high diagnostic performance in asymptomatic patients at intermediate / high cardiovascular risk . 
the reservation regarding the use of the technique in this patient population remains the dose of ionising radiation . la ct - ca ha una elevata performance diagnostica nei pazienti asintomatici a rischio intermedio / alto . 
two readers evaluated independently the quality of the dynamic examination ( q : nondiagnostic , diagnostic , optimal ) , condylar motion ( cm : limited , suboptimal , optimal ) , condylar orientation ( co : in - plane , through - plane shift ) , disc visibility and movement ( dv : visible , nonvisible ; dm : normal , reducing , nonreducing dislocation ) and joint effusion ( je : present , absent )  . 
sessantadue pazienti con disfunzione condilo - meniscale ( 124 atm ) sono stati studiati con tecnica rm dinamica dellatm su apparecchio da 1 , 5 t durante movimento fisiologico di apertura e chiusura buccale . 
due lettori hanno valutato indipendentemente la qualit dellesame ( q : non diagnostico , diagnostico , ottimale ) , il movimento condilare ( mc : limitato , subottimale , ottimale ) , lorientamento condilare ( oc : nel piano , fuori dal piano ) , visibilit e movimento del disco ( vd : visibile , non visibile ; m : normale , dislocazione ridotta , dislocazione non ridotta ) e il fluido articolare ( f : presente , assente )  . 
la valutazione qualitativa del movimento condilo - meniscale e della presenza di fluido intraarticolare nellimaging dinamico dellatm solo minimamente dipendente dalla stima dellosservatore , mentre la misurazione del tracciato condilare presenta una variabilit inter - osservatore pari a 30% . parole chiave articolazione temporo - mandibolare variabilit inter - osservatore risonanza magnetica introduction introduzione condyle - disc disorders are the most common abnormalities of the temporomandibular joint ( tmj ) , with an incidence of symptoms of 3572% [ 1 , 2 ]  . 
although disc abnormalities may also be asymptomatic [ 3 ] , patients affected by tmj disorders tend to have more evident signs and symptoms , which may include , in addition to discomfort and articular clicks , joint pain , reduced mandibular movement and limited mouth opening [ 4 , 5 ]  . 
mr study of the tmj is generally performed with a standard protocol [ 14 ] that includes acquisition of static sagittal and coronal images during opening and closing of the mouth . 
 a technical aid to help the patient maintain an openmouth position during mr examination is to use jawopening devices [ 15 , 16 ] that allow acquisition of mr images at maximal mouth opening . 
to verify the condyle disc relationships at the different degrees of mouth opening , the use of an incremental jaw - opening device has been suggested [ 17 ]  . 
moreover , with the use of mechanical jaw le disfunzioni condilo - meniscali sono le pi comuni anomalie dellarticolazione temporo - mandibolare ( atm ) , con incidenza di sintomi stimata del 35%72% [ 1 , 2 ]  . 
 sebbene le alterazioni discali si manifestino anche in soggetti asintomatici [ 3 ] , i pazienti che soffrono di disordini dellatm presentano una sintomatologia pi rilevante , che pu includere oltre a fastidio e rumori articolari ( click ) , anche dolore articolare , ridotta escursione mandibolare e limitata apertura buccale [ 4 , 5 ]  . 
la valutazione radiologica di un sospetto clinico di disfunzione articolare condilo - meniscale si ottiene attraverso limaging di risonanza magnetica ( rm ) [ 6 , 11 , 12 ]  . 
lo studio rm dellatm viene generalmente eseguito con un protocollo standardizzato [ 14 ] che include lacquisizione di immagini sagittali e coronali statiche , in posizione di chiusura ed apertura buccale . 
per verificare i rapporti condilomeniscali a diverse fasi di apertura stato suggerito limradiol med ( 2011 ) 116 : 13031312 1305 openers , it may be difficult to reproduce the optimal mouth opening distance at which the discal dislocation manifests , given that disccondyle incoordination and mouth opening are both prone to wide intersubject variability [ 15 ]  . 
these mr techniques offer additional information on the range of motion , help define the orbit of the disccondyle relationship during repeated movements and allow for evaluation of the dynamic position of the disc and of any disc dislocations [ 15 , 16 ]  . 
to estimate the clinical potential of this technique , it is important to know to what extent the radiologists assessment of dynamic images can affect the variability of the diagnostic result . 
because the reproducibility of the technique has not been investigated , we carried out this study to evaluate interobserver variability in the interpretation of dynamic mr imaging of the tmj . materials and methods patients mr imaging was conducted on 62 symptomatic patients ( 20 men and 42 women ; age range 1266 years ; mean age 33.7 ) selected from a referral centre specialised in the evaluation of disccondyle dysfunction . 
inclusion criteria were a diagnosis of tmj dysfunction based on the presence of articular clicking sound associated with pain , discomfort and / or limited joint motility , with a clinical indication for morphological mr imaging of the tmj . 
con limpiego di distanziatori meccanici pu risultare inoltre indaginoso riprodurre la distanza di apertura buccale ottimale alla quale si manifesta la dislocazione discale , essendo lincoordinazione disco - condilare e la stessa apertura buccale due fenomeni soggetti ad ampia variabilit interindividuale [ 15 ]  . 
queste tecniche rm offrono informazioni aggiuntive sullampiezza del movimento , aiutano a definire lorbita della relazione disco - condilare durante i movimenti ripetuti e consentono una valutazione della posizione dinamica del disco e di sue eventuali dislocazioni [ 15 , 16 ]  . 
al fine di stimare le potenzialit cliniche di questa metodica importante conoscere quanto la valutazione delle immagini dinamiche da parte di un radiologo possa incidere sulla variabilit del risultato diagnostico . 
pertanto , il nostro scopo stato di valutare la variabilit inter - operatore nellinterpretazione dellimaging rm dinamico dellatm . materiali e metodi pazienti sono stati studiati con metodica rm 62 pazienti clinicamente sintomatici ( 20 uomini / 42 donne , range di et 1266 , et media 33 , 7 anni ) selezionati da un centro di riferimento clinico specializzato nella valutazione delle disfunzioni disco - condilari . 
sono stati inclusi nello studio pazienti con diagnosi di disfunzione dellatm basata sulla presenza di rumori articolari associati a dolore , fastidio e / o limitata mobilit articolare , nei quali era stata posta lindicazione clinica ad una valutazione rm morfologica dellatm . 
le 124 atm ( 622 ) includevano 78 casi di incoordinazione ( stadio 1 ) , 22 casi di dislocazione con riduzione ( stadio 2 ) e 24 casi di dislocazione senza riduzione ( stadio 3 ) [ 1921 ]  . risonanza magnetica statica e dinamica dellatm the static images were acquired in the closedand open - mouth positions . 
for the closed - mouth position , lesame delle atm stato effettuato su apparecchi rm da 1 , 5 t ( ge medical system , milwaukee , wi )  . 
i soggetti sono 1306 radiol med ( 2011 ) 116 : 13031312 we acquired ten sagittal images per side ( total 20 ) with a slice thickness of 2 mm , interslice gap 0.3 mm , field of view ( fov ) 12 cm , with fast spin - echo ( fse ) and gradient echo ( gre ) sequences . 
the parameters used for the fse sequence were time to repetition ( tr ) / time to echo ( te ) 4220 / 12 ms and matrix 256224 , whereas those used for the gre sequence were tr / te 600 / 15 ms , flip angle ( fa ) 20 and matrix 256192 . 
 the dynamic study was done with fast imaging steadystate precession ( fisp ) technique in a single sagittal plane localised on the centre of the condyle head identified in the axial plane of the scout image . 
in chiusura buccale sono state acquisite 10 immagini sagittali per ciascun lato ( totale = 20 ) con spessore di immagine di 2 mm , gap tra le immagini di 0 , 3 mm , campo di vista ( fov ) di 12 cm , con tecniche fast spin echo ( fse ) e gradient echo ( gre )  . 
per la sequenza fse sono stati utilizzati i seguenti parametri : tempo di ripetizione ( tr ) / tempo di eco ( te ) 4220 / 12 ms ; matrice 256224 . 
ogni frame ( 130 ) rappresentato nella figura , procedendo da sinistra a destra e dallalto in basso , rappresenta unimmagine acquisita dinamicamente durante il movimento spontaneo di apertura e chiusura buccale ( risoluzione temporale di ogni frame = 0 , 76 s )  . radiol med ( 2011 ) 116 : 13031312 image analysis a preliminary assessment of the quality of the dynamic study was conducted during the examination . 
 using the cine display mode and graphic tools provided with the workstation software , two operators ( fm , lg , with 7 and 2 years of experience , respectively , of mr imaging of the tmj ) independently evaluated quantitative and qualitative parameters . 
the qualitative evaluation took into account diagnostic quality of the examination ( q ) , condylar motion ( cm ) , condylar orientation ( co ) , disc visibility ( dv ) , disc motion ( dm ) and the presence of joint effusion ( je )  . 
cm was evaluated as optimal if the condyle moved beyond the apex of the articular eminence , suboptimal if it aligned with the apex of the articular eminence and limited if it stopped before the articular eminence . 
co was assessed as being in - plane if the condyle remained visible in the scan plane during anterior rotationtranslation and as through - plane shift if the condyle disappeared from the scan plane during movement . 
dm was assessed as normal if no disccondyle alterations were present , reducing if there was a reduction of the anterior dislocation during movement and nonreducing if the anterior dislocation persisted throughout the movement resulting in a discal obstacle . 
this quantitative assessment was made by marking the position of the centre of the condyle in the different frames to trace the curved trajectory covered by the condyle from the mouth - close position to spontaneous maximal opening . 
the condyle pathway in millimetres was measured on each side independently by the two operators . statistical analysis we calculated interobserver variability in the qualitative estimations and quantitative measurements of the condyle path . 
 lo studio dinamico stato effettuato con tecnica fast imaging steady state precession ( fissp ) su singolo piano sagittale , localizzato sul centro della testa del condilo identificata sul piano assiale dello scout . 
nella valutazione qualitativa sono stati considerati : la qualit diagnostica dellesame ( q ) , il movimento condilare ( mc ) , lorientamento condilare ( oc ) , la visibilit del disco ( vd ) , il movimento discale ( md ) , la presenza di fluido intraarticolare ( v )  . 
mc stato valutato secondo le categorie ottimale se il condilo andava oltre lapice delleminenza articolare temporale , subottimale se il condilo si allineava allapice delleminenza articolare , limitato se il condilo si arrestava prima delleminenza articolare . 
oc stato valutato secondo le categorie persistenza nel piano , se durante il movimento rototraslazionale anteriore il condilo era sempre visibile sul piano di scansione , attraversamento nel piano , se il condilo durante il suo movimento dinamico scompariva dal piano di scansione . 
md stato valutato secondo le categorie normale se non erano presenti alterazioni disco - condilari , dislocazione riducibile se si verificava una riduzione della dislocazione anteriore durante il movimento dinamico , dislocazione non riducibile se la dislocazione anteriore persisteva durante tutto il movimento dinamico determinando una condizione di ostacolo meniscale . 
v stato valutato secondo le categorie presente o assente . con gli strumenti grafici del software presenti sulla workstation stato inoltre tracciato il percorso condilare 1308 radiol med ( 2011 ) 116 : 13031312 fig . 
confronto tra un paziente con incoordinazione condilo - meniscale , stadio 1 ( a - e ) ed un paziente con dislocazione discale anteriore non riducibile , stadio 3 ( f - l )  . 
la linea curva che interconnette i punti rappresenta il tracciato condilare misurato in millimetri . percentage differences and the limits of agreement ( la ) , according to the blandaltman method [ 22 , 23 ]  . results the dynamic mr study was completed without difficulty in all patients . 
tale valutazione quantitativa stata effettuata marcando la posizione del centro della testa del condilo nei vari frame in modo da tracciare la distanza curva percorsa dal condilo dalla posizione di chiusura a quella di apertura massimale spontanea . 
il percorso del condilo in mm stato misurato indipendentemente dai due operatori per ogni lato . analisi statistica stata calcolata la variabilit interosservatore nelle stime qualitative e nelle misurazioni del percorso condilare . 
sullasse delle ascisse sono riportate le medie delle misurazioni effettuate dai due operatori ( average ) mentre sulle ordinate riportata la differenza percentualizzata rispetto alla media delle due misurazioni ( difference % )  . 
per misurare la variabilit del percorso condilare stata calcolata la differenza tra le due misurazioni effettuate dai 2 operatori , in percentuale rispetto alla media tra le due misurazioni stesse . 
sono stati quindi calcolati la media tra le differenze percentualizzate e i limiti di concordanza ( lc ) , secondo il metodo di blandaltman [ 22 , 23 ]  . risultati lo studio rm dinamico stato completato senza difficolt in tutti i soggetti . 
la qualit delle immagini , valutata preliminarmente sullapparecchio , risultata sempre soddisfacente da un punto di vista tecnico ( rapporto segnale / rumore , eventuale presenza di artefatti )  . 
il movimento discale stato valutato come normale , dislocazione riducibile e dislocazione non riducibile rispettivamente nel 66 , 1% ( 82 atm ) , 14 , 8% ( 18 atm ) e 19 , 1% ( 24 atm ) ( concordanza buona : = 0 , 64 ; p < 0 , 01 ) ; la presenza di fluido intra - articolare stata giudicata come presente o assente rispettivamente nel 41 , 3% ( 51 atm ) e 58 , 7% ( 73 atm ) ( concordanza buona : = 0 , 67 ; p < 0 , 01 )  . 
lorientamento del condilo stato identificato nel piano o al di fuori del piano di scansione rispettivamente nel 94 , 2% ( 117 atm ) e 5 , 8% ( 7 atm ) ( concordanza moderata : = 0 , 41 ; p < 0 , 01 )  . 
i risultati ottenuti hanno evidenziato una concordanza tra i due operatori elevata nella valutazione della qualit dellesame , del movimento condilare e della visibilit del disco , buona per il movimento discale e per la presenza di fluido intra - articolare , ed una concordanza moderata nella mean of the percentage differences was 1.2% , the lower la was 35% and the upper la was 32.6%. 1310 discussion this study assessed interobserver variability in the evaluation of dynamic mr imaging of the tmj . 
the results obtained by the two operators showed a high level of agreement in evaluating examination quality , condylar motion and disc visibility , a good agreement for disc movement and joint effusion , and moderate agreement in determining condyle orientation . 
in the quantitative evaluation performed on the condylar path , we found a variability of 30% compared with the measurements expressed in millimetres . mr imaging is the reference diagnostic modality for evaluating intracapsular and muscular tmj disorders . 
a serial dynamic acquisition in the same scan plane and with a temporal resolution of 1.25 images per second , during mouth opening and closing may depict in cine mode the movement of condyledisc rotationtranslation . 
 the fisp sequence is particularly suitable for this kind of imaging owing to the high temporal resolution and the good signal - to - noise ration between the bony structures ( hyperintense ) and the discal - ligamentous structures ( hypointense )  . 
moreover , as the movement is voluntary and spontaneous , this type of imaging effectively depicts the condyle - disc relationship and allows the type of discal movement to be defined in a natural and spontaneous manner . the same dynamically acquired images allowed identification of at least two morphological parameters : disc visibility and joint effusion . 
in view of the association existing between increased joint fluid and tmj disorders , a favourable finding was the good level of agreement between the two evaluations of the presence or absence of joint effusion . dynamic evaluation of cine mr acquisitions took into radiol med ( 2011 ) 116 : 13031312 definizione dellorientamento del condilo . 
nella valutazione quantitativa effettuata sul percorso condilare stata misurata una variabilit di 30% rispetto alle misurazioni espresse in millimetri . limaging rm rappresenta la metodica diagnostica di riferimento nella valutazione delle disfunzioni intra - capsulari e muscolari dellatm . 
unacquisizione dinamica , seriata , su uno stesso piano di scansione , con una risoluzione temporale di 1 , 25 immagini per secondo , durante il movimento di apertura e chiusura , pu rappresentare in cine il movimento di rototraslazione condilomeniscale . 
rispetto alle acquisizioni statiche , le immagini visualizzate in modalit cine hanno consentito una valutazione dellintero range di relazione condilo - meniscale , con una qualit diagnostica del 99 , 2% . 
la sequenza fissp , in tal senso , si presta a tale tipo di imaging per lelevata risoluzione temporale ed il buon rapporto segnale - rumore esistente tra le strutture ossee ( iperintense ) e quelle discoligamentose ( ipointense )  . 
il movimento buccale durante lacquisizione dinamica copre tutte le fasi della rototraslazione condilo - meniscale da una condizione di chiusura buccale completa in occlusione fino a quella di unapertura massimale . 
inoltre , essendo il movimento volontario e spontaneo , con questo tipo di tecnica dimaging si rappresenta effettivamente la relazione condilo - meniscale e si definisce il tipo di movimento discale in maniera naturale e spontanea . nelle stesse immagini acquisite in maniera dinamica sono stati identificati almeno due parametri morfologici : la visibilit del disco ed il fluido intra - articolare . 
considerata lassociazione esistente tra laumento del fluido intraarticolare e le disfunzioni dellatm , un dato favorevole stato che nella definizione di presenza o assenza di raccolta fluida articolare la concordanza tra le due valutazioni risultata buona . nella valutazione propriamente dinamica dellacquisizione cine - rm sono stati considerati il movimento del condilo , il movimento del disco e lorientamento condilare . 
however , the range of agreement of 30% between measurements made by the two observers must be related to the extent of condylar excursion , which normally does not exceed 3 c in consideration of the fact that this distance is relatively small , it may be that millimetric differences such as those detected by digital measurements were more relevant compared with those made over greater distances . 
identification of the condylar path using a visual estimate of the position of the condyle centre may have contributed to this variability , which must nonetheless be taken into account before proposing a quantitative method for determining a possible limitation to condyle excursion . there are some potential limitations to this study . 
 in conclusion , qualitative assessment of disc - condyle motion and the presence of joint effusion with dynamic tmj imaging is only minimally operator - dependent , whereas measurement of the condylar path has an interobserver variability of 30% . mento del condilo e del disco risultata rispettivamente ottimale e buona . 
tuttavia il range di concordanza del 30% tra le misurazioni effettuate dai due operatori va tenuto in relazione allentit dellescursione condilare , che normalmente non supera i 3 cconsiderando che questa distanza relativamente contenuta , possibile che differenze millimetriche , quali quelle normalmente presenti nelle misurazioni digitali , siano risultate pi rilevati rispetto a quelle effettuate su distanze maggiori . 
 lidentificazione del tracciato condilare utilizzando una stima visiva della posizione del centro del condilo pu avere inoltre contribuito a tale variabilit , che va considerata se si vuole proporre un metodo quantitativo per stimare uneventuale limitazione dellescursione condilare . in questo studio ci sono delle potenziali limitazioni . 
these additional cancers were located in the same quadrant as the index cancer in 13 women ( 4% ) , in a different quadrant in 12 ( 4% ) and in the contralateral breast in the remaining two ( 1% )  . 
the cancer detection rate in the subgroup of index cancers with lobular histological type was 25% , significantly higher ( p = 0.03 ) than the detection rate of 11% recorded in the subgroup of ductal cancers . 
the cancer detection rate in the subgroup of index cancers > 2 cm was 27% , significantly higher ( p = 0.001 ) than the rate of 8% found in the subgroup of index cancers < 2 c riassunto obiettivo . 
i dati sono stati analizzati con il test esatto di fisher ( p < 0 , 05 ) secondo i seguenti parametri : caratteri istologici della lesione principale ( istotipo tumorale e dimensione ) , densit mammografica ( classificazione breast imaging reporting and data system [ bi - rads ] in categorie da 1 = adiposa a 4 = densa )  . 
le lesioni maligne identificate dalla rm erano nello stesso quadrante rispetto alla lesione principale in 13 pazienti ( 4% ) , interessavano un altro quadrante in 12 pazienti ( 4% ) e la mammella controlaterale nei rimanenti 2 pazienti ( 1% )  . 
una correlazione significativa positiva ( p = 0 , 03 ) emersa tra il tasso di identificazione rm di lesione maligna e istotipo lobulare del carcinoma principale ( lesioni maligne sincrone sono state rilevate nel 25% dei tumori lobulari vs 11% dei tumori duttali )  . 
 una correlazione significativa ( p = 0 , 001 ) stata osservata tra identificazione rm di lesione maligne e dimensione radiol med ( 2011 ) 116 : 12261238 1227 mammographic density was not correlated ( p = 0.48 ) with mr detection of additional cancer , with 14% of additional malignancies being detected in both dense and fatty breasts . 
the use of preoperative mr imaging as an adjunct to conventional breast imaging in women with an infiltrating lobular index cancer and an index cancer > 2 cm is especially beneficial . keywords breast cancer diagnosis breast mri lobular carcinoma dense breast della lesione principale superiore a 2 cm ( lesioni maligne sincrone sono state diagnosticate dalla rm nel 27% dei tumori superiori a 2 cm vs 8% dei tumori inferiori a 2 cm )  . 
il tasso diagnostico superiore quando la neoplasia principale ha istotipo lobulare e dimensioni > 2 c parole chiave tumore mammario diagnosi rm mammaria carcinoma lobulare seno denso introduction introduzione increasing early detection of breast cancer is the primary goal of screening programmes and technological advances . 
conservative surgery necessitates an extremely precise evaluation of disease extent to contain both the number of repeat excisions due to positive surgical margins and local recurrences arising from disease foci outside the radiotherapy field . 
mammography has proved effective as the conventional imaging modality for establishing local disease extent by targeted magnification of the index lesion and of any suspicious abnormalities in the same and contralateral breast [ 3 ]  . 
the use of supplemental screening with us in women with denser breasts quite common in europe and less so in north america is being under evaluation in specifically designed controlled studies [ 5 , 6 ]  . 
 thanks to its high sensitivity [ 7 , 8 ] in detecting invasive breast cancers , magnetic resonance ( mr ) imaging is able to identify neoplasms occult to other imaging modalities [ 9 , 10 ] and has been proposed for local staging of breast cancer [ 11 ] , although this indication is a matter of debate [ 12 , 13 ]  . 
in addition to being a source of anxiety for the patient , false - positive results on mr imaging generate additional costs and delays in definitive surgery and unneclampia diffusione dei programmi di screening e il progresso tecnologico nella diagnostica preventiva per il cancro della mammella hanno comportato il sempre pi frequente riscontro di lesioni mammarie neoplastiche . 
la chirurgia conservativa ha ormai ricevuto definitiva conferma grazie alla dimostrata equivalenza in termini di sopravvivenza della terapia chirurgica conservativa associata a radioterapia e della mastectomia [ 1 , 2 ]  . 
 lespletamento di interventi conservativi imprescindibile da una valutazione estremamente precisa della estensione della malattia onde contenere da una parte il numero di re - escissioni dovute alla presenza di malattia sui margini chirurgici e , dallaltra , le recidive locali che possono insorgere da focolai di malattia esterni al campo della radioterapia . 
lo strumento radiologico tradizionale per il bilancio dellestensione tumorale locale rappresentato dallindagine mammografica con ingrandimenti mirati della lesione principale e delle alterazioni sospette nella stessa mammella e in quella controlaterale [ 3 ]  . 
il carcinoma lobulare e le neoplasie senza microcalcificazioni rappresentano un limite dellindagine mammografica in quanto costituiscono entit che possono essere misconosciute soprattutto in seni con densit elevata [ 4 ]  . 
lassociazione sistematica dellecografia mammaria alla mammografia in donne con seno denso , moderatamente utilizzata in europa e molto meno in usa , attualmente in corso di valutazione in studi controllati appositamente disegnati [ 5 , 6 ]  . 
 in ragione della elevata sensibilit [ 7 , 8 ] nella diagnosi dei tumori mammari invasivi , la risonanza magnetica ( rm ) capace di identificare neoplasie occulte alle altre tecniche di imaging [ 9 , 10 ] e viene proposta per la stadiazione lo1228 radiol med ( 2011 ) 116 : 12261238 essarily extensive surgical procedures . 
to reduce the economic and diagnostic cost , it would be more appropriate to perform preoperative mr imaging only on a subset of patients for whom there is evidence that the examination is beneficial [ 13 ]  . 
 this aim of this study was to verify the existence of parameters allowing selection of patients to be referred to mr evaluation as their risk of additional malignances is significantly higher to justify the use of preoperative mri . 
to this end , we analysed the role of preoperative mr imaging in a series of breast cancers in terms of : ( 1 ) detection rate of synchronous lesions occult to conventional breast imaging ; ( 2 ) distribution of the additional malignant lesions according to size and histological type of index lesion and mammographic density . materials and methods population between january 2006 and november 2009 , we analysed a consecutive series of 291 patients ( age 3387 years ; mean age 54 years ) with a surgical histological diagnosis of invasive breast cancer who had undergone mammography , ultrasound and mr imaging prior to surgery . 
all patients underwent complete breast workup , during which a diagnosis of breast cancer had been established by means of cytological or core biopsy of suspicious abnormalities identified on mammography and ultrasound . 
after undergoing mammography and ultrasound in the same diagnostic centre or , in a minority of cases , in other practices , the patients were referred to our department for preoperative mr staging . 
patients with invasive cancer treated with preoperative adjuvant chemotherapy or hormone therapy , those who had not undergone mammography and ultrasound prior to mr imaging and those with incomplete or unavailable breast cancer documentation at the time of interpreting the mr examination were excluded from the study . histopathology of the surgical specimens revealed invasive ductal carcinoma in 218 ( 75% ) patients , lobular carcinoma in 61 ( 21% ) and other histological types in the remaining patients ( one tubular carcinoma , two mucinous carcinomas , three medullary carcinomas , six papillary carcinomas )  . 
 mr examination and management of additional mr findings mr examinations were performed with the patient in the cale del tumore mammario [ 11 ] , sebbene questa indicazione sia in discussione [ 12 , 13 ]  . 
per ridurre i costi economici e diagnostici , sarebbe ottimale avviare a indagine rm pre - operatoria pazienti selezionate , per le quali vi sia evidenza di beneficio dallespletamento dellesame rm [ 13 ]  . 
 in questo contesto , il presente studio stato condotto allo scopo di verificare lesistenza di parametri che consentano di selezionare le pazienti da avviare a rm , essendo in tali casi significativamente superiore il riscontro di lesioni maligne addizionali . 
pertanto , stato analizzato il ruolo della rm preoperatoria nella serie personale di tumori invasivi della mammella considerando : ( 1 ) il tasso diagnostico di lesioni sincrone occulte alla indagine senologica convenzionale ; ( 2 ) la distribuzione delle lesioni maligne addizionali secondo dimensione e istotipo della lesione principale e secondo la densit mammografica della paziente . materiali e metodi popolazione nel periodo tra gennaio 2006 e novembre 2009 , stata analizzata una serie consecutiva di 291 pazienti ( et 3387 anni ; et media 54 anni ) con diagnosi istologica su pezzo operatorio di carcinoma infiltrante della mammella sottoposte a indagine mammografica , ecografica ed rm prima dellintervento chirurgico . 
tutte le pazienti incluse nello studio hanno effettuato esame senologico completo nel corso del quale stata formulata diagnosi di neoplasia mammaria mediante prelievo per esame citologico o microistologico di alterazioni sospette individuate allesame mammografico ed ecografico . 
dopo aver espletato mammografia ed ecografia nella stessa sede o , in una minor parte dei casi , in altri centri di diagnosi senologica , le pazienti afferivano allindagine rm per la valutazione pre - operatoria dellestensione della malattia . 
sono state escluse dallo studio i casi di neoplasia invasiva avviate a chemioterapia adiuvante o terapia ormonale prima dellintervento chirurgico , quelli che non avevano espletato indagine mammografica ed ecografica prima della rm e quel li in cui la documentazione senologica era incompleta o non disponibile al momento dellinterpretazione dellindagine rm . dallesame patologico del pezzo operatorio , listotipo era duttale infiltrante in 218 ( 75% ) pazienti , lobulare in 61 casi ( 21% ) e altri istotipi nei rimanenti casi ( tubulare in 1 caso , mucinoso in 2 casi , midollare in 3 casi , papillare in 6 casi )  . 
la dimensione media della lesione infiltrante ( deviazione standard ) era di 21 , 511 mm nei casi di istotiradiol med ( 2011 ) 116 : 12261238 1229 prone position in 1.5 - t equipment ( symphony , siemens medical system , erlangen , germany )  . 
the dynamic 3d t1 - weighted gradient echo ( gre ) sequence , performed in the coronal plane until october 2007 ( time to repeat [ tr ] / time to echo [ te ] 12 / 5.65 ms ; flip angle 25 ; matrix 254320 pixels ; field of view [ fov ] 38075 ; thickness 1.24 mm ; acquisition time 60 s ) and in the axial plane thereafter ( tr / te 10 / 4.76 ms ; flip angle 25 ; matrix 38490 pixels ; fov 38591.7 ; thickness , 1.10 mm ; acquisition time 74 s ) was acquired prior to administration of contrast material and repeated six and four times after the intravenous injection of 0.2 ml / kg of gadoterate meglumine ( dotarem ; guerbet s.p.a. ) until december 2008 and after that 0.2 ml / kg of dimeglumine gadobenate ( multihance ; bracco s.p.a. ) at a flow rate of 2.5 ml / s followed by 20 ml of saline solution . 
a region of interest ( roi ) of five to nine pixels was placed on the subtraction images , on the areas of enhancement visualised in the first postcontrast acquisition in the case of coronal sequences and in the second postcontrast acquisition in the case of axial sequences , for timeintensity curve construction . when interpreting the mr images , the readers reviewed patients previous bilateral mammograms and sonograms . 
to establish lesion depth , its distance was measured from the nipple and from the skall radiologists were skilled in breast imaging ( > 3 years of experience ) and breast mr imaging ( > 200 breast mr examinations / year )  . 
areas of enhancement were analysed according to the fischer parameters and in relation to degree of suspicion based on the breast imaging reporting and data system ( bi - rads ) mr imaging classification system of the american college of radiology [ 14 ]  . 
additional lesions detected on mr imaging underwent clinical review , second - look ultrasound and any other appropriate investigations and then monitored for at least 12 months . data analysis results of the clinical examination , imaging investigations , biopsies and surgical procedures were retrospectively reviewed . 
 lesions detected on mr imaging alone were classified as positive for cancer if confirmed by histopathology within 12 months and negative for cancer if they displayed stable features of benignity for at least 12 months . 
malignant lesion detected with mr imaging and interpreted as suspicious at mammography and / or us performed prior to mr imaging po duttale e di 44 , 624 mm nei casi con istotipo lobulare . 
 indagine rm e gestione dei reperti addizionali identificati allindagine rm lindagine rm stata eseguita con paziente in posizione prona e apparecchio da 1 , 5 t ( symphony , siemens medical system , erlagen , germania )  . 
sono state acquisite una sequenza short tau inversion recovery ( stir ) nel piano trasversale e coronale e una sequenza sagittale turbo spin echo ( tse ) t2 - dipendente . 
la sequenza dinamica gradient echo ( gre ) 3d t1 - dipendenti , espletata nel piano coronale fino a ottobre 2007 ( tempo di ripetizione [ tr ] / tempo di eco [ te ] : 12 / 5 , 65 ms ; flip angle 25 ; matrice 254320 pixel ; campo di vista [ fov ] 38075 ; spessore 1 , 24 mm ; tempo di acquisizione 60 secondi ) e successivamente nel piano assiale ( tr / te : 10 / 4 , 76 ms ; flip angle 25 ; matrice 38490 pixel ; fov 38591.7 ; spessore 1 , 10 mm ; tempo di acquisizione 74 secondi ) , stata acquisita prima della somministrazione di mezzo di contrasto ( mdc ) e ripetuta rispettivamente per sei e quattro volte dopo liniezione endovenosa di 0 , 2 ml / kg di gadoterate meglumina ( dotarem , guerbet spa , francia ) fino a dicembre 2008 e successivamente 0 , 2 ml / kg di gadobenato di dimeglumina ( multihance , bracco spa , italia ) di peso corporeo alla velocit di 2 , 5 ml al secondo seguita da 20 ml di fisiologica . 
nelle immagini ottenute per sottrazione , posizionando una regione di interesse ( roi ; 59 pixels ) sulle aree di impregnazione visualizzate nella prima sequenza dopo somministrazione di mdc in caso di acquisizione nel piano coronale e nella seconda sequenza dopo somministrazione di mdc in caso di acquisizione nel piano assiale , sono state costruite curve delle variazioni di segnale intensit / tempo . nella fase di interpretazione delle immagini rm , liconografia relativa alla mammografia bilaterale e alla ecografia immediatamente precedenti stata revisionata . 
per la individuazione della sede della lesione , sono stati presi come punti di riferimento il capezzolo e i piani assiale e sagittale passanti per esso in modo da suddividere la mammella in quadranti . 
tutti i radiologi erano operatori dedicati allimaging senologico ( esperienza in imaging senologico superiore a 3 anni ) esperti di rm mammaria ( espletamento di pi di 200 rm mammarie / anno )  . 
le aree di impregnazione sono state analizzate secondo i parametri di fischer ed in rapporto al giudizio di sospetto secondo la classificazione breast imaging reporting and data system ( bi - rads ) dellamerican college of radiology system [ 14 ]  . 
le lesioni addizionali diagnosticate dallindagine rm sono state sottoposte a rivalutazione dellesame senologico , a second look ecografico e altri 1230 radiol med ( 2011 ) 116 : 12261238 were excluded from the analysis of mr - detected cases , and their detection was ascribed to conventional breast imaging . 
data were analysed with fishers exact test , with significance set a p < 0.05. results synchronous occult malignant lesions detected at mr imaging mr imaging detected 55 malignant lesions synchronous to the index tumour in 38 / 291 patients ( 13% )  . 
in 15 / 55 lesions , the diagnosis of malignancy was established on the basis of ultrasound - guided biopsy , as mr lesions had a sonographic correlate on second - look ultrasound . 
they had a multifocal growth pattern in the same breast quadrant in 13 / 291 ( bifocal in four , trifocal in nine ) , whereas they were located in another quadrant in 12 / 291 ( bifocal in eight , trifocal in four )  . 
histological diagnosis of ipsilateral malignancies was invasive cancer in 17 / 25 cases ( 68% ) and in situ cancer in 8 / 25 ( 32% ) and of contralateral cancer foci was invasive cancer in both cases . 
with regard to lesion size , 5 / 40 ( 12.5% ) malignancies had a diameter 5 mm , 26 / 40 ( 65% ) between 6 and 10 mm , 8 / 40 ( 20% ) between 10 and 20 mm and only 1 / 40 ( 2.5% ) > 20 mm . distribution of malignancies malignant lesions detected with mr imaging were evaluaccertamenti in base alle alterazioni evidenziate , quindi monitorate per un periodo di almeno 12 mesi . analisi dei dati i risultati dellesame clinico , delle metodiche imaging , di biopsie e dellintervento chirurgico sono stati sottoposti a revisione retrospettiva . 
le lesioni identificate dalla sola indagine rm sono state classificate positive per cancro se patologicamente confermate entro 12 mesi e sono state considerate negative per cancro se hanno conservato caratteri di benignit stabili per un periodo di almeno 12 mesi . 
i casi di lesione maligna identificati dalla rm e considerati come portatori di alterazioni di sospetto alla mammografia e / o allecografia espletate prima della rm , sono stati esclusi dalla considerazione dei casi identificati dalla rm e la loro diagnosi stata attribuita allesame senologico convenzionale . 
i dati sono stati analizzati con il test statistico di fisher ( significativit : p < 0 , 05 )  . risultati lesioni maligne occulte sincrone identificate dalla rm lindagine rm ha identificato 55 lesioni maligne sincrone alla neoplasia principale in 38 / 291 pazienti ( 13% )  . 
in 15 / 55 lesioni la diagnosi di malignit stata formulata mediante prelievo sotto guida ecografica trattandosi di lesioni rm con corrispettivo reperto al second look ecografico espletato dopo indagine rm . 
le lesioni maligne sincrone identificate dalla rm erano omolaterali alla lesioradiol med ( 2011 ) 116 : 12261238 1231 table 1 site , histological diagnosis and size of the 40 additional cancers detected with mr imaging study variable category cases , n ( % ) location from the index cancer same quadrant different quadrant contralateral breast histology of mr additional cancer infiltrating carcinoma in situ carcinoma size 5 mm 610 mm > 10 mm 22 ( 55 ) 16 ( 40 ) 2 ( 5 ) 32 ( 80 ) 8 ( 20 ) 5 ( 12.5 ) 26 ( 65 ) 9 ( 22.5 ) tabella 1 sede , diagnosi istologica e dimensioni in 40 lesioni maligne diagnosticate dalla rm , sincrone rispetto al tumore principale ne principale in 25 casi ; avevano crescita multifocale nello stesso quadrante in 13 / 291 ( bifocale in 4 casi , trifocale in 9 casi ) mentre interessavano un altro quadrante in 12 / 291 ( bifocale in 8 casi , trifocale in 4 casi )  . 
la diagnosi istologica delle lesioni maligne omolaterali stata di patologia infiltrante in 17 / 25 casi ( 68% ) e di lesione in situ in 8 / 25 casi ( 32% )  . 
per quanto riguarda il risultato patologico in rapporto alle dimensioni della lesione , 5 / 40 ( 12 , 5% ) lesioni maligne avevano diametro inferiore o uguale a 5 mm , 26 / 40 ( 65% ) avevano diametro compreso tra 6 e 10 mm , 8 / 40 ( 20% ) erano estese tra 10 e 20 mm e solamente 1 / 40 ( 2 , 5% ) lesioni maligne era maggiore di 20 mm . variabile in studio categoria numero di casi ( % ) distribuzione della patologia maligna sede delle lesioni addizionali rispetto al tumore principale stesso quadrante differente quadrante mammella controlaterale 2 ( 5 ) 22 ( 55 ) 16 ( 40 ) diagnosi istotologica lesioni infiltranti lesioni in situ dimensioni 5 mm 610 mm > 10 mm 32 ( 80 ) 8 ( 20 ) 5 ( 12 , 5 ) 26 ( 65 ) 9 ( 22 , 5 ) ated according to histological type of the index cancer and as a mammographic density . 
in particolare , la rm ha evidenziato focolai neoplastici sincroni in 25 / 218 ( 11% ) casi di carcinoma duttale infiltrante versus 15 / 61 ( 25% ) casi di carcinoma lobulare ( p = 0 , 03 )  . 
la dimensione della neoplasia principale si dimostrata correlata con la diagnosi rm di malignit in quanto la rm ha evidenziato tumori sincroni in 14 / 176 ( 8% ) casi in cui il tumore principale aveva dimensioni inferiori a 2 cm versus 26 / 115 ( 27% ) con dimensioni superiori ( p = 0 , 001 )  . 
in 38 donne la biopsia ha confermato la presenza di malignit ( 37% : veri positivi della serie complessiva ) ; nelle rimanenti 64 donne ( 63% falsi positivi della serie complessiva ) la biopsia ha rilevato patologia benigna . 
considerando le lesioni solo rm visibili , prive di corrispettivo al second look ecografico , la verifica istologica ha rilevato patologia maligna in 27 / 52 casi ( 52% : veri positivi rm ) e patologia benigna nei rimanenti 25 / 52 casi ( 48% : falsi positivi rm )  . 
la distribuzione della patologia benigna nella serie complessiva stata la seguente : adenosi ( 24 / 64 : 39% ) e fibroadenomi ( 8 / 64 : 13% ) rappresentano le lesioni pi frequenti , seguite dal mastopatia fibrocistica e da fibro1232 radiol med ( 2011 ) 116 : 12261238 table 2 magnetic resonance imaging ( mri ) detection rate of otherwise occult additional cancers according to histological type and tumour size of the index tumour and mammographic density study variable no . 
in 38 / 102 cases , mr findings were malignant ( 37% true - positive findings for the overall series ) ; in the remaining 64 women ( 63% false - positive findings for the overall series ) biopsy revealed benign disease . 
analyzing lesions visible on mr imaging only ie , without a correlate on second - look ultrasound histological examination revealed malignant disease in 27 / 52 cases ( 52% true - positive mr findings ) and benign disease in the remaining 25 / 52 cases ( 48% false - positive mr findings )  . 
 distribution of benign disease in the overall series was adenosis ( 24 / 64 , 39% ) and fibroadenomas ( 8 / 64 , 13% ) , followed by fibrocystic disease and fibrosis ( 12 / 64 , 19% ) , proliferative sclerotic lesions ( 9 / 64 , 14% ) , papillomas ( 4 / 64 , 6% ) and miscellaneous benign entities ( 6 / 64 , 9% )  . 
 a tale fine stata analizzata la serie consecutiva di 291 carcinomi della mammella alla ricerca di criteri che consentano di radiol med ( 2011 ) 116 : 12261238 1233 fig . 
mammograms show a 3 - cm cluster of pleomorphic calcifications ( arrow ) in the upper inner quadrant of the left breast and in the central area of the right breast . 
preoperative breast mr imaging ( f - i ) ( axial plane , subtracted t1 - weighted , contrast - enhanced images ) shows clumped linear and ductal enhancement adjacent to the biopsy sites , corresponding to residual disease ( f , g )  . 
mr image of the right breast shows additional , irregularly shaped , irregularly marginated , heterogeneously enhancing masses in right lower outer ( h ) and upper inner ( i ) quadrants . 
nel quadrante supero - mediale della mammella sinistra e in regione retroareolare della mammella destra si notano numerose microcalcificazioni pleomorfe estese in unarea di circa 3 cle sedi vengono sottoposte a prelievo microistologico sotto guida stereotassica ( carcinoma duttale infiltrante , in entrambe le sedi )  . 
lindagine rm pre - operatoria ( f - i : piano assiale , immagini di sottrazione con mezzo di contrasto ) documenta una vasta area di impregnazione tipo non massa del parenchima adiacente alla camera bioptica , in entrambe le sedi sottoposte a prelievo compatibile con malattia residua ( f , g )  . 
ulteriori aree di impregnazione , separate da quelle precedenti , si rilevano nei rimanenti quadranti della mammella destra , rispettivamente nel quadrante infero - esterno ( h ) e in quello supero - mediale ( i )  . 
lesame isologico del pezzo operatorio ha confermato la presenza di neoplasia duttale infiltrante , solida e cribriforme , con crescita multicentrica a destra e lesione proliferativa residua a sinistra . 1234 radiol med ( 2011 ) 116 : 12261238 fig . 
preoperative breast mr imaging ( e , f ) ( axial plane , subtracted t1 - weighted contrast - enhanced images ) shows an irregular spiculated heterogeneously enhancing mass ( arrow in e ) corresponding to the index cancer , with an additional irregular spiculated mass in the contralateral breast ( arrow in f )  . 
allindagine mammografica ( a - d ) , nel quadrante supero - esterno della mammella destra , verso il prolungamento ascellare , si nota una formazione espansiva di aumentata densit , con margini spiculati ( frecce in a e c )  . 
lindagine rm preoperatoria ( e , f ) ( piano assiale , immagini di sottrazione dopo somministrazione di mezzo di contrasto ) conferma la lesione proliferativa al prolungamento ascellare di destra ( freccia in e ) e mostra una lesione nel quadrante supero - mediale della mammella sinistra ( freccia in f )  . 
il prelievo sotto guida ecoscopica per esame microistologico depone per lesione maligna sincrona ( carcinoma lobulare infiltrante )  . radiol med ( 2011 ) 116 : 12261238 1235 at 6 months , which confirmed their stability over time ( follow - up range : 1236 months )  . discussion the aim of this study was to verify the benefit of mr imaging in the preoperative assessment of infiltrating breast cancers diagnosed with conventional breast imaging . 
with this in mind , we analysed a consecutive series of 291 breast cancers looking for criteria that could help identify patients who might benefit from breast mr imaging on the grounds of the higher rate of additional cancer foci detected by mr imaging . 
in fact , in addition to being the most reliable tool for determining the index cancer size [ 16 , 17 ] and identifying the associated extensive intraductal component [ 18 , 19 ] , mr imaging detects additional mammographically and sonographically occult cancer foci ipsilateral to the index cancer in 27% of cases [ 20 ] and contralateral foci in 35% of cases [ 21 ]  . in this series , mr imaging detected 55 synchronous malignancies in 38 / 291 ( 13% ) patients . 
to guarantee the effective negativity of conventional breast imaging , it was deemed necessary to distinguish between lesions with a correlate on second - look ultrasound ( n = 15 / 55 ; 27% ) and those effectively visible on mr imaging only that is , the remaining 40 / 55 lesions ( 63% )  . 
 the controversy regarding the contribution of preoperative breast mr imaging revolves around the high number of false - positive findings and the doubtful clinical significance of the additional cancer foci detected with mr imaging in terms of recurrence and prognostic impact . 
in the contralateral breast , the incidence of suspicious mr imaging findings is estimated to be 9.3% , with a positive predictive value of 48% and a false - positive rate of 52% [ 23 ]  . 
 in this series , preoperative mr imaging detected additional findings in 102 / 291 patients ( 35% ) ; histology confirmed the presence of malignancy in 38 / 102 cases ( 37% ) and revealed benign disease in the remaining 64 / 102 cases ( 63% )  . 
the use of second - look ultrasound allowed identification of approximately half ( 50 / 102 cases ) of the findings incidentally detected with mr imaging and consequently reduced the rate of false - positive findings from 63% to 48% . 
 nonetheless , even after second - look ultrasound , the falseidentificare le pazienti che possano giovare dellesecuzione della rm mammaria in quanto il tasso di lesioni maligne sincrone individuate dalla rm maggiore . 
infatti oltre a rappresentare lo strumento pi affidabile per la valutazione dimensionale della lesione principale [ 16 , 17 ] e per la identificazione della estesa componente intraduttale associata [ 18 , 19 ] , lesame rm identifica focolai di malignit occulti alla mammografia ed ecografia omolaterali alla neoplasia principale nel 27% [ 20 ] e controlaterali nel 3%5% dei casi [ 21 ]  . nella presente serie , lindagine rm ha identificato 55 lesioni maligne sincrone alla neoplasia principale in 38 / 291 pazienti pari al 13% . 
a garanzia delleffettiva negativit dellesame senologico convenzionale , si ritenuto opportuno un distinguo tra le lesioni identificate al second - look ecografico e pari a 15 / 55 ( 27% ) e quelle realmente diagnosticate solo dalla rm ovvero le restanti 40 / 55 lesioni ( 63% )  . 
 le questioni tuttora dibattute riguardo al contributo della rm mammaria pre - operatoria vertono attorno allelevato numero di falsi positivi e al dubbio significato clinico dei focolai neoplastici identificati dalla rm , in termini di recidive ed impatto prognostico . 
nella mammella controlaterale , lincidenza di lesioni rm sospette stimata pari al 9 , 3% , con un valore predittivo positivo del 48% e un tasso di falsi positivi del 52% [ 23 ]  . 
 nella serie in esame , lindagine rm pre - operatoria ha evidenziato reperti addizionali complessivamente in 102 / 291 pazienti ( 35% ) ; lesame istologico ha confermato la presenza di malignit in 38 / 102 casi ( 37% ) e di lesione benigna nei restanti 64 / 102 casi ( 63% )  . 
lintroduzione del second look ecografico ha permesso il riconoscimento di circa la met ( 50 / 102 casi ) dei reperti incidentalmente rilevati dalla rm e di conseguenza il contenimento del numero dei falsi positivi dal valore del 63% a quello del 48% . 
anche dopo lapplicazione del second look ecografico , il tasso dei falsi positivi rimane considerevole , ci a dire che circa la met delle lesioni sospette solo rm visibili non sono maligne . 
quindi di essenziale importanza che queste lesioni vengano sottoposte a biopsia prima di qualsiasi decisione terapeutica chirurgica . per quanto riguarda limpatto clinico , nello studio retrospettico di solin et al . 
 [ 24 ] , che analizza il tasso di recidiva , di sopravvivenza e di insorgenza di metastasi a distanza e di neoplasie controlaterali dopo terapia chirurgica conser1236 radiol med ( 2011 ) 116 : 12261238 positive rate resulted high , implying that about half of the suspicious lesions visible on mr imaging alone are not malignant . 
it is therefore mandatory to obtain a biopsy of these lesions before making any decision on surgical treatment . as concerns clinical impact , the retrospective study by solin et al . 
 [ 24 ] , who analysed the rates of recurrence , survival , distant metastasis and contralateral cancers after conservative surgery over an 8 - year follow - up period , found no difference between the group of women who underwent preoperative mr imaging and those who underwent conventional breast imaging alone . 
mr imaging identified synchronous malignancies in both histological types of index cancer , and specifically in 11% of ductal cancers and 25% of lobular cancers , even though there was a statistically significant difference in favour of the lobular type . 
 the data are accounted for by the biology of lobular cancer with its multicentric growth pattern frequently missed at conventional breast imaging and by the high sensitivity of mr imaging in detecting lobular cancer [ 2628 ]  . 
with regard to tumour size , patients with breast cancer who benefit most from mr imaging are those with a cancer > 2 c synchronous lesions were seen in 27% of larger cancers and in only 8% of smaller cancers . 
in fact , increasing the size of the tumor , increases the likelihood of a multifocal growth pattern . considering that the accuracy of mr imaging is unaffected by mammographic density [ 29 ] , we analysed the mr detection rate in dense versus fatty breasts . 
this finding is in disagreement with the theoretical assumptions but is similar to that reported by previous studies [ 20 , 21 ]  . despite the large patient population , our study considers a clinical series of self - referring women . 
furthermore , vativa con follow - up della durata di 8 anni , non sono state evidenziate differenze nel gruppo di donne sottoposte a rm pre - operatoria rispetto a quelle sottoposte al solo esame senologico convenzionale . i risultati preliminari dello studio comparative effectiveness of magnectic resonance imaging in breast cancer ( comice ) provenienti dallo studio randomizzato di 1623 pazienti [ 25 ] , non hanno rilevato differenze nel tasso di reinterventi nelle donne sottoposte a rm pre - operatoria n differenze nel tasso di sopravvivenza libera da malattia fino ad ora , dopo follow - up medio di 3 , 1 anni . 
 in attesa dei risultati definitivi degli studi prospettici riguardo allimpatto clinico della rm , in questo lavoro stata verificata leventuale esistenza di gruppi di pazienti che possano avere maggior beneficio dallindagine rm , considerando come variabili in studio istotipo della lesione principale , dimensioni tumorali e densit radiologica . 
 lindagine rm ha identificato lesioni maligne sincrone in entrambi gli istotipi di lesione primitiva , nell11% delle neoplasie duttali e nel 25% delle neoplasie lobulari , tuttavia con differenza statisticamente significativa a vantaggio dellistotipo lobulare . 
il risultato trova ragione nella biologia del carcinoma lobulare , con pattern di crescita multicentrico , frequentemente misconosciuto allesame senologico convenzionale e nella elevata sensibilit della rm per la diagnosi di carcinoma lobulare [ 2628 ]  . 
in quanto alle dimensioni tumorali , le pazienti con neoplasia mammaria che giovano maggiormente dellesecuzione dellindagine rm sono le pazienti con tumore superiore a 2 clesioni sincrone sono state osservate nel 27% dei tumori con cospicue dimensioni e solo nel 8% dei tumori con dimensioni inferiori . 
infatti , allaumentare delle dimensioni tumorali aumenta la crescita con proliferazione multifocale . considerando che laccuratezza della rm non risente della densit mammografica [ 29 ] stato analizzato il tasso diagnostico rm nei seni densi e nei seni adiposi . 
il dato in disaccordo con i presupposti teorici ma simile a quanto riscontrato in altre esperienze [ 20 , 21 ]  . nonostante la popolazione sia numerosa , la casistica in esame considera una serie clinica con afferenza spontanea . 
nella popolazione in esame , i carcinomi di istotipo duttale rappresentano la grande maggioranza dei casi ( 75% ) e quelli lobulari sono solo circa un quinto della casistica complessiva . 
inoltre , i carcinomi di istotipo lobulare presentano dimensioni medie decisamente superiori a quelle dei carcinomi di istotipo duttale ( 44 , 6 mm versus 21 , 5 mm )  . 
even the literature suggests that lobular carcinomas tend to have a slightly larger mean size compared with ductal carcinomas and that cancers > 5 cm are more likely to be of the lobular type [ 3032 ]  . 
however , we cannot exclude with certainty that the incidence of additional cancer foci was influenced by the larger size of lobular carcinomas , as multifocality is dependent both on the intrinsic growth pattern of lobular cancers and on tumour size . 
in contrast , in our series , mr imaging detected additional malignancies in 25% of cases of lobular carcinoma , and this result is not significantly different from that reported in mann et al . 
if the frequency of additional cancer foci detected in cases of lobular carcinoma had been influenced by the size factor , we would have expected a higher incidence of additional lesions than that reported in the literature . 
overall , this was a retrospective analysis of a consecutive series of infiltrating breast cancers and , as such , it cannot be considered definitive evidence validating the use of preoperative breast mr imaging as a routine investigation . 
 in conclusion , mr imaging detects additional cancer foci to the index cancer that are occult to mammography and ultrasonography in 9% of patients affected by an infiltrating breast cancer . 
the detection rate for malignancies is higher when index cancer shows lobular type histology or size higher than 2 cm , as the mr detection rate for additional cancer foci in these patient groups increased to 25% and 27% , respectively . 
on the other hand , in consideration of the high number of false - positive findings , the detection rate of additional lesions on mr imaging results in a substantial number of further tests and requires correlation with conventional breast imaging as well as confirmation by an imaging - guided pathological examination . 
on the basis of our results , the number of breast mr imaging studies could be contained by selection of patients with a greater likelihood of multifocal and multicentric disease . 
 tuttavia , non si pu escludere con certezza che lincidenza di focolai neoplastici aggiuntivi sia stata influenzata dalle maggiori dimensioni dei lobulari rispetto ai duttali , essendo la multifocalit dipendente dalle caratteristiche intrinseche di crescita tumorale proprie del carcinoma lobulare piuttosto che di altri istotipi tumorali , ma anche dalle dimensioni della neoplasia . 
per contro , nella serie in esame lindagine rm ha diagnosticato lesioni maligne addizionali nel 25% dei casi di carcinoma lobulare e questo risultato diagnostico non si discosta in modo significativo da quello riportato nella revisione di mann et al . 
se la frequenza di lesioni addizionali rilevate nellistotipo lobulare fosse stata influenzata dal fattore dimensionale , nella serie in esame ci si dovrebbe aspettare una frequenza di lesioni addizionali pi elevata rispetto a quella riportata in letteratura . 
nel complesso , si tratta di una analisi retrospettiva condotta in una serie consecutiva di lesioni mammarie infiltranti e come tale non pu costituire un elemento definitivo per validare luso della rm pre - operatoria come esame di routine . 
il tasso diagnostico di lesioni maligne maggiore in presenza di carcinoma lobulare , di neoplasie con dimensioni superiori a 2 cm in quanto in queste categorie di pazienti la identificazione rm di carcinomi sincroni rispettivamente del 25% e del 27% . 
daltra parte in considerazione dellelevata percentuale di falsi positivi , il rilievo di lesioni addizionali allindagine rm genera un cospicuo numero di approfondimenti diagnostici , necessita di correlazione con lindagine senologica mammografica ed ecografica e conferma patologica mediante prelievo sotto guida imaging . 
 conflict of interest none radiol med ( 2011 ) 116 : 1313 doi 10.1007 / s11547 - 011 - 0727 - 0 erratum hypoxic liver perfusion with mitomycin - c for treating multifocal metastases and unresectable primary tumours : a single - centre series of 42 patients infusione intra - arteriosa epatica in ipossia di mitomicina - c per il trattamento di metastasi epatiche multiple e di tumori primitivi inoperabili : esperienza mono - centrica in 42 pazienti a . 
comino , corso re umberto 141 , 10134 torino , italy , tel . : + 39 - 011 - 3181211 , e - mail : mariacom@tiscalinet.it received : 8 october 2010 / accepted : 18 november 2010 / published online : 10 july 2011 springer - verlag 2011 abstract the radiology report has always been considered as the most important step in the clinical radiological act . 
italy aside , this issue has been thoroughly investigated and debated abroad since the 1970s and , in the past as well as more recently , many interesting contributions have been published both on the need for verbal communication , particularly in certain settings , and on the best manner to approach this task . 
the author hopes that in italy , as in other countries , an extensive debate will give rise to a fuller awareness of the issue , thereby providing a range of shared solutions . keywords radiological report patientdoctor communication riassunto il referto radiologico stato considerato da sempre il momento pi significativo dellatto clinico radiologico . 
a differenza che in italia , allestero questo problema stato ampiamente approfondito e dibattuto fin dagli anni 70 e sono stati presentati , in passato come recentemente , numerosi interessanti contributi riguardanti sia la necessit del colloquio verbale specie in determinate circostanze , sia le migliori modalit di esecuzione del colloquio stesso . 
lautore si augura che anche in italia un ampio dibattito sullargomento possa far nascere una migliore presa di coscienza del problema fornendo quindi soluzioni possibili e condivise . parole chiave referto radiologico comunicazione medico - paziente introduction introduzione not so long ago , francesco dalla palma , at the time president of the italian society of medical radiology , stated that the major product of the radiologists profession is the report , which represents the most significant step in the clinical radiological act . 
at the same time , several publications ( mostly by francesco schiavon ) and a large number of conferences extensively discussed the radiology report with the laudable aim of standardising its features and , more importantly , of avoiding omissions or errors . this attention surrounding the report tended , however , to in un passato abbastanza recente , lallora nostro presidente francesco dalla palma affermava che la completa realizzazione della professione del radiologo trova la sua massima espressione nel referto che rappresenta il momento pi significativo dellatto clinico radiologico . 
contemporaneamente , numerosi scritti ( merito soprattutto di francesco schiavon ) e ancor pi numerosi convegni approfondivano in ogni dettaglio il referto con il lodevole scopo di uniformarne le caratteristiche e soprattutto di evitare omissioni o errori . 1154 radiol med ( 2011 ) 116 : 11531160 obscure the indisputable fact that the report does not in any way fulfil the duty of the physician , and therefore of the clinical radiologist , to communicate with the patient , as we are reminded in art . 
taking into account his or her ability to understand .... unfortunately , the tradition of face - to - face communication between the radiologist and the patient was lost in the 1960s as a result of a series of objective factors but also , in my opinion , as a result of new cultural attitudes that i now attempt to delineate . 
the first reason is the expansion of health care , which has dramatically increased the number of radiological procedures ; second , the emergence of the radiology technician , an allied profession that has often deprived us of direct contact with the patient ; third , the development of new technologies ( computed tomography , ultrasound , interventional radiology and magnetic resonance imaging ) , which has further expanded the commitments and responsibilities of the radiologist , taking up more time and making communication with the patient increasingly infrequent and difficult . 
 in addition , the idea has taken hold that it is not essential for the radiologist to communicate with the patient ( now that specialist medicine prioritises communication with the general practitioner or the referring specialist ) , in part because the radiologist may not know the patient and does not know how he or she might react to bad or worrying news . 
the radiologist may also be afraid to say too little or too much , perhaps causing embarrassment to the general practitioner or specialist , and may think that the patient would prefer to have the diagnosis communicated and explained by someone else . finally , todays radiologists are not always adequately trained to communicate with patients or explain a report , being used to maintaining a certain detachment and concentrating on the accuracy and completeness of the diagnosis ; they have long had an almost ancillary status with respect to clinicians to whom the patients refer for interpretation of the report when not of the images themselves . this forced association between the report and its communication has meant that in italy , apart from sporadic mention by a few influential authors [ 14 ] , the question of the desirability or even the need for the radiologist to communicate verbally the results of radiological examinations to patients has never been addressed . 
the first contribution bringing radiologists attention to the increasing lack of information to patients with regard to examination results was the famous and much - quoted editorial by berlin [ 5 ] in 1977 , titled the radiologist : doctors doctor or patients doctor ? at the latest european congress of radiology questa attenzione concentrata sul referto metteva per in ombra il fatto , incontestabile , che il referto non esauriva in alcun modo il dovere del medico , e quindi anche del medico radiologo , di comunicare con il paziente , come ci viene ben ricordato dallart . 
 purtroppo , labitudine al dialogo fra il medico radiologo ed il paziente si perduta negli anni 60 per una serie di fattori oggettivi , ma anche , a mio modesto parere , per nuovi atteggiamenti culturali che cercher ora di ricordare . 
anzitutto , lestendersi dellassistenza sanitaria che ha moltiplicato vertiginosamente gli esami radiologici ; poi , la comparsa della nuova figura professionale del tecnico di radiologia che ci ha privato sovente del contatto diretto con i pazienti ; in seguito , laffermarsi delle nuove tecnologie ( tomografia computerizzata , ecotomografia , radiologia interventistica , risonanza magnetica ) che ha ancora dilatato gli impegni e le responsabilit del medico radiologo impegnandone sempre pi il tempo e rendendo sempre pi difficile e raro il colloquio . oltre a ci , si fatto strada negli anni il concetto che non sia compito essenziale del medico radiologo comunicare con il paziente ( ormai la medicina specialistica considera prioritaria la comunicazione con il medico di base o quantomeno inviante ) , anche perch il medico radiologo non lo conosce o quasi e non sa come potrebbe reagire ad una notizia cattiva o anche solo inquietante , ha inoltre paura di dire troppo o troppo poco mettendo forse in difficolt il curante o un altro specialista e talora pensa che il paziente stesso preferisca ricevere da altri la comunicazione della diagnosi e le spiegazioni ad essa legate . infine , il medico radiologo oggi non sempre adeguatamente preparato a dialogare con il paziente o anche solo a spiegare adeguatamente un referto , abituato a mantenere un certo distacco dal paziente occupandosi di pi dellesattezza e della completezza della diagnosi , mantiene da tempo una condizione quasi ancillare nei confronti del clinico al quale il paziente si rivolge per interpretare il referto quando non le stesse immagini . la forzata identificazione fra referto e comunicazione ha fatto s che in italia , tranne pochi cenni di pochi autorevoli autori [ 14 ] , non fosse mai affrontato il problema dellopportunit o forse della necessit della comunicazione verbale ai pazienti dei risultati delle indagini radiologiche . 
il primo articolo che pose allattenzione dei medici radiologi la sempre crescente disinformazione dei pazienti sui risultati delle loro indagini fu il celebre , citatissimo , editoriale di berlin [ 5 ] del 1977 , dal titolo the radiologist : doctors doctor or patients doctor ? e nel pi recente european congress radiol med ( 2011 ) 116 : 11531160 1155 ( more than 30 years later ! ) the same author again took up and developed what he wrote back in 1977 . of radiology ( dopo pi di trentanni ! ) lo stesso autore ha ripreso e potenziato quanto scritto allora . the numerous papers that followed mainly concerned the two basic aspects of communication : if and why and how . 
according to several authors , the question remains open : the ethical and deontological requirement for communication is not in question ( and improved communication can help avoid malpractice litigation ) , whereas the controversy remains as to whether it should be the radiologist to communicate with the patient and whether this is indeed what the patient wants [ 610 ]  . 
other authors , following surveys conducted both in europe and the united states , show that about 90% of patients want to hear the results of imaging investigations directly from the radiologist in all cases , whereas the remaining 10% want this done only following an explicit request . 
other , especially french , authors have taken for granted the need for verbal communication with the patient to explain the procedures and have moved on to analyse the various possibilities and opportunities of verbal communication [ 1826 ] , dispensing many at times interesting but often obvious suggestions and providing some protocols [ costruire , raliser , ecouter , donner informations , organiser ( credo ) , partnership , excuses ( apology ) , respect , legitimization , empathy , support ( perles ) , setting up , perception , invitation , knowledge , emotions , strategy ( spikes ) ] to improve and standardise communication . what happens in italy ? there are few who deny the right of patients to be informed of the results of imaging procedures , whereas many ( in varying percentages according to the subspecialty ) , for reasons of time and work organisation , overlook this right and consider the report as the only required form of communication . 
to better assess the situation and determine whether and to what extent patients receive verbal communication of the results of procedures in addition to the written report , a brief survey was conducted in the diagnostic imaging unit of a public hospital and a noncontracted private clinic . 
the question put to my colleagues was : was the patient informed verbally of the results of the procedure ? if yes , please specify whether the information was conveyed using a few quick and generic words or via a complete and comprehensive report . 
the results are presented in tables 1 and 2 . as can be seen , the difference between the two situations is substantial as far as conventional radiology is concerned , where the constant and predominant presence of the radiology technician makes any communication with the radiologist almost impossible ; this is much less the case for all the other imaging modalities . 
secondo i diversi autori il problema rimane aperto : lesigenza etica e deontologica della comunicazione non in discussione ( e la maggiore comunicazione pu mettere al riparo dalle denunce per malpractice ) , mentre permane controversa lopportunit che sia proprio il medico radiologo a parlare e che sia proprio questo che i pazienti desiderano [ 610 ]  . 
altri autori , a seguito di indagini svolte in nazioni europee e negli stati uniti , hanno dimostrato che circa il 90% dei pazienti desidera che il medico radiologo comunichi loro sempre lesito degli esami , mentre il restante 10% lo desidera solo a seguito di unespressa richiesta . 
solo il 50% dei medici curanti desidera invece la comunicazione verbale al paziente da parte del medico radiologo , ma la percentuale aumenta considerevolmente ( circa il 70% ) quando si tratta di situazioni gravi o urgenti [ 1117 ]  . 
ancora altri autori , specie francesi , considerata come acquisita la necessit del colloquio con il paziente per la spiegazione degli esami , hanno analizzato le diverse e le migliori possibilit ed opportunit della comunicazione verbale [ 1826 ] dispensando numerosi , talora interessanti ma sovente scontati consigli e fornendo anche alcuni protocolli standard ( construire , raliser , ecouter , donner informations , organiser [ credo ] , partnership , excuses ( apolology ) , respect , legitimization , empathy , support [ perles ] , setting up , perception , invitation , knowledge , emotions , strategy [ spikes ] ) per migliorare e standardizzare il colloquio stesso . 
 cosa avviene in italia ? sono ormai pochi quelli che negano il diritto da parte dei pazienti di essere informati sui risultati delle indagini di diagnostica per immagini , mentre sono moltissimi ( in diversa percentuale a seconda delle sub - specialit ) che per ragioni di tempo e di organizzazione del lavoro non ne tengono alcun conto e considerano il referto la sola forma dovuta di comunicazione . 
al fine di meglio verificare la situazione , stata condotta una breve inchiesta nel servizio di diagnostica per immagini di un ospedale pubblico e di un poliambulatorio privato non convenzionato al fine di verificare se ed in quale misura i pazienti ricevevano , oltre al referto scritto , una comunicazione verbale sui risultati degli esami . 
la domanda formulata al collega era questa : stata data al paziente una comunicazione verbale sullesito dellesame ? in caso positivo si doveva precisare se tale comunicazione era stata fornita con poche rapide e generiche parole ( a ) oppure con una completa ed esauriente relazione ( b )  . 
i risultati sono presentati nelle tabelle 1 e 2 . come si pu osservare , la differenza fra le due situazioni sensibile per quanto riguarda la radiologia tradizionale , dove la costante e prevalente attivit del tecnico radiologo 1156 radiol med ( 2011 ) 116 : 11531160 table 1 san giovanni bosco public hospital , turin , italy table 2 ci . 
 the brief survey showed , however , that in the most serious cases , verbal communication usually does take place . nothing can be said with regard to the quality of the verbal communication , if not to restate that the radiologist is not always sufficiently trained to communicate with patients , given that this tradition has been long lost , and radiology specialty schools offer no opportunity for communication and do not ( yet ? ) teach doctorpatient communication techniques , there being no conviction that this is either useful or necessary . a recent and highly recommended book by de santi and simeon [ 27 ] suggests the characteristics of ideal consultation , lasting not less than 10 min ! here is a summary : 1 . 
welcome : the setting , privacy , the possible assistance of a family member , listening ( patients usually ending what they have to say in 92 s ) ; 3 . 
information : supplied gradually and simply , leaving room for other questions and respecting what the patient does not want to know , to the point of reaching if possible the diagnosis ; rende quasi impossibile il colloquio con il medico ; lo assai meno per tutte le altre metodiche . 
la differenza segnalata fra il colloquio breve e generico e quello pi dettagliato e completo sembra in gran parte legata alla complessit e gravit della patologia riscontrata e in qualche misura anche allimpressione soggettiva del medico radiologo . 
 non possibile alcuna considerazione a proposito della qualit del colloquio , se non ribadendo che il medico radiologo non sempre sufficientemente preparato a parlare con il paziente : se ne da tempo perduta la tradizione , le scuole di specializzazione non ne evidenziano anche solo lopportunit e non insegnano ( ancora ? ) le migliori modalit del colloquio stesso , fa difetto la convinzione che sia davvero utile e necessario . un recente e consigliabilissimo libro italiano di de santi e simeoni [ 27 ] suggerisce le caratteristiche di un colloquio ideale , della durata non inferiore a 10 minuti ! eccone una sintesi : 1 . 
accoglienza : i locali , la privacy , leventuale assistenza di un familiare , lascolto ( di solito il paziente conclude il suo discorso in 92 secondi ) ; 3 . 
support : not only describing the subsequent diagnostic and therapeutic procedures , but also covering the benefits and possible risks , and a general assessment of the prognosis ; 5 . 
conclusion : a friendly goodbye with the offer of further consultations and a telephone number . such an ideal consultation is no doubt difficult , if not impossible , to carry out but , without succumbing to the easy temptation of thinking that it is the duty of clinicians only , certain perhaps necessary considerations need to be made , such as : verbal communication with patients is always appropriate and sometimes indispensable ( in severe cases and emergencies ) ; spazio ad altre domande del paziente e rispettando quanto non vuole sapere fino a giungere se possibile alla diagnosi ; 4 . 
conclusione : un saluto amichevole , la possibilit di un ulteriore colloquio , un numero di telefono . un colloquio ideale come quello proposto certamente difficile e forse impossibile da realizzarsi , ma senza cedere alla comoda tentazione di pensare che sia solo compito dei clinici sono possibili e forse doverose alcune considerazioni : sempre opportuno e talora indispensabile ( casi gravi , urgenze ) il colloquio verbale con i nostri pazienti ; the fact that the referring physician may object to this il fatto che non sempre il curante lo desideri non ci esime activity does not exempt us from this duty ; da questo dovere ; the real problem is mainly to find the time and to acquire il vero problema anzitutto quello di trovare il tempo e and maintain the best possible level of preparation . poi di avere e mantenere la migliore preparazione . preparation la preparazione this is based on two premisses : the first , concerning the radiologists personally , is that the consultation should be considered as an integral part of the examination and not as an added extra to be granted only under certain circumstances ; the other is to ensure that the patient understands that this consultation is his or her right and may prove very useful . 
it is also essential to : humbly read books or magazines that can help to adapt sono necessarie due premesse : la prima , che riguarda personalmente il medico radiologo , quella di considerare il colloquio verbale come parte integrante dellesame e non come un di pi che pu essere concesso solo in determinate circostanze e laltra quella di far comprendere al paziente che tale colloquio un suo diritto e pu essere per lui di grande utilit . 
 time il tempo this is the main problem with one major premiss : it is clear that the radiologist rarely has the time or opportunity to talk to every patient , and this often imposes the difficult choice of whether to say very little to everyone ( or almost everyone ) or something in depth to those who need it most . 
 but which patients have the most need for verbal communication ? apart from the more serious and urgent cases , it is very difficult if not impossible to distinguish those who want to listen and talk from those who cannot wait to get back to their own doctor to talk to him or her , bearing in il principale problema con una sola importante premessa : evidente che ben raramente si ha il tempo e quindi la possibilit di parlare con tutti e sovente si imporr la difficile scelta se dire poco a tutti ( o quasi ) o qualcosa di pi a chi ne ha maggiormente bisogno . 
ma quale paziente ha maggiore bisogno del colloquio verbale ? a parte i casi pi gravi e quelli pi urgenti ben difficile se non impossibile riconoscere chi vorrebbe ascoltare e parlare e chi invece non aspetta che di ritornare dal suo medico per parlare con lui , ben consapevoli che anche il paziente con un radio1158 radiol med ( 2011 ) 116 : 11531160 fig . 
but why not discuss it with the radiologist ? the radiologist is a specialist physician who can guide you as to the most suitable diagnostic pathway for each medical condition . 
dialoga con lui , il confronto davvero importante ( societ italiana di radiologia medica )  . mind that the patient with a normal chest x - ray often needs to know the value and limitations of the examination , when ( or if ) it should be repeated , the risks associated with exposure to so many x - rays , and so forth . 
currently , the choice made in most areas of diagnostic imaging is to speak with those who need it most , although this choice , while often necessary , excludes many ( and all those who have a right to it ) from the possibility of a verbal consultation . 
it should , however , be noted that : gramma toracico normale ha sovente bisogno di conoscere il valore ed i limiti di tale indagine , quando la dovr eventualmente ripetere , se si prendono tanti raggi , ecc . 
 attualmente , la scelta concreta che viene fatta nella gran parte dei servizi di diagnostica per immagini quella di parlare con chi ne ha maggiormente bisogno , ma con tale scelta pur sovente necessaria si toglie a molti che lo desiderano ( e a tutti quegli altri che ne hanno un certo diritto ) la possibilit del colloquio verbale . 
va per ricordato che : radiol med ( 2011 ) 116 : 11531160 1159 the consultation may be deferred to a later date ( a phone number , as recommended in de santi and simeones book on the ideal consultation ) or just slightly delayed if this makes it possible ; it is not strictly necessary that the person reporting on the examination be the same one to engage in the consultation , which may certainly be carried out by a colleague ; it is important that there is a real possibility of a verbal consultation with the radiologist for each patient who wants one . a notice listing the radiologists availability ( as seen in every division of care ) , perhaps accompanied by the posters proposed by the italian society of medical radiology , ought to be displayed at the entrance to each diagnostic imaging department . 
this would be helpful both to remind the radiologist of his or her duty to communicate verbally with patients and to teach patients not to flee or ignore ( as happens not infrequently ) that specialist who can and often wants to communicate numerous things to them . il colloquio verbale pu essere posticipato ( un numero di telefono , come si raccomandava in precedenza nel libro di de santi e simeoni [ 27 ] a proposito del colloquio ideale ) o anche solo differito di poco se questo lo rende possibile ; non strettamente necessario che sia lesecutore del referto ad avere il colloquio verbale con il paziente ma un collega certamente in grado di supplirlo ; importante che vi sia , per ogni paziente che lo desidera , la concreta possibilit del colloquio verbale con il medico radiologo . un cartello con una disponibilit oraria dei medici ( come avviene in ogni divisione di cura ) , magari accompagnato dalle figure proposte dalla sirm auspicabile possa essere affisso allingresso di ogni servizio di diagnostica per immagini . 
sar utile per ricordarci la necessit se non il dovere del colloquio verbale con i pazienti e sar utile a loro che impareranno a non pi sfuggire o ignorare ( come oggi non raramente avviene ) quello specialista che pu e sovente vuole dir loro tante cose . conclusions conclusioni i do not think that these simple musings of an old radiologist ( as i was going to title this short article ) about a problem of the past that has become highly relevant today can provide any easy solutions or resolve uncertainties . 
i do hope , however , that they may help raise awareness of the situation and provide a stimulus for debate in the search for possible and shared solutions . non penso che queste semplici considerazioni di un vecchio radiologo ( cos avevo intenzione di titolare questo breve articolo ) su un problema del passato e oggi pi che mai del presente possano indicare facili soluzioni n risolvere incertezze : spero possano essere unutile presa di coscienza di una realt ed uno stimolo al dibattito ed alla ricerca di soluzioni possibili e condivise . 
 conflict of interest none radiol med ( 2011 ) 116 : 1314 doi 10.1007 / s11547 - 011 - 0726 - 1 erratum adenomyosis : from the sign to the diagnosis . 
senologia clinica e screening mammografico , dipartimento di radiodiagnostica , apss , trento , italy 2dipartimento di radiodiagnostica , apss , trento , italy 3centro di prevenzione senologica ( cps ) , po marzana , ulss 20 , verona , italy 4crr , centro di riferimento regionale per lo screening mammografico , torino , italy correspondence to : s . 
 proportional incidence was determined according to breast cancers expected in the absence of screening , estimated on the basis of patients / year at risk and age - specific incidence . 
 the review of screening mammograms preceding ics was performed by an external ( three radiologists ) and an internal ( five radiologists ) panel and aimed at assessing the proportion of ic reviewed as screening errors . 
ic proportional incidence was 15.90% for the first year ( ec standard < 30% ) and 25.77% for the second year ( ec standard < 50% ) of the interval . 
at external review , 18.4% of cases were reviewed as screening errors ( identified by at least two of three reviewers ) , whereas at internal review ( identified by at least three of five reviewers ) it was 17.4% ( ec standard < 20% )  . 
la revisione dei radiogrammi di screening precedenti i ci stata operata da un panel di radiologi esterno ( 3 radiologi ) e uno interno ( 5 radiologi ) , per la definizione del tasso di ci valutati come errori di screening . 
il tasso proporzionale di ci stato del 15 , 90% nel primo anno dellintervallo ( standard ce < 30% ) e del 25 , 77 % nel secondo anno ( standard ce < 50% )  . 
alla revisione esterna , la frazione di casi rivalutati come errori di screening ( identificati da almeno 2 su 3 revisori ) stata del 18 , 4% : alla revisione interna ( almeno 3 su 5 revisori ) stata del 17 , 4% ( standard ce < 20% )  . 
lapparente equivalenza della revisione esterna e interna suggerisce che la seconda , certamente pi agevole , possa essere impiegata nella routine per la definizione di questo indicatore precoce di efficacia . keywords breast carcinoma diagnosis mammography screening interval cancers parole chiave carcinoma della mammella mammografia diagnosi screening carcinomi di intervallo introduction introduzione mammography screening for early diagnosis of breast cancer has proved effective in reducing breast cancer mortality rates and is recommended by the european community ( ec ) [ 1 ] and implemented in the entire italian territory following specific recommendations of the ministry of health [ 2 ]  . 
as the impact of single screening programmes on mortality rates cannot be determined in the short term , a variety of early indirect indicators of efficacy has been proposed and recommended [ 1 ] for early assessment of screening programme performance [ 3 ]  . 
among these , interval cancer ( ic ) frequency and review to assess screening false negatives are considered as the most reliable indicators of sensitivity and the best indirect indicators of efficacy [ 1 , 3 ]  . 
 the analysis of ic observed in the trento province mammography screening programme was carried out , with a methodology comparable with other italian studies [ 37 ] , based on assessing the proportional incidence of ic and the fraction of ic classified as screening errors at review . 
the results of such analyses are the objects of this report . materials and methods a population - based mammography screening programme was started in trento province in october 2000 , a preliminary 3 - month pilot study being carried out in the district of trento , with further extension to the entire province . 
the screening test was performed at six different sites in trento province , and reading was centralised at the trento screening unit using recommended double reading [ 8 ]  . 
 in 2005 film - screen mammography was abandoned and digital mammography was adopted [ direct ( full - field digital mammography ) at trento centre and indirect ( computer radiography ) at the other screening sites ]  . 
 lo screening mammografico per la diagnosi precoce del carcinoma mammario pratica di provata efficacia , correntemente raccomandata dalla comunit europea ( ce ) [ 1 ] e implementato in tutto il territorio italiano a seguito di raccomandazione del ministero della salute [ 2 ]  . 
vista limpossibilit di definire , sul breve termine , limpatto di un programma di screening sulla mortalit , sono stati suggeriti e raccomandati [ 1 ] una serie di indicatori indiretti di efficacia che consentano una valutazione precoce della performance del singolo programma [ 3 ]  . 
tra questi lanalisi della frequenza dei carcinomi di intervallo ( ci ) e la loro revisione , al fine di definire leventuale errore radiologico , sono considerati i migliori indicatori della sensibilit di un programma di screening e , quindi , indirettamente della sua efficacia [ 1 , 3 ]  . 
in analogia con precedenti esperienze italiane di una simile verifica [ 37 ] , nel programma di screening mammografico della provincia di trento stata effettuata lanalisi dei ci osservati , sia per il calcolo della incidenza proporzionale che per il tasso di errori di screening alla revisione . 
i risultati di tale analisi sono oggetto del presente lavoro . materiali e metodi lo screening mammografico in provincia di trento ha avuto inizio a ottobre del 2000 , con un primo studio pilota condotto per circa tre mesi nel distretto di trento ed in seguito con generalizzazione su tutto il territorio provinciale . 
lesame di screening stato eseguito in sei diverse sedi , dislocate nel territorio provinciale , con centralizzazione delle mammografie presso il presidio di trento dove sono state esaminate da parte di radiologi senologi dedicati secondo la raccomandata procedura della doppia lettura [ 8 ]  . 
dal 2005 dalla mammografia analogica si passati progressivamente alla mammografia digitale , diretta presso il distretto di trento ed indiretta in tutte le altre sedi . gli indicatori di performance del programma , regolarradiol med ( 2011 ) 116 : 12171225 1219 performance indicators for the screening programme are regularly provided , and are available online , to the national screening observatory [ 2 ]  . 
ic were identified by linking screening archives with those of the local cancer registry and the local pathology department and with hospital discharge records ( hdr ) provided by local health authorities . 
all histologically confirmed invasive breast cancers occurring within 2 years of a negative screening episode from 2001 to 2006 ( negative screening test or positive screening test with negative assessment ) were assumed as ic . 
considering that follow - up for ic identification was complete up to june 2008 , ic relative to 2006 screening are underestimated for the second year of the interval , and those relative to 2007 do not contribute to the proportional incidence in the second year of the interval . 
the estimate of expected cancers was obtained by multiplying patient age groups ( 5054 , 5559 , 6064 , 6569 ) by the age - specific breast cancer incidence for trento province , as provided by the local cancer registry and relative to 19962000 . the review of negative screening mammograms preceding ics was performed in a blinded modality [ 9 ] , as recommended by the ministry of health [ 10 ] , by adding negative controls ( at least one subsequent negative screening ) randomly drawn for screening archives and matched to ic with a 3 : 1 ratio . 
external independent review was carried out by a panel of three radiologists with varying screening experience ( fc > 9 years , af > 20 years , sc > 30 years )  . 
internal review was carried out by a panel of five radiologists actively involved in screening reading , with varying screening experience ( db 11 years , sdm 10 years , pt 7 years , cf 3 years , mv 1 year )  . 
the reviewer was requested to mark on a paper scheme of the four mente comunicati e desumibili on line dal sito dellosservatorio nazionale screening [ 2 ] per la survey del 2008 riportano una estensione corretta dell85 , 5% ( biennale 80 , 9% ) , una popolazione bersaglio di 26000 soggetti invitati e 19400 aderenti ( adesione grezza = 74 , 8% , corretta = 79 , 2% )  . 
sono stati considerati ci tutti i carcinomi invasivi di cui sia stata comprovata la diagnosi in data successiva ed entro due anni da una mammografia di screening con esito negativo ( o positivo con successivo approfondimento negativo ) eseguita nellambito del programma di screening da gennaio 2001 a dicembre 2006 . 
poich il follow - up per la identificazione dei ci completo a giugno 2008 , i ci relativi agli esami eseguiti nel 2006 sono sottostimati per il secondo anno dellintervallo , e quelli relativi agli esami eseguiti nel 2007 non contribuiscono alla incidenza relativa per il secondo anno . 
il numero dei ci osservati rispetto a quelli attesi in assenza di screening ha fornito lincidenza proporzionale di ci : i ci attesi sono stati determinati moltiplicando il numero di pazienti / anno per quinquenni di et ( 5054 , 5559 , 6064 , 6569 ) per lincidenza et specifica per carcinoma mammario nella provincia di trento fornita dal registro tumori locale e relativa al periodo 19962000 la revisione dei radiogrammi di screening negativi precedenti i ci stata fatta secondo la modalit della revisione cieca [ 9 ] , in ottemperanza alle raccomandazioni del ministero della salute [ 10 ] , con aggiunta di controlli negativi ( almeno un esame di screening successivo negativo ) tratti a random dal programma di screening e accoppiati in rapporto di tre controlli per ogni caso di ci . 
le immagini ( analogiche , relativamente al periodo in studio ) sono state montate su visori rotanti in modo casuale e il revisione stato chiamato a indicare leventuale anormalit mammografica meritevole di approfondimento su uno schema grafico delle quattro proiezioni mammografiche . 
 in the following evaluation of review results , the exact correspondence of the breast abnormality indicated by the reviewer and the actual site of cancer occurrence was verified for each ic . 
attribution to occult , minimal sign or screening error review categories was based on majority report , that is , if no , one or two to three reviewers ( external review ) or no , one to two or three to five reviewers ( internal review ) had marked the abnormality . results relative to ic proportional incidence and review were compared with ec guidelines [ 1 ] : recommended standards for proportional incidence are < 30% in the first year , < 50% in the second and < 40% on a biennial basis , whereas for ic review , < 20% of cases should be reviewed as screening error . 
observed differences were checked by the chi - square test , with statistical significance being set at p < 0.05. nella successiva valutazione dei risultati della revisione , leffettiva corrispondenza della alterazione mammografica indicata dal revisore con la sede esatta di comparsa della neoplasia stata verificata in tutti i casi di ci . 
lattribuzione alle categorie occulto , segni minimi e errore di screening avvenuta a maggioranza : per la revisione esterna combinando le tre revisioni , rispettivamente nel caso che nessuno , uno solo , o almeno due revisori avessero identificato il ci , e per la revisione interna combinando le cinque revisioni , rispettivamente nel caso che nessuno , 12 o 35 revisori avessero identificato il ci . i risultati in termini di incidenza proporzionale dei ci e della loro revisione sono stati confrontati con la letteratura e con gli standard raccomandati dalla ce [ 1 ] che prevedono per lincidenza proporzionale un massimo del 30% nel primo anno , del 50% nel secondo anno , e del 40% nel biennio rispetto alla incidenza attesa in assenza di screening e , per la revisione , un massimo del 20% dei casi revisionati attribuiti alla categoria errori di screening . 
le differenze osservate sono state valutate mediante il test chi quadrato , ponendo la significativit statistica a un livello di p < 0 , 005 . linkage to the cancer registry , pathology registry and hdr allowed identification of 101 ics during the study period . 
the corresponding sensitivity figures were 84.10% at 1 year , 64.33% at 2 years and 79.61% on a biennial basis . ic review considered a total of 434 cases ( 103 ic , 331 controls )  . 
a slightly higher number of ic compared with those considered to assess proportional incidence is explained by the fact that a few ic cases relative to calendar periods with no follow - up coverage were included in the review set . 
similarly , a slight excess of controls compared with the intended 3 : 1 ratio was retrieved from archives and left in the review set . results of the external review are shown in table 2 . 
overall , ic identified by two to three reviewers and thus classified as screening errors were 18.4% ( 19 / 103 ) , that is , below the maximum acceptable 20% standard recommended by the ec [ 1 ]  . 
lincidenza proporzionale relativa al primo anno dellintervallo risultata quindi del 15 , 90% ( 43 / 270 , 4 ) , quella relativa al secondo anno dellintervallo risultata del 25 , 77% ( 58 / 225 ) , e quella relativa al biennio del 20 , 39% ( 101 / 495 , 3 ) , in tutte le circostanze al di sotto dei valori massimi consentiti dalle raccomandazioni ce . 
il valori di sensibilit equivalenti sono dell84 , 10% a un anno , 64 , 33% a due anni e 79 , 61% nel biennio . la revisione dei ci ha riguardato un totale di 434 casi ( 103 ci e 331 controlli ) : il numero lievemente maggiore di ci rispetto a quelli valutati per il calcolo della incidenza proporzionale risulta dalla inclusione di tutti i ci osservati , anche relativi a periodi con follow - up incompleto . 
anche un lieve eccesso di controlli rispetto alla prevista ratio di 3 : 1 stato acquisito dagli archivi e lasciato nel set di revisione . i risultati della revisione esterna sono riportati nella tabella 2 . 
complessivamente i ci identificati da 2 o 3 lettori e quindi codificati come errori di screening sono stati il 18 , 4% ( 19 / 103 ) , quindi al di sotto del 20% , valore massimo accettabile seconde le raccomandazioni ce [ 1 ]  . 
overall , ic identified by three to five reviewers and thus classified as screening errors were 17.4% ( 18 / 103 ) , that is , below the maximum acceptable 20% standard recommended by the ec [ 1 ] and comparable to what was obtained at external review . 5 indica la probabilit di identificazione di ci di un richiamo ad approfondimento da parte di uno o pi revisori interni . 
complessivamente i ci identificati da 35 lettori e quindi codificati come errori di screening sono stati il 17 , 4% ( 18 / 103 ) , quindi al di sotto del 20% , valore massimo accettabile seconde le raccomandazioni ce [ 1 ] , un tasso non differente da quanto ottenuto con la revisione esterna . discussion this study was based on a sufficiently large series allowing for reliable analysis of ic within the mammography screening programme of trento province . 
the entire province is covered by a single department for breast cancer diagnosis , and symptomatic women referring to any hospital / district in the province and having a previous screening mammography are systematically referred to the central screening unit in trento for diagnostic assessment . 
 this condition definitely made ic identification easier , but the linkage of three archives ( cancer registry , pathology registries , hdr ) would have equally allowed for ic identification , particularly of those with no histological confirmation or those diagnosed / treated outside the province . 
 migration outside the province for treatment is very low , but the identification of cases treated elsewhere is guaranteed through the hdr archive , providing data with only a short delay after discharge . the estimate of cancers expected in the absence of screening appears reliable in this study , as it is based on a local official cancer registry , and the age - specific incidence data used were relative to the period immediately preceding the onset of the screening programme . 
the latter condition allows for a reliable estimate of cancer incidence in the absence of screening , as it excludes major long - term incidence temporal trends and takes into account spontaneous access to mammography available before screening onset . although the ec guidelines indicate that in situ carcinomas should be considered among ic , they cannot be included in the evaluation of the proportional incidence , which is based on the estimate of expected cancers . 
 thus , in situ carcinomas were excluded in order to allow discussione lo studio si basa su una casistica sufficientemente ampia da consentire una valutazione affidabile dei ci nellesperienza di screening della provincia di trento . 
tale centralizzazione garantisce che la donna sintomatica che si presenti in ogni distretto / ospedale diverso da trento , in presenza di una mammografia di screening precedente , venga sistematicamente inviata per gli approfondimenti presso il centro di riferimento . 
peraltro lincrocio dei tre archivi ( registro tumori , anatomia patologica , sdo ) , che garantisce lidentificazione anche di eventuali casi senza identificazione istologica o diagnosticati / trattati al di fuori della provincia , resta il riferimento informativo essenziale ed risultata pi che sufficiente . 
si sottolinea che la migrazione per la terapia verso altre regioni assai modesta in trentino ; anche in quei casi lidentificazione viene per lappunto garantita dalla verifica delle sdo che sono disponibili entro breve tempo dal ricovero . 
 la stima dei ci attesi in assenza di screening , nel nostro caso , appare affidabile sia perch basata su un registro tumori ufficiale , sia perch per lo studio sono stati utilizzati tassi et specifici di incidenza riferibili al periodo immediatamente precedente allo screening , garantendo quindi un quadro affidabile della incidenza attesa in assenza di un programma di screening organizzato : esso infatti esclude variazioni temporali di incidenza sul lungo termine , e tiene conto dellaccesso spontaneo alla mammografia disponibile prima dellavvento del programma di screening . nonostante le linee guida ce indichino che i ci comprendono anche i carcinomi in situ , questi ultimi non possono essere valutati nel calcolo della incidenza proporzionale che si basa sul calcolo dei carcinomi attesi , a loro volta derivati da registri di incidenza , che considerano sono i carcinomi invasivi . 
in situ carcinomas might have been included in the review , but we chose to limit it to invasive lesions : ( a ) for a better comparison with other italian experiences [ 37 ] adopting the same crite rion , and ( b ) as we assume that most in situ carcinomas detected within the interval are usually asymptomatic and identified by spontaneous annual early rescreening . 
 the review of screening mammograms preceding ics was carried out in a blind modality , which has been reported to be the most unbiased condition , better approaching the scenario in which a screening error could potentially occur [ 9 , 10 ]  . 
in fact , the recall rate was higher than in the everyday practice ( external review 5.210.3% ; internal review 5.111.4% ) though less elevated compared with other similar experiences [ 37 ]  . 
at external review , the choice of assuming as screening errors cases with two to three recalls is supported by a high probability of ic being detected and no significant difference between two or three recalls . 
similarly , assuming cases identified by one reviewer only as minimal sign ( a category that does not imply a diagnostic error ) is supported by the low probability of ic being detected in these cases , very similar to that of cases with no recall . 
based on the observed findings , performance of the screening programme was also satisfactory according to the rate of screening errors at review , which was within the limits recommended by the ec [ 1 ] at both external and internal review . overall , the results indicate that the trento province mammography screening programme has a good performance as to sensitivity based on observed ic , and this may predict a good efficacy in reducing breast cancer mortality rates . 
the beneficial effects of screening on mortality rates are visible only some years after screening onset [ 11 ] and bero potuto essere compresi nella revisione , ma abbiamo ritenuto di limitare questultima alle sole forme invasive sia per un migliore confronto con altre esperienze italiane , che hanno adottato lo stesso criterio [ 37 ] , sia anche nella convinzione che i carcinomi in situ diagnosticati nellintervallo , abitualmente asintomatici , siano per la maggior parte relativi alluso di una mammografia intermedia ( annuale ) , di impiego assai varabile nelle diverse realt , e che quindi possano costituire un confondente nella comparazione con altri scenari . 
 la performance del programma di screening in termini di incidenza proporzionale di ci del tutto soddisfacente , decisamente al di sotto dei limiti massimi consentiti dalle raccomandazioni ce . la revisione dei radiogrammi di screening negativi precedenti i ci stata fatta secondo la modalit della revisione cieca , che risulta essere la meno influenzata e la pi vicina alla condizione in cui si pu supporre sia stato commesso un errore diagnostico [ 9 , 10 ]  . 
inevitabilmente i revisori , consci comunque di condurre una revisione a posteriori , hanno probabilmente adottato una soglia di sospetto lievemente inferiore alla norma , come dimostrato dal tasso di richiamo ( revisione esterna = 5 , 2%10 , 3% ; revisione interna = 5 , 1% 11 , 4% ) , che pure risulta abbastanza contenuto in confronto di altre esperienze simili [ 37 ]  . 
 la scelta di attribuire la codifica di eventuale errore di screening non in base ad un unico revisore ma alla maggioranza di un panel di revisori derivata dal desiderio di fornire una valutazione pi bilanciata , dal momento che noto che il giudizio del singolo revisore soffre di una certa soggettivit , come dimostrato anche dalle modeste differenze riscontrate tra le revisioni di questo studio . 
nella revisione esterna , la scelta di codificare come errore di screening i casi nei quali il ci era stato individuato da almeno due lettori confortata dal fatto che la probabilit di identificazione di ci assai elevata e non differisce sia che due o tre revisori abbiano individuato il ci . 
parimenti , laver omologato a segni minimi , categoria che non configura un errore diagnostico , i casi con riconoscimento del ci da parte di un solo revisore confortato dal fatto che la probabilit di identificazione di ci non diverso dai casi negativi per tutti i revisori . 
in base ai risultati dello studio , anche il tasso di ci revisionati e considerati errore di screening risultato essere contenuto entro i limiti consentiti dalle raccomandazioni ce [ 1 ] ad entrambe le revisioni . complessivamente i risultati del presente studio dimostrano che il programma di screening mammografico della provincia di trento ha una buona performance quanto a sensibilit , stimata in base ai ci osservati , e questo consente di prevedere una efficacia altrettanto buona nel ridurre la mortalit per carcinoma della mammella , dato che tende ad essere osservabile con una certa latenza rispetto allinizio radiol med ( 2011 ) 116 : 12171225 1225 will be evaluated in a further study . 
comparison between the external and internal reviews showed similar results , which might suggest the adoption of an internal review , which is easier to implement on a local and regular basis , as a standard quality control procedure . del programma di screening [ 11 ] , ed attualmente in corso di valutazione . 
coronary angiography with multidetector - row computed tomography ( mdct - ca ) allows quantification of coronary artery stenosis with a high level of accuracy ; however , a better estimation of stenosis can be achieved by using appropriate reformatting filters , especially in stents and calcified segments . 
langiografia coronarica ( ac ) con tomografia computerizzata multistrato ( tcms ) permette di quantificare la stenosi delle arterie coronarie con un alto livello di accuratezza ; tuttavia una migliore stima della stenosi pu essere calcolata usando appropriati filtri di ricostruzione , soprattutto nei segmenti con stent o calcificazioni . 
filtri particolari possono aiutare a stimare meglio lesatta percentuale della stenosi . keywords multidetector ct coronary angiography kernel quantitative coronary angiography reformatting filter parole chiave angiografia coronarica - tcms kernel angiografia coronarica quantitativa filtri di ricostruzione introduction introduzione coronary angiography with multidetector - row computed tomography ( mdct - ca ) is a robust and accurate imaging technique for the noninvasive study of coronary arteries [ 1 ]  . 
the correct estimate of coronary artery stenosis is crucial for planning patient treatment from follow - up in cases of nonsignificant stenosis to by - pass surgery in cases of chronic total coronary artery occlusion [ 2 ]  . 
coronary artery evaluation is based on analysis of curved multiplanar reconstructions ( mpr ) , maximum intensity projection ( mip ) reconstructions and volume - rendered ( vr ) images . 
 these techniques , however , are subjective , being based on the quality of the examination and reconstructions obtained and , above all , operator experience [ 3 ]  . 
the objective discrimination of stenosis proves additionally difficult in cases of calcified plaque or coronary artery stents , where the blooming effect alters visualisation of the true lumen of the coronary artery segment . 
 a number of semiautomatic systems for identifying and evaluating stenosis [ quantitative computed tomography angiography ( qcta ) ] have been proposed as postprocessing techniques for objective quantification of stenosis . 
however , in cases in which the stenosis is accompanied by calcified plaque or stents , evaluation with normal convolution filters has been shown to be suboptimal or imprecise [ 5 , 7 ]  . 
 the aim of this study was to evaluate the accuracy of quantitatively estimating coronary artery stenosis using qcta with all available convolution filters . langiografia coronarica ( ac ) con tomografia computerizzata multistrato ( tcms ) rappresenta una valida ed accurata metodica imaging per lo studio non invasivo delle arterie coronarie [ 1 ]  . 
la corretta stima di stenosi coronarica di fondamentale importanza per determinare il destino terapeutico di un paziente dal follow - up in caso di stenosi non significative al by - pass in caso di occlusione totale cronica [ 2 ]  . 
attualmente la valutazione coronarica basata sulla analisi di ricostruzioni multiplanari curvilinee , ricostruzioni in proieizione multiplanare ( mip ) e volume rendering , tuttavia soggettiva , basata sulla qualit dellesame e delle ricostruzioni ottenute e soprattutto sullesperienza delloperatore [ 3 ]  . 
loggettiva discriminazione di stenosi risulta inoltre pi difficoltosa in caso di placche calcifiche o di stent coronarici a causa dellartefatto blooming che altera la percezione del lume vero del segmento arterioso ; per ovviare a tale fenomeno ci si avvale di riformattazioni con filtri di convoluzione specifici consigliati dalle case in modo da ridurre al minimo il blurring originato dal calcio o dalle maglie dello stent [ 46 ]  . 
 esistono sistemi semiautomatici di identificazione e valutazione delle stenosi definiti sistemi di analisi quantitativa computerizzata dei vasi ( qcta ) proposti come tecnica di post - processing per una quantificazione oggettiva del grado di stenosi ; tuttavia in caso di stenosi sostenuta da placche calcifiche o stent , la valutazione con i normali filtri di ricostruzione rimane subottimale o inesatta [ 5 , 7 ]  . 
 scopo del presente lavoro valutare laccuratezza diagnostica nella stima quantitativa di stenosi coronariche utilizzando il qcta con tutti i filtri di convoluzione disponibili . materials and methods study population materiali e metodi popolazione in studio the study population consisted of 17 consecutive patients ( 13 men and four women ; mean age 63.5 years ) who underwent mdct - ca due to suspected coronary artery disease sono stati valutati prospetticamente 17 pazienti consecutivi ( 13 maschi e 4 femmine , et media 63 , 5 anni ) sottoposti radiol med ( 2011 ) 116 : 12031216 1205 ( cad ) between 15 december 2009 and 29 june 2010 . 
all examinations were performed with a 64 - slice system ( brillance 64 , philips , best , the netherlands )  . a ac - tcms per sospetta patologia delle coronarie nel periodo compreso tra il 15 - 12 - 2009 e il 29 - 06 - 2010 . 
tutte le indagini sono state acquisite mediante apparecchiatura tc a 64 strati ( brilliance 64 , philips , best , paesi bassi )  . inclusion and exclusion criteria inclusion criteria were heart rate < 65 bpm and the ability to sustain a breath - hold for 1012 s . 
indications for the examination were an absence of critical cad in patients with atypical chest pain and low - to - medium pretest risk , disagreement between functional tests and patient symptoms and study of stent and bypass graft patency . 
exclusion criteria were refusal to provide informed consent , previous adverse reactions to iodinated contrast material , renal impairment ( creatininaemia > 120 mmol / l ) , pregnancy , respiratory insufficiency , unstable clinical condition or marked cardiac insufficiency , prior angioplasty or cardiac surgery and insufficient diagnostic quality of the data sets . 
the local ethics committee approved the study , and all patients examined provided informed consent . patient preparation patients with heart rate 65 bpm received 515 mg of atenolol intravenously immediately prior to the examination . 
patients were studied in the supine position during an inspiratory breath - hold from the level of the pulmonary arteries up to the proximal abdomen to include the base of the heart . 
in patients with bypass graft , the scan was extended cranially to cover the area from the initial portion of the aortic arch to the base of the heart . scan protocol we intravenously administered 80100 ml of nonionic iodinated contrast material ( iomeprol 400 mgi / ml , iomeron , bracco , milan , italy ) at a rate of 5 ml / s , followed by 40 ml of saline solution at the same speed . 
the contrast material was injected with a dual - head automatic injector ( stellant , medrad , pittsburgh , pa , usa ) into an antecubital vein through a 16 - gauge needle cannula . 
 acquisition and reconstruction parameters are summarised in table 1 [ 9 , 10 ]  . data processing images were retrospectively reconstructed with the ecggated technique [ 11 , 12 ] using data acquired during a single heart beat . 
data sets were reconstructed during the mid - / criteri di inclusione ed esclusione i criteri di inclusione per gli esami ac - tcms comprendevano un ritmo cardiaco < 65 battiti per minuto ( bpm ) e la capacit di trattenere lapnea inspiratoria per 1012 s . 
le indicazioni allesame erano rappresentate da : esclusione di coronaropatia critica in pazienti con dolore toracico atipico in pazienti a basso medio rischio pre - test , discordanza tra prove funzionali e sintomatologia del paziente , controllo perviet stent e by - pass . 
i criteri di esclusione erano rappresentati da : rifiuto al consenso informato per lo studio , precedenti reazioni avverse al mezzo di contrasto iodato , insufficienza renale , ( creatininemia > 120 mmol / l ) , gravidanza , insufficiente funzionalit respiratoria , condizioni cliniche instabili o marcata insufficienza cardiaca , precedente angioplastica o interventi cardiaci e qualit diagnostica insufficiente dei datasets . 
il comitato etico locale ha approvato lo studio e tutti i pazienti esaminati hanno fornito il consenso informato . preparazione del paziente in caso di frequenze cardiache uguali o superiori a 65 bpm , sono stati somministrati 515 mg di atenololo endovena ( ev ) immediatamente prima dellesecuzione dellesame . 
i pazienti sono stati studiati in posizione supina in apnea inspiratoria dal livello delle arterie polmonari fino alla porzione prossimale delladdome in modo tale da comprendere anche la base del cuore . 
in pazienti con bypass il limite della scansione stato innalzato cranialmente alla porzione iniziale dellarco aortico fino alla base del cuore . protocollo di scansione abbiamo somministrato per via endovenosa 80100 ml di mezzo di contrasto non ionico iodato ( iomeprol 400 mgl / ml , iomeron , bracco , milano , italia ) con un flusso di 5 ml / s , seguito da 40 ml di soluzione salina allo stesso flus so . 
il mezzo di contrasto stato introdotto tramite un iniettore automatico a doppia pompa ( stellant , medrad , pittsburgh , pa , usa ) connesso ad una vena antecubitale con unagocannula da 16 g . 
i parametri di acquisizione e di ricostruzione sono riassunti in tabella 1 [ 9 , 10 ]  . 1206 radiol med ( 2011 ) 116 : 12031216 end - diastolic phase , with reconstruction windows from 300 ms to 450 ms from the next r - wave or from 60% to 70% of the r - r interval . 
in cases with insufficient image quality ( three patients ) , additional reconstructions were done during the end - systolic phase ( from 25% to 35% of the r - r interval )  . 
in cases of slightly irregular heart rate , such as bundle - branch block or premature beats , temporal variability in the reconstruction phase was manually compensated with ecg gating . 
the inaccurate detection for rwaves was corrected , and the temporal windows applied to ectopic beats were eliminated , thus compensating the subsequent diastolic interval with one or more windows . 
all diagnostic data sets were then reconstructed from the raw data using the convolution filters available on our systems , with section thickness 0.9 mm , reconstruction increment 0.4 mm and field of view 250 mm . image analysis target lesions were identified for each patient . 
the following criteria were used to select target lesions : ( 1 ) presence of haemodynamically significant stenosis identified at conventional coronary angiography ( cca ) ; ( 2 ) presence of coronary artery stent ; ( 3 ) presence of borderline stenosis . 
the diameter and length of the lesion or stent was defined for each segment . image evaluation visual score data sets used for the score were those corresponding to the standard ( xcc ) in the optimal acquisition window . 
a range of values was obtained in the rotation elaborazione dei dati per la ricostruzione delle immagini stata utilizzata una tecnica retrospettica ecg - gated [ 11 , 12 ]  . 
i pacchetti di dati sono stati ricostruiti durante la fase meso - / tele - diastolica , con finestre di ricostruzione da - 300 ms fino a - 450 ms dalla successiva onda r o 60% fino a 70% dellintervallo r - r . 
in caso di qualit delle immagini non sufficiente ( 3 pazienti ) sono state eseguite ricostruzioni aggiuntive durante la fase tele - sistolica ( 25% fino a 35% dellintervallo r - r )  . 
 stato corretto il rilevamento non accurato delle onde r e sono state eliminate le finestre temporali applicate ai battiti ectopici , compensando il successivo intervallo diastolico con uno o pi finestre . 
lo spessore di sezione acquisito corrispondeva a 0 , 75 mm , con un incremento di ricostruzione di 0 , 4 mtutti i datasets sono stati filtrati con un kernel di ricostruzione medio - morbido . 
tutti i dataset diagnostici sono stati poi ricostruiti a partire dai dati grezzi mediante i filtri di convoluzione disponibili sulla nostra apparecchiatura con spessore di sezione di 0 , 9 mm e incremento di ricostruzione pari a 0 , 4 mm con campo di vista fisso a 250 mm . analisi delle immagini per ogni paziente sono state identificate le lesioni target . 
il criterio di selezione delle lesioni target era il seguente : ( 1 ) presenza di stenosi emodinamicamente significativa riscontrata in angiografia coronarica ; ( 2 ) presenza di stent coronarico ; ( 3 ) presenza di stenosi borderline al limite della significativit . 
per ogni segmento stato definito il calibro e la lunghezza della lesione o dello stent . valutazione delle immagini score visuale il dataset utilizzato per lo score corrispondeva a quello standard ( xcc ) nella finestra di acquisizione ottimale . 
per ogni lesione target stata effettuata una stima di stenosi visuale distinta secondo i criteri internazionali [ 3 , 14 ] : 0%20% : assenza di stenosi o irregolarit parietali ; 20%50% : stenosi non significativa ; 50%70% : stenosi significativa ; 70%100% : stenosi severa occludente o suboccludente . radiol med ( 2011 ) 116 : 12031216 1207 fig . 
1 ricostruzione mpr rettilinea dellarteria discendente anteriore con detezione automatica dei bordi del vaso con qcta ne differenti filtri di convoluzione , utilizzando 15 differenti filtri di ricostruzione da a in alto a sinistra a cd in basso a sinistra ; confronto con angiografia coronarica , in basso a destra . 
 of the main vessel , and these were recorded in absolute terms and later grouped into the stenosis categories described above . qcta conventional coronary angiography cca was performed within 15 days of the mdct - ca examination . 
on the basis of the per - segment analysis , an operator blinded to the mdct - ca findings identified the segments with stenosis between 20% and 70% , including cases of borderline stenosis in mdct - ca and subocclusive stenosis . 
nella rotazione del vaso principale stato ottenuto per ogni singola misurazione un range di valori che sono stati registrati in termini assoluti e successivamente raggruppati nelle categorie di stenosi sopra descritte . angiografia coronarica langiografia coronarica ( ca ) stata eseguita entro 15 1208 radiol med ( 2011 ) 116 : 12031216 table 1 scan parameters of 64 - slice multidetector - row computed tomography coronary angiography ( mdct - ca ) scan parameter detector collimation kilovolt milliampere / s rotation time tube modulation effective time resolution maximal time resolution effective spatial resolution pitch scan time ( interval 120140 mm ) reconstruction effective slice thickness ( mm ) increase reconstruction ( mm ) time window reconstruction cardiac field of view thoracic field of view reformatting filter / kernel contrast medium synchronisation technique region of interest trigger threshold pre - delay preparation time to delay volume flow rate time to contrast administration saline solution venous access 64 slice 0.6250 mm 8001 , 000 330 ms systolic 165 ms 87 ms 0.30.30.4 mm 12 s bolus tracking ascending aorta + 100 hu 10 s 45 s 80100 ml 5 ml / s 15 s 40 ml , 5 ml / s antecubital end diastolic and end systolic 180250 mm entire thorax section medium ( xcc ) quantitative coronary angiography the segments with stenosis were then studied with a software application for the quantitative study of coronary stenosis ( qca ) ( caas , pie medical , maastricht , the netherlands )  . 
the percentage of stenosis was recorded in absolute terms and then grouped in the categories described above . statistical analysis statistical analysis was performed using spss ( version 11.5 , chicago , il , usa 19892002 )  . 
sulla base di una analisi per segmento un operatore in cieco rispetto ai dati rilevati in ac - tcms ha identificato i segmenti con stenosi comprese tra 20% e 70% , comprendendo quindi stenosi borderline in ac - tcms e sub occludenti . 
il valore di stenosi stato poi raggruppato nelle categorie di stenosi sopra descritte . angiografia coronarica quantitativa i segmenti stenotici sono stati poi studiati mediante il software di calcolo quantitativo di stenosi coronarica ( caas , pie medical , maastricht , paesi bassi )  . 
la percentuale di stenosi stata registrata in termini assoluti e poi raggruppata nelle categorie di stenosi sopra descritte . analisi statistica lanalisi statistica stata ottenuta mediante spss ( versione 11.5 , chicago , illinois 19892002 )  . 
gli indici di correlazione tra le radiol med ( 2011 ) 116 : 12031216 1209 tabella 1 parametri di scansione nella angiografia coronarica con tomografia computerizzata ( tc ) 64 strati parametro di scansione detettori collimazione chilovolt milliamperes tempo di rotazione modulazione della tensione del tubo risoluzione temporale effettiva risoluzione temporale massima risoluzione spaziale effettiva pitch tempo di scansione ( intervallo 120140 mm ) ricostruzione spessore di fetta effettivo ( mm ) incremento di ricostruzione ( mm ) finestra temporale campo di vista cardiaco campo di vista torace filtro di convoluzione / kernel mezzo di contrasto tecnica di sincronizzazione roi soglia di attivazione della scansione pre - delay tempo di preparazione al delay volume flusso tempo di somministrazione del mdc soluzione salina accesso venoso tc 64 strati 0 , 6250 mm 8001000 330 ms sistolica 165 ms 87 ms 0 , 30 , 30 , 4 mm 12 s bolus tracking aorta ascendente + 100 hu 10 s 46 s 80100 ml 5 ml / s 15 s 40 ml , 5 ml / s antecubitale tele - diastolica e tele - sistolica 180250 mm lintera sezione del torace medio ( xcc ) roi , regione di interesse ; mdc , mezzo di contrasto the exception of one examination that suffered from motion artefacts at the site of the target lesion , thus precluding both evaluation with qcta and use of the 15 convolution filters available . 
the segments most frequently affected by stenosis and therefore most frequently analysed were the proximal ( 11 cases , 44% ) and intermediate ( four cases , 16% ) tracts of the left anterior descending coronary artery and the proximal ( six cases , 24% ) and intermediate ( four cases , 16% ) tracts of the right coronary artery . 
in particular , comparison between mdct - ca and qca for the 2050% category shows agreement in 83.3% of cases ; for the catdifferenti metodiche sono stati espressi mediante analisi di regressione lineare usando il coefficiente di correlazione di pearson . 
un valore di p inferiore o uguale a 0 , 05 stato considerato statisticamente significativo . risultati tutti gli esami sono risultati di qualit sufficiente per essere analizzati mediante quantificazione visuale ac - tcms , qcta , ac , qca fatta eccezione per un esame soggetto ad artefatti da movimento in corrispondenza della lesione target che non ha quindi permesso lo studio del segmento mediante qcta con i 15 filtri di convoluzione a disposizione . 
i segmenti pi frequentemente soggetti a stenosi e quindi pi frequentemente analizzati sono risultati essere il tratto prossimale ( 11 casi , 44% ) ed intermedio ( 4 casi , 16% ) dellarteria interventricolare anteriore e il tratto prossimale ( 6 casi , 24% ) ed intermedio dellarteria coronaria destra ( 4 casi , 16% )  . 
agreement between mdct - ca and qca was 100% in the per - category analysis of stenosis in both types of plaque risultata pari a 17 , 467 , 43 millimetri e il calibro medio del segmento analizzato stato pari a 2 , 6 mm0 , 91 . le lesioni target sono state distinte a seconda che la stenosi fosse sostenuta da una placca fibrolipidica ( 10 casi ) , mista / calcifica ( 7 casi ) o vi fosse uno stent ( 8 casi )  . 
considerando come standard di riferimento il qca secondo lanalisi per categorie di stenosi vi una concordanza globale del 100% , 0 , 859 , tra ac - tcms e qca . 
per - category comparison between qca and qcta of the various filters in the study of fibrofatty plaques alone showed a low correlation for filter e ( rho = 0.095 ) ; good but not excellent correlation for filters a , b , c , d , cc , ya and xcc ; and excellent correlation for filters cb , cd , xca , xcb and xcd . 
lagreement tra ac - tcms e qca del 100% nellanalisi di stenosi per categoria in entrambi i tipi di placca ( 0 , 700 ; p < 0 , 0001 )  . 
nel confronto per categorie tra qca e qcta dei vari filtri nello studio delle sole placche fibrolipidiche vi una bassa correlazione per il filtro e ( 0 , 095 ) , buona ma non eccellente per i filtri a , b , c , d , cc , ya , xcc , eccellente per i filtri cb , cd , xca , xcb , xcd . 
nel confronto per categorie tra qca e qcta dei vari filtri nello studio delle sole placche miste / calcifiche vi una bassa correlazione per i filtri e , ca , ya , xcc , una correlazione inversa per i filtri a , b , c , cb , cc , cd , xca , xcb , xcd , discreta per il filtro ca , buona ma non eccellente per i filtri d ( 0 , 453 )  . 
objective evaluation of stenosis is , however , fraught with even greater difficulties in cases of calcified plaques or coronary artery stents that cause the blooming artefact and alter the perception of the true lumen of the segment [ 2233 ]  . 
to avoid this phenomenon , the expert operator performs reformatting with specific convolution filters recommended by the system manufacturers in order to minimise blurring caused by the calcium or the stent mesh . 
this system , known as qcta , autonomously traces the outline of the vessel and the segment discussione lac - tcms rappresenta una valida ed accurata metodica di imaging per lo studio non invasivo delle arterie coronarie [ 1621 ]  . 
la corretta stima di stenosi coronarica di fondamentale importanza per determinare il destino terapeutico di un paziente dal follow - up in caso di stenosi non significative al by - pass in caso di occlusione totale cronica . 
la stima di stenosi coronarica ad oggi basata sulla valutazione visuale di ricostruzioni multiplanari curvilinee , ricostruzioni in proiezione di massima intensit ( mip ) e volume rendering che rappresentano le tipiche ricostruzioni di cui il radiologo si serve per linterpretazione dei vasi maggiori , per lidentificazione e la caratterizzazione delle stenosi coronariche . 
la oggettiva valutazione di stenosi risulta inoltre pi difficoltosa in caso di placche calcifiche o di stent coronarici a causa dellartefatto blooming che altera la percezione del lume vero del segmento [ 2233 ]  . 
loperatore esperto per ovviare a tale fenomeno si avvale di riformattazioni con filtri di convoluzione specifici consigliati dalle case in modo da ridurre al minimo il blurring originato dal calcio o dalle maglie dello stent . 
the software , in fact , depends on the initial image ; therefore , if the vessel is poorly enhanced or if the atheromatous plaque being studied is prevalently calcified , the software will provide relatively unreliable information . qcta has been proposed as a postprocessing technique for objective quantification of the degree of stenosis , but often in cases of stenosis characterised by calcified plaques or stents , evaluation with normal reconstruction pacchetto comprehensive cardiac in dotazione alla workstation della tcms brilliance 64 . 
tale software infatti dipendente dalla immagine iniziale e quindi se il vaso sar poco opacizzato o se la placca aterosclerotica in esame sar prevalentemente calcifica il software sar tratto in errore fornendo informazioni poco attendibili . il qcta viene proposto come tecnica di post processing che permetta una quantificazione oggettiva del grado di stenosi ma spesso in caso di stenosi sostenuta da placche calci1214 radiol med ( 2011 ) 116 : 12031216 filters is suboptimal or imprecise . 
the results obtained in the analysis of our patient population show that the visual score obtained with mdct - ca is completely reliable in cases of calcified plaque , fibrofatty plaque and coronary stents . 
the use of qcta is also valid in evaluating fibrofatty plaque and with certain filters ( in our case , ya ) , also for studying stents , but with correlation values far from those required for a broad use of the technique . 
the low correlation between stenosis values identified at qcta and at qca is even more evident in the study of calcified plaque and stents where the reconstruction filters normally recommended are not effective for the mathematical models of qcta that identify vessel edges . 
we did not perform this procedure in order to avoid introducing bias when comparing performances of the various filters associated with qcta , although this technique should always be applied in cases of calcified plaque or stents . 
 whereas vessel edge editing may be considered a source of bias in accurate software validation , it can contribute to limiting errors of overor underestimating the degree of stenosis if performed properly and can even provide data much closer to those produced by qca . 
our study shows that oscillation of absolute values of stenosis quantified by qcta with varying filters is greater in cases of calcified plaques or stents than in cases of fibrofatty plaques . 
only by using the particularly hard filters ya and yb ( without margin correction ) was stent margin evaluation optimal , although the correlation index was still quite far from the value achieved with the visual score . 
although qcta without vessel edge editing did not prove particularly effective in estimating stenosis , it has been reported that optimal quantitative evaluation of the degree of coronary artery stenosis can be achieved with vessel edge editing . 
indeed , an attenuation of in - stent hounsfield unit density of around 37% has been reported with nondedicated filters , thus compromising correct estimation , both visual and automatic , of in - stent restenosis [ 35 , 36 ]  . 
the appropriate filters for stents ( in our case , xcd ) significantly reduce the background noise and increase overall image quality , thus allowing a more objective estimation of stenosis [ 37 ]  . there are a number of limitations to our study . 
lutilizzo del qcta valido daltra parte nella valutazione di placche fibrolipidiche e con particolari filtri duri ( nel nostro caso ya ) anche per lo studio degli stent ma con valori di correlazione lontani da quelli attesi per un largo impiego della tecnica . 
la bassa correlazione tra i valori di stenosi riconosciuti al qcta e al qca risulta ancor pi evidente per lo studio delle placche calcifiche e degli stent dove i filtri di ricostruzione normalmente consigliati non sono efficaci per i modelli matematici di identificazione dei contorni propri del qcta . 
nel nostro studio non abbiamo effettuato tale procedimento in modo da non introdurre un bias nel confronto tra le performance dei vari filtri accoppiati al qcta ma una tecnica che deve essere sempre usata in caso di placca calcifica o stent . 
 lediting dei contorni dei vasi , se da una parte infatti costituisce un bias nella corretta validazione del software , se adeguatamente eseguito contribuisce a limitare lerrore di sovra o sottostima del grado di stenosi e addirittura si avvicina maggiormente ai dati forniti dal qca . 
anche nel nostro lavoro abbiamo rilevato come loscillazione dei valori assoluti di stenosi quantificata dal qcta con i vari filtri sia molto maggiore in caso di placca calcifica o stent rispetto alla placca fibrolipidica . 
solamente con il filtro ya e yb ( senza correzione dei bordi ) particolarmente duro viene ottenuta una valutazione dei bordi dello stent ottimale ma con un indice di correlazione sempre distante da quello espresso dallo score visuale . 
sebbene il qcta senza editing dei contorni del vaso non risulti particolarmente efficace nella stima di stenosi gi stato descritto come mediante editing dei bordi sia possibile una valutazione quantitativa ottimale del grado di stenosi coronarica . 
inoltre lutilizzo di appropriati filtri di convoluzione sempre consigliabile in caso di placche calcifiche e ancor di pi in caso di stent in quanto stato dimostrato come vi sia una attenuazione della densit hounsfield intrastent di circa il 37% con filtri non dedicati , inficiando quindi una corretta stima sia visuale sia automatica della restenosi intrastent [ 35 , 36 ]  . 
i filtri appropriati per stent ( nel nostro caso xcd ) riducono significativamente il rumore di fondo dei dataset incrementando la qualit dellimmagine globale e permettendo cos una stima pi obiettiva della stenosi [ 37 ]  . questo lavoro presenta alcuni limiti . 
 the accuracy of the technique is suboptimal , especially if no vessel edge editing is performed , particularly in cases of calcified plaques or stents . il qcta una metodica promettente per lo studio del grado di stenosi dei segmenti coronarici , e risulta pi efficace se basata su filtri di convoluzione appropriati . 
cademartiri1 , 2 1department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands 2department of radiology and cardiology , azienda ospedaliero - universitaria di parma , parma , italy 3department of radiology , sdn - irccs foundation , napoli , italy 4department of radiology , azienda ospedaliera s . 
cademartiri , department of radiology , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 0521 - 703516 , fax : + 39 - 0521 - 703630 , e - mail : filippocademartiri@gmail.com received : 18 may 2009 / accepted : 08 july 2009 / published online : 4 september 2011 springer - verlag 2011 abstract purpose . 
twenty - one patients with stable and 20 with unstable angina pectoris scheduled for conventional coronary angiography ( cca ) underwent msct - ca using a 64 - slice scanner offering a fast rotation time ( 330 ms ) and higher x - ray tube output ( 900 mas )  . 
to determine the msct coronary plaque burden , we assessed the extent ( number of diseased segments ) , size ( small or large ) , type ( calcific , noncalcific , mixed ) of plaque , its anatomic distribution and angiographic appearance in all available 2 - mm segments . 
ventuno pazienti con angina stabile e 20 pazienti con angina instabile , in attesa di eseguire langiografia coronarica convenzionale ( acc ) , sono stati sottoposti ad angiografia coronarica con tcms a 64 strati caratterizzata da un tempo di rotazione veloce ( 330 ms ) e da una pi elevata emissione del tubo radiogeno ( 900 mas )  . 
langiografia coronarica mediante tcms fornisce importanti informazioni riguardo il carico aterosclerotico coronarico nei pazienti con angina stabile ed instabile . parole chiave malattia coronarica imaging tomografia computerizzata multistrato coronarografia ecografia intra - coronarica introduction introduzione multislice computed tomography ( msct ) is a rapidly developing technique . 
the latest 64 - slice msct scanners have a higher x - ray tube rotation speed and allow scanning with a higher tube current , providing increased temporal resolution and contrast - to - noise ( cnr ) ratio when compared with previous - generation 16 - row scanners . 
preliminary in vivo and ex vivo studies using previous - generation 16 - row scanners showed that msct coronary imaging holds promise for detecting nonobstructive coronary plaques and allows identification of different plaque tissue components [ 38 ]  . 
these observations prompted us to evaluate the msct coronary plaque burden defined as presence , severity , distribution and type of coronary plaques using a 64 - slice msct scanner . 
la tcms a 64 strati di ultima generazione ha una pi elevata velocit di rotazione del tubo radiogeno e consente scansioni con maggiore intensit di corrente del tubo , che si traduce in una maggiore risoluzione spaziale e un miglior rapporto contrasto / rumore rispetto alla precedente generazione di tcms a 16 strati . 
studi preliminari in - vivo ed ex - vivo , condotti con la precedente generazione di tcms a 16 strati , hanno dimostrato che limaging coronarico mediante tcms risulta promettente nella rilevazione di placche coronariche non ostruttive e consente lidentificazione delle diverse componenti tissutali della placca stessa [ 38 ]  . 
queste osservazioni ci hanno spinto a valutare il carico aterosclerotico coronarico mediante tcms , definito come la presenza , la severit , la distribuzione ed il tipo di placche coronariche utilizzando uno scanner tcms a 64 strati . 
abbiamo confrontato questi risultati con quelli ottenuti con langiografia convenzionale e , in un sottogruppo di pazienti , con lecografia intra - coronarica ( icus )  . during a 3 - month period , 21 patients [ 17 men , four women ; mean age ( standard deviation ; sd ) 59.09.2 years ] with stable angina pectoris and 20 patients [ 15 men , 5 women , mean age ( sd ) 60.011.3 years ] with unstable angina pectoris underwent 64 - slice msct coronary angiography materiali e metodi soggetti durante un periodo di tre mesi , 21 pazienti ( 17 maschi , 4 femmine , et mediadeviazione standard [ ds ] = 59 , 09 , 2 ) 1176 radiol med ( 2011 ) 116 : 11741187 ( ca ) prior to diagnostic ca followed , in case of amenable lesions , by percutaneous coronary intervention . 
patients were eligible for inclusion if they were in sinus rhythm , had a heart rate of < 70 bpm ( spontaneously or - blocker induced ) and able to breath - hold for 20 s . 
exclusion criteria were known contrast allergy , significant renal dysfunction ( serum creatinine > 120 mmol / l ) , braunwald class ia , iia , iiia ( unstable angina caused by noncardiac illness ) and previous percutaneous or surgical revascularisation . 
in order of preference , the left anterior descending artery ( lad , n = 8 ) , right coronary artery ( rca , n = 4 ) or circumflex artery ( cx , n = 3 ) were selected . 
 the institutional review board of our centre approved the study , and all patients gave written informed consent . msct - ca all msct examinations were performed using a 64 - slice scanner ( sensation 64 cardiac , siemens , forchheim , germany ) equipped with a faster x - ray tube rotation time ( 330 ms ) and a higher tube output ( up to 900 mas )  . 
other scan parameters were : detector collimation 3220.6 mm , table feed 3.84 mm / rotation , tube voltage 120 kv ; no prospective x - ray tube modulation was applied . 
radiation exposure using this scan protocol was estimated as being between 15 and 21 msv ( male / female ) using dedicated software ( windose , institute of medical physics , erlangen , germany )  . 
patients with a prescan heart rate 65 bpm received a single oral dose of 100 mg metoprolol ( selokeen , astrazeneca pharmaceutics , uk ) 1 h before the scan . 
 a bolus of 100 ml of iodinated contrast material ( iomeron 400 , bracco , milan , italy ) followed by a saline bolus chaser of 40 ml was administered through an arm vein ( flow rate : 45 ml / s )  . 
data sets were reconstructed during different time points of the cardiac phase using a retrospective electrocardiographic ( ecg ) - gated reconstruction algorith this algorithm uses data of a single heart beat obtained in half gantry rotation time , resulting in a temporal resolution of up to 165 ms . 
 con angina pectoris stabile e 20 pazienti ( 15 maschi , 5 femmine , et mediads = 60 , 011 , 3 anni ) con angina pectoris instabile sono stati sottoposti ad angiografia coronarica mediante tcms a 64 strati prima dellesecuzione della coronarografia diagnostica , seguita , in presenza di lesioni suscettibili da trattare , da intervento coronarico percutaneo . 
i pazienti erano eleggibili per linclusione se erano in ritmo sinusale , con frequenza cardiaca < 70 battiti / minuto ( spontanea o indotta mediante somministrazione di beta - bloccanti ) e se erano in grado di trattenere lapnea per 20 secondi . 
 i criteri di esclusione sono stati la presenza di una nota allergia al mezzo di contrasto , una significativa disfunzione renale ( creatinina sierica > 120 mmol / l ) , classe ia , iia , iiia di braunwald ( angina instabile causata da patologia non cardiaca ) e precedente rivascolarizzazione percutanea o chirurgica . 
un sottogruppo di 15 pazienti ( angina stabile : 7 ; angina instabile : 8 ) sono stati sottoposti ad un esame icus di un vaso per cui non era programmato lintervento percutaneo . 
sono state selezionate , in ordine di preferenza , larteria coronaria discendente anteriore sinistra ( lad , n = 8 ) , larteria coronaria destra ( rca , n = 4 ) o larteria circonflessa ( cx , n = 3 )  . 
il comitato etico della nostra istituzione ha approvato lo studio e tutti i pazienti hanno fornito un consenso informato scritto . angiografia coronarica mediante tcms tutti gli esami tcms sono stati eseguiti utilizzando una tcms a 64 strati ( sensation 64 cardiac , siemens , forchheim , germania ) , dotata di una maggiore velocit di rotazione ( 330 ms ) e una pi elevata emissione ( fino a 900 mas ) del tubo radiogeno . 
altri parametri di scansione : collimazione del detettore 3220 , 6 mm , velocit del lettino 3 , 84 mm / rotation , voltaggio del tubo 120 kv , non stata applicata modulazione prospettica della corrente del tubo . 
lesposizione radiogena utilizzando questo protocollo di scansione stata stimata tra i 15 e i 21 msv ( uomo / donna ) usando un software dedicato ( windose , institute of medical physics , erlangen , germania )  . 
ai pazienti che presentavano allarrivo una frequenza cardiaca 65 battiti / minuto stata somministrata per via orale una dose singola di 100 mg di metoprololo ( selokeen , astrazeneca pharmaceutics , uk ) unora prima della scansione . 
 stato iniettato per via endovenosa attraverso una vena del braccio un bolo di 100 ml di mezzo di contrasto iodato ( iomeron 400 , bracco , milano , italia ) seguito da un bolo di 40 ml di soluzione fisiologica ( velocit dinfusione : 45 ml / s )  . 
i datasets ricostruiti allinterno della fase meso - telediastolica generalmente forniscono una qualit dimmagine quasi priva di artefatti da movimento , tuttavia , quando ritenuto necessario , sono state eseguite ricostruzioni in differenradiol med ( 2011 ) 116 : 11741187 1177 the diameters of all coronary segments and branches were measured using a quantitative ca ( qca ) algorithm ( caas , pie medical imaging , maastricht , the netherlands )  . 
 one observer , unaware of the msct results , classified these segments as normal ( no luminal encroachment ) , wall irregularities ( < 20% lumen narrowing ) , moderately diseased ( 20% to < 50% lumen narrowing ) or significantly diseased ( 50% lumen narrowing )  . 
 msct analysis : assessment of the coronary plaque burden in all available 2 - mm coronary segments to evaluate the msct coronary plaque burden , we assessed the extent , type , size and anatomic distribution of plaque along all segments 2 mm , including the main coronary arteries and 2 - mm side branches . 
interand intraobserver variability was calculated for plaque extent , type and size , and differences in stable and unstable patients were compared using the students t test ( p values < 0.05 were considered significant )  . 
the tip of the icus catheter was positioned at least 10 mm distal to the distal landmark , and an automated pullback ( speed 0.5 mm / s ) of the complete roi was performed . 
 tutti i datasets con il minor numero di artefatti da movimento sono stati analizzati su una workstation off - line ( mmwp , siemens , forchheim , germania )  . 
il diametro di tutti i segmenti coronarici e dei rami collaterali stato misurato utilizzando un algoritmo di angiografia coronarografica quantitativa ( qca ; caas , pie medical imaging , maastricht , olanda )  . 
un osservatore , non a conoscenza dei risultati dellesame tcms , ha classificato questi segmenti come normali ( assenza di ristringimento del lume ) , con irregolarit parietale ( restringimento del lume < 20% ) , con malattia moderata ( restringimento del lume 20%50% ) o con malattia significativa : restringimento del lume 50% . analisi tcms : valutazione del carico aterosclerotico coronarico in tutti i segmenti coronarici disponibili 2 mm per determinare il carico aterosclerotico coronarico mediante tcms , abbiamo valutato lestensione , il tipo , la dimensione e la distribuzione anatomica delle placche lungo tutti i segmenti 2 mm , includendo le arterie coronarie principali e i loro rami di calibro 2 mtutti i segmenti coronarici sono stati esaminati per identificare la placca utilizzando immagini multiplanari ricostruite su piani longitudinali e trasversali . 
due osservatori , in cieco rispetto ai risultati delle altre tecniche di imaging , hanno effettuato in modo indipendente tutte le analisi per la valutazione del carico aterosclerotico alla tcms . 
stata selezionata una regione di interesse ( roi ) sullangiogramma , dopo lidenti1178 radiol med ( 2011 ) 116 : 11741187 semiautomated vessel - tracking software package ( circulation , siemens , forchheim , germany ) was used to create a central lumen line throughout the roi . 
plaques with a ct density below the coronary lumen and above the adjacent epicardial fat were classified as noncalcific , whereas plaques with a ct density 130 hu were classified as calcific . 
precision of the overall parameters with respect to plaque detection was expressed with a 95% confidence interval ( ci )  . results fifty - six percent ( 23 / 41 ) of patients was on long - term - blockade . 
demographics of stable and unstable patients are listed in table 1 . evaluation of the msct coronary plaque burden and comparison with conventional angiography a total of 473 coronary segments 2 mm were assessed . 
noncalcific plaques were found in 32% ( 93 / 292 ) , calcific in 25% ( 73 / 292 ) and mixed in 43% ( 126 / 292 ) of diseased segments . 
la punta del catetere icus stata posizionata almeno 10 mm distalmente al repere distale ed stata eseguito un trascinamento retrogrado automatico del catetere ( velocit : 0 , 5 mm / s ) nellintera roi . 
per eseguire tutte le misurazioni icus , stato utilizzato un software precedentemente validato basato su immagini acquisite con gating retrospettivo ( curad , wijk bij duurstede , olanda ) [ 10 ]  . analisi tcms : valutazione delle placche coronariche in una roi selezionata e confronto con licus inizialmente la roi selezionata stata identificata sulle immagini acquisite mediante angiografia coronarica tcms . 
 un software semi - automatico di vessel - tracking ( circulation , siemens , forchheim , germania ) stato utilizzato per creare una linea centrale nel lume allinterno della roi selezionata . 
le placche con densit inferiore al lume coronarico e al tessuto adiposo epicardio adiacente sono state classificate come non calcifiche , mentre le placche con densit 130 unit hounsfield ( uh ) sono state classificate come calcifiche . 
leventuale disaccordo tra i due osservatori stato risolto con il consenso di entrambi in una sessione congiunta . la roi selezionata stata suddivisa in sezioni di 5 mm per confrontare i risultati della tcms e dellicus . 
sono stati considerati significativi valori di p < 0 , 05 bserver agreement regarding plaque extent was 78% and 82% , plaque type was 69% and 74% and plaque size was 70% and 72% , respectively . 
 overall , plaque was found in 71% ( 115 / 161 ) of proximal segments , in 71% ( 79 / 111 ) of mid segments and in 49% ( 98 / 201 ) of distal segments and side branches of the main coronary arteries [ left main ( lm ) , lad , cx , rca ]  . 
al 51% ( 21 / 41 ) stata somministrata una dose ( supplementare ) di beta - bloccanti poich prima della scansione tc presentava una frequenza cardiaca superiore ai 70 battiti / minuto . 
la frequenza cardiaca mediads durante la procedure di scansione in pazienti con angina stabile ed instabile stata rispettivamente di 57 , 02 , 8 e 60 , 711 , 3 . 
i dati demografici dei pazienti con angina stabile ed instabile sono elencati nella tabella 1 . valutazione del carico aterosclerotico coronarico alla tcms e confronto con langiografia convenzionale per la valutazione del carico aterosclerotico coronarico alla tcms stato incluso un totale di 473 segmenti coronarici 2 millimetri . 
placche non calcifiche sono stati riscontrate nel 32% ( 93 / 292 ) dei segmenti malati , placche calcifiche nel 25% ( 73 / 292 ) e placche miste nel 43% ( 126 / 292 )  . 
i valori k per il grado di accordo inter - e intra - osservatore sono stati rispettivamente del 78% e 82% per lestensione delle placche , del 69% e 74% per il tipo di placca e del 70% e 72% per le dimensioni di placca . 
 lestensione , il tipo , le dimensioni , e relativa frequenza dei diversi tipi di placca per vaso coronarico nei pazienti con angina stabile ed instabile sono riportati nella tabella 2 . 
nel complesso , sono state riscontrate placche ateromasiche nel 71% ( 115 / 161 ) dei segmenti prossimali , nel 71% ( 79 / 111 ) dei segmenti medi e nel 49% ( 98 / 201 ) dei segmenti distali e rami collaterali delle arterie coronarie principali ( tronco comune [ lm ] , lad , cx e rca )  . 
inoltre , la presenza di placca stata rilevata nel 33% dei segmenti coronarici classificati come normali allangiografia convenzionale , mentre le irregolarit parietali allangiografia erano associate con il 72% ( 98 / 138 ) dei segmenti che alla tcms presentavano una placca coronarica . 
in general , large plaques were more frequently found in segments with more luminal encroachment on the conventional angiograplaque was detected in nearly all ( 99% , 126 / 128 ) coronary segments performance diagnostiche della tcms vs . 
licus nel rilevare placche significative in una roi selezionata un totale di 92 sezioni ( ognuna di 5 mm ) sono state incluse per il confronto tra tcms e icus . 
cx , arteria coronaria circonflessa ; d1 , primo ramo diagonale ; lad , arteria coronaria discendente anteriore sinistra ; lm , tronco comune ; pda , arteria coronaria discendente posteriore ; prox , prossimale ; rca , arteria coronaria destra . with nonsignificant or significant stenoses . 
as well as in 33% of coronary segments classified as normal with cca ; angiographic wall irregularities were associated with 72% ( 98 / 138 ) of the segments with msct coronary plaque involvement . 
nel complesso , la sensibilit e la specificit dellangiografia coronarica mediante tcms nel rilevare placche coronariche significative sono state rispettivamente dell83% ( 25 / 30 , 95% intervallo di confidenza [ ci ] : 65% 95% ) e 87% ( 54 / 62 , 95% ci : 76%94% )  . 
la sensibilit stata maggiore nei segmenti contenenti una componente calcifica di placca ( placche calcifiche : 91% [ 10 / 11 , 95% ci : 58%97% ] , placche miste : 82% [ 9 / 11 , 95% ci : 48%95% ] ) rispetto ai segmenti con placche costituite da componente esclusivamente non calcifica ( placche non calcifiche : 75% [ 6 / 8 , 95% ci : 34%93% ] )  . 
un esempio che mostra un confronto tra i risultati tcms e icus mostrato in figura 3 . radiol med ( 2011 ) 116 : 11741187 1183 table 4 diagnostic accuracy of multislice computed tomography coronary angiography for detecting coronary plaques compared with intracoronary ultrasound noncalcific calcific mixed overall true positive false positive false negative true negative sensitivity specificity 6 / 8 : 75% ( 3493% ) 10 / 11 : 91% ( 5897% ) 9 / 11 : 82% ( 4895% ) 25 / 30 : 83% ( 6595% ) 54 / 62 : 87% ( 7694% ) tabella 4 accuratezza diagnostica dellangiografia coronarica mediante tcms nellidentificazione delle placche coronariche a confronto con licus non calcifiche calcifiche miste totale veri positivi falsi positivi falsi negativi veri negativi sensibilit specificit 6 / 8 : 75% ( 3493% ) 10 / 11 : 91% ( 5897% ) 9 / 11 : 82% ( 4895% ) 25 / 30 : 83% ( 6595% ) 54 / 62 : 87% ( 7694% ) coronary plaques was 83% ( 25 / 30 , 95% ci 6595% ) and 87% ( 54 / 62 , 95% ci 7694% ) , respectively . 
a higher sensitivity was found in segments containing calcific plaque tissue [ 91% ( 10 / 11 , 95% ci 5897% ) , mixed plaques 82% ( 9 / 11 , 95% ci 4895% ) ] compared with segments with exclusively noncalcific plaque tissue [ 75% ( 6 / 8 , 95% ci 3493% ) ]  . 
a comparison between msct and icus findings is shown in figure 3 . discussion coronary atherosclerosis begins early in life , and it takes several decades for plaques to advance into vulnerable plaques that underlie progression to acute coronary syndromes ( unstable angina pectoris or myocardial infarction ) or progression of coronary stenosis . 
sixtyfour - slice msct - ca has a nearly isotropic submillimetre discussione laterosclerosi coronarica inizia a svilupparsi in et precoce e levoluzione in placche vulnerabili , che sono alla base dello sviluppo di sindromi coronariche acute ( angina pectoris instabile o infarto miocardico ) o la progressione della placca in stenosi coronarica sono processi che richiedono diversi decenni . 
di conseguenza , gli esami icus sono di solito limitati ai tratti prossimali e medi di una sola arteria coronaria , precludendo in tal modo la valutazione del carico aterosclerotico complessivo coronarico . 
questo ha incoraggiato il bisogno di tecniche di imaging non invasive in grado di valutare le placche coronariche , ad esempio la risonanza magnetica nucleare ( rmn ) e la tcms . 
langiografia coronarica mediante tcms a 64 strati ha una risoluzione spaziale sub - millimetrica quasi isotropica che permette la valutazione della parete vasale in tutti i segmenti coronarici 2 mm , fornendo cos una valutazione pi completa , rispetto allicus , dellaterosclerosi coronarica in tutto lalbero coronarico . nel nostro studio abbiamo dimostrato che langiografia coronarica mediante tcms in grado di valutare la presenza , lestensione , la severit , la distribuzione e il tipo di placche coronariche . 
abbiamo riscontrato una elevata sensibilit e specificit ( rispettivamente del 83% e dell87% ) della tcms nel rilevare placche coronariche significative a confronto con licus , dati in linea con gli studi prece1184 radiol med ( 2011 ) 116 : 11741187 fig . 
3 maximum intensity projected computed tomography ( mip - ct ) image showing a nonsignificant obstructive coronary lesion located at the midsection of the right coronary artery ( rca ) , which was also found on the conventional coronary angiogram ( cca )  . 
cross - sectional ct images at the lesion site demonstrate the presence of a large , mixed plaque with both calcific ( a1 ) and noncalcific ( b1 ) plaque tissue , which was confirmed with intracoronary ultrasound ( a2 and b2 )  . 
3 immagine tc di proiezione di massima intensit che mostra una lesione coronarica ostruttiva non significativa localizzata nel tratto medio dellarteria coronaria destra ( rca ) , riscontrata anche allangiografia coronarica convenzionale ( acc )  . 
immagini tc trasversali in corrispondenza della lesione dimostrano la presenza di unestesa placca mista con entrambe le componenti tissutali calcifiche ( riquadro a1 ) e non calcifiche ( riquadro b1 ) , che stata confermata allecografia intra - coronarica ( riquadri a2 e b2 )  . spatial resolution that allows evaluation of the coronary vessel wall in all 2 - mm coronary segments , thereby providing a more comprehensive evaluation compared with icus of coronary atherosclerosis throughout the coronary tree . 
we found a high sensitivity and specificity ( 83% and 87% , respectively ) compared with icus , which is in line with previously published studies [ 6 , 7 ]  . 
this observation may be the result of improved image quality offered by 64 - slice msct scanners due to a higher x - ray tube current , which provides a more favourable cnr . 
 we evaluated the presence of coronary plaques in all available 2 mm coronary segments ( according to the aha classification ) and classified plaques into calcific , noncalcific and mixed [ 48 ]  . 
questo dato pu essere il risultato di una migliore qualit dellimmagine offerta dagli scanners tcms a 64 strati , grazie allapplicazione di una pi elevata corrente del tubo radiogeno che garantisce un miglior rapporto contrasto - rumore . 
in particolare , quando il rumore dellimmagine diventa pi evidente , possono non essere individuate piccole placche non calcifiche . abbiamo valutato la presenza di placche coronariche in tutti i segmenti coronarici disponibili 2mm ( secondo la classificazione dellaha ) e abbiamo classificato le placche come calcifiche , non calcifiche e miste [ 48 ]  . 
stato interessante notare che un terzo delle placche erano non calcifiche e che circa il 40% delle placche era costituito da tessuto non calcifico , mentre il 25% delle placche erano prevalentemente calcifiche . 
preliminary in vivo studies suggest that plaques with predominantly lipid or fibrous tissue could be distinguished on the basis of tissue density differences ( in hounsfield units ) with msct when comparing these tissue - density values ( low , moderate ) with the degree of tissue echogenicity ( hypoor hyperechogenicity ) with icus [ 3 , 5 , 7 , 8 ]  . 
however , classifying noncalcified plaques is limited by high variability in density values within a single plaque , which makes it difficult to reliably distinguish between lipid and fibrous plaque tissue . 
furthermore , distinction between different plaque tissues on the basis of density values is hampered due to partial voluming and interpolation , which may improve when scanners with higher spatial resolution become available [ 11 ]  . plaque extent and distribution was almost similar in stable and unstable patients , but we found significantly more noncalcified plaques in patients with unstable vs . 
 we also demonstrated that coronary plaques were most frequently located in the proximal and mid segments of the large coronary arteries [ lad , left circumflex ( lcx ) , rca ] , as has been demonstrated in earlier pathologic and icus studies . 
 in addition to previous studies , we evaluated the angiographic appearance of coronary plaques detected by msct and found that coronary atherosclerosis was present in one third of angiographically normal coronary arteries , indicating that msct is able to detect earlier stages of coronary artery disease when compared with cca . 
more specifically , plaques without encroachment of the coronary lumen due to compensatory outward remodelling of the vessel wall , thereby alleviating reduction of luminal size ( known as positive remodelling ) remain undetected by cca but have been associated with acute coronary syndromes . 
tuttavia , la classificazione delle placche non calcifiche limitata dallelevata variabilit intraplacca dei valori di densit nel contesto di una singola lesione , che rende difficile distinguere in maniera affidabile tra componente lipidica e fibrosa della placca . 
inoltre , la distinzione tra differenti componenti tissutali della placca sulla base dei valori di densit ostacolata da effetti di volume parziale ed interpolazione , che potranno ridursi con la disponibilit di scanners con maggiore risoluzione spaziale [ 11 ]  . lestensione e la distribuzione delle placche erano pressoch simili nei pazienti con angina stabile ed instabile , tuttavia abbiamo riscontrato una prevalenza significativamente pi elevata di placche non calcifiche nei pazienti con angina pectoris instabile vs . 
 [ 12 ] che ha riscontrato un numero significativamente maggiore di placche non calcifiche nei pazienti con infarto miocardico acuto rispetto ai pazienti con angina stabile [ 1216 ]  . 
tuttavia , da questi risultati non deve derivare linterpretazione che i pazienti con prevalenza di placche calcifiche siano meno vulnerabili , o che una placca calcifica sia stabile . abbiamo inoltre dimostrato che le placche coronariche interessavano pi frequentemente i segmenti medio - prossimali delle principali arterie coronarie ( lad , lcx e rca ) , come stato anche dimostrato in precedenti studi anatomopatologici e mediante icus . in aggiunta rispetto a studi precedenti , abbiamo inoltre valutato laspetto angiografico delle placche coronariche rilevate dalla tcms . 
abbiamo riscontrato che laterosclerosi coronarica era presente in un terzo delle arterie coronarie angiograficamente normali , dimostrando che la tcms in grado di identificare la malattia coronarica in stadi pi precoci rispetto alla coronarografia convenzionale . 
nello specifico , le placche che non impegnano il lume coronarico a causa del rimodellamento compensatorio verso lesterno della parete del vaso , che contrasta la riduzione del diametro luminale ( noto come rimodellamento positivo ) , non vengono rilevate allangiografia convenzionale , tuttavia sono state associate allo sviluppo di sindromi coronariche acute . il nostro studio dimostra che la valutazione del carico aterosclerotico coronarico mediante tcms fornisce importanti informazioni sulla presenza e lestensione dellaterosclerosi coronarica nei pazienti con angina pectoris stabile e instabile . 
ulteriori studi prospettici sono necessari per determinare se la valutazione del carico aterosclerotico coronarico mediante tcms abbia un valore prognostico nellidentificazione di pazienti a rischio di futuri eventi cardiaci . limiti nel nostro studio stata studiata una popolazione di pazienti relativamente ristretta e sono stati inclusi pazienti con ritmo cardiaco lento e regolare , che sono variabili che 1186 limitations we studied a relatively small patient population and included patients with a low and regular heart rhythm , which are variables of high - quality msct imaging . 
it should be noted that the diagnostic performance of msct was compared with the presence of a coronary plaque that had a minimum thickness of 1 mm as determined with icus , excluding smaller plaques from the analysis . 
 although these plaques were not associated with significant coronary lumen obstructions , they should be classified as advanced plaques according to the pathological classification described by stary [ 17 ]  . 
a serious concern is the high radiation exposure during msct - ca , which is estimated as being between 15 and 21 msv ( male / female ) using this scan protocol . 
radiation exposure can be reduced by technical adjustments , such as prospective x - ray tube - current modulation , which reduces radiation exposure by nearly 50% in patients with low heart rates . 
 however , we did not apply this feature because it limits image reconstruction during the early diastolic phase , which can be important for evaluating the rca [ 1 ]  . 
deve essere notato che nel nostro studio la performance diagnostica della tcms stata confrontata con la presenza allesame icus di placche coronariche con spessore minimo di 1 mm , escludendo dallanalisi le placche di dimensioni inferiori . 
sebbene queste placche non erano associate ad una ostruzione significativa del lume coronarico , dovrebbero essere classificate come placche avanzate secondo la classificazione patologica descritta da stary [ 17 ]  . 
questi risultati suggeriscono che la tcms non sia in grado di rilevare gli stadi pi precoci dellaterosclerosi coronarica , che sono associati alla presenza di placche non - calcifiche di piccole di dimensioni . 
un problema rilevante lesposizione ad alte dosi di radiazioni durante langiografia coronarica mediante tcms , stimata tra i 1521 msv ( maschi / femmine ) utilizzando questo protocollo di scansione . 
lesposizione alle radiazioni pu essere ridotta da alcuni adattamenti tecnici come la modulazione prospettica della corrente del tubo radiogeno , che riduce lesposizione alle radiazioni di circa il 50% nei pazienti con bassa frequenza cardiaca . 
tuttavia , non abbiamo applicato questa tecnica perch non consente la ricostruzione delle immagini durante la fase proto - diastolica , che pu essere importante per la valutazione della rca [ 1 ]  . 
 the aim of this pictorial review is to analyse the features of adenomyosis by illustrating the most usual and typical imaging patterns , along with the unusual appearances , seen in a vast array of gynaecological imaging modalities . 
 the different findings of focal and diffuse adenomyosis along with the diagnostic limitations of ultrasound , hysterosalpingography and magnetic resonance imaging are described , as are the pitfalls and differential diagnosis with other pathological conditions that are often misdiagnosed as adenomyosis . 
the role of the different imaging modalities in planning appropriate treatment and their usefulness in monitoring therapy are also discussed . keywords female pelvic pain infertility magnetic resonance imaging transvaginal ultrasound hysterosalpingography riassunto ladenomiosi caratterizzata dallinvasione benigna del miometrio da parte dellendometrio ed spesso sottostimata o diagnosticata con ritardo , nonostante sia invalidante in quanto possibile causa di menorragia , metrorragia , dismenorrea ed infertilit . 
lo scopo del lavoro quello di analizzare gli aspetti diagnostici delladenomiosi mostrando i quadri pi semplici e quelli pi rari e difficili da caratterizzare , raccolti in una ampia galleria che prende in esame tutte le pi note tecniche di imaging ginecologico . 
i limiti e possibilit delle varie tecniche di imaging , ecografia , isterosalpingografia e risonanza magnetica , saranno illustrate ponendo anche particolare attenzione alla diagnostica differenziale con le altre forme morbose pi facilmente equivocabili . 
sar infine discusso il ruolo delle metodiche di imaging nella pianificazione del tipo di trattamento e nel monitoraggio dellefficacia terapeutica . parole chiave dolore pelvico infertilit risonanza magnetica ecografia transvaginale isterosalpingografia 1268 introduction adenomyosis is the benign , non - neoplastic infiltration of the endometrium into the myometrium characterised by ectopic glands and stroma , surrounded by hypertrophic and hyperplastic myometrium [ 1 ]  . 
therefore , the haemorrhagic foci that characterise endometriosis ( patches of ectopic endometrial tissue ) and which are helpful in identifying this disease may not be present in adenomyosis , thus making characterisation difficult [ 2 ]  . 
risk factors for adenomyosis are essentially related to : ( 1 ) reproductive activity , with an increased risk in multiparity , miscarriage and endometriosis ; ( 2 ) lifestyle factors such as smoking ; and ( 3 ) surgical trauma such as caesarean section , induced abortion or curettage [ 4 ]  . 
around 20% of cases of adenomyosis involve women of reproductive age ( < 40 years ) : the remaining 80% of cases involve women between 40 and 50 years , and the most severe symptoms are associated with this age group . 
 the aim of this paper is to illustrate the typical imaging characteristics and the less common and more insidious appearances of adenomyosis , as well as discuss the role of the different imaging modalities and their diagnostic contribution , with particular reference to transvaginal ultrasound ( tvus ) , hysterosalpingography ( hsg ) and magnetic resonance ( mr ) imaging . 
by presenting a series of cases , some of which are illustrated with combined imaging , the fundamental radiological signs useful for the diagnosis are analysed , along with possible diagnostic pitfalls and differential diagnosis . 
traditional and more recent treatment approaches are also described , with reference to the need for a thorough preliminary diagnostic assessment for treatment planning and the utility of imaging in monitoring treatment effectiveness . radiol med ( 2011 ) 116 : 12671287 introduzione viene definita adenomiosi linvasione benigna , non neoplastica , del miometrio da parte dellendometrio caratterizzata da ectopia di ghiandole e stroma , circondati da miometrio ipertrofico e iperplastico [ 1 ]  . 
pertanto , i foci emorragici che caratterizzano lendometriosi ( zolle di tessuto endometriale in sede ectopica ) e che sono di aiuto nellidentificazione di tale patologia , possono non essere presenti nelladenomiosi con conseguenti possibili difficolt di tipizzazione [ 2 ]  . 
 i fattori di rischio delladenomiosi sono essenzialmente legati : ( 1 ) allattivit riproduttiva , con incremento del rischio di adenomiosi nella pluriparit , aborti spontanei ed endometriosi ; ( 2 ) alle abitudini di vita quali il fumo ; ( 3 ) ai traumi chirurgici quali parti cesarei , aborti indotti o raschiamenti [ 4 ]  . 
la presentazione clinica poliforme : in circa 1 / 3 dei casi , ladenomiosi completamente asintomatica ; nei restanti 2 / 3 i sintomi pi frequenti sono la menorragia ( 50% ) , la dismenorrea ( 30% ) e la metrorragia ( 20% ) ; si rilevano anche dispareunia ed infertilit [ 2 , 6 ]  . 
questa patologia interessa nel 20% dei casi donne in et fertile , di et inferiore ai 39 anni , mentre nell80% dei casi sono affette donne tra i 40 e 50 anni , e in questo intervallo di et sono associati i sintomi pi severi . 
 scopo del presente articolo illustrare limaging tipico e i quadri meno usuali e pi insidiosi di adenomiosi di scutendo il ruolo delle differenti metodiche e il loro ap porto diagnostico , con particolare riferimento allecogra fa transvaginale ( etv ) , allisterosalpingografia ( isg ) e alla risonanza magnetica ( rm )  . 
attraverso una serie di casi , illustrati talora con imaging integrato , saran no analizzati gli elementi di semeiotica elementare utili alla diagnosi , i possibili errori diagnostici e la diagno stica differenziale . 
verranno anche descritti i classici e pi recenti presidi terapeutici per la cui pianificazione consigliabile una attenta preliminare valutazione diagnostica , utile anche nel controllo dellefficacia del trattamento . radiol med ( 2011 ) 116 : 12671287 1269 histopathological considerations and introduction to imaging considerazioni istopatologiche e premesse allimaging the endometrium - myometrium junctional zone is usually irregular since the endometrial mucosa is directly joined to the underlying myometrium without interposition of the submucosa [ 7 ]  . 
therefore , in order to speak of adenomyosis and not physiological penetration , the endometrial tissue needs to extend at least 2.5 mm below the junctional zone [ 8 ] or for at least 25% of the myometrial thickness [ 2 ]  . 
 the diagnostic imaging appearances can be best understood by considering that adenomyosis in the uterus can be either diffuse or focal and that due to this variation , it may manifest with more or less insidious characteristics . in the diffuse form of adenomyosis the uterus appears enlarged and globular . 
the focal forms have a different appearance , which can be recognised as follows : the localised change in the myometrium at the level of one of the uterine walls , characterised by the same changes mentioned above , causes local enlargement , which in imaging is defined as pseudowidening ; the adenomyoma is a circumscribed and nodular aggregate of smooth muscle cells , endometrial glands and stroma , which can be identified in the myometrium ; adenomyoma may involve the endometrium by projecting into the cavity in the form of a polyp . 
in around 2% of cases , the appearance is one of an endometrial polyp when in fact the lesion is a polypoid adenomyoma [ 9 ] ; the adenomyotic cyst is the focal form in which there is significant haemorrhagic cavitation caused by repeated bleeding . the broad appearances of the diffuse and various focal forms can be visualised with the various imaging modalities . 
these lesions appear to be confined to the internal third of the cervical wall [ 10 ] and usually manifest in patients with a history of trauma ( curettage or biopsy ) or arise from residual mllerian tissue located in the cervical stroma . 
it is more appropriate to speak of cervical endometriosis rather than adenomyosis because the cervical mucosa is not strictly joined to the fibromuscular portion but is separated from it by the submucosa [ 7 ]  . 
pertanto , perch si possa parlare di adenomiosi , e non di penetrazione cosiddetta fisiologica , necessario che il tessuto endometriale si approfondi per almeno 2 , 5 mm al di sotto del tratto di giunzione [ 8 ] o penetri almeno il 25% dello spessore miometriale [ 2 ]  . 
per meglio comprendere gli aspetti dellimaging diagnostico bene ricordare che ladenomiosi pu interessare lutero in maniera diffusa o focale e che proprio per il suo polimorfismo pu manifestarsi con quadri pi o meno insidiosi . nella forma diffusa di adenomiosi lutero globoso , aumentato in toto in relazione alla presenza di miometrio globalmente ispessito per coesistenza di cisti ghiandolari e ipertrofia delle cellule muscolari lisce a distribuzione non ordinata ; le ghiandole e lo stroma delle zolle adenomiosiche sono spesso di tipo proliferativo [ 2 ]  . 
le forme focali hanno aspetti differenti , che vanno conosciuti : lalterazione del miometrio localizzata a livello di una delle pareti dellutero , caratterizzata dalle medesime alterazioni sopraelencate , provoca un ingrandimento settoriale che allimaging corrisponde a quello che in lingua inglese viene definito pseudowidening ; ladenomioma un circoscritto e nodulare aggregato di cellule muscolari lisce , ghiandole endometriali e stroma , identificabile nel contesto del miometrio ; ladenomioma pu coinvolgere lendometrio protrudendo in cavit sotto forma di polipo e quello che sembra un polipo endometriale in circa il 2% dei casi in realt un adenomioma polipoide [ 9 ] ; la cisti adenomiosica la forma focale in cui c ampia cavitazione emorragica , determinata da sanguinamenti ripetuti . gli aspetti fino ad ora considerati , quello diffuso e le varie differenti forme focali , hanno un corrispettivo nelle varie tecniche di imaging , talora di difficile caratterizzazione , che andremo a valutare di seguito nel dettaglio . 
illustreremo per completezza anche le localizzazioni del collo uterino , anche se in questo caso pi corretto parlare di endometriosi piuttosto che di adenomiosi ; queste appaiono confinate al terzo interno della parete cervicale [ 10 ] e solitamente si manifestano in pazienti con storia di traumi ( curettage o biopsie ) o insorgono su residui mlleriani allocati nello stroma cervicale . 
si parla di endometriosi cervicale e non di adenomiosi perch la mucosa del collo non strettamente congiunta alla porzione fibro - muscolare ma da essa separata mediante la sottomucosa [ 7 ]  . 
 1270 radiol med ( 2011 ) 116 : 12671287 diagnostic imaging and fundamental radiological signs imaging diagnostico e semeiotica elementare not always is diagnostic imaging prompted by the clinical suspicion of adenomyosis . 
nonetheless , mr imaging is particularly useful both in supplementing doubtful tvus cases and in providing a complete evaluation of the disease , thanks to its high contrast resolution , its ability to characterise lesions with blood and fat content and its panoramic views . 
 for example , in cases of pelvic pain that may be a result of adenomyosis or many other causes , tvus is the first - line technique able to raise the diagnostic suspicion of adenomyosis . 
similarly , infertility may prompt imaging workup , and the suspicion of adenomyosis may also be based on hsg , which is traditionally requested in these cases . transvaginal ultrasound the tvus diagnosis of adenomyosis in b - mode is based on changes to the echostructure , which are readily recognised with the intracavitary study and which reflect histological changes . 
the fundamental tvus signs include : increased myometrial echogenicity or linear hyperechoic bands extending deep into the myometrium , which indicates the presence of islets of ectopic endometrial tissue ; hypoechoic areas in the myometrium compatible with hyperplasia of the muscle tissue surrounding the ectopic tissue ; anechoic areas due to glandular dilatation or myometrial cysts ; poor definition of the junctional zone ; enlargement of the uterus with asymmetrical thickening of one of the walls ( pseudowidening )  . finding at least three of these signs is highly suggestive of adenomyosis [ 11 ]  . 
colour or power doppler tvus may reveal hypervascularity in the case of diffuse or focal adenomyosis , but above all it provides important information regarding the course of the non sempre il sospetto clinico di adenomiosi ad indirizzare la paziente allimaging diagnostico . 
tuttavia , la rm risulta particolarmente utile sia a completamento dei casi ecografici dubbi che per linquadramento completo della malattia , in base alle note caratteristiche di elevata risoluzione di contrasto , per la capacit di tipizzazione delle lesioni a contenuto ematico e adiposo e per la panoramicit . 
analogamente , lo stato di infertilit pu motivare un work - up mediante imaging e il sospetto di adenomiosi pu anche essere basato sullisg classicamente richiesta in questi casi . ecografia transvaginale la diagnosi ecografica di adenomiosi in tecnica b - mode si basa sulle alterazioni dellecostruttura , ben apprezzabili con lo studio ecografico endocavitario e che rispecchiano le modificazioni istologiche . 
gli elementi di semeiotica elementare sono : aumentata ecogenicit miometriale o strie lineari iperecogene che si approfondano nel miometrio , espressione della presenza di isole di tessuto endometriale ectopico ; aree ipoecogene nel contesto del miometrio che rispecchiano liperplasia del tessuto muscolare che circonda il tessuto ectopico ; aree anecogene dovute ad ectasia ghiandolare o cisti miometriali ; trio ; scarsa definizione della giunzione endometrio / miomeaumento dimensionale dellutero con ispessimento asimmetrico di una delle pareti ( pseudowidening )  . rilevare almeno 3 di questi segni molto suggestivo per adenomiosi [ 11 ]  . 
i falsi negativi della isg sono legati alla mancanza di comunicazione delle ghiandole con la cavit uterina , e quindi alla loro mancata opacizzazione e conseguente mancato apprezzamento delle spicule ; i falsi positivi sono possibili in presenza di contorni molto irregolari della cavit uterina dovuti a differente patologia , ad esempio esiti flogisti [ 13 ]  . 
la scansione longitudinale mostra i seguenti elementi di semeiotica elementare : scarsa definizione della giunzione endometrio - miometrio ( freccia bianca grande ) ; aumento della ecogenicit miometriale dovuta a piccole aree iperecogene ( frecce bianche piccole ) espressione delle isole di tessuto endometriale ; aree ipoecogene nel contesto del miometrio che rispecchiano liperplasia del tessuto muscolare che circonda il tessuto eterotopico ( freccia vuota piccola ) ; aree anecogene dovute ad ectasia ghiandolare o cisti miometriali ( frecce vuote grandi )  . vessels at the lesion level . 
 if the patches of ectopic endometrium communicate with the cervical lumen , the dilated glandular lumina terminatle con quelle relative alla presenza di un fibroma cervicale ; la diagnostica differenziale isg tra endometriosi e fibroma cervicale , analogamente a quanto riportato per ladenomiosi del corpo e fondo uterino , non agevole e si basa essenzialmente sulla valutazione dei margini lesionali che sono pi sfumati nelladenomioma e pi netti nel fibroma . risonanza magnetica la rm metodica affidabile nella diagnosi di adenomiosi , con sensibilit variabile in letteratura tra 78% e 88% vs . 
la rm particolarmente utile nella tipizzazione delladenomiosi focale poich in grado di dirimere eventuali dubbi ecografici o isterosalpingografici sulla base di precisi elementi di semeiotica elementare e di importanti segni morfologici , utili per la diagnostica differenziale . 
la tipologia di distribuzione dei foci iperintensi nelle sequenze t2 dipendenti nelladenomioma , oltre allaspetto sfumato dei margini , elemento distintivo importante nella diagnostica differenziale con unaltra patologia , rara ma equivocabile , ovvero il tumore adenomatoide . 
oblique view of the uterus shows vessels ( arrows ) surrounding a hypoechoic , well - defined lesion in the wall of the uterine body , corresponding to a leiomyofig . 
la scansione obliqua con studio power doppler ben documenta il decorso dei vasi intra - uterini che abbracciano ( frecce ) una lesione ipoecogena a margini netti localizzata nel contesto del corpo uterino , da riferire a fibroma . ing in a cul - de - sac may be appreciated . 
sagittal transvaginal tvus of the cervix ( a ) demonstrates a iso / hypoechoic , ill - defined mass ( callipers ) with hypoechoic areas embedded , corresponding to ectopic endometrial dilated glands with internal echoic debris ( white arrows ) ; a nabothian cyst is visible near the lesion , appearing as a simple anechoic image ( void arrow )  . 
l ecografia transvaginale , scansione longitudinale ( a ) , documenta in sede cervicale unarea ipoecogena sfumata ( calipers ) nel cui contesto si evidenziano alcune formazioni ipo - / iso - ecogene , riferibile a zolle di endometrio con lumi ghiandolari ectasici e materiale corpuscolato nel loro contesto ( frecce bianche ) ; in sede adiacente una cisti di naboth di aspetto ecografico anecogeno ( freccia vuota )  . 
la scansione rm coronale gradient echo t1 pesata con saturazione del segnale del tessuto adiposo ( b ) , mostra minuti foci iperintensi in regione cervicale ( frecce bianche ) cui si associa formazione iperintensa dellannesso di sinistra , da riferire ad endometrioma ( freccia vuota )  . 
in corrispondenza di tali piccole aree iperintense , nella sequenza assiale fast spin echo t2 pesata ( c ) si osserva una formazione ipointensa a margini sfumati con foci iperintensi nel contesto ( frecce ) , riferibile ad endometrio in posizione ectopica . of faecal matter in the rectum , or to confuse them with signs produced by a cervical fibroma . 
the differential diagnosis with hsg between endometriosis and cervical fibroma , not unlike the situation reported for adenomyosis of the uterine body and fundus , is no simple task and is essentially based on evaluation of lesion margins , which tend to be ill - defined in adenomyoma and better - defined in fibroma . magnetic resonance imaging mr imaging is a reliable modality for diagnosing adenomyosis , with a sensitivity varying in the literature between 78% and 88% vs . 
the classic mr imaging signs [ 12 ] for identifying diffuse adenomyosis include : le ; lanamnesi pu essere di aiuto nella caratterizzazione . la localizzazione cervicale non di facile tipizzazione in rm per la possibile confusione con forme flogistiche ( cervicite glandulo - cistica ) o con la semplice dilatazione cistica delle ghiandole di naboth . 
tuttavia , poich il materiale proteico mostra segnale iperintenso nelle sequenze t1 pesate , analogamente al materiale ematico , un elemento di semeiotica rm utile alla diagnosi lo slargamento dello stroma cervicale nella sede della lesione . 
anteroposterior projection shows small outpouchings ( small white arrows ) perpendicular to internal uterine contour , located in the fundus and right uterine wall , which indicate dilated glandular ducts of the dislocated endometrial tissue . 
la proiezione anteroposteriore documenta , in corrispondenza del fondo e della parete laterale di destra dellutero , la presenza di estroflessioni del contorno terminanti a cul di sacco ( frecce bianche piccole ) , perpendicolari al margine uterino , compatibili con lumi ghiandolari ectasici , che si approfondano nella parete uterina , in rapporto alla presenza di adenomiosi . 
mr imaging is particularly useful in characterising focal adenomyosis because it is able to eliminate doubts raised at tvus or hsg on the basis of precise fundamental imaging signs and important morphological features , which are useful for differential diagfig . 
la proiezione anteroposteriore documenta una estroflessione pseudo - diverticolare del fondo uterino , riferibile ad adenomiosi ( freccia ) con lume ghiandolare particolarmente ectasico della zolla di endometrio indovato nel miometrio , comunicante con la cavit uterina . 
la terapia chirurgica , di tipo radicale o conservativo , molto dipende dal grado di infiltrazione miometriale e la pianificazione del tipo dintervento non pu prescindere dallattenta e preliminare valutazione di eventuale patologia aderenziale pelvica associata , che possibile definire in anticipo . 
 trattamento medico il trattamento medico delladenomiosi ha oggi molteplici opzioni , che spaziano dal trattamento locale con rilascio di farmaci attraverso un dispositivo intra - uterino ( iud ) alle preparazioni di tipo sistemico . 
limpiego di farmaci progestinici rilasciati dallo iud nella prevenzione dei disordini di tipo mestruale , per la riduzione dellentit del sanguinamento nelle donne con mestruazioni particolarmente abbondanti , noto [ 15 ]  . 
tali farmaci , comportando la decidualizzazione dellendometrio [ 16 ] e le conseguenti modificazioni di tipo atrofico che riducono lentit del sanguinamento , riducono anche lentit dei depositi adenomiotici ; ne conseguono laumento della contrattilit uterina , la conseguente riduzione del volume dellutero e il miglioramento del quadro clinico per riduzione della dismenorrea . 
analogamente , stato proposto il rilasciamento attraverso lo iud di ormoni sintetici derivati dal testosterone [ 17 ] la cui azione quella di sopprimere la produzione di gonadotropine inducendo uno stato di pseudo - menopausa . tra i farmaci a somministrazione sistemica , sono stati segnalati gli analoghi dellormone gonadotropo ( agonisti gnrh ) che , avendo una struttura chimica del tutto analoga a questultimo , conducono ad una saturazione dei recettori fig . 
nella sequenza sagittale fse t2 pesata , si segnala utero antiverso con zona di giunzione ispessita ( > 12 mm ) ( freccia bianca piccola ) e fluido a segnale disomogeneo in sede endouterina ( calipers ) ed endovaginale ( freccia bianca grande ) riferibile a materiale ematico in rapporto alla fase mestruale del ciclo . radiol med ( 2011 ) 116 : 12671287 1277 fig . 
sagittal t1 - weighted gradient echo fat - saturated image , high signal intensity foci in the myometrium in the posterior wall of the uterine body ( a , void arrows ) ; sagittal t2weighted fast spin echo image ( b ) ill - defined , low - signal - intensity nodule containing bright foci ( arrows ) corresponding to adenomyoma is visualised in that area ; diffuse widening of the anterior junctional zone is also well visualised . 
la scansione sagittale gre t1 pesata con saturazione del segnale del tessuto adiposo documenta piccoli spots iperintensi nel contesto del miometro della parete posteriore del corpo uterino ( a , frecce vuote ) ; nella scansioni sagittale ( b ) fse t2 pesata , in corrispondenza delle aree iperintense segnalate in a , si osserva nodulo a margini sfumati , di aspetto ellittico e con foci iperintensi diffusamente distribuiti nel suo contesto ( frecce ) relativo ad adenomioma ; si documenta anche lispessimento marcato della zona di giunzione anteriore . 
the distribution of hyperintensive foci in t2 - weighted sequences in adenomyoma , ipofisari del gnrh cui conseguono la riduzione dei livelli del gnrh e uno stato di menopausa indotto . 
se la terapia viene interrotta , tale effetto reversibile e per tale motivo questo tipo di trattamento non pu essere considerato una cura definitiva per ladenomiosi ; di solito , viene protratto per 36 mesi prima dellescissione chirurgica per i vantaggi derivanti dalla riduzione del sanguinamento in corso dintervento e dal minor trauma tissutale [ 16 ]  . 
la soppressione della biosintesi degli estrogeni mediante gli agonisti gnrh e gli inibitori dellaromatase sembra possa significativamente ridurre il rischio di recidive dopo terapia conservativa delladenomiosi [ 15 ]  . 
questo tipo di approccio terapeutico , ovvero di tipo medico , pu essere facilmente supportato da tecniche di monitoraggio diagnostico , rappresentate in particolare dalletv e dalla rm che sono impiegabili per il controllo dimensionale dellutero e dei noduli di adenomiosi in corso di trattamento . chirurgica radicale nelladenomiosi diffusa quando sia in predicato una iste1278 radiol med ( 2011 ) 116 : 12671287 fig . 
la scansione assiali spin echo ( se ) t1 pesata ( a ) documenta una formazione protrudente nel lume endometriale , ad elevata intensit di segnale ( freccia ) come per contenuto ematico ; le scansioni sagittali spoiled gradient echo ( spgr ) t1 pesate con saturazione del segnale del tessuto adiposo dopo somministrazione di mdc , mostrano sia nella fase arteriosa ( b ) , che in quella portale ( c ) e tardiva ( d ) , una ridotta impregnazione della lesione rispetto al miometrio circostante ; la formazione appare inscritta nella zona giunzionale , che aperta a coppa come ben si documenta in fase arteriosa ( b , freccia ) ove essa riconoscibile per il segnale pi marcatamente intenso rispetto al restante miometrio ; il segnale della zona giunzionale si omogeneizza gradatamente col miometrio esterno nelle altre fasi ( d )  . 
tuttavia , a riguardo delle complicanze dellisterectomia transvaginale , in uno studio effettuato su pazienti con leiomiomi e affette da adenomiosi [ 18 ] si riporta un pi elevato rischio di lesioni della vescica nelle pazienti del secondo gruppo . 
la scansione assiale gre t1 pesata con saturazione del segnale del tessuto adiposo ( a ) documenta grossolana formazione ad elevata intensit di segnale , come per presenza di sangue ( freccia ) , dotata di livello endoluminale e localizzata nel contesto della parete miometriale posteriore del fondo , riferibile a cisti adenomiosica ; nella scansione assiale fse t2 pesata ( b ) si conferma la presenza di materiale ematico con sedimento declive ( freccia )  . located and dilated mesothelial tubules . adenomyotic cyst enters the differential diagnosis with the outcomes from recent myomectomy , as blood material may be encountered in the residual uterine cavity and misinterpreted . 
patient history can be helpful in characterising the findings . ectopic endometrial tissue located in the cervix is not easy to characterise with mr imaging given the possible confusion with inflammation ( glandularcystic cervicitis ) or with simple cystic dilatation of the nabothian glands . 
la scansione sagittale fse t2 pesata documenta una lesione ipointensa nel contesto della parete posteriore dellutero , con effetto massa , a margini netti e con foci iperintensi distribuiti perifericamente ( frecce bianche piccole ) , riferibile a tumore adenomatoide ; anteriormente ( freccia vuota ) un fibroma a parziale sviluppo sottosieroso . 1280 radiol med ( 2011 ) 116 : 12671287 fig . 
axial t1 - weighted gradient echo fat - saturated image ( a ) shows a large , hyperintense lesion , indicating haemorrhage ( white arrow ) in the cervix ; an endometrioma can also be seen in the left ovary ( void arrow )  . 
in addition , even aderenze , e una possibile spiegazione nel fatto che ladenomiosi e lendometriosi , nella quale le aderenze pelviche sono pressoch costanti , pur essendo due condizioni patologiche differenti possono coesistere nella stessa paziente . 
 la preliminare valutazione delle aderenze pelviche , quindi , essenziale nella pianificazione del tipo dintervento e la rm particolarmente adatta a tale controllo . chirurgica conservativa la chirurgia conservativa ( escissione / enucleazione chirurgica ) solitamente riservata alladenomiosi focale , ma il tipo di trattamento molto dipende dal tipo di lesione e dal grado di interessamento miometriale della malattia . 
 farquhar e brosens [ 15 ] hanno recentemente riportato i radiol med ( 2011 ) 116 : 12671287 1281 in cases of medical or interventional treatment , a reliable evaluation of the treatment and monitoring its effectiveness are necessary , and imaging can guarantee this . medical treatment medical treatment of adenomyosis has a wide variety of options , which range from local treatment with the release of medications by a intrauterine device ( iud ) to systemically administered treatment . 
these hormones act to suppress the production of gonadotropin , thus inducing a state of pseudomenopause . medications available for systemic administration include gonadotropin - releasing hormone ( gnrh ) agonists , which have a chemical structure analogous to gonadotropin and therefore interact with the gnrh receptors . 
this type of treatment approach ( medical treatment ) can be easily supported by diagnostic monitoring techniques , in particular by tvus and mr , which can be used to monitor the size of the uterus and the adenomyotic nodules being treated . radical surgery in cases of diffuse adenomyosis in which a hysterectomy fig . 
la scansione assiale fast spin echo t2 pesata documenta un grappolo di formazioni iperintense ( freccia ) come per contenuto fluido , riferibili ad estasia cistica delle ghiandole cervicali ( cisti di naboth ) , localizzate medialmente allo stroma . differenti trattamenti chirurgici proposti in letteratura per ladenomiosi focale basati sulla localizzazione delladenomioma , in sede sottomucosa , intramurale , e sub - peritoneale o intra - ligamentosa : ( 1 ) per ladenomioma a sviluppo sottomucoso , ovvero per la forma polipoide a protrusione intra - luminale , e per quella pi superficiale o pseudowidening , vengono proposte rispettivamente lescissione isteroscopica o la resezione endometriale trans cervicale ; ( 2 ) lenucleazione viene suggerita per la localizzazione intramurale , ovvero per ladenomioma che risparmia il contorno uterino ; tuttavia la lesione potrebbe essere vicina alle tube di falloppio o coinvolgere i vasi maggiori e in tal caso viene proposta anche una cito - riduzione preliminare mediante agonisti gnrh ; listerectomia viene proposta se il miometrio comunque interessato in profondit ; ( 3 ) per ladenomioma sottosieroso o sub - peritoneale , localizzato nella parete posteriore dellutero in prossimit di endometriomi ovarici strettamente adesi allutero , viene suggerita lescissione superficiale o anche laparoscopica . intuitivo che la preliminare pianificazione del tipo dintervento mandatoria e che non solo vada accertata preliminarmente leventuale coesistenza di aderenze pelviche ma anche lentit del coinvolgimento miometriale . 1282 radiol med ( 2011 ) 116 : 12671287 is being considered , transvaginal access is preferable to transabdominal access due to the lower morbidity and shorter hospital stay of the former , this of course being dependent on the experience of the surgeon . 
nonetheless , with regard to complications of transvaginal hysterectomy , a study on two groups of patients , one with leiomyomas and the other with adenomyosis [ 18 ] , reported a higher risk of lesions to the urinary bladder in patients from the latter group . 
this may be explained by the fact that despite being two separate pathological conditions , adenomyosis and endometriosis may coexist in the same patient , and pelvic adherences are very frequent in the latter condition . 
a preliminary evaluation for pelvic adherences , therefore , is crucial in planning the type of procedure , and mr imaging is particularly suited to this type of study . conservative surgery conservative surgery ( surgical excision / enucleation ) is usually reserved for focal adenomyosis , but the type of treatment is heavily dependent on the type of lesion and the extent of myometrial involvement . 
farquhar and brosens [ 15 ] recently reported the different surgical procedures proposed in the literature for focal adenomyosis based on adenomyoma location , whether submucosal , intramural , subperitoneal or intraligamentous : ( 1 ) approaches proposed for adenomyoma with submucosal development , i.e. 
the polypoid form with intraluminal protrusion and the more superficial or pseudowidening form , are hysteroscopic or transcervical endometrial excisions , respectively ; ( 2 ) enucleation is suggested for lesions with intramural location , i.e. 
hysterectomy is instead the preferred option if there is deep involvement of the myometrium ; ( 3 ) superficial excision or even laparoscopy are proposed for subserosal adenomyomas located in the posterior wall of the uterus in the vicinity of ovarian endometriomas tightly adhering to the uterus . clearly , preliminary planning intervention type is mandatory , and not only should the coexistence of pelvic adherences be evaluated , but the degree of myometrial involvement also . embolisation embolisation of the uterine artery is a therapeutic approach adopted for treating fibromas . 
adenomyosis and uterine fibromas may embolizzazione lembolizzazione dellarteria uterina noto presidio terapeutico nel trattamento dei fibromi per il controllo della cui efficacia le metodiche di imaging , ed in particolare la rm , sono stati utilmente impiegati [ 19 ]  . 
 tuttavia , nonostante alcuni risultati incoraggianti riportati in letteratura [ 20 , 21 ] la possibilit di fallimento suggerisce ulteriori studi per chiarire il ruolo effettivo di questo tipo di trattamento . ultrasuoni focalizzati labilit delle onde ultrasonore di provocare incremento della temperatura tissutale nota da tempo [ 22 ] ma le onde ultrasonore utilizzate in diagnostica sono distribuite su unampia area e quindi lincremento della temperatura da esse provocata impercettibile . 
se il pattern delle onde ultrasonore viene modificato di modo che esse possano confluire su un unico punto , si pu provocare un incremento localizzato della temperatura in quel punto , con denaturazione delle proteine per temperature che superano i 55c e conseguente morte cellulare irreversibile e necrosi coagulativa [ 23 ]  . 
questa il principio sul quale si basa la terapia ad ultrasuoni focalizzati , per il controllo della quale stato proposto limpiego della rm sia per la sua eccellente risoluzione anatomica che per la sensibilit allimaging termico [ 24 ]  . 
pertanto , nonostante la tecnica possa sembrare una utile alternativa nel trattamento delladenomiosi , essa necessita di ulteriori studi per il chiarimento del suo ruolo effettivo [ 23 ]  . discussione i goals dellimaging in tema di adenomiosi sono essenzialmente : ( 1 ) il corretto inquadramento della malattia ; ( 2 ) la valutazione dellambiente peri - uterino e del grado di interessamento del miometrio , per un corretto approccio terapeutico e ( 3 ) il monitoraggio delle pazienti trattate con terapia conservativa . 
da quanto fino ad ora esposto , emerge che la rm ha un ruolo importante nella diagnosi di adenomiosi , essenziale per linquadramento globale della malattia , a causa dellelevata capacit di caratterizzazione tissutale e per la sua panoramicit . 
however , despite some encouraging results reported in the literature [ 20 , 21 ] , the possibility of failure suggests the need for further studies to clarify the effective role of this treatment . high - intensity focused ultrasound the ability of ultrasound waves to increase tissue temperature has been known for some time [ 22 ] , but the ultrasound waves used in diagnostic imaging are distributed over a wide area and therefore the temperature increase they produce is imperceptible . 
if the pattern of the ultrasound waves is modified such that they are made to converge at a single point , a localised increase in temperature may be produced at that point , with protein denaturation at temperatures > 55c and the consequent irreversible cell death and coagulation necrosis [ 23 ]  . 
this is the principle of high - intensity focused ultrasound , for which mr imaging has been proposed as the guidance technique due to its excellent anatomical resolution and sensitivity to thermal imaging [ 24 ]  . 
therefore , although the technique seems to be a useful alternative , further studies are needed to clarify its effective role [ 23 ]  . discussion the imaging goals in relation to adenomyosis are essentially the following : ( 1 ) correct identification of the disease ; ( 2 ) evaluation of the periuterine environment and extent of myometrial involvement for choosing the most appropriate treatment ; ( 3 ) monitoring patients treated with conservative therapy . as the above demonstrates , mr imaging plays an important role in diagnosing adenomyosis , given its remarkable capacity for tissue characterisation and the panoramic views it offers . 
the accuracy of the technique is , on the whole , greater than that of tvus , with percentages ranging from 85% to 90.5% against the 6886% of tvus [ 12 ]  . 
foci of bleeding may not necessarily be identified in adenomyosis , as only the basal layer of the endometrium , which does not respond to hormonal stimulation , is located ectopically . 
nonetheless , it is always worthwhile to perform the examination in the subacute phase of a possible bleeding , because the hyperintense foci identified a quella della etv , con percentuali pari all85%90 , 5% vs . 
anche se nelladenomiosi possibile non rilevare necessariamente foci di sanguinamento , a causa della posizione ectopica del solo strato basale dellendometrio non rispondente agli stimoli ormonali , sempre bene eseguire lindagine nella fase subacuta di un possibile sanguinamento , perch in tal caso i foci iperintensi nelle sequenze t1 pesate sono in grado di caratterizzare una endometriosi eventualmente associata . 
opportuno , pertanto , osservare con attenzione sempre tutte le sequenze e le varie immagini per evitare errori diagnostici ; lo spasmo non potr essere sempre costantemente rilevato nel corso di una indagine rm , che notoriamente piuttosto lunga . abbiamo anche visto come lapproccio terapeutico necessiti di una corretta pianificazione preliminare . 
la presenza di aderenze pu condizionare lapproccio chirurgico , laparoscopico o classico trans - addominale , e le possibilit della rm nellidentificare le aderenze in maniera indiretta [ 25 ] o mediante cine - rm con immagini dinamiche che documentano la mobilit degli organi , sono note [ 26 ]  . la scelta chirurgica radicale o di tipo conservativo molto dipende anche dal grado di infiltrazione miometriale da parte delladenomiosi e la rm pu accertarlo mediante lattenta valutazione del grado di enhancement lesionale dopo mdc . 
 [ 27 ] ha dimostrato che il grado di interessamento miometriale da parte della neoplasia dellendometrio pi facilmente determinabile nella fase di equilibrio in cui la lesione neoplastica , con segnale pi 1284 radiol med ( 2011 ) 116 : 12671287 in t1 - weighted sequences are able to characterise any associated endometriosis . 
mr imaging identifies adherences indirectly [ 25 ] or with cinemr dynamic images , which demonstrate organ mobility [ 26 ]  . choosing between radical and conservative surgery is also heavily dependent on the extent of myometrial infiltration by the adenomyosis ; mr imaging allows verification of this , with a thorough evaluation of the degree of lesion enhancement after contrast agent administration . 
 [ 27 ] showed that the extent of myometrial involvement by endometrial carcinoma can be easily recognised in the equilibrium phase in which the neoplastic lesion , which has lower signal intensity than the myometrium , is best identified within the myometriu however , if the endometrial carcinoma arises from an adenomyosis , which is also an enhancing lesion and therefore with a less intense signal than the myometrium , it may be useful to exploit junctional zone enhancement in the arterial phase to identify whether the endometrial carcinoma has infiltrated the myometrium [ 5 ]  . 
la scansione assiale t2 pesata mostra a livello della parte posteriore del fondo unarea ipoecogena ( a , frecce ) con foci iperintensi nel contesto , di morfologia ellittica e a margini sfumati ( pseudowidening ) ; la scansione assiale spgr t1 pesata con saturazione del segnale del tessuto adiposo in fase tardiva dellenhacement dopo somministrazione di mdc , conferma la ridotta impregnazione rispetto al circostante miometrio della lesione adenomiosica che si approfond marcatamente nel miometrio ( b , freccia )  . basso rispetto al miometrio , meglio si identifica nel contesto miometriale . 
tuttavia , se la neoplasia endometriale insorge su adenomiosi , anchessa con enhancement e , quindi , con segnale ridotto rispetto al miometrio , pu essere utile sfruttare il potenziamento della jz nella fase arteriosa per identificare leventuale sconfinamento miometriale della lesione neoplastica dellendometrio [ 5 ]  . 
tvus , especially for its ability to evaluate reduction in the size of the uterus and the presence of focal lesions , and mr imaging , for global and complete evaluation of the uterus and its environment , without doubt play a useful role in monitoring this kind of treatment . 
the role that the two imaging modalities , particularly mr imaging , may play in the new interventional techniques still needs to be clearly defined , even though the recent studies appear promising . in conclusion , tvus and above all , mr imaging are particularly useful modalities for studying adenomyosis , both for characterising the disease and monitoring treatment . 
il ruolo delle metodiche di imaging , e in particolare della rm , in relazione alle nuove tecniche terapeutiche di tipo interventistico ancora da definire con certezza , anche se gli studi attuali sembrano promettenti . 
hlpm consists of selective catheterisation of the common hepatic artery , permanent occlusion of the gastroduodenal artery at its origin using metal coils , an inflated balloon catheter placement at the origin of the proper hepatic artery to block blood flow and induce hypoxia for around 10 min , mmc infusion and vascular - bed occlusion through injection of an absorbable haemostatic agent . 
 hlpm consiste nella cateterizzazione selettiva della arteria epatica comune , occlusione permanente della arteria gastro - duodenale alla sua origine mediante spirali metalliche ; posizionamento di un catetere da occlusione con palloncino gonfiato alla origine della arteria epatica propria per bloccare il suo flusso ed indurre ipossia per circa 10 minuti ; infusione di mmc ; occlusione del letto vascolare mediante iniezione di un agente emostatico riassorbibile . 
il ricovero dei pazienti in ospedale durato 1240 radiol med ( 2011 ) 116 : 12391249 a partial response ( pr ) in 29% , stable disease ( sd ) in 45% and progressive disease ( pd ) in 26% of patients . 
it may be considered a palliative treatment option in patients with advanced liver disease in centres with adequately experienced medical teams . keywords hypoxic liver perfusion multifocal liver metastases mitomycin - c in media 10 giorni ( range 715 )  . 
lesame tc condotto dopo 30 giorni dal trattamento ha documentato una risposta parziale ( pr ) nel 29% dei pazienti , una stabilit di malattia ( sd ) nel 45% , ed una progressione di malattia ( pd ) nel 26% . 
essa pu essere considerata una opzione come trattamento palliativo in pazienti con malattia epatica in stato avanzato , nei centri ove sia disponibile team medico dotato di adeguata esperienza . parole chiave infusione intra - arteriosa epatica in ipossia metastasi epatiche multiple mitomicina - c introduction introduzione colorectal cancer ( crc ) is the most frequent cause of liver metastases . 
after systemic chemotherapy , mean survival rates have recently been reported to be approximately 20 months [ 4 , 5 ] , with a 3 - year survival rate of around 10% [ 4 ]  . 
 in addition to crc , liver metastases may complicate the course of many other cancers , such as ocular melanoma and neuroendocrine tumours , and are the main cause of death in the majority of cases . 
only a minority of patients has surgically resectable lesions , most of them being candidates for regional therapies [ 6 ]  . the liver has a double blood supply : the portal vein accounts for 7080% of blood supply , which explains the high rate of metastases from mesenteric regions ; the hepatic artery and its branches allows detection of hypervascular liver metastases . 
infusion therapy consists of administering chemotherapeutic agents directly into the hepatic artery using superselective catheterisation [ hepatic arterial infusion ( hai ) ] ; this may il cancro del colon - retto ( ccr ) la causa pi frequente di metastasi epatiche . 
nel 10%20% dei pazienti con ccr le metastasi epatiche sono sincrone , e rappresentano lunico fattore limitante laspettativa di vita sino a circa il 60% dei pazienti [ 2 ]  . 
dopo chemioterapia sistemica la sopravvivenza media stata recentemente riportata intorno ai 20 mesi [ 4 , 5 ] con una sopravvivenza a 3 anni di circa il 10% [ 4 ]  . 
 oltre al ccr , le metastasi epatiche possono complicare il decorso di molte altre neoplasie , come il melanoma oculare , i tumori neuroendocrini , ed altri ancora , e rappresentano la principale causa di morte nella maggior parte dei casi . 
 il fegato ha un doppio apporto ematico : la vena porta fornisce il 70%80% del sangue e ci spiega lalta frequenza di metastasi che giungono dai territori mesenterici ; larteria epatica ed i suoi rami permettono di evidenziare le metastasi epatiche iper - vascolarizzate . 
la terapia infusionale consiste nella somministrazione di chemioterapici radiol med ( 2011 ) 116 : 12391249 1241 be followed by vascular occlusion [ transarterial chemoembolisation ( tace ) ]  . 
hai , tace and hae have the same palliative and symptomatic indications and contraindications , and in particular , the percentage of hepatic parenchyma involvement ( > 75% ) and the portalvein thrombosis resulting from hepatic artery occlusion by the embolisation agents used in tace . 
 the technique , consisting of comprehensive hepatic arterial infusion of mitomycin - c under hypoxic conditions , followed by embolisation with spongostan [ hypoxic liver perfusion with mmc ( hlpm ) ] was first described by ricci et al . 
 the purpose of our analysis was to evaluate treatment feasibility and toxicity and its impact on os and diseasefree ( dfs ) survival . materials and methods forty - two patients ( 25 men , 17 women ) , mean age 57 ( range 3378 ) years , refractory to other locoregional and / or systemic treatments , were treated with hlpm between june 2001 and may 2009 . 
the patients had multifocal , unresectable liver metastases originating from different primary tumours : crc ( n = 25 ) , neuroendocrine tumour ( n = 2 ) , pancreatic tumour ( n = 3 ) , uveal melanoma ( n = 2 ) , gastric cancer ( n = 2 ) , ovarian cancer ( n = 1 ) and fibrosarcoma ( n = 1 )  . 
in 14 of the 56 procedures , the ecog score was 2 . inclusion criteria were : presence of multifocal liver metastases that were unresectable or nontreatable with local ablative therapies and refractory to at least one direttamente nella arteria epatica mediante un cateterismo super - selettivo ( infusione arteriosa epatica , iae ) ; essa pu essere seguita dalla occlusione vascolare ( chemio - embolizzazione trans - arteriosa , tace )  . 
iae , tace e eae , presentano le stesse indicazioni palliative e sintomatiche , cos come le stesse controindicazioni , con particolare attenzione alla percentuale di coinvolgimento del parenchima epatico ( superiore al 75% ) e alla trombosi della vena porta in relazione alla occlusione della arteria epatica da parte degli agenti embolizzanti usati durante la tace . 
 la tecnica , che consiste nella infusione arteriosa epatica globale con mitomicina - c in condizioni di ipossia , seguita dalla embolizzazione con spongostan ( hypoxic liver perfusion with mmc , hlpm ) stata descritta per la prima volta da ricci et al . 
in questo lavoro , descriviamo la nostra esperienza in 42 pazienti trattati con hlpm . lo scopo della nostra analisi di valutare la fattibilit del trattamento , la tossicit associata al trattamento e limpatto di questo sulla sopravvivenza globale e sulla sopravvivenza libera da malattia . 
 materiali e metodi quarantadue pazienti ( 25 maschi e 17 femmine ) , et media 57 anni ( range 3378 ) , refrattari ad altre terapie locoregionali e / o a trattamenti sistemici , sono stati trattati con hlpm da giugno 2001 a maggio 2009 . 
i pazienti erano affetti da multiple metastasi epatiche non - resecabili , a partenza da tumori primitivi differenti : 25 / 42 erano affetti da ccr , 2 da tumori neuroendocrini , 3 da tumore del pancreas , 2 da melanoma delluvea , 2 da tumore dello stomaco , uno da tumore dellovaio ed uno da fibrosarcoma . 
sei pazienti presentavano tumore epatico primitivo , colangiocarcinoma : uno di questi era stato precedentemente trattato chirurgicamente , mentre gli altri erano stati classificati come inoperabili ( tabella 1 )  . 
 patients with a surgically unresectable primary liver tumour refractory to other locoregional therapies were also considered candidates for treatment . total - body assessment , each patient underwent complete biochemical and anaesthesiological computed tomography ( ct ) and complete analyses of the risks and benefits of hlpm . 
 then , the balloon of the catheter ( occlusion balloon catheter ) was inflated at the origin of the common hepatic artery to block blood flow and infuse mmc diluted in 200 ml of saline solution at 2050 mg . 
finally , vascular occlusion was achieved by injecting the absorbable gelatine sponge ( spongostan , johnson & johnson medical limited , gargrave , skipton , uk ) suspended in 1520 ml of contrast material . 
the overall duration of the procedure varied between 45 and 120 m during the procedure , usually at the embolisation stage , many patients reported abdominal pain and were treated with analgesic therapy managed by the anaesthetist . 
 in ogni paziente stata eseguita una completa valutazione biochimica ed anestesiologica , una tomografia computerizzata ( tc ) total - body , ed una completa pianificazione dei rischi e dei benefici dellhlpm . 
 al termine , stata eseguita locclusione vascolare con la iniezione di gelatina riassorbibile spugnosa ( spongostan , jonson and jonson medical limited , gargrave , skipton , gran bretagna ) solubilizzata con 1520 ml di mezzo di contrasto . 
la risposta biochimica al trattamento stata valutata confrontando i valori del markers ( antigene carcinoembrionario , cea , e antigene carboidratico , ca , 19.9 ) , prima e 30 giorni dopo il trattamento . 
una tc delladdome stata eseguita ad 1 , 3 e 6 mesi dal termine della procedura , e la risposta stata valutata in accordo con i criteri response evaluation criteria in solid tumors ( recist ) [ 11 ]  . 
per valutare lo tossicit epatica e quella sistemica , sono stati confrontati i valori degli enzimi epatici ( ast , alt ) , di - gt , di pseudo - colinesterasi , di bilirubina totale , di lattico - deidrogenasi ( ldh ) e di fosfatasi alcalina prima e dopo la procedura . i valori numerici sono stati espressi come valori medi ed stato indicato il range corrispondente ; le variabili considerate pree post - hlpm sono graficamente rappresentate come box - plots e confrontate usando il wilcoxon ranks test . 
 la sopravvivenza globale ( overall survival , os ) e quella libera da malattia ( progression free - survival , pfs ) sono state valutate usando il metodo di kaplan - meier [ 12 ]  . 
in un paziente con tumore gastrico in stato avanzato ed iniziale lieve insufficienza epatica si registrata una insufficienza epatica ; nellaltro caso il paziente deceduto in seguito ad una emorragia cerebrale non correlabile con la procedura . 
1 limmagine arteriografica mostra il cateterismo selettivo della arteria epatica e la occlusione permanente del tratto prossimale della arteria gastro - duodenale con spirali metalliche . the biochemical response to treatment was assessed by comparing marker values carcinoembryonic antigen ( cea ) and cancer antigen ( ca ) 19.9 before and 30 days after treatment . 
an abdominal ct scan was performed 1 , 3 and 6 months after the procedure , and response was assessed according to the response evaluation criteria in solid tumours ( recist ) criteria [ 11 ]  . 
to assess hepatic and systemic toxicity , we compared the values of liver enzymes [ aspartate aminotransferase ( ast ) , alanine aminotransferase ( alt ) , gamma - glutamyltranspeptidase ( - gt ) , pseudocholinesterase , total bilirubin , lactate dehydrogenase ( ldh ) and alkaline phosphatase ( ap ) before and after the procedure [ 11 ]  . numeric values are expressed as means with the corresponding range ; variables considered before and after hlpm are graphically represented as box plots and compared using the wilcoxon rank test . 
the other died of cerebral haemorrhage unrelated to the procedure . with reference to pain relief , on average , a single dose of a nonsteroid anti - inflammatory drug , four doses of mild opioids and nine doses of major opioids were administered during the hospital stay . 
pre - treatment values of cea [ 62 ng / ml ( sd142.39 ) , range 1507 ng / ml ] compared with those obtained 30 days after treatment [ cea 30 ng / ml ( sd111.6 ) , range 0.60312 ng / ml ] revealed no statistically significant difference . 
four patients were alive at the time of writing this report , one with crc metastases , one with a neuroendocrine tumour and two with liver metastases from uveal melanoma . 
no variable could be correlated to pfs ( table 2 )  . riguardo al trattamento del dolore , una media di una singola dose di farmaci antinfiammatori non steroidei ( fans ) , 4 dosi di oppioidi minori e 9 di oppioidi maggiori sono state somministrate ai nostri pazienti durante il ricovero . 
i valori di cea pre - trattamento ( 62 ng / ml , sd142 , 39 , range 1507 ng / ml ) confrontati con quelli ottenuti 30 giorni posttrattamento ( cea : 30 ng / ml , sd111 , 6 , range 0 , 60312 ng / ml ) non hanno mostrato una differenza statisticamente significativa . 
le variabili statisticamente associate con una migliore os erano : et giovane , intervallo tra la diagnosi del tumore e lhlpm ed intervallo tra la comparsa delle metastasi ed il trattamento in questione . 
nessuna variabile risultata correlabile con la pfs ( tabella 2 )  . discussione i pazienti con ampio coinvolgimento epatico , non responsivi o non candidabili ad altri tipi di trattamento possono radiol med ( 2011 ) 116 : 12391249 1245 fig . 
2a - d le immagini tc documentano un caso di risposta parziale ( pr ) ( a , b ) ed uno di stabilit di malattia ( sd ) ( c , d ) un mese dopo il trattamento . discussion patients with extensive liver involvement unresponsive to or not candidates for other forms of treatment may benefit from intra - arterial infusion of mitomycin c under hypoxic conditions . 
questi dati sono risultati in linea con le nostre aspettative , considerando che la mmc viene somministrata localmente ed in questo modo i rischi di tossicit sistemica sono pi bassi che non con la chemioterapia sistemica . 
la tossicit epatica e sistemica sono state valutate confrontando i valori di transaminasi , - gt , pseudo - colinesterasi , bilirubina totale , ldh e fosfatasi alcalina pree post - trattamento . 
nella nostra esperienza , la procedura ha una mortalit correlata al trattamento del 2% ( 1 / 56 ) : in un paziente affetto da cancro 1246 radiol med ( 2011 ) 116 : 12391249 fig . 
3a - g i diagrammi mostrano : a , b i valori medi di emoglobibna ( hb ) e della conta piastrinica ( plt ) prima e 30 giorni dopo il trattamento ; c - g i livelli di ast , alt , bilirubina , lattico deidrogenasi ( ldh ) e pseudocolinesterasi ( pce ) prima e dopo il trattamento . ment - related mortality rate of 2% ( 1 / 56 ) : one patient with advanced - stage gastric cancer suffered severe acute liver failure ; another died due to causes that were judged unrelated to this treatment . 
in 31 / 56 cases , the ct scan performed at 1 month never showed a complete response , whereas a partial response was obtained in 29% of cases , stable disease in 45% and progressive disease in 26% . 
in 31 / 56 casi , la tc disponibile dopo 1 mese dal termine della procedura , non ha mai mostrato una risposta completa , mentre una risposta parziale si avuta nel 29% dei casi , una stabilit di malattia nel 45% ed una progressione nel 26% . 
4a , b curve di sopravvivenza globale : per tutti i pazienti ( a ) , e solo per i pazienti affetti da carcinoma del colon - retto ( b )  . os ( months ) os ( months ) 4 months ( range 36 ) , and mean os from the diagnosis of liver metastasis was 20 months . 
 1248 radiol med ( 2011 ) 116 : 12391249 comparison with other similar procedures is made harder by the scarcity of data available in the literature concerning the hypoxic procedure and by the difficulty comparing patients with different characteristics . 
in order to obtain statistically comparable results , it may be useful to conduct a randomised trial to compare our data with those of other locoregional treatments ( hai , superselective tace )  . in conclusion , however , intra - arterial liver infusion with mmc can be considered a feasible approach to liver metastases . 
the feasibility of this procedure , even in patients with advanced - stage metastasised liver diseases , makes it an interesting option as a palliative treatment provided that an expert team is available to administer the treatment . tutti i pazienti con ccr erano stati precedentemente trattati con approcci sistemici standard . 
prendendo in considerazione gli studi in cui i pazienti presentavano caratteristiche simili a quelle dei nostri , la os era di 13 , 8 e 23 mesi in quelli trattati rispettivamente con tace e con iae . 
 [ 15 ] hanno riportato una os media di 343 giorni nel trattamento di lesioni epatiche non chirurgiche ; i pazienti sono parte di uno studio multicentrico pertanto difficile delineare esattamente le loro caratteristiche , ma questi erano stati considerati non candidabili per altri trattamenti . 
per avere dei risultati statisticamente confrontabili , pu essere utile , un trial randomizzato per confrontare i nostri dati con quelli ottenuti eseguendo altri trattamenti loco - regionali ( iea , tace super - selettiva )  . tuttavia , in conclusione , linfusione epatica intra - arteriosa di mmc pu essere considerata un approccio possibile alle metastasi epatiche . 
bazzocchi1 1institute of diagnostic radiology , university of udine , p.le santa maria della misericordia 15 , 33100 udine , italy 2dpmsc medical liver transplantation unit , internal medicine , university of udine , udine , italy correspondence to : l . 
this study was performed to assess the role of magnetic resonance cholangiography ( mrc ) in the clinical decision - making process of referring physicians when managing liver - transplanted patients . 
referring physicians were asked to prospectively state , before and after mrc , the leading diagnosis ; the level of confidence ( on a 0100% scale ) ; the most appropriate diagnostic / therapeutic plan . 
in modo prospettico , ai clinici di riferimento stato richiesto di indicare , prima e dopo la crm : la diagnosi presuntiva ; il livello di confidenza ( su scala 0%100% ) ; il piano diagnostico / terapeutico pi appropriato . 
lanalisi dei dati ha valutato : la resa diagnostica ; la proporzione di diagnosi presuntive modificate ; lefficacia terapeutica ( vale a dire , proporzione di piani diagnostico / terapeutici modificati ) ; lefficacia diagnostica presuntiva ( vale a dire , guadagno in confidenza diagnostica )  . 
lanalisi dei dati ha dimostrato : una resa diagnostica del 85 , 7% ; una proporzione di diagnosi presuntive modificate del 19 , 0% ; unefficacia terapeutica del 42 , 8% ; unefficacia diagnostica presuntiva rispettivamente pari a 18 , 8% e 78 , 7% per diagnosi presuntive concordanti e discordanti ( p < 0 , 01 )  . 
la crm radiol med ( 2011 ) 116 : 12501266 1251 keywords liver transplantation magnetic resonance imaging magnetic resonance cholangiography biliary complications clinical decision making ha inoltre determinato una modifica nella gestione dei pazienti in una proporzione significativa di casi , portando ad un beneficio clinico grazie alla sua elevata accuratezza . parole chiave trapianto di fegato risonanza magnetica colangiografia in risonanza magnetica complicanze biliari diagnosi introduction introduzione to date , endoscopic retrograde cholangiography ( erc ) or percutaneous transhepatic cholangiography ( ptc ) remain the standard of reference in evaluating biliary disease [ 1 , 2 ]  . 
in recent years , magnetic resonance cholangiography ( mrc ) has been advocated as an ideal noninvasive alternative to direct cholangiography [ 5 ] , as this highly fluid - sensitive technique allows panoramic and detailed representation of the biliary tree with no need for i.v. 
an increasing amount of evidence suggests that mrc is comparable with direct cholangiography in evaluating a wide spectrum of biliary diseases [ 6 , 7 ] , including biliary complications after orthotopic liver transplantation ( olt ) [ 815 ]  . 
 materials and methods the institutional review board approved this prospecad oggi , la colangiografia retrograda endoscopica ( cre ) e la colangiografia transepatica percutanea ( ctp ) ri mangono gli standard di riferimento nella valutazione della patologia biliare [ 1 , 2 ]  . 
negli ultimi anni , la colangiografia in risonanza magnetica ( crm ) stata proposta come alternativa ideale non invasiva alla colangiografia diretta [ 5 ] , dal momento che questa tecnica , altamente sensibi le ai liquidi , permette una rappresentazione panoramica e dettagliata dellalbero biliare senza bisogno delliniezione endovenosa di mezzo di contrasto . 
una sempre maggiore evidenza scientifica suggerisce che la crm sia comparabile alla colangiografia diretta nella valutazione di un ampio spettro di patologie biliari [ 6 , 7 ] , incluse le complicanze biliari dopo trapianto ortotopico di fegato ( tof ) [ 815 ]  . 
rispetto alla cre o alla ctp , la crm consente una rappresentazione dei dotti biliari sia a monte che a valle dellostruzione , fornendo unaccu rata mappa prima delle procedure interventistiche . 
a nostra conoscenza , nessun precedente studio ha investigato simili aspetti nei pazienti trapiantati di fegato , nei quali le complicanze biliari si verificano frequentemente , ovvero in pi del 30% dei casi [ 8 , 9 ]  . in relazione a ci , lo scopo del nostro studio stato definire il ruolo della crm nella gestione clinica dei pazienti trapiantati di fegato con sospette complicanze biliari . 
in particolare , lanalisi ha avuto lo scopo di investigare se la crm impatti in maniera significativa nel processo di decision - making dei clinici di riferimento e nella determinazione del work - up dei pazienti . 
the study was performed according to the principles of the declaration of helsinki and subsequent amendments . materiali e metodi patient population il comitato etico della struttura ha approvato questo studio di coorte prospettico senza necessit del consenso informato da parte del paziente . 
lo studio stato condotto in accordo ai principi della dichiarazione di helsinki e dei successivi emendamenti . over a 6 - month period ( january 2009june 2009 ) , all livertransplanted patients with suspected biliary complications were referred for mrc by the medical or surgical division of our hospital . 
exclusion criteria included any current contraindication to mr examination . pazienti imaging technique studies were performed on a 1.5 - t scanner ( magnetom avanto , siemens medical system , erlagen , germany ) using the combination of a six - channel abdominal phased - array surface coil and a spine - array coil and with the implementation of the generalized autocalibrating partially parallel acquisitions ( grappa ) algorithm of parallel imaging . 
 mrc was performed with the multislice technique using a heavily t2 - weighted , volumetric , nearly isotropic , respiratory - triggered turbo spin - echo ( tse ) sequence acquired in coronal and in some cases axial planes with the following acquisition parameters : repetition time ( tr ) 2 , 500 ms ; echo time ( te ) , 682 ms ; matrix size , 357384 ; field of view ( fov ) , 380380 mm ; slices 72 ; thickness 1 mm ; thickness in z direction 1.1 mm ; parallel imaging acceleration factor 3 ; nominal acquisition time 2 min 59 s . 
preliminary coronal and axial half - fourier acquisition single - shot turbo spinecho ( haste ) t2 - weighted sequences ( tr 1 , 000 ms ; te 88 ms ; matrix size 192256 ; fov , 178103 mm ; slices 20 ; thickness 5 mm ; slice gap 20% ; acquisition time 10 s ) were performed to allow a panoramic evaluation of the abdominal region . 
both thin slices and maximum intensity projection ( mip ) reconstructions were evaluated on a dedicated workstation . study design and data analysis the study was designed to achieve three main goals . 
with a well - codified approach [ 22 ] , experienced referring hepatologists ( pt , db ) compiled a questionnaire for each patient before in un periodo di 6 mesi ( gennaio 2009luglio 2009 ) , tutti i pazienti trapiantati di fegato con sospette complicanze biliari sono stati indirizzati alla crm dalla clinica medica o chirurgica del nostro ospedale . 
i criteri di esclusione consistevano nella presenza di controindicazioni allesecuzione della risonanza magnetica ( rm )  . tecnica gli studi sono stati realizzati su un magnete da 1 , 5 t ( magnetom avanto , siemens medical system , erlagen , germania ) utilizzando la combinazione di una bobina di superficie a 6 canali di tipo phased - array e di una bobina spine con limplementazione dellalgoritmo di imaging parallelo generalized autocalibrating partially parallel acquisitions ( grappa )  . 
la crm stata eseguita con tecnica multislice , utilizzando una sequenza turbo spinecho ( tse ) volumetrica , quasi isotropica , con trigger respiratorio , fortemente pesata in t2 , acquisita sul piano coronale ed in alcuni casi su quello assiale , con i seguenti parametri di acquisizione : tempo di ripetizione ( tr ) , 2500 ms ; tempo di eco ( te ) , 682 ms ; matrice , 357384 ; campo di vista ( fov ) , 380380 mm ; fette , 72 ; spessore , 1 mm ; spessore nella direzione z , 1 , 1 mm ; fattore di accelerazione di imaging parallelo , 3 ; tempo di acquisizione nominale , 2 min 59 s . 
sono state eseguite sequenze preliminari halffourier acquisition single - shot turbo - spin - echo ( haste ) t2 - pesate coronali ed assiali ( tr , 1000 ms ; te , 88 ms ; matrice , 192256 ; fov , 178103 mm ; fette , 20 ; spessore , 5 mm ; gap , 20% ; tempo di acquisizione , 10 s ) per una valutazione panoramica della regione addominale . 
sono state valutate su workstation dedicata sia le partizioni sottili che le ricostruzioni tridimensionali maximum intensity projection ( mip )  . disegno dello studio ed analisi dei dati lo studio stato mirato ad ottenere tre obiettivi principali . 
after mrc execution , the physicians indicated the post - mrc diagnosis , the level of confidence in it ( on a 0100% scale ) and the diagnostictherapeutic plan taking into account the mrc results . 
criteria to record preand post - mrc diagnoses were based on a previously described [ 14 ] standard classification of biliary complications in livertransplanted patients , as reported in table 1 . 
accordingly , complications were classified into three main categories : ( 1 ) strictures ( intraor extrahepatic ) ; ( 2 ) bile leakage ; ( 3 ) table 1 spectrum of biliary complications in liver - transplanted patients 1 . 
altre complicanze tabella 1 spettro delle complicanze biliari in pazienti trapiantati di fegato abbiamo valutato limpatto della crm nel processo di clinical decision - making dei clinici di riferimento [ 21 ] , ovvero la capacit della crm di modificare la diagnosi pretest ed il management pianificato , indipendentemente dalla sua performance diagnostica . 
dopo lesecuzione della crm , i clinici hanno indicato la diagnosi post - crm , la confidenza in questa ( su scala 0%100% ) ed il piano diagnostico - terapeutico tenendo conto dei risultati della crm . 
i criteri per riportare le diagnosi pre - crm e crm sono stati basati su una classificazione delle complicanze biliari nei pazienti trapiantati di fegato precedentemente descritta [ 14 ] e riportata nella tabella 1 . 
in accordo con tale classificazione , le complicanze sono state divise in tre categorie maggiori : ( 1 ) stenosi ( intrao extraepatiche ) ; ( 2 ) leakage biliare ; ( 3 ) varie , includendo entit patologiche meno frequenti come la cosiddetta vanishing bile duct syndrome ( gruppo di disordini acquisiti ed associati a distruzione progressiva e scomparsa dei dotti biliari intraepatici con colestasi ) [ 23 , 24 ] , la dilatazione non - ostruttiva , la disfunzione ampollare , il kinking , calcoli biliari / sludge / coaguli , le complicanze legate allanastomosi bilioenterica ed il leakage anastomotico . 
alla luce dei risultati della crm , sono state calcolate : ( 1 ) la proporzione delle diagnosi pre - crm che sono state cambiate dai clinici di riferimento dopo limaging ; ( 2 ) la proporzione dei piani diagnostico - terapeutici modificati dopo la crm rispetto alla valutazione pre - crm . 
le diagnosi pree postcrm sono state valutate come concordi quando stato segnalato lo stesso tipo di complicanze biliari , in accordo con la classificazione elencata nella tabella 1 , indipendentemente dalla presenza di altri reperti alla crm . 
 [ 22 ] , lanalisi ha valutato il guadagno in confidenza diagnostica ( la cosiddetta efficacia diagnostica presuntiva ) come segue : quando la diagnosi pree post - crm stata la stessa , il guadagno di confidenza stato calcolato sottraendo il valore assoluto della confidenza pre - crm da quella post - crm . 
in caso di diagnosi pree post - crm discordanti , la confidenza nella diagnosi finale prima della crm stata preliminarmente valutata sulla base dellassunto che la somma delle probabilit della diagnosi scelta e di tutte le diagnosi alternative del 100% . 
se la confidenza diagnostica per la diagnosi formulata prima della crm era eguale o maggiore del 50% , allora la confidenza diagnostica dedotta per la diagnosi rivista stata stimata del 100% meno la probabilit stabilita per la prima scelta diagnostica . 
in the light of the mrc results , the following measures were calculated : ( 1 ) the proportion of pre - mrc diagnoses that were changed by the referring physicians after imaging ; ( 2 ) the proportion of modified diagnostic therapeutic plans post - mrc compared with the pre - mrc evaluation . 
preand post - mrc diagnoses were assessed as concordant when the same type of biliary complication was reported , according to the classification listed in table 1 , regardless of additional mrc findings . 
 [ 22 ] , the analysis evaluated the gain in diagnostic confidence ( so - called diagnostic thinking efficacy ) as follows : if the preand post - mrc diagnosis was the same , the gain in confidence was calculated by subtracting the absolute values of the clinicians post - mrc and pre - mrc confidence . 
in the case of discordant preand post - mrc diagnosis , the confidence in the final diagnosis before mrc was preliminarily assessed based on the assumption that the sum of the probabilities of the chosen diagnosis and all other unstated diagnoses is 100% . 
if the diagnostic confidence for the selected diagnosis before mrc was 50% , then the inferred diagnostic confidence for the revised diagnosis was estimated to be 100% minus the stated probability of the first diagnostic choice . 
on the other hand , if the diagnostic confidence for the selected diagnosis before mrc was < 50% , the inferred diagnostic confidence percentage was estimated to be the same as the diagnostic confidence level given by the physicians . 
all statistical analyses were performed using commercially available software ( spss 16.0.0 for macintosh ; spss , chicago , il , usa )  . finally , mrc performance in the clinical setting was evaluated by calculating sensitivity , specificity , positive ( ppv ) and negative ( npv ) predictive values and overall accuracy after data cross - tabulation . 
direct cholangiographic procedures , such as erc and ptc , hepatic biopsy , and a follow - up period of at least 1 year were considered as standards of reference . results patient population twenty - one liver - transplanted patients ( 18 men , 3 women ; mean age 59 years ; range 4267 years ) underwent mrc in la percentuale di confidenza diagnostica dedotta stata stimata essere pari alla confidenza diagnostica formulata dai clinici . 
tutte le analisi statistiche sono state realizzate utilizzando un software disponibile in commercio ( spss 16.0.0 for macintosh ; spss , chicago , ill )  . infine , stata valutata la performance della crm calcolando la sensibilit , la specificit , i valori predittivi positivo e negativo e laccuratezza globale , dopo una tabulazione incrociata dei dati . 
sono stati considerati come standard di riferimento le procedure di colangiografia diretta , quali cre e ctp , la biopsia epatica ed un periodo di follow - up di almeno un anno . risultati pazienti sono stati considerati 21 pazienti trapiantati di fegato ( 18 uomini , 3 donne ; et media , 59 anni ; range 4267 anni ) che hanno effettuato una crm nel periodo specificato . 
non sono state clinicamente sospettate o riscontrate alla crm altre complicanze . determinazione della resa diagnostica e dellaccuratezza diagnostica sono state considerate positive 18 su 21 crm , con una resa diagnostica pari all85 , 71% ( intervallo di confidenza [ ic ] 95% 70 , 7100 , 0 )  . 
per quanto riguarda i due casi di crm falsi positivi ( pazienti 5 e 13 ) i reperti crm sono stati interpretati come compatibili con stenosi anastomotiche , non confermate alla successiva cre . 
reperti aggiuntivi della crm sono stati un kinking biliare in un paziente con stenosi extraepatica ( paziente 2 ) e due stenosi extraepatiche in pazienti con vanishing bile duct syndrome ( pazienti 4 e 12 )  . 
 nel corso della loro storia clinica , i pazienti privi di reperti biliari alla crm hanno effettuato , per un periodo di follow - up di almeno un anno , multipli esami di diagnostica per immagini tra cui crm ripetute , indagini ecografiche e di radiol med ( 2011 ) 116 : 12501266 1255 the specified period and were therefore considered . 
concerning the two false - positive mrc cases ( patients 5 and 13 ) , mrc findings were interpreted as consistent with anastomotic stricture , not confirmed at subsequent erc . 
additional mrc findings were bile - duct kinking in a patient with extrahepatic stricture ( patient 2 ) and two extrahepatic strictures in patients with vanishing bile - duct syndrome ( patients 4 and 12 )  . 
 patients with no biliary findings at mrc underwent multiple imaging examinations over a follow - up period of at least 1 year , including repeated mrcs , ultrasonography ( us ) and computed tomography ( ct ) scans . 
no biliary complications occurred in any of them . influence of mrc on the clinical decision making process the proportion of presumptive diagnoses modified in the light of mrc was 4 / 21 ( 19% ) patients . 
in three cases , physicians had a clinical suspicion of extrahepatic stricture ( patients 1 , 10 , and 11 ) but subsequently modified their leading diagnosis according to negative mrc . 
in one case ( patient 21 ) , vanishing bile - duct syndrome was clinically suspected , whereas mrc revealed an anastomotic stricture and regular intrahepatic bile ducts , as subsequently confirmed at therapeutic erc . 
 influenza della crm nel processo di clinical decision making la proporzione di diagnosi presuntive modificate alla luce della crm stata di 4 / 21 , corrispondente al 19% dei pazienti . 
in tre casi i clinici avevano sospettato una stenosi extraepatica ( pazienti 1 , 10 e 11 ) , ma hanno successivamente modificato la loro diagnosi in seguito allesito negativo della crm . 
in un caso ( paziente 21 ) a fronte di un sospetto clinico di vanishing bile duct syndrome la crm ha evidenziato una stenosi anastomotica , con dotti biliari intraepatici regolari , come successivamente confermato dalla cre terapeutica . 
dopo il test diagnostico , la confidenza media nella diagnosi crm stata pari al 98 , 7% , con un corrispondente guadagno medio in confidenza diagnostica del 78 , 7% . 
la confidenza media dei clinici nella diagnosi presuntiva nei restanti 17 / 21 casi con uguale diagnosi prima e dopo la crm stata pari a 80% e 98 , 8% rispettivamente , dando luogo cos ad un guadagno medio in confidenza del 18 , 8% ( statisticamente significativo , p = 0 , 0026 )  . 
in particolare la crm ha evitato lesecuzione di 2 cre pianificate in pazienti con esame negativo ( pazienti 10 e 11 ) , ha indotto lesecuzione di 4 cre e 1 ctp in 5 pazienti ( pazienti 2 , 5 , 13 e 14 con diagnosi crm di stenosi extra - epatica e paziente 12 con diagnosi crm di vanishing bile duct syndrome e stenosi extra - epatica ) ed ha modificato lapproccio terapeutico in due casi attraverso la conversione di una ctp in cre e di una cre in ctp ( pazienti 3 e 9 , rispettivamente )  . 
nei rimanenti 12 / 21 pazienti ( 57 , 1% ) ( 4 cre ; 4 ctp ; 4 follow - up ) non c stata modificazione del piano diagnostico - terapeutico prima e dopo la crm . 
 delle procedure colangiografiche invasive previste , 3 ( 2 ctp e 1 cre ) non state effettuate a causa delle condi1256 radiol med ( 2011 ) 116 : 12501266 radiol med ( 2011 ) 116 : 12501266 1257 1258 radiol med ( 2011 ) 116 : 12501266 fig . 
coronal t2 - weighted haste image ( a ) and t2 - weighted thin mip magnetic resonance cholangiography image ( b ) demonstrate a severe bile - duct stenosis at anastomotic site ( arrows )  . 
questi casi sono stati comunque inclusi nellultimo sottogruppo di pazienti descritto sulla base del miglior trattamento possibile cos come programmato dai clinici sulla base dei risultati crm . radiol med ( 2011 ) 116 : 12501266 1259 table 3 confidence rates in concordant and discordant presumptive and magnetic resonance cholangiography ( mrc ) diagnoses , with corresponding gain in confidence patient no . 
 confidence in the presumptive confidence in the mrc diagnosis ( % ) diagnosis ( % ) diagnoses before and after mrc gain in confidence ( % ) a again in confidence was calculated according to carrico et al . 
 [ 22 ] , as explained in the text tabella 3 percentuali di confidenza nelle diagnosi presuntive e colangiografia in risonanza magnetica ( crm ) , concordanti e discordanti , con il rispettivo guadagno in confidenza caso confidenza nella diagnosi presuntiva ( % ) confidenza nella diagnosi crm ( % ) diagnosi prima e dopo la crm guadagno in confidenza ( % ) a 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 100 discordant concordant concordant concordant concordant concordant concordant concordant concordant discordant discordant concordant concordant concordant concordant concordant concordant concordant concordant concordant discordant discordante concordante concordante concordante concordante concordante concordante concordante concordante discordante discordante concordante concordante concordante concordante concordante concordante concordante concordante concordante discordante 100 100 ail guadagno in confidenza stato calcolato in accordo con quanto descritto da carrico et al . 
 [ 22 ] , come spiegato nel testo 1260 radiol med ( 2011 ) 116 : 12501266 table 4 diagnostic - therapeutic plans before and after mrc , and corresponding standard of reference patient no . 
diagnostic - therapeutic plan before mrc diagnostic - therapeutic plan after mrc standard of reference mrc , magnetic resonance cholangiography ; erc , endoscopic retrograde cholangiography ; ptc , percutaneous transhepatic cholangiography aptc was planned but not performed due to contraindications to interventional procedures . 
la crm eseguita nel follow - up ha confermato i reperti precedenti . cla ctp stata programmata ma non stata eseguita per sanguinamento gastrico acuto e rapido peggioramento delle condizioni del paziente . 
la crm eseguita nel follow - up ha confermato i reperti precedenti . radiol med ( 2011 ) 116 : 12501266 1261 before and after mrc and the final standard of reference for each patient . 
in particular , mrc saved planned ercs in two patients with negative examination ( patients 10 and 11 ) , led to four erc and one ptc in five patients ( patients 2 , 5 , 13 and 14 with an mrc diagnosis of extrahepatic stricture , and patient 12 with an mrc diagnosis of vanishing bile - duct syndrome and extrahepatic stricture ) and modified the therapeutic approach in two cases by converting one ptc to erc and vice versa ( patients 3 and 9 , respectively )  . 
in the remaining 12 / 21 ( 57.1% ) patients ( four erc ; four ptc ; four follow - up ) , there was no modification of the diagnostictherapeutic plan before and after mrc . 
 discussion over the last few years , mrc has gained acceptance as a reliable tool for biliary imaging , providing noninvasive diagnosis and accurate preinterventional road maps for biliary complications after olt [ 14 ]  . 
as mrc is noninvasive , performs better than erc in some settings and reduces unnecessary ercs and ptcs in patients with low or intermediate risk of interventional procedures , it has been advocated as the new diagnostic gold standard for the biliary tract [ 7 ]  . 
thus , even though the role for mrc after olt has been poorly investigated and most studies lack a comparison with direct cholangiography [ 25 , 26 ] , mrc is more than promising in evaluating liver - transplanted patients and provides equivalent diagnostic performance compared with direct cholangiography , at least for strictures [ 13 ]  . nonetheless , the primary goal of this study was to assess the impact of mrc on clinical decisions rather than its diagnostic performance . 
such an impact on patients diagnostic and therapeutic management has been traditionally assessed , for imaging techniques , by the hierarchic model of efficacy proposed by thornbury and fryback [ 27 , 28 ]  . 
 according to the model , we investigated the efficacy of mrc in liver - transplanted patients with a combined analysis of level ii ( diagnostic accuracy ) , level iii ( diagnostic thinking efficacy ) and level iv ( therapeutic efficacy ) using a previously described methodology [ 21 , 22 ]  . 
as far as we know , very few studies evaluated levels of efficacy iii and discussione negli ultimi anni la crm diventata strumento affidabile per limaging delle vie biliari , fornendo , in particolare per quanto riguarda le complicanze biliari dopo tof , la possibilit di ottenere una diagnosi non invasiva ed unadeguata mappa pre - interventistica [ 14 ]  . 
essendo una procedura non invasiva , che in alcuni casi permette di ottenere risultati migliori della cre e che riduce lesecuzione di cre e ctp non necessarie in pazienti a rischio basso o indeterminato per procedure interventistiche , la crm stata proposta come nuovo standard diagnostico di riferimento per le vie biliari [ 7 ]  . 
quindi , anche se il ruolo della crm dopo tof stato poco investigato e nonostante nella maggior parte degli studi manchi un confronto con la colangiografia diretta [ 25 , 26 ] , la crm pi che promettente per la valutazione dei pazienti trapiantati di fegato e fornisce una performance diagnostica equivalente a quella della colangiografia diretta , almeno per quel che riguarda le stenosi [ 13 ]  . lobiettivo primario di questo studio stato valutare limpatto della crm sulle decisioni cliniche , piuttosto che misurare la sua performance diagnostica . 
utilizzando tale modello , abbiamo investigato lefficacia della crm nei pazienti trapiantati con unanalisi congiunta di livello ii ( accuratezza diagnostica ) , livello iii ( efficacia diagnostica presuntiva ) e livello iv ( efficacia terapeutica ) , mediante una metodologia descritta in precedenza [ 21 , 22 ]  . 
a nostra conoscenza , solo pochi studi hanno valutato i livelli iii e iv di efficacia per la crm [ 17 , 20 ] e nessuno nel peculiare contesto dei pazienti trapiantati di fegato . 
di conseguenza , a parte il concetto generale delle potenzialit diagnostiche , in gran parte non noto se la crm incida sulle decisioni cliniche che riguardano i pazienti trapiantati di fegato e sul piano diagnostico - terapeutico adottato qualora questo strumento diagnostico non fosse disponibile . preliminarmente , abbiamo valutato la resa diagnostica della crm , parametro che esprime la proporzione di esami positivi tra i pazienti con una particolare indicazione per lindagine stessa [ 21 ]  . 
come regola generale , si presume che i pazienti per i quali un test stato richiesto abbiano una maggiore probabilit di esame con esito positivo rispetto a quelli per cui non stato richiesto . 
pertanto , poich le complicanze biliari sono relativamente frequenti ( tasso di occorrenza del 5 , 8%30% ) e spesso coesistono con altre complicanze maggiori dopo tof [ 14 ] , i pazienti di questo studio , indirizzati alla crm , avevano elevata probabilit di 1262 radiol med ( 2011 ) 116 : 12501266 iv for mrc [ 17 , 20 ] , and there are none in the peculiar setting of liver - transplanted patients . 
consequently , apart from the general issue of diagnostic capability , it is largely unknown whether mrc affects clinical decisions on livertransplanted patients and modifies the diagnostictherapeutic plan that would have been adopted in the absence of this tool . 
 preliminarily , we investigated the diagnostic yield of mrc , which expresses the proportion of positive examinations among patients with a particular indication for the test [ 21 ]  . 
as a general rule , it is assumed that patients in whom a test is ordered are more likely to have a positive result than those in whom the test is not ordered . 
thus , since biliary complications are relatively frequent ( occurrence rate 5.830% ) and often coexist with other major complications after olt [ 14 ] , patients referred for mrc in this study were likely to show biliary disease . 
in fact , a diagnostic test must have a sufficiently high diagnostic yield to be considered useful in a certain clinical setting , as a majority of negative results would imply that patients do not benefit from the test ( because their management remains unchanged ) [ 21 ]  . 
on the other hand , the high diagnostic yield corresponded to a sensitivity of 100% , ppv of 88.9% , npv of 100% and overall accuracy of 92.3% ( 19 / 21 )  . 
apart from the general aforementioned considerations on mrc diagnostic capability , all patients underwent repeated imaging examinations over a reasonable follow - up time ( at least 1 year ) , showing no development of biliary complications . 
thus , the risk of missing mrc - induced false - negative cases is minimal and in any case lower than that of overtreating with invasive procedures ( such as erc or ptc ) in patients with a low likelihood of having biliary complications . 
on the other hand , such likelihood may be inferred by the confidence values in preand post - mrc clinical diagnosis . overall , the use of mrc led to a change in pretest diagmanifestare patologie biliari . 
infatti , un test diagnostico deve determinare una resa diagnostica sufficientemente alta per essere considerato utile in un dato contesto clinico , dal momento che una maggioranza di risultati negativi implicherebbe che i pazienti non traggono beneficio dal test ( perch la loro gestione non viene modificata ) [ 21 ]  . 
daltra parte , lelevata resa diagnostica stata accompagnata da una sensibilit del 100% , un valore predittivo positivo del 88 , 9% , un valore predittivo negativo del 100% e da unaccuratezza globale del 92 , 3% ( 19 / 21 )  . 
ciononostante , la specificit risultata bassa ( 60% ) , in relazione alla presenza di due casi falsi positivi indotti dalla crm , ovvero di due stenosi biliari lievi non confermate alla successiva cre . 
una possibile spiegazione legata al fatto che la crm tende a sovrastimare il grado e lestensione delle stenosi [ 31 ] e che stenosi lievi non fibrotiche possono essere state non visibili alla cre , perch distese dalliniezione del mezzo di contrasto [ 4 , 32 ]  . 
 discutibile se la biopsia epatica o il follow - up mediante imaging rappresentino un valido standard di riferimento in quei 9 pazienti su 21 nei quali la colangiografia diretta non stata effettuata . 
a parte le considerazioni generali sulle capacit diagnostiche della crm descritte sopra , tutti questi pazienti sono stati sottoposti a ripetuti esami strumentali per un periodo di follow - up ragionevole ( almeno un anno ) , senza che si palesassero complicanze biliari . 
il rischio di perdere casi falsi negativi indotti dalla crm dunque minimo , in ogni caso pi basso di quello di trattare eccessivamente mediante procedure invasive ( come cre o ctp ) pazienti con bassa probabilit di avere complicanze biliari . 
tale probabilit pu essere inoltre dedotta dai valori di confidenza nella diagnosi clinica pree post - crm . complessivamente , il ricorso alla crm ha portato ad un cambiamento della diagnosi pre - test in un basso numero di casi ( 4 / 21 ) , corrispondente al 19% dei pazienti . 
tuttavia , la diagnosi clinica delle complicanze biliari difficile , in quanto i sintomi e le alterazioni biochimiche sono spesso indistinguibili da quelle di diverse altre condizioni , rappresentate in buona parte dal rigetto del trapianto [ 25 , 33 ]  . 
nevertheless , clinical diagnosis of biliary complications is difficult , as symptoms and biochemical features are often indistinguishable from those of several different conditions , mainly represented by graft rejection [ 25 , 33 ]  . 
 consequently , in clinical practice , imaging is required to assess biliary findings requiring interventional or surgical procedures and to provide a preoperative road map [ 4 , 34 ]  . 
 however , our study was performed by expert physicians of a tertiary referral centre , who showed except for few cases a high level of confidence in presumptive diagnosis ( mean rating of 80% )  . 
thus , the crucial issue in the clinical decision - making process was to determine whether mrc further increased physicians confidence in a clinically difficult diagnosis rather than to confirm that clinicians were expert in their field . 
 in the remaining four cases , corresponding to those in which mrc led to a final diagnosis discordant from the pre - mrc diagnosis , clinicians showed confidence ratings ranging from 60100% . 
cases included three suspected extrahepatic bile - duct strictures ( with lithiasis in one case ) assessed as negative mrcs , and one suspected vanishing bile - duct syndrome that was finally assessed as an anastomotic stricture . 
 thus , clinicians appeared to consider mrc as a standard of reference , as the examination increased diagnostic confidence irrespective of concordance with pretest diagnosis [ 7 ]  . analysis of therapeutic efficacy showed that clinicians modified the therapeutic plan that would have been applied in the absence of mrc information in 42.8% ( nine ) cases . 
 first , mrc improved therapeutic planning by modifying the interventional approach in two cases of ptc converted in erc and vice versa , which were effective in determining symptom relief . 
daltra parte , il nostro studio stato effettuato da clinici esperti di un centro di riferimento terziario , che hanno dimostrato ad eccezione di pochi casi elevata confidenza nelle diagnosi presuntive ( valore medio dell80% )  . 
il punto cruciale nel processo clinico decisionale stato quindi determinare se la crm avesse aumentato la confidenza dei clinici nelle diagnosi clinicamente difficili , piuttosto che confermare la loro esperienza nel proprio campo . 
in 17 casi ( 81% ) , le diagnosi pree post - crm sono state similari , portando ad un guadagno in confidenza diagnostica statisticamente significativo e pari al 18 , 8% . 
 nei restanti 4 / 21 casi , corrispondenti a quelli nei quali la crm ha indotto una diagnosi finale discordante rispetto a quella pre - esame , i clinici hanno dimostrato una confidenza variabile dal 60% al 100% . 
i casi comprendevano 3 sospette stenosi extraepatiche ( con associata litiasi in un caso ) valutate come negative alla crm ed una sospetta vanishing bile duct syndrome successivamente inquadrata come stenosi anastomotica . 
i clinici sembrano dunque considerare la crm come uno standard di riferimento , dal momento che lesame ha aumentato la confidenza diagnostica indipendentemente dalla concordanza con la diagnosi pre - test [ 7 ]  . lanalisi di efficacia terapeutica ha dimostrato che i clinici hanno modificato il piano terapeutico che sarebbe stato applicato in assenza delle informazioni fornite dalla crm nel 42 , 8% dei casi ( 9 / 21 )  . 
in primo luogo , la crm ha migliorato il piano terapeutico modificando lapproccio interventistico in 2 casi di conversione da ctp a cre e viceversa , indagini che sono state efficaci nel determinare un miglioramento dei sintomi . 
 [ 35 ] , non abbiamo usato la riduzione del carico di lavoro della cre come outcome per valutare lutilit della crm , dal momento che i pazienti possono trarre beneficio non solo dallevitare procedure invasive ( come successo in due pazienti con esami negativi )  . 
in our opinion , mrc was useful in those in whom imaging follow - up was confirmed , as alternative diagnostic techniques such as us or ct provide less accurate information on the biliary tract , as previously demonstrated [ 3639 ]  . 
in these cases , although mrc cannot be considered useful according to the purposes of the study , it can be argued that indirectly it would avoid invasive monitoring of the treatment . our study has several limitations . 
nevertheless , our results reflect clinical practice because anastomotic and / or nonanastomotic strictures represent the most frequent biliary complications , both early and late , after transplantation [ 14 ]  . 
nevertheless , us has been repeatedly shown to be inaccurate in assessing biliary complications , particularly the site of stricture and biliary dilation upstream , with sensitivity < 50% [ 12 , 36 , 40 ]  . 
 in conclusion , in the clinical setting of liver - transplanted patients , mrc shows a high diagnostic yield due to the prevalence of disease and to the well - established diagnostic accuracy . 
mrc significantly increases diagnostic confidence of referring physicians irrespective of the concordance between the preand posttest diagnosis , although with a limited risk of overtreatment of false - positives cases . 
 moreover , mrc leads to a change in patient management that is effective in at least one third of patients . nostro parere , la crm stata utile nei casi in cui tale indagine ha confermato la scelta pre - test di follow - up mediante imaging , dal momento che le tecniche diagnostiche alternative alla crm ( quali ecografia e tc ) forniscono informazioni sulle vie biliari meno accurate , come precedentemente dimostrato [ 3639 ]  . 
inoltre , nei pazienti nei quali la scelta della colangiografia diretta stata confermata , la crm ha fornito un quadro basale da confrontarsi con le successive rivalutazioni rm post - interventistiche . 
anche se , in questi casi , la crm non pu essere considerata utile secondo gli scopi dello studio , si pu desumere che , indirettamente , essa possa evitare un monitoraggio invasivo post - trattamento . il nostro studio presenta diversi limiti . 
tuttavia i nostri risultati riflettono la pratica clinica , in quanto le stenosi anastomotiche e / o nonanastomotiche sono le complicanze biliari post - trapianto ( precoci e tardive ) pi frequenti [ 14 ]  . 
un limite ancora pi importante legato al fatto che la confidenza pre - crm dei clinici di riferimento possa essere stata falsata dai risultati di precedenti indagini di imaging , ad esempio dallecografia . 
tuttavia , lecografia si pi volte dimostrata poco adeguata nella valutazione delle complicanze biliari , in particolare nella rilevazione della sede della stenosi e della dilatazione a monte , con una sensibilit inferiore al 50% [ 12 , 36 , 40 ]  . 
pertanto , limpatto dellecografia sulla confidenza diagnostica dovrebbe essere ragionevolmente basso e in ogni caso non dovrebbe pregiudicare la capacit della crm di influenzare il processo clinico di decision making . 
 inoltre , dal momento che lecografia una tecnica di primo livello a basso costo e largamente utilizzata nella valutazione dei pazienti dopo tof , sarebbe non etico non farne ricorso . 
complessivamente , ulteriori studi dovrebbero indagare livelli pi elevati di efficacia diagnostica , mediante valutazioni degli effetti sulloutcome dei pazienti o analisi costo - efficacia [ 27 , 28 ]  . in conclusione , nel contesto clinico dei pazienti trapiantati di fegato la crm dimostra unelevata resa diagnostica , grazie alla prevalenza della patologia biliare ed alla ben codificata accuratezza diagnostica . 
la crm incrementa significativamente la confidenza diagnostica dei clinici di riferimento indipendentemente dalla concordanza tra le diagnosi pree post - test , al costo di un limitato rischio di overtreatment per i casi falsi positivi . 
grassi4 1department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 2department of radiology , scientific institute hospital css , viale cappuccini 1 , 71013 san giovanni rotondo , foggia , italy 3department of radiology , university of ancona , hospital torrette , via conca 60 , 60100 ancona , italy 4department of rheumatology , universit politecnica delle marche , via dei colli 52 , 60035 jesi , ancona , italy correspondence to : g . 
forty - three consecutive patients with sacroiliitis as the predominant symptom of a rheumatic disorder were retrospectively studied . radiography , computed tomography ( ct ) and magnetic resonance ( mr ) imaging were performed . 
the following imaging findings were evaluated : bone marrow oedema , intra - articular effusion , synovial reaction , joint - space widening , bone sclerosis or hyperostosis , subchondral erosions and , in final stages , joint - space narrowing and ankylosis . 
radiography demonstrated bone sclerosis in 10 patients ( 23% ) , subchondral erosions in 15 ( 34% ) , jointspace widening in 8 ( 18% ) , joint - space narrowing in 17 ( 39% ) and ankylosis in 3 ( 6% )  . 
ct examination showed sclerosis of the sacroiliac joint in 17 patients ( 41% ) , subchondral erosions in 21 ( 53% ) , joint - space widening in 22 ( 53% ) , joint - space narrowing in 18 ( 43% ) and ankylosis in 7 ( 17% )  . 
at mr , we found bone marrow oedema in 25 patients ( 92% ) , intra - articular effusion in 26 ( 96% ) , synovial reaction in 21 ( 77% ) and joint - space widening in 5 ( 18% )  . 
la radiografia convenzionale ha dimostrato la sclerosi ossea in 10 pazienti ( 23% ) , erosioni subcondrali in 15 pazienti ( 34% ) , ampliamento dello spazio articolare in 8 pazienti ( 18% ) e restringimento in 17 pazienti ( 39% ) , anchilosi in 3 pazienti ( 6% )  . 
allesame tc sono stati osservati sclerosi dellarticolazione sacroiliaca in 17 pazienti ( 41% ) , erosioni subcondrali in 21 pazienti ( 53% ) , ampliamento dello spazio articolare in 22 pazienti ( 53% ) , restringimento dello spazio articolare in 18 pazienti ( 43% ) e anchilosi in 7 pazienti ( 17% )  . 
alla rm abbiamo riscontrato edema del midollo osseo in 25 pazienti ( 92% ) , radiol med ( 2011 ) 116 : 292301 problem of difficult diagnostic evaluation due to the complexity of the anatomical region and the variability of radiographic findings . 
the integrated use of conventional radiography , ct and mr imaging is suggested to avoid misdiagnosis . keywords spondyloarthropathies sacroiliac joint sacroiliitis conventional radiography computed tomography magnetic resonance imaging versamento intrarticolare in 26 pazienti ( 96% ) , reazione sinoviale in 21 pazienti ( 77% ) e lampliamento dello spazio articolare in 5 pazienti ( 18% )  . 
lo studio radiologico delle articolazioni sacro - iliache in pazienti affetti da diverse malattie reumatiche rappresenta un problema di difficile valutazione diagnostica sia per la complessit della regione anatomica sia per la variabilit dei risultati radiografici . 
 parole chiave spondilo - artropatie articolazioni sacroiliache sacro - ileite radiologia convenzionale tomografia computerizzata risonanza magnetica introduction introduzione the sacroiliac joints ( sij ) represent an amphidiarthrosis with features between amphiarthrosis and diarthrosis . 
involvement of the sij is a major and characteristic feature of the early spondyloarthropathies ( spa ) , and the most common symptom in adults is inflammatory low back pain due to sacroiliitis [ 2 ]  . included in the spectrum of spa are ankylosing spondylitis ( as ) , psoriatic arthritis ( psa ) , enteropathic spa ( enspa ) , reactive arthritis and undifferentiated spondyloarthropathy ( uspa )  . 
spa is classified according to the european spondyloarthropathy study group criteria ( essg ) [ 5 ] and amor criteria [ 6 ] and as by the modified new york criteria [ 7 ]  . in the case of early as in particular , criteria sets fall short because the classification of as depends on the presence of radiological sacroiliitis , which often appears late in the course of the disease [ 8 , 9 ]  . 
the international assessment in ankylosing spondylitis ( asas ) working group has recognised imaging as an important domain in spa and recommends further development for use in clinical trials [ 11 ]  . magnetic resonance ( mr ) imaging is becoming an important tool for assessing inflammation and structural damage in as . 
the advantages of mr imaging compared with computed tomography ( ct ) and radiography are that it also provides early visualisation of active inflammatory changes , making it possible to diagnose sacroiliitis before le articolazioni sacro - iliache ( asi ) rappresentano un anfidiartrosi con caratteristiche tra lanfiartrosi e la diartrosi . 
il coinvolgimento delle asi una caratteristica importante e tipica delle spondilo - artropatie in fase iniziale , e il sintomo pi comune negli adulti il dolore lombare dovuto alla sacro - ileite [ 2 ]  . sono incluse nello spettro delle spondilo - artropatie la spondilite anchilosante , lartrite psoriasica , le spondilo - artropatie enteropatiche , lartrite reattiva e le spondilo artropatie indifferenziate . 
gli attuali criteri di classificazione delle spondilo - artropatie sono quelli definiti dalleuropean spondyloarthropathy study group ( essg ) [ 5 ] , nonch i criteri amor [ 6 ] e quelli per la classificazione della spondilite anchilosante , i criteri di new york modificati [ 7 ]  . comunque , soprattutto nel caso di una spondilite anchilosante in fase iniziale , i criteri sopra menzionati sono meno presenti , poich la classificazione della spondilite anchilosante dipende dalla presenza di segni radiologici di sacroileite , che appare spesso tardivamente nel corso della malattia [ 8 , 9 ]  . 
linternational assessment in ankylosing spondylitis ( asas ) working group ha riconosciuto limaging come un importante aspetto nella diagnosi radiologica delle spondilo - artropatie e ne raccomanda un ulteriore sviluppo e lutilizzo nelle sperimentazioni cliniche [ 11 ]  . 
la risonanza magnetica ( rm ) sta diventando uno strumento sempre pi importante nella valutazione della flogosi e del 294 radiol med ( 2011 ) 116 : 292301 definite joint destruction is detectable on ct or radiography [ 1215 ]  . the aim of this study was to retrospectively evaluate the role of the different imaging techniques in the study of the sij in patients with spa and other rheumatic conditions and to assess potential pitfalls in the radiological diagnosis . materials and methods patients this retrospective study included 43 consecutive patients ( 19 men and 24 women ; age 2181 years ; mean age 51 years ) who were either inpatients and outpatients of our hospital with clinically confirmed spa and other rheumatic conditions involving the sij and a history of inflammatory back pain ( ibp ) and were evaluated between september 2007 and january 2009 . 
 characteristics , radiological imaging techniques conventional radiography was obtained with a 20 caudal tube tilt and included an anteroposterior projection of the sacru the anatomical sites studied were the entire sacrum and the sij . 
grade 2 , definite early changes including pseudowidening of the joint space and / or focal erosions , sclerosis of the bone usually on both sides of the joint space and frequent blurring of the joint margins ; 2a unilateral changes and 2b bilateral changes . 
grade 3 , severe destructive changes , erosions and pseudowidening of joint space more marked than in grade 2 ; arthritic changes are always bilateral , and there may be small bony bridges . grade 4 , regressive changes with bilateral arthritic changes , narrowing of the joint space with bony bridges in one or both sij and slight sclerosis of the joints . 
grade 5 , terminal changes , with pronounced signs of bony ankylosis in both sij and slight sclerosis of the joints . ct study ( tct 900s toshiba , japan ) was performed under basal conditions only . 
i vantaggi della rm rispetto alla tomografia computerizzata ( tc ) e alla radiografia convenzionale consistono nella capacit della metodica di rilevare precocemente alterazioni infiammatorie attive , rendendo possibile la diagnosi di sacro - ileite prima della diagnosi tardiva caratterizzata da alterazioni articolari rilevabili alla tc o alla radiografia [ 1215 ]  . lobiettivo di questo studio stato quello di valutare retrospettivamente il ruolo delle diverse tecniche di imaging nello studio delle asi , nei pazienti con spondilo - artropatie ed altre patologie reumatiche e per valutare potenziali errori nella diagnosi radiologica . materiali e metodi pazienti in questo studio retrospettivo , sono stati valutati , da settembre 2007 a gennaio 2009 , 43 pazienti consecutivi ( 19 maschi e 24 femmine ) , dai 21 agli 81 anni ( et media 51 anni ) , comprendenti pazienti sia ambulatoriali che in regime di ricovero del nostro ospedale , con spondilo - artropatie ed altre patologie reumatiche coinvolgenti le asi , confermate clinicamente dai colleghi reumatologi e con una storia clinica di dolore lombare irradiato al sacro . 
nella nostra popolazione di studio , 19 pazienti erano affetti da spondilite anchilosante , 11 pazienti da artrite psoriasica , 7 pazienti da spondilo artropatie enteropatiche , 4 pazienti da artrite reattiva e 2 pazienti da spondilo artropatie indifferenziate . tecniche di imaging il radiogramma tradizionale stato ottenuto con uninclinazione caudale del tubo di 20 e comprende la proiezione antero - posteriore del sacro . 
le regioni anatomiche studiate sono state il sacro e le articolazioni sacro - iliache ; le alterazioni morfologiche analizzati sono state : lampliamento dello spazio articolare , la sclerosi ossea o iperostosi , le erosioni subcondrali e , nelle fasi finali , il restringimento degli spazi articolari e lanchilosi . 
 mr images were obtained using a pelvic array coil in the semiaxial and semicoronal planes along the main axis of the sij and with patient lying in the supine decubitus . 
the sequences performed on mr ( signa 1.5 - t unit , ge medical spazio articolare , margini articolari spesso sfumati ; 2a : le alterazioni sopra descritte sono unilaterali ; 2b : le alterazioni descritte sono bilaterali ; grado 3 , severe alterazioni distruttive , erosioni e pseudo - ampliamento dello spazio articolare pi marcato rispetto al grado 2 ; le alterazioni di tipo artritico sono sempre bilaterali ; piccoli ponti ossei possono essere presenti ; grado 4 , alterazioni regressive ; alterazioni di tipo artritico bilaterali , restringimento dello spazio articolare con ponti ossei in una o entrambe le articolazioni , modesta sclerosi sub condrale ; grado 5 , 296 radiol med ( 2011 ) 116 : 292301 systems , milwaukee , wi , usa ) were : semicoronal t1weighted spin echo ( se ) with fat saturation ( tr / te 500 / 20 ; thickness 3 mm ; intersection gap 1 mm ; nex 2 ; matrix 256224 ; fov 18 cm ; time 3 min 52 s ; slices 68 ) , semiaxial t2 - weighted fast spin echo ( fse ) and semicoronal short - tau inversion recovery ( stir ) - fse ( tr / te / etl 3 , 000 / 90 / 8 ; matrix 256256 ; ti 150 ms ; time 3 min24 s ; slices 68 fse and 6 stir - fse ) under basal conditions , and semicoronal and semiaxial t1 - w with fat saturation ( tr / te 500 / 20 ; matrix 256224 ; time 3 min 52 s ; slices 68 ) after intravenous administration of gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa ) ( magnevist , bayer , berlin , germany )  . 
 all imaging studies were independently reviewed by two musculoskeletal radiologists ( gg and ac , the first with more than 20 years of experience in the field and the second with less experience ) who were blinded to the results . 
from a pathological point of view , articular involvement consists of an inflammatory process with proliferation of the serous lining cells , exudative effusion and synovial pannus , which erodes the articular cartilage and penetrates trabecular bone with geode formation . 
in early as and uspa , sacroiliitis table 2 radiological features evaluated with the different imaging techniques and number of patients , expressed as absolute number and percentage , in whom these findings were observed hyperostosis bone sclerosis joint - space widening joint - space narrowing subchondral erosions ankylosis synovial reaction intra - articular effusion bone marrow oedema x - ray 5 ( 11% ) 10 ( 23% ) 8 ( 18% ) 17 ( 39% ) 15 ( 34% ) 3 ( 6% ) 5 ( 18% ) 15 ( 36% ) no 17 ( 41% ) no 22 ( 53% ) 18 ( 43% ) no 22 ( 53% ) no 7 ( 17% ) 21 ( 77% ) 26 ( 96% ) 25 ( 92% ) ct , computed tomography ; mri , magnetic resonance imaging tabella 2 aspetti radiologici valutati con le diverse tecniche di imaging e numero di pazienti , espressi in valore assoluto ed in percentuale , nei quali sono state riscontrate le alterazioni iperostosi sclerosi ossea ampliamento spazio articolare riduzione spazio articolare erosioni subcondrali anchilosi reazione sinoviale versamento intrarticolare edema del midollo osseo 5 ( 11% ) 10 ( 23% ) 8 ( 18% ) 15 ( 36% ) no 17 ( 41% ) no 22 ( 53% ) 5 ( 18% ) 17 ( 39% ) 18 ( 43% ) no 15 ( 34% ) 3 ( 6% ) 22 ( 53% ) no 7 ( 17% ) 21 ( 77% ) 26 ( 96% ) 25 ( 92% ) rx , radiografia ; tc , tomografia computerizzata ; rm , risonanza magnetica alterazioni irreversibili ; segni evidenti di anchilosi ossea in entrambe le articolazioni , lieve sclerosi delle articolazioni . 
le scansioni di serie sono state ottenute con il paziente in posizione supina con una inclinazione craniale del gantry di 2530 per ottenere immagini semicoronali attraverso entrambe le parti cartilaginee e legamentose delle asi e con uno spessore di fetta di 2 mm ; scansioni contigue sono state ottenute a intervalli di 2 millimetri , con tecnica ad alta risoluzione . 
 le immagini rm sono state ottenute utilizzando una bobina pelvica , lungo piani di scansione semiassiali e semicoronali , lungo lasse principale delle articolazioni sacro - iliache e con il paziente in decubito supino . 
alla rm ( signa 1 , 5 t , ge medical systems , milwaukee , wis ) , le sequenze eseguite sono state : semicoronale t1 - pesata con saturazione del grasso ( spin echo [ se ] t1 - w ; tempo di ripetizione [ tr ] / tempo di eco [ te ] 500 / 20 ; spessore 3 mm ; intersection gap 1 mm ; nex 2 ; matrice 256224 , campo di vista [ fov ] 18 cm ; tempo 3 min e 52 s ; 68 slices ) , semiassiale t2 - pesata ( fast spin echo [ fse ] t2 - w ) e semicoronale short - tau inversion recovery ( stir ) radiol med ( 2011 ) 116 : 292301 fse ( tr / te / echo train length [ etl ] 3000 / 90 / 8 ; matrice 256256 ; ti 150 m ; tempo 3 min e 24 s ; 68 slices fse e 6 stir - fse ) in condizioni basali , e semicoronale e semiassiale t1 - pesata con saturazione del grasso ( tr / te500 / 20 ; matrice 256224 ; tempo 3 min e 52 s ; 68 slices ) dopo somministrazione di gadobenato dimeglumina ( gd - dtpa ) ev ( magnevist , bayer , berlino , germania )  . 
 tutte le indagini radiologiche sono state soggette a revisione indipendente da due radiologi muscolo - scheletrici ( gg e ac , il primo con pi di 20 anni di esperienza nel settore , il secondo con meno esperienza ) , che non erano a conoscenza dei risultati . 
lindagine tc ha dimostrato meglio dello studio radiologico tradizionale le lesioni ossee reattive a livello delle articolazioni sacro - iliache , perch non influenzato da problemi proiettivi tipici dellesame radiologico . 
da un punto di vista anatomo - patologico , il coinvolgimento articolare consiste in un processo infiammatorio , con proliferazione delle cellule di rivestimento sieroso , effusione essudativa e nella formazione del panno sinoviale che erode la cartilagine articolare e penetra nell osso trabecolare con la formazione di geodi . 
2 immagine tc semicoronale che dimostra erosioni subcondrali bilaterali e sclerosi , con riduzione dello spazio articolare . is also the most common early clinical finding and the presumed first manifestation of the disease . 
especially in the case of early spa , criteria sets fall short , so a long delay may exist between the start of symptoms and establishing a diagnosis [ 16 , 17 ]  . radiography has a high specificity but a low sensitivity , which can delay the diagnosis for several years . 
5 immagine rm semicoronale t1 - pesata che mostra edema del midollo osseo a livello del sacro . are related to the overlap of the ilium with the sacrum on standard anteroposterior projections , because the s - shaped joint structures course obliquely from a lateral to a medial position . 
4 immagine rm semicoronale t1 - pesata che mostra edema ed iperemia dellosso sub - condrale , principalmente sul versante iliaco delle articolazioni . allanchilosi , inizialmente fibrosa e successivamente ossea [ 13 ]  . 
specialmente nel caso di spondilite anchilosante in fase iniziale , i criteri di classificazione comunemente utilizzati sono meno presenti , cos pu esserci un ritardo tra linizio dei sintomi e la diagnosi [ 16 , 17 ]  . 
i limiti di questa tecnica sono legati alla sovrapposizione dellileo con losso sacro sulla proiezione antero - posteriore standard , perch le strutture articolari , a forma di s , hanno decorso obliquo in senso latero - mediale . nonostante i suoi limiti noti , lo studio radiologico sempre lo strumento iniziale per la valutazione delle articolazioni sacro - iliache [ 18 ]  . 
 la tc e la rm , come dimostrato nel nostro studio , sono superiori al radiogramma per lindividuazione dei segni di base , quali erosioni , sclerosi , distruzione della cartilagine ed edema del midollo osseo e quindi per la diagnosi di sacroileite . 
in particolare , per lindividuazione precoce di alterazioni ossee , come erosioni e anchilosi , la tc si dimostrata superiore alla rm ; daltra parte , la rm permette una valutazione della cartilagine e delledema del midollo osseo , non rilevati alla tc [ 1928 ]  . 
non c un metodo stabilito per la valutazione dei reperti patologici delle articolazioni sacro - iliache alla rm , anche se la necessit di questo evidente come riportato da puhakka et al . radiol med ( 2011 ) 116 : 292301 fig . 
b immagine rm semicoronale con soppressione del grasso t1 - pesata dopo somministrazione di gadolinio che mostra aree di ipervascolarizzazione , segno di infiammazione attiva . imaging ; on the other hand , mr imaging is better for depicting the cartilage and bone marrow oedema , which is not detected by ct [ 1928 ]  . 
 [ 20 ] introduced a method mainly based on signal changes on t1 , t2 , and phase - contrast sequences : type i lesions were characterised by low signal intensity on t1 - weighted images and a high signal intensity on both phase - contrast and t2weighted images . 
 [ 12 ] described a grading system for disease activity based on quantitative evaluation of contrast enhancement at dynamic mr imaging and used the new york criteria to evaluate joint involvement [ 7 ]  . 
 [ 20 ] hanno introdotto un metodo basato principalmente sui cambiamenti del segnale in t1 , t2 e nelle sequenze in contrasto di fase : le lesioni di tipo i sono caratterizzate da una bassa intensit di segnale nelle immagini t1 pesate e da una elevata intensit di segnale sia nelle sequenze in contrasto di fase sia nelle immagini pesate in t2 . 
usando questo sistema di punteggio , si potuto dimostrare che la risonanza magnetica in grado di rilevare le alterazioni patologiche delle articolazioni sacroiliache nei pazienti con scarse o nessuna evidenza clinica di malattia [ 17 ]  . 
nella nostra esperienza , la tc e la rm possono aiutare nella diagnosi precoce e nella diagnosi differenziale da altre condizioni morbose quali 300 radiol med ( 2011 ) 116 : 292301 clinical findings [ 17 ]  . 
in our experience , ct and mr imaging may help in the early diagnosis and differentiation from other conditions such as bone tumours or nerve root pathologies , which can cause sacroiliitis [ 29 ]  . this study has some limitations . 
finally , inflammatory back pain , the most important clinical sign we considered , is not always indicative of sij involvement . despite these limitations , this study confirmed that the diagnosis of sacroiliitis in the course of rheumatic diseases remains a challenge and that integration of the various imaging techniques is needed for correct clinical and radiological classification . tumori ossei o le patologie delle radici nervose che si manifestano clinicamente con una sacro ileite [ 29 ]  . il presente lavoro mostra alcuni limiti . 
tra questi dobbiamo considerare la eterogeneit della popolazione di studio in relazione allet , al sesso , alla durata dei sintomi clinici e alla malattia da cui i pazienti erano affetti . 
pur con queste limitazioni , il presente studio ha confermato che la diagnosi di sacro ileite in corso di patologie reumatiche rappresenta un problema di difficile valutazione diagnostica e che lintegrazione delle diverse tecniche di imaging fondamentale per un corretto inquadramento clinico - radiologico . 
rossi , universit di verona , verona , italy 3radiologia , ospedale misericordia , grosseto , italy 4cardiologia , 5radiologia clinica , ospedale c foncello treviso , treviso , italy correspondence to : a . 
twenty - two consecutive patients with a known diagnosis of hcm were prospectively evaluated , with echocardiography and cardiac mr imaging performed within 2 weeks of each other ( mean interval 7 days , range 214 days )  . 
the following parameters were calculated for both techniques : myocardial mass , wall thickness , end - diastolic volume ( edv ) , end - systolic volume ( esv ) , ejection fraction ( ef ) , systolic anterior motion ( sam ) of the mitral valve and degree of myocardial fibrosis ( based on the ultrasonic reflectivity at echocardiography and degree of late enhancement at cardiac mr imaging )  . 
ventidue pazienti consecutivi con diagnosi nota di cmi sono stati prospetticamente valutati mediante eco - cardiografia e cardio - rm eseguite entro 2 settimane ( scarto medio 7 giorni , range 214 giorni )  . 
per entrambe le tecniche sono stati calcolati massa cardiaca , spessori di parete , volume telediastolico ( vtd ) e telesistolico ( vts ) , frazione di eiezione ( fe ) , spostamento anteriore del lembo mitralico ( sam ) , grado di fibrosi parietale ( basato sul valore di eco - rinfrangenza alleco - cardiografia e sullentit di impregnazione tardiva alla cardio - rm )  . 
la diagnosi di cmi stata confermata in tutti i pazienti con entrambe le metodiche , con concordanza 198 radiol med ( 2011 ) 116 : 197210 terms of the site of disease . 
cardiac mr imaging correlates well with echocardiography in defining the morphological and functional parameters useful for the imaging diagnosis of hcm and therefore , in selected cases ( poor acoustic window , doubtful echocardiography findings ) , it may be a valid alternative to echocardiography . assoluta per quanto riguarda la sede . 
la cardio - rm correla bene con lecocardiografia nella definizione dei parametri morfologici e funzionali utili per la diagnosi strumentale di cmi e pu pertanto rappresentare , in casi selezionati ( scarsa finestra acustica , rilievi eco - cardiografici dubbi ) , una valida alternativa alleco - cardiografia . keywords hypertrophic cardiomyopathy echocardiography cardiac magnetic resonance myocardial fibrosis parole chiave cardiomiopatia ipertrofica ecocardiografia risonanza magnetica cardiaca fibrosi parietale introduction introduzione hypertrophic cardiomyopathy ( hcm ) is an autosomal dominant hereditary disease with variable penetrance and is characterised by left ( lv ) and / or right ( rv ) ventricular hypertrophy in the absence of demonstrable organic causes , both at the cardiac and systemic levels [ 1 , 2 ]  . 
the disease is characterised by possibly fatal cardiac arrhythmias and is an important cause of sudden death in individuals younger than 35 years of age ( 3%6% of cases per year ) [ 3 ]  . 
disease prevalence is around 0.1%0.2% , but these figures are based on screening by physical examination and electrocardiogram , which may show no alterations in patients with hcm [ 4 ]  . echocardiography , which is able to quantify myocardial thickening and evaluate lv motion , is the first - choice imaging technique for diagnosing hcm [ 5 , 6 ]  . 
however , the intrinsic limitations of the technique ( operator dependence and adequate acoustic window ) limit its ability to confirm diagnosis and correctly assess the disease [ 68 ]  . various studies have demonstrated the accuracy of cardiac magnetic resonance ( mr ) imaging in evaluating ventricular disease , thanks to its ability to provide both morphological and functional data , as well as information on myocardial perfusion [ 911 ]  . 
in addition , cardiac mr imaging is useful in diagnosing apical hcm , which , due to the poor acoustic window , is particularly difficult to evaluate with echocardiography [ 7 ]  . 
 the aim of this study , therefore , was to prospectively la cardiomiopatia ipertrofica ( cmi ) una malattia ereditaria autosomica dominante a penetranza variabile che consiste nella presenza di ipertrofia ventricolare sinistra e / o destra in assenza di cause organiche dimostrabili , sia a livello cardiaco che sistemico [ 1 , 2 ]  . 
tale patologia predispone ad aritmie cardiache fatali ed una importante causa di morte improvvisa in et inferiore ai 35 anni ( 3%6% di casi allanno ) [ 3 ]  . la prevalenza della malattia di circa 0 , 1%0 , 2 % , ma questi dati derivano da screening svolti mediante esame obiettivo ed elettrocardiogramma , che possono risultare non alterati in pazienti con cmi [ 4 ]  . leco - cardiografia rappresenta la metodica di prima linea per la diagnosi strumentale di cmi , consentendo di quantificare lispessimento miocardico e valutare la cinetica del ventricolo sinistro ( vsn ) [ 5 , 6 ]  . 
tuttavia , i limiti intrinseci della metodica ( dipendenza dalloperatore e dalla finestra acustica del paziente ) , rendono leco - cardiografia talora insufficiente per una diagnosi di certezza e per un corretto bilancio di malattia [ 68 ]  . 
diversi studi hanno dimostrato laccuratezza della risonanza magnetica cardiaca ( cardio - rm ) nella valutazione delle patologie ventricolari , grazie alla sua capacit di fornire informazioni di tipo morfologico , funzionale , nonch sulla perfusione miocardica [ 911 ]  . 
inoltre la cardio - rm utile nella diagnosi di cmi apicale , forma che per la scarsa finestra acustica spesso particolarmente difficile da valutare con eco - cardiografia [ 7 ]  . 
tuttavia , sono pochi gli studi in letteratura che descrivono il ruolo ed i criteri diagnostici della cardio - rm nella valutazione della cmi [ 10 , 12 , 13 ]  . 
 radiol med ( 2011 ) 116 : 197210 compare morphological and functional findings obtained with echocardiography and cardiac mr imaging to determine which ones are useful in evaluating hcm , with special attention to evaluating associated myocardial fibrosis . 
 pertanto , lobiettivo di questo studio confrontare in maniera prospettica i rilievi morfologici e funzionali ottenuti mediante eco - cardiografia e cardio - rm utili nella valutazione della cmi , con particolare attenzione alla valutazione della fibrosi miocardica associata . 
 materials and methods materiali e metodi patients and inclusion criteria pazienti e criteri di inclusione a review of the cardiology database performed between december 2005 and february 2009 identified 105 patients with hcm who were eligible for inclusion in our study . only patients with a known diagnosis of primary hcm , obtained according to the world health organization criteria ( clinical and m - mode echocardiography demonstrating increased wall thickness in end diastole > 15 mm at the level of the septum or posterior wall ) , in the absence of other demonstrable causes of ventricular hypertrophy [ 14 ] , were included in the study and examined prospectively with echocardiography and cardiac mr imaging within 2 weeks of each other ( mean interval 7 days , range 214 days )  . 
patients affected by possible causes of secondary hcm ( aortic stenosis , amyloidosis or arterial hypertension ; n = 44 ) and those without a comparative study with both techniques ( n = 39 ) were excluded . 
in agreement with the ethics committee , all patients enrolled gave written informed consent before the diagnostic examinations were performed . echocardiography protocol the echocardiography examination was performed with an acuson sequoia 512 device ( mountain view , ca , usa ) with a 3 - v , 2 - c transducer and software for calculating myocardial mass and digitising the epicardial and endocardial profiles in the short axis . 
the lv was then divided into 17 segments according to the guidelines of the american society of echocardiography , and maximum lv wall thickness values were recorded in end diastole and end systole . 
sono stati inclusi solo i pazienti con diagnosi nota di cmi primitiva , ottenuta secondo i criteri della world health organization ( esame clinico ed eco - cardiografico mmode tramite dimostrazione di aumentato spessore parietale in telediastole > 15 mm a livello del setto o della parete posteriore ) , in assenza di altre cause dimostrabili di ipertrofia ventricolare [ 14 ] , studiati prospetticamente mediante ecocardiografia e cardio - rm entro 2 settimane ( scarto medio 7 giorni , range 214 giorni )  . 
sono stati esclusi dallo studio i pazienti affetti da possibili cause di cmi secondaria ( stenosi aortica , amiloidosi o ipertensione arteriosa ; n = 44 ) e quelli che non disponevano di studio comparativo con entrambe le metodiche ( n = 39 )  . 
in accordo con il comitato etico tutti i pazienti arruolati nello studio hanno firmato un consenso informato prima dellesecuzione di entrambi i test diagnostici . protocollo eco - cardiografia per leco - cardiografia stato utilizzato un apparecchio acuson sequoia 512 ( mountain view , ca , usa ) con trasduttore 3v2c dotato di software per il calcolo della massa cardiaca con digitalizzazione dei profili dellepicardio e dellendocardio in asse corto . 
il ventricolo sinistro stato quindi suddiviso in 17 aree , in accordo alle linee guida della societ americana di eco - cardiografia , e sono stati ottenuti i valori di massimo spessore del vsn in telediastole ( td ) ed in telesistole ( ts )  . 
 cardiac mr imaging protocol protocollo cardio - rm all cardiac mr examinations were performed with a 1.5tutte le indagini cardio - rm sono state eseguite con un 200 radiol med ( 2011 ) 116 : 197210 t magnet ( avanto , siemens medical systems , erlangen , germany ) and a phased - array coil . 
images were acquired in the axial and coronal planes with half - fourier acquired single - shot turbo spin - echo ( haste ) sequences and balanced true fast imaging with steady - state precession ( true - fisp ) sequences to obtain cine images along three axes ( short , two - chamber long and four - chamber views ) , with breathhold acquisitions of around 15 cardiac cycles . 
the following parameters were used for the cine sequences : tr / te = 35 ms / 1.8 ms ; flip angle , 60 ; slice thickness , 8 mm ; acquisition time , 1520 s according to heart rate ; receiver bandwidth , 930 hz / pixel ; matrix , 256256 ; fov , 300350 m the images for evaluating delayed enhancement ( de ) were obtained after administration of 0.2 mmol / kg of gadolinium chelates ( dotarem , guerbet , france ) at a flow rate of 2 ml / s . 
images were obtained 10 min after the injection of contrast material in the same planes with t1 - weighted 3d inversion recovery ( ir ) sequences and the following acquisition parameters : tr / te = 7 ms / 3 ms ; flip angle , 15 ; voxel dimensions , 1.41.41.2 mm , 32 lines of the k - space calculated for each r - r interval in end diastole ; fov , 340265 cm ; matrix , 192256 ; 16 cardiac cycles sampled over a single breath - hold . 
to increase diagnostic confidence , the de images were also obtained with phase - sensitive ir ( psir ) true - fisp sequences with the following parameters : tr / te = 2.2 / 11 ; flip angle , 50 ; voxel dimensions , 1.41.41.2 mm ; fov , 340265 cm ; matrix , 192102 ; 16 cardiac cycles sampled during a single breath - hold . mean acquisition time was 30 m postprocessing analysis of the true - fisp sequences to calculate the myocardial mass and ef was performed with a dedicated software package ( argus , siemens , erlangen , germany )  . turbo - flash image analysis echocardiography and cardiac mr studies were evaluated blind by a cardiologist and a radiologist , respectively , who were both expert in cardiac imaging and unaware of the prior clinical and imaging findings . 
on the basis of a series of images acquired during an entire cardiac cycle in the short axis , from the base to apex of the heart , the images magnete da 1 , 5 t ( avanto , siemens medical systems , erlangen , germania ) con bobina phased - array . 
sono state acquisite immagini nei piani assiale e coronale con sequenze half - fourier acquired single - shot turbo spin - echo ( haste ) e successive sequenze bilanciate truefast imaging with steady state precession ( fisp ) per ottenere immagini cine lungo i tre assi ( asse corto , due camere asse lungo e 4 camere ) , con acquisizioni in apnea della durata di circa 15 cicli cardiaci . 
i parametri utilizzati per la sequenza cine sono stati : tempo di ripetizione ( tr ) / tempo di eco ( te ) = 35 ms / 1 , 8 ms ; flip angle : 60 ; spessore di fetta : 8 mm ; tempo di acquisizione : 1520 s a seconda della frequenza cardiaca del paziente ; ampiezza della banda di ricezione : 930 hz / pixel ; matrice 256256 ; field of view ( fov ) : 300350 m la immagini post - contrastografiche per la valutazione del delayed enhancement ( de ) sono state ottenute dopo somministrazione di 0 , 2 mmol / kg di chelati del gadolinio ( dotarem , guerbet francia ) con un flusso di 2 ml / s . 
le immagini sono state ottenute dopo 10 minuti dalla iniezione nei medesimi piani spaziali tramite sequenza 3d turbo - flash inversion recovery ( ir ) t1 - pesata con i seguenti parametri di acquisizione : tr / te = 7 ms / 3 ms ; flip angle : 15 ; dimensioni del voxel : 1 , 41 , 41 , 2 mm , 32 linee del k spazio calcolate per ciascun intervallo r - r in telediastole , fov : 340265 cm ; matrice : 192256 ; 16 cicli cardiaci campionati nellarco di una singola apnea . 
il tempo di inversione ( ti ) stato modificato progressivamente al fine di annullare completamente il segnale del miocardio , con un range di valori compreso tra 220 e 290 ms . 
lanalisi in post - processing delle sequenze true - fisp , al fine di calcolare la massa cardiaca e la frazione di eiezione , stata eseguita tramite software dedicato ( argus , siemens , erlangen , germania )  . analisi delle immagini le indagini eco - cardiografiche e cardio - rm sono state valutate in cieco , rispettivamente da un cardiologo e da un radiologo esperti in imaging cardiaco , entrambi non a conoscenza degli eventuali dati clinici e strumentali precedenti . 
in tutti i casi il profilo dellendocardio stato giudicato riconoscibile : a partire da una serie di immagini radiol med ( 2011 ) 116 : 197210 corresponding to the end diastole and end systole were automatically selected , and the margins of the endocardium and the epicardium were traced on thethe papillary muscles were included in the calculation , whereas trabeculae projecting into the cardiac cavity were excluded , as they were judged to be a possible source of error . 
the software calculates the volume [ area times the slice thickness ( 8 mm ) and the gap between the slices ( 1 mm ) ] and ventricular mass ( myocardial volume times the value of the myocardial density : 1.05 g / ml ) in the phase in question , with evaluation of the curves that define the endocardium and epicardiu edv , esv and ef were calculated with the simpson method ( the volume of an object can be estimated by adding the individual areas in each section and multiplying them by the slice thickness ) [ 14 , 15 ]  . with a parasternal approach and in the m - mode longaxis view and with the cursor perpendicular to the septum , measurements of the septum and posterior wall were manually performed during both diastole and systole . diastolic function was obtained by calculating the peak velocity of the e - wave and a - wave . 
the presence of systolic anterior motion ( sam ) was verified , considered as a displacement of both mitral flaps > 2 mm below the cd line during systole ( overall ventricular systole ) , and the degree of mitral regurgitation was quantified with doppler . 
fibrosis was estimated with a qualitative comparison between the degree of ultrasonic reflectivity in the areas considered to be fibrotic and the parts of the myocardium considered to be healthy [ 14 ]  . 
at cardiac mr imaging , myocardial mass , edv , esv and ef values were calculated during postprocessing on true - fisp sequences with a dedicated software package ( argus , siemens , erlangen , germany ) , considering the curvature of the lv , with the electronic callipers in the short axis for the septum and the long axis for the posterior wall perpendicular to the segment subjectively evaluated most often in end diastole . myocardial thickness was estimated on images acquired in two - chamber short - axis and four - chamber long - axis views in end diastole . 
the degree of myocardial fibrosis was evaluated with the subjective demonstration of intramural areas of late enhancement characterised by signal hyperintensity in a region of hypointense myocardiu no quantitative methods were adopted . 
however , to be acquisite in un intero ciclo cardiaco in asse corto , dalla base allapice del cuore , sono selezionate automaticamente le immagini corrispondenti alla td e alla ts e su queste sono stati tracciati manualmente i bordi dellendocardio e dellepicardio . 
il software calcola il volume ( area per lo spessore della fetta , 8 mm , e del gap tra le fette , 1 mm ) e la massa ventricolare ( volume miocardico moltiplicato per il valore della densit miocardia : 1 , 05 g / ml ) nella fase considerata , valutando larea delle curve che definiscono lendoe lepicardio . 
il volume telediastolico ( vtd ) , il volume telesistolico ( vts ) e la frazione di eiezione ( fe ) sono stati calcolati col metodo di simpson ( il volume di un oggetto pu essere stimato sommando le singole aree in ciascuna sezione e moltiplicandole per lo spessore della fetta ) [ 14 , 15 ]  . con approccio parasternale , nella proiezione asse lungo m - mode e cursore ortogonale al setto , sono state eseguite in modo manuale le misurazioni del setto e della parete posteriore , sia in diastole che in sistole . 
mediante lanalisi doppler stata calcolata la velocit massima e media dellefflusso ventricolare sinistro ed i relativi gradienti ; si ricercato lo spostamento anteriore del lembo mitralico ( sam ) , considerato uno spostamento in sistole dei lembi mitralici > 2 mm al di sotto della linea cd ( sistole ventricolare complessiva ) e quantificato con doppler il grado di rigurgito mitralico . 
alla cardio - rm la massa cardiaca , i valori di vtd , vts e fe sono stati calcolati in post - processing sulle sequenze true - fisp , tramite software dedicato ( argus , siemens , erlangen , germania ) , tenendo conto della curvatura del vsn , con caliper elettronico , rispettivamente in asse corto per il setto ed in asse lungo per la parete posteriore , perpendicolarmente al segmento soggettivamente valutato pi spesso in td . 
il sam stato valutato mediante sequenze a contrasto di fase , insieme con levidenziazione di eventuale insufficienza mitralica associata e in base alla valutazione qualitativa dellescursione valvolare nelle sequenze cine true - fisp . 
la alterazione di segnale 202 radiol med ( 2011 ) 116 : 197210 considered , signal alteration needed to be confirmed in at least two acquisition planes . tuttavia per essere segnalata doveva confermarsi in almeno due piani di acquisizione . statistical analysis analisi statistica the following values were considered normal : myocardial mass between 118 and 238 g ; ef between 56% and 78% ; lv wall thickness at the level of the septum and inferior wall between 8 mm and 10 mcontinuous variables are expressed as mean standard deviation ( sd ) and categorical variables as proportions and percentages . 
statistical correlation was performed using student t test and spearmans correlation coefficient ( r ) for comparison of continuous variables , and fishers exact test was used to compare categorical variables . 
 sono stati considerati normali i seguenti valori : massa cardiaca tra i 118 e i 238 g ; fe tra il 56% ed il 78% ; spessore parietale del vsn a livello del setto e della parete inferiore tra gli 8 mm e 10 mle variabili continue sono state espresse come mediadeviazione standard , le variabili categoriche come proporzioni e percentuali . 
la correlazione statistica stata eseguita usando il test t di student e lindice di correlazione r di spearman per il confronto tra variabili continue ; il test di fisher stato utilizzato per confrontare le variabili categoriche . 
uniforme ispessimento di tutto il miocardio del ventricolo sinistro , particolarmente evidente al setto interventricolare ed alla parete anteriore , evidenziato sia allecocardiografia ( a , b ) che alla cardio - rm ( c , d )  . radiol med ( 2011 ) 116 : 197210 fig . 
2a - d assessment of myocardial mass and ventricular function by means of echocardiography and cardiac magnetic resonance ( mr ) imaging : at echocardiography , in the parasternal short - axis view , at the end - diastolic phase , the epicardial ( a ) and endocardial ( b ) borders are measured , including the papillary muscles , which are often hypertrophic . 
2a - d calcolo della massa e funzione ventricolare in ecocardiografia ( a - c ) e in rm ( d ) : allecocardiografia , in parasternale asse corto in tele - diastole , viene planimetrato il contorno dellepicardio ( a ) e dellendocardio ( b ) , includendo i muscoli papillari ( spesso ipertrofici )  . 
3a - d underestimation of myocardial mass with cardiac mr imaging ; geometric representation of the lv cut by several sections in the short - axis view : the volume could be overestimated or underestimated depending on the position of lv within the section , considering identical thickness ( grey ) and gap ( white spaces ) between sections . 
the most caudal section could be included in assessing the myocardial mass ( a ) or excluded because < 50% of this slice is included in the assessed volume ( b )  . 
3a - d sottostima della massa cardiaca alla cardio - rm : rappresentazione schematica della geometria del vsn tagliato da multiple sezioni in asse corto ( a , b )  . 
pur ammettendo uguali spessori di fetta ( in grigio ) e dei gap tra le sezioni ( spazi bianchi ) , il volume pu essere sia sovra che sottostimato a seconda della posizione del vsn rispetto alla fetta in questione . 
la fetta pi caudale pu venire inclusa ( a ) nel calcolo del volume , mentre potrebbe essere esclusa dal software perch compresa nella zona di interessa per meno del 50% ( b )  . 
si ottenuta una buona correlazione ( r = 0 , 75 ) tra gli spessori del setto calcolati allecocardiografia ( 1236 mm ) ed alla cardio - rm ( 1639 mm ) , mentre non stata verificata correlazione tre le metodiche riguardo lo spessore della parete posteriore ( r = 0 , 04 )  . 
lostruzione dinamica era presente in 9 / 22 pazienti ( 40 , 9% ) analizzati con eco - cardiografia e in 12 / 22 pazienti ( 54 , 5% ) studiati con rm ( p = 0 , 5 )  . 
alla cardio - rm , la concordanza fra la presenza di de con lo spessore massimo in telediastole stata statisticamente non significativa sia per il setto ( p = 0 , 6 ) che per la parete posteriore ( p = 0 , 9 )  . 
il confronto fra i parametri morfologici e funzionali valutati con eco - cardiografia e cardio - rm schematizzato nelle tabelle 1 e 2 . discussion discussione clinical diagnosis of hcm is not simple , as patients tend to be asymptomatic at onset without apparent cause of the la diagnosi clinica di cmi non risulta sempre agevole , trattandosi generalmente di pazienti asintomatici allesordio , radiol med ( 2011 ) 116 : 197210 fig . 
5a - c differenti pattern di fibrosi miocardica alla cardio - rm : distribuzione focale ( a , b ) e diffusa a zolle ( c ) myocardial hypertrophy [ 1 , 2 ]  . 
cardiac mr imaging , which is comparable with echocardiography in terms of diagnostic sensitivity , is more accurate in measuring wall thickness and cardiac motion and can be considered the most reliable technique in demonstrating the presence of disorganisation in muscle structure , inefficient myocardial contraction and myocardial fibrosis [ 7 , 17 , 18 ]  . 
la cardio - rm , paragonabile alleco - cardiografia in termini di sensibilit per la diagnosi , presenta maggior accuratezza nella determinazione degli spessori di parete e della cinetica cardiaca , potendo inoltre essere considerata la metodica pi affidabile nel dimostrare la presenza di disorganizzazione nella struttura muscolare , di uninefficiente contrazione miocardica e di fibrosi parietale [ 7 , 17 , 18 ]  . 
 in accordo con i dati della letteratura [ 5 , 12 , 13 , 16 , 17 , 19 ] , i nostri risultati dimostrano unassoluta concordanza fra eco - cardiografia e cardio - rm nella determinazione della sede e dellestensione di malattia , con differenze statisticamente non significative nella definizione dei valori di vtd ( p = 0 , 31 ) , vts ( p = 0 , 1 ) , fe ( p = 0 , 05 ) , e della presenza di ostruzione dinamica ( p = 0 , 5 )  . 
tale sovrastima relativa da attribuirsi ai differenti metodi di misurazione utilizzati : mentre alleco - cardiografia il calcolo dello spessore automatico , previa acquisizione di immagini mmode in asse lungo , alla rm la misurazione tiene conto della curvatura del vsn , e viene effettuata mediante caliper elettronico , in asse corto per il setto ed in asse lungo per la parete posteriore . 
in our data set , however , the relatively small area at the level of the apical sections produced a minimal amount of error in the quantification of mass and ef , whereas the effect described above is more evident at the base , where the area of the section is greater ( p < 0.001 ) [ 19 ]  . 
the superiority of cardiac mr in diagnosing sam lies in its more objective interpretation and the possibility of obtaining a more precise assessment of its functional repercussions with the acquisition of phasecontrast sequences . 
also important in these cases is the presence of secondary mitral regurgitation , which can be demonstrated as a systolic jet in the left atrium and is quantifiable with phase - contrast sequences [ 8 , 20 ]  . 
the lack of a reference standard , such as a histological examination , prevented absolute verification of the causes of those differences , which we believe are correlated with the radically different methods used for the diagnosis ( increase in ultrasonic reflectivity at echocardiography vs delayed enhancement at mr )  . 
the site of fibrosis in this sense does not seem to correspond with areas supplied by epicardial branches of the coronary arteries , which are thought to be more compromised where the wall is thicker . livello , ed alla base , a causa del movimento verso lapice ( mediamente circa 1 , 3 cm ) che il cuore attua durante la sistole [ 10 ]  . 
nel nostro dataset tuttavia , larea relativamente piccola a livello delle sezioni apicali ha introdotto una minima componente di errore nella quantificazione della massa e della fe , mentre leffetto sopra descritto pi evidente a livello della base , ove larea di sezione maggiore ( p < 0 , 001 ) [ 19 ]  . 
 nella nostra esperienza , anche la delimitazione automatica dei profili cardiaci , del vtd e del vts presenta errori intrinseci al software tali da richiedere un ritocco manuale da parte delloperatore dei contorni endocardici ed epicardici con inevitabile incremento dei tempi necessari per il post - processing . 
 anche se la cardio - rm si rilevata lievemente superiore alla eco - cardiografia nel rilevare il fenomeno del sam , permettendo di individuare anche le forme lievi o in fase iniziale , la differenza di performance non stata significativa ( p = 0 , 1 )  . 
la superiorit della cardio - rm nella diagnosi del sam da ricercare nella maggiore obiettivit interpretativa nonch nella possibilit di poter effettuare una pi precisa valutazione anche delle ripercussioni funzionali del fenomeno con la acquisizione di sequenze a contrasto di fase . 
inoltre importante in questi casi documentare la presenza di una eventuale insufficienza mitralica secondaria , dimostrabile come jet sistolico in atrio sinistro , e quantificabile alla rm mediante sequenze in contrasto di fase [ 8 , 20 ]  . 
in accordo con i dati della letteratura , la cardio - rm si rilevata superiore alla eco - cardiografia nella identificazione della fibrosi parietale [ 9 , 21 ] , e questo aspetto da recenti lavori sembra poter correlarsi alla maggior probabilit di eventi fatali [ 22 ] : tuttavia , la differenza di performance tra le metodiche non stata significativa ( p = 0 , 15 )  . 
la totale concordanza riguardante la sede della fibrosi parietale stata raggiunta in soli 3 / 9 pazienti ( 33% ) , rispettivamente in un caso di localizzazione apicale e due casi di localizzazione diffusa . 
la mancanza di uno standard di riferimento , quale lesame istologico , ha impedito di verificare con certezza le cause di tali differenze che riteniamo comunque correlate ai metodi radicalmente diversi utilizzati per la diagnosi ( aumento della rifrangenza alleco - cardiografia versus delayed enhancement alla rm )  . 
alla cardio - rm , la fibrosi era presente nella maggior parte dei pazienti in quelle sezioni di miocardio ove lipertrofia risultata maggiore : tuttavia , anche il tentativo di cercare una correlazione tra la presenza di impregnazione tardiva con lo spessore massimo in telediastole ( del setto e / o della parete posteriore ) non risultato significativo ( setto p = 0 , 6 ; parete posteriore p = 0 , 9 )  . 
la sede della fibrosi sembrerebbe in questo senso non corrispondere ai territori di perfusione dei rami epicardici delle arterie radiol med ( 2011 ) 116 : 197210 despite the nonsignificant difference in overall performance , in our experience , cardiac mr imaging has the advantage of offering an objective and repeatable evaluation of the morphological parameters ( wall thickness , extent of myocardial fibrosis ) and functional parameters ( edv , esv , sam , ef ) , which is crucial in the follow - up of these patients to facilitate comparison and evaluate disease progression . 
in addition , with the technique of myocardial tagging , mr imaging is better able to demonstrate changes in lv motion resulting from hypertrophy [ 23 ] and better still with a 3 - t system [ 24 ]  . 
 there are , however , some limitations to this study . first , the number of patients enrolled was relatively small insofar as the population can be considered representative , as it included only asymptomatic patients and patients without identifiable causes of cardiac hypertrophy . second , evaluating myocardial fibrosis was based on imaging findings described in the literature , with no reference standard such as histological examination . 
last , clinical and / or radiological follow - up is available for a limited number of patients only , and therefore the findings described cannot be correlated with disease progression and prognostic data . in conclusion , echocardiography and cardiac mr imaging are accurate techniques for diagnosing hcm . given its greater accessibility , echocardiography is the first - line technique , whereas mr being more objective in its measurement , more accurate in identifying sam and more sensitive in recognising myocardial fibrosis is a useful diagnostic integration to be recommended in doubtful cases or in the apical form , in which the poor acoustic window can limit echocardiographic study . 
the correlation between prognosis and the presence of fibrosis in recently published studies [ 22 ] validates the role of mr imaging not only in diagnosing the disease but also , and above all , in the follow - up of these patients , who are often young . coronarie che dovrebbero risultare maggiormente compromessi laddove vi sia maggior spessore di parete . nonostante differenze non significative di performance globale , nella nostra esperienza la cardio - rm presenta il vantaggio di permettere una valutazione obiettiva e ripetibile dei parametri morfologici ( spessore di parete , entit della fibrosi parietale ) , e funzionali ( vtd , vts , sam , fe ) , fatto di fondamentale importanza nel caso di follow - up di questi pazienti per favorire il confronto e la valutazione dellevoluzione del quadro . 
inoltre , mediante la tecnica di tagging miocardico , la rm meglio evidenzia le alterazioni della cinetica del vsn conseguente allipertrofia [ 23 ] , meglio ancora se mediante apparecchiature 3 tesla [ 24 ]  . 
 questo studio tuttavia presenta dei limiti : primo , il numero di pazienti arruolati relativamente basso , per quanto la coorte possa essere ritenuta rappresentativa , comprendendo solo pazienti asintomatici e senza cause evidenziabili di ipertrofia cardiaca . 
secondo , la valutazione della fibrosi parietale si basata su rilievi di imaging descritti in letteratura , mancando uno standard di riferimento di tipo istologico . terzo , uno studio di perfusione miocardica stato eseguito solo in alcuni pazienti , per cui non stato possibile effettuare una correlazione fra fibrosi ed ipoperfusione tissutale . 
infine , un follow - up clinico e / o radiologico disponibile , allo stato attuale , per un numero limitato di pazienti , e pertanto non stato possibile correlare i rilievi descritti con la capacit di evolvere della malattia e con i dati prognostici . in conclusione , eco - cardiografia e cardio - rm rappresentano metodiche accurate per la diagnosi di cmi . 
lecocardiografia , in relazione alla maggiore accessibilit , rappresenta lindagine di prima linea , mentre la rm , grazie alla maggiore obiettivit delle misurazioni , alla maggiore accuratezza nellinquadramento del sam , e alla maggiore sensibilit nel riconoscere la fibrosi parietale rappresenta utile integrazione diagnostica da raccomandarsi in particolare nei casi dubbi o nelle forme apicali laddove la scarsa finestra acustica pu limitare lesame ecografico [ 17 ]  . 
le ricadute prognostiche correlate alla presenza di fibrosi riportate in recenti lavori della letteratura [ 22 ] avvalorano limportanza del ruolo della rm non solo nella diagnosi di malattia ma anche e soprattutto nel follow - up di questi spesso giovani pazienti . conflict of interest none radiol med ( 2011 ) 116 : 336 doi 10.1007 / s11547 - 011 - 0659 - 8 erratum off - label use of intravascular iodinated organic and mr contrast media utilizzo off - label dei mezzi di contrasto organo - iodati e per risonanza magnetica per via iniettiva o . 
david4 1dipartimento di radiologia cardiovascolare , 3dipartimento di cardiochirurgia , 4dipartimento di radiologia demergenza , ospedale san camillo - forlanini , circonvallazione gianicolense 87 , 00152 rome , italy 2dipartimento di scienze radiologiche , universit di roma sapienza , ospedale santandrea , via di grottarossa 1035 , 00189 rome , italy correspondence to : c.n. 
the aim of our work was to compare image quality and radiation dose in a group of patients who underwent cardiac dual - source computed tomography ( dsct ) with prospective electrocardiographic ( ecg ) gating with those of a control group studied with retrospective gating . 
coronary ct with prospective ecg gating , a standard feature on new scanners , allows for a significant reduction in radiation dose without causing any significant decrease in image quality or in the number of segments assessed . 
la dose normalizzata di radiazioni stata di 4 , 910 , 4 msv per il gruppo prospettico , e di 14 , 62 msv4 , 36 per il gruppo retrospettivo ( p < 0 , 01 )  . 
la tc coronarica con tecnica di radiol med ( 2011 ) 116 : 178188 keywords dual - energy computed tomography coronary angiography prospective gating retrospective gating sincronizzazione prospettica , utilizzabile negli scanners di ultima generazione , permette una significativa riduzione della dose di radiazioni somministrata al paziente senza determinare alcuna riduzione rilevante nella qualit delle immagini e nel numero di segmenti valutabili . 
per tale ragione , attualmente consigliabile l utilizzo di tale tecnica nei soggetti che presentano una frequenza cardiaca inferiore ai 70 bpm ed un bmi inferiore ai 30 kg / m2 . parole chiave tomografia computerizzata dual - energy angiografia coronarica gating prospettico gating retrospettivo introduction introduzione multidetector computed tomography ( mdct ) has proved to be an accurate method for evaluating coronary atherosclerosis [ 15 ]  . 
owing to the technological limits of older ct scanners , cardiac ct studies have been carried out until recently with retrospective electrocardiographic ( ecg ) gating , in which the whole heart cycle is acquired to obtain a large number of cardiac phases to assess the coronary arteries [ 8 ]  . 
in this context , different dose - reduction strategies have been developed that rely either on dose - modulation algorithms during the cardiac cycle ( ecg pulsing ) [ 9 ] or on tube current reduction [ 10 ]  . although such strategies have allowed for a significant reduction in radiation exposure , the dose nonetheless remains high , even higher than that delivered by conventional coronary angiography . 
 the most effective dose - reduction technique developed to date is prospective ecg gating , in which only a portion of the cardiac cycle is acquired in a sequential , step - andshoot mode . 
however , these limitations have now been overcome by the latest - generation ct equipment in which different engineering solutions including increased number of x - ray tubes [ 11 ] or detectors [ 12 ] have allowed reliable prospective gating techniques to be developed [ 13 ]  . the purpose of this study was to compare image quality and radiation dose in a group of patients studied with dualsource ct ( dsct ) coronary angiography with prospective ecg gating compared with a control group studied with retrospective gating . la tomografia computerizzata ( tc ) multidetettore ( tcmd ) ha dimostrato di essere una metodica che permette unaccurata valutazione dellaterosclerosi coronarica [ 15 ]  . 
a causa di limitazioni tecnologiche presenti nelle tc di vecchia generazione stata utilizzata sinora una tecnica di sincronizzazione dellelettrocardiogramma ( ecg ) di tipo retrospettivo in cui viene acquisito lintero ciclo cardiaco , in modo da poter disporre di un elevato numero di fasi in cui valutare le coronarie [ 8 ]  . 
per tale motivo sono state sviluppate diverse strategie per la riduzione delle radiazioni basate su algoritmi di modulazione della dose durante il ciclo cardiaco ( ecg pulsing ) [ 9 ] o sulla riduzione dellintensit della corrente del tubo radiogeno [ 10 ]  . 
in tal modo stata ottenuta una significativa riduzione delle radiazioni somministrate al paziente , che per rimangono ancora a livelli elevati , superiori a quelli di unangiografia coronarica tradizionale . attualmente la tecnica pi efficace nella riduzione della dose risulta essere la sincronizzazione prospettica dellecg , in cui viene acquisita solo in una parte del ciclo cardiaco effettuando cos unacquisizione in modalit sequenziale . 
alcuni limitazioni tecniche , quali la velocit di rotazione del gantry , non avevano permesso sinora un ampio utilizzo di questa seconda modalit di acquisizione se non per finalit di ricerca . 
tali limitazioni risultano attualmente superate nelle tc di ultima generazione in cui soluzioni ingegneristiche differenti , come laumento dei tubi radiogeni [ 11 ] o lincremento del numero di detettori [ 12 ] , hanno permesso lo sviluppo di tecniche di sincronizzazione prospettica affidabili [ 13 ]  . 180 materials and methods patient population between january and march 2009 , noninvasive dsct coronary angiography was used to study 60 patients who were randomly assigned to two groups of 30 . 
exclusion criteria were allergy to iodinated contrast material , nephropathy ( creatinine > 120 mmol / l ) , nonsinus rhythm , haemodynamic instability , heart rate > 70 bpm and body mass index ( bmi ) > 30 kg / m2 . 
written informed consent was obtained from all patients enrolled in the study . study protocol examinations were conducted on a dual - source scanner ( somatom definition , siemens medical solutions , forchheim , germany )  . 
the studies were conducted with a biphasic intravenous injection of iodinated contrast material ( iomeron 400 , 400 mgi / ml , bracco , milan , italy ) delivered at high flow rates ( 56 ml / s ) through a dual - head injector . 
group a was studied with the following parameters : detector collimation 320.6 mm ; acquisition slices 640.6 mm with moving focal spot ; voltage 120 kv ; current 506 mas . 
in the prospective acquisition with dsct , the scan angle was extended from 260 to 460 , resulting in 8% of r - r cycle phases to be reconstructed compared with the selected phase . 
in group b patients , scans were performed using the following parameters : detector collimation 320.6 mm ; acquisition slices 640.6 mm acquired with a moving focal spot and adaptive pitch ( 0.20.35 ) ; gantry rotation time 330 ms ; tube voltage 120 kv ; current 350 mas . 
to reduce the dose in group b patients , automatic current modulation ( ecg pulsing ) was used , with maximum tube intensity applied between 30% and 80% of the cardiac cycle . 
this prevented unnecessary exposure during cardiac phases in which the image quality of the coronary arteries is classified as nondiagnostic ( table 1 )  . radiol med ( 2011 ) 116 : 178188 lo scopo di tale lavoro di comparare la qualit dimmagine e la dose di radiazioni di un gruppo di pazienti sottoposto ad angiografia coronarica con tc dual source ( tcds ) con tecnica di sincronizzazione prospettica dellecg rispetto ad un gruppo di controllo studiato con tecnica di sincronizzazione retrospettiva . materiali e metodi popolazione di pazienti nel periodo compreso tra gennaio e marzo 2009 , sono stati studiati mediante angiografia coronarica non invasiva con tcds 60 pazienti randomizzati in due gruppi di 30 pazienti ciascuno . 
i criteri di esclusione sono stati i seguenti : allergia al mezzo di contrasto iodinato , nefropatia ( creatinina > 120 mmol / l ) , ritmo non sinusale , instabilit emodinamica , frequenza cardiaca > 70 battiti per minuto ( bpm ) , body mass index ( bmi ) > 30 kg / m2 . 
tutti i soggetti esaminati hanno fornito il consenso informato scritto . protocollo di studio lesame stato eseguito utilizzando uno scanner dual source ( somatom definition , siemens medical solutions , forchheim , germania )  . 
la scansione stata eseguita con una iniezione intravenosa bifasica con un iniettore a doppia testata di mezzo di contrasto iodato ( iomeron 400 , 400 mgi / ml , bracco , milano , italia ) a flussi elevati ( 56 ml / s ) ad una dose di 70 ml per la scansione retrospettiva e di 8090 ml per la scansione prospettica , il tutto seguito da 50 ml di soluzione salina . 
nel gruppo a sono stati utilizzati i seguenti parametri : collimazione dei detettori 320 , 6 mm ; strati di acquisizione 640 , 6 mm acquisiti mediante macchia focale mobile ; stato applicato un voltaggio di 120 kv ed una intensit di corrente di 506 mas . 
to evaluate calcified segments , reconstructions were obtained with a sharp kernel ( b46f ) [ 15 ]  . image reconstructions were transferred to an external workstation ( leonardo , siemens medical solutions ) equipped with dedicated software for cardiac postprocessing ( syngo circulation ii , siemens medical solutions )  . 
images were evaluated using axial scans , multiplanar reformations ( mpr ) , maximum intensity projections ( mip ) , volume rendering ( vr ) and curved multiplanar reconstructions . two blinded radiologists independently evaluated image quality of the coronary arteries according to the 16 - segment classification of the american heart association [ 16 ]  . 
la scansione stata eseguita nel gruppo b utilizzando i seguenti parametri : collimazione dei detettori 320 , 6 mm ; strati di acquisizione 640 , 6 mm acquisiti mediante macchia focale mobile e pitch adattativo ( 0 , 20 , 35 ) ; tempo di rotazione del gantry 330 ms . 
nel grupppo b , al fine di ridurre la dose somministrata stata utilizzata una modulazione automatica della corrente del tubo ( ecg pulsing ) , con la massima intensit applicata tra il 30% e 80% del ciclo cardiaco , evitando lesposizione del paziente a dosi di radiazioni non necessarie durante le fasi del ciclo cardiaco nelle quali la qualit delle immagini delle arterie coronarie pu risultare non diagnostica ( tabella 1 )  . 
 ricostruzione ed analisi delle immagini per il gruppo a , le immagini sono state ricostruite in fasi del 2% dellintervallo r - r allinterno della finestra di acquisizione prospettica ( 67%83% )  . 
in entrambi i casi le immagini sono state ricostruite utilizzando uno spessore di strato di 0 , 75 mm un incremento di ricostruzione di 0 , 4 mm ed un filtro b26f . 
per la valutazione dei segmenti calcifici sono state effettuate ricostruzioni con l utilizzo di un filtro sharp ( b46f ) [ 15 ]  . le immagini ricostruite sono state trasferite ad una workstation esterna ( leonardo , siemens medical solutions ) equipaggiata con un software dedicato al post - processing cardiaco ( syngo circulation ii , siemens medical solutions )  . per la valutazione delle immagini sono state applicate scansioni assiali , ricostruzioni multiplanari ( mpr ) , proiezioni di massima intensit ( mip ) , immagini in volume rendering ( vr ) e ricostruzioni multiplanari curve . 
due radiologi in cieco hanno valutato indipendentemente la qualit delle immagini delle arterie coronarie basandosi sulla classificazione in 16 segmenti dellamerican heart associations [ 16 ] : larteria coronaria destra include i segmenti 14 , il tronco comune e larteria discendente anteriore comprendono i segmenti 510 e larteria circonflessa i segmenti 1115 . 
a grado 4 , immagine di eccellente qualit diagnostica esente da artefatti ; b grado 3 , immagine di buona qualit diagnostica con artefatti minori ; c grado 2 , immagine di qualit diagnostica sufficiente per escludere patologie coronariche significative ; d grado 1 , immagine non valutabile per la presenza di severi artefatti . evaluation of radiation dose for both groups , we measured the dose - length product ( dlp ) and the scan length in centimetres . 
the conversion factor for the chest [ k = 0.017 msv / ( mgycm ) ] was calculated using human phantoms in a monte carlo simulation [ 17 ]  . since the scan length varied according to the clinical indication , the effective dose was normalised for the length of a standard 12 - cm heart scan [ 18 ]  . 
all statistical analyses were performed using the spss statistical software ( version 14.0 , statistical package for the social sciences spss , chicago , il , usa )  . significative ; grado 3 , immagine con artefatti minori e di buona qualit diagnostica per escludere patologie coronariche e valutare il grado di stenosi ; grado 4 , immagine senza artefatti di eccellente qualit diagnostica . valutazione della dose di radiazioni fattore di conversione per in entrambi i gruppi stato registrato il dose - lenght product ( dlp ) e la lunghezza in cm della scansione . 
dato che la lunghezza della scansione risultata variabile a seconda del tipo di indicazione clinica , la dose effettiva stata normalizzata per la lunghezza di una scansione standard del cuore di 12 cm [ 18 ]  . 
use of the best reconstruction interval for each segment resulted in excellent diagnostic quality ( score 4 ) of images in 40.1% ( 176 / 439 ) of cases in group a and in 42.0% ( 187 / 445 ) of cases in group b . 
minor artefacts ( good image quality , score 3 ) were seen in 54.2% ( 238 / 439 ) and in 55.5% ( 244 / 445 ) and moderate artefacts in 4.3% ( 19 / 439 ) and in 2.5% ( 11 / 445 ) of cases in groups a and b , respectively . 
il test della u di mannwhitney stato utilizzato al fine di rilevare eventuali differenze tra la qualit delle immagini e la dose media di radiazione dei due gruppi in esame . 
tutte le analisi statistiche sono state effettuate utilizzando il software statistico spss ( versione 14.0 , statistical package for the social sciences spss , chicago , illinois , usa )  . risultati langiografia coronarica mediante tcds stata eseguita con successo in tutti i pazienti , senza complicanze . 
non sono state riscontrate differenze significative nella composizione dei gruppi per quanto riguarda il sesso , l et , il bmi , la frequenza cardiaca e la variabilit della frequenza cardiaca ( p > 0 , 05 )  . qualit delle immagini sono stati valutati un totale di 439 segmenti coronarici nel gruppo a e 445 nel gruppo b . 
utilizzando per ogni segmento il miglior intervallo di ricostruzione , stata osservata rispettivamente una eccellente qualit diagnostica dellimmagine ( grado 4 ) rispettivamente nel 40 , 1% ( 176 / 439 ) dei casi del gruppo a e nel 42 , 0% ( 187 / 445 ) nel gruppo b ; si sono riscontrati artefatti minori ( buona qualit immagine , grado 3 ) nel 54 , 2% ( 238 / 439 ) e nel 55 , 5% ( 244 / 445 ) ; artefatti di grado moderato sono stati osservati rispettivamente nel 4 , 3% ( 19 / 439 ) e nel 2 , 5% ( 11 / 445 )  . 
la presenza di artefatti di grado severo che non permetteva la valutazione dei segmenti in esame stata riscontrata nel 1 , 4% ( 6 / 439 ) e nel 0 , 7% ( 3 / 445 ) ( tabella 3 )  . complessivamente , applicando il miglior intervallo di ricostruzione sono risultati diagnostici il 98 , 6% dei segmenti nel gruppo prospettico ed il 99 , 3% in quello retrospettico . 
la dose normalizzata di radiazioni per una scansione di 12 cm stata di 4 , 910 , 4 msv ( range 3 , 765 , 6 msv ) per il gruppo prospettico e di 14 , 62 msv4 , 36 ( 9 , 0818 , 51 msv ) per il gruppo retrospettivo . 
complessivamente , stata ottenuta una riduzione della dose di radiazioni del 62 , 4%9 , 1% ( range 51 , 0%68 , 3% ) ( p < 0.01 ) ( tabella 4 )  . tabella 3 qualit media delle immagini gruppo a ( prospettico ) gruppo b ( retrospettivo ) discussione 40 , 1% 54 , 2% 4 , 3% 1 , 4% 3 , 30 , 6 42 , 0% 55 , 5% 2 , 5% 0 , 7% 3 , 40 , 6 artefacts hindering segment evaluation were present in 1.4% ( 6 / 439 ) and in 0.7% ( 3 / 445 ) ( table 3 ) of patients , respectively . 
tale risultato stato possibile grazie al fatto che nella tecnica prospettica non viene acquisita in realt una sola fase , ma si ha una finestra di 8% rispetto al centro di acquisizione selezionato . 
a coronaria destra ; b arteria discendente anteriore ; c arteria circonflessa . radiation dose mean scan length was 14.12.0 cm ( range 11.218.7 cm ) for the prospective gating group and 13.72.6 cm ( range 11.917.3 cm ) for the retrospective gating group . 
this result was made possible by the fact that with the prospective technique , one acquires not a single phase but a 8% range relative to the selected scan centre . 
this implies the possibility of acquiring additional phases , which although limited in number are fundamental in the event of artefacts . on the other hand , the mean radiation dose was reduced by around 62.4 % , with a dose of 4.9 msv for the prospective technique as against 14.6 msv for the retrospective method . 
con tale dato viene meno il principale argomento a sfavore della tc coronarica che era rappresentato dellelevata dose somministrata . per tale motivo ragionevole aspettarsi in futuro , grazie alla diffusione degli scanners di ultima generazione , unespansione delle indicazioni della tc coronarica ed un notevole aumento del ricorso alla stessa in diagnostica coronarica rispetto alla coronarografia invasiva che attualmente presenta una morbidit ed una mortalit [ 20 ] pi elevate ed una dose di radiazioni comparabile se non superiore . i dati del nostro studio confermano e supportano quelli 186 radiol med ( 2011 ) 116 : 178188 coronary ct , i.e. , its high radiation dose . 
therefore , it can be reasonably expected that the wider diffusion of latestgeneration scanners will expand the indications for coronary ct and considerably increase its use in coronary diagnostics compared with invasive coronary angiography , which has higher morbidity and mortality rates [ 20 ] and similar , if not higher , radiation doses . our study findings confirm and corroborate those of other reports [ 13 , 18 , 2125 ] investigating prospective ecg gating and demonstrate the clinical feasibility of the technique as an effective method to reduce radiation exposure without affecting image quality . 
the prospective gating technique is applied to patients with low heart rates ( < 70 bpm ) and average bmi only to minimise the risk of artefacts that would prove impossible to eliminate given the small number of phases available . 
in our view , the need to administer beta - blockers once again , a need that dual - source technology had considerably reduced is an acceptable price to pay for a significant reduction in the radiation dose delivered , particularly to young patients [ 26 , 27 ]  . 
the technique would thus also allow the study of particular patients , such as heart - transplant patients with a high resting heart rate and reduced response to beta - blockers requiring serial follow - up imaging for possible allograft coronary disease [ 29 ]  . 
 finally , the prospective technique can provide diagnostic - quality images even in patients with arrhythmia , thanks to the sequential nature of the examination that makes it possible to avoid acquiring the segment when an ectopic beat is recognised prior to the scan , or to repeat the scan when the extrasystole occurs during acquisition . 
 conclusions coronary ct and the prospective ecg gating technique featured by the latest - generation scanners allows for a significant reduction in radiation dose , greater than that in conventional angiography , without deterioration of image quality or reduction in the number of assessable segments . this technique can therefore be recommended for patients with a heart rate < 70 bpm and a bmi < 30 kg / m2 . ottenuti da altri gruppi di ricerca [ 13 , 18 , 2125 ] sulla tecnica di sincronizzazione prospettica , e ne dimostrano lapplicabilit nella pratica clinica come metodo efficace nella riduzione della dose di radiazioni somministrata al paziente senza inficiare la qualit dimmagine dello studio . 
infatti , la tecnica di sincronizzazione prospettica viene applicata attualmente in pazienti con frequenze basse ( inferiori ai 70 bpm ) e con un bmi non elevato , al fine di ridurre al minimo la possibilit di artefatti che , data il basso numero di fasi a disposizione , non sarebbe possibile eliminare . 
a nostro giudizio la necessit di betabloccare nuovamente i pazienti , che sembrava essersi notevolmente ridotta con l avvento della tecnologia dual source , ci sembra un prezzo accettabile da pagare a fronte di una significativa riduzione della dose somministrata , in particolare nei soggetti giovani [ 26 , 27 ]  . 
in tal modo sarebbe possibile studiare con tale tecnica anche soggetti particolari come i pazienti sottoposti a trapianto cardiaco in cui presente unelevata frequenza basale ed una scarsa risposta ai farmaci beta - bloccanti e che necessitano di controlli ripetuti nel tempo per leventuale insorgenza della coronaropatia da rigetto [ 29 ]  . 
 infine , da sottolineare come con lutilizzo della tecnica prospettica possibile ottenere esami di qualit diagnostica anche in pazienti aritmici , grazie alla possibilit offerta dalla natura sequenziale dellesame , di evitare lacquisizione del segmento quando viene riconosciuto un battito ectopico prima della scansione o di ripetere la scansione quando lextrasistole avviene durante lacquisizione . 
 conclusioni la tc coronarica con tecnica di sincronizzazione prospettica , utilizzabile negli scanners di ultima generazione , permette una significativa riduzione della dose di radiazioni somministrata al paziente , inferiore anche a quella dellangiografia tradizionale , senza determinare alcuna riduzione rilevante nella qualit delle immagini e nel numero di segmenti valutabili . 
per tale ragione , attualmente consigliabile lutilizzo di tale tecnica nei soggetti che presentano una frequenza cardiaca inferiore ai 70 bpm ed un bmi inferiore ai 30 kg / m2 . conflict of interest none 1 . 
gandini1 1department of radiology , complex operational structure for radiological diagnosis , cardinal guglielmo massaia hospital , via conte verde 125 , 14100 asti , italy 2institute of diagnostic and interventional radiology , university of turin , via genova 3 , 10126 turin , italy 3department of biomedical sciences and human oncology , university of turin , turin , italy correspondence to : c . 
between november 2003 and march 2009 , 98 patients ( 78 women ; 20 men ) with a clinical and imaging suspicion of osteoporotic vertebral compression fractures underwent coaxial biopsy in conjunction with pvp of the thoracic and lumbar vertebrae . 
despite the number of biopsy samples considered insufficient or unsuitable , coaxial biopsy during pvp is useful in verifying the presumed aetiology of vertebral compression fractures , which is often unclear on the basis of clinical and imaging examinations . 
nel periodo compreso fra novembre 2003 e marzo 2009 98 pazienti , 78 femmine e 20 maschi , con sospetto clinico - strumentale di crolli vertebrali porotici sono stati sottoposti a biopsia coassiale in corso di vp di uno o pi metameri dorso - lombari . 
nonostante il discreto numero di prelievi considerati insufficienti / non idonei dall ' anatomopatologo , la biopsia coassiale in corso di vp utile per verificare la sospetta eziologia del crollo vertebrale , che si pu soltanto supporre sulla base degli esami clinici e strumentali . 
 quindi opportuno e consigliabile procedere a biopsia coassiale in tutti i pazienti che vengono sottoposti a vp . radiol med ( 2011 ) 116 : 302309 keywords vertebroplasty coaxial vertebral biopsy osteoporosis vertebral collapses parole chiave vertebroplastica biopsia vertebrale coassiale osteoporosi crolli vertebrali introduction introduzione vertebral fractures are one of the leading causes of hospitalisation both in italy and worldwide [ 1 , 2 ]  . 
most cases of vertebral compression fractures occur in osteoporotic patients . another , albeit less common , cause is malignancy , whether primary ( myelomas , lymphomas and other haematological dyscrasias ) or secondary to nonskeletal primary neoplasms . imaging alone is often unable to distinguish a neoplastic from osteoporotic aetiology [ 3 ]  . 
many patients who develop one or more vertebral compression fractures gain no benefit or pain relief from medication or containment devices ( braces , orthopaedic corsets ) , whereas percutaneous vertebroplasty ( pvp ) has recently been shown to be effective for both pain control and rapid functional recovery [ 47 ]  . 
 pvp is an interventional radiological procedure that involves injection of radio - opaque acrylic cement within the compressed vertebral bodies under fluoroscopic or combined fluoroscopic and computed tomography ( ct ) guidance . 
nonetheless , one should always consider the possibility that the cause is neoplastic , given that this is not a rare occurrence , and misdiagnosis results in delayed treatment and worse prognosis . 
for this reason , it is important to undertake a biopsy of one or more of the vertebral bodies being treated in all patients undergoing pvp for the first time in order to obtain histological confirmation of the clinical and imaging suspicion [ 9 ]  . 
 the aim of this study was to retrospectively analyse our experience to highlight the importance of biopsy sampling during pvp . materials and methods between november 2003 and march 2009 , 98 consecutive patients ( 78 women ; 20 men ) with a mean age of 72.6 ( range 5090 ) years and a total of 182 thoracolumbar vertebral compression fractures of a suspected osteoporotic nature were subjected to pvp and coaxial bone biopsy . 
each patients indications for spinal stabilisation were evaluated according to the guidelines le fratture vertebrali del rachide sono una delle principali cause di ospedalizzazione in italia e nel mondo [ 1 , 2 ]  . nella maggior parte dei casi i crolli vertebrali insorgono in pazienti osteoporotici , laltra principale causa , pur percentualmente inferiore rispetto allosteoporosi , quella neoplastica sia primitiva ( mieloma , linfoma ed altre discrasie ematologiche ) che secondaria a tumori primitivi extraossei . 
molti pazienti che vanno incontro ad uno o pi crolli vertebrali non trovano giovamento o sollievo dalla terapia farmacologica o contentiva ( busti , corsetti ortopedici ) mentre negli ultimi anni la vertebroplastica percutanea ( vp ) si dimostrata efficace sia per il controllo del dolore sia per un rapido recupero funzionale del soggetto [ 47 ]  . la vp una procedura di radiologia interventistica che consiste nelliniezione di cemento acrilico radiopaco , sotto guida radioscopica o combinata radioscopica - tomodensitometrica , allinterno di corpi vertebrali crollati . nella maggior parte dei casi la procedura si avvale del solo ausilio dellanestesia locale e periostale , solo pochi autori preferiscono ricorrere allanestesia generale [ 8 ]  . data la prevalenza dellosteoporosi nella popolazione naturale aspettarsi che alla base dei cedimenti vertebrali vi sia nella maggior parte dei casi una eziologia porotica . tuttavia bisogna sempre considerare la possibilit che la causa del crollo vertebrale sia neoplastica , poich questa un evenienza non rara e le conseguenze di una mancata diagnosi si riflettono in un ritardo terapeutico per il paziente con conseguente peggioramento della prognosi . per tali motivi importante procedere in tutti i pazienti che per la prima volta vengono sottoposti a vp ad un prelievo bioptico su uno o pi corpi vertebrali trattati per ottenere una conferma istologica del sospetto clinico - strumentale [ 9 ]  . lo scopo del lavoro quello di sottolineare limportanza del prelievo bioptico in corso di vp riportando retrospettivamente la nostra esperienza . materiali e metodi nel periodo compreso tra novembre 2003 e marzo 2009 , 98 pazienti consecutivi ( 78 femmine e 20 maschi ) , con una et media di 72 , 6 anni ( range 5090 anni ) ed un totale di 182 304 radiol med ( 2011 ) 116 : 302309 of the society of interventional radiology [ 10 ]  . 
all patients were entered into a database that included their ages , sex , medical history , presumed aetiology of the vertebral compression fracture ( s ) , imaging investigations and the visual analogue scale ( vas ) scores obtained before and after pvp [ 11 ]  . 
in particular , seven patients had a history of breast cancer , four had hepatocarcinoma associated with hepatitis c virus ( hcv ) related cirrhosis , three had a history of lung cancer , three of colorectal cancer , two of prostate cancer , two of stomach cancer , two were being treated for pleural mesothelioma , one had a history of thyroid cancer , one of laryngeal cancer , one of chondrosarcoma of the hand and one of laryngeal cancer . 
 all procedures were carried out by two operators with the patient in the prone position and employing combined fluoroscopic ct guidance using an image intensifier ( oec 9800 plus , ge healthcare , wi , usa ) and a ct scanner ( lightspeed qx / i , ge healthcare , wi , usa )  . 
in each procedure , after two preliminary scout views in the anteroposterior and laterolateral view , a volume was acquired that comprised the metamere immediately above and immediately below the one ( s ) requiring treatment . 
the scan parameters were as follows : helical scanning ; rotation time 0.8 s ; slice thickness 5 mm ; table speed 30 mm / s ; reconstruction interval 5 mm ; fov wide ; 80 kv ; 4060 ma [ 12 ]  . 
as far as fluoroscopy was concerned , we used the systems automatic exposure control . only local subcutaneous or periosteal anaesthesia was used , with 23 ml of 1% lidocaine , or , particularly in vertebral compression fractures of the thoracic spine , with a mixture of 1% lidocaine and triamcinolone . 
the biopsy cannula was 2 cm greater than the vertebroplasty needle , allowing it to penetrate deeply into the vertebral body to collect the bone sample , but this procedure requires careful fluoroscopic monitoring to avoid injury to the vertebral cortex . 
tutti i pazienti sono stati preventivamente informati sugli aspetti procedurali , sui benefici e sui rischi correlati alla vp e alla biopsia vertebrale ed stato chiesto loro il consenso , per iscritto , allesecuzione del trattamento . lindicazione allintervento di stabilizzazione vertebrale stata valutata seguendo le linee guida redatte dalla society of interventional radiology [ 10 ]  . 
tutti i pazienti coinvolti nello studio sono stati inseriti in un database comprendente let , il sesso , lanamnesi patologica remota e prossima , la sospetta eziopatogenesi del / dei cedimento / i vertebrali , le indagini strumentali eseguite ed il visual analogue scale ( vas ) score pree post - vp [ 11 ]  . 
in particolare : 7 pazienti con pregressa neoplasia mammaria , 4 pazienti con epatocarcinoma ( hcc ) in cirrosi positiva al virus dellepatite c ( hcv + ) , 3 pazienti con pregressa neoplasia polmonare , 3 pazienti con pregressa neoplasia del colon - retto , 2 pazienti con pregressa neoplasia prostatica , 2 pazienti con pregressa neoplasia gastrica , 2 pazienti con mesotelioma pleurico in trattamento , 1 paziente con pregressa neoplasia tiroidea , 1 paziente con pregressa neoplasia laringea , 1 paziente con pregresso condrosarcoma della mano ed , infine , 1 paziente con pregressa neoplasia laringea . tutte le procedure sono state condotte con paziente in posizione prona da due operatori con lausilio di una guida combinata radioscopica - tomodensitometrica utilizzando un intensificatore di brillanza ( oec 9800 plus , ge healthcare wis ) ed una tomografia computerizzata ( tc ) ( lightspeed qx / i , ge healthcare wis )  . 
in ogni procedura , dopo aver eseguito due scout preliminari in proiezione anteroposteriore e latero - laterale , si proceduto a confezionare un pacchetto comprendente il metamero immediatamente soprastante e quello immediatamente sottostante a quello / quelli da trattare . 
i parametri di scansione erano : helical scanning , tempo di rotazione 0 , 8 s , spessore di slice 5 mm , velocit del tavolo 30 mm / s , intervallo di ricostruzione 5 mm , campo di vista ( fov ) largo , 80 kv , 4060 ma [ 12 ]  . 
per ci che concerne la scopia si utilizzava lesposizione automatica dellapparecchiatura . stata utilizzata esclusivamente anestesia locale sottocutanea e periostale con 23 ml di lidocaina all1% o , soprattutto nei crolli vertebrali del tratto dorsale del rachide , con una miscela di lidocaina all1% e triamcinolone . 
il prelievo bioptico stato eseguito immediatamente prima dellinfusione del cemento biologico radiol med ( 2011 ) 116 : 302309 utilizzando sempre la tecnica coassiale attraverso lago da vertebroplastica il cui calibro era di 13 g o 10 g . 
essa ha una lunghezza di 2 cm superiore a quella dellago da vertebroplastica , ci permette di penetrare profondamente nel corpo vertebrale per ottenere il frustolo osseo , ma richiede un accurato controllo fluoroscopico intraprocedurale per evitare lesioni della corticale vertebrale . 
il prelievo ottenuto stato fissato in formalina neutra tamponata con tampone fosfato 0 , 05 m e successivamente posto , per 3 ore , in una soluzione di sodio citrato tribasico e acido formico fino a completa demineralizzazione ed infine incluso in paraffina dopo processazione con processatore automatico leica asp200 s . 
per ogni blocchetto contenente il materiale incluso in paraffina sono state allestite delle sezioni dello spessore di 3 micron le quali sono state poi colorate con ematossilina - eosina tramite coloratore automatico leica 5010 . 
for each block containing paraffin - embedded material , 3 - m - thick sections were prepared , which were then stained with haematoxylineosin using an automated leica 5010 stainer . 
immunohistochemical analyses with a ventana benchmark automated immunostainer ( ventana , tucson , az , usa ) employing antibodies against specific tumour antigens were performed in cases requiring further investigation . results in 83 of 98 patients ( 85% ) undergoing pvp , histological examination on the biopsy confirmed the diagnostic suspicion of osteoporotic vertebral compression fracture . 
in 13 cases ( 13% ) , the biopsy nei 98 pazienti sottoposti a vp lesame istologico sul prelievo bioptico ha confermato lipotesi diagnostica in 83 casi ( 85% )  . 
il tempo procedurale aggiuntivo imputabile allesecuzione della biopsia con tecnica coassiale stato in tutti i casi contenuto , compreso fra 3 e 5 minuti , anche in considerazione del fatto che ci si sempre limitati ad 12 prese bioptiche mentre altri autori adottano lesecuzione routinaria di multiple prese bioptiche [ 13 ]  . discussione malgrado vengano effettuate indagini diagnostiche , 306 radiol med ( 2011 ) 116 : 302309 fig . 
in our experience , the majority of patients undergoing pvp had a prebiopsy suspicion of osteoporotic vertebral compression fracture , whereas a smaller proportion had a well - founded suspicion of secondary neoplasm or localisation of a blood dyscrasia . 
nella nostra esperienza la maggior parte dei pazienti che sono andati incontro a vertebroplastica avevano un sospetto prebioptico di crollo vertebrale su base osteoporotica mentre una percentuale inferiore aveva un fondato sospetto prebioptico di tipo neoplastico secondario o di localizzazione di discrasia ematologica . 
in questo lavoro sono stati presi in considerazione solo i pazienti con sospetto pre - bioptico di cedimento vertebrale su base porotica . in letteratura vi sono pochi lavori che descrivono lassociazione tra vp e biopsia con tecnica coassiale [ 9 , 13 , 16 ] , tuttavia il numero di complicanze estremamente basso e comunque non superiore a quello legato alla semplice esecuzione di vp . 
il tempo aggiuntivo per la procedura bioptica assolutamente trascurabile . il razionale della biopsia coassiale quello di confermare la natura del crollo vertebrale , questo dopo aver gi formulato unipotesi sulla base dei dati clinici , laboratoristici e strumentali . 
histological identification of myeloma , lymphoma or spinal metastases in patients linfoma o localizzazioni secondarie al rachide in pazienti con un crollo vertebrale su iniziale sospetta base porotica ha portato diversi autori [ 1416 ] a sostenere la necessit e limportanza di procedere sempre ad un prelievo bioptico in pazienti sottoposti a vp per la prima volta . 
lesame istologico su prelievo bioptico si rilevato utile anche nella nostra esperienza , evidenziando una localizzazione neoplastica al rachide in 2 pazienti ( carcinoma ad origine prostatica e mieloma ) che avevano un sospetto clinico308 radiol med ( 2011 ) 116 : 302309 fig . 
biopsies confirmed diagnoses insufficient or unsuitable material unexpected result 83 ( 85% ) 13 ( 13% ) 2 ( 2% ) tabella 1 risultati istologici dei prelievi bioptici numero biopsie conferme diagnostiche materiale non idoneo o insufficiente risultato non atteso 83 ( 85% ) 13 ( 13% ) 2 ( 2% ) presenting with presumed osteoporotic vertebral compression fracture has led several authors [ 1416 ] to recommend that a biopsy be performed in all patients undergoing pvp for the first time . 
the value of histological examination of the biopsy was confirmed in our experience , as spinal metastases were revealed in two patients ( from prostate cancer and myeloma ) who had a clinical and imaging suspicion of osteoporotic fractures . 
although this percentage of clinically unexpected results is undeniably very small , a correct histological diagnosis can indeed allow a prompt change in the treatment , which is quite different from that for an osteoporotic patient . the number of inadequate or unsuitable samples could be attributed to three factors : firstly , to limit the additional time required for the biopsy , we collected only one or two samples during each pvp procedure , whereas other authors [ 13 ] routinely collect two to six samples . 
certo questa una percentuale esigua di risultati clinicamente inattesi , tuttavia la corretta diagnosi istologica permette di modificare prontamente la terapia , del tutto diversa da quella di un paziente porotico . riguardo al numero di prelievi insufficienti o non idonei vanno considerati tre fattori : in primo luogo nella nostra esperienza ci si limitati ad 12 prelievi bioptici durante vp mentre , come gi detto , alcuni autori [ 13 ] adottano lesecuzione routinaria di un numero maggiore ( 26 ) di prelievi ; il razionale quello di contenere il tempo aggiuntivo legato alla biopsia . 
in secondo luogo nel nostro istituto , per ragioni logistiche e organizzative , non abbiamo la possibilit di avere presente un anatomopatologo al momento della biopsia in grado di valutare estemporaneamente qualit e quantit del prelievo , a differenza di ci che avviene per le biopsie su organi parenchimatosi dove radiol med ( 2011 ) 116 : 302309 centres where biopsies on parenchymatous organs reach adequacy rates of 98%99% , our institute has no on - site pathologist to provide immediate evaluation of the quantity and quality of the sample due to local logistical and organisational reasons . 
the cost related to the histological examination of the biopsy sections is also very small . in conclusion , performing coaxial biopsy in conjunction with pvp should be considered in all patients undergoing pvp for the first time given that it is a safe procedure that does not prolong procedures times excessively , entails only a small additional cost whatever kit is used and , more importantly , is invaluable for characterising vertebral lesions and confirming the clinical and imaging suspicion , thereby helping to establish a correct diagnosis . lidoneit raggiunge percentuali del 98%99% . 
included in the study are patients at the first documented episode of acute pe , with 6 month follow - up . patients with severe pre - existent cardiopulmonary pathology or neoplastic diseases were excluded from the study . 
ct angiography evaluated right ventricular ( rv ) / left ventricular ( lv ) ratio , obstruction index according to qanadli and total clot burden ( ghanima score )  . 
stata riscontrata una significativa associazione tra lo score ghanima e quello di qanadli : i due indici sono risultati equivalenti nel quantificare lostruzione del circolo arterioso polmonare ( p < 0 , 001 )  . 
tra i parametri angio - tc lo score ghanima ha dimostrato di possedere la pi alta accuratezza nellindividuare i pazienti che svilupperanno il radiol med ( 2011 ) 116 : 230245 ( 76% )  . 
this approach allows to obtain , with just one test , both the diagnosis and a rather accurate acute pe risk stratification . keywords pulmonary embolism computed tomography pulmonary artery obstruction index risk stratification cuore polmonare cronico ( 76% )  . 
lo score ghanima pu essere utilizzato nella diagnosi angio - tc in urgenza come marker prognostico per una rapida stratificazione del rischio di cuore polmonare o decesso dei pazienti con ep acuta . 
lutilizzo di questo score consente di ottenere , con un unico esame , sia la diagnosi che una valutazione di gravit abbastanza accurata dellep acuta . parole chiave embolia polmonare angio - tc indice di ostruzione arteria polmonare stratificazione del rischio introduction introduzione pulmonary embolism ( pe ) represents a relatively common cardiovascular emergency that , by occluding the pulmonary arterial bed , may lead to severe acute but potentially reversible right ventricular ( rv ) failure . 
multislice computed tomography ( msct ) pulmonary angiography has recently gained widespread acceptance as a primary imaging technique to confirm the clinical suspicion of acute pe , replacing ventilation - perfusion scintigraphy and conventional pulmonary angiography [ 13 ]  . 
scintigraphy still plays a major role in nuclear medicine facilities by providing round - the - clock emergency imaging , thanks to its high negative predictive value ( npv )  . 
in its new guidelines for diagnosing and treating acute pe , the european society of cardiology recently included ct angiography ( cta ) as the reference standard modality to be used following initial clinical evaluation [ 5 ]  . the development of multidetector scanners has brought a number of technical advantages ( increased spatial and temporal resolution , excellent vascular opacification , reduced image noise , etc . ) and diagnostic improvements ; the possibility of performing a rapid examination in patients with prominent dyspnoea ; minimised motion and breathing artefacts [ 6 ] ; direct visualisation of the thrombus in segmental or subsegmental arteries ; and good interobserver agreement [ 7 ]  . if the examination is extended to include the lower limbs and abdomen , there is the additional possibility of performing ct venography with a single injection of contrast material [ 8 ]  . furthermore , ct provides visualisation of both mediastinal and parenchymal structures , allowing for alternative diagnoses , a particularly important aspect if one considers that the clinical presentation is often nonspecific and the differential diagnosis includes many cardiopulmonary conditions . in recent years , an increasing number of studies has lembolia polmonare ( ep ) rappresenta unemergenza cardiovascolare relativamente comune che , determinando lostruzione del letto arterioso polmonare , pu indurre grave scompenso acuto del ventricolo destro anche se potenzialmente reversibile . 
langio - tomografia computerizzata ( tc ) polmonare multistrato si affermata negli ultimi anni come principale metodica di imaging nel confermare il sospetto clinico di ep acuta , sostituendo la scintigrafia ventilo / perfusionale e langiopneumografia [ 13 ]  . 
la concordanza di risultati tra la scintigrafia e la tc molto elevata in particolare quando le due indagini vengono effettuate entro 2448 ore dallinsorgenza del sospetto clinico [ 4 ]  . 
recentemente , la european society of cardiology ( esc ) nelle nuove linee guida per la diagnosi ed il trattamento della ep acuta , ha inserito langio - tc come indagine gold - standard , dopo liniziale valutazione clinica [ 5 ]  . lo sviluppo delle apparecchiature multidetettore ha portato una serie di vantaggi tecnici ( aumento della risoluzione spaziale e temporale , ottimale opacizzazione vascolare , diminuzione del rumore , ecc . ) e diagnostici : possibilit di eseguire lesame rapidamente anche in pazienti sofferenti ed intensamente dispnoici ; minimizzazione degli artefatti classici della tc generati dal movimento e dagli atti respiratori [ 6 ] ; visualizzazione diretta del trombo , fino ai rami subsegmentari con un buon accordo interobserver [ 7 ]  . 
con lestensione dellesame agli arti inferiori e alladdome vi la possibilit di eseguire anche una venografiatc con ununica iniezione di mezzo di contrasto ( mdc ) [ 8 ] ; inoltre la tc offre la possibilit di visualizzare sia le strutture mediastiniche che parenchimali e consente di formulare anche ipotesi diagnostiche alternative , aspetto 232 radiol med ( 2011 ) 116 : 230245 emphasised that decisions to adopt a more or less aggressive approach to pe should be based on risk stratification . progressive rv failure is the most frequent cause of death related to pe . 
the interventricular septum may protrude into an otherwise normal right ventricle , thus narrowing its lumen and causing incomplete filling , leading to decreased lv output and reduced systemic arterial pressure and coronary artery flow . 
additionally , the increase in rv wall tension produces compression of the right coronary artery and may trigger myocardial ischaemia and rv infarction . the new guidelines of the american college of chest physicians [ 9 ] confirm that treatment during the acute phase should be tailored to the individual patient based on clinical risk . 
lastly , high - risk patients , especially those with evidence of shock or hypotension , should receive thrombolytic therapy . clinical trials have demonstrated that cta can play a major role in evaluating the severity of acute pe , as it helps to assess numerous parameters : in particular , rv / lv ratio [ 1012 ] , interventricular septum displacement [ 11 ] and pulmonary artery [ 11 ] and superior vena cava [ 11 , 13 ] diameter . the presence , position and degree of pulmonary artery occlusion may be quantified by using vascular obstruction indices . 
despite their proven value in quantifying arterial obstruction , their use is limited by their complexity . recently , the qanadli score [ 14 ] , based on evaluation of all arterial branches involved in the obstruction , has been replaced by a score proposed by ghanima et al . 
 [ 15 ] , which is easier to apply in clinical practice . the aim of this study was to analyse the cta findings reflecting pe severity ; correlate them with clinical , laboratory and haemodynamic data ; and determine their value in predicting the development of chronic rv overload . 
lincremento delle resistenze vascolari polmonari determina un aumento della tensione di parete del ventricolo destro con conseguente dilatazione e alterazione funzionale . il setto interventricolare pu protrudere allinterno del ventricolo sinistro , di per s normale , restringendone la cavit e determinando un incompleto riempimento , con riduzione della portata ventricolare sinistra , della pressione arteriosa sistemica e del flusso coronarico . 
laumento della tensione di parete del ventricolo destro provoca inoltre una compressione sullarteria coronaria destra e pu scatenare unischemia cardiaca ed un infarto ventricolare destro . le ultime linee guida dellamerican college of chest physicians ( accp ) [ 9 ] confermano come la terapia in fase acuta dovrebbe essere personalizzata in ogni singolo paziente sulla base del rischio clinico . 
i pazienti a rischio intermedio , in apparenti condizioni di stabilit emodinamica al momento del ricovero , ma con segni di disfunzione ventricolare destra , necessitano di unintensificazione della terapia durante lospedalizzazione . 
infine i pazienti a rischio elevato , soprattutto se con segni di shock o ipotensione , devono essere sottoposti a terapia trombolitica . studi clinici hanno dimostrato come langio - tc possa avere un ruolo importante nella valutazione di gravit dellep acuta attraverso la valutazione di numerosi parametri : in particolare quelli maggiormente utilizzati sono stati il rapporto ventricolo destro ( vd ) / ventricolo sinistro ( vs ) [ 1012 ] , la deviazione del setto interventricolare [ 11 ] , il diametro dell arteria polmonare [ 11 ] , il diametro della vena cava superiore [ 11 , 13 ]  . 
from analysis of the ed registers for ct pulmonary angiography studies performed at the radiology unit of the ed , 79 patients with a diagnosis of acute pe were identified . patients with severe pre - existing cardiopulmonary disease were excluded from the study ( n = 14 ) , as were those with current neoplastic disease ( n = 8 ) , with previous episodes of pe ( n = 4 ) , for whom pe was not the primary diagnosis at presentation ( n = 5 ) and for whom no follow - up examination was carried out ( n = 3 )  . 
therefore , the study included 45 patients 29 women ( 65% ) and 16 men ( 35% ) aged 2692 ( mean 71 ) years at their first documented episode of acute pe and were followed up after 6 months . clinical presentation on admission to the ed was characterised by dyspnoea in 18 patients ( 40% ) , chest pain in ten ( 22% ) , syncope or lipothymia in nine ( 20% ) , asthenia and lower - limb oedema in seven ( 16% ) and shock in one ( 2% )  . in 30 patients ( 67% ) , the presence of deep venous thrombosis was demonstrated by ct venography ( n = 8 ) , lowerlimb compression ultrasound ( n = 25 ) or both ( n = 12 )  . patients clinical records were reviewed for troponin i levels , sonographic findings and length of stay in hospital and in the intensive care unit ( icu )  . 
only one patient underwent thrombolysis with a 10 - mg intravenous bolus of recombinant tissue plasminogen activator ( rtpa ) , followed by 85 mg administered over 2 h . patients were followed up by cta performed 6 months after the acute episode . 
the onset of chronic rv overload ( caused by ventricular free wall thickening and ventricular cavity enlargement ) or death during the hospital stay or within the 6 months prior to the first follow - up examination were considered negative outcomes . ct scanning protocol both diagnostic and follow - up cta was performed with a determinare la loro capacit di predire lo sviluppo di sovraccarico cronico del ventricolo destro . 
si voluto inoltre individuare quale , tra i parametri proposti in letteratura , sia pi affidabile e semplice , per una rapida applicazione alla diagnosi in urgenza . materiali e metodi popolazione di studio il nostro uno studio retrospettivo che ha preso in considerazione i pazienti afferiti consecutivamente al pronto soccorso di un policlinico universitario sede di un dipartimento di emergenza e accettazione ( dea ) di 2 livello , nel periodo compreso tra novembre 2007 e dicembre 2008 . 
consultando i registri degli esami angio - tc per lo studio delle arterie polmonari eseguiti presso la radiologia del pronto soccorso , sono stati individuati 79 pazienti con diagnosi di ep acuta . 
sono stati esclusi dallo studio i pazienti con gravi patologie cardio - polmonari pre - esistenti ( 14 ) , con patologie neoplastiche in atto ( 8 ) , con precedenti episodi di ep ( 4 ) , quelli per cui lep non era la diagnosi principale al momento del ricovero ( 5 ) ed infine quelli nei quali non stato possibile eseguire un esame di controllo ( 3 )  . 
sono stati quindi inclusi nello studio 45 pazienti , di cui 29 donne ( 65% ) e 16 uomini ( 35% ) , di et compresa tra 26 e 92 anni ( et media 71 anni ) al primo episodio documentato di embolia polmonare acuta , con follow - up a 6 mesi . il quadro di presentazione clinica al momento dellingresso in pronto soccorso era caratterizzato da : dispnea in 18 pazienti ( 40% ) , dolore toracico in 10 ( 22% ) , sincope o lipotimia in 9 ( 20% ) , astenia ed edema di arto inferiore in 7 ( 16% ) , shock in 1 ( 2% )  . 
in 30 pazienti ( 67% ) stata dimostrata la presenza di trombosi venosa profonda attraverso venografia - tc ( 8 ) , ultrasonografia compressiva ( cus ) degli arti inferiori ( 25 ) o entrambe le metodiche ( 12 )  . 
nello stesso giorno del ricovero veniva iniziata la terapia anticoagulante orale ( tao ) con warfarin 5 mg con lobiettivo di raggiungere un range terapeutico tale da mantenere il valore dellin234 radiol med ( 2011 ) 116 : 230245 multislice ct ( msct ) scanner ( somatom emotion 6 , siemens , forchheim , germany ) , following the ct protocol for pe [ 16 ]  . 
acquisitions were obtained using the spiral technique before and after intravenous administration of 100 cc nonionic iodinated contrast material ( iomeron 350 , bracco spa , milan , italy ) administered via a vein in the arm at a flow rate of 3 ml / s . the automatic care bolus scan - triggering system was used , with the scan starting 4 s after the contrast medium had reached the common pulmonary artery . 
the study of the lower limbs to identify deep venous thrombosis was done with the sequential technique and image acquisition from the popliteal fossa up to the upper kidney poles , with 10 - mm slice thickness and 180 - s delay . ternational normalized ratio ( inr ) tra 2 e 3 . 
un solo paziente stato sottoposto a trombolisi con attivatore tissutale del plasminogeno ricombinante ( rtpa ) in bolo endovenoso di 10 mg , seguito da infusione di 85 mg in 2 ore . levoluzione a distanza stata valutata attraverso lo studio degli esami angio - tc di controllo effettuati a 6 mesi dallepisodio acuto . 
lo sviluppo di un sovraccarico cronico del ventricolo destro ( determinato dallispessimento della parete libera del ventricolo e dallingrandimento della cavit ventricolare ) o il decesso , durante il periodo di ricovero o entro i 6 mesi fino al primo controllo , sono stati considerati come esiti negativi . protocollo di scansione tc image analysis all cta studies were assessed for the following parameters : rv / lv ratio obtained by calculating the ratio between the diameters of the rv and lv short axes in the axial plane , measured from the endocardial margin of the free wall to the interventricular septum [ 17 ] ; axial diameter of the superior vena cava , 2.5 cm from its entrance into the right atrium [ 11 ] ; maximum diameter of the common trunk of the pulmonary artery in the axial plane [ 11 ] ; vascular obstruction score according to qanadli [ 14 ] ( 0100% obstruction ) defined by the number of obstructed segmental arteries and corrected on the basis of the estimated degree of occlusion of each vessel ( correction factor : 1 = partial obstruction ; 2 = complete obstruction ) ; obstruction score according to ghanima [ 15 ] based on proximal extension of the thrombus relative to the main pulmonary arteries ( clot burden )  . 
the pulmonary artery tree is subdivided into four components , and the score is determined according to the level of the proximal extension of the thrombus in each lung : mediastinal arteries ( 4 points ) , lobar arteries ( 3 points ) , segmental arteries ( 2 points ) and subsegmental ( 1 point )  . 
for a more detailed description of vascular obstruction scores , see appendix 1 . statistical analysis gli esami angio - tc sono stati eseguiti sia in fase diagnostica che durante il controllo evolutivo utilizzando tomografo computerizzato multistrato ( tcmd ) somatom emotion 6 ( siemens , forcheim , germania ) seguendo il protocollo tc embolia polmonare [ 16 ]  . 
le scansioni sono state effettuate senza sincronizzazione elettrocardiografica ( ecg ) , comprendendo il parenchima polmonare dagli apici alle basi con spessore di acquisizione 1 , 25 mm , ricostruzioni a 0 , 8 mm , 120 kv , 110 mas . 
le acquisizioni sono state eseguite con tecnica spirale prima e dopo somministrazione di 100 cc di mezzo di contrasto iodato non ionico ( iomeron 350 , bracco spa , milano , italia ) endovena , al flusso di 3 ml / s introdotto a livello di una vena del braccio . 
il completamento diagnostico a livello degli arti inferiori stato effettuato con tecnica sequenziale mediante acquisizioni dai cavi poplitei fino al margine superiore dei reni , con spessore di strato di 10 mm e delay di 180 s , per identificare eventuali trombosi venose profonde . analisi delle immagini per ogni paziente , dallesame angio - tc sono stati valutati i seguenti parametri : rapporto vd / vs ; ottenuto valutando il rapporto tra i diametri degli assi minori del vd e del vs in sezione assiale misurati dal margine endocardico della parete libera a quello del setto interventricolare [ 17 ] ; diametro assiale della vena cava superiore a 2 , 5 cm dallo sbocco nellatrio destro [ 11 ] ; diametro massimo del tronco comune dellarteria polmonare in sezione assiale [ 11 ] ; the kruskal - wallis test was used to compare the continindice di ostruzione vascolare secondo qanadli [ 14 ] radiol med ( 2011 ) 116 : 230245 uous values of the qanadli scoring system with the groups obtained with the ghanima score . 
fishers exact and chisquare tests were used to assess the significance of the association between outcome and parameters examined . receiver operating characteristic ( roc ) curve was used to identify the cutoff values for the rv / lv ratio and the qanadli score . 
sensitivity , specificity and positive predictive values ( ppv ) and npv were measured using openepi software ( the open source initiative )  . results follow - up cta angiography showed complete embolism resolution in 15 patients ( 33% ) , residual thrombi in some arterial branches in 13 ( 29% ) and chronic rv overload ( pulmonary heart disease ) in 13 ( 29% )  . 
death caused by cardiocirculatory failure occurred in four patients ( 9% )  . altogether , the outcome was positive in 28 patients ( 62% ) and negative in 17 ( 38% )  . 
median obstruction , corresponding to level 1 of the ghanima system , corresponds to 7.5% in the qanadli index ; levels 2 , 3 and 4 correspond to a 20% , 35% and 50% median obstruction , respectively . 
distribution of the study population according to the ghanima score was as ( ostruzione 0%100% ) , definito dal numero di arterie segmentarie ostruite , corretto in base alla stima del grado di occlusione di ogni singolo vaso ( fattore di correzione : 1 ostruzione parziale , 2 ostruzione completa ) ; indice di ostruzione secondo ghanima [ 15 ] , basato sulla prossimalit della trombosi rispetto allarteria polmonare principale ( burden embolico )  . 
lalbero arterioso polmonare suddiviso in 4 componenti : lestensione dellembolo a livello delle arterie mediastiniche conferisce un punteggio di 4 , arterie lobari 3 , arterie segmentali 2 e subsegmentali 1 . 
si individuano pertanto 4 livelli di gravit , in senso crescente dal livello 1 al livello 4 . per una descrizione pi dettagliata degli indici di ostruzione vascolare , vedi appendice 1 . analisi statistiche il test di kruskall - wallis stato utilizzato per confrontare i valori continui dellindice qanadli con i gruppi dellindice ghanima . 
lostruzione mediana corrispondente al grado 1 dello score ghanima pari al 7 , 5% secondo lo score qanadli ; i gradi 2 , 3 e 4 corrispondono rispettivamente ad unostruzione mediana del 20% , 35% e 50% . 
 236 radiol med ( 2011 ) 116 : 230245 risultati lo studio angio - tc di controllo in 15 pazienti ( 33% ) ha documentato una risoluzione completa dellembolia ; in 13 pazienti ( 29% ) erano visibili residui trombotici in alcuni rami arteriosi ; un sovraccarico cronico del ventricolo destro ( cuore polmonare ) stato riscontrato in 13 pazienti ( 29% )  . 
il decesso , per linstaurarsi di uno scompenso cardiocircolatorio , si verificato in 4 pazienti ( 9% )  . complessivamente 28 pazienti ( 62% ) hanno avuto una prognosi positiva e 17 ( 38% ) prognosi negativa . stata riscontrata una significativa associazione tra lo score ghanima e quello di qanadli : i due indici risultano equivalenti nel quantificare lostruzione del circolo arterioso polmonare ( significativit : p < 0 , 001 )  . 
lostruzione mediana corrispondente al grado 1 dello score ghanima pari al 7 , 5% secondo lo score qanadli ; i gradi 2 , 3 e 4 corrispondono rispettivamente ad unostruzione mediana del 20% , 35% , e 50% . 
la popolazione di studio secondo lo score ghanima cos distribuita : 5 pazienti di grado 1 , 5 di grado 2 , 11 di grado 3 e 24 di grado 4 . 
i pazienti a prognosi negativa ( cuore polmonare cronico o decesso ) e quelli a prognosi positiva ( risoluzione completa o risoluzione con residui embolici ) si distribuiscono diversamente nei 4 gradi del nuovo score . 
2 , lo score ghanima permette una stratificazione prognostica dei pazienti gi al momento della diagnosi in urgenza attraverso lo studio delle immagini angio - tc : il grado 4 riunisce l88% dei pazienti a prognosi peggiore ( 15 pazienti ) , in particolare vi appartengono tutti e quattro i casi di decesso . 
considerando come cut - off il grado 4 , in relazione alla prognosi lindice di ghanima ha mostrato sensibilit 88% , specificit 68% , valore predittivo positivo ( vpp ) 62% , valore predittivo negativo ( vpn ) 90% e accuratezza 76% , con il riscontro di 9 falsi positivi e 2 falsi negativi ( tabella 1 )  . analizzando il periodo di ricovero emerso come la degenza media aumenti in relazione al grado di ostruzione vascolare : i pazienti del gruppo 1 hanno avuto una media di 6 giorni di ricovero ( 2 deviazioni standard [ ds ] ) ; quelli del gruppo 2 una media di 8 giorni ( 4 ds ) ; gruppo 3 di 11 giorni ( 8 ds ) ; e gruppo 4 di 13 giorni ( 8 ds )  . 
infatti un solo paziente ( 20% ) al grado 1 ed uno solo ( 20% ) al grado 2 della classificazione di ghanima sono stati ricoverati in reparti di terapia intensiva ed entrambi per una sola giornata ; al grado 3 i ricoveri salgono fig . 
il 18% dei pazienti di grado 3 ( 2 pazienti ) hanno sviluppato un sovraccarico cronico del ventricolo destro ( 12% del totale dei pazienti a prognosi negativa )  . 
2 , the ghanima score allows for a prognostic stratification of patients at the time of diagnosis with emergency cta : level 4 was identified in 88% of patients with the worst outcomes ( n = 15 ) , and in particular in all four cases of death . 
if we consider level 4 as the cutoff value , radiol med ( 2011 ) 116 : 230245 the ghanima score in relation to outcome had 88% sensitivity , 68% specificity , 62% ppv , 90% npv and 76% accuracy , with nine false positive and two false negative results ( table 1 )  . analysis of the length of hospital stay showed that the average hospital stay increases with the degree of vascular obstruction : the average hospital stay was 6 days [ 2 standard deviation ( sd ) ] for level 1 patients , 8 days ( 4 sd ) for level 2 , 11 days ( 8 sd ) for level 3 and 13 days ( 8 sd ) for level 4 . 
the qanadli score cutoff value for poor outcome was set at 40% vascular obstruction , yielding 82% sensitivity , 61% specificity , 56% ppv , 85% npv , 69% accuracy and 11 false positive and three false negative results . 
the cutoff value for the rv / lv ratio was set at 1.4 , yielding 62% sensitivity , 83% specificity , 76% ppv , 71% npv and 73% accuracy , with four false positive and eight false negative results ( table 1 )  . 
cutoff values were consistent with those reported in numerous previous studies [ 10 , 12 , 14 , 15 ]  . troponin i values > 0.01 ng / ml were considered positive . this test had 89% sensitivity , 77% specificity , 74% ppv , 91% npv and 82% accuracy in identifying patients with poor outcome , with six false positive and two false negative results . 
ricordando che valori prossimi a 1 , 0 indicano unelevata accuratezza diagnostica , i nostri risultati hanno portato ad un auroc rispettivamente di 0 , 791 ( 95% indice di confidenza [ ic ] , 0 , 6500 , 932 ) e di 0 , 853 ( 95% ic , 0 , 7460 , 960 )  . 
per la popolazione in studio il cut - off dellindice di qanadli predittivo di esito negativo stato posto al 40% di ostruzione vascolare , con sensibilit 82% , specificit 61% , vpp 56% , vpn 85% , accuratezza 69% e il riscontro di 11 falsi positivi e 3 falsi negativi . 
per il rapporto vd / vs il cut off pari a 1.4 , con sensibilit 62% , specificit 83% , vpp 76% , vpn 71% , accuratezza 73% , con 4 falsi positivi e 8 falsi negativi ( tabella 1 )  . 
i valori cut - off identificati sono risultati in accordo con quelli di numerosi altri studi [ 10 , 12 , 14 , 15 ]  . un valore di troponina i superiore a 0 , 01 ng / ml stato considerato come positivo . 
questo test ha mostrato sensibilit 89% , specificit 77% , vpp 74% , vpn 91% e accuratezza 82% nellindividuare i pazienti a prognosi negativa , con 6 falsi positivi e 2 falsi negativi . 
lecocardiografia ha mostrato sensibilit 79% , specificit 65% , vpp 62% , vpn 81% e accuratezza 71% , con 9 falsi positivi e 4 falsi negativi ( tabella 1 )  . 
i dati relativi al diametro della vena cava superiore e del tronco comune dellarteria polmonare non sono risultati statisticamente significativi ( p > 0 , 05 )  . discussione importante poter quantificare lostruzione vascolare vista con langio - tc , perch la tomografia computerizzata usata quotidianamente come metodo iniziale e al tempo stesso pi accurato per diagnosticare lep acuta . 
il grado di ostruzione permette una stratificazione del rischio : pu prospettare lesito infausto , lo sviluppo di cuore polmonare cronico ed essere di aiuto per le scelte terapeutiche da seguire . 
consentono infatti di differenziare tra unostruzione parziale ed una totale e , nonostante le loro differenze metodologiche , hanno 238 radiol med ( 2011 ) 116 : 230245 radiol med ( 2011 ) 116 : 230245 vd / vs reference line specificity fig . 
auroc rispettivamente di 0 , 791 ( 95% ic , 0 , 6500 , 932 ) e di 0 , 853 ( 95% ic , 0 , 7460 , 960 )  . stratification : it may predict a fatal outcome or onset of chronic pulmonary heart disease and help in selecting the most appropriate treatment . the first scoring systems were those proposed for angiography by miller et al . 
although the scores were also adapted for ct , they were limited by an inability to differentiate partial from complete obstruction of pulmonary artery branches . the scoring systems suggested by qanadli et al . 
in fact , they can facilitate distinguishing partial from complete obstruction and , despite their methodological differences , have shown excellent correlation with each other in several studies [ 21 ] , as well as proving to be reliable for patient stratification . 
 [ 11 ] , patients with severe pe ( with evidence of haemodynamic instability ) had an obstruction index of 54%11% , whereas those with nonsevere pe ( stable and treated with heparin ) had an index of 24%18% . 
 [ 23 ] analysed 33 consecutive cases of massive pe , defined as pe associated with systolic arterial pressure < 90 mmhg or a pressure mostrato uneccellente correlazione reciproca in differenti studi [ 21 ] dimostrandosi affidabili anche nella stratificazione di gravit dei pazienti . 
nello studio di collomb et al . [ 11 ] i pazienti con ep severa ( con segni di instabilit emodinamica ) presentavano un indice di ostruzione di 54%11% , mentre quelli con ep non severa ( stabili e trattati con leparina ) di 24%18% . 
lo studio di qanadli et al . [ 14 ] propone un cut - off del 40% , atto ad individuare pi del 90% dei pazienti con disfunzione acuta del ventricolo destro . 
 [ 10 ] studiarono il rapporto tra la disfunzione del vd e lindice di ostruzione tc nei pazienti con ep acuta emodinamicamente stabili e trovarono che il valore medio di ostruzione era 31 , 8%22 , 9% . 
 [ 23 ] analizzarono 33 casi consecutivi di ep massiva , definita come unep associata a pressione arteriosa sistolica < 90 mmhg o a un calo pressorio 40 mmhg per almeno 15 minuti . 
necessita infatti di unaccurata valutazione delle arterie segmentarie e subsegmentarie , che spesso non possibile effettuare , soprattutto 240 radiol med ( 2011 ) 116 : 230245 drop 40 mmhg for at least 15 min 61% of cases , the embolus affected the main pulmonary artery , and in all cases except one it was bilateral . 
as a result , risk is stratified by using other ct parameters , such as the rv / lv ratio , or by ecg and laboratory tests . an important predictive role is that played by troponins , which are nonetheless limited by the need to wait for the test results , with waiting times that vary according to the medical centre . 
an increase in these biomarkers has been found to correlate with the ecg and cta findings of rv dysfunction , and they have a high npv both in terms of mortality and morbidity [ 24 , 25 ]  . 
ecg , whether transthoracic or transoesophageal , has a high sensitivity in screening patients for ventricular dysfunction , although not all these patients will develop chronic rv overload . furthermore , except in rare cases , this method is unable to provide definite confirmation of the presence of pe and is therefore used as a second - line modality for patient assessment [ 26 ]  . the ghanima score [ 15 ] proved to be easy to calculate and equivalent to the other more complex obstruction indices used to quantify embolisit allows determination of the total clot burden on the basis of the proximal extension of the thrombus relative to the main pulmonary artery and its bilateral presence . 
our study shows that the ghanima score has the best prognostic accuracy compared with other cta parameters , as well an ability to screen patients for chronic pulmonary heart disease that is more accurate than that of ecg . 
lincremento di questi biomarkers stato correlato ai dati ecocardiografici ed angio - tomografici di disfunzione ventricolare destra ed ha alto valore predittivo negativo sia in termini di mortalit che di morbilit [ 24 , 25 ]  . 
inoltre questa metodica non permette , salvo casi eccezionali , di documentare con certezza la presenza di embolia polmonare ed quindi utilizzata come metodica di 2 livello nella valutazione del paziente [ 26 ]  . 
il nostro studio ha dimostrato che lindice di ghanima possiede la migliore accuratezza prognostica rispetto agli altri parametri angio - tc e una capacit superiore anche allecocardiografia di individuare i pazienti che svilupperanno il cuore polmonare cronico . 
lo studio dimostra come lelevazione dei valori della troponina i ( valore cut - off utilizzato > 0 , 08 ng / ml ) ha sensibilit 53 , 8% , specificit 92 , 3% , vpp 70% e vpn 85 , 7% nellevidenziare lostruzione embolica dei rami arteriosi maggiori . le arterie polmonari principali risultano coinvolte nel 70% dei pazienti con elevazione della troponina i e solo nel 14 , 3% dei pazienti con valori sottosoglia . la figura 4 si riferisce allangio - tc di un paziente di 79 anni , con sintomatologia di dispnea ingravescente . 
a , b computed tomography angiography ( cta ) performed as the initial diagnostic investigation : obstruction of middle lobe branch and right basal pyramid ( arrows in a ) ; obstruction of superior lingular segment ( arrow in b )  . 
ghanima score was level 3 ; qanadli obstruction index was 35% ; right ventricular / left ventricular ratio was 1 ; troponin i was 0.01 ng / ml ; echocardiography was normal . 
le immagini a e b si riferiscono allangio - tc eseguita in fase diagnostica iniziale : ostruzione del ramo lobare medio e piramide basale destra ( frecce in a ) ; ostruzione del segmento lingulare superiore ( freccia in b )  . 
fig. 5a , b refers to cta performed on admission and show bilateral obstruction of the central pulmonary arteries ( a ) with dilatation of the right atrium and ventricle ( b )  . 
troponin i level was 0.05 ng / ml , and ecg revealed rv dilatation . figure 5c , d refers to follow - up cta and show the partial resolution of embolism with few persisting segmental and subsegmetal filling defects ( c , arrows )  . 
a , b computed tomography angiography ( cta ) performed as the initial diagnostic investigation : massive pulmonary embolism with bilateral obstruction of the main pulmonary arteries ( a ) ; right atrial and ventricular enlargement ( b )  . 
ghanima score level 3 ; qanadli obstruction index 35% ; right ventricular / left ventricular ratio was 1 ; troponin i was 0.01 ng / ml ; echocardiography was normal . 
score ghanima grado 4 ; indice di ostruzione qanadli 60% ; rapporto vd / vs 2 , 1 ; troponina i 0 , 05 ng / ml ; allecocardiografia dilatazione ventricolo destro . 
le immagini c e d si riferiscono allangio - tc di controllo e mostrano la risoluzione parziale dellembolia con persistenza di alcuni difetti di riempimento segmentari e sub - segmetari ( frecce in c )  . 
il ventricolo destro risulta ancora lievemente dilatato ( d )  . our data suggest that clinical severity and outcome of pe are associated with the proximal extension and bilateral presence of the thrombus . 
pulmonary circulation , which normally has a low resistance , is able to compensate for increases in pressure , even when these are produced by a very marked obstruction of the pulmonary circulation ; however , this is unlikely to occur if both lungs are involved and if the embolism affects , even in part , the major arteries . 
instead , it is much easier and more reliable to determine the most proximal level reached by the thrombus inside the pulmonary artery branches . logistic analysis was not performed owing to the e la bilateralit della trombosi . 
la circolazione polmonare , normalmente a bassa resistenza , riesce a compensare gli aumenti pressori dovuti allostruzione anche di una quota elevata di circolo polmonare , questo per avviene difficilmente se entrambi i polmoni sono colpiti e se lembolia coinvolge , anche parzialmente , le arterie di maggior calibro . 
non risulta pertanto vantaggioso conteggiare ogni singolo embolo per calcolare la percentuale di letto vascolare ostruito , bens molto pi semplice , ma allo stesso tempo affidabile , determinare il livello pi alto raggiunto dal trombo nei rami arteriosi polmonari . le limitazioni dovute alla retrospettivit e al basso numero di casi presi in esame hanno fatto s che lo studio non sia stato completato con unanalisi logistica dei risultati . 
in our opinion , a larger study correlating the ghanima score and troponin determination could provide a diagnostic protocol for rapid stratification of cases of embolism with cardiorespiratory instability . total clot burden could be useful to limit the use of cardiac biomarkers and select patients for ecg , thus streamlining the management of acute pe and resource utilisation . 
radiology reports usually describe the location of the emboli : including an indication of clot burden as well could represent a valuable step in this direction . relazione lo score di ghanima con il dato laboratoristico delle troponine sarebbe possibile , a nostro avviso , identificare un protocollo diagnostico per la stratificazione rapida dei casi di embolia con instabilit cardio - respiratoria . 
il total clot burden potrebbe essere utile per restringere luso dei biomarkers cardiaci e per selezionare i pazienti da inviare allo studio ecocardiografico , permettendo in questo modo di snellire il management dellep acuta e di usufruire in maniera razionale delle risorse disponibili . 
la posizione degli emboli solitamente descritta nei referti radiologici : indicare anche il grado del burden embolico potrebbe essere un importante passo in questa direzione . conclusions conclusioni the extent of embolic burden , determined according to the ghanima score , may be used in cta diagnosis as a prognostic marker for rapid stratification of pulmonary heart disease or death risk in patients with acute pe . 
this approach provides , with the use of a single test , both a diagnosis of pe and a relatively accurate risk stratification . lestensione del burden embolico , calcolata secondo lo score ghanima , pu essere utilizzata nella diagnosi angiotc in urgenza come marker prognostico per una rapida stratificazione del rischio di cuore polmonare o decesso dei pazienti con ep acuta . 
indici di ostruzione vascolare qanadli score qanadli score pulmonary arteries are subdivided into ten segmental arteries in each lung ( three to the upper lobe , two to the middle lobe and lingula , five to the lower lobe )  . 
the presence of an embolus in a segmental artery is scored as 1 point , and more proximal emboli are scored a value equal to the number of segmental branches arising from the affected vessel . 
each score is multiplied by 0 , or 1 , or 2 according to the estimated degree of vascular occlusion ( 0 = no obstruction ; 1 = partial occlusion ; 2 = complete occlusion )  . 
the percentage value is then calculated as : ( nd ) / 40100 [ n = score of the embolus multiplied by the number of dependent segments ( min = 1 ; max = 20 ) ; d = degree of obstruction ( min = 0 , max = 2 ) ]  . le arterie polmonari vengono suddivise in 10 arterie segmentarie per polmone ( 3 per il lobo superiore , 2 per il lobo medio e per la lingula , 5 per il lobo inferiore )  . 
la presenza di un embolo in unarteria segmentaria viene calcolato con 1 punto , la presenza di un embolo pi prossimale viene calcolato con tanti punti quanto sono i vasi segmentari che nascono dal vaso colpito . 
ogni singolo punteggio viene moltiplicato per 0 oppure 1 oppure 2 , in relazione alla stima del grado di occlusione del vaso ( 0 = nessuna ostruzione ; 1 = occlusione parziale ; 2 = occlusione totale )  . 
il rilievo di un embolo subsegmentario viene calcolato come un embolo nella corrispondente arteria segmentaria , con sola parziale occlusione ( valore 11 = 1 )  . lintervallo del qanadli score varia da 0 ( normale ) a 40 ; la misura percentuale viene quindi calcolata : ( nd ) / 40100 ( n = valore embolo per il numero di segmenti dipendenti [ min 1 ; max 20 ] ; d = grado di ostruzione [ min = 0 , max = 2 ] )  . ghanima score ghanima score this score measures the proximal extension of the embolus relative to the main pulmonary artery and its branches . 
the pulmonary artery tree is divided into four components : an embolus at the level of the mediastinal lindice valuta il grado di prossimalit della trombosi polmonare rispetto allarteria polmonare principale e alle sue branche . 
lalbero arterioso polmonare suddiviso in 4 componenti : se lembolo si trova a livello delle arterie 244 radiol med ( 2011 ) 116 : 230245 arteries is scored 4 points , at the lobar arteries 3 points , at the segmental arteries 2 points , and at the subsegmental arteries 1 point . 
the score identifies four levels of severity ranging from 1 to 4 . mediastiniche si applica un punteggio di 4 , arterie lobari 3 , arterie segmentali 2 e subsegmentali 1 . 
in this phase , we exposed a polymethyl - methacrylate ( pmma ) phantom to the two mammography units and recorded the exposure parameters used by thethe phantom was subsequently replaced by a dedicated radcal ionisation chamber on which preliminary dose assessments were conducted . 
scopo del nostro lavoro stato quello di veri care quale tipo di mammografo digitale sia meglio dedicare alle indagini di screening in base al noto principio as low as reasonably achievable ( alara ) della radioprotezione di limitazione della dose . 
si quindi proceduto alla comparazione della qualit delle immagini prodotte avvalendosi di un fantoccio con inserti geometrici impostando , su ciascun mammografo , i parametri di esposizione utilizzati per le valutazioni dosimetriche . 
stato riscontrato un risparmio di dose impartita alle pazienti avvalendosi del sistema con anodo in tungsteno ; il selenia - w stato , per tanto , adibito alle attivit di screening della mammella . 
 parole chiave mammogra a digitale dose radiol med ( 2011 ) 116 : 310318 introduction introduzione the purpose of this study was to compare the performance of two digital mammography units produced by the same company ( hologics lorad selenia model ) , featuring similar structural characteristics but using different materials for their target / lter combinations [ 1 , 2 ]  . 
the second unit was installed in early 2009 , giving us a choice as to which unit to assign to screening activities . when choosing a unit to be allocated to screening mammography , special care should be taken to apply the principle of optimisation [ 1 , 2 ] of radiological procedures . 
the aim is to comply with italian legislative decree 187 / 2000 [ 3 ] , which in article 4 ( optimisation ) and article 9 ( special practices ) focuses in particular on screening programmes , as they involve a large number of potentially healthy people [ 4 ]  . 
as a result , we decided to perform a patient dose and image quality evaluation for the two systems at our disposal . the dose indicators compared were breast entrance surface dose ( esd ) and average glandular dose ( agd )  . 
 the former parameter is used as a reference to optimise the examination for evaluating as envisaged by legislative decree 187 / 00 compliance with reference diagnostic levels ( rdl ) , whereas the latter is recognised internationally as an indicator of radiological risk associated with the examination . 
 scopo del presente lavoro il confronto delle prestazioni offerte da due mammogra digitali prodotti dalla stessa ditta ( hologic lorad , modello selenia ) , con caratteristiche costruttive analoghe , ma diversi materiali per laccoppiata anodo / ltro [ 1 , 2 ] ; il ne ultimo del lavoro decidere quale mammografo sia da preferire per le indagini di screening della popolazione femminile . 
il primo mammografo ( selenia - molibdeno [ mo ] ) , utilizzato nella nostra realt a partire dallanno 2006 , soddisfacendo alle richieste di screening e di mammogra a clinica ; nei primi mesi del 2009 stata installata la seconda apparecchiatura , consentendoci di dedicare un mammografo allattivit di screening . nella scelta dellapparecchiatura da dedicare allo screening mammogra co particolare cura deve essere posta al principio di ottimizzazione [ 1 , 2 ] della pratica radiologica in oggetto ; questo anche al ne di ottemperare al d.lgs. 
4 ( ottimizzazione ) e 9 ( pratiche speciali ) pone particolare attenzione proprio ai programmi di screening dal momento che coinvolgono un gran numero di persone potenzialmente sane [ 4 ]  . 
 gli indicatori di dose confrontati sono la dose in ingresso alla mammella ( esd ) e la dose ghiandolare media ( agd ) ; il primo parametro utilizzato come riferimento per lottimizzazione dellesame ai ni della valutazione prevista dal d.lgs 187 / 00 per il rispetto dei livelli diagnostici di riferimento ( ldr ) , mentre il secondo riconosciuto a livello internazionale come rappresentativo del rischio radiologico associato allesame . 
lo studio sulla qualit dimmagine stato condotto da medici radiologi di comprovata esperienza nella refertazione delle immagini mammogra che ; a tal ne ci si avvalsi delle immagini ottenute dallesposizione di fantocci geometrici e delle immagine cliniche . 
 materials and methods materiali e metodi the mammography units in question are equipped with the same dr detector , made of amorphous selenium [ 5 , 6 ] , 24 30 cm2 in size , but differ in the materials used for targets and additional lters . 
the selenia device , hereafter referred to as selenia - mo , is tted with a molybdenum ( mo ) target and molybdenum and rhodium ( rh ) additional ltration , whereas the selenia - w has a tungsten ( w ) anode and rhodium and silver ( ag ) additional ltration . 
upon receiving the devices , we collaborated with hologics technicians to optimise the response of the digital detector , and a i mammogra oggetto di studio sono dotati dello stesso rivelatore dr , in selenio amorfo [ 5 , 6 ] di dimensioni 2430 cm2 , essi differiscono per il materiale costituente gli anodi ed i ltri aggiuntivi . 
il selenia , indicato nel seguito con seleniamo , corredato di anodo in molibdeno e ltri aggiuntivi di mo e rodio ( rh ) , mentre il selenia - w ha lanodo in tungsteno ( w ) e ltri aggiuntivi di rodio e argento ( ag )  . 
entrambe le apparecchiature sono state sottoposte ad un rigido programma di garanzia di qualit che ha seguito lintero processo diagnostico dallacquisizione delle immagini alla loro visualizzazione su monitor di refertazione e alla stampa su pellicola . 
in fase di accettazione delle apparecchiature si collaborato con i tecnici della ditta hologic per ottimizzare la risposta del rivelatore digitale , si quindi messo a punto un programma di controllo di qualit secondo le indicazioni 312 radiol med ( 2011 ) 116 : 310318 quality assurance programme was devised based on indications of the european guidelines for quality assurance in breast cancer screening [ 7 ]  . 
these guidelines focus mainly on training the radiology technicians involved in the weekly quality checks and period detector calibration [ 8 ]  . the reporting workstation is a 5 - mp double - monitor system calibrated to offer the same response by both monitors . 
after the acquisition chain was optimised and before using the selenia - w clinically , we performed a dosimetric comparison between the two mammography units on a standard breast simulated by a semicircular polymethyl - methacrylate ( pmma ) phantom ( 240 mm in diameter and 45 mm thick )  . 
at this preliminary stage , we exposed the standard phantom in a completely automatic mode , allowing the automatic exposure control of each unit to select the optimal working parameters ( target / lter combination , kv , mas ) , hereunder referred to as the standard exposure parameters . the dose delivered with the standard exposure parameters was measured with a radcal 20 6 - 6 m ionisation chamber placed in the reference point at 60 mm from the chest wall and 45 mm from the breast support table [ 10 ]  . 
after these preliminary evaluations , the seleniaw was introduced into clinical practice and , after nearly 1 month of operation , the doses effectively delivered to patients were assessed . all exposure parameters applied by each mammography unit to a sample of more than 400 women ( around 1 , 600 exposures ) were recorded using the digital imaging and communications in medicine ( dicom ) data sent automatically by the imaging system to the picture archiving and communications system ( pacs )  . 
the dicom header contains the patients name , age , exposure parameters ( kv , mas , projection , target lter combination , compression force ) and thickness of the compressed breast detected by the breast compression device with millimetric accucontenute nelleuropean guidelines for quality assurance in breast cancer screening [ 7 ] ; tale programma pone particolare attenzione alladdestramento dei tecnici sanitari di radiologia medica ( tsrm ) coinvolti nellesecuzione dei controlli settimanali e della periodica calibrazione del detettore [ 8 ]  . la stazione di refertazione costituita da un sistema doppio monitor da 5 mp ; essa stata calibrata in modo da garantire la stessa risposta per i due monitor e periodicamente controllata conformemente alle indicazioni dellamerican association of physicists in medicine ( aapm ) task group ( tg ) 18 [ 9 ]  . 
una volta ottimizzata la catena di acquisizione , prima dellutilizzo clinico del selenia - w , si proceduto ad un confronto dosimetrico tra i due mammogra su mammella standard simulata da fantoccio di polimetilmetacrilato ( pmma ) semicircolare di diametro 240 mm e spessore 45 mm ; in questa fase preliminare si scelto di esporre il fantoccio standard , in modalit totalmente automatica , lasciando al sistema del controllo automatico dellesposizione di ciascun mammografo , la scelta dei parametri ottimali di lavoro ( selezione anodo / ltro , kv , mas ) , nel seguito indicati come parametri di esposizione standard . la dose erogata con i parametri di esposizione standard , stata misurata avvalendosi di una camera a ionizzazione radcal 206 - 6m posta nel punto di riferimento sito a 60 mm dalla parete toracica e 45 mm dal piano di appoggio [ 10 ]  . 
 la qualit dimmagine stata valutata su entrambe le apparecchiature servendosi di un fantoccio contenente inserti geometrici ( leeds , tor max ) ; tale fantoccio , dello spessore di una mammella standard , stato esposto impiegando i parametri standard precedentemente determinati , quindi le immagini prodotte sono state esaminate dai medici radiologi . 
 il fantoccio tor max contiene al suo interno : mire a diversa frequenza spaziale ( da 1 a 20 lp / mm ) per la risoluzione ad alto contrasto nelle due direzioni parallela e ortogonale alla parete toracica , inserti circolari di diametro 5 , 6 mm a contrasto decrescente per la valutazione della sensibilit a basso contrasto , due gruppi di 11 inserti puntiformi di diametro 0 , 5 mm e 0 , 25 mm , per la valutazione dei micro - dettagli ad alto contrasto . 
successivamente a queste valutazioni preliminari , il selenia - w stato introdotto nella pratica clinica e , dopo circa un mese dallinizio del suo impiego , sono state valutate le dosi realmente impartite alle pazienti . stato possibile registrare tutti i parametri di esposizione impiegati su ciascun mammografo per un campione di oltre 400 donne ( circa 1600 esposizioni ) avvalendosi dei dati digital imaging and communications in medicine ( dicom ) inviati automaticamente dal sistema di acquisizione al picture archiving and communications system ( pacs )  . 
the s factor [ 13 , 14 ] corrects for differences between the various x - ray spectra that can be used with the different selected target / lter combinations . 
 results and discussion the exposures of a standard semicircular pmma phantom ( diameter 240 mm , thickness 45 mm ) for a preliminary dose evaluation were performed in a full automatic mode , allowing the unit to select the optimal parameters providing diagnostic images ; every measurement was repeated ten times to test the systems reproducibility . 
these same parameters were used when exposing the geometrical phantom ( tor max ) containing the high and low - contrast resolution inserts ; results of the evaluations conducted by the radiologists on the visible inserts are given in table 1 . the preliminary results of phantom exposures might seem to indicate that the two systems are substantially equivalent in terms of image quality but , at the same della dose in ingresso e della dose ghiandolare media nelle reali condizioni di esposizione . mediante la camera a ionizzazione stato misurato il kerma in aria in ingresso ( esak ) per unit di carico nel punto di riferimento , misurato alle diverse tensioni di utilizzo con tutte le combinazioni anodo / ltro disponibili ( r ) ; successivamente stato possibile stimare la dose in ingresso ( esd ) impartita alle pazienti nelle reali condizioni cliniche , avvalendo della formula : esd = rmas ( d1 / d2 ) 2bsf ( 1 ) dove d1 la distanza fuoco - punto di riferimento , d2 la distanza fuoco - pelle paziente e bsf il fattore di retrodiffusione tabulato in funzione del sev del mammografo [ 10 ]  . per la stima della dose ghiandolare media ( agd ) si utilizzata la formula delleuref [ 10 ] : agd = rmas ( d1 / d2 ) 2gcs ( 2 ) dove g e c sono valori tabulati in funzione dello spessore della mammella e della qualit del fascio ( hvl ) : il fattore g corrisponde ad una mammella costituita per il 50% da tessuto ghiandolare ed derivato dai valori calcolati in [ 11 , 12 ] , mentre il fattore c corregge per ogni variazione dalla composizione tipica del seno ( 50% di tessuto ghiandolare ) in funzione dellet della paziente ( < 50 anni e > 50 anni ) [ 11 , 12 ]  . 
 risultati e discussione le esposizioni su fantoccio standard semicircolare di pmma ( diametro 240 mm e spessore 45 mm ) per una valutazione preliminare delle dosi , sono state eseguite in modalit totalmente automatica lasciando al sistema la selezione dei parametri ottimali per il raggiungimento dellimmagine diagnostica ; ogni misura stata ripetuta 10 volte per testare la riproducibilit del sistema . 
 i valori medi di esposizione standard , registrati per le due apparecchiature , sono schematizzati in tabella 1 : il seleniamo ha sempre selezionato laccoppiamento anodo / ltro mo / mo , una tensione di 28 kv ed un carico medio di 68 , 7 mas ; il selenia - w ha sempre selezionato laccoppiamento anodo / ltro w / rh , una tensione di 28 kv ed un carico medio di 81 , 7 mas . 
questi stessi parametri sono stati impiegati per lesposizione del fantoccio geometrico ( tor max ) contenente gli inserti di risoluzione ad alto e basso contrasto ; i risultati delle valutazioni effettuate dai medici radiologi sugli inserti discriminabili sono schematizzati in tabella 1 . i risultati preliminari delle esposizioni su fantoccio , sembrerebbero indicare una sostanziale equivalenza dei due sistemi in termini di qualit dimmagine e , nel contempo , sembrerebbe sussistere un risparmio in termini di dose mediante limpiego del selenia - w . 
data required for analysis were identi ed within the dicom header , dividing to mammography them according unit , patients age , compressed breast thickness and target / lter combination . 
we found that selenia - w tends to select mainly the w / rh combination , with the w / ag combination being selected only for compression thicknesses of 70 mthe seleniamo , conversely , shows more variability in the combinations it selects , although for compression thicknesses 60 mm , it almost invariably selects the mo / rh . 
i dati necessari per lanalisi , sono stati ricercati allinterno dellheader dicom , suddividendoli in base al mammografo utilizzato , allet della paziente , allo spessore della mammella compressa e dellaccoppiata anodo / ltro utilizzata . 
 i tecnici di radiologia medica , nella pratica clinica , lavorano in modalit totalmente automatica , quindi il sistema a selezionare non solo i parametri di esposizione ottimali ma anche laccoppiata anodo / ltro pi indicata alla densit della mammella . 
abbiamo riscontrato che il selenia - w tende a selezionare prevalentemente laccoppiata w / rh e solo per spessori di compressione maggiori o uguali a 70 mm il sistema imposta laccoppiata w / ag . 
il selenia - mo , invece , presenta una variabilit maggiore nelle accoppiate selezionate , anche se per spessori di compressione superiori od uguali a 60mm , quasi esclusivamente impiegata la mo / rh . 
le valutazioni di dose su entrambi i sistemi sono state eseguite considerando tutte le quattro diverse accoppiate anodo / ltro selezionate nella realt clinica . i risultati riportati in figura 2 evidenziano che il ldr radiol med ( 2011 ) 116 : 310318 fig . 
1a , b distribuzione in classi di frequenza degli spessori di mammella compressa dellintero campione analizzato ( a ) e del campione relativo alla sola proiezione cc ( b )  . ering all four target / lter combinations used in clinical practice . the results given in fig . 
figure 3 shows the agd delivered by the two units , which are , in both cases , within the highest values accepted by the rispettato , con ampio margine , da entrambe le apparecchiature e che la dose impartita dal selenia - w risulta quasi dimezzata rispetto a quella del selenia - mo ; tale differenza risulta statisticamente signi cativa allanalisi di un test t di student condotto con un livello di con denza dell1% ( p = 0 , 00001 )  . lagd per esposizione il parametro dosimetrico correlato al rischio di tumore radioindotto , pertanto riveste fondamentale importanza per la valutazione del rapporto rischio / bene cio nei programma di screening mammogra co . 
in figura 3 si riportano le dosi ghiandolari medie impartite dai due mammogra che risultano , in entrambi i casi , inferiori ai valori massimi accettabili da [ 7 ] , tuttavia il confronto tra le due apparecchiature evidenzia un seppur lieve risparmio di dose ghiandolare media con limpiego del selenia - w . 
2a , b confronto tra selenia - mo e selenia - w in termini di esd impartita per a sola proiezione cc e b tutte le proiezioni . european guidelines for quality assurance in breast cancer screening [ 7 ] , even though the comparison between the two devices indicates a slightly lower ags being delivered by the selenia - w . 
mean agd values estimated for each device were analysed with students t test and a 1% con dence level ( p = 0.00001 ) , con rming the dose reduction obtained with the selenia - w . 
 conclusions the dose evaluations conducted by setting the exposure parameters used for standard breasts revealed given the valori medi di agd stimati per ciascuna apparecchiatura sono stati sottoposti a test t di student all1% ( p = 0 , 00001 ) di con denza che ha confermato la riduzione di dose mediante limpiego del selenia - w . 
in tabella 2 si riporta il riepilogo delle dosi stimate ed impartite dai due sistemi . conclusioni le valutazioni di dose effettuate impostando i parametri di esposizione impiegati per una mammella standard , hanno evidenziato a parit di qualit dimmagine , valutata su fantoccio contenente inserti geometrici , un risparmio di dose in termini di kerma in aria nellutilizzo del selenia - w ; questo dato preliminare ha trovato conferma nella pratica clinica , dove si assiste ad un quasi dimezzamento delle dosi in inradiol med ( 2011 ) 116 : 310318 fig . 
the indisputably lower dose delivered by the selenia - w mammography unit led us to allocate this equipment to the mammography screening examinations performed at our facility . disfano ai limiti di agd suggeriti dalleuropean reference organisation for quality assured breast screening and diagnostic services ( euref ) ; inoltre le immagini prodotte dai due selenia sono qualitativamente sovrapponibili . 
i valori di esd e agd impartiti da ciascun mammografo sono stati confrontati tramite test t di student e le differenze stimate sono risultate statisticamente signi cative con un livello di ducia dell1% . 
triulzi poletto editore srl , vermezzo ( milano ) , 2010 published online : 4 february 2011 springer - verlag 2011 on my desk rests a 647 - page book dedicated to paediatric radiology and neuroradiology . 
more than a third of the endeavour is dedicated to neuroradiology ( the main author and some of his co - authors are well - recognised neuroradiologists ) in its various aspects , from the very early stages of brain development to normal and abnormal ndings ( malformations , cerebralvascular pathology , metabolic and degenerative diseases , in ammation and infectious pathology , skull shape and hydrocephalus , tumours and trauma ) through different age groups . 
further information on spinal problems ( spine and spinal cord development , malformations , acquired lesions , craniocervical junction , anatomical variants and trauma ) is also presented . as magnetic resonance imaging is the ideal diagnostic tool for studying and documenting each of the above , the lions share of images is devoted to it , integrated with ultrasonography ( not extensively represented ) and a few computed tomographic images . 
in this respect , great importance is given to radiation protection for young patients , stressing that radiologists should use the least dangerous available instruments to safely image children . at the end of the neuroradiology section , the reader is introduced to general radiology , where lung , cardiovascular , gastrointestinal , genitourinary , osteoarticular apparatuses and trauma are extensively described . 
as in the neuroradiology section , there is usually an introduction , followed by sulla mia scrivania fa bella mostra di s un volume di 647 pagine dedicato alla radiologia e neuroradiologia pediatrica . 
pi di un terzo dellopera dedicato alla neuroradiologia ( lautore principale ed alcuni dei co - autori sono dei ben noti e rispettati neuroradiologi ) nei suoi vari aspetti , dagli stadi precoci dello sviluppo del cervello , ai reperti normali e patologici ( malformazioni , problemi cerebro - vascolari , malattie metaboliche e degenerative , infezioni e patologia infettiva , morfologia del cranio ed idrocefalia , tumori e trauma ) nelle differenti et . 
inoltre , vengono presentati e discussi dati ed informazioni sui problemi del rachide ( sviluppo del rachide e del midollo , malformazioni , lesioni acquisite , cerniera cranio - cervicale , varianti anatomiche e trauma )  . 
 dal momento che la risonanza magnetica ( rm ) lo strumento ideale per lo studio e la documentazione dei problemi di cui sopra , essa ricopre la parte del leone nelle immagini presentate , integrate da quelle ecogra che ( non in gran numero ) a da saltuarie immagini di tomogra a computerizzata ( tc )  . 
da questo punto di vista viene data grande importanza alla protezione dalle radiazioni , mettendo in evidenza come il radiologo dovrebbe utilizzare le apparecchiature disponibili meno pericolose nello studio per immagini dei bambini . al termine della parte dedicata alla neuroradiologia , il lettore viene messo davanti a quella dedicata alla radiologia generale in cui vengono trattati per esteso gli apparati respiratorio , cardiovascolare , gastrointestinale , genitourinario , osteoarticolare ed il trauma . 
 come gi nella sezione dedicata alla neuroradiologia , anche nelle altre lo schema del testo quello di dare un rapido inquadramento clinico - radiologico , seguito poi da nozioni di embriologia , anatomia e tecniche di immagine e dalla presentazione e discussione della malattia in questioradiol med ( 2011 ) 116 : 334335 embryology , anatomy and imaging techniques , followed by presentation and discussion of the affecting disease , giving attention to the different presentations in newborns ( premature babies , in particular ) and children . 
in this respect , one should note that the latest editions of the cited books are not always reported and also that some iconic texts are omitted ( for instance , see the sections on bone malformation )  . 
 da questo punto di vista il lettore dovrebbe tener conto che non sempre vengono indicate le ultime edizioni dei testi citati e che anche alcuni testi fondamentali sono stati dimenticati ( come per esempio nella sezione sulla malformazioni dello scheletro )  . 
simonetti2 1terapia radiante , universit degli studi di roma tor vergata ( ptv ) , viale oxford 81 , 00133 roma , italy 2dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica , roma , italy correspondence to : s . 
lobiettivo del nostro studio di valutare la capacit della risonanza magnetica ( rm ) nellidentificare localizzazione ed estensione del danno ischemico acuto , nel predire la reversibilit del danno e nel distinguere fra aree ischemiche acute e croniche nei pazienti con ischemia miocardica senza elevazione del tratto st ( nstemi )  . 
the use of routine imaging techniques such as echocardiography , which relies on contractility changes and possible myocardial thinning , does not always permit an optimal differential diagnosis , and in many cases , the true condition tends to be underestimated . 
the recent introduction of cardiac magnetic resonance ( mr ) imaging , with sequences for evaluating delayed enhancement , and the use of t2 - weighted blackblood short - tau inversion recovery turbo spin - echo ( t2 bbstir - tse ) acquisitions has made it possible to discriminate between the two pathological conditions by visualising the presence of myocardial oedema , which is usually associated with an ischaemic cardiac event . 
the mechanism underlying the formation of myocardial oedema in acute ischaemia is an injury to the cytoplasmic membrane and changes in transmembrane ion transport , which first trigger intracellular oedema - promoting conditions and then cytotoxic oedema , which involves a marked increase in locoregional extracellular water that can be revealed by t2 stir sequences [ 1 , 2 ]  . 
this condition tends to manifest within the first hours after the ischaemic event ( first 3 h ) and continues to increase over the following 2 weeks , when replacement fibrosis develops to an extent directly proportional to the duration of the ischaemic event [ 15 ]  . 
these pathophysiological mechanisms make it possible to ascertain the true conditions of the ventricular myocardium in the immediate subacute phase once the patients haemodynamic status has been stabilised and a certain and highly reliable prognosis has been established [ 6 ]  . 
in delineating the recovery of ventricular function in a patient who has suffered an acute coronary syndrome ( acs ) , magnetic resonance ( mr ) imaging allows both the identification of nonviable myocardium or myocardial scar from previous , more - or - less recent , episodes of ischaemiainfarction and depiction of any reactive oedema that has formed in the infarcted area . this allows identification of the so - called ischaemic penumbra that could be salvaged by immediate revascularisation [ 79 ]  . 
mr imaging has been shown to identify with a high level of sensitivity and specificity the area of mismatch il poter differenziare una condizione ischemica acuta da un quadro ischemico cronico pre - esistente attualmente il quesito diagnostico che pi frequentemente si propone nella routine clinica , soprattutto nelle condizioni acute o subacute ; ed il poter stabilire con certezza tale differenziazione alla base di una successiva e valida scelta terapeutica . 
ricorrendo alle tecniche strumentali di routine come lecocardiografia , basandosi sulle alterazioni della contrattilit e leventuale assottigliamento miocardico , non sempre si giunge ad una ottimale diagnosi differenziale ed in molte situazioni si tende a sottostimare la reale condizione . 
la recente introduzione della risonanza magnetica ( rm ) cardiaca , con sequenze per la valutazione dellenhancement tardivo e limpiego di scansioni black - blood ( bb ) turbo spin echo ( tse ) t2 ( short tau inversion recovery [ stir ] ) , dai dati presenti in letteratura stato possibile discriminare tra le due entit patologiche sfruttando proprio la possibilit di poter evidenziare la presenza delledema miocardico , che solitamente si associa ad un evento ischemico cardiaco . 
il meccanismo di base dello sviluppo delledema miocardico , negli eventi ischemici acuti , consiste in un danno della membrana citoplasmatica e soprattutto in una alterazione dei trasportatori ionici nei meccanismi di trasporto transmembrana , che dapprima innescano una condizione edemigena intracellulare e successivamente una condizione edemigena citotossica , che comporta un notevole aumento della componente idrica locoregionale extracellulare tale da poter essere rivelata con limpiego di sequenze t2 stir [ 1 , 2 ]  . 
tale condizione tende a manifestarsi nelle prime ore dellevento ischemico ( nelle prime 3 ore ) e successivamente continua ad incrementarsi nelle seguenti 2 settimane , lasciando gradualmente il posto a processi di sostituzione fibrotica del tessuto miocardico con unentit direttamente proporzionale alla durata dellevento ischemico [ 15 ]  . 
proprio sulla base di tali meccanismi fisiopatologici possibile discriminare la reale condizione del miocardio ventricolare nellimmediata fase sub - acuta una volta stabilizzato il quadro emodinamico del soggetto cos da poter delineare una prognosi sicura ed altamente affidabile [ 6 ]  . 
proprio nellottica di poter delineare la reale ripresa della funzione ventricolare di un soggetto colpito da una sindrome coronarica acuta , la rm consente di identificare sia il miocardio non vitale ovvero la scare esitata da pregressi eventi ischemici - infartuali pi o meno recenti e simultaneamente di delineare la condizione edemigena reattiva che si potrebbe innestare sulla stessa pregressa radiol med ( 2011 ) 116 : 163177 between chronic and acute ischaemic events in a noninvasive and highly reliable manner [ 1014 ]  . 
 the 2006 appropriateness criteria for cardiac computed tomography ( ct ) and mr imaging recognised that evaluating the location and extent of myocardial necrosis , including no - reflow regions , was an appropriate indication for cardiac mr viability assessment during the subacute phase of infarction [ 1518 ]  . 
the guidelines clearly also recognised as appropriate viability studies prior to revascularisation procedures , those performed to establish the likelihood of functional recovery , and to quantify viable areas in cases with equivocal results at single - photon - emission computed tomography ( spect ) or at dobutamine stress echocardiography [ 19 ]  . 
in addition to representing the gold standard in evaluating left ventricular wall thickness and kinetics , mr imaging is the only noninvasive technique capable of visualising directly not only the areas of myocardial necrosis through the delayed washout of contrast material but also left ventricular wall oedema through the use of t2 - weighted stir sequences . 
 the aim of this study was to assess the role of mr imaging in identifying the location and extent of acute ischaemic injury , predicting the reversibility or irreversibility of the injury and distinguishing acute from chronic ischaemic regions in patients with myocardial ischaemia with non - st - elevation myocardial infarction ( nstemi ) by using cine - mr imaging , delayed enhancement and t2 bb - stir sequences with fat suppression . 
 materials and methods between november 2006 and december 2007 , cardiac mr was performed on 22 patients ( 14 men and eight women ; mean age 5311 years ) with symptoms and electrocardiographic and cardiac enzyme changes ( troponin ) suggestive of nstemi infarction . 
the diagnosis was confirmed by coronary angiography ( ca ) that , combined with intracoronary ultrasound ( icus ) , allowed identification of the culprit lesion responsible for the acute event . 
on admission to the emergency department , all patients underwent preliminary echocardiography , which demonstrated a reduction in all ventricular function indices and segmental kinetic defects referable to coronary artery disease subsequently identified with ca . 
images were acquired with a 1.5area infartuale ; cos da poter individuare la cosiddetta zona di penombra ischemica , che potrebbe essere salvata dal progredire del fronte donda ischemico da un immediato e repentino trattamento di rivascolarizzazione [ 79 ]  . 
secondo questo punto di vista la rm consente di identificare con elevati valori di sensibilit e specificit larea di mismatch tra levento ischemico cronico ed acuto in modo non invasivo ed altamente affidabile [ 1014 ]  . 
 secondo le linee guida pubblicate nel 2006 sui criteri di appropriatezza nellesecuzione di esami di tomografia computerizzata ( tc ) e rm del cuore stata riconosciuta lappropriatezza degli studi di vitalit con rm nei pazienti nelle fasi post - acute dellinfarto al fine di valutare la localizzazione e lestensione della necrosi miocardica e delle regioni di non - reflow [ 1518 ]  . 
stato ovviamente riconosciuto come appropriato anche lo studio della vitalit prima di interventi di rivascolarizzazione , sia per la stima prognostica del recupero funzionale , sia per la quantificazione delle aree vitali nei casi con risultati dubbi alla tomografia computerizzata a emissione di fotoni singoli ( spect ) o alleco - stress con dobutamina [ 19 ]  . 
 materiali e metodi da novembre 2006 a dicembre 2007 sono stati sottoposti ad esame cardio - rm 22 soggetti ( 14 maschi e 8 femmine ; et media 5311 anni ) con sintomatologia , alterazioni del tracciato elettrocardiografico ( ecg ) e movimento enzimatico ( troponina ) riconducibili ad un quadro di infarto nstemi , confermato allesame coronarografico che integrato con valutazione icus ha consentito di individuare la lesione culprit responsabile dellevento acuto . 
tutti e 22 i pazienti , alla loro accettazione al dipartimento di emergenze , sono stati sottoposti ad un preliminare esame ecocardiografico , che ha documentato una riduzione in toto degli indici di funzionalit ventricolare , con i relativi deficit segmentari di cinetica da correlare con la coronaropatia successivamente individuata dallesame coronarografico . 
da tutti i pazienti stato ottenuto il consenso informato scritto e lo studio stato approvato dal comitato etico interno . 166 radiol med ( 2011 ) 116 : 163177 tesla scanner ( gyroscan intera , philips medical systems , best , the netherlands ) equipped with master gradients ( maximum gradient strength 30 mt ; slew rate 150 mt / m / ms . ) and dedicated five - element phased - array surface coil with sensitivity encoding ( sense ) technique . the examination protocol involved a preliminary cinemr study reduced to two planes biventricular short axis and subsequent four - chamber long axis view with turbo field echo , true fast imaging with steady precession , steady - state free precession ( tfe true - fisp - ssfp ) with retrospective electrocardiographic gating during inspiratory breath - holding , with the following scan parameters : tr 3.8 ms ; te 1.8 ms ; flip angle 70 ; matrix 256256 ; fov 400 ; slab 10 mm ; gap 0 ; sense acceleration factor 2.00 ; cardiac phases / cycle 20 ; retrospective gating ; two slabs per breath - hold ; breath - hold duration 1518 s . subsequently , t2 bb - stir - tse sequences with fat suppression were acquired with prospective electrocardiographic gating , through which we were able to identify and locate the reactive myocardial oedema . 
these scans are respectively obtained along the biventricular short axis ( six slices ) and twoor four - chamber long axis ( three slices ) , depending on the location of the ischaemic area , with the following parameters : tr 1333 ms ; te 100 ms ; epi factor 1 ; turbo factor 33 ; matrix 512512 ; fov 350 ; slab 8 mm ; gap 0.8 ; sense acceleration factor 1.00 ; diastolic phase ; slabs per breath - hold 1 ; breath - hold duration 1518 s . 
then , 1015 min after contrast administration , 3d t1 tfe - ir images were obtained to evaluate delayed enhancement . these sequences were acquired with retrospective electrocardiographic gating in the end - diastolic phase and oriented in the same planes as used for the cine - mr sequences and with the following parameters : tr 4.6 ms ; te 1.4 ms ; flip angle 15 ; matrix 256256 ; fov 400 ; slab 14 mm ; gap 7 mm ; sense acceleration factor 2.00 ; ti 260310 ms ; duration , 16 s . 
the results concerning segmental extent of delayed enhancement or signal hyperintensity in the t2 bb - tse sequences were expressed according to the standard 17 - segment model proposed by the american heart association ( aha ) [ 20 ]  . 
the analysis also included measurement of the indices of global left ventricular function , qualitative and quantitative analysis of end - diastolic wall thickness , systolic wall thickening and wall motility , with the aim of identifying segments with contractile abnormalities . 
 lesame rm stato eseguito circa 12 giorni dopo lo studio coronarografico e leventuale trattamento endovascolare , mentre lintervallo di tempo trascorso fra la comparsa dei sintomi e lesame stato in media di 2 , 7 giorni ( 1 , 4 giorni )  . 
sono stati esclusi dallo studio soggetti con quadro di ischemia miocardica acuta con elevazione del tratto st ( stemi ) , scompenso cardiaco di grado severo , claustrofobia e tutte le controindicazioni assolute allesame rm . 
le immagini sono state acquisite con magnete a 1 , 5 tesla ( gyroscan intera , philips medical systems , best , olanda ) equipaggiato con sistema di gradienti dinamici master ( ampiezza massima 30 mt ; slew rate 150 mt / m / ms ) e bobina di superficie dedicata a 5 elementi con tecnica sense . il protocollo desame risulta composto da un preliminare studio cine - rm ridotto a due soli piani di scansione asse corto bi - ventricolare ed un successivo piano asse lungo 4camere con tecnica turbo field echo ( tfe ) true fast imaging with steady state precession ( fisp ) steady - state free - precession ( ssfp ) con trigger elettrocardiografico retrospettivo in apnea inspiratoria , con i seguenti parametri di scansione : tempo di ripetizione ( tr ) 3 , 8 ms ; tempo di eco ( te ) 1 , 8 ms ; flip angle ( fa ) 70 ; matrice di acquisizione 256256 ; field of view ( fov ) 400 ; spessore di strato 10 mm ; gap 0 ; fattore di accelerazione sense 2.00 ; fasi cardiache / ciclo 20 ; sincronizzazione retrospettiva ; 2 slice ad apnea ; durata apnea 1518 secondi . 
successivamente sono state eseguite scansioni bb t2 pesate a soppressione del grasso ( stir ) con tse con trigger elettrocardiografico prospettico , attraverso le quali stato possibile identificare e localizzare ledema miocardio reattivo . 
tali scansioni vengono eseguite rispettivamente secondo asse corto biventricolare ( 6 slice ) ed asse lungo 2 o 4 camere ( 3 slice ) in relazione alla localizzazione dellarea ischemica , con i seguenti parametri di scansione : tr 1333 ms ; te 100 ms ; fattore epi 1 ; fattore turbo 33 ; matrice di acquisizione 512512 ; fov 350 ; spessore di strato 8 mm ; gap 0 , 8 ; fattore di accelerazione sense 1 , 00 ; fase diastolica ; slice ad apnea 1 ; durata apnea : 1518 secondi . 
successivamente al preliminare studio basale viene somministrato un bolo di mezzo di contrasto paramagnetico pari a 0 , 2 mmoli di gadobenato dimeglumina ( gd - dtpa ) per kg di peso corporeo . 
dopo un intervallo di tempo di 1015 minuti vengono eseguite scansioni inversion recovery ( ir ) 3d tfe t1 pesate per la valutazione del delayed enhancement , ecg - sincronizzate retrospettivamente in fase telediastolica e orientate secondo gli stessi piani delle sequenze cine - rm con i seguenti parametri : tr 4 , 6 ms ; te 1 , 4 ms ; fa 15 ; matrice di acquisizione 256256 ; fov 400 ; spessore di strato 14 mm ; gap 7 mm ; fattore di accelerazione sense 2 , 00 ; tempo di inversione ( ti ) 260310 ms ; durata : 16 secondi . 
 elaborazione dei dati lelaborazione dei dati stata eseguita rispettivamente da radiol med ( 2011 ) 116 : 163177 statistical analysis all the quantitative results [ end - diastolic volume ( edv ) , end - systolic volume ( esv ) and ejection fraction ( ef ) ] were expressed as meanstandard deviation . 
we calculated sensitivity , specificity , diagnostic accuracy , negative predictive value ( npv ) and positive predictive value ( ppv ) of t2 hyperintensity , delayed enhancement and decreased systolic wall thickening , respectively , in identifying areas of acute myocardial infarction and of decreased diastolic wall thickness in identifying myocardial scar . 
results of the latter analysis were expressed as percentages , and sensitivity and specificity values were compared using the mcnemar test . a value of p < 0.05 was considered statistically significant . results mr examination was well tolerated by all patients , and no complications were observed . 
in the 22 patients examined , a total of 374 segments were evaluated , 31 of which ( 8.2% ) showed full - thickness signal hyperintensity in the t2 - weighted sequences . 
twelve patients ( 50% ) showed evidence of myocardial scar from a known previous infarction , which were depicted as areas of delayed enhancement in the viability assessment , for a total of 26 segments ( 6.9% of the total )  . 
contractile abnormalities were identified in 56 segments ( 14.9% ) , of which 28 ( 50% ) were due to acute myocardial ischaemia , 26 ( 46.4% ) to scar from previous infarction and two ( 3.6% ) to left bundle branch block . 
finally , in only 14 ( 53.8% ) of the 26 segments with myocardial scar due to previous infarction was the end - diastolic wall thickness decreased , whereas all healthy segments and those affected by acute myocardial ischaemia showed preserved end - diastolic thickness . 
in all patients , the plaque responsible for the current ischaemic event was identified on the basis of the extent of coronary stenosis or the correspondence between the site of significant stenosis at ca and the electrocardiographic changes ( table 1 )  . 
a comparison between echocardiography performed on admission and subsequent mr imaging demonstrated almost identical results for the function indices , even though the mr study enabled a more analytical and precise assessment of function . 
moreover , mr imaging allowed for a better assessment of ventricular segmental kinetics , especially as regards segments that are difficult to explore with transthoracic un cardiologo ed un radiologo , indipendentemente a doppio cieco . 
stata inoltre condotta la misurazione degli indici di funzionalit globale del ventricolo sinistro e lanalisi qualitativa e quantitativa dello spessore parietale telediastolico , dellispessimento parietale durante la sistole e della motilit parietale , con lo scopo di identificare i segmenti con anomalie contrattili . 
 analisi statistica tutti i risultati quantitativi ( volume telediastolico [ vtd ] , volume telesistolico [ vts ] e frazione di eiezione [ fe ] ) sono stati espressi con valore mediodeviazione standard . 
sono stati calcolati i valori di sensibilit , specificit , accuratezza diagnostica , valore predittivo negativo ( vpn ) e positivo ( vpp ) rispettivamente per liperintensit nelle immagini t2 pesate , il delayed enhancement e la riduzione dellispessimento parietale sistolico nellidentificazione delle aree di infarto miocardico acuto e per il ridotto spessore diastolico nellidentificazione degli esiti di pregresso infarto . 
nei 22 pazienti sottoposti allo studio sono stati valutati un totale di 374 segmenti , di cui 31 ( 8 , 2% ) hanno mostrato iperintensit del segnale a tutto spessore nelle sequenze t2 pesate . 
in un solo paziente ( 4 , 1% ) non stata identificata alcuna area di iperintensit di segnale . in 12 pazienti ( 50% ) sono stati riscontrati esiti di pregresso evento infartuale , noto in anamnesi , visualizzati con aree di iperenhancement tardivo nello studio di vitalit , per un totale di 26 segmenti ( 6 , 9% del totale )  . 
sono state riscontrate anomalie contrattili in 56 segmenti ( 14 , 9% ) , di cui 28 ( 50% ) per lischemia miocardica acuta , 26 ( 46 , 4% ) per esiti di pregressi eventi infartuali e 2 ( 3 , 6% ) per blocco di branca sinistra . 
infine , solo in 14 ( 53 , 8% ) dei 26 segmenti con esiti di pregresso evento infartuale lo spessore parietale telediastolico risultato essere ridotto rispetto alla norma , mentre tutti i segmenti sani o interessati da ischemia miocardica acuta hanno mostrato spessore telediastolico conservato . 
of segments affected segments site of culprit lesion table 1 tabella 1 apical septal middle inferior septal basal inferior apical anterior basal anterior apical lateral basal anterior lateral middle anterior lateral middle inferior lateral apicale settale medio infero - settale basale inferiore apicale anteriore basale anteriore apicale laterale basale antero - laterale medio antero - laterale medio infero - laterale radiol med ( 2011 ) 116 : 163177 proximal third of right coronary middle third of right coronary middle third of right coronary distal third of left anterior descending middle third of left anterior descending middle third of left anterior descending distal third of left circumflex middle third of left circumflex middle third of left circumflex iii prossimale coronaria destra iii medio coronaria destra iii medio coronaria destra iii distale discendente anteriore iii medio discendente anteriore iii medio discendente anteriore iii distale ramo circonflesso arteria coronaria sinistra iii medio ramo circonflesso arteria coronaria sinistra iii medio ramo circonflesso arteria coronaria sinistra numero segmenti segmenti interessati sede placche culprit lesion echocardiography . 
in the detection of myocardial scar due to previous infarction , decreased diastolic wall thickness had a sensitivity and specificity of 53.8% and 100% , respectively , with a ppv of 100% , npv of 96.6% and an overall diagnostic accuracy of 96.7%. 
 discussion acs represents a major diagnostic challenge due to its incidence and high rate of associated mortality and morbidity . more specifically , nstemi infarction is a clinical entity of intermediate severity among the various presentations of acs and one in which the treatment strategy to be adopted is not always clear . 
the use of mr imaging in patients with dellattuale evento ischemico in tutti i pazienti stata identificata sulla base della significativit della stenosi coronarica o della corrispondenza fra la localizzazione della stenosi significativa alla coronarografia e delle alterazioni elettrocardiografiche ( tabella 1 )  . 
lanalisi della funzionalit globale del ventricolo sinistro nei pazienti esaminati ha mostrato un vtd medio di 151 , 232 , 4 ml , un vts medio di 87 , 522 , 4 ml e una fe media di 49 , 367 , 8% . 
un rapido confronto tra il preliminare esame ecocardiografico , eseguito allaccettazione del paziente , ed il successivo studio rm ha documentato una pressocch sovrapposizione dei dati relativi agli indici di funzionalit tra le due metodiche seppur lo studio rm ha permesso una valutazione pi analitica e precisa del quadro funzionale . 
liperintensit nelle immagini t2 pesate , il delayed enhancement e la riduzione dellispessimento parietale sistolico nellidentificazione delle aree di infarto miocardico acuto hanno presentato rispettivamente una sensibilit 96 , 8% , 45 , 8% e 87 , 5% , una dpecificit di 100% , 96 , 9% e 91 , 8% con un vpp di 100% , 68 , 7% e 50% e vpn di 99 , 7% , 92 , 3% e 98 , 7% ed infine unaccuratezza diagnostica complessiva di 99 , 7% , 90 , 3% e 91 , 4% . sono state identificate differenze statisticamente significative fra i valori di sensibilit , valore prognostico positivo e accuratezza diagnostica fra liperintensit del segnale nelle sequenze t2 pesate e le altre due variabili analizzate , radiol med ( 2011 ) 116 : 163177 acs has already been proposed and recognised by the major cardiological and cardioradiological associations as a highly appropriate examination for assessing the extent of necrotic injury due to infarction in the subacute phases of acs and for planning revascularisation procedures , above all in cases in which spect and dobutamine echocardiography have produced equivocal results [ 19 ]  . 
 infarction the results of our study , in agreement with the international literature , showed t2 signal hyperintensity to be an excellent indicator of the presence of acute myocardial ischaemia in patients with nstemi infarction . 
numerous experimental studies have not only documented that myocardial is associated with myocardial oedema , but also clarified that the extent of intramyocardial water accumulation is linearly correlated with signal intensity in t2 - weighted sequences [ 2124 ]  . 
the likely mechanisms leading to increased water content in the myocardial tissue are hyperaemia caused by inflammation resulting from ischaemia , associated with cellular swelling due to changes in cell membranes [ 23 ]  . 
 the correlation of t2 signal hyperintensity with interstitial oedema is also consistent with the observation that the spatial extent of myocardial oedema is usually greater than that of the irreversible myocardial injury ; in fact , the areas showing t2 hyperintensity in the acute phase may subsequently undergo functional recovery , suggesting a mismatch between myocardial oedema and necrosis , which probably indicates myocardium at risk [ 22 , 25 , 26 ]  . numerous clinical studies have demonstrated that delayed enhancement is present in both acute and chronic infarction as a result of the increased volume of distribution of gadolinium chelates due to expansion of the extracellular space in the affected areas : whereas delayed enhancement in acute infarction is related to disruption of cardiac cell membranes with communication between the intraand extracellular space , in chronic infarction , expansion of the extracellular space is due to deposition of collagen matrix in the absence of oedema [ 2729 ]  . 
suggest its persistence for approximately 28 days after coronary occlusion with complete resolution within 36 months , krauss et al . described its persistence over 7 months after an anterior infarction . 
the discrepancy is probably related to the presence or absence of reperfusion in the ischaemic region , which influences the extent and resorption of the interstitial oedema [ 30 , 32 ]  . 
furthermore , the oedema - related t2 cos come fra i valori di specificit solo rispetto allispessimento parietale sistolico e i valori predittivi negativi solo rispetto alliperenhancement tardivo ( p < 0 , 05 )  . 
il ridotto spessore diastolico nellidentificazione degli esiti di pregresso infarto ha invece mostrato una sensibilit e una specificit rispettivamente di 53 , 8% e 100% , con un vpp e un vpn rispettivamente di 100% e 96 , 6% e unaccuratezza diagnostica complessiva di 96 , 7% . 
 discussione la sindrome coronarica acuta ( sca ) rappresenta una sfida di particolare rilievo in ambito cardiologico per lincidenza con cui si manifesta e soprattutto per lelevata percentuale di mortalit e morbidit a cui si accompagna . 
lutilizzo della rm nei pazienti con sca stato gi proposto e riconosciuto dalle pi importanti associazioni di cardiologia e cardioradiologia come esame con elevato grado di appropriatezza nella valutazione dellestensione del danno necrotico infartuale nelle fasi sub - acute della sindrome coronarica acuta , per la programmazione di eventuali interventi di rivascolarizzazione , soprattutto nei casi in cui spect ed eco - stress con dobutamina abbiano conseguito risultati dubbi [ 19 ]  . 
 i dati del nostro studio , in accordo con i dati della letteratura internazionale , hanno mostrato come liperintensit del segnale nelle sequenze t2 pesate sia un ottimo indicatore della presenza di ischemia miocardica acuta nei pazienti con infarto nstemi . 
numerosi studi sperimentali non solo hanno documentato come linfarto miocardico acuto sia associato ad edema miocardico , ma hanno anche chiarito che lentit dellaccumulo intramiocardico di liquidi correli linearmente con lintensit del segnale nelle sequenze t2 pesate [ 2124 ]  . 
verosimilmente i meccanismi che determinano laumento del contenuto idrico del tessuto miocardico sono costituiti dalliperemia indotta dallinfiammazione associata allischemia , in associazione al rigonfiamento cellulare indotto dallalterazione delle membrane cellulari [ 23 ]  . la correlazione delliperintensit del segnale nelle sequenze t2 pesate con ledema interstiziale concorda anche con losservazione che lestensione spaziale delledema miocardico solitamente molto pi ampia dellestensione del danno miocardico irreversibile ; infatti le aree con elevato segnale nelle sequenze t2 pesate nelle fasi acute , possono successivamente andare incontro a recupero funzionale , suggerendo lesistenza di un mismatch fra ledema miocardico e la necrosi che indica probabilmente il miocardio a rischio [ 22 , 25 , 26 ]  . numerosi studi clinici hanno dimostrato come liperenhancement tardivo sia presente nellinfarto miocardico sia acuto che cronico in relazione sostanzialmente allaumento del volume di distribuzione dei chelati del gadolinio 170 radiol med ( 2011 ) 116 : 163177 fig . 
1a - f t2 - weighted black - blood turbo spin echo spectral presaturation inversion recovery images in the biventricular short - axis plane ( a , b )  . 
the most important of these is collagen deposition , a dynamic process that occurs within days of the acute event and continues over the following years : because t2 relaxation time is inversely related to collagen content in muscle , the signal will be significantly lower in mature fibrous tissue [ 32 , 33 ]  . 
the better results can probably be explained in part by the different acquisition paraper lespansione dello spazio extracellulare in tali aree : mentre nellinfarto acuto liper - enhancement tardivo determinato dalla perdita di integrit delle membrane dei miocardiociti edematosi con linstaurarsi di comunicazioni fra lambiente intra ed extra - cellulare , nellinfarto cronico lespansione dello spazio extracellulare derivato dalla deposizione di matrice collagene in assenza di edema [ 2729 ]  . 
in reality , the specificity and ppv were heavily influenced by the low prevalence of disease per segment ( only 32 diseased segments out of a total 374 ) and by patient selection and were both overestimated . 
la discrepanza fra i risultati probabilmente legata alla presenza o meno di riperfusione dellarea ischemica che influenza lentit delledema interstiziale ed il suo riassorbimento [ 30 , 32 ]  . 
inoltre , liperintensit edema - correlata nelle sequenze t2 pesate sensibile ad altri processi che insorgono nella fase di organizzazione dellinfarto , che possono contribuire alla normalizzazione del segnale nel periodo successivo allinfarto , primo fra tutti la deposizione di collagene che un processo dinamico attivo gi pochi giorni dopo levento acuto e persistente negli anni successivi : il tempo di rilassamento t2 inversamente proporzionale alla quota di collagene nel tessuto muscolare , pertanto il segnale risulter significativamente pi basso nel tessuto fibroso maturo [ 32 , 33 ]  . 
the finding of oedema in the t2weighted sequences without delayed enhancement in the viability assessment in some patients with nstemi infarction may be explained by the fact that in the presence of elevated troponin values , the injury does not always cause irreversible segmental or macroscopic subsegmental changes . 
nella nostra casistica con lutilizzo di questa sequenza solamente in un paziente non stato possibile identificare larea di edema miocardico , tuttavia il controllo coronarografico in questo caso ha documentato la presenza di una placca significativa determinante stenosi del lume vasale del 70% a carico del secondo tratto della circonflessa non dominante , con lieve rialzo della sola troponina ed ecg non dirimente per la presenza di alterazioni pre - esistenti del tracciato . 
in realt la specificit ed il vpp sono stati fortemente influenzati dalla bassa prevalenza della patologia per segmento ( solo 32 segmenti colpiti su 374 totali ) e dalla selezione dei pazienti , risultando entrambi sovrastimati . 
di fatto in questi casi , nonostante i risultati di ecg e dosaggio enzimatico siano indicativi di infarto nstemi , i risultati clinici di apparente reversibilit e le caratteristiche miocardiche rilevate dalla rm sarebbero pi affini alle caratteristiche della ua . 
in reality , these values , as with those pertaining to the other myocardial parameters evaluated in our study , were overestimated , particularly as regards specificity and npv , opportuno validare questa ipotesi con controlli rm a distanza di tempo per verificare leffettiva reversibilit del deficit contrattile e la mancata comparsa di delayed enhancement anche nelle fasi croniche . 
se ci fosse dimostrato , si dovrebbe ulteriormente distinguere due categorie di infarti nstemi verosimilmente con due differenti valori prognostici ed indirizzi terapeutici . risultati pi soddisfacenti sono stati ottenuti dallidentificazione del deficit contrattile nelle sequenze cine - rm con sensibilit e specificit rispettivamente di 87 , 5% e 91 , 8% . in realt questi valori , cos come quelli delle altre caratteristiche del miocardio valutate nel nostro studio , risultano sovrastimati , soprattutto riguardo alla specificit ed al valore predittivo negativo , in relazione alla bassa prevalenza segmentaria delle anomalie identificate . 
in questo caso , infatti , il deficit contrattile , identificato nei 26 segmenti con esiti di pregresso infarto del miocardio e nei 2 segmenti settali per la presenza di blocco di branca , radiol med ( 2011 ) 116 : 163177 fig . 
5 a - f immagini su piano asse corto biventricolare ( a , b , f ) e asse lungo quattro camere ( c , d , e ) di sequenza cine - rm balanced - tfe . as a result of the low segmental prevalence of the abnormalities identified . 
in this case , the contractile defect identified in 26 segments with myocardial scar due to previous infarction and in two septal segments due to bundle branch block was a false positive that lead to a specificity of 91.8% in that it compared with 314 segments correctly diagnosed as having normal contractility . 
by contrast , the 50% ppv in identifying segments affected by nstemi infarction is influenced by the low specificity of contractile defects , as both the true positive and false positive segments amounted to 28 . 
 decreased end - diastolic wall thickness , despite having rappresenta un falso positivo che per determina una specificit del 91 , 8% perch contrapposto a 314 segmenti correttamente diagnosticati come normo - contrattili . 
il valore prognostico positivo del 50% nella identificazione dei segmenti colpiti da infarto nstemi risente invece della bassa specificit del deficit contrattile , poich sia i segmenti veri positivi che i falsi positivi sono risultati entrambi 28 . questo significa che il riscontro di un deficit contrattile solo in un paziente su due corrisponde ad unarea ischemica acuta . 
 la riduzione dello spessore parietale telediastolico , sebbene consenta di escludere con elevata accuratezza lischemia acuta , risulta altamente specifico , ma molto poco sensibile nella identificazione dellinfarto cronico con valori rispettivamente di 100% e 53 , 8% , visto che un ridotto radiol med ( 2011 ) 116 : 163177 fig . 
this is explained by the fact that a necrosis involving only a small number of subendocardial myocardial fibres does not necessarily lead to significant myocardial thinning , making this parameter heavily influenced by the intrasegmental extent of the injury . in conclusion , on the basis of data reported in the literature and our preliminary results , we can state that the combination of t2 bb - stir - tse and t1 tfe - ir sequences after administration of contrast material allows precise localisation and differentiation of acute and chronic ischaemic areas . 
although recent reports in the literature have described promising results being achieved with cardiac multidetector computed tomography ( mdct ) in evaluating delayed enhancement [ 35 ] , this option cannot yet be considered satisfactory , especially in view of the radiation dose delivered to patients , which is still definitely too high in relation to the diagnostic information obtained . 
at the same time , it should be noted that to date , mdct is the only noninvasive modality capable of locating the culprit spessore parietale stato riscontrato solo in 14 dei 26 segmenti con esiti infartuali : la spiegazione a questi dati fornita dal fatto che , se la necrosi ha interessato solamente una piccola quota di fibre miocardiche subendocardiche , non necessariamente lo spessore miocardico subisce una significativa riduzione , quindi evidente come questo parametro sia fortemente condizionato dallestensione intrasegmentaria del danno . 
venturi1 1uoc nint neuroimmagini e neurointerventistica , dipartimento di neuroscienze , azienda ospedaliera universitaria senese , policlinico santa maria alle scotte , viale mario bracci , 16 , 53100 siena , italy 2dipartimento di patologia umana ed oncologica , sezione di radiologia universitaria , universit di siena , policlinico santa maria alle scotte , viale mario bracci 16 , 53100 siena , italy 3uoc neurologia malattie neurometaboliche , dipartimento di scienze neurologiche , neurochirurgiche e del comportamento , universit di siena , policlinico santa maria alle scotte , viale mario bracci 16 , 53100 siena , italy 4uoc rianimazione generale , dipartimento di terapia intensiva e anestesia , azienda ospedaliera universitaria senese , policlinico santa maria alle scotte , viale mario bracci 16 , 53100 siena , italy 5dipartimento di neuroscienze , sezione di neurologia , universit di siena , policlinico santa maria alle scotte , viale mario bracci 16 , 53100 siena , italy correspondence to : a . 
the dorsal medulla , red nuclei , cranial nerve nuclei , cerebellum , corpus callosum , frontal and parietal cerebral cortex are less common sites of involvement although they are more frequently affected in nonalcoholic patients . 
paramagnetic contrast material may help to identify lesions not otherwise visible . keywords wernickes encephalopathy computed tomography magnetic resonance riassunto lo scopo di questa rassegna iconogra ca presentare i possibili reperti alla tomogra a computerizzata ( tc ) e alla risonanza magnetica ( rm ) dellencefalopatia di wernicke , una rara grave sindrome neurologica acuta da de cit di tiamina ( vitamina b1 ) , con elevate morbilit e mortalit . 
sedi meno tipiche di interessamento , e pi frequentemente coinvolte nei pazienti non - etilisti , sono la porzione dorsale del bulbo , il nucleo rosso e i nuclei dei nervi cranici , il cervelletto , il corpo calloso e la corteccia fronto - parietale . 
il mezzo di contrasto paramagnetico pu mostrare la presenza di lesioni non altrimenti evidenti . parole chiave encefalopatia di wernicke tomogra a computerizzata risonanza magnetica 320 introduction wernickes encephalopathy is a rare but severe neurological disorder de ned in its various forms by several authors and in particular by karl wernicke in the second half of the nineteenth century [ 15 ]  . 
the classical form is characterised by sudden onset of the clinical triad of eye disorders ( ophthalmoparesis ) , ataxia and cognitive impairment , but the clinical presentation varies widely to the point that it can delay diagnosis and signi cantly worsen the prognosis . 
in the most severe cases , particularly in patients with late diagnosis , there may be progression to persistent severe neurological and psychiatric de ciencies , if not coma and death . 
the study of the brain with computed tomography ( ct ) and especially magnetic resonance imaging ( mri ) plays an essential role in guiding the diagnosis and ruling out other diseases , even though the ndings may be equivocal [ 1034 ]  . 
the purpose of this pictorial essay is to present the ct and mri ndings of wernickes encephalopathy and discuss them in the light of pathogenicity and clinical history . epidemiology wernickes encephalopathy is de nitely more frequent in chronic alcoholics , but it has also been reported to complicate various other conditions , such as uraemia , hyperemesis gravidarum , anorexia nervosa , protracted infectious or febrile conditions , aids , malignancies , dialysis , chronic gastrointestinal disorders , parenteral nutrition or protracted infusional treatment with a glucose solution for instance , following abdominal surgery [ 49 ]  . 
the condition has no racial predilection ; the male sex is the most commonly affected ( m : f ratio = 1.7 : 1 ) , most likely because alcoholism is three to four times more frequent among men than women . 
 aetiopathogenesis the mechanism underlying the development of encephalopradiol med ( 2011 ) 116 : 319333 introduzione lencefalopatia di wernicke una rara ma grave sindrome neurologica de nita nelle sue varie forme cliniche da vari autori , e soprattutto da karl wernicke , nella seconda met del xix secolo [ 15 ]  . 
la malattia consegue a de cit di tiamina ( vitamina b1 ) e colpisce pi frequentemente i soggetti etilisti cronici , anche se pu complicare molte condizioni di malnutrizione in soggetti non - etilisti . 
la forma classica si caratterizza per la comparsa improvvisa della triade clinica costituita da disturbi oculari ( oftalmoparesi ) , atassia e disturbi cognitivi , ma la presentazione clinica estremamente variabile , tale da poterne ritardare la diagnosi e determinarne un notevole peggioramento della prognosi . 
nei casi pi gravi , infatti , ed in particolare nei pazienti con diagnosi tardiva , possibile la progressione verso il coma e la morte o comunque la persistenza di gravi de cit neurologici e psichiatrici . 
il sospetto clinico , la diagnosi precoce e la relativa tempestiva terapia integrativa con tiamina possono consentire , invece , la regressione del danno neurologico e migliorare fortemente la prognosi [ 69 ]  . 
lo studio dellencefalo mediante tomogra a computerizzata ( tc ) e , soprattutto , risonanza magnetica ( rm ) riveste un ruolo fondamentale nellorientamento diagnostico e nellesclusione di altra patologia , seppure i reperti possano non essere univoci [ 1034 ]  . 
lo scopo di questa rassegna iconogra ca presentare i possibili reperti tc e rm dellencefalopatia di wernicke e discuterli alla luce di patogenesi e storia clinica . epidemiologia lencefalopatia di wernicke certamente pi frequente negli etilisti cronici , ma stata descritta come complicanza di molte altre condizioni quali uremia , iperemesi gravidica , anoressia nervosa , condizioni infettive o febbrili protratte , sindrome da immunode cienza umana acquisita ( aids ) , tumori maligni , dialisi , patologie gastrointestinali croniche , nutrizione parenterale o terapia infusionale prolungata con soluzione glucosata come ad esempio nei soggetti sottoposti a chirurgia addominale [ 49 ]  . 
studi autoptici hanno dimostrato lesioni tipiche di encefalopatia di wernicke nello 0 , 8%2 , 8% della popolazione generale ; la frequenza pu arrivare al 12 , 5% nelle popolazioni di etilisti cronici . 
la condizione non ha predilezione razziale ; il sesso maschile pi colpito ( rapporto m : f = 1 , 7 : 1 ) , molto probabilmente poich lalcolismo 34 volte pi frequente negli uomini che nelle donne . 
 radiol med ( 2011 ) 116 : 319333 athy has not been completely elucidated , but it is thought to be dependent on alteration of the metabolism of glial cells and neurons due to the absence of thiamine , a water - soluble vitamin needed to convert glucose into energy . 
in particular , thiamine acts as a cofactor for various enzymes ( transketolase , pyruvate dehydrogenase , ketoglutarate dehydrogenase ) of carbohydrate metabolism and is usually stored in the liver . 
hence , it may be induced by a de cient diet ( typical of populations who mainly eat white rice without the outer husk , i.e. , the part containing most thiamine ) or by alcohol intoxication ( mostly in chronic alcoholics , because alcohol reduces thiamine absorption )  . 
thiamine de ciency causes beriberi ( from the term beri , which in the sinhalese language indicates debilitation ) , a disease causing damage to the nervous system , which then extends to the cardiovascular and gastrointestinal system , even though the most evident symptoms affect one of these systems only . 
 the response to thiamine de ciency tends to be populationspeci c , as asians tend to develop cardiovascular ( or wet ) beriberi , whereas europeans develop neurological ( or dry ) beriberi and wernickes encephalopathy . in the absence of thiamine , the cycles of krebs and of pentose phosphates cannot metabolise glucose , resulting in intracellular accumulation of glutamate , which is subsequently released into the extracellular spaces following homeostatic imbalance and excitotoxic damage [ 23 ]  . 
excess extracellular glutamate may bind to either n - methyl - daspartate ( nmda ) receptors , allowing entry of calcium ( ca2 + ) ions into the cells , with resulting cell injury and death due to necrosis or apoptosis ; or to non - nmda receptors , allowing entry of sodium ( na + ) , with resulting cell injury and death due to cellular oedema ( direct cytotoxic damage )  . 
 the fact that wernickes encephalopathy develops in a few chronic or malnourished alcoholics only has led investigators to hypothesise a genetic predisposition related to variants of the enzymes involved , such as transketolase , but this has not yet been conclusively demonstrated [ 35 ]  . pathology in wernickes encephalopathy the damage occurs more eziopatogenesi il meccanismo attraverso cui si instaura lencefalopatia non stato ancora del tutto chiarito , ma generalmente si ritiene che dipenda dallalterazione del metabolismo energetico delle cellule gliali e dei neuroni indotta dallassenza di tiamina , una vitamina idrosolubile necessaria alla conversione del glucosio in energia . 
in particolare , la tiamina funziona da cofattore per vari enzimi ( transchetolasi , piruvato deidrogenasi , chetoglutarato deidrogenasi ) del metabolismo dei carboidrati e normalmente viene accumulato nel fegato . 
 essa , quindi , pu essere determinata da una dieta carente ( diffusa in popolazioni che si nutrono prevalentemente di riso senza la cuticola , che la parte contiene la maggior parte della tiamina ) , o a unintossicazione da alcool ( per lo pi presente in alcolisti cronici , poich lalcool diminuisce lassorbimento di tiamina ) , ma anche da situazioni particolari , come ipertiroidismo , gravidanza , allattamento o febbre , che portano a una richiesta maggiore di tiamina . 
 la carenza di tiamina provoca beriberi ( dal termine beri della lingua senegalese che indica debilitazione ) , una malattia con danni al sistema nervoso che poi si estendono al sistema cardiovascolare e gastrointestinale , ma i sintomi pi evidenti riguardano uno solo dei sistemi . 
la risposta alla carenza di tiamina tende ad essere popolazione - specica , in quanto gli asiatici tendono a sviluppare soprattutto un beriberi cardiovascolare ( o umido ) , mentre gli europei sviluppano un beriberi neurologico ( o secco ) e lencefalopatia di wernicke . in assenza di tiamina , il ciclo di krebs e dei pentosofosfati non possono metabolizzare il glucosio , con conseguente accumulo intracellulare di glutammato che viene poi rilasciato negli spazi extracellulari per perdita dellomeostasi cellulare e danno citotossico [ 23 ]  . 
leccessivo glutammato extracellulare pu legarsi ai recettori delln - metild - aspartato ( nmda ) , consentendo lingresso di ioni ca2 + nelle cellule che quindi vanno incontro a sofferenza e morte per necrosi o apoptosi , o ai recettori non - nmda , consentendo lingresso intracellulare di na + con conseguente sofferenza e morte da edema cellulare ( danno propriamente citotossico )  . 
involvement of these less typical regions is more frequent in nonalcoholics and is associated in most cases with involvement of the more typical sites [ 32 , 33 ]  . 
1a , b acute wernickes encephalopathy in a nonalcoholic man : serial nonconsecutive iodineenhanced axial computed tomography ( ct ) images obtained at clinical presentation ( a ) , and unenhanced ct images obtained 6 days later ( b )  . 
six days later , they show hypoattenuation in both the mamillary bodies ( arrowhead ) , periaqueductal region ( white arrow ) and both medial thalami ( black arrows ) fig . 
1a , b encefalopatia di wernicke acuta in uomo non - etilista cronico : immagini tc assiali seriali non consecutive dopo iniezione ev di mdc iodato alla presentazione clinica ( a ) e nelle condizioni di base dopo sei giorni ( b )  . 
sei giorni dopo , dimostra ipodensit di entrambi i corpi mammillari ( punta di freccia ) , della regione periacqueduttale ( freccia bianca ) e di entrambi i talami mediali ( frecce nere )  . radiol med ( 2011 ) 116 : 319333 fig . 
2a - e acute wernickes encephalopathy in a nonalcoholic woman : serial nonconsecutive axial ct images ( a ) , and coronal dw ( b ) , adc ( c ) ( b : 1 , 000 s / mm2 ) , axial flair ( d ) and serial nonconsecutive gadolinium - enhanced t1 - weighted ( e ) mri . 
despite negative or doubtful ct images , on flair and gadolinium - enhanced t1 - weighted images , there is slight signal hyperintensity and partial contrast enhancement in both the medial thalami ( black arrows ) , and after i.v. 
2a - e encefalopatia di wernicke acuta in donna non - etilista cronica : immagini tc assiali seriali non consecutive ( a ) e rm coronali dwi ( b ) e adc ( c ) ( b : 1000 s / mm2 ) , assiali flair ( d ) e t1 dipendenti dopo iniezione ev di mdc paramagnetico ( e ) seriali non consecutive . 
a fronte di immagini tc negative o dubbie , alla rm si nota tenue iperintensit di segnale nelle immagini flair e parziale impregnazione dopo mdc dei talami mediali bilateralmente ( frecce nere ) e pi marcata iperintensit , con parziale impregnazione dopo iniezione ev di mdc paramagnetico della corteccia frontale e parietale bilateralmente ( punte di freccia nere )  . 
la regione periacqueduttale ( punta di freccia bianca ) ed i corpi mammillari ( punta di freccia vuota ) presentano solo impregnazione dopo somministrazione di mdc , in assenza di alterazioni dellintensit di segnale . 
the cranial nerve nuclei , on the other hand , would be typically affected in nonalcoholic patients : some authors have even suggested that alcohol protects those regions [ 32 ]  . 
linteressamento dei nuclei dei nervi cranici , invece , sarebbe caratteristico dei pazienti non - etilisti , tanto che alcuni autori ipotizzano un effetto protettivo dellalcol nei confronti di tali regioni [ 32 ]  . 
in et pediatrica , possibile linteressamento della sostanza nera , dei nuclei dei nervi oculomotori , dei nuclei rossi , dei nuclei 324 radiol med ( 2011 ) 116 : 319333 fig . 
high signal intensity is observed in the dorsal medulla ( white arrow ) , facial nerve nuclei ( black arrows ) , periaqueductal grey matter ( white empty arrow ) and mamillary bodies ( black empty arrow ) fig . 
si nota iperintensit di segnale della porzione dorsale del bulbo ( freccia bianca ) delle aree dei nuclei dei nervi facciali ( frecce nere ) , della sostanza grigia periacqueduttale ( freccia vuota bianca ) e dei corpi mammillari ( freccia vuota nera )  . as a result of the high thiamine - dependent metabolism of the nuclear - basal regions in children [ 14 , 21 , 34 ]  . 
 histological ndings include demyelination , alterations of the bloodbrain barrier ( bbb ) with vasogenic oedema and petechial haemorrhage , astrocyte swelling and cellular necrosis in the mamillary bodies , thalamic and hypothalamic nuclei , periaqueductal gray matter , walls of the third and oor of the fourth ventricle and , less frequently , in the caudate nucleus and the frontal and parietal cortex [ 23 , 36 , 37 ]  . 
the progressive loss of neurons in these regions may be responsible for the atrophic alterations found in chronic alcoholics [ 36 ]  . dentati del cervelletto e , soprattutto , dei nuclei della base , ed in particolare del putamen , probabilmente determinato da un elevato metabolismo tiamina - dipendente delle regioni nucleo - basali in et pediatrica [ 14 , 21 , 34 ]  . i rilievi istologici includono demielinizzazione , alterazioni della barriera emato - encefalica con edema vasogenico ed emorragie petecchiali , rigon amento degli astrociti e necrosi cellulare nei corpi mammillari , nei nuclei del talamo e dellipotalamo , sostanza grigia periacqueduttale , pareti del terzo e pavimento del quarto ventricolo e , meno comunemente , nel nucleo caudato e nella corteccia frontale e parietale [ 23 , 36 , 37 ]  . 
la progressiva perdita di neuroni in tali regioni sarebbe responsabile delle alterazioni atro che riscontrate negli etilisti cronici [ 36 ]  . clinical presentation the classic clinical triad of wernickes encephalopathy consists of the abrupt appearance of eye disorders , ataxia and cognitive impairment [ 1 , 2 , 49 ]  . 
the most frequent ocular la triade clinica classica dellencefalopatia di wernicke costituita dalla comparsa improvvisa di disturbi oculari , presentazione clinica radiol med ( 2011 ) 116 : 319333 fig . 
4a - d acute wernickes encephalopathy in a nonalcoholic man : sagittal ( a ) and serial nonconsecutive axial ( b ) t2 - weighted and axial uid attenuated inversion recovery ( c ) and dw ( b : 2 , 500 s / mm2 ) ( d ) images . 
t2 - weighted images show high signal intensity in the dorsal upper medulla , in the area of vestibular nuclei ( short white arrows ) , periaqueductal region ( black arrows ) , both mamillary bodies ( empty arrowheads ) , paramedial nuclei of both thalami ( black arrowheads ) and bilateral frontal and parietal cortex in the central sulci ( long white arrows )  . 
mean adc values of the midbrain and lenticular nuclei , with normal signal intensity , were 0.5310 - 3 mm2 / s and 0.6310 - 3 mm2 / s , respectively . 
4a - d encefalopatia di wernicke acuta in uomo non - etilista cronico : immagini rm sagittale ( a ) e assiali ( b ) t2 - dipendenti seriali non consecutive e assiale flair ( c ) e dwi ( b : 2500 s / mm2 ) ( d )  . 
si nota iperintensit di segnale nelle immagini t2 - dipendenti nella porzione dorsale superiore del bulbo , nella regione dei nuclei vestibolari ( frecce bianche corte ) , della regione periacqueduttale ( frecce nere ) , di entrambi i corpi mammillari ( punta di freccia vuota ) , dei nuclei paramediali di entrambi i talami ( teste di freccia nere ) e della corteccia frontale e parietale in prossimit dei solchi centrali bilateralmente ( frecce bianche lunghe )  . 
i valori medi delladc del mesencefalo e dei nuclei lentiformi di intensit di segnale normali erano di 0 , 5310 - 3 mm2 / s e 0 , 6310 - 3 mm2 / s rispettivamente . 
le lesioni non presentavano impregnazione nelle immagini t1 - dipendenti dopo iniezione ev di mdc paramagnetico ( non mostrate )  . disorders are alterations in eye movements , nystagmus , diplopia and sluggish pupillary re ex ; less frequently there is decreased bilateral visual acuity leading to blindness . 
however , because the classic triad is seen in one third of patients only , it has been suggested that a suspicion of wernickes encephalopathy should be based on two of the following four conditions : malnutrition , oculomotor disorders , cerebellar disorders , altered mental state or even moderate memory defects [ 6 ]  . 
i disturbi oculari pi frequenti sono rappresentati da alterazioni dei movimenti oculari , nistagmo , diplopia , e rallentamento del ri esso pupillare , pi raramente diminuzione bilaterale del visus no alla cecit . 
la triade clinica classica , tuttavia , presente solo in un terzo dei malati , ed stato proposto di sospettare la encefalopatia di wernicke in presenza di due delle seguenti quattro condizioni : malnutrizione , disturbi delloculomozione , disfunzione cerebellare e alterazioni dello stato mentale o difetti mnesici anche moderati [ 6 ]  . 
la sensibilit e la speci cit di tali ultimi criteri , tuttavia , non ancora nota [ 33 ]  . la presentazione clinica , in particolare , estremamente variabile sia in et adulta che in et pediatrica [ 34 ]  . 
5a - d subacute wernickes encephalopathy in a nonalcoholic woman : serial nonconsecutive t2 - weighted ( a , b ) , unenhanced ( b ) and gadolinium - enhanced ( c ) t1 - weighted axial magnetic resonance images . 
t2 - weighted images show swelling and hyperintensity of the mamillary bodies ( empty arrowhead ) and slight signal abnormality of the medial thalami ( short white arrows )  . 
5a - d encefalopatia di wernicke subacuta in donna non - etilista cronica : immagini rm assiali seriali non consecutive t2 - dipendenti ( a , b ) , e t1 prima ( b ) e dopo ( c ) iniezione ev di mdc paramagnetico . 
nelle immagini t2dipendenti si notano tumefazione ed iperintensit di segnale dei corpi mammillari ( punta di freccia vuota ) e pi tenue alterazione di segnale dei talami mediali ( frecce bianche corte )  . 
nelle immagini t1 - dipendenti dopo mdc , si nota dubbia impregnazione dei collicoli inferiori ( frecce nere ) , specie di quello destro . sion , hypothermia , coma , gradual development over several days and without the presence of any element of the classic clinical triad , with bilateral blindness , dysphagia or signs typical of another disease , such as millerfishers syndrome . 
symptoms such as peripheral polyneuropathy ; olfactory discrimination de cits ; bilateral hypacusia ; vestibular paralysis ; cardiovascular signs such as tachycardia , dyspnoea on exertion , postural hypotension ; syncope , hypothermia as an indicator of involvement of the posterior hypothalamus ; but also epileptic seizures may be observed . 
 especially in the later stages of the disease , the appearance of hyperthermia as a sign of involvement of the anterior hypothalamus , pyramidal hemisyndromes ( babinski sign , hyperre exia , muscle hypertonia ) , choreic dyskinesia , and coma are common . 
in these individuals , diagnosis may be achieved before death in only 20% of patients , as the most common presentation is mental confusion without any further symppossibile , ad esempio , lesordio con ipotensione , ipotermia , coma , graduale evoluzione in vari giorni e senza la presenza di nessun elemento della triade clinica classica , con cecit bilaterale , con disfagia oppure con reperti tipici di altra patologia quale , ad esempio , la sindrome di miller - fisher . 
 sono da segnalare sintomi come la polineuropatia periferica , de cit della discriminazione olfattoria , ipoacusia bilaterale , paresi vestibolare , segni cardiovascolari quali tachicardia , dispnea da sforzo , ipotensione posturale , sincope , ipotermia quale indice di coinvolgimento delle regioni posteriori dellipotalamo , ma anche manifestazioni epilettiche . 
soprattutto nelle fasi pi avanzate di malattia , sono comuni la comparsa di ipertermia quale segno di coinvolgimento delle regioni anteriori dellipotalamo , emisindromi piramidali ( segno di babinski , iperre essia , ipertono muscolare ) , discinesie coreiche ed in ne coma . 
in questultima popolazione , infatti , possibile che la diagnosi sia raggiunta prima del decesso solo nel 20% degli affetti , poich lesordio pi frequente radiol med ( 2011 ) 116 : 319333 fig . 
6a - c acute wernickes encephalopathy in a nonalcoholic man : coronal , sagittal and axial uid attenuated inversion recovery ( flair ) ( a ) , axial and sagittal gadolinium - enhanced t1 - weighted ( b ) and late thin - section axial ( c ) magnetic resonance images . 
flair images show high signal intensity not only in typical sites ( periaqueductal area and inferior colliculi , medial thalami and mamillary bodies ) but also in the cerebellar vermis ( full arrowheads ) , dorsal medulla and midbrain ( black arrows ) , fornix ( white arrows ) and frontal - parietal cortex ( empty white arrowheads )  . 
gadolinium - enhanced images show enhancement of mamillary bodies ( black arrows ) and inferior colliculi ( empty black arrowheads ) , which becomes increasingly evident in the late thin - section sequences fig . 
6a - c encefalopatia di wernicke acuta in uomo non - etilista cronico : immagini rm coronale , sagittale e assiale flair ( a ) , assiale e sagittale t1 - dipendenti immediatamente dopo iniezione ev di mdc paramagnetico ( b ) e assiale t1 - dipendente a strato sottile ottenuta successivamente ( in fase tardiva ) ( c )  . 
 nelle immagini flair , oltre che nelle sedi tipiche ( regione periacqueduttale e collicoli inferiori , talami mediali e corpi mammillari ) , si nota iperintensit di segnale nel verme cerebellare ( punte di freccia piene ) , nella porzione dorsale del bulbo e del mesencefalo ( frecce nere ) , nel fornice ( frecce bianche ) e nella corteccia frontale e parietale ( punte di freccia vuote bianche )  . 
dopo somministrazione di mdc si nota impregnazione dei corpi mammillari ( frecce nere ) e dei collicoli inferiori ( punte di freccia vuote nere ) che diviene sempre meglio evidente nelle sequenze acquisite pi tardivamente e con strato sottile . toms [ 6 , 8 , 9 ]  . 
on the other hand , any condition that may mimic wernickes encephalopathy needs to be clinically excluded , especially in individuals at risk presenting with neurological symptoms , such as sleepiness and altered state of consciousness . 
in this situation , the differential diagnosis between pancreatic and wernickes encephalopathy is extremely dif cult , even though thiamine administration can prevent deterioration of the neurological state in individuals with the latter disease . 
daltra parte , clinicamente vanno escluse le condizioni che possono simulare lencefalopatia di wernicke , soprattutto nei soggetti a rischio che si presentino con sintomi neurologici quali la sonnolenza e lalterazione della coscienza . la diagnosi differenziale , quindi , comprende le metastasi ed i tumori cerebrali , le emorragie o lischemia dei tessuti nervosi intracranici , linsuf cienza epatica , la mielinolisi pontina centrale e le infezioni cerebrali . 
in tale condizione , infatti , la diagnosi differenziale tra encefalopatia pancreatica ed encefalopatia di wernicke estremamente dif cile , ma la somministrazione di tiamina pu evitare laggravamento dello stato neurologico nei malati con encefalopatia di wernicke . 
7a - f acute wernickes encephalopathy in an alcoholic man : t2 - weighted sagittal ( a ) , serial nonconsecutive flair ( b , c ) , dw ( d ) and adc ( e ) ( b : 1 , 000 s / mm2 ) axial magnetic resonance images ( mri ) obtained at clinical presentation , and axial flair ( f ) mri obtained 1 week later . 
at clinical presentation , there is high signal intensity on long tr images in the dorsal medulla , in the area of the vestibular nuclei ( full black arrowhead ) , periaqueductal grey matter and inferior colliculi ( white arrow ) and in both medial thalami ( black arrows ) , which show increased diffusion . 
note the atrophy and signal intensity abnormality of the mamillary bodies ( empty arrowheads ) , consistent with a history of chronic alcoholis prompt treatment with thiamine resulted in rapid ( within days ) clinical improvement . 
7a - f encefalopatia di wernicke acuta in uomo etilista cronico : immagini rm sagittale t2 - dipendente ( a ) , assiali seriali non consecutive flair ( b , c ) e dwi ( d ) e adc ( e ) ( b : 1000 s / mm2 ) alla presentazione clinica e assiali flair ( f ) una settimana dopo . 
alla presentazione clinica , si notano alterazione di segnale della porzione dorsale del bulbo nellarea dei nuclei vestibolari ( punta di freccia piena ) , della sostanza grigia peri - acqueduttale e dei collicoli inferiori ( freccia bianca ) e dei talami mediali ( frecce nere ) che presentano incremento della diffusione . 
il controllo rm condotto dopo una settimana dimostra signi cativa regressione dei reperti patologici . wernickes encephalopathy is more complicated , especially in individuals with chronic gastrointestinal diseases , such as crohns , being treated with metronidazole . 
the clinical manifestations of these conditions are very similar , whereas some sites of involvement considered characteristic of metronidazole - induced encephalopathy , such as cerebellar dentate nuclei , cranial nerve nuclei and splenium , may also be affected in wernickes encephalopathy , although they are not typical sites . 
it has been suggested that the neurological damage in these patients is due to both thiamine de ciency and metronidazole neurotoxicity and that the latter may be mediated by mechanisms similar to those responsible for wernickes encephalopathy [ 32 ]  . 
in the most advanced stages of disease , patients may lose their ability to learn new information ( anterograde amnesia ) , lling in the gaps with their past memories without realising their problem , progressing to full - blown psychosis or wernicke korsakoffs syndrome [ 3 , 7 ]  . 
 ziale tra encefalopatia da metronidazolo ed encefalopatia di wernicke , in particolare in soggetti con patologie gastrointestinali croniche , come il morbo di crohn , in trattamento proprio con metronidazolo . 
le manifestazioni cliniche di tali condizioni risultano infatti sostanzialmente sovrapponibili , mentre alcune sedi di lesione considerate caratteristiche della encefalopatia da metronidazolo , quali nuclei dentati del cervelletto , nuclei dei nervi craniali e splenio del corpo calloso , possono essere coinvolte anche nellencefalopatia di wernicke , sebbene non ne rappresentino le sedi tipiche . 
stato ipotizzato che in tali pazienti possa essere presente un danno neurologico conseguente sia alla carenza di tiamina che alla neurotossicit del metronidazolo , nonch la possibilit che questultima possa essere mediata da meccanismi simili a quelli responsabili della encefalopatia di wernicke [ 32 ]  . la prognosi dellencefalopatia di wernicke estremamente variabile , dalla completa remissione della sintomatologia alla irreversibilit delle manifestazioni cliniche [ 59 ]  . 
 nelle fasi pi avanzate i pazienti possono perdere la capacit di apprendere nuove informazioni ( amnesia anterograda ) , riempiendo i vuoti coi ricordi passati , senza rendersi conto del loro problema , sino alla vera e propria psicosi o radiol med ( 2011 ) 116 : 319333 fig . 
8a - e acute wernickes encephalopathy in a nonalcoholic woman : t2 - weighted sagittal and axial ( a ) , serial nonconsecutive coronal uid attenuated inversion recovery ( b ) , gadolinium - enhanced t1 - weighted coronal and axial ( c ) mri at clinical presentation ; and flair coronal ( d ) and gadoliniumenhanced t1 - weighted axial ( e ) mri obtained 10 days later . 
at clinical presentation , high signal intensity areas are visible on long tr images in the inferior colliculi ( black arrows ) and medial thalami ( white arrows ) , with intense contrast enhancement of the inferior colliculi ( empty arrows )  . 
8a - e encefalopatia di wernicke acuta in donna non - etilista cronica : immagini rm sagittale e assiale t2 - dipendenti ( a ) , coronali seriali non consecutive flair ( b ) , coronale e assiale t1 - dipendenti dopo iniezione ev di mdc paramagnetico ( c ) alla presentazione clinica e coronale flair ( d ) e assiale t1 - dipendente dopo iniezione ev di mdc paramagnetico ( e ) dieci giorni dopo . 
alla presentazione clinica , si notano le aree di elevata intensit di segnale nelle immagini a tr lungo nei collicoli inferiori ( frecce nere ) e nei talami mediali ( frecce bianche ) , con intensa impregnazione dopo mdc dei collicoli inferiori ( frecce vuote )  . 
il controllo rm eseguito dieci giorni dopo dimostrava netta regressione dei segni patologici . involvement of less typical sites , especially the cortex , is considered a negative prognostic sign indicating progression and irreversibility of the encephalopathy [ 33 ]  . 
early diagnosis and an adequate supplementation with thiamine ( 100 to 500 mg / day intravenously ) are essential for rapid improvement and to prevent the appearance of irreversible neurological complications and death [ 59 ]  . 
determination of serum thiamine , thiamine monophosphate and erythrocyte transketolase activity can con rm the clinical suspicion , but the tests have limited sensitivity and availability [ 38 ]  . 
neuroradiological investigations are essential for con rming the clinical suspicion and obtaining an early diagnosis [ 8 , 9 ]  . sindrome di wernicke - korsakoff [ 3 , 7 ]  . 
la diagnosi precoce e ladeguato reintegro di tiamina ( da 100 a 500 mg / die per via endovenosa ) sono essenziali per il rapido miglioramento della sintomatologia ed evitano linstaurarsi di complicanze neurologiche irreversibili no al decesso [ 59 ]  . 
il dosaggio della tiamina sierica , della tiamina monofosfato e dellattivit della transchetolasi eritrocitaria possono supportare il dubbio clinico , ma purtroppo sono poco sensibili e scarsamente disponibili [ 38 ]  . 
the absence of neuroradiological ndings does not allow the diagnosis to be excluded , as many cases have been reported of wernickes encephalopathy with negative mri scans [ 12 , 19 ]  . 
 lassenza di reperti neuroradiologici , infatti , non consente di escludere la diagnosi , essendo ampiamente riportati in letteratura casi di encefalopatia di wernicke con esame rm negativo [ 12 , 19 ]  . 
liniezione del mdc paramagnetico , quindi , consente di ridurre la percentuale di falsi negativi dellesame rm e va considerato indicato nel dubbio clinico di encefalopatia di wernicke [ 33 ]  . 
 areas of enhancement in the mamillary bodies and thalami after contrast administration would be more frequent in chronic alcoholics , suggesting a higher sensitivity of these regions to the toxic effect of alcohol [ 32 ]  . 
areas of reduced diffusion are compatible with cytotoxic oedema of astrocytes and neurons due to excitotoxicity , whereas lesions with normal or increased adc values indicate the presence of vasogenic oedema . 
the dwi - adc study is likely to bene t from the availability of images with a thickness < 5 mm and with b values > 1 , 000 s / mm2 , as this has already proved useful in identifying hyperacute and acute lesions of intracranial nerve tissues , both supraand infratentorial [ 39 , 40 ]  . mr spectroscopy the few mr spectroscopy studies performed on wernickes encephalopathy [ 16 , 17 ] have demonstrated an increased lactate peak to be an isolated nding or associated with a reduction in the n - acetylaspartate / creatine ratio . 
le aree di impregnazione dopo mdc di corpi mammillari e talami sarebbero pi frequenti negli etilisti cronici , suggerendo una maggiore sensibilit di tali regioni alleffetto tossico dellalcool [ 32 ] , ma anche tale correlazione non univoca [ 26 ]  . 
 diffusione - rm con misura del coef ciente di diffusione apparente il ruolo dello studio rm in diffusione ( dwi ) con misura del coef ciente di diffusione apparente ( adc ) non ancora de nito . 
proprio per la natura dinamica della siopatologia dellencefalopatia di wernicke , peraltro , possibile la presenza contemporanea di aree di restrizione della diffusione e aree con diffusione normale o aumentata [ 29 ]  . 
le aree di restrizione della diffusione sono compatibili con edema citotossico di astrociti e neuroni da danno eccitotossico , mentre le lesioni con valori di adc normali o aumentati corrispondono alla presenza di edema vasogenico . 
alcuni autori ipotizzano che la presenza di aree di restrizione della diffusione con riduzione dei valori di adc possa rappresentare un fattore prognostico negativo , tuttavia sono necessari ulteriori studi per chiarire se il tipo di alterazioni riscontrate nelle sequenze dwi - adc correlino o meno con la prognosi . 
probabile che lo studio dwi - adc si possa avvantaggiare dalla disponibilit di immagini di spessore inferiore ai 5 mm e con valori di b superiori a 1000 s / mm2 , come gi stato dimostrato utile nellidenti cazione di lesioni iperacute e acute dei tessuti nervosi intracranici , soprae sotto - tentoriali [ 39 , 40 ]  . spettroscopia - rm gli studi di spettroscopia - rm in corso di encefalopatia di wernicke sono pochi [ 16 , 17 ] e generalmente hanno dimostrato lincremento del picco di lattato come reperto isolato o associato a riduzione del rapporto n - acetilaspartato / creatina . 
laumento del picco di lattato , evidente gi in fase acuta , sembra rappresentare unalterazione reversibile , congrua con liperintensit di segnale nelle immagini t2 - pesate ; stato ipotizzato che questo possa dipendere dallaumento del metabolismo anaerobio dei carboidrati conseguente al de cit di tiamina . 
in general , clinical manifestations also regress rapidly after the beginning of the therapy , even though residual de cits may often persist , and clinical progression cannot be excluded if treatment is not timely [ 59 ]  . 
in genere , anche le manifestazioni cliniche regrediscono rapidamente dopo linizio della terapia , ma non rara la persistenza di de cit residui , cos come non pu essere esclusa la progressione clinica in caso di trattamento non suf cientemente tempestivo [ 59 ]  . 
tutto ci conferma la necessit di una diagnosi quanto pi possibile precoce in ogni caso e , comunque , dimostra lopportunit di trattamento preventivo con tiamina nei malati a rischio . conclusions conclusioni wernickes encephalopathy should be suspected not only in chronic alcoholics , but in all clinical conditions involving malabsorption or malnutrition and in patients requiring protracted parenteral nutrition , especially if associated with the infusion of glucose solutions . 
the technique of choice is mri with a dwi - adc study and intravenous injection of gadolinium , bearing in mind that a negative mri does not allow the diagnosis to be excluded . 
mri diagnosis relies on knowledge of typical and atypical sites of involvement and on assessment of clinical and case history ndings . lencefalopatia di wernicke deve essere sospettata non solo negli etilisti cronici , ma in tutte le condizioni cliniche che comportano malassorbimento o malnutrizione e nei malati che necessitano di prolungati periodi di nutrizione parenterale , soprattutto se associata ad infusione di soluzioni glucosate . 
lesame elettivo rappresentato dalla rm comprensivo di studio dwi - adc e studio dopo iniezione ev di mdc paramagnetico , ma la negativit dellesame rm non consente di escludere la diagnosi . 
proportions of cases classified as categories 2 , 3 and 4 were 27.5% ( 90 / 327 ) , 44.3% ( 145 / 327 ) and 7.9% ( 26 / 327 ) , respectively . 
scopo del nostro lavoro stato valutare la resa diagnostica della tomografia computerizzata multidetettore ( tcmd ) del torace nellembolia polmonare acuta ( ep ) e la proporzione di altri reperti clinicamente rilevanti in unampia coorte di pazienti consecutivi , sia ricoverati che provenienti dal pronto soccorso ( ps )  . 
sono stati retrospettivamente considerati 327 referti radiologici di tcmd del torace eseguite per sospetta ep acuta in 327 pazienti ( 158 m , 169 f ; et media , 69 anni , deviazione standard [ ds ] 17 , 33 anni ; 233 ricoverati , 94 provenienti dal ps )  . 
 parole chiave tomografia computerizzata embolia polmonare polmonite introduction introduzione pulmonary embolism ( pe ) is the third most common acute cardiovascular disease and a frequent cause for acute hospital admission , with a reported associated mortality rate exceeding 15% in the first 3 months after diagnosis [ 1 , 2 ]  . 
in clinical practice , the diagnosis of acute pe continues to pose a challenge , because the presenting symptoms and signs are nonspecific and vary widely from one patient to another [ 3 ]  . 
 among diagnostic imaging modalities , multidetector computed tomography ( mdct ) is now considered the technique of choice for depicting the pulmonary vasculature when acute pe is suspected , replacing pulmonary angiography as the reference standard in this clinical scenario [ 5 ]  . 
the widespread availability , noninvasiveness and rapidity of image acquisition are determinant features of mdct , given that an early diagnosis may improve health outcomes and reduce mortality from pe [ 6 , 7 ]  . 
due to its inherent capability to provide detailed visualisation of chest anatomical structures , mdct can also give additional diagnostic the pulmonary parenchyma , mediastinum and thoracic wall , therefore leading to identification of alternative causes for the patients clinical presentation [ 810 ]  . 
 information on given the diagnostic potentialities of chest mdct and its frequent use in clinical practice when acute pe is suspected , the aim of this study was to evaluate over a lengthy period the clinical impact of chest mdct in a large cohort of consecutive patients clinically suspected of having acute pe and referred to our radiology institute . this was done by calculating the diagnostic yield of chest mdct and the proportion of clinically relevant findings other than pe , with particular attention to those requiring intervention . 
a secondary aim was to compare the proportion of chest mdct findings between hospitalised patients ( inpatients ) and patients referred from the emergency department ( outpatients )  . immediate and specific lembolia polmonare ( ep ) considerata la terza pi comune patologia cardiovascolare e rappresenta una causa frequente di accesso ad unit ospedaliera in acuto , con un tasso di mortalit stimato in circa il 15% nei primi tre mesi dalla diagnosi [ 1 , 2 ]  . 
a causa della presentazione con segni e sintomi non specifici , estremamente variabili da paziente a paziente , da un punto di vista clinico la diagnosi rimane un problema aperto [ 3 ]  . 
in soggetti selezionati , la diagnostica di laboratorio si pu avvalere del dosaggio del d - dimero : tale test , dotato di alta sensibilit e di alto valore predittivo negativo , risulta utile specie nellescludere la diagnosi di ep , soprattutto nelle unit di pronto soccorso ( ps ) [ 4 ]  . fra le tecniche di imaging , la tomografia computerizzata multidetettore ( tcmd ) rappresenta attualmente lindagine di prima scelta per la valutazione dellanatomia vascolare polmonare in presenza di sospetto di ep acuta e sostituisce nello scenario clinico odierno langiografia polmonare [ 5 ]  . caratteristiche determinanti della tcmd sono sicuramente la vasta disponibilit , la non invasivit e la rapidit desecuzione , dal momento che una diagnosi precoce fondamentale nel ridurre la mortalit e migliorare loutcome dei pazienti [ 6 , 7 ]  . 
stante la sua intrinseca capacit di fornire informazioni dettagliate anche sul parenchima polmonare e sulle altre strutture toraciche , come il mediastino e la parete , la tcmd pu consentire lindividuazione di eventuali altre cause responsabili della sintomatologia manifestata dal paziente [ 810 ]  . 
 alla luce delle potenzialit espresse dalla tcmd del torace e vista la sua alta frequenza di esecuzione , lo scopo di questo studio stato quello di valutare , in un lungo arco temporale , limpatto clinico della tcmd del torace in una serie consecutiva di pazienti sottoposti allesecuzione della stessa in regime durgenza con sospetto di ep acuta presso il nostro istituto . 
questo stato fatto valutando la resa diagnostica della tcmd e calcolando la proporzione di altri reperti clinicamente rilevanti , ponendo particolare attenzione per quelli che richiedevano un intervento immediato e specifico . 
un obiettivo secondario stato quello di confrontare la proporzione di reperti riscontrati nella sottopopolazione di pazienti ricoverati rispetto a quelli provenienti dallunit di ps . radiol med ( 2011 ) 116 : 219229 materials and methods materiali e metodi the institutional review board approved this retrospective cohort study and waived the patient informed consent requirement . 
the study was conducted in accordance with the principles of the declaration of helsinki . il comitato etico della struttura ha approvato questo studio di coorte retrospettivo senza necessit del consenso informato da parte del paziente . 
lo studio stato condotto in accordo ai principi della dichiarazione di helsinki . study population popolazione di studio through a systematic review of the mdct database of our institute , the examinations of all patients who underwent a chest mdct between january 2003 and june 2009 were considered . 
technical parameters were as follows : tube rotation time 0.5 s ; raw thickness 1 mm ; helical pitch 1.4 ; reconstruction width 1.5 macquisition was made at end - inspiration breath - hold and in the caudalcranial direction to minimise breathing artefacts in the lower lobes , where most emboli are located [ 11 ]  . 
an intravenous injection of 100 ml of 400 mgi / ml iomeprol ( iomeron 400 , bracco diagnostics , italy ) was administered at a flow rate of 4 ml / s , and the bolus - tracking technique ( toshiba sure - start ) was used with a region of interest ( roi ) placed at the level of the main pulmonary artery . 
all images were evaluated using three different window / level settings : one specific for pulmonary angiography ( 700 hu / 100 hu ) , one for pulmonary parenchyma ( 2 , 000 hu / 550 hu ) and one for mediastinum ( 350 hu / 50 hu )  . 
successivamente , sono state selezionate tutte le indagini condotte per sospetto di ep acuta in regime durgenza . stata inoltre valutata la proporzione di pazienti che hanno eseguito lesame provenendo dal pronto soccorso rispetto a quelli ricoverati . tecnica di indagine tutte le indagini sono state acquisite mediante lutilizzo di apparecchiatura tc multidetettore a 4 strati ( aquilion , toshiba medical systems , tokyo , giappone )  . 
successivamente allesecuzione di una scan view comprensiva di tutto il torace , dalla base del collo ai seni costo - frenici , stato posizionato un pacchetto di acquisizione compreso tra la convessit dellarco aortico e le vene polmonari inferiori . 
i parametri tecnici utilizzati sono stati i seguenti : tempo di rotazione 0 , 5 s ; collimazione 1 mm ; pitch 5 , 5 ; intervallo di ricostruzione 1 , 5 mlacquisizione avvenuta ad apnea inspiratoria in direzione caudo - craniale , al fine di minimizzare gli artefatti da respiro ai lobi polmonari inferiori , ove si riscontrano la maggior parte degli emboli [ 11 ]  . 
per ogni esame stato utilizzato un mezzo di contrasto iodato , iomeprolo , in concentrazione pari a 400 mgi / ml ( iomeron 400 , bracco diagnostics , milano , italia ) con un volume di 100 ml e un flusso ottimale di 4 ml / s tramite tecnica bolus tracking ( toshiba sure - start ) , con regione dinteresse posizionata sul tronco comune dellarteria polmonare . 
la documentazione dellesame stata effettuata con tre diverse finestre di visualizzazione : una finestra dedicata per ep ( livello 100 uh , larghezza 700 uh ) , una per parenchima polmonare ( livello - 550 uh , larghezza 2000 uh ) ed una per mediastino ( livello 50 uh , larghezza 350 uh )  . 
 data analysis analisi dei dati two radiologists in consensus retrospectively evaluated all mdct reports , and each examination was classified into one of four different categories using criteria modified from richman et al . 
 [ 8 ] e di seguito citati : categoria 1 : tc positive per embolia polmonare acuta ; categoria 2 : tc negative per embolia polmonare acuta ma positive per altri reperti richiedenti un intervento immediato e specifico ( 2a , sospetta polmonite ; 2b , 222 radiol med ( 2011 ) 116 : 219229 pericardial or pleural effusion ; 2e , lung nodules or masses suspected for lung cancer ; 2f , pneumothorax ; 2g , a new or changed mediastinal mass ; 2h , pneumomediastinum ) ; category 3 : completely negative or positive for findings with potential for significant morbidity requiring specific action on follow - up [ 3a negative ; 3b chronic obstructive pulmonary disease ( copd ) ; 3c stigmata of previous inflammatory / infectious processes ; 3d hepatic , renal or adrenal focal lesions ; 3e hiatal hernia ; 3f small pleural effusion ( 2 cm ) ; 3g atelectasis ; 3h lung metastasis with known cancer or known lung cancer ; 3i lung nodules or masses of uncertain aetiology ; 3j adenopathy ( 1 cm ) ; 3k unhealed rib fractures ; 3l new lung fibrosis ] ; category 4 : indeterminate examination due to degraded images that could not be interpreted ( 4a ) or questionable findings that could not be classified as category 2 or 3 ( including findings labelled as questionable or requiring clinical correlation ) ( 4b )  . if the description of findings in the radiological report was not completely clear , the two radiologists retrospectively reviewed the examination on a dedicated workstation ( vitrea , vital images , minneapolis , mn , usa ) ; any discrepancies were resolved by consensus . 
when findings classified in different categories were described , priority was given to the findings classified as category 1 , followed by category 2 , category 3 and category 4 . 
 statistical analysis the diagnostic yield , defined as the proportion of chest mdct considered positive for acute pe ( corresponding to cases classified as category 1 ) , and the proportions of other findings classified as category 2 and 3 , were calculated for the entire population . 
all statistical analyses were performed using commercially available software ( med - calc , version 9.2.0.1 , mariakerke , belgium )  . results through the systematic review of our mdct database , we identified 8 , 117 mdct examinations performed in the period specified . 
qualora nel referto vi fossero descritti pi reperti appartenenti a diverse categorie , per la classificazione stata attribuita maggior importanza ai reperti ascrivibili alla categoria 1 e successivamente alla categoria 2 e cos di seguito . 
 analisi statistica sono stati calcolati la resa diagnostica , definita come proporzione di casi positivi per riscontro di ep acuta ( casi classificati in categoria 1 ) , e la proporzione degli altri reperti toracici individuati nella popolazione generale . 
si inoltre stimata la proporzione di casi positivi per ep acuta e di casi con altri reperti , rispettivamente nel sottogruppo di pazienti provenienti dal ps e nei pazienti ricoverati . 
absolute values with the corresponding percentages in parenthesis entire population category 1 66 ( 20.18 ) category 2 90 ( 27.52 ) category 3 145 ( 44.34 ) category 4 26 ( 7.95 ) total 327 ( 100 ) tabella 1 ripartizione in categorie degli esami tcmd del torace nellintera popolazione . 
the proportion of examinations negative for pe but positive for other findings requiring specific and immediate intervention ( category 2 ) was 27.52% ( corresponding to 90 / 327 cases )  . 
in this tanti pazienti in regime durgenza con il sospetto clinico di ep acuta ( 158 maschi , 169 femmine ; et media , 69 anni ; deviazione standard ( ds ) , 17 , 33 anni ; range , 2198 anni )  . novantaquattro pazienti ( 28 , 75% ) sono stati sottoposti allindagine provenendo dal ps mentre i rimanenti 233 ( 71 , 25% ) erano pazienti ricoverati . 
la distribuzione dei reperti nelle quattro categorie nellintera popolazione riassunta in tabella 1 . nella popolazione generale , la resa diagnostica della tcmd del torace , proporzione dei reperti classificati in categoria 1 , risultata pari al 20 , 18% ( 66 / 327 casi )  . 
a limmagine tcmd del torace , visualizzata con settaggio angiografico , evidenzia la presenza di un parziale difetto di riempimento circondato da unesile rima di mezzo di contrasto a livello dellarteria per il lobo superiore del polmone destro , reperto diagnostico per embolia polmonare . 
b limmagine tcmd in riformattazione coronale conferma il difetto di riempimento occlusivo e ne dimostra lestensione nei rami segmentari per il lobo superiore . 224 radiol med ( 2011 ) 116 : 219229 fig . 
a chest mdct image displayed with angiographic window / level setting shows no filling defects in the pulmonary artery or its main branches . bilateral consolidation is visible in the posterior region of both lungs . 
b mdct image with parenchymal window / level setting clearly depicts a parenchymal consolidation with air bronchogram in the posterior segment of the right upper lobe , strongly suggestive of pneumonia . 
b limmagine tcmd visualizzata con settaggio per parenchima polmonare dimostra chiaramente la presenza di un consolidamento parenchimale con broncogramma aereo a carico del segmento dorsale del lobo superiore del polmone destro , fortemente suggestivo per polmonite . 
the proportion of chest mdct completely negative or positive for findings with potential for significant morbidity requiring specific action on follow - up ( category 3 ) was 44.34% ( corresponding to 145 / 327 cases )  . 
 in the subgroup of 94 outpatients , the diagnostic yield for the presence of acute pe was 23.40% ( corresponding to the 22 / 94 cases classified as category 1 )  . 
the proportion of examinations negative for pe but positive for other findings requiring specific and immediate intervention ( category 2 ) was 19.15% ( corresponding to 18 / 94 cases )  . 
 in the subgroup of 233 inpatients , the diagnostic yield for the presence of acute pe was 18.88% ( corresponding to the 44 / 233 cases classified as category 1 )  . 
the proportion of examinations negative for pe but positive for other findings requiring specific and immediate intervention ( category 2 ) was 30.90% ( corresponding to 72 / 233 cases )  . 
examinations classified as category 3 were 99 / 233 ( 42.49% ) , and those tivi per reperti richiedenti unazione immediata e specifica ( categoria 2 ) risultata pari a 27 , 52% ( 90 / 327 casi )  . 
in questa categoria , il reperto pi frequente stato quello della sotto - categoria 2a ( sospetta polmonite ) , per un totale di 37 / 327 casi ( 11 , 37% )  . 
la proporzione di tcmd del tutto negative o positive per reperti di potenziale morbilit meritevoli di follow - up ( categoria 3 ) stata del 44 , 34% ( 145 / 327 casi )  . 
 nella sottopopolazione dei 94 pazienti provenienti dal pronto soccorso , la proporzione di casi positivi per ep stata pari al 23 , 40% ( 22 / 94 casi classificati in categoria 1 ) ; quella di casi appartenenti alla categoria 2 pari al 19 , 15% ( 18 / 94 casi ) ; alla categoria 3 pari al 48 , 94% ( 46 / 94 casi ) ed infine pari al 8 , 51% quella dei casi classificati in categoria 4 ( 8 / 94 casi )  . nel sottogruppo dei 233 pazienti ricoverati il 18 , 88% ( 44 / 233 casi ) delle indagini stato classificato in categoria 1 ; il 30 , 90% ( 72 / 233 casi ) in categoria 2 ; il 42 , 49 ( 99 / 233 ) in categoria 3 ed il 7 , 73% ( 18 / 233 casi ) in categoria 4 . 
there were no significant differences in the distribution of mdct findings between inpatients and outpatient . in recent years , ct pulmonary angiography has become a widely accepted first - line imaging technique in evaluating suspected acute pe [ 12 , 13 ]  . 
substantial advances in mdct technology have guaranteed improvement in spatial and temporal resolution and in overall diagnostic performance . data from a variety of studies revealed a sensitivity of i risultati del nostro studio dimostrano che la tcmd del torace ha un grande impatto clinico nei pazienti con sospetta ep acuta , con una resa diagnostica del 20 , 2% e una proporzione aggiuntiva di reperti clinicamente rilevanti con necessit di intervento immediato e specifico del 27 , 5% . non stata dimostrata una differenza statisticamente significativa nella distribuzione dei reperti fra i pazienti provenienti dal pronto soccorso e quelli ricoverati . 
i risultati di diversi studi hanno dimostrato , nella diagnosi di ep acuta , una sensibilit della tcmd del torace compresa fra 83% e 100% e una specificit compresa fra 89% e 98% [ 1417 ]  . 
unelevata accuratezza delle metodiche di imaging di cruciale importanza , in quanto la maggior parte dei casi di decesso per embolia polmonare prevenibili dovuta ad un misconoscimento della diagnosi piuttosto che a un fallimento dellapproccio terapeutico , oramai codificato [ 3 ]  . 
i progressi tecnici e la validazione clinica hanno condotto la fleischner society a stabilire che la 226 radiol med ( 2011 ) 116 : 219229 table 3 division into categories of the chest mdct exams in patients referred from the emergency department ( outpatients ) and in inpatients . 
absolute values with the corresponding percentages in parenthesis category 1 category 2 category 3 category 4 total outpatients inpatients 22 ( 23.40 ) 44 ( 18.88 ) 18 ( 19.15 ) 72 ( 30.90 ) 46 ( 48.94 ) 99 ( 42.49 ) 8 ( 8.51 ) 18 ( 7.73 ) 94 ( 100 ) 233 ( 100 ) tabella 3 ripartizione in categorie degli esami tcmd eseguiti nei pazienti provenienti dal pronto soccorso e nei pazienti ricoverati . 
i valori sono espressi come valori assoluti e fra parentesi riportata la percentuale categoria 1 categoria 2 categoria 3 categoria 4 totale pazienti esterni pazienti interni 22 ( 23 , 40 ) 44 ( 18 , 88 ) 18 ( 19 , 15 ) 72 ( 30 , 90 ) 46 ( 48 , 94 ) 99 ( 42 , 49 ) 8 ( 8 , 51 ) 18 ( 7 , 73 ) 94 ( 100 ) 233 ( 100 ) 83%100% and a specificity of 8998% for chest mdct in diagnosing acute pe [ 1417 ]  . 
a high accuracy of imaging modalities is crucial , as the majority of preventable deaths related to acute pe can be ascribed to a missed diagnosis rather than to a failure of codified therapies [ 3 ]  . 
technical advances and clinical validation of the diagnostic modality led the fleischner society to establish that ct pulmonary angiography has fulfilled the conditions to replace conventional pulmonary angiography as the standard of reference for diagnosing acute pe [ 5 ]  . 
recently , the use of mdct scanners with more than 16 slices has been shown to decrease the incidence of nondiagnostic examinations and to increase the confidence level in the clinical scenario of suspected acute pe [ 10 ]  . 
in agreement with the literature [ 19 ] , we found no statistically significant difference in terms of diagnostic yield between the two subgroups , thus confirming the importance of ct as the first - line diagnostic imaging modality in both inpatients and outpatients . 
when pe is suspected , a further advantage of chest ct over other imaging methods relates to its ability to rule out or detect alternative diagnoses [ 21 ]  . 
 in our study , we classified all chest mdct findings in a tcmd del torace soddisfa tutte le condizioni necessarie per sostituire langiografia polmonare convenzionale come metodica di riferimento nella diagnosi di ep acuta [ 5 ]  . recentemente , inoltre , lutilizzo di apparecchiature tcmd con 16 strati ed oltre ha dimostrato una riduzione delle indagini non diagnostiche ed un aumento della confidenza nella diagnosi nel sospetto clinico di ep acuta [ 10 ]  . la percentuale di casi positivi per ep stata rispettivamente del 23 , 4% in pazienti provenienti dal pronto soccorso e del 18 , 9% nei pazienti ricoverati . 
questo dato in accordo con quanto espresso in precedenti studi , dove le percentuali variano rispettivamente dall8 , 5% al 29 , 8% e dal 19 , 5% al 27 , 4% . 
in accordo con la letteratura [ 19 ] , non stata evidenziata una differenza statisticamente significativa nella distribuzione dei reperti in categoria 1 , a conferma dellimportanza della tcmd del torace quale indagine di prima istanza in regime durgenza sia nei pazienti ricoverati che in quelli provenienti dal pronto soccorso . 
un ulteriore vantaggio della tcmd del torace rispetto ad altre indagini , nel sospetto di ep , quello conseguente alla capacit di consentire eventuali diagnosi alternative [ 21 ]  . 
 stato dimostrato che la tomografia computerizzata ( tc ) aggiunge informazioni diagnostiche che possono suggerire una diagnosi alternativa in ben il 67% di pazienti privi di ep [ 22 ]  . 
 [ 19 ] hanno riscontrato che nei pazienti senza evidenza di ep , i reperti alternativi individuati dalla tcmd del torace variano fra l89 , 8% ed il 76 , 2% del totale dei reperti in una popolazione di pazienti ricoverati e in una di pazienti provenienti dal pronto soccorso , rispettivamente [ 19 ]  . 
lesame ha rivelato la presenza di reperti negativi per ep e compatibili con una diagnosi specifica ed radiol med ( 2011 ) 116 : 219229 categorisation system modified from that proposed by richman et al . 
in that study , a multicentre cohort of outpatients with suspected pe was considered , and chest ct revealed findings compatible with a specific , alternative diagnosis to pe requiring immediate treatment in 7% of cases negative for pe . 
these data are similar to results of a recent study in which acute clinically relevant thoracic non - pe findings were discovered in 25.5% of patients referred from the emergency department for suspected pe [ 10 ]  . the difference between richman et al.s and our series in terms of proportion of outpatients with alternative diagnosis to pe requiring specific and immediate intervention can be partially explained by the fact that , unlike richman et al . , we included in this category four patients with extensive pleural effusion . 
 suspected pneumonia ( category 2a ) was the most frequent alternative diagnosis disclosed ( 14.2% of non - pe findings ) in our study , which in agreement with previous studies that reported frequencies ranging from 6% to 33% of non - pe findings [ 8 , 10 18 , 22 , 23 ]  . 
the presence of such findings confirms that lung cancer is a relatively uncommon but not rare finding on chest mdct studies performed to rule out acute pe [ 9 ]  . 
in agreement with previously reported data [ 24 ] , a per - year analysis of chest mdct requested to rule out acute pe revealed an increasing use of this imaging technique over recent years , without a significant change in the frequency of pe detected . our study has several limitations . 
for this reason , the described distribution of findings is solely dependent on radiological reports . second , all examinations were performed with a four - slice mdct scanner , without evaluating cardiac diseases and with inherent limitations concerning scan time and the alternativa , richiedente intervento immediato , nel 7% dei casi . 
i nostri risultati mostrano che nel 30 , 9% dei pazienti ricoverati e nel 19 , 1% dei pazienti provenienti dal pronto soccorso la tcmd del torace fornisce informazioni riguardanti reperti negativi per embolia ma richiedenti un intervento immediato e specifico ( categoria 2 )  . 
tali dati sono simili a quanto riportato in un recente studio in cui , in un gruppo di pazienti provenienti dal pronto soccorso e sottoposti allesecuzione di tcmd del torace per sospetta ep , emerso un 25 , 5% di reperti toracici acuti alternativi clinicamente rilevanti [ 10 ]  . 
 [ 8 ] e la nostra casistica in termini di pazienti provenienti dal pronto soccorso con reperti alternativi alla ep e meritevoli di intervento specifico ed immediato pu essere in parte attribuita al fatto che , a differenza di richman et al . 
un altro aspetto di cui tenere conto la differenza riscontrata nella proporzione di casi di sospetta polmonite ( il reperto pi frequente fra quelli richiedenti un intervento immediato e specifico in entrambe le casistiche ) , pari al 9 , 6% ( 9 / 94 casi ) nel nostro studio ed al 5 , 3% ( 54 / 1025 casi ) in quello di richman et al . 
 la diagnosi alternativa pi frequente ( 14 , 2% delle tcmd negative per embolia ) stata quella di sospetta polmonite , in accordo con precedenti studi che hanno evidenziato frequenze di polmonite comprese fra il 6% e il 33% di tc negative per embolia [ 8 , 10 , 18 , 22 , 23 ]  . 
nel 2 , 1% dei pazienti ( 7 / 327 ) si sono riscontrate nodularit polmonari o tumefazioni sospette per presenza di processo produttivo primitivo polmonare ( categoria 2e )  . 
la presenza di tali reperti conferma che le neoplasie del polmone sono un reperto alternativo infrequente ma non cos raro in esami tcmd del torace eseguiti per sospetta ep [ 9 ]  . 
in accordo con risultati precedenti [ 24 ] , unanalisi per anno delle richieste di tcmd del torace per sospetta ep ha dimostrato un incremento del ricorso a questa metodica di imaging negli ultimi anni senza significative differenze nella frequenza di ep riscontrate . 
secondo , tutte le indagini sono state eseguite mediante lutilizzo di unapparecchiatura tcmd a 4 strati , senza la possibilit di valutare patologie cardiache e con limiti intrinseci riguardanti la velocit di esecuzione e la presenza di artefatti da movimento respiratorio . 
fourth , only the overall diagnostic yield of acute pe was evaluated , without considering different levels of pretest clinical probability or d - dimer test results , which could have influenced the reported percentage of examinations positive for acute pe . 
the other side of the coin is represented by half cases without an apparent cause justifying the examination in an emergency setting , thus confirming the importance of a specific indication for each single chest mdct performed . 
 acknowledgements authors thank daniela drigo for her valuable contribution to the statistical analysis of this work . riportato in precedenti pu aver influenzato il numero di esami totalmente negativi ( categoria 3 ; 11 , 9% dei casi ) o quello di esami in cui stata rilevata la presenza di reperti non richiedenti un intervento immediato ( categoria 3b - l ; 32 , 1% dei casi ) , con possibile mancata individuazione di condizioni rilevanti ( ad esempio , piccoli emboli polmonari periferici )  . 
nonostante ci , la percentuale di reperti indeterminati ( categoria 4 , 7 , 95% ) simile a quanto lavori ( 6 , 1%10 , 4% ) [ 10 ]  . 
tuttavia , un ridotto volume di acquisizione funzionale a una riduzione della dose [ 25 ] ed a un miglioramento della qualit complessiva delle immagini quando si utilizza una apparecchiatura tcmd a 4 strati . quarto , stata valutata solo la resa diagnostica globale per la presenza di ep , senza considerare diversi livelli di probabilit pre - test da correlare alla clinica o al dosaggio del d - dimero ; ci potrebbe aver influenzato la percentuale di esami positivi per la presenza di ep acuta . in conclusione , in pazienti con sospetta ep acuta la tcmd del torace pu riconoscere sia ep sia reperti che suggeriscano una diagnosi alternativa richiedente un intervento immediato e specifico ( vale a dire , pazienti classificati in categoria 1 e 2 ) in circa il 50% dei casi , senza differenze tra i pazienti ricoverati e quelli provenienti dal pronto soccorso . 
shimizu1 1department of respirology and rheumatology , faculty of medicine , tottori university , 36 - 1 nishimachi , yonago 683 - 8504 , japan 2department of respirology san - in rosai hospital , 1 - 8 - 1 kaikesinden , yonago 683 - 8504 , japan correspondence to : m . 
it has been reported that the prognosis differs between patients who have collagen vascular diseaseassociated interstitial pneumonia ( cvd - ip ) and those with idiopathic ip ( iip )  . 
measuring the llv / tlv ratio by threedimensional ct can help distinguish between cvd - ip and iip at initial diagnosis , especially in patients with cvd - ip who have pulmonary involvement before other organ diseases and symptoms caused by cvd . keywords collagen vascular disease interstitial pneumonia lower - lobe volume total lung volume three - dimensional computed tomography abstract obiettivo . 
non sono state evidenziate differenze significative nel rapporto llv / tlv tra i due gruppi di pazienti . nonostante questo , il rapporto risultava inferiore a 0 , 33 in 9 pazienti su 23 con cvd - ip e in 2 pazienti su 24 affetti da iip , ed stata dimostrata una differenza significativa nella percentuale di pazienti con un rapporto inferiore a 0 , 33 tra i due gruppi ( p = 0 , 001 )  . 
la misurazione del rapporto llv / tlv tramite tc tridimensionale pu aiutare a distinguere , nelle fasi iniziali , la polmonite interstiziale associata a patologia del collagene da quella idiopatica , specialmente nei pazienti con patologie del collagene che hanno una manifestazione polmonare prima dellinizio della sintomatologia e prima del coinvolgimento degli altri organi . parole chiave patologie del collagene vascolare polmonite interstiziale volume del lobo inferiore volume totale del polmone tc tri - dimensionale 212 introduction it has been reported that the prognosis of patients who have collagen vascular disease - associated interstitial pneumonia ( cvd - ip ) is better than that of patients with idiopathic ip ( iip ) [ 15 ]  . 
iip is classified into seven types based on various clinical , radiological and pathological features [ 6 ]  . the majority of patients with iip have idiopathic pulmonary fibrosis ( ipf ) [ 7 ] , whereas the next most common type is nonspecific ip ( nsip ) [ 7 ]  . 
however , most patients with cvd - ip are now classified as having nsip , and only a minority of them shows a uip pattern [ 5 , 811 ]  . 
unlike the case for iip , the prognosis of nsip is not different from that of uip in patients with cvd - ip [ 12 ]  . accordingly , distinguishing cvd - ip from iip is very important for predicting the prognosis , because cvd - ip has a better prognosis than iip , irrespective of the histological pattern of lung disease [ 15 ]  . high - resolution computed tomography ( hrct ) can diagnose ipf with a sensitivity of 4378% and a specificity of 9097% [ 13 ]  . 
furthermore , lung biopsy is performed in < 15% of patients with interstitial lung disease , even though it is an effective method for distinguishing between cvd - ip , nsip and ipf [ 14 ]  . this study was performed to investigate whether differences of ct findings between cvd - ip and iip were helpful for making a differential diagnosis . 
however , there is little available literature about the lower - lobe volume ( llv ) and total lung volume ( tlv ) in either cvd - ip or iip . 
we calculated the llv / tlv ratio 3d computed tomography ( ct ) to investigate the difference of lower - lobe shrinkage between cvd - ip and iip patients at initial diagnosis . materials and methods participants study participants were 23 patients with cvd - ip and 24 with iip . 
for the diagnosis of iip , we used the american thoracic society / european respiratory society consensus classification [ 6 ]  . surgical lung biopsy was performed in seven of 24 patients with iip , including five with uip and two with nsip . 
the diagnosis of iip was made by exclusion of other diffuse parenchymal lung diseases that could be detected with bal and tblb , such as infections , sarcoidosis , hypersensitivity pneumonitis , pneumoconiosis , bronchiolitis obliterans organizing pneumonia , eosinophilic pneumonia and pulmonary histiocytosis x . 
patients were not diagnosed as having iip if they were positive for one or more of the following : ( 1 ) antinuclear antigen ; ( 2 ) rheumatoid factor ; ( 3 ) anti - scleroderma ( scl - 70 ) antibody ; ( 4 ) sjgrens syndrome a or b ; and ( 5 ) jo - 1 antibody . pulmonary dysfunction was defined by a percentage of predicted forced vital capacity ( %fvc ) or percentage of predicted single - breath diffusion capacity for carbon ( %dlco ) < 80% . 
as a result , there were two patients with systemic lupus erythematosus ( sle ) , two with mixed connective tissue disease dermatomyositis / polymyositis ( mctd ) , ( dm / pm ) , one with microscopic polyangiitis ( mpa ) , six with rheumatoid arthritis ( ra ) , one with sjgrens syndrome ( ss ) and six with systemic sclerosis ( ssc )  . 
ten healthy controls who were referred to our hospital because abnormal findings were detected on chest radiographs at other hospitals but who had no significant abnormalities on chest ct were also enrolled . radiol med ( 2011 ) 116 : 211218 pulmonary function tests pulmonary function tests were done three times consecutively with a dry spirometer ( minato , tokyo , japan ) , and the highest values were recorded . 
the following parameters were measured : vital capacity ( vc ) , forced vital capacity ( fvc ) , forced expiratory volume in 1 s ( fev1 ) , residual volume ( rv ) using the helium dilution method , total lung capacity ( tlc ) , single - breath - diffusing capacity for carbon monoxide ( dlco ) and alveolar volume ( va ) using the single - breath method . 
rv was determined in three patients with cvd - ip , 11 with iip and one healthy control . calculation of lung volume chest ct was performed in the supine position with a multislice scanner ( aquilion , toshiba , tokyo , japan )  . 
all images were obtained at maximal inspiration using the following parameters : 120 kv , auto ma , 1 - mm collimation at 5 - mm intervals , window level of 600 hounsfield units ( hu ) and window width of 1 , 600 hu . 
after tlv was measured , the lower lobe was traced by confirming the major fissure on each slice and then the lower - lobe volume ( llv ) was calculated by the software . all procedures were done by two experienced respiratory physicians . data analysis results are shown as the mean standard deviation ( sd )  . associations between tlv and tlc were assessed by linear regression analysis and by creating a bland - altman plot [ 29 ]  . 
spss software ( japanese version 16.0 for windows ; spss japan inc . , tokyo , japan ) was used for statistical analysis and creating receiver - operating - characteristic ( roc ) curves . 
there were significant differences of age , gender , smoking history , %dlco , and partial pressure of arterial carbon dioxide ( paco2 ) between cvd - ip and iip patients . 
however , %fvc and alveoloarterial oxygen difference ( aado2 ) did not differ significantly between the groups . accuracy of calculating tlv by ct volumetry in 15 individuals ( one control , three patients with cvd - ip and 11 patients with iip ) , the tlv calculated by ct volumetry was plotted against the tlc measured by spirometry . 
there was no bias between spirometry and ct volumetry for measurement of lung volume ( p = 0.28 ) , and 93% of values were within the limits of agreement . ct volumetry and roc analysis the mean tlv was 4 , 640225 ml in the ten controls , 3 , 968167 ml in the 24 patients with iip and 3 , 599163 ml in the 23 patients with cvd - ip . 
1a , b relationship between total lung capacity ( tlc ) measured by spirometry and total lung volume ( tlv ) measured by 3d computed tomography ( ct )  . 
closed triangle is a healthy control , closed circles are patients with iip and open circles are patients with collagen vascular disease - associated interstitial pneumonia ( cvdip )  . 
1a , b relazione tra capacit totale polmonare ( tlc ) misurata con spirometria e volume totale del polmone ( tlv ) misurato con tc tridimensionale . correlazione tra tlv e tlc . 
le linee punteggiate orizzontali indicano la media + o 1 , 96 di deviazione standard . radiol med ( 2011 ) 116 : 211218 * * p < 0.001 controls cvd - ip * p < 0.001 cvd - ip fig . 
3 comparison of patients with a lower - lobe volume / total lung volume ( llv / tlv ) ratio < 0.33 in the idiopathic interstitial pneumonia ( iip ) and collagen vascular disease - associated interstitial pneumonia ( cvd - ip ) groups . 
the llv / tlv ratio was < 0.33 in 9 / 23 cvd - ip patients and 2 / 24 iip patients . iip patients with an llv / tlv ratio < 0.33 were dissociated from the other patients . 
3 confronto tra i pazienti con un rapporto llv / tlv < 0 , 33 nel gruppo della polmonite interstiziale idiopatica ( iip ) e nel gruppo della polmonite interstiziale associata a patologie del collagene vascolare ( cvd - ip )  . 
i pazienti con iip che hanno un rapporto < 0 , 33 si presentavano dissociati dagli altri pazienti.si dimostrava una differenza significativa nella frequenza di un rapporto < 0 , 33 tra i due gruppi cdv - ip e iip ( p = 0 , 01 )  . less or more than 0.33 ( table 2 )  . 
2 lower - lobe volume / total lung volume ( llv / tlv ) ratio of controls , idiopathic interstitial pneumonia ( iip ) patients and collagen vascular disease - associated interstitial pneumonia ( cvd - ip ) patients . 
2 volume del lobo inferiore / volume totale ( llv / tlv ) nei controlli , nel gruppo di pazienti con iip e nel gruppo di pazienti con cdv - ip . 
iip contro cvd - ip , non significativo . discussion it has been reported that patients with cvd - ip have a better prognosis than patients with iip [ 15 ] , suggesting that it is important to distinguish cvd - ip from iip . 
in this study , we investigated the difference in frequency of an llv / tlv ratio < 0.33 at initial diagnosis between patients with cvdip and iip using 3d ct . 
we found that there was marked lower - lobe shrinkage in more patients with cvd - ip , suggesting that measuring the llv / tlv ratio by 3d ct may be useful to distinguish between cvd - ip and iip at an early stage without the need for surgical lung biopsy . calculation of lung volume by 3d ct although lung function tests are very useful , it is impossible to assess the volume of each lobe separately . 
when we investigated the validity of calculating the lung volume by 3d ct , a significant correlation was found between tlc measured by spirometry and tlv obtained with 3d ct . 
accordingly , we propose that 3d ct is a useful and reliable method for calculating lung volume . detection of the major fissure was easy on 2d ct and the lower lobe was traced by confirming the major fissure on each ct slice . 
there have also been many reports about measurement of the volume of organs and tumours by tracing [ 26 , 27 ] , indicating that 3d ct can be used to calculate llv . 216 radiol med ( 2011 ) 116 : 211218 fig . 
our results suggest that lower - lobe shrinkage was marked in some patients with cvd - ip at an early stage of disease . an llv / tlv ratio < 0.33 showed a high specificity but low sensitivity for distinguishing cvd - ip from iip at an early stage judging from the results of roc analysis . patients with cvd - ip had a wider range of llv / tlv ratios than patients with iip . 
this difference in the distribution of llv / tlv ratio data explains the high specificity and low sensitivity of a cutoff value of 0.33 for distinguishing cvd - ip from iip . 
therefore , our findings suggest that ip in a patient with an llv / tlv ratio < 0.33 is probably pulmonary involvement of cvd , and a cutoff value llv / tlv ratio < 0.33 is useful to discriminate between early cvd - ip and iip . patients with an llv / tlv ratio < 0.33 nearly all had cvd - ip . 
our findings suggest that patients with ip and an llv / tlv ratio < 0.33 probably have cvd - ip , and thus will have a good prognosis , even if the histological appearance is uip . there are two possible mechanisms by which the lower lobe may shrink so markedly in patients with cvd - ip from an early stage compared with iip . 
one is a difference in the intrapulmonary distribution of ip , and the other is dysfunction of the diaphragthe lower lobes are predominantly involved in ipf , nsip and cvd - ip compared with the other lobes . 
mild dysfunction of the diaphragm might enhance lower - lobe shrinkage , even in patients with early ip , such as our cases 1 , 2 , 6 and 8 ( table 3 )  . 
197 , rui jin er road , shanghai , 200025 , china 2ct laboratory of ge healthcare , beijing economic and technology development area , beijing , china correspondence to : z - l . 
this study compared the performance of prospectively electrocardiographically ( ecg ) - triggered axial computed tomography ( ct ) angiography with retrospective technique in evaluating coronary artery stent restenosis by 64 - slice ct . 
a pulsing cardiac phantom with artificial coronary artery in - stent restenosis was examined by ct angiography with different types of scan modes . the visibility of in - stent restenosis was evaluated with a three - point score . 
artificial lumen narrowing [ ( inner stent diameter - measured lumen diameter ) / inner stent diameter ] , lumen attenuation increase ratio [ ( in - stent attenuationcoronary artery lumen attenuation ) / coronary artery lumen attenuation ] , measurement error of restenosis percent [ ( known restenosis percent - measured restenosis percent ) / known restenosis percent ] and imaging noise were analysed . 
prospective acquisition showed better visibility than retrospective acquisition ( p < 0.05 ) : 61% of in - stent restenoses had good visibility on the prospective acquisition compared with 17% on the retrospective acquisition . 
artificial lumen narrowing ( mean 40% ) , lumen attenuation increase ratio ( mean 33% ) and measurement error of restenosis percent were not different between types of ct acquisitions . 
lacquisizione prospettiva ha dimostrato una migliore identificazione rispetto allacquisizione retrospettiva ( p < 0 , 05 ) : il 61% delle restenosi intrastent ha dimostrato una buona identificazione nelle acquisizioni prospettiche a fronte del 17% ottenuto con le acquisizioni retrospettiche . 
il lume artificiale stenotico ( media del 40% ) , il rapporto di incremento di attenuazione del lume ( media del 33% ) , e lerrore di 190 radiol med ( 2011 ) 116 : 189196 technique , prospective coronary ct angiography offers improved image quality and reduces effective radiation dose in evaluating in - stent restenosis . keywords stent coronary artery cta introduction whereas stent implantation is a successful treatment for coronary artery disease , 9.631.6% of coronary artery stents develop restenosis [ 1 , 2 ]  . 
consequently a noninvasive and available method of stent follow - up becomes indispensable . recently , 64 - slice coronary computed tomography angiography ( cta ) has played an increasing role in assessing coronary arteries and in coronary artery stent imaging [ 35 ]  . however , blooming and streak artefacts from high - attenuation material , such as stent struts that interfere with visualising the stent lumen , are still a common problem for 64slice scanners with improved spatial and temporal resolution . although retrospective electrocardiographically ( ecg ) gated helical ( reh ) scans are mainly used , with advances in technique , prospective ecg - triggered axial ( pea ) scans allow a substantial reduction in radiation dose compared with reh scans ( 15 msv reduced to 1.05 msv ) while having a possible advantage for in - stent restenosis imaging owing to the reduction of artefacts compared with reh scans [ 610 ]  . 
therefore , the purpose of our study was to clarify the influence of scan modes and tube voltage on the in - stent visibility , artificial lumen narrowing and lumen attenuation by using in - stent 50% and 75% restenosis vessel models . 
we also compared in - stent visibility obtained for different heart rates and coronary artery diameters . materials and methods cardiac phantom we used a prototype cardiac phantom ( developed by the ct lab of ge health care , china )  . 
a confronto con la tecnica retrospettiva tradizionale , langio tc conorarica prospettiva offre una migliore qualit delle immagini e riduce la dose di radiazioni effettiva nella valutazione della restenosi intrastent . 
 parole chiave stent arterie coronarie angio - tc coronary artery stent and in - stent restenosis models coronary artery models were made of acrylicsilicon tubes with an inner diameter of 3 or 4 mm and filled with contrast material ( iopamidol 350 , bracco , italy ) diluted to 300 hu . they were closed at both ends and positioned in an orientation parallel to the z - axis of the scanner . 
for prospective scanning , the centre of the temporal window corresponded to 75% of the r - r interval , and the exposure time was set to the minimum ( 233 ms )  . 
in order to compare image quality with different tube voltages under the same radiation dose , 100 kvp and 720 ma , 120 kvp and 500 ma and 140 kvp and 360 ma were used following the equation : ma1 / ma2 = kvp1 2 / kvp2 radiol med ( 2011 ) 116 : 189196 fig . 
2 coronary artery stent and in - stent restenosis models showing configuration of the cypher stent with a strut thickness of 0.14 mthe stent with artificial in - stent stenosis was inserted into a coronary artery model . 
2 modelli di stent coronarici e di restenosi intra - stent mostrano la configurazione di uno stent cypher con spessore delle maglie di 0 , 14 mlo stent con stenosi artificiale era stato inserito in un modello di arteria coronaria . 
il diametro delle arterie coronarie era di 3 o 4 mle arterie erano riempite con mezzo di contrasto diluito a 300 uh e chiuse ad entrambi i lati da un tappo di silicone . image analysis lumen visibility all images were analysed on a separate workstation ( advantage workstation version 4.4 , ge healthcare , waukesha , wi , usa ) by two independent , experienced radiologists blinded to the ct protocols . 
disagreements were resolved by a third observer . 192 radiol med ( 2011 ) 116 : 189196 measurement of artificial lumen narrowing by using electronic callipers , two independent observers measured inner stent diameter and visible lumen diameter with in - stent restenosis , on the line parallel to the x - axis on each image , using the workstation semiautomatic software vessel analysis ( advantage workstation with cardiq software , version 4.4 , ge healthcare , milwaukee , wi , usa )  . 
all measurements were repeated three times and the mean of the measurements by two observers was calculated separately . artificial lumen narrowing was calculated using the following equation [ 9 , 10 ] : artificial lumen narrowing = ( inner stent diameter visible lumen diameter ) / inner stent diameter . lumen attenuation increase ratio to quantify the effects of blooming artefacts on luminal ct attenuation , lumen attenuation increase ratio was calculated according to the following equation : lumen attenuation increase ratio = ( in - stent attenuation coronary artery lumen attenuation ) / coronary artery lumen attenuation [ 9 ]  . attenuation values inside the visible stent lumen were measured using a region of interest ( roi ) , the size of which was drawn as small as possible to avoid stent struts and artefacts . 
two observers plotted out the vessel segment with restenosis , restenosis diameter was measured , the percent was calculated using the following equation : measured restenosis percent = measured restenosis diameter / inner stent diameter . 
measurement errors of the 50% and 75% in - stent restenosis were compared using repeated measurements and analysis of variance ( anova )  . noise was defined as the standard deviation ( sd ) of an roi density measuring the water inside the rubber balloon . measurements were repeated three times to avoid intraobserver variation , and mean value was calculated . 
3 la visibilit della restenosi intrastent stata valutata con un punteggio di qualit dimmagine a tre punti : valore 1 , buono ( chiara visibilit del lume dello stent coronarico con restenosi ) ; valore 2 , moderato ( restenosi visibile ma grado di stenosi non valutabile ) ; valore 3 , basso ( lume dello stent coronarico non valutabile a causa di importanti artefatti )  . consequently , dlp is defined with the assumption that the heart ranges by 14 cm in the z - axis , and the dlp is thus calculated by the following equation : dlp ( mgycm ) = volume computed tomography dose index ( mgy ) 14cm . the effective dose ( e ) was calculated using the following equation : e = kdlp , where k is a conversion coefficient for the anatomical region examined , i.e. 
interobserver reliability for measuring diameter or attenuation was tested by pearsons correlation coefficient . anova for continuous variables and the kruskalwallis test for categorical data were used to compare the effects of the scan type , heart rate , vessel calibre and tube voltage on assessing and measuring stent imaging . 
a two - sided significance level of 0.05 was used in all analyses . results lumen visibility the dose - length product ( dlp ) displayed on the phantom study is not suited for simulating dlp on real patients . kruskal - wallis test proved that there was a significant radiol med ( 2011 ) 116 : 189196 fig . 
one - way anova revealed that this was not different between stent calibres for 75% and 50% restenosis ( p = 0.82 for 75% ; p = 0.71 for 50% ) , heart rates ( p = 0.44 for 75% ; p = 0.93 for 50% ) , scan modes ( p = 0.43 for 75% ; p = 0.59 for 50% ) and tube voltages ( p = 0.27 for 75% ; p = 0.52 for 50% restenosis ) for both 75% and 50% . noise mean noise of water inside the rubber balloon was 24.85 , which was similar to the enhanced aortic root in the clinical routine . 
 radiation dose discussion recent advances in technique of 64 - slice ct , including larger detector coverage , higher temporal and spatial resolution and real - time ecg signal monitoring , make it possible to use pea scans for coronary cta [ 68 ]  . 
for pea scans , x - ray exposure is applied only during the required phase of the cardiac cycle , with complete pausing during the rest of the cardiac cycle . 
accordingly , low - dose pea coronary 64 - slice cta has the important advantage of allowing the follow - up of patients after stent implantation and coronary artery bypass grafts . 
first , as an axial scan mode , the table is stationary during data acquisition of pulmonary artery ( pa ) cta compared with the constant movement of the reh technique during the scan . second , the shorter scan time of pa - cta permit less image degrading due to high and unstable heart rate . due to a combination of partial volume averaging and beam - hardening , the blooming artefacts create a spill - over effect from higher ct attenuation voxels to adjacent lower voxels . 
these two ct artefacts obscured the coronary artery lumen , degraded visibility of in - stent restenosis , produced the artificial lumen narrowing and increased the evaluated thickness of stent struts and in - stent lumen attenuation . 
the visibility of in - stent restenosis with 3.5 - mm stent calibre was significantly better than with the 3 mm , and the artificial lumen narrowing with 3.5 mm was higher than that with 3 m this indicated that coronary artery radiol med ( 2011 ) 116 : 189196 lumen evaluation with bigger stent calibre is more credible than with smaller stent calibre . 
 for pea 64 - slice coronary cta , a low and stable heart rate is an important factor in obtaining high - quality images . the reported ideal heart rate is 56.963 bpm for pea acquisition [ 6 , 16 ]  . 
in our study , there was no difference of restenosis visibility between 50 , 60 and 70 bphowever , there is no accepted heart rate range for pea technique or for in - stent lumen evaluation . 
image quality was degraded by stents with thicker struts ( > 0.14mm ) and stents with smaller diameter ( 3.0 mm ) [ 17 , 18 ] .we tested only one type of stent , the cypher , with a 3and 3.5 - mm inner diameter , 13and 23 - mm length and 0.14 - mm strut thickness . 
second , artificial restenosis consisted of polypropylene with a homogeneous density of approximately 60 hu , whereas in vivo intimal hyperplasia and atheromatous plaque are often heterogeneous . that may limit the extent of our findings in humans . 
gatta2 1unit operativa di senologia , ospedale san paolo , contrada capo scardicchio , bari , italy 2sezione di radiodiagnostica , dipartimento di internistica clinica e sperimentale , seconda universit degli studi di napoli , piazza miraglia 2 , napoli , italy correspondence to : g . 
this study sought to evaluate the accuracy of vacuum - assisted biopsy ( vab ) in the diagnosis of atypical ductal hyperplasia ( adh ) by determining the rate of vab underestimation compared with de nitive histology . 
patients with a diagnosis of adh associated with other lesions ( lobular intraepithelial neoplasia , papilloma ) , atypical lobular hyperplasia , lobular carcinoma in situ and any lesions with a microhistological diagnosis other than adh were excluded . 
mammographic appearance of lesions was as follows : 152 mostly clustered microcalci cations ( 86% ) ; ve opacities with microcalci cations ( 3% ) ; 12 single opacities ( 3% ) ; and eight parenchymal distortions ( 4% ) , of which ve were without and three were with microcalci cations . 
the decision to either perform or not perform surgery was based on combined analysis of the following parameters : patient age ; risk factors in the patients history ; mammographic riassunto obiettivo . 
sono state incluse nel nostro studio 177 pazienti con diagnosi vab di adh pura ; sono state escluse le pazienti con diagnosi di adh associata ad altre lesioni ( neoplasia intraepiteliale lobulare [ lin ] , papilloma ) , iperplasia lobulare atipica ( alh ) , carcinoma lobulare in situ ( lcis ) e tutti le lesioni con diagnosi microistologiche differenti . 
la tipologia mammogra ca di tali lesioni stata la seguente : 152 microcalci cazioni per la maggior parte in cluster ( 86% ) ; 5 opacit con microcalci cazioni ( 3% ) ; 12 opacit singole ( 3% ) ; in ne , 8 distorsioni parenchimali ( 4% ) di cui 5 senza microcalci cazioni e 3 con microcalci cazioni . 
the most relevant parameters affecting the decision to proceed to surgical excision were lesion diameter > 7 mm on mammography , > 2 adh foci , incomplete removal of the calci cations and a family and / or personal history of breast cancer . 
dai dati emersi nel nostro studio i parametri pi rilevanti per la decisione allexeresi della lesione sono stati : diametro mammogra co > 7 mm , estensione delladh > 2 foci , incompleta rimozione delle calci cazioni ed anamnesi familiare e / o personale di neoplasia . 
however , the growing numbers of asymptomatic women self - referring for periodic mammography and the advent of screening programmes have increased the detection rate of subclinical or nonpalpable breast lesions that appear suspicious on diagnostic imaging [ 1 , 2 ]  . 
before the advent of mammography as a screening test , breast carcinoma in situ was diagnosed in only 5% of all cases of breast cancer , and the lesions were usually palpable . 
in parallel with the increased detection rate of subclinical lesions , there has been a higher diagnostic incidence of high - risk proliferative lesions , including atypical ductal hyperplasia ( adh ) [ 3 ]  . 
with the recent world health organisation ( who ) 2003 pathological classi cation , tavassoli introduced the term ductal intraepithelial neoplasia ( din ) to cover the possible changes that lead from epithelial hyperplasia to invasive carcinoma , in agreement with the commonly accepted progression model of breast cancer whereby adh , ductal carcinoma in situ ( dcis ) and in ltrating il carcinoma della mammella la pi frequente malattia tumorale nella popolazione femminile . 
tuttavia , con il costante aumento di donne asintomatiche che spontaneamente e periodicamente si sottopongono alla mammogra a e con lavvento dei programmi di screening organizzato , si determinato un sempre pi frequente riscontro di lesioni mammarie sospette alle metodiche strumentali senza un corrispettivo clinico ( lesioni infracliniche ) , vale a dire lesioni non palpabili [ 1 , 2 ]  . 
prima dellavvento della mammogra a soprattutto come esame di screening , il carcinoma in situ della mammella rappresentava solo il 5% di tutti i tumori mammari e tali lesioni erano comunemente palpabili . 
in contemporanea al maggior riscontro diagnostico di lesioni infracliniche , c stata una sempre maggiore incidenza diagnostica di lesioni proliferative della mammella ad alto - rischio tra cui appunto liperplasia duttale atipica ( adh ) [ 3 ]  . 
considerando che la diagnosi precoce uno degli elementi principali in grado di modicare la prognosi del carcinoma mammario , appare chiaro come tale obiettivo risulti essere una s da sia per il radiologo senologo che per lanatomopatologo . 
tale lesione , considerata un potenziale precursore del cancro invasivo , deve pertanto essere accuratamente e precocemente identi cata al ne di de nirne al meglio il suo signi cato prognostico . 
 con la recente classi cazione anatomo - patologica world 278 radiol med ( 2011 ) 116 : 276291 ductal carcinoma ( idc ) form a continuum of proliferative breast disease [ 4 ]  . 
in the eld of percutaneous biopsy , in 1995 , a particular technique known as vacuumassisted biopsy ( vab ) was proposed that uses a vacuum aspiration system to sample several cores with a single needle pass . the aim of our study was to evaluate the accuracy of vab in adh diagnosis by determining the rate of vab underestimation in comparison with nal histology ( the gold standard ) and to identify any imaging criteria that might help determine appropriate patient management . materials and methods we retrospectively reviewed 1 , 776 percutaneous vab procedures conducted for equivocal / suspicious subclinical breast lesions visible only at mammography on 1 , 765 patients ( age range 3276 years ) between november 1999 and january 2008 all patients had previously undergone mammography in the craniocaudal and oblique projections , supplemented by magni cation views of microcalci cation clusters and / or spot compression views of suspicious ndings . 
in six patients , sampling was bilateral and in ve two biopsies were obtained in different areas of the same breast . the level of suspicion of all lesions had preliminarily been assessed according to the breast imaging reporting and data system ( bi - rads ) classi cation [ 5 , 6 ]  . 
in all cases , percutaneous biopsy was performed with a digital fischer stereotactic prone table unit and a mammotome device ( ethicon endo - surgery , breast care , norstedlt , germany ) , which allows multidirectional ( 360 ) sampling of the lesion with forced aspiration ( 2325 mmhg )  . 
exclusion criteria were : a diagnosis of adh associated with other lesions [ adh with lobular intraepithelial neoplasia ( lin ) , papillomas ] ; atypical lobular hyperplasia ( alh ) ; lobular carcinoma in situ ( lcis ) ; any diagnosis other than adh . 
mammographic pattern heath organization ( who ) 2003 tavassoli [ 4 ] introduce un nuovo termine , quello di neoplasia duttale intraepiteliale ( din ) , per racchiudere in un unico termine quelle possibili lesioni che dalliperplasia epiteliale giungono al carcinoma invasivo secondo un modello evolutivo ormai comunemente accettato per il quale ladh , il carcinoma duttale in situ ( dcis ) ed il carcinoma duttale in ltrante ( cdi ) potrebbero rappresentare un continum di una malattia proliferativa della mammella [ 4 ]  . 
nellambito della biopsia percutanea , nel 1995 stata proposta una particolare tecnica di prelievo istologico percutaneo , chiamata vacuum - assisted ( vab ) , che consente con ununica inserzione dellago il prelievo di pi frustoli tissutali tramite un sistema di aspirazione interna . scopo del nostro lavoro stato dunque quello sia di valutare laccuratezza della vab nella diagnosi di iperplasia duttale atipica , calcolando dunque la percentuale di sottostime diagnostiche della metodica stessa rispetto allesame istologico de nitivo ( gold standard ) , sia di cercare eventuali criteri dimaging utili per il corretto management di tali pazienti . materiali e metodi stata effettuata unanalisi retrospettiva di 1776 biopsie percutanee vacuum assisted per lesioni mammarie dubbie / sospette infracliniche , visibili solo mammogra camente , eseguite nel periodo compreso da novembre 1999 a gennaio 2008 in 1765 pazienti , di et compresa tra 32 e 76 anni . 
 tutte le pazienti avevano precedentemente eseguito una mammogra a nelle due proiezioni cranio - caudale ed obliqua completate da ingrandimenti mirati sui cluster di microcalci cazioni e / o particolari in compressione mirata su altri reperti sospetti . 
in 6 pazienti il prelievo era stato bilaterale ed in altre 5 erano stati eseguiti due prelievi , in zone differenti della stessa mammella . le lesioni erano state preliminarmente valutate , relativamente al grado sospetto , in accordo con la classi cazione breast imaging reporting and data system ( bi - rads ) [ 5 , 6 ]  . 
 in tutti i casi per la microbiopsia percutanea era stato utilizzato un tavolo prono stereotassico digitale fischer associato a sistema mammotome ( ethicon endo - surgery , breast care , norstedlt , germania ) , che permette la campionatura multidirezionale ( 360 ) della lesione con aspirazione forzata ( 23 25 mmhg )  . 
in tutti i casi era stata posizionata sullarea bioptizzata una clip metallica amagnetica per obiettivare lesatta sede del prelievo . il nostro criterio di inclusione stato la diagnosi di adh puro ; i nostri criteri di esclusione sono stati : diagnosi di adh associato ad altre lesioni ( adh con neoplasia intraepiteliale lobulare [ lin ] , papillomi ) ; iperplasia lobulare atipica ( alh ) ; carcinoma lobulare in situ ( lcis ) e qualsiasi altra diagnosi diversa dalladh . 
la tipologia mammogra a di tali lesioni era stata la seguente : 152 microcalci cazioni per la maggior parte in cluster ( 86% ) ; 5 opacit con microcalci cazioni ( 3% ) ; 12 opacit singole ( 3% ) ; 8 distorsioni parenchimali ( 4% ) di cui 5 senza microcalci cazioni e 3 con microcalci cazioni . tutte le biopsie effettuate avevano fornito materiale adeguato per la diagnosi ( 100% )  . 
le pazienti in esame sono state successivamente suddivise in due gruppi : il primo costituito dalle pazienti inviate allintervento chirurgico ; il secondo invece dalle pazienti inviate a follow - up , prima a sei mesi e poi , se negativo , annuale . 
the purpose of this analysis was to identify parameters that might help determine the most appropriate management of patients with a vab diagnosis of adh . similarly , in patients referred for follow - up care , we analysed both the rate of lesions showing progression over time and the imaging , clinical and microhistological features of these lesions to determine the existence of parameters predicting lesion progression . statistical analysis the parameters age , personal and / or family history , bi - rads assessment , lesion diameter , complete or incomplete excision at vab and microhistological extent ( or > 2 adh foci ) were compared in cases underestimated and not underestimated at vab using the two - tailed t and chi - square tests . 
per il gruppo di pazienti sottoposte ad intervento chirurgico stato confrontato , il giudizio microistologico con quello fornito dallistologia de nitiva , considerata come gold standard , al ne di valutare le sottostime diagnostiche con mammotome . 
nei casi sottostimati stata effettuata successivamente unulteriore analisi retrospettiva delle caratteristiche radiologiche e microistologiche ; in particolare stato valutato retrospettivamente come parametro microistologico , fornito pertanto dallanatomopatologo , lestensione delladh allinterno dei dotti e / o lobuli , vale a dire il numero di foci di adh presenti al loro interno in una sezione , suddividendo pertanto le pazienti in due sottogruppi : pazienti con adh2 foci e pazienti con adh > 2 foci ( tabella 2 )  . 
il ne di tale analisi stato di valutare parametri utili per il management dei pazienti con diagnosi vab di adh . con le medesime nalit , anche per il gruppo di pazienti inviate a stretto monitoraggio clinico - strumentale sono state invece valutate sia la percentuale di lesioni evolute nel tempo sia le caratteristiche radiologiche , anamnestiche e microistologiche delle lesioni evolute , al ne dunque di valutare se esistono parametri predittivi di uneventuale evoluzione nel tempo . analisi statistica i parametri et , storia personale e familiare , giudizio birads , diametro delle lesioni , exeresi completa o incompleta alla vab , estensione microistologica ( adh2 o > 2 foci ) sono stati confrontati nelle pazienti sottostimate e non sottostimate alla vab e nelle pazienti stabili ed evolute con t test a due code e 2 . 
stato calcolato il rischio relativo delle pazienti sottoposte a intervento chirurgico e delle pazienti sottoposte a follow - up con lesioni > 15 mi parametri et , storia personale e familiare , giudizio bi - rads , diametro delle lesioni , exeresi completa o incompleta alla vab , estensione microistologica ( adh2 o > 2 foci ) sono stati confrontati nelle pazienti stabili o evolute al follow - up con test t di student a due code e test del 2 . radiol med ( 2011 ) 116 : 276291 fig . 
the patient was referred for surgery owing to the nonexcision of the microcalci cations at vacuumassisted biopsy and microhistological suspicion [ atypical ductal hyperplasia ( adh ) > 2 foci ]  . 
successivamente , dallanalisi retrospettiva delle caratteristiche radiologiche e microistologiche di ogni singola lesione sottostimata emerso che per ladh , i fattori di rischio di malignit signi cativi sono stati ( tabella 3 ) : il giudizio radiologico espresso : nei casi sottostimati il giudizio radiologico bi - rads 4 - 5 stato assegnato nell84% dei casi ( 16 / 19 )  . 
tuttavia anche nel gruppo di radiol med ( 2011 ) 116 : 276291 eter > 15 mm of a total of 46 / 98 patients with mammographic extent 1.5 cm referred for surgery . 
only 6 / 72 follow - up patients ( 8% ) showed a change in mammographic pattern , consisting in all cases of an increase in the number of microcalcications . 
the lesion had progressed to idc in four cases ( 66.7% ) and dcis in two ( 33.3% ) over a mean interval of 56 months ( 2482 months )  . 
a comparative analysis of the radiological and microhistological features of progressed adh lesions ( table 4 ) revealed that parameters predicting malignant disease were , even in this case , the combination of bi - rads category 45 , which was present in 5 / 6 cases ( 83.3% ) ; maximum lesion diameter and > 2 adh foci . 
furthermore , in 5 / 6 cases of lesion progression ( 83.3% ) , excision at vab had been incomplete , a parameter that increases the risk of subsequent progression . in patients referred for surgery , comparison of the main parameters ( age , personal and / or family history , bi - rads assessment , lesion diameter , complete or incomplete excision at vab , microhistological extent or > 2 foci ) between underestimated and nonunderestimated lesions revealed a statistically signi cant difference with regard to patient age ( p = 0.034 ) , lesion extent ( p = 0.007 ) and complete or incomplete lesion excision ( p = 0.010 , table 5 )  . 
in unanalisi comparativa delle caratteristiche radiologiche e microistologiche delle lesioni di adh evolute nel tempo considerato ( tabella 4 ) emerso che i parametri predittivi di malignit sono stati rappresentati , anche in questo caso , dalla combinazione del giudizio radiologico del tipo bi - rads 4 - 5 , presente in 5 / 6 casi ( 83 , 3% ) , diametro massimo della lesione 284 radiol med ( 2011 ) 116 : 276291 lesion extent ( p = 0.001 ) and complete or incomplete lesion excision ( p = 0.006 , table 6 )  . discussion and conclusions dcis is a heterogeneous entity from the point of its histological , molecular and radiological features [ 8 ]  . 
a , c , parenchymal distortion on the internal equator region , with a diameter of 1.5 cm and intralesional lobular microcalci cations ( breast imaging reporting and data system 4 )  . 
a , c distorsione parenchimale a sede equatoriale interna , del diametro di 1 , 5 cm , con microcalci cazioni lobulari intralesionali ( bi - rads 4 )  . 
in particolare lestensione mammogra ca media nei casi evoluti stata di 2 , 1 cnessuna lesione con diametro < 1 cm evoluta nel tempo ( diametro medio delle lesioni 1 , 6 cm ) ed in 5 / 6 casi era presente un adh > 2 ( 83 , 3% )  . 
inoltre , in 5 / 6 lesioni evolute ( 83 , 3% ) lexeresi alla vab era stata incompleta , parametro che pertanto , aumenta il rischio di successiva evoluzione . 
 nelle pazienti sottoposte ad intervento chirurgico , il confronto dei principali parametri ( et , storia personale e familiare , giudizio bi - rads , diametro della lesione , exeresi completa o meno alla vab , estensione microistologica , 2 foci o > 2 foci ) nelle lesioni sottostimate e nelle lesioni non sottostimate ha evidenziato una differenza statisticamente signi cativa relativa allet della paziente ( p = 0 , 034 ) , allestensione della lesione ( p = 0 , 007 ) e allexeresi completa o meno della lesione ( p = 0 , 010 ) ( tabella 5 )  . 
nelle pazienti sottoposte a follow - up il confronto dei principali parametri ( et , storia personale e familiare , giudizio bi - rads , diametro della lesione , exeresi completa o meno alla vab , estensione microistologica , 2 foci o > 2 foci ) nelle lesioni stabili e nelle lesioni evolute ha evidenziato una differenza statisticamente signi cativa relativa alla storia familiare ( p = 0 , 001 ) , allestensione della lesione ( p = 0 , 001 ) e allexeresi completa o meno della lesione ( p = 0 , 006 ) ( tabella 6 )  . discussione e conclusioni il cdis si con gura come unentit eterogenea dal punto di vista delle sue caratteristiche istologiche , molecolari e radiologiche [ 8 ]  . 
accettando oramai un modello di tipo evolutivo del carcinoma mammario , il cdis non compare improvvisamente come tale , ma insorge e si accresce nel contesto di un processo di iperplasia delle cellule epiteliali , accompagnato dalla comparsa di atipie cellulari ( iperplasia atipica , adh )  . 
 utile sottolineare , che sebbene esista un modello progressivo di evoluzione del carcinoma mammario ormai unanimemente accettato , non bisogna dimenticare che non tutti i carcinomi in ltranti seguono questo tipo di storia naturale : alcuni potrebbero avere una fase intraduttale molto breve e quindi divenire invasivi prima che la fase in situ possa venire identi cata , altri potrebbero insorgere ab initio come invasivi [ 9 ]  . 
la precisa distinzione tra adh e cdis dunque importante in quanto ladh considerato come un fattore di rischio per lo sviluppo di carcinoma invasivo , mentre cdis un precursore diretto del cdi e necessita sempre dellexeresi chirurgica . negli ultimi anni lintroduzione del mammotome ( vab ) , vale a dire di sistema di prelievo microistologico multidirezionale con aghi trancianti dotati di un dispositivo aspirante sottovuoto , ha migliorato laf dabilit e la sensibilit delle micro biopsie . 
 however , it is important to recall that , although the progression model of breast cancer has been universally accepted , not all in ltrating carcinomas follow this progression in their natural history : some may have a very short intraductal phase and become invasive before the in - situ phase is identi ed , whereas others may be invasive from the beginning [ 9 ]  . 
precise distinction between adh and dcis is therefore important in that adh is considered a risk factor for the development of invasive carcinoma , whereas dcis is a direct precursor to idc and always requires surgical excision . the recent introduction of the mammotome vab device for multidirectional microhistological biopsy with core needles equipped with a vacuum aspiration system has improved the reliability and sensitivity of core biopsy . 
 in fact , the reported diagnostic accuracy of vab is fully comparable with that achieved by surgical biopsy with marker clips , a method that has been widely used for many years . 
in the case of small lesions , especially those only visible at mammography such as foci of microcalci cations , small opacities or areas of parenchymal distortion accuracy is de nitely higher compared with core needle biopsy thanks to the presence of the aspiration system that allows larger tissue cores ( approximately three times larger ) to be collected , needle calibre being equal [ 10 , 11 ]  . tura , del tutto confrontabile con i dati della biopsia chirurgica su repere , metodica ampiamente utilizzata per lunghi anni . 
nel caso di lesioni di piccole dimensioni , in particolare quelle visibili solo mammogra camente , quali focolai di microcalci cazioni , piccole opacit o aree di distorsione parenchimale , laccuratezza decisamente maggiore rispetto alla core biopsy , grazie alla presenza dei dispositivi di aspirazione che consentono di ottenere , a parit di calibro , frustoli di maggiore volume ( circa 3 volte ) [ 10 , 11 ]  . tuttavia , nonostante laf dabilit diagnostica della metodica , lescissione chirurgica ancora attualmente raccomandata dopo una diagnosi di adh alla vab a causa del rischio di upgrade a cdis o a cancro invasivo allistologia de nitiva ; la percentuale di sottostime riportate in letteratura variano infatti dal 11% al 87% [ 1221 ]  . 
lestrema variabilit delle percentuali di sottostima riportate in letteratura legata da un lato alla diversa metodologia utilizzata ed al diametro dellago utilizzato , dallaltro allesperienza dellanatomopatologo ; percentuali di sottostime pi basse sono state infatti riscontrate sia con lutilizzo dei sistemi vab che con lutilizzo di aghi trancianti di pi grosso calibro ( 11 g o 9 g piuttosto che 14 g ) [ 18 , 2227 ] , accorgimenti che permettono campionamenti di numero e dimensioni ( inteso come peso del frustolo ) maggiori . 
un recente studio di tonegutti e girardi [ 28 ] riporta una sottostima diagnostica di adh della vab rispetto allistologia de nitiva del 19% ( 5 / 27 casi ) , dato perfettamente concordante radiol med ( 2011 ) 116 : 276291 fig . 
istologia de nitiva : iperplasia duttale atipica . however , despite the methods diagnostic reliability , surgical excision is still recommended after a vab diagnosis of adh owing to the risk of an upgrade to dcis or to invasive cancer at nal histology . 
lower underestimation rates have been found both with vab systems and with larger - core needles ( 11or 9 - gauge rather than 14 - gauge ) [ 18 , 2227 ] , which allow collection of more and larger ( intended as weight of the core ) tissue cores . 
a recent study by tonegutti and girardi reported the rate of underestimation of adh by vab compared with nal histology to be 19% ( 5 / 27 ) , which is perfectly in line with the results obtained in our series [ 28 ]  . our study aimed to retrospectively analyse the results obtained with mammotome biopsy to determine not only the possible underestimates but also whether a subset of patients with an adh diagnosis could be identi ed in whom surgical excision could be omitted . 
the current trend when faced with adh is to proceed to surgical excision , although some authors have attempted to establish the conditions that mandate excision and those that warrant follow - up . 
 [ 19 ] , the presence of one of the following parameters should prompt surgical excision : ( a ) personal history of breast cancer , ( b ) lesion diameter > 1 cm , ( c ) presence of adh in the last fragment removed con i risultati da noi ottenuti [ 28 ]  . 
 il nostro lavoro si proposto di analizzare in maniera retrospettiva i risultati ottenute su biopsie con mammotome al ne di individuare , oltre alle sottostime diagnostiche , se esiste un sottogruppo di pazienti con diagnosi di adh che potrebbe non esser sottoposto a escissione chirurgica ; per tale lesione lorientamento attuale infatti quello dellexeresi chirurgica , sebbene alcuni autori abbiano tentato di dettare delle condizioni in cui lexeresi necessaria , riservando il follow - up nei rimanenti casi . 
 [ 29 ] , only patients with complete removal of adh at vab or those > 70 years without additional risk factors were referred for follow - up . in our experience , although personal and / or family history was among the criteria for surgical referral , the parameter was not in uential in the group of underestimates in that only 1 / 19 ( 5% ) underestimated patients had a previous history of breast cancer . 
this parameter was instead in uential in the group of patients referred for follow - up who were found to have progressed to malignancy ( 50% of cases )  . 
furthermore , the parameters predictive of malignancy in the two groups of patients in our study were > 2 adh foci , larger mammographic lesion extent , bi - rads category 45 and incomplete lesion excision at vab . 
 [ 30 ] , in a study of 24 cases of adh at core biopsy , did not identify any case of underestimation among cases with only one or two foci of adh . 
in contrast to ely and sneige , our study identi ed an underestimation rate of 8.7% ( 7 / 80 cases of 2 adh foci ) among lesions with 2 adh foci ; this parameter also had a low incidence among patients referred for follow - up who showed lesion progression ( 1 / 6 , 17% )  . 
the combined analysis of the different radiological and microhistological features of underestimated adh lesions shows that the seven underestimated cases with 2 foci had suspicious radiological features , such as a larger mammographic extent and / or missed excision at vab ( table 3 )  . 
a nding of bi - rads category 45 alone , although very high in the group of underestimates ( 84.2% ) , was not a signi cant parameter in that a high percentage of patients undergoing vab ( 96% ) had been classi ed as bi - rads 45 ( 132 / 144 adh ) ; additionally , the incidence of this parameter was the same ( 85% ) in cases con rmed by nal histology . our study was therefore unable to identify any single radiological criterion predictive of malignancy . 
 [ 20 ] and other authors [ 18 , 21 , 31 , 32 ] reported so carcinoma mammario ; tale dato si invece dimostrato in uente nel gruppo di pazienti che sottoposte a follow - up hanno mostrato una successiva evoluzione della lesione in senso maligno ( 50% dei casi )  . 
nel nostro studio inoltre , i parametri predittivi di malignit nei due gruppi di pazienti sono stati : numero di foci di adh maggiore di 2 , maggiore estensione mammogra ca della lesione , giudizio radiologico bi - rads 4 - 5 e incompleta exeresi della lesione stessa alla vab . 
 [ 30 ] , su un totale di 28 adh non riportano alcun upgrade per lesioni limitate ad 1 o 2 foci usando aghi da 11 e 14 gauge con tecnica vab . 
 [ 20 ] , la sottostima diagnostica per lesioni con adh2 foci stata dell8 , 7% ( 7 / 80 casi di adh2 foci ) ; tale parametro stato comunque basso anche nel gruppo di pazienti che , sottoposte a follow - up , hanno mostrato unevoluzione nel tempo : solo in 1 / 6 di tali lesioni ( 17% ) aveva adh2 foci . 
tuttavia , nellanalisi combinata tra le varie caratteristiche radiologiche e microistologiche delle lesioni sottostimate di adh si pu evincere che i 7 casi di adh2 foci sottostimati possedevano comunque caratteristiche radiologiche sospette , quali una pi estesa lesione mammogra ca e / o mancata exeresi della stessa alla vab ( tabella 3 ) ; analoga osservazione per la singola lesione con adh2 foci evoluta nel tempo ( tabella 4 )  . 
il giudizio radiologico bi - rads 4 - 5 , per quanto sia stato elevato nel gruppo di pazienti sottostimate ( 84 , 2% ) , non un parametro signi cativo da solo , in quanto unalta percentuale delle lesioni sottoposte a vab , pari al 96% , era stata classi cata come bi - rads 4 - 5 ( 132 / 144 adh ) ; inoltre anche nel gruppo di pazienti confermate allistologia de nitiva tale parametro ha avuto la stessa incidenza ( 85% )  . 
 [ 20 ] , cos come altri autori [ 18 , 21 , 31 , 32 ] , hanno riportato nei loro studi unassenza di upgrade delladh per tutte le lesioni completamente escisse alla vab ; nel nostro studio invece , una percentuale seppur bassa , pari al 26% ( 5 / 19 ) , di lesioni completamente escisse hanno dimostrato un successivo upgrade delladh ; tuttavia , in unanalisi combinata emerge che ciascuna di queste 5 lesioni aveva comunque un numero di foci di adh > 2 . 
in our study , by contrast , a low percentage ( 26% , 5 / 19 ) of completely excised lesions showed subsequent upgrade of adh ; however , the combined analysis demonstrated that each of these ve lesions had > 2 adh foci . 
similarly , only 1 / 6 ( 16.7% ) lesions that subsequently showed progression had been removed completely . the combined analysis of all parameters at our disposal shows that the extent of adh is an important indicator for lesions 7 mm and < 15 mm in diameter . 
however , the extent of adh is no longer a relevant parameter with lesions 15 mm in diameter , where surgical excision is prompted by the lesion diameter itself regardless of adh extent . 
this nding is statistically signi cant despite the wide ci ( rr in followup patients 12.17 ; 95% ci 3.1047.73 ) , which re ects only the small size of our study population . 
in con rmation of this , 80% of lesions that had progressed at follow - up also had a diameter 15 mconversely , as none of the underestimated lesions or any adh that progressed had a diameter < 0.7 cm , regardless of the number of adh foci , we considered this parameter to be protective against a possible upgrade . 
in conclusion , although surgical excision is strongly recommended for adh diagnosed at vab with an 11 - gauge needle , it is reasonable to believe that follow - up could constitute a valuable alternative for a subset of patients . in our study , the most relevant parameters leading to a decision to treat the lesion surgically were , in order of importance : ( a ) mammographic lesion diameter > 7 mm ; ( b ) adh extent > 2 ; ( c ) incomplete removal of calci cations ; ( d ) and personal / family history of breast cancer . 
generally , the presence of at least two of these parameters is suf cient to decide on a surgical referral , whereas a high grade of cellular atypia must be considered in itself a parameter determining excision . 
il nostro risultato statisticamente signi cativo nonostante lampio intervallo di con denza ( rr pazienti in follow - up 12 , 17 ic 95% : 3 , 1047 , 73 ) legato esclusivamente alla scarsa numerosit del campione . 
inoltre , il diametro medio di tutte le lesioni di adh stato infatti di 1 , 3 cm versus 1 98 cm per le lesioni di adh sottostimate ; a conferma di ci , anche le lesioni evolute nel follow - up avevano per l80% un diametro 15 mviceversa , poich nessuna lesione sottostimata n nessuna lesione di adh evoluta aveva diametro inferiore a 0 , 7 cm , indipendentemente dal numero di foci di adh , abbiamo ritenuto tale parametro protettivo per un eventuale upgrade . 
in conclusione sebbene lexeresi chirurgica sia attualmente raccomandata per adh diagnosticato alla vab con ago da 11 gauge , si pu ragionevolmente ritenere che il follow - up potrebbe essere valida alternativa per un ristretto gruppo di pazienti . 
 nel nostro studio i parametri pi rilevanti per la decisione allexeresi chirurgica della lesione , sono stati , in ordine dimportanza i seguenti : diametro mammogra co della lesione > 7 mm , estensione delladh > 2 , incompleta rimozione delle calci cazioni ed in ne storia personale / familiare di neoplasia . 
in genere suf ciente che siano presenti almeno due dei suddetti parametri per decidere di inviare la paziente ad exeresi chirurgica , mentre lelevato grado di atipia deve essere da solo considerato parametro decisivo per lexeresi . 
poletti2 1area di radiologia , irstistituto romagnolo studio e cura dei tumori , meldola , forl , italy 2unit operativa di pneumologia interventistica , ospedale pierantoni - morgagni , forl , italy 3istituto di anatomia patologica , universit di verona , verona , italy 4unit operativa di anatomia patologica , ospedale pierantoni - morgagni , forl , italy 5istituto di radiologia , universit campus bio - medico , roma , italy 6unit operativa di radiologia , azienda ospedaliera santa maria di terni , italy correspondence to : s . 
piciucchi , e - mail : s.piciucchi@alice.it received : 13 november 2009 / accepted : 6 may 2010 / published online : 10 february 2011 springer - verlag 2010 abstract purpose . 
transbronchial biopsy was performed in all but four patients ( one case of alveolar haemorrhage and three cases of lipoid pneumonia ) in whom the diagnosis was established with bal . assessment of the hrct images revealed the following patterns : noncardiogenic pulmonary oedema ( n = 13 ) ; organising pneumonia ( op ) ( n = 9 ) ; hypersensitivity riassunto obiettivo . 
tutti i pazienti erano sottoposti a broncoscopia , con biopsia transbronchiale o broncolavaggio ( bal ) in seguito ad una hrct che poneva il sospetto di dr - ild . due radiologi ( un senior ed un junior ) hanno riportato in cieco i dati riguardanti i singoli reperti , la distribuzione e il pattern predominante alla hrct . 
quarantadue pazienti sono stati inclusi nello studio ( 25 maschi ; 17 femmine ; range di et 2084 anni )  . la biopsia transbronchiale stata effettuata in tutti i casi , fatta eccezione per un caso di emorragia alveolare e tre casi di polmonite lipoidea , in cui la diagnosi stata raggiunta con il bal . 
le interpretazioni tc includevano i seguenti pattern : edema polmonare non cardiogeno radiol med ( 2011 ) 116 : 246263 pneumonitis ( hp ) ( n = 2 ) ; alveolar haemorrhage ( ah ) ( n = 2 ) ; nonspecific interstitial pneumonia ( nsip ) ( n = 5 ) ; lipoid pneumonia ( lp ) ( n = 1 ) ; sarcoid - like pattern ( n = 1 )  . cytohistological diagnosis revealed diffuse alveolar damage ( dad ) in 11 patients , op in seven , hp in three , ah in three , chronic interstitial pneumonia ( cip ) in eight , lp in three and pseudosarcoidosis in one . 
in cases in which its specificity was low , hrct was nonetheless useful for biopsy planning and clinicalradiological monitoring after discontinuation of the drug treatment . keywords pulmonary toxicity interstitial lung diseases hrct transbronchial biopsy bronchoscopy ( n = 13 ) ; organizing pneumonia ( op ) ( n = 9 ) ; hypersensitivity pneumonitis ( hp ) ( n = 2 ) ; alveolar haemorrage ( ah ) ( n = 2 ) ; non specific interstitial pneumonia ( nsip ) ( n = 5 ) ; lipoid pneumonia ( lp ) ( n = 1 ) ; sarcoid - like pattern ( n = 1 )  . 
la diagnosi anatomopatologica ha mostrato : danno alveolare diffuso ( dad ) in 11 pazienti , op in 7 , hp in 3 , ah in 3 , polmonite interstiziale cronica ( cip ) in 8 , lp in 3 ; pseudosarcoidosi in 1 . 
dividendo i farmaci in antineoplastici e nonantineoplastici , i pattern pi frequenti sono stati cip ( n = 6 ) ; dad ( n = 2 ) ; op ( n = 2 ) per il gruppo degli antineoplastici . 
nei casi in cui la hrct ha mostrato bassa specificit , stata utile nel planning di una corretta biopsia e nel monitoraggio clnico - radiologico dopo la sospensione del farmaco . parole chiave tossicit polmonare malattia interstiziale del polmone hrct biopsia transbronchiale broncoscopia introduction introduzione drug - related respiratory disease is a major cause of morbidity and mortality , and the relationship between the use of different pharmaceutical drugs and lung disease is increasingly recognised [ 1 ]  . 
many agents have been recognised as being toxic to the pulmonary parenchyma [ 24 ]  . the diagnosis of drug - related interstitial lung disease ( drild ) involves three elements : clinical suspicion , differentiation from other respiratory diseases with similar presentation [ by highresolution computed tomography ( hrct ) and clinical tests ] and a compatible histological pattern . symptoms are often nonspecific and include rapidly developing dyspnoea and a dry , unproductive cough [ 3 , 5 ]  . 
the radiography and ct appearance of the various forms of drild have been variously described in the literature [ 7 , 8 ]  . ct enables precise assessment of the presence , pattern and distribution of parenchymal and airway abnormalities and has higher sensitivity compared with chest radiography , which may be normal in the early stages of dr - ild [ 8 ]  . the radiological manifestations of dr - ild correspond to the underlying histological findings : nonspecific interstitial pneumonia ( nsip ) , usual interstitial pneumonia ( uip ) , hypersensitivity pneumonia ( hp ) , pulmonary oedema , le patologie respiratorie da farmaci rappresentano unimportante causa di morbilit e mortalit . 
la diagnosi di tossicit polmonare da farmaci ( dr - ild ) coinvolge tre elementi : sospetto clinico , la distinzione di patologie respiratorie con manifestazioni simili ( mediante tomografia computerizzata [ tc ] ad alta risoluzione e test clinici ) e infine un pattern istologico . 
la tc offre una precisa valutazione della presenza , pattern e distribuzione delle alterazioni parenchimali e delle vie aeree , con una sensibilit maggiore rispetto alla radiografia , potendo infatti , questultima , essere normale negli stadi iniziali di dr - ild [ 8 ]  . 
la manifestazione radiologica di una tossicit polmonare da farmaci pu avere diversi corrispettivi istologici : polmonite interstiziale non specifica ( nsip ) , usual interstitial pneumonia ( uip ) , polmonite da ipersensibilit 248 radiol med ( 2011 ) 116 : 246263 organising pneumonia ( op ) and alveolar haemorrhage ( ah )  . 
the diagnosis of these patterns has often been obtained by surgical biopsy [ 4 ]  . ( hp ) , edema polmonare polmonite organizzativa ( op ) e emorragia alveolare diffusa ( ah )  . 
spesso la diagnosi di tali pattern stata riservata alla biopsia chirurgica [ 4 ]  . the purpose of this study was to determine the sensitivity and specificity of high - resolution ct ( hrct ) compared with the cytohistological diagnosis provided by bronchoscopy used as the gold standard with the aim of identifying what proportion of patients could be diagnosed with dr - ild by using semi - invasive tests and to what extent ct is specific as well as sensitive in this context . la proposta di questo studio cercare di individuare la specificit e la sensibilit della tc ad alta risoluzione considerando come termine di confronto la diagnosi citoistologica fornita dalla broncoscopia . 
la finalit di questo studio stato infatti cercare di individuare in quale percentuale di pazienti sarebbe effettivamente possibile porre diagnosi di dr - ild con manovre semi - invasive e quanto la tc rappresenta unindagine specifica oltre che sensibile a tal proposito . materials and methods patients patients were included into this prospective study protocol between september 2002 and may 2007 , and the study was approved by the local ethics committee . 
 imaging technique and image analysis non - antineoplastici , causa di tossicit polmonare . sono stati inclusi nello studio i farmaci antineoplastici e hrct ( light speed , ge medical system , milwaukee wi , usa ; aquilon , toshiba ) was performed with volumetric technique , a collimation thickness of 1 or 1.5 mm and scans extending from the lung bases to apices . 
images were reconstructed with a high - spatial - frequency algorithm ( kernel b70 ) with appropriate settings and viewing window ( level 700 hu , width 1 , 0001 , 600 hu )  . 
two chest radiologists ( one senior with > 15 years of experience and one junior with < 2 years of experience ) unaware of the histological patterns analysed all hrct images independently . 
honeycombing. the distribution of findings was recorded as : ( a ) central , tecnica di imaging e analisi delle immagini stata effettuata una tc ( light speed , ge medical systemmilwaukee , aquilon - toshiba ) ad alta risoluzione ( hrct ) con tecnica volumetrica , spessore di collimazione a 1 o 1 , 5 mla scansione si estendeva dalle basi allapice polmonare . 
le immagini erano ricostruite utilizzando un algoritmo con alta frequenza spaziale ( kernel b70 ) con appropriati setting e finestra di visualizzazione ( window level 700 hu , window width 10001600 hu )  . 
due radiologi toracici ( un senior con oltre 15 anni di esperienza ed un junior con esperienza inferiore ai 2 anni ) , non a conoscenza del pattern istologico hanno analizzato indipendentemente tutte le hrct . 
la tc mostra una modesta distorsione dellarchitettura lobulare secondaria nei lobi inferiori ( b ) la tc 3 mesi dopo mostra la riduzione dellattenuazione parenchimale , pur con il persistere del pattern reticolare ( c )  . when predominantly located in the central third of the lung in perihilar location ; ( b ) peripheral , when predominantly seen in the outer third in subpleural location ; ( c ) patchy , when located anywhere in the lung . 
hrct interpretations comprised the following patterns : ( a ) noncardiogenic pulmonary oedema ; ( b ) organising pneumonia ( op ) ; ( c ) nonspecific interstitial pneumonia ( nsip ) ; ( d ) usual interstitial pneumonia ( uip ) ; ( e ) hypersensitivity pneumonitis ( hp ) ; ( f ) lipoid pneumonia ( lp ) ; ( g ) alveolar haemorrhage ( ah )  . 
honeycombing. la distribuzione dei reperti stata registrata come : ( a ) centrale , se i reperti sono localizzati prevalentemente nel terzo centrale del polmone , n sede perilare ; ( b ) periferica , se i reperti sono prevalentemente nel terzo esterno in sede mantellare ; ( c ) patchy , se la distribuzione indifferente a tutto il polmone . 
la diagnosi istologica stata di dad . bronchoscopy broncoscopia bronchoscopy was performed with the patient under deep sedation and with a rigid or flexible bronchoscope . written informed consent was obtained from all patients . bronchoalveolar lavage ( bal ) was performed by instilling 150 ml 0.9% saline solution into the segment to be studied or into the middle lobe if the parenchymal abnormalities were diffuse . 
all samples were reviewed by a pathologist with extensive experience in lung pathology . each histological section was stained with haematoxylin and eoswhere sampling was considered unnecessary , bal alone was carried out . lesame broncoscopico era effettuato in sedazione profonda , con broncoscopio rigido o flessibile . 
il lavaggio bronco - alveolare ( bal ) stato effettuato instillando 150 ml di soluzione salica 0 , 9% , nel segmento da studiare o , in alternativa nel lobo medio , qualora le alterazioni parenchimali fossero diffuse . 
la tc ( a , b ) mostra delle aree di ground glass di tipo patchy e piccole consolidazioni in entrambi i lobi superiori ed ai segmenti apicali dei lobi inferiori . 
una modesta quota di fibrina presente nellalveolo . statistical analysis analisi statistica interobserver agreement of the radiological diagnoses was studied using cohens kappa statistic with a 95% confidence interval ( ci )  . 
in addition , the specificity and sensitivity of hrct was calculated against the cytohistological diagnosis , which was considered the reference standard . linterobserver agreement delle diagnosi radiologiche stato descritto utilizzando lindice kappa di cohen , con un intervallo di confidenza del 95% . 
patients underlying diseases included non - hodgkins lymphoma in seven ( 17% ) , hodgkins lymphoma in one ( 2% ) , psoriatic arthritis in one ( 2% ) , atrial fibrillation in nine ( 21% ) , systemic hypertension in three ( 7% ) , chronic lymphatic leukaemia in two ( 5% ) , depression in two ( 5% ) , colorectal carcinoma in one ( 2% ) , multiple myeloma in one ( 2% ) , constipation in one ( 2% ) , nasal disorders in two ( 5% ) , rheumatoid arthritis in four ( 10% ) , breast cancer in two ( 5% ) , ewings sarcoma in one ( 2% ) , hydrocephalus in one ( 2% ) , bipolar syndrome in one ( 2% ) , hepatitis c virus infection in two ( 5% ) and cannabis - use disorder in one ( 2% )  . 
la biopsia transbronchiale ( tblb ) stata effettuata in tutti i pazienti , eccetto in un caso di emorragia alveolare e tre casi di polmonite lipoidea in cui la diagnosi era ottenuta con il bal . 
le patologie di base comprendevano : linfoma non - hodgkin in 7 pazienti ( 17% ) ; linfoma di hodgkin in 1 ( 2% ) ; artrite psoriasica in 1 ( 2% ) ; fibrillazione atriale in 9 ( 21% ) ; ipertensione sistemica in 3 ( 7% ) ; leucemia linfatica cronica in 2 ( 5% ) ; depressione in 2 ( 5% ) ; carcinoma colon - rettale in 1 ( 2% ) ; mieloma multiplo in 1 ( 2% ) ; costipazione in 1 ( 2% ) , disturbi nasali in 2 ( 5% ) ; artrite reumatoide in 4 ( 10% ) ; carcinoma mammario in 2 ( 5% ) ; sarcoma di ewing in 1 ( 2% ) ; idrocefalo in 1 ( 2% ) ; sindrome bipolare in 1 ( 2% ) ; virus dellepatite c ( hcv ) in 2 ( 5% ) , abuso di cannabinoidi in 1 ( 2% )  . 
la durata dei radiol med ( 2011 ) 116 : 246263 table 1 clinical data patient no . gender underlying diagnosis drug non - hodgkins lymphoma psoriatic arthritis non - hodgkins lymphoma hodgkins lymphoma atrial fibrillation systemic hypertension chronic lymphatic leukaemia major depression non - hodgkins lymphoma colorectal cancer multiple myeloma constipation non - hodgkins lymphoma nasal discomfort rheumatoid arthritis breast cancer non - hodgkins lymphoma ewings sarcoma non - hodgkins lymphoma rheumatoid arthritis hydrocephalus bipolar syndrome atrial fibrillation hepatitis c cannabis abuse atrial fibrillation breast cancer rheumatoid arthritis atrial fibrillation atrial fibrillation atrial fibrillation systemic hypertension chronic lymphatic leukaemia rheumatoid arthritis atrial fibrillation systemic hypertension atrial fibrillation hepatitis c atrial fibrillation major depression nasal disorder atrial fibrillation bleomycin methotrexate macop - b bleomycin , adriamycin , vinblastine amiodarone valsartan fludarabine venlafaxine bleomycin vincristine 5 - fluorouracile oxaliplatin cytosine arabinoside vaseline oil macop - b vaseline oil methotrexate cyclophosphamide adriamycin macop - b , mabthera busulfan , melphalan bleomycin antimonoclonal ab valproic acid lithium amiodarone interferonribavirin cannabinoid amiodarone taxol antimonoclonal ab amiodarone amiodarone amiodarone acebutolol fludarabine leflunomide amiodarone amlodipine amiodarone interferonamiodarone amitriptyline rhinological solution amiodarone macop - b , methotrexate , adriamycin , cyclophosphamide , oncovin , prednisone , and bleomycin four patients died due to the severity of symptoms [ three patients with diffuse alveolar damage ( dad ) and one with a histological diagnosis of chronic interstitial pneumonia ( cip ) ]  . 
interlobular septal thickening was seen in stato documentato un agreement da buono ad eccellente , nella valutazione dei reperti tc e della relativa distribuzione dei reperti ( k = 0 , 72 fino a 1 , 00 )  . 
lispessimento dei setti intertabella 1 caratteristiche cliniche e farmaci somministrati alla presentazione iniziale dei sintomi sesso patologia sottostante farmaco radiol med ( 2011 ) 116 : 246263 linfoma non - hodgkin artrite psoriasica linfoma non - hodgkin linfoma non - hodgkin fibrillazione atriale ipertensione sistemica leucemia lifantica cronica depressione maggiore linfoma non - hodgkin tumore del colon mieloma multiplo costipatione linfoma non - hodgkin rinorrea artrite reumatoide tumore mammario linfoma non - hodgkin sarcoma di ewing linfoma non - hodgkin artrite reumatoide idrocefalo disturbo bipolare fibrillazione atriale abuso di cannabis fibrillazione atriale tumore mammario artrite reumatoide fibrillazione atriale fibrillazione atriale fibrillazione atriale ipertensione sistemica leucemia linfatica cronica artrite reumatoide fibrillazione atriale ipertensione sistemica fibrillazione atriale fibrillazione atriale depressone maggiore rinorrea fibrillazione atriale bleomicina metotrexate macop - b bleomicina , adriamicina , vinblastina amiodarone valsartan fludarabina velfalaxina bleomicina vincristina 5 - fluorouracile oxaliplatino citosina arabinoside olio di vaselina macop - b olio di vaselina metotrexate ciclofosfamide adriamicina maco - b busulfan , alkeran bleomicina anti monoclonal ab acido valproico litio amiodarone interferone ribavirina paraquat amiodarone taxolo anticorpi anti monoclonali amiodarone amiodarone amiodarone acetabulolo anticorpi anti monoclonali leflunomide amiodarone amlodipine amiodarone interferone amiodarone amitriptilina soluzione rinologica amiodarone 25 patients ( 60% ) , centrilobular nodules in three ( 7% ) , peripheral consolidation in nine ( 21% ) , patchy consolidation in 15 ( 35% ) , peripheral ground - glass pattern in six ( 14% ) , central ground - glass pattern in four ( 10% ) , diffuse ground - glass pattern in ten ( 23% ) and ground - glass pattern in ten ( 23% )  . 
there was good interobserver agreement in interpretation of the radiological pattern , in particular with lobulari stato osservato in 25 pazienti ( 60% ) , i noduli centrolobulari in 3 ( 7% ) ; i consolidamenti periferici in 9 ( 21% ) ; i consolidamenti patchy in 15 ( 35% ) ; il ground glass periferico in 6 ( 14% ) ; il ground glass centrale in 4 ( 10% ) ; il ground glass diffuso in 10 ( 23% ) e il ground glass in 10 ( 23% )  . 
noncardiogenic pulmonary oedema was seen in 13 patients ( 30% ) , op in nine ( 21% ) , hp in two ( 5% ) , ah in two ( 5% ) , nsip in five ( 12% ) , lp in one ( 2% ) and pseudosarcoidosis in one ( 2% )  . an indeterminate pattern was identified in seven ( 16% )  . parenchymal findings were confined to the upper lobes in 14% of patients ( n = 6 ) , the lower lobes in 31% ( n = 13 ) and extended to the entire lung in 55% . 
there was no statistical difference between extension of the parenchymal changes and type of drug taken ( antineoplastic or nonantineoplastic )  . cytohistological interpretation pattern radiologico , in particolare per lnsip ( k = 0 , 68 ) ; op ( k = 0 , 67 ) ; dad ( k = 0 , 67 ) ; pattern indeterminato ( k = 0 , 72 ) ; hp ( k = 0 , 78 )  . 
il 14% dei pazienti ( n = 6 ) ha mostrato alterazioni parenchimali ai lobi superiori ; il 31% ( n = 13 ) ai lobi inferiori ed il 55% mostrava un diffuso coinvolgimento del parenchima polmonare . 
non stata registrata alcuna differenza statistica tra la tipologia della estensione delle alterazioni parenchimali e il tipo di farmaco assunto dai pazienti ( antineoplastico o non - antineoplastico )  . histological examination documented dad in 11 patients ( 26% ) , op in seven ( 16% ) , hp in three ( 7% ) , ah in three ( 7% ) , cip in eight ( 19% ) , lp in three ( 7% ) and pseudosarinterpretazione cito - istologica i reperti istologici hanno documentato dad in 11 casi 256 table 2 results of high - resolution computed tomography ( hrct ) and cytohistology for 13 patients treated with antineoplastic drugs patient no . 
in eight patients , histological diagnosis was cip , for which the corresponding radiological pattern was indeterminate pattern ( n = 5 ) ; dad ( n = 2 ) and op ( n = 1 )  . 
dei restanti pattern , nonostante lesiguo numero dei casi per ciascun pattern , si segnala : ah ( sensibilit 0 , 66 ; specificit 1 ) ; hp ( sensibilit e specificit 1 ) ; lp ( sensibilit 0 , 33 ; specificit 0 )  . 
in 8 pazienti , stata posta diagnosi istologica di cip , tale pattern ha presentato come corrispettivo radiologico : pattern indeterminato ( n = 5 ) ; dad ( n = 2 ) ; op ( n = 1 )  . 
lnsip invece ha documentato specificit pari a 1 , contro una sensibilit piuttosto bassa ( 0 , 38 )  . comparison between antineoplastic and nonantineoplastic drugs confronto tra il gruppo dei farmaci antineoplastici e farmaci non - antineoplastici histological patterns documented in the group of antineoplastic drugs were cip ( n = 6 ) and dad ( n = 2 )  . 
distribution of parenchymal findings , histological results and hrct findings are summarised in tables 2 and 3 . il pattern istologico documentato nel gruppo dei farmaci antineoplastici stato : cip ( n = 6 ) e dad ( n = 2 )  . 
la distribuzione delle alterazioni parenchimali , il dato istologico ed i reperti hrct sono sintetizzati nelle tabelle 2 e 3 . table 3 results of high - resolution computed tomography ( hrct ) and cytohistology for 29 patients treated with nonantineoplastic drugs patient no . 
the reason for this includes the use of chest radiography as a first - line modality in evaluating nonspecific dyspnoea , a modality that is often unable to detect interstitial disease [ 9 , 10 ]  . 
whereas idiopathic interstitial pneumonias , as classified by the 2002 consensus of the american thoracic society and european respiratory society [ 10 , 11 ] , tends to show characteristic patterns at hrct , parenchymal changes produced by pharmaceutical drugs are highly variable and often investigated with surgical lung biopsy [ 1215 ]  . in this study , we attempted to compare cytohistological patterns provided by transbronchial biopsy or bal and radiological findings identified with hrct . 
la ragione di questo fenomeno include il ricorso alla radiografia del torace come tecnica di prima scelta nella valutazione di una dispnea non ben specificata che pu spesso non individuare una patologia interstiziale [ 9 , 10 ]  . 
mentre le pneumopatie interstiziali idiopatiche come sono state classificate dal consensus del 2002 [ 10 , 11 ] dallats e dallers , spesso mostrano dei pattern tipici allindagine hrct , i farmaci possono indurre invece delle alterazioni parenchimali altamente variabili , che spesso finiscono alla biopsia chirurgica [ 1215 ]  . in questo studio abbiamo cercato di confrontare il pattern cito - istologico come veniva fornito dalla biopsia trans bronchiale o dal bal ed i reperti radiologici individuati alla tc ad alta risoluzione . 
7 alveolar haemorrhage in a 40 - year - old man affected by non - hodgkins lymphoma and treated with methotrexate , adriamycin , cyclophosphamide , oncovin , prednisone , and bleomyccomputed tomography shows several subpleural consolidations in both lower lobes . 
even though the fibrosing variant of nsip often shows a predominantly reticular pattern [ 24 , 25 ] , radiologists were unable to distinguish between the two subgroups on the basis of hrct findings alone , probably as a result of the wide variability of the nsip pattern . 
in addition , hrct findings of nsip showed significant overlap with those of other patterns , such as dad , hp and ah [ 19 , 25 ]  . radiologica , in particolare per op e dad , con valori che oscillano tra 0 , 8 e 1 . 
anche se la variante fibrosante dellnsip spesso mostra un pattern prevalentemente reticolare [ 24 , 25 ] , i radiologi non hanno potuto distinguerne i due sottogruppi sulla sola base dellaspetto hrct : probabilmente in considerazione della forte variabilit del pattern nsip ; per questo pattern stato registrato il valore pi basso di sensibilit ( 0 , 38 ) , pur mantenendo elevati valori di specificit che raggiungeva lunit . 
il bal mostra le inclusioni di olio nei macrofagi alla colorazione red oil sta it may be that by observing the characteristics of our patient series and emphasising the patchy distribution of the ground - glass pattern and lack of any severe parenchymal disruption , improvement in sensitivity could be obtained . noncardiogenic pulmonary oedema ( figs 3 , 4 ) with its histological counterpart dad was observed in ten patients ( macop - b in one ; amiodarone in four ; busulfan in one ; taxol in one and amlodipine in one )  . 
in our series , imaging findings considered strongly indicative of dad were rapidly progressive ground - glass pattern , normal - sized heart and peripheral thickening of the interlobular septa in the absence of other clinical explanations . 
specificity and sensitivity values obtained for dad were high . hp was observed in three patients ( amitriptyline in one , interferon in one and cytosine arabinoside in one ) ( fig 5 )  . many drugs can cause hp , the most common being methotrexate , bleomycin , penicillamine , cyclophosphamide , nitrofurantoin and carmustine . 
in one patient , we observed a pulmonary pattern that was sarcoid - like , induced by treatment with interferon - alfa ( 2628 ) , and characterised by a diffuse nodular pattern with upper - lobe quali : dad ; hp e ah [ 19 , 25 ]  . 
nel nostro gruppo abbiamo considerato fortemente convincente per dad : un ground glass rapidamente progressivo , in presenza di un cuore di normali dimensioni , con ispessimento periferico dei setti interlobulari , in assenza di altre spiegazioni cliniche . 
molti sono i farmaci che possono indurre una hp , tra questi i pi comuni sono il metotressato , la bleomicina , la penicillamina , la ciclofosfamide , la nitrofurantoina e la carbustina . 
the patient was 78 years old , an unusual age for sarcoidosis , and the clinical findings were a reduction in diffusion lung capacity for carbon monoxide ( dlco ) , coinciding with the administration of ifn -  . 
in seven patients , radiologists were unable to identify any characteristic hrct pattern and defined it as indeterminate pattern ; that is , ground - glass attenuation that did not reflect any specific pattern of interstitial pneumonia . 
in these cases , histological patterns were lp ( n = 1 ) , op ( n = 1 ) and nsip ( n = 5 ) , which further confirms the overlap of the various radiological patterns . despite adequacy of samples obtained with transbronchial lung biopsy , diagnosis proved inconclusive in 14 patients ; eight of them were thus studied with video - assisted thoracoscopy , which yielded four cases of nsip , two of uip and two of hp . 
in una paziente abbiamo osservato un quadro polmonare sarcoid - like , indotto da terapia con interferone - alfa ( 2628 ) , caratterizzato da un pattern nodulare diffuso , con predominanza ai lobi superiori e slargamento dei linfonodi del mediastino . 
inoltre , la paziente aveva 78 anni , unet inusuale per la sarcoidosi , con un quadro clinico caratterizzato da riduzione della diffusione polmonare del monossido di carbonio ( dlco ) , in coincidenza con la somministrazione di ifn . 
sono molti gli studi che hanno documentato la correlazione tra la somministrazione di tale farmaco e la manifestazione polmonare di sarcoidosi , indotta dallattivazione dei macrofagi [ 24 ]  . 
in ben sette pazienti i due radiologi , non potendo meglio caratterizzare il quadro tc , lo hanno definito come pattern indeterminato , cio un ground glass che non configurava alcun quadro specifico di pneumopatia interstiziale . 
il corrispettivo istologico di tali casi era : lp ( n = 1 ) ; op ( n = 1 ) e nsip ( n = 5 ) : questi dati confermano ulteriormente loverlap dei vari pattern radiologici . 
malgrado il buon campionamento della tblb , in 14 pazienti la diagnosi non stata conclusiva e 8 di questi sono stati sottoposti a vats , ottenendone 4 casi di nsip ; 2 uip e 2 hp . 
 262 radiol med ( 2011 ) 116 : 246263 as op , ep or dad , the diagnosis could be fairly straightforward , whereas in cases in which the diagnosis requires larger samples , such as uip , dip and nsip , transbronchial lung biopsy is often insufficient , leading to a need for video - assisted thoracoscopy . 
in particular , for nsip , the difficulties surrounding the microhistological diagnosis have been well described in the literature and will most likely remain one of the main causes of surgical biopsy in dr - ild . 
the first was : what sensitivity and specificity values can be expected of hrct in the diagnosis of dr - ild ? ; the second was : to what extent is transbronchial lung biopsy able to provide a confident diagnosis of dr - ild ? with regard to the first question , we obtained excellent sensitivity , with a loss of specificity for the ground - glass opacity defined as indeterminate pattern ( 16% of cases ) ; nonetheless , in these cases , ct proved to be an excellent aid in planning transbronchial lung biopsy . 
as for the second question , transbronchial lung biopsy proved to be a highly reliable diagnostic tool , especially in cases with a monomorphic histological pattern such as op , dad and hp . 
additionally , no significant complications were observed , and the technique could also be used in patients who were ineligible for any surgical diagnostic approach . there are three main limitations to this study : small series size ; inability to document improvement after drug discontinuation in all patients due to the death of four ( respiratory failure ) ; and it did not add any information about drug interactions . 
in the event of combined administration , demonstration of lung toxicity was empirical and based on suspension of the combination ( e.g. , bleomycin - vincristine ; bleomycin - adriamycin - vinblastine )  . in conclusion , hrct allows the radiologist to make a confident diagnosis , above all in cases with a rapidly progressive picture , such as dad and ah . 
this allows the drug to be promptly discontinued and support treatment to be initiated . la causa della necessit di un approccio chirurgico ( 2932 ) risiede nelle dimensioni del campione istologico ottenuto con la tblb . 
per pattern monomorfi come op , ep o dad la diagnosi potrebbe essere piuttosto agevole , mentre in casi in cui la diagnosi approcciabile spesso su campioni di maggiori dimensioni come uip , dip , nsip , la tblb si pone spesso la necessit di ricorrere a vats . 
in particolare per lnsip , le difficolt correlate alla diagnosi microistologica sono ben descritte in letteratura e probabilmente rimarr tra le cause maggiori di biopsia chirurgica nelle dr - ild . 
 il nostro studio ha cercato di rispondere a due domande . la prima era : che valori di sensibilit e specificit ci si pu aspettare dalla hrct nella diagnosi di dr - ild ; la seconda : quanto la tblb pu essere confidente nella diagnosi di drild . 
per quanto riguarda la prima domanda , abbiamo ottenuto unottima sensibilit , con perdita di specificit di fronte al ground glass definito come pattern indeterminato ( ben il 16% della serie ) , in tali casi la tc ha rappresentato tuttavia un ottimo strumento nel planning della tblb . 
 le limitazioni di questo studio sono state principalmente tre : le dimensioni modeste del campione , limpossibilit di documentare in tutti un miglioramento dopo la sospensione del farmaco , per il decesso di quattro pazienti ( da insufficienza respiratoria ) e il non aver aggiunto alcuna informazione riguardante le interazioni tra farmaci . 
in caso di somministrazione in associazione , la dimostrazione della tossicit stata empirica , basata sulla sospensione della miscela di farmaci ( come ad esempio il caso della associazione bleomicina - vincristina , bleomicina - adriamicina - vinblastina )  . 
ci permette il pronto intervento con sospensione del farmaco e inizio della terapia di supporto . acknowledgements we are very grateful to lawrence r . goodman , department of radiology , medical college of wisconsin , milwaukee and nestor muller , department of radiology , university of british columbia , vancouver , for their revision of the manuscript . ringraziamenti un profondo ringraziamento al lawrence r . 
there were 43 benign lesions ( 13 fibrocystic disease , eight fibroadenoma , seven adenosis , five normal breast tissue , four inflammatory lesions , three intramammary lymph nodes , two scleroelastosis and one fat necrosis ) and 35 malignant lesions ( 30 invasive ductal carcinoma , two invasive lobular carcinoma , one ductal carcinoma in situ , one carcinomatous mastitis and one metastasis from neuroendocrine carcinoma )  . 
with the cutoff value set at 1.52 , dwi sensitivity ( 35 true positive , no false negative ) was 100% and specificity was 86% ( ci 75.7%96.3% ) due to 37 true negatives and six riassunto obiettivo . 
43 lesioni sono risultate benigne ( 13 casi di mastopatia fibrocistica , 8 di fibroadenoma , 7 di adenosi , 5 di tessuto mammario normale , 4 di lesioni flogistiche , 3 di linfonodi intramammari , 2 di scleroelastosi ed 1 di steatonecrosi ) e 35 maligne ( 30 carcinomi duttali infiltranti , 2 carcinomi lobulari infiltranti , 1 carcinoma duttale in situ , 1 mastite carcinomatosa ed 1 metastasi da carcinoma neuroendocrino )  . 
ponendo il cut off di adc pari a 1 , 48 , la dwi ha raggiunto una sensibilit ( 31 veri positivi ; 4 falsi negativi , rappresentati da 3 carcinomi duttali infiltranti e da una mastite carcinomatosa ) dell88 , 6% ( intervallo di confidenza [ ic ] : 78 , 1%99 , 1% ) ed una specificit ( 41 veri negativi ; 2 falsi positivi , dovuti ad un caso di steatonecrosi e ad un fibroadenoma ) del 95 , 3% ( ic : 88 , 9%100% )  . 
dwi is a reliable tool for characterising focal breast lesions . keywords breast cancer magnetic resonance imaging diffusion weighted imaging sensibilit ( 35 veri positivi ; nessun falso negativo ) risultata del 100% e la specificit ( 37 veri negativi ; 6 falsi positivi , per laggiunta ai due falsi positivi riscontrati con cut off di 1 , 48 di 2 fibroadenomi e 2 casi di mastopatia fibrocistica ) dell86% ( ic : 75 , 7%96 , 3% )  . 
con entrambi i cut off laccuratezza globale della dwi ( 72 risultati esatti su 78 casi ) stata del 92 , 3% ( ic : 86 , 4%98 , 2% )  . 
la dwi uno strumento affidabile nella tipizzazione delle lesioni focali mammarie . parole chiave carcinoma mammario risonanza magnetica diffusione rm introduction introduzione specificity ( 68%96% ) with its ability to provide high - resolution morphological imaging combined with information about intralesional blood flow based on spatial and temporal contrastenhancement patterns , conventional dynamic magnetic resonance imaging ( mri ) has widely demonstrated its diagnostic value in breast imaging [ 1 , 2 ]  . 
mri is able to detect tumours missed at mammography or ultrasonography [ 38 ] , stage tumours more accurately ( especially the intraductal component ) and characterise lesions as benign or malignant [ 913 ]  . 
however , there is still room for improvement in breast mri : the need to use a contrast agent prolongs ( albeit not unreasonably ) imaging times , makes the examination expensive and carries a risk of potential toxicity of paramagnetic contrast material . furthermore , although highly sensitive , breast mri has suboptimal in diagnosing neoplasms [ 1418 ]  . 
with the elimination of artefacts related to field nonuniformity [ 21 ] such as magnetic susceptibility and chemical shift [ 22 ] made possible by technological progress and in particular by parallel imaging [ 11 , 19 , 20 ] , diffusion - weighted imaging ( dwi ) has successfully been introduced into routine clinical practice . 
dwi which has higher contrast resolution than mri and does not require contrast administration [ 19 , 23 ] was initially used to diagnose cerebral ischaemia . however , it has also shown to be valuable in characterising expansile lesions in different organs and systems thanks to its ability to reflect structural features ( histological composition and cellularity ) [ 2433 ] that do not affect lesion appearance on conventional mri , which is unable to visualise tumour histology and quantitative cell / stroma ratio [ 19 , 21 ]  . 
although with some minor differences in opinion , numerous studies have reported the potential advantages of dwi compared with mri in evaluating expansile breast lesions [ 14 , 16 , 19 , 31 , 3436 ]  . the aim of this study was to examine the diagnostic grazie alla capacit di desumere dal pattern spaziale e dallandamento temporale della captazione del mezzo di contrasto para - magnetico ( mdc ) dati relativi alla circolazione ematica intra - lesionale e di acquisire parallelamente fini dettagli morfologici in immagini ad elevata risoluzione spaziale , la risonanza magnetica ( rm ) convenzionale dinamica ha ampiamente dimostrato , negli ultimi 15 anni , la sua efficacia diagnostica in ambito senologico [ 1 , 2 ]  . 
la rm infatti in grado di identificare neoplasie non riconoscibili allesame mammo - ecografico [ 38 ] , di valutarne pi accuratamente di questo lestensione ( specie nella componente intraduttale ) e , in molti casi , di definire la natura benigna o maligna delle neoformazioni [ 913 ]  . 
la rm della mammella rimane , tuttavia , unindagine ancora suscettibile di miglioramenti : la necessit di ricorrere al mdc ne prolunga ( seppure in misura non insormontabile ) la durata , la rende costosa e la espone ai rischi potenziali di tossicit impliciti nella somministrazione degli agenti para - magnetici . 
da quando levoluzione tecnologica in seguito soprattutto allintroduzione della tecnica di imaging parallelo [ 11 , 19 , 20 ] stata in grado di rimuovere gli artefatti causati dalla non - uniformit del campo magnetico [ 21 ] quali quelli di suscettibilit e di chemical shift [ 22 ] , la rm con imaging pesato in diffusione ( diffusion - weighted imaging , dwi ) stata introdotta con successo nella pratica clinica . 
inizialmente impiegata nella diagnosi dellischemia cerebrale , la dwi che rispetto alla rm dotata di pi alta risoluzione di contrasto e non presenta gli effetti sfavorevoli connessi alla necessit del ricorso al mdc [ 19 , 23 ] si dimostrata utile nella tipizzazione delle lesioni espansive di diversi organi e apparati , grazie alla sua capacit di riflettere caratteri strutturali delle lesioni stesse ( essenzialmente la composizione istologica e la cellularit ) [ 2433 ] che non ne condizionano 266 radiol med ( 2011 ) 116 : 264275 performance of dwi in a series of patients with focal breast lesions , all studied by mri and cytology and / or histology . materials and methods inclusion criteria between november 2006 and june 2008 , we recruited 241 women with mammographic and sonographic findings of at least one focal breast lesion deserving further investigation with mri . 
four patients were excluded because of contraindications to mri ( two had claustrophobia ; two wore a pacemaker ) ; 17 patients were not eligible , as the long axis of the focal lesion was 6 mm or less on mri . 
in addition , 140 patients had pathognomonic signs of benign disease on mri and dwi so that no pathological examination was required . finally , one patient refused cytological evaluation , and another did not provide consent to participate . 
our series therefore included 78 patients ( mean age 44.1 years ; range : 1877 ) for a total of 78 focal breast lesions with a long axis of 7 mm or more on mri , which were studied by both conventional mri and dwi and for whom an adequate cytological and / or histological examination was available . diagnostic investigations mri all examinations were performed with a 1.5 - t scanner ( signa excite , general electric medical systems , milwaukee , wi , usa ) with axial scans acquired with a four - channel surface coil and the patient in prone position . in our protocol , precontrast conventional mri is carried out with one t2 - weighted fat - suppressed sequence ( tr / te 4000 / 31.6 ms ; acquisition matrix 256256 ; nex = 2 ; field of view 3232 cm ; slice thickness 4 mm with 0.4 interval ; duration 3 h 49 s ) , and one t1 - weighted fast spin - echo sequence ( tr / te 540 / 7.1 ms ; acquisition matrix 320256 ; nex = 2 ; field of view 3434 cm ; slice thickness : 4 mm with 0.4 interval ; duration : 256 )  . 
alcuni lavori apparsi negli ultimi anni in letteratura testimoniano , seppure con qualche marginale discordanza di opinioni , i vantaggi che la dwi potenzialmente in grado di apportare rispetto alla rm nella valutazione delle lesioni espansive della mammella [ 14 , 16 , 19 , 31 , 3436 ]  . scopo di questo lavoro esaminare la performance diagnostica della dwi in una serie di lesioni focali mammarie , tutte sottoposte sia ad indagine rm sia a verifica citologica e / o bioptica . materiali e metodi criteri di inclusione lesione nel periodo compreso fra novembre 2006 e giugno 2008 sono state prese in considerazione , per linclusione in questo studio , 241 pazienti di sesso femminile nelle quali lesame mammo - ecografico aveva messo in evidenza almeno una focale giudicata meritevole di approfondimento diagnostico mediante rm . 
quattro pazienti sono state escluse dallo studio per la loro impossibilit ad espletare lindagine rm ( 2 in quanto claustrofobiche ; 2 portatrici di pace - maker ) ; 17 pazienti sono state giudicate non eleggibili per la valutazione dwi in quanto portatrici di lesioni focali il cui asse maggiore risultato alla rm pari o inferiore a 6 min 140 pazienti , inoltre , sia lindagine rm che quella dwi hanno dato esito a reperti patognomonici di benignit , che non hanno fatto ritenere necessario il ricorso alla tipizzazione anatomo - patologica . infine , una paziente ha rifiutato di sottoporsi allapprofondimento citologico propostole , mentre unaltra non ha espresso il proprio consenso alla propria inclusione nello studio . 
through linear regression analysis of the natural logarithm of the signal intensity versus the diffusion gradient ( b ) used ( 0 and 800 s / mm2 ) inside an operator - defined region of interest ( roi ) , the software quantified the extent of diffusion and produced an apparent diffusion coefficient ( adc ) expressed in millimetres squared per second . reference standard all 78 lesions in the study underwent fine - needle ( 2022 gauge ) aspiration cytology under mammographic or sonographic guidance , depending on which was considered more appropriate by the operator . 
in lesions with inadequate or doubtful cytology and with a high index of suspicion at sonography / mammography and / or mri , the diagnostic evaluation was completed by histological examination of a 14 - gauge cutting - needle core biopsy . 
in the case of cytological or biopsy findings of uncertain malignant potential or suspicious for malignancy ( b3 or higher ) , the lesion was surgically excised , and histological examination was performed on the surgical specimen . statistical analysis for the purposes of this study , lesions were classified as probably malignant or probably benign on the basis of the mri findings . 
statistical significance of the differences in mean adc values between benign and malignant lesions was determined by applying the mann - whitney test . results pathological characterisation was obtained for all 78 lesions : in 49 cases by histology ( in 38 cases on the surgical specimen , in 11 on the biopsy specimen ) and in 29 by cytology . 
among malignant lesions , infiltrating ductal carcinoma not otherwise specified ( nos ) was by far the most frequent histological type , whereas the most frequent benign conditions were fibrocystic mastopathy , fibroadenoma and adenosis ; in five cases , breast tissue showed no pathological abnormality . 
lesame rm convenzionale pre - contrastografico prevede , nel nostro protocollo , una sequenza t2 con tecnica di fat suppression ( tempo di ripetizione [ tr ] / tempo di eco [ te ] : 4000 / 31 , 6 ms ; matrice di acquisizione : 256256 ; nex = 2 ; field of view : 3232 cm ; spessore di fetta : 4 mm con intervallo di 0 , 4 ; durata : 3 min 49 s ) ed una sequenza t1 fast spin - echo ( tr / te : 540 / 7 , 1 ms ; matrice di acquisizione : 320256 ; nex = 2 ; field of view : 3434 cm ; spessore di fetta : 4 mm con intervallo di 0 , 4 ; durata : 2 min 56 s )  . 
lindagine dinamica consiste in una sequenza t1 gradient - echo ( tr / te : 4 , 6 / 2 , 1 ms ; matrice di acquisizione : 256256 ; nex = 1 ; field of view : 3232 cm ; spessore di fetta : 4 mm con intervallo di 0 , 4 ; flip angle : 10 ; durata : 7 min 13 s ) , che prevede una acquisizione basale e 6 acquisizioni successive della durata di circa un minuto ciascuna , dopo la somministrazione endovenosa di mezzo di contrasto a base di acido gadoterico ( dotarem , guerbet , roissy cdg cedex , francia ) alla dose di 0 , 2 ml / kg e con velocit di infusione di 2 , 5 ml / s . dwi le immagini pesate in diffusione sono state acquisite , in scansione assiale , mediante una sequenza echo - planar ( asset ) con tecnica di imaging parallelo ( tr / te : 4000 / 55 , 2 ms ; matrice di acquisizione : 6464 ; nex = 8 ; field of view : 3434 cm ; spessore di fetta : 7 mm con intervallo di 0 , 4 ; durata : 2 min 08 s )  . 
il software , allinterno di una zona di interesse selezionata dalloperatore ( region of interest , roi ) , mediante analisi di regressione lineare del logaritmo naturale dellintensit del segnale versus il gradiente di diffusione ( b ) utilizzato ( 0 e 800 s / mm2 ) , ha quantificato lentit della diffusione ricavando un valore di apparent diffusion coefficient ( adc ) espresso in mm2 / s . 
 reference standard tutte le lesioni incluse nello studio , il cui quadro non sia stato considerato patognomonico di lesione benigna sia allindagine rm che a quella dwi , sono state sottoposte ad esame citologico con ago sottile ( 2022 g ) guidato dalla metodica di imaging ( mammografia o ecografia ) giudicata nel singolo caso pi opportuna dalloperatore . 
nelle lesioni con risultato citologico inadeguato o dubbio in concomitanza di un livello di sospetto elevato allindagine ecomammografica e / o rm liter diagnostico stato proseguito tramite verifica istologica mediante micro - biopsia percutanea con ago tranciante da 14 g . 
in caso di reperto citologico o micro - bioptico indicativo o sospetto di natura maligna ( giudicato in classe b3 o superiore ) la lesione stata asportata chirurgicamente con successiva verifica istologica del pezzo operatorio . 
laffidabilit diagnostica della dwi stata confrontata con il gold standard rappresentato dal reperto citologico e / o istologico utilizzando i due cut off di adc ( 1 , 48 e 1 , 52 10 - 3 mm2 / s ) che secondo lesperienza personale garantiscono adottando le modalit tecniche di esecuzione dellindagine sopra riportate le performance pi efficaci . 
accelerated by membrane permeability between the intraand extracellular compartments and transmembrane transport mechanisms and hindered by risultati di tutte le 78 lesioni comprese in questo studio stata ottenuta la tipizzazione anatomo - patologica : in 49 casi mediante esame istologico ( in 38 casi su analisi istologica del pezzo operatorio , in 11 mediante biopsia percutanea ) , in 29 attraverso indagine citologica . 
although extensive neoangiogenesis implies abundant perfusion [ 6 , 15 , 16 ] , the speed of diffusion is slower in malignancies than in normal tissues and benign lesions [ 14 , 15 ]  . 
this presumably is because of the dominant hindering effect of high cellularity , which reduces the amount of extracellular water and increases barriers to motion [ 14 , 15 , 20 ] , as demonstrated in both spontaneous and experimental tumours [ 34 , 39 ]  . the sensitivity of dwi in detecting breast malignancies varies between being close to that of mri in some reports [ 20 , 23 ] and definitely lower in others [ 16 , 32 ] : in particular , dwi is limited in identifying lesions < 810 mm , for which adc values cannot as yet be determined with certainty [ 15 ]  . 
the risk of not being able to reliably evaluate the speed of water diffusion in small lesions led us to exclude lesions 6 mm , even though we have seen that some 5and 6 - mm masses that are well depicted by mri can also be correctly identified by dwi . in this study , we applied what we have found to be the ( nas ) , mentre le patologie benigne pi rappresentate sono state mastopatia fibrocistica , fibroadenoma ed adenosi ; in 5 casi stato riscontrato tessuto mammario esente da alterazioni anatomo - patologiche . 
la tabella 3 esprime in dettaglio i singoli risultati ottenuti con i due cut off , riportando anche per completezza la performance diagnostica che nella stessa serie di pazienti avrebbe avuto la rm , classificando i reperti esclusivamente come probabilmente benigni o probabilmente maligni . la differenza fra i valori di adc misurati nelle lesioni maligne e in quelle benigne risultata altamente significativa allanalisi statistica ( p < 0 , 001 ) espletata mediante il test di mann - whitney . due impulsi successivi di radiofrequenza di intensit uguale e di direzione opposta , applicati su una sequenza spin echo prima e dopo limpulso rifocalizzante a 180 , destinati ad elidersi a vicenda se interagiscono con bersagli statici , danno luogo a un segnale diverso da zero ( e quantificabile ) nel caso le molecole da essi incontrate siano in movimento [ 28 , 37 ]  . 
su questo presupposto fisico fondato limpiego diagnostico della dwi , che allinterno di una zona di interesse selezionata dalloperatore sullimmagine rm preliminare consente di misurare mediante un apposito parametro numerico ( adc ) la velocit della diffusione , ovvero del movimento casuale dei protoni legati allacqua contenuta nel fluido extra - cellulare [ 14 , 21 , 28 ]  . 
accelerato dalla permeabilit di membrana fra i compartimenti intraed extra - cellulare e dai meccanismi di trasporto attivo trans - membrana ed ostacolato dalla viscosit dei fluidi e dalla quantit di macromolecole e di membrane cellulari presenti [ 38 ] , il movimento di diffusione dipende fondamentalmente dalla perfusione tessutale e dal numero di cellule presenti . nonostante la ricchezza della neoangiogenesi vi comporti una perfusione elevata [ 6 , 15 , 16 ] , nei tumori maligni la velocit della diffusione risulta inferiore a quella osservata nei tessuti normali e nelle lesioni benigne [ 14 , 15 ] , presumibilmente per il prevalere delleffetto di ostacolo esercitato dalla cellularit elevata , che riduce la quantit di acqua extra - cellulare e aumenta le barriere contro il movimento [ 14 , 15 , 20 ] , come stato dimostrato in tumori sia spontanei che sperimentali [ 34 , 39 ]  . 
 la sensibilit della dwi nellidentificare le lesioni maligne della mammella , per quanto prossima a quella radiol med ( 2011 ) 116 : 264275 most appropriate cutoff values for imaging protocols that used and achieved dwi accuracy of 92.3% in differentiating between benign and malignant lesions ( table 3 )  . 
these levels are only slightly different from those achieved with mri , which having to classify the findings as either benign or malignant only produced only one error less than did dwi ( table 3 )  . to our knowledge , all studies on this topic have reported a statistically significant difference between the mean adc values of malignant lesions ( range 0.951.22 , depending on the b value ) and benign lesions ( 1.441.67 ) [ 1416 , 19 , 20 , 23 , 28 , 29 , 32 , 33 ]  . 
in our experience , adc values were moderately higher than those reported in the literature , presumably because our protocol involved lower b values ( 0800 mm / s2 ) than used by most authors ( 01 , 000 ) , a decision dictated by the need to obtain a high signal - to - noise ratio even with a four - channel coil . 
however , we did della rm in alcuni studi [ 20 , 23 ] , secondo altri autori alquanto inferiore [ 16 , 32 ] : in particolare , la dwi dimostra difficolt nel riconoscere lesioni con diametro inferiore a 810 mm , nelle quali non al momento possibile determinare con certezza i valori di adc [ 15 ]  . 
il rischio di una valutazione non del tutto attendibile della velocit di diffusione dellacqua nelle lesioni di dimensioni esigue ha indotto ad escludere da questo studio i reperti con diametro pari o inferiore a 6 mm , sebbene nellesperienza personale alcune formazioni con maggior asse di 5 e 6 mm , ben evidenti allindagine rm , siano state correttamente inquadrate mediante dwi . in questo studio , adottando i valori di cut off pi appropriati secondo lesperienza personale , laccuratezza della dwi nella diagnosi differenziale fra lesioni benigne e maligne risultata pari al 92 , 3% ( tabella 3 ) , ovvero lievemente superiore a quella riportata dai pi ottimistici fra i lavori presenti in letteratura : i dati pubblicati oscillano infatti fra l83 , 6% ed il 91% [ 14 , 15 , 29 , 33 ]  . 
sensibilit e specificit sono ovviamente influenzate dai cut off di adc scelti dai singoli autori , i quali oscillano allinterno di un intervallo piuttosto ampio ( da 1 , 1 a 1 , 610 - 3 mm2 / s ) ; nellesperienza personale si ottengono ferma restando laccuratezza globale del 92 , 3% sensibilit dell88 , 6% e specificit del 95 , 3% ponendo il cut off a 1 , 48 , parametri che diventano rispettivamente 100% e 86% se il valore scelto aumentato a 1 , 52 ( tabella 3 )  . 
1a , b scansioni rm assiali dinamica ( a ) e pesata in diffusione ( b ) di una mammella destra dove si dimostra la presenza di una lesione rotondeggiante a margini spiculati . 
2a , b axial dynamic magnetic resonance image ( a ) and diffusionweighted image ( b ) showing a rounded spiculated lesion in the left breast . both the enhancement pattern and the apparent diffusion coefficient value ( region of interest 1.10 ) are typical of a malignant lesion . 
2a , b scansioni rm assiali dinamica ( a ) e pesata in diffusione ( b ) dove si dimostra la presenza di una lesione rotondeggiante a margini spiculati nella mammella sinistra . 
listologia ha dimostrato un carcinoma duttale nas . not perform this evaluation in our series , as we restricted out analysis to focal lesions and had very few cases of normal breast tissue at histology ( tables 1 and 2 )  . even though relatively few reports exist on the subject , among the possible causes of false negative results in addition to the low cellularity of some histological types such as scirrhous [ 14 ] , lobular [ 29 ] , apocrine [ 21 ] and radiol med ( 2011 ) 116 : 264275 in tutti i lavori di cui siamo a conoscenza risulta statisticamente significativa la differenza fra i valori medi di adc misurati nelle lesioni maligne ( compresi , a seconda dei valori di b adottati , fra 0 , 95 e 1 , 22 ) e in quelle benigne ( 1 , 441 , 67 ) [ 1416 , 19 , 20 , 23 , 28 , 29 , 32 , 33 ]  . 
nellesperienza personale i valori di adc sono modestamente superiori a quanto riportato in letteratura , presumibilmente in conseguenza delladozione , nel nostro protocollo , di valori di b ( 0800 mm / s2 ) pi bassi di quelli utilizzati dalla maggior parte degli autori ( 01000 ) : tale scelta stata motivata dallintenzione di ottenere un rapporto segnale / rumore elevato anche con la bobina a 4 canali impiegata in questo studio . 
la nostra casistica priva di falsi negativi con la scelta del cut off sensibile di 1 , 52 ne annovera 4 adottando il cut off specifico di 1 , 48 . 
in tre evenienze ( tabella 1 ) lerrore stato sostenuto da carcinomi duttali infiltranti nas ( peraltro ampiamente prevalenti fra le lesioni maligne riscontrate in questa casistica ) ; del quarto caso di falsa negativit stata invece fig . 
4a , b axial dynamic mri ( a ) and diffusion - weighted image ( adc ) ( b ) showing a rounded , irregularly margined lesion in the remaining portion of a left breast after quadrantectomy . 
4a , b scansioni rm assiali dinamica ( a ) e pesata in diffusione ( b ) dimostranti la presenza di una lesione rotondeggiante a margini irregolari nella porzione rimanente di una mammella sinistra dopo quadrantectomia . 
laspetto rm suggerisce una recidiva di malattia , mentre il valore di adc ( molto basso : 1 , 32 ) tipico di una lesione maligna ; tuttavia listologia ha dimostrato una zona di steatonecrosi . 
 mucinous [ 15 ] carcinomas is the possible presence of fluid areas capable of raising the adc values , such as areas of haemorrhage and intratumoural necrosis [ 15 , 29 ]  . 
our series , which did not yield any false negative results when the sensitive cutoff value of 1.52 was selected , revealed only four false negatives with the specific cutoff value of 1.48. 
in three cases ( table 1 ) , the error was due to infiltrating ductal carcinomas nos ( the most common malignancy in our series ) ; in the fourth case , the false negative result was related to carcinomatous mastitis , in which it is reasonable to suppose that the lack of a well - defined focal lesion may have misled both the mri and dwi study the latter with regard to the choice of the roi . the high cellularity typical of some benign lesions ( intraductal papilloma and fibrocystic mastopathy ) has been implicated [ 14 , 29 , 31 ] as the possible cause of false positive dwi findings . 
the lowest adc values were recorded in a case of fibrocystic mastopathy ( 1.45 ) , a finding consistent with previous reports [ 14 , 29 ] and , surprisingly , in a case of fat necrosis . 
to our knowledge , the literature offers no explanation for this finding : however , it may be speculated that the naturally hydrophobic complex lipids leaking out of necrotic fat cells form an insurmountable barrier to the motion of water molecules and thus significantly reduce diffusion velocity . in our study , given the small number of patients and the responsabile una forma di mastite carcinomatosa , nella quale lecito supporre che lassenza di una lesione focale ben delimitata abbia verosimilmente ingannato sia lindagine rm che quella dwi , questultima forse nella fase di scelta della regione di interesse . la elevata cellularit di alcune lesioni benigne ( papillomi intra - duttali e mastopatia fibrocistica ) stata invocata in letteratura [ 14 , 29 , 31 ] per giustificare i reperti dwi di falsa positivit . 
nella nostra serie il numero di falsi positivi ( tabella 2 ) , adottando il cut off sensibile di 1 , 52 , pari a 6 ( 3 fibroadenomi , 2 casi di mastopatia fibrocistica ed un caso di steatonecrosi ) ; la cifra si riduce a 2 con il cut off specifico di 1 , 48 . 
i valori pi bassi di adc sono stati misurati in un caso di mastopatia fibrocistica ( 1 , 45 ) , reperto compatibile con i dati della letteratura [ 14 , 29 ] e , piuttosto sorprendentemente , in un caso di steatonecrosi . 
non siamo a conoscenza di spiegazioni pubblicate in merito nella letteratura : possiamo ipotizzare che fuoriusciti dalla lipidi complessi membrana di cellule adipose necrotiche costituiscano , per il loro naturale comportamento idrofobico , un ostacolo difficilmente sormontabile allo spostamento delle molecole di acqua , riducendo pertanto significativamente la velocit di diffusione rilevata . in questo studio , stante la consistenza numerica della casistica e la ripartizione qualitativa delle lesioni maligne ( tabelle 1 e 2 ) , non stato possibile espletare valutazione statistica riguardo alleventuale correlazione tra valori di adc e tipo istologico , correlazione affermata da alcuni 274 radiol med ( 2011 ) 116 : 264275 qualitative distribution of malignant lesions ( tables 1 and 2 ) , we were unable to perform a statistical evaluation of the possible correlation between adc and histology a correlation supported by some authors [ 15 , 35 , 39 ] but refuted by others [ 19 ]  . this study has some limitations . 
because we selected only patients with lesions deserving investigation with mri and , among them , only those requiring pathological characterisation , our series does not contain findings with a low index of suspicion , the presence of which might have reduced the diagnostic performance of dwi . 
the roi in which to determine the adc was selected by the operator on the basis of a subjective judgement on the mri and may not have accurately reflected the behaviour of the entire lesion . in conclusion , we believe that dwi , an inexpensive and relatively rapid technique , is a useful diagnostic complement for characterising focal breast lesions in patients undergoing mri , even though it is as yet unable to avoid the need for pathological characterisation . autori [ 15 , 35 , 39 ] , ma negata da altri [ 19 ]  . 
essendo state selezionate solo pazienti portatrici di lesioni giudicate meritevoli di essere sottoposte a rm e fra queste quelle nelle quali si ritenuto necessario il ricorso alla tipizzazione anatomo - patologica , la casistica non contiene reperti con livello di sospetto basso la cui presenza potrebbe ridurre lefficacia diagnostica della dwi . 
marini4 1radiologia durgenza , ospedale san camillo , c.ne gianicolense 87 , 00152 roma , italy 2dipartimento di otorinolaringoiatria , sapienza universit di roma , italy 3radiologia generale , ospedale san camillo , roma , italy 4dipartimento di scienze radiologiche , sapienza universit di roma , italy correspondence to : a . 
 keywords computed tomography magnetic resonance chronic otitis media preoperative assessment riassunto scopo del presente lavoro puntualizzare limportanza dellimaging integrato con tomografia computerizzata ( tc ) ed risonanza magnetica ( rm ) nella gestione dellotite media cronica , con particolare riguardo alle informazioni chiave necessarie allotoiatra per una corretta pianificazione della terapia chirurgica . parole chiave tomografia computerizzata risonanza magnetica otite media cronica valutazione preoperatoria introduction introduzione due the ever - growing role of computed tomography ( ct ) and magnetic resonance imaging ( mri ) in evaluating the temporal bone , many authors [ 17 ] have studied the middle ear after a surgical procedure , whereas only a few [ 8 , 9 ] , and not recently , have focused on the relevant aspects of these techniques for a more accurate preoperative planning in chronic otitis media ( com )  . 
when treatment regime , either surgical or conservative , a seguito del crescente impiego della tomografia computerizzata ( tc ) e della risonanza magnetica ( rm ) nello studio dellosso temporale , numerosi autori hanno affrontato il tema dellorecchio medio operato [ 17 ] , mentre pochi lavori , e nessuno di recente , sono focalizzati sugli aspetti rilevanti per un corretto planning preoperatorio dellotite media cronica ( omc ) [ 8 , 9 ]  . 
quando il trattamento chirurgico , pur non programmato , radiol med ( 2011 ) 116 : 114124 upon , represents an option to be evaluated after failure of medical treatment . 
a negative ct scan thanks to its high negative predictive value is able to exclude the presence of a significantly sized cholesteatoma in the dry middle ear [ 10 ]  . 
in the chronically inflamed ear , however , different tissue components may be present at the same time , and their characterisation may determine treatment decisions ( whether conservative or surgical )  . 
la tc , grazie ad un elevato potere predittivo negativo in grado di escludere la presenza di un colesteatoma di dimensioni significative nellorecchio medio ben aerato [ 10 ]  . il materiale patologico pi frequentemente riscontrabile con tc in corso di omc il tessuto di granulazione , che non provoca generalmente erosioni n dislocazioni della catena ossiculare [ 11 ]  . 
nellorecchio cronicamente infiammato , tuttavia , possono coesistere varie componenti tissutali , la caratterizzazione delle quali pu condizionare in modo decisivo la scelta di un approccio conservativo o chirurgico : se lorecchio contiene essudato , tessuto di granulazione o fibrosi , il trattamento dipende soprattutto da fattori clinici ( stato uditivo dellorecchio , entit delle secrezioni , ecc . ) , mentre la dimostrazione di un granuloma colesterinico o di un colesteatoma impone generalmente un approccio chirurgico . 
 la diagnosi differenziale tra i tessuti che possono riscontrarsi nellorecchio medio non possibile in tc su rilevazioni densitometriche [ 10 , 12 ] e dovrebbe basarsi sul riconoscimento di precisi segni elementari : ispessimento mucoso , segni di versamento , segni di lesione occupante spazio . 
nellorecchio parzialmente aerato tale semeiotica pu essere impiegata con la massima efficacia , mentre in un orecchio completamente opacato , la discriminazione tra le varie componenti diventa inattendibile [ 13 , 14 ] e richiede limpiego di rm con sequenze in diffusione ed acquisizioni multifasiche dopo somministrazione di mezzo di contrasto ( mdc ) endovena ( ev ) [ 1517 ]  . 116 radiol med ( 2011 ) 116 : 114124 exudate , granulation tissue or fibrosis , treatment depends above all on clinical factors ( auditory state , extent of secretions , etc . ) , whereas demonstration of a cholesterol granuloma or cholesteatoma normally warrants a surgical approach . 
 differential diagnosis among the various tissues that might be detected in the middle ear is not possible by densitometric ct analysis [ 10 , 12 ] and should be based on precise evidence : mucosa thickening ; signs of effusion or a spaceoccupying lesion . 
in a partially aerated ear , such analysis can be effectively carried out , but in an entirely opacified ear , differentiation among the various components is totally unreliable [ 13 , 14 ] and may require the use of mri with diffusion - weighted imaging ( dwi ) and delayed contrastenhanced postgadolinium sequences [ 1517 ]  . ct depiction of the middle - ear mucosal lining always suggests inflammation [ 10 ] , whereas the diagnosis of effusion is based on the presence of gasfluid levels within the partially opacified ear . 
detecting an occupying - space lesion is compatible with both inflammatory ( granulomatous polyps , unusually extensive fibrous scarring foci , cholesterol granulomas , cholesteatomas ) and noninflammatory processes ( such as glomus tympanicum , the most frequent tumour occurring in the middle ear ) and is based identifying , even partially , lesion margins , dislocation / lysis of ossicular elements , surrounding bone walls of the middle ear and protrusion of the tympanic membrane . 
once the presence of a spaceoccupying lesion has been determined , its characterisation may be based on direct ( margins , density , signal , epicentre ) or indirect ( associated changes to the ossicles and middleear walls )  . 
the correlation between the condition of the ossicular chain as depicted by ct and as seen at surgery is controversial [ 2225 ]  . la visibilit del rivestimento mucoso dellorecchio medio sempre segno di flogosi [ 10 ] , mentre la diagnosi di versamento si basa sulla dimostrazione di livelli idroaerei nel contesto dellorecchio parzialmente opacato . la dimostrazione di una lesione occupante spazio compatibile con patologie flogistiche ( polipo granulomatoso , focolai fibrocicatriziali insolitamente ampi , granuloma colesterinico , colesteatoma ) e non flogistiche ( ad esempio , glomo timpanico , il pi frequente tumore dellorecchio medio ) e si basa sul riconoscimento almeno parziale dei margini della lesione , sulla dislocazione / lisi degli elementi ossiculari , sul rimaneggiamento espansivo o litico delle circostanti pareti ossee dellorecchio medio , sullestroflessione della membrana timpanica . 
stabilita la presenza di una lesione occupante spazio , la sua ulteriore caratterizzazione pu essere effettuata su segni diretti ( margini , densit , segnale , epicentro ) ed indiretti ( alterazioni associate degli ossicini e delle pareti dellorecchio medio )  . 
granuloma colesterinico : tessuto epitimpanico iperintenso in t1 e t2 ( non mostrata )  . of particular interest for the surgeon is assessment of the incudostapedial joint and the stapes . 
lapproccio canal - up necessita di una accesso pi ampio , possibilmente attraverso un sistema cellulare ampio , mentre lapproccio canal - down preferibile nelle mastoidi sclerotiche [ 9 ]  . natura dei tessuti la mastoidectomia nelle otiti croniche non colesteatomatose non sembra presentare sicuri vantaggi rispetto alla sola timpanoplastica , associandosi peraltro ad un maggior rischio di complicanze operatorie [ 26 ]  . estensione di malattia nellosso temporale anche quando la diagnosi natura della lesione ( ad esempio , un colesteatoma ) otoscopicamente certa , resta da determinare la reale estensione della patologia : lotoscopia infatti potrebbe non evidenziare che la propaggine pi superficiale di una lesione imprevedibilmente estesa . 
descrivere con propriet la / le sede / i entro i cui limiti confinata la lesione ( cassa timpanica , attico , antro , tuba , labirinto , fossa media ) determinante ai fini della scelta chirurgica . 
the radiologist , however , should be very cautious in providing a diagnostic aetiology in the absence of adequate otoscopic ( lesion colour and pulsatility ) and clinical ( characteristics of otorrhea , tinnitus and type of associated hypoacousia ) findings . preoperative planning temporal - bone cellularity it is important to define the general architecture of the mastoid process by considering a pneumatised mastoid as the opposite of a sclerotic mastoid . 
the approach to a closed and intact canal wall requires a wide access , ideally through a large cellular mastoid , whereas a in smaller canal - wall - down approach is preferable estensione di malattia nellorecchio medio propriamente detto sedi di particolare interesse chirurgico sono il recesso epitimpanico anteriore , il seno timpanico ed il recesso del facciale . 
the modified radical cavity of larger cellular systems holds poorer prospects for healing . equally , the intact canal wall technique in a tiny mastoid cavity is technically difficult because of its poor access [ 9 ]  . fistola labirintica nature of the tissues compared with tympanoplasty alone , mastoidectomy for noncholesteatomatous com does not seem to be advantageous , and procedure - related complications with this technique occur in a higher number of patients [ 26 ]  . 
 disease extension to the temporal bone the diagnostic origin of a lesion ( e.g. , a once cholesteatoma ) is otoscopically confirmed , its real extension should then be determined . 
accurately describing the lesions site ( s ) and boundaries ( tympanic cavity , attic , antrum , eustachian tube , labyrinth , middle fossa ) is vitally important in surgical planning . 
smaller lesions can be treated by targeted and minimally invasive procedures , whereas lesions involving three or more of the abovementioned spaces usually require a radical mastoidectomy [ 2729 ]  . la presenza di una fistola labirintica in caso di colesteatoma varia dal 3 , 6% [ 39 ] al 12 , 9% [ 40 ]  . 
la presenza di pneumolabirinto un segno certo di fistola , ma di raro riscontro . fistole del canale semicircolare laterale ( csl ) o della coclea sono di agevole dimostrazione , perch associate a discontinuit del relativo rivestimento osseo . 
difficile la dimostrazione di fistole della finestra rotonda , che ricoperta da unesile membrana invisibile in tc : il sospetto suggerito dalla sola presenza di tessuto loco - regionale ed avvalorato da aspetti erosivi dellosso circostante ; la dimostrazione di fluido isolato nel seno del timpano ( fluidi endolabirintici scolati nella cassa timpanica ) un segno altamente sospetto . 
anche nel caso di fistola della finestra ovale deve essere valorizzata la semplice presenza di tessuto nellomonima fossa , specialmente in presenza di erosioni ossee ; la compresenza di aspetti erosivi della staffa , la sua frammentazione o dislocazione nella finestra ovale sono particolarmente suggestivi di fistola [ 42 ]  . 
 deiscenza dei tegmina la discontinuit ( deiscenza ) del tetto dellorecchio medio radiol med ( 2011 ) 116 : 114124 disease extension in the middle ear as such the anterior epitympanic recess , the tympanic sinus and the facial recess are anatomical sites of particular surgical interest . 
the presence of a pneumolabyrinth is a definite sign of fistulas , but its detection is unusual ; lateral semicircular canal or cochlear fistulas are instead easily depicted , since their presence is associated with a discontinuity of the related bone layer . 
depicting fistulas of the round window , which is covered by a thin membrane not visualised by ct , is difficult ; a clue is provided by the presence of locoregional tissue , whereas signs of erosion of the surrounding bone corroborate the diagnosis . as an additional sign , demonstration of an isolated collection within the tympanic sinus ( endolabyrinthine fluids draining within the tympanic cavity ) is highly suspicious for fistula formation . 
even in the case of fistulas of the oval window , the mere presence of tissue in the oval fossa should be highlighted , especially if bone erosions are also present . 
fistola del canale semicircolare laterale ( freccia corta ) e superiore ( freccia lunga )  . deve essere segnalata perch si associa al rischio di lesioni infiammatorie durali o cerebrali ( lobo temporale ) nella sovrastante fossa cranica media . 
 complicanze endocraniche tra le possibili complicanze endocraniche dellotite media , meningite , trombosi dei seni durali ed empiema subaracnoideo sono caratteristiche delle otiti medie acute ; lascesso cerebrale ( del lobo temporale o del cervelletto ) invece di solito una complicanze dellotite cronica [ 43 ]  . lascesso facilmente dimostrabile in rm e dovrebbe essere escluso ogni qual volta si apprezzi una deiscenza delle limitanti ossee per la fossa posteriore o per la fossa media ( tegmina ) di un orecchio non precedentemente operato contenente materiale infiammatorio . 
 tegmina dehiscence elementi anatomici caratteristici del paziente any discontinuity ( dehiscence ) of the tegmen tympani should be noted , as it might be associated with the risk of a dural or cerebral ( temporal lobe ) inflammatory lesion in the overlying middle cranial fossa . procidenza della dura madre la dura madre della fossa cranica media generalmente separata dal lume del condotto uditivo estgerno ( cue ) da radiol med ( 2011 ) 116 : 114124 uno strato di cellule aeree dette tegmentali ( cio del tetto del cue ) ; lassenza di tali cellule mette la dura in diretta apposizione con il periostio del cue e limita laccesso alladitus e allepitimpano per il conseguente rischio di lesione iatrogena della dura e del lobo temporale . 
 procidenza e deiscenza del seno laterale il seno laterale separato dalla parete posteriore del cue da una distanza variabile ; considerato procedente quando la sua distanza dalla parete posteriore del cue < 10 mm e costituisce un rischio chirurgico [ 44 ] anomalie di decorso o deiscenze del seno laterale sono riscontrabili in circa il 2%3% dei pazienti [ 45 ]  . il bulbo giugulare si pone in circa il 6% dei casi al di sopra del livello dellannulus timpanico inferiore ( bulbo giugulare alto ) [ 46 ] interferendo potenzialmente con lapproccio chirurgico . 
oltre ad essere altoposto , il bulbo giugulare pu mancare del suo normale rivestimento osseo ( settoipotimpano giugulare ) e trovarsi in diretta apposizione con tessuto patologico nellorecchio medio ( rischio di flebite e trombosi ) oppure a rischio di lesione iatrogena per lesioni ipotimpaniche o interessanti le celle retrofacciali o durante il sollevamento di un flap timpanomeatale . 
 [ 47 , 48 ]  . decorso della carotide interna la deiscenza della carotide rara ( 1 , 4% ) [ 44 ] e mette il paziente a rischio di una grave emorragia arteriosa anche anatomical characteristics of the patient bulging of the dura mater bulbo della giugulare endocranial complications among the various possible endocranial complications of com , meningitis , dural sinus thrombosis and subarachnoid empyema are typical of acute otitis media ; a cerebral abscess ( of the temporal lobe or the cerebellum ) is , instead , usually a complication of chronic otitis [ 43 ]  . 
an abscesseasily depicted by mri - should be excluded whenever posterior or middle cranial fossa are exposed to pathological tissues in the middle ear by dehiscence of the adjacent bone structures . the dura mater of the middle cranial fossa is usually separated by the lumen of the external auditory canal by an aircell layer ( tegmental cells )  . 
the absence of these cells places the dura mater directly in touch with the periosteum of the external auditory canal and limits access to the aditus and the epitympanum due to the related risk of iatrogenic lesions to the dura mater and temporal lobe . 
course anomalies or dehiscences of the lateral sinus are detected in about 2%3% of patients [ 45 ]  . jugular bulb in approximately 6% of cases , the jugular bulb is placed above the level of the lower annulus tympanicus ( high jugular bulb ) [ 46 ] , thus precluding translabyrinthine approaches . 
in addition to this anomaly , if the normal covering bony layer is also missing , the jugular bulb is directly juxtaposed to the pathological tissue of the middle ear , thus being at risk of thrombosis / phlebitis or of an iatrogenic lesion induced by hypotympanic traumas or involving retrofacial cells , or during the raising of a tympanomeatal flap [ 47 , 48 ]  . internal carotid course carotid dehiscence is rare ( 1.4% ) [ 44 ] and may induce a serious arterial haemorrhage , even during minor inpatient fig . 
an aberrant carotid artery is an extremely rare event and is due to the lack of cervical segment development of this vessel [ 45 ] and is frequently associated with the presence of an aberrant stapedial artery . 
una carotide aberrante estremamente rara e dovuta al mancato sviluppo del segmento cervicale della carotide interna [ 45 ] , in associazione alla presenza di una arteria stapediale persistente . un prelievo bioptico o una lesione chirurgica possono in tal caso provocare grave emorragia od ictus cerebrale . conclusions conclusioni imaging techniques provide key elements in managing com : ct is able to reliably exclude the presence of middleear anomalies , whereas characterisation of pathological tissues , which is ideal but not always possible despite the use of both ct and mri , remains mainly dependent on the combined evaluation of clinical , otoscopy and biopsy findings . 
la caratterizzazione dei tessuti patologici altamente desiderabile ma non sempre possibile , nonostante limpiego combinato di tc ed rm , restando spesso legata alla valutazione integrata di dati clinici , otoscopici e bioptici . 
guney1 1department of radiology , 2department of cardiology , 3department of psychiatry , maltepe university school of medicine , feyzullah cad , no : 39 , 34843 , maltepe , istanbul , turkey correspondence to : r . 
2016 , fax : + 90 - 216 - 3830271 , e - mail : rahmicubuk@yahoo.com received : 24 november 2009 / accepted : 2 march 2010 / published online : 17 september 2010 springer - verlag 2010 abstract purpose . 
the participating patients were randomly assigned to one of the two study groups : a control group ( no medication administered for anxiety reduction ) and an anxiolytic medication group , with 30 patients in each group . 
the presence of motion artefacts and image quality for each coronary artery segment were evaluated using a four - point grading systeto estimate hrv , the duration of each heartbeat during mdct data acquisition was measured in each patient . 
i pazienti che hanno partecipato allo studio sono stati casualmente assegnati ad uno dei due gruppi di studio : il gruppo di controllo ( ai quali non veniva somministrato ansiolitico per ridurre lo stato dansia ) ed il gruppo dei pazienti trattati con ansiolitici , questultimo composto da 30 pazienti . 
stata riscontrata una moderata correlazione tra la variabilit della frequenza cardiaca ( hrv ) durante lacquisizione delle immagini mdct e la media della qualit dellimmagine per tutti i segmenti coronarici studiati ( r = 0 , 47 , p < 0 , 01 )  . 
vi era una concordanza tra la variabilit della frequenza cardiaca ( hrv ) ed il livello dansia in tutti i radiol med ( 2011 ) 116 : 4755 that oral premedication to reduce anxiety is also effective in decreasing hrv and improves image quality . 
we also suggest that further studies in larger series are required to validate this finding . keywords multidetector computed tomography coronary angiography heart rate benzodiazepines premedication casi ( r = 0 , 370 , p < 0 , 01 )  . 
la variabilit della frequenza cardiaca ( hrv ) nei pazienti trattati con alprazolam era significativamente pi bassa che nei controlli ( p < 0 , 05 )  . anche la qualit delle immagini nei pazienti trattati con alprazolam era significativamente pi elevata che nei controlli ( p < 0 , 05 )  . 
il riscontro del nostro studio che la premedicazione con ansiolitici per via orale riduce lo stato dansia ed efficace anche nel ridurre la variabilit della frequenza cardiaca ( hrv ) e nel migliorare la qualit delle immagini . 
pertanto , suggeriamo che lutilizzo dellalprazolam in combinazione con gli - litici potrebbe migliorare la qualit delle immagini nei pazienti sottoposti ad angiografia coronarica mediante tc multidetettore ( mdct - ca )  . 
 parole chiave tomografia computerizzata multidetettore angiografia coronarica frequenza cardiaca benzodiazepine premedicazione introduction the main limitation to the use of multidetector row computed tomography ( mdct ) in coronary angiography ( ca ) is temporal resolution [ 13 ]  . 
with the introduction of 64 - detector mdct , the problem of temporal resolution has been substantially resolved , but image quality remains poor in patients with high heart rates ( hr ) [ 35 ]  . 
in another study in which they compared mdct - ca and invasive ca , they reported that a low hrv increases the diagnostic accuracy of 64 - detector mdct - ca [ 7 ]  . 
currently , - blocker administration for premedication is used as the standard procedure to reduce hr in ca performed by mdct with low detector counts , including 64 detectors [ 811 ]  . 
it is reported that blocker administration increases image quality by reducing the hr or , additionally , the hrv [ 6 , 7 ]  . as in many medical procedures , patients can be stressed before undergoing mdct - ca , and the complication rates increase due to impaired patient compliance [ 12 , 13 ]  . 
in addition to the stress originating from mdct imaging , the potentially bad results of the examination can produce high anxiety , especially in patients with coronary artery disease ( cad ) for whom the outcome is of vital importance . we performed a literature review and could find no study evaluating the relationship between the use of anxiolytic premedication before mdct - ca , patients anxiety status and hrv / image quality . 
therefore , the purposes of this study were to investigate the relationship between image quality in 64 - detector mdct and preimaging anxiety status and hrv and to evaluate the efficacy of an orally administered anxiolytic medication on hrv and image quality . materials and methods patient population a total of 91 patients were referred for mdct - ca due to radiol med ( 2011 ) 116 : 4755 table 1 demographic and clinical data of patients with and without alprazolam medication tabella 1 dati demografici e clinici dei pazienti trattati e non trattati con alprazolam characteristics total p value no . 
of patients age ( years ) male - to - female ratio body mass index ( kg / m2 ) average heart rate ( beats / min ) heart rate variability ( beats / min ) a family history hypertension hyperlipidaemia diabetes mellitus smoking no . 
we also excluded 11 patients who had a history of anxiety reduction medication or coronary artery bypass surgery , although they were examined with mdct . at the time of ct , 23 ( 38.3% ) patients were taking receptor antagonists ( n = 18 ) and calcium - channel blockers ( n = 5 )  . 
there were no statistically significant differences in patients ages , body mass index ( bmi ) , gender , average hr , risk factors or chronic consumption of cardiovascular drugs between the two subgroups . 
 anxiety assessment method all patients anxiety levels were assessed with the statetrait anxiety inventory ( stai ) 60 min before the procedure by an investigator ( pg ) [ 19 ]  . 
the stai is a 40 - item self - reported questionnaire ( 20 state anxiety statements and 20 trait anxiety statements )  . responses to each of the 40 questions are given according to a scoring scale from 1 ( not at all ) to 4 ( very much so )  . each anxiety score can range between 20 and 80 . 
the test has been validated in various patient groups and college students [ 19 ]  . the participating patients were randomly assigned to one of the two study groups : a control group ( no medication administered for anxiety reduction ) and an anxiolytic medication group . 
the scan parameters were 640.5 - mm detector collimation , pitch 0.20.45 ( depending on hr ) , rotation time 400 ms , tube voltage 120 kv , current 600900 effective mas . 
electrocardiogram ( ecg ) - dependent tube current modulation was applied in regular hrs < 65 bpm . scan direction was craniocaudal during a single midinspiratory breath - hold . a bolus of 80 ml iodine contrast agent iobitridol ( xenetix 350 , 350mg / ml ; guerbet , france ) was administered intravenously into an antecubital vein at a flow rate of 56 ml / s using a dual - head power injector , followed by 50 - ml saline chaser ( 5 ml / s )  . 
the scanning range covered the entire heart from the level of the tracheal bifurcation to the diaphraga - blocker was given intravenously before the mdct scan if the hr was > 70 beats per min ( 515 ml metoprolol ) , regardless of grouping . 
none of the patients reported any discomfort due to the ct protocol or the use of contrast media or alprazolam medication . mdct image reconstruction and analysis during the scan , ecg was recorded simultaneously . 
images were reconstructed with a section thickness of 0.5 mm , a reconstruction increment of 0.3mm , image matrix 512512 and fov of 180240 m data were transferred to software vitrea 2 workstation ( vital images inc . , plymouth , mn , usa ) , and images were reconstructed with multiple postprocessing methods . mdct images were evaluated and classified by two radiologists ( rc , nt ) experienced in cardiovascular radiology . when the two radiologists had different opinions , the final decision was obtained by consensus . 
segmental evaluation of the coronary arteries was performed according to the american heart associations ( aha ) 15 - segment classification [ 20 ] : right coronary artery ( rca ) 14 ; left main ( lm ) and left anterior descending artery ( lad ) 510 ; left circumflex artery ( lcx ) 1115 . 
the presence of motion artefacts and image quality for each coronary artery segment were evaluated in a semiqualitative fashion using a four - point grading system , where a score of 1 indicates no motion artefacts , radiol med ( 2011 ) 116 : 4755 clear delineation of the segment ; a score of 2 indicates good , with minor artefacts , mild blurring of the segment ; a score of 3 indicates adequate , with moderate artefacts , moderate blurring without structure discontinuity ; and a score of 4 indicates nonevaluable , with doubling or discontinuity in the course of the segment preventing evaluation or vessel structures not differentiable . from the recorded ecg information , the hr in each cardiac cycle was noted by another author ( sy ) , who did not participate in image assessment . 
from this set of measurements , the variability in hr during scanning was calculated as the sd from the average hr [ 6 ]  . statistical analysis the statistical software ncss 2007 & pass 2008 ( ut , usa ) was used for statistical analyses . 
in analysing the study data , students t test was used to evaluate parameters with a normal distribution between groups for quantitative data , besides descriptive statistical methods ( mean , sd , frequency ) ; and the relationships between parameters were tested by pearsons correlation analysis and linear regression analysis . 
chi - square test and fishers exact test were used to analyse categorical data in the two groups . results were evaluated at 95% confidence interval ( ci ) at the significance level p < 0.05. results the average hr was 60.79.6 ( range 4494 beats per min )  . a total of 17 cases ( 28% ) had stable heartbeat , and there was only one to two beats difference during the whole mdct imaging [ 6 ]  . 
heart rate showed mild / moderate variability within a range below and above baseline values in the other cases ( 65% )  . image quality of the coronary arteries a total of 881 coronary artery segments were evaluated . nineteen segments could not be evaluated due to a very low calibre ( < 1.5 mm ) or anatomical variations . 
the best reconstruction interval was used to evaluate image quality . percentages for the coronary segment scores observed were 65% ( 575 / 881 ) for score 1 , 26% ( 226 / 881 ) for score 2 and 8% ( 69 / 881 ) for score 3 . 
1a - d curved multiplanar reformations of 64 - slice multidetector computed tomography ( mdct ) images of right coronary artery ( rca ) in patients with four different semiquantitative four - point image - quality scores . 
1 a - d immagini di ricostruzione mpr - curved , ottenute con tc multidetettore a 64 strati , dellarteria coronaria destra ( rca ) in pazienti con quattro differenti punteggi semiquantitativi di qualit dellimmagine , calcolati in base a quattro punti . 
although there was a weak negative association between hrv and state anxiety scores ( r = - 0.104 , p > 0.05 ) and trait anxiety scores ( r = - 0.315 , p > 0.05 ) in patients who received alprazolam , it was not statistically significant . 
on the other hand , there was a statistically significant positive relationship between hrv and state anxiety scores ( r = 0.636 , p < 0.01 ) and trait anxiety scores ( r = 0.610 , p < 0.01 ) in patients who did not use alprazolam . discussion in bearing with previous studies [ 4 , 6 , 7 ] , a correlation was found between hrv and mean image quality of all coronary segments . 
hrv was lower and image quality higher in patients who received alprazolam when compared with the control group . it has been reported that hrv occurring during mdct imaging influences image quality [ 4 , 6 , 7 ]  . 
in their study using 64 - detectorrow mdct , they reported that hrv is associated with mean image quality of all coronary segments , and in particular , rca is more heavily affected by hrv [ 6 ]  . 
dualsource mdct - ca is reported to be sufficient for diagnosis in high hr and hrv , but image quality deteriorates in the case of both high and variable hrs [ 4 ]  . 
image quality of rca , lad , lm and lcx deteriorated due to hrv in an order from higher to lower . the main limitation to the use of mdct - ca has been temporal resolution and cardiac motion . 
however , there was no statistically significant relationship between trait anxiety scores , which reflect how an individual feels independent of the situation and conditions ( a more general and longstanding condition ) , and hrv . 
it is remarkable that trait anxiety scores and hrv do not change . therefore , we can hypothesise that if we reduce the momentary anxiety in patients prior to mdct imaging , we can decrease the hrv and avoid deterioration in image quality . in our literature search , we could not identify any previous study related to anxiety reduction specifically for mdct - ca . benzodiazepines are the most commonly used anxiolytic drugs in the radiology department and are considered safe , with minimal respiratory and cardiovascular effects [ 12 ]  . alprazolam used in our study is one of the most frequently prescribed benzodiazepines for treating panic disorders [ 24 ]  . benzodiazepines act selectively on central g - aminobutyric acid ( gaba ) - a receptors and enhance response to the gaba inhibitory neurotransmitter . 
benzodiazepines inhibit increased noradrenergic activity in the locus ceruleus as well . according to the american society of anesthesiologists , the definition for minimal sedation ( anxiolysis ) is a drug - induced state during which patients respond normally to verbal commands . 
we think that oral alprazolam used in our study is a feasible anxiolytic premedication agent for use prior to mdct , with its short half - life , rapid effect , inexpensiveness and ease of use when compared with the other benzodiazepines . we achieved anxiolytic effect with oral alprazolam in our study without affecting respiratory and cardiovascular functions . 
nevertheless , it is known that in the presence of other central nervous system depressants , particularly alcohol , they may cause severe respiratory depression , especially in the elderly , children and critically ill patients , as they may result in apnoea [ 27 ]  . 
this kind of effect is out of scope of radiol med ( 2011 ) 116 : 4755 this particular study , as we excluded such patients initially . on the other hand , hrv decreased and image quality increased significantly in patients receiving alprazolam when compared with the control group . 
additionally , whereas hrv increased in parallel with the increase in state anxiety scores in patients not taking alprazolam , there was no such relationship in patients who received alprazolam . we drew the conclusion that alprazolam , used as an anxiolytic , breaks the vicious cycle comprising increased anxiety , increased noradrenergic activity , increased hrv and low image quality . the first limitation in our study was that we could not examine the individual effects of the - blocker and alprazolam on image quality . 
the reasons for this were the relatively small number of patients included in the study , preexisting usage of a - blocker by some patients or our use of a - blocker during mdct to reduce high hr . 
the second limitation was lack of patient demographic data other than age and gender , such as education , marital status and ethnicity , which may be related with stai evaluation . 
however , as our first aim was to lower the hrv and increase image quality rather than evaluate the effect of alprazolam on mood , we neither used combined placebo administration nor collected the postprocedure state anxiety scores of our patients . 
cademartiri1 , 2 1department of radiology and cardiology , azienda ospedaliero - universitaria , parma , italy 2department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands 3healthcare and social agency , regione emilia romagna , bologna , italy 4sdn foundation nuclear diagnostic institute , naples , italy 5department of radiology , university of verona , italy correspondence to : f . 
cademartiri , department of radiology , c / o piastra tecnica piano 0 ct section , azienda ospedalierouniversitaria di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703516 , fax : + 39 - 052 - 1704838 , e - mail : filippocademartiri@hotmail.com received : 31 december 2009 / accepted : 22 february 2010 / published online : 6 october 2010 springer - verlag 2010 abstract purpose . 
the authors investigated the prognostic value of computed tomography coronary angiography ( ctca ) for major adverse cardiac events ( mace ) in patients with suspected or known coronary artery disease ( cad ) , with particular focus on left main ( lm ) disease and obstructive vs . 
a total of 117 mace [ five cardiac deaths , 11 acute myocardial infarctions ( ami ) , five unstable angina , 86 percutaneous coronary interventions , ten coronary artery bypass grafts ] occurred during a mean follow - up of 20 months . 
settecentoventisette pazienti consecutivi ( 485 maschi , et 6211anni ) con cad sospetta ( 514 ; 70 , 1% ) o nota ( 213 ; 29 , 9% ) sono stati sottoposti a ctca . 
sono stati osservati un totale di 117 mace ( 5 morti cardiache , 11 ami , 5 angine instabili , 96 rivascolarizzazioni ) durante un follow - up medio di 20 mesi . 
la valutazione del carico aterosclerotico alla ctca ha un valore prognostico indipendente per i mace . i pazienti con coronarie normali mostrano prognosi eccellente . keywords computed tomography coronary angiography prognosis coronary artery disease left main disease major adverse cardiac events parole chiave angiografia tc delle coronarie prognosi malattia coronarica tronco comune eventi avversi cardiaci maggiori introduction introduzione coronary artery disease ( cad ) is the leading cause of death in the developed world . 
noninvasive imaging is widely used to establish the diagnosis in symptomatic patients with suspected cad and to evaluate cad progression in patients with known cad in order to further stratify the risk of cardiac events beyond clinical data and traditional cardiovascular risk factors . 
noninvasive evaluation is primarily performed using stress nuclear myocardial perfusion imaging and stress echocardiography , given their widely demonstrated diagnostic accuracy and prognostic value tomography coronary angiography [ 13 ]  . 
computed ( ctca ) has demonstrated high diagnostic accuracy for detecting obstructive cad compared with standard coronary angiography in selected populations , and it is increasingly used in the clinical setting as a gatekeeper to coronary angiography [ 47 ]  . 
 the aim of this study was to evaluate the prognostic value of ctca for major adverse cardiac events ( mace ) in patients with suspected or known cad , with particular focus on lm disease and obstructive vs . 
la valutazione di cad mediante test di imaging non invasivo largamente utilizzata nella diagnosi dei pazienti sintomatici con sospetta cad e nella valutazione della progressione di malattia nei pazienti con cad nota , al fine di ottenere una stratificazione del rischio di eventi cardiaci che vada oltre i dati clinici e i tradizionali fattori di rischio cardiovascolare . 
la valutazione viene eseguita , in prima istanza , mediante indagine non invasiva con test - stress nucleare di perfusione miocardica e stress ecocardiografico , per lelevata accuratezza diagnostica e valore prognostico di tali metodiche [ 13 ]  . 
langiografia tramite tomografia computerizzata ( tc ) delle coronarie ( ctca ) ha mostrato unelevata accuratezza diagnostica nella valutazione di cad ostruttiva quando confrontata allangiografia coronarica convenzionale , in una selezionata popolazione di pazienti , ed sempre pi utilizzata nel percorso clinico come apri porte allangiografia coronarica [ 47 ]  . 
 lo scopo di questo studio di valutare il valore prognostico della ctca per eventi avversi cardiovascolari maggiori ( mace ) in pazienti con cad sospetta o nota con particolare attenzione alla malattia del tronco comune ed al confronto tra malattia ostruttiva e non ostruttiva . 
exclusion criteria were renal failure ( creatinine clearance < 60 ml / min ) , known previous reaction to iodinated contrast materiali e metodi disegno dello studio e popolazione di pazienti questo uno studio retrospettivo osservazionale eseguito su 986 pazienti con cad sospetta o nota inviati al nostro istituto per una valutazione con ctca tra gennaio 2005 e aprile 2008 . 
the following risk factors were considered [ 8 ] : hypertension ( defined as arterial pressure 140 / 80 mmhg or need for antihypertensive therapy ) hypercholesterolaemia [ low - density lipoprotein ( ldl ) cholesterol > 130 mg / dl or current treatment with lipidlowering therapy ] diabetes mellitus ( current need for antidiabetic or insulin therapy ) smoking habit obesity [ body mass index ( bmi ) > 30 ] family history of cardiac disease . ( dolore toracico , dispnea sotto sforzo ) , test - stress dubbio o anormale ed elevato profilo di rischio cardiovascolare . invece , i criteri di esclusione sono stati insufficienza renale ( clearance della creatinina < 60 ml / min ) , allergia nota allagente di contrasto iodato e gravidanza . 
the clinical end points were : cardiac death nonfatal acute myocardial infarction ( ami ) unstable angina requiring hospitalisation percutaneous coronary revascularisation ( pci ) coronary artery bypass graft ( cabg )  . 
the end point was the occurrence of one mace at follow - up . ctca all examinations were performed with a single - source 64slice ct system ( sensation 64 cardiac , siemens , germany )  . 
ctca was performed after administration of 100 ml of nonionic contrast material ( iomeprol 400 mgi / ml , iomeron 400 , bracco , milan , italy ) at a flow rate of 45 ml / s depending on patient status . 
all injections were performed by dual - head power injector ( stellant , medrad , usa ) via an antecubital vein and were followed by 50 ml of saline bolus chaser at the same flow rate . 
ctca was performed with ( 322 ) 0.6 - mm collimation , 330 - ms gantry rotation time , i sintomi sono stati classificati come dolore toracico tipico , dolore toracico atipico , dispnea da sforzo . 
le i dati del follow - up sono stati raccolti a seguito di visita ambulatoriale o schede clinico / ospedaliere dei pazienti sono state sottoposte a screening per confermare gli eventi clinici di cui si avuto notizia . 
sono stati considerati i seguenti end - point : morte cardiaca ; infarto miocardico acuto ( ami ) non fatale ; ricovero per angina instabile ; intervento di rivascolarizzazione coronarico percutaneo ( pci ) ; bypass aorto - coronarico ( cabg )  . 
intravenous beta - blocker ( atenolol 510 mg ) was administered to all patients with a heart rate > 65 beats / min and without contraindication ( known asthma or bronchospasm , systolic blood pressure < 100 mmhg )  . 
to obtain optimal image quality , data sets were reconstructed at least at two points of the cardiac cycle using a retrospective ecg gating algorithm ( one diastolic cardiac phase usually at 350 ms from the r waves and one end - systolic phase at + 275 ms )  . 
coronary plaques were defined , as described previously [ 11 ] , as structures of > 1 mm2 within and / or adjacent to the coronary artery lumen , which are clearly distinguishable from the vessel lumen and surrounding pericardial tissue . 
patients were classified as belonging to one of three groups based on ctca findings : ( 1 ) patients with normal coronary arteries , ( 2 ) patients with nonobstructive coronary artery disease and ( 3 ) patients with obstructive coronary artery disease ( presence of at least one plaque > 50% )  . 
la ctca stata eseguita con i seguenti parametri di scansione : collimazione dello strato ( 322 ) 0 , 6 mm , tempo di rotazione del gantry 330 ms , 700900 mas ad una tensione del tubo di 120 kv , pitch 0 , 24 , risoluzione temporale di 165 ms , e risoluzione spaziale isotropica di 0 , 4 mm3 . 
i data - set sono stati ricostruiti con uno spessore di strato di 0 , 75 mm ed un incremento di 0 , 5 m tutti i pazienti con frequenza cardiaca > 65 battiti per minuto ( bpm ) e senza controindicazioni ( asma o broncospasmo noti , pressione sistolica < 100 mmhg ) hanno ricevuto uniniezione intra - venosa di beta - bloccante ( atenololo 510 mg )  . 
inoltre , stata somministrata una dose sublinguale di 0 , 3 mg nitroglicerina a tutti i pazienti senza controindicazioni ( stenosi aortica severa , pressione sistolica < 100 mmhg )  . 
per ottenere una qualit dimmagine ottimale , i data - set sono stati ricostruiti mediante gating elettrocardiografico ( ecg ) retrospettico in due fasi del ciclo cardiaco ( fase telediastolica , 350 ms prima dellonda r successiva , fase tele - sistolica , + 275 ms dopo londa r successiva )  . 
le ricostruzioni in asse corto sono state trasferite su di una workstation dedicata per le successive valutazioni ed il post - processing ( leonardo , siemens medical solutions , forchheim , germania )  . 
le placche coronariche sono state radiol med ( 2011 ) 116 : 1531 statistical analysis categorical baseline characteristics , expressed as numbers and percentages , were compared using the chi - square test . continuous variables , expressed as mean and standard deviation ( sd ) , were compared using the two - tailed t test and analysis of variance if normally distributed or by means of the kruskalwallis method if not normally distributed . 
 results patient population of 986 consecutive patients , 259 ( 26% ) were lost to followup ; therefore , 727 patients ( 485 men ; mean age 6211 years ) were available for the study . 
the majority of patients ( 514 , 70.1% ) were referred for suspected cad , whereas 213 patients ( 29.9% ) had a history of previous mi and / or previous coronary revascularisation by means of cabg or pci . 
patients with no history of cad and nonobstructive disease ( n = 237 ) were subclassified as follows : normal coronary arteries ( subgroup 1 ) , nonobstructive cad ( luminal stenosis < 50% ) in lm ( subgroup 2 ) , nonobstructive cad in other vessels ( subgroup 3 ) and nonobstructive cad in lm and other vessels ( subgroup 4 )  . 
patients with no history of cad and obstructive disease ( n = 103 ) were considered a single cohort . patients with a history of cad and nonobstructive disease ( n = 36 ) were subclassified as follows : normal coronary arteries ( subgroup 1 ) , nonobstructive cad in other vessels ( subgroup 2 ) and nonobstructive cad in lm and other vessels ( subgroup 3 )  . 
patients with a history of cad and obstructive disease ( n = 159 ) were considered a single cohort . definite , come precedentemente descritto [ 11 ] , come strutture > 1 mm2 situate allinterno / o adiacenti al lume del vaso , e chiaramente distinguibili da esso e dal tessuto pericardico circondate . 
le placche ostruttive sono state definite come placche determinanti un restringimento > 50% del lume del vaso ; mentre , le placche non ostruttive sono state definite come placche determinanti un restringimento 50% . 
sono stati messi a confronto i valori e le differenze mediante test t di student per dati appaiati , e mediante analisi della varianza se normalmente distribuiti oppure con il metodo kruskal - wallis . 
la sotto - analisi per la stratificazione pre - test del rischio cardiovascolare stata calcolata con scala morise ( rischio basso , intermedio , e alto )  . risultati popolazione di pazienti nella popolazione di 986 consecutivi pazienti eleggibili per lo studio , 259 ( 26% ) sono stati esclusi al follow - up , radiol med ( 2011 ) 116 : 1531 fig . 
patients with no history of cad and nonobstructive disease : normal coronary arteries ( subgroup 1 ) , nonobstructive cad ( luminal stenosis < 50% ) in lm ( subgroup 2 ) , nonobstructive cad in other vessels ( subgroup 3 ) , nonobstructive cad in lm and other vessels ( subgroup 4 )  . 
patients with history of cad and nonobstructive disease : normal coronary arteries ( subgroup 1 ) , nonobstructive cad in other vessels ( subgroup 2 ) , nonobstructive cad in lm and other vessels ( subgroup 3 )  . 
nei pazienti senza storia di malattia delle coronarie ( cad ) e con cad non ostruttiva : coronarie normali ( sotto - gruppo i ) , cad non - ostruttiva ( stenosi luminare < 50% ) nel tronco comune ( lm ) ( sotto - gruppo ii ) , cad non - ostruttiva negli altri vasi ( sotto - gruppo iii ) e cad non - ostruttiva nel lm e negli altri vasi ( sotto - gruppo iv )  . 
nei pazienti con storia di pregressa cad e cad non ostruttiva : coronarie normali ( sotto - gruppo i ) , cad non - ostruttiva negli altri vasi ( sotto - gruppo ii ) e cad non - ostruttiva nel lm e negli altri vasi ( sotto - gruppo iii )  . 
mace , eventi coronarici avversi maggiori ; 1vd , malattia mono - vasale ; mvd , malattia multi - vasale . the detailed baseline characteristics of the population are given in fig . 
la maggioranza dei pazienti ( 514 pazienti , 70 , 1% ) stata inviata per sospetta cad , mentre 213 pazienti ( 29 , 9% ) hanno avuto un pregresso infarto miocardico e / o un pregresso intervento di rivascolarizzazione coronarica mediante bypass aortocoronarico o angioplastica coronarica percutanea . 
in prima istanza , i pazienti sono stati classificati sulla base della storia di pregressa cad ( assente / presente ) e poi ( non sulla base della ostruttiva / ostruttiva )  . 
i pazienti senza storia di pregressa cad e malattia non ostruttiva sono stati sotto - classificati come segue ( 237 ) : coronarie normali ( sotto - gruppo i ) , cad non - ostruttiva ( stenosi luminare < 50% ) nel lm ( sotto - gruppo ii ) , cad non - ostruttiva negli altri vasi ( sotto - gruppo iii ) e cad non - ostruttiva nel lm e negli altri vasi ( sotto - gruppo iv )  . 
i pazienti senza storia di severit della malattia radiol med ( 2011 ) 116 : 1531 table 1 baseline characteristics of patients with no history of cad and nonobstructive cad subgroup 1 ( n = 204 ) subgroup 2 ( n = 10 ) subgroup 3 ( n = 142 ) subgroup 4 ( n = 55 ) data are presented as mean ( standard deviation ) or number ( percentage )  . 
subgroups : normal coronary arteries ( subgroup 1 ) , nonobstructive cad ( luminal stenosis < 50% ) in lm ( subgroup 2 ) , nonobstructive cad in other vessels ( subgroup 3 ) , nonobstructive cad in lm and other vessels ( subgroup 4 )  . 
 cad , coronary artery disease ; sd , standard deviation ; lm , left main ; bmi , body mass index ; bpm , beats per minute tabella 1 caratteristiche di base dei pazienti senza storia di pregressa malattia delle coronarie ( cad ) e con cad non ostruttiva sotto - gruppo i ( n = 204 ) sotto - gruppo ii ( n = 10 ) sotto - gruppo iii ( n = 142 ) sotto - gruppo iv ( n = 55 ) clinical characteristics age [ years ; mean ( sd ) ] male gender ( % ) bmi [ kg / m2 ; mean ( sd ) ] mean heart rate [ bpm ; mean ( sd ) ] ( sd ) ] follow - up [ months ; mean ( sd ) ] risk factors no . 
ds , deviazione standard ; lm , tronco comune ; bmi , indice di massa corporea ; bpm , battiti per minuto follow - up results the mean follow - up was 204 ( range 527 ) months . 
during the follow - up period , 117 mace ( five cardiac deaths , 11 ami , five unstable angina , 86 pci , ten cabg ) occurred pregressa cad e malattia ostruttiva ( 103 ) sono stati considerati come una unica coorte . 
i pazienti con storia di pregressa cad e malattia non ostruttiva sono stati classificati come segue ( 36 ) : coronarie normali ( sotto - gruppo i ) , cad non - ostruttiva negli altri vasi ( sotto - gruppo ii ) e radiol med ( 2011 ) 116 : 1531 table 2 baseline characteristics of patients with no history of coronary artery disease ( cad ) and obstructive cad data are presented as mean ( sd ) or number ( percentage ) sd , standard deviation ; bmi , body mass index ; bpm , beats per minute tabella 2 caratteristiche di base dei pazienti senza storia di pregressa malattia delle coronarie ( cad ) e con cad ostruttiva . 
nine events occurred in patients with no history of cad and nonobstructive disease ( two cardiac deaths in subgroup 3 and seven pci in subgroups 3 and 4 )  . 
 radiol med ( 2011 ) 116 : 1531 table 3 baseline characteristics of patients with history of coronary artery disease ( cad ) and nonobstructive cad subgroup 1 ( n = 10 ) subgroup 2 ( n = 33 ) subgroup 3 ( n = 11 ) data are presented as mean ( sd ) or number ( percentage )  . 
subgroups : normal coronary arteries ( subgroup 1 ) , nonobstructive cad in other vessels ( subgroup 2 ) , nonobstructive cad in lm and other vessels ( subgroup 3 )  . data are presented as mean ( standard deviation ) or number ( percentage )  . 
 sd , standard deviation ; lm , left main ; bmi , body mass index ; bpm , beats per minute tabella 3 caratteristiche di base dei pazienti con storia di pregressa malattia delle coronarie ( cad ) e cad non ostruttiva sotto - gruppo i ( n = 10 ) sotto - gruppo ii ( n = 33 ) sotto - gruppo iii ( n = 11 ) clinical characteristics age [ years ; mean ( sd ) ] male gender ( % ) bmi [ kg / m2 ; mean ( sd ) ] mean heart rate [ bpm ; mean ( sd ) ] follow - up [ months ; mean ( sd ) ] risk factors no . 
i dati sono riportati come media ( deviazione standard ) o numero ( percentuale )  . ds , deviazione standard ; bmi , indice di massa corporea ; bpm , battiti per minuto radiol med ( 2011 ) 116 : 1531 table 4 baseline characteristics of patients with history of coronary artery disease ( cad ) and obstructive cad patients ( n = 159 ) sd , standard deviation ; bmi , body mass index ; bpm , beats per minute tabella 4 caratteristiche di base dei pazienti con storia di pregressa malattia delle coronarie ( cad ) e cad ostruttiva pazienti ( n = 159 ) clinical characteristics age [ years ; mean ( sd ) ] male gender ( % ) bmi [ kg / m2 ; mean ( sd ) ] mean heart rate [ bpm ; mean ( sd ) ] follow - up [ months ; mean ( sd ) ] risk factors no . 
in patients with a history of cad and obstructive disease , 52 events occurred ( four unstable angina ; four ami ; two cardiac deaths ; 38 pci ; four cabg )  . risultati dellangiografia a tomografia computerizzata delle coronarie la valutazione del carico aterosclerotico stata valutata in un numero totale di 10178 segmenti coronarici . 
tra questi , 158 segmenti ( 1 , 5% ) sono stati esclusi per la presenza di artefatti da movimento cardiaco o di cal cio intra - coronarico o per ridotto lume del vaso . 
durante radiol med ( 2011 ) 116 : 1531 table 5 major adverse cardiac events ( mace ) recorded during the follow - up no history of cad nonobstructive obstructive obstructive history of cad nonobstructive hard events unstable angina death subtotal revascularisations cabg subtotal total eventi maggiori angina instabile morte sub - totale ri - vascolarizzazioni cabg sub - totale totale patients with no history of cad and nonobstructive disease : normal coronary arteries ( subgroup 1 ) , nonobstructive cad ( luminal stenosis < 50% ) in lm ( subgroup 2 ) , nonobstructive cad in other vessels ( subgroup 3 ) , nonobstructive cad in lm and other vessels ( subgroup 4 ) patients with history of cad and nonobstructive disease : normal coronary arteries ( subgroup 1 ) , nonobstructive cad in other vessels ( subgroup 2 ) , nonobstructive cad in lm and other vessels ( subgroup 3 ) cad , coronary artery disease ; ami , acute myocardial infarction ; pci , percutaneous coronary revascularisation ; cabg , coronary artery bypass graft tabella 5 eventi . 
la tabella mostra tutti gli eventi avversi cardiovascolari maggiori ( mace ) raccolti durante il follow - up senza storia di cad non ostruttiva ostruttiva ostruttiva storia di cad non ostruttiva nei pazienti senza storia di pregressa malattia delle coronarie ( cad ) e con cad non ostruttiva : coronarie normali ( sotto - gruppo i ) , cad non - ostruttiva ( stenosi luminare < 50% ) nel tronco comune ( lm ) ( sotto - gruppo ii ) , cad non - ostruttiva negli altri vasi ( sotto - gruppo iii ) e cad non - ostruttiva cad nel lm e negli altri vasi ( sotto - gruppo iv )  . 
among patients with no history of cad and obstructive disease , the prognosis was worse for patients with multivessel disease compared with la ctca la frequenza cardiaca media stata di 6210 bp la ctca ha mostrato assenza di aterosclerosi coronarica in 214 ( 29 , 5% ) pazienti , malattia coronarica non ostruttiva in 251 ( 34 , 5% ) e malattia ostruttiva in uno o pi vasi in 262 ( 36 , 0% )  . 
inoltre , la ctca ha rivelato la presenza di malattia mono - vasale in 116 ( 16 , 0% ) pazienti , e malattia multi - vasale in 146 ( 20 , 1% ) pazienti . 
nei pazienti senza storia di pregressa cad o malattia non ostruttiva sono stati osservati 9 eventi ( 2 morti cardiache nel sotto - gruppo iii e 7 pci nel sotto - gruppo iii e iv )  . 
nei pazienti senza storia di pregressa cad e malattia ostruttiva sono stati osservati 51 eventi ( 1 angina instabile , 5 ami , 1 morte cardiaca , 39 pci , 5 cabg )  . 
nei pazienti con pregressa cad e malattia non ostruttiva sono stati osservati 5 venti ( 2 ami nel sottogruppo ii , 3 pci nel sottogruppo ii e iii )  . 
mentre , nei pazienti con pregressa cad e malattia ostruttiva sono stati osservati 52 eventi ( 4 angine instabili , 4 ami , 2 morti cardiache , 38 pci , 4 cabg )  . 
normal coronary arteries ( subgroup 1 ) , nonobstructive cad ( luminal stenosis < 50% ) in lm ( subgroup 2 ) , nonobstructive cad in other vessels ( subgroup 3 ) , nonobstructive cad in lm and other vessels ( subgroup 4 )  . 
coronarie normali ( sotto - gruppo i ) , cad non - ostruttiva ( stenosi luminare < 50% ) nel tronco comune ( lm ) ( sotto - gruppo ii ) , cad non - ostruttiva negli altri vasi ( sotto - gruppo iii ) e cad non - ostruttiva nel lm e negli altri vasi ( sotto - gruppo iv )  . 
 indipendenti per i mace ( cad ostruttiva hr : 9 , 87 , 95% intervallo di confidenza [ ci ] 3 , 2929 , 57 , p < 0 , 001 ; diabete hr : 3 , 45 95%ci 1 , 438 , 46 , p = 0 , 006 )  . discussione il seguente studio ha dimostrato la capacit della ctca nella stratificazione di eventi di rischio cardiovascolare gi dopo la seconda fase del follow - up . 
bench sia semplice estrapolare dai dati il valore predittivo di et , malattia ostruttiva , storia di pregressa cad , malattia ostruttiva del lm / lad per la definizione della prognosi , il ruolo della malattia del lm in questo senso non fig . 
normal coronary arteries ( subgroup 1 ) , nonobstructive cad in other vessels ( subgroup 2 ) , nonobstructive cad in lm and other vessels ( subgroup 3 )  . 
coronarie normali ( sotto - gruppo i ) , cad non - ostruttiva negli altri vasi ( sotto - gruppo ii ) e cad non - ostruttiva nel lm e negli altri vasi ( sotto - gruppo iii )  . 
the capability to stratify nonobstructive disease may render the identification of lm disease ( both obstructive and nonobstructive ) a more difficult task to perforwhereas it is very easy to extract the role of age from this data , obstructive disease , history of cad , lm / lad obstructive disease and diabetes in determining prognosis , the role of lm disease remains uncertain fact , multivariate analysis showed that the only independent predictors of mace were the presence of obstructive coronary disease and diabetes . 
in particular , patients with significant lm stenosis , three - vessel disease or two - vessel disease with an lad artery stenosis > 90% are at higher risk of events [ 1214 ]  . 
in particolare , i pazienti con stenosi significativa del tronco comune , con malattia trio bi - vasale e coronaria discendente anteriore sinistra con stenosi > 90% sono a pi elevato rischio di eventi [ 1214 ]  . 
in particolare , i nostri dati convalidano il ruolo della ctca come metodica non invasiva per la valutazione dellaterosclerosi coronarica e dimostrano il suo elevato valore prognostico indipendente nella valutazione del carico aterosclerotico . il diabete mellito associato ad un elevato rischio di morbilit e mortalit cardiovascolare ed universalmente riconosciuto come un fattore equivalente alla cad . 
nonostante i pazienti con pregresso infarto miocardico siano considerati ad elevato rischio di ricaduta in eventi cardiaci , probabile che il carico aterosclerotico , radiol med ( 2011 ) 116 : 1531 ings . 
specifically , our study confirms that ctca permits the noninvasive evaluation of coronary atherosclerosis and shows that the atherosclerotic burden detected on ctca is a significant and independent prognostic factor . diabetes mellitus is associated with an elevated risk of cardiovascular morbidity and mortality and is widely recognised as a cad equivalent . 
patients with previous mi are considered at high risk for the recurrence of cardiac events ; however , it is likely that atherosclerotic burden , which is usually high in these patients , may be the most important prognostic factor . 
at 1 year , patients with cad had a 34% event rate , whereas patients with normal coronary arteries had a cardiac event rate of 0% [ 22 ]  . 
 it has been suggested that ctca may be used to rule out the presence of significant coronary disease in patients with suspected cad and intermediate pretest risk [ 47 ]  . 
in fact , a number of studies have demonstrated the very high negative predictive value of ctca ( values ranging from 92% to 99% ) for obstructive cad compared with coronary angiography [ 47 ]  . 
in our study , patients without coronary atherosclerosis had a favourable prognosis , with a 0% cardiac event rate during follow - up , thus confirming the high negative predictive value of ctca . study limitation in our study , the presence of lm or proximal lad disease was not an independent predictor at multivariate analysis . this difference may be explained by the limited number of patients with lm / lad disease and by the different stenosis cutoff used by angiographic scores , which is solitamente elevato in tali pazienti , possa essere il fattore prognostico pi importante . 
in questo studio , la presenza e lestensione di cad significativa , classificati mediante la scala modificata di duke per le coronarie , sono stati considerati predittori di tutte le cause di mortalit [ 19 ]  . 
 [ 23 ] hanno valutato 517 pazienti con sospetta cad sottoposti a mpi e ctca , ed hanno riportato una frequenza di eventi annuali di 4 , 8% nei pazienti con cad significativa alla ctca e 1 , 8% nei pazienti con assenza o non significativa cad [ 23 ]  . 
ad un anno di distanza , i pazienti con cad hanno avuto una frequenza di eventi del 34% , mentre i pazienti con coronarie normali dello 0% [ 22 ]  . 
 la ctca stata proposta come modalit dindagine per escludere la presenza di malattia coronarica significativa nei pazienti con sospetta cad e rischio pre - test intermedio [ 47 ]  . 
infatti , numerosi studi hanno dimostrato che la ctca ha un valore predittivo negativo pi elevato ( range 92%99% ) nella cad ostruttiva rispetto allangiografia coronarica convenzionale [ 47 ]  . 
 gli studi prognostici sono importanti per determinare in quali pazienti la ctca possa escludere con certezza la presenza di cad ostruttiva ed evitare cos un sicuro intervento di angiografia coronarica convenzionale . 
in questo studio , i pazienti senza aterosclerosi coronarica hanno una prognosi favorevole , con una frequenza di eventi cardiaci al follow - up dello 0% , confermando lelevato valore predittivo negative della ctca . 
questa differenza potrebbe esser dovuta al limitato numero di pazienti con malattia del lm / lad e dal differente cut - off utilizzato in angiografia per la valutazione della stenosi , solitamente superiore al cut - off del 50% utilizzato alla ctca . 
ci legato alle caratteristiche di base della popolazione , comprendente una coorte di pazienti ambulatoriali con rischio cardiovascolare principalmente intermedio , e alla durata relativamente breve del follow - up . 
 lelevata esposizione alle radiazioni ionizzanti radiol med ( 2011 ) 116 : 1531 usually higher than the 50% ctca cutoff . the main limitation of our study is that the number of clinical events at follow - up was relatively low . 
recently , dose modulation algorithms that reduce the tube current by 80% during the systolic phase and prospective ecg - gating protocols have been developed that allow a significant reduction of radiation exposure down to 34 msv [ 25 , 26 ] , with preserved diagnostic accuracy [ 27 ]  . 
more recently , with the introduction of newer hardware and software , a potential for ctca with < 1 msv has been shown [ 2830 ]  . erogata durante lesecuzione della ctca eseguita mediante acquisizione gating ecg retrospettivo una questione da risolvere . 
recentemente , sono stati sviluppati degli algoritmi di modulazione della dose in grado di ridurre all80% lerogazione raggi durante la fase sistolica e protocolli gating ecg prospettici che permettono una significativa riduzione di esposizione al di sotto dei 34 msv [ 25 , 26 ] con conservazione dellaccuratezza diagnostica [ 27 ]  . 
pi recentemente , con lintroduzione dei pi innovativi hardware e software ha permesso di ottenere con la ctca una potenziale riduzione della dose < 1 msv [ 2830 ]  . conclusioni conclusions our study shows that ctca is able to reliably identify coronary atherosclerotic burden and to stratify cardiovascular risk at follow - up . 
obstructive and nonobstructive lm disease will probably require larger populations and longer follow - up studies to show their prognostic impact questo studio dimostra labilita della ctca nellidentificazione del carico aterosclerotico coronarico e nella stratificazione del rischio cardiovascolare al follow - up . 
la valutazione della malattia ostruttiva e non ostruttiva del lm necessita di una pi vasta popolazione di pazienti e di una maggior durata del follow - up per dimostrare il loro valore prognostico . 
a retrospective analysis was undertaken of 45 patients ( 26 male , 19 female ; age range 1468 years , mean age 39 years ) with skull - base lesions . diffusion - weighted mr images were acquired with a bfactor of 500 and 1 , 000 s / mm2 using single - shot echoplanar imaging . 
the mean adc value of malignant tumours was ( 1.0020.21 ) 10 - 3 mm2 / s and that of benign tumours was ( 1.630.29 ) 10 - 3 mm2 / s . 
we conclude that diffusion - weighted mr imaging is a promising , noninvasive approach that can be used to characterise skull - base lesions in that it can help differentiate malignant tumours from benign lesions and evaluate the pathological grading of malignant tumours . 
la rm in diffusione rappresenta un approccio promettente e non invasivo che pu essere utilizzato per caratterizzare le lesioni della base cranica e pu essere di aiuto per differenziare i tumori maligni dai benigni e valutare il grading delle lesioni tumorali maligne . keywords diffusion mr imaging skull base tumour parole chiave diffusione risonanza magnetica base cranica tumori 126 introduction tumours of the skull base pose a difficult diagnostic challenge , as the skull base may be involved by a spectrum of intrinsic lesions , systemic diseases and lesions arising in the extracranial head and neck or in the intracranial compartment . 
differentiation of malignant skull - base tumours from benign lesions and definite pathological diagnosis are the cornerstones of proper management of the patient and in prognosis prediction [ 15 ]  . 
besides , bone marrow of the skull base shows different signal intensity on different mr pulse sequences that may be mistaken as a tumour [ 7 , 8 ]  . 
ct - guided biopsy is commonly used but it is an invasive procedure that requires a skilled operator and may give false results with hazards of nerve injury [ 9 ]  . diffusion - weighted echoplanar mr imaging is a technique for evaluating the rate of microscopic water diffusion in tissues . 
eight patients were excluded due to uncertain pathology in five patients and poor image quality due to motion artefacts in three . thus , 45 patients ( 26 male , 19 female ; age range1468 years , mean age 39 years ) were finally included . 
the study was approved by the review board , and informed consent was waived . mr imaging was performed with a 1.5 - tesla mr unit ( symphony , siemens medical systems , erlangen , germany ) using a head and neck circular polarisation surface coil . 
all patients underwent t1 - weighted imaging ( tr / te , 800 / 15 radiol med ( 2011 ) 116 : 125132 ms ) and t2 - weighted fast spin echo ( fse ) imaging ( tr / te 4 , 500 / 80 ms ) with a section thickness of 5 mm , an interslice gap of 12 mm , a field of view ( fov ) of 2025 cm and an acquisition matrix of 256256 . diffusion - weighted mr images were obtained using a multislice single - shot spin - echo echoplanar sequence . imaging parameters were tr / te 10 , 000 / 108 ms ; fov 2025 cm ; acquisition matrix 256128 ; section thickness 5 mm with a 1to 2 - mm interslice gap . 
diffusion - weighted mr images were acquired with a diffusion - weighting b - factor of 500 and 1 , 000 s / mm2 , and adc maps were generated . data acquisition time was 1 mfinally , contrast - enhanced t1 - weighted images ( tr / te 800 / 15 ms ) were obtained after an intravenous bolus injection of 0.1 mmol / kg of body weight of gadopentetate dimeglumine ( magnevist , bayer schering pharma , berlin , germany )  . 
 a quantitative analysis of the adc map was made by a radiologist with 20 years of experience in head - and - neck imaging ( aa ) who was blinded to the pathology and clinical results . 
a region of interest ( roi ) was drawn using an electronic cursor around the margin of the solid portion of the mass , taking care to avoid the cystic parts as far as possible , as these could give falsely elevated adc values . the final diagnosis was made by histopathological examination after surgery ( n = 19 ) or endonasal endoscopy - guided biopsy ( n = 20 )  . 
diagnoses of angiofibroma and glomus tumours ( n = 6 ) were based on the typical mr appearance and angiography in addition to a retrospective review of the pathology results . 
to compare between two groups , students t test was applied . receiver operating characteristic ( roc ) curves were generated to determine the cutoff value , with high accuracy and sensitivity . 
the p value was considered significant if 0.05 at 95% confidence interval ( ci )  . results malignant tumours ( n = 32 ) were squamous - cell carcinoma ( n = 7 ) , chordoma ( n = 7 ) , metastasis ( n = 6 ) , rhabdomyosarcoma ( n = 4 ) , plasmacytoma ( n = 3 ) , mucoepidermoid carcinoma ( n = 2 ) , osteosarcoma ( n = 2 ) and adenoid cystic carciradiol med ( 2011 ) 116 : 125132 fig . 
a axial contrast t1 - weighted image of the skull base shows an enhancing lesion involving the left petrous apex that extends to abut the left cerebellar hemisphere and associated retained secretions in the left mastoid air cells . 
b apparent diffusion coefficient ( adc ) map shows low signal intensity of the mass ( black arrows ) with low adc value ( 0.8710 - 3 mm2 / s ) with high signal intensity and high adc value of the retained secretions in the left mastoid ( white arrow )  . 
a limmagine assiale t1 - dipendente dopo mezzo di contrasto della base cranica evidenzia una lesione con enhancement che coinvolge lapice della rocca petrosa di sinistra e si estende verso lemisfero cerebellare di sinistra , con associate secrezioni ritenute nelle celle mastoidee di sinistra . 
b la mappa del coefficiente di diffusione apparente ( adc ) evidenzia una bassa intensit del segnale ( frecce nere ) con basso valore di adc ( 0.8710 - 3 mm2 / s ) con elevata intensit del segnale e elevato adc delle secrezioni ritenute nella mastoide di sinistra ( freccia bianca )  . 
b la mappa del coefficiente di diffusione apparente ( adc ) evidenzia una bassa intensit del segnale con basso valore di adc ( 0 , 9710 - 3 mm2 / s )  . noma ( n = 1 )  . 
the lowest adc value of malignant tumours was detected in a patient with osteosarcoma ( 0.65 ) 10 - 3mm2 / s . the highest value was seen in a patient with adenoid cystic carcinoma ( 1.64 ) 10 - 3mm2 / s , which was misdiagnosed as a benign tumour . 
the bone marrow of the skull base displays variable patterns of signal intensity depending on the proportion of fat cells and cellular marrow that may be mistaken as a pseudolesion . 
in 2006 [ 17 ] found a statistically significant difference ( p = 0.05 ) in adc values between benign and malignant lesions involving the paranasal sinuses and skull base . 
 [ 18 ] added that the mean adc value of nasal and paranasal sinus malignant lesions ( 1.100.2510 - 3mm2 / s ) is significantly different ( p = 0.001 ) from that of benign lesions ( 1.780.4110 - 3mm2 / s )  . 
moreover , diffusion - weighted mr imaging has been used in diagnosing abscesses of the skull base [ 21 , 22 ] as well as detecting bone marrow infiltration of the lumbar spine . 
tumour infiltration appeared as areas of low signal intensity on the adc map , with a low adc value [ 23 , 24 ]  . in this study , the mean adc value of malignant skullbase tumours was significantly lower ( p = 0.001 ) than that of benign tumours . 
this is explained by the difference in histopathological features of benign and malignant tumours . malignant tumours show structural changes , such as enlarged nuclei , hyperchromatism and angulation of nuclear contour . 
these histological features accompany the reduction of extracellular matrix and the diffusion space of water protons , which lead to an increase in the impediment to the motion of water molecules and a decrease in adc values [ 1017 ]  . radiol med ( 2011 ) 116 : 125132 fig . 
a mean adc tumours values of malignant ( 1.0020.2110 - 3 mm2 / s ) are significantly lower ( p = 0.001 ) than those of benign lesions ( 1.630.2910 - 3 mm2 / s )  . 
b mean adc values ( 1.080.2110 - 3 mm2 / s ) are significantly different ( p = 0.01 ) than those of sarcoma ( 0.840.1310 - 3 mm2 / s )  . 
 [ 26 ] added that squamous - cell carcinoma has a higher adc value than lymphoma because carcinoma may contain small foci of necrosis on histopathological examination , which is not identifiable on mr images . 
in our study , there was a significant difference in the adc value of carcinoma and sarcoma , a finding that may be attributed to the higher cellularity of sarcoma compared with carcinoma [ 1013 ]  . 
 in our study , highly vascular benign tumours such as glomus tumours and angiofibromas showed higher adc values than did the other benign solid tumours owing to excess extracellular spaces with free diffusion within the vascular lesions [ 28 ]  . 
chondromyxoid fibroma exhibited a low adc value that was mistaken for a malignant tumour . this is attributed to the excess fibrous tissue within the tumour , with subsequent restriction of diffusion [ 29 ]  . 
the high adc value of adenoid cystic carcinoma is attributed to its high mucous content and cystic components [ 30 ]  . 130 radiol med ( 2011 ) 116 : 125132 fig . 
a cutoff apparent diffusion coefficient ( adc ) value used for differentiating malignant tumours from benign lesions is 1.310 - 3mm2 / s with area under curve ( auc ) of 0.923. 
a il valore di cutoff utilizzato per differenziare i tumori maligni dai benigni di 1.3x10 - 3mm2 / s con area sotto la curva ( auc ) di 0 , 923 . 
the main trade - off of the echoplanar pulse sequence is that it is very sensitive to radiol med ( 2011 ) 116 : 125132 magnetic susceptibility effects , resulting in geometric distortion artefacts that tend to be more severe with increasing b - values . 
recently , 3 - tesla diffusionweighted mr imaging has been used to evaluate head - andneck lesions , including those in the skull base [ 31 , 32 ]  . 
second , the smallest detected lesion was 1 cm , and further studies are recommended for evaluating smaller skull - base lesions . third , there were few cases for each type of histopathological diagnosis . conclusions diffusion - weighted mr imaging is a promising new , noninvasive imaging approach to characterising skull - base masses , as it can help differentiate malignant tumours from benign lesions . 
mr images were assessed for the following features : skin thickening ( > 4 mm ) , skin oedema , architectural distortion , enhancement pattern ( mass - like / non - mass - like ) , time - signal intensity curve ( continuouspersistent type / wash - out type ) , skin enhancement . 
gli aspetti rm analizzati sono stati : ispessimento della cute ( > 4 mm ) , edema cutaneo , distorsione architetturale , pattern di impregnazione ( tipo massa / tipo non - massa ) , curva dellintensit di segnale nel tempo ( tipo continuativo / persistente / tipo wash - out ) , impregnazione della cute . 
comparando i rilievi rm nel carcinoma infiammatorio rispetto al tumore localmente avanzato sono state osservate significative differenze per quanto riguarda le alterazioni cutanee pi frequenti nel carcinoma infiammatorio e il pattern di impregnazione . 
in particolare , ispessimento cutaneo si rilevato in 16 / 30 ( 53% ) ibc vs 8 / 30 ( 27% ) labc ( p = 0 , 06 ) , edema cutaneo era presente in 26 / 30 ( 87% ) ibc vs 8 / 30 ( 27% ) labc radiol med ( 2011 ) 116 : 7183 suggestive of ibc and should prompt a skin biopsy to confirm or rule out the diagnosis . 
le alterazioni della cute ( ispessimento , edema , impregnazione ) sostenute dallinfiltrazione neoplastica dei linfatici del derma sono segni suggestivi di carcinoma infiammatorio e devono guidare al controllo bioptico della cute per confermare o escluderne la diagnosi . parole chiave tumore mammario imaging tumore mammario localmente avanzato carcinoma infiammatorio della mammella rm introduction introduzione inflammatory breast cancer ( ibc ) and locally advanced breast cancer ( labc ) were once considered inoperable at presentation and / or with poor survival rate if treated with locoregional therapies alone . 
despite being often grouped together , in particular in clinical trials , ibc and labc have different epidemiological features and , more importantly , different clinical and biological presentations [ 1 ]  . 
ibc has a higher incidence of locoregional recurrence and metastasis to soft tissue and bone , has worse outcomes and lower survival rates compared with noninflammatory labc [ 24 ] , and its treatment requires a multidisciplinary radiological , chemotherapeutical and surgical approach . 
ibc and labc are treated in the same manner only in the initial stage , where treatment consists of systemic neoadjuvant therapy to improve surgical options and prolong survival [ 5 ]  . 
subsequently , selected patients with labc , but not those with ibc , can undergo conservative treatment provided it is started early on , at the time of treatment planning [ 1 ]  . 
in routine practice , however , the final diagnosis is only established after surgical biopsy , since the clinical presentation of ibc and labc is similar and preoperative pathology may provide inadequate samples for the correct diagnosis , even when large - core needles are used . identifying ibc and differentiating it from labc remains a challenge in breast imaging . 
increasingly sensitive and accurate diagnostic techniques are needed to identify patients il carcinoma infiammatorio ( inflammatory breast cancer , ibc ) della mammella e il carcinoma mammario localmente avanzato ( locally advanced breast cancer , labc ) sono stati in passato considerati come tumori della mammella inoperabili allesordio e / o con ridotta sopravvivenza se trattati con le sole terapie loco - regionali . 
anche se spesso vengono raggruppati assieme , soprattutto nelle sperimentazioni cliniche , ibc e labc hanno diverse presentazioni epidemiologiche e , fatto pi importante , diversi aspetti clinico - biologici [ 1 ]  . 
il carcinoma infiammatorio ha una pi alta incidenza di recidiva loco - regionale e di metastasi a distanza nei tessuti molli e nelle ossa , risultando in una prognosi peggiore e in un minore tasso di sopravvivenza rispetto al carcinoma mammario localmente avanzato noninfiammatorio [ 24 ] ; il suo trattamento richiede un approccio multidisciplinare radiologico , chemioterapico e chirurgico . 
il trattamento del ibc e del labc similare solo nella fase iniziale e si avvale di una terapia sistemica neoadiuvante allo scopo di aumentare le opzioni chirurgiche e di incrementare la sopravvivenza [ 5 ]  . 
successivamente , in pazienti correttamente selezionate con labc , ma non nelle pazienti portatrici di ibc , pu essere applicata una terapia conservativa che per dovrebbe essere presa in considerazione precocemente , al momento della programmazione del trattamento [ 1 ]  . 
nella pratica quotidiana per la diagnosi definitiva viene raggiunta solo dopo biopsia chirurgica , visto che la clinica pu essere similare in caso di ibc e di labc e che la diagnosi patologica pre - operatoria pu fornire campioni tissutali quantitativamente insufficienti per la corretta diagnosi anche con luso di aghi grossi . 
breast magnetic resonance ( mr ) imaging has become a valuable tool in staging invasive breast cancer [ 7 , 8 ] and monitoring response to chemotherapy [ 911 ]  . although several studies have reported the characteristic signs of ibc [ 1220 ] , few have specifically investigated its mr imaging patterns [ 1215 ] , and only one recent paper has addressed the mr appearance of ibc and the differential diagnosis with labc [ 21 ]  . 
the purpose of this study was to verify the existence of mr imaging patterns specific to ibc and to evaluate their accuracy in the differential diagnosis between ibc and labc . materials and methods patients from january 2004 to january 2009 , 52 patients with a diagnosis of ibc were retrospectively considered candidates for this study . 
inclusion criteria were : ( 1 ) histological diagnosis of ibc ( stage t4d ) characterised by the presence of invasive breast cancer with diffuse tumour embolisation of the subdermal lymph vessels according to the american joint committee on cancer ( ajcc ) guidelines [ 22 ] ; ( 2 ) clinical signs and symptoms of inflammation ( swelling and hardening of the breast , pain , peau dorange ( orange skin ) appearance , increased skin temperature , redness of the skin extending to at least one third of the breast ) ; and ( 3 ) mr imaging performed before surgery and neoadjuvant chemotherapy . 
patients who had undergone mr imaging after chemotherapy ( n = 3 ) or surgery ( n = 2 ) and patients who had not undergone mr imaging or for whom mr images were unavailable ( n = 7 ) were excluded from the study . 
the ibc group consisted of 30 patients ( mean age 49 years , range 3181 ) ; of these , 24 were premenopausal and six postmenopausal , and 24 had had pregnancies with a mean number of two children . 
the labc group included 22 premenopausal and eight postmenopausal women ( mean age 54 years , range 4377 ) ; 22 had had pregnancies , with a mean number of two children . 
the control group was made up of patients with labc with a histological diagnosis of stage iiia and iiib invasive breast cancer according to the ajcc staging system [ 22 ] and who had undergone mr imaging before surgery and chemotherapy . 
in the labc group , there were ten patients with positive lymph nodes ( pn2 ) and tumours ranging in size from 1 to 5 cm ( pt1cpt2 ) ; 14 with tumours > 5 cm ( pt3 ) and six with invasion into the skin ( without infiltration into or involvement of the dermal lymphatics ) or chest wall ( pt4a - c )  . linquadramento del carcinoma infiammatorio e la sua differenziazione dal labc rimane una sfida nella diagnostica per immagini della mammella . 
lindagine di risonanza magnetica ( rm ) della mammella diventata un valido strumento nella stadiazione [ 7 , 8 ] e nel monitoraggio della risposta alla chemioterapia [ 911 ] nei tumori invasivi della mammella . 
 in letteratura , alcuni lavori si sono occupati dei rilievi semeiotici del ibc [ 1220 ] , pochi di questi hanno trattato gli aspetti di imaging rm [ 1215 ] e solo un recente lavoro analizza le manifestazioni rm del ibc e la diagnosi differenziale con il labc [ 21 ]  . 
lo scopo di questo studio quindi verificare lesistenza di rilievi rm specifici di carcinoma infiammatorio e dimostrarne laccuratezza statistica nella diagnosi differenziale tra carcinoma infiammatorio e tumore localmente avanzato della mammella . materiali e metodi pazienti tra gennaio 2004 e gennaio 2009 , 52 pazienti con diagnosi di ibc sono state considerate retrospettivamente come candidate per questo studio . 
i criteri di inclusione sono stati : diagnosi istologica di ibc ( stadio t4d ) caratterizzata dalla presenza di carcinoma mammario invasivo con estesa embolizzazione tumorale dei vasi linfatici subdermici secondo le linee guida dellamerican joint committee on cancer ( ajcc ) [ 22 ] ; il rilievo clinico di sintomi / segni di infiammazione ( aumento volumetrico e indurimento della mammella , dolore , pelle a buccia darancia , aumento della temperatura cutanea , rossore cutaneo di almeno un terzo della mammella ) ; esame rm eseguito prima del trattamento chirurgico e della chemioterapia neoadiuvante . 
sono stati esclusi i casi in cui lindagine rm stata espletata dopo la chemioterapia ( 3 casi ) o dopo il trattamento chirurgico ( 2 casi ) e i casi di ibc in cui lesame rm non stato espletato o non era disponibile ( 7 casi )  . 
il gruppo di ibc in studio quindi costituito da 30 pazienti ( et media 49 anni , range 3181 ) ; 24 donne erano in fase fertile e 6 in menopausa , 24 pazienti hanno avuto gravidanze con un numero medio di 2 figli . 
il gruppo di pazienti controllo con labc costituito da 22 donne in fase fertile e 8 in menopausa ( et media 54 anni , range 4377 ) ; 22 pazienti avevano avuto gravidanze con un numero medio di 2 figli . 
familiarit positiva per tumore della mammella era presente in 15 casi . sono stati inclusi nel gruppo controllo , i casi di labc con radiol med ( 2011 ) 116 : 7183 two experienced breast pathologists ( fb and em ) examined the haematoxylineosin stained surgical specimens to determine tumour histological type , grade and immunohistochemical expression . 
histological type was defined according to the world health organization ( who ) classification [ 23 ] ; grade was established on the basis of the nottingham grading system ( elston - ellis modification of the scarffbloomrichardson system ) [ 24 ]  . 
the presence of prognostic markers such as oestrogen receptor ( er ) , progesterone receptor ( pgr ) , ki - 67 , e - cadherin and human epidermal growth factor receptor ( her ) - 2 / neu protein overexpression was assessed and interpreted as either negative or positive according to the standard international recommendations . 
only the 3 + category was considered positive . image analysis all patients underwent mammography and ultrasonography ( us ) with the exception of two women who did not undergo mammography . 
mammographic findings in the ibc group showed skin thickening in 14 ( 46% ) , asymmetrical density with distorted architecture in ten ( 33% ) , focal masses in ten ( 33% ) and calcifications in eight ( 27% )  . 
in two patients , mammography was attempted but not completed owing to breast paamong ibc patients , us showed the presence of a hypoechoic focal lesion in eight ( 27% ) , an irregular hypoechoic area with posterior shadowing in 14 ( 73% ) , skin thickening in 16 ( 53% ) and lymphatic ectasia in six ( 20% )  . mammographic findings in the labc group were skin thickening in four patients ( 13% ) , asymmetrical density with architectural distortion in six ( 20% ) , presence of a focal mass in 12 ( 40% ) and focal mass associated with calcifications in six ( 20% )  . 
mammography failed to identify any abnormality in one case of extremely dense breast . among labc patients , us showed a hypoechoic focal lesion with ill - defined margins in 12 ( 40% ) , an irregular hypoechoic area with posterior shadowing in 20 ( 67% ) and skin thickening in four ( 13% )  . mr imaging was performed with a 1.5 - t magnet ( symphony ; siemens medical system , erlangen , germany )  . images were acquired with a bilateral breast coil and the patient in the prone position . 
in particolare , vi erano 10 casi di tumore con linfonodi positivi ( pn2 ) e dimensioni comprese tra 1 cm e 5 cm ( pt1c - pt2 ) ; 14 casi di tumore con dimensioni superiori a 5 cm ( pt3 ) e 6 casi di tumore infiltrante la cute ( senza infiltrazione o coinvolgimento dei vasi linfatici dermici ) o la parete toracica ( pt4a - c )  . 
 due anatomo - patologici esperti in patologia mammaria ( fb e em ) hanno esaminato i preparati in ematossilinaeosina allestiti da campioni di pezzi operatori al fine di determinare il tipo istologico , il grado tumorale e lespressione immunoistochimica . 
il tipo istologico tumorale stato definito in accordo con la classificazione world health organization ( who ) [ 23 ] ; il grado stato assegnato sulla base del the nottingham grading system ( the elston - ellis modification of the scarff - bloom - richardson system ) [ 24 ]  . 
la presenza di markers prognostici , quali la sovra - espressione di recettori per gli estrogeni ( er ) , per il progesterone ( pgr ) , del ki - 67 , delle - caderina e della proteina her - 2 / neu stata valutata e interpretata come negativa o positiva sulla base delle raccomandazioni standard internazionali . 
solo la categoria 3 + stata considerata positiva . analisi delle immagini tutte le pazienti sono state sottoposte a indagine mammografica ed ecografica , eccetto due dove non stata eseguita la mammografia . 
i rilievi mammografici nel gruppo di ibc hanno evidenziato ispessimento cutaneo in 14 casi ( 46% ) , densit ghiandolare asimmetrica con distorsione dellarchitettura in 10 casi ( 33% ) , massa focale in 10 ( 33% ) , e calcificazioni in 8 casi ( 27% )  . 
lindagine ecografica nelle pazienti con ibc ha identificato la presenza di una lesione focale ipoecogena in 8 casi ( 27% ) , unarea ipoecogena , irregolare con sbarramento posteriore in 14 casi ( 73% ) , ispessimento cutaneo in 16 casi ( 53% ) e ectasia dei vasi linfatici in 6 casi ( 20% )  . 
nel gruppo dei labc sono stati rilevati i seguenti rilievi mammografici : ispessimento cutaneo in 4 casi ( 13% ) , densit ghiandolare asimmetrica con distorsione dellarchitettura in 6 casi ( 20% ) , presenza di massa focale in 12 casi ( 40% ) e massa focale associata a calcificazioni in 6 casi ( 20% )  . 
the dynamic study was performed with a 3d gradient recalled echo ( gre ) sequence in the coronal plane ( tr / te : 12 / 5.65 ms ; angle 25 ; matrix 254320 pixel ; fov 38075 ; thickness 1.24 mm ; acquisition time 88 s ) acquired before the administration of contrast material and repeated six times after intravenous injection of 0.1 mmol of gadoterate meglumine ( dotarem , guerbet co . ) per kilogram of body weight at a rate of 2.5 ml / s followed by 20 ml of saline solution . baseline sequences were assessed for the following morphological features : skin thickening ( skin thickness > 4 mm ) , skin oedema ( increased signal intensity of the skin on the stir sequences ) , architectural distortion ( subversion of the parenchymal and stromal compartments , appearing as coalescence or retraction ) and axillary lymphadenopathy ( lymph nodes > 1.5 cm , with a rounded shape long - axis / short - axis ratio 0.5 and with loss of hilar fat tissue were considered pathological , whereas those > 1.5 cm with an oval shape and preservation of the hilar fat structure were considered benign and reactive )  . dynamic studies were assessed for areas of increased parenchymal enhancement , time - signal intensity curves and skin enhancement . image postprocessing involved subtraction of precontrast acquisitions from postcontrast images and generation of multiplanar reconstructions ( mpr ) and maximum intensity projections ( mip )  . 
time - signal intensity curves were obtained by placing a region of interest ( roi , 59 pixels in width ) over the areas of enhancement seen on the second postcontrast acquisition . 
the time - signal intensity curve was analysed during the first 2 min after contrast administration ( slow , moderate , fast ) and its course followed over the subsequent minutes , thereby identifying three possible curve patterns : steadily progressive enhancement , type 1 ; rapid wash in followed by plateau , type 2 ; rapid wash in and wash out , type 3 [ 25 ]  . statistical analysis mr findings of ibc and labc were compared with the fishers exact test . 
significance was set at a p < 0.05. results distribution of histological type , grade and immunohistoipoecogena irregolare con sbarramento posteriore in 20 casi ( 67% ) e ispessimento cutaneo in 4 casi ( 13% )  . trasversale lo studio rm stato effettuato con magnete da 1 , 5 t ( symphony , siemens medical system , erlagen , germania )  . le immagini sono state acquisite con paziente in posizione prona e con bobina bilaterale dedicata allo studio della mammella . 
lo studio basale stato condotto con una sequenza short tau inversion recovery ( stir ) nel piano ( tempo di ripetizione [ tr ] / tempo di eco [ te ] : 5960 / 70 ms ; matrice 254320 pixel ; field of view [ fov ] 350100 ; spessore 3 , 00 mm ) , una sequenza stir nel piano coronale ( tr / te : 4840 / 68 ms ; matrice 254320 pixel ; fov 350100 ; spessore 3 , 00 mm ) e una sequenza turbo spin echo ( tse ) nel piano sagittale ( tr / te : 3910 / 95 ms ; matrice 254320 pixel ; fov 320100 ; spessore 3 , 80 mm )  . 
lo studio dinamico stato eseguito con sequenze gradient echo ( gre ) 3d nel piano coronale ( tr / te : 12 / 5 , 65 ms ; angolo 25 ; matrice 254320 pixel ; fov 38075 ; spessore 1 , 24 mm ; tempo di acquisizione 88 secondi ) acquisita prima della somministrazione di mezzo di contrasto e ripetuta per sei volte dopo liniezione endovenosa di 0 , 1 mmol di gadoterate meglumina ( dotarem , guerbet co . ) pro kg di peso corporeo alla velocit di 2 , 5 ml al secondo seguita da 20 ml di soluzione fisiologica . 
 i rilievi morfologici analizzati nelle sequenze basali sono stati : ispessimento cutaneo ( spessore cutaneo > 4 mm ) , edema cutaneo ( aumento dellintensit del segnale della cute nelle sequenze stir ) , distorsione architetturale ( sovvertimento del traliccio parenchimo - stromale con aspetto di convergenza o di retrazione ) , linfoadenopatia ascellare ( sono stati considerati come patologici i linfonodi ascellari con dimensione superiore a 1 , 5 cm , morfologia rotondeggiante , rapporto asse corto - asse lungo 0 , 5 , e con perdita della rappresentazione del tessuto adiposo ilare ; sono stati considerati linfonodi benigni e reattivi quelli con dimensioni > 1 , 5 cm , morfologia ovale e conservazione della struttura adiposa ilare )  . 
i reperti valutati durante lo studio dinamico sono stati i seguenti : presenza di aree di aumentata impregnazione del parenchima ghiandolare , curva intensit / tempo del segnale e impregnazione della cute . le immagini sono state elaborate mediante sottrazione delle acquisizioni pre - contrasto da quelle post - contrasto e con ricostruzioni multiplanari ( mpr ) e in proiezione di massima intensit ( mip )  . 
posizionando una regione dinteresse ( roi , estesa 59 pixels ) sulle aree di impregnazione visualizzate nella seconda acquisizione dopo mezzo di contrasto sono state costruite le curve dellandamento del segnale nel tempo . 
all eight cases of ibc with successivi minuti , configurando cos tre possibili curve intensit - tempo : incremento progressivo e graduale , tipo 1 ; rapido wash in e successivo plateau , tipo 2 ; rapido wash in e wash out , tipo 3 [ 25 ]  . analisi statistica il confronto tra i rilievi rm nel ibc e quelli nel labc stato analizzato mediante il test esatto di fischer . 
the mass - like enhancement pattern was inhomogeneous in 4 / 8 cases ( 50% ) , homogeneous in two ( 25% ) and peripheral ring - like in two ( 25% )  . 
distribution of the non - mass - like rale e del profilo immuno - istochimico stata simile nei casi di carcinoma infiammatorio e nei casi di tumore localmente avanzato ed riportata in dettaglio in tabella 1 . 
b sagittal t2 - weighted turbo spin echo image shows architectural distortion in the upper quadrant . c axial t1 - weighted contrast - enhanced gradient recalled echo subtraction image shows a large , non - mass - like enhancement derived from the coalescence of multiple nodules . 
c sequenza gre - t1 dopo somministrazione di mezzo di contrasto ( mdc ) , immagini di sottrazione , piano assiale : estesa e asimmetrica impregnazione del parenchima ghiandolare sinistro , di tipo non - massa a noduli multipli , confluenti con distribuzione irregolarmente triangolare . 
la cute sovrastante , ispessita , dopo somministrazione di mdc mostra impregnazione disomogenea e settoriale . d ricostruzione mip dopo somministrazione di mdc , piano coronale obliquo : meglio evidente lestensione regionale della impregnazione . enhancement pattern was focal in 4 / 22 cases ( 18% ) , segmental in six ( 27% ) and diffuse in 12 ( 55% )  . 
the masslike enhancement pattern was homogeneous in 8 / 22 cases ( 36% ) , inhomogeneous in 12 ( 55% ) and reticular / dendritic in two ( 9% )  . 
mass - like enhancement pattern was homogeneous in 2 / 18 cases ( 11% ) , inhomogeneous in 12 ( 67% ) and peripheral ring - like in four ( 22% )  . 
il coinvolgimento macroscopico dei linfonodi ascellari allindagine rm stato rilevato in 20 / 30 ( 67% ) casi di ibc e in 26 / 30 ( 86% ) casi di labc ( p = 0 , 12 )  . 
il pattern di impregnazione di tipo massa stato disomogeneo in 4 / 8 ( 50% ) casi , omogeneo in 2 / 8 ( 25% ) casi e con radiol med ( 2011 ) 116 : 7183 fig . 
a sagittal t2 - weighted tse image shows two space - occupying lesions the more cranial one with oval shape and well - defined margins and the caudad one with irregular shape and ill - defined margins . 
a sequenza tse - t2 , piano sagittale : due formazioni espansive , solide , quella craniale con morfologia ovalare e profili netti , laltra caudale con morfologia irregolare e contorni irregolari . 
the non - mass - like enhancement pattern was homogeneous in 4 / 12 cases ( 33% ) , inhomogeneous in six ( 50% ) and reticular / dendritic in two ( 17% )  . 
unifocal growth was seen in 8 / 12 ( 67% ) cases of non - mass - like enhancement . comparison of enhancement patterns between the two segno dellanello periferico in 2 / 8 ( 25% ) casi . 
il pattern di impregnazione di tipo non - massa stato omogeneo in 8 / 22 ( 36% ) casi , non omogeneo in tutti i 12 / 22 casi ( 55% ) e reticolare / dendritico in 2 / 22 ( 9% ) casi . 
il pattern diimpregnazione tipo non - massa stato omogeneo in 4 / 12 ( 50% ) casi e ( 33% ) casi , disomogeneo reticolare / dendritico in 2 / 12 ( 17% ) casi . 
 in 6 / 12 confrontando il pattern di impregnazione nei due gruppi , impregnazione diffusa tipo non - massa stata documentata in 22 / 30 ( 73% ) carcinomi infiammatori vs 12 / 30 ( 40% ) tumori localmente avanzati ( p = 0 , 02 )  . 
la curva intensit / tempo del segnale aveva andamento a wash - out in 22 / 30 ( 73% ) casi di ibc e in 20 / 30 ( 67% ) casi di labc ( p = 0 , 77 )  . nei rimanenti casi landamento della curva intensit / tempo stata a plateau . 
le indagini strumentali classiche ( mammografia ed ecografia ) sottostimano spesso lestensione della malattia e non sono idonee per lo studio della cute , che pu essere valutato solo con lesame clinico analizzando i segni destensione alla cute ( infiltrazione , noduli , ulcerazione ) e ai vasi linfatici intraparenchimali ( edema e / o eritema )  . il carcinoma infiammatorio , la forma pi aggressiva di radiol med ( 2011 ) 116 : 7183 discussion diagnostic imaging plays a crucial role in the study of ibc , where it is used to assess locoregional extension of disease , diagnose distant metastases and monitor the response to treatment [ 911 , 26 ]  . 
conventional imaging techniques ( mammography and us ) often underestimate the extent of disease and are inappropriate for studying the skin , which can only be assessed clinically by detecting signs of skin involvement ( infiltration , nodules , ulcerations ) and intraparenchymal lymphatics ( oedema and / or erythema )  . ibc , the most aggressive form of locally advanced cancer , is a distinct entity , which can be defined clinically on the basis of oedema and erythema extending to the entire mammary gland , often without a palpable mass , and with diffusely increased breast density . 
skin involvement is therefore both a typical finding in ibc even though it is absent in the occult forms and a manifestation of noninflammatory labc , which carries a worse prognosis . in this difficult setting , pathological examination is required to distinguish the underlying disease and help plan the most appropriate treatment strategies . 
in some cases , however , histology fails to identify the pathognomonic sign of ibc namely , neoplastic infiltration into dermal lymphatics owing either to incorrect skin and breast - tissue sampling or inadequate amount of material . 
as a consequence , the patient is often wrongly directed to treatment following labc management protocols and the diagnosis of ibc is only established later , after surgical excision and pathological analysis of the entire breast . our study was therefore designed to verify the existence of mr findings specific to ibc that might be used to differentiate this form from labc . 
in addition , mr imaging revealed the presence of skin oedema in a higher tumore localmente avanzato , rappresenta una malattia a s stante che nella forma tipica clinicamente definibile in base alla presenza di edema ed eritema esteso allintera ghiandola mammaria , spesso senza una massa palpabile ma con un diffuso aumento di consistenza della mammella . 
linteressamento cutaneo rappresenta quindi da una parte il reperto clinico tipico del carcinoma infiammatorio , tuttavia assente nelle forme occulte , e dallaltra la manifestazione del carcinoma non - infiammatorio localmente avanzato con prognosi pi sfavorevole . in questo difficile contesto clinico , lesame anatomopatologico pi che mai opportuno per distinguere la malattia sottostante e quindi lottimale planning terapeutico . 
nel caso di neoplasia localmente avanzata , il prelievo istologico , fornendo le informazioni indispensabili per limpostazione del trattamento , pi utile rispetto al prelievo citologico [ 27 , 28 ]  . 
lesame istologico , tuttavia , non consente in tutti i casi lindividuazione del segno patognomonico di carcinoma infiammatorio linfiltrazione neoplastica dei linfatici cutanei vuoi per il non corretto campionamento della cute oltre che della mammella vuoi per lesigua quantit di materiale . 
di conseguenza accade frequentemente che la paziente venga erroneamente avviata al trattamento secondo i protocolli del carcinoma localmente avanzato e che , solo in un secondo tempo , ovvero alla escissione chirurgica , dopo lesame patologico dellintera mammella venga formulata la diagnosi di carcinoma infiammatorio . il presente studio stato pertanto disegnato con lintento di verificare lesistenza di rilievi rm specifici di carcinoma infiammatorio utili nella diagnosi differenziale tra carcinoma infiammatorio e tumore localmente avanzato della mammella . 
il rilievo pi tipico in corso di carcinoma infiammatorio linteressamento della cute con diffuse alterazioni che sono descritte dagli autori in letteratura in circa il 75% dei casi [ 14 , 21 ]  . 
le alterazioni della cute possono essere associate anche a tumori localmente avanzati , ma in percentuale significativamente minore , pari al 27% ( p < 0 , 0001 )  . 
per tale ragione , le presenza di alterazioni cutanee associate a neoplasia mammaria dovrebbe essere approfondita con esame patologico della cute per confermare o escluderne linteressamento neoplastico , definire il tipo di interessamento cutaneo ( infiammatorio o non infiammatorio ) e quindi radiol med ( 2011 ) 116 : 7183 percentage of ibc cases compared with mammography and us ( 87% vs 53% )  . 
for this reason , the presence of skin changes associated with breast cancer should be investigated with pathological examination to confirm or exclude neoplastic involvement , define the type of involvement ( inflammatory or noninflammatory ) and consequently allow for correct diagnosis and treatment . ibc has been reported to show either mass - like or nonmass - like enhancement , with variable frequencies . 
ibc showed a non - mass - like enhancement pattern in most cases ( 73% ) , whereas labc generally had a mass - like enhancement ( 60% )  . 
with regard to distribution , ibc cases show diffuse breast involvement [ 12 , 13 , 15 , 21 ] , whereas labc appears as single or multifocal lesions with mass - like enhancement . 
this finding was significantly different compared with labc that typically does shows no skin enhancement ( p = 0.02 ) , even though markedly lower than reported in the literature . 
focal skin enhancement in labc cases is rare , although it was detected in 28% of cases in renz et al.s [ 21 ] study and in 7% of cases in our series . previous authors have suggested additional evaluation of the pectoralis major muscle and of coopers ligaments . pectoral enhancement and loss of the fat cleavage plane are reliable signs of neoplastic involvement of the pectoralis muscle [ 21 ]  . 
enhancement of thickened connective septa of coopers ligaments is a useful indicator of infiltration when the need arises to distinguish inflammatory carcinoma from nonneoplastic inflammatory processes of the breast [ 14 ]  . in conclusion , ibc is an aggressive clinical and biological entity , which is separate from labc and shows with distinctive mr imaging features . 
il carcinoma infiammatorio ha presentato impregnazione di tipo non massa nelle maggior parte dei casi ( 73% ) ; il tumore localmente avanzato si manifestato generalmente con impregnazione di tipo massa ( 60% )  . 
per quanto riguarda la distribuzione della crescita neoplastica , i casi di ibc coinvolgono la mammella in modo diffuso [ 12 , 13 , 15 , 21 ] mentre i casi di labc si presentano come lesione focale singola o multipla e con estensione tipo massa . 
nella maggioranza dei casi di ibc e labc , la distribuzione macroscopica della lesione proliferativa e il pattern di enhancement rm sono elementi suggestivi per sospettare il corretto tipo di tumore . 
tale risultato appare statisticamente significativo se confrontato con il labc che di solito non mostra impregnazione della cute ( p = 0 , 02 ) , ma molto inferiore a quanto riportato in letteratura ove descritto con una frequenza pi elevate che in quella presente . 
la presenza di impregnazione delle fibre pettorali e la scomparsa del piano di clivaggio adiposo sono risultati segni affidabili per il coinvolgimento neoplastico del muscolo pettorale [ 21 ]  . 
limpregnazione dei setti connettivali ispessiti dei legamenti di cooper pare essere un indice di infiltrazione utile , qualora ve ne fosse bisogno , nel distinguere il carcinoma infiammatorio dai processi infiammatori non - neoplastici della mammella [ 14 ]  . in conclusione , il carcinoma infiammatorio rappresenta unentit clinica e biologica aggressiva distinta dal carcinoma localmente avanzato risultante in peculiari rilievi allimaging rm . 
la presenza di segni di infiammazione contigui alla neoformazione tumorale elemento suggestivo di embolizzazione neoplastica e nei casi dubbi dovrebbe guidare allesteso esame bioptico della cute . lindagine rm riveste un ruolo importante nella diagnosi radiol med ( 2011 ) 116 : 7183 cases . 
moreover , it is essential in treatment planning , as it supplies information about disease extent . differenziale fornendo criteri indicativi di carcinoma infiammatorio oltre che nel bilancio di estensione della malattia , risultando metodica fondamentale per lottimale planning terapeutico . 
these developmental lesions are often isolated , but the association of two or more anomalies is not infrequent . contrast - enhanced multidetector computed tomography ( mdct ) , thanks to multiplanar and 3d reconstructions , allows for detailed studies of these malformations , achieving better accuracy compared with conventional techniques such as chest x - ray , fluoroscopy , ventilation and perfusion scintigraphy and ultrasonography . 
recently , improved ct scanners and optimised ct protocols have made available to children all the benefits of mdct , thanks to a significant reduction in radiation dose and an improved riskbenefit ratio . 
the aim of our paper was to evaluate mdct in children with bronchopulmonary malformations by reporting our experience ( about 2 , 400 studies in 30 months with a 64 - slice mdct scanner ) and comparing it with the available literature . keywords lung congenital malformations multislice computed tomography riassunto le malformazioni congenite broncopolmonari rappresentano un ampio spettro di patologie che interessano il parenchima polmonare , il sistema vascolare , le vie aeree centrali e lesofago . 
la tomografia computerizzata ( tc ) volumetrica multidettetore ( mdct ) con mezzo di contrasto permette di analizzare dettagliatamente le strutture toraciche coinvolte nelle malformazioni , con ricostruzioni multiplanari e 3d , con unaccuratezza superiore ad altre indagini tradizionalmente utilizzate tra cui il radiogramma toracico , gli studi fluoroscopici , lecografia e la scintigrafia ventilatoria perfusionale . 
recentemente levoluzione tecnologica degli scanner tc e la definizione di protocolli pediatrici dedicati ha permesso una significativa riduzione della dose assorbita , pertanto oggi possibile usufruire delle potenzialit della mdct nello studio del torace del bambino con un rapporto rischio - beneficio ragionevolmente vantaggioso . 
il nostro articolo si propone di valutare i differenti aspetti dellimpiego della tc sul bambino analizzando la letteratura e confrontandola con lesperienza personale , unica in italia : circa 2400 tc del torace in 30 mesi in pazienti compresi tra 1 giorno e 16 anni con un apparecchio a 64 strati . 
 134 radiol med ( 2011 ) 116 : 133151 parole chiave polmone malformazioni congenite tomografia computerizzata multidetettore introduction introduzione the innovation potential of multidetector computed tomography ( mdct ) in chest imaging has been emphasised ever since the first papers on this new modality appeared in the literature [ 1 ]  . 
generally , the limited commercial interest , less funding and greater caution involve delays in transferring to paediatric care any knowledge , drugs and equipment that have become available for adult patients [ 2 ]  . 
in fact , in february 2001 , three studies published in the american journal of roentgenology [ 35 ] , which were immediately echoed by the media , not only alarmed parents worldwide , but also raised awareness of a problem that had been neglected , above all in the usa . 
as a consequence , in november 2001 , the us food and drug administration published a notification on radiation risk to paediatric patients from ct , and in particular from mdct [ 6 ]  . 
in fact , mdct was thought to be a source of higher radiation doses compared with single - detector ct in that it enabled the study of extensive thin - slice areas in multiple phases ( often unnecessary in children ) [ 7 ] and allowed for a greater range of settings in the absence of well - defined paediatric protocols [ 8 ]  . in recent years , the use of new - generation scanners [ 9 ] and the definition of paediatric protocols have led to a significant reduction in radiation dose , especially in chest imaging [ 1012 ]  . 
mdct has therefore changed the study of the airways and thoracic vessels in children , thanks to extensive anatomical coverage with increased contrast enhancement , isotropic acquisitions allowing for multiplanar reconstructions ( mpr ) [ 13 ] , and high spatial and temporal resolution with fewer motion artefacts in studying the heart and lung [ 11 , 1416 ]  . 
although magnetic resonance ( mr ) imaging does not use ionising radiation , it is inaccurate in depicting the lung parenchyma and has long acquisition times , requiring sedation / anaesthesia in the majority of children . 
sedation often does not provide sufficient immobility and may be problematic in patients with airway obstruction , such that general anaesthesia with intubation is often needed . intubation in turn may interfere with depiction of tracheal size and shape . 
as regards contrast enhancement , the use of gadolinium - based agents ( necessary for mr imaging ) is considered a risk factor in children due to the possible onset le possibilit innovatrici della tomografia computerizzata ( tc ) multistrato ( mdct ) nello studio del torace vennero messe in risalto gi nei primi articoli che descrissero la nuova tecnologia [ 1 ]  . 
in generale , scarso interesse commerciale , minori finanziamenti e maggior cautela comportano un ritardo nel trasferire al bambino le conoscenze , i farmaci e le attrezzature divenute disponibili nelladulto [ 2 ]  . 
nel febbraio 2001 , infatti , la pubblicazione sullamerican journal of roentgenology di tre studi sui rischi legati alle radiazioni in et pediatrica [ 35 ] immediatamente ripresi dai mass media provoc non solo timori nei genitori di tutto il mondo , ma anche la presa di coscienza dellesistenza di un problema fino ad allora trascurato specie negli usa . 
in seguito a ci , negli stati uniti la food and drug administration ( fda ) pubblic nel novembre 2001 una notifica sui rischi nel bambino dovuti a radiazione derivante da tc con particolare attenzione verso la mdct [ 6 ]  . 
la mdct sarebbe infatti potuta diventare fonte di maggior irradiazione rispetto alla single detector tc per la possibilit di studiare ampie aree a strato sottile anche con fasi multiple ( spesso inutili nel bambino ) [ 7 ] e per la maggior quantit di settaggi possibili in assenza di protocolli pediatrici definiti [ 8 ]  . nel corso degli ultimi anni limpegno dellindustria con generazioni successive di apparecchiature [ 9 ] e la definizione di protocolli pediatrici hanno portato specie nello studio del torace ad una significativa riduzione della irradiazione [ 1012 ]  . 
la mdct ha cos trasformato lo studio delle vie aeree e dei vasi toracici nel bambino grazie alla sua ampia copertura anatomica con pi consistente contrast enhancement , alla acquisizione isotropica con possibilit di ricostruzione multiplanare [ 13 ] e allalta risoluzione sia temporale ( con minori artefatti da movimento nello studio di cuore e polmone ) che spaziale [ 11 , 1416 ]  . 
la risonanza magnetica ( rm ) non utilizza radiazioni ionizzanti , ma non offre accurate informazioni sul parenchima polmonare e presenta lunghi tempi di acquisizione che richiedono la sedazione / anestesia nella maggior parte dei pazienti pediatrici . 
la sedazione spesso non consente una sufficiente immobilit e rappresenta un problema nei pazienti con ostruzione radiol med ( 2011 ) 116 : 133151 of nephrogenic systemic fibrosis ( nsf ) related to immature renal function [ 17 ]  . 
the choice between these two imaging modalities is therefore based on the individual patients needs , even though the limited radiation dose of modern mdct tends to support the use of this modality . whereas the italian literature contains numerous studies on mdct techniques and applications in the adult population , there are no published studies focusing on its use in children . 
our paper evaluates the use of mdct in children by reviewing the literature and comparing it with our personal experience , unique in italy : approximately 2 , 400 chest ct scans performed over 30 months with a 64 - row scanner in patients 1 day to 16 years of age . 
we discuss the technical and radiation protection aspects and the clinical indications of ct in bronchopulmonary malformations , without inclusion of heart disease as such , which , due to its vastness , would require a separate discussion . mdct : technical considerations the ultimate goal of mdct is to acquire diagnostic images with a radiation dose as low as reasonably achievable ( alara principle ) [ 18 ]  . 
the radiologist must be aware of the clinical question to be able to optimise the examination variables to attain the best possible result . patient preparation on the basis of our experience with 64 - slice mdct , sedation is seldom needed . 
it is usually required in patients 6 months to 4 years of age in whom the approach of specialised personnel together with the help of the parents and patient restraint devices do not ensure sufficient immobility . 
we normally use an automatic injector ( empower cta , e - z - e - m , inc . , lake success , ny , usa ) with the following parameters : 1 ml / s for 24 - gauge catheters ( rarely , with the greatest caution ) , 1.52.0 ml / s for 22 - gauge catheters , 23 ml / s for 20 - gauge catheters , with a pressure limit adjusted to a maximum of 150 psi ( 1 , 034 kpa ) [ 19 ]  . we empirically begin the scan at the end of the injection . ct technique selection of technical parameters is dependent on delle vie aeree , pertanto molto spesso richiesta lanestesia generale con intubazione . 
per quanto concerne limpiego del mezzo di contrasto , ricordiamo come limpiego di prodotti a base di gadolinio ( necessario in rm ) sia considerato fattore di rischio nei pazienti pi piccoli per linsorgenza di fibrosi sistemica nefrogenica ( nephrogenic systemic fibrosis , nsf ) , considerata limmaturit della funzione renale [ 17 ]  . 
perci la scelta tra queste due modalit di imaging si basa sui requisiti del singolo paziente , anche se il contenimento della dose radiante oggi ci fa propendere per la mdct . bench vi sia unampia pubblicistica nella letteratura italiana riguardo le tecniche e le applicazioni della mdct nelladulto , non esiste ad oggi una trattazione focalizzata sullutilizzo in et pediatrica . 
il nostro articolo si propone di valutare limpiego della mdct nel bambino analizzando la letteratura e confrontandola con lesperienza personale , unica in italia : circa 2400 tc del torace eseguite in 30 mesi con un apparecchio a 64 strati in pazienti di et compresa tra 1 giorno e 16 anni . 
approfondiremo gli aspetti tecnici , radioprotezionistici e le indicazioni cliniche , avendo per oggetto le malformazioni bronco - polmonari escludendo la patologia cardiaca strictu sensu che , per la sua vastit , richiederebbe una trattazione a parte . 
 mdct : considerazioni tecniche lesecuzione dellesame deve avere come obiettivo finale lacquisizione di immagini diagnostiche alla pi bassa dose di radiazione ragionevolmente raggiungibile ( principio as low as reasonably achievable , alara ) [ 18 ]  . 
il radiologo deve conoscere il quesito clinico per ottimizzare tutte le variabili dellindagine ai fini del miglior risultato . preparazione del paziente in base alla nostra esperienza con mdct a 64 strati , la sedazione necessaria solo in pochi casi . 
di solito riguarda pazienti di et compresa tra 6 mesi e 4 anni per i quali lapproccio dedicato del personale con laiuto dei genitori e i mezzi di contenzione non permettono di ottenere una sufficiente immobilit . 
in pratica , utilizziamo un mezzo di contrasto non ionico a bassa osmolarit ( 300 mgi / ml ) alla dose di 2 ml / kg fino a 125 ml [ 14 ]  . 136 radiol med ( 2011 ) 116 : 133151 indications . 
high - resolution sequential acquisitions ( stepand - shoot method ; conventional hrct ) , characterised by significant dose reduction , are only used in the follow - up of diffuse lung diseases . 
we use two types of nonelectrocardiographically gated acquisitions focusing on either the vascular anatomy ( high temporal resolution ) or the finer details of the lung parenchyma ( high spatial resolution ) with the following equipment and settings : somaton sensation 64 ( siemens medical solutions , erlangen , germany ) : acquisition 640.6 ( z - flying focal spot ) ; rotation time 0.33 s ; pitch 0.90 ; kvp 80 ( < 15 kg ) 100 ; ref . 
an isotropic data set is thus obtained , which , memorised on the picture archiving and communications system ( pacs ) database , allows for high - quality 2d and 3d reconstructions . postprocessing workstations : syngo ct.3d mm ( siemens medical solutions ) , aquarius ws ( terarecon inc . , san mateo , ca , usa ) , carestream healths 3d virtual desktop ( carestream health , rochester , ny , usa )  . in uncooperative patients , the examination is performed during free breathing . 
anatomical coverage routinely extends from the mediastinal inlet to the diaphragin some cases , we extend the acquisition to include a larger volume ; for example , in suspected extralobar pulmonary sequestration , which may be located in the upper abdomen and / or be supplied by the abdominal aorta , the scan is extended to the plane of the renal arteries [ 20 ]  . in our experience , indications for retrospective ecg gating ( which entails at least a fourfold higher dose , with only a portion of the dose being used for image creation ) are limited , as the origin of the coronary arteries can also be clearly identified in most cases with nongated sequences [ 16 ]  . 
in pratica limitiamo le acquisizioni sequenziali ad alta risoluzione ( step and shoot method ; tc ad alta risoluzione [ hrct ] convenzionale ) , caratterizzate da notevole riduzione della dose , al follow - up delle patologie polmonari diffuse . 
utilizziamo 2 tipi di acquisizione non cardiosincronizzate che privilegiano o lanatomia vascolare ( elevata risoluzione temporale ) o il fine dettaglio del parenchima polmonare ( elevata risoluzione spaziale ) ed i seguenti materiali e settaggi : somaton sensation 64 ( siemens medical solutions , erlangen , germania )  . 
mas : 45 ; 85 . incremento : 1 mricostruzione : 1 mfiltro b30f ; b60f . otteniamo cos un dataset isotropico che , memorizzato nel picture archiving and communication system ( pacs ) , permette ricostruzioni 2d e 3d di alta qualit . workstation di post - elaborazione : syngo ct.3d mm ( siemens medical solutions ) , aquarius ws , ( terarecon inc . , san mateo , usa ) , carestream healths 3d virtual desktop ( carestream health , rochester , usa )  . nei pazienti non collaboranti eseguiamo lesame a respiro libero . 
talora lacquisizione deve essere ampliata , come nel dubbio di sequestro polmonare extralobare che pu essere situata nella cavit addominale superiore e / o avere vascolarizzazione che origina dalla aorta addominale : in tal caso la scansione va estesa al piano delle arterie renali [ 20 ]  . 
volume di computed tomography dose index ( ctdivol ) e dose lenght product ( dlp ) : valori medi e deviazioni standard ( ds ) da noi osservati in 3 differenti fasce det chiaramente individuata nella maggioranza dei casi con sequenze non - gated [ 16 ]  . 
la nostra esperienza invece ancora limitata per quanto concerne le indagini eseguite con cardiosincronizzazione prospettica . il controllo dei fattori di esposizione rappresenta un elemento decisivo per il contenimento della dose . 
passando da 140 a 80 kvp , a corrente di tubo costante , la dose si riduce di un fattore di circa 3 , 4 [ 22 ] con un incremento di contrasto e di rumore ( pochi fotoni prodotti )  . 
nel bambino sottoposto a tc con mezzo di contrasto siegel [ 23 ] ha dimostrato che la ridotta energia del fascio riduce la dose senza incidere in modo significativo sul contrasto dellimmagine . daccordo con herzog [ 24 ] , noi preferiamo utilizzare gli 80 kvp al di sotto dei 15 kg , utilizzando 100 kvp per pesi 15 kg . 
 [ 24 ] ed osservati nel bambino con la nostra stessa apparecchiatura . la dose efficace genericamente riportata in letteratura per la tc del torace in pediatria di 3 msv [ 26 ]  . 
 [ 11 ] , sulla base di unesperienza con apparecchio a 16 strati utilizzato per le acquisizioni angiografiche con collimazione 0 , 75 mm , riferiscono dosi efficaci che si incrementano al crescere del peso da 1 a 2 , 5 msv . 
lo stesso autore attribuisce dosi efficaci variabili da 0 , 21 a 0 , 59 msv per la hrct sequenziale e da 0 , 00487 a 0 , 01769 msv per il radiogramma antero - posteriore ( ap ) del torace . ricordiamo che esistono dei coefficienti di conversione ( et e regione specifici ) da dlp a dose efficace [ 27 ]  . recentemente sono stati pubblicati dati che confermerebbero la affidabilit del metodo [ 28 ]  . 
in tal caso , mentre per il cranio i fattori di conversione sarebbero corretti anche nel bambino , per quanto riguarda il corpo 138 radiol med ( 2011 ) 116 : 133151 we recall that there are ageand region - specific coefficients for conversion from dlp to effective dose [ 27 ]  . 
manufacturers often derive dlp values from adult phantoms with a head diameter of 16 cm and a body diameter of 32 cin this case , whereas for the head , the conversion factors would also apply to children , for the body , the dlp should be multiplied by two before applying the conversion coefficient . postprocessing is an essential part of the investigation . as with adult patients , the common reconstruction techniques are used : 2d mpr and 3d multiplanar volume reconstruction ( mpvr ) , maximum intensity projection ( mip ) , minimum intensity projection ( minip ) , shadedsurface display ( ssd ) , volume rendering technique ( vrt ) and virtual bronchoscopy ( vb )  . 
mpvr ( fast and easy ) is particularly useful in that it combines the spatial resolution of mpr with the visualisation of thicker slices ; in studying the pulmonary parenchyma , it minimises interpretation problems arising from small - size anatomical structures appearing blurred due to the noise of low - dose ct . 
other reconstruction techniques ( some very time consuming ) are also used according to the case to be interpreted [ 11 , 29 ]  . clinical applications according to panicek et al . 
 [ 30 ] , all the most common developmental anomalies of the lung , such as congenital lobar emphysema ( cle ) , bronchogenic cysts , congenital cystic adenomatoid malformation ( ccam ) or congenital pulmonary airway malformation ( cpam ) , pulmonary sequestration , hypogenetic lung syndrome and pulmonary arteriovenous malformation represent a continuum of malformations from cle ( anomalous lung , normal vessels ) to pulmonary arteriovenous malformation ( anomalous vessels , normal lung )  . 
the theory of bronchopulmonary vascular malinosculations suggests a temporal coincidence ( without any causal relationship ) of abnormal connections between respiratory mesenchyma and bronchial epithelium or between rudiments of the foregut , respiratory tract and aortopulmonary vascular system [ 31 ]  . in this light , newman [ 32 ] recently introduced the notion of bronchopulmonary and foregut malformations . 
as a result , there may be associated anomalies , such as pulmonary agenesis / hypoplasia , sequestration , atresia and tracheal bronchus , pulmonary artery sling , alveolar capillary sarebbe opportuno moltiplicare il dlp per un fattore due prima di applicare il coefficiente di conversione . 
 il post - processing una parte fondamentale dellindagine . come per ladulto si utilizzano le comuni tecniche di ricostruzione disponibili sulle consolle : 2 - d : multiplanar reformation o reconstruction ( mpr ) , 3 - d : multiprojective volume reconstruction ( mpvr ) , maximum intensity projection ( mip ) , minimum intensity projection ( minip ) , shaded - surface display ( ssd ) , volume rendering technique ( vrt ) e virtual bronchoscopy ( vb )  . 
la mpvr ( facile e immediata ) particolarmente utile perch unisce la risoluzione spaziale dellmpr con la visualizzazione anatomica di strati pi spessi ; nello studio del parenchima polmonare limita i problemi interpretativi dovuti alle piccole strutture anatomiche confuse nel rumore da bassa dose . 
 [ 30 ] le pi comuni anomalie di sviluppo del polmone come enfisema lobare congenito ( congenital lobar emphysema , cle ) , cisti broncogena , malformazione adenomatoide cistica congenita ( congenital cystic adenomatoid malformation , ccam o congenital pulmonary airway malformation , cpam ) , sequestro polmonare , sindrome del polmone ipogenetico e malformazione arterovenosa polmonare si inseriscono in un continuum malformativo che ha ad una estremit il cle ( polmone anomalo , vasi normali ) e allaltra la malformazione arterovenosa polmonare ( vasi anomali , polmone normale )  . 
la teoria delle bronchopulmonary vascular malinosculations propone la coincidenza temporale ( senza rapporto causaeffetto ) delle anomalie di connessione tra mesenchima respiratorio e epitelio bronchiale o tra abbozzi dellintestino primitivo , dellapparato respiratorio e del sistema vascolare aorto - polmonare [ 31 ]  . 
di conseguenza possono essere associate tra loro anomalie come agenesia / ipoplasia polmonare , sequestro , atresia e bronco tracheale , sling dellarteria polmonare , displasia alveolo capillare , cisti esofagee / neuroenteriche , fistole tracheo - esofagee / diverticoli / stenosi , ecc . 
si deduce che , a fronte di una sospetta anomalia dei vasi toracici e delle vie aeree , limaging deve fornire una valutazione completa di tutte le componenti anatomiche del torace . evidente come la mdct rappresenti la tecnica di imaging elettiva con un ruolo fondamentale nella acquisizione di radiol med ( 2011 ) 116 : 133151 dysplasia , oesophageal / neuroenteric cysts , tracheoesophageal fistula ( tef ) / diverticula / stenoses , etc . 
mdct clearly represents the imaging technique of choice , as it has a primary role in providing knowledge of the natural history , overlapping , terminology , classification and management of these malformations [ 33 ]  . tracheobronchial anomalies always look at the airway is one of the fundamental maxims of paediatric radiology . 
clinical respiratory manifestations often remain unexplained radiologically because the study has only focused on the pulmonary parenchyma [ 34 ]  . tracheomalacia tracheobronchomalacia is a condition deriving from the softening of the tracheobronchial wall or cartilaginous ring , resulting in pathological expiratory collapse . 
 [ 36 ] suggest that the diagnosis be made with mdct with scans acquired during maximum inspiration and expiration . however , this may prove difficult in uncooperative patients , and in these instances , the authors describe a procedure performed under general anaesthesia after intubation , when forced inspiration and expiration are achieved by varying the ventilatory pressure . tracheal stenosis congenital tracheal stenosis is a rare disorder characterised by the presence of single or multiple , complete or nearcomplete , tracheal cartilage rings , resulting in narrowing of the tracheal lumen . 
types of tracheal stenosis include focal stenosis ( 50% of cases ) , generalised stenosis ( 30% of cases ) and segmental carrotor funnel - shaped stenosis ( 20% of cases ) usually located in the lower third of the trachea . given that resistance to laminar airflow increases linearly in proportion to length of stenosis and fourfold relative to calibre decrease , a tight stenosis produces worse symptoms compared with a long and moderate stenosis . 
il problema per si pone di solito nei non collaboranti e , in questo caso , gli stessi autori descrivono una procedura in anestesia generale a paziente intubato con inspirazione ed espirazione forzate ottenute facendo variare la pressione ventilatoria . stenosi tracheale la stenosi tracheale congenita una rara patologia causata dalla presenza di anelli cartilaginei tracheali completi ( o quasi ) , singoli o multipli , causanti restringimento del lume tracheale . 
le tipologie di stenosi tracheale includono la stenosi focale ( 50% dei casi ) , la stenosi generalizzata ( 30% dei casi ) e la stenosi segmentale a forma di carota o ad imbuto ( 20% dei casi ) solitamente localizzata al terzo inferiore tracheale . 
dato che la resistenza al flusso aereo laminare aumenta linearmente con la lunghezza della stenosi e con la quarta potenza della riduzione di calibro , una stenosi serrata provoca sintomi pi importanti di una stenosi lunga e moderata . 
gli anelli tracheali congeniti completi possono presentarsi isolatamente o la loro presenza pu essere associata a sling polmonare ( arteria polmonare sinistra che origina dalla destra e , passando davanti allesofago , circonda il bronco principale di destra e la trachea distale causando compressione )  . 
i tipici reperti alla mdct sono rappresentati dalla riduzione della circonferenza estesa a tutta la trachea , la fusione degli anelli tracheali cartilaginei posteriormente 140 radiol med ( 2011 ) 116 : 133151 fig . 
tracheal bronchus is more common in children affected by other malformations , such as congenital heart defects , tef , tracheal stenosis and down syndrome [ 37 ]  . in the majority of cases , tracheal bronchus consists of a right upper bronchus with anomalous origin or an apical portion with anterior and posterior branches arising from the right mainstem bronchus or , less frequently , a supernumerary bronchus directed towards the right upper lobe territory ( sometimes with a blind ending )  . 
la presenza di bronco tracheale pi comune in bambini con altre malformazioni , come anomalie cardiache congenite , fistola tracheoesofagea , stenosi tracheale e sindrome di down [ 37 ]  . 
nella maggior parte dei casi , il bronco tracheale costituito da un bronco superiore destro che origina in sede anomala , o dal suo ramo apicale con rami anteriori e posteriori che nascono dal bronco principale destro , o raramente un bronco sopranumerario diretto al lobo superiore destro ( talvolta a fondo cieco )  . 
il bronco tracheale spesso un riscontro incidentale in un paziente asintomatico , anche se le dimensioni ridotte della via aerea e il ristagno di secrezioni possono essere causa di stridore espiratorio destro e / o bronchiectasie , atelettasie e ripetute infezioni . 
limmagine segnalata dalla freccia corrisponde al bronco pieno di muco distale al tratto atresico . of the airway and retained secretions may produce right expiratory stridor and / or bronchiectasis , atelectasis and recurrent infections . 
the introduction of mdct has led to a significant increase in the number of cases detected ; indications for the use of mdct include evaluation of heart malformations or study of recurrent bronchopulmonary disease . bronchial atresia congenital bronchial atresia results from atresia or obstruction of a segmental or subsegmental bronchus with normal development of the distal airway . 
although the majority of patients with bronchial atresia are asymptomatic and the diagnosis is made on chest radiographs performed for other reasons , some authors report a history of recurrent pneumonia . 
this should not be mistaken for a nodule or for lung abnormalities such as lobar emphysema or intralobar sequestration with air trapping [ 39 ]  . sono di solito la valutazione di malformazioni cardiache o lo studio di broncopneumopatie ricorrenti . 
spesso lintrappolamento di aria proveniente dallinterstizio e dai pori di kohn provoca liperinsufflazione del segmento polmonare a valle del bronco ostruito . sebbene la maggior parte dei pazienti con atresia bronchiale siano asintomatici e la diagnosi sia ottenuta da un radiogramma del torace eseguito per altri motivi , qualche autore riferisce una storia di polmoniti ricorrenti . 
tale reperto non deve essere confuso con un nodulo o con anomalie polmonari quali enfisema lobare o sequestro intralobare con air trapping [ 39 ]  . cisti broncogene le cisti broncogene sono lesioni congenite che originano dallintestino primitivo ventrale e possono essere localizzate in sede mediastinica ( 60% ) , al iii medio polmonare ( 30% ) o , 142 bronchogenic cysts bronchogenic cysts are congenital lesions that originate from the embryonic foregut and may be located in the mediastinal space ( 60% ) , in the middle third of the lung ( 30% ) or , less frequently , in the lower neck ( 10% )  . 
two - thirds of patients present with cough , stridor , dyspnoea and pneumonia as a result of tracheal and / or bronchial compression . occasionally the mass effect may produce air trapping and / or atelectasis [ 36 ]  . 
a provisional diagnosis of bronchogenic cyst should be considered whenever a well - circumscribed lesion with fluid density is identified in the middle third of the mediastinum adjacent to the bronchial tree . 
only after infection does the cyst show wall enhancement . pulmonary anomalies pulmonary underdevelopment the clinical spectrum of pulmonary underdevelopment includes agenesis of the bronchus , vascular structures and lung ( pulmonary agenesis ) ; the presence of a blind - ending rudimentary bronchus without lung tissue ( pulmonary aplasia ) ; and bronchial hypoplasia with variable reduction in parenchymal lung volume ( pulmonary hypoplasia ) [ 41 ]  . pulmonary agenesis is a rare congenital malformation . mortality rates are high owing to the associated congenital anomalies , which include heart disease , tracheoesophageal atresia , spinal and renal malformations . 
abnormal development of the pulmonary vasculature is frequently associated and includes alveolar capillary dysplasia , pulmonary artery sling , absence of the pulmonary artery , absence of the pulmonary vein and scimitar syndrome [ 42 ]  . 
due terzi dei pazienti sono affetti da tosse , stridore , dispnea , e polmonite in conseguenza della compressione della trachea e / o dei bronchi da parte della cisti . 
 anomalie del polmone iposviluppo polmonare lo spettro dei quadri di iposviluppo polmonare include lagenesia del bronco , delle strutture vascolari e del polmone ( agenesia polmonare ) , la presenza di un abbozzo bronchiale che termina a fondo cieco senza tessuto polmonare ( aplasia polmonare ) e lipoplasia bronchiale con riduzione di volume del parenchima polmonare di grado variabile ( ipoplasia polmonare ) [ 41 ]  . 
frequente la coesistenza di anomalie di sviluppo della vascolarizzazione polmonare tipo displasia capillare alveolare , sling dellarteria polmonare , assenza dellarteria polmonare , assenza della vena polmonare , sindrome della scimitarra [ 42 ]  . 
vena polmonare anomala ( freccia ) che drena nella vena cava inferiore . vaso sistemico arterioso che rifornisce il polmone destro ( freccia aperta )  . ipoplasia dellarco aortico ( asterisco )  . completely ( agenesis ) or partially ( atresia ) absent : in the latter case , the peripheral circulation is normal . 
unilateral agenesis is often associated with cardiac malformations ; if isolated , it may be asymptomatic or manifest over the years as pulmonary hypertension , haemoptysis and recurrent infection [ 43 ]  . 
chest radiographs show a small , harmonious lung ( disharmonious in the case of lobar agenesis / aplasia ) ; the hilum on the affected side is small . mdct demonstrates the absence of the artery , typically on the side contralateral to the aortic arch usually on the right and helps identify associated heart defects and systemic collateral vessels . 
lagenesia unilaterale si associa spesso a malformazioni cardiache ; se isolata pu essere asintomatica o manifestarsi negli anni con ipertensione polmonare , emottisi e infezioni ricorrenti [ 43 ]  . 
la radiografia del torace mostra il cosiddetto piccolo polmone armonico ( disarmonico se agenesia / aplasia lobare ) ; dallo stesso lato lilo piccolo . la mdct evidenzia lassenza dellarteria , tipicamente dal lato opposto dellarco aortico di solito a destra e permette di identificare le anomalie cardiache associate e i vasi sistemici collaterali . 
 sindrome del polmone ipogenetico la sindrome del polmone ipogenetico , anche conosciuta come sindrome venolobare polmonare congenita o sindrome della scimitarra , una forma di connessione venosa 144 radiol med ( 2011 ) 116 : 133151 fig . 
other less common sites of confluence include the superior vena cava , the right atrium , the azygos vein , the portal vein and the hepatic vethanks to mpr , mdct also allows accurate assessment of the anomalous systemic arterial supply . 
images obtained with lung window settings and 3d reconstructions of the central airways can demonstrate the presence of abnormal parenchymal findings , polmonare anomala verso la vena cava inferiore associata ad altre anomalie come polmone destro e arteria polmonare ipoplasici , destrocardia , anomala vascolarizzazione sistemica arteriosa del polmone destro . 
possono essere presenti anche altre malformazioni come difetti del setto interatriale e interventricolare , dotto arterioso di botallo pervio , tetralogia di fallot , anomalie del diaframma , sequestri polmonari e polmoni a ferro di cavallo . i pazienti affetti da sindrome del polmone ipogenetico presentano una gamma di sintomi variabile in relazione allet di presentazione e al grado di shunt . 
le immagini con finestra polmonare e le ricostruzioni 3d delle vie aeree centrali possono dimostrare la presenza di reperti parenchimali polmonari anomali quali consolidazioni , radiol med ( 2011 ) 116 : 133151 such as consolidation , bronchiectasis , abnormal lung lobation and abnormal bronchial branching . bronchiectasie , lobature polmonari anomale e anomalie della diramazione bronchiale . 
 congenital cystic adenomatoid malformation ( ccam ) malformazione adenomatoide cistica congenita ( ccam ) ccam is characterised by a pulmonary mass deriving from the hamartomatous and adenomatoid proliferation of primary bronchioles communicating with the bronchial tree to the detriment of the alveolar component , and it is often associated with airway cartilage defects . 
there is no consensus concerning its classification and nomenclature . recently , the term congenital pulmonary airway malformation ( cpam ) has been favoured , as not all lesions are cystic and only type 3 is adenomatoid [ 33 ]  . 
the natural history of the condition , characterised by regression and disappearance or by persistence , is not completely explained , and there is disagreement as to the best time to operate on these asymptomatic lesions . 
it has been suggested that low - grade cystic pleuropulmonary blastoma , which presents as a cystic mass , could go undetected , as it is virtually indistinguishable from ccam with currently available diagnostic techniques . 
in the case of pleuropulmonary blastoma , the typical mass effect with lobar expansion , the mediastinal shift and the associated parenchymal opacities produce a pattern that is identical to that of ccam type 4 . ccam may be distinguished from sequestration in that it la ccam una massa polmonare che deriva dalla proliferazione amartomatosa e adenomatoide di bronchioli primari comunicanti con lalbero bronchiale a discapito della componente alveolare , ed spesso associata a difetti cartilaginei delle vie aeree . 
recentemente stato preferito il termine malformazione congenita delle vie aeree polmonari ( cpam ) perch non tutte le lesioni sono cistiche e solo il tipo iii adenomatoide [ 33 ]  . 
 [ 45 ] classificarono queste lesioni in tre tipi : tipo i , macrocistica ( > 2 cm ) ; tipo ii , piccole cisti multiple ; tipo iii , forma solida ( cisti microscopiche )  . 
pi recentemente stata proposta una classificazione ampliata ( da tipo 0 a tipo 4 ) per rappresentare le malformazioni delle vie aree di calibro maggiore sino a quelle di calibro minore [ 46 ]  . 
le ccam sono sempre pi frequentemente identificate in epoca prenatale : le dimensioni maggiori si riscontrano durante il ii trimestre per poi ridursi progressivamente sia in senso assoluto che relativo . 
 stato ipotizzato che il blastoma pleuropolmonare cistico di basso grado che si manifesta come una massa cistica possa non essere identificato in quanto praticamente indistinguibile da una ccam con le tecniche diagnostiche attualmente disponibili . 
in caso di blastoma pleuropolmonare il caratteristico effetto massa con espansione lobare , lo shift mediastinico e le opacit parenchimali associate , realizzano 146 radiol med ( 2011 ) 116 : 133151 fig . 
angio tc : a piano assiale e b piano coronale . massa cistica destra con setti interni che determina spostamento controlaterale del mediastino . has no anomalous systemic arterial supply typical of pulmonary sequestration , although ccam and sequestration may coexist and be present as a mixed lesion [ 50 ]  . 
in patients with bacterial superinfection , airfluid levels and parietal contrast enhancement may also be identified [ 32 , 36 ]  . pulmonary sequestration the term sequestration refers to the presence of a portion of lung parenchyma having no connection with the tracheobronchial tree and a systemic vascular supply [ 32 , 36 ]  . 
 la ccam pu essere distinta dal sequestro sulla base dellassenza di un apporto arterioso sistemico anomalo , tipico del sequestro polmonare , sebbene la ccam e il sequestro possano coesistere e presentarsi come lesione mista [ 50 ]  . 
 sequestro polmonare con il termine sequestro si intende la presenza di una porzione di parenchima polmonare priva di connessione con lalbero tracheo - bronchiale e con un apporto vascolare sistemico [ 32 , 36 ]  . 
sono state definite due forme principali : extralobare , rivestita da pleura viscerale , e intralobare , posizionata tra aree di parenchima normale . spesso coesiste un difetto del diaframma , e circa il 15% dei casi dei sequestri extralobari sono addominali . 
presenza di arteria anomala che origina dalla aorta discendente ( freccia )  . sequestrations typically have normal venous connections . nonetheless , any type of arterial or venous vascularisation is possible . un sequestro intralobare solitamente ha connessioni venose normali . 
 the parenchyma of pulmonary sequestration is usually underdeveloped , and it may be associated with cysts covered by columnar or cubic epithelium , or it may be entirely characterised by structures similar to alveolar ducts . mucus can distend the multiple intercommunicating spaces , making the lesion appear radiologically solid or sonographically hyperechoic unless , as in the case of intralobar sequestration , air penetrates through the pores of kohn . 
an increasing number of authors suggest that intralobar sequestration may also derive from recurrent infections that produce anomalous arterial branches from the aorta ( such as the pulmonary ligament arteries ) [ 51 ]  . sequestration is identified in the prenatal period as a hyperechoic mass , usually in the posterior basal hemithorax . colour doppler ultrasonography is useful for demonstrating the presence of anomalous vessels that can be studied from their orig mdct is crucial for the diagnosis and for preoperative planning . 
il muco pu distendere i multipli spazi intercomunicanti , conferendo un aspetto radiologicamente solido alle lesioni o iperecogeno allecografia , a meno che , in caso di sequestro intralobare , laria vi penetri tramite i pori di kohn . 
un sempre maggiore gruppo di autori ipotizza che il sequestro intralobare possa anche derivare da infezioni ricorrenti che producono rami arteriosi anomali dallaorta ( come le arterie del legamento polmonare ) [ 51 ]  . 
 il sequestro identificato in epoca prenatale come una massa iperecogena , solitamente in sede postero - basale . leco - color doppler utile per dimostrare la presenza di vasi anomali che possono essere valutati sino allorigine . 
the typical presentation consists of a limited number of overdistended alveoli ; by contrast , in the recently identified polyalveolar form , there are more alveoli than under normal conditions [ 52 ]  . the most frequent location is the left upper lobe . 
patients usually have respiratory difficulties in the neonatal period , mostly when there is a marked hyperinflation of the affected lobe and a mass effect on the adjacent parenchyma and on the mediastinusurgical lobectomy is indicated above all in cases of progressive hyperinflation , as this condition is potentially fatal . 
once the neonatal lung fluid is reabsorbed from the lymphatic system and replaced by air , the affected lobe becomes hyperlucent , with a mass effect on the adjacent lobes . mdct shows the presence of a hyperinflated lobe with displaced pulmonary vessels . 
when the lesion reaches large dimensions and has a mass effect on the surrounding structures , a contralateral mediastinal dislocation is observed , together with an increase in intercostal spaces and ipsilateral diaphragmatic descent [ 36 , 41 ]  . 
cle may be mistaken for pneumothorax or for simple or acquired cysts : in cle the bronchovascular markings are seen inside the overdistended lobe . lenfisema lobare congenito ( cle ) ora chiamato iperinsufflazione lobare congenita ( congenital lobar hyperinsufflation , clh ) in quanto non c distruzione delle pareti alveolari [ 32 ] descritto come il risultato di una progressiva sovradistensione di un lobo polmonare , secondaria ad ostruzione intrinseca o estrinseca o a deficit di cartilagine bronchiale . la forma classica ha un numero ridotto di alveoli sovradistesi ; invece , nella forma poli - alveolare recentemente descritta esistono pi alveoli del normale [ 52 ]  . 
occasionalmente possono essere interessati o parte di un lobo o pi di un lobo . i pazienti solitamente presentano difficolt respiratorie nel periodo neonatale , specialmente quando c una marcata iperinsufflazione del lobo coinvolto ed effetto massa sul parenchima adiacente e sul mediastino . 
la lobectomia chirurgica indicata soprattutto nei pazienti con progressiva iperinsufflazione , perch pu essere una condizione mortale . la diagnosi di cle dovrebbe essere considerata nei casi in cui unopacit lobare alla rx torace diventa progressivamente ipertrasparente e iperinsufflata dopo la nascita . 
quando la lesione raggiunge ampie dimensioni e ha effetto massa sulle strutture limitrofe si osserva dislocazione mediastinica controlaterale , incremento degli spazi intercostali e abbassamento diaframmatico omolaterale [ 36 , 41 ]  . 
il cle pu essere confuso con il pneumotorace o con cisti semplici o acquisite : nel cle si vede il disegno polmonare allinterno del lobo sovradisteso . oesophageal anomalies anomalie esofagee we previously mentioned the unitary concept involved in defining bronchopulmonary and foregut malformations [ 32 ]  . 
on this subject , we recently reported on two unknown cases of tracheoesophagel fistula ( in two girls 5 and 9 years of age , respectively ) diagnosed at mdct performed for recurrent airway infections . 
in both girls , a marked gaseous distension of the digestive tract was present in the abdomen [ 53 ]  . abbiamo gi accennato alla visione unitaria compresa nella definizione malformazioni bronco - polmonari e dellintestino primitivo [ 32 ]  . 
in tal senso , abbiamo recentemente pubblicato 2 casi misconosciuti di fistola tracheo esofagea ( rispettivamente in 2 bambine di 5 e 9 anni ) diagnosticati con mdct eseguita per infezioni ricorrenti delle vie aeree . 
 vascular anomalies anomalie vascolari we previously mentioned that development of the airways abbiamo gi detto come lo sviluppo delle vie aeree e del radiol med ( 2011 ) 116 : 133151 and circulatory system runs parallel [ 30 , 31 ] and described anomalies such as pulmonary agenesis / hypoplasia , sequestration and scimitar syndrome . 
this section briefly describes the compressions and dislocations of the tracheobronchial tree produced by anomalous anatomical relations , as in the case of the double aortic arch [ 54 ] or dilatation of the heart or pulmonary vessels in a setting of congenital heart defects . these cases can now be studied by mdct and / or mr imaging . 
in our opinion , mdct should be preferred when a study of the pulmonary parenchyma and airways is deemed necessary and in the case of critical patients needing short scanning times without sedation or anaesthesia . 
mr imaging is ideal in conditions requiring serial studies , screening , flow evaluation , biventricular function or intracardiac anatomy [ 16 ]  . sistema vascolare corrano paralleli [ 30 , 31 ] e abbiamo gi descritto anomalie come agenesia / ipoplasia polmonare , sequestro e sindrome della scimitarra . 
facciamo ora un accenno alle compressioni e dislocazioni dellalbero tracheo - bronchiale causate da anomali rapporti anatomici , come nel caso del doppio arco aortico [ 54 ] , o dalla dilatazione del cuore o dei vasi polmonari nellambito di cardiopatie congenite . 
a nostro parere da preferire la mdct quando si ritenga necessaria una valutazione anche del parenchima polmonare e delle vie aeree , e nel caso di paziente critico che necessiti di tempi brevi di scansione che evitino sedazione o anestesia . 
la rm ideale per le condizioni che richiedano studi seriati , screening o valutazione flussi , funzioni biventricolari , anatomia intracardiaca [ 16 ]  . conclusions conclusioni thanks to isotropic resolution and the multiplanar capabilities of mdct , which significantly increase diagnostic confidence even in the most complex cases , the indications for ct in paediatric chest imaging have been significantly extended . 
in the setting of pulmonary malformations , the wide range of associated anomalies requires a multisystem evaluation , an area in which mdct is gaining a key role as a noninvasive approach . 
the maxim : always look at the airway must constantly be borne in mind . la mdct grazie alla risoluzione isotropica e alle conseguenti possibili ricostruzioni multiplanari , che rinforzano significativamente la confidenza diagnostica anche nei casi pi complessi , ha incrementato in modo significativo le indicazioni della tc nellimaging del torace pediatrico . 
intravascular contrast media used in diagnostic imaging are drugs in the complete sense of the term , even though they have unique characteristics which in many ways distinguish them from other pharmacological agents . 
the off - label use of contrast media in diagnostic imaging is a little - investigated field and most commonly , but not exclusively , applies to gadolinium - based contrast media used in mr angiography as well as cardiac and paediatric applications . 
as contrast media are to all effects pharmaceutical agents , their off - label use can be considered admissible within the limitations laid down by the italian law in force ( article 3 of law 94 / 98 ) and its interpretation , i.e. 
the use of contrast media in modern imageriassunto scopo del nostro studio stato analizzare lutilizzo offlabel dei mezzi di contrasto ( mdc ) organo - iodati e per risonanza magnetica ( rm ) utilizzati in diagnostica per immagini e valutare i profili di responsabilit ed i risvolti medico - legali che possono derivare da tale impiego . il termine off - label indica , per lo pi , lutilizzo di farmaci conosciuti , ma per i quali nuove evidenze scientifiche propongono un loro uso con modalit ed in situazioni cliniche non espressamente previste nella scheda tecnica ed al di fuori dei limiti di autorizzazione allimmissione in commercio . 
i mezzi di contrasto endovascolari utilizzati in diagnostica per immagini sono farmaci a tutti gli effetti , seppure con caratteristiche uniche che per molti versi li distinguono dagli altri preparati farmacologici . 
lutilizzo off - label dei mezzi di contrasto in diagnostica per immagini risulta un campo ancora poco esplorato che trova pi spesso , ma non solo , applicazione tra gli agenti di contrasto a base di gadolinio usati in angio - rm , in applicazioni cardiache e pediatriche . 
in cases in which the information contained in the information leaflet is modified and updated in any way whatsoever ( indications , dosage , at others ) , specifically if restrictions are introduced in accordance with the law in force , the pharmaceutical industry must provide formal and timely notification to radiologists . 
laddove vengano modificati ed aggiornati in qualsiasi senso ( indicazione , posologia , ecc . ) , specificatamente in senso restrittivo , gli elementi riportati nel foglio illustrativo , ai sensi delle normative vigenti , lindustria deve darne tempestiva e formale comunicazione ai medici radiologi . 
si propone , infine che nella refertazione venga segnalato non solo il tipo ma anche la dose di mdc utilizzato . parole chiave mezzi di contrasto indicazioni introduction introduzione the prescription and administration of drugs outside their approved indications , route of administration or use , which is defined as off - label , is still an open question in medical and legal settings . 
the term off - label generally indicates the use of known drugs for which new scientific evidence suggests use in a manner and in clinical scenarios not explicitly addressed by the drug data sheet and is outside the indications for which the drug was approved . however , the term off - label also indicates the use of drugs with a different route of administration and dosage from those indicated in the information leaflet . 
in some cases off - label prescriptions provide a valid therapeutic alternative for diseases that do not respond to current treatment . in addition , compassionate drug use is defined as the use of nonapproved pharmaceuticals in a group of patients affected by a life - threatening , chronic or severely disabling disease and who cannot be treated satisfactorily with an approved medication . 
il termine off - label indica , per lo pi , lutilizzo di farmaci conosciuti ma per i quali nuove evidenze scientifiche propongono un loro uso con modalit ed in situazioni cliniche non espressamente previste nella scheda tecnica ed al di fuori dei limiti di autorizzazione allimmissione in commercio . 
648 introduce per la prima volta nellordinamento la possibilit di prescrivere e utilizzare farmaci al di fuori delle indicazioni terapeutiche . scopo di questo lavoro quello di analizzare lutilizzo off - label dei mezzi di contrasto ( mdc ) organo - iodati e per risonanza magnetica ( rm ) utilizzati in diagnostica per immagini e quello di valutare i profili di responsabilit ed i risvolti medico - legali che possono derivare da tale impiego . radiol med ( 2011 ) 116 : 114 characteristics that in many ways distinguish them from other pharmacological agents . regulatory framework definitions as laid down in italian legislative decree no . 
i , article 1 , a drug product or drug is defined as : any substance or compound presented as having curative or prophylactic properties of human diseases ; any substance or compound which can be used in humans or administered to humans with the aim of restoring , correcting or modifying physiological functions , by exerting an immunological or metabolic action , or used to establish a medical diagnosis . 
 ( therefore , the definition fully includes not only the iodinated organic and mr contrast media considered in this paper , but also all other contrast media oral and sonographic and radiotracers . ) intravascular contrast media are pharmaceuticals with special characteristics . 
multidetector computed tomography ( mdct ) ] , almost always with high concentrations and without the aim of producing pharmacological effects . conditions for the use of drugs an approved medication is defined as a reference - listed drug . 
a generic drug is a drug that is bioequivalent to a reference drug with an expired patent and is approved with identical amounts of the same active ingredients , the same formulation / presentation , the same route of administration and the same treatment indications . 
the term generic has proven to be unfortunate in that it is perceived by the general public to mean similar but not the same as the reference drug for the same condition . 
24 april 2006 contains detailed regulations regarding the procedures and the phases of launching and maintaining drugs on the e tanto perch , come preciseremo in seguito , i mezzi di contrasto endovascolari utilizzati in diagnostica per immagini sono farmaci a tutti gli effetti , seppure con caratteristiche uniche che per molti versi li distinguono dagli altri preparati farmacologici . la normativa definizioni ai sensi del dl 24 aprile 2006 , n . 
1 , si definisce prodotto medicinale o medicinale : ogni sostanza o associazione di sostanze presentata come avente propriet curative o profilattiche delle malattie umane ; ogni sostanza o associazione di sostanze che possa essere utilizzata sulluomo o somministrata alluomo allo scopo di ripristinare , correggere o modificare funzioni fisiologiche , esercitando unazione immunologica o metabolica , ovvero di stabilire una diagnosi medica ( quindi tale definizione comprende a pieno diritto non solo i mezzi di contrasto organo - iodati e per rm , oggetto di questo lavoro , ma tutti i mezzi di contrasto digestivi , ecografici ed i radio farmaci )  . i mezzi di contrasto endovascolari sono farmaci con caratteristiche particolari : sono , infatti , farmaci iniettati spesso in larghe dosi ed a velocit estremamente rapida , con limpiego degli iniettori automatici ( ad esempio in tomografia computerizzata multidetettore [ tcmd ] ) , quasi sempre a concentrazioni elevate e non hanno lobiettivo di determinare effetti farmacologici . condizioni di utilizzabilit dei farmaci un medicinale autorizzato viene definito medicinale di riferimento . 
si definisce medicinale generico un medicinale che bioequivalente rispetto ad un medicinale di riferimento , con brevetto scaduto , autorizzato con la stessa composizione quali - quantitativa in principi attivi , la stessa forma farmaceutica , la stessa via di somministrazione e le stesse indicazioni terapeutiche . 
per questa ragione i prodotti generici sono stati ridefiniti medicinali equivalenti ( legge [ l ] 149 del 26 luglio 2005 ) [ 2 ]  . nessun medicinale pu essere immesso in commercio sul territorio nazionale senza aver ottenuto lautorizzazione allimmissione in commercio ( aic ) dallagenzia italiana del farmaco ( aifa ) o unautorizzazione comunitaria a norma del regolamento ( ce ) n . 
219 contiene una dettagliata disciplina relativa alle procedure ed alle fasi di immissione e mantenimento in commercio dei farmaci , disciplinando , non solo le modalit di etichettatura del farmaco e di redaradiol med ( 2011 ) 116 : 114 market , regulating not only the labelling of drugs and the format and contents of the information leaflet , but also modifications regarding drugs that have already received marketing approval and suspension of the marketing of a drug . whereas the reader should refer to the full text of the law in question for a complete listing of all of regulatory points , it seems appropriate , given the aims of this paper , to emphasise that this law provides a detailed regulatory framework regarding the conditions for marketing drugs and the considerations to adopt in terms of safeguarding public health , by laying down specific obligations for the marketing authorisation holder ( which cover drug labelling , the format and content of the information leaflet ) and regulating the manner of disposing of stocks or withdrawing products from the market in the event of approval of modifications with respect to the original prescriptions . 
 zione del foglio illustrativo , quanto anche le ipotesi di modifiche relative ai farmaci di cui sia stato gi autorizzato il commercio e di sospensione della commercializzazione del farmaco . nel rinviare al testo integrale della legge per una esaustiva e puntuale elencazione di tutti i dettami normativi , appare opportuno stante la finalit del presente lavoro evidenziare che con il citato provvedimento normativo viene dettata una dettagliata disciplina in ordine alle condizioni di commercializzazione dei farmaci ed agli accorgimenti da adottare a tutela della salute pubblica , sia prescrivendo specifici obblighi per il titolare dellaic ( tra i quali , letichettatura dei farmaci , le modalit di redazione del foglietto illustrativo ed il contenuto dello stesso ) , sia disciplinando le modalit di smaltimento delle scorte o di ritiro delle confezioni nelle ipotesi di autorizzazione di modifiche rispetto alle prescrizioni originarie . 
 off - label use of drugs off - label use may include a use not present in the product characteristics , or when the clinical indication has been approved but the dosage and route of administration are different from those registered . 
the off - label use of a drug is a risk activity ( with possible consequences for the physician of both a regulatory and civil and / or criminal nature ) that is possible only under certain conditions . 
 the following conditions are , in fact , indispensable : provision of information for the patient and formal consent ; inability of satisfactorily treating the patient with already tested drugs ( and therefore also contrast media ) in rigorous adherence to the specifications of the information leaflet ; an authoritative and documented scientific basis of international standing that supports and endorses the off - label treatment choice [ 5 , 6 ]  . off - label can be classified into : off - evidence : regardless of the indication , there is insufficient information available on safety , activity and efficacy of the drug to establish the riskbenefit ratio ; absolute off - label : the prescription of a drug for a nonapproved indication ; relative off - label : when the indication is approved for the disease in question but the dosage or route of administration or duration are different from those approved [ 7 ]  . uso dei farmaci off - label luso off - label si pu verificare per un impiego non presente nella scheda tecnica , oppure quando lindicazione clinica autorizzata , ma il dosaggio e le modalit di somministrazione sono diverse rispetto a quanto indicato nella registrazione . 
luso off - label di un farmaco unattivit a rischio ( dalla quale possono , peraltro , derivare conseguenze per il medico sia disciplinari , sia civili e / o penali ) possibile solo a determinate condizioni . 
 fin da ora si indica che indispensabile che ricorrano le seguenti condizioni : linformazione al paziente e la formale raccolta del consenso ; limpossibilit di trattare utilmente il paziente attraverso i farmaci ( e quindi anche i mezzi di contrasto ) gi sperimentati , nel rigoroso rispetto di quanto riportato nel foglio illustrativo ; un autorevole documentato fondamento scientifico , di livello internazionale , che sostenga ed avalli la scelta terapeutica off - label [ 5 , 6 ]  . possibile classificare lutilizzo loff - label in : off - evidence : indipendentemente dallindicazione , le informazioni a disposizione sulla sicurezza , attivit ed efficacia del farmaco non sono sufficienti a documentare il rapporto rischio - beneficio ; off - label assoluto : consiste nella prescrizione di un farmaco per un indicazione non prevista ; off - label relativo : quando lindicazione esiste per quella malattia ma , ad esempio , si usa un dosaggio diverso o una diversa via di somministrazione o una durata non prevista [ 7 ]  . regulations the off - label use of drugs has over time been regulated , and although the framework is not systematically strucla pratica di utilizzo dei farmaci off - label ha trovato nel riferimenti normativi radiol med ( 2011 ) 116 : 114 tured , it does have some relatively well - defined components . 
prior to 1998 , the subject was regulated by the general principle of professional responsibility : the physician was free to prescribe any drug to resolve any condition whenever she or he thought it appropriate for the health of the patient . 
23.12.1996 [ 9 ] , introduced into the italian legal system for the first time the possibility of prescribing and using drugs charged to the national health service ( nhs ) outside their indications approved by the regulatory body . 
in particular , article 1 , paragraph 4 of the law states that : ...whenever there is no valid ( therapeutic ) alternative , the following drugs may be fully charged to the national health service : innovator drugs approved for use in other countries but not in italy , drugs undergoing clinical trial but not yet approved and drugs used for a ( therapeutic ) indication different from the approved indication . 
these drugs shall be included in a list which shall be periodically updated by the national drug evaluation board [ commissione unica del farmaco ( cuf ) ] in compliance with the procedures and criteria adopted by the board . the list of drugs consists of medications for which phase ii trials have been conducted and also contains provisions indicating the conditions and manner of use of each individual drug . 
the request to include a drug in the list can be made by the technical scientific committee [ commissione tecnico scientifica ( cts ) ] of aifa or upon request by various associations , scientific bodies , hospital trusts , universities and scientific institutions . 
the request requires that these bodies deliver to the cts detailed documentation demonstrating the seriousness of the disease and the lack of valid treatment options or diagnostic alternatives in the case of contrast media the description of the proposed treatment plan , data indicating the likely cost incurred by the patient for 1 months treatment or for a cycle of treatment , approval of the drug in italy or abroad and all scientific documentation with the relevant clinical data . 
similarly important is the information that needs to be provided by the physician to the patient to obtain written consent , which should state that the patient is aware of the possible risks and benefits of the proposed treatment . 
648 [ 9 ] , viene introdotta per la prima volta nel nostro ordinamento la possibilit di prescrivere e utilizzare , a carico del sistema sanitario nazionale ( ssn ) , farmaci al di fuori delle indicazioni approvate dallautorit regolatoria . 
1 , comma 4 della legge , dispone testualmente che qualora non esista valida alternativa ( terapeutica ) , sono erogabili a totale carico del ssn i medicinali innovativi la cui commercializzazione autorizzata in altri stati ma non sul territorio nazionale , i medicinali non ancora autorizzati ma sottoposti a sperimentazione clinica e i medicinali da impiegare per unindicazione ( terapeutica ) diversa da quella autorizzata , inseriti in apposito elenco predisposto e periodicamente aggiornato dalla commissione unica del farmaco ( cuf ) conformemente alle procedure ed ai criteri adottati dalla stessa . lelenco dei farmaci composto da medicinali che alla loro base hanno studi clinici di fase ii e contiene , anche , provvedimenti e determinazioni attraverso le quali vengono indicate quali sono le condizioni e le modalit duso dei singoli medicamenti . 
 la richiesta di inserimento di un farmaco nella lista , pu avvenire per iniziativa della commissione tecnico scientifica ( cts ) dellaifa o tramite la richiesta da parte di associazioni varie , societ scientifiche , aziende sanitarie , universit e tutte quelle strutture a carattere scientifico . 
per richiedere linserimento necessario che questi enti facciano pervenire alla cts una documentazione articolata , nella quale viene dimostrata la gravit della patologia e lassenza di valide alternative terapeutiche e di alternative diagnostiche in caso di mdc , la descrizione del piano terapeutico proposto , i dati indicativi del costo del trattamento mensile o per ciclo di terapia per paziente , lautorizzazione del medicinale in italia o allestero e tutta la documentazione scientifica con relativi dati clinici . 
di natura altres importante linformazione che deve essere fornita dal medico al paziente per poi acquisire il consenso per iscritto da parte del paziente , dove viene espresso che il paziente a conoscenza degli radiol med ( 2011 ) 116 : 114 april 1998 ( known as the di bella law ) [ 10 ] codified the principle according to which the therapeutic activity of the physician is only fully legitimate when the drug has been previously approved by the regulatory body for the same route of administration , dosage or indication for which it is effectively prescribed to the patient . 
article 3 of this law , in fact , explicitly lays down the conditions according to which drugs may be prescribed under direct responsibility of the physician for indications not contemplated by the drug data sheet : compliance with the approved therapeutic indications article 3 , paragraph 1 : except for the provisions of paragraphs 2 and 3 , when prescribing a speciality medicine or other industrially produced medication , the physician shall comply with the therapeutic indications , the route of administration and dosage outlined in the marketing authorisation issued by the ministry of health . article 3 , paragraph 2 : in individual cases the physician may , under her / his own responsibility and after having informed the patient and having received their consent , use an industrially produced medication for an indication or route of administration or use other than those approved , i.e. 
23 december 1996 , if the physician herself / himself believes , on the basis of documented data , that the patient cannot be satisfactorily treated with drugs and therefore with contrast media for which that therapeutic indication or route of administration or dosage has already been approved and provided that the use is known and in compliance with studies appearing in internationally accredited scientific publications . therefore , this regulation outlines the degree of discretion available to the physician in her / his clinical evaluation provided that international scientific publications are available that confirm that the proposed use is already known and has already been tested . 
in addition to this regulation , it should be noted that the off - label use of drugs is also regulated by the general prescription of the professional code of physicians [ 11 ] , in particular , section iv : diagnostic examinations and therapeutic treatment , article 12 : prescription and therapeutic treatment : ...the prescription of a diagnostic examination and / or treatment involves the professional and ethical responsibility of the physician and must follow an evidence - based diagnosis , or at least a well - founded diagnostic suspicion . 
given this requirement , the physician is free to plan , choose and apply any diagnostic and treatment aid even on an in - patient basis , notwithstanding the freedom of the patient to refuse and accept the responsibility for that refusal... 
94 ( cosiddetta legge di bella ) [ 10 ] ha invece trovato codificazione normativa il principio secondo il quale lattivit curativa del medico reputata pienamente legittima soltanto allorquando il medicinale sia stato preventivamente autorizzato dallautorit regolatoria per le medesime modalit di somministrazione , dosaggi o indicazioni terapeutiche per le quali effettivamente prescritto al paziente . 
larticolo 3 della suddetta legge stabilisce infatti espressamente le condizioni alle quali consentito , sotto diretta responsabilit del medico prescrivere farmaci per indicazioni non contemplate nella scheda tecnica : osservanza delle indicazioni terapeutiche autorizzate : 1 . 
fatto salvo il disposto dei commi 2 e 3 , il medico , nel prescrivere una specialit medicinale o altro medicinale prodotto industrialmente , si attiene alle indicazioni terapeutiche , alle vie e alle modalit di somministrazione previste dallautorizzazione allimmissione in commercio rilasciata dal ministero della sanit . 
in singoli casi il medico pu , sotto la sua diretta responsabilit e previa informazione del paziente e acquisizione del consenso dello stesso , impiegare un medicinale prodotto industrialmente per unindicazione o una via di somministrazione o una modalit di somministrazione o di utilizzazione diversa da quella autorizzata , ovvero riconosciuta agli effetti dellapplicazione dellarticolo 1 , comma 4 , del decreto - legge 21 ottobre 1996 , n . 
536 , convertito dalla legge 23 dicembre 1996 , n . 648 , qualora il medico stesso ritenga , in base a dati documentabili , che il paziente non possa essere utilmente trattato con medicinalie quindi anche mezzi di contrasto per i quali sia gi approvata quella indicazione terapeutica o quella via o modalit di somministrazione e purch tale impiego sia noto e conforme a lavori apparsi su pubblicazioni scientifiche accreditate in campo internazionale . 
 quindi questa norma si premura di delineare i margini di discrezionalit consentiti al medico nella sua valutazione clinica , a condizione che esistano pubblicazioni scientifiche accreditate in campo internazionale , che confermino come limpiego proposto gi noto e sperimentato . 
pur prendendo atto del dato normativo deve tuttavia rilevarsi che lutilizzo off - label dei farmaci regolamentata anche dalle regole e prescrizioni generali dettate dal codice deontologico dei medici [ 11 ] , in particolare al capo iv accertamenti diagnostici e trattamenti terapeutici , allart . 
12 prescrizione e trattamento terapeutico stabilisce che la prescrizione di un accertamento diagnostico e / o di una terapia impegna la responsabilit professionale ed etica del medico e non pu che far seguito a una diagnosi circostanziata o , quantomeno ad un fondato sospetto diagnostico . 
su tale presupposto al medico riconosciuta autonomia nella programmazione , nella scelta e nellapplicazione di ogni radiol med ( 2011 ) 116 : 114 and not approved is allowed provided their efficacy and tolerability have been scientifically documented . 
in these cases , once written consent has been provided by the informed patient , the physician accepts responsibility for the treatment and s / he is held to monitor its effects . 
the physician is obliged to immediately inform the competent bodies of any adverse reactions which may arise during the treatment . off - label use of intravascular gadolinium - based and iodinated organic contrast media and adverse reactions in diagnostic imaging , the off - label use of contrast media [ 12 ] mostly involves gadolinium - based contrast media , especially in mr angiography , cardiac and paediatric applications [ 13 , 14 ] and patients younger than 2 years [ 15 ]  . 
the off - label use must be based on scientific evidence , serve the patients best interest , and requires greater care than would generally be the case in medicalradiological practice [ 16 ]  . 
nephrotoxicity from gadolinium chelates has been documented in both animals and humans , and nephrotoxic effects associated with high doses has been reported following the intra - arterial administration of gadolinium chelates [ 17 ]  . 
given their hypothesised low level of nephrotoxicity ( due to the small osmolar load ) in the past , gadolinium derivatives have been used to substitute iodinated organic contrast media for radiographic and mdct examination in patients at risk of nephrotoxicity from iodinated organic agents [ 15 , 18 , 19 ]  . however , the quality of the images of radiographic examinations obtained with gadolinium - based contrast media is lower than the image quality obtained with iodine - based agents [ 20 ]  . 
in order to deal with the inferior image quality , data regarding the relative toxicity of gadoliniumbased contrast media were extrapolated to the doses used in mr examinations to use them in radiographic procedures [ 21 ]  . 
this fact , together with the suggested role of gadolinium in nephrogenic systemic fibrosis ( nsf ) , prompted the european society of urogenital radiology ( esur ) to contraindicate their use for radiographic procedures [ 22 ]  . 
the use of double or even triple doses of gadolinium - based contrast media ( off - label use ) required in mr angiography procedures may expose patients to greater risk [ 23 , 24 ]  . 
the relationship between gadolinium - based contrast media and nsf has been reported not only in a dose - dependent manner but also in relation to the type of contrast medium presidio diagnostico e terapeutico anche in regime di ricovero , fatta salva la libert del paziente di rifiutare e di assumere la responsabilit del rifiuto stesso . 
obbligo del medico segnalare tempestivamente alle autorit competenti , le reazioni avverse eventualmente comparse durante un trattamento terapeutico . utilizzo off - label dei mezzi di contrasto a base di gadolinio e organoiodati per via iniettiva e reazioni avverse in diagnostica per immagini lutilizzo off - label dei mezzi di contrasto [ 12 ] trova applicazione con maggiore frequenza per quanto riguarda gli agenti di contrasto a base di gadolinio ( gd ) , e segnatamente in angiografia mediante rm , in applicazioni cardiache e pediatriche [ 13 , 14 ] , ed in pazienti di et inferiore ai due anni [ 15 ]  . 
luso off - label si deve basare sulle evidenze scientifiche , utilizzate nel miglior interesse del paziente , e richiede prudenza maggiore di quella che deve essere comunque esercitata nella pratica medico - radiologica in generale [ 16 ]  . 
la nefrotossicit dei chelati di gadolinio stata documentata in uomini ed animali e lincidenza di effetti nefrotossici riportata per lutilizzo di alte dosi , a seguito di somministrazione intra - arteriosa dei chelati di gadolinio [ 17 ]  . 
per la loro ipotizzata bassa nefrotossicit ( dovuta al minimo carico osmolare ) in passato si segnala lutilizzo dei derivati di gadolinio come sostituti dei mdc organoiodati per esami radiografici e tcmd , in pazienti a rischio di nefropatia da contrasto organo - iodati [ 15 , 18 , 19 ]  . 
ma la qualit delle immagini di esami radiografici ottenuta con agenti a base di gadolinio inferiore rispetto alla qualit delle immagini ottenute con mdc a base di iodio [ 20 ]  . 
per far fronte a tale inferiore qualit di immagini , si estrapolarono i dati relativi alla tossicit dei mdc a base di gadolinio alle dosi utilizzate per esami rm , per impiegarli in procedure radiografiche [ 21 ]  . 
essi infatti per avere una migliore capacit di attenuazione del fascio radiante devono essere somministrati a concentrazioni ed a dosi pi elevate che sono , per , anche pi nefrotossiche . 
lutilizzo di dosi doppie o addirittura triple di mdcgd ( uso off - label ) richieste in procedure di angio - rm possono esporre i pazienti ad un maggiore rischio [ 23 , 24 ]  . perci consigliato in linea generale limpiego della dose pi bassa compatibile con le esigenze diagnostiche di gd per evitare anche il rischio di nsf . 
la relazione tra agenti radiol med ( 2011 ) 116 : 114 used on the basis of its physical and chemical properties . this suggests the clear need to avoid inappropriate use , excessive doses , and the need to select the contrast medium with the most appropriate characteristics for the clinical case [ 25 ]  . 
this is in line with the emea press release of 20.11.2009 circulated by aifa [ 26 ]  . apart from the risk of immediate adverse reactions , one of the pathological conditions of greatest concern produced by iodinated organic contrast media is contrastinduced nephropathy ( cin )  . 
the definition of cin states that within 4872 h from the administration of the contrast medium , there is an increase of at least 25% or at least 0.5 mg / dl of creatininaemia with respect to the baseline value [ 27 ]  . 
after having reached a peak in the third / fourth day after injection of contrast medium , creatininaemia falls and returns to baseline values within 1015 days [ 17 , 28 ]  . 
the issue is still wide open , considering also the fact that some authors [ 32 ] have suggested that so - called cin can be induced even without administration of contrast mediu the nephrotoxic potential of various contrast media fundamentally depends on the dose administered . 
it is therefore understandable why the reported incidence of cin varies from values of 1%2% in patients with normal kidney function to 11% in hospitalised patients and up to 20%50% in some at - risk categories ( end - stage kidney failure and diabetes mellitus ) [ 33 , 34 ]  . although the nephrotoxicity of iodinated organic contrast media with normal kidney function is very low , it should be borne in mind that nephrotoxicity is dose dependent ; therefore , the risk of kidney damage is directly proportional to the dose of contrast medium injected [ 35 ]  . with regard to the type of iodinated organic contrast medium , it should be emphasised that data in the literature are not fully in agreement . 
therefore , at present , it is best to assume that all nonionic contrast media , both low osmolarity and iso - osmolar types , can further deteriorate kidney function in patients with impaired kidney function [ 21 ]  . as high doses of iodinated organic contrast media can trigger the onset of cin , caution in the off - label use of such media is advisable . 
even gadolinium - based contrast media can induce nephrotoxicity , especially in high doses in patients with kidney failure , because the pharmacokinetics are very similar to those of iodinated organic contrast media [ 3638 ]  . di contrasto a base di gd e nsf segnalata non solo dose dipendente , ma anche legata al tipo di agente di contrasto impiegato , in base alle caratteristiche fisico - chimiche : pertanto occorre evitare logicamente luso inappropriato , dosi eccessive , selezionando lagente di contrasto con le caratteristiche pi appropriate per il caso clinico [ 25 ]  . 
e tanto anche ai sensi del comunicato stampa emea del 20.11.2009 diffuso dallaifa [ 26 ]  . al di l del rischio di reazioni avverse immediate , una delle condizioni patologiche di maggior interesse indotto dai mdc organo - iodati la nefropatia da mdc . 
la contrast induced nephropahy ( cin ) o nefropatia da mdc organoiodati , definita in genere come un deterioramento acuto della funzione renale susseguente alla somministrazione di mdc in assenza di altre possibili cause di insufficienza renale acuta . 
la definizione di nefropatia da mdc prevede che dopo 4872 ore dalla somministrazione del mdc si verifichi un aumento almeno del 25% o almeno di 0 , 5 mg / dl della creatininemia rispetto al valore basale [ 27 ]  . 
dopo aver raggiunto il picco in terza / quarta giornata dalliniezione del mdc , la creatininemia scende e torna ai valori basali in 1015 giorni [ 17 , 28 ]  . 
la cin rappresenta la terza causa ( 11% ) dei casi di insufficienza renale acuta nei pazienti ospedalizzati , dopo lipoperfusione renale e linsufficienza renale postchirurgica [ 29 ]  . 
comprensibile perci il motivo per cui lincidenza della cin riportata variare da valori di 1%2% in pazienti con normale funzionalit renale all11% nei pazienti ospedalizzati fino al 20%50% in alcune categorie a rischio ( ir allo stato terminale e diabete mellito ) [ 33 , 34 ]  . nonostante la nefrotossicit da mdc organo - iodati in pazienti con normale funzionalit renale sia molto bassa , bene tenere presente che la nefrotossicit dose dipendente , quindi il rischio di danno renale tanto maggiore quanto maggiore la dose di mdc iniettata [ 35 ]  . 
per quanto riguarda il tipo di mdc organo - iodato bene sottolineare che i dati in letteratura non sono univoci : pertanto , al momento attuale bene considerare che tutti i mdc non ionici , sia a bassa osmolarit che iso - osmolari , possono deteriorare ulteriormente la funzionalit renale in pazienti con funzionalit renale gi compromessa [ 21 ]  . 
anche gli agenti di contrasto a base di gd possono indurre nefrotossicit specie ad alte dosi in pazienti in insufficienza renale poich la loro farmacocinetica molto simile a quella dei mdc organo - iodati [ 3638 ]  . radiol med ( 2011 ) 116 : 114 role of the ethics committee for the off - label use of drugs ( and for compassionate use ) ruolo del comitato etico per lutilizzo dei farmaci offlabel ( e per uso compassionevole ) the establishment of an italian national committee for bioethics followed resolution no . 
6 - 00038 , approved on 5 july 1988 by the assembly of the chamber of deputies at the end of a debate on the problems of life that saw the government involved in promoting a dialogue , at both the national and international level , on the state of biomedical and genetic engineering research with a view to ensuring respect for human dignity and freedom [ 39 ]  . 
the committee has been entrusted with the task of guiding the legislative and administrative instruments required for defining the criteria to use in medical and biological practice to protect human rights . 
it also has the task of guaranteeing correct information for public opinion on the problematic aspects and the implications of therapy , diagnostic techniques and progress in the biomedical sciences . 
the opinion expressed by the ethics committee is compulsory and binding for beginning clinical testing , which nonetheless can only begin with approval from the executive directors of the hospital trust . as with all healthcare treatment , informed consent is a fundamental prerequisite for performing diagnostic and therapeutic activity , and even more so for experimental studies . 
therefore , the physician prescribing the drug and in the specific case the radiologist , with indications other than those approved in terms of dosage , frequency of administration , duration or route of administration is directly responsible for the off - label use of the drug , informing the patient and obtaining informed consent as well as for monitoring the patient throughout the treatment . a special aspect regards the off - label use of drugs such as contrast media in emergency conditions . 
in these cases , where there is the so - called state of need , it is the radiologist who takes responsibility for the use of the drugs with dosage and route of administration that , based on both science and conscience , she or he believes is necessary for the individual clinical case . listituzione del comitato nazionale per la bioetica ha fatto seguito alla risoluzione n . 
6 - 00038 , approvata il 5 luglio 1988 dallassemblea della camera dei deputati al termine di un dibattito su i problemi della vita , nella quale il governo veniva impegnato a promuovere un confronto , anche a livello internazionale , sullo stato della ricerca biomedica e dellingegneria genetica nella prospettiva e nel rispetto della libert umana [ 39 ]  . 
ha , inoltre , il compito di garantire una corretta informazione dellopinione pubblica sugli aspetti problematici e sulle implicazioni dei trattamenti terapeutici , delle tecniche diagnostiche e dei progressi delle scienze biomediche . come gi detto , i farmaci disponibili in italia vengono autorizzati allimmissione in commercio dallaifa . 
pertanto il medico prescrittore , e quindi nel caso specifico il medico radiologo ai fini diagnostici , di farmaci con indicazioni diverse da quelle autorizzate , per dosaggio , frequenza di somministrazione , durata o via di somministrazione direttamente responsabile delluso offlabel del farmaco , dellinformazione al paziente e dellacquisizione del consenso informato da parte dello stesso nonch del monitoraggio durante tutto il trattamento . 
un aspetto particolare riguarda leventuale impiego off - label di farmaci , quali i mezzi di contrasto in urgenza indifferibile / emergenza : in questi casi , laddove si configuri il cosiddetto stato di necessit , il medico radiologo che si assume la responsabilit dellimpiego degli stessi farmaci a dosaggio e via di somministrazione che , in scienza e coscienza , riterr utili per il singolo caso clinico . medicolegal aspects : liability of the radiologist in the off - label use of contrast media aspetti medico - legali : la responsabilit del medico radiologo nellimpiego off - label dei mezzi di contrasto the main problem for the radiologist regarding the off - label use of contrast media is undoubtedly related to the liability profiles [ 40 ] resulting from this practice . 
94 / 1998 establishes that when prescribing and therefore using a speciality medicine , the physician shall comply with the therapeutic indications , the route of administration and dosage outlined in the marketing authorisation issued by the ministry of health . 
3 il problema principale per il medico radiologo relativo allutilizzo off - label dei mezzi di contrasto , indubbiamente , legato ai profili di responsabilit [ 40 ] conseguenti alla applicazione di tale pratica . 
come detto , la legge 94 / 1998 stabilisce che il medico nel prescrivere , e quindi nellimpiegare , una specialit medicinale si attiene alle indicazioni terapeutiche , alle vie e alle modalit di somministrazione previste dallautorizzazione allimmissione in commercio rilasciata dal ministero della sanit . 
al comma radiol med ( 2011 ) 116 : 114 of that law establishes that in individual cases , the physician may , under her or his own responsibility and after having informed the patient and having received their consent , use an industrially produced medication for an indication or route of administration or use other than those approved , i.e. recognised in terms of the application of article 1 , paragraph 4 of italian legislative decree no . 
23 december 1996 , if the physician herself / himself believes , on the basis of documented data , that the patient cannot be satisfactorily treated with drugs and therefore with contrast media for which that therapeutic indication or route of administration or dosage has already been approved and provided that the use is known and in compliance with studies appearing in internationally accredited scientific publications . 
 anomalous behaviour , so to speak , by the radiologist must be limited to specific and individually defined hypotheses prompted by the benefit that the patient will presumably enjoy [ 41 ]  . 
648 / 98 that provides for the lawful prescription of nonapproved drugs on the condition that they are already included in the list drawn up by the cuf given the lack of alternative therapies . 
 in addition to creating a regulatory framework for the prescription of drugs outside the approved indications , the law also established the applicable sanctions for the physician who prescribes and / or uses a drug off - label outside the regulations . 
94 / 98 states that the violation by the physician of the dispositions of this article is cause for disciplinary proceedings in accordance with the legislative decree of provisional head of state dd . 
233. in addition to the implicit legal liability of professional activities performed under the supervision of a professional body , the off - label use of drugs entails even more complex forms of civil and criminal liability for the physician who chooses to carry out this practice . 
in fact , in the absence of a clear , organised and systematic regulatory framework , the outlines and limitations to legitimate off - label use of drugs have been traced through the interpretation of the courts [ 41 ]  . 
 the assumption of direct liability for pharmacological treatment and / or diagnostic activity and the preliminary identification of scientific evidence supporting off - label use of a drug are still not enough to satisfy all the obligations a physician must meet for the legitimate use of offlabel drugs . 
3 di tale legge , dispone che in singoli casi il medico pu , sotto la sua diretta responsabilit e previa informazione del paziente e acquisizione del consenso dello stesso , impiegare il medicinale / farmaco prodotto industrialmente per un indicazione o una via di somministrazione o una modalit di somministrazione o di utilizzazione diversa da quella autorizzata , ovvero riconosciuta agli effetti dellapplicazione dellart . 
648 , qualora il medico stesso ritenga , in base a dati documentabili , che il paziente non possa essere utilmente trattato con medicinali per i quali sia gi approvata quella indicazione terapeutica o quella via o modalit di somministrazione e purch tale impiego sia noto e conforme a lavori apparsi su pubblicazioni scientifiche accreditate in campo internazionale . 
 la condotta , per cos dire , anomala , da parte del medico radiologo deve essere circoscritta in relazione ad ipotesi specifiche ed individualmente definite , sulla base dei criteri dettati dal beneficio che ci si potrebbe presumibilmente attendere per il paziente [ 41 ]  . 
1 comma 4 l 648 / 98 in cui prevede la lecita prescrizione di farmaci non autorizzati a condizione che siano gi inclusi in un elenco predisposto dalla commissione unica del farmaco in ragione dellassenza di alternative terapeutiche . 
 la vigente normativa oltre a dettare le regole cui deve soggiacere la prescrizione di medicinali al di fuori delle indicazioni autorizzate , disciplina anche le sanzioni applicabili qualora il medico contravvenga alla specifica disciplina legislativa prescrivendo e / o utilizzando un farmaco off - label al di fuori dei vincoli normativi . 
3 della legge 94 / 98 stabilisce che la violazione da parte del medico delle disposizioni del presente articolo oggetto del procedimento disciplinare ai sensi del decreto legislativo del capo provvisorio dello stato 13 settembre 1946 n 233 . al di l di profili di responsabilit disciplinare connaturali ad attivit professionali espletate sotto il controllo di un organo di categoria , dallutilizzo di medicinali off - label possono derivare ben pi complesse forme di responsabilit civile e penale per il sanitario che ricorre a tale pratica . sotto tale profilo in assenza di un dato normativo di riferimento preciso , organico e sistematico i contorni e i limiti del legittimo utilizzo di medicinali off - label sono stati delineati in via interpretativa dalla giurisprudenza di merito e , soprattutto , di legittimit [ 41 ]  . 
 lassunzione di una responsabilit diretta rispetto alla terapia farmacologica e / o allattivit diagnostica ipotizzata e la preliminare identificazione di un avallo esterno di ordine scientifico non esauriscono tuttavia gli obblighi che il medico deve soddisfare ai fini di un legittimo utilizzo off - label dei farmaci . 
accanto alla complessiva valutazione clinica , infatti , necessario che si proceda ad unappropriata informazione del paziente e allottenimento del suo consenso scritto . presupposto per la validit del consenso per un informaradiol med ( 2011 ) 116 : 114 essence must be honest . 
in particular , in the setting of the off - label use of a drug , the information should cover the characteristics of the proposed treatment , the possibility of choosing a more conventional and consolidated treatment and the side effects and adverse events directly connected with the off - label use of drugs . 
the physician must be the bearer of a simplified truth commensurate with the patients level of comprehension at that particular time and in those circumstances , taking care to describe all important issues , especially in terms of risks and benefits . 
on the other hand , whereas implicit consent may be considered admissible and understood in the doctor - patient relationship during delivery of a routine healthcare service , consent must be explicit when the chosen treatment involves the use of off - label drugs : although the law does not enforce written consent in such circumstances , the provision of such consent by the patient will have clear significance for legal purposes [ 42 ]  . the requirement for potential off - label use is that the radiologists choice , notwithstanding the above - mentioned conditions , is backed up by experimental evidence and / or scientific documents that support the rationality of the choice made , especially with reference to the possible advantages / disadvantages of the known and consolidated use for the indication in question . 
lastly , it should always be borne in mind that off - label prescribing obliges the physician to pay special attention to monitoring side effects or possible inefficacy in relation to the expected results [ 42 ]  . zione da parte del sanitario che deve essere essenzialmente onesta . 
in particolare , nel contesto dellimpiego di un farmaco off - label , linformazione deve riguardare le caratteristiche del trattamento ipotizzata , leventualit di una scelta che confermi un trattamento pi tradizionale e consolidato , ovvero gli effetti collaterali e gli eventi avversi direttamente connessi allimpiego di farmaci off - label . 
il medico deve farsi portatore di una verit semplificata e commisurata al livello di comprensione che il paziente pu avere maturato nello specifico momento storico , ambientale o psicologico , avendo cura di descrivere ogni aspetto significativo , con particolare riguardo al rapporto rischio - beneficio . 
daltra parte , mentre un consenso implicito pu considerarsi ammissibile e sottointeso alla relazione tra medico e paziente qualora la prestazione sanitaria abbia contenuti ordinari , esso dovr essere esplicitato quando il trattamento prescelta attinga ad utilizzo del farmaco non autorizzato , cio off - label : in tal caso , pur non essendovi precetto normativo che imponga la forma scritta , la sottoscrizione del consenso da parte del paziente avr certamente una chiara rilevanza ai fini probatori [ 42 ]  . il presupposto per un utilizzo eventuale in off - label che la scelta del medico radiologo , fatti salvi i presupposti suddetti , sia sostenuta da prove sperimentali e / o documenti scientifici che possono supportare la razionalit delle scelta effettuata soprattutto se riferita ai possibili vantaggi / svantaggi di impiego gi noto e consolidato per lindicazione in oggetto . 
infine , non va mai dimenticato che la prescrizione offlabel impone al sanitario una particolare cura ed attenzione nei confronti di una sorveglianza degli effetti collaterali o di un eventuale inefficacia , rispetto le aspettative attese [ 42 ]  . conclusions conclusioni recent data published in the literature suggest that , in general , the off - label use of drugs is a routine practice in 23% of prescriptions [ 12 ] and that off - label use is widely practised in various specialities to the point of being standard practice in paediatrics and intensive care . 
on the basis of scientific data , under his or her direct responsibility and after having obtained informed consent from the patient , the radiologist may decide to treat the patient with a medication or drug ( contrast medium ) produced for an indication , a dosage or route of administration other than those registered . 
whereas it may appear to be logical that a contrast medium should dai dati pi recenti della letteratura emerge che in generale luso di farmaci off - label una pratica routinaria in circa il 23% delle prescrizioni [ 12 ] e che comunque loff - label ampiamente diffuso in varie specialit rappresentando finanche una pratica standard in et pediatrica ed in terapia intensiva . 
ed a tale proposito si precisa che mancano allo stato dati precisi e sufficienti per definire lentit di questo fenomeno in diagnostica per immagini . nella nostra attivit , lopportunit di usare un farmaco , e quindi di un mezzo di contrasto , off label spetta al medico radiologo , che , sulla base di documentazione scientifica e sotto la sua diretta responsabilit , dopo aver informato il paziente e ottenuto il consenso , pu decidere di trattare il proprio assistito con un medicinale / farmaco ( mezzo di contrasto ) prodotto per una indicazione , un dosaggio ed una modalit di somministrazione diverse da quelle registrate . 
per quanto appare logico che il mezzo di radiol med ( 2011 ) 116 : 114 not be administered in the absence of a clear indication , it is worth recalling that modern image - guided medicine cannot effectively forego the use of contrast media . in light of the concept that the behaviour of different molecules is not identical in terms of microcirculation , capillary permeability and distribution haemodynamics of the various compartments and is further differentiated in terms of the organ or body region being examined , these substantial differences in behaviour suggest the preferential use of one molecule rather than another . 
as contrast media are , to all effects , pharmaceutical agents , their off - label use can be considered admissible within the limitations laid down by the italian law in force ( article 3 of law 94 / 98 ) and its interpretation , i.e. , the following criteria must be present : the lack of a valid diagnostic alternative supported by published data ; written informed consent by the patient ; the presence of scientific publications validated at the international level ; assumption of responsibility by the radiologist . of course it is logical , and also highly desirable , that if the information leaflet of a drug is modified and updated in any sense ( indication , dosage , etc . ) , in accordance with the law in force , the pharmaceutical industry shall promptly and formally inform radiologists . 
in conclusion , while emphasising that modern image - guided medicine cannot forego the use of contrast media , we propose that the radiological report indicate not only the type of contrast medium used but also the dose . contrasto non dovrebbe essere somministrato in assenza di una chiara indicazione , bene tener presente che nella medicina moderna image guided non possibile in concreto rinunciare allimpiego dei mezzi di contrasto . sottolineando il concetto che le diverse molecole hanno un comportamento non sovrapponibile nei confronti del microcircolo , della permeabilit capillare e dellemodinamica di ripartizione dei vari compartimenti , in maniera ulteriormente differenziata secondo lorgano o il distretto in esame , si precisa che queste sostanziali differenze di comportamento suggeriscono limpiego preferenziale di una molecola piuttosto che dellaltra . 
rossi1 1sezione di scienze radiologiche , dipartimento di scienze cliniche , 2sezione di medicina legale , dipartimento di anatomia umana , farmacologia e scienze medico - forensi , universit degli studi di parma , ospedale maggiore di parma , via gramsci 14 , 43100 parma , italy 3istituto di radiologia , policlinico universitario campus di germaneto , viale europa , 88100 catanzaro , italy 4radiologia cardio - toracica , dipartimento cardio - toraco - vascolare , policlinico s . 
some important weaknesses emerged , especially regarding requests for radiological examinations ( 22% lacked the clinical question , 27.6% were inappropriate ) , potentially limiting the effectiveness of the diagnostic process and leading to negative effects on the correct risk management process . 
abbiamo riscontrato una elevata percentuale di richieste inappropriate ( 27 , 6% ) e mancanti del quesito clinico ( 22% ) e una discreta precisione del dato anamnestico ( 80 , 6% ) e della formulazione del quesito diagnostico ( 76 , 8% )  . 
sono emerse importanti criticit , soprattutto nelle richieste di esami radiologici ( 22% di richieste senza quesito clinico ; 27 , 6% di richieste inappropriate ) , in grado di limitare lefficacia del processo diagnostico e comportare ripercussioni negative per la corretta gestione del riskradiol med ( 2011 ) 116 : 152162 keywords radiological request radiological report management . 
si palesa la necessit di una maggiore e migliore collaborazione tra clinico e radiologo . parole chiave richiesta radiologica referto radiologico introduction introduzione clinicalanamnestic evaluation , with an assessment of any previous examinations ; con quesito clinico ; the work of the radiologist involves similar or identical duties of documentation and certification to those of other medical specialist areas , even though diagnostic radiology appears to be characterised by a series of unique operating features that set this discipline apart . 
the radiological medical procedure is a specialist medical service having diagnostic and / or interventional aims [ 1 ] and consisting of a set of closely interdependent elements : a justified request by a referring physician that contains a clinical question ; justification for the proposed examination ( or motivated lack of justification , with possible suggestions for alternative modalities and techniques ) ; information for consent and patients consent ; technical execution of the examination and production of interpretation , reporting , communication and discussion images ; with the clinician ; image archiving . the radiologists diagnostic professionalism has two fundamental and distinct expressions : a physical medium ( the radiological finding ) and a paper - based medium ( the report ) , which must be , for the validity and usefulness of the investigation , exactly complementary to each other and together available for further analysis and possibly reproducible on demand . 
the radiologist is also still the only person responsible for producing a written report of the examination or for interpreting a radiological image with clinical and health purposes [ 2 ]  . 
the radiological report is therefore a scientific statement to be used at a scientific level ; it must be understood as an official , final and written interpretation , which must support each diagnostic imaging study and represents , together with the images produced , its final result . lattivit del radiologo comporta problematiche di documentazione e di certificazione analoghe o identiche a quelle di altri settori medico - specialistici , sebbene la radiologia diagnostica appaia contraddistinta da alcune peculiari ed esclusive necessit operative , che conferiscono a tale disciplina caratteri del tutto propri . 
latto medico radiologico rappresenta una prestazione professionale specialistica medica con finalit diagnostiche e / o interventistiche [ 1 ] , costituita da un insieme di elementi strettamente interdipendenti tra loro : motivata richiesta di prestazione del medico prescrivente inquadramento clinico - anamnestico , con valutazione di eventuali esami precedenti ; giustificazione dellesame proposto ( o non giustificazione motivata , con possibile proposta di tecniche e metodologie sostitutive ) ; informativa per il consenso e relativo consenso ; esecuzione tecnica e produzione del referto iconografico ; interpretazione / refertazione / comunicazione / discussione con il clinico ; archiviazione . la professionalit diagnostica del radiologo si concretizza attraverso due fondamentali e distinte espressioni : un supporto fisico ( il reperto radiologico ) ed un supporto cartaceo ( il referto ) , che devono necessariamente , per la validit e lutilit dellindagine compiuta , essere luno esattamente complementare allaltro ed entrambi disponibili per verifiche ulteriori , nonch eventualmente riproducibili a richiesta . 
se lesecuzione tecnica dellesame pu essere delegata al tecnico sanitario di radiologia medica ( tsrm ) , garante anche della qualit tecnica delliconografia , comunque il medico radiologo lunico responsabile cui competono , sulla base dei principi di giustificazione e ottimizzazione ( rispettivamente indicati dagli articoli 3 e 4 del d.lgs. 187 / 00 ) , la scelta della metodologia e delle tecniche idonee ad ottenere il maggior beneficio clinico con il minore detrimento individuale , nonch la valutazione sulle possibilit di utilizzare tecniche sostitutive non basate su radiazioni ionizzanti . di certo , ancora ed esclusivamente al radiologo compete lonere e la responsabilit della refertazione dellesame in forma scritta , ovvero linterpretazione dellimmagine radiologica con finalit clinico - sanitarie [ 2 ]  . 
il referto radiologico rappresenta dunque una dichiarazione di scienza finalizzata alla sua utilizzazione sul piano scientifico ; essa va intesa come 154 radiol med ( 2011 ) 116 : 152162 the aim of this study was to review a series of radiological requests and their matched radiological reports with a view to analysing their correctness and completeness , with reference to the principles presented in the literature and recommended by the italian national referral guidelines [ 3 ] as a means to achieve a reduction in the number of inappropriately prescribed and performed examinations . materials and methods we retrospectively selected 500 reports from our radiology information systempicture archiving and communications system ( ris - pacs ) and subsequently retrieved the related paper - based clinical request form from our radiological archive . 
a total of 167 computed tomography ( ct ) , 166 ultrasound ( us ) and 167 conventional radiology ( x - ray ) examinations were chosen randomly from among 3 , 100 diagnostic studies performed over 3 months and reported by six radiologists of the university hospital of parma . 
two radiologists , with 8 and 10 years experience , respectively , carried out an analysis of the requests and reports according to the parameters listed below . evaluation criteria following are evaluation criteria for radiology requests and reports , which are summarised in table 1 . table 1 criteria used to evaluate requests and reports requests reports presence / absence of the diagnostic question appropriateness of indication completeness of the information formal aspects presence / absence of answer to the diagnostic question completeness of the response given tabella 1 criteri di valutazione delle richieste e dei referti richieste referti presenza / assenza del quesito diagnostico appropriatezza dellindicazione completezza dellinformazione presenza / assenza risposta al quesito diagnostico completezza della risposta aspetti formali interpretazione ufficiale , finale e scritta , che deve accompagnare tutti gli studi di diagnostica per immagini e che , insieme alliconografia prodotta , ne costituisce il risultato . il nostro lavoro si proposto , mediante una revisione casistica di richieste cliniche e relative refertazioni radiologiche , unanalisi delle problematiche correlate alla correttezza e completezza delle richieste e dei referti radiologici , in riferimento ai principi presenti nella letteratura di merito ed a quanto suggerito dalle linee guida nazionali [ 3 ] , il cui fondamentale obiettivo proprio quello di voler perseguire una riduzione del numero di esami inappropriatamente richiesti ed eseguiti . 
 materiali e metodi abbiamo selezionato retrospettivamente dal nostro sistema informatico ( radiology information system - picture archiving and communications system , ris - pacs ) 500 referti ; successivamente sono state recuperate le rispettive richieste cliniche in cartaceo , presenti nellarchivio radiologico . sono stati scelti con metodica random , su 3100 esami diagnostici eseguiti in 3 mesi e refertati da un totale di 6 medici radiologi dellazienda ospedaliero - universitaria ( aou ) di parma , 167 tomografie computerizzate ( tc ) , 166 ecografie e 167 esami di radiologia tradizionale . 
tra questi , 343 esami erano eseguiti in regime di ricovero ospedaliero , i rimanenti 157 erano esami ambulatoriali ; complessivamente il maggior numero desami ( 80% ) stata condotto in regime di elezione . 
 appropriateness of requests from the critical analysis of the 500 requests , 138 ( 28% ) appeared not to fulfil the appropriateness criteria set out in the national referral guidelines . 
specifically , 78 ( 56.5% ) examinations requested were defined as not indicated due a lack of rationale for the investigation , and the remaining 60 examinations ( 43.5% ) were not routinely indicated , i.e. not supported by incontrovertible arguments . 
with regard to the referrers , whereas the absolute number of inappropriate requests differed slightly among those made by intrahospital specialists ( n = 62 ) and by general practitioners ( n = 76 ) , only 18% ( 62 / 343 ) of intrahospital requests was inappropriate , compared with a significant percentage risultati richieste cliniche assenza o presenza del quesito sul totale delle 500 richieste , in 110 casi ( 22% ) il quesito clinico risultato del tutto assente , pur in presenza di unindicazione della metodica da utilizzare . 
nello specifico 78 ( 56 , 5% ) sono definibili come non indicate per mancanza di una base logica allesecuzione dellindagine stessa mentre le rimanenti 60 ( 43 , 5% ) rivestono caratteri di indagini non indicate di routine , cio non sostenute da motivazioni incontrovertibili . 
 completeness of information regarding the requests rated as appropriate ( 362 / 500 ) , the inclusion of clinicalanamnestic information and data from previous imaging investigations appeared to be parameters of specific relevance for assessment of completeness , and substantial correctness was found with regard to the accuracy of this information . 
previous imaging investigations were mentioned in 98 requests , but the radiological history was only vaguely reported in 61 cases ( 62% )  . another qualitative parameter in judging completeness of the request was identified in the generality or specificity of the question in relation to the clinical diagnostic suspicion . it was found that in 12% of cases , the question other was included in the diagnostic question , maybe an expression of the referrers propensity towards so - called defensive medicine . 
in fact , the question other even assuming a legitimate demand for diagnostic completeness in the answer appears too vague and general and likely to raise expectations that cannot always by met by a radiological response . formal errors although no grammatical errors were identified , 39.6% of requests , especially from intrahospital physicians ( 43.7% ) contained acronyms that , although referring to routine medical terms , were not always easy to understand , in part due to legibility problems . 
in 98 richieste si segnalavano gli esami radiologici effettuati in precedenza dal soggetto , ma in ben 61 casi ( 62% ) tale anamnesi radiologica appariva formulata in maniera imprecisa . 
stato rilevato che , nel 12% dei casi , stato utilizzato linterrogativo altro ? nella formulazione del quesito diagnostico , espressione forse di uneccessiva propensione del medico prescrivente verso la cosiddetta medicina difensiva . 
questo termine infatti , pur presupponendo doverose esigenze di completezza diagnostica nella risposta , appare comunque eccessivamente vago e generico , idoneo a suscitare aspettative non sempre esaudibili da una risposta radiologica . 
 errori formali nonostante non siano emersi errori grammaticali , nel 39 , 6% delle richieste , ed in particolare in quelle provenienti dai medici intraospedalieri ( 43 , 7% dei casi ) , sono state utilizzate sigle e / o acronimi che , seppure legati a termini di uso abituale nella pratica medica , non sempre risultano di cos immediata comprensione anche perch legati alla differente intelligibilit delle varie grafie . 
pu segnalarsi , al riguardo , la mancanza del timbro o della firma del medico nell11% ( 55 / 500 ) delle richieste totali , soprattutto in quelle intraospedaliere . radiol med ( 2011 ) 116 : 152162 form was incompletely filled in 40% of cases , and the physicians stamp or signature was missing in 11% ( 55 / 500 ) of total requests , especially those from intrahospital physicians . referti radiologici risposta al quesito diagnostico radiology reports answer to diagnostic question of 362 requests in which the diagnostic question was appropriately and accurately formulated , 22 were not met with any clear and specific answer to the clinical question in the radiologists report . 
these 362 requests were further divided into appropriate requests ( n = 285 ) and appropriate requests with imprecise question ( n = 77 ) to evaluate whether the report effectively identified the condition for which examination had been requested or whether it identified a different condition from that suspected clinically or even the absence of any pathological findings . 
with regard to reports in response to appropriate requests , 28% ( 80 / 285 ) , most of which concerned conventional radiology studies , ruled out the presence of pathological findings ; a large proportion ( 47.5% , 135 / 285 ) confirmed the suspected diagnosis , and the remaining 24.5% ( 70 / 285 ) identified a different condition from that mentioned in the request . 
of the reports responding to the 77 appropriate requests with imprecise question , 36 ( 46.7% ) described conditions at any rate related to the clinical suspicion , 23 ( 30% ) reported a different diagnosis , and 18 ( 23.3% ) excluded the presence of pathology . 
with regard to this group , it should be noted that in terms of the principle of justification and optimisation , the report ruled out the presence of pathology in about one third of requests lacking a diagnostic question . 
 completeness of report apart from the patients demographic data , which were always present , none of the reports made any mention of the clinical information received , or specified , with the exception of cases of dental arch ct ( dental - scan ) , the equipment used and / or the examination technique ( or software reconstructions )  . 
of 47 reports that mentioned previous radiological examinations , more than half reported them incompletely , with no precise reference to the patients radiological history ( date and type of examination )  . 
finally , the majority of reports lacked diagnostic a fronte di 362 richieste in cui il quesito diagnostico stato formulato con criteri di appropriatezza e precisione , in 22 casi il referto del radiologo non ha fornito nessuna chiara e specifica risposta al quesito clinico . 
queste 362 richieste sono state poi ulteriormente suddivise in prescrizioni appropriate ( 285 ) e in prescrizioni appropriate con quesito impreciso ( 77 ) , e in questi due gruppi si voluto valutare se nelle risposte fosse stata effettivamente riscontrata la patologia per la quale lesame era stato richiesto , ovvero segnalati quadri patologici differenti da quelli sospettati clinicamente o , ancora , lassenza di qualsiasi reperto patologico . per quanto riguarda le prescrizioni appropriate , nel 28% dei casi ( 80 / 285 ) , in gran parte relativi ad accertamenti di radiologia tradizionale , lesame ha escluso la presenza di segni patologici , in una buona parte dei casi ( 47 , 5% , 135 / 285 ) stata confermata lipotesi diagnostica e nel rimanente 24 , 5% ( 70 / 285 ) sono state riscontrate patologie differenti da quelle riportate nella richiesta . 
delle restanti 77 richieste appropriate , in cui il quesito diagnostico era per impreciso , in 36 casi ( 46 , 7% ) sono state fornite risposte contenenti descrizioni di patologie comunque attinenti al quadro clinico , in 23 ( 30% ) stata posta una diagnosi differente da quella sospettata ed in 18 ( 23 , 3% ) la risposta radiologica ha escluso patologie in atto . 
 anche nelle richieste valutate come non appropriate ( 138 / 500 , 27 , 6% ) il radiologo ha comunque compilato un referto ; di questo gruppo da sottolineare , in rapporto al principio di giustificazione e ottimizzazione , come in circa 1 / 3 delle richieste senza quesito la risposta abbia escluso la presenza di qualsiasi patologia . completezza del referto a parte i dati anagrafici del paziente , risultati sempre presenti , in nessun referto stata riportata , nemmeno sinteticamente , linformazione clinica ricevuta , n mai stata precisata , ad eccezione dei casi di tc delle arcate dentarie ( dental - scan ) , lapparecchiatura utilizzata per lindagine e / o la tecnica di esecuzione ( unitamente ad eventuali ricostruzioni con software )  . 
da evidenziare come in 37 referti su 75 ( 49 , 3% ) , in cui , a nostro giudizio , sarebbero stati necessari ulteriori approfondimenti diagnostici , questi non sono stati n consigliati n programmati . 
va infine rimarcata , nella gran parte dei referti , lassenza delle conclusioni diagnostiche , riportate infatti solo nel 9 , 8% dei casi ( 49 / 500 ) , quasi tutti esami tc . 158 radiol med ( 2011 ) 116 : 152162 conclusions , which were present in only 9.8% of cases ( 49 / 500 ) , nearly all of which were ct examinations . errori formali formal errors grammatical errors were detected in 12% ( 60 / 500 ) of reports and in particular in reports of ct examinations , presumably due to the need to provide more in - depth and lengthy answers . 
 discussion there is no doubt that diagnostic imaging is undergoing profound changes , with significant organisational and professional implications for the radiologist , who has had to adapt to these rapid changes brought about by technology and market developments . 
a new concept of the healthcare act is emerging , intended as a complex and articulated set of services , skills and knowledge of several professions as a service provided by a healthcare team not through simultaneous interventions but rather through a series of consequential and concurrent actions performed by different professionals and directed towards the same goal . 
only the clinical radiologist will be able to relate on a par with the clinician and take on that central role as envisaged by the existing laws . it is therefore vital that precise , appropriate and universal communication the professionals take place among involved in requesting , interpreting and reporting [ 4 ]  . 
the radiological medical act represents a professional service that , although characterised by a series of integrated procedures with specific diagnostic / interventional aims , counts the request and the report as its fundamental steps , and there are often difficulties and problems in both interpreting the diagnostic question and in writing up the report . 
the most prevalent cause of these difficulties is often a lack of precise methodological indications , resulting in inconsistencies in the type of requests and high variability in the responses [ 5 ]  . the latter , even though generally adequate to allow for a correct diagnostic classification , sometimes appear at risk of ambiguous and nonunivocal interpretation . 
this leads to a possible negative impact on the patients health and a secondary risk of litigation or malpractice charges against the radiologist [ 6 ] , the incidence of which has recently become almost comparable with that in the united states , gli errori grammaticali si sono rilevati nel 12% ( 60 / 500 ) dei referti ed in particolare tra gli esami tc , presumibilmente in relazione alla necessit di risposte pi articolate e prolisse . 
grazie ai sistemi computerizzati , tutte le risposte sono dattiloscritte e in tutti i referti compare il nome del medico radiologo dattiloscritto , con relativa firma / sigla manoscritta . discussione indubbio che la diagnostica per immagini stia vivendo profondi cambiamenti , con significative ripercussioni organizzative e professionali per lo specialista radiologo che si dovuto adattare ai rapidi mutamenti determinati e condizionati dallevolversi della tecnologia e del mercato . 
 emergente una nuova concezione dellatto sanitario , inteso come un insieme complesso ed articolato di prestazioni , competenze e conoscenze di pi professioni , come una prestazione sanitaria di quipe , non nel senso della contestualit degli interventi , ma nel senso di una serie di atti consequenziali e di azioni concorrenti dirette ad un fine unitario e svolte da diverse figure professionali . 
solo il radiologo clinico potr confrontarsi paritariamente con il clinico , assumendo quel ruolo centrale che le normative vigenti gi gli assegnano . fondamentale dunque una precisa ed adeguata modalit di comunicazione universale tra le varie figure professionali che orbitano attorno alla richiesta , alla stesura e allinterpretazione di tale atto [ 4 ] ; esso rappresenta una prestazione professionale che , pur contraddistinta da una serie di procedure operative integrate tra loro , con specifiche finalit diagnostico / interventistiche , riconosce , quali momenti fondamentali , quello della richiesta e del referto , spesso comportanti problematiche e difficolt sia nellinterpretazione dei dati correlati al quesito diagnostico sia nella compilazione della risposta scritta . 
la causa prevalente di tali difficolt spesso identificabile in una carenza di precise indicazioni metodologiche , con conseguente disomogeneit nella tipologia delle richieste e contestuale notevole variabilit nelle risposte [ 5 ] ; questultime , sebbene generalmente idonee a consentire un corretto inquadramento diagnostico , appaiono talora a rischio di ambigua e non univoca interpretazione dei dati , con possibili ripercussioni negative per la salute del paziente e secondari rischi di contenzioso od accuse per malpractice [ 6 ] , la cui incidenza ha assunto , negli ultimi anni , frequenza quasi paragonabile a quella degli stati uniti , dove il numero di denunce secondo solo a quello delle discipline chirurgiche [ 7 ]  . 
 radiol med ( 2011 ) 116 : 152162 where the number of claims in radiology is second only to that of surgical disciplines [ 7 ]  . richieste cliniche radiology requests the first link between the radiological image and the report is the referring physicians clinical question , which must meet the criteria of appropriateness and relevance . 
it should be noted that 110 / 500 requests in our series ( 22% ) completely lacked a clinical question , thus potentially undermining the very foundation of the radiological procedure , given that the diagnostic question is an essential component of the radiology request as provided for by legislative decree no . 
when a referral is not accompanied by a clinical question or the question is clearly insufficient , the radiologist must contact the requesting physician for details or decide not to conduct the investigation because of the lack of essential information about the patients condition . 
alternatively , he or she must personally obtain the patients history and clinical data to appreciate why the radiological investigation is needed in relation to the patients presumed or suspected condition ; provide justification for the investigation ; and deliver the imaging service . in our study , even in the absence of a clinical question , the radiologist nevertheless wrote up a report , presumably after obtaining the patients history and clinical data , a fact that was not recorded . 
whereas the role of the referring physician is clearly important in proposing the investigation to be undertaken , the radiologist remains , for medicolegal purposes as well , the central reference figure in the diagnostic process the one who has the additional task of informing the patient about the examination and obtaining informed consent . in addition to appropriateness , another essential requirement of the request is accuracy of the anamnestic data , with concise and accurate reconstruction of the patients medical history , which helps the radiologist on the basis of his or her expertise to correctly classify the single case and establish the most appropriate investigation according to justification of the proposed examination . 
when describing the patients clinical history , the il primo collegamento fra limmagine radiologica e la sua refertazione rappresentato dal quesito clinico del medico richiedente , che deve rispondere a criteri di pertinenza e soprattutto al concetto di appropriatezza . 
riguardo tale primo momento , va sottolineato come , nella nostra casistica , in 110 / 500 casi ( 22% ) il quesito clinico era del tutto assente , cos da inficiare potenzialmente la base del procedimento diagnostico - radiologico ; il quesito diagnostico infatti uno dei principi indispensabili della richiesta radiologica previsti dal d.lgs. 
nei casi in cui linvio della persona non sia accompagnato da nessun quesito clinico o questo risulti palesemente insufficiente , al radiologo non resta che contattare in prima persona il medico richiedente per precisazioni a riguardo , o scegliere di non procedere a nessun accertamento in carenza delle indispensabili informazioni sulle condizioni del paziente , qualora queste non siano altrimenti acquisibili ; diversamente dovr effettuare lui stesso un adeguato inquadramento clinico - anamnestico , mirato a comprendere le esigenze di indagine radiografica dello stesso , in rapporto alla presunta patologia di base o al semplice sospetto diagnostico , portando a compimento la prestazione e adoperandosi da professionista a giustificarla . nel nostro studio , anche in assenza di quesiti clinici , lo specialista radiologo ha comunque steso un referto , verosimilmente dopo una fase anamnestica ed un inquadramento clinico che comunque non risultano essere stati documentati . 
pur rilevando infatti limportanza del medico prescrivente nella proposta dellesame da effettuare , lo specialista radiologo , anche ai fini medico legali , la figura essenziale di riferimento nel processo diagnostico , con il compito aggiuntivo dellinformazione al paziente circa la tipologia dellesame e lacquisizione del relativo consenso . oltre al fondamentale requisito dellappropriatezza , riteniamo necessario sottolineare limportanza della precisione del dato anamnestico , con sintetica e puntuale ricostruzione della storia clinica del paziente , utile al radiologo , sulla base delle proprie competenze , per inquadrare correttamente il singolo caso clinico , cos da definire la tipologia dindagine pi idonea ai sensi della giustificazione dellesame proposto . 
against the individual detriment that the exposure might cause , taking into account the efficacy , benefits and risks of available alternative techniques having the same objective but involving less exposure to ionizing radiation . 
this concept also applies to medicolegal exposure ( procedures performed for insurance or legal purposes without a clinical indication ) that does not produce a direct health benefit for the person all doses due to medical exposure ... 
taking into account the diagnostic reference levels ( drl ) in accordance with guidelines indicated in annex ii , and particular care shall be taken to keep the dose delivered during medico - legal exposure as low as reasonably achievable... tabella 3 principi di giustificazione e ottimizzazione , secondo il d.lgs. 
ovvero comportano una minor esposizione alle radiazioni ionizzanti , questo concetto vale anche per lesposizione di persone nellambito di procedure medico - legali ( procedimenti effettuati a fini assicurativi o legali , anche senza indicazione clinica ) che non presentano un beneficio diretto per la salute della persona ... 
this fact could hinder communication of correct and complete clinical information , leading not only to possible difficulty in carrying out del caso , ma anche , e soprattutto , in relazione al principio di giustificazione , gi pi volte menzionato . 
it is the step embodying the radiologists exclusive and specific competence , and it has official medicolegal value [ 9 ]  . the written nature of the radiologists interpretation makes the radiology report similar to a medical certificate , especially in terms of essential requirements [ 10 ]  . 
with regard to the medicolegal aspects , these two documents are quite different in their purposes ( the certificate is a statement of technical facts designed to demonstrate their truth and produces legal certainty ; the report is a scientific statement ) and intended readers ( the patient for the certificate ; the referring physician for the radiology report )  . in our study , we found that radiologists had a good reporting ability . 
they were almost always able to correctly answer the clinical question by correctly framing the condition being investigated , despite the fact that some situations are too complex to allow for a univocal interpretation and that findings may be nonspecific and subject to multiple interpretations that need to be considered in the differential diagnosis and can be better defined with further diagnostic investigations . 
in contrast , we found some lack of accuracy in the clinical information provided , in the description of the examination technique ( including equipment specifications and use of contrast medium ) , in the presence of individual physical factors potentially limiting the accuracy of the survey and in the suggestion for further diagnostic investigations . 
in particular , whereas no report contained any description of the clinicalanamnestic data and only a few described the examination technique , very few cases , indeed , contained the conclusions with suggested diagnoses or recommendations for further investigation , all of which are elements that can help improve communication with the referring physician . il referto rappresenta il momento successivo , indispensabile e complementare allesecuzione del supporto radiologico e pu dirsi il vero e proprio atto medico del radiologo . esso infatti linterpretazione ufficiale , finale e scritta , che deve accompagnare tutti gli studi di diagnostica per immagine e che , insieme alliconografia prodotta , ne costituisce il risultato , configurandosi quale momento di esclusiva e specifica competenza dello specialista radiologo , con valore medico - legale ufficiale [ 9 ]  . il carattere di verbalizzazione scritta del referto radiologico accomuna tale documentazione al certificato medico , specie nei requisiti essenziali di compilazione [ 10 ]  . 
sul piano medico legale invece i due elaborati non possono essere sovrapponibili , sia per differente finalit ( il certificato unattestazione di fatti di natura tecnica destinata a provarne la verit , nonch produttiva di una certezza legale ; il referto una dichiarazione di scienza ) , sia per il diverso destinatario ( il paziente per il certificato , il medico prescrivente per il referto radiologico )  . nel nostro studio abbiamo riscontrato una buona capacit di refertazione da parte degli specialisti , quasi sempre in grado di rispondere correttamente al quesito proposto inquadrando la patologia indagata , anche se , data la complessit di talune problematiche , non sempre possibile fornire interpretazioni e risposte univoche ai quesiti clinici , ma piuttosto evidenziare reperti non sempre specifici , soggetti a pi ipotesi , da porsi fra loro in diagnosi differenziale e meglio definibili con eventuali ulteriori accertamenti . 
in contrapposizione emersa , tuttavia , una certa mancanza di precisione nellinformazione clinica ricevuta , nella descrizione della tecnica di esecuzione dellesame ( comprese le precisazioni circa lapparecchiatura utilizzata e leventuale uso di mdc ) , nella presenza di potenziali fattori fisici individuali limitanti laccuratezza dellesame e nella raccomandazione di ulteriori indagini di approfondimento diagnostico . 
in particolare , se in nessun referto era indicato , neppure sinteticamente , il quadro clinico - anamnestico e solo in alcuni era descritta la metodologia dellesame , in pochissimi casi erano segnalate le conclusioni con eventuali indirizzi diagnostici o suggerimenti al curante per ulteriori indagini , tutti elementi utili per una migliore e pi completa comunicazione con il medico richiedente . conclusions our experience has shown a high percentage of errors in writing requests for radiological examinations ( 50% ) ; 22% of requests lacked the clinical question , and 27.6% most of which were from general practitioners were inappropriate . 
the reports were found to be substantially accurate , nella nostra esperienza emersa unelevata percentuale di errori nella formulazione della richiesta di esami radiologici ( 50% circa ) ; 22% di richieste mancanti del quesito clinico e 27 , 6% di richieste inappropriate , provenienti prevalenteconclusioni 162 radiol med ( 2011 ) 116 : 152162 with only 6% not providing a specific response to the clinical question . in conclusion , the high percentage of inappropriate requests and requests lacking a clinical question identified in this study may potentially undermine the effectiveness of the diagnostic process , with negative consequences on proper risk management [ 11 ]  . 
moreover , audits should be promoted to discuss , with the coordination of the radiologist and the participation of general practitioners and hospital physicians , the pitfalls and advantages of each imaging modality in relation to different clinical questions and to optimise the flow of radiology requests . mente da medici di medicina generale . 
nei referti radiologici si evidenziata una sostanziale correttezza ; solo nel 6% non era presente una risposta specifica al quesito clinico . in conclusione , lelevata percentuale di richieste inappropriate e mancanti di quesito clinico emersa in questo studio pu potenzialmente limitare lefficacia del processo diagnostico e comportare ripercussioni negative in termini di corretta gestione del risk - management [ 11 ]  . 
this study evaluated with ultrasonography ( us ) the presence of epiaortic vessel lesions in hiv - positive individuals receiving highly active antiretroviral therapy ( haart ) and compared them with nave patients and healthy individuals to highlight the differences among the different vascular damage patterns . 
a total of 222 hiv - infected patients receiving haart , 64 hiv - infected patients nave to antiretroviral therapy and 135 hiv - negative control patients underwent us of the carotid vessels . 
scopo dello studio stato quello di valutare , mediante ecografia ( us ) , la presenza di lesioni intimali nei vasi epiaortici di pazienti positivi al virus della immunodeficienza umana ( hiv ) trattati mediante terapia antiretrovirale altamente attiva ( haart ) , confrontando i risultati ottenuti con quelli provenienti dallo studio delle carotidi di pazienti hiv + che non ricevevano haart e di individui sani utilizzati come controllo . 
abbiamo studiato con us le carotidi di 222 pazienti hiv - positivi trattati con haart , di 64 hivpositivi nave per la terapia antiretrovirale e di 135 soggetti hiv - negativi , utilizzati come popolazione di controllo . 
abbiamo rilevato lesioni intimali carotidee in misura significativamente maggiore nei pazienti hivpositivi trattati con haart rispetto a quelli che non ricevano haart ( p < 0 , 0000001 ) , e ai controlli ( p < 0 , 0001 )  . 
in cinque soggetti in terapia haart abbiamo radiol med ( 2011 ) 116 : 6170 that were consistent with arteritis rather than with classic atheroma , but the percentage was too small to suggest any robust hypothesis . 
come gi segnalato da altri autori , abbiamo osservato lesioni carotidee compatibili con arterite piuttosto che con il classico ateroma , ma in una percentuale attualmente troppo esigua ( 0 , 02% ) per supportare valide ipotesi diagnostiche . 
ulteriori studi sono necessari per confermare questultimo dato . parole chiave hiv terapia antiretrovirale ateroscelrosi eco - color doppler placche carotidee introduction introduzione the introduction of new and potent drugs in combination regimens , commonly defined as highly active antiretroviral therapy ( haart ) , has significantly changed the natural history of hiv infection , leading to a significant reduction in morbidity and mortality from hiv / aids and related diseases [ 1 ]  . 
however , concern has been raised about their several adverse metabolic side effects , which include dyslipidaemia , lipodystrophy , insulin resistance and premature atherosclerosis [ 2 , 3 ]  . 
various vascular complications have been described in patients subjected to prolonged treatment with protease inhibitors ( pis ) , an important component of haart , prompting the hypothesis that pis can contribute to atherosclerotic damage of the vascular wall . 
indeed , patients treated with pi - based regimens present significantly higher levels of triglycerides and lower levels high - density lipoprotein ( hdl ) cholesterol [ 49 ]  . 
however , the actual role of these drugs in increasing the risk of atherosclerotic lesions of the carotid vessels in hiv - infected patients is still controversial [ 1013 ]  . 
several factors are related to the onset of vascular lesions in hiv - infected patients , including the direct role of the virus in endothelial damage [ 9 , 1315 ] and the immune reconstitution subsequent to haart [ 16 ]  . 
indeed , whereas some carotid lesions identified are consistent with typical atheromatous plaques , others have a different structure , more similar to inflammatory infiltration of the carotid wall , even though it cannot be excluded that they may subsequently evolve towards the classic features of atheroma . 
 con lintroduzione nellultimo decennio di nuovi efficaci farmaci somministrati in combinazione tra loro ( terapia antiretrovirale altamente attiva , haart ) , la storia naturale dellinfezione da virus dellimmunodeficienza umana ( hiv ) si radicalmente modificata . 
lhaart infatti ha ridotto significativamente morbilit e mortalit da hiv / sindrome da immunodeficienza acquisita ( aids ) e delle malattie correlate [ 1 ] , ma al contempo il suo utilizzo ha provocato la comparsa di molteplici effetti collaterali metabolici come la dislipidemia , la lipodistrofia , la resistenza alla insulina e laterosclerosi prematura [ 2 , 3 ]  . 
questo riscontro ha suggerito lipotesi che gli pis possano contribuire al danno aterosclerotico della parete vascolare , anche se i pazienti trattati con pis presentano livelli pi alti di trigliceridi che non di colesterolo highdensity lipoprotein ( hdl ) [ 49 ]  . 
a tuttoggi rimane tuttavia controverso il reale ruolo di questi farmaci nel determinare linsorgenza di lesioni aterosclerotiche nei pazienti hiv positivi [ 1013 ] la cui genesi potrebbe riconoscere molteplici fattori , come il ruolo diretto del virus sullendotelio [ 9 , 1315 ] o la ricostituzione immunitaria successiva alla haart [ 16 ]  . 
infatti , mentre alcune delle lesioni carotidee riscontrate sono compatibili con placche ateromasiche tipiche , altre presentano una struttura diversa , pi simile allinfiltrazione infiammatoria della parete carotidea , anche se non pu essere esclusa una loro successiva evoluzione verso il classico ateroma . 
 colour - doppler us is a well - established , noninvasive method of assessing the presence and degree of epiaorticvessel pathology and can therefore be used to detect onset leco - color doppler metodica non invasiva , affidabile nella valutazione delle patologie dei vasi epiaortici , e pu essere utilizzata nel paziente hiv positivo per rilevare le radiol med ( 2011 ) 116 : 6170 and progression of carotid lesions in hiv individuals . 
the objective of this study was to use us to evaluate the presence of carotid artery lesions in hiv - positive patients receiving or not receiving haart and to verify whether endothelial damage is more consistent with arteritis or with classic atheromatous plaques . 
 lesioni carotidee iniziali e studiare la loro progressione . obbiettivo di questo studio di valutare mediante ecografia ( us ) la presenza di lesioni intimali nei vasi epiaortici dei pazienti hiv positivi , trattati o non trattati con haart , e verificare se le lesioni endoteliali siano riconducibili a placche aterosclerotiche classiche o a lesioni di tipo infiammatorio , simili a quelle identificabili in corso di arterite . 
 materials and methods between december 2004 and february 2008 , 222 hivinfected patients receiving haart , 64 hiv - infected patients nave to antiretroviral therapy and 135 hiv - negative control patients underwent us of the carotid vessels . the local ethics committee approved the study , and all individuals provided informed consent . 
for each patient , we evaluated risk factors for cardiovascular diseases ( angina , myocardial or cerebral infarction ; transitory ischaemic attack ) , including family history , cigarette smoking , active drug abuse , arterial hypertension , hyperglycaemia , hypercholesterolaemia and hypertriglyceridaemia . 
no patients used lipid - lowering drugs . duplex us grading of the carotid arteries was performed in accordance with the principles established by the atherosclerosis risk in communities ( aric ) study [ 18 ] and the previous consensus meeting regarding quantification of extracranial carotid artery stenosis [ 19 ]  . bilateral carotid artery us was performed by the same specifically trained radiologist ( mc ) , with 15 years experience in colour - doppler imaging , on two scanners equipped with high - frequency broadband linear - array transducers . 
the scanners used were an astro ( esaote biomedica , genoa , italy , 69 mhz ) since 2004 and an iu22 ( philips , eindhoven , the netherlands , 517 mhz ) since 2005 . 
in accordance with the literature data [ 7 , 19 ] , we assessed lesions for echogenicity with respect to the vessel wall and homogeneity , presence of calcifications , parietal and endoluminal surface profiles , presence of ulceration and presence of a cleavage plane . 
a materiali e metodi nel periodo compreso tra dicembre 2004 e febbraio 2008 , presso il nostro istituto , abbiamo valutato prospetticamente con us dei vasi epiaortici 222 pazienti hiv positivi trattati con haart , 64 pazienti hiv positivi nave per la terapia antiretrovirale e 135 soggetti hiv negativi , questi ultimi utilizzati come popolazione di controllo . 
per ogni paziente sono stati valutati i fattori di rischio per patologie cardiovascolari ( angina , infarto del miocardio o cerebrale , attacchi ischemici transitori ) : la storia familiare , il fumo , lassunzione di droghe , lipertensione arteriosa , la iperglicemia , la ipercolesterolemia , la ipetrigliceridemia . 
 lo studio ecografico delle carotidi stato eseguito in conformit con i principi stabiliti dallo studio atherosclerosis risk in communities ( aric ) [ 18 ] e dal precedente consensus meeting sulla quantificazione del grado di stenosi dellarteria carotide extracranica [ 19 ]  . 
lesame eco doppler delle carotidi stato eseguito dallo stesso operatore ( mc ) , specialista radiologo con esperienza di 15 anni nella tecnica eco color doppler , utilizzando due apparecchi dotati di sonde lineari ad alta frequenza , dal 2004 un astro 69 mhz ( esaote biomedica , genova , italia ) , e dal 2005 un u22 517 mhz ( philips , eindhoven , olanda )  . 
lesame morfologico stato eseguito bilateralmente , mediante piani assiali e sagittali con tecnica b - mode , color e power doppler al fine di evidenziare meglio le lesioni e limt . stata eseguita una analisi spettrale pulsed - wave doppler a carico delle arterie carotidi comuni ed interne bilateralmente . 
in base ai dati della letteratura [ 7 , 19 ] abbiamo valutato : lecogenicit delle lesioni in confronto alla parete vascolare e la loro radiol med ( 2011 ) 116 : 6170 fig . 
a p value < 0.05 was considered statistically significant . results omogeneit , soprattutto se fossero presenti calcificazioni ; il profilo della superficie endoluminale e parietale , specialmente la presenza di ulcerazioni e di un piano di clivaggio . abbiamo definito come placca un ispessimento della parete carotidea , focale e > 1 mm : aterosclerotica quando si lispessimento era iso - iperecogeno , senza o con calcificazioni , con superficie parietale ed endoluminale irregolare e con piano di clivaggio ; di tipo infiammatorio quando si lispessimento era iso - ipoecogeno , senza piano di clivaggio , con superficie parietale ed endoluminale liscia e regolare o solo lievemente irregolare . 
la superficie della placca stata definita come irregolare quando abbiamo osservato una variazione di altezza tra 0 , 4 e 2 mm lungo il contorno della lesione . le differenze statistiche fra i pazienti sono state valutate con il test del chi - quadro o con il test di fisher per le variabili qualitative . 
the epidemiological characteristics and cardiovascular risk factors of the three groups of individuals ( hiv - infected patients on haart , hivinfected patients without haart , non - hiv - infected individuals ) are shown in table 2 . 
hiv - positive patients were more frequently cigarette smokers in comparison with hiv - negative patients ( p < 0.0001 ) , but no difference risultati la tabella 1 mostra i dati epidemiologici dei pazienti hiv positivi . 
la tabella 2 documenta i dati epidemiologici e i fattori di rischio cardiovascolari nei tre gruppi in esame ( pazienti hiv positivi in trattamento haart , pazienti hiv positivi non sottoposti a haart , pazienti hiv negativi )  . 
hiv - infected patients on haart had a significantly higher prevalence of hypertriglyceridaemia when compared with either hiv - positive patients nave to antiretroviral therapy or hiv - negative individuals . 
in incidenza di fumatori rispetto ai pazienti hiv negativi ( p < 0 , 0001 ) , mentre non si sono rilevate differenze in tal senso fra i pazienti hiv positivi sottoposti ad haart e quelli nave per la terapia antiretrovirale . 
no alterations in pulsation index , resistance index , minimal speed , peak speed and mean speed were observed in the three groups of patients . discussion the widespread diffusion of haart has deeply modified the characteristics and epidemiology of hiv / aids , leading to a prolonged asymptomatic period after infection , prolonged survival after aids diagnosis and changes in the natural history of hiv - related diseases . 
nei tre gruppi di pazienti non sono stati registrati valori anomali di indice di resistenza , di indice di pulsatilit , di velocit di picco sistolica , diastolica o media . 
 discussione lampia diffusione dellhaart ha profondamente modificato le caratteristiche e lepidemiologia dellhiv / aids , determinando un lungo periodo asintomatico dopo linfezione , un lungo periodo di sopravvivenza dopo la diagnosi di aids e modificando la storia naturale delle patologie associate allhiv . 
3 classica placca ateromasica ulcerata nella carotide comune di un paziente hiv - positivo in trattamento con haart . vascular lesions in hiv - infected patients , including the direct role of the virus and immune reconstitution subsequent to haart , and especially changes in lipid and glycidic metabolism induced by haart and , in particular , by pis [ 6 , 25 ]  . 
pis have been thought to promote atherosclerotic lesion formation independently of dyslipidaemia through cholesterol accumulation in macrophages of the arterial wall , [ 26 ] , although some authors observed that the presence of atherosclerotic plaques in femoral and carotid arteries of hiv - infected patients was more closely related to gender , age , cigarette smoking and plasma cholesterol levels than to pi use [ 27 ]  . 
in our study , there was no difference in age , gender and cholesterol level between hiv - positive and hiv - negative patients . regarding cigarette smoking , hiv - positive patients were significantly more frequently smokers than hiv - negative individuals . 
however , in our hiv - positive population , cigarette smoking did not seem to influence the frequency of carotid lesions , and no difference in cigarette smoking was found between hiv - positive patients on haart and hiv - positive patients nave to antiretroviral therapy . 
haarttreated patients showed a higher prevalence of hypertriglyceridaemia in comparison with either haart - nave or hiv - negative patients , even though hypertriglyceridemia is rarely responsible for premature atherosclerosis [ 28 ]  . 
4 lesione di tipo infiammatorio nella carotide comune di un paziente hiv - positivo in trattamento con haart . coronariche e linfarto del miocardio , sono segnalate con frequenza crescente [ 2124 ] , anche se la dimensione reale del problema ancora poco chiara . molteplici fattori sono stati collegati con linstaurarsi di lesioni vascolari in pazienti hiv positivi : il ruolo diretto del virus e della ricostituzione immunitaria a seguito di haart , ma soprattutto i cambiamenti nel metabolismo lipidico e glucidico indotti dallhaart e dagli pis in particolare [ 6 , 25 ]  . 
stato ipotizzato che gli pis possano causare la formazione di lesioni aterosclerotiche provocando un aumento del colesterolo nei macrofagi della parete arteriosa , indipendentemente dalla dislipidemia [ 26 ] , tuttavia alcuni autori hanno osservato che la presenza di placche aterosclerotiche nelle arterie femorali e carotidee dei pazienti hiv positivi correlata rigorosamente con il sesso , let , il tabagismo ed il livello di colesterolo del plasma piuttosto che alluso di pis [ 27 ]  . 
tuttavia , nella nostra popolazione hiv positiva , il tabagismo non sembra influenzare lincidenza delle lesioni carotidee e nessuna differenza nel tabagismo stata riscontrata fra i pazienti hiv positivi in haart ed i pazienti hiv positivi nave per la terapia antiretrovirale . i pazienti trattati con haart hanno mostrato una pi alta prevalenza di ipertrigliceridemia rispetto sia ai pazienti nave per haart che ai pazienti hiv negativi , anche se la ipertrigliceridemia raramente responsabile della aterosclerosi precoce [ 28 ]  . 
nella nostra casistica nei pazienti hiv positivi trattati con haart sono state riscontrate ecograficamente placche aterosclerotiche nel 32 , 9% dei casi versus il 3 , 2% dei pazienti hiv negativi ( p < 0 , 0001 )  . radiol med ( 2011 ) 116 : 6170 vascular disorders affecting small and medium - sized visceral arteries , and the occurrence of vasculopathy has been reported even in large arteries [ 5 , 13 , 29 ]  . 
in these cases , no evidence of atherosclerotic plaques was reported ; the lesions had histological features characterised by proliferation of vascular channels in the adventitia and the presence of a vasculitis of the vasa vasorum , with or without an intimomedial arteritis . 
however , recent studies failed to find a correlation between the classic mediators of atheromatous lesions , such as c - reactive protein and carotid imt in hiv - positive individuals , reinforcing the hypothesis that there could be an alternative pathway for this damage [ 11 , 30 ]  . 
we observed lesions consistent with inflammatory lesions rather than classic atheroma in five patients on haart . the different us patterns between inflammatory and atheromatous lesions are due to the different pathological substrate . 
furthermore , the atheromatous plaque involves only the endothelium and luminal portion of the intima , which accounts for the presence of the cleavage plane between the lesion and the underlying tissues , and its surface is frequently ulcerated . 
further investigations are warranted to better define the structure and mechanisms of onset of these inflammatory - type lesions and clarify the role of the different antiretroviral drugs in the pathogenesis of coronary and systemic atherosclerosis . 
as suggested by some authors [ 14 , 17 ] , vascular damage may develop in two phases : an initial , inflammatory phase probably triggered by haart directly or through immune reconstitution , and a second phase in which the lesions could be maintained by the classic atheromatous risk factors . 
the characteristics of us make it the ideal tool for the periodic study of the carotid vessels , which should , in our experience , be included in the general follow - up of hiv patients , in particular those with pre - existing cardiovascular risk factors , regardless of their antiretroviral therapy status . 
 i pazienti hiv positivi possono mostrare una vasta gamma di vasculopatie che interessano le arterie viscerali piccole e medie e , recentemente , stato segnalato un caso di vasculopatia anche in una grande arteria [ 5 , 13 , 29 ]  . 
nei casi in cui le lesioni non erano di tipo aterosclerotico , istologicamente erano caratterizzate dalla proliferazione di strutture vascolari nellavventizia e dalla presenza di una vasculite dei vasa vasorum , associata o meno ad unarterite dellintima e della media . 
in letteratura non ci sono ancora riscontri che stabiliscono una correlazione fra i classici mediatori delle lesioni ateromasiche , quali la proteina c reattiva e lispessimento di media ed intima nei pazienti hiv positivi , il che rafforza lipotesi che potrebbero esserci altre cause nella patogenesi di queste lesioni [ 11 , 30 ]  . 
in cinque soggetti della nostra casistica in terapia haart abbiamo documentato la presenza di lesioni carotidee di tipo infiammatorio . il differente substrato anatomo - patologico determina i differenti aspetti ecografici delle placche ateromasiche e di quelle tipo infiammatorio . 
laspetto iperecogeno direttamente proporzionale al contenuto fibroso , la disomogeneit alla presenza di lipidi , fibre e calcio , per questo motivo lateroma , generalmente , iperecogeno e disomogeneo . inoltre , la placca ateromasica coinvolge solo lendotelio e la pozione superficiale dellintima , il che si conferma con la presenza di un piano di clivaggio fra le lesione ed i tessuti sottostanti , e la sua superficie frequentemente ulcerata . ulteriori studi saranno necessari sia per meglio definire la struttura e la patogenesi delle lesioni di tipo infiammatorio , sia per chiarire il ruolo dei differanti farmaci antiretrovirali nella patogenesi della aterosclerosi coronarica e sistemica . ad oggi si ritiene che i farmaci antiretrovirali potrebbero svolgere un ruolo chiave nella patogenesi delle lesioni carotidee che lhaart induce . 
alcuni autori hanno ipotizzato [ 14 , 17 ] che il danno vascolare potrebbe svilupparsi in due fasi : la prima , essenzialmente flogistica , innescata dallhaart , direttamente o tramite la ricostituzione immunitaria indotta , la successiva evoluzione delle lesioni potrebbe essere sostenuta dai fattori di rischio ateromasici classici . 
li contributed equally to this study received : 5 january 2010 / accepted : 15 february 2010 / published online : 6 october 2010 springer - verlag 2010 abstract purpose . 
follow - up inferior vena cavagrams demonstrated complete resolution of the chronic ivc thrombi and full ivc patency , without occurrence of pulmonary embolism at any time during the study . 
questo studio stato condotto per valutare la sicurezza e la fattibilit del trattamento trombolitico con urochinasi dopo pre - dilatazione in pazienti con sindrome di budd - chiari ( bcs ) con trombosi cronica della vena cava inferiore ( ivc )  . 
i risultati immediati ed a lungo termine della tecnica procedurale hanno avuto successo in tutti pazienti . le flebografie di follow - up della vena cava inferiore hanno dimostrato una completa risoluzione della trombosi cronica dell ivc e totale pervieta dell ivc , senza alcun caso di embolia polmonare durante lo studio . 
i nostri risultati preliminari indicano che la trombolisi con infusione continua di urochinasi dopo predilatazione un approccio sicuro e fattibile per il trattamento dei pazienti bcs con trombosi cronica dell ivc . keywords budd - chiari syndrome inferior vena cava thrombus thrombolysis parole chiave sindrome di budd - chiari vena cava inferiore trombosi trombolisi radiol med ( 2011 ) 116 : 5660 introduction primary budd - chiari syndrome ( bcs ) is a rare form of hepatic venous outflow obstruction at the suprahepatic inferior vena cava ( ivc ) , the hepatic veins ( hv ) or both , whereas bcs with ivc thrombosis is even rarer , particularly with fresh ivc thrombosis . 
a number of thrombolytic agents , such as acylated streptokinase - plasminogen complex , urokinase , tissue plasminogen activator and streptokinase have been administered either through peripheral intravenous catheters or through ivc or hepatic catheters for successfully dissolving the fresh clots [ 13 ]  . 
prior to the procedures , during which the patients were monitored continuously for vital signs and bleeding complications , inferior vena cavagraphy of the right groin revealed the location and size of the thrombus and the occluded section of the ivc . 
for predilation , a straight 5 - fr catheter with multiple side holes ( cook , inc . , bloomington , in , usa ) was inserted in the ivc and positioned below the occluded segment . 
to prevent rethrombosis , warfarin was administrated orally 5 mg / day from the second day after the procedure for about 36 months . follow - up evaluation the followup investigations , including final clinical evaluation , colour - doppler sonography or inferior vena cavagraphy , were performed 1 week and 1 , 3 , 6 and 12 months posttreatment and then annually thereafter . 
at each visit , procedural technical , angiographic and ultrasonic outcomes , as well as mortality , morbidity and the final clinical outcome , were evaluated . results primary procedural results predilation and urokinase thrombolysis were technically successful in all patients , without occurrence of any procedure - related complications such as acute pulmonary embolisation . 
 discussion membranous obstruction of the ivc or hv or both is the most common cause of bcs in asia and accounts for up to 6070% of the total number of patients [ 58 ]  . 
due to obstruction of the proximal ivc , the blood flow is slow , turbulent or reverse , which leads , together with the hypercoagulable blood state , to formation of thrombi in these patients . 
mostly , ivc in bcs patients presenting in our hospital is already chronic , since disease onset is often asymptomatic , and thus the onset time is often difficult to indicate . 
 thrombosis current medication or procedures to treat ivc thrombosis include thrombolytic agents [ 1 ] , transjugular intrahepatic portosystemic shunts [ 911 ] , surgical shunts [ 12 ] , balloon angioplasty and metallic stents [ 2 , 3 ] or retrieval stent filtres [ 4 ]  . 
thus , our hypothesis was that local continuous infusion of thrombolytic agents may be beneficial in treating bcs patients with chronic ivc thrombosis after restoring the blood flow in the obstructed ivc by interventional procedures . 
therefore , we attempted a relatively simple thrombolytic approach for our bcs patients by infusing urokinase after predilation of the ivc . acute pulmonary embolisation represents a potential risk after predilation and thrombolysis with urokinase ; however , none of the patients in this study experienced this symptom radiol med ( 2011 ) 116 : 5660 fig . 
1a - i a 55 - year - old man with a 10 - year history of budd - chiari syndrome ( bcs ) , with varices in the thoracicoabdominal region and the legs , as well as hepatomegaly , splenomegaly and pigmentation . 
a colour - doppler sonography exhibits a chronic thrombus in the inferior vena cava ( ivc ) ( arrow ) , with ivc occlusion ( arrowhead ) ; b sagittal - plane multiplanar reconstruction ct image of the ivc showed a low - density ivc thrombus with irregular margins ( arrow ) ; c inferior vena cavagram reveals an irregular chronic thrombus in the left ivc wall ( arrow ) ; d anteroposterior fluoroscopy shows dilation of the occluded ivc by a 16 - mm balloon dilator ( arrow ) after rupture of the membrane ; e inferior vena cavagram displays partial patency of the ivc after predilation . 
1a - i un uomo di 55 anni con una storia di sindrome di budd - chiari da 10 anni ( bcs ) , con varici in regione toracoaddominale e alle gambe , epatomegalia , splenomegalia e pigmentazione . 
a lecografia color doppler ha mostrato trombosi cronica della vena cava inferiore ( ivc ) ( freccia ) , con occlusione dell ivc ; b le immagini di ricostruzione tc multiplanare dell ivc sul piano sagittale , hanno mostrato bassa densit della trombosi dell ivc con margini irregolari ; c la flebografia della vena cava inferiore rivela un irregolare trombosi cronica nella parete sinistra dell ivc ( freccia ) ; d la fluoroscopia antero - posteriore mostra dilatazione dellocclusione dellivc con un dilatatore a palloncino di 16 mm ( freccia ) , dopo la rottura della membrana ; e la flebografia illustra la perviet parziale della vena cava inferiore dopo pre - dilatazione ; f l ecografia color doppler evidenzia una parziale perviet dell ivc con stenosi della membrana allorifizio dellatrio destro e una trombosi cronica dell ivc ( freccia ) ; g la flebografia mostra una perviet parziale dell ivc che priva di trombi a 12 giorni dalla trombolisi ; h la flebografia sottolinea lassenza di trombo in corrispondenza dellivc dopo dilatazione con dilatatore a palloncino di 30mm ; i l ecografia color doppler mostra una perviet da trombi dellivc ad un mese dalla trombolisi . 
the success of our approach may be attributable to the following : ( 1 ) the chronic thrombus was incorporated in the ivc wall and would not easily fall off ; ( 2 ) the fresh thrombus was treated with continuous infusion of urokinase for 30 min at the beginning of thrombolysis ; ( 3 ) predilation of the obstructed ivc with a small dilator ( 1216 mm in diameter ) allowed sufficient blood flow through the occluded ivc to prevent the large thrombus from migrating through the occluded ivc . 
however , this approach is not appropriate for patients with segmental obstruction of the ivc or huge thrombi completely obstructing the ivc . normally , chronic thrombi in occluded ivcs are difficult to dissolve , but dissolving them in dilated ivcs with the help of continuous urokinase infusion has proven successful in our patients . 
the former contains mainly erythrocytes and less leucocytes , platelets and fibr therefore , these thrombi are being formed more loosely and can be dissolved more easily and gradually , for instance , by increasing blood flow in the dilated ivc and by then infusing urokinase for about 730 days . 
also , use of a 30 - mm balloon dilator includes the risk of ivc wall rupture ; thus , the device must be used correctly and with great caution according to the instructions of the manufacturer . in conclusion , our preliminary results indicate that thrombolysis with urokinase after ivc predilation may be a safe and feasible approach for treating bcs patients with chronic ivc the results are thrombosis . 
passariello1 1dipartimento di scienze radiologiche , 2dipartimento di scienze cardiovascolari e respiratorie , sapienza universit di roma , policlinico umberto i , v.le regina elena 324 , 00161 roma , italy 3cardiovascular magnetic resonance unit , royal brompton hospital , imperial college , national heart and lung institute , london , uk correspondence to : m . 
in ischaemic heart disease , t2w - stir represents the technique of choice for detecting oedema in patients with acute myocardial infarction ( mi ) , allowing discrimination of acute and chronic injuries . 
myocardial haemorrhage may also be depicted as a region of signal abnormality characterised by a central hypointense core with a peripheral hyperintense rim , presumably reflecting the presence of intracellular methaemoglobin within the necrotic area . 
in the acute setting , elevated t2 relaxation times in association with regional contractile dysfunction but no signs of delayed enhancement may also signify a reversible ischaemic injury without necrosis . 
in acute myocarditis , the distribution pattern of t2w hyperintensity may be focal in approximately 30% of patients or diffuse in the remaining 70% , and myocardial oedema may be the only marker of disease . 
t2w - stir riassunto in risonanza magnetica cardiaca , le sequenze short tau inversion recovery ( stir ) pesate in t2 rappresentano la tecnica ideale per lidentificazione delledema tissutale grazie allapplicazione di un triplo impulso di presaturazione che consente di combinare la soppressione del segnale dei fluidi in movimento e del tessuto adiposo . scopo di questa pictorial review di illustrare lutilit clinica e lo spettro applicazioni di questa sequenza nella patologia cardiaca ischemica e non ischemica . 
nella cardiopatia ischemica , ledema tissutale rappresenta un marker di danno miocardico acuto e definisce larea di miocardio a rischio che contiene sia tessuto necrotico che segmenti miocardici non contrattili ma vitali . 
lemorragia rappresenta invece la conseguenza della terapia riperfusiva con stravaso di eritrociti nellinterstizio e pu essere identificata in stir t2 come unalterazione caratterizzata da un core centrale ipointenso , che riflette la presenza di metaemoglobina nel contesto dellarea di necrosi . 
ledema tissutale pu essere inoltre osservato in numerose altre cardiopatie non ischemiche , come varie cardiomiopatie primitive e secondarie , pericarditi acute , lipertensione polmonare ed il rigetto di trapianto cardiaco . 
in aggiunta alle tradizionali sequenze radiol med ( 2011 ) 116 : 3246 represents an appealing and versatile technique that can be applied in a wide variety of ischaemic and non - ischaemic conditions , allowing detection of segmental or global increase of myocardial free water content , reflecting an acute myocardial injury . 
 keywords t2w - stir myocardial oedema myocardial infarction myocarditis hypertrophic cardiomyopathy tako - tsubo syndrome pericarditis heart transplantation morfo - funzionali , le sequenze stir t2 costituiscono uninteressante e versatile tecnica di imaging che pu trovare applicazione in una vasta gamma di cardiopatie ischemiche e non , consentendo di identificare un incremento focale o diffuso del contenuto di acqua libera intramiocardica e fornendo molto spesso informazioni di rilevante impatto clinico . parole chiave stir t2 pesate edema miocardico infarto del miocardio miocardite cardiomiopatia ipertrofica sindrome di tako - tsubo pericardite acuta trapianto di cuore introduction introduzione use of t2 - weighted imaging for assessing acutely injured myocardium was initially proposed by higgins et al . 
 [ 1 ] , who described the presence of a linear correlation between t2 - relaxation time and percentage of myocardial free water content in an animal model , allowing depiction of infarcted tissues as areas of increased signal . 
myocardial oedema does not necessarily reflect necrosis and represents a nonspecific marker of acute inflammatory response in numerous other nonischaemic clinical settings , such as tumours , primary cardiomyopathies ( cmp ) , storage disease , cardiac transplant rejection , pulmonary hypertension and acute myocarditis [ 2 , 3 ]  . 
the best imaging approach for oedema - weighted cardiac magnetic resonance imaging ( mri ) is segmented fast spin - echo using a triple inversion recovery preparation module ( t2w - stir ) , which allows signal suppression from flowing blood and from fat [ 2 ]  . 
 [ 1 ] hanno per primi descritto , su modello animale , la presenza di una correlazione lineare tra tempo di rilassamento t2 e quota di acqua libera intramiocardica , identificando la necrosi miocardica acuta come unarea di focale incremento del segnale in t2 dovuta alla presenza di edema tissutale [ 1 ]  . ledema miocardico non necessariamente riflette la presenza di necrosi e rappresenta il segno di una risposta infiammatoria aspecifica del tessuto miocardico e pericardico riscontrabile in numerose cardiopatie di tipo nonischemico , dalle malattia infiammatorie ( miocarditi e pericarditi ) , alla patologia neoplastica , malattie autoimmuni e rigetto dorgano nei trapianti , cardiomiopatie primitive e secondarie ( soprattutto malattie da accumulo ) [ 2 , 3 ]  . 
lo stato dellarte dellimaging pesato in t2 o edema - weighted in rmc si basa sullutilizzo di una tecnica fast spin - echo inversion recovery ( short tau inversion recovery , stir ) , con applicazione di un triplo impulso di presaturazione che consente di combinare la soppressione del segnale dei fluidi in movimento e del tessuto adiposo [ 2 ]  . 
 scopo di questa pictorial review di illustrare lutilit clinica e lo spettro applicazioni di questa sequenza in una variet di condizioni ischemiche e non - ischemiche . design della sequenza la stir t2 una sequenza spin - echo inversion - recovery a sangue nero ( black - blood ) , in cui vengono applicati due impulsi di preparazione ( rispettivamente non - selettivo e selettivo ) a 180 , seguiti da un lungo tempo di inversione ; la soppressione del tessuto adiposo viene successivamente ottenuta con un terzo impulso di presaturazione a tempo di inversione ( ti ) breve e selettivo per il grasso . 
the underlying pathophysiological mechanism leading to accumulation of water within the intraand extracellular spaces of necrotic regions seems to be related to the presence of osmotically active substances and disruption of the adenosine triphosphatase ( atp ) - regulated ionic transport mechanisms across the cell membrane in the acute phase after necrosis [ 5 ]  . 
in the acute phase of mi , regional hyperintensity on t2w - stir is usually larger than true infarct size compared with histology or delayed - enhancement ( de ) imaging measurements [ 6 , 7 ]  . 
 una volta annullata la magnetizzazione del sangue , viene applicato un terzo impulso a 180 , con ti breve per annullare selettivamente il segnale proveniente dal tessuto adiposo ( impulso stir ) , amplificando le differenze di segnale tra tessuti con t1 lungo ( come per esempio il miocardio edematoso ) e tessuti con t1 breve ( come il grasso ) ; il ti di circa 120 ms quando si utilizzano magneti a 1 , 5 t . 
dal punto di vista fisiopatologico , ledema miocardico nellinfarto acuto sia di tipo interstiziale sia intracellulare rispettivamente per accumulo di sostanze osmoticamente attive nellinterstizio che richiamano liquidi dal microcircolo e per la deregolazione delle pompe sodio - potassio atp - mediate con perdita di funzione di membrana dei miociti [ 5 ]  . 
on t2 - weighted short - tau inversion recovery ( a ) , tissue oedema is depicted as a homogeneous transmural area of hyperintense signal located in the inferior and inferoseptal left - ventricular wall ( arrow )  . 
nelle sequenze stir t2 pesate ( a ) , ledema tissutale viene identificato come una zona di omogenea iperintensit del segnale ad estensione transmurale , localizzata a livello della parete inferiore ed infero - settale del ventricolo sinistro ( freccia )  . 
nella stessa sede , le sequenze inversion recovery contrast enhanced ( ir - ce ) mostrano una circoscritta area di potenziamento patologico ad estensione non trans murale ( b )  . 
clearly demonstrated the relationship between t2w abnormality and the area of myocardium at risk using an animal model in which cardiac mri data were compared with histology and the ischaemic region was demarcated by injecting fluorescent microspheres at the time of the induced coronary occlusion [ 8 ]  . 
thus , t2w abnormality in acute mi defines the area at risk at the time of the ischaemic insult , which includes zones of reversibly and irreversibly injured myocardium [ 79 ]  . 
lestensione dellarea edematosa quantificata con stir t2 costantemente maggiore sia rispetto ai rilievi istopatologici che alle misurazioni effettuate con tecnica di delayed enhancement ( de ) in rmc [ 6 , 7 ]  . 
 [ 6 ] hanno ipotizzato come questa differenza tra segmenti iperintensi in stir t2 e segmenti con de potrebbe riflettere la presenza della cosiddetta area perinfartuale contenente segmenti miocardici disfunzionanti radiol med ( 2011 ) 116 : 3246 fig . 
3a , b double acute and chronic mi in a 62 - year - old man in whom a combined approach of t2w - stir ( a ) and ce - ir magnetic resonance image ( b ) allows differentiation an old anterior mi from an area of recent necrosis ( day 5 ) located in the inferoseptal left - ventricular ( lv ) wall and extending to the inferior right ventricular ( rv ) wall . 
chronically infarcted region exhibits lower signal intensity on t2w imaging ( a ) ( arrowheads ) compared with normal adjacent segments , presumably because of the lower free water content of the fibrous scar . 
in questo paziente stato utilizzato un approccio combinato utilizzando sequenze stir t2 pesate ( a ) ed ir - ce ( b ) , per differenziare un pregresso infarto anteriore rispetto ad unarea di necrosi recente ( 5 giorno ) , localizzata in sede infero - settale del ventricolo sinistro e con estensione alla parete inferiore del ventricolo destro . 
nella sede del pregresso infarto , la cicatrice presenta bassa intensit del segnale nelle sequenze t2 pesate ( a ) ( punta di freccia ) , se confrontata con i segmenti contigui , verosimilmente per il minore contenuto di acqua libera nel contesto della cicatrice fibrosa . 
in stir t2 inoltre osservabile lestensione delledema a livello della parete inferiore del ventricolo destro , elemento che ne suggerisce il coinvolgimento , poi confermato dalle immagini in asse corto ir - ce ( b ) ( freccia )  . revascularisation are minimal compared with the extent of reperfusion - related damage [ 1012 ]  . myocardial oedema also represents a promising target of early reperfusion of a thrombotic occlusion preceding the onset of myocardial necrosis in the ischaemic cascade . 
in the acute setting , therefore , elevated t2 relaxation times in association with regional contractile dysfunction but no signs of de might signify a reversible ischaemic injury without tissue necrosis , resulting in an aborted mi , a term first used by gename et al . 
 myocardial haemorrhage is a reperfusion - related injury with severe microvascular damage caused by extravasation of erythrocytes into the interstitium during the reflow period caused by disruption of capillary integrity . 
 [ 14 , 15 ] recently demonstrated with cardiac mri the importance of haemorrhage as an independent and strong predictor of left - ventricular ( lv ) remodelling at short - term follow - up , regardless of the initial infarct size . ma vitali , che possono beneficiare con successo della rivascolarizzazione [ 6 ]  . 
 [ 8 ] hanno ulteriormente chiarito tali osservazioni dimostrando su modello animale la stretta correlazione tra larea di segnale iperintenso in stir t2 e lestensione istopatologica dellarea a rischio utilizzando una tecnica di immunofluorescenza con iniezione intracoronarica di microsfere al momento dellinduzione dellocclusione del vaso [ 8 ]  . 
in tal senso , il concetto fondamentale che le sequenze stir t2 , definiscono ed identificano non tanto lestensione della necrosi quanto larea di tessuto miocardico a rischio interessato dallinsulto ischemico e che comprende sia i segmenti non contrattili ma vitali ( miocardio stordito ) , che quelli danneggiati irreversibilmente ( miocardio necrotico ) [ 79 ]  . 
4a - e haemorrhagic myocardial infarction due to iatrogenic dissection of a first marginal branch of the left circumflex artery during selective coronary angiography . intramyocardial haemorrhage is characterised on t2w - stir ( a , b ) by a central hypointense core with a peripheral hyperintense rim located within the lateral left ventricular wall . regional t2 relaxation time shortening is most likely related to the presence of intracellular methaemoglobin due to haemorrhage and infarct resorption . 
lemorragia intramiocardica caratterizzata nelle sequenze stir t2 ( a , b ) da un core centrale ipointenso , circondato da unarea periferica ad elevate intensit del segnale localizzata nel contesto della parete laterale del ventricolo sinistro ; laccorciamento del tempo di rilassamento t2 verosimilmente legato alla presenza di metaemoglobina intracellulare , secondaria allemorragia ed al rimodellamento infartuale . 
 myocarditis interstitial myocardial oedema is part of the inflammatory response in acute myocarditis , and its presence has been miocardica conseguenza del danno da riperfusione ed espressione dei fenomeni flogistici contestuali alla necrosi con perdita di integrit dellendotelio e distruzione delle arteriole e dei capillari , e conseguente stravaso di eritrociti radiol med ( 2011 ) 116 : 3246 fig . 
in questo paziente di 57 anni , riperfuso tempestivamente su discendente anteriore dopo linsorgenza dei sintomi ( 60 minuti ) , le sequenze stir t2 pesate acquisite in asse corto mostrano imbibizione edematosa della parete antero - settale in sede medioventricolare ( a ) , in assenza di segni di potenziamento nelle immagini ir - ce ( b )  . 
in the diffuse pattern , its presence may be better detected by comparing myocardial signal intensity with that of surrounding normal skeletal muscle in order to obtain an absolute estimate of signal increase ( t2w signal intensity ratio ) [ 3 , 17 ]  . 
 interestingly , it has been shown that in contrast to acute mi , the extent of t2w hyperintensity in myocarditis is very often smaller than de , with lack of correlation between volume of oedema and tissue fibrosis [ 16 ]  . 
furthermore , the t2w abnormality is not always associated with the presence of de , and depending on different stages of disease , oedema or de may be detected separately . 
these observed differences between t2w - stir and de abnormalities in acute mi and myocarditis may be an indirect sign of the different pathophysiological mechanisms underlying processes [ 16 , 17 ]  . 
 [ 13 ] hanno recentemente dimostrato come lemorragia si associ in genere ad una maggiore evidenza dei fenomeni di rimodellamento ventricolare positivo a breve - medio termine , indipendentemente dallestensione iniziale dellinfarto , con prognosi sfavorevole per i pazienti . un ulteriore pattern recentemente descritto e rilevabile in pazienti con ima o sindrome coronarica acuta riperfusi precocemente caratterizzato dalla presenza di edema parietale in stir t2 senza segni di de dopo somministrazione di mezzo di contrasto ( mdc )  . 
tale quadro rappresenta la manifestazione morfologica di un evento ischemico acuto con rivascolarizzazione coronarica precoce prima che si sia manifestato danno tissutale e definisce il cosiddetto aborted myocardial infarction o infarto abortito , termine utilizzato per la prima volta da weaver et al . 
come gi detto per lima , il valore aggiunto fornito dallimaging edema - weighted nelle miocarditi consiste nella possibilit di distinguere i pazienti che hanno radiol med ( 2011 ) 116 : 3246 fig . 
6a - c miocardite focale in un uomo di 21 anni , che si presenta alla nostra osservazione con febbre , doloro toracico acuto e lieve aumento dei livelli di troponina . 
al follow - up a 3 mesi , ledema miocardico completamente risolto ( c )  . primary cardiomyopathies as for ischaemic and inflammatory disease , t2w imaging has been proposed in previous reports in different cardiomyopathies ( cmp ) [ 3 ]  . 
showed that t2w hyperintensity usually matches location and distribution of late - enhancement areas in cmp and hypothesised that this phenomenon could be related to focal oedema accompanying ischaemia and / or inflammation or to different genotypes of the disease or to characteristics of collagen accumulated within the interstitium [ 20 ]  . 
in tako - tsubo cmp , the main hallmark of disease is characterised by a transitory ischaemia with completely reversible regional contractile dysfunction , most frequently involving apical segments with no angiographic signs of coronary artery disease [ 21 ]  . 
the name attributed to this entity relies on the shape of the lv , which appears as the bottle with a round bottom and a narrow neck used for trapping octopus . 
in this entity , t2w - stir could be useful un processo infiammatorio in atto da quelli che presentano forme croniche ; le sequenze t2 pesate offrono inoltre informazioni complementari alla tecnica di delayet enhancement ( de ) per la loro migliore correlazione con i markers biochimici della flogosi e quindi con lo stato di attivit della malattia [ 17 ]  . 
 a differenza dellinfarto acuto , stato inoltre dimostrato come lestensione dellarea di iperintensit del segnale nelle sequenze t2 pesate sia molto spesso inferiore rispetto alla zona di de , e non esista alcuna correlazione tra volume di edema e quota di tessuto fibroso [ 16 ]  . 
le sequenze stir t2 pesate acquisite in 4 camere mostrano una diffusa imbibizione edematosa del miocardio , che coinvolge i segmenti medio - apicali ( t2w ratio 2 , 8 )  . 
previous studies have shown focal infiltrates depicted on t2w images as zones of intramural increased three different from oedema , stages : neamente in pazienti con miocardite acuta come avviene ad esempio nellima ma rappresentano diversi stadi del processo flogistico ( ledema in genere precede la fibrosi ) e non raramente vengono rilevati isolatamente [ 16 , 17 ]  . 
 cardiomiopatie primitive oltre che per la valutazione delle patologie ischemiche ed infiammatorie , le sequenze stir t2 possono essere utilizzate anche in pazienti con cardiomiopatie primitive ( cmp ) [ 3 ]  . nella cmp ipertrofica , ledema potrebbe essere correlato alla presenza di caratteristiche aree di ischemia miocardica radiol med ( 2011 ) 116 : 3246 fig . 
t2w - stir images in the short - axis ( a ) and horizontal long - axis ( b ) planes show severe concentric left - ventricular symmetric hypertrophy of both cardiac chambers , with patchy areas of high signal intensity consistent with the presence of tissue oedema . 
le immagini stir t2 in asse corto ( a ) ed asse lungo orizzontale ( b ) mostrano una severa ipertrofia simmetrica e concentrica del ventricolo sinistro , con alcune aree ad elevata intensit del segnale e a distribuzione irregolare , compatibili con fenomeni di edema . 
le sequenze ir - ce dimostrano un tipico pattern , caratterizzato da multiple aree di potenziamento a distribuzione irregolare , dovuta al disarray delle fibre muscolari . signal intensity reflecting the oedema associated with inflammation [ 3 , 19 ]  . 
 [ 20 ] hanno dimostrato lesistenza di una stretta correlazione in rmc tra i segmenti di edema e di le , ipotizzando come lalterazione del segnale in stir t2 possa essere espressione di deposizione di matrice collagene ad elevato contenuto di acqua nellinterstizio o in alternativa dipendere dalledema che si associa ad eventi ischemici o forme di miocardite focale tipiche di questa cmp [ 20 ]  . 
9a - c tako - tsubo cardiomyopathy in a 49 - year - old woman with atypical chest pain , ischaemic electrocardiographic changes ( st - elevation < 2mm ) and mildly elevated troponin levels . 
end - systolic cine ssfp image on the vertical long axis shows the typical appearance of the apical ballooning phenomenon characterised by apical dyskinesis and basal hyperkinesis ( ejection fraction 41% in the acute phase ) ( a )  . 
9a - c cardiomiopatia di tako - tsubo in una donna di 49 anni , con dolore toracico atipico alterazioni elettrocardiografiche compatibili con patologia ischemica ( sovraslivellamento st < 2 mm ) e lieve incremento dei valori di troponina . 
le sequenze cine - ssfp acquisite in asse lungo in fase tele diastolica mostrano il tipico aspetto dellapical ballooning , caratterizzato da discinesia apicale ed ipercinesia basale ( frazione di eiezione 41% in fase acuta ) ( a )  . le sequenze stir t2 pesate acquisite in asse lungo evidenziano unarea di omogenea iperintensit del segnale coinvolgente i segmenti medio - apicali ( b )  . le immagini di ce - ir acquisite secondo gli stessi piani anatomici non evidenziano segni di potenziamento patologico miocardico . 
durante il follow - up ( immagini non mostrate ) , si riscontrato un buon recupero della funzionalit cardiaca ( fe 64% ) , con completa regressione delledema tissutale . myocardial oedema has been identified in experimental models correlating lv dysfunction with distribution of interstitial water . 
hypothesised that hypertension may affect fluid balance by both increasing filtration and decreasing lymph flow due to impaired lv venous drainage into the coronary sinus caused by increased rightventricle filling pressures [ 25 ]  . 
lipotesi pi probabile per spiegare la presenza di edema interstiziale pu essere legata alla ipersecrezione catecolaminica che si associa al tako - tsubo con edema vasogenico secondario . cardiomiopatie secondarie : sarcoidosi e amiloidosi dal punto di vista fisiopatologico , la sarcoidosi coinvolge il miocardio con pattern di distribuzione focale o diffuso , progredendo attraverso tre stadi , dalledema alla granulomatosi non caseosa fino alla fibrosi . 
inoltre evidente una focale area di potenziamento mesocardico a livello della giunzione interventricolare posteriore ( freccia )  . heart - transplant disease noninvasive detection of acute heart transplant rejection represents a serious clinical challenge , with endomyocardial biopsy remaining the preferred approach for early detection of acute rejection before allograft dysfunction [ 27 ]  . 
myocardial oedema may be an early indicator of acute organ rejection , probably due to an increase in water content caused by oedema and congestion , but it may also be related to the presence of focal haemorrhage and myocyte necrosis [ 27 , descritto aree focali di infiltrazione , visualizzate nelle sequenze t2 pesate come zone di incrementata intensit del segnale ad estensione transmurale , per la presenza di fenomeni edemigeni associati alla flogosi [ 3 , 19 ]  . 
nellamiloidosi cardiaca , ledema stato descritto sia in numerosi lavori di patologia che in studi effettuati con rmc e sembra essere correlato allaccumulo interstiziale di matrice amiloide con richiamo osmotico di fluidi [ 24 ]  . ipertensione polmonare nei pazienti con ipertensione polmonare primitiva o secondaria , ledema miocardico stato identificato attraverso modelli sperimentali che hanno permesso di correlare il grado di disfunzione del ventricolo sinistro ( vs ) con laccumulo di acqua nella matrice interstiziale . 
 [ 25 ] hanno ipotizzato che laumentata pressione nel circolo polmonare pu alterare lequilibrio degli scambi fluidi , incrementando i meccanismi di filtrazione e riducendo il flusso linfatico , a causa dellincompleto ritorno venoso a livello del seno coronarico e delle aumentate pressioni di riempimento del cuore destro [ 25 ]  . 
value of t2w imaging in this field of cardiac mri was emphasised in a previous paper by marie et al . , who found that t2w mri was a sensitive technique for detecting biopsy - proven acute rejections [ 27 ]  . sequenze stir t2 stato sottolineato in uno studio realizzato da marie et al . 
 [ 27 ] , che hanno mostrato con correlazione istologica come questa tecnica abbia elevata sensibilit nellidentificare fenomeni di rigetto acuto . conclusions conclusioni t2 - weighted stir represents an appealing and versatile technique that can be applied in a wide variety of ischaemic and nonischaemic conditions , allowing detection of segmental or global increase of myocardial free water content with high contrast difference between oedele sequenze stir t2 costituiscono uninteressante e versatile tecnica di imaging che pu trovare applicazione in una vasta gamma di patologie ischemiche e non , consentendo di identificare un incremento focale o diffuso del contenuto di acqua libera allinterno del miocardio , con elevata differenza di radiol med ( 2011 ) 116 : 3246 matous myocardium and surrounding tissues . 
raffaele dimiccoli , via ippocrate , 70051 barletta , italy 3department of radiology , scientific institute hospital casa sollievo della sofferenza , viale cappuccini 1 , 71013 san giovanni rotondo , italy correspondence to : s . 
between november 2007 and may 2008 , we performed shoulder mr examinations for shoulder pain or disability on 94 patients ( 46 males , 48 females ; age range 1679 years ; mean age 54.0915.09 years ) for a total of 104 shoulders ( 62 right , 42 left )  . 
rc was more easily detectable in oblique coronal scans where it appeared as a crescent - shaped , regularly marginated structure adjacent to the articular surface of the supraspinatus tendon and medial to the insertion point of this tendon on the greater tuberosity . 
il rc pi agevolmente individuabile nelle scansioni coronali - oblique ove appare come una struttura a forma di semiluna , con margini regolari , adiacente alla superficie articolare del tendine sopraspinato , medialmente al punto dinserzione di questo tendine sulla grande tuberosit . 
in our sample it did not seem to influence shoulder function in patients with cuff lesions . keywords magnetic resonance imaging shoulder rotator cable shoulder pain disability riguardava let tra pazienti con o senza evidenza di rc ( test t di student = 0 , 05 ; p = 0 , 82 )  . 
nel nostro campione di studio esso non sembra influenzare la funzionalit della spalla in pazienti con lesioni di cuffia . parole chiave risonanza magnetica spalla rotator cable dolore di spalla limitazione funzionale introduction introduzione tendon lesions of the rotator cuff are the most frequent cause of shoulder pa the incidence of full - thickness rotator cuff lesions ranges from 18% to 26% . 
this fibrotic structure arises from the coracohumeral ligament , with fibres that are perpendicular to the axis of the supraspinatus tendon , and arches anteriorly and posteriorly to attach onto the humerus [ 35 ]  . 
the latter is a thin sheet of the distal supraspinatus and infraspinatus tendon that is bound proximally by the rc and that corresponds to the [ 6 ] and codman and akerson [ 7 ] , in which cuff lesions occur most frequently . 
burkhart [ 2 ] considered the rc to be a functional system in which there is stress transfer from the rotator cuff to the thick cable and stress shielding of the thin capsular tissue distal to the cable , thus allowing the individual with a cuff lesion to preserve normal shoulder function . 
the aim of our study was to evaluate the rc with magnetic resonance ( mr ) imaging and to investigate its possible role in the biomechanics of the shoulder affected by cuff lesions . zone described by codman critical le lesioni della cuffia dei rotatori sono la causa pi frequente di dolore alla spalla . 
questa struttura fibrotica origina dal legamento coraco - omerale , con fibre perpendicolari allasse maggiore del tendine del sovraspinoso , e si inserisce sullomero con decorso arcuato [ 35 ]  . 
questultimo costituito da un sottile strato delle fibre di inserzione dei tendini sopraspinato e infraspinato , ed prossimamente in continuit con il rc . esso , inoltre , corrisponde alla critical zone descritta da codman [ 6 , 7 ] , in cui si verificherebbero pi frequentemente le lesioni di cuffia . 
burkhart [ 2 ] ha ipotizzato che il rc agisca come un sistema funzionale in cui si ha un trasferimento delle forze tensive dalla cuffia dei rotatori al cable che proteggerebbe il sottile tessuto capsulare situato distalmente al cable consentendo ai soggetti con lesioni di cuffia di conservare la normale funzionalit della spalla . 
secondo gli stessi autori [ 2 , 3 ] il rc tenderebbe ad ispessirsi con lavanzare dellet e ci lo renderebbe pi facilmente identificabile nei soggetti con et superiore ai 65 anni . 
lo scopo del nostro studio stato valutare il rc con la rm e definire il suo possibile ruolo nella biomeccanica della spalla in pazienti con lesione della cuffia dei rotatori . 104 radiol med ( 2011 ) 116 : 102113 fig . 
1 , tendine del sovraspinato ; 2 , rc ; 3 , testa omerale ; 4 , rotator crescent . materials and methods materiali e metodi our study comprised a morphological and a functional phase . abbiamo organizzato il nostro studio in due fasi : una fase morfologica ed una funzionale . morphological phase fase morfologica in this phase , we evaluated the mr appearance of the rc . we studied the morphological features of the structure attempting to establish in which sequences and sections the structure was more easily recognisable . 
moreover , in view of previous reports [ 3 ] of better evidence of the rc in elderly individuals ( > 65 years ) , we investigated whether this result was also confirmed in our sample . in questa fase abbiamo valutato laspetto rm del rc . abbiamo studiato le caratteristiche morfologiche della struttura cercando di individuare le sequenze ed i piani di scansione in cui essa risultava pi facilmente riconoscibile . inoltre , abbiamo valutato se il rc fosse pi evidente in soggetti con et superiore ai 65 anni come riportato in precedenti studi [ 3 ]  . functional phase fase funzionale in this phase , we evaluated whether the rc imaged with mr contributed to preserve shoulder function in patients in questa fase abbiamo cercato di valutare se il rc individuato con la rm sia in grado di preservare la f radiol med ( 2011 ) 116 : 102113 with rotator cuff lesions , as stated by other authors [ 2 , 3 ]  . unzionalit della spalla nei soggetti con lesione della cuffia dei rotatori come descritto da altri autori [ 2 , 3 ]  . patients between november 2007 and may 2008 , we enrolled 94 patients ( 46 males , 48 females ) for a total of 104 shoulders ( 62 right , 42 left )  . 
prior to mr examination , we obtained patient history , in particular , age , sex , reason for the examination and treatment with corticosteroids and / or ultrasoundguided treatment in the period before the examination . patients underwent a clinical examination based on jobes test ( arm abducted to 20 in the plane of the scapula , thumb pointing down ) [ 8 ] , to evaluate the presence of shoulder pain and shoulder disability . 
patients were excluded from the study if they had undergone surgical treatment for rotator cuff injury or were affected by diseases such as bone tumours that could affect shoulder function . mr imaging protocol mr scans were obtained with a 1.5 - t unit ( philips intera achieva , philips medical systems , best , the netherlands ) at centre 1 , a 0.2 - t unit ( esaote e - scan xq , genoa , italy ) at centre 2 and a 1.0 - t unit ( philips gyroscan nt , philips medical systems , best , the netherlands ) at centre 3 . 
patients were placed in a supine decubitus position , with the shoulder and scapula horizontal on the mr table to minimise motion artefacts , and the arm by the side in a neutral position or in mild external rotation . 
 presence or absence of degenerative alterations of the images were assessed for : supraspinatus tendon ; presence or absence of supraspinatus tendon tear , described as partial - thickness or full - thickness tear ; presence or absence of the rc . statistical analysis pazienti tra novembre 2007 e maggio 2008 abbiamo reclutato 94 pazienti ( 46 maschi e 48 femmine ) , per un totale di 104 spalle ( 62 spalle destre e 42 spalle sinistre )  . 
il reclutamento ha coinvolto 3 centri ( centro 1 , centro 2 e centro 3 )  . tutti i pazienti eseguivano lesame di rm della spalla su prescrizione di uno specialista in medicina dello sport o in ortopedia . 
in particolare ci siamo informati su : et , sesso , motivo dellesame , trattamento con cortisonici e / o con ultrasuoni ( us ) effettuato in data anteriore allesame rm . 
lesame clinico prevedeva leffettuazione del test di jobe ( braccio abdotto di 20 , sul piano della scapola , con pollice che punta in basso ) [ 8 ] , per valutare la presenza di : dolore di spalla , limitazione funzionale di spalla . 
abbiamo escluso dal nostro studio : pazienti sottoposti a trattamento chirurgico per lesione della cuffia dei rotatori , pazienti con patologie , quali ad esempio tumori ossei , che potessero alterare la funzionalit della spalla . protocollo rm lesame rm stato eseguito su 104 spalle . 
a p value < 0.05 was considered statistically significant . presenza o assenza di alterazioni degenerative del tendine sovraspinoso ; presenza o assenza di lesioni del tendine sovraspinoso descritte come lesioni parziali o complete ; presenza o assenza di rc . results morphological phase the rc was identified as a hypointense structure with respect to the tendon structures on proton density ( pd ) images . 
in oblique coronal scans , the structure appeared crescent - shaped , with almost regular margins , adjacent to the articular surface of the supraspinatus tendon medial to the tendons insertion point on the greater tuberosity . 
in those shoulders in which rc was observed ( 64 / 104 ) , the structure was identified in the oblique coronal scan in 53 / 64 ( 83% ) cases only , in the axial scan in 1 / 64 cases ( 2% ) only and in analisi statistica lanalisi statistica stata condotta con un software spss , versione 12.0 ( spss , chicago , illinois )  . 
un valore di p < 0 , 05 stato considerato statisticamente significativo . risultati fase morfologica allesame rm , il rc apparso riconoscibile come una struttura ipointensa rispetto alle strutture tendinee nelle immagini a densit protonica ( dp )  . 
nelle scansioni coronali - oblique , la struttura si presentava a forma di semiluna , con margini piuttosto regolari , adiacente alla superficie articolare del tendine sovraspinoso , medialmente al punto dinserzione di questultimo sulla grande tuberosit . 
moreover , in 7 / 64 cases ( 11% ) the structure was recognised in both the oblique coronal scan and the axial scan ; in 2 / 64 cases ( 3% ) , it was observed in both the oblique coronal scan and the sagittal scan . 
 functional phase functional data ( shoulder pain and / or disability on jobes test ) were available for 78 patients for a total of 84 shoulders ( 50 right , 34 left )  . 
a partial - thickness or full - thickness supraspinatus tendon tear was found in 28 / 84 cases ( 33% ) , in which no statistically significant difference was found between the presence or absence of the rc and disability on jobes test ( 2 = 1.17 ; p > 0.05 ) ( table 3 )  . 
similarly , in the remaining group ( 56 / 84 ; 67% ) with no supraspinatus tendon injury , there was no statistically significant difference between the presence or absence of rc and disability on jobes test ( 2 = 2.55 ; p > 0.05 ) , ( table 4 )  . 
nessuna differenza statisticamente significativa relativa allet stata trovata tra pazienti con presenza di rc e con assenza di rc ( test t di student = 0 , 05 ; p = 0 , 82 )  . 
nelle spalle in cui il rc stato individuato ( 64 / 104 ) , la struttura stata riconosciuta in 53 / 64 ( 83% ) casi solo in scansioni coronali - oblique , in 1 / 64 ( 2% ) casi solo in scansioni assiali , in 1 / 64 ( 2% ) casi solo in scansioni sagittali . 
inoltre , in 7 / 64 ( 11% ) casi la struttura stata individuata sia in scansioni coronali - oblique che in scansioni assiali ; in 2 / 64 ( 3% ) casi stata osservata sia in scansioni coronali - oblique che sagittali - oblique . fase funzionale i dati funzionali ( dolore alla spalla e / o limitazione funzionale al test di jobe ) si sono resi disponibili per 78 pazienti per un totale di 84 spalle ( 50 spalle destre e 34 sinistre )  . 
 stata osservata una correlazione statisticamente significativa tra presenza di lesione del sovraspinoso e limitazione funzionale al test di jobe ( beta = 1 , 649 ; p = 0 , 006 )  . 
inoltre , una correlazione statisticamente significativa stata riscontrata tra tendinopatia e dolore di spalla al test di jobe ( beta = 1 , 564 ; p = 0 , 05 )  . 
in questi ultimi non stata osservata alcuna differenza statisticamente significativa tra presenza o assenza di rc e limitazione funzionale al test di jobe ( 2 = 1 , 17 ; p > 0 , 05 ) , ( tabella 3 )  . 
allo stesso modo , nel rimanente gruppo senza evidenza di lesione del tendine alla rm ( 56 / 84 casi ; 67% ) , non stata riscontrata alcuna differenza statisticamente significativa tra radiol med ( 2011 ) 116 : 102113 table 3 functional data for patients with rotator cuff lesion on jobes test jobes test + for d 11 24 jobes test + for d 13 absence of rc presence of rc total rc , rotator cable ; d , disability 2 = 1.17 ; p > 0.05 assenza di rc presenza di rc totale rc , rotator cable ; d , impotenza funzionale 2 = 1 , 17 ; p > 0 , 05 absence of rc presence of rc total rc , rotator cable ; d , disability 2 = 2.55 ; p > 0.05 assenza di rc presenza di rc totale rc , rotator cable ; d , impotenza funzionale 2 = 2 , 55 ; p > 0 , 05 tabella 3 dati funzionali dei pazienti con lesione dei tendini della cuffia dei rotatori al test di jobe jobe test positivo per d jobe test negativo per d totale table 4 functional data for patients with no rotator cuff lesion on jobes test jobes test for d total tabella 4 dati funzionali dei pazienti senza evidenza di lesione dei tendini della cuffia dei rotatori al test di jobe jobe test positivo per d jobe test negativo per d totale jobes test for d 1 4 total fied on mr imaging in > 50% of cases ( 62% )  . 
 in contrast to the findings of burkhart et al . , who reported a mean rc thickness of 4.7 mm [ 2 , 3 ] , the rc reached a mean thickness of 2.8 mm in our sample . 
in our sample , the mean age of individuals with rc evidence at mr imaging was 55.314.9 years versus a mean age of 52.2815.5 years in presenza o assenza del rc e limitazione funzionale al test di jobe ( 2 = 2 , 55 ; p > 0 , 05 ) , ( tabella 4 )  . 
 jobes test is one of the most commonly used clinical tools for investigating shoulder pain and disability . however , its reproducibility is not high , thus leading to subjective evaluation errors . 
thus , jobes test proved to be a reliable tool for clinical examination of the shoulder . moreover , previous investigators [ 1113 ] reported a lack of association between shoulder disability on jobes test and rotator cuff lesions . 
conversely , we found a statistically significant correlation between shoulder disability on jobes test and rotator cuff lesions . shoulder pain is one of the most common symptoms reported by the patient . 
as a consequence , to limit the influence of variable pain on shoulder disability , we investigated individuals who received treatment with corticosteroid agents and / or ultrasound - guided therapy in the period prior to the mr examination . 
moreover , according to his hypothesis [ 2 , 3 ] , the presence of the rc could somehow influence preservation of normal shoulder function in patients with rotator cuff lesions , partly explaining why some individuals with rotator possiamo affermare che il rc una struttura riconoscibile in pi del 50% dei casi ( 62% )  . 
inoltre , attraverso le nostre sequenze di immagine , la sua identificazione risulta pi agevole nelle scansioni coronali - oblique , mentre pi difficoltosa nelle scansioni assiali e sagittali - oblique . 
che hanno riportato uno spessore medio del rc pari a 4 , 7 mm [ 2 , 3 ] , nel nostro campione tale struttura raggiunge uno spessore medio di 2 , 8 mtuttavia i risultati di burkhart et al . 
nel nostro campione , let media dei soggetti con rc alla rm era 55 , 314 , 9 anni contro unet media di 52 , 2815 , 5 anni dei pazienti nel quale il rc non era riconoscibile . 
inoltre , non stata osservata nessuna differenza statisticamente significativa tra questi due gruppi ( p = 0 , 82 )  . il test di jobe uno dei test clinici pi utilizzati per studiare il dolore di spalla e la limitazione funzionale . come noto , esso non ha unelevata riproducibilit essendo operatore - dipendente . 
di conseguenza , per limitare linfluenza della variabile dolore sulla limitazione funzionale di spalla , abbiamo valutato i pazienti che avevano effettuato terapia cortisonica e / o con us in data antecedente lesame di rm . 
nel nostro campione , i 7 / 84 ( 8% ) pazienti che avevano effettuato questo tipo di trattamento non hanno riferito alcun cambiamento significativo nella limitazione funzionale di spalla . 
per di pi , in accordo con la sua ipotesi [ 2 , 3 ] , la presenza del rc potrebbe in qualche modo condizionare la preservazione della normale funzionalit della spalla in pazienti con lesioni di cuffia giustificando in parte perch alcuni soggetti con lesioni della cuffia dei rotatori sono negativi al test di jobe . i nostri dati non mostrano alcuna differenza statisticamente significativa tra presenza e assenza di rc e limitazione funzionale al test di jobe in pazienti con lesioni del tendine sovraspinoso . 
pur considerando che i nostri risultati potrebbero essere stati in parte condizionati dalla bassa numerosit del campione e dal fatto che i macchinari rm a nostra disposizione potrebbero non aver potuto consentire di riconoscere il rc in alcuni casi , i nostri dati sembrano confutare le funzioni biomeccaniche attribuite alla struttura escludendo lipotesi che la presenza del rc potrebbe condizionare la funzionalit della cuffia dei rotatori . 
even considering that our results could be partly influenced by a small study sample and by the fact that mr scanners at our disposal did not allow recognition of the rc in some cases , our data seem to refute the biomechanical functions attributed to the rc and the hypothesis that the presence of this structure could condition rotator cuff function . 
second , our sample had a small number of young individuals ( mean age 54.09 years ) , and we were therefore unable to obtain any reliable estimation of possible evidence of the rc in the young population and of its possible influence on shoulder function . 
third , to make up for the small number of individuals with rotator cuff lesion ( 28 / 84 ) , we analysed our data in terms of presence or absence of lesions , without distinguishing between partialor full - thickness injuries . 
furthermore , mr imaging is known to have a high accuracy in diagnosing full - thickness lesions , reaching a sensitivity of 100% , but its performance in diagnosing partial - thickness tears is lower [ 15 ]  . 
this consideration adds to the fact that in the three centres involved in the study , shoulder mr imaging was performed with three different scanners and study protocols . nonetheless , we noted no substantial differences in shoulder imaging among the three centres . 
an additional limitation was that we had no follow - up data about surgical treatment in patients with rotator cuff injury and rc evidence on mr examination who did not show shoulder disability on jobes test . 
all three individuals had a partial - thickness supraspinatus tendon lesion . this finding , even though not statistically significant , allows us to hypothesise a possible biomechanical role for the rc in the case of partial - thickness tendon lesions in larger samples . 
further studies are needed to determine whether presence of the rc in patients with rotator cuff lesions could play a role in preserving shoulder function and partly influence the surgical management of such patients . 
questo risultato , pur non raggiungendo la significativit statistica , potrebbe far supporre in un campione pi grande un possibile ruolo biomeccanico del rc in caso di lesioni parziali del tendine . il nostro studio ha alcuni limiti . 
per compensare il basso numero di soggetti con lesione della cuffia dei rotatori ( 28 / 84 ) , abbiamo dovuto analizzare i nostri dati in termini di presenza o assenza di lesioni , senza distinguere tra lesioni parziali o complete . 
 inoltre noto che la rm ha unelevata accuratezza nel diagnosticare le lesioni complete ove raggiunge una sensibilit del 100% , ma le sue potenzialit nella diagnosi di lesioni parziali sono inferiori [ 15 ]  . 
questa considerazione si aggiunge al fatto che nei tre centri coinvolti nello studio , gli esami di rm della spalla sono stati effettuati utilizzando macchinari e protocolli di studio differenti . 
ad ogni modo non abbiamo notato differenze sostanziali nellimaging di spalla nei tre diversi centri.inoltre , non abbiamo dati di follow - up relativi ad un eventuale trattamento chirurgico effettuato in quei pazienti con lesioni della cuffia dei rotatori e presenza di rc allesame rm che non mostravano limitazione funzionale al test di jobe . in conclusione , nel nostro campione il rc stato individuato in pi del 60% dei casi . 
lambranzi , 1 , 37142 marzana , verona , italy 2centro di screening mammografico , dipartimento interaziendale di radiologia , azienda ospedaliera , padova , italy 3direzione generale ulss 20 , verona , italy correspondence to : s . 
lapprofondimento diagnostico stato eseguito indipendentemente dallarbitrato e il risultato dellapprofondimento ha costituito lo standard di riferimento ai fini dello studio . ipotizzando che un arbitrato negativo neghi la necessit di approfondimento , limpatto dellarbitrato stato valutato in termini di ridotto tasso di richiamo e di ridotto tasso diagnostico di carcinoma . 
i richiami alla doppia lettura sono stati 528 ( 6 , 8% ) dei quali 230 ( 43 , 5% ) concordanti e 298 ( 56 , 5% ) discordanti . 
complessivamente sono stati diagnosticati 49 carcinomi ( 6 , 39 tra soggetti esaminati , 9 , 2% tra soggetti richiamati ) : 43 carcinomi sono stati diagnosticati in richiami concordanti ( 5 , 6 tra soggetti esaminati , 18 , 6% tra richiami concordanti ) , 6 tra richiami discordanti ( 0 , 7 tra soggetti esaminati , 2 , 0% tra richiami discordanti )  . 
arbitration is a cost - effective procedure that could be employed as a first measure to counterbalance excess recall rate observed in a double - reading scenario . keywords breast cancer screening mammography double reading arbitration avrebbe risparmiato 216 procedure di approfondimento diagnostico ( riduzione del tasso di richiamo : 2 , 8% assoluta , 40 , 9% relativa ) e mancato la diagnosi di un carcinoma ( riduzione del tasso diagnostico : 0 , 13 assoluta , 2 , 0% relativa )  . 
larbitrato una procedura efficace e conveniente dal lato economico , che potrebbe essere impiegata correntemente quale prima misura di correzione ove si osservi un tasso di richiamo eccessivo , specie in scenari che impieghino la doppia lettura . parole chiave carcinoma mammario screening mammografia doppia lettura arbitrato introduction introduzione mammography screening has been demonstrated to be effective in reducing breast cancer mortality [ 1 ] and is currently recommended by the european commission ( ec ) [ 2 ]  . 
full coverage by organised programmes has been achieved or is under way in almost all western countries . in italy , real coverage was estimated to be 62.3% by the end of 2007 according to the last survey of the osservatorio nazionale screening [ 3 ]  . 
double reading , which is also recommended as a standard policy , as it substantially increases sensitivity [ 4 ] , is associated with increased rr [ 5 , 6 ]  . 
arbitration of discordant double readings has been recommended as a measure to reduce excess rr [ 7 , 8 ]  . arbitration of discordant double readings was first evaluated in italy in the florence programme [ 9 ] , and its usefulness in reducing rr was confirmed , together with a very limited and acceptable reduction in cancer detection rate ( dr )  . 
in this study , we evaluated the role of arbitration of discordant double readings in the screening programmes of the cities of verona and padua , veneto region , italy . lo screening mammografico stato dimostrato essere efficace nel ridurre la mortalit per carcinoma mammario [ 1 ] ed correntemente raccomandato dalla comunit europea ( ce ) [ 2 ]  . 
in italia la copertura reale stata stimata essere del 62 , 3% alla fine del 2007 , in base alla ultima analisi diffusa dallosservatorio nazionale screening [ 3 ]  . 
tra questi , il tasso di richiamo ( recall rate , rr ) ad approfondimento diagnostico di casi positivi allo screening non dovrebbe eccedere il 7% al primo screening e il 5% agli screening successivi . 
la doppia lettura , anchessa raccomandata come pratica corrente perch capace di aumentare sostanzialmente la sensibilit [ 4 ] , associata ad un aumento del rr [ 5 , 6 ]  . larbitrato delle doppie letture discordanti stato raccomandato come misura atta a ridurre leccesso di rr causato dalla doppia lettura [ 7 , 8 ]  . 
larbitrato delle doppie letture discordanti stato valutato una prima volta in italia nel programma di firenze [ 9 ] e la sua utilit nel ridurre il rr stata confermata , unitamente ad una riduzione , molto limitata ed accettabile , del tasso diagnostico di carcinoma ( detection rate , dr )  . 
nel presente studio viene valutato il ruolo dellarbitrato delle doppie letture discordanti nei programmi di screening delle citt di verona e padova , regione del veneto . material and methods materiali e metodi verona ( 2008 target - year population = 28 , 760 ) and padua ( 2008 target - year population = 27 , 377 ) mammography screening programmes were implemented in 1999 and i programmi di screening delle citt di verona ( popolazione obiettivo per lanno 2008 , 28760 ) e di padova ( popolazione obiettivo per lanno 2008 , 27377 ) sono in attivit rispettivaradiol med ( 2011 ) 116 : 8491 2001 , respectively . 
overall rr has been reported to be higher than recommended standards at both first and repeat screening [ 10 ] , and a study of the impact of arbitration of discordant double readings by a third reader was designed and performed in 2009 - 2010 . 
recalls to diagnostic assessment by one of two readers only ( henceforth referred to as discordant ) were arbitrated by a third reader ( sc , with > 30 years experience and > 200 , 000 readings in screening mammography )  . 
all cases , irrespective of arbitration result , underwent diagnostic assessment , the result of which was assumed as the reference standard for the study purpose . diagnostic assessment was based on bilateral palpation and ultrasonography in all cases . 
data for each recalled case were patients id , screening date , firstand second - reader report ( negative , recall ) , arbitration report for discordant double readings ( negative , recall ) and final outcome ( cancer , no cancer ) for assessed cases ( concordant or discordant recalls )  . 
 cost analysis of the introduction of arbitration in the screening process was also attempted , although this was not easy , as detailed screening cost estimates in the italian scenario are few and relate to different calendar periods . we chose the 2005 florence scenario as a reference , as data allowing for adjustment by discount rate and conversion to euros were available for this setting only . 
arbitration cost implied adding only a third additional reading : cost per digital mammography reading in the florence scenario was estimated to be 0.25 euros in 2005 by ciatto et al . 
in particolare impiegano entrambi la mammografia digitale diretta con doppia lettura differita : sei radiologi , aventi esperienza di lettura mammografica da 2 a oltre 10 anni , sono attualmente addetti alla lettura delle mammografie di screening . 
il rr complessivo stato riportato essere pi elevato degli standard accettabili raccomandati sia al primo screening che ai successivi [ 10 ] : per questo , uno studio dellimpatto dellarbitrato delle doppie letture discordanti da parte di un terzo lettore stato disegnato e condotto nel periodo 20092010 . 
i richiami richiesti da un solo dei due lettori ( dora in avanti indicati come discordanti ) sono stati arbitrati da un terzo lettore ( sc ) con una esperienza di oltre 30 anni e oltre 200000 mammografie lette . 
tutti i casi , a prescindere dai risultati dellarbitrato , sono comunque stati sottoposti ad accertamento diagnostico , il cui risultato stato assunto come standard di riferimento ai fini dello studio . 
i dati disponibili per ogni caso di richiamo sono stati : identificativo della paziente , data dellesame di screening , diagnosi posta dal primo e dal secondo lettore ( negativo , richiamo ) , risultato dellarbitrato per i casi discordanti ( negativo , richiamo ) , esito finale ( carcinoma , altro ) per i casi sottoposti ad accertamento diagnostico ( concordanti o discordanti alla doppia lettura )  . 
stato in particolare calcolato quale sarebbe stato limpatto dellarbitrato in termini di rr e di dr di carcinoma se i casi discordanti arbitrati come negativi non fossero stati avviati ad approfondimento . stata tentata anche una analisi dei costi conseguenti alla introduzione dellarbitrato nel processo di screening , anche se questo non stato facile , dal momento che stime dettagliate del costo dello screening nello scenario italiano sono state poche e riferite a periodi diversi . 
abbiamo scelto lo scenario del programma di screening di firenze nel 2005 , dal momento che solo i dati di questo studio consentivano lapplicazione del tasso di sconto e la conversione ad euro . 
i costi relativi allarbitrato consistono sostanzialmente nel costo aggiuntivo di una terza lettura : il costo relativo alla lettura con mammografia digitale diretta stato stimato nel 2005 da ciatto et al . 
 [ 12 ] nel 1995 in 83 , 3136 , 3 dollari statunitensi per accertamento : dopo aggiustamento per tasso di sconto 19952005 e tasso di radiol med ( 2011 ) 116 : 8491 $5 , 1807 , 424 in 1995 after adjustment for the 19952005 discount rate and conversion to euros corresponded to 4 , 1956 , 013 erous per screen - detected cancer . 
overall , 49 cancers were detected ( 6.39 among screened , 9.2% among recalled ) : 43 were detected among concordant recalls ( 5.6 among screened , 18.6% among concordant recalls ) and six among discordant recalls ( 0.7 among screened , 2.0% among discordant recalls )  . six were observed among arbitrated cases : five ( 6% ) in positive and 1 ( 4.6 ) in negative arbitrations . 
if discordant recalls arbitrated as negative had not been assessed , returning to periodic screening , 216 assessment procedures would have been spared and one cancer would have been missed . 
the results are summarised in table 1 , where they are compared with those of the only other italian report on the arbitration procedure [ 9 ] , studying a larger series from another population - based screening setting employing different operators . 
the chosen study setting was suitable , as it had a high rr compared with recommended standards : an average rr of 6.8% is high , considering that the large majority of screened women were at repeat screening and that the recommended acceptable highest rr at repeat screening is 5% [ 2 ]  . 
 the choice of arbitrating only discordant double readings proved correct : in fact , discordant double readings conversione dollaro statunitense / euro il costo corrispondente risultato di 67 , 4110 , 4 euro per approfondimento . 
le differenze osservate nello studio sono state valutate mediante test chi - quadrato ( 2 ) , ponendo la significativit statistica a un livello di p < 0 , 05 . 
i richiami totali ad approfondimento alla doppia lettura sono stati 528 ( 6 , 8% ) dei quali 230 ( 43 , 5% ) concordanti e 298 ( 56 , 5% ) discordanti . 
questi ultimi sono stati sottoposti ad arbitrato , risultato rispettivamente negativo in 216 ( 72 , 4% ) e positivo in 82 ( 27 , 6% )  . complessivamente sono stati diagnosticati 49 carcinomi ( 6 , 39 tra soggetti esaminati , 9 , 2% tra soggetti richiamati ) : 43 carcinomi sono stati diagnosticati in richiami concordanti ( 5 , 6 tra soggetti esaminati , 18 , 6% tra richiami concordanti ) , e solo 6 in richiami discordanti ( 0 , 7 tra soggetti esaminati , 2 , 0% tra richiami discordanti )  . 
dei 6 cancri osservati nei casi arbitrati , in 5 ( 6% tra soggetti arbitrati ) larbitrato era stato positivo , e in un solo caso ( 4.6 tra soggetti arbitrati ) era stato negativo . 
se i casi con doppia lettura discordante arbitrati come negativi non fossero stati sottoposti ad approfondimento diagnostico , sarebbero stati risparmiati 216 approfondimenti e non sarebbe stato diagnosticato un carcinoma . 
i risultati sono riassunti nella tabella 1 , dove sono confrontati con quelli ottenuti dallaltro studio italiano in tema di arbitrato [ 9 ] , che aveva valutato una serie assai pi numerosa in un altro scenario di screening coinvolgente altri operatori . 
per quanto riguarda lanalisi dei costi nello scenario di studio , il costo relativo allarbitrato ( 298 terze letture di doppie letture discordanti ) stato pari a 74 euro mentre quello dei 216 approfondimenti risparmiati pari a 14558 , 423346 euro . 
 la scelta di arbitrare solo le doppie letture discordanti si dimostrata corretta : infatti le doppie letture discordanti hanno un valore predittivo positivo molto basso ( 2 , 0% ) rispetto alle concordanti ( 18 , 6% ) e danno il massimo contributo ai richiami inutili ( 60 , 9% )  . 
larbitrato negativo avrebbe consentito una drastica riduzione del rr che sarebbe rientrato negli standard raccomandati : infatti le doppie letture concordanti e gli arbitrati positivi di doppie letture discorradiol med ( 2011 ) 116 : 8491 tion . 
the arbitrated subset setting allows for a biased sensitivity assessment : first , cancers detected only by one of two readers are considered to be difficult , being selected among those with borderline and subtle signs ; second , the aim of arbitration is not to detect ( the lesion has already been detected by one reader ) but to classify another readers finding . 
with all these limitations and using assessment outcome as the reference standard , arbitration had a sensitivity of 83.3% ( five of six cancers in the arbitrated subset )  . 
 that introducing the arbitration procedure is highly convenient from the cost viewpoint is quite evident , although sparing the cost of a substantial proportion of assessment procedures will not ultimately have a major impact on screening costs ( cost per woman screened ) , which are mainly accounted for by organisation and firstscreening level [ 12 ]  . 
the net balance of 23 , 272 eruos in this study setting was much higher than the estimated cost of 4 , 195 - 6 , 013 euros per cancer detected at screening . 
not that we should necessarily consider missing one cancer as a cost to be negotiated ; nevertheless , in a context such as italy , where full real coverage of the eligible population by organised screening is still far from 100% , the money saved by introducing the arbitration procedure could be properly invested in the screening process , allowing for increased coverage . according to our findings , for each cancer missed due to false negative arbitration , the resources saved by arbitration could allow for three to five additional cancers being detected in women who are presently unscreened due to a lack of resources . 
second , assessment of discordant readings , often managed by simple additional views or ultrasonography , is likely to have a lower cost compared with assessment of concordant recalls , which is more likely to prompt costly invasive procedures . 
considering such possible biases in cost estimates , cost analysis was repeated by doubling the cost per mammography reading to 0.50 euros and by reducing the cost per assessment procedure to 50 euros . 
even with these changes , the net balance of introducing the arbitration procedure remains favourable , with an overall saved cost of 10 , 651 euros , which , if invested in screening more women , would allow for two additional cancers detected per each cancer missed by false negative arbitration . danti assommano a 312 casi , pari ad un rr del 4 , 0% . 
da un lato i casi arbitrati vengono comunemente ritenuti difficili , in quanto diagnosticati da uno solo di due lettori e quindi associati a segni radiologici sottili e al limite del normale . dallaltro il fine dellarbitrato non quello di percepire ( la lesione gi stata percepita da uno dei due lettori ) , ma di classificare il giudizio di un altro lettore . 
 che introdurre la pratica dellarbitrato sia conveniente sul piano dei costi ben evidente , anche se risparmiare i costi di un numero sia pure sostanziale di approfondimenti alla fine non avr un impatto ingente sui costi complessivi dello screening ( costo per donna esaminata ) che sono determinati in maggior misura dai costi organizzativi e dal primo livello di screening [ 12 ]  . 
in ogni caso lanalisi dei costi consente un punto di vista particolare per quantizzare la rilevanza delle mancate diagnosi di carcinoma dovute a arbitrato negativo . il bilancio netto di 23272 euro risparmiati per ogni mancata diagnosi di carcinoma osservato in questo studio assai pi elevato del costo per carcinoma diagnosticato allo screening , stimato in 41956013 euro . 
non che questo significhi in assoluto che la mancata diagnosi di un carcinoma debba essere necessariamente negoziata : tuttavia , in un contesto quale quello italiano , dove la copertura totale della popolazione eleggibile da parte di screening organizzato ancora lontana dal 100% , le risorse risparmiate introducendo la pratica dellarbitrato potrebbero essere utilmente reinvestite nel processo di screening , consentendo un aumento della copertura . 
in base alle nostre osservazioni , per ogni carcinoma non diagnosticato con lintroduzione dellarbitrato , il risparmio economico avrebbe consentito la diagnosi di 35 carcinomi aggiuntivi in soggetti attualmente non sottoposti a screening per mancanza di risorse . 
anzitutto questi sono stati stimati in base a quelli determinati in un centro di eccellenza , dove ci si pu attendere che la lettura sia pi efficiente che in uno scenario nazionale medio . 
inoltre lapprofondimento delle doppie letture discordanti , spesso risolto con semplici particolari mammografici o con la sola ecografia , potrebbe avere un costo inferiore a quello dei richiami per doppia lettura concordante , che pi facilmente generano i costi relativi a procedure invasive . 
anche con queste variazioni il bilancio netto relativo alla adozione dellarbitrato resta favorevole , con un costo medio risparmiato di 10651 euro , che , se investito in estensione della copertura da screening , consentirebbe la radiol med ( 2011 ) 116 : 8491 relatively few literature studies address the issue of arbitration of discordant double readings used as a current procedure . 
kopans [ 13 ] reports that a third reading substantially reduces recall rate to diagnostic assessment . in a study comparing computer - aided detection and arbitration of discordant double readings , james and cornford [ 14 ] confirm that arbitration reduces overall recalls and is substantially more specific compared with computer - aided detection while missing a limited number of cancers due to false negativity . 
 [ 7 ] , in which arbitration by a panel of three experts of discordant double readings persisting after consensus reduced discordant recalls by 51% and overall recalls by 14% , with a limited number of false negatives . 
however , this study is based on an extremely low recall rate ( 1% ) , quite common in dutch programmes , and is hardly comparable with other european scenarios . similar comparison of our study findings with the florence experience is particularly interesting . 
although the overall settings were ( organised population - based screening of 50to 69 - year - old women , most at repeat screening , using delayed double reading ) , the operators involved were different ( sc , who did the arbitration in the study reported here , was working in florence in 2005 but had no active role in double reading or arbitration of that series ) and the programmes had a different history : florence was a well - known excellence centre with 35 years experience in population - based screening and 10 years practice of double reading , whereas the verona and padua screening programmes are current service screening entities in which double reading has only recently been introduced . 
nevertheless , a substantial concordance of results observed between the florence experience and our study adds to the reproducibility and generalisability of our study findings to any other italian service screening scenario . 
 in conclusion , arbitration is confirmed to be a costeffective procedure and might be employed as a first measure to counterbalance the excess rr observed in a double - reading scenario . diagnosi di 2 carcinomi aggiuntivi per ogni cancro con mancata diagnosi a causa di arbitrato negativo . relativamente poco stato pubblicato in letteratura in merito alluso corrente dellarbitrato di doppie letture discordanti . 
in un confronto tra diagnosi computer assistita e arbitrato james e cornford [ 14 ] confermano la riduzione del tasso di richiamo operata dallarbitrato , che risulta decisamente pi specifico della computed assisted diagnosis ( cad ) , anche se perde qualche carcinoma per false negativit . 
levidenza pi interessante forse quella riportata da duijm et al . [ 7 ] : larbitrato da parte di un panel di tre esperti delle doppie letture discordanti anche dopo consenso riduce i richiami discordanti del 51% e i richiami complessivi 14% , con un numero limitato di falsi negativi : peraltro tale esperienza , che parte da un tasso di richiamo eccezionalmente basso ( 1% ) come comunemente in uso in olanda , mal confrontabile con le altre esperienze europee . 
anche se lo scenario complessivo simile ( screening organizzato di popolazione di donne residenti dai 50 ai 69 anni di et , per lo pi a screening ripetuto , con doppia lettura differita ) gli operatori coinvolti erano diversi ( sc , che ha eseguito larbitrato nel presente studio , operava nello screening di firenze nel 2005 ma non aveva partecipato n alla doppia lettura n allarbitrato relativamente a quello studio ) e i programmi presentavano differenze . 
firenze era un centro di eccellenza noto , con 35 anni di esperienza di screening di popolazione e 10 anni di pratica corrente di doppia lettura , mentre verona e padova sono , sia pure con buona qualit , realt di screening di servizio dove la doppia lettura differita stata introdotta solo recentemente . 
passariello1 1department of radiological science , university of rome la sapienza policlinico umberto i , viale regina elena 328 , 00161 rome , italy 2igea biophysics laboratory , carpi , modena , italy correspondence to : c.v. 
ad - sos and ubpi were measured at the phalangeal metaphysis using a dbm sonic device . multiple logistic regression analysis was performed to estimate the odds ratio ( or ) for vertebral fractures . 
confronto fra i parametri ultrasonografici quantitativi ( qus ) amplitude dependent speed of sound ( ad - sos ) e ultrasound bone profile index ( ubpi ) a livello delle falangi della mano con la densit minerale ossea ( bmd ) alla colonna lombare e al femore prossimale mediante tecnica dual energy x - ray absorptiometry ( dxa ) nel discriminare le fratture vertebrali . 
fractures resulting from osteoporosis lead to high rates of morbidity and mortality and reduce quality of life and are responsible for a sharp increase in healthcare costs [ 2 , 3 ]  . 
demographic studies also indicate a continuing increase in the proportion of women older than 50 years , and this segment of the population is expected to become predominant in the decades to come . 
in postmenopausal women , it would be both useful and desirable to adopt a preventive approach to the problem , with the aim of slowing disease progression and preventing many fractures [ 5 ]  . 
in order to promote a more rational allocation of resources , a reliable diagnostic method is required that is capable of identifying women at increased risk of fracture . over the past 25 years , many noninvasive methods have been developed that rely on the attenuation of ionising radiation to quantify bone mineral density ( bmd ) at the peripheral , axial and total skeletal level . 
these methods provide a measure of bmd , which is currently considered the best predictor of osteoporotic fractures [ 7 ]  . however , these techniques are still only able to explain 60%80% of the variability in bone strength , and it has been demonstrated that other mechanical aspects of the bone are important in determining fracture risk [ 8 ]  . 
these factors include microarchitectural parameters and geometric and elastic properties of bone tissue , which cannot be assessed using densitometric techniques [ 9 ]  . quantitative ultrasound ( qus ) methods have been developed over the past 10 years to determine bone quality and the state of the skeleton on the basis of various studies that suggest that sonographic parameters were able to provide information not only about bone density but about its structure and elastic properties [ 1012 ]  . 
the qus devices currently available can be applied to different peripheral sites of the skeleton : the calcaneus , the proximal phalanges of the hand and the tibial sha interest in this technique stems from practical , economic and health safety aspects : it is much faster , simpler and more portable than dxa ; it is less expensive , and it does not employ ionising radiation . these features suggest a role for qus as an effective losteoporosi una malattia scheletrica sistemica caratterizzata da ridotta massa ossea e deterioramento della microarchitettura del tessuto , con un conseguente aumento della fragilit ossea e del rischio di frattura [ 1 ]  . 
le fratture conseguenti allosteoporosi portano ad elevata morbilit e mortalit , riducono la qualit della vita degli individui affetti , e sono responsabili di un forte aumento dei costi del sistema sanitario [ 2 , 3 ]  . 
nelle donne in post - menopausa un approccio preventivo al problema , prima dellevento frattura , sarebbe utile e auspicabile , con la finalit di rallentare la progressione della malattia ; in tal modo molte fratture potrebbero essere evitate [ 5 ]  . 
per favorire una pi razionale allocazione delle risorse importante quindi utilizzare una metodica diagnostica affidabile per identificare le donne a maggior rischio di frattura . negli ultimi 25 anni sono state sviluppate molte metodiche non invasive basate sullattenuazione delle radiazioni ionizzanti per quantificare la densit minerale ossea ( bmd ) a livello scheletrico periferico , assiale e totale . 
i metodi maggiormente utilizzati sono : la densitometria a doppio raggio x ( dxa ) e la tomografia quantitativa computerizzata ( qct ) [ 6 ]  . questi metodi forniscono la misura della bmd , che attualemtne considerata il migliore predittore delle fratture osteoporotiche [ 7 ]  . 
comunque , queste tecniche sono in grado di spiegare solo il 60%80% della variabilit della resistenza ossea , inoltre stato evidenziato che altri aspetti meccanici dellosso sono importanti nella determinazione del rischio di frattura [ 8 ]  . 
questi fattori includono i parametri microarchitetturali , le propriet elastiche e geometriche del tessuto osseo , che non sono valutabili mediante le tecniche densitometriche [ 9 ]  . i metodi ultrasonografici quantitative ( qus ) sono stati sviluppati negli ultimi 10 anni per la determinazione della qualit dellosso e dello stato dello scheletro sulla base di varie esperienze che suggerivano che i parametri ultrasonografici potessero fornire informazioni non solo sulla densit ossea , ma anche sulla struttura e sulle propriet elastiche del tessuto [ 1012 ]  . 
linteresse verso questa metodica nasce da aspetti pratici : infatti molto pi veloce , semplice e trasportabile rispetto alla dxa ; da aspetti economici : infatti meno costosa ; da aspetti di sicurezza : non utilizza radiazioni ionizzanti . 
queste caratteristiche suggeriscono per radiol med ( 2011 ) 116 : 92101 screening tool for osteoporosis in postmenopausal women . the purpose of this study was to assess the ability of the ultrasound parameters of amplitude - dependent speed of sound ( ad - sos ) and ultrasound bone profile index ( ubpi ) when compared with those of dxa in identifying women with and without osteoporotic vertebral fractures . la qus una collocazione come efficace strumento di screening per losteoporosi nella popolazione femminile postmenopausale . 
lo scopo di questo studio di valutare labilit dei parametri ultrasonografici amplitude dependent speed of sound ( ad - sos ) e ultrasound bone profile index ( ubpi ) in confronto con i parametri dxa nellidentificare le donne con e senza fratture vertebrali da osteoporosi . materials and methods study population materiali e metodi popolazione a total of 692 postmenopausal italian women aged between 45 and 84 years were enrolled in the study . 
women receiving antiosteoporosis agents , such as calcitonin , oestrogen , raloxifene , bisphosphonates , anabolic steroids , parathyroid hormone , teriparatide , calcium and vitamin d were also excluded , as were all those with a history of severe trauma or previous fractures . 
lindice di massa corporea ( body mass index , bmi ) stato calcolato come rapporto fra peso espresso in kg e il quadrato dellaltezza espresso in metri [ 13 ]  . 
inoltre sono state escluse le donne in trattamento con farmaci utilizzati per la cura dellosteoporosi quali calcitonina , estrogeni , raloxifene , bifosfonati , anabolizzanti , paratormone , teriparatide , calcio e vitamina d . 
lo studio stato approvato dal comitato etico locale . bone densitometry densitometria ossea bone densitometry using a dxa device ( hologic qdr 2000 plus , bedford , ma , usa ) was performed on all individuals . 
a technician with 15 years of experience ( em ) obtained scans of the lumbar spine ( l1l4 ) and proximal femur ( neck and total hip ) in the posteroanterior projection . the individuals for whom it was impossible to assess at least three vertebral bodies were excluded from the analysis . individuals with fractured lumbar vertebrae and vertebrae exhibiting major degenerative changes on radiography were excluded from the analysis to avoid artefacts in the measurement of the bmd . 
results are expressed as bmd ( g / cm2 ) obtained by dividing the mineral content in the region of interest ( roi ) by the area of the region . 
da un tecnico con circa 15 anni di esperienza ( em ) , utilizzando uno strumento dxa ( hologic qdr 2000 plus , bedford , ma , usa )  . 
i risultati sono espressi in termini di bmd ( g / cm2 ) ottenuta dal rapporto fra il contenuto minerale rilevato nella regione di interesse e larea della regione stessa . 
ogni individuo stato classificato sulla base del suo t - score in normale ( t - score > 1 , 0 ) , osteopenico ( t - score compreso tra 1 , 0 e 2 , 5 ) , o osteoporotico ( tscore2 , 5 ) in accordo con i criteri diagnostici della organizzazione mondiale della sanit [ 15 ]  . 
la precisione a lungo termine ( coefficiente di variazione ) stato determinato ripetendo 2 volte sullo stesso soggetto , la scansione entro 5 settimane in 80 donne con et compresa tra 30 e 55 anni . radiol med ( 2011 ) 116 : 92101 phalangeal ultrasonography ultrasound measurements were performed on all individuals at the distal metaphysis of the proximal phalanges of the last four digits of the hand using the dbm sonic bone profiler device ( igea , carpi , italy )  . 
the device consists of two piezo - electric transducers coaxially mounted on a high - precision calliper , the first acting as a transmitter and the second as a receiver . 
the device automatically calculates the speed of signal transmission through the phalanx by measuring the thickness of the digit ( including soft tissues ) and the time required for transmission . 
in this way , the calculated speed is dependent on amplitude and thus termed amplitude - dependent speed of sound ( ad - sos ) [ 17 ]  . we also assessed an additional parameter known as the ultrasound bone profile index ( ubpi ) , which is derived from three sonographic parameters combined to maximise discrimination between individuals with and without fractures , as recently reported [ 14 , 18 ]  . 
to determine reproducibility of the method , the same operator who carried out the study measurements calculated the variation coefficient by performing six repeated measurements on five individuals . assessing vertebral fractures to assess for the presence of vertebral fractures ( either lowenergy or spontaneous ) , lateral radiographs of the thoracolumbar spine were obtained with an x - ray system identical to that employed in thoracic imaging [ 18 ] ; all study participants were subjected to spinal radiography with standardised procedures that we have recently reported [ 19 ]  . radiographs were evaluated by two independent radiologists ( cva and rp ) using the semiquantitative method proposed by genant et al . 
 le misure sono state eseguite sulla mano non dominante , anche se stato osservato in precedenti studi che non ci sono differenze statisticamente significative fra le misure sulle due mani [ 16 ]  . 
lapparecchio costituito da due sonde piezoelettriche montate coassiali su un calibro di precisione , una agisce come emittente e una come ricevente ; le sonde vengono posizionate da una parte e dallaltra rispetto alla falange da misurare sulle superfici latero - mediale della stessa . 
lo strumento calcola automaticamente la velocit di trasmissione del segnale attraverso la falange misurando lo spessore del dito ( inclusi i tessuti molli ) e il tempo di trasmissione del segnale : il rapporto fra le due grandezze fornisce la velocit di trasmissione . 
il tempo di trasmissione definito come il tempo trascorso fra lemissione del segnale da parte della sonda emittente e la ricezione del segnale quando esso raggiunge una ampiezza predeterminata ( 2 mv ) per la prima volta ; in tal modo la velocit calcolata viene detta dipendente dallampiezza e chiamata ad - sos [ 17 ]  . 
 abbiamo inoltre valutato un ulteriore parametro chiamato ubpi che deriva da 3 parametri ultrasonografici combinati per ottimizzare la discriminazione fra soggetti con e senza fratture , come riportato recentemente [ 14 , 18 ]  . 
per determinare la riproducibilit dello strumento , stato calcolato il coefficiente di variazione , ottenuto dallo stesso operatore che ha effettuato le misure dello studio , effettuando 6 misure ripetute su 5 soggetti . valutazione delle fratture vertebrali per valutare la presenza di fratture vertebrali ( a bassa energia o spontanee ) , sono state eseguite delle radiografie del rachide dorso - lombare in proiezione laterale utilizzando lo stesso strumento radiologico per immagini toraciche [ 18 ] ; tutti i partecipanti allo studio sono stati sottoposti a radiografia spinale mediante procedure standardizzate come da noi riportato recentemente [ 19 ]  . 
 quality assurance ulteriori controlli di qualit quotidiani sono stati eseguiti sulle apparecchiature dxa e qus in accordo con le linee guida delle aziende produttrici per verificare la stabilit e calibrazione degli strumenti . 
 radiol med ( 2011 ) 116 : 92101 turers guidelines to verify device stability and calibration . analisi statistica statistical analysis data analysis was performed using spss 15.0 software ( spss inc . , chicago , il , usa )  . 
based on roc analysis , we calculated the area under the curve ( auc ) and its standard errors ( se ) with significance levels using the method of hanley and mcneil [ 21 ]  . 
la regressione logistica multipla stata eseguita per determinare gli odds ratio ( or ) per le fratture vertebrali e i corrispondenti intervalli di confidenza al 95% ( ci )  . 
gli or sono stati aggiustati per le variabili antropometriche risultate significative et , altezza , peso per calcolare il rischio di frattura per diminuzione di una deviazione standard della variabile considerata . 
dallanalisi roc stata calcolata larea sotto la curva ( auc ) e gli errori standard con i relativi livelli di significativit seguendo il metodo di hanley e mcneil [ 21 ]  . 
valori di significativit inferiori a 0 , 05 sono stati considerate statisticamente significativi . risultati i dati raccolti durante le procedure di quality assurance per entrambi gli strumenti non hanno rilevato nessun malfunzionamento o scostamento dai valori di calibrazione durante lintero periodo di durata dello studio . 
la precisione delle misure e lintervallo di confidenza al 95% sono state calcolate per la bmd a livello lombare e femorale rispettivamente : 1 , 0% ( 0 , 9%1.1% ) , 1 , 2% ( 1 , 0%1 , 3% )  . 
although not strong , the correlations were all highly significant ( p < 0.00001 ) , as shown in table 2 . lanalisi della regressione lineare tra le variabili qus e dxa ha evidenziato la migliore correlazione rispettivamente tra il parametro ad - sos e la bmd del rachide lombare ( r = 0 , 31 )  . 
le correlazioni , sebbene non elevate , sono risultate tutte altamente significative ( p < 0 , 00001 ) come riportato in tabella 2 . radiol med ( 2011 ) 116 : 92101 table 1 clinical , anthropometric , dual - energy x - ray absorptiometry ( dxa ) and quantitative ultrasound ( qus ) characteristics in individuals with and without osteoporotic vertebral fractures . 
however , both the dxa and qus variables showed higher levels of significance ( p < 0.0001 ) in discriminating fractures when compared with age and the other anthropometric parameters ( table 3 )  . 
in the multiple logistic model , all dxa and qus measurements contributed significantly to the discrimination of fractures ( p < 0.0001 ) , as can be seen in table 3 . 
comunque sia le misure dxa che qus hanno mostrato un migliore livello di significativit ( p < 0 , 0001 ) nella discriminazione delle fratture rispetto alla variabile et e agli altri parametri antropometrici ( tabella 3 )  . nel modello logistico multiplo tutte le misure dxa e qus hanno mostrato un significativo contributo alla discriminazione delle fratture ( p < 0 , 0001 ) , come si pu osservare nella tabella 3 . 
comunque i valori di ors , che indica laumento del rischio per diminuzione di 1 deviazione standard della misura , sono risultati maggiori per la bmd alla colonna lombare ( or 4 , 01 ) , seguiti dallad - sos ( or 3 , 81 ) e dalla bmd total hip ( or 3 , 77 ) e neck ( or 3 , 62 )  . 
applicando lanalisi roc ai soggetti con e senza fratture vertebrali , la migliore prestazione nella discriminazione stata osservata di nuovo per la bmd lombare ( auc 0 , 840 , 03 ) , la bmd total hip ( auc 0 , 810 , 03 ) , ad - sos ( auc 0 , 790 , 03 ) e per la bmd neck ( auc 0 , 790 , 03 ) ( tabella 3 )  . discussion discussione this paper reports the results of a cross - sectional study conducted on a large cohort of italian women who underwent dxa of the lumbar spine and proximal femur and qus with ad - sos and ubpi of the phalanges to assess the ability of the techniques to discriminate between individuals with and without osteoporotic vertebral fractures . 
the results suggest that bmd measurements at the lumbar spine and proximal femur , as well as the qus parameters adsos and ubpi , are able to distinguish postmenopausal women with vertebral fractures . numerous studies have examined the correlation between dxa and qus parameters measured at various skeletal sites . 
the discriminatory potential in classifying individuals with or without vertebral fractures was tested in cross - sectional studies using a range of qus methods , including qus of the phalanx , and dxa in a sample of older postmenopausal women [ 23 ]  . 
in addition , a multicentre european study assessed the performance of five different ultrasound devices and their association with vertebral fractures compared with dxa in a group of european women [ 24 ]  . analysis of fracture discrimination showed that qus has a similar ability to femoral bmd in identifying vertebral fractures . 
furthermore , after adjusting for age , weight and height , the increased risk arising from a decrease of 1 sd reached the value of 4.20 for ad - sos , practically equivalent to bmd of the lumbar spine . 
la potenzialit discriminatoria nel classificare soggetti con o senza fratture vertebrali stata testata in studi trasversali con vari strumenti qus , inclusa la qus alla falange e la dxa in un campione di donne anziane in postmenopausa [ 23 ]  . 
uno studio multicentrico europeo ha pubblicato inoltre le prestazioni di 5 diversi strumenti a ultrasuoni e la loro associazione con le fratture vertebrali , in confronto con la dxa in un gruppo di donne europee [ 24 ]  . lanalisi di discriminazione delle fratture ha rivelato che la qus possiede una abilit simile alla bmd femorale nellidentificazione delle fratture vertebrali . 
inoltre , aggiustando per et , peso e altezza , laumento di rischio per diminuzione di una deviazione standard raggiunge il valore di 4 , 20 per ad - sos , praticamente equivalente alla bmd del rachide lombare . 
altri studi [ 2325 ] hanno ottenuto valori di or inferiori nella discriminazione delle fratture vertebrali , ci radiol med ( 2011 ) 116 : 92101 100 radiol med ( 2011 ) 116 : 92101 obtained lower or values in discrimination of vertebral fractures , perhaps due to differences in the characteristics of the study populations . 
it should be noted that all these studies provided the same results in terms of comparison with dxa , and they all obtained similar ors , as reported in our study . 
only in the osteoporosis prevention using soy ( opus ) study [ 24 ] was a slight but significant area under the roc curve found for ad - sos when compared with lumbar bmd . 
 [ 26 ] reported very similar or values for ad - sos and ubpi compared with lumbar , distal radius and total - body bmd measurements in discriminating vertebral fractures but lower than those obtained using femoral neck and total hip bmd . the limitations of our study are mainly due to lack of information on important risk factors for osteoporosis unrelated to menopause , age and anthropometric variables . in conclusion , the ad - sos ultrasound parameter demonstrated sensitivity similar to lumbar dxa in discriminating postmenopausal women with osteoporotic vertebral fractures from those without fractures . pu essere dovuto a differenze nelle caratteristiche delle popolazioni in studio : bisogna notare che in tutti questi studi lo stesso risultato stato ottenuto in termini di confronto con la dxa ; infatti gli ors ottenuti in ogni studio fra le due metodiche sono risultati simili fra loro , esattamente come nel nostro studio . 
sartor springer - verlag berlin heidelberg , 2010 isbn 978 - 3 - 540 - 00818 - 7 e - isbn 978 - 3 - 540 - 68889 - 1 doi 10.1007 / 978 - 3 - 540 - 68889 - 1 published online : 8 march 2011 springer - verlag 2011 this is a very special book : it addresses a very dif cult , peculiar topic yet special ; special because the topic is treated with incredible ease , showing the authors profound knowledge of anatomy , clinical situations and ndings , diagnostic procedures and ensuing therapeutic options and end - results . 
 special , also , because the reader in case he is not aware or has poor knowledge of the subject must humbly start from scratch in general , review anatomy , in order to fully appreciate what is poured into the text . there are ten chapters addressing in 311 pages : historical considerations ; anatomy of the cavernous sinus ; classi cation of the cavernous sinus and dural arteriovenous stulas ; etiology , prevalence and natural history of dural cavernous sinus stulas ; neuro - ophthalmology in dural cavernous sinus stulas ; radiological diagnosis ; endovascular treatment ; alternative treatment options ; hemodynamic aspects of dural cavernous sinus stula plus a few summary pages at the end . the bulk of the book ( 176 pages ) includes two chapters on radiological diagnosis and endovascular treatment , where one will nd all possible information on how to properly diagnose and treat these malformations . impressive , among the other chapters , the one on neuroophthalmology : one will nd valuable information regarding signs and symptoms related to the underlying pathology . treatment options and devices to be used for this endeavour are described in depth with a special focus on transvenous embolization rather than the transarterial approach . 
besides high - quality angiographic equipment and suf cient training , profound knowlquesto un libro molto speciale : speciale perch il suo un argomento molto dif cile , eppure speciale ; speciale perch largomento trattato con incredibile facilit a dimostrazione della profonda conoscenza , da parte dellautore , dellanatomia , dei quadri e delle situazioni cliniche , delle procedure diagnostiche , delle conseguenti opzioni terapeutiche e dei loro risultati nali . 
libro speciale anche perch il lettore , in caso non ne sia informato o abbia poca conoscenza dellargomento , deve con umilt affrontarlo partendo dagli elementi di base , rivedendo le sue conoscenza di anatomia , per apprezzare in pieno tutto quanto viene profuso ed insito nel testo . dieci capitoli , per un totale di 311 pagine trattano i seguenti punti : considerazioni storiche ; anatomia del seno cavernoso ; classi cazione delle stole del seno cavernoso e delle stole arterovenose durali ; eziologia , prevalenza e storia naturale delle stole del seno cavernoso durale ; neuro - oftalmologia delle stole del seno cavernoso durale ; diagnosi radiologica ; trattamento endovascolare ; opzioni terapeuriche alternative ; aspetti emodinamici delle stole del seno cavernoso durale per terminare con alcune pagine di sommario nale . la parte del leone del volume ( 176 pagine ) rappresentata dai due capitoli che trattano della diagnosi radiologica e del trattamento endovascolare delle stole del seno cavernoso , capitoli in cui si troveranno tutte le possibili informazioni su come diagnosticare in modo corretto e poi trattare queste malformazioni . di notevole spessore ed importanza tra gli altri capitoli quello sulla neuro - oftalmologia : vi si troveranno assai utili informazioni circa i segni ed i sintomi alla base della patologia in questione . 
oltre ad una attrezzatura angiogra ca di alta qualit e ad una suf ciente preparazio674 radiol med ( 2011 ) 116 : 673674 edge of the vascular anatomy , including its angiographic appearance , remains the essential basis for successful and safe endovascular occlusion of cavernous sinus stulas as well as : good three dimensional understanding of the cavernous sinus are required for optimal use of tools and devices . i would , humbly , also add that when reading the book one needs or must , have a very good memory in order to properly recall the meaning of the enormous number of abbreviations ( two full pages at the beginning ) , used to tag vessels and other paraphernalia . regarding this last point , the author and springer should think about devising and providing some loose or hard bound pages to have on hand , to be used in the translation of abbreviations ( unless one has a pico della mirandolas memory ) instead of making the reader shuf e back and forth from the page with the shortening in question to the abbreviation list . anatomic , radiological , clinical images many in colour are of enviable quality : each caption for most of the compound gures is a tiny booklet in itself due to the precise , in depth speci cations . in summary this is a must have book for all those who deal with this sort of problem : interventional radiologists , neurosurgeons and neurologists , and optional for the general radiologist who wants to keep in touch with the advances in this peculiar eld of radiology . ne , una profonda conoscenza dellanatomia vascolare e del suo aspetto angiogra co , rimangono le basi essenziali per ottenere una occlusione endovascolare riuscita e sicura delle stole del seno cavernoso ed inoltre che : richiesta una buona comprensione dellaspetto tridimensionale del seno cavernoso per un uso ottimale degli strumenti e delle attrezzature . 
 vorrei umilmente aggiungere che leggendo il libro necessario o meglio si deve avere una buona memoria per ricordare in modo corretto il signi cato dellenorme numero di abbreviazioni ( due intere pagine di elenco allinizio del volume ! ) usate per indicare i vasi ed altri elementi accessori . a questultimo proposito sia lautore che la casa editrice dovrebbero pensare di realizzare alcune pagine sfuse o su cartoncino da avere sempre a disposizione per la traduzione / interpretazione delle abbreviazioni ( a meno che non si abbia una memoria da pico della mirandola ) in modo da evitare il continuo andare avanti ed indietro dalla pagina che riporta quelle in questione rispetto alla lista delle stesse . le immagini anatomiche , radiologiche , cliniche , di cui molte a colori , sono di una qualit invidiabile : ogni didascalia , per la maggior parte delle gure composte , un piccolo trattatello a s stante , date le informazioni precise ed accurate che vi si ritrovano . in conclusione , questo un libro da possedere , obbligatorio per tutti coloro che si occupano di questo tipo di problemi : radiologi interventisti , neurochirurghi e neurologi ; facoltativo per il radiologo generale che si vuol tenere in contatto con i progressi in questo campo particolare della radiologia . 
simonetti dipartimento di diagnostica per immagini ed imaging molecolare , radioterapia e radiologia interventistica , fondazione policlinico universitario tor vergata ( ptv ) , viale oxford 81 , 00133 rome , italy correspondence to : e . 
eighteen female patients with a diagnosis of pelvic oor disorder ( physical examination and conventional defecography ) underwent dynamic mr defecography ( mrd ) with a 0.25 - t tilting mr system ( g - scan , esaote )  . 
diciotto pazienti donne con diagnosi di patologia del pavimento pelvico ( esame clinico e defecogra a convenzionale ) hanno eseguito una defecogra a con risonanza magnetica dinamica ( mrd ) , utilizzando un sistema di rm da 0 , 25 t ribaltabile ( g - scan , esaote )  . 
una buona qualit delle immagini stata ottenuta in 15 / 18 pazienti ; 3 pazienti hanno presentato gravi artefatti dovuti al movimento , 3 pazienti presentavano incontinenza che ha impedito gli studi funzionali . 
la mrd dinamica con un sistema di rm aperto a basso campo ribaltabile uno strumento radiol med ( 2011 ) 116 : 620633 keywords mr defecography pelvic oor disorders loweld mr tilt system mr attuabile e promettente per lo studio del pavimento pelvico . 
 parole chiave defecogra a rm patologia del pavimento pelvico rm a basso campo rm a decubito variabile introduction introduzione pelvic oor disorders encompass a spectrum of conditions that are very common in the general population , especially among women and in the older age groups [ 1 , 2 ] , and which greatly affect quality of life [ 3 ]  . 
pelvic oor disorders include a series of anatomical and functional changes affecting the three anatomical compartments of the pelvis : the anterior compartment , which comprises the bladder and the urethra ; the middle compartment , consisting of the uterus , the adnexa and the vaginal fornix ; and the posterior compartment , composed of the rectum and anal canal . 
a survey conducted on a sample of 1 , 200 , 000 italian women aged 5575 years found a prevalence of pelvic oor disorders of approximately 22% [ 4 ]  . 
although conventional defecography has considerably improved the diagnosis of evacuation disorders , the examination often proves inadequate in evaluating abnormalities affecting the other compartments [ 5 , 6 ]  . 
 magnetic resonance defecography ( mrd ) , although still an experimental technique , allows the study of the pelvic oor with the double advantage of sparing the patient exposure to ionising radiation and permitting optimal evaluation of soft tissues and support structures of the pelvic organs . the aim of this study was to investigate the possibility of using an open - con guration , loweld ( 0.25 t ) , tilting mr system normally used for imaging the lumbar spine and knee under weight - bearing conditions in evaluating pelvic oor disorders and to compare results obtained in the same individual but imaged from the supine and orthostatic positions . le disfunzioni del pavimento pelvico rappresentano uno spettro di patologie largamente diffuse nella popolazione , in particolare nel sesso femminile e nelle fasce di et pi avanzate [ 1 , 2 ] , e in uenzano in maniera determinante la qualit di vita dei soggetti che ne soffrono [ 3 ]  . 
tali disturbi comprendono una serie di alterazioni anatomiche e funzionali a carico dei tre compartimenti anatomici della pelvi : il compartimento anteriore , che comprende vescica e uretra ; il compartimento medio , costituito dallutero , dagli annessi e del fornice vaginale ; il compartimento posteriore , formato dal retto e dal canale anale . 
in italia uno studio effettuato su un campione di 1.200.000 donne det compresa tra i 55 e 75 anni ha documentato una prevalenza delle disfunzioni del pavimento pelvico pari a circa il 22% [ 4 ]  . 
la defecograa convenzionale ha migliorato notevolmente la diagnosi dei disturbi della defecazione , ma risulta spesso inadeguata alla valutazione delle anomalie degli altri compartimenti [ 5 , 6 ]  . 
la defeco - risonanza magnetica ( rm ) ( mrd ) seppur rivesta ancora un ruolo sperimentale , consente lo studio del pavimento pelvico e presenta il duplice vantaggio di evitare lesposizione dei pazienti a radiazioni ionizzanti e quello di una ottimale valutazione dei tessuti molli e delle strutture di supporto degli organi pelvici . scopo di questo studio quello di esaminare la possibilit di utilizzare , nella valutazione dei disturbi del pavimento pelvico , un sistema di rm aperto , a basso campo ( 0 , 25 t ) e a decubito variabile , dedicato usualmente alle studio del rachide lombare e del ginocchio sotto carico , confrontando i risultati ottenuti nello stesso soggetto in decubito supino ed in ortostasi . materials and methods patients materiali e metodi pazienti eighteen patients presenting with symptoms due to pelvic oor disorders were enrolled between october 2009 and april 2010 . 
 only two women were nulliparous , and one woman had had a hysterectomy . nel periodo compreso fra ottobre 2009 e aprile 2010 sono stati arruolati nello studio 18 pazienti che riferivano sintomi da disfunzioni del pavimento pelvico . 
tutti i soggetti riferivano sintomi clinici ( tabella 1 ) e da ciascuno di loro stato tabella 1 sintomatologia clinica dei pazienti sottoposti allo studio table 1 clinical symptoms in our patients 622 symptom sense of incomplete evacuation pain during defecation faecal incontinence chronic constipation sintomo senso di incompleta evacuazione dolore durante defecazione incontinenza fecale stipsi cronica imaging techniques mr colpocystodefecography patients , n 10 / 18 9 / 18 3 / 18 12 / 18 pazienti , n 10 / 18 9 / 18 3 / 18 12 / 18 the mr examinations were performed on an open - con guration , tilting - gantry , permanent magnet with a stationary magnetic eld of 0.25 t , a dynamic gradient strength of 20 mt / m and a slew rate of 25 mt / m / s ( g - scan , esaote , italy ) and passive shimming . 
the receiver coil was a lumbar spine dpa surface coil consisting of a rigid base ( width 320 mm , depth 280 mm , height 45 mm ) and a exible belt available in two sizes ( large , 8918.5 cm ; small , 6918.5 cm ) to t the dimensions of the individual to be studied . 
prior to the study , the patients rectum was lled with approximately 200 ml of suspension medium containing 1 ml of gadobutrol paramagnetic contrast medium ( gadovist 1.0 mol / l , bayer schering ag , berlin , germany )  . 
three different suspensions were used : sonographic gel ( n = 2 ) , a psyllium bre compound ( psyllogel ) ( n = 2 ) and mashed potatoes ( prepared by adding water to different commercial products in the examination room ) ( n = 4 )  . 
the bladder was opaci ed with 180 ml of saline solution added to 3 ml of gadobutrol contrast medium ( gadovist 1.0 mol / l , bayer schering ) after having inserted a 16 - french , two - way foley catheter during the examination . 
uno dei soggetti in esame aveva subito unisterectomia . tecniche di imaging colpo - cisto - mrd gli esami rm sono stati eseguiti su magnete permanente aperto a decubito variabile con campo magnetico stazionario di 0 , 25 t gradienti dinamici con potenza di 20 mt / m e slew rate di 25 mt / m / s ( g - scan , esaote , italia ) e shimming passivo . 
il tavolo del magnete provvisto di un meccanismo di ribaltamento da 0 a 90 con passi di 2 che ha consentito lo studio del paziente in decubito supino ed ortostatico . 
 come bobina di ricezione stata utilizzata una bobina di super cie lombar spine dpa , costituita da una base rigida ( lunghezza [ l ] profondit [ p ] altezza [ h ] = 320 mm280 mm45 mm ) e una fascia essibile anteriore di dimensioni variabili ( fascia grande 8918 , 5 cm ; fascia piccola 6918 , 5 cm ) in funzione della taglia del soggetto in esame . 
prima dellesame il retto dei soggetti in esame stato riempito con circa 200 ml di mezzo di sospensione unito ad 1 ml di mezzo di contrasto paramagnetico gadobutrolo ( gadovist 1 , 0 mol / l , bayer schering ag , berlin , germania )  . 
 sono state utilizzate 3 diverse sospensioni : gel ecogra ci ( n = 2 ) , composto di bre ( psyllogel ) ( n = 2 ) , purea di patate ( sono stati utilizati vari prodotti commerciali preparati in sede di esame mediante aggiunta di acqua ) ( n = 4 )  . 
stata opacizzata anche la vescica mediante 180 ml di soluzione siologica unita a 3 ml di mezzo di contrasto paramagnetico gadobutrolo previo posizionamento di catetere foley a doppia via da 16 french , lasciato in sede durante lesame . 
lo studio statico ha previsto lutilizzo sui tre piani ortogonali dello spazio di sequenze 3d hybrid contrast enhanced ( hyce ) , gradient echo ( ge ) bilanciata con le seguenti caratteristiche : tempo di ripetizione ( tr ) 10 ms ; tempo di eco ( te ) 5 ms ; ip angle ( fa ) 90 ; strati 20 ; spessore di strato 2 , 5 mm ; campo di vista ( fov ) 280280 ; matrice 200160 . 
sono state inoltre acquisite immagini statiche sul piano sagittale durante rilassamento , contrazione s nteriale e ponzamento , mediante sequenze ge t1 - pesate con le seguenti caratteristiche : tr 35 ms ; te 10 ms ; fa 90 ; atrati 1 ; spessore di strato 5 , 5 mm ; fov 300300 ; matrice 192128 . 
in ne stato condotto lo studio dinamico durante evacuazioradiol med ( 2011 ) 116 : 620633 static study included acquisition of 3d hybrid contrast - enhanced ( hyce ) gradient echo ( ge ) sequences and three orthogonal spatial planes with the following parameters : repetition time 10 ms ; echo - train length 5 ms ; ip angle 90 ; slices 20 ; slice thickness 2.5 mm ; eld of view 280280 ; matrix , 200160 . 
static images were also acquired in the sagittal plane at rest and during sphincter contraction and straining using t1 - weighted ge sequences with the following parameters : repetition time 35 ms ; echo - train length 10 ms ; ip angle 90 ; slices 1 ; slice thickness 5.5 mm ; eld of view 300300 ; matrix 192128 . 
finally , a dynamic study was performed during rectal evacuation using an axial t1weighted ge sequence with the following parameters : repetition time 30 ms ; echo - train length 6 ms ; ip angle 90 ; slices 1 ; slice thickness 5.5 mm ; eld of view 300300 ; matrix 192128 ; acquisition time 3 s / image . 
overall mr room time for the examinations in the two patient positions , and including re lling of the rectum , was approximately 68 ( range 4293 ) min . image analysis mr images acquired in the sagittal plane were analysed by two radiologists who took the measurements separately . 
to allow measurement standardisation and determine severity of the pelvic oor disorder , we considered the pubococcygeal line ( pcl ) , which delimits the base of the pelvic oor and extends from the inferior border of the pubic symphysis and the last coccygeal joint . 
to evaluate pelvic oor laxity , measurements of the h and m lines were obtained : the h line is measured by tracing a line from the inferior border of the pubic symphysis to the posterior wall of the rectum at the anorectal junction level . 
this line represents the most caudal portion of the levator ani complex ( puborectalis muscle ) and corresponds to the puborectal hiatus , which allows grading of the maximal widening in the anteroposterior direction of the pelvic sling during straining . 
the m line exceeding 2 cm was considered pathological . organ prolapse was de ned as protrusion of any organ ( bladder , urethra , vagina , small bowel ) through the h line . 
anterior rectocele was quanti ed by prolonging upwards to the level of the rectum the tangent to the anterior wall of the anal canal and measuring the disne dellampolla rettale mediante sequenza ge t1 - pesata orientata sul piano sagittale con le seguenti caratteristiche : tr 30 ms ; te 6 ms ; fa 90 ; strati 1 ; spessore di strato 5 , 5 mm ; fov 300300 ; matrice 192128 ; tempo di acquisizione 3 s / immagine . 
il tempo complessivo di occupazione della macchina per la completa acquisizione dellesame nei due decubiti , compreso il secondo riempimento del retto , stato in media di 68 minuti ( range 4293 minuti )  . analisi delle immagini le immagini rm acquisite sul piano sagittale sono state analizzate da due radiologi che hanno effettuato separatamente le rispettive misurazioni . 
per consentire una standardizzazione delle misure e per determinare la gravit delle disfunzioni del pavimento pelvico stata identi cata la linea pubo - coccigea ( lpc ) , delimitante la base del pavimento pelvico , tesa tra il margine inferiore della sin si pubica e lultima articolazione del coccige . 
al ne di valutare la lassit del pavimento pelvico abbiamo misurato la linea h e la linea m : la linea h misurata tracciando una linea dal margine inferiore della sin si pubica alla parete posteriore del retto a livello della giunzione ano - rettale e rappresenta la porzione pi caudale del gruppo dei muscoli elevatori dellano ( muscolo pubo - rettale ) ; inoltre , essa corrisponde allo iato pubo - rettale , che consente la massima apertura in senso antero - posteriore dellanello pelvico durante il ponzamento . 
in accordo con i dati in letteratura abbiamo considerato lampliamento dello iato puborettale patologico quando la linea h supera la lunghezza di 6 cm [ 7 ] ; la linea m si estende perpendicolarmente dal piano della lpc alla ne della linea h . 
abbiamo considerato patologica una lunghezza della linea h superiore ai 2 cm . abbiamo considerato il prolasso come la protrusione di qualsiasi organo ( vescica , uretra , vagina , piccolo intestino ) attraverso lo iato pubo - rettale ( linea h )  . 
la quanti cazione del rettocele anteriore avvenuta prolungando superiormente a livello del retto la tangente alla parete anteriore del canale anale e misurando la distanza tra tale linea e la parete anteriore del bulging nel punto di maggiore ampiezza . 
abbiamo considerato patologico un rettocele di almeno 2 cm [ 7 ]  . qualit delle immagini abbiamo valutato la qualit delle immagini analizzando il rapporto segnale / rumore ed il livello di artefatti mediante 624 radiol med ( 2011 ) 116 : 620633 tance between this line and the anterior wall of the rectal bulge at the point of maximum depth . 
we considered a rectocele of at least 2 cm to be pathological [ 7 ]  . image quality image quality was evaluated by analysing the signal - tonoise ratio ( snr ) and the severity of artefacts on a qualitative scale from 1 to 3 . 
snr was scored 1 if the noise was greater than the signal , 2 if noise and signal were equivalent and 3 if the signal was greater than the noise . 
artefact severity was scored 1 if no artefacts or only minor artefacts were present , 2 if there were artefacts of intermediate severity and 3 in the event of major or severe artefacts . 
these evaluations were performed on both static images obtained with the balanced 3d hyce ( at baseline ) and t1 - weighted gradient echo sequences ( at rest , during contraction and straining ) , and on the single dynamic images . 
riguardo al rapporto segnale / rumore , stato attribuito un punteggio di 1 se il rumore risultava superiore al segnale , 2 in caso di parit e 3 se il segnale era superiore al rumore . 
per quanto riguarda il livello di artefatti , stato assegnato un punteggio di 1 in caso di artefatti minori o assenti , 2 se erano presenti artefatti di grado medio e 3 in caso di artefatti maggiori o gravi . 
tali valutazioni sono state effettuate sia sulle immagini statiche ottenute con le sequenze 3d - hyce bilanciate ( basale ) e ge t1 - pesate ( rilassamento , contrazione e ponzamento ) , sia sulle singole immagini dinamiche . 
ci nonostante , le valutazioni effettuate sul rapporto segnale / rumore e sul livello di artefatti , sono state soddisfacenti per tutte le tipologie di immagini , anche se punteggi inferiori sono stati ottenuti dalle immagini dinamiche ( tabelle 2 e 3 )  . 
 table 3 evaluation of artefacts patient 3d - hyce rest contraction straining cine ( mean ) radiol med ( 2011 ) 116 : 620633 626 mean media hyce , hybrid contrast - enhanced sequence tabella 3 valutazione del livello di artefatti paziente 3d - hyce rilassamento contrazione ponzamento cine ( media ) 1.4 1 , 4 1.5 1 , 5 1.6 1 , 6 1.4 1 , 4 hyce , hybrid contrast - enhanced sequence pelvic oor laxity and anterior rectocele , and compared the results obtained in the orthostatic and supine position . 
the supine position resulted in an underestimation of all disorders : in particular , six bladder prolapses were missed , which were graded as mild in the orthostatic position , whereas two moderate prolapses in the orthostatic position were graded as mild in the supine position . 
sono evidenti bolle daria nelle immagini b e c ma soprattutto in b . moderate prolapses in the orthostatic position , one of which was graded as mild it the supine position ; and three mild prolapses in the orthostatic position , which were all missed in the supine position . 
five cases of severe pelvic oor laxity were graded as severe in the orthostatic position , one of which was underestimated as moderate in the supine position ; one case of moderate laxity in the orthostatic position was graded as mild in the supine position ; and two cases graded as mild laxity in the orthostatic position were missed in the supine position . 
of the 11 anterior rectoceles classied as severe in the orthostatic position , only eight were also graded as severe in the supine position ; three severe and one moderate anterior rectocele were underestimated , whereas one mild rectocele in the orthostatic position was missed in the supine position ( table 4 )  . discussion the true prevalence of pelvic oor disorders is underestimated , as these disorders tend to remain asymptomatic no . 
cinque lassit del pavimento pelvico sono risultate gravi in ortostasi ed 1 stata sottostimata moderata in supino , 1 valutata di grado moderato in ortostasi stata sottostimata lieve in decubito supino e 2 lievi in ortostasi misconosciute in supino . 
degli 11 rettoceli anteriori osservati , classi cati come gravi in decubito ortostatico , solo 8 sono altrettanto severi in supino ; 3 gravi ed 1 moderato sono stati sottostimati , mentre 1 rettocele misconosciuto in decubito supino risultato lieve in ortostasi ( tabella 4 )  . 
 discussione la reale prevalenza delle disfunzioni del pavimento pelvico sottostimata in quanto tali patologie sono spesso asintomatiche per lunghi periodi o paucisintomatiche ( dolore pelvico , senso di peso , sensazione di incompleta evacuazione ) soprattutto in caso di iniziale prolasso degli organi pelvici [ 1 , 2 , 8 ]  . 
lesame sico inoltre spesso insuf ciente e difcoltoso per una completa valutazione anatomica e funzionale della pelvi [ 9 ]  . radiol med ( 2011 ) 116 : 620633 628 fig . 
le immagini ottenute con psyllogel ( b ) e gel ecogra co ( c ) forniscono una ottimale intensit di segnale ma nella fase evacuativa non consentono una suf ciente dilatazione del canale anale lasciandolo liforme ( punte di freccia )  . or poorly symptomatic ( pelvic pain , sense of weight , feeling of incomplete evacuation ) for years , especially in the early stages of pelvic organ prolapse [ 1 , 2 , 8 ]  . 
moreover , physical examination is often dif cult and inadequate for a complete anatomical and functional assessment of the pelvis [ 9 ]  . preoperative planning is based on clinical assessment and data provided by conventional defecography , in some cases supplemented by mrd . 
previous published studies have been conducted with closed - con guration , higheld ( 1.5 - t ) systems and t2 - weighted multiplanar acquisitions , with the patient in the supine position or lateral decubitus with exed knees [ 1012 ]  . 
the development of open - con guration 0.5 - t systems with dedicated supports and suf ciently wide gantry aperture has allowed mrd examinations of the patient in a sitting position [ 13 , 14 ]  . 
all published studies comparing mrd performed with the two patient positions have therefore been conducted using difil planning pre - operatorio si basa sulla visita clinica e sui dati forniti dalla defecogra a tradizionale , coadiuvati talvolta da quelli ottenuti con la defeco - rm . 
i lavori riportati in letteratura sullargomento sono stati eseguiti su magnete chiuso ad alto campo ( 1 , 5 t ) ed acquisizioni t2 pesate su multipli piani dello spazio , con paziente in decubito supino o posto sul anco a ginocchia esse [ 1012 ]  . 
la realizzazione di magneti aperti da 0 , 5 t , dotati di supporti dedicati e apertura del gantry suf cientemente ampia , ha permesso di eseguire lo studio defeco - rm con paziente in posizione seduta [ 13 , 14 ]  . gli studi nora pubblicati in letteratura per la valutazione comparativa degli esami defeco - rm in due differenti decubiti utilizzano pertanto magneti a diversa intensit del campo magnetico stazionario ( 1 , 5 t per il decubito supino e 0 , 5 t per la posizione seduta )  . 
questo , a nostro parere , rappresenta un limite per limpossibilit di compararne i risultati a causa delle differenti performance dei due magneti e radiol med ( 2011 ) 116 : 620633 fig . 
images obtained in the orthostatic position at rest ( a ) , during contraction ( c ) and straining ( e ) and during the same phases in the supine position ( b , d , f )  . 
immagini ottenute in ortostatismo a riposo ( a ) , durante contrazione ( c ) e ponzamento ( e ) ed in posizione supina nelle medesime condizioni ( b , d , f )  . 
il prolasso risulta evidente in fase di ponzamento ma solamente in ortostatismo ( frecce )  . ferent magnetic eld strengths ( 1.5 t for supine decubitus and 0.5 t for the sitting position )  . 
this is a limitation , in our opinion , that precludes comparison of results owing to the different performance of the two magnets and the sequences used [ 13 , 15 ]  . in our study , we used a new open - con guration permanent magnet with a 0.25 - t stationary magnetic eld equipped with a 0 - 90 tilting table , which allowed us to apply the same imaging protocol in the two patient positions . 
nel nostro studio abbiamo utilizzato un magnete permanente aperto di nuova concezione con campo magnetico stazionario di 0 , 25 t , equipaggiato con tavolo ribaltabile da 0 a 90 , che ha consentito di eseguite lo stesso protocollo desame nei due differenti decubiti . 
lesame defeco - rm in ortostasi stato inoltre acquisito con tavolo inclinato a 80 per aumentare la stabilit del soggetto in esame e ridurre gli artefatti da movimento indotti dalla stazione eretta . analogamente allo studio defecogra co convenzionale , sono state acquisite sequenze statiche in fase di riposo , contrazione e ponzamento . 
la possibilit di studiare la fase evatable 4 results obtained in the upright and supine positions condition mild moderate severe total upright supine upright supine upright supine upright supine radiol med ( 2011 ) 116 : 620633 630 bladder pse vaginal prolapse rectal pelvic oor laxity ctocele anterior pse prola prola escicale prolasso aginale prolasso ettale prolasso lassit del pavimento 2 ante rettocele riore tabella 4 valutazione dei reperti ottenuti rispettivamente in ortostasi ed in posizione supina patologia lieve moderato grave totale ortostasi supino ortostasi supino ortostasi supino ortostasi supino patient stability and reduce movement artefacts resulting from the standing position . as in conventional defecography , static sequences were acquired with the patient at rest , during contraction and while straining . 
the possibility of studying the evacuation phase appears essential for increasing diagnostic accuracy of the examination , providing complete clinical assessment and guiding appropriate patient management , given that some pathological ndings are underestimated in the static images acquired during straining . 
the three suspensions we used have different density and texture and , although all three can be used , we found that mashed potatoes achieve greater opening of the anal canal and thus a more accurate assessment of any disorder . 
the suspensions composed of sonographic gel and psyllogel have optimal signal intensity but fail to dilate the anal canal suf ciently in the evacuation phase , leaving it liform , which makes it dif cult , albeit possible , to carry out assessments according to the methods used . 
in our experience , this feature makes it the best medium by which to obtain opacication in our experience . because the mr system we used does not provide steady - state free precession ( balanced ) sequences , which are commonly used for the evacuation phase , we adapted the t1 - weighted turbo eld - echo sequences . 
a reasonable cuativa appare indispensabile per aumentare laccuratezza diagnostica e fornire un completo quadro clinico ed un corretto inquadramento terapeutico del paziente , poich alcuni reperti patologici risultano sottostimati nelle acquisizioni statiche in fase di ponzamento . 
le tre sospensioni utilizzate , hanno una differente densit e consistenza e nonostante risulti possibile utilizzare tutte e tre le sospensioni abbiamo dimostrato come la purea di patate abbia una maggiore capacit di far aprire il canale anale , consentendo una valutazione pi accurata delle eventuali patologie presenti . 
le sospensioni composte dal gel ecogra co e dallo psyllogel danno una ottimale intensit di segnale , ma nella fase evacuativa non dilatano suf cientemente il canale anale lasciandolo liforme , ci rende dif coltoso , seppur possibile , fare le dovute valutazioni secondo i metodi utilizzati . 
 questa sua caratteristica che lo rende nella nostra esperienza il mezzo di opacizzazione migliore . non essendo per il momento disponibili sul magnete utilizzato sequenze di tipo steady state free precession ( balanced ) , attualmente in voga per la fase evacuativa , stato necessario adattare le sequenze turbo eld echo ( tfe ) t1 pesate . 
un compromesso ragionevole fra la risoluzione spaziale , risoluzione temporale e lintensit del segnale ha consentito lottimizzazione della sequenza dinamica utilizzata nella fase evacuatoria con tempi di acquisizione di 3 s / immagine . 
una migliore risoluzione temporale potrebbe proradiol med ( 2011 ) 116 : 620633 compromise between spatial resolution , temporal resolution and signal intensity allowed us to optimise the dynamic sequence used in the evacuation phase with acquisition time of 3 s / image . 
a better temporal resolution could probably be obtained by constructing speci c mrd sequences that do not require calibration between one image and the next and with a suf cient snr to reduce acquisition times , as well as by developing dynamic ( balanced ) steady - state free precession sequences . 
moreover , axial images allowed widening of the puborectal hiatus to be assessed in evaluating pelvic oor laxity . in agreement with previous reports , the comparison of results obtained with the two different patient positions showed that the supine decubitus resulted in an underestimation of the severity of all disorders [ 7 , 11 ] ( table 4 )  . 
in our series , only three out of 18 patients were able to complete the mrd examination in the supine position , whereas all patients succeeded in performing the evacuation phase in the orthostatic position . for quantitative image analysis , we used the h line , m line and organ prolapse with respect to the h line ( hmo ) system in order to de ne , differentiate and grade the severity of organ prolapse and pelvic oor musculature laxity ( table 2 ) [ 1013 , 16 ]  . 
comparison of prolapses and anterior rectocele severity seen in the two imaging positions showed that the supine position resulted in an underestimation in all patients ( table 4 )  . 
the different results of the mrd examination in the two positions are most likely related to the direction of the force of gravity exerted along a vertical axis , bearing completely on the muscularfascial structures of the pelvic oor in the orthostatic position , and along an anteroposterior axis in the supine position . 
in the latter position , the force of gravity is not exerted directly on the pelvic oor , and the underestimation of ndings is related to the fact that the only force bearing on the pelvic oor in the craniocaudal direction is that of bearing down with the abdominal muscles during straining and evacuation . 
our ndings demonstrate that mrd in the orthostatic position , even though not physiological , allows for better evaluation of pelvic oor disorders compared with the patient in the supine position . 
this was due to the con guration of the mr system , which was devised for dynamic osteoarticular studies and is not compatible with a dedicated support due to lack of space ( 35 cm )  . 
a further limitation is related to the sequences used and the relatively babilmente essere facilmente ottenibile grazie alla costruzione di sequenze speci che per lesame defeco - rm esenti dalla calibrazione fra unimmagine e laltra e con rapporto segnale / rumore suf ciente a ridurre i tempi di acquisizione e dalla messa a punto di sequenze dinamiche di tipo steady state free precession ( balanced )  . 
le immagini orientate sul piano assiale hanno inoltre permesso di valutare lo slargamento dello iato pubo - rettale in caso di lassit del pavimento pelvico . nella nostra casistica , in accordo con i dati in letteratura , la comparazione dei risultati nei due differenti decubiti , ha mostrato nel decubito supino una sottostima della gravit per tutte le patologie osservate ( tabella 4 ) [ 7 , 11 ]  . 
un ulteriore limite del decubito supino consiste nella dif colt ad effettuare la fase evacuativa , che risulta invece di fondamentale importanza per un corretto inquadramento clinico - diagnostico del paziente . 
nella nostra casistica infatti solamente 3 soggetti su 8 arruolati sono stati in grado di completare lesame defeco - rm in decubito supino , mentre tutti i soggetti sono riusciti ad effettuare la fase evacuativa in ortostatismo . per lanalisi quantitativa delle immagini ottenute stato utilizzato il sistema hmo ( linea h , linea m e prolasso degli organi pelvici rispetto alla linea h ) , al ne di de nire , differenziare e valutare la gravit del prolasso degli organi pelvici e la lassit della muscolatura del pavimento pelvico stesso ( tabella 2 ) [ 1013 , 16 ]  . 
confrontando la gravit dei prolassi e dei rettoceli anteriori riscontrati nei due decubiti , abbiamo osservato una sottostima del decubito supino in tutti i pazienti ( tabella 4 )  . 
i differenti risultati fra gli esami rm nei due decubiti sono da correlare verosimilmente alla direzione della forza gravitazionale che viene esercitata secondo un asse verticale in ortostasi , gravando interamente sulle strutture muscolo - fasciali del pavimento pelvico , e secondo un asse antero - posteriore in decubito supino . 
in questultimo decubito la forza gravitazionale non viene esercitata direttamente sul pavimento pelvico e la sottostima dei reperti legata al fatto che lunica forza diretta verso il pavimento pelvico in senso cranio - caudale quella del torchio addominale durante ponzamento ed evacuazione . 
i nostri dati dimostrano che lo studio rm in posizione ortostatica , sebbene non siologica , consente una migliore valutazione delle patologie del pavimento pelvico rispetto allesame rm con paziente in decubito supino . 
 il principale limite del nostro studio stato limpossibilit di valutare il paziente in posizione seduta in quanto la conformazione della macchina , concepita per lo studio dinamico osteo - articolare , ha impedito , a causa dellesiguo spazio ( 35 cm ) , di adattare un supporto dedicato . 
the speci cally adapted dynamic sequences do not have optimal temporal resolution , and the presence of a calibration interval between frames could lead to an underestimation of the more transient ndings . 
in addition , the possibility of acquiring only one 5.5 - mm slice during the dynamic phase required not only absolute patients immobility throughout the examination , but also extreme operator precision in setting the geometrical parameters to achieve perfect centring of the axis of the anal canal . 
the use of t1 - weighted sequences in the dynamic study made it necessary to opacify the bladder , vagina and rectum , resulting in increased costs , greater patient discomfort and longer examination time . le sequenze dinamiche adattate allo scopo non possiedono una ottimale risoluzione temporale e la presenza di un intervallo di calibrazione tra un frame ed il successivo potrebbe determinare una sottostima dei reperti pi fugaci . 
la possibilit di acquisire un solo strato di 5 , 5 mm in fase dinamica ha inoltre reso obbligatoria non solo lassoluta immobilit del paziente durante tutto lesame , ma anche una estrema precisione delloperatore nellimpostazione dei parametri geometrici al ne di centrare perfettamente lasse del canale anale . 
lutilizzo di sequenze t1 pesate nello studio dinamico ha reso , inoltre , indispensabile lopacizzazione della vescica , della vagina e del retto , con conseguente aumento dei costi dellesame , del disagio dei pazienti e del tempo complessivo dellesame . conclusions mrd with a permanent 0.25 - t magnet is feasible and provides high diagnostic quality . 
the study in the orthostatic position is more accurate for evaluating pelvic oor disorders compared with the supine position , which may be hampered by dif culties completing the evacuation phase . 
the hmo measurement system in evaluating pelvic oor disorders appears to be the most reliable method ; by evaluating separately two distinct and often coexisting pathological entities ( pelvic oor relaxation and organ prolapse ) , it allows a more accurate clinical assessment and therefore provides information that is vital for selecting the most appropriate treatment strategy . 
 the continuous technological improvements , especially in dedicated dynamic t2 sequences , will improve image diagnostic quality while reducing examination times . conclusioni lo studio defeco - rm risulta fattibile e di elevata qualit diagnostica con un magnete permanente da 0 , 25 t . 
lo studio in posizione ortostatica risulta pi accurato nella valutazione delle patologie del pavimento pelvico rispetto allesame in decubito supino , talvolta in ciato dalla dif colt a completare la fase evacuatoria . 
il sistema di misurazione hmo nella valutazione delle disfunzioni del pavimento pelvico appare , a nostro parere , il metodo pi af dabile perch , valutando separatamente due entit patologiche distinte e spesso coesistenti ( lassit del pavimento e prolasso degli organi ) , consente un pi corretto inquadramento clinico e fornisce quindi informazioni indispensabili per la scelta della migliore strategia terapeutica . 
mdct - ca provides parameters of cardiac function comparable to those found in echocardiography . mdct - ca although used primarily for coronary noninvasive imaging can provide additional information on riassunto obiettivo . 
sono stati analizzati per entrambe le metodiche i seguenti parametri comunemente campionati in ecocardiografia e correlati con quelli ottenuti in actcms : spessore del setto , spessore della parete posteriore , diametro dellaorta ascendente , diametro e volume tele sistolico e tele diastolico , frazione di eiezione , stroke volume , gittata cardiaca e massa cardiaca . 
stata riscontrata una buona correlazione tra le misure dello spessore del setto ( r = 0 , 470 e p = 0 , 001 ) e del diametro dellaorta ascendente ( r = 0 , 777 e p < 0 , 001 ) in ecografia e in tc , mentre una scarsa correlazione tra le misure dello spessore della parete posteriore ( r = 0 , 243 e p = 0 , 104 )  . 
la tcms ha sovrastimato in modo consistente i valori medi dei volumi rispetto allecocardiografia ma i volumi tele diastolico e tele sistolico derivati dalla 2dse e dalla actcms hanno mostrato una correlazione significativa ( rispettivamente r = 0 , 456 e p = 0 , 002 ; r = 0 , 640 e 506 radiol med ( 2011 ) 116 : 505520 ventricular function useful to the diagnostic workup of cardiac patients . keywords mdct coronary angiography ventricular function left ventricle parameters ejection fraction cardiac failure p < 0 , 001 )  . 
come indicatore di funzione sistolica globale del ventricolo sinistro ( vs ) , la frazione di eiezione ( fe ) misurata tramite tcms o ecocardiografia ha mostrato uneccellente correlazione ( r = 0 , 626 e p < 0 , 001 )  . 
la ac - tcms sebbene utilizzata prevalentemente per limaging non invasivo delle arterie coronarie , pu fornire informazioni aggiuntive allo studio delle coronarie utili al work up diagnostico dei pazienti con patologie coronariche e cardiache . 
 parole chiave angiografia coronarica tcms funzione ventricolare parametri ventricolari sinistri frazione di eiezione scompenso cardiaco introduction introduzione morbidity and mortality for cardiac pathologies have an inverse correlation with global left ventricular ( lv ) systolic function [ 1 , 2 ] as preserved ventricular function represents the most important prognostic factor in the short and long ter in routine clinical cardiology practice , critical decision - making such as defibrillator implantation , biventricular pacing and treatment of congestive heart failure is heavily based on ejection fraction ( ef )  . 
for decades , the 2d nature of ultrasound ( us ) imaging has affected the quantification of lv size and function by errors that stemmed mainly from foreshortened views and inaccurate geometric modelling . 
the inadequacy of this methodology has been demonstrated by several investigators who compared 2d echocardiographic ( ecg ) measures against magnetic resonance imaging ( mri ) reference [ 4 ]  . 
 recent multidetector computed tomography ( mdct ) scanners have been introduced in cardiac imaging to provide accurate and reproducible noninvasive visualisation of the coronary tree [ 5 , 6 ]  . 
however , these scanners not only provide a morphological visualisation of the coronaries but also a comprehensive evaluation of the heart during the heart cycle . these scanners are capable of continuous volumetric imaging of the beating heart allowing highly reproducible quantification of ventricular size and function . 
image reconstructions are easily obtained in each phase of the heart cycle from the diastolic to the systolic phase but are usually used only in order to assess the best data set for coronary evaluation , thus utilising only a small part of the large amount of information that is usually available . 
this technique has been increasingly la mortalit e la morbilit per malattie cardiache sono inversamente correlate con la funzione globale del ventricolo sinistro ( vs ) [ 1 , 2 ] dal momento che una funzione ventricolare preservata rappresenta il pi importante fattore prognostico a breve e lungo termine . 
nella pratica clinica cardiologica , la strategia terapeutica in situazioni critiche , come il posizionamento di un defibrillatore , di un pacemaker bi - ventricolare o il trattamento di uninsufficienza cardiaca congestizia principalmente basata sulla frazione deiezione ( fe )  . 
per decenni tale compito stato assolto dalla ecografia , limitata dalla natura bidimensionale dellimaging ecografico a causa di errori principalmente dovuti a poche proiezioni efficaci e allinaccuratezza del modello geometrico . 
linadeguatezza di questa metodica peraltro stata dimostrata da numerosi studi che hanno comparato i parametri ottenuti con lecocardiografia 2d con quelli di riferimento ottenuti con la risonanza magnetica [ 4 ]  . 
la valutazione qualitativa e quantitativa della funzione ventricolare rappresenta la pi comune applicazione dellecocardio nella pratica quotidiana . i pi recenti scanner di tomografia computerizzata multistrato ( tcms ) sono stati introdotti nello studio del cuore al fine di ottenere una visualizzazione accurata dellalbero coronarico , riproducibile , non invasiva [ 5 , 6 ]  . 
questi scanner sono in grado di effettuare un imaging volumetrico continuo del cuore , permettendo radiol med ( 2011 ) 116 : 505520 referred to as a potential tool for combined assessment of coronary anatomy , myocardial perfusion , and lv function [ 7 ] the purpose of this study was to compare global lv systolic function assessment by mdct with ecg in a routine cardiology practice setting . materials and methods patient population between april 2008 and september 2009 , 282 consecutive patients ( 178 men , mean age 64.02 years ) who underwent mdct coronary angiography ( mdct - ca ) for evaluation of coronary artery disease were considered . 
 patients selected for the study were subjected to mdctca according to indications of international guidelines [ 8 ] ( atypical chest pain , equivocal or nondiagnostic exercise test , follow - up of stents or bypass grafts )  . 
 mdct - ca protocol examination all patients included in the protocol were studied with a 64slice mdct scanner ( brilliance 64 , philips , best , the netherlands )  . 
the postcontrast scan was acquired by injecting 80 ml of a high - concentration iodinated contrast agent ( iomeron400 , bracco , milan , italy ) via the antecubital left arm vein at the rate of 5 ml / s followed immediately by a 40 - ml saline bolus . 
the acquisition protocol is summarised in table 2 . raw data obtained were used to retrieve ten different reconstruction datasets every 10% of the r - r interval ranging from systolic to diastolic phases of the cardiac cycle . 
 image analysis images obtained from data sets were analysed in consensus by a radiologist and a cardiologist with six years experience una quantificazione ben riproducibile della dimensione e della funzione ventricolare ; vengono ottenute ricostruzioni di immagini per ogni fase del ciclo cardiaco dalla fase diastolica alla fase sistolica ; normalmente vengono utilizzati solo i migliori dataset per la valutazione delle coronarie , usando quindi una minima parte delle molteplici informazioni generalmente disponibili . 
 la angiografia coronarica ( ac ) - tcms stata considerata sempre di pi , di fatto , come un potenziale strumento per la valutazione combinata della anatomia coronarica , della perfusione miocardica e della funzione del vs [ 7 ]  . 
 lo scopo di questo studio comparare la valutazione della funzione sistolica del vs mediante tcms con lecografia ( eco ) nellambito di una pratica cardiologica routinaria . materiali e metodi popolazione campione nel periodo compreso tra aprile 2008 e settembre 2009 , 282 pazienti ( 178 m , 104 f , et media 64 , 02 anni ) sono stati sottoposti ad ac - tcms per la valutazione di patologie delle arterie coronarie . 
per lo studio finale sono stati quindi considerati 116 pazienti . i pazienti selezionati per lo studio presentavano indicazioni cliniche contemplate nelle guide internazionali [ 8 ] , vale a dire pazienti con dolore toracico atipico , stress test non dirimenti o discordanti , pazienti in follow - up per stent e bypass . 
tutti i pazienti avevano eseguito in precedenza una studio ecocardiografico.il setting clinico della popolazione di pazienti riassunto in tabella 1 . i criteri di esclusione comprendevano insufficienza renale grave ( creatinina 120 mol / l ) , precedenti reazioni allergiche al mezzo di contrasto iodato , gravi malattie polmonari . 
sono stati esclusi quindi i pazienti con aritmie quali fibrillazione atriale cronica con risposta ventricolare elevata e flutter atriale , cos come pazienti con frequenti battiti prematuri atriali e ventricolari ; inoltre pazienti che sono stati sottoposti alla ac - tcms con sincronizzazione prospettica . ac - tcms : tecniche e metodi di indagine tutti i pazienti inclusi nel protocollo sono stati studiati mediante apparecchio con 64 detettori ( brilliance 64 , philips , best , olanda )  . 
images were postprocessed using the philips comprehensive cardiac package included in an off - line external workstation ( ebw64 , brilliance 64 , philips , best , the netherlands )  . 
 stato somministrato un mezzo di contrasto iodato alla concentrazione iodica di 400 mgi / ml ( iomeron 400 , bracco , milano , italia ) , per via endovenosa , attraverso una vena antecubitale del braccio sinistro mediante unagocannula da 1820 gauge somministrato al flusso di 5 ml / s , alla dose standard di 80100 ml seguito da un radiol med ( 2011 ) 116 : 505520 table 2 scan protocol , raw data reconstruction and contrast material administration imaging parameters scan detectors collimation ( mm ) kilovolt mas / slice rotation time ( ms ) scan time ( s ) temporal resolution reconstruction slice thickness ( mm ) reconstruction increment ( mm ) fov ( mm ) convolution filter / kernel contrast material volume ( ml ) flow rate ( ml / s ) iodine concentration [ i ] ( mgi / ml ) bolus chaser venous access 0.625 120 / 80 1201000 912 210 ms 250300 medium ( xcc ) 80 / 100 40 ml@5 ml / s antecubital tabella 2 parametri di scansione utilizzati nella acquisizione ac - tcms scansione detettori collimazione ( mm ) voltaggio ( kv ) amperaggio ( mas ) tempo di rotazione ( ms ) avanzamento ( mm / rot ) tempo per una scansione ( s ) ricostruzione spessore effettivo dello strato ( mm ) indice di ricostruzione ( mm ) campo di vista ( mm ) filtro di convoluzione finestra ( ampiezza / centro ) mezzo di contrasto volume ( ml ) velocit di somministrazione ( ml / s ) tempo di somministrazione ( s ) concentrazione [ i ] ( mgi / ml ) bolus chaser ( soluzione fisiologica ) accesso venoso 0 , 625 120 / 80 1201000 19 , 2 912 250300 medio ( xcc ) 600 / 200 80 / 100 40 ml@5 ml / s antecubitale using simpsons method [ 10 ]  . 
interobserver variability was calculated by means of kappa statistics . end - diastolic volume , end - systolic volume , stroke volume , cardiac mass , ef and cardiac output were automatically available on the biplane view . 
per ogni dataset sono stati tracciati automaticamente i contorni epicardico ed endocardico della cavit ventricolare sinistra in modo da ricavare i volumi del vs attraverso il metodo di simpson [ 10 ]  . 
la variabilit interoperatore stata calcolata tramite statistica k . il volume telediastolico , il volume telesistolico , lo stroke volume , la massa cardiaca , la frazione di eiezione e la portata cardiaca sono risultati cos disponibili per le ricostruzioni biplanari . 
gli operatori hanno misurato manualmente in una sezione sullasse corto , al di sotto del piano mitralico , sia lo spessore del setto interventricolare e della parete posteriore , sia i diametri tele diastolico e tele sistolico del vs . 
stato inoltre calcolato il diametro principale dellaorta ascendente . dalle ricostruzioni 2d e 4d ottenute mediante compattazione di ogni dataset in modalit cine gli operatori sono stati in grado di giudicare la cinetica di parete del ventricolo basandosi sul modello a 17 segmenti dellamerican heart association ( aha ) [ 10 ]  . 
tale modello si basa su una divisione del vs in tre porzioni sullasse corto : basale e media con 6 segmenti , apicale con 4 segmenti ; lapice considerato lultimo segmento . 
2a - d scansioni 2 camere e 4 camere ottenute in ac - tcms in a e b ed ecocardiografia in c e d che dimostrano la parete ventricolare sinistra assottigliata e la camera ventricolare dilatata . ters of septal thickness , posterior lv wall thickness and end - systolic and end - diastolic diameter . 
finally , the mean diameter of the ascending aorta above the valsalva sinuses ( sinotubular junction ) was calculated , as it is a constant parameter reported in each ecg examination . 
 from 2d and 4d cine views obtained by compacting lesame eco e lo studio con ac - tcms sono stati eseguiti radiol med ( 2011 ) 116 : 505520 fig . 
3 epicardial ( arrow ) and endocardial ( arrowhead ) automatic borders of the left ventricular ( lv ) cavity automatically traced to derive lv volume calculations using simpsons method . 
3 bordi automatici lungo la superficie epicardica ( freccia ) ed endocardica ( testa di freccia ) della parete ventricolare sinistra calcolati per valutare i volumi ventricolari con il metodi di simpson . 
 each reconstruction into cine mode , operators were able to judge the wall motion of the ventricle based on the 17segment model of the american heart association ( aha ) [ 10 ] , with six segments each in the basal and mid - lv section , four segments in the apical section and one segment representing the lv apex . 
 nellintervallo di tempo variabile da 1 giorno a un mese . la valutazione ecocardiografica della funzione del vs stata eseguita da un cardiologo esperto , in cieco rispetto ai risultati della ac - tcms . 
the frame at the peak of the r wave was determined as the end - diastolic frame , and the chamber size with the smallest dimension was determined as the end - systolic frame . 
septal thickness and posterior lv wall thickness , end - systolic and end - diastolic diameter and the mean diameter of the ascending aorta were also calculated in a submitral short - axis plane . 
a visual score of 1 if normal , 2 if hypokinetic , 3 if akinetic , 4 if dyskinetic was assigned to each segment . statistics categorical variables were presented as numbers and percentages . 
accuracy of mdct - ca compared with ecg considered as the reference standard was obtained by calculating sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv )  . 
mean heart rate during data acquisition was 62 bpm ranging from 5570 bpthe time required for image analysis of each data set ( including data retrieval ) ranged from 15 to 40 mmanual correction of the epicardial and endocardial borders was necessary to optimise the position of the boundaries in 82% of patients despite the overall good image sistolica . 
la frazione di eiezione stata calcolata dalle immagini convenzionali apicale , a 2 - camere , a 4 - camere , utilizzando il metodo area - lunghezza e un software disponibile in commercio ( ge prosolv analyzer )  . 
sono stati riportati il volume telediastolico , il volume telesistolico , lo stroke volume , la massa cardiaca , la frazione di eiezione e la portata cardiaca ; sono stati misurati in una sezione sullasse corto , al di sotto del piano mitralico , lo spessore del setto interventricolare e della parete posteriore del vs , i diametri tele diastolico e tele sistolico e il diametro principale dellaorta ascendente . 
dai cine 2d registrati , gli operatori hanno giudicato la cinetica del vs , basandosi sullo stesso modello usato in actcms . ad ogni segmento ottenuto stato assegnato un punteggio di 1 se normale , 2 se ipocinetico , 3 se acinetico , 4 se discinetico . analisi statistica le variabili categoriche sono state presentate come numeri e percentuali . 
laccuratezza della ac - tcms nei confronti delleco , lo standard di riferimento , stata ottenuta calcolando la sensibilit , la specificit , il valore predittivo positivo e il valore predittivo negativo . 
la frequenza media durante lacquisizione era di 62 bpm con un range di 55 - 70 bp il tempo necessario per lanalisi delle immagini di ogni dataset ( comprendente caricamento dati ) ha richiesto tra i 15 e i 40 minuti . 
il diametro telediastolico medio risultato di 52 , 82 mm , il diametro telesistolico di 37 , 87 m il volume telediastolico medio risultato di 160 , 61 ml , il volume telesistolico medio di 54.95 ml , la frazione di eiezione media ( lvef ) di 59 , 17% ( range 17%85% )  . 
lo stroke volume , la massa cardiaca e la portata cardiaca medi sono risultati rispettivamente di 81 , 48 ml , 95 , 73 g , radiol med ( 2011 ) 116 : 505520 quality of data sets . 
mean end - diastolic diameter was 52.82 mm and end - systolic diameter 37.87 mmean end - diastolic volume was 160.61 ml , end - systolic volume 54.95 ml and mean lvef 59.17% ( range 17%85% )  . 
mean aortic diameter was 32.94 mm ( range 1949.5 mm ) , mean septum thickness 8.83 mm ( range 2.515.5 mm ) and mean posterior wall 9.67 mm ( range 621 mm )  . 
the coefficient of agreement between operators and software in wall motion analysis was r = 0.7 echocardiography the time required for cine - loop analysis of each patient ranged from 5 to 20 mmean end - diastolic diameter was 52.24 mm and end - systolic diameter 31.57 mmean enddiastolic volume was 99.43 ml , end - systolic volume 43.81 and mean lvef 58.76% ( range 30%75% )  . 
mean aortic diameter was 35.53 mm ( range 2751 mm ) , mean septum thickness 11.03 mm ( range 715 mm ) and mean posterior wall 9.7 mm ( range 715 mm )  . 
the correlation between mdct - ca and ecg in end - diastolic volume , end - systolic volume , stroke volume , ef and cardiac output summarised in table 3 . 
according to blandaltman plots , there was a 74% mean difference between posterior wall on ecg and that on mdct - ca , 2.2% mean difference between interventricular septum , 7.7% between ascending aorta , 5.9% for end - diastolic diameters , 8.7 for end - systolic diameters , 5446 , 68 ml / mil diametro medio dellaorta risultato di 32 , 94 mm ( range 1949 , 5 mm ) , lo spessore medio del setto 8 , 83 mm ( range 2 , 515 , 5 mm ) , della parete posteriore 9 , 67 mm ( range 621 mm )  . 
il diametro telediastolico medio risultato di 52 , 24 mm , il diametro telesistolico di 31 , 57 m il volume telediastolico medio risultato di 99 , 43 ml , il volume telesistolico medio di 43 , 81 , la lvef di 58 , 76% ( range 30%75% )  . 
il diametro aortico medio risultato di 35 , 53 mm ( range 2751 mm ) , lo spessore medio del setto di 11 , 03 mm ( range 715 mm ) , della parete posteriore di 9 , 7 mm ( range 715 mm )  . lo stroke volume , la massa cardiaca e la portata cardiaca medi sono risultati rispettivamente di 78 , 78 ml , 205 , 53 g , 4171 , 79 ml / m la correlazione tra la actcms e lecocardiografia in termini di diametro telediastolico e telesistolico , diametro aortico , spessore del setto e della parete posteriore , volume telediastolico e telesistolico , frazione di eiezione , stroke volume , massa cardiaca e portata cardiaca stata riassunta nella tabella 3 . 
nellanalisi per paziente della cinetica globale del vs la correlazione tra lac - tcms e leco risultata in una concordanza tra le due tecniche nel 73 , 07% dei casi . 
 stata riscontrata una buona correlazione tra le misure dello spessore del setto e del diametro dellaorta ascendente in eco e in tc , mentre una scarsa correlazione tra le misure dello spessore della parete posteriore . 
la tcms ha sovrastimato in modo consistente i valori medi dei volumi rispetto allecocardiografia . in ogni caso , i volumi telediastolico e telesistolico derivati dalla 2dse e dalla tcms hanno mostrato una correlazione significativa . 
come indicatore di funzione sistolica globale del vs , la fe misurata tramite tcms o ecocardiografia ha mostrato uneccellente correlazione . lo stroke volume e la portata cardiaca sono risultati non correlare bene , mentre per lindice di massa cardiaca si 514 radiol med ( 2011 ) 116 : 505520 table 3 comparison between multidetector - row computed tomography coronary angiography ( mdct - ca ) and echocardiography ( ecg ) linear and volumetric parameters in the evaluation of left ventricular function . 
global lv systolic function assessment is performed in daily practice by ecg , although there are other noninvasive imaging techniques such as magnetic resonance imaging ( mri ) , single - photon emission ct ( spect ) and positron emission tomography ( pet ) for evaluation of lv volumes and global systolic function [ 11 ]  . depending on the mdct - ca acquisition technique , assessing cardiac function may be possible [ 9 ]  . 
secondo i grafici di bland - altman le differenze medie tra eco - cardiografia e ac - tcms nella valutazione della parete posteriore , risultata del 7 , 4% , per il setto interventricolare del 2 , 2% , per laorta ascendente del 7 , 7% , per i diametri telediastolici 5 , 9% , telesistolici 8 , 7% , 0% per la gittata cardiaca , 10% per la frazione di eiezione e 2 , 4% per lo stroke volume . 
i risultati sono riassunti in figura 5 . discussione i nostri risultati hanno dimostrato una buona concordanza generale tra i parametri della ac - tcms e quelli rilevati dalleco nella valutazione della funzione sistoradiol med ( 2011 ) 116 : 505520 in our study , only 15 cases were excluded due to prospective triggering , but there was no need for lv analysis . time for lv function analysis with mdct - ca is higher compared with ecg . 
 according to the blandaltman plot , the mean differences between the two techniques are relatively low ; however , not all data fall into sd limits , thus indicating that the results using the two modalities may not be interchangeable . 
 [ 14 ] , although many papers show excellent concordance of mri and ct in assessing lv function , it is very unlikely that ct or mri can be used as first - line investigations . 
however , if the same raw data provided by ct - ca are used to reconstruct a multiphase data set , lv function can be assessed without exposing the patient to any further investigation , and the coronary artery study can be integrated with a functional study that has the same accuracy as mri . 
 our study , compared with previously published reports , investigated several parameters that are routinely recorded on ecg and not on mdct - ca [ 7 ] for example , bansal et al . [ 13 ] compared lv function in evaluating volumes and ef , whereas our study is more comprehensive and considers the diameters of the posterior wall , septal thickness and many other parameters routinely assessed in an ecg study . 
moreover , in our department , aortic root diameter is constantly part of the evaluation of the heart with ecg , and for this reason , this parameter was also retrieved from the data sets . 
la valutazione della funzione del vs viene eseguita nella pratica quotidiana tramite leco , sebbene esistano numerose altre tecniche dimaging non invasive , come la risonanza magnetica ( rm ) , la tomografia computerizzata a emissione di fotoni singoli ( spect ) e la tomografia ad emissione di positroni ( pet ) , per la valutazione dei volumi e della funzione sistolica globale [ 11 ]  . 
a seconda della tecnica di acquisizione actcms , possibile ottenere una valutazione della funzione cardiaca [ 9 ] ; nella sincronizzazione elettrocardiografica ( ecg ) retrospettiva vengono infatti raccolte informazioni durante tutto il ciclo cardiaco che rendono possibile la valutazione funzionale cardiaca , sia da un punto di vista qualitativo che quantitativo . 
dal nostro studio sono stati esclusi 15 casi a causa del triggering prospettico che non ha permesso la valutazione funzionale essendo in questo caso effettuata una acquisizione solo in fase telediastolica . il tempo necessario per lanalisi della funzione ventricolare sinistra con la ac - tcms risultato maggiore rispetto a quello con leco . 
questo fatto dovuto principalmente allacquisizione dei dati e alla necessit dellanalisi dei contorni nella ac - tcms ; va sottolineato per che questa metodica presenta una variabilit irrilevante tra i vari operatori , mentre lecocardiografia rappresenta una metodica fortemente operatore dipendente . 
rispetto a quanto gi riportato da altri autori abbiamo ottenuto simili risultati di buona concordanza tra le due tecniche nella valutazione della frazione di eiezione , diametri , volumi telediastolico e telesistolico , anche se abbiamo riscontrato una sovrastima dei volumi rispetto a quelli misurati con lecocardiografia . 
questa sovrastima , comunque , un fattore noto e riconosciuto e concorda con quanto riportato da altri autori [ 13 , 14 ]  . secondo i grafici di bland - altman le differenze medie tra le due tecniche sono relativamente basse , tuttavia i valori non cadono sempre nei limiti delle deviazioni standard , evidenziando cos come i risultati delle due tecniche possono non essere intercambiabili . 
 the standard of reference in assessing lvef is cardiac eccellente tra rm e tc nella valutazione del vs , non comune che la rm o la tc possano essere utilizzante come metodiche di prima battuta . 
4 risultati della analisi di regressione lineare tra ecocardiografia e ac - tcms nella misurazione dei volumi ventricolari , frazione di eiezione , parametri lineari , gittata cardiaca e massa cardiaca . 
we performed no comparison with this technique , and this can be considered a limitation of the study . however , in our department , mri is performed for cardiac purposes in very selected cases only , whereas ecg is widely used . 
this aspect is not a contraindication to mdct - ca , which also can thus provide important information on lv function in this subgroup of patients . indagini e lo studio delle arterie coronarie pu essere integrato con lo studio funzionale con la stessa accuratezza della rm . il nostro studio si differenzia da quelli precedentemente pubblicati in quanto prende in considerazione pi parametri della funzione cardiaca routinariamente registrati in ecocardiografia [ 7 ]  . 
 [ 12 ] hanno comparato solamente i volumi e la frazione di eiezione , mentre in questo nostro lavoro sono stati valutati parametri lineari quali i diametri , lo spessore della parete posteriore e del setto . 
questo pu essere spiegato dalla differenti tecniche usate in ecocardiografia nel ricavare questi dati , talvolta dipendenti da calcoli automatici ottenuti dalla workstation , talvolta calcolati tramite formule a partire da parametri lineari ; un metodo questo che pu essere responsabile di errori maggiori perch tali formule ricavano volumi e coefficienti a partire da misure lineari ed errori di misura anche minimi possono essere amplificati enormemente [ 15 ]  . lo standard di riferimento nella valutazione della funzione ventricolare sinistra la risonanza magnetica cardiaca [ 1619 ] ; non essendo per stata eseguita in questo lavoro una comparazione tra queste tecniche , sar necessario approfondire questo aspetto nei prossimi studi . 
in ogni caso nel nostro dipartimento la cardio - rm viene eseguita in casi selezionati , mentre lecocardiografia viene utilizzata come indagine di prima battuta per la valutazione della funzione . 
inoltre la rm non pu essere utilizzata in pazienti portatori di pacemaker che spesso hanno uno scompenso cardiaco cronico ; questo aspetto non invece una controindicazione alla actcms . il nostro studio ha preso in considerazione anche lanalisi della cinetica regionale della parete del vs , dimostrando una buona concordanza tra la ac - tcms e lecocardiografia nel valutare il deterioramento della cinetica di parete e nel distinguere le aree acinetiche da quelle ipocinetiche , risultando questa metodica estremamente utile e significativa nella valutazione dellinsufficienza cardiaca cronica [ 20 ]  . 
our study demonstrated an overall good concordance between mdct - ca and ecg in assessing impaired motion and distinguishing stationary areas or an overall impaired function , thus helping assess dilated cardiomyopathy [ 20 ]  . 
on mdct - ca , this rate is higher due to the automated calculation of the borders of the ventricle wall , whereas in ecg , kinetics is judged from a qualitative point of view . 
questo dovuto principalmente al fatto che solo il 3 , 85% di questi segmenti stato giudicato come discinetico in ecocardiografia ; questa percentuale risultata pi alta nella ac - tcms per il calcolo automatico dei bordi della parete del vs , mentre in ecocardiografia la cinetica stata giudicata da un punto di vista qualitativo . 
tuttavia il ruolo definitivo della ac - tcms in questa applicazione funzionale deve essere validata ulteriormente per poter usare questa metodica nella pratica quotidiana . conclusions conclusioni our study demonstrates that mdct - ca provides parameters of cardiac function comparable with those retrieved in ecg . 
thus , mdct - ca can provide additional information to the study of the coronary arteries and is available for diagnostic workup of patients with coronary artery disease and cardiac disease . 
 questo studio dimostra che la ac - tcms ottiene parametri equivalenti rispetto quanto campionato con lecocardiografia nella valutazione della funzione ventricolare quindi la ac - tcms pu essere usata come una valida alternativa per valutare allo stesso tempo la patologia delle arterie coronarie e la funzione cardiaca . radiol med ( 2011 ) 116 : 505520 fig . 
the rst chapter is about the general aspects of fractures in child abuse ( discussion of the differences between paediatric and adult fractures , their differential diagnosis and types of fractures in child abuse )  . 
il primo capitolo tratta degli aspetti generali delle fratture nellabuso ( con discussione delle differenze tra le fratture del bambino e delladulto , la loro diagnosi differenziale ed il tipo di fratture nellabuso )  . 
i successivi otto capitoli trattano : il cranio ; le coste ; le clavicole , le scapole , lo sterno , le vertebre e il bacino ; le ossa lunghe ; il trauma accidentale ; le varianti normali e le malattie congenite ed acquisite ; la radiologia di fronte al sospetto di abuso del bambino ; la datazione della frattura ( alcune pagine di questultimo capitolo 672 radiol med ( 2011 ) 116 : 671672 are also devoted to histological fracture dating of fresh and dried bone tissue from the forensic point of view )  . each chapter follows a rather strict lay - out : introduction , clinical presentation , radiological ndings ; differential diagnosis ; data from the literature ; conclusions and closes with an up - dated literature reference list ( the same reference list is printed twice in the last chapter ! )  . each type of non - accidental trauma can be described more than once according to the relevant literature references , detailing occurrence numbers , percentages etc . image reproduction is quite good and the use of detailed reproduction or photo - enhancement to improve fracture visibility should be praised . 
 there is also a valuable chapter on how to radiograph a child in case of suspected child - abuse related fractures : forget the old fashioned baby - gram and follow the strict rules of the british society of paediatric radiology , implemented by the british society of radiology and those of the american society for pediatric radiology . this is a must - have book , particularly in italy where nonaccidental fractures are not commonly encountered and described ( the very few references from the italian literature are proof of this ) , in order to be prepared , in the unpleasant occurrence of such an event , on how to appraise and report it and to raise awareness on what to do and the related consequences . 
biondetti2 1school of residency , universit degli studi di milano , via di rudin 8 , milano , italy 2foundation irccs , ca granda ospedale maggiore policlinico , via francesco sforza 28 , milano , italy 3dipartimento di scienze dellinformazione ( dsi ) , universit degli studi di milano , via comelico 39 / 41 , milano , italy correspondence to : f . 
this study sought to identify not only hepatodiaphragmatic intestinal interpositions , de ned as chilaiditi , but also other forms of intestinal interposition , which we termed non - chilaiditi . 
moreover , a questionnaire investigating the clinical symptoms reported to be associated with chilaiditi syndrome was given to patients exhibiting any form of intestinal interposition and to a control sample . 
of the 4 , 338 patients examined , 130 ( 3% ) were found to have intestinal interposition , for a total of 143 forms : 90 chilaiditi and 53 non - chilaiditi . 
 in tale studio , sono state evidenziate sia interposizioni di tipo epatodiaframmatico , che sono state de nite chilaiditi come da letteratura , sia altri tipi di interposizione de nite secondo i diversi rapporti anatomici : splenorenale , retrogastrica , epatocavale , retrosplenica e retrorenale , che sono state raggruppate sotto il termine non - chilaiditi . 
su 4338 pazienti sono stati osservati 130 ( 3% ) pazienti con interposizione colica per un totale di 143 manifestazioni , 90 chilaiditi e 53 non - chilaiditi : 30 interposizioni di tipo splenorenale , 12 di tipo retrogastrico , 5 epatocavale , 4 retrosplenico e 2 retrorenale . 
abbiamo inoltre evidenziato che anche le forme non - chilaiditi sono statisticamente pi sintomatiche dei casi controllo . keywords chilaiditi sign chilaiditi syndrome intestinal interposition retrosplenic colon retrogastric colon parole chiave segno di chilaiditi sindrome di chilaiditi interposizione intestinale colon retrosplenico colon retrogastrico introduction introduzione intestinal interposition is a condition in which a section of intestine is temporarily or permanently interposed either between the liver and the diaphragm ( a condition known as chilaiditis sign ) or between the spleen and the diaphragm , the spleen and the left kidney , the stomach and the pancreas , the liver and the inferior vena cava or the kidney and the diaphragm ( these latter conditions being classi ed by us as non - chilaiditi forms )  . 
although colonic interposition is no doubt the most frequent , small - bowel interposition may also be observed ( at the hepatodiaphragmatic level ) , whereas simultaneous interposition of the two segments is rare [ 1 ]  . 
 in 1910 , demetrius chilaiditi [ 2 ] described the radiographic ndings of intermittent hepatodiaphragmatic interposition of the large bowel in three patients , and since then , the term chilaiditis sign has been commonly used to describe this condition [ 3 ]  . 
other forms of colonic and / or small - bowel interposition have only occasionally been investigated [ 4 ] , probably as a result of the fewer symptoms reported and the imaging modalities employed before the age of computed tomography ( ct )  . 
the aim of this paper is therefore to describe the prevalence and clinical impact of non - hepatodiaphragmatic forms of intestinal interposition in an adult population undergoing ct for a range of indications . materials and methods linterposizione intestinale una condizione nella quale un tratto di intestino si trova interposto temporaneamente o permanentemente tra fegato e diaframma ( condizione nota come segno di chilaiditi ) o tra milza e diaframma posteriormente , tra milza e rene sinistro , tra stomaco e pancreas , tra fegato e vena cava inferiore , tra rene e diaframma ( condizioni da noi raggruppate come forme non - chilaiditi )  . 
 linterposizione colica decisamente la pi frequente , ma si osserva talvolta interposizione del piccolo intestino ( in sede epatodiaframmatica ) , mentre linterposizione contemporanea dei due segmenti ancora pi rara [ 1 ]  . nel 1910 demetrius chilaiditi [ 2 ] studi con radiogrammi convenzionali tre pazienti con interposizione epatodiaframmatica intermittente del grosso intestino e da allora il termine segno di chilaiditi stato usato comunemente per descrivere questa condizione [ 3 ]  . 
probabilmente per la minore sintomatologia espressa , nonch per le metodiche utilizzate prima dellera della tomogra a computerizzata ( tc ) , le altre forme di interposizione colica e / o dellintestino tenue non sono state indagate se non saltuariamente [ 4 ]  . 
la sintomatologia clinica eventualmente espressa dai portatori di interposizione epatodiaframmatica , condizione nota come sindrome di chilaiditi [ 5 ] , stata ampiamente trattata , mentre nessun autore si riferisce in tal senso alle forme non - chilaiditi , n vi sono articoli relativi alla loro prevalenza globale nella popolazione generale . 
per tali motivi , in questo articolo abbiamo voluto descrivere la prevalenza delle forme di interposizione intestinale non epatodiaframmatica nonch il loro impatto clinico , in una popolazione adulta sottoposta a tc per differenti patologie . from november 2008 to april 2009 we looked for the presence of intestinal interposition in 4 , 338 adult patients undergoing abdominal , chest ( to mid - kidney level ) or whole - body ct for a range of medical and surgical indications . 
 interposition was de ned as hepatodiaphragmatic when the colon or small bowel were found to lie between the liver and the diaphragm at or above the level of t11 ; splenorenal when the colon was located between the left kidney and spleen at or above the level of the renal hilum ; retrogastric or gastropancreatic when the large bowel lay between the stomach and the pancreas ; hepatocaval when the colon was located between the liver and the inferior vena cava not below the portal plane ; retrosplenic if the colon was interposed between the spleen and the diaphragm at or above the level of the splenic hilum ; and retrorenal when the organ was located between the left kidney and the diaphrag patients who had undergone splenectomy were excluded from the analysis because of the possible anatomical changes brought about by the surgical procedure , as were patients with ascites , given that free uid creates a space between the liver and the diaphragm into which the bowel can easily migrate , as reported in the literature [ 6 ]  . the different conditions were grouped into two classes , separating the better known and studied hepatodiaphragmatic interposition from all the other forms , which we dened as non - chilaiditi . 
 patients with intestinal interposition as well as a control group were administered a questionnaire on the clinical symptoms reported to be associated with chilaiditi syndrome , in particular , abdominal pain , abdominal distension , constipation and atulence . 
linterposizione stata da noi de nita epatodiaframmatica quando il colon o lintestino tenue sono localizzati tra fegato e diaframma non inferiormente a un piano passante per d11 ; splenorenale quando il colon situato tra rene sinistro e milza , non inferiormente a un piano passante per lilo renale ; retrogastrica o gastropancreatica quando lintestino crasso posto tra stomaco e pancreas ; epatocavale quando il colon localizzato tra fegato e vena cava inferiore , non inferiormente al piano portale ; retrosplenica quando il colon si trova interposto tra milza e diaframma posteriormente , non inferiormente a un piano passante per lilo splenico ; retrorenale quando il viscere si trova tra rene sinistro e diaframma . 
 non sono stati inclusi i pazienti sottoposti a splenectomia per le possibili modi cazioni anatomiche dovute alla procedura chirurgica , n i pazienti con ascite poich , come descritto in letteratura [ 6 ] , la presenza di liquido libero crea uno spazio tra fegato e diaframma nel quale lintestino pu facilmente migrare . abbiamo raggruppato queste diverse condizioni in due classi , separando linterposizione epatodiaframmatica , pi conosciuta e studiata , da tutte le altre forme , de nite da noi non - chilaiditi . 
tenendo conto dei differenti rapporti anatomici che in queste si creano , le abbiamo anche considerate distintamente , per valutarne la prevalenza . ai pazienti con interposizione intestinale e ad un campione controllo , stato successivamente sottoposto un questionario relativo ai sintomi clinici che in letteratura risultano legati alla sindrome di chilaiditi , in particolare : dolori addominali , distensione addominale , costipazione e atulenza . 
sono state quindi valutate le manifestazioni cliniche dei pazienti portatori di forme non - chilaiditi , comparandole con la forma di chilaiditi e col gruppo controllo , per veri care se esistessero delle differenze statisticamente signi cative . 610 radiol med ( 2011 ) 116 : 607619 associated with the symptom , assuming the value 1 if the symptom is present and the value 0 where no symptom is present . 
to overcome the small sample size , the yates correction was applied , obtaining a 2 value = 7.3667 , indicating that the difference in symptoms between the three groups was signi cant at a probability level p3% , implying a probability of p97% that the values obtained for the symptoms were not due to chance . results of 4 , 338 patients undergoing ct , intestinal interposition was identi ed in 130 ( 3% ) , of whom 92 were men and 38 women ( age range 3887 years ; mean 66 years )  . 
table 1 shows the intestinal anatomical variants observed in ten patients curiously , all women who presented with more than one interposition , for a total of 23 cases of interposition . overall , the chilaiditi form was observed 90 times . 
in 83 cases , the interposition involved the colon , whereas in the remaining seven cases , it involved the small bowel ( in each case , the ileum )  . 
colon interposto tra fegato e diaframma ( frecce bianche )  . analisi statistica per la valutazione della sintomatologia abbiamo calcolato la media campionaria e la deviazione standard della variabile casuale legata al sintomo , supponendo che essa assuma i valori 1 ( nel caso in cui sia presente un sintomo ) e 0 ( nel caso in cui non ci sia sintomo )  . 
per sopperire alla scarsa numerosit del campione abbiamo applicato la correzione di yates , ottenendo un valore di 2 pari a 7 , 3667 ; ci consente di ritenere che la differenza di sintomatologia fra i tre gruppi sia signi cativa al livello di probabilit p3% , ovvero che ci sia una probabilit p97% che i valori di sintomatologia ottenuti non siano casuali . risultati su 4338 pazienti sottoposti a esami tc abbiamo evidenziato 130 ( 3% ) pazienti portatori di una condizione di interposizione intestinale , 92 maschi e 38 femmine , di et compresa tra i 38 e gli 87 anni , con una media di 66 anni . 
nella tabella 1 sono riportate le varianti anatomiche intestinali dei dieci pazienti , curiosamente solo femmine , che presentavano pi di uninterposizione , per un ammontare di 23 manifestazioni . nel complesso , la forma di chilaiditi stata evidenziata 90 volte , in 83 era interposto lintestino crasso , mentre nei rimanenti 7 casi linterposizione coinvolgeva lintestino tenue ( sempre ileo )  . 
delle 90 forme di chilaiditi , 76 sono state riscontrate in maschi , mentre 14 erano presenti in femmine ; per quanto riguarda le 53 forme non - chilaiditi , 16 erano presenti in maschi e 37 in femmine . da novembre 2008 ad aprile 2009 , 80 pazienti , per un totale di 82 manifestazioni di interposizione intestinale , hanno dovuto sottoporsi a pi esami tc , osservandosi lincostanza di 30 forme , di cui 27 condizioni di chilaiditi e 3 radiol med ( 2011 ) 116 : 607619 fig . 
 stata quindi riscontrata unincostanza della condizione epatodiaframmatica del 42 , 9% e del 15 , 8% per le altre tipologie di interposizione . per quanto riguarda la sintomatologia , nella tabella 3 sono riportati i dati relativi ai disturbi clinici dei tre gruppi ai quali stato sottoposto il questionario ( forme chilaiditi , forme non - chilaiditi , casi controllo ) , con i valori di media e derivazione standard campionari . 
analizzando i valori delle medie campionarie ottenuti per i tre gruppi si deduce che le forme che procurano una maggiore sintomatologia sono le forme di chilaiditi ( media = 0 , 2444 ) , a cui seguono quelle non - chilaiditi ( media = 0 , 1887 ) e in ne quelle dei casi controllo ( media = 0 , 1077 )  . 
paziente con colon retrogastrico ( freccia in a ) , retrosplenico ( fraccia in b ) e splenorenale ( fraccia in c )  . table 1 patients with two or more forms of intestinal interposition patient no . 
 chilaiditi non - chilaiditi splenorenal retrogastric retrosplenic retrorenal radiol med ( 2011 ) 116 : 607619 ileal ileal ileale ileale tabella 1 pazienti portatori di due o pi forme di interposizione intestinale paziente no . 
non - chilaiditi : retrosplenica ( media = 0 , 50 ) e variabilit maggiore rispetto a tutti gli altri gruppi ( ds = 0 , 5774 ) ; 3 . 
non - chilaiditi : retrogastrica e retrorenale ( media = 0 ) , ovvero nessuna frequenza di sintomatologia e nessuna variabilit ( ds = 0 )  . nella tabella 4 abbiamo applicato il test di signi cativit 2 alla matrice delle sintomatologie . 
it should be discussione linterposizione intestinale epatodiaframmatica fu descritta per la prima volta radiologicamente , da antoine bclre nel 1899 , ma fu nel 1910 che demetrius chilaiditi [ 2 ] , radiologo greco nato a vienna , descrisse tre casi di pazienti con temporanea interposizione epatodiaframmatica del colon . 
 prima dellera tc , le condizioni di malposizione dellintestino differenti dalla chilaiditi , da noi de nite come forme non - chilaiditi , sono state oggetto di poche pubblicazioni , nonch descritte di solito singolarmente . nel 1942 poppel e herstone descrivono uninterposizione sinistra ( left - side interposition ) [ 7 ]  . 
nel 1960 poppel descrive una apposizione duodenocolica ( duodenocolic apposition ) [ 8 ] e postula la persistenza di bande peritoneali embrionarie che comporterebbero lo sviluppo di un mesocolon trasverso corto . 
nel 1977 balthazar [ 10 , 11 ] espone una revisione degli aspetti radiologici delle anomalie congenite della posizione anatomica del colon , total ( n = 273 ) asymptomatic , n ( % ) symptomatic , n ( % ) radiol med ( 2011 ) 116 : 607619 table 4 matrix for calculating the signi cance testa chilaiditi ( n = 90 ) non - chilaiditi ( n = 53 ) control group ( n = 130 ) 68 ( 75.6 ) 43 ( 81.1 ) 116 ( 89.2 ) amatrix does not take into account the separation of forms of intestinal interposition into subgroups , as these were too small to allow statistical signi cance to be tested tabella 4 matrice per il calcolo del test di signi cativita totale ( n = 273 ) asintomatici , n ( % ) sintomatici , n ( % ) chilaiditi ( n = 90 ) non - chilaiditi ( n = 53 ) controllo ( n = 130 ) 68 ( 75 , 6 ) 43 ( 81 , 1 ) 116 ( 89 , 2 ) atale matrice non tiene conto della separazione delle forme di interposizione intestinale nei sottogruppi , in quanto queste sono composte da un numero di campioni troppo basso ai ni del calcolo del test di signi cativit 22 ( 24.4 ) 10 ( 18.9 ) 14 ( 10.8 ) 22 ( 24 , 4 ) 10 ( 18 , 9 ) 14 ( 10 , 8 ) ma non parla di colon retrogastrico . 
nel 1993 old eld e wilbur [ 4 ] descrivono il colon retrogastrico alla tc , ma includono sotto questo termine anche la posizione splenorenale e retrosplenica . nel nostro lavoro , partendo dalle forme di interposizione non epatodiaframmatica descritte in letteratura , abbiamo voluto mantenere una divisione maggiore delle varianti anatomiche intestinali , per studiare la prevalenza di ogni singola forma e osservare se ci fossero delle differenze sintomatologiche tra i gruppi . 
 before the age of ct , the literature contained few studies of forms of intestinal malposition other than chilaiditi , and these were usually reports of single cases . in 1942 , poppel and herstone described a case of leftsided interposition [ 7 ]  . 
in 1960 , poppel reported a case of duodenocolic apposition [ 8 ] and postulated the persistence of embryonic peritoneal bands that would lead to the development of a short transverse mesocolon . 
in 1977 , balthazar published a review of the radiological features of congenital anomalies of the anatomical position of the colon but did not mention retrogastric colon [ 10 , 11 ]  . 
in 1993 , old eld and wilbur described retrogastric colon on ct , but included both splenorenal and retrosplenic positions under this term [ 4 ]  . in our study , starting from the forms of non - hepatodifig . 
note colonic air located posteriorly with respect to the portal vein ( white arrow ) , between the liver ( asterisk ) and inferior vena cava ( black arrow ) ( a )  . 
c piano coronale : colon ( freccia nera a sinistra ) , vena cava inferiore ( freccia bianca ) , diaframma ( freccia nera a destra )  . aphragmatic interposition described in the literature , we sought to maintain a greater division of intestinal anatomical variants with the aim of studying the prevalence of each form and ascertaining whether symptoms differed between the groups . 
in particular , among the single non - chilaiditi forms reported in the literature , we separated the splenorenal and retrogastric forms , which were grouped together in the literature [ 4 ] , and the hepatocaval forms , which were previously evaluated alongside retrogastric forms under the grouping of posterior hepatodiaphragmatic interposition [ 13 ]  . 
this said , however , we also considered the cases of non - hepatodiaphragmatic interposition as a single group of non - chilaiditi forms in order to increase the statistical value of data relating to the symptoms . 
 whereas non - hepatodiaphragmatic forms have been correlated with congenital anomalies [ 7 ] , a range of mainly epatocavali , che in letteratura sono state valutate assieme alla forma retrogastrica , con il nome di epatodiaframmatica posteriore [ 13 ]  . 
lidenti cazione delle haustrae o delle pliche conniventi aiuta in questa differenziazione . se le forme non epatodiaframmatiche sono state correlate ad anomalie congenite [ 7 ] , per la condizione di chilaiditi , pi studiata , sono chiamate in causa diverse eziologie , principalmente acquisite . 
choussat e chaussat - clausse [ 14 ] suggeriscono problemi intestinali ( megacolon , motilit anomale del colon , accumulo anomalo di gas ) , diaframmatici ( diaframma alto , degenerazione muscolare , patologie del frenico ) e / o epatici ( fegato piccolo , interventi chirurgici )  . 
 [ 1 ] e murphy [ 15 ] postulano altre cause associate , come la broncopneumopatia cronica ostruttiva , radiol med ( 2011 ) 116 : 607619 acquired aetiologies have been suggested for the more thoroughly investigated chilaiditi forms . 
choussat and choussat - clausse suggested that conditions affecting the bowel ( megacolon , abnormal colonic motility and abnormal gas accumulation ) , the diaphragm ( high diaphragm , muscular degeneration and phrenic diseases ) and / or liver ( small liver , surgery ) were the main causes [ 14 ]  . 
 murphy demonstrated that in obese individuals , fat deposition between the liver and the diaphragm can be a determining factor in the pathogenesis of hepatodiaphragmatic interposition [ 15 ]  . 
other causes include bowel malrotation [ 10 ] dolichocolon , an abnormal length of the mesentery , laxity of hepatic suspensory ligaments [ 16 ] or bowel mal xation [ 14 ]  . 
the literature reports a highly variable prevalence of hepatodiaphragmatic interposition [ 6 ] , from 0.02% to 1% , if one excludes a single study of cirrhotic patients in whom the condition affected 22% , and a distribution dependent on sex ( male : female ratio 4 : 1 ) and age ( being more common in men > 65 years )  . 
 in our series , 2% of patients had hepatodiaphragmatic interposition , a relatively high percentage compared with the literature , and probably justi ed by the fact that most of our patients had some form of liver disease , resulting in abnormal liver morphology . 
nakagawa and toda have shown that the prevalence of the chilaiditi form in a population composed solely of cirrhotic patients is much higher than that found in the general population , reaching 22% in their study [ 6 ]  . 
in our study , in addition , patients with ascites were excluded , as the uid creates a free space between the liver and diaphragm into which the intestines can easily migrate . to our knowledge , no study to date has satisfactorily assessed the prevalence of non - hepatodiaphragmatic forms of interposition . 
this sex distribution is unexpectedly different from the chilaiditi forms , which affected 76 men and 14 women , with a ratio similar to that reported in the literature [ 5 ]  . 
among the non - chilaiditi forms , splenorenal interposition was by far the most frequent , accounting for 56.6% of cases , followed by the retrogastric form with 22.8% , whereas the other non - chilaiditi forms did not exceed 10% . kolju showed that in one third of patients with chilaiditis sign , the condition is temporary , whereas in two thirds , it is permanent and con rmed by subsequent radiographic examinations [ 5 ]  . 
we found a transiency rate of 42.9% for chilaiditi forms , higher than that reported in the literature ( 33% ) , whereas for the non - chilaiditi forms , the transiency rate was 15.8%. 
altre cause possono essere malrotazione [ 10 ] , dolicocolon , anomala lunghezza del mesentere , lassit dei legamenti sospensori del fegato [ 16 ] o mal ssazione [ 14 ]  . 
la letteratura riporta una prevalenza dellinterposizione epatodiaframmatica molto variabile [ 6 ] , dallo 0 , 02% all1% , se si eccettui uno studio effettuato per solo su pazienti cirrotici , in cui si raggiunto il 22% , presentandosi con una distribuzione dipendente dal sesso ( rapporto maschi : femmine 4 : 1 ) e dallet ( pi frequente nei maschi oltre i 65 anni )  . nella nostra casistica il 2% dei pazienti presentava interposizione epatodiaframmatica , percentuale abbastanza alta rispetto alla letteratura , giusti cata verosimilmente dal fatto che la maggior parte dei nostri pazienti sono epatopatici , con conseguente alterazione della morfologia epatica . 
 nakagawa e toda [ 6 ] hanno dimostrato infatti che la prevalenza della forma di chilaiditi in una popolazione di soli cirrotici molto superiore alla popolazione generale , arrivando nel loro studio al 22% . 
in questo lavoro , tra laltro , non sono stati considerati i pazienti con ascite , poich il liquido libero crea uno spazio tra fegato e diaframma nel quale lintestino pu facilmente migrare : per tal motivo abbiamo escluso tali pazienti dalla nostra casistica . dai dati disponibili risulta che ancora nessuno in letteratura abbia valutato soddisfacentemente la prevalenza delle forme di interposizione non epatodiaframmatica . 
questultimo dato si differenzia in modo inaspettato dalle forme di chilaiditi , dove su 90 portatori della condizione epatodiaframmatica , 76 erano maschi e 14 femmine , mostrando un rapporto percentuale come da letteratura [ 5 ]  . 
tra le forme non - chilaiditi quella splenorenale stata di gran lunga la pi frequente , rappresentando il 56 , 6% dei casi , seguita da quella retrogastrica , con il 22 , 8% , mentre le altre forme non - chilaiditi non hanno superato il 10% . kolju [ 5 ] ha dimostrato come in un terzo dei pazienti portatori di chilaiditi tale condizione sia incostante , mentre nei due terzi confermata da controlli radiogra ci a distanza di tempo . 
abbiamo riscontrato unincostanza dei reperti di chilaiditi del 42 , 9% , superiore a quella della letteratura ( 33% ) , mentre per le forme non - chilaiditi lincostanza stata del 15 , 8% . 
questo dato pu essere spiegato dallipotesi , gi presentata in letteratura , di una patogenesi congenita delle forme non epatodiaframmatiche . linterposizione epatodiaframmatica solitamente asintomatica , ma , come descritto in letteratura , pu essere associata ai seguenti sintomi : dolori addominali , disten618 radiol med ( 2011 ) 116 : 607619 pothesis , already presented in the literature , of a congenital pathogenesis of non - hepatodiaphragmatic forms of interposition . hepatodiaphragmatic interposition is usually asymptomatic , but it may be associated with abdominal pain , abdominal distension , atulence , constipation , nausea , vomiting , shortness of breath , substernal pain and anorexia [ 1 , 17 , 18 ]  . 
the symptoms tend to be worse towards the end of the day and when the patient remains sitting or standing for long periods of time , as this facilitates the descent of the liver and the ascent of the distended bowel . 
the symptoms are also more frequent when the interposition involves the small bowel and when it occurs in persons with mental retardation [ 1 , 17 ] , due to aerophagia . 
in our study , the symptoms considered to be discriminant were abdominal pain , abdominal distension , constipation and atulence , given that these are reported to be the most signi cantly correlated with intestinal interposition [ 1 ]  . 
 with regard to the single groups , however , we encountered an unusual pattern of symptom frequency ( the control group showing a higher frequency of symptoms when compared with some of the non - chilaiditi cases ) , but this may be in uenced by the fact that the sample size available for the subgroups of chilaiditi and non - chilaiditi was small and therefore of limited statistical signi cance . it should be noted that the ileal hepatodiaphragmatic forms were found to be more symptomatic than the colonic forms , as reported in the literature [ 1 ]  . 
although the small sample size does not allow for any statistically valid statements regarding these ndings , it would be interesting to assess the presence or absence of symptoms when encountering these forms in other ct studies . 
 conclusions although intestinal interposition is generally infrequent , the lesser known forms ( non - hepatodiaphragmatic ) account sione addominale , atulenza , costipazione , nausea , vomito , respiro corto , dolore sottosternale , anoressia [ 1 , 17 , 18 ]  . 
i sintomi sono peggiori al termine della giornata e quando il paziente sta seduto o rimane in posizione eretta per lungo tempo , poich ci facilita la discesa del fegato e la risalita del viscere intestinale ripieno di gas . 
il trattamento richiesto di solito conservativo , come riposo a letto o decompressione mediante sondino nasogastrico , mentre la chirurgia raramente richiesta , come per esempio nei casi di volvolo intermittente . partendo da tale quadro sintomatologico , abbiamo voluto valutare la prevalenza della sintomatologia nei pazienti con altre forme di interposizione intestinale . 
nel nostro studio abbiamo considerato come sintomi discriminanti il dolore , la distensione addominale , la costipazione e la atulenza , poich , dalla letteratura [ 1 ] , erano quelli pi signi cativamente correlati ai quadri di interposizione intestinale . 
la nostra analisi statistica ha evidenziato come la sintomatologia delle forme di chilaiditi sia superiore sia a quella delle forme non - chilaiditi , sia a quella del gruppo controllo . 
allo stesso modo , le forme non - chilaiditi presentano una sintomatologia statisticamente maggiore rispetto ai casi controllo . per quanto riguarda i singoli gruppi abbiamo invece avuto un insolito ordinamento delle frequenze di sintomi ( i casi controllo presentano una maggiore frequenza di sintomi rispetto ad alcuni casi non - chilaiditi ) , ma ci pu essere in uenzato dal fatto che per i sottogruppi di chilaiditi e non - chilaiditi a volte disponibile un numero di campioni poco elevato e quindi statisticamente poco signi cativo . da rilevare che le forme epatodiaframmatiche ileali sono risultate essere pi sintomatiche delle corrispettive coliche , come da letteratura [ 1 ]  . 
per quanto riguarda le forme nonchilaiditi , quella epatocavale in 5 casi su 5 sempre sintomatica , mentre un comportamento inverso stato riscontrato nelle forme non - chilaiditi retrogastrica e retrorenale . 
tali dati , per la bassa numerosit del campione , non consentono di fare affermazioni statisticamente valide , tuttavia sarebbe interessante , riscontrando tali forme anche in altri studi tc , valutare la presenza o assenza della sintomatologia . conclusioni per quanto le forme di interposizione intestinale siano poco frequenti , da considerare come quelle meno conosciute ( quelle non epatodiaframmatiche ) ne rappresentino comunque una discreta parte , pi della met secondo radiol med ( 2011 ) 116 : 607619 for a fair proportion of cases more than half , according to our study . 
in view of this aspect and of our ndings with respect to symptomatology , we believe it might be useful to indicate as a descriptive nding in the radiology report the presence of anatomical variants of the small and / or large bowel . 
faletti1 1 dipartimento di diagnostica per immagini , uoa di radiologia diagnostica , azienda ospedaliera cto - crf - maria adelaide , torino , italy 2 sezione di scienze radiologiche , di.bi.me.f , universit di palermo , italy 3 dipartimento di traumatologia , ortopedia e medicina del lavoro , azienda ospedaliera cto - crf - maria adelaide , torino , italy 4servizio di anatomia patologica , a.o. 
between january 2003 and may 2010 , 66 suspected neurinomas were evaluated according to their sonographic features ( solid fusiform mass with well - de ned margins located in direct continuity with the nerve that was not always discernible and heterogeneous as a result of the presence of small cystic areas or calci cations )  . 
the lesions were examined using a sonographic contrast medium consisting of sulphur hexa uoride microbubbles and equipment with dedicated contrast - speci c software [ contrast tuned imaging ( cnti ) ]  . 
 of these lesions , ve were excluded from the analysis because the de nitive diagnosis was not available ( in two cases , the follow - up was still in progress , whereas in the remaining three , there was no follow - up )  . 
in 41 / 61 cases ( 67.2% ) , we identi ed an enhancement pattern that we termed reticular owing to the interweaving of blood vessels , of which two subtypes were identi ed depending on whether the interwoven vessels were densely or sparsely packed : loose - knit riassunto obiettivo . 
nel periodo compreso tra gennaio 2003 e maggio 2010 sono state valutate nel nostro dipartimento 66 lesioni sospette per neurinoma in base alle loro caratteristiche ecogra che ( formazioni solide , fusiformi , a margini netti , in diretta continuit con la bra nervosa , non sempre riconoscibile , disomogenee per leventuale presenza di piccole aree similcistiche o calci cazioni ) , ed esaminate con mezzo di contrasto ( mdc ) ecogra co , costituito da microbolle a base di esa uoruro di zolfo e apparecchiatura dotata di software dedicato contrast tuned imaging ( cnti ) contrasto speci co . 
di queste lesioni , 5 sono state escluse dallanalisi in quanto non era disponibile una diagnosi de nitiva ( n = 2 follow - up in corso ; n = 3 assenza di follow - up )  . 
in 41 / 61 ( 67 , 2% ) casi abbiamo identi cato una distribuzione del mezzo di contrasto de nita a reticolo in base allintreccio formato dalle strutture vascolari , in cui si riconoscono due sottotipi : reticolo a maglie larghe in 18 / 41 e reticolo a maglie strette in 23 / 41 , radiol med ( 2011 ) 116 : 634643 reticular in 18 / 41 , and tight - knit reticular in 23 / 41 . 
results showed that all neurinomas studied could be divided into two groups according to the type of enhancement pattern observed : reticular or diffuse heterogeneous . keywords schwannoma ultrasound power doppler imaging contrast media distinti in base allaspetto dellincrocio dei vasi , se pi rado o pi tto . 
i risultati ottenuti in questo studio hanno dimostrato che tutti i neurinomi analizzati possono essere distinti in due gruppi , in base al tipo di pattern vascolare riscontrato : di tipo reticolare o ad impregnazione diffusa disomogenea . parole chiave schwannoma ecogra a power doppler mezzi di contrasto ecogra ci introduction introduzione neurinomas , or schwannomas , are benign tumours that originate from the sheath of peripheral nerves , in relation to which they may align themselves either eccentrically or peripherally [ 1 ]  . 
when stimulated mechanically , they often give rise to pain that feels like an electric shock [ 2 ] , a feature that allows for a well - founded diagnostic hypothesis . 
recent neurinomas are usually fusiform , hypoechoic and homogeneous [ 35 ] , whereas older ones may exhibit cystic areas and , more rarely , calci cations [ 1 , 68 ]  . 
high - resolution us ( hrus ) performed with high - frequency linear - array probes is an excellent modality for visualising and in some cases differentiating peripheral nerve tumours , as in most cases it allows for the easy recognition of direct continuity between the nerve and the two poles of the lesion on longitudinal sections [ 10 ]  . 
power - doppler ( pd ) is an essential complement to baseline us , as the presence of blood vessels within the lesion will in uence any diagnostic suspicion [ 3 ]  . 
however , although power doppler imaging is particularly sensitive to low ows , it is insuf cient to provide a real estimate of lesion vascularity . recent years have seen the increasing use of contrastspeci c us techniques , which optimise recording of the harmonic signal produced by the contrast microbubbles that amplify the signal from the blood vessels [ 11 , 12 ]  . 
 i neurinomi , o schwannomi , sono tumori benigni che prendono origine dalla guaina dei nervi periferici , rispetto ai quali possono disporsi eccentricamente o perifericamente [ 1 ]  . 
sono spesso accompagnati da sintomatologia dolorosa , tipo scossa elettrica [ 2 ] , qualora sollecitati meccanicamente , caratteristica , questa , che ne permette un sospetto diagnostico fondato ; a volte il quadro clinico dubbio o poco signi cativo . 
 la morfologia e lecostruttura dei neurinomi pu variare a seconda del grado di crescita ; quelli di data recente solitamente si presentano fusiformi , ipoecogeni e omogenei [ 35 ] ; quelli di pi vecchia data , invece , possono presentare al loro interno areole similcistiche e , raramente , calci cazioni [ 1 , 68 ]  . 
 lecogra a ad alta risoluzione , ovvero effettuata con sonde lineari ad alta frequenza , costituisce unottima metodica per visualizzare e , talora , differenziare i tumori del sistema nervoso periferico , poich permette agevolmente di dimostrare , nella maggior parte dei casi , la diretta continuazione con la terminazione nervosa ai due poli della lesione , evidenziabile nelle scansioni longitudinali [ 10 ]  . 
 da qualche anno sempre pi frequente limpiego di tecniche ecogra che contrasto speci che , che ottimizzano la registrazione del segnale armonico prodotto dalle microbolle del mezzo di contrasto ( mdc ) ecogra co , le quali consentono un potenziamento del segnale proveniente dai vasi [ 11 , 636 radiol med ( 2011 ) 116 : 634643 unlike diffusive contrast media ( such as those used in magnetic resonance imaging and computed tomography ) that enter the extracellular spaces , us contrast agents remain con ned within the vessels , allowing for clear visualisation of even the smallest vascular structures ( the parenchymal microvasculature )  . 
us contrast agents have a wide range of applications , especially in studying liver and breast focal lesions and in the eld of cardiovascular imaging and haemodynamics [ 1315 ]  . 
few studies have investigated the use of contrast agents in the musculoskeletal system , and no scienti c contributions to date have studied the use of us contrast agents for studying neurinomas [ 16 ]  . 
a differenza dei mezzi di contrasto diffusivi ( utilizzati in risonanza magnetica [ rm ] e tomogra a computerizzata [ tc ] ) , che si dispongono anche negli spazi extracellulari , il mezzo di contrasto ecogra co rimane con nato , per le sue caratteristiche siche , allinterno dei vasi , consentendo cos una precisa visualizzazione anche delle strutture vascolari pi piccole ( microvascolarizzazione parenchimale )  . 
il mdc ecogra co presenta un ampio campo di applicazione soprattutto in ambito epatico e mammario , per lo studio delle lesioni focali , nel distretto cardio - vascolare e nellemodinamica [ 1315 ]  . 
in letteratura limpiego del mdc in ambito muscolo - scheletrico scarsamente rappresentato e non sono stati attualmente riscontrati contributi scienti ci in merito allo studio dei neurinomi con mdc ecogra co [ 16 ]  . 
 scopo del nostro studio valutare se esiste una distribuzione caratteristica dei vasi allinterno dei neurinomi e tentare in tal modo una caratterizzazione degli stessi . materials and methods materiali e metodi between january 2003 and may 2010 , 66 lesions were identi ed as possible neurinomas on the basis of for their us features ( solid , fusiform masses with well - de ned margins , at times in direct continuity with the nerve bre or heterogeneous as a result of the presence of small cystic areas or calci cations )  . 
five of these lesions were excluded from the analysis because a de nitive diagnosis was not available ( n = 2 with follow - up still in progress ; n = 3 without follow - up )  . 
all of these were single lesions except in the case of a woman who had two separate lesions , one in her right thigh ; the other in her left leg . 
these 61 lesions therefore form the basis of our study . the patients ( 35 females , 25 males ) were aged between 15 and 90 ( mean 47 ) years . 
lesion size ranged from 0.9 cm to 7 cm ( table 1 )  . us examinations were performed using an esaote technos mpx unit equipped with la424 14 - 8 mhz , la523 13 - 8 mhz and la532e 8 - 3 mhz linear - array probes and dedicated low - mechanical - index ( 45 kpa ) cnti software , which allows real - time analysis of the signal generated by the contrast mediu all examinations were performed by two operators , both experts in us imaging . 
di queste lesioni , 5 sono state escluse dallanalisi in quanto non era disponibile una diagnosi de nitiva ( n = 2 followup in corso ; n = 3 assenza di follow - up )  . 
le lesioni asportate chirurgicamente e confermate come neurinomi allesame istologico , considerato come gold standard , sono state 61 , tutte uniche tranne nel caso di una donna che presentava due lesioni distinte , una alla coscia destra e una alla gamba sinistra ; dunque unicamente su queste lesioni che si basa il nostro studio . i pazienti ( 35 femmine , 25 maschi ) avevano unet compresa tra 15 e 90 anni ( et media 47 anni ) ; 38 neurinomi erano disposti in sede inframuscolare e 23 sottocutanea ; 24 interessavano larto superiore , 35 larto inferiore , 1 il dorso e 1 la regione cervicale ; le dimensioni variavano da 0 , 9 a 7 cm ( tabella 1 )  . 
 gli esami sono stati condotti con ecografo technos mpx esaote ( biosound esaote , inc , indianapolis , usa ) , dotato di sonde lineari la424 14 - 8 mhz , la523 13 - 8 mhz e la532e 8 - 3 mhz e di software dedicato ( cnti ) a basso indice meccanico ( 45 kpa ) , che consente lanalisi in real time del segnale proveniente dal mezzo di contrasto . 
tutti i pazienti sono stati esaminati in posizione supina o prona , a seconda della sede della lesione , inizialmente con esame ecogra co basale , successivamente con valutazione colorpower doppler . 
at the end of the injection , a timer was started that allowed determination of the time elapsed between the entry of the contrast medium in the circulation and its arrival in the lesion . 
contrast medium time of arrival and distribution pattern was documented on video clips , each lasting about 30 s and which highlighted the most signi cant moments of the study . 
all lesions were studied for at least 3 min ( late phase )  . con 5 cc di soluzione siologica ; ai pazienti non sono stati richiesti digiuno o particolari esami di laboratorio ; in tutti i casi non si sono mai veri cati eventi avversi . 
a ne iniezione viene fatto partire un timer che consente di valutare il tempo che intercorre tra il passaggio in circolo del contrasto e larrivo dello stesso nella lesione esaminata . 
la presenza di spot iperecogeni intraparenchimali dimostra larrivo del mdc nella lesione ; il tempo di arrivo e la modalit di distribuzione sono documentate mediante la registrazione di videoclips , ciascuno della durata di circa 30 secondi , che evidenziano i momenti pi signi cativi dello studio . 
the neurinomas examined at baseline us exhibited a predominantly fusiform appearance ( 40 / 61 ) , with the nerves from which they had arisen being visible at either pole ( 37 / 61 )  . 
sometimes , they appeared as rounded ( 14 / 61 ) or as lobular ( 7 / 61 ) , and it was not possible to visualise the nerve from which they had originated ( 23 / 61 )  . 
often , anechoic areas were observed inside them ( 22 / 61 ) , and , more rarely , ( 3 / 61 ) intralesional calci cation was seen . after us contrast agent administration , neurinomas showed the following characteristics : in 41 / 61 cases , the contrast material distributed from the periphery to the centre , with an interweaving of blood vessels of varying thickness some straight , others tortuous leaving spaces of varying size without visible blood vessels . 
in 20 / 61 lesions , however , the contrast agent did not follow a reticular distribution but diffused within the parenchyma , with densely packed , homogeneously distributed blood vessels , except for the presence of one or more circumscribed areas that exhibited no contrast enhancement . 
this subtype was termed diffuse heterogeneous enhancement ( pattern type 2 ) and was further divided into two subtypes based , in 7 / 21cases , on the presence of a single unenhancing area ( pattern 2a ) , or with more than risultati gli esami sono stati eseguiti da un pool di colleghi esperti della metodica , secondo le indicazioni precedentemente menzionate , ed in seguito revisionati esclusivamente da due di essi , che sono risultati materialmente gli esecutori dellesame nel 88 , 5% dei casi ( 54 / 61 casi )  . 
i neurinomi esaminati , nello studio in basale , hanno presentato prevalentemente un aspetto fusiforme ( 40 / 61 ) ai cui poli si riconosceva la struttura nervosa dalla quale si sviluppavano ( 37 / 61 ) ; talvolta apparivano rotondeggianti ( 14 / 61 ) o bozzuti ( 7 / 61 ) e non si riusciti a visualizzare la struttura nervosa di appartenenza ( 23 / 61 )  . 
spesso , nel loro contesto si sono osservate aree anecogene ( 22 / 61 ) ; pi raramente , in 3 / 61 casi , presentavano calci cazioni intralesionali . dopo somministrazione di mdc ecogra co , i 61 neurinomi esaminati hanno presentato le seguenti caratteristiche : in 41 / 61 casi il mdc si distribuiva dalla periferia al centro , con un intreccio di vasi , costituito da linee pi o meno spesse , a decorso tortuoso o rettilineo , che si intersecano lasciando spazi di differenti dimensioni privi di vasi . 
in 20 / 61 lesioni , invece , il mdc non seguiva una distribuzione di tipo a reticolo , ma si diffondeva allinterno del parenchima con vasi tti , omogeneamente distribuiti , eccezion fatta per la presenza di una o pi aree circoscritte prive di enhancement . 
in tutti i 61 casi losservazione stata protratta no a tre minuti dalliniezione per studiare 640 radiol med ( 2011 ) 116 : 634643 fig.1a , b longitudinal sections of two lesions studied with an 8 - 3 mhz la532 linear probe after intravenous administration of ultrasound contrast material : example of patterns 1a ( a ) loosely - knit reticular and 1b ( b ) tightly - knit reticular . 
1a , b due differenti lesioni studiate mediante scansioni longitudinali dopo somministrazione endovena di mdc ecogra co , con sonda lineare la532 8 - 3 mhz : esempio di pattern 1a ( a ) reticolo a maglie larghe e di pattern 1b ( b ) reticolo a maglie strette . 
i disegni a anco ( a e b ) , chiariscono la distribuzione dei vasi , con il caratteristico intreccio vascolare de nito da noi a reticolo , il cui aspetto , se pi rado o pi tto , permette di contraddistinguere i due sottogruppi . 
we noted that the lesions showing reticular enhancement ( pattern 1 , subtype a or b ) tended to exhibit diffuse and homogeneous distribution of contrast medium during the late venous phases , whereas all neurinomas with diffuse heterogeneous enhancement ( pattern 2 ) maintained the same appearance even 3 min after the injection . discussion according to the international literature , neurinomas , or il comportamento delle lesioni anche nei tempi venosi tardivi . 
 dallanalisi percentuale risulta pertanto che il 67 , 2% dei neurinomi presenta un pattern di tipo 1 , a reticolo , mentre il 32 , 8% presenta un pattern di tipo 2 a impregnazione diffusa disomogenea ( tabella 1 )  . 
abbiamo in ne notato che le lesioni che presentavano un pattern 1 a reticolo , sia di tipo a che di tipo b , nelle fasi venose tardive tendevano ad una diffusa ed omogenea distribuzione del contrasto allinterno della lesione , mentre tutti i neurinomi che appartenevano al gruppo con pattern di tipo 2 impregnazione diffusa disomogenea mantenevano lo stesso aspetto anche a tre minuti dalliniezione . discussione i neurinomi , o schwannomi nella letteratura internazionale , sono tumori benigni a partenza dalla guaina nervosa ; sono riconoscibili come una massa fusiforme disposta eccentricaradiol med ( 2011 ) 116 : 634643 fig . 
2a , b longitudinal sections of two lesions studied with an 8 - 3 mhz la532 linear probe after intravenous administration of ultrasound contrast agent : example of diffuse heterogeneous enhancement , pattern 2a ( a ) showing the presence of a single nonenhancing area and pattern 2b ( b ) due to the presence of several nonenhancing areas . 
2a , b due differenti lesioni studiate mediante scansioni longitudinali dopo somministrazione endovena di mdc ecogra co , con sonda lineare la532 8 - 3 mhz : esempio di pattern 2a ( a ) impregnazione diffusa disomogenea per la presenza di una singola area priva di enhancement e di pattern 2b ( b ) impregnazione diffusa disomogenea per la presenza di pi aree prive di enhancement . 
a anco , i disegni ( a e b ) chiariscono la diffusione del mdc allinterno della lesione attraverso vasi tti e omogeneamente distribuiti ad eccezione delle aree avascolari . schwannomas , are benign tumours originating in the nerve sheath and are recognisable as fusiform masses arranged eccentrically to the nerve and surrounded by a capsule known as the epineuriu the presence of the capsule allows for complete surgical excision of the lesion . 
a location eccentric to the nerve bres is indicative for a diagnosis of neurinoma , but this nding is not very frequent , and the presence of intralesional cystic spaces is typical of cystic neurinomas but very rare in neuro bromas . 
 our research aimed to investigate this aspect , in part in consideration of the fact that few studies have evaluated the vascular appearance of neurinomas and those that have mente al nervo e circondata da una capsula detta epinevrio . 
la localizzazione eccentrica rispetto alle bre nervose suggestiva per la diagnosi di neurinoma , ma questo riscontro non cos frequente ; la presenza di lacune cistiche intralesionali tipica dei neurinomi , molto rara nei neuro bromi . 
nei casi dubbi , per la mancanza della caratteristica morfologia ecogra ca o della tipica sintomatologia , tipo scossa elettrica , la diagnosi risulta meno agevole . attualmente , grazie allimpiego dei moderni ritrovati tecnologici , possibile aggiungere preziose informazioni circa la distribuzione dei vasi allinterno della lesione [ 1720 ] , sfruttando il massimo segnale armonico proveniente dalle microbolle del mezzo di contrasto ecogra co , quando insonate da un fascio ultrasonoro vicino ai 33 , 5 mhz . 
la nostra ricerca si inserisce in questa prospettiva , anche in considerazione del fatto che gli studi in letteratura internazionale , riguardanti la valutazione dellaspetto vascolare dei neurinomi , sono scarsi e riguardano esclusivamente la rm . 642 radiol med ( 2011 ) 116 : 634643 fig . 
3a , b stessa lesione studiata mediante scansioni longitudinali al pd e dopo somministrazione endovena di mdc ecogra co , con sonda lineare la532 8 - 3 mhz : il pd ( a ) visualizza pochi spot vascolari intralesionali , sottostimando la reale vascolarizzazione della lesione , dimostrata dallenhancement della lesione dopo contrasto ( b )  . were conducted with magnetic resonance imaging . 
the added value of us contrast agents is related to the precise evaluation of the distribution of both large and small blood vessels , which allows differentiation into the two main subtypes : reticular , and diffuse heterogeneous enhancement . 
the recognition of either pattern , associated with the morphological characteristics of the lesion , proved useful in directing us towards the diagnosis . conclusions the results obtained in this study show that all neurinomas examined could be divided into two groups according to the type of vascular pattern observed : reticular , or diffuse heterogeneous enhancement . 
il valore aggiunto del mezzo di contrasto ecogra co dato dalla precisa valutazione della distribuzione dei vasi sia di grandi che di piccole dimensioni , in base alla quale sono stati differenziati due principali pattern di distribuzione : a reticolo e a impregnazione diffusa disomogenea . 
il riconoscimento di uno dei due pattern , associato alla caratteristiche morfologiche della lesione , utile ad indirizzarci verso il sospetto diagnostico . conclusioni dai risultati ottenuti in questo studio si evince che tutti i neurinomi analizzati possono essere distinti in due gruppi , in base al tipo di pattern vascolare riscontrato : di tipo reticolare o ad impregnazione diffusa disomogenea . 
dallesperienza acquisita possiamo affermare che un accurato esame ecogra co di base , mirato alla ricerca delle caratteristiche morfo - strutturali dei neurinomi e delleventuale visualizzazione della continuazione delle bre nervose suggestiva per la diagnosi di neurinoma ; se a questo segue poi lo studio con mdc , il riscontro della tipica distribuzione della vascoradiol med ( 2011 ) 116 : 634643 noma . 
if this is followed up by a contrast - enhanced us examination , the nding of a characteristic vascular pattern in the two subtypes identi ed as reticular ( either loose knit or tight knit ) and diffuse heterogeneous enhancement ( due to the presence of one or more nonenhancing areas ) assists in characterising these masses , thus increasing the operators diagnostic con dence . 
this is particularly useful in doubtful cases , especially in lesions that do not exhibit the typical clinical and morphological features of neurinomas and that may mimic more aggressive lesions . larizzazione nei due pattern identi cati come reticolo ( a maglie larghe o a maglie strette ) e impregnazione diffusa disomogenea ( per la presenza di una o pi aree prive di enhancement ) contribuisce a riconoscere come tali queste formazioni , aumentando cos la con denza diagnostica delloperatore . 
bellomi1 , 3 1department of radiology , european institute of oncology , via ripamonti 435 , 20141 milan , italy 2division of epidemiology and biostatistics , european institute of oncology , milan , italy 3school of medicine , university of milan , milan , italy 4division of thoracic surgery , european institute of oncology , milan , italy correspondence to : s . 
 trans ssural course and type of needle were associated with pneumothorax using univariate analysis , whereas trans ssural course was associated with intrapulmonary haemorrhage using both univariate and multivariate analysis . 
sono state valutate caratteristiche relative al paziente , alla lesione , allago e al tragitto intrapolmonare in relazione al risultato patologico e allesperienza degli operatori , alleventuale presenza post - bioptica di pneumotorace e di soffusione parenchimale . 
 il tragitto trans - scissurale dellago spesso associato radiol med ( 2011 ) 116 : 548563 pneumothorax and intrapulmonary haemorrhage , and the type of the needle is related to pneumothorax . con pneumotorace e soffusione , gli aghi citologici con pneumotorace . keywords ct - guided lung biopsy risk factors complications parole chiave biopsie polmonari tc - guidate fattori di rischio complicanze introduction introduzione the growing use of chest computed tomography ( ct ) and the detection of an increasing number of small lung lesions have heightened the interest in percutaneous ct - guided lung biopsy [ 1 ]  . 
when biopsy is used to de ne the diagnostic and therapeutic workup of a lung lesion , the cost bene t ratio must be carefully evaluated for each patient , resulting in a need to take into consideration the most frequent complications of the procedure : pneumothorax and parenchymal haemorrhage [ 2 , 3 ]  . 
although both complications usually resolve spontaneously , the occurrence of pneumothorax during the procedure may lead to an inconclusive result and , in a variable percentage of cases , worsening pneumothorax may require placement of a chest drain whereas parenchymal haemorrhage may require hospitalisation [ 4 ]  . 
knowledge of the possible risk factors for pneumothorax and parenchymal haemorrhage following ct - guided biopsy allows for more accurate communication with patients when obtaining written informed consent , as well as better organisation of the biopsy procedure . 
many variables have been studied as possible risk factors for pneumothorax and parenchymal haemorrhage , with con icting results [ 57 ]  . the purpose of this study was to assess the correlation between pneumothorax and parenchymal haemorrhage following ct - guided lung biopsies and various risk factors related to the patient , the lesion , the needle path , the operators experience and the type of needle employed . luso crescente della tomogra a computerizzata ( tc ) del torace che porta allindividuazione di un numero sempre pi alto di piccole lesioni polmonari , ha portato ad un sempre maggiore interesse per le biopsie percutanee tc - guidate del torace [ 1 ]  . 
quando la biopsia percutanea serve per de nire liter diagnostico - terapeutico di una lesione polmonare , il rapporto costo / bene cio deve essere attentamente valutato per ogni singolo paziente e pertanto le complicanze pi frequenti della procedura , che sono pneumotorace e soffusione parenchimale , vanno prese in considerazione [ 2 , 3 ]  . 
sebbene di solito entrambe le complicanze si risolvano spontaneamente , linsorgenza di pneumotorace durante la procedura pu portare ad un esito non diagnostico e , in una percentuale variabile di casi , lincremento dello pneumotorace potrebbe richiedere il posizionamento di un drenaggio toracico , mentre la soffusione parenchimale potrebbe richiedere lospedalizzazione [ 4 ]  . 
la conoscenza dei possibili fattori di rischio per linsorgenza di pneumotorace e soffusione parenchimale dopo biopsie tc - guidate permette di comunicare ai pazienti informazioni pi precise al momento della rma del consenso informato , e di organizzare al meglio la procedura bioptica . 
molte variabili sono state studiate come possibili fattori di rischio per linsorgenza di pneumotorace e di soffusione parenchimale , con risultati contrastanti [ 57 ]  . lo scopo di questo studio di valutare la correlazione tra linsorgenza di pneumotorace e di soffusione parenchimale dopo biopsie polmonari tc - guidate , con vari fattori di rischio legati ai pazienti , alla lesione , al tragitto della biopsia , allesperienza degli operatori e al tipo di ago . materials and methods patient selection materiali e metodi selezione dei pazienti a retrospective electronic search on our database of all ct scans performed between january 2007 and july 2008 was carried out to select investigations recorded under the institutional code for thoracic interventional procedure . 
the exclusion criteria were previous lung resection ( because of possible postoperative adhesions that may explain the absence of pneumothorax ) , biopsies performed on mediastinal masses , lesions of pleural origin or presence of pleural effusion . una ricerca elettronica retrospettiva dal nostro database di tutti gli esami tc eseguiti tra gennaio 2007 e luglio 2008 stata condotta al ne di selezionare gli esami registrati con il codice istituzionale di procedura interventistica toracica . 
 i criteri di esclusione sono stati : precedenti resezioni polmonari ( per possibili aderenze post - chirurgiche che possono giusti care lassenza di pneumotorace ) ; biopsie eseguite su masse mediastiniche ; lesioni di origine pleurica ; presenza di versamento pleurico . 
 550 ct parameters all examinations were performed on a 16 - slice lightspeed ct system ( ge medical systems , milwaukee , wi , usa ) and were acquired in a craniocaudal direction from the lung apex to the base . 
iodinated contrast agents used in the period under review were iomeron 350 ( bracco , milan , italy ) , xenetix 350 ( guerbet , paris , france ) and visipaque 320 ( bayer schering pharma , germany )  . 
the scans were acquired in the course of a single inspiratory breath - hold with the following standard scan parameters : collimation 160.625 ( 10 mm ) ; thickness 2.5 mm ; eld of view 320360 mm ; 120 kv ; 240380 ma ( automatic tube current modulation ) ; tube rotation speed 0.8 s ; pitch 1.75 ; standard reconstruction lter ; lung window ( centre 450 , width 1 , 300 )  . ct - guided lung biopsy the indication for the procedure was determined by the patients referring physician and agreed to by the radiologist . 
any platelet antiaggregant and anticoagulant treatments were discontinued prior to the procedure and during subsequent recovery in agreement with the indications of the cardiologist or the haematologist . after establishing the ideal needle path from the skin to the lesion , the acquisition of 15 , 2.5 - mm - thick slices was planned to be repeated as many times as required to follow the needle path throughout the procedure . 
the needles employed were chibell ( biopsybell , modena , italy ) for ne - needle sampling and speedybell ( biopsybell , modena , italy ) for histological core biopsies . 
no on - site pathologist was present during the procedure for immediate evaluation of the biopsy sample . the presence of pneumothorax was evaluated using chest radiography during expiration and / or a ct scan after the procedure . 
if , however , it showed signs of increasing , a thoracic surgeon was consulted to assess the need to place a chest drathe onset of parenchymal haemorrhage was diagnosed when ct showed increased lung attenuation with preserved bronradiol med ( 2011 ) 116 : 548563 parametri tc tutti gli esami sono stati eseguiti su una tc 16 - slice lightspeed ( ge medical system , milwaukee wi , usa ) e sono stati acquisiti in direzione cranio - caudale dagli apici alle basi polmonari . 
i mezzi di contrasto iodati in uso nel periodo in esame sono stati : iomeron 350 ( bracco , milano , italia ) , xenetix 350 ( guerbet , paris , fr ) , visipaque 320 ( bayer schering pharma , germania )  . 
le scansioni sono state acquisite nel corso di ununica apnea inspiratoria con i seguenti parametri standardizzati : collimazione 160 , 625 ( 10 mm ) ; spessore 2 , 5 mm ; campo di vista 320360 mm ; 120 kv ; 240380 ma ( modulazione automatica della corrente del tubo ) ; 0 , 8 secondi di rotazione del tubo ; pitch 1 , 75 ; ltro di ricostruzione standard ; nestra di visualizzazione per polmone ( centro 450 , ampiezza 1300 )  . 
la coagulazione dei pazienti stata sempre valutata prima della biopsia attraverso i seguenti esami ematobiochimici : attivit di protrombina ( pa ) , tempo di tromboplastina parziale ( ptt ) e international normalized ratio ( inr ) , con valori normali rispettivamente di : 70%120% , 1726 s , e 0 , 81 , 2 . 
 dopo aver stabilito il tragitto ideale dellago dalla cute alla lesione , stata programmata unacquisizione di 15 fette di 2 , 5 mm di spessore da ripetere tante volte quante necessario per seguire il percorso dellago durante la procedura . 
gli aghi usati sono stati : chibell ( biopsybell , modena , italia ) per prelievi con ago sottile , e speedybell ( biopsybell , modena , italia ) per biopsie istologiche ( corebiopsy )  . 
 nel caso in cui lo pneumotorace fosse stabile o ridotto , il paziente stato dimesso ; nel caso in cui fosse invece incrementato , stato consultato un chirurgo toracico per valutare la possibilit di posizionare un drenaggio toracico . 
 linsorgenza di soffusione parenchimale stata diagnosticata quando la tc ha mostrato , lungo il tragitto dellago , un aumento di densit del polmone , con conservazione dei radiol med ( 2011 ) 116 : 548563 chial and vascular margins along the needle path . 
leventuale ospedalizzazione stata considerata valutando la clinica del paziente . quanti cazione dellen sema emphysema quanti cation data from the chest ct scans obtained at the time of the procedure were transferred from the digital archive to a workstation ( advantage windows , ge medical systems )  . 
 the values for total lung volume , and volume and percentage of emphysema , were obtained with a software package for the semiautomatic calculation of lung density ( volume viewer 2 , ge medical systems ) and entered on an excel spreadsheet ( microsoft of ce excel 2003 , richmond , va , usa )  . 
lung volume was calculated from scans reconstructed at a thickness of 2.5 mm by selecting a threshold between 1023 and 200 houns eld units ( hu ) to exclude both the soft tissue around the lung and the large intrapulmonary vessels . 
the speci c threshold used to discriminate normal from emphysematous lung parenchyma was 950 hu , an experienced radiologist manually selected and excluded measurement of air contained in the colon , trachea and main bronchi if it was included in the reconstructed volume . other factors on the basis of ct images , the following factors were also recorded and taken into account : patient position ( supine , lateral , prone ) ; needle access site ( anterior , lateral , posterior ) ; lesion site ( upper right , middle , lower right , upper left , lower left lobe ) ; lesion type ( solid , partially solid , nonsolid ) and trans ssural needle path ( present or absent )  . 
 elements recorded by the reporting workstation ( advantage windows , ge medical systems ) were : lesion diameter , angle of incidence between needle and pleura ( indicated as perpendicular if equal to 9010 and oblique in all other cases ) and length of the needles intrapulmonary trajectory . 
 needle characteristics noted were : type ( aspiration or core biopsy ) and diameter ( expressed in gauge )  . ct - guided lung biopsies were performed by one of ten radiologists , each with at least 2 years of experience , subdivided into two groups according to experience level : group 1 , with < 150 biopsies ; group 2 , with > 150 biopsies . 
 cytohistological biopsy reports ( provided by the pathologist within 1 week ) were reviewed , along with a short medical history regarding possible previous malignancies and associated therapies . i dati ottenuti dalle scansioni tc del torace acquisite al momento della procedura sono stati trasferiti dallarchivio digitale ad una workstation ( advantage windows , ge medical system , milwaukee , wi , usa )  . 
i valori del volume polmonare totale , del volume dellen sema e della percentuale di en sema sono stati ottenuti utilizzando un software per il calcolo semi - automatico della densit polmonare ( volume viewer 2 , ge medical system , milwaukee , wi , usa ) e registrate su un foglio di lavoro excel ( microsoft of ce excel 2003 , richmond , usa )  . 
il volume polmonare stato calcolato da scansioni ricostruite a spessore di 2 , 5 mm selezionando una soglia compresa tra 1023 e 200 unit houns eld ( hu ) , per escludere sia i tessuti molli attorno al polmone che i grossi vasi intrapolmonari . 
 altri fattori considerati sulla base delle immagini tc , sono stati considerati e registrati anche i seguenti fattori : posizione del paziente ( supina , laterale o prona ) ; posizione di accesso dellago ( anteriore , laterale o posteriore ) ; sede della lesione ( lobo superiore destro , lobo medio , lobo inferiore destro , lobo superiore sinistro , lobo inferiore sinistro ) ; tipo di lesione ( solida , parzialmente solida , non solida ) ; tragitto transscissurale dellago ( presente o assente )  . 
elementi registrati dalla workstation di refertazione ( advantage windows , ge medical system , milwaukee , wi , usa ) sono stati : diametro della lesione ; angolo di incidenza tra ago e pleura ( indicato come perpendicolare se uguale a 9010 e obliquo in tutti gli altri casi ) , lunghezza del tragitto intrapolmonare dellago . 
 le biopsie tc - guidate del polmone sono state eseguite da dieci diversi radiologi con almeno 2 anni di esperienza , suddivisi in base alla esperienza personale in due gruppi : gruppo 1 con esperienza < 150 biopsie , gruppo 2 con esperienza > 150 biopsie . 
il referto cito - istologico della biopsia ( fornito dal patologo entro 1 settimana ) stato valutato insieme ad una breve anamnesi su eventuali precedenti patologie oncologiche e terapie connesse . 
 statistical analysis analisi statistica baseline characteristics of the study population are le caratteristiche basali della popolazione in studio sono 552 radiol med ( 2011 ) 116 : 548563 expressed as meanstandard deviation ( sd ) for continuous variables and as frequencies and percentages for categorical variables . 
the nonparametric wilcoxon test was used to assess whether continuous variables differed signi cantly between patients exhibiting the complications under review and patients without such complications . factors identi ed by univariate analysis as being signi cantly associated with the presence of postbiopsy complications were subsequently included in multivariate logistic regression models to assess their contribution , independent of other variables , to the occurrence of parenchymal haemorrhage and pneumothorax . 
 the risk of having a complication in our sample was estimated as : e ( o + i xi ) l + e ( o + i xi ) where 0 is the intercept calculated in the multivariate logistic regression model and i represent the coef cient of the variable xi . 
the above - described statistical analyses were carried out using sas software , version 8.2 ( sas institute inc . , cary , nc , usa )  . state espresse come media deviazione standard per le variabili continue , come frequenze e percentuali per le variabili categoriche . 
il test non parametrico di wilcoxon stato utilizzato per valutare se le variabili continue erano signi cativamente differenti tra i pazienti con le complicanze in esame rispetto ai pazienti senza complicanze . 
 i fattori identi cati come signi cativamente associati alla presenza di complicanze post - bioptiche nellanalisi univariata sono stati successivamente inclusi in modelli di regressione logistica multivariata , per valutare come contribuivano indipendentemente da altre variabili , allinsorgenza di soffusione parenchimale e di pneumotorace . 
 il rischio di avere una complicanza nel nostro campione e stata stimata come : e ( o + i xi ) l + e ( o + i xi ) dove 0 lintercetta calcolata nella regressione logistica multivariata e i il coef ciente della variabile xi . 
laccuratezza del modello nel predire il rischio di complicanze nel nostro campione stata misurata con la statistica c e rappresentata gra camente da curve roc ( receiver operating characteristics )  . 
le suddescritte analisi statistiche sono state effettuate utilizzando il software sas , versione 8.2 ( sas institute inc . , cary , nc , usa )  . results risultati out of 222 procedures performed , 157 were included in the study . 
none of the values relating to emphysema , assessed in 138 / 157 ( table 1 ) , was found to be signi cant for the occurrence of pneumothorax and effusion . 
patient position , needle site , location of the lobe containing the lesion , type of nodules and angle between the needle and the parietal pleura demonstrated no signi cant association with the onset of parenchymal haemorrhage and pneumothorax . average lesion diameter was 40.1125.58 mm and was nel presente studio sono state incluse 157 / 222 procedure eseguite . 
la posizione dei pazienti , laccesso dellago , la sede del lobo della lesione , il tipo di noduli e langolo di incidenza tra lago e la pleura parietale , non hanno mostrato alcuna associazione signi cativa con linsorgenza di soffusione parenchimale e pneumotorace . 
similarly , pneumothorax rate was lower for larger lesions , ranging from 61% for il diametro medio delle lesioni stato di 40 , 1125 , 58 millimetri , ed risultato associato ( p < 0 , 05 ) con la soffusione parenchimale e con lo pneumotorace sia allanalisi univariata che alla multivariata . 
analogamente , la percentuale di pneumotorace stata inferiore per lesioni di dimensioni maggiori , passando dal 61% per lesioni < 20 mm al 19% per lesioni > 60 mm ( adjusted odds ratio 0 , 16 ( 0 , 050 , 59 ) )  . 
multivariate analysis showed that for every 10 - mm increase in length of the intrapulmonary trajectory increased the risk of pneumothorax and parenchymal haemorrhage by 3% ( adjusted or for both of 1.03 ; 95% ci 1.011.05 ) ] ( table 2 )  . 
lanalisi multivariata ha mostrato che per ogni aumento della lunghezza del tragitto intrapolmonare dellago di 10 mm , aumenta il rischio di soffusione pa556 parenchymal haemorrhage occurring in 9 / 12 ( 75% ) of cases and pneumothorax in 10 / 12 ( 83% )  . 
multivariate analysis showed that a trans ssural path increased the risk of parenchymal haemorrhage and pneumothorax fourfold ( table 2 ) , although this increased risk was statistically signi cant ( p < 0.05 ) for parenchymal haemorrhage only . 
on the other hand , a small but signi cant correlation ( p < 0.04 ) was identi ed between the type of needle used and the type of nodule , as cytology needles were used more frequently than core - biopsy needles for procedures performed on nonsolid nodules . 
on multivariate analysis , only a marginal association was found between the needle type and pneumothorax risk . the risk of a complication developing in our study population was calculated using the coef cients of the complete model with the continuous variables shown in table 2 . 
 for example , a patient with a lesion diameter of 30 mm , an intrapulmonary needle trajectory of 50 mm , the use of a radiol med ( 2011 ) 116 : 548563 fig . 
il tragitto intrapolmonare dellago stato di 77 mm ( a ) e lungo il percorso dellago si veri cata linsorgenza di soffusione parenchimale appena dopo la procedura ( b )  . renchimale e di pneumotorace del 3% ( valori di adjusted odds ratio per entrambi 1 , 03 ( 1 , 011 , 05 ) ) ( tabella 2 )  . 
 il tragitto dellago stato trans - scissurale in 12 casi ( 8% ) ed risultato signi cativamente associato ( p < 0 , 05 ) ad entrambe le complicanze allanalisi univariata : in 9 / 12 ( 75% ) casi si veri cata soffusione parenchimale , in 10 / 12 ( 83% ) pneumotorace . 
il decorso transcissurale ha aumentato di oltre 4 volte il rischio di soffusione parenchimale e pneumotorace ( tabella 2 ) alla analisi multivariata , sebbene tale incremento del rischio sia risultato statisticamente signi cativo ( p < 0 , 05 ) solo per le soffusioni parenchimali . 
2 axial computed tomography image showing the onset of pneumothorax during a lung biopsy performed with a 22 - gauge aspiration needle on a partially solid nodule of the lower right lobe . 
2 immagine tc assiale che mostra linsorgenza di pneumotorace nel corso di una biopsia polmonare eseguita usando un ago per prelievo citologico da 22 g , in un nodulo parzialmente solido del lobo inferiore di destra . 
3 axial computed tomography image showing no pneumothorax during a lung biopsy performed with an 18 - gauge core biopsy needle on a solid nodule of the lower right lobe . 
histological ndings of biopsies showed primary lung cancer in 100 cases , absence of cancer in 22 , metastases in 13 and inadequate material in 22 cases ( 16 / 22 obtained with aspiration biopsy )  . 
4 axial computed tomography image showing a percutaneous lung biopsy of a nonsolid nodule using a 25 - gauge aspiration needle , and onset of subtle pneumothorax during the procedure . 
4 immagine tc assiale che mostra una biopsia polmonare di un nodulo non solido eseguita con un ago citologico da 25 g e linsorgenza di una sottile falda di pneumotorace nel corso della procedura . 
il materiale estratto stato comunque suf ciente al patologo per fare diagnosi di carcinoma polmonare non a piccole cellule . gli aghi per prelievi istologici ( core biopsy ) in 102 / 157 casi ( 65% )  . 
daltra parte , si riscontrata una correlazione leggermente signi cativa ( p < 0 , 04 ) tra il tipo di ago usato e il tipo di nodulo , poich lago per prelievo citologico stato usato pi frequentemente rispetto allago per core biopsy nelle procedure eseguite su noduli non solidi . 
 allanalisi multivariata , si riscontrata unassociazione solo marginale tra il tipo di ago e il rischio di pneumotorace . il rischio di avere una complicanza nei pazienti inclusi nel nostro studio pu essere calcolato usando i coef cienti del modello completo con le variabili continue presentate nella tabella 2 . 
in this study , the rate of pneumothorax fell within this range ( 46% ) , even though a minimal amount air in the pleural cavity was considered evidence of pneumothorax . 
indeed , multivariate analysis shows an increased risk of pneumothorax and parenchymal haemorrhage with decreasing lesion diameter , with a reduction in laccuratezza del modello multivariato nel prevedere il veri carsi di complicanze 0 , 76 e 0 , 79 per le soffusioni parenchimali e per il pneumotorace , rispettivamente . 
le curve roc per il modello completo modi cato e per i modelli che includono solo la dimensione della lesione e il tragitto intrapolmonare dellago , sono presentate nelle figure 5 e 6 . le biopsie polmonari tc - guidate sono state eseguite da dieci radiologi differenti e nessuna correlazione signi cativa stata riscontrata tra lesperienza degli operatori e il veri carsi delle due complicanze in esame . 
i risultati istologici delle biopsie hanno dimostrato un tumore primitivo polmonare in 100 casi ; assenza di patologia oncologica in 22 casi ; metastasi in 13 casi ; materiale inadeguato in 22 casi ( 16 / 22 ottenuti da aspirati citologici )  . 
6 curve roc del modello modi cato completo e dei modelli che includono solo la dimensione della lesione e la biopsia intrapolmonare per linsorgenza di pneumotorace . risk of 4% and 3% , respectively , for each increasing increment of 10 mm in the lesions diameter . 
in the case of pneumothorax , this may be due to the number of pleural needle passes required to obtain correct needle direction , which increases the number of minor pleural injuries ; in the case of parenchymal haemorrhage , it is perhaps a result of the quantity of lung parenchyma traversed by the needle . 
have shown a high rate of complications for smaller lesions , with a particularly signi cant relationship between smaller lesion size and risk of parenchymal haemorrhage [ 3 ]  . 
showed a similar rate of pneumothorax for both small and large pulmonary nodules , with a diameter of 15 mm representing the threshold between the two groups [ 15 ]  . 
il 69 % ( 9 / 13 ) di questi pazienti era stato sottoposto a chemioterapia o ormonoterapia in passato . discussione le percentuali di pneumotorace dopo biopsie polmonari tc - guidate , riportate in letteratura , variano dal 4% [ 8 ] al 62% [ 9 ]  . 
in questo studio , la percentuale di complicanze compresa in questo range ( 46% ) , nonostante anche falde aeree pleuriche di minima entit comparse dopo la procedura siano state considerate come presenza di pneumotorace . 
infatti , lanalisi multivariata mostra un rischio maggiore di pneumotorace e soffusione parenchimale quando si riduce il diametro della 560 radiol med ( 2011 ) 116 : 548563 lesione , con una riduzione del rischio rispettivamente del 4% e del 3% , per ogni incremento di 10 mm del diametro della lesione . 
questo potrebbe essere dovuto : per il pneumotorace al numero di passaggi necessari per ottenere la corretta direzione dallago , che incrementerebbe il numero di piccoli traumi sulla pleura ; per la soffusione emorragica alla quantit di parenchima polmonare attraversata dallago . 
al contrario , yeow et al non hanno riscontrato alcuna associazione tra il diametro della lesione e linsorgenza di pneumotorace , ma hanno comunque mostrato una correlazione tra dimensione della lesione e soffusione allanalisi univariata [ 14 ]  . 
 [ 15 ] hanno mostrato una percentuale di pneumotorace analoga per noduli polmonari piccoli e grandi , usando come limite tra i due gruppi un diametro di 15 mm . la lunghezza del tragitto intrapolmonare risultata associata in modo signi cativo allinsorgenza di soffusione e pneumotorace . 
 [ 14 ] hanno mostrato che un lungo tragitto intrapolmonare dellago il pi importante fattore predittivo di soffusione parenchimale , con la pi alta percentuale di soffusione in particolare per le lesioni distanti pi di 20 mm dalla parete . 
altri studi hanno mostrato che la lunghezza del tragitto intrapolmonare signi cativamente associata con la soffusione [ 16 ] o lo pneumotorace [ 2 , 13 , 17 ]  . 
 [ 18 ] , un tragitto pi lungo dellago potrebbe danneggiare la pleura e il parenchima polmonare con maggior probabilit , giusti cando lalta percentuale di pneumotorace e soffusione intrapolmonare . 
dallanalisi multivariata effettuata sui fattori considerati in questo studio , il rischio di soffusione e pneumotorace aumenta del 3% per ogni aumento di 10 mm della lunghezza del tragitto intrapolmonare dellago . 
 [ 20 ] , rispetto alle nostre ( 12 / 157 ) , si dovrebbero raccogliere pi casi e correlarli al tipo di ago utilizzato come fattori indipendenti . allanalisi univariata abbiamo riscontrato una differenza signi cativa nellinsorgenza di pneumotorace per il fig . 
8 immagine dettagliata e ingrandita della punta di un ago per prelievo istologico ( cortesemente fornita da biopsybell )  . most important predictor of parenchymal haemorrhage , the highest rates of haemorrhage being observed in lesions > 20 mm from the wall [ 14 ]  . 
 other studies have shown that the length of the intrapulmonary trajectory is signi cantly associated with haemorrhage [ 16 ] or pneumothorax [ 2 , 13 , 17 ]  . 
as suggested by kinoshita et al . , a longer needle trajectory may be more likely to damage the pleura and pulmonary parenchyma , explaining the high rate of pneumothorax and intrapulmonary haemorrhage [ 18 ]  . 
multivariate analysis of the factors considered in this study shows that the risk of haemorrhage and pneumothorax increases by 3% with each increase of 10 mm in the length of the intrapulmonary needle trajectory . 
compared with our own experience ( 12 / 157 ) , we need to gather more cases and correlate them with the types of needle used as independent factors . univariate analysis revealed a signi cant difference in the onset of pneumothorax by type of needle used , regardless of its diameter . 
showed a higher rate of pneumothorax occurring with needle aspiration ( 40% ) than with core biopsies ( 24.3% ) [ 21 ]  . in our series , there was a higher rate of parenchymal haemorrhage in lesions that proved to be metastatic , which was unrelated to coagulation disorders in the patient . 
 because of the small number of this subset of patients and the lack of further information on risk factors for bleeding , larger studies are needed to determine whether previous treatments may have damaged the patients entire microvasculature , including pulmonary vessels [ 22 , 23 ]  . strangely , in our series , there was no correlation between emphysema extent and the development of pneumothorax . 
although there is still no unanimous opinion on the threshold in terms of houns eld units to be used to discriminate emphysematous and normal lung parenchyma , we chose a threshold of 950 hu , as it has been shown at both macroscopic and microscopic levels to provide good quanti cation of emphysema extent on thin - slice ct [ 25 , 2730 ]  . 
showed that patients with severe respiratory impairment have a high prevalence of pneumothorax [ 10 ] , but this difference could be related to the use of spirometry values to quantify the emphysema . 
however , in our series , emphysema was calculated for the entire parenchyma and not in particular for the portion of lung parenchyma traversed by the needle . as in previous reports [ 31 , 32 ] , this study found a lower percentage of inadequate samples with core biopsies than with aspiration biopsy . one limitation of this study is that there was no use of coaxial needles , as it was a retrospective study and coaxial needles were not used at our institution during the period tipo di ago usato , indipendentemente dal diametro dellago . 
a causa del piccolo numero di questo sottogruppo di pazienti e dellassenza di maggiori informazioni sui fattori di rischio per sanguinamento , sarebbero necessari studi pi ampi per stabilire se le precedenti terapie possano aver danneggiato la microvascolarizzazione dellintero organismo , ivi inclusi i vasi polmonari [ 22 , 23 ]  . 
sebbene non vi sia ancora un parere unanime sulla soglia in unit houns eld ( uh ) da usare per discriminare il parenchima polmonare en sematoso da quello normale , la soglia di - 950 uh stata scelta in questo studio perch stato dimostrato sia a livello macroscopico che microscopico che quanti ca bene lentit dellen sema in esami tc a strato sottile [ 25 , 2730 ]  . 
 [ 10 ] hanno mostrano che i pazienti con una severa compromissione della funzionalit respiratoria hanno avuto unalta prevalenza di pneumotorace [ 10 ] , ma questa differenza potrebbe essere legata alluso di valori spirometrici per quanti care len sema . 
tuttavia , nella nostra casistica len sema stato calcolato per lintero parenchima , e non in particolare per la parte di parenchima polmonare attraversata dallago . analogamente a studi precedenti [ 31 , 32 ] , in questo studio si ottenuta una percentuale pi bassa di materiale inadeguato per le core biopsies rispetto ai prelievi citologici . un limite di questo studio che non stato incluso alcun utilizzo di aghi co - assiali , poich uno studio retrospettivo e durante il periodo in esame gli aghi coassiali non erano in uso presso la nostra divisione . 
another limitation is that we did not investigate the rationale behind the choice of aspiration or core - biopsy needles for each procedure , and this may have in uenced the occurrence of complications . 
we have , however , shown that in this series , the choice of an aspiration needle was in uences by nodule characteristics rather than by distance of the lesion from the wall , and that an aspiration needle was preferred for nonsolid nodules . 
furthermore , in our series the number of pleural passes was not included among the variables assessed , as a retrospective evaluation of this parameter could perhaps only have been obtained by counting the number of ct series acquired during each procedure . 
however , this number may not re ect the real number of pleural passes , and it was therefore omitted from the collection of data on possible risk factors . permettendoci di eseguire , relativamente alle variabili in esame , unanalisi statistica adeguata . 
un altro limite che non abbiamo indagato il razionale nella scelta degli aghi per prelievo citologico o istologico in ogni singola procedura , e questo potrebbe aver in uenzato linsorgenza di complicanze . 
tuttavia abbiamo dimostrato che in questa casistica la scelta di un ago per prelievo citologico non stata in uenzata dalla distanza della lesione dalla parete , ma dalle caratteristiche del nodulo , ed stato preferito lago per prelievo citologico per noduli non solidi . 
inoltre , nella nostra casistica il numero di passaggi pleurici non stato incluso tra le variabili valutate , poich in una valutazione retrospettiva questo parametro sarebbe stato forse ottenibile solo contando il numero delle serie tc acquisite durante la procedura , ma questo dato potrebbe non ri ettere il numero reale di passaggi pleurici , pertanto stato omesso dalla raccolta dei dati relativa ai possibili fattori di rischio . conclusions statistically signi cant features for the occurrence of pneumothorax and pulmonary haemorrhage following ct - guided lung biopsies were smaller lesions and long intrapulmonary needle trajectory . 
no signi cant association was found between complication onset and the other risk factors investigated , including emphysema , t nodule type , patient position , needle access site , angle between the needle and pleura and needle gauge . conclusioni caratteristiche statisticamente signi cative per linsorgenza di pneumotorace e soffusione polmonare dopo biopsie polmonari tc - guidate sono risultate : piccole dimensioni delle lesioni e lungo tragitto intrapolmonare dellago ; il tragitto transcissurale dellago risultato rilevante per la soffusione intrapolmonare ; il tipo di ago appare invece correlato allinsorgenza di pneumotorace . 
we identi ed 7 / 23 benign lesions ( three myxoid , four nonmyxoid ) and 16 / 23 malignant tumours ( four myxoid , 12 nonmyxoid ) with a mean diameter between 21 mm and 20 cqualitative analysis of dwi showed persistence of high signal intensity for increasing b - values in all malignant tumours . 
abbiamo riscontrato 7 / 23 lesioni benigne ( 3 a matrice mixoide , 4 non mixoide ) e 16 / 23 maligne ( 4 a matrice mixoide , 12 non mixoide ) , con diametro compreso tra 21 mm e 20 clanalisi qualitativa della dwi ha dimostrato persistenza delliperintensit di segnale al crescere dei tre b value in tutte le lesioni maligne . 
 parole chiave rm diffusione dwi tumori dei tessuti molli sarcoma radiol med ( 2011 ) 116 : 644656 introduction introduzione magnetic resonance ( mr ) imaging plays a major role in diagnosis , staging and follow - up of soft - tissue tumours . 
in recent years , dwi has been used to characterise soft - tissue tumours and differentiate benign from malignant lesions [ 7 , 8 ] and to monitor the ef cacy of treatment in patients affected by sarcoma [ 9 , 10 ]  . 
 the aim of this study was to evaluate the role of mr imaging with spin - echo echo - planar diffusion - weighted imaging ( se - epi - dwi ) in characterising primary and secondary tumours of the soft tissues by correlating qualitative and quantitative dwi data with the results of histology . materials and methods between june 2008 and may 2009 , we retrospectively reviewed 23 patients ( 14 men , nine women ; median age 70 years ; range 2587 ) at rst diagnosis of a soft - tissue mass . 
included in the study were also the most common lesions that enter into the differential diagnosis with primary soft - tissue tumours , such as muscular metastasis , lymphomas and schwannomas . 
diagnostic workup prior to mr examination included ultrasound ( us ) in eight patients , us and computed tomography ( ct ) in ve , ct in ve and no examination in four ; one patient had directly undergone biopsy . 
all lesions were subjected to histological assessment following biopsy ( 11 / 23 ) or surgical excision ( 9 / 23 ) ; in 3 / 23 patients , the lesion was surgically excised after biopsy . 
mr imaging was done with a 1.5 - t superconductive magnet ( avanto , siemens medical solutions , forcheim , germany ) , gradient strength 45 mt / m , slew rate 200 t / m / ms and phased - array surface coil . 
lesions were studied at baseline ( precontrast scan ) with the following sequences : axial t1 - se ( tr 610 ms , te 11 ms , fa 150 , matrix 281448 , acceleration factor 2 , thickness 3 mm ) ; axial t1 - se fat la risonanza magnetica ( rm ) riveste un ruolo importante nella diagnosi , nello staging e nel follow - up delle neoplasie dei tessuti molli . 
recentemente la dwi stata utilizzata per caratterizzare i tumori dei tessuti molli , differenziando i tumori benigni dai tumori maligni [ 7 , 8 ] , e controllare i risultati del trattamento in pazienti affetti da sarcoma [ 9 , 10 ]  . 
 lo scopo di questo lavoro valutare il ruolo della rm con sequenze spin echo ( se ) - echo planar imaging ( epi ) diffusion - weighted imaging ( dwi ) nella caratterizzazione dei tumori primitivi e secondari dei tessuti molli , correlando i dati qualitativi e quantitativi offerti dallimaging dwi con i riscontri anatomopatologici ( istologici )  . materiali e metodi sono stati valutati retrospettivamente , nel periodo compreso tra giugno 2008 e maggio 2009 , 23 pazienti ( 14 maschi , 9 femmine , di et compresa tra i 2587 anni , et mediana 70 anni ) con tumefazioni dei tessuti molli al primo riscontro . 
i criteri di esclusione hanno previsto i pazienti gi sottoposti a chemioe radioterapia ed i pazienti con lipoma tipico , prevedendo la sequenza dwi un pre - impulso di radiofrequenza per la soppressione del segnale del grasso . 
 nello studio sono state comprese anche le lesioni pi comuni che entrano in diagnosi differenziale con i tumori primitivi dei tessuti molli come le metastasi muscolari , i linfomi e gli schwannomi . 
nelliter diagnostico precedente allindagine rm , 8 pazienti avevano eseguito una ecogra a , 5 pazienti una ecogra a ed una tomogra a computerizzata ( tc ) , 5 pazienti una tc e 4 pazienti nessun esame ; in un 1 paziente era stata eseguita direttamente la biopsia . 
tutte le lesioni sono state sottoposte ad esame istologico dopo biopsia ( 11 / 23 pazienti ) o ad asportazione chirurgica ( 9 / 23 pazienti ) ; in 3 / 23 pazienti dopo la biopsia si proceduto ad asportazione chirurgica della lesione . 
lindagine rm stata eseguita in tutti i pazienti con apparecchiatura dotata 646 radiol med ( 2011 ) 116 : 644656 saturation ( fat - sat ) ( tr 610 ms , te 11 ms , ti 150 ms , fa 150 , matrix 281448 , acceleration factor 2 , thickness 3 mm ) , coronal t2 - se - fat - sat ( tr 4 , 000 ms , te 265 ms , ti 150 ms , fa 150 , matrix 314448 , acceleration factor 2 , thickness 3 mm ) , single - shot ( ss ) - se - epi - dwi with three different b values ( 50 - 400 - 800s / mm2 ) and parallel imaging with an acceleration factor of 2 [ interactive project for assistive technology ( ipat ) - 2 ]  . 
subsequently , all patients were imaged with t1 - weighted se sequences ( tr 610 ms , te 11 ms , fa 150 , matrix 281448 , acceleration factor 2 , thickness 3 mm ) after the intravenous administration of 0.2 mmol / kg paramagnetic contrast material ( magnevist , bayer schering pharma , berlin , germany )  . 
the ss - se - epi - dwi sequence has the following technical parameters : tr 4 , 100 ms , te 70 ms , ti 150 ms , matrix 160160 , slice thickness 6 mpost - processing was performed on a dedicated workstation ( leonardo , siemens medical solutions , forchheim , germany )  . 
lesions were histologically classi ed into benign and malignant according to the world health organization ( who ) classi cation of soft tissue tumors [ 11 ] and subdivided into myxoid or nonmyxoid depending on the amount of myxoid matrix ( table 1 )  . 
the qualitative analysis of the dwi evaluated the loss of high signal intensity with increasing b values ( from the lowest value of 50s / mm2 to the highest of 800s / mm2 )  . 
persistence of high signal intensity with increasing b values was evaluated semiquantitatively using the following scale : + + + marked persistence of signal ; + + good persistence of signal ; + poor persistence of signal ; absence of signal . quantitative analysis was obtained by mathematically calculating the apparent diffusion coef cient ( adc )  . 
adc maps are automatically generated by the workstation based on the three b values according to the formula adc = ln ( s0 / s1 ) / ( b1 - b0 ) , where s0 and s1 are the signal intensity before and after application of diffusion gradients , and b1 and b0 are the different b values applied . 
values of the considered variables ( b50 , b400 , b800 , adc ) were compared between the group of seven benign lesions and the group of 16 malignant lesions using the nonparametric mannwhitney u test . 
to evaluate di magnete superconduttivo da 1 , 5 t ( avanto , siemens medical solutions , forcheim , germania ) , intensit di risalita dei gradienti di 45 mt / m , slew rate di 200 t / m / ms , bobina di super cie phased - array . 
lo studio delle lesioni stato condotto nelle condizioni di base mediante sequenze t1 - se assiale ( tempo di ripetizione [ tr ] 610 ms , tempo di eco [ te ] 11 ms , ip angle [ fa ] 150 , matrice 281448 , fattore di accelerazione 2 , thickness 3 mm ) , t1 - se - fat - sat assiale ( tr 610 ms , te 11 ms , ti 150 ms , fa 150 , matrice 281x448 , fattore di accelerazione 2 , thickness 3 mm ) , t2 - se con saturazione del grasso ( fat - sat ) coronale ( tr 4000 ms , te 265 ms , tempo di inversione [ ti ] 150 ms , fa 150 , matrice 314448 , fattore di accelerazione 2 , thickness 3 mm ) , single shot ( ss ) - se - epi - dwi con 3 differenti valori di b value ( 50 - 400 - 800 s / mm2 ) ed imaging parallelo con fattore di accelerazione pari a 2 ( ipat - 2 )  . 
successivamente in tutti i pazienti sono state acquisite sequenze se t1 pesate ( tr 610 ms , te 11 ms , fa 150 , matrice 281448 , fattore di accelerazione 2 , thickness 3 mm ) dopo somministrazione ev di 0 , 2 mmol / kg di mezzo di contrasto ( mdc ) paramagnetico ( magnevist , bayer schering pharma , berlino , germania )  . 
la sequenza ss - se - epi - dwi impiegata nello studio prevede i seguenti parametri tecnici : tr 4100 ms , te 70 ms , ti 150 ms , matrice 160160 , slice thichness 6 mil post - processing stato eseguito su consolle dedicata ( leonardo , siemens medical solutions , forcheim , germania )  . 
 lanalisi delle immagini stata effettuata , separatamente , da due radiologi ( eg , mga ) esperti in risonanza magnetica , con particolare riferimento alla patologia muscolo - scheletrica , non sono emerse discordanze tra i risultati . 
le lesioni sono state classi cate istologicamente in benigne e maligne secondo la world health organization ( who ) classi cation of soft tisssue tumors [ 11 ] e suddivise a seconda della loro matrice mixoide e non mixoide ( tabella 1 )  . 
lanalisi qualitativa delle immagini dwi stata effettuata valutando la perdita di iperintensit di segnale nella successione di 3 valori di b value ( dal valore pi basso di 50 s / mm2 , a quello pi alto di 800 s / mm2 )  . 
la persistenza delliperintensit di segnale al crescere dei tre b value stata valutata semi - quantitativamente utilizzando la scala di valori sotto riportata : + + + notevole persistenza di segnale ; + + buona persistenza di segnale ; + scarsa persistenza di segnale ; assenza di segnale . lanalisi quantitativa stata ottenuta mediante calcolo matematico del valore del coef ciente di diffusione apparente ( adc )  . 
i valori delle variabili prese in considerazioni ( b50 , b400 , b800 , adc ) sono state confrontate tra il gruppo delle 7 lesioni benigne e quello delle 16 lesioni maligne con il test non parametrico di mann - whitney . 
 qualitative analysis of dwi demonstrated persistence of high signal intensity with increasing b values ( 50 - 400800 s / mm2 ) in all malignant lesions , although with differences among the various histological types ( table 1 )  . 
le lesioni maligne a matrice mixoide ( 4 pazienti ) hanno compreso i liposarcomi mixoidi g1 e g3 , il mixo brosarcoma ad alto grado , il sarcoma polimorfo con componente mixosarcomatosa . 
low adc values were obtained in lymphomas ( lowest value 0.410.2610 - 3 mm2 / s ) , in muscular metastases from in ltrating ductal breast cancer ( 0.9680.7610 - 3 mm2 / s ) and in the hepatocellular carcinoma ( 1.0100.5010 - 3 mm2 / s ) , all classi ed as nonmyxoid malignant lesions . 
high adc values were recorded in the elasto bromas , with adc between 1.310.4610 - 3mm2 / s and 1.340.510 - 3 mm2 / s , classi ed as nonmyxoid malignant lesions . 
in the single case of softtissue localisation of castlemans disease , we obtained an adc value of 0.780.9010 - 3 mm2 / s , similar to lymphomas , and for this reason , they were included among lesions with benigne a matrice mixoide ( 3 pazienti ) abbiamo inserito lo schwannoma , il neuro broma e langiomixoma . 
 lanalisi qualitativa della dwi ha dimostrato la persistenza delliperintensit di segnale al crescere dei tre b value ( 50 - 400 - 800 s / mm2 ) in tutte le lesioni maligne , anche se in misura differente nei diversi istotipi tumorali ( tabella 1 )  . 
c - e sequenze ssse - epi - dwi acquisite con tre differenti b value ( 50 , 400 , 800 s / mm2 ) : assenza di iperintensit di segnale al crescere del b value . a high grade of biological activity . 
we found a small difference between adc values of the schwannoma ( 1.740.8110 - 3 mm2 / s ) and the myxoid liposarcoma ( 1.560.1710 - 3 mm2 / s ) , but the difference was suf cient to enable distinction between benign and malignant lesions , according to our ndings . 
 statistical analysis conducted with the mannwhitney u test for each parameter considered separately ( b50 , b400 , b800 and adc ) demonstrated a signi cant difference ( p < 0.05 ) between the group of seven benign lesions and that of 16 malignant lesions . 
roc curve analysis allowed us to establish the sensitivity and speci city of each parameter considered ( b50 , b400 , b800 and adc ) in discriminating between benign and malignant lesions . 
 the area under the curve ( auc ) at the cutoff point ( below which are lesions with a low grade of biological activity 0 , 410 , 2610 - 3 mm2 / s ) , nelle metastasi muscolari da carcinoma duttale in ltrante della mammella ( 0 , 9680 , 7610 - 3 mm2 / s ) e nel epatocarcinoma ( hcc ) ( 1 , 0100 , 5010 - 3 mm2 / s ) , classi cati come lesioni maligne non mixoidi . 
elevati valori di adc sono riscontrati negli elasto bromi , con adc compreso tra 1 , 310 , 4610 - 3 mm2 / s e 1 , 340 , 510 - 3 mm2 / s , classi cati come lesioni benigne non mixoidi . 
 nellunico caso di localizzazione nei tessuti molli di malattia di castleman da noi riscontrato abbiamo ottenuto un valore di adc pari a 0 , 780 , 9010 - 3 mm2 / s , simile ai linfomi e per tale motivo incluso nelle lesioni ad alto grado di attivit biologica . 
abbiamo rilevato una ristretta differenza nei valori di adc ottenuti nello schwannoma ( 1 , 740 , 8110 - 3 mm2 / s ) e nel liposarcoma mixoide ( 1 , 560 , 1710 - 3 mm2 / s ) , tuttavia suf ciente , secondo i nostri risultati , a distinguere tra lesioni benigne e maligne . 
according to some authors , lesions with a low grade of biological aggressiveness where the water lanalisi statistica , eseguita con il test di mann - whitney per ogni parametro considerato singolarmente ( b50 , b400 , b800 e adc ) , ha dimostrato una differenza statisticamente signi cativa ( p < 0 , 05 ) tra il gruppo delle 7 lesioni benigne e delle 16 maligne . 
lanalisi statistica mediante curve roc dei dati raccolti ha permesso di stabilire la sensibilit e la speci cit di ciascuno dei parametri considerati ( b50 , b400 , b800 e adc ) nel discriminare tra lesioni benigne e maligne . 
 larea sottesa alla curva al valore di cut - off ( al di sotto del quale si trovano le lesioni a basso grado di attivit biologica e al di sopra del quale quelle ad alto grado di attivit biologica ) rappresenta un parametro fondamentale , in quanto costituisce una misura di accuratezza non dipendente dalla prevalenza . 
qualsiasi variazione del contenuto di protoni di acqua in questi due compartimenti comporta una restrizione della diffusivit , che si traduce in una diversa intensit di segnale nella immagine dwi a diversi b value . 
secondo alcuni autori , allaumentare del b value le lesioni dotate di bassa aggressivit biologica , dove le molecole di h2o sono pi libere di muoversi ( alto coef ciente di diffusione ) perdono intensit di segnale . 
al contrario le lesioni dotate di alta aggressivit biologica , dove le molecole hanno minore libert di movimento ed il coef ciente di diffusione risulta pi basso , persistono iperintense al b value pi alto [ 3 ]  . 
le applicazioni emergenti del dwi in campo oncologico consistono nella caratterizzazione tumorale [ 13 ] ed hanno ottenuto i migliori risultati a livello cerebrale [ 1 , 2 ] ed epatico [ 46 ]  . 
tuttavia in letteratura la maggior parte dei lavori sono incentrati sullef cacia del dwi nel follow - up post - terapia [ 5 , 1430 ] , in particolare nella preradiol med ( 2011 ) 116 : 644656 where molecules have less freedom of movement and the diffusion coef cient is lower , continue to show high signal intensity at higher b values [ 3 ]  . 
the emerging applications of dwi in oncology involve tumour characterization [ 13 ] and have achieved the best results in the brain [ 1 , 2 ] and liver [ 46 ]  . 
however , most published studies have focused on dwi ef cacy for follow - up after treatment [ 5 , 1430 ] , particularly to predict the response to chemotherapy for sarcomas [ 14 , 15 ] and the possibility of discriminating between tumour recurrence and necrosis in musculoskeletal tumours , which are particularly prone to recurrence after surgery [ 1730 ]  . 
 adc , as already widely demonstrated in other body regions , is closely related to the degree of tumour cellularity [ 1 , 2 , 22 , 31 ]  . 
despite there are no unequivocally normal adc values in soft tissues [ 16 ] , the dwi technique appears to have the potential to characterize tissues and de ne their biological activity . 
 [ 8 ] , in a study conducted on 23 patients with histologically proven softtissue tumours , reported signi cantly higher mean adc values in benign ( 1.7110 - 3 mm2 / s ) compared with malignant ( 1.0810 - 3 mm2 / s ) tumours . 
 [ 7 ] , in a small study conducted on 29 patients ( 16 benign lesions and 13 sarcomas ) with two different b values of 0 and 600 s / mm2 , concluded that there is no signi cant difference between the two groups owing to the overlap of adc values in benign lesions ( mean value 1.810 - 3 mm2 / s ) and sarcomas ( mean value 1.710 - 3 mm2 / s )  . 
 [ 17 ] used a sequence called line - scan diffusion - weighted imaging with b values of 5 and 1 , 000 s / mm2 in 44 patients affected by 18 benign and 26 malignant tumours . 
the adc value of myxoid and nonmyxoid tumours ( both benign and malignant ) differs signi cantly , as the structural properties of the extracellular matrix contribute to restricting diffusion . 
the adc of soft - tissue tumours containing myxoid matrix was 1.920.4110 - 3 mm2 / s , whereas that of nonmyxoid tumours was 0.970.3310 - 3 mm2 / s . 
the adc value of benign and malignant soft - tissue tumours was 1.450.5910 - 3 mm2 / s and 1.500.6410 - 3 mm2 / s , respectively , and the difference was not statistically signi cant [ 17 ]  . 
in a larger study of 88 histologically proven lesions studied with se - epi - dwi sequences with b values of 0 and 1 , 000 s / mm2 , nagata et al . 
this is because the adc value is affected by tissue cellularity as well as by the extracellular matrix which , in myxoid tumours , contains large amounts of dizione della risposta dei sarcomi alla chemioterapia , come dimostrano alcuni risultati preliminari [ 14 , 15 ] , e nella possibilit di discriminare tra recidiva e necrosi tumorale nello studio dei tumori del sistema muscoloscheletrico , data la frequenza delle recidive post - chirurgiche [ 1730 ]  . 
nonostante nello studio dwi dei tessuti molli non esistono univoci valori di normalit adc [ 16 ] , questa tecnica sembra avere la potenzialit di tipizzare i tessuti e di de nire la loro attivit biologica . 
 [ 8 ] , in uno studio eseguito su 23 pazienti affetti da tumori dei tessuti molli istologicamente provati , riportano un valore medio di adc signi cativamente maggiore nelle lesioni tumorali benigne ( 1 , 7110 - 3 mm2 / s ) rispetto alle lesioni maligne ( 1 , 0810 - 3 mm2 / s )  . 
 [ 7 ] su una casistica limitata di 29 pazienti ( 16 lesioni benigne e 13 sarcomi ) , usando due diversi b value rispettivamente di 0 e 600 s / mm2 , giungono alla conclusione che non c una differenza signi cativa tra i due gruppi a causa della sovrapposizione dei valori adc nelle lesioni benigne ( valore medio di 1 , 810 - 3 mm2 / s ) e nei sarcomi ( valore medio di 1 , 710 - 3 mm2 / s )  . 
 [ 17 ] hanno utilizzato una sequenza detta line - scan - diffusion - weighted imagingcon due differenti b value di 5 e 1000 s / mm2 in 44 pazienti affetti da 18 tumori benigni e 26 maligni . 
il valore adc tra tumori mixoidi e non mixoidi ( sia benigni che maligni ) differisce in maniera statisticamente signi cativa in quanto le propriet strutturali della matrice extra - cellulare contribuiscono a determinare la restrizione alla diffusione . 
 ladc nei tumori dei tessuti molli contenente matrice mixoide risultava di 1 , 920 , 4110 - 3 mm2 / s , al contrario nei tumori non mixoidi era di 0 , 970 , 3310 - 3 mm2 / s . 
tuttavia , secondo questi autori , il valore adc di tumori benigni e maligni dei tessuti molli rispettivamente di 1 , 450 , 5910 - 3 mm2 / s e di 1 , 500 , 6410 - 3 mm2 / s , con una differenza statisticamente non signi cativa [ 17 ]  . 
 [ 18 ] , su una casistica pi ampia di 88 lesioni istologicamente provate , utilizzando sequenze se - epi - dwi con due b value differenti di 0 e 1000 s / mm2 , affermano che il valore adc discrimina tra lesioni maligne e benigne a matrice non mixoide , mentre non in grado di discriminare tra tumori benigni e maligni a matrice mixoide , poich il valore adc non in uenzato solo dalla cellularit del tessuto , ma anche dalla matrice extra - cellulare , che contiene una grande quantit di acqua nei tumori mixoidi , tale da non consentire la discriminazione tra tumori benigni e maligni . 
ladc riportato nei tumori mixoidi risulta signi cativamente pi elevato rispetto ai non mixoidi , con valori medi rispettivamente di 2 , 080 , 5110 - 3 654 radiol med ( 2011 ) 116 : 644656 water . 
the adc value for myxoid tumours was signi cantly higher than for nonmyxoid tumours , with mean values of 2.080.5110 - 3 mm2 / s and 1.130.4010 - 3 mm2 / s , respectively , in line with the previous study by maeda et al . 
those authors reported no statistically signi cant difference between the mean adc value of benign and malignant myxoid tumours ( 2.100.5010 - 3 mm2 / s and 2.050.5810 - 3 mm2 / s , respectively )  . 
conversely , the adc value of benign nonmyxoid tumours was 1.310.4610 - 3 mm2 / s , which was signi cantly higher ( p < 0.001 ) than that of malignant nonmyxoid tumours ( 0.940.2510 - 3 mm2 / s )  . 
 in our limited experience , the use of three b values ( 50 - 400 - 800 s / mm2 ) enabled us to discriminate the group of seven benign lesions from that of 16 malignant lesions on each parameter considered individually ( b50 , b400 , b800 , adc )  . 
 in our experience , the qualitative analysis of dwi demonstrated an absence of high signal intensity at all b values in benign lesions and persistence of high signal intensity with increasing b value ( 800 s / mm2 ) in all malignant tumours . 
most investigators tend to concentrate exclusively on the adc value for differentiating between benign and malignant tumours [ 7 , 8 , 17 , 18 ] , even though large studies including a variety of tumour types have reported that myxoid lesions show a certain degree of overlap in adc , which nonetheless contributes greatly to the differentiation of malignant and benign nonmyxoid lesions [ 17 , 18 ]  . 
in our opinion , partly in consideration of this overlap , it is useful to combine qualitative and quantitative analyses of dwi , clearly without omitting evaluation of the t1 and t2 morphological sequences . 
the reason for this lies in the high content of mucin and low content of collagenous bres in these lesions , which translates into increased water in the extracellular matrix and high diffusivity . the best correlation between the qualitative / quantitative analysis of dwi and histology was seen in lymphomas and muscular metastases from hepatocellular carcinoma and ductal breast carcinoma , which were characterised as frankly malignant on the basis of the low adc value mm2 / s e 1 , 130 , 4010 - 3 mm2 / s , in linea con il precedente studio di maeda et al . 
non riportata una differenza signi cativa tra il valore medio di adc nei tumori benigni e maligni mixoidi ( rispettivamente 2 , 100 , 5010 - 3 mm2 / s e 2 , 050 , 5810 - 3 mm2 / s )  . 
anche nella nostra casistica il valore di adc pi alto riscontrato nei tumori maligni non mixoidi di 1 , 3410 - 3 mm2 / s , in un sarcoma ad alto grado . 
 nella nostra esperienza , seppur ridotta , utilizzando tre diversi b value ( 50 - 400 - 800 s / mm2 ) , stato possibile discriminare il gruppo delle 7 lesioni benigne dalle 16 maligne su ogni parametro considerato singolarmente ( b50 , b400 , b800 , adc )  . 
 nella nostra esperienza , lanalisi qualitativa della dwi dimostra assenza di ipersegnale in tutti i b value nelle lesioni benigne e persistenza delliperintensit di segnale al crescere del b value ( 800 s / mm2 ) in tutti i tumori maligni . 
 la maggior parte degli autori tendono a concentrare la loro attenzione esclusivamente sul valore di adc nella differenziazione tra tumori benigni e maligni [ 7 , 8 , 17 , 18 ] , ma su casistiche ampie e con diversi tipi di tumori si osservato che le lesioni mixoidi risentono di una certa sovrapposizione tra i valori di adc , che comunque offre un signi cativo contributo nella diagnostica differenziale tra lesioni maligne e benigne a matrice non mixoide [ 17 , 18 ]  . 
a nostro giudizio , anche in relazione a questa sovrapposizione dei valori di adc , utile integrare le analisi qualitativa e quantitativa della dwi , senza prescindere dalle sequenze morfologiche t1 e t2 . 
hence , there is a need for noninvasive methods , such as mr with dwi , which may provide a diagnosis as close as possible to the histological diagnosis , through an evaluation that goes beyond the surgical specimen to include staging . 
 these results form the basis for a promising future in which dwi is able to provide information on the effectiveness of treatment at an earlier stage than with conventional morphological imaging , given that molecular changes precede the macroscopic volumetric changes . 
da qui la necessit di utilizzare metodiche non invasive , quali la rm con dwi , che possano condurre ad una diagnosi il pi vicino possibile a quella istologica , con unanalisi non limitata al solo pezzo anatomico prelevato , ma completa di staging . 
 questi risultati , pongono le basi per un promettente futuro in cui la dwi in grado , pi precocemente dellimaging morfologico convenzionale , di dare informazioni sullef cacia del trattamento , in quanto i cambiamenti molecolari , precedono quelli macroscopici volumetrici . 
 conclusioni conclusions dwi , supplemented with conventional morphological imaging , may offer valuable assistance in the study of softtissue tumours , providing essential information on lesion biological aggressiveness and stage in a single examination . 
in our admittedly limited experience , the use of three different b values enabled correct differentiation between benign and malignant lesions , both myxoid and nonmyxoid , with total agreement with the histological ndings . 
larger and more extensive studies are required to validate this imaging technique and the bene ts deriving from the use of different b values . limaging dwi , corredato al convenzionale studio morfologico , pu fornire un valido aiuto nello studio delle lesioni dei tessuti molli , fornendo in un unico esame preziose informazioni circa laggressivit biologica e la stadiazione della lesione . 
lutilizzo di tre differenti b value ha consentito nella nostra esperienza , bench limitata , una corretta differenziazione tra lesioni benigne e maligne , sia mixoidi che non mixoidi , con una completa concordanza con il risultato istologico . 
 questa sua decisione lo aveva portato da noi per analizzare il funzionamento di un reparto di radiodiagnostica centralizzato di recente istituzione . a ne incontro ci recammo in una tipica trattoria romana . 
nonostante il tempo trascorso , ricordo molto bene quella sosta alla trattoria antico falcone che mentalmente riporto allinizio di un lavoro in corso dopera che , nel tempo , ha prodotto coinvolgenti iniziative formative di gruppo , in ambito toracico , dif cili da dimenticare . parlammo della sua non semplice scelta , di radiologia , e , ovviamente , di radiologia toracica , delle possibili innovazioni della stessa , anche per le prime ricadute dei voli spaziali ( assenza di gravit ) sul circolo polmonare , di radiologia clinica del torace . 
considerazioni che contrastavano con una terminologia radiologica corrente , lontana dalla realt siopatologica , come accentuazione della trama bronco vascolare del polmone , sostituita successivamente da riscontri radiologici strettamente correlati alle nuove cognizioni di siopatologia cardio - polmonare . quel nostro incontro , irrobustito nel tempo dal coinvolgimento attivo di altri quali cati colleghi , port alle giornate pneumo - radiologiche bresciane ( 1975 ) , alla costituzione della sezione di studio di radiologia toracica della sirm ( 1976 ) , allistituzione del premio pigorini ( 1978 ) con il contributo economico della famiglia pigorini , allattivazione dei corsi itineranti regionali di radiologia toracica ( 1979 )  . interventi che , pur nella loro diversit , hanno inciso tutti , nel tempo , sulla formazione professionale del radiologo italiano , annullando o forse anche invertendo , di fatto , un non trascurabile gap culturale di allora . le giornate pneumo - radiologiche bresciane , giunte quasi alla loro ventesima edizione sono , ormai , parte essenziale della radiologia toracica italiana , come possono ben testimoniare radiologi , pneumologi e anatomopatologi bresciani coinvolti in questa iniziativa . in questi lunghi anni di attivit professionale e formativa presso gli spedali civili di brescia , renato bergonzini diventato , di fatto , bresciano di adozione , pur rimanendo profondamente e nostalgicamente emiliano e modenese il ricordo di renato bergonzini mi riporta a uno dei nostri primi incontri , allinizio degli ormai lontani anni settanta , nellistituto di radiologia della facolt di medicina e chirurgia delluniversit cattolica di roma , diretto dal prof . 
 ricordo , per i pi giovani , due dati : il progresso delle conoscenze e delle tecnologie in medicina e in radiologia era , in quegli anni , graduale e lento , a differenza della crescita esponenziale di oggi , e la specializzazione era solo in radiologia . lo specializzando nel suo tirocinio formativo frequentava le tre diverse strutture dellistituto , reparto degenti della radioterapia incluso ; da medico specializzato , poi , aveva possibilit di operare professionalmente , secondo necessit , nei tre diversi ambiti della radiologia . 
 esigenze professionali diverse hanno portato , nel tempo , ad una progressiva diversi cazione delle tre diverse branche della radiologia e alla successiva istituzione di tre diverse scuole di specializzazione , radiodiagnostica ( poi diagnostica per immagini ) , radioterapia e medicina nucleare . renato bergonzini , laureato in medicina e chirurgia e specializzato in radiologia e in oncologia a modena , sua 668 radiol med ( 2011 ) 116 : 667668 nellanimo e nel carattere , sempre pronto a commentare le vicende della rossa ferrari , con tipiche espressioni dialettali modenesi che rispolverava spesso incontrando colleghi della sua citt natale . la sezione di radiologia toracica , concepita nel lontano 1973 , come riporta lo stesso bergonzini su torax del 1997 , ai piedi della montagna incantata di davos da un gruppo di cultori della materia ( barone , bergonzini , corda , marano ) , fu istituita uf cialmente a brescia il 16 ottobre del 1976 , con renato bergonzini primo presidente . 
 il premio luigi pigorini tuttora , per i cultori della materia , il pi importante riconoscimento uf ciale della radiologia toracica italiana ; ha cadenza biennale ed assegnato durante il convegno nazionale della sezione , contemporaneamente alla presentazione della conferenza pigorini , presentata dal vincitore del biennio precedente . con i corsi itineranti , la sezione di radiologia toracica della sirm introdusse uninnovazione metodologica nella formazione professionale del radiologo italiano , coinvolgendolo attivamente nella propria formazione . cesare fava nella sua interessante lettura alle giornate pneumo - radiologiche bresciane del 2005 ricordava che , con lavvio dei corsi itineranti , la sezione di radiologia toracica della sirm completava una manovra a tenaglia nei confronti dei radiologi italiani . 
208 , euro 18 , 00 published online : 22 march 2011 springer - verlag 2011 pasquale marano has occupied , and still occupies , such a prominent place in italian radiological culture that we cannot fail to draw attention to his most recent ( latest , but not least ) book , ritorno al paziente ( back to the patient ) , which was presented at our last national congress . ritorno al paziente is both a wish and a commitment , an anthology that allows us to participate in maranos tribulations as a physician , teacher and faculty dean , in his complex and almost dramatic oscillations between holistic medicine and web 2.0 , past and future , pessimism and hope . 
although there is rare mention of actual facts and exact dates , marano describes the most intimate details and deepest recollections in a story of sentiments and experience that is gripping in its concreteness and almost touching in its empathy . its the diary of a lifetime , as well as a valuable opportunity to gain insight into the evolution of medicine and medical teaching , but with also a keen and interested eye to the possible future . what does the book contain ? a beautiful introduction which is also a synopsis . 
some useful notions of epidemiology ( the current predominance of chronic degenerative diseases ) , the evolution of society and the new doctor - patient relationship , the increasing trust in medicine and simultaneous distrust in doctors , the fragmentation of knowledge and competencies , the dif culties in teaching , the crisis of the ethical - moral values and certainties that once founded western societies... the other chapters offer some beautiful pages on error in medicine and defensive medicine , experimental and clinical research , research and innovation , and the market approach to healthcare , on which subject the author makes an ominous prediction : i fear that by operating in this way the italian healthcare system based on social cohesion and solidarity will follow in the steps taken many years ago by the american healthcare system , with the result of being sold off to insurance companies and private enterprises , among the indifference of the public . pasquale marano ha occupato e occupa un posto di grande importanza nella cultura radiologica italiana , perch possa passare sotto silenzio questa ultima ( latest , but not least ) sua fatica ritorno al paziente che stata messa a nostra disposizione durante il nostro recente congresso nazionale . ritorno al paziente un augurio e un impegno dellautore , uno zibaldone che ci permette di assistere al suo travaglio di medico , di docente e di preside , alle sue oscillazioni complesse e quasi drammatiche fra la medicina olistica ed il web 2.0 , fra il passato e lavvenire , fra il pessimismo e la speranza . 
sono rari i riferimenti a fatti concreti e a date precise , ma marano ssa i particolari pi intimi e le ricordanze pi profonde in una storia di sentimenti e di esperienze appassionante nella sua concretezza e quasi commovente nella sua partecipazione . il diario di una vita , ma anche un prezioso aiuto per capire qualcosa di pi dellevoluzione della medicina , e soprattutto dellinsegnamento della medicina ieri e oggi , con uno sguardo interessato e partecipe anche al possibile futuro . cosa c nel libro ? una bellissima introduzione che ne anche la sintesi . 
qualche utile cenno di epidemiologia ( il predominio attuale delle malattie cronico - degenerative ) , levoluzione della societ e il nuovo rapporto medico - paziente , laccresciuta ducia nella medicina e la contemporanea s ducia nel medico , la frammentazione delle conoscenze e delle competenze , le dif colt dellinsegnamento , la crisi dei valori etico - morali e delle certezze su cui poggiavano le societ occidentali poi , negli altri capitoli che non elenco , alcune bellissime pagine sullerrore in medicina e sulla medicina difensiva , sulla ricerca sperimentale , clinica e sulla cosiddetta ricerca e innovazione , sulla sanit - mercato al cui proposito c una preoccupante previsione : io temo che cos operando si stia portando , nellindifferenza generale , la sanit sociale e solidaristica italiana sulla stessa strada percorsa molti anni fa dalla sanit americana nendo con svenderla ad assicurazioni e imprese private . the second part of the book is devoted to teaching , both la seconda parte del libro dedicata allinsegnamento , 670 radiol med ( 2011 ) 116 : 669670 at university and in other settings . 
marano was perhaps the rst to involve general practitioners and hospital doctors in university teaching ; while in no way repudiating these choices , today he doesnt conceal his bitterness and disappointment for a message that was never understood and only in part implemented . 
he realises that still today the doctors rst duty remains the illness , so that talking to patients , looking after people rather than their illnesses becomes an additional personal characteristic and , as such , one that is not codi ed or compulsory . 
 a book that interested and stimulated me , a book that i found useful and that i think could be useful to many radiologists , above all those who are or have been involved in teaching . 
marano stato forse il primo a coinvolgere medici di base e medici ospedalieri nellinsegnamento universitario ; oggi non rinnega affatto queste scelte anche se non nasconde amarezza e delusione per un messaggio non compreso e solo in parte attuato . 
si rende infatti conto che ancora oggi il compito prioritario del medico resta la malattia per cui il parlare con i pazienti , loccuparsi delle persone e non delle loro malattie diviene un qualcosa di aggiuntivo e personale e , pertanto , non codi cato e non obbligatorio . 
mazziotti , via consolare pompea 1871 , 98165 messina , italy , tel . : + 39 - 090 - 3973213 , fax : + 39 - 090 - 2937427 , e - mail : smazziotti@unime.it accepted : 26 november 2009 / accepted : 15 december 2009 / published online : 19 march 2011 springer - verlag 2011 abstract purpose . 
the entire course of the tympanic canaliculus was identi ed in 80 / 97 petrous pyramids ( 82.4% ) , 57 of which were normal ( 75.4% detection rate ) and 40 pathological ( 90% detection rate )  . 
il canalicolo timpanico stato identi cato in tutto il suo decorso in 80 / 97 rocche petrose ( 82 , 4% ) , 57 normali ( tasso di individuazione del 75 , 4% ) e 40 patologiche ( tasso di individuazione del 90% )  . 
la tc multidetettore rappresenta lunica possibilit di valutare in vivo , in maniera multiplanare e con elevata frequenza ( 82 , 4% ) il canalico timpanico . parole chiave canalicolo timpanico orecchio medio tc multidetettore 658 introduction jacobsons nerve ( jn ) represents the rst efferent branch of the glossopharyngeal nerve above the plane of the jugular foramen [ 1 , 2 ]  . 
in fact , the jn originates from the inferior ganglion of the glossopharyngeal nerve , which lies at the level of the petrosal fossula , located at the level of the anterior border of the petrosal foramen . 
the location of the tc inlet is , however , somewhat variable , as it may lie either at the level of border of the caroticojugular spine or anteriorly or posteriorly to it ; it frequently has a central location , although it may also be found laterally or medially . 
at the level of the tympanic cavity , the tc opens onto the lowermost portion of the hypotympanum , at the base of the promontory , in a position anteroinferior fig . 
1 , forame giugulare ; 2 , setto carotido - giugulare ; 3 , canale carotideo ; freccia lunga , forame dingresso del canalicolo timpanico ; freccia corta , fossula petrosa . 
 radiol med ( 2011 ) 116 : 657666 introduzione il nervo di jacobson ( nj ) rappresenta il primo dei rami ceduti dal nervo glossofaringeo ( ngf ) al di sopra del piano che identi ca il forame giugulare ( fg ) [ 1 , 2 ]  . 
la sede dellorizio di ingresso del ct , tuttavia , alquanto variabile , potendo collocarsi sia a livello del margine della spina carotido - giugulare , che anteriormente o posteriormente ad esso ; pi sovente in sede centrale , ma talvolta anche alquanto laterale o mediale . 
da quanto sopra , appare di tutta evidenza come il decorso complessivo del nj sia suddividibile in un segmento intratimpanico costituito dal plesso omonimo e da un segmento infra - timpanico contenuto interamente nel ct . 
va , in ne , ricordato come il ct dia alloggio oltre che al nj anche alla sottilissima arteria timpanica ( at )  . il presente lavoro , eminentemente di tipo morfologico , nalizzato a valutare le possibilit della tomogra a computerizzata ( tc ) multistrato nella visualizzazione multiplanare del ct , segnatamente alle sue varianti anatomiche ed alle sue caratteristiche morfologiche , sia in condizioni normali che in corso di patologia in ammatoria cronica dellorecchio medio . 
in letteratura esistono solo sporadiche citazioni nelle quali riportata limmagine coronale del ct , senza peraltro alcuna indicazione di ordine tecnico e nelle quali si evidenzia limportanza di distinguere il ct da eventuali rime di frattura [ 35 ]  . 
per il resto , nella letteratura , sia precedente alla introduzione della tc multidetettore , sia in quella pi recente , il ct o non viene citato o ci si riferisce ad esso solo in termini di identi cazione esclusivamente sul piano assiale , nelle immagini acquisite ad alta risoluzione [ 611 ]  . radiol med ( 2011 ) 116 : 657666 to the round window . 
it is clear from this description that the overall course of the jn may be subdivided into an intratympanic segment , represented by the tympanic plexus , and an infratympanic segment , completely enclosed in the tc . 
 this morphological study was aimed at assessing the potential of multidetector computed tomography ( mdct ) for multiplanar imaging of the tc , in particular , as regards its anatomical variations and its morphological features , both in the normal ear and in chronic in ammatory middleear disease . 
to our knowledge , only few published citations exist on coronal imaging of the tc ; they do not , however , provide any technical indications or highlight the importance of differentiating the tc from fracture lines [ 35 ]  . 
 besides these citations , in papers published before or after the introduction of mdct , the tc is either not mentioned at all or only referred to in terms of detection in the axial plane in high - resolution images [ 611 ]  . materials and methods this study consisted of two phases : a preparatory phase and a phase focusing on clinical application . phase 1 to determine beforehand the most effective technique for multiplanar imaging of the tc in living individuals , we conducted a study on three dried skulls in which a very thin copper wire was placed as a landmark in the tc lumen to facilitate its detection . 
 all examinations were performed with a 16 - channel system ( sensation 16 , siemens , erlangen , germany ) with the following technical parameters : collimation 0.75 mm , pitch 0.55 mm , fov 300 mm , reconstruction increment 0.5 mm , high - resolution bone lter . 
on the paracoronal image , a further oblique parasagittal reconmateriali e metodi la metodologia di impostazione del lavoro ha previsto due fasi : un primo approccio di ordine preparatorio , propedeutico alla seconda fase focalizzata allapplicazione clinica . prima fase al ne di determinare preventivamente la tecnica pi ef cace per dimostrare in maniera multiplanare il ct nel vivente , stato realizzato uno studio basato sullimpiego di 3 crani secchi nei quali , al ne di facilitarne la individuazione , il ct stato evidenziato ponendo nel suo lume un repere metallico rappresentato da un sottilissimo lo di rame . tutti gli esami sono stati eseguiti con apparecchiatura con 16 canali di lettura ( sensation 16 , siemens , erlangen , germania ) con i seguenti parametri tecnici : collimazione : 0 , 75 mm , pitch : 0 , 55 mm , campo di vista ( fov ) : 300 mm , indice di ricostruzione : 0 , 5 mm , ltro ad alta risoluzione per losso . 
lacquisizione sul piano assiale stata eseguita senza alcuna angolazione del gantry ( inclinazione del gantry = 0 )  . le procedure di elaborazione post - processing sono state le seguenti : ricostruzione para - assiale obliqua secondo un piano con inclinazione di circa 1520 , orientato secondo la linea basale o canto - meatale . 
quindici pazienti erano affetti da otite cronica non colesteatomatosa , 18 da otite colesteatomatosa di cui 4 portatori degli esiti di pregresso intervento di antro - atticotomia con timpanoplastica ( tre con ogosi della cavit chirurgica ed uno con 660 radiol med ( 2011 ) 116 : 657666 ripresa di malattia colesteatomatosa )  . 
delle 100 rocche petrose studiate , pertanto , ne sono valutate ai ni del presente studio solo 97 ( 57 normali e 40 patologiche ) in quanto le tre , nelle quali si confermata la presenza del tumore glomico timpano - giugulare , sono state escluse , stante le gravi alterazioni ossee presenti nellarea del ct . 
 analisi statistica tutte le analisi statistiche sono state effettuate utilizzando il pacchetto software statistical package for the social sciences ( spss ) 10.0 ( spss , inc . , chicago , il )  . 
 we prospectively recruited 50 patients ( 28 men , 22 women ; age range 2074 years ) who were candidates for ct studies of the temporal bone due to suspected or proven chronic middle ear disease . 
fifteen patients were affected by chronic noncholesteatomatous otitis and 18 by cholesteatomatous otitis , four of whom had previously undergone antroatticotomy followed by tympanoplasty reconstruction ( three with in ammation of the surgical cavity and one with recurrent cholesteatomatous disease )  . 
therefore , of the 100 petrous pyramids examined , only 97 ( 57 normal and 40 pathological ) were included in this study , as the three cases with a con rmation of jugulotympanic glomus tumour were excluded owing to severe bone changes in the tc region . statistical analysis all statistical analyses were performed using the spss 10.0 sono state globalmente valutate 97 rocche petrose . 
per determinare se la differenza nel tasso di individuazione nei due sottogruppi sia statisticamente signi cativa , i dati sono stati analizzati mediante un test non parametrico ( test 2 di pearson )  . 
in tutti i casi lestremit timpanica del ct si collocava alla base del promontorio che , pertanto , ha rappresentato un signi cativo repere anatomico di riferimento . radiol med ( 2011 ) 116 : 657666 fig . 
the p line indicates the oblique paracoronal reconstruction plane centred on the tympanic canal inlet and oriented towards the caroticojugular septub paracoronal reconstruction showing the tympanic canal ( short arrow )  . 
d ricostruzione parasagittale che dimostra il canalicolo timpanico ( freccia corta ) con decorso lievemente obliquo rispetto al piano coronale ( c )  . software package ( spss , inc . , chicago , il , usa )  . 
 pearsons chi - square test was used to determine differences between groups ; cohens kappa test was used to measure interobserver agreement . results a total of 97 petrous pyramids were evaluated . 
in the rst group , the tc detection rate was 42 / 57 ( 73.7% ) , whereas in the second group , pathological pyramids , the detection rate was 36 / 40 ( 90% )  . 
p paracoronal oblique reconstruction plane oriented on the caroticojugular septu b depiction of the tympanic canal ( arrows ) in a paracoronal oblique reconstruction , with approximately 45 obliquity in the horizontal plane , lateromedial and caudocranial inclination . 
 on the basis of the criteria , 61.1% of tc depicted within state dimostrate signi cative differenze di incidenza di ct alterato nei pazienti portatori di otite cronica colesteatomatosa o non colesteatomatosa ( p > 0 , 1 )  . 
 discussione dalla analisi dei risultati ottenuti possibile affermare che la tc multidetettore rappresenta lunica possibilit di valutare in vivo , in maniera multiplanare e con elevata frequenza ( 80 , 4% ) , il ct . fino ad oggi la descrizione del ct era af data alla letteratura anatomica , che basava le proprie valutazioni sullimpiego di tecniche di dissezione . 
la suddetta considerazione spiega , verosimilmente , le differenze di lunghezza del ct riscontrate nel nostro lavoro , che appaiono minori ( media di 7 , 3 mm ) rispetto a quelle riferite dagli studi anatomici ( media 9 , 5 mm )  . 
tali discrepanze , peraltro trascurabili , sono da ricondursi in prima ipotesi , oltre che alla differente metodologia di misura , anche ai diversi reperi anatomici posti alla base delle due modalit di approccio . 
nelle dissezioni anatomiche , infatti , nella misura del ct viene anche inclusa la regione della fossula petrosa . il nostro studio trova , per converso , perfetta coincidenza con le analisi anatomiche nella documentazione dei due gradi di obliquit del ct ( in senso latero - mediale ed antero - posteriore ) con una precisa quanti cazione degli angoli stessi . 
bisogna sottolineare , peraltro , che , nella nostra casistica , in un non trascurabile numero di casi , il ct non presentava alcuna inclinazione antero - posteriore , decorrendo pressoch parallelo ( a 0 ) al piano frontale . 
in fact , the measurement of tc length at anatomical dissection is inclusive of the petrosal fossula . by contrast , our results coincide perfectly with anatomical studies with regard to the nding of the two degrees of tc inclination ( lateromedial and anteroposterior ) , with precise quanti cation of the angles . 
this variation in course has not been described in any anatomical study . another consideration emerging from our study is the dif culty detecting the tc in the presence of extreme pneufig . 
tale problematica trova riscontro anche nella letteratura non radiologica , poich la suddetta condizione rappresenta un ostacolo anche in corso di dissezione anatomica , oltre che durante le manovre chirurgiche nalizzate alla resezione del nj cos che , sovente , in presenza di iperpneumatizzazione infra - timpanica la procedura debba essere abbandonata . 
si rileva nella ricostruzione paracoronale obliqua una modesta quantit di tessuto patologico a livello dellori zio prossimale del canalicolo timpanico ( freccia corta ) , questultimo appare signi cativamente slargato ( freccia lunga )  . 
this problem has also been highlighted in nonradiological studies , as the condition hampers anatomical dissection as well as surgical manoeuvres aimed at jn resection , leading to interruption of the procedure in the presence of infratympanic hyperpneumatisation . our ndings regarding pathological tc are also interesting . 
this is probably due to the very low position of the tc , which facilitates and prolongs the contact of the products of in ammation and in amed tissues with the tympanic opening of the canaliculus . 
the former are caused by a proliferation of cells of the nonchromaf n paraganglial system , which are present in a quantitatively signi cant amount ( almost one fth of the total ) along the intracanalicular course of the jn . 
conversely , tc alterations and jn involvement in the presence of in ammatory changes are in merito alla analisi del ct in condizioni patologiche . il coinvolgimento del ct risulta assai frequente ( 61 , 1% ) in presenza di patologia ogistica , senza alcuna differenza signi cativa tra otite cronica colesteatomatosa e non colesteatomatosa . 
ci verosimilmente in ragione della sua sede estremamente declive che facilita e prolunga il contatto dei prodotti della in ammazione e del tessuto ogistico con lo sbocco timpanico del canalicolo . 
le prime sono secondarie alla proliferazione delle cellule dellapparato non cromaf ne paragangliare , che si localizzano in maniera quantitativamente non trascurabile ( circa un quinto del totale ) lungo il decorso intra - canalicolare del nj . 
 il nj rappresenta uno dei rami terminali del ngf ed pertanto deputato a diverse funzioni nellambito delle atti666 radiol med ( 2011 ) 116 : 657666 less well known and completely lacking from the radiological literature . the jn represents one of the terminal branches of the glossopharyngeal nerve and has therefore several parasympathetic neurovegetative functions [ 2 , 9 ]  . 
in addition , there seems to be a ( not completely clear ) correlation between jn dysfunction and tinnitus , another disorder that was often successfully treated with jn resection . 
anatomical studies , supported by electromyographic ndings , have shown that bres from the jn and the tympanic plexus participate in this function by way of synapses at the level of the pons , from which other efferent bres regulate the tone and function of the elevator and constrictor muscles of the auditory tube . given that our study focused mainly on morphological aspects of the tc , no correlation emerged between the alterations identi ed and the above functional aspects . 
analysis of our results did not take into consideration possible correlations with those clinical aspects ( tinnitus , salivary function alterations , disease duration , etc . ) that could have con rmed or denied the role of jn alterations in the origin and natural history of in ammatory diseases of the middle ear . 
in this perspective , our study was preliminary and preparatory to another study aimed at analysing jn alterations and their correlation with such clinical aspects . vit neuro - vegetative ad impronta parasimpatica [ 2 , 9 ]  . 
studi anatomici , confortati dal riscontro elettromiogra co , hanno dimostrato , infatti , come contingenti di bre del nj e dal plesso timpanico intervengano in tale funzione mediante collegamenti sinaptici a livello del ponte , dal quale altre bre efferenti sono in grado di regolare il tono e la funzionalit dei muscoli elevatore e costrittore della tuba . poich il presente lavoro ha inteso focalizzare principalmente gli aspetti morfologici relativi al ct , da esso non sono emerse correlazioni tra le alterazioni documentate ed i suddetti aspetti funzionali . 
nellanalisi dei risultati , infatti , non sono state prese in considerazione le possibili correlazioni con quegli aspetti clinici ( presenza di tinnito , alterazioni della funzione salivare , durata della malattia , ecc . ) , che avrebbero potuto confermare o smentire il ruolo della alterazione del nj nella con gurazione e nella storia naturale della patologia ogistica dellorecchio medio . 
the learning objectives of this review are to : illustrate radiographic anatomy of the mediastinum with particular attention to mediastinal lines ; describe radiographic signs that allow identi cation of mediastinal abnormalities that are dif cult to detect on conventional chest radiographs ; describe ndings that help localise abnormalities in the anterior , middle or posterior mediastinuthe anterior junction line obliteration , the hilum overlay sign , the preservation of the posterior mediastinal lines and the silhouette sign with the right cardiac border are radiographic signs that allow identi cation and localisation of anterior mediastinal lesions . 
widening of the right paratracheal stripe , distortion of the azygo - oesophageal recess and the convex border of the aortopulmonary window indicate the presence of a middle mediastinal abnormality . 
 gli obiettivi diagnostici della nostra review sono stati : illustrare lanatomia radiogra ca del mediastino con particolare riferimento alle linee mediastiniche ; descrivere i segni che aiutano ad identi care alterazioni mediastiniche di dif cile diagnosi radiogra ca ; descrivere le alterazioni radiogra che che consentono di localizzare la lesione a livello del mediastino anteriore , medio o posteriore . 
la cancellazione della linea di giunzione anteriore , il segno dellilo sovrapposto , la conservazione delle linee mediastiniche posteriori ed il segno della silhouette con il margine destro del cuore sono segni di semeiotica radiogra ca indicativi di patologie del mediastino anteriore . 
 inoltre questo approccio permette di localizzare il radiol med ( 2011 ) 116 : 532547 keywords mediastinal lines mediastinal masses chest radiograph compartimento mediastinico interessato dalla patologia e quindi di porre indicazione al successivo iter diagnostico pi appropriato . 
 preservation , obliteration , thickening or distortion of these lines represent the key to diagnosing and localising mediastinal abnormalities that are dif cult to detect on chest radiographs . the mediastinum is often divided into convenient compartments . 
even if there are no physical boundaries between mediastinal compartments , a simpli ed classi cation can help to more accurately localise an abnormality and may help narrow the differential diagnosis prior to obtaining additional information with chest computed tomography ( ct )  . 
the felson method of division is based on ndings at lateral chest lthe anterior mediastinum is bounded anteriorly by the sternum and posteriorly by a line extending from the thoracic inlet to the diaphragm along the anterior aspect of the trachea and the back of the heart . 
the posterior mediastinum is localised between the line that connects points 1 cm behind the anterior margins of the vertebral bodies and the posterior thoracic wall [ 1 ]  . heitzman divided the mediastinum into the following anatomic regions : thoracic inlet , anterior mediastinum , supra - aortic area ( above the aortic arch ) , infra - aortic area ( below the aortic arch ) , supra - azygos area ( above the azygos arch ) and infra - azygos area ( below the azygos arch ) [ 2 ]  . anterior mediastinum the anterior mediastinum is bounded anteriorly by the sternum , posteriorly by the anterior wall of the trachea and the back of the heart , superiorly by the thoracic inlet and inferiorly by the diaphrag its contents include thymus , lymph nodes , adipose tissue , heart and ascending aorta . 
la conservazione , lobliterazione , lispessimento o la distorsione di queste linee rappresenta la chiave per la diagnosi e la localizzazione di alterazioni mediastiniche di dif cile identi cazioni radiogra ca . il mediastino convenzionalmente suddiviso in alcuni compartimenti . 
sebbene non esistano precise barriere anatomiche che suddividano tali compartimenti , una classi cazione sempli cata pu aiutare nel localizzare in modo pi preciso uneventuale alterazione e nel restringere il ventaglio delle possibilit diagnostiche prima di ottenere ulteriori informazioni con lesame in tomogra a computerizzata ( tc )  . 
il mediastino anteriore delimitato anteriormente dallo sterno e posteriormente da una linea che si estende dalladitus mediastinico al diaframma decorrendo per la parete anteriore della trachea e per il margine posteriore del cuore . 
 il mediastino posteriore compreso tra una linea passante un centimetro dietro i corpi vertebrali e la parete toracica posteriore [ 1 ]  . la classi cazione di heitzman divide il mediastino nelle seguenti regioni : laditus mediastinico , il mediastino anteriore , la regione sovra - aortica ( al di sopra dellarco aortico ) , la regione infra - aortica ( al di sotto dellarco aortico ) , la regione sovra - azygos ( al di sopra dellarco dellazygos ) e la regione infra - azygos ( al di sotto dellarco dellazygos ) [ 2 ]  . mediastino anteriore il mediastino anteriore delimitato anteriormente dallo sterno , posteriormente dalla parete anteriore della trachea e dal pro lo posteriore del cuore , superiormente dalladitus mediastinico ed inferiormente dal diaframma . 
obliteration of the anterior junction line , the hilum overlay sign , preservation of the posterior mediastinal lines and the silhouette sign with the right cardiac border are radiographic signs that allow identi cation and localisation of anterior mediastinal lesions [ 36 ] : anterior junction line : this is seen at frontal chest radiography . 
a small amount of fat is normally found within the line ; however , increased amounts of intervening mediastinal fat and possibly thymus in younger patients may cause the anterior junction line to appear as a stripe . 
anterior mediastinal masses can obliterate the anterior junction line , although it is usually the preservation of more posterior lines at chest radiography that helps to correctly localise an anterior mediastinal mass . hilum overlay sign : this is present when the normal in tale spazio sono contenuti il timo , i linfonodi , il tessuto adiposo , il cuore e laorta ascendente . 
le masse del mediastino anteriore comprendono lesioni timiche ( timoma , carcinoma , iperplasia timica , cisti timiche e timolipoma ) , linfomi , tumori a cellule germinali e cisti pleuro - pericardiche . 
lobliterazione della linea di giunzione anteriore , il segno dellilo sovrapposto , la conservazione delle linee mediastiniche posteriori ed il segno della silhouette con il margine destro del cuore sono segni radiogra ci che permettono di identi care e correttamente localizzare patologie espansive del mediastino anteriore [ 36 ]  . 
 la linea di giunzione anteriore visibile sulla radiogra a del torace in proiezione frontale ; questa linea formata dallapposizione anteriore della pleura viscerale e parietale della porzione antero - mediale dei due polmoni unitamente ad una modesta quota di tessuto adiposo mediastinico interposto . 
una modesta quantit di grasso normalmente presente allinterno della linea ; tuttavia , laumento della quantit di tessuto adiposo e la presenza del timo nei pazienti giovani possono determinare un aspetto a banda della linea di giunzione antefig . 
1a , b drawing on the frontal chest radiograph ( a ) shows the anterior junction line running obliquely from the upper right to the lower left and not extending above the manubriosternal junction . 
1a , b la linea disegnata sulla proiezione frontale del torace ( a ) rappresenta la linea di giunzione anteriore che decorre obliquamente dallalto verso il basso e da destra verso sinistra e non si estende al di sopra dellarticolazione manubrio - sternale . 
la scansione tc ( b ) passante per la porzione superiore del torace mostra il normale aspetto della linea di giunzione anteriore ( freccia ) formata dallaccollarsi della pleura viscerale e parietale dei due polmoni e dal tessuto adiposo interposto . 
posteroanterior chest radiograph ( a ) clearly depicts the hilum ( arrow ) , which indicates that the mass is either anterior or posterior to the hiluin addition , the descending aorta is clearly seen ( arrowhead ) , indicating that the mass is not within the posterior mediastinuchest computed tomography scan ( b ) con rms the presence of an anterior mediastinal mass . 
la visualizzazione dellilo polmonare ( freccia ) nella radiogra a del torace in proiezione postero - anteriore ( a ) indica che la massa localizzata in un piano anteriore o posteriore rispetto allilo . 
an abnormal convex aspect of the cardiac border or the presence of an additional line along the pro le of the heart can also suggest the presence of an anterior mediastinal mass . middle mediastinum the middle mediastinum is bounded anteriorly by the anterior wall of the trachea and the back of the heart , posteriorly by the vertebral bodies , superiorly by the thoracic inlet and inferiorly by the diaphragits contents include the superior vena cava ( svc ) , the inferior vena cava ( ivc ) , brachiocephalic vessels , pulmonary vessels , trachea and main riore . 
la radiogra a del torace ( a ) mostra unopacit a margini netti verso il parenchima polmonare che si proietta a livello della nestra aorto - polmonare ( frecce )  . 
4a , b la proiezione postero - anteriore della radiogra a del torace ( a ) mostra una massa espansiva del mediastino anteriore che determina cancellazione del margine destro del cuore . 
knowledge of the contents of this compartment facilitates development of a differential diagnosis for middle mediastinal masses that includes lymphadenopathy , foregut duplication cysts ( bronchogenic , oesophageal , neurenteric ) , pericardial cyst and neurogenic tumours . 
un anomalo aspetto convesso del margine cardiaco o la presenza di una linea aggiuntiva lungo il pro lo del cuore possono ugualmente essere segni radiogra ci indicativi di una massa localizzata nel mediastino anteriore . 
computed tomography scan ( b ) shows the right wall of the trachea with airsoft tissue interfaces caused by air within the tracheal lumen and right lung ( arrowhead )  . 
la scansione tc ( b ) mostra la parete laterale destra della trachea come uninterfaccia aria - tessuti molli dovuta allaria contenuta allinterno del lume tracheale ed allaria del parenchima polmonare destro adiacente ( testa di freccia )  . 
the right paratracheal stripe should be uniform in width , with a normal width ranging from 1 to 4 mm ; a right paratracheal stripe 5 mm or more wide is considered abnormally enlarged . 
 the lateral aspect of the aortopulmonary window , seen as the aorticpulmonary ( ap ) window re ection , is due to the interface between the left lung and the mediastinu at radiography , the edge of the window extends from the aortic knob to the left pulmonary artery . 
this edge should have a concave or straight border with the adjacent lung , with a straight border being considered normal unless mediastino medio il mediastino medio delimitato anteriormente dalla parete anteriore della trachea e dalla super cie posteriore del cuore , posteriormente dai corpi vertebrali , superiormente dalladitus mediastinico ed inferiormente dal diaframma . 
 esso contiene la vena cava superiore ( vcs ) , la vena cava inferiore ( vci ) , i vasi epiaortici , i vasi polmonari , la trachea , i bronchi principali , lesofago , i linfonodi , il nervo frenico , il nervo vago ed il nervo laringeo ricorrente di sinistra . 
la conoscenza del contenuto di questo compartimento facilita la diagnosi differenziale tra le masse del mediastino medio che includono linfoadenopatie , cisti disembriogenetiche da duplicazione ( broncogene , esofagee , neuroenteriche ) , cisti pericardiche e tumori neurogeni . 
nella radiogra a del torace in proiezione frontale ( a ) la linea paratracheale destra non pi apprezzabile in quanto obliterata da una massa paratracheale destra ( frecce )  . 
la scansione tc ( b ) dimostra la presenza di tumefazioni linfoghiandolari in sede paratracheale destra le quali determinano cancellazione dellinterfaccia aria - tessuti molli tra il parenchima polmonare aerato e la parete laterale destra della trachea . 
anterior to the ap window re ection , the aorticpulmonary re ection extends from the aortic arch to the level of the left main bronchus , where it usually continues the border of the left side of the heart . 
the contents of the ap window include left recurrent laryngeal nerve , left vagus nerve , radiol med ( 2011 ) 116 : 532547 dovrebbe presentare spessore uniforme compreso fra 1 e 4 mm ; una linea paratracheale di spessore superiore o uguale a 5 mm considerata patologicamente slargata . 
la porzione laterale della nestra aorto - polmonare , identi cabile come ri essione della nestra aorto - polmonare , dovuta allinterfaccia tra il parenchima polmonare sinistro ed il mediastino . 
questo margine dovrebbe avere un aspetto concavo o rettilineo rispetto al polmone adiacente ; laspetto rettilineo pu essere considerato normale a meno che esami radiogra ci precedenti non abbiano dimostrato un aspetto concavo . 
anteriormente alla ri essione della nestra ap , la ri essione aorto - polmonare si estende dallarco aortico no a livello del bronco principale sinistro , dove solitamente si continua con il pro lo sinistro del cuore . 
 nella nestra aorto - polmonare sono contenuti il nervo laringeo ricorrente di sinistra , il nervo vago di sinistra , il legamento arterioso , il tessuto adiposo mediastinico , i linfonodi e le arterie bronchiali di sinistra . 
7a - d a 14 - year - old girl with frontal view of the chest radiograph ( a ) shows a slightly convex border of the aortopulmonary window suspicious ( arrow ) for the presence of a mass in the middle mediastinu on ( c ) , computed enlarged lymph nodes are clearly seen in the aortopulmonary window ( arrow ) , causing the abnormality seen on chest radiography . 
la proiezione frontale della radiogra a del torace ( a ) mostra un margine leggermente convesso della nestra aorto - polmonare ( freccia ) sospetto per la presenza di una localizzata massa espansiva nel mediastino medio . 
nella sua porzione inferiore il recesso azygos - esofageo pu essere slargato in caso di patologia esofagea o ernia iatale [ 4 , 13 ]  . mediastino posteriore il mediastino posteriore delimitato anteriormente dallesofago , antero - inferiormente dal diaframma , posteriormente dalla parete toracica posteriore e superiormente dalladitus mediastinico . 
the lateral pro le of the descending aorta maintains a normal airsoft tissue interface with the aerated left lung , thereby preserving the normal radiographic appearance of the paraortic line . 
 la scansione tc assiale dopo somministrazione di contrasto ( c ) evidenzia una massa solida ( freccia ) ben circoscritta localizzata nel mediastino medio in contiguit con larteria polmonare sinistra . 
limmagine in risonanza magnetica ( rm ) t2 - pesata sul piano assiale ( d ) e le immagini t1 - pesate dopo somministrazione di mezzo di contrasto sul piano coronale ( e ) e sagittale ( f ) documentano una massa solida con segnale iperintenso ( frecce ) , risultata essere un tumore neurogeno ( schwannoma )  . della enopathy may cause deviation of the azygo - oesophageal line . 
 posterior mediastinum the posterior mediastinum is bounded anteriorly by the oesophagus , anteroinferiorly by the diaphragm , posteriorly le masse del mediastino posteriore sono prevalentemente causate dai tumori neurogeni , dagli ascessi paraspinali o dalleritropoiesi extramidollare ; queste masse determinano unobliterazione della linea di giunzione posteriore ed ispessimento o deformazione della linea paraortica e / o delle linee paraspinali [ 1417 ]  . 
 la linea di giunzione posteriore una linea mediastinica posteriore visibile al di sopra del livello della vena azygos e dellaorta ; essa determinata dal contatto delle super ci pleuriche viscerale e parietale della porzione radiol med ( 2011 ) 116 : 532547 fig . 
9a , b la radiogra a del torace in proiezione frontale ( a ) mostra un anomalo aspetto convesso della ri essione aorto - polmonare causato da dilatazione dellarteria polmonare sinistra come dimostrato nella scansione tc corrispondente ( b )  . 
10a - d frontal view of the chest radiograph ( a ) shows a normal azygo - oesophageal line ( arrows ) with mild leftwards convexity superiorly and a straight edge inferiorly . 
10a - d la radiogra a del torace in proiezione frontale ( a ) raf gura un aspetto normale della linea azygos - esofagea ( frecce ) che mostra una lieve convessit verso sinistra nella sua porzione superiore ed un andamento rettilineo nella sua porzione inferiore . 
le scansioni tc dopo somministrazione di mezzo di contrasto ( c ) ed rm t1 - pesata sul piano assiale dopo mezzo di contrasto ( d ) documentano la presenza di una formazione espansiva liquida nel mediastino medio ( frecce ) , risultata essere una cisti disembriogenetica . 542 radiol med ( 2011 ) 116 : 532547 fig . 
corresponding computed tomography scans ( c , d ) con rm a middle mediastinal mass ( arrows ) located in the azygooesophageal recess , which proved to be a bronchogenic cyst . 
le scansioni tc corrispondenti ( c , d ) confermano la presenza di una massa espansiva del mediastino medio ( frecce ) localizzata a livello del recesso azygos - esofageo , risultata essere una cisti broncogena . 
il margine destro del cuore ed i corpi vertebrali conservano una normale interfaccia con il parenchima polmonare destro e questo spiega la mancata cancellazione delle linee corrispondenti alla radiogra a del torace . by the posterior chest wall and superiorly by the thoracic inlet . 
posterior mediastinal masses are mostly due to neurogenic tumours , paraspinal abscess or extramedullary haematopoiesis ; these masses determine obliteration of the posterior junction line and thickening or disruption of the paraortic line and / or paraspinal lines [ 1417 ] : posterior junction line : this is a posterior mediastinal line seen above the level of the azygos vein and aorta and is formed by apposition of the visceral and parietal pleura of the posteromedial portion of the lungs posterior to the oesophagus and anterior to the third through fth thoracic vertebrae . 
it appears as a straight or mildly leftwards convex line , typically projecting postero - mediale dei due polmoni , posteriormente allesofago ed anteriormente alle vertebre toraciche dalla terza alla quinta . 
la linea di giunzione posteriore presenta una maggiore estensione craniale rispetto alla linea di giunzione anteriore e , a differenza di questultima , visibile al di sopra delle clavicole e si estende prevalentemente in senso verticale , mentre la linea di giunzione anteriore devia verso sinistra . 
12a - f frontal view of the chest radiograph ( a ) shows normal posterior junction line ( arrows ) as a straight line projecting through the trachea and extending above the clavicles . 
axial nonenhanced computed tomography ( c , d ) and sagittal preand postcontrast t1 - weighted magnetic resonance scans ( e , f ) help con rm the posterior location of the lesion , corresponding to a well - circumscribed solid mass located in the posterosuperior mediastinum between trachea and spine . 
12a - f nella radiogra a del torace in proiezione frontale ( a ) la linea di giunzione posteriore ( frecce ) rappresentata come una linea diritta che si proietta allinterno della trachea e si estende al di sopra delle clavicole . 
le scansioni assiali tc senza contrasto ( c , d ) ed rm t1 - pesate sul piano sagittale prima e dopo somministrazione di contrasto ( e , f ) confermano la localizzazione posteriore della lesione che corrisponde ad una massa solida localizzata nel mediastino posterosuperiore tra la trachea e la colonna vertebrale . 
the posterior junction line demonstrates more cranial extension than the anterior junction line and , unlike its counterpart , is seen above the clavicles and lies almost vertical , whereas the anterior junction line deviates to the lea posterosuperior meditoracica ed il polmone sinistro adiacente normalmente ventilato . 
computed tomography scans in axial ( c ) and sagittal ( d ) planes show a well - circumscribed hypodense lesion ( arrow in c and arrowhead in d ) abutting the posterolateral pro le of the descending aorta . 
le scansioni tc sul piano assiale ( c ) e sagittale ( d ) mostrano una lesione ipodensa ben circoscritta ( freccia in c e testa di freccia in d ) a contatto con il margine posterolaterale dellaorta discendente . 
the left paraspinal line is seen more frequently than the right paraspinal line due to the presence of the descending thoracic aorta on the left , which promotes the tangential contact of the left lung necessary to produce the lungmediastinum interface . 
la linea paraspinale di sinistra determinata dal contatto tangenziale del polmone sinistro e della pleura con il tessuto adiposo del mediastino posteriore , i muscoli paraspinali di sinistra ed i tessuti molli adiacenti . 
la linea paraspinale sinistra pi frequentemente visibile della linea paraspinale destra perch a sinistra la presenza dellaorta toracica discendente agevola il contatto tangenziale del polmone sinistro necessario a determinare linterfaccia polmone - mediastino . 
axial postcontrast computed tomography scans ( c , d ) help con rm a solid mass ( arrows ) located in the middle and posterior mediastinum effacing the left paraspinal and paraortic lines and extending into the spine . 
 le scansioni tc assiali eseguite dopo somministrazione di mezzo di contrasto ( c , d ) mostrano una massa solida ( frecce ) localizzata nel mediastino medio e posteriore , a contatto con le linee paraspinale sinistra e paraortica , la quale mostra estensione intraspinale . 
al contrario , le masse anteriori localizzate al di sopra delle clavicole non hanno uninterfaccia con il parenchima polmonare , e di conseguenza i loro margini non appaiono netti ; queste masse anteriori potrebbero essere totalmente intratoraciche , localizzate tipicamente nel mediastino anteriore , oppure potrebbero rappresentare unestensione intratoracica di masse localizzate nel collo . 
on the lateral chest lm ( b ) , the opacity ( arrow ) projects into the posterior mediastinu computed tomography scan ( c ) shows bilateral soft - tissue paraspinal masses ( arrows ) , representing extramedullary haematopoiesis , in a young thalassaemic patient . 
la proiezione frontale della radiogra a del torace ( a ) mostra una linea aggiuntiva ( freccia ) che decorre medialmente rispetto al margine destro del cuore e che cancella la linea paraspinale destra . 
16a - c frontal chest lm ( a ) shows enlargement of the right superior mediastinuabove the level of the clavicles , the margins of the mass are sharp ( arrow ) due to the interface with adjacent lung , indicating that the mass is located in the posterior mediastinucoronal ( b ) and sagittal ( c ) postcontrast t1 - weighted magnetic resonance scans con rm the presence of a solid inhomogeneous mass located in the posterior mediastinum , with intraforaminal extension . 
al di sopra delle clavicole i margini della lesione appaiono netti ( freccia ) per linterfaccia con il parenchima polmonare adiacente , e ci indica che la massa localizzata nel mediastino posteriore . 
le immagini rm t1 - pesate sui piani coronale ( b ) e sagittale ( c ) acquisite dopo somministrazione di contrasto confermano la presenza di una massa solida a struttura disomogenea localizzata nel mediastino posteriore con estensione intraforaminale . 
tale lesione risultata essere un tumore neurogeno . radiol med ( 2011 ) 116 : 532547 conclusions conclusioni knowledge of the normal radiographic mediastinal anatomy and the mediastinal lines is crucial to identifying subtle mediastinal abnormalities that can be easily missed on conventional radiography . 
moreover this approach allows identi cation on chest radiographs of the involved mediastinal compartment , thereby leading to the most appropriate further diagnostic workup . la conoscenza della normale anatomia radiogra ca del mediastino e delle linee mediastiniche fondamentale per identi care minime alterazioni mediastiniche che potrebbero essere facilmente misconosciute sulla radiogra a convenzionale del torace . 
giglio , cefal , italy 4department of radiology , university of verona , verona , italy 5department of radiology and cardiology , university hospital , parma , italy 6department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands correspondence to : l . 
patients with suspected cad presented the following prognostic outcome ( p < 0.0001 ) : in 41 patients with normal coronary arteries at mdct - ca , the event rate was 0% ; ve of 49 patients with nonobstructive cad had major cardiac events ; two of 35 patients with obstructive cad suffered cardiac death and 19 underwent revascularisation . 
centoventicinque pazienti ( 82 uomini , et media 57 , 410 , 3 anni ) con sospetta mac sottoposti ad ac - tcms sono stati inclusi in un follow - up a 2 anni per eventi cardiaci maggiori . 
i pazienti presentano il seguente outcome prognostico ( p < 0 , 0001 ) : nessun evento in 41 pazienti con coronarie normali alla ac - tcms ; 5 eventi cardiaci maggiori fra i 49 pazienti con mac non ostruttiva ; 2 morti cardiache e 19 rivascolarizzazioni fra i 35 pazienti con mac ostruttiva . 
nella routine clinica la ac - tcms presenta un eccellente valore prognostico a 2 anni in caso di 522 radiol med ( 2011 ) 116 : 521531 with normal coronary arteries . 
il numero di eventi cardiaci maggiori aumenta con la severit della patologia riscontrata . keywords coronary artery disease prognostic value coronary angiography multidetector row computed tomography parole chiave malattia aterosclerotica coronarica valore prognostico angiogra a coronarica tomogra a computerizzata multistrato introduction introduzione noninvasive coronary angiography ( ca ) with multidetector - row computed tomography ( mdct ) is one of the most advanced and technologically inspiring diagnostic imaging applications of the last 10 years . 
other clinical applications of mdct - ca are the follow - up of coronary artery revascularisation procedures with aortocoronary bypass surgery [ 7 ] or stenting of proximal segments [ 8 ] and evaluating the coronary circulation as part of the planning of aortic valve surgery [ 9 ]  . 
in this regard , consensus documents have been drawn up by panels of european and american experts that de ne the appropriateness and reliability of the clinical applications of the technique [ 10 , 11 ]  . 
in terms of routine clinical implementation of the technique , however , evaluating patient outcome should also be considered that is , to what extent can mdct - ca positively in uence prognosis [ 12 ] and reduce the morbidity of major cardiac events [ 13 ]  . 
whereas there are numerous studies in the literature on the diagnostic accuracy of the technique , there are very few that deal with the prognostic impact of mdct - ca [ 1418 ]  . 
the aim of our study was to de ne the prognostic value in routine clinical use over a 2 - year follow - up period of mdct - ca in patients with suspected cad . langiogra a coronarica non invasiva mediante tomogra a computerizzata multistrato ( ac - tcms ) rappresenta una delle applicazioni pi avanzate e tecnologicamente affascinanti dellultimo decennio in ambito di diagnostica per immagini . 
altre applicazioni cliniche della ac - tcms sono il follow - up delle procedure di rivascolarizzazione coronarica , mediante by - pass aorto - coronarici [ 7 ] o stenting dei segmenti prossimali [ 8 ] , e la valutazione del circolo coronarico in previsione di chirurgia della valvola aortica [ 9 ]  . 
a tale proposito , alcuni consensus documents di panel di esperti europei ed americani hanno de nito lappropriatezza e laf dabilit delle applicazioni cliniche della metodica [ 10 , 11 ]  . 
nellottica di una implementazione clinica di routine non deve essere tralasciata , tuttavia , una valutazione delloutcome del paziente ovvero in quale misura lesecuzione di una ac - tcms possa in uire positivamente sulla prognosi [ 12 ] e ridurre la morbilit degli eventi cardiaci maggiori [ 13 ]  . 
 scopo del nostro studio quello di de nire il valore prognostico nella routine clinica della ac - tcms in pazienti con sospetta mac con follow - up a 2 anni . materials and methods population materiali e metodi popolazione one hundred and twentyve patients ( 82 men , mean age 57.410.3 ) with suspected cad who underwent 64 - slice mdct - ca between september 2006 and march 2008 in our department were included in the study . 
patients underwent mdct - ca for the following clinical indications : atypical chest pain ( n = 59 ) , typical angina with inconclusive stress test ( n = 21 ) , high risk of major coronary event ( n = 24 ) and evaluation of coronary artery circulation as a part of planning for aortic valve surgery ( n = 21 )  . 
each patient centoventicinque pazienti ( 82 uomini , et media 57 , 410 , 3 anni ) con sospetta mac sottoposti ad ac - tcms a 64 strati tra settembre 2006 e marzo 2008 nel nostro dipartimento sono stati inclusi nello studio . 
i pazienti sono stati sottoposti ad ac - tcms con le seguenti indicazioni cliniche : dolore toracico atipico ( n = 59 ) , angina tipica con stress - test non conclusivo ( n = 21 ) , alto rischio di eventi coronarici maggiori ( n = 24 ) , valutazione del circolo coronarico in previsione di chirurgia della valvola aortica ( n = 21 )  . 
per ogni paziente stata inizialmente valutata la presenza di fattori di rischio radiol med ( 2011 ) 116 : 521531 was initially evaluated for the presence of cardiovascular risk factors and symptoms ( typical and atypical chest pain , angina - like symptoms )  . 
the following cardiovascular risk factors were considered : hypertension ( de ned as arterial pressure > 140 / 80 or the need for antihypertensive agents ) , hypercholesterolaemia [ low - density lipoprotein ( ldl ) > 130 mg / dl or use of statins ] , diabetes mellitus , tobacco smoking , obesity [ body mass index ( bmi ) > 27 ] and a family history of cardiovascular disease . 
the morise test was calculated for each patient to evaluate the pretest risk [ 19 ] ( table 1 )  . the following exclusion criteria were adopted : refusal to provide informed consent , severely compromised kidneys ( creatininaemia > 120 mol / l ) , known allergy to iodinated cardiovascolare e sintomi ( dolore toracico tipico ed atipico , equivalenti anginosi )  . 
sono stati considerati i seguenti fattori di rischio cardiovascolare : ipertensione ( de nita come pressione arteriosa > 140 / 80 o necessit di terapia antipertensiva ) , ipercolestorelemia ( colesterolo low density lipoprotein [ ldl ] > 130 mg / dl o assunzione di statine ) , diabete mellito , abitudine al fumo , obesit ( body mass index [ bmi ] > 27 ) , anamnesi familiare di malattie cardiovascolari . 
 the ethics committee approved the study protocol , and all patients provided informed consent . tiche , grave compromissione della funzione respiratoria , nota coronary artery disease ( cad ) ( pazienti con pregresso infarto miocardico acuto o pregresse procedure di rivascolarizzazione miocardica mediante stent o by - pass aorto - coronarici )  . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito consenso informato scritto . parametri di scansione e ricostruzione scan and reconstruction parameters all examinations were done with a 64 - slice ct system ( brilliance 64 , philips medical systems , cleveland , oh , usa )  . 
 cs was measured using a prospectively gated acquisition protocol with the following parameters : fov 140200 mm , kv 120 , mas 100 , slice thickness 3 mmdct - ca scans were performed with the following parameters : slices / collimation 64 / 0.6 mm , rotation time 420 ms , effective temporal resolution ( with 180 algorithm ) 210 ms , 120 kv , 8001040 mas , table feed 11.9 mm / s , effective slice thickness 0.8 mm , reconstruction increment 0.4 mm , fov 140240 mm ( extended cranially only for evaluating ascending aorta aneurysms )  . 
patients with a heart rate > 65 bpm were given a dose of 2040 mg of propranolol by mouth ( inderal , astrazeneca reims , reims , cedex , france ) 1 h prior to the scan to lower the heart rate . 
in the information lea et informing patients on how to prepare for the examination , treatment with 2040 mg propranolol twice daily under physician supervision was recommended in the 3 days prior to the examination to lower and stabilise the heart rate in patients with tachycardia . 
a bolus of 100120 ml of nonionic iodinated contrast agent ( iomeprol , iomeron 400 , bracco , milan , italy ) , dosed according to the scan range , was administered at an injection rate of 5 ml / s using an automatic injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an 18 - gauge needle cannula placed in a right antecubital ve intracoronary enhancement was optimised by using the bolus - tracking technique , which involved placing a region of interest ( roi ) at the level of the ascending aorta in order to synchronise the beginning of the scan with the arrival of the contrast agent in the scan target . 
data were retrospectively reconstructed in the end - diastolic phase ( from 65% to 80% of the rr interval ) and end - systolic phase ( 4045% )  . tutte le indagini sono state eseguite mediante tc a 64 - strati ( brilliance 64 , philips medical systems , cleveland , ohio , usa )  . 
il cs stato eseguito mediante acquisizione cardio - sincronizzata prospettica con i seguenti parametri : eld of view ( fov ) 140200 mm , kv 120 , mas 100 , spessore di strato 3 m le scansioni ac - tcms sono state effettuate con i seguenti parametri : strati / collimazione 64 / 0 , 6 mm , tempo di rotazione 420 ms , effettiva risoluzione temporale ( con algoritmo a 180 ) 210 ms , 120 kv , 8001040 mas , avanzamento del tavolo 11 , 9 mm / s , spessore effettivo di strato 0 , 8 mm , incremento di ricostruzione 0 , 4 mm , fov 140240 mm ( esteso cranialmente solamente per la valutazione di aneurismi dellaorta ascendente )  . 
i pazienti con frequenza cardiaca > 65 battiti per minuto ( bpm ) hanno ricevuto una dose di 2040 mg di propranololo cloridrato per via orale ( inderal , astrazeneca reims , reims , cedex , francia ) unora prima della scansione per ridurre la frequenza cardiaca . 
nella nota informativa preliminare di preparazione allesame era stato consigliato un trattamento con 2040 mg due volte al giorno sotto controllo medico nei tre giorni precedenti lindagine per ridurre e regolarizzare la frequenza cardiaca nei pazienti con tachicardia . 
allintera popolazione stata , altres , somministrata una dose di 2 , 5 mg di diazepam ( tranquirit , aventis pharma , waterford , irlanda ) unora prima della scansione . 
un bolo di 100120 ml di mezzo di contrasto iodato non - ionico ( iomeprol , iomeron 400 , bracco , milano , italia ) , a seconda del range di scansione , stato iniettato con un usso di 5 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 18 gauge , posizionata in una vena antecubitale destra . 
allo scopo di ottimizzare lenhancement intracoronarico la sincronizzazione dellinizio della scansione con il passaggio del bolo di mezzo di contrasto stata eseguita mediante bolus tracking , con una region of interest ( roi ) posizionata al livello dellaorta ascendente . 
i dati sono stati ricostruiti con tecnica retrospettiva in fase telediastolica ( dal 65% all80% dellintervallo r - r ) e telesistolica ( 40%45% )  . image and data analysis analisi delle immagini e dei dati the examinations were evaluated by two radiologists le indagini sono state valutate da due radiologi con esperadiol med ( 2011 ) 116 : 521531 with experience in mdct - ca [ 21 ] who transferred the data sets to a dedicated workstation ( extended brilliance workspace , version 3.0.1.3200 , philips medical systems ) for image postprocessing , with no information on patient history . 
data from the mdct - ca scans were analysed with the following postprocessing techniques : multiplanar reconstructions ( mpr ) , curved mpr ( cmpr ) , maximum intensity projections ( mip ) and volume rendering ( vr )  . 
the atherosclerotic coronary plaques were recognised as structures with a thickness of at least 1 mm2 , either within or adjacent to the coronary artery lumen and clearly distinguishable from the opaci ed lumen and the surrounding epicardial tissue [ 23 ]  . 
obstructive cad was de ned as the presence of plaque causing > 50% lumen reduction ; nonobstructive cad was de ned as the presence of plaque causing 50% lumen reduction . 
patients were therefore classi ed as belonging to the following groups based on the mdct - ca ndings : patients with normal coronary arteries , patients with nonobstructive cad and patients with obstructive cad . follow - up follow - up was carried out with an outpatient visit or by telephone , with additional checks in the archives of the pertinent centre . 
all patients were followed up for 2 years to record the following major cardiac events : cardiac death , myocardial infarction , hospitalisation and myocardial revascularisation procedures . statistical analysis patient characteristics were compared using the chi - squared test . 
statistical analysis was carried out with a dedicated software package ( spss 12.0 , spss , chicago , il , usa )  . rienza in ac - tcms [ 21 ] , che hanno caricato i set di dati in una workstation dedicata ( extended brilliance tm workspace , version 3.0.1.3200 , philips medical systems , cleveland , ohio , usa ) per il post - processing delle immagini , in assenza di notizie anamnestiche . 
tutti i dati delle scansioni ac - tcms sono stati analizzati mediante mezzi di postprocessing quali ricostruzioni multiplanari ( mpr ) , mpr curve ( cmpr ) , proiezioni massima intensit ( mip ) , e volume rendering ( vr )  . 
le placche aterosclerotiche coronariche sono state identi cate come strutture dello spessore di almeno 1 mm2 , entro o adiacenti il lume coronarico , chiaramente distinguibili dal lume opacizzato e dal circostante tessuto epicardico [ 23 ]  . 
la mac ostruttiva stata de nita dalla presenza di placche determinanti > 50% di stenosi del lume ; la mac non ostruttiva stata de nita dalla presenza di placche determinanti 50% di stenosi del lume . 
i pazienti sono stati pertanto classi cati come appartenenti ai seguenti gruppi sulla base dei risultati della ac - tcms : pazienti con coronarie normali , pazienti con mac non ostruttiva , pazienti con mac ostruttiva . follow - up il follow - up stato effettuato mediante visita ambulatoriale o contatto telefonico , con ulteriore veri ca negli archivi dellospedale di riferimento . 
tutti i pazienti sono stati inclusi in un follow - up di 2 anni con attenzione ai seguenti eventi cardiaci maggiori : morte cardiaca , infarto miocardico , ospedalizzazione ed eventuali interventi di rivascolarizzazione miocardica . analisi statistica le caratteristiche dei pazienti sono state confrontate mediante test del chi - quadrato . 
la valutazione statistica stata eseguita con software dedicato ( spss 12.0 , spss , chicago , iiiinois )  . results risultati a total of 1824 segments ( 97.3% ) were evaluated ; 51 sono stati complessivamente valutati 1824 segmenti ( 97 , 3% )  . 
alla ac - tcms evidente una stenosi > 50% ( testa di freccia ) del tratto prossimale della arteria discendente anteriore mediante immagini vr ( a , b ) e mappe coronariche ( c , d )  . 
mdct - ca identi ed 41 patients ( 32.8% ) with normal coronary arteries , 49 ( 39.2% ) with nonobstructive cad and 35 ( 28% ) with obstructive cad . 
single - vessel obstructive cad was found in 19 patients , two - vessel disease in ten and three - vessel disease in six , with a prevalence of disease in the proximal and mid segments of the coronary arteries ( 72% )  . 
la ac - tcms ha evidenziato 41 pazienti ( 32 , 8% ) con coronarie normali , 49 ( 39 , 2% ) con mac non ostruttiva e 35 ( 28% ) con mac ostruttiva . 
stata riscontrata mac ostruttiva monovasale in 19 pazienti , bivasale in 10 pazienti , trivasale in 6 pazienti , con prevalenza nei segmenti prossimali e medi delle arterie coronarie ( 72% )  . 
2 curve di kaplan - meier per tutti gli eventi in pazienti ( n = 125 ) con arterie coronarie normali , con mac non ostruttiva ed ostruttiva ( log rank test , p < 0 , 0001 )  . 
 variabile indipendente messa in evidenza dallanalisi multivariata ( hazard ratio [ hr ] 10 , 1393 , 95% intervallo di con denza [ ic ] 3 , 218931 , 9379 , p < 0 , 0001 )  . 
 other clinical applications of mdct - ca are the followup of coronary artery revascularisation procedures with aortocoronary bypass surgery [ 7 ] or stenting of proximal segments [ 8 ] and evaluating the coronary circulation as part of the planning of aortic valve surgery [ 9 ]  . 
consensus documents have been drawn up by panels of european and american experts that de ne the appropriateness and reliability of the clinical applications [ 10 , 11 ]  . 
 [ 14 ] presented a preliminary demonstration of how mdct - ca can provide independent prognostic that provided by conventional risk factors in predicting cardiac events in patients with suspected or known cad . 
in a study information superior la ac - tcms fornisce risultati eccellenti nella valutazione della patologia aterosclerotica coronarica con elevata sensibilit e notevole valore predittivo negativo , che suggeriscono un impiego della metodica per lesclusione e lidenti cazione della mac [ 15 ]  . 
si rileva , pertanto , un suo sempre maggior utilizzo nella pratica clinica per la valutazione di una sospetta aterosclerosi coronarica con valori di sensibilit e valore predittivo negativo rispettivamente del 97 , 6% e del 93 , 5% [ 6 ]  . 
altre applicazioni cliniche della ac - tcms sono il follow - up delle procedure di rivascolarizzazione coronarica mediante by - pass aorto - coronarico [ 7 ] e stenting dei segmenti prossimali [ 8 ] , nonch la valutazione del circolo coronarico in previsione di chirurgia della valvola aortica [ 9 ]  . 
consensus documents di panel di esperti europei ed americani hanno de nito lappropriatezza diagnostica delle applicazioni cliniche della metodica nel tentativo di delimitarne opportunamente il raggio di azione [ 10 , 11 ]  . 
tuttavia , una implementazione clinica di routine della metodica necessita di una valutazione del suo impatto prognostico a seconda delle speci che possibili indicazioni [ 12 , 13 ]  . 
 [ 14 ] hanno preliminarmente dimostrato come la ac - tcms sia radiol med ( 2011 ) 116 : 521531 done with a 16 - slice scanner and 12 months of follow - up , gilard et al . 
at the same time , electron - beam ct has demonstrated independent incremental value over the conventional risk factors in predicting mortality in patients with suspected cad over a lengthy follow - up period of 78 months [ 16 ]  . 
the presence of obstructive cad takes on a signi cant predictive value with regard to cardiac events in the follow - up . our study ts into this area of research , which still requires thorough investigation . 
we evaluated patients who underwent mdct - ca with precise clinical indications based on the applications laid down in the european and american reference documents [ 10 , 11 ]  . 
the ndings of our 24 months of follow - up are in agreement with previous studies and con rm the excellent prognostic outcome of mdct - ca in patients with healthy coronary arteries at mdct - ca , with independent additional value with respect to conventional risk factors ( table 2 )  . 
in agreement with other recent studies [ 24 , 25 ] , the technique provides an incremental value over cs , as obstructive cad was identi ed in some patients with cs = 0 . 
mdct - ca displays a high prognostic value in cases with the precise clinical indication for the technique and especially in patients at intermediate risk [ 11 , 26 ]  . our study provides no prognostic indications regarding the clinical application of mdct - ca in the follow - up of patients after myocardial revascularisation with stent deployment or aortocoronary bypass surgery [ 27 , 28 ]  . 
 mdct - ca is nonetheless limited in this setting ( stent diameter and material , vessel diameter , massive calci cations , metal clips ) and therefore requires selected clinical indications ( symptomatic patients with chest pain ) [ 10 , 11 ]  . 
prognostic considerations in this setting must take into account these intrinsic limitations , as well as the greater risk of major cardiac events in patients with known cad . the limitations of our study include the medium - term follow - up and the limited number of patients studied considering the heterogeneity of the clinical indications . 
the high prevalence of in grado di fornire informazioni prognostiche indipendenti e superiori rispetto a quelle dei convenzionali fattori di rischio nel predire gli eventi cardiaci in pazienti con sospetta o nota mac attraverso un follow - up a 12 mesi [ 14 ]  . 
 [ 15 ] hanno confermato che una ac - tcms negativa per mac in una popolazione di pazienti con sospetta malattia associata a ridotti tassi di mortalit ( 0% ) ed infarto miocardico ( 0 , 7% ) in un follow - up condotto a 12 mesi . 
 parallelamente la tc a fascio di elettroni ha mostrato un valore addizionale ed indipendente sopra i fattori di rischio convenzionali nel predire le cause di mortalit in pazienti con sospetta mac in un lungo follow - up condotto a 78 mesi [ 16 ]  . 
 [ 17 ] in un follow - up a 144 mesi di pazienti con sospetta o nota mac sottoposti ad ac - tcms a 64 strati hanno riscontrato un tasso di eventi cardiaci del 34% nei pazienti con mac , mentre nessun evento stato rilevato nei pazienti con coronarie normali . 
la presenza di mac ostruttiva assume invece un signi cativo valore predittivo riguardo eventi cardiaci nel follow - up . il nostro studio si inserisce in questo lone di letteratura non ancora estensivamente analizzato . 
 stata presa in considerazione una popolazione di pazienti sottoposta ad ac - tcms con precise indicazioni cliniche sulla base delle applicazioni suggerite dai documenti di riferimento europei ed americani [ 10 , 11 ]  . 
i risultati del nostro followup a 24 mesi sono in linea con gli studi precedenti e confermano leccellente outcome prognostico della ac - tcms in pazienti con coronarie indenni alla ac - tcms , con un valore addizionale indipendente rispetto a quello dei fattori di rischio convenzionali ( tabella 2 )  . 
in accordo con altre recenti esperienze [ 24 , 25 ] , la metodica presenta peraltro un valore incrementale sul cs , dal momento che in alcuni pazienti con cs = 0 stata identi cata mac ostruttiva . 
la ac - tcms trova rilevanti correlati prognostici nella precisa indicazione clinica allindagine ed in particolare nella popolazione a rischio intermedio [ 11 , 26 ]  . la nostra esperienza non fornisce indicazioni prognostiche circa lapplicazione clinica della ac - tcms nel follow - up dei pazienti sottoposti a rivascolarizzazione miocardica mediante posizionamento di stent o confezionamento di by - pass aorto - coronarico [ 27 , 28 ]  . 
la ac - tcms presenta comunque note limitazioni in tale contesto ( diametro e materiale degli stent , calibro dei vasi , massive calci cazioni , clips metalliche ) e , pertanto , richiede selezionate indicazioni cliniche ( pazienti sintomatici con dolore toracico ) [ 10 , 11 ]  . 
considerazioni prognostiche in tale ambito non possono prescindere da tali limitazioni intrinseche e dal rischio superiore di eventi cardiaci maggiori associati a pazienti con nota mac . nel novero delle limitazioni del nostro studio , possono essere inclusi il follow - up effettuato a medio termine ed il 530 radiol med ( 2011 ) 116 : 521531 disease identi ed with mdct - ca ( 67.2% ; nonobstructive cad 39.2% ; obstructive cad 28% ) could be interpreted as a study limitation , although this prevalence may be seen as the result of selecting a clinically justi ed population based on the examination appropriateness criteria . 
the rapid technical progress in multislice technology may further facilitate the use of the technique , especially with the implementation of prospective gating , which markedly reduces the radiation dose delivered [ 2931 ]  . conclusions ridotto numero di pazienti , in considerazione delleterogeneit delle indicazioni cliniche . 
una ulteriore limitazione pu essere costituita dallalta prevalenza di malattia identi cata con ac - tcms ( 67 , 2% ; mac non ostruttiva 39 , 2% , mac ostruttiva 28% ) , sebbene possa essere considerata risultato della selezione di una popolazione clinicamente giusti cata dai criteri di appropriatezza dellindagine . 
il rapido progresso tecnico della tecnologia multistrato potr ulteriormente facilitare lutilizzo clinico della metodica , specialmente con unimplementazione della cardio - sincronizzazione prospettica , che implica una netta riduzione della dose di radiazioni somministrata ai pazienti [ 2931 ]  . the use of mdct - ca in routine clinical practice on the basis of precise indications offers an excellent prognostic value in 2 years of follow - up in cases of normal coronary arteries ; the number of major cardiac events increases with increasing severity of the disease identi ed . 
national and multinational prognostic trials coupled with the adoption of new technological solutions aimed at signi cantly reducing the radiation dose delivered to the patient will further facilitate the clinical use of this technique . conclusioni la ac - tcms eseguita nella routine clinica sulla base di de nite indicazioni presenta un eccellente valore prognostico nel follow - up a 2 anni in caso di coronarie normali ; il numero di eventi cardiaci maggiori aumenta con la severit della patologia riscontrata . 
recall rate and cancer detection rate at rst reading or informed second reading only were assessed in a cohort of 23 , 629 women aged 5069 years screened during 20072008 . 
sono stati valutati il tasso di richiamo alla prima e alla sola seconda lettura informata osservati in una coorte di 23629 donne di et compresa fra 50 e 69 anni , sottoposte a screening durante gli anni 20072008 . 
il tasso di richiamo ad approfondimento stato del 13 , 0% alla prima e del 2 , 7% alla sola seconda lettura ( tasso incrementale di richiamo + 21 , 1% )  . 
il tasso diagnostico di carcinoma stato del 7 , 06 ( 167 casi ) alla prima lettura e dello 0 , 93 ( 22 casi ) alla sola seconda lettura ( tasso incrementale diagnostico di carcinoma + 13 , 1% )  . 
il costo dellaggiunta della seconda lettura stato di + 3 , 65 euro per soggetto sottoposto a screening , o 3.926 , 61 euro per carcinoma aggiuntivo diagnosticato . 576 radiol med ( 2011 ) 116 : 575583 gures are within the range of literature reports on doublereading performance . 
lo studio conferma lutilit della seconda lettura anche in aggiunta alla lettura diretta con approfondimento immediato : il tasso incrementale di richiamo risulta accettabile in considerazione del tasso incrementale diagnostico di carcinoma , con valori entrambi nel range di quanto riportato in letteratura in tema di doppia lettura . 
 parole chiave carcinoma mammario screening mammogra a doppia lettura introduction introduzione double reading has been shown to increase cancer detection rate compared with single reading , at the acceptable cost of a moderate increase in recall rate [ 13 ] , and has been recommended for many years as a standard procedure in mammography screening [ 4 ]  . 
the main features of the programme have been already reported [ 5 ] , as well as a favourable sensitivity estimate , based on the proportional incidence of interval cancers [ 6 ]  . 
double reading has not been adopted for several years on the assumption that immediate assessment , by allowing for an easier , and thus higher , recall rate of minor mammography abnormalities , would equally achieve a good sensitivity level [ 5 ]  . 
 la doppia lettura si dimostrata capace di aumentare il tasso diagnostico di carcinoma sospetto alla lettura singola , al costo di un accettabile aumento del tasso di richiamo [ 13 ] , e viene raccomandata da molti anni come procedura standard per lo screening mammogra co [ 4 ]  . 
le principali caratteristiche del programma sono gi state riportate [ 5 ] , cos come una stima favorevole della sensibilit basata sullincidenza proporzionale di carcinoma di intervallo [ 6 ]  . 
la doppia lettura non stata adottata dal programma per molti anni , in base alla convinzione che la lettura diretta con possibilit di approfondimento immediato , facilitando un maggior tasso di richiamo di anomalie mammogra che , consentisse una buona sensibilit , analoga alla doppia lettura differita [ 5 ]  . 
recentemente le autorit regionali hanno diffuso speci che raccomandazioni per ladozione di protocolli di screening omogenei a livello regionale e la doppia lettura quindi stata adottata a partire da marzo 2007 . 
il presente studio analizza i risultati delladozione di questa seconda lettura differita quando af ancata alla prima lettura diretta con approfondimento immediato . material and methods materiali e metodi during the study period , 23 , 629 women resident in the local health unit and aged 5069 years were invited and examined . 
real - time rst reading with immediate assessment was carried out by one radiologist at a rate of ten cases per hour ( corresponding to the workload of two radiographers ) for a total of 60 cases per 6 - h session . 
 cases with negative rst reading or positive rst reading durante il periodo di studio sono state invitate ed esaminate 23.629 donne residenti nellunit locale socio - sanitaria di et compresa fra 50 e 69 anni . 
la prima lettura diretta con eventuale approfondimento immediato stata condotta da un radiologo in ragione di 10 casi lora ( corrispondente al carico di lavoro di due tecnici di radiologia ) per un totale di 60 casi per sessione di 6 ore . 
le donne con prima lettura negativa o prima lettura radiol med ( 2011 ) 116 : 575583 and negative assessment were informed that second reading would follow and that a nal report would be sent by mail or that they would be recalled for further assessment . 
three radiologists were involved in reading in the study period : two were expert readers ( > 5 years experience in mammography reading ) and one had a lower level of experience ( 1 year )  . 
 all radiologists were involved in rst reading , whereas only the two more expert radiologists were involved in second reading . variables in the study database were patients age , ndings at rst reading and immediate assessment ( if any ) , ndings at second reading and delayed assessment ( if any ) and breast density currently reported according to breast imaging reporting and data system ( bi - rads ) d14 classi cation system [ 7 ]  . 
the nal outcome of immediate or delayed assessment , including excision histology ( if any ) , was available in all cases . the study evaluated incremental recall rate and incremental cancer detection rate at second reading ( cases recalled and cancers detected by the second reader only ) compared with rst reading with immediate assessment . 
assuming an average of 1 min of radiologists working time per case read at delayed second reading [ 8 ] , that is , at least 300 cases read per working session , it was estimated that 23 , 629 second readings could be easily managed within a radiologists yearly workload . 
the cost of incremental assessment [ unit cost of physical breast examination ( pbe ) , ultrasonography ( us ) , ne - needle aspiration cytology ( fnac ) , core needle biopsy ( cnb ) and surgical benign biopsies ] generated by second reading was calculated according to health service of cial tariffs , as previously reported [ 9 ]  . 
 positiva e approfondimento negativo sono state informate che sarebbe seguita una seconda lettura e che il risultato nale sarebbe stato inviato per posta o ci sarebbe stato un richiamo per ulteriore approfondimento . 
tre radiologi sono stati coinvolti nella lettura : due erano lettori esperti ( oltre 5 anni di pratica mammogra ca ) , uno era meno esperto ( 1 anno di pratica mammogra ca )  . 
 tutti i radiologi sono stati coinvolti nella prima lettura , mentre solo i due lettori pi esperti sono stati coinvolti nella seconda lettura . le variabili disponibili nel materiale in studio erano : et della paziente , risultato alla prima lettura e alleventuale approfondimento immediato , risultato alla seconda lettura e alleventuale ulteriore approfondimento , densit del seno ( classi cata secondo la classi cazione breast imaging reporting and data system [ bi - rads ] d1 - 4 [ 7 ] )  . 
il risultato nale delleventuale approfondimento immediato o differito , compresa listologia chirurgica , era disponibile in tutti i casi . lo studio ha valutato il tasso incrementale di richiamo e il tasso incrementale diagnostico di carcinoma generati dalla sola seconda lettura ( casi richiamati e cancri diagnosticati solo grazie alla seconda lettura ) confrontandoli con i risultati della lettura diretta con approfondimento immediato . 
i costi della seconda lettura sono stati equiparati al costo medio annuale di un radiologo ( dirigente di primo livello ) : assumendo un tempo di lettura medio per caso di 1 minuto alla lettura differita [ 8 ] , cio almeno 300 letture per turno giornaliero , si ritenuto che le 23.629 seconde letture potessero facilmente essere erogate in un tempo pari a un anno / radiologo . 
il costo incrementale dellapprofondimento diagnostico ( costo unitario di esame clinico [ ec ] , ecogra a [ us ] , citologia [ ne needle aspiration cytology , fnac ] , core biopsy [ ncb ] , e biopsie chirurgiche benigne ) generato dalla sola seconda lettura stato calcolato in base alle tariffe del servizio sanitario , come riportato in una precedente pubblicazione [ 9 ]  . 
 associata allet ( d3 - 4 per 5059 anni = 25 , 0% , per 6069 anni = 5 , 7% , p < 10 - 6 ) , anche se la frazione complessiva di soggetti con seno denso risultata relativamente bassa ( 17 , 1% )  . 
complessivamente sono stati diagnosticati 189 carcinomi ( 7 , 99 ) , 167 ( 7 , 06 ) alla prima lettura e 22 ( 0 , 93 ) alla sola seconda lettura . 
cost per incremental cancer detected ( n = 22 ) was 3 , 926.61. discussion this study is based on a large consecutive screening series , alla prima stato di + 13 , 1% . 
as previously reported in detail [ 5 ] , real - time reading with immediate assessment is a common procedure in clinical mammography practice but has been rarely adopted in screening , as the recommendation for double reading was issued and diffusely adopted . 
the main reason for this is the dif culty combining real - time rst reading with second reading the latter being necessarily delayed and managing the large workload required by screening , given the limitation in the number of cases screened per session when the immediate assessment approach is adopted . 
other minor negative aspects are represented by : ( a ) the need for a temporary negativity being reported to the woman after rst reading , whereas a de nitive report has to be delayed until second reading , and ( b ) the problematic but unlikely ( about 3% of cases ) event of a woman with a negative rst reading but recalled for a positive second reading : evident discrepancy between readers occasionally caused the rst reader to be blamed for inaccuracy or the second reader to be blamed for excess suspicion when assessment was negative . 
 as expected , the major determinant of recall at rst discussione questo studio si basa su una ampia casistica di screening che consente una valutazione af dabile del contributo della seconda lettura differita aggiunta ad un protocollo di lettura diretta con approfondimento immediato . 
come precedentemente riportato in dettaglio [ 5 ] , la lettura diretta con approfondimento immediato una procedura comune per la mammogra a clinica , ma stata raramente adottata nello screening , da quando la raccomandazione della doppia lettura stata diffusa e recepita . 
la ragione principale sta nella dif colt di combinare la lettura diretta con la seconda lettura , necessariamente differita , e di gestire il massiccio carico di lavoro imposto dallo screening , data la limitazione nel numero di casi esaminati per seduta quando si impieghi la lettura diretta con approfondimento immediato . 
altri aspetti negativi minori sono rappresentati da : ( a ) la necessit di comunicare alla donna una negativit temporanea dopo la prima lettura , mentre la risposta de nitiva rimandata al completamento della seconda lettura ; ( b ) levento problematico , ma raro ( circa il 3% dei casi ) di una donna con una prima lettura negativa , poi richiamata ad approfondimento diagnostico per una seconda lettura positiva . 
la discrepanza tra i due lettori risulta evidente ed ha occasionalmente causato rimostranza per linaccuratezza del primo lettore o , in caso di approfondimento negaradiol med ( 2011 ) 116 : 575583 reading was the presence of a dense breast . 
this is easily explained by the reader being less con dent in issuing a negative report in the presence of multiple superimposed opacities with ill - de ned , masked margins . 
breast density justi ed a higher recall rate in the younger decade , although such a difference was less marked due to the low overall prevalence of dense breasts in both considered age groups . 
such a low overall prevalence of dense breasts is not surprising , as the screening population was mostly postmenopausal , and this explains why most recalls occurred in d1 - 2 breasts . 
the possibility of immediate assessment favoured recall , which was in fact very high ( 13.0% ) , especially considering that most cases in the study series were at repeat screening , which is usually associated with lower recall rates ( reference european commission guidelines standard for repeat screening is < 5% )  . 
incremental recall rate at second reading was not particularly high ( + 2.7% ) , and the increase relative to rst reading ( + 21.1% ) was comparable with what has been previously reported [ 1 ] , although comparisons with the literature may be biased , as the relative increase depends on the high recall rate at rst reading . 
the rationale of facilitating and increasing recall rate to improve sensitivity is challenged by the observation of similar sensitivity estimates with quite different levels of recall rate [ 10 , 11 ] and denied by a study comparing screening practice in the us and uk , where it is quite evident that excess recall rates over recommended standards translate into higher costs but not into higher sensitivity [ 12 ]  . 
other studies investigating the optimal recall rate to improve sensitivity suggest that recall rates > 67% are unlikely to provide cost - effective extra bene ts for cancer detection [ 13 , 14 ]  . in this study , the relative incremental cancer detection rate by second reading ( + 13.1% ) was substantial , at the upper limit of what is commonly reported with conventional double reading [ 13 ]  . 
of course , the performance of rst or second reading as to cancer detection rate depends only on the procedure itself but also on the skill of the radiologists involved . 
it might be argued that in this study , the involvement of one reader with limited experience more likely to have a low sensitivity facilitated a better performance of second reading , but this does not seem to be the case , as a substantial contribution of second reading to cancer detection rate persists even after excluding cases in which the inexperienced reader was involved ( + 9% )  . the study con rms the ef cacy of second reading . 
the incremental recall rate ( + 21.1% ) is acceptable in view of the incremental cancer detection rate ( + 13.1% ) , and both gures are within the range of literature reports on tivo , di eccesso di sospetto per il secondo lettore . come atteso , lelemento che maggiormente in uenza il tasso di richiamo alla prima lettura la presenza di seno denso : questo si spiega facilmente per la minore tranquillit del radiologo nel rilasciare un referto negativo in presenza di opacit multiple sfumate e sovrapposte . 
la densit del seno giusti ca il maggior tasso di richiamo nella decade pi giovane , anche se la differenza per et meno marcata per la frequenza comunque bassa di seni densi nelle due classi di et considerate . 
una bassa frequenza di seni densi non sorprende , trattandosi di una popolazione prevalentemente in menopausa , e spiega perch comunque la maggior parte dei richiami avviene in donne con seno di densit d1 - 2 . 
la possibilit di eseguirlo immediatamente ha favorito il richiamo stesso alla prima lettura , con un tasso molto elevato ( 13 , 0% ) , specie tenendo conto che la maggioranza dei soggetti in studio era ad uno screening ripetuto , in genere associato ad un tasso di richiamo pi basso ( il valore di riferimento delle linee guida della comunit europea per lo screening ripetuto < 5% )  . 
il tasso di richiamo alla sola seconda lettura non stato particolarmente alto ( + 2 , 7% ) , e laumento relativo dei richiami rispetto alla prima lettura ( + 21 , 1% ) paragonabile a quanto riportato in altre esperienze [ 1 ] anche se il confronto con la letteratura discutibile , essendo laumento relativo in uenzato dallelevato tasso di richiamo alla prima lettura . 
il contenimento del tasso di richiamo resta un riferimento per la performance di screening : il razionale di facilitare e aumentare il tasso di richiamo per migliorare la sensibilit contraddetto dallosservazione di sensibilit paragonabili pur con tassi di richiamo molto diversi [ 10 , 11 ] : uno studio ha confrontato pratiche di screening negli usa e nel regno unito , dimostrando chiaramente che un eccesso di richiami oltre gli standard raccomandati si traduce in costi pi elevati , ma non in maggiore sensibilit [ 12 ]  . 
altre esperienze che hanno studiato il tasso di richiamo ottimale per migliorare la sensibilit suggeriscono che tassi di richiamo superiori al 6%7% abbiano poca probabilit di fornire vantaggi aggiuntivi e costo - ef caci quanto a tasso diagnostico di carcinoma [ 13 , 14 ]  . nel presente studio , il tasso incrementale diagnostico di carcinoma relativo alla sola seconda lettura ( + 13 , 1% ) stato piuttosto elevato , ai limiti superiori di quanto stato comunemente riportato in letteratura per la doppia lettura convenzionale [ 13 ]  . 
ovviamente la prestazione della prima o della seconda lettura quanto a tasso diagnostico di carcinoma non dipende solo dalla procedura di per s , ma anche dalla capacit dei radiologi coinvolti . 
si potrebbe osservare che nel presente studio linclusione tra gli addetti alla prima lettura di un radiologo meno esperto , pi esposto al rischio di una bassa sensibilit , potrebbe aver facilitato una buona performance della seconda lettura , ma non sembra che questo sia il caso dal momento che anche escludendo i casi in cui era coinvolto il lettore meno esperto il contributo della seconda lettura resta sostanziale ( + 9% )  . lo studio conferma lef cacia della seconda lettura . 
the positive predictive value at rst reading was 5.4% , largely inferior to recommended standards , and was due to a tendency for higher recall speci c to the readers , further magni ed by the opportunity for immediate assessment . 
the positive predictive value of recall at second reading only was 3.3% , comparable with that reported in other screening experiences with a much higher positive predictive value at rst reading [ 1 ]  . 
a tendency for cancers detected at second reading only to be depicted as isolated microcalci cations or distortions could be explained , as most suspicious presentations , such as irregular mass densities , were easily picked up at rst screening . 
although the sample size does not allow for statistical signi cance , cancers detected at second reading only were less advanced in stage , which adds further value to the bene ts of second reading in terms of incremental cancer detection rate . the direct cost of screening in the programme reported here has not yet been assessed in this study due to the complexity of such an evaluation . 
however , assuming a cost of 50100 per woman screened and of 67 , 000 per cancer detected in accordance to what has been estimated for other italian programmes when single reading was in use [ 15 ] , the incremental costs of 3.65 per woman screened and 3 , 926.61 per incremental cancer detected seem fully acceptable . in conclusion , our study ndings con rm the usefulness of second reading of screening mammograms and the limitations of single reading , even if read in real time with immediate assessment . 
as a consequence of these ndings , in this scenario , the real - time reading plus immediate assessment policy has been abandoned in favour of conventional delayed double reading , as in the rest of italian screening programmes . 
 bile in considerazione del tasso incrementale diagnostico di carcinoma ( + 13 , 1% ) ed entrambi questi valori sono compatibili con quanto riportato in letteratura sulle prestazioni della doppia lettura [ 13 ]  . 
il valore predittivo positivo alla prima lettura stato del 5 , 4% , ampiamente inferiore agli standard raccomandati , ed ascrivibile ad una maggiore tendenza al richiamo dei lettori coinvolti , ulteriormente potenziata dallopportunit dellapprofondimento immediato . 
il valore predittivo positivo alla sola seconda lettura stato del 3 , 3% , confrontabile con quanto riportato in altre esperienze che osservano un valore predittivo positivo pi elevato alla prima lettura [ 1 ] : una caduta sostanziale del valore predittivo positivo alla seconda lettura atteso , considerando la prevalenza pi bassa di carcinomi ancora disponibili per lidenti cazione dopo la prima lettura . 
 la tendenza dei carcinomi identi cati alla sola seconda lettura a apparire in forma di microcalci cazioni e distorsioni si pu spiegare con il fatto che le presentazioni pi sospette , come le densit di massa a margini irregolari , sono tendenzialmente identi cate alla prima lettura . 
anche se il campione in esame non consente di raggiungere la signi cativit statistica , i carcinomi identi cati alla sola seconda lettura risultano in stadio meno avanzato , il che aggiunge ulteriore valore ai bene ci della seconda lettura in termini di diagnosi aggiuntive di carcinoma . il costo diretto dello screening nel presente programma , dal momento che tale valutazione assai complessa , non stato possibile in questo studio e non disponibile un preciso riferimento con cui confrontare i costi della seconda lettura differita nello stesso scenario . 
rispetto a una assunzione approssimativa di 50100 euro per donna esaminata e di 60007000 euro per cancro diagnosticato , in analogia a quanto stato stimato per altri programmi italiani quando la lettura singola differita era ancora in uso [ 15 ] , il costo di 3 , 65 euro per donna esaminata e di 3926 , 61 euro per cancro aggiuntivo diagnosticato appaiono del tutto accettabili . in conclusione , i risultati del presente studio confermano lutilit della seconda lettura delle mammogra e di screening e segnalano i limiti della lettura singola , anche se refertata in diretta con eventuale approfondimento immediato . 
in seguito a questi risultati la pratica della lettura diretta con approfondimento immediato stata abbandonata in favore della doppia lettura differita convenzionale , protocollo comune al resto dei programmi di screening italiani . 
pansini 5 , 80131 napoli , italy 2istituto di bioimmagini e biostrutture ( c.n.r. ) , napoli , italy 3dipartimento di endocrinologia e oncologia molecolare e clinica , universit degli studi di napoli federico ii , napoli , italy 4dipartimento di medicina interna , clinica e sperimentale , seconda universit di napoli ( sun ) , napoli , italy 5u.o.c. 
radiol med 111 ( suppl 1 ) 2006 received : 1 april 2010 / accepted : 25 may 2010 / published online : 1 february 2011 springer - verlag 2011 abstract purpose . 
fourteen consecutive patients ( eight men and six women , aged 2654 years ) with men 1 underwent mdct performed with a 4 ( n = 5 ) or 64 ( n = 9 ) detector - row system and eus done with a radial transducer ( 7.520 mhz ) within 728 days of each other . 
 prior to mdct examination , patients were given 750 cc of water and asked to lie down in the right lateral decubitus for 15 mmultiphase mdct images were acquired both before and after the injection of nonionic iodinated contrast material ( 2 cc / kg ) at an injection rate of 4 ml / s , with technical parameters and scan delay varying in relation to the system used . 
quattordici pazienti consecutivi ( 8 maschi , 6 femmine ; 2654 anni ) affetti da men - 1 sono stati sottoposti sia a tcms , eseguita con 4 ( n = 5 ) o 64 le di detettori ( n = 9 ) , che ad eus eseguita con strumento radiale ( 7 , 520 mhz ) entro 728 giorni . 
gli esami tc sono stati acquisiti con tecnica multifasica previa distensione gastro - duodenale con acqua ed assunzione del decubito laterale destro ( 15 min ) , prima e dopo iniezione a bolo ( 4 ml / s ) di mezzo di contrasto ( mdc ) iodato idro - solubile non ionico ( 2 cc / kg ) con parametri tecnici e ritardi di scansione variabili in funzione del tipo di apparecchiatura . 
alla tcms sono state riscontrate 16 lesioni nodulari ( 518 mm ) a livello del pancreas ( 3 testa , 7 corpo e 6 coda ) e 9 ( 37 mm ) a carico della parete duodenale in 9 pazienti . 
our preliminary data indicate that mdct is complementary to eus in the identi cation of pets in men - 1 patients . 22 sono state identi cate prospetticamente ( 18 iper - , 4 ipo - ecogene o cistiche ) e 3 alla luce del dato endoscopico . 
la tcms rappresenta un utile complemento alleco - endoscopia nella identi cazione dei tepd . keywords multiple endocrine neoplasia ( men ) 1 pancreaticoduodenal endocrine tumours multidetector ct ( mdct ) endoscopic ultrasonography ( eus ) parole chiave multiple endocrine neoplasia ( men ) - 1 tumori endocrini duodeno - pancreatici tomogra a computerizzata multistrato ( tcms ) eco - endoscopia ( eus ) introduction introduzione multiple endocrine neoplasia type 1 ( men 1 ) , also known as wermer syndrome , is a rare autosomal dominant disorder with variable penetrance and clinical manifestations and a prevalence of around 220 cases every 100 , 000 individuals [ 1 ]  . 
the genetic alteration is located on the long arm of chromosome 11 where frameshift and nonsense mutations may be found prevalently at the level of hexons 2 , 7 , 9 and 10 [ 2 ]  . 
 patients affected by men 1 are therefore genetically predisposed to a series of functioning and nonfunctioning tumours arising from the parathyroid glands ( 9095% ) , the pituitary gland ( 2065% ) and the endocrine pancreas and duodenum ( 3080% ) [ 3 ]  . 
in most patients , the rst clinical manifestation is hyperparathyroidism ( hpt ) , which may be the result of hyperplasia of one or all four of the parathyroid glands or parathyroid hormone ( pth ) - secreting adenomas , possibly with ectopic location [ 4 ]  . 
although they are less frequent as a possible cause of clinical onset of the disease , pancreaticoduodenal endocrine tumours ( pets ) are nonetheless the leading cause of mortality , with a mean prevalence that has been increasing over the years and is currently around 6070% [ 5 ]  . 
this is quite likely due to the continuous re nement of imaging examinations and in particular the diffusion of endoscopic ultrasound ( eus ) , which is the technique of choice for the identi cation of these often subcentimetric lesions , especially in asymptomatic patients [ 68 ]  . 
although the treatment of choice for pets in men 1 is still debated , there is a general consensus on the importance of an early diagnosis , as malignancy potential is considered to be closely correlated with tumour size [ 9 ]  . 
where available , eus has proven to have a signi cant impact on the clinical management of these patients [ 10 ]  . the progress achieved with multidetector - row computed tomography ( mdct ) systems and in particular with the use of multiphase protocols has nonetheless markedly increased the diagnostic accuracy of ct in pet diagnosis [ 1114 ] , even la neoplasia endocrina multipla tipo 1 ( men - 1 ) , conosciuta anche come sindrome di wermer , una rara malattia ereditaria a trasmissione autosomica dominante , con penetranza ed espressivit clinica variabile ed una prevalenza di circa 220 casi ogni 100.000 individui [ 1 ]  . 
 lalterazione genetica stata localizzata sul braccio lungo del cromosoma 11 ove possibile riscontrare mutazioni frame - shift e nonsense a livello prevalentemente degli esoni 2 , 7 , 9 e 10 [ 2 ]  . 
i pazienti affetti da men - 1 risultano pertanto geneticamente predisposti ad una serie di lesioni neoplastiche , funzionanti e non funzionanti , a carico delle ghiandole paratiroidi ( 90%95% ) , della adenoipo si ( 20%65% ) , del pancreas endocrino e del duodeno ( 30%80% ) [ 3 ]  . 
nella maggior parte dei pazienti la prima manifestazione clinica rappresentata dalliperparatiroidismo ( ipp ) che pu essere sostenuto sia dalla iperplasia di una o di tutte e quattro le paratiroidi che dalla presenza di adenomi secernenti paratormone ( pth ) , talvolta in sede ectopica [ 4 ]  . 
sebbene meno frequenti come possibile causa di esordio clinico della malattia , i tumori endocrini pancreatico - duodenali ( tepd ) ne rappresentano tuttavia la principale causa di mortalit con una prevalenza media che andata aumentando nel corso degli anni e che attualmente si attesta intorno al 60%70% [ 5 ]  . 
ci verosimilmente in relazione con il continuo af namento delle indagini strumentali ed in particolare con la diffusione delleco - endoscopia che rappresenta la metodica di elezione per la identi cazione di tali lesioni che risultano di dimensioni spesso sub - centimetriche , specie nei pazienti asintomatici [ 68 ]  . 
nonostante il trattamento di scelta per i tepd nella men - 1 sia ancora dibattuto , c un generale consenso nellimportanza della diagnosi precoce di tali neoplasie la cui potenzialit maligna sarebbe strettamente correlata alle dimensioni [ 9 ]  . 
to our knowledge , there are no published works on the role of mdct in the detection of hereditary endocrine tumours , which often are nonfunctioning and as such render their clinical identi cation dif cult [ 8 ]  . the aim of our study was to assess the role of mdct performed with a multiphase protocol in pet screening in men - 1 patients and to compare the ndings with eus . materials and methods population between july 2004 and june 2009 , 14 consecutive patients ( eight men , six women ; mean age 4111 years ) with men 1 and belonging to seven different kindreds were referred to our centre . 
two had zollinger - ellison syndrome with gastrinaemia levels of 750 and 1 , 200 pg / ml ( normal value 080 ) , of whom one had already undergone total parathyroidectomy for primary hyperparathyroidism ( php )  . 
of the remaining 12 patients , three had undergone total parathyroidectomy following php , and eight had clinical and laboratory signs of hyperparathyroidism with pth values between 180 and 213 pg / ml ( normal value < 65 )  . study methods the patients underwent a total of 22 mdct examinations , all performed with a 4 - detector - row ( n = 8 ) or 64 - detectorrow ( n = 14 ) system , with a time interval between 9 and 18 months . 
prior to the mdct examination , patients were given 7501 , 000 cc water and asked to lie down in the right lateral decubitus for 15 min to achieve distension of the duodenum and facilitate the identi cation of lesions in the duodenal wall . 
in particular , mdct ( aquilion , toshiba , japan ) scans were acquired before , during and after the injection of 130150 cc ( 2 cc / kg ) of nonionic iodinated contrast material ( 370 mgi / ml , ultravist , bayer schering pharma , berlin germany ) at an injection rate of 4 ml / s , followed by saline solution ( 80 cc ) with an automatic dual - head injector ( stellant injection system , medrad inc , indianola , ia , usa )  . 
a three - phase protocol was performed with acquisitions in the arterial ( 3040 s ) , pancreatic ( 4555 s ) and portal ( 7080 s ) phases , with scan delay varying in relation to the duration of the injection and the mdct system used [ 19 ]  . 
examinations performed with a 4 - row system used a beam collimation of 3 4 mm dica di notevole impatto sulla gestione clinica di tali pazienti [ 10 ]  . 
 i progressi della tecnologia della tomogra a computerizzata multistrato ( tcms ) ed in particolare limpiego di protocolli multi - fasici hanno tuttavia notevolmente incrementato la accuratezza della tomogra a computerizzata ( tc ) nella diagnosi delle neoplasie del pancreas endocrino [ 1114 ] , anche se alcuni studi hanno sollevato problemi di ordine metodologico [ 14 ]  . 
tali lavori hanno tuttavia riguardato le forme sporadiche ed in particolare gli insulinomi e , al meglio della nostra conoscenza , non ci sono dati in letteratura sul ruolo della tcms nella identi cazione dei tumori endocrini eredo - familiari che risultano spesso non funzionanti ed in quanto tali di dif cile inquadramento clinico [ 8 ]  . scopo del presente studio stato quello di veri care il ruolo della tcms eseguita con tecnica multi - fasica nello screening dei tepd nella men - 1 e di confrontarne i risultati con quelli delleco - endoscopia . materiali e metodi popolazione nel periodo compreso tra luglio 2004 e giugno 2009 sono pervenuti alla nostra osservazione 14 pazienti ( 8 maschi , 6 femmine ; et media 4111 anni ) consecutivi affetti da men - 1 ed appartenenti a 7 diversi ceppi familiari . 
due pazienti erano affetti da sindrome di zollingerellison con valori di gastrinemia di 750 e 1200 pg / ml ( valori normali [ vn ] = 080 ) , di cui uno gi sottoposto a para - tiroidectomia totale per iperparatiroidismo primitivo ( ipp )  . 
dei restanti dodici pazienti , tre erano stati anchessi gi sottoposti a para - tiroidectomia totale per ipp e 8 avevano segni clinici e bio - umorali di iperparatiroidismo con valori di pth compresi tra 180 e 213 pg / ml ( vn < 65 )  . 
 metodiche di studio i pazienti sono stati sottoposti ad un totale di 22 esami tc , tutti eseguiti con tecnologia multistrato con 4 ( n = 8 ) o 64 ( n = 14 ) le di detettori ad intervalli temporali compresi tra i 9 ed i 18 mesi . 
 gli esami tc sono stati tutti eseguiti previa somministrazione orale di acqua ( 7501000 cc ) ed assunzione del decubito laterale destro ( 15 min ) per favorire la distensione dellansa duodenale e facilitare il rilievo di eventuali lesioni a carico della parete duodenale . 
examinations performed with a 64 - row system used a beam collimation of 1 32 mm for the arterial and pancreatic phases , both limited to the pancreatic area ( t11l3 ) and acquired with 25 - cm fov , and 2 16 mm for the baseline and portal phase scans , both with a 35 - cm fov extended to the upper abdomen , and all acquired with 0.75 s gantry rotation speed , 120 kev , 0.87 pitch and automatic dose modulation . 
once the endoscope had been introduced into the gastric lumen , any air or liquid present was aspirated , and the sonographic exploration of the pancreatic body and tail was performed with the transducer in contact with the gastric wall . 
 once the pancreatic study was complete , the duodenal wall was assessed using a frequency of 20 mhz to obtain higher resolution . image analysis mdct images were analysed at a dedicated workstation ( merlino enteprise , rem ) , both prospectively and in light of eus ndings . 
eus criteria for diagnosing endocrine lesions of the pancreas and / or duodenum included identifying hypoechoic nodular areas with homogeneous echotexture , oval or round in shape and with wellde ned margins , located in the pancreatic parenchyma or the second or third layer of the duodenal wall , corresponding to the deep portion of the mucosa and submucosa , respectively . 
 more rarely , endocrine tumours may appear as isoechoic lesions bounded by a hypoechoic rim [ 15 ]  . reference standard in ve patients , ne - needle aspiration was performed on colare , la tcms ( aquilion , toshiba , giappone ) stata eseguita prima , durante e dopo iniezione a bolo ( 4 ml / s ) di 130150 cc ( 2 cc / kg ) di mezzo di contrasto ( mdc ) iodato idro - solubile non - ionico ( 370 mg / i / ml , ultravist , bayer schering pharma , berlin , germany ) seguita da soluzione siologica ( 80 cc ) mediante iniettore automatico a doppia siringa ( stellant injection system , medrad inc . , indianola , usa )  . 
stato eseguito un protocollo trifasico con acquisizioni in fase arteriosa ( 3040 s ) , pancreatica ( 4555 s ) e portale ( 7080 s ) , con ritardi di scansione variabili in funzione della durata delliniezione e del tipo di apparecchiatura [ 19 ]  . 
negli esami eseguiti con tc multistrato ( 4 ) stata impiegata una collimazione del fascio di 34 mm per le fasi arteriosa e pancreatica , entrambe limitate alla loggia pancreatica ( d11 - l3 ) con campo di vista ( fov ) di 25 cm , e 54 mm per la fasi pre - contrastogra ca e portale , entrambe con fov di 35 cm ed estese allintero addome superiore , con correnti al tubo di 350 e 250 mas , rispettivamente , 120 kev , tempo di rotazione di 0 , 5 s , beam pitch 0 , 75 . 
con la tc multistrato con 64 le di detettori la collimazione del fascio impiegata stata di 132 mm per le fasi arteriosa e pancreatica , entrambe limitate alla loggia pancreatica ( d11 - l3 ) ed acquisite con fov di 25 cm e di 216 mm per le fasi pre - contrastogra ca e portale , entrambe estese allintero addome superiore con fov di 35 cm , tutte acquisite con tempo di rotazione di 0 , 75 sec , 120 kev , beam pitch 0 , 87 e modulazione automatica della dose . 
una volta introdotto lo strumento nel lume gastrico si provveduto ad aspirare laria ed il liquido eventualmente presente e si condotta lesplorazione ultrasonogra ca del corpo e della coda del pancreas ponendo il trasduttore a contatto con la parete gastrica . 
per il confronto con i dati delleco - endoscopia sono stati alla ne selezionati 14 esami tc di cui 7 eseguiti con tcms aquilion 4 e 7 con tcms aquilion 64 . 
sono state valutate le sole radiol med ( 2011 ) 116 : 595606 ve lesions ( one duodenal , four pancreatic ) with a 22 - gauge needle , the results of which con rmed their neuroendocrine nature . 
in the remaining nine patients , the eus study was considered the reference standard . results adequate distension of the duodenum was obtained in 11 of the 14 patients examined ( 78% )  . 
in that location , as many as nine nodules were identi ed , of which ve were in the same patient , all hypervascular and between 3 and 7 mnodular formations with similar attenuation but larger in size ( 518 mm ) were also identi ed in the pancreatic parenchyma , i.e. 
i criteri eco - endoscopici per la diagnosi di lesioni endocrine del pancreas e / o del duodeno sono rappresentati dallidenti cazione di aree nodulari ipoecogene ad eco - tessitura omogenea , di morfologia ovalare o rotondeggiante ed a margini netti , situate nel contesto del parenchima pancreatico o a livello del ii o iii strato della parete duodenale , corrispondenti rispettivamente alla porzione profonda della mucosa ed alla sotto - mucosa . 
pi raramente i tumori endocrini possono apparire come lesioni isoecogene delimitate da orletto ipoecogeno [ 15 ]  . gold standard in cinque pazienti altrettante lesioni , duodenali ( 1 ) e pancreatiche ( 4 ) , sono state sottoposte ad ago - aspirazione ( fna ) con ago sottile ( 22 g ) che ne ha confermato la natura neuro - endocrina . 
in particolare , 16 formazioni nodulari ( 518 mm ) sono table 1 multidetector - row computed tomography ( mdct ) in patients with multiple endocrine neoplasia type 1 ( men 1 )  . 
numero , dimensioni e topogra a delle lesioni nodulari identi cate prospetticamente e retrospettivamente in 9 pazienti lesioni nodulari ( n = 25 ; 318 mm ) duodeno ( 37 mm ) testa ( 818 mm ) corpo ( 514 mm ) coda ( 610 mm ) 600 radiol med ( 2011 ) 116 : 595606 fig . 
1a , b four - row multidetector - row computed tomography ( mdct ) and endoscopic ultrasound ( eus ) in multiple endocrine neoplasia type 1 ( men 1 )  . 
alla tc ( a ) , acquisita in fase arteriosa , focale bozzatura del margine ghiandolare anteriore si apprezza a carico del corpo pancreatico ( testa di freccia ) in assenza di alterazioni densitometriche . 
2a , b four - row multidetector - row computed tomography ( mdct ) and endoscopic ultrasound ( eus ) in multiple endocrine neoplasia type 1 ( men 1 )  . 
alla tc ( a ) acquisita in fase arteriosa piccola area nodulare di anomala impregnazione ( testa di freccia ) si apprezza a carico della parete della ii porzione duodenale . 
leco - endoscopia ( b ) documenta a tale livello piccola ( 5 , 2 mm ) formazione nodulare sotto - mucosa ipo - ecogena . detectable in the arterial phase , as the quantitative analysis for the three lesions > 1 cm shows , with absolute attenuation values of 1904 hu and differential values with respect to the surrounding parenchyma of 5912 hu for the arterial phase and 219 hu for the pancreatic phase . 
four ( 16% ) pancreatic lesions had a hypoattenuating ( n = 1 ) or frankly state riscontrate a livello del pancreas , di cui 3 alla testa , 7 al corpo e 6 alla coda , e 9 ( 37 mm ) a carico dellansa duodenale , di cui 1 al bulbo , 4 al ginocchio inferiore , 2 al ginocchio superiore , 1 alla parete mediale della seconda porzione , 1 alla terza porzione duodenale ( tabella 1 )  . 
arterial - phase mdct ( a ) shows a small ( 5 mm ) nodular area of abnormal enhancement on the anterior margin of the pancreatic body , which is still evident but less conspicuous in the pancreatic phase ( b )  . 
in a ben evidente una piccola ( 5 mm ) formazione nodulare ipervascolarizzata a livello del corpo pancreatico che risulta ancora apprezzabile , ma meno evidente , in fase pancreatica ( b )  . 
arterial - phase mdct ( a ) shows a nodular ( 9 mm ) area of abnormal enhancement on the anterior margin of the pancreatic tail ( arrowhead ) , which becomes isoattenuating to the surrounding parenchyma and as such is no longer appreciable in the pancreatic phase ( b )  . 
in a ben evidente formazione nodulare ( 9 mm ) ipervascolarizzata a carico del margine anteriore della coda ghiandolare ( testa di freccia ) che non risulta pi apprezzabile in fase pancreatica in quanto isodensa al circostante parenchima ( b )  . 
la lesione non stata evidenziata dalla eco - endoscopia . cystic ( n = 3 ) appearance and as such were better appreciable in the pancreatic phase ( table 2 )  . the eus study , instead , identi ed 32 nodular pets ( 218 mm ) in 11 patients . 
dei 25 tumori pancreatico - duodenali , 22 sono stati identicati prospetticamente e 3 alla sola luce del dato endoscopico , di cui due isodensi al circostante parenchima ed uno ipodenso . 
in particolare , una formazione nodulare di 12 mm a carico del corpo pancreatico stata identi cata solo retrospettivamente grazie alla focale bozzatura da 602 radiol med ( 2011 ) 116 : 595606 table 2 multidetector - row computed tomography ( mdct ) in patients with multiple endocrine neoplasia type 1 ( men 1 )  . 
number , location and attenuation characteristics of the nodular lesions identi ed prospectively in nine patients nodular lesions ( n = 22 ; 318 mm ) duodenum head body tail tabella 2 tcms nei pazienti con men - 1 . 
numero , dimensioni , sede ed aspetto delle lesioni nodulari identi cate dalla eco - endoscopia in 11 pazienti lesioni nodulari ( n = 32 ; 218 mm ) duodeno ( 212 mm ) testa ( 518 mm ) corpo ( 813 mm ) coda ( 8 mm ) table 3 endoscopic ultrasound ( eus ) in patients with multiple endocrine neoplasia type 1 ( men 1 )  . 
number , size , location and appearance of the nodular lesions identi ed by eus in 11 patients nodular lesions ( n = 32 ; 218 mm ) duodenum ( 212 mm ) head ( 518 mm ) body ( 813 mm ) tail ( 8 mm ) located in the pancreas and 13 in the duodenal wall ; three appeared isoechoic ( 10% ) , of which two were located in the duodenal wall and one in the pancreas ( table 3 )  . 
pets , on the other hand , arise in 6070% of patients with men 1 [ 5 ] , and in 50% of cases , they constitute the clinical onset of the disease [ 16 ]  . 
 le suddette formazioni nodulari sono risultate meglio apprezzabili nella fase arteriosa di studio come supportato dallanalisi quantitativa eseguita per le sole tre formazioni di dimensioni > 1 cm che ha evidenziato valori densitometrici assoluti di 1904 uh e valori differenziali rispetto al circostante parenchima pancreatico di 5912 uh per la fase arteriosa e 219 uh per la fase radiol med ( 2011 ) 116 : 595606 fig . 
5a - c four - row multidetector - row computed tomography ( mdct ) ( a , b ) and endoscopic ultrasound ( eus ) ( c ) in multiple endocrine neoplasia type 1 ( men 1 )  . 
quattro ( 16% ) lesioni pancreatiche risultavano di aspetto ipodenso ( 1 ) o francamente cistico ( 3 ) e come tali meglio apprezzabili nella fase pancreatica ( tabella 2 )  . allesame eco - endoscopico sono state evidenziate invece 32 lesioni nodulari pancreatico - duodenali ( 218 mm ) in 11 pazienti ( 78 , 5% )  . 
in particolare , per i gastrinomi stato dimostrato che lincidenza di metastasi epatiche direttamente correlata alle dimensioni della lesione e risulta signi cativamente pi elevata per lesioni di dimensioni > 2 cm [ 5 ]  . assume pertanto particolare signi cato il monitoraggio di tali lesioni per la cui identi cazione la eco - endoscopia rappresenta sicuramente la metodica pi accurata con una sensibilit del 93%95% [ 10 , 12 ] che ben si correla con i risultati ottenibili con la palpazione bi - manuale del pancreas e risulta solo di poco inferiore a quelli riportati dallecogra a intra - operatoria ( 96 , 4% ) [ 12 ]  . 
 la diffusione della tecnologia multistrato in tc ha tuttavia considerevolmente incrementato la accuratezza della metodica nella diagnosi delle neoplasie endocrine del pancreas grazie alla possibilit di eseguire studi multi604 radiol med ( 2011 ) 116 : 595606 associated with the disease . 
in particular , it has been demonstrated for gastrinomas that the incidence of liver metastases is directly correlated with the lesion size and is signi cantly higher for lesions > 2 cm [ 5 ]  . monitoring these lesions becomes particularly important , and eus is undoubtedly the most accurate technique for their identi cation , with a sensitivity of 9395% [ 10 , 12 ] , which correlates well with the results obtained with bimanual palpation of the pancreas and is only a little lower than intraoperative us ( 96.4% ) [ 12 ]  . 
 the increasing diffusion of mdct systems has nonetheless considerably increased the accuracy of this technique in diagnosing endocrine tumours of the pancreas , thanks to the possibility of performing multiphase studies of the upper abdomen with collimations in the order of 13 mm [ 1114 ]  . 
in our experience , however , mdct proved to be complementary to eus in that it identi ed ve nodular formations of the pancreatic tail that were not detected by eus ( tables 1 , 2 )  . 
this small number does not allow solid conclusions to be drawn regarding the role of mdct , but these observations are supported in the literature , where the lower sensitivity of eus in the exploration of the pancreatic tail when using a radial transducer has been highlighted [ 17 ]  . 
the quantitative analysis performed on the three lesions > 1 cm also displayed higher attenuation differences compared with the surrounding parenchyma in the arterial phase rather than in the portal phase . 
this is in disagreement with the most recent ndings in the literature , according to which pets are said to be better appreciated in the pancreatic phase [ 14 ]  . 
in particular , in our study , the bolus - tracking technique was not used ; rather , a variable scan delay was implemented in relation to the injection rate and the mdct system used , considering a mean transit time of 10 s [ 19 ]  . 
our ndings are also supported by the experience of other authors , who claimed the importance of the arterial phase in the identi cation of endocrine tumours , although sporadic [ 11 , 12 ]  . 
nella nostra esperienza la tcms si tuttavia rivelata complementare alleco - endoscopia avendo identi cato cinque formazioni nodulari a carico della coda pancreatica non rilevate dallesame eco - endoscopico ( tabelle 1 e 2 )  . 
lesiguit di tali numeri non consente di trarre considerazioni conclusive sul ruolo della tcms ma tali osservazioni trovano un riscontro nella letteratura nella quale sottolineata la minore sensibilit della eco - endoscopia nella esplorazione della coda pancreatica quando si utilizza una sonda radiale [ 17 ]  . 
anche lanalisi quantitativa eseguita per le sole tre lesioni di dimensioni sovra - centimetriche ha rivelato valori densitometrici differenziali con il circostante parenchima pancreatico maggiori nella fase arteriosa che in quella portale . 
in particolare , nel presente studio non si fatto ricorso al bolus tracking ma si utilizzato un ritardo di scansione variabile in funzione della durata delliniezione e del tipo di apparecchiatura considerando un tempo medio di transito di 10 s [ 19 ]  . 
nonostante un tale approccio empirico non possa ritenersi rigoroso da un punto di vista metodologico esso trova ampio supporto in letteratura [ 20 ] ed appare giusti cato dalla et media dei nostri pazienti ( 40 , 611 anni )  . 
i nostri dati sono inoltre supportati dallesperienza di altri autori che sostengono limportanza della fase arteriosa nelle identi cazione dei tumori endocrini anche se sporadici [ 11 , 12 ]  . 
 [ 11 ] il 94% ( 18 / 19 ) degli insulinomi identi cati dalla tcms risultato essere ipervascolarizzato e come tale meglio apprezzabile nella fase arteriosa [ 11 ]  . 
per le loro caratteristiche densitometriche tali lesioni sono risulradiol med ( 2011 ) 116 : 595606 al . , 94% ( 18 / 19 ) of insulinomas identi ed by mdct were hypervascular and as such were better appreciated in the arterial phase [ 11 ]  . 
in our study , the combined use of mdct and eus made it possible to identify a total of 37 pets in 11 patients with an incidence of 3.4 lesions per patient and a prevalence of 78.5% , which is in agreement with the most recent data in the literature [ 6 ]  . 
with the exception of the ve lesions subjected to ne - needle aspiration , we do not know which of the lesions identi ed by one or both techniques are in fact endocrine tumours . 
the combined use of the two techniques permitted identi cation of 100% ( 18 / 18 ) of pancreatic insulinomas , all of which were subjected to surgical excision [ 12 ]  . 
this is , however , largely justi ed by the subcentimetric and paracentimetric size of the lesions identi ed , for which the current guidelines recommend only clinical and imaging follow - up [ 9 ]  . 
in fact , no bene t is expected from the surgical treatment of lesions of those dimensions in patients with men 1 , and there is a general consensus to reserve the surgical option only for lesions > 2 cm , for which a higher incidence of liver metastases is reported [ 22 ]  . in conclusion , the results of our study indicate a complementary role of multiphase mdct and eus in the identi cation of hereditary endocrine tumours . tate tutte meglio apprezzabili nella fase pancreatica . 
nel presente studio limpiego combinato della tcms e della eco - endoscopia ha pertanto consentito di identi care un totale di 37 lesioni pancreatico - duodenali in 11 pazienti con una incidenza di circa 3 , 4 lesioni / paziente ed una prevalenza del 78 , 5% che in accordo con i pi recenti dati della letteratura [ 6 ]  . 
 [ 12 ] limpiego combinato delle due metodiche ha consentito di identi care il 100% ( 18 / 18 ) di insulinomi pancreatici , tutti sottoposti ad escissione chirurgica [ 12 ]  . 
nel presente studio non stato possibile confrontarsi con i riscontri anatomo - patologici e ci ne rappresenta il limite principale , in gran parte giusti cato dalle dimensioni sube para - centimetriche delle lesioni identi cate , per le quali le attuali linee guida prevedono il solo follow - up clinico - strumentale [ 9 ]  . 
 non infatti atteso alcun bene cio nel trattamento chirurgico di lesioni di tali dimensioni nei pazienti con men - 1 e c un generale consenso nel riservare lopzione chirurgica solo alle lesioni di dimensioni > 2 cm per le quali sole riportata una maggiore incidenza di metastasi epatiche [ 22 ]  . in conclusione , i risultati del presente studio indicano un ruolo complementare della tcms multifasica e della eco - endoscopia nella identi cazione dei tumori endocrini eredo - familiari . 
del maschio1 1radiology department , vita - salute university , san raffaele scienti c institute , via olgettina 60 , 20132 milan , italy 2nuclear medicine department , vita - salute university , san raffaele scienti c institute , milan , italy 3surgical department , vita - salute university , san raffaele scienti c institute , milan , italy 4pathology department , vita - salute university , san raffaele scienti c institute , milan , italy correspondence to : e . 
allinterno della lesione sono stati iniettati macro - aggregati di albumina umana marcata con tecnezio99 ; nel caso di guida ecogra ca ( 221 / 288 soggetti ) , linoculo ha prodotto iperecogenicit in corrispondenza della lesione ; nel caso di guida mammogra ca ( 67 / 288 soggetti ) , dopo il radiotracciante stato inoculato mezzo di contrasto iodato per il successivo controllo mammogra co . 
la guida radiologica nella roll ha garantito lesito della localizzazione e rimozione di lesioni mammarie singole non palpabili nella maggioranza dei casi . radiol med ( 2011 ) 116 : 564574 keywords breast lesion radioguided localisation mammography ultrasonography parole chiave lesione mammaria localizzazione radioguidata mammogra a ecogra a introduction introduzione a variety of preoperative localisation techniques for nonpalpable breast lesions has been described in the literature : hypodermic needles , wires ( the most widely accepted technique ) , carbon solution , methylene blue dye [ 110 ]  . 
radioguided occult lesion localisation ( roll ) , introduced in 1998 , involves the inoculation of macroaggregates of human serum albumin labelled with radioactive technetium99 ( 99mtc ) directly into the site of a nonpalpable breast lesion , with mammography ( mx ) or ultrasound ( us ) guidance . 
after radiotracer injection , a gamma - detecting probe ( gdp ) was used to locate the lesion during surgery , allowing the surgeon to evaluate its skin projection and decide the best approach with an acceptable cosmetic outcome [ 15 , 16 ]  . 
the same group that described roll for the rst time compared this technique with wire localisation and concluded that roll was rapid , easy and accurate , with reduced excision volume and better lesion centring [ 17 ] , and also safe in terms of radiation exposure [ 18 ]  . following this experience , other groups tested roll alone or in combination with the sentinel node ( sn ) procedure in different clinical settings [ 1922 ]  . 
prospective randomised trials compared roll with wire - guided lumpectomy and concluded that roll was as effective as wire for localising and excising breast lesions , was simple , reduced localisation time and pathologically positive margins and gave better cosmetic results [ 2326 ]  . 
 the aim of this prospective study was to evaluate the methods , technical aspects and impact of patient - tailored preoperative radiological guidance in roll in a large series of women with single , nonpalpable breast lesions . 
 materials and methods study population we evaluated 288 women ( mean age 57.5 years ; range 3288 years ) with single , nonpalpable breast lesions who were sono state descritte in letteratura varie tecniche di localizzazione preoperatoria di lesioni mammarie non palpabili : ago ipodermico , lo guida ( la tecnica pi largamente accettata ) , soluzione di carbone , blu di metilene [ 110 ]  . 
la radioguided occult lesion localization ( roll ) , introdotta nel 1998 , prevede linoculo di macro - aggregati di albumina umana marcata con tecnezio99 radioattivo ( 99mtc ) direttamente nella sede della lesione mammaria non palpabile , con guida mammogra ca o ecogra ca . 
dopo liniezione del radiotracciante , viene utilizzata una sonda per la rilevazione dei raggi gamma ( gdp ) al ne di localizzare la lesione sul tavolo operatorio , permettendo cos al chirurgo di valutarne la proiezione cutanea e di decidere il miglior approccio operatorio , con un buon risultato cosmetico [ 15 , 16 ]  . 
lo stesso gruppo che ha descritto la roll per la prima volta ha poi paragonato questa tecnica con quella del lo guida ed ha concluso che la roll era rapida , facile ed accurata , con ridotto volume di tessuto escisso e migliore centratura della lesione [ 17 ] , ed era inoltre sicura in termini di radioesposizione [ 18 ]  . a seguito di questa esperienza , altri gruppi hanno valutato la roll in differenti situazioni cliniche , anche combinata con la procedura del linfonodo sentinella ( sn ) [ 1922 ]  . 
studi prospettici randomizzati hanno paragonato la roll alla nodulectomia con lo guida ed hanno concluso che la roll era ef cace quanto il lo guida per la localizzazione ed escissione di lesioni mammarie , riduceva il tempo per la localizzazione e la positivit dei margini , e dava migliori risultati cosmetici [ 2326 ]  . 
la maggioranza degli articoli internazionali ha posto lattenzione sulla valutazione della roll dal punto di vista chirurgico , con particolare attenzione alla durata dellintervento , alla scelta dellaccesso , al risultato cosmetico . 
 relativamente poca attenzione stata rivolta al ruolo della guida radiologica con mammogra a ( mx ) e ecogra a ( us ) nella roll . lo scopo di questo studio prospettico stato quello di valutare i metodi , gli aspetti tecnici e limportanza della guida radiologica nella roll , personalizzata per ogni paziente , su ampia casistica di donne con lesione mammaria singola non palpabile . 
when the lesion was detected exclusively or also by us ( 221 / 288 lesions , 76.7% ) , us - guided ne - needle aspiration cytology ( fnac ) or core biopsy ( cb ) were performed . 
 when the lesion was detected by mx only ( 67 / 288 lesions , 23.3% ) and appeared as a group of suspicious microcalcications , it underwent mx - guided stereotactic vacuumassisted biopsy ( vab )  . 
se la lesione era stata evidenziata esclusivamente o anche con us ( 221 / 288 lesioni , 76 , 7% ) , erano state eseguite citologia con ago sottile ( fnac ) o core biopsy ( cb ) sotto guida us . 
se la lesione era stata evidenziata esclusivamente con mx ( 67 / 288 lesioni , 23 , 3% ) e aveva laspetto di un gruppo di microcalci cazioni , esse erano state sottoposte a biopsia vacuum - assisted ( vab ) sotto guida mx . 
i criteri di esclusione dalla roll sono stati evidenza di malattia mammaria multicentrica e stato di gravidanza . radiocomposto e tecniche di medicina nucleare il radiocomposto iniettato consistito in 0 , 10 , 2 cc di macro - aggregati di albumina umana marcati con 3 , 77 , 4 mega - bequerel ( mbq ) di 99mtc . 
questa quantit corrispondeva ad una dose di 100200 micro - curie ( ci ) ed era stata calcolata sulla base della stima del tempo medio intercorrente fra linoculo del radiocomposto e la procedura chirurgica . 
la dimensione dei macro - aggregati variata da 10 a 150 micron ( m ) e , a causa della loro dimensione , la maggioranza delle particelle rimasta allinterno della lesione e non stata diffusibile come le particelle usate per la procedura sn , che ha potuto essere eseguita insieme alla roll senza interferenza [ 21 , 2729 ]  . 
in queste pazienti , sono state iniettate in sede intradermica , nellarea peritumorale , particelle nanocolloidi di albumina umana marcate con 14 , 8 mbq di 99mtc ( dose 400 ci )  . 
la dimensione dei nanocolloidi stata minore di 80 m e ci , come gi menzionato , ha permesso che esse si diffondessero nel sistema linfatico e raggiungessero il sn ascellare . 
dopo liniezione del radiotracciante per la roll , la paziente stata sottoposta a scintigra a biplanare ( valutata da c.c. , con 8 anni di esperienza ) per veri care la corretta localizzazione del 99mtc . 
in these cases , craniocaudal and mediolateral mammographic views were acquired to localise the lesion properly ( senographe essential and senographe dmr + , ge medical systems , cedex , france )  . 
the radiologist decided the best approach to the lesion ( frontal , lateral or medial ) and asked the patient to sit on a chair with arms along the body . 
the position of the 22 g needle , which should be inside the lesion or within 1 cm , was then checked with other orthogonal mammograms ; this was done more than once if the tip of the needle was not in the correct position , which can happen , especially in the case of small clusters of microcalci cations and in large breasts . 
 finally , the nuclear physician inserted on the needle the rst insulin syringe lled with 0.10.2 cc of radioactive tracer , and the radiologist inserted a second syringe with 1 cc of iodinated contrast medium ( iopamiro , iopamidol , bracco , italy )  . 
the cost of the roll procedure , including the biplanar scintigraphy and excluding the surgical intervention , was 250300 euro on average . surgical procedure in the operating room ( or ) , a gdp ( 15 lvr , pol.hi.tech , carsoli , italy ) was held by the surgeon to guide lesion removal . 
the pathological specimen was sent to the radiology department where the presence of the suspicious lesion was checked with us or mx , depending on the radiological guidance technique used previously . 
in questi casi , con la paziente supina e con le braccia estese sopra il capo , il radiologo ha localizzato la lesione ed ha posizionato un ago ipodermico 22 gauge ( g ) direttamente allinterno della lesione o presso di essa ( quando la lesione era troppo dura per iniettare liquido ) sotto guida us real - time eseguita con una sonda lineare da 12 mhz ( technos mp , esaote , genova , italia )  . 
nelle 67 su 288 pazienti ( 23 , 3% ) che erano state sottoposte a biopsia stereotassica mx - guidata preoperatoria , la procedura di localizzazione stata eseguita con guida mx . 
in questi casi , sono stati acquisiti mammogrammi nelle proiezioni cranio - caudale e medio - laterale , per localizzare correttamente la lesione ( senographe essential e senographe dmr + , ge medical systems , cedex , francia )  . 
il radiologo , dopo aver scelto il miglior approccio alla lesione ( frontale , laterale o mediale ) , ha chiesto alla paziente di sedere su una sedia con le braccia lungo il corpo . 
la posizione dellago 22 g , che doveva essere allinterno della lesione o entro 1 cm da essa , stata poi veri cata con altri mammogrammi ortogonali , anche pi di una volta nel caso in cui la punta dellago non fosse nella corretta posizione , e questo si pu veri care in particolare per piccoli gruppi di microcalci cazioni o in mammelle voluminose . 
in ne , il medico nucleare ha inserito sullago la prima siringa da insulina contenente 0 , 10 , 2 cc del tracciante radioattivo , ed il radiologo ha inserito poi una seconda siringa con 1 cc di mezzo di contrasto iodato ( iopamiro , iopamidolo , bracco , italia )  . 
il costo della roll , includendo la scintigra a biplanare ed escludendo lintervento chirurgico , stato in media di circa 250300 euro . procedura chirurgica in sala operatoria ( or ) , il chirurgo ha utilizzato una gdp ( 15 lvr , pol.hi.tech , carsoli , italia ) per guidare la rimozione della lesione . 
il pezzo operatorio stato inviato al dipartimento di radiologia , dove la presenza della lesione sospetta stata veri cata mediante us o mx , a seconda della tecnica di guida radiologica precedentemente adottata . 
il risultato della valutazione radiologica stato comunicato al chirurgo in or , il quale poteva decidere se lescissione era adeguata o doveva essere allargata , a seconda che i margini , orientati con li chirurgici di seta e clips metalliche , fossero radiologicamente liberi ( lesione ad almeno 1 cm da tutti i margini del pezzo operatorio )  . 
 procedura istologica tutti i 288 pezzi operatori sono stati sottoposti a valutazione macroscopica della totalit dei margini , i quali sono stati considerati liberi da malattia se la lesione era almeno ad 1 cm da essi . 
1a - c ultrasound guidance for a 12 - mm nonpalpable lesion ( cytology : c3 ) in the upper outer quadrant of the right breast of a 44 - year - old patient . 
1a - c guida ecogra ca per una lesione non palpabile di 12 mm ( citologia : c3 ) al quadrante supero - esterno della mammella destra di una paziente di 44 anni . 
c valutazione del pezzo operatorio dopo lescissione : la lesione bene visibile ( vedi freccia )  . tutte le procedure sono state ben tollerate e non si sono veri cati eventi avversi importanti . 
in 1 caso la radioattivit del 99mtc scomparsa poich la procedura chirurgica non stata eseguita in tempo ( entro 24 ore ) per problemi tecnici ( sciopero del personale della or )  . 
2a - e mammographic guidance for a cluster of microcalci cations ( histology : ductal carcinoma in situ ) in the upper outer quadrant of the left breast ( para - areolar ) of a 67 - year - old patient . 
2a - e guida mammogra ca per un cluster di microcalci cazioni ( istologia : carcinoma duttale in situ ) nel quadrante supero - esterno , in parareolare , della mammella sinistra di una paziente di 67 anni . 
e radiogramma del pezzo operatorio che mostra che le microcalci cazioni sono contenute nella porzione escissa di mammella ( vedi freccia )  . of the radiological evaluation of the specimen was communicated to the surgeon in the or , who could decide whether the excision was adequate or should be enlarged , depending on the radiological clearance of margins ( lesion 1 cm away from all the specimen margins ) , which were oriented with surgical silk threads and metallic clips . 
in questo sottogruppo , 6 soggetti ( 2 , 6% ) sono stati sottoposti ad una seconda procedura chirurgica poich i margini del tessuto escisso non erano liberi dopo il primo intervento . 
la localizzazione delle lesioni con roll stata corretta in tutti questi 6 casi . in totale , lescissione di sn stata eseguita in 205 diately analysed in all 198 cases in order to decide whether axillary dissection had to be performed in the same surgical session . 570 results all procedures were well tolerated , and no major adverse event occurred . 
in one case , the 99mtc radioactivity declined because the surgical procedure could not be performed in time ( within 24 h ) due to technical problems ( strike of the or personnel )  . 
the surgeons observed no interference between the radioactive signals from the breast lesion and from the sn . discussion breast cancer screening has increased the number of detected nonpalpable breast lesions and , once a suspicious lesion is detected at imaging , a cytological or histological diagnosis is needed . 
our approach to nonpalpable breast lesions is characterised by a preoperative diagnosis obtained either with us - guided fnac or core biopsy or with mx - guided stereotactic vacuum - assisted biopsy . 
it has been demonstrated that even when the breast carcinoma diagnosis is known before surgery , preoperative wire localisation can be inaccurate and lead to reintervention in up to 20% of cases [ 30 , 31 ]  . 
moreover , wire - guided localisation has some well - known drawbacks that affect the entire course of the procedure , such as accidental displacement and need for repositioning , pneumothorax and wire migration into the pleural cavity . 
or availability is fundamental because the radiol med ( 2011 ) 116 : 564574 soggetti su 288 ( 71 , 2% ) , sia nella stessa sessione chirurgica dellescissione della lesione ( 198 casi , 96 , 6% ) , insieme alla roll , che durante una seconda procedura chirurgica ( 7 casi , 3 , 4% )  . 
i chirurghi non hanno osservato alcuna interferenza fra i segnali radioattivi derivanti dalla lesione mammaria e dal sn . discussione i programmi di screening hanno aumentato il numero di lesioni mammarie non palpabili che vengono individuate . 
 stato dimostrato che anche quando la diagnosi di carcinoma mammario nota prima della chirurgia , la localizzazione preoperatoria con lo guida pu essere poco accurata e condurre al re - intervento no al 20% dei casi circa [ 30 , 31 ]  . 
inoltre , la localizzazione con lo guida ha alcuni ben noti problemi che riguardano lintero svolgersi della procedura , come la dislocazione accidentale e la necessit di riposizionamento , lo pneumotorace e la migrazione del lo nella cavit pleurica . 
in or , il lo pu interferire con lincisione chirurgica ed spesso cos sottile che non pu essere seguito nel suo corso dalle mani del chirurgo , o pu essere reciso dal bisturi . 
 in ne , abbiamo gi citato il disagio della paziente , ma si possono anche veri care eventi avversi come reazioni vaso - vagali [ 14 , 15 , 3235 ]  . 
tuttavia , le principali limitazioni di questa tecnica sono la dif coltosa localizzazione delle lesioni in mammelle grandi e dense , la formazione di granulomi se il carbone non viene completamente rimosso durante lintervento chirurgico , la distorsione della lesione e la dif colt della preparazione del pezzo operatorio per la valutazione istologica [ 10 , 36 ]  . 
tuttavia , i reports in merito sono ancora pochi , probabilmente per la limitata radiol med ( 2011 ) 116 : 564574 patient cannot keep the wire in the breast for a long time , as it is uncomfortable and can be accidentally displaced . 
 in the or , the wire can interfere with the surgical incision and is often so thin that its course cannot be followed by the surgeons hands , or it can be cut by the scalpel . 
 the use of vital dyes , such as methylene blue , is anecdotal in the literature and unsatisfactory due to fast dispersion into tissues [ 8 , 10 ]  . 
however , the main limitations of this technique are dif cult lesion localisation in large and dense breasts , granuloma formation if charcoal is not completely removed during surgery , lesion distortion and dif culty in specimen preparation for histological evaluation [ 10 , 36 ]  . 
moreover , seeds can accidentally be lost in the operating room because of their small size [ 13 , 14 ]  . the roll procedure with 99mtc proved to be effective , safe and easy to use . 
in our patients , we used us guidance for the radiotracer injection whenever possible because us allowed us to follow the hypodermic needle in real time throughout the procedure , increasing our con dence in lesion centring . 
 when the lesion was too hard , it was not possible to inject the tracer into the core , so we injected beside it . it is important that the radiologist maintains adequate pressure on the us probe during the injection . 
if not , there is a possibility that the hypodermic needle will come out of the lesion because the breast tissues are no longer compressed , and the tracer is thus injected at a distance from the lesion . 
 this can represent a problem , especially in large breasts , and warrants a new localisation procedure . mx guidance was performed freehand because the stereotactic technique implies very high breast compression , which represents an obstacle during radiotracer injection . 
inoltre , i semini possono accidentalmente essere perduti in or a causa delle loro esigue dimensioni [ 13 , 14 ]  . la procedura di roll con 99mtc si dimostrata ef cace , sicura e facile da utilizzare . 
nelle nostre pazienti stata utilizzata la guida us per liniezione del radiotracciante in tutti i casi in cui stato possibile , poich lus permette di seguire lago ipodermico in tempo reale lungo tutta la procedura , aumentando la con denza riguardo alla centratura della lesione . 
quando la lesione era troppo dura , non stato possibile iniettare il tracciante allinterno della lesione , ed abbiamo iniettato a lato della stessa . importante che il radiologo mantenga adeguata pressione sulla mammella con la sonda us durante liniezione . 
 se ci non accade , esiste la possibilit che lago ipodermico esca dalla lesione perch i tessuti mammari non sono pi compressi ed il tracciante venga iniettato lontano dalla lesione stessa . 
questo pu rappresentare un problema soprattutto nelle mammelle voluminose , e richiede una nuova procedura di localizzazione . la guida mx stata eseguita a mano libera poich la tecnica stereotassica prevede una compressione della mammella assai intensa , che rappresenta un ostacolo durante liniezione del radiotracciante . 
nella nostra esperienza , la procedura a mano libera stata pi facile e sicura . solamente 6 lesioni su 288 ( 2 , 1% ) sono state centrate in modo non corretto . 
lerrore del radiologo stato quello di diminuire la compressione della mammella prima che liniezione del radiotracciante si concludesse , e ci ha causato dislocazione dellago e iniezione del radiotracciante nella sede non corretta . 
in questo caso , il chirurgo non stato in grado di percepire al tatto la lesione e la paziente stata sottoposta ad una ulteriore iniezione del 572 radiol med ( 2011 ) 116 : 564574 the 2 incorrect procedures occurred with mx guidance at the beginning of our experience . 
in this case , the surgeon was not able to feel the lesion , and the patient underwent a further injection of radiotracer a week later , for a second intervention . 
at histology , the specimens turned out to contain diffuse cystic disease , leading us to believe that the radiotracer was dispersed in the acinarlobular syste the remaining case of unsuccessful roll procedure , as mentioned , was due to unavailability of the or because of a personnel strike and subsequent fading of radioactivity at the lesion site . 
roll could be thus considered an almost harmless procedure due to the small diameter of the hypodermic needle ( 22 g ) , so that even when adjustments in needle position were needed , they bore no noticeable consequence . 
moreover , local anaesthesia was unnecessary . it is important to emphasise that when the surgical procedure could not be performed at the scheduled time , radioactivity at the lesion site decayed , with no risks for the patient . 
the surgeons observed no interference between radioactive signals from the breast lesion and from the sn , demonstrating that the two techniques can be used at the same time , with the same gdp , as already stated in the literature [ 21 , 2729 ]  . the main limitations of our study were that we did not perform a side - by - side comparison with conventional wire placement methods ; moreover , the technique requires the presence of a nuclear medicine department in the hospital to ensure correct preparation and handling of the radiotracer . 
 this can be a limitation , especially in small hospitals . in conclusion , radiological guidance in roll guaranteed the reliability , ef cacy and accuracy of the entire procedure of localisation and removal of single nonpalpable breast lesions and ensured the nal outcome in the majority of cases . 
il restante caso di procedura roll senza successo , come gi menzionato , stato dovuto allindisponibilit della or a causa di uno sciopero del personale con conseguente declino della radioattivit nella sede di lesione . 
la roll pu quindi essere considerata una procedura pressoch innocua grazie al piccolo calibro dellago ipodermico ( 22 g ) , cosicch anche quando sono stati necessari aggiustamenti della posizione dellago , essi non hanno causato alcuna signi cativa conseguenza . 
inoltre , non stata necessaria lanestesia locale . importante sottolineare che , quando la procedura chirurgica non stata eseguita in tempo , la radioattivit in sede di lesione declinata e non ci sono stati rischi per la paziente , mentre nel caso di guida con lo , esso avrebbe dovuto essere rimosso , causando ancor pi disagio . 
i chirurghi non hanno osservato alcuna interferenza fra i segnali radioattivi derivanti dalla lesione mammaria e dal sn , dimostrando che le due tecniche possono essere utilizzate contemporaneamente , con la stessa gdp , come gi affermato in letteratura [ 21 , 2729 ]  . i principali limiti dello studio sono stati che non abbiamo eseguito un paragone in parallelo con i metodi convenzionali di posizionamento di lo guida ; inoltre , stato necessario un dipartimento di medicina nucleare allinterno dellospedale per le corrette preparazione e gestione del radiotracciante . 
questo pu essere un limite soprattutto in piccoli ospedali . in conclusione , la guida radiologica nella roll ha garantito laf dabilit , lef cacia e laccuratezza dellintera procedura di localizzazione e rimozione di lesioni mammarie singole non palpabili e ne ha garantito il risultato nale nella maggioranza dei casi . 
simonetti dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e terapia radiante , universit degli studi di roma tor vergata ( ptv ) , viale oxford 81 , 00133 roma , italy correspondence to : c.a. 
il secondo esame ecogra co , eseguito successivamente alla mammogra a , ha confermato 123 / 147 lesioni nodulari solide , 53 / 67 casi di sbarramento del fascio ultrasonoro e 183 / 193 aree di disomogeneit ecostrutturale . 
sono state inoltre individuate 13 ulteriori lesioni nodulari non evidenziate alla preliminare ecogra a ed in due casi abbiamo riscontrato la presenza di substrato nella sede del reperto mammogra co di microcalci cazioni . 
dal nostro studio emerso che lecogra a effettuata senza la possibilit di riscontro mammogra co , ha dato luogo ad erronee interpretazioni diagnostiche intese sia come falsi positivi che come falsi negativi e secondo i nostri dati , qualora eseguita successivamente alla mammogra a , ha consentito di incrementare il valore della detection rate dellindagine ecogra ca da 4 , 16% a 5 , 5% . 
 parole chiave mammella ecogra a mammogra a iter diagnostico radiol med ( 2011 ) 116 : 584594 introduction introduzione in italy , mortality rates from breast cancer among women < 49 years of age have decreased by around 11% over the past 5 years [ 1 ]  . 
conventional imaging modalities , namely , mammography and ultrasound ( us ) , allow early detection of breast disease when performed according to strict methodological criteria and correct temporal sequence [ 2 ]  . 
mammography is the rst - line modality for early diagnosis of breast cancer in women > 3540 years of age , whereas us is an important complementary technique that increases sensitivity and speci city of mammography [ 3 , 4 ] , helps solve possible diagnostic doubts in dense breasts and is the only examination that can be performed in young women or to assess the solid or uid nature of opacities detected on mammography [ 2 , 5 ]  . 
however , the intrinsic limitations of us and its lower sensitivity compared with mammography in detecting suspicious breast lesions , in part as a result of the structural features of the glandular component and the operators experience , prevent this modality from being used as the sole technique for early detection of breast disease [ 69 ]  . sonographic detection of suspicious ndings is often facilitated by previous mammographic detection in relation to site and morphological characteristics . 
 although guidelines have been developed that indicate the correct sequence of diagnostic procedures [ 10 ] , inappropriate requests for us examinations as an alternative or prior to mammography continue to occur in clinical practice . 
consequently , women often appear confused by a lack of clarity regarding the best modality or the correct combination of modalities to be used and are sometimes led to undergo inappropriate investigations and to regard as dangerous and useless examinations that , instead , would effectively contribute to protecting their health . the aim of this study was to evaluate the role of the correct temporal sequence of conventional mammographic and us imaging . 
in particular , we aimed at analysing the increase in sensitivity for detecting suspicious ndings brought about by us performed following mammography . materials and methods from january 2008 to march 2010 , we studied 600 consecutive patients aged from 35 to 75 years referred to our department by their gynaecologist and / or family doctor with an inappropriate request for us to investigate a speci c clinical nding . 
requests were considered inappropriate negli ultimi cinque anni , in italia , la mortalit per carcinoma della mammella nelle donne al di sotto dei 49 anni diminuita di circa l11% [ 1 ]  . 
limaging convenzionale , rappresentato dalla mammogra a e dallecogra a , consente di ottenere una precoce individuazione della patologia mammaria qualora eseguito mediante rigorosi criteri metodologici e corretta successione temporale [ 2 ]  . 
lesame mammograco rappresenta lindagine di prima istanza nella diagnosi precoce del carcinoma della mammella nelle donne di et al di sopra dei 3540 anni , mentre lecogra a costituisce , ad oggi , unimportante tecnica complementare allesame mammogra co in grado di incrementarne la sensibilit e la speci cit [ 3 , 4 ] e dirimerne i dubbi diagnostici nei casi di mammelle a prevalente componente broghiandolare , come unica indagine in donne di giovane et e nella valutazione della natura solida o liquida di radiopacit nodulari evidenziate [ 2 , 5 ]  . 
tuttavia , i limiti intrinseci dellecogra a e la sua inferiore sensibilit rispetto allindagine mammogra ca nellindividuare la presenza di lesioni mammarie sospette , anche in relazione alle caratteristiche strutturali della componente ghiandolare ed allesperienza delloperatore , non consentono di utilizzare tale metodica come unica tecnica per la diagnosi precoce della patologia mammaria [ 69 ]  . 
a tuttoggi , seppur esistano delle linee guida che indicano la corretta successione delle indagini strumentali [ 10 ] , nella pratica clinica continuano a veri carsi richieste non idonee di esami ecogra ci in sostituzione o antecedenti lesame mammograco . 
la donna appare quindi spesso disorientata a seguito della scarsa chiarezza su quale sia la migliore tecnica o sul corretto percorso dintegrazione delle stesse , indotta , talora , a ricorrere ad indagini improprie ed a ritenere pericolosi ed inutili esami che , invece , contribuirebbero ef cacemente alla tutela della sua salute . 
in particolare abbiamo valutato lincremento di sensibilit nellindividuazione di reperti sospetti che lesame ecogra co determina quando effettuato successivamente ad esame mammogra co . 586 radiol med ( 2011 ) 116 : 584594 when no mammographic study had been performed in the previous 12 , 18 , or 24 months , depending on the patients age and structural features of the breast . 
as , according to the current guidelines , us is the rst - line imaging modality for assessing lesions in women < 35 years of age , as well as in breastfeeding and pregnant women , these patients were excluded from our study , as were those with breast implants , so as to obtain the most homogeneous results possible . all patients underwent preliminary us and subsequent mammography in standard projections ( craniocaudal , mediolateral oblique , mediolateral ) , when necessary with targeted compression and / or direct image magni cation . 
all patients with suspicious lesions proceeded to cytology / histology , vacuum - assisted biopsy ( vab ) and / or magnetic resonance ( mr ) imaging to obtain a correct diagnostic assessment , except in the event of ndings that had already been characterised or showed lesion stability over time . 
suspicious us ndings , deemed worthy of further investigation , were solid nodular lesions , posterior acoustic shadowing and areas of heterogeneous echostructure , the latter being de ned as focal areas of alteration of normal breast structure in particular of the regular alternation of supporting structures , fatty tissue and parenchymal component producing a different tissue response to the us beathese ndings could represent direct and / or indirect signs of a tumour . 
for the purposes of our study , we measured the detection rate of preliminary us and that of us performed after mammography . results preliminary us identi ed the presence of 147 hypoisoemateriali e metodi da gennaio 2008 a marzo 2010 abbiamo studiato 600 pazienti consecutive di et compresa tra i 35 ed i 75 anni giunte alla nostra osservazione con richiesta incongrua di esame ecogra co da parte del ginecologo e / o del medico curante al ne di valutare uno speci co reperto clinico . 
la richiesta stata considerata inappropriata in mancanza di un esame mammogra co recente ovvero antecedente ai 12 , 18 o 24 mesi in relazione alla fascia di et della paziente ed alle caratteristiche strutturali della mammella . 
secondo le attuali linee guida , essendo lecogra a lindagine di primo livello per la valutazione di lesioni in donne di et inferiore a 35 anni , in allattamento ed in gravidanza , tali pazienti non sono state incluse nel nostro studio , cos come abbiamo escluso le pazienti con protesi al ne di ottenere risultati il pi omogenei possibile . 
 le pazienti sono state tutte sottoposte , in fase preliminare , ad esame ecogra co e successivamente ad esame mammogra co , condotto mediante proiezioni standard ( cranio - caudale , medio - laterale - obliqua , medio - laterale ) , integrate , qualora necessario , con acquisizioni aggiuntive di dettaglio a compressione mirata e / o con ingrandimenti diretti di immagine . 
in tutti i casi studiati , nella prima indagine ecotomogra ca , non sono stati presi in considerazione i precedenti esami effettuati dalle pazienti e portati in visione , al ne di poter ottenere incondizionatamente un giudizio interpretativo . 
i reperti da noi considerati sospetti allesame ecogra co su cui abbiamo ritenuto opportuno effettuare ulteriori approfondimenti diagnostici , sono stati rilievi ecogra ci di lesioni nodulari solide , sbarramenti del fascio ultrasonoro ed aree di disomogeneit eco - strutturale ; con aree di disomogeradiol med ( 2011 ) 116 : 584594 choic solid nodular lesions ranging in size from 5 to 35 mm , 67 cases of acoustic shadowing ranging in size from 3 to 15 mm and 193 areas of heterogeneous echostructure ranging from 15 to 47 mat mammography , the 147 solid nodular lesions detected with us were depicted as nodular opacities with regular margins and well - de ned borders in 92 / 147 cases and as pseudonodular areas of radiolucency corresponding to fat lobules in 24 / 147 cases ; in 31 / 147 cases of highly dense breasts , no abnormal nding was detected . 
the 67 ndings identi ed as acoustic shadowing on us appeared as stellate radiopacities in 21 / 67 cases and areas of architectural distortion in 32 / 67 cases ; no mammographic correlate was detected in 14 / 67 cases . 
the 193 areas of heterogeneous echostructure proved to be areas of glandular asymmetry in 102 / 193 cases and areas of structural distortion in 81 / 193 ; no mammographic correlate was identi ed in 10 / 193 cases . 
 mammography enabled the detection of 13 additional faint nodular radiopacities in fatty breasts missed at preliminary us and 11 cases of microcalci cations , two of which were associated with an indistinct radiopacity . the second us scan , performed after mammography , con rmed 123 / 147 solid nodular lesions , 92 / 147 corresponding to the nodular opacities depicted by mammography and 31 / 147 missed at mammography in dense breasts . 
areas of heterogeneous echostructure previously identi ed at preliminary us were con rmed in 183 / 193 cases , 102 of which corresponding to areas of glandular asymmetry at mammography and 81 to areas of structural distortion . 
thirteen additional nodular lesions were identi ed , 12 of which were hypoisoechoic and one hyperisoechoic , corresponding to the nodular radiopacities missed at preliminary us owing to their subcentimetre size , hardly visible in a context of fatty breasts . 
in the 113 cases of architectural distortion , neit eco - strutturale intendiamo aree focali di alterazione della normale struttura della mammella , in particolare della regolare alternanza di strutture di sostegno , tessuto adiposo e componente parenchimale , che siano tali da determinare una differente risposta del tessuto al fascio ultrasonoro . 
 ai ni del nostro studio abbiamo quindi valutato il valore della detection rate dellindagine ecogra ca preliminare e di quella successiva alla mammogra a . risultati la prima indagine ecotomogra ca ci ha permesso di individuare la presenza di 147 lesioni nodulari solide ipo - isoecogene delle dimensioni comprese tra 56 mm e 35 mm , 67 sbarramenti del fascio ultrasonoro delle dimensioni comprese tra i 3 ed i 15 mm , e 193 aree di disomogeneit ecostrutturale delle dimensioni comprese tra i 15 mm ed i 47 mallesame mammogra co le 147 lesioni nodulari solide documentate allindagine ecogra ca sono state evidenziate come opacit nodulari a margini regolari e limiti netti in 92 / 147 casi , come aree pseudonodulari di radiotrasparenza riferibili a loggette adipose in 24 / 147 casi ed in ne in 31 / 147 casi non stato individuato alcun reperto in un contesto di mammella ad elevata densit ghiandolare . 
i 67 reperti apprezzabili come sbarramenti del fascio ultrasonoro sono risultati in 21 / 67 casi radiopacit stellariformi , in 32 / 67 casi aree di distorsione architetturale ed in ne in 14 / 67 casi non c stato corrispettivo riscontro mammograco . 
le 193 aree di disomogeneit ecostrutturale si sono rivelate in 102 / 193 casi aree di asimmetria ghiandolare , in 81 / 193 aree di distorsione strutturale ed in 10 / 193 casi non c stato corrispettivo riscontro mammogra co . lindagine mammogra ca ci ha permesso inoltre di individuare ulteriori 13 tenui radiopacit nodulari in mammelle a prevalente componente adiposa , non evidenziate al preliminare esame ecogra co , e 11 casi di microcalci cazioni , delle quali 2 / 11 casi sottesi a sfumate radiopacit . il secondo esame ecogra co , quello eseguito successivamente alla mammogra a , ha confermato 123 / 147 lesioni nodulari solide , di cui 92 / 147 corrispondenti alle opacit nodulari descritte alla mammogra a e 31 / 147 non distinguibili mammogra camente in un contesto di mammella broghiandolare . 
depending on our level of suspicion , 12 / 113 patients were referred for us follow - up at 6 months ( which con rmed lesion stability ) , 12 / 113 for mr imaging ( which excluded neoangiogenic components ) , 9 / 113 for cytology ( grade c2 ) and 11 / 113 for vab . 
seven of the latter 11 cases were brotic ndings , and the remaining four were radial scars ; these ndings were also con rmed by histological analysis of the surgical specimen . the 21 cases of stellate radiopacities underwent histological characterisation with us - guided vab , which revealed in ltrating carcinomas , which were con rmed by surgical histology in all cases . 
of the 13 cases of nodular radiopacities detected at mammography , eight were preexisting nodular formations that had remained virtually mati in 53 / 67 casi , di cui 21 / 67 casi erano rappresentati da radiopacit stellariformi e 32 / 67 casi da aree di distorsione architetturale ; in accordo con la mammogra a , in 14 / 67 casi non c stato corrispettivo riscontro ecogra co . 
le aree di disomogeneit ecostrutturale individuate precedentemente al primo esame ecotomogra co sono state confermate in 183 / 193 casi , di cui 102 / 193 erano riferibili ad aree di asimmetria ghiandolare allindagine mammogra ca e 81 / 193 ad aree di distorsione strutturale . 
sono state inoltre individuate 13 ulteriori lesioni nodulari , di cui 12 / 13 ipo - isoecogene ed 1 / 13 iper - isoecogena , corrispondenti alle radiopacit nodulari descritte , non evidenziate al preliminare esame ecogra co in considerazione delle loro esigue dimensioni subcentimetriche dif cilmente individuabili in un contesto di mammelle a prevalente componente adiposa . 
 nei 113 casi di distorsione architetturale , il confronto con i precedenti esami ci ha permesso di confermare la stabilit dei reperti in 69 / 113 casi , di cui 41 in pazienti gi sottoposte a chirurgia e , in base al nostro grado di sospetto , di inviare 12 / 113 casi al controllo ecogra co a 6 mesi , che ha successivamente confermato la stabilit dei reperti , 12 / 113 casi ad approfondimento diagnostico mediante esame rm , che ne ha escluso la presenza di componenti neoangionetiche , 9 / 113 casi allesame citologico con esito c2 e 11 / 113 casi al prelievo istologico tramite procedura vab . 
di questi ultimi 11 / 113 casi , si sono rivelati reperti di natura brosa 7 / 11 lesioni e radial scar le restanti 4 / 11 lesioni ; tali riscontri sono successivamente stati confermati anche allistologico de nitivo della chirurgia . i 21 casi di radiopacit stellariformi sono stati sottoposti a prelievo istologico mediante procedura vab sotto guida ecogra ca e si sono rivelati tutti carcinomi in ltranti , confermati allistologico chirurgico . 
dei 13 casi di radiopacit nodulari riscontrate alla mammogra a , 8 / 13 erano rappresentate da formazioni nodulari gi presenti e sostanzialmente invariate rispetto ai precedenti controlli , mentre i restanti 5 / 13 casi di primo riscontro sono stati sottoposti a caratterizzazione cito - istologica , il cui esito stato in 2 / 5 casi di benignit , in 2 / 5 casi di carcinoma in situ ed in 1 / 5 casi di carcinoma in ltrante . 
degli 11 casi di microcalci cazioni , in 2 casi si dimostrato un substrato ecogra co in tale sede ed i reperti sono stati quindi sottoposti a caratterizzazione istologica tramite prelievo vab con esito di carcinoma in ltrante ; dei restanti 9 / 11 casi sono state sottoposte a prelievo vab sotto guida mammogra ca 6 / 11 casi , il cui esito stato in 3 / 6 casi di benignit , in 1 / 6 casi di iperplasia duttale atipica ed in 2 / 6 casi di carcinoma in situ , mentre nei restanti 3 / 11 casi le caratteristiche morfologiche delle microcalci cazioni deponevano per la loro benignit . secondo i nostri dati quindi il valore della detection rate dellindagine ecogra ca subisce un incremento qualora questultima sia effettuata successivamente alla mammogra a e guidata da questultima : la detection rate della prelifig . 
1 proiezioni mammogra che medio - laterali - oblique in cui si documenta a destra , in corrispondenza del prolungamento ascellare , una sfumata radiopacit a margini irregolari , che si conferma allesame di dettaglio a compressione mirata . 
la successiva indagine ecotomogra ca ha permesso di evidenziare a tale livello millimetrica area ipoecogena . unchanged since the previous examinations , whereas the remaining ve cases of initial detection underwent cytological and histological characterisation , which revealed a benign lesion in 2 / 5 cases , carcinoma in situ in 2 / 5 and in ltrating carcinoma in 1 / 5 . 
of the 11 cases of microcalci cations , us showed a sonographic correlate at the site in two cases , and the lesions were further characterised with vab , which yielded a diagnosis of in ltrating carcinoma . 
of the remaining nine cases , six underwent mammographically guided vab , which indicated a benign lesion in three cases , atypical ductal hyperplasia in one case and carcinoma in situ in two cases . 
morphology in the remaining three cases indicated a benign nature . according to our results , the detection rate of us increases when the examination follows mammography and is guided by it : the detection rate of preliminary us was 4.16% , whereas that of us performed following mammography rose to 5.5%. 590 radiol med ( 2011 ) 116 : 584594 fig . 
2 proiezioni mammogra che cranio - caudali e medio - laterali in cui si documenta a destra , in corrispondenza del quadrante infero - interno , una centimetrica sfumata radiopacit in un quadro di mammelle a prevalente componente adiposa . 
3 craniocaudal and mediolateral mammograms showing right breast opacity with ill - de ned borders and irregular margins associated with typical irregular calci cations , con rmed by targeted compression . 
3 proiezioni mammogra che cranio - caudali e medio - laterali in cui si documenta a destra , in corrispondenza della porzione di passaggio dei quadranti esterni , una radiopacit a limiti sfumati e margini irregolari , che si conferma allesame di dettaglio a compressione mirata , nel contesto della quale si apprezzano alcune ni calci cazioni . 
la successiva indagine ecotomogra ca ha permesso di evidenziare a tale livello unarea iso - ipoecogena a margini irregolari di circa 1 cm . radiol med ( 2011 ) 116 : 584594 minare indagine ecogra ca risultata del 4 , 16% , mentre la detection rate della seconda ecogra a stata del 5 , 5% . discussione la riduzione della mortalit per carcinoma mammario , cui si assistito negli ultimi anni in italia , dovuta senzaltro allaumento della sensibilit delle donne a sottoporsi spontaneamente a controlli strumentali periodici ed anche alla maggiore diffusione dei programmi di screening , che consentono di diagnosticare questa patologia in fasi sempre pi precoci [ 11 ]  . 
a tale proposito le tecniche ad oggi disponibili per la diagnosi precoce del carcinoma mammario sono rappresentate fondamentalmente dallimaging convenzionale mammogra co ed ecogra co e solo tramite una loro rigorosa e scrupolosa applicazione si giunge ad una diagnosi tempestiva al ne di unef cace prevenzione secondaria [ 10 ]  . 
la mammogra a attualmente lesame di prima istanza in donne di et superiore ai 35 anni , in quanto permette in modo suf cientemente ripetibile e confrontabile , lesplorazione della mammella ; ci fa ritenere lesame mammogra co la tecnica pi importante per lo studio della patologia mammaria [ 2 , 10 , 11 ]  . 
lecogra a rappresenta la pi importante modalit di imaging complementare dopo la mammogra a , in quanto contribuisce insieme allesame clinico ad elevare la sensibilit della diagnosi sino al 90% e la speci cit sino al 98% [ 10 ]  . 
lesame richiede lutilizzo di sonde ad elevata frequenza ( 10 mhz ) di tipo small parts lineare , che assicurano la corretta penetrazione del fascio ultrasonoro anche in mammelle voluminose con una focalizzazione dinamica ed una buona esplorazione del parenchima . 
la speci cit dellindagine ecogra ca inoltre aumentata dallimpiego di tecnologie quali color e power doppler per la valutazione del pattern vascolare peried intralesionale e pi recentemente mediante lausilio della metodica elastosonogra ca . 
 nonostante lecogra a sia diventata strumento diagnostico indispensabile nella valutazione della patologia mammaria , tuttavia necessario puntualizzare che tale metodica non entra in competizione con le altre tecniche diagnostiche , in particolar modo con la mammogra a [ 12 , 13 , 14 ]  . 
lecogra a mammaria deve infatti essere effettuata a complemento della mammogra a , piuttosto che in sostituzione di essa , ed entrambe devono costituire ununit diagnostica nella valutazione della patologia mammaria [ 6 , 12 , 13 , 15 ]  . 
tale ultima considerazione trova ulteriore riscontro nel fatto che negli ultimi 20 anni si assistito ad una crescente incidenza del carcinoma mammario pi signi cativa nelle donne in et fertile , nelle quali lutilizzo della mammogra a richiede necessariamente il completamento ecogra co in relazione alla densit ed alle caratteristiche strutturali della componente ghiandolare [ 1 , 11 , fig . 
4 proiezione mammogra ca cranio - caudale ed esame di dettaglio a compressione mirata della mammella destra in cui si documenta , a livello dei quadranti esterni , una tenue area radiopaca pseudonodulare a limiti sfumati , nel contesto della quale si apprezzano alcune microcalci cazioni . 
 discussion the lower mortality rate of breast cancer recently observed in italy is no doubt a consequence of womens heightened awareness of the need to undergo periodic imaging investigations , as well as the greater availability of screening programmes that allow for increasingly earlier detection of the disease [ 11 ]  . 
the techniques available for an early diagnosis of breast cancer include conventional mammography and us imaging , and only a rigorous and scrupulous application of these modalities can lead to a timely diagnosis and effective secondary prevention [ 10 ]  . 
us represents the main adjunctive imaging modality after mammography , as it helps along with the clinical examination to increase diagnostic sensitivity to 90% and speci city to 98% [ 10 ]  . 
the examination requires the use of high - frequency ( 10 mhz ) small - parts lineararray probes , which ensure correct penetration of the us beam even in large breasts , with dynamic focusing and good parenchymal exploration . 
the speci city of us is further increased by the use of techniques such as colour and power doppler for evaluating periand intralesional vascular patterns and , more recently , by the use of elastosonography . although us has become an essential diagnostic tool 592 radiol med ( 2011 ) 116 : 584594 fig . 
5 proiezioni mammogra che cranio - caudali , medio - laterali ed ingrandimento dimmagine con zoom elettronico in cui si apprezza a sinistra , a livello della porzione di passaggio dei quadranti esterni in corrispondenza della camera posteriore , una tenue radiopacit a limiti sfumati . 
la successiva indagine ecotomogra ca ha documentato , in corrispondenza del reperto mammogra co , la presenza di una formazione nodulare ad ecostruttura disomogenea prevalentemente iperecogena di circa 1 cm . in evaluating breast disease , it must be emphasised that it is not in competition with other diagnostic modalities , notably with mammography [ 12 , 13 , 14 ]  . 
in fact , breast us is to be used as an adjunct rather than a replacement for mammography , with the two modalities forming an integrated diagnostic tool in evaluating breast disease [ 6 , 12 , 13 , 15 ]  . 
this is also supported by the fact that the last 20 years have seen a growing incidence of breast cancers , especially among women of childbearing age in whom mammography necessarily requires supplementation with us in relation to density and structural features of the glandular component [ 1 , 11 , 16 ] , given that mammographic sensitivity is reduced in dense breasts . 
in fact , even though us used as the only imaging technique is able to yield a diagnosis of malignant nodular lesions when these are well de ned , as reported in the literature [ 17 , 18 ] , combined mammography and sonography increases the diagnostic accuracy of the each modality to 95% [ 11 ]  . 
in particular , when us is performed after mammography , it markedly increases in sensitivity and speci city [ 13 ]  . this was also con rmed by our study , which aimed at evaluating the correct temporal sequence of the modalities . 
 in particular , we found that us performed after mammography not only improves the assessment of known mammographic ndings but also in many cases , us ndings are guided by the results of the mammographic study ( lesion site and dimensions )  . 
 [ 19 ] , this observation was found to apply in particular to 16 ] in quanto la sensibilit della mammogra a si riduce se la componente adiposa poco rappresentata . 
sebbene lecogra a utilizzata come unica indagine strumentale sia attualmente in grado di porre diagnosi di lesioni nodulari maligne qualora ben circoscritte , in accordo con alcuni dati della letteratura [ 17 , 18 ] , tuttavia la diagnostica senologica integrata mammo - ecogra ca aumenta no al 95% laccuratezza diagnostica delle singole metodiche [ 11 ] ed in particolare , qualora lecogra a sia eseguita successivamente allesame mammogra co , ne aumenta notevolmente la sensibilit e la speci cit [ 13 ]  . tale ultimo dato stato confermato dal nostro lavoro , che ha avuto lobiettivo di valutare la loro corretta successione temporale ; in particolare abbiamo evidenziato che lecogra a eseguita successivamente allindagine mammogra ca non solo migliora la valutazione di reperti mammogra ci gi noti , ma spesso lo stesso rilievo ecogra co in uenzato dalla conoscenza del reperto mammogra co ( sede e dimensioni della lesione )  . 
 [ 19 ] tale considerazione ha trovato particolare riscontro nella valutazione delle mammelle a prevalente componente broghiandolare [ 7 , 19 ] e nel nostro studio anche nei casi di lesioni focali in mammelle adipose e nella ricerca di un eventuale substrato patologico nei casi di microcalci cazioni . 
 [ 14 ] , lesame ecogra co , qualora necessario , se eseguito successivamente alla mammogra a , aumenta laccuratezza diagnostica della metodica e ne fornisce importante complemento . radiol med ( 2011 ) 116 : 584594 dense breast evaluations [ 7 , 19 ] , as well as in our study to focal lesions in fatty breasts and to the search for a possible pathological substrate in cases of microcalci cations . 
 [ 14 ] , that when needed , us imaging performed after mammography improves its diagnostic accuracy and provides a valuable complement . in our experience , us following mammography enabled the identi cation of 12 cases of small isohypoechoic lesions in prevalently fatty breasts that were missed owing to the limits of us in fatty breasts . 
two cases of hypoechoic areas were identi ed as substrates for microcalci cation clusters only recognisable at mammography , as was one case of a hyperisoechoic nodule that could only be identi ed knowing its anatomical position , which was provided by orthogonal mammographic projections . 
lastly , histology demonstrated that the us detection rate increases when the modality is performed after mammography to further investigate doubtful mammographic ndings rather than as a rst - line imaging test . 
 in addition , our study showed that us performed without mammographic assessment led to diagnostic misinterpretations false positive ( 8% ) or false negative ( 4% ) which may result in additional diagnostic tests that are often unnecessary and burdensome in a context of increasingly scarce healthcare resources . nella nostra esperienza lindagine ecogra ca eseguita successivamente alla mammogra a ha consentito di identi care 12 casi di lesioni di piccole dimensioni iso - / ipoecogene in mammelle a prevalente componente adiposa , misconosciute a causa dei limiti della metodica ecogra ca in mammelle adipose . 
sono stati individuati due casi di aree ipoecogene quali substrati di cluster di microcalci cazioni apprezzabili unicamente allesame mammogra co ed in ne un caso in cui la lesione , rappresentata da nodulo iper - / isoecogeno , poteva essere identi cata unicamente conoscendone la sede anatomica mediante le proiezioni ortogonali mammogra che . 
al contrario , 24 casi di lesioni ipoecogene evidenziate allesame ecogra co si sono rivelate aree di radiotrasparenza alla mammogra a e quindi di nessun signicato patologico da un punto di vista diagnostico . 
in ne , secondo i risultati istologici ottenuti , il valore della detection rate dellindagine ecogra ca subisce un incremento qualora questultima sia effettuata successivamente alla mammogra a , quale approfondimento di reperti mammogra ci dubbi e non come esame di prima istanza : infatti la detection rate della preliminare indagine ecogra ca risultata del 4 , 16% , mentre la detection rate della seconda ecogra a stata del 5 , 5% . 
dal nostro studio emerso inoltre che lindagine ecogra ca effettuata senza la possibilit di riscontro mammogra co , ha dato luogo ad erronee interpretazioni diagnostiche intese sia come falsi positivi , approssimativamente l8% , che come falsi negativi , circa il 4% , che talvolta portano allesecuzione di ulteriori accertamenti diagnostici spesso inutili e gravosi in un contesto sanitario in cui le risorse economiche sono sempre pi carenti . conclusioni conclusions despite an increased awareness of prevention , women are often confused about the most appropriate imaging modality and the best approach for integrating conventional breast imaging techniques . 
they therefore require counselling by a healthcare professional who can direct them towards a correct and timely diagnosis , in consideration of the clinical picture and patient history . in conclusione , sebbene le donne negli ultimi anni siano pi sensibili alla prevenzione , spesso si ritrovano disorientate su quale sia la migliore indagine strumentale da effettuare e quale possa essere il corretto percorso dintegrazione delle stesse . 
the clinical outcome is shown by the use of clinical scores : visual analogue scale ( vas ) , constants score and shoulder pain disability index ( spadi )  . 
boccalini radiology department , school of medicine , universita` di genova , largo rosanna benzi 8 , 16138 genoa , italy common painful condition that occurs in up to 7.5 % of otherwise healthy adults . 
in adhesive capsulitis , different therapeutic ultrasound - guided techniques such as corticosteroid injection , capsular distension ( sodium chlorate solution ; sodium chlorate and corticosteroids ; air ) and viscosupplementation are evaluated . 
the treatment of rotator cuff tendinosis and partial tears with ultrasound - guided injection of concentrated autologous platelets is also described . keywords ultrasound injection ( cid : 2 ) rotator cuff calcication ( cid : 2 ) viscosupplementation ( cid : 2 ) platelet - rich plasma ( cid : 2 ) adhesive capsulitis j . 
martinoli radiology department , dissal , universita` di genova , largo rosanna benzi 8 , 16138 genoa , italy the aim of this review is to describe the techniques of interventional ultrasound for the treatment of shoulder pathology . 
shoulder ultrasonography ( us ) is an accurate method to perform diagnostic studies , because it evaluates both morphology and function by means of dynamic evaluations [ 1 ]  . 
us is also a very radiol med ( 2014 ) 119 : 318326 table 1 constants score combines two subjective variables like pain and pain in relation to daily activities ( value range 035 ) and two objective measurements like strength and range of motion ( value range 065 ) as assessed by a physician item pain none mild moderate severe full work activities of daily living full recreation / sports unaffected sleep hand position up to wrist up to xiphoid up to top of head above head range of motion abduction forward elevation internal rotation external rotation shoulder power pounds to resist total useful tool to guide interventional procedures around the shoulder and sometimes to inject intra - articular contrast media before magnetic resonance ( mr ) arthrography [ 6 , 7 ]  . 
blind injections may fail in a signicant percentage of cases , so the use of a low - cost and safe tool such as us improves the success of the interventional procedures [ 8 ]  . the comparison of us - guided against landmark - guided injection in shoulder pathology shows a statistically signicant difference in pain control [ 9 , 10 ] in favour of usguided methods . mild vagal reactions may be considered the most frequent immediate complications as reported in the literature [ 11 ]  . 
the visual analogue scale ( vas ) , a well - known 10 - cm graduated scale ranging from 0 ( no pain ) to 10 ( unbearable pain ) , is commonly employed in clinical practice [ 11 ]  . 
constants ( score score constant_shoulder_score.html ) combines two subjective variables ( pain and pain in relation to daily activities , value range 035 ) and two objective measurements ( strength and range of movement , value range 065 ) assessed by a physician . 
the shoulder pain and disability index ( spadi ) questionnaire is a self - administered index designed to measure the effects of different pathologic conditions on the functional status of the shoulder [ 12 , 13 ]  . the spadi questionnaire is also used to measure the response to treatment over time . 
the questionnaire consists of 13 items divided into 2 subcategories reecting the disability ( 8 items ) and pain ( 5 items ) associated with the clinical syndrome of painful shoulder . 
all items are rated by using a vas from no pain or no difculty to worst imaginable pain or so difcult it required help . a numeric value was obtained by dividing the scale into 11 segments from 0 to 10 for each itefigure 1 and tables 1 and 2 show different scales to assess shoulder disability . rotator cuff calcication rotator cuff calcication is a common painful condition which occurs in up to 7.5 % of otherwise healthy adults . women are more frequently affected than men , especially during the fth decade of life [ 11 ]  . 
deposition of calcium hydroxyapatite crystal may be due to a relative hypoxia in the so - called critical zone ( about 1 cm from the tendinous insertion of supraspinatus on the greater humeral tuberosity ) [ 14 ]  . it is believed that the decrease of oxygen concentration may be responsible for brocartilaginous metaplasia and cellular necrosis followed by calcium deposit formation . tendon calcications are considered a self - healing condition , but may cause chronic pain and functional disability with a negative impact on everyday life . 
the supraspinatus tendon is most commonly affected , followed by the infraspinatus tendon and the subscapularis tendon [ 1 ]  . the formation of calcication may be considered a disorder that occurs in four stages : stage 2 stage 1 precalcic , with brocartilaginous transformation is usually tendon . 
in this phase 320 table 2 the shoulder pain and disability index ( spadi ) questionnaire is a selfadministered index that consists of 13 items divided into 2 subcategories reecting the disability ( 8 items ) and pain ( 5 items ) associated with the clinical syndrome of painful shoulder all items are rated by using a visual analogue scale from no pain or no difculty to worst imaginable pain or so difcult it required help . 
pushing with the involved arm no pain 0 1 2 3 4 5 6 7 8 9 10 worst pain imaginable disability scale how much difculty did you have : 1 . 
removing something from your back pocket no pain 0 1 2 3 4 5 6 7 8 9 10 worst pain imaginable stage 4 severe pain and restriction of movement could be associated with systemic symptoms . postcalcic phase with self - healing and repair of the rotator cuff . 
this phase lasts several months and may be associated with pain and restricted function [ 1 ]  . three types of calcic deposits have been described on us depending on the amount of calcium in the deposits . type i is hard , rich in calcium and hyperechoic with welldened acoustic shadowing and corresponds to the formative phase ( this kind of calcication is supposed to be present in up to 80 % of cases )  . 
type ii and type iii calcications are dened slurry calcication and correspond to the resorptive phase in which the deposits are almost liquid [ 1 ]  . in the presence of calcications , asymptomatic patients are treated conservatively with no need for preventive interventional procedures . 
the complications of usguided treatment are vasovagal reaction ( during the procedure ) , late painful bursitis and infection ( septic arthritis )  . different techniques are described in literature . 
1 the visual analogue scale ( vas ) is a 10 - cm graduated scale ranging from 0 ( no pain ) to 10 ( unbearable pain ) puncturing it 1015 times and then simultaneously injecting and aspirating saline solution using two 1819 - gauge needles . 
propose a less aggressive technique with a single ne needle ( 22 gauge ) to perform the procedure . this approach consists in puncturing and fragmenting the calcication with intra - calcication injection of saline solution or local anaesthetic and needle beak rotation in a single procedure . 
better results have been obtained in patients who had calcium fragments successfully aspirated from the rotator cuff compared with patients who had no calcium radiol med ( 2014 ) 119 : 318326 fragments aspirated [ 14 ]  . 
 [ 16 ] chose a 20 - gauge needle because the needles with smaller bore tend to become obstructed by the calcic fragments . the rst step of the two - needle technique proposed by serani et al . 
this step is repeated several times ( 1020 , with a total amount of 300400 ml of saline solution injected ) until the ushed uid is completely free of visible calciuone needle is then extracted and the tip of the second needle is inserted into the subacromialsubdeltoid bursa where soluble cortisone is injected . 
this study demonstrated clinical improvement , as shown by the scoring system , at 1 - month follow - up in the treated patients , but not in the controls . 
at 1 - year follow - up , no tendon cuff tear was seen [ 11 ]  . conclusion , percutaneous us - guided therapy improves the clinical outcome and accelerates the healing process . 
however , the use of two needles generates a continuous inand outow of the saline solution , thus allowing control of the saline solution pressure inside the calcication during the injection . 
the ute - beak tip of needle has to be rotated upward . at the end of the procedure , the thin calcic wall is leone or two needles may be used rim , which can cause calcium leakage into the surrounding tissue that correlates with postprocedural bursitis . 
with the one - needle technique , operators were unable to retrieve calcium from all patients [ 6 ] , while with the two - needle technique calcium retrieval was demonstrated in 100 % of the patients [ 11 ]  . 
moreover , the one - needle technique may increase the risk of postprocedural bursitis related to calcication rim disruption . viscosupplementation intra - articular injection of hyaluronic acid ( viscosupplementation ) is a new therapeutic approach for the treatment of shoulder pathology . 
several shoulder pain aetiologies have been evaluated : osteoarthritis ( oa ) , rotator cuff tear and tendinosis , periarthritis , duplays disease , adhesive capsulitis . the prevalence of oa increases with age . 
hand , knee , ankle , spine and hip joints are more frequently involved . more experience has been acquired in oa of the knee . several studies have shown the efcacy of hyaluronic acid in the treatment of oa of the knee , with positive effects on articular function , pain , subjective global assessment and reduction of nsaid consumption . 
the benet is evident within following 3 months 612 months [ 17 ]  . persists hyaluronic acid ( ha ) is a linear polymer formed of the disaccharide units n - acetyl - d - glucosamine and na - d - glucuronate and it is a physiological component of the synovial uid ( of which it represents the major chemical component ) produced by type b synoviocytes and broblasts . 
native ha ( 410 mda ) has viscoelastic properties , due to its high viscosity , which promote joint lubrication that is essential for shock - wave absorption and has protective effects on the articular cartilage and soft tissue surfaces of the joints . 
this would explain why ha has a long - term clinical effect compared to the short half - life of the preparations . nowadays , there are several commercially available ha by - products obtained from rooster combs or with recombinant technology that differ in molecular weight and therefore in rheologic properties [ 18 ]  . molecular preparations ( lmw weight 0.51.5 mda ) demonstrate a good penetration in the extracellular matrix of synovial uid . 
the limit of these 322 radiol med ( 2014 ) 119 : 318326 preparations is the low viscoelasticity compared to the native ha ( in vitro and animal model studies ) [ 17 , 18 ]  . 
for this reason , more recently , attention has been shifted to high molecular weight preparations ( hmw 67 mda ) formed by a cross - linked ha ( hylan f - 20 )  . 
in osteoarthritis , treatment with weekly ha injections for three consecutive weeks improves the clinical scores and achieves pain relief at 6 months follow - up [ 19 ]  . in elderly patients there are several problems in the management of shoulder pathe classic approach is based on nonpharmacological strategies such as the use of orthotics , physiotherapy , exercise and activity modication . 
chronic use of oral nsaids increments the risk of gastrointestinal ( gi ) effects ; the use of selective nsaids reduces the risk of gi effects , but is linked to cardiovascular complications . 
one rare , but severe complication is osteonecrosis . viscosupplementation is indicated in patients where the pain relief strategies have failed , those with intolerance to nsaids and in those with intermediate kellgrenlowrence score ( iiiii )  . 
the contraindications are hypersensitivity to egg proteins and rheumatologic systemic diseases ( rheumatoid arthritis , gout , psoriasis , chondrocalcinosis )  . in particular , an open - label non - randomised trial evaluated the efcacy of us - guided high molecular weight ha injection in elderly patients with massive rotator cuff tear arthropathy and advanced osteoarthritis . 
these were all patients for whom surgery was not feasible because of coexisting medical conditions and because of the poor results expected with any kind of surgical intervention . the injection is performed under us guidance ( this approach is mandatory since blind injection is associated with high failure rate )  . 
then , the physician induces local anaesthesia in the subacromial chloridrate without space 2 % mepivacaine using adrenaline ( maximum 400 mg of local anaesthetic during the entire procedure )  . 
the results showed signicant improvement of the vas and constant score in the rst 4 months of follow - up in the treated patients , but not in the control subjects . 
after 5 months the outcome of treated and nontreated patients was not different [ 20 ]  . in rotator cuff lesions without complete tear , the subacromial injection of sodium hyaluronate is effective . 
in 25 patients , 25 mg / week of sodium hyaluronate was administered into the subacromial bursa for 5 consecutive weeks . the control group was given 2.5 ml of sodium chloride with the same injection protocol . 
the second group did not demonstrate global improvement or signicant differences in the constant and vas scores after the injection [ 21 ]  . the efcacy of ha is also demonstrated in supraspinatus tendinosis . 
the technique differs from subacromial injections in that after determining supraspinatus tendon thickness and its superior border , the needle is introduced as far as the surface of the superior border and then the solution is injected . the patients were divided into two groups : a sodium hyaluronate group and a sodium chloride group . 
note the absence of the needle ( arrows ) and the injection of supraspinatus tendon , hyaluronic acid ( hypoechoic area ) radiol med ( 2014 ) 119 : 318326 group , shoulder disability resolved after three ( 6 out of 28 ) , four ( 13 out of 28 ) and ve ( 6 out of 28 ) injections of sodium hyaluronate . 
in the second group , all patients were unsatised ( no signicant variation of pretreatment vas score at 4 and 12 weeks follow - up ) and none of them reported a sufcient improvement after ve injections of lidocaine and sodium chloride solution [ 22 ]  . the limitations of these open - label studies are the use of nsaids after the procedure , low patient number and short follow - up period . viscosupplementation under us guidance may constitute a valid tool in pain relief and functional recovery in elderly patients with massive rotator cuff tear arthropathy , noncomplete rotator cuff tears , mild osteoarthrosis ( kellgrenlowrence iiiii ) and supraspinatus tendinosis , but more studies , with particular attention to long - term evaluation , are necessary to validate this new therapeutic approach in shoulder pathology . adhesive capsulitis adhesive capsulitis is a condition of varying severity characterised by the gradual development of global limitation of active and passive shoulder motion where radiographic ndings other than osteopenia are absent [ 23 ]  . in 1872 , duplay [ 24 ] described a condition called periarthritis scapulo - humerale , and later codman [ 25 ] described this disorder as frozen shoulder and until now adhesive capsulitis of the shoulder remains a class of cases which are difcult to dene , difcult to treat , and difcult to explain from the point of pathology . 
it has been suggested that frozen shoulder is precipitated by degeneration of the supraspinatus tendon and is associated with chronic inammation of the subacromial bursa and glenohumeral capsule . several conditions are related to adhesive capsulitis such as female sex , trauma and age of more than 40 years , diabetes , prolonged immobilisation , thyroid disease , stroke and myocardial infarction , presence of autoimmune disease , epilepsy , parkinson and dupuytren disease . 
histologic and immunocytochemical investigations have demonstrated active broblastic proliferation accompanied by the transformation of broblasts into myobroblasts [ 26 ]  . this condition is widely reported as a typical middle age disease and is characterised by three phases : a painful phase , lasting between 3 and 8 months , followed by a phase of progressive stiffness or adhesive phase that typically lasts 46 months . 
the nal resolution phase of gradual return of motion usually lasts 524 months [ 27 ]  . the most characteristic mr arthrography ndings in frozen shoulder are the thickening of the coracohumeral ligament and of the capsule at the rotator cuff interval and the complete obliteration of the fat triangle under the coracoid process ( subcoracoid triangle sign ) [ 28 ]  . surgical treatment ( arthroscopic capsulotomy ) is the best choice when conservative treatment fails . injection therapy is often used when ice therapy , oral nsaids and corticosteroids are not enough to improve the clinical outcome . 
corticosteroid injection , ha injection , distension with sodium chlorate , distension with sodium chlorate and steroids and distension with air and physical therapy ( exercise , transcutaneous electrical nerve stimulation , us ) are used for conservative management of adhesive capsulitis . to the biceps interval medial us - guided corticosteroid and lidocaine injection into the tendon shows rotator improvement in primary outcome ( spadi score after 12 weeks ) and in secondary outcome ( increase in active and passive range of motion ) [ 30 ]  . 
capsular distension with lidocaine and ha is effective as well as steroid injection in pain relief and functional improvement [ 31 ]  . comparison of different treatments demonstrates that ha injection is an alternative therapy in adhesive capsulitis . 
isolated intra - articular hyaluronate injection has an equivalent outcome compared to intra - articular corticosteroid injection [ 32 ]  . moreover , us - guided injection associated with shoulder exercises ensures pain relief in the medium - term follow - up with respect to injection alone [ 33 ]  . 
when corticosteroids are contraindicated , hyaluronic acid injection is a proper alternative tool . acromion - clavicular joint osteoarthrosis of the acromionclavicular ( ac ) joint is a common pathology observed in elderly patients and in young adults in some cases . 
the joint is injected with the use of a local anaesthetic have evolved from open repair with transosseous suture to arthroscopic techniques ( single - row , double - row , transosseous - equivalent suture , anchor constructs )  . 
cytokines and growth factors ( including pdgf , tgf - a , tgf - b , interleukin - 1 and broblast growth factor ) play an important role in chemotaxis , matrix synthesis , proliferation and cell differentiation , and a combination of these factors may improve healing of the tendon insertion site . platelet - rich plasma ( prp ) is a fraction of plasma that has been isolated and used to enhance the regeneration of bones and soft tissues . 
blood is taken from the patient ; the prp fraction is separated and transferred to a bottle without air contact to prepare a membrane of autologous brthe nal product , the membrane , obtained by high - speed centrifugation of prp is a thin layer that is very rich in platelets containing approximately 50 times the platelet concentration of initial blood . 
a systematic review demonstrated that prp does not have any effect on overall re - tear rates or shoulder - specic outcomes after arthroscopic rotator cuff repair in patients with full - thickness rotator cuff tears [ 38 ]  . surgical intervention allows debridement of degenerated cuff and partial thickness cuff tears , subacromial bursitis , impinging bone spurs and osteophytes together with rotator cuff repairs . 
repairs of degenerated and torn tissue are often prone to failure due to many intrinsic and extrinsic factors . prp might improve clinical , mechanical and histological outcomes [ 39 ]  . 
thus , the treatment of tendinosis with a usguided injection of concentrated autologous platelets may be a nonsurgical alternative . some studies are trying to validate the role of prp tendon injection . 
in chronic lateral epycondilitis , prp improves pain and function more effectively than corticosteroid injection sustained over a 2 - year follow - up time with no reported complications [ 40 ]  . 
5 needle ( arrows ) in subacromialsubdeltoid bursa ( asterisk )  . the bursa is distended with the use of corticosteroids the level of the ac joint are the typical x - ray ndings in ac osteoarthritis . 
ac injection of steroid and lidocaine solution is indicated in the conservative treatment ( tossy and allman classication type i - ii [ 36 ] ) of painful ac osteoarthrosis . 
clinical improvement evaluated through vas at rest , vas with local pressure ( exerting pressure on the joint space area ) , and constant and murley scores is considerable , especially in the rst week after therapy [ 37 ]  . platelet - rich plasma rotator cuff tears are common injuries that require surgical treatment . 
 [ 42 ] concluded that patients who received prp injection demonstrated modest improvement in functional outcome measures , while the mri appearance of diseased achilles tendons remained largely unchanged following prp injection [ 42 ]  . us guidance can be a valid tool to perform a procedure with a proper selection of injection site , because it allows one to identify the disrupted tendon bres with loss of normal echostructural brillary areas . 
patients were followed up for up to 12 months . results a complete response was obtained in 87 % lesions treated with pla and in 93 % lesions treated with rfa ( p = ns )  . 
angelico epatologia , policlinico universitario tor vergata , viale oxford 81 , 00133 rome , italy conclusions rfa is more effective in the treatment of hcc compared to pla for lesions c21 mhowever , pla should be considered a viable treatment option for incidence of hcc b20 mm , complications . in view of the lower keywords hepatocellular carcinoma ( cid : 2 ) liver cirrhosis ( cid : 2 ) percutaneous laser ablation ( cid : 2 ) radiofrequency thermoablation introduction hepatocellular carcinoma ( hcc ) is the sixth most worldwide malignancy for incidence [ 1 ] and the third leading cause of global cancer mortality [ 2 ] , causing 600 , 000 deaths per year [ 2 , 3 ]  . 
in the western world , more than 90 % of hcc develop in patients with liver cirrhosis [ 4 ]  . surgical resection is the rst - choice treatment , but it is not always feasible due to the location and number of lesions , and the progressive deterioration of liver function in patients with cirrhosis [ 5 , 6 ]  . 
today , the gold standard is liver transplantation ( lt ) , which is , however , difcult to implement for lack of donors [ 7 ]  . over the years , several techniques for locoregional ablation have been developed for the treatment of patients with hcc nodules smaller than 4 cm , who are not candidates for resection or transplantation . 
these techniques include percutaneous ethanol injection ( pei ) , percutaneous injection of acetic acid ( pai ) , microwave thermoablation ( mw ) , cryoablation , high - intensity focused ultrasound ( hifu ) , radiofrequency ablation ( rfa ) and percutaneous laser ablation ( pla ) [ 8 ]  . 
a meta - analysis of prospective randomised trials has shown that rfa of liver radiol med ( 2014 ) 119 : 298308 tumours has greater efciency compared to pei in terms of ease of implementation , safety , applicability and costeffectiveness [ 10 ]  . 
pla can be compared to rfa in the treatment of patients with hcc , in terms of technical reliability and efcacy [ 14 ]  . to our knowledge , few studies have compared and analysed the results obtained with the two techniques [ 15 ]  . the aim of this study was to compare pla and rfa in terms of complete response at 30 days , local recurrencefree survival , complications such as postablation syndrome and postprocedural tnfa production , in cirrhotic patients with unifocal hcc b4 cm . materials and methods this study was approved by the ethics committee of our institution . 
the afetoprotein levels recorded before the procedure were on average 561.67 684 ng / ml ( range 251 , 870 ) ( table 1 )  . all patients were selected during the follow - up for liver cirrhosis , and the choice of percutaneous ablative treatment was made by a multidisciplinary team of hepatologists , surgeons and interventional radiologists [ 16 ]  . 
we selected patients with a single hcc nodule with a maximum diameter of 40 mthe diagnosis of hcc was established in accordance with the guidelines of the european association for the study of the liver ( easl , european association for the study of liver ) [ 17 ] for the diagnosis of hcc in cirrhotic patients . 
exclusion criteria were child class c , poor clotting function ( quick test \50 % , platelets \40 , 000 / ml ) and the presence of multiple lesions . randomisation software was used to allocate each patient to a treatment group . 
to assess any changes in the size of the nodule and / or the appearance of new lesions , within 2 weeks of treatment all patients underwent dynamic multislice ct ( light speed 64 ct , ge medical systems , milwaukee , usa ) with triphasic technique ( 30 , 65 and 180 s ) administration of 125175 ml of 350 mgi / ml iodinated contrast medium , depending on body mass index , injected at a rate of 35 ml / s via automatic injector and followed by 2030 ml of saline solution . 
if necessary , conscious sedation was achieved with fentanyl or midazolam administered intravenously , and drug administration was modulated case by case . local anaesthesia of the insertion point was achieved with the administration of 10 ml of 2 % lidocaine . 
needle introduction was also guided by ceus in the case of iso - echogenic lesions or those poorly detectable with conventional ultrasound . needle size was made in relation to lesion width and desired safety margin ( at least 5 mm )  . 
the needle electrode was introduced under ultrasound guidance ( iu22 ultrasound system philips healthcare , best , the netherlands ) using a 3.5 - mhz convex probe ( c5 - 1 philips healthcare , best , the netherlands )  . 
at the end of the procedure , after automatic cooling of the rf system , the generator was reactivated to ablate the needle tract so as to prevent tumour dissemination . 
an unenhanced ct scan was performed at the end of each treatment . percutaneous laser ablation assessment of treatment effectiveness and follow - up percutaneous laser ablation ( pla ) was done with the echolaser xvg systethis system is composed of a mylab7070xv - l ultrasound scanner ( esaote biomedica , italy ) and an echolaser x4 laser generator ( esaote el.en. , florence , italy ) which uses a neodymium yttriumaluminiumgarnet light source , nd - yag laser , with a continuous wavelength of 1.064 lm 10 ninsertion of the bres within the lesion was performed using the method described by pacella et al . 
the bres were positioned in a square conguration with the tips placed 11.5 cm apart to obtain a correct ablation geometry and complete necrosis with a sufcient safety margin of at least 5 mchiba needles were inserted within the lesion using ultrasound guidance with a 3.5 - mhz convex probe ( ca621 , esaote biomedica , italy ) , through a single point of entry . 
their correct positioning was then evaluated with ct . each stylet was extracted and replaced with a exible , attip , sterile 300 - lm - diameter quartz bre with a bare tip . 
after treatment , the bres were retracted with the laser switched on so as to avoid possible tumour seeding . an unenhanced ct scan was performed at the end of each treatment . radiofrequency thermoablation radiofrequency thermoablation ( rfa ) was performed using an rf 3000 generator ( boston scientic corporation , natick , ma , usa ) , which provides a maximum power of 200 w . 
we used expandable 15to 17 - gauge leveen needles ( boston scientic corporation , natick , ma , usa ) with hook extension ranging from 2 to 5 cm in diameter . 
the image acquisition technique was the same as described for preprocedural evaluation . the pretreatment tumour volumes and the ablation lesion volumes were calculated on a ct console ( advantage workstation 4.3 ge medical systems , milwaukee , usa ) with the use of volume rendering reconstructions . the volumes were selected by means of manual segmentation using the images acquired during the arterial phase , in which the tumour mass was more easily visualised . subsequently , the same phase was used for the evaluation of the parenchyma after thermal ablation . 
the preand postprocedural images were then merged using the same eld of view and six translation and rotation parameters in three reformatting planes , to make them comparable . treatment response was evaluated according to the mrecist criteria [ 18 ]  . 
based on the ct results , tumour ablation and thus response to treatment were dened as complete ( cr , complete response ) when there was disappearance of all signs of lesion and no pathological enhancement was detectable on the edges of the area treated . 
ablation was considered partial or incomplete ( pr , partial response ) in the case of a partial destruction of the lesion , with a reduction of at least 30 % of the volume ; in the case of incomplete ablation , a second treatment was carried out during the following 2 weeks . patients with cr entered the follow - up programme , which included clinical evaluation and a - fetoprotein assay . three - phase dynamic ct at 3 , 6 and 12 months was performed in all patients . 
the medium - term results were assessed according to local progression of disease , meaning the presence of enhancement in proximity to the ablation site and the onset of new lesions at a distance . complications intraand postprocedural complications were evaluated according to the classication of the international society radiol med ( 2014 ) 119 : 298308 of radiology ( sir , society of interventional radiology ) [ 19 ] distinguishing between major complications ( events that lead to substantial morbidity and disability , an increase of care , hospitalisation or a longer hospital stay ) and minor complications . 
the presence of a postablation syndrome , dened as fever , nausea , vomiting and abdominal pain referred to the shoulder , was investigated during the rst 48 h after treatment . evaluation of tnfa production by peripheral blood cells for each treatment , blood samples were obtained 4 h before the beginning of the ablation procedure , and again 24 h and 5 days after the procedure . 
pbmc were cultured at a concentration of 2 9 106 for 18 h in 20 ng / ml of phorbol - 12 - myristate - 13acetate ( pma ) and 500 ng / ml ionomicine ( io ) ( calbiochem - novabiochem intl , la jolla ca )  . 
they were then resuspended at a concentration of 2 9 105 in 20 ll of buffered saline and incubated for 15 min with the monoclonal antibody cy - chrome - conjugated ( cy - chrometm ) anti - cd14 ( pharmingen , san diego , ca )  . 
tnfa production was evaluated cd14 ? tnfa ? cells compared to total cd14 ? cells . five healthy subjects , comparable in terms of age and sex with the two patient groups , were enrolled as controls . calculating percentage statistical analysis the nonparametric mannwhitney test and fischers exact test were used to compare the two treatment groups . 
therefore , a cr was obtained in 87 % of lesions treated with pla and 93 % of those treated with rfa , and a sufcient safety margin was obtained in all of these patients . 
the three patients who failed to achieve a cr , even after the second procedure , were treated with another type of procedure ( chemoembolisation )  . twenty - seven patients entered the follow - up programme of our study . 
in particular , these included pleural effusion ( 1 pla vs 4 rfa ) , perihepatic effusion ( 1 pla vs 3 rfa ) and subcapsular haematoma ( 1 rfa )  . 
4 a 74 - year - old woman affected by chronic hepatitis with hepatitis b virus ( hbv ) - related hepatocellular carcinoma ( hcc ) the level of hepatic segment vi treated with nodule located at percutaneous laser ablation . 
preprocedural computed tomography ( ct ) study : axial ( a ) and volume rendering image ( b ) show the size ( 20 mm ) and location of the nodule ( black arrow )  . 
5 a 69 - year - old woman affected by chronic hepatitis with hepatitis c virus ( hcv ) - related hcc nodule located at the level of hepatic segment vii treated with percutaneous laser ablation . preprocedural ct study : axial ( a ) and volume rendering image ( b ) showing the size ( 24 mm ) and location of the nodule ( black arrow )  . 
ct scan at 30 days : c axial image shows the success of the treatment and volume rendering image shows the size of the area of ablated tumour parenchyma compared to the volume rendering dimensions at preprocedural ct ( d )  . 
ct follow - up at 6 months : e , f axial images show disease recurrence below glissons capsule ( white arrow ) radiol med ( 2014 ) 119 : 298308 fig . 
preprocedural ct study : axial ( a ) and volume rendering image ( b ) show the size ( 23 mm ) and location of the nodule ( white arrow )  . 
 [ 23 ] in a study investigating the variables affecting local progression of disease , which indicates , however , a 3 - cm cutoff under which the best results are obtained . formation of an inadequate safety margin is one of the most signicant risk factors for local disease progression , and many authors agree that this margin should be between 5 and 10 mm [ 24 , 25 ]  . 
as a result , the lower survival rate seen in patients with tumours larger than 2 cm treated with pla may be justied by the absence of an adequate safety margin . this condition may be essentially due to the limited capacity to monitor tissue necrosis formation during treatment . ultrasound and ct are the most widely used low - cost imaging techniques used to monitor ablation procedures . however , the heating of tissue , which occurs during the 306 radiol med ( 2014 ) 119 : 298308 thermal ablation procedures , leads to the formation of gas which , while providing an indication of the tissue destruction , hinders evaluation with ultrasound [ 26 ]  . 
therefore , as it is impossible to use a lowcost imaging technique that is unaffected by this limit , local ablation systems have been developed to try to recreate a volume of tissue necrosis which is easily reproducible , using standard protocols that are independent of the monitoring technique used . 
therefore , a feedback system is necessary to enable tissue changes to be monitored during treatment , and in this sense rfa seems to have a signicant advantage over pla : the continuous recording of tissue impedance during rfa provides , albeit briey , the tumour ablation process . achieving power roll - off , which indicates tissue coagulation , can improve the effectiveness of the locoregional treatment itself [ 29 ]  . 
furthermore , an additional variable that can make it difcult to obtain a precise safety margin might be the relative difculty in placing multiple pla needles in the correct ablation geometry needed to induce an adequate and reproducible necrosis volume [ 23 ]  . 
moreover , the rigidity of the cirrhotic liver [ 30 ] can make it difcult to control the needle trajectory owing to the exibility of the needles , such as the pla needles used in our study , which have a smaller calibre ( 21 gauge ) than the rfa needles ( 1517 gauge )  . information about the main limitations of our study lie in the small size of the population sample ( 30 patients ) and the midterm follow - up ( 12 months )  . 
however , the possibility of carrying out a prospective randomised study , with no evidence of any statistically signicant difference between groups , allowed us to minimise possible bias in the statistical analysis . 
similarly , the fact that we focused on few variables , such as lesion size and type of treatment , made it possible and feasible for us to evaluate results as early as 1 year after treatment . 
in fact , the aim of our study was to evaluate the locoregional effectiveness of the single treatment , because the results of long - term evaluations are often not directly related to the effects of the treatment . 
indeed , especially in hcc , disease - free survival time and overall survival may be related to the aetiology and severity of the liver failure associated with cirrhosis and histological type of tumour . 
in contrast , the end point evaluated in our study , local disease progression - free survival or recurrence - free survival , could be considered a direct expression of the effectiveness of a locoregional ablation procedure [ 31 ]  . with regard to the evaluation of periprocedural complications , both techniques proved to be safe . 
in particular , asymptomatic perihepatic effusion was observed in four patients , pleural effusion in ve patients and subcapsular haematoma in one . these complications occurred more frequently in patients treated with rfa than with pla . 
in particular , in our study we documented the onset of a postablation syndrome in only one of the patients treated with pla , whereas 12 patients treated with rfa developed this syndrome . in this regard , we also examined the possible postprocedural increase of tnfa in the two treatment groups . tnfa is one of the possible mediators of a systemic inammatory response that can occur following treatment with rfa or cryoablation and is therefore one of the factors that inuence the occurrence of postablation syndrome [ 3436 ]  . 
 [ 34 ] , who evaluated the production of serum proinammatory cytokines , including tnfa , in a cohort of 13 patients with liver cancer subjected to pla under mr guidance . in our study , the nding that tnfa production did not increase might account for the lower rate of onset of postablation syndrome in patients undergoing pla . 
this higher concentration of tnfa in subjects treated with rfa may thus in part explain the more frequent occurrence of the postablation syndrome in the rfa compared to the pla group seen in our study . conclusions the ability to induce complete tumour necrosis did not show statistically signicant differences between the two ablation techniques ; however , for lesions with diameter c21 mm rfa yielded better results 1 year after treatment . a small number of minor complications were observed in patients treated with pla . 
morganti received : 20 september 2012 / accepted : 30 january 2013 / published online : 6 december 2013 ( cid : 2 ) italian society of medical radiology 2013 abstract objective this study was done to assess the impact of clinical factors and in particular the use of drugs for concomitant illnesses on late radiation - induced rectal bleeding in patients with prostate cancer . materials and methods patients with histologically proven prostate adenocarcinoma treated with radical radioleast 6 months were therapy and followed up for at selected . 
the correlation between late rectal bleeding and a number of factors was investigated by univariate and multivariate analysis . results a total of 278 patients who underwent radiotherapy at our institution between october 2002 and may 2011 were selected . 
if these results are reconrmed by larger clinical series , calcium channel blockers may be tested as radioprotector agents in clinical trials . keywords radiotherapy ( cid : 2 ) rectal bleeding ( cid : 2 ) radioprotector ( cid : 2 ) hypertension ( cid : 2 ) calcium channel blockers introduction prostate cancer is the most frequently diagnosed cancer in men [ 1 ]  . 
nevertheless , it is likely that the role of modern dose - escalated radiotherapy will further increase even in low and intermediate risk prostate cancer , since recent data suggest it could provide better biochemical disease - free survival than surgery in all risk classes [ 3 ]  . gastrointestinal and bladder complications represent the main limit to radiation dose escalation in prostate cancer . particularly rectal bleeding is the most commonly reported bowel toxicity , with a cumulative incidence of up to 50 % in 5 years in patients undergoing three - dimensional ( 3d ) dose - escalated radiotherapy [ 4 ]  . 344 radiol med ( 2014 ) 119 : 343347 in recent years , several results have demonstrated a clear correlation between rectal dose - volume histograms and the risk of rectal bleeding [ 5 , 6 ]  . 
in order to spare as much volume of rectum as possible while delivering higher radiation dose to the prostate , more advanced and often more expensive techniques , such as intensitymodulated image - guided radiotherapy ( igrt ) have been introduced in clinical practice , leading to a reduction in the risk of rectal bleeding [ 7 ]  . radiotherapy ( imrt ) besides dosimetric factors , also clinical variables such as previous abdominal surgery , presence of haemorrhoids , and use of antihypertensive medications can affect the risk toxicity after radiotherapy [ 8 ]  . 
although of late rectal arterial hypertension or the use of antihypertensive drugs seems to be protective for the development of late effects [ 8 , 9 ] , no clear effect has been shown for any specic antihypertensive drug . the objective of this analysis was to assess the impact of clinical factors and in particular the use of drugs for arterial hypertension on late radiation - induced rectal bleeding . 
the effects of several potentially confounding parameters ( comorbidity , abdominal surgery , radiotherapy dose and technique ) were also analysed . materials and methods study design patients with histologically proven prostate adenocarcinoma treated with either 3d conformal radiotherapy ( 3dcrt ) or imrt for radical intent and followed up for a minimum of 6 months were selected for this retrospective analysis . 
to this end , if no previous prostatectomy had been performed , patients had intra - prostatic gold ducials implanted . comorbidities , previous abdominal / pelvic surgery , use and type of drugs , previous / concomitant locoregional diseases , height and weight , were recorded before radiotherapy . 
rectal toxicity occurring during and within 3 months after the end of radiotherapy , was also recorded according to radiation therapy oncology group ( rtog ) criteria [ 11 ]  . the end of statistical analysis the correlation between late rectal bleeding and a number of factors was investigated by univariate and multivariate analysis . 
the following parameters were considered : body mass index ( [ or b30 ) , pre - treatment morbidities ( arterial hypertension , diabetes mellitus , chronic pulmonary disease ) , hormone therapy , drug prescription during radiotherapy ( use and / or anticoagulants ) , abdominal surgery prior to radiotherapy ( radical prostatectomy or other surgical procedures including rectum - sigma resection , kidney resection , cholecystectomy , appendectomy , prostatic adenomectomy ) , irradiation of pelvic nodes , delivered dose ( equivalent dose in 2 gy per fraction with a / b = 3 , eqd2 [ or b70 gy ) , and technique used ( imrt or 3dcrt )  . antihypertensives and type of standard time - to - event ( survival analysis ) methodology was used to assess the rst reported incidence of toxicity . events were timed from the end of radiotherapy , and the differences between the treatment groups were rst tested using the log - rank test . 
relative risks of late rectal bleeding according to treatment are summarised using hazard ratios from cox ( hr ) with 95 % condence intervals ( ci ) regression models . the difference of the incidence of grade c2 acute rectal toxicity between the treatment groups was assessed using the chi - square test with yates correction . results a total of 278 patients who underwent radiotherapy at our institution between october 2002 and may 2011 were selected for this analysis . 
even the presence of chronic pulmonary disease seemed to favour the development late rectal bleeding , although statistical signicance was not reached . biochemical disease - free survival was not affected by calcium blockers use or radiation dose . discussion in recent years many attempts have been made to protect the rectum against radiation damage by using topical or oral medications [ 1215 ]  . 
both misoprostol rectal suppositories [ 13 ] , and amifostine enemas [ 14 ] seem to exert some protective effect on late proctitis , while oral balsalazide appears to be effective in reducing the symptoms of acute proctitis [ 12 ]  . 
in this analysis , we found that the use of calcium channel blockers for arterial hypertension during and after radiol med ( 2014 ) 119 : 343347 radiotherapy may exert some protective effect against the development of rectal toxicity . 
although many authors have reported that arterial hypertension or antihypertensive medications may be protective for the development of late radiationinduced rectal effects [ 8 , 9 ] , this is the rst time a protective effect was shown for a specic antihypertensive drug . the potential use of calcium antagonists as radioprotectors was suggested by battaini et al . 
furthermore calcium channel blockers have antioxidant properties and have been shown to protect against free radical - mediated injury of cardiovascular cells [ 17 ] suggesting a possible mechanism for radioprotection . until recently , it was considered that the initial damage of the intestinal toxicity of irradiation was the destruction of epithelial stem cells within the crypts of lieberkuhn , causing the destruction and progressive failure of cell renewal , which explains the time delay between rectal mucosa irradiation and the onset of symptoms [ 18 , 19 ]  . more recently it has been suggested that an endothelial injury may occur before crypt stem cell damage in the evolution of the radiation - induced gastrointestinal syndrome [ 20 ]  . 
nifedipine , a calcium channel blocker , has been shown to improve endothelial function in patients with hypertension , at least partly , by enhancing endothelial thus preserving progenitor cell numbers and activity , endothelial integrity [ 21 , 22 ]  . in addition , calcium channel blockers are well tolerated and associated with minimal side effects [ 23 ] , the most common being ushing , headache , hypotension , and pedal oedema . 
adverse effects have been reported in approximately 17 % of patients using nifedipine , in 9 % of patients using verapamil , and in 4 % of those using diltiazem [ 24 ]  . although with the limits of a retrospective analysis , in our experience the use of calcium channel blockers resulted in a protective effect against late rectal bleeding . a recent systematic review of 11 published reports including 4 , 559 patients suggests there is at a minimum no difference , and in many cases superiority , imrt compared with 3dcrt for the radical treatment of localised prostate cancer in terms of acute and late gastrointestinal and genitourinary side effects in the setting of doseescalated ( [ 70 gy / 2 gy fractions ) radiotherapy [ 25 ]  . 
laparoscopy and histopathology anna lia valentini benedetta gui maura micco` maria carla mingote valeria ninivaggi maurizio guido gian franco zannoni eleonora marrucci lorenzo bonomo received : 21 january 2013 / accepted : 20 may 2013 / published online : 3 december 2013 ( cid : 2 ) italian society of medical radiology 2013 abstract objective to verify whether the capability of magnetic resonance imaging ( mri ) in diagnosing deep inltrating colorectal endometriosis ( dice ) is improved using an association of mri ndings . methods and materials the imaging database of our institute of radiology was retrospectively reviewed to identify patients subjected to mri for a suspicion of deep inltrating endometriosis . 
gemelli 8 , 00168 rome , italy the rst section and the second criterion in the second one . mri results were compared with la or histopathology as the gold standard by 2 9 2 tables and statistically analyzed ( k statistics )  . 
likelihood - ratio test was also performed , being independent from the prevalence of the disease . results by consulting case sheets , 33 / 50 females ( ranging age 2439 years , mean age 32.2 years ) who were subjected to mri also underwent la . 
intestinal resection for dice was performed in 11 / 33 patients ; in 22 / 33 supercial intestinal foci , adhesions / nodules in the fat plane were simply removed . 
among the imaging techniques employed in the preoperative evaluation of deep inltrating colorectal endometriosis ( dice ) , transvaginal or transrectal ultrasound as well as computed tomography enteroclysis has been used [ 3 , 4 ]  . 
however , they are limited by the small eld of view and radiation exposure , respectively . magnetic resonance imaging ( mri ) is employed to investigate chronic pelvic pain in women [ 5 ] and is currently used in the assessment of deep endometriosis [ 68 ]  . 
applied lters were : interval technique , mri ; udc ( cost - centre diagnostic unit ) , gynaecology ; uld ( logistic diagnostic unit ) , dysfunctional gynaecological unit ( endometriosis clinic )  . 
the radiologists assessing the mri data were not aware of the patients clinical symptoms or outcome . mri technique the mri protocol applied in our department for the investigation of suspected pelvic endometriosis involves the use of a 1.5 - t superconducting magnet ( vectra , ge medical systems , milwaukee , usa ) with a phased - array coil and no rectal distension . 
to limit intestinal peristalsis and to attenuate uterine contractions , patients receive an intramuscular injection of 1 mg of hyoscine nbutylbromide ( buscopan , schering , berlin , germany ) before the examination and are always studied after the 8th day of the menstrual cycle , to better identify hyperintense bleeding lesions . axial t1 - weighted spin echo images , axial coronal and sagittal t1 - weighted gradient - echo images with fat suppression ( to better evaluate hyperintense bleeding lesions ) , axial , coronal and sagittal t2 - weighted fast spin echo images and axial t2 - weighted fast spin echo images extending to the upper abdomen ( to evaluate hydronephrosis ) are always obtained . 
dynamic axial and delayed phase sagittal images acquired with lava ( liver acquisition with volume acquisition ) sequence ( 3d t1 - weighted gradient echo ) after intravenous injection of gadoliniumbased contrast material are employed in selected cases . 
in particular , lava sequences with fat saturation are usually employed when endometriomas exclude degeneration , or also in the case of adenomyosis to verify the grade of inltration of the myometrial surface . this study was retrospective and images after contrast medium injection ( gadobenate dimeglumine , multihance 0.5 m , bracco , milan , italy ) were not always available . 
for this reason and since no signicant benet of intravenous gadolinium has been reported in the literature for deep pelvic endometriosis [ 8 ] , the mri evaluation was performed only on the t2 - weighted images . 
both types of lesions can be found in the fat plane adjacent to the bowel wall in the case of deep endometriosis , such as fresh nodules in the recto - vaginal septum or brotic lesions at the uterine torus . 
bowel wall thickness was not evaluated in terms of millimetres , as it is a relative rather than absolute evaluation , related to the morphology of the near proximal and distal portion of the same intesthickness of the bowel wall tinal segment . 
the term radial and retracting shape can be considered a 1.5 - t version of the mushroom cap sign [ 2 ] and resembles the fan shape conguration of the bowel wall , as recently described at 1.5 - t imaging for the diagnosis of dice [ 11 ]  . to assess what association of signs improves dice diagnosis , mri evaluation was carried out twice by two radiologists with 10 and 15 years of experience in female pelvic mri , who reviewed the images in consensus in two separate sessions . 
in the rst evaluation ( rst diagnostic criterion ) , any general thickness of the bowel wall combined with nodules or plaque - like lesions in the adjacent fatty plane was considered abnormal , while in the second evaluation ( second diagnostic criterion ) , only the characteristic radial and retracting shape of the thickened bowel wall was considered abnormal when associated with nodules or plaque - like lesions in the adjacent fatty plane . when no nodule or plaque - like lesion was identied in the adjacent fatty plane , the presence of bowel thickness , even without adjacent fat - plane interface , was always considered a normal result . 
la or histopathology specimens in the case of surgical resection were taken as the gold standard . reference standard and statistical analysis la was always performed at the hospital by a single skilled gynaecological surgeon specialised in endometriosis who was assisted by an intestinal surgeon in the case of bowel resection . supercial , or serosal , involvement of the bowel was directly diagnosed by la visualisation and was treated by supercial excision , serosal shaving and adhesion removal . dice was suspected in the event of large or disc - like implants retracting the wall and was treated by segmental bowel resection . all surgical specimens were sent to the hospitals histopathology service and were xed in 10 % formalin for 24 h . 
the diagnosis of endometriosis was made on the basis of the presence of endometrial - type epithelium and endometrial stroma on bowel resection specimens . the mri results in dice diagnosis obtained using the two previously described criteria ( see mri data ) were compared by 2 9 2 tables with the gold standard histopathology in the case of bowel resection for dice . 
comparison of mri results with la was used in patients not subjected to bowel resection because of the absence of disease or presence of supercial foci ( no dice ) and were statistically analysed ( k statistic )  . 
the likelihood ratio test was also applied , being independent of the prevalence of disease . results thirty - three patients ( age range 2439 years ; mean age 32.2 ) met the inclusion criteria . 
first criterion : absence or presence of generally thickened intestinal wall surrounded by fat - plane interface represents a normal result ( no deep inltrating colorectal endometriosis ) ; the simultaneous presence of nodules or hypointense plaque - like lesions in the fat plane and is an abnormal result ( deep generally thickened intestinal wall inltrating colorectal endometriosis )  . 
the better diagnostic performance of the second diagnostic criterion was also conrmed with the likelihood ratio test . to our knowledge , the overall accuracy of t2 - weighted mri is higher in this study ( 97 % ) than in other published reports on the same subject ( 7596 % ) [ 4 , 6 , 7 , 10 , 11 ]  . some reports identied a typical mri morphology of the intestinal wall thickness in the case of dice : the mushroom cap sign was rst reported at 3.0 - t magnet imaging [ 2 ] , but it was not statistically validated because of the small number of patients in that series . 
taking into consideration a combination of signs , or the contemporary presence of nodules or plaque - like lesions in the adjacent fat - tissue plane and the typical bowel thickness morphology for the correct assessment of dice , as this study suggests , can be justied by the course of the disease . 
even if retracting adhesions and muscle layer invasion are responsible for in a typical producing the protrusion which results semicircular morphology of the involved intestinal tract variously known as the mushroom cap sign , the fan shape image or the radial and retracting shapeit should be noted that dice is improbable when no nodules or plaque - like lesions are detectable in the fat - tissue plane closely adjacent to the bowel wall . 
the results of this study conrm the usefulness of this association of signs . including pelvic pain , colorectal endometriosis can cause severe intestinal symptoms , rectal bleeding and problems with defaecation , but needs to be surgically treated by intestinal resection only in the deeply inltrating type , since brosis invading the intestinal wall muscularis does not respond to medical therapy and advanced disease can be complicated by lumen obstruction [ 8 ]  . 
supercial endometriosis lesions located on the serosa surface are not easily evaluated by imaging [ 2 ] , but are negligible since they do not require bowel resection and are usually diagnosed and simply removed during la . 
in the past , the imaging evaluation of colorectal involvement due to endometriosis was especially assessed by dcbe , which seems to correlate with the patients clinical history and clinical ndings and was shown to be capable of detecting bowel wall involvement requiring intestinal surgery [ 9 ]  . 
recently , some reports have demonstrated the ability of mri to detect dice using t2 - weighted images without or with air , 296 radiol med ( 2014 ) 119 : 291297 defaecation problems . 
2 deep inltrating endometriosis of the rectosigmoid juncsuffering from chronic pelvic tion in a 32 - year - old patient pain histopathology . t2 - weighted sagittal mri a shows thickened rectosigmoid junc ( a white tion wall showing radial and retracting shape arrows ) and adhesions ( a void arrow ) which converge on the the uterine torus , as shown hypointense plaque - like lesion at on the t2 - weighted axial fat - saturated image ( b arrow )  . 
histopathology specimen after bowel inltrating type of colorectal endometriosis showing endometrial typical glands ( white arrow ) and stroma ( white star ) within the muscular layer ( void star ) of the large bowel . 
t2 - weighted sagittal mri a shows a thickened colorectal junction wall typically showing a radial and retracting shape ( white arrows ) associated with hypointense plaquelike lesion at the uterine torus ( black arrow )  . 
u uterus , rsj rectosigmoid junction radiol med ( 2014 ) 119 : 291297 water or gel distension of the rectum [ 2 , 7 , 13 , 14 ] , employing contrast - enhanced mri [ 8 ] or mr colonography [ 4 ] or also using 3.0 - t superconductive magnets [ 2 , 13 ]  . 
by contrast , mri is an all - in - one examination able to detect endometriotic foci in different sites , including the colorectal site [ 4 , 6 , 7 , 10 , 11 ] , as well as remaining the examination of choice for the detection of deep pelvic implants [ 4 ]  . 
patient management is improved by using a preoperative assessment of the disease by mri , as decisions to perform intestinal surgery will involve the need for a colorectal surgeon . the retrospective analysis of data could be considered a limitation of this study . 
however , it should be noted that mri and la , as well as the histopathological evaluation , that mri was were always performed at always carried out by the same pool of radiologists using the same study protocol , and that the mr images were reviewed by the same two radiologists with 10 and 15 years of experience in female pelvic mri , who were not aware of the patients specic symptoms and outcome . the hospital , in conclusion , the contemporary presence of nodules or hypointense plaque - like lesions in the fat - tissue plane and thickened intestinal wall characteristically showing a radial and retracting shape improves mri capability in dice diagnosis . 
di mola received : 17 october 2012 / accepted : 17 march 2013 / published online : 12 march 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract purpose a tumour score for venous invasion in patients with pancreatic adenocarcinoma was evaluated by means of computed tomography ( ct ) , in order to improve the assessment of medical treatment and clinical outcome with special attention to borderline resectable disease . materials and methods fifty - six consecutive patients who underwent curative surgical resection for pancreatic cancer were analysed . 
on the basis of ct criteria , tumour involvement of the portal vein ( pv ) and superior mesenteric vein ( smv ) was graded according to an adapted 4 - point scale : score 1 , denite absence of invasion ; score 2 , probable absence of invasion ; score 3 , probable presence of invasion ; score 4 , denite presence of invasion . 
correlations between the venous inltration scores and the patients clinical features were also evaluated . results after radiological evaluation of pv and smv grades of inltration , 21 / 56 ( 37 % ) and 37 / 56 ( 66 % ) patients , respectively , were found to have borderline resectable disease . 
the 4 - point scale achieved a sensitivity of 80 % , a specicity of 96 % and an accuracy of 93 % in the evaluation of the pv , and a sensitivity of 100 % , a specicity of 94 % and an accuracy of 95 % in the evaluation of the smv . 
di mola unit of surgical oncology , g bernabeo hospital , ortona , italy radiol med ( 2014 ) 119 : 334342 keywords pancreatic cancer ( cid : 2 ) vein inltration ( cid : 2 ) prognostic factors ( cid : 2 ) ct scan ( cid : 2 ) borderline resectable lesion abbreviations smv superior mesenteric vein computed tomography portal vein introduction pancreatic carcinoma represents the fourth leading cause of death due to malignant disease [ 1 ]  . 
surgical unresectability may include metastatic disease of the liver and peritoneum , invasion of contiguous structures ( stomach , colon , spleen , left adrenal , kidney or spine ) , invasion of peripancreatic arteries ( common hepatic / proper hepatic artery ; superior mesenteric artery ; celiac axis ) [ 3 ]  . 
otherwise , primary pancreatic cancers with radiological characteristics suggesting limited involvement of the superior mesenteric vein ( smv ) , portal vein ( pv ) , superior mesenteric artery ( sma ) , or celiac axis in the absence of metastatic disease have recently been dened as borderline resectable [ 4 , 5 ]  . 
in addition , considering the involvement of the smv / pv , the impingement and narrowing or segmental venous occlusion should enable a sufcient venous ow above and below the occlusion in order to allow surgical venous reconstruction . with regard to borderline resectable cancers , venous invasion remains a controversial point for pancreaticoduodenectomy , and one of the most difcult steps in preoperative staging is to determine local resectability and to dene a stage - specic therapy [ 6 ]  . 
in addition , in patients with clear venous involvement ( either borderline resectable or locally advanced unresectable ) , the tumour can often be reduced in size and converted to an anatomically resectable lesion with preoperative neoadjuvant therapy , strongly increasing the likelihood of subsequently achieving an r0 resection [ 59 ]  . 
in some cases , tumour ingrowths into the adjacent vessels might be detected only at a late phase of the surgical procedure . spiral computed tomography ( ct ) allows for improved imaging of the pancreas and peripancreatic vessels and is regarded as the most important non - invasive staging technique [ 1315 ]  . 
the accuracy of spiral ct for predicting vascular invasion ranges from 62 to 92 % , suggesting that a lack of complete agreement with regard to vascular inltration exists [ 18 , 19 ]  . in this study we aimed to evaluate a multiparametric score for venous tumour inltration ( portal and superior mesenteric veins ) using multidetector spiral ct , and to assess its inuence on medical treatment and clinical outcome , especially in patients with borderline resectable pancreatic cancer . materials and methods patient population we searched the pathology databases in our electronic medical records system from may 2004 to june 2009 for patients with pathologically proven pancreatic adenocarcinoma . 
in order to have pathologically proven diagnoses associated with intraoperative ndings conrming or not the venous involvement , we included in the analysis 56 consecutive patients who underwent radical surgical resection due to pancreatic cancer ( 23 female , 33 male ; median age 64 years ; range 3582 years )  . tumour localization was pancreatic head ( n = 45 ) , uncinate process ( n = 1 ) , body ( n = 5 ) and in ve patients the tumour involved the head and body or the body and tail as a borderline tumour . 
according to the international classication of the uicc ( union for international cancer control ) there were four , stage ia ; two , stage ib ; 13 , stage iia ; 32 , stage iib ; four , stage iii ; and one , stage iv cancers . pylorus - preserving pancreaticoduodenectomy was performed in 45 patients , left pancreatectomy in 7 and total pancreatectomy in 4 patients . 
nineteen ( 34 % ) patients underwent venous resections due to macroscopic vascular inltration : 10 portal vein ( pv ) and 9 superior mesenteric vein ( smv ) resections . the study was conducted with the approval of the ethics committee of all centres involved in the study and written informed consent was obtained from each patient . 336 ct imaging protocol all examinations were performed with a 16 - row spiral ct system ( siemens somatom sensation 16 , erlangen , germany )  . 
our hydro - ct techniques included intravenous injection of 40 mg n - butyl scopolamine bromide ( buscopan ) for intestinal paralysis , gastric and duodenal wall distension by oral administration of an average of 1.5 l tap water , and right anterior oblique ( rao ) patient positioning [ 16 , 20 ]  . 
then , for arterial and portal phases , we used the care - bolus technique with 120 ml contrast medium ( 5 ml / s , ultravist 370 , bayer )  . 
the arterial ( delay of 8 s after the threshold ) and portal ( delay of 35 s after the threshold ) phases were performed with the following protocol : detector collimation , 0.75 mm ; table speed , 12 mm / rotation ; slice , 3 mm ; 170 mas , 120 kvp . 
in both phases two secondary reconstructions ( 2 and 3 mm ) were performed . image analysis radiol med ( 2014 ) 119 : 334342 table 1 score of venous inltration using computed tomography ( ct ) criteria grade tumour contact with vessel length of tumour contact with vessel circumferential vein involvement stenosis = 0 mm = 0 ( cid : 3 ) no stenosis = 0 ( cid : 3 ) 90 ( cid : 3 ) = 0 ( cid : 3 ) 90 ( cid : 3 ) no stenosis flattened [ 90 ( cid : 3 ) \180 ( cid : 3 ) [ 180 ( cid : 3 ) occlusion thrombus grade grade c \5 mm [ 5 mm grade grade d [ 5 mm grade e or f 1 denitely absence of invasion 2 probably absence of invasion 3 probably presence of invasion 4 denitely presence of invasion type of stenosis : no stenosis attened occlusion thrombus . images were reviewed retrospectively and independently by two abdominal radiologists with 10 years of clinical experience . the criteria considered for venous invasion were : tumour contact with vessel , according to loyer et al . [ 21 ] : grade a : fat plane visible between tumour and vessels grade b : normal pancreatic tissue between tumour and vessels grade c : tumour adjacent to vessel with a convex contour towards vessels grade d : tumour adjacent to vessel with a concave contour towards vessels grade e : circumferential involvement of vessels grade f : vascular occlusion . a 4 - point scale was devised as follows ( table 1 ) : 1 . 
denite absence of invasion : tumour contact = grade ab , length of tumour contact = 0 mm , circumferential involvement of vein = 0 ( cid : 3 ) , no stenosis ; 2 . 
probable absence of invasion : tumour contact = grade c , length of tumour contact \5 mm , circumferential involvement of vein = 0 ( cid : 3 ) 90 ( cid : 3 ) , no stenosis 3 . 
denite presence of invasion : tumour contact grade e or f , circumferential involvement [ 180 ( cid : 3 ) ; narrowing of vessel ; association of tumour convexity d with length [ 5 mm and circumferential [ 90 ( cid : 3 ) \180 ( cid : 3 )  . length of tumour contact with vessel : statistical analysis circumferential involvement of vein : 0 mm \5 mm [ 5 mm . 0 ( cid : 3 ) 0 ( cid : 3 ) 90 ( cid : 3 ) 90 ( cid : 3 ) 180 ( cid : 3 ) [ 180 ( cid : 3 )  . sensitivity , specicity , positive and negative predictive values for vascular involvement were calculated for each reader separately . 
spiral computed tomography ( ct ) ( a , b ) shows a tumour in the pancreatic head with evident fat plane between dilated pancreatic duct and pv ( grade a ) ( arrow ) , without contact between the tumour and vein , which was conrmed intraoperatively ( c )  . 
spiral ct shows a tumour of the pancreatic head ( red arrow ) with a convex contour towards vessel ( grade c ) ( black arrow ) and a grade of contact between 0 ( cid : 3 ) and 90 ( cid : 3 )  . 
spiral ct shows a tumour in the pancreatic head and body with a attened vessel wall ( arrow ) and a length of contact [ 5 miv 52 - year - old man with score 4 . 
spiral ct shows a thrombus ( arrow ) in the conuence between the pv and the splenic vea 75 - year - old man with score 4 ( a )  . 
spiral ct shows a tumour in the head of pancreas with narrowing of pv before the conuence with splenic vein ( b ) radiol med ( 2014 ) 119 : 334342 fig . 
a 66 - year - old man with tumour of the pancreatic head . we evaluated the pv as score 3 ( ab ) ( grade c , length of tumour contact [ 5 mm and attened ) but the surgical results ( c ) demonstrated that the vein was not inltrated but only attached by an inammatory adhesion . 
statistical associations between the patients characteristics ( age , gender , tumour location , grading , tumour staging , classication and status of resection margins ) and each score of venous inltration were assessed using the fisher exact test and the kruskal wallis test for categorical and continuous variables , respectively . 
time - to - event analyses for overall survival ( dened as the time between the diagnosis and the occurrence ) was performed using the kaplanmeier ( km ) method and by log - rank test . 
all analyses were performed using sas release 9.1 ( sas institute , cary , nc , usa )  . results image analysis portal vein there was a high agreement between two readers ; the k value was [ 0.80. evaluation of the pv on the ct images dened 21 / 56 ( 37 % ) as borderline resectable cases . 
we evaluated the pv as score 2 ( ab ) ( tumour convexity grade c , length of tumour contact \5 mm , circumferential involvement of vein = 0 ( cid : 3 ) 90 ( cid : 3 ) , no stenosis ) but surgical exploration demonstrated that the vein was inltrated and a pv en bloc resection was required ( c ) table 2 radiological evaluation of portal vein and superior mesenteric vein inltration using the 4 - point scale 80 % sensitivity , 96 % specicity , 80 % positive predictive value ( ppv ) , 96 % negative predictive value ( npv ) and 93 % overall accuracy ( table 2 )  . true positive true negative false positive false negative accuracy ( % ) sensitivity ( % ) specicity ( % ) ppv ( % ) npv ( % ) pv portal vein , smv superior mesenteric vein , ppv positive predictive value , npv negative predictive value had denite absence of invasion ( score 1 ) , 11 patients had probable absence of invasion ( score 2 ) , 7 patients had probable presence of invasion ( score 3 ) and 3 patients had denite presence of invasion ( score 4 )  . 
in particular , the absence of vascular inltration was then subsequently proved during surgical intervention in 96 % of the cases ( 44 / 46 ) , while portal vein inltration was present during surgical intervention in 80 % of the cases ( 8 / 10 )  . 
using this score for the evaluation of pv inltration and in comparison with the intraoperative assessment , the results were : superior mesenteric vein evaluation of the smv on the ct images classied 37 / 56 ( 66 % ) as borderline resectable cases . in detail , 19 patients had denite absence of invasion ( score 1 ) , 25 patients had probable absence of invasion ( score 2 ) , 6 patients had probable presence of invasion ( score 3 ) and 6 patients had denite presence of invasion ( score 4 )  . 
in detail , the number of patients without evidence of metastasis to distal organs ( m0 ) was higher in patients with low smv scores than in those with high smv scores ( p = 0.028 ) : 56 , 72 , 17 and 17 % of patients with smv scores 1 , 2 , 3 and 4 , respectively . 
score 34 : hr = 0.30 ; 95 % ci 0.051.75 , p = 0.183 and hr = 0.28 ; 95 % ci 0.041.88 , p = 0.192 from univariate and multivariate cox regressions , respectively ; score 2 vs . 
however , this classication is relatively subjective and authors do not differentiate between venous and arterial invasion . we have revised those criteria , including in only one group ( score 1 ) grade a ( fat plane visible between tumour and vessels ) and grade b ( normal pancreatic tissue between tumour and vessels ) because in our opinion there are not many differences between these two grades in terms of surgical outcome since both are clearly resectable . in addition , we have considered also the length of contact between the tumour and vascular wall . 
 [ 25 ] evaluated isolated ct criteria and a combination of two criteria for venous invasion in 65 patients who underwent surgery for pancreatic cancer , considering length of tumour contact , degree of stenosis , circumferential involvement of vein , irregularity of the vessel margin and tumour convexity towards the vessel . 
they concluded that narrowing of the smv and pv seems the most reliable criterion , as well as circumferential involvement of the pv [ 90 ( cid : 3 )  . 
the best combination , however , was tumour concavity with circumferential involvement [ 90 ( cid : 3 ) , with a sensitivity of 60 % and a positive predictive value of 90 % . 
in this study a length of tumour contact [ 5 mm with pv and smv had a sensitivity of 47 and 57 % and a specicity of 80 % , respectively . 
it is worth noting that in order to ensure that the radiological scores were in line with the intraoperative ndings of venous inltration ( associated with the histological report ) we included only patients who underwent radical surgical pancreatic resection . in addition , klauss et al . 
by using this score we have improved the sensitivity , specicity , ppv and npv , with a good correlation with surgical results especially when we considered the group of borderline resectable tumours . 
patients with pv score 34 had shorter survival ( median survival = 10 months ) as compared to those with pv score 1 ( median survival = 13 months )  . log - rank test p value = 0.106 discussion many studies report that multidetector spiral ct has improved pancreatic tumour detection , with an overall accuracy between 89 and 97 % [ 1517 ]  . 
 [ 21 ] have classied tumour contact as forming either a convexity or a concavity against the vessel wall : six different types ( af ) of tumour contact to major vessels ( both veins and arteries ) were described . 
these data suggested that if the tumour is radiologically found in contact with vessels without inltrating the vessel wall , it is 342 radiol med ( 2014 ) 119 : 334342 these data are of interest in addition , when we compared the pv and smv inltration scores with the patients clinical characteristics we found that both scores were associated with metastatic disease and status of resection margins . 
although not surprising , if we consider that sometimes the tumour may be locally resectable but the disease has rapid progression after surgery maybe due to the presence of microscopic metastasis at diagnosis . 
moreover , although it is difcult to imagine that a radiological score might be related to disease - free survival , the log - rank tests suggested that pv inltration scores might correlate with the patients overall survival . 
these data might at least suggest that the present score system is reliable and must be tested in a large number of patients . in conclusion , smv and pv scores can predict resectability , and their correlation with tumour metastatic state and resection margins conrms their reliability in pancreatic cancer . conict of interest tiziana marinelli , antonella filippone , francesca tavano , andrea fontana , fabio pellegrini , jorg koninger , gotz m . 
survival is slightly but steadily increasing , thanks to the early diagnosis of mets and to the availability of new systemic therapies [ 1 ]  . a limit to the usefulness of local treatments of hepatic mets from breast cancer is therefore a tendency towards systemic metastases ( unlike , for example , mets from colorectal carcinoma which tend to affect the liver in an exclusive manner ) [ 2 ]  . therapeutic options include chemotherapy but also metastasectomy and radiofrequency ablation ( rfa ) in selected patients [ 3 ]  . 
until now , hepatic rfa was used primarily for the treatment of hepatocellular carcinoma and mets from colorectal cancer , but a small number of reports also 328 radiol med ( 2014 ) 119 : 327333 concern mets from breast , stomach , kidney and lung carcinoma , and from cholangiocarcinoma and melanoma [ 5 ]  . the aim of this study was to review our personal series of consecutive rfa of hepatic mets from breast cancer , performed on the basis of a multidisciplinary clinical indication , to evaluate the midterm safety , efcacy and clinical utility of this therapy . materials and methods our series is taken from a consecutive series of nearly 1 , 000 rfa procedures performed on mets from breast cancer at the two centres of our academic institution from 1998 to 2011 . includes 45 women ( age range 3381 years ; mean 55 years ) with metastatic disease from breast cancer . 
the study was carried out in accordance with the guidelines for retrospective reviews established by our institutional review board . patients and lesions the indication for treatment was given after multidisciplinary assessment by a medical oncologist , an intervenradiologist and an anaesthesiologist . 
the rfa tional technique was established on the basis of the technical evaluation of the interventional radiologist . the alternative option to surgery was chosen for the following reasons : oncological therapeutic strategy , contraindications to surgery or anaesthesia ( cardiovascular , respiratory , etc . ) , other comorbidities , advanced age , presence of extra - hepatic disease , lesions not surgically resectable , refusal of the patient to undergo surgery . a total of 87 mets were treated in 45 patients ( mean age 56 years ; average 1.9 mets per patient )  . 
six of 45 ( 13 % ) cases were already metastatic at diagnosis of the primary tumour ( synchronous mets ) ; 18 / 45 ( 40 % ) patients also had extra - hepatic mets , already controlled or treated with other therapies . 
the size of the lesions ranged from 10 to 45 mm , with an average of 23 mm . at the time of selection for rfa treatment , breast cancer histology was not considered a selection criterion , nor were previous or current systemic therapies . 
this , because we privileged the potential usefulness of the local treatment in the management of the single patient with a specic stage of disease ; rfa was therefore included as an adjunctive treatment in a constantly multimodal therapy . histology and other treatments were therefore not correlated with the results of rfa . pre - procedural assessments before each treatment , we evaluated age , performance status and cardiorespiratory condition . 
in addition , preprocedural staging with whole - body computed tomography ( ct ) , magnetic resonance ( mr ) imaging , and / or positron emission tomography ( pet ) ct , preferably not earlier than 1 month before the scheduled date for the rfa procedure was always requested . 
each patient underwent coagulation tests ( for possible correction of thrombocytopenia or increased inr / ptt ) , a chest x - ray and electrocardiogram , and an anaesthesiological assessment . 
any anti - coagulation or anti - platelet treatments were adapted or suspended . the indication , risks and potential benets of the procedure were discussed with the patients , who provided written informed consent . procedural aspects rfa was performed in the interventional radiology room , in conditions of local sterility after injection of a local anaesthetic at the site of entry of the needle - electrode ( 10 ml of buffered lidocaine hydrochloride 2 % ) and under anaesthesiological monitoring ( ecg , blood pressure , arterial oxygen saturation ) and analgosedation . all procedures were performed under ultrasound guidance , using esaote technos and mylab scanners ( genoa , italy )  . 
in the case of isoechoic mets , visualisation of the lesion and monitoring of electrode insertion was carried out after intravenous administration of second - generation ultrasound contrast agent ( sonovue , bracco , milan , italy )  . we used expandable needle - electrodes rita starburst ( rita medical systems , inc . , mountain view , ca , usa ) or leveen ( boston scientic , waltham , ma , usa )  . 
it is well known that the ablation protocol is based on temperature for the rita system and tissue impedance for the boston scientic system , so the choice of equipment was linked to their availability rather than to other variables . the average time for each rfa procedure was approximately 20 min , with differences imposed by the size of the radiol med ( 2014 ) 119 : 327333 mets and the different equipment protocols , in accordance with the manufacturers indications . prognostic factors for survival , one of them being maintained local effectiveness ( ca ) : at the end of the procedure , the electrode pathway was ablated during extraction , in order to avoid neoplastic seeding and to achieve haemostasis ; after about 15 min a nal post - procedural ultrasound scan was obtained to exclude immediate complications . patients were kept under observation for one night after the treatment in order to monitor their clinical condition and complete blood count . evaluation of adverse events all adverse events were recorded and categorised according to the society of interventional radiology ( sir ) criteria into minor complications ( low or no clinical relevance ) and major complications ( requiring prolonged hospitalisation and / or interventional radiological or surgical intervention ) , and counted in terms of numbers and percentages . outcome even considering that the clinical goal of rfa was the multimodal management of breast cancer mets rather than achieving local results with radical intent , we considered it useful to assess the outcome at 1 month by means of contrast - enhanced ct to identify any partial ablation ( pa ) with residual tumour tissue . 
where the examination indicated complete ablation ( ca ) , given the high probability of local progression in rfa of liver mets , the ablation site was re - assessed with contrast - enhanced ct 1 year after the treatment in order to verify possible maintained ca and diagnose local recurrences . 
for the assessment of clinical utility , the number of deaths in the studied population was counted . possible local or clinical outcomes of disease were : no evidence of residual / local recurrence ( ca ) , evidence of local residual tumour tissue ( pa ) , evidence of local recurrence ( lr ) , death . on the basis of these parameters , we were able to calculate : the local effectiveness ( ca versus pa ) at initial ct follow - up ( ca versus pa ) and 1 year after the procedure ( ca versus pa ? lr ) , time to progression ( ttp ) , and survival curves in the medium term . also on the basis of our previous experience with rfa of liver mets , we analysed the size of the lesion ( lesion diameter and a threshold diameter of 30 mm ) as potential prognostic factors for local effectiveness at 1 year . given the greater importance of evaluating the clinical impact of the procedure , we analysed several possible single or multiple lesions at the time of treatment , m0 / m1 at the time of diagnosis , absence or presence of extra - hepatic mets , size of the lesions , maintained effectiveness of rfa versus treatment failure ( tf ) at 1 year . statistical analysis all variables were inserted in a microsoft ( microsoft , inc . , redmond , wa ) excel spreadsheet . 
in particular , to identify possible correlations between dimensional variables and local outcome , we applied a multivariate analysis ( the unpaired two - tailed t test to compare averages and the fisher exact test to assess the signicance of threshold diameters ) ; kaplan meier survival curves were stratied based on the variables described above with signicance of the differences being calculated using a multivariate analysis ( cox )  . results complications the periprocedural mortality was nil . 
the rst was a case of protracted pain with evidence of thrombosis of the left portal branch , while the other was a case of sepsis due to serratia temporally related to the procedure . local effectiveness the initial ct follow - up revealed ca in 90 % of cases ( 78 / 87 )  . 
1 mean diameter ( sd ) of metastases ( mets ) with complete ablation ( ca ) maintained 1 year after radiofrequency ablation ( rfa ) ( 22 7.4 mm ) compared with mean diameter of those with treatment failure ( tf ) [ partial ablation ( pa ) or local recurrence ( lr ) ] ( 30 10 mm ) : at the statistical test the difference was considered extremely signicant ( p = 0.0005 , hr 7 , 965 , 95 % ci 3 , 64612 , 284 ) fig . 
more than 50 % of women with breast cancer develop hepatic mets , but only 518 % of patients have metastatic disease conned to the liver [ 7 ]  . 
metastatic breast cancer should therefore be treated by chemotherapy and / or hormone therapy , both standard systemic therapies [ 8 ] , and even so reported survival rarely exceeds 2 years [ 9 ]  . considering the toxicity of chemotherapy , it is increasingly common for patients with limited hepatic disease ( onset or residual after standard therapy ) and controlled extra - hepatic disease , to require a local treatment to be integrated within a broader therapeutic strategy , in a socalled multimodal approach . 
the majority of patients , however , are not eligible for surgery due to the oncologists or the patients decision based on general condition , age , advanced state of the disease or other contraindications . for this reason , in recent years there has developed an increasing interest in ablative therapies , with the aim of managing a given stage of the disease and the hope of improving the prognosis of the patients . in our series , the indications for hepatic rfa were based on what has been said so far . 
similar to previous studies , we therefore rst evaluated the complications and the effectiveness of local rfa , intended as ca demonstrated at contrast - enhanced ct at initial and medium term follow - up . 
with regards to local effectiveness , our results at initial ct follow - up ( 90 % ca ) were broadly in line with those in the few studies reported in the literature , in which ca varies from 79 to 96 % [ 8 , 1014 ]  . 
it was not possible to nd published results comparable with our data ( 74 % ) regarding the local effectiveness ( maintained ca ) at 1 year . in the search for factors that inuence local effectiveness , the literature lists several variables , including the size of the tumour and its proximity to the branches of greater calibre of the hepatic veins and the portal vein [ 15 ]  . 
apart from having limited signicance due to the small size of the sample , interpret : given the nonstatistical signicance of maintained ca as a predictor of survival at 3 years , it seems that survival may depend more on other variables , such as ineffectiveness of systemic therapy and the resulting generalised tumour progression . 
in fact , the vast majority of patients died due to progression of extra - hepatic disease , even though almost all of them underwent systemic therapies until these proved ineffective to stop the disease ( or had to be interrupted due to toxicity )  . these results are difcult thus , considering hepatic rfa as a local therapy that is useful for managing a given stage of metastatic disease , we can conclude with two further considerations . 
as previously mentioned , a large proportion of patients is not eligible for surgery , and a review of the major surgical studies shows that rfa of hepatic mets has a lower mortality and periprocedural complication rate ( table 1 )  . 
on the other hand , due to the poor local effectiveness of rfa in treating mets larger than 3 cm in diameter , surgery remains better for larger lesions . regarding the clinical indications for metastasectomy , a recent literature review attempted to make recommendations in selected patients ( young patients , low surgical risk , long interval between breast cancer surgery and liver metastases , positive hormone receptor status of primary tumour , no extra - hepatic disease , demonstrated disease regression or stability with systemic therapy before resection , normal liver function tests , resection with intent of a complete resection of liver metastases )  . 
owing to the limitations of the few published studies , however , even the impact of surgery on survival is considered to be merely potential [ 3 ]  . the nal consideration is that , even in the light of the lack of correlation between local effectiveness and survival , hepatic rfa should not be used as the only treatment for metastatic breast cancer . 
nonetheless , rfa may be proposed as an alternative to surgery in the context of a multimodal strategy , as it is safe and effective in achieving local control of limited disease , especially when the burden of systemic therapy needs to be decreased , improve the quality of life of patients . in part conclusions rfa of hepatic metastases from breast cancer , intended as a local treatment during multimodal therapeutic management of the disease , has high technical effectiveness in tumours up to 30 mm , but it is not relevant in determining mid - term patient survival . 
the results were analysed statistically using the students t test for independent samples and the k statistic . results among the 97 patients included in the study , a diagnosis of right ventricular infarction was established in 12 , 14 and 24 cases on the basis of the clinical data , the ecg and echocardiography , respectively . 
fedele dipartimento di scienze cardiovascolari e respiratorie , policlinico umberto i , universita` di roma sapienza , viale regina elena 324 , 00161 rome , italy myocardial oedema and late enhancement of the right ventricle in 48 and 32 cases , respectively . 
all patients gave their informed consent before being included in the study . clinical diagnosis of rvmi all patients underwent a complete cardiological assessstandard ment : patient history , physical examination , 12 - lead ecg ( with additional right precordial leads when rvmi was suspected ) and echocardiography . clinically , the contemporary presence of arterial hypotension ( systolic blood pressure \90 mmhg ) , clear lungs on auscultation and jugular venous distension ( kussmaul sign ) [ 14 ] was considered suggestive of rvmi . electrocardiographically , the infarction was dened as anterior when detected on leads v1v4 and inferior on leads ii , iii and avf . 
rvmi was dened as an elevation greater than 1 mm in v1 or v4r within 12 h of symptom onset . the echocardiographic study of the ventricular chambers was performed using standard apical and parasternal projections , with dedicated equipment ( acuson sequoia , siemens , erlangen , germany )  . 
for each mri study , the images were semiquantitatively evaluated using regions of interest as shown below : tissue signal at myocardial oedema ( me ) and late enhancement ( le ) were respectively evaluated on stir and irge sequences in the short axis planes . 
based on the literature data , me was dened by an increase of the pathological myocardial standard deviations ( sd ) as compared to the signal of healthy myocardium ; similarly , assessment of le was based on an increase of the signal of at least 4 sd [ 16 ]  . on each test , the areas of me and le of the left ventricle were manually outlined with dedicated software and quantied in terms of mass and percentage ( injured myocardial mass / myocardial mass ) of the ischaemic area and area at risk ( respectively , ia and aar )  . least the presence of right ventricle le ( rvle ) was identied as an increase of the signal coming from the region of the rv myocardium adjacent to the left ventricle le ( lvle )  . 
as previously reported , a similar criterion was used to evaluate the rv oedema [ 13 ]  . the segmental wall motion assessment was performed on cine - mr using the 17 - segmentation american heart association scheme for the lv , and the isner classication into 12 regions ( 4 basal , 4 mid - ventricular and 4 apical ) for the rv [ 17 ]  . using the semiquantitative evaluation proposed by masci et al . 
 [ 13 ] , each segment was assigned a motion score from 1 to 5 ( 1 = normal , 2 = moderate hypokinesia , 3 = severe hypokinesia , 4 = akinesia , 5 = dyskinesia )  . 
statistical analysis was conducted with dedicated software ( spss 11.0 for windows , spss , chicago , illinois )  . results cardiological assessment nine out of 97 ( 9 % ) patients showed simultaneously the three clinical signs of rv ischaemic involvement . 
thirtyseven patients ( 38 % ) showed ecg signs of inferior infarction , whereas 59 ( 61 % ) showed ecg signs of radiol med ( 2014 ) 119 : 309317 fig . 
t2 - weighted stir ( short - tau inversion recovery ) ( a , c ) and t1weighted irge ( inversion recovery gradient echo ) ( b , d ) images show an extensive area of myocardial oedema at the level of the interventricular septum and the free wall of the right ventricle ( white arrow ) , which corresponds to transmural enhancement in the late enhancement images ( white arrow )  . 
it is associated with a diffuse thickening and enhancement of the pericardial leaets ( white arrowheads ) due to postinfarction inammation ( post - infarction pericarditis epistenocardica ) anterior infarction . 
of the 26 / 97 patients in whom the right leads were acquired , 14 showed an st elevation ( in 13 cases associated with an st elevation in leads dii , diii and / or avf ) in lead v4r . echocardiography revealed an impairment of right ventricular function in 24 cases , and more specically : in 18 cases it showed hypocontractility of at least one segment ( free wall , inferior wall or apex ) , in 17 cases a dilatation of the rv , and in 10 cases a dyskinesia of the interventricular septum ( table 1 )  . magnetic resonance cmr conrmed the presence of a le area within the lv myocardium in 95 / 97 cases . 
in the remaining two patients , both with anterior mi , the mr pattern was characterised by tissue oedema ( hyperintensity in t2 - stir ) in the distribution territory of the culprit lesion in the absence of le ( aborted infarction ) [ 18 ]  . 
2 a 63 - year - old man with acute inferior myocardial infarction due to distal right coronary artery occlusion . t2 - weighted stir ( a ) and t1 - weighted irge ( b ) images acquired in the short axis show a large ischaemic area at the infero - septal and inferior left ventricular segments with typical extension of the area of myocardial oedema ( black arrow ) and late enhancement ( white arrow ) to the inferior wall of the right ventricle fig . 
ad stir images show a wide area of oedema involving the interventricular septum , the left ventricular anterior wall and the right ventricular free wall , both at basal , intermediate and level ( white arrows )  . 
sparing of the free wall ( white arrowhead ) and apical segments ( black arrow ) of the right ventricle conrms the greater the right ventricular myocardium to the ischaemic insult resistance of criteria and the cmr signs is shown in table 1 . 
finally , in le imaging , inversion time to be selected to null the signal of the healthy myocardium may vary between rv and lv , causing artefacts or requiring a double acquisition for each plane with considerably longer duration of the examination [ 22 , 23 ]  . to overcome these difculties , many authors recommend to use high - spatial resolution thin - slice sequences and le sequences with fat suppression , and to consider as pathological only the myocardium which is in continuity with the pathological left ventricular myocardium . in a study by kumar et al . 
 [ 19 ] , among 37 cases of inferior mi subjected to clinical , instrumental and mri investigation , 57 % patients ( 21 / 37 ) showed rvle , while only 19 , 35 and 16 % , respectively , demonstrated signs of rvmi at cardiological examination , on the v4r lead at ecg or at echocardiography . in our population , the rv had an ischaemic involvement in 46 % of cases of inferior mi and in 30 % cases of anterior mi , differing from the values given by jensen et al . [ 21 ] , which were 47 and 65 % , respectively . rv involvement during an anterior mi could be affected by the presence of anatomical variants of the anterior descending artery , with perfusion of the free wall and right para - apical region by particularly long anterior interventricular branches extending beyond the apex , or alternatively from the origin of the moderator branch of the distal anterior descending artery [ 13 ]  . 
this potential anatomical variability may , therefore , account for the discrepancy in the anterior mi values seen in our study population compared to those reported by jensen et al . 
in our population , there was a radiol med ( 2014 ) 119 : 309317 316 radiol med ( 2014 ) 119 : 309317 considerable frequency of rvme in both inferior ( 59 % ) and anterior ( 48 % ) mi , signicantly higher as compared to the frequency of rvle , which was present in 46 and 30 % of patients , respectively . 
therefore , this nding supports the notion of a greater resistance of the rv myocardium to the ischaemic insult as compared to the lv tissue , which for an ischaemia of the same duration showed increased susceptibility to necrotic damage in the at - risk area ( 98 % of patients had lvle )  . as stated by goldstein , the term right ventricle myocardial infarction is to some extent a misnomer because often the acute ischaemic dysfunction of the rv is represented by viable myocardium , in contrast to what happens for the lv [ 4 ]  . multiple reasons contribute to the increased resistance to ischaemia of the rv : the different load conditions due to the lower resistance of the pulmonary circulation , myocardial thickness which results in a lower oxygen demand and a greater oxygen reserve [ 4 ]  . 
furthermore the dual blood supply of the rv free wall , coming from branches of the anterior descending artery and from conal branches of the right coronary , allows for a ready provision in the event of vessel occlusion [ 13 , 26 ]  . 
another limitation is the absence of proper follow - up or clinical monitoring of the study population , which could have provided prognostic information but which we decided not to include in the results because of the limited observation time and because it was the subject of other recently published papers [ 14 , 19 , 24 , 25 ]  . conclusions in our study population , rvle was seen in 25 % of patients with acute mi and , in consideration of the literature data that demonstrates how this nding adversely affects the patients prognosis [ 19 , 24 , 25 ] , it is clear that this is not a negligible element . 
in particular , effective doses were evaluated using the tissue weighting ( wt ) factors reported both in icrp60 ( wt , 60 ) and in icrp103 ( wt , 103 )  . results a decrease in the frequency of pr skull examinations and an increase in the frequency of mammography , ct of the abdomen , chest , and headneck were found during the decade . 
moro 21 , 40127 bologna , italy with the use of wt , 60 until 2007 and wt , 103 from 2008 seem to be consistent and coherent . keywords ct ( cid : 2 ) dose , population ( cid : 2 ) exposure measurements ( cid : 2 ) patient protection ( cid : 2 ) radiography ( cid : 2 ) x - ray introduction the use of ionising radiation in medical radiology is by far the greatest source of radiation exposure of anthropic origin as stated by the united nations scientic committee on the effects of atomic radiation ( unscear ) [ 1 ] and thus the evaluation and quantication of medical exposure is a key subject in radiation protection for many aims : verifying whether there are signicant differences between the dose delivered in different regions or countries ; comparing the contributions from different kinds of x - ray examinations to provide best guidance on where efforts on dose reduction can concentrate ; monitoring the trends in annual per caput doses as associated with changes in radiology practice ; comparing the dose from medical radiology with that due to natural background radiation . many nations have reported population dose estimates through diagnostic imaging procedures [ 16 ] , but no similar study has been reported with regard to italy yet . 
the frequency of examinations ( both inand out - patient ) was based on data provided between 2001 and 2010 directly by all 17 public trusts of the regional health service for each type of procedure , grouped according to national ministry of health nomenclature code , to reduce terminology errors ( table 1 )  . 
to relate those dose quantities to e , conversion coefcients calculated by monte carlo techniques were used : a set of these coefcients was calculated taking into account the wt , 60 and another set was calculated using the wt , 103 . 
to calculate effective dose according to the methods described in the literature [ 1417 ] some data concerning the examination protocols ( kvp , total ltration , etc . ) were also requested : the mean ( weighted for the number of examinations carried out in each hospital ) and the range of these parameters are reported in tables 2 and 3 for pr and ct , respectively . 
in this way the trends of collective effective dose values calculated by three different methods were shown to make a direct comparison . radiol med ( 2014 ) 119 : 348358 results the e percentage contributions of pr and ct procedures to collective dose calculated by different conversion coefcients with regard to the last year of data collection ( 2010 ) are reported in fig . 
the highest relative frequency was found in pr chest examinations ( 35.4 % ) , but they accounted for only 1.4 % of collective effective dose as calculated with both wt , 60 and wt , 103 factors . the total number of examinations per 1 , 000 inhabitants between 2001 and 2010 , subdivided by procedure , are reported in fig . 
in projection radiology , a decrease in the frequency of skull examinations ( - 67 % ) and an increase in the frequency of mammography ( ? 40 % ) were found during the decade . 
as far as the ct procedures are concerned , during the same period ct of abdomen , chest , and headneck increased by 89 , 90 and 57 % , respectively . 
when the same wt factors are used , generally the doses did not change noticeably through the years : the most remarkable decrease and increase in the e / procedure between 2001 and 2010 were found in pr of the skull ( - 22.1 % ) and pelvis ( ? 30.8 % ) , respectively . 
1 contributions to emiliaromagna collective dose ( calculated by different conversion coefcients ) and examinations frequency from projection radiology ( pr ) and computed tomography ( ct ) procedures ( reference year : 2010 ) 352 fig . 
4 : the analogous temporal trends for ct procedures are all e / procedures this shown increased during the decade ( mean percentage increment ? 151 % )  . case , in table 5 the percentage contributions from pr and ct procedures to per caput annual effective dose are reported in detail for each examination : in particular , the ct contributions are calculated with both e103 , rat and e103 , cal . 
the temporal trend of per caput effective dose from 2001 to 2010 ( calculated with both wt , 60 and wt , 103 factors ) for the examinations under consideration is shown in fig . 
5. discussion projection radiology represents the largest contributor to the frequency of examinations in emilia - romagna in 2010 , although ct examinations provide the greatest doses whichever conversion factors for e are used . the trend in the frequency of ct examinations per 1 , 000 inhabitants reported in fig . 
3 temporal trends of effective dose per projection radiology ( pr ) examination between 2001 and 2010 , subdivided for procedure : a abdomen , lumbar spine , pelvis and urography ; b chest , mammography and skull examinations , possibly reecting the recent trend to prefer ct to plain radiography when the patient presents with a cervical trauma [ 2426 ]  . in the years of this study ( 20012010 ) , s evaluated with e60 was always in between the collective effective doses calculated with e103 , rat and e103 , cal : for example , the values of s were 1 , 934.9 man sv2 , 065.4 man sv2 , 196.8 man sv in 2001 and 5 , 855.1 man sv6 , 169.2 man sv6 , 665.5 man sv in 2010 when e103 , cale60e103 , rat were used , respectively . 
the fact that e60 is not denitely higher or lower than e103 reects the fact that the use of wt , 60 or wt , 103 is not a one - way street , and the quantity e / procedure increases or decreases when the old or the new weighting factors are used depending on the anatomic regions irradiated . 
as an example , pr of the skull and pelvis might be compared : in 2010 the doses for pr of the skull calculated with wt , 60 were 36 % lower than those evaluated with wt , 103 , because according to the icrp 103 recommendations the radiosensitive organs in the head are now four ( brain and salivary glands with specic tissue weighting factors ; extrathoracic region and oral mucosa as remainder organs ) , while according to icrp 60 the only structure in the head and neck region explicitly listed as a remainder organ was the braon the other hand , in 2010 the doses 354 fig . 
5 , the line of per caput effective dose calculated with wt , 60 factors lies in between the lines of the same quantity evaluated by different methods ( e103 , rat , e103 , cal ) from wt , 103 coefcients : thus doses calculated with the use of wt , 60 ( until 2007 ) and wt , 103 ( from 2008 ) on the same chart seem to be consistent and coherent . 
in the specic case of the emilia - romagna region reported in this study , this comparison has been shown to be still important and useful to keep the results obtained in the previous surveys : the wt , 60 factors can be used until 2007 , while the wt , 103 coefcients can be used from 2008 . 
thus the emilia - romagna per caput effective dose rose from 0.5 msv in 2001 to 1.5 msv in 2010 : the latter value can be compared with the gure of 3.0 msv quoted in the usa in 2006 [ 29 ] and the corresponding value of 1.9 msv assessed by unscear [ 1 ] as the average dose for healthcare level 1 countries . a major limit of this study lay in the data collection that in the very rst years was not complete : a few trusts did not provide all the parameters requested and many interpolations were needed to have a full picture of frequency of examinations and dose distribution in the region . 
nonetheless , in the last years increasingly complete datasets were returned from the trusts because a culture of patient radiation protection and procedure optimisation became widespread in all hospitals , and the surveys were thus more reliable . 
moreover , radiological information systems ( ris ) are being effectively integrated with the hospital information systems ( his ) and that can provide better and faster the radiological data about departments . 
5 temporal trend of per caput effective dose from 2001 to 2010 calculated with both e60 and e103 conversion factors in pr of the pelvis calculated with wt , 60 were 38 % higher than those evaluated with wt , 103 , due both to the large decrease in the weighting factor for the gonads and to the reduction in the wt for the bladder that compensates for the introduction of the prostate as a remainder organ . the e103 , cal were generally lower than e60 for ct procedures : this might be related to the fact that deak et al . [ 19 ] calculated conversion factors for new ct equipment and not for the ct scanners that were used in the early 1990s like in the european commission report [ 15 ]  . the per caput effective dose due to pr and ct incremented by approximately 170 % from 2001 to 2010 , basically due to increment in both frequency and e per procedure of ct examinations : the contribution of pr to per caput effective dose was 25 % in 2001 and 10 % in 2010 with an increment of 12 % in pr frequency , while ct accounted for 75 and 90 % of per caput effective dose in 2001 and in 2010 , respectively , with an increment of 52 % in the number of total ct procedures . 
therefore , in particular the highest dose - contributor examinations , appropriate strategies with regard to medical exposure justication and optimisation need to be adopted to contain e , and tools for minimising the dose per procedure without affecting the quality of diagnostic information need to be identied , in accordance with the european union and international guidelines [ 8 , 27 , 28 ] : in ct that means , amongst other factors , reducing the number of scan phases , limiting the scan length , using the dose modulation facilities and , last but not least , selecting the appropriate scanning technique . the emilia - romagna annual per caput effective dose from ct was 1.3 msv in 2010 : this value is lower than the corresponding gure of 1.5 msv from ct in the usa [ 29 ] though it is higher than the level of 0.74 msv recently found in canada [ 30 ]  . 
therefore , though the dose level from this specic practice is in good agreement with other countries levels , something in the way those high - dose procedures are carried out can still be done , in accordance radiol med ( 2014 ) 119 : 348358 have been included because italian legislation denes the term radiodiagnostic as pertaining to medical diagnostic radiology and diagnostic nuclear medicine in vivo [ 7 ] , but there are not yet effective dose calculations based on new icrp weighting factors for all the examinations . 
it is still important to study trends in medical exposure of the population but dose estimates preand post - icrp publication 103 must be compared carefully , because changes due to different radiological practices could be confused with changes due to the use of different wts : in this paper indications on how a comparison of per caput and collective effective doses might be carried out have been suggested . 
fileni received : 3 september 2012 / accepted : 30 january 2013 / published online : 3 december 2013 ( cid : 2 ) italian society of medical radiology 2013 abstract purpose since radiologists and radiotherapists can be occupationally exposed to signicant psychosocial risk factors , some may nd themselves in a state of distress . the aim of this study was to investigate the association of work - related stress with the presence of symptoms of anxiety , depression and psychological malaise and to evaluate the risk of psychic disorder in radiologists suffering from work - related stress . methods a total of 654 radiologists responded to our invitation to complete a questionnaire designed to evaluate work - related stress and associated medical conditions : the general health questionnaire and goldbergs anxiety and depression scales . results scores on the anxiety , depression and psychological malaise scales rise with an increase in effort and over - commitment , while control and support exert a protective effect . 
now a major effort must also be made to improve the mental wellbeing of radiologists , both in the interests of the workers themselves , and also in those of their patients and the quality of the treatment they have the right to receive . keywords work - related stress ( cid : 2 ) radiologist ( cid : 2 ) depression ( cid : 2 ) anxiety ( cid : 2 ) distress introduction the work of radiologists and radiotherapists exposes them to considerable occupational risk factors . 
these may be of a structural nature on account of excessive workloads or organisational difculties [ 1 ] , of a compassionate nature in relation to the suffering of patients [ 2 ] , or due to accusations of malpractice or concern about errors committed [ 3 ]  . 
compared with other medical categories , radiologists have the highest levels of work - related stress [ 4 ]  . distress is a mixed and loosely dened term describing a subjective , negative and unpleasant reaction to stress . 
this type of disorder is very widespread ; in europe , it is estimated that the prevalence of mood disorders in the course of working life is 14.0 % , and the prevalence of anxiety 13.6 % , while , in the nal year of work , these become 4.2 and 6 % , respectively [ 6 ]  . distress and its resulting mental disorders are critical factors when work is being performed . 
the percentage of doctors affected by symptoms of depression is very high both in western and eastern countries , although there are relatively few serious cases [ 9 ]  . young physicians are at greater risk [ 10 ]  . 
it has been seen that the pressure of psychosocial factors , such as excessive work demand and low discretionary power , reduce the affective commitment to work and encourage physicians to abandon their occupation [ 11 ]  . there are three reasons why it is important to diagnose srds . 
for example , in italy , it has become compulsory for all employers to evaluate the risk of stress in the work environment and to arrange appropriate measures of prevention should these prove necessary [ 12 ]  . 
at an individual level , the occupational physician can prescribe specic temporary or permanent intervention to facilitate a return to work or to improve the quality of occupational life . theories have been developed to evaluate the negative mental health effects on workers exposed to psychosocial risk factors . 
the most inuential are karaseks demandcontrol - support ( dcs ) model [ 13 ] and the effortreward imbalance ( eri ) model devised by siegrist [ 14 ]  . 
both theories suggest that distress is the result of an imbalance , in the karaseks model between demand and control over ones work , and in the siegrists model between effort and reward . 
the aim of this study was to ascertain whether there is an association between a state of distress in radiologists and the presence of srd : anxiety , depression and psychological malaise . during a national congress of the italian society of medical radiology , radiologists were invited to complete a methods questionnaire that included , amongst other things , a section for evaluating work - related stress and one for estimating its consequences . 
karaseks questionnaire provided scores relating to the demand scale , psycho - physical demands of the job ; the control scale concerning the amount of discretionary power the worker has in performing his work ; and the support scale indicating support from colleagues and superiors . 
job strain can be dened as the proportion of workers who simultaneously psychological workload ( demand values above the median ) and low control ( values below the median )  . 
siegrists questionnaire provided an effort scale ( the psychological work effort or extrinsic stress ) , an over - commitment scale ( high work commitment , or intrinsic stress ) and a reward scale ( rewards received for work performed )  . 
subjects with a score [ 1 were considered to be stressed as they subjectively perceived an imbalance between effort and reward . elevated have the consequences of distress were evaluated using the general health questionnaire ( ghq12 ) and goldbergs anxiety and depression scales , both in their italian versions [ 17 , 18 ]  . 
the level beyond which the risk of suffering from a psychic illness increases signicantly , is set at 2 points since it is the level that provides the best sensitivity and specicity [ 20 ] ; thus from 3 points onwards , the subject could become a case . we should remember that the concept of caseness in social psychiatry has only an epidemiologic value and radiol med ( 2014 ) 119 : 359366 corresponds to a probability , not a psychiatric diagnosis . 
the nal score results from the total number of afrmative answers . caseness , dened as a more than 50 % probability that the diagnosis will be conrmed by a specialist , corresponds to a score of six or more points on the anxiety scale , and three or more points on the depression scale [ 21 ]  . 
in the second and third models , we added the variables indicating work - related stress , by separately adding karaseks ( demand , control , support ) variables and those of siegrist ( effort , reward , over - commitment )  . 
in the nal model , we introduced all the variables relating to stress and the sociodemographic variables simultaneously as predictors of each of the effect variables ( anxiety , depression , psychological malaise )  . 
the standardised correlation coefcient ( b ) indicated the degree of association between the variables . the capacity of each equation to correctly interpret variations in the phenomenon studied was indicated by the adjusted coefcient of determination ( r2 )  . second , we wanted to ascertain what risk radiologists have of suffering from psychic disorders when they are in a state of distress . 
for this purpose , we used binary logistic regression , taking the dependent variable to be the state of anxiety , depression and psychological malaise ( caseness ) as dened above . 
as the independent variable we separately introduced the state of distress evaluated as job strain ( the subject is exposed to high demand and low control ) and the state evaluated as eri ( subjects with eri [ 1 ) , the state of social isolation ( support = below the median ) and that of excessive involvement in work ( over - commitment = above the median )  . 
the value we obtained ( raw or non - adjusted ) was subsequently adjusted by adding to the equation the variables indicating gender , age , length of employment , type of organisation , where subjects were employed , and hierarchical role . 
this enabled us to calculate the odds ratio ( or ) and their 95 % condence intervals ( or 95 % )  . results the characteristics of the study population are illustrated in table 1 . 
table 2 shows the mean values of the variables indicating work - related stress and mental disorders . among the radiologists who completed our questionnaire , there were 286 ( 43.7 % ) probable cases of anxiety ( score of [ 5 on the goldberg a scale ) ; 287 ( 43.9 % ) cases of depression ( score of [ 3 on the d scale ) and 140 ( 21.4 % ) cases of psychological malaise ( ghq [ 2 )  . linear regression analysis ( table 3 ) enabled us to determine to what degree the value of each of the measurements of psychiatric pathology could be predicted using data on sociodemographic factors and the level of work - related stress . 
a signicant association was observed between some of the sociodemographic variables and the scores for anxiety , depression and psychic disorders , but on the whole , sociodemographic factors accounted for a small fraction of the variation in psychic problems ( coefcients of determination r2 ranged from 3 to 7 % )  . 
a positive association was observed between age and depression , but the former was negatively related with acute psychic disorder measured by the ghq12 and this relationship also remained signicant in the more complex model . 
even allowing for rst type error ( false positive ) , we must conclude that the prevalence of psychic disorders in radiologists is not negligible and could exceed values reported in other occupational populations [ 6 ]  . 
moreover , individuals with psychic problems may report working conditions in a less favourable light since they are the type of subjects who complain about everything [ 32 ]  . 
the opposite may also be true ; that is , there are workers who tend to deny the existence of both environmental and health problems , they are the ones who never complain about anything [ 33 ]  . 
the simultaneous presence of these two types of workers lowers the reliability of cross - sectional studies in which participants are asked to make a self - evaluation of both environmental and personal conditions . 
in our the fact particular case , physicians probably increased the objectivity of responses . the interviewees were their that all on the basis of our ndings , we believe that the work of radiologists would benet from primary preventive intervention at a number of levels . 
the dcs model shows that radiologists would benet from programs designed to improve the management of workloads ( especially working hours ) , productive processes and group work , and company policies for enhancing social support . 
the eri model indicates that any reorganisation should include a reduction in extrinsic effort , especially in younger subjects or those who are new to the job , with fairer distribution of workloads , less overtime and a sufcient number of breaks , an increase in rewards ( including immaterial ones ) for work performed . 
it seems to be particularly important to reduce intrinsic stress resulting from over - commitment concentrate on the technical aspects of the job and by teaching subjects to introduce protective factors against stress such as better lifestyles and recreational and sports activities . 
these tasks , which are often disregarded in our country , are an essential part of the general protection that employers , and therefore also public and private health authorities , are legally called upon to implement . 
the mr studies were reviewed according to the mr - bi - rads classication system ; lesions assessed as mr - bi - rads 1 and 2 were considered negative for malignancy , categories mr - bi - rads 3 , 4 and 5 indicated malignant lesions . 
mr sensitivity , specicity , positive predictive value ( ppv ) and npv were calculated . results the nal population consisted of 71 lesions . showed malignancy in six cases histologic analysis ( malignancy rate 8 % )  . 
mr sensitivity was 33 % , specicity 86 % , ppv 18 % and npv 93 % . conclusions because of its relatively low npv , mr imaging is not able to safely exclude malignancy in the a . 
the relatively high malignancy rate found in this study might support svab in the case of bi - rads 3 microcalcications . keywords bi - rads 3 ( cid : 2 ) microcalcications ( cid : 2 ) breast mri ( cid : 2 ) stereotactically guided vacuumassisted - biopsy ( cid : 2 ) dcis introduction the estimated probability of malignancy in breast imaging and reporting data system ( bi - rads ) category 3 mammographic lesions ( including both microcalcications and masses ) is lower than 2 % [ 1 , 2 ] ; therefore , periodic mammography follow - up is recommended in the management of these lesions . 
however , some authors have found disturbingly high rates of malignancy in women with microcalcications assessed as probably benign ( bi - rads 3 ) , ranging from 0 to 19 % [ 37 ]  . 
as a consequence , many bi - rads 3 microcalcications are recommended for stereotactically guided vacuum - assisted biopsy ( svab ) instead of mammographic follow - up , because of referring physician or patient concern that there could be a substantial risk of malignancy [ 4 , 8 ]  . the large majority of patients with bi - rads 3 microcalcications referred for biopsy have benign lesions , in a high number of unnecessary biopsy which result procedures . breast magnetic resonance ( mr ) imaging has very high sensitivity for breast cancer [ 9 ] , and in selected scenarios , a negative breast mr examination is able to safely exclude malignancy [ 10 ]  . 
 [ 11 ] found that mr imaging has sufciently high negative predictive value ( npv ) to rule out malignancy and avoid 394 radiol med ( 2014 ) 119 : 393399 invasive procedures in noncalcied bi - rads 3 mammographic lesions . 
conversely , a denitive conclusion about the role of mr imaging in bi - rads 3 microcalcications could not be drawn because of the small number of microcalcications included in the study [ 11 ]  . 
the purpose of this study was to evaluate whether mr imaging is able to rule out malignancy in the case of bi - rads 3 microcalcications , providing a sufcient npv for early work - up , and therefore to decrease the number of unnecessary svab procedures . materials and methods this study was performed in a university referral hospital for breast diseases . 
all patients provided written informed consent to participate in the study . patient population between september 2006 and june 2011 , we prospectively enrolled consecutive women with screen - detected probably benign ( bi - rads 3 ) microcalcications , who subsequently underwent mr examination of the breast and svab of the microcalcications . 
microcalcications were classied according to bi - rads descriptors for mammographic features including calcication morphology ( punctate , amorphous , pleoregional , morphic , clustered , segmental and linear )  . 
according to the birads lexicon , clusters of punctate / amorphous microcalcications were dened as bi - rads 3 . and distribution ( diffuse , linear ) mr imaging technique breast mr imaging studies were performed on a 1.5 - t scanner ( magnetom avanto , siemens medical system , erlangen , germany ) with a dedicated , bilateral , 7 - channel phased - array coil and the patient in prone position . 
from september 2006 to may 2009 , the dynamic contrast study was obtained using a coronal t1 - weighted three - dimensional ( 3d ) fast low - angle shot ( flash ) pulse sequence with the following parameters : tr / te , 15 / 4.7 ms ( ms ) ; ip angle , 25 ( cid : 3 ) ; matrix , 197 9 448 ; eld of view , 350 9 175 mm ; section thickness , 1.8 mm ; acquisition time , 1 : 28 min . from june 2009 to june 2011 , the dynamic contrast study was obtained using an axial t1 - weighted 3d flash pulse sequence with the following parameters : tr / te , 9 / 4.7 ms ; ip angle , 25 ( cid : 3 ) ; matrix , 512 9 512 ; eld of view , 340 9 340 mm ; section thickness , 2 mm ; acquisition time , 1 : 20 mgadobenate dimeglumine ( gd - boptamultihance , bracco imaging , milan , italy ) was administered intravenously with an automated bolus injection at a dose of 0.1 mmol / kg body weight with a ow rate of 2 ml / s , immediately followed by a 20 - ml saline ush , using an automatic injector ( spectris solaris , medrad )  . 
images were acquired sequentially once before and ve times after injection of contrast agent , beginning 12 s after initiation of the contrast injection and with no interscan delay . postprocessing and construction of dynamic curves were performed by one of the ve radiologists with more than 2 years of experience in breast mr imaging using a syngo multimodality workplace ( leonardo , siemens healthcare , erlangen , germany )  . 
postprocessing included temporal subtraction ( all contrast - enhanced series minus noncontrast - enhanced series ) , and the acquisition of multiplanar reconstructions ( mpr ) and maximum intensity projections ( mip )  . dynamic signal intensitytime curves were constructed for regions of interest ( 3 9 3 pixels ) positioned within the lesion on subjectively determined areas of maximal enhancement . it is our standard of practice to perform targeted sonographic examination ( second - look ) in the case of incidental mr ndings that were occult on mammography or whole - breast initial sonography . mr imaging analysis the study coordinator ( with more than 5 - year experience in breast imaging ) , who was not involved in further mr evaluation , reviewed all imaging available and annotated on a breast map the location of each microcalcication lesion using a clock - face reference and the relative distance radiol med ( 2014 ) 119 : 393399 from the nipple . 
mr evaluation was performed on noncontrast - enhanced and contrast - enhanced series . the mr images were classied as negative / normal if no contrast enhancement was identied in the area of the lesion ( mr - bi - rads 1 ) or if only homogeneous or stippled enhancement representing normal glandular tissue ( mr - bi - rads 2 ) was seen bilaterally . 
lesions that were detected on mr and corresponded to the area of microcalcications were classied as focus , mass enhancement or nonmass enhancement and were assessed as mr - birads 3 , 4 or 5 [ 13 ]  . 
with the patients lying prone on a digital stereotactic table ( mammobed , giotto , ims srl ) , svab was performed using a directional vacuumassisted biopsy ( vab ) device ( mammotome , ethicon endo - surgery , cincinnati , oh , usa ) with an 11 - gauge needle . 
after the procedure , a clip ( mammomark , ethicon endo - surgery , cincinnati , oh , usa ) was placed through the 11 - gauge needle to mark the biopsy site for subsequent surgical excision . if pathologic examination demonstrated a malignancy or a high - risk lesion ( such as atypical ductal hyperplasia ) , surgical excision after placement of a hook - wire under stereotactic guidance was recommended . 
if a benign lesion was pathologically proven on svab , the patient was scheduled for repeat mammography of the ipsilateral breast at 6 months and annual screening mammography was recommended thereafter . data analysis for histologic analysis , we grouped the microcalcications into two main categories , benign and malignant . 
in patients who underwent a surgical procedure after svab ( because of malignant or high - risk lesions demonstrated in biopsy samples ) , the most severe histologic result was considered . in the case of high - risk lesions conrmed at surgical excision , the lesion was considered benign . a malignant lesion was considered to be diagnosed successfully by mr imaging ( true positive ) if contrast uptake in the area of microcalcications was shown ( birads 3 , 4 or 5 )  . 
a false negative nding was dened as the absence of focal contrast uptake in the area of microcalcications ( bi - rads 1 and 2 ) that proved to be malignant at histologic analysis . we calculated the sensitivity , specicity , positive ( ppv ) and npv of mr imaging in diagnosing malignant lesions presenting mammography . 3 microcalcications as bi - rads results patient population seventy - four bi - rads 3 microcalcication lesions were initially considered eligible . 
the mean interval from mr imaging to svab was 9 days ( range 143 ) ; the mean interval from svab to surgical procedure was 20 days ( range 1345 days )  . histologic and follow - up results stereotactically guided vacuum - assisted biopsy demonstrated malignancy in ve cases [ four intermediate - grade ductal carcinoma in situ ( dcis ) and one low - grade dcis ] , that were all conrmed at surgical excision . 
five high - risk lesions were diagnosed at svab ( 3 lobular neoplasia , 1 radial sclerosing lesion and 1 at epithelial atypia ) ; one lobular neoplasia was upgraded to low - grade dcis at surgical excision , while the remaining high - risk lesions were conrmed . 
b , c axial t1 - weighted nonenhanced ( b ) and contrast - enhanced subtracted ( c ) magnetic resonance ( mr ) images ( 9 / 4.7 , 25 ( cid : 3 ) ip angle ) show the absence of pathologic enhancement in the area of microcalcications . 
this examination was assessed as mr - bi - rads 1 ( false negative ) therefore , among the 71 lesions included in the study , nal histologic analysis showed dcis in 6 ( 8 % ) , high - risk lesions in 4 ( 6 % ) , and benign lesions in 61 ( 86 % )  . mr imaging analysis versus reference standard at breast mr analysis , 60 ( 85 % ) lesions were assessed as negative ( 52 mr - bi - rads1 and 8 mr - bi - rads 2 )  . 
of these , 4 ( 7 % ) proved to be malignant at nal histologic examination ( 2 low - grade dcis and 2 intermediate - grade dcis )  . 
of these , 2 ( 18 % ) were malignant . one lesion was assessed as mr - bi - rads 3 and was an intermediate - grade dcis at svab , conrmed at nal pathologic examination . 
2 a 63 - year - old woman with benign disease in the left breast ( stereotactically guided vacuum - assisted - biopsy : brocystic changes ; no calcication progression at 24 - month follow - up )  . 
b , c axial t1weighted nonenhanced ( b ) and contrast - enhanced subtracted ( c ) mr images ( 9 / 4.7 , 25 ( cid : 3 ) ip angle ) show a mass - like lesion with faint enhancement and poorly dened borders ( arrow ) located in the central , prepectoral area of the left breast , corresponding to the location of microcalcications . 
breast mr had a sensitivity of 33 % [ 95 % condence interval ( ci ) 2346 % ] , specicity of 86 % ( 95 % ci 7593 % ) , ppv of 18 % ( 95 % ci 1029 % ) and npv of 93 % ( 95 % ci 8498 % )  . nineteen patients ( 27 % ) underwent second - look sonographic examination because of incidental ndings ( all assessed as mr - bi - rads 3 ) located outside the area of microcalcications and that were occult at mammography and initial whole - breast ultrasound . 
in 18 cases , secondlook examination showed normal or benign ndings ( cysts , intraparenchymal lymph nodes , or broadenomas )  . in these patients , no malignant lesion was seen during follow - up . 
one incidental lesion was occult at second - look ultrasound and was followed up with 6and 12 - month mr examinations that demonstrated no interval changes . 398 discussion our data show that mr imaging does not have sufciently high npv ( 93 % ) to exclude the presence of malignancy in the case of bi - rads 3 microcalcications . 
therefore , mr imaging is not able to guide the work - up ( biopsy or follow - up after 6 months ) of patients with bi - rads 3 lesions . our results are in contrast with those reported by dorrius et al . 
 [ 10 ] , who found a 100 % npv for malignancy in the case bi - rads 3 lesions . however , those studies included only eight cases of birads 3 microcalcications each . several studies evaluated the role of mri in patients with mammographic microcalcications ; however , those studies included also bi - rads 4 [ 14 ] or bi - rads 4 and 5 microcalcications [ 7 ] and global mr performance was calculated , without a by - category analysis . 
these were two low - grade and two intermediategrade dcis , all smaller than 8 mdespite the high sensitivity of mr imaging for invasive cancers and high - grade dcis , an absence of enhancement has been observed in 2060 % of intermediateand low - grade dcis [ 1517 ]  . in addition , it has been demonstrated that mr imaging leads to the detection of incidental benign ndings . 
in our study , in 19 ( 27 % ) of 71 patients , mr imaging detected additional ndings , which resulted in 19 sonographic examinations and 2 follow - up mr examinations in the same patient . 
in none of these cases was malignancy found at additional imaging or at follow - up . in our series , 6 ( 8 % ) of 71 bi - rads category 3 microcalcications were malignant . 
the recommended percentage among bi - rads 3 lesions is 2 % or fewer ; however , these low malignancy rates are based on followup mammograms and not on biopsy series [ 1 , 2 ]  . 
in addition , the stated low malignancy rate in bi - rads 3 lesions is probably related to the broad spectrum of mammographic ndings included in this group , which also includes well - dened masses [ 3 ]  . 
malignancy rates of bi - rads 3 microcalcications in svab series range from 0 to 16 % [ 37 ] , which is not tolerated for lesions managed with short - interval follow - up . radiol med ( 2014 ) 119 : 393399 on the other hand , most of bi - rads 3 microcalcications correspond to intermediateor low - grade dcis at pathologic examination ( 4 and 2 lesions respectively , in our study )  . 
intermediateand low - grade dcis have a benign biologic prole and if left undetected ( and untreated ) , they are likely to remain dormant or to exhibit slow ( decades long ) progression to invasive carcinoma [ 18 ]  . 
therefore , diagnostic delay due to noninvasive management ( imaging follow - up ) would probably not have a substantial effect on prognosis . however , interval changes at follow - up in the number and morphology of probably benign microcalcications may be difcult to assess , in particular if there are sufcient technical differences between the two studies . 
at the same time , the microcalcications seen in low - grade dcis may remain unchanged for many years [ 19 ]  . moreover , a recent study reported a high percentage of noncompliance in women recommended to undergo shortinterval follow - up for probably benign ndings , even in the context of a clinical trial [ 20 ]  . therefore , svab might still be considered an approchoice management bi - rads priate microcalcications . our study has some limitations . 
in addition , because of the difculties and variability in the classication of clusters of punctate / amorphous , an external review of our mammographic cases classied as bi - rads 3 would have been of great benet . in conclusion , we found that , unlike for noncalcied birads lesions , mr imaging is not useful in guiding the management of bi - rads 3 microcalcications . 
at the end of observation , the bowel was excised for histological analysis . results 7t l - mri t2 - w sequences acquired 15 min after sbo , showed early evidence of bowel wall hyperintensity and a small amount of peritoneal free uid . 
at 1 h , a hyperintensity of the loop proximal to the obstruction was found and , after 4 h , free uid between the loops , bowel wall thickening and increased wall hyperintensity were also found . 
after 6 h hypotonic reex ileus ( only gas - lled dilated loops ) was detected , which became paralytic ileus ( dilation with airuid levels ) after 8 h . 
the mri ndings were all conrmed at histological examination . conclusions this study allows denition of the early mri features of sbo ( peritoneal free uid and hyperintensity of the injured bowel ) and their chronological evolution , also conrmed by histological examination . 
the chance to achieve an early detection of bowel injury and to correlate the histological pattern with imaging ndings could contribute to a ner and earlier diagnosis and a more effective treatment . keywords small bowel obstruction ( cid : 2 ) magnetic resonance imaging ( cid : 2 ) experimental study ( cid : 2 ) animal model introduction small bowel obstruction ( sbo ) is a common clinical condition , often presenting with signs and symptoms similar to those found in other acute abdominal disorders . imaging , sbo despite recent advances in abdominal remains complex to diagnose and to treat [ 1 ]  . 
the morbidity and the mortality associated with acute sbo continue to be signicant , accounting for 1216 % of all surgical admissions in patients with acute abdominal conditions [ 1 ]  . imaging is important in the diagnosis and management of patients with sbo because it allows us to determine the presence and severity of obstruction , the transition point , and the cause of obstruction [ 2 ]  . previous investigations have demonstrated that accuracy of abdominal plain lm in determining the presence of obstruction is 4680 % [ 3 ] and that airuid levels are the most specic sign [ 3 ]  . 
unfortunately , air uid levels are not sensitive because they may be absent , especially in the late phase of small bowel volvulus and incarceration , when the loops become completely full of uid [ 4 ]  . 
ultrasonography ( us ) is widespread in several countries but this technique is operator dependent and it has inherent limitations because of the artefacts of gas378 radiol med ( 2014 ) 119 : 377383 containing structures [ 5 ]  . 
however , the ct technique suffers some limitations , the amount of delivered radiation dose and the need to administer iodinated contrast material [ 57 ]  . in particular magnetic resonance imaging ( mri ) , thanks to its excellent soft - tissue contrast and absence of ionising radiation exposure , has several characteristics that would make it an ideal imaging technique for the analysis of the small bowel , resulting in a promising alternative to ct in the evaluation of acute sbo . 
the purpose of this experimental study was to identify the early mri ndings of sbo and to analyse their evolution over time comparing them with histological ndings in an animal model . materials and methods animal preparation all procedures performed on animals were approved by our institutional animal care and use committee . 
ten adult male spraguedawley rats ( 250340 g ; harlan , usa ) , maintained on a 12 / 12 h light / dark cycle and allowed free access to food and water , were randomly divided into two groups of ve rats each ( group 1 and group 2 )  . 
group 1 underwent macroscopic observation , group 2 underwent 7t l - mri examination ; the animals in each group were examined at predetermined time points : basal ( before bowel occlusion ) , 15 min , 1 , 4 , 6 and 8 h after sbo . 
the rats were anaesthetized with ketamine hydrochloride 100 mg / kg im ( cu chemieuetikon gmbh , lahr , germany ) and medetomidine hydrochloride 0.25 mg / kg im ( domitor , pzer , new york , usa ) injections . 
photographs of the exposed bowel were taken after the occlusion at the ve predetermined time points described above . macroscopic analysis was assessed for the following parameters : ( 1 ) spastic reex ileus ( sri ) , consisting in contraction of the semilunar folds ; ( 2 ) hypotonic reex ileus ( hri ) , consisting in bowel wall dilation ( more than 2.5 mm in calibre ) ; ( 3 ) chromatic change of the bowel wall ( which is physiologically pink )  . magnetic resonance imaging group 2 animals underwent mri of the abdomen using a 7t l - mri scanner ( biospec 70 / 16us , bruker medical systems , ettlingen , germany )  . animals turborare sequences ( tr = 4 , 428.7 ms , te = 36 ms ; 180 ( cid : 3 ) ip angle ; 38 slices ; slice thickness , 1 mm ; interslice distance , 1 mm ; eld of view , scan time = 7 min 5 s 156 ms ) were performed just before sbo to act as basal imaging and after sbo at the above - mentioned ve time points . acquisition matrix , 256 9 256 ; 6 cm ; mr images were assessed for the following parameters : ( 1 ) presence of free uid in the abdomen ; ( 2 ) hri , consisting in bowel gas - lled dilation ( more than 2.5 mm in calibre ) ; ( 3 ) gasuid mixed stasis dilated loops ( paralytic ileus , pi ) ; ( 4 ) bowel wall thinning or thickening ( physiological thickness 11.3 ) ; ( 5 ) wall signal intensity on t2weighted sequences . histological analysis in all rats sbo was induced by performing a surgical procedure : after midline laparotomy , the most supercial small bowel loop in the upper right abdomen was isolated for light microscopy , the small bowels in both groups of rats were excised from the duodenum to the cecum , and stored in 10 % buffered formalin acetate for at least 2 days . 
transverse sections 3 lm in thickness were cut and stained with haematoxylineosthe sections were mounted on chrome alum / gelatin - coated slides , dehydrated and coverslipped . slides were imaged with a zeiss axio skope microscope equipped with a high - resolution digital camera ( orcahr c4742 - 95 - 12hr , 10 mp ; hamamatsu photonics k.k. , hamamatsu city , japan )  . results macroscopic evaluation in group 1 imaging the physiological appearance of rat at basal intestine before inducing the obstruction is given in fig . 
2 7 - tesla mri scan of the abdomen : basal image immediately before sbo : the loops appear with normal diameter and normal wall thickening , peritoneal free uid is absent ( a )  . 
at 15 min after bowel ligation , evidence of bowel wall hyperintensity ( arrow ) associated with a small amount of peritoneal free uid ( arrowhead ) ( b )  . 
in ( c ) bowel wall thickening , hyperintense signal in the bowel wall ( arrow ) of the loop proximal to the obstruction and a mild increase of peritoneal free uid ( arrowheads ) 1 h after sbo . 
four hours after sbo , a further increase of free uid among loops and of wall hyperintensity , associated with a mural thickening were detected ( d )  . hri ( arrow ) was appreciated after 6 h ( e )  . 
this study , based on an animal model of sbo , was designed to identify the mri ndings until 8 h of observation and to monitor their evolution in that time comparing them with the histological ndings . 
thus far , the discussion chronological sequence of early obstructive bowel damage has not been described , and the role of mri is still widely debated . the increase of intraluminal there has been a global change in the spectrum of aetiology of acute sbo over the past few years . 
even if some authors divide acute sbo into eight aetiological forms [ 1720 ] ( table 1 ) , just considering the surgical and imaging ndings , sbo can be classied as simple , decompensated and complicated [ 17 , 18 ]  . 
a thin layer of free peritoneal uid between the intestinal loops can be detected , which may increase , lling radiol med ( 2014 ) 119 : 377383 initial fig . 
3 at 15 min after sbo , the histology of the bowel sections showed damage in the proximal segment close to the sbo site , ischaemic damage and initial cleavage of consisting in : supercial epithelial cells . 
in the same region , 1 h after sbo , the histology of the bowel sections showed an increase of blood cell elements within the lamina propria ( b1 ) and in the medium magnication images increased damage of supercial enterocytes was detected ( b2 )  . 
at 6 h after ligation ( 3f ) the lumen was lled with necrotic material , bowel cellular debris and the brovascular axis appeared more congested ( 3d )  . 
at 8 h after bowel ligation , at high magnication , the peak of the villi appeared necrotic and a partial detachment of the villi was clearly visible ( e1 , e2 ) table 1 aetiological mechanisms of acute small bowel obstruction ( sbo ) 1 . 
complex mechanisms the lumen and peritoneal cavity in a more advanced stage . a correlation between the free peritoneal uid and a prompt surgical approach has been previously demonstrated [ 5 , 17 , 19 , 22 ]  . 
this stage requires immediate surgery [ 21 ]  . other authors distinguish two types of sbo , on the basis of vascular involvement : uncomplicated ( without vascular involvement ) and strangulation ( with vascular involvement ) , with a mortality rate varying from 3 to 7 % in uncomplicated cases to around 15 % in cases of strangulation [ 17 , 19 , 23 ]  . levels of severity and medical / surgical approaches [ 17 , 19 ]  . 
active these evolutionary stages exhibit different collaboration between the radiologist , emergency physicians , and general surgeons is necessary to optimise the diagnostic evaluation and management of this common and potentially dangerous problem [ 20 ]  . 
the role of radiologists in sbo is to conrm the obstruction , establish the cause , determine the level , and predict whether strangulation is present [ 24 ]  . at present when sbo is suspected , the diagnostic imaging protocol consists in plain abdominal radiography and ct whereas the utility of mri in acute settings is still a matter of debate . 
the diagnosis of sbo can be made with plain abdominal lms in 5060 % of cases but this technique may be unremarkable in 20 % of cases [ 25 ]  . 
the role of ultrasound ( us ) has been widely applied to evaluate various abdominal diseases and several articles have dealt with the usefulness of us in sbo [ 24 , 26 , 27 ]  . in the last few years , investigations have shown that mri can allow visualisation of the entire bowel , without overlapping bowel loops , and the detection of extraluminal pathological conditions [ 28 ]  . 
moreover , improvements in mri software and hardware have enabled imaging to assume a major role in the evaluation of the small bowel . the ability to provide cross - sectional information combined with the lack of ionising radiation can make mri well suited for small bowel imaging [ 28 ]  . 382 radiol med ( 2014 ) 119 : 377383 previous studies showed that mri using the half - fourier acquisition single - shot turbo spin - echo ( haste ) sequence is accurate for the diagnosis of sbo . 
 [ 29 ] proved mri ability to study the normal appearance of small bowel in haste sequence and to reveal small bowel disease such as crohns and sbo avoiding artefacts related to peristalsis and breathing [ 30 ]  . 
moreover , comparative studies between fast mri and helical ct proved that mri using haste sequences was more accurate than the helical ct ( 96 % with mri vs 71 % for ct ) [ 30 ]  . in this study , we used t2 - weighted mri sequences because , as shown in a previous study [ 31 ] , they allow us to identify , without using contrast media , the hyperintensity of the loop proximal to the obstruction site and peritoneal free uid . in the rats of group 1 , at 15 min after the obstruction , no pathological ndings related to obstructive damage were detected , while , in the rats in group 2 , 7t l - mr imaging without contrast material gave early evidence of bowel wall hyperintensity and mural thickening associated with a small amount of peritoneal free uid . 
the histology of the bowel sections , at this time point , showed initial ischaemic damage and an initial cleavage of the supercial epithelial cells . the submucosal vessels appeared ectasic and congested . in rats of group 1 , 1 h after the obstruction , sri of the loop proximal to the obstruction was observed , which was an early and transient reaction of the semilunar folds to the obstruction insult . 
the histological images showed increase of blood cell elements within the lamina propria and damage of the supercial epithelial cells . at 4 h , in the rats in group 1 , the sri was associated with a chromatic change of the ligated loop . 
within the adipose tissue ecstatic and congested venules were observed and the brovascular axis appeared more congested . in the rats of group 1 some previous ndings were still present at the 8th hour after the obstruction such as dilation and chromatic change . 
in group 2 , the dilation caused the arrest of the progression of the intestinal content , with resulting formation of airuid levels in the lumen ( pi ) , which were evident at the end of observation beyond other reported ndings . 
these results were conrmed at histological examination where a progressive mucosal ( at 15 min after sbo ) and transmural injury ( in the subsequent examination time points ) were found . although ct remains a valid diagnostic tool for the visualisation of signs of sbo [ 32 , 33 ] , mri , which does not require the use of a contrast medium or ionising radiation , can play an important role in the diagnostic and therapeutic management of patients with acute sbo . 
the aim of our paper is to report the frequency of this cerebrovascular disease in a series of patients affected by nf1 , using magnetic resonance angiography ( mra )  . 
in our study , mra proved to be critical , especially for the detection of stenoses in the branches of the circle of willis . conclusion few case series have investigated the incidence of vascular complications of nf1 , and most of them have used mri . 
melis department of pediatrics , university federico ii of naples , naples , italy keywords neurobromatosis type 1 ( cid : 2 ) arterial stenosis ( cid : 2 ) magnetic resonance angiography ( cid : 2 ) magnetic resonance imaging introduction neurobromatosis type 1 ( nf1 ) is a multisystem autosomal dominant disorder that primarily involves the skin and the nervous system , affecting approximately one in 2 , 500 / 3 , 500 individuals [ 1 , 2 ]  . 
it is caused by a mutation of a gene which encodes a protein known as neurobromin , localised on the long arm of chromosome 17 . vascular dysplasia is becoming increasingly recognised as a feature of nf1 with an estimated frequency between 2 and 6 % [ 8 , 9 ] , and the involvement of the circle of willis can be an extremely serious complication [ 4 , 5 ] , especially in the case of development of moya - moya disease . 
the cause of this variability is probably due to the fact that not all the patients with nf1 underwent magnetic resonance imaging and magnetic resonance angiography ( mri / mra ) of the brain [ 7 , 9 ]  . 
3 , all the stenoses of time ( 6 and the intracranial vessels worsened over 12 months follow - up mri / mra scans ) leading to a moya - moya disease clearly evident on the third followfig . 
three - dimensional time - of - ight ( 3d tof ) sequence , maximum intensity projection ( mip ) reconstruction - axial the left middle cerebral artery with view shows occlusion of hypertrophy of the ipsilateral middle meningeal artery up scan . 
1 , 2 , 4 , and 6 , in keeping with the majority of studies on nf1 - related brain vasculopathy , had no neurological signs or symptoms that could be related to the arterial stenoses , while patient no . 
3 had developed a severe mental retardation ( in connection with the worsening of the stenosis of the intracranial vessels )  . on t2 - weighted images all of the six patients showed the typical unidentied bright objects ( ubos ) also known as neurobromatosis bright objects ( nbos ) [ 10 ]  . 
 [ 6 ] classied the nf1 - associated vascular lesions into three types : stenotic , aneurysmal and mixed . all our patients had only stenotic lesions , a nding in agreement with rea et al . 
3d tof coronal mip reconstruction ( left ) shows complete bilateral disappearance of the supraclinoid internal carotid arteries and of the right posterior cerebral artery , with many secondary collaterals , delineating a typical feature of moya - moya syndrome ( puff of smoke ) , more evident on the right side . 
thus , children with nf1 have a far greater risk of having stenotic rather than aneurysmal lesions ( which have been described but are very rare [ 29 ] ) , at least in the cerebral circulation . to our knowledge , there are only ve papers investigating the prevalence of cerebral arteriopathy in populations of patients with a clinical diagnosis of nf1 [ 79 , 27 , 28 ] and few case reports [ 24 , 25 ]  . 
 [ 9 ] , who studied the largest series of children with nf1 , found a prevalence of 6 % ( 17 / 266 children who underwent mri )  . 
cairns and north [ 8 ] reported seven patients with brain arteriopathy out of 144 nf1 children with a clinical indication for a brain mri scan ( 5 % )  . 
even in these two latter studies mra was only performed when vascular abnormalities had already been detected at mri . in our study , we presume that the presence of a wider age range ( 435 years ) does not constitute a bias . 
computed tomography ( ct ) angiography mip reconstruction of the extracranial tract of the right internal carotid artery clearly depicting a severe postbulbar stenosis frequency of vascular dysplasia in younger children [ 8 ] but it also well known that vascular stenosis may become progressive month to years after the diagnosis [ 9 ]  . regarding our higher prevalence of brain vasculopathy , it could be partially due to the fact that mra is not routinely performed in all patients with nf1 . 
mra is not included in the brain mr protocols of patient with nf1 , even in the studies focusing on nf1 - related vasculopathy . all the authors performed mra only when they noted direct or indirect signs of stenosis on mri examination [ 9 ]  . in particular , these were characterised by cortical strokes and / or white matter hyperintensities . 
therefore , mra is critical in detecting arterial narrowing of distal vessels of lesser calibre , which are undetectable by mri only . furthermore , in agreement with other authors , we found an increased prevalence of arteriopathy in patients with optic glioma , detected in four patients ( 66 % ) ; this could , however , result from a selection bias given that the patient 420 radiol med ( 2014 ) 119 : 415421 with optic glioma is often symptomatic and for this reason always undergoes mri examination [ 79 ]  . regarding the clinical status of our group of patients , only the intermittent headache of patient no . 
3 , although probably due to atrophy of the right fronto - sylvian region , could be also related to the fact that the patient had previously undergone radiotherapy for a large optic chiasm glioma . 
it is important to highlight that in all these studies the majority of patients did not have neurological symptoms related to the brain arteriopathy . we performed follow - up mri / mra examinations after 36 months and 1215 months in four patients with vascular dysplasia , nding only in patient no . 
3 that all the stenoses of the intracranial vessels had worsened over time ( 6 and 12 months follow - up mri / mra scans ) leading to a moya - moya disease clearly evident at the third followup scan . a longer follow - up , which is currently underway , is needed to obtain more information about the real progression of brain arteriopathy in patients with nf1 . 
there are no clear indications in the literature about the frequency of the follow - up in patients with nf1 - related vasculopathy because of the low incidence of the condition . 
in addition , we must consider the fact that mra extends the time of a brain mri examination by about 10 % only [ 9 ] , and that the costs of a permanent impairment due to a stroke could be very high . 
indeed the cost of care for a patient with a stroke in only the rst year after diagnosis has been estimated to be $42 , 338 [ 9 , 12 ]  . 
thus , the early identication of a cerebral vasculopathy could reduce the costs of long - term care , especially for children with lifelong disability from stroke . a possible bias in our study is linked to patient no . 
3 because she had previously ( at the age of 5 years ) been treated with radiotherapy for a right optic nerve glioma ( a procedure no longer indicated for treatment of optic gliomas in children [ 13 , 26 ] )  . 
the atrophy could be due either to the radiation therapy or to the right ica stenosis itself or to a coexistence of both the conditions [ 14 , 15 ]  . 
3 was located contralaterally to the irradiation eld , so that it was probably unrelated to the radiotherapy , and should be considered an incidental nding . conclusion we believe that the protocol for patients affected by nf1 with a clinical indication for brain mri should include an mra as well , so as to detect any stenoses of branches of the circle of willis including those of small and moderate degree . 
of these , 92 / 120 nodules ( 76.6 % ; mean diameter 18.4 mm ) showed the typical hcc vascular pattern : 90 / 92 nodules appeared hypointense and 2 / 92 were hyperintense on hepatobiliary phase images . 
an additional 28 / 120 hypointense , nonhypervascular nodules ( 23.3 % ; mean diameter 11 mm ) were detected on hepatobiliary phase images , 15 of which showed hypointensity also on the equilibrium phase images . 
david ospedale santandrea , via di grottarossa 1035 , 00189 rome , italy conclusions gadoxetic acid - enhanced mr imaging is useful for detecting hcc as well as hypovascular nodules with potential progression to hcc . 
it is therefore crucial to identify those patients at high risk of developing hcc by establishing a proper surveillance programme aimed at an early diagnosis . hepatocarcinogenesis should be considered a multistep process arising in a cirrhotic liver ; the tumour develops by evolving from a regenerative to a dysplastic nodule , progressing from an initially well - differentiated hcc ( early to a poorly differentiated hcc and nally to hcc ) undifferentiated neoplasia . 
nodules with a high grade of dysplasia represent pre - neoplastic lesions that evolve into hcc with a reported frequency of 4680 % over 15 years [ 2 ]  . in this scenario , it is important to use diagnostic techniques allowing for the early detection and characterisation 368 radiol med ( 2014 ) 119 : 367376 of focal liver lesions . 
dynamic computed tomography ( ct ) or magnetic resonance ( mr ) imaging , performed with an arterial contrast phase with extracellular contrast agents , are recommended by the american association for the study of liver disease ( aasld ) as the imaging techniques of choice for the detection and characterisation of hcc in cirrhotic patients [ 3 ]  . 
a nding of the typical vascular pattern of hcchypervascularity in the arterial phase , washout in the portal venous and / or equilibrium phasein nodules larger than 1 cm is considered diagnostic , and biopsy is not required . 
however , as a result of the lack of the typical tumour neoangiogenesis , well - differentiated early hccs may appear hypovascular in the arterial phase , and thus easily evade detection on dynamic ct or mr imaging [ 4 ]  . 
great interest is growing around the new mr imaging approaches to the liver and bile ducts made possible by the recent introduction of hepatocytespecic contrast agents , such as the gadoxetic acid disodium ( gd - eob - dtpa )  . 
this is a mixed paramagnetic contrast agent that combined the properties of vascularinterstitial agents and hepatobiliary agents , which are taken up by the hepatocytes and excreted through the biliary systea new imaging phasethe hepato - specic phaseacquired 1520 min after intravenous contrast injection is added to the standard dynamic study , and it seems to improve signicantly the diagnostic performance of mr imaging [ 5 , 6 ]  . the aim of our study was to assess the diagnostic accuracy of gadoxetic acid - enhanced mr imaging in the diagnosis of hcc and in the identication of early - stage lesions , evaluating the evolution and progression of the tumour . materials and methods study population fifty - six patients with hcv - , hbvor alcohol - related liver cirrhosis who underwent gadoxetic acid - enhanced dynamic mr imaging ( gd - eob - dtpa , primovist , bayer healthcare pharmaceuticals ) of the liver between march 2009 and july 2012 were retrospectively reviewed . 
the mr examinations were carried out to characterise indeterminate lesions found on ultrasonography ( us ) or dynamic ct scans performed within the previous 14 weeks , or to investigate elevated a - fetoprotein levels . the criteria for inclusion in the study were the following : ( 1 ) the presence of hypervascular nodules in the arterial phase with washout on the portal and / or equilibrium phase images , or presence of nodules with hypointensity on hepatobiliary phase images , ( 2 ) availability of at least 3 months of dynamic ct and / or gadoxetic acidenhanced mr imaging follow - up . 
the exclusion criteria were lesions with features of cysts , adenomas , focal nodular hyperplasia or haemangiomas ( n = 8 ) ; no evidence of focal liver lesion at mr imaging ( n = 3 ) ; no availability of mr or ct follow - up ( n = 4 )  . 
finally , 41 patients ( 30 men and 11 women ; age range 5287 years ; mean age 70 years ) with a total of 120 nodules were enrolled in the study . the diagnosis of hcc for nodules larger than 1 cm was made according to the aasld criteria of 2010 [ 3 ] , or was based on the histopathological ndings in surgical or biopsy specimens . 
histopathological examination of surgical or biopsy specimens was carried out in seven patients with nodules showing the typical vascular pattern but smaller than 1 cm in size or appearing hyperintense in the hepatobiliary phase . 
the other non - hcc nodules detected during the study underwent gadoxetic acid - enhanced mr imaging follow - up every 3 months for at least 12 months . this retrospective study was approved by the institutional review board of our hospital and informed consent was obtained from all patients . mr imaging protocol mr imaging was performed using a 1.5 - tesla scanner ( sonata siemens , erlangen , germany ) , with a phased - array body surface coil . 
axial t1weighted gradient echo in - phase and out - of - phase and t2weighted turbo spin - echo fat - saturated ( tse - fs ) sequences were obtained as baseline mr images . 
subsequently , volumetric interpolated breath - hold examinations ( vibe ) were acquired before and after intravenous bolus injection of 0.025 mmol / kg of body weight of gd - eob - dtpa , at a rate of 0.81 ml / s , followed by a 10 - cc saline ush at the same injection rate . 
arterial phase images were obtained 2535 s after the contrast medium injection ; portal venous phase and equilibrium phase images were obtained 7080 and 150180 s , the contrast agent injection . 
hepatobiliary phase images were acquired with a delay of 15 and 20 min after gd - eob - dtpa injection , using a vibe sequence ( axial and coronal planes ) and a fat - saturated 2d t1 - weighted high - resolution fast lowangle shot ( flash ) sequence . 
to reduce the examination time , t2 - weighted half - fourier acquisition single - shot ( haste ) fs and t2 - weighted respiratory - triggered tsefs sequences were performed in the interval between the dynamic and hepatobiliary phases . 
the same assessment was performed throughout the follow - up period . a lesion was considered as being an hcc when it showed the following characteristics : ( 1 ) a nodule larger than 10 mm displaying the typical vascular pattern for hcc according to the aasld criteria [ 3 ] ( contrast enhancement on arterial phase , washout on portal and / or equilibrium phase images ) ; ( 2 ) hypointense or hyperintense lesions on hepatobiliary phase images with typical vascular pattern on dynamic mr imaging . a lesion was dened as a dysplastic nodule / early hcc when it showed the following characteristics : ( 1 ) nodule showing hypointensity only on hepatobiliary phase images ; ( 2 ) lesions without hypervascularity on arterial phase images , showing hypointensity on equilibrium ( 150180 s ) and hepatobiliary phase images . statistical analysis statistical analysis was performed using systat software on the group of patients with dysplastic nodules / early hcc . continuous variables were analysed using descriptive statistics . 
given the small sample size , proportions were compared using the nonparametric fishers exact test . a total of 120 nodules were detected in 41 patients ( table 2 )  . 
none of the remaining seven nodules ( 46.6 % ; size range 413 mm ; mean size 8 mm ) showed evolution over the 3to 12 - month follow - up . 
of these six , three were larger than 1 cm at the rst examination , whereas the remaining three were 10 , 10 and 7 mm in size at the rst examination and increased in size ( [ 1 cm ) over the follow - up period . 
at the rst examination , 11 / 28 nodules of the second group were larger than 1 cm in size and 9 / 11 ( 81.8 % ) developed hcc during the follow - up period . 
2 dynamic contrastenhanced mr images show a focal liver lesion ( arrow ) , 20 mm in size , with early arterial enhancement ( a ) and washout in the portal ( b ) and equilibrium phase images ( c )  . the hepatobiliary phase axial ( d ) and coronal ( e ) images show hyperintense nodule ( arrow ) , implying gadoxetic acid uptake . f the histological result shows well - differentiated hcc ( haematoxylineosin stain ) discussion the crucial role of imaging in the evaluation of liver cirrhosis and diagnosis of hcc has already been established as critical improving patient management . 
however , curative treatments at the time of diagnosis , such as liver transplantation , liver resection or loco - regional therapies , are achievable only in a limited number of patients [ 3 , 7 , 8 ]  . mr imaging with its intrinsic high - contrast resolution may be seen as a problem - solving tool , and is now recognised as an accurate method in the study of the liver , with high sensitivity and specicity in the detection and characterisation of focal liver lesions . 
nevertheless , conventional dynamic imaging with extracellular contrast agents may at times provide inconclusive ndings in the characterisation of focal liver lesions . gadoxetic acid disodium ( gd - eob - dtpa ) is a contrast agent characterised by a biphasic nature : approximately 50 % of the administered gd - eob - dtpa is taken up by normal hepatocytes and subsequently excreted into the 372 fig . 
a hypointense nodule ( white arrow ) , 12 mm in size , is seen in the equilibrium phase image ( b )  . c hepatobiliary phase image demonstrates two hypointense nodules ( black arrows ) radiol med ( 2014 ) 119 : 367376 biliary tract , while the remaining 50 % is excreted via the kidney ; therefore , it combines the properties of a conventional extracellular uid contrast agent , allowing accurate dynamic assessment of lesion vascularity , and of a hepatobiliary agent , accumulating in hepatocytes during the information hepatobiliary phase , providing functional about the presence or absence of functioning hepatocytes within the lesion [ 9 ]  . 
the hepatobiliary phase is obtained at 1520 min after intravenous injection of the contrast agent . recent studies [ 1015 ] have shown that the use of gdeob - dtpa does not signicantly increase examination time : gadoxetic acid does not cause signicant effects on t2 - weighted images or dw images , which can therefore be performed immediately after the dynamic study with a total examination time of about 2530 min . in our study , 92 / 120 nodules showed a typical vascular pattern for hcc with enhancement on arterial phase and rapid washout on portal and / or equilibrium phase images . this behaviour is considered pathognomonic for hcc due to a process of arterialisation of the nodule : as its dimension increases , perfusion of the neoplastic lesion is ensured by the development of unpaired arteries originating from the hepatic artery , while the contribution from the portal blood ow is reduced . 
in the hepatobiliary phase , 90 nodules ( 97 % ) appeared hypointense compared to the surrounding liver parenchyma , suggesting the lack of functional hepatocytes , and conrming the diagnosis of hcc . 
hypointensity on hepatobiliary phase images is strongly suggestive of hcc [ 9 , 13 ]  . it should be noted that , in our experience , none of the 92 hypervascular nodules appeared isointense on portal or equilibrium phase images . 
on mr imaging or ct performed using an extracellular contrast agent , small hccs often appear isointense [ 13 , 14 ] causing uncertain differential diagnoses with non - neoplastic arterial - enhancing pseudolesions commonly found in cirrhotic liver , such as arterioportal shunts . 
this behaviour might be caused by the increase in signal intensity of the liver parenchyma already in the portal phase , thanks to the early hepatic uptake of gadoxetic acid , which highlights even faint contrast differences between focal lesions and the liver parenchyma . 
in this group of lesions , the added value of the hepatobiliary phase , compared with dynamic mr imaging , leads to an increase in the diagnostic condence for hcc ; however , it must be emphasised that the failure to nd equivocally isointense nodules during the equilibrium phase is not of secondary importance in that it reduces the incidence of interpretation errors and false negative results . 373 radiol med ( 2014 ) 119 : 367376 fig . 
recent studies [ 16 , 17 ] have demonstrated that gadoxetic acid is transported into the hepatocytes through organic anion transporting polypeptides ( oatps ) and that increased expression of this carrier is responsible for the uptake of contrast agent by well - differentiated hcc . the most interesting nding of our study concerns the group of 28 hypovascular nodules showing hypointensity on hepatobiliary phase images . 
the surveillance programme showed an evolution of 17 / 28 ( 60.7 % ) of these nodules and a process of arterialisation in 14 nodules ( 50 % ) during the 3to 12 - month follow - up . 
in these 14 lesions , the diagnosis of hcc was achieved thanks to evidence of a typical hcc vascular pattern in a nodule larger than 1 cthese ndings are explained by the multistep carcinogenesis process : at the beginning , portal perfusion is still present with no evidence of dominant arterial blood supply ; the portal blood supply then decreases and the development of neoangiogenesis typical of hcc is subsequently evident . 
the hypovascular nodule , without enhancement in the arterial phase and detected due to hypointensity in the portal and equilibrium phase images , can be dened as an early - stage tumour or as early hcc [ 18 , 19 ]  . in our study , the progression to hypervascular hcc was also observed among nodules that appeared hypointense radiol med ( 2014 ) 119 : 367376 fig . 
no focal lesions are depicted in either the arterial ( a ) or equilibrium phase ( b ) images . c hepatobiliary phase image shows 12 mm hypointense nodule ( arrow )  . 
furthermore , our results demonstrated that hypointense nodules on hepatobiliary phase images , greater than 10 mm in size , are at a higher risk of developing hcc than are lesions less than 10 mm in diameter . 
caiazzo mri research center sun - fism , second university of naples , c / o hermitage clinics , via cupa le tozzole , 80138 naples , italy results conrm previous conclusions our reports regarding the increase in vrsd in nonactive phases of ms and support the immunological role of the vrs within the central nervous systethe lack of correlation between vrsd and the degree of gca and their prevailing localisation in atypical sites in ms patients make vrsd a potential marker of inammatory - demyelinating disease . keywords perivascular spaces ( cid : 2 ) virchowrobin spaces ( cid : 2 ) multiple sclerosis ( cid : 2 ) magnetic resonance introduction virchowrobin spaces ( vrs ) are small , pial - lined , interstitial uid - lled channels that house small vessels in their subarachnoid intracerebral course and may be involved in inammatory brain events [ 1 , 2 ]  . 
they are physiological ndings in magnetic resonance ( mr ) studies and , according to some authors [ 57 ] , they are present in 100 % of subjects . vrs are dened as dilated if their short axis is greater than 2 mm [ 5 , 8 ] or , according to some authors , greater than 3 mm [ 6 ]  . 
this is the reason why the number and size of vrs may change in the course of inammatory diseases such as multiple sclerosis ( ms ) [ 1 , 2 , 10 ]  . 
the exclusion criteria were : relapses either ongoing or occurring in the month before the examination , corticosteroid therapy in the month before the examination , presence of other neurological diseases , contraindications to the mr study . 
using this fast and accurate semi - automatic postprocessing application the vrsd of all the patients and controls were identied and evaluated in terms of their morphological and volumetric features and their signal . each individual vrs was identied and manually circumscribed through the placement of a volume of interest ( voi ) with semi - automatic delineation of the contours . 
1 mipav ( medical image processing , analysis and visualisation ) system display screen , with co - registered t1w , t2w and flair sequences and magnied views of the dilated virchowrobin spaces on t2w and t1w images . 
then we calculated the ratio between the three different parts of the brain so as to obtain the brain parenchyma fraction ( bpf ratio ) , an expression of the degree of global cerebral atrophy ( gca )  . statistical analysis the student t test was used to evaluate differences between the ms patients ( msnd and msd ) and the healthy volunteers in terms of vrsd volume , number , and sites , and fig . 
type i is commonly seen at the substantia perforata and anterior commissure along the course of the lenticulostriate arteries : a t2w , b t1w , c flair ( uid attenuated inversion recovery )  . type ii occurs in the white matter of the convexity and semioval centres , along the path of the perforating medullary arteries : d t2w , e t1w , f flair . 
a statistically as regards vrsd distribution , in ms patients the vrsd with typical locations were predominant in the anterior perforated substance ( type i ) compared with the convexity ( type ii ) ; there were no cases of vrsd in the midbrain ( type difference iii ) ( p = 0.0069 ) was found in the frequency of vrsd location at atypical sites : 34 vrsd in ms patients vs one vrsd in controls . 
the fisher test revealed that vrsd location was independent ( p = 0.93 , p = 0.51 ) of the clinical form of disease ( msnd vs msd )  . 
table 2 describes the data in detail . signicant correlation with global cerebral atrophy the volume and number of vrsd , both in patients and controls , are not dependent on the degree of gca , expressed in terms of bpf . 
conversely , with mr imaging , and especially with high - eld mr imaging [ 6 , 19 ] , vrs are routinely observed along the course of intracerebral arteries , arterioles , venules and veins [ 9 , 20 ]  . 
here , the arterioles have an angled trajectory and multiple grouped branches , with a prevalence twice as high [ 10 ] compared to the distal branches of the middle cerebral artery and ten times higher compared to the distal lenticulostriate arteries [ 10 ]  . the immunological rationale for vrs was rst proposed by w . 
his in 1865 , who considered them to be lymphatic spaces of the cns on account of both their structure and cell content ; their relationship with the immune system was further explored in later studies . human brain studies using tracers and histopathological analyses conrm that , in addition to transporting solutes , soluble proteins and leukocytes [ 2 ] , vrs are physiologically [ 6 ] a real route for cerebral lymphatic drainage between the periarterial space and the lymphatic system [ 12 ] , and are implicated in the case of bloodbrain barrier abnormality and inammation [ 18 ]  . 
histopathological studies demonstrate that , in normal conditions , vrs contain , in addition to dendritic cells and perivascular microglia , macrophages and t cells , which give them a key role in immune surveillance [ 2 ]  . the macrophages contained in vrs , besides adjusting some proteins involved in inammatory processes ( mch class ii , interleukins - 1b ) , have contact with the circulating t lymphocytes [ 12 ] from which the immune response starts the periphery of the [ 5 ]  . 
t cell activation begins at radiol med ( 2014 ) 119 : 408414 lymphoid compartment ( extracerebral area ) and then reaches the cns , with the t cells circulating in the vrs [ 2 ]  . immunohistochemical studies compared to post - mortem brain mr imaging studies of patients with demyelinating disease demonstrate the presence in the vrs of cd68positive macrophages in all stages of demyelinating lesions , with perivascular leukocyte inltrates , much more frequent in chronic inactive lesions than in active lesions [ 17 ] and vrs have also been described in experimental ms models [ 2 , 17 ]  . in spite of the growing interest for the role of vrs in immune surveillance , until recently they were underestimated [ 2 ]  . 
ms , a chronic inammatory disease of the cns , is characterised by the presence of immune cells in brain parenchyma , with local inammation , demyelinating lesions and axonal and neuronal damage [ 2 ] and this would in patients with active ms , brain mr explain why , imaging shows dilation of the vrs , which are reserves of inammatory cells [ 6 , 18 ]  . it has been hypothesised that the inammatory activity in ms occurs in the vrs , leading to their increase in size due to inltration by inammatory cells and oedema , resulting in a greater number of vrs being visible in mr imaging studies of the brathis is conrmed by a longitudinal study [ 2 ] which found a signicant increase in both the volume and number of vrs in patients with active ms compared to healthy controls , suggesting the immunological role of vrs in active demyelinating disease , or when the bloodbrain barrier was damaged [ 18 ]  . 
more recent studies indicate nonspecic vrs enlargements as a sign of ms inammatory changes , having observed bihemispheric white matter vrs in 55 % of ms patients and , in 85 % of cases , a vrs number greater than four [ 3 , 4 ]  . in our study , we identied more than four vrsd in each ms patient in 12.5 % of the cases compared with controls ( 0 of 30 subjects ) and more than three vrsd for each ms patient in 17.5 % of the cases compared to controls ( 0 of 30 )  . 
this discrepancy is probably due to the different cutoff size used in our study . unlike previous studies [ 2 ] , in which the number of vrs did not differ between ms patients and healthy subjects in any region of the brain , our study found not only a statistically higher number of vrsd in ms patients compared to controls , but also a signicant increase in the volume and area of the vrsd . we also found a signicantly higher number of vrsd in these ndings may ms patients ; related methodological differences since we only considered vrs with a diameter greater than 2 mm or to differences in the population examined , having assessed only nonacute phase ms patients . the considerable increase in our study in vrsd number , area and volume in patients with nonactive ms compared to controls could result from the possibility of identifying a larger number of perivascular spaces due to their expansion rather than reecting a real increase in their number . another important nding in our study , not previously reported in the literature , is the identication in the group of ms patients compared to healthy controls of a greater number of statistically signicant vrsd located in atypical sites . 
this nding of uncertain signicance could be explained with the need , in this category of patients , of alternative or supplementary cerebral lymphatic drainage pathways , compared with conventional areas . conclusions our mr imaging study of the brain , performed with a 3t system in patients with nonactive ms compared with a group of healthy controls shows that the area , volume and number of dilated vrs are signicantly higher in ms patients than in controls , conrming previous reports of brain mr imaging studies carried out with less powerful equipment and in patients with active ms . the signicance of this nding is validated by the lack of correlation between vrs and bpf , both for ms patients and for control subjects , which rules out any inuence of gca . 
no signicant intragroup difference was observed in the volume and number of vrsd based on degree of disability ( msnd and msd )  . unlike previous investigators [ 13 ] , we did not observe a signicant prevalence in the shape of vrsd ( round or oval ) between patients and controls , the round shape prevailing in both groups . 
the wilcoxon test was used for comparisons . results the least difference between artefact extent and actual valve size ( 0.1 mm ) was obtained with a steady - state free precession ( ssfp ) sequence . 
no signicant differences were found comparing the pg measured with cmr , echocardiography and catheter . conclusions we showed in vitro that the ssfp sequence produced the most accurate valve measurement . 
after ppvi , cmr showed a strong decrease of pg and rf with a signicant improvement of rv function . keywords congenital heart diseases ( cid : 2 ) cardiac magnetic resonance ( cmr ) ( cid : 2 ) percutaneous pulmonary valve implantation ( ppvi ) ( cid : 2 ) right ventricle ( rv ) ( cid : 2 ) pulmonary artery ( pa ) introduction patients with congenital heart defects are usually treated in the rst year of life and they may also undergo multiple surgical interventions over the life course [ 1 ]  . 
malan , 20097 san donato milanese , milan , italy radiol med ( 2014 ) 119 : 400407 implanted to repair numerous congenital heart defects [ 2 ]  . however , the good function of conduits is limited during the life of these patients and multiple re - interventions are often required . 
as a consequence , a surgical procedure may be performed too late for a good rv function recovery [ 7 ]  . in the last decade , bonhoeffer et al . 
 [ 8 ] developed a new approach to treat the rv conduit dysfunction such as stenosis and / or regurgitation : a noninvasive percutaneous pulmonary valve implantation ( ppvi ) using a bovine valve sutured on a platinumiridium alloy stent , with welded joints of gold ( melody , medtronic , inc . , minneapolis , mn , usa )  . 
this assessment may be performed using echocardiography as a rst - line technique . however , cmr has been demonstrated to largely outperform echocardiography in the evaluation of cardiac chambers , in particular the rv , and it is considered as a rst - choice technique in this setting [ 13 ]  . 
moreover , no the pulmonary pressure study has reported data about gradient ( pg ) measured by cmr in these patients . in this study , we rst report the results of a preliminary in vitro mr study of the melody valve aimed at measuring the extent of artefact . 
all 27 patients underwent cmr before ppvi but not all patients performed all the three cmrs after ppvi : 13 / 27 patients were studied after 1 month , 20 / 27 after 3 months , and 21 / 27 after 6 months . cmr protocol we used a 1.5 - t unit with 40 - mt / m gradient power ( magnetom sonata maestro class , siemens , erlangen , germany ) and a four - channel cardio - thoracic phased - array coil . 
before ppvi , the slice was located in the pulmonary conduit , perpendicular to the vessel long axis , immediately distal to the valve ; after ppvi , the slice was located 4 mm distal to the stent artefact . before the implanting valve procedure [ 10 ]  . 
before and 3 months after ppvi conduit , the mean pulmonary pg was calculated with echocardiography by tracing the border of continuous - wave spectral doppler recordings and integrating the area under the curve . 
maximum instantaneous pg was also estimated by echocardiography [ 16 ]  . statistical analysis differences between the two readers of the in vitro study were tested with the wilcoxon test . 
2. catheterisation and echocardiography in vivo study the peak - to - peak rvpa gradient was calculated during the interventional procedure as the difference in systolic pressure between rv outow tract and main pa distal to the conduit all cmr examinations were diagnostic , with metallic artefacts limited to the valve inner space as shown in fig . 
regarding the lv , no signicant differences were found in terms of esvi respectively ; after ppvi , table 2 patients characteristics and spectrum of diseases mean males females total original diagnosis tetralogy of fallot aortic valve disease ( ross procedure ) transposition of great arteries double outlet right ventricle truncus arteriosus pulmonary atresia pulmonary stenosis total rvot conduit type homograft shelhigh matrix hancock contegra monocuspid homograft ionescu - shiley conduit not implanted total rvot right ventricle outow tract , sd standard deviation of the lv and ejection fraction . 
this in vitro / in vivo study showed that : ( 1 ) the artefact from mr sequences is sufciently small not to inuence qualitative and quantitative mr evaluation after ppvi and ( 2 ) there is a signicant reduction in pg and rf and a signicant increase in rv function . single - shot acquisition the low interobserver variability of the artefact size ( cov 3.44.6 % ) showed the reliability of our measurements . 
looking at the artefact size , we showed that ssfp , spin - echo half - fourier ( haste ) , and turbo spin - echo ( tse ) sequences produced the most accurate valve measurement , i.e. 
this means that these mr sequences are suitable for clinical evaluation of the heart with a melody valve , as previously demonstrated for different types of vessel stents in an in vitro model [ 17 ]  . turbo in the in vivo study , we evaluated the pre - treatment and follow - up cmr study of patients treated with a ppvi . 
evolution of right ( rv ) and left ventricle ( lv ) end - diastolic volume index ( edvi ) and end - systolic volume index ( esvi ) up to 6 months after the percutaneous pulmonary valve implantation differences were found for lv . 
however , cmr is commonly considered more reproducible than echocardiography in the evaluation of the right chambers , rv outow tract and pulmonary artery [ 13 , 18 ]  . 
the last limitation is that there is no comparison with a different pulmonary valve stent . in conclusion , the signal void produced in vitro by the metallic structure of melody pulmonary valve is limited to its inner space with a maximal extent to the external space equal to \5 mmoreover , cmr evaluation of patients after 6 months from ppvi shows a drastic decrease of rf and pg and a signicant improvement of all rv parameters . 
pomerri radiologia oncologica , iov , ircss , via gattamelata , 35128 padua , italy radiological documentation ( hrct ) of disease , clinical and radiological follow - up of 1 year and the beginning of any therapy within 1 month from the diagnosis . results among subjects not receiving therapy , the comparison between the two groups showed that the radiological ndings remained stable in subjects with a typical pattern , while they worsened in more than 70 % of cases with atypical appearance . 
re - evaluation of hrct within 1 year revealed no correlation between clinical deterioration and radiological changes . conclusions the ndings of this study suggest that persistence of the inammatory process rather than the radiological pattern at onset is a prognostic factor for recurrence . keywords sarcoidosis ( cid : 2 ) nodular sarcoidosis ( cid : 2 ) hrct introduction sarcoidosis is a multisystem granulomatous syndrome of unknown aetiology . 
it is ubiquitous and has almost equal sex , race and age distribution , with a slight higher prevalence among african american women . it usually affects adults younger than 40 , with a peak in the age group from 20 to 40 years . 
in italy , the prevalence is about 10 per 1 , 00 , 000 population [ 1 ]  . pulmonary involvement with hilar lymphadenopathy is by far the most common manifestation followed by lesions of the eyes and skin ; other organs may also be involved ( liver , spleen , salivary glands , heart , nervous system , radiol med ( 2014 ) 119 : 384392 muscles and bones )  . 
a sudden onset presenting with only erythema nodosum or asymptomatic bilateral hilar lymph node enlargement may predict a self - limiting course , whereas subtle symptoms and the presence of multiple nonpulmonary lesions could lead to progressive brosis of the lungs or of other organs . 
the overall mortality rate is between 1 and 5 % [ 24 ]  . imaging investigations are used to conrm a clinical suspicion , and chest x - ray is always the rst test to be performed . 
high - resolution computed tomography ( hrct ) has 95 % sensitivity and a 99 % specicity , and it enables detection of lung abnormalities which might be missed on a plain lm [ 5 , 6 ]  . 
it has indeed been demonstrated that 15 % of symptomatic patients have normal chest x - ray but pathological ndings on ct scans [ 7 ]  . pulmonary sarcoidosis is typically classied in stages on the basis of the interstitial and hilar - mediastinal abnormalities seen on chest x - ray ( stage 0 : normal ; stage i : bilateral hilar lymph node enlargement with or without paratracheal lymphadenopathy , not associated with visible lung disease ; stage ii : bilateral hilar lymph node enlargement associated with visible lung disease ; stage iii : diffuse lung disease without lymph node enlargement ; stage iv : lung brosis with honeycombing pattern ) [ 1 , 7 ]  . the therapeutic approach is still debated . 
the study compares the incidence of typical and atypical sarcoidosis and the clinical and radiological differences in disease progression between these two groups ; nally , it evaluates whether pharmacological therapy can inuence the evolution of the disease , on the basis of the radiological patterns . materials and methods we retrospectively reviewed the clinical and radiological records of 350 patients with a proven diagnosis of pulmonary sarcoidosis , who were assessed at the institute of immunology and haematology from 1997 to 2010 . inclusion criteria were an hrct study at the time of diagnosis or during an active phase of disease ; diagnosis established by histopathology or immunophenotype analysis on bronchoalveolar lavage ( bal ) ; a 1 - year clinical and radiological follow - up ( the same amount of time for treated and untreated patients ) ; initiation of therapy within 1 month of the diagnosis , in the case of treated patients . patients with a brotic hrct pattern were excluded because of the irreversibility of the ndings . most patients showed a clinical and radiological improvement by the early phase of the follow - up , and only a minority who experienced a relapse or worsening clinical conditions underwent further radiological re - evaluation . therefore , in patients with stable or improved clinical status during the rst year of the follow - up , we assessed the clinical evolution of the disease . 
in patients who developed a clinical relapse and underwent radiological re - evaluation , we assessed the correlation between clinical worsening and the radiological ndings . on the basis of the above inclusion criteria , a total of 56 patients were selected ( 23 males and 33 females ; average age , 49.8 years ; range 2972 years ; all caucasian )  . 
according to the hrct pattern , the patients were classied as being affected by typical or atypical sarcoidosis [ 9 ] ( table 1 )  . table 1 typical and atypical hrct characteristics of pulmonary sarcoidosis in 56 patients typical pattern ( 39 patients ) lymph node enlargement : hilar , bilateral , symmetric and mediastinal ( right paratracheal ) nodules : micronodules ( 14 mm in diameter , well dened , bilateral ) , they can coalesce perilymphatic distribution : peribronchovascular , subpleural , interlobular septa thickening of the interlobular septa mainly distributed in upper lobes and middle lobe ground glass associated with nodules atypical pattern ( 17 patients ) large nodules or masses ( 14 cm in diameter , ill dened , multiple , bilateral ) , with or without air bronchogram galaxy sign lymph node enlargement : as in the typical pattern 386 radiol med ( 2014 ) 119 : 384392 table 2 hrct pattern of typical and atypical sarcoidosis in examined patients typical pattern ( 39 patients ) lymph nodes ( ln ) lymph nodes ? reticulo - nodular ( ln ? rn ) lymph nodes ? reticulo - nodular ? ground glass ( ln ? rn ? gg ) reticulo - nodular ? ground glass ( n ? gg ) atypical pattern ( 17 patients ) lymph nodes ? large nodules / masses ( ln ? nm ) large nodules / masses ( nm ) remission , stability or worsening of the disease was dened on the basis of this comparison . the patients exhibiting typical and atypical sarcoidosis imaging patterns were subdivided into patients who received therapy ( steroids , antimalarial drugs or immunosuppressants ) and those who did not . the clinical course was then analysed in treated and untreated patients , evaluating again improvement / remission , stability or worsening of the symptoms . 
ground - glass opacities superimposed on the reticulonodular pattern . for atypical sarcoidosis , the hrct features considered were large nodules and masses , alone or associated with enlarged lymph nodes ( 14 cm in diameter , large illdened opacities on ct )  . 
small satellite nodules are often visible at the periphery of these masses , leading to the galaxy sign appearance [ 10 ]  . the two main patterns were further divided into subtypes : four subtypes for the typical group and two for the atypical group ( table 2 )  . for the typical pattern , we considered the following abnormalities : lymph nodes ( ln ) lymph nodes ? reticulo - nodular pattern ( ln ? rn ) lymph glass ( ln ? rn ? gg ) reticulo - nodular pattern ? ground glass ( rn ? gg )  . nodes ? reticulo - nodular pattern ? ground for the atypical pattern , the abnormalities considered lymph nodes ? large nodules / masses ( ln ? nm ) large nodules / masses ( nm )  . the course of the radiological picture was assessed by comparing the hrct studies performed at the time of diagnosis with those obtained within 1 year . 
improvement / were : of the 56 patients selected , 39 ( 69.6 % ) had a typical sarcoidosis pattern , whereas 17 ( 30.3 % ) had an atypical pattern . 
among the group with atypical pattern ( n = 17 ) , two patients ( 11.7 % ) presented with respiratory symptoms , nine patients ( 52.9 % ) had extrapulmonary / systemic symptoms , four patients ( 23.5 % ) had pulmonary and extrapulmonary complaints , and two patients ( 11.7 % ) were asymptomatic . the clinical features are listed in table 3 . treatment regimen ( steroids , hydroxychloroquine / chloroquine , methotrexate , singularly or combined ) was administered to 44 ( 78.5 % ) patients : 31 ( 79.4 % ) of them showed a typical radiological pattern , a specic radiol med ( 2014 ) 119 : 384392 fig . 
1 radiological patterns of patients included in the study table 3 characteristics of patients sarcoidosis number of patients mean age ( years ) gender m / f diagnosis made by biopsy / bal pulmonary symptoms pulmonary ? extrapulmonary / systemic symptoms extrapulmonary and / or systemic symptoms asymptomatic typical therapy 11 / 20 27 / 4 atypical therapy 12 / 1 no therapy no therapy table 4 clinical evolution of treated patients resolved symptoms chronic symptoms typical atypical 25 ( 80.6 % ) 10 ( 77 % ) 6 ( 19.4 % ) 3 ( 3 % ) whereas 13 ( 76.4 % ) had an atypical one . 
treatment decisions were based on the reported symptoms and on the involvement of specic organs . spontaneous remission was observed in 10 / 12 ( 83.3 % ) patients who did not receive pharmacological treatment . only two patients affected by typical sarcoidosis ( dry cough ) reported an improvement of the symptoms but not a complete remission . in the typical pattern group , 25 patients ( 80.6 % ) demonstrated complete recovery after therapy , whereas six patients ( 19.4 % ) showed only a mild response . 
2 first high - resolution computed tomography ( hrct ) study . large parenchymal consolidation with air bronchogram in both upper lobes ( a , b ) , with galaxy sign ( arrow ) and small nodules with perilymphatic distribution ( arrowhead )  . 
follow - up hrct after therapy with hydroxychloroquine and steroids , and 1 year of improvement of dyspnea : marked reduction of the consolidations , but progression to brosis in the same location ( c , d ) , with traction bronchiectasis and retraction of ssures table 5 radiological evolution of treated patients remission stability progression typical atypical 16 ( 36.4 % ) 3 ( 6.8 % ) 11 ( 25 % ) 7 ( 15.9 % ) 4 ( 9.1 % ) 3 ( 6.8 % ) prognosis for those with medically treated atypical sarcoidosis ( p = ns )  . 
clinical manifestations subsided in 25 patients with a typical pattern and 21 of them ( 84 % ) further improved or remained stable during the follow - up , whereas 4 worsened . as for the atypical group , of the 10 patients who reported regression of the symptoms , 7 ( 70 % ) had concordant hrct ndings , whereas in 7 patients imaging revealed an aggravation . the hrct pattern was stable or better in all of the nine untreated patients with typical and atypical pattern who reported stationary clinical condition . the course of all the radiological subtypes of typical sarcoidosis was investigated to evaluate whether they could correlate with the prognosis . regression or stability was found in 10 / 11 ( 90.9 % ) patients with a ln ( lymph node involvement ) radiological pattern ( eight of them treated and two untreated )  . 
only one untreated radiological worsening . showed clinical patient extrapulmonary symptoms progressed in two treated patients ( 15.4 % ) with an atypical pattern , whereas the imaging features remained stable ; none of the untreated patient with atypical pattern relapsed or worsened . discussion the radiological abnormalities of sarcoidosis are usually well dened and they include hilar bilateral lymph node enlargement and lung disease , alone or in combination . 
nodules measuring 2 and 5 mm can be seen in both upper lobes ( a , arrows )  . minimum nodular thickening of the septa in the apical segment of the right upper lobe and nodules along the ssures in the upper lobes bilaterally ( b , arrow )  . 
appearance of another nodule in the right upper lobe ( c , arrow ) and increased perilymphatic nodular pattern in the right apex 390 radiol med ( 2014 ) 119 : 384392 typical pattern of sarcoidosis consists of small nodules along the lymphatics in the peribronchovascular interstitial space , sometimes mildly thickened , and in the interlobular septa ( perilymphatic distribution ) [ 11 ]  . 
in this situation , the differential diagnosis is challenging [ 12 ]  . several previous studies have evaluated the prognostic signicance of the radiographic signs of sarcoidosis [ 13 , 14 ]  . the detection of ground - glass opacities , nodules and thickening of the interlobular septa suggests a possible resolution , whereas honeycombing indicates an irreversible course . it is unclear whether the evolution of the typical and atypical patterns is inuenced by sarcoidosis therapy and table 6 radiological evolution of untreated patients remission stability progression typical atypical 3 ( 25 % ) 1 ( 33 % ) 5 ( 41.67 % ) 3 ( 25 % ) stable whether the nding of specic patterns can guide decisions to initiate immunosuppressive treatment . 
5 first hrct study in a patient with dyspnoea and dry cough . typical pattern with perilymphatic nodules in the upper lobes , tending to coalesce in the left parahilar region ( a , b )  . 
marked increase of nodular pattern ( c ) with initial reduction in volume of the right upper lobe ( d ) radiol med ( 2014 ) 119 : 384392 the atypical abnormalities detected in our study were large nodules , masses or areas of pulmonary consolidation : all these features are potentially reversible with drugs . large nodules ( 14 cm in diameter ) were found in 1525 % of patients [ 9 , 10 ]  . in our study , 30 % of patients had an atypical radiological pattern , a nding consistent with the literature data [ 9 ]  . 
this nding seems to be conrmed by the study done by fazzi in 2003 [ 16 ] , in which steroids alone or associated with other drugs ( methotrexate or chloroquine ) were used to treat specic symptoms . 
the presence of clinical features requiring treatment is a greater risk factor for relapse than is the radiological pattern seen at onset . analysis of the efcacy of treatment on radiological progression demonstrates that immunosuppressants are more effective on the typical pattern : 50 % of the typical cases improved compared to 20 % of atypical cases , in which only stability was achieved . another interesting nding , even though partially limited by the small number of cases in our series , is that most of the untreated patients showed a stable radiological course . 
on the other hand , more than 70 % of the untreated patients with atypical appearance experienced a worsening . this result suggests that initiating treatment in patients with an atypical pattern , independently of clinical symptoms or from organ involvement , can arrest the progression of disease . treatment for typical cases should be decided on the basis of clinical parameters because the risk of relapse bears no relation to the radiological pattern . typical patients with lymph node enlargement and those with lung disease ( reticulo - nodular pattern and / or ground glass ) showed no important differences with regard to the progression of disease . 
on the contrary , other recent studies [ 14 ] suggest that ground - glass opacities could predict a chronic course of disease and could precede honeycombing changes . immunosuppressant clinical symptoms in both groups ( typical and atypical ) , leading to complete resolution in 80 % of the cases . therapy improved the our study also indicated that long - term radiological relapses are uncommon , whereas clinical relapses are more frequent ( typical and atypical )  . in conclusion , clinical relapse and worsening are not always related to a radiological progression , but they need to be analysed within the specic clinical context . 
the aim of this study was to investigate the knowledge of radiation exposure doses and risks among interns , resident doctors , and radiographers . materials and methods a questionnaire , consisting of 14 questions in multiple choice format , was distributed to 300 participants ( 100 interns , 100 radiographers , 100 resident doctors ) working in the emergency department . 
the questionnaire was designed to determine the participants knowledge about radiation - related hazards . results none of the radiation doses delivered by the imaging modalities was 100 % correctly estimated . 
this result could imply that we are not aware of the radiation risks , and we are inattentive in informing our patients about the radiation exposure related to the different imaging modalities . keywords radiation awareness ( cid : 2 ) radiological imaging ( cid : 2 ) emergency department ( cid : 2 ) ionising radiation doses introduction in emergency medicine practice , diagnostic imaging techniques and interventional radiological procedures are increasingly used to diagnose a wide range of diseases and injuries , and to provide life - saving treatment . 
according to the international commission on radiological protection ( icrp ) , understanding of the health effects of ionising radiation is central [ 3 ] , but the knowledge of doctors about radiological investigations using ionising radiation is inadequate [ 49 ] , regardless of the eld of expertise . the aim of this study was to investigate the knowledge of radiation exposure doses and risks among interns , resident doctors , and radiographers . materials and methods this prospective observational study was conducted in the emergency department of the ankara university school of medicine . 
the questionnaires , consisting of 14 questions in multiple choice format ( appendix ) , were selfadministered to 100 interns , 100 radiographers , 100 resident doctors ( 10 emergency medicine resident doctors , 10 radiology resident doctors , 40 general surgery resident doctors , and 40 internal medicine resident doctors )  . 
assuming that a single chest radiograph equalled one unit of radiation , the participants were asked to estimate the radiation dose that patients received during the different radiological imaging modalities . 
the participants marking correct intervals were grouped into the correct answer group , the ones who marked higher values into the more than equivalent number of chest x - ray ( overestimated ) group , and the ones who marked lower values were grouped into the less than equivalent number of chest x - ray ( underestimated ) group . 
participants who presented no opinion were grouped into the no idea group . the questionnaire was designed to determine the participants knowledge about the lifetime risks of inducing a fatal cancer , their knowledge of the selection of imaging modalities for pregnant patients , and their knowledge of risks for the foetus [ 11 ]  . 
when the p value obtained from the kruskalwallis anova test was statistically signicant , a multiple comparison test was used to assess which group differed from the others [ 12 ]  . 
a p value less than 0.05 was considered to be signicant . results the answers to the questions related to the radiation doses of various radiological examinations given by the study participants were grouped as correct , more than equivalent number of chest x - rays less than equivalent number of chest x - rays ( underestimated ) , and no idea . 
this was the highest rate for a correct answer , while 3 % stated that us used ionising radiation , and 4.3 % stated they had no idea on the radiation dose of the abdominal us . 
the answers given for the rst question are shown in table 3 . there was no statistically signicant difference between the groups in the rates of correct answers given for abdominal us and abdominal mri . 
when different imaging modalities for the same anatomical region were considered , none of the resident doctors correctly estimated all of the doses for the abdominal examination ( x - ray , us , ct , and mri ) , whereas only one intern correctly estimated the radiation doses in all of these modalities . 
while the correct answer to that question was a pelvic ct , the abdominal ct was the most frequently given answer by all of the participants . discussion it is important that doctors who request diagnostic imaging procedures , and radiographers who perform these requests , are well trained about radiation doses and the risks from radiation exposure . 
this is particularly signicant in the emergency department , because radiological investigations 444 radiol med ( 2014 ) 119 : 440447 using ionising radiation are an accepted part of emergency medicine , and emergency doctors rely heavily on medical imaging procedures in their daily practice . to the best of our knowledge , this is the rst study in turkey that compares resident doctors , interns , and radiographers knowledge about patient exposure to ionising radiation and its risks during radiological imaging examinations in the emergency department . in our study , none of the participants was able to correctly estimate the radiation doses in every single one of the nine different imaging modalities . 
these results were important since they show that the side effects of radiation exposure have potentially been underestimated by clinicians , resulting in an unnecessarily high number of orders . we found that there are still medical practitioners who fail to recognise mri and us as radiation - free modalities . this might be a decit in the knowledge of basic scientic principles . 
these results are consistent with previous studies which reported that the us and mri were associated with radiation by 411 % and 828 % of participants , respectively [ 8 , 9 , 11 , 13 ]  . another result in our study was that the radiographers had a statistically signicant rate of correct estimation of the radiation doses of different imaging studies based on the anatomical regions of the body when compared to other study groups . 
this can be explained by the most common body region for the radiological imaging being the abdomen , and the radiographers knowledge level in particular imaging studies for that body region . the vast majority of patients are unaware of the radiation dose that they are exposed to during radiological investigations and the associated risks [ 6 ]  . 
this is another indication of the radiographers being exposed to radiation at greater levels when compared with other study groups , and a higher level of knowledge about the side effects of radiation exposure and related safety measures to reduce these side effects . the knowledge of the radiology resident doctors is not as good as expected . 
 [ 6 ] mentioned that emergency department physicians did not perceive a possible increased cancer risk associated with a diagnostic ct scan , while nearly half of the radiologists did . 
in our study , we found that emergency resident doctors had a statistically signicantly higher rate of giving correct answers for the lowest and highest radiation sources for a foetus when compared with other groups . 
this may be the result of the more common use of radiological studies in emergency medicine practice , and an increased level of knowledge of the emergency resident doctors in the effects of radiation . our study showed that the doctors , interns , and radiographers knowledge of radiation exposure from radiological investigations and associated risks is poor . 
the question is to ask how knowledge can be improved in all of the emergency departments staff . attendance at training courses can be adequate for radiographers ; however , doctors are likely to benet from a mandatory curriculum on the effects and risks of radiation taught in medical schools . we believe that medical staff working in the emergency department should have this as basic knowledge ; x - rays should be ordered only for real medical indications and should be more cautiously used in paediatric and pregnant patients . 
in addition , the doctors should base their orders on whether the imaging examinations are appropriate to diagnose the patients clinical problems . furthermore , establishing continuous communication between emergency department and radiology staff , developing joint protocols for radiological interventions , and documenting radiation doses of different interventions on the order forms can increase the awareness among clinicians . to increase patients awareness of the effects and risks of radiation , attractive posters can be prepared and presented in the waiting rooms . 
also , presenting basic fact the topic and having an sheets to the patients about radiol med ( 2014 ) 119 : 440447 emergency doctor verbally explain the related risks prior to radiology orders can be helpful . the main limitation of the study is the heterogeneity among resident doctors . 
also , this study cannot be directly compared as the methodology and group of resident doctors / interns / radiographers are different , but it supports the global concern of substandard appreciation of radiation doses given to the patients . 
when the effective dose of a plain chest x - ray is considered 1 unit , how many units would a patient absorb in the following investigations ? 010 1050 50100 100500 [ idea conclusions radiological investigations using ionising radiation are an important part of emergency medicine . 
the main points about protection from the adverse effects of radiation are to educate clinicians and patients on the tolerable levels of radiation exposure , prevent overexposure by increasing awareness , consider irradiation - free modalities like us and mri when these are appropriate alternatives , and remember that all requests for imaging investigations should be expected to do more good than harm . acknowledgments the authors wish to thank atilla elhan for his assistance with the statistical interpretation of the data and nezaket o zgur for contributing to this research . cranial x - ray pelvic x - ray abdominal abdominal x - ray chest ct abdominal abdominal pelvic ct cranial ct 446 radiol med ( 2014 ) 119 : 440447 2 . 
when ordering a diagnostic radiological exam , do you notify your patients about the potential side effects of radiation prior to the examination ? ( ) yes ( ) no 4 . 
images were postprocessed with the software and evaluated independently by three physicians in terms of ramris ( rheumatoid arthritis magnetic resonance imaging score ) , samis ( simplied rheumatoid arthritis magnetic resonance imaging score ) correlated techniques were and ceus grade . 
the most painful joint was consistently found to be the joint with most synovitis . conclusions ce - mr imaging may be used prior treatment and for long - term follow - up . 
ceus might be useful in the short - term follow - up , as it seems to provide an indication of the presence or absence of disease , though not of its severity . 
the software is a very useful tool that can supplement , but not replace , the other techniques . keywords rheumatoid arthritis ( cid : 2 ) mr ( cid : 2 ) ceus ( cid : 2 ) us r . 
raffeiner rheumatology unit , department of medicine , general hospital of bolzano , bolzano , italy introduction rheumatoid arthritis ( ra ) is a chronic inammatory disease characterised by synovial inammation leading to progressive joint involvement with erosions , disabling pain and functional impairment . 
ra almost invariably affects the proximal interphalangeal joints ( pip ) , the metacarpophalangeal joints ( mcp ) and the radiocarpal joints : synovitis in these joints is a marker of generalised joint disease [ 1 ]  . the formation of new vessels is an essential pathogenic feature of progressive synovitis since synovial vascularity correlates with disease activity and aggressiveness [ 24 ]  . 
currently , no quantication system exists that enables the correct assessment of response to therapy and disease progression [ 5 ]  . several studies have demonstrated the usefulness of colour doppler and power doppler ultrasound ( cdus and pdus ) in the evaluation of synovial vascularity , but these radiol med ( 2014 ) 119 : 422431 applications are somewhat limited in detecting the slow ow of very small vessels such as those typically seen in synovial proliferation [ 610 ]  . 
contrast - enhanced ultrasound ( ceus ) has drastically improved the sensitivity of cdus and pdus , enabling the better depiction and quantication of inammation and consequently a more accurate distinction between brous synovial proliferation and active synovitis [ 1113 ] ; however , the technique has yet to become standard in the diagnostic workup of patients with ra . resonance contrast - enhanced magnetic ( ce - mr ) imaging is currently considered the gold standard morphological investigation . 
it is able to depict the synovial pannus , uid distension of the joint , bone erosions and bone oedema , but it is hampered by well - known problems such as high cost , limited availability and considerable discomfort for the patient who has to be imaged in a prone position with arms raised above the head [ 14 , 15 ]  . the aims of this study were to evaluate the reliability of ce - mr imaging and ceus in detecting and quantifying the presence of synovitis ; to compare ceus grade ( scored by three different radiologists ) and clinical severity ( as measured by the das28 score ) in order to determine the level of radiological - rheumatological agreement ; to assess inter - observer agreement for both modalities ( ce - mr and ceus ) ; to compare two mr imaging assessment systems , namely ramris ( rheumatoid arthritis magnetic resonance imaging score ) and samis ( simplied rheumatoid arthritis magnetic resonance imaging score ) [ 1618 ] ; to test the reliability of a specially developed software programme capable of measuring synovial volume . materials and methods we analysed a total of 16 patients affected by ra and receiving treatment with biological agents [ mean age 50 11 years ( 3268 ) ] , 14 of whom were women ( mean age 51 12 years ) and two were men ( mean age 42 6 years )  . average disease duration was 17 12 years ( 137 years )  . the patients met the ra criteria drawn up by the american college of rheumatology ( acr ) in 1987 . 
the same joints were then imaged with pdus to assess synovial vascularity . contrast - enhanced mr imaging the patients underwent ce - mr imaging with a 1.5 - tesla system ( magnetom avanto , siemens , erlangen , germany ) using a body coil ( body matrix coil , siemens , erlangen , germany )  . 
the samis classication is based on the assessment , still in the hand - wrist district , of erosions ( scored 010 ) , bone oedema ( only expressed as the presence or absence , and therefore scored 0 or 1 ) and synovitis ( scored 02 )  . 
the ramris system requires the study of 46 areas ( 23 for each limb ) for the assessment of bone erosions and oedema , and of 14 areas ( 7 per limb ) for the assessment of synovitis . 
conversely , the samis system entails the study of one hand only ( the more painful ) and , in particular , of 15 areas to assess bone erosions and oedema , and 6 areas to assess synovitis [ 16 18 ]  . each patients scores for oedema , erosion and synovitis determined in the various joints considered were calculated based on the data obtained from the two classication systems . the volume of tissue affectedshowing contrast enhancementwas calculated . 
1 magnetic resonance ( mr ) sequences used in the study . coronal isovolumetric t1 3d ( a ) , coronal stir ( b ) , coronal pre ( c ) and postcontrast ( d ) vibe ( gre 3d fs ) , subtraction image between post and precontrast coronal vibe , subsequently reconstructed with maximum intensity projection ( mip ) ( e ) radiol med ( 2014 ) 119 : 422431 and quartiles were calculated for the clinical data , as these were not normally distributed . in order to compare the ceus and the clinical data ( crp , esr , vas , ptga , prga , das28 ( crp ) , das28 ( esr ) , cdai , sdai and haq ) , we applied the wilcoxon rank test after calculating the median values and quartiles of the ceus examination . 
the spearman nonparametric test was used to assess the linear correlation between the two scales ( ramris and samis ) applied to ce - mr reading . statistical signicance was set at 5 % ( p \ 0.05 ) ; correlate the volume of synovitis calculated by the software with the clinical parameters and the sum of the scores assigned to synovitis with the ramris and samis systems ; correlate separately the 28 joints assessed with pdus and the sum of the samis and ramris scores for synovitis , erosions and oedema with the clinical data ( crp , esr , vas , haq , das28 - crp , das28 - esr , cdai , sdai , ptga , prga )  . correlate the sum of erosions with the erosions seen on ultrasound by the rheumatologist at the level of the 28 joints examined . the wilcoxon rank test was used to correlate the synovitis detected with ceus and ce - mr imaging . inter - reader agreement was compared for the ceus examination and for the samis and ramris protocols . we calculated the kendall coefcient of concordance for the ordinal variables ( sum of the samis and ramris scores ) and the kappa coefcient for the nominal variables . given that the ceus scores in this study could take on only one of two values , the kappa coefcient was used to assess the inter - operator agreement of ceus , for which the agreement on each single item is also provided . 
2 enhanced tissue volume after contrast medium administration , based on automatic analysis of mr data in detail , we examined nine radiocarpal joints ( ve rightsided , four left - sided ) , ve metacarpophalangeal ( mcf ) joints ( one fourth mcf and two fth mcf on the left , one second mcf and one fourth mcf on the right ) and two interphalangeal proximal joints ( ifp ) ( third ifp on the left )  . the mechanical index ( mi ) and acoustic pressure ( pa ) were set at 0.1 and 30 kpa , respectively . 
the patients hand was immersed in a basin lled with water , used instead of us gel , at constant temperature ( 28 1 ( cid : 3 ) c ) ; the transducer was placed approximately 1 cm away from the joint and held in place by the bracket of a radiographic stand so as to minimise movement , a method described in previous studies [ 20 , 21 ]  . 
3 graphic representation of contrast - enhanced ultrasound ( ceus ) grade 1 and grade 2 median values compared with c - reactive protein ( crp ) ( a ) and erythrocyte sedimentation rate ( esr ) ( b ) , respectively 75 % ( 12 / 16 patients )  . 
no patient with laboratory ndings of active disease ( das28 [ 2.6 and cdai [ 2.8 ) had a ceus grade 0 . ra is a very widespread and potentially disabling disease , for which different therapeutic approaches are currently available ( from anti - inammatory drugs to biological agents ) [ 2225 ]  . the choice of drug requires adequate disease staging and consequently a sensitive imaging technique . discussion diagnostic imaging has long had a dominant role in rheumatology , but the correct timing and combination of modalities have not yet been standardised [ 26 , 27 ]  . 
previous studies have compared different imaging techniques ( x - ray , us , pdus , ceus , ce - mr ) in an attempt to identify the most appropriate procedure for the diagnosis and follow - up [ 2 , 28 ]  . ce - mr imaging is a reliable , reproducible and non operator - dependent modality . 
ce - mr imaging was superior to us and ceus in the overall assessment of synovitis and erosions , proving to be the most appropriate instrument for evaluating the actual damage produced by radiol med ( 2014 ) 119 : 422431 fig . 
subtraction images therefore make it relatively easy to assess active disease as well as to monitor disease progression at subsequent follow - up examinations . right wrist left 4 mcp right 4 mcp right 3 pip right wrist left 2 mcp left wrist left 5 mcp right wrist right carpus left 5 mcp left 3 pip left wrist right wrist left wrist left wrist 430 radiol med ( 2014 ) 119 : 422431 fig . 
for this reason , calculation of the volume of reactive synovial thickening cannot replace the radiologists assessment but should be used as a diagnostic complement , especially useful for quantitatively assessing the degree of involvement of the single patients joints over time . the nding that the most severely affected joint in each patient corresponded to the one reported as being clinically the most painful suggests that the reliability of this criterion for the choice of which joint should be examined with ceus . according to our results , ceus and ce - mr ( samis and ramris ) did not correlate statistically with each other , just as no correlation was found between the ceus values and the clinical parameters . 
on the other hand , analysis of the hematochemical and clinical data shows that the sample considered was homogeneous with regard to disease activity ( table 2 )  . microscopic examination of synovial biopsies demonstrates that the development of synovial microvasculature is the earliest sign of ra , and previous studies have shown that neoangiogenesis correlates with disease activity [ 3 , 4 ]  . by exploiting the purely intravascular nature of the sonographic contrast medium , the ceus examination is highly sensitive in detecting slow blood ows such as those seen in the synovial microvasculature [ 31 ]  . to conclude , ceus , with its sensitivity of 100 % in detecting active disease , is a highly useful modality for the short - term ( 36 months ) monitoring of treatment response ; the examination should not be considered for radiol med ( 2014 ) 119 : 422431 assessment of disease severity but for evaluating the presence or absence of residual disease activity . 
conversely , ce - mr imaging is a panoramic modality which , by providing comprehensive images of the hand and wrist , allows for a complete assessment of the disease , with detection of not only synovial enhancement but also bone oedema , erosions and other , at times delayed , complications such as subluxations , geodes and tenosynovitis . 
ce - mr imaging is therefore fundamental for the mid long - term ( 12 years ) monitoring of disease , to establish disease severity and extent of damage . the limitation of this study lies in its size . 
surgery is the rst - line approach , and the correct timing of radiation therapy has not yet been dened since early radiation therapy improves relapse - free survival but not overall survival . 
clinical and therapeutic factors were entered into the analysis overall ( os ) and progression - free ( pfs ) survival , and the distribution in two accrual periods identied based on the evolution of imaging procedures and radiotherapy techniques were compared . 
for 6 / 18 long survivors ( ls ) without evidence of disease , neurocognitive evaluation was obtained and the dose to the hippocampus region was retrospectively calculated . results univariate analysis of os showed a statistically signicant advantage for grade 1 and oligodendroglioma histology , better performance status [ karnofsky index ( ki ) ] , age \40 years , radical surgery , no steroid treatment ; a . 
facchetti pathology department , spedali civili hospital , p.le spedali civili 1 , 25123 brescia , italy e - mail : facchettif@gmail.com radiol med ( 2014 ) 119 : 432439 pfs was signicantly related with younger age , better ki and early radiotherapy . 
memory impairment was evident in 4 / 6 of the ls tested ; quality of life was good and executive functions were normal . conclusion radiotherapy remains an essential component in the treatment of low - grade glioma . 
prospective studies are needed to evaluate the relative contributions of the disease itself and of surgery , radiation and chemotherapy to long - term neurocognitive damage . keywords low - grade glioma ( cid : 2 ) radiotherapy ( cid : 2 ) survival ( cid : 2 ) neurocognitive evaluation introduction low - grade gliomas ( lgg ) include tumours arising from neuroepithelial tissue classied as grade i and ii by the who ( 2007 )  . 
they represent 1015 % of gliomas in adults and are almost all grade ii [ 13 ]  . the treatment of lgg and especially the timing of the different modalities are controversial since clinical trials with long - term follow - up are lacking , in contrast with the long survival times of these patients . 
favourable prognostic factors are : age \40 years , tumour size \6 cm , no neurological decits at diagnosis , karnofsky index ( ki ) [ 70 , single hemisphere disease , no enhancement at magnetic resonance ( mr ) imaging and oligodendroglial histology ( 1p / 19q co - deletion )  . 
the european organisation for research and treatment of cancer ( eortc ) 22845 trial demonstrated better progression - free survival ( pfs ) in patients treated with rt early after surgery compared with those treated after disease progression [ 13 ]  . 
no randomised trial has demonstrated a survival advantage for the use of chemotherapy [ 16 ]  . the late neurocognitive toxicity of rt represents another controversial issue , especially in young , potentially table 1 baumanns prognostic classes prognostic class age b40 and ki c70 age b40 and ki \70 age [ 40 , ki c70 and no contrast enhancement age [ 40 , ki c70 and contrast enhancement age [ 40 and ki \70 ki karnofsky index long - surviving patients , as the literature data provides conicting results . 
the aim of this study was to evaluate the evolution of the treatment for in a lgg single institution over the past 25 years , relating the use of rt to survival and toxicity . materials and methods from january 1985 to december 2009 , a total of 95 adult patients with lgg were consecutively treated with rt at the radiation oncology department of the spedali civili , brescia university . all patients were retrospectively classied according to baumanns ve prognostic classes [ 17 ] ( table 1 ) and were divided into two groups : early radiotherapy ( ert ) if radiotherapy was given less than 3 months after the surgery and late radiotherapy ( lrt ) if radiotherapy was given thereafter or at recurrence . 
the cut - off year ( 1996 ) was chosen on the basis of changes in rt and diagnostic work - up ( use of three - dimensional conformal rt and magnetic resonance imaging )  . 
distribution of the diagnostic , clinical and therapeutic features in the two periods was compared with the v2 test . overall survival was the interval between the date of diagnosis and the last follow - up visit or death , while pfs was the interval between the date of diagnosis and the rst evidence of disease progression . 
the remaining six patients were submitted in 2012 table 2 distribution of patients diagnostic , clinical and therapeutic characteristics table 2 continued gender male female 90100 prognostic class steroid therapy antiepileptic therapy histology astrocytoma oligodendroglioma ependymoma other unknown treatment period 19851995 19962009 type of surgery biopsy partial resection total resection no surgery radiotherapy timing post - surgical at recurrence radiotherapy dose b50 gy 5060 gy [ 60 gy radiol med ( 2014 ) 119 : 432439 chemotherapy ki karnofsky index , mri magnetic resonance imaging , who world health organization ( 36 years after rt ) to the following neurocognitive tests : visual analogue scale ( vas ) for pain , sf - 12 health survey questionnaire [ 18 ] , mini mental state examination ( mmse ) [ 19 ] , neuropsychiatric inventory ( npi ) [ 20 ] , rey auditory verbal learning test ( immediately and after 15 min ) [ 21 , 22 ] , trail making test ( tmt ) [ 2325 ] and clock drawing test [ 26 , 27 ]  . 
the sf - 12 is a quality - of - life test ( physical and mental health ) , based on the scores of 12 questions ( 0100 ) , where zero score indicates the lowest level and 100 the highest level of health . 
the mmse , a brief questionnaire used to evaluate cognitive impairment , includes simple questions and problems such as the time and place of the test , repeating lists of words , arithmetic , language , and basic motor skills . 
the clock drawing test represents a screening test for executive dysfunction . for ve of these six patients bilateral hippocampus regions were retrospectively outlined and the dose to these structures calculated . results patients were evenly distributed with regard to sex and age ( median age 41 years )  . 
the type of tumour was astrocytoma in 41 % of patients and other types in 55 % ; histology was unknown in 4 % of cases in whom biopsy radiol med ( 2014 ) 119 : 432439 was judged not possible owing to the site of disease ( table 2 )  . 
no signicant differences were noted in the distribution of these characteristics according to the accrual period . about two - thirds of the patients ( 68 % ) were treated before 1996 . 
most patients were treated on limited volumes : site of disease with margin ( n = 71 ) or site of disease with coning down technique ( n = 16 )  . 
the distribution of patient and disease features ( grading , age and performance status ) in the two groups was not statistically different . overall and pfs after a median follow - up of 12 years ( 2310 months ) , 45 patients ( 49 % ) were alive and 31 % of them ( 14 / 45 ) had no evidence of disease . actuarial os of the entire series was 89 , 60 and 51 % at 1 , 5 and 10 years , respectively . 
in particular , no differences in pfs or os according to recruitment period were observed . multivariate analysis of os conrmed that young age ( p = 0.009 ) , good performance status ( p = 0.001 ) , oligodendroglioma histology ( p = 0.023 ) and the absence of steroids ( p = 0.005 ) were independent factors in predicting better survival . 
good performance status ( p = 0.05 ) and ert ( p = 0.006 ) were independent factors in predicting better pfs ( table 3 )  . neurocognitive assessment and doses to the hippocampus regions the results are shown in table 4 . 
the rey auditory verbal learning test showed pathological values in immediate execution in two patients , pathological memory decit at recall in one patient and values below the standard in other two patients . 
the sf - 12 was administered to all the patients , who reported having a discrete quality of life after rt , with only minor changes in daily living . despite the lack of a randomised controlled trial , the evidence for the benets of extensive surgical resection is discussion growing . 
a prospective randomised clinical trial should be conducted to evaluate the statistical advantages of total gross resection , but even without this evidence it is considered good practice to perform a resection that is as radical as possible without causing functional decits . 
curative surgery , partial or radical , was also the rst treatment in the majority of the patients in our series ( 51 and 27 % , respectively )  . 
the indication for immediate rt can be limited to young patients belonging to baumann prognostic class 1 with mr imaging contrastenhanced disease and subjected to partial resection . to reduce the risk of toxicity , many studies have evaluated a reduction of total and fractional dose and of treatment volumes . 
 [ 29 ] evaluated the adverse long - term effects of radiotherapy and underlined the higher incidence of leukoencephalopathy and cognitive decits in patients treated with whole - brain rt in comparison with patients treated with focal rt . 
also taphoom [ 30 ] and laack [ 31 ] reported that small - volume rt could be linked with a less negative impact on cognition ; accordingly , in our series we commonly prescribed 5054 gy on treatment volumes mostly limited to the disease site . 
the few patients studied with neurocognitive tests are a good example of the radiol med ( 2014 ) 119 : 432439 different factors impacting the risk of toxicity apart from rt ( site of disease , extent of surgery , steroids and antiepileptic drug use )  . the usefulness of chemotherapy for patients progressing after the surgery and rt is relatively well established , with more data available for patients with oligodendroglial 1p / 19q co - deleted tumours [ 16 ]  . 
the results of a phase iii study , comparing radiotherapy with radiotherapy followed by pcv , showed that the addition of chemotherapy provides a benet in pfs but not in os [ 35 ]  . chemotherapy has been tested as post - surgical treatment in high - risk patients but complete responses are generally lacking [ 36 , 37 ]  . 
it is not possible to attribute a prognostic role in terms of survival to this variable . mr imaging is useful for diagnosis , to guide surgery , to plan rt and to monitor response to therapy . 
dynamic susceptibility contrast mri ( dsc - mri ) and measurement of relative cerebral blood volume ( rcbv ) correlates with vascularity and can predict high - grade transformation [ 43 ]  . 
our series reects the increased use of mr imaging in recent years . the late effects of rt might consist of rare episodes of radiation necrosis , multifocal leukoencephalopathy and damage caused by the inclusion in treatment elds of organs such the optic chiasthe leukoencephalopathy may appear months or years after rt and may lead to progressive deterioration in personality , gait and balance , urinary continence , attention , memory and executive function . 
in our series , only three patients had radiologically proven late toxicity , without any symptom : leukoencephalopathy in one patient and cerebral radionecrosis in two others [ 2931 ]  . itself , the cognitive decits may have several sources : the tumour treatments and tumour - related epilepsy , psychological distress . 
 [ 44 ] found neurocognitive decits in 91 % of the patients before the surgery : patients with tumour in the dominant hemisphere have more memory problems and poorer attention , verbal uency and verbal learning and have less chance to normalise following surgery . 
 [ 45 ] reported the analysis of cognitive and quality - oflife outcomes in 65 patients with a 12 - year median followup ; 53 % of patients who received rt had cognitive decits compared to 27 % of nonirradiated patients . 
neurocognitive function is increasingly being incorporated as an outcome measure in clinical trials in patients with lgg . with the limits of the small number of patients , our data conrm prevalent involvement of the memory network and of visual scanning , visual - motor coordination and visualspatial ability , while executive functions appeared to be normal . 
this seems relevant since the patients available for analysis are recently treated patients with a good prognosis . it is important to underline that more studies are needed to correlate cognitive decits with tumour size and site and with the overall treatment burden ( surgery , radiotherapy , chemotherapy )  . 
the italian society of radiation oncology recently published a pattern - of - practice paper on the use of radiotherapy for gliomas [ 48 ] but data on neurocognitive outcome are scarcely available . 
therefore , it may be of interest to organise a multicentric data collection , with information about neurocognitive outcome including also patients subjected to surgery alone . conclusions with the limitations of a retrospective analysis , most of the results obtained are consistent with the literature . 
the already known prognostic factors were conrmed : good performance status , younger age , oligodendroglioma histology and the absence of steroid therapy provide an advantage in terms of os . 
a careful , prospective evaluation of the possible advantages of the use of modern radiation technology for target identication and treatment delivery is therefore needed in order to dene efcacy in sparing the organ at risk ( oar )  . 
sofocleous received : 6 june 2014 / accepted : 11 june 2014 / published online : 1 july 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract surgical resection is the standard treatment for early - stage primary lung cancer and selected cases with pulmonary metastases . 
however , lung resection may not be possible in patients with compromised pulmonary function , concurrent medical conditions , or previous lung resections . image - guided ablation has emerged as a less invasive treatment option for unresectable lung tumors that allows for preservation of pulmonary function and promising efcacy . 
hereby we describe the indications for and outcomes of image - guided ablation performed for the management of pulmonary malignancies . keywords lung ( cid : 2 ) early - stage lung cancer ( cid : 2 ) non - small cell lung cancer ( cid : 2 ) pulmonary metastases ( cid : 2 ) colorectal pulmonary metastases ( cid : 2 ) image - guided ablation ( cid : 2 ) thermal ablation ( cid : 2 ) radiofrequency ablation ( cid : 2 ) microwave ablation ( cid : 2 ) outcomes introduction surgical resection is the standard treatment for stage i nonsmall cell lung cancer ( nsclc ) and confers the best outcomes ; however , only one in four patients is diagnosed in this stage [ 1 ]  . 
sofocleous interventional radiology and image guided therapy , department of radiology , memorial sloan kettering cancer center , room h118 , 1275 york ave , new york , ny 10065 , e - mail : petree@mskcc.org conventional external - beam radiotherapy [ 2 ]  . 
although selected patients may benet from metastasectomy or pneumonectomy for the treatment of metastatic lung disease [ 5 ] , the majority of these patients have diminished pulmonary reserve prohibiting surgery or radiotherapy . unresectable patients with primary or metastatic lung tumors can be successfully treated with non - surgical therapies such as ablation and stereotactic body radiotherapy ( sbrt )  . 
two small retrospective series demonstrated acceptable morbidity and efcacy proles of thermal ablation for the treatment of recurrence after pneumonectomy [ 8 , 9 ] , a clinical scenario that often has no therapeutic option . 
ablation is also suitable for patients who have persistent pulmonary nodules in the setting of 542 radiol med ( 2014 ) 119 : 541548 other lung metastases that are responding to chemo / radiotherapy . finally , ablation can be offered to selected patients with pulmonary metastases that are surgical candidates within the test - of - time concept , as it has been described for liver tumors [ 10 ]  . 
according to this concept patients who could undergo surgery are treated with ablation instead . patients successfully treated by ablation alone and patients who subsequently developed multifocal progression of disease are spared unnecessary surgery with signicant morbidity . several sources of energy have been used for ablation of tissues and tumors . 
more recently , reports on the safety prole and the early clinical experience of irreversible electroporation ( ire ) , a non - thermal modality , have surfaced . pre - procedural planning the decision to treat lung tumors with ablation is generally made by a multidisciplinary team including a thoracic surgeon , an oncologist , a radiation oncologist , a pulmonologist , an anesthesiologist , and an interventional radiologist experienced in oncologic interventions ( interventional oncologist ) , and in particular lung ablation . 
in addition to the medical pre - procedural evaluation , a recent cross - sectional ct and / or pet / ct , preferably within 1 month before the procedure , is necessary in order to assess tumor size , nodal involvement , and proximity to neighboring structures [ 11 ]  . 
patients who are healthy enough to undergo a ctguided needle biopsy of the lung and can tolerate general anesthesia ( ga ) or heavy sedation are generally good candidates for ablation [ 12 ]  . 
ct is also the most frequently used imaging modality for guidance [ 13 ]  . post - ablation imaging ablation produces a rim of ground - glass attenuation ( gga ) around the tumor , seen immediately after the procedure . 
ground - glass attenuation has been regarded as an early indicator of treatment success when it forms a tumor , representing the ablation zone , rim of at least 5 mm all around the ablated lesion , representing the margin of ablation [ 14 ]  . 
subsequent imaging studies every 3 months up to at least 1 year are recommended to detect local or other tumor recurrence [ 15 ]  . pet / ct imaging is a valuable tool follow - up , depending on the [ 18f ] uorodeoxyglucose ( fdg ) characteristics of the index tumor on pre - procedural imaging . a rim of fdg avidity is usually seen surrounding the ablation zone for weeks and even months after ablation . this rim represents hyperemic reactive changes . 
the same pet and ct ndings accompanied by fever , pain , and leukocytosis may indeed indicate the development of abscess as a result of infection of the ablation zone . 
collapse of an ablation cavity may be accompanied by small increase of the suv values in pet without signifying local tumor progression ( ltp )  . subsequent follow - up is critical to show decrease in suv and lesion size . 
when suv increase persists in subsequent follow - ups or when it has a nodular or irregular conguration it may represent ltp . ablation modalities radiofrequency ablation ( rfa ) radiofrequency ablation delivers high - frequency alternating electric current to the target tissue through a needle electrode . 
due to the limited thermal conductivity of the aerated lung [ 16 ] , rfa may result in lower energy deposition into the target tumor , thus preventing adequate ablation with sufcient margin [ 17 ]  . 
another limitation that is inherent to the rfa technique is the heat - sink phenomenon that occurs as a result of adjacent blood ow in nearby vessel or airow in nearby airway that dissipates the thermal energy . 
this perfusion / air mediated cooling is responsible for an ablation zone smaller than it was intended and incomplete treatment or relatively small margins [ 18 ]  . radiol med ( 2014 ) 119 : 541548 fig . 
the light is delivered through 400 - mm long bers terminated by a specially developed diffuser which emits laser light to an effective distance of up to 1215 mm [ 19 ]  . 
the use of thermal mappings allows realtime monitoring under mri . cryoablation the cellular damage caused by cryoablation is the result of complex combination of cellular events during cycles of tissue freezing and thawing . 
crystallization that occurs in the extracellular tissue and intracellular compartment disrupts organellar membranes and causes dehydration and further compromise in cellular function . during the thawing cycle the crystals coalesce into larger sizes , membranes are disrupted , and vessels occlude resulting in cell death [ 20 ]  . cryoablation has several advantages , namely visualization of the ablation zone known as the ice ball . 
this can be visualized on computed tomography ( ct ) and mri and correlates well with the pathologic zone of ablation [ 21 ]  . sequential freezing and thawing cycles result in larger ice ball and extensive ablation zones [ 22 ]  . 
cryoablation preserves the collagenous architecture of the ablated tissue microwave ablation ( mwa ) microwave ablation ( mwa ) utilizes high - frequency waves that cause water molecules to oscillate creating friction , causing heat and tissue destruction by coagulation necrosis similarly to rfa . 
microwave ablation has several theoretical advantages when compared to the technical limitation of rfa : achieves higher temperatures thus limiting the cooling by large vessels or the airway nearby and providing 544 radiol med ( 2014 ) 119 : 541548 that may be particularly benecial when treating lesions adjacent to the tracheobronchial tree and mediastinum [ 23 ]  . ablation in early - stage nsclc the main indications of ablation in early - stage nsclc are high risk , unresectable patients , and those with recurrent tumors after radiation therapy , surgery or chemotherapy [ 2426 ]  . 
tumors \3 cm in largest diameter , located away from the large airways and vessels , surrounded completely by aerated lung are the best candidates for ablation [ 27 ]  . 
another factor associated with local tumor control is the ablation margideally , immediately after ablation , a 10 - mm margin of the gga relative to the ablated tumor should be demonstrated . 
as described before , tumor proximity to large vessels or airways has also been reported as a negative predictive factor for completeness of ablation in lung [ 29 ]  . two recent studies compared ablation to surgery in early - stage nsclc . 
the most recent ( 2011 ) study compared the survival between surgery and rfa in a retrospective review of 22 matched patients and found no difference between the two groups [ 31 ]  . 
the study concluded that there was no signicant difference in outcomes between the three therapeutic modalities . rates after similarly , overall survival image - guided ablation of nsclc are equivalent to those reported after sbrt [ 33 ] , between 40 and 60 % at 3 years for patients with early - stage medically inoperable lung cancer [ 7 , 34 40 ]  . 
along with this consideration , the cost being a fraction of that of sbrt , the ease of use and repeatability and , the safe prole of pulmonary ablation , makes this technique a competitive option for the treatment of inoperable earlystage nsclc . 
ideally , of course , randomized controlled trials should be performed although this is not an easy task . outcomes of thermal ablation in early - stage nsclc are seen in table 1 . ablation in metastatic lung disease ablation is considered in the treatment of selected patients with pulmonary metastases . 
in general ablation is indicated when the number of lesions per hemithorax are \5 , ( preferably \3 ) and the largest lesion diameter is smaller than 3.5 cm surrounded by well - aerated lung [ 24 , 4143 ]  . ablation of metastatic disease should also be contemplated when there is no or limited and controlled extrapulmonary disease . 
more precisely , keywords mrgfus ( cid : 2 ) high - intensity focused ultrasound ( hifu ) ( cid : 2 ) musculoskeletal interventions ( cid : 2 ) benign bone lesions ( cid : 2 ) management of oncologic bone lesions ( cid : 2 ) noninvasive treatment introduction magnetic resonance ( mr ) - guided focused ultrasound surgery ( mrgfus ) is a totally noninvasive ablation technique based on the ability of ultrasound waves to penetrate the tissues and to release energy . 
its limits are , however , due to its indications . currently under investigation is its use for the treatment of breast , pancreas and liver cancer , along with the essential tremor in parkinsons disease . 
a real challenge , considering the social impact , is represented by its use for the treatment of chronic pain in diseases affecting the joints and spine [ 2 ]  . the use of focused ultrasound waves for the treatment of bone lesions has aroused great interest in the scientic community . 
technological advances , however , are needed to reduce treatment times and costs . the management of bone lesions still remains a crucial issue both for the physician and the patient . 
metastases account for the most frequent types of tumoural bone lesions , being a source of pain and functional impairment , due to fractures , medullary compression and hypercalcaemia , all conditions leading to a signicant worsening of life quality . 
the patients take high doses of analgesic drugs such as morphine , and radiol med ( 2014 ) 119 : 470475 therefore , the achievement of pain relief is both a challenge the management of skeletal and the primary aim of metastases [ 5 ]  . 
moreover , since rt is poorly tolerated by the normal tissues , the treatment cannot be repeated in a previously treated area , in the case of recurrence . these problems with rt have urged the researchers to nd alternative procedures . 
several studies have been published on radiofrequency ( rf ) ablation describing palliative treatments of bone metastases , with good results in terms of pain relief [ 79 ]  . 
in these studies , rf ablation is suggested as an alternative to rt to treat painful bone metastases [ 79 ]  . another crucial issue is represented by the management of benign lesions . 
surgical procedure invasiveness and lesion aggressiveness raise the crucial issue of therapeutic management of bone lesions of benign nature , which are nonetheless a source of severe discomfort , functional disability and often invalidating pasince the presence of a benign bone lesion does not necessarily mean lack of aggressiveness , histologically benign lesions may be locally highly aggressive , causing severe discomfort to the patient . 
as a consequence , the therapeutic approach must be as radical as possible to prevent lesion recurrences . depending on the lesion nature and site , surgical treatment includes curettage , excision of a piece of bone and , in the most severe cases , prosthetic implantation . during the last decades , less invasive therapeutic approaches have been developed and performed under radiological guidance . 
the method of choice in the treatment of osteoid osteoma is today represented by thermoablation as an alternative to surgical repair . in more recent times , a new completely noninvasive ablation technique has been developed , mrgfus . 
some authors suggest its use also for the treatment of bone lesions , particularly metastases [ 10 ]  . rationale the focused ultrasound waves are based on two principles , namely denervation of the periosteum , which is quite rich in nervous bres , and ablation of the bone lesion . 
they destroy the tissue by means of heat , by increasing its temperature over 56 ( cid : 3 ) c for at least one second and reaching a coagulative thermal necrosis due to protein denaturation . ultrasound waves are acoustic mechanical waves with higher frequencies than those on average heard by humans ( [ 20 khz )  . 
propagating through matter , they apply pressure to the particles composing it and make them oscillate . the oscillation of the single particles , if observed as a whole , appears as a wave front transmitting ultrasound energy to the matter , through compression and rarefaction . when a transition point is reached , by which the interface between two acoustically and physically different matters is meant , the ultrasound waves are partially reected and partially transmitted . 
either quantity depends on the different tissue impedance : the higher the impedance , the lower the transmission . ultrasonography is based on reection and , particularly , on the possibility that the reected waves be recorded . ultrasound thermoablation is based on the transmission of energy to the tissue . 
this , however , will decrease the beam precision , since the deeper the beam penetrates , the less precisely the area to be treated will be dened and targeted . 
from this description , it becomes clear that great accuracy must be adopted in the choice of the tissue to be targeted by the ultrasound beam and that everything interposing between the skin and the targeted area ( i.e. , bone , air , metallic devices , scars ) must be avoided so as to avoid impairing of the us penetration as well . 
microbubbles between the skin and the transducer must be totally eliminated . 472 radiol med ( 2014 ) 119 : 470475 in principle , these characteristics suggest that mrgfus can be efciently applied to the treatment of bone lesions . timing is of utmost importance in pain management . 
the use of mrgfus provides much shorter times than the other techniques such as rt of bone metastases . mr guidance the high contrast resolution of mr imaging allows for an accurate treatment planning as well as the correct detection of the lesions and the neighbouring sensitive structures to be avoided for the safeguard of their integrity . 
an additional advantage of mr imaging lies in the possibility to use the same technique ( with specic sequences and administration of contrast media ) for imaging and treatment of the lesions . 
moreover , it is possible to monitor in real - time the temperature reached in the target area , thanks to specic sequences ( prf , proton resonance frequency ) that allow detection of mr phase changes , depending on temperature . 
with these sequences , it is possible to subtract the images acquired during the procedure ( as the tissue temperature increases progressively ) from those acquired at time 0 , i.e. 
in this way , it is possible to monitor both the temperature reached in the region of interest and the status of the neighbouring structures . available equipment at present two mr - guided systems are available : the exablate mrgfus system ( insightec ltd , haifa , israel ) , which received us food and drug administration ( fda ) approval for the treatment of uterine broids and bone metastases and ce marks for the treatment of uterine broids and bone metastases . the sonalleve mr - hifu system ( koninklijke philips electronics nv , eindhoven , the netherlands ) , which received ce mark for treatment of uterine broids and bone metastases . 
fda studies for palliative treatment of bone metastases and breast cancer are in phase ii / iii clinical trials . the use of focused ultrasound waves in the treatment of pain related to bone metastases was rst described in 2006 bone metastases by catane et al . 
in 10 out of 13 patients , there was a good pain relief without adverse reactions and with a drastic reduction in medicament ( table 1 )  . these results were conrmed by gianfelice et al . 
in addition , an important and original characteristic of the study was that the authors described the possibility to evaluate bone density demonstrating that the latter showed an increase at the level of the treated lesion after the procedure . 
however , there is still a long way to go to demonstrate that the use of this technique may provide structural effects in addition to the palliation , and further studies on larger series are needed ( table 1 )  . in 2008 , lieberman et al . 
thirty - one patients with 36 bone lesions were submitted to mrgfus , representing both the number of patients and the follow - up duration the driving force of the study . 
twenty - ve out of 31 patients were evaluated at 3 - month follow - up . average visual analogue scale ( vas ) score decreased from 5.9 prior to treatment to 1.8 at 3 - month follow - up . 
in 2013 [ 14 , 15 ] ( table 1 ) reported feasibility and efcacy of mrgfus treatment for pain palliation in patients with both benign ( osteoid osteoma ) and malignant ( bone metastases ) lesions . 
this study was carried out in patients not previously treated with external beam radiation therapy ( ebrt ) in target metastases and demonstrated that mrgfus can be effectively applied as a primary noninvasive technique for pain palliation related to bone metastases . 
of lesions treated decrease in pain scores follow - up bone metastases bone metastases bone metastases bone metastases bone metastases osteoid osteoma 92 % 69 % 100 % 59 days 3 months 3 months up to 3 months 6 months standard pain palliation treatments , including ebrt . 
although this study was performed with a system that was conceptually built for bone pain palliation , they demonstrated a potential role of this noninvasive technique for local tumour control yielded by a reduction in lesion viability following mrgfus procedure and by re - mineralization of spongious bone according to the mda criteria . 
according to the mda criteria , a complete response to treatment was observed in 2 / 18 ( 11.1 % ) patients , a partial response in 4 / 18 ( 22.2 % ) patients , stable disease in 10 / 18 ( 55.6 % ) patients and progressive disease in 2 / 18 ( 11.1 % ) patients [ 14 ]  . other bone lesions the therapeutic management of benign bone lesions such as osteoid osteoma , periosteal chondroma , broangiomas and bromyxomas represents a crucial issue . 
on the one hand , the surgical treatment is quite complex and should be as invasive as possible to avoid recurrence , which is reported to be high in conservative procedures . 
the crucial issue is therefore to reach the right balance between procedural aggressiveness . invasiveness and lesion in recent years , new techniques have been developed with the aim of reducing therapeutic invasiveness . 
interventional radiology nowadays offers a variety of new possibilities such as percutaneous ablation using rf , microwaves , cryoablation . osteoid osteomas are currently treated with satisfactory results by means of interventional radiology procedures , such as percutaneous thermoablation [ 16 ]  . 
almost complete absence of complications is observed using this technique along with a low percentage of minor adverse reactions ( 15 % ) , including reactive synovitis and inammation of soft tissue and nervous roots . the percutaneous treatment of the other benign lesions is scarcely described in literature . 
the lesions described in our study ( periosteal chondroma , broangiomas and myxobromas ) are submitted to surgery only when they cannot be treated with medication and / or present high local aggressiveness . the target in 2013 , napoli et al . 
 [ 15 ] treated six consecutive patients with limited joint function and reduced quality of life due to painful osteoid lesion conrmed at mr and ct . mrgfus was proposed as an alternative treatment among other consolidated modalities , including rf ablation . 
patients with lesions located in the vertebral body were excluded , while patients with lesions in close proximity to joints , tendons , tendon sheaths or neurovascular bundles were individually evaluated for accessibility . 
one of the main problems in the management of these lesions is represented by the presence of a proper acoustic window allowing the us beams to reach the lesion and treat it properly [ 18 ]  . in three cases , mrgfus was employed in combination with surgery . 
this combination , with surgery used both as neo - adjuvant and adjuvant technique , allowed the reduction in surgical aggressiveness . no major complications were observed in keeping with the literature . 
this condition was healed within a few days with administration of anti - inammatory medications , conrming the safety of mrgfus . conclusions mrgfus is a newly developed noninvasive therapeutic technique , mainly employed for the treatment of uterine broids . 
satisfying results have been achieved in the relief of pain caused by metastases [ 14 ]  . the noninvasiveness of the procedure combined with the possibility to check the temperature achieved in the targeted and surrounding areas over time allows drastic reduction in adverse reactions including damage to sensitive organs . there is limited literature about the use of mrgfus in the treatment of benign lesions . 
in one study alone , the authors describe its use in the treatment of osteoid osteomas , with results comparable to ours , particularly in terms of pain relief [ 15 ]  . the treatment of this type of lesions requires specic knowledge and competences both in the clinical as well in the diagnostic elds . 
extremely important , during treatment planning , is the study of the lesion characteristics : growth patterns , matrix , size and location , possible cortical involvement , relationships to the adjacent structures . 
the most sensitive structures in terms of ultrasound - induced damage are the scarcely vascularised tissues , such as ligaments and tendons , followed by nervous roots , which in our experience have never been damaged , though crossed by the beams . 
the lesion must be easily approached by the ultrasound waves , without interposition of scars or bone structures , but it also has to be far from more sensitive structures , such as tendons and ligaments , which absorb well due to the lack of vascularisation . 
as ow helps to lose heat rapidly , vessels are the less sensitive structures . a careful evaluation of the district to be treated has to be carried out , both in terms of anatomy and pathophysiology . in the presence of osteoid osteomas , the targeted area is represented by the periosteal bres and the nidus , source of pain due to inammation . 
as the cortical bone by denition absorbs the ultrasound waves , to achieve the proper temperature increase ( more than 56 ( cid : 3 ) per 1 s ) in the nidus , some technical requirements are to be met . 
in this way , in our experience , a major penetration was obtained as well as a hyperthermal area of 12 mm within the cortical bone . in the rst two cases , high energies were employed . subsequently , we realized that with energies inferior to 1 , 000 j an efcient hyperthermia could be achieved both on the cortex and on the nidus . 
in very young patients , it is extremely important that energies delivered be as low as possible to preserve cartilage growth . radiol med ( 2014 ) 119 : 470475 mrgfus is applied without problems on supercial lesions that do not offer any obstacles to the ultrasound waves . 
these procedures were performed without major complications . on the basis of the safety and efciency in terms of pain relief , it is believed that mrgfus represents a promising technique in the treatment of metastatic and benign bone lesions , though with the limitations due to the peculiarity of the method itself , which requires further studies on larger series . 
naguib abbas darvishi babak bazrafshan emmanuel mbalisike thorsten burkhard stephan zangos received : 19 february 2014 / accepted : 26 march 2014 / published online : 4 june 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract surgery is currently considered the treatment of choice for patients with colorectal cancer liver metastases ( crlm ) when resectable . 
we searched the medical literature to identify studies and reviews relevant to radiofrequency ( rf ) ablation , microwave ( mw ) ablation and laser - induced thermotherapy ( litt ) in terms of local progression , survival indexes and major complications in patients with crlm . 
however , further competitive evaluation should clarify the efcacy and priority of these therapies in patients with colorectal cancer liver metastases . keywords colorectal cancer ( cid : 2 ) liver metastases ( cid : 2 ) radiofrequency ablation ( cid : 2 ) laser - induced thermotherapy ( cid : 2 ) microwave ablation introduction the liver is the second most common site of metastatic spread of epithelial cancers , after lymph nodes . 
systemic chemotherapy with response rates between 36 and 66 % , and a median survival of 1426 months is a good treatment option for unresectable crlm [ 4 ]  . according to variety of tumor locations , liver function and different responses to systemic or loco - regional chemotherapy , ablative therapies have been used in the management of patients with crlm [ 46 ]  . 
the effects of these methods may prolong patients survival and improve quality of life [ 6 ]  . this article was formulated with the aim of reviewing the literature on thermal ablation therapies in the management of patients with crlm . 
searches were conducted via the 452 radiol med ( 2014 ) 119 : 451461 following databases , covering the period from their commencement to 01 / 10 / 2011 : medline , premedline , embase , cochrane library and other databases . 
in this review , the outcome of these techniques and the authors views on the current status of treatments are outlined . thermal ablation therapy thermal ablative techniques have been used to destroy tumor lesions by thermal energy without damaging adjacent vital structures . 
during radiofrequency ( rf ) and microwave ( mw ) ablation and laser - induced thermotherapy , tumor cells can be effectively destroyed by cytotoxic heat from different sources [ 6 , 8 ]  . with all the heating techniques , the aim is to raise the temperature of the tissue between 60 and 100 ( cid : 3 ) c . 
thermal ablation involves placement of a needle ( electrode / antenna / laser ber ) directly into the target tumor , typically under ultrasound ( us ) guidance [ 6 ]  . the ability to generate heat in biological tissue was rst reported in the late nineteenth century . 
rf electrodes such as water - cooled single or cluster electrodes as well as expandable electrodes have been improved , especially in the last three decades with the aim of achieving larger volumes of necrosis specically in tumor lesions [ 510 ]  . microwaves can produce coagulative necrosis with an ultra - high - speed ( 9002 , 450 mhz ) alternating electric eld , causing the rotation of water molecules . 
percutaneous mw ablation was rst used as an adjunct to liver biopsy in 1986 , but since then it has been used for hepatic tumor ablation [ 6 , 8 ]  . lasers have been used successfully in tumor ablation . hyperthermia and necrosis can be produced by photon absorption and heat conduction . 
laser delivery is possible with exible thin bers or a water - cooled laser applicator . a point source from a bare - tip ber will produce a sphere of necrosis , whereas a diffuser ber will produce an elliptical ablation [ 6 , 8 , 11 ]  . radiofrequency ablation electrodes are deployed from the end of the needle into the tissue . 
the size of the ablated area is determined largely by the size of the electrode needle , the temperature of the tissue and the duration of time the energy is applied . 
a sharp boundary separates dead tissue and unaffected surrounding tissue [ 9 , 10 , 14 ]  . three radiofrequency devices are used for tissue ablation . none of the devices is specically for the ablation of hepatic tumors . 
however , just recently the food and drug administration has approved the use of these devices for the treatment of liver tumors that are surgically unresectable [ 9 ]  . radiofrequency ablation has been performed either percutaneously or with laparoscopic surgery . 
the procedure has been used with a cooled - tip or a non - cooled - tip electrode , though the former system is normally preferred in cases of larger lesions as it gives a larger area of ablation due to reduced charring at the tip [ 11 ]  . indications radiofrequency ablation has usually been used for inoperable patients with colorectal cancer liver metastases . in a multidisciplinary concept , rf ablation for isolated colorectal cancer liver metastases may be indicated in patients with the following conditions : ( a ) resectable lesion as an adjunct to resection and ( b ) inoperable lesions which demonstrate complete or partial response after chemotherapy ( c ) recurrent and progressive lesions [ 5 , 915 ]  . contraindications relative contraindications for rf ablation include : tumor located \1 cm from the main biliary duct intrahepatic bile duct dilation anterior exophytic location of the tumor bilioenteric anastomosis absolute contraindications for rf ablation include : radiofrequency ablation has been explained technically in all related studies [ 715 ]  . 
coagulopathy with international normalized ratio radiol med ( 2014 ) 119 : 451461 progression , the development of new hepatic lesions , or the emergence of extra - hepatic disease . 
a recommended follow - up protocol includes ct or mr examinations at 3 , 6 , 9 , and 12 months after the treatment and at 6 - month interval thereafter for the subsequent 3 years [ 19 ]  . figure 2 shows local changes after rf ablation in patient with liver metastases from colorectal cancer . complications radiofrequency ablation ( rfa ) is a relatively low - risk procedure with a low rate of morbidity and mortality [ 22 ]  . few complications are associated with rf ablation [ 2325 ]  . major complications are related to tumor size , number of ablation sessions , electrode type and operator experience . post - ablation syndrome is a common phenomenon after rf ablation of solid abdominal tumors [ 24 ]  . 
most patients should be able to resume normal activity within 710 days . possible complications with an incidence \5 % include shoulder pain , cholecystitis , damage to the bile ducts resulting in biliary obstruction , damage to the bowel , bleeding , hematoma , pneumothorax , pleural effusion , intraperitoneal bleeding or ascites , hemobilia , infection and portal thrombosis , liver abscess , needle tract seeding , collateral damage to proximal vital organs and self - limiting subcutaneous cellulites [ 2325 ]  . in a multicentric study , livraghi et al . 
there were six deaths ( 0.3 % ) , 2.2 % additional major complications including intra - abdominal hemorrhage requiring treatment , tract seeding , liver abscess , intestinal perforation , cardiac arrest , pulmonary embolism , pneumothorax , biloma , and cholecystitis . 
an increased number of rf sessions were related to a higher rate of major complications , whereas the number of complications was not although most institutes have reported treating lesions b5 , there is no contraindication as to the number of lesions [ 9 , 10 , 1416 ]  . imaging techniques radiofrequency ablation is typically used under us - guidance but ctand mr - guided rf ablation are also available in the treatment of crlm patients [ 1018 ]  . 
contrast - enhanced ultrasound can be performed after the end of the procedure for an initial evaluation of treatment effects . ct and mr images obtained 46 weeks after therapy demonstrate successful treatment as a non - enhancing area with or without peripheral enhancing rilater follow - up imaging studies should be aimed at detecting local tumor fig . 
1 transverse t1 - weighted magnetic resonance ( mr ) image ( tr 100 , te 4.76 , st 8 ) in a 53 - year - old female patient with a metastatic lesion from colorectal cancer in segments four and seven of the liver fig . 
some authors consider prfa as the therapeutic standard in the treatment renal neoplasms in non - operable patients due to comorbid conditions and in patients with mild - moderate renal failure , to preserve residual renal functionality . 
the use of prfa has become more and more widespread due to a rise in the incidental detection of renal cell carcinomas with the ever - increasing use of imaging for the study of abdominal diseases . 
lanzara , second university of naples , naples , italy e - mail : antonio.rotondo@unina2.it ablation is an effective therapy with a low level of risk of complications , which provides good results in selected patients over short and medium term periods of time , however up to now few long - term studies have been carried out which can conrm the effectiveness of prfa . keywords renal cell carcinoma ( cid : 2 ) percutaneous radiofrequency thermal ablation introduction in recent years , an increase in renal cell carcinoma ( rcc ) has been observed ( with more than 65.150 new cases expected in the united states in 2014 ) [ 1 ] , due to the everincreasing use of imaging methods . more than half of the new cases are detected incidentally and the number of cases of renal tumors has doubled during the past 50 years [ 25 ]  . for many years , radical nephrectomy surgery was considered the best therapeutic approach for patients with rcc conned to the kidney . there is a low risk of mortality for young patients who undergo surgical resection , however , it is often responsible for serious morbidities [ 6 , 7 ]  . partial resection with the preservation of renal parenchyma has increased for the treatment of small and localized rcc . 
this technique has recently met with success as it has proved to give similar results to total nephrectomy in a 5 - year follow - up reported in an oncological study [ 8 ]  . the preservation of renal functionality is essential in patients with rcc , multiple rcc and / or hereditary renal cancer syndromes and various comorbidities . this requirement has led to the development of minimally invasive ablative techniques , since many tumors 500 radiol med ( 2014 ) 119 : 499511 identied incidentally are low grade , smaller and with rates when detected in asymptomatic longer survival patients compared to other types of cancer [ 9 ]  . for some years , the percutaneous radiofrequency ablation ( rfa ) of renal tumors has been proposed as a therapeutic option for patients with important comorbidities , such as solitary / single functioning kidney , reduced kidney function and transplanted kidney , to prevent the impairment of renal functionality . although radiofrequency needle electrodes can also be used during surgery , most of the benets and experience deriving from this technique were achieved by means of imaging guidance percutaneous procedures [ 10 ]  . this review reports the principles , techniques , indications , effectiveness , complications , the ways of imaging guidance of the needle electrode and the follow - up of the thermal ablation radiofrequency percutaneous treatment of renal neoplasms . physical principles of radiofrequency ablation radiofrequency ablation or radiothermal ablation ( rita , radiofrequency interstitial tissue ablation ) is a tissuedestruction technique which uses thermal energy generated current high - frequency ( 100500 khz )  . alternating electric the current passes from the tip of the needle electrode to the surrounding tissue by means of ionic vibration , which in turn causes the resistive heating of tissues adjacent to the electrode ( joule effect ) ; the needle actively performs at a depth of 12 mm , while the subsequent phenomenon of thermal conduction allows for the heating of much deeper areas . 
when the tissue temperature reaches 60 ( cid : 3 ) c , alterations of the tertiary structure of intracellular proteins occur causing the denaturation of collagen and lipid bilayer damage ; thermal coagulation starts at about 70 ( cid : 3 ) c , while the drying of the tissues occurs at about 95100 ( cid : 3 ) c , causing coagulative necrosis . 
higher temperatures are not recommended as they induce tissue charring , thus causing an increase in impedance and a reduction in the effectiveness of the treatment [ 11 ]  . the amount of thermal damage depends on the diameter of the needle electrode gauge , on the length of the exposed tip and on the duration of the thermal energy administration as well as the average local temperature achieved during the procedure [ 12 ]  . procedural aspects of a radiofrequency generator connected to the main electricity network , a needle electrode ( with a variable gauge ) placed within the lesion to be treated and dispersive electrodes ( ground pads or grounded plates ) closing the circuit [ 13 ]  . needle electrodes are available on the market which release metal hooks that allow for the distribution of thermal energy over a larger area of tissue by means of a special control button located on the handle . 
each application lasts 15 min until the prescribed temperature is reached . the needle electrodes available today are equipped with cooling systems composed of an automated infusion pump connected to a 0 ( cid : 3 ) saline solution which is emitted from each hook to prevent or limit the charring of the surrounding tissue [ 14 ]  . percutaneous treatment technique there are several possible techniques for carrying out radiofrequency treatment : intra - operative , laparoscopic and percutaneous imaging - guided treatment . in this study , we focused our attention on imagingguided percutaneous treatment . 
the advantages and disadvantages of each technique will be discussed in a later section . most of percutaneous treatments are performed in mild sedation , although for certain patients a general anesthetic may be required . according to the imaging technique used , patients are placed in a supine , prone or lateral position , depending on the location of the tumor , the presence of anatomical obstacles ( abdominal viscera , ribs , etc . ) and also on the shortest possible route for the needle electrode . 
the ct and mr guidance usually foresee that the patient is placed in prone position . after capturing a pre - procedural image to locate the tumor , it is necessary to determine the exact point in which to insert the needle electrode before disinfecting the skin and administering a 1 % xylocaine subcutaneous injection . a further image is then obtained to conrm that the needle electrode is in the correct position . 
it is then possible to proceed with the procedure by supplying electricity for 1015 min depending on the technology used [ 15 ]  . if residual vital tumor tissue is detected during a postprocedural imaging check up , the needle electrode may be reused and repositioned during the same session . the procedure requires an instrument which makes the patient part of a closed - circuit electrical network composed as suggested by ogan et al . 
1 left bifocal adenocarcinoma in a 67 - year - old woman with a previous right nephrectomy for rcc , who underwent ct - guidance rf thermal ablation ( double treatment in single session )  . 
14 - mm solid lesion in anterior lip of solitary left kidney ( a , b , arrows ) and 16 - mm solid lesion in interpolar region of the same kidney ( c , d , arrows )  . 24 - month follow - up conrms the complete necrosis of two lesions ( e , f , g , h , arrows ) 502 radiol med ( 2014 ) 119 : 499511 absolute contraindications to percutaneous renal rf ablation include sepsis and severe obesity ; patients with bleeding disorders can only undergo these procedures following coagulopathic correction . 
congestive heart failure should not be considered an absolute contraindication for ablation and the risks of the procedure must be evaluated on an individual basis [ 4 , 21 , 28 , 29 ]  . to obtain good results from prfa , the tumor should not have spread beyond gerotas fascia , into the renal vein or lymph nodes ( stage i or ii in the robson classication system or stage t1 - t3a in the tnm classication system ) [ 19 ]  . 
patients should stop taking aspirin and other antiplatelet agents or anticoagulants a few days before undergoing treatment so that coagulation parameters and renal function can return to normal [ 19 ]  . indicators of outcome the outcome indicators of prfa - treated patients are the size and location of tumor . in a multivariate analysis of 100 prfa of rcc , gervais et al . 
2 47 - year - old male patient with 10 - mm renal adenocarcinoma region of right kidney ( contrastlocated in anterior enhanced ct ) , who underwent ct - guidance rf thermal ablation . prior to rf treatment ( a ) , ct scan in venous phase shows a small interpolar solid lesion with minimum contrast enhancement ( arrow )  . 
30 - day ( b ) and 36 - month ( c ) follow - up contrast - enhanced ct in arterial phase show no evidence of residual neoplastic disease ( arrows ) radiol med ( 2014 ) 119 : 499511 fig . 
3 73 - year - old man with 15 - mm adenocarcinoma originating in the interpolar region of right kidney , with endophytic development , undetectable at unenhanced ct , who underwent ct - guidance rf thermal ablation . 
4 73 - year - old male with a nodular renal adenocarcinoma treated with ct - guidance rf thermal ablation in the presence of an anatomical anomaly ( fusion of two kidneys on the right side )  . contrast - enhanced ct : renal solid rounded 22 - mm lesion , hypervascular and exophytic ( a , arrow )  . 
during the follow - up , contrast - enhanced ct scan at 1 month ( c , arrow ) and contrast - enhanced mr scan at 24 months ( d , arrow ) show no evidence of enhancement of treated lesion in agreement with complete necrosis . 
5 84 - year - old patient with a 38 - mm adenocarcinoma in upper right renal pole , who underwent two sessions of ct - guidance rf thermal ablation . 
one month after treatment , a large necrosis with a small apical - medial eccentric zone was observed by means of contrast enhancement , attributed to residual neoplastic disease ( b , arrow ) , submitted to a second prfa 2 weeks later . 
the placement of the needle electrode during the rst treatment at axial oblique mpr image ( d ) ; the needle electrode placement in apical - medial region ( site of residual neoplastic disease ) during the second prfa session ( e ) ct guidance guarantees a higher level of safety during the procedure compared to the us guidance since ct denes more accurately and comprehensively the relationship between the hooks / electrodes ( from 3 to 9 ) and the anatomical structures that may be damaged by hyperthermia ( bowel loops , large vessels , adrenal gland )  . moreover , ct also enables us to take the shortest posthe needle while avoiding anatomical sible route for obstacles ( ribs , vertebral pedicles , viscera and abdominal vessels ) by carrying out multiplanar reformations ( mpr ) [ 37 , 38 ] ; conversely , ultrasound imaging forces the operator to insert the needle into internal organs that act as an acoustic window ( liver parenchyma for the right kidney , spleen for the left kidney )  . as observed by boss and lewin [ 33 , 3942 ] , mr is well suited for guidance during prfa of renal tumors , due to its intrinsically high soft - tissue contrast and its ability to obtain almost real - time images ( rapid t1 - weighted gradient - echo sequences and t2 - weighted : steady - state free procession sequences )  . 
post - ablation modications in tumor tissue are detectable in both t1and t2 - weighted sequences . the evaluation of small central nodules without repeated injections of contrast medium , as in ct , mr makes it an excellent potential guidance of percutaneous rf ablation of renal malignancies , but the low prevalence of open mr system high - eld - strength and the high cost of non - magnetic materials used in these procedures , currently limit the application of this imaging methods in clinical practice [ 33 , 3942 ]  . role of pre - ablation biopsy some researchers suggest that in most cases biopsy does not signicantly alter diagnosis compared to non - invasive imaging ; furthermore , the percutaneous biopsy of renal neoplasms measuring \3 cm , can be complicated by sampling issues which can cause diagnostic errors [ 30 ]  . with the increased use of percutaneous ablation , the role of pre - procedural biopsy is being reconsidered , as these techniques do not allow for histopathological analysis relative to surgical resection [ 43 ]  . radiol med ( 2014 ) 119 : 499511 fig . 
6 85 - year - old male patient with a 4.5 - cm clear - cell adenocarcinoma originating in right kidney , which presented a peripheral pseudocapsule and a minute zone of central necrosis , who underwent single session of ct - guidance rf thermal ablation . 
contrastenhanced ct oblique axial mpr ( a , c ) and parasagittal mpr ( b , d ) scans in the arterial phase before ( a , b ) and 1 month after ( c , d ) prfa . 
at 1 - month follow - up ct , there is no evidence of enhancement of the treated lesion due to the radicality of treatment ( c , d )  . 
no evidence of enhancement of renal lesion prfatreated ( arrows ) indicates the radicality of the treatment ( b , arrows )  . a small cortical renal cyst coexists ( a e b , head - arrows ) several studies of rcc ablation have in fact included patients diagnosed radiologically with renal cancer who did not undergo a percutaneous biopsy [ 21 , 22 ]  . this might have lead to an overestimation of the positive results of rf as benign tumors such as angiomyolipomas and oncocytomas may have been included in these data [ 43 ]  . 506 radiol med ( 2014 ) 119 : 499511 fig . 
note that the treated lesion is devoid of contrast enhancement with unchanged volume over time , increases in density in unenhanced scans due to an initial calcication of coagulative necrosis ( a , small arrows )  . 
among these , 95 rccs were smaller than 3.7 cm , 21 rcc out of 30 larger tumors ( [ 3.7 cm ) were completely ablated after a second treatment with rf , with 9 ndings of residual tumor at follow - up . only a small number of patients with hereditary forms of renal cancer were included in the various clinical cases mentioned above . in the clinical records studied by hwang et al . 
 [ 45 ] composed of 24 patients with hereditary forms of kidney cancer , 17 patients were successfully treated with rf at average term follow - up ( 1 year )  . 
15 of the 17 patients were suffering from von hippellindau disease , while one had birthogg dube syndrome and another had hereditary rcc . some authors [ 46 ] showed that prfa ( 86 patients ) affects renal function less than partial or radical nephrectomy ( 85 and 71 patients , respectively ) , in whom a greater decrease in gfr was observed at each control . renal function is preserved even in solitary kidney patients as observed by jacobson et al . 
9 66 - year - old woman with a prior right nephrectomy and partial surgical resection of left lower renal pole for adenocarcinoma , who underwent prfa treatment of a residual 20 - mm tumor located in resection margin of solitary left kidney . 
oblique axial ct reconstructions ( mpr ) show the follow - up contrast - enhanced ct , 1 month after positioning of the needle electrode into the lesion ( b )  . 
it is important to note at procedure ( c , arrow ) and at contrast - enhanced mr 3 months after the procedure ( d , arrow ) , avascular tissue indicates complete necrosis . 
36 - month follow - up conrms the radicality of the treatment ; note the no evidence of contrast enhancement ( e , arrow ) hereditary renal neoplasms complications particular attention should be paid when treating patients with familial or hereditary renal malignancies as the ablation procedure must be optimized to take into consideration nephron - sparing , which is an important prerogative as it could lead to the development of metachronous tumors . 
for this purpose , it is necessary to reduce the margin of the treatment to a few millimeters in close vicinity of the tumor . in this type of patients , the impact of thermal ablation on glomerular ltration is minimal compared to surgery according to the urine creatinine levels observed 24 h after the procedure [ 48 ]  . one study analyzed the glomerular ltration rate in patients affected by von hippel - lindau disease who underwent prfa and previous renal surgery , which conrmed a limited decrease in renal functions following the ablation procedure ( 6.4 % increase in serum creatinine and 12.8 % reduction in gfr ) [ 49 ]  . according to observations found in recent literature , the complication rate following prfa of rcc seems to be lower than that observed in partial or radical nephrectomy . prfa is in fact related to lower morbidity and no mortality . 
the incidence of complications arising from partial or total nephrectomy is 1426 % , whereas the complication rate for ct - guided prfa is 011 % [ 3 , 5052 ]  . some authors [ 53 ] divided the complications into two groups , namely major and minor complications , according to the classication system of the society of interventional radiology ( sir ) [ 54 ] table 1 . minor complications ( classes a and b ) include : mild hematomas , neuromuscular complications , pneumothorax , hematuria and bladder globe , tumor seeding of needle electrode track . major complications ( class c ) include ureteral injuries , retroperitoneal hematomas requiring transfusion , bowel 508 radiol med ( 2014 ) 119 : 499511 table 1 complications of radiofrequency thermal ablation of renal tumors minor complications ( a ) no therapy , no consequences evolution ; no consequences major complications ( b ) therapy during hospitalization for observation of clinical ( c ) required therapy , minor hospitalization ( \48 h ) ( d ) required therapy , prolonged hospitalization ( [ 48 h ) permanent consequences ( f ) exitus perforation and perirenal abscess ( treated with percutaneous drainage )  . class a and b complications hematomas are a common complication of prfa with an incidence of 68 % [ 55 ]  . 
 [ 56 ] , caused by local side or paraspinal musculature traumas which occur in 5 % of all thermal ablation procedures . iatrogenic pneumothorax occurs during the prfa treatment of renal tumors located at the upper pole and is more frequent in ultrasound - guided procedures compared to ct - guided treatment . 
a 24 % incidence of this complication was observed in zagorias [ 22 ] clinical cases . another prfa side effect is mild hematuria which is self - limiting within the rst 24 h after the procedure , especially in centralized renal tumors . 
globe bladder rarely occurs [ 57 ]  . the risk of tumor seeding occurring at the entry point of the needle electrode is an extremely rare complication and has only been observed in one case of studies that we examined [ 58 ]  . class c complications the thermal ablation procedure of renal tumors located in close proximity or against the renal pelvis , ureteropelvic junction and proximal ureter can be risky as it can cause damage to the ureteral or collecting system , which can then cause ureteral obstruction and urinoma . these complications were observed by weizer et al . [ 59 ] in 4 % of cases ( one case out of 24 patients ) at a follow - up 1 month after the procedure . hemorrhage or signicant bleeding following prfa occurs in 18 % of the cases with blood transfusion requirements in 12 % , as observed in a multicenter study carried out on 271 patients by zagoria and gervais et al . 
bleeding is caused by mechanical injuries to major vessels and occurred mainly in the past due to the use of larger needle electrodes which were consequently more difcult to insert . 
 [ 21 ] performed the follow - up of the patients with ct or mr imaging with and without intravenous administration of contrast medium at 1 , 3 and 6 months after procedure . 
10 75 - year - old woman with a 35 - mm adenocarcinoma arising from right kidney , who underwent ct - guidance rf thermal ablation . prior to prfa treatment , a strong contrast enhancement of the right renal lesion is observed in which there is a thin rounded calcication and neoplastic tissue in the middle ( a , arrow )  . 
 [ 64 ] have analyzed the dimensional variations of treated renal tumors during follow - up , examining 18 patients at prospectively mr , and observed a 10 % increase in size of the area treated with prfa within the rst 2 weeks and a subsequent 30 % decrease during the following 6 months . hypervascular portion ( c , arrow ) , that could be due to residual disease . 
the mwa has some technical advantages such as the ability to 510 radiol med ( 2014 ) 119 : 499511 treat larger lesions thanks to a wider range of application ; moreover , the diffusion of heat in vital tissue is not limited by the impedance tissue and therefore it is possible to reach higher temperatures within the tumor lesion [ 66 ]  . cryoablation also seems to be an alternative to rfa and has some technical advantages such as the possibility of visualizing the area to be ablated ( well dened and hypodense at ct scans ) during treatment [ 67 ]  . 
over the years , much has been done on prevention and cure of this disease by surgery , chemotherapy and radiotherapy [ 1 ]  . the landscape of medicine is constantly changing , and for the past 40 years , interventional radiologists have been responsible for much of the medical innovation and development of the minimally invasive procedures that are commonplace today . 
thus , interventional radiology ( ir ) can be inserted as the fourth pillar in tumour therapy [ 1 ]  . appropriate treatment of malignancy is dependent on a timely denitive diagnosis and on accurate staging of disimaging techniques have ease . 
biopsies to establish histological diagnosis are increasingly performed using minimally invasive techniques by interventional radiologists . these minimally invasive techniques are applicable to a wide range of biopsy sites and , in most organ systems , have g . 
in an ir technique similar to that used in chemoembolisation , genetic agents may be administered directly into the tumour mass by selective arterial injection , after which the vessel is embolised thus limiting adverse effects and prolonging agent dwell time which is believed to improve genetic transfer rate . 
although there are few studies limited to small patient cohorts , this techniques is a promising one [ 3 ]  . as one can observe ir has improved majorly in recent years and can be inserted as the fourth pillar in cancer therapy alongside surgery , chemotherapy and radiotherapy . in my opinion , the essence of the treatment modality of 450 radiol med ( 2014 ) 119 : 449450 interventional oncology is technical skill , although it may also sometimes depend upon various kinds of devices and drugs . 
modications to the various applications , in particular combining the techniques with highquality imaging and intra - operative approach has enabled real - time treatment monitoring and signicant improvements in safety . 
brunese department of radiology , universita` degli studi del molise , campobasso , italy keywords pancreatic cancer ( cid : 2 ) radiofrequency ablation ( cid : 2 ) microwave ablation ( cid : 2 ) high frequency focused ultrasound ( cid : 2 ) cryoablation ( cid : 2 ) irreversible electroporation ( cid : 2 ) review introduction the term tumor ablation is dened as the direct application of chemical , thermal or electrical energy to a specic focal tumor in an attempt to achieve eradication or cytoreduction inducing cellular necrosis [ 1 ]  . the methods of tumor ablation most commonly used in current practice are divided into two main categories : thermal ablation [ radiofrequency ( rfa ) , microwave ( mwa ) , high - intensity focused ultrasound ( hifu ) and cryoablation ] and chemical ablation . irreversible electroporation ( ire ) is a non - thermal tissue ablation technology that uses very short pulses of highvoltage , low - energy direct current to induce cellular death by creating cellular membrane disruption [ 1 ]  . over the last decade , ablation has become increasingly accepted for the treatment of solid parenchymal lesions , in particular liver tumors [ 2 ]  . 
we identied additional studies through hand searches of bibliographies from primary studies , review articles and key we considered also case reports . we excluded papers that contained data reported previously . the primary endpoint was to investigate safety and complications of these techniques . 
totally , 94 males and 71 females were treated , with a mean age of 65 years old ; 2 articles did not report the sex of 13 patients [ 9 , 16 ]  . 
the tumor size ranging from 13 to 65 mm , with a mean size of 42 mm . tumor was located in the pancreatic headuncinate process in 112 patients and in the bodytail in 55 patients . 
only 4 patients were treated percutaneously with ct guided ; the other 176 underwent laparotomy and open ablation , associated in most cases with palliative surgery : biliary bypass , gastric bypass or double bypass . 
in another case , 10 days after rfa , radioactive 125 i seeds were implanted into the residual lesion area close to the bowel using the same approach [ 4 ]  . 
rfa was performed from 2 to 15 min for open technique and up to 18 min for percutaneous approach , at a temperature variable from 30 to 105 ( cid : 3 ) c . 
the power at which rfa was performed was reported in seven studies and also varied across studies , ranging from 40 to 500 w [ 3 , 5 , 8 , 9 , 11 , 15 , 16 ]  . complications related to rfa included , by incidence : ascites , vomiting , pancreatic stulae , acute pancreatitis , gastrointestinal bleeding , portal vein thrombosis , pleural effusion , pneumonia , duodenal lesion , and pancreatic pseudocystis . 
complications related with surgery included : biliary leak , hemoperitoneum , abdominal uid collection , gastric bypass stula , and gastric ulcer . systemic complications were : septic shock ( 1 / 180 ) , acute renal failure ( 1 / 180 ) , hepatic failure ( 1 / 180 ) , and psychosis ( 1 / 180 )  . 
data regarding long - term pain control and quality - of - life assessment were not available in all the studies selected , and this represented a drawback for the clinical application of rfa . 
registered post - operatively severe lifethreatening complication : a pancreatico - cutaneous stula with bleeding from splenic artery and a necrotizing pancreatitis . discussion rfa of the pancreas was initially applied to animal models . 
 [ 8 ] published the rst clinical study in 2000 . since then , few studies and case reports have been published from various groups of investigators [ 35 , 817 ]  . the revision of the studies revealed some important factors to prevent the occurrence of complications . the temperature at which rfa is performed should not exceed a maximum of 90 ( cid : 3 ) c . 
 [ 17 , 20 ] underlined that temperatures higher than 90 ( cid : 3 ) c carried a double risk of thermal injuries : portal and / or mesenteric vein thrombosis and duodenal ulcer and bleeding . 
whole tumor ablation should be avoided , prevent high temperatures diffusing to healthy surrounding tissues ( the pancreas itself , common bile duct , duodenum )  . a peripheral rim should be left and considered as a safety margin to prevent thermal damage [ 20 ]  . moreover , the distance between the rfa needle and surrounding structures should be [ 5 mm from porto - mesenteric vessels and [ 10 mm from duodenum . furthermore , thermal damage to the duodenum can be prevented by intraluminal duodenal cooling [ 21 ]  . the largest series was reported by cantore et al . 
the authors suggested that the use of a multimodal approach ( rfa , rct and iasc - triple approach strategy ) achieved survival benet in different ways : rct has been shown to be effective in local disease control ; rfa is a local ablative method that destroys tumor by thermal coagulation and protein denaturation ; regional drug delivtumor sites and ery increased drug concentrations at reduced complications due to systemic drug exposure . those patients who received the multimodal treatment had an overall survival of 26 months . 
they nally identied three independent prognostic factors for overall survival : performance status , triple approach strategy , and basal ca 19 - 9 value [ 17 , 20 , 22 ]  . increased evidence indicates that rfa induces the expression of hsp70 which inuences a variety of immunological processes [ 21 ]  . 
the aim of treatment was to obtain a cytoreductive effect of the tumor associated with destruction of celiac ganglia . to our knowledge , there is no other report of palliative surgery associated with rfa of a pancreatic mass and celiac plexus in literature . although the results obtained from rfa studies are very heterogeneous , rfa appears to be a feasible option for the local control of pancreatic tumor . however , safety still remains under debate : the quite high rate of postoperative complications , the thermal damage of the surrounding organs and the inevitable heat - sink effect still limit the application of this method . two retrospective studies involving a total of 25 patients with locally advanced pancreatic cancer treated with mwa were analyzed ( table 2 ) [ 23 , 24 ]  . totally , 16 males and 9 females were treated . 
mwa was performed from 1 to 10 min maintaining a power ranging from 45 to 100 w . one major complication ( 4 % ) related with mwa was registered in one patient that developed one pseudoaneurysm of the gastroduodenal artery , which was treated with an endovascular approach [ 24 ]  . 
over the last three decades , multiple loco - regional approaches such as transarterial chemoembolization or radioembolization were shown to effectively achieve local tumor control , offering signicant survival benets for selected patients with intermediate to advanced - stage disease ( barcelona clinic liver cancer stage b and c )  . 
these therapies provide a dual benet of safely delivering a highly cytotoxic payload directly to the tumor while reducing systemic toxicity . this capability maintained the advantage of iats over conventional systemic chemotherapy . 
the introduction of sorafenib as a systemically applicable drug , the rst of its kind to provide survival benets by means of oral monotherapy , contributed to a paradigm change . 
the idea of combining this novel agent with iats seemed intriguing , and a variety of national and international clinical trials were initiated to explore the potential benets of this exciting new option . 
in this review , we will provide a brief state - of - the - art update on the most frequently used intra - arterial modalities and discuss the molecular mechanism , potential biomarkers as well as the safety prole of sorafenib . 
geschwind ( & ) division of vascular and interventional radiology , russell h . morgan department of radiology and radiological science , the johns hopkins hospital , sheikh zayed tower 7203 , 1800 orleans st , baltimore , md 21287 , usa e - mail : jfg@jhmi.edu keywords liver cancer ( cid : 2 ) hepatocellular carcinoma ( cid : 2 ) tace ( cid : 2 ) deb - tace ( cid : 2 ) radioembolization ( cid : 2 ) intra - arterial therapy ( cid : 2 ) sorafenib introduction hepatocellular carcinoma ( hcc ) is currently a major public health problem worldwide . 
the past 30 years have seen advances in several catheter - based intra - arterial therapies ( iats ) such as transarterial chemoembolization ( tace ) and yttrium ( y ) 90 radioembolization [ 2 ]  . 
the scientic rationale for all iats lies in the fact that in contradistinction to healthy liver tissue which is supplied by the portal vein , most liver tumors draw their blood almost exclusively from the artery . this can then be exploited for selective targeting and treatment . 
indeed , this characteristic allows for tace and radioembolization to deliver a high dose of chemotherapy or radiation directly to the tumor , while preserving normal hepatic parenchyma [ 4 ]  . almost all iats involve the element of embolization as a key step of the procedure , thus preventing the washout of the payload and achieving massive necrosis through radiol med ( 2014 ) 119 : 476482 devascularization [ 5 ]  . 
indeed , the stabilization of the hypoxiainducible factor 1 alpha ( hif - 1 alpha ) causes the expression of the vascular endothelial growth factor ( vegf ) , leading to rebound neovascularization , tumor regrowth , progression and ultimately reduced overall survival [ 6 , 7 ]  . since hcc is known to rely on the formation of new blood vessels for local progression , signicant efforts were made to understand the role of microvascular changes that occur due to the imbalance of proand anti - angiogenic signaling within tumor tissue . 
as a result of these ndings , inhibiting the angiogenic pathway during treatment with tace is a promising goal . since angiogenesis has been rst described as one of the hallmarks of tumor growth , targeting molecular mechanisms of hypoxia and neovascularization has become an organizing principle for drug discovery [ 9 ]  . 
however , no drug with antiangiogenic activity that has entered clinical trials since the 1980s achieved signicant clinical benets in patients with advanced hcc , with one exception : sorafenib [ 10 ]  . 
the successful introduction of sorafenib was preceded by two phase iii trials [ sorafenib hepatocellular carcinoma assessment randomized protocol ( sharp ) and the asia - pacic study ] [ 10 , 11 ]  . 
breaking through the 6 - month median , overall survival ceiling with selected patients surviving for up to a median of 10.7 months , sorafenib quickly received wide acceptance and was adopted throughout multiple disciplines . 
the positive results from the sharp trial lead to the approval of sorafenib by the food and drug administration ( fda ) as well as the european counterpart for the treatment of advanced hcc in 2007 [ 12 ]  . 
given this scientic rationale and the demonstrated impact of this new agent on patient survival , several prospective clinical trials have been designed ( and many are still underway ) to assess the potential of the truly unique combination of iats with sorafenib . in this review , we will provide a brief update on the iats used in this combination and discuss the molecular mechanism , potential biomarkers as well as the safety prole of sorafenib , the knowledge of which has evolved signicantly since the introduction of this drug . 
finally , this review will examine the evidence for clinical outcomes for the combination of different iats with sorafenib . intra - arterial techniques : what are the differences ? conventional tace ( ctace ) the concept of the conventional tace has been introduced over 30 years ago [ 13 ]  . 
during ctace , a mixture of conventional chemotherapeutic agents combined with an oil - based contrast medium ( lipiodol ultrauide ; laboratoire guerbet , france ) is selectively delivered to the tumorfollowed by temporary or permanent feeding artery , embolization . 
in the usa and europe , most reported protocols now include doxorubicin and mitomycin c since the powder form of cisplatin is no longer available . regardless of the drug used , the key component of tace is the mixture of lipiodol as a drug carrier and chemotherapy which results in the formation of an emulsion ( water in oil ) that allows the drug to be delivered to the cancer cells . 
due to the hypervascularized character of most hcc lesions and the absence of kupffer cells , lipiodol can persist within tumor nodules for several weeks after embolizing tumor vasculature up to the capillaries [ 15 , 16 ]  . 
the subsequent administration of embolic material [ such as gelfoam , polyvinyl alcohol ( pa ) particles or trisacryl gelatin ( tg ) microspheres ] serves a dual purpose ; it causes stasis in segmental and sub - segmental arterial branches and prevents washout of the previously deposited emulsion of chemotherapy - lipiodol [ 17 ]  . 
embolization with gelfoam ( a biodegradable gelatin sponge ) has proven safe and effective for the occlusion of larger blood vessels [ 18 ] , but it has been largely replaced by nonbiodegradable tg microspheres ( merit medical , usa ) which can be used to occlude very distal tumor - supplying blood vessels [ 19 ]  . drug - eluting beads - tace ( deb - tace ) the development of polymer - based drug - eluting microspheres ( drug - eluting beads , debs ) as a robust drug delivery system improved on the ability of ctace to deliver higher concentration of cytotoxic agents directly to the tumors while minimizing systemic toxicities caused by chemotherapy [ 20 ]  . 
the pharmacodynamic benets of this technique led to a shift away from ctace toward debtace in the treatment of patients with hcc especially in the usa and europe [ 21 , 22 ]  . 
although two major types of drug - eluting microsphere are available ( dc beads made by biocompatibles / btg in the uk and quadspheres / hepaspheres made by merit medical in the usa ) , clinically neither is approved as a drug delivery system but rather as embolic material . 
these microspheres can be loaded with several ionic agents ; however , doxorubicin ( debdox ) is the most commonly used in the treatment of hcc [ 23 , 24 ]  . 478 radiol med ( 2014 ) 119 : 476482 the bulk of the clinical trials utilized the dc beads that are made of nonbiodegradable materials , such as polyvinyl alcohol ( pva ) and are soft , compressible , spherical particles . 
they range in size from 75 to 900 lthe smaller bead diameters achieve a more distal embolization and more extensive necrosis as compared to larger beads [ 25 ]  . the drug uptake of the dc beads occurs through an ionexchange mechanispharmacokinetic studies have demonstrated that drug elution occurs gradually and only in an ionic environment once the microspheres are delivered to the tumor . 
furthermore , histopathological analysis described the high efciency of debmediated drug delivery and release to the tumor tissue , causing local coagulative necrosis and an inammatory brotic tissue [ 27 ]  . radioembolization radioembolization utilizes the same scientic rationale as the one used for tace . 
a marked difference , however , is the payload in this procedure which consists of radiation in the form of yttrium 90 that is being delivered to the tumor . the infusion of small embolic particles made of or loaded with 90yttrium ( y90 ) , a pure b particle - emitting radionuclide with a half - life of 64.1 h , is a suitable technique to achieve tumoricidal effects while preserving healthy liver tissue and reducing systemic toxicities [ 28 ] that are typically encountered with external beam radiation [ 29 ]  . 
there are two radioembolization devices currently available for clinical use ; the resin - based sir spheres ( sirtex medical ltd . , australia ) and the glass - based theraspheres ( mds nordion , canada ) [ 30 ]  . 
however , only the 2030 lm sized theraspheres are approved for radioembolization of hcc under a human device exemption ( hde ) from the fda . both glass and resin microspheres deliver high cumulative doses to the tumor , which can vary from 100 gy to more than 3 , 000 gy . sorafenib : targets , safety and biomarkers of response sorafenib ( nexavar , bayer health care , berlin , germany ) is an orally applicable multi - kinase inhibitor with activity against raf - 1 , b - raf , vegf2 receptors , pdgf receptors and c - kit receptors [ 10 ]  . 
initially designed as a selective inhibitor of the raf - 1 protein , its broad activity against multiple targets involving several pathways of angiogenesis and tumor apoptosis was soon conrmed , which is also being attributed to a relatively broad toxicity prole [ 31 , 32 ]  . 
although sorafenib was generally well tolerated in the sharp trial as well as in the asia - pacic trial , it caused a range of adverse effects ( aes )  . 
among the grade 3 drug - related aes , diarrhea ( 8 % ) , hand - foot skin reactions ( hfsr 8 % ) , hypertension ( 2 % ) as well as abdominal pain ( 2 % ) were among the most common toxicities [ 10 ]  . 
additional data on the overall safety prole of the drug is currently being collected by the global investigation of therapeutic decisions in hepatocellular carcinoma and of its treatment with sorafenib ( gideon ) , which is an ongoing , prospective phase iv trial . 
this international study investigates the use of sorafenib in advanced - stage , unresectable hcc patients under real - life conditions [ 33 ]  . the recently published second interim analysis conrmed the previously established safety prole of sorafenib across child - pugh and barcelona clinic liver cancer ( bclc ) stages [ 34 ]  . the absence of a reliable biomarker for tumor response in these patients continues to be an unresolved issue in both , the systemic delivery alone as well as combination of sorafenib with iats [ 14 , 35 ]  . 
the results of this large , placebocontrolled study , which was conducted in over 300 patients , appeared to be consistent with the mechanism of angiogenesis - dependent disease progression of hcc . 
while most trials continue to rely on imaging response parameters , such as the response evaluation criteria in solid tumors ( recist ) , modied recist ( mrecist ) as well as the european association for the study of the liver ( easl ) guideline , a recent radiological pathological analysis did not identify one of these markers as a reliable predictor of tumor response to the treatment with sorafenib [ 37 ]  . sequence of administration : what is the rationale ? in order to correctly interpret the plethora of data emerging from the completed and ongoing trials for the combination treatment , three categories of administration regimen have been proposed : sequential , interrupted and continuous [ 38 ]  . the sequential schedule applies a consecutive approach , radiol med ( 2014 ) 119 : 476482 the sequential application might where the systemic therapy is given after the completion of the last session of the intra - arterial treatment . 
the rationale for the sequential schedule lies in the observation that vegf , the main molecular switch to induce neo - angiogenesis in hcc lesions , is upregulated within the rst 36 h after embolization [ 39 ]  . 
furthermore , there is evidence supporting the role of angiogenesis in liver regeneration after parenchymal damage , which is also being inicted by intra - arterial approaches [ 40 ]  . 
although safety seems to be the focus of the interrupted schedule , a clear disadvantage is the sub - therapeutic level of sorafenib within tumor tissue precisely when it is needed the most . the continuous administration of sorafenib during intraarterial therapy is used with the intent to balance the effects toward efcacy , while accepting the risk of increased toxicity . 
this approach may lead to an increased intratumoral level of sorafenib , thus making the tumor more susceptible for the toxic effects of the intra - arterially delivered payload [ 41 ]  . 
thus , it can be assumed that only a prospective , randomized trial will ultimately be able to address all questions arising from the variety of possible combinations . clinical outcome : is there a benet ? intra - arterial therapy and sorafenib one of the rst fda - sanctioned experiences with the combination of deb - tace and sorafenib in the usa was a single - center prospective phase ii trial , conducted in order to evaluate the safety and efcacy of concurrent sorafenib and deb - tace therapy . 
according to the protocol , patients were treated on a 6 - week cycle regimen , in which one cycle consisted of 400 mg sorafenib twice daily , initiated 7 days prior to the rst deb - tace . 
the 35 patients were treated with a total of 128 cycles of therapy . all patients received deb - tace and the mean dose of doxorubicin decreased over time ; cycle one : 75 mg ; two : 60 mg ; three : 49 mg . 
according to easl guidelines for tumor response assessment , 58 % of the patients showed objective tumor response , and the disease control rate was 100 % with no patient showing progression . 
as for the secondary end point of this trial , the published data also demonstrated promising survival outcomes , and follow - up studies will provide a more detailed answer for this important question . the sorafenib or placebo in combination with debtace for intermediate - stage hcc ( space ) trial is the rst international , multicenter attempt to investigate the role of the combination of deb - tace with sorafenib . 
this phase ii randomized , double - blinded , placebo - controlled clinical trial enrolled patients across 85 centers in europe , north america and asia and was recently presented ( not yet published )  . 
here , a total of 307 eligible patients were randomized to receive either sorafenib ( n = 154 ) or placebo ( n = 153 ) in combination with deb - tace . 
the dosage was similar to the trial described above , and patients received a dose of 400 mg sorafenib twice daily or a matching placebo continuously on cycle duration of 4 weeks . 
all patients received deb - tace within the rst week after the rst dose of sorafenib / placebo and subsequently on day 1 of cycle 3 , 7 and 13 , respectively . 
when further stratied , ttp at the 480 radiol med ( 2014 ) 119 : 476482 25th and 75th percentile was 112 days / 88 days and 285 days / 224 days in the sorafenib and placebo groups , respectively . 
interestingly , the hazard ratios were quite low favouring the combination treatment over the placebo arm . however , the overall preliminary results were somewhat disappointing as no statistically signicant benets regarding overall survival and ttp were shown and the authors concluded that the observed differences were not clinically meaningful [ 43 ]  . multiple trials investigating the outcome of ctace in combination with sorafenib are also available . 
in particular , a south korean nonrandomized prospective single - arm phase ii study investigating the combination of transcatheter arterial chemoembolization and sorafenib for patients with unresectable hepatocellular carcinoma ( cotsun ) focused specically on safety , tolerability and ttp . 
in this study , handfoot skin reactions were the most common reason for dose reduction or interruption and 17 out of 50 patients discontinued the combined treatment due to disease progression . 
the nal results regarding overall survival will hopefully provide a nal verdict in this asian population . the interim analysis of the ongoing study in asia of the combination of ctace with sorafenib in patients with hepatocellular carcinoma ( start ) trial provided more insight in a similar subset of patients . 
this prospective phase ii single - arm trial investigates the role of the combination in intermediate - stage hcc and subjects the patients to an interrupted treatment schedule with the ctace sessions being performed on demand . 
with a median ttp of 9 months and an objective tumor response rate of 54 % , the combination of ctace and sorafenib showed a similar trend as compared to deb - tace . 
however , no nal results regarding progression - free and overall survival were presented and can be expected until the end of 2014 [ 45 ]  . multiple further trials are underway combining debtace as well as ctace with sorafenib . 
it might be very well possible that the answer about the combination and treatment regimen of sorafenib and tace will be provided by the only phase iii trial that is already underway in the usa . 
this randomized , double - blinded , placebo - controlled multicenter trial which was proposed by one of cooperative oncology groups ( e1208 ) will compare the outcomes of deb - tace with or without sorafenib in hcc patients with invasion ( nct01004978 )  . 
the results of this trial should be made available at the end of 2014 . or without vascular very little data are available for the combination of radioembolization and sorafenib as most of these trials are at an early stage or have not yet started . 
this truly unique , two - arm study correlated the radiological and pathological tumor response for patients treated with ( n = 7 ) or without ( n = 9 ) sorafenib . 
as a result , the adjunct of sorafenib did not achieve any signicant improvement of radiological or pathological response to radioembolization which in itself is a disappointing outcome for sorafenib [ 37 ]  . other ongoing studies should shed more light as to the potential benet of this combination therapy . summary in summary , the combination of sorafenib and intra - arterial therapy in patients with unresectable hcc is safe and appears to be well tolerated regardless of the sequence of administration . 
only then should the combination of sorafenib and intra - arterial therapy be recommended for patients and included in treatment guidelines . conict of interest julius chapiro has no potential conicts of interest and nothing to disclose . 
filippiadis sean tutton alexis kelekis received : 27 january 2014 / accepted : 1 april 2014 / published online : 4 june 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract benign tumors and metastatic bone lesions can be treated by ablation techniques performed either alone or in combination with other percutaneous techniques . 
ablation techniques include ethanol or acetic acid injection and thermal ablation by means of energy deposition [ including laser , radiofrequency , microwave , cryoablation , radiofrequency ionization and magnetic resonance ( mr ) - guided high - intensity focused ultrasound ( hifu ) ]  . 
depending on the lesions location ablation can be combined with cementation with or without further metallic augmentation ; local tumor control can be enhanced by combining ablation with transarterial bland embolization or chemoembolization . 
tutton division of vascular and interventional radiology , medical college of wisconsin , 9200 west wisconsin av , milwaukee , wi 53226 , usa about safety and effectiveness of percutaneous imagingguided ablation for benign and malignant ( primary and metastatic ) lesions . keywords bone ( cid : 2 ) ablation ( cid : 2 ) thermal ( cid : 2 ) chemical ( cid : 2 ) benign ( cid : 2 ) malignant introduction pain is a common complaint in oncologic patients . 
osseous metastasis is the most common source of pain ( 80 % ) in cancer patients with * 25 % meeting no relief from analgesics [ 1 , 2 ]  . 
benign bone tumors are by far more common than malignant forms [ 4 ]  . ablation techniques aim at generating cytotoxic temperatures ( [ 60 and \ - 20 ( cid : 3 ) c ) ( table 1 )  . 
percutaneous ablation techniques include injection of chemical substances such as ethanol or acetic acid , delivery of energy ( radiofrequency , microwave , laser ) aiming at temperature increase , application of extreme cold ( cryoablation ) and high - intensity focused ultrasound ( usually performed under magnetic resonance ( mr ) guidance which totally lacks any invasive character ) [ 511 ]  . 
mwa offers many benets of other ablation techniques and offers several other advantages : higher intratumoral temperatures , larger tumor ablation volumes , faster ablation times , the ability to use multiple applicators simultaneously , optimal heating of cystic masses and tumors close to the vessels and less procedural pathis review aims to provide the reader with an overview about the state of the art of microwave ablation for renal tumors and to cast a glance on the new development trends of this technique . keywords microwave ( cid : 2 ) renal cell cancer ( cid : 2 ) percutaneous ablation ( cid : 2 ) nephrectomy c . 
brunese department of radiology , university of molise , campobasso , italy introduction for several decades , the most pronounced increase in the incidence of new renal cell carcinoma cases has been for clinically localized , small tumors \2.0 cthis trend for small , low - stage tumors has been proposed to be a reection of earlier diagnosis primarily as a result of the widespread and increasing use of non - invasive abdominal imaging modalities such as ultrasound ( us ) , computerized tomography ( ct ) , and magnetic resonance imaging ( mri )  . this increased utilization of modern imaging techniques has unquestionably altered the clinical landscape of solid renal tumors . 
generally , the majority of all renal tumors will be being detected incidentally and the most of them are small ( \4 cm , clinically stage t1a ) , low grade , with a slow growth rate ( 0.35 cm / year ) , a low metastatic potential [ 1 ]  . 
small renal tumors are often diagnosed in elderly patients , older than 65 years , with medical comorbidities 534 radiol med ( 2014 ) 119 : 533540 whom the risk of surgical complications may pose a greater risk of death than that due to the tumor itself , at least in short term [ 2 , 3 ]  . 
furthermore , the high risk of end - stage renal disease after a radical nephrectomy than with a nephron - sparing surgery has encouraged the development of minimally invasive approach such as ablative modalities for selected patients [ 1 , 4 , 5 ]  . 
the continuous improvements and innovations of thermal ablative modalities , as rening probe design and real - time imaging capabilities , allow to renew the great interest in these techniques , in particular for the treatment of t1 renal malignancies [ 1 ]  . thermal ablation is a less invasive , less morbid treatment option thanks to reduced blood loss , lower incidence of complications during the procedure and a less long convalescence compared with traditional surgical approach . retrospective non - randomized studies have demonstrated good efcacy in oncologic short and intermediate term , however still be inferior than partial nephrectomy ( pn ) [ 6 ]  . finally , ablation has some advantages in terms of cost compared to open partial and radical nephrectomy [ 7 ]  . currently , european guidelines recommend the use of ablative techniques in patients with small renal masses , with comorbidities unt for surgery , and in patients with impaired renal function or with only a functional kidney [ 8 ]  . 
at present , the most widely used thermal ablative techniques are cryoablation ( ca ) , radiofrequency ablation ( rfa ) and microwave ablation ( mwa ) [ 9 ]  . 
cryoablation , using tissue temperatures to between - 20 and - 50 ( cid : 3 ) c , causes ice formation within the extracellular space leading cellular dehydration , cell membrane rupture , and nally tissue ischemia [ 11 ]  . 
differently , rfa utilizes alternating electrical currents to induce thermal injury to a lesion [ 12 ]  . advantages of rfa include its minimally invasiveness , reduced pain , and a shorter hospitalization , among disadvantages we found the lack of long - term clinical data , heat sink effect and charring , leading to decreased ablation zones [ 12 ]  . 
mwa offers many benets of other ablation techniques , in particular , rfa , and offers several other advantages , temperatures , including higher intratumoral larger faster ablation times ( maximum 10 min ) , the ability to use multiple applicators simultaneously , optimal heating of cystic masses and tumors close to the vessels , and less procedural pain [ 14 ]  . thanks to its better convection prole , microwave energy tumor ablation volumes , allows a more uniform cell kill in the ablation zone tending to , thanks to new developments of antennas design , a better roundness [ 14 ]  . 
mwa is a relative new technique and it is starting to emerge in the literature now ; however , only few studies have documented its efcacy and longremains term outcomes and much about mwa still unknown , especially in comparison to other ablative methods [ 9 ]  . the following sections aim to provide the reader with an overview about the state of the art of microwave ablation for renal tumors and to cast a glance on the new development trends . microwave energy : physic principles important microwave radiation lies between infrared and radiowave radiation in the portion of the electromagnetic spectrum between 300 mhz and 30 ghz , and including those most commonly used for microwave ablation procedures : 915 mhz and 2.45 ghz [ 14 , 15 ]  . 
heating of the tissue is based on agitation of water molecules inducing cellular death via coagulation necrosis ; the electrical charge on the water molecule ips back and forth 25 billion times a second , depending on the frequency of the microwave energy [ 14 ]  . 
the most feature is that microwaves propagate through all types of tissues and non - metallic materials including water vapor , dehydrated , charred and desiccated tissues created during the ablative process [ 16 ]  . 
in most tissues , the dielectric properties can be considered isotropic and can change substantially during treatment , but microwave propagation is not hindered by these changes [ 14 ]  . microwaves may also , offering more direct heating than other ablation energies , be more potent in organs with high blood perfusion or near larger vessel thanks to reduced heat sink effect [ 14 ]  . microwave ablation in kidney : experimental studies some preclinical studies have been published to evaluate morphology , size , and histologic features of the ablated areas in animal renal cancer . 
the unique physiology of the kidney has important implications in ablation planning . the kidney is a highly perfused organ with approximately four times the perfusion of the liver [ 17 ]  . 
this difference in radiol med ( 2014 ) 119 : 533540 perfusion signicantly alters the results of the bio - heat equation , which estimates the amount of energy that can be deposited in tissue , by increasing the energy lost [ 18 ]  . convection of heat due to overall perfusion and to perfusion by large central vessels can also contribute to a heat sink effect that may result in under treatment of renal tumors [ 18 ]  . experimental comparison to other thermal ablative techniques microwave and radiofrequency ( rf ) ablation are two techniques that generate heat and induce cellular death by coagulative necrosis in two different ways [ 18 ]  . 
heat in rf ablation is generated by converting electrical current into thermal energy by the creation of a closed - loop circuit [ 19 ]  . application of current results in marked agitation of the ions present in the tissues that immediately surround the electrode with resultant frictional heat and thermal damage to the surrounding tissues [ 12 ]  . 
for adequate destruction of tumor tissue , the entire volume of an index tumor must be treated with temperatures that are above the threshold for cell death , typically 5060 ( cid : 3 ) c [ 19 ]  . 
rfa is a reliable and safe ablation technique that has been used successfully for years in the treatment of small renal cell cancer ( rcc ) [ 1 , 20 ]  . 
however , it has some drawbacks : size and sinus extension of the tumor to be treated can increase the risk of technical failure , difculty to completely ablate irregular - shape tumors , major inuence by heat sink effect by blood circulation , depends on tissue impedance [ 21 ]  . cryoablation has been used in the treatment of skin , breast , liver , brain , and bone tumors during the past four decades [ 1 , 9 , 19 ]  . 
during cryoablation , the freezing and thawing process destroys cell membranes and organelles due to the mechanical stresses associated with phase change and ice formation [ 1 , 9 , 19 ]  . 
subsequently after increasing the intracellular osmotic pressure , an inow of water occurs during thawing resulting in tumor cells bursting [ 9 , 19 ]  . cryoablation has the major advantage of real - time monitoring of the ablation zone by direct visualization of the physical changes caused by freezing , whether using ct , mri or us [ 9 , 19 ]  . there is no denaturing of protein , as in hyperthermic treatment , in the architecture of supporting tissues , particularly urothelial tissue , which is therefore conserve [ 1 , 9 ]  . the disadvantages consist in pain or paresthesia at the probe insertion site and the potential systemic side effects associated with this use [ 1 , 9 ]  . during microwave ablation , tissue heating is induced by extremely fast realigning dipoles generated by an oscillating electric eld [ 18 ]  . 
water molecules are dipoles with unequal electric charge distribution , they attempt to continuously reorient at the same rate in the microwaves oscillating electric eld [ 14 , 18 ]  . 
therefore , temperatures clearly rise due to water molecules friction beyond 60 ( cid : 3 ) c , sufcient to create irreversible cell damage , as demonstrated by sommer et al . 
 [ 22 ] in porcine kidneys . the benets expected from microwave ablation compromise a more rapid and homogeneous ablation , lower sensitivity to local variation in tissue physical properties ( electrical and thermal conductivity ) , less inuenced by heat sink effects of blood circulation as demonstrated by sommer et al . 
studies conducted in rabbits that previously had tumor implantation show that percutaneous microwave ablation can achieve results similar to those of open nephrectomy having thus the potential of being a nephron salvaging treatment for small renal tumors [ 23 ]  . 
however , microwaves have some limitations in particular in relation to the design of the antenna that does not allow a complete control of the lesion during the ablation with an oval shape of coagulation [ 24 , 25 ]  . microwave ablation in kidney : clinical studies in the literature , it is possible to nd clinical studies on mwa for the treatment of rcc in humans since the last decade . 
first in japan , mw technology has been applied to partial nephrectomy to reduce intraoperative bleeding : in this study , a mw tissue coagulator is used not for tumor ablation but is applied peripherally in the healthy parenchyma surrounding the cancer with circumferential punctures producing coagulation of a conical - shaped portion of tissue [ 26 ]  . 
the intent of the study was to test the performance characteristics and safety of a microwave ablation system in the management of renal lesions , so were not placed limitations on the size of the renal lesion to treat [ 27 ]  . 
the results of this phase 1 study 536 radiol med ( 2014 ) 119 : 533540 show that microwave thermal energy can be used to generate reproducible large ablative lesions in 10 - min treatment in solid rcc [ 27 ]  . 
also it was demonstrated , unlike radiofrequency ablation , that microwave ablation can be performed with multiple probes simultaneously , up to three probes , allowing an easily management of large tumors [ 27 ]  . 
histochemical examinations revealed no cell death beyond the ablation area : this is particularly important in renal ablation to preserve healthy parenchyma and , above all , vascular and caliceal structures [ 28 ]  . 
 [ 23 ] published another phase i study with the aim to determine the tolerability of the amica - probe in vivo in patients with solid renal masses and the effects of heating on renal tumors and normal renal parenchyma . 
the results of these studies described have been summarized in table 1 . percutaneous mwa of renal tumors : clinical series after clinical phase i studies , since the last years were published some works about personal experience in vivo for the treatment of small rcc with mwa . 
technical success rate was 100 % , in all cases the antenna was correctly placed in the lesion ; clinical effectiveness was 100 % , no patient showed a recurrence on imaging at follow - up ( table 2 ) [ 30 ]  . 
 [ 31 ] published in 2011 a retrospectively review intermediateterm clinical outcomes after microwave ablation ( mwa ) of renal cell carcinoma ( rcc ) demonstrating , according to carraello et al . 
a very high technical effectiveness ( 98 % ) , with a cancer - specic survival rate of 100 % at 1and 2 - year and of 97.8 % at 3 - year follow - up ( table 2 )  . therefore , the study conrms the safety and efcacy of mwa [ 31 ]  . 
however , open partial nephrectomy ( opn ) and laparoscopic partial nephrectomy ( lpn ) are technically challenging and they may have serious complications , such as excessive blood loss and urinary stula [ 13 ]  . 
in a recent retrospective study was also compared mwa to open radial nephrectomy ( orn ) in the treatment of rcc : although the overall survival after mwa was lower than that after orn ( p = 0.002 ) , rcc - related survival was comparable to orn ( p = 0.78 ) [ 34 ]  . 
estimated 5 - year overall survival rates were 67.3 % after mwa and 97.8 % after orn ; for rcc - related survival , estimated 5 - year rates were 97.1 % after mwa and 97.8 % after orn [ 34 ]  . 
bosniak iii or iv cystic lesions may carry a particular risk for malignancy even if some of these lesions ( particularly bosniak iii lesions ) are proven to be benign after biopsy or surgery [ 35 ]  . 
 [ 35 ] treated seven cystic renal lesions with a total applied energy of 45 w for an ablation time of 10 min and reported a technical success , 538 radiol med ( 2014 ) 119 : 533540 dened as the correct positioning of the antenna into the lesion , of 100 % ; a technical effectiveness , as the absence thermo - ablative residues on cect performed at 1 month after mwa treatment , of 100 % ; and no major complications were recorded . 
this preliminary experience shows a potential role of us / ct - guided percutaneous mwa in treating bosniak category iii or iv cystic renal lesions , as a safe approach to treat selected patients unsuitable for surgery [ 35 ]  . as the most common benign renal mesenchymal neoplasm , renal angiomyolipoma ( aml ) originates from perivascular epithelioid cells and contain a variable proportion of adipose tissue , smooth muscle , and blood vessels [ 37 ]  . 
in 19 lesions treated they found a technical effectiveness of 78.9 % with no aml recurrence observed during the follow - up ( median , 10 months ) [ 37 ]  . complications were recorded in 14.2 % of patients : a stula of the descending colon in one patient was observed , and local infection around the ablation zone was found in another patient [ 37 ]  . 
in conclusion , mwa can provide an effective treatment also for aml with an acceptable percentage of complications [ 37 ] ( table 3 )  . new development trends in mwa to obtain an ablation as complete as possible , it is necessary to improve the ablation technique and also rening imaging guidance . 
imaging guidance improvement currently relies on the use of cone beam ct ( cbct ) which , thanks to a at panel detector and a c - arm gantry , allows to a pathway guidance , to a prediction of ablation area , an immediate imaging control and an evaluation of ablation area , allowing an immediate complication of problem solving . mwa has some technical limitations , which cause disadvantages such as wavelength elongation and unpredictable shape and size of ablation area . 
1 82 - year - old man with left kidney rcc ; a enhanced ct image of renal lesion ; b us image shows the antenna inside the renal lesion ( white arrow ) ; c photo of percutaneous mw antenna placement in left ank ; d follow - up enhanced ct image shows a complete ablation of the left renal lesion with no contrast enhanced of ablated area limitations . 
thermospheretm technology ( covidien ) with its new probes , provides three kinds of spatial energy control thermal , eld and wavelength , holding a predictable spherical ablation zones throughout procedures . 
by employing this system could overcome the uncertain clinical outcomes of other ablative technologies , giving an increased freedom and condence to plan and execute with predictable outcomes in every procedure . 
from this derives the idea that the ablation mw area will be all the more spherical it will be possible to completely ablate the renal lesion . conclusion ablative techniques have been introduced with the aim to control the spreading of a local tumor and to preserve the surrounding parenchymas function , with curative or local control as the primary objectives , when surgery is not feasible [ 79 , 11 , 13 ]  . 
different ablation techniques such as cryoablation , or microwave radiofrequency ablation , ablation have been available for some time , resulting in few complications , most of which are self - limited or readily treated , with great advantages if compared with surgical management [ 1 , 9 ]  . 
this technology can be applied in selected patients who are not candidates for surgery , as an alternative to other ablative techniques [ 11 , 2931 ]  . though mwa achieved comparable results to those obtained with rf ablation or cryoablation , mwa needs a relatively short ablation time and may be more suitable for patients with a variety of comorbidities who cannot tolerate long - time anesthesia [ 31 ]  . 
mwa is a technology that can reliably and reproducibly produce a large ablative lesion of solid renal neoplasms with a uniform tissue necrosis without skip areas [ 27 ]  . 
these recommendations are based on a comprehensive analysis of the current literature , the results of multicenter studies , and expert consensus . keywords thyroid ( cid : 2 ) us ( cid : 2 ) ceus ( cid : 2 ) radiofrequency ( cid : 2 ) ablation ( cid : 2 ) thyroid nodules ( cid : 2 ) thyroid recurrent cancers ( cid : 2 ) intervention radiology introduction thyroid nodules are very common in the adult population with a prevalence of 2076 % [ 1 ]  . 
although most thyroid nodules are benign and do not require treatment , some for associated benign nodules may require treatment symptoms and / or because of cosmetic problems [ 2 , 3 ]  . 
as curative surgery has several drawbacks and the efcacy of thyroid hormone - suppressive therapy has not yet been determined , nonsurgical , minimally invasive treatment modalities , such as ethanol ablation ( ea ) , percutaneous laser ablation , and radiofrequency ( rf ) ablation , have been used to treat thyroid nodules [ 27 ]  . thermal ablation using radiofrequency is a new , minimally invasive modality that may be an alternative to surgery in selected patients with benign thyroid nodules and recurrent thyroid cancers [ 8 ]  . this paper provides information regarding the basic principles , indications , devices , and techniques that have been especially designed to optimize thyroid rf ablation , as well as the clinical results and complications . principles of radiofrequency ablation ( rfa ) rf ablation uses the heat generated from high - frequency alternating electric current oscillating between 200 and 1 , 200 khz [ 2 , 9 ]  . 
although this heat creates immediate damage to tumor tissue , the damage is signicant only in regions very close to ( thus , within a few mm of ) the electrode . 
in addition , ea is a simple and less expensive procedure [ 20 ]  . according to the different clinical problems , it is possible to divide the patients in three group [ 10 , 1517 , 23 , 25 ]  . group 1 symptomatic patients : symptoms as neck pain , dysphasia , foreign body sensation , discomfort , and cough should be directly self - measured by patient using a visual analogue scale from a grade of 0 to a grade of 10 [ 18 , 19 , 35 ]  . group 2 cosmetic problems : a score , based on cosmetic impact of the nodules presence , can be measured by a physician in four grades : grade 1 , no palpable mass ; grade 2 , palpable mass ; grade 3 , a cosmetic problem on swallowing only ; and grade 4 , a readily detected cosmetic problem [ 14 , 16 , 1820 , 35 ]  . group 3 thyrotoxicosis problems : patients with aftn causing problems related to thyrotoxicosis [ 14 , 16 , 17 , 23 , 3640 ]  . recurrent thyroid cancers surgery is the standard treatment for recurrent thyroid cancers as lymph nodes in operation bed , followed by radioactive iodine and thyroid hormone therapy . 
rf ablation , however , can be used in patients with a high - surgical risk and / or in patients who refuse surgery [ 21 , 23 , 26 , 27 ]  . pre - procedural evaluation at least two separate us - guided ne needle aspirations and / or core needle biopsies are necessary to conrm the benign nature of a nodule , and caution should be taken when performing rf ablation of nodules with malignant us features even when there are benign results seen on ne needle aspiration or core needle biopsy [ 12 , 4246 ]  . laboratory tests usually include a complete blood count , a blood coagulation battery , and measurements of thyrotrophin , thyroid autoantibodies , and calcitonin [ 2 ]  . thyroid hormones , if any serum concentrations are abnormal , rf ablation should be performed only after the correction of these abnormal values [ 8 ]  . us examination is important for characterizing and evaluating the surrounding anatomical structures [ 47 ]  . 
in fact with us should be evaluated many characteristics of the nodule : size , shape , margin , proportion of solid / cystic components , echogenicity , calcication , internal , and extracapsular vascularity [ 47 ]  . size could be well dened taking the three orthogonal nodule diameters , including the largest diameter , and the nodule volume could be calculated using the equation : v = pabc / 6 , where v is the volume , a is the maximum diameter , and b and c are the other two perpendicular diameters [ 2 ]  . scintigraphy with 99mtc pertechnetate can be used to differentiate cold nodules from aftns , particularly in with a decreased serum concentration of thyrotrophin [ 2 ]  . prior to the treatment of recurrent thyroid cancers , tumor recurrence should be conrmed by positive us - guided ne 514 radiol med ( 2014 ) 119 : 512520 needle aspiration cytology and measurements of washout thyroglobulin concentration [ 8 ]  . 
a neck ct may be used when appropriate for the evaluation of a recurrent tumor prior to rf ablation [ 8 ]  . patient preparation the patient , during the procedure , should be supine with neck slightly extended [ 48 ]  . to prevent an infection or abscess , the puncture site should be sterilized before rf ablation and prophylactic antibiotics can be used [ 8 ]  . 
local anesthesia could be achieved with an underneath injection of the skin near the cervical - surrounding soft tissue and thyroid capsule with lidocaine or xilocaine [ 16 , 17 , 26 ]  . 
painkillers and sedatives can relieve pain during the ablation but these drugs are not recommended during the ablation because the early detection of complications is impossible in patients under deep sedation , which disturbs communication [ 8 ]  . 
physicians should monitor blood pressure , pulse rate and the voice of each patient by regular conversations during the procedure . if a voice change is suspected during the ablation , the physician should stop the procedure immediately [ 4 ]  . 
an application of an ice bag during the ablation may prevent skin burns at the electrode puncture site . currently , there are above all two types of rf techniques for thyroid nodules [ 4 ]  . the rst technique is called the xed ablation technique , it can be performed using a multitined expandable electrode [ 14 , 16 , 49 ]  . 
in xed ablation , under us guidance , rst lidocaine should be injected into supercial cervical tissue and on the thyroid gland ; then the electrode , always under us guidance , is guardedly inserted along the greatest diameter of the nodule avoiding injury to vital structures [ 14 , 16 , 49 ]  . 
each hook is recommended to be 10 mm away from thyroid capsule , 56 mm from pseudocapsule of the outer edge of nodule , and 15 mm from heat - sensitive cervical structures [ 14 ]  . the correct position of electrode tips and hooks is dened by us exawith xed ablation technique , a spherical ablative zone is usually achieved [ 14 , 16 , 49 ]  . after the ablation , the hooks are retracted and the electrode is slowly withdrawn after the rf energy has been switched off [ 14 , 16 , 49 ]  . the second rf ablative technique is called the moving shot technique , rst described by baek et al . 
a shorter and smaller electrode allows a better control and variation of ablation option in particularly for the treatment of small nodule and / or closed to vital structure closed thyroid nodule . 
in the moving shot technique , the target thyroid nodule is divided into multiple small conceptual ablation units and during the procedure , each conceptual unit is being ablated by the moving ablation electrode tip [ 10 , 22 ]  . 
it is important to preserve from the ablation the danger triangle : the region close to the trachea - esophageal groove to avoid injury to the recurrent laryngeal nerve , trachea , and esophagus . ultrasound monitoring during the ablation is also important to detect hemorrhage [ 3 , 10 , 51 ]  . 
hematomas usually disappear completely within 2 weeks [ 3 , 10 ]  . follow - up patient condition should be monitored after the procedure [ 3 , 10 ]  . 
we recommend that patients be followed up at 12 , 6 and 12 months after rf ablation , as well as every 612 months thereafter , depending on the status of the treated nodules [ 3 , 10 , 18 , 22 ]  . 
additional treatments may be indicated in patients with unresolved clinical symptoms or with a viable growing portion of the nodule detected on imaging [ 3 , 4 , 10 ]  . radiol med ( 2014 ) 119 : 512520 516 clinical results benign nodules rfa therapy has mainly been aimed at decreasing pressure improving the cosmetic results as well as symptoms , resolving thyrotoxic status in hot nodules . 
 [ 11 , 14 , 16 , 1820 , 33 , 34 , 49 , 5254 ]  . three studies were one - armed observational studies utilizing rfa alone [ 14 , 16 , 53 ]  . two studies were one - armed observational studies investigating rfa before and / or after percutaneous ethanol injection ( pei ) [ 19 , 34 ]  . 
one study was a randomized prospective trial comparing the effectiveness of one rfa treatment to two rf ablation treatments [ 20 ]  . the efcacy of rf ablation of cold nodules has been evaluated in terms of reduction of nodule volume , symptoms and cosmetic problems improvement . 
in this study , 20 patients were assigned to the rf ablation group while the other 20 patients to the control group ( conservative treatment ) [ 49 ]  . after 12 months , patients of the rf ablation group had a signicantly decreased mean nodule size ( 13.31.8 ml , p \ 0.001 ) while , in the control group , the mean nodule size was nearly static ( 11.211.8 ml , p [ 0.05 ) [ 49 ]  . 
regrowth of more than 50 % was very uncommon ( 5.6 % ) , it depends on the proportion of cystic component within the ablated nodule [ 54 ]  . 
in cystic nodules with \10 % solid component , rf ablation could achieve a reduction [ 90 % at 6 - month after ablation [ 11 , 53 , 55 ]  . 
1 female45 years , at us and ecd imaging , we found a benign - vascularized nodule in the left lobe with a largest diameter of 41.1 mm and required more sessions and was more expensive [ 11 , 55 ]  . 
in fact the treatment of benign cystic thyroid nodules , the mean volume reduction was 96.9 % in pei while it was 93.3 % in rf ablation , thus demonstrating the superiority of pei to rfa [ 55 ]  . 
authors concluded that pei may be used as the rst - line treatment modality for cystic thyroid nodules , which has comparable therapeutic efcacy to , but is less expensive than , rf ablation [ 55 ]  . 
on the other hand , predominant cystic nodule ( 1050 % solid component ) might be suitable for rf ablation as 6.121 % failure rates in pei were reported for this type of nodules [ 34 , 40 , 56 ]  . rf ablation is generally good for the treatment of the solid component of these refractory nodules [ 19 , 34 ]  . 
in a solid nodule with a predominantly solid component [ 50 % , rf ablation could achieve a 2337 % volume reduction at the 1st month and 5177 % volume reduction at the 6th month [ 22 , 49 , 53 ]  . 
2 female45 years , us image shows during rfa procedure the straight internally cooled electrode contrast - enhanced us ( ceus ) imaging shows a rich vascularization of the benign nodule in the left lobe fig . 
3 female45 years , ( 15 cm length , 17 gauge ) into the benign nodule in the left lobe improved thyroid function reducing the need for antithyroid medication [ 14 , 22 , 49 ]  . 
in a series of 28 patients reported that all patients with pretoxic thyroid nodule and 53 %of patients with toxic thyroid nodule stopped antithyroid medication at 12 - month follow - up after rf ablation . 
therefore , more sessions of rfa are generally needed [ 22 ]  . recurrent thyroid cancers rf ablation can be used for locoregional control of cancer or the treatment of cancer - related symptoms in patients with recurrent thyroid cancer who have a high - surgical risk fig . 
5 female45 years , after a month from rfa , us shows a signicative reduction of the largest diameter ( 33.7 mm ) of the benign nodule of left lobe , compared to fig . 
rf ablation of recurrent thyroid cancers in the neck resulted in a mean volume reduction of 5693 % , with 4258 % of nodules completely disappearing , 64 % of patients experiencing symptom improvement , and serum thyroglobulin concentration decreasing [ 21 , 23 , 26 , 27 ]  . 
however , longterm follow - up data have not been published yet . complications it is necessary to know the broad spectrum of complications of thyroid ra ablation to prevent or minimize complications and sequelae [ 4 , 59 ]  . 
reported complications of thyroid rf ablation include pain , hemorrhage , voice change , skin burn , hypothyroidism , hyperthyroidism , infection and nodule rupture [ 10 , 1416 , 18 , 22 ]  . 
rf ablation does not require general anesthesia , does not induce scarring of the neck , and when performed by 518 radiol med ( 2014 ) 119 : 512520 well - trained physicians , is associated with a low complication rate [ 10 , 1418 ]  . 
during the ablation , most patients could complain of various degrees of pain in the neck and / or radiating to the head , ear , teeth , shoulders , back or chest . 
a voice change is a major complication of rf ablation , caused by the damage of the recurrent laryngeal or vagus nerve ; so , it is necessary to detect vagus nerve before rf ablation [ 60 , 61 ]  . 
to prevent voice change , rf ablation should be performed using the moving shot technique . there is a potential risk of a sympathetic ganglion damage during the extrathyroidal penetration of the electrode if it is not detected during the ablation procedure because it is located posterior to common carotid artery near the thyroid gland [ 8 ]  . 
to avoid this complication , continuous and cautious us - guided tracing of the electrode tip is mandatory during the rf ablation [ 8 ]  . hematomas , resulting from electrode - induced mechanical injury , can occur in the perithyroidal , supcapsular , and intranodular locations [ 59 ]  . 
hematomas can usually be controlled by mild compression of the neck for several minutes , with most hematomas disappearing within 1 or 2 weeks , serious hematomas may compress the airways , close observation is recommended during and after procedure [ 3 ]  . 
hypothyroidism has been reported in patients with nonfunctioning thyroid nodules and those with aftn , thyroid function laboratory analysis are recommended during the following days after rf ablation [ 10 , 15 , 22 , 57 , 62 ]  . 
prophylactic antibiotics and a sterilization of puncture site before rf ablation are recommended to prevent an infection or abscess [ 8 ]  . thyroid nodule rupture after rf ablation may be suspected in patients complaining of sudden neck bulging and pain at the treatment site , us examination usually shows a breakdown of the anterior thyroid capsule and the formation of a new nodule in the anterior neck [ 3 , 59 , 63 ]  . delayed sudden perinodular hemorrhage might be a cause of nodule rupture . 
spontaneous improvement without treatment is possible , but surgery is required when an abscess forms [ 3 , 59 , 63 ]  . skin burns have been reported only at the puncture site , instead the risk of burns at the pad attachment site is relatively low , because rf energy is lower in the thyroid than in the other organ ablation as liver [ 15 , 23 , 59 ]  . 
severe tension , pain , or hypersensitivity to lidocaine could cause nausea and vasovagal reection [ 59 ]  . no life - threatening complications , as injury to trachea and heart attack , have been reported in literature in patients underwent rf ablation of thyroid gland [ 29 , 30 , 33 , 64 , 65 ]  . 
to prevent thermal injury to the esophagus , patients should be asked to swallow cold water during the ablation of a conceptual unit adjacent to the esophagus [ 3 , 29 , 31 , 59 ]  . to prevent life - threatening complications , the operators should strictly trace the electrode tip during the procedure , and should have knowledge of the necks anatomy and experience of an image - guided intervention . conclusions thyroid rf ablation is an effective and safe treatment modality in patients with benign thyroid nodules . 
in this paper , we highlight the technical aspects and clinical applications of cbct imaging and navigation in the most common loco - regional oncological treatments . interventional oncology ( cid : 2 ) cone - beam keywords computed tomography ( cid : 2 ) imaging guidance ( cid : 2 ) percutaneous treatments ( cid : 2 ) embolization ( cid : 2 ) ablation introduction interventional oncology is a growing eld offering new minimally invasive , image - guided treatment options for a variety of primary and metastatic solid tumors . 
imaging is at the core of this approach and selection of the optimal diagnostic and interventional modalities is critical for a safe and effective treatment delivery [ 1 ]  . 
rotondo department of radiology , seconda universita` degli studi , naples , italy 522 radiol med ( 2014 ) 119 : 521532 two - dimensional ( 2d ) angiography is the main imaging technique during embolotherapy . 
ultrasound offers a versatile imaging technology for liver and kidney tumor ablation with real - time imaging . however , tumor and needle or antenna visibility are often suboptimal for deep locations and / or large patients . 
electromagnetic tracking of ablation devices and fusion between real - time ultrasound and preprocedural ct , mri or pet / ct have shown to facilitate targeting of lesions that are sonographically invisible [ 5 ]  . this solution requires dedicated software , hardware and disposables , and does not solve the limitations related to ultrasound for direct thermal ablation monitoring . 
in addition , real time requires ct uoroscopy which is not always available and leads to a signicant increase in radiation exposure to the patient and operator . pet / ct and mri guidance are emerging options for percutaneous tumor ablation , offering real - time imaging , excellent tumor visibility and novel approaches in ablation monitoring [ 7 , 8 ]  . 
however , limited accessibility and increased associated costs have currently limited the use of these modalities and research institutions . to dedicated centers c - arm cone - beam computed tomography ( cbct ) is a new imaging technology that enables acquisition of crosssectional imaging with modern angiographic systems equipped with a at panel detector [ 9 ]  . 
volumetric tomographic images can be combined and co - displayed with conventional 2d angiographic imaging and dedicated software during interventional procedures to plan treatment , navigate / position the catheter or device , monitor the treatment , and assess the nal result or verify margins . 
the motion path includes an acceleration and deceleration phase encompassing a phase of constant speed of 3060 ( cid : 3 ) per second ( s ) and projection acquisition is performed in pulsed mode . 
a complexity for tomographic reconstruction on interventional c - arm systems is the need to accurately measure the true system position , which needs to be taken into account during back - projection . 
for abdominal imaging , typical tube parameters are 510 ms pulses per projection at 120 kv tube voltage including copper ltration with frame rates of 3060 frames per sec . recent detectors cover a planar region of 30 9 40 cm at a high spatial resolution up to 1502 lm2 [ 12 ]  . 
2 schematic representation of a dual - phase cbct acquisition as it is used for tace procedures achieved by adapting the focal spot size , detector readout resolution , and the reconstruction lter . 
satisfactory offset ( off - midline , to include skin entry ) should be taken into account for percutaneous procedures . radiation ceiling - mounted monitors shields should be arranged so that they can be promptly moved and cbct imaging can be performed safely . 
armrest accessories are recommended if available to improve patient comfort during cbct imaging , but should not obstruct rotational movements [ 15 ]  . radiation exposure the x - ray exposure associated to cbct has been the subject of several studies performed on phantoms , animals , patients and the medical team [ 1619 ]  . 
the estimated effective dose to the patient for one cbct scan of the abdomen is approximately 310 msv , generally lower than the comparable abdominal mdct scan ( 1012 msv ) [ 16 , 20 ]  . 
as for all interventional procedures using x - ray exposure , the operators should wear protective devices and leave the examination room when performing 3d scans , and cbct acquisition should be used judiciously . dose therapy planning and navigation software the availability of volumetric datasets showing tumor location , vascular territory and parenchymal environment at the time of the procedure provides an excellent platform to dene a safe and effective route to the lesion and guide device positioning . 
intraarterial therapy planning software ( emboguide , philips healthcare or flight plan for liver , ge healthcare ) is capable to automatically identify the feeding arteries to the targeted lesion ( s )  . 
the basic workow involves the 3d segmentation of the targeted lesion ( s ) on the cbct dataset and the automatic extraction of candidate feeders from a starting point ( normally the micro - catheter tip ) to the targets . 
needle planning software ( xperguide ablation , philips healthcare or innova trackvision , ge healthcare or iguide , siemens healthcare ) provides a simple technique to dene the needle trajectory from the skin entry point to the target . 
the needle paths can be drawn in any direction and multiple paths can be concurrently shown [ 22 ]  . cbct datasets are acquired in a calibrated space where the position of the acquired 3d dataset is known with respect to the x - ray beam generation and the mechanical movements of both c - arm and angiographic table . 
the 3d dataset and the needle or feeding vessel paths follow the rotation and angulation movements of the c - arm , translations of the table , and automatically adjusts to magnication changes . 
the operator can then follow the graphical overlays for device manipulation and / or automatically move the c - arm into pre - dened positions that facilitate catheterization or accurate needle alignment towards the targeted lesion ( s )  . 524 clinical applications cbct and embolotherapy transarterial chemoembolization the use of cbct in the visualization and localization of hepatic lesions at the time of intervention is crucial for effective intra - arterial therapy in seeing and reaching the lesion and in assessing response [ 21 ]  . 
dsa can provide excellent vascular visualization but it has less sensitivity for tumor detection than ct or cbct due to its low softtissue contrast and 2d projection nature [ 15 , 2328 ]  . 
cbct with its 3d nature , soft - tissue contrast , and especially coupled with post - processing software is superior to dsa in lesion detection and tumor feeding vessel identication [ 23 , 3037 ]  . 
dual phase has increased tumor detection versus single - phase cbct alone and is comparable to the gold standard of contrast - enhanced mdct and mri in lesion detection and in predicting therapy response [ 28 , 42 , 43 ]  . with these highlights of cbct in lesion detection , tumor feeding vessel identication , and therapy assessment , the addition of cbct along with dsa can prolong patient survival [ 44 ]  . selective internal radiation therapy selective internal radiation therapy ( sirt ) is a relatively new , catheter - directed treatment modality of both primary [ 45 ] and secondary [ 46 , 47 ] liver tumors . 
in contrast to transarterial chemoembolization ( tace ) , an angiographic work - up is required prior to yttrium - 90 ( y - 90 ) loaded microsphere infusion into the hepatic artery [ 48 ]  . 
angiographic work - up mainly consists in identifying ( and , if indicated , coil - embolizing ) hepatoenteric arteries , originating from the hepatic arteries [ 49 ] ; dening the vascular territory of all targeted hepatic arteries ; and identifying the tumoral lesions within these vascular territories . 
cbct depicts perfused tissue location , which is essential for correct segment classication or pre - treatment portal vein embolization . radiol med ( 2014 ) 119 : 521532 rupture of intratumoral aneurysms . 
cbct has shown potential utility in this procedure to avoid untargeted vessel embolization ( inferior vesical artery or rectal artery with subsequent collateral off - target damage ) and to optimize catheter placement and selective embolization [ 58 ]  . the role of dual - phase cbct with automatic vessel detection software ( emboguide , philips healthcare ) during pae may dene vessels and perfused tissue territory . 
dualphase cbct can be acquired using the following protocol : 24 cc of iodine contrast at 2 cc / s , delay 4 s , considering a single cbct scan duration of 8 s . 
the arterial phase cbct is acquired with a 4 s delay after contrast injection , while the delayed phase cbct is obtained 5 s after the end of the rst cbct scan . 
software - assisted detection of prostatic vessels is feasible and collateral non - target vessels may also be successfully depicted on cbct . cbct and tumor ablation image - guided percutaneous ablation is a minimally invasive , therapeutic option for localized disease . 
note that the lesion depiction on the preand intra - procedural imaging matches with the post - tace imaging , and especially with the hypoenhancement 1 month post - ta renal embolization arterial embolization indications in oncologic kidney therapy are uncommon with the success of partial nephrectomy and percutaneous ablation . 
the main indications are embolization of hypervascular cancers and associated renal vein thrombosis to limit blood loss during renal cell carcinoma ( rcc ) surgery [ 51 ] , or to primarily treat or prevent hemorrhage risk for angiomyolipoma ( aml ) [ 52 ]  . aml is a common benign renal tumor . 
6 ad cbct imaging during y90 work - up in a 60 - year - old patient suffering from chemorefractory colorectal liver metastases clearly shows a small hepatoenteric vessel , feeding the gastric wall : right gastric artery . 
subsequently , proximal coil embolization of the right gastric artery was performed as with embolotherapy , cbct can assist in all steps of thermal ablation ( planning , positioning needles , ablation monitoring , modication of needle plan , post - ablation assessment and verication of completion ) for both thotumors , racic and abdominal tumors . 
for thoracic respiratory gating may minimize motion mis - registration , thus facilitating navigation . indeed , once the patient is positioned on the angiographic table , a pre - procedural cbct is performed to visualize the target lesion and plan the procedure . radiol med ( 2014 ) 119 : 521532 figs . 
ct 1 month after procedure showed complete devascularization of the tumor ( unenhanced ct 9a and enhanced ct 9b ) the operator can segment the lesion and determine the skin entry point as well as the target . 
previous literature concerning cbct - guided lung and bone biopsies demonstrated that unenhanced pre - procedural cbct is sufcient to delineate the lesion and enable segmentation [ 22 , 61 ]  . 
the same could be applied in ablation cases [ 62 ] ; for difcult lung ablations close to vital structures , a contrast enhancement cbct may be needed . most abdominal ablations will also require a contrastenhanced cbct pre - procedurally and post - procedurally . several techniques are possible for contrast injection during cbct scan . in a preliminary study , morimoto et al . 
peripheral intravenous injection is an alternative option which is the method used by the authors during the pre - procedural cbct ( data unpublished ) to provide an optimal visualization of lesion target ( both hepatic and renal tumors ) and adjacent structures , used for ablation planning . moreover , in a preliminary series including 12 hepatic lesions treated with rfa , iwzawa et al . 
 [ 64 ] concluded the efcacy of intravenous contrast - enhanced c - arm ct for assessing ablative areas and safety margins immediately after treatment is nearly equivalent to that of mdct performed 37 day after rfa . contrast - enhanced cbct can be avoided in cases of contrast allergy or renal failure . 
 [ 65 ] , previous diagnostic imaging such as contrast - enhanced ct , pet - ct or mri can be co - registered with unenhanced pre - procedural cbct to plan the procedure and with the post - procedural cbct to assess the completion of the ablation . c - arm cbct intrinsically has also potential disadvantages in terms of contrast resolution , image quality and fov . 
however , the use of co - registration / fusion with diagnostic imaging or enhanced or other phaseenhanced cbct may overcome some of these limitations [ 66 ]  . in addition , the image quality can also be affected by thus , patient setup and support staff motion artifacts ; training are vital to improve image quality [ 67 ]  . radiol med ( 2014 ) 119 : 521532 figs . 
13 ablation planning : mw virtual probe with predicted ablation area ( manufacturer specic ) overlaying to segmented lesion with 5 mm safe margins covered in axial ( 13a ) and progression view visualization ( 13b )  . 
14 intra - procedural cbct : wrong mw probe placement ( 14a , b ) with upper zone of lesion uncovered by the predictable ablation area ( 14b ) ; and subsequent repositioning with all lesion with 5 mm safe margins covered by the predictable ablation area . 
fig. 15 post - procedural cbct , any complication demonstrated 530 conclusion cbct imaging is a new and empowering imaging technology to add to the arsenal of the interventional radiologist / interventional oncologist . 
given the current body of evidence for transarterial chemoembolization and promising future applications such as radioembolization and prostatic arterial embolization , cbct is expected to become a mainstay imaging modality in tumor embolotherapy . 
multimodality navigation , semi - automatic vessel detection , dual - phase cbct , ablation planning , and synergy with ultrasound are early and emerging options , whose added values and potential advantages are in the process of being dened . semi - automatic fusion , certainly , cbct is one of the most interesting and empowering ir / io tools to emerge in recent times . acknowledgments this study supported in part by the intramural research program of the nih and the nih center for interventional oncology ( bjw & naj )  . 
 [ 2 ] found that antero - posterior supine chest radiograph had a sensitivity of only 20.9 % in the detection of pneumothorax if compared with computed tomography ( ct ) , the current gold standard in this setting . thoracic ultrasound ( us ) has proved to be a promising tool [ 3 ] , a bedside technique that can rapidly detect occult pneumothorax , hence avoiding serious potential consequences such as tension pneumothorax , especially in mechanically ventilated patients . 
in patients with major initial , rst - line us examination is generally trauma , radiol med ( 2014 ) 119 : 674680 performed with a fast ( focused assessment with sonography for trauma ) protocol able to depict intraperitoneal collections of free uid that are an indirect sign of solid organ injury and require urgent surgical exploration [ 4 ]  . after the initial fast survey , the us examination may be extended to the thorax to rule out haemothorax and pneumothorax ; when extended to the thorax this examination is known as extended - fast ( e - fast )  . in the trauma setting , the fast examination is usually performed in hypotensive and haemodynamically unstable patients because it helps to determine whether immediate surgery is needed before the patient undergoes a ct evaluation ; in fact , if intra - abdominal bleeding is present , the probability of death increases by about 1 % for every 3 min that elapses before surgical exploration [ 5 ]  . 
in all unstable patients , in addition to the fast acquisition , a right and left longitudinal anterior thoracic view could be quickly obtained to rule out pleural effusion and pneumothorax . 
several authors [ 46 ] have investigated the accuracy of us for the detection of pneumothorax in trauma patients and in those subjected to interventional procedures such as lung biopsy . 
 [ 7 ] who compared the use of antero - posterior chest radiograph with transthoracic us for the diagnosis of pneumothorax , pooled sensitivity and specicity were 88 and 99 % , for us , and 52 and 100 % for chest respectively , radiograph . the aim of this retrospective study was to assess , in our level - 1 trauma centre , the diagnostic accuracy of thoracic us ( e - fast ) in the rapid detection of traumatic pneumothorax in the emergency room in unstable patients with major trauma compared with ct scans and thoracostomy tube placement . the logistic organisation of our level - 1 trauma centre ( emergency room close to the ct room and operating room , staff radiologist present 24 / 24 h and readily available in the emergency room at the arrival of major trauma patients to perform bedside thoracic us ) has allowed us to improve the use of bedside thoracic us in unstable patients . all e - fast examinations were performed by a staff radiologist of our department ( with at least 6 years experience in clinical us and ct ) at the bedside in the emergency room and recorded on videotape . 
because of the need for immobilisation of trauma patients , thoracic us involves scanning only the anterior and lateral wall , not the posterior wall . the presence of pneumothorax is determined on the basis of accepted sonographic criteria ( disappearance of lung sliding and lung pulse , loss of b lines and identication of the lung point )  . 
we dene mild , moderate or massive pneumothorax through the identication ( with lateral scans ) of the lung point on the parasternal line ( mild ) , mid - clavicular line ( moderate ) or anterior / mid / posterior - axillary line ( massive )  . the ct images were interpreted by a staff radiologist without knowledge of the us ndings . 
for every patient , we recorded the time of arrival at the emergency department , the time of e - fast , and the time of multidetector ct ( mdct )  . 
the nal us reports and images were reviewed by all authors in independent reading sessions ( si , vdg , bs , and vm ) and compared with the mdct images for verication ; all images and reports were stored in our ris / pacs system . materials and methods technical equipment study protocol this retrospective case series included 368 consecutive unstable patients admitted to our hospitals emergency department ( a level - 1 trauma centre ) between january 2011 and december 2012 because of a major trauma [ injury severity scale ( iss ) c 15 ]  . 
patients were eligible for inclusion in the study if they had undergone , upon arrival in the emergency department , chest us as part of the e - fast examination before the ct examination , the or ( operating room for damage control ) and before the placement of a thoracostomy tube . 
institutional review board approval was obtained prior to commencement of this study . in our institution e - fast is performed at the bedside , with the patient in the supine position , using a portable us imaging unit ( esaote mylab 75 , italy ) and a 7.5 - mhz linear probe . 
the linear high - frequency probe is suitable for visualisation of the pleural line ; convex probes , working at lower frequencies ( 23.5 mhz ) , are indicated to evaluate the peritoneal cavity , pericardium , and lateral hemithoraces to detect haemothorax . ct is performed with a 16 - channel ct scanning unit ( ct lightspeed 16 , ge medical systems , milwaukee , wis , usa )  . ( visipaque intravenous contrast material 320 mg / ml , ge medical systems , milwaukee , wis , usa ) is always employed for the evaluation of whole - body trauma . 
on the other hand , the visualisation of lung sliding on the anteroinferior chest wall in the supine patient has 100 % negative predictive value in the diagnosis of pneumothorax . another important sign we look for is the presence of b lines , which correspond to thickened interlobular septa in the interstitial syndromes such as pulmonary oedema and lung contusions [ 11 ]  . 
b lines are comet - tail artefacts : they arise from the pleural line , spread up without fading to the edge of the screen and are synchronous with the respiratory movements . 
us detection of the comet - tail artefact allows pneumothorax to be discounted [ 12 ]  . when lung sliding and b lines are absent in the anteroinferior chest area , thus suggesting pneumothorax , the sonologist should check the lateral - inferior chest wall looking for the lung point . 
the lung point conrms the diagnosis of pneumothorax with a specicity of 100 % [ 13 ] and its location provides information about the extent and severity of pneumothorax [ 14 ]  . in some cases , even if lung sliding is absent , sonologist may note the presence of the lung pulse . 
this sign is a vertical movement of the pleural line that is synchronous to the heart beat and it is common in those conditions that cause a consolidated motionless lung ( massive atelectasis and main - stem intubation ) through which the heart movement is transmitted . 
visualisation of lung pulse excludes the diagnosis of pneumothorax because the presence of the air in the pleural space does not allow the cardiac beat to be transmitted [ 8 ]  . 
2. statistical analysis estimates of sensitivity , specicity , positive predictive value , negative predictive value , and overall accuracy were calculated for thoracic us , using mdct as the reference standard for pneumothorax detection in all patients . 
in patients in whom us showed massive pneumothorax and a chest drainage tube was placed before ct , we considered escape or aspiration of intrapleural air at the time of drainage in the emergency room ( as documented in the clinical record ) to be the criterion suggestive of pneumothorax . 
1 thoracic ultrasound : echogenic pleural line ( white arrow ) ; on top , of us ( parasternalline / anterioraxillarline / posterioraxillarline ) scans lines sonographic semeiology in a trauma setting , us evaluation for pneumothorax begins from the antero - inferior chest wall before moving to the lateral chest . 
the pleural line represents either the parietal and visceral layers of the pleura in the normal subject and only the parietal pleura in cases of pneumothorax . the basic sign that indicates normality is the presence of lung sliding , that is , a twinkling movement visible at the pleural line corresponding to the visceral pleura adhering to the parietal pleura . 
when pneumothorax occurs , the air between the two pleural layers causes abolition of the lung line appears motionless . sliding so that according to previous studies [ 810 ] , the abolition of lung sliding does not necessarily conrm pneumothorax because other common conditions occurring in the critically ill the pleural radiol med ( 2014 ) 119 : 674680 fig . 
3 thoracic ultrasound , extended - focused assessment with sonography for trauma ( e - fast ) : mild left pneumothorax in a stabbed pregnant patient ( 24 years old ) ; absent lung sliding and b lines admitted to our emergency department . 
among these , 368 ( 273 men and 95 women ; average age , 25 years ; range , 1668 years ) haemodynamically unstable major trauma patients underwent e - fast upon arrival in the emergency room ( during the primary survey , 010 min after the patients arrival ) for the detection of pneumothorax , haemothorax and haemoperitoneuextended - fast examination , followed by mdct , was performed in all patients . 
these 368 patients , for a total of 736 hemithoraces , represent our study population . the time interval between us and mdct ranged 1075 min , depending on clinical condition on arrival and the need for immediate measures for patient survival . among the 736 lungs in the 368 patients , chest us detected 67 pneumothoraces , while 87 pneumothoraces were either detected by mdct or diagnosed based on the presence of air ush during thoracic decompression in the 678 radiol med ( 2014 ) 119 : 674680 table 1 extended ( to thorax ) values : preliminay results of emergency radiologist parameter thoracic ultrasound sensitivity ( % ) sensitivity during 2011 sensitivity during 2012 specicity ( % ) false positive rate ( % ) false negative rate ( % ) 77 ( 67 / 87 ) 74.5 % ( 38 / 51 ) 80.5 % ( 29 / 36 ) 99.8 ( 668 / 669 ) 0.13 ( 1 / 736 ) 2.7 ( 20 / 736 ) positive predictive value ( % ) 98.5 ( 67 / 68 ) negative predictive value ( % ) 97 ( 668 / 688 ) accuracy ( % ) prevalence ( % ) data pneumothoraces = 87 parentheses 97.2 ( 67 ? 668 / 67 ? 668 ? 1 ? 20 ) 11.8 ( 87 / 736 ) numbers hemithoraces = 736 / emergency room ( 5 / 87 )  . 
us missed 20 / 87 cases of pneumothorax ; 17 of immediately life them were not threatening as they had a thickness less than 5 mm on ct . there was one false positive result in the diagnosis of pneumothorax by us : this was misdiagnosed in the apical region of the left lung in an emphysematous patient . dening the learning curve for thoracic us , all of the false negatives and the single false positive result occurred during the rst ve e - fast examinations performed by each of the staff radiologists ; 13 / 20 false negatives occurred during the rst year ( 2011 ) , and 7 / 20 during the second year ( 2012 ) of our experience . 
therefore , the sensitivity of e - fast for pneumothorax detection was 74.5 % during 2011 but 80.5 % during 2012 ( 668 true negative , negative predictive value 97 % )  . 
in the rst 2 years of experience with chest us in our level - 1 trauma centre ( 2011 - 2012 ) , the overall diagnostic accuracy of this diagnostic tool for the diagnosis of pneumothorax in major trauma in the emergency room was 97.2 % ( table 1 )  . discussion although mdct has been considered the imaging modality of choice in patients with major trauma since the late 1990s , it is often used in conjunction with us for the urgent assessment of patients who have sustained major trauma , particularly in europe . pneumothorax occurs in a large proportion of blunt thoracic traumas [ 1 ] and , even when mild , its detection carries a great clinical relevance because it may quickly progress to cause haemodynamic instability as a consequence of invasive ventilation . 
on the contrary , several studies have demonstrated that lung us has high sensitivity in diagnosing pneumothorax and that the location of the lung point in the supine patient allows evaluation of the extension of pneumothorax . we have investigated , at our level - 1 trauma centre , the use of thoracic us to rapidly detect pneumothorax during the initial resuscitation of unstable patients in the emerthere are limited gency rooin this setting , diagnostic options and even large pneumothoraces could be missed by either clinical examination or antero - posterior chest radiograph ; every us diagnosis was compared with mdct . in fact , in the emergency department of our hospital , critically injured patients are resuscitated by a trauma team guided by a team leader . 
patients suspected of having pneumothorax on physical examination undergo immediate tube or needle thoracostomy without awaiting imaging studies [ 16 ] ; those patients were excluded from the present study . 
patients not requiring immediate invasive intervention undergo a bedside us examination ( e - fast encompassing standard fast and extended thoracic examination ) performed immediately after the physical examination by a staff radiologist ( operational 24 h / day )  . 
although our overall sensitivity was 77 % , if we analyse the 2 years separately , sensitivity was 74 % during 2011 and 80.5 % during 2012 ( a good result for an initial experience with a new method )  . 
in addition , e - fast is performed in only a few minutes , during the primary survey in the emergency room , and this is obviously a important factor to be taken into account compared with other chest us studies , not performed in the same complex conditions . than that of supine chest there was only one false positive result in the diagnosis of pneumothorax by chest us : this was misdiagnosed in the apical region of left lung in an emphysematous patient . subcutaneous in our study , no cases of signicant radiol med ( 2014 ) 119 : 674680 emphysema caused false determination of the presence of pneumothorax . 
in our series , us missed 20 / 87 cases of pneumothorax : 13 / 20 of which were during the rst year ( maybe due to less specic experience ) ; 17 of them were not immediately life - threatening as they had a thickness less than 5 mm on ct ; 3 / 20 moderate pneumothoraces were missed in large habitus patients . 
pneumothorax was bilateral in nine of our cases , but this fact did not affect the sensitivity of the e - fast examination . some limitations to our study should be acknowledged . first , it was a retrospective study , so the us examinations were performed by different operators , with different levels of skill . 
all of the staff radiologists were at their rst experience with thoracic us ( though well - experienced in clinical us ) ; nevertheless the diagnostic performance of e - fast was high . 
a second limitation is that , because this was a retrospective study , we were unable to evaluate the accuracy of us in predicting the extension of pneumothorax in comparison with mdct . 
even if there is no strict correlation between extension on the chest wall and the volume of intrapleural air , the extension of pneumothorax allows semiquantication of the volume , accurately discriminating between large and mild forms . 
during these rst 2 years of experience at our level - 1 trauma centre , we found that examining the chest with us can allow fast recognition ( during the rst 10 min of the golden hour ) of the presence of pneumothorax with very good sensitivity and specicity , either in patients who undergo mdct after us or who need immediate surgical exploration . 
in all cases , the team leader is informed about the presence of pneumothorax and the subsequent need to insert a chest drainage tube if he decides not to insert it immediately in the emergency room . third , with regard to the value of the lung pulse , the sonographic diagnostic algorithm for pneumothorax detection is well codied ; in all reports the lung pulse is the last criterion to be considered because in most cases lung sliding ? b lines ? lung point are sufcient to establish a condent diagnosis . 
in our study , only one patient had left - sided complete absence of lung sliding ? b lines ? lung point but the presence of lung pulse , due to right main - stem intubation with complete left atelectasis . 
we do not have sufcient data to discuss the impact of this sign . conclusions according to our results , bedside thoracic us is a fast and helpful tool with very good accuracy in the workup of unstable major trauma patients , allowing a rapid and highly accurate diagnosis of pneumothorax . 
us does not require sophisticated equipment and it is readily available in the emergency department . in our emergency department , thoracic us is always used during the fast examination in haemodynamically unstable patients , in who time sparing is crucial to allow an immediate treatment . 
we believe that thoracic us , allowing a fast and accurate diagnosis of pneumothorax , is an effective tool during the golden hour , and affects patient survival after a major trauma . 
a protocol limited to the antero - lateral chest wall is sufcient to denitely rule out pneumothorax because , in our series , ct analysis ( with patients in the supine position ) of occult pneumothorax showed that the anterior area was involved in almost all cases . 
the aim of this study was to evaluate correlations between cte ndings with cd activity . materials and methods the cte datasets from 62 retrospectively reviewed for different patients were parameters : bowel wall thickening and hyperenhancement , mesenteric alterations , abdominal free uid and complications related to the disease ( stulas , strictures , abscesses )  . 
activity was assessed using the crohns disease activity index ( cdai ) and some biochemical markers ( creactive protein , erythrocyte sedimentation rate , alpha 2 - globulins , brinogen , platelets , haemoglobin )  . 
in the past , this evaluation was based on clinical indexes , mainly the crohns disease activity index ( cdai ) , integrated by laboratory parameters including c - reactive protein ( crp ) , erythrocyte sedimentation rate ( esr ) , and orosomucoids , and endoscopic ndings [ 2 , 3 ]  . 
indeed , endoscopy can assess only mucosal in a transmural disease like cd , inammation , which , might not be enough [ 4 ]  . recently , a few papers have suggested the role of radiological techniques such as computed tomography enteroclysis or enterography ( cte ) and magnetic resonance enteroclysis or enterography ( mre ) not only in detecting extramural complications but also in the evaluation of disease activity [ 59 ]  . the cte nding of either enteric signs such as mural stratication and hyperenhancement or perienteric signs like mesenteric hypertrophy or engorged vasa recta , the socalled comb sign , has been found to correlate either with radiol med ( 2014 ) 119 : 658666 table 1 demographic , clinical and laboratory features of 62 consecutive crohns disease patients endoscopic or histological inammation or with acutephase proteins , with sometimes discrepant results [ 6 , 7 , 10 12 ]  . 
the importance of recognising the different patterns of disease , especially early in the disease course , may help in tailoring specic therapies , predicting future complicatiming of surgical tions , and possibly offering better interventions [ 13 ]  . 
a good classication of the patient is of primary importance , and sometimes a clinical suspicion is not conrmed on more invasive investigation [ 14 ]  . in this context , cte today appears as a valid technique for the detection of disease complications , and thus a valid alternative for disease staging . 
it seems to be a very powerful technique which can be performed quickly in most radiological departments , even though some concerns have been raised regarding radiation exposure [ 15 , 16 ]  . 
in this respect , correlating cd clinical activity with the cte ndings could help to select patients to be referred for cte , reducing unnecessary radiation exposure [ 9 ]  . however , the relationships between the cte ndings of bowel inammatory activity , and clinical and serum biochemical markers of inammation have not yet been thoroughly investigated . 
the aim of this study was to correlate the cte ndings with cd clinical activity , assessed by cdai , and biochemical activity , assessed by a comprehensive panel of markers including esr , crp , alpha 2 - globulins , brinogen , platelets and haemoglobin . materials and methods patients we retrospectively reviewed all the clinical records of cd patients followed up in our inammatory bowel disease clinic ( a tertiary referral centre for gastroenterological disease ) , between september 2008 and september 2011 . patients were included if they had a denite diagnosis of small bowel cd based on clinical , endoscopic and histological ndings [ 17 ] and had been subjected to cte , ordered as part of routine clinical workup by experienced gastroenterologists for suspicion of strictures or abscesses . exclusion criteria , routinely applied at our department for this type of studies , were age younger than 18 years , renal insufciency ( serum creatinine [ 2 mg / dl ) , pregnancy , intestinal obstruction and documented allergic reaction to iodinated contrast material . 
the study population consisted of 62 patients ( 33 male ; median age 40 years ; range 2066 years ; median duration of disease 52 months ; range 1468 months ) with cd . 
clinical activity was assessed using the cdai . biochemical activity was evaluated with clinical data and biochemical data , obtained within 2 weeks before cte ( esr , crp , complete blood count , serum alpha 2 - globulins and brinogen )  . 
all patients enrolled were 660 radiol med ( 2014 ) 119 : 658666 table 2 computed tomography enterography features of 62 consecutive crohns disease patients cd ( n = 62 ) asked to sign an informed consent form for the processing of their personal data in accordance with the law , and each patient had also read an informative report about tutelage of the personal data , in accordance with the same law . 
statistical analyses were done after removing personal data . cte technique prior to the examination , all patients underwent an intestinal preparation according to the following plan : a diet free of fruit and vegetables for at least 3 days before the examination ; a semiliquid diet and 2 l of water and macrogol 4 , 000 solution ( selg - esse 1000 , promefarm , milan , italy ) the day before the examination . 
to minimise potential artefacts due to peristaltic bowel movement , to obtain homogeneous small bowel distension and to reduce abdominal discomfort , all patients underwent intravenous ( iv ) administration of an anticholinergic compound , 20 mg of n - butyl - joscine bromide ( buscopan , boehringer ingelheim , reggello , florence , italy ) 10 min before the ct scan [ 18 ]  . 
all patients were studied with a 64 - slice mdct scanner ( brilliance 64 , philips medical system , cleveland , ohio , usa ) using the following scan parameters : collimation , 64 9 0.625 mm ; gantry rotation time , 420 ms ; slice thickness , 1.5 mm ; slice increment , 0.7 mm , 140 kv , 250 mas . 
the dose reduction method for all reduction software allowed modulation of the mas parameter during the scan using a maximum of 250 mas with a doselength product mean of 730 mgy * cm with a range of 678923 mgy * cm [ 1921 ]  . 
ct images were analysed in random order and were reviewed by two experienced gastrointestinal radiologists , blinded to all endoscopic and clinical data to ensure objective interpretation of image ndings . 
in each patient we assessed site and number of abnormal bowel segments , bowel wall thickening ( bwt ) , mural hyperenhancement , mural stratication and mesenteric alterations ( table 2 )  . 
mural hyperenhancement was dened as segmental enhancement in all or part ( in the case of mural stratication ) of the small bowel wall , greater than in the adjacent small bowel loops . 
mesenteric alterations included bro - fatty proliferation ( known as creeping fat of the mesentery ) , increased fat density , hypervascularity ( consisting of the presence of the comb sign ) and lymph nodes . 
fibro - fatty proliferation refers to radiol med ( 2014 ) 119 : 658666 loops to noninamed bowel fatty deposition along the mesenteric border of bowel it was dened as a focally segments affected by cd ; increased and inhomogeneous uid attenuation in the mesenteric fat [ ? 20 / ? 60 hounseld units ( hu ) ] , compared with the appearance of subcutaneous fat or perien [ 23 ]  . teric fat adjacent increased fat density refers to uid density in the fat surrounding thickened or abnormally enhancing bowel , resulting from inammatory inltration of the perienteric adipose tissue . 
the comb sign refers to hypervascularity of the involved mesentery because of the presence of dilated and tortuous vasa recta that penetrate the bowel wall perpendicular to the bowel lumen , mimicking the appearance of a comb [ 24 ]  . 
each of these mesenteric effects were graded along a three - point scale as not present ( 0 ) , denitely present to a mild - moderate ( 1 ) or a severe ( 2 ) degree . finally , the presence of abdominal free uid and other complications related to the disease ( stulas , strictures , abscesses ) were assessed . 
all the cte features are summarised on table 2 . statistical analysis all continuous variables were described as median and range , while categorical variables were expressed as frequency and percentage . 
the patients were grouped according to the clinical activity of disease : inactive ( cdai \150 ) ; mild activity ( cdai 150220 ) ; moderate activity ( cdai 220450 )  . 
21 % had nonstricturing nonpenetrating disease , 38 % stricturing , 9 % penetrating , 16 % both stricturing and penetrating disease and ten patients ( 16 % ) had perianal involvement . 
computed tomography enterography shows increased fat density with the comb sign ( arrowhead ) and a bowel stricture ( arrow ) in the axial contrast - enhanced images and in an oblique coronal contrastenhanced reconstruction image fig . 
univariate analysis showed that the presence of lymph nodes ( p = 0.009 ) and comb sign ( p = 0.05 ) were signicantly associated with a high platelet count ( table 4 )  . 
cte provides both anatomical and practical advantages : depiction of the entire bowel wall , multiplanar imaging and no obscuration of small bowel loops due to superimposition , and better evaluation of both luminal and extramural manifestations [ 29 ] ; in addition , it is not an technique [ 30 ]  . 
4 male patient , 52 - year old , with moderate crohns disease activity ( cdai 195 )  . axial and coronal contrastenhanced images of computed tomography enterography show an ileocolic stula ( arrow ) and mural hyperenhancement of the small bowel wall ( arrowhead ) mesenteric adipocytes which are supposed to play a major role in the cd inammatory cascade [ 32 ]  . 
compared to the increased fat density is an bro - fatty proliferation , earlier change and is also more specic than bowel wall thickening , which could give false - positive ndings in the presence of underdistended bowel loops . conicting data have appeared in the medical literature concerning the relationship between radiological signs of inammation ( approached by either cte or mre ) and disease activity in cd . 
 [ 33 ] reported a signicant correlation between mr signs of intestinal inammation ( oedema in the perienteric fat , wall thickening , contrast enhancement ) with a biological activity score which included white blood cells , orosomucoid levels and crp in 20 cd patients . 
 [ 8 ] evaluated both mural signs ( parietal thickness , target sign or alternating rings of low and high density in the bowel wall ) and extraenteric inammation . there was a positive correlation between the target sign and bro - fatty proliferation with the cdai and among wall thickness , the comb sign and perienteric stranding with crp . 
when we explored the relationship between the biomarkers and the cte ndings , we found a correlation of alpha 2 - globulins and platelet count with vascular extraluminal ndings ( comb sign )  . 
alpha 2 - globulins are a fraction of serum proteins containing orosomucoids , in particular alpha 1 - acid glycoprotein , which , though less commonly used in clinical practice , had been shown to have a better correlation with cdai than crp [ 38 ]  . 
axial images of computed tomography enterography show an ileocolic stula ( arrow ) and an abscess ( arrowhead ) perspective , cte has the advantage of being less invasive because it does not require intubation or uncomfortable palpation , it only requires getting on and off the table once , and it is generally faster . 
cte adds useful information to the clinical assessment providing denition of extraluminal involvement characterisation . detection ensuring stricture our study shows that a cte nding of increased fat density has a good correlation with the cdai score . although the cdai has been criticised because of its subjectivity and interobserver variability , it remains the most widely used index for evaluating outcome in clinical trials on crohns disease [ 31 ]  . 
there are some discrepancies between our results and those of previous studies , which could be explained by differences in sample size , patient recruitment and referral and heterogeneity of technical approach . 
our case series has the advantage of being totally homogenous since all patients are referred to the radiology department by a single gastroenterology team dedicated to the care of ibd patients and the technical approach was uniforour study conrms the role of cte as a useful tool not only in the diagnostic workup of suspected cd but also in the evaluation of disease activity , which we believe is an integrated process which involves clinical symptoms and signs , serum acute - phase reactants and endoscopic ndings . to our knowledge , few studies in the literature have correlated cdai , biochemical activity and cte signs with attention focused also on nodal involvement and abdominal free uid . 
in conclusion , cte might help to better address and monitor response to therapy , for example , to dene the so - called window of opportunity for biologics , and this aspect deserves further studies since it has not been evaluated in the present study or in the literature . 
6 computed tomography enterography : axial contrast - enhanced images in a 39 - year - old male with active crohns disease ( cdai 256 ) demonstrating increased fat density and comb sign ( arrowhead ) more advanced and extensive cd , could suggest the presence of prolonged active disease . 
the image characteristics included the number of tumours , tumour location and size , tumour margins , the presence of calcication / necrosis / cavity , the presence of perivascular location , the presence of pleural lesions , tumour homogeneity at contrastenhanced ct , tumour enhancement relative to the adjacent muscle and the presence of extrapulmonary lesions . results multiple nodules / masses with irregular margin were shown in all cases , and reticulonodular opacities and ground - glass opacities were found in one case . 
zhou department of oncology , shanghai medical college , fudan university , shanghai 200032 , china nodules / masses were mostly ( 93 % , 166 / 178 ) located in the subpleural region ( \2 cm from the pleura )  . 
on contrast - enhanced ct , ehe showed a mildly heterogeneous hyperdense appearance . conclusions with predilection for subpleural and perivascular typical pulmonary ehe appears as multiple irregular nodules with punctate calcication and pleural indentation . location , keywords lung ( cid : 2 ) epithelioid hemangioendothelioma ( cid : 2 ) computed tomography introduction pulmonary epithelioid haemangioendothelioma ( ehe ) is a rare endothelium - originating tumour of borderline malignancy [ 1 , 2 ]  . 
ehe was rst described as an intravascular bronchioloalveolar tumour ( ivbat ) by dail and liebow in 1975 ; however , the angiogenic nature of ivbat was revealed by later studies showing that ivbat and epithelioid haemangioendothelioma are different manifestation of the same disease [ 1 , 36 ]  . several studies have reported the ct features of pulmonary ehe [ 25 , 713 ] , but most of them are case reports , so the total reported sample size is small and the ct features of pulmonary ehe , therefore , need further study . 
the aim of this retrospective study was to analyse the clinical and ct features of six cases of pulmonary ehe . radiol med ( 2014 ) 119 : 705713 patients materials and methods ct imaging the ct images of six patients with pathologically proved pulmonary ehe were retrospectively reviewed . 
institutional review board permission was obtained to review patient medical records , and patient informed consent was not required . the clinical features of the six cases of pulmonary ehes are shown in table 1 . 
the serum levels of tumour markers ( a - 1 - fetoprotein , carcinoembryonic antigen , ca19 - 9 , ca125 ) were normal . four patients underwent surgical pulmonary lobectomy and two patients underwent ct - guided transthoracic biopsy using an 18 - gauge needle . 
one patient was lost to follow - up immediately after biopsy ; the remaining ve patients were still alive at the time of writing this paper ( 361 , 197 post - operative days )  . in this study noncontrast ct images were available for three patients and contrast - enhanced ct images for three patients . the ct examinations were performed with an mdct scaner ( somaton sensation 40 or 64 , siemens , germany )  . the ct technical parameters were as follows : tube voltage , 120 kvp ; rotation time , 0.5 s ; pitch , 1.4 ( 60 9 0.6 or 40 9 0.6 ) ; reconstruction slice thickness , 5 mm ( kernel , b70f very sharp and b31f medium smooth ? ) ; tube current was adjusted for each subject by using the care dose 4d technique . 
a bolus contrast material ( 300 mg i / ml of iopamidol at 1.5 ml / kg body weight ) was injected intravenously at a rate of 2 ml / s using an automated injector . nonionic a radiologist evaluated the tumours ct features , including ( 1 ) the number of tumours , ( 2 ) tumour location , ( 3 ) tumour size ( maximum axial diameter ) , ( 4 ) tumour margin , ( 5 ) the presence of calcication , ( 6 ) the presence of necrosis and cavity , ( 7 ) perivascular location , ( 8 ) tumour homogeneity on contrast - enhanced ct and tumour enhancement relative to the adjacent muscle ( hypo - , iso - , or hyper attenuating ) , ( 9 ) the presence of pleural lesions table 1 clinical and computed tomography ( ct ) features of pulmonary epithelioid haemangioendothelioma female chest pain multiple subpleural irregular female none multiple subpleural irregular mild female chest pain multiple subpleural irregular female cough multiple male none multiple subpleural subpleural irregular irregular non - contrast ct heterogeneous no image no image homogeneous no image heterogeneous enhanced ct no image heterogeneous and no image heterogeneous and no image heterogeneous and hyperdense hyperdense hyperdense right frontal bone lesion right thyroid mass multiple bone retroperitoneal mediastinal left inguinal mass lesions mass mass female none multiple subpleural irregular age ( years ) symptom multiple / single location maximum axial diameter ( cm ) margin calcication necrosis cavity perivascular location pleural indentation pleural thickening pleural effusion extrapulmonary lesion radiol med ( 2014 ) 119 : 705713 fig . 
chest computed tomography ( ct ) images show multiple irregular subpleural nodules / masses with the pleural indentation sign ( b , c , e ) , perivascular location ( a , c , e ) , as well as punctate calcication in partial nodules / masses ( d , f ) and pleural thickening ( c , d )  . 
the tumour cells were positive for cd34 , factor - viii - related antigen ( i , j ) ( pleural indentation , pleural thickening , pleural effusion ) and ( 10 ) the presence of extrapulmonary lesions . results the ct ndings of the six ehes are described in table 1 . multiple nodules / masses were shown in all cases and reticulonodular opacities and ground - glass opacities were each found in one case . 
chest ct images show multiple irregular subpleural nodules / masses ( ad ) with pleural indentation ( a , c ) , perivascular location ( a , c ) , as well as punctate calcication in partial nodules / masses ( b , d ) , pleuralthickening ( c , d ) and pleural effusion ( ad )  . 
furthermore , the size of the largest nodules / masses was 5.2 cm in diameter ( b ) and the pulmonary epithelioid haemangioendothelioma showed a mild heterogeneous hyperdense appearance relative to muscle on contrast - enhanced ct ( b ) 709 radiol med ( 2014 ) 119 : 705713 fig . 
chest ct images show multiple irregular subpleural nodules / masses ( ad ) , with pleural indentation sign ( a , c ) , perivascular location ( a , c ) , as well as punctate calcication in partial nodules / masses ( d ) and pleural thickening ( c )  . furthermore , the size of the largest nodules / masses was 3.0 cm in diameter ( a , b ) fig . 
however , in our study the average age was 53 years , in contrast to the ndings of previous reports in which most patients were younger than 40 years [ 1 , 6 , 18 ]  . our results showed that all cases had multiple irregular nodules / masses . 
the average number of nodules / masses in each case was 30 ( range 1170 ) , and most nodules / masses ( 90 % , 160 / 178 ) were \1 cm in diameter . 
these ndings are similar to those reported in past studies which report that the most characteristic feature of ehe on ct is the presence of multiple perivascular nodules with welland ill - dened margins in both lungs and nodules up to 2 cm in size , although most are \1 cm in diameter [ 4 , 5 , 8 , 9 , 11 , 12 , 19 ]  . 
chest ct images show ground - glass opacities ( a ) and multiple irregular subpleural nodules / masses ( af ) with pleural indentation sign ( a , c , e ) , perivascular location ( a , c ) and pleural thickening ( c , e )  . 
the size of the largest nodules / masses was 3.5 cm in diameter bronchioles and lymphatic vessels , especially small arteries , lymphatics and venules of 1 mm or less in diameter within or adjacent to the nodules ; less frequently vessels of several millimetres in diameter may be involved [ 1 , 4 , 9 ]  . to our knowledge , pulmonary hamartoma , leiomyoma and metastasis usually show nodule / mass with smooth margins ; wegener granulomatosis usually appears as multiple nodules / masses with cavity ( size from a few millimetres to over 10 cm ) and the number of lesions are often \10 [ 20 23 ] , which is not similar to that of ehe . in our study , pulmonary ehe showed predominant subpleural location , which was conrmed by gross pathology revealing an increased number of lesions in the immediate subpleural area [ 5 , 24 ]  . 
this feature of ehe was different from pneumoconiosis in which the nodules tend to be most numerous in the upper lobe , from metastatic pulmonary nodules which tend to be distributed in the basal portion of the lung , from wegener granulomatosis which has peribronchovascular , subpleural and angiocentric nodules / masses [ 20 , 23 , 25 , 26 ]  . in our study , the pulmonary ehes showed perivascular reecting the gross pathology nding that location , tumours are usually found in relation to small and mediumsized vessels and bronchi . 
additionally light microscopy shows that tumour vascularity is inapparent , only a rare small capillary can be identied in the tumour itself , and the tumour cells are near vessels and adjacent to alveolar septa , which suggest that ehe has metabolic requirements and its nutrient and oxygen supply is by diffusion [ 1 ]  . 
this ct feature is usually not found in pneumoconiosis , metastatic pulmonary nodule , wegener granulomatosis , pulmonary hamartoma , or benign metastasising leiomyoma [ 2023 , 25 , 26 ]  . in our study , 48 % ( 86 / 178 ) of nodules / masses showed punctate calcication in four of six cases , a feature also reported by other studies [ 7 , 9 , 11 , 13 , 24 ]  . 
nodules of pulmonary ehe show an acellular sclerotic central area and the acellular pale pink centres undergo coagulative necrosis , then dystrophic calcication , chondrication , ossication , and rarely positive congo red staining radiol med ( 2014 ) 119 : 705713 fig . 
chest ct images show multiple irregular subpleural nodules / masses ( af ) with pleural indentation sign ( a , e , f ) , perivascular location ( c , e )  . however , the size of the largest nodules / masses was too small ( 1.1 cm in diameter ) to analyse the enhancement of lesion ( a , b ) reactions can be seen in these necrotic central cores [ 1 ]  . punctate calcication can occur in a metastatic sarcoma , but other ct features including smooth margin , tendency to distribute in the basal portion of the lung may be used for the differential diagnosis [ 26 ]  . in our study , pleural indentation was found in all cases . this corresponds histologically to thickened , brotic connective tissue septations with indrawing of the visceral pleura and reects desmoplastic reaction [ 27 ]  . 
alternatively , the tissue processing shrinkage artefact may be attributed to the fact that the tumour extends into each alveolus from just one focus and a moderate amount of brosis [ 1 ]  . 
usually pneumoconiosis , metastasis , wegener granulomatosis , pulmonary hamartoma and leiomyoma do not show pleural indentation [ 2023 , 25 , 26 ] , unlike pulmonary ehe . in our study , ve cases showed pleural thickening , and two cases showed pleural effusion . 
the ct ndings of pleural ehe are nonspecic and usually demonstrate a pleural effusion with localised or diffuse nodular pleural thickening [ 2 ] , which typically affects older men , induces chest pain and dyspnoea and is easily mistaken for pleural infections or malignant mesothelioma [ 3 , 4 , 28 ]  . 
patients with brinous pleuritis and extrapleural proliferation of tumour cells or spindle tumour cells generally have a worse prognosis [ 18 , 29 ]  . due to the small size and non availability of contrastenhanced ct images , the enhancement of ehe could not be analysed . 
two cases in our study showed that ehe had a mild - heterogeneous hyperdense appearance on contrastenhanced ct , similar to that described in a case report 712 radiol med ( 2014 ) 119 : 705713 revealing a left hilar mass mimicking central lung cancer [ 30 ]  . furthermore , some studies have reported atypical ct manifestations of pulmonary ehe which included diffuse reticulonodular opacities and ground - glass opacities [ 4 , 10 ] ; however , these ct features were each found in one case in our study and are attributed to interstitial inltration presenting focally in interlobular septa or pleura and around bronchopulmonary rays [ 1 ]  . additionally , the extremely long and indolent growth of pulmonary ehe needs to be emphasised . 
some authors reported that pulmonary ehe showed little or no growth on serial radiographs [ 4 , 5 , 31 ] and that even partial spontaneous regression [ 32 ] and life expectancy may be up to 30 years [ 4 , 5 , 31 ]  . some authors have reported the antitumour effects of interferon , chemotherapy using carboplatin and etoposide [ 14 , 33 ]  . 
a monoclonal antibody against vascular endothelial growth factor ( vegf ) ( bevacizumab ) together with chemotherapy was recently used for preventing tumour spread in the early period as these tumours express high levels of vegf [ 34 ]  . 
additionally , the uorodeoxyglucose positron emission tomography ( fdg - pet ) scan can provide useful information concerning the malignant potential of each nodule more than 6 mm in diameter . 
fdg - pet may be useful to select the more clinically malignant nodules , which worsen the prognosis [ 31 , 35 ]  . sometimes ehe involves extrapulmonary organs and may be multifocal ; the liver and bone are the most frequently affected organs [ 6 ]  . 
hepatic ehe typically appears as multifocal conuent peripheral nodules with adjacent capsular retraction and a low - signal halo ; additionally hepatic ehe frequently occurs in older children [ 36 , 37 ]  . bone ehe typically shows a lytic lesion without matrix mineralisation , even though osseous expansile remodelling may be seen [ 19 ]  . the present study was limited by a small sample size because pulmonary ehe is rarely encountered . 
fundamental signs ( extraluminal air , solution of continuity ) and secondary signs ( thickening of the mesentery , free or perilesional uid , wall thickening ) were considered . results ct alterations were found in 31 / 35 ( 88.6 % ) patients : extraluminal air ( 30 / 35 , 85.7 % ) , solution of continuity ( 11 / 35 , 31.4 % ) , intra - abdominal uid ( 27 / 35 , 77.1 % ) , thickening of the mesentery ( 20 / 35 , 57.1 % ) , and wall thickening ( 14 / 35 , 40 % )  . 
in 25 / 35 cases ( 71.4 % ) pneumoperitoneum was detected , associated with secondary signs ( 23 / 25 , 82 % ) , conrmed as free perforations at surgery . 
in 5 / 35 patients ( 14.2 % ) , peri - intestinal air bubbles and secondary signs were evident , while in 1 / 35 cases ( 2.8 % ) only secondary signs were seen , namely covered perforations . 
angelelli dim - interdisciplinary department of medicine , section of diagnostic imaging , aldo moro university of bari medical school , piazza giulio cesare 11 , 70124 bari , italy e - mail : marirosacristallo@alice.it conclusion ct investigation is essential in the recognition of a small - bowel perforation and in the denition of its nature . keywords small bowel ( cid : 2 ) free and covered perforation ( cid : 2 ) introduction jejunalileal perforation represents a pathological condition which can be caused by trauma ( blunt or penetrating trauma , foreign body ingestion , iatrogenic injury ) or by nontraumatic inammatory ( enteritis , crohns disease ) , ischaemic ( mesenteric infarction , volvulus , intussusception , vasculitis ) , and neoplastic conditions [ 1 , 2 ]  . 
it is an uncommon condition , as the small bowel is involved in only 515 % of all closed abdominal traumas and the nontraumatic perforations are even more uncommon with a reported incidence of one case / year / 350 , 000 inhabitants [ 3 , 4 ]  . from a clinical point of view , a jejunalileal perforation is characterised by the appearance of an acute abdomen caused by the peritoneal inammatory reaction secondary to the leakage of intestinal content , although in some cases the clinical features may be nonspecic , for example in patients with covered perforation , those receiving treatment with steroid drugs or immunocompromised patients [ 5 , 6 ]  . in the diagnostic management of these patients , a plain radiography in different positions is usually performed as a rst imaging assessment . 
this tool could be decisive for diagnosis , but it is not very sensitive since it is only rarely able to demonstrate the occurrence of pneumoperitoneum because of the small amount of air in the small bowel as compared to other bowel segments . 
it does not allow identication of a possible covered perforation , which 652 radiol med ( 2014 ) 119 : 651657 arises in the small bowel due to the rapid tendency of the omentum , mesentery and adjacent loops to cover the perforated bowel segment [ 7 , 8 ]  . 
in the event of a clinically suspected bowel perforation , not detected on abdominal x - ray , the contribution of computed tomography ( ct ) is crucial ; it has 92 % sensitivity in detecting perforations in the whole gastrointestinal [ 9 , 10 ]  . 
despite the importance of the issue , only few studies regarding jejunal ileal perforations have been reported in the literature , probably due to the limited incidence of this nding . tract the purpose of this study was to evaluate the ct semeiotics of small - bowel free and covered perforations and to evaluate the potential of ct in recognising their aetiology . materials and methods we retrospectively evaluated 35 patients , 19 females ( 54 % ) and 16 males ( 46 % ) , aged between 21 and 90 years , studied between april 2006 and october 2012 , suffering from surgically proven small - bowel perforations . in 10 cases ( 28.5 % ) , perforation was located at the jejunum while in the remaining 25 ( 71.5 % ) at the ileuthe perforation was due to various causes : loop strangulation ( n = 11 ) , hernia ( n = 3 ) , adhesions ( n = 5 ) , volvulus ( n = 3 ) ; traumatic injuries ( n = 6 ) , including three blunt trauma , two knife lesions and rearm lesion ; foreign bodies ( n = 5 ) , represented by three toothpicks , one phytobezoar , and one shbone ; crohns disease ( n = 4 ) ; metastases ( n = 4 ) ; peritoneal carcinomatosis intestinal tuberculosis ( n = 1 ) ; small - bowel diverticulitis ( n = 1 )  . ( n = 3 ) ; the list of patients was obtained from the computerised registry of the operating room using the keyword jejunal ileal perforation . 
the images were acquired during the arterial phase , with a scan delay of 3040 s from contrast medium injection , and in the venous phase after 6070 s . the ct images were transferred to , and analysed on , a workstation ( hp xw8600 ) equipped with dedicated image reconstruction software ( vitrea fx 2.1 , vital images , minneapolis , minnesota , usa )  . 
the duration of the postprocessing was approximately 15 mthe axial and reconstructed images were assessed in consensus by two experienced radiologists in the eld of gastrointestinal imaging , who were aware of the nal diagnosis at the time of the study . 
the images were evaluated with the usual ct windows for the study of the abdomen and with very large windows ( [ 800 / hu ) similar to those used for the study of the lung parenchyma , to facilitate the identication of extraluminal air . to determine the presence of bowel perforation , the following ct parameters were considered : fundamental signs : extraluminal air , assessing quantity ( air bubbles , free air ) [ 1113 ] and distribution ( supramesocolic , infra - mesocolic compartment , pelvis , retroperitoneum ) [ 14 , 15 ] ; solution of continuity of the wall [ 16 ]  . secondary signs : periluminal mesentery streaking ( increase in the density of the mesentery from - 100 to - 160 hu to - 40 to - 60 hu ) [ 8 , 1720 ] ; free uid or perilesional uid [ 8 ] ; wall thickening . 
they were associated with extraluminal air in 28 / 35 patients ( 80 % ) , with free perforation in 23 ( 82 % ) and with covered perforation in 5 ( 18 % ) ; out of 35 cases , they were isolated in 1 ( 2.8% ) , which surgery conrmed to be a covered perforation by a tip of toothpick . 
in four patients it was possible to obtain only partial information on the nature of the injuries ; these were cases of bowel perforation secondary to metastatic disease . in these patients , a neoplastic disease could be suspected by the presence of circumscribed irregular wall thickening , but a differential diagnosis with a primary lesion was not possible . 
it was represented by pneumoperitoneum in 25 / 35 cases ( 71.4 % ) , always easy to identify , with a maximum thickness of about 1 cm and associated , in 18 / 35 cases ( 51.4 % ) , with peri - intestinal air bubbles . 
with regard to the distribution of the pneumoperitoneum , among the 25 / 35 patients ( 71.4 % ) with pneumoperitoneum , the air small - bowel perforations are uncommon and may represent a complication of a number of inammatory ( crohns disease , small - bowel diverticulitis , tuberculosis ) , neoplastic ( primary or secondary ) , ischaemic ( mesenteric infarction , venous obstruction by loop strangulation , vasculitis ) , and systemic ( paralytic ileus ) diseases or can be caused by trauma ( blunt trauma , knife , rearm , iatrogenic ) or foreign bodies [ 6 , 9 , 2325 ]  . 
regardless of the nature of perforations , they can be divided into covered or free perforations ; this differentiation is crucial in the therapeutic approach . free perforations require immediate surgical treatment , which can be delayed in covered forms [ 8 , 26 ]  . in the diagnostic management of these patients , who typically show clinical signs of an acute abdomen , plain radiography of the abdomen in different positions remains 654 radiol med ( 2014 ) 119 : 651657 fig . 
a transverse ct scan ; b coronal reconstruction ; c sagittal reconstruction . presence of numerous diverticula of the small bowel ( a , b arrows ) ; only extraluminal peri - intestinal air ( arrowheads ) and an increase in the mesenteric density are associated ( b , c empty arrows ) fig . 
the shbone is well evident ( curved arrows ) ; small peri - intestinal air bubbles ( arrowheads ) and an increase in the mesenteric density are associated ( empty arrows ) the rst feasible diagnostic tool . 
in the diagnosis of gastrointestinal perforation , as pointed out in the literature , this investigation has important limitations such as a low sensitivity ( 5070 % ) in the detection of small amounts of extraluminal air , and generally the impossibility of dening the location and nature of the perforation [ 13 , 27 , 28 ]  . ct is today the gold standard in the study of patients with acute abdomen and provides a crucial contribution in radiol med ( 2014 ) 119 : 651657 fig . 
in these cases , appropriate indications for the use of ct are : negative x - ray examination with clinical signs strongly indicative of bowel perforation ; patients difcult to explore with plain radiography due to serious clinical condition ; the need to obtain additional information after a poorly diagnostic x - ray examination [ 22 ]  . potential of ct for suspected intestinal perforation has been widely discussed and an overall sensitivity of 92 % has been reported in the detection of this condition [ 11 ] and values of 86 and 37 % , respectively , in dening the site and nature [ 15 , 32 ]  . in the literature , in our study , ct signs of small - bowel perforation were detected overall in 88.6 % ( 31 / 35 ) of patients , whereas the ct examination was negative in only 11.4 % ( 4 / 35 )  . 
in particular , as shown by the results , ct can show pathological changes in 100 % ( 25 / 25 ) of free perforations and in 60 % ( 6 / 10 ) of the covered forms . with regard to ct semeiotics , extraluminal air was detected in 85.7 % of cases ( 30 / 35 ) , secondary alterations in 82.8 % ( 29 / 35 ) and a solution of continuity of the bowel wall in 31.4 % ( 11 / 35 )  . 
extraluminal air was recognised with greater frequency than reported by some authors , who state that it is possible to recognise a pneumoperitoneum in only 33.3 % of cases of small - bowel perforation [ 33 ]  . 
this discrepancy is probably due to technological developments , which now allow for a slice thickness less than 1 mm , able to highlight even small extraluminal air bubbles , as demonstrated in the literature [ 16 ]  . the analysis of the location of the extraluminal air reveals interesting data , namely the fact that pneumoperitoneum associated or not with peri - intestinal air bubbles is always indicative of free perforation , whereas peri - intestinal air alone is always correlated to covered perforations . therefore , these elements allow the differentiation between free and covered perforations and may contribute to the choice of surgical timing . in the case of a free perforation , the distribution of air within the peritoneal compartments is similar to what has already been reported by other authors . 
 [ 15 ] have pointed out that in the lower perforations ( ileum / colon ) , the air is localised in the supraand inframesocolic compartments , while the predominant presence of air in the supramesocolic compartment orientates towards a gastroduodenal perforation . 
in the examined series , which assessed 25 patients affected by free perforation , the air was localised exclusively in the infra - mesocolic compartment in 16 % of cases ( 4 / 25 ) , in the supraand infra - mesocolic compartments in 64 % ( 16 / 25 ) , in the supraand infra - mesocolic compartments and in the pelvis in 20 % ( 5 / 25 ) of patients . 
in no case was air detected exclusively in the supramesocolic space , in the pelvis or in the retroperitoneutherefore , the recognition of air only in such districts can be considered a clue for the exclusion of small - bowel perforation . the recognition of extraluminal air is not only indicative of bowel perforation , being also observed in physiological conditions , more frequently in women ( sport , sex , catamenial ) , pathological conditions ( extension of a pneumo ( paracentesis , thorax ) or after biopsies , peritoneal dialysis , laparoscopy ) and surgery [ 34 ]  . the differential diagnosis of extraluminal air from gastrointestinal perforation or from other causes is usually readily achieved by considering the patients clinical , medical history and the alterations associated with peritoneal and intestinal walls . iatrogenic procedures as reported in the results , the identication of a solution of continuity of the bowel wall is useful to dene the presence and especially the site of perforation , and this was achieved in 31.4 % of the examined patients ( 11 / 35 ) ; it was 656 radiol med ( 2014 ) 119 : 651657 never the only sign . 
in fact , in 90 % of cases ( 10 / 11 ) it was associated with extraluminal air and secondary signs and in 10 % ( 1 / 11 ) of cases with extraluminal air alone . 
this alteration was never highlighted by other authors [ 33 ] in the case of small - bowel perforation , while it was more frequently observed ( 40 % ) in perforations affecting the remaining gastrointestinal tract [ 15 , 16 , 35 ]  . among the signs seen in the examined series , secondary alterations were recognisable in 82 . 
% of patients ( 29 / 35 ) and were associated with extraluminal air in 51.4 % ( 18 / 35 ) , and extraluminal air and solution of continuity in 28.5 % ( 10 / 35 ) ; only in 2.9 % ( 1 / 35 ) did they represent the only nding . 
the analysis of the results suggests that small foreign bodies cannot be identied , and generally correlate with covered perforations ; all other situations can be fully diagnosed if in the presence of characteristic changes , and sometimes only assumed among different diseases with common ct features . this research conrms the potential of ct in the diagnosis of small - bowel perforations . 
however , it has important is a retrospective analysis performed by radiologists who were aware of the surgical ndings at the time of the study . limitations in that conclusion ct remains the gold standard in the study of small - bowel perforations , as it is able to highlight pathological changes in 100 % of free perforations and in 60 % of covered forms . 
the presence of extraluminal air ( free or periintestinal air ) and solutions of continuity in the bowel wall , generally associated with minor alterations ( intra - abdominal uid , mesenteric thickening , bowel wall thickening ) represents essential ndings for diagnosis . 
the latter ones are involved in development of craniofacial and skull base deformities . materials and methods we retrospectively reviewed 27 children with complex synostosis ( n = 21 ) and anterior synostotic plagiocephaly ( n = 6 )  . 
high - resolution ct images with bone denition algorithm and tridimensional volume rendering reconstructions were assessed . results sutures in 27 children we found different involved in the synostotic process , including both major and minor skull suture synostosis , and synostosis of synchondroses . 
superior orbital rim deformity , nasal root deviation , anterior endocranial axis deviation ( ethmoidal axis ) are found in children with coronal arch synostosis , while reduced size of the posterior fossa and chiari 1 malformation are noted in children with lambdoid arch synostosis . conclusions high - resolution ct allows an accurate identication of both major and minor skull base suture synostosis and it represents the gold standard for the r . 
gemelli 8 , 00168 rome , italy diagnosis of craniostenosis and for planning the proper surgical approach . keywords craniosynostosis ( cid : 2 ) coronal arch ( cid : 2 ) minor sutures introduction the deformity of the skull in the newborn represents a common and signicant diagnostic problem , particularly in distinguishing positional plagiocephaly from deformity caused by craniostenosis [ 1 , 2 ]  . positional plagiocephaly is an alteration of the morphology of the skull in the absence of premature cranial suture synostosis caused by a dynamic distortion of the skull secondary to preand / or postnatal external forces without malformative alterations [ 3 , 4 ]  . 
craniostenosis , by contrast , is a pathological condition of skull deformity caused by premature sutural closure of the vault and / or skull base , occasionally associated with early closure of cranial fontanels [ 5 , 6 ]  . 
sutures are brous bands of tissue that connect the bones of the skull , allowing their growth from the inside to the outside during development , whereas the fontanels are membranes covering parts of the skull where the bones have not yet settled , allowing the skull bones to adapt to brain expansion ( functional mobility during the birth and during the rst year of life ) [ 7 ]  . normally , sutures and fontanels ossify ( that is , they form synostoses ) at different times after the birth . 
specically the metopic suture normally ossies between 9 and 11 months , and the other sutures ( sagittal , coronal and lambdoid ) close completely at approximately 3040 years of age . 
the anterior fontanel ( bregmatic fontanel ) typically ossies within the second year of life , the posterior fontanel ( lambdoid fontanel ) radiol med ( 2014 ) 119 : 694704 fig . 
1 sagittal arch a this is composed of the metopic suture ( white arrow in b1 patent suture ; black arrow in b2 synostotic suture ) , the sagittal suture ( white arrows in c1 patent suture ; black arrows in c2 synostotic suture ) and the ethmoido - frontal ( minor sutures ) ( white arrows in d1 patent sutures ; black arrows in d2 ; synostotic sutures )  . 
2 coronal arch a this begins at the bregma and is composed of coronal sutures ( b white arrow patent suture on the right side ; black arrow synostotic suture on the left side ) , each divided into an anterior branch composed of the fronto - sphenoidal ( minor sutures ) ( c white arrow patent suture on the left side ; black arrow synostotic suture on the right side ) and ethmoido - sphenoidal ( minor sutures ) synchondrosis ( black arrow synostotic suture in d1 ; white arrow patent suture in d2 ) , and a posterior branch composed of the spheno - squamous ( minor sutures ) ( e white arrow patent suture on the right side ; black arrow synostotic suture on the left side ) , the spheno - parietal ( minor sutures ) ( f white arrow patent suture on the left side ; black arrow synostotic suture on the right side ) and spheno - petrosal ( minor sutures ) synchondrosis ( g white arrow patent suture on the right side ; black arrow synostotic suture on the left side ) is no longer palpable after the rst 3 months of life , the sphenoid fontanels ( pteric fontanels ) close after the rst year of life , and the mastoid fontanels ( asteric fontanels ) ossify more often within the rst 18 month of life [ 7 , 8 ]  . in craniostenosis , the welding of the skull sutures , which is sometimes associated with premature closure of the fontanels , occurs in the prenatal period , perinatal epoch , or during early infancy [ 1 , 5 ]  . 
3 lambdoid arch a this starts at lambda and it is composed of the lambdoid sutures ( b white arrow patent suture on the left side ; black arrow : synostotic suture and a copper - beaten appearance of the skull on the right side ) , the spheno - occipital ( minor sutures ) synchondrosis ( c white arrow ) and occipito - mastoid ( minor sutures ) ( d white arrow patent suture on the right side ; black arrow synostotic suture on the left side ) pathological and premature sutural closure , progresses over time ; therefore , timely diagnosis and immediate treatment are required . 
the incidence of craniostenosis is 1 in 2 , 1002 , 500 newborns without any ethnic predilection [ 8 ]  . traditionally craniostenosis has been classied according to the sutures involved , the deformity of the head , the presence or absence of a skull - facial syndrome and the degree of progression of the anomaly [ 5 , 8 , 9 ]  . 
therefore , craniostenosis can be classied as simple ( monosutural ) or complex ( multisutural ) or as a primary defect of ossication or secondary to systemic disorders ( endocrine , haematological , metabolic alterations ) or iatrogenic causes . most cases of craniostenosis ( 84 % ) are found as an isolated defect ( non - syndromic craniostenosis ) , although 15 % of cases are part of a syndromic condition ( syndromic craniostenosis ) [ 5 , 8 , 9 ]  . 
non - syndromic craniostenoses occur more commonly with the premature closure of a single or two major sutures , whereas cases of syndromic craniostenosis more frequently involve the fusion of several sutures and are often associated with facial deformities and brain anomalies [ 10 ]  . 
however , important to note that the severity of the cranial deformity does not reect the severity or the extent of the synostotic process ; indeed , skull symmetry can be preserved when multiple sutures are symmetrically fused [ 11 , 12 ]  . since its introduction , computed tomography ( ct ) has emerged as the technique of choice to conrm the clinical diagnosis , to dene the extent of the synostosis and to exclude any associated anomalies and , consequently , to determine a prompt and accurate treatment . therefore , ct with three - dimensional ( 3d ) reconstructions represents the gold standard in the evaluation of skull sutures but is used , for radioprotective reasons , with a low - dose technique and only when it is deemed clinically necessary . 
several studies have reported the high sensitivity ( 96.4 % ) and specicity ( 100 % ) of 3d ct in the identication of the vault sutures involved by the synostotic process , but no study has ever evaluated the accuracy and utility of spiral ct ( low - dose technique ) in identifying the extension of the synostotic process towards the skull base in children with a clinical suspicion of craniosynostosis [ 5 , 9 ]  . radiol med ( 2014 ) 119 : 694704 fig . 
4 parieto - squamosal arch a this is the junction of the coronal and lambdoid arches and it is responsible for the vertical growth of the skull . parieto - squamous ( b white arrow patent suture on the right side ; black arrow synostotic suture on the left side ) and parieto - mastoid ( minor sutures ) ( c white arrow patent suture on the right side ; black arrow synostotic suture on the left side ) are a part of this arch time along the four the lack of ct data in the involvement of the skull base the synostotic sutures contradicts scientic reports that process progresses over sutural arches of the skull [ 1315 ]  . 
the synchondroses normally ossify ( i.e. , they form synostoses ) before or after birth at different times . the intra - sphenoidal synchondrosis ( is ) in particular , ossies before or spheno - ethmoidal synchondrosis ( se ) ossies by the age of 6 years ; and the spheno - occipital ( so ) between the 17th and 20th year . 
the anterior intra - occipital synchondrosis ( io a ) begins to ossify by year 12 and nishes by year 710 , and the posterior intra - occipital synchondrosis ( io p ) begins to close by year 12 and nishes by year 47 . 
anterior intra - occipital synchondroses ( white arrows in a patent synchondroses ) ; posterior intraoccipital synchondroses ( white arrow in b patent synchondrosis ; black arrow in b synostotic synchondrosis ) ; temporo - occipital synchondroses ( white arrows in c patent synchondroses ) ; anterior intra - sphenoidal synchondroses ( white arrow in d1 patent synchondrosis ; black arrow in d2 : synostotic synchondrosis ) ; spheno - ethmoidal synchondrosis ( white arrow in e1 patent synchondrosis ; black arrow in e2 synostotic synchondrosis ) ; spheno - petrosal synchondroses ( white arrows in f1 patent synchondroses ; black arrows in f2 synostotic synchondroses ) ; spheno - occipital synchondrosis ( white arrow in g1 patent synchondrosis ; black arrow in g2 synostotic synchondrosis ) between the coronal and lambdoid arches . 
in addition , we demonstrate that both the minor sutures and the synchondroses play a remarkable role in determining asymmetries of the cranial fossae and alterations of the facial skeleton [ 18 ]  . materials and methods patients we retrospectively reviewed high - resolution ct images of 27 children with cranio - facial deformities secondary to craniosynostosis . 
twenty - one children ( 14 males , 7 females ) 167 months old ( average , 18 months old ) exhibited complex or multisutural synostoses ( 14 syndromic and 7 non - syndromic children ) , whereas six children ( four males , two females ) between the ages of 7 and 114 months old ( average 37 months old ) exhibited anterior synostotic plagiocephaly ( table 1 )  . radiol med ( 2014 ) 119 : 694704 classication patients diagnosed with table 1 craniosynostosis synostosis syndromic pansynostosis non - syndromic pansynostosis anterior synostotic plagiocephaly m male , f female patients sex age ( months ) the ct scan was performed using a multidetector scanner ( lightspeed pro 64 , ge medical system , milwaukee usa ) without the injection of contrast mediuthe scanner was equipped with automatic tube current modulation techniques . 
image acquisition was performed 100120 kvp , with parameters : following 50280 mas , scan time 1 s , small eld of view ( fov 1820 cm ) , slice thickness 1.25 mm and convolution lter for soft tissue . beginning from the native axial images , the data were processed using multiplanar reconstructions with bone radiol med ( 2014 ) 119 : 694704 table 5 orbital rim deformity in patients with coronal arch synostosis synostosis coronal arch orbital rim deformity coronal suture coronal and fs sutures none elevated ( harlequin deformity ) depressed and recessed syndromic pansynostosis non - syndromic pansynostosis anterior plagiocephaly fs fronto - sphenoidal table 6 chiari 1 malformation in patients with lambdoid arch synostosis synostosis lambdoid arch major sutures minor sutures ( om ) major and minor sutures chiari insertion of the tentorium children exhibited synostosis of the sutures of the coronal arch , ve children exhibited harlequin deformity of the orbit , and one child exhibited superior orbital roof displacement ( table 5 )  . in the group of newborns with complex craniostenosis ( syndromic and non - syndromic ) , in which the synostotic process involves the sutures of the lambdoid arch , 11 out of 15 children exhibited a low insertion of the tentoriuof these 11 children , nine exhibited caudal herniation of the cerebellar tonsils towards the magnum foramen ( chiari 1 ) ( table 6 )  . syndromic pansynostosis nonsyndromic pansynostosis om occipito - mastoid algorithms with a thickness of 0.65 mm and 3d volume rendering reconstructions ( 3d vr )  . using complementary 2d multiplanar images with bony algorithm and 3d vr reconstructions , all of the sutures ( minor and major ) , the synchondroses of the four sutural arches and any synostosis were assessed in each child . moreover , the remaining synchondroses of the skull base and cranial fontanels were also identied . results the results of our study are presented in tables 2 , 3 , 4 , 5 and 6 . 
all of the examined children with craniosynostosis exhibited synostosis of both the major and minor sutures of the four sutural arches of the skull ( table 2 ) as well as synostosis of the synchondroses and the fontanels ( table 3 )  . 
the patients consequently exhibited craniofacial alterations ( cranial deformity , superior orbital rima deformity , nasal root deviation , ethmoidal axis deection ) ( table 4 )  . facial alterations were observed in the majority of children with synostosis of the coronal arch . 
in the group of children with complex craniostenosis ( syndromic and nonsyndromic ) , 18 out of 21 children exhibited synostosis of the sutures of the coronal arch , 10 children exhibited harlequin deformity of the orbit , and only one child exhibited superior orbital roof displacement ( table 5 )  . 
in the group with anterior synostotic plagiocephaly , all discussion the evaluation of cranial deformities in newborns necessitates that clinicians be able to distinguish , above all , between positional plagiocephaly and craniostenosis . 
in particular , 3d ct has revolutionised the diagnostic evaluation , the planning of surgical procedures , the post - surgical evaluation and the follow - up [ 5 , 18 ]  . diagnostic imaging is useful to evaluate the involvement of the sutures in the synostotic process and to assess intracranial alterations that can be associated with craniostenosis . 
however , it should be emphasised that the use of the ct , although it allows the rapid acquisition of images without the use of anaesthesia , exposes newborns to a nonnegligible dose of radiation [ 5 ]  . 
 [ 19 , 20 ] have also demonstrated that this risk dramatically decreases with increasing age , especially during the rst year of life . the diagnostic technique of choice in children with craniostenosis remains a point of controversy and is partially dependent on the skull - facial malformations of the child . 
some authors have suggested the utility of alternative techniques to ct , such as ultrasound and conventional radiography of the skull , in children with cranial deformities associated with a lower clinical suspicion of 702 radiol med ( 2014 ) 119 : 694704 craniosynostosis or in children with the clinical suspicion of simple monosutural craniostenosis [ 19 ]  . 
nevertheless , other authors underline the high sensitivity ( 96.4 % ) and specicity ( 100 % ) of low - dose ct with 3d maximum intensity projection ( mip ) reconstructions for the identication of synostosis of the vault sutures in newborns with craniosynostosis skull - facial deformities ( complex craniostenosis ) [ 18 , 21 ]  . associated with serious in this regard , almost all of the modern mdct scanners are currently equipped with some type of automatic exposure control ( aec ) or automatic tube current modulation ( atcm ) technique [ 22 ]  . 
in our study , in most of the patients , we used the dose modulation technique called automa 3d , whereas more recently in two cases , default asir algorithm was used . 
the authors have also described other 3d reconstruction algorithms , including for craniostenosis , surface projection rendering ( spr ) although this algorithm is not as widely available as 3d mip [ 21 , 23 ]  . to date , however , no study has considered the effectiveness and the importance of low - dose spiral ct in identifying and assessing the vault sutural extension toward the skull base [ 18 , 24 ]  . 
consistent with many previous studies [ 14 , 2529 ] , our data conrmed the high frequency of facial alterations and the hemibase asymmetry of the anterior cranial fossa in all of the newborns in whom the synostotic process involved the sutures of the coronal arch , especially the coronal and the fronto - sphenoidal sutures [ 13 ]  . 
indeed , most of studied children with craniostenosis exhibited synostosis of one or more sutures of the coronal arch ( 24 out of 27 ) and consequently skull shape deformity , median axis deviation of the anterior skull base ( ethmoidal axis ) and orbit deformation ( table 4 )  . the coronal in agreement with current data , our results conrm that the orbital harlequin deformity is present both in children with isolated synostosis of suture ( major suture of coronal ring ) , and in children with associated ipsilateral synostosis of the coronal and frontosphenoidal sutures ( major suture and minor suture of the ba of the coronal ring ) [ 30 ]  . 
nevertheless , unlike anterior synostotic plagiocephalies , newborns with multiple synostosis ( syndromic and nonsyndromic synostosis ) in which coronal ring synostosis was identied , the severity of the facial deformity ( particularly orbital dysmorphism ) and the asymmetry of the anterior skull base was not very evident ; this may be a result of the symmetry of the synostotic process along the sutures of the coronal ring or the time course of the synostotic process . to date , different authors have conrmed the utility of low - dose spiral ct in children with complex or multisutural synostosis in avoiding irradiation in newborns with the clinical diagnosis of monosutural synostosis [ 18 , 19 , 21 ]  . 
however , we believe that low - dose spiral ct can be suitable in children with anterior synostotic plagiocephaly because high - resolution ct has the ability to identify the minor sutures of the coronal arch and , therefore , to radiol med ( 2014 ) 119 : 694704 fig . 
threedimensional computed tomography ( 3d ct ) ( a1 , a2 ) and axial ct image ( a3 , a4 ) show , on the right side , coronal synostosis ( black arrows in a2 , a3 ) and a patent fronto - sphenoidal suture ( arrow heads in a2 , a4 )  . 
note the elevation and relative vertical overgrowth of the right sphenoid , especially in the lateral portion of the greater wing , creating the harlequins eye ( a1 )  . 
3d ct scan ( b1 , b2 ) and axial ct images ( b3 , b4 ) show , on the left side , an absent frontosphenoidal suture ( arrow heads in b2b4 ) and a patent coronal suture ( black arrows in b2 , b3 )  . 
the roof of the left orbit is depressed with obvious retrusion of the lateral part of the supraorbital rim ( b1 )  . coronal and fronto - sphenoidal sutures are patent on the right side ( white arrows in b3 , b4 ) child with left fronto - sphenoidal and coronal sutures synostosis . 
3d ct scan ( c1 , c2 ) and axial ct image ( c3 , c4 ) show , on the left side , both fronto - sphenoidal suture ( arrow head in c2c4 ) and coronal suture synostosis ( black arrow in c2 , c3 )  . 
coronal and fronto - sphenoidal sutures are patent on the right side ( white arrow in c3 , c4 ) evaluate the extension of the synostotic process toward the skull base and the consequent asymmetric deformity of the anterior cranial base . these data can modify the therapeutic choice guiding toward timely and appropriate treatment . 
in our study of 15 children with complex craniostenosis in which the synostotic process involved the sutures of the lambdoid arch , 11 out of 15 children exhibited a low insertion of the tentorium , and 9 out of 15 exhibited caudal herniation of the cerebellar tonsils in the magnum foramen ( chiari 1 malformation ) ( table 6 )  . 
different authors have described the frequent evidence of chiari 1 malformation in children with syndromic multisutural or monosutural craniostenosis , describing the main contribution of the synostosis of the lambdoid suture in this dynamic and complex process [ 31 ]  . other authors have explained the onset of the chiari 1 malformation not only with the reduction in volume / deformity of the posterior cranial fossa secondary to synostosis of the lambdoid suture but also with the altered uid dynamics [ 32 ]  . 
our data conrm the importance of the lambdoid arch as well as the involvement of both the major and minor sutures ( individually or in combination ) in the onset of the chiari 1 malformation . therefore , we are proceeding to volumetrically evaluate , using magnetic resonance ( mr ) imaging , the posterior cranial fossa and the infra - tentorial compartment . 
in the 704 radiol med ( 2014 ) 119 : 694704 same study , we are evaluating some of the morphometric parameters of the posterior cranial fossa ( diameter of the foramen magnum , tentorial angle , and supraoccipital and basioccipital lengths ) in children with craniostenosis and with other syndromic conditions in which chiari 1 malformation is present to better explain the mechanisms of the cerebellar herniation and the variable timing of development . in conclusion , in the study of craniostenosis , low - dose ct with 3d vr reconstructions allows the prompt and precise identication of the extension of the synostotic process towards the skull base , which has important implications for surgical planning . conict of interest r calandrelli , g . 
x - ray ( n = 18 ) , computed tomography ( ct ) ( n = 24 ) and magnetic resoretrospectively nance evaluated . results five tumours were located in the cervical spine , 15 tumours were located in the thoracic spine and 10 tumours in the lumbar spine . 
197 , ruijin 2nd road , shanghai 200025 , china e - mail : rjzhangwb@yahoo.com.cn 682 introduction giant cell tumour ( gct ) is a relatively common skeletal neoplasm , accounting for approximately 45 % of all primary bone tumours and 20 % of benign bone neoplasms in adults [ 1 , 2 ]  . 
they occur infrequently in the spine , mostly in the sacrutheir presence in the mobile spine above the sacrum is even more exceptional , representing only 6.5 % of bone gcts according to the mayo clinic [ 5 ]  . previously published reports on gcts in the mobile spine were predominantly in the orthopaedic and neurosurgical domathere are a few reports of the imaging features of gcts in the mobile spine , which are limited to case reports or a few examples included in general reviews of spinal lesions [ 69 ]  . 
in this article , we discuss and illustrate the radiographic , computed tomography ( ct ) and magnetic resonance ( mr ) features of 30 cases of gct in the mobile spine . 
the purpose is to dene the characteristic imaging features of these unusual lesions , and to discuss our results with respect to the current literature . materials and methods patients we performed a retrospective review of 30 cases of gct occurring in the mobile spine under surgical treatment at 2 institutions between january 1990 and march 2012 . 
all 30 surgical specimens were reviewed by 2 pathologists experienced in musculoskeletal oncology in each institution to reconrm the diagnosis . the patients were evaluated on plain radiograph , ct and / or mr imaging before biopsy or surgery . 
informed consent was not required . imaging procedures anteriorposterior and lateral plain radiographs were performed in 18 patients . ct examination was performed in 24 patients with a 4or 16 - slice multidetector spiral ct scanner ( lightspeed , general electric medical systems , milwaukee , wi , usa ) radiol med ( 2014 ) 119 : 681693 using a routine protocol . 
unenhanced t1weighted spin - echo ( se ) images were obtained with a tr of 500600 ms and a te of 1525 ms , and t2 - weighted fast se or se images were obtained with a tr of 2 , 2004 , 000 ms and a te of 80110 ms . 
contrastenhanced images of sagittal and axial planes were obtained in 15 patients using a t1 - weighted spin - echo sequence with fat suppression . in addition , a plain radiograph or ct of the chest was performed to rule out pulmonary metastasis at presentation . imaging interpretation the imaging studies were evaluated retrospectively and independently by two experienced musculoskeletal radiologists at each institution . 
twenty patients had neurological decits including paralysis ( n = 3 ) , different degree of muscle weakness and numbness ( n = 17 ) , paraesthesia ( n = 6 ) , etc . 
five of the tumours involved the cervical spine , 15 involved the thoracic spine , and 10 the lumbar spine . dened in 13 cases and ill dened in ve cases . 
according to the campanacci grading system [ 10 ] , no case was classied as grade i , 5 cases were classied as grade ii , 13 cases as grade iii . radiographic ndings plain radiograph was performed in 18 cases . 
however , ct scan outlined the cortical alterations in a more accurate way , such as minor cortical erosion , bony ridges , absence of mineralised matrix and margin sclerosis . 
c on computed tomography ( ct ) , peripheral bony ridges ( white arrow ) created by endosteal scalloping of a lobulated tumour gave a radiographic soap bubble appearance which indeed were pseudotrabeculations . 
manipulation and rotation of the 3d images allows the surgeon to better understand the extent of the mass and to plan the operation . mr ndings the mr ndings of 21 cases of spinal gcts are summarised in table 5 . 
according to previous studies [ 9 , 11 ] , areas of low - signal intensity seen on t2 - weighted and gradientecho sequences may result from the presence of hemosiderin which is detected in more than 63 % of gcts . 
a , b plain radiograph showed a lytic and multiloculated lesion with a soap bubble appearance in the vertebral body of t7 , the border of the tumour was partially separated from the surrounding normal bone by an area of sclerosis of thin thickness ( black arrows )  . 
magnetic resonance imaging ( mri ) showed the tumour with homogeneous low signal intensity on t1 - weighted image and markedly high signal intensity on t2 - weighted image , without contrast enhancement , suggesting cystic components which may be consequential to haemorrhages or to secondary aneurysmal bone cyst formation . 
a band of low signal intensity surrounding the tumour on t1and t2 - weighted images ( white arrows ) partially corresponded to both brous capsule or reactive sclerosis seen on radiograph fig . 
a plain radiograph showed a lytic lesion in the t9 vertebral body , which was separated from the surrounding normal bone by a clearly depicted sclerotic border ( black arrow )  . 
peritumoural oedema was uncommon , mainly seen in patients with a history of trauma . radiol med ( 2014 ) 119 : 681693 table 4 computed tomography features of 24 giant cell tumours of the mobile spine case site eccentric pathologic fractures margin sclerosis bony ridges cortical destruction soft - tissue mass tpvb involvement spinal canal involvement right right centre centre left centre left left left left left right right right centre centre centre centre left left left centre left centre ? , local ? , local ? , local ? , short ? , short ? , long ? , short ? , short ? , short ? , short ? , long ? , short ? , long ? , short ? , short ? , short ? , short ? , long ? , long ? , short ? , short ? , short ? , short ? , long plus sign ( ? ) , present ; minus sign ( - ) , absent ; tpvb terminal plate of vertebral body fig . 
the border of the tumour was not well demonstrated due to bowel gas interference . c axial ct scan well depicted a thin area of sclerosis in the posterior margin of the tumour , separating it from the surrounding normal bone ( white arrow )  . 
mri showed the tumour with heterogeneous low signal intensity on t1 - weighted image and markedly high signal intensity on t2 - weighted image , suggesting polycystic components which may be consequential to haemorrhages or to secondary aneurysmal bone cyst formation . 
a band of low signal intensity ( thin black arrows ) was seen in the posterior margin of the tumour , partially corresponding to the sclerotic border seen on ct 688 radiol med ( 2014 ) 119 : 681693 fig . 
c , d ct scan showed a large and ill - dened soft - tissue mass involving the whole vertebra with spinal canal involvement ; contrast - enhanced ct showed intensive and heterogeneous enhancement of the mass ( white arrows )  . 
e , f thin - slice helical acquisitions with 2d and 3d reconstructions were routinely performed in sagittal and coronal planes , which clearly demonstrate the size and the outline of the tumour . 
after the solid intravenous administration of gadolinium , portion was enhanced with a marked and heterogeneous signal pattern discussion gcts of the mobile spine frequently develop 20 and 40 years of age and demonstrate a high female predilection in most series , with ratios ranging from 2.3 : 1 to 2.5 : 1 [ 14 ]  . the peak prevalence of our series is also in the third and fourth decades of life ( 83.3 % , 25 / 30 ) , although no predominance was found in female patients . 
in our series , the thoracic segment was also the most frequent location ( 50 % , 15 / 30 ) , but followed by the ( 33 % , 10 / 30 ) ; only ve cases were lumbar segment detected in the cervical segment ( 17 % , 5 / 30 )  . 
campanacci grade iii tumours [ 10 ] as well as the rate of soft - tissue extension are higher in our series than in patients with typical gct of long bone [ 10 , 17 ]  . 
on the one hand , the diagnosis might be delayed as the initial symptom , spinal pain , is extremely frequent in the orthopaedic practice and can easily be misinterpreted . 
on the other hand , it might be assumed that the gcts of the mobile spine are more aggressive [ 17 ]  . plain radiograph remains the mainstay of the diagnosis of gct . 
for gcts in the epiphyseal - metaphyseal areas of long bones , the location is one of the most important features suggesting the diagnosis [ 12 , 18 ]  . 
as a result , the radiographic presentations are less diagnostic for gcts of the mobile spine . ct scans are more useful in complex - shaped bones such as vertebrae , because the details of the lesion may not be depicted well on radiograph . 
ct improves detection of cortical thinning , pathological fracture , periosteal reaction , radiol med ( 2014 ) 119 : 681693 table 5 magnetic resonance features of 21 giant cell tumours of the mobile spine case site signal on t1weighting signal on t2weighting cystic areas haemorrhage fluid peritumoural oedema tpvb involvement spinal cord compression heterogeneous iso - low with small high area heterogeneous iso - low heterogeneous iso - low heterogeneous heterogeneous iso - low heterogeneous iso - low with small high area with polycystic high heterogeneous with polycystic high heterogeneous iso - low with small high area iso - low with polycystic high with polycystic high heterogeneous iso - low with small high area heterogeneous heterogeneous heterogeneous heterogeneous iso - low iso - low heterogeneous heterogeneous with polycystic high with polycystic high heterogeneous heterogeneous iso - low heterogeneous iso - low heterogeneous markedly high heterogeneous iso - low with small high area heterogeneous with polycystic high heterogeneous heterogeneous heterogeneous iso - low iso - low iso - low heterogeneous iso - low with small high area t10 heterogeneous iso heterogeneous iso t10 heterogeneous iso - low heterogeneous iso - low with small high area t11 heterogeneous iso heterogeneous iso t11 heterogeneous heterogeneous t12 heterogeneous iso - low iso - low with polycystic high heterogeneous iso - low with small high area heterogeneous polycystic marked iso - low high centre low and peripheral iso with small high area centre high and peripheral iso with small high area uid levels softtissue mass large ? , slight ? , slight ? , slight small large small large small large large small ? , slight ? , slight ? , slight ? , moderate ? ? , slight 690 table 5 continued radiol med ( 2014 ) 119 : 681693 case site signal on t1weighting signal on t2weighting cystic areas haemorrhage fluid uid levels softtissue mass peritumoural oedema tpvb involvement spinal cord compression heterogeneous heterogeneous iso - low with polycystic high plus sign ( ? ) , present ; minus sign ( - ) , absent fig . 
c marked and heterogeneous enhancement was seen after intravenous administration of contrast agent ( thin black arrow )  . d sagittal t1 - weighted image , e sagittal t2 - weighted image , f axial t2 - weighted image , g contrast - enhanced sagittal t1 - weighted image . the lesion contained a small high - signal - intensity area on t1weighted images , suggesting relatively recent haemorrhage ( white arrow )  . 
after intravenous administration of gadolinium , the mass was enhanced with a heterogeneous signal pattern degree of osseous expansion and matrix mineralisation compared with radiograph [ 12 , 19 ]  . 
in our series , ct detected minor cortical destruction in two cases ( cases #21 and #27 ) and a small soft - tissue mass in one case ( case #30 ) , which had been missed on radiography . 
on ct , peripheral bony ridges due to endosteal scalloping of a lobulated tumour gave a radiographic soap bubble appearance which were in fact pseudotrabeculations [ 18 , 19 ]  . 
however , the bony ridges in these lesions are usually much longer . mr has a better soft - tissue resolution and multiplanar imaging features , which allows for an accurate evaluation of the soft - tissue extent and the relationship with surrounding tissues . 
a axial and b sagittal t1weighted mr image showed a large and heterogeneous mass presenting a uiduid level with superior / inferior layer signal intensity as high / low pattern ( black arrows ) although artefacted by an internal metal xation structures and blood supply [ 12 , 13 , 15 , 18 ]  . 
the solid components of gct demonstrated low - to - iso signal intensity on t2 - weighted images in the majority of our cases , which is reported to result from hemosiderin deposition or high collagen content [ 12 , 13 , 20 , 21 ]  . 
 [ 11 ] found that in ten cases with low signal intensity on t2 - weighted mr images , neither dense collagenous matrix nor bone formation was prominent in the specimens , whereas large amounts of hemosiderin in the mononuclear stromal cells and multinuclear giant cells were pathologically conrmed . 
the authors believed that the diffusely dispersed extravascular erythrocytes found in their study was a characteristic pathological nding of gct , and was accordingly considered to be an important cause for the frequent and massive hemosiderin deposition in the tumour . 
they concluded that the low - signal - intensity areas on t2weighted mr images were probably the rst radiological evidence of the phagocytic nature of gct and could be a sign of relatively high differentiation or low aggressiveness of the tumour . 
it can also be a key differential feature in excluding other tumours such as metastasis , myeloma , lymphoma , and chordoma that generally demonstrate high signal intensity on t2 - weighted mr images [ 12 , 16 , 22 ]  . gct is the most common lesion associated with secondary abc , accounting for 39 % of the lesions [ 12 , 20 , 2325 ]  . 
mr imaging is also sensitive for detection of cystic components and uiduid levels secondary to abc . contrast - enhanced mr imaging is especially helpful in distinguishing cystic from solid regions of gct , which can be vital for patients treatment for two important reasons : rst , to prevent misdiagnosis of the lesion as a primary abc which contains only cystic components ; and second , to guide biopsy directly to the solid portions of the lesions which harbour diagnostic tissue , as opposed to abc regions which yield nonspecic blood [ 12 ]  . 
 [ 23 ] reported that bone tumours which had uiduid levels with superior / inferior layer signal intensity as high / low on t1 - weighted images were 2.3 - times more likely to be malignant than those with low / high - signal - intensity pattern . 
however , in our series , three lesions ( cases #10 , #14 and #21 ) were partially separated from the surrounding normal bone by a thin sclerotic border on radiograph or ct and a band of low signal intensity on mri , corresponding to both brous capsule and reactive sclerosis [ 11 ]  . 
since bony sclerosis is a host reaction against the tumour and correlates with a less aggressive radiographic appearance , a better prognosis might be predicted when the tumour is contained within this sclerotic margin suggestive of a slow - growing lesion [ 12 , 18 ]  . when encountering a single osteolytic mass in the the differential diagnosis includes abc , mobile spine , brown tumour of hyperparathyroidism , bony metastasis to the spine , haemangioma , chordoma or chondrosarcoma , tuberculosis , etc . 
mr imaging reveals the detailed characteristics of the internal contents with uiduid levels in one or more granular spaces , haemorrhage , and a hypointense circular rim surrounding the entire lesion which correlates with the pathological nding of a brous capsule [ 25 ]  . 
to differentiate a primary abc from a gct with prominent abc components , mr imaging may help by demonstrating a purely cystic appearance in the former lesion , compared with solid components in the latter [ 16 , 22 , 26 ]  . 
brown tumour of hyperparathyroidism is expansile and well marginated and highly likely to show low signal intensity on mr images that can mimic gct , but it must be accompanied by other manifestations of hyperthyroidism and can be excluded by measuring levels of serum calcium and alkaline phosphatase [ 1113 ]  . 
haemangioma is a benign vasoformative neoplasm of endothelial origin , usually with a characteristic presentation as honeycombed or sunburst appearance with spindles radiating towards the periphery [ 28 ]  . 
chordoma or chondrosarcoma are characterised by a high signal on t2weighted images , generally not a feature of gct , so such a nding would favour a diagnosis of chordoma or chondrosarcoma [ 13 ]  . 
the most common site of spinal tuberculosis is the thoracolumbar junction and the most common symptom is back pain , while cough , fever , night sweats and weight loss are less frequent . 
paraspinal , prevertebral or spinal abscess is frequent and the intervertebral discs are often involved [ 30 ]  . although the vast majority of gcts are benign lesions , malignant gcts ( dened as a sarcomatous growth ) account for 510 % of all gcts [ 12 ]  . 
imaging features of gct suggesting local aggressiveness include a large size , rapid growth , illdened boundaries , and invasion of the surrounding soft tissues [ 2 ]  . in conclusion , although rare , gct can occur in the mobile spine . 
radiologia , dipartimento cardio - toraco - vascolare , azienda ospedaliero universitaria , policlinico sant orsolamalpighi , bologna , italy e - mail : giangasparemineo@alice.it subsequently , a clinical - instrumental evaluation was performed , and the response to therapy and histopathological reports were evaluated . results radiological evaluation based on hrct ndings revealed 29 patients as pvod - suspicious and 67 as not pvod - suspicious . 
the ct scan showed 95.5 % sensitivity , 89 % specicity , 72.5 % positive predictive value , and 98.5 % negative predictive value , with a diagnostic accuracy of 90.5 % in identifying patients with pvod . conclusions chest ct can be considered a screening test in the assessment of patients with pah of unknown aetiology , and the radiologist can help the clinician to identify patients with ct ndings that make pvod highly probable . keywords pulmonary veno - occlusive disease ( cid : 2 ) pulmonary hypertension ( cid : 2 ) hrct ( cid : 2 ) differential diagnosis c . 
radiologia , sezione radiologia durgenza , dipartimento di emergenza / urgenza , chirurgia generale e dei trapianti , azienda ospedaliero universitaria , policlinico sant orsola - malpighi , bologna , italy a . 
cardiologia , dipartimento cardio - toraco - vascolare , azienda ospedaliero universitaria , policlinico sant orsola - malpighi , bologna , italy with less than 200 cases described in the literature , pulmonary veno - occlusive disease ( pvod ) is a rare form of pulmonary arterial hypertension ( pah ) [ 1 ] which is associated with a worse prognosis compared to idiopathic pah ( ipah ) [ 2 , 3 ]  . 
although the aetiology has not yet been identied , several risk factors are thought to be involved including infection , chemotherapy toxicity [ 4 ] , radiation , autoimmunity and genetic predisposition [ 58 ]  . signs and symptoms are not specic and mimic those of other disorders ; they include dyspnoea , fatigue , chest pain , haemoptysis , cyanosis , pulmonary crackles on auscultation 668 radiol med ( 2014 ) 119 : 667673 and clubbing on physical examination . 
haemosiderin - laden macrophages in the bronchoalveolar lavage ( bal ) uid , low diffusion of carbon monoxide ( dlco ) in pulmonary function tests as well as low partial pressure of oxygen in arterial blood ( pao2 ) may also be found . the obstructed venous vessel the key histopathological hallmark is a widespread brous intimal proliferation , typically patchy in distribution that predominantly involves the pulmonary venules and small veins , with a gradual reduction of the vascular lumen until complete occlusion [ 9 ] ; the central recanalisation of is frequently observed [ 10 ]  . 
in the lung parenchyma , patchy areas of alveolar capillary dilatation ( socalled loop - like appearance ) are present upstream from the narrowed and occluded veins ; in these areas there is often interstitial brosis , haemorrhage , and intra - alveolar haemosiderin - laden macrophages , probably due to chronic passive congestion . 
with regard to the pulmonary arterial circulation , the muscular pulmonary arteries show medial hypertrophy , while the arterioles become muscularised secondary to post - capillary obstruction of venous drainage [ 11 , 12 ]  . pvod remains a clinical entity difcult to classify ; it shares some features with pre - capillary forms of pah , but there are histopathological , clinical and therapeutic differences . 
table 2 summarises the instrumental ndings suggestive of pvod . in pvod , the x - ray examination only shows kerley b lines and peripheral interstitial thickening in addition to the classic signs of pah ( ectasia of the pulmonary arteries / pulmonary trunk and cardiomegaly with a prevalence of right sections )  . computed tomography ( ct ) , especially the high - resolution study of the lung parenchyma ( hrct ) , is nowadays considered an integral part of the diagnostic workup of pvod [ 16 ] , owing to the detection of smooth thickening of the interlobular septa , ground - glass opacities , increased size of the mediastinal lymph nodes , pleural and pericardial effusions [ 17 , 18 ] ( even though the importance of pleuropericardial effusion is still controversial ) [ 19 ]  . because of the lack of response of ipah to drug therapy which consists in vasodilators ( prostanoids , antagonists for the endothelin receptor , inhibitors of phosphodiesterase type 5 ) and which might even worsen the prognosis due to the onset of severe , at times fatal , pulmonary oedema , the only curative therapy for pvod is represented by cardiopulmonary or lung transplantation [ 20 , 21 ]  . 
therefore , a correct and timely diagnosis becomes crucial to start an adequate medical treatment . the aim of our study was to evaluate the diagnostic accuracy of hrct for povd in a large group of patients with pre - capillary pah of unknown aetiology , and assess the inuence of hrct ndings in determining the diagnosis and subsequent treatment . materials and methods we retrospectively evaluated the ct scans of 131 patients with pre - capillary pah of unknown aetiology performed between 2005 and 2012 , as part of the diagnostic algorithm arterial blood gases pulmonary function tests bronchoalveolar lavage haemosiderin - containing pwp b15 mmhg pao2 \70 mmhg dlco \55 % macrophages ventilation / perfusion lung normal or patchy perfusion defects scan mpap value c25 mmhg at rest , measured by right heart catheterisation , is suggestive of pulmonary hypertension mpap pulmonary arterial pressure , pwp pulmonary wedge pressure , pao2 partial pressure of oxygen , dlco lung diffusion capacity for carbon monoxide pulmonary hypertension of our institute . 
we subsequently evaluated the results of other noninvasive clinical and instrumental investigations , such as pao2 , dlco and the 6 - minute walking test ( 6mwt ) , based on which the therapy was started . 
finally , a post - therapy assessment was performed based on the development of pulmonary oedema secondary to treatment with vasodilators , and on the histological results , if available . statistical analysis the signicance of each hrct nding for the diagnosis of povd was calculated with the fisher exact test . 
sensitivity , specicity , positive predictive value , negative predictive value , diagnostic accuracy of ct and likelihood ratio were calculated using the software openepi ( com , copyright the open source initiative )  . results on the basis of the presence of at least two hrct ndings specic to povd , 29 patients ( 8 men and 21 women ) were considered povd - suspicious ( 30 % , group 1 ) , and 67 not povd - suspicious ( 70 % , group 2 )  . 
all patients had both a dilatation of the pulmonary arteries and right heart chambers , consistent with pah ; in no case was thromboembolism or cardiopulmonary malformations documented . as a result of the clinical - instrumental analysis , among the 29 patients of group 1 , 15 were nally classied as ipah and therefore received treatment with vasodilators ; post - therapy eight patients present complications , while seven patients developed pulmonary oedema leading to a subsequent reclassication of their diagnosis from ipah to povd . 
1 diagnostic efcacy of high - resolution computed tomography ( hrct )  . according to the hrct ndings , patients were subdivided into pulmonary veno - occlusive disease ( pvod ) - suspicious and not pvod - suspicious . 
in none of the six patients with a histological diagnosis of ipah , were septal thickening or enlarged lymph nodes documented , while ground - glass opacities were observed in three cases . discussion and conclusions in the diagnostic classication of patients with evidence of pah of unknown aetiology and pre - capillary pulmonary hypertension at right heart catheterisation , the early identication of those with povd and the differential diagnosis with ipah are crucial . 
moreover , thanks to the high negative predictive value of ct ( 98.5 % ) , the absence of specic hrct signs allows the exclusion of povd . from the comparison between the hrct ndings and the histological examination , we found that all patients with a histological diagnosis of povd showed smooth thickening of the interlobular septa , ground - glass opacities and enlarged lymph nodes . 
pulmonary oedema with bilateral pleural effusion and ground - glass opacities after vasodilatator therapy glass only ; this is further evidence of the importance of the association of the three hrct signs for the diagnosis of povd . our study has some limitations , including the small number of histological examinations and the lack of data from bal , which is not routinely performed . 
in our opinion , bal should be integrated with other radiological and clinical investigations because it is a repeatable and easy examination which allows the identication of haemosiderin - laden macrophages ( frequently observed in povd and rarely in ipah ) [ 2527 ]  . to conclude , chest ct should be considered in the screening of patients with pah of unknown aetiology ; the radiologist could cooperate with the clinician in the recognition of individuals with a suspected povd , whose treatment is different from that of ipah due to the risk of a fatal pulmonary oedema . 
changes in patient body contours were evaluated by comparing the volumes within the external skin outline . results apart from two patients requiring re - planning due to substantial weight loss , our results evidenced no signicant shifts of ptvs and pgs . 
pg volume decreased with a trend in volume reduction for the ipsilateral parotid . no signicant shift of spinal cord at c1 and c6 level was detected , in either the ap or ll direction . 
giovanni battista hospital , torino , italy data demonstrated a trend in external skin contour volume loss . conclusions our preliminary results reect the literature data and indicate that an off - line adaptive rt approach is appropriate in clinical practice . keywords head and neck cancer ( cid : 2 ) intensity - modulated radiotherapy ( cid : 2 ) planning target volumes ( cid : 2 ) organs at risk ( cid : 2 ) computed tomography ( cid : 2 ) adaptive radiotherapy introduction intensity - modulated radiation therapy ( imrt ) is becoming the standard technique for the treatment of head and neck cancer ( h&n ) , because it permits high - dose conformity around complex target volumes while improving sparing of critical structures , leading to an improved therapeutic index . 
through online or off - line interventions at different timescales , adaptive radiation therapy ( art ) is an approach to correct for temporal morphological changes in a patients anatomy during imrt , using computed tomography ( ct ) techniques such as megavoltage ct , ct on rails and cone - beam ct in the treatment room [ 2 , 3 ]  . 
the art process is closely linked to imageguided radiotherapy ( igrt ) , which is commonly interpreted as the use of in - room imaging to perform set - up correction , and aimed to reduce clinical target volume ( ctv ) and planning target volume ( ptv ) margins . the purpose of this prospective study , carried out in an academic department of radiation oncology not equipped with in - room volumetric imaging systems , is to assess the radiol med ( 2014 ) 119 : 714720 volumetric and positional changes of ptvs and selected organs at risk ( oars ) in patients treated with imrt , using consecutive off - board conventional ct scan studies . dosimetric aspects were not investigated in this preliminary study . 
ctv1 was generated by adding a 1 - cm margin to gtv , or by including the postoperative tumour table 1 selected patient , tumour , and therapy characteristics bed in the positive / close margin and dissected lymph node level with extracapsular extension ( ece )  . 
ctv2 was dened as the volume near the tumour at risk of subclinical disease ; in adjuvant settings , ctv2 included the tumour bed plus dissected lymph node levels with positive lymph nodes without ece . 
ctv3 included clinically negative lymph node levels at lower risk . outlined critical structures were optic nerves , optic chiasm , parotid glands , temporomandibular joints , mandible , lens , eye globes , temporal lobes , posterior fossa , inner ear and larynx . 
for the brainstem and spinal cord ( sc ) , an additional 3and 5 - mm margin to create a planning risk volume ( prv ) was added , respectively [ 5 ]  . radiotherapy planning baseline h&n imrt planning involves 7 or 9 coplanar , 6 mv elds using the step - and - shoot technique . 
it is important to underline that our tps supports only rigid body and not deformable image registration , not allowing calculation of cumulative dose distribution on the re - scanned ct sets [ 2 , 6 ]  . 
external contours were delineated in all the new ct scans . positional analysis and volume comparisons based on tps , positional changes of ptvs and sc as well as positional and volumetric changes of pgs were obtained in all patients for each ct set . 
the com coordinates were automatically obtained from tps , asking the system to set the beam isocentre in the geometric centre of the volumes of interest . the positional vectors between the virtual isocentre , dened on the plan - ct and identied by radiopaque markers on each subsequent ct study , and the ptv / pgs com were calculated . the distance d between the virtual isocentre and the com of each volume of interest was simply computed as follows : ( cid : 2 ) x ( cid : 3 ) x1 2 y ( cid : 3 ) y1 2 z ( cid : 3 ) z1 ( cid : 3 ) where ( x , y , z ) are the com coordinates and ( x1 , y1 , z1 ) are the virtual isocentre coordinates . 
1 spinal cord displacements into the spinal canal along the anteriorposterior and latero - lateral axes positive shift sign indicated a sc displacement towards the posterior wall of the vertebral canal and a sc shift towards the left side along the ll axis . as a representation of patient weight loss , the change in the patient contour was evaluated by calculating the volume within the external skin outline [ 7 ]  . statistical analysis linear regression was used to analyse the relative variation in volumes of the parotids and external contour correlated with dose . 
the distribution of shift values during the treatment course of ptvs , pg and sc was simply analysed in terms of mean , standard deviation and range of variability ( 1st and 99th percentile )  . 
the mean value , the p value of the one - sample t test and range of variation of the relative shifts measured for ptvs , pgs and sc are reported in table 2 . 
collected data out of this range are related to signicant weight loss ( [ 5 % ) , which occurred in two patients ( patient #4 and #6 reported in table 1 ) with replacement of the thermoplastic mask and mandatory imrt re - planning ( table 3 )  . 
ptvs and oar contours were imported from the plan - ct to the new image set and re - delineated according both to the new set - up and the anatomical variations . 
to investigate the correlation between ipsilateral pg volume with total dose , the relative volume variation was analysed with linear regression , grouping data between ipsilateral and contralateral pg , both for left and right glands . 
the one - sample t test p values were always [ 0.05 , showing the random data of the shiaccording to these values , the safety 5 - mm margin applied for prv was appropriate . external patient contours the collected data demonstrated a trend towards volume loss of external skin contours , with a mean reduction less than 5 % for all patients . 
in our study population , as weight loss [ 5 % only occurred in 20 % of treated patients , volume reductions of external patient contours did not correlate with nutritional status . 
our data showed a volume loss of both pgs , greater for the ipsilateral pg , of 30 % at an accumulated dose c40 gy , recording no shift for either pg . 
although a signicant variation of the left pg through the course of treatment has been previously reported , this statistically signicant value appeared to be of uncertain clinical meaning , in relation to the small number of patients enrolled and the wide variation in data found for both the left and right pg . the prospective study of bhide et al . 
on 20 h&n cancer patients studied by repeat ct scans at weeks 2 , 3 , 4 , and 5 during induction chemotherapy followed by chemo - imrt , showed a statistically signicant reduction of ctvs volumes at week 2 due to therapeutic effects , resulting in dosimetric changes to the ptvs . 
reported the results of a prospective art program for 23 h&n patients who underwent planned ct at 11 , 22 , and 33 fractions with mandatory re - planning based on comparative dosimetric analyses [ 13 ]  . 
quantify both volumetric and dosimetric changes in selected oars during a course of imrt for 26 oropharyngeal carcinomas using repeat cone - beam ct planned weekly during therapy [ 14 ]  . 
all evaluated oars underwent volumetric modications from baseline and the largest volume reduction ( * 30 % ) was observed for pgs , consistent with our results . the same data about the shrinkage of pg was evidenced in the study by loo et al . 
carried out a study to assess the feasibility of routine art in h&n cancer patients and to determine which patients may be selected for this approach [ 15 ]  . twenty patients undergoing denitive chemo - rt and fig . 
however , older art approaches can be still adopted using implanted ducial markers or repeating the imaging study to guide manual re - planning . as our linear accelerator ( synergy platform ; elekta atlanta , ga , usa ) is not equipped with cone - beam ct , we implemented a protocol of serial ct scans to optimise imrt delivery for h&n cancer patients , reporting the magnitude of volumetric and / or positional changes of ptvs and selected oars . we need to emphasise that our tps is not able to perform cumulative dosimetric plan analysis . 
conducted a study on 14 h&n cancer patients using an integrated ct - accelerator imaging system throughout the rt course to investigate geometric and volumetric changes relative to gtvs and oars [ 1 ]  . 
even though gtv was modied during rt due to tumour shrinkage , the authors concluded that re - planning was not necessary because no signicant dosimetric modications to the target were observed , while the main benet of re - planning is the improved sparing of pgs . 
since target volumes were not redelineated during imrt , our results show that re - planning is only mandatory in patients with a weight loss [ 5 % . 720 radiol med ( 2014 ) 119 : 714720 adjuvant rt were enrolled . 
our data suggest that weight loss is correlated to re - planning benet without difference between patients treated in adjuvant or denitive modality . the literature data show that routine re - planning is probably not necessary in all h&n cancer patients and that signicant weight loss is correlated with positional shifts of ptvs . 
a way to identify weight loss is to evaluate changes in the patients body contour using repeat ct scans [ 16 ]  . probably , the appropriate time for adaptive interventions might be in week 2 after the beginning of irradiation , because most anatomical changes are observed in the second and third week of imrt [ 17 ]  . in clinical practice , online art is the ideal treatment modality but remains a difcult and time - consuming approach [ 17 , 18 ]  . 
on the contrary , off - line art remains more useful , because real - time intervention is not a pressing need as most anatomic variations in h&n cancer patients take place gradually [ 17 ]  . consistent with the literature data , our results suggest that shifts of the ptv and pgs are relatively small . 
bonucci radiotherapy unit ifca , university of florence , florence , italy keywords cyberknife ( cid : 2 ) radiosurgery ( cid : 2 ) brain metastases ( cid : 2 ) brain tumour ( cid : 2 ) stereotactic radiotherapy introduction the development of brain metastases is a dismal event which can occur in up to 20 % of all cancer patients throughout their disease progression [ 1 ]  . 
traditionally , whole - brain radiotherapy [ 2 ] has represented the only treatment modality available in the case of lesions not amenable to surgical resection , patients deemed not operable , or both . 
in the last two decades , stereotactic radiosurgery has emerged as an alternative approach for not operable , single brain metastases or for selected patients with multiple metastatic brain lesions . 
oligometastatic disease refers to a limited metastatic burden , and conventionally authors have dened patients with this entity as any burden from 1 to 5 sites of disease [ 3 ]  . 
it has been level - 1 evidence consistently supports the shown that adoption of different treatment strategies [ surgical resection ( sr ) , stereotactic radiosurgery ( srs ) , whole - brain radiotherapy ( wbrt ) , either alone or combined with one the management of patients with brain another ] metastases [ 4 ]  . the choice of a local treatment alone or in association with whole - brain radiotherapy is usually made in patients with a better prognosis depending on performance status , number of brain metastases , controlled systemic disease and histology [ 5 ]  . 
recently , two large randomised studies have shown similar survival benets and functional independence between patients with 13 brain metastases treated with srs alone and srs plus wbrt [ 6 , 7 ]  . radiosurgery may result in a better local control in patients with radioresistant histology and it can defer the 722 radiol med ( 2014 ) 119 : 721726 different notwithstanding wbrt as salvage treatment . 
the ideal candidate for radiosurgery is the patient with controlled extracranial metastases and an excellent performance status [ 8 , 9 ]  . therapeutic however , approaches attempted , a signicant number of these patients develop a local relapse within the surgical bed or a previously irradiated area . 
for selected cases , when all other treatment modalities are either ineffective or not possible , re - irradiation ( ri ) with cyberknife stereotactic radiosurgery ( csrs ) could be the only viable therapeutic strategy . 
to a lesser extent , the potential of ri by means of csrs has been also explored in the context of well - dened , previously irradiated recurrent high - grade gliomas , with promising results . 
there are few experiences in the literature that report on the efcacy and toxicity of patients who had various courses of radiotherapy within the same radiotherapy eld [ 10 ]  . the literature remains scarce regarding the role of ri for selected patients with recurrent single / oligometastases or primary brain tumours . 
the aim of our study was to retrospectively evaluate the feasibility and clinical benet of csrs in 13 patients treated at florence university for recurrent , pre - irradiated brain lesions . materials and methods from december 2011 to may 2012 , 13 patients underwent ri at the university of florence for a previously irradiated , recurrent brain lesion . 
none of the patients received concurrent chemotherapy , all metastatic patients underwent ri after failure of a chemotherapy regimen and the metronomic chemotherapy was started for these patients at least 15 days from the end of ri . 
in the two patients with high - grade glioma , ri was delivered as salvage treatment due to the haematological toxicity of the systemic therapy . five patients underwent srs as upfront therapy and were re - irradiated with csrs while in six cases wholebrain radiotherapy was followed by srs and at recurrence table 1 patient characteristics characteristics no . 
of patients % c6 m karnofsky performance status time from radiotherapy to cyberknife \6 m irradiation volume \10 cc c10 cc re - irradiation volume \10 cc c10 cc stereotactic radiosurgery dose \20 gy c20 gy no . 
in the two cases of primary brain tumours , 3 - dimensional conformal radiotherapy was delivered to the surgical bed , with a total dose of 60 gy with standard fractionation ( 2 gy / fr ) ; at recurrence , ri was performed with csrs . 
all patients underwent a brain mr scan which showed a local progression at the previously irradiated area . mean tumour volume at csrs measured on planning software was 40.43 cc ( 7374 cc )  . 
the radiation therapy oncology group ( rtog ) central nervous system ( cns ) toxicity criteria [ 11 ] were adopted to evaluate toxicity . the cyberknife system the cyberknife ( accuray incorporated , sunnyvale , ca , usa ) is an image - guided frameless radiosurgery system capable of fractionated treatment . 
a 1 - mm uniform margin from gtv to ptv was applied to take into account the total targeting error ( whole procedure of image guidance and treatment delivery ) as derived by dedicated end - to - end tests performed on an anthropomorphic head phantoplans were optimised using stepwise multicriteria optimisation in the sequential module of the multiplan dedicated treatment planning system ( tps ) ( accuray incorporated , sunnyvale , ca , usa ) , and dose was calculated by a ray tracing algorithdoses were prescribed at the 80 % isodose line . 
together with ptv coverage ( percentage of volume inside the prescription isodose line ) and oar constraints , conformity indexes and doses to healthy brain tissue were also considered during plan optimisation . the conformity index was calculated as the ratio of the volume inside the prescription isodose to the ptv . 
doses to healthy tissue were minimised during the optimisation process by means of automatic shell volumes around the ptv and were quantied using the gradient index ( gi ) dened as the ratio of the volume of half the prescription isodose to the volume of the prescription isodose . treatment planning and plan qa the average value over 13 plans for ptv coverage ( percentage of volume inside the prescription isodose ) was 97.5 % ( max = 100 % ; min = 92.5 % ) ; the lower coverage values were obtained for those plans where the brain stem was tangential to the ptv . 
according to the macdonald criteria , complete response ( cr ) was dened as no visible gross tumour or absence of contrast enhancement , partial response ( pr ) as more than 50 % decrease , no change ( nc ) as \50 % decrease and progressive disease ( pd ) as more than 25 % increase of gtv [ 14 ]  . 
local control and progression - free survival rates were calculated as the time interval between re - irradiation and progression ( kaplan and meier method )  . results in terms of compliance to csrs , the majority of patients did not develop any acute side effects . 
in fact , in 54.6 % of patients steroid medication was not changed and in 30 % it was reduced ( including the replacement of dexamethasone by prednisolone )  . 
in particular , one patient was treated as a rst treatment with srs on 25 cc of tumour volume with 27 gy / 3f at 80 % isodose . the csrs volume was 41.60 cc and the dose delivered was 24 gy / 3f at 80 % . 
the second patient received as a treatment whole - brain radiotherapy ( 30 gy / 10 f ) rst followed by srs on 5 cc tumour volume ( 27 gy / 3f at isodose of 80 % )  . 
the csrs volume was 6.07 cc and the dose delivered was 16 gy to the 80 % isodose in a single fraction . the small number of patients and the short follow - up limit the statistical analysis . 
at the time of analysis we did not report any local progression in the bratwo patients had distant progression with new metastases outside of the braat the time of analysis all patients are alive . discussion recurrent brain lesions present a special treatment challenge for patients already treated with radiation . 
conventional salvage radiation therapy has been tried in selected patients , but whether survival is enhanced without intolerable toxicity is unclear [ 15 , 16 ]  . a rapid treatment response , short treatment time , and reduced doses to normal tissue make radiosurgery a rearecurrent brain lesions ( table 4 )  . sonable option for radiosurgery has shown to be as effective as surgery plus whole - brain radiotherapy ( wbrt ) in patients with a single brain metastasis [ 21 ]  . 
it is thought that prior radiotherapy increases the risk of radiation - induced toxicity from salvage radiosurgery because the cumulative dose to the brain is absolutely higher than that of upfront treatment [ 23 ]  . 
some reports have suggested a short - term benet of salvage radiosurgery for recurrent brain lesions [ 24 , 25 ] but the incidence of long - term radiation toxicity has not been investigated thoroughly and clear guidelines for assessing the risk of radiation toxicity from summated radiation do not exist . 
in order to explore the potential role of re - irradiation with csrs as a possible salvage treatment patients already subjected to srs , our study aimed to analyse the clinical benet and tolerability in this subset of patients . 
even if haemorrhagic transformation ( ht ) of ischaemic brain tissue after rt - pa thrombolysis as detected by magnetic resonance imaging ( mri ) can be asymptomatic , it may impair neustudies have rological recovery [ 3 ]  . 
moreover , mri symptomatic 176 radiol med ( 2014 ) 119 : 175182 suggested that microbleeds ( mb ) may be a potential marker of a haemorrhage - prone state [ 46 ] or of vascular cognitive impairment [ 7 ]  . 
therefore , it is necessary to early and accurately detect mb or ht before and after thrombolysis [ 811 ]  . although mb may be markers of increased risk of secondary haemorrhage after thrombolytic therapy in stroke patients [ 1013 ] , secondary mb or ht from ischaemic infarction is not necessarily associated with poor prognosis . 
the key question is an early and accurate detection of mb or ht , as well as a rapid treatment decision - making according to neuroimaging ndings . these measures are helpful to prevent mb , ht , or parenchymal haemorrhage ( ph ) , and to further decrease the incidence of mb or ht , and to benet neurological recovery . 
only brain imaging can conrm the diagnosis of mb or ht , and differentiate haemorrhage from ischaemia with a high level of accuracy . therefore , we believe that making rapid treatment decisions after thrombolysis according to swi may optimise the patients neurological recovery based on an early detection of mb , ht or ph . 
recently , susceptibilityweighted imaging ( swi ) and t2 - weighted imaging have become sensitivity markers for the accurate detection of mb or ht after ischaemic stroke [ 10 , 12 , 1416 ] , but several studies have shown that swi is superior to t2weighted sequences in detecting mb [ 1719 ]  . 
thus , the purpose of this study was to evaluate the effect of swi for antiplatelet therapy on post - thrombolysis mb . materials and methods study design this prospective clinical study was conducted between january 2009 and december 2011 . 
the institutional review board approved the study , and patient ( or legal representative ) consent was obtained before study enrolment . patients were eligible for thrombolysis if they met the following criteria : ( 1 ) documented clinical signs and symptoms of acute circulation stroke ; ( 2 ) national institutes of health stroke scale ( nihss ) scores [ 20 ] ranging from 4 to 22 at baseline ; ( 3 ) age between 18 and 80 years ; thrombolytic therapy administered within 6 h of symptom onset ; ( 5 ) the absence of intracranial haemorrhage conrmed by computed tomography ( ct ) before and within 24 h of thrombolysis . patients were excluded from thrombolysis if any of the following criteria was present : ( 1 ) intracranial haemorrhage , cerebral stroke of any aetiology , or myocardial infarction in the past 3 months ; ( 2 ) history of alimentary canal or urinary system haemorrhage , or trauma in the last 3 weeks ; ( 3 ) current anticoagulation therapy ; ( 4 ) personal or family history of haemorrhagic tendency or haemorrhagic disease ; ( 5 ) history of circulatory failure or unconrenal , or hepatic trolled hypertension , severe cardiac , inadequacy , severe diabetes , or current pregnancy . addition , patients were also excluded for the following reasons : ( 1 ) lacunar infarctions on mri ; ( 2 ) mri follow - up or clinical scoring was refused ; ( 3 ) mri was incomplete because of technical reasons or the subjects inability to cooperate ; ( 4 ) an apparent diffusion - weighted imaging ( dwi ) lesion exceeding 70 % of the territory of the ipsilateral hemisphere . a total of 204 consecutive patients with acute stroke were screened by mri within 6 h after symptom onset before thrombolysis . 
mri revealed no infarction in 21 patients , lacunar infarction in 19 patients , haemorrhage ( mb = 12 , ht = 2 ) in 14 patients and huge acute ischaemic lesion in four patients . 
the standard dosage for intravenous rt - pa therapy was 0.9 mg / kg body weight , with a maximum dose of 90 mg ; 10 % of the total dosage ( 0.9 mg / kg ) was injected as an intravenous bolus for 1 min , while the remainder was given by continuous intravenous infusion over the next 59 min . after thrombolysis , none of the patients presented sich on ct within 24 h and they were randomly allocated to two groups : group a ( n = 72 ) received antiplatelet therapy 24 h after rt - pa for 10 days , independent of the presence of swi - detected mb or ht . 
the protocol include , dwi , axial fast spinecho ( fse ) with t1and t2 - weighted imaging , threeresonance dimensional time - of - ight magnetic radiol med ( 2014 ) 119 : 175182 angiography ( 3d - tof ) and axial ow - attenuated inversion recovery , and perfusion - weighted imaging ( pwi )  . 
the areas of hyperintensity on dw images were manually traced on each slice , summed and multiplied by the slice thickness and inter - slice gap to obtain the dwi lesion volume [ 21 ]  . denition of different kinds of haemorrhage mb was dened as punctate , homogeneous , rounded , hypointense lesions \0.5 cm in size on swi sequences [ 11 ]  . 
ph was dened as blood clots in the infarcted area with at least slight space - occupying effect . sich was dened as any signs of haemorrhage on followup scans associated with clinical deterioration c4 points on the nihss within 36 h [ 23 ]  . 
the modied rankin scale ( mrs ) [ 24 ] was used together with a semi - structured interview conducted either by telephone or in person to assess clinical outcome at 30 and 90 days after thrombolysis . 
all outcome variables ( favourable outcome , independent outcome , haemorrhage and death ) were assessed independently by physicians unaware of the patients initial stroke severity , time to treatment and imaging modality applied . 
a favourable outcome at day 90 was dened as a mrs score of 1 , and an independent outcome as a mrs score of 2 . statistical analysis after antiplatelet we predicted that favourable outcome at 90 days would be &80 % in group b ( swi - detected haemorrhage patients without thrombolysis ) therapy and &40 % in group a ( swi - detected haemorrhage therapy )  . 
we estimated that patients with antiplatelet 2025 swi - detected haemorrhage patients after thrombolysis in each group would need to be enrolled for the study to have a statistical power of 80 % with a two - sided alpha level of 0.05. 
this power was based on the ability to detect an absolute difference of 40 % in the nal favourable outcome at 90 days . data are presented as mean standard deviation . group comparisons were made using the mannwhitney u test for continuous variables and the fishers exact test for categorical variables . 
all statistical analyses were performed using the spss package , version 13.0 ( spss , chicago , il , usa )  . results demographic data , clinical outcomes and patient ow after thrombolysis of the 146 patients in groups a and b are shown in fig . 
nihss scores at baseline and 6 h after thrombolysis were signicantly worse in group b than in group a , and the hospital stay in group b was shorter than that in group a ( table 1 )  . 
there were no other signicant differences in age , sex , time to thrombolysis , affected hemisphere , nihss score at 24 h , 7 and 14 days 178 fig . 
conrmed diagnosis and differentiation are critical in making acute treatment decisions ; especially , in regard to patient eligibility for thrombolytic and antiplatelet therapy before and after rt - pa thrombolysis [ 25 ]  . this study was designed to evaluate the effect of swi for antiplatelet therapy on post - thrombolysis mb . 
nihss scores at baseline and 6 h after thrombolysis were signicantly worse in group b ( haemorrhage patients not receiving antiplatelet therapy ) than in group a ( haemorrhage patients receiving antiplatelet therapy ) , and hospital stay in group b was shorter than that in group a . 
in addition , the nihss scores at 7 , 14 days and mrs at 30 days after thrombolysis were signicantly lower in the haemorrhage patients in group b than in those in group a ; moreover , hospital stay was signicantly shorter and the rate of favourable outcome at 90 days after thrombolysis was signicantly higher ( table 2 ) in the haemorrhage patients not treated with heparin . a total of 22 ( 78.6 % ) of the 28 haemorrhage patients in group b at 90 days after thrombolysis had a favourable outcome ( mrs b 1 ) ; while 14 ( 63.6 % ) of the 22 haemorrhage patients in group a at 90 days after thrombolysis were moderately disabled ( 2 b mrs b 3 )  . 
although this was an institutional protocol that was not based on solid scientic evidence , the different effect on the patients neurological recovery in swi - detected haemorrhage patients in our two groups with and without antiplatelets conrmed the value of swi - based guidance for antiplatelet therapy after thrombolysis . some studies suggest mb is a potential marker of a haemorrhage - prone state [ 46 ] , and anecdotal case reports have described patients with mb who developed therapyrelated catastrophic post - ischaemic haemorrhage [ 14 ]  . 
in our study , the results demonstrated that mb , ht and ph could progress into each other if no appropriate treatment plan for rt - pa thrombolysis is available . 
the reason for the higher rate of mb is mainly attributed to the application of swi , which may be superior to t2 - weighted imaging in detecting mbs [ 1719 ]  . our study has several limitations : it was a prospective study , but it was not randomised or controlled . 
the mri or ct examinations were performed only in patients with sich or an increase of nihss scores c4 points after rt - pa thrombolysis so as to subsequently stop antiplatelet therapy that sich was detected . 
2 a 69 - year - old female patient from group a with acute ischaemic stroke for 120 min and a baseline nihss ( national institutes of health stroke scale ) score of 12 . 
a , e baseline diffusionweighted imaging ( dwi ) shows a slighter hyperintense area of the right basal ganglia , and susceptibility - weighted imaging ( swi ) shows the haemorrhage - free temporal lobe . 
b , f after 24 h of thrombolysis , dwi shows a mixed hyperintense area of the right basal ganglia , and swi shows the temporal lobe with blurred haemorrhagic transformation ( ht ) at the lateral part of the lenticular nucleus . 
c , g after 7 days of thrombolysis , dwi still shows a mixed hyperintense area of the right basal ganglia , and swi shows the temporal lobe with distinct ht . 
d , h after 14 days of thrombolysis , dwi shows a slighter hyperintense area with some microbleeds , as seen on relatively late for this examination and thus more difcult to identify mb or ht , which further delayed the patients neurological recovery , as occurred in the haemorrhage patients in group a . 
although detection of haemorrhage by mri at 6 and 24 h after rt - pa may be inconvenient , early accurate detection of haemorrhage and prompt treatment decisions according to swi play an important role for the patients neurological recovery . 
another study limitation was that mri scan times were obviously longer than those of ct . in conclusion , our results indicated swi was an effective approach for the guidance of antiplatelet therapy after thrombolysis . 
imaging , along with clinical and laboratory evaluation , is an important tool to reach a correct diagnosis and to provide a precise grading of disease progression , inuencing both clinical management and therapy . 
computed tomography ( ct ) demonstrates with a very high spatial resolution the tiny structural alterations of cortical and spongy bone before they become evident on plain lm radiographs . magnetic resonance imaging ( mri ) is the only modality that provides demonstration of bone marrow oedema , f . 
cimmino dipartimento di medicina interna , clinica reumatologica , universita` degli studi di genova , viale benedetto xv 6 , 16132 genoa , italy which reects vasodilatation and inammatory hyperaemia . 
the primary aim of this review article was to examine the involvement of the spine and sacroiliac joints in spa using a multimodal radiological approach ( radiography , ct , mri ) , providing a practical guide for the differential diagnosis of these conditions . keywords spondyloarthritis ( cid : 2 ) spine ( cid : 2 ) sacroiliac joints ( cid : 2 ) sapho ( cid : 2 ) ankylosing spondylitis introduction ( spa ) seronegative spondyloarthropathies represent a group of chronic articular inammatory diseases which differ from rheumatoid arthritis for the typical absence of rheumatoid factor in serum , and have in common several epidemiological , pathological , clinical and radiological features . 
the positivity for class i human histocompatibility leukocyte antigen ( hla ) b27 is related to a 20 - fold increased risk of developing a spa as compared to the general population [ 1 ]  . 
in 2005 , it was proposed to divide spa into ve subgroups [ 2 ] : ankylosing spondylitis , psoriatic spondyloarthritis , reactive spondyloarthritis ( reiters syndrome ) , ( related to inammatory bowel diseases such as crohns disease and ulcerative colitis ) and undifferentiated spondyloarthropathies . 
regardless of subgroup , the main clinical manifestations of spa include inammatory back pain ( mainly at night , which worsens with rest and improves with movement ) caused by sacroiliitis or inammatory involvement thoracic spine ; peripheral of the lumbar and / or distal arthritis ( often oligoarticular and asymmetric ) ; enthesitis and extra - skeletal manifestations , such as uveitis [ 3 ]  . 
with the development of more extensive and exible criteria by spondyloarthritis enteropathic radiol med ( 2014 ) 119 : 156163 the european spondyloarthropathy study group [ 3 ] , the sapho syndrome ( synovitis , acne , pustulosis , hyperostosis and osteitis ) may also be considered a spa , even though there is no general agreement in this regard . 
sapho syndrome and spa have in common many clinical and laboratory features , primarily seronegativity for rheumatoid factor and inammatory involvement of the axial skeleton , despite only a weak association with hla - b27 antigen having been identied for the sapho syndrome . 
in spa , the most characteristic targets of the autoimmune process are entheses , anatomical structures made up of brous or bro - cartilaginous tissue , which provide anchorage for tendons and ligaments to the bone surface [ 5 , 6 ]  . 
enthesitis is accompanied by the appearance of small erosions in the cortical bone , typically surrounded by subcortical reactive osteosclerosis ( osteitis ) , which can often prevail over bone reabsorption ; in the later stages osteoproliferation leads to the ossication of ligaments , tendons and joint capsules , and , eventually , to ankylosis [ 6 , nonhomologous including ankylosing spondylitis the incidence of ankylosing spondylitis , the archetype of spa , is between 0.1 and 2 % , and the age of onset is less than 30 years in 80 % of patients . 
the classic form ( primary or idiopathic ) must be distinguished from the secondary one , which can appear during the course of psoriasis or enteropathic arthritis [ 9 ]  . 
subchondral osteosclerosis decreases in the following stages , which are characterised by an increase in the fatty content of cancellous bone ( post - inammatory fatty conversion of bone marrow )  . 
the remnants of the joint space are sometimes visible as a thin sclerotic line on plain lm radiographs , which appears hyperdense on ct images [ 12 ]  . in the light of new and promising treatment options , such as anti - tnf ( tumour necrosis factor ) a agents , early diagnosis is of great clinical signicance . 
magnetic resonance imaging ( mri ) is the only imaging modality that may provide an early diagnosis , showing bone marrow oedema , which appears hypointense on t1 - weighted images and hyperintense on uid - sensitive stir ( short - tau inversion recovery ) or t2 - weighted images with fat signal suppression . 
gadolinium - enhanced fat - suppressed t1weighted images can help in the diagnosis by showing contrast enhancement of the subchondral cancellous bone and / or joint space [ 5 , 12 ]  . 
spinal involvement , which may be earlier , contemporary or subsequent to the onset of sacroiliitis , occurs with greater frequency at disco - vertebral junctions and at the level of interapophyseal and costo - vertebral includes enthesitis with bone erosion , post - inammatory fatty conversion of red bone marrow , osteosclerosis and osteoproliferation with ectopic bone formation . 
the enthesitis of the disco - vertebral junction , which occurs at the level of the anterior and posterior corners of vertebral bodies , is associated with erosions , resulting in the typical lesions of romanus . 
osteosclerotic foci develop at the site of corner erosions ( bright corners or shiny corners ) ; they progressively enlarge , causing the squaring of the endplates joints . 158 radiol med ( 2014 ) 119 : 156163 fig . 
a anteroposterior radiograph shows bilateral grade 3 sacroiliitis with diffuse subchondral sclerosis involving the iliac ( antero - inferior ) portion of both sacroiliac joints and widening of the joint space , which is more evident on the left side ( arrows )  . 
c axial ct scan shows bilateral grade 3 sacroiliitis with dense spongiosclerosis along the iliac side of sacroiliac joints ( arrows ) and some left - sided erosions ( small arrows )  . 
in advanced stages the ossication of vertebral ligaments may ( longitudinal , supraand interspinous ) occur , leading to ankylosis [ 5 , 19 ]  . the presence of symmetric syndesmophytes along the whole spine ( cervical spine is the last rachidian region to be leads to the characteristic bamboo spine involved ) appearance . 
in about 8 % of patients with ankylosing spondylitis an extensive inammatory involvement of the intersomatic disc and adjacent vertebral endplates may occur , the so - called andersson spondylodiscitis [ 20 ]  . 
on mri examination spondylodiscitis is characterised by a diffuse hypointense signal on t1 - weighted images involving the intersomatic disc and adjacent vertebral endplates . it appears hyperintense on uid - sensitive sequences and shows signicant enhancement after intravenous administration of gadolinium - based contrast agents [ 7 , 21 ]  . 
3 a , b 37 - year - old man with primary ankylosing spondylitis . a sagittal t2 - weighted and b corresponding t2 - weighted fatsuppressed magnetic resonance ( mr ) images show a focus of high signal intensity at the antero - superior corner of l1 body ( arrow in a and b ) , which is called shiny corner . 
unilateral asymmetric distribution and separation from the lateral aspect of the vertebral bodies are the main radiological features differentiating psoriatic from those of syndesmophytes ( para - syndesmophytes ) ankylosing spondylitis and spondylitis associated with inammatory bowel diseases . 
according to de vlam et al . [ 27 ] , the morphology of syndesmophytes is related to the degree of functionality of the spinal motion segment in which they develop . 
if the interapophyseal joints of this segment maintain a normal mobility , the tensile forces acting on the spine prevent the formation of linear and thin syndesmophytes , and the 160 radiol med ( 2014 ) 119 : 156163 fig . 
5 a , b pathological vertebral fracture in a 58 - year - old man with ankylosing spondylitis of 21 years duration after a minor trauma . a sagittal multiplanar reformation and b corresponding surfacerendered ct image clearly dene the through - and - through fractures ( arrows in a ) involving the anterior longitudinal ligament , intervertebral space , the spinous processes , the interand supraspinous ligaments . 
note the ossication of interspinous and supraspinous ligaments ( thin arrows in a and b ) and the fracture line on the latter ( arrowhead in a and b ) fig . 
a coronal multiplanar reformatted ct image shows subchondral bone sclerosis and multiple erosions involving the iliac aspect of the left sacroiliac joint associated with ( pseudo - ) widening of the joint space ( arrow )  . 
b coronal t2 - weighted fat - suppressed mr image demonstrates a large area of bone marrow oedema on the iliac aspect of the left sacroiliac joint ( asterisk )  . 
these ndings are typical of active sacroiliitis . c anteroposterior radiograph of the lumbar spine and d the corresponding coronal multiplanar reformatted ct image show a left - sided nonmarginal bulky syndesmophyte ( arrow in c and d ) ; its coarse and wavy appearance is different from the short and thin syndesmophyte of ankylosing spondylitis paravertebral ossication has a solid and coarse appearance ( non - marginal bulky syndesmophytes , or para - syndesmophytes ) ; on the contrary , reduced mobility of the interapophyseal joints leads to the development of thin and linear syndesmophytes . 
the authors [ 27 ] observed a direct relation between ankylosis of interapophyseal joints and the development of thin and linear syndesmophytes ( like those of ankylosing spondylitis ) ; on the contrary , they found coarse paravertebral ossication in cases where articular mobility was maintained . the main radiological ndings of psoriatic sacroiliitis , which may also occur in the absence of spondylitis , are : erosions , which are more frequent on the iliac portion of joint space narrowing , and , the joint , osteosclerosis , radiol med ( 2014 ) 119 : 156163 fig . 
7 a , b 52 - year - old man with crohns disease and sacroiliitis . a axial ct enterography image shows thickening and mural stratication with mucosal hyper - enhancement of an ileal loop affected by crohns disease ( arrow in a )  . 
note the total bony ankylosis of the right sacroiliac joint ( arrows ) and partial ankylosis ( thin arrow ) of the left sacroiliac joint rarely , ankylosis [ 28 ]  . 
interapophyseal joints of the cervical spine are frequently involved ( in contrast to what happens in the thoraco - lumbar spine ) , and they may eventually become ankylotic , while anterior atlo - axial subluxation is much more rare [ 29 ]  . reactive spondyloarthritis ( reiters syndrome ) the eponym reiters syndrome indicates a clinical syndrome characterised by conjunctivitis , urethritis or gastroenteritis , followed by the onset of aseptic arthritis after an interval of 14 weeks . 
according to this theory , an infection of the conjunctival , intestinal or urethral - genital mucosa may represent the trigger for a systemic autoimmune reaction which determines an aseptic inammatory process involving the axial skeleton or appendicular joints . the involvement of the appendicular skeleton is typically represented by asymmetrical oligoarthritis , often unilateral , which shows a predilection for the large synovial joints of the lower limbs [ 30 , 31 ]  . 
the involvement of the sacroiliac joints is frequent ( 510 % in the early phase , up to 4060 % in the advanced stages ) and has the same radiological features of psoriatic sacroiliitis [ 30 ]  . 
in fact , a typical early nding is represented by coarse syndesmophytes , which are not distinguishable from those of psoriasis and are located most frequently at the level of the lower three thoracic and the upper three the interapophyseal involvement of lumbar vertebrae . joints is associated with erosions , osteosclerosis and ankylosis , but these ndings are less frequent than those observed in ankylosing spondylitis [ 31 ]  . enteropathic spondyloarthritis ( enteroarthritis ) often transient asymmetrical , enteropathic spondyloarthritis , or enteroarthritis , related to the two major chronic inammatory bowel diseases , ulcerative colitis and crohns disease , of which they are considered extraintestinal manifestations . 
with regard to axial arthritis , the incidence of sacroiliitis varies from 10 to 20 % , while that of spondylitis from 7 to 12 % [ 33 ]  . 
in a recent study [ 34 ] , the review of 221 ct enterography examinations of patients with histologically conrmed crohns disease showed a prevalence of sacroiliitis ( up to 24 % ) higher than that of the other extraintestinal manifestations . 
radiological features of both spondylitis and sacroiliitis are closely similar to those of primitive ankylosing spondylitis [ 35 ]  . sapho syndrome the acronym sapho was rst used by charmot et al . 
according to the more widely accepted pathogenetic hypotheses , sapho syndrome has been considered a reactive osteitis , which in genetically predisposed represents the consequence , 162 radiol med ( 2014 ) 119 : 156163 fig . 
8 ae 24 - year - old man with palmoplantar pustulosis and low back paa sagittal t1 - weighted , b t2 - weighted fat - suppressed , and c contrast - enhanced t1 - weighted fat - suppressed mr images of the lumbar spine show two signal alterations at the level of the anterosuperior corners of l4 and l5 vertebrae ( arrows in a , b and c )  . 
d axial t2 - weighted fat - suppressed mr image passing through l5 body conrms the corner lesion ( arrow ) and e the corresponding axial ct scan clearly demonstrates the corner erosion of the vertebral endplate surrounded by spongiosclerosis ( arrow ) individuals , of a nonspecic and inadequate immune response , triggered by infection with some microorganisms [ 37 ]  . 
sapho is currently considered a rare disease with an incidence of 1 in 10 , 000 individuals , although this gure probably underestimates the real incidence of the disease , because of the wide spectrum of clinical manifestations and the lack of valid diagnostic criteria . 
the syndrome shows a slight preference for females with a mean age at diagnosis of 28.6 years , and a chronic relapsing and remitting course . many clinical features of sapho syndrome , including involvement of the axial skeleton and entheses , seronegativity for rheumatoid factor , and the association with some varieties of psoriasis and enteroarthritis , suggest a link with spa , even if a signicant correlation with histocompatibility antigen hla - b27 has not yet been clearly demonstrated [ 38 ]  . 
according to the criteria dened by kahn et al . [ 39 ] , sapho syndrome should be suspected in patients with pustular skin lesions and musculoskeletal pain caused by an osteoarticular aseptic inammation . 
the bone involvement concerns mainly the sterno - costo - clavicular region ( 7090 % ) , the spine ( 30 % ) and the sacroiliac joints ( 1352 % ) [ 38 ]  . 
franchi department of pathology , university of florence , florence , italy patients underwent wide excision ( 32 out of 38 ) and ve patients had marginal surgery ; only one patient underwent amputation . 
at the time of our analysis 13 patients ( 34.2 % ) had died due to metastatic spread of the disease . in our series , dfs in relation to distant metastases ( dm ) showed a signicant result for lower limb involvement ( p = 0.038 ) and marginal excision ( p = 0.024 ) , both predictors of a worse dfs , histology was statistically signicant although it was not possible to evaluate the risk for specic histology due to the small number of events in the different subtypes . conclusions the results obtained from our study are encouraging with regard to the feasibility and efcacy of preoperative rt in the treatment of soft tissue sarcoma in view of the results obtained in terms of local control , limb sparing and safety . keywords neoadjuvant ( cid : 2 ) chemotherapy ( cid : 2 ) radiation ( cid : 2 ) chemoradiation ( cid : 2 ) soft tissue sarcoma introduction soft tissue sarcomas ( sts ) are rare malignant neoplasms that originate from mesenchymal cells that can differentiate into different types of connective tissues . 
local management of sts usually consists of surgery combined with radiotherapy ( rt )  . for many years local excision of the tumour with postoperative rt was a well - established treatment approach providing good local control and acceptable 196 radiol med ( 2014 ) 119 : 195200 functional outcome [ 2 , 3 ]  . 
in the case of bulky disease or tumours located in critical areas , neoadjuvant rt with or without chemotherapy is employed to improve the chance of limb sparing , local control and functional outcome [ 4 ]  . neoadjuvant rt has the advantage of delivering a lower total dose and involving a smaller target volume than postoperative rt , and this results in less brosis and tissue damage and a theoretically better functional outcome [ 5 ]  . on the other hand , the preservation of function could be impaired due to the higher incidence of wound complications after preoperative rt [ 68 ]  . 
in high - grade sts , the risk of developing distant metastases increases with the increasing tumour size , reaching about 58 % in 15.120 cm lesions [ 9 ]  . 
the aim of our study was to evaluate disease - free survival ( dfs ) , overall survival ( os ) and toxicity of patients who underwent preoperative rt for soft tissue sarcoma . materials and methods neoadjuvant chemo - radiation our study analysed the data of 38 consecutive patients affected by soft tissue sarcoma . 
patients younger than 18 years at diagnosis , histological diagnoses of ewings sarcoma , rhabdomyosarcoma , desmoid tumours , dermatobrosarcoma protuberans , previously irradiated patients or with recurrent disease were not considered eligible for the study . clinical stage was dened according to the enneking surgical staging system for musculoskeletal tumors [ 10 ]  . tumour size , calculated on the major axis of the lesion , was measured on clinical evaluation and conrmed by preoperative imaging . 
before treatment 32 patients underwent a diagnostic magnetic resonance imaging ( mri ) study and 6 of them a computed tomography ( ct ) scan to dene tumour size and extension ; all patients underwent chest ct or radiogram for staging . 
to dene the histological characteristics of the tumour all patients underwent a biopsy , 32 ( 94.7 % ) received an incisional biopsy , 2 an excisional one . preoperative chemotherapy was administered concurrently with rt in the event of high - grade neoplasm , prognostically unfavourable histology , and bulky primary tumour : it consisted of two cycles of epirubicine ( 60 mg / m2 for days 12 ) and ifosfamide ( 1 , 800 mg / m2 for days 15 )  . nrt was performed with 3d conformal technique delivering 2 gy fractions up to total dose of 50 gy . 
at pathological assessment , margin status was assigned using the criteria of enneking [ 10 ]  . histological grade was classied by fcnlcc ( federation nationale des centres de lutte contre le cancer ) fourtiered system ( grades i to iv ) [ 11 ]  . 
occurrence of late toxicity was recorded all along the follow - up period and classied according to the rtog ( radiation therapy oncology group ) toxicity scale . statistical analysis the end of rt was used as the start of observation for the survival analyses . 
stage iii disease predicted a worse prognosis than lower stages , even though this difference did not reach statistical signicance ( p = 0.10 ) at univariate analysis , probably as a result of the small number of events among stage i patients . 
chemotherapy did not reach any signicant value in terms of reducing distant metastases in sarcoma patients . at multivariate analysis , the main independent dm predictors were stage iii and marginal surgery ( table 3 )  . regarding treatment tolerance , acute skin toxicity was mild : only two patients experienced grade 2 toxicity . 
in a recent survey , the choice of a neoadjuvant treatment was shown to be not only inuenced by well - dened treatment volume , increased acute morbidity and decrease in late morbidity but also mostly by specialty and clinical experience or institutional preferences , resulting in lack of clear consensus on eligibility criteria for preoperative treatment [ 15 ]  . 
expected benets from preoperative rt consist of dose reduction with respect to postoperative rt , with a better functional outcome [ 16 ] , narrower treatment elds allowed by lack of surgical contamination , shrinking of tumour boundaries that facilitates resection , and the formation of capsular brosis potentially preventing intraoperative tumour scattering [ 5 , 17 ]  . 
we reported data from 38 consecutive patients who underwent preoperative radiation treatment for soft tissue sarcoma at our institution . local control was achieved in 36 ( 95 % ) of cases , with 2 patients ( 5 % ) showing in - eld relapse . 
in our review , we found that dfs was signicantly inuenced by surgical margins status , histology and tumour site . in sts management , several studies underline the impact of negative surgical margins in predicting the clinical outcome [ 2022 ]  . 
three patients ( all with positive margins ) experienced local failure as rst relapse ( two isolated , one with distant failure ) , and two additional patients ( all with margin \1 mm ) had late local failure after distant metastasis . 
the authors concluded that no local recurrences were observed with surgical margins equal or larger than 1 mm , and it these may be adequate for patients with appears that extremity sts treated with preoperative rt [ 23 ]  . 
sts are heterogeneous diseases , and some histological subtypes can differ in the natural tumour history and prognosis : for example , well - differentiated liposarcomas are considered low - grade tumours owing to the low incidence of distant recurrence , whereas pleomorphic liposarcomas have a poor prognosis [ 28 ]  . 
a strong clinical interest therefore guides the choice of more aggressive treatment approaches depending on the histological type . at the time of our analysis , 13 patients had died due to metastatic spread of the primary disease . 
 [ 29 ] in a retrospective series of 112 cases including surgery alone ( sa ) ( n = 36 ) , ncrt ( n = 39 ) , and neoadjuvant radiotherapy ( nrt ) ( n = 37 ) reported that ncrt did not improve the rate of margin - negative resections over sa or nrt . locoregional relapse - free survival , distant metastasesfree survival , and overall survival ( os ) were not different among the treatment groups . 
patients with relapsed disease ( or 11.6 ; p = 0.01 ) and tumour size greater than 5 cm ( or 9.4 ; p = 0.01 ) were more likely to have a locoregional recurrence on logistic regression analysis . the eortc 62874 trial is the only randomised clinical study that investigated the role of neoadjuvant chemotherapy for the treatment of high - risk soft tissue [ 30 ]  . 
at a median follow - up of 7.3 years no large benet was shown for preoperative chemotherapy , and the chemotherapy group had a slightly higher 5 - year dfs rate and overall survival than the surgery group but the study was not powered for statistical signicance due to slow patient accrual . 
the data for neoadjuvant chemotherapy are still few and controversial , and this is due to the difculty in performing large , randomised trials for a rare disease such as soft tissue sarcoma . 
new drugs such as biological approaches have to be investigated . acute treatment tolerance was generally excellent , even though six patients ( 15.8 % ) had wound complications ( ve cases of wound dehiscence and one of stula ) , with only two requiring minor surgical procedures . 
the multitumours with a limb - salvage modal management of approach could favour impaired wound healing in the postoperative period and the occurrence of long - term complications [ 3133 ]  . 
although preoperative treatment is associated with an increased risk of major wound complications in the order of 35 % [ 31 ] , local anatomy and tumour size are important prognostic factors for acute complications [ 24 , 34 , 35 ]  . the results obtained in our study are encouraging with regard to the feasibility and efcacy of preoperative rt in terms of local control , limbs sparing and safety . conict of interest daniela greto , lorenzo livi , calogero saieva , pierluigi bonomo , icro meattini , mauro loi , lucia di brina , giovanni beltrami , domenico campanacci , guido scoccianti , rodolfo capanna , monica mangoni , fabiola paiar , alessandro franchi , giampaolo biti declare no conict of interest . radiol med ( 2014 ) 119 : 195200 retrospective comparative evaluation of disease outcome . 
al yami a , grifn am , ferguson pc et al ( 2010 ) positive surgical margins in soft tissue sarcoma treated with preoperative radiation : is a postoperative boost necessary ? int j radiat oncol biol phys 77 : 11911197 21 . 
davis am , osullivan b , bell rs et al ( 2002 ) function and health status outcomes in a randomized trial comparing preoperative and postoperative radiotherapy in extremity soft tissue sarcoma . 
curtis kk , ashman jb , beauchamp cp et al ( 2011 ) neoadjuvant chemoradiation compared to neoadjuvant radiation alone and surgery alone for stage ii and iii soft tissue sarcoma of the extremities . 
davidge km , wunder j , tomlinson g et al ( 2010 ) function and health status outcomes following soft tissue reconstruction for limb preservation in extremity soft tissue sarcoma . 
livi l , santoni r , paiar f et al ( 2006 ) late treatment - related complications in 214 patients with extremity soft - tissue sarcoma treated by surgery and postoperative radiation therapy . 
tseng jf , ballo mt , langstein hn et al ( 2006 ) the effect of preoperative radiotherapy and reconstructive surgery on wound complications after resection of extremity soft - tissue sarcomas . ann surg oncol 13 : 12091215 35 . 
the ss and sr were assessed and the results were expressed in terms of sensitivity , specicity , positive predictive value ( ppv ) and negative predictive value ( npv )  . 
simonetti dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , fondazione policlinico universitario tor vergata , viale oxford 81 , 00133 rome , italy e - mail : ire.coco@hotmail.it keywords thyroid nodules ( cid : 2 ) elastography ( cid : 2 ) strain ratio ( cid : 2 ) stiffness score ( cid : 2 ) fnac introduction thyroid nodules are frequently encountered clinically . 
the incidence increases in direct proportion to age , and is greater in women with an f / m ratio of 4 : 1 , in geographic areas with iodine deciency as well as following exposure to ionising radiation [ 1 ]  . although the incidence of thyroid carcinoma is estimated at around 4 / 100 , 000 individuals / year , it should be noted that the majority of thyroid nodules are benign ; in fact , it is known that the percentage of carcinomas in palpable nodules is only 4 % and rises to 8 % if we consider the various surgical series [ 2 ]  . 
therefore , the main objective of the evaluation of thyroid nodules is to exclude malignancy [ 3 ]  . the rigidity of nodular thyroid tissue is considered an important indicator of malignancy . 
elastosonography ( es ) is a newly developed method that provides information on parenchymal elasticity by colour coding the different degrees of mechanical - elastic deformation suffered by the structures being analysed in response to radiofrequency pulses ( rf )  . 
this new ultrasound method therefore aims to provide a real - time noninvasive characterisation of tissue during the same session as conventional ultrasound imaging and without takes advantage of the different mechanical properties of the various tissue components and the loss of the physiological elasticity in many diseases . 
it 150 radiol med ( 2014 ) 119 : 149155 the vascularity of each nodule was assessed by power doppler ( pd ) and classied as : no ow ( pattern i ) , predominantly peri - nodular ow ( pattern ii ) , intra - nodular and peri - nodular ow ( pattern iii )  . elastosonography the es study was carried out together with conventional ultrasound . 
use of the iu22 philips system and probe provided repeatable and nonoperator - dependent measurements since axial compression is applied automatically by the probe and not manually by the operator . deformation of the structures was achieved with mechanical compression obtained by the emission of lowfrequency pulses [ 7 ]  . during the examination , the system calculates the levels of resulting tissue deformation and displays them as a green and grey bar ( feedback bar ) on the side of the image . the bar indicates an appropriate ( green ) or inappropriate ( grey ) tissue deformation in order to obtain a good - quality elastograthe bar displays the tissue deformation in real time , and if the extent of the deformation is excessive the system does not show the corresponding elastography image . 
the data obtained were processed using dedicated q - lab software which employs a suitable algorithm to assess the degree of tissue distortion . in a very short time , the system processes the information coming from the lesion in the form of rf pulses . 
this information is obtained using the normal ultrasound probe and applying a vertical compression to the tissues ; compression can be obtained manually or automatically by the probe , as done in our study . 
this way , the tissues undergo varying degrees of deformation in relation to their elasticity , and return different signals . in recent years , the value of this technique has been demonstrated in the diagnosis of breast nodules , prostate cancer and liver brosis . 
more recently , this method has been proposed for the characterisation of thyroid nodules , and many authors have investigated the usefulness of this method based on the analysis of qualitative colour data [ 5 , 6 ]  . 
this parameter , by exploiting the difference of the elastic coefcients , allows for quantication of the stiffness of the nodule in comparison to the surrounding healthy parenchyma , by studying the deformation ratio ( sr - strain ratio )  . the aim of our study was to determine the diagnostic accuracy of es in the differential diagnosis of thyroid nodules , by means of a qualitative and quantitative evaluation . materials and methods study population the retrospective single - centre study was conducted between december 2010 and march 2012 . 
2 colour score of the thyroid nodules for increasing degree of stiffness ( score 1 for elastic nodules ; score 2 and 3 for intermediate stiffness and score 4 for anelastic nodules ) fig . 
this cut - off value was dened through the analysis of receiver operating characteristic ( roc ) curves in order to maximise the sum of the specicity and sensibility . fine - needle aspiration cytology and histological evaluation all nodules underwent us - guided ne - needle aspiration cytology ( fnac ) , after approval by the local ethics cominformed consent . mittee and obtaining the patients 152 sampling was performed using 21 - gauge needles with a 10 - ml syringe ; the material collected and prepared with the thin - prep method was sent to the medical pathologist together with a statement containing the patients data , the clinical question , the characteristics of the aspirate , and the number of samples taken for each nodule . the results of the cytological study were classied into ve categories , indicated by the abbreviation tir ( siapec consensus review , 2007 ) : tir 1 : nondiagnostic ( inadequate ) ; tir 2 : negative for malignant cells ( benign ) ; tir 3 : indeterminate ( follicular proliferation ) ; tir 4 : suspicious for malignancy ; tir 5 : positive for malignant cells . patients with indeterminate or suspicious for malignancy cytology underwent surgical treatment ; the surgical specimen was subjected to histological analysis to determine the nature of the lesion . statistical analysis continuous variables ( real numbers ) were expressed as mean and standard deviation and discrete variables ( natural numbers ) as number and percentage . 
roc curves were also used to extrapolate the optimum cut - off value for sr . cytological analysis , combined with histological analysis , was used to determine the benignity and malignancy of nodules . 
overall , the cytological and histological analysis revealed 316 benign nodules and 52 malignant nodules . b - mode and power doppler ultrasound the demographic and ultrasonographic characteristics of the study population are shown in table 1 . 
therefore , the differential diagnosis of nodules is crucial to allow the early diagnosis of cancers and ensure appropriate treatment . currently , thyroid ultrasound is the rst - line examination for the identication and follow - up of nodules since it makes it possible to formulate a suspicion of malignancy and select the nodules to be subjected to fnac ( table 4 )  . cytological evaluation is considered the most accurate diagnostic technique [ 9 ]  . 
however , it has two limitations : nondiagnostic results due to inadequate cytology sampling and the presence of follicular proliferation or hartle cells . fnac is also reserved for nodules with a maximum diameter exceeding 10 msmaller nodules are not subjected to fnac unless they show suspicious ultrasonographic features and ow . follicular proliferation or in the presence of hartle cells , cytology does not differentiate adenoma from carcinoma , as the differential diagnosis is based on the presence of capsular or vascular invasion , which can only be evaluated histologically after thyroidectomy . in the case of elastosonography allows for noninvasive , real - time tissue characterisation which provides additional information to b - mode and power doppler ultrasound . 
although sonographic and doppler features are the criteria taken into consideration for fnac performance and allow an accurate identication and follow - up of thyroid nodules , they do not contribute signicantly to their characterisation , which requires cytological evaluation . on this basis , our study compared the information provided by ultrasound and es with the cytological diagnosis achieved by fnac in on a cohort of patients with a sonographic diagnosis of thyroid nodules . the es technique made it possible to evaluate the mechanical - elastic properties of tissues , and in particular the stiffness of the nodules analysed . 
stiffness was analysed in terms of colour map ( ss ) and by comparison with the stiffness of the surrounding healthy parenchyma , by calculating the deformation ratio ( sr )  . 
the results obtained proved to be superior to those of conventional ultrasound . in fact , although the typical ultrasonographic features of malignancymicrocalcications ( p = 0.003 ) and vascularity pattern iii ( p = 0.0016 ) were signicantly present in malignant nodules , with sensitivity of 27 and 63 % and specicity of 96 and 80 % , respectively , degree of malignancy was more strongly correlated with analysis of the es colour scores ( p = 0.0002 ) , reaching 91 % sensitivity and 68 % specicity . the nding of 104 false - positive results , represented by scores c3 , with a ppv of 27 % , indicates an important limitation of this technique and requires caution in drawing conclusions . from another point of view , it should be emphasised that score 1 was found in benign lesions only , with 98 % npv . 
this nding , if conrmed in a larger study , may exclude immediate recourse to fnac , which would be reserved for nodules showing a change in size or morphology over time . with regard to the calculation of the sr , the signicant values reported in recent studies were not reached [ 1012 ] in discriminating benign from malignant forms . 
however , although our case series was limited , it was still possible to the presence of higher values in malignant highlight nodules . a limitation of our study is the failure to assess intraand interobserver variability in both the qualitative and quantitative indexes . in agreement with the research published to date , our study conrmed that the benets of es are many : it is easy to perform , fast , accurate and reproducible ; it provides a qualitative assessment of tissue elasticity in real time ; it provides a semiquantitative evaluation of the sr ; increases the sensitivity , specicity and npv of conventional ultrasound in the diagnosis of thyroid cancer ; it can potentially help to select patients requiring invasive diagnosis ( fnac ) , thus lowering the costs for further investigations . conclusions currently available knowledge indicates that es is a complementary tool in the diagnosis of thyroid cancer , as it radiol med ( 2014 ) 119 : 149155 can complement conventional ultrasound for the identication and follow - up of thyroid nodules . 
we believe that es can be used as an additional imaging method in the differential diagnosis of nodular thyroid disease , since its values has been documented particularly in combination with sonographic features and vascularity . moreover , considering the absence of false - negatives in our study , es could be an alternative in the differential diagnosis in the case of nondiagnostic fnac , in nodules that do not meet the criteria for performing fnac ( e.g. , maximum diameter \10 mm ) , or in the case of technical difculties in fnac execution . compared to es with free - hand compression , the method used in our study has shown certain advantages . 
to evaluate whether these indices may be determinants of success in prosthetic surgery for stress urinary incontinence , we conducted a retrospective study of patients treated with tension - free vaginal tape - obturator ( tvt - o ) surgery and assessed , by measuring the pubourethral distance and angle after tvt - o , whether there was any quantitative difference between the mean values measured in the group of cured patients and uncured patients . materials and methods we selected 51 patients who underwent tvt - o and evaluated the failure rate by means of urogynaecological assessment . 
schettino department of gynaecology , obstetric and reproductive science , second university of studies of naples , largo madonna delle grazie 1 , 80100 naples , italy e - mail : mt.s76@libero.it introduction the mechanisms of urinary continence is ensured by the coexistence of several morphological and functional factors which guarantee regular micturition in its two phases of bladder lling and voiding . 
more specically , these factors are detrusor stability , anatomical and neurovascular integrity of the urethra [ 1 ] , adequate competence and tone of the external urethral sphincter , optimal functional synergy between the pelvic and urogenital diaphragm , and the presence of adequate oestrogen levels . 
stress urinary incontinence ( sui ) is dened by the international continence society ( ics ) as a pathological condition characterised by involuntary urine loss during a rise in intra - abdominal pressure in the absence of detrusor contraction [ 2 ]  . 
the incidence of sui is rising in part as a result of the higher average age of the female population and of the associated risk factors that exasperate the condition , with a signicant impact on daily life due to both incontinence episodes and greater susceptibility to urinary tract infections [ 3 , 4 ]  . in view of the extent of the problem and of the fact that it also affects young women and , to a lesser extent , even young athletes [ 5 ] , in recent decades the treatment of sui has represented one of the most interesting areas of research in the urogynaecological eld . 
evidence that in most cases the defect underlying sui is urethral hypermobility in addition to an intrinsic sphincter deciency induced specialists to look for minimally invasive surgical techniques capable of restoring and preserving a correct urethral axis , allowing adequate dynamic closure of the urethra during exertion . 
for these reasons , the introduction of midurethral slings has revolutionised stress incontinence surgery , becoming the gold standard in the treatment of sui . since the advent over 10 years ago of the rst retropubic midurethral sling , tension - free vaginal tape ( tvt ) , many 190 radiol med ( 2014 ) 119 : 189194 attempts have been made to increase the success rate of these devices by reducing the risk of complications . 
to this end , in 2001 delorme introduced the rst trans - obturator sling ( tvt - o , tension - free vaginal tape obturator ) , which , by involving a trans - obturator approach and avoiding the retropubic space , reduced the risk of vesical , intestinal and vascular lesions , even though the success rates are slightly lower than those of tvt [ 69 ]  . 
success is intended as the restoration of a physiological urethral mobility guaranteeing continence even in the presence of a rise in intra - abdominal pressure . an ability to quantify the degree of urethral mobility by means of imaging modalities would therefore make it possible not only to recognise the exact type of anatomical defect but also to quantify it and rationally stratify the different treatments available , with a view to selecting the most appropriate treatment and optimising the results . urethral mobility is currently evaluated in a general manner using the q - tip test , but the need to standardise this evaluation is becoming increasingly clear , and the international continence society recommends and encourages research aimed at developing diagnostic techniques for the objective assessment of urethral mobility . 
to this end , the introduction of perineal ultrasound in the diagnostic workup of sui is being intensely discussed , as it has shown to be the most sensitive examination for evaluating urethral mobility . 
the technique , in fact , enables measurement of the pubo - urethral distance and angle both under exertion and at rest . the aim of this study was therefore to evaluate whether the degree of urethral mobility can be a determinant of success of a minimally invasive prosthetic procedure . 
a retrospective study of all patients treated with tvt - o for pure sui was conducted to establish whether there was a quantitative difference in the pubo - urethral distance and angle between the group of patients successfully cured with tvt - o and the group of patients with persistent sui despite tvt - o placement . materials and methods the study was approved by our departments ethics committee and informed consent was obtained from all the patients enrolled in the study . we selected 51 patients [ mean age 54.3 ( 3 ) years ] who underwent a tvt - o procedure ( tvt - o ethicon ) between january 2006 and january 2011 to correct urethral hypermobility and restore urinary continence [ 7 ]  . 
we included only patients with a preoperative diagnosis of severe pure sui with no symptoms of urgency , no genital organ prolapse or with mild cystocoele , with a body mass index ( bmi ) of exclusion criteria were age greater 18.5 kg / m2 , parity of 2 or less , no history of pelvic surgery , and no associated chronic respiratory or metabolic disease . than 60 and \48 years , bmi greater than 26 kg / m2 , urge incontinence , hyperactive bladder or detrusor instability , pelvic organ prolapse , previous pelvic surgery , parity [ 2 , previous or current oestrogen therapy , and associated chronic respiratory or metabolic diseases . following tvt - o each patient underwent urogynaecological history and clinical assessment , inclusive of urogynaecological examination , voiding diary , q - tip test , stress test , urodynamic assessment ( cystomanometry , uroowmetry , pressure - ow test ) and perineal pelvic ultrasound . 
the ultrasound examination included a static and dynamic assessment of urethral mobility . the rst goal was to establish the success rate of the tvt - o procedure , dening cure as the total absence of urine leakage on exertion . 
to this end , we divided the patients into two groups : group a , patients cured following tvt - o ; group b , patients with persistent sui after tvt - o . having dened the success rate , we evaluated whether there was any difference in the measurementsboth static and dynamicof the pubo - urethral distance and angle between group a and group b . the pubo - urethral distance represents the line joining the pubis and the midpoint of the urethra . 
reference values for women aged 4860 years are 85.50 ( cid : 3 ) 8.94 ( cid : 3 ) at rest and 105.20 ( cid : 3 ) 10.16 ( cid : 3 ) under stress , as demonstrated by di pietto et al . 
patients were imaged with a half - full bladder ( 250 cc ) so as to avoid excessive lling that might collaboration in performing a valsalva affect their the measurements [ 11 , 12 ]  . 
the manoeuvre and alter examination was conducted with the patient in dorsal lithotomy position and using a 3.5 - mhz convex probe ( volusonr 730 expert , general electric ) , placed longitudinally to the vulvar orice and slightly tilted upwards . 
this position of the probe also allowed for midsagittal scans through the anterior perineum [ 13 , 14 ]  . the pubic bone appears as an oval image surrounded by a regular wrapping ( curved ligament ) , on the left of the screen . the transonic longitudinal structure in the middle of the screen is the urethra , above which are the bladder and , more superior , the uterus . 
the pubic bone is the only xed structure within the eld of observation and is therefore used as a landmark for measuring the pubic - urethral distance and angle [ 15 ]  . 
in the dynamic phase , the increase in intra - abdominal pressure was achieved through coughing and the measurement was obtained on a still image generated at the time of maximum abdominal pressure thanks to the use of the cine - loop technique ( ability to memorise and reproduce images )  . 
it should be noted that the valsalva manoeuvre is not standardised so diagnostic sensitivity is not only operator dependent but also inuenced by the patients ability to cooperate in achieving a valid increase in intra - abdominal pressure . statistical analysis the data are presented as mean and standard deviation . 
this was found to be 10 % , that is , persistent sui after tvt - o was seen in ve patients ( group b ) , whereas the other 46 patients were completely cured ( group a )  . 
7 inclination angle of urethral axis under stress in recurrent ius post tvt - o ( p pubic bone , b bladder , u urethra ) radiol med ( 2014 ) 119 : 189194 discussion in the work - up of patients with pelvic oor dysfunction it is fundamental to obtain an in - depth evaluation of any defects in the individual structures that contribute to the anatomical and functional integrity of the pelvic oor , with a view to dening the most appropriate surgical approach . 
perineal ultrasound , in particular , is the most commonly used technique thanks to ease of use , lack of invasiveness and low cost . ultrasound generally allows for an evaluation of all the anatomical structures making up the pelvic oormuscular components , recesses , and pelvic organs ; more specifically , the perineal approach allows the identication of any qualitative and quantitative abnormalities affecting the structures involved in guaranteeing urinary continence [ 1618 ]  . 
according to the literature , the results of perineal ultrasound demonstrate a close correlation among a diagnosis of sui , bladder neck funnelling and hypermotility of the urethrovesical junction [ 19 , 20 ]  . moreover , this examination also permits a targeted preand postoperative assessment to provide a precise , repeatable and objective index of surgical outcome . 
patients with complex disorders following surgery for stress incontinence or incontinence due to pelvic organ prolapse [ 21 ] should , in fact , undergo ultrasound to study the position of the tape and / or mesh in relation to the urethra and pelvic organs [ 22 , 23 ]  . 
many studies have conrmed the failure of sling insertion techniques , using ultrasound to measure the quantitative reference indices ( pubo - urethral distance and angle ) [ 24 ]  . 
perineal ultrasound therefore represents a useful technique in the diagnosis and follow - up of sui patients who have undergone a sling - placement procedure . starting from these premisses , we carried out perineal ultrasound in all women treated with tvt - o for severe sui , so as to assess whether there was any parameter that might serve as an indicator of surgical failure . 
this suspicion stemmed from the fact that all women had similar preoperative characteristics , had no risk factors associated with treatment failure and had all been operated on by the same surgeon who was highly experienced in the technique . the rst assessment aimed at establishing whether the sling was in the correct position and well suspended , and all patients , both cured and uncured , showed a well - positioned sling . 
we then evaluated the pubo - urethral indices , and found that the mean values of pubo - urethral distance and angle were higher in the group of patients with persistent sui compared to those in cured patients . the nding of a well - positioned sling even in the case of treatment failure and the evidence of greater pubo - urethral angles and distances in uncured women suggests that these patients may have had higher values of both pubo - urethral indices already before sling placement and that therefore the suspension achieved with the trans - obturator technique was inadequate to reduce pubo - urethral angles and distances strongly deviating from the physiological values . this means that very probably , if we had subjected all patients undergoing tvt - o to preoperative perineal ultrasound , we would have realised that the treatment had been successful in the patients with preoperative pubourethral indices closer to what we considered to be the the success of physiological values . 
this suggests that trans - obturator sling placement decreases in proportion to the increase in the mean pubo - urethral distance and angle . confronted with these ndings , we considered whether there had been some evaluation error in selecting tvt - o in cases of failure and whether the classic tvt technique might have ensured complete cure in these patients . this hypothesis is based on the fact that , by producing a greater degree of tension compared to the trans - obturator approach , the retropubic approach may succeed in restoring normal ranges of pubic - urethral indices even when these are considerably increased [ 10 ]  . 
should this be true , it would mean that perineal ultrasound with determination of the pubo - urethral distance and angle should become a necessary diagnostic step for selecting the most appropriate sling - placement technique for sui correction [ 10 , 25 , 26 ] , and one to be included in the diagnostic work - up of patients with pelvic oor dysfunction . for this hypothesis to be conrmed , larger case series are required as are new , prospective studies allowing comparison of preand postoperative pubo - urethral values to dene whether and to what extent these values inuence the likelihood of success of a specic minimally invasive slingplacement procedure for the treatment of sui [ 10 , 24 ]  . conclusions our data show that patients with persistent sui after tvto have a mean pubo - urethral distance and angle greater than those in women with successful treatment . 
rossi sara seitun giulio bovio umberto valente received : 7 august 2012 / accepted : 2 october 2012 / published online : 20 december 2013 ( cid : 2 ) italian society of medical radiology 2013 abstract purpose this study was undertaken to evaluate primary stenting in patients with inferior vena cava torsion after orthotopic liver transplantation performed with modied piggyback technique . materials and methods from november 2003 to october 2010 , six patients developed clinical , laboratory and imaging ndings suggestive of caval stenosis , after a mean period of 21 days from an orthotopic liver transplantation performed with modied piggyback technique . 
all patients were treated with primary stenting followed by in - stent angioplasty in three cases . results in all patients , the stents were successfully positioned at the caval anastomosis and the venous gradient pressure fell from a mean value of 10 to 2 mmhg . 
valente dipartimento di chirurgia addominale e dei trapianti dorgano , irccs azienda ospedaliera ed universitaria san martino , ist - istituto nazionale per la ricerca sul cancro , largo rosanna benzi 10 , 16132 genoa , italy conclusions primary stenting of inferior vena cava stenosis due to torsion of the anastomoses in patients receiving orthotopic liver transplantation with modied piggyback technique is a safe , effective and durable treatment . keywords orthotopic liver transplantation ( cid : 2 ) torsion ( cid : 2 ) inferior vena cava ( cid : 2 ) stent introduction orthotopic liver transplantation has become the treatment of choice for patients suffering from end - stage liver disease . 
the piggyback technique for orthotopic liver transplantation , rst performed by calne and williams [ 1 ] , is an alternative surgical technique that has gained increasing popularity , especially with the advent of paediatric transplants , living donors and other split liver transplantation techniques [ 2 ]  . 
the main advantages of the piggyback technique are the fact that the blood return from the inferior vena cava is maintained during the anhepatic phase , with a signicant increase in haemodynamic stability , reduced cold ischaemia times , less kidney damage and no need for the veno - venous bypass [ 3 , 4 ]  . 
the main complications of the anastomoses between the inferior vena cava and suprahepatic veins may arise in the postoperative period , mainly due to technical factors , torsion or compression of the inferior vena cava , or during follow - up , mainly as a result of brosis or hyperplasia in the anastomotic area [ 5 8 ]  . 
other ndings include ascites , oedema of limbs , hepatomegaly , pleural effusion and altered liver function the lower 184 radiol med ( 2014 ) 119 : 183188 [ 811 ]  . 
arterial and biliary stenoses are the most commonly reported complications [ 5 , 6 ] , which may require a percutaneous and / or endoscopic and / or surgical approach . however , when managing anastomotic complications of the inferior vena cava , most medical reports recommend an exclusively endoscopic approach [ 714 ]  . 
in this study , we present a group of six patients who developed stenosis of the inferior vena cava at the level of suprahepatic veins , due to torsion of the inferior vena cava following orthotopic liver transplantation using the modied piggyback technique . 
we describe our approach to the endovascular treatment by primary stenting using gianturco cook - z vena caval and venous design stent ( cook , bloomington , in , usa ) , with special reference to selection of stent diameter and length , access and the need for primary stenting in view of the poor response to percutaneous angioplasty alone . materials and methods patients and liver transplants from november 2003 to october 2010 , out of a total of 316 orthotopic liver transplantations performed using the modied piggyback technique , 6 patients were referred to our interventional radiology centre with clinical evidence suggesting stenosis of the inferior vena cava with clinical onset between 3 and 94 days ( mean 11 days ) after surgery . these patients , ve of whom had undergone transplantation at our centre and one elsewhere , received endovascular treatment of the inferior vena cava alone . 
the pretransplant liver diseases were : hepatitis c - related cirrhosis ( n = 4 ) , exotoxic cirrhosis ( n = 1 ) , cryptogenic cirrhosis ( n = 1 )  . diagnosis in all six patients , stenosis of the inferior vena cava and of the suprahepatic veins was included in the differential diagnosis on the basis of the clinical presentations consisting of ascites , diffuse abdominal pain , increase in weight , oedema of the lower limbs , pleural effusion , hepato - splenomegaly , and on the basis of liver biochemistry tests such as bilirubinaemia , albuminaemia , coagulation parameters , natraemia and transaminases . 
all patients underwent a colour doppler ultrasound ( us ) examination . the main us ndings such as a reduction in caval diameter in the peri - anastomotic region , monophasicity of the ow velocity wave in the hepatic veins , increase in the ow velocity in the suprahepatic and inferior caval veins , and a reduction in the portal veins , are generally nonspecic , but highly indicative for diagnosing stenosis of the inferior cava [ 15 ]  . 
for the treatment of steno - occlusions of large venous vessels , numerous steel or nitinol stents are available on the market ( e.g. , sinus xl ; optimed , germany , e - xl ; jotec , germany , wallstent ; boston scientic , ma , usa , etc . ) ; however , most of these are closed - cell stents , which may obstruct venous return from the suprahepatic veins and , above all , may cause difculties in passing through the mesh for further procedures . therefore , in all six patients , we selected the gianturco cook - z - vena cava and venous design stent ( cook , bloomington , in , usa )  . 
this is a steel self - expanding stent with 25 - mm z - shaped modules , available with diameters of 20 , 30 and 40 mm and lengths of 25 , 50 and 75 mthe diameter was selected based on the inferior vena cava measurements on preliminary ct angiography and conrmed at pre - stenting cavography . 
ideally , a large literature and the stent manufacturers part of medical themselves recommend oversizing the stent by 1525 % with respect to the maximum diameter of the unaffected vena cava ; however , we preferred a slightly larger oversizing ( by approximately 30 % ) to ensure greater expansile strength of the stent and resolve the stenosis . 
therefore , after obtaining a right transjugular sonographic and uoroscopic access in all six patients , a 9 - fr introducer sheath radiol med ( 2014 ) 119 : 183188 fig . 
1 a axial multidetector computed tomography ( ct ) and b coronal maximum intensity projection ( mip ) reconstruction in a 42 - year - old patient on day 14 after liver transplantation , which demonstrated inferior cava vena steno - torsion at the level of anastomosis ( arrow head ) and dilatation of the hepatic veins ( arrows ) fig . 
the system used to release the z - stent is the radiol med ( 2014 ) 119 : 183188 table 1 patients liver disease , days from transplantation to onset of symptoms , and size and length of the stents and balloon catheters patient no . liver disease days from transplantation to onset of signs and symptoms stent size ( mm ) stent modules ( no . ) pta size / length ( mm ) hcv - related cirrhosis exotoxic cirrosi hcv - related cirrhosis hcv - related cirrhosis hcv - related cirrhosis cryptogenic cirrhosis 40 / 75 30 / 75 40 / 75 30 / 75 30 / 75 30 / 75 no pta no pta 14 / 40 14 / 40 no pta 12 / 40 pta percutaneous transluminal angioplasty , hcv hepatitis c virus introducer set ( cook , bloomington , cook - z stent usa ) , which consists in an introducer with reinforced sheath with dilator and pusher , available in the 10 - , 12and 14 - fr sizes , with a pull - back release systethe 30 - mm stents were released by means of a 12 - fr introducer , while the 40 - mm stents were released by means of a 14 - fr introducer . on two patients , we performed in - stent angioplasty using xxl balloon catheters ( boston scientic , natick , ms , usa ) with diameters of 12 and 14 mm and a length of 40 mm as , despite an optimal radial force , the stent was not sufcient to resolve the steno - torsion satisfactorily by over 50 % . 
3 pressure gradient ( mmhg ) positioning of the stent and iatrogenic vascular lesions . recurrence was dened as an increase in the pressure gradient c3 mmhg , clinical and biochemical signs of liver insufciency , and re - stenosis at the level of the inferior vena cava on colour doppler us . results technical success was achieved in all patients ( 100 % )  . 
an immediate pressure response ( b3 mmhg ) was shown in three patients ( 50 % ) , whereas the remaining three patients ( 50 % ) , showed a persistent high pressure gradient of 7 , 5 and 8 mmhg , respectively . 
no major or recurring complication was found in the other patients . discussion the importance of preserving the graft and thus the management of complications is crucial in this type of patient . as in all surgical procedures requiring anastomosis , orthotopic liver transplantations using the modied piggyback technique are subject to complications , including stenosis [ 5 , 6 ] , which may concern one or more of the four main anastomoses . 
torsion of the inferior vena cava at the level of the anastomosis following orthotopic liver transplantation is an even rarer complication when using the modied piggyback technique , and occurs with a frequency of roughly 12 % [ 58 ]  . 
in general , torsion affects the inferior vena cava at the level of the suprahepatic veins with a tendency to develop below the surgical anastomosis . the colour doppler us ndings are normally nonspecic , variable and unfortunately unable to quantify the haemodynamic signicance of the caval stenosis [ 18 ]  . however colour doppler imaging is highly suggestive for stenosis of the post - transplant suprahepatic veins . 
in these patients , persistence of monophasicity of the wave at the level of the suprahepatic veins is a sensitive , but not specic , sign of inferior caval stenosis at an anastomotic level . persistent phase waves with breathing or three - phase on colour doppler us may exclude the possibility of a consistent stenosis of the suprahepatic veins [ 19 ]  . 
ct angieasily ography , performed on all of our patients , demonstrated stenosis due to torsion of the inferior cava and enabled planning of endovascular treatment thanks to preliminary measurements of the caval diameters , subsequently conrmed by venography . 
venography by image subtraction , with measurement of trans - stenotic pressure gradients , remains the gold standard for the diagnosis of caval anastomotic complications in this type of patient [ 7 ]  . steno - torsion appears as a streaked image on the longitudinal axis , rather than an actual focal stenosis , with varying alterations in density and uniformity of the intraluminal contrast column in the context of the anomaly [ 7 ]  . we considered technical success as a reduction in the pressure gradient of b3 mmhg ; in the literature , however , there is no clear level of pressure gradient above which patients may develop specic symptoms [ 16 , 2022 ]  . 
in our group of patients , the presentation of clinical signs and symptoms developed over an average of 28 days from the transplant ; however , this average was strongly inuenced by a single patient who developed symptoms 94 days after the transplant . 
in our experience , torsion of the inferior vena cava is a typical complication of the early postoperative period , and in this period patients can have a large variety of complicated medical complaints that occur simultaneously , such as ischaemic injury due to reperfusion , rejection , oedema and liver enlargement . 
it is for these very reasons that the treatment should always be patient - specic , considering the clinical scenario , biochemical values , radiological examinations , morphology of the stenosis and above all the trans - stenotic pressure gradients . 
currently , angioplasty and stenting are considered the rst - choice treatments for inferior cava steno - torsion , but most studies agree that angioplasty alone of the inferior vena cava is not sufcient to ensure adequate patency in the long term [ 5 , 9 , 1113 ]  . 
although there is justiable reticence to treating the above - described anastomosis percutaneously by angioplasty , we have found no contribution in the literature regarding the rupture or breakdown of the anastomosis , and therefore we maintain that the risk is decidedly limited . 
in this case , because of the mixed aetiology of both torsion and intimal hyperplasia and because no change in the pressure gradient was detected after angioplasty due to immediate re - stenosis , it was decided to position the stent . 
each patient was treated with three - module stents , for length of 75 mm , because we believe that an a total extended coverage is crucial to avoid recurrence and migration of the torsion to a caudal level [ 7 , 8 , 23 ]  . 
post - stenting angioplasty was carefully considered for each patient on the basis of the response of the stenosis to stenting , and reserved for stenoses with a greater brotic component . we believe that the wait - and - see approach is the most appropriate when choosing to perform angioplasty , and staggering , on the basis of the pressure gradient readings , the dilation procedure over the following days . 
in fact in the three patients who did not undergo angioplasty , the 188 radiol med ( 2014 ) 119 : 183188 stent was sufciently expanded after 3 days and the pressure gradient was below 3 mmhg . 
this approach ensured good stability of the introducer , optimal control on release and avoided the possibility of migration to the right atriuwe found no major procedure - correlated complications , or signs of recurrence on an average follow - up of 49 months . we must stress that the choice of the correct stent characteristicsincluding diameter , radial force , low compressibility and good resistance to pressureis crucial [ 12 , 24 ]  . 
the main limitation of this study was the small number of patients , largely due to the rarity of this complication ; other cases will be needed to conrm the correct choice of technique and materials used . in conclusion , in our case series of steno - torsion of the inferior vena cava following orthotopic liver transplantation using the modied piggy - back technique , the use of large - mesh stents with the transjugular approach was found to be fast and free of complications and ensured a denite and lasting response in symptomatic caval torsion . conict of interest carlo ferro , enzo andorno , andrea guastavino , umberto g . 
imaging of lumbar spine with the patient in a supine , nonweight - bearing position is likely to misrepresent the degree and potential risk of spinal stenosis . materials and methods in the period between september 2008 and may 2011 , we selected 630 symptomatic patients aged 4065 years ( mean age 56 ) who underwent conventional mr in clinostatic position . 
the biomechanical parameters were also considered . changes in the dimension of the neural foramina were compared using the presence of disc and facet degeneration by statistical analysis . results stenosis of the intervertebral foramen was never found in the presence of normal intervertebral discs either in the presence or in the absence of facet disease , in either clinostatic or orthostatic position . 
in all of these cases , disc disease was associated with facet pathology . conclusion our data show that the association between disc pathology and facet osteoarthrosis can cause occult foraminal stenosis . 
gallucci department of radiology , university of laquila , 67100 laquila , italy e - mail : alessandra.splendiani@cc.univaq.it physiological load conditions may improve the clinical diagnosis of radicular pain . keywords dynamic mri ( cid : 2 ) spine pathology ( cid : 2 ) lumbar arthrosis ( cid : 2 ) new technological mr application ( cid : 2 ) weight - bearing mr application introduction foraminal stenosis is a painful and incapacitating condition caused by the pathological narrowing of the intervertebral foramen , with consequent compression of the nerve roots involved . 
the quantity of space available to the nerve along its anatomical path is related to the morphology of the structures delimiting the canal , which are the intervertebral disc , ava ligaments and interapophyseal joints . 
a congenitally narrow canal , possibly associated with increased thickness of the ava ligaments and hypertrophy of the joint facets , asymptomatic in the rst 10 years of life with symptoms often appearing in adult years . 
in fact , the combination of degenerative arthritis with further thickening of the aval ligaments , protrusion of the intervertebral discs , and osteopathy of the joint facets leads to deterioration of the main symptoms , as described in a number of studies [ 1 , 2 ]  . the exact incidence of spinal stenosis in the general population is not well known , although numerous studies have shown that its prevalence increases with age [ 3 , 4 ]  . between 4 and 28 % of asymptomatic patients on computed tomography ( ct ) or magnetic resonance ( mr ) radiol med ( 2014 ) 119 : 164174 fig . 
1 mcgill pain questionnaire examinations show radiological signs of stenosis [ 5 , 6 ]  . however , a large number of diagnostic examinations ( ct and mr ) on symptomatic patients show no signs of the pathology [ 7 ]  . 
therefore , spinal stenosis must represent a dynamic and intermittent process which intervenes when the spinal column is subjected to stress [ 8 ]  . the objective of this study was to assess , in symptomatic patients , the presence of foraminal stenosis not revealed on conventional mr examinations , but detected in the on examinations performed with the patient orthostatic position using dedicated mr equipment able to examine the spinal column in both the orthostatic and particular , we positions . that mr examinations tested clinostatic in weight - bearing hypothesis conditions ( orthostatic position ) are able to detect presence of dynamic stenosis of the intervertebral foramen , as demonstrated by anatomicalpathological studies [ 9 ]  . materials and methods in the period between september 2008 and may 2011 symptomatic ( 33 months ) , we selected a number of 166 radiol med ( 2014 ) 119 : 164174 fig . 
examination in clinostatic position ( 0.25 t tilting permanent magnet g - scan , esaote , genoa , italy ) patients aged between 40 and 65 years ( average age 56 ) who underwent conventional mr in clinostatic position because of reported pain in the lumbosacral region ( total number of patients 630 )  . 
the study excluded patients suffering from pain attributable to the following causes : primary tumours originating from the vertebral canal , metastatic disease from another region , positive clinical intervention on the trauma , surgical history for spinal spine , spondylolysis and spondylolisthesis , arthritic disease affecting more than one metameric level . 
these patients were examined by means of mr examination in the clinostatic and orthostatic positions carried out on a dedicated mr unit ( g - scan , esaote , genoa , italy ) equipped with a tilting system allowing immediate rotation of the patient bed and the magnet . 
these safety straps are also important in the emergency procedure , due to the fact that when changing from the clinostatic to the orthostatic position , some patients may suffer from vaso - vagal or vaso - depressor syncope . 
in the supine position , t1 fast spin echo ( fse ) , t2 relaxation fse , t2 sagittal and 3d scans were acquired ( total duration 17 min ) , whereas in the erect position only the last two types of scan were performed ( duration 11 min )  . 
the three - dimensional ( 3d ) mr images were acquired using a 3d steady - state hybrid contrast - enhanced ( hyce ) sequence with the following parameters : 10 / 5 ( repetition time ms / echo time ms ) , ip angle of 80 ( cid : 3 ) , two sequential scans . 
the other typical acquisition parameters included an acquisition matrix of 180 9 180 for a eld of view of 200 9 200 mm ( from 0 to 512 in both directions to optimise effective resolution ) , a single plate with a thickness of 220 mm , 64 sections and a bandwidth of 185 hz per pixel . 
the a morphological , clinically nonpathological condition of intersomatic discs , joint facets and aval ligaments was evaluated on both levels for a total of 145 ? 145 cases . morphological characterisation of the state of the various structures under examination was performed on the basis of previously described [ 6 ] mr features : radiol med ( 2014 ) 119 : 164174 fig . 
the morphological evaluations were made by two reading panels , each made up of one expert neuroradiologist and two junior neuroradiologists , who examined the images acquired in the orthostatic and clinostatic positions at random and independently from each another . 
the distribution of the patients on the basis of the appearance of intervertebral disc was as follows : 81 / 230 highly degenerated , 34 / 230 degenerated , 35 / 230 normal , 80 / 230 physiologically altered . 
therefore , the discs taken as a reference were at a metameric level below the pathological level in only 25 / 115 cases ( 22 % )  . the interapophyseal joints and aval ligaments were considered pathological in 73 / 230 levels considered . evaluation of all disc - vertebral levels examined ( 230 levels ) showed disc pathology to be associated with a normal appearance of the interapophyseal joints in 54 / 230 levels ; at 61 levels , there was an association between disc abnormality and alteration of the facets ; at 103 levels , the nonpathological disc was associated with a normal appearance of the joint facets ; at 12 levels , there were arthritic changes to the interapophyseal joints in the absence of disc degeneration . the intervertebral foramen was considered , on the basis of the previously stated denitions , to be stenotic at 61 / 230 levels and nonstenotic at 169 / 230 . 
at the level with normal disc and facet appearance , there was no change in the neural foramina from supine to upright position radiol med ( 2014 ) 119 : 164174 fig . 
according to conventional criteria , this difference is considered statistically highly signicant . the spinal parameters were altered in 87 / 115 patients ( 76 % ) , in particular : the lumbar lordosis angle ( with a physiological value of approximately 50 ( cid : 3 ) ) [ 7 ] was altered in 68 patients , of whom 46 had a decreasing angle both in the clinostatic and orthostatic positions ( with an average value of 40 ( cid : 3 ) ) ; 22 patients showed an increased angle ( average value of \60 ( cid : 3 ) ) which was not modied in the orthostatic position ; the lumbosacral angle ( with a physiological value of approximately 120 ( cid : 3 ) 135 ( cid : 3 ) ) [ 7 ] was altered in 47 patients ( 53 % )  . 
in all these patients , we measured an angle greater than 135 ( cid : 3 ) , with no modication in the dynamic study ; both angles were found to be altered in 21 patients . discussion in the industrialised parts of the world , low back pain is extremely common with a prevalence ranging from 60 to 90 % . 
symptoms normally evolve during the 5th or 6th 170 radiol med ( 2014 ) 119 : 164174 decade of life , and are associated with arthritic variations of the vertebral column . 
the societal impact of low back pain in older adults is demonstrated by medicare data from 1991 to 2002 that show a 132 % increase in low back pain patients and 387 % increase in related charges for low back pain . despite the fact that low back pain is common and associated with poor outcomes in vulnerable older adults , little research has focused on low back pain in people over the age of 65 [ 10 ]  . lumbar spinal stenosis is a debilitating chronic pathology , which generally starts with degeneration of intervertebral discs and joint facets , causing a narrowing of the vertebral canal and neural foramen . 
a fundamental contribution to the study of the problem is provided by ct and mri ; in particular , the latter enables a high degree of spatial resolution and contrast , and provides a precise evaluation of intervertebral discs , vertebrae , ligaments , spinal canal and intervertebral foramen . 
despite the unquestionable diagnostic accuracy of these methods for the morphological evaluation of these anatomical structures , when diagnosing foraminal stenosis , the number of false negative results is considerable , as shown in the literature [ 11 ]  . 
by subjecting in vitro cadaveric lumbar segments to movements of axial rotation , extension , bending and lateral curvature , a compression of the spinal nerve was observed , not detected in examinations without the application of weight show that compression results involving the spinal roots is associated with disc and facet pathology with signicant p values , and this conrms that there is an association between the risk factor ( osteoarthritis of facets ) and the disease ( disc pathology )  . 
this correlation agrees with the pathological and biomechanical studies which identify as one of the causes of brosis of the aval ligament the loss of disc elasticity in response to an increase in mechanical stress . 
radial rupture of the annulus brosus or a reduction in disc signal intensity , seen on mri , indicates a serious reduction in elasticity , which leads to brosis and hypertrophy of the aval fig . 
b sagittal t2 - weighted image : 3d hyce reformatted slice on the axial plane . the upright mri study shows an increase in disc protrusion and a reduction of intra - articular uid collection with consequent thickening of the aval ligament which cause a stenosis not seen on supine mri ( white arrow )  . 
in the erect position , the static weight on the spinal column strongly reduces the thickness of the degenerated disc , unlike what occurs on the nonpathological disc , and enlargement and protrusion of the aval ligament can be observed inside the intervertebral foramen . 
the foramen therefore appears to be occupied by the table 2 the p value was calculated with mcnemars test with continuity correction control total case total chi - squared equals 25.470 with one degree of freedothe twotailed p value is less than 0.0001. 
furthermore , in some of the cases , we were able to highlight intersegmental hypermobility with bearing of the facet itself in orthostatic conditions . the advent of dedicated mr has enabled in vivo investigations in orthostatic condition and thus an evaluation of the disc - vertebral structures and of their biomechanical properties . 
the laxity of the ligament also causes shifting of the facet ( black arrow ) structures , and thanks to this that discs in the rear section are subject to greater pressure , which tends to maintain the nuclear gel in a more forward position , thus preventing protrusion [ 17 , 18 ]  . 
the results obtained with dynamic mr under weight - bearing conditions conrm previous studies ( rajnic ) , which show a signicant decrease both in the angle of lumbar lordosis and the sacral angle in patients with disc alterations . 
if the lumbosacral angle is greater than 180 ( cid : 3 ) , this means there is a reduction in lumbar lordosis , with verticalisation of the sacrum and suffering of the front portion , with repercussions on the nuclear content of the disc . 
on the contrary , if the angle is less than 120 ( cid : 3 ) , this means that there is an increase in lumbar lordosis and horizontalisation of the sacrum with an increase in the compression on rear structures . 
in fact , in the erect position , under physiological conditions , the interapophyseal joints support most of the cutting force which acts on the vertebral column [ 19 ] and 16 % of the compression forces [ 20 ]  . 
in the presence of disc pathology ( reduction in disc height , loss of water content , degeneration ) , the facet may enter in close apposition to support 70 % of the compression forces , with overload of the joint . the latter can lead to degenerative arthritis which , as mentioned above , is one of the causes of narrowing of the conjugate foramen [ 20 ]  . radiol med ( 2014 ) 119 : 164174 one of the salient limits to the dynamic investigation of the vertebral column lies in the reproducibility of the cutting planes . 
in fact , movements of the patient and even normal vibrations under the effect of the weight can represent the cause of enormous or small modications to the selected scanning plane . 
for this reason , we used a 3d scan protocol ( 3d hyce both in clinostatic and orthostatic positions ) and precise post - processing reconstruction using the mpr algorithm with an effective thickness of 1 mm , parallel to the vertebral endplate in the coronal and sagittal planes . 
these reformatted images enabled a study of the vertebral foramen and the relationship between the internal structures both in normal and pathological conditions such as the aval ligament ( inside the foramen ) and its relation to the spinal nerve and nerve roots . 
however , in orthostatic conditions may have less the images favourable signal - to - noise ratio compared to those obtained in clinostatic conditions , while maintaining the same diagnostic capacity . 
dynamic imaging techniques may increase our ability to locate the original site of nerve root compression in patients suffering from low back pain or radicular patherefore , the dedicated mr unit used in this study is proposed as an instrument able to provide useful dynamic studies that may help obtain correct diagnoses [ 21 ]  . prompt diagnosis of the site and characteristics of foraminal stenosis may provide useful guidance for correct treatment procedures . 
cbct scans at treatment days 10 , 15 , 20 and 25 were used to transfer the original plan ( cbctplan i , ii , iii , iv , respectively ) using rigid registration between the two . 
the pgs were retrospectively contoured and evaluated with the dosevolume histograthe mean dose , the dose to 50 % of volume , and the percentage of volume receiving 30 and 50 gy were evaluated for each pg . 
the wilcoxon sign ranked test was used to evaluate the effects of dosimetric variations and values \0.05 were taken to be signicant . results from february to june 2011 , ten patients were enrolled and ve imrt plans were evaluated for each patient . 
fiorentino department of radiation oncology , sacro cuore - don calabria hospital , negrar - verona , italy checking the pg volume and dose could be indicated during the third week of treatment . keywords head and neck cancer ( cid : 2 ) imrt ( cid : 2 ) conebeam ct ( cid : 2 ) organ at risk ( cid : 2 ) parotid glands introduction in the treatment approach for patients affected by head and neck ( h&n ) cancer , radiotherapy plays an important role to increase local control and survival . 
the introduction of intensity - modulated radiotherapy ( imrt ) has increased the possibility to deliver higher doses to the target with sparing of the organs at risk ( oar ) compared to conformal radiotherapy [ 1 ]  . volume changes and / or anatomical deformations of both the target and oar are independent of the immobilisation systems used but , due to these changes , there is a risk of administering higher or lower doses compared to the planned dose [ 27 ]  . to reduce the risk of xerostomia , the parotid glands ( pgs ) have been widely studied in terms of volumes and dose changes [ 3 , 4 , 712 ] , and several trials highlighted that imrt re - planning is mandatory for selected patients [ 7 , 10 ]  . the shrinkage of pgs has important implications for the daily dose distribution [ 13 , 14 ]  . 
 [ 10 ] reported similar results : all pg dosimetric values increased during week 3 of treatment . to intercept and correct set - up errors , image - guided radiotherapy ( igrt ) has proved useful [ 1420 ] and in our institution , a trilogy varian medical system cone - beam computed tomography ( cbct ) is available for controlling 202 radiol med ( 2014 ) 119 : 201207 the set - up position of all anatomical regions and for evaluating pg changes [ 3 ]  . moreover , cbct scans have also been used for dose reconstruction , and some authors have reported their value for clinical decisions regarding re - planning [ 21 , 22 ]  . in consideration of the 1530 % volume reduction observed at weeks 34 of treatment [ 3 ] , this study aimed to investigate whether and when re - planning is required to spare the pgs during a course of headneck imrt , by evaluating the dosimetric consequences of pg shrinkage with cbct scans obtained at four time points ( days 10 , 15 , 20 , 25 )  . materials and methods patients patients , with histologically proven headneck cancer , aged more than 18 years and treated with imrt , were analysed . 
patient immobilisation was obtained using a headshoulder thermoplastic mask and type s - fixator ( civco , orange city , iowa , usa )  . treatment plans noncontrast - enhanced ct scans were acquired in the treatment position ( 2.5 mm slice thickness )  . 
all imrt plans were performed with an eclipse 8.6 treatment planning system ( varian medical system , palo alto , ca ) and were based on a seven - eld sliding window technique with a nominal energy of 6 mv . imrt with simultaneous integrated boost dose consisted of 7072 gy to macroscopic disease ( clinical target volume , ctv1 ) ; 6066 gy to microscopic high - risk disease ( ctv2 ) and 5458 gy to microscopic low - risk disease ( ctv3 )  . 
the quantec guidelines were used to evaluate oar [ 23 ]  . every other day during radiotherapy , all patients underwent cbct scans ( slice thickness of 2.5 mm ) to verify the set - up positioning . 
the cbct low - dose head model was used to generate images with full - fan acquisition , with 360 projections being acquired over a gantry rotation of 200 ( cid : 3 )  . 
the position of each patient was adjusted based on the rigid registration between cbct images and planning ct images ( 3d / 3d match )  . 25 ( cbctplan i , cbctplan ii , cbctplan iii and cbctplan iv , respectively )  . 
since this is an observational study , patients continued to be treated according to the original ctplan . statistics plan comparisons were made between the ctplan and the cbctplan i , ii , iii and iv , respectively . 
pg dosimetric variations were analysed for both pgs and , separately , for the ipsilateral and contralateral glands ( ipgs and cpgs , respectively )  . the wilcoxon sign ranked test was used to evaluate the effects of variations and values \0.05 were taken to be signicant . results patients from february to june 2011 , ten patients were analysed ( table 1 )  . 
all but two patients completed imrt : one patient died due to another disease , whereas the other table 1 patients characteristics age / gender subsite stage histology concurrent 41 / f 46 / m 54 / f 60 / f 63 / m 48 / m 77 / m 77 / m 78 / m 75 / m oral cavity oropharynx oral cavity oral cavity hypopharynx oropharynx oropharynx oral cavity larynx larynx t4n0m0 t4n2cm0 t4n2am0 t2n2bm0 t3n0m0 t2n1m0 t3n1m0 t4n1m0 t3n1m0 t4n0m0 the original treatment plan ( ctplan ) was transferred to the corresponding cbct scan at treatment days 10 , 15 , 20 and scc squamous cell carcinoma plan on cbct radiol med ( 2014 ) 119 : 201207 fig . 
1 the increase in average dmean , d50 , v30 and v50 between time 0 ( original plan ) and the subsequent cbct - based plans ( 10152025 fractions )  . 
error bars indicate 95 % condence interval patient missed the last four fractions because of grade 4 skin toxicity . parotid glands forty cbct plans were generated and compared to the corresponding ctplan and , for each patient , ve imrt plans and ten pgs were analysed . 
the average of increase in dmean , d50 , v30 and v50 for both pgs and for ipg and cpg separately are shown in table 2 . the ipg dosimetric variations were higher than those reported for the cpg at each time points , except for the cbctplan i ( table 2 )  . 
2 shows an example of dose change in both pgs . discussion for headneck cancer , imrt has achieved an excellent dose distribution , with a reduction in toxicity [ 16 , 25 ]  . patient immobilisation systems are effective in reducing set - up errors , but due to anatomical and volume variations in the target and oar and the patients weight loss [ 26 ] during treatment , they could increase the risk of missing the target or applying higher doses to the oars . several papers documented that the largest changes occur in the pgs with a volume loss of about 15 % at week 2 of treatment [ 3 , 5 , 11 , 13 ]  . 
 [ 28 ] analysed ten headneck cancer patients and observed that , due to the shrinkage , the delivered dmean increased for both pgs . although several studies have shown an increase in dose over a course of radiation treatment [ 3 , 26 , 28 ] , it is not clear whether and when re - planning should be carried out . thus , the aim of our study was to assess the optimal timing of re - planning to spare the pgs in headneck cancer patients by analysing the dosimetric variations during a course of imrt . in this study , all patients underwent cbct to verify the set - up positioning and , to investigate the correct re - planning time , we selected four time points ( day 10 , 15 , 20 and 25 of treatment ) and the corresponding cbct scans . 
since several studies showed that the imrt dose reconstruction based on cbct was an effective dosimetric basis for clinical decision to replan [ 21 , 22 ] , we transferred the original treatment plan on each cbct to evaluate the pg dose features . we observed that all the dosimetric end - points , except for v50 , increased signicantly if ctplan was compared to cbctplan i and ii . 
 [ 10 ] reported an increase in pg dose at week 3 of treatment in 33 patients with nasopharyngeal carcinoma , who repeated ct scans after 15 5 imrt fractions . 
the authors observed an increase of dmean , d50 and v46 for cpg compared to the original plan ( p = 0.03 , p = 0.04 , p = 0.03 , respectively ) , while the increase in dose for ipg was not signicant . 
the ipg dose was signicantly higher at weeks 4 and 5 ( p = 0.006 , p = 0.01 ) with an average increase compared to the planned dose of 2.7 gy , and the contralateral dmean increased signithe week 4 ( p = 0.03 ) [ 11 ]  . 
2 an example of the change in dose for both parotid glands : a original plan ; b original plan transferred on the cone - beam ct at treatment day 15 only one other study investigated dosimetric monitoring using cbct during parotid - sparing imrt in ten patients with headneck cancer . 
2 and table 3 , we found that the deep part of the pgs could be much more irradiated during an imrt course , there being in fact an increase in the percentage of volume that received 30 and 50 gy . 
in addition , recent papers have shown signicant differences in damage when the cranial or caudal part of pgs was irradiated ; the reduction in ow was much more severe with irradiation of the cranial part of pg [ 30 , 31 ]  . 
our analysis did not evaluate this aspect due to the short follow - up for evaluating xerostomia , but it could be interesting for improving the treatment plan : parotid - sparing imrt is used despite the possibility of parotid recurrences after treatment [ 32 ] , so perhaps cranial - parotid - sparing could be proposed to reduce the damage . another limit of the study was the monitoring of pgs dosimetric changes without using hounseld correction algorithm for cbct . 
 [ 29 ] showed that the differences between dose to the organ structures before and after tissue correction based on the planning ct and cbct were not clinically signicant ( \2 % )  . conclusions the pgs showed major modications in volume , resulting in a signicant dosimetric change during the course of imrt . 
our data showed that cbct is a feasible method to control the dosimetric variations even though the method is still to be validated for dosimetric monitoring and replanning . evaluation of the pgs by monitoring the dose and analysing the different pg regions could be indicated during the imrt course [ 33 ]  . 
the results obtained should be reported , at the end of each working day , on a special dose card , in order to record each workers exposure to the static magnetic eld . moreover , this dose card could be an important tool if long - term effects occur because it provides a complete history of the occupational exposure in an mri site . materials and methods to conduct measurements , three hall - sensor probes were used . 
quadrelli department of biotechnology and life sciences , university of insubria , varese , italy when the strength of the magnetic eld was [ 200 mt the weighted function overestimated the exposure , so that it represents a highly precautionary measure taking into account possible acute and long - term effects . 
in addition , from the data recorded during patient positioning operations by mri staff the db / dt curve was obtained . conclusions the areas obtained from the integral of the weighted static magnetic eld strength over time can be indicative of the global exposure of the occupational staff . these values should be reported on a special dose card that could be considered as an important if long - term effects occur because it provides a complete history of the occupational exposure in an mri site . tool keywords mri staff exposure ( cid : 2 ) mri safety ( cid : 2 ) exposure limits ( cid : 2 ) static magnetic eld introduction the human population is chronically exposed to natural and man - made sources of nonionising radiation . 
recent advances in technologies using static magnetic elds and , particularly , in magnetic resonance imaging ( mri ) , have resulted in increased values of static magnetic elds available for example for applications . 
consequently , diagnostics exposure levels have also increased , and this is especially relevant for mri staff . and medical whilst acute effects are evident , especially for exposure to high - intensity static magnetic elds , [ 1 ] , biological effects derived from chronic exposure to static magnetic elds are less understood . 
the possible interaction mechanisms of static magnetic elds with living tissue and radiol med ( 2014 ) 119 : 208213 resulting detrimental biological effects have been investigated [ 1 ] , highlighting the potential risks of long - term effects due to chronic exposure . 
one related concern is the chronic , repetitive , and lengthy occupational exposure to magnetic elds from mri equipment . currently , international commission on non - ionising radiation protection ( icnirp ) safety regulations [ 2 ] recommend limiting the time - weighted exposure to 200 mt per working day with instantaneous maxima of 5 t for extremities and 2 t for head or trunk . 
the more conservative italian safety regulations1 impose the following limits of exposure to static magnetic elds : ( a ) 200 mt for a maximum of 60 min in one working day ( 8 h ) , and ( b ) 2 t for a maximum of 15 min in one working day . in 2004 , the european union ( eu ) drafted a new directive to be implemented in eu national regulations by 20132 , 3 , 4 on occupational exposure to static magnetic elds , recognising the limitations of present guidelines and the need for new studies to advance knowledge . 
in particular , the new scientic studies on the impact on health of exposure to electromagnetic radiation , made public after the directive was adopted , have been brought to the attention of the european parliament , the council and the commission . 
the results of those scientic studies are currently being examined by the icnirp as part of the ongoing review of its recommendations . the icnirp guidelines on limits of exposure to static magnetic elds recommend that occupational exposure be restricted to a maximum ( acute ) magnetic ux density of 2 t for head / trunk and of 8 t for the limbs . 
the exposure limit of the general public is derived from the former , by applying a reduction factor of 5 , thereby obtaining a maximum acute exposure of 400 mt for any part of the body [ 2 ]  . in the context of static magnetic elds , the evaluation of the dose is complicated because it involves multiple factors related to the characteristics of the eld and its interaction with living matter . 
02 / 08 / 1991 . 2 directive 2004 / 40 / ec of the european parliament and of the council of 29 april 2004 on the minimum health and safety requirements regarding the exposure of workers to the risks arising from physical agents ( electromagnetic elds ) ( 18th individual directive within the meaning of article 16 ( 1 ) of directive 89 / 391 / eec )  . 3 directive 2008 / 46 / ec of the european parliament and of the council of 23 april 2008 amending directive 2004 / 40 / ec on minimum health and safety requirements regarding the exposure of workers to the risks arising from physical agents ( electromagnetic elds ) ( 18th individual directive within the meaning of article 16 ( 1 ) of directive 89 / 391 / eec )  . 4 directive 2012 / 11 / eu . exposure guidelines not only for patients , but also for staff chronically exposed to static magnetic elds . 
from that work , the authors concluded that the adoption of personal dosimeters is essential to both protect the worker and permit the collection of relevant exposure levels and duration to monitor the health of medical and paramedical mri staff . of particular interest in this paper is the category of occasional and permanent mri staff who are chronically exposed to varying levels of magnetic elds during tasks including patient positioning and removal , system verication tests , calibration . 
therefore , the focus in this paper is on the identication of an equivalent exposure level to static magnetic elds , by incorporating information on both magnetic eld strength and exposure time , to estimate the occupational dose for preventative occupational health and safety . exposure is generally dened as the product of time duration and disturbance ( e.g. , the concentration of a toxic chemical ) [ 4 ]  . 
for the denition of exposure to static magnetic elds , the parameter used as disturbance can be interpreted in different ways , for example , in [ 5 ] it is taken as the square of the magnetic ux density normalised to a specic value . 
however , in this paper , it is recognised that to decouple the possible effects from the cause , the simplest approach is to use the magnetic ux density as a measure of the disturbance . the magnetic ux density , although time - independent , typically varies as a function of position . 
by recording the magnetic ux density to which staff are exposed , as a function of time and integrating this information over time , it is possible to monitor occupational exposure levels . the spatial variation of the eld and the relative movement of mri staff within the magnetostatic eld are included in the present formulation by assuming that the magnetic ux density is time - dependent , bt . 
thus , the cumulative exposure , [ 6 ] , eb ( in tesla ( cid : 2 ) hour = t ( cid : 2 ) h ) is dened as the product of the magnetic ux density by the exposure time , as also used in [ 6 ] : eb btdt where the magnetic density given y b2 x b2 , with bx , by , and bz obtained ( cid : 3 ) fw 0 : 8333b 1 ; b ( cid : 3 ) 0 : 2t b [ 0 : 2t measurements are : radiol med ( 2014 ) 119 : 208213 experimentally from the measurements as detailed in the following . in this paper , the authors propose a further precautionary step to protect occupational staff , by introducing a weighting function incorporating the exposure limits imposed by the legislation of interest . 
one interpretation of the above two different exposure limits is that larger magnetic ux density values carry a more signicant risk , i.e. , a heavier weight , by a factor of 2.5 with respect to a unit weight assigned to lower eld levels . 
to include this distinction in the proposed denition of weighted occupational exposure the weighting function is dened , in the rst instance , as for precautionary limits the individual , personal probes should be calibrated using the most conservative exposure limit indicated in the legislation of interest as a maximum exposure limit to dene the weighting function , example , 0.2 t ( cid : 2 ) h in the case of the italian legislation . the above denition of weighted occupational exposure , eq . 
 ( 2 ) , gives the exibility of modifying appropriately the weighting function ( 3 ) in the light of new regulations , and also in the light of possible new quantitative ndings of the biological effects of static magnetic elds . 
the proposed weighted occupational exposure denition enables the integration of the information on magnetic eld levels and exposure times , and the quantication of the magnetic exposure during the working day for healthcare staff . the physical consequence of the implicit time - variation of the magnetic ux density b ( t ) is the induction of currents in body parts of occasional and permanent staff particularly during patient positioning . 
one of the concerns in high - eld mri is related to the induction of in situ electric elds and associated current densities caused by rapid movement of the body within the nonuniform , strong static magnetic eld [ 7 ]  . in such cases , a number of physiological responses have been reported , including headache , nausea , vertigo , phosphene , numbness and tingling , loss of proprioception , and balance [ 8 ]  . 
theoretical models for the evaluation of electric elds and current densities induced in whole body , in male and the methodology followed in the present work involved the following steps : identication of suitable clinical and research mri equipment ; 2 . 
measurement of the magnetic ux density as a function of time over the operating period , using different isotropic personal probes worn by mri staff , following informed consent ; analysis and interpretation of the results in the context of present national and international regulations . the three hall - sensor probes used for the isotropic ( ets ( a ) holaday hi3550 magnetic field monitor lindgren , cedar park , tx , usa ) : range 0.1 mt \ b \ 0.3 t , measuring both instantaneous and time - integrated magnetic eld , with a measurement update period of 3 s . 
the results of the measurements are shown , in real time , on a liquid crystal display . ( b ) metrolab thm1176 magnetometer ( ght photonics srl , italy ) : range b \ 20 t , probe managed by visa labview runtime ( national instruments ) installed on a handheld computer . 
1 results obtained from the measurements using the three probes : thm 1176 ( solid line ) , tsmd ( dotted line ) , hi3550 [ numeric values of the cumulative exposure , eq . 
 ( 2 ) , obtained for the duration of the measurements , expressed in mt ( cid : 2 ) h ] table 1 cumulative exposure derived from the experimental data of fig . 
the same results have been processed and integrated over time for the duration of the measurements , and listed in table 1 . the kruskalwallis test was used to evaluate the consistency of the experimental data presented in fig . 
having assessed the consistency of the probes , for practical reasons the remaining measurements were conducted using only the talete system ( tsmd )  . a typical example of recording obtained during the operation of patient positioning ( duration of approximately 7 min ) in a 0.35 t scanner is presented in fig . 
the cumulative exposure during a single operation of patient positioning was measured to be eb = 0.7 mt ( cid : 2 ) h , well below the limits imposed by the legislation . 
2 a magnetic ux density measured during positioning of the patient ( approximately 7 min ) in a 0.35 t clinical mri scanner , using the tsmd probe , and ( b ) corresponding db / dt curve limits [ 11 ] as they have been quantied to be \17 mt / s over the whole duration of the operation . in contrast , experimental data taken in the same type of operation ( patient positioning , 5 min duration ) , but in a more powerful ( 3t ) mri scanner are presented in fig . 
the resulting ( measured ) cumulative exposure was eb = 26.83 mt ( cid : 2 ) h , corresponding to a weighted occupational exposure ewb = 35.31 mt ( cid : 2 ) h . in addition , the db / dt curve resulting from exposure levels reported in fig . 
as an alternative , a weighted average is proposed here for the denition of occupational exposure to include limits and guidelines specied by regulatory bodies . radiol med ( 2014 ) 119 : 208213 conveniently , the proposed denition permits to account for possible health effects due to chronic exposure to static magnetic elds by simply modifying the weighting function , always complying with the ofcial recommended limits of exposure . the occupational exposure dened here also permits to determine the number of patients that can be positioned and treated by an individual mri worker in a working day , thus providing further precautionary occupational guidelines . 
in fact , while the cumulative exposure of mri staff operating clinical mri equipment ( b \ 2 t ) typically does not exceed the limit value indicated by the italian regulations , 200 mt ( cid : 2 ) h per day , it may indeed exceed such value in the case of advanced / high - denition and research - type mri equipment ( b [ 2 t )  . 
particularly for the italian case , the relevant authority , the italian national institute for occupational safety and prevention ( ispesl ) , now incorporated into the italian workers compensation authority ( inail ) , requires that the methodology for magnetic dosimetry be specied at the institute level . 
therefore , a detailed record of exposure to static magnetic elds for individual mri staff would be essential to provide data for future epidemiological studies on this category of workers for both acute and chronic effects , especially in view of possible changes in ofcial mri protection guidelines . 
by insisting on the use of personal probes for workers operating mri scanners it will be possible to gather a wide and statistically signicant pool of data to assist studies on health hazards due , specically , to chronic exposure to static magnetic elds . 
the recorded data could be stored daily on a dedicated exposure card to provide a complete history of the occupational exposure to mri - originated static magnetic elds , particularly for consultation from occupational health doctors . 
in view of the above considerations , the following data recording sheet is proposed to permit a full record of the occupational exposure to static magnetic elds . acknowledgments the authors wish to thank f . 
liver biopsy , the current gold standard for the diagnosis and staging of brosis and inammation , may be associated with complications such as bleeding , inherent limitations such as sampling error or interobserver variability and is not readily accepted by all patients [ 5 , 6 ]  . including biochemical and haematological noninvasive diagnosis of hepatic brosis has evolved rapidly in recent years [ 13 ]  . 
several noninvasive techtests niques , and a scoring system using a combination of clinical and laboratory tests are used to predict hepatic brosis , but predict their overlapping cannot results 904 radiol med ( 2014 ) 119 : 903909 necroinammatory activity [ 3 , 5 , 7 ]  . 
ultrasonographybased transient elastography , real - time elastography and acoustic radiation force impulse elastography are used for the evaluation of hepatic brosis but they are operator dependent and may be difcult in obese patients with narrow intercostal space [ 8 , 9 ]  . 
limited studies discuss the role of double - contrast magnetic resonance ( mr ) imaging , mr elastography and mr spectroscopy in the assessment of hepatic brosis in adults , but these pulse sequences are not widely available in clinical practice and their results are preliminary [ 10 , 11 ]  . diffusion - weighted mr imaging depends on the microscopic mobility of water protons . 
to our knowledge , no study to date has addressed the role of diffusion mr imaging in quantication of the degree of inammation in children with chronic hepatitis . the aim of this study was to prospectively evaluate the usefulness of the apparent diffusion coefcient ( adc ) value in the diagnosis and grading of hepatic brosis and inammation in children with chronic hepatitis . materials and methods this study was conducted on 53 consecutive untreated children with pathologically proven chronic hepatitis . three patients were excluded from the study due to motion artefacts at diffusion weighted mr imaging . 
informed consent from parents of patients and controls and institutional review board approval were obtained . mr examinations were performed using a 1.5 - t ( magnetom symphony ; siemens , erlangen , germany )  . 
the machine is equipped with a self - shielded gradient set ( 30 mt / m maximum gradient strength and 120 t / m / s slew rate ) for echoplanar imaging . 
the applied parameters were tr of 2 , 800 ms , te of 74 ms , epi factor of 102 , fov of 25 9 25 cm , section thickness of 7 mm , interslice gap of 20 % , acquisition matrix of 192 9 154 and number of excitations of 6 . 
the adc map was automatically calculated from the data set three b - values by commercially available obtained at software ( leonardo , version 2.0 ; siemens ag medical systems , forchheim , germany )  . 
the adc value was calculated according to the following formula : adc_ ( lnsb2 lnsb1 ) / ( b2 b1 ) , where ln is the natural log , and sb1 and sb2 are the signal intensities in the roi placed on sections corresponding to the two different b values ( b1 and b2 ) [ 30 , 31 ]  . 
the mean of these nine values was calculated and represents the nal adc value per subject that was used for statistical analysis . percutaneous liver biopsy was performed by a paediatric hepatologist ( b.t. ) with 7 years experience in liver biopsy . 
the stages of brosis were f0 ( no brosis ) , f1 ( mild expansion of some portal tracts by brosis ) , f2 ( expansion of most portal tracts by brosis ) , f3 ( occasional bridging brosis ) , f4 ( marked bridging brosis ) , f5 ( incomplete cirrhosis ) and f6 ( complete cirrhosis )  . 
the control children were regarded as having necroinammatory activity grade a0 and brosis stage f0 . statistical analysis was done using statistical package for the social sciences ( spss , inc . , chicago , il , usa ) software , version 16 . 
for statistical analysis , the stages of brosis were classied into mild ( f1 , f2 and f3 ) and advanced ( f4 , f5 and f6 ) and the grades of necroinammatory activity were classied into mild ( a1 , a2 ) and advanced ( a3 , a4 )  . receiver operating characteristic ( roc ) curves were done to evaluate the diagnostic capability of the adc value in differentiating hepatic brosis from normal liver , as well as in staging hepatic brosis and grading hepatic necroinammation . 
the area under the curve ( auc ) , sensitivity , specicity , accuracy , positive predictive value ( ppv ) and negative predictive value ( npv ) were calculated . 
diffusion mr imaging has been used for assessment of diffuse diseases in different regions of the body [ 4042 ] as well as in chronic diffuse liver diseases [ 1327 ]  . in the literature , various studies of diffusion mr imaging reported that adc values of hepatic brosis are lower than those of normal livers in adults [ 1421 ] and in children [ 29 ]  . 
in accordance with most of the previous studies [ 1623 ] , the adc values of the study group were also lower than the adc values of the control group . 
the mechanism of restricted diffusion in brosis is deemed to be multifactorial , mostly due to diminished hepatic perfusion and , to a lesser extent , to the presence of increased connective tissue , which contains fewer protons . 
the deposition of brous tissue leads to a reduction in the size or obliteration of small venules , with a resultant increase in portal venous pressure and consequent compensatory increased arterial blood ow [ 1517 ]  . 
the presence of increased connective tissue in the liver in addition to deposition of collagen bres , fatty inltration , hepatitis , cell necrosis / apoptosis and inammatory cell responsible for restricted diffusion with low adc value in patients with hepatic brosis [ 1419 , 29 ]  . inltration is the role of diffusion mr imaging in the study of diffuse liver disease , therefore , is still under debate . 
6 receiver operating characteristic ( roc ) curve of the adc value used for differentiating mild ( a1 , a2 ) from advanced ( a3 , a4 ) grades cutoff adc value was b1.64 9 10 - 3 mm2 / s with an auc of 0.807 , a sensitivity of 87.5 % , a specicity of 61 % and an accuracy of 74 % necroinammation . 
this may be attributed to more accurate calculation of the adc value in this study which was calculated from three b values ( 0 , 400 and 800 s / mm2 ) whereas other studies calculated the adc value only from two b values . 
last , this study was conducted on children who have better adc maps without noise or susceptibility artefacts compared to the adult patients . in this work , the adc value of hepatic parenchyma changed according to the stages of brosis . 
5 scatter plot of the adc value at different grades of hepatic necroinammation 908 radiol med ( 2014 ) 119 : 903909 know the usefulness of adc in distinguishing between the early and intermediate stages . 
also , linear regression analysis showed that hepatic adc values were a good predictor of brosis stage ( r2 = 0.19 , p = 0.0001 ) [ 19 ]  . in this study , there is a negative correlation between the adc values and necroinammatory activity . 
the adc value is signicantly lower in patients with high grades of hepatic inammation compared to those with low grades . the aggressiveness of chronic hepatitis is indicated by the degree of necroinammation , also called the activity ; the more severe the necroinammation , the more aggressive the disease . 
 [ 24 ] found a statistically relationship between the adc values and signicant hepatic activity index scores although this relationship was not as strong as that between adc values and brosis scores . 
in addition , entropy , which is a measure of the variability in the volume histogram analyses of the adc values , showed a greater correlation with the brosis stage and inammatory activity grade than did mean adc , with a sensitivity of 0.91 and a specicity of 0.92 in the detection of inammation [ 27 ]  . 
recent advances in mr software technology such as 3 t scanners with parallel imaging and respiratory triggering will likely continue to improve image quality and also promise the potential application of multiple and higher b values than 1 , 000 mm2 / s [ 43 , 44 ]  . 
also , further studies with application of diffusion tensor mr imaging with multichannel coils will likely improve the results [ 14 ]  . application of advanced postprocessing methods such as entropy [ 27 ] , bi - exponential , non - gaussian ( diffusion kurtosis ) modelling or k - means clustering algorithms [ 4447 ] may provide a better characterisation of diffuse liver disease . there are a few limitations to this study . 
second , we excluded three patients due to susceptibility artefacts , and we expect that future studies with application of parallel imaging will increase the image contrast and decrease susceptibility artefacts . 
if the registration method works correctly , parameters which bring the images into alignment must always be the same . results automatic registration performed by the software did not prove satisfactory , whereas if a specic tool [ volume of interest ( voi ) tool ] allowing the calculation to be limited to the landmark region was used , the registration s . 
stancampiano dipartimento di specialita` medico - chirurgiche , scuola di specializzazione in fisica medica , universita` degli studi di catania , via santa soa 78 , 95123 catania , italy parameters were comparable with those of the manual registration . 
regarding the repeatability of the automatic registration , the software brought the images in the correct alignment performing translations and rotations along the longitudinal axis up to 40 ( cid : 3 ) , while it was not satisfactory for rotations along the transverse axes . conclusion the experimental clinical application automatic registration is reliable if the voi tool that includes visible landmarks in both studies is used . 
however , because the algorithm did not prove sensitive to rotations along the transverse axes , the position of the patient during the examinations plays a crucial role . results showed that keywords radiotherapy treatment planning ( cid : 2 ) computed tomography ( cid : 2 ) magnetic resonance imaging ( cid : 2 ) image registration ( cid : 2 ) phantom ( cid : 2 ) quality assurance introduction radiotherapy relies on images to plan , guide , and assess treatments [ 1 ]  . 
spatially accurate medical images are , indeed , an essential tool in three - dimensional conformal radiation therapy ( 3d - crt ) and intensity - modulated radiation therapy ( imrt ) treatment planning [ 2 ]  . 
computed tomography ( ct ) is the current standard modality for image - based radiation therapy treatment planning because of its ability to convert hounseld units ( hu ) into electron densities [ 3 ]  . a few years after the introduction of ct in routine clinical practice , it became clear that coupling of information provided by ct with that coming from other diagnostic modalities would improve the quality of the denition of tumours [ 4 ]  . 
this is divided into two phases : registration , which achieves the spatial alignment of the two studies , followed by fusion , which consists in the visual representation and combination of data [ 10 ]  . 
the techniques to perform this process are different , but all include the same basic components : the transformation model ( rigid , afne , projective and deformable ) and the metric ( geometry - based and voxel - based )  . another important feature is the level of interaction between the registration algorithm and the user . 
in the semi - automatic case , the interaction can be of two different kinds : the user can initialise the algorithm ( such as segmenting the data ) , or drive the algorithm ( i.e. , by refusing or accepting the suggested registration ) [ 11 , 12 ]  . the timing required in clinical application undoubtedly favours an automated approach to the image registration both as regards the speed of the operation as its standardisation . nevertheless , it requires a careful analysis of the effectiveness of registration , with the purpose of correcting and / or limiting errors that may occur in clinical implementation [ 13 ]  . that each radiotherapy application demands requirements of quality assurance ( qa ) protocols are met . therefore , also image registration applied to planning and execution of treatment requires a verication of results [ 1 ]  . several groups recommend guidelines for qa of registration in radiosurgery and general planning [ 3 , 1418 ]  . recently , the american association of physicists in medicine ( aapm ) formed task group 132 to review techniques for image registration , to identify issues related to their clinical implementation , to determine the best methods to assess accuracy and to outline issues related to acceptance and qa [ 1 ]  . many reports describe methods and evaluations for registration in the head and neck region [ 3 , 17 , 19 , 20 ] ; far fewer describe results for the pelvis [ 6 , 21 , 22 ]  . 
in this case , as the delineation of the target volume is an important source of geometric uncertainty , it is becoming customary to integrate ct and mri studies [ 13 ]  . the main objective of this work was to evaluate the accuracy of the registration of ct and mri images performed by a software dedicated to treatment planning ( focal , elekta )  . 
for this purpose , a phantom [ stylized anatomy with a registration objective ( s.a.r.o. ) ] dedicated to quality control for the registration of images obtained by ct and mri scanners was designed and built . 
it reproduces in a stylised way that the planning target volume ( ptv ) and organs at risk ( oars ) related to the treatment of the prostate . materials and methods the properties of focal software and s.a.r.o. 
phantom and the main steps of the analysis protocol are described below . description of the registration algorithm the registration algorithm of the focal software uses as a metric mutual information ( mi ) , a voxel - based metric which measures the statistical dependence of information between intensities of corresponding voxels in both images . 
it is supposed that mi is maximum when the two studies are geometrically aligned [ 23 ]  . moreover , the registration algorithm uses a model of rigid transformation with six degrees of freedom : three translations and three rotations . 
a rigid transformation can be described by a single matrix equation in homogenous coordinates by : where , xi and yi ( i = 1 , 2 , 3 ) are , respectively , the components of the new and the old coordinate vectors of the voxel , t is an arbitrary translation vector and r is a 3 9 3 rotation matrix dened by : ril r1 i ; j r2 j ; k r3 with r1 r2 r3 sin a1 0 cos a1 ( cid : 3 ) sin a1 cos a1 sin a2 cos a2 ( cid : 3 ) sin a2 cos a2 cos a3 ( cid : 3 ) sin a2 sin a3 cos a3 each matrix r ( i ) rotates the image about the ith axis by an angle ai [ 11 , 12 ]  . 944 radiol med ( 2014 ) 119 : 942950 once chosen the set of reference images , which constitute the primary study and will be kept xed , the algorithm will perform transformations on the other set of images , the secondary study , until the correct alignment is achieved . finally , focal provides that the transformations are carried out through a semi - automatic interaction with the user . 
once the primary and secondary studies are selected , the software proposes a rst registration founding its calculation on the entire content of the images ( intensity of each voxel )  . 
to check the alignment , the software shows the result of the fusion in various modalities ( panels , strips , merging of voxels ) and in each section ( axial , sagittal , coronal )  . 
it also shows the parameters and the transformation matrix as well as the value of mi in the current alignment . to improve the registration quality , it is possible to select a limited region in the three axes [ volume of interest ( voi ) tool ] within which the algorithm calculates the mi and performs its maximisation . 
since mi is a measure of the information common to both images , the selection of a region with well - dened landmarks allows the mi to be increased and the registration to be improved . 
although the selection of voi is user - dependent , even in this case the registration is automatic . finally , the user can customise the registration by directly applying the necessary transformations to the secondary study , assisted by a continuous view of the two studies in fusion on the three sections . description of the phantom the accuracy of the registration algorithm was evaluated by performing a study on a phantom with appropriate inserts of known size and composition . 
it simulates the pelvis region in a stylised way and it is dedicated to the registration of ct and mri images : s.a.r.o. the phantom consists of a cubical tank ( volume of 200 mm3 ) in which the landmarks shown in fig . 
figure 1 shows the axial section of the phantom with the corresponding anatomical landmarks , while table 1 shows the main properties of the inserts . since the two modalities are based on different physical principles , it is necessary to use materials that give signicant signals in both . 
for this reason , inserts are made of pmma , pvc and teon , tissue - equivalent materials in ct acquisition with slightly different densities , but that provide very weak signals in mri acquisition . 
were acquired with a 64 - slice multislice ct600 scanner ( ge medical systems ) using a protocol for radiotherapy treatment of the pelvis . mri images were acquired with a signahdtx scanner ( ge medical systems ) using a protocol suggested by literature regarding the radiotherapy treatment of the prostate [ 14 ]  . 
table 2 shows the main parameters of the ct and mri images . automatic and manual registration the rst part of the study was dedicated to the verication of automatic registration with focal . radiol med ( 2014 ) 119 : 942950 manual registration : the registration is performed manually by means of a visual inspection of the images in fusion . 
the new transformation parameters are marked down to be compared with those of automatic registration . in this way , it is possible to verify if the automatic registration is comparable to the manual registration . repeatability of the registration transformation parameters , a after identifying the best further study was conducted on the repeatability of the transformation performed by the software . for this purpose , a reverse approach was carried out : starting from the ideal alignment , known transformations were performed to the correctly aligned secondary study to verify whether and to what extent the algorithm was able to return to its original position . 
deviations were calculated using the following expression : transformation between where wi , t are the transformation parameters ( translations and rotations along the ith axes ) imposed to the properly aligned secondary study and wi , a are the transformation parameters found by the software . 
a correct transformation corresponds to a situation in which wi , t and wi , a are equal and opposite and , therefore , dwi equal to zero . results the analysis involved testing the as mentioned above , accuracy of the registration algorithm and the repeatability of the transformations the automatic version of ct computed tomography , mri magnetic resonance imaging , fov eld of view dwi wi ; t wi ; a fig . 
phantom during the ct acquisition table 2 main characteristics of the images acquired in the two modalities slice thickness matrix size 5 mm 500 mm 512 9 512 5 mm 400 mm 512 9 512 once the ct series had been selected as the primary study and the mri series as the secondary study , the analysis was divided into three sections . global registration : the software performs an automatic registration basing its calculation on the overall content of images . 
hence , the studies are shown in fusion , and it is possible to assess directly the registration quality . registration with voi tool : through this tool , the region in which the landmarks are visible is selected on the three sections ( axial , coronal , and sagittal ) , as shown in fig . 
the results of the study are shown below . automatic registration the automatic registration performed using the entire contents of the images showed the limits of this procedure . figure 4 shows the fusion of the ct study ( upper panel ) and the mri study ( lower panel ) after this transformation . the overlap of images indeed , the translation returns , belonging to different planes . table 3 shows the transformation parameters and the corresponding matrix . 
the expressions x ( r ? l ) , y ( s ? i ) and z ( a ? p ) indicate , respectively : translation from right ( r ) to left ( l ) , from cranial [ superior ( s ) ] to caudal [ inferior ( i ) ] and from anterior ( a ) to posterior ( p )  . the registration algorithm only ran translations along the three axes . 
as can be seen from this gure , the planes of the two studies coincide , as well as the position of landmarks . the parameters and the transformation matrix obtained through the voi tool are shown in table 4 . as a nal step , translations and rotations were performed manually based on a view of images in fusion . 
the error associated with the manual registration was evaluated by considering the spatial resolution of the images ( 1 mm in the axial plane , 5 mm in the sagittal and coronal planes )  . 
table 5 shows the parameters of the manual transformation and the corresponding matrix . comparing the results obtained with manual registration ( table 5 ) and those of automatic registration obtained by the voi tool ( table 4 ) , it can be noticed that the differences are minimal when compared to the spatial resolution of the images ( calculated from the eld of view size and the sampling matrix )  . 
these differences are included , according to the previously indicated resolution limit , in the error related to the manual registration . to quantitatively evaluate the accuracy of registration , the landmarks were contoured separately in the mri and ct studies . 
6. to further verify the correct operation of the algorithm , a registration of the ct study with itself was performed . the algorithm returned null values for each parameter and the transformation matrix corresponded with the identity matrix . 
for greater rotations , the algorithm was not able to nd the proper registration even with the use of the voi tool . rotations along x : the algorithm failed to nd the correct alignment for small rotations ( 2 ( cid : 3 ) ) even if the voi tool was used . rotations along z : as in rotations along the x axis , the algorithm , running into local maxima , failed to properly register the images with rotations of more than 2 ( cid : 3 )  . complex performing transformations : exclusively translations , the registration algorithm was able to properly align the studies , especially if the voi tool was used . 
table 6 shows some examples of deviations for rotations along y , x , z axis and an arbitrary translation along the three axes . as anticipated , for rotations along the x and z , even with the use of the voi tool , deviations remained signicant . discussion the major advances in radiation therapy have highlighted the need to improve the ability to locate and delineate tumour , healthy tissue and oars accurately . 
the nal image shows that the registration is satisfactory imposed and the for this purpose , the differences between the transfortransformation mation parameters parameters found by the software to properly align the two studies were evaluated . 
although physical spatial resolution along the coronal and sagittal planes is 5 mm , 0.001 mm ( as can be seen in the tables showing the transformation parameters ) , a value that goes far beyond the spatial resolution of the images . 
since , this part of the study was addressed to the ability of the algorithm to nd numerically the same transformation parameters , the same limit was set for all three planes . algorithm computation grid extends to evaluate the automated version of focal , a global registration was rst performed , followed by a registration with voi tool . 
phantom was designed to ensure significant signals in both imaging modalities . first of all , the optimisation procedure of the registration requires , depending on the algorithm , some precautions during image acquisition . 
in addition , since any change in patient position and organ lling represent sources of geometric uncertainties , registration algorithms that use models of rigid transformation must be evaluated carefully to ensure acceptable coherence between the modalities employed . 
respecting these precautions in routine procedures already represents a denite improvement as regards both the quality of the registration and the required timing . during the study , after obtaining images of the phantom according to these precautions , an automatic registration was performed allowing the software to exploit the entire contents of the ct and mri images . 
for this reason , the registration of ct studies with other diagnostic studies is emerging strongly in many centres and it is becoming an integral part of treatment planning . to minimise the possibility of human or software errors , clinical image acquisition and registration processes should be managed where possible in an integrated way to ensure their cogency , sequentiality and reproducibility [ 1 ]  . 
the registration algorithm is , in its automatic version , reliable for rotations along the y - axis up to 40 ( cid : 3 ) only if the voi tool is used . 
the algorithm is indeed able to assure the alignment of the studies if the voi tool is used . on the other hand , automatic registration did not prove satisfactory with regard to rotations along the x and z axis . 
this leads to the criticism of the correct patient position in the two studies as even small differences could affect is therefore desirable to use appropriate outcome . systems for patient immobilization with high precision positioning . 
this objective is certainly favoured by performing the studies on the same day and at a short temporal distance from one another . conclusion this the main objective of this work was to verify the accuracy and the repeatability of the registration of ct and mr images using the automatic version of the focal software . for this purpose , images of the s.a.r.o. 
the results show that , using the manual registration as a reference because it allows one to visually assess the quality of alignment , automatic registration is comparable when the voi tool is in clinical used . applications , the algorithm is reliable and fast if the voi includes that are clearly visible on both modalities . 
the ndings of ceus were compared with those of contrast - enhanced computed tomography scans at level - 1 diagnostic tests . results out of the 22 patients , 21 were diagnosed with blunt pancreatic injury using ceus , including 8 patients with lesions in the neck of pancreas , 9 in the body , 3 in the tail and 1 in the head . 
using ct as a reference standard , the detection rate of ceus in blunt pancreatic trauma was 95.5 % ( 21 / 22 )  . conclusions ceus ndings can be used to provide a reliable diagnosis for blunt pancreatic trauma . 
ceus is thus promising in the assessment of blunt pancreatic trauma , especially in institutions where emergency ceus is used as an initial diagnostic instrument . keywords pancreas ( cid : 2 ) trauma ( cid : 2 ) diagnosis ( cid : 2 ) contrastenhanced ultrasonography ( cid : 2 ) microbubbles introduction trauma [ 1 ]  . 
however , pancreatic trauma is rare , occurring in about 0.2 % of patients with abdominal accompanied with a high mortality rate of 7080 % when injury involves the aorta , the superior mesenteric artery or the vena cava , which is adjacent to the pancreas . 
nie department of radiology , chinese peoples liberation army general hospital , beijing , china e - mail : nieyongkang@gmail.com radiol med ( 2014 ) 119 : 920927 pancreatic injuries result in complications ( severe haemorrhage , pancreatic stula , and abscess ) in 2030 % of cases and mortality in more than 20 % [ 2 ]  . prompt diagnosis of pancreatic injuries has been challenging , particularly in blunt trauma patients . 
diagnosis has relied on amylase levels , computed tomography ( ct ) scans , magnetic resonance imaging ( mri ) and ultrasound ( us ) , with various levels of success . 
this number rises to 84 % following 3 - h elapse between trauma and the time of measurement [ 2 , 7 , 8 ]  . undoubtedly , the best diagnostic tool for pancreatic trauma is ct [ 9 ]  . 
moreover , mr cholangiopancreatography ( mrcp ) can be more useful because it can demonstrate clear delineation of the duct and its integrity . however , ct and mr equipment is large and difcult to use at the bedside for early diagnosis , or at trauma scene for point - ofcare diagnosis . 
however , conventional us cannot sufciently display the location and severity of pancreatic lesions . the introduction of us contrast agents has led to an increase in the diagnostic accuracy of us in many organs , and the technique now has a wide range of applications [ 1115 ]  . 
in 2013 , cokkinos [ 16 ] reported that contrastenhanced us ( ceus ) accurately dened organ injuries , capsular extension and even vascular injury with very good correlation with ct . the portability of ceus makes it a good tool in trauma settings because examinations can be performed quickly at a patients bedside and benets patients with either stable or unstable haemodynamics . 
the purpose of our study was to present the application of ceus in diagnosing adult pancreatic injuries caused by blunt abdominal trauma . materials and methods this study was approved by the ethics committee of the chinese peoples liberation army general hospital and complies with the health insurance portability and ( hipaa )  . regulations , in accordance with our accountability act for ceus institutions examination and use of related data for future research was obtained from each patient ( or the patients relatives if he / she was unconscious )  . informed consent patients from march 2007 to june 2012 at two institutions equipped with modern laboratory , ultrasonographic and radiological equipment , a retrospective review of the charts of 22 consecutive patients with pancreatic injuries due to blunt abdominal trauma assessed by contrast - enhanced ct ( cect ) , was undertaken . the patients demographic data and the mechanism of injury were retrieved from the medical les . 
seven patients had isolated pancreatic injury and 15 patients had complex injury , including 4 with hepatic injury , 6 with splenic injury , 2 with renal injury , 2 with hepatic and splenic injuries , and 1 with renal and splenic injuries . 
the mechanisms of injury included accidental fall , motorcycle crash , motor vehicle crash , and automobile - pedestrian collision . ultrasound imaging the ultrasound contrast agent used in this study was sonovue ( bracco , milan , italy ) , which is a second - generation contrast medium approved in china in 2003 for diagnostic imaging . 
the agent consists of stabilised microbubbles containing inert gas ( sulphur hexauoride , 8 ll / ml of solution ) , and is covered by a phospholipid membrane [ 17 ]  . 
the intravenous injection of this contrast agent can be repeated . conventional us and ceus were performed at patients bedside in the emergency department , using a mobile sequoia 512 machine ( siemens medical solutions , mountain view , ca ) or a portable cx50 system ( philips medical systems , andover , ma )  . 
the scan settings ( including gain , 922 radiol med ( 2014 ) 119 : 920927 scanning depth , and time gain control ) were optimised on each target region independently . 
a lesion involving more than 50 % of the thickness of the pancreas indicated impending disruption [ 18 ] , the diagnosis of pancreatic ductal injury was done indirectly by using ceus . ct imaging following the instruction of the emergency department , all patients were scanned within 1 h of admission by an emergency systematic ct scan after or before ceus examination . 
differences between group means were determined with analysis of variance ( systat ver 13.0 , spss , inc , chicago , il ) with chi - square test , consistency checking t or t test , where applicable . 
using cect as a reference standard , ceus value in the diagnosis of blunt pancreatic trauma was evaluated . kappa values were calculated to assess inter - reader agreement on ceus and us . 
b contrast - enhanced transverse ultrasound image shows the injury site as an anechoic and hypoechoic perfusion defect area with an irregular border in the pancreatic body ( short arrows )  . 
these changes were also shown on the cect images . discussion pancreatic trauma , especially contusion , is a relative enigma , even in modern medical practice with advanced diagnostic technologies . 
however , delayed diagnosis of mild pancreatic injuries could cause major therapeutic challenge to the medical team and potentially disastrous situations for the patients . therefore , improving the sensitivity and specicity of diagnosing pancreatic injuries is essential for effective treatment . ceus has largely improved us accuracy in detecting parenchymal organ injury after blunt abdominal trauma [ 15 , 1921 ]  . 
it can help depict ndings that are not accessible on conventional us , such as tissue hypoperfusion , nonperfusion , hyperaemia and contrast extravasation . in 2006 , valentino et al . 
the portability of ceus makes it a good tool in trauma settings because examinations can be performed quickly at the patients bedside and benets patients with either stable or unstable haemodynamics . 
although a case study has been recently reported , the value of ceus in pancreatic injuries has not yet been evaluated with doubleblind comparisons of ceus and cect . on the ceus images and animations , pancreatic disruption or lacerations appear as anechoic and / or hypoechoic perfusion defect area in arterial and parenchymal phases , ideally with separated structures , which can be missed on conventional us images . 
b contrast - enhanced transverse ultrasound image shows the injury site as an anechoic and hypoechoic perfusion defect area with an irregular border in the pancreatic neck ( arrow )  . 
in this group , 16 patients were considered as having pancreas injuries by us on the basis texture . of pancreas enlargement and heterogeneous however , us did not conrm the lesion size and injury severity because it could not depict the lesion borders clearly . 
while ceus has signicantly improved the ability to visualise the peripancreatic space , the reason for this phenomenon may be the difference in blood supply , which makes it possible for ceus to have a better view of pancreas and peripancreatic microcirculation perfusion . 
of note , ceus visualised pancreatic ductal injury , which was consistent with cect . this study also showed that a ceus examination for pancreatic injuries could be completed in less than 5 min using a single dose of contrast agent with operators skill and experience . 
 ( 2 ) it is portable , therefore it can be performed in the emergency room , ct department and at the bedside in radiol med ( 2014 ) 119 : 920927 fig . 
especially for patients with unstable haemodynamics , ceus is the preferred imaging method . ( 3 ) the examination is timely , with a room time \5 min . ( 4 ) ceus examination can be simultaneously performed while performing other physical examination or resuscitation procedures . some disadvantages of ceus have also emerged in this study . 
 ( 2 ) ceus requires rapid and skilful diagnosis because the duration of a single ceus examination is only 68 min . ( 3 ) timely identication of major pancreatic ductal injury is imperative because delayed diagnosis is largely responsible for the high morbidity and mortality associated with blunt pancreatic trauma . 
either ceus or cect indirectly diagnosed pancreatic ductal injury on the basis of a lesion involving more than 50 % of the thickness of pancreas , and the diagnostic accuracy are both lower . 
endoscopic retrograde cholangiopancreaticography ( ercp ) is the most reliable diagnostic method to accurately dene the continuity of the main pancreatic duct following pancreatic trauma , and it has been strongly suggested as an effective procedure for diagnosis and therapeutic interventions , including stent placement [ 25 ]  . 
however , the invasive nature and associated complications are the major drawbacks of ercp , limiting its use in unstable and uncooperative patients . pancreatic injuries sustained by blunt abdominal trauma are extremely rare . 
it should not be intended as a substitute for ct , but as a selective possibility to boost the role of us in the initial screening of patients with pancreatic trauma . in conclusion , ceus showed the site of pancreatic injury as anechoic and / or hypoechoic perfusion defect region with irregular borders in both the arterial and parenchymal phases , on which basis the diagnosis can be 926 radiol med ( 2014 ) 119 : 920927 fig . 
d conventional us shows that the pancreatic neck injury has become larger , the thin pancreatic parenchyma remains ( arrow ) and a peripancreatic liquid collection has appeared on the 16th day after trauma . 
the purpose of this study was to analyse the radiological and clinicopathological features of sfts in the extracranial head and neck region . materials and methods we retrospectively reviewed the clinical , computed tomography ( ct ) , magnetic resonance imaging ( mri ) , and pathological features in 18 patients ( 12 men and 6 women ) , aged 1875 years , with histologically proven sfts in the extracranial head and neck region . fourteen patients underwent ct scanning and nine techniques included underwent mri . 
639 , zhi zao ju road , shanghai 200011 , china e - mail : xiaofengtao2012@126.com enhancing and slow washout pattern on dynamic contrastenhanced mri and dual - phase ct . 
rapidly enhancing and slow washout pattern tics may be additional valuable features . keywords solitary brous tumours ( cid : 2 ) head and neck ( cid : 2 ) magnetic resonance imaging ( cid : 2 ) dynamic contrast enhanced imaging ( cid : 2 ) diffusion - weighted imaging ( cid : 2 ) computed tomography solitary brous tumours computed tomography abbreviations sfts mri magnetic resonance imaging diffusion weighted imaging dynamic contrast enhanced introduction solitary brous tumours ( sfts ) are mesenchymal neoin the pleura [ 1 ]  . frequently occur plasms that most although rare , there has been an increasing incidence of the tumour being found in extrapleural sites such as the abdomen , pelvis , trunk and meninges . 
it can also arise in the extracranial head and neck region such as the orbit , cheek , laryngeal , parapharyngeal space , oral cavity and thyroid gland [ 2 , 3 ]  . radiol med ( 2014 ) 119 : 910919 despite their characteristic , histological and immunohistochemical features , sfts of the extracranial head and neck region remain a diagnostic challenge to both clinicians and radiologists , because they are often poorly recognised and confused with other more common neoplasms . 
here , we conduct a retrospective review of the computed tomography ( ct ) and magnetic resonance ( mr ) imaging features of these 18 cases of sfts and evaluate the clinicopathological features and prognosis . there is only somewhat materials and methods from june 2004 to december 2012 , review of medical records based on the electronic data base of our institution , approved by our institutional review board , revealed 18 patients with pathology - proven sfts occurring in the extracranial head and neck region . 
we retrospectively reviewed the ct and mr ndings obtained from these patients . all ct scans ( 14 patients ) were obtained with a light speed 16 ( ge healthcare , milwaukee , wi , united states ) or brilliance 64 ( philips healthcare , best , the netherlands )  . 
of the 14 patients , 2 underwent plain ct scan only and 12 underwent contrast - enhanced ct scan ( three with single - phase ct with a 45 - s delay and nine with dual - phase ct with 30 and 60 s delay ) [ 4 ]  . 
the scanning parameters were as follows : 5 - mm slice thickness with 11.25 mm reconstructions , 23 cm eld of view ( fov ) , 120140 kv voltage , 200300 ma current , and 256 9 256 matrix . 
a imaging protocols neurovascular array coil was used . contained at least an unenhanced axial t1 - weighted ( tr / te , 600 / 11 ms ) spin - echo sequences , axial t2 - weighted ( tr / te 4 , 700 / 85 ms ) fast spin - echo sequences with fat saturation , and coronal t2 - weighted ( tr / te 3 , 200 / 100 ms ) fast spin - echo sequences ; and contrast - enhanced axial , and coronal t1 - weighted ( tr / te 600 / 11 ms ) sequences . 
an intravenous dose of 0.1 mmol / kg of contrast agent ( gadolinium - dtpa , magnevist ; schering ) had been administered to the patients undergoing conventional contrast - enhanced mri . 
the dwi parameters were as follows : tr / te , 2 , 5003 , 000 / 70 ms for a b factor of 0 and 1 , 000 s / mm2 , thickness / space , 5 / 0.5 mm ; matrix , 128 9 128 ; fov , 24 cm ; and eight acquisitions . the ct and mr images were reviewed by two dedicated head and neck radiologists in consensus . 
we evaluated the imaging ndings with emphasis on the number , size , margin , shape , internal architecture , and pattern and degree of enhancement of the lesion [ 4 ]  . 
as for internal architecture , we compared the attenuation of the lesion on plain ct and the signal intensity of the lesion on t1and t2weighted mr images with that of the neck musculature . we also recorded the presence of any calcications based on plain ct scans . 
as for the degree of enhancement on ct scan , we relied on early - phase contrast - enhanced axial images , viewed with the same window width ( 350 hu ) and level ( 40 hu )  . 
in nine patients examined with dual - phase ct , we also measured the attenuation values in the axial plain , earlyand late - phase ct scans to plot the time - attenuation graph . 
apparent diffusion coefcient ( adc ) values were obtained on dwi , and the time - intensity curves ( tics ) and the maximum slope of increase on dce - mri . clinical data were retrieved from the medical records . sixteen patients underwent complete excision of tumour and two patients underwent partial excision at our institution . 
immunohistochemical included staining for cd34 , vimentin , cd99 , b cell lymphoma protein 2 ( bcl - 2 ) , s - 100 protein , smooth muscle antibody ( sma ) and cytokeratin analysis table 1 summary of clinical ndings in 18 patients case age / sex symptom preoperation diagnosis treatment follow - up ( months ) radiol med ( 2014 ) 119 : 910919 30 / m 27 / m 68 / m 55 / m 23 / f 49 / m 22 / m 59 / f 18 / f 54 / m 31 / m 62 / m 48 / f 46 / m 45 / m 75 / f 24 / f 49 / m proptosis palpable mass facial palsy palpable mass proptosis proptosis sore pain palpable mass sore pain sore pain palpable mass palpable mass palpable mass palpable mass swelling proptosis r ; parotid gland adenolymphoma oropharynx bleeding l ; parapharyngeal space pleomorphic adenoma palpable mass l ; parapharyngeal space schwannoma sfts haemangioma haemangioma haemangioma haemangioma sfts schwannoma location r ; orbit r ; masticator space l ; masticator space r ; orbit r ; orbit r ; maxillary l ; orbit l ; orbit l ; cheek r ; cheek l ; orbit l ; orbit r ; infratemporal fossa r ; cheek malignant neoplasm malignant neoplasm l ; submandibular space haemangioma granulomatous lesions schwannoma / sfts haemangioma / sfts malignant neoplasm schwannoma / haemangioma complete complete complete complete complete complete complete complete complete partial complete partial complete complete complete complete complete complete lost m male , f female , r right , l left , sft solitary brous tumour , complete complete excision , partial partial excision ( ck )  . 
prognosis was assessed by clinic service and telephone interview . operation , 17 patients were in good health with no evidence of recurrent tumour during a follow - up of 2102 months ( mean 36 months )  . results clinical data the clinical features of 18 patients with sfts in the extracranial head and neck region are summarised in table 1 . 
seven of the 18 lesions arose from the orbit , 3 / 18 from the cheek , 2 / 18 from the masticator space , 2 / 18 from the parapharyngeal space , 1 / 18 from the infratemporal fossa , 1 / 18 from the maxillary , 1 / 18 from the submandibular space , and 1 / 18 from the parotid gland . 
sfts were often misdiagnosed as being another type of common tumour , such as cavernous haemangioma ( 7 / 18 ) , schwannoma ( 4 / 18 ) , pleomorphic adenoma adenolymphoma ( 1 / 18 )  . 
after the granulomatous lesions ( 1 / 18 ) , ( 1 / 18 ) imaging ndings the ct and mr imaging features of 18 patients with sfts in the extracranial head and neck region are summarised in table 2 . 
the presence of rounded or linear tissues low - intensity foci was attributable to the collagen content , low cellularity , and associated reduced proton mobility . sfts are vascular tumours that are vigorously enhancing . discussion solitary brous tumours are rare spindle - cell neoplasms originating from mesenchymal tissue . 
although mostly occurring in the pleura , this tumour has also been recently reported in a number of extrapleural sites , including the mediastinum , lung , liver , pancreas , retroperitoneum , kidney , meninges , and extracranial head and neck region such as the orbit , nasal cavity , paranasal sinus , epiglottis , thyroid gland , salivary gland , infratemporal fossa , buccal space and parapharyngeal space [ 2 , 3 ]  . 
in our study , 18 sfts in extracranial head and neck region were located in the orbit , cheek , masticator space , the parapharyngeal space , infratemporal fossa , maxillary , submandibular space and the parotid gland , respectively . clinically , the symptoms and signs of sfts depend on the location of the tumour and the involved organs or tissues , as shown in our series . 
k the inlet shows that the tumour cells and the capillary endothelial cells have immunohistochemically positive cd34 results ( original magnication 9200 )  . l immunohistochemistry of the tumour cells showing positive staining for vimentin ( original magnication 9200 ) space , the initial symptom may not be obvious , and their sizes are usually much bigger . 
patients with sfts occurring in the supercial soft tissues like the parotid gland often present with an asymptomatic palpable mass . sft most commonly present during the fth and sixth decades of life , and there is no signicant sex predilection [ 6 ]  . 
in our study , the age range was also 1875 years , but the incidence was higher in men than in women with a sex ratio of 12 : 6 . 
although local excision is usually curative , sfts have been reported to recur and metastasise . complete surgical excision appears to be the treatment of choice for sfts in the extracranial head and neck region . the prognosis of sfts might be strongly related to initial treatment , and total resection is associated with longer progression - free survival [ 7 ]  . 
in our series , except for one patient who was lost to follow - up , the remaining patients made uneventful recoveries and they are still clinically and radiologically free from tumour recurrence during the follow - up period . microscopically , sfts are well - circumscribed , nonencapsulated tumours that are known to have a characteristic patternless arrangement of alternating hypercellular and hypocellular regions of spindle cells against a collagenous background of variable vascularity . 
in addition to cd34 , sfts are also immunoreactive for mesenchymal markers ( vimentin ) , but they are usually negative for epithelial , vascular , neural and muscle markers [ 8 ]  . 
in our study , sfts were immunoreactive for cd34 , vimentin , partial cd99 and bcl - 2 , but negative for s - 100 protein , ck and sma . 
out of the 18 cases , we were able to identify only 3 cases as having atypical or malignant features . the reported imaging ndings of sfts in the extracranial head and neck region are rather nonspecic [ 9 ]  . 
 [ 11 ] , sfts were mostly isodense on plain ct , homogeneously isointense or mildly hypointense to muscle on the t1 - weighted images , and heterogeneously and mildly hyperintense on the t2 - weighted images . 
 [ 4 ] reported that isointensity to hypointensity on t2weighted images reected brous tissue with high collagen content , and hyperintensity was related to internal haemorrhage , cystic degeneration , or relatively fresh brosis . 916 radiol med ( 2014 ) 119 : 910919 fig . 
a the t1 - weighted image shows a well - dened , irregular mass ( star ) is isointense to muscle with inner hypointense linear septa ( arrow )  . 
we also believe that this variable signal intensity depends mainly on the differences in the main components of the tumour , namely , the amount of cellular components , collagen and broblasts , and also on the presence of degeneration . 
we also observed an interesting nding , that is , the linear septa within the tumours in two cases . those lines corresponded to the hypocellular collagenous stroma intervening in the hypercelluar area . 
even if these hypointense lines were not specic for sfts , we suggest 918 table 3 summary of the histological features of sfts in the present series case benign / malignant cd34 vimentin cd99 bcl - 2 s - 100 benign benign benign benign benign benign benign borderline benign benign malignant malignant benign benign benign benign benign benign radiol med ( 2014 ) 119 : 910919 ? positive ; negative ; partial positivity that they are helpful for including this rare tumour in the differential diagnosis of masses involving the extracranial head and neck region . 
large necrosis or cystic degeneration was present in one case which was proven to be the malignant neoplasm . enhancement of a certain tumour can best be assessed radiologically by dynamic ct or mr imaging . 
in this study , all nine lesions examined with dual - phase ct demonstrated rapid , intense enhancement at early - phase axial scanning , followed by slow washout of contrast material at on late - phase axial images . 
on the dce - mri , the tics also exhibited a rapidly enhancing and slow washout pattern in our cases , which may be an additional clue to establish the correct diagnosis . 
 [ 4 ] reported that the timeattenuation curves of orbital sfts on dual - phase ct demonstrated rapid , intense enhancement at early - phase axial scanning , followed by signicant progressive washout of contrast material at late - phase axial and delayedphase coronal scanning . the dwi ndings of the sfts in the extracranial head and neck region have been rarely reported . 
owing to the limited number of cases , we could not compare adc values between the benign and malignant sfts . on the basis of the aforementioned imaging ndings for sfts of the extracranial head and neck region , this tumour is often misdiagnosed as other common tumours on the initial images , such as cavernous haemangioma , schwannoma , pleomorphic adenoma and adenolymphoma . 
in our cases , cavernous haemangioma and schwannoma should be the main lesions to be included in the differential diagnosis . cavernous haemangiomas may be the most difcult tumours to differentiate from sfts in the extracranial head and neck region on imaging studies . 
their typical feature shows phleboliths in the tumour which are hyperdense on plain ct scan , hypointense on both t1 - weighted and t2 - weighted images and unenhanced on the contrast - enhanced images . 
on the other hand , the other parts show marked hyperintensity on t2weighted images with fat saturation , and delayed pooling of contrast material on dynamic studies [ 15 , 16 ]  . 
they are usually solitary , slowly growing benign lesions and , along with neurobromas , they are the most common nerve sheath tumours . radiol med ( 2014 ) 119 : 910919 extracranial schwannomas have a distinct tendency to originate in the head and neck region . 
unlike sfts , schwannomas have more cystic degeneration , so they are heterogeneously hyperintense on t2 - weighted images and show moderate heterogeneous enhancement on t1 - weighted contrast - enhanced images . 
a solitary , ovoid and well - dened mass with isodensity on plain ct , isointensity on t1 - wi , mild hyperintensity on t2 - wi and strong enhancement after contrast agent injection is suggestive of this diagnosis . 
the prognosis of sfts might be strongly related to initial treatment , and total resection is associated with longer progression - free survival . acknowledgments the authors thank henghua zhou for her help in pathology . 
signal changes and enhancement of vertebral bodies , involvement of paravertebral soft tissues and epidural spaces , nerve root and cord compression and abscess formation were assessed . results of 63 patients with spinal brucellosis , eight had thoracic , 35 had lumbar , ten had cervical vertebral , seven had both thoracic and lumbar , and three had both lumbar and sacral vertebral involvement . 
zhang ( & ) department of orthopaedics , yuncheng central hospital , yuncheng 044000 , shanxi , china e - mail : zhangqin19762@126.com conclusion brucella is still a public health problem in endemic areas . 
mr imaging is a highly sensitive and noninvasive imaging technique which should be rst choice spondylodiscitis . diagnosis imaging early keywords spine ( cid : 2 ) brucella ( cid : 2 ) spondylodiscitis ( cid : 2 ) mri introduction situation became more brucellosis is a systemic infection caused by genus brucella which is a facultative intracellular organism [ 1 ]  . although rarely found in industrialised countries , it is still endemic and considered a public health problem in many developing countries including china [ 2 ]  . 
osteoarticular manifestations , including sacroiliitis , peripheral arthritis , spondylitis , osteomyelitis , and bursitis are the most frequent complications of brucellosis and occur in one - third of the patients [ 5 ]  . 
diagnosing brucellar spondylodiscitis is often difcult ; clinical ndings are usually nonspecic , and radiological features may mimic those of other bacterial , fungal , inammatory , and neoplastic diseases . 
it has been reported that magnetic resonance ( mr ) imaging can differentiate brucellar spondylitis from other spinal infections , along with a good clinical background [ 68 ]  . severe the aim of this retrospective study was to report the clinical features and imaging ndings of patients with brucellar spondylodiscitis . 929 radiol med ( 2014 ) 119 : 928933 fig . 
b the t1 - weighted image reveals hypointense signal intensities corresponding to the same level . c fat - suppressed t2 - weighted image showing hyperintense signal intensities corresponding to the same level . 
d t2weighted axial image showing increased homogeneous signal intensity due to paravertebral abscess materials and methods this retrospective study included 63 cases ( 19 women and 44 men ; mean age 54.7 years ; age range 1874 years ) of brucellar spondylodiscitis , recruited from the archive system of the imaging services among 314 patients with presumed spondylodiscitis by the department of infectious diseases between 2009 and 2012 . 
the diagnosis of brucella infection was considered when seroagglutination tests were positive at a titre of 1 / 160 or higher , and / or brucella spp . was isolated in the blood or sample cultures . 
the diagnosis of spinal brucellosis was made upon ndings consistent with infection in at least one vertebra or intervertebral disc on mr imaging , and positive clinical ndings . each patients medical history , physical examination and laboratory ndings were recorded . 
all of the images were evaluated by two radiologists and a diagnosis was made . results the study involved 19 ( 30 % ) female and 44 ( 70 % ) male patients with spondylodiscitis ( mean age 54.7 , range 1874 )  . 
b the t1 - weighted image reveals hypointense signal intensities corresponding to the same level . c fat - suppressed t2 - weighted image showing hyperintense signal intensities corresponding to the same level . 
thirteen patients had cord compression , six had root compression , four had facet - joint involvement and one had erector spinae muscle involvement at multiple levels . gibbus deformity was not observed in any patient . 
in the acute stage , mr imaging showed low signal intensity on t1 - weighted images and high signal intensity on t2weighted images of the vertebral bodies , endplates and intervertebral disc space . 
infectious spondylitis is an infection by a specic organism of one or more components of the spine , namely , intervertebral discs , paraspinal abnormal soft tissues , and epidural space . 
a the t2 - weighted image shows a focal epidural collection at the posterior aspect of the c6 and c7 bodies . b the t1 - weighted image reveals hypointensity signal intensities at the posterior aspect of the c6 and c7 bodies . 
c a sagittal gadoliniumenhanced , t1 - weighted magnetic resonance imaging scan of the cervical spine shows an epidural uid collection with an enhancing rim , representing an epidural abscess . 
c fat - suppressed t2 - weighted and adjacent image showing hyperintense signal intensities correspond to the same level at the t1 - weighted image erythrocyte sedimentation rate ( esr ) in patients with spondylitis [ 13 ]  . 
the sexes were affected equally . 932 radiol med ( 2014 ) 119 : 928933 according to the time from onset of symptoms in the group with spondylitis , 17 ( 26 % ) brucellosis patients were classied as acute and 31 ( 49 % ) as subacute . 
generally , two vertein six patients , three adjacent brae were involved , but vertebral bodies were involved , these involved vertebrae are mostly contiguous , but noncontiguous spine levels are rare in brucella spondylodiscitis [ 16 ]  . 
cervical involvement , however , is accompanied by more severe manifestations , due to frequent epidural masses with spinal cord compression and neurological disabilities [ 1821 ]  . superior endplate is the rst involved part of the vertebrae because of its rich blood supply and causes bone destruction in the early stage [ 9 , 22 ]  . 
however , epidural masses may be together with spondylodiscitis and sometimes compress nerve roots or spinal cord and mimic disc herniation , which occurred in three of our patients . mr imaging is very useful in differentiating brucellar spondylodiscitis from other spinal pathologies , including tuberculous spondylitis , pyogenic spondylitis , postoperative changes , spinal degenerative diseases , and vertebral metastases [ 9 , 23 ]  . 
in the acute stage , mr imaging depicted low and high signal intensities on t1 and t2 - weighted images , respectively , on vertebral bodies , vertebral end plates and intervertebral discs [ 11 , 22 , 24 , 25 ]  . 
in the subacute and chronic stages , mr imaging revealed hypointense and heterogeneous signal intensities in t1and t2 - weighted images , respectively . contrast - enhanced images reveal contrast enhancement of discs and affected vertebrae in acute , subacute and chronic stages [ 26 ]  . 
paravertebral and / or epidural abscess formation is a rare nding , compared with other infective spondylodiscitis in brucella spondylodiscitis involvement of vertebral mostly unifocal , but multifocal and multilevel involvements may also be seen [ 27 ]  . 
for this reason , the initial clinical evaluation of the patient segments acute [ 5 ]  . with other laboratory ndings like c - reactive protein ( crp ) and esr and follow - up of the patients symptoms and response to therapy are very important in the consideration of spinal involvement . spinal brucellosis may mimic other diseases that affect the spine , such as tuberculous spondylitis , pyogenic osteomyelitis . 
tuberculous ( tb ) spondylitis remains the most important disease in differential diagnosis because of similar mr imaging appearances of both diseases in some cases [ 28 , 29 ]  . 
the size of the paraspinal mass in tb spondylitis is usually larger than paraspinal mass of brucellar spondylitis [ 30 , 31 ]  . imaging modalities and is very useful spondylodiscitis is a rare but important complication of brucellosis which can cause transient or persistent neurological decits resulting in spinal deformities if not appropriately treated . 
the ndings of ceus were compared with those of contrast - enhanced computed tomography scans at level - 1 diagnostic tests . results out of the 22 patients , 21 were diagnosed with blunt pancreatic injury using ceus , including 8 patients with lesions in the neck of pancreas , 9 in the body , 3 in the tail and 1 in the head . 
using ct as a reference standard , the detection rate of ceus in blunt pancreatic trauma was 95.5 % ( 21 / 22 )  . conclusions ceus ndings can be used to provide a reliable diagnosis for blunt pancreatic trauma . 
ceus is thus promising in the assessment of blunt pancreatic trauma , especially in institutions where emergency ceus is used as an initial diagnostic instrument . keywords pancreas ( cid : 2 ) trauma ( cid : 2 ) diagnosis ( cid : 2 ) contrastenhanced ultrasonography ( cid : 2 ) microbubbles introduction trauma [ 1 ]  . 
however , pancreatic trauma is rare , occurring in about 0.2 % of patients with abdominal accompanied with a high mortality rate of 7080 % when injury involves the aorta , the superior mesenteric artery or the vena cava , which is adjacent to the pancreas . 
nie department of radiology , chinese peoples liberation army general hospital , beijing , china e - mail : nieyongkang@gmail.com radiol med ( 2014 ) 119 : 920927 pancreatic injuries result in complications ( severe haemorrhage , pancreatic stula , and abscess ) in 2030 % of cases and mortality in more than 20 % [ 2 ]  . prompt diagnosis of pancreatic injuries has been challenging , particularly in blunt trauma patients . 
diagnosis has relied on amylase levels , computed tomography ( ct ) scans , magnetic resonance imaging ( mri ) and ultrasound ( us ) , with various levels of success . 
this number rises to 84 % following 3 - h elapse between trauma and the time of measurement [ 2 , 7 , 8 ]  . undoubtedly , the best diagnostic tool for pancreatic trauma is ct [ 9 ]  . 
moreover , mr cholangiopancreatography ( mrcp ) can be more useful because it can demonstrate clear delineation of the duct and its integrity . however , ct and mr equipment is large and difcult to use at the bedside for early diagnosis , or at trauma scene for point - ofcare diagnosis . 
however , conventional us cannot sufciently display the location and severity of pancreatic lesions . the introduction of us contrast agents has led to an increase in the diagnostic accuracy of us in many organs , and the technique now has a wide range of applications [ 1115 ]  . 
in 2013 , cokkinos [ 16 ] reported that contrastenhanced us ( ceus ) accurately dened organ injuries , capsular extension and even vascular injury with very good correlation with ct . the portability of ceus makes it a good tool in trauma settings because examinations can be performed quickly at a patients bedside and benets patients with either stable or unstable haemodynamics . 
the purpose of our study was to present the application of ceus in diagnosing adult pancreatic injuries caused by blunt abdominal trauma . materials and methods this study was approved by the ethics committee of the chinese peoples liberation army general hospital and complies with the health insurance portability and ( hipaa )  . regulations , in accordance with our accountability act for ceus institutions examination and use of related data for future research was obtained from each patient ( or the patients relatives if he / she was unconscious )  . informed consent patients from march 2007 to june 2012 at two institutions equipped with modern laboratory , ultrasonographic and radiological equipment , a retrospective review of the charts of 22 consecutive patients with pancreatic injuries due to blunt abdominal trauma assessed by contrast - enhanced ct ( cect ) , was undertaken . the patients demographic data and the mechanism of injury were retrieved from the medical les . 
seven patients had isolated pancreatic injury and 15 patients had complex injury , including 4 with hepatic injury , 6 with splenic injury , 2 with renal injury , 2 with hepatic and splenic injuries , and 1 with renal and splenic injuries . 
the mechanisms of injury included accidental fall , motorcycle crash , motor vehicle crash , and automobile - pedestrian collision . ultrasound imaging the ultrasound contrast agent used in this study was sonovue ( bracco , milan , italy ) , which is a second - generation contrast medium approved in china in 2003 for diagnostic imaging . 
the agent consists of stabilised microbubbles containing inert gas ( sulphur hexauoride , 8 ll / ml of solution ) , and is covered by a phospholipid membrane [ 17 ]  . 
the intravenous injection of this contrast agent can be repeated . conventional us and ceus were performed at patients bedside in the emergency department , using a mobile sequoia 512 machine ( siemens medical solutions , mountain view , ca ) or a portable cx50 system ( philips medical systems , andover , ma )  . 
the scan settings ( including gain , 922 radiol med ( 2014 ) 119 : 920927 scanning depth , and time gain control ) were optimised on each target region independently . 
a lesion involving more than 50 % of the thickness of the pancreas indicated impending disruption [ 18 ] , the diagnosis of pancreatic ductal injury was done indirectly by using ceus . ct imaging following the instruction of the emergency department , all patients were scanned within 1 h of admission by an emergency systematic ct scan after or before ceus examination . 
differences between group means were determined with analysis of variance ( systat ver 13.0 , spss , inc , chicago , il ) with chi - square test , consistency checking t or t test , where applicable . 
using cect as a reference standard , ceus value in the diagnosis of blunt pancreatic trauma was evaluated . kappa values were calculated to assess inter - reader agreement on ceus and us . 
b contrast - enhanced transverse ultrasound image shows the injury site as an anechoic and hypoechoic perfusion defect area with an irregular border in the pancreatic body ( short arrows )  . 
these changes were also shown on the cect images . discussion pancreatic trauma , especially contusion , is a relative enigma , even in modern medical practice with advanced diagnostic technologies . 
however , delayed diagnosis of mild pancreatic injuries could cause major therapeutic challenge to the medical team and potentially disastrous situations for the patients . therefore , improving the sensitivity and specicity of diagnosing pancreatic injuries is essential for effective treatment . ceus has largely improved us accuracy in detecting parenchymal organ injury after blunt abdominal trauma [ 15 , 1921 ]  . 
it can help depict ndings that are not accessible on conventional us , such as tissue hypoperfusion , nonperfusion , hyperaemia and contrast extravasation . in 2006 , valentino et al . 
the portability of ceus makes it a good tool in trauma settings because examinations can be performed quickly at the patients bedside and benets patients with either stable or unstable haemodynamics . 
although a case study has been recently reported , the value of ceus in pancreatic injuries has not yet been evaluated with doubleblind comparisons of ceus and cect . on the ceus images and animations , pancreatic disruption or lacerations appear as anechoic and / or hypoechoic perfusion defect area in arterial and parenchymal phases , ideally with separated structures , which can be missed on conventional us images . 
b contrast - enhanced transverse ultrasound image shows the injury site as an anechoic and hypoechoic perfusion defect area with an irregular border in the pancreatic neck ( arrow )  . 
in this group , 16 patients were considered as having pancreas injuries by us on the basis texture . of pancreas enlargement and heterogeneous however , us did not conrm the lesion size and injury severity because it could not depict the lesion borders clearly . 
while ceus has signicantly improved the ability to visualise the peripancreatic space , the reason for this phenomenon may be the difference in blood supply , which makes it possible for ceus to have a better view of pancreas and peripancreatic microcirculation perfusion . 
of note , ceus visualised pancreatic ductal injury , which was consistent with cect . this study also showed that a ceus examination for pancreatic injuries could be completed in less than 5 min using a single dose of contrast agent with operators skill and experience . 
 ( 2 ) it is portable , therefore it can be performed in the emergency room , ct department and at the bedside in radiol med ( 2014 ) 119 : 920927 fig . 
especially for patients with unstable haemodynamics , ceus is the preferred imaging method . ( 3 ) the examination is timely , with a room time \5 min . ( 4 ) ceus examination can be simultaneously performed while performing other physical examination or resuscitation procedures . some disadvantages of ceus have also emerged in this study . 
 ( 2 ) ceus requires rapid and skilful diagnosis because the duration of a single ceus examination is only 68 min . ( 3 ) timely identication of major pancreatic ductal injury is imperative because delayed diagnosis is largely responsible for the high morbidity and mortality associated with blunt pancreatic trauma . 
either ceus or cect indirectly diagnosed pancreatic ductal injury on the basis of a lesion involving more than 50 % of the thickness of pancreas , and the diagnostic accuracy are both lower . 
endoscopic retrograde cholangiopancreaticography ( ercp ) is the most reliable diagnostic method to accurately dene the continuity of the main pancreatic duct following pancreatic trauma , and it has been strongly suggested as an effective procedure for diagnosis and therapeutic interventions , including stent placement [ 25 ]  . 
however , the invasive nature and associated complications are the major drawbacks of ercp , limiting its use in unstable and uncooperative patients . pancreatic injuries sustained by blunt abdominal trauma are extremely rare . 
it should not be intended as a substitute for ct , but as a selective possibility to boost the role of us in the initial screening of patients with pancreatic trauma . in conclusion , ceus showed the site of pancreatic injury as anechoic and / or hypoechoic perfusion defect region with irregular borders in both the arterial and parenchymal phases , on which basis the diagnosis can be 926 radiol med ( 2014 ) 119 : 920927 fig . 
d conventional us shows that the pancreatic neck injury has become larger , the thin pancreatic parenchyma remains ( arrow ) and a peripancreatic liquid collection has appeared on the 16th day after trauma . 
liver biopsy , the current gold standard for the diagnosis and staging of brosis and inammation , may be associated with complications such as bleeding , inherent limitations such as sampling error or interobserver variability and is not readily accepted by all patients [ 5 , 6 ]  . including biochemical and haematological noninvasive diagnosis of hepatic brosis has evolved rapidly in recent years [ 13 ]  . 
several noninvasive techtests niques , and a scoring system using a combination of clinical and laboratory tests are used to predict hepatic brosis , but predict their overlapping cannot results 904 radiol med ( 2014 ) 119 : 903909 necroinammatory activity [ 3 , 5 , 7 ]  . 
ultrasonographybased transient elastography , real - time elastography and acoustic radiation force impulse elastography are used for the evaluation of hepatic brosis but they are operator dependent and may be difcult in obese patients with narrow intercostal space [ 8 , 9 ]  . 
limited studies discuss the role of double - contrast magnetic resonance ( mr ) imaging , mr elastography and mr spectroscopy in the assessment of hepatic brosis in adults , but these pulse sequences are not widely available in clinical practice and their results are preliminary [ 10 , 11 ]  . diffusion - weighted mr imaging depends on the microscopic mobility of water protons . 
to our knowledge , no study to date has addressed the role of diffusion mr imaging in quantication of the degree of inammation in children with chronic hepatitis . the aim of this study was to prospectively evaluate the usefulness of the apparent diffusion coefcient ( adc ) value in the diagnosis and grading of hepatic brosis and inammation in children with chronic hepatitis . materials and methods this study was conducted on 53 consecutive untreated children with pathologically proven chronic hepatitis . three patients were excluded from the study due to motion artefacts at diffusion weighted mr imaging . 
informed consent from parents of patients and controls and institutional review board approval were obtained . mr examinations were performed using a 1.5 - t ( magnetom symphony ; siemens , erlangen , germany )  . 
the machine is equipped with a self - shielded gradient set ( 30 mt / m maximum gradient strength and 120 t / m / s slew rate ) for echoplanar imaging . 
the applied parameters were tr of 2 , 800 ms , te of 74 ms , epi factor of 102 , fov of 25 9 25 cm , section thickness of 7 mm , interslice gap of 20 % , acquisition matrix of 192 9 154 and number of excitations of 6 . 
the adc map was automatically calculated from the data set three b - values by commercially available obtained at software ( leonardo , version 2.0 ; siemens ag medical systems , forchheim , germany )  . 
the adc value was calculated according to the following formula : adc_ ( lnsb2 lnsb1 ) / ( b2 b1 ) , where ln is the natural log , and sb1 and sb2 are the signal intensities in the roi placed on sections corresponding to the two different b values ( b1 and b2 ) [ 30 , 31 ]  . 
the mean of these nine values was calculated and represents the nal adc value per subject that was used for statistical analysis . percutaneous liver biopsy was performed by a paediatric hepatologist ( b.t. ) with 7 years experience in liver biopsy . 
the stages of brosis were f0 ( no brosis ) , f1 ( mild expansion of some portal tracts by brosis ) , f2 ( expansion of most portal tracts by brosis ) , f3 ( occasional bridging brosis ) , f4 ( marked bridging brosis ) , f5 ( incomplete cirrhosis ) and f6 ( complete cirrhosis )  . 
the control children were regarded as having necroinammatory activity grade a0 and brosis stage f0 . statistical analysis was done using statistical package for the social sciences ( spss , inc . , chicago , il , usa ) software , version 16 . 
for statistical analysis , the stages of brosis were classied into mild ( f1 , f2 and f3 ) and advanced ( f4 , f5 and f6 ) and the grades of necroinammatory activity were classied into mild ( a1 , a2 ) and advanced ( a3 , a4 )  . receiver operating characteristic ( roc ) curves were done to evaluate the diagnostic capability of the adc value in differentiating hepatic brosis from normal liver , as well as in staging hepatic brosis and grading hepatic necroinammation . 
the area under the curve ( auc ) , sensitivity , specicity , accuracy , positive predictive value ( ppv ) and negative predictive value ( npv ) were calculated . 
diffusion mr imaging has been used for assessment of diffuse diseases in different regions of the body [ 4042 ] as well as in chronic diffuse liver diseases [ 1327 ]  . in the literature , various studies of diffusion mr imaging reported that adc values of hepatic brosis are lower than those of normal livers in adults [ 1421 ] and in children [ 29 ]  . 
in accordance with most of the previous studies [ 1623 ] , the adc values of the study group were also lower than the adc values of the control group . 
the mechanism of restricted diffusion in brosis is deemed to be multifactorial , mostly due to diminished hepatic perfusion and , to a lesser extent , to the presence of increased connective tissue , which contains fewer protons . 
the deposition of brous tissue leads to a reduction in the size or obliteration of small venules , with a resultant increase in portal venous pressure and consequent compensatory increased arterial blood ow [ 1517 ]  . 
the presence of increased connective tissue in the liver in addition to deposition of collagen bres , fatty inltration , hepatitis , cell necrosis / apoptosis and inammatory cell responsible for restricted diffusion with low adc value in patients with hepatic brosis [ 1419 , 29 ]  . inltration is the role of diffusion mr imaging in the study of diffuse liver disease , therefore , is still under debate . 
6 receiver operating characteristic ( roc ) curve of the adc value used for differentiating mild ( a1 , a2 ) from advanced ( a3 , a4 ) grades cutoff adc value was b1.64 9 10 - 3 mm2 / s with an auc of 0.807 , a sensitivity of 87.5 % , a specicity of 61 % and an accuracy of 74 % necroinammation . 
this may be attributed to more accurate calculation of the adc value in this study which was calculated from three b values ( 0 , 400 and 800 s / mm2 ) whereas other studies calculated the adc value only from two b values . 
last , this study was conducted on children who have better adc maps without noise or susceptibility artefacts compared to the adult patients . in this work , the adc value of hepatic parenchyma changed according to the stages of brosis . 
5 scatter plot of the adc value at different grades of hepatic necroinammation 908 radiol med ( 2014 ) 119 : 903909 know the usefulness of adc in distinguishing between the early and intermediate stages . 
also , linear regression analysis showed that hepatic adc values were a good predictor of brosis stage ( r2 = 0.19 , p = 0.0001 ) [ 19 ]  . in this study , there is a negative correlation between the adc values and necroinammatory activity . 
the adc value is signicantly lower in patients with high grades of hepatic inammation compared to those with low grades . the aggressiveness of chronic hepatitis is indicated by the degree of necroinammation , also called the activity ; the more severe the necroinammation , the more aggressive the disease . 
 [ 24 ] found a statistically relationship between the adc values and signicant hepatic activity index scores although this relationship was not as strong as that between adc values and brosis scores . 
in addition , entropy , which is a measure of the variability in the volume histogram analyses of the adc values , showed a greater correlation with the brosis stage and inammatory activity grade than did mean adc , with a sensitivity of 0.91 and a specicity of 0.92 in the detection of inammation [ 27 ]  . 
recent advances in mr software technology such as 3 t scanners with parallel imaging and respiratory triggering will likely continue to improve image quality and also promise the potential application of multiple and higher b values than 1 , 000 mm2 / s [ 43 , 44 ]  . 
also , further studies with application of diffusion tensor mr imaging with multichannel coils will likely improve the results [ 14 ]  . application of advanced postprocessing methods such as entropy [ 27 ] , bi - exponential , non - gaussian ( diffusion kurtosis ) modelling or k - means clustering algorithms [ 4447 ] may provide a better characterisation of diffuse liver disease . there are a few limitations to this study . 
second , we excluded three patients due to susceptibility artefacts , and we expect that future studies with application of parallel imaging will increase the image contrast and decrease susceptibility artefacts . 
if the registration method works correctly , parameters which bring the images into alignment must always be the same . results automatic registration performed by the software did not prove satisfactory , whereas if a specic tool [ volume of interest ( voi ) tool ] allowing the calculation to be limited to the landmark region was used , the registration s . 
stancampiano dipartimento di specialita` medico - chirurgiche , scuola di specializzazione in fisica medica , universita` degli studi di catania , via santa soa 78 , 95123 catania , italy parameters were comparable with those of the manual registration . 
regarding the repeatability of the automatic registration , the software brought the images in the correct alignment performing translations and rotations along the longitudinal axis up to 40 ( cid : 3 ) , while it was not satisfactory for rotations along the transverse axes . conclusion the experimental clinical application automatic registration is reliable if the voi tool that includes visible landmarks in both studies is used . 
however , because the algorithm did not prove sensitive to rotations along the transverse axes , the position of the patient during the examinations plays a crucial role . results showed that keywords radiotherapy treatment planning ( cid : 2 ) computed tomography ( cid : 2 ) magnetic resonance imaging ( cid : 2 ) image registration ( cid : 2 ) phantom ( cid : 2 ) quality assurance introduction radiotherapy relies on images to plan , guide , and assess treatments [ 1 ]  . 
spatially accurate medical images are , indeed , an essential tool in three - dimensional conformal radiation therapy ( 3d - crt ) and intensity - modulated radiation therapy ( imrt ) treatment planning [ 2 ]  . 
computed tomography ( ct ) is the current standard modality for image - based radiation therapy treatment planning because of its ability to convert hounseld units ( hu ) into electron densities [ 3 ]  . a few years after the introduction of ct in routine clinical practice , it became clear that coupling of information provided by ct with that coming from other diagnostic modalities would improve the quality of the denition of tumours [ 4 ]  . 
this is divided into two phases : registration , which achieves the spatial alignment of the two studies , followed by fusion , which consists in the visual representation and combination of data [ 10 ]  . 
the techniques to perform this process are different , but all include the same basic components : the transformation model ( rigid , afne , projective and deformable ) and the metric ( geometry - based and voxel - based )  . another important feature is the level of interaction between the registration algorithm and the user . 
in the semi - automatic case , the interaction can be of two different kinds : the user can initialise the algorithm ( such as segmenting the data ) , or drive the algorithm ( i.e. , by refusing or accepting the suggested registration ) [ 11 , 12 ]  . the timing required in clinical application undoubtedly favours an automated approach to the image registration both as regards the speed of the operation as its standardisation . nevertheless , it requires a careful analysis of the effectiveness of registration , with the purpose of correcting and / or limiting errors that may occur in clinical implementation [ 13 ]  . that each radiotherapy application demands requirements of quality assurance ( qa ) protocols are met . therefore , also image registration applied to planning and execution of treatment requires a verication of results [ 1 ]  . several groups recommend guidelines for qa of registration in radiosurgery and general planning [ 3 , 1418 ]  . recently , the american association of physicists in medicine ( aapm ) formed task group 132 to review techniques for image registration , to identify issues related to their clinical implementation , to determine the best methods to assess accuracy and to outline issues related to acceptance and qa [ 1 ]  . many reports describe methods and evaluations for registration in the head and neck region [ 3 , 17 , 19 , 20 ] ; far fewer describe results for the pelvis [ 6 , 21 , 22 ]  . 
in this case , as the delineation of the target volume is an important source of geometric uncertainty , it is becoming customary to integrate ct and mri studies [ 13 ]  . the main objective of this work was to evaluate the accuracy of the registration of ct and mri images performed by a software dedicated to treatment planning ( focal , elekta )  . 
for this purpose , a phantom [ stylized anatomy with a registration objective ( s.a.r.o. ) ] dedicated to quality control for the registration of images obtained by ct and mri scanners was designed and built . 
it reproduces in a stylised way that the planning target volume ( ptv ) and organs at risk ( oars ) related to the treatment of the prostate . materials and methods the properties of focal software and s.a.r.o. 
phantom and the main steps of the analysis protocol are described below . description of the registration algorithm the registration algorithm of the focal software uses as a metric mutual information ( mi ) , a voxel - based metric which measures the statistical dependence of information between intensities of corresponding voxels in both images . 
it is supposed that mi is maximum when the two studies are geometrically aligned [ 23 ]  . moreover , the registration algorithm uses a model of rigid transformation with six degrees of freedom : three translations and three rotations . 
a rigid transformation can be described by a single matrix equation in homogenous coordinates by : where , xi and yi ( i = 1 , 2 , 3 ) are , respectively , the components of the new and the old coordinate vectors of the voxel , t is an arbitrary translation vector and r is a 3 9 3 rotation matrix dened by : ril r1 i ; j r2 j ; k r3 with r1 r2 r3 sin a1 0 cos a1 ( cid : 3 ) sin a1 cos a1 sin a2 cos a2 ( cid : 3 ) sin a2 cos a2 cos a3 ( cid : 3 ) sin a2 sin a3 cos a3 each matrix r ( i ) rotates the image about the ith axis by an angle ai [ 11 , 12 ]  . 944 radiol med ( 2014 ) 119 : 942950 once chosen the set of reference images , which constitute the primary study and will be kept xed , the algorithm will perform transformations on the other set of images , the secondary study , until the correct alignment is achieved . finally , focal provides that the transformations are carried out through a semi - automatic interaction with the user . 
once the primary and secondary studies are selected , the software proposes a rst registration founding its calculation on the entire content of the images ( intensity of each voxel )  . 
to check the alignment , the software shows the result of the fusion in various modalities ( panels , strips , merging of voxels ) and in each section ( axial , sagittal , coronal )  . 
it also shows the parameters and the transformation matrix as well as the value of mi in the current alignment . to improve the registration quality , it is possible to select a limited region in the three axes [ volume of interest ( voi ) tool ] within which the algorithm calculates the mi and performs its maximisation . 
since mi is a measure of the information common to both images , the selection of a region with well - dened landmarks allows the mi to be increased and the registration to be improved . 
although the selection of voi is user - dependent , even in this case the registration is automatic . finally , the user can customise the registration by directly applying the necessary transformations to the secondary study , assisted by a continuous view of the two studies in fusion on the three sections . description of the phantom the accuracy of the registration algorithm was evaluated by performing a study on a phantom with appropriate inserts of known size and composition . 
it simulates the pelvis region in a stylised way and it is dedicated to the registration of ct and mri images : s.a.r.o. the phantom consists of a cubical tank ( volume of 200 mm3 ) in which the landmarks shown in fig . 
figure 1 shows the axial section of the phantom with the corresponding anatomical landmarks , while table 1 shows the main properties of the inserts . since the two modalities are based on different physical principles , it is necessary to use materials that give signicant signals in both . 
for this reason , inserts are made of pmma , pvc and teon , tissue - equivalent materials in ct acquisition with slightly different densities , but that provide very weak signals in mri acquisition . 
were acquired with a 64 - slice multislice ct600 scanner ( ge medical systems ) using a protocol for radiotherapy treatment of the pelvis . mri images were acquired with a signahdtx scanner ( ge medical systems ) using a protocol suggested by literature regarding the radiotherapy treatment of the prostate [ 14 ]  . 
table 2 shows the main parameters of the ct and mri images . automatic and manual registration the rst part of the study was dedicated to the verication of automatic registration with focal . radiol med ( 2014 ) 119 : 942950 manual registration : the registration is performed manually by means of a visual inspection of the images in fusion . 
the new transformation parameters are marked down to be compared with those of automatic registration . in this way , it is possible to verify if the automatic registration is comparable to the manual registration . repeatability of the registration transformation parameters , a after identifying the best further study was conducted on the repeatability of the transformation performed by the software . for this purpose , a reverse approach was carried out : starting from the ideal alignment , known transformations were performed to the correctly aligned secondary study to verify whether and to what extent the algorithm was able to return to its original position . 
deviations were calculated using the following expression : transformation between where wi , t are the transformation parameters ( translations and rotations along the ith axes ) imposed to the properly aligned secondary study and wi , a are the transformation parameters found by the software . 
a correct transformation corresponds to a situation in which wi , t and wi , a are equal and opposite and , therefore , dwi equal to zero . results the analysis involved testing the as mentioned above , accuracy of the registration algorithm and the repeatability of the transformations the automatic version of ct computed tomography , mri magnetic resonance imaging , fov eld of view dwi wi ; t wi ; a fig . 
phantom during the ct acquisition table 2 main characteristics of the images acquired in the two modalities slice thickness matrix size 5 mm 500 mm 512 9 512 5 mm 400 mm 512 9 512 once the ct series had been selected as the primary study and the mri series as the secondary study , the analysis was divided into three sections . global registration : the software performs an automatic registration basing its calculation on the overall content of images . 
hence , the studies are shown in fusion , and it is possible to assess directly the registration quality . registration with voi tool : through this tool , the region in which the landmarks are visible is selected on the three sections ( axial , coronal , and sagittal ) , as shown in fig . 
the results of the study are shown below . automatic registration the automatic registration performed using the entire contents of the images showed the limits of this procedure . figure 4 shows the fusion of the ct study ( upper panel ) and the mri study ( lower panel ) after this transformation . the overlap of images indeed , the translation returns , belonging to different planes . table 3 shows the transformation parameters and the corresponding matrix . 
the expressions x ( r ? l ) , y ( s ? i ) and z ( a ? p ) indicate , respectively : translation from right ( r ) to left ( l ) , from cranial [ superior ( s ) ] to caudal [ inferior ( i ) ] and from anterior ( a ) to posterior ( p )  . the registration algorithm only ran translations along the three axes . 
as can be seen from this gure , the planes of the two studies coincide , as well as the position of landmarks . the parameters and the transformation matrix obtained through the voi tool are shown in table 4 . as a nal step , translations and rotations were performed manually based on a view of images in fusion . 
the error associated with the manual registration was evaluated by considering the spatial resolution of the images ( 1 mm in the axial plane , 5 mm in the sagittal and coronal planes )  . 
table 5 shows the parameters of the manual transformation and the corresponding matrix . comparing the results obtained with manual registration ( table 5 ) and those of automatic registration obtained by the voi tool ( table 4 ) , it can be noticed that the differences are minimal when compared to the spatial resolution of the images ( calculated from the eld of view size and the sampling matrix )  . 
these differences are included , according to the previously indicated resolution limit , in the error related to the manual registration . to quantitatively evaluate the accuracy of registration , the landmarks were contoured separately in the mri and ct studies . 
6. to further verify the correct operation of the algorithm , a registration of the ct study with itself was performed . the algorithm returned null values for each parameter and the transformation matrix corresponded with the identity matrix . 
for greater rotations , the algorithm was not able to nd the proper registration even with the use of the voi tool . rotations along x : the algorithm failed to nd the correct alignment for small rotations ( 2 ( cid : 3 ) ) even if the voi tool was used . rotations along z : as in rotations along the x axis , the algorithm , running into local maxima , failed to properly register the images with rotations of more than 2 ( cid : 3 )  . complex performing transformations : exclusively translations , the registration algorithm was able to properly align the studies , especially if the voi tool was used . 
table 6 shows some examples of deviations for rotations along y , x , z axis and an arbitrary translation along the three axes . as anticipated , for rotations along the x and z , even with the use of the voi tool , deviations remained signicant . discussion the major advances in radiation therapy have highlighted the need to improve the ability to locate and delineate tumour , healthy tissue and oars accurately . 
the nal image shows that the registration is satisfactory imposed and the for this purpose , the differences between the transfortransformation mation parameters parameters found by the software to properly align the two studies were evaluated . 
although physical spatial resolution along the coronal and sagittal planes is 5 mm , 0.001 mm ( as can be seen in the tables showing the transformation parameters ) , a value that goes far beyond the spatial resolution of the images . 
since , this part of the study was addressed to the ability of the algorithm to nd numerically the same transformation parameters , the same limit was set for all three planes . algorithm computation grid extends to evaluate the automated version of focal , a global registration was rst performed , followed by a registration with voi tool . 
phantom was designed to ensure significant signals in both imaging modalities . first of all , the optimisation procedure of the registration requires , depending on the algorithm , some precautions during image acquisition . 
in addition , since any change in patient position and organ lling represent sources of geometric uncertainties , registration algorithms that use models of rigid transformation must be evaluated carefully to ensure acceptable coherence between the modalities employed . 
respecting these precautions in routine procedures already represents a denite improvement as regards both the quality of the registration and the required timing . during the study , after obtaining images of the phantom according to these precautions , an automatic registration was performed allowing the software to exploit the entire contents of the ct and mri images . 
for this reason , the registration of ct studies with other diagnostic studies is emerging strongly in many centres and it is becoming an integral part of treatment planning . to minimise the possibility of human or software errors , clinical image acquisition and registration processes should be managed where possible in an integrated way to ensure their cogency , sequentiality and reproducibility [ 1 ]  . 
the registration algorithm is , in its automatic version , reliable for rotations along the y - axis up to 40 ( cid : 3 ) only if the voi tool is used . 
the algorithm is indeed able to assure the alignment of the studies if the voi tool is used . on the other hand , automatic registration did not prove satisfactory with regard to rotations along the x and z axis . 
this leads to the criticism of the correct patient position in the two studies as even small differences could affect is therefore desirable to use appropriate outcome . systems for patient immobilization with high precision positioning . 
this objective is certainly favoured by performing the studies on the same day and at a short temporal distance from one another . conclusion this the main objective of this work was to verify the accuracy and the repeatability of the registration of ct and mr images using the automatic version of the focal software . for this purpose , images of the s.a.r.o. 
the results show that , using the manual registration as a reference because it allows one to visually assess the quality of alignment , automatic registration is comparable when the voi tool is in clinical used . applications , the algorithm is reliable and fast if the voi includes that are clearly visible on both modalities . 
in females , brain , lumbar spine , and abdominal ct scans , pre - / postcontrast neck ct scans , and post - contrast liver dynamic ct scans were performed . 
breast shielding during neck and liver dynamic ct was the most effective compared with breast or thyroid shielding during other ct scans . conclusions we recommend breast shielding during neck and liver dynamic ct in young female patients to avoid unnecessary radiation exposure . keywords radiation protection ( cid : 2 ) multidetector computed tomography ( cid : 2 ) breast ( cid : 2 ) thyroid introduction increased radiation exposure may be one of the causes of the recent rapid increase in breast cancer in korea [ 1 ] in addition to westernised diet changes , a decreasing birth rate , and an increasing maternal age [ 2 ]  . 
a recent study from the national cancer institute in the united states has projected 29 , 000 excess cancers from the 72 million ct scans performed on americans in 2007 alone [ 6 ]  . 
scans of the abdomen , pelvis , chest , and head were deemed most likely to cause cancer , and 952 radiol med ( 2014 ) 119 : 951957 in female patients , noncontrast - enhanced ct of the brain , lumbar spine , and abdomenpelvis , preand postcontrast neck ct , and preand post - contrast liver dynamic ct were performed . in male patients , noncontrastenhanced brain ct was carried out . 
with this technique , the supercial breast or thyroid skin doses , not the absorbed doses in the deep tissues , were women aged 3554 years were particularly more likely to develop cancer as a result of ct scans than any other age group because of the high frequency of ct use [ 6 ]  . 
twothirds of the excess cancers will occur in women primarily because of the higher frequency of use ( 60 % of scans ) as well as the higher breast and lung cancer risks associated with scans that expose the chest [ 6 ]  . currently , ct scans of the abdomen , lumbar spine , and brain have been performed without shielding of adjacent organs such as the breasts or thyroid glands . 
in general , two - view screening mammography ( \3 mgy standard , equivalent dose for the breast ) , which can cause breast cancer by itself , has not been recommended in women aged less than 35 years because of the radiosensitivity of breast tissue [ 7 ]  . 
during abdominal ct , however , a radiation dose 5 ( single scan ) to 20 times ( post - contrast dynamic scan ) greater than screening mammography is introduced to the abdomen , and a signicant radiation dose is simultaneously exposed to the breast adjacent to the abdomen due to scatter radiation . 
signicant radiation doses can also be introduced to the thyroid and breast during brain ( less than 2 mgy equivalent dose for thyroid ) and neck ct [ 7 ]  . breast tissue is also exposed during lumbar ct . 
therefore , the tissues outside the primary beam should be protected against scatter radiation if the image quality will not be sacriced [ 811 ]  . in the present study , we investigated the efcacy of lead shielding for radiation protection of the breast and thyroid by measurement of the entrance skin dose of radiation exposure during ct of the brain , neck , abdomen , and lumbar spine in young patients . materials and methods institutional review board approval for this prospective study was obtained from our institution , and all patients volunteered to participate and signed the informed consent form . patient selection this study included 150 patients ( 25 patients consecutively in each group ; male : female 25 : 125 , mean age 32.8 years , age range 1545 years ) referred for a ct study of the brain , neck , abdomen , or lumbar spine for objective medical reasons . 
the sensors were also attached to the skin of both thyroids , 2 cm apart from the midline of the lower neck and 45 cm above the suprasternal notch . therefore , two sensors were at the same distance from lumbar spine in each the head , neck , abdomen , or measurement . ct equipment singleor multi - phase , preor post - contrast ct scans were performed using a 16 - row multidetector ct scanner ( mdct ; somatom sensation 64 ; siemens medical solutions , erlangen , germany ) for variable clinical information . 
preand post - contrast ct images were obtained in neck and liver dynamic studies , using intravenous administration of 120150 ml of nonionic iodinated contrast media ( ultravist 300 ; bayer schering pharma ag , berlin , germany ) administered by an automatic injector at 34 ml / s . 
ct parameters used in the variable ct studies are listed in table 1 . body constitution the body mass index ( bmi = body weight / height2 ) was calculated in each patient . 
this unit started dose accumulation , individually for connected sensors , when the dose rate exceeded a trigger level of about 10 lgy / s ( 60 mr / min ) and stopped dose accumulation when the dose rate was below a level of approximately 5 lgy / s ( 30 mr / min )  . 
the sensor is calibrated to entrance skin dose at 90 kvp in gy and the energy dependence is \10 % for the energy range 60110 kvp ( \15 % for the energy range 40140 kvp ) at a tube ltration of 6 mm al . 
regarding thyroid shielding on brain ct , the entrance skin doses in the reduced by 17.9 % ( range shielded thyroids were 1.555.7 % ) in female patients and 20.6 % ( range 1.848.5 % ) in male patients compared with those of unshielded thyroids ( table 2 )  . 
there was no correlation between bmi and the reduced radiation dose in the shielded breast or thyroid . discussion the radiosensitive structures that lie within the primary beam cannot easily be protected , and the organs outside the ct scanning planes are exposed only to scatter radiation . during brain ct examination , internal scatter radiation propagates caudally through the neck , reaching the breasts as well [ 8 ]  . 
a signicant amount of scatter radiation , generated in the head and in the gantry , reaches supercial organs , particularly the thyroid and breasts , from the outside and can be reduced effectively by lead shielding . 
in our study , however , there was no correlation between bmi and the reduced radiation dose in the shielded breasts or thyroid , as reported previously by brnic et al . 
additionally , the shielded and unshielded breasts or thyroids are close , which can cause the possible perturbation effect of the shield in the unshielded portion due to scattering and characteristic x - rays from the shield to the unshielded portion . 
this effect can increase the difference between shielded and unshielded portions with an overestimation of the usefulness of the shield . the radiation dose measured on the surface of the breast or thyroid is obviously higher than the actual glandular dose because of scattered and low - energy x - ray radiation [ 13 , 1921 ]  . 
assuming a weighting factor of 0.05 for the breast and a breast dose of 0.01 gy probability ( 0.01 sv ) , 5.6 9 10 - 2 9 5 9 10 - 2 9 10 - 2 = 2.8 9 10 - 5 . in our study , the mean skin dose on the unshielded breast during preand post - contrast liver dynamic ct was about 0.002 gy ( 2 , 387 lgy )  . 
we believe that causes may be as follows : ( a ) the neck is closer to the breast than the brain , abdomen or lumbar spine , so the breast receives more radiation exposure during neck ct . ( b ) liver dynamic ct consists of four scans : pre - contrast and post - contrast arterial , portal , and equilibrium phase radiation imaging . 
therefore , exposure in liver dynamic ct is higher than other singleor double - phase ct scanning , and breast or thyroid shielding during this ct scan results in more effective elimination of radiation exposure than the unshielded breast or thyroid . the absolute amount of compared to previously published studies , this study differs in several respects . 
 ( a ) this study compared the radiation dose reduction in the multi - organ ct scans ( brain , neck , abdomen , and lumbar spines ) by lead shielding of breasts or thyroids , and investigated which one radiol med ( 2014 ) 119 : 951957 is more effective shielding in the ct scans of different organs . 
 ( b ) we used the unfors psd ( cid : 3 ) unit to measure the entrance skin dose , whereas other studies used a thermoluminescent dosimeter which was relatively more complex to use . 
 ( c ) this study did not use the in - plane shielding such as breast shielding during chest ct or eye lens shielding during brain ct which could evaluate the effect on image quality of using in - plane shielding . our study has several limitations : ( 1 ) neither thermoluminescent dosimeters nor a phantom study to measure the actual glandular dose were included because we only compared the reduction of entrance skin doses in shielded and unshielded organs . 
in the radiation elds of mdct , the direct or scattered radiation from the back or sides of the thorax or neck could not be protected by our shields . in conclusion , breast shielding during preand postcontrast neck ct and liver dynamic ct was most effective in reducing the entrance skin dose compared with breast or thyroid shielding during other ct scanning . 
wholebody dw - mr imaging ndings were compared with results obtained at skeletal scintigraphy and ct bone survey . results the mean examination time for whole - body dwmr imaging was 25.5 mall bone metastases regardless of the size were identied with whole - body dw - mr imaging ; mr imaging depicted more bone metastases than ct . 
skeletal scintigraphy depicted osseous metastases in 13 patients ( with greater sensitivity to the lower limb ) , whereas whole - body dw - mr imaging revealed osseous metastases in 13 patients ( with greater sensitivity to the spine )  . 
schena department of biomedical engineering , campus bio - medico university of rome , rome , italy seen with mr imaging were conrmed at follow - up examinations and some had a change in therapy . 
on a per - patient basis , whole - body dwmr imaging revealed sensitivity and specicity values of 100 % . conclusion whole - body dw - mr imaging was more sensitive in the detection of osseous metastases than were skeletal scintigraphy and ct bone survey . keywords mr ( cid : 2 ) whole - body mr ( cid : 2 ) metastasis ( cid : 2 ) bone lesions ( cid : 2 ) ct ( cid : 2 ) bone scintigraphy introduction diffusion - weighted imaging ( dwi ) is a quantitative magnetic resonance technique that measures the random ( brownian ) motion of water molecules in biological tissues . 
in human tissues , water motion is locally hindered by the presence of cell membranes , vascular structures and brotic tissues , so the degree of restriction to water diffusion is inversely correlated to tissue cellularity and the integrity of the cell membranes . 
widely used in the study of intracranial diseases and cerebrovascular accidents [ 1 ] , dwi is of increasing interest for the detection of primary or metastatic cancers [ 2 , 3 ] , as tumoural tissue consists of densely cellular and highly vascularised structures . radiol med ( 2014 ) 119 : 758766 diagnostic work - up in the evaluation of oncological patients includes some staging procedures that play key therapeutic and prognostic roles . 
since metastases may affect any organ , imaging techniques most commonly involve computed tomography ( ct ) , magnetic resonance ( mr ) , ultrasonography ( us ) and bone scintigraphy ( bs )  . bone scintigraphy is one of the most frequently ordered investigations for suspected bone metastases , particularly during oncological follow - up , and it remains a reference modality for oncologists [ 4 ] , although there are wellknown limitations affecting its specicity and sensitivity [ 5 ]  . 
despite the increasing use of dwi as an adjunct in evaluating tumour patients due to its relatively easy and time - effective application , systematic reports evaluating its technical feasibility , especially in terms of image quality and robustness of apparent diffusion coefcient ( adc ) measurements are rare and only focus on limited parts of the body , with few experiences addressing whole - body dwi . 
moreover , experience with dwi within the concept of whole - body mri including conventional t1w and shorttau inversion recovery ( stir ) sequences in the diagnostic practice is still limited [ 6 ]  . including dwi sequences , the aim of our study was to assess the diagnostic value of whole - body mri , in the detection of skeletal metastases in comparison with wholebody ct and bs to determine the utility of whole - body dwi as a component of the whole - body mr examination for the diagnosis and follow - up in patients affected by bone metastases . 
moreover , we wanted to verify the application and diagnostic value of each technique depending on the different anatomical distributions of skeletal metastases . materials and methods patients from january 2011 to march 2012 , a total of 17 patients ( 11 women and six men ; mean , age 57 years ; age range 4076 years ) with malignant tumours were included in this retrospective study to detect bone metastasis . 
they were examined using whole - body dwmr imaging as well as whole - body ct and bs , with an average interval of 14 days ( range 030 days )  . 
the inclusion criteria were as follows : adults with histologically table 1 patient characteristics patient age ( years ) gender primary tumour breast breast breast breast breast prostate prostate pancreas lung thyroid colon breast lung lymph node proven primary tumour , curative treatment at least 1 year before the examination and no history of another malignancy . the patients characteristics are summarised in table 1 . whole - body dw - mr imaging due to convention derived from various reports in the literature [ 68 ] , the examination was designed as a wholebody examination , although only regions from the head to the middle of the tibia were considered . all mri examinations were performed using a 1.5 - t siemens magnetom avanto system ( siemens healthcare , erlangen , germany ) with the patient in supine and feetrst position with arms in adduction . 
a moving tabletop and tabletop extender were used , generating a longitudinal eld of view ( fov ) of 2 , 000 mm and a transverse fov of 530 mthe larger fov enables head - to - toe scanning of all adult patients without repositioning [ 9 ]  . two sequences were used for the whole - body mri : t1 gradient echo sequences ; single - shot stir spin - echo ( se ) echo - planar imaging sequences for dwi , conducted with two b values of 50 and 500 s / mm2 . 
diffusion weighting was archived by applying pairs of motion - probing gradients before and after the 180 ( cid : 3 ) radiofrequency pulse of the spin - echo t2 - weighted sequence in three orthogonal directions ( x , y and z )  . 
conventional t1 turbo spin - echo ( tse ) and t2 stir were acquired both in the axial plane from the base of the skull to the middle of the tibia and for the whole spine in the sagittal plane , divided into ve stacks . 
the average interpretation time for the whole - body mr images was approximately 9 min . computed tomography all ct exams were performed using a 64 - slice ct scanner ( siemens , somatom sensation )  . 
an intravenous iodine - based contrast medium was administrated and bone lesions were studied during the portal venous phase . the mean acquisition time , including needle insertion for the administration of contrast medium , was 7 min . metastases were classied as osteolitic , mixed and osteoblastic , with regard to their density measured in hounseld units tumour ( hu ) , characteristics . depending primary bone scintigraphy whole - body planar imaging in the anterior and posterior positions was performed 3 h after intravenous injection of 740 mbq of tc99m - hmdp ( schering pharma , brussels , belgium )  . images were acquired using a dual - headed whole - body scanner with a low - energy , high - spatial - resolution collimator . 
the preset scan speed was 12 cm / min and the matrix size 256 9 1 , 024 pixels . image analysis on whole - body mr , a lesion was considered positive for metastatic bone disease when there was a focal , or a diffuse , hypointense bone marrow signal compared with adjacent muscle on t1 - weighted images and intermediate or high signal intensity relative to the surrounding marrow on stir imaging , which could not be explained by a degenerative , inammatory or traumatic cause [ 10 ]  . 
furthermore , criteria for malignancy were periosteal tumour inltration or , for evaluation of the spine , signal changes extending into the pedicles and bulging of the anterior or posterior margin of the vertebral body [ 11 ]  . 
lesions were considered benign if there was a high signal intensity on t1 - weighted images or if they were located close to degenerative changes of the vertebral endplates or near joint surfaces . on dwi , a lesion was considered malignant when there was a focal or diffuse signal intensity increase in conjunction with the b value increment . 
bs was not considered for this classication due to the difculty in obtaining an accurate value of lesion size . on ct , images obtained with the bone window permitted measurement of the hu in healthy and pathological bone tissue . 
in the spine , on bs , a focal lesion was regarded to be malignant when the distribution and pattern of focal tracer accumulation could not be explained by degenerative or posttraumatic changes . a classication system was created for each technique , based on the anatomical distribution of bone metastases . considering the low sensitivity of dw - mr imaging in the evaluation of skeletal metastases in regions such as the skull and ribs and , on the other hand , the high sensitivity of bs in detecting metastases in regions such as skull and thorax bones [ 14 , 15 ] , the division into locations considers three regions for each examination : axial skeleton ( as : cervico - thoracic and lumbo - sacral spine , clavicle , pelvis ) lower limbs ( ll : lower extremities up to the tibial diaphysis ) and chest ( ch : sternum , ribs , scapula , including the proximal humerus and the mandible )  . 
the division by anatomical distribution is intended to ensure maximum uniformity of the data and the best comparison among the radiological techniques considered . the analysis was carried out on each of the 17 patients , for a total of 48 examined areas . radiol med ( 2014 ) 119 : 758766 fig . 
1 a 46 - year - old female patient with breast cancer : whole - body magnetic resonance imaging in the coronal plane shows a vertebral bone lesion in t1 - weighted ( a ) and diffusion - weighted ( b ) sequences ( arrows )  . 
fourteen of 17 patients completed all three of the examinations ; the other three patients , after a diagnosis of bone metastases on ct , showed negative results on mri so these patients were not subjected to bs . 
we compared the results of wholebody dw - mri with those of ct and bs . the total number of lesions identied with the three different procedures was n = 74 for ct , n = 162 for whole - body dw - mri and n = 133 for bs . 
in these two cases , mri detected multiple metastases in the axial region and lower limbs ; the other one ( case #4 ) had negative results on both examinations . radiol med ( 2014 ) 119 : 758766 fig . 
3 a 69 - year - old male patient with prostate cancer : whole - body magnetic resonance imaging in the coronal plane demonstrates a left acetabular lesion in t1 - weighted ( a ) , diffusion - weighted ( b ) and adc maps ( b ) sequences ( white arrows ) , while bone scintigraphy ( d ) was considered negative for bone metastases in the same district for 12 / 14 patients , whole - body mri and bs concordantly demonstrated metastatic lesions , but were disconcordant for lesion number and involvement site in only 1 / 12 ( 8.3 % ) patients ( case #7 )  . 
one patient , conversely , had positive bs and negative whole - body mri ( case #4 ) results ; in this patient , bs detected a total of three metastases , two of them in the axial skeleton ( pelvis ) and the other in the chest ( rib )  . hence , mr identied 22 % more metastatic lesions when compared to bs and 119 % more than ct . 
bone scintigraphy identied 80 % more metastatic lesions when compared to ct . the lesions observed using the different diagnostic procedures are shown in table 2 and are categorised by anatomical site . 
whole - body dw - mri is characterised by an advanced sensitivity in identifying lesions in the lower limbs and axial skeleton , while presenting a limited receptivity in the chest . 
in both whole - body dw - mri and ct , a subdivision based on lesion size was made , underlining how whole - body dwmri had a higher sensitivity in detecting bone metastases independently from size in comparison with ct , and it also showed that in both procedures , the majority of lesions were included in the dimension group beneath 10 mm . patient - by - patient analysis revealed multiple lesions on bs in 11 / 13 ( 84 % ) of the patients with positive mri ndings and multiple lesions on mri in 12 / 13 ( 92 % ) of the patients with positive bs . 
none of the enrolled patients was classied as an equivocal case . particular , regarding the axial district , whole - body dwmri showed a higher number of lesions , followed by bs and then by ct . 
for the chest region , there was a marked higher sensitivity of bs in detecting bone metastases ; otherwise , whole - body dw - mri had a lower sensitivity in detecting bone lesions in the chest . discussion one of the most common sites of distant metastases is the cellular bone marrow ( 5070 % ) , especially in patients with breast and prostate cancer . 
traditionally , bs has been the standard graph 1 anatomical distribution of bone metastases . whole - body dw - mri results are in light grey , bs results are in dark grey and ct results are in black 764 graph 2 detection of bone metastasis considering lesions size . 
whole - body dw - mri versus ct radiol med ( 2014 ) 119 : 758766 imaging investigation used for the detection or exclusion of skeletal metastases , and it is widely used to assess metastatic spread in patients with breast , prostate or lung cancer [ 17 , 18 ] , as bs is more sensitive when sufcient osteoblastic reaction has occurred . 
however , supplemental imaging studies are needed to dene unclear ndings , as bs has limited specicity [ 19 ]  . whole - body mri within a single session has become feasible for the evaluation of the presence of metastases and / or for the evaluation of primary cancers , due to recent advances [ 15 , 20 , 21 ] such as short data - acquisition times , no ionising radiation and no injection of isotopes or contrast mediuin several studies , whole - body mri has shown better results than skeletal scintigraphy [ 12 , 16 , 22 24 ] in the detection of bone metastases . 
 [ 7 ] , high spatial resolution whole - body dwi has become available . the diagnostic added value of whole - body dwi sequences has been established [ 12 ]  . 
in comparison with conventional whole - body mri , its sensitivity , specicity and positive predictive value ( ppv ) in detecting bone metastases are superior to those of both conventional mri and bs . particularly , whole - body dwi excels at bone marrow assessment for diagnosis and for therapy evaluation , where it can potentially address unmet clinical and pharmaceutical needs for reliable measurement of tumour response [ 25 ]  . 
with this modality , no ionising radiation is administered and no injection of any contrast medium is necessary , allowing whole - body dwi to be used in routine clinical practice . moreover , multislice ct has been proposed as an alternative to bs for whole - body screening of the skeletal system due to an equivalence found by groves et al . 
however , a recent study comparing multidetector ct with mri in the detection of osseous metastases of the spine found a greater sensitivity of mri , with equivalent specicities [ 27 ]  . all of these data are in agreement with our study that demonstrates that whole - body dw - mri can be used for assessment of bone metastases in patients with cancer . comparative studies of imaging methods have the major bias that none of them can guarantee 100 % diagnostic accuracy as each may be affected by false - positive and false - negative results . 
validation of a new imaging method , such as whole - body dw - mri , requires a comparison with the most consolidated standard in the clinical management of patients [ 28 ]  . our results also demonstrate that whole - body mri has a higher diagnostic accuracy than ct and a comparable level of agreement to bs in detecting bone metastases , independently from the primary tumour site . 
more importantly , there were two cases in our sample in which bs was completely negative for axial bone metastases , with positive results shown by whole - body dw - mri . 
whole - body dw - mri failed to depict a considerable number of lesions in the ribs but depicted more lesions in the spine , pelvis and lower limbs . thus , in an uncertain diagnosis concerning an axial skeletal metastasis , the availability of dw sequences can help to conrm / deny the suspect lesion . 
it has been suggested that this limitation is due to artefacts related to pulsation and breathing movements in the thorax , which make examination of the ribs , sternum and scapula more difcult . 
motion - related signal intensity decreases may explain why metastatic lesions in the bone marrow of the anterior chest wall are sometimes relatively less conspicuous than lesions found in the spine and paraspinal regions [ 25 ]  . 
in terms of the dimensions of bone metastases , greater the ability of whole - body dw - mri to nd it in comparison to ct . the larger the size of the lesion , in our series , a majority of cases were concerned primary breast and prostate cancers , in which there were too many lesions to count , in some cases hundreds [ 26 ]  . many of these lesions are often very small and not identied on scintigraphy , but can be seen on mri or ct . 
the detection of other extra - small lesions probably makes a difference in patient management , even if it is minimucomparing the results obtained using whole - body mri and ct and classifying them based on lesion dimension , it might be inferred that more lesions are observable using mr regardless of lesion dimension . further , whole - body dw - mri has a more extensive anatomical coverage , which results in an ability to identify also extraskeletal lesions with therapeutic and prognostic signicance . this study has certain limitations . 
also due to ethical reasons , ct examinations , intended as total - body scans , were done not covering the portion between the femoral diaphysis and tibial proximal epiphysis . 
thus , the very high difference in detecting metastases ( in particular in the lower limbs ) between whole - body dw - mri and ct could be a result of this limitation . 
another limitation is related to the heterogeneity of the patients in which metastases are primary tumours , usually depicted when sufcient osteoblastic reaction has occurred , may demonstrate a lower sensitivity in tumours eliciting a particularly poor osteoblastic response [ 30 ]  . in that bs , dwi seems to be a sensitive but rather unspecic modality for the detection of bone metastatic disease . high - quality prospective studies regarding whole - body mri in detecting bone metastases still need to be conducted [ 21 ]  . in conclusion , to the best of the knowledge , no previous studies have compared concurrently ct , whole - body dwmri and bs . 
radiological density was assessed with the birads classication ; a quantra density cut - off value was sought on the 2d images only to discriminate between birads categories 12 and birads 34 . 
use of the automated system requires the adoption of a cut - off value ( set at 21 % ) to effectively discriminate birads 12 and 34 , and could be useful in clinical practice . keywords breast density ( cid : 2 ) digital mammography ( cid : 2 ) computer assessment e . 
bergamasco dipartimento di scienze chirurgiche , azienda ospedaliera citta` della salute e della scienza di torino presidio molinette , universita` di torino , corso bramante 88 , 10126 turin , italy introduction high breast density is an important risk factor for cancer development and reduces the sensitivity of mammographic evaluation [ 14 ]  . over the years numerous methods , both qualitative and quantitative , have been developed for the evaluation of mammographic density . 
in recent years , algorithms for the computerised evaluation of breast density have been proposed . these methods have the advantage of a very high reproducibility compared to traditional visual assessment , and a study of correlation between visual and computerised assessments has recently been published [ 1 ]  . the purpose of our study was to compare the denition of mammographic density between visual assessment with the birads classication and the automatic quantra r2 breast density assessment software ( 1.3 hologic corp , bedford ma , usa )  . 
in particular , the objectives of the study were to evaluate the concordance of the visual assessment of breast density based on conventional ( 2d ) digital mammography and tomosynthesis ( 3d ) ; to determine the correlation between the birads classication of mammographic density and the automatic quantra assessment and choose the best quantra cut - off value for discriminating between birads density categories 12 and 34 ; to estimate correlations between breast density and age , use of hormone therapy and tumour histotypes ; to assess whether the quantra system can be helpful in clinical practice in the case of malignant disease . materials and methods study population the study sample includes 200 cases of women ( mean age 56.04 years ; range 3593 ) who underwent mammography between february 2010 and december 2011 at the diagnostic breast clinic of the radiology university of torino , department of diagnostic imaging and radiotherapy , azienda ospedaliero - universitaria citta` della salute e della scienza di torino . 
of the 200 cases , 100 women ( mean age 60.40 years ; range 3793 ) , who were symptomatic and referred to our clinic for diagnostic mammography or selfreferred for screening mammography in the absence of clinical symptoms , were selected based on the detection of histologically conrmed malignant breast disease ; patients undergoing neoadjuvant chemotherapy , those with breast implants or with a previous mastectomy were excluded . 
the other 100 cases ( mean age 51.79 years ; range 3578 ) were selected from among women who underwent mammography during the same time period and for the same reasons ( symptomatic patients referred for diagnostic mammography or asymptomatic patients self - referred for screening radiological signs of mammograms ) , but negative for malignant breast disease and negative follow - up maintained for at least 1 year ; patients with a previous mastectomy were also excluded in this group . each patients history was collected taking special care to investigate family history of breast disease , previous breast surgery and past and present hormone treatment . image acquisition after giving their informed consent , patients underwent two - dimensional ( 2d ) digital mammography and 3d tomosynthesis with a single compression ( combo mode ) using the same imaging session . 
the mammograms were performed with a lorad selenia dimensions digital mammography system ( hologic corp , bedford ma , usa ) set for tomosynthesis in the two standard craniocaudal ( cc ) and mediolateral oblique ( mlo ) projections . 
for tomosynthesis , the scan was performed along an angle of 15 ( cid : 3 ) ( 7.5 ( cid : 3 ) ) and 15 exposures were acquired ( one exposure for each degree )  . image analysis a radiologist with 23 years of experience in breast imaging and 4 years in tomosynthesis reviewed in a single session the images acquired in 2d and 3d modes and dened visual density according to the american college of radiology ( acr ) birads classication [ 5 ]  . 
only the 2d images were subsequently processed by quantra r2 automatic software ( quantra ( cid : 4 ) 1.3 , hologic corp , bedford ma , usa ) [ 8 ]  . 
this evaluation algorithm is based on a physical model that correlates the attenuation of the x - ray due to the breast tissue and the digital mammography images provided to the radiologist . 
the assessments are based on physical parameters specic to the breast tissue and imaging system , as well as on information relating to individual x - ray exposures including attenuation coefcients for breast tissue [ 9 ] , radiographic spectra of the target material [ 10 ] , kvp , mas and thickness of the tissue reproduced in the images . 
quantra estimates the amount of broglandular and fatty tissue that an x - ray must have crossed to deposit a specic amount of energy on the detector , and it provides a result ( height ) in centimetres of broglandular tissue penetrated corresponding to each pixel of the image . after completing the analysis of the pixels ( excluding the pectoral muscle ) , the system combines the values in the volume of the broglandular tissue , expressed in cubic centimetres . 
the system then calculates the ratio between the volume of the broglandular tissue and the total estimated breast volume in order to determine the percentage of broglandular tissue volume in the breast , for both the left and right side ( combined cc and mlo projections ) radiol med ( 2014 ) 119 : 741749 fig . 
this technique was rst applied to analogue images and then , thanks to semiautomatic procedures , to digital mammograms [ 16 ]  . more recently , a system developed by shepherd et al . 
the image is then analysed to determine breast thickness , percentage of broglandular tissue in each pixel and dense tissue in the mammogram . among fully automated volumetric systems , the standard mammographic form ( smf ) is a technique that divides breast tissue into interesting ( healthy normal tissue and neoplastic tissue ) and uninteresting ( adipose tissue ) and is based on different x - ray attenuation coefcients : the volume resulting from the volume of interesting tissue is regarded as the volume of dense tissue [ 18 ]  . 
to provide a practical criterion and relate the quantra measurements to the birads visual scale , the percentage of quantra breast density which best discriminated dense ( birads 34 ) from nondense breast ( birads 12 ) was sought . 
the rst step was to calculate the two density distributions for the two classes to be discriminated : any technique able to identify the two distributions should only allow for a small overlap . 
therefore , the best quantra density value ( cut - off value ) discriminating between the two birads categories was chosen , evaluating sensitivity , specicity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy ( da )  . 
the correlation between breast density and age , both in positive and negative patients , and the correlation between breast density and history of hormone therapy were quantied by pearsons linear correlation coefcient . 
a paired students test was used to analyse , in positive patients and in particular in the subgroup of patients who had or were taking hormone therapy , the difference in quantra density between the pathological ( case ) and healthy side ( control ) , and also subdividing the patients into two age groups ( b50 and [ 50 years )  . 
in all other cases anova analysis of variance was used to 744 table 1 breast density assessed by the visual american college of radiology birads classication : comparison between 2d digital mammography and 3d digital breast tomosynthesis density ( birads ) digital breast tomosynthesis 3d 2d digital mammography d1 fat ( \25 % glandular ) , d2 scattered broglandular ( 2550 % ) , d3 heterogeneously dense ( 5175 % ) , d4 extremely dense ( [ 75 % glandular ) compare continuous variables . 
the average quantra density was 24.89 % ( 95 % ci , 22.8226.96 ) for patients aged \50 years and 17.28 % ( 95 % ci , 16.0118.55 ) for those aged c50 years . 
the anova test on the quantra density values corresponding considering the whole group of patients , 95 out of 200 women reported having taken hormone therapy in a time interval between a few months and 30 years ( oestrogen progestin therapy in 77 cases , hormone replacement therapy in 8 and tamoxifen in 10 )  . 
b linear correlation between quantra density and birads classication . c distribution of the density value measured by the quantra software , considering cases classied as birads 12 and birads 34 . d roc curve in which the value of the area under the curve ( c [ 0.9 ) corresponds to a very good ability of the quantra software to discriminate between birads 12 and birads 34 density analysis of both breasts in relation to breast disease , hormone therapy and age because hormone therapy affects density , we analysed only the positive subgroup of patients with unilateral disease ( n = 94 ) to identify correlations between the presence of malignant disease and density , and evaluated differences in density between healthy breast and diseased breast . 
comparison with paired students t test ( considering the diseased side as a case and the healthy one as a control ) clearly indicated ( p = 0.001 ) that the density of the affected side was statistically signicantly greater than that of the healthy side . 
denitive histological examination revealed the presence of 66 inltrating ductal carcinomas ( idc ) , four idc associated with lobular component ( idc ? ilc ) , one idc with ductal carcinoma in situ component ( dcis ? idc ) , 14 dcis , seven inltrating lobular carcinomas ( ilc ) , one lobular carcinoma in situ ( lcis ) , one inltrating tubular carcinoma ( itc ) , one idc associated with inltrating tubular component ( idc ? itc ) , one papillary carcinoma , and one mucinous carcinoma . 
applying the anova analysis of variance we observed that dcis and idc have equivalent density ( p = 0.44 ) , while a borderline difference ( p = 0.08 ) was noted between them and ilc due to the small number of ilc . all we know today about the meaning and impact of mammographic density on the risk of disease and failure to discussion fig . 
in the left breast mammogram it difcult to assess a clinically palpable lump reported by the patient in the lower quadrants ; at ultrasound examination we found an inhomogeneous hypoechoic area . 
denitive histological examination was invasive ductal carcinoma associated with ductal carcinoma in situ measuring 2 cm . the density values assessed by quantra software were 34 % for the right breast , and 50 % for the left breast ( difference between the right and the left breast was 16 % ) diagnose is based primarily on visual classication . 
while waiting for controlled studies on the value of the automatic density as a risk factor to be repeated , the adoption of a simple system to convert the quantra value into a visual value is currently the only solution if we are to continue using automatic evaluation in current practice . 
the similarity of the results between the two studies also applies to the range of quantra values for the individual birads categories , except for category d4 , in which we observe a discrepancy in the value of the lower range . 
if one applies the same intent to ciatto et als study , the cut - off value that correctly identies all d34 visual cases is \15 % , whereas in our study this corresponds to a cut - off value \9 % . 
 [ 11 ] who used quantra as evaluation software for mammographic density , the pearson correlation coefcient between the age and density parameters was - 0.20 ( p \ 0.0001 ) ; specically , menopausal status showed a signicant correlation with breast density with perior post - menopausal women having a lower density compared to premenopausal women . 
 [ 23 ] in a large meta - analysis including 42 studies used 21 % as a cut - off density value stating that the risk of developing breast cancer in women with dense breasts ( [ 21 % ) was up to 4.6 times higher compared to those with lower density . the literature reports many experiences related to a reduction in the sensitivity of mammography in the detection of breast cancer in dense breasts . 
conducted on women participating in mammography screening from 1988 to 1993 in whom primary invasive breast cancer was diagnosed within 24 months of a screening examination and therefore before the next inspection . 
the odds ratio ( or ) for interval cancers among women with very dense breasts was 6.14 ( 95 % ci , 1.8519.4 ) compared with women with extremely fatty breasts [ 24 ]  . 
specically , a summary or of 3.6 ( 95 % ci , 2.74.8 ) was calculated for the quantitative method , compared to an or of 1.8 ( 95 % ci , 1.52.1 ) for the wolfe method . 
many studies using quantitative methods for the evaluation of breast density reported a higher or , in terms of developing breast cancer , in women with dense breasts compared to studies in which subjective evaluation methods were used . 
 [ 25 , 26 ] conrmed the importance of using precise methods for evaluating mammographic density since they found a 2 % increase in the relative risk of breast cancer for each percentage point increase in breast density . 
in our study , albeit with low test power ( p = 7 % ) , we found that the group of patients aged b50 years and density greater than 21 % had a greater tendency to disease ( probability of 26.9 % ) compared to the group with density \21 % . moreover , comparison between denitive histology and breast density showed that idc and dcis have equivalent density ( p = 0.44 ) , while there was a borderline difference ( p = 0.08 ) between these and ilc due to the small number of ilc which reduced the statistical power ( p = 23 % ) ( probability of false negative , 77 % )  . 
conversely in two other recent studies , the data failed to demonstrate a statistically signicant correlation between density and tumour histology . in particular , in the study by eriksson et al . , which analysed 1 , 747 patients diagnosed with tumour between 1993 and 1995 , the breast density estimated by computerised algorithm was found to be associated with tumour size ( regression coefcient 0.031 , p = 0.017 ) , but not with histopathological classication or receptor status . 
for each of the conditions identied , we dened the overall incidence , the incidence based on the site , gender , average age and age range . results computed tomography examination was positive in 125 out of 143 patients ( 87.4 % ) , 74 men and 51 women , with an average age of 51.1 years , aged between 10 and 90 years . 
we found 79 inammatory / infectious conditions ( 63.2 % of positive cases , 55.2 % of total cases ) , 46 men and 33 women , with an average age of 47 years . 
based on the clinical diagnosis and pathology , they can be divided into subgroups : inammatory / infectious diseases [ 3 , 4 ] , trauma , foreign body ingestion [ 5 ] , tumours [ 6 ] , functional disorders , sensorineural disorders , respiratory diseases , vascular disorders , and spinal and vertebral disorders . with the increasing use of computed tomography ( ct ) to evaluate patients in the emergency department , in our daily activity the number of cases of non - traumatic emergencies of the neck is growing , as demonstrated in a study published in radiology in 2011 [ 7 ]  . 
the aim of this study was to collect information on the incidence and distribution of acute , non - traumatic conditions of the neck seen at the emergency radiology department of our hospital and to review the literature about this topic . radiol med ( 2014 ) 119 : 784789 materials and methods we used our institutions data archives to conduct a descriptive observational study , collecting retrospectively consecutive patients who underwent neck ct in the from 1 december 2008 to 31 emergency department december 2012 . 
during this time , in the emergency radiology department of our hospital , 201 ct examinations of the neck were performed out of a total of 38 , 768 ct examinations ( 0.5 % ) ; considering that we excluded 19 patients whose clinical history was not known and 39 patients ( 19.4 % ) who underwent ct as a result of trauma , we found 143 out of 38 , 768 patients ( 0.37 % of the total emergency ct requests ) , with a non - traumatic condition . among the examined 143 patients , 86 out of 143 were men ( 60.1 % ) and 57 ( 39.9 % ) were women , with an average age of 51.7 years and age range between 10 and 90 years . all the patients underwent multidetector ct scans using a ge lightspeed qxi scanner ( milwaukee , usa ) with section thickness of 1.25 mm and a siemens somatom denition flash scanner ( erlangen , germany ) with a section thickness of 0.6 mm , before and after the intravenous administration of contrast media . patients underwent ct to answer clinical questions that respected the referral guidelines for imaging of european commission directorate - general for the environment in conjunction with the uk royal college of radiologists ( 2000 ) and appropriateness criteria of the american college of radiology . 
we collected demographic and clinical data from the ct requests and medical records . this study was reviewed and approved by the fondazione irccs ca granda maggiore policlinico hospital of milan institutional review board . results the ct examination was negative in 18 out of 143 patients ( 12.6 % ) , 12 men and 6 women , with an average age of 56.1 years and age range between 21 and 88 years . 
computed tomography examination was positive in 125 out of 143 patients ( 87.4 % ) , 74 men out of 125 ( 59.2 % ) and 51 women out of 125 ( 40.8 % ) , with an average age of 51.1 years and age range between 10 and 90 years . 
table 1 shows the incidence of the abscesses based on the site , gender and age . 786 radiol med ( 2014 ) 119 : 784789 table 2 distribution of inammatory alterations based on site , gender and age women average age inammatory alterations submandibular space larynx tonsils parotids submental space masticator and parapharyngeal spaces parapharyngeal space oropharynx and supraglottic larynx paravertebral and parapharyngeal spaces parapharyngeal and laterocervical spaces total 19 out of 79 ( 24.1 % ) 4 out of 19 ( 21.1 % ) 3 out of 19 ( 15.8 % ) 3 out of 19 ( 15.8 % ) 2 out of 19 ( 10.6 % ) 2 out of 19 ( 10.6 % ) 1 out of 19 ( 5.3 % ) 1 out of 19 ( 5.3 % ) 1 out of 19 ( 5.3 % ) 1 out of 19 ( 5.3 % ) 1 out of 19 ( 5.3 % ) inammatory alterations tumours 49.6 ( range 1891 ) 65.2 ( range 2191 ) 66 ( range 5873 ) 29.6 ( range 2436 ) 34.5 ( range 2346 ) 55.5 ( range 3972 ) in this group we considered patients with ct signs of inammation , such as cellulitis , thickening of the fascia , and oedematous swelling of muscles or organs , without documentation of abscesses or phlegmons . 
table 2 shows inammatory alterations based on site , gender and age . phlegmons ct revealed 16 cases : 9 men and 7 women , with an average age of 53.1 years and age range between 23 and 83 years . 
table 3 shows the incidence of phlegmons based on site , gender and age . abscesses together with phlegmons we observed two cases : one man and one woman , with an average age of 56 years and age range between 36 and 76 years . 
the man presented submandibular abscesses together with phlegmons that had spread to the submental and parapharyngeal spaces . table 3 distribution of phlegmons based on site , gender and age ct revealed 26 cases : 19 men and 7 women , with an average age of 68.5 years and age range between 49 and 97 years . 
table 4 shows the incidence of tumours based on site , gender and age . ingestion of foreign bodies ct revealed six cases : three men and three women , with an average age of 64.8 years ( range 3580 years )  . 
all the patients had previously undergone standard x - rays of the airways that had proved non - conclusive . benign swellings computed tomography revealed ve cases : three men and two women , with an average age of 44.8 years and age range between 21 and 79 years . 
1 contrast - enhanced computed tomography ( ct ) in a 37 - yearold patient demonstrates an abscess in the submandibular space ( white arrows ) with strands of the subcutaneous fat . 
2 in a 53 - year - old male patient , unenhanced ct demonstrates marked swelling ( white arrows ) of the larynx , pre - epiglottic space , hypopharynx and retropharyngeal space , with a stula ( black arrow ) between the vertebral body and larynx branchial cyst ( one infected , one not ) , two cases showed a struma , and one case , a lipoma . vascular disorders ct revealed ve cases : two men and three women with an average age of 50.8 years and age range between 33 and 64 years . 
four cases showed a haematoma ( two laterocervical and two para - retro - pharyngeal ) and one case a dissection of the vertebral artery . oedema of the larynx computed tomography revealed four cases : three women and one man , with an average age of 70 years and age range between 49 and 85 years . 
the cause of the oedema was not determined in any of the cases . from 1 december 2008 to 31 december 2012 , requests for ct examinations for non - traumatic conditions of the neck accounted for 0.4 % of all ct scans performed in the emergency radiology department of our hospital . 
although the incidence rate of these requests is low in relation to the total number of ct examinations performed , is not without signicance in the daily activity of our department , with nearly one case every 10 days . 
 [ 16 ] , imaging of infectious / inammatory processes has ve crucial roles : to conrm the clinical hypothesis , to dene the extension , to evaluate the presence of complications , to differentiate a drainable abscess from cellulitis and to follow up the infection progression . sonography allows one to distinguish an abscess from cellulitis , to evaluate the presence of thrombophlebitis in the infrahyoid neck , but gives little information on the anatomical extension . 
it also allows assessment , with bone window setting , of the causative periapical abscess and mandibular cortical dehiscence . patients with tonsillitis and peritonsillar abscess had sore throat , fever , cervical lymphadenopathy , dysphagia and pharyngotonsillar exudate . 
they underwent ct examination when clinical diagnosis was uncertain and when there was a deep neck space extension . unfortunately , the aetiopathogenesis of infectious and inammatory conditions remains unclear in 1767 % of cases [ 14 , 16 , 17 ]  . 
in our study , as many patients were discharged without an aetiological diagnosis , it was not possible to make a correlation between clinical examination , imaging and infectious pathogen ; however , we observed that the majority of the submandibular abscesses ( 7 / 13 cases , 53.8 % ) were due to an odontogenic infection process , with a mainly bacterial aetiology . 
as regards inammatory processes of the pharynx and tonsils , which can deteriorate into tonsillar abscesses and phlegmons in the case of superinfection , the initial aetiology is mainly viral . 
however , all the microbial species responsible for respiratory infections may cause pharyngitis and tonsillitis [ 18 ]  . newly found tumours were the second most frequent pathology after infectious / inammatory diseases . 
these conditions may determine airway obstruction , bleeding , compression of the spinal cord , bilateral palsy of the vocal cords and septic thrombophlebitis , all disorders that require an immediate diagnosis and a rapid intervention of ent specialists , surgeons and radiologists [ 6 ]  . in our study , neoplastic pathology was more frequent in males with an average age of 68.5 years , higher than that of the infectious / inammatory processes . 
3 in a 51 - year - old female patient , contrast - enhanced ct demonstrates a newly diagnosed tumour arising from the right thyroid lobe ( arrows ) , displacing the trachea and vessels and causing airway obstruction fig . 
 [ 11 ] , inammatory and infectious conditions ( abscesses , inammatory alterations and phlegmons ) , were the most commonly observed with 79 cases out of 125 ( 63.2 % ) , mostly in males ( 58.2 % ) and in patients with an average age of 47 years . the three neck spaces most frequently involved in the infectious / inammatory processes were the submandibular space [ 1215 ] , followed by the tonsillar and pharyngeal spaces . among the infectious / inammatory conditions , we found a greater incidence of abscesses ( 53.2 % ) , particularly of the submandibular ( 31 % ) and tonsillar ( 31 % ) spaces . 
patients with submandibular abscess on clinical examination showed a visible swelling in the submandibular region , pain , dysphagia and radiol med ( 2014 ) 119 : 784789 performed ct to evaluate the location and extent of airway obstruction and the degree of intrinsic versus extrinsic compression for therapeutic planning . the third most in a smaller percentage , frequent pathology we examined was ingestion of foreign bodies . usually , the most common foreign bodies are sh bones , chicken bones , small pieces of glass , dentures , coins and needles . 
 [ 5 ] , ct can detect ingested foreign bodies such as slightly calcied objects that are missed by conventional radiographs and it allows the assessment of complications . all the other pathologies of the neck found by various authors had a low incidence . 
our study of emergency ct of non - traumatic conditions of the neck fundamentally revealed infectious / inammatory diseases and newly found neoplasms . imaging may be requested in a patient who presents with an acute condition of the neck and the clinical presentation may vary . 
trovato received : 9 may 2013 / accepted : 22 august 2013 / published online : 5 february 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract interest in transthoracic ultrasound ( us ) procedures increased after the availability of portable us equipment suitable for use at the patients bedside . 
it is possible to detect space - occupying lesions of the pleura , pleural effusion , focal or diffuse pleural thickening and subpleural lesions of the lung , even in emergency settings . transthoracic us is useful as a guidance system for thoracentesis and peripheral lesion biopsy , where it minimises the occurrence of pneumothorax and haemorrhage . 
transthoracic us imaging is strongly inuenced by physical interaction of the ultrasonic beam at the tissue / air interface , which gives rise to reverberations classied as simple ( a - line ) , comet tail and ring down ( b - line ) artifacts . although these artifacts can be suggestive of a disease condition , they are essentially imaging errors present even in normal subjects and in empty - pleura post - pneumonectomy patients . 
in order to clarify some confusion and to report on the state of the art , we present a review of the literature on transthoracic us in diseases of the pleura and peripheral lung regions and our own clinical experience over 3 decades . 
thoracic us is much more than shing for the moon in the well . keywords thoracic ultrasound ( tus ) ( cid : 2 ) contrast - enhanced ultrasound ( ceus ) ( cid : 2 ) lung ( cid : 2 ) pleurisy ( cid : 2 ) copd m . 
feragalli department of clinical sciences and bioimaging , institute of radiology , ss annunziata hospital , chieti , italy e - mail : b.feragalli@unich.it introduction ultrasound ( us ) imaging depends on the different physical interactions between ultrasonic waves and the target tissues : in transthoracic ultrasound the images are strongly inuenced by the features of the chest wall and by air in the lungs . 
their interference gives rise to various artifacts , and more than 95 % of the us beam is reected by the tissue / air interface , so it is not available for further imaging [ 13 ]  . the reverberations generated by this interaction have been classied as simple ( horizontal a - line ) , comet - tail and ring - down ( vertical b - line ) artifacts , although some misunderstanding of these terms is apparent from the literature [ 4 , 5 ]  . 
nevertheless , these artifacts all arise owing to the great difference in acoustic impedance in the pleural spaces and are visible to a certain extent when the lung is lled with air . 
similar artifacts are also visible in the pneumonectomy space , which contains residual air , liquid lms and / or oedema and scar tissue : this fact appears to 730 radiol med ( 2014 ) 119 : 729740 disprove attempts to read such artifacts as specic disease markers [ 6 ] the us examination should always be used in conjunction with standard x - ray or ct scans of the chest and is not in itself able to provide a denitive diagnosis [ 7 ]  . methods and techniques one of the main hindrances to the reproducibility of transthoracic us is the machine settings because available equipment does not provide predetermined settings for this application . 
the frequency will need to be adjusted to suit the application , which means a change from 3 to 8 mhz for the convex probe , as will the probe depth , which should range from 70 to 140 . 
tissue harmonics are preferable , in an effort to reduce the natural artifacts , and the time gain compensation ( tgc ) should not exceed 55 % [ 8 ]  . 
it is also important not to forget that the speed of us in the abdominal organs is on average 1 , 520 m / s , with minimal variation between organs , while in the lungs the speed falls to less than a third ( 450 m / s )  . 
the acoustic impedance of lung tissue is 0.0008 rayl 9 10 - 6 , which is very different from the acoustic impedance of the abdominal ( 1.65 rayl 9 10 - 6 ) and kidney organs like the liver ( 1.62 rayl 9 10 - 6 )  . 
this large difference in acoustic impedance at the interface between the surface tissues and air in the lung ( the so - called pleural line ) generates all the artifacts visible under us ( simple reverberations , ring downs and comet tails )  . 
the us beam should be electronically focused on this pleural line , and similar settings should be pre - set for the high - frequency linear probe ( 812.5 mhz ) [ 9 ]  . 
to the right , this is supplied by the liver , while the spleen provides the window on the lethoracic examination must be completed with laterocervical scans , and scans of the armpit in cases where lymphadenopathy is suspected [ 10 ]  . 
this means that us is useful for viewing pleural and subpleural disease in that portion of the pleura , which corresponds to a very small part of the entire pulmonary tissue [ 11 ]  . 
the diaphragm , however , is highly visible on the right using subcostal scans at the radiol med ( 2014 ) 119 : 729740 level of the posterior face of the liver parenchyma . 
it is seen as a hyperechoic line made up of three separate layers , namely the liver capsule / diaphragm muscle interface ( hyperechoic layer ) , the diaphragm muscle ( hypoechoic layer ) and the mirror effect artifact ( hyperechoic layer )  . at the pleural space , the air in the lungs reects almost all of the us beam ( more than 95 % ) , as there is a great difference in acoustic impedance between the soft tissues and pulmonary air at this point . 
these comprise simple reverberations , also known as horizontal , or a - line artifacts , and comet - tail , ( b - line ) artifacts [ 13 ]  . ring - down and vertical fig . 
the thickness of this line does not correspond anatomically to the parietal or visceral pleura or the pleural space , whose thickness does not exceed 300400 lindeed , a similar line is also visible , albeit xed ( without sliding or gliding sign ) , in the residual cavity of pneumonectomy patients . this is due to a considerable difference in impedance between the soft tissues and the postpneumonectomy cavity , which contains air and uid [ 14 ]  . in addition to these artifacts , others are generated by posterior acoustic shadowing at the dense bones of the thoracic cage ( ribs , sternum and scapula ) [ 15 ] and by the so - called mirror effect . 
mirror effect artifacts are typically seen on right subcostal scans and arise , for example , from hepatic lesions being mirrored on the opposite side of the hyperechoic diaphragm line at the base of the lung [ 16 ]  . in the normal lung , simple reverberations ( horizontal or a - line artifacts ) are seen as multiple hyperechoic signals of decreasing intensity parallel to the pleural line and spaced apart by a xed period that is determined by the time between the emission and reception of the us signal . another type of reverberation , the ring downs ( vertical or b - line artifacts ) , described by avruch and cooperberg [ 17 ] , are very distinctive ( and relatively easy to distinguish from comet tail artifacts )  . 
these can be seen posterior to areas where uid and gases are collected , for example in the bowel loops [ 1719 ] , and they have occasionally been misinterpreted as comet tails [ 20 ]  . 
 [ 4 ] , are broad reverberation echoes that travel distally along the direction of propagation of the us beathey take on a triangular shape with a distal tip and resemble the tail of a comethence the name . 
these comet tails originate at highly echoic interfaces , for example , cholesterol crystals on the anterior wall of the gallbladder , metal clips in the parenchyma and gas bubbles inside the bile duct [ 2123 ]  . 
in pleuropulmonary us , comet tails are also due to the presence of two contiguous tissues with a marked difference in acoustic impedance ( soft tissue / pulmonary air interface ) , and they are found in both the normally aerated lung and in other cases where such interfaces occur , i.e. , distal to pleural lesions ( plaques or pleuritis exudate ) or subpleural lesions of any type [ 23 ]  . the number and intensity of the visible vertical artifacts ( b lines ) depend on the type and frequency of the probe used , as well as the degree of total gain compensation ( tgc )  . 
the erroneous use of a medium - to - low frequency or excessive total gain and the lack of tissue harmonic imaging can generate a large number of such artifacts especially in pleuropulmonary us . 
the number of horizontal artifacts ( a - line ) and / or vertical artifacts ( ringdowns or b - lines ) is determined by the relationship between the curve of the probe used with respect to the curve of the pulmonary surface examined . 
whether tissue harmonics are or are not used can produce discrepancies , or at the very least a lack of homogeneity , between images from the same us scan [ 23 , 24 ]  . 
in - depth knowledge of us physics and artifacts enables an operator appropriately preset the us machine , limiting the poor reproducibility due to the use of unsuitable settings ( frequency , tgc , tissue harmonic and electronic beam focusing ) and / or different probes ( convex , sectoral or linear )  . 
this is fundamental because several pathological conditions of the lung can cause these artifacts to increase in number and intensity . these pictures are usually strikingly different from those of the healthy lung , which features a normal ratio between air in the alveoli , quantity of liquid lm ( uids , exudate ) , vascular circulation and pulmonary parenchyma . 
hence , it is essential that we have good and accurate knowledge of the nature of these artifacts and how they appear on - screen , so that we can avoid false , and potentially detrimental interpretations [ 24 ]  . 
4b , after the image gain has been set correctly , the uid is seen as anechoic ( correct diagnosis )  . pleural and extrapleural disease thoracic us is the method of choice for the assessment of pleural effusion , as the diagnosis is simple and accurate using this technique . 
the effusion will show up as anechoic ( black ) area with distinct margins accompanied by movement deeper into the eld of the pleural line . under this , the aerated , consolidated or atelectasic lung will be visible . 
it is possible to quantify the degree of effusion on us by determining the longitudinal and transversal dimensions of the nonechoic area . greatest radiol med ( 2014 ) 119 : 729740 fig . 
left a : homogeneously hyperechoic pleural effusion with elevated gain level ( diagnostic pitfall )  . right b the image in the same patient with normal gain level in anechoic pleural effusion ( correct diagnosis ) several authors have provided formulae to calculate the volume of the effusion , or the degree of compressive atelectasis and its organisation . 
it allows very small collections of uid to be detected , even \10 ml in the costophrenic angle . pathological processes encroaching on the pleural space ( mesothelioma or metastases ) are easy to identify using us , especially if associated with pleural effusion . 
these are visible as hyperechoic lesions or , in certain cases , as mixed echogenic structures associated with a varying extent with pleural thickening , small discontinuities in the diaphragm and , on some occasions , invasion of the thoracic wall . 
us also enables the identication of pleural adhesions , which are visible as circumscribed hyperechoic lesions , which may on occasion be calcied [ 28 ]  . in the diagnosis of pneumothorax , the negative predictive value of us reaches almost 100 % , as the presence of the sliding sign of the pleural line recognisable at b - mode us in real time and well documented by time - motion ( mmode ) us excludes the possibility of this condition [ 29 , 30 ]  . 
the positive predictive value of us in the diagnosis of pneumothorax , however , is reported to vary between 55 and 90 % , because the absence of the sliding sign associated with a reduction in vertical artifacts is not a denitive clue , being also found in severe pulmonary brosis , brothorax , panlobular emphysema , in some intubated patients and those tted with a thoracotomy drainage tube , in cancer invading the chest wall , in pleurisy sequelae and in other conditions . 
furthermore , it should be taken into account that the sliding sign is scarcely visible in scans of the pulmonary apex of healthy lungs , especially in obese subjects , due to the particular anatomy of the region , namely the presence of three ligaments ( transverse - pleural , costal - pleural and vertebral - pleural ) , which limit the visibility of the sliding sign [ 31 , 32 ]  . certain extrapleural parietal lesions can also be visible in us ; these include cysts , abscesses , haematomas , benign tumours , costal metastases , bacterial and tubercular osteomyelitis and tumours of the soft tissues of the thoracic cage ( myelomas )  . 
5 pleural effusion features a anechoic ; b complex nonloculated ; c homogenous hyperechoic ; d complex loculated units , where chest x - ray performed at the bedside is the most widely used and valuable imaging method in the follow - up of critically ill patients [ 33 ]  . 
6 segmental thickening of hyperechoic pleural line ( 3.9 mm ) subsequent to pleurisy in a patient with a previous pneumonitis enlargement , interruption or dislocation of the pleural line , as well as respiratory immobility . 
this is particularly relevant in intensive care pathological processes of the lung can be examined by means of us when the beam is able to reach the pleura , i.e. , there is no air obstructing the beams passage towards the lesion . 
a layer of air - containing tissue , even as thin as 0.3 cm , is sufcient to block the signal and prevent visualisation of a space - occupying lesion , even if it is very large . 
in all normal peripheral lung diseases , us is only radiol med ( 2014 ) 119 : 729740 the pleural thickening of able to image the lesion in cases in which the surrounding consolidated , atelectatic or effusive parenchyma provides an adequate acoustic window [ 34 ]  . 
however , on occasion , when the subpleural or peripheral pulmonary regions are involved , it is possible to identify subpleural nodules , particularly in the dorsal regions at the apices in silicosis , or plaques at the periphery of the inferior lobes in asbestosis . 
pulmonary atelectases , which are categorised as either central ( caused by some kind of obstruction to the bronchial branches ) , or peripheral ( due to compression of the lung parenchyma by effusion , pneumothorax , trauma , severe brosis or tumours ) can easily be diagnosed using thoracic us . 
in cases of atelectasis , the parenchyma will be visible on us as a fairly homogeneous structure , with an echogenicity equal to or lower than that of the liver . 
on occasion , uid - containing tubular structures with echogenic walls are visible inside these are the pulmonary blood vessels and / or mucus - lled bronchi ( us uid bronchogram )  . 
the sonographic picture of bronchopneumonia densities is characterised by the presence of a hypoechoic / echo - free area , which may be mixed hypo / hyper - echogenic , with ill - dened borders . 
hyperechoic stripes or spotsthe air - lled bronchi ( us air bronchogram ) and / or hypoechoic / echo - free tubular structures trapped blood vessels or oedematous bronchi ( us uid bronchogram ) can be seen as well . 
that being said , us is useful after the diagnosis , in the follow - up of pulmonary densities undergoing treatment , as it enables their healing / regression to be monitored [ 38 ]  . 
also in children , as in adults , after a preliminary and mandatory chest x - ray diagnosis , necessary to avoid misleading understatements or clinical decisions , thoracic us should monitor subpleural pneumonitis consolidation and the response to therapy . 
in this context it is a suitable and repeatable alternative to other laboratory measurements and to further radiation exposure of children . echo - free lesions , which are usually well circumscribed , could also be generated by malformation , bronchogenic or pleural cysts , or cysts caused by parasites , or , very rarely , sterile pulmonary infarcts . 
pulmonary abscesses , which appear as circumscribed , uid lled and corpuscular lesions , are only visible on us when they are peripherally located and in contact with the pleuroparietal surface . 
solid lesions , which typically present slightly irregular margins and varying degrees of hypoechogenicity and uniformity , without a particular typical of neoplastic structure are , generally speaking , masses , although these may also present as either hyperechoic , or hypoechoic / echo - free ( in liquefactive necrosis )  . in lung carcinoma , it is possible to see areas of air and / or uid bronchogram , like those found in inammatory consolidation [ 40 ]  . 
any subpleural lesion identied on us must necessarily be conrmed by radiological techniques like computed tomography ( ct ) , positron emission tomography ( pet ) - ct or magnetic resonance imaging ( mri ) , as there is no denitive diagnostic us pattern . 
in fact , even the use of colour doppler inside the lesion , as well as being impeded by the presence of movement artifacts ( ash artifacts ) is unable to accurately distinguish between neoplastic and non - neoplastic disease [ 41 ]  . 
in some cases , there were unenhanced areas consistent with zones of necrosis and these areas were avoided during ne - needle aspiration biopsy ( fnab ) [ 42 ]  . lung cancers have a different behaviour when challenged by ceus and the ceus pattern is different from that of inammatory conditions , such as pneumonitis . 
differences are signicant both as averages and using the most current appearance of nodule conventional cut - off enhancement , which is \10 s for the so - called early enhancement . 
actually , among all the lung cancers , only small - cell carcinoma has a more distinctive pattern , with very early image enhancement and quite early enhancement disappearance , in comparison both with the other cancer histotypes and pneumonitis , so that this information cannot have a practical use . 
one of them is 736 radiol med ( 2014 ) 119 : 729740 identication of the exact location and the direct guidance of the needle under the eyes of the physician . 
the most reliable biopsy - adapted probes have a central hole through which the biopsy set is introduced and that is followed all the time in its path with an image exactly perpendicular to the target and to the transducer , linear array or convex . skipping necrotic areas is a useful information which is provided by ceus , which enables the choice of the most suitable point ( s )  . 
both provide diagnostically useful information on peripheral lung lesions and increase the diagnostic yield of transthoracic fnab by reducing the risk of inadequate tissue sampling . the densities was greater thoracic us is not suitable for formulating hypotheses based on conjecturally specic clues that are , however , confusing when functional - pathological diagnostic patterns do not exist . 
theories put forward on the basis of signs allegedly visible in pulmonary interstitial disease ( acute pulmonary oedema ) seem to be difcult to demonstrate and their results are not reproducible . 
these theories postulated that in the presence of more than six or seven vertical artifacts described as comet tail ( but in actual fact ringdowns or b - lines ) per intercostal space , this pattern could enable distinction between acute pulmonary oedema from other diffuse lung disease ( for example , acute phase obstructive bronchopneumopathy )  . 
in fact , the idea that a subjective visual count of the number of wandering artifacts can be pathognomonic of any one type of lung disease is , to say the least , scientically weak and open to doubt [ 44 , 45 ]  . 
furthermore , artifacts are in essence imaging errors , dependent on a variety of factors and could not alone be a pathognomonic pattern of a single disease state . in fact , an increase in the number of ring - downs and b - lines per intercostal space is generated every time the us beam is intercepted by an excessive quantity of air and liquid lm or exudate or by the presence of brosis in the pleural space . 
this condition is a feature of many diffuse lung and interstitial diseases of various nature , like pulmonary brosis , acute exacerbation of chronic obstructive pulmonary disease ( copd ) , acute bronchial asthma , uniformly distributed pleural effusion and lymphangitis and cannot , therefore , be considered pathognomonic of a particular disease state ( acute pulmonary oedema )  . 
moreover , this clinical condition has been studied and reported in the literature [ 4446 ] , and no statistical signicance has been attributed to such artifacts in the wet lung of patients affected by acute pulmonary oedema , with respect to those affected by other pleuropulmonary diseases ( acute exacerbations of copd , carcinomatous lymphangitis , acute bronchial asthma , pleural effusions and / or chronic cardiac decompensation )  . 
the need for procedure standardisation is obvious : overall b - line measurements or score , as dened and used by some authors , is only a synthetic personal measure of wandering artifacts [ 47 ]  . 
although paved with good intentions such studies fail to reach their goal , i.e. , lung water measurement , a frail methodological basis and weak data can lead to deceptive conclusions , like shing for the moon in the well . us - guided interventions the earlier experiences with us - guided transthoracic puncture of the pleura or pericardium are reported in haemopericardium when emergency intervention was needed for preventing cardiac tamponade and when the subxyphoid approach is less suitable [ 48 ]  . 
as written above , linear - array or convex probes with a central hole are most suitable for fnab : both allow a biopsy needle or a therapy probe to be inserted through the centre of the transducer . the needle , therefore , enters in the centre of the image , perpendicular to the lesion , facilitating difcult procedures like intercostal biopsies . 
7 large number of ring - downs or b - lines in patients with different conditions : a copd ; b acute pulmonary oedema ; c pulmonary brosis in a patient with systemic sclerosis visible on chest x - ray ( for example , to distinguish between effusion and the opaque base of pulmonary consolidation )  . the international literature reports a percentage of pneumothorax in unassisted thoracenteses as between 7 and 16 % , which falls to 0.5 % when us guidance is used . 
in our 10 - year experience , comprising 2 , 850 consecutive usassisted drainage procedures ( diagnostic and therapeutic ) , it was possible to obtain a diagnosis of neoplastic effusion in 228 patients ( 8 % ) through cytological testing and the identication of neoplastic cells in the drainage uid . 
in this sample , the rate of major complications such as pneumothorax was 0.11 % ( three patients , two of whom suffered minimal pneumothorax and another , a subtotal pneumothoraxboth resolving spontaneously ) [ 49 ]  . ultrasound is also very useful in the emergency department , where it can be used to conrm the clinical suspicion of massive pleural effusion in cases of acute respiratory disease and guide its drainage to reduce the risk of pneumothorax to almost zero . 
8 the tip of the needle is visible within the uid of a left - basal pleural effusion needle beginning at the skin line and allows difcult biopsies to be performed with instant feedback on the precise location of the needle tip . 
furthermore , us enables determination of the type of effusion ( simple , loculated or laminar ) and better characterisation of the opaque areas 738 radiol med ( 2014 ) 119 : 729740 through certied training and the use of accurate up - to - date equipment and settings . 
9 us - guided fnab of a hypoechoic subpleural pulmonary lesion ( right lower - basal ) ; the needle ( 20g ) can be seen inside the lesion during withdrawal of the histological cylinder specimen and cytological material ( squamous carcinoma ) pleural lesions in which us - guided transparietal needle biopsy can be useful are nodular pleural thickening , which appear as micronodular hypoechoic structures , often associated with thickening of the pleural line . 
pleural mesothelioma which appears as a mixed hyperechoic lesion is very often associated with ipsilateral serosanguinous effusion [ 51 ]  . it is rare to nd benign lesions like broma or lipoma . all pulmonary lesions visible on us can be aspirated using 2021g cutting / aspirating needles . 
bronchopneumonic densities or pneumonitis , especially in immunodepressed patients , whose origin is undetermined by the usual battery of tests ( sputum material , other effusions , blood culture , serum and urine tests ) , may need to be identied through us - guided fnab ( 22g ) [ 52 , 53 ]  . in cases of pleural empyema , us - guided drainage is a fundamental procedure , and in lung cancer us - guided needle biopsy allows a diagnostic accuracy of 8596 % , depending on the tumour . 
the complication rate for this procedure was 0.2 % ( one case of spontaneously healed partial pneumothorax and one case of total pneumothorax treated by drainage tube ) [ 49 ]  . despite some confusion , enthusiasm and overstatements in the current medical literature and the advent of more advanced imaging systems , transthoracic us is a valuable diagnostic / treatment tool in pleuropulmonary imaging and interventional medicine . 
all patients were studied with thin - section mr imaging of the eye using surface coils . results high - resolution mr imaging of the eye excluded extrascleral extension of disease in 8 / 12 patients : in 4 / 8 cases it revealed vascular ectasia and in the other 4 / 8 cases the linear hypointensity of the sclera was unbroken . 
seven of these eight patients were followed up by ultrasound , which showed stability of melanoma for at least 2 years , while the last patient underwent enucleation , and the histological examination conrmed the mr diagnosis . 
in 4 / 12 patients , high - resolution mr suggested a diagnosis of extrascleral extension of melanoma , which was conrmed at histological examination after enucleation . conclusion high - resolution mr imaging of the eye with surface coils allowed us to evaluate extrascleral extension therapeutic of uveal melanoma and choose the correct t . 
blasi dipartimento di scienze chirurgiche per le patologie della testa e del collo , istituto di oftalmologia , policlinico agostino gemelli , ucsc , rome , italy approach , avoiding unnecessary enucleation in 7 / 12 patients . keywords malignant melanoma ( c04.557.465.625.650.510 ) ( cid : 2 ) uveal neoplasm ( c04.588.364.978 ) ( cid : 2 ) mri ( e01.370.350.500 ) introduction uveal melanoma arises from melanocytes and accounts for less than 1 % of human cancers ; in spite of its rarity , it is the most common primary intraocular malignancy in the white adult population , where it represents 7988 % of primary intraocular cancers , followed by metastatic carcinoma and retinoblastoma in the paediatric population [ 1 , 2 ]  . 
about 90 % of uveal melanomas arise from the choroid , about 510 % from the ciliary body and 23 % from the iris [ 1 ]  . fewer than 1 % of patients are younger uveal melanoma is uncommon in children and young adults ; than 20 years [ 1 ]  . 
it is more frequently seen in older age groups , with a mean age of 5560 years for both males and females and a progressive age - related incidence with a peak at 70 years ( 24.5 per million in males and 17.8 per million in females ) [ 2 , 3 ]  . 
the highest incidence is reported in northern european populations , especially among scandinavians , with 59 cases per million / year and it is more common in the white race [ 2 ]  . 
choroidal melanomas are more frequent in patients with fair complexion and light coloured eyes ( grey / blue ) than in patients with dark eyes , although the role of the sun in the pathogenesis is still unclear [ 4 , 6 ]  . 776 radiol med ( 2014 ) 119 : 775783 several local factors have an independent effect on tumour shape , tumour size , determining the prognosis : degree of pigmentation , optic nerve invasion , retinal detachment and extrascleral extension [ 1 , 710 ]  . 
extrascleral extension of uveal melanoma is a known negative prognostic factor which reduces patient survival and increases the risk of disease recurrence ; it is found more often in larger choroidal melanomas , although it has also been reported in small ones [ 1 , 11 , 12 ]  . 
these prognostic factors inuence therapy , helping to choose between conservative treatment and enucleation [ 1113 ] ; in particular , according to the collaborative ocular melanoma study group ( coms ) , brachytherapy with plates of 106ru and 125i is currently the most common conservative therapy in patients with medium size melanomas ( thickness of 2.510 mm or maximum diameter \16 mm ) , since there is no difference in survival compared to patients undergoing eye enucleation [ 5 , 6 , 14 ]  . 
at present , enucleation is reserved for larger tumours ( thickness c10 mm or maximum diameter c16 mm ) or tumours with extrascleral extension [ 5 , 14 ]  . because of their posterior anatomical location uveal melanomas are not amenable to biopsy without intraocular surgery , so the diagnosis is usually based on clinical and imaging examination , and especially on transocular ultrasound ( us ) [ 5 , 6 , 9 ]  . transocular us is highly sensitive and inexpensive examination commonly used for the evaluation of intraocular tumours and for detection of scleral inltration . 
it has , however , been shown to have some pitfalls : it cannot always allow for a correct evaluation of extrascleral extension , particularly when choroidal melanomas are close to the optic nerve , because of shading of physiological sheaths ; moreover , it may overestimate tumour inltration when there [ 9 ]  . furthermore there are other signs that can simulate extrascleral extension : vessel congestion , venous ectasia or inammatory phenomena of tenons space and extrinsic muscles [ 6 , 7 , 11 , 15 ]  . 
the insertion of extrinsic muscles , especially the inferior oblique muscle , can be misinterpreted as retrobulbar extension of the tumour [ 13 , 15 , 16 ]  . excavation choroidal magnetic resonance ( mr ) imaging may be useful in doubtful cases and allows better visualisation of tumour invasion of surrounding structures compared to transocular us , a and b scan [ 10 ]  . 
mr imaging with surface coils , given its high spatial resolution , multiplanar capabilities and high intrinsic contrast can be useful in the assessment of intraocular tumour and extrascleral extension , especially in posterior choroidal melanomas [ 5 , 7 , 1724 ]  . 
melanomas show a characteristic signal pattern on mr images , being hyperintense to the vitreous on t1w images , hypointense on t2w images , with enhancement after intravenous contrast medium administration ; this specic signal behaviour helps the differential diagnosis with other ocular tumours . 
because of this correlation between melanin content and signal intensity , melanomas with lower melanin content show a lower signal intensity on t1w images compared to those with high content , which are strongly hyperintense [ 1 , 5 , 8 , 15 , 25 , 26 ]  . the primary aim of this study was to evaluate the role of thin - section mr of the eye with surface coils in patients with a us suspicion of extrascleral spread of uveal melanoma . materials and methods in a prospective study , we enrolled 12 patients with a reliable diagnosis of uveal melanoma ( three men , nine women ; age range 3287 ; median age 64.3 ) , 10 of whom previously treated with brachytherapy . 
the us examination , carried out by a single experienced radiologist at the department of ophthalmology of our university hospital , was performed with the standardised a and b scan method , according to the ossoinig qualitative ( b scan ) and quantitative criteria ( a scan )  . 
in 5 / 12 patients , the transocular us diagnosis was conrmed by histological examination . in 10 previously treated patients , extrascleral extension was suspected on follow - up transocular us examination performed after brachytherapy , while in the remaining two patients it was already suspected at the rst us examination . 
extrascleral growth is generally suspected on transocular us and is based on demonstration of a retrobulbar hypoechoic area , next to the melanoma , even without discontinuity of the scleral wall [ 28 ]  . 
vascular ectasia can simulate extrascleral extension because it appears as a retrobulbar hypoechoic nodule , hardly distinguishable from radiol med ( 2014 ) 119 : 775783 excite 1.5t superconducting system , using a phased - array ( temporomandibular joint ) surface coil formed by two exible receive - only elements , each with a maximum diameter of 11 cm and a central opening of 8 cspecial care was taken to correctly position the surface coils above the eyes , with each exible element perpendicular to the long axis of the respective orbit , in order to avoid an asymmetric signal reduction from the centre to the periphery of the acquisition eld . 
to reduce motion artefacts , the patients head was immobilised with pillows on either side and the patient was instructed to x their gaze on a central spot during image acquisition . 
the axial plane included a stack of sections from the inferior to the superior border of the orbital cavity thereby obtaining a good view of the ocular globe , medial and lateral straight muscles , medial and lateral bone boundaries of the orbital cavity and the optical canal . 
the coronal plane included a stack of sections from the anterior margin of the ocular globe to the posterior margin of the dorsum sellae so as to obtain a good visualisation of the superior , inferior , medial and lateral portion of the ocular globe , all of the straight muscles , and an optimal view of the optic nerve and pituitary gland . 
the study was performed before and after intravenous injection of contrast mediupatients received multihance ( 0.2 mmol / kg ) , followed by 20 ml of saline solution at 1 ml / s ow rate , with a delay of 40 s after the injection of paramagnetic contrast medium , before the start of the 3d - fame sequence . the mr images were read by two neuroradiologists in fig . 
visualisation of vascular structures afferent to the nodule can be an important criterion for the differential diagnosis , but these are not always easily recognisable on transocular us . mr with 3d fast acquisition with multiphase - enhanced fast gradient - echo sequences ( 3d - fame ) after contrast medium injection can easily show the continuity of retrobulbar vascular structures , conrming the benign nature of disease . all 12 patients underwent high - resolution mr to evaluate tumour extension . 
the inclusion criteria were the following : age above 18 years ; no other melanomas in any other part of the body at the time of diagnosis ; extrascleral extension ; transocular us suspicion ( preor post - treatment ) of consensus who evaluated : transocular us maximum diameter of the tumour \16 mm or thickness \10 mm ( larger tumours are always enucleated in accordance with the coms guidelines ) [ 5 , 6 , 14 ] ; no pregnancy . all patients signed a patient consent form , after being accurately instructed on the requirements of mr imaging with surface coils and the need to keep a xed gaze and avoid movements during image acquisition . 
mr imaging of the eyes was performed with the patient supine , with a signa the location of the tumour : anterior vs posterior , taking as reference the equator of the ocular globe . 
in the same patient , the contrastenhanced mr fat - saturated image ( d ) shows an enhancing nodule in the retrobulbar space ( arrowhead ) , unrecognisable on the t1 - weighted unenhanced image ( b ) table 2 patient data : information on uveal melanomas , their evolution and correlation with the histological ndings patient age , location shape max . 
one of these four patients underwent enucleation because of extremely rapid growth of the lesion during transocular us follow - up , even though mr did not show any sign of extrascleral extension . 
these intravenous patients underwent enucleation and in all four cases the mr diagnosis was histopathological conrmed evaluation . in 4 / 12 patients the transocular us suspicion of extrascleral extension was induced by the proximity of the melanoma to the optic nerve ; only in two of these cases was extrascleral extension of disease conrmed by histopathology , and correctly diagnosed by mr . in each case , neoplastic tissue and retrobulbar nodules showed marked enhancement after contrast injection allowing for a clear delineation of the lesion with respect to surrounding structures . 
in 5 / 12 patients , we had to repeat some mr sequences because ocular motion artefacts degraded the images ; however , in all patients the images were denitively diagnostic . clinically stable melanomas are usually monitored by clinical and imaging examination and treatment is required only in the case of proven dimensional growth [ 9 ]  . 
in our study , patients who did not undergo ocular enucleation were re - evaluated every 4 months for at least 24 months by transocular us follow - up performed by the same skilled operator who suspected extrascleral extension . regarding the coms studies , transocular us examination shows the same accuracy as histopathology in the evaluation of uveal melanoma dimensions and growth [ 34 ]  . therefore , the absence of extrascleral extension on mr images , the morphological and dimensional stability of the bulbar melanoma / retrobulbar alteration on transocular us follow - up exclude extrascleral extension [ 28 ]  . discussion in our study , we conrmed the prognostic value of the morphology of uveal melanomas . 
mound - shaped melanomas have a large base implant that is usually observed in advanced stages of disease and 4 / 9 cases were found to be positive for extrascleral extension both with mr and histopathology . 
mushroom - shaped morphology , according to the literature , represents an important sign of tumour progression suggesting interruption of the layer that lies between the retina and uvea ( bruchs membrane ) , but this evidence was not conrmed in the single case observed in our study [ 1 , 5 , 9 ]  . retinal detachment , if associated with uveal melanoma , is a sign of progression of disease because it mainly appears in advanced stages of tumour growth ; however , it can be present in small melanomas for individual and still unknown predisposing factors . 
in our study , the only patient with a mr diagnosis of retinal detachment showed extrascleral extension of disease both on mr imaging and histopathology after enucleation , conrming the evidence from the literature [ 5 , 6 , 22 , 26 , 33 ]  . on the other hand , in our experience the difference of average basal diameters of juxtafoveal compared to nonjuxtafoveal melanomas was not signicant , in contrast to the ndings of other authors , who reported that the diagnosis of juxtafoveal melanoma occurs earlier because of the early onset of more severe visual decits [ 5 ]  . extrascleral extension is the most important factor in the choice of the correct therapeutic management , as its presence increases the risk of metastasis ; therefore , according to the coms guidelines , extrascleral extension is an absolute indication for ocular enucleation [ 5 , 14 ]  . 
in our experience , t1 - weighted fat - saturated images obtained after contrast medium injection were the most useful images for the evaluation of extrascleral extension because of the strong contrast between retrobulbar fat ( signal suppressed ) and enhancing melanoma [ 8 , 25 , 32 , 33 , 35 ]  . unenhanced t1w images allowed a better evaluation of orbital anatomy [ 15 , 33 ]  . 
t2 - weighted images proved to be less useful for the evaluation of extrascleral extension because they are more prone to motion artefacts , and have lower signal - to - noise and contrast - to - noise ratios [ 8 , 15 , 33 ]  . 
we had some difculty evaluating extrascleral extension of melanoma in cases of tumour location close to the bulbar insertion of the extraocular muscles , where generally the and muscle enhancement can simulate an extrascleral extension of disease [ 36 ]  . 
venous ectasia / engorgement can be confused with extrascleral extension of disease as it shows marked enhancement after contrast medium injection ; however , in our experience , high - resolution contrast - enhanced 3d - fame images allowed an immediate distinction of ectasia from neoplastic tissue by depicting small serpiginous vascular structures . sclera becomes thinner the greatest difculties encountered in the use of highresolution mr with surface coils were motion artefacts in noncompliant patients , which in many cases induced us to repeat the mr sequences [ 21 , 23 , 25 , 29 , 37 , 38 ]  . 
nevertheless , high - resolution mr of the eye with surface coils provided a correct diagnosis of deep disease extension in all the patients examined . the limits of our study are essentially two : ( 1 ) the patient sample was too small , even considering the rarity of uveal melanoma and the infrequent use of mr examination in patients with more anterior lesions , in which transocular us is often exhaustive , ( 2 ) the lack of histopathological conrmation of the mr data in 7 / 12 non - enucleated patients , without extrascleral extension on mr and followed up with transocular us for at least 2 years ; however , we assumed that the lack of dimensional growth of the melanoma after a long - term transocular us follow - up can be considered a certain sign of absence of extrascleral extension . in our experience , albeit limited , diagnostic evaluation with high - resolution ocular mr in cases of suspected extrascleral extension of melanoma on transocular us allowed destructive surgery ( bulbar enucleation ) to be avoided in 7 / 12 patients , contributing to improve their quality of life . 
high - resolution mr of the orbit proved to be superior to transocular us especially in cases with vascular ectasia , where the mr demonstration of vascular 782 radiol med ( 2014 ) 119 : 775783 structures led to the correct diagnosis . 
similarly , in lesions adjacent to optic nerve or extraocular muscles , the evaluation of the signal pattern and the greater morphological capability of mr compared to us allowed the transocular suspicion to be solved by demonstrating scleral continuity and no extrascleral nodules / plaques . the results of this preliminary study need to be conrmed by clinical trials involving larger patient samples ; however , they suggest that high - resolution mr with surface coils could assume a primary role in therapeutic planning for patients with a transocular us suspicion of extrascleral extension of disease . 
in our single - centre study , we investigated the efcacy of intravenous ( iv ) administration of rt - pa within 4.5 h of stroke onset , in terms of clinical and radiological outcome , using a 3t magnetic resonance ( mr ) scanner in a cohort of patients similar to that of multicentre clinical trials . materials and methods consecutive patients treated with iv rt - pa were compared with an historical cohort of untreated patients ( controls )  . 
inclusion criteria were : ( 1 ) infarction of the middle cerebral artery territory , ( 2 ) eligibility for iv rt - pa treatment , and ( 3 ) 3t perfusionand diffusion - weighted mr imaging and mr angiography performed within 4.5 h and repeated after 57 days . 
growth of the dwi lesion , saved hypoperfused tissue , and clinical outcome was assessed and compared in treated patients and controls . results forty - three patients treated with rt - pa and 69 controls were eligible for the analysis . 
this practical approach aims to treat a higher number of stroke patients at the earliest possible time , also extending the use of thrombolytic treatment to a higher number of stroke centres . 
single - centre studies have demonstrated the usefulness of magnetic resonance imaging ( mri ) in selecting patients for thrombolytic treatment , as well as its feasibility in monitoring rt - pa safety and efcacy [ 9 , 10 ]  . earlier studies have described the efcacy of iv rt - pa up to 6 h after the onset of symptoms , measured by mri and clinical parameters [ 8 , 11 ]  . 
more recently , the safety and efcacy of an mri - based selection protocol stroke treatment within and beyond 3 h compared with standard ct - based treatment have been underlined [ 12 ]  . in that study , the authors concluded that patient selection is more important for a good outcome . than time - to - treatment however , the usefulness of perfusionand diffusionweighted ( pwidwi ) mri mismatch for predicting response to treatment before iv administration of thrombolytic agents has not yet been demonstrated . 
currently , the international guidelines recommend the use of nonenhanced ct or mri in the selection of patient undergoing iv thrombolysis in the time period b4.5 h from the ischaemic event , to exclude an intracranial haemorrhage . 
perfusion mri and the evaluation of the pwidwi mismatch have a key role not yet clearly dened ; in particular , the guidelines say : mri perfusion and diffusion imaging , including measures of infarct in order core and penumbra , may be considered for the selection of patients for acute reperfusion therapy beyond the time windows for intravenous brinolysis . 
these techniques provide additional information that may improve diagnosis , mechanism , and severity of ischemic stroke and allow more informed clinical decision making [ 13 , 14 ]  . the aim of our single - centre study was to evaluate the safety and efcacy of iv thrombolytic treatment administered up to 4.5 h after onset of symptoms by evaluation of clinical parameters and changes in lesion volume on pwi and dwi using a 3t mri unit . materials and methods study population between july 2008 and june 2012 , 361 patients diagnosed with acute ischaemic stroke presented to our emergency department . 
forty - three ( 12 % ) patients were treated with iv rt - pa within 4.5 h from symptom onset and satised the following criteria : ( 1 ) ischaemic cerebral infarction in the territory of the middle cerebral artery ( mca ) , ( 2 ) availability of pretreatment 3t mri with dwi and pwi sequences and mr angiography ( mra ) , ( 3 ) 3t follow - up mri repeated 57 days after symptom onset , ( 4 ) written informed consent of patients or relatives for the necessary diagnostic procedures and therapies . 
patients treated with iv rt - pa were compared with a historical cohort of 69 untreated patients ( controls )  . among the control group , 43 ( 62 % ) patients were selected among consecutive patients admitted to our stroke unit between january and september 2006 , before iv rt - pa administration had been authorised as the standard treatment for acute ischaemic stroke in our hospital . 
all these patients were admitted between 3 and 4.5 h from the onset . the remaining 26 ( 38 % ) patients were selected among patients admitted to our hospital between 3 and 4.5 h from stroke onset , between october 2006 and june 2008 , before iv rt - pa treatment within 4.5 h from symptom onset had been authorised by our local ethics committee . 
all patients were admitted to our stroke unit and managed according to the current guidelines [ 615 ]  . patient information was prospectively entered into a stroke registry by the stroke teaiv rt - pa treatment was administered according to the international guidelines ( 0.9 mg / kg , max 90 mg dose , 10 % in a bolus and the remainder in a 60 - min infusion ) [ 1 , 7 ]  . 
stroke severity was radiol med ( 2014 ) 119 : 767774 assessed with the national institutes of health stroke scale ( nihss ) at admission , 24 h , discharge , and 3 months after stroke onset . 
for functional outcome , a modied rankin scale ( mrs ) score of 2 or less at 3 months indicated functional independence . image acquisition voxel 320 9 157 ; axial t2 - flair imaging all mr images were obtained with a 3t mr scanner ( achieva , philips medical systems , best , the netherlands ) , with an 8 - channel sense head coil . 
this procedure was performed on images acquired on admission and at the 24 h follow - up mri examination . colour maps of relative cerebral blood volume ( rcbv ) , time and time - to - peak ( ttp ) were obtained by relative cerebral blood ow ( rcbf ) , mean transit ( mtt ) processing the initial perfusion images with a curve t algorithm using the software on the philips viewforum console . 
a follow - up mra was performed after 57 days in patients with evidence of intracranial stenoocclusive disease on the baseline scan for vessel patency . the presence of any haemorrhagic transformation on follow - up mri was recorded . 
symptomatic haemorrhagic transformation was dened according to the national institute of neurological disorders and stroke denition ( i.e. , any intracranial haemorrhage that was not seen on a previous imaging scan and any decline in neurological status )  . statistical analysis descriptive statistics was used for baseline and demographic data in both treated patients and controls . 
haemorrhagic transformation of the ischaemic lesion was observed in 9 out of 43 ( 21 % ) treated patients and in 5 out of 69 ( 7 % ) controls ( p = 0.02 ) ( table 2 )  . 
no stroke recurrences or deaths occurred in the treated group , while the 3 - month follow - up revealed two deaths in the control group . regression analysis performed in untreated patients between mean pwi volume and nal dwi lesion volume ( as measured on the follow - up mri scan ) showed that rcbv and rcbf were the haemodynamic parameters which better correlated with the volume of the nal radiol med ( 2014 ) 119 : 767774 fig . 
hence , signicantly increased rates of haemorrhagic transformation of ischaemic lesions were associated with rt - pa treatment which , however , did not determine a clinical worsening or death in any patient . contrarily to the control group , a signicant clinical improvement was observed in treated patients at each follow - up time point , while functional outcome did not differ signicantly in the two groups after 3 months . although the efcacy of thrombolysis has been evaluated extensively using clinical scores , only a few studies have analysed the effects of thrombolytic treatment through mri evaluation . our results are in accordance with the two largest multicentre studies that used mri to select patients for thrombolysis : the defuse [ 16 ] and the epithet [ 17 ] studies . 
our single - centre study has the advantage of not being subject to the potential bias of multicentric studies . in comparison to defuse [ 16 ] , which was the rst prospective multicentre study to perform mri with diffusion , perfusion , and mra sequences , before and after the administration of a thrombolytic agent in consecutive patients treated 36 h after symptoms onset , our study was performed using a 3t mri systethe second found that multicentre the epithet [ 17 ] , study , 772 radiol med ( 2014 ) 119 : 767774 fig . 
follow - up dwi ( g ) and mra ( h ) after iv thrombolysis show recanalisation of the mca with a nal infarction area that is smaller than the initial dwi lesion alteplase was nonsignicantly associated with lower infarction growth compared to the placebo group ( p = 0.054 ) , but reperfusion was more common with alteplase than with placebo . 
not only does our study conrm these results , but it also demonstrates a signicant reduction in growth of the ischaemic area , as measured by dwi ; these results can be explained by the better quantication of the infarcted area and the ischaemic penumbra using a 3t mri scanner . recently , nagakane et al . 
 [ 18 ] demonstrated that , using coregistration of diffusion and perfusion mri maps , it is possible to evaluate the effects of alteplase vs placebo in a more accurate way : in particular , these authors demonstrated that in patients treated with rt - pa the growth in volume of the infarct , measured in dwi , is signicantly lower than in untreated patients . in our study , we were able to obtain similar results without coregistration . 
a metanalysis elaborated from these studies demonstrated that instead of an increased rate of haemorrhagic transformation , iv rt - pa administration has reduced signicantly the incidence of death / dependence both in patients treated within the rst 3 h and patients treated between 3 and 6 h after stroke onset . our observations conrm previous ndings reported in the literature . 
 [ 11 ] observed that , when compared to untreated patients , stroke patients who received iv rt - pa within 6 h after stroke onset had a higher percentage of vessel recanalisation and a better clinical outcome , as measured by mrs . 
the rate of recanalisation was 66.2 % in treated patients , and 32.7 % in controls , which appears to be similar to our ndings ( 65 and 27.5 % , respectively )  . 
unlike previous evidence [ 2 , 7 , 17 , 21 ] , we could not demonstrate a better functional outcome in patients treated with rt - pa , when compared to controls . more severe strokes ( i.e. , higher baseline nihss scores and larger dwi lesion volumes ) in treated patients versus controls , as well as our relatively small patient population , could explain why in our series similar proportions of treated patients and controls were functionally independent at 3 months ( 62 and 65 % , respectively )  . 
however , not all authors agree upon using volume and ow measures to estimate the mismatch and to predict the volume of nal infarct , suggesting ttp or mtt as preferable haemodynamic parameters [ 2629 ]  . our study shows that iv rt - pa administration can modify the natural evolution of the ischaemic lesion . 
in particular , compared to untreated patients , stroke patients treated with iv rt - pa showed a signicantly smaller enlargement of the initial core lesion , as shown by changes in the volume of the 3t dwi lesion , and a signicant reduction of hypoperfused tissue infarction . although we could not demonstrate a signicantly better functional outcome in treated patients compared with controls , treated patients had a signicant improvement in the nihss at each follow - up time point , and nearly twothirds of them were functionally independent at 3 months . to our knowledge , this is the rst series reporting the efcacy of iv rt - pa administration within 4.5 h from acute ischaemic stroke symptom onset evaluated by combined clinical and mri evaluation using a 3t mri unit . 
boulter zoran rumboldt giuseppe bonaldi mario muto alessandro cianfoni received : 27 august 2012 / accepted : 20 january 2013 / published online : 15 february 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract percutaneous spine procedures can be performed with computed tomography ( ct ) guidance . 
the use of ct guidance is cumbersome for procedures where an oblique needle trajectory is imposed by the spatial orientation of the spine , often requiring complex needle triangulation relative to the true axial scan plane . 
a combination of variable ct gantry tilt , and strategic bolster placement under the patient can be used to obtain optimal imaging planes for guidance along the desired needle trajectory . 
we describe our clinical experience using the modied procedure relative to the conventional technique , and provide representative examples . keywords spine interventions ( cid : 2 ) spine procedures ( cid : 2 ) ct guidance ( cid : 2 ) gantry tilt d . 
cianfoni ( & ) neuroradiology , neurocenter of southern switzerland , ospedale regionale di lugano , via tesserete 46 , 6900 lugano , switzerland e - mail : alessandro.cianfoni@eoc.ch introduction many diagnostic and therapeutic percutaneous spine procedures can be performed under imaging guidance , most commonly with uoroscopy or computed tomography ( ct )  . ct guidance has some advantages over uoroscopy , such as cross - sectional anatomical visualization , precise target localization , and superior depiction of osseous and soft tissue structures [ 1 ]  . 
it is limited , however , by the lack of panoramic view and by more cumbersome procedural aspects , due to the necessity for intermittent scans to verify correct needle placement . 
an additional limitation of ct guidance arises from the fact that the ideal needle trajectory often has a cranio - caudal ( cc ) obliquity different from the true axial scan plane , due to the complex anatomical spatial orientation and curvatures of the spine . with conventional axial ct guidance , the operator must scan a large anatomical region to account for the entire needle course , and then must triangulate the needle trajectory over multiple images to predict the nal tip position following advancement . 
this might lead to cumbersome , lengthy , and at times inaccurate needle placement . as a solution to this commonly encountered problem , we describe a simple procedural modication using two features of modern ct scanners , gantry tilt and laser beams , for performance of ct - guided percutaneous spine procedures . the ct gantry can be tilted in the cc direction parallel to the desired needle trajectory , thereby simulating , at least in part , the en - face or bulls eye views , commonly used with uoroscopic guidance . 
we describe the ct - guided percutaneous access to the l5s1 disc , the sacral wing long - axis , the upper thoracic vertebral body , as well as the cervical anterior vertebral elements and discs , as representative radiol med ( 2014 ) 119 : 750757 procedures to illustrate this technique . 
we also describe our clinical experience using the modied technique in a series of patients relative to the conventional method . technique localizing ct scan : choosing the degree of gantry tilt the patient is positioned prone or supine on the ct cradle , with a metallic grid applied over the skin of the presumed region of needle entry . 
the localizing ct scan is then performed through the region of interest with the chosen gantry tilt , to select the single oblique axial image that shows the entire desired needle path , from the skin entry to the target . 
the size and shape of the bolster can be modied by adding or removing rolled or folded sheets and blankets , depending on the requirements of the individual procedure and body habitus . needle - gantry alignment the ct laser beam projects a planar guidance beam aligned with the tilt of the gantry onto the patient . 
most ct systems project two parallel beams in the same planar orientation , one inside the gantry , corresponding to the scan plane , and another a xed distance away . 
both of these beams can be used interchangeably , however , we prefer to use the beam just outside of the bore to perform the procedures , as it allows greater freedom of movement for the operator . 
the right - to - left needle trajectory is left to the experience and ability of the operator as usual , guided by the localizing ct image of interest . procedural imaging guidance intermittent ct scans are obtained throughout the procedure between needle advancements . 
typically three overlapping low - dose images are acquired at each check , with the central image showing the entire length of the inserted needle , from the skin entry to the tip , with one slice above and one slice below in which no needle is visualized . 
of these , 47 were performed in the lumbosacral , 31 in the thoracic , and 15 in the cervical region . procedures performed included vertebral body access radiol med ( 2014 ) 119 : 750757 fig . 
a bolster under the lower abdomen ( c ) attens the lordotic curvature and reduces the l5s1 disc plane obliquity ; under the chest ( d ) attens the thoracic kyphosis and reduces the upper thoracic pedicles obliquity ; under the hips ( e ) increases the lordosis and brings the long - axis of the sacrum closer to the axial plane . the desired needle path for spinal accesses can be paralleled by gantry tilt ( solid lines on c e ) relative to straight axial orientation ( dashed lines on c e )  . 
f gantry - needle alignment , with laser beam precisely bisecting the needle at the hub and the skin entry point . maintaining this alignment keeps the needle in plane and allows visualization of the entire needle throughout its trajectory on a single ct slice through a pedicular or extra - pedicular approach , access to foramina , discs , epidural space , facet joint spaces , sacro - iliac joint spaces , dural sac , paraand peri - vertebral spaces for the purpose of tissue biopsies , drainages , pain management blocks , radiofrequency denervation , percutaneous disc decompression , and cement augmentation procedures . with the conventional method , an initial axial planning ct scan was performed to cover both the needle access point and desired needle target ( generally at least two vertebral body segments )  . 
the true axial scan plane was used to plan the right - to - left component of needle access . sagittal multiplanar reformatted ( mpr ) images were used to determine the cc distance from the skin access site to the nal needle target . 
following this , adjustments to needle trajectory were made using triangulation in the true axial and mpr sagittal images . gantry tilt after initiating the gantry tilt and gantry - needle alignment technique , 315 procedures were performed over a 2 - year period . 
b straight axial ct images of the l5s1 disc ( dashed lines on a ) , which includes portions of l5 and s1 vertebral bodies on the same ct image . 
disc access can be performed in this plane , with the entire needle visualized on a single ct slice in each case , gantry - needle - target alignment was performed using the technique described in detail previously . results overall , the gantry - needle alignment technique required shorter z - axis ct coverage at each localizing scan . 
operator condence in performing complex accesses , such as cervical antero - lateral , paramaxillary , or high thoracic vertebral bodies , was also improved in the gantry - tilt technique . 
the procedure planning time was roughly the same for both techniques . technical challenges difculties were encountered with both techniques due to patient motion , procedure - related discomfort , or anatomical obstructions to access . 
patient movement interfered with the procedure when it occurred either between the scout view and localizing scan , between localizing scan and skin radiol med ( 2014 ) 119 : 750757 fig . 
b tilting the ct gantry allows the longaxis of the sacrum to be visualized on a single image . c bilateral long - axis sacral access , with the entire needle visualized on a single ct slice marking , or during the procedure . 
the incidence of patient motion was approximately equal with both techniques . among the gantry - tilt procedures , patient motion necessitated a new localizing ct scan with new scout view , gantry tilt , and skin marking in 12 cases . 
in two of these patients , pain occurred during a high thoracic sympathetic block with access to the perivertebral space , which resolved shortly after the procedure in both cases . 
in a third patient pain occurred during an intervertebral disc biopsy , which reportedly persisted for over 1 month post - procedure without motor or sensory decit . follow - up of all patients was performed with a phone call at 24 h and 1 week post - procedure , and / or with a follow - up visit 4 weeks post - procedure , depending on the type of percutaneous spine procedures are often characterised by oblique needle accesses in the cc and right - to - left directions discussion follow - up 755 radiol med ( 2014 ) 119 : 750757 fig . 
note that the pedicles are imaged obliquely , and the plane includes both the disc space , ( arrowheads ) and the vertebral body ( black asterisk ) of the level above . b by placing a wedge beneath the chest and angling the ct gantry , the scan plane now parallels the needle alignment for vertebral body access . c trans - pedicular thoracic vertebral body access , with entire needle course visualized . d extra - pedicular thoracic vertebral body access , with gantry - needle - target alignment to account for the complex spatial anatomy and curvatures of the spine . 
in fact , operators using ct guidance for spine procedures often need to perform complex triangulations to calculate the oblique needle path across multiple axial ct slices , to predict nal needle tip location after a certain depth of needle advancement . 
more recently , application of gantry tilt has been described for ct - guided sacroplasty to better depict the path of the needle and improve the safety of the procedure [ 11 ]  . 
while some operators may commonly use some of the technical additions suggested in this report , to the best of our knowledge a combined gantry tilt and gantry - needle alignment technique has not been formally described for a wide range of ctguided spine procedures . 
d the ct gantry can be tilted to different degrees ( dashed lines ) through a combination of neck exion / extension and bolsters , depending on the intended target ( clivus to c3 )  . e localizing scan obtained during iv contrast injection to depict relevant vascular anatomy . 
tilting the gantry differently , and aligning the needle to the gantry , from the same skin entry point the needle can be directed to c1 ( f ) and c2 ( g )  . 
as an example , an l3 pedicular access to the vertebral body can be modied with a minor degree of gantry tilt if the target is in the inferior versus superior portion of the vertebral body . 
the use of gantry - needle alignment holds valid for each ct - guided spine procedure , whether a gantry tilt is applied or not , as it reproduces , at least in part , the en - face or bulls eye technique used in uoroscopy - guided procedures . we have found that adherence to these recommendations increase the versatility and the precision of ct guidance , ensures greater needle control , while obviating the need for complex , time - consuming , and often unreliable needle triangulations . 
gantry - needle alignment using the ct gantrys laser beam also greatly reduces the number of ct sections required at each ct check ( usually 3 slices are sufcient , compared with an average of 12 slices with the standard technique ) , and consequently has the potential to reduce procedure time and radiation dose . radiol med ( 2014 ) 119 : 750757 conclusions the simple addition of gantry tilt and gantry - needle alignment for ct - guided spine interventions allows precise access to the target while minimizing uncertainty of needle trajectory , with a potential to improve procedure ease and accuracy , reduce procedure time and radiation exposure . conict of interest daniel j . 
there are currently many different therapeutic strategies for these rare tumours and combining several different multi - modality strategies have not proved to have superior long - term clinical results . 
in particular , the role of radiation therapy , treatment - related side effects and the use of modern radiation treatment techniques will be discussed . materials and methods a comprehensive literature search was conducted using pubmed in january 2011 . relevant international articles published from january 1980 to january 2011 were assessed . 
orecchia istituto europeo di oncologia , milan , italy by the authors and selected for inclusion based on relevance to this article . conclusions the addition of radiation therapy ( rt ) to wide surgical excision for rps has improved local control rates when compared with surgery alone . 
emerging therapies that employ charged particles ( such as protons and carbon ions ) are expected to be superior in sparing of normal tissues and efcacy over conventional photon therapy radiation , due to their physical and radiobiological properties . keywords retro - peritoneal sarcoma ( cid : 2 ) imrt ( cid : 2 ) proton therapy ( cid : 2 ) carbon ion therapy introduction soft tissue sarcomas ( sts ) are rare , heterogeneous mesenchymal neoplasms arising from the remnant embryonal mesoderma . 
the common histological variants include liposarcoma , leiomyosarcoma , and malignant brous histiocytoma ( mfh ) , which make up 40 , 30 and 10 % of all rps [ 2 ]  . biological behaviour and histological subtypes the distribution of histologic subtypes in rps differs from that of sts arising at other anatomic sites . 
molecular test results should therefore only be interpreted in the context of the clinical and pathologic features of a sarcoma . improvements in diagnosis with the use of magnetic resonance imaging ( mri ) radiographic imaging is a key component of the evaluation of a patient with a retroperitoneal mass . 
the preferred diagnostic study is a computed tomography ( ct ) scan of the abdomen and pelvis to evaluate the primary site , as well as a chest ct to rule out metastatic disease to the lungs . mri rarely adds important information . 
it can also detect metastases to the liver or peritoneuthe radiographic appearance of the primary tumour on ct can also offer clues as to the histologic subtype and grade , which may guide decisions as to the need for pre - treatment biopsy as well as treatment . 
however , the ability to differentiate benign soft tissue from low or intermediate grade sarcomas is limited , and pet and pet / ct are not routinely recommended for the initial workup of a soft tissue mass . the median survival duration is 74 months and the median 5 - year overall survival ( os ) rate is 3658 % [ 4 ]  . 
clinical symptoms are nonspecic and include vague abdominal discomfort ( from the compression on the gastrointestinal system and neural structures ) , weight loss , early satiety and swelling of the lower extremities . 
a surgical resection is considered oncologically adequate only when the tumour is macroscopically completely excised and negative microscopic margins ( r0 ) have been achieved . this is possible only when diagnoses are made in the early stages . 
this may be explained by the high risk of residual disease ( microscopically and macroscopically ) leading to a high risk for local recurrence ( 3782 % at 5 years )  . 
the role of frontline aggressive surgery and how this may impact on the need for adjunctive radiotherapy is the subject of clinical trials [ 7 ]  . radiotherapy ( rt ) is important for tumour eradication and yet it is difcult to deliver high doses ( [ 60 gy ) to the tumour and keep within the dose tolerance of the adjacent organs ( small bowel , spleen and bone marrow ) [ 9 , 10 ]  . 
charged particles therapy is an emerging therapy for rps and currently only preliminary single - centre experiences have been reported [ 11 ]  . although commonly applied for rps in either the preoperative or postoperative setting , there has been a lack of level - 1 evidence for rt specically in the management of rps . 
table 1 shows the results from published studies involving radiotherapy for the treatment of rps . despite the improvement in diagnostic and therapeutic strategies , patients aficted by rps have a poor prognosis . the results of systemic as well as intraperitoneal chemotherapy are disappointing [ 12 ]  . 
preoperative regional 792 radiol med ( 2014 ) 119 : 790802 radiol med ( 2014 ) 119 : 790802 794 radiol med ( 2014 ) 119 : 790802 hyperthermia with systemic chemotherapy is a therapeutic option for high - risk primary or locally recurrent tumours and is the subject of clinical studies . biological marker - directed therapy tumours ( gists ) more recently , a number of targeted therapies have shown promising results in patients with certain histological types of advanced or metastatic sts ( outside of the retroperitoneal space )  . 
imatinib and sunitinib have shown efcacy in patients with advanced and / or metastatic sts other than gastrointestinal stromal ( alveolar soft part sarcoma , chordoma , pigmented villonodular synovitis / tenosynovial giant cell tumour and solitary brous tumour / haemangiopericytoma )  . 
sirolimus has shown promising results in patients with metastatic perivascular epithelioid cell tumours ( pecomas ) and in patients with recurrent lymphangioleiomyomatosis or angiomyolipomas . bevacizumab in combination with temozolomide was well tolerated and effective in patients with locally advanced , recurrent , and metastatic hemangiopericytoma and malignant solitary brous tumour . this review analyses the available published literature and discusses the role of radiation therapy , the related side effects and how the modern radiation treatment techniques may improve the care of patients with sarcomas of the retroperitoneum . materials and methods a comprehensive literature search was conducted using pubmed in january 2011 . 
the keywords for search purposes were : retroperitoneum , sarcoma , radiotherapy and radiation therapy . the search was limited to articles published in english . only peer - reviewed publications dealing with patient outcome were selected . 
rt planning studies ; short communications ; publications without details on rt technique ; publications on paediatric timing , dose , or tumours ; and publications concerning desmoid tumours , dermatobrosarcoma sarcoma , round - cell sarcoma , and angiosarcoma were excluded , because these histopathology types also are excluded from the american joint committee on cancer ( ajcc ) staging systerhabdomyosarcoma , round - cell sarcoma and primitive neuroectodermal tumour were not included protuberans , kaposi soft because of their well - known radiosensitivity . 
finally , articles were selected for this review according to the following criteria : series with a minimum of ten patients presenting rps with at follow - up and least 24 months of addressing various aspects of preoperative , postopintensity - modulated radiotherapy ( imrt ) , erative , intraoperative radiotherapy ( iort ) , intraoperative electron radiotherapy ( ioert ) , brachytherapy ( bt ) , proton therapy and ion therapy . the outcomes of interest were tumour control and toxicity of radiation therapy . in total , 425 reports related to radiation for rps had been retrieved from the initial pubmed search . 
all articles were read in full by the authors and selected for inclusion based on relevance to this article . results preoperative radiation therapy although the majority of published data are about postoperative rt , preoperative rt has several potential advantages . 
 [ 14 ] enrolled 35 consecutive patients with resectable rps who received preoperative external - beam radiotherapy ( ebrt ) with concomitant doxorubicin in a dose escalation trial of 1850.4 gy , followed by surgery plus iort ( 15 gy )  . 
the chemoradiation regimen was completed in an outpatient fashion in 31 of 35 patients ( 89 % ) , while four patients ( 11 % ) required hospital admission for dehydration and / or anorexia . 
grade 34 gastrointestinal toxicities recorded were : nausea ( no vomiting or diarrhoea ) in three patients ( 20 % ) at the 46.8 gy level , and in two patients ( 18 % ) for 50.4 gy level , while patients at the 41 gy level did not record any toxicity . 
 [ 8 ] analysed 83 patients treated at md anderson cancer centre ( mdacc ) and found no difference in local control regarding rt timing with higher doses ( [ 50 gy ) of ebrt or with the specic use of iort . 
 [ 19 ] combined the data from the two prospective trials conducted at the princess margaret hospital ( pmh ) and mdaac to analyse long - term recurrence and survival rates . 
in both prospective studies , the selection of patients who received iort or bt was based on the surgeons intraoperative assessment . fifty - four patients completed the planned preoperative rt and underwent r0 or r1 resection with curative intent . 
although both bt and ioert offered similar local control , bt was associated with signicantly higher toxicity rates . in 2003 , the american college of surgeons oncology group opened the only multi - institutional phase iii trial ( acosog z9031 ) to determine the effect of preoperative rt on patients with untreated primary rps , but unfortunately it was closed in 2005 due to poor patient accrual . this randomized controlled trial was needed to obtain denitive data about the role of rt . intraoperative radiation therapy ( iort ) iort uses low energy x - rays directed to the tumour bed at the time of surgery , commonly by a mobile linear accelerator , which produces electrons ( ioert )  . 
iort may allow delivery of high rt doses to high - risk areas while limiting small bowel toxicity by direct shielding during iort delivery . to date , a trial performed between 1980 and 1985 at the national cancer institute represents the single published randomized control trial involving rt for patients with rps [ 20 ]  . 
these patients were randomly compared with 15 patients who received intravenous misonidazole ( a radio - sensitizer ) plus ioert ( 20 gy ) , administered using abutting or overlapping elds with high - energy electrons of 1115 megaelectron volts ( mev ) , followed by postoperative ebrt ( 3540 gy )  . 
rt morbidity was more signicant in the iort arm : 60 % of the patients in the ioert arm versus 5 % in the ebrt arm 796 radiol med ( 2014 ) 119 : 790802 developed peripheral neuropathy ; 13 % of patients in iort - ebrt arm versus 50 % in ebrt without iort developed enteritis . 
 [ 21 ] reported on 67 patients who underwent surgery and ioert ( median dose , 15 gy ) ; 45 patients underwent additional postoperative ebrt ( median 45 gy ) and the 5and 10 - year actuarial loco - regional control rates were 40 and 33 % , respectively . these authors emphasised that dose escalation with the combination of ioert and postoperative ebrt decreased the risk of recurrence , after macroscopically complete resection . 
furthermore , the 5 - year local - control rate within the ioert eld was 72 % regardless of the resection status , but increased to 84 % after gross resection and 95 % after complete resection . 
intensity - modulated radiation therapy ( imrt ) utilising a simultaneous integrated boost has been used for further dose escalation to high risk margins [ 6 ]  . postoperative radiation therapy the natural history of rps and the high risk for local recurrences support the use of postoperative local treatments . 
postoperative rt is widely used for its advantages that it does not delay the surgery and it can provide selective treatment in the high - risk group depending on biopsy results or when the complete resection is not possible . 
therefore , it is performed mainly in the cases of high grade , resection margins . resection or incomplete inadequate therefore , rt in addition to surgery is widely accepted in the management of rps . 
thirty - six of 45 patients who had undergone macroscopic total resection and postoperative rt had a delayed time to local recurrence compared to patients treated with surgery alone ( p = 0.06 ) for radiation doses higher than 35 gy . 
when only patients with in - eld difference reached statistical signicance ( p = 0.02 ) , suggesting a theoretical role of further dose escalation and boosting the margins at higher risk of recurrence , to improve local control and survival . recurrences considered , stoeckle et al . 
 [ 25 ] reported on 21 patients ( 19 of 21 irradiated postoperatively ) and found radiation doses [ 55.2 gy yielded 75 % of local control , whereas 62 % was obtained for doses \55 gy . 
the outcomes of postoperative rt for rps and the experiences extrapolated from extremity sarcomas [ 2628 ] support a theoretical optimal tumour killing dose 60 gy or higher , to achieve a signicant improvement of local control . 
the ability to deliver such high doses in the retro - peritoneum is limited by the close proximity of radiosensitive organs such as the small bowel , which cannot tolerate more than 45 gy [ 29 ]  . in a postoperative setting , dose escalation is possible by delivering a boost in a focal area at high risk for local recurrence . 
different delivery techniques have been suggested to overcome the limit related to bowel toxicity , targeting the dose selectively to areas at risk for tumour recurrence . discussion levels of evidence of current protocols as opposed to limb sarcoma , adjuvant rt in rps is not considered a standard , since no randomised trial has addressed the question of surgery combined with adjuvant rt , compared with surgery alone . 
in a multi - institutional study where surgery for rps was classical ( limited to tumour only ) , adjuvant postoperative rt reduced the risk of local relapse by a factor of 3 [ 5 ]  . radiol med ( 2014 ) 119 : 790802 level 2a : based on lower level evidence , there is uniform consensus that the intervention is appropriate for resectable disease surgery iort , biopsy should be performed ( to exclude gist or desmoid tumours ) , surgery ? postoperative radiotherapy chemotherapy . 
if a biopsy was not done , further management will be guided by intraoperative frozen section ( i.e. , in the case of iort ) or nal pathology evaluation . for unresectable or stage iv disease preoperative chemotherapy , radiotherapy or combination may be considered to downsize the tumour and surgery may be considered when the tumour becomes resectable . otherwise , management will be palliative in nature and be guided by patients symptoms and performance status . level 2b : based on lower level evidence , there is consensus that the intervention is appropriate after biopsy , preoperative rt may be considered . 
if the patient had preoperative rt , postoperative boost rt is recommended . highly selected patients ( high risk factors ) with r0 resection may be offered postoperative rt . several factors have contributed to a lack of quality evidence regarding optimal management . 
due to the rarity of this disease and the controversial role of postoperative rt , it would be difcult to conduct a randomised study radiodirectly comparing three - dimensional conformal therapy ( 3dcrt ) , imrt and iort or preand postoperative rt . 
furthermore , it is also unknown how the benet might vary among treatment modalities regarding different disease stages , characterised by tumour size , grade , and lymph node involvement . 
although there have been reports on several cohort studies or case series based on singleinstitution experiences with surgical treatment and rt , it is unclear to what extent these ndings from small numbers of patients can be generalised to most patients with rps . there may be substantial variation among surgical ( margin status ) and radiotherapy techniques ( treatment volumes , rt dose ) in the various series . radiation therapy - related toxicity ( comparison among different approaches ) preoperative rt has been associated with lower morbidity rates compared to postoperative rt . 
 [ 18 ] reported on 37 patients treated at the massachusetts general hospital with preoperative rt . of the 25 patients who received a boost with iort , four patients had severe side effects . 
out of these patients , three ( 12 % ) received iort to 1020 gy and experienced gastrointestinal / genitourinary toxicity versus 8 % of whole series treated with preoperative ebrt ( median dose 45 gy )  . 
patients who received ebrt doses up to 50 gy did not have an increase in the rates of complications . the trials from the princess margaret hospital and the md anderson cancer centre are informative because acute toxicities of preoperative rt were prospectively and separately recorded from other toxicities [ 14 , 31 ]  . 
preoperative ebrt was delivered at a median dose of 45 gy and associated with acute toxicity scores of the radiation therapy oncology group ( rtog ) grade b2 in all patients . 
wound complications were observed in 5 % of patients , whereas acute toxicity of rtog grade c3 was recorded in 39 % of patients after receiving surgery and / or bt . 
moreover , 58 % of patients who underwent bt needed hospitalisation with two deaths and one life - threatening illness owing to upper abdominal bt . consequently , the upper abdominal bt was subsequently excluded from the treatment protocol . regarding radiation tolerance of healthy tissues , krempien et al . 
 [ 21 ] recorded grade 2 or higher late toxicity in 21 % of the patients : 13 % of acute gastrointestinal morbidity , 4.5 % gastrointestinal stulae , 6 % small bowel stenosis and 7 % neuropathies . 
in general , severe gastrointestinal morbidity results in patients treated with iort plus postoperative ebrt using a dose of 4555 gy [ 20 , 798 radiol med ( 2014 ) 119 : 790802 21 , 32 , 33 ] , and drastically decreased for doses \45 gy . such low doses ( \45 gy ) , on the other hand , even if well tolerated by the small bowel , are not sufcient to have a tumoricidal effect [ 20 ]  . 
in the randomised study from the national cancer institute , all patients received the same dose with ioert boosts ( 20 gy ) and the rate of peripheral neuropathy was 60 % . 
conventionally , the radiation beam arrangements that have been employed are antero - posterior and oblique elds using computed tomography ( ct ) treatment planning to conform to the target volume and shield the organs at risk . 
co - registration between pre - surgery and post - surgery ct should be done when possible to facilitate the delineation of the posterior involvement of the tumour in the retroperitoneal space . 
the retroperitoneal surface at higher risk of recurrence is dened as the contact area between the resected preoperative gtv and remaining adjacent organ structures ( ipsilateral psoas muscle , ipsilateral muscles of the posterior abdominal wall , pre - vertebral surface around the great vessels )  . 
1 planning ct scan showing a typical gross tumor volume for a typical retroperitoneal sarcoma ( rps ) radiol med ( 2014 ) 119 : 790802 rt and includes more of the intestinal cavity . 
imrt allows delivering of differential doses to different areas at risk , selectively escalating the dose , and hopefully local control . preoperative imrt has the potential to further improve the therapeutic index by permitting dose escalation to the area of the tumour while minimising the dose to normal tissues at risk for radiation toxicity [ 13 ]  . 
it is possible to reduce overall treatment time using an integrated boost concept with simultaneously increased dose per fraction in parts of the target volume which are at increased risk for incomplete resection during planned surgery . 
other than grade 3 nausea / vomiting , no other severe acute toxicity was noted in 16 patients . however , the small patient numbers and short follow - up period prevented assessment of long - term toxicity to peripheral nerves . 
 [ 13 ] described a novel approach for the denition of the ctv for liposarcoma of the retroperitoneuthe suggested ctv included only the region between the tumour and the posterior abdominal wall . 
eighteen consecutive patients were irradiated preoperatively with the imrt technique : the complication proton beam radiotherapy ( pbrt ) : protons are charged particles that deposit most of their energy at a depth proportional to their energy , resulting in the characteristic dose distribution known as the bragg peak . 
based on qualitative analysis of normal tissue effects in the clinic ( quantec ) benchmarks , the dosimetric advantage of proton therapy may be less gastrointestinal and genitourinary toxicity [ 37 ]  . mgh reported a study of pbrt and / or imrt ( median dose of 50 gy ) with ioert ( single fraction 1020 gy ) in 28 patients with rps [ 38 ]  . 
after a median follow - up of 33 months , only two patients ( 10 % ) with primary disease experienced local recurrence ( lr ) , while three patients ( 37.5 % ) with recurrent disease experienced local recurrence . 
this strategy may minimise radiationrelated morbidity and reduce local recurrence , especially in patients with primary disease . current trials in proton therapy at the moment , there are two active trials in north america to address the issue of proton therapy in rps . 
the university of florida is assessing treatment feasibility of preoperative proton therapy for resectable intermediate or high - grade retroperitoneal sarcoma . high linear energy transfer ( let ) radiotherapy sarcoma has been traditionally considered to be resistant to conventional let radiation . 
the reason may be from the 800 radiol med ( 2014 ) 119 : 790802 mechanism of cell damage : low let radiations generate injuries indirectly through the formation of free radicals and / or directly with ionizations in the patient . 
the formation of radicals depends heavily on oxygenation level . consequently , the sensitivity of tissue to low let radiation depends on the degree of blood supply to the tissues and also on the types of tissues , presence of free radical scavengers and cell cycle phase . the degree of ionisation of low let radiation is sparse in tissue ; the mean distance between two ionisation events is far greater than the diameter of deoxyribonucleic acid ( dna ) double helix . 
the physical advantages are low dose deposition in the entry channel , followed by a steep dose deposition in the target region ( the bragg peak ) , and then a sharp dose fall - off with no exit dose . 
from the biological point of view , heavy ions can produce dense ionisations within the tumour , resulting in multiple clustered dna breaks , which are more difcult to be repaired by the intrinsic cellular repair pathways . 
minor differences between the two are a sharper lateral penumbra and a dose tail beyond the bragg peak for the carbon bealike all charged particles , carbon ions have a variable let that increases with the depth of penetration into tissues . 
carbon ions therefore produce sparse ionisations in the entrance channel and dense ionisations in the bragg peak . in the last part of their track , carbon ions release a higher dose and results in a higher effectiveness in the target volume ( compared to protons )  . 
carbon has an rbe ratio in the bragg peak to ions . rbe in the plateau region higher therefore , carbon ion radiotherapy ( cirt ) has to combine the optimal dose conformality of potential proton therapy with the increased local control of neutron therapy without the increase in unwanted side effects of the latter [ 3941 ]  . 
moreover , cirt possesses various biologic advantages such as high let radiation , decreased oxygen enhancement ratio ( oer ) , diminished capacity for repair of sublethal and potentially lethal damage , and diminished cell cycle - dependent radiosensitivity when compared with those observed with low let radiation . than other from 1993 , cirt has been performed at the national institute of radiological sciences ( nirs ) in chiba , japan . the optimal dose for inoperable , residual or recurrent bone and sts has been determined within dose escalation trials to be at 70.4 gye ( gray equivalent ) in 16 fractions over 4 weeks [ 4244 ]  . 
therefore , cirt could be considered for patients with rps with residual macroscopic disease after surgery due to inltration of surrounding organs or unresectable tumours . existing and planned carbon ion facilities in asia and europe are activating clinical protocols in rps and more time is needed to verify these preliminary experimental data . conclusions a multidisciplinary team with expertise in sts should manage all patients with rps . 
preoperative rt is preferred to postoperative rt especially in patients with high - grade or intermediate - grade rps and for selected cases of lowgrade rps ( e.g. , extremely large or appearing unresectable or borderline resectable )  . 
for patients with either intermediateor high - grade histology or positive margins who have undergone surgical resection without preoperative rt , postoperative rt is a reasonable option . iort with / without preor postoperative ebrt is also a reasonable option , especially for patients with tumour close to critical organs or gross residual disease after surgery . new types and delivery techniques in rt could further improve patient outcomes . 
due to their physical and radiobiological properties , charged particle rt ( such as protons and carbon ions ) are expected to be better in tissues and with higher efcacy than sparing normal radiol med ( 2014 ) 119 : 790802 conventional photon therapy rt . 
however , in the absence of a randomized controlled trial , it is impossible to determine whether any putative improvement in tumour outcome is a consequence of selection bias or other confounding factors . 
in light of the growing awareness of the issue of ionising radiation dose and the possible risk for the individual and the population , there is a need for radiologists , medical physicists and radiographers to s . 
salerno dipartimento di biotecnologie e biotecnologie mediche e forensi , universita` di palermo , aoup policlinico , via del vespro 127 , 90127 palermo , italy e - mail : sergio.salerno@unipa.it play an active role in dose management . 
in this review , the authors try to delineate the problem in a consequential and multifaceted way : radiationpatient interaction , possible mechanisms of damage , main ct dose units , risk and its quantication in the population , with the aim of optimising the acquisition dose without diagnostic drawbacks . 
for an up - to - date use of ct , radiologists must know the dose concerns for the single patient and population , and use the ct apparatus with the best dose care ; substitute ct with other diagnostic techniques when possible , especially in children ; reduce the number / extension of scans and phases , and the dose in single scans and single examinations . keywords ct ( cid : 2 ) radiation exposure ( cid : 2 ) dlp ( cid : 2 ) ctdi ( cid : 2 ) radiation dose ( cid : 2 ) absorbed dose introduction exposure to ionising radiation in computed tomography ( ct ) is a problem that is becoming progressively more important as ct has acquired the role of a rapid , total - body exploratory examination ; is very popular with both patients and clinicians and is considered a defensive tool in the diagnostic setting . 
an increase not only in the absolute number of ct examinations , but also in terms of both length of coverage and number of phases obtained while scanning ( baseline , arterial , sometimes two , venous , late ) has been observed [ 1 , 2 ]  . 
in some places , this is the product of an expedient exchange of the ease and speed of acquisition against appropriateness ; however , there is an abuse of the technique . 
the exposures to be reduced without 804 radiol med ( 2014 ) 119 : 803810 problem is compounded by scanners that seem friendly , but are in fact becoming increasingly complex , favouring the adoption of new practices without giving full regard to the optimal use of dose reduction algorithms . 
it is thus possible that a given instrument , in a single department , as used by various operators for examination of a single body district may yield doses that no longer depend predominantly on the limits of the machine but are operator dependent , with the important implication that some choices of the technicians and radiologists may not be justiable from diagnostic or dose limitation perspectives . the extent of this problem is not entirely known and cannot be adequately addressed without proper knowledge of all the phases that lead to the effective dose calculation [ 3 , 4 ]  . however , there is no doubt that ct investigations are increasing from every point of view : numbers of requests , extension , and scan phases [ 1 , 2 ]  . in light of the growing awareness of the issue of radiation dose and the possible risk for the individual and population there is a need for radiologists , medical physicists and radiographers to take on an active role in dose management . 
the purpose of this review is to delineate the problem in a consequential and multifaceted manner : radiationpatient interaction , possible mechanisms of damage , main ct dose units , risk and its quantication in the population , with the aim of optimising the acquisition dose without diagnostic drawbacks . 
this is extremely important because of the increased awareness of patients , as well as some recent decisions by the american college of radiology and legislative measures by individual american states ( california state dose bill [ 5 ] ) , which change the professional and legal perspective on the practice of ct , establishing a model that might be quickly and uncritically emulated elsewhere . radiation damage table 1 computed tomography dosimetric values acronym symbol unit measure dose in air locally absorbed dose total absorbed dose effective dose ctdiair ctdi100 ctdiw ctdivol mgy cm ctdi computed tomography dose index , dlp dose length product inuenced by the structure ; in fact the transcription zones are repaired faster than the silent zones , using enzymes and co - factors that recognise the damage . 
their lack does not allow a timely repair inuencing the survival and then the probability of inducing mutations and carcinogenesis processes [ 6 ]  . the calculation of dose in ct the rapid evolution of ct technology and the consequent spread of new clinical applications have determined a deep understanding of all information regarding ct dose calculation and awareness of primary denitions of parameters for this estimate , which should be revised following the evolution of technology . 
the ctdi is a basic concept to understand dose measurement in ct and is dened by : ctdi dzdz mgy ionising radiation interacts with the medium in which it propagates yielding its energy . 
in the case of photons ( x - rays ) , low let radiation , it is more probable that the interaction takes place with the water molecules that are present in billions of copies in the cell and represent 80 % of the weight . 
this primary transfer , in living organisms , starts a complex series of chemical reactions that are a prerequisite for cell changes and the possible beginning of pathological alterations . there is solid experimental evidence that dna is the main target of ionising radiation and that the damage is not uniformly distributed along the molecule . 
even repair is where : d ( z ) is the prole of the absorbed dose along the z axis , n is the number of slices acquired in a single axial rotation ; the value of n may be less than or equal to the maximum number of channels available on the system ( for example 64 for a multislice ct detector with 64 rows )  . 
the ctdiair is characteristic for each scanner and depends on tube current intensity and voltage , beam collimation , ltration and the radiol med ( 2014 ) 119 : 803810 complete ct examination and is dened as the product of the ctdivol multiplied by the irradiated scan length l . the dlp expressed in mgy cm is : dlp ctdivol ( cid : 3 ) l the dlp is a comprehensive dose descriptor and allows the assessment of risk by an estimation of the effective dose using the appropriate conversion factors dened by anatomical region . 
these conversion factors have been dened in a document of the european commission [ 7 ] and updated after the release of icrp 103 in 2007 to consider the weighting factors for the different tissues shown in table 2 [ 8 ]  . obviously , this approach does not take into account the individual patient size or the specic examination , but allows a rough estimate of the effective dose for protocol optimisation . 
however , there is a debate in the scientic community about the fact that ctdivol and consequently , dlp are no longer adequate ct dose descriptors for a number of reasons . 
the 100 - mm - long ionisation chamber is not suitable for multislice ct , because it is not long enough to measure the wider beam width or to include the contribution of the tails of the dose prole , resulting in an underestimation of the measured ctdivol . 
finally , the ctdi is not suitable for ct exposures where the patient remains immobile ( or almost immobile ) during acquisition ( cone - beam ct or perfusion studies ) , in which case the value reported on the scanner console is an overestimation of the mean absorbed dose in the scan volume . these criticisms are in fact based on the false assumption that the ctdivol should estimate the dose to the patient . 
in reality , the variety of patient types , scan protocols and clinical applications is such that no single existing phantom is able to accurately estimate the dose in all patients . 
since dose distribution in the phantom is generally not uniform , the measurements are acquired at ve different positions ( in the centre and at the four cardinal points ) , thus introducing the weighted ctdi ( ctdiw )  . ctdiw ctdi100 ; c ctdi100 ; p where ctdi100 , c and ctdi100 , p are measured at the centre and at the periphery of the phantom , respectively , and the index 100 indicates that the ctdi was measured with a 100 - mm - long ionisation chamber . 
the ctdiw , however , does not take into account the pitch used during a spiral acquisition . it was , therefore , necessary to dene the volumetric ctdi , the ctdivol , i.e. 
ctdivol ctdiw pitch it should be noted that the term mas indicated on some manufacturers consoles does not refer to true mas , but to mas per rotation divided by the pitch . 
finally , as we do not acquire a single - slice but a whole volume , we should also consider the length of the scan and introduce a second dose descriptor : the dose length product ( dlp )  . 
furthermore , as the ctdivol is displayed on the console before starting a scan and recorded in the dose report at the end of the examination , many users assume that this is the individual patient dose . 
the ctdivol is no doubt still useful , but it should be clear that it is a standardised phantom measurement of the ct system output , which enables users to optimise and compare radiation output between different protocols or different scanners and not the real dose delivered to the patient . patient dose population dose from ct was a radiation protection concern before the advent of ultrafast multidetector scanners ; in fact , diagnostic reference levels ( drls ) for ct examinations have been dened in european guidelines [ 7 ] and in the italian law d.lgs. 
87 / 00 since 2000 [ 9 ]  . even though drls should not be applied to individual exposures but are reference doses for common examinations , they can help to optimise radiation protection to avoid unnecessarily high doses to the patient . 
for ct , the ctdiw and the dlp were suitable quantities to be used as drls . the italian drls for ct are derived from a european document based on a british study performed in the early 1990s . 
since then , ct has undergone major evolution and while ctdiw was a good metric at the time of single - slice ct scanners , now it has been replaced by the ctdivol commonly displayed by the ct scanner console . in 2006 , shrimpton et al . 
 [ 10 ] published a national survey , a review of patient doses from ct examinations in the uk in 2003 , conducted on the basis of data received from over a quarter of all uk scanners , of which 37 % had multislice capability . 
the mean uk doses for adult patients were in general lower by up to 50 % than previous ones , although doses were slightly higher for multislice relative to single - slice scanners . 
the relative increase in reference dose was larger for scans of the head and the chest ( high resolution )  . these examinations both involve axial scanning with narrow beam collimations , where beam penumbral effects and differences in z axis geometrical efciency between single and multislice scanners were most pronounced [ 10 ]  . a similar investigation , prior to the widespread adoption of multislice ct was conducted in italy in 2004 and published in 2006 [ 11 ]  . 
the survey was carried out for seven adult clinical ct protocols , and showed that ctdiw and dlp were always below the drls set by the european guidelines [ 7 ]  . 
now the rst italian nationwide survey about adult exposures from mdct and including multiphase studies is at last available [ 12 ]  . the subsequent advances in ct technology made it possible to collect multiple images per rotation and to acquire a given volume of data in a much shorter time interval . 
this caused a general increase in the dlp , due to the wide use of multiphase examinations and a larger application in paediatric radiology . in paediatric patients , ct radiation protection became greater concern due to inherently higher radiosensitivity of growing tissues ( such as cartilage , red marrow ) , and childrens longer life expectancy that involves a longer interval in which one can develop a possible neoplasm . analysis of the risks associated with paediatric ct mainly refers to the study by brenner [ 13 ] , which highlighted the increase in the probability of occurrence of tumours when patient age decreased . 
it should be noted that abdominal ct in a child increases the probability of tumour occurrence to more than 20 % . however , the main dosimetric aspects connected with the use of ct in paediatrics are still poorly standardised : 1 . 
the classic ct dose descriptors are based on phantoms with diameter simulating the geometry of an adult and introducing signicant uncertainties in the evaluation of organ doses in children . various tools have been used by different research groups to perform size - dependent dose evaluations . 
 [ 19 ] used the monte carlo n - particle ( mcnp ) radiation transport code to calculate normalised effective dose values for three different scanners and mathematical anthropomorphic phantoms with ages ranging from newborn to adult . 
they demonstrated the high dependence on patient age and size : the effective dose in a newborn was 1.5 times greater than that of an adult for all types of examinations . 
other dosimetric aspects associated with paediatric ct regard optimisation procedures [ 20 ]  . dose reduction systems dose reduction is one of the main problems in ct , and many techniques have been developed to face this problem , such as tube current modulation and voltage reduction . automatic dose modulation is based on the principle that the operator decides on the desired image quality in terms of noise index , reference mas , or reference image , depending on the ct system manufacturer , and the scanner radiol med ( 2014 ) 119 : 803810 table 3 iterative dose reduction system and corresponding acronym , producer and year of commercialisation acronym meaning producer year of commercialisation asir adaptive statistical general 2008 iterative reconstruction electric trade name ( mbir ) general 2009 electric iris image reconstruction in siemens 2009 image space safire sinogram - afrmed siemens 2010 iterative reconstruction idose aidr trade name philips adaptive iterative dose toshiba 2009 2010 reduction automatically selects the right tube currenttime product ( mas )  . 
the system automatically regulates tube current referring to scout images in the z ( longitudinal modulation ) and xy ( transverse modulation ) axes . the limits of these modalities in obtaining additional dose reduction are determined by the inverse correlation between mas value and image noise . 
hence , a new algorithm called iterative reconstruction ( ir ) has been proposed by manufacturersused in the past and abandoned because of the long reconstruction time imposed by older computerswhich is currently capable of additional dose reduction [ 21 ]  . 
 [ 22 ] published an extensive review of the different modalities of dose reduction systems ( table 3 )  . iterative modalities are based on mathematical algorithms , which are not fully accessible because various vendors produce them as black boxes mainly for the commercial impact of these tools . 
however , it is possible to divide these modalities into two types : those working on the control of the images , using a statistical method for noise reduction , and those directly managing the raw data domathe latter allow for a further dose reduction , but imply a complex analysis with longer processing time [ 22 ]  . radiation dose and associated cancer risk although ct accounts for less than 19 % of radiological examinations [ 3 ] , its contribution in radiation dose for the general population is becoming signicantly higher . 
for doses lower than 100 msv ( 100 mgy with wr equal to 1 ) , the risk calculation is based on the linear no - threshold model ( lnt ) that is mainly accepted and adopted by the large majority of international organisations in the eld of radiation protection as icrp , beir , nrpb , unscear , etc . 
103 guideline modied the estimation of cancer risk from low radiation levels . in fact , they increase the risk for the induction of somatic damage in the population up to 6 % per sv received , remaining unchanged at 0.2 % for genetic risk . 
for risk reduction , at low dose levels , in addition to the linear model without threshold ddrf ( dose and dose rate effectiveness factor ) , a factor of 1.5 was used ; conversely , the icrp adopted a factor equal to 2 [ 23 ]  . estimation of cancer risk represents a complex problem and many factors must be considered in cancer induction , not only low - dose x - rays used in ct . 
due to the greater sensitivity of young subjects to radiation damage , the risk factor is 34 times more than in adults [ 27 , 28 ]  . in ct examinations , only body segments and not the entire body ( such as brain , chest and abdomen ) are usually exposed , so the risk calculation should take into account 808 radiol med ( 2014 ) 119 : 803810 tissue - specic weighting factors ( such as the breast in chest exposure , which increases the risk )  . many publications consider it incorrect to calculate a single individual risk , and underline the lack of sound evidence of cancer risk for doses less than 50 msv . 
finally , the risk estimation based on the japanese nuclear bomb survivors compared to the dose commonly used in ct is considered questionable [ 29 ]  . as the icrp guidelines well outline , it is incorrect to extrapolate an individuals cancer risk [ 30 ] , as the guidelines are for the cumulative cancer risk of a population . following brenners publication [ 31 , 32 ] some papers calculated the effective cancer risk with a simple arithmetical calculation ( number of ct examinations multiplied by mean exposure in msv of the population ) resulting in impressive and overestimated rates of cancer related to medical exposures in the general population [ 29 ]  . 
the study determined that the increased cancer incidence rates after ct exposure in these cohorts are mostly due to irradiation [ 35 ]  . incidence rates another additional criticism of exponential cancer risk is related to the evidence of the linear relation of the damage in opposition to the nonlinear relation of the cellular reparative mechanism , with consequent overestimation of the damage [ 36 ]  . 
 [ 38 ] underlined that the accidental chronic exposure to low gamma radiation from cobalt 60 determined protective effects against tumours ; in fact the expected tumour rate in this population is lower than expected . although the scientic community is still debating the effects of low dose levels , some misinterpretations of scientic papers and some questionable ct practices have resulted in internet forums and newspaper articles on ct linked to cancer in single groups of patients . 
the fda has established an initiative to reduce unnecessary radiation exposure from medical imaging ; the california state government has promoted a law imposing a dose report in every ct scan ( dose bill ) [ 5 ] , including cases of overdose and a strict annual control of the dose used for every protocol by the medical physicist . 
moreover , a european community ( ec ) directive aiming to impose the dose report in the radiological report ( council directive 242 , 2012 laying down basic safety standards for protection against dangers arising from exposure to ionising radiation ) is risk denial and risk under evaluation . 
are radiologists and clinicians sufciently prepared on the subject of cancer risk ? dose risk knowledge are all the subjects involved in ct prescription and execution prepared on dose risk ? according to some experiences published in the bmj [ 39 , 40 ] , doctors working in the uk national health service have insufcient knowledge about radiation protection , despite serious continuous education programmes for health professionals and a widely available publication for referring physicians entitled how to make the best use of the diagnostic radiology department , in which the practice of dose reduction is extensively described [ 41 ]  . introduction of radiation protection in medical school programmes is also recommended in european guidelines to all state members ( european commission medical exposure directive ) [ 10 , 42 , 43 ]  . in italy , possible knowledge gaps among referring physicians , radiographers and radiologists have not been investigated despite the fact that since 1995 italy has had detailed legislation regulating the patients radiation protection and operator education and training [ 43 ]  . 
an increased attention to the problem should be adopted in young radiologists , who are more involved in emerging radiation technologies and new applications . in june 2009 , the american college of radiology and the radiological society of north america set up a task force to increase radiation protection knowledge and reduce unnecessary imaging in particular in paediatric patients . radiol med ( 2014 ) 119 : 803810 conclusions dose reduction in ct relies on the correct implementation / optimisation of protocols and everyday practice . we can signicantly reduce unnecessary radiation exposure by being aware of patient risk and using all the available resources in the ct apparatus to the best advantage . 
to synthesise what radiologists are required to do to ensure an up - to - date use of ct , we can state that they should : know the dose concerns for the single patient and population , in the knowledge of possible risks and using the ct apparatus with the best dose utilisation ; involving referring physicians substitute ct with other diagnostic techniques when possible especially in children ; reduce the number / extension of scans , phases , the dose in single scans and examinations , also optimising contrast and reducing costs . glossary and denitions to facilitate reading of this review , this section recalls the unit measures used in radiation protection and dosimetry in alphabetical order . absorbed dose d is the measure of all types of ionising radiation and is dened a d de dm where de represents the mean energy deposited to the mass dm by the ionising radiation . 
the adsorbed dose in si system is measured in joule per kilogram ( j kg - 1 ) and named gray ( gy )  . the absorbed dose is calculated from the energy deposited ( e ) , does not reect the single event of interaction and its value is obtained as a mean on a generic element of mass ( dm )  . the radiation damage for low dose levels is supposed to be correlated with the value of adsorbed dose related to a specic organ or tissue . 
to account for the different modalities of radiation interaction and different radiation sensitivities of tissue two other values need to be introduced : the equivalent dose ( ht ) and the effective dose ( e )  . the unit measure is the same as the adsorbed dose j kg - 1 , but it is called sievert ( sv )  . diagnostic references levels ( drl ) are dened dose levels used in diagnostic and nuclear medicine for typical groups of patients of standard body mass or a standard phantom dened for different systems . 
it may also be interesting to compare doses from different diagnostic the use of similar technologies or procedures and / or technologies or procedures across hospitals or countries to compare technologies for the same medical investigations . the effective dose , however , is not recommended for epidemiological evaluation either for detailed retrospective analysis on exposure and risk of single individuals . the interpretation of effective dose , in patients exposed for medical purposes , remains complex especially when organs or tissue is subjected to partial or heterogeneous exposure . pitch in multislice spiral ct is dened as the ratio of the table increment over the detector collimation . 
one can assume that the detector collimation for each of n detector arrays is the same , excluding cases of either different collimations or combined measurement row . conict of interest stefano colagrande , daniela origgi , giovanna zatelli , andrea giovagnoni , sergio salerno declare no conict of interest . radiol med ( 2014 ) 119 : 803810 23 . 
verdun fr , bochud f , gundinchet f et al ( 2008 ) quality initiatives radiation risk : what you should know to tell your patient . radiographics 28 : 18071816 28 . 
krille l , zeeb h , jahnen a et al ( 2012 ) computed tomographies and cancer risk in children : a literature overview of ct practices , risk estimations and an epidemiologic cohort study proposal . radiat environ biophys 51 : 103111 29 . 
meer ab , basu pa , baker lc , atlas sw ( 2012 ) exposure to ionizing radiation and estimate of secondary cancers in the era of high - speed ct scanning : projections from the medicare population . 
pearce ms , salotti ja , little mp et al ( 2012 ) radiation exposure from ct scans in childhood and subsequent risk of leukaemia and brain tumours : a retrospective cohort study . 
matthews jd , forsythe a , brady z et al ( 2013 ) cancer risk in 680000 people exposed to computed tomography scans in childhood or adolescent : data linkage study of 11 million australians . 
chen wl , luan yc , shieh mc et al ( 2007 ) effects of cobalt - 60 exposure on health of taiwan residents suggest new approach needed in radiation protection . 
royal college of radiologists ( 2007 ) making the best use of clinical radiology services ( mbur ) referral guidelines , 6th edn . royal college of radiologists , london 42 . 
identication of af prior to rfca is paramount to select those patients who are truly amenable to the ablation procedure , which is expensive and not entirely free of risks . keywords atrial brillation ( cid : 2 ) atrial brosis ( cid : 2 ) magnetic resonance ( cid : 2 ) late enhancement introduction atrial brillation ( af ) is the most frequently encountered cardiac arrhythmia in clinical practice , with a prevalence of 0.51 % in the general population and up to 6 % among those older than 65 years [ 13 ]  . 
ablation procedures to electrically disconnect the pv from the left atrium ( la ) have become a common alternative in patients refractory to medical therapy [ 58 ] , and their efcacy is inversely proportional to the extent of atrial brosis produced by the arrhythmia ( electrical , mechanical and anatomical remodtherefore a elling ) [ 912 ]  . 
to integrate the dicom images with the carto3 system , anatomical evaluation of the la - pv complex was carried out on the basis of a three - dimensional ( 3d ) flash angiography sequence acquired during the administration of a 10 ml bolus of gadobenate dimeglumine ( multihance , bracco , milan , italy ; 0.1 mmol / kg ) at a ow rate of 2 ml / s . 
acquisition began 15 min after the injection of the paramagnetic contrast material and the sequences lasted 1520 min on average , depending on respiratory variability and heart rate . on le - mr , brosis was dened as an area of high signal intensity of the atrial wall relative to the normal myocardiuthe la was divided into seven segments ( pv antra , oor , anterior wall and posterior wall - roof )  . 
the presence of brosis was qualitatively evaluated by two radiologists with different levels of experience in cardiac mr imaging ( m.c. , 7 years ; g.c. , 3 years ) who were blinded to any previous ablation procedures . 
the basic anatomical structure was displayed in different colours indicating the voltage levels and correlating with the hearts electrical vitality . the bipolar voltage of the atrial endocardium is normally around 0.39.5 mv ; values \0.5 mv are considered to be low amplitude whereas those lower than 0.05 mv are usually associated with areas of brosis [ 17 ]  . as done in the analysis of the le - mr images , the la was divided into seven segments , each of which was assessed for the presence of brosis . a qualitative analysis was performed by comparing the areas of le on the mr images with the segments radiol med ( 2014 ) 119 : 595600 displaying low voltage values on eam : anatomical agreement was assessed by comparing the segments of brosis and / or healthy tissue detected by the two modalities , with agreement being dened as optimal whenever there was concordance of at least six out of seven segments . sensitivity ( se ) , specicity ( sp ) , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy were nally calculated . results at the time of the examination , 11 / 37 patients were in af . five of 37 patients ( 14 % ) were excluded because of poor quality of the mr images : in two cases because of failure to suppress the cardiac signal ( incorrect ti choice inuenced , in one case , by the presence of af ) ; in two cases resulting from irregular because of major artefacts breathing and af ; in one case because of inadequate sampling of the thoraco - abdominal interface by the respiratory navigator . 
a , b late - enhancement ( le ) - mr axial images of the left atriuc , d 3d electroanatomical maps integrated with mr angiograms ( carto3 ) in posterior ( c ) and anterior ( d ) views ; the functional information is dened by a colour code that provides an immediate evaluation of atrial electrical activity . 
a , b le - mr axial images of the left atriuc , d 3d electroanatomical maps integrated with mr angiograms ( carto3 ) in posterior ( c ) and anterior ( d ) views . 
the le - mr image ( arrow in a ) does not show pathological late enhancement close to the ostium of the left superior pulmonary vein , whereas the electroanatomical map identied ( arrow in c ) an area of brosis at this level . 
the le - mr image shows a hyperenhanced area ( brosis ) in the anterior wall of the left atrium ( arrow in b ) whereas the electroanatomical map shows normal potential ( purple ) at this location ( arrow in d )  . 
the resulting atrial remodelling promotes the development of af and , with time , makes spontaneous reconversion to sinus rhythm increasingly less likely [ 9 ]  . atrial brosis is therefore both a cause and a consequence of af . 
the effectiveness of the new treatments aiming at electrically disconnecting the pv from the atrium is to the extent of brosis [ 13 ]  . inversely proportional radiol med ( 2014 ) 119 : 595600 detection of brosis is therefore paramount when selecting candidates for af ablation procedures , which are costly and not free of risks [ 14 ]  . in our work , we tried to identify atrial brosis noninvasively , using a le - mr imaging sequence ; in addition , unlike most studies on the subject [ 13 , 14 , 18 ] , we decided not to use post - processing techniques to maximise signal hyperintensity , so as to simplify the diagnostic process of brosis detection . 
in comparison to spragg et al.s work [ 22 ] , which selected patients who had already undergone the ablation procedure , our series consisted of mixed group of patients , 32 % of whom had undergone a previous ablation procedure . 
these two factors may account for the discrepancy in results ; while the se was lower ( 66 vs 84 % ) , the sp was higher ( 87 vs 68 % ) with a resulting npv of 85.5 vs 73 % , which makes the le - mr technique a good candidate for stratifying patients to be treated with ablation . 
in an attempt to eliminate the artefact , at the beginning of the study the navigator was shifted to the more lateral and anterior sectors of the right hemidiaphragm ; however , this approach led to incorrect sampling of right hemidiaphragm excursion , resulting in a longer sequence without eliminating the artefact . in the present study , eam was considered the reference standard . 
several comparative studies have , however , reported a spatial error for eam equal to 510 mm [ 24 , 25 ] ; in addition , by expressing the prevalent voltage of endocardial rather than epicardial myocytes , eam may provide data that are not always correct with reference to the overall thickness of the atrial wall . 
in light of these the le - mr considerations , we could hypothesise that sequence has a greater rate of brosis detection compared to eam . study limitations the poor technical quality of le - mr images ( 14 % of examinations were not assessable ) is dependent on patient compliance , the presence of arrhythmia during the study and the difculty selecting the ti . 
however , these sequences have sufcient signalto - noise ratio only for slice thickness of at least 6 mm , which makes them inappropriate for the study of the atrial wall ( thickness , 13 mm [ 19 ] )  . 
re lucia calculli luca frulloni roberto pozzi mucelli received : 9 august 2012 / accepted : 30 july 2013 / published online : 18 march 2014 ( cid : 2 ) italian society of medical radiology 2014 computed enlargement shows diffuse abstract multidetector - row tomography ( mdct ) and magnetic resonance ( mr ) imaging are currently the most frequently performed imaging modalities for the study of pancreatic disease . 
in cases of suspected autoimmune pancreatitis ( aip ) , a dynamic quadriphasic ( precontrast , contrast - enhanced pancreatic , venous and late phases ) study is recommended in both techniques . 
in the diffuse form of autoimmune pancreatitis ( daip ) , the pancreatic parenchyma appears , during the mdct and mr contrast - enhanced pancreatic phase , diffusely hypodense and hypointense , respectively , compared to the spleen because of lymphoplasmacytic inltration and pancreatic brosis . 
in the focal form of autoimmune pancreatitis ( faip ) , the parenchyma shows segmental enlargement involving the head , the body - tail or the tail , with the same contrast pattern as the diffuse form on both modalities . faip needs to be differentiated from pancreatic adenocarcinoma to avoid unnecessary surgical procedures , since both diseases have similar clinical and imaging presentation . 
finally , in all cases of uncertain diagnosis , mdct and / or mr follow - up short - term treatment ( 23 weeks ) with high - dose steroids can identify a significant reduction in size of the pancreatic parenchyma and , in faip , normalisation of the calibre of the upstream main pancreatic duct . after keywords chronic pancreatitis ( cid : 2 ) autoimmune pancreatitis ( cid : 2 ) acute pancreatitis ( cid : 2 ) computed tomography ( cid : 2 ) magnetic resonance ( cid : 2 ) steroid treatment autoimmune pancreatitis ( aip ) : denition and classication autoimmune pancreatitis ( aip ) is a form of chronic pancreatitis associated with autoimmune processes . 
distinct histological and clinical proles reveal two subtypes of aip , indistinguishable on the basis of imaging alone : type 1 , or lymphoplasmacytic sclerosing pancreatitis ( lpsp ) , radiol med ( 2014 ) 119 : 558571 and type 2 , or idiopathic duct - centric pancreatitis ( idcp ) [ 1 ]  . 
type 1 , lpsp , or aip without granulocyte epithelial lesions , seems to be an igg4 - related multiorgan disease , characterised by elevated serum igg4 levels , multiple extrapancreatic organ involvement and igg4 - rich lymphoplasmacytic inltrate on histology in all the affected organs [ 2 , 3 ]  . 
in type 2 aip , idcp or aip with granulocyte epithelial lesions , there is no extrapancreatic organ involvement or igg4 - rich inltrate on histology , and serum igg4 elevation is unlikely . 
this form appears to be a pancreas - specic disorder and is histologically characterised by the presence of neutrophils with typical granulocyte epithelial lesions . the diagnosis of aip is challenging even at expert centres and many different diagnostic criteria have been developed . 
the comprehensive criteria that must be fullled for the diagnosis include pancreatic imaging of the parenchyma and ductal system , serological and histopathological ndings , other organ involvement and response to steroid treatment [ 1 ]  . the clinical presentation overlaps with other forms of acute and chronic pancreatitis , but without a history of alcohol or tobacco abuse or biliary stone disease . 
aip may vary in its clinical presentation depending on the pancreatic distribution of disease ( focal or diffuse ) and on the specic site involved ( head , body or tail of the pancreas ) [ 421 ]  . 
in diffuse forms or in focal distribution in the pancreatic body - tail , patients may present pancreatic abdominal pain in the epigastric region , irradiating to the back with or without jaundice [ 821 ]  . 
therefore , the clinical presentation of aip may mimic pancreatic adenocarcinoma in the focal forms and pancreatic lymphoma or non - necrotizing acute pancreatitis ( nnap ) in the diffuse forms [ 2226 ]  . in evaluating patients with suspected pancreatic disease , acute or chronic pancreatitis or pancreatic neoplasms , multidetector - row computed tomography ( mdct ) and magnetic resonance ( mr ) are the imaging modalities of choice [ 1517 , 2733 ]  . 
in the specic case of suspected aip , a dynamic quadriphasic study ( precontrast , contrastenhanced arterial , pancreatic , venous and late phases ) is recommended for both techniques . technically , in mdct of the pancreas , contrast medium administration typically involves the use of bolus tracking software with a region of interest ( roi ) placed over the aorta and a predetermined attenuation threshold of 100 hu . pancreatic arterial and portal venous phase images are acquired 2030 and 6070 s after bolus tracking , respectively , and the delayed phase images 180 s after the beginning of the injection . 
the standard reconstruction thickness used during the pancreatic and portal venous phase is 1 mm , with an interval of 0.5 mm , whereas during the late phase it is 21 mm , with a range of 10.5 mpostprocessed coronal and curved mdct multiplanar reconstruction ( mpr ) images are recommended in cases of suspected aip . pancreatic mr and mr cholangiopancreatography ( mrcp ) imaging must be performed on a 1.5 t scanner using a surface phased - array body coil . 
to eliminate overlapping uid - containing organs on t2 - weighted mrcp images , 50150 ml of superparamagnetic iron oxide particles is administered 1020 min before the mr examination . pancreatic mr imaging includes the following sequences : axial t1 - weighted gradient echo , axial t1 - weighted fatsaturated , axial t2 - weighted fat - saturated rapid acquisition with relaxation enhancement ( rare ) , t2 - weighted halffourier rare , coronal true fast imaging in the steady - state precession ( true - fisp ) , axial and coronal , coronal oblique 2d half - fourier rare cholangiopancreatography , axial fat - saturated 3d volumetric gradient echo . 
a quadriphasic dynamic study is performed during injection of 0.1 mmol / kg body weight of gadolinium chelates by means of a power injector at 22.5 ml / s , by acquiring the precontrast - phase , late arterial / pancreatic phase ( 3545 s ) , portal venous phase ( 7580 s ) , and delayed phase ( [ 180 s )  . 
for diffusion - weighted imaging ( dwi ) , a spin - echo echoplanar sequence is performed with a b value of 0 , 50 , 600 s / mm2 . 
the intrapancreatic segment of the common bile duct is slightly dilated ( arrow head ) ; the intrahepatic bile ducts are normal . in the left kidney , a solid cortical lesion is present which later proved to be chronic autoimmune pyelonephritis on biopsy ( black arrows ) ; the right kidney shows a cystic lesion . 
according to some authors , this peripheral rim of delayed contrast enhancement is due to the presence of a chronic inammatory process and brous tissue involving the peripancreatic fat [ 15 , 20 , 21 , 44 ]  . 
the periductal inammatory cell inltration and brous tissue centred around the pancreatic ducts [ 12 , 13 , 4449 ] produce diffuse narrowing of the main pancreatic duct ( mpd )  . 
patients with aip often demonstrate duct the mpd wall on ct imaging ( the enhancement of enhanced duct sign ) [ 42 , 43 ] and this could reect periductal inammatory changes . 
the enhanced duct sign is strongly associated with the abnormal enhancement area of the pancreas in aip and , although relatively uncommon , this nding may be useful for the diagnosis of aip . both the enhanced duct sign and the inability to visualise the mpd lumen within a daip lesion can aid in the diagnosis of aip . 
also peripancreatic stranding , represented by inammatory changes of peripancreatic fat in mild acute non - necrotizing pancreatitis , recorded as a hypodense peripancreatic halo in all phases of ct examination [ 32 , 37 ] is absent in daip [ 50 ]  . daip must be differentiated from nnap and lymphoma since both these pathological conditions show diffuse enlargement of the pancreatic parenchyma [ 19 , 25 , 51 , 52 ]  . in both daip and nnap , pancreatic abdominal pain with epigastric location irradiating to the back , increase of serum amylase and lipase and diffuse pancreatic enlargement are frequently present [ 2831 ]  . 
recently , this vascularisation pattern of daip has been assessed using the rate of relative variation in enhancement from the previous phase or relative enhancement rate across all phases of the mdct study [ 50 ]  . 
a statistically signicant difference in the two groups of patients ( daip and nnap ) regarding the presentation of peripancreatic stranding and retroperitoneal uid has been demonstrated [ 50 ]  . 
in conclusion , the pattern of mdct contrast enhancement of daip and nnap , particularly considering the relative enhancement rate parameters [ 50 ] , provides qualitative and quantitative clues for differentiating the diseases . 
the pancreatic gland is surrounded by a hypodense halo in all mdct phases ( peripancreatic stranding : arrow head ) due to mild inammatory changes of peripancreatic fat . pancreatic lymphoma ( e , f )  . 
secretin is a polypeptide hormone that induces pancreatic bicarbonate - rich uid secretion into the duodenum and increases the tone of the sphincter of oddi with a temporary distension of the pancreatic ducts . 
the pancreatic parenchyma appears hypodense compared to the spleen and unaffected adjacent parenchyma of the body - tail during the contrastenhanced mdct pancreatic phase ( b , d )  . 
the main pancreatic duct is partially invisible because of focal ductal stenosis due to lymphoplasmacytic inltration and areas of brosis in the pancreatic body and head , with upstream main duct dilatation . 
the pancreatic head lesion ( short arrow ) appears more hypodense compared to the spleen and to the body - tail during pancreatic ( b ) , venous ( c ) and late ( d ) phases . 
the mesenteric vein lumen ( arrow head ) near the solid lesion in the pancreatic head has a reduced diameter ( vascular inltration ) mpd stricture resolves after secretin stimulation , this rules out a malignancy and is suggestive of aip ( the so - called duct penetrating sign ) [ 61 ]  . 
on the other hand , dwi and adc values are variable in pancreatic cancer , allowing for this modality to differentiate between massforming focal aip and pancreatic carcinoma . the nal differential diagnosis between focal daip and pancreatic cancer can only be conrmed by a ne - needle aspiration biopsy [ 62 , 69 , 70 ]  . extrapancreatic aip : mdct and mr ndings ct and mr can identify some of the many extrapancreatic manifestations of aip , most commonly biliary , renal and retroperitoneal [ 17 , 71 ]  . biliary involvement , present in up to 80 % of aip patients , is the most common extrapancreatic involvement . both intrahepatic and extrahepatic bile ducts can be involved , showing multifocal stenosis and wall thickening 566 radiol med ( 2014 ) 119 : 558571 fig . 
axial 3d volumetric t1 - weighted fat - suppressed gradient - echo images after intravenous contrast medium administration during pancreatic ( a ) , venous ( b ) and delayed phase ( c )  . 
diffusion - weighted mr steady - state precession ( true - fist ) spin - echo echoplanar dw image with imaging ( dwi ) : axial b value = 600 s / mm2 ( e ) ; axial apparent diffusion coefcient ( adc ) map calculated from baseline images obtained with b value of 0 , 50 , 600 ( f )  . 
the overall pancreatic gland is enlarged with sharp borders ( ad ) and presents decreased enhancement in the arterial pancreatic phase ( a , d ) compared to the spleen , with an increased progressive contrast uptake during the venous ( b ) and the delayed ( c ) phases . 
the affected pancreatic parenchyma appears slightly hyperintense in the dw images ( e ) with lower adc value ( f ) than patients without pancreatitis due to a severe inammatory cellular inltration ( lymphocytes , plasma cells and granulocytes ) resembling primary sclerosing cholangitis . 
this is an important technique to evaluate involvement of the biliary ducts , which is frequently associated because the periductal inltration can extend to the intrapancreatic cbd and even to its suprapancreatic segment . 
axial 3d volumetric t1 - weighted fat - suppressed gradient - echo images before ( a ) and after intravenous contrast medium administration during the pancreatic ( b ) , venous ( c ) and delayed phases ( d , f )  . 
the parenchyma of the pancreatic body - tail shows focal enlargement ( arrows ) with sharp borders and abnormal signal intensity : it appears hypointense in the t1 - weighted images ( a ) compared to the unaffected parenchyma . 
in the dynamic study , the aip - affected parenchyma shows decreased enhancement during the pancreatic phase ( b ) , with a homogeneous and progressive contrast uptake during the venous ( c ) and delayed phases ( d )  . 
the main pancreatic duct is not visible within the faip ( e : arrowhead ) , compressed by the crowded cellularity all around , with an upstream dilation ( e )  . 
in both cases ( a , b , cf ) , diffuse pancreatic enlargement and hypodense pancreatic parenchyma are present during the pancreatic phase . mdct also shows a retroperitoneal soft tissue mass surrounding peripancreatic vessels ( a , b : arrows ) and right side pelvic vessels ( d : arrow )  . 
both in diffuse and focal aip , the pancreatic parenchyma appears isovascular to the spleen in the enhanced radiol med ( 2014 ) 119 : 558571 pancreatic phase and hypovascular in the venous phase , with wash - out in the delayed phase . 
finally , mdct and mr imaging can easily identify normalisation of the calibre of the intraand suprapancreatic common bile duct [ 19 , 20 , 37 ]  . the japan pancreas society has proposed diagnostic criteria for the diagnosis of aip [ 7478 ]  . 
these criteria include : the nding of typical pancreatic imaging results ( enlargement of the pancreatic parenchyma and mpd narrowing ) , positive laboratory tests ( autoantibodies and elevated serum levels of immunoglobulin g4 ) and positive histopathologic al ndings ( lymphoplasmacytic inltrate and pancreatic brosis )  . 
the differential diagnosis of aip is difcult when a patient with typical clinical ndings has other associated autoimmune disorders with only non - specic imaging and / or histopathological ndings . 
in all the cases in which aip is strongly suspected but the diagnosis is uncertain , mdct and mr are useful imaging modalities to suggest the correct diagnosis . repeated mdct and / or mr examinations after short - term treatment ( 23 weeks ) with high - dose steroids can identify a signicant reduction in the size of pancreatic parenchyma , and the normalisation of the calibre of the mpd and bile ducts . 
the response at short - term imaging follow - up after steroid treatment was recently considered a diagnostic criterion of aip [ 1 ]  . conict of interest rgraziani , s . 
we veried whether adding and combining proton mr spectroscopic imaging ( 1h - mrsi ) , diffusion - weighted imaging ( dwi ) and perfusion - weighted imaging ( pwi ) information at 3 tesla facilitate such discrimination . materials and methods twenty - nine patients with histologically veried high - grade gliomas , who had undergone surgical resection and radiotherapy , and had developed new contrast - enhancing lesions close to the treated tumour , underwent mri , 1h - mrsi , dwi and pwi at regular time intervals . 
the metabolite ( cho ) / normal ( n ) chon , n - acetylaspartate ( naa ) / naan , creatine ( cr ) / crn , lactate / lipids ( ll ) / lln , cho / crn , naa / crn , cho / naa , choline ratios naa / cr and cho / cr were derived from 1h - mrsi ; apparent diffusion coefcient ( adc ) from dwi ; and the relative cerebral blood volume ( rcbv ) from pwi . results in serial mri , recurrent gliomas showed a progressive enlargement , and radiation injuries showed regression or no modication . 
tedeschi dipartimento di neuroscienze , seconda universita` di napoli , naples , italy radiol med ( 2014 ) 119 : 616624 keywords radiation injury ( cid : 2 ) recurrent brain tumour ( cid : 2 ) magnetic resonance spectroscopy ( cid : 2 ) diffusion - weighted imaging ( cid : 2 ) perfusion - weighted imaging introduction standard - of - care therapy of high - grade brain gliomas includes surgical resection followed by radiotherapy and chemotherapy , but the tumour most often recurs or progresses after this multiple therapeutic approach [ 1 ]  . 
in a frequency up to 30 % , patients develop a radiation injury that mimics tumour recurrence or progression on conventional magnetic resonance ( mr ) imaging [ 1 , 2 ]  . 
histopathological analysis is currently considered the gold standard for the correct diagnosis [ 2 ] , but it requires the acquisition of tumour samples by open craniotomy or stereotactic biopsy , procedures which place the patients at an increased risk for morbidity and mortality [ 3 ]  . 
thus , a noninvasive technique is highly needed . imaging methods that emphasise metabolic , structural and haemodynamic properties of tissues , namely proton magnetic resonance spectroscopic imaging ( 1h - mrsi ) , diffusionweighted imaging ( dwi ) and perfusion - weighted imaging ( pwi ) respectively , may be helpful for the discrimination of tumour recurrence / progression from radiation effects [ 1 , 4 ] , and could limit the need for brain biopsy . 
considering such limitations , several authors have used a variable combination of 1h - mrs , dwi and / or pwi information in addition to mri features for improving such discrimination [ 612 ] , and some of these studies have been performed at 3 tesla [ 6 , 810 ]  . 
switching to high magnetic eld strengths allows several advantages , such as higher signal - to - noise ratio and better spatial , temporal and spectral resolution [ 13 , 14 ]  . this study aims to further evaluate the usefulness of combining metabolic , diffusion and haemodynamic information in the differentiation between recurrent glioma and radiation injury using a pattern recognition analysis . 
to our knowledge , there is no study in which 3 - t1h - mrsi , dwi and pwi parameters have been combined in a discriminant function - based pattern recognition approach to enhance such differentiation . materials and methods patients and treatments thirty - three patients with pathologically veried highgrade gliomas , who had apparently total surgical resection , radiotherapy and chemotherapy , and had conventional treatment development of new contrast - enhancing lesions in the vicinity of the original treated tumours , were consecutively included in this study . 
the remaining 29 patients ( 18 men and 11 women ; median age , 62.5 years ; range 3874 years ) had a histopathologic diagnosis of glioblastoma multiforme ( who grade iv )  . 
postsurgical radiotherapy ( daily fractions of 2 gy for a total of 60 gy , 5 days a week during 6 weeks ) plus temozolomide at a dose of 75 mg / m2 / day followed by six cycles of adjuvant temozolomide ( 150 mg / m2 / day in the rst cycle and then 200 mg / m2 / day , for 5 days during each 28 - day cycle )  . follow - up mr examinations started between 4 and 8 weeks after completion of radiotherapy and continued at 2to 3 - month intervals during the rst year and at 3to 6 - month intervals during the following years , depending on the clinical course . 
the local ethics committee approved the research protocol and informed consent was obtained from all patients . imaging mr studies were executed with a mr scanner at 3.0 tesla ( general electric medical systems , milwaukee , wis . ) with the standard quadrature head coil . 
mri , dwi , 1h - mrsi and pwi were acquired in that order during the same examination to allow exact comparison of results , and acquisition data were analysed by an automated software package ( functool , ge medical systems ) in a remote workstation . 
all image data were checked for overall image quality and motion artefacts before analysis . the mr imaging protocol included : ( a ) sagittal t1weighted localising images by fast spoiled gradient - echo ( fspgr ) sequence ( slice thickness 5 mm ; gap 1 mm ; repetition time , tr , 225 ms ; echo time , te , 2.5 ms ; eld of view , fov , 24 cm ; ip angle , fa , 75 ( cid : 3 ) ; number of excitations , nex , 2 ; matrix 512 9 256 ; acquisition time 1 min 57 s ) ; ( b ) transverse t2 - weighted fast spin - echo ( fse ) images ( slice thickness 5 mm ; gap 1 mm ; tr 5 , 000 ms ; te 85 ms ; fov 24 cm ; nex 1 ; matrix 448 9 320 ; acquisition time 2 min 39 s ) ; ( c ) transverse uid - attenuated inversion recovery ( flair ) images ( slice thickness 5 mm ; gap 1 mm ; tr 11 , 000 ms ; te 140 ms ; inversion time 2 , 250 ms ; fov 24 cm ; nex 2 ; matrix 288 9 192 ; acquisition time 5 min 53 s ) ; ( d ) gadolinium618 radiol med ( 2014 ) 119 : 616624 enhanced t1 - weighted volume fspgr images ( slice thickness 1.4 mm ; tr 225 ms ; te 3.2 ms ; fov 24 cm ; fa 15 ( cid : 3 ) ; nex 1 ; matrix 320 9 288 ; acquisition time 23 min ) which were acquired nally , after pwi . two - dimensional 1h - mrsi was performed with the proton brain exam - spectroscopic imaging ( probe / si ) protocol ( ge medical systems )  . 
point - resolved spectroscopy ( press ) pulse sequence ( slice thickness 10 mm ; tr 1 , 500 ms ; te 144 ms ; fov 24 cm ; phase 16 ; acquisition time 6 min 53 s ) , preceded by chemical shift selective saturation ( chess ) pulses for water suppression , was used . 
the peak amplitude of each metabolite was obtained by computing the maximum peak values in the range : lactate and / or lipids ( ll ) , 1.581.0 ppm ; n - acetylaspartate ( naa ) , 2.182.01 ppm ; creatine ( cr ) , 3.153.0 ppm ; choline ( cho ) , 3.363.21 ppthe normalized ratios cho / chon , naa / naan , cr / crn , ll / lln , cho / crn and naa / crn ( where n means normal ) were obtained by dividing each metabolite value within the pathological roi by that within an exactly contralateral and symmetrical normal roi , when possible , or within a contralateral representative normal roi . the non - normalized ratios cho / naa , naa / cr and cho / cr were calculated by dividing the metabolite values in the same spectrum [ 19 ]  . diffusion - weighted imaging was performed using single shot , spin - echo type echo - planar imaging resulting in axial images ( slice thickness 5 mm ; gap 1 mm ; tr 11 , 000 ms ; te 66.6 ms ; fov 24 cm ; matrix 164 9 192 ; acquisition time 44 s ) at b = 0 mm2 / s and b = 1 , 000 mm2 / s as the maximum b value applied along the three orthogonal directions . images with b = 0 provided a set of t2 - weighted images , whereas those with b = 1 , 000 mm2 / s provided three sets of true diffusion images in the x , y , and z directions that were geometrically averaged to obtain one diffusion - weighted image . 
immediately before the acquisition , a 0.01 - mmol / kg pre - bolus dose of gadopentetate dimeglumine was administered to minimise contrast leakage and t1 shortening effects from enhancing lesions [ 15 ]  . 
after the rst ten acquisitions , a bolus of gadopentetate dimeglumine ( 0.1 mmol / kg ) was injected with a mechanical injection pump ( 4 ml / s ) through a 20 - gauge intravenous catheter , followed by a 20 - ml saline ush . 
the echo - planar images were transferred to the remote workstation where the software calculated on a voxel by voxel basis : the curves of signal intensity changes over time , the t2 * relaxation rate ( dr2 * ) , the baseline to be subtracted to the dr2 * curve , and nally the area under the tted dr2 * curve . 
the dr2 * was calculated by the equation dr2 ( cid : 3 ) ( cid : 4 ) ln st = s0 = te , where st is the signal intensity at time t , s0 is the pre - contrast signal intensity ( excluding the rst one or two images acquired during the reaching of the steady - state mr signal ) and te is the echo time . 
cbv maps were generated by the numerical integration of dr2 * for the rst - pass bolus through each pixel , and rcbv was calculated by rcbv = cbv [ lesion ] / cbv [ contralateral tissue ]  . 
the enhancing rois were divided into two groups : recurrent glioma , characterised by steady growth or marked enlargement of enhancement and mass effect , despite steroid therapy , on at least two follow - up examinations , and radiation injury , characterised by stable - appearing or regressing regions of enhancement on at least four follow - up examinations . 
measurements derived from the rst examination showing new contrastenhancing lesion ( s ) in the vicinity of the original treated radiol med ( 2014 ) 119 : 616624 tumours were used for the statistical analysis , whereas the following examinations were only used for recurrent glioma or radiation injury attribution . two experienced neuroradiologists identied in consensus the rois , and when in four cases they disagreed , a third neuroradiologist adjudicated . 
however , to reduce errors linked to the presence of distortion in echo - planar images and / or the non - optimal superimposition between images of various types , rois were manually resized and repositioned on the basis of anatomical references . 
the square root of cho / chon and the reciprocal of square root of ll / lln and cho / crn helped to improve the distribution shape . group differences ( recurrent glioma vs . radiation injury rois ) were evaluated by the independent - samples t test , using the levenes test for equality of variances and the bonferroni correction for multiple comparisons . 
with the leave - one - out method , discriminant analysis is performed times , once for each sample in the data set , several including all samples except one . 
the case that is left out is used for testing the classiers elaborated by the analysis . classication accuracy was dened as the ratio between the number of cases correctly classied and the total number of cases in the set . 
all examined parameters showed a large intraand inter - subject variability , with a large overlap between the two groups ( table 1 )  . stepwise discriminant analysis showed that the predictor set including cho / chon , adc and rcbv maximised the discrimination between recurrent glioma and radiation injury rois ( table 2 )  . 
the leave - one - out method , in fact , showed that 79.3 % of the cases were correctly reclassied when considering all 1h - mrsi ratios or just the normalized ratios ( predictor set , cho / crn ) , 86.2 % when considering 1h - mrsi ratios and adc ( predictor set , cho / crn and adc ) , 89.7 % when considering 1h - mrsi ratios and rcbv ( predictor set , cho / crn , cho / cr and rcbv ) , and 96.6 % when considering ratios , adc and rcbv ( predictor set , cho / chon , adc and rcbv ) ( table 2 )  . 
among the single parameters , rcbv showed the best classication accuracy ( 86.2 % ) , followed by adc ( 82.8 % ) and cho / crn ( 79.3 % ) ; naa / crn , ll / lln , naa / cr and cho / cr were not qualied for the analysis ( table 2 )  . discussion in the follow - up of treated high - grade gliomas , the correct classication of newly appearing enhancing lesions on conventional mri is often a challenge . 
both recurrent gliomas and radiation injury , in fact , can show indistinguishable features , such as contrast enhancement , mass effect and vasogenic oedema [ 1 , 2 ]  . 
1h - mrsi , dwi and pwi help to discriminate tumour recurrence from radiation injury [ 1 , 4 ] , but alone have a limited diagnostic accuracy [ 1 , 5 ]  . 
in fact , stepwise discriminant analysis with a leave - one - out method , including 3 - t 1hmrsi ratios , adc and rcbv , allowed us to achieve 96.6 % classication accuracy ( table 2 )  . the metabolic proles of radiation injury and tumour recurrence / progression have been extensively studied , but there is still no consensus about which spectroscopic parameter ( s ) and / or which threshold level ( s ) ensure the better discrimination accuracy [ 6 , 8 , 9 , 1628 ]  . 
nonnormalized ratios have been largely used and several studies have reported that recurrent tumours have higher cho / naa [ 6 , 8 , 1618 , 26 ] and cho / cr [ 6 , 8 , 1618 , 26 ] and lower naa / cr [ 1618 ] than radiation injury . 
taking into account the threshold values that maximised the discriminative power , the reported diagnostic accuracy of cho / naa and / or cho / cr ranged between 81 and 96.2 % [ 6 , 8 , 16 , 18 , 26 ] , and that of naa / cr reached 84 % only in 620 radiol med ( 2014 ) 119 : 616624 fig . 
1 tumour recurrence in a 54 - year - old man who underwent surgery followed by chemoradiation for a left temporal glioblastoma . t2 - weighted ( a ) and contrast - enhanced t1 - weighted ( b ) images , adc ( c ) and rcbv ( d ) maps , localising flair image ( e ) and proton mr spectra ( 14 ) ( f ) from selected rois , acquired 3 months after completion of radiotherapy . 
in our study , cho / naa and cho / cr were found to be higher and naa / cr lower in recurrent glioma than in radiation injury rois , but only cho / naa reached the signicance level ( table 1 )  . 
furthermore , discrimination analysis showed that cho / naa showed a diagnostic accuracy ( 62.1 % ) substantially lower than previously reported , while cho / cr and naa / cr did not enter into any of predictor sets ( table 2 )  . 
our results were in general agreement with those of other studies that reported no signicant differences for cho / naa [ 8 , 9 , 20 ] , cho / cr [ 8 , 9 , 16 , 19 , 24 ] and naa / cr [ 19 , 26 ]  . normalized ratios have been less widely used . nonetheless our results ( table 1 ) are in line with several studies showing that high cho is correlated with tumour recurrence / progression [ 20 , 22 , 23 , 27 ] , whereas low cr [ 21 , 27 ] and low naa [ 21 , 25 , 28 ] are more consistent with radiation injury . 
however , these authors performed the histopathologic analysis in 10 out of 25 patients . studies obtaining histopathologic conrmation in all patients reported good discriminative power for cho / chon [ 20 , 22 , 23 ] and cho / crn [ 19 , 20 ]  . 
cho / crn , in particular , allowed for the correct diagnosis in 16 out of 17 ( 94 % ) radiol med ( 2014 ) 119 : 616624 fig . 
2 radiation injury in a 57 - year - old woman who underwent surgery followed by chemoradiation for a glioblastoma in the left frontal and contrast - enhanced t1 - weighted ( b ) images , adc ( c ) and rcbv ( d ) maps , localising flair image ( e ) and proton mr spectra ( 14 ) ( f ) from selected rois , acquired 6 months after completion of radiotherapy . 
in fact , comparing diffusion features between radiation injury and recurrent tumour groups , some authors [ 7 , 8 , 10 , 29 , 30 ] measured signicantly higher adc values in the rst group , whereas others [ 31 ] found signicantly higher adc values in the second one and others still [ 9 , 32 ] did not nd any signicant differences in mean adc values . 
the high cellularity that generally characterises neoplasms contributes to lower adc in recurrent / progressed gliomas , while necrotic materials concur to higher adc in radiation injury [ 30 , 31 ]  . 
however , inammatory cell invasion , ischaemic cell swelling , gliosis , brosis , hyperviscosity and vascular changes are possible causes of low adc in radiation injury , while necrotic and / or cystic phenomena and vasogenic oedema can cause higher adc in recurrent tumour [ 7 , 31 ]  . 
in the present study , the adc values were higher in radiation injury than in recurrent glioma , but the difference was not signicant after bonferroni correction ( table 1 )  . 
the radiol med ( 2014 ) 119 : 616624 rois mean range mean range table 1 means , standard deviations and ranges of magnetic resonance ( mr ) parameters in the selected regions of interest ( rois ) no . 
in effect , as a consequence of increased metabolic activity and neoangiogenesis , gliomas tend to have higher rcbv values than radiation necrosis that mainly consists of ischaemia - related changes caused by occlusive vasculopathy . 
however , the presence of telangiectasias , aneurysms and vascular elongation in radiation necrosis , which might result in an increase of rcbv , and the radiation - induced micro - bleeding in recurrent tumour , which could cause a decrease of rcbv , might lead to a misclassication of suspicious lesions [ 35 , 36 ]  . 
however , in agreement with several studies [ 6 , 3537 ] , we found signicantly higher rcbv values in recurrent glioma than in radiation injury rois and the diagnostic accuracy we calculated ( 86.2 % ) was similar to that reported in the literature , ranging between 80 and 87.2 % [ 6 , 8 , 35 ]  . the extreme histopathological heterogeneity of gliomas [ 38 ] and radiation injury [ 39 ] , the frequent mixture of both ndings in the same biopsy specimen [ 19 , 20 , 35 ] , the signicant overlap of metabolic , diffusion and perfusion values between the radiation injury and recurrent glioma groups , as reported in most studies , and the differences in the methodological approaches and number of observations are possible explanations for the variability and discrepancy of the above reported results . considering that no single technique is completely reliable , some authors have combined the results acquired radiol med ( 2014 ) 119 : 616624 with the advanced mr techniques to better characterise newly appearing enhancing lesions [ 612 ]  . 
 [ 11 ] , combining information from adc and several 1hmrsi parameters , found that adc increased the odds of correct differentiation between pure tumour and pure necrosis , while the addition of this parameter did not provide further information beyond that of 1hmrsi ratios in distinguishing mixed tumour and necrosis from either pure tumour or pure necrosis . 
 [ 8 ] , combining 3 - t 1hmrsi , dwi and pwi information using a simple , multiparametric scoring system , improved the diagnostic accuracy from 84.6 % for cho / naa and cho / cr , 86.7 % for adc and 86.7 % for rcbv up to 93.3 % [ 8 ]  . 
 [ 6 ] evaluated and compared the diagnostic performances of 1h - mrs , dwi and pwi without combining data in a pattern recognition analysis [ 6 , 9 ]  . 
on the basis of previous studies combining 1h - mrsi [ 40 ] or 1h - mrsi , dwi and pwi [ 41 ] parameters in a discriminant function - based pattern recognition analysis improved the differentiation between tissues , we applied such approach to differentiate radiation injury from tumour recurrence . 
 [ 10 ] who used a similar approach , although they did not add pwi parameters to the analysis . in which we demonstrated that notable limitations to our study are the lack of histological conrmation and the small number of patients . although histopathological diagnosis should be desirable in all patients , it is not always practicable because of increased risk of morbidity and mortality [ 3 ]  . 
patients received ultrasound ( us ) - guided injection of 7 ml of naropin 0.75 % in t7 , t9 and t11 levels , below the costo - vertebral ligament , until we observed an anterior displacement of the parietal pleura . for the subcapsular lesions , a cervical right phrenic nerve block was associated . 
finally , we investigated statistical correlations between pain and lesions ( histological type , site , dimensions ) , and ablation time and technique ( microwave or radiofrequency ablation )  . results technical success was achieved in all patients . despite the correct anaesthetic diffusion during the ablation , c . 
citta` della salute e della scienza , san giovanni battista , turin , italy 10 patients ( 33.3 % ) reported medium / severe pain and intravenous sedation was required . 
we recommend performing a tpvb in the presence of the anaesthetist . keywords paravertebral block ( cid : 2 ) percutaneous thermal ablation ( cid : 2 ) liver tumours introduction coagulative necrosis , induced by the percutaneous ablation of liver tumours , can cause intense pain both during the procedure and in the following hours , particularly in presence of subcapsular nodules [ 1 ]  . conventional analgesia includes , in addition to local anaesthesia with hydrochloride lidocaine , intravenous infusion of remifentanil and midazolam [ 2 ] ; however , a signicant number of patients experience severe pain especially in the following 24 h . 
detailed anatomical knowledge is required [ 7 ] ; furthermore , we believe ultrasound ( us ) guidance can be useful , even though no reports about its effect are present in the literature . the purpose of this paper was to critically report and discuss the results of our preliminary experience with analgesia by means of a unilateral visceral somatic block in patients undergoing percutaneous thermal ablation of hepatic nodules . comorbidities hypertension diabetes arrhythmia obesity hcc nodules mts nodules total materials and methods patients between october 2011 and august 2012 , a total of 30 patients ( 24 males and 6 females aged between 47 and 85 years , mean age 67.5 years ) undergoing percutaneous ablation of 36 primary or secondary liver tumours by radiofrequency ( rfa , 24 nodules ) or microwave ( mwa , 12 nodules ) were given a right paravertebral block prior to the procedure . more precisely , 21 patients had hepatocellular carcinoma ( hcc ) , whereas in 9 cases lesions from metastatic colorectal carcinoma ( mts ) were present . 
all hcc had developed on cirrhotic livers ( three hbv , seven hcv , four alcoholic , one hbv ? hcv and six cryptogenic )  . seventeen patients had a single neoplasia , while four patients had a bifocal cancer . 
lesions were distinguished into parenchymal , more than 10 mm away from the capsule surface and subcapsular ( tables 2 , 3 )  . procedure the day before the procedure all patients gave written informed consent for the anaesthesiological protocol . 
in the us suite , after cannulation of the radial vein , the vital parameters were monitored ( electrocardiogram , pulse oximetry and blood pressure )  . the patient was positioned with the back facing the two operators : a radiologist and an anaesthetist . 
3 the tip of the needle ( arrow ) reaches the paravertebral space ( head arrow ) uid ( csf ) conrmed that no vessels or dural sac had been damaged . 
if the patient reported an nrs score [ 2 , intravenous remifentanil and propofol was administered in the course of the procedure and a therapy with paracetamol ( 1 g every 8 h ) and tramadol ( 1 vial as required for the next 24 h ) was recommended . statistical analysis possible correlations between pain and thermal ablation were evaluated . 
in 10 / 30 cases ( 33.3 % ) , the patient reported burning pain ( nrs [ 2 ) , which required an increase in infusion speed of remifentanil ( from 0.03 up to a maximum of 0.08 c / kg / min ) in combination with administration of midazolam and acetaminophen ( 1 g every 8 h ) and tramadol ( 1 vial as needed every 5 h ) in the following 24 h . 
three patients ( 10 % ) reported a medium pain intensity ( nrs 36 ) , while seven patients ( 23.3 % ) experienced severe pain ( nrs 710 )  . pain irradiation was visceral , sometimes accompanied by nausea ( 5 / 10 ) , epigastric ( 1 / 10 ) and right shoulder pain ( 4 / 10 )  . 
there were no major complications ; subcutaneous haematoma . reported patient small during the study , considering the progressive optimisation of the technique , we obtained a reduction in time fig . 
in patients with subcapsular lesions , an additional right phrenic nerve block was performed ; with the patients head turned to the left , the cervical segment of the phrenic nerve was located next to the anterior scalene muscle under us guidance , and was anaesthetised with 3 cc of 2 % lidocaine . a skin landmark was placed for the insertion of the thermal ablation needle ; at that level , local anaesthesia with 10 ml of carbocaine was performed . 
an expandable ( with curved , deployable tines ranging from 3 to 5 cm ) needle electrode ( med italia , medolla , italy ) was used to perform , for each lesion , two successive cycles between 80 and 190 w , for a total duration of 2045 min , reaching a temperature of 105 ( cid : 3 ) c . as for the microwave technique ( mw ) ( covidien , dublin , ireland and hs amica , aprilia , latina , italy ) , several cycles were performed : power varied between 45 and 80 w for 1020 min , reaching an intratumoral temperature of 180 ( cid : 3 ) c . hypotension , dened as a decrease in systolic blood pressure [ 30 % from baseline , was treated with intravenous uid infusion . 
it may be noted , however , that lesion histology and number are the variables most closely related to the onset of pain . discussion only two experiences are reported in literature on the use of tpvb during hepatic ablation procedures : ning et al . 
in 2011 [ 7 ] , who prospectively evaluated 20 patients with primary and secondary liver lesions treated with radiofrequency , and a case report published by culp et al . 
5 a , b relationship between pain and technique group a : nrs < or = 2 group b : nrs > 2 13 patients 6 patients 7 patients 4 patients nrs , numerical rating scale ; rfa , radiofrequency ablation ; mwa , microwave ablation . 
in particular , a vasovagal reaction can be related to an accidental migration of the anaesthetic into the epidural space : therefore , we believe that the use of us can be very useful for identifying the paravertebral space , guiding for percutaneous puncture and controlling for the distribution of the anaesthetic . 
in fact , in our experience we have seen accidental epidural migration of the drug , which can cause anaesthesia and motor decit in the lower limbs in addition to a vasovagal reaction . for the evaluation of results , we adopted the same rating scale as used by ning ( nrs ) and established a precise cutoff value ( nrs 2 ) to evaluate the effectiveness of analgesia , considering , with this very restrictive criterion , values above this limit as a treatment failure . 
moreover , the comparison of results is complicated by the fact that half of the patients treated in the chinese experience ( 10 / 20 ) was sedated with propofol during the procedure . 
ning also reported using a multiple injection technique , as done in other experiences reported in the literature about vertebral blocks performed for other reasons [ 15 , 16 ] : ning emphasises the importance of this technique in pain control , suggesting that it may also be responsible for the high rate ( 35 % ) of contralateral blocks in his experience , much higher than the previously reported rates of 20 [ 15 ] and 1.1 % [ 16 ]  . in our experience , complete technical success is based on the us evaluation : in all cases , the correct spread of the anaesthetic with pleural detachment was always demonstrated . 
from our point of view , the most likely hypothesis is that the diffuse visceral pain reported by some patients is due to the stimulation of left sympathetic bres and vagal bres ; the liver presents in fact a dual innervation : both orthosympathetic ( from the seventh to tenth thoracic segment of the spinal cord , which reaches the liver through the splanchnic nerves and the celiac plexus ) and parasympathetic [ 17 ]  . 
this could be a limit of the unilateral vertebral block , even if the high rate of contralateral unexpected block reported by ning represents an interesting matter . unlike ning , we tried to correlate the pain sensation to the different characteristics of the patients : analysis of the data showed no statistically signicant relationship between the variables considered ( procedure duration , technique , location , number and histology of the lesions ) and pain onset . 
the most signicant relationship , however , was between lesion number and histology : considering these results , we can hypothesise that patients with multiple metastases are less responsive to the vertebral block and consequently good candidates for alternative forms of analgesia or additional therapies . in view of the absence of factors that can unequivocally be related to the ineffectiveness of the treatment , we hope to develop as soon as possible a block efcacy test to be used before the ablation procedure . 556 radiol med ( 2014 ) 119 : 549557 fig . 
 however , we believe that our study , designed and conducted in collaboration with the anaesthetists of our interventional radiology unit , conrms the results of nings experience , highlighting the versatility , potentiality and advantages of paravertebral block , during algogenic treatments such as percutaneous hepatic ablation . 
this is a pilot study based on respect for the desires of each patient , who were adequately informed of the benets , possible ineffectiveness and complications of the paravertebral block , assuring intravenous analgesia if needed . these results have led us to design a prospective randomised two - arm study ( vertebral block vs intravenous analgesia ) , for which we have already requested the approval of the hospital ethics committee . 
in fact , we believe that the paravertebral block technique could be extended to other interventional radiology procedures , and especially to liver and biliary procedures such as percutaneous biliary drainage , as already reported in the literature [ 18 , 19 ] , portal embolisation , intrahepatic portosystemic shunt . transjugular theoretically , this technique could be managed independently by the radiologist because naropin is a common anaesthetic that does not require the presence of the anaesthetist for its management . 
however , our long and effective collaboration with anaesthetists suggests that a multidisciplinary management is essential , because of the possible need for intravenous analgesia . conclusions the thoracic paravertebral block is a well - tolerated and safe technique for the anaesthesia of patients undergoing percutaneous thermal ablation of malignant liver tumours . 
in particular , we considered the rate of second treatment with interventional technique or conservative or radical surgery , the incidence of postprocedural complications , and the absorbed radiation dose . results immediate technical success , dened as the cessation of active bleeding , was achieved in all cases . 
at the 12 - month follow - up after embolisation , 22 / 49 conservatively treated patients were found to be pregnant and successfully completed their pregnancy . conclusions selective uterine artery embolisation allows for safe and complete control of haemorrhage in patients with obstetric disease , with a very low incidence of complications and preservation of fertility . keywords obstetric haemorrhages ( cid : 2 ) selective embolization ( cid : 2 ) conservative management ( cid : 2 ) postpartum haemorrhage ( cid : 2 ) ectopic pregnancy introduction obstetric haemorrhage has a strong clinical impact because it constitutes a major risk for the health of the woman and the foetus and for preserving the patients fertility [ 1 ]  . the most common causes of haemorrhaging are postpartum haemorrhage ( pph ) [ 2 ] , congenital or acquired arteriovenous malformation ( the latter usually related to uterine curettage or removal of intrauterine devices ) [ 3 ] , instrumental delivery [ 4 ] , or complications in the treatment of ectopic pregnancy [ 5 ]  . 
in obstetrics , pph is the most frequent cause of admissions to intensive care and is associated with a higher mortality and morbidity rate than other types of haemorrhage [ 6 ]  . in recent years , transcatheter or percutaneous interventional radiology techniques have been applied to different pathological conditions , including disorders of the female pelvis and obstetric and gynaecological pathology [ 7 , 8 ]  . 
in table 1 summary of main clinical data and embolisation results embolisation technique sufcient haemostasis effective dose ( e ) uterine salvage complications pregnancies after 12 months 22 yes 4.3 msv none 10 yes radiol med ( 2014 ) 119 : 607615 diagnosis 22 cervical pregnancy fixed angiography 41 pph 38 yes 12 lsv 27 yes none 11 yes mobile angiography oec 32 pva 14 hysterectomies selective 16 pva 5 ibc 1 gelfoam selective 6 ibc 2 gelfoam 1 pva ? coils 3 no ( a second procedure was needed ) pph postpartum haemorrhage , pva polyvinyl alcohol , ibc isobutyl cyanoacrylate particular , transcatheter embolisation was rst used after bilateral ligation of the hypogastric artery [ 9 ] for the control of severe obstetric haemorrhage . 
this procedure is currently considered the rst choice treatment for controlling potentially fatal bleeding , with the aim of avoiding hysterectomy and preserving the fertility of these patients [ 10 ]  . according to some case series [ 11 ] , when used immediately after bleeding onset , embolisation has an efcacy varying between 85 and 95 % . 
of the 1 , 256 patients treated with interventional procedures at our establishment during that period , 104 were treated for a pathology shown to be at high risk of blood loss . 
the transvaginal approach was preferred in patients with abnormal insertion of the placenta and with placenta praevia . in cases of placental anomaly [ 15 ] , either suspected or conrmed on us analysis ( 22 / 63 ) , we proceeded with integration with mr imaging to obtain a fuller characterisation of the placenta and to permit correct planning of the procedure to avoid fatal haemorrhage . mr imaging was carried out with a 1.5 tesla scanner ( eclipse , pickermarconi , philips , eindhoven , netherlands )  . 
t2 - weighted fast spin - echo axial images were also acquired with suppression of fat tissue and t1 - weighted signals . anaesthesiaresuscitaiton protocol the anaesthesiaresuscitation protocol provided for a careful anaesthesiological evaluation with history taking , physical examination and evaluation of comorbidities and standard preoperative tests including haemochrome , coagulation prole [ prothrombin time ( pt ) , partial thromboplastin time / international normalised ratio ( ptt / inr ) , antithrombin iii ( atiii ) ] dimer and brinogen , glycaemia , urea , creatinine , total and fractional bilirubin , transaminase , lactate dehydrogenase ( ldh ) , creatine phosphokinase ( cpk ) , total protein , albumin , electrolytaemia , urinalysis , blood group and blood type screening . 
this phase was completed with the request of at least 4 units of concentrated erythrocytes of cross - matched blood for the operation and provision of a bed in postoperative intensive the interventional care for procedure . intensive monitoring after the intervention was always performed with local anaesthesia , whereas before the caesarean section balanced anaesthesia was introduced using drugs such as remifentanil in continuous infusion ( 0.050.25 mcg / kg / min ) , propofol 45 mg / kg on induction , cisatracurium 0.2 mg / kg and mixtures of anaesthetic gases ( o2 and sevourane )  . intervention protocol arteriography and subsequent superselective uterine artery embolisation were performed both as elective and emergent procedures , in the operating theatre with a mobile angiograph ( oec 9800 plus , general electric company , milan , italy ) , by an expert interventional radiologist on iliac 24 - h duty . 
selective angiography of the internal arteries and superselective angiography of the uterine arteries were always done with femoral access , generally on the right side . embolisation was achieved with a 5 f cobra catheter ( william cook europe , bjverskov , denmark ) with subsequent use of coaxial microcatheters ( progreat , terumo , tokyo , japan )  . 
vessel occlusion was obtained by injecting 700900 l polyvinyl alcohol ( pva ) ( contour se , boston scientic , natick , ma ) ( 48 / 63 cases ) or reabsorbable particles ( spongel , yamanouchi , tokyo , japan ) ( 3 / 63 cases ) to exclude the ow of blood , as shown by periprocedural angiographic imaging . 
in only one case was pva used in combination with metal coils to occlude the blood vessels , whereas in 11 cases , acrylic glue ( isobutyl cyanoacrylate , ibc ) was used ( in ve cases of cervical pregnancy and in six of re - operation for pph after hysterectomy ) ( table 1 )  . where pva was used , the choice of embolising material was dictated by the clear hypervascularity seen at preoperative angiography , which permitted a durable but not permanent treatment . 
in e , f selective catheterisation of the right uterine artery and its embolisation with ibc results superselective embolisation of the uterine arteries was chosen in all cases with complete exclusion of blood ow from the lesion . 
in particular , there were three cases of pph previously treated with pva which required re - operation ; in two of these patients also the cervicalvaginal branches ( pva ) were embolised and in one case of massive haemorrhage also the hypogastric artery ( spongel )  . 
finally , in 14 cases treated for massive pph , it was impossible to perform conservative treatment and hysterectomy was necessary to control the haemorrhage and achieve haemodynamic stability ( table 1 )  . the entire interventional procedure was conducted while limiting as much as possible the dose of ionising 611 radiol med ( 2014 ) 119 : 607615 fig . 
2 case of placenta praevia in a 34 - year - old woman treated with uterine artery embolisation with polyvinyl alcohol ( pva )  . in a , b the longitudinal and coronal t2 - weighted magnetic resonance ( mr ) images show the abnormal placentation without signicant signs of percretisin c , d selective catheterisation of the left uterine artery and its embolisation with pva . 
in e , f selective catheterisation of the right uterine artery and its embolisation with pva radiation absorbed by the patient and particularly by the uterus , with the aim of avoiding iatrogenic damage that could have compromised the fertility and thus the quality of life of these patients . 
after they returned to the obstetrics unit for the following 2448 h . this , at clinical - imaging follow - up at 1 and 6 months , no adverse reactions correlated to the embolisation procedure were observed . 
in g , h , the second treatment performed with catheterisation of the left hypogastric artery ( early and late time point , respectively ) : no signs of haemorrhage were shown . 
in l embolisation with coils radiol med ( 2014 ) 119 : 607615 22 / 49 ( 44.9 % ) patients treated with superselective embolisation of the uterine arteries and preservation of the uterus were found to be pregnant and carried their pregnancy to term ( table 1 )  . 
in the remaining patients , ovulation proceeded regularly from the ovaries after embolisation procedure , as shown by routine ultrasound and from case - history records . discussion in this study , we retrospectively reviewed the angiographic examinations performed from 2009 to 2010 on 63 patients affected by obstetric conditions with a high risk of bleeding and treated with an interventional approach as a rst - line strategy . 
using this approach , immediate technical success was obtained in all cases , with total cessation of the blood ow , as shown by periprocedural angiography , and limitation of the dose of ionising radiation to which the patients were exposed . these results are consistent with those reported in the literature , although therapeutic success in treating the specic causes of obstetric haemorrhaging has often been evaluated on small patient series . 
 [ 5 ] , for example , published the largest study on the conservative treatment of cervical ectopic pregnancy , with only four cases successfully treated using arterial embolisation of branches of the uterine and transverse cervical arteries using gelfoain this study , the 22 cervical ectopic pregnancies were treated with immediate technical success using embolisation with pva , gelfoam or ibc , with no need for a second embolisation for haemostatic control and without encountering any complications at clinicalimaging follow - up at 1 , 6 , and 12 months . recently , delotte et al . 
other authors [ 14 ] , conversely , have compared the efcacy of preventive embolisation treatment with the classic posthaemorrhagic treatment , nding equivalent success rates for the two groups , but with a signicant reduction in the time for embolisation and in the blood loss for the group receiving preventive treatment . 
in our series , an overall success rate of 100 % for the manoeuvre for the prevention of haemorrhage was found in 41 patients treated for pph , with an immediate technical success rate solely for arterial embolisation of 92.68 % ( 38 / 41 )  . 
it is also necessary to consider the different causes of pph [ 17 ] that may also benet , with varying success rates , from superselective embolisation of the uterine arteries . 
in particular , even if the overall success rate for interventional treatment of pph is between 85 and 95 % [ 11 ] , this percentage diminishes in those cases where the pph is due to placental anomalies , with a range that varies from 20 to 100 % [ 18 ]  . at this time , it is not yet clear what determines this wide range of results ; nevertheless , it may be correlated to the time and the intensity of the forces used to remove the placenta , as well as to patients condition at the time of the intervention . 
in this regard , it is interesting to note that in the 14 cases in which hysterectomy was necessary , the pph in 13 of these was due to placenta previa percreta . 
in patients with placental anomalies , where magnetic resonance ( mr ) imaging led to a suspicion of percretism [ 19 , 20 ] , later conrmed at surgery , hysterectomy was done immediately , without waiting for the afterbirth , to limit further possible sources of bleeding . in three cases of pph , positioning of an intrauterine balloon was combined with the embolisation , and in one of these cases the technique of compressive uterine suture , using the method of b - lynch [ 21 ] was used to render the haemostasis even more efcient . 
in one case of uncontrollable pph after spontaneous birth with episiotomy , embolisation of the uterine arteries and the cervicalvaginal branches with pva was performed after application of vaginal tampons and abdominal packing . 
upon removal of these after 48 h , an aorto - iliac angiogram was obtained to verify the loss of further vascular branches . regarding a second embolisation or subsequent surgery for the control of haemostasis , in 4.76 % of cases ( 3 / 63 ) , the embolisation of several vascular branches had to be combined with the primary embolisation treatment , and in 22.22 % ( 14 / 63 ) , surgical treatment with hysterectomy was required . 
these data are consistent with the literature [ 16 , 22 , 23 ] , in which , especially for phh control and resolution of the underlying pathology , hysterectomy must be combined with arterial embolisation . 
the different results of the embolisation treatment in our series may be due to the percentage of placental anomalies included in the pph , which , as analysed previously , respond signicantly less well to interventional treatment , often requiring the integration of a second treatment with hysterectomy . 
retrothe effective dose of spective analysis of radiation delivered to patients treated with the interventional approach has shown slightly higher doses for patients undergoing embolisation for ectopic pregnancy compared to those treated for pph , obtaining in both cases an effective haemostatic control with limited exposure to ionising radiation . 614 radiol med ( 2014 ) 119 : 607615 early and late complications linked to the interventional procedure include fever , vascular perforations , ischaemia of the lower limbs , and necrosis of the uterus or of the walls of the bladder or rectuin our study , at 1and 6 - month follow - up , no complications related to the interventional procedure were observed . 
this information is in keeping with the low complication rate ( about 3 % ) reported in some other studies [ 22 ] , and correlates with the nature of the embolising agent chosen [ 24 ]  . with respect to hysterectomy , considered the standard treatment the control of both pph and obstetric haemorrhages in general , embolisation has proved efcient in guaranteeing and preserving the fertility of the patient treated with superselective embolisation of the uterine arteries and preservation of the uterus [ 2527 ]  . 
some studies [ 10 ] , for example , have reported preservation of the uterus in 95 % of cases of pph treated with embolisation and the return of menstrual ow in all patients , with a pregnancy rate of 20 % in these patients . 
the increased pregnancy rate in our study compared with the current literature [ 10 , 25 , 28 ] can presumably be ascribed to the greater safety of the preventive treatment compared to the standard approach that results in reduced operating times and a lower blood loss [ 14 ] , as well as reduced length of stay in postoperative intensive care ( about 2448 h )  . 
only one case of amenorrhoea due to hypothalamic hypogonadism after embolisation with gelfoam was reported in the literature [ 29 ] , which may be resolved with the aid of hormone stimulation . even though the small series is a limitation of our study , easy access to dedicated instruments in the operating theatre , team work and professional expertise accounted for the high rate of immediate success found in our study . 
in the assessment of long - term outcomes following the interventional approach to pathologies at high risk of bleeding , such as ectopic pregnancy and pph , conicting results continue to be reported with regard the recurrence rate after subsequent pregnancies [ 10 , 28 , 30 ]  . 
this relatively new question is probably the product of the high success rate of the interventional procedure in these pathologies which allows the conservative treatment of patients who would otherwise be subjected to hysterectomy . 
however , the lack , for clinical reasons , of a real control group treated only with hysterectomy and followed in parallel to the embolising treatment , certainly represents the main limitation of this study . 
a longer follow - up period would perhaps have permitted clarication of this aspect and will certainly be the subject of further studies . future prospects for study are thus analysis of this treatment on a greater number of patients and over a longer follow - up period . 
furthermore , given the excellent safety and effectiveness demonstrated by this type of treatment and the low exposure to ionising radiation during the interventional procedure , a pilot study will soon be begun on the possibility of performing the embolisation in the immediate ante - partum period with a view to further reducing the risks of massive haemorrhaging for this type of patient . conclusions the percutaneous method in the prevention / treatment of obstetric haemorrhage is currently an example of the integration of imaging and clinical methods , and it proves extremely useful in reducing the rate , although still high , of mortality linked to postpartum haemorrhage . 
guglielmi department of radiology , university of foggia , viale luigi pinto , 1 , 71100 foggia , italy mechanical properties of achilles tendon in children with clubfoot . keywords real - time elastosonography ( rte ) ( cid : 2 ) clubfoot ( cid : 2 ) achilles tendons introduction congenital clubfoot is a common disorder present at birth that affects the musculoskeletal system with an overall incidence of 1 : 1000 newborns . 
this congenital defect includes four main types of foot alteration : equinus foot , hindfoot varus , forefoot adductus and cavus [ 1 ]  . congenital several theories have been suggested in order to explain clubfoot , idiopathic the pathogenesis of including genetic factors and vascular deciencies . 
abnormal development of leg muscles , genetic defects in growth of the connective tissue , abnormal tendon insertions , and tight deltoid ligaments , have all been described [ 36 ] as possible aetiologies . idiopathic clubfeet usually show resistance to manipulation due to deformity of the affected feet . 
this pathology has been classied into two systems , the dimeglio and the pirani classications , both correlating the severity of this condition with physical ndings [ 7 ]  . 
currently , the ponseti method is the preferred nonsurgical technique used for treatment , and it consists in a deep stretching of the peronei and foot dorsi - exor muscles , in order to normalise foot position and to provide correct posture [ 8 ]  . to the best of our knowledge , there are no studies investigating the properties of mechanical stiffness of achilles tendon in patients affected by unilateral idiopathic 602 radiol med ( 2014 ) 119 : 601606 clubfoot . 
it was observed that unilateral clubfoot might be associated with a lower calf circumference , and this may result in quantitative differences of the muscular masses , when two series of patients with unilateral clubfoot are compared [ 9 ]  . 
moreover , it has been reported by several authors , such as ippolito and ponseti , that a greater presence of brous tissue can be observed in the muscles , in the fascia , in the ligaments and in the tendon sheaths [ 10 ] : this may lead to an increased stiffness of all the involved anatomical structures . recently , real - time elastosonography ( rte ) has been proposed as a technique able to assess the differences in stiffness between diverse tissues using ultrasound ( us )  . 
it has also been suggested for the evaluation of tissue distortion , as well as of muscle and tendon stiffness [ 11 ]  . the aim of our study was to assess the usefulness of rte of the achilles tendon in the clinical evaluation of a cohort of children affected by unilateral clubfoot , not surgically treated . materials and methods study population after the approval from the ethics committee of our institution , 20 young patients ( 8 males and 12 females ) affected by unilateral idiopathic clubfoot were consecutively examined . 
written informed consent was obtained from the parents of all children , in accordance with the declaration of helsinki . the clinical evaluation for all enrolled patients was performed by a single orthopaedic surgeon with 35 years of clinical experience at our institution . 
children who were found to be affected by any systemic condition , any connective tissue disorder , any metabolic and / or endocrine disease , or patients with a history of tendon injury and surgery were excluded from the study group . 
the entire study group was then divided into two subgroups , according to age : the rst group ( group 1 ) included 13 children aged between 0 and 18 months , while the second group ( group 2 ) included 7 children aged from 18 to 60 months . 
b - mode ultrasound was performed along the entire length of the achilles tendon , bilaterally , from the distal enthesis to the proximal myotendinous junction , dening its echotexture and searching for sonographic signs of previous traumatic injury or signs of tendon degeneration . 
the total amount of deformation used to compute the strain of elastogram is represented by the sum of the inherent or physiologic patient - motion and the external compression form the probe . the probe is held in place manually , while the patient is kept at rest . 
a range of colours shows the relative hardness and softness of the roi , conventionally varying from blue to red . first , tendons from the affected clubfoot were evaluated , and then measurements were obtained from the contralateral healthy tendons . 
overall examination time was approximately 14 min for each patient ( 7 min per side )  . the colour - coded images were analysed on a personal computer using the qlab ( developed by philips medical systems ) , which allows the operator to select a 30 - frame images / cine - loop and to position manually two circular rois , with the same area of 4 mm , identied in our study as roi 1 and roi 2 . roi 2 was used as a reference standard and it was positioned on the bone tissue . 
analysis was repeated in quadruplets ( one for each examination ) and nal data were expressed as an average value of the different results . data analysis the students t test and standard deviation ( sd ) were used to assess variation of continuous parameters in order to obtain an average value of the different real - time measurements . 
2 a conventional axial b - mode ultrasound scan and superimposed , b sonoelastogram of the achilles tendon , at the distal third , in clubfoot showing a diffuse hyperechoic pattern , in grey scale , associated with low elasticity of the structure , evaluated by sonoelastography . 
in our study , a sonoelastosonography evaluation was performed to obtain a tensile test which shown a condition of chronic tendinopathy involving the entire achilles tendon . a chronic state of tendinopathy might lead to softening and weakening of collagenic and elastin structures increasing the risk of tendon rupture [ 15 ]  . 
although no signs of achillodynia were present , after rte a decreased elasticity of achilles tendons was observed in clubfoot . tendons while b - mode morphological ultrasound provided structural information , sonoelastography showed a light red colour code along the structure of achilles tendon with reduced values of elasticity comparing to the normal internal control [ 16 ]  . ( healthy ) contralateral therefore us sonoelastography is considered to be a helpful technique for detection and characterisation of achilles tendinopathy for its high sensitivity and specicity in the detection of intratendon alterations [ 17 ]  . 
main rte alterations were observed on the distal portion of the tendon , which was represented by a weaker structure , both at rest and on stress , characterised by decreased values of elasticity and a green colour [ 18 ]  . 
4 a longitudinal b - mode ultrasound scan and superimposed , b sonoelastogram of the achilles tendon , at clubfoot showing a diffuse hyperechoic pattern highlighted in grey scale , associated with low elasticity of the structure , evaluated by sonoelastography . 
the same ratio in group 2 ( patients aged 1860 months patients ) was statistically different , but a lower discrepancy could be observed between the values from the two different groups ( table 1 )  . 
in longitudinal scans , homogenous , hyperechoic , linear continuous shadows with regular margins appeared , in the achilles tendons ; while , in transverse scans , the achilles tendons were elliptical , homogenous and echogenic in appearance . idiopathic clubfoot is one of the most common musculoskeletal congenital disorders with several deformities affecting bone , ligaments and tendons [ 12 , 13 ]  . 
a nonsurgical treatment technique , named the ponseti method , is the currently preferred treatment method and is usually discussion radiol med ( 2014 ) 119 : 601606 to standardise the evaluation of the tendon itself . 
in fact , during the growth of the tendons , these structures undergo morphological changes , such as an increased vascularisation occurring on the distal and proximal thirds and an associated loss of vascularisation in the middle third [ 19 ]  . moreover , de zordo et al . 
 [ 17 ] have observed a distinct softening of symptomatic achilles tendons , occurring on the distal and middle third more frequently than the proximal third of the tendon . a strongly heterogeneous pattern was found , and this result is probably associated with the different mechanical properties of the various tissue components within normal and pathologic tendons [ 18 ]  . 
moreover , we were able to assess both resting and stress conditions of the tendon in real time , using sonoelastography . in our present study , a strong correlation was found between the patients age and rte appearance , without any inuence of the patients sex . one of the main limitations of the study is that intraand inter - observer agreement of rte is still an open question , which has been little investigated in the medical literature . however , all the operators had the same learning curve with regard to rte examination , each with 32 months of experience . 
therefore , we decided to perform the statistical analysis on the mean values of elastic ratios obtained in the different subgroups of patients by three independent operators with the same level of expertise in rte . conclusion rte is a feasible and simple technique , which allows the evaluation of mechanical properties of the achilles tendons in clubfoot , including homogeneous or relatively homogeneous patterns . 
one of the main limitations of this study was a lack of correlation of the us data with the histopathological ndings in achilles tendons from the patients affected by clubfoot . 
another limitation was the overall small cohort of children enrolled , as well as the wide range included in group 2 , ( relatively too small a subgroup for such a broad range )  . 
all examinations were acquired after contrast - agent administration in a craniocaudal direction from the lung apex to base during a single inspiratory breath - hold , with standardised parameters . 
each lesion was scanned with 1315 slices that could be repeated whenever necessary to document the needle track and for lesion centring , by positioning a metallic marker perpendicular to the centring light to indicate the point of needle access . 
berti department of diagnostic sciences , uoc of pathology , san carlo borromeo hospital , via pio ii 3 , 20153 milan , italy results age was found to be a factor inuencing the complications : pneumothorax in young subjects ( 31 % ) and parenchymal haemorrhage in the elderly ( 30 % ) , with cnb but not with fnab . 
we had more complications with the right lung : 50 % of pneumothorax cases in the upper lobe with cnb and 40 % of cases of haemorrhage in the lower lobe with fnab . 
when percutaneous biopsy is used to establish the diagnostic and therapeutic workup of a lung lesion , one must carefully evaluate the costbenet ratio as well as the most frequent complicationspneumothorax and parenchymal haemorrhage [ 5 , 9 , 11 ]  . 
although both complications usually resolve spontaneously , the occurrence of pneumothorax during the procedure may lead to an inconclusive result and , in a variable percentage of cases , worsening pneumothorax may require placement of a chest drain , whereas parenchymal haemorrhage may necessitate hospitalisation [ 12 ]  . the rst aim of this study was to assess the type and incidence of complications arising in ct - guided lung biopsies performed with ne - needle aspiration ( fnab ) or cutting needle ( cnb ) , by analysing the different variables related to the patient ( age ) , the lesion ( dimension , nature , side ) and the procedure ( number of passes , access and needle calibre )  . 
1 lung biopsy with an 18 - g trucut needle of a lesion of the dorsal segment of the right upper lobe , performed with a single pass with posterior access fig . 
2 fine - needle aspiration biopsy ( fnab ) with a 22 - g needle of a 1.2 - cm nodule in the dorsal segment of right lung lower lobe with a single pass and posterior access materials and methods this retrospective study was performed by analysing a series of 121 patients , 15.3 % of them with known oncological disease , who underwent ct - guided lung biopsy using cnb or fnab between 01 - 01 - 2010 and 31 - 12 - 2011 . a total of 122 biopsies were performed in 76 men and 45 574 radiol med ( 2014 ) 119 : 572594 fig . 
any platelet antiaggregant and anticoagulant treatment was suspended a few days prior to the procedure and subsequently resumed by the patient , in accordance with the haematologists indications . all patients had previously undergone a ct or highresolution ct ( hrct ) examination which identied and dened the lesion . 
all the biopsies were carried out as inpatient or day - case procedures . radiol med ( 2014 ) 119 : 572594 all patients received verbal explanations about biopsy procedure and its possible complications , and they subsequently read and signed the written informed consent form , which included consent for using their anonymised clinical data for scientic purposes . the possible complications of a ct - guided lung biopsy are pneumothorax , haemorrhage , haemothorax , haemoptysis , rarely seeding of neoplastic cells along needle path , cardiac effusion , and pulmonary infections ( pneumonia , empyema ) , as well as risks attributable to the administration of the drugs used during the procedure . 
we recorded as pneumothorax any amount of air appearing between the lung and pleura . expiratory chest radiography was performed in all patients 46 h after the procedure to assess the appearance or the growth of a pneumothorax previously detected on postprocedure ct . 
if it became stable or smaller , the patient was discharged , whereas if it increased the surgeons advice was sought for possible placement of a chest drain the event of complications arising in patients fig . 
4 cnb age cnb age . hemoptysis suffusion suffusion + pnx ( 0% ) ( 50% ) 6 ( 30% ) 2 ( 10% ) ( 10% ) young emottisi ( 0% ) ( 50% ) 6 ( 30% ) 2 ( 10% ) ( 10% ) giovane ( 9% ) ( 35% ) ( 17% ) ( 30% ) ( 9% ) elderly ( 9% ) ( 35% ) ( 17% ) ( 30% ) ( 9% ) vecchio hemoptysis suffusion suffusion + pnx 100% 100% young 100% 100% elderly giovane vecchio cnb et . soffusione emorragica soffusione emorragica e pnx emottisi soffusione emorragica soffusione emorragica e pnx 100% 100% 576 radiol med ( 2014 ) 119 : 572594 who underwent the biopsy as a day - case procedure , the need for hospitalisation was assessed in relation to the clinical symptoms and signs . biopsy protocol the examinations were performed on a 16 - slice lightspeed ct system ( ge medical system , milwaukee wi , usa ) and on a 128 - slice somatom denition as ? ct system ( siemens healthcare , erlangen , germany )  . all examinations were acquired in a craniocaudal direction from the lung apex to base , during a single inspiratory breath - hold with the following standardised parameters : thickness 2.5 mm , collimation 10 mm , eld of view 320360 mm , pitch 1.75 , 120 kv ; automatic tube current modulation ( ma ) ; standard reconstruction lter ; lung window . 
patients received iodinated contrast agents : ioversolo 350 ( covidien , italy ) and iopromide 370 ( bayer schering pharma , germany )  . according to lesion location , the ideal needle trajectory from the skin to the lesion was established . 
lesion centring was performed on the axial image of the image stack , in which the lesion presents the greatest extension and needle access is less hampered by the presence of anatomical structures . 
on the chosen image , a metallic marker is placed perpendicular to the centring light , which indicates the point that will be used for needle access . the needles used were chibell ( biopsybell , modena , for fnab italy ) with a calibre of 20 and 22 g , procedures , and biomol ( hp service hospital , latina , italy ) with a calibre of 18 , 20 and 21 g for cnb procedures . 
during the cnb procedures , no pathologist was present in the room , whereas during the fnab procedures , a pathologist was on site to extemporarily evaluate the adequacy of the sample . 
sample adequacy was assessed in real time alternately by two equally experienced pathologists , who subsequently performed also the nal microscope slide . reading of we used test tubes with and without xative , skin disinfectant , bevelled glass slides , cover slips , racks , xatives , haematoxylineosin staining scale , papanicolaou stain , and a diagnostic room set up with a hood and an optical microscope . in relation to the pathological report , the result of each procedure was classied as diagnostic or nondiagnostic . samples were dened nondiagnostic in the event of insufcient , cell - free , or strongly haematic material . diagnostic samples were grouped by histological type . the ct images were assessed for the following parameters : needle access ( anterior , posterior , lateral ) , lesion site ( upper or lower right lobe , middle lobe , upper or lower left lobe ) , lesion size ( large if [ 3.5 cm or small if b3.5 cm ) , patients age [ \65 years ( young ) and c65 years ( elderly ) ] , needle gauge , number of needle passes , and lesion histology ; all variables were correlated to the type and incidence of complications recorded with the two biopsy methods . 
5 fnab with an 18 - g needle of a lesion of the right upper lung lobe with single pass and lateral access ( a ) ; at the end of the procedure , a small parenchymal detachment , and circumscribed haemorrhage along the needle track ( b ) radiol med ( 2014 ) 119 : 572594 statistical analysis results complications the baseline characteristics of the study population were expressed as mean standard deviation for continuous variables , and as percentages for categorical variables . correlation between the variables considered and the presence of ( pneumothorax , parenchymal haemorrhage , haemoptysis ) was calculated using the chisquare test . 
in the graphs on the left , each histogram represents the number of observations classied according to the labels / classes placed under the columns , with an indication , within each label / class , of the type of complication ( the various colours of the histogram )  . 
no case of parenchymal haemorrhage necessitated either hospitalisation ( of the day cases ) or additional treatments ( of the inpatients )  . table 3 fine - needle aspiration biopsy vs . 
6 fnab : age fnab ne - needle aspiration biopsy , cnb core - needle biopsy 578 radiol med ( 2014 ) 119 : 572594 the patients were analysed in relation to age and type of biopsy . 
haemoptysis occurred in 9 % of elderly patients , either immediately or a few hours after the end of the procedure ; no case of haemoptysis was recorded among the young patients . 
7 cnb : lesion size cnb lesion size . hemoptysis suffusion suffusion + pnx hemoptysis suffusion suffusion + pnx 100% ( 6% ) ( 44% ) ( 17% ) ( 28% ) ( 6% ) large ( 6% ) ( 44% ) ( 17% ) ( 28% ) ( 6% ) grande ( 7% ) ( 33% ) ( 27% ) ( 20% ) ( 13% ) small ( 7% ) ( 33% ) ( 27% ) ( 20% ) ( 13% ) piccolo 100% large 100% 100% small 100% grande piccolo cnb dimensione nodulo . emottisi soffusione emorragica soffusione emorragica e pnx emottisi soffusione emorragica soffusione emorragica e pnx 100% radiol med ( 2014 ) 119 : 572594 fig . 
10 fnab : needle approach fnab needle approach . radiol med ( 2014 ) 119 : 572594 suffusion suffusion + pnx 100% 100% 100% suffusion suffusion + pnx ( 50% ) ( 21% ) ( 29% ) ( 0% ) rear ( 50% ) ( 21% ) ( 29% ) ( 0% ) ( 56% ) ( 22% ) ( 11% ) ( 11% ) ( 80% ) ( 20% ) ( 0% ) ( 0% ) anterior lateral ( 56% ) ( 22% ) ( 11% ) ( 11% ) ( 80% ) ( 20% ) ( 0% ) ( 0% ) lateral rear anterior fnab accesso ago . soffusione emorragica soffusione emorragica e pnx soffusione emorragica soffusione emorragica e pnx 100% 100% 100% 100% anteriore laterale posteriore anteriore laterale posteriore in addition , we correlated complications with lesion location , in terms of side and lobe . 
11 cnb : right lung cnb right lung . hemoptysis suffusion suffusion + pnx 100% 100% 100% lower 100% 100% middle emottisi soffusione emorragica soffusione emorragica e pnx 100% 100% upper cnb polmone destro . ( 0% ) ( 20% ) 100% 100% 100% hemoptysis suffusion suffusion + pnx ( 0% ) ( 20% ) ( 50% ) ( 0% ) ( 0% ) ( 0% ) ( 30% ) ( 0% ) lower middle upper emottisi soffusione emorragica soffusione emorragica e pnx ( 14% ) ( 29% ) ( 14% ) ( 29% ) ( 14% ) ( 14% ) ( 29% ) ( 14% ) ( 29% ) ( 14% ) ( 50% ) ( 30% ) ( 0% ) ( 0% ) ( 0% ) ( 0% ) inferiore medio superiore inferiore superiore medio patients undergoing cnb had inammatory disease , or lesion histology since the histological results were widely heterogeneous . the rate of nondiagnostic samples at denitive histological examination , assessed on the basis of the pathology reports , was 18.1 % for cnb and 10.7 % for fnab ( table 6 )  . we then calculated the diagnostic accuracy of the two evaluation revealed that fnab , methods . 
12 fnab : right lung fnab right lung . suffusion suffusion + pnx radiol med ( 2014 ) 119 : 572594 suffusion suffusion + pnx 100% 100% ( 0% ) ( 0% ) ( 17% ) 0 ( 17% ) ( 0% ) middle upper 100% middle fnab polmone destro . soffusione emorragica soffusione emorragica e pnx soffusione emorragica soffusione emorragica e pnx 100% 100% 100% ( 67% ) ( 67% ) 100% lower 100% 100% ( 0% ) ( 0% ) ( 17% ) 0 ( 17% ) ( 0% ) inferiore medio superiore inferiore medio superiore ( 40% ) ( 20% ) ( 40% ) ( 0% ) lower ( 40% ) ( 20% ) ( 40% ) ( 0% ) upper discussion in pulmonary lesions , it is very important to distinguish correctly between benign and malignant lesions , since the pathological diagnosis will determine the treatment to be applied [ 13 ]  . one diagnostic method used in the evaluation of lung cancer is bronchoscopy , but when this is not sufcient for the diagnosis , particularly in peripheral pulmonary lesions or pleural lesions , a trans - thoracic biopsy is performed [ 14 ]  . 
13 cnb : left lung cnb left lung . hemoptysis suffusion suffusion + pnx 100% 100% 100% lower 100% upper cnb polmone sinistro . emottisi soffusione emorragica soffusione emorragica e pnx 100% 100% hemoptysis suffusion suffusion + pnx ( 11% ) ( 56% ) ( 11% ) ( 11% ) ( 11% ) ( 0% ) ( 67% ) ( 17% ) ( 0% ) ( 17% ) lower upper emottisi soffusione emorragica soffusione emorragica e pnx ( 11% ) ( 56% ) ( 11% ) ( 11% ) ( 11% ) ( 0% ) ( 67% ) ( 17% ) ( 0% ) ( 17% ) inferiore superiore inferiore superiore who had inammatory disease . 
this did not allow us to evaluate diagnostic accuracy in relation to the benign or malignant nature of the lesion . the literature contains heterogeneous data on this topic . fnab has a diagnostic accuracy that varies from 64 to 97 % [ 7 ]  . 
this can in part be justied by the severity of the judgement to which the samples were subjected : material lacking malignant cells should not be considered negative for malignancy , unless it is possible to formulate a clear and specic diagnosis of a benign disease [ 19 ]  . in some studies , diagnostic accuracy appears to be higher in the case of larger lesions and of fnab performed in the presence of a pathologist to assess sample adequacy is not [ 4 ]  . 
14 fnab : left lung radiol med ( 2014 ) 119 : 572594 fnab left lung . suffusion ( 56% ) ( 22% ) ( 22% ) lower ( 56% ) ( 22% ) ( 22% ) ( 71% ) ( 14% ) upper ( 71% ) ( 14% ) ( 14% ) ( 14% ) 100% 100% 100% suffusion lower upper fnab polmone sinistro . soffusione emorragica soffusione emorragica 100% 100% 100% inferiore superiore inferiore superiore available for extemporaneous evaluation of the samples . this may lead the operator to use cutting needles even when in the presence of small nodules [ 20 , 21 ]  . charig and phillips [ 20 ] have shown that the diagnostic accuracy of cnb is similar to that of fnab , if performed with a pathologist on site . 
tsukada [ 24 ] found a gradual and progressive decrease of diagnostic accuracy values with decreasing lesion size , from 100 % ( for lesions \5 cm ) to 67 % ( for lesions \1 cm )  . 
we therefore recorded , regardless of the reported rate of pneumothorax after ct - guided lung biopsies ranges from 4 % [ 26 ] to 62 % [ 27 ]  . 
in the present study , where any air ap between the pleura and the lung was considered a pneumothorax , the incidence was 21.3 % and thus falls within the reported range ( table 2 )  . 
17 cnb : number of passes 100% 0%0% 100% hemoptysis suffusion suffusion e pnx 100% 100% emottisi soffusione emorragica soffusione emorragica e pnx 100% 0%0% 100% 100% 100% 100% 100% 590 radiol med ( 2014 ) 119 : 572594 results are consistent with the percentages reported in other studies [ 29 ]  . lesions [ 30 , 31 ] or even a 4 % decrease in risk for each 10 - mm increment in lesion diameter [ 5 ]  . the onset of pneumothorax was found to correlate with variables related to both the procedure and the patient ( table 3 )  . 
18 fnab : number of passes fnab number of passes . suffusion suffusion + pnx suffusion suffusion + pnx 100% 100% 100% ( 55% ) ( 27% ) ( 14% ) ( 5% ) ( 55% ) ( 27% ) ( 14% ) ( 5% ) ( 67% ) ( 33% ) ( 0% ) ( 0% ) ( 67% ) ( 33% ) ( 0% ) ( 0% ) fnab numero passaggi . soffusione emorragica soffusione emorragica e pnx soffusione emorragica soffusione emorragica e pnx 100% 100% 100% radiol med ( 2014 ) 119 : 572594 ( 7% ) ( 29% ) ( 21% ) ( 29% ) ( 14% ) 100% ( 7% ) ( 29% ) ( 21% ) ( 29% ) ( 14% ) 100% cnb histologic type . hemoptysis suffusion suffusion + pnx ( 0% ) ( 0% ) ( 0% ) ( 0% ) ( 0% ) ( 100% ) ( 40% ) ( 0% ) ( 0% ) ( 0% ) ( 20% ) ( 20% ) ( 40% ) ( 40% ) ( 20% ) ( 20% ) ( 0% ) ( 40% ) 2 ( 20% ) notevaluable adenocarcionoma bronchioloalveolar sccl squamos ( 0% ) ( 0% ) inflammation ( 100% ) 100% 100% ( 100% ) 100% 100% 100% 100% 100% 100% 100% 100% 100% 100% 100% 100% adenocarcinoma bronchioloalveolar sccl squamous not evaluable inflammation cnb istologia . emottisi soffusione emorragica soffusione emorragica e pnx ( 0% ) ( 0% ) ( 0% ) ( 0% ) ( 0% ) ( 100% ) ( 40% ) ( 0% ) ( 0% ) ( 0% ) ( 20% ) ( 20% ) ( 40% ) ( 40% ) ( 20% ) ( 20% ) ( 0% ) ( 40% ) 2 ( 20% ) non valutabile k adenocarcinoma k bronchioloalveolare k microcitoma k spinocellulare patologia infiammatoria ( 0% ) ( 0% ) ( 17% ) ( 67% ) 100% ( 17% ) ( 67% ) 100% k adenocarcinoma k bronchioloalveolare k microcitoma k spinocellulare non valutabile patologia infiammatoria fig . 
this can be ascribed to the fact that many of these patients normally took anti - aggregating or anticoagulant therapies and thus suffered from coagulation disorders , a nding in contrast with other authors reports [ 5 ]  . as described in the literature [ 5 ] , posterior access ( table 5 ) carries a greater risk of complications . 
21 diagnostic accuracy of fnab and cnb based on dimension of lesions 594 conclusions fnab seems to be burdened by a lower complication rate than cnb in terms of both absolute values and in relation to variables inherent to the patient , the procedure and the lesion . 
the diagnostic accuracy is higher for fnab and , if this technique is performed in the presence of a pathologist , it is characterised by a lower rate of inadequate samples than cnb . 
a protocol with exposure parameters based on patient body mass index ( bmi ) and with images reconstructed using fbp ( group a ) was compared with a protocol with images acquired using tube current decided by an automatic exposure control system and reconstructed using aidr ( group b )  . 
gravina laboratory of radiobiology , division of radiotherapy , department of biotechnological and applied clinical sciences , university of laquila , via vetoio 1 , 67100 laquila , italy noise was signicantly lower in group b with consequent higher signal - to - noise ( snr ) and contrast - to - noise ( cnr ) ( p \ 0.0001 ) compared with group a . 
subjective quality parameters were also signicantly higher in group b . conclusions comparative analysis by propensity score matching conrms that aidr 3d with automatic exposure control is able to reduce signicantly the mean radiation dose and improve the image quality compared with traditional fbp without exposure modulation . keywords coronary ct angiography ( cid : 2 ) adaptive iterative reconstruction ( cid : 2 ) image noise ( cid : 2 ) radiation dose ( cid : 2 ) image quality introduction coronary artery disease ( cad ) is the leading cause of death in developed countries [ 1 , 2 ] , and cardiac catheterisation remains the standard of reference for the evaluation of the coronary arteries . 
these methods provide signicant reductions in radiation dose and have been reported to result in similar image quality in multicentre studies [ 6 ]  . three recent reports [ 79 ] have indicated that adaptive iterative dose reduction ( aidr 3d ) with built - in automatic exposure control ( sureexposure 3d ) has better performance than traditional ltered back - projection ( fbp ) without automatic dose modulation . 
in order to mitigate methodological biases , the image quality and mean radiation doses of aidr 3d with sureexposure 3d were compared with traditional fbp without automatic dose modulation using a 640 - slice ct scanner and a one - beat prospective acquisition by propensity score matching . 
this powerful statistical approach , attempting to reduce the bias due to confounding variables that could be found in an estimate of the outcome measure obtained from simply comparing outcomes among units belonging to different study groups , simulates a randomisation process by creating an absolute comparability of clinical characteristics among groups . 
thus , the aim of this study was to conrm , using this powerful statistical approach , whether the use of aidr 3d with sureexposure 3d really provides clinical and dosimetric advantages with respect to traditional fbp without dose modulation . materials and methods patients from october 2011 to december 2012 , 272 consecutive patients scheduled for coronary ct were prospectively studied with a 640 - slice ct scanner ( aquilion one , toshiba medical systems )  . 
exclusion criteria were impaired renal function ( serum creatinine [ 1.5 mg / dl ) , previous coronary artery interventions , heart rate [ 65 beats per minute ( bpm ) after beta - blocker premedication and severe calcication of the major coronary arteries . 
images were evaluated for the presence of signicant stenosis , which was dened as a narrowing of the coronary lumen equal to or exceeding 50 % of the cross - sectional area . 
institutional review board approval was obtained and all patients provided informed consent before the procedures . acquisition protocol injector all ct scans were acquired using a 640 - slice ct scanner . one hour before imaging , the patients blood pressure and heart rate were recorded . 
just before the acquisition , 0.3 mg of sublingual nitroglycerin ( isosorbide dinitrate , carvasin 5 mg , wyeth lederle ) was administered to all patients [ 10 ]  . 
sixty millilitres of nonionic contrast medium ( iomeron 400 , bracco diagnostic , milan , italy ) was injected into the antecubital vein at 5 ml / s , followed by 40 ml of saline solution at the same ow rate , using a dual power ( stellant , medrad , indianola , pa , usa )  . 
the timing to start the ct acquisition was determined using bolus tracking ( sure start ) in the descending aorta with a scan start threshold of 300 hounseld units ( hu )  . 
for each patient , the phase with the least artefacts was automatically 644 radiol med ( 2014 ) 119 : 642649 determined by the systea motion map of the sinogram was traced by the system and the phase with the least movement was chosen ( phasexact , toshiba medical systems , tochigi , japan )  . 
the maximum number of reconstructed slices was 640 with 0.5 mm thickness and 0.25 mm interval , obtained by means of the proprietary double - slice technique and cone - beam reconstruction algorithm ( conexact , toshiba medical systems , tochikiken , japan )  . 
issues such as motion and poor gating were not taken into account in the subjective assessment , as they could not be ascribed to the reconstruction algoriththe coronary arteries were subdivided into 15 segments according to the american heart association classication [ 11 ]  . 
the 15 coronary artery segments were categorised into three segmental classes as follows : ( 1 ) proximal [ proximal right coronary artery ( rca ) , left main coronary artery ( lm ) , proximal left circumex artery ( lcx ) , proximal left anterior descending artery ( lad ) ] ; ( 2 ) mid [ mid rca , distal rca , ramus intermedius ( r . intermedius ) , obtuse marginalis ( om ) , rst diagonal branch ( d1 ) , mid lad ] ; and ( 3 ) distal segmental classes [ posterior descending artery ( pda ) , distal lcx , second diagonal branch ( d2 ) , distal lad ] [ 8 ]  . 
1 a , b measurement of signal and noise in the ascending aorta , above the coronary ostia , in two patients with the same body mass index of 26 . 
the signal ( vi ) of the proximal coronary arteries was measured as the mean attenuation value ( hu ) within circular rois drawn in the central portion of both the left main coronary artery and right coronary artery , with care to avoid inclusion of the coronary vessel wall [ 8 ]  . 
ct density of the epicardial fat ( ve ) surrounding the artery was measured by placing a roi immediately next to the artery ( both left main coronary artery and right coronary artery ) [ 10 ]  . 
snr and cnr were calculated as follows : snr = vi / n , cnr = ( vi - ve ) / n ; snr was calculated by dividing the density by the image noise and , as for the cnr , ct density of the epicardial fat ( ve ) was subtracted from signal ( vi ) , which was then divided by the image noise [ 10 ]  . estimation of radiation dose for each patient radiation dose was assessed by multiplying the dlp ( dose length product ) by the conversion coefcient for the chest ( 0.014 msv / mgy cm ) [ 16 ]  . statistical analysis continuous variables were condensed by means , standard deviation ( sd ) , standard error ( se ) or 95 % condence intervals ( ci ) as appropriate . 
a propensity score was arranged using gender , age , weight and bmi as covariates . a 1 : 1 matched analysis was performed where one case was matched with one control . 
twenty - one subjects were excluded due to previous coronary artery interventions ( 15 patients with coronary artery by - pass graft ) and hr [ 64 bpm after beta - blocker premedication ( 6 patients )  . 
in group a , 24 patients ( 24 % ) did not have signicant stenosis , 36 ( 36 % ) had single - vessel disease , 18 ( 18 % ) had two - vessel disease , and 22 ( 22 % ) had threevessel disease . 
among 1 , 600 segments analysed , 257 segments in group a and 242 in group b were considered to be unevaluable because the segment was absent ( 224 and 215 segments , respectively ) , too small ( diameter \1.5 mm ; 30 and 23 segments , respectively ) or completely occluded ( 3 and 4 segments , respectively )  . 
noise was the results of objective image quality analysis are descrihigher ( p = 0.0018 ) in group a while the snr and cnr were signicantly higher in group b ( table 5 )  . 
a previous study reported that coronary ct using a 320 - detector scanner has the potential to signicantly reduce the radiation dose while maintaining high diagnostic accuracy [ 20 ]  . 
moreover , the aec systems now available for multidetector ct scanners are able to adjust the radiation dose according to the patients attenuation while sustaining diagnostic image quality [ 21 ]  . 
sureexposure ( toshiba medical , tokyo , japan ) , the aec system that we used , provides both patient - size and z - axis aec [ 21 ]  . 
the aidr 3d works in both the raw data and the image domafirst , the algorithm works on the raw data performing a noise reduction process of the sinogram based on a projection noise estimation considering a noise model and a scanner model . 
at the end of the iterative process , a weighted blending between the original image and the image obtained by the process is automatically applied by the systeaidr 3d improves the snr , preserving and enhancing the edge of the anatomical structures and the spatial resolution . 
a limit of a general iterative reconstruction is the unnatural look of the images ; aidr 3d gives images a natural look by increasing the snr and the spatial resolution . 
the amount of dose reduction with a xed level of noise is automatically determined by the sureexposure3d with aidr 3d integrated into the acquisition protocols . in this study , we evaluated the effect of aidr 3d and aec on image quality and mean radiation dose in comparison with conventional fbp that employs exposure parameters based on patient bmi , on a 640 slice ct scanner 648 radiol med ( 2014 ) 119 : 642649 [ 8 , 22 ]  . 
its application in ct was limited by the time - consuming repetitive reconstruction process until a few years ago , when advances in computer performance made iterative reconstruction feasible also for ct , which produces much more projection data than emission tomography [ 23 ]  . 
indeed , both subjective and objective image quality analysis showed signicantly higher quality in the aecaidr - 3d group . subjective analysis showed signicant improvement of the image quality in the aidr group images for all the segments evaluated . 
 [ 8 ] found an improvement in image quality using aidr 3d with a built - in aec system but they did not evaluate the effects of these technologies on radiation doses . 
 [ 9 ] also found both a signicant improvement in image quality and a reduction in radiation dose using aidr 3d but the quality assessment was made on a per - patient rather than a per - segment level . 
this is showed because particularly improvement of the image quality in the aidr 3d group , especially in the intermediate and distal segmental class , which are generally the segments with lowest image quality , primarily due to the small calibre of these vessels ( \1.5 mm in diameter )  . 
the aec system , taking into account the aidr3d reconstruction , automatically selects the tube current on the basis of the body prole and the attenuation information derived from the scanogram , to reach the target standard deviation of pixel values for a specied target image quality . 
moreover , aidr 3d improves the snr . important results the main limitation of this study is clearly the estimation of the current reduction generated by the introduction of the aidr 3d with respect to the current chosen from the bmi table . 
the same bmi , indeed , may be present in a patient with a very large abdomen and small chest diameter . in our study we investigated only the dose reduction due to the contribution of aidr 3d . 
the results in dose reduction obtained with aidr 3d suggest that coronary ct imaging could be further improved by modifying the reconstruction kernel [ 24 ] and the contrast injection protocol [ 25 ]  . 
it is worthy of note that aidr 3d is more efcient when the tube voltage is low and , in this study , we use a protocol that employed a tube voltage of 120 kv . 
the next step will be the possible introduction of 80 kv . conclusions the main strength of our study lies in the use of propensity score analysis which helped us to obtain two groups of patients virtually randomised for important clinical characteristics . thus , the comparative analysis by propensity - matched pairs made the results less prone to methodological biases compared with other usual statistical methods and allowed us to conrm that aidr 3d with aec is able to reduce signicantly the mean radiation dose and improve the image quality with respect to traditional fbp without dose modulation . acknowledgments the present work beneted from the input of eng . 
colagrande ( & ) dipartimento di scienze biomediche sperimentali e cliniche , struttura complessa di radiodiagnostica ( sod 2 ) , universita` di firenze , azienda ospedaliero - universitaria careggi , largo brambilla 3 , 50134 florence , italy e - mail : stefano.colagrande@uni.it 626 radiol med ( 2014 ) 119 : 625633 conclusion the pretreatment adc value of a liver metastasis does not seem useful in predicting the cht outcome . 
a trend towards early adc increase , alone or occurring with dimensional decrease , may be a good indicator of a responding lesion . keywords magnetic resonance imaging ( cid : 2 ) diffusionweighted imaging ( cid : 2 ) apparent diffusion coefcient ( cid : 2 ) chemotherapy ( cid : 2 ) liver metastasis least two dimensions , without intralesional necrosis / calcication involving [ 30 % of the volume ; ( b ) a karnofsky performance scale score c60 % ; ( c ) being at least 18 years old ; ( d ) not being pregnant ; ( e ) being scheduled to begin a new cht regimen for metastatic disease , with no contraindications to cht . 
the exclusion criteria were a history of any other malignant disease not included in the entry criteria and contraindications to mr imaging . introduction magnetic resonance diffusion - weighted imaging ( mr - dwi ) allows the quantitative assessment of changes in the diffusion properties of water molecules in vivo by apparent diffusion coefcient ( adc ) calculation . 
mr - dwi acquisition is noninvasive , with no contrast medium administration being required , and possible use in patients with renal dysfunction can be obtained quickly and easily incorporated into routine examination protocols . 
mr - dwi is increasingly being used in extracranial applications , such as in the breast , liver and prostate , as well as in general abdominal imaging , because of its added value in the detection and characterisation of focal lesions , in particular malignant lesions [ 13 ]  . 
mr - dwirelated parameters are appealing as imaging biomarkers because their changes during therapy could potentially be compared with other biomarker changes such as serum tumour markers or with recist and / or who measurements of tumour size . 
in this sense , they could be useful for the early assessment of tumour response to chemotherapy ( cht ) , as already found in previous studies [ 2 , 4 , 5 ]  . given this background , the aim of our multicentric study was to evaluate the potential of mr - dwi in both the prediction and early assessment of response to cht of liver metastases , by itself and along with early dimensional assessment . methods and materials patients the local ethics committee approved the study protocol ( number 470 / 10 , azienda ospedaliera - universitaria careggi , firenze )  . 
the inclusion criteria for patients were : ( a ) the presence of nonconuent liver metastases pancreatic ( including neuroendocrine ) or breast carcinoma diagnosed at the time of primary tumour staging or during the follow - up , histologically conrmed or clinically proved ( by means of serial imaging and serum tumour markers ) , measuring at least 1 cm in diameter and measurable in at from gastrointestinal , imaging technique all patients were scanned by contrast - enhanced ( ce ) - ct and mr - dwi before the beginning of cht ( baseline , time 0 )  . 
the time between these two initial studies did not exceed 1 week . mr - dwi was then repeated 1015 days ( time 1 ) and 2025 days ( time 2 ) after the beginning of the rst cycle of cht . 
the detailed mr protocol is shown in table 1 and included the following sequences : axial breath - hold ge t1w in / out of phase , axial and coronal free - breathing single - shot tse t2w with and without fat suppression , axial free - breathing echo - planar dw multi - b imaging ( b value ranging from 0 to 800 s / mm2 with consecutive steps of 50 s / mm2 )  . 
for each lesion , a dimensional analysis was performed at all times measuring the two maximum perpendicular diameters visible on the axial portal phase contrast - enhanced ct images and on the axial dw images obtained with low b value ( b = 50100 s / mm2 ) where the signal from vessels is erased and lesion conspicuity is greater ; all sums of the diameters were recorded . 
the lesion was again visualised on images obtained at b = 50 s / mm2 ; a region of interest ( roi ) was manually drawn including the entire lesion and taking care to avoid adjacent vessels ; thereafter the same roi was copied and pasted to all remaining b value images acquired . 
an roi of similar size was also drawn in the normal liver parenchyma of the central part of the right lobe ( to avoid cardiac motion artefacts ) where data show higher reproducibility and repeatability [ 6 ] , excluding large blood vessels , biliary vessels and hepatic borders . 
lesion and parenchyma adc values were obtained by tting mono - exponential model to the dwi signal obtained at different b values using the following equation : exp ( cid : 3 ) b ( cid : 4 ) adc assessment of therapeutic response and statistics therapeutic response was determined on a lesion - by - lesion basis by evaluating changes in tumour size at time 3 with respect to baseline , according to recist 1.1 criteria [ 7 ]  . 
a metastatic lesion presenting a 20 % or more increase in the maximum transverse diameter with respect to time 0 was classied as progressive disease ( pd ) ; a lesion showing at least 30 % of reduction in the maximum transverse diameter with respect to time 0 was classied as partial response ( pr )  . 
from a clinical point of view , lesions remaining stable or regressing ( sd and pr , respectively ) were also labelled as responding ( r ) , while those progressing were classied as not responding ( nr )  . 
mean diameter and adc value ( with corresponding standard deviations ) were calculated in pd , pr and sd lesion groups at the different times using mixed linear regression models , with subjects as a random - effect . 
2 box and whisker plots showing distribution of dimensional changes of progressive disease ( pd ) , stable disease ( sd ) and partial response ( pr ) lesions at different times . 
the horizontal line in each box is the median of measured values ; the top and bottom of boxes represent 25th and 75th percentile ; points represent outlier values . although there are several overlaps between groups at different times , some statistically signicant differences were found and are listed in tables 2 and 3 fig . 
the horizontal line in each box is the median of measured values ; the top and bottom of boxes represent the 25th and 75th percentile ; points represent outlier values . 
changes in adc values ( either as absolute values or as lesion / parenchyma ratio ) , early dimensional changes assessed on low - b dw images and a combination of the two were evaluated in pd , pr and sd lesions to determine the performance of these assessments in correctly classifying a lesion . 
table 2 also lists all p values found with analysis of variance ( anova ) using pd group as reference , showing possible differences among the pd , sd and pr groups for each time . 
now , they are even more debated because hospitals around the world are cutting budgets reserved for these treatments and , at the same time , new cht regimens tend to have higher costs . 
early knowledge of whether an expensive new drug will be effective has therefore become crucial . prediction of response based on pre - treatment adc continues to be controversial , as can be seen from the literature . 
tumours with necrotic areas are often surrounded by hypoxic , but viable cells , and were shown to be less sensitive to ionising radiation [ 8 ] , more prone to aggressive behaviour and probably less sensitive to cytotoxic agents [ 9 ]  . 
therefore , it may be hypothesised that such lesions would be presenting higher pre - treatment adc and have a worse treatment outcome . even though some important studies conrm this theory [ 5 , 10 ] , others [ 1113 ] do not show any signicant correlation between pre - treatment adc and response to chemoor radiotherapy . 
in our series , the mean pre - treatment adc value of r ( both sd and pr ) lesions did not turn out to be signicantly different from that of nr ( pd ) lesions ( table 2 ) ; as a consequence , adc failed to predict the cht response of lesions and our result cannot conrm the above hypothesis . early assessment of cht response is the second issue we tried to address in our study : in other words , if dwi would be able to provide early marker ( s ) for treatment efcacy . most published studies [ 3 , 5 , 10 , 1620 ] have shown that adc changes may precede dimensional ones , since early radiol med ( 2014 ) 119 : 625633 diffusion - weighted ( dw ) - mr images fig . 
however , it has also been demonstrated that the timing of imaging is of crucial importance : changes in adc could precede changes in tumour size , but may even disappear after a certain time because of repair mechanisms such as decrease of oedema and organisation of necrosis [ 21 ]  . 
assessment of the cht response of liver metastases in our experience appears feasible after 2025 days since the beginning of cht using both the conventional approach based on evaluation of dimensional changes and adc analysis . 
dimensional assessment is easy , fast and reproducible when performed on dwi acquired with b values of 50100 s / mm2 ; on these images , in fact , changes . 
according to lowenthal et al . [ 22 ] small lesions ( in particular , those with diameter\1 cm ) tend to appear larger on dwi than on mr delayed images after liver - specic contrast administration , and the reason for that remained unclear ; however , this did not affect our results because we compared measurements obtained with the same acquisition sequence . 
as our results show , when assessing lesion diameters 2025 days after the beginning of cht , we should adopt different comparison criteria from those postulated in the recist guidelines . 
because of this and the relatively small sample of lesions analysed , at this point it does not make sense to search for a cutoff increase / decrease in transverse maximum diameters to correctly classify a lesion as r or nr . 
however , the relatively good 632 radiol med ( 2014 ) 119 : 625633 auc value conrms that changes in size at this time directly reect later dimensional changes . when examining adc changes at different times , rst of all we can notice that at time 1 there is an increase in mean values of all groups with respect to the corresponding pretreatment values , so it does not appear possible to discriminate r and nr lesions at this time . 
however , at time 2 and 3 the mean adc values of r lesion groups ( both sd and pr ) become signicantly higher than the corresponding pretreatment values , conrming the hypothesis of reduced cellularity and increased diffusion of water molecule into the extracellular space for r lesions . 
on the other hand , the mean adc of nr lesions , after the above - mentioned initial increase , actually drops to the pre - treatment level , where it remains stable . 
we can therefore conrm that an early ( 2025 days after the beginning of the rst cycle ) evaluation of adc changes appears useful for an early assessment of clinical response . 
nonetheless , moving from a per - group adc analysis to a lesion - by - lesion one ( which means translating these facts into clinical practice ) , things become more difcult and often controversial . 
among the intrinsic factors we should consider the location of the lesion ( in particular , when a lesion is located on or near organs subject to respiratory or other kinds of movement ) , its histotype , the presence of internal necrotic areas and calciuamong the extrinsic factors we should consider those related to cht ( type of drugs used , duration , days past since the beginning , etc ) and others related to the mr - dwi acquisition technique and adc calculation ( in particular , images low signal - to - noise ratio , acquisition artefacts , b value adopted and lesion sampling )  . what the clinician needs is a method capable of overcoming most of these factors and in particular the dependence from primary tumour histotype and type / duration of cht used , to easily manage the scheduling of different patients . besides , both the acquisition process and adc measurement should be kept as quick and reproducible as possible , to be implemented in routine clinical practice . 
based on these considerations , we chose this particular study design , especially with regard to the inclusion of metastatic lesions from a wide range of primaries , the decision to use average time for early evaluations , the choice to acquire multi - b dw images ( to calculate adc by a tting procedure and keep off the dependency from b value ) and the very easy and fast lesion sampling method ( both for adc and for dimensional comparison among times )  . 
all of these variables in our study indeed may have represented the major limitations for us to obtain relevant and not contradictory results , along with the relatively small sample of lesions analysed , in particular nr lesions . 
it should not be completely excluded that inclusion of a larger sample of nr lesions , and thus a comparison between more homogenous lesion groups , would make it possible to extrapolate both analysis method and criteria lesion by lesion allowing early discrimination of clinically r lesions from nr ones . 
the latter point seems to be critical because oncologists usually need to recognise nr patients early on and , if necessary , move them to a different cht regimen , thus avoiding unnecessary side effects and costs . conclusions mr - dwi can provide different tools to perform an early assessment of the response of liver metastases to cht , including the conventional evaluation of dimensional changes and adc analysis . 
however , a trend of early ( 2025 days since the beginning ) adc increase alone or in combination with dimensional decrease may be a good indicator of a responding lesion . 
radiochemotherapy is the treatment of rst choice in non - metastatic disease . intensity - modulated radiation therapy ( imrt ) allows the sparing of parotid glands , improving the toxicity prole . 
the aim of this study was to compare the results obtained with imrt with those obtained with conventional 2d ( 2drt ) and 3d conformal radiation therapy ( 3dcrt ) in terms of tumour control , survival , acute and late toxicity . materials and methods we reviewed the clinical records of 52 patients with histologically proven carcinoma of the nasopharynx ( stage iivb according to the 2002 american joint committee on cancer staging system ) treated with curative intent between january 2003 and august 2011 : 26 patients were treated with 2d or 3d technique ( arm a ) and 26 with imrt technique ( arm b ) with simultaneous integrated boost . 
fifty patients ( 96 % ) received chemotherapy . local control ( lc ) , locoregional control ( lrc ) , diseasefree survival ( dfs ) , overall survival ( os ) , acute and late toxicity were retrospectively evaluated . results after a median follow - up of 37.6 months ( 69 months in arm a and 23 months in arm b ) , 69 % of patients were alive and disease - free , 10 % were alive with disease and 21 % died of disease , with an os of 81 % at 2 years and 79 % at 5 years , a lc rate of 88 % at 2 years and 78 % at 5 years , a lrc rate of 80 % at 2 years and 73 % at 5 years and a dfs of 74 % at 2 years and 65 % at 5 years , with no statistically signicant differences between imrt and 2drt / 3dcrt . 
pecorari dipartimento di scienze chirurgiche , otorinolaringoiatria 1 - u , universita` di torino , turin , italy radiol med ( 2014 ) 119 : 634641 moderately hypofractionated regimens , allows good disease control with better results in terms of late xerostomia , although without statistically signicant differences compared to 2drt and 3dcrt . 
the hypothesis of an impact of imrt on survival has yet to be conrmed . keywords nasopharyngeal cancer ( cid : 2 ) radiotherapy ( cid : 2 ) treatment techniques introduction nasopharyngeal carcinoma ( npc ) is a pathological , epidemiological and clinical entity distinct from other head and neck cancers . 
it is rare in the united states and other western countries , but common in southern china , southeast asia , the middle east and north africa [ 1 , 2 ]  . in these countries , most patients have differentiated nonkeratinizing or undifferentiated carcinoma ( who types 2 or 3 ) , while keratinizing squamous cell carcinoma or who type 1 is rare , but more common in western countries [ 3 , 4 ]  . 
many patients present with locally advanced disease . the standard of care for locally advanced npc is a combination of radiotherapy ( rt ) and chemotherapy [ 2 ]  . the overall survival ( os ) rate at 5 years ranges from 32 to 52 % in large series of patients with locally advanced disease treated with rt alone [ 2 ]  . 
no signicant reduction in the risk of locoregional recurrence and / or distant metastases , and no improvement of os were shown for adjuvant chemotherapy after chemo - radiation . the addition of neoadjuvant chemotherapy to radiation signicantly reduced the risk of locoregional recurrence and distant metastases , but without a signicant improvement in os [ 10 ]  . npc has a relatively good prognosis also in locally advanced cases : the disease is often chemoand radiosensitive and patients are usually younger and less exposed to tobacco and alcohol than the majority of head and neck cancer patients . conformal radiotherapy ( 3dcrt ) was considered the standard technique when intensity - modulated radiation therapy ( imrt ) emerged as a technique able to better conform the dose around target volumes and to better spare organs at risk . 
because of a steep dose gradient and a high conformity index , the risk of target missing with imrt is higher than with conformal technique , as the integral dose . xerostomia is a common and disturbing late effect of conventional rt . 
several authors demonstrated the superiority of imrt over 2drt or 3dcrt in parotid gland sparing and two randomised controlled trials have proved a better salivary toxicity prole [ 11 , 12 ]  . since 2006 , at the radiation oncology department of the university of turin , patients affected by nasopharyngeal cancer were treated with imrt , with or without chemotherapy . 
the aim of the present study was to retrospectively review clinical outcomes ( efcacy and toxicity ) of this subgroup of patients and to compare these results with a previous series of patients treated in the same institution with 2drt and 3dcrt . materials and methods patients all patients affected by histologically proven , stage iivb ( according to the 2002 american joint committee on cancer staging system ) nasopharyngeal carcinoma treated with curative intent between january 2003 and august 2011 at our institution were included , with a minimum follow - up time of 6 months . 
patients with a previous history of cancers other than non - melanomatous skin carcinoma or in situ cervical carcinoma were excluded . fifty - seven patients met the inclusion criteria : 30 patients underwent 2drt or 3drt ( arm a ) and 27 imrt ( arm b )  . five patients ( four from arm a and one from arm b ) were excluded from the analysis because of a history of malignancies . 
patients characteristics are summarised in table 1 . radiation therapy all patients were immobilised with a thermoplastic mask . in the 2drt group , to dene treatment elds , facial cervical radiograms were taken using a conventional x - ray simulator . 
the lower neck was treated with 5054 gy through a single anterior eld with midline shielding . megavoltage photons ( 6 mv ) were used to treat the primary tumour and neck lymph nodes , with high - energy electron boost ( 1020 gy ) for posterior neck lymph nodes . in the 3dcrt group , a planning ct without contrast enhancement was performed . 
radiation elds were chosen according to the extent of the tumour as evaluated by clinical examination , contrast - enhanced ct and / or mri and / or ct - pet . 
the gross tumour volume ( gtv ) included the primary tumour and abnormal lymph nodes . clinical target volume 1 ( ctv 1 ) included the nasopharynx , bilateral upper cervical lymph nodes ( levels ib iiiii , upper part of level v ) and retropharyngeal lymphatics ; ctv2 included low cervical and supraclavicular nodes . 
2d and 3d plans were delivered with a 6 mv linac ( elekta sl - 75 , stockholm , sweden )  . twenty - six patients were treated with imrt . 
twenty of them were treated with a split - eld technique ( with a unique anterior eld for inferior neck and supraclavicular fossa ) and six with a whole - eld technique , to treat the entire volume with a single plan . in the imrt group a planning ct without contrast enhancement was performed . 
ctv1 was generated after a 510 mm expansion of the gtv ; ctv2 included all lymph node levels at risk of subclinical disease ( levels ibiiiiiiv - upper part of v level )  . 
the ptvs in nasopharynx and upper neck were treated using 79 coplanar beams ; a variety of fractionations was used , for example 69.44 gy in 32 fractions , 69.96 gy in 33 fractions or 70 gy in 35 fractions were prescribed to the ptv1 and 51.2 gy in 32 fractions , 54.25 gy in 35 fractions or 59.4 gy in 33 fractions to the node - negative regions ( ptv2 )  . 
imrt plans were delivered with a 6 mv linac ( elekta precise or elekta synergy , stockholm , sweden )  . an optimal sparing of at least one parotid gland was attempted , especially the contralateral one with respect to the tumour or metastatic lymph nodes . 
twelve patients in the arm a and 11 patients in arm b had bilateral neck involvement . chemotherapy all patients but two ( with t1n0m0 and t2bn0m0 disease , respectively ) were treated with chemotherapy ; 33 patients ( 63.5 % ) underwent induction chemotherapy plus concurrent chemotherapy in 31 patients ( table 2 )  . 
for 30 patients a cisplatin - based chemotherapy was scheduled at the dose of 100 mg / m2 every 21 days , and 14 patients were treated with weekly doses ( 30 mg / m2 )  . radiol med ( 2014 ) 119 : 634641 toxicity . 
the follow - up time was counted from the date of completion of radiation therapy . univariate and multivariate analyses were performed for evaluation of the prognostic factors and factors correlated to late toxicity . 
stata statistical package version 11.0 ( statacorp lp , texas , usa ) was used for statistical computations . results after a median follow - up of 37.6 months , 69 months in arm a ( range 7108 ) and 23 months in arm b ( range 874 ) , 36 patients ( 69 % ) were alive and without evidence of disease , 5 ( 10 % ) were alive with disease , 11 ( 21 % ) died from disease . 
twoand ve - year lc rates were 88 and 78 % ; 2and 5 - year lrc rates were 80 and 73 % ; and 2and 5 - year dfs rates were 74 and 65 % , respectively . in arm a , ve patients had persistent disease after rt : a nasopharyngeal mass in one case , lymph node metastases in two cases and disease in both locations in other two cases : three patients with residual nodal disease also developed distant metastases . 
during follow - up , other ve patients relapsed , two locally ( one of whom then developed distant metastases ) , one in the neck , one in both the nasopharynx and neck and another one with bone metastases , respectively . two patients with persistent lymph node metastases underwent salvage surgery , but only one was still alive when the study was concluded . 
one patient underwent photodynamic therapy for a local recurrence , and then a neck dissection was performed for a regional recurrence , without evidence of disease at the last follow - up . table 3 chemotherapy regimens in the two treatment arms timing of chemotherapy drugs neoadjuvant cisplatin ? 5fu patients ( arm a ) patients ( arm b ) concurrent cisplatin ( 100 mg / m2 ) cisplatin ? paclitaxel / docetaxel cisplatin ? 5 - fu ? paclitaxel cisplatin ? epirubicin paclitaxel ? bleomycin cisplatin ( 30 mg / m2 ) cisplatin ? 5 - fu carboplatin paclitaxel adjuvant cisplatin ? 5 - fu in arm a , 14 patients were treated with induction chemotherapy ( median , two cycles ) and 23 patients received concurrent chemotherapy , followed by adjuvant chemotherapy in ve patients . 
tolerance to concurrent chemotherapy was quite good : nine of 14 patients completed the three planned cycles of high - dose cisplatin and four of seven patients completed at least ve cycles of weekly dose cisplatin ve patients , amifostine was used before every rt session . in arm b , 19 patients were treated with induction chemotherapy ( median , two cycles ) followed by concurrent treatment , with good compliance : 13 of 16 patients completed three cycles of high - dose cisplatin and seven of eight patients nished at least ve cycles with weekly dose cisplatthree patients were given additional adjuvant chemotherapy ( table 3 )  . follow - up patients underwent weekly examinations during treatment . the rst follow - up evaluation occurred at 2 months and then every 36 months during the rst 2 years , every 6 months during years 35 and then annually with clinical examination and contrast - enhanced ct or mri , chest radiograms every year and thyroid function tests every year . 
acute and late toxicity was scored according to ctcae v3.0 ( common terminology criteria for adverse events ) and rtog / eortc ( radiation therapy oncology group / european organisation for research and treatment of cancer ) , respectively . statistics the endpoints were os , disease - free survival ( dfs ) , local control ( lc ) , locoregional control ( lrc ) , acute and late fig . 
1 overall survival in the two treatment arms 638 radiol med ( 2014 ) 119 : 634641 on multivariate analysis , age , gender , histology , t stage , n stage , tnm stage , rt technique , biological equivalent dose ( bed ) , high - dose ptv volume , fractionation schedule , overall radiation treatment time ( ott ) , timing of chemotherapy and comorbidities were evaluated and none was correlated with os , but tnm stage iii ( p = 0.021 ) ptv volume c275 ml ( p = 0.014 ) were statistically correlated to better dfs . high - dose there were no treatment - related deaths and no grade 4 acute toxicity . 
parenteral nutrition was necessary in one patient in arm a and in two patients in arm b and enteral feeding tube in two patients in arm a and in three patients in arm b . 
the median treatment interruption was 2 days in arm a and arm b ( range 012 days , the same in the two groups ) , with a median rt overall treatment time ( ott ) of 63.5 days in arm a ( range 4684 ) and 47.5 days in arm b ( range 4264 ) , because a programmed electron boost was administered to 23 patients after treatment with photons in arm a . late toxicity data were unknown for three patients ( two in arm a and one in arm b )  . 
at 5 years of follow - up xerostomia cg2 was 67 and 41 % for arm a and b , respectively ( p = 0.10 ) , chronic dysphagia cg2 was 17 and 12 % ( p = 0.81 ) , hearing loss cg2 was 29 and 35 % ( p = 0.22 ) and dysgeusia cg2 was 4 and 11 % ( p = 0.54 ) , respectively , for arm a and b . possible correlations between late toxicity and variables such as age , gender , stage of disease , high - dose ptv volumes , total radiation dose and fractionation , rt technique , timing of chemotherapy , amifostine use and severe acute toxicity were assessed . 
furthermore imrt was shown to be superior in terms of better target coverage and better sparing of organs at risk [ 11 , 12 ]  . in our study , the median age ( 53 years old ) and the male / female ratio ( 3.7 / 1 ) were the same as in most clinical trials [ 7 , 8 , 1115 ]  . 
in our there was no statistically signicant difference study , between standard and hypofractionated regimen , in terms of os , lc , acute and late toxicity . in our retrospective study , there was no signicant difference in os between 2drt / 3dcrt and imrt techniques , although a marginal survival benet could be expected with imrt because of the better dose distribution and the acceleration of radiation treatment . 
unfortunately , our sample size was too small and follow - up time was quite short in arm b to demonstrate any survival advantage . imrt use did not correlate with a signicant difference in lc , but a weak trend for better lrc was found . 
some data in favour of a better lc with imrt have been reported in the literature [ 20 ]  . in our study , almost all patients were treated with chemotherapy . 
in the treatment of nasopharyngeal cancer , the most recommended neoadjuvant therapy was a combination of two [ 14 , 21 ] or three [ 2224 ] cycles of cisplatin and 5 - fu , but in the literature associations of cisplatin with epirubicin [ 23 , 25 , 26 ] , bleomycin [ 27 ] or taxanes [ 28 , 29 ] are described . 
tpf chemotherapy ( cisplatin - paclitaxel - 5 - fu ) , which correlated with a survival benet in two trials on squamous head and neck tumours [ 30 , 31 ] , is being tested in ongoing international nasopharyngeal cancer trials [ gortec - npc2006 , nct00828386 ; nct01245959 ]  . 
in our study , 82 % of patients underwent induction chemotherapy , almost always two cycles , with a certain variety of schedules and doses ( table 3 )  . 
actually some reports suggested a benet in distant disease control [ 9 , 10 ] , but with potentially higher toxicity and difculty in completing an adequate concomitant phase . in the present study , 92 % of patients were treated with concurrent chemotherapy . 
in our practice , there is a large use of weekly dose cisplatin , due to its low toxicity , but there are some controversies about this schedule [ 3 , 13 , 15 ]  . globally , in our study , it was not possible to show any relationship between chemotherapy timing and patients outcome , but the biases were numerous : the use of several different drugs and schedules , the absence of a control group , the lack of formal restaging after induction , the low number of events and the inadequate number of cycles given after radiation therapy . reports , in historical the 5 - year survival rate was 4050 % with a lc of 6070 % before 1990 [ 32 , 33 ]  . 
in the 90s , improvements in imaging and the use of conformal rt combined with chemotherapy resulted in 5 - year survival rates of 75 % and lc rates of 85 % [ 34 ]  . 
after that , an increasing number of publications reported even better results with the use of imrt , despite the shorter follow - up time : lc up to 90 % and similar survival rates at 3 years [ 1820 , 3538 ]  . 
taking into account the different followup time , the results obtained in our institution compare quite well with those previously reported , particularly with studies using neoadjuvant [ 27 , 29 ] or concurrent and adjuvant chemotherapy [ 58 ]  . the outcome of our patients treated with imrt is similar to that reported in randomised and retrospective trials , suggesting the appropriateness of our practice in terms of radiation doses , target volume denition and chemotherapy . 
patients were staged iiiiv in 75 % of cases ; 70 % of patients were treated with induction plus concurrent chemotherapy and 20 % with concurrent chemotherapy only . no analysed factor was related to os or tumour control , but stage and volumes of ptv treated with high dose were related to dfs . 
in particular , the relationship between higher ptv volumes and a better dfs appears paradoxical . some elements could make this nding a little more sensible : rst , gtvs , ptvs and disease stage are linked in a nonlinear way ; second , ptv delineation is also related to the treatment technique ; third , there was an imbalance between treatment arms : patients treated with imrt also had larger planning treatment volumes and higher prescription doses . the acute toxicity rate in our sample is similar to that of clinical trials and retrospective surveys [ 4 , 11 , 12 , 16 , 18 , 19 ] , even if a underestimation is quite likely because of the retrospective collection of data . two randomised controlled trials [ 11 , 12 ] demonstrated the benet of parotid - sparing imrt in late xerostomia and stimulated salivary ow . 
with regard to late xerostomia , while in the absence of a signicant advantage with imrt , 640 radiol med ( 2014 ) 119 : 634641 our data are similar to those of other studies except for the typically , patients treated with parotid - sparing timing : imrt experience a recovery ; on the contrary late xerostomia after conventional rt is irreversible . 
in our cases , while in arm b , xerostomia had some stabilisation after the toxicity rate little more than 1 year of follow - up , increased with time in arm a , with an advantage that became more evident over time . our dosimetric data compared favourably with published studies : if in our series the mean dose to the spared parotid was about 32 gy , in the randomised study by pow et al . 
the parotid gland sparing imrt technique led to excellent results in terms of late xerostomia , although it was not possible to demonstrate a statistically signicant difference as compared to conventional and conformal rt . 
gemelli 8 , rome , rm , italy pseudoaneurysms and six cases of lower limb ischaemia . five of ten complications occurred in patients presenting calcication of the common femoral arteries , whereas 4 / 10 were in patients with complex groin anatomy . 
it has traditionally been performed 836 radiol med ( 2014 ) 119 : 835841 femoral artery access by surgical ( open , o - evar ) , although recently percutaneous femoral access ( p - evar ) has developed . 
this innovative technique became feasible with the advent of devices for percutaneous closure of large - bore arterial access sheaths , such as prostar xl ( abbott vascular , abbott park , il , usa ) [ 1 ]  . since the development of the totally percutaneous approach , many investigators have discussed the advantages of this technique [ 211 ]  . 
some authors demonstrated a complication rate of 820 % in unselected populations of patients who underwent o - evar [ 4 , 12 , 13 ] , whereas complications of p - evar account for 4.4 % [ 1 ]  . 
in the past , obesity , calcication of the common femoral arteries ( cfa ) , scars in the groin and a large introducer sheath size ( larger than 18 or 20 fr ) were considered to be contraindications to p - evar [ 2 , 3 , 6 , 911 , 14 ] , as they represent the main factors for technical failures . however , more recently , some authors have investigated the possibility to treat with p - evar even patients with obesity , severe calcication of cfa and scarred groin [ 1 , 4 , 8 ]  . the aim of this study was to evaluate the safety and feasibility of p - evar in an unselected population , including patients with calcication of cfa , scarred groin and also obese patients . 
technical success was dened as correct device deployment with closure of the arteriotomy , without the need of conversion to surgery . during each procedure , there were at least two operators , two nurses and one radiologic technologist . 
we performed an accurate dissection from the skin to the femoral arterial wall , by slightly enlarging the incision to allow the advancement of prostar xl deeper into the subcutaneous tissue . 
the guidewire was removed , and the device was advanced until adequate blood marking was achieved through the marker lumen , indicating that the sutures and the needles were inside the arterial lumen . 
1 pre - operative maximum intensity projection ( mip ) image of contrast - enhanced computed tomography ( ct ) scan a shows the presence of an abdominal aortic aneurysm in a 71 - year - old patient with tortuous , ectatic and calcied iliac arteries . 
post - operative mip image of contrast - enhanced ct scan b shows the correct deployment of device with successful exclusion of the abdominal aneurysm and regular patency of the stent grastents were also placed into the renal arteries . 
three - dimensional volume - rendered image ( c ) better depicts the position of aortic and renal stent grafts radiol med ( 2014 ) 119 : 835841 out after inserting a guidewire through the wire lumen . after placing the sutures of the prostar xl closure device , a large vascular sheath compatible with the stent - graft system was introduced into the artery ( sheath size ranged between 18 and 24 fr for the main body access site and between 12 and 18 fr for the contralateral limb access )  . then , the stent - graft system was deployed with a main body access site of 1824 fr and a contralateral limb access site of 1218 fr . 
thus , the sheath was removed , maintaining the guidewire inside the arterial lumen , and the sutures of the closure device were immediately tied using a sliding knot ( rst the white suture and then the green one )  . a knot pusher was used to ensure proper tightening of the knot and positioning of the knot near the vessel wall . patients received a bolus of 5 , 000 iu of heparin during the procedure . all patients were hospitalised for at least 2 days , they received elastic compression of the femoral artery , and they were kept at bed rest for 24 h . 
statistical analysis was performed using spss 12.0 for windows ( spss , chicago , il )  . results among the 200 consecutively enrolled patients , 123 / 200 ( 61.5 % ) were men and 77 / 200 ( 38.5 % ) patients were women . 
in 60 / 200 patients ( 30 % ) a complex groin anatomy was recorded , consisting of patients with a thick pannus in the groin , high femoral bifurcation , small femoral artery calibre or scarred groin from multiple prior catheterisations or surgical procedures . cfa calcications were identied in 144 / 200 patients ( 72 % ) by retrospective review of ct angiographies performed before intervention . 
the patients characteristics are listed in table 1 . the stent grafts used included : 170 zenith cook , three anaconda , six jotec , six lp zenith cook , 14 gore excluder and one ovation . 
we used one prostar xl closure device for each arterial access , except in ve cases which required placement of another device ( primarily because of difculties with nitinol needles and their sutures )  . 
four of ten complications occurred in patients with complex groin anatomy , showing a table 1 characteristics of 200 patients undergoing p - evar using the prostar xl closure device renal impairment : creatinine [ 1.4 mg / dl cfa common femoral artery patient demographics male sex obese renal impairment arterial hypertension 61.5 complex groin anatomy cfa calcications 838 radiol med ( 2014 ) 119 : 835841 fig . 
2 thrombosis of the common femoral artery ( cfa ) thrombosis occurred as an early complication ( few hours ) of p - evar in a 75 - year - old male . 
eight of ten complications ( 80 % of cases ) occurred in the access site of the main body of the prosthesis using a sheath size [ 20 fr , and two in patients with post - surgical scarred grofurther 2 / 10 complications ( 20 % of cases ) regarded the contralateral limb access , using a sheath size of 16 fr . 
no midand long - term complications related to the access sites were recorded during the follow - up period . discussion nowadays , p - evar is more attractive than traditional o - evar because of the wide range of advantages it offers . thanks to the advent of closure devices such as prostar xl , p - evar has become technically feasible , but today the main interest of the interventionist is focused on the patient population for whom it might be performed and on the safety of the technique itself . 
the possible benets of percutaneous closure of the femoral artery are a decreased number of wound complications , a more frequent use of local or regional anaesthesia , shorter operation and hospitalisation times and earlier patient mobilisation [ 10 ]  . 
these advantages of p - evar stand in contrast to the complications of o - evar , such as wound infection , wound dehiscence , lymphocele and haematomas [ 4 , 8 ]  . 
in particular , bleeding , inability to achieve haemostasis and lower limb ischaemia are the main endovascular complications which have been shown to require the conversion to surgery [ 14 ]  . the main end - point of our study was to assess the feasibility and safety of p - evar in a population of patients not selected by any clinical feature ( obesity , previous evar or groin surgery , peripheral arterial disease , type of treatmentelection or emergency ) or anatomical features ( calcications , diameter , groin anatomy and tortuous iliac arteries )  . 
previous studies have shown that severely or circumferentially calcied cfas , large introducer sheath size , scarred groins , obesity or morbid obesity , tortuous iliac arteries and operators inexperience with the procedure increase the likelihood of technical failures or complications [ 4 , 9 , 10 , 17 ]  . 
these risk factors , variously combined , were considered exclusion criteria for using percutaneous closure devices , but more recently a few studies using different percutaneous techniques began to include also patients presenting them [ 3 , 13 , 18 ]  . the technical success obtained in our study ( 100 % ) with an unselected population of patients , accompanied by a complication rate of 2.5 % in all femoral accesses , conrms the feasibility and safety of p - evar in all patients . radiol med ( 2014 ) 119 : 835841 in the literature , the technical success rate with percutaneous closure devices ranges from 66 to 100 % [ 2 , 4 , 8 , 10 , 17 , 19 ]  . 
 [ 1 ] reported that there is no statistically signicant difference in the percutaneous closure success rate between studies that considered all - comers and studies considering the most important exclusion criteria ( i.e. scarred groin and cfa calcications )  . 
in our study , we retrospectively reviewed the ct angiographies performed before the intervention , which revealed the presence of cfa calcications in 144 / 200 ( 72 % ) patients . 
these results show the safety of performing p - evar even on patients with cfa calcications , which are very common in subjects suffering from aortic aneurysms . as regards scarred groins , we experienced two cases of complications in these patients , although it is impossible to determine the concomitant role of larger sheath access size ( [ 20 fr ) used in this subset of patients . 
the majority of complications ( 8 / 10 , 80 % ) reported in our series occurred using sheath size larger than 20 fr , representing 7 % ( 8 / 114 cases ) of all access sites [ 20 fr . 
future advances in stent - graft design will allow for smaller delivery systems , resulting in a possible reduction in the inuence of sheath size on technical failures . however , large sheath size is not the only factor to be considered , as in our experience 2 / 10 complications ( 20 % ) occurred in the contralateral limb access ( 2 / 200 contralateral accesses , 1 % ) , using a sheath size of only 16 fr . 
an accurate dissection from the skin to the femoral arterial wall is fundamental to eliminate all possible brous bands of scar tissue and avoid incorrect device deployment . furthermore , it is very important to tie the sutures of the closure device using an accurate sliding knot , avoiding many loops around the rail end of the suture and allowing sliding of the non - rail end through a loop . 
as reported in other studies [ 2 , 17 , 22 ] , there is a learning curve associated with the use of these closure devices , which may explain the technical errors and the complications that occurred in the initial phase of our experience . 
even if it is not easy to quantify a precise number of interventions to become condent with prostar xl , we hypothesise that 3040 procedures should be performed . in our opinion , a key factor for a successful procedure is the patients groin anatomy . 
indeed , in our series , we observed 4 / 10 ( 40 % ) complications in subjects presenting with a complex groin anatomy , showing a statistically signicant difference between patients with complex groin anatomy and those without overall incidence of complications is very low ( 4 / 200 ; 2 % ) and not signicant in terms of safety of the procedure . 
however , complications in our series , we observed different kinds of complications , including six cases of lower limb ischaemia ( 5 / 6 after a few hours and 1 / 6 after a few days in a patient with peripheral arterial disease ) and four pseudoaneurysms ( 4 / 10 complications , 40 % )  . 
two of ve cases of early lower limb ischaemia occurred in patients with small femoral artery calibre ( complex groin anatomy ) coarse cfa calcications . patients with pseudoaneurysms were treated conservatively ( with usguided compression )  . 
thus , p - evar performed in unselected populations of patients constitutes a feasible and safe procedure that does not require specic selection criteria . furthermore , we recorded this low complication rate among 200 patients , a sizeable population if compared to other published studies . comparing our access - related complication rate with the best o - evar studies published in the literature [ 1 ] , our results demonstrate the attractiveness of p - evar . 
in fact , the o - evar approach for aortic aneurysm repair may be burdened by several complications , such as infection , thrombosis , pseudoaneurysm arterial dissection , arterial lymphoceles and femoral formation , groin haematoma , nerve injury , which occur in up to 14 % of patients and are probably related to the injury that the lymphatic and arterial vessels suffered during the procedure [ 14 , 25 , 26 ]  . some authors have reported a local complication rate between 8 and 20 % in patients who underwent o - evar [ 8 , 2730 ]  . 
the only prospective randomised trial published in the literature comparing the results of o - evar versus p - evar showed a lower complication rate at the access site in the percutaneous group [ 8 ]  . furthermore , o - evar has a much longer and more uncomfortable post - operative stay than p - evar [ 27 , 31 , 32 ] with a longer time to ambulation [ 8 , 27 ]  . 
patients might benet from p - evar time - saving , which may lead to considerable cost reductions for hospitals , in terms of staff resource use and expenses [ 33 ]  . 
costs should be included in a global evaluation of the differences between the two procedures ( o - evar and p - evar ) [ 1 , 31 ] and should include costs of devices and costs of hospitalisation ( procedure time , time to discharge and time to ambulation )  . 
 [ 33 ] found a signicant reduction in total procedure time ( approximately 1 h ) using the prostar xl device compared to surgical cut - down . however , to date , no evidence has been reported on the cost - effectiveness of the prostar xl device compared with surgical cut - down [ 33 ]  . the main limitation of our study is represented by the absence of a control group undergoing o - evar , with subsequent lack of comparison between the two procedures in terms of complications and overall costs . 
however , most published studies about the evar technique were retrospective or prospective non - randomised , with only one randomised controlled trial [ 8 ] ; this should be considered when interpreting results . 
further studies are needed to clearly compare p - evar with o - evar , focusing not only on the cost - effectiveness of prostar xl but also on the operators learning curve . conclusions percutaneous endovascular aneurysm repair in unselected populations is safe and efcient , with a very low risk of access - related complications , comparable to p - evar in selected populations and to the best o - evar series . important complex groin anatomy represents the most factor in the occurrence of complications , though the overall complication rate is very low . the operators experience and their mastery in the use of the prostar xl device are essential for successful outcomes . 
the results obtained in this study need to be conrmed with prospective randomised trials . conict of interest all the authors , sergio petronelli , maria teresa zurlo , silvia giambersio , lucia danieli , mariaelena occhipinti , declare no conict of interest . ethical standard all procedures followed were in accordance with the ethical standards of the responsible committee on human experimentation ( institutional and national ) and with the helsinki declaration of 1975 , as revised in 2008 . 
technical success , diagnostic accuracy , sensitivity , specicity , positive predictive value ( ppv ) , negative predictive value ( npv ) and complications were evaluated . results of 100 nodules ( mean size 5.19 cm ) , 68 were diagnosed as malignant , 27 as benign , and ve as indeterminate . 
only 33 of 100 patients underwent surgery : the nal pathological diagnosis was concordant with the biopsy diagnosis in 26 cases and discordant in 7 cases ( false negatives )  . 
rotolo center for thoracic surgery , university of insubria , viale borri 57 , 21100 varese , italy conclusions cbct - xperguide navigation is a new , accurate and safe imaging guidance for percutaneous lung biopsies . keywords c - arm cone - beam ct ( cid : 2 ) percutaneous lung biopsy ( cid : 2 ) pulmonary nodule introduction percutaneous transthoracic needle biopsy of lung nodules with image guidance is a safe and accurate diagnostic technique for assessing their benign or malignant nature [ 1 , 2 ]  . 
the use of computed tomography ( ct ) as image guidance does not allow the visualisation of the needle insertion in real time , unless it is carried out using ct uoroscopy ( uoro - ct ) [ 3 ]  . 
cone - beam ct ( cbct ) is a recently developed imaging technique available in c - arm angiography systems equipped with a at - panel detector integrated with a cone beam x - ray . 
the system produces images similar to those of ct providing the operator with the possibility of real - time uoroscopy visualisation and it offers a greater exibility in the orientation of the detector around the patient compared to the closed ct gantry . 
coupled with cbct it is also available a navigation software , vendor specic ( xperguide , philips healthcare , best , the netherlands ) which allows the operator to direct the needle in real time with uoroscopy , once the trajectory has been established by the images acquired in 3d cbct . 
the study was approved by the ethics committee of our hospital and before any procedure patients were adequately informed on the procedure and any possible complications , and all of them signed the informed consent forall patients had undergone a chest ct at our institution or elsewhere which was evaluated by the operator before the procedure to determine the feasibility of the biopsy . 
in particular , the size , location and distance from the pleura were determined for each lesion ( table 1 )  . technical execution all lung biopsies included in the study were performed in the angiography suite equipped with a c - arm cbct system ( philips allura xper fd20 , philips best , the netherlands ) and a dedicated software programme xperguide ( philips healthcare , best , the netherlands )  . 
in particular , with the aid of the xperguide software on the workstation monitor , the radiologist or trainee radiologist established the target point in the context of the lesion ( target point ) and the access point of the needle on the cutaneous plane ( entry point )  . 
1 first cone - beam computed tomography ( cbct ) scan to dene lesion location position of the angiographic c - arm to display the entry point of the needle on the patients skthis phase of the procedure , followed by the angiographic c - arm positioning in the angiography suite was called entry point position . after disinfection of the skin at the area of access and local anaesthesia ( 10 cc of 2 % mepivacaine , angelini , rome , italy ) , via uoroscopy the operator positioned the tip of the needle on the patients skin at the entry point following the cbct image that appeared on a dedicated monitor as a fusion image of the 3d volume previously acquired with cbct and the bi - dimensional plane obtained with realtime uoroscopy . 
3 second sagittal cbct scan to evaluate the correct positioning of the needle if correctly positioned , previously determined and displayed in real time , under uoroscopy on the dedicated monitor . 
in all cases , we used a 20 - gauge trocar ( biopsy bell , medical device , modena , italy ) as a biopsy needle . finally , at the end of the procedure , a third and nal scan was acquired to assess the presence of any complications fig . 
at least 4 h after the biopsy , on advice of the radiologist , a chest x - ray in posteroanterior and maximum expiration projection was performed to highlight possible pneumothorax . data analysis we calculated the rates of technical success , diagnostic accuracy , sensitivity , specicity , positive predictive value ( ppv ) and negative predictive value ( npv )  . 
true positive ( tp ) results were dened as biopsy results of a malignant lesion that agreed with the denitive histological ndings in patients undergoing surgery or with the results of the follow - up ( disease progression or response to radio - chemotherapy established by an oncologist ) in patients not undergoing surgery . 
true negatives ( tn ) were biopsy results of benign disease ( tumour , specic or nonspecic inammatory reaction , brotic tissue ) which resolved or remained unchanged during the follow - up . 
false negatives ( fn ) were patients in which the histological table 2 sir ( society of interventional radiology ) classication of complications table 3 results of cone - beam computed tomography ( cbct ) xperguide percutaneous transthoracic needle pulmonary biopsies radiol med ( 2014 ) 119 : 820827 minor complications ( a ) no therapy , no consequence ( b ) minimal therapy , no consequence major complications ( c ) need therapy , minor hospitalisation ( d ) need major therapy , long hospitalisation ( [ 48 h ) ( e ) permanent sequelae ( f ) death results of the biopsy sample were negative for malignancy and thus were discordant with the examination of the surgical specimen , which instead documented malignancy . complications were classied into major and minor according to the sir classication ( society of interventional radiology ) [ 5 ] ( table 2 )  . 
finally , the technical success rates , diagnostic accuracy , sensitivity , specicity , ppv , npv and complications were analysed by subdividing the data into two subgroups according to lesion size ( b3 and [ 3 cm )  . calculation of radiation dose the dose calculation method with cbct was carried out in collaboration with our hospitals medical physicists . 
the data were acquired through the application of dosimeters on the surface of a phantom ( rando phantom , model ran 10 , churchin associates , smithtown , ny , usa ) and using the pcxmc software ( version 2.0 ) according to the icrp [ 6 ]  . 
depending on the site of the lesion and the patients position ( x - ray tube as close as possible to the lung lesion ) , either a lr or rl projection was chosen . 
a single arc was divided into 43 steps of 5 ( cid : 3 ) each , and the calculation was made by taking into account the patients position ( supine or prone )  . 
forty - four lesions had a diameter b3 cm and 56 a diameter [ 3 cof the 100 lung lesions biopsied using cbct with xperguide software , 68 were diagnosed as malignant and 27 as benign . 
the features and size of the lesions in which the bioptic sample was not diagnostic were : three lesions located in the left upper lobe with the greatest transverse diameter of 9 , 16 and 30 mm ; two lesions located in the right lower lobe with a diameter of 55 and 32 monly 33 / 95 lesions were subjected to surgical resection . 
the 62 cases that were not subjected to surgery underwent clinical and radiological follow - up in collaboration with colleagues from the departments of internal medicine and surgery ( range 126 months ; mean followup period , 14 months )  . 
among the 33 patients who underwent surgery , 24 / 33 patients had malignant disease according to the analysis of the surgical specimen , agreement with the biopsy results ( tp ) , and two patients had benign pathology ndings ( hamartoma and chronic inammation , tn )  . 
these seven cases were judged false negatives ( fn ) , considering the histological examination of the surgical specimen showed the presence of primary or secondary malignant lung lesions ( adenocarcinoma , squamous cell carcinoma , a small cell lung tumour , a sarcomatoid carcinoma , three metastases )  . 
among these patients , the biopsy results revealed the presence of an inoperable malignant lesion in 44 cases ( tp , 26 adenocarcinomas , ve metastases , two carcinoids , four sarcomatoid carcinomas , four squamous cell carcinoma , two small cell lung tumours and one mesothelioma )  . 
there were 18 benign lesions ( seven bronchopneumonia , ve brous tissues , three nonspecic inammation , one tuberculosis and one round atelectasis )  . all 18 patients with benign lesions underwent clinical and radiological follow - up . 
in particular , the radiological follow - up ( range 1226 months , median 15 months ) documented lesion regression in 11 / 18 cases and no change in 7 / 18 cases ; in agreement with the clinical data provided by the clinicians , these cases were all considered true negatives . 
overall diagnostic accuracy was 92.6 % , the sensitivity was 90.9 % , the specicity was 100 % , the ppv was 100 % and the npv was 72 % . 
there were no major complications , while the overall rate of minor complications ( pneumothorax ) was 21 % ( 20 / 95 ) : eight cases of discussion over the last 30 years , numerous studies have demonstrated the diagnostic accuracy and safety of percutaneous transthoracic lung biopsies [ 811 ]  . 
published studies describing the technical aspects of lung biopsies with imaging guidance [ 8 , 9 , 12 ] point out that , despite the different guide used ( uoroscopy , ultrasound , multislice ct , uoro - ct , cbct , cbct with xperguide navigation software ) , the results obtained also depend on the learning curve and , consequently , on the level of condence gained over time by the operator . 
the authors showed that for supercial and voluminous lesions uoroscopic guidance alone may still be usable , having the advantage of exposing the patient to a lower radiation dose ( about 7 times lower than the dose measured in patients undergoing cbct - guided lung biopsy )  . 
other authors performed several studies using ct guidance , demonstrating the safety and diagnostic accuracy for benign and malignant lesions of the chest [ 1 , 11 , 14 ] ; in particular , li et al . 
the authors showed that the diagnostic accuracy for lung biopsies under ct increased signicantly in lesions [ 10 mm and in cases in which the route of the needle from the skin to the lesion was b40 mcurrently , the gold standard technique used to guide percutaneous biopsies of pulmonary nodules is uoro - ct , which is able to follow the progression of the needle from the skin to the target in real time [ 15 ]  . 
compared to conventional ct , uoro - ct allows monitoring of the progress of the needle radiol med ( 2014 ) 119 : 820827 with a smaller number of steps compared to procedures that use the conventional ct guidance [ 12 ]  . 
however , uoroct can lead to higher radiation doses to the patient and to the operator , and it is not available in all radiology services [ 14 , 16 , 17 ]  . 
 [ 15 ] published the result of 99 lung biopsies performed with uoro - ct guidance in 85 patients , reporting accuracy , sensitivity and specicity rates of 96 , 95 and 100 % , respectively , with a complication rate of 26 % . 
these results not only conrmed that the diagnostic accuracy of lung biopsies with uoro - ct guidance was comparable to that of lung biopsies performed under simple ct guidance , but also showed that uoro - ct guidance was indicated especially in small lesions , in which a high complications was diagnostic obtained . 
 [ 22 ] showed that cbct is as reliable as ct an imaging guidance technique in percutaneous interventional procedures because they demonstrated , in a phantom model , that ct and cbct have a similar sensitivity in detecting parenchymal nodules . 
a retrospective analysis showed that two of these four lesions had dimensions of b2 cm and were biopsied in the initial phase of the learning curve and in the other three cases ( lesions c3 cm ) the needle was placed in a peripheral area of the lesion , where necrotic tissue was sampled . excluding the ve nondiagnostic cases , the sensitivity , specicity , accuracy , ppv and npv were 90.9 , 100 , 92.6 , 100 and 72 % , respectively . 
lesion size did not affect the quality of the diagnostic results and safety of the method , as is clear from a comparison of the overall data with those of the two groups of patients divided by lesion size ( b3 and [ 3 cm ) , which showed no signicant differences . 
in the past 2 years , several studies have been published reporting the results obtained in lung biopsies with the guidance of cbct alone [ 13 , 2326 ] and cbct associated with the proprietary xperguide navigation software [ 22 , 2729 ] ( table 5 )  . 
 [ 23 ] reported an initial experience of needle biopsies of 71 pulmonary nodules all b3 cm using cbct guidance alone without navigation : their technical success rate was 100 % , with good sensitivity , specicity and accuracy ( 97 , 100 and 98.4 % , respectively )  . 
on the basis of our results and the data from the literature regarding lung biopsies performed with cbct guidance with or without the aid of the xperguide software , despite the limited amount of currently available data and the lack of homogeneity , a slight reduction in dose could be hypothesised with the use of xperguide guidance . in our opinion the use of xperguide software in cbct guided lung biopsies could reduce the total dose delivered because it can reduce the number of cbct scans needed , by allowing greater precision in the approach to lesion sampling . study has some limitations that need to be acknowledged : the biopsy results of 5 out of 100 nodules were not diagnostic at histological examination ; the followup of patients undergoing surgical verication was not homogeneous ( range 126 months , mean 14 months ) ; nally , the radiation dose was exclusively calculated on the patients and not directly on the operator . 
however , we can 826 radiol med ( 2014 ) 119 : 820827 conclude that in lung biopsies performed using cbct with the aid of the xperguide navigation system the results could be almost similar to those of uoro - ct as concerns the technical success , diagnostic accuracy and complications . 
for cases with the above - mentioned features , we suggest that the higher recurrence rate can be taken into full consideration when choosing appropriate surgical procedures . keywords giant cell tumour ( cid : 2 ) curettage ( cid : 2 ) recurrence ( cid : 2 ) magnetic resonance introduction l . 
197 , ruijin 2nd road , shanghai 200025 , china giant tumour of bone ( gctb ) is a benign bone lesion most often found in the extremities of bones [ 1 , 2 ]  . 
tumours arise in the meta - epiphyseal region of long bones , predominantly in the distal femur and the proximal tibia , but they can occur in the entire skeleton [ 2 ]  . 
histologically , these tumours are classied as a benign neoplastic lesion consisting of three cell types : mononuclear histiocytic cells , multinucleated giant cells that resemble osteoclasts , 862 and neoplastic stromal cells [ 3 ]  . 
en bloc resection has been recommended for aggressive tumours [ 2 ]  . although complete removal of the lesion provides a low recurrence rate , wide resection requires complex reconstruction of the adjacent joints , which increases the rate of surgical complications and disabilities [ 4 , 5 ]  . 
nevertheless , the recurrence rate remains relatively high [ 4 , 6 , 7 ]  . risk factors for local recurrence of gctb after intralesional curettage have been previously studied in depth [ 1 , 8 11 ]  . 
some studies demonstrated that demographic factors ( age , gender ) and disease - related factors ( location , pathological fractures and soft tissue extension ) did not inuence the risk of recurrence [ 1 , 8 ]  . 
however , van der heijden [ 12 ] reported that soft tissue extension strongly increased the risk of local recurrence , whereas age , sex , location and pathological fractures did not . 
the prognostic relevance of soft tissue extension of gctb remains controversial [ 8 ]  . magnetic resonance imaging ( mri ) appears to be more sensitive than computed tomography ( ct ) and radiography in detecting soft tissue extension of gctb for its excellent soft tissue contrast which allows for easier identication of the tumour and its extent . 
in addition , mri can provide visualisation of the number and margins of soft tissue extension and involvement of adjacent tissues , as well as depicting liquefaction and necrosis with the use of intravenous gadolinium injection [ 812 ]  . to our knowledge , all previous studies investigated the soft tissue extension of gctb as one of risk factors for local recurrence . 
in this study , we focused on the soft tissue extension of gctb , with a view to identifying some characteristics that can serve to indicate the recurrence of gctb after intralesional curettage . patients and methods database a total of 48 patients ( 22 women and 26 men ; average age , 30 years ; range 1646 years ) were consecutively enrolled in this study from january 1998 to june 2011 . 
all patients underwent table 1 location of giant cell tumour of bone ( gctb ) with soft tissue extension in 48 patients radiol med ( 2014 ) 119 : 861870 location no . 
of patients distal femur proximal femur femoral shaft distal tibia proximal tibia proximal humerus distal radius sacrum total intralesional curettage with pmma ( polymethylmethacrylate ) , which is the preferred standard treatment for gctb in our hospital , and were all followed up for over 2 years . recurrence occurred in 16 ( 33.33 % ) of the 48 cases . 
the mr examinations were carried out after the patients had been fully informed about the procedure and had given their consent . informed consent was also obtained from all patients for the use of all clinical and imaging data for this study . mr protocols fat - suppressed fast all mr examinations were performed using a 1.5 - t superconducting whole - body imager ( signa , general electric medical system ) with dedicated extremity coils or body phased - array coils . 
all measurements were performed on a postprocessing workstation ( ge healthcare )  . the following sequences were obtained : spin - echo t1weighted ( tr range / te range , 450 - 600 / 15 - 20 ) , fast spinecho t2 - weighted ( tr range / te range , 3500 - 4000 / 80spin - echo t2 - weighted ( tr 120 ) , range / te range 3 , 5004 , 000 / 80120 )  . 
when the volume of soft tissue extension exceeded 50 % of the volume of whole tumour , we dened the soft tissue extension as being large . finding size large small number multiple single margins adjacent tissue involvement with bone envelope integrity without bone envelope integrity signal intensity characteristics t1 : low , homogeneous t1 : intermediate / low , heterogeneous t2 : high , homogeneous t2 : intermediate / high , heterogeneous static enhancement homogeneous enhancement heterogeneous enhancement jaffe grade grade i grade ii grade iii soft tissue extension size of tumour and soft tissue extension the size of gctb and soft tissue extension was measured directly on the contrast - enhanced mr images which best depicted thethe diameters of both the tumour and the soft tissue extension were recorded in three axes : anterioposterior , transverse , and craniocaudal . 
the volume of each tumour and soft tissue extension was calculated using the standard equation for the volume of an ellipsoid : v = ( 4p / 3 ) xyz , in which x , y , number when the number of soft tissue extensions was greater than or equal to two , and the extended soft tissues were isolated in consecutive images , we dened the nding as multiple soft tissue extensions . 
when there was only one soft tissue extension , we dened it as a single soft tissue extension . when the extended soft tissue was expressed as a mass with several lobules , we also dened it as a single soft tissue extension . adjacent tissue involvement ( such as muscle , the absence or presence of adjacent soft tissue involvement ligament , capsula articularis ) , dened as abnormal signal intensity areas and foci ( low on t1 - weighted images and high on t2 - weighted images with fat suppression ) was determined . soft tissue extension margins cortical breach around the soft tissue extension was established when outer cortical integrity was disturbed by the presence of abnormal signal intensity . 
if continuity of the band of low signal intensity on mr images attributed to marginal scleroses was completely broken off , we dened the bone envelope around the extended soft tissue as not having integrity . signal intensities of soft tissue extension relative to muscle on spin - echo t1 - weighted and t2 - weighted images ( higher , equal , or lower ) were determined . static enhancement the pattern of soft tissue extension enhancement on t1weighted gadopentetate dimeglumine - enhanced images ( homogeneous or heterogeneous ) was recorded . jaffe grade gctb was originally described by jaffe et al . 
 [ 13 ] , who classied the tumour into three categories : grade i ( benign ) without appreciable atypia of stromal cells , few mitoses , none abnormal ; grade ii ( intermediate ) with stromal cells showing only slight or more marked atypia , but not enough to justify a diagnosis of malignancy ; and grade iii soft tissue extension was dened as a complete breakthrough of the cortex and additional extension into adjacent soft tissue [ 12 ]  . signal intensity characteristics 864 radiol med ( 2014 ) 119 : 861870 ( malignant ) with obvious features of malignancy . 
on completion of the retrospective review , the mr images were correlated with surgery results . data analysis analysis of the local recurrence rate of gctb with soft tissue extension considered seven aspects including soft tissue extension size , number , margins , adjacent tissue involvement , signal intensity characteristics , static enhancement and jaffe grade . 
when gctb had large soft tissue extension , multiple soft tissue extensions and lacked integrity of the bone envelope around the extended soft tissue , the local recurrence rate after intralesional curettage was higher . 
there was no statistically signicant difference in the groups of adjacent tissue involvement and jaffe grade . giant cell tumour of bone is a benign bone lesion most often found in the extremities of bones [ 1 , 2 ]  . 
tumours arise in the meta - epiphyseal region of long bones , predominantly in the distal femur and the proximal tibia , but they can occur in the entire skeleton [ 2 ]  . 
surgery is the mainstay of for gctb . although en bloc resection provides a low recurrence rate , wide resection requires complex reconstruction of the adjacent joints , which increases the rate of surgical complications and disabilities [ 4 , 5 ]  . 
2 20 - year - old man with gctb with two soft tissue extensions at the sacrua coronal t1 - weighted image shows the soft tissue has low / intermediate signal intensity on t1 - weighted image . 
the image also shows high signal intensity of adjacent tissues around the soft tissue extension . c axial contrast - enhanced t1 - weighted image with fat suppression tissue extension . shows heterogeneous enhancement of the soft d sagittal contrast - enhanced t1 - weighted image with fat suppression shows the two soft tissue extensions . 
some studies demonstrated that demographic factors ( age , gender ) and disease - related factors ( location , pathological fractures and soft tissue extension ) did not inuence the risk of recurrence [ 1 , 8 ]  . 
however , van der heijden [ 12 ] reported that soft tissue extension strongly increased the risk of local recurrence , whereas age , sex , location and pathological fractures did not . 
in this study , we focused on soft tissue extension , to assess the relationship between soft tissue extension of gctb and the recurrence rate after intralesional curettage . there were signicant differences among the groups of size , number , and margins of soft tissue extension . 
the reason might be that for gctb with large or multiple soft tissue extension and lack of bone intralesional curettage proves to be envelope integrity , technically more difcult , and is less likely to completely remove the whole tumour . 
3 35 - year - old woman with gctb with two small soft tissue extensions at the femoral shathe case did not develop recurrence . a , b axial contrast - enhanced t1 - weighted images show two small soft tissue extensions with homogeneous enhancement ( arrow )  . 
on t2 - weighted images , the signal intensities tend to be between those of muscle and fat . most lesions are inhomogeneous due to bleeding , liquefaction and necrosis especially in large soft tissue extension . 
jaffes grading system proved to be difcult to apply in practice and was unable to predict the clinical behaviour and prognosis of gctb [ 16 ]  . 868 radiol med ( 2014 ) 119 : 861870 fig . 
ac axial spin - echo t2 - weighted image with fat suppression , t2 - weighted image , and t1 - weighted image show cortical breach around the soft tissue extension ( arrow )  . 
f photomicrograph of the soft tissue extension shows a number of osteoclast - type giant cells and mononuclear stromal cells ( haematoxylin and eosin 9250 )  . jaffe grade ii intralesional curettage is the least invasive surgical option and usually provides the possibility to save the joint adjacent to the tumour [ 17 ]  . 
intralesional curettage may be combined with the use of local adjuncts , such as pmma void lling , hydrogen peroxide , phenol , and cryotherapy [ 9 , 17 , 18 ] with the intention to further reduce the risk of local recurrence . 
we tissue speculated that extension received intralesional curettage , the recurrence rate would be higher . if all gctb patients with soft tissue extension , multiple soft based on these ndings , we can conclude that gctb with large soft tissue extensions and lacking bone envelope integrity have an increased risk of intralesional curettage . recurrence after local several limitations of this study should be mentioned . first , only a small number of patients were evaluated , which limited the power of the statistical results . 
more patients and multi - institutional studies are necessary for a conrmation of the results with additional statistical power . second , we found that several objective features may appear in one case , such as gctb with large soft tissue extension , mr images of adjacent tissue involvement and a lack of bone envelope integrity . 
we did not analyse the interrelation of objective features because of the small radiol med ( 2014 ) 119 : 861870 table 3 comparison of recurrence rate in each group objective features no . 
 [ adjacent ] represents the adjacent soft tissue involvement around the soft tissue extension * signicant statistical difference ( p \ 0.05 ) the denition and concept of number of cases . 
fourth , we did not sufciently investigate the relationship between histopathological changes and characters on mr images of gctb with soft tissue extension , especially as regards changes of adjacent soft tissue involvement in explaining the mr signal changes . 
fifth , although we found that the local recurrence rate was higher if gctb had large soft tissue extension , multiple soft tissue extensions and a lack of bone envelope integrity , we failed to investigate whether there were any other reasons which might affect the recurrence rate following intralesional curettage . 
this study could provide new clues to identify the characteristics of the soft tissue extension that might best predict recurrence of gctb after intralesional curettage . conclusions in summary , the recurrence rate of gctb with soft tissue extension is higher when the extended soft tissue is large , multiple and lacking bone envelope integrity after intralesional curettage . 
the aim of this study was to compare colonic transit time with radiopaque markers and defaecography in female patients with obstructed defaecation . materials and methods in a prospective observational study , between january 2010 and december 2012 , a total of 30 female patients , mean age 60 years , with symptoms of obstructed defaecation were subjected to colonic transit time and defaecography , and divided into two groups : normal or abnormal colon transit time . 
the results were statistically compared using the chi - square test . results the comparison of data between colonic transit time and defaecography showed the following groups : group 1 ( 6 / 30 = 20 % ) with normal colonic transit time but abnormal defaecography , and group 2 ( 24 / 30 = 80 % ) with abnormal colonic transit time ; the latter was further divided into two subgroups : group 2a ( 4 / 24 = 17 % ) , patients with inertia coli ; group 2b ( 20 / 24 = 83 % ) , m . 
beati dipartimento di scienze chirurgiche , unita` di colo - proctologia , ospedale san carlo borromeo , via pio ii , 3 , 20153 milan , italy patients with impaired defaecation demonstrated at defaecography . 
there was a signicant statistical difference between the radiological ndings in these groups . conclusions this study conrmed the value of both defaecography and colonic transit time in assessing clinically obstructed women . 
the differential diagnosis between colonic slow transit constipation and constipation due to pelvic oor disorders is essential for an adequate strategy of care . keywords colonic transit time ( cid : 2 ) defaecography ( cid : 2 ) constipation ( cid : 2 ) obstructed defaecation introduction normal defaecation requires normal colonic motility ( colonic transit ) , anorectal sensation , expulsion force and a coordinated function of the pelvic oor to evacuate [ 1 ]  . chronic constipation is the second most commonly reported disorder in the western world with an estimated incidence of 20 % [ 2 ] , and it represents a signicant economic burden , often compromising the quality of life [ 3 ]  . 
constipation can be considered not only a disease , but a symptom related to delay in passing of stools . primary constipation can be divided into two forms : constipation due to delayed colonic transit : slow progression of faecal material in the transverse and descending colon . constipation due to pelvic oor dysfunction / alteration , characterised by difculty in expelling the accumulation of stools in the rectum [ 4 ]  . 814 radiol med ( 2014 ) 119 : 813819 table 1 rome iii diagnostic criteria for functional defaecation disorders 1 . 
the aim of this study was to compare colonic transit time with radiopaque markers and defaecography in female patients with obstructed defaecation . materials and methods patients between january 2010 and december 2012 , a total of 30 female patients ( mean age 60 years , range 2986 years ) with symptoms of constipation potentially candidate to surgery were included in this study . 
the surgical procedure may involve a transanal approach like starr , transstarr , or delorme technique in patients with obstructed defaecation or an abdominal approach such as subtotal colectomy with ileorectal anastomosis in patients with severe slow colonic transit time . 
any change in the colonic distribution of markers may indicate one of three patterns of colonic hypomotility : colonic inertia , hindgut dysfunction , or outlet the results of marker studies have obstruction . 
thus , practical consequences in the clinical management of patients with chronic constipation [ 12 ]  . thirty radiopaque markers ( these are inert and nondigestible , radiopaque cylinders 3.5 mm in diameter ) are administered to the patient and the transit is monitored after 24 h and at the fth day by plain abdominal x - ray . the markers are located and counted on the abdominal radiographs with bony landmarks and clear bowel outlines ( spinal processes and imaginary lines from the fth lumbar vertebra to the pelvic outlet serving as landmarks , dened projection zones of the right and left colon and rectosigmoid ) [ 12 ]  . a transit time corresponding to the evacuation of at least 90 % of the markers is assumed to be considered normal ; the retention of more than 20 % of the markers was indicative of slow transit time according to bouchouca et al . 
at least three subtypes of slow colonic transit were identied by colonic transit times , measured on the basis of the distribution of markers visible on abdominal radiographs , although there may have been an overlap between these subtypes : colonic transit is slow , the major site of delay being the ascending colon ( colonic inertia ) ; the delay is predominantly found in the descending colon ( hindgut dysfunction ) ; and marker retention is visible mainly in the rectosigmoid area ( outlet obstruction )  . 
the overlap between patterns of colonic hypomotility may be due to the dysfunction of a colonic segment or to distal faecal impaction , which can cause nonpropagation or backpropagation of the markers [ 14 ]  . the stagnation prevailing in the right colon argues in favour of a signicant alteration of colonic motility ( colonic inertia or functional constipation ) with a prolonged intestinal transit of stools . defaecography defaecography is a morphodynamic examination that simulates the act of defaecation and evaluates some disorders of the rectum and the pelvic oor [ 15 , 16 ]  . 
the entire examination is recorded on videotape and each video clip is analysed using a computer video capture and digitising system combined with an image analysis programme [ 19 , 20 ]  . without any prior bowel preparation , ileal opacication is obtained after oral intake of 300 ml of dilute barium suspension at 60 % ( prontobario 60 % bracco s.p.a. milan , italy ) approximately 3060 min before the examination , opacication of the vagina is obtained with a swab impregnated with iodinated contrast medium to demonstrate the effect of defaecation on the posterior vaginal wall , and rectal ampulla opacication with 180 ml of thick barium sulphate paste of a consistency similar to faeces , injected with a syringe with the patient in the left lateral position . defaecography was divided into pre - evacuation , evacuation and post - evacuation stages and so an anteroposterior radiograph was taken with the patient at rest in the supine position with a focus on the ampulla lled with barium ; after that , ve lateral radiographs were taken : at rest with the patient seated on a comfortable dedicated device in the standard seated position , which is considered more physiological . 
the uoroscopic table is moved into the upright position ; a single latero - lateral radiographic lm is then obtained to document the rectum and pelvic oor conguration at maximum contraction ( on voluntary contraction of the pelvic oor muscles ) and at straining ; a videouorographic recording ( a videotape recorder is also used to allow a good dynamic observation of evacuation ) is obtained at evacuation and a nal image after evacuation . fluoroscopy images were recorded during several such manoeuvres to assess and measure the descent of the pelvic oor and to diagnose any rectocele , enterocele or rectal intussusception . 
perineal descent was determined by measuring the level of the anorectal junction at rest and during straining and was dened as either descent of the anorectal angle ( it was measured at the intersection of the axis of the anal canal and rectal ampulla ) to more than 2 cm below the pubococcygeal line at rest or descent to more than 3 cm below the pubococcygeal line on straining . an enterocele was dened as descent of the small bowel below the pubococcygeal line . 
rectal intussusception was dened as a circumferential descent of the entire thickness of the rectal wall without passing through the anal canal [ 1621 ]  . the examination was considered normal if none of these alterations were present . 
the chi - square test was used for statistical analysis of the colonic transit time an defaecography results . 816 results incomplete the main disorders reported by patients were : reduced frequency of evacuation with multiple unsuccessful attempts ; evacuation efforts ; manual manoeuvres to void ( endorectal or endovaginal ) ; prolonged use of laxatives and enemas for which the patients have complained progressive loss of effectiveness . 
the risk factors for pelvic oor dysfunction include pregnancy , multiparity , advanced age , menopause , obesity and any other factors that result in a chronic rise in intraabdominal pressure . 
4 defaecographic signs in patients with normal ( 6 / 30 ) and abnormal colonic transit time ( 24 / 30 ) , the latter divided into patients ( 4 / 24 ) with inertia coli and patients ( 20 / 24 ) with impaired defaecation gynaecological , and urological evaluations and also the use of panoramic radiological investigations that provide a wide and detailed view of the pelvis [ 22 ]  . in routine practice , the diagnosis of chronic constipation relies primarily on subjective evidence ( rome iii criteria )  . colonic transit study and defaecography play an important role in qualifying and quantifying constipation . 
oral - anal transit time examination is a simple , repeatable , reliable , inexpensive study that uses indigestible objects , with the ability to track delayed transit times in the large intestine [ 23 ]  . 
to assess whether a patients whole gut transit time lies within the normal range , a single type of marker can be used and an abdominal radiograph performed at 12 and 120 h . 
this method provides an overall estimation of the whole gut transit [ 24 ]  . defaecography is a relatively well - tolerated examination , which is fast , highly diagnostic and simple to perform . defaecography can detect structural abnormalities ( rectocele , enterocele , rectal prolapse ) and descending perineum . rectocele and enterocele are common alterations in defaecation disorders . 
particularly , some degree of rectocele formation is present in a large percentage of asymptomatic elderly pluriparous women , suggesting that only rectoceles [ 2 cm in depth should be considered abnormal [ 1 , 25 ]  . 
the wearing out of the rectovaginal septum after vaginal delivery , particularly related to the volume of the babys head , could be a cause of rectoceles [ 2026 ]  . 
large rectoceles do not impede evacuation , but sequestration of stool within a rectocele leads to a sense of incomplete voiding and the need for digital manoeuvres to complete evacuation [ 27 , 28 ]  . 
intussusception associated with rectocele also had a higher incidence in patients with vaginal deliveries [ 29 ]  . obstructed defaecation may be suspected at defaecography : increase or decrease of the anorectal angle during straining and an incomplete opening of the anal canal ( \1 cm diameter ) resulting in delayed and incomplete rectal emptying are considered . 
 [ 32 ] showed that dynamic anorectal endosonography ( dae ) and dynamic magnetic resonance imaging ( mri ) defaecography have a similar accuracy in assessing pelvic oor disorders such as rectocele , perineal descent , and enterocele when conventional defaecography is used as the criterion standard . 
 [ 34 ] have described a very interesting classication of grade of anorectocele observed with three - dimensional dynamic anal ultrasonography ( echodefaecography ) this technique is of particular interest in the assessment of posterior pelvic oor dysfunctions . conventional defaecography is currently the only technique that can be performed with the patient in a physiological defaecation position . 
it not only has the advantage compared with conventional defaecography that it does not involve harmful ionising radiation , but it also can show rectal intussusceptions , which cannot be assessed by dae because of the presence of the probe in the rectum . however , dynamic mri defaecography is a longer , expensive , and not widely available procedure [ 32 ]  . echodefaecography may be used as an alternative method to assess patients with obstructed defaecation because it is minimally invasive , well tolerated , inexpensive , avoids exposure to radiation , and clearly shows all the anatomic structures involved in defaecation [ 34 , 35 ]  . defaecography therefore has still to be considered the rst - line investigation , while echodefaecography and dynamic mri defaecography could add further information in selected patients [ 32 ]  . our study compared defaecography and colonic transit time in women with obstructed defaecation potentially candidate to surgery . 
these patients can benet from pelvic reconstructive surgery , which may greatly improve the abnormal defaecation mechanisthe correction of rectocele and / or rectal prolapse ( starr , trans - starr , delorme technique ) resolves constipation by eliminating terminal obstruction . 
by contrast , 24 of the 30 observed constipated patients ( 80 % ) had abnormal colonic transit time : 17 % of them due to inertia coli , and 83 % due to impaired defaecation . 
this second group shows that a high percentage of obstructed patients with abnormal transit time had defaecographic signs of abnormal defaecation . these data conrm the values of both defaecography and colonic transit time in assessing clinically obstructed women . 
patients with signs of obstructed defaecation may have an abnormal colonic transit time and / or abnormal defaecography . our results showed a subgroup of clinically and defaecographically obstructed patients who probably have a limited benet from surgical procedures to correct abnormal perineal anatomy ( rectocele , enterocele , rectal prolapsed , descending perineum )  . 
descending perineum was the most common defaecographic sign in patients with normal colonic transit time and / or in patients suffering from inertia coli ; these data may be due to continuous straining at defaecation . in patients with obstructed defaecation , defaecography has been considered the rst - line investigation , while colonic transit time has not been routinely performed . 
our study demonstrated that 24 / 30 patients ( 80 % ) had abnormal colonic transit time mainly associated with descending intussusception , prolapse and anterior perineum , rectal rectocele . in 20 % of the obstructed patients , there was no clear correlation between defaecography and colonic transit time . 
in these cases , the obstructed defaecation syndrome is due to pelvic oor dysfunction and should not be correlated with chronic constipation . the differential diagnosis between colonic slow transit constipation and constipation due to pelvic oor dysfunction is essential for an adequate therapeutic strategy . despite the small number of patients , it should be possible to conclude that colonic transit time is useful in female patients with obstructed defaecation and should be associated with defaecography . 
adequacy and false - negative rate were compared specimen with radiological length and complications to assess any statistically relevant association with a multivariate logistic regression model . results a total of 290 / 308 ( 94.1 % ) samples were adequate . 
we encountered 11 / 308 ( 3.5 % ) minor complications and no major complications . conclusion ct - guided biopsy of bone lesions in cancer patients allows for a nal diagnosis in 94 % of cases . 
negative biopsies with positive positron emission tomography or magnetic resonance imaging and specimen shorter than 1 cm should be repeated to avoid a false - negative result . keywords ct - guided bone biopsy ( cid : 2 ) cancer patients ( cid : 2 ) bone metastases introduction bone is a relatively common site of metastases , accounting for more than 50 % of patients with advanced breast cancer [ 1 ]  . 
the suspicion of a bony or soft tissue lesion does not necessarily imply the need for histology [ 2 ] , because the diagnosis of metastases may be made by a combination of symptoms , clinical and radiological signs . 
however , percutaneous bone biopsy usually performed under computed tomography ( ct ) guidance is an accepted procedure and could be safe and consistently ensure the diagnosis of bone metastases [ 3 , 4 ]  . management of metastatic cancer patients with chemotherapy , or immunologic agents is usually based on the characteristics of the primary cancer [ 5 ]  . 
however , given the need for a condent histological diagnosis , the rate of biopsies on metastases is increasing , mainly due to the radiol med ( 2014 ) 119 : 852860 possibility of cancer to change its biological behavior . 
this evidence has been proven for breast cancer and should be carefully considered because of its important impact on treatment choice : any case of systemic progression should be biopsied for possible hormonal and immunological prole modication [ 6 ]  . the purpose of this study was to assess the adequacy and sensitivity of ct - guided bone biopsy in 308 procedures performed in 286 cancer patients with suspected metastases . 
as an advance in knowledge we tried to detect their correlation with radiological features and specimen length to identify any possible element suggesting biopsy repetition in the event of negative result . materials and methods this retrospective evaluation was approved by the institutional review board . 
written informed consent to undergo the procedure , including the consent to the use of anonymised clinical data for scientic and / or educational purposes , was obtained from all patients . the identication of the present study population was performed using the radiology division biopsy database of the european institute of oncology in milan . 
an electronic search of all ct - guided bone biopsies done between january 1997 and december 2012 was retrospectively performed to select patients with a previous history of primary cancer and suspected bone metastases . the assessed baseline characteristics of the patient population were : age at biopsy , sex distribution , and histology of the primary tumor . 
we evaluated biopsy adequacy and sensitivity and their relation with baseline characteristics , with site and morphological ct pattern ( osteolytic , mixed and osteosclerotic ) of bone metastatic lesions , with their mr and pet features and with bone biopsy specimen length . 
post procedural complications were also recorded . biopsy specimens were dened by the pathologist as adequate when they provided enough abnormal tissue to comfortably make a diagnosis and , for breast cancer metastases , to evaluate a reliable receptor status . all patients underwent clinical and radiological followup for at least 1 year after the procedure to assess any recurrence in negative outcomes and to detect any possible late complication . for negative biopsy results , any clinical and imaging evidence of recurrence at the site of biopsy was considered as a false - negative outcome . ct - guided bone biopsy procedure indication to perform the procedure came from the referring oncologist and was approved by the radiologist . patients coagulation was always tested before the bone biopsy by checking prothrombin activity ( pa ) , partial thromboplastin time ( ptt ) , and international normalized ratio ( inr ) ; patients with values out of the following ranges 70120 % , 1726 s , and 0.81.2 , respectively , were excluded . 
a peripheral antecubital vein was preventively accessed before the procedure for the administration of contrast media and / or drugs , if needed . the shortest path from the skin to the lesion was always chosen to avoid neurovascular structures and other solid organs . 
when the axial plane did not include both the optimal entry point of the needle and the target , the gantry was angled to facilitate accurate needle alignment and to avoid traversing other structures . 
all the examinations were performed on a 16 - slice lightspeed ct scanner ( general electric medical system , milwaukee wi , usa )  . scans were acquired during a single breath - hold with the following thickness slice 2.5 mm ; 120 kv ; 240300 ma ; 0.8 s tube rotation ; pitch 1.75. reconstructed parameters : all bone biopsies were performed using local anesthesia ( mepivacaine 200 mg ) that was injected under ct guidance giving special attention to inltrate the periosteum , where the needle was supposed to penetrate the cortical bone layer . we used cutting needles ( speedybell ; biopsybell , modena , it ) when the lesion was soft and the cortical bone was interrupted ; trap - lock 11g needle system ( angiotech ; medical device technologies , gainesville , usa ) , when the lesion showed a normal or thickened bony cortex . 
the samples of osteolytic metastatic lesions were xed in formalin while mixed and osteosclerotic metastatic lesions were decalcied by mielodec ( bio - optica , milan , italy ) according to the manufacturers instructions . 
1 flowchart of selection of patients for the analysis radiol med ( 2014 ) 119 : 852860 286 patients : two biopsies were performed on 22 patients 308 bone biopsies 18 inadequate biopsies for diagnosis 290 adequate biopsies for diagnosis 155 metastases from breast cancer 90 metastases from other or primary 45 normal bone marrow inadequate biopsies 4 inadequate biopsies for receptor assessment 40 with follow - up 5 lost at follow - up antibodies formalin - xed , in the case of breast cancer , er and pgr status , and her2 / neu overexpression were evaluated immunocytochemically . 
a 3 - lm - thick parafnembedded whole tumor sections were incubated following proper heat - induced antigen retrieval with the specic primary mouse monoclonal from dako ( glostrup , denmark ) to er and pgr ( clone1d5 , 1 : 100 dilution and clone 1a6 , 1 : 800 dilution , respectively ) or er / pr pharmdxtm ( dako ) , and a rabbit polyclonal antibody ( 1 / 3 , 200 dilution ; dako ) or herceptesttm ( dako ) to her2 for 30 min at room temperature , and subsequently treated with a high - sensitivity detection kit ( envision plus - hrp , dako ) the manufacturers instructions , using an automatic immunostainer ( autostainer ; dako )  . according statistical analysis fishers exact test was used to evaluate the association between clinical and pathological variables and the two outcomes . 
in the 22 patients with inadequate result , the biopsy was repeated . among adequate diagnoses , 45 / 290 histological ( 15.5 % ) had normal bone marrow as biopsy outcome ; 5 / 45 such patients were lost at 1 - year follow - up , but 40 / 45 were retrospectively evaluated after 1 year , and 10 / 40 ( 25 % ) patients had progression at the site of biopsy identied with ct or mr imaging . 
therefore , 10 / 303 ( 3.3 % ) biopsies were considered false - negative results , and the consequent overall sensitivity of bone biopsy was 96.7 % ( 293 / 303 )  . all biopsies were performed under ct guidance . 
similar , but not statistically signicant ndings ( p = 0.112 ) were seen for pet : among the 10 false - negative biopsies 8 / 10 had a positive pet , 1 / 10 had a negative pet , and 1 / 10 did not undergo a pet scan . finally , the proportion of false - negative biopsies decreased signicantly with increasing age ( p = 0.032 ) and specimen length ( p = 0.002 ) : in the group of specimens longer than 20 mm no false negative was evident . 
odds ratio is estimated using a multivariable fractional polynomial logistic regression models baseline demographic features , site of primary tumor , site of bone lesion , imaging characteristics , specimen length , and their correlation with adequacy are summarized in table 1 . 
for negative biopsies ( n = 40 ) , correlation with the false - negative rate is reported in table 2 . none of the baseline demographic features , site of primary tumor , site of bone lesion , and imaging characteristics showed correlation with biopsy adequacy . 
in contrast , specimen length showed a statistically signicant trend ( p = 0.036 ) : the proportion of unsuccessful biopsies was 13.6 % ( 6 / 44 ) if specimen length was less than 5 mm , percutaneous needle biopsy is a major and valuable tool in the diagnosis of musculoskeletal lesions . 
in a breast cancer patients , ct scan showed a subcortical hyperdense area of the left iliac bone ( a ) and mr showed an hypointense well dened lesion in t1 - weighted sequence ( b )  . ct - guided bone biopsy gave a negative result ( c ) , but after 26 months the patient had mr evidence of progression ( d ) they do not mention sensitivity , specicity and diagnostic accuracy , and the overall rate of diagnostic ct - guided bone biopsy of 69 % is lower than in other series . 
moreover , they use the clinical follow - up mainly to verify the so - called indeterminate biopsy results , while in our study , we followed - up patients with normal bone marrow at bone biopsy , nding a different clinical and / or imaging behavior than expected in 10 / 303 cases , thus ; leading to a sensitivity of 96.7 % ( 293 / 303 )  . 
in a standard clinical setting of suspected bone metastases , an indeterminate result is discussed for further biopsy , while a negative result is usually accepted as absence of bone metastases . 
even if mr - guided biopsies or fusion imaging techniques [ 14 ] may allow for increased accuracy of musculoskeletal biopsies , ct guidance is still considered the reference technique . 
indeed , in this series , we found 19 / 308 samples as performed on lesions undetectable or almost undetectable . among them , 5 / 19 were negative at histology . 
specically , in this subgroup of patients , only 1 / 19 ( 5.3 % ) proved to be inadequate and only 1 / 5 ( 20 % ) was a false negative . 
mrguided biopsies or fusion imaging techniques are available to increase specimen accuracy of such bone lesions [ 14 ] , but those options often are not easily available due to additional costs and because they are more time consuming . 
therefore , there could be some preliminary evidence that ct scan alone can be used for bone biopsy in patients previously studied with pet or mr . in this series , we found a correlation between specimen length and both adequacy and false - negative results . 
5 a case of suspected bone metastasis in the right ischium bone in a breast cancer patient with a hardly detectable softly hyperdense area of the inner bone marrow at ct scan ( a ) , a well - shaped focal lesion hypointense in t1 - weighted sequence ( b ) and hyperintense in stir sequences at mr scan ( c )  . 
a percutaneous ct - guided biopsy ( d ) conrmed the presence of a bone metastasis from breast cancer fragmentation , crush artifact and trabecular distortion . however , adequacy is not mentioned and the maximum specimen length of sample allowed by the in vitro model is 1 cm [ 15 ]  . 
the rst consideration is that one of the two most performing needles for specimen quality was the same as used in our study ( trap - lock 11g needle system ; angiotech ; medical device technologies inc . , gainesville , usa ) for normal or thickened bony cortex lesions . 
furthermore our in vivo analysis was focused also on samples longer than 1 cm revealing a signicant statistical association between specimen length and both the probability of an inadequate result and the probability of a falsenegative result : the longer the specimen , the lower the probability of an inadequate and false - negative result . 
second , the pathologists did not perform a blind evaluation of the specimen being aware of the patients history as in a normal clinical setting and we know this could affect the nal diagnosis . in conclusion , ct - guided bone biopsy in cancer patients with suspected metastases is safe and should be considered as an important tool in the diagnostic workup ; especially , when receptor assessment is needed . 
correlation with surgical and pathological data maria pia bondioni diego gatta vassilios lougaris nicoletta palai marino signorelli silvia michelini giuseppe di gaetano paola tessitore lorella mascaro andrea tironi giovanni boroni roberto maroldi daniele alberti received : 16 october 2013 / accepted : 22 november 2013 / published online : 8 march 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract purpose the aim of this study was to evaluate the diagnostic accuracy of postnatal multidetector computed tomography ( mdct ) compared with prenatal ultrasound ( us ) , surgical ndings , and histology , in 33 patients with congenital cystic lung disease . methods thirty - three patients , 17 males and 16 females , were evaluated by mdct . 
lung lobectomy , segmentectomy , atypical resection , lesion resection were performed in 31 patients and surgical specimens were analysed . results prenatal us and mdct correctly diagnosed 76.9 and 94 % of respectively . 
lougaris pediatrics clinic , department of clinical and experimental sciences , university of brescia , brescia , italy the essential role of imaging , in particular ct , in providing invaluable preoperative information on congenital cystic lung diseases recognised in uterus . keywords multidetector computed tomography ( cid : 2 ) congenital cystic lung disease ( cid : 2 ) congenital lung malformation ( cid : 2 ) prenatal ultrasound introduction the rst bud of the respiratory tract appears around the fourth week of gestation and originates from the ventral anterior primitive intestine ( respiratory diverticulum )  . errors at this stage of development are responsible for congenital lung malformations that can be divided into two groups : ( a ) dysmorphic lung , namely lung agenesis , aplasia and hypoplasia , ( b ) focal malformations or congenital cystic lung diseases ( ccld ) , namely congenital pulmonary airway malformation ( cpam ) , pulmonary sequestralobar emphysema ( cle ) , and tion ( ps ) , congenital n . 
1. according to tukeys notation [ tukey , john ( 1977 ) , exploratory data analysis , addisonwesley ] , reported minimum and maximum values are ltered excluding all the outlier points , i.e. 
these last malformations are the focus of our study [ 1 ]  . cpams make up almost 3040 % of all congenital lung lesions , and are characterised by an excessive overgrowth of the terminal respiratory bronchioles and lung structures with alveolar growth suppression [ 2 ]  . 
genes such as hoxb5 , fgf7 , and platelet - derived growth factor - b ( pdgf - b ) have been implicated in the pathogenesis of cpam [ 35 ]  . 
the rst stocker classication from 1977 [ 6 ] has been modied and now includes lesions from type 0 to type iv based on the origin of the malformation [ 7 ]  . 
ps is the second most common lesion after cpam , characterised by a portion of lung parenchyma that does not connect with the tracheobronchial system and is therefore not ventilated whereas a systemic arterial supply is always present [ 2 ]  . 
based on the age of onset , ps may be distinguished in intralobar and extralobar ; the latter may be associated with other congenital anomalies [ 1 , 8 , 9 ]  . 
finally , bc occurs at a very early age and originates from an abnormal budding tracheobronchial tree , followed by its non - branching process [ 1 , 8 ]  . the rst imaging approach to detect ccld disease is prenatal ultrasound ( pus ) , which is usually performed at 1822 weeks of gestation and allows screening and denition of foetal lung lesions in the majority of cases [ 10 ]  . foetal magnetic resonance imaging is also a valuable tool for prenatal diagnosis of ccld , but for the time being it is only available in few centres . after birth , multidetector computed tomography ( mdct ) plays a key role in the radiological diagnosis of ccld in children , conrming type and number of lesions and their characterisation , and allowing a thorough preoperative evaluation [ 8 ]  . 
mdct offers the highest spatial resolution and enhanced diagnostic quality , together with multiplanar reformation , which is very informative for the surgeon [ 11 ]  . our study aimed to retrospectively evaluate the diagnostic accuracy of mdct in 33 patients with ccld . 
we also compared mdct with pus and with surgical and histological ndings ( and with histology ) to evaluate the diagnostic performance of mdct in dening the right diagnosis and the best surgical planning . materials and methods patient population our institutional review board approved the review of this radiological , surgical , and pathological data for fig . 
samples of the specimens were taken for histology , particularly including cysts , nodules and apparently normal lung when recognised , or random when no gross differences were evident . after sample processing and parafn embedding , slides for microscopy examination were stained with haematoxylin eoshistochemical or immunohistochemical stains were performed when considered appropriate . 
in all cases , dose modulation was used to minimise the radiation dose . mdct was performed after intravenous injection of 2 ml / kg of non - ionic contrast medium ( 320 mg i / ml )  . contrast medium was injected into an antecubital vein with a power injector at a rate of 1.0 ml / s for a 24 - gauge catheter , and 1.52.0 ml / s for a 22 - gauge catheter . 
two patients with intralobar ps had also cpam type i and ii , respectively , for a total of 17 lesions . lesions were detected in the right lung in ten patients ( four cpams were located in the right upper lobe , two in the middle lobe , and four in the right lower lobe ) , and in the left lung in eight patients ( two cpams were located in the upper lobe , one in the lingula , and ve in the lower lobe )  . ps was detected in 14 patients ( 42.4 % ) : ps was intralobar in 4 patients and extralobar in 10 . 
in two patients , the lesions detected 20 / 26 ( 76.9 % ) 31 / 33 ( 94 % ) p = 0.122 lesion was found under the left side of the diaphragm . lesions were located in the left lower thoracic cavity in 50 % of cases ( 7 / 14 ) and in the right lower thoracic cavity in 35.7 % of the cases ( 5 / 14 ) ; in 14.2 % of the cases ( 2 / 14 ) , the lesions were next to the left adrenal gland . in three patients ( 9.1 % ) , the diagnosis was consistent with cle in the left upper and lower lobe and in the right lower lobe , respectively . in one patient ( 3.0 % ) , the diagnosis was consistent with right bc in the right lower lobe . 
the ten patients with extralobar ps underwent lesion resection , the four patients with intralobar ps underwent atypical pulmonary resection including the sequestration in two cases , and lobectomy in two patients . 
patients with cle underwent lobectomy , and the only patient with bc underwent evacuation by puncture and cystic resection . no postoperative complications were observed . 846 radiol med ( 2014 ) 119 : 842851 fig . 
unenhanced mdct scans in axial ( b , c ) and coronal planes ( d ) show , in the left lower lobe , multiple small thin - wall cysts ( arrows )  . 
pus was suggestive of the correct diagnosis in 20 out of 26 lesions ( 76.9 % ) , 11 cpam , eight ps , and one bc , as conrmed by histology . of the two cases of cpam associated with ps , us correctly identied the two different lesions in only one case , while the other case was diagnosed as ps only . 
for cpam detection , pus sensitivity and specicity were respectively 100 and 60 % , whilst they were 66.7 and 100 % respectively for ps . comparison between mdct and histological ndings out of the 33 mdct patients , 31 underwent surgery for a total of 33 lesions . 
postcontrast mdct scans ( b , c ) reveal a hyperdense lesion in the left lower lung ( arrowhead ) with a large artery originating from the aorta ( black arrow )  . 
low power view of intralobar sequestration ( e ) shows pleural brosis and mild inammatory changes in pulmonary parenchyma with mucus in some alveoli ( h&e , 940 ) in the only observed case of bc , both pus and mdct diagnoses were conrmed by histology ; in cle , only two out of three cases in which mdct raised a suspicion were histologically conrmed ( ppv = 66 % ) , the remaining case being a cpam type i . 
in particular , mdct overestimated the extent of the lesions in three patients with cpam . discussion congenital cystic lung diseases include a heterogeneous group of anomalies affecting bronchi , lung parenchyma , arterial supply , and venous drainage . 
the spectrum of these abnormalities includes cpam , ps , cle , and bc [ 1 ]  . the rst diagnostic examination is pus , usually performed at 1822 weeks of gestation , during the rst scheduled morphological evaluation of the foetus [ 14 ]  . 
pus at 21 weeks of gestation ( a , b ) , displays a homogenous hyperechoic lesion ( clippers ) with an arterial vessel ( arrow ) entering the mass . mdct scans after contrast medium administration ( c , d ) show a homogeneously hyperdense mass in the left lower lobe ( asterisk )  . 
a feeding artery arising from the aorta ( white arrowhead ) with a venous drainage through the azygous system ( black arrowheads ) can be seen . mip reconstructions ( e , f ) show a marked vascularity of the lesion ( asterisk ) , and systemic venous drainage ( white arrows )  . 
in our series , lesions increased in size in 30 % of cases , decreased in size in 30 % of cases , and were no longer detectable at the last pus in 40 % of cases . after birth , chest x - ray is no longer the rst imaging approach , as it fails to detect lesions in about 60 % of asymptomatic patients [ 19 ]  . 
our mdct examinations were performed with ageand weight - based protocol in accordance with the literature , achieving a reduced biological aggressiveness in paediatric patients , particularly in newborn babies and little infants , as were many patients in this study [ 2023 ]  . 
furthermore , out of the four patients with no longer detectable lesion at the last pus , mdct showed the presence of cpam in three cases and of ps in one case . the accuracy of pus and mdct diagnosis was then compared with the histological data . 
agreement between pus and histology and mdct and histology was observed in 76.9 % ( 20 / 26 ) and 94 % ( 31 / 33 ) of the cases , respectively . 
overall , the ppv of the survey mdct scans compared with histology was 93.3 % , compared with a reported value of 70 % in the literature [ 19 ]  . 
as most surgeons consider surgical resection of these lesions mandatory , mdct can provide detailed anatomical localisation of lesions , with the possibility of 3d reconstruction and high spatial resolution . 
postprocessing reconstruction can also provide detailed information on vascular afferents , and 3d reconstructions in our study proved to be very helpful to the surgeon during preoperative planning [ 24 , 25 ]  . 
the analysis of our data shows that mdct should be used as rst - step imaging in the postnatal evaluation of patients with ccld , and our work suggests that mdct can be considered the best imaging modality in the postnatal evaluation of patients with ccld detected in uterus , with higher specicity values for cpam lesions and higher sensitivity for ps compared to pus ndings . 
patelli risk management , ospedale san gerardo , via pergolesi , 33 , 20900 monza , italy e - mail : c.patelli@hsgerardo.org nephropathy ( cin ) , when in the angiographic unit , we have used a 20 - item checklist named time - out derived from the cirse sc . 
the main items are : in the time - out phase , active verbal commuidentication of the nication within the team ; correct patient and of the procedure site and side . 
additionally , during the preprocedure ( sign - in ) and postprocedure ( signout ) stages a series of clinical data are collected such as administration of prophylaxis against contrast allergy or contrast - induced needed informed consent , discontinuation of anticoagulation therapy , fasting , correct labelling of biological samples , etc . results preliminary educational sessions were held to sensitise all the staff involved in the time - out project ( physicians , nurses , radiographers ) and ensure satisfactory compliance from the outset in consideration of the increased time and paperwork that checklist implementation would involve . conclusions the use of a checklist in ir , named timeout in our experience was feasible and effective allowing elimination of adverse events in the rst year of use and involvement and awareness of promoting signicant patient safety among the health - care teathe level of implementation , completeness and acceptability of the sc within the team increased after adequate training had been provided . interventional radiology ( cid : 2 ) patient safety ( cid : 2 ) keywords checklist introduction c . 
battisti 3 , 20854 vedano al lambro ( mb ) , italy adverse events are unexpected situations which occur during clinical activities and may result in temporary or permanent , physical , emotive or economic damage to the patient and increased health - care costs to society . radiol med ( 2014 ) 119 : 828834 it has been estimated that 50 % of all in - hospital adverse events are related to surgery and at least 50 % of these could be avoided because they are caused by errors [ 1 , 2 ]  . apart from the surgical risk itself , also the patients stay and transfer to and from the operating theatre , the different specialities and health professionals involved in surgical activity and the complexity of the procedures make the surgical disciplines more prone to error and therefore to adverse events [ 3 , 4 ]  . of all the targeted and effective actions that can be undertaken to reduce adverse events , the use of safety checklists ( scs ) might have a prominent role . 
this checklist led to a signicant reduction in clinical adverse events [ 5 ]  . even similar disciplines to surgery , such as endoscopy or interventional radiology ( ir ) , are potentially at risk of producing adverse events [ 2 ]  . 
ir procedures have many aspects in common with surgical operations ( complexity , fast patient turnover , urgency and emergency procedures , multilevel or diffuse pathologies , teamwork , etc ) and consequently carry a risk for potential error . 
the analysis revealed a lack of clarity regarding the organisation and duties of the various healthcare professionals working in the radiology suite ( denition of roles ) and the procedure for side identication . 
as a corrective measure , together with our hospitals risk manager we decided to plan , develop and implement a radiological sc with the aim of identifying and therefore reducing the probability of avoidable accidents or adverse events , or at least lessening their negative effects . to prepare our sc , we referred to the scientic literature on errors , adverse events and complications in ir , including the available standards and guidelines [ 6 , 8 ]  . 
in november 2011 , a workgroup made up of a radiologist , a nurse and a radiographer , coordinated by our risk manager , drafted a rst sc named time - out that reected our departments logistic reality . 
after completing each phase , the compiler , who is responsible for the check , must sign at the bottom of each block of items . in detail , after the patient is admitted to the ir department , a radiologist checks the blood tests ordered for the procedure and veries that the patient has received the required information regarding the interventional procedure . 
extensive instructions were given on how to ll in the sc correctly , especially in consideration of the time - consuming nature of the task and the need to ensure compliance . 
an initial trial period of 1 month was planned . at the end of the trial period , we addressed any general issues and doubts and assessed the completeness of the sc , making adjustments if necessary . after 3 months , the compilation rates were re - evaluated the team and a questionnaire was administered to all members , investigating satisfaction with the checklist , their experience with the use of the sc and evaluations of patient safety , and eliciting suggestions and ideas for improving the results . 
eight months after the introduction of the sc , another meeting was held to communicate the results of the rst 6 months and the critical points identied , leading to a nal revision of the sc . in december 2012 , data on adverse events related to ir procedures performed during the rst year of implementation of the sc were extracted from the intra - hospital software events . results the results at 1 and 3 months are reported in table 1 as regards the type of procedure performed on different patient groups and in table 2 as regards sc compilation . radiol med ( 2014 ) 119 : 828834 table 2 completeness of time - out safety checklist checklist complete incomplete incomplete hour barcode biological samples ac therapies / prophylaxis procedure signature ward fasting patient name site / side ac anticoagulation 13 january 17 february 100 / 112 62 ( 64.5 % ) 38 ( 35.5 % ) 29 ( 76.3 % ) 23 ( 60.5 % ) 16 ( 42.1 % ) 12 ( 31.5 % ) 4 ( 10.5 % ) 3 ( 7.9 % ) 3 ( 7.9 % ) 3 ( 7.9 % ) 2 ( 5.2 % ) 1 ( 2.6 % ) 13 april 17 may 90 / 101 76 ( 84.4 % ) 14 ( 15.6 % ) 6 ( 42.8 % ) 2 ( 14.2 % ) 2 ( 14.2 % ) 1 ( 7.1 % ) 4 ( 28.5 % ) 1 ( 7.1 % ) during the rst month , scs were compiled for 89.3 % of procedures ( 100 checklists out of 112 procedures )  . 
in particular , in the rst version of the sc , the query time of procedure was omitted in 76.3 % of the cases : considering that this information can be obtained both from the radiological images stored in the pacs and from the nursing assessment form ( used for a long time in the angiographic suite ) , the item was removed . 
other deleted items were the patient requires postprocedure care and insert operative report : in the rst case , because the information is already noted in the nursing assessment form and , in the second , because the operative reported is already contained in the radiological report , the completion and inclusion of which is veried in the sign - out phase . an anonymous survey was distributed to all of the 27 team members ( three physicians , 10 nurses and 14 radiographers ) , 17 of which were collected ( 63 % ) and analysed . 
starting from 2000 in the usa , the institute of medicine supported by the quality of health care in america committee launched a 10 - year project for the development and implementation of strategies to increase the quality and safety of health care by adopting verication procedures ( such as checklists ) and standardising processes to limit reliance on human memory , which is known to be far from infallible [ 9 ]  . a recent systematic review reported that the total average incidence of adverse events in hospitals is 9.2 % ( range 4.612.4 % ) , almost one in ten patients . 
moreover , ir procedures place the team in situations very similar to those experienced in operating theatres ( prolonged stress , operator fatigue , team inexperience ) that can lead to mistakes ( table 3 ) : this explains the need to enhance patient safety measures through greater standardisation of procedures and increased quality of care in ir procedures . in addition to the most commonly recognised errors in medicine , some errors are specic to ir and can potentially occur at any time during the patients stay in the angiographic suite . 
most of them are preventable and are listed in a table of 62 items published by the society of interventional radiology ( sir ) task force on medical error [ 8 ]  . for instance , a patient with bilateral or diffuse vascular disease depicted on ct or mr angiography might undergo different treatments without the appropriate preprocedural communication . 
the orientation of the radiological images must be set according to the patients position on the angiographic bed , which is not constant but related to operative requirements ( head / feet ; right / left ank ; prone / supine ) : if an incorrect setting is not rapidly detected by the team , e.g. , due to large sterile drape masking the anatomical landmarks , this could potentially lead to wrong - side errors . the operator must be aware of most common potential problems occurring before , during and after an interventional procedure , so that the use of a checklist should provide an opportunity for additional reection and evaluation . not many reports exist in the scientic literature on the use of sc in ir . 
since 2003 , at the boston childrens hospital , a time - out checklist has been used in paediatric ir procedures ; this follows the indication of the universal protocol , whose appropriateness is veried monthly by independent professionals [ 12 ]  . 
in 2007 , after an adverse event occurred in ir at the end of a dialysis catheterisation , stecker and mcnamara introduced a short postprocedural checklist so as not to omit administration of intracatheter heparin , afxation of closure caps or placement of dressing on the insertion site [ 13 ]  . an sc can be used in different health - care environments because it includes three important safety goals of the joint commission on accreditation in healthcare organizations ( jcaho ) : ( 1 ) improving accuracy in patient identication ; ( 2 ) improving communication between health - care coworkers ; ( 3 ) eliminating all wrong - site , wrong - patient and wrong - procedure interventions [ 14 ]  . 
the advantage of an sc for ir is that it ensures reduction of human error in terms of omitting key steps in pre - , intraand postoperative care , and therefore minimises potential harm to the patient . two papers recalling the jacho recommendations have described the application of the universal protocol to settings other than the operating theatre , adapting it to ir procedures [ 6 , 12 ]  . 
the universal protocol focuses on prevention of wrong - site / wrong - side procedures , while radiological sc aim to improve the entire ir process , from patient positioning to the use of intraprocedural images for site and side determination . in 2010 , england and wales introduced a specic sc for ir , derived and adapted from the who checklist . 
this list is made up of 28 items divided into three parts : sign - in ( before anaesthesia ) , time - out ( before the beginning of the procedure ) and sign - out ( before any member of the team leaves the angiographic theatre ) and includes a box with all the personal data of the patient . 
each section should be read out loud by one of the team members . in the same year , a radiological sc ( radpass , radiological patient safety system ) was also introduced in holland , at the academic medical centre of amsterdam . developed based on the available literature and expert opinion , the radpass checklist is divided into two parts : part a ( planning and preparation ) and part b ( procedure )  . the latter is divided into a series of checks to be done just before the beginning of the procedure ( b1 ) and items regarding postoperative care immediately after the procedure ( b2 )  . 
this checklist was to be applicable to a variety of interventional procedures , adjustable and modiable to meet the needs of different centres and should be satisfactory to the vast majority of interventional radiologists [ 16 ]  . 
in addition , unlike other scs , it requires the name and signature of the compiler to be inserted at the end of each section . in comparison to the cirse checklist , we decided to produce a more balanced and synthetic checklist to ensure better compliance and completion rates , while guaranteeing high standards of care , compliance with the guidelines and patient safety during all of the phases of ir procedures . out of the 32 items recommended by the cirse checklist , we extracted some essential items that better suited the specic needs of our centre . 
this led to the development of a nal checklist consisting of 20 items ( slightly shorter than the english and the dutch versions , which contain 21 and 27 items , respectively ) , which contributed to eliminating adverse events during the rst year of application , thus conrming its efcacy . the majority of patient safety interventions and some checklists require humans to modify their behaviour . 
we think that the positive effect of an sc is due to several mechanisms : direct prevention of mistakes through checklist performance ; optimisation of processes triggered by sc implementation ; improved team working stimulated by the sc ; improved team communication and attitudes towards safety and quality . the only complaint about checklists regards the amount of time required to perform thehaynes et al . 
these data have been inferred from the respondents comments , such as : explain which information / evaluations are to be done by the nurse , radiographer or physician ; establish , at beginning of each procedure , who does what ; its always the same people who perform the checklist , everybody should perform it . 
these uncertainties about responsibilities were subsequently analysed and claried at a team meeting the content of which was reported in a quality document of the radiological suite ( operative procedure of the angiography suite ) that can be found on our hospitals intranet . in the near future , the integration of checklists in digital patient information systems could help to develop more checklists capable of offering information and links to other sources . 
if the public health mission of ir relied until recently on the dramatic technological development of imaging - guided therapies ( sir , mission statement 2011 , whoweare ) , nowadays we are less centred on technology and more on the patient , in terms of treatment effectiveness , team dynamics , changing health behaviours , constant improvement of the quality of care , standardisation of care and reduction of costs [ 18 ]  . conclusion in conclusion , the use of an sc in ir may constitute a valid tool to maximise patient safety during interventional procedures , by intercepting possible adverse events and reducing or avoiding human errors at key points , such as patient preparation , procedure initiation or postprocedural care . the introduction of an sc ( called time - out in our experience ) into routine ir practice was found to be feasible and helped us to eliminate adverse events during the rst year of implementation , generating strong commitment and greater awareness of patient safety among the health - care teaapplicability , completeness and acceptance of the sc by the team improved after adequate training and after encouraging the different professional categories to communicate , cooperate and share responsibilities , which favoured the realisation of our objectives in terms of safety standards . conict of interest r corso , f . 
the efciency of automatic tube current modulation ( z - dom and d - dom ) , shaping lters ( smartshape and intellibeam ) and asymmetric collimator ( eclipse ) was evaluated using appropriate phantoms . results the scattered radiation contribution from the peripheral regions to the cumulative dose is not negligible . the cnrd is 20 % better compared to a traditional 16 - slice scanner , with a dose reduction of 40 % . 
the application of d - dom and z - dom modulations reduces the currenttime product ( mas ) values by 23 and 18 % , respectively , but they are not yet is not negligible , integrated . 
radiodiagnostica , azienda ospedaliera san gerardo , monza , italy conclusions brilliance ict dose reduction tools are efcient , but should be analysed carefully and used correctly . keywords multislice computed tomography ( cid : 2 ) radiation dosimetry ( cid : 2 ) patient radiation protection ( cid : 2 ) bow - tie lters ( cid : 2 ) over - ranging introduction in the last decade , computed tomography ( ct ) has undergone a remarkable development in particular with the advent of multi - layer technology ( multislice computed tomography , msct ) and , according to italian legislative decree 187 / 2000 , ct examinations are classied as diagnostic procedures involving a high radiation dose to the patient . recent papers emphasise the increase in the number of ct examinations and some of these studies have correlated the dose escalation to the population with the probability of tumour induction . 
in italy , particularly in the emilia romagna region , the contribution to collective effective dose from ct examinations is around 66 % of the total [ 1 ] ; in the us it is 67 % [ 2 ] and in the uk 40 % [ 3 ]  . 
in 1989 the national radiation protection board ( nrpb ) estimated that an abdominal ct scan carried a 1 : 2 , 000 risk of fatal cancer in 1669 - year - old patients [ 4 ]  . an increased risk of cancer induction has been observed in epidemiological studies on atomic bomb survivors , who were exposed to an effective dose of about 10100 msv [ 5 ] : a ct scan may result in an effective dose of the same order and the patient may be subjected to multiple ct examinations during their lifetime . 
in 2007 , approximately 72 million ct scans were performed in the us , grouped for 872 radiol med ( 2014 ) 119 : 871877 effective dose as follows : 78 % low dose ; 20 % moderate exposure ( 320 msv ) ; 2 % high ( [ 20 msv ) and very high ( [ 50 msv ) dose [ 6 , 7 ]  . optimisation of the acquisition technique may substantially reduce the dose per examination and , at the same time , the dose contribution of ct examinations to the population . 
the aim of this study was to provide a dosimetric characterisation of a 256 - slice ct scanner with particular attention to the available dose modulation and reduction tools used in clinical practice . materials and methods the multislice brilliance ict scanner ( philips healthcare , cleveland , oh , usa ) is able to acquire up to 256 slices of 0.625 mm thickness for each x - ray tube rotation , obtaining high quality 3d images . 
at the end of each examination , the volumetric computed tomographic dose index ( ctdivol ) along with the dose - length product ( dlp , dened as the product of ctdivol and scan length ) should be displayed on the control panel and indicated in the dosimetric report [ 9 ]  . 
to dene ctdivol , it is necessary to introduce another physical quantity : the ctdi100 corresponding to the ratio between the dose prole integral and the length of the pencil ionisation chamber ( with 100 mm integration length )  . 
two standard phantoms , consisting of a polymethylmethacrylate ( pmma ) cylinder with a height of 14 cm and a diameter of 16 cm ( head phantom ) or 32 cm ( body phantom ) , were used to measure ctdi100 . 
the ctdi weighted ( ctdiw ) , which expresses the average dose in the scan plane , is calculated from the measurements of ctdi100 at the centre and the periphery of these phantoms [ 10 ]  . 
hence ctdivol is obtained as ctdiw divided by pitch value , because in ct the dose is inversely proportional to the ratio between pitch and collimation . with the introduction of multislice ct scanners , the collimation may also reach values equal to or higher than 80 mm , so the ionisation chamber length ( 100 mm ) is inadequate for ctdiw measurement . 
standard methods are no longer applicable because they neglect the dose contributions of the penumbra and of diffusion from the adjacent tissues placed outside the primary bearecently the american association of physicists in medicine ( aapm ) has suggested to use , as an alternative to the ctdi , the equilibrium dose ( deq ) [ 11 ]  . 
for a xed scan length l along the longitudinal axis , the cumulative dose at the midpoint of scanning lengthdl ( 0 ) includes both the primary dose and the scattered radiation . 
as l increases , dl ( 0 ) increases asymptotically towards an upper limiting value , deq , such that the source of scatter radiation is sufciently remote as to make a negligibly small additional contribution . under the same exposure conditions , dl ( 0 ) was measured for different scan lengths using a 0.6 cm3 ionisation chamber ( 10x5 - 0.6ct , radcal corporation , ca , usa ) and a phantom created by inserting the body phantom between two 32 9 32 9 30 cm3 pmma parallelepipeds . 
to determine the deq , the cumulative dose was measured increasing the scan length from 8 to 45 ca 32 9 32 9 30 cm3 pmma parallelepiped was used as a phantom within which properly calibrated 30 9 1 cm2 gafchromic ( cid : 3 ) xr - qa2 dosimetric lms ( lot number a10071002a , isp technologies inc . , nj , usa ) [ 12 ] were included . 
the lms were digitalised by epson 10000xl atbed scanner 24 h after exposure and dose proles in the longitudinal direction were calculated using picodose xpro software ( tecnologie avanzate , turin , italy )  . contrast - to - noise ratio ( cnr ) the physical quantity for structure and detail identication in msct is the cnr . 
these lters work along with bow - tie lters , named smartshape ( small , medium and large ) , which change the beam intensity as a function of patient size . the bow - tie lters provide more ltration in peripheral regions than in the central one , where patient thickness is greater , to improve dose distribution and standardise image noise . 
furthermore , intellibeam and smartshape lter attenuation proles , expressed as number of counts sampled along a row of the array detectors , were analysed for different acquisition settings using philips proprietary software available on the workstation . values in the xy plane were determined from air - kerma measurements by placing the pencil ionisation chamber at 0 ( cid : 4 ) , 45 ( cid : 4 ) , 90 ( cid : 4 ) , 135 ( cid : 4 ) and 180 ( cid : 4 ) inside the gantry tunnel . 
for each x - ray tube rotation , mas values corresponding to 0 ( cid : 4 ) ( minimum ) and 90 ( cid : 4 ) ( maximum ) were calculated by multiplying the mas average value supplied by the ct scanner by the chamber percentage value equal to 1 for 90 ( cid : 4 ) instead of 0.86 for 0 ( cid : 4 ) and whole phantom or 0.81 for 0 ( cid : 4 ) and half phantom . over - ranging and eclipse asymmetric collimation over - ranging means an increase in scan length due to the additional rotations at the beginning and at the end of a spiral scan required for data interpolation to reconstruct the rst and the last slice of the imaged body region . 
the brilliance ict scanner has an asymmetric collimator , called eclipse , which automatically occurs at the beginning and at the end of the helical acquisition , reducing patient dose without any deterioration in image quality . dose proles of 1 9 30 cm2 gafchromic ( cid : 3 ) xr - qa2 strips irradiated with helical modality at the isocentre were analysed to verify the asymmetric collimator efciency and to estimate over - ranging . 
furthermore , the lms were placed between the cervical and the upper chest region of the anthropomorphic phantom alderson rando surface , to compare the effect of collimation to patient dose reduction . automatic current modulation system dosimetric audit the aim of the automatic current modulation system is to deliver an optimised current ( ma ) value for the type of patient for the anatomical region being studied . 
the brilliance ict scanner ma modulation system is structured as follows : the automatic control system ( acs ) which establishes maximum patient diameter and tissue density on the basis of the scanogram and automatically suggests the optimal x - ray current value to control dose and noise level ; the z - axis dose modulation system ( z - dom ) that modulates ma along the patient longitudinal axis using the attenuation prole ; nally , the dynamic angular dose modulation system ( d - dom ) which modies the ma as a function of patient eccentricity and tissue attenuation for each x - ray tube rotation . 
as there is a direct proportionality between mas and dose , the mas in february , june and september 2011 the dosimetric parameters and the over - ranging of 30 abdominal ct examinations ( 10 examinations / month ) were collected from the ct scanner dosimetric report . 
the dosimetric audit was carried out before installation of the idosetm iterative reconstruction algorithm . the ctdivol and the size - specic dose estimate ( ssde ) were considered to evaluate the patient absorbed dose ; ssde is a dosimetric quantity which takes into consideration corrections based on patient size and is dened as follows : ssde fsize ( cid : 2 ) ctdivol where fsize is the correction factor depending on patient diameter and on ctdivol phantom dimension ( 16 or 32 cm ) [ 14 ]  . 
the patient diameter was calculated by measuring the lateral abdomen dimension on the scanografurthermore , for the upper abdomen single scan , the effective dose was calculated by multiplying the dlp value by 0.015 sv mgy - 1 mm - 1 conversion factor [ 15 ]  . 874 radiol med ( 2014 ) 119 : 871877 figure 2 shows the number of counts sampled along a row of detector array for the ve default acquisition modalities . 
automatic current modulation systems figure 3 shows longitudinal ma prole in the philips calibration phantom as a function of different modulations . the system provides only the average mas for d - dom modulation . 
figure 5 shows the comparison between 64 9 0.625 and 128 9 0.628 mm collimation for mas and dose proles obtained with the alderson rando phantom and gafchromic ( cid : 3 ) xr - qa2 lms . 
the accuracy of mas modulation depends on collimation , especially at the transition of the x - ray beam over adjacent anatomical regions of different anatomical districts ( e.g. , neck - chest )  . 
dosimetric audit figure 6 summarises the ctdivol ( mgy ) , ssde ( mgy ) , effective dose ( msv ) and over - ranging ( mm ) mean values of 10 examinations collected in april , june and september 2011 . discussion an accurate evaluation of ct patient dose reduction tools is necessary for a proper use in clinical practice [ 1618 ]  . the contribution of scatter radiation to the cumulative dose from the phantom / patient peripheral region is not to be underestimated . 
the dl ( 0 ) value arises from 27 mgy ( minimum scanning length ) to 42 mgy ( 45 cm scanning length ) with an increase of 64 % . 
1 cumulative dose dl ( 0 ) at the midpoint of the irradiated length ( a ) and cumulative dose proles in function of irradiated length ( b ) results 1 . 
6 dosimetric audit results : ctdivol ( mgy ) , ssde ( mgy ) , effective dose ( msv ) and overranging ( mm ) mean values the brilliance ict scanner has a better gure of merit than a traditional 16 - slice scanner ( brilliance ct 16p )  . indeed , the new nanopanel3d detector in association with the clearray2d anti - scatter grid allows an improvement in cnrd of approximately 20 % , which means a patient dose reduction of 40 % . the smartshape and intellibeam lters reduce the peripheral patient dose in a variable percentage according to the acquisition modality employed . 
in fact , the dose distribution is not affected by the lter with trauma modality because the full dose is needed to perform a diagnostic examination extending to for body the patients extremities . 
on the contrary , modality and in particular for the cardiac protocol , the lter reduces the dose in the peripheral region , corresponding to a lower diagnostic interest . application of modulation along longitudinal axis ( zdom ) implies a dose reduction less than angle modulation ( d - dom )  . 
the dose to the thyroid increases by about 60 % switching from 64 9 0.625 to 128 9 0.628 mm collimation due to a greater over - ranging and to an inadequate mas modulation . the installation of increasingly complex ct scanners designed for highly specialised performance requires accurate optimisation of acquisition protocols to achieve adequate image quality without involving an unjustied increase in patient dose . 
a total dose of 3651 gy was delivered to the 50 % isodose line covering the planning target volume at 35 gy / fraction , whereas a total dose of 6085 gy was delivered at 57 gy / fraction to the gross target volume . 
the local control rate ( lc ) and overall survival rate ( os ) were calculated using the kaplanmeier method . results patient follow - up ended in march 2013 and the follow - up rate was 100 % . 
xia department of radiation oncology , air force general hospital , beijing 100142 , peoples republic of china e - mail : wangyj9999@163.com individualised treatment and a combination of multiple therapeutic approaches ; this will be a primary research trend in the future . keywords renal cell carcinoma ( cid : 2 ) radiotherapy , stereotactic body radiotherapy ( cid : 2 ) gamma - ray ( cid : 2 ) asynchronous bilateral tumour introduction renal cell carcinoma ( rcc ) is one of the most frequently occurring malignant tumours of the urinary system , and its incidence is rising worldwide [ 1 ]  . 
however , the probability of tumour after rn is developing a contralateral approximately 415 % [ 3 ] and the treatment for this asynchronous bilateral renal cell carcinoma ( brcc ) remains clinically challenging ; there is currently no unied therapeutic scheme . 
however , a considerable number of the patients cannot undergo surgery because of advanced local disease or other medical conditions . renal stereotactic gamma - ray body radiation therapy ( c - sbrt ) is widely known as an independent chinese innovation which is especially effective in the treatment of solid tumours such as lung and pancreatic cancer [ 47 ]  . 
herein , we report our experience regarding c - sbrt in the treatment of nine patients with asynchronous brcc between february 2002 and may 2012 . to our knowledge , there have been no previous published studies that have focused on asynchronous brcc radiol med ( 2014 ) 119 : 878883 treated using c - sbrt . 
the purpose of this retrospective study was a preliminary evaluation of the feasibility , efcacy and toxicity of c - sbrt in the treatment of asynchronous brcc . materials and methods ethics statement this study was approved by the institutional review boards ( irbs ) for the cancer center , air force general hospital , peoples republic of china . 
written informed consent was obtained from all patients in accordance with the irb regulations . general information the clinical data from nine patients with asynchronous brcc who had received c - sbrt between february 2002 and may 2012 were retrospectively evaluated . 
the inclusion criteria were as follows : ( 1 ) patient age 2085 years ; ( 2 ) a history of rn for the primary renal malignancy that was histopathologically or radiologically diagnosed as rcc ; ( 3 ) computed tomography ( ct ) or positron - emission tomography ( pet ) performed to identify any remaining renal lesions that were unresectable or medically unsuitable for resection ; ( 4 ) no loss of renal function ; ( 5 ) no history of radiotherapy involving the abdomen ; ( 6 ) an eastern cooperative oncology group ( ecog ) performance status scale b2 ; and ( 7 ) informed patient consent obtained for radiotherapy . 
patients who suffered from hereditary syndromes or who had a history of another invasive cancer were excluded from the study . the median age of the patients treated with brcc was 70 ( range 5884 ) years ; seven of these patients were male . the median maximum tumour diameter was 4 ( range 2.74.5 ) cthe median disease - free interval was 42 ( range 1302 ) months after surgery . 
tumours were staged according to the international union against cancer tnm classication ( 2006 )  . treatment methods stereotactic gamma - ray body radiation therapy ( ourqgd , shenzhen , china ) was carried out using a body gamma knife ; this consisted of a radiation source , collimator and treatment couch , as previously described [ 4 ]  . the system , which is a co60 stereotactic radiosurgery apparatus , is recognised worldwide as an effective method for the treatment of benign and malignant brain diseases , as well as body tumours [ 510 ]  . patients were immobilised by means of vacuum bags which covered the body from the head to the pelvis in a stereotactic frame ; patients were located in the supine or prone position based on the shorter distance from the lesion to surface . 
quiet breathing ( no special breathing restrictions ) was required throughout the period of slow ct scanning ( 10 s / slice ) with a ct slice thickness and slice interval of 5 mm ( somatom emotion 16 ct scanner : siemens , germany )  . 
then ct images were transferred to the planning system via the internet . the gross tumour volume ( gtv ) was the visible extent of the kidney tumour on the ct images . 
to protect renal function , the planning target volume ( ptv ) was formed from the gtv by enlarging it by 510 mm in accordance with tumour size , patient respiratory movements , positioning system error and the relationship dose . 
normal kidney volume was dened as the total kidney volume minus the gtv . three groups of chambers with collimator aperture diameters of 10 , 30 and 50 mm were used . 
the full width at half - height of the dose - eld range at the target was 10 , 30 and 50 mthe treatment plan used a combination of different collimators in the target area depending on the size of the tumour [ 4 ]  . 
dose - volume planning objectives for the oars were dened as follows : normal kidney , liver , mean dose b18 gy ; small mean dose b15 gy ; fig . 
1 dose distribution in the axial view of a patient who had suffered radical nephrectomy of the right renal malignancy and who underwent stereotactic gamma - ray body radiation therapy for a left renal tumour . 
the 50 % isodose line could cover 100 % of the planning target volume ( ptv ) and the 70 % isodose line could cover 95 % of the gross tumour volume ( gtv ) 880 radiol med ( 2014 ) 119 : 878883 intestine , maximal dose b30 gy ; stomach , maximal dose b35 gy ; and spinal cord , maximal dose \27gy . 
for the small intestine and stomach , the maximal dose was expressed as the d0.5cc. follow - up and curative effect assessment after completion of c - sbrt , all of the surviving patients were regularly examined until death or the last clinical follow - up . 
follow - up included medical history , physical examination , blood work and a ct scan on the 1st , 3rd , 6th and 12th month in the rst year after treatment and every 612 months ; thereafter . 
the information regarding recurrence , toxicity and survival were recorded via telephone , mail and local hospital imaging reports . clinical effects were classied on the basis of single diameter measurement and solid tumour response evaluation criteria [ response evaluation criteria in solid tumours [ 11 ] as complete remission ( cr ) , partial ( recist ) ] remission ( pr ) , stable disease ( sd ) and progressive disease ( pd ) according to the ct images . 
reaction to irradiation was classied as early or late side effects according to the radiation therapy oncology group and the european organization for research and treatment of cancer toxicity criteria . statistical analysis statistical analysis was performed using the spss 13.0 software packages ( spss inc , chicago , usa )  . 
the follow - up period was dened as the time from the date of c - sbrt to the date of either death or the last clinical follow - up in months . 
comparison of the renal function index of the nine patients before and after c - sbrt was analysed using the paired t test ; a p value \0.05 was considered statistically signicant . results technical and dosimetric ndings the planning objectives were reached in all of the c - sbrt plans and all of the patients completed radiotherapy . 
2 dose - volume histograms ( dvh ) for stereotactic gamma - ray body radiation therapy illustrating the delivery of a high radiation dose to the gross tumour while sparing adjacent normal structures . 
left kidney mean dose , 13.6 gy ; spinal cord maximum dose , 12.5 gy ; stomach maximum dose , 10.0 gy ; small intestine maximum dose , 9.8 gy ; liver mean dose , 0.1 gy radiol med ( 2014 ) 119 : 878883 table 1 tumour features and treatment outcomes case sex age ( years ) pathology of the primary renal tumour stage clinical effects follow - up ( months ) survival m 71 m 67 m 70 m 77 m 73 m 84 m 58 c clear cell carcinoma , g granular cell carcinoma , p papillary renal cell carcinoma , pr partial remission , sd stable disease , pd progressive disease , pm pulmonary metastasis , mm multiple metastasis , c cardiac diseases , s survival these patients was gradually phased out of the use of analgesics within 3 months after c - sbrt , and the pain experienced by the other two patients was in cr after treatment with oral drugs at low maintenance doses . 
seven patients had died by the end of the follow - up period ; death was caused by multiple metastases in three patients , respiratory failure in three patients as a result of pulmonary metastasis and fig . 
neither temporary nor permanent dialysis was required . discussion the incidence of brcc has been reported to vary from 1.811.0 % [ 12 ] , and it can be subdivided into synchronous and asynchronous tumour types according to the occurrence over time [ 13 ]  . 
the clinical symptoms of brcc are similar to those of unilateral rcc in showing a typical trilogy including lumbago , gross haematuria and a palpable mass , or paraneoplastic syndrome such as fever , hypertension and others . 
however , the applications of nss or minimally invasive surgical techniques are currently limited in patients with large tumours , cardiopulmonary comorbidities , and adhesions between the lesion and the surrounding intestine , or in patients who are unwilling to undergo surgery . 
in these patients , ongoing maintenance haemodialysis after rn results in a poor quality of life . renal cell carcinoma has traditionally been labelled as radioresistant when treated with conventional external beam radiotherapy . 
with constant improvements and the wide application of modern imaging technologies and radiotherapy , clinical outcomes have been further improved . our retrospective study demonstrated that c - sbrt is a promising treatment for local disease control with only minor toxicities in the management of asynchronous brcc . the prominent characteristics of c - sbrt can be summarised as higher precision , higher target dose , higher target conformity and delivery in a lower number of fractions . 
in the present study , a total dose of 3651 gy was delivered to the 50 % isodose line covering 100 % of the ptv at 35 gy per fraction , with 6085 gy to the 70 % isodose line covering 95 % of the gtv . 
the biological equivalent dose ( bed ; a / b = 3 ) regarding the gtv was 160227 gy , which represents an obvious increase as compared with conventional radiotherapy . 
the toxicity of c - sbrt in the current study was very tolerable . the side effects of therapy were mainly myelosuppression and digestive tract reaction which was relieved after symptomatic treatment . 
the gfr had not signicantly declined relative to previously measured values ( p [ 0.05 ) , which indicated that c - sbrt was safe and could effectively preserve renal function . untreated brcc carries a poor prognosis with no survival beyond 1 year . 
the 5 - year survival rate in our study was 35.6 % , which was similar to a 5 - year survival rate of 38 % reported in the literature [ 15 ]  . 
the survival of one of our patients treated using c - sbrt combined with interleukin - 2 ( il - 2 ) was 122 months ; another patient who underwent c - sbrt for pulmonary metastasis as well as combined il - 2 and sorafenib after radiotherapy survived for 65 months , underlining the necessity of comprehensive treatment . the pathologies of brcc are not always the same [ 16 ] and gene mutation may lead to inconsistency [ 17 ]  . 
 [ 18 ] suggested that the characteristics of contralateral metastatic disease were : ( 1 ) multiplicity of tumours on the contralateral side ; ( 2 ) a similar histological pattern ; ( 3 ) absence of encapsulation ; and ( 4 ) occurrence at a short interval after the primary tumours . 
analysis of the clinical information in this series indicated that : ( 1 ) the interval between the tumours appearances on the contralateral side was relatively long ( 42 months ) ; and ( 2 ) the tumours on the contralateral side were relatively large ( 4 cm ) and they were mostly solitary . 
it was also uncertain as to whether the different toxicities were related to the doses received by the oars because of a lack of grade 3 or 4 toxicity in our cohort ; thus , a prospective randomised controlled study is required to further conrm the value of c - sbrt in these patients . ours is the rst study that has focused on asynchronous brcc treated using c - sbrt . 
the results revealed that csbrt could be a feasible treatment for asynchronous radiol med ( 2014 ) 119 : 878883 brcc , especially for the patients who are unable to undergo surgery . 
imaging evaluation of fai , mainly based on plain lm and magnetic resonance evaluation , must be performed according to precise guidelines and is fundamental for reaching a nal diagnosis . 
sconenza dipartimento di scienze biomediche per la salute , universita` degli studi di milano , via morandi 30 , 20097 san donato , milanese ( mi ) , italy imaging techniques used in the diagnosis , and the main radiological signs that may be encountered . keywords hip ( cid : 2 ) femoro - acetabular impingement ( cid : 2 ) pelvis radiography ( cid : 2 ) magnetic resonance arthrography introduction first described by the swiss orthopaedic surgeon reinhold ganz et al . 
 [ 1 ] , femoro - acetabular impingement ( fai ) is a pathological condition that is frequently seen in young active subjects , often in conjunction with top - level sport activities , in which bony components of the hip joint do not match correctly . 
this pathological condition can be caused by an anomalous junction between the femoral head and neck , by an anomalous acetabular shape or orientation , or by a combination of both factors ( the latter event being the most common , occurring in up to 86 % of cases ) [ 2 ]  . femoro - acetabular impingement is currently considered one of the main causes of early hip osteoarthritis , especially in young active subjects [ 2 ]  . despite the extensive literature on this topic , the diagnosis of fai is still challenging and is based on a combination of hip pain , reduced range of movement , positive conict tests , and specic radiological ndings . 
in this setting , normal movements performed when an abnormal anatomical situation is present lead to abnormal contact between the articular surfaces , causing important degenerative abnormalities [ 3 ]  . 
finally , cam - type fai may be also associated with an acetabular undercoverage , which represents residual dysplasia and may have different the load is grades of in this condition , severity . radiol med ( 2014 ) 119 : 103112 fig . 
1 femoro - acetabular impingement : a normal hip ; b cam type ; c pincer type concentrated over a limited area of cartilage , thus favouring early damage and instability , in turn leading to the typical morphostructural alterations [ 9 ]  . symptoms femoro - acetabular impingement generally has a subtle onset . 
sometimes , the hip may snap or partially block due to labral tears [ 10 ]  . radiol med ( 2014 ) 119 : 103112 clinical tests clinical examination of a patient with suspected fai includes three tests [ 11 ]  . ( a ) anterior conict test ( exion , adduction , intra - rotation = fadir ) is considered the most sensitive and specic test . 
with the patient lying supine on the table , the physician exes 90 ( cid : 3 ) the patients knee and rotates it internally , then adding an adduction movement . 
with the patient lying on the table , the physician moves the patients foot of the affected side on the contralateral knee , then applying a mediallateral pressure on the knee of the affected side . 
when positive , the test elicits posterior - lateral gluteal pain . imaging x - ray evaluation patients with a clinical suspicion of fai generally undergo x - ray evaluation rst . 
the anterior acetabular margin is lateral to the posterior margsolid line bottom of the acetabulum ; dotted line ilioischiatic line ; dashed line anterior acetabular margin ; dasheddotted line posterior acetabular margin this condition , both on the femur and on the acetabuluat the beginning of the disease , subtle fai ndings can be seen , while characteristic signs of hip osteoarthritis are not already visible [ 2 ]  . anteriorposterior ( preferably performed with patient standing ) and axial 45 ( cid : 3 ) femoral exion ( also known as 45 ( cid : 3 ) dunn view ) projections should be always performed . 
radiographic evaluation must be always performed on both hips [ 2 , 12 ]  . ( a ) anteriorposterior projection : the patient stands with the lower limbs in 15 ( cid : 3 ) of internal rotation . 
the anterior bump can be detected only in the anteriorposterior projection when located on the superior - lateral headneck junction ; only in the axial projection when located anterior to the headneck junction ; or in both projections when it has a larger extension . 
such abnormality can be quantied by calculating the angle between the major axis of the femoral neck and the base of the femoral headneck junction abnormality [ 1 ]  . 
what was once dened as a herniation pit is now considered as bro - osteitis at the site of impact with the acetabulum in cam - type fai [ 15 ]  . 
for example , an anterior bony bump can be frequently seen in elderly patients affected by plain hip osteoarthritis . the diagnostic performance of radiographic evaluation in fai demonstrated variable results depending on the anteriorposterior the projection considered . 
the bottom of the acetabulum ( arrowheads ) is medial to the ilio - ischiatic line ( dotted line ) when the femoral head is projected medially to the ilioischiatic line , a protrusion acetabuli can be diagnosed . the relationship between the margin of the anterior and posterior acetabular proles on the anteriorposterior projection allows for assessing the physiological acetabular anteversion or retroversion . 
moreover , a lateral pelvic projection is useful to assess the anteriorposterior tilt ( normal value approximately 60 ( cid : 3 ) ) [ 14 ]  . radiol med ( 2014 ) 119 : 103112 fig . 
a the antero - posterior view shows a cross of the anterior ( dashed line ) and the posterior ( dashed dotted line ) acetabular margins . the typical 8 - like pattern can be seen . 
6 wibergs angle can be calculated by tracing a line perpendicular to the transverse pelvic axis and passing over the centre of the femoral head and another line that joins the superior - lateral acetabular roof and the centre of the femoral head . 
for the axial hip projection , the same data were 7074 % and 63 % , respectively , while the dunn projection reached values of 9169 % and 88 % , respectively [ 17 , 18 ]  . 
a recent paper on acetabular retroversion reported that the evaluation of such parameter is burdened by strong interobserver variability , which progressively decreases with increasing observers experience [ 19 ]  . ultrasonography the importance of ultrasonography in the diagnosis of fai is limited . 
7 acetabular intersecting a line that connects the acetabular drops ( arrows ) and another line that courses along the superior - lateral margin of the acetabulum and the femoral head . 
values over 10 ( cid : 3 ) indicate potential instability evaluation of the neonatal hip [ 20 ] , in adults ultrasonography is limited to the detection of intra - articular effusion , evaluation of inammatory , degenerative or post - traumatic conditions , or to the guidance of diagnostic or therapeutic intra - articular injections [ 21 ]  . because the hip is a deep joint , ultrasonography is commonly performed using a low - frequency convex probe . some authors reported that ultrasonography was able to detect most acetabular degenerative tears [ 22 ]  . 
 [ 23 ] , who suggested three qualitative criteria to evaluate the anterior and anteriorsuperior proles of the femoral headneck junction , and to quantify the a angle in cam - type fai . the features of ultrasonography ( low cost , wide availability and lack of ionising radiation ) would make it the ideal imaging modality for preliminary cam - type fai screening . 
however , the results [ 23 ] do not support such a hypothesis , particularly because the evaluation of the a angle alone may not be sufcient for the diagnosis of fai [ 23 ]  . 
finally , as it is unable to evaluate intra - articular 108 radiol med ( 2014 ) 119 : 103112 multiplanar reconstructions oriented along the neck axis , with submillimetre slice thickness . 
computed tomography allows for an accurate evaluation of calcic metaplasia of the labrum , scarcely detectable using magnetic resonance imaging ( mri )  . conversely , mri allows for a more precise evaluation of subcortical bone damage , represented with low signal on t1 - weighted sequences and high signal on t2 - weighted sequences . 
however , the simple mri evaluation allows for a limited analysis of the labrum and of the cartilagelabrum complex , which are of paramount importance when a surgical approach is anticipated [ 24 , 25 ]  . 
it is advisable to perform intra - articular injection under imaging guidance , as it has been demonstrated that hip injection without guidance is burdened by a 40 % rate of failure [ 27 ]  . 
the contrast agent must be injected very slowly , explaining to the patient that the procedure may be variably painful and may be associated with lameness lasting from few minutes to 7 days . within the magnet , the patient is positioned in the supine position , and the feet should be bound together with thus allowing for adhesive tape in 15 ( cid : 3 ) intra - rotation , muscle arthrography examination starts with axial and coronal t1and t2weighted fat - saturated and non - fat - saturated sequences , including the iliac wings and the lesser femoral trochanter . then , t1 - weighted or proton density sequences should be performed , with axial and coronal oblique orientation centred on the femoral neck and with double oblique sagittal orientation centred on the labruthe examination can be completed with radial sequences oriented along the major axis of the femoral neck : these sequences can be included in the standard package provided with the mr system , or isotropic volumetric t1 - weighted sequences can be reformatted in radial planes . 
these sequences have the greater advantage of sections that are always perpendicular to the labrum , with a low occurrence of artefacts , thus allowing a 360 ( cid : 3 ) evaluation of femoral headneck junction [ 28 ]  . 
magnetic resonance in the diagnostic setting of fai , several aspects should be considered . ( a ) evaluation of skeletal morphology : presence of pistol grip - like headneck complex deformity and bumplike irregularity of the femoral headneck junction fig . 
9 computed tomography axial scan ( slice thickness = 3 mm )  . presence of a typically round - shaped os acetabuli ( arrow ) and calcic metaplasia of the anterior labrum ( arrowhead ) abnormalities , ultrasonography has a limited value in the assessment of patients with painful hip . 
10 proton density - weighted fat - saturated coronal oblique scan ( te = 15 ms ; tr = 3 , 310 ms ; slice thickness = 3 mm )  . 
b proton density - weighted fat - saturated coronal oblique scan ( te = 15 ms ; tr = 3 , 310 ms ; slice thickness = 3 mm )  . 
this parameter can be also evaluated on routine noncontrast sequences . ( b ) evaluation of chondral erosion and damage of the femoral head and acetabular surface : it is important to describe the articular rim ( width and symmetry ) [ 29 ] and calculate the extent of chondral damage ( as a percentage or in centimetres )  . 
these parameters cannot be adequately evaluated using standard mri , except for advanced chondropathy associated with subchondral oedema ( hyperintense on t2 - weighted sequences ) , which is extremely important for surgical planning . 
regarding the site , chondral damage occurs more frequently on the anterior superior portion of the acetabulum in cam - type fai , while an posterior inferior localisation is more frequent in pincer - type 110 radiol med ( 2014 ) 119 : 103112 therapeutic options in the literature , there is little agreement on the use of drugs and physiotherapy in patients with fai . 
however , it is a widely held opinion that conservative treatment , being unable to modify the morphological aspects of this condition , cannot represent a real solution [ 33 ]  . patients with hip pain lasting over 6 months , unresponsive to conservative treatment , in whom radiographic signs of fai are present , should undergo surgical treatment [ 34 ]  . three surgical techniques are available for treating the morphological abnormalities underlying fai and the associated lesions : ( a ) open surgery : rst described by ganz et al . 
some orthopaedic surgeons also perform cartilage repair using mitmcroperforations or chondroplasty [ 36 ]  . ( b ) arthroscopy : this is a less invasive technique , but more difcult to perforwithin the articular space , it is possible to treat cartilage tears and reduce the acetabular margin , detaching and re - inserting the labrum ; outside the joint space , it is possible to reduce the femoral bump , checking the disappearance of conict by using dynamic manoeuvres [ 37 ]  . ( c ) mini - open technique : this is a mixed technique , in which femoral neck osteoplasty is performed in open luxation through a small anterior surgery without incision , while intra - articular abnormalities are treated using arthroscopy [ 38 ]  . at similar rates of post - surgical shortand long - term success , arthroscopy has a lower complication rate [ 39 ]  . 
in open surgery , possible complications are trochanter pseudoarthrosis and trochanteric bursitis , heterotopic calcications , and capsular brosis , while in mini - open surgery lateral femorocutaneous nerve lesion is the most frequent complication ( 1745 % ) , followed by transitory neuroapraxis of the pudendal and femoral nerve [ 39 ]  . in patients in whom fai led to advanced osteoarthritis , conservative surgery is contraindicated and hip prosthesis represents the only solution . the role of the general radiologist in consideration of the above , it is clear that fai diagnosis is extremely complex and involves a series of different parameters that cannot be summarised in a single radiological examination . 
13 proton density - weighted fat - saturated coronal oblique scan ( te = 15 ms ; tr = 3 , 310 ms ; slice thickness = 3 mm )  . 
similarly to what happens for the shoulder , conventional mri is able to detect large abnormalities of the labrum , especially when associated with joint effusion that may mimic the arthrographic effect . 
previous studies have shown that conventional mri has 30 % sensitivity and 36 % accuracy in the detection of labral tears , in comparison to 90 and 91 % , respectively , of mra . radiol med ( 2014 ) 119 : 103112 a few years , the scientic community is now facing a possible problem of overdiagnosis . 
indeed , abnormalities that are found in fai are present in a number of asymptomatic subjects and can lead to an incorrect diagnosis if not closely correlated to clinical symptoms [ 2 ]  . in this setting , the general radiologist has a crucial role . on the one hand , some subtle diagnostic signs are not clearly visible on routine radiological examinations . 
this is particularly important , as it is thought that early conservative treatment is able to slow the progression of osteoarthritis , although long - term studies on this topic are still lacking [ 2 , 7 ]  . information to request conclusions fai is a pathological condition with multiple clinical and diagnostic aspects that affect the hip joint . 
orsola - malpighi , bologna , italy results saber - sheath trachea was found in 18 / 71 ( 25.4 % ) patients , with a greater prevalence in patients with lower tiffenau index ( p = 0.02 ) , gold stages iiiiv and visual severity score 3 ( severe ) on chest ct . 
moreover , 52 / 71 ( 73.2 % ) had a chest computed tomography ( ct ) scan available for review ( 16 - slice somatom sensation cardiac 16 , siemens , forchheim , germany )  . images were assessed for the presence of saber - sheath trachea ; radiographic / ct pattern ( negative , emphysematous , bronchitic , mixed ) ; in patients with ct : visual severity score ( 1 = mild , 2 = moderate , 3 = severe ) , visual emphysema score , tracheo - bronchial diverticula , bronchiectases , signs of inammation of the small airways , ossication of cartilage rings , tracheomalacia on expiratory scans , if acquired . 
the nonparametric wilcoxons test for independent samples and the v2 test or fishers exact test were used to compare the continuous and categorical variables with the presence or absence , respectively , of saber - sheath trachea . linear regression was used to verify the relationship between the tracheal index at ct and radiography . 
similarly , the prevalence of saber - sheath trachea was higher among patients with severe - to - very severe copd ( gold stages iiiiv ) as compared to those with mild - to - moderate copd ( gold stages iii ) , with a trend towards statistical signicance ( p = 0.05 , table 3 )  . 
by contrast , no signicant difference was found between patients with and without saber - sheath trachea and the parameters age , sex and radiological pattern of disease . finally , the serial evaluation of patients with more than one available chest radiogram ( 32 / 71 , 45.1 % ) demonstrated that the tracheal index tended to remain constant over time without signicant dimensional changes . at ct , considered the gold standard , 18 / 52 ( 34.6 % ) patients showed saber - sheath trachea . 
he explained that the nding was a result of aging and did not put it in relation to obstructive airway disease , even though the majority of the cadavers examined had emphysema . 
it was not until the 60s that this sign was also reported on standard chest radiography and correlated with copd [ 7 ] , and thus added to the wide range of airway abnormalities that may be encountered in patients with copd [ 813 ]  . nowadays saber - sheath trachea is known to be a specic sign ( specicity , 92.9 % ) of copd , although its reported sensitivity is low ( 39.1 % ) [ 14 ]  . 
among the possible causes of airway remodelling with tracheal narrowing we should recall : stenoses ( post - infectious or iatrogenic ) , neoplasms ( benign , malignant and metastases ) , other conditions ( amyloidosis , sarcoidosis , behcet syndrome , wegener granulomatosis , tracheorelapsing polychrondritis , ulcerative bronchitis associated with crohns disease , etc . ) [ 1 , 15 , 16 ]  . only a few , older , studies have attempted to correlate the presence of saber - sheath trachea with functional parameters : is still a matter of debate whether its development is to be ascribed to parenchyma hyperinsufation [ 3 , 14 , 1719 ]  . 
5 saber - sheath trachea ( st ) is not linked to the radiological pattern of copd : a , b coronal ct reconstruction and axial image in a patient with copd with severe emphysema phenotype ( emphysema visual score , 63 % ) and st ( tracheal index 0.51 ) , c , d coronal ct reconstruction and axial image in a patient with copd with mild bronchitic phenotype and st ( tracheal index 0.56 ) radiol med ( 2014 ) 119 : 9096 fig . 
6 axial inspiratory ( a ) and expiratory ( b ) ct scans in a patient with saber - sheath trachea : tracheomalacia is not documented the results of our study show that saber - sheath trachea is not a constant sign in patients with copd ( 25.4 % prevalence ) , but it is correlated with functional severity , being more frequent in patients with low tiffenau index and with gold stages iiiiv . 
moreover , it is independent of the patients age and sex , in contrast to previous reports , which found a clear predominance among men [ 3 ]  . saber - sheath trachea is therefore a prognostic element that can be detected with no more than standard chest radiography . 
thus , these results require conrmation by a larger study with prospective design . in conclusion , saber - sheath trachea seems to constitute one of the many radiological subphenotypes that copd patients may present with , it is independent from the other radiological signs of disease and it represents an excellent marker of functional severity . 
anxiety may affect ctca image quality in women . comfort , overall greater keywords coronary artery disease ( cid : 2 ) anxiety ( cid : 2 ) conventional coronary angiography ( cid : 2 ) ct coronary angiography introduction computed angiography with tomography coronary ( ctca ) has emerged as one of the most technologically fascinating imaging tools over the last years [ 13 ]  . 
ctca has achieved high sensitivity and negative predictive value in the evaluation of coronary artery disease with applications extending to various clinical settings [ 49 ] and recently reinforced by the excellent prognostic outcome [ 1012 ]  . however , the point of view of the patient and the social acceptance of a method should also be tested for a comprehensive assessment of a modern medical technology the success of a method is undeniably [ 13 ]  . 
in fact , radiol med ( 2014 ) 119 : 128134 associated with the intrinsic acceptance of the method by the patients , who are increasingly pursuing noninvasive and outpatient diagnostic examinations [ 14 ]  . 
exclusion criteria were : refusal to provide informed consent , severe renal impairment ( creatininaemia [ 120 mmol / l ) , known allergy to iodinated contrast media , possible pregnancy , presence of hyperkinetic arrhythmias , severe impairment of respiratory function . 
patients underwent ctca with the following clinical indications : suspected coronary artery disease ( n = 299 ) , atypical chest pain ( n = 152 , 34 % ) , typical angina with inconclusive stress test ( n = 47 , 11 % ) , high cardiovascular risk prole ( n = 52 , 12 % ) , or candidates for aortic valve replacement surgery ( n = 48 , 11 % ) ; follow - up of myocardial revascularisation procedures performed at least 2 years before ctca ( n = 143 ) , including the assessment of the patency of proximal stents ( n = 75 , 17 % ) and bypass grafts ( n = 68 , 15 % )  . 
a history of cca was present in 181 patients . all patients underwent the endler multidimensional assessment of anxiety ( endler multimodality anxiety scales , emas ) before and after ctca , and a multiple choice questionnaire with a ve - point likert scale for the evaluation of acceptance after ctca . 
ct scans were performed with the following parameters : slices / collimation 64 / 0.6 mm , rotation time 420 ms , effective temporal resolution ( with 180 ( cid : 3 ) algorithm ) 210 ms , 120 kv , 8001040 mas , table feed 11.9 mm / s , effective slice thickness 0.8 mm , reconstruction increment 0.4 mm , eld of view ( fov ) 140240 mm ( extended cranially only for evaluating ascending aorta aneurysms and by - pass grafts )  . 
patients with a heart rate [ 65 beats per minute ( bpm ) were given a dose of 2040 mg of propranolol by mouth ( inderal , astrazeneca reims , reims cedex , france ) 1 h prior to the scan to lower the heart rate . 
in the leaet - informing patients on how to prepare for the examination , treatment with 2040 mg propranolol twice daily under physician supervision was recommended in the 3 days prior to the examination to lower and stabilise the heart rate in patients with tachycardia . 
a bolus of 100120 ml of nonionic iodinated contrast agent ( iomeprol , iomeron 400 , bracco , milan , italy ) , according to the scan range , was administered at an injection rate of 5 ml / s using an automatic injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an 18 - gauge needle cannula placed in a right antecubital vein . intracoronary enhancement was optimised by using the bolus - tracking technique , with a region of interest ( roi ) positioned at the level of the ascending aorta in order to synchronise the start of the scan with the arrival of the contrast agent . 
the emas test , while maintaining the traditional constructs of the distinction between state and trait anxiety , represents a multidimensional scale of anxiety that can accurately assess individual responses and anxiety reactions in different situations . 
the emas test is composed of three parts : the emas - state ( emas - s ) , which evaluates state anxiety in relation to autonomic emotional and cognitive components ; the emas - trait ( emas - t ) , which assesses anxiety proneness in four different general contexts [ social evaluation ( se ) , physical danger ( pd ) , ambiguous situations ( am ) , and daily routine ( dr ) ] ; the emas - perception of the situation ( emas - p ) , fundamental control in a research context , which represents a measure of the respondents subjective perception of the type of situation and degree of threat evoked by that situation at the time of testing [ 25 ]  . 
in particular , the following aspects were evaluated : preparation and information before the imaging examination , degree of preceding concern , comfort , helplessness during the examination , pain experienced , degree of overall satisfaction . 
the same questionnaire was formulated also with reference to cca and given to the 181 patients who reported having a history of cca imaging . statistical analysis in all patients before the results of the emas - s test ( emas - si ) and after the performance of ctca ( emassii ) were compared by using students t test ( p \ 0.01 ) , further dividing subjects into subgroups based on gender and presence of cca history . 
the process of the health technology assessment ( hta ) investigates not only the technical reliability and diagnostic performance of a new method , but also aims to assess its prognostic , economic , and social impact , with the primary goal of improving health and wellbeing of the population , by integrating both medical and nonmedical multidisciplinary knowledge and strategies [ 13 ]  . 
therefore , hta needs to combine clinical and scientic evidence with social , cultural and ethical aspects , largely involving the patients , who are the protagonists and beneciaries of a health service [ 27 ]  . 
it is now recognised that full acceptance of a medical procedure or a diagnostic tool by the patient provides more satisfaction , better clinical results , and radiol med ( 2014 ) 119 : 128134 fig . 
in this respect , the following missions are essential for the spread of a modern imaging technique : adequate information and preparation of the patient in a recovered doctorpatient the adoption of noninvasive investigations relationship ; reducing associated anxiety and pain ; less time spent in health facilities , with lower impact on the patients psyche and work activities [ 28 ]  . several studies exist in the radiological literature that investigate the patients acceptance of new noninvasive it was demonstrated that imaging methods [ 1517 ]  . noninvasive methods such as ct virtual colonoscopy [ 15 ] , mr cholangiopancreatography [ 16 ] , and mr angiography of the carotid arteries [ 17 ] are more widely accepted by patients than the traditional invasive approaches [ 1823 ]  . computed tomography coronary angiography provides excellent results in the evaluation of atherosclerotic coronary artery disease due to high sensitivity and negative predictive value , which have enabled its clinical implementation [ 19 ]  . 
the effective 132 radiol med ( 2014 ) 119 : 128134 strategies to reduce the dose of radiation introduced by the latest generation of scanners have helped to further improve the clinical applicability of ctca [ 30 ]  . in our study , the focus was instead oriented on examining the psychological impact of ctca on the patients anxiety and the acceptance of the technique . 
we used the emas test , a tool considered the gold standard for the assessment of anxiety in a clinical / hospital and research context , due to the excellent psychometric properties and the several validation studies of validity and reliability , as well as the presence of italian standardised norms [ 31 , 32 ]  . the advantages of the emas test include : the ease and speed of administration , which is pivotal in a clinical / hospital setting , where the patient is already unavoidably concerned about his own health and the medical procedure ; a very accurate assessment of anxiety in relation to different contexts ; the exibility of using three measurement scales ; the ability to apply the control of perceived anxiety of the situation ( emas - p ) to state anxiety scale ( emas - s ) [ 25 ]  . anxiety was more intense prior to ctca than after , and higher in patients with a previous history of cca . 
ctca had an excellent prole of acceptance by the patient , and better than cca with respect to parameters such as preparation and information , comfort , degree of concern , helplessness , pain experienced , and overall satisfaction [ 14 , 19 ]  . there are a number of limitations to our study . 
the heart rate parameter was inuenced by the pharmacological preparation ( beta - blockers , benzodiazepines ) ; however , diazepam was given before the administration of the emas test in order to equalise the heart rate - state anxiety readings . 
another limitation is that the surveys carried out with specic reference to cca were exclusively performed in 181 patients on the basis of their previous medical history ; the comparison was made only in this subgroup and not on a population undergoing both methods because of the compulsory containment of biological costs of ionising radiation [ 30 ]  . finally , it seems appropriate to emphasise that recovery of the traditional doctorpatient relationship in radiology should be built on the balance between diagnostic performance and patient acceptance , avoiding the consolidation of distorted alliances based on the use of defensive medicine , corporate interests , and patient self - referrals inuenced by the mass - media [ 3638 ]  . conclusions from the point of view of a thorough and multidisciplinary evaluation of diagnostic imaging , ctca , as seen by patients , proved to have an excellent acceptance prole . higher levels of anxiety should be taken into account in women undergoing the examination , because they may partially affect image quality . 
chai ( & ) department of radiology , ruijin hospital , shanghai jiao tong university , school of medicine , ruijin er road 197 , shanghai 200025 , china e - mail : anchorzjrj@yahoo.cn small , prominently solid tumours showing enhancement patterns typical of spts may suggest a diagnosis of spt . keywords solid pseudopapillary tumour ( cid : 2 ) pancreas ( cid : 2 ) computed tomography ( cid : 2 ) male introduction solid pseudopapillary tumour ( spt ) of the pancreas was rst reported in 1933 [ 1 ] , described very well by frantz [ 2 ] , and then dened by the world health organization in 1996 as solid pseudopapillary tumours of the pancreas . 
spt is a relatively indolent tumour ; the prognosis for spt is excellent , with 5 - year survival rates reaching 95100 % [ 3 ]  . solid pseudopapillary tumour is an exceptionally rare neoplasm in males . 
the radiological characteristics of spts have yet to be fully claried in male patients ; thus , spts in men present a diagnostic problein this paper , the imaging features and clinical characteristics of spt in males are described and compared with those of females . 
the ndings obtained will help radiologists recognise distinct characteristics and provide more accurate diagnoses . materials and methods patient selection the institutional review board approved the present retrospective study , and the requirement for informed consent was waived . 
given the unavailability of computed tomography ( ct ) studies for seven patients , only the clinical data and ct studies of 102 patients were included in the present review . 
patients were divided into two groups on the basis of gender : 16 were males ( mean age , 38.5 years ; range 1567 years ) and 86 were females ( mean age 28.7 years ; range 1163 years )  . available records of clinical manifestations , as well as surgical and pathological reports , were reviewed for each patient . 
after each operation , patients were assessed clinically and then followed up by ultrasonography and multidetector ct ( mdct ) for a period of 2162 months ( mean , 97 months )  . ct technique all 102 patients underwent mdct of the abdomen ; different ct machines were used . 
twelve patients underwent 4 - slice , 40 underwent 16 - slice , and the rest underwent 64 - slice mdct scan ( lightspeed 4 , 16 , 64 ; ge medical systems , milwaukee , wi , usa )  . 
after fasting for at least 4 h , all patients were administered 500800 ml of water 30 min prior to the study , and an additional 250300 ml of water was provided immediately prior to the study to achieve adequate distension of the stomach and duodenum . nonionic iodinated contrast material ( omnipaque 300 mg i / ml , ge healthcare ) was administered to all of the patients by a power injector ( ulrich medical , germany ) at a rate of 2.53.5 ml / s through an 18 - gauge intravenous catheter placed in an antecubital vethe dose of contrast material delivered was 1.52 ml / kg body weight . 
sixty patients underwent dual - phase ct during the unenhanced , pancreatic , and hepatic venous phases , while 42 patients underwent triple - phase ct during the unenhanced , arterial , pancreatic , and hepatic venous phases . 
the items included in the imaging analysis were the following : location ( head , neck , body , or tail ) , shape ( round , oval , or lobulated ) , encapsulation ( present or absent ) , and calcication ( present or absent )  . 
the tumours were also evaluated and classied into one of four types according to the existence and proportion of solid and cystic components : purely solid , solid with minor cystic component ( \10 % of tumour with cystic component ) , mixed solid and cystic , and purely cystic . 
the internal ct attenuation characteristics of the tumours were compared with those of surrounding pancreatic tissues and described as follows : hypo - , iso - , or hyperattenuation on enhanced pancreatic phase images ; enhancement pattern ( peripheral or complete ) ; dilatation of the pancreatic duct ; or atrophy of the pancreatic parenchyma . 
images were also evaluated for bile duct dilatation and spread to regional vasculature , lymph nodes , adjacent organs , and distant abdominal sites . statistical analysis quantitative variables were expressed as mean standard deviation . 
no signicant differences were observed between the imaging features of spts in male and female patients with respect to the shape , encapsulation , attenuation , enhancement grade , enhancement pattern , and calcication of tumours . 
radical surgery was performed on 10 male patients , including distal pancreatectomy without splenic preservation on two , whipples operation on three , and concurrent resection of other organs on ve . 
portal vein involvement was seen in four male patients , who subsequently underwent venous resection and reconstruction . thirteen male cases were histopathologically diagnosed as benign spts , whereas the rest were found to be malignant . no signicant differences were found between male and female groups with respect to surgical procedures or malignant spts . 
1 pathologically conrmed benign solid pseudopapillary neoplasms ( spt ) in a 67 - year - old man . a unenhanced computed tomography ( ct ) scan showing a 4.3 cm oval neoplasm in the head of the pancreas with solid lesions . 
b , c pancreatic and hepatic parenchyma phases , respectively : dynamic contrastenhanced ct reveals an illdened mass in the head of the pancreas with initially weak enhancement and slightly progressive ll - in pattern . 
the tumour invaded the adjacent duodenud coronal reconstruction image showing a blurred interface between the tumour and the adjacent duodenumthe tumour had apparently inltrated the duodenum unenhanced and enhanced images . 
c computed axial tomography scan of a pancreas obtained during the hepatic parenchyma phase revealing an almost isodense tumour ( compared with surrounding pancreatic parenchyma )  . d coronal arterial phase ct image shows a hypodense lesion with clear borders fig . 
4 pathologically conrmed benign spt in a 63 - year - old man . a unenhanced ct scan showing a 3.8 cm oval neoplasm in the head of the pancreas with solid lesions with minor cystic components . calcication is seen in the periphery and centre of the lesion . b , c pancreatic and hepatic parenchyma phases , respectively ; dynamic contrast - enhanced ct reveals solid components with progressive ll - in enhanced pattern , however , minor cystic remained unenhanced . 
d coronal pancreatic phase ct image shows minor cystic components in the head of the pancreas characteristics of the pancreatic parenchyma , pancreatic showed tumours with hyperattenuation phase images ( n = 1 ) , isoattenuation ( n = 2 ) , and hypoattenuation ( n = 13 ) in the male patients . 
no statistical difference was observed between male and female patients in terms of calcication . no marked differences were observed in the prevalence of parenchymal atrophy or pancreatic ductal dilatation between the two groups . 
in the male group , parenchymal atrophy ( 2 / 16 ; 12.5 % ) and pancreatic duct dilatation ( 1 / 16 ; 6.2 % ) were present . was achieved in only three patients because of mixed components . discussion solid pseudopapillary tumours currently constitutes about 23 % of all primary pancreatic tumours [ 6 ]  . 
spt is a very rare pancreatic tumour that mainly aficts young females , and only 8.313.5 % of all cases discovered involve males [ 3 , 4 , 911 ]  . 
in 2009 , a total of 1 , 014 cases were reported in a large review of english publications ; only 137 of these were males [ 4 ]  . 
to the best of the authors knowledge , the present study is the largest single - centre study to have analysed the imaging features and clinical characteristics of spts in males . 
furthermore , no prior report comparing the imaging features of spts in males and females has yet been published . the mean age of male patients at the time of diagnosis was signicantly higher than that of female patients [ 46 ]  . our ndings generally agree with this statistic . 
in our retrospective study , the male patients tended to have solid masses ( eight cases had purely solid lesions ) ; this nding agrees with other reports [ 9 , 12 ]  . in the present study , calcication was observed in all parts the tumours , including their periphery , centre , and capsule . 
in our series , none of the patients had a denitive preoperative diagnosis and a correct diagnosis radiol med ( 2014 ) 119 : 8389 a classic ct image of an spt of a young woman showed a large , well - encapsulated mass with internal haemorrhage , solid and cystic components ( often ) brous pseudocapsule and peripheral contrast enhancement , which supports the diagnosis of spt [ 12 , 13 , 15 , 16 ]  . 
imaging ndings for other factors , including shape , encapsulation , attenuation , enhancement grade , and enhancement pattern of the spt , in men are very similar to those in women [ 11 , 12 , 15 , 17 ]  . 
awareness of the radiological and clinical features of spts in males is extremely important in establishing an accurate diagnosis before operation and further operative plans . surgery is the main therapeutic modality for lowgrade malignant spts . 
a good prognosis is expected after surgical resection of primary tumours ; even patients who exhibit distant metastasis have good prognoses as long as the metastatic lesions are resected completely [ 18 , 19 ]  . 
its incidence has been for years considered very low , but the considerable increase in patients receiving anticoagulation therapy for various diseases [ 59 ] ( atrial brillation , valvular heart disease , prophylaxis of deep vein thrombosis / pulmonary thrombo - embolism in addition to the development of increasingly effective anticoagulant , antiplatelet and antithrombotic agents ) has made this complication highly relevant [ 1012 ] , with the annual incidence of major bleeding in patients on oral anticoagulant therapy currently estimated to be 0.23 % [ 13 , 14 ]  . seh treatment consists in suspending anticoagulation therapy with correction of coagulation and restoration of blood volume through uid replacement and blood transfusions [ 3 , 4 ]  . in the case of haemorrhage refractory to transfusions and of arterial bleeding , transcatheter embolisation represents the most valuable therapeutic option because it is able to stop the bleeding with less intraprocedural risk as compared to open surgery [ 3 , 15 ]  . few studies have evaluated the efcacy of endovascular treatment of seh and most of them are limited by small patients series [ 3 , 1621 ]  . 
the objective of this study was to analyse our experience with transcatheter embolisation 122 radiol med ( 2014 ) 119 : 121127 in the treatment of seh to evaluate its effectiveness in terms of immediate and late clinical success , and to compare our data with those reported in the literature . table 1 risk factors risk factors comorbidities materials and methods thirty patients , who underwent endovascular treatment for seh between january 2005 and december 2010 were retrospectively included in the study . 
the study protocol consisted of axial scans at the site of suspected haemorrhage and scans before and after the administration of contrast medium , with post - processing ( table 2 )  . 
on baseline ct , bleeding site was identied as a hyperdense mass attributable to the presence of fresh blood with attenuation values ranging from 60 to 80 hu ; after contrast administration , active bleeding was displayed as a focal area of high density in the arterial phase . in 2 / 30 cases ( 6.6 % ) , the ct study was not performed because of haemodynamic instability ( systolic blood pressure \90 mmhg ) , and the patients underwent digital subtraction angiography ( dsa )  . 
dsa was performed in all patients in the angiography room ( integris v5000 philips , eindhoven , the netherlands ) , with approach through the common femoral artery ( 5f introducer terumo corp . , tokyo , japan ) and local anaesthesia ( 10 ml of lidocaine 2 % )  . 
in cases , where the ct study clearly indicated the bleeding vessel , the treatment involved selective catheterisation of the vessels by means of angiographic catheters ( cobra and vertebral , terumo corp . , tokyo , japan ) ; where the ct scan was not conclusive , angiography with a pigtail catheter ( terumo corp , tokyo , japan ) followed by selective catheterisation of the injured vessel was performed . in the presence of bleeding from small vessels superselective catheterisation was achieved using 0.025 a progreat microcatheter ( terumo corp . , tokyo , japan ) and its 0.021 micro - guidewire which allowed embolisation no . 
of patients anticoagulant therapy ( heparin ) deep vein thrombosis , coronary artery disease , cardiac valve replacement anticoagulant atrial brillation , cardiac valve therapy ( warfarin ) replacement anticoagulant therapy ( fondaparinux ) deep vein thrombosis , coronary artery disease , unstable angina with microcoils ( boston scientic , natick , ma , usa ) and microparticles ( contour 150250 , 250355 , 355500 lm , boston scientic , natick , ma , usa )  . 
when the active bleeding vessels could not be reached , we proceeded to embolise the main afferent vessel with coils of larger calibre ( balt extrusion , montmorency , france )  . the treatment algorithm was as follows : in the case of a bleeding vessel calibre of\1.5 mm ( calculated on the basis of the calibre of the 5f catheter used in the diagnostic phase ) we employed microparticle embolisation , whereas in the case of a calibre larger than 1.5 mm we always used coils , with preliminary use of microparticle injection before coil release in the presence of multiple haemorrhagic foci . 
preliminary contrast - enhanced ct scan shows the presence of a large haematoma in the anterolateral abdominal wall with active bleeding from the supercial circumex artery ( a ) , successfully treated by transcatheter embolisation with particles and coils ( b , c ) inammatory diseases ; especially , of the kidneys or adrenal glands [ 26 ]  . 
in recent years , the incidence of this condition has greatly increased because of anticoagulant therapy and related risks [ 10 ] : in our experience , we have observed a progressive increase in the incidence of seh , with doubling of the cases observed from four cases in 2005 to eight cases in 2010 . endovascular arterial embolisation is nowadays an established therapeutic option in the management of many haemorrhagic conditions [ 2832 ]  . 
there are numerous requests for embolisation of spontaneously bleeding vessels in patients on oral anticoagulants / heparin : we therefore considered it important to present our experience in terms of clinical and therapeutic management and results . not much is known about seh pathophysiology : supposed risk factors are atherosclerosis of small vessels , minor trauma , occult vascular disease of the kidneys and adrenal glands and immune - mediated microangiopathy induced by heparin [ 33 ]  . identifying the site of bleeding and the blood vessels responsible [ 20 ]  . 
in agreement with the literature [ 34 ] , in the case of negative ct , dsa has to be considered the rst option for a correct diagnostic and therapeutic interpretation . the rst - line treatment of seh is conservative : suspension , when possible , of anticoagulant therapy , identication and correction of coagulation disorders , uid infusion and blood transfusion [ 3 , 4 ]  . endovascular treatment with transcatheter embolisation has become the rst choice in seh management because surgery is limited by the difculty identifying and treating bleeding vessels the context of a massive haematoma and the risk that surgical manoeuvres may increase bleeding or re - start a tamponaded bleed [ 30 ]  . the indication for angiography in emergency / urgent settings is established in the presence of persistent anaemia despite adequate transfusion therapy that can be identied in [ 4 u of packed red blood cells in 24 h or [ 6 u of packed red blood cells in 48 h [ 28 ] and on the basis of the considerable experience gained with the treatment of posttraumatic haemorrhage [ 3739 ]  . the diagnosis of seh is essentially based on clinical and laboratory ndings ; ct , however , plays a key role in the diagnostic and therapeutic effectiveness of dsa in the treatment of seh has been documented by recent radiol med ( 2014 ) 119 : 121127 fig . 
dsa is indicated in the case of negative ct examination if required by the patients clinical condition ; in haemodynamically unstable patients , dsa should be performed as the rst - choice examination as the time factor is essential in this setting [ 40 ]  . treatment modalities depend on the operators condence with different materials : in our experience we favoured the use of coils and microparticles as we believe these materials to be more easily handled . 
other reports , however , have widely described the use of absorbable gel ( gelfoam , pharmacia and upjohn , kalamazoo , michigan ) with optimal results [ 40 ]  . 
in cases of difcult micromultiple bleeding vessels catheterisation , proximal embolisation with larger calibre coils is performed . in our experience , transcatheter embolisation achieved complete ( 100 % ) technical success . 
the therapeutic efcacy of dsa was also demonstrated by the statistically signicant reduction of transfusion requirements : is also consistent with the literature [ 27 ] and demonstrates that the technical success of the treatment ( cessation of active contrast leakage at nal angiography ) is associated with clinical success . this result concordance of all published studies on the effectiveness of arterial embolisation in the management of seh allows us to consider this approach the rst - choice treatment option . despite a technical success of 100 % , we observed a postoperative mortality of 10 % ( 3 / 30 patients )  . 
one of 126 radiol med ( 2014 ) 119 : 121127 these patients had arrived with substantially compromised cardiovascular condition ( haemodynamic shock ) and died at 24 h due to multiorgan failure , despite correct embolisation of the bleeding vessels . 
the other two patients died at 48 h due to massive bleeding from new , previously unaffected sites as the patients failed to reach the angiography suite in time for further treatment . 
 [ 33 ] , that spontaneous haemorrhage can be related to a widespread small - vessel disease in coagulated patients which , associated with microtrauma , can produce massive haemorrhagic manifestations . mortality at 6 and 12 months was 14.8 % ( 4 / 27 patients ) and 26 % ( 6 / 23 patients ) , respectively , and not related to haemorrhage or embolic treatment in all cases . this result is consistent with the literature data , documenting a high rate of mortality post - embolisation : pathi et al . 
 [ 20 ] reported that 3 / 4 patients with spontaneous haemorrhage successfully treated endovascularly , died within 30 days of treatment for reasons not related to embolisation or its complications ; rimola et al . [ 17 ] observed that , compared with a complete technical success of embolisation in 12 patients with seh , three patients died within 8 days and four patients within 30 days of treatment , again for reasons not related to in a recently published study , haemorrhage . 
 [ 40 ] , in a total of 25 patients with seh successfully treated with embolisation , observed one postoperative death due to massive bleeding from other sites not previously treated and a 48 % mortality rate at 12 months due to co - morbid conditions . 
these results indicate that even though the treatment is associated with a high technical success rate and a low postoperative mortality , seh occurs in patients with heavily compromised general condition and is , therefore , associated with a poor prognosis [ 40 ]  . in conclusion , on the basis of our experience and the literature data , endovascular treatment of seh represents the treatment of choice , as it can provide complete therapeutic success . 
all prostheses were imaged with both a clinical 1 tesla ( t ) ( signa horizon , general electrics ) and 1.5 t ( achieva , philips ) mri system , using spin echo ( se ) and gradient echo ( gre ) sequences : sagittal t1 se , coronal t2 fast se ( fse ) , axial t1 se , axial t2 fse , sagittal t2 gre , axial t2 * gre , coronal t1 gre , axial t1 gre . 
magnetic resonance imaging ( mri ) may be useful , but it is limited by magnetic susceptibility artefacts that hinder the evaluation of periprosthetic structures , local complications of arthroplasty such as mechanical loosening , prosthetic or periprosthetic fracture , dislocation , infections , heterotopic bone formation and foreign body granulomatosis . 
in computed tomography ( ct ) , beam - hardening artefacts degrade image quality causing errors in image reconstruction [ 3 ]  . mri has a role in the detection of complications owing to its ability to characterise soft tissues and potential bone 114 radiol med ( 2014 ) 119 : 113120 fig . 
1 a prosthesis in cobaltchromemolybdenum ( head and stem )  . a1 axial t2 gre ( gradient echo ) ; a2 coronal t2 fse ( fast spin echo ) ; a3 coronal t1 gre . 
in mri of periprosthetic tissues , some studies have focused on sequence optimisation and on the use of techniques and strategies to reduce ferromagnetic artefacts [ 8 , 11 , 1319 ]  . 
with identical imaging parameters for the different materials , cobalt chrome produced the largest artefacts both in se and gre sequences , followed by titanium and cobaltchrome molybdenum ; ceramic produced the smallest artefacts in all sequences . 
the arrows show the direction of the frequency encoding gradient [ 9 ] but also due to misregistration artefact ; in fact , the clover - leaf pattern became more pronounced with the cobaltchrome prosthesis . around the femoral stem , the signal void followed the longitudinal axis of the prosthesis , with a variable degree of artefact in the direction of the frequency - encoding gradient , as expected [ 10 , 11 ]  . 
substances can be classied as diamagnetic , paramagnetic , superparamagnetic , or ferromagnetic [ 10 ] and the resulting artefacts are different depending on these characteristics . the major mri artefacts associated with implants include geometric distortion of signal intensity in the frequency - encoding direction ( also known as misregistration ) , section thickness variation due to altered excitation proles in two - dimensional imaging , increased signal intensity loss due to diffusion effects from the paramagnetic implant and increased dephasing at ge imaging [ 11 , 12 ]  . misregistration in the frequency - encoding direction creates characteristic signal intensity variations , depending on the implants shape and orientation . 
there is no misregistration in the phase - encoding direction because phase encoding performed with variable amplitudes is immune to misregistration . variation in section thickness is a result of altered excitation proles in a distorted primary magnetic eld . 
in the presence of a mildly distorted primary magnetic eld , an excited section takes on a warped appearance , as it follows isomagnetic lines within the imaging volume . diffusion - related signal - intensity loss increases in the proximity of an implant due to randomly moving water molecules which , in the presence of very large magnetic eld gradients , undergo increased spin dephasing that is not completely recoverable with a refocusing pulse . 
therefore , near an orthopaedic implant , a long echo time , such as that in t2 - weighted se imaging , causes increased signal intensity loss from random processes such as diffusion . there is additional unfortunately , in ge imaging of implants there is no refocusing pulse so that intravoxel dephasing ( t2 * ) which creates marked signal voids . although decreasing the voxel size or shortening the echo time can improve gradient - echo imaging to some degree , the extent of intravoxel dephasing with this sequence usually precludes its use in the evaluation of tissue around the implants . in mri of periprosthetic tissues , some studies have focused on sequence optimisation and on the use of strategies to reduce ferromagnetic artefacts [ 8 , 11 , 1322 ]  . 
in addition , new materials have been introduced . in this study , a comparison of magnetic susceptibility artefacts depending on the physical composition of prostheses was performed , and the utility of some techniques to minimise artefacts produced by orthopaedic hip prostheses has been conrmed . with regard to the physical composition of prostheses , it is important to bear in mind that cobalt is ferromagnetic , radiol med ( 2014 ) 119 : 113120 whereas chrome and molybdenum are not , having molar susceptibilities of 167 9 10 - 6 and 72 9 10 - 6 cm3 / mol - 1 , respectively [ 23 ]  . 
this was followed in decreasing order by titanium which showed a slightly greater artefact size than cobaltchromemolybdenum , both in se and in gre sequences , even though titanium is not ferromagnetic ; by contrast , ceramic had the smallest artefact size . with regard to the inuence of the type of sequence adopted , cobaltchrome was again the material showing the greatest discrepancy in signal loss between gre and se sequences ; thus , cobaltchrome is the most affected by the intravoxel additional dephasing ( t2 * ) characteristic of gre sequences . imaging of periprosthetic structures should avoid gre acquisitions , because of the severity of associated magnetic susceptibility artefacts . titanium instead showed a greater susceptibility to increasing magnetic eld , with greater increases in artefact size at increasing magnetic eld strength . 
in general , all materials showed susceptibility to increases in eld strength ; thus , it could be useful to decrease the eld strength , as this would proportionally reduce both the geometric distortion artefact with the same frequency - encoding gradient strengths , and signal - to - noise resolution . the head of these prostheses has a spherical geometry . the signal void around the head has a clover leaf - like pattern , because of the variations in section thickness around a spherical source , related to the complex section thickness variations at this level , as reported by white et al . [ 1 , 5 ] , but also due to the misregistration artefact ; in fact , the clover leaf pattern becomes more pronounced with cobaltchrome prostheses . 
around the femoral stem , the signal void followed the longitudinal axis of the prostheses , with a variable degree of artefact in the direction of the frequency - encoding gradient , as expected [ 6 , 7 ]  . 
therefore , at clinical mri of a joint prosthesis , it is very important to choose the frequency encoding direction away from the intra - articular structures of interest , and to position the patient with the long axis of the prosthetic implant parallel to the primary magnetic eld [ 14 , 19 ] to disclose them as possible . this study presents some limitations . 
the aim of this retrospective study was to assess the impact of pet / ct on the planning of appropriate treatment for known recurrent disease in operated dtc patients . materials and methods the study concerned 44 consecutive dtc patients ( 36 papillary , 8 follicular ) , who underwent total thyroidectomy and thyroid remnant ablation with 131i and pet / ct . 
all patients had proven or strongly suspected recurrent disease judging from neck ultrasound ( us ) and ne - needle aspiration cytology , and detectable basal tg levels . results pet / ct ndings were positive in 25 / 44 patients ( 56.81 % ) and negative in 19 . 
a positive pet / ct result predicted resectable tumour recurrences in 19 / 25 patients , but also detected additional tumour sites that prompted changes to the treatment plan in 6 / 25 patients ( 24 % )  . 
local recurrences in the thyroid bed or cervical lymph nodes do occur , however , in 1435 % of patients with dtc [ 24 ]  . the clinical follow - up of treated dtc patients is usually based on measuring serum tg levels and various imaging modalities [ 5 , 6 ]  . 
measuring serum tg has its weaknesses ; however , tg autoantibodies cause false low serum tg measurements ; serum tg measurements obtained during thyroid hormone suppression of tsh may fail to identify patients with small residual tumours ; and patients may have aggressive poorly differentiated tumours , despite low tg levels [ 79 ]  . 
procedures for locating recurrences or metastases in the routine followup of dtc patients primarily involve neck ultrasound ( us ) and 131i whole - body scan ( wbs ) [ 5 , 10 ]  . 
neck us has radiol med ( 2014 ) 119 : 97102 proved highly sensitive and specic in assessing the thyroid bed and locoregional lymph nodes [ 1012 ] and is considered the rst - line technique for identifying suspected cervical recurrences during follow - up [ 11 ] ; us - guided neneedle aspiration cytology ( fnac ) can also be performed to increase its sensitivity [ 13 ]  . 
on the other hand , us cannot easily detect recurrences in the central compartment of the neck or in cases of metastatic lesions outside the neck , making it necessary to perform a total body assessment of the extent of the disease by other diagnostic means . wbs has been considered one of the most sensitive diagnostic tools in the follow - up of dtc [ 14 ] , but the ndings are negative in 1030 % of patients with detectable serum tg levels because the tumour cells may lose the ability to trap radioiodine , or the tumours volume may be too small to be detectable at scintigraphy [ 3 , 1517 ]  . 
several studies have shown that 18f - uorodeoxyglucose ( fdg ) - positron emission tomography / computed tomography ( pet / ct ) can identify locally recurrent disease or distant metastases in iodine - negative and tg - positive dtc patients [ 1829 ] , but the diagnostic accuracy of pet / ct vis - a` - vis tg levels is still a matter of debate . 
some authors found that pet / ct performed better in patients with high tg levels [ 20 , 23 , 25 ] , others found it helpful even in cases with low tg levels [ 20 , 22 ] , and some investigators reported nding no correlation between the results of pet / ct and serum tg levels [ 28 ]  . 
there is also no denite cut off at which an optimal accuracy of pet / ct can be assumed [ 24 , 27 ]  . although several studies have focused on the diagnostic accuracy of pet / ct in operated dtc patients with high serum tg levels , but negative wbs ndings , there is still a paucity of information available on other possible indications for pet / ct . 
the aim of this retrospective study was to ascertain whether pet / ct can contribute to the planning of therapy for known local recurrent disease in operated dtc patients , irrespective of their serum tg levels . materials and methods patients this study was conducted in full accordance with the guidelines issued by the local institutional review board . the need for direct informed consent was waived . 
the study was a retrospective analysis of the medical records of patients with dtc who underwent total thyroidectomy and had at least one cycle of rai therapy for thyroid remnant ablation between january 2008 and december 2009 . 
overall , 44 / 104 dtc patients ( 42.30 % ) met these inclusion criteria and gender female male histology papillary follicular stage i stage ii stage iii stage iv surgery 30 ( 68.18 % ) 14 ( 31.81 % ) 57 ( 2881 ) 36 ( 81.81 % ) 8 ( 18.18 % ) 10 ( 22.72 % ) 3 ( 6.81 % ) 19 ( 43.18 % ) 12 ( 27.27 % ) 40 ( 90.90 % ) 4 ( 9.10 % ) table 1 patient characteristics characteristics total ( n = 44 ) median age , range ( years ) initial disease staging ( according to 6th edition ajcc ) a total thyroidectomy total thyroidectomy plus lymphadenectomyb 7 ( 15.90 % ) 37 ( 84.09 % ) rai ablative activity ( gbq ) a american joint committee on cancer ( 2002 ) b unilateral cervical lymph node dissection formed our study sample , which included 14 men and 30 women ( median age 57 years )  . 
the characteristics of the study population are reported in table 1 . tg measurement blood samples for serum tg ( and anti - tg antibody ) evaluation were collected during thyroxine suppressive therapy . 
serum tg levels were considered pathological if measurable ( value [ 1 ng / ml )  . pet / ct technique all pet / ct studies were performed at our institution on a biography 16 scanner ( siemens medical solutions , il , us )  . 
together with the pet system , the ct scanner is used both to correct radiol med ( 2014 ) 119 : 97102 the attenuation of the pet data and to locate fdg uptake on the pet images . 
patients fasted for at least 6 h prior to imaging and were asked to drink mineral water freely within the fdg uptake time to stimulate diuresis and obtain an adequate distension of the intestinal walls . 
the gaussian lter was applied to the reconstructed image in the axial and transaxial directions . the data were reconstructed over a 128 9 128 matrix with a pixel size of 5.25 mm and a slice thickness of 5 mthe processed images were displayed in the coronal , transverse , and sagittal planes . the pet / ct images were interpreted by two experienced physicians . 
a standardized uptake value ( suv ) was measured for all positive lesions and presented as the maximal suv ( suvmax )  . wbs technique diagnostic wbs was performed after thyroxine had been discontinued for at least 4 weeks and a low - iodine diet followed for at least 6 weeks . 
in brief , wbs was performed 72 h after the oral administration of 185 mbq of radioiodine , using a dual - head gamma camera ( ecam ; siemens medical solution , il , us ) equipped with a high - energy collimator . anterior and posterior wbss were obtained , plus spot images of the neck and chest ( acquisition with matrix 256 9 256 , zoom 1 )  . 
finally , progressive disease was considered in the presence of increased serum tg levels and / or evidence of disease progression on imaging . a patient - based analysis was performed . 
cohens k statistics was used to measure agreement between procedures . results in all 44 patients , the use of pet / ct was based on the nding or strong suspicion of recurrent disease at a single neck site after us and fnac . 
on a patient - based analysis , pet / ct conrmed recurrent disease at a single neck site in 25 / 44 patients ( 56.81 % ) who underwent this test for the purposes of planning curative re - surgery ; the method also detected additional tumour sites that prompted changes to the treatment plan in 6 / 25 patients ( 24 % )  . 
among these 19 patients with negative pet / ct ndings , 11 were only followed - up , 5 had further rai therapy , and 3 underwent repeat surgery with radical intent . at the time of our analysis , overall 19 of the 44 patients ( 43.18 % ) were disease free , 9 ( 20.45 % ) had a stable disease , 11 ( 25 % ) had a progression of disease and 5 ( 11.36 % ) were lost . 
neck us is considered the most sensitive diagnostic tool for local recurrences in dtc patients [ 32 ] , but the chances of curative surgery in cases with localised disease justify the search for residual cancer at sites inaccessible to us - guided fnac , or unexpected metastases outside the neck . to date , there have been few studies involving pet or pet / ct in the work - up of dtc patients with recurrences detected by various other imaging techniques . 
although some authors observed no correlation between fdg uptake and thyroid hormone levels [ 22 , 28 , 34 ] , other studies showed that the chances of positive ndings on pet / ct increase with high or rising tg levels [ 20 , 21 , 24 , 35 ]  . 
another explanation for the number of patients found negative at pet / ct in our series lies in the fact that patients were not selected in the light of an increase in their tg levels between two successive measurements . 
our results also indicate , however , that pet / ct ndings could be positive in patients with serum tg levels below 5 ng / ml as well , which is consistent with the fact that there is still no precise tg cut off for selecting dtc patients that warrant pet / ct examination . we found that pet / ct had a clinical impact even when its outcome was negative : the absence of fdg uptake correlated with a less aggressive disease and prompted a follow - up more conservative treatment approach ( i.e. , alone in most cases )  . there was a lack of agreement between pet / ct and wbs ndings in this study ( k = 0.1 ) , conrming that the sensitivity of these two techniques in thyroid cancer depends on the cells metabolic activity [ 24 , 36 ] , and suggesting that one of the two methods cannot be used in lieu of the other . it would be most interesting to know whether using pet / ct in patients whose us - guided fnac demonstrate or raise a strong suspicion of recurrent disease at a single neck site would inuence their clinical course and ultimate survival , but this question remains to be answered . limitations of the present study are the short follow - up period ( since dtc is known to grow slowly ) , and the small number of subjects evaluated . 
for this reason , our ndings should be validated on a larger series of patients . to conclude , pet / ct can add to the information provided by neck us and fnac when it comes to diagnosing recurrent or metastatic dtc , thus helping to improve the clinical management of patients after thyroidectomy and rai therapy . 
stavropoulos soa anagnostopoulou received : 19 april 2012 / accepted : 28 may 2012 / published online : 3 december 2013 ( cid : 2 ) italian society of medical radiology 2013 abstract purpose this paper presents a technique of ultrasoundguided localisation and block of the musculocutaneous nerve through the anterior wall of the axilla . materials and methods twenty patients ( 7 males and 13 females ; mean age , 35 years ) had axillary nerve block for upper extremity trauma . 
with the arm adducted , ultrasound probe was positioned on the anterior axillary wall ; the axillary artery , coracobrachialis and pectoralis major muscles and lateral cord of brachial plexus were visualised in cross section . 
with continuous imaging of the axillary artery in cross section , the ultrasound probe was slowly moved towards the biceps muscle until the musculocutaneous nerve appeared crossing the coracobrachialocalisation lis muscle . 
the quality of sensory and motor nerve block , as well as of ultrasound imaging were evaluated . results ultrasound - guided block of the musculocutaneous nerve was excellent and complete in 18 of the 20 z . 
no patient experienced pain or tourniquet discomfort during surgery , or any other nerve block - related complication . conclusion the anterior axillary ultrasound view provides for complete nerve block and imaging of the entire course of the musculocutaneous nerve and its relations with adjacent structures with excellent quality . keywords musculocutaneous nerve ( cid : 2 ) ultrasound imaging ( cid : 2 ) axillary block ( cid : 2 ) anterior axilla wall introduction the axillary block is the most distal block performed on the brachial plexus . 
however , because the musculocutaneous nerve leaves the brachial plexus sheath proximal to the site of injection , axillary block often results in inconsistent coverage for tourniquet pain , as well as anaesthesia of the volar aspect of the skin below the elbow that extends to the thenar eminence [ 17 ]  . the musculocutaneous nerve arises from the lateral cord of the brachial plexus , opposite the lower border of the pectoralis major muscle , its bres being derived from c5 , c6 and c7 nerve roots . 
the median , ulnar and radial nerves all travel with the axillary artery within the axillary sheath [ 14 ] , whereas the musculocutaneous nerve has already left this sheath , crossing the coracobrachialis muscle [ 5 ]  . therefore , the musculocutaneous nerve must be blocked separately during an axillary nerve block . 
however , 136 radiol med ( 2014 ) 119 : 135141 variations and irregularities of the musculocutaneous nerve , such as double , short or absent nerve , adherence or fusion with the median nerve and variable course through or beneath the coracobrachialis and biceps brachii muscle may complicate localisation and blockade of the musculocutaneous nerve in the axilla [ 1 , 2 , 6 , 7 ]  . ultrasound - guided nerve block has greatly facilitated nerve localisation and blockade in regional anaesthesia [ 8 10 ] , especially for nerves such as the musculocutaneous nerve that do not have predictable relationship to easily identiable vascular structures [ 1014 ]  . 
using a standard axillary ultrasound - guided approach to the musculocutaneous nerve , the patient is placed in the supine position with the arm abducted and externally rotated ; the ultrasound probe is positioned at the base of the axilla , at the junction of the pectoralis major and biceps muscle [ 1012 ]  . the musculocutaneous nerve is found at the juncture between the biceps and coracobrachiales muscle [ 1012 ]  . however , anatomical and ultrasound studies have described variations in the exact anatomical location of the musculocutaneous nerve in 022 % of cases [ 7 , 1526 ] ; in these cases , the nerve was outside the coracobrachialis muscle , near the axillary artery , or more frequently near or fused with the median nerve in a common trunk [ 17 , 18 ]  . 
in addition , using a standard axillary ultrasound - guided approach to the musculocutaneous nerve the position of the nerve outside the coracobrachialis muscle and its course from the lateral cord of the brachial plexus to the biceps brachii muscle could not be detailed [ 26 ]  . 
moreover , the injection needle of the local anaesthetic is brought into the ultrasound beam in the axial section , and could be easily missed as it appears as a small dot in the ultrasound images . 
to address these problems , we performed this study to present a technique for axillary nerve block of the musculocutaneous nerve using an anterior axillary ultrasoundguided approach . materials and methods twenty patients had an axillary nerve block for surgical treatment of upper extremity trauma including distal radius fractures ( 14 patients ) and scaphoid fractures ( 6 patients ) from february 2009 to april 2010 . 
all axillary nerve blocks were performed using the same technique as described below , by the same anaesthesiologist ( t.s. ) with an 8 - year experience in ultrasound - guided regional anaesthesia . 
motor and sensory block was graded as normal motion / sensation or incomplete block , decreased block and complete block . inability to move the ipsilateral biceps brachii muscle against gravity was considered the motor block endpoint . complete absence of pinprick sensation to the lateral aspect of the forearm ( lateral antebrachial cutaneous nerve ) was considered the sensory block endpoint . 
the quality of ultrasound imaging of the entire course of the musculocutaneous nerve in the axilla , the axillary artery and vein , and the coracobrachialis , pectoralis major and biceps brachii muscles was graded as excellent , difcult or unfeasible . 
in both these patients , the nerve block was repeated successfully with the same technique . the quality of ultrasound imaging of the musculocutaneous nerve , the axillary artery and vein , the coracobrachialis , biceps brachii and pectoralis major muscles was excellent in all patients , without any difference between the two ultrasound scanners and probes with different resolution used in this series . 
the musculocutaneous nerve was clearly seen along its entire course from the lateral cord of the brachial plexus , crossing coracobrachialis muscle , to the junction with the biceps brachii muscle . 
fusion of the musculocutaneous with the median nerve was observed in one patient , while in another patient the nerve was not found and was probably also fused with the median nerve . 
in addition , the next day no residual patient anaesthesia , or any other nerve block related complication . dysaesthesia , paraesthesia , reported discussion traditionally , anatomical landmarks have been used to identify needle insertion sites for nerve blockade [ 5 ]  . however , the degree to which these landmarks are appreciated depends on multiple variables , such as body habitus , distortion of anatomy from prior surgical operations , ability to position the patient and vascular disease . 
therefore , alternative techniques for nerve localisation , such as ultrasound - guided techniques for regional anaesthesia in both the upper and lower extremities have evolved [ 12 , 14 , 27 , 28 ]  . 
inset pulse wave doppler used for the identication of the axillary vessels ( v axillary vein , a axillary artery , m - mcm musculocutaneous - median nerve , p posterior cord , l lateral cord ) that it affords the anaesthesiologist the real - time ability to visualise the target nerve of interest , direct the needle and witness local anaesthetic spread [ 27 ]  . 
the musculocutaneous nerve does not have predictable relationship to adjacent structures in the axilla [ 1014 ] ; localisation of the nerve is atypical in up to 22 % of axillary blocks [ 7 ]  . 
our results showed that this technique provides for excellent localisation of the musculoskeletal nerve and its entire course from the lateral cord of the brachial plexus to the biceps muscle , and complete motor and sensory nerve block . at the axilla , the lateral , medial and posterior cords of the brachial plexus are divided into their terminal nerve branches . 
the lateral cord divides into the musculocutaneous nerve and radiol med ( 2014 ) 119 : 135141 the lateral portion of the median nerve , the medial cord divides into the ulnar nerve and the medial portion of the median nerve , and the posterior cord divides into the radial nerve and axillary nerve . 
in most arms , the nerve pierces the coracobrachialis muscle and then passes between the biceps brachii and brachialis muscle , supplying each of these muscles [ 7 , 29 , 30 ]  . however , in 830 % of arms , the musculocutaneous nerve may accompany or fuse with the median nerve , as occurred in 2 of the 20 patients in this series , without entering the coracobrachialis muscle [ 13 ]  . 
it may adhere for some distance to the median nerve and then pass outwards , beneath the biceps brachii , instead of through the coracobrachialis muscle , or it may pass under the coracobrachialis or through the biceps brachii muscle [ 1 , 2 , 6 ]  . 
these variations may complicate localisation and blockade of the musculocutaneous nerve in the axilla [ 7 ]  . currently , multiple techniques are used to localise the musculocutaneous nerve for local anaesthetic nerve block . these techniques include direct injection into the coracobrachialis muscle , injection along the humerus , paraesthesia seeking , generation of a biceps contraction by use of nerve stimulation , ultrasound , perivascular and transarterial techniques [ 5 , 31 ]  . 
with the paraesthesia - seeking and nerve - stimulating approaches , all four nerves ( median , ulnar , radial and musculocutaneous ) can be individually identied and anaesthetised in the axilla ; both these methods seem to be equally successful . however , in procedures using the nerve - stimulation technique , actual stimulation of the musculocutaneous nerve leads to a more successful outcome than a simple injection into the coracobrachialis muscle . 
moreover , the aforementioned techniques rely on anatomical assumptions of normal neural anatomy and on palpation of internal anatomy , such as the coracobrachialis muscle , biceps muscle and axillary artery to guide needle placement [ 12 , 32 ]  . 
the degree to which these landmarks are appreciated depends on multiple variables , such as body habitus , prior surgical distortion of anatomy , ability to position the patient and vascular disease [ 12 ]  . ultrasound guidance is an attractive option for neural structures , such as the musculocutaneous nerve , that do not have predictable relationships to easily identiable vascular structures [ 12 ]  . 
needle insertion can be done with the in - plane approach ( the needle itself is imaged in its long - axis ; complete needle visualisation ) , or the out - of - plane approach ( the needle is imaged in its short - axis ; limited view , the operator cannot be assured that the needle tip is being imaged in contrast to part of the shaft )  . 
the main downside to the in - plane technique is that the ultrasound beam is very thin and it can be frustrating and difcult to continuously maintain needle imaging [ 32 ]  . the frequency of the ultrasound system is directly related to the resolution of the system [ 7 ]  . 
however , higher frequency systems do not penetrate deeply into the body , thus preventing effective imaging of deep structures because of ultrasound attenuation ; higher frequency ultrasound attenuates at more supercial depths than lower frequency ultrasound [ 7 ]  . since the initial report of a high - resolution ultrasound technique to visualise and block the musculocutaneous nerve [ 12 ] , no large clinical study on musculocutaneous nerve localisation in the axillary area has been available . 
in that study [ 12 ] , the authors identied the musculocutaneous nerve by placing the transducer over the base of the axillary pyramid where the musculocutaneous nerve seems to exit the axillary cavity by piercing the coracobrachialis muscle . an ultrasound study in healthy volunteers described median , ulnar and radial nerve localisations around the axillary artery , but their limited ultrasound resolution rate precluded any musculocutaneous nerve localisation [ 26 ]  . other authors described the ultrasound appearance of the musculocutaneous nerve in the axilla to suggest potential areas to target neural block [ 13 ]  . 
however , placing the ultrasound probe at the base of the axilla , as per the standard ultrasoundguidance techniques , often makes it difcult to accurately visualise the origin of the musculocutaneous nerve from 140 radiol med ( 2014 ) 119 : 135141 the lateral cord of the brachial plexus , and its relationship with the coracobrachialis muscle [ 12 , 26 , 38 ]  . 
by sliding the ultrasound probe at the base of the axilla and trying to follow the musculocutaneous nerve to the apex , the axillary cavity further narrows ; hence , it is almost unfeasible to depict the entire anatomical course of the musculocutaneous nerve from the lateral cord of the brachial plexus to the biceps brachii muscle without having to angulate the ultrasound probe considerably . 
placing the probe at the base of the axilla , also makes it difcult to visualise the lateral cord of the plexus , the exit of the musculocutaneous nerve from the lateral cord , the coracobrachialis muscle and the axillary artery because these structures are located deep in the axillary fossa [ 7 , 12 , 29 , 30 , 38 ]  . 
last , during injection of the local anaesthetic , if the needle is brought into the ultrasound beam in the axial section , the needle shaft appears as a small dot which can be easily missed . 
in the present study and our practice , positioning the ultrasound probe on the anterior wall of the axilla provides for crosssection visualisation of the lateral cord of the brachial plexus , the musculocutaneous nerve , the axillary artery and vein and the coracobrachialis muscle . 
although the probe is slowly brought towards the biceps brachii muscle , the entire course of the musculocutaneous nerve from the brachial plexus cords , crossing the coracobrachialis muscle to its terminal branches , its relationship with the anatomical structures of the axilla , and any anatomical variations can be clearly recognised . 
finally , the injection needle is advanced in the longitudinal plane of the ultrasound beam ( in - plane technique ) ; therefore , the operator can see the entire needle and make adjustments as needed . we see three limitations in this study : rst , this study did not include a control group of patients , and has not been compared with anatomical dissection . 
second , the resolution of our ultrasound device may have not allowed us to explore the thin connections between musculocutaneous and median nerves , which could be observed in up to 46 % of arms in cadavers [ 23 , 25 ]  . 
furthermore , by increasing the resolution of the system ( higher mhz ) , the depth of penetration would have been reduced [ 23 , 25 ]  . third , we used two different ultrasound scanners and probes with different resolution . 
however , with the probes used in the present series , no difference was observed regarding imaging quality during the procedure ; both ultrasound probes are new generation ones and of the same frequency bandwidth . in conclusion , the technique presented uses an anterior ultrasound axillary view of the musculocutaneous nerve . the advantages of this approach are ( 1 ) the musculocutaneous nerve can be followed throughout its course in the axilla , from the cords to the terminal branches , thus identifying possible variations and abnormalities , ( 2 ) it allows cross - section visualisation of the lateral cord of the plexus , the musculocutaneous nerve , the axillary artery and vein , and the coracobrachialis muscle and ( 3 ) the injection needle is advanced in the longitudinal plane of the ultrasound beam , so the operator can see the entire needle and make adjustments as needed . 
in this study , our aim was to investigate the relationship between work stress and metabolic syndrome in a population of radiologists . materials and methods radiologists and radiotherapists taking part in scientic conferences were invited to compile a questionnaire to evaluate work stress and the main parameters for diagnosing metabolic syndrome ( obesity , hypertension , elevated cholesterol level , elevated triglycerides , and hyperglycemia )  . results most of the doctors taking part in the survey ( n = 383 , 58.6 % ) were found to have at least one pathological component ; 47 subjects ( 7.1 % ) had metabolic syndrome . 
all the variables indicating work stress , whether derived from karaseks demand / control model or from the effort / reward model devised by siegrist , were signicant predictors of metabolic syndrome components . 
in fact , it is thought that the latter together with life styles accounts for approximately one - third of the effect of stress on the risk of cardiovascular disease [ 4 ]  . radiologists can be exposed to considerable environmental pressure [ 5 , 6 ] that may lead to a prolonged state of occupational stress [ 7 ] and a reduction in job satisfaction [ 8 ]  . 
our cross - sectional study is a rst attempt to address this issue . materials and methods since italian radiologists and radiotherapists are increasingly being accused of alleged malpractice [ 1018 ] , we decided to use a questionnaire to investigate the possible health effects resulting from such accusations [ 19 ]  . 
a total of 654 completed responses were returned . the questionnaire examined the perception of occupational stress through the simultaneous use of the two commonest stress models : the karasek demandcontrol support ( dcs ) model [ 20 ] and the effortreward imbalance ( eri ) model devised by siegrist [ 21 ]  . according to the dcs model , a work environment where there is a high level of psychological demand ( frenetic pace , contradictory , and excessive demands ) and a low level of job control , exposes the worker to job stress . 
high strain jobs characterized by elevated demand and low control , lead to a greater risk of negative mental and physical health effects as compared to the other three groups . 
in active jobs , characterized by high demand and high decisional power , enhanced autonomy enables workers to avoid becoming the victims of stress . similarly , in the other two categories , workers with low strain and high discretionary power , or passive workers ( with low demand and low control ) are not exposed to occupational strathe four groups are established by dividing the scores of the demand and control scales at the median . 
the dcs model was the rst to demonstrate the association between stress and pathologies ; much of the literature is based on this model [ 23 27 ]  . according to the eri model , stress originates from an imbalance between the effort required to perform work and the material or immaterial rewards obtained thereby . 
in this model , imbalance is calculated once more as a weighted ratio between effort and reward and is a continuous variable that can be divided at the median to obtain categories of workers who are more or less exposed to stress . 
although the karasek model provides a perfect picture of the repetitive tasks of the rst industrial revolution when work was conditioned by machinery , the siegrist model seems better suited to interpret the occupational conditions of the second industrial revolution where work has taken on a more immaterial aspect and is more invasive . 
in fact , in recent years , there has been a considerable increase in the number of studies based on this model . their ndings have shown that the combination of high effort and low reward constitutes a risk factor in numerous illnesses [ 2933 ]  . 
however , the two models offer a complementary rather than alternative solution , so a combination of the two questionnaires can provide better information on the relationship between work and health [ 34 , 35 ]  . both questionnaires are available in different versions . despite their different composition , these provide homogeneous results [ 3638 ]  . 
the questionnaire included a third , overcommitment , scale ( alpha = 0.91 ) made up of six questions ( e.g. , people who know me well say that i am too committed to my work )  . 
the responses were scored on a 5 - point scale where a value of 1 corresponded to : strongly disagree , does not apply ; a value of 2 to : agree but i am not distressed and a value of 5 to : strongly agree , i am greatly distressed . metabolic factors were investigated using the following questions : level ? ( threshold : 40 mg / dl males , 50 mg / dl females )  . 
what is is your hdl - cholesterol what 144 radiol med ( 2014 ) 119 : 142148 table 1 characteristics of the study population your blood pressure ? ( threshold : 130 / 85 mmhg )  . 
what is your fasting glycemia level ? ( threshold : 100 mg / dl )  . what is your waist circumference ? ( threshold : 102 cm males , \88 females )  . 
table 1 illustrates the characteristics of the study population . a total of 274 subjects ( 41.9 % ) reported abnormal hdl cholesterol levels , while 74 subjects ( 11.3 % ) reported an increase in triglycerides . 
forty - six subjects ( 7.1 % ) who manifested three or more simultaneous pathological abnormalities were diagnosed as having metabolic syndrome ( table 2 )  . by analyzing the variables correlated to work stress ( table 3 ) , we were able to build up a prole of this category of workers . 
on average , radiologists claimed that they had a high workload ( the mean score for the demand variable was close to maximum values for the scale ) , but a good level of control over their work . 
on the other hand , those who worked at an excessively fast pace and were unable to adequately control their work ow were exposed to risk . the mean score for the job strain variable was higher than one , indicating excessive psychological strain compared to that could be exercised . 
the tendency towards overcommitment was quite widespread and this aggravated the situation . linear regression analysis indicated that all the occupational stress variables were signicantly associated with a prevalence of metabolic syndrome components . 
the increase in demand , effort , overcommitment , job strain or effort / reward imbalance , and the reduction in support or reward were associated with more frequent signs of pathology . 
data adjustment for age , gender , and lifestyles did not alter these associations ( table 4 )  . logistic regression provided proof that radiologists with higher stress levels , measured by both models , were at greater risk of manifesting a complete metabolic syndrome . even after correction for confounding factors ( sex , age , and the relationship was still statistically highly lifestyles ) , signicant . 
the mean psychological effort needed to perform tasks was not held to be excessively elevated ( we must consider that we are dealing with highly qualied and professional physicians ) , but the immaterial rewards they receive from their work were not always satisfactory . 
this meant that a signicant number of radiologists worked in a state of effortreward imbalance , as they obtained less than they our study demonstrated that radiologists with higher stress levels run a fourfold to sixfold greater risk of being affected by metabolic syndrome than radiologists with lower levels of stress . 
to our knowledge , this was the rst study to take this category of workers into consideration to examine the association between stress and metabolic diseases . our study ndings are in agreement with the literature . stressful life events have been found to induce the onset of metabolic syndrome in the general population [ 40 ]  . 
in workers who develop a post - traumatic disorder after 146 radiol med ( 2014 ) 119 : 142148 exposure to traumatic events , there was a signicant increase in metabolic syndrome [ 41 ]  . 
other occupational risk factors , such as loss of sleep due to shift work [ 42 , 43 ] and depression , which is also often associated with stress , are linked to metabolic syndrome [ 44 ]  . 
workers affected by burnout show a signicant increase in the prevalence of metabolic syndrome components , such as hypercholesterolemia , high blood pressure , and obesity [ 47 ]  . the relationship between stress and obesity is rather complex and there are conicting ndings in the literature . a study conducted in finland with the two stress models we used in this study showed that the lowest control and demand values and the highest levels of job strain and effort / reward imbalance are associated with an increase in body mass index ( bmi ) in males [ 48 ]  . 
these discrepancies can be explained by the fact that researchers used a cross - sectional study design or , in longitudinal studies , failed to take into consideration the physical condition of the workers at the beginning of the experiment . 
findings from the whitehall ii study indicated that thin subjects who were exposed to high job strain and low control tend to get thinner , while those who are initially overweight tend to put on more weight when they are under stress [ 50 ]  . 
a recent analysis summarizing the ndings of 13 studies conducted in europe , conrmed that there is a u - shaped association between stress and body weight , whereby thin subjects lose weight , while obese individuals get fatter [ 51 ]  . clearly the relationship between stress and metabolic syndrome is so complex that it would be difcult for a single cross - sectional study to draw any denite conclusions . 
our single study is not sufcient to exclude the possibility of inverse causality , i.e. , that it is the onset of metabolic syndrome or its components that are responsible for an increase in work stress , even though knowledge of the literature would seem to exclude such a hypothesis . the second important in our study regards the voluntary participation of the radiologists . because the cases were not randomized , the prevalence of the disorders reported cannot be extended to all italian radiologists . 
a study conducted in the marche region of italy found a metabolic syndrome prevalence of 11.5 % in the 3642 age group and of 22.5 % in subjects between the age of 43 and 60 years [ 54 ]  . 
this demonstrated that sample group at least , the health level of italian doctors was higher than that of the general populationa fact that had already been ascertained in previous epidemiological studies [ 55 ]  . 
it also indicated that the subjects taking part in our study were not prompted to do so because they were suffering from one of the conditions under investigation . this was important since we know that being affected by any morbid condition induces individuals to be more precise when recalling all the possible causal factors for that illness . 
our statistics were , however , also adjusted for gender . since there was no collection of analytical or objective data in our study , the third limitation concerns the fact that it was not possible to verify the accuracy of the responses given . 
in epidemiological studies where self - assessment is made of both the risk factors and their consequences , what is known as common method variance may occur , i.e. , individuals with negative affectivity tend to give a negative answer to all the questions , thus , inuencing the strength of the association between risk factors and outcome . 
however , it has been shown that this is not an automatic process and that when it occurs it has little effect [ 56 ] and tends to diminish the strength of the association rather than boost it [ 57 ]  . 
in our case , the fact that the radiol med ( 2014 ) 119 : 142148 individuals questioned were all doctors makes us condent with regard to the accuracy of the clinical parameters reported . our study demonstrated that radiologists are an occupational category that is exposed to considerable number of critical situations and that they often suffer from stress even though they carry out their work in a highly protected and controlled environment . 
the prevalence of blood pressure , obesity , dyslipidemia , and diabetes was higher in subjects with a more elevated level of job strathis nding should encourage researchers to carry out more prospective studies . 
depending on their position relative to the heart , they are classied into ( 1 ) an anterior group situated between radiol med ( 2014 ) 119 : 2026 fig . 
3 axial computed tomography ( ct ) scan showing the position of the extrapleural lymph nodes ( white ) in adipose paraspinal tissue near the costovertebral joints they receive afferent vessels from the parietal pleura , diaphragm , liver and abdominal wall [ 6 , 7 ]  . 
extrapleural lymph nodes are located in a triangular area at the costovertebral joint , near the head of the rib , in the adipose paraspinal tissue [ 7 ]  . 
the retrocrural space communicates with the posterior mediastinum above and with the retroperitoneal space below , without clear anatomical limitations , representing a potential conduit for the spread of pathological processes between thorax and abdomen [ 8 ]  . 
lymphatics of the posterior mediastinum , the posterior portion of the diaphragm , the spine and the posterior parietal pleura drain into the extrapleural lymph nodes ; those of the anterior parietal pleura drain into the internal mammary chain for the upper and middle part of the thorax and into the cardiophrenic lymph nodes for the lower part [ 7 ]  . 
several neoplastic and nonneoplastic diseases can spread easily from thoracic organs to the abdomen along these lymphatic chains [ 912 ]  . thoracic lymph nodes can be evaluated with various methods , such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) and uorodeoxyglucose - positron emission tomography ( fdg - pet )  . 
lymph node abnormalities are depicted by ct and mri as an increase in nodal size and / or number , and patterns of thoracic lymph node involvement can provide important clues in the diagnosis of many pulmonary and extrapulmonary diseases . 
2 axial computed tomography ( ct ) scan showing the pericardium ( arrow ) as a relatively hyperdense line that separates the epicardial adipose tissue ( ? ) from the cardiophrenic space ( asterisk ) the pericardium posteriorly and the xiphoid process of the sternum and costochondral articulation of the seventh rib anteriorly ; ( 2 ) a middle or lateral group located between the pericardium medially and lung hilum laterally in the region where the phrenic nerves run ; and ( 3 ) a posterior group located near the oesophagus , posteromedial to the inferior vena cava , which goes down to the aortic hiatus [ 5 ]  . 
generally , lymph nodes with a short - axis diameter [ 1 cm are considered pathological [ 13 , 14 ]  . there are little data on the normal size of cardiophrenic and extrapleural lymph nodes , for which no denite cutoff value has yet been established . materials and methods patient population we included in our study 750 consecutive patients ( 430 men , 320 women ; mean age , 59 6 years ) referred to our institution between january and september 2009 for multidetector - row ct ( mdct ) of the chest for different clinical reasons . 
according to their primary disease , these patients were divided into four groups : 340 nonneoplastic patients , 270 patients with extrathoracic neoplasms , 120 patients with intrathoracic neoplasms and 20 patients with pleural metastasis . 
we also included 91 patients ( 61 men , 30 women ; mean age , 67 9 years ) with histologically proven malignant pleural mesothelioma ( mpm ) who had undergone mdct of the chest at our institute between january 2001 and september 2009 . scan protocol and image acquisition ct studies were performed on a four - channel mdct ( somatom volume zoom , siemens medical solutions , forchheim , germany ) using standard parameters mdct of the chest : 120 kv ; effective 400 ma ; gantry rotation time , 500 ms ; table speed , 6 mm / rotation . 
images were reconstructed with a slice width of 1 mm and reconstruction interval of 1 mm . multiplanar reconstructions were obtained in selected cases , especially in mpm patients , for staging purposes . a dose of 90100 ml of nonionic contrast medium ( iomeron 300 mg iodine / ml , bracco , milan , italy ) was injected via an antecubital vein at 23 ml / s . 
a standard scan delay of 25 s was selected in all patients ; in patients with mpm , we performed another acquisition with a 45to 50 - s scan delay to obtain better enhancement of pleural surfaces and disease . imaging evaluation and statistical analysis axial ct images were independently evaluated by two chest radiologists who assessed the presence , number ( single or multiple ) and short - axis diameter ( b5 mm ; 610 mm ; [ 10 mm ) of the extrapleural and cardiophrenic nodes . 
images were analysed using a mediastinal window ( width , 400 hu ; level , 40 hu )  . for statistical purposes , the prevalence of extrapleural and cardiophrenic nodes of each size category ( b5 mm ; 610 mm ; [ 10 mm ) was calculated in patients with mpm and in each patient group ( nonneoplastic , extrathoracic neoplasm , intrathoracic neoplasm , and pleural metastasis )  . comparison of the prevalence between patients with mpm and the remaining four groups was done using the chi square test , with signicance set at p \ 0.05. 
interobserver agreement was analysed using kappa statistics . results the 750 patients in the study comprised 340 nonneoplastic , 270 with extrathoracic neoplasm , 120 with intrathoracic neoplasm and 20 with pleural metastasis . cardiophrenic lymph nodes results regarding cardiophrenic lymph nodes are summarised in table 1 . 
cardiophrenic nodes , independent of their size , were found in 66 ( 8.8 % ) of 750 patients assessed ; in particular , they were b5 mm in 47 patients , 610 mm in 15 and [ 10 mm in the remaining four . considering each category of patients , cardiophrenic nodes were present in 26 of 340 ( 7.6 % ) nonneoplastic patients ( b5 mm in 19 , 610 mm in ve , [ 10 mm in two ) , in 22 of 270 ( 8.1 % ) patients with extrathoracic neoplasm ( b5 mm in 15 , 610 mm in six , [ 10 mm in one ) , in 16 of 120 ( 13.3 % ) patients with intrathoracic neoplasm ( b5 mm in 12 , 610 mm in three , [ 10 mm in one ) and in 13 of 20 ( 65 % ) patients with pleural metastasis ( b5 mm in two , 610 mm in six , [ 10 mm in ve )  . 
extrapleural nodes , independent of their size , were present in only eight ( 1.3 % ) of 750 patients assessed ; in particular , they were b5 mm in four patients , 610 mm in two and [ 10 mm in the remaining two . considering each category of patients , extrapleural lymph nodes were present in three of 340 ( 0.9 % ) nonneoplastic patients ( b5 mm in one , 610 mm in one , [ 10 mm in one ) , in two of 270 ( 0.7 % ) patients with extrathoracic neoplasm ( both b5 mm ) , in two of 120 ( 1.6 % ) patients fig . 
4 axial computed tomography ( ct ) scan showing three lymph nodes \5 mm in the right cardiophrenic angle ( arrows ) in a 52 - yearold woman without known disease fig . 
5 axial computed tomography ( ct ) scans showing the presence of nodes [ 5 mm in the right cardiophrenic space in a patient with right pleural effusion related to malignant pleural mesothelioma ( mpm ) radiol med ( 2014 ) 119 : 2026 table 2 results regarding extrapleural nodes nonneoplastic pts . 
6 axial and coronal computed tomography ( ct ) images show typical extrapleural nodes located in the paraspinal extrapleural fat tissue adjacent to the rib heads in a patient with circumferential pleural involvement due to malignant pleural mesothelioma ( mpm ) with intrathoracic neoplasm ( b5 mm in one , 610 mm in one ) and in one of 20 ( 5 % ) patients with pleural metastasis ( 610 mm )  . 
despite the well - known limits , node size is the main criterion used to evaluate the possible involvement of these nodes [ 13 ] : hilar and mediastinal nodes are considered involved if the short - axis diameter is c10 mm [ 15 , 16 ]  . 
whereas this dimensional criterion is well accepted for hilar and mediastinal nodes , to our knowledge , no cutoff value has been established to date for cardiophrenic and extrapleural nodes . on the basis of the study by dorfman et al . , cardiophrenic nodes with a short - axis diameter [ 8 mm should be considered pathological [ 17 ] , but other studies indicate a different cutoff of 5 mm [ 18 ]  . 
no standard dimensional criteria are available for extrapleural and internal mammary lymph nodes , which are always considered pathological when present , even when the short - axis diameter is \5 mm [ 9 ]  . several papers about nodal involvement in mpm have recently been published . 
they concluded that hilar node involvement , in contrast with the tnm staging system of mpm , is secondary to parenchymal inltration and not due to direct spread from the pleura , whereas extrapleural and cardiophrenic nodes are primarily involved in the presence of mpm . 
 [ 20 ] conducted a retrospective study on 92 patients with a histological diagnosis of mpm and found a prevalence of cardiophrenic radiol med ( 2014 ) 119 : 2026 nodes of 46 % ( 42 / 92 )  . 
this study did not , however , evaluate extrapleural nodes . diagnosis of malignant pleural diseases , whether primary or secondary . our department conducted a study on 91 patients with histologically proven mpm to verify the frequency of early ct signs of this neoplasthe most frequent ct signs in patients with mpm were diffuse or focal thickening of the mediastinal pleura ( 96 % ) , thickening of the costal pleura ( 87 % ) , unilateral pleural effusion ( 85 % ) , volume loss of the pathological hemithorax ( 80 % ) and presence of extrapleural ( 68 % ) and cardiophrenic ( 67 % ) lymphadenopathy . 
we concluded that the presence of extrapleural and cardiophrenic nodes , associated with other signs of mpm and especially involvement of the mediastinal pleura and volume loss of the affected hemithorax , could have an important diagnostic role in the early diagnosis of this neoplasm . the few published reports concerning involvement of cardiophrenic and extrapleural nodes led us to investigate their prevalence in patients with different neoplastic and nonneoplastic diseases and to dene a dimensional cutoff value for these nodes . 
the overall prevalence of these nodes was 1.3 % , with a minimum value of 0.7 % in patients with extrathoracic neoplasm and a maximum value of 5 % in patients with pleural metastasis . by contrast , the prevalence of these nodes was signicantly higher in patients with mpm ; in particular , 62 of 91 patients with mpm ( 68 % ) showed involvement of extrapleural nodes , 18 ( 20 % ) with a diameter b5 mm , 25 ( 27 % ) , with a diameter 610 mm and 19 ( 21 % ) with a diameter [ 10 mthis means that extrapleural nodes should be considered pathological independently of their size , even when \5 mm ; considering that they are extremely rare in all categories of patients except those with mpm , these nodes could have an important diagnostic value in mpm patients when associated with other ndings of this disease , such as unilateral pleural effusion , hemithorax volume loss and mediastinal pleura thickening . regarding the prevalence of cardiophrenic nodes b5 mm , we found no signicant differences between patients with mpm and the other four groups , including patients without neoplaswhen we consider nodes [ 5 mm , the prevalence of these nodes in mpm patients was signicantly higher than in any other group , except for patients with pleural metastasis . 
this means that cardiophrenic nodes , unlike extrapleural nodes , should be considered pathological only when they are [ 5 mm in size . because they are enlarged both in mpm and in pleural metastasis , these nodes could have an important role in the conclusion extrapleural nodes of b5 mm and cardiophrenic nodes of [ 5 mm have signicant diagnostic value in both primary and secondary malignant pleural disease , whereas they are extremely rare in other diseases , whether neoplastic or not . conict of interest b feragalli , c . 
two different techniques were used according to lesion size ( cine mode ; sequential mode )  . after 24 h , each study was repeated to assess repeatability . lesion blood volume ( bv ) , blood ow ( bf ) , mean transit time ( mtt ) and peak enhancement intensity ( pei ) were automatically calculated by two chest radiologists in two different reading sessions . 
inhibition of tumour - related angiogenesis is now an attractive target for anticancer therapy . lung cancer ( nsclc ) , antiangiogenic therapies are yielding promising results in terms of response rate , overall survival ( os ) and progression - free survival ( pfs ) when combined with chemotherapy [ 2 , 3 ]  . 
to evaluate the effects of antiangiogenic drugs , it is advisable to estimate tumour vascularity . in patients with non - small - cell an emerging non - invasive imaging modality that allows in vivo assessment of tumour vascularization is computed tomography perfusion ( ctp ) with a multidetector - row scanner [ 4 , 5 ]  . 
a correlation between ctp parameters and histological markers of tumour neovascularisation , such as microvessel density or vascular endothelial growth factor ( vegf ) , has been demonstrated in lung cancer [ 68 ]  . 
ctp allows the processing of dynamic image data and generates radiol med ( 2014 ) 119 : 412 functional perfusion parameters based on changes in tissue attenuation over time during the injection of a contrast medium bolus . 
during the rst - pass phase ( within the rst 4050 s from contrast medium injection ) , contrast material is predominantly intravascular , and tumour contrast enhancement essentially reects blood ow ( bf ) and blood volume ( bv ) , without interference of blood recirculation on perfusion quantication . 
delayed enhancement ( after 60 s from the start of contrast medium injection ) is determined by the passage of contrast material into and out of the extravascular space and is used to calculate tumour vascular permeability [ 5 ]  . evidence exists that ctp allows monitoring the therapeutic effect of antiangiogenic treatment in lung cancer [ 4 , 9 , 10 ]  . 
 [ 9 ] demonstrated that perfusion parameters calculated with 64 - detector - row ct were higher in patients with lung adenocarcinoma that responded to chemotherapy associated with antiangiogenic drugs than in non - responding patients . good reproducibility and repeatability of any quantitative measurement repeated on the same patient is an essential prerequisite in clinical practise , as in estimating tumour treatment response . 
in the last few years , there has been considerable improvement in the ctp technique , moving from single - tumour - level studies to whole - tumour perfusion studies , providing more reliable results in terms of reproducibility [ 1113 ]  . 
in particular , to the best of our knowledge , no previous studies have been published on the repeatability of wholetumour rst - pass perfusion with 64 - detector - row ct in lung cancer . 
therefore , the purpose of our study was to assess repeatability and intraand interobserver variability of whole - tumour rst - pass perfusion technique in nsclc carried out with a 64 - detector - row ct scanner and commercial software for image postprocessing . materials and methods patient population this study received the approval of the local medical ethics committee and was performed in accordance with the ethical standards laid down in the 1964 declaration of helsinki . 
the cine - mode technique consists of 80 acquisitions encompassing the lesion site and was carried out with the following parameters : detector conguration 64 9 0.625 mm ( total coverage , 40 mm ) ; reconstruction slice thickness , 5 mm ( eight images per rotation ) ; tube voltage , 80 kvp ; xed tube current , 120 ma ; tube rotation time , 0.5 s ; total scan duration , 40 s . the total number of ct images was 640 ( eight images per rotation 9 80 acquisitions )  . 
after 24 h , each patient underwent a second ctp acquisition using the same technical and contrast material injection parameters to assess repeatability of both perfusion techniques . technical adequacy of dynamic ct fullled the following criteria : ( a ) absence of contrast medium extravasation at the site of injection , ( b ) appropriate enhancement of vascular structures ( enhancement c150 hu ) , ( c ) no marked reaction to contrast medium that interfered with image acquisition , ( d ) adequate z - axis coverage of the whole lesion and ( e ) absence of signicant patient respiratory misregistration that hampered the automatic calculation of perfusion parameters . image postprocessing and analysis all 24 ctp scans , 12 of which were obtained at time 0 ( rst scan , t0 ) and 12 at time 1 ( second scan , t1 ) were transferred to a commercial workstation ( aw4.4 , ge medical systems ) for quantitative assessment of perfusion parameters using a commercial ctp software ( ct - perfusion 4 , ge medical systems )  . 
firstly , a circular region of interest ( roi ) was manually placed at the centre of the thoracic aorta included in the tumour scan volume with the aim of obtaining a timeattenuation curve ( arterial input ) expressed in hounseld units per second . 
the reading session was repeated by the same two radiologists with the same modality 1 month following ( second reading session ) the rst evaluation ( rst reading session ) to assess intraobserver variability . statistical analysis mean and standard deviation ( sd ) were used for descriptive statistics . 
differences between measurements yielded at the rst ( t0 ) and at the second ( t1 ) scans were plotted against the average of the differences using data collected from the rst reading session . 
computed tomography ( ct ) native images at mediastinal window and colourimetric images of blood volume ( bv ) , blood ow ( bf ) and mean transit time ( mtt ) are shown at a similar position along the patient z - axis on rst ( t0 ) and second ( t1 ) scans . 
computed tomography ( ct ) native images at mediastinal window and colourimetric images of blood volume ( bv ) , blood ow ( bf ) and mean transit time ( mtt ) are shown at a similar position along the patient z - axis on t0 and t1 scans . 
for this purpose , cronbachs a coefcient was calculated [ 17 ]  . interobserver variability was assessed by evaluating intraclass correlation coefcient ( icc ) with 95 % condence intervals ( 95 % ci ) by comparing measurements obtained by the two observers at each ctp scan ( t0 ; t1 )  . 
ten of 12 tumours were located in the upper lobes and two in the lower lobes ; nine tumours were peripheral and three were centrally located . all dynamic ct scans were considered technically adequate , without signicant patient respiratory misregistration , and included the entire tumour . 
all ctp scans were successfully analysed by the software . mean and sd of the four ctp measurements obtained by the two observers at t0 and t1 on both reading sessions are shown in table 1 . 
2 and 3 , showing two lesions located at the left lung base , a site that could potentially be affected by respiratory and cardiac motion artefacts . radiol med ( 2014 ) 119 : 412 analysis of intraobserver variability showed a high repeatability of measurements for each of the four parameters , as demonstrated by cronbachs a coefcient reported in table 2 . 
tumour vasculature shows temporal heterogeneity [ 19 ] , which cannot be exceeded in practise ; and spatial heterogeneous distribution , which seems to be compensated by increasing the tumour volume coverage assessed with the ctp technique [ 12 , 13 , 20 ]  . 
technique repeatability and intraand interobserver variability assessment of perfusion measurements is clearly relevant for accurate quantitative estimation of lung cancer perfusion , especially when considering treatment effect . until now , published studies on ctp technique repeatability have been performed using a 16 - detector - row ct scanner and different techniques [ 12 , 13 , 21 ]  . 
 [ 12 , 13 ] , a non - commercial software was used to assess whole - tumour perfusion parameters , and only bv and permeability were evaluated due to the low temporal resolution of the scanner , which did not allow whole - tumour bf measurement . 
 [ 21 ] , a rst - phase cine - mode scan for assessing rst - pass perfusion parameters , which covered only 20 mm of volume , was followed by a delayed phase , with a total duration scan time of 125 s . 
in that study , the absolute values and reproducibility of perfusion parameters were markedly inuenced by motion artefacts and long acquisition time , for permeability [ 21 ]  . indeed , the main advantage of rst - pass perfusion over permeability assessment in the delayed phase is the short scan time , which limits motion artefacts [ 22 ]  . in particular the use of 64 - detector - row ct evaluating lung cancer to improve misregistration perfusion has the potential fig . 
6 blandaltman agreement plot of mean transit time ( mtt )  . the plot shows the difference in mtt between the rst ( t0 ) and second ( t1 ) scans against the mean of mtt values . 
 [ 23 ] assessed the feasibility of rst - pass whole - tumour perfusion with 64 - detector - row ct but only tested intraobserver variability , not technique repeatability . 
the technique used in that study consisted of 12 repeated helical ct scans with a total acquisition time of * 55 s , a temporal resolution of 4.6 s and a maximum covered volume of up to 5 cm . in our study , we tested the repeatability and reproducthe rst - pass perfusion performed with a ibility of 64 - detector - row ct scanner that enabled coverage of tumours with a diameter of up to 8 cm with higher temporal resolution ( 0.5 s for cine mode ; 2.7 s for shuttle ) and shorter scan duration time ( \50 s ) than did the abovementioned study . 
we observed good overall repeatability of the whole lung tumour rst - pass perfusion technique with low coefcients of variation and narrow limits of agreement for all parameters , in particular for bv and mtt . 
moreover , we noted better results in comparison with those reported in the three previous studies performed using a 16 - row ct scanner [ 12 , 13 , 21 ] , which enrolled a similar overall number of patients ( respectively 10 , 10 and 11 patients ) to our study ( 12 patients )  . 
improved perfusion parameter repeatability measured using 64 - detector - row ct , in our experience , is mainly due to the higher temporal resolution of the scanner and perfusion protocols used , which allowed technically adequate ct scans without relevant patient respiratory misregistration . 
in addition , limits of agreement for the cine - mode technique measurements in our study were narrower than those for the sequential - mode technique , which may be explained by the better performance in terms of temporal resolution of the cine - mode technique . 
our results in terms of good repeatability could be also due to the patient respiratory training performed before starting the examination and to the prevalent location of tumours in the upper lobes ( 10 / 12 , 83 % ) , which are less affected by respiratory motion artefacts . in the clinical context of assessing lung cancer response to treatment , the intrinsic variability of perfusion measurements should be small enough to allow the identication of changes in tumour vascularization induced by the treatment . 
in a study that used the ctp technique to determine the effects of an antiangiogenic drug ( combretastatin a4 phosphate ; ca4p ) on tumour vascularisation in patients with advanced nsclc , a reduction in bv of 29.4 % was demonstrated after 72 h from ca4p administration [ 10 ]  . 
the intrinsic variability we observed for bv in the ctp technique was 26 % , a value small enough to assess bv changes induced by the therapeutic agent , according to data mentioned above . 
this result suggests that the ctp technique may be considered quite repeatable for detecting perfusion parameter changes and that it could have a clinical application in assessing therapy response . as regards intraobserver agreement , the high consisresults demonstrated in our study for both tency of observers and all parameters may be explained by the adequate period of training in the ctp technique received by the two radiologists . 
this result was expected , considering the variability due to manual drawing of rois along the tumour margins , which is closely operator dependent , but did not affect the interobserver reliability . 
similar results were reported for colorectal cancer perfusion technique [ 24 ]  . in summary , all our results , in terms of technique repeatability and agreement among observers , are indicative of the possible clinical use of the ctp techniques tested , with the advantage of employing commercial software for postprocessing . 
first is the small number of patients enrolled , even though other published studies [ 12 , 13 , 21 ] on the same topic also included few patients ( 10 , 10 and 11 , respectively )  . 
to assess repeatability of the ctp technique , two examinations were performed at t0 and t1 after 24 h , with a considerable overall effective radiation dose to each patient , in particular for the cine - mode technique ( 25 msv )  . 
secondly , patient clinical outcome on the basis of perfusion parameters was not analysed , as this was beyond our aiin fact , this study represented only a laboratory test of technique repeatability . 
largescale trials are required to investigate the usefulness of the rst - pass perfusion ct technique in assessing prognosis and survival of lung cancer patients . in conclusion , rst - pass perfusion with 64 - detector - row ct proved to be feasible to quantitatively assess wholetumour perfusion in lung lesions measuring up to 8 cm , with good technique repeatability and high intraand interobserver agreement . 
pneumologia , ospedale morgagni - pierantoni , via c.forlanini 34 , forl` , italy their diagnosis is a challenge for clinicians , pathologists , and radiologists , and any additional knowledge about the ct ndings may help the diagnosis in the case of patients affected by ph of unknown origin . keywords pulmonary hypertension ( cid : 2 ) tumour embolism ( cid : 2 ) pulmonary artery sarcomas introduction pulmonary hypertension ( ph ) is dened as an increase in mean pulmonary arterial pressure ( pap ) c25 mmhg at rest as assessed by right heart catheterisation , in the presence of normal left atrial pressure . 
chest radiography , echocardiography , and electrocardiography are run as rst level investigations but in many cases the diagnostic process requires further investigations , including a computed tomography ( ct ) study . 
ph can be associated with several clinical conditions , which have been classied into six groups according to specic characteristics ( dana point 2008 ) [ 1 ] : 1 . 
pulmonary hypertension with multifactorial mechanisms . the relevant literature and presenting our personal series of 26 cases . in order to adopt recently published guidelines by the european society of cardiology and the european respiratory society emphasise the importance of a correct diagnosis in patients the appropriate affected by ph [ 1 ] , therapeutic approach . 
whereas thromboendarterectomy is a potentially curative option for cteph , non - embolic ph can be treated by specic drugs and supportive therapy or , in the case of inadequate clinical response , by balloon atrial septostomy and / or heartlung transplantation . 
it is also important to recognise patients affected by pvod or pch , because the administration of vasodilators in such patients can lead to a fatal pulmonary oedema [ 1 , 2 ]  . histology may be required to conrm the diagnosis , but lung biopsies are high - risk procedures and , therefore , not recommended [ 2 , 3 ] ; hence , the need to nd a less invasive approach for a correct aetiopathogenetic diagnosis of patients . under these circumstances , high - resolution computed tomography ( hrct ) of the chest , especially in the angiographic phase after injection of contrast material ( ct pulmonary angiography , ctpa ) , plays a central role because it allows both evaluation of indirect signs of ph and identication of any underlying disease that might lead to secondary ph . ct features common to all forms of ph [ 4 , 5 ] are : dilatation of the pulmonary artery trunk , which may exceed that of the ascending aorta ( ratio greater than 1 : 1 )  . 
the presence of a diameter greater than or equal to 29 mm has a positive predictive value ( ppv ) [ 95 % and a specicity [ 90 % in the diagnosis of ph in the absence of diffuse pulmonary brosis . 
its aetiology is not wellknown , and among the suggested hypotheses are immunemediated causes ; viral aetiology ; an excessive immune response to chemotherapy or radiation or bone marrow transplants in cancer patients [ 6 ] ; smoke and exposure to anorectic agents derived from fenuramine [ 2 ]  . 
both the clinical and haemodynamic features of pvod are non - specic but radiology is of great help because the signs of pulmonary hypertension and of interstitial oedema are evident , even when the anatomical obstruction is post - capillary ( pap is high and pulmonary wedge pressure is normal or low )  . pvod is histologically characterised by intimal brosis , which causes narrowing and occlusion of the pulmonary veins of any size , with a preference for venules with a diffuse or patchy distribution [ 7 ]  . 
however , the absence of the typical radiological ndings does not exclude a diagnosis of pvod and cardiac catheterisation remains necessary , with precise documentation of the transcapillary wedge pressure [ 9 ]  . recent reports have highlighted the usefulness of pulmonary function tests in the diagnostic workup of pvod , as they typically show a decrease in diffusing capacity of the lung for carbon monoxide ( dlco ) , hypoxaemia at rest in arterial blood gases analysis and signicant desaturation at the 6 - minute walk test ( 6mwt )  . bronchoalveolar lavage ( bal ) might show macrophages containing haemosiderin , which is a manifestation of occult intra - alveolar haemorrhage [ 2 , 3 ]  . ct and clinical - laboratory ndings allow for a sufciently reliable diagnosis of pvod , thus averting the need radiol med ( 2014 ) 119 : 4153 fig . 
1 our ct ndings are in agreement with literature ; indeed all 6 patients had smooth septal thickening ( a , b ) , groundglass opacities with preferential centrilobular distribution ( a , b ) and mediastinal adenopathy ( c ) ; 3 patients had also pericardial and pleural effusion for lung biopsy and consenting the planning of a treatment schedule and the addition of patients to transplant waiting lists [ 2 , 9 ]  . capillary haemangiomatosis pulmonary capillary haemangiomatosis ( pch ) , just one personal case , is an extremely rare form of post - capillary ph , identied for the rst time in 1978 by wagenvoort . pch affects mainly young adults ( 2040 years ) and it shows a median survival of 3 years [ 6 , 9 ]  . 
a high frequency of haemoptysis and pleural effusion ( haemorrhagic in many cases ) are clinically reported ; pulmonary function tests show the reduction of dlco and hypoxaemia [ 2 ]  . 
nodular opacities probably reect focal angiomatous proliferation within bronchovascular structures along the alveolar septa and within the vessel walls , while the ground - glass background can be ascribed to the small vessel growth [ 10 ]  . septal thickening , pleural effusion ( clinically in 50 % of cases ) , and mediastinal node enlargement are rarely present , as in pvod . 
with disease progression , common signs of pulmonary arterial hypertension , such as dilation of the main pulmonary artery and right heart chambers , start to arise [ 11 ]  . pulmonary hypertension due to non - thrombotic pulmonary embolism non - thromboembolic pulmonary embolism is a rare cause of precapillary ph . 
it is dened as the embolisation of the pulmonary circulation by different cell types ( adipocytes , amniotic , cancer , etc . ) , bacteria , fungi , foreign material or gas [ 1 ]  . 
in contrast embolism , the effects of non - thrombotic emboli are not only purely mechanical but also related to the nature of the embolic agent . chest x - ray may be in the norm or shows signs of ph such as enlargement of central pulmonary arteries and cardiomegaly . 
2 hrct : diffuse centrilobular ground glass opacities with some nodules superimposable ( a c ) emphasized by min - ip reconstruction ( d ) ; no mediastinal adenopathies or pleural effusion ( d ) radiol med ( 2014 ) 119 : 4153 artery ( fleischner sign ) ; peripheral area of oligaemia with minimal change in lung volume ( westermark sign ) or diaphragm elevation . 
the presence of single or multiple pulmonary infarcts , most frequent in the basal regions , may be noticed as well : it is classically described as hamptons hump and consists of a homogeneous wedge - shaped consolidation in the lung periphery with a base contiguous to a visceral pleural surface and a rounded convex apex directed towards the hilum [ 12 , 14 ]  . frequent ct features common to cteph [ 4 , 6 , 15 ] include : complete or partial obstruction of the vessel lumen . characteristic mosaic pattern of perfusion in the pulmonary parenchyma , due to the blood ow redistribution and the presence of hypoperfused areas with low attenuation high hyperperfused attenuation . areas enlargement of both bronchial and non - bronchial systemic arteries ( phrenic , mammary , intercostal ) with a diameter [ 2 mm , which helps to keep the blood ow in the presence of pulmonary arterial vascular obstruction by participating in gas exchange . 
blood ow in these arteries , which in normal conditions represents 1 % of the cardiac output , may reach almost 30 % of the systemic blood ow [ 16 ]  . lymphadenopathy , pleural effusion and pleura - based triangle opacities with thickening of parenchymal adjoining visceral pleura or parenchymal bands , representing scars of pulmonary infarcts . it is important to emphasise that chronic thrombi , after the injection of the contrast agent , often show signicant enhancement , depending on the thrombus organisation [ 17 ]  . tumour embolism a case of ph caused by tumour emboli in the pulmonary circulation was rst reported in 1937 . 
many types of malignant tumour can give rise to this picture , the most frequent of which is gastric cancer , followed by renal cell carcinoma , breast , prostate , hepatocellular carcinoma , and choriocarcinoma [ 12 , 18 , 19 ]  . tumour thrombi are frequently formed by malignant cells , platelets , and brin , and are highly resistant to recanalisation and lead to a progressive and irreversible obstruction ; in many cases , they are associated with vascular tissue reaction with intimal proliferation and brosis ( thrombotic microangiopathy )  . 
when 6080 % of pulmonary arterial bed is involved , cor pulmonale occurs which leads the patient to death [ 18 , 20 ]  . ct in the angiographic phase , as in the single case we observed , shows the presence of intraluminal lling defects or multifocal dilatations and strictures in affected segmental and subsegmental arteries associated with hypopshow carcinomatous erfused areas ; ct can also radiol med ( 2014 ) 119 : 4153 fig . 
common ndings in these cases consist of : a or b kerley lines ( expression of thickening septa ) ; thickening with unior bilateral reticular pattern with or without adenopathy and , in some cases , thickening and / or pleural or pericardial effusion . 
hrct enables the detection of the disease in more than 50 % of patients with compatible symptoms and negative x - ray : it shows nodular thickening of the septa , subpleural and peribronchovascular interstitium , in the absence of distortion of the brotic lung parenchyma . 
this nding may be focal or bilateral and diffuse [ 22 ]  . a tree - in - bud - like pattern has recently been described as an expression of tumour intravascular pulmonary embolisin these cases , two different pathogenetic mechanisms are involved : the lling of centrilobular arterioles by tumour cells and the so - called carcinomatous endarteritis , which is a rare form pathologically characterised by marked intimal hyperplasia brocells initiated by the presence of microemboli tumour [ 19 , 23 ]  . hydatid disease hydatid disease is a parasitic disease , particularly widespread in the mediterranean , most frequently caused by larvae or cysts of echinococcus granulosus . 
the parasite can reach any part of the body , but the liver ( 75 % ) and lung ( 15 % ) are the most frequent sites of infection [ 24 , 25 ]  . pulmonary embolism is a rare complication of heart or liver echinococcosis resulting from the rupture of a hydatid cyst in the right heart or , more rarely , because of haematogenous dissemination after the rupture of a cyst in the hepatic veins and inferior vena cava . 
in many cases , a chronic course with acute recurrences can be observed [ 19 ]  . ct in the angiographic phase , as in the single case we observed , shows occlusion of the pulmonary arterial branches caused by cystic lesions that appear as multiple bilateral nodules of variable diameter and well - dened margins with characteristic hypodense homogeneous postcontrast enhancement . 
embolism of numerous segmental and subsegmental arteries ending in hydatid cysts , some of which partially calcied ( b , c ) ; two partially calcied hydatid cysts are present in the mediastinum : one between aortic root and right atrium , the other prior to right atrium ( d ) radiol med ( 2014 ) 119 : 4153 magnetic resonance ( mr ) imaging can be useful in the diagnostic workup of these patients both for the characterisation of cardiac hydatid cysts and for the evaluation of lung nodules : homogeneous hyperintense signal with hypointense peripheral rim , which represents the pericystic capsule , on t2 weighted images and hypointense on t1 weighted images [ 26 ]  . 
knowledge of the radiological characteristics is important because urgent surgical treatment ( endoarterectomy or lung transplantation ) is required , where possible , to avoid the occurrence of complications or death . talcosis there are several forms of lung talcosis ( talcosilicosis , talcoasbestosis and talcosis alone ) caused by inhalation of talc , a mineral widely used in factories ( ceramic , cosmetic , paper , plastic and paint ) [ 27 ]  . 
pulmonary talcosis affects drug abusers who inject drugs made out of crushed tablets containing talc as a binding agent , and the disease progresses with the chronic intravenous injection of such substances , as in the single case we observed . 
clinically , most patients are asymptomatic or show non - specic symptoms such as worsening dyspnoea , cough , and chest pain , but there are also fulminant forms ; the clinical ndings are dose - related but may progress even after cessation of drug abuse . 
when injected intravenously , talc is trapped in the pulmonary arterioles because of its insolubility , resulting in thrombosis and inammation ; as a consequence , brosis and architectural distortion of the lung may arise , especially in the upper lobes [ 12 , 20 ]  . chest x - ray may show varying ndings , from small nodules 13 mm in diameter in the early stages to extensive areas of increased opacity , predominantly located in the perihilar region with sparing of the apical regions and costophrenic sinuses which may enter the differential diagnosis with the progressive massive brosis affecting patients with silicosis , coal workers pneumoconiosis and stage iv sarcoidosis . 
elevation of the hila , hyperlucency of the lung bases and signs of ph are also reported [ 27 ]  . in the early stages , ct also dedepicts perilymphatic micronodules with both centrilobular and lymphatic distribution and ground - glass areas that can evolve into areas radiol med ( 2014 ) 119 : 4153 fig . 
5 ( a , b , c , d ) : widespread and severe interstitial lung disease ( with involvement of approximately 75 % of lung parenchyma ) characterized by ground - glass opacities and thickening of interlobular septa with sparing of some secondary lobules . 
hilar or mediastinal nodal enlargements are rare [ 19 , 27 , 28 ]  . bronchoalveolar typically shows the lavage ( bal ) presence of lymphocytosis with a prevalence of cd8 lymphocytes and macrophages with intracellular microcrystals of talc which have a typical birefringent appearance under polarisation microscopy [ 20 , 27 ]  . pulmonary artery sarcomas pulmonary artery sarcoma ( pas ) is a rare malignant intraluminal mesenchymal tumour rst described during autopsy by mandelstamm in 1923 . 
pas tends to grow quickly and has an unfavourable prognosis , with an average survival of 12 months in surgical patients ; death is usually due to heart failure caused by obstruction of the pulmonary arteries [ 29 , 30 ]  . clinical presentation is not specic and the most common symptoms are : progressive dyspnoea ( 67 % ) , chest pain ( 54 % ) , cough ( 42 % ) , and haemoptysis ( 22 % ) ; weight loss , anaemia , and fever are not common symptoms and tend to suggest malignant disease rather than pulmonary embolism [ 3032 ]  . 
the correct diagnosis is often delayed because pas generally mimics acute or chronic pulmonary embolism , lung cancer or mediastinal masses , with a consequent delay in surgical treatment and worse prognosis [ 30 , 31 ]  . many pas involve , and probably arise from , the pulmonary artery trunk near the pulmonary valve and often involve the main pulmonary artery [ 29 , 31 ]  . the chest x - ray may be normal or , more frequently , show hilar masses , lung consolidation or oligaemia , heart and pulmonary artery enlargement or evidence of metastasic disease , but such ndings are generally considered non - specic [ 31 ]  . ct can help to differentiate pas from pulmonary embolism by showing a low - attenuation lling defect which occupies the entire luminal diameter of the main pulmonary trunk and / or main branches of the pulmonary artery with extraluminal tumour extension in the mediastinugenerally , this defect shows inhomogeneous contrast enhancement because of the presence of internal areas of necrosis or thrombi covering the tumour ; this heterogeneous appearance can be due to the presence of haemorrhagic foci , cysts or intralesional calcic spots [ 29 , 30 , 33 ]  . 
cases without any signicant contrast enhancement have also been observed . the presence of extraluminal tumour extension or mediastinal , pulmonary or distant metastases allows the late denitive differential diagnosis , but these fig . 
6 ctpa : large lling defect in the pulmonary artery trunk and its branches ( main , lobular and segmental ) ( a , b , c )  . the tissue has contrast enhancement and there is fdg uptake in the pet - ct study ( d ) radiol med ( 2014 ) 119 : 4153 manifestations [ 33 ]  . 
besides , pet plays a central role in the diagnostic process of pas associated with thrombosis as it may be used to isolate pas from thrombosis by showing site , size , and the extension of the tumour , which presents intense contrast enhancement as opposed to the thrombotic area , which is not fdg - avid because thrombi contain few macrophages and inammatory cells [ 30 , 34 ]  . neurobromatosis neurobromatosis type 1 ( nf1 ) , known also as von recklinghausens disease , is a genetic autosomal dominant disorder characterised by nf1 tumour suppressor gene mutation on chromosome 17 . 
7 widespread alteration of lung parenchyma , which has cystic appearance in the upper lobes ( b ) and reticular appearance , with areas of ground - glass , in the lower lobes ( c , d ) ; extension bigger than 50% of the lung parenchyma ; no ndings typical ct of ph . diagnosis of ph at heart catheterization ( papm 35 mmhg , pwp 10 mmhg ) pulmonary brosis has also been reported [ 38 ]  . 
the disease has an estimated incidence of 1035 cases / 100 , 000 people in the usa , with a mortality of 15 % and an average age at diagnosis of 40 years [ 39 ]  . the typical lesion is a non - caseating sarcoidosis granuloma consisting of a central core of t lymphocytes surrounded by epithelioid and giant multinucleated cells ; broblasts and brosis that evolve along a centripetal direction to ll the granuloma during the course of the disease are situated in the external area . frequently , the diagnosis is made with chest x - ray , because of the presence of hilar and mediastinal lymph node enlargement , with or without lung parenchymal involvement . 
the affected lung has a typical nodular interstitial pattern characterised by several solid nodules varying from 1 to 5 mm , associated with linear and irregular opacities [ 22 ]  . subpleural distribution , the hrct features can vary and mimic other diffuse inltrative diseases ; characteristic ndings of active sarcoidosis include several small well - dened nodules showing perilymphatic along the interlobular septa and bronchovascular bundles , often predominant in the upper lobes . 
the earliest nding of brosis is the posterior displacement of the upper lobar bronchi associated with reticular septal thickening due to the evolution of the brotic lesions which can develop from peribronchial brosis into perihilar masses , which distort the bronchi and vessels and cause traction bronchiectasis [ 22 ]  . 
the nding of areas of honeycombing is rare [ 14 , 40 ]  . once considered a rare manifestation of sarcoidosis , ph associated with sarcoidosis ( saph ) , of which we have observed six cases , is now acknowledged as an important complication that signicantly worsens morbidity and mortality . in the recently published guidelines by the european society of cardiology and the european respiratory society , ph associated with lung diseases or hypoxaemia is classied in group iii , while saph is included in group v ( miscellaneous ) because its pathogenesis is complex and multifactorial [ 1 ]  . 
the presence of ph despite the absence of hypoxaemia or a diffuse parenchymal damage can be caused by : pvod , a recognised complication of sarcoidosis characterised by an occlusive venopathy with intimal brosis and haemosiderosis [ 39 ]  . intrinsic sarcoid vasculopathy , granulomatous involvement of the pulmonary vessel wall occurring in 70100 % of patients with saph ; in fact , because of the perilymphatic distribution of sarcoidosis , granulomas are located close to arterial or venous pulmonary septa vessels , and they may penetrate the intima , media or adventitia of the arteries causing occlusion , or they may affect the veins , haemodynamically mimicking pvod [ 45 , 46 ]  . other causes include : extrinsic compression of pulmonary vessels by mediastinal or hilar lymphadenopathy or mediastinal brosis [ 40 ] ; myocardial dysfunction for direct myocardial involvement by sarcoidosis [ 42 ] ; portopulmonary hypertension resulting from hepatic sarcoid inltration with consequent cirrhosis and portopulmonary hypertension [ 39 , 40 ] ; obstructive sleep apnea syndrome ( osas ) , which is common in patients with sarcoidosis and can contribute to a high pulmonary pressure [ 39 ]  . is important to identify the occurrence of ph in patients with sarcoidosis as early as possible because ph signicantly worsens the prognosis , with a median 5 - year survival rate of less than 60 % [ 46 ]  . ph should be suspected in all patients with sarcoidosis with dyspnoea , hypoxaemia or clinical ndings compatible with right heart failure ( such as peripheral oedema or syncope ) , especially if these symptoms are out of proportion to the extent of pulmonary parenchymal damage . some parameters and clinical laboratory parameters predictive of ph have been studied including : increased need for supplemental oxygen , dlco \30 % in patients with stage iv sarcoidosis on chest x - ray or dlco \50 % in radiographic evidence of pulmonary patients without radiol med ( 2014 ) 119 : 4153 fig . 
 ( b , c , d ) : hrct permits clearer imaging of diffuse and irregular cystic pattern ( involving more than 50% of lung parenchyma ) that simmetrically involves the middle and upper lung zones and sparing the costophrenic sulci brosis [ 47 ] , or oxygen saturation at the 6mwt \90 % and dlco \60 % [ 48 ]  . debate about the usefulness of a specic therapy for ph is still open , but it has been shown that vasodilators should be used with caution in patients with a pvod - like pattern because they may precipitate pulmonary oedema [ 42 , 46 ]  . hrct is therefore fundamental as it can raise a suspicion of pvod in the presence of its typical features ( smooth septal thickening , ground - glass opacities and mediastinal nodal enlargement ) , which are frequently present in patients with non - brotic sarcoidosis and ph [ 45 ]  . pulmonary langerhans cell histiocytosis pulmonary langerhans cell histiocytosis ( plch ) or histiocystosis x or eosinophilic granuloma is a rare smokerelated disease predominantly affecting young people ( 2040 years ) [ 49 ]  . plch belongs to the group of langerhans cell histiocytosis ( lch ) , an idiopathic disorder that affects the specialised immune langerhans cells , which can accumulate in tissues as a result of local reaction to inammatory or neoplastic stimuli [ 50 ]  . 
its course is unpredictable because it can improve or even reverse with smoking cessation or corticosteroid therapy , but in a minority of cases it may progress to pulmonary brosis that can lead to death or lung transplantation [ 51 , 52 ]  . 
the cessation of smoking does not always lead to the resolution of the pathology [ 49 , 50 ]  . from a histological point of view , the characteristic lesion of plch is the bronchiole - centric inammation supported by aggregates of langerhans cells , inammatory cells and brosis [ 52 ] , similar to a sheath extending proximally and distally along the damaged bronchioles . chest radiography shows nodules with irregular margins of variable size ( 110 mm ) , usually with bilateral and symmetrical distribution predominantly in the upper and middle lobe , with sparing of the costophrenic sinuses [ 50 , 51 ]  . hrct , as we observed in our ve cases , is much more sensitive and specic than chest x - ray in the assessment of the extent and activity of the disease , and it leads to a correct diagnosis in 90 % of patients . 
in particular , the initial stages of the disease are characterised by a nodular pattern that reects the presence of bronchiolocentric granuloma : nodules usually sized less than 5 mm with typical peribronchiolar and centrilobular distribution , in variable number depending on the degree of disease activity . 
during disease progression , the nodules become cavitated and the thickening of bronchiolar walls and the formation of cystic spaces with walls of variable thickness from perceptibility to some millimetres become clear . 
cysts are the most typical features of this disease ; they may be of variable shapes ( round , lobular or bizarre ) , usually smaller than 10 mm , but they may coalesce or break into the pleural space causing pneumothorax [ 22 ]  . 
numerous studies have shown that , in the advanced stages of plch , the decrease in exercise capacity does not appear to be related to ventilatory limitation , but rather to a severe and widespread vascular pulmonary disease . 
in fact , as opposed to patients with chronic obstructive pulmonary disease ( copd ) or other interstitial lung disease ( ild ) , patients with plch have ph out of proportion to their indices of ventilator or gas - exchange limitation . 
this theory is supported by the fact that , while the ph secondary to chronic obstructive or other interstitial brotic diseases rarely exceeds 35 mmhg , in plch the pulmonary artery pressure is 60 mmhg on average , that is , similar to that observed in idiopathic ph [ 50 ]  . histopathological observations conrm that pulmonary vascular involvement may be a central process in advanced plch . 
the causes of such vascular remodelling is still unknown [ 50 , 52 ]  . conclusion ph is a frequent clinical diagnosis often associated with high patient morbidity and mortality . 
diseases leading to ph cause a wide spectrum of ct ndings , and the recognition and further knowledge of the ct features of rare forms of ph are important because , when combined with the clinical and laboratory data , they can help radiologists to provide a sufciently reliable diagnosis without lung an appropriate biopsy . 
mcloud received : 27 october 2013 / accepted : 4 november 2013 / published online : 22 november 2013 ( cid : 2 ) italian society of medical radiology 2013 lung cancer remains the leading cause of death from malignancy with approximately 1.3 million deaths occurring world wide per year [ 1 ]  . 
the overall 5 - year survival still remains very low at only 14 % [ 1 ]  . lung cancer , however , which is detected early in its course , demonstrates much better survival data . 
survival in non - small - cell lung cancer stage i is greater than 70 % and small peripheral less than 1 cm lung cancers have survival rates of greater than 80 % [ 2 ]  . 
diagnosis of lung cancer early in preclinical stages has a higher cure rate and , therefore , high - risk asymptomatic individuals are likely to benet from screening . the introduction of helical and subsequently multidetector ct in the 1990s led to a number of feasibility studies in which ct was used as a screening tool for the detection of early asymptomatic lung cancer . 
mcloud ( & ) thoracic radiology , massachusetts general hospital , harvard medical school , 55 fruit street , boston , ma 02114 , usa e - mail : tmcloud@partners.org least in regard to diagnostic algorithms , three times that of standard positive rate was at radiographs . these studies provided evidence that peripheral nodules greater investigation than 810 mm in size required further because of the high likelihood of lung cancer . 
smaller nodules ( \8 mm diameter ) could be managed with ct follow - up to determine interval growth indicating the likelihood of malignancy . these single arm feasibility and observational studies the effectiveness of provided compelling evidence of helical and mdct as a screening tool for early detection of lung cancer . 
only randomized controlled trials can determine effectiveness of screening where the end point must be a decrease in mortality in the screened group as compared to a non - screened control . subsequently , several prospective randomized controlled trials were undertaken both in the united states and europe . 
these included the national lung cancer screening trial ( nlst ) in the united states [ 10 ] and the nelson trial and others in europe [ 1115 ]  . 
it was a randomized national study and the population group included individuals between the ages of 55 and 74 with history of c30 - pack years of current or prior smoking . the enrollees underwent three annual screens . 
the study was designed to determine lung cancer - specic mortality and had a 90 % power to detect a 20 % reduction in lung cancer in the screened group . 
a positive screen consisted of the detection of a nodule or nodules greater than 4 mm in diameter or other abnormalities suspicious of lung cancer . follow - up was recommended based on nodule size and larger nodules required diagnostic workup . 
there were few major complications from diagnostic workups conducted on cases suspicious for lung cancer . however , there were a number of important disadvantages of screening reported by this study . 
39 % of subjects in the ct arm had a positive scan over the course of the 3 - year screening period and 95 % of the positive screens were false positives with no evidence of conrmed lung cancer . 
however , the technique delivered a mean whole body effective dose of 1.4 msv in the nlst trial which represents about one - fth of the dose of a diagnostic chest ct scan [ 16 ]  . the potential benets of ct screening for high - risk individuals outweigh the small risk of cancer deaths related to cumulative radiation exposure [ 17 ]  . there are methods to improve the positive predictive value and decrease the large number of false positives encountered with ct screening for lung cancer . 
the nelson trial in europe is a two - step process which has been able to decrease the number of false positive ndings based on nodule size [ 11 ]  . 
another method of improving the positive predictive value is to better dene risk proling . although the greatest risk for lung cancer is smoking , the risk is less than 20 % for the development of lung cancer . however , patients with copd may have up to a sixfold increased risk for malignancy . 
it is also possible that medical biomarkers may be used to further identify highrisk populations . many american professional societies have recommended lung cancer screening for individuals meeting the criteria of the nlst trial with some slight modications . these include the american college of chest physicians , the american cancer society , the american association of thoracic surgery , and the national comprehensive cancer network [ 17 , 18 ]  . 
this will ultimately mean that in the us , there will be insurance coverage for lung cancer screening probably within the course of a year . the cost - effectiveness data from the nlst trial have not yet been published . 
estimates of the cost - effectiveness of screening ct have relied on decision analysis modeling with estimates ranging from $50 , 000 up to $2 , 000 , 000 per quality - adjusted life year gained [ 19 ]  . is extremely important for institutions to develop programs for lung cancer screening . 
in europe , there has been much discussion of the possibility of training physician extenders ( such as technologists or radiographers ) , interpretation of to provide the initial screening examinations . 
evidence - based infrastructure must be in place to secure that patients have access to uniform quality care and a similar life saving benet from ct examinations that was demonstrated in the national lung cancer screening trial . 
on the basis of the clinicalradiological evolution , we analysed complete ablation ( ca ) versus partial ablation ( pa ) at the rst computed tomography ( ct ) scan and during the follow - up ( mean 23 months ) , time to progression ( ttp ) and survival . 
a threshold of 30 mm ( p = 0.0030 ) and the histological type ( nsclc 75 % / mts 94 % ; p = 0.0305 ) were also predictive of ca . 
filippini dipartimento di scienze chirurgiche , universita` di torino , corso bramante 88 , 10126 turin , italy conclusion rfa for thoracic malignancies is accurate for lesions up to 30 mm , especially if metastatic ; survival is more closely related to staging factors than to the local effectiveness of rfa . keywords radiofrequency ( cid : 2 ) thermal ablation ( cid : 2 ) tumour ( cid : 2 ) lung ( cid : 2 ) thorax introduction primary tumours of the lung are the leading cause of cancer mortality worldwide , amounting to 1.2 million deaths each year [ 1 ]  . 
improving survival in nonsmall - cell lung cancer ( nsclc ) requires early diagnosis and effective treatment . lobectomy with hilar and mediastinal lymph node sampling is still the gold standard treatment for nsclc in stages i and ii . 
unfortunately , many patients are not good candidates for lobar resection [ 2 ]  . pulmonary metastases ( mts ) are present in 2530 % of patients suffering from different types of cancer ; for some patients with oligometastatic pulmonary disease , metastasectomy seems to be associated with improved survival [ 3 ]  . radiotherapy ( rt ) has been offered as an alternative to surgery for both nsclc and mts ; however , the 5 - year survival after traditional rt remains low ( 1520 % ) , with a high rate of local recurrence ( lr ) [ 4 ]  . the last few decades have seen an increase in the detection of smaller neoplasms ( in part as a result of low - dose ct screening for nsclc [ 5 ] ) and , at the same time , the development of new local therapeutic possibilities , e.g. 
initially applied to other solid tumours , it has been also used in the chest to increase the possibility of local control of the tumour in inoperable patients [ 7 ]  . radiol med ( 2014 ) 119 : 3340 this study discusses the safety , efcacy and clinical utility of thermal ablation of nsclcs and pulmonary mts ( mainly from colorectal cancercrc ) by presenting our results in terms of survival and prognostic factors and comparing them with the literature data . materials and methods of a total of 1 , 591 patients who underwent rfa at our institution since the late 1990s , 94 ( 5.9 % ) were treated for thoracic cancers . 
to assess the signicance of rfa in this type of cancers , we conducted a retrospective study on a series treated between 2002 and 2011 , consisting of 81 consecutive patients who underwent rfa for 100 thoracic lesions . the study was carried out in accordance with the guidelines on retrospective analyses established by our hospitals institutional review board . patients and lesions each patient was referred for treatment on the basis of clinical indications , after a multidisciplinary assessment by an interventional radiologist , a thoracic surgeon , a medical oncologist and an anaesthesiologist . 
the rfa technique was established based on the interventional radiologists technical evaluation . the lesions treated with rfa were not candidates for surgery due to the following reasons : reduced pulmonary function ; compromised general and / or cardiovascular condition ; advanced age of the patient ; location of the lesions in both lungs ; presence of extrapulmonary disease , but of limited extent ; refusal of the patient to undergo surgery . depending on the histological type of neoplasm , our patients can be divided into two groups : a group suffering from primary lung cancer ( nsclc ) and a second group with pulmonary mts , mainly from crc . at the time of rfa , 61 of the 81 patients were male ( 75 % ) with a mean age of 61.6 years ( median 66 ) and 20 were females ( 25 % ) with a mean age of 68.7 years the average age was 61.7 years ( median 70.5 ) ; overall ( range 1788 years ; median 66 )  . fifty - ve of the eighty - one patients ( 67.9 % ) had received other treatments prior to thoracic rfa ( including six liver rfa ) ; nine patients suffering from mts from crc underwent liver rfa synchronous to the pulmonary rfa . 
thirty - four of the eighty - one patients ( 42 % ) were also affected by extrapulmonary mts . one hundred lesions were treated : 30 nsclc ( 30 % ) and 70 mts [ 51 / 70 from crc ( 72.8 % ) , 6 / 70 from sarcomas ( 8.5 % ) , four from hepatocellular carcinoma , two from gastric carcinoma and the remaining seven from cholangiocarcinoma , laryngeal , breast , ovary , parotid , prostate and kidney cancer , respectively ]  . 
specically 79 lesions ( 79 % ) a diameter \3 cm , and 40 lesions ( 40 % ) had a diameter \2 cm . the lung lesions were solitary in 48 cases ( 48 % ) and multiple in 52 cases ( 52 % )  . preprocedural assessment before treatment , general and cardiorespiratory condition ( performance status ) was evaluated . 
in addition , preprocedural ct or positron - emission tomography ( pet ) ct staging was requested , preferably not more than 1 month before the procedure . pathological diagnoses were available for all of the nsclcs ; the mts were mostly recognised as such on the basis of their clinical evolution and imaging characteristics ; in a few cases only ( e.g. those with atypical imaging appearance ) biopsies were performed . for each patient we requested clotting tests ( in case they needed correction of thrombocytopenia or inr or ptt elongation ) and electrocardiograsubsequently , an anaesthesiological consultation was held . 
finally , any antitherapy was modied or coagulation or antiplatelet suspended . the indications , potential benets and risks of the procedure were discussed with the patients , who always signed a consent form . procedure the rfa was performed percutaneously in all 81 patients . the needle electrodes used for thoracic rfa were always of the expandable type . 
in particular , the systems used were rita ( rita medical systems , usa ) ( 15 / 100 cases ) , leveen ( boston scientic corporation , usa ) ( 75 / 100 ) and meditalia ( meditalia biomedica , italy ) ( 10 / 100 ) , with different opening diameters . 
the rita system is regulated by the temperature reached in the tissues ( based on the application time ) , the leveen system is impedance based , and the meditalia system can be based on either impedance or temperature . 
this , in addition to preventing neoplastic seeding , allows drainage of any pneumothorax during withdrawal . four hours after the procedure , a chest x - ray was obtained in all cases . 
in any case , patients were kept under observation for one night after treatment to monitor their clinical condition and blood count , and follow the possible evolution of pneumothorax . all adverse events were recorded , categorised according to the sir criteria into minor events ( clinically relevant ) and major complications ( requiring interventional radiological or surgical intervention ) [ 7 ] , and counted in terms of numbers and percentages . follow - up the result of the rfa was evaluated by performing contrast - enhanced ct 1 month after the procedure , to highlight the possible presence of residual viable tissue . 
in the case of complete ablation ( ca ) at the rst ct scan , patients were placed on a protocol of follow - up with 4 monthly ct studies ( but for patients with mts , follow - up intervals were sometimes changed on the basis of the evolution of metastatic disease and / or in relation to systemic therapy ) ; doubtful cases were examined by petct to establish possible lr . the possible local or general evolutions of pathology were considered as : no evidence of residual / local recurrence of disease ( ca ) ; evidence of residual local disease ( partial ablation , pa ) ; evidence of local recurrence of disease ( lr ) ; death . in particular , the ct appearance of ca was assessed by applying the ve possible patterns indicated in a recent classication by palussiere et al . 
 [ 8 ] ( atelectasis , cavitation , disappearance , nodule and brosis )  . based on these parameters , it was possible to calculate : local effectiveness ( ca versus pa ) at the rst ct scan ; follow - up ( range 1115 months ; local effectiveness at mean 23 months ) ( ca versus pa ? lr ) , time to progression ( ttp ) , and mid - term survival . 
in this regard , since there was a problem of patients being affected by two different neoplasms ( nsclc and mts ) , we were unable to carry out a study of cancer - specic survival ( to be further divided , in the case of mts , according to the different primary tumours ) , because the numbers would be so small fig . 
at the follow - up ct scan , appearance of a uid collection , with a small air - uid level : the patient required prolonged hospitalisation and antibiotic therapy fig . 
at ct scan 1 month later , favourable appearance of the ablated area ( mixed nodular - atelectatic evolution ) , and regression of the pneumatocele discussion among all the rfa applications , the indication for treatment of thoracic tumours is still marginal , as attested by our experience ( only 6 % of all patients undergoing rfa at our institution , despite it receiving referrals from important regional thoracic surgery and oncology centres ) and the fact that the sir reporting standard for these procedures was only published in 2009 , while more general ones were issued in 2003 . 
furthermore , with regard to nsclc , no evidence - based approach is available to date which claries the role of various treatments in general or the specic indications for rfa [ 7 ]  . rfa is therefore suggested in patients with primary lung cancers or mts ( especially from crc ) who are considered inoperable due to medical conditions or to the unfavourable position of the tumour [ 9 , 10 ]  . 
at the rst follow - up ct scan , complete ablation is diagnosed on the basis of the absence of contrast enhancement ; a subsequent ct scan shows evidence of local progression of the tumour on the anteriormedial side of the lesion fig . 
5 bulky metastasis from humeral osteosarcoma at the apex of the left the follow - up ct scan , after multiple needle placements , an enhancing ring of viable tissue can still be seen , due to partial ablation ( pa ) lung : at regards the treatment of mts , the choice was the result of a multidisciplinary assessment and it was included in a multimodal therapeutic strategy . during the rfa sessions , all patients were treated using conscious sedation rather than general anaesthesia . 
this implies some advantages , such as the partial respiratory collaboration of the patient and the possibility of using the usual radiological roonot being able to place the patient in a prone position constitutes the main disadvantage , which can be overcome by having patients lie in the lateral position . 
in the literature , comparisons of general anaesthesia and conscious sedation during thoracic rfa did not show signicant differences in terms of feasibility , technical success and complication rate [ 11 ]  . rfa of thoracic tumours is an excellent option to prehealthy function , without sacricing lung serve fig . 
the absence of extrapulmonary metastases was a favourable predictive factor for survival at 3 years ( p = 0.0261 ) parenchyma , and it is a relatively safe procedure , with low mortality ( about 0.4 % ) [ 12 ]  . 
these data are similar to those reported by de baere [ 17 ] , who described a higher rate of local control for mts from crc compared with nsclc , renal cell carcinoma or hepatocellular carcinoma ( p = 0.023 ) ; however , multivariate analysis showed that the relative risk of local progression of a particular type of cancer was comparable to that of other histological types . 
 [ 15 ] showed a better local control in the treatment of mts from crc compared to nsclc ( and also to mts from other types of cancer ) , but without reaching a statistically signicant correlation . in our study , overall survival at 1 , 2 and 3 years after treatment was 84 , 65 and 51 % , respectively . the rst stratication curves , based on the different tumour histological types , showed no statistically signicant differences between nsclc and mts , but this nding could be affected by the relatively short average follow - up and by the limited sample size , especially for nsclc . 
the local efcacy of radiofrequency ablation was not signicant for survival at 3 years , but the observation of the two survival curves suggests an advantage for patients with maintained ca at shorter intervals our results are in line with those of the best series reported in the literature , in particular as regards the rate of major complications ( 7 % ) ; in fact , the development of a limited pneumothorax , which affects a large percentage of patients , often resolves without any medical intervention or with a simple drainage and could therefore be counted among the minor complications [ 15 ]  . in the literature , while a consensus regarding the denition of ca has been reached , there are different denitions for pa . 
when there is radiographic evidence that ca has been reached at the rst follow - up after rfa , ca shall be deemed to be maintained until the new development of viable tumour during the follow - up , in which case it is commonly called lr , even though the term local tumour progression should be preferred , since the lr is essentially a lesion not completely ablated [ 16 ]  . in our study , we used univariate analysis to evaluate possible variables that can inuence the effectiveness of local rfa . 
 [ 17 ] indicated , as favourable factors for local effectiveness , a tumour size threshold of 2 cm and the use of expandable needle electrodes ; conversely , proximity with radiol med ( 2014 ) 119 : 3340 7 . 
rose sc , dupuy de , gervais da , for the technology assessment committee of the society of interventional radiology et al ( 2009 ) research reporting standards for percutaneous thermal ablation of lung neoplasms . 
hoffmann rt , jakobs tf , lubienski a et al ( 2006 ) percutaneous radiofrequency ablation of pulmonary tumors : is there a difference between treatment under general anaesthesia and under conscious sedation ? eur j radiol 59 : 168174 12 . 
de bae`re t , palussie`re j , auperin a et al ( 2006 ) mid - term local efcacy and survival after radiofrequency ablation of lung tumors with minimum follow - up of 1 year : prospective evaluation . radiology 240 : 587589 13 . 
hiraki t , sakurai j , tsuda t et al ( 2006 ) risk factors for local progression after percutaneous radiofrequency ablation of lung tumors : evaluation based on a preliminary review of 342 tumors . cancer 107 : 28732888 16 . 
goldberg sn , grassi cj , cardella jf , for the society of interventional radiology technology assessment committee and the international working group on image - guided tumor ablation et al ( 2009 ) image - guided tumor ablation : standardization of terminology and reporting criteria . 
fernando hc , de hoyos a , landreneau rj et al ( 2005 ) radiofrequency ablation for the treatment of non - small - cell lung cancer in marginal surgical candidates . 
lencioni r , crocetti l , cioni r et al ( 2008 ) response to radiofrequency ablation of pulmonary tumors : a prospective , intentionto - treat , multicentric clinical trial ( the rapture study )  . 
remembering that diameter is one of the cornerstones of tumour staging , at least for nsclcs , the better survival rate of patients with smaller lesions is believed to be partly related to the natural history of the disease . 
to verify the real impact of the rfa on survival , we therefore stratied the patients by local effectiveness of rfa : the difference between the survival curves at 3 years of ca versus treatment failures ( pa and lr ) was not statistically signicant , consistent with what was reported until the last decade [ 23 ] ; the observation of a trend in favour of effective treatment in the rst 2 years , however , lets us hope that the clinical utility of these treatments can be demonstrated later , preferably by randomised trials . conclusions the growing experience with rfa of thoracic tumours , including our rst 100 cases , demonstrates the safety and efcacy of local treatment for small tumours ; the predictive factors for a longer survival are mainly related to staging ( tumour diameter and presence of extrapulmonary disease ) , as for the other cancer therapies . 
the accuracy , sensitivity , specicity , positive predictive value ( ppv ) , and negative predictive value ( npv ) of measures used to detect ps were determined by patient - based and aberrant systemic artery - based evaluations . 
the capability of cta to provide a working view and the accuracy of measurements in choosing a coil were also assessed . results digital subtraction angiography and / or surgery revealed ps in 38 patients , and 7 patients had no ps . 
the patient - based evaluation yielded an accuracy of 97.8 % , sensitivity of 97.4 % , specicity of 100 % , ppv of 100 % and npv of 87.5 % , in the detection of ps . 
li department of interventional radiology , the first afliated hospital , zhengzhou university , no.1 , east jian she road , zhengzhou 450052 , henan , republic of china e - mail : rjzjrk@126.com conclusions 64 - row cta appears to be effective in terms of supporting accurate diagnosis and pre - treatment planning in ps . 
cta is not only able to provide clear visualisation of aberrant systemic arteries but also provides detailed images of abnormal lung parenchyma and the airways . keywords pulmonary sequestration ( cid : 2 ) angiography ( cid : 2 ) dsa ( cid : 2 ) endovascular introduction pulmonary sequestration ( ps ) is a rare congenital pulmonary disorder dened by an area of dysplastic and nonfunctioning pulmonary tissue which has an anomalous systemic blood supply [ 1 ]  . 
in recent years , less invasive imaging techniques , particularly helical multislice computed tomographic angiography ( cta ) , have proved to be equally effective and safer alternatives to dsa [ 313 ]  . 
cta can provide the precise visualisation of the site , size and number of aberrant systemic arteries and their relationship to the aorta , which are fundamental factors that must be assessed before choosing between endovascular and neurosurgical treatments . previous reports in the literature have assessed the sensitivity and specicity of cta compared with dsa [ 3 13 ]  . 
however , these investigations have not analysed the clinical implications of a protocol that replaces dsa with cta as the only diagnostic and pre - treatment planning tool for patients with ps . 
therefore , the purpose of the current study was to evaluate the clinical implications and clinical results of a prospective protocol using 64 - row cta for the diagnosis and endovascular treatment of ps . materials and methods study design the institutional review board approved the study protocol , and patients or qualifying family members provided informed consent before participation . 
the site of origin , distribution , and course of ps were evaluated on the basis of mpr , mip , and vr by adjusting the value of translucency or slab thickness . 
conventional 2d - dsa was performed on a monoplanar unit ( axiom artis vb22n , siemens ) with a 1 , 024 9 1 , 024 matrix and a 17 9 20 cm eld of view . the access routes for angiography were the umbilical artery ( neonates ) and the femoral artery . 
this was classied as insufcient information provided , endovascular treatment probably possible or probably not possible , or endovascular treatment denitely possible , or denitely not possible . the treatment which was actually carried out was recorded in each case . 
in the case of surgery , direct conrmation was obtained by means of visualisation of the aneurysin the case of endovascular treatment , indirect conrmation was partially provided using the following two additional parameters , which were evaluated using mpr : 1 . 
the possibility of obtaining a view on cta of the aberrant systemic artery in ps in relation to the aorta that could be reproduced on the c arthis was classied as either possible or impossible . 
this parameter was classied as the correct or incorrect choice of coil . statistical analyses the categorical demographic and basic characteristic variables , expressed as numbers and percentages , were compared using the chi squared test . 
the diagnostic performance parameters of cta for the diagnosis of pulmonary sequestration compared with those of dsa [ that is , accuracy , sensitivity , specicity , positive predictive values ( ppv ) , and negative predictive values ( npv ) ] were expressed as percentages ( 95 % ci )  . 
aberrant systemic arteries originating from the thoracic artery were evident in 38 patients , and no aberrant systemic artery was exhibited in the remaining 7 patients . dsa or surgery results according to the reference standard , ps was detected in 38 patients and 7 patients had no demonstrable ps . 
dsa revealed 46 aberrant systemic arteries in 38 of the 44 patients : in 2 patients , 3 arteries were detected ; 4 patients each had 2 arteries detected ; and a single artery was detected in 32 patients . diagnostic performance of cta the diagnostic accuracy , sensitivity , specicity , ppv , and npv of cta in the patient - based and aberrant systemic artery - based evaluation on cta are detailed in table 2 . single - patient sample images acquired with cta and dsa are shown in fig . 
cta also revealed 45 aberrant systemic arteries in 38 of the 45 patients : in 1 patient , 3 arteries were detected ; 5 patients each had 2 arteries detected ; and a single artery was detected in 32 patients . 
a axial multiplanar reconstruction ( mpr ) image demonstrates a homogenous solid mass in the posterobasal segment of the right lower lobe with an aberrant systemic artery ( arrow )  . 
b coronal maximum intensity projection ( mip ) exhibits an aberrant systemic artery ( arrow ) arising from the hepatic artery supplying the mass in the right lower lobe . c pre - embolisation aortography shows the aberrant artery ( arrow ) from the hepatic artery . d post - embolisation angiography conrms complete occlusion of the aberrant artery with coils ( arrow ) aberrant systemic arteries detected in one patient was falsenegative on cta . potential for endovascular treatment in 38 patients with ps , mpr images provided sufcient information on the site , number and size of aberrant systemic arteries in 37 ( 97 % ) of 38 patients , and insufcient information in one patient with multiple aberrant systemic arteries . 
in fact , endovascular treatment was performed in 36 patients with ps , and 2 patients opted for surgery due to other complications . radiol med ( 2014 ) 119 : 2732 the surgery carried out in these patients demonstrated that cta ndings about the aberrant systemic arteries had been correct . view for performing endovascular treatment ( working view ) in 36 patients with ps where endovascular treatment was possible , mpr analysis allowed us to easily nd the working view that clearly demonstrated the location of the aberrant systemic artery and could be used to perform endovascular treatment . 
this working view was then reproduced on the c arthe resultant cta series was always similar to the dsa view and satisfactory for performing endovascular treatment . size of the aberrant systemic artery in the 36 patients with pss suitable for coil embolisation , measurements the size of the aberrant systemic artery were performed on mpr . 
the coil selected was appropriate in 35 ( 97 % ) of 36 treated patients with ps . discussion this prospective study was based on our hypothesis that cta could replace dsa as a reliable diagnostic and pretreatment planning tool for patients with ps . 
in this study , the high accuracy ( [ 95 % ) and sensitivity ( [ 95 % ) of cta for detecting ps was equivalent to the gold standard , dsa , indicating that cta cannot only replace the dsa for the diagnosis of ps but can also differentiate ps from other similar conditions . 
when compared with actual treatment decisions made using dsa or surgery , cta provided an effective diagnostic performance , delineating aberrant systemic arteries and enabling appropriate coil selection prior to embolisation in 37 of 38 patients with ps . 
this suggests the potential of cta as an effective tool which could be used alone in treatment planning for most patients with ps . pulmonary sequestration is a rare congenital malformation that represents 0.156.4 % of all pulmonary malformations [ 14 , 15 ]  . 
traditionally , the diagnosis of ps requires arteriography to identify abnormal systemic vessels feeding the abnormal portion of the lung and to provide valuable information for preoperative planning [ 2 , 16 ]  . 
recently , the quality and accuracy of cta , particularly helical multi - slice cta , has been seen to be approaching that of catheter dsa , which has been the gold standard diagnostic tool malformations . in patients with pulmonary the advantages of cta are that , compared with dsa , it is noninvasive , has a much lower risk of complication or morbidity , can be performed much more quickly , requires is not fewer resources ( stafng , equipment , and cost ) , painful to the patient , does not require sedation ( in most patients ) , and is more suitable for critically ill or unstable patients . 
conversely , while dsa can clearly identify aberrant feeding arteries in ps , it is invasive , associated with radiation , time - consuming , relatively expensive , and requires hospitalisation . although there have been many reports in the literature that assess the validity of cta as a diagnostic technique for the detection of ps , few have evaluated the clinical implications of a protocol that uses cta instead of dsa as a diagnostic and pre - treatment planning tool . 
if cta is to serve as a non - invasive replacement for dsa in pre - treatment planning , it must provide precise visualisation of the site and number of aberrant systemic arteries and their relationships to the aorta . 
in addition , it is essential to know the shape and the size of the feeding artery before performing endovascular treatment using coil embolisation . our study showed that therapeutic decisions could be based on information provided by cta alone in most cases because 64 - section cta is capable of three - dimensional reconstructions in unlimited projections . 
we found that certain reconstruction algorithms , such as vr reconstructed images and mprs , may provide useful anatomical information about the ps that closely approximates intraoperative ndings . in the investigation of a suspected case of ps , ct , and cta have two principal objectives : to rule out other pathologies and to conrm the presence of an anomalous arterial supply [ 4 , 9 , 16 ]  . 
cta is able not only to identify the systemic artery supply , but also yields the maximum information about the lung parenchyma including the airsuch as bronchiectasis , atelectasis ways . 
these are not amenable to diagnosis by colour doppler sonography , magnetic resonance imaging or dsa , whereas they can be detected with high accuracy by ct [ 17 ]  . 
in other words , cta is the sole diagnostic method which can delineate the origin and course of anomalous systemic arteries and venous drainage accurately as well as evaluating abnormal lung parenchyma and the airways . recently , endovascular coil embolisation has provided a less invasive alternative to surgery [ 1823 ] , especially for neonates or children . 
while cta facilitates a simple and reproducible angiographic protocol , dsa has been part of our angiographic protocol in undetermined cases . for endovascular treatment , one must use a twodimensional view that clearly depicts the aberrant systemic artery in relation to adjacent vessels and could be used to perform treatment in optimal conditions . 
precise measurements of the size of the aberrant systemic artery that were obtained by using mprs on cta imaging helped us in this important and difcult choice , especially in determining the coil diameter . 
last , the dose of the contrast material may be high for paediatric patients ; therefore , a more extensive evaluation of patient dose should be performed taking age into consideration . in conclusion , 64 - row cta appears to be effective in terms of supporting accurate diagnosis and pre - treatment planning in ps . 
we aimed to investigate the impact of a breathing - control system on irradiated volumes and dosimetric parameters in three - dimensional conformal radiotherapy ( 3d - crt ) and stereotactic radiotherapy ( srt ) treatments . materials and methods twelve patients were scheduled for radical radiotherapy : ve for srt and seven for 3dcrt . 
signicant differences were found both in srt and in 3d - crt , peripheral and apical lesions . conclusion in our experience , abc has the potential to reduce lung toxicity in the treatment of lung cancer ; it can allow the prescribed dose to be alternatively , increased while maintaining the same risk of lung toxicity . keywords active breathing control ( abc ) ( cid : 2 ) internal target volume ( itv ) ( cid : 2 ) lung dose ( mld ) ( cid : 2 ) radiotherapy ( cid : 2 ) target volumes introduction treating lung cancer with radiotherapy ( rt ) or radiochemotherapy ( rct ) is hindered by the tolerance of normal tissues in the thorax [ 1 ]  . 
local control is known to be correlated with improved overall survival , both in nsclc and in sclc . in conventional 3d - conformal rt ( 3d - crt ) , treatment eld sizes are usually large enough to take into account tumour motion . 
the reduction of organ motion and the correlated increased accuracy in patient positioning is under investigation in stereotactic radiotherapy ( srt ) [ 9 ]  . radiol med ( 2014 ) 119 : 1319 table 1 clinicalpathological features of the 12 lung cancer patients several methods exist to coordinate respiratory motion , including active breathing control or coordination ( abc ) [ 10 ] , real - time tumour - tracking systems [ 11 ] , respiratory gating systems , voluntary deep inspiration breath - hold ( dibh ) [ 12 , 13 ] and abdominal compression . 
the aim of this study was to evaluate the impact of abc on treatment volumes and to correlate the variations in predicting lung toxicity . materials and methods from march to october 2011 , 12 patients ( nine men and three women ) , 5 scheduled for srt and 7 for 3d - crt for lung lesions , were selected for our study . 
the active breathing coordinator device ( abc , elekta oncology systems ltd . , crawley , west sussex , uk ) consists of a mouthpiece connected to a ow meter system to measure the volume of air that moves through the transducer as a function of time , thus monitoring patient respiration . 
no breath - hold was performed , but after recording normal respiration , the patient was asked to breathe in a window as narrow as possible . this window was established in a rst training phase . 
for each patient affected by lung lesions , together with the freebreathing ct scan , four additional sets of ct slices were acquired : two in the maximum and minimum phases of a free - breathing cycle and two in the maximum and minimum phases of a breathing cycle controlled by the abc system . the tumour was outlined by only one operator . 
the freebreathing internal target volume ( itv ) [ 14 ] was created from enlargement of lesion visualised in the free - breathing ct scan with fusion images of the tumour in the maximum and minimum phases of a free - breathing cycle . 
the controlled - breathing itv was created from the sum of the tumour volume in free - breathing ct scan and maximum and minimum phases of a controlled - breathing cycle . 
in the case of 3d - crt treatment , gross tumour volume ( gtv ) for primary lesion ( gtvt ) and a gtv for metastatic lymph nodes ( gtvn ) were contoured . 
the planning target volume ( ptv ) was obtained by an isotropic automatic expansion of 1 cm to ctvt ( ptvt ) and 0.7 cm to ctvn ( ptvn )  . 
for srt , gtv was contoured on the lung window , and ptv was obtained by an isotropic automatic expansion of 1 cspinal cord , normal affected lung ( dened as normal tissue of affected lung minus ptv ) , normal unaffected lung ( dened as lung volume opposite the target lesion ) , oesophagus and heart were outlined as organs at risk . 
in particular , abc allowed for a signicant reduction in volumes in both srt and 3d - crt treatments . results all 12 selected patients were able to tolerate the abc device during the study procedures . target volumes ( itv and ptv ) figure 1 shows itv for both free and controlled breathing in all patients . 
signicant differences in v20 were found in 3dlesions crt plans ( p = 0.034 ) and in apex lesions ( p = 0.012 ) ( table 4 )  . in peripheral ( p = 0.026 ) , target figure 3 shows mld values for both free and controlled breathing in all patients . 
many discussion studies show that radiation dose and volume to lungs are associated with the risk of radiation pneumonitis , such as mld [ 17 ] , normal tissue complication probability ( ntcp ) value and relative volume of lung receiving more than a threshold dose ( v dose ) [ 18 ]  . 
in the royal marsden experience [ 20 ] , the majority of patients suitable for radical radiotherapy tolerated abc ; compliance was conrmed in our study , where all patients were able to understand the instructions and follow the procedures for the abc device . 
our data show a 1734 % reduction in v20 in both srt and 3d - crt treatments , whereas the advantage is smaller but still statistically signicant in mld reduction ( 6 and 9 % reduction srt and 3d - crt , respectively )  . 
previous studies show that lower - lobe tumours tend to move more than upper - lobe tumours during free breathing [ 21 ] : these data are apparently in contrast with our results . 
however , we believe that the greater variability in inter - breath - hold itv and the smaller number ( four vs . eight ) of lower - lobe tumours in our series can be a bias in the interpretation of our results . 
v20 is the metric or surrogate for the risk of lung toxicity [ 22 ] , and the reduction in tumour motion is a key concept that is correlated with this dosimetric parameter in the dosevolume histogram . reduced v20 can be considered a primary endpoint for obtaining a safe dose escalation in treating lung cancer . alternatively , abc may allow dose escalation while maintaining the same risk of lung toxicity [ 23 ]  . radiol med ( 2014 ) 119 : 1319 radiol med ( 2014 ) 119 : 1319 luca cardillo , g . 
lesions with a diameter b3 cm were treated with a single antenna , lesions with a diameter [ 3 cm were treated by positioning two or more antennae , simultaneously . 
all patients underwent computed tomography ( ct ) follow - up with and without contrast administration at 1 , 3 and 6 months and then yearly in combination with complete blood and metabolic tests . results technical success was 100 % . 
partial necrosis was obtained in 30.8 % ( 8 / 26 lesions ) ; in one case ( 3.8 % ) a progression of the disease was recorded and in another case ( 3.8 % ) a stability was observed . conclusions our preliminary experience may be considered in accordance with literature dates , in terms of efcacy and safety . keywords microwave ablation ( cid : 2 ) lung tumours ( cid : 2 ) technical results introduction surgery remains the optimal treatment for early - stage lung cancer , with a reported 5 - year survival rate of approximately 70 % , but the majority of patients present with advanced disease are not suitable for surgery [ 1 ]  . the lungs are also a common site of metastatic spread , and to date , the standard treatment for isolated pulmonary metastasis has been surgical resection with an overall 5 - year survival after resection ranged 2040 % [ 2 ]  . while the treatment of choice has historically been resection , newer therapies that do not require pulmonary resection are arising such as ablation techniques to enable local control of unresectable tumours . 
over the years , various ablation techniques for the treatment of lung tumours have been developed , including ethanol ablation , laser ablation , cryoablation , radiofrequency ( rf ) ablation and microwave ( mw ) ablation . radiol med ( 2014 ) 119 : 7582 mw ablation offers all the benets of rf ablation as well as some substantial advantages , such as a larger volume of cell necrosis in a shorter procedure time , a larger zone of active heating , less susceptibility to heat - sink effect and less intraprocedural pamw ablation uses dielectric hysteresis to produce heat [ 3 , 4 ]  . 
heating of the tissue is based on agitation of water molecules inducing cellular death via coagulation necrosis ; the electrical charge on the water molecule ips back and forth 25 billion times per second , depending on the frequency of the microwave energy [ 5 , 6 ]  . 
this mechanism of heating differs from rf ablation , which creates heat via resistive heating when electrical current passes through the ionic tissue medium , resulting in heating of tissues only immediately adjacent to the electrode [ 3 ]  . comparing ablation zones obtained with a 14 - gauge microwave antenna vs those obtained with a 17 - gauge radiofrequency electrode in an in vivo normal porcine lung model , that one generated with the use of microwaves was 25 % larger in mean diameter and signicantly more circular , and developed faster than those achieved with radiofrequency energy [ 6 , 7 ]  . the aim of this study was to demonstrate the technical success , safety and efcacy of mw ablation in patients affected by unresectable lung cancer . materials and methods this retrospective study was approved by the ethics committee of our centre . 
twenty - four patients ( 15 men , 9 women ) with a mean age of 71.7 years ( range 4683 ) who underwent percutaneous mw ablation of 26 intraparenchymal pulmonary masses ( mean 1.08 lesions per patient ) in 36 ablation sessions between 26 november 2007 and 12 august 2011 were enroled in the study . a central tumour was dened as being entirely located within the inner two - thirds of the lung . 
a tumour was dened as peripheral if a portion of it resided in the outer one - third of the lung . all selected patients had neoplastic disease that was judged to be inoperable on the basis of tumour stage , comorbidities , advanced age and / or refusal to undergo surgery . 
the coagulation prole was in the normal range for all patients . patients undergoing anticoagulant and / or antiaggregant therapy interrupted treatment at least 7 days before the procedure , with the introduction of fractionated heparin when necessary . 
written informed consent was obtained from all patients . baseline imaging pre - treatment imaging consisted of a 64 multidetector - row computed tomography ( mdct ) chest scan extending to the abdomen ( aquilion 64 , toshiba , japan ) with and without contrast medium administration . 
the contrast - enhanced scans were acquired after injection of 100 ml of iodinated contrast agent ( visipaque 320 , ge healthcare , usa ) at an injection rate of 3 ml / s , followed by injection of 40 ml saline at a rate of 2 ml / s . 
one week prior to the ablation treatment , all patients underwent percutaneous pulmonary biopsy under computed tomography ( ct ) guidance , with histological conrmation of malignancy for all lesions . pre - treatment procedure the patient is in supine or prone position according to the site of the lesion . 
each patient is kept in a state of moderate sedation through intravenous administration of a combination of midazolam ( ipnovel 15 ; roche , milan , italy ) ( 0.070.08 mg / kg ) , propofol ( diprivan , astrazeneca spa . , caponago , italy ) ( 0.52.0 mg / kg / h ) and fentanyl ( fentanest ; pharmacia & upjohn , milan , italy ) ( 12 lg / kg )  . heart rate , electrocardiographic trace , oxygen saturation , respiratory frequency and blood pressure are continuously monitored throughout the procedure . 
at the end of the procedure , a ct scan or a cbct was performed to evaluate the presence of pneumothorax ; if present , the patients underwent chest radiography 2 h later to monitor the pneumothorax . follow - up yearly in combination with complete blood and metabolic tests . the following imaging characteristics were evaluated : total volume of the ablated area , presence of cavitation , absent enhancement of the lesion ( \15 hu ) , pleural effusion and adenopathy ( short axis [ 1 cm ) , according to the response evaluation criteria in solid tumours ( recist ) [ 3 , 4 , 8 ]  . all complications were recorded and classied in accordance with the common terminology criteria for adverse events version 4.0 ( ctcae ) [ 9 ]  . outcomes : technical success , safety and efcacy of the technique all patients underwent ct follow - up with and without contrast administration at 1 , 3 and 6 months and technical success was dened as the correct positioning of the antennae within the lesion . 
the efcacy of the technique was evaluated on the basis of imaging characteristics , using the recist criteria [ 8 , 11 ]  . efcacy statistical analysis overall survival ( os ) was estimated using the kaplan meier method [ 12 ]  . 
a wilcoxon matched - pairs test was used to compare the size of the tumours before and after ablation using the medcalc 12.0 statistical package ( medcalc software , broekstraat 52 , 9030 mariakerke , belgium )  . 
a difference with p value \0.05 was considered statistically signicant . results tumours were measured in the three dimensions ( transverse , anteriorposterior and longitudinal ) obtaining a mean index of the maximum diameter of 30.96 mm ( range 8100 mm )  . 
histological analysis showed that the lesions were : 14 non - small cell lung carcinoma ( nsclc ) ( 6 squamous cell pulmonary carcinomas , 7 adenocarcinomas and 1 neuroendocrine carcinoma ) , 11 metastasis ( from primary tumours located elsewhere ) and 1 microcytoma . safety no major complications were recorded in the intraand peri - procedural period . 
there were no cases of symptomatic grade - 2 pneumothorax , nor were there any cases of skin burns induced by microwave - related thermal damage [ 13 , 14 ]  . 
additional ct scans were performed at intervals of 1 ( all patients ) , 3 ( 23 / 24 patients ) , 6 months ( 6 / 24 patients ) and yearly ( 11 / 24 patients )  . after an initial increase of the maximum diameters , there was a persistent reduction in diameter of the ablated areas at subsequent examinations , consistent with consolidation of the pulmonary parenchyma . 
no statistically signicant correlation ( p \ 0.1 ) was found between tumour size ( \ or c3 cm ) , location ( central or peripheral ) , and type ( primary tumour or metastasis ) and os . 
c ct scan reveals cavitation ( star ) of the lesion after treatment mw ablation is a relatively new technique that can be applied to different types of tumour and offers all the benets of rf ablation as well as some substantial advantages . 
 [ 14 ] showed that , with a microwave ablation system tuned for the lung , large circular ablation zones in porcine lungs in vivo could be obtained with a single antenna . 
coagulation zones created with bronchial occlusion and multiple antennas placed and activated simultaneously were signicantly larger than those seen without bronchial occlusion and with a single antenna , respectively [ 7 , 14 ]  . 
the electromagnetic waves associated with mw are not limited by lower thermal conductivity of lung , or by the increased impedance of charred tissues [ 7 , 16 ]  . 
 [ 13 ] percutaneously treated 82 lung masses ( primary lung tumours and metastatic disease ) in 50 patients , using a 915 - mhz generator ( evident / covidien , boulder , co , usa ) and obtained a 67 % local control rate ( based on serial follow - up imaging with ct and positron emission tomography ) at 1 year , with a mean time to rst they observed an actuarial recurrence of 16.2 months ; survival of 65 % at 1 year , 55 % at 2 years , and 45 % at 3 years from ablation . 
cancer - specic mortality yielded a 1 - year survival of 83 % , a 2 - year survival of 73 % , and a 3 - year survival of 61 % ; these values were not signicantly affected by an index size of larger than 3 cm or 3 cm or smaller or presence of residual disease . 
pneumothorax was observed in 39 % of cases but 66 % of them were not drained . thermal ablation incites an inammatory / cytotoxic response in adjacent normal lung tissue that appears as ground - glass opacity or frank consolidation that initially increases the apparent size of the tumour . 
in fact , the size of the ground - glass opacity surrounding the ablated lesion on immediate post - ablation imaging has been shown to be predictive of an effective ablation . 
cavitation has been reported in up to 30 % of patients following mw and rf ablation and is associated with effective ablation and further complicates interpretation of post - ablation imaging [ 10 , 11 ]  . 
given the apparent increase in lesion volume following ablation , the authors follow - up protocol includes a post - ablation ct scan within 1 month of the procedure ( to serve as a new baseline ) and then contrast - enhanced ct at 3 - month intervals to determine treatment response . 
tumour morphology , volume , and contrast enhancement can be followed over time , and the authors consider tumours that are stable or decreasing in size and do not demonstrate more than 10 hu of contrast enhancement to be completely ablated [ 19 , 20 ]  . radiol med ( 2014 ) 119 : 7582 fig . 
f ct scan performed after the 2nd session of microwave ablation reveals complete necrosis in the recent and largest study to date on the mid - term outcomes of lung metastasis treated with mw ablation ( 130 lesions in 90 patients ) , vogl et al . 
 [ 21 ] showed successful tumour ablation was signicantly more frequent for lesions with a maximal axial diameter of 3 cm or smaller than for larger lesions and for peripheral lesions than for centrally located lesions . 
our results showed an os after mw ablation of 75 % after 12 months and 55 % after 24 months ; the overall 30 - day mortality rate was 0 % . 
3 overall survival ( os ) after microwave ablation was 75 % after 12 months and 55 % after 24 months radiol med ( 2014 ) 119 : 7582 fig . 
4 multiple logistic regression analysis ( p \ 0.02 ) showed a trend towards improvement of os in patients with metastasis ( a ) , with a diameter \3 cm ( b ) , and located peripherally ( c ) ( m metastasis , pr primary tumour , c central lesion , p peripheral lesion ) ( primary tumours and metastasis ) , our results may be considered to be in agreement with those of vogl [ 21 ]  . moreover , vogl et al . [ 21 ] observed a volumetric increase in size of the ablated metastases in all lesions at the 24 - hour follow - up study , attributed to the inammatory response and to the oedema created by the heat energy applied during the ablation process itself . 
the authors suggest the 3 - month follow - up study theoretically shows the true tumour volume after complete subsidence of the ablation - associated inammation response . in our experience as well there was a volumetric increase of the lesions after ablation . that positron emission tomography ( pet ) - ct has also been employed after ablation , and it can be advantageous as it is not limited to an anatomical evaluation . 
fluorodeoxy - glucose ( fdg ) uptake should decrease in tumours as early as 2 months following ablation , and nodules with a percentage reduction in fdg uptake \60 , or an absolute suv of 3.0 or greater at 2 months should be considered incompletely ablated and possibly requiring further treatment [ 20 , 22 ]  . 
given the above , we could hypothesise an important role for pet - ct in following up pulmonary ablations during the rst 3 months , to be followed by ct after the rst 3 months . a median 28 % ( range 4.561.1 % ) was reported for rf ablation in a recent metaanalysis with approximately 11 % ( range 3.338.9 % ) of these requiring chest tube placement [ 23 ]  . 
however , differential diagnosis is not always straightforward and the diagnosis of granulomatous disease , considering separately the clinical , radiological and pathological aspects , is at times incomplete or uncertain and requires multiin this paper , we propose a disciplinary assessment . combined hrct - pathological approach to assess both the topographical and morphological features of the lesions . based on topography , we can distinguish between granulomatous lesions distributed along the lymphatic vessels , with random distribution or centred on the airways . 
barozzi servizio di radiologia , ospedale bellaria maggiore , ausl di bologna , bologna , italy distribution of granulomas are those with haematogenous spread , the most typical of which is miliary tuberculosis ( tb )  . 
the anatomical approach is completed by the assessment of the morphological aspects of the lesions and associated signs , reecting both the possible mechanisms of spread and the different types of pathological and / or reparative tissue related to the disease . keywords granulomatous lung disease ( cid : 2 ) sarcoidosis ( cid : 2 ) tuberculosis ( cid : 2 ) hypersensitivity pneumonitis ( cid : 2 ) hrct introduction granulomatous lung diseases form a heterogeneous group of clinical entities which share the presence of granulomas presenting in the form of nodular clusters of macrophages , usually with epithelioid appearance , possibly associated with giant cells as a manifestation of t immunity ( cellmediated )  . 
they represent a frequent nding for pathologists and may be seen in the lung in a number of conditions , more commonly diffuse [ 1 ]  . there are several granulomatous lung diseases which have been classied according to different criteria . 
the most common classication is based on aetiology , with the diseases being divided into infectious and noninfectious ( table 1 ) ; this criterion is crucial for the implications on frequent and management and treatment . 
granulomas may be distributed along the lymphatics , randomly or along the small airways [ 3 , 4 ]  . the topographical approach is completed with the evaluation of lesions and a description of associated lesions , which are sometimes predominant and valuable to the diagnosis of these diseases . the morphological aspects of parasitic infections sarcoidosis dirolaria intravenous or inhalational talcosis vasculitis ( wegeners granulomatosis , churgstrauss syndrome ) lymphatic distribution the clinical diagnostic approach to this wide spectrum of diseases always includes imaging and in particular computed tomography ( ct )  . 
high - resolution ct ( hrct ) is the most commonly used investigation because granulomatous lung diseases are often diffused diseases and hrct provides a precise in vivo depiction , with accurate demonstration of their distribution and morphological features . 
less commonly , adenopathy affects internal mammary , paraverteberal perilymphatic distribution with a predilection for the upper lung zones , together with typically located adenopathies , is highly suggestive of sarcoidosis and helps to differentiate sarcoidosis from other granulomatous or nongranulomatous conditions with lymphatic distribution such as carcinomatous lymphangitis and lymphoproliferative disorders . 
the radiological differential diagnosis with berylliosis and silicosis may be impossible . berylliosis chronic berylliosis is caused by prolonged inhalation of dusts or fumes containing beryllium - based compounds or products . 
the pathological and hrct patterns are similar to those of sarcoidosis ; the differential diagnosis requires a history of exposure to beryllium or beryllium compounds [ 3 , 17 ]  . lymphocytic interstitial pneumonia ( lip ) granulomas are commonly present in lymphocytic interstitial pneumonia , even though this entity cannot be formally considered a granulomatous disease , as it is classied fig . 
the ct image with mediastinal window shows symmetrically enlarged bilateral hilar and subcarinal lymph nodes with amorphous calcications inside ( b ) radiol med ( 2014 ) 119 : 5463 fig . 
in over 50 % of the cases granulomas are scattered , small and located along the lymphatics or in the peribronchiolar interstitium [ 18 ]  . on hrct , the subpleural nodules are dense , with sharp margins and often associated with thin - walled cysts . 
they are the result of air trapping due to peribronchiolar lymphoid inltration [ 19 ]  . random distribution in the random distribution pattern , granulomas appear uniformly distributed within the secondary lobule and lung parenchyma . 
similarly to lymphatic nodules , random nodules show high density and sharp margins ( like opaque beads ) as they are interstitially located ; they are often small ( miliary ) and may be cavitated , as a result of necrosis suggestive of an infectious process . the prototype of random granulomatous lung disease is including miliary tb . 
even haematogenous metastases can mimic haematogenous granulomatous diseases . miliary infections ( tb and fungal infections ) infections , in particular those due to mycobacteria and fungi ( including pneumocystis jiroveci ) , are still considered the most common cause of lung granulomas so that the detection of granulomas should suggest a thorough search for microorganisms . 
the attempt to isolate the micro - organisms starts with the rst examination of the slide with haematoxylin eosin and proceeds with special stains and in particular ziehlneelsen ( for tb ) and grocott ( for fungi ) stains . 
4 miliary infection ( tb )  . the hrct sagittal view shows innumerable tiny nodules quite uniformly scattered throughout both lungs with a random distribution , only some of them touching the pleura ( a )  . 
5 airway - centered ( centrilobular ) soft nodules appear both pathologically ( a ) and radiologically ( b ) separated from the pleural surfaces and ssures by several millimetres ( pavid of pleura ) disease with nodular pattern is extrinsic allergic alveolitis , also called hypersensitivity pneumonitis . 
the branching opacities ( tree ) reect the presence of dilated and thickened bronchioles , whereas the nodular opacities ( buds ) represent clusters of partially or completely lled alveoli ( centrilobular nodules )  . 
these changes may have an acute or chronic infectious nature ( often in mycobacteriosis , especially when atypical ) or noninfectious nature ( allergic bronchopulmonary aspergillosis , aspiration syndrome , bronchiolitis associated with chronic intestinal infections , bronchocentric granulomatosis , hot tub lung and inhalation talcosis ) ( table 1 )  . 
the tree - in - bud sign , however , may also be present in other nongranulomatous conditions ( diffuse panbronchiolitis , follicular bronchiolitis , some cases of organising bronchiolitis , neoplasms and the so - called vascular tree in bud in thrombotic microangiopathy due to haematogenous micrometastasis ) [ 23 ]  . extrinsic allergic alveolitis ( hypersensitivity pneumonitis ) extrinsic allergic alveolitis ( also known as hypersensitivity pneumonitis ) in its subacute form is pathologically characterised by the presence of interstitial pneumonia , foci of bronchiolitis and small , poorly formed interstitial granulomas centred along the small airways [ 24 ]  . 
the branching opacities ( the tree ) reect the presence of dilated thickened bronchioles , whereas the nodular opacities ( the buds ) are due to clusters of lled alveoli ( centrilobular nodules ) fig . 
the ct image depicts ill - dened lowdensity centrilobular nodules ( snowake - like ) ; the nodules are diffusely and uniformly distributed through both lungs ( a )  . 
in approximately 80 % of the patients , there is also a diffuse ground - glass opacity secondary to extensive diffuse interstitial pneumonia . the possible combination of ground - glass opacity , reduced pulmonary attenuation and areas of normal parenchyma may give rise to an unusual appearance dened as head - cheese pattern , which is not pathognomonic but only suggestive of the disease in patients with a history of allergy [ 25 , 26 ]  . hot tub lung hot tub lung is caused by exposure to water contaminated by nontuberculous mycobacteria ( mycobacterium avium complex , mac )  . 
pathologically , this form presents several similarities with hypersensitivity pneumonitis ( interstitial inltrate , bronchiolar - centred but also random granulomas which are rarely necrotising ) [ 27 ]  . 
consistent with the pathological features , the hrct signs are similar to those seen in extrinsic allergic alveolitis and characterised by low - density centrilobular nodules , ground - glass opacities and possible lobular air trapping [ 28 ]  . mycobacterial infection the histological features of mycobacteriosis are several necrotising or non - necrotising granulomas distributed along the airways ( bronchi and bronchioles )  . 
it is often impossible to distinguish tuberculous from nontuberculous mycobacteria on the basis of morphology alone ; the differential diagnosis therefore relies on special stains , cultures or molecular biology techniques [ 21 , 29 ]  . radiologically , airway involvement manifests through tree - in - bud appearance resulting from granulomatous cellular bronchiolitis and bronchial wall thickening with or without bronchiectases , dense nodules and bronchocentric consolidations , at times cavitated due to necrosis . 
the nonclassic variant of atypical mycobacterioses is predominantly in the middle lobe and lingula in the form of bronchiectases , bronchiolectases and centrilobular nodules associated with mosaic hypoperfusion due to oblitrative bronchiolitis . 
in the classic form , the ct coronal view shows tree - in - bud pattern and sporadic airway - centred nodules in the upper lobes ( a )  . in another female patient with nonclassic form ( lady windermere syndrome ) , bronchiectases are prevalent in the middle and lingular lobes ; mosaic hypoperfusion also coexists in the lower lobes ( b ) fig . 
there may also be consolidations , at times transient [ 32 ]  . chronic aspiration syndrome aspiration often concerns particles , such as food remnants ( especially vegetables ) , pill fragments , excipients , drugs or lipids . 
alcoholism is probably the most exogenous important predisposing factor in adults , even though other factors ( for example , structural abnormalities of the pharynx or oesophagus , neuromuscular disorders and deglutition abnormalities ) may also play a role in chronic aspiration . 
in the chronic form , ct may show a typical pattern consisting of fatty density in the context of parenchymal consolidations / nodules / masses , and often symmetrically which are bronchocentric associated with inammatory radiol med ( 2014 ) 119 : 5463 fig . 
bilateral gravitational areas with bronchial thickening and minimal tree - in - bud pattern ( a )  . ct scan with mediastinal window demonstrates oesophageal dilatation with an air - uid level ( b ) arranged in the posterior - basal segments . 
the presence of fatty attenuation values is noted in 7080 % of patients ; in the others , the radiological ndings are nonspecic [ 36 , 37 ]  . granulomatous vasculitides ( churgstrauss , wegener ) the granulomatous forms of vasculitis are characterised by an inammatory process affecting the vessel wall as a main feature ; rarely they manifest pathologically as a granulomatous interstitial pneumonia . churgstrauss syndrome ( css ) churgstrauss syndrome ( css ) , also known as allergic granulomatous angiitis , is a rare multisystem disease characterised by chronic rhinosinusitis , asthma and prominent eosinophilia in peripheral blood . 
the granulomas are well formed , necrotising , rich in eosinophils , and readily identied both in the vessel walls and around the bronchioles [ 38 , 39 ]  . radiologically , the most common manifestations are bilateral consolidations and ground - glass opacities which may be migratory and peripheral without predilection for site , a pathological expression of inammatory eosinophil or granulomatous involvement . 
in some cases , there may be associated mediastinal lymphoadenopathy due to reactive hyperplasia and eosinophil inltration [ 39 , 40 ]  . wegeners granulomatosis ( wg ) wegeners granulomatosis ( wg ) is a systemic necrotising vasculitis , which manifests with the classic triad of involvement of the upper and lower airways and kidney . the most common pathological nding is a combination of vasculitis and necrotising granulomatous inammation in a background of intense lymphoplasmacytic inltrate . 
the necrosis consists of large geographic areas and typically appears basophilic ( blue ) at low power [ 4 , 38 ]  . radiologically , the necrosis may appear in form of cavitation in the context of unior bilateral nodules or masses , which are multiple in about 85 % of the cases . these manifestations are often the initial signs of pulmonary disease . 
the alveolar haemorrhage may be diffuse in about 10 % of patients as a result of necrotising capillaritis , and present on ct as diffuse areas of parenchymal consolidation , ground - glass opacities and scattered low - density nodules ( 2550 % of cases )  . 
involvement of the airways is a late complication and may be present in 1525 % of patients . tracheal stenosis most frequently involves the subglottic portion ; it may be smooth or irregular [ 42 ]  . conclusions the heterogeneity of pulmonary granulomatous diseases may present to the clinician with patterns that are difcult to diagnose . 
correct diagnosis and treatment often relies on an interdisciplinary approach including clinical , imaging and pathological aspects . a combined pathological - hrct approach can help to understand and diagnose these diseases , similar to what has radiol med ( 2014 ) 119 : 5463 been demonstrated by other authors with regard to interstitial lung diseases . 
radiodiagnostica , universita` degli studi di bari , bari , italy 18fdg - pet / ct is useful in evaluating the conclusions extent of sarcoidosis and recognising lesions at different sites , including lymph nodes , lungs , liver , spleen and bone . it also improves the interpretation of the morphological lesions seen on mdct and depicts a larger number of lesions . 
therefore , 18fdg - pet / ct could be used to complement other more traditional techniques for the restaging and follow - up in patients with sarcoidosis . keywords sarcoidosis ( cid : 2 ) 18fdg ( cid : 2 ) pet / ct ( cid : 2 ) mdct ( cid : 2 ) follow - up introduction first described by hutchinson in 1877 [ 1 , 2 ] , sarcoidosis is a chronic , systemic , idiopathic disease ; the pathological hallmark of which is non - caseating granuloma characterised by macrophages surrounded by a rim of mononuclear cells . 
although sarcoidosis may involve any organ or system , it most commonly affects the chest structures and the upper respiratory tract , such that the lungs and mediastinal lymph nodes are almost invariably affected , even when the patient is asymptomatic [ 1 , 3 ]  . 
extrathoracic manifestations , usually associated with thoracic involvement , are seen in 2550 % of cases [ 1 ] and are represented by cervical , axillary and inguinal lymphadenopathies in one - third of patients with sarcoidosis . sarcoidosis has a chronic - progressive course in 30 % of cases , whereas 4090 % of patients , depending on the series , show spontaneous regression . 
in 15 % of cases , cardiorespiratory complications may lead to death , whereas a subtle and non - specic onset , associated with different possible localisations , often underlies the failure in obtaining an early diagnosis [ 17 ]  . radiol med ( 2014 ) 119 : 6474 in the early stages of disease , the diagnosis requires biopsy , whereas diagnostic imaging and in particular chest radiography ( cxr ) and computed tomography ( ct ) can provide highly suggestive , though not pathognomonic , ndings and represent a crucial tool for staging the disease , planning treatment and predicting the prognosis [ 8 , 9 ]  . numerous retrospective studies since 1990s have dened the role of cxr , ct , high - resolution ct ( hrct ) and magnetic resonance ( mr ) imaging in chest sarcoidosis and in the assessment of extrathoracic lesions [ 10 , 11 ]  . 
in recent years , the potential of diagnostic imaging in the study of this disease has expanded with the 18uorodeoxyglucose positron - emission introduction of tomography / ct ( 18fdg - pet / ct )  . 
some authors have proposed 18fdg - pet / ct for the differential diagnosis of solid lesions of the chest and for evaluating inammation and response to corticosteroids in patients with sarcoidosis [ 4 , 14 ]  . the published studies about thoracic and systemic sarcoidosis are retrospective and conducted on small series and heterogeneous groups of patients without precise inclusion criteria [ 13 , 1522 ] , and the usefulness of wholebody 18fdg - pet / ct in the diagnosis and follow - up of patients with thoracic and systemic sarcoidosis has not yet been completely dened . 
multidetector ct ( mdct ) is currently the standard of reference for the diagnosis and follow - up of this disease , but no comparative study with 18fdg - pet / ct for the restaging and follow - up of sarcoidosis has been conducted to date . the aim of this study was to evaluate , through a retrospective study of a rigorously selected and homogeneous clinical series , the role of 18fdg - pet / ct in restaging and follow - up of patients with histologically proven sarcoidosis . 
the results obtained with 18fdg - pet / ct were compared with those of mdct in the management of patients with thoracic and systemic sarcoidosis . materials and methods we carried out a retrospective evaluation of 39 patients with histologically conrmed sarcoidosis referred to us for clinical and radiological assessment for suspected relapse or disease follow - up over a period of 49 months ( from september 2006 to march 2010 )  . 
from the initial group of 39 patients , 21 patients were selected who met the following inclusion criteria : histologically proven diagnosis of sarcoidosis ; stage ii and iii sarcoidosis ; 18fdg - pet / ct performed for restaging and follow - up of sarcoidosis ; time interval between mdct and 18fdg - pet / ct not exceeding 40 days . the group of 21 patients included 16 women and ve men aged 2680 years ( mean 57.28 years ) who had , at the time of 18fdg - pet / ct , histological evidence of non - caseating granuloma ( sarcoid ) on a biopsy obtained from at least one lesion site ( table 1 )  . 
all cases were assessed for clinical course [ symptoms , serum angiotensin - converting enzyme ( ace ) , kveim reaction ] and morphological imaging ndings ( cxr , ct and mri ) useful for the follow - up of sarcoidosis . 
at the time of the 18fdg - pet / ct study , all patients had given their consent for their demographic , clinical and diagnostic data to be used in clinical research . 
all patients had suspended all forms of therapy at least 30 days before both mdct and 18fdgpet / ct . ct technique ct studies were performed with a 16 - slice mdct scanner ( tsx - 101 , aquilion 16 , toshiba medical system , tokyo , japan ) , using the following acquisition parameters : slice thickness 1 mm , pitch 1.75 , table feed 0.6 mm , gantry rotation time 0.5 s , kv / mas 120 / 250 . 
all patients were administered 1.5 cc / kg contrast medium through an antecubital vein at a ow rate of 3.55 cc / s , with postcontrast acquisitions starting 60 s after injection . the beginning of 18fdg - pet / ct technique pet - ct images were acquired with a combined pet - ct scanner ( ge , discovery lsa ) incorporating a pet scanner ( advance nxi ) and a 16 - slice ct system ( light speed plus )  . 
prior to the administration of uorine - 18 - fdg , all patients , who had fasted for at least 8 h , underwent capillary glucose sampling ( \160 mg / ml ) and , to avoid artefacts due to muscle activity , they were instructed not to do any physical activity prior to the scan . image acquisition was started approximately 50 min after the intravenous injection of 37 mbq / 10 kg of 18fdg . during this time all patients were instructed to drink at least 500 ml of water and to void their bladders as needed . table 1 characteristics of patients considered patient sex age symptoms other imaging studies biopsy site radiol med ( 2014 ) 119 : 6474 history tumour treatment for sarcoidosis ( cortisone ) ( years ) respiratory respiratory , evening fever , night sweats and weight loss anorexia , vomiting , slight evening fever anorexia , vomiting magnetic resonance imaging of brain : multiple lesions in both cerebral hemispheres and hypophyseal pedicle ultrasound of neck and abdomen : bilateral latero - cervical and retroperitoneal lymphadenopathies , advanced chronic liver disease , splenomegaly normal 67 ga - scintigraphy scan 18fdg pet / ct with pathological uptake at liver hilum , celiacmesenteric , para - aortic and inguinal regions bilaterally , hilar - mediastinal , right latero - cervical , left retroclavicular , right diaphragmatic pillar and right subphrenic peritoneal and pelvic regions mediastinal lymph node latero - cervical lymph node bone latero - cervical lymph node latero - cervical lymph node latero - cervical lymph node mediastinal lymph node liver latero - cervical lymph node mediastinal lymph node lung node lung lung mediastinal lymph node lung inguinal lymph node mediastinal lymph node lung mediastinal lymph node lung respiratory whole - body 67 ga scintigraphy : axillary lymph tracer uptake in the lungs and hilarperihilar and mediastinal region respiratory respiratory radiol med ( 2014 ) 119 : 6474 no muscle relaxants were administered . 
the low - dose ct ( ldct ) acquisition parameters : 340 ma ( auto ) , 120 kv ; slice thickness , 3.75 mm ; gantry rotation time , 0.8 ms ; eld of view ( fov ) collimation , 50 cct images were reconstructed with ltered backprojection . 
pet acquisition was obtained in the caudo - cranial direction , via three - dimensional interactive technique reconstruction . acquisition with before injecting the fdg , patients to take their medical histories , view previous diagnostic examinations and to provide information about the examination procedure ( informed consent )  . the physicians met image analysis all images obtained with the two modalities ( mdct and 18fdg - pet / ct ) were evaluated independently by two mixed groups of radiologists and nuclear medicine specialists with similar levels of experience ; the readers in the two groups were not aware of the patients clinical history , but only of the diagnostic suspicion . 
in case of doubt , the 18fdg - pet / ct images were reviewed by consensus reading . mdct images were assessed for the presence , distribution and predominance of radiological evidence of sarcoidosis in all body regions [ 6 ]  . 18fdg - pet / ct images were visualised in the three orthogonal planes , as pet images , ct images and fusion images . 
pet / ct images , used for the detection of lesion site and type and for tracer uptake ( focal vs diffuse ) , were evaluated both separately and as fusion images . moreover , as a quantitative index of 18fdg uptake , we determined the body - weighted standard uptake value ( suvbw ) , expressed in g / ml , using commercial software that calculates it as the ratio between 18fdg ( mbq / ml ) in a region of interest ( drawn on the attenuation - corrected images ) and the administered activity ( mbq ) per body weight ( kg )  . data analysis for all patients without signs of relapse or progression of disease , the longest available follow - up , always greater than 12 months , was taken as the reference standard . 
patients were considered false positive if , despite being positive on imaging , they did not show signs of relapse during the follow - up . patients were considered true negative if they had negative imaging results conrmed by an absence of relapse on follow - up . 
false - negative patients had clinical evidence of disease relapse or progression at follow - up , but negative results on imaging . statistical analysis sensitivity , specicity and accuracy of both pet / ct and mdct were evaluated in relation to the follow - up , taken as the standard of reference . 
the results of the comparison between mdct and 18fdg - pet / ct with follow - up are given in table 2 , which provides the sensitivity , specicity and accuracy both for the entire group of 21 patients and for the subgroup of 16 patients who underwent whole - body mdct . 
the disease most commonly occurs between the ages of 20 and 50 years , and the incidence is slightly higher in women than in men [ 6 ]  . the clinical presentation is highly variable and nonspecic , and instrumental diagnosis , consisting of standard blood chemistry tests ( including ace ) , cxr and chest ct does not permit a denitive diagnosis . radiol med ( 2014 ) 119 : 6474 fig . 
1 whole - body 18fdgpet / ct ( 18uorodeoxyglucose positron - emission tomography / computed tomography ) maximum intensity projection ( mip ) ( a ) and pet / ct coronal fusion image ( b ) , multidetector ct ( mdct ) ( c ) and pet / ct fusion image of the neck ( c , d ) , chest ( e , f ) and abdomen ( g , h ) trans - axial sections of a patient with systemic sarcoidosis diagnosed by biopsy of the latero - cervical lymph nodes . 
both techniques revealed multiple lesions of the supraclavicular and thoracic lymph nodes , lungs , abdominal lymph nodes , liver and spleen ct is the most commonly used technique , and to date the standard of reference ; in routine clinical practice the examination is limited to the chest without whole - body imaging . 
when positive , the results of diagnostic imaging are fundamental for choosing the biopsy site and evaluating disease extent . in the past , lung and whole - body 67 ga scintigraphy has been used to identify thoracic sarcoidosis , including cardiac localisations , and lesions in other body regions [ 21 ]  . 
metabolic imaging has also been proposed for distinguishing active lesions from the nal stage of irreversible brosis . 18fdg - pet / ct has recently been proposed for differentiating solid lesions of the chest seen on ct into malignant and benign based on the 18fdg metabolism [ 24 ]  . 
the possibility of identifying active sites of sarcoidosis is based on the capability of 18fdg to accumulate within the sarcoid granuloma characterised by the presence of a rich inltrate of lymphocytes and macrophages [ 25 , 26 ]  . 
all selected patients had stage ii and table 3 comparison of pet / ct and mdct by lesion site iii sarcoidosis , in which active lesions are present but there is no end - stage irreversible brosis . unlike previous reported series , the population included in our study was a selected and homogeneous group of patients , all undergoing follow - up and with a histological diagnosis of sarcoidosis . 
our study evaluated the possibility of detecting sites of sarcoid lesions with 18fdg - pet / ct and compared the data with mdct , which is normally performed as the examination of reference in the standard management of these patients . 
in particular , in patients with sarcoidosis mdct can reveal enlarged lymph nodes and pulmonary inltrates with predominantly perihilar distribution , even though in cases of negative mdct ndings for thoracic or mediastinal lesions there was histopathological evidence of disease on transbronchial biopsy samples [ 11 ]  . 
it should also be noted that , despite its panoramic capabilities , mdct is very often used for regional imaging of the chest , which explains the smaller number of extrathoracic localisations detected . 18fdg - pet / ct is a whole - body examination , which always allows the exploration of the entire body including the brain , with the possibility of detecting all sites of disease and affected organs [ 27 ]  . 
its use has been proposed not only for staging but also for identifying occult sites of disease to be sampled for histological examination [ 28 ]  . ours was a retrospective study that considered the standard clinical use of two imaging modalitiesthe more commonly used mdct with 18fdg - pet / ct performed as a complementary examinationto evaluate their current role in the restaging and follow - up of sarcoidosis . 
the two modalities revealed lymph nodes in the superior mediastinuwhole - body pet / ct also showed 18fdg uptake in the supraclavicular , axillary and abdominal lymph nodes and in the spleen . 
pet / ct revealed a greater extent of disease whole - body imaging techniques are difcult to organise in the context of diagnostic imaging with ionising radiation . while allowing a rigorous comparison by site of disease , they do not reect real clinical practice . in our study , one patient with negative whole - body mdct was found to be positive on 18fdg - pet / ct and showed disease relapse during the follow - up ( true positive )  . 
nine patients with positive mdct ndings showed a greater number of lesion sites on 18fdg - pet / ct ; eight of these nine patients had disease relapse at follow - up ( true positive )  . 
mdct depicts the morphological changes of active or acute inammation and end - stage brosis , whereas 18fdg - pet / ct describes only the inammation of the active stage , and the patients included in our study were in stage ii or iii . frequent the mdct follow - up studies in patients with pulmonary sarcoidosis demonstrated that nodular opacities are the most ( 80100 % ) and potentially reversible lesions , whereas cystic airspaces and architectural distortion are usually irreversible regardless of treatment [ 30 32 ]  . 
findings of ground - glass and linear opacities are considered both reversible and irreversible [ 30 , 31 , 33 , 34 ]  . 18fdg - pet / ct showed 17 thoracic localisations compared to the 23 detected by mdct , with moderate concordance for neck lymph nodes and fair concordance for mediastinal , hilar and pulmonary nodes , whereas there was no concordance for bony lesions of the cervico - thoracic region ( table 3 )  . parenchymal pulmonary lesions were detected with a fair level of concordance between the two techniques ( one out of six patients was false positive at 18fdg - pet / ct , two out of eight patients were false positive at mdct )  . in sarcoidosis , asymptomatic involvement of the liver and spleen occurs in respectively 4080 and 3877 % of patients , but organ - related symptoms are rare ( 26 % ) [ 6 ]  . in our study , there was no concordance between the two modalities for liver localisations , and poor concordance for splenic lesions . 
the literature reports that ct scans of the abdomen in addition to the chest are used to assess intraabdominal extent of disease and response to therapy . abdominal lymphadenopathy is the most frequent nding in 76 % of cases , the most common sites being the portal vein ( 86 % ) , the para - aortic region ( 77 % ) and the coeliac axis ( 59 % )  . 
although the morphological and dimensional criteria ( greater / less than 1 cm ) for dening positive nodal status at ct have often been questioned , our study found the level of concordance with 18fdg - pet / ct to be moderate for cervical nodes , fair for mediastinal nodes , and poor for lymph nodes at other sites . in our series , 18fdg - pet / ct revealed 26 abdominal localisations compared to the nine detected by mdct , with poor concordance between the two examinations ( table 3 )  . radiol med ( 2014 ) 119 : 6474 fig . 
both modalities depicted localisations of disease in the pulmonary hilar lymph nodes , liver and splenic hilum radiol med ( 2014 ) 119 : 6474 however , it should be noted that this observation is limited by the fact that only 16 out of 21 patients had a ct scan extending to the abdomen and pelvis . the literature reports that 18fdg - pet / ct can be useful in some patients with bone , neurological and cardiac involvement [ 35 ]  . 
bone lesions were detected at 18fdgpet / ct alone in patients who were found to be true positive at follow - up . brauns study [ 5 ] as well reported that 18fdg - pet / ct proved to be particularly useful in describing site of extrathoracic involvement . 
in another cohort of 20 patients with biopsy - proven sarcoidosis , 18fdg - pet / ct had a sensitivity of 87 % and was useful for the evaluation of response to therapy in patients treated with corticosteroids [ 5 ]  . moreover , sarcoid lesions may coexist with sites of malignancy in 413 % of cancer patients , and it important to bear in mind that the presence of sarcoid lesions showing 18fdg uptake may cause problems in interpreting 18fdg - pet / ct studies obtained for cancer staging and restaging [ 36 ]  . 18fdg uptake by sarcoid lesions is not specic and may mimic other pathological processes , including lymphomas and diffuse metastatic disease [ 37 ]  . 
the use of the suvbw is still being debated ; in that no specic guidelines exist that provide a cut - off value for differentiating benign from malignant lesions [ 38 ]  . 
in the three patients in our study who had a diagnosis of both sarcoidosis and malignant disease ( endometrial carcinoma , biliary carcinoma ) , histological examination of the surgical specimen conrmed that the lesions affecting the cervical , mediastinal and abdominal lymph nodes and the spleen were indeed due to sarcoidosis . non - invasive overall evaluation of disease activity by means of whole - body 18fdg - pet / ct may prove to be increasingly important in helping to choose the best site for the biopsy [ 5 , 17 , 19 , 29 ]  . in 18fdg - pet / ct , irradiation depends on the dose administered and not on the body section being imaged , while in mdct the scans are performed on the body segments suspected of harbouring disease , so as to limit the dose of ionising radiation [ 39 ]  . 
in 18fdg - pet / ct , however , the dose delivered by ldct performed for attenuation correction and suv determination must be added to the radiation dose resulting from the radio - pharmaceutical . the possibility of using 18fdg - pet / ct combined with is an contrast - enhanced ct for diagnostic purposes example of excellent synergy in the eld of diagnostic imaging , which requires a pet scanner combined with shows , pet / ct 8 / 16 - slice ct . 
as our experience combined with mdct is not yet a clinical reality in the follow - up of patients with sarcoidosis , but recent studies have demonstrated the advantages of multimodal imaging for the diagnosis of severe neoplastic diseases , which are difcult to dene [ 28 , 40 , 41 ]  . moreover , techniques are being developed to lower the dose delivered by ct while obtaining all the possible diagnostic information in a single examination [ 42 ]  . therefore , further clinical studies are needed to establish the most effective diagnostic strategy in this eld . the role of 18fdg - pet / ct in the follow - up of patients with sarcoidosis is currently still being dened , but the literature supports its value as an important aid for clinicians [ 37 ]  . 
of particular interest is its use to avoid repeated mdct studies of the abdomen and pelvis in patients with thoracic sarcoidosis , considering that it detects active and reversible lesions in all body regions [ 43 ]  . however , thanks to the growing availability of pet / ct scanners and recognition of its usefulness in depicting occult disease and identifying sites amenable to biopsy , and 18fdg - pet / ct demonstrating appears to be very promising for the functional evaluation of sarcoidosis . response therapy , some limitations to our study need to be acknowledged . the case series included only 21 patients ; however , they were rigorously selected based on the histological diagnosis and active stage of disease , and no larger series with such selection criteria have been published in the literature . histological conrmation was obtained on a single site and not on all localisations identied with the two diagnostic modalities , but this was in part due to the fact that it is not requested for either initiating treatment . the diagnosis or conclusions whole - body 18fdg - pet / ct depicts a larger number of disease localisations compared with mdct , in part as a result of the fact that the latter is often limited to the single body sections only . 
combined pet / ct facilitates the localisation of hypermetabolic areas and anatomical improves the interpretation of the morphological lesions depicted by mdct , allowing an accurate assessment of disease extent . 
therefore , even though not necessary for the diagnosis , 18fdg - pet / ct could be used in the future to complement other , more traditional modalities for assessing the course of stage ii and iii sarcoidosis and for guiding patient management . 
integration of 18fdg - pet / ct and mdct into a single examination , even though more complex to organise , deserves greater attention in clinic research and further studies are required to evaluate its impact on the management of patients with sarcoidosis . radiol med ( 2014 ) 119 : 6474 conict of interest g rubini , s cappabianca , c . 
zuiani institute of diagnostic radiology , university of udine , p.le santa maria della misericordia 15 , 33100 udine , italy e - mail : clauser.p@hotmail.it provide valuable information for the preoperative evaluation of lesions . keywords breast cancer ( cid : 2 ) breast ultrasound ( cid : 2 ) breast mri 3 - dimensional ultrasonography ( cid : 2 ) introduction ultrasound ( 2d - us ) in breast imaging proved to be an accurate , available , noninvasive and inexpensive one which is frequently used in the study of breast disease . 
it can be combined with mammography especially in women with dense breasts , in the differential diagnosis of palpable lesions or in presence of equivocal mammographic ndings [ 1 , 2 ]  . 
however , it is an operator - dependent examination and its quality is strongly related to the doctors expertise and knowledge , with limited possibilities for standardisation [ 1 ]  . when a space - occupying lesion is identied on ultrasound , its volume can be estimated using the three orthogonal diameters [ antero - posterior ( ap ) , latero - lateral ( ll ) and cranio - caudal ( cc ) ] and applying the formula for calculating the volume of a sphere ; however , this may be only an approximation when the lesion has irregular morphology . in the last few years , 3d ultrasound ( 3d - us ) has been increasingly used in clinical practice , also in breast imaging [ 3 , 4 ]  . 
images can be archived and then visualised and reviewed at a later date . the possibility of saving a series of images of the lesion , rather than a single image , makes the examination easier to radiol med ( 2014 ) 119 : 240248 review and less operator - dependent . 
currently , the bulkiness of 3d probes with square or circular arrays makes their use difcult in everyday clinical practice : 2d - us is still irreplaceable for the identication of suspicious lesions . magnetic resonance imaging ( mri ) of the breast is a very good technique for the detection and staging of disease prior to surgery in women with breast cancer [ 6 ]  . 
in these nine women , the biopsy was performed because of suspicious ndings on mri . images obtained with a 3d probe were collected for 26 lesions ( 72.0 % ) before biopsy and for 10 lesions ( 28.0 % ) when the patient came for positioning of the needle - wire , about 1 month after biopsy . 
histology revealed 28 invasive ductal carcinomas ( idc ) ( 9 grade i , 15 grade ii and 4 grade iii , one of which with a widespread intraductal component ) , one high - grade ductal carcinoma in situ ( dcis ) , two intermediate grade dcis with a lobular component , two grade - ii invasive lobular carcinomas ( ilc ) , two mucinous carcinomas ( one grade i and the other grade ii ) , and one papillary carcinoma . 
these ndings were conrmed by analysis of the surgical specimen ( 23 quadrantectomies and 13 mastectomies )  . imaging evaluation ultrasound all patients underwent 2d - us , performed by a resident following specic training in breast imaging and by a radiologist experienced in breast imaging , with the aim of locating and characterising lesions , and measuring the three diameters ( antero - posterior , latero - lateral and cranio - caudal )  . 
then , before the biopsy or while positioning the wire , the resident acquired the volumetric images on the same ultrasound unit using a 616 mhz 3d4d rsp squarearray probe , which automatically scans the area of interest . 
this probe is able to obtain 3d images on an area with a maximum diameter of 4.0 cm ; lesions larger than 4.0 cm cannot be correctly assessed . breast magnetic resonance imaging magnetic resonance imaging was performed on a 1.5 - t system ( magnetom avanto , siemens medical system , erlangen , germany ) using a dedicated bilateral multichannel coil . 
patients were studied in prone position . axial t1 - weighted images were obtained with a 3d flash sequence with the following parameters : tr / te , 9 / 4.7 ms ; ip angle , 25 ( cid : 3 ) ; matrix , 512 9 512 ; eld of view , 340 9 340 mm ; slice thickness , 2 mm ; acquisition time , 80 s . 
of averages , 1 ; oversampling , 7 ; acquisition time , 239 s . volume measurement with 3d - us volumes were calculated at the end of the session by the same resident who performed the 3d4d acquisition . specic software was used ( vocal , virtual organ computer - aided analysis , 4d view ; ge healthcare , kretztechnik , zipf , austria )  . 
of the three planes available for image display [ axial ( a ) , sagittal , ( b ) , and coronal ( c ) ] , we selected plane a to trace the lesion margins . 
the same trainee radiologist who measured the volumes with 3d - us traced the lesion borders in each axial plane , using the rst acquisition of subtracted post - contrast images . volume evaluation based on the three diameters on the images acquired with breast mri , the cranio - caudal , latero - lateral and anteroposterior diameters of each lesion were measured , and the mean diameter was calculated . 
the same test was then used to identify a signicant difference in volumes evaluated with imaging and at histopathologic examination . concordance was evaluated between the volumes calculated by : 3d - us and 2d - us ; 3d - us and mri and between those three imaging modalities and histology using the interclass correlation coefcient ( icc )  . 
the gure is visualised in three planes ; the axial and longitudinal planes can also be obtained with a 2d probe , while the third plane is a reconstruction in the coronal plane . after the operator traces the borders of the lesion , dedicated software ( vocal , virtual organ computer - aided diagnosis ) calculates the volume and represents it with a surface rendering modality ( b ) radiol med ( 2014 ) 119 : 240248 results the maximum diameters of the lesions considered are described in table 1 , in terms of range , mean and standard deviation . 
concordance between imaging and histology was also good , with 0.79 for 3d - us , 0.82 for 2d - us and 0.79 for mri , respectively . lesions with a volume \1 cm3 were slightly overestimated by 3d - us ( 16 / 20 cases ) , while 12 of 16 lesions with a volume c1 cm3 were underestimated . 
image processing performed by a single operator to calculate volumes took 24 min , depending on dimensions and morphological features of the area . discussion 2d - us is an easy and useful approach , which is irreplaceable in recognising and characterising breast lesions . once identied , the lesion can be studied with a 3d probe and the area of interest can be acquired and stored with a volumetric acquisition that includes the lesion and a small portion of surrounding tissues . 
this can be achieved with a liner - array probe that scans the area of interest , with or without systems to localise ( tracked freehand systems or untracked freehand systems ) , obtaining 2d - images from which volumetric images are reconstructed [ 4 ]  . as an alternative , one can use a probe with a square or circular 2d - matrix ( two - dimensional arrays ) that is kept still while it automatically scans the area of interest to give 3d real - time information [ 4 ]  . 
the images acquired can be presented with surface rendering ( showing the acquired volume with 3d appearance ) , multiplanar reformatting ( showing the three perpendicular planes , with the possibility to move within the slices acquired ) or volume rendering [ 4 ]  . 
several studies comparing the sensitivity , specicity , predictive values and accuracy of 3d - us with those 2d imaging in the differential diagnosis of breast masses showed that 3dus does not improve diagnostic accuracy [ 14 ]  . 
cho [ 14 ] found a high level of concordance between different operators in identifying a lesion as benign or malignant using 3d probes , and concluded that this technique could improve diagnostic condence and reproducibility . 
d volume is calculated on breast mr with dedicated software ( vitrea 2 - vital images , plymouth , mn , usa ) , after drawing the area of the lesions in all the slices . 
histology of the lesion after surgery conrmed the dimensions identied by 3d - us and breast mr imaging than one study underlined the usefulness of the coronal plane ( c ) , which is perpendicular to the two planes usually visualised on 2d ultrasound . 
the mathematical estimation of volume has also lower intraand inter - operator reproducibility . many authors have shown that reproducibility in volume measurement is better when using a volumetric probe , with an inter - operator concordance of almost 100 % , example , in the study of thyroid or focal liver lesions [ 17 , 19 ]  . 
the use of ultrasound with 2d probes has also been proposed for measuring renal volume in healthy subjects and in patients with impaired renal function : the accuracy , radiol med ( 2014 ) 119 : 240248 fig . 
6 graph showing the results of blandaltman analysis applied in the comparison of the volumes measured with 3d ultrasound and histology reproducibility and correlation with other techniques such as computed tomography were interesting [ 15 , 16 ]  . the limits of measuring the three diameters are particularly evident for masses or organs with irregular margins and morphology [ 17 , 18 ] , which is a typical aspect of malignant breast lesions [ 11 ]  . acquiring 3d images requires only a few seconds ( 36 s ) , and overall the examination is extended by no more than 1 min , necessary to activate the probe and identify the lesion . 
this operation entails a short learning curve : the operator has to become familiar with a slightly different image representation from that of the 2d probe . the volume measurement can be performed at the end of the session after the acquisition , by a different operator and by more than one operator , as can the morphological evaluation of the lesion and surrounding tissues . 
volume measurement requires a maximum of 4 min , especially in lesions with a greater diameter and undened margins . the vocal software used in our study has already been reported to have good accuracy in the volumetric measurement of irregular lesions , especially when margins are traced manually and not automatically [ 5 ]  . 
its reliability improves with the number of planes used to describe the the same time margins of the area of interest , but at increases the time needed for the analysis . 
 [ 20 ] as well as our own experience , we decided to use a 30 ( cid : 3 ) angle , which appears to be a good compromise , as it is simple , with no signicant differences with respect to measurements obtained at 6 ( cid : 3 ) , 9 ( cid : 3 ) or 15 ( cid : 3 ) , but at the same time less time - consuming . 246 radiol med ( 2014 ) 119 : 240248 it has already been underlined that mri can be superior in describing lesion characteristics and extension : for this reason , we decided to compare also the volumes obtained with this technique [ 7 , 8 , 21 ] , even though our standard of reference has been histology of the specimen . in the literature , we have found only one article [ 22 ] comparing the volumes of benign and malignant breast lesions measured with 2d - us , 3d - us and mammography , and the authors reported a good correlation . we are not aware of studies that evaluated the correspondence of 2d - us , 3d - us , mri and histology for malignant breast lesions . 
c , d in this case the volume calculated with the three methods was surgery ( 2dcomparable to that obtained by histology after us = 1.2 cm3 ; breast mr = 0.87 cm3 ; histology = 0.9 cm3 ) 3d - us = 1.05 cm3 ; radiol med ( 2014 ) 119 : 240248 histology comparable to that of mri , which is considered the standard of reference among imaging modalities for a correct evaluation of lesion extension . 
 [ 7 ] , 2d - ultrasound underestimated tumour diameter during the follow - up of patients treated with neoadjuvant chemotherapy , while mri showed a better performance with a slight tendency to overestimation . however , the particular situation and hence the modications related to chemotherapy could probably explain the limited ability of us in identifying post - therapy changes , especially compared to mri , which is able to visualise contrast - enhancement only where there is vascularisation . the 95 % limits of agreement calculated with blandaltman analysis between imaging and histology overlapped for all modalities , proving that 3d - us is at least comparable to other imaging techniques in evaluating the volume of malignant breast lesions . in the literature , other possible applications of 3d - us can be found . 
for example , its use in interventional procedures : 3d images allow a better evaluation of needle position , thus improving the accuracy of tissue sampling and reducing the number of cores necessary [ 24 , 25 ]  . in addition , the possibility of using cad ( computeraided diagnosis ) on volumetric images acquired with 3dus has already been evaluated , with the aim of improving sensitivity and specicity in the identication of lesions , especially those classied as bi - rads 3 [ 26 ]  . conclusions on the basis of our initial experience , 3d ultrasound appears to be a reliable and easy - to - use method which is at least as accurate as 2d ultrasound and mri in measuring volumes of malignant breast lesions . 
 [ 3 ] reported that in men the mean age at diagnosis was signicantly higher , the size was signicantly smaller and fnh showed more often atypical than those in women . 
furthermore , was not studies have demonstrated that detection of the typical imaging features of fnh is often heavily dependent on lesion size , being less frequent in lesions smaller than therefore , undertook this study in an 3 cm [ 57 ]  . 
we , attempt to clarify whether radiologists should expect any gender differences in the imaging ndings of fnh detected in men or women . radiol med ( 2014 ) 119 : 222230 materials and methods patient population and imaging techniques institutional review board approval was obtained and full informed consent was waived for this retrospective study . our study complied with the terms of the declaration of helsinki [ 8 ]  . we searched our hospitals medical records ( radiology , pathology , surgical pathology and discharge summary ) to identify patients with fnh treated during a 6 - year period ( from january 2006 to december 2011 )  . 
patients were eligible for enrolment on the basis of the following inclusion criteria : ( 1 ) a conclusive diagnosis of fnh ( see reference standard ) ; ( 2 ) they had undergone at least one of the following imaging studies : ( a ) baseline and contrastenhanced ultrasound ( ceus ) scan ; ( b ) multiphase multidetector computed tomography ( mdct ) scan ; ( c ) magnetic resonance imaging ( mri ) with hepatocellular - specic contrast agent . 
patients were excluded from the analysis if the imaging protocol was suboptimal or if the images could not be retrieved from our imaging archives . computed tomography ct studies were performed with a 64 - slice mdct scanner ( brilliance 64 , philips medical systems , eindhoven , the netherlands )  . 
to determine the scanning delay for the hepatic arterial phase , the time - topeak aortic enhancement was assessed using an automatic bolus - tracking technique with automated scan - triggering software ( bolus pro ultra , philips medical systems , eindhoven , the netherlands )  . 
a triphasic dynamic contrast - enhanced study was obtained after the administration of an iv bolus of 0.1 mmol / kg of gadobenate dimeglumine ( multihance , bracco , italy ) into an antecubital vein at a ow rate of 2 ml / s through a 20 - gauge intravenous catheter by means of a power injector ( mr spectris ; medrad , pittsburgh , pa , usa ) and ushed by 20 ml of sterile saline solution . 
images were acquired using an automated bolus - detection technique ( smartprep technique , ge healthcare ) during the arterial ( 14 s after bolus injection ) , hepatic venous and delayed phase ( 60 and 180 s after bolus injection , respectively )  . the dynamic study was followed by a hepatocellular - specic phase obtained 2 h after the injection of contrast material , with the same scanning parameters . contrast - enhanced ultrasound two experienced radiologists ( more than 5 years of ceus of the liver ) , who were aware of the patients clinical histories , performed us scanning using either an hdi 5000 ( atl , bothell , wash , usa ) or an iu22 unit ( philips ultrasound , bothell , wash , usa ) , both of them equipped with c5 - 2 / c5 - 1 convex - array probes and pulse inversion imaging software . 
the us contrast agent used in the present study was sonovue ( bracco , milan , italy ) , which was injected intravenously as a 2.4 ml bolus followed by 10 ml of normal sterile saline ush using a 20or 22 - gauge peripheral intravenous cannula . 
in patients with multiple lesions , a 2.4 ml further bolus of sonovue was administered for each lesion , with an interval time at least of 15 min to allow for clearance of the previously injected contrast . digital cineloops were recorded during both baseline and postcontrast us in the arterial , hepatic venous and extended hepatic venous or late phase ( 540 s , 5590 s and injection , up to 200300 s from the beginning of 224 radiol med ( 2014 ) 119 : 222230 respectively )  . 
all images and cineloops were digitally stored as raw data in a pc - based workstation connected to the us units via a standard ethernet link and sent to our pacs ( impax , agfa - gevaert , milan , italy )  . image analysis two abdominal radiologists ( more than 10 years of experience ) randomly reviewed all imaging studies by consensus . 
neither of the readers was involved in the scanning and both were blinded to the nal diagnosis , as well as to the identity , clinical histories and other imaging ndings of the patients . 
five consecutive interpretation sessions , with a seven - day interval to prevent recall bias , were held to complete the review process . on each imaging modality , the two readers were asked to report on the size and segment location of each lesion according to the couinaud classication system and to visually assess echogenicity / attenuation / signal intensity ( the latter in all mri sequences ) in comparison with adjacent liver parenchyma on both the unenhanced and the contrast - enhanced images obtained during the arterial , hepatic venous and delayed ( or extended hepatic venous for ceus ) phases . 
for us and ceus studies , the colour doppler images and spectral waveforms were also evaluated for each lesion , as were the following parameters [ 911 ] : central scar : a central or eccentric hypoor hyperechoic area at baseline us and / or unhenancing at ceus in the arterial and hepatic venous and extended hepatic venous phase , also showing distinctly different attenuation / intensity on unenhanced scans or at different phases of enhancement . feeding vessel : an arterial vessel , appreciable at baseline cd / pd and / or at ceus in the arterial phase , branching from the hepatic arterial tree and directed towards the lesion and penetrating it ; spoke - wheel sign : a radial arterial vascularity within the lesion appreciable at baseline colour and power doppler and / or centrifugal enhancement of the lesion with a central vessel branching from the centre towards the periphery at ceus in the arterial phase . presence and type ( arterial or venous ) of any intralesional ow , other than the above signs , at baseline colour and power doppler examination . reference standard the nal diagnosis was established by core biopsy performed with an 18 - g needle ( n = 1 ) or by demonstrating that fnh was isoor hyperintense to the surrounding liver in the hepatobiliary phase of mri ( n = 81 )  . 
for the remaining 29 lesions , a combination of size stability during a follow - up period of at least 1 year and imaging features consistent with fnh was used . the ceus diagnostic criteria for fnh were based on arterial phase centrifugal lling and stellate vascularity , followed by sustained contrast enhancement on the hepatic venous phase and extended hepatic venous or late phase [ 10 ]  . 
the ct diagnostic criteria were : mild hypoattenuation or isoattenuation on precontrast scan ; rapid , homogeneous and strong enhancement in the arterial phase except for the central scar ; near isoattenuation to liver parenchyma in the hepatic venous and delayed phases . 
to assess the statistical signicance of the difference between two genders with respect to us , colour doppler , ceus , mdct and mri patterns and with respect to the presence and appearance of the central scar , the z test for proportions or the fischer exact test were used , as appropriate . 
statistical signicance was considered to be present at a p value of \0.05. results overall , 195 complete imaging studies pertaining to 111 fnhs ( size range 0.59.2 cm , mean 3 1.8 cm ) in 91 patients were retrieved ( table 1 )  . 
b during the arterial phase a markedly hypervascular lesion ( arrow ) is evident in segment viii showing a tiny hypoattenuating central area corresponding to the central scar ( arrowhead )  . 
seventy - three ( 65.8 % ) lesions were located in the right liver and the remaining 38 ( 33.2 % ) in the left liver . computed tomography eleven out of the 17 ( 64.7 % ) fnhs studied by means of mdct were slightly hypoattenuating , whereas 4 / 17 226 radiol med ( 2014 ) 119 : 222230 table 2 multidetector ct pattern of 17 focal nodular hyperplasia ( fnh ) lesions no . 
in the delayed phase , these four lesions were either isoattenuating ( n = 3 ) or hyperattenuating ( n = 1 )  . a central scar was depicted on mdct images as an unenhancing hypoattenuating central area in 7 / 15 ( 46.7 % ) fnhs occuring in women and in one of the two ( 50 % ) fnhs in men . 
a unenhanced mr shows a 3.5 - cm isointense ( arrow ) lesion in segment vi which shows a small central scar that is hypointense with respect to the surrounding liver parenchyma on t1 - weighted imaging ( arrowhead )  . 
further multicentric studies sampling a larger population may be warranted to elucidate this issue . in our series , no statistically signicant differences between men and women were found on unenhanced images from us , mdct and mri . after contrast agent injection , our ndings conrm the previously reported strong arterial enhancement on dynamic contrast - enhanced images followed by sustained enhancement , without any statistically signicant difference among imaging modalities [ 5 , 7 , 10 , 13 ]  . 
interestingly , in that study the two men with fnh without central stellate area on mr images had small lesions ( 25 and 30 mm in diameter , respectively ) , with no central brous area on gross examination of the surgical specimen . several studies have demonstrated that the detection of typical imaging features of fnh is often strongly , heavily dependent on lesion size , being less frequent in lesions smaller than 3 cm [ 57 ]  . 
consequently , considering our series , it might be hypothesised that the difference found in that study may be , at least in part , more closely related to the different lesion size reported in the two different groups of male and female patients than to real pathological differences . 
did not use gadolinium chelate with hepatocellular - specic properties , so the hepatobiliary phase could not be exploited and , eventually , the seven male patients with fnhs lacking at least one typical nding on mri underwent surgery . 
it is noteworthy that all the fnhs studied in our serieswhether in men or womenshowed uptake of hepatocellular - specic contrast agent , demonstrating the hepatocellular nature of lesions and , in the proper clinical setting , their substantial benignity . 
hence , our data also support the hypothesis made by other researchers that exploiting the properties of the newer hepatocellular - specic mr contrast agents enables us to depict the morphological and functional characteristics of fnh noninvasively and may aid in the differential diagnosis of these lesions , thus reducing the need for biopsy and even surgery [ 1315 ]  . this retrospective study has some important limitations . first , we had a selection bias . 
consequently , those with fnh lesions lacking the characteristic imaging ndings may have been missed . nevertheless , if atypical appearance of fnh is a feature mainly observed in men we should have observed a dramatic reduction of typical fnhs found in men in comparison with women , but this was not the case . 
however , all lesions were well characterised at ceus , multiphase contrast - enhanced ct and / or mri on the basis of the typical enhancement patterns , which we considered to be established diagnostic criteria , as done in other studies [ 14 ]  . 
in one patient selective renal arteriography was negative probably because the bleeding observed at ct angiography was self - limited . twenty - one embolisation procedures were performed in 20 patients ; one patient required a second embolisation 3 h after the rst one . 
no statistically signicant differences in egfr or renal function stage appeared after rae . conclusions percutaneous treatment can be proposed as a injuries , rst - line treatment resulting in a safe and effective procedure . in iatrogenic renal arterial keywords transarterial embolization ( cid : 2 ) iatrogenic renal vascular injuries ( cid : 2 ) emergency embolization introduction the kidney is the most common injured genitourinary and abdominal organ . 
advances in imaging and treatment strategies over the past 20 years 262 radiol med ( 2014 ) 119 : 261268 have decreased the need for surgical increased renal preservation . intervention and iatrogenic renal artery injuries are usually reported after renal artery angioplasty or stenting , and have an incidence of 1.6 % [ 2 ]  . 
in addition , as nephron - sparing surgery ( nss ) has recently become the procedure of choice to treat localised renal tumours in selected patients , complications are more frequent , affecting mainly the renal vascular and collecting system [ 4 , 5 ]  . 
furthermore , although relatively uncommon , iatrogenic renovascular injuries have increased due to the increasing number of interventional procedures . possible radiological ndings in iatrogenic vascular lesions are arteriovenous stulae , pseudoaneurysms , arterial dissection , or contrast extravasation . 
traditional therapy for acute iatrogenic rupture of the main renal artery has been renal artery ligation followed by bypass grafting or nephrectomy , but nowadays , approaches conservative or minimally invasive increasingly favoured over surgery , including selective transarterial embolisation ( tae ) and the placement of stents / stent grafts . tae is a well - established nonsurgical endovascular treatment for iatrogenic renal arterial injuries , with many advantages , such as rapid recovery , short hospital stay and early resumption of physical activities [ 1 ]  . 
the aim of our study was to review our experience and long - term followup in the treatment of iatrogenic renal vascular injuries using transcatheter embolisation . materials and methods patients the medical les and imaging data of all patients who renal arterial embolisation ( rae ) between underwent january 2006 and july 2012 in two centres with established interventional retrospectively radiology service were reviewed . 
indications for diagnostic angiography and endovascular treatment included : signs and symptoms suggestive of vascular injury , ( such as haemodynamic instability necessitating blood transfusion , non - resolving haematuria in a haemodynamically stable patient , and non - remitting ank pain ) , suspicious laboratory ndings ( decrease in haematocrit or haemoglobin levels ) ; uncontrolled intraoperative blood loss ; imaging evidence of vascular injury ( pseudoaneurysm formation , active extravasation of contrast medium , creation of arteriovenous stula , etc . ) ( table 1 )  . 
haemodynamically stable patient means stabilisation of blood pressure ( bp ) and haematocrit level , further decrease of haemoglobin value by no more than 1.5 g / dl , and haemodynamic stabilisation without the need for blood transfusion . 
moreover , rae was implemented only when renal bleeding was not controlled by conservative measures , such as nephrostomy tube clamping , adequate hydration , and correction of coagulation disorders , or in any case of severe bleeding leading to haemodynamic instability . written informed consent was obtained from all patients except those deemed non - competent who were in hypovolaemic shock . baseline imaging computed tomography ( ct ) angiography ( aquilion 64 , toshiba , japan ) ( 16 - siemens , erlangen , germany ) was performed with a baseline non - contrast acquisition and an arterial contrast phase following the administration of 120 ml of 320 mgi / ml iodinated contrast medium ( visipaque 320 , ge healthcare , usa ) at an injection rate of 4 ml / s , immediately followed by 40 ml of normal saline solution at the same injection rate , using a double head automatic injector ( stellant d , medrad , usa )  . 
optimal arterial enhancement was achieved using the bolus - tracking technique , with a region of interest ( roi ) placed on the abdominal aorta ( at level ) with an enhancement threshold 100 hu higher than the baseline arterial density . 
when clinical conditions permitted , a delayed enhancement phase was acquired 5 min after contrast medium administration . on ct angiography , haemorrhage was dened as an active extravasation of contrast media , pseudoaneurysm as a round or ovoid cavity communicating with a ruptured vessel wall , arteriovenous stula as an early or simultaneous opacication of one or more intraparenchymal arteries and veins during the arterial phase , and arteriocalyceal stula as the presence of contrast medium in a calyceal group during the arterial phase . the suprarenal procedure all endovascular procedures were performed by an interventional radiologist . 
1 selective left renal arteriography shows a psedoaneurysm ( psa ) in a patient with a percutaneous nephrostomy ( a ) ; the angiogram performed at the end of the embolisation procedure ( carried out with microcoils ) revealed complete exclusion of the psa the procedure was performed in the angiography suite ( bv 300 allura xper fd20 ; philips and axiom artis siemens ) under local anaesthesia and continuous cardiovascular and respiratory monitoring . 
before treatment each patient received an intravenous dose of 5 % mannitol , 3 ml / kg / min of dopamine plus 600 mg of intravenous n - acetylcysteine as a protection against the ischaemia - related production of free radicals and contrast medium - induced renal damage . 
shortterm antibiotic prophylaxis with a rst - generation cephalosporin ( cefazolin 2 gr b.i.d. ) was initiated at the beginning of each endovascular procedure . in all patients , from a common femoral approach , a unilateral renal angiography was initially performed , using a 5f pig - tail catheter , followed by selective renal digital subtraction angiography of the affected side using a selective cobra - type or sim - 1 catheter . 
the interval between completion of the intervention and rst imaging follow - up was in the range of 3 days2 months . a minimum 6 - month follow - up was available for all of our patients who underwent rae . 
values of egfr ( estimated glomerular ltration rate ) were assessed and classied according to the national kidney foundation scale [ 7 ]  . in each patient , the egfr before injury was compared with the egfr after rae . 
the last egfr measurement reported in the patients medical records within the following 6 months after rae was selected as a reference , to avoid interference with other variables such as hypotension and contrast agent - induced nephrotoxicity after renal bleeding and embolisation . 
patients without a follow - up egfr measurement within 6 months after rae were excluded from the analysis of renal function because a decrease in egfr observed beyond that period could be associated with other factors . 
individual changes in egfr and renal function stage before renal artery injury and after rae were evaluated by the student t test . outcomes the technical success , clinical success and complications were independently evaluated . 
clinical success after rae was dened as the absence of clinical or imaging evidence of further bleeding as determined by the resolution of haematuria , retroperitoneal bleeding , and hypotension after rae , in 24 h and within 1 week after the fig . 
2 selective right renal arteriography shows early opacication of draining veins ( white arrow ) during the arterial phase due to postnephrostomy iatrogenic arteriovenous stula ( a ) ; an 8 mm amplatzer plug inside the delivery catheter ( b ) ; performed at arteriovenous stula ( c ) the angiogram the end of the procedure revealed closure of the radiol med ( 2014 ) 119 : 261268 in the absence of endovascular procedure . follow - up imaging , bleeding cessation was dened as stabilisation of blood pressure ( bp ) and haematocrit level , further decrease of haemoglobin value by no more than 1.5 g / dl , and haemodynamic stabilisation without the need for blood transfusion . 
all complications were recoraccording interventional radiology classication [ 8 ]  . the society classied results renal injuries complicating biopsy ( n = 4 ) , percutaneous eswl ( n = 4 ) , nephron - sparing surgery ( n = 4 ) , guidewire - induced arterial perforation during coronary angiography or renal stenting ( n = 3 ) , percutaneous nephrostomy renal endopyelotomy / pyeloplasty ( n = 2 ) and ( n = 3 ) , surgical nephrectomy ( n = 1 ) , were all causes of iatrogenic vascular lesions necessitating endovascular treatment . 
the procedures involved 20 native kidneys and one renal allograall patients presented with haemoglobin / haematocrit drop , which was associated with persistent macroscopic haematuria in 16 ( 76.2 % ) and ank pain in 11 patients ( 524 % )  . 
in the case of severe renal failure ( n = 3 ) , colour doppler visualisation of a pseudoaneurysm in the site of previous renal biopsy in association with laboratory data and clinical signs , were considered sufcient to justify a digital subtraction angiography ( dsa ) examination . diagnostic renal angiography revealed nine actively bleeding vessels , six pseudoaneurysms , four arteriovenous stulas and one arteriocalyceal stula . 
in all cases the injuries were intraparenchymal . twenty - one embolisation procedures were performed in 20 patients ; one patient required a second embolisation 3 h after the rst rae for persistent pain and evidence of persistent bleeding at ct scan . the technical success rate was 100 % , as shown by the complete exclusion of bleeding demonstrated with angiography performed at the end of the procedure . 
one patient who was referred late to the interventional radiology unit required massive after percutaneous biopsy , renal transfusions , died 48 h later in the intensive care unit due to disseminated intravascular coagulation . 
during this period , no recurrence of bleeding or complications related to rae were observed . overall , endovascular treatment was well tolerated , even though minor complications such as vasovagal reactions or temporary spasm of a catheterised artery were not registered . the long - term effects of rae on renal function could not be reliably assessed in all of our patients ; because in four cases the follow - up egfr assessment was done after more than 1 year following rae and this measurement could be affected by other causes . 
in available patients , no statistically signicant differences in egfr or renal function stage appeared after rae . discussion as the number of interventional procedures in modern clinical practice increases , so does the number of iatrogenic renovascular injuries , which have become the most common ( [ 50 % ) cause of renal vascular lesions [ 4 , 5 ]  . 
the present study was performed to evaluate the immediate radiological and clinical success and the long - term followup of transcatheter embolisation of iatrogenic renal vasis worth noting that during the early cular injuries . 
it postoperative period after partial nephrectomy , major haemorrhage is the most common complication , with a reported incidence between 0 and 5.26 % [ 3 , 9 , 10 ]  . in a retrospective series of 21 iatrogenic renovascular lesions resulting from surgical ( nephron - sparing surgery ) , minimally invasive surgical or percutaneous procedures we found that rae is a safe and effective treatment for either the prevention or treatment of renal haemorrhage . 
in a patient presenting with gross haematuria or acute ank pain 266 radiol med ( 2014 ) 119 : 261268 after invasive and non - invasive renal procedures , examinations such as contrast - enhanced ct , colour doppler sonography , or magnetic resonance angiography should be performed . 
the advantage of ct is that it enables imaging of the entire urinary tract [ 10 ]  . most vascular injuries are minor with spontaneous healing in the majority of patients , so conservative management is preferred . 
in the event of massive bleeding , renal haemorrhage persisting for more than 72 h , or progressively deteriorating renal function , surgical or percutaneous treatment of vascular lesions has been recommended [ 11 , 12 ]  . the alternative treatment method to percutaneous embolisation is emergent nephrectomy or clamping of the renal artery which results in kidney loss [ 1 , 5 ]  . 
previous studies have also shown that embolisation of iatrogenic renal arterial injuries is a safe , tissuepreserving treatment method for renovascular injuries , associated with high technical and clinical success rates , using various agents for embolisation [ 1316 ]  . 
 [ 16 ] reported a similar series ( 15 patients with the same iatrogenic lesions and causes ) treated with superselective embolisation using coils or n - butyl cyanoacrylate ( nbca ) iodised oil mixture or pva particles or nbca iodised oil mixture when the lesion could not be superselectively catheterised . 
as in our series , embolisation was performed as superselectively as possible ; when possible , we preferred coils or plug to limit as much as possible non - target embolisation and we usually use pva particles and ncba iodised oil mixture only in superselective embolisation , even though reported experiences [ 1316 ] have not described non - target embolisation . 
furthermore , in agreement with our results , percutaneous embolotherapy had a high success rate and a low complication rate ( i.e. , major parenchymal infarction ) [ 17 ] in the management of iatrogenic haemorrhage in cases of vascular injuries of renal allografts . considering that the choice of embolisation material is important for efcient treatment of vascular injuries , the material should be chosen according to the site , size and the ow pattern of the vessels to be occluded , material availability , and the experience of the interventionalist . percutaneous angiography with selective coil embolisation is the initial treatment of choice in renal arterial haemorrhage [ 18 ]  . 
superselective embolisation as distally as possible is mandatory , at least at the level of the interlobar arteries , to keep parenchymal loss to a minimuthis can usually be achieved using microcatheters and microcoils as embolic agents [ 13 ]  . 
the main disadvantage of coil embolisation is that usually more than one coil is required for adequate occlusion , which increases the cost and time of the procedure [ 5 ]  . 
one arteriovenous stula ( avf ) in our series was embolised using a single amplatzer vascular plug iv of 8 mm in diameter ( aga medical corporation , usa ) , delivered through a 5f catheter successfully placed immediately proximal to the site of interest . 
in this case , the avf occlusion was immediate and safe and the total cost may be comparable to the combined cost of several coils . control of the polyvinyl alcohol particles ( pva ) during injection is difcult , and inadvertent embolisation may occur [ 5 ]  . 
even when more than one feeding artery needs to be occluded ( e.g. , in the case of multiple bleeding sites or pseudoaneurysms or multiple arteries contributing to the bleeding site ) , only minor renal parenchymal loss post embolisation is still possible . 
additional renal arterial trauma , inadvertent or nonselective embolisation of the main renal artery or occlusion of non - target sites may lead to postembolisation functional syndrome , systemic hypertension , and renal impairment as the most frequent possible complications . these complications have not been noted in recent reports using superselective embolisation [ 5 , 14 , 2123 ]  . 
we did not encounter any of these complications in our series . no long - term renal function impairment was found in our patients , which is also indicative of the limited renal parenchymal loss after embolisation . 
as reported in the literature [ 14 ] , patients who present with iatrogenic renal vascular trauma often manifest other comorbidities , such as diabetes or pre - existing hypertension and renal disease , which are known to be associated with worsening renal function . 
finally , we have to consider that the initial vascular trauma even though deemed renal sparing , may nonetheless radiol med ( 2014 ) 119 : 261268 be responsible for some loss of renal tissue . 
in the literature , a transient elevation of the serum creatinine level during the days following the procedure is described , but this may reect the larger amount of contrast material used in some more complex procedures [ 10 ]  . potential limitations and difculties associated with this technique are impaired renal function , vascular anatomical difculties , or stenosis of the main renal artery [ 5 , 14 ]  . bleeding from a segmental artery is rare ; however , when this more proximal artery is occluded , keeping major parenchymal loss to a minimum may be a probleif renal function before embolisation was not impaired , more extensive parenchymal loss is still a preferred solution over total nephrectomy [ 5 , 14 ]  . limitations of the present study are the small number of patients and the lack of comparison with a cohort of patients treated surgically . 
because of the rarity of this type of lesions , it is unlikely that a prospective randomised trial with a high number of patients will be conducted to compare the percutaneous and open approaches . in conclusion , perirenal haemorrhage , intrarenal bleeding with pseudoaneurysm formation or the occurrence of an arteriocalyceal stula are all serious iatrogenic renovascular complications requiring prompt diagnosis and treatment . 
giannitrapani department of clinical medicine and emerging pathologies , university of palermo , via del vespro 127 , 90147 palermo , italy resonance imaging , during the unenhanced phase , hepatic arterial phase and venous phase were recorded . 
no statistically signicant difference in venous enhancement was found among the mrecist groups . conclusions mrecist showed a more favourable response compared to recist 1.1 in patients with unresectable hcc receiving sorafenib . keywords liver ( cid : 2 ) ct ( cid : 2 ) mr ( cid : 2 ) hcc ( cid : 2 ) sorafenib introduction hepatocellular carcinoma ( hcc ) is a major health problem worldwide and the main cause of death among cirrhotic patients [ 1 ]  . 
the introduction of this new therapy has led to search for new radiological endpoints / biomarkers able to measure and predict tumour response to treatment [ 3 , 511 ]  . response evaluation criteria in solid tumours ( recist ) are typically used to assess response to cytotoxic therapy . 216 radiol med ( 2014 ) 119 : 215221 however , these criteria may not adequately reect tumour response to sorafenib , because changes in tumour vascularity and necrosis may occur without major changes in tumour size [ 6 , 8 , 1115 ]  . 
therefore , modied recist ( mrecist ) have been developed which differ from recist in that the target lesion measured is not the whole lesion but only the viable tumour , dened as the contrast - enhanced portion of the tumour on hepatic arterial phase images [ 9 , 12 , 16 , 17 ]  . we hypothesised that the anti - angiogenic effect of sorafenib could be measured on contrast - enhanced computed tomography ( ct ) and magnetic resonance ( mr ) imaging as changes in tumour enhancement . 
therefore , the purpose of our study was to compare tumour response according to recist and mrecist and to describe changes in hcc enhancement before and after sorafenib treatment . patients and methods study population review board approval was obtained , with a waiver for informed patient consent . through a computerised search of our gastroenterology department database from december 2007 to january identied 40 patients who 2010 , a study coordinator received anti - angiogenic treatment with sorafenib ( nexavar , bayer healthcare , germany ) in a standard dose of 800 mg daily for unresectable hcc . 
these patients were deemed inoperable or untransplantable either because tumour burden exceeded the united network of organ sharing ( unos ) or university of california sans francisco ( ucsf ) criteria or because of comorbidities . 
patients with previous locoregional treatment ( n = 15 ) and patients without available baseline or follow - up contrast - enhanced ct / mr imaging studies ( n = 4 ) were excluded . 
there were 12 men ( mean age 68 years ; range 5879 years ) and ve women ( mean age 73 years ; range 6778 years ) with an overall mean age of 69 years ( range 5879 years )  . 
the underlying cause of cirrhosis was hepatitis c in 11 ( 64 % ) patients , hepatitis b in three ( 18 % ) in three ( 18 % ) patients and ethanol patients . 
seven ( 41 % ) patients had one measurable lesion and 10 ( 59 % ) patients had multiple measurable lesions . the study coordinator noted the following clinical data for each patient : alphafetoprotein level , performance status , child - pugh class , barcelona clinic liver cancer ( bclc ) stage , treatment starting date and duration , previous vascular surgery and association with other vascular hepatic diseases . imaging studies baseline examinations were performed at a median of 30 days ( range 2836 days ) before the start of treatment . thirteen ( 76 % ) patients had one follow - up imaging study available , two ( 12 % ) patients had two follow - up imaging studies available , and two ( 12 % ) patients had three followup imaging studies available . 
the baseline examination was performed with either ct ( n = 10 ) or mr imaging ( n = 7 )  . computed tomography ct imaging was performed using a 64 - section scanner ( philips brilliance , royal philips electronics , eindhoven , the netherlands )  . 
the following ct parameters were used : detector conguration , 64 9 0.625 mm ; peak , 120 kvp ; scan time , 4 s ; mas , 250300 ; section thickness , 3 mm ; no section overlap . 
the contrast medium was administered with a mechanical power injector ( invision ct , medrad ) at a rate of 35 ml / s through an 18to 20 - gauge intravenous catheter inserted into an arm vein , followed by a ush of 25 ml of saline administered at the same injection rate . automatic bolus - tracking techniques with automated scantriggering software ( bolus pro ultra , philips medical systems ) were used . 
hepatic arterial phase and venous phase scanning were started automatically 18 and 58 s , respectively , after the trigger threshold ( 150 hu ) was reached at the level of the suprarenal abdominal aorta . 
the delayed phase was started 180 s after the start of contrast material injection . mr imaging mr imaging was performed using a 1.5 - t scanner ( signa excite hdxt , general electric , healthcare , milwaukee , wi , usa )  . 
contrast administration consisted of 0.1 mmol / kg body weight of gadobenate dimeglumine ( multihance ; bracco imaging , milan , italy ) in six patients or 0.025 mmol / kg of gadoxetate disodium ( primovist , bayer , berlin , germany ) in one patient , injected at 12 ml / s through a 20 - gauge intravenous catheter with a power injector ( spectris ; medrad , pittsburgh , pa , usa ) , followed by 20 - ml saline ush at the same rate . 
if a patient had multiple follow - up ct or mr imaging studies , the latest was considered for analysis . diagnosis of hcc was made using a combination of imaging and laboratory criteria ( i.e. , size [ 1 cm ; enhancement during the hepatic arterial phase and washout during hepatic venous and / or delayed phase ; interval growth ; mild hyperintensity on t2 - weighted imaging ; signal loss on out - ofphase imaging due to the presence of lipids ; tumour invasion of the portal vein ; elevated alphafetoprotein ) [ 1 ]  . 
when multiple hcc lesions were noted at baseline ct or mr examinations , a maximum of two target lesions were selected for further analysis ; a target lesion was selected if the following conditions were satised : ( a ) the lesion could be accurately measured in at least one dimension ; ( b ) it was suitable for repeat measurement ; ( c ) it showed intratumoural arterial enhancement on contrast - enhanced ct or mr imaging . 
the roi values of lesion attenuation measured on the ct images or the signal intensity values measured on the mr images during the unenhanced , hepatic arterial and venous phase were recorded . 
enhancement values during the hepatic arterial phase and venous phase were calculated for each lesion as : hepatic arterial phase enhancement = [ ( attenuation / signal intensity during hepatic arterial intensity during unenhanced phase attenuation / signal unenhanced phase ) / attenuation / signal phase ] 9 100 ; venous phase enhancement = [ ( attenuation / signal intensity during venous phase attenuation / signal intensity during unenhanced phase ) / attenuation / signal intensity during unenhanced phase ] 9 100 . 
no patient had been treated with transjugular intrahepatic portosystemic shunt or surgical spleno - renal shunt . recist vs mrecist response was slightly different depending on whether recist or mrecist was used . 
according to recist , two of 17 ( 12 % ) patients showed partial response , ten of 17 ( 59 % ) patients showed stable disease and ve of 17 ( 29 % ) showed progression disease . 
according to mrecist , three of 17 ( 18 % ) patients showed partial response , ten of 17 ( 59 % ) patients showed stable disease and four of 17 ( 23 % ) patients showed progression disease . 
similarly , patients with partial response had a greater decrease in venous phase enhancement than did those with stable disease or progressive disease , but the differences were not statistically signicant . 
four patiens had tumor invasion of the portal vein and one patient had bland portal vein thrombosis . discussion in this study , we compared recist and mrecist in assessing response in 17 patients with unresectable hccs treated with sorafenib . 
since mrecist measures only the viable ( i.e. , the enhancing ) portion of the tumour , as opposed to recist 1.1 , which measures the whole tumour regardless of the enhancing components , the results of our study are not surprising , because sorafenib acts as a cytostatic drug causing a reduction in tumour vascularity rather than in tumour size . 
those authors compared recist and mrecist in 70 patients with unresectable hccs treated with sorafenib and found a good agreement between the two methods ( pearsons coefcient r = 0.818 ) , whereas ten of 70 patients ( 18 % ) 219 radiol med ( 2014 ) 119 : 215221 fig . 
1 transverse unenhanced ( a , d ) and contrast - enhanced fatsuppressed three - dimensional gradient - echo images acquired in the hepatic arterial phase ( b , e ) and venous phase ( c , f ) in a 61 - year - old man with hepatitis c virus ( hcv ) - related cirrhosis and multiple hepatocellular carcinomas . 
a target lesion in liver segment iv is shown before ( ac ) and 180 days after anti - angiogenic treatment ( de )  . thick lines indicate mrecist evaluation ( b , e )  . 
this case represents an example of discordance between mrecist and recist criteria and demonstrates that arterial enhancement variation after sorafenib is a useful marker of therapy response who had stable disease according to recist had partial response according to mrecist [ 9 ]  . 
in our study , no patient showed complete response according to either recist and mrecist , possibly as a result of the relatively small size of our study population . the second purpose of our study was to describe changes in hcc enhancement before and after sorafenib treatment . 
in our series , patients with partial response had a statistically signicant decrease in hepatic arterial phase enhancement at followup in comparison to patients with stable disease and progressive disease . 
our results are , however , preliminary and should be analysed with caution because the low number of subjects included in this study prevents any denitive conclusion . we also compared venous phase enhancement among the mrecist groups . 
 [ 16 , 17 ] reported that changes in tumour vascularity were the most specic indicators of treatment response in patients with gastrointestinal stromal tumours ( gist ) on imatinib and proposed new criteria based on evaluation of either tumour size or tumour attenuation after contrast enhancement . 
these and our results suggest that a different method for measuring hcc response after cytostatic therapy , taking into account the changes in enhancement and not only the size of the viable tumour portion , should be incorporated into clinical practice . 
however , this procedure is more time consuming in comparison to recist and mrecist , because three rois within each target lesion need to be recorded on nonenhanced and postcontrast images and compared at baseline and follow - up . 
furthermore , roi placement can be more prone to bias than a single tumour dimension measurement . some authors have reported the potential of perfusion ct and mr imaging examinations as an emerging tool for response to anti - angiogenic the evaluation of tumour fig . 
however , long delivered by ct , breathing and cardiac motion , postprocessing time required to obtain perfusion parameters [ 19 ] and measurement variability are all limitations to the dissemination of this technique . 
one additional means for monitoring the effects of targeted therapy agents on hcc with mr imaging is diffusion - weighted imaging , whose potential , however , has still to be further investigated [ 8 ]  . there are several limitations to our study . 
moreover , contrast media were administered at different rates for ct ( 35 ml / s ) and mr ( 12 ml / s ) imaging , and different mr contrast agents with different doses of gadolinium were also administered . 
fifth , the clinical importance of these ndings is limited owing to the small study population , and further prospective studies would require a more systematic design and a precise timing to evaluate response to treatment using mrecist criteria on the basis of ct or mr changes in tumour density or intensity , respectively . in conclusion , our preliminary results suggest that , in comparison to recist 1.1 , mrecist may show a more favourable treatment response in patients with unresectable hccs treated with sorafenib . 
ulivieri francesco sardanelli received : 28 july 2012 / accepted : 20 february 2013 / published online : 3 december 2013 ( cid : 2 ) italian society of medical radiology 2013 abstract purpose our aim was to estimate the in vivo reproducibility of bone mineral density ( bmd ) at dual - energy x - ray absorptiometry ( dxa ) and to compare fast array , array , and high - denition scan modes . materials and methods a total of 378 patients ( 38 males and 340 females ; mean age 63 9 years ) underwent dxa using a qdr - discovery a densitometer ( hologic )  . 
considering the three scan modes on lumbar spine and right femur , six independent groups of 30 patients were examined twice ( for a total of 180 patients )  . 
the remaining 198 patients underwent three scans of the lumbar spine ( n = 92 ) or of the right femur ( n = 106 ) , one for each scan mode . 
bandirali facolta` di medicina e chirurgia , scuola di specializzazione in radiodiagnostica , universita` degli studi di milano , via festa del perdono 7 , 20122 milan , italy l . 
as a consequence , although the absolute reduction in time and radiation dose is relatively low , when bmd measurement is the aim of dxa , fast array can be generally preferred . keywords dual - energy x - ray absorptiometry ( cid : 2 ) bone mineral density ( cid : 2 ) scan modes ( cid : 2 ) reproducibility osteoporosis is the most common metabolic bone disorder , characterised by low bone mass and microarchitectural deterioration , which leads to diminished biomechanical competence of the skeleton , with a subsequent increase in bone fragility and susceptibility to low - trauma or atraumatic fracture . 
such fractures can occur in any site but are most common in the spine , wrist and hip , and all regions of the skeleton with a high percentage of trabecular bone . osteoporosis is asymptomatic and not clinically manifested until a patient suffers a fracture [ 1 ]  . 258 radiol med ( 2014 ) 119 : 257260 dual - energy x - ray absorptiometry ( dxa ) is recognised as the reference method to measure bone mineral density ( bmd ) accurately and reproducibly , capable of detecting bone mineral loss at an early stage [ 2 ]  . 
moreover , the world health organization ( who ) has established dxa as the best densitometric technique for estimating bmd in postmenopausal women and based the denitions of osteopenia and osteoporosis on dxa results [ 3 ]  . hologic qdr - discovery a , like other densitometers , allows for various scan modalities , i.e. 
however , to the best of our knowledge , a comparison among the three scan modes has never been performed on patients with known or suspected osteoporosis undergoing dxa in clinical practice . since small differences in magnitude of bmd may change the diagnosis and since patient monitoring is based on the capability of detecting such small differences , there is a rationale for estimating the reproducibility of these three scan modes and assessing possible differences among them . our aim was to estimate the in vivo reproducibility of bmd measurements obtained using dxa and to compare the three scan modes of the hologic qdr - discovery a densitometer . each of the three scan modes , without repositioning . 
finally , the percent |dbmd| was obtained . all examinations were performed using a qdr - discovery a densitometer ( hologic , rome , italy ) and processed by a technician with 3 years experience with dxa . scan times were recorded and radiation doses were estimated using the weighting factors issued by the icrp60 [ 6 ]  . results the mean bmd of right femur and lumbar spine obtained with the three scan modes on the six independent subgroups is shown in table 1 . 
however , all |dbmd| were lower than the best sdd , while percent |dbmd| was lower than all lscs except for the lsc of the femur obtained with the fast array scan mode . materials and methods discussion this study was approved by the local ethics committee . patient consent was obtained for using the results of dxa scans for scientic purposes . 
a total of 378 patients ( 38 males and 340 females ; mean age 63 9 years ) underwent a dxa examination for known or suspected osteoporosis . considering the combination of the three scan modes and two anatomical sites ( lumbar spine and right femur ) , six independent subgroups of 30 patients were considered , for a total of 180 patients who repeated the scans twice without repositioning . 
these data were used to estimate intra - scan mode bmd reproducibility . reproducibility was expressed in terms of least signicant change ( lsc ) and smallest detectable difference ( sdd )  . 
in particular , lsc was estimated using the method outlined in the ofcial paper issued by the international society of clinical densitometry [ 4 ] , while sdd was estimated using the blandaltman method [ 5 ]  . 
for sdd calculation , we did the following : with reference to the difference of the two compared datasets , we calculated the coefcient of repeatability as 1.96 multiplied by the standard deviation . the remaining 198 patients underwent one scan of the lumbar spine ( n = 92 ) or of the right femur ( n = 106 ) for the who has established dxa as the best densitometric technique for measuring bmd in postmenopausal women , and has consequently based the denitions of osteopenia and osteoporosis on dxa results [ 7 ]  . 
there is a large body of evidence on osteoporosis that led to the publication of the international society for clinical densitometry 2007 adult and pediatric ofcial positions [ 2 ]  . 
a summary of the advantages of dxa over other densitometric techniques may be found in the review by blake and fogelman [ 8 ]  . most dxa densitometers provide the operator with different scan modes , which differ from each other in terms of spatial resolution , scan time , and patient radiation exposure . 
the densitometer installed at our institution is produced by one of the manufacturers ( hologic ) ofcially accepted by the frax model for fracture risk assessment . regarding the choice of the appropriate scan mode , each manufacturer / model has its own policy . 
for example , our densitometer is set up to always propose the fast array mode and the operator is allowed to change it based on a subjective evaluation of the patients anthropometric characteristics . 
however , as it is well known , it is not feasible to obtain the true patients bmd value in clinical practice . considering that in clinical practice very small bmd differences may result in a different who diagnosis , our study was aimed to assess whether a difference does exist among the three scan modes of our densitometer . besides accuracy there is reproducibility , which is important for the patient follow - up . 
in clinical practice , the most common situation is the comparison of two bmd measurements of a given individual obtained at different times using the same instrument . when a second measurement is performed on a patient , the clinician needs to identify a true change in bmd and , in this regard , only changes greater than the lsc can be ascribed to treatment effects or worsening of the disease . smaller changes may be due to the measurement error . 
in this scenario , the precision of the measurement is more important than accuracy . in the present study , we obtained a very high intra - scan mode reproducibility for all of the three scan modes . 
5.3 % for the values recommended by the iscd , lumbar spine and 5.0 % for the total hip [ 2 ]  . apart from the methodology proposed by the iscd , we also calculated the sdd using the blandaltman method . 
moreover , it has been demonstrated that , to express variability on a percentage basis using the coefcient of variation leads to underestimated variability in patients with low bmd and to overestimated variability in patients with high bmd [ 10 ]  . 260 radiol med ( 2014 ) 119 : 257260 the comparison among the three scan modes highlighted a substantial homogeneity of data . 
moreover , this result holds for both the spine and the femur . the above considerations on precision and bmd comparisons should be integrated with comments on scan time and radiation dose . 
regarding the scan time , we should note that , once the scan mode is chosen , the moving speed of the x - ray tube / detector system is constant in time , i.e. 
even though both scan time and radiation exposure are very low for each scan mode when compared with other x - ray or magnetic resonance examination , the fast array mode has the lowest radiation dose and is the fastest one . from this study , we may conclude that , in clinical practice , the fast array scan mode may be preferred over the other two scan modes . 
however , this general conclusion may be reviewed for particular patients ( such as obese patients or those with a marked arthritis ) , in which the clinicians may decide to use a more reliable scan mode like hd . 
cova received : 24 april 2012 / accepted : 23 january 2013 / published online : 12 december 2013 ( cid : 2 ) italian society of medical radiology 2013 abstract purpose this study was undertaken to compare the different acquisition protocols available in a last - generation multislice computed tomography scanner used for cardiovascular studies , with particular attention to dosimetric aspects . materials and methods our study compared prospective and retrospective electrocardiographic - gating techniques for cardiac imaging . 
for each patient , we performed in vivo dose measurements , using gafchromic lwe compared the effective dose values estimated from the experimental measurements and the dose data reported on the ct console . 
image quality was also assessed . results prospective acquisition allows for major dose savings compared to retrospective acquisition ( mean effective dose , 4.5 msv with prospective acquisition versus 27.5 msv with retrospective acquisition )  . 
fisica sanitaria , ospedale maggiore , azienda ospedalierouniversitaria ospedali riuniti di trieste , strada di fiume 447 , trieste , italy keywords multislice computed tomography ( cid : 2 ) ct coronary angiography ( cid : 2 ) radiation dose ( cid : 2 ) gafcromich lm introduction coronary angiography with multislice computed tomogrpahy ( msct - ca ) is one of the most important innovations in medical diagnostics of the past 10 years [ 1 ]  . since its introduction into clinical practice in 1998 , diagnostic imaging of the heart and coronary arteries has constituted one the most attractive applications of msct [ 2 , 3 ]  . 
despite the major epidemiologic and health economics ischemic heart disease [ 4 ] , intrinsic limitations signicantly hindered the noninvasive study of the coronary tree for several decades , with cardiac and coronary imaging being almost exclusively left to selective coronary angiography , a procedure burdened by non - negligible rates of mortality and morbidity [ 57 ]  . implications of the high spatial and temporal resolution achieved especially by 16 - , 32 - , 40and 64 - detector - row ct scanners and the possibility of obtaining adequate cardiac synchronization have allowed at least some of the limitations to be overcome , leading to a revolution in the management of patients with coronary heart disease [ 8 , 9 ]  . 
the numerous clinical studies published in recent years have widely demonstrated that msct has achieved high levels of diagnostic accuracy , both in the assessment of coronary stenosis and for the follow - up of the patency of aortocoronary bypass grafts [ 1017 ]  . the main pitfalls of msct are related to limitations in resolution . 
as a result , as emphasized by achenbach in the key to obtaining an increasingly accurate 2004 , 250 radiol med ( 2014 ) 119 : 249256 table 1 characteristics of the patients and clinical indications table 2 scanning and reconstruction parameters ; contrast medium clinical indications thoracic aorta evaluation known or suggested coronaropathy evaluation of left atrium and pulmonary veins stable or unstable angina patients with surgical indications asymptomatic patients with multiple risk factors previous bypass planned ptca previous stent placement ptca percutaneous transluminal coronary angioplasty 10 ( 22 ) 8 ( 18 ) 7 ( 16 ) 6 ( 14 ) 6 ( 14 ) 4 ( 9 ) 1 ( 2 ) 1 ( 2 ) 1 ( 2 ) diagnostic performance is to increase the techniques spatial and temporal resolution [ 18 ]  . the rapid technological advances of msct have indeed increased the diagnostic accuracy of noninvasive coronary imaging , improving image quality in terms of both spatial and temporal resolution . the increasingly widespread use of msct - ca has highlighted the need for controlling the radiation dose delivered to the patient in the course of these imaging procedures . 
ever since the early years of msct - ca , the development of the modality has been inuenced by the issue of radiation dose [ 19 , 20 ] , with dose being one of its major problems . 
in the absence of contraindications , sublingual nitrate was administered ( 0.61.2 mg of nitroglycerin , natispray , teofarma srl , salimbene , italy ) a few minutes before the scan . materials and methods scan protocols between november 2010 and may 2011 , we enrolled a total of 41 patients ( 29 men and 12 women , mean age 63 years , age range 3489 years ) who underwent msctca with a 256 - slice ct scanner ( brillance ict , philips healthcare , eindhoven ; the netherlands )  . for some patients ( n = 16 ) , when requested by the referring physician , we obtained a pre - contrast scan for the quantication of coronary calciuthe amount of calcium at the level of the coronary artery walls was assessed using the agatston protocol for calcium scoring . radiol med ( 2014 ) 119 : 249256 during the post - contrast phase , a high - concentration iodinated contrast agent ( iomeprol 400 mgi / ml , iomeron 400 , bracco , italy ) was administered through an 18 - gauge needle cannula into an antecubital vein of the right arm ; the contrast agent was injected at a ow rate of 46 ml / s , for a total volume ( tv ) calculated with the following formula : tv flow ( cid : 3 ) scan delay scan time 10 cc differences in ow rate were dependent on the availability of a viable peripheral access . 
administration of the contrast agent was followed by a 40 ml bolus of saline injected at the same rate , using a dual - head stellant automatic injector ( medrad , indianola , usa )  . the scan was synchronized with the contrast bolus by using a proprietary bolus tracking protocol , which involves drawing a region of interest ( roi ) over the ascending aorta and setting a threshold enhancement value of 100 hu above baseline . 
examinations were acquired with prospective triggering ( with axial scans generally centered at 78 % of the rr interval ) or retrospective gating ( based on a helical scan with retrospective reconstruction of images obtained during the same cardiac phase ) , depending on the clinical needs and the patients heart rate after the betablocker . 
the scan parameters are summarized in table 2 . dose evaluations in addition to recording the ct dose index ( ctdi ) and dose - length product ( dlp ) at the console , in vivo dose measurements were obtained for each patient using special self - developing lm , commercially known as gafchromic xr - qa , which becomes progressively darker during exposure . the lm , cut into 1 - cm - wide strips and protected by a plastic sheet to avoid contact with the skin , was placed and left on the patients throughout the examination , at the level of the sternum , along the right and left middle axillary line and in the interscapular space . 
the strips placed on the chest had a length of * 24 cm , and the others were of 10 cm . the lm is calibrated to provide the dose as a function of the degree of lm darkening obtained by acquiring an image with a scanner . 
to calculate the desper , the dlp value was calculated as the product of the experimental dose indicator ( dsin ) multiplied by the scan range . results of the 41 patients initially enrolled in the study , ve were excluded owing to technical problems related both to the lm reading system and to failures of the software generating the ct dose report . 
the population nally eligible for the study therefore comprised 36 patients ( 24 men and 12 women )  . on the basis of each patients diagnostic needs and physique , the examinations were carried out using ve different acquisition protocols : as shown in table 3 , 42 % ( 15 / 36 ) of patients were imaged with the prospective pro ( prospective alone or prospective with calcium tocol score ) , 50 % ( 18 / 36 ) with the retrospective protocol ( also divided into retrospective alone or retrospective with calcium score ) , mainly reserved for patients with elevated heart rate ( [ 75 bpm ) or frequent extrasystoles or when imaging of the entire chest was required ( indications for heart surgery or follow - up of internal mammary artery bypass grafts )  . 
a small minority of patients ( 3 / 36 ) underwent two imaging procedures because of extrasystoles and movement artefacts causing non - diagnostic results of the prospective protocol ; in this situation , the retrospective protocol allows safer management of extrasystoles , especially in view of the need for a second contrast agent injection , which was always administered after verifying that the total dose of contrast medium was compatible with the patients renal function . 
in these cases , we decided to perform a second scan with retrospective gatingmore likely to provide diagnostic results ( through postprocessing ) partly on account of the inability to administer a 252 radiol med ( 2014 ) 119 : 249256 fig . 
b complex pattern of the dosimetric curve of an axial scan with acquisition of four slabs , the last of which is only partially included in the graph as it extends beyond the gafchromic l ( in this patient , the entire thorax was acquired as the clinical question required investigation of the coronary arteries and thoracic aorta ) the high temporal resolution of the 256 - slice ct system used in our study allows for cardiac ct investigations to be carried out with the prospective technique also in patients with high heart rate , who are difcult to assess with older - generation systems . 
the dose savings are evident , even though it should be pointed out that the mean effective dose estimated for the group of patients investigated with the retrospective protocol was particularly high due to the extent of the mean scan range ( mean 30.6 cm for studies without calcium score and 19.1 cm for those with calcium score )  . 
in several cases , in fact , to investigate specic problems , we selected larger areas extending beyond the cardiac region alone , since in routine clinical practice it is often necessary to assess also the thoracic aorta or the course of internal mammary artery bypass grafts , in addition to the coronary arteries . 
if the effective dose is renormalized to a typical scan range for a cardiac study ( around 16 cm ) , the estimated mean desper value is 15.1 msv , which is identical to the doses reported in the literature ( 1418 msv ) [ 3133 ]  . 
pharmacological management with betablocking agents is therefore mandatory [ 36 , 37 ]  . one of the main arguments raised against msct - ca by the cardiological community is that the patient exposure is greater than that involved in conventional coronary angiography ( cca ) ; this issue would therefore be overcome by the possibility of using the prospective technique , characterized by a low radiation dose . 
it should , however , be borne in mind that this is a merely diagnostic examination , which requires a careful selection of patients who should have a high pre - test probability of no disease [ 32 , 34 ]  . the discriminating factors in selecting the acquisition protocol are regularity of the ecg trace and the heart rate , which should not exceed 75 bpm with our ct system . control of the heart rate is therefore a fundamental aspect of the msct - ca protocol [ 35 ] , without which the advantages offered by better - performing equipment cannot be fully exploited and the results will fall short of the if we subdivide the examinations by tube voltage applied , we can appreciate important dose savings with those performed at low voltage ( 80100 kv ) compared to high voltage ( 120 kv )  . the mean value of the percentage variations between desper and dephilips , lower than 10 % , indicates that the estimates of effective dose obtained with the in vivo dose measurements and the ct system dose reports , respectively , have excellent agreement , considering that degree of uncertainty of gafchromic lm measurements is in the order of 1012 % . 
the ct dose report provided by the systems software can therefore be considered reliable . the analysis of the skin dose proles obtained by scanning the 24 - cm - long lm strip placed on the sternum proved instrumental to understanding the methodological principles underlying the two techniques . radiol med ( 2014 ) 119 : 249256 fig . 
this seems to depend on the temporal duration of the tracker scan , in turn related to the single patients circulation time , with higher doses in patients with impaired pump function . this observation allowed us to optimize the imaging protocol by lengthening the interval between tracker scans ( from 1 scan / 0.5 s to 1 scan / s ) and allowing the patient dose to be reduced . the scanner in use at our institute , having a temporal resolution of 135 ms , allows for safe prospective imaging of patients with heart rates up to 75 bpm , with substantial dose savings . 
use of a beta - blocker thus appears necessary not only to improve the quality of the investigation , but also to extend low - dose prospective imaging to a larger number of patients . 
the entrance surface air kerma values for the hospitals of this survey exceeded the korean reference level of 100 lgy . conclusions the different reference levels might be appropriate for the same examination conducted on children of different ages . 
jeon department of radiology , seoul national university hospital , seoul 110 - 744 , korea e - mail : radiologistray@nate.com pediatric patients are different from typical adult patients and the difference is very important in radiological diagnostic imaging . 
in general , pediatric radiological examinations use as short exposure times and as high ma as possible to minimize image blurring that may result from patient motion because pediatric patients are uncooperative . 
pediatric patients vary in size and a small pediatric patient is smaller than the size of the automatic exposure control ( aec ) chambers , so that for pediatric examinations manual technique is selected . 
selecting the imaging modality , using the appropriate positioning and technical parameters , proper geometry , immobilizing the patient , and using gonadal shielding should be considered in pediatric 232 radiol med ( 2014 ) 119 : 231239 tool projection imaging . 
the concept of drl was subsequently adopted by the international commission on radiological protection in icrp publications 60 and 73 [ 3 , 4 ] and provides guidance on appropriate dose levels for typical examinations for groups of standard - sized patients or standard phantoms [ 5 ]  . 
in korea , a recent survey of pediatric patient doses in chest radiological examinations has been carried out on 135 institutions nationwide by the national institute of food and drug safety evaluation ( nifds ) and the drl which is derived from median values of dose distributions is 100 lgy for chest examinations of the average dimensions of 5 - year - old children [ 7 ]  . however , the entrance surface air kerma ( esak ) values in a signicant number of pediatric patients were larger than the korean reference levels . 
in general , higher detective quantum efciency ( dqe ) , which is a measure of the overall efciency of the detector , offers the potential to reduce patient dose or enable better quality images at the same dose [ 1 , 8 ]  . the main purpose of this study was to investigate the technical parameters for dose reduction in chest radiological examinations by evaluating effective detective quantum efciency ( edqe ) including the scatter radiation from the object , the blur caused by the focal spot , geometric magnication and detector characteristics . 
the secondary objective was to measure the esak values for the standard pediatric chest phantom based on data collected from major hospitals of korea and to compare them with the esak values for pediatric chest radiological examinations from data published in the nrpb - report 318 . methods and materials equipment a typical digital radiographic imaging system was used as a platform for dose optimization in pediatric chest examinations . 
this phantom was designed by the food and drug administration ( fda ) for use in the nationwide evaluation of x - ray trends ( next ) program [ 9 , 10 ]  . 
the bsf for diagnostic x - ray beam qualities are reported in the literature [ 11 ] and extrapolation and interpolation of the bsf data , when necessary , were used . average technical parameters and esak values for each hospital are presented in table 1 . effective dose the patient dose is described by the esak , as illustrated in a previous publication , because of the simplicity of its measurement [ 6 , 7 ]  . 
this may be reasonable in some cases , but it is not sufcient for comparing patient doses of different x - ray examination techniques because the esak is not directly related to radiation risk . 
the effective dose quanties the stochastic radiation risk to a patient undergoing any diagnostic x - ray examination and takes into account the dose and the relative radiosensitivity of all irradiated organs [ 2 , 12 ]  . 
pcxmc is a monte carlo program for calculating the doses in 25 organs and the effective doses in pediatric and adult patients of various ages , heights and weights in medical x - ray examinations [ 13 ]  . 
for tube voltages ranging from 40 to 90 kv in 10 kv increments at the fdd of 100 , 110 , 120 , 150 , 180 cm , the entrance air kerma was measured and converted into an effective dose by using each conversion factor which was obtained as the effective dose per mgy . 
in this study , we examined the effects of the radiation eld size , fdd and choice of projection by comparing the effective dose simulated by pcxmc . effective detective quantum efciency ( edqe ) linear system analysis metrics such as detective quantum efciency ( dqe ) had limited usefulness in characterizing the quality of the image obtained with realistic clinical conditions . 
 [ 14 , 15 ] developed the concept of edqe including the scatter radiation from the object , the blur caused by the focal spot , geometric magnication and detector characteristics and the edqe was determined using the following equation : edqef 0 emtff 021 ( cid : 3 ) sf2 ennpsf 0 ( cid : 2 ) tf ( cid : 2 ) k ( cid : 2 ) q where emtf is an effective modulation transfer function ; ennps is an effective normalized noise power spectra ; sf is a scatter fraction ; tf is a transmission factor through the phantom ; k is an incident air kerma corrected to the detector plane ( mr ) ; q is a number of photons per mm2 / mr ; f0 = magnication - corrected spatial frequency . 
the edge test device was placed on the front face of the phantom and was tilted at about 23 ( cid : 3 ) with respect to the detector pixel array to generate a composite edge spread function ( esf ) , which had an than the pixel pitch . 
2 a side - view of the setup system for measurement of scatter fraction , b an image of a beam - stop array device composed of a 14 9 16 array of 224 6 - mm - thick and 3 - mm - diameter lead cylinders smoothed and differentiated to obtain the line spread function ( lsf ) , as described in a previous publication [ 16 , 17 ]  . 
the rois used in the centers of the beam - stop shadows were 10 - pixel - wide squares , and similar rois adjacent to the beam stop were used . we investigated the effects of the radiation eld size to the area of interest , fdd and choice of projection by using results pcxmc . 
the radiation eld size with xed exposure parameters of 50 kv and 2 mas at a fdd of 100 cm was collimated to approximately 17 9 20 , 19 9 22 and 21 9 24 cm2 . 
the effective dose of 156.70 lsv , was calculated for 50 kv and l mgy of entrance air kerma without backscatter fraction in pcxmc dose calculation , was taken to be the standard dose for various fdds . 
figure 3 shows a comparison of the organ doses resulting from chest anteroposterior ( ap ) and posteroanterior ( pa ) projections for pediatric chest phantoall doses correspond to an entrance air kerma of 1 gy without the backscatter fraction . 
technical parameters of 50 kv with a focus - to - detector distance ( fdd ) of 100 cm and ltration of 2.7 mmal are used for 1 - year - old patient phantom various tube voltages . 
6a , the conventional mtf for the system evaluated in this study was also evaluated using standard beam quality , rqa 5 described by an international electrotechnical commission ( iec ) standard [ 20 ]  . 
4 scatter fraction a for the standard pediatric chest phantom with and without an anti - scatter grid as a function of tube voltage and b for the phantom without an anti - scatter grid as a function of fdd . the solid line is a least square t to a second - order polynomial fig . 
this result indicates that the edqe reects the performance of the whole system , while conventional dqe is reective of detector performance alone . the effective dose quanties the radiation risk to a patient undergoing any diagnostic x - ray examination and includes the ability to compare patient doses associated with various in this study , we types of radiographic examination . investigated the effective dose for various technical parameters in pediatric chest examinations using pcxmc dose calculation version 1.5.1. 
although tight collimation can be difcult because a substantial fraction of pediatric patients are uncooperative , radiation eld size should be reduced in order to reduce unnecessary patient dose and scatter radiation . 
the conventional mtf estimate in the horizontal direction obtained with an edge test device at 71 kvp and 21 mmal ltration ( iec - specied rqa 5 beam quality )  . 
b measured emtf with an antiscatter grid as a function of tube voltage discussion pediatric chest phantom , thus reducing the blur caused by focal spot magnication . figure 8 illustrates the edqe results without and with an anti - scatter grid , as well as the effect of variations in tube voltage . 
on the other hand , when an anti - scatter gird was used the largest peak edqe was similar at 70 kvp and the edqe was smallest at 40 kvp . 
the edqe increased with increasing fdd because greater emtf with the lower radiol med ( 2014 ) 119 : 231239 the effect of pediatric chest ap and pa projections by comparing the effective and organ doses . 
these results indicate that organs in the radiation eld are shielded by the rest of the body . thus , the effective and organ doses can be reduced signicantly with proper choice of projection . average technical parameters and esak values from seven major hospitals in korea for the chest radiological examination of a 15 - month - old infant are presented in table 1 . 
we investigated the effect of various technical parameters for dose reduction in pediatric chest radiological examinations by evaluating edqe including the scatter radiation from the object , the blur caused by the focal spot , geometric magnication and detector characteristics . 
comparing the results of the conventional mtf and emtf , the emtfs were notably lower , and these emtf results reect the actual resolutions that might affect chest images obtained using this system in a clinical setting . 
9. the conventional dqe reects the signal - to - noise ratio ( snr ) performance of the image detector alone , while the edqe reects the performance of the overall imaging systethis suggests that the edqe , as a comprehensive metric of image quality , has the possibility of being used for optimization of various technical parameters . 
in this study , the edqe was largest at 60 kvp without and with an anti - scatter grid when comparing the edqe at different is similar when compared to tube voltage . 
the other edqes were evaluated at 50 kvp and a gaussian t was performed 238 radiol med ( 2014 ) 119 : 231239 primary radiation by the grid in order to compensate for a decrease in the snr ratio . 
for small pediatric patients , the amount of scattered radiation is lower , and the amount of grid attenuation increased unnecessary radiation dose . when the grid is not used the edqe increased with increasing fdd because of the greater emtf with the lower focal spot blurring . 
however , most of the major hospitals in korea employed a short fdd of 100 cm with an anti - scatter grid for the chest radiological examination of a 15 - month - old infant , as shown in table 1 . 
the radiation safety management series for pediatric chest radiographic imaging has been released by nifds in korea and drl which are derived from median values of dose distributions is 100 lgy for chest examinations of the average dimensions of 5 - year - old children [ 7 ]  . 
this is because the chest x - ray examinations for 5 - year - olds are usually performed at a longer fdd which usually varies between 150 and 180 cm , while the chest x - ray examinations for the standard pediatric chest phantom representing a 15 - month - old , 24 - pound infant are used at a shorter fdd of 100 cmoreover , the chest ap projection for a 15 - month - old infant is used because the patient cannot be turned . 
it is necessary to rene the technical parameters to perform pediatric chest examinations in korea . conclusion the majority of esak measured in pediatric chest examinations for a 15 - month - old infant are found to be higher than the korean reference level . 
the purpose of this paper was to investigate the effect of these technical parameters by evaluating the edqe , which was designed to reect the actual snr performance of the entire x - ray imaging systeas a result , some of the reasons for the high esak were found to be use of the grid , short fdd and high mas . 
if an anti - scatter grid is required , for older or more obese children , the composition and grid ratio of the device should be considered to keep doses as low as possible . 
dalba unit of innovation , development , strategic planning and management control , university hospital tor vergata , rome , italy conclusions nonmedical costs heavily affect patients nances as well as having an indirect impact on national health expenditure . 
our results show that petct performed with standard dose cect in a single session provides benets in terms of both medical and nonmedical costs . keywords computed tomography ( cid : 2 ) positronemission tomography ( cid : 2 ) costbenet analysis ( cid : 2 ) petct ( cid : 2 ) image fusion introduction in modern oncology , combined imaging based on positronemission tomography and computed tomography ( petct ) plays a central role in the diagnosis , staging and post - treatment follow - up of patients with neoplastic disease [ 14 ]  . two different ct protocols for combined petct are currently used in diagnostic imaging departments . 
the second uses standard contrast - enhanced ct ( cect ) protocols with intravenous or oral administration of contrast medium in order to obtain high - quality diagnostic images and thus make the examination fully diagnostic . several studies have in fact demonstrated the increase in diagnostic value resulting from combined petct . 
recent studies have shown that petct is the best imaging modality for tumour staging , superior both to pet and to pet and ct performed separately [ 6 ]  . by combining diagnostic morphostructural and vascularity information with metabolic data , petct increases 284 radiol med ( 2014 ) 119 : 283289 diagnostic accuracy in the staging and restaging of lung cancer , gastrointestinal tract cancer , breast cancer , kidney and genitourinary tract cancer , melanoma , head and neck cancer , and lymphoma [ 79 ]  . 
according to the authors , the combined petct examination changed the clinical management in 23.1 % of patients , increasing the sensitivity and specicity of the diagnosis in doubtful cases of recurrent cervical carcinoma at pet alone . 
therefore , in addition to enabling a better clinicalradiological management of patients , petct also has a signicant impact on disease - free survival [ 12 ]  . at our institute , close collaboration between radiologists and nuclear medicine specialists and the availability of the appropriate technology enables us to perform petct with cect , when not contraindicated . this petct acquisition technique is used to improve the diagnostic value of the examination and to implement the concept of one - stop - shop recently introduced in modern medicine . 
the possibility of performing tnm staging with a single examination provides a full diagnosis immediately and reduces the time required for the patient to undergo separate diagnostic examinations [ 13 ]  . 
moreover , in a period of general economic difculty , the evaluation of economic resources and their use is important for effective and efcient healthcare management . different types of costs exist that can be evaluated in the healthcare setting : ( 1 ) direct costs , related to prevention , diagnosis and treatment ; ( 2 ) indirect costs , also known as nonmedical costs , which patients and / or family members have to face to receive care ( cost of transport , cost of lost productivity )  . 
loss of productivity should be recorded for both the patient undergoing the test and those who accompany him . their consequently , the choice of partial or total inclusion of the different cost categories in economic analyses depends on the perspective from which the analysis is conducted . the national health system considers only the direct medical costs , while the service users ( the patients ) bear both the direct and indirect costs . 
the literature shows , however , that even studies with a social perspective often fail to include estimates of loss of productivity , even though this represents on average about half of the total cost of a disease . 
these data were obtained from our hospitals accounts department . as regards personnel costs , we started from the contractual annual salary which we divided by the number of working hours and then minutes to arrive at the cost per minute . 
to calculate the duration of the examination and the use of medical personnel , we used the information provided by the italian society of medical radiology ( sirm ) in its document on the qualitativequantitative appropriateness criteria in diagnostic imaging [ 14 ]  . nonmedical costs of combined petct and cect our survey was conducted on a random sample of 100 patients referred to our institute between october and november 2010 . 
the questions elicited current working status at the time of the questionnaire and the type of work done , the distance from home to the institute , and the means of transport used ( public or private )  . 
moreover , to evaluate the costs of informal care , they were asked to indicate whether someone accompanied them to the institute and the type of work done by the person . 
the question on the type of work done was aimed at dening a mean value for each patients working day . in the assessment of transport costs , where the patient used public transport , this cost was approximated to the cost of the fare indicated in the questionnaire . 
where the patient used their own transport , we referred to the italian automobile club tables to identify the cost per kilometre ( km ) for vehicles with the corresponding cylinder size . 
we therefore calculated the cost of transport by multiplying the cost per km by the distance travelled . statistical analysis a general descriptive statistical analysis was performed by considering gender , age , working status of the patient , presence of person accompanying them and their occupation . 
the results of the statistical evaluation , expressed as mean standard deviation and percentage , were obtained using a microsoft ofce excel 2000 spreadsheet . results medical costs of examinations to calculate the costs of the different types of diagnostic examination , we noted that the performance of ct alone involves the use of the ct room for at least 20 min addition , the medical staff is employed for 30 min , the technical staff for 30 min , the nursing staff for 20 min and the auxiliary staff for 15 min ( table 1 )  . 
performance of a petct examination involves the use of a medical doctor for 90 min , a radiology technician for 40 min , a nurse for 25 min and auxiliary staff for 15 min ( table 1 )  . 
all questionnaires were correctly lled in and the data were subsequently recorded correctly in 100 % of cases . our analysis showed that , at the time of the survey , 35 / 100 patients were currently employed , 51 / 100 were retired , 3 / 100 were unemployed , 4 / 100 were students and 7 / 100 were economically inactive ( table 3 )  . 
to reach our centre , each patient travelled an average of 67.4 km for a total travel time of 186 mproductivity loss in monetary terms was estimated on the whole working day , in consideration of the time needed to travel to and from our centre and the overall duration ( about 3 h ) of the examination . 
the cost of a working day was calculated based on data from the european and italian statistical ofces , eurostat - istat , which indicate a median yearly salary of 22 , 701 euro for the industrial sector , 24 , 843 euro for the tradetransport catering sectors , 27 , 134 euro for the insurance , research and service sectors and 23 , 406 euro for the private sector . for an 8 - h working day lost productivity amounted to 102.16 euro ( range 94.58113.05 ) ( table 4 )  . the 35 currently employed patients , 23 were accompanied by employed individuals and two by pensioners . 
in the evaluation of informal care , among the 80 carers we identied 57 currently employed persons , one student and 23 pensioners ( table 3 )  . the productivity loss for these currently employed patients and carers was calculated by estimating the loss of daily income sustained to attend hospital for the examination or to accompany the patient . 
our evaluation shows that 13.5 % of this expenditure is fully borne by the patients and their families . discussion the aims of oncological imaging are to detect and localise lesions , including their relation with adjacent anatomical radiol med ( 2014 ) 119 : 283289 structures and vessels , characterise the lesions , stage the disease and evaluate response to treatment . 
iodinated contrast mediumoreover , the use of pet with specic tracers for the measurement of tumour cell metabolism allows one to dene the grade of malignancy , the presence and distribution of distant metastases , and the effect of chemoand / or radiotherapy , as well as to differentiate between tumour recurrence and necrosis after radiation therapy . 
with this examination it is possible to obtain a clinical diagnosis and more accurate staging , limiting the number of invasive diagnostic procedures . the main limitations of pet are represented by a poor anatomical depiction , which makes the detection of lesions difcult , especially small size ones , and physiological tracer uptake by normal organs and tissues such as the brain , muscle , salivary glands , thyroid , myocardium , gastrointestinal tract and urinary tract , which makes it difcult to interpret images when lesions are situated in such organs . moreover , there may be no tracer uptake by tumours with low metabolism ( neuroendocrine tumours , bronchioloalveolar carcinoma ) and increased uptake in nonmalignant diseases , such as benign or inammatory lesions . it is recognised that fdg - pet and ct are complementary modalities , and that their combined use is essential in oncological clinical practice . 
the introduction of combined petct has made it possible to reduce the noise during attenuation correction making the procedure faster with a 2030 % reduction in acquisition times and improving image quality . 
moreover , fusion of the highimages of ct with the pet resolution morphological images helps to localise the anatomical site of increased tracer uptake on the pet images ( corresponding to a tumour ) , while ct can provide additional information to complete the clinical picture , such as tumour size and the presence of small lesions not identiable on pet . 
at the same time , the ct data can be used to correct the limitations of pet , as in the calculation of the suv ( standardised uptake value ) or correction of the partial volume effect . few authors have investigated the value and efcacy of combined petct performed with simultaneous diagnostic ct . 
diagnostic multiphase cect as part of the combined petct protocol increased petct sensitivity by detecting lesions that were negative on petct in 17 % of patients and exactly identifying the location of 39 % of tumours in suspected sites , especially in patients inuences clinical management with gastrointestinal tract cancers . 
the same authors [ 16 ] , analysing the results obtained in patients with non - smallcell lung cancer , found that diagnostic ct as part of a pet / ct protocol in a substantial number of patients , especially as a result of better planning of surgical interventions and radiotherapy . 
 [ 17 ] also consider petct with diagnostic ct as the examination of choice in patients who require re - evaluation for recurrent cancer of the colon and rectum . additionally , in the assessment of response to chemotherapy in patients with hodgkins lymphoma , orlacchio et al . 
in fact , according to the authors , the use of contrast agents can discriminate between lymph nodes and physiological uptake of 18f - fdg in the urinary and intestinal tract or uptake in the vascular systestill according to the same authors , assessment with cect is also indispensable in the staging of lymphomatous diseases with extranodal involvement , as in this case pet with nonenhanced ct is not always able to detect focal sub - centimetre lesions due to disease persistence . it is therefore clear that pet and ct support each other and that their combined use leads to signicant benets . 
in diagnostic imaging centres with appropriate technology and competence , petct should be performed with a diagnostic ct protocol both because of the undoubted diagnostic value and to reduce the dose of ionising radiation . 
in fact performing the examinations separately could lead to a diagnostic delay which in turn could delay treatment decisions , with unquantiable clinical and economic disadvantages . according to our experience , there was no evidence of any increase in waiting lists when performing petct with cect compared to petct without cect . 
the examination time is in fact the same for the different techniques ( about 90 min ) and the possibility to perform diagnostic ct at the same time as pet allows a reduction of the daily ct lists . 
the nal result is a possible reduction in the 288 radiol med ( 2014 ) 119 : 283289 time to complete diagnosis and savings in terms of both medical and nonmedical costs ( working days )  . the aim of our study was to evaluate the costs of performing petct with diagnostic ct , both in terms of medical and nonmedical costs . 
as a result , these studies tend to be incomplete and imprecise because they only evaluate the direct medical costs without considering the specic situation of the single patient [ 21 ]  . however , even if the costs borne by the patient are invisible to the national health system , in an economically difcult period it is necessary to perform a detailed analysis of costs deriving from the provision of a health service , of whatever kind it may be [ 22 ]  . regarding medical costs , our evaluation shows clearly that the costs of combined petct are lower than the sum of the costs of the two examinations performed separately . our study shows the importance of nonmedical costs and informal care in economic evaluations in health care . 
in fact , our results show that these costs amount to 13.5 % of the costs deriving from the examination . to our knowledge , there are no other studies that correlate the nonmedical costs of petct and ct examinations . 
consequently , hypofractionation would result in a reduction of nonmedical costs and , when the patient is accompanied , also of informal care costs . with this assessment we can deduce that reducing the number of hospital visits by performing the examination in a single session is useful for lowering the total costs , both medical and nonmedical . performance of petct with cect , instead of separate petct and cect , results in a signicant decrease in nonmedical and informal care costs in addition to reducing the direct medical costs . 
our experience also emphasises the need for dedicated resources for carrying out cost analyses and for a close interaction between clinical and economic researchers , with periodic meetings to update the cost assessments of the various examinations . with respect to costs , the cost of petct with cect is lower than the sum of the costs of the two examinations performed separately . 
moreover , petct with cect could also allow for lower nonmedical costs compared to the sum of cect and petct performed on separate occasions ( cost of transport and loss of productivity for patients )  . these evaluations can be extended to other diagnostic methods . 
also in this case , it would be appropriate for mri to be of diagnostic value rather than just useful for pet attenuation correction and the anatomical localisation of pet ndings . conclusions the petct examination performed with cect should be offered in centres that have the appropriate technology , on account of both its high sensitivity and specicity and the possibility of reducing patient radiation exposure . moreover , the results of our study indicate that nonmedical costs are considerable , so that petct with cect performed during the same session rather than at different times is absolutely efcient and provides signicant advantages in terms of costbenet for the patient , because it halves the costs related to transport and loss of productivity . 
to evaluate the effectiveness of this process , t cells loaded with 111in - radiolabelled aunps were injected directly into the right lung of nude mice for in vivo imaging by micro - spect / ct . 
t cells loaded with 64cu - radiolabelled aunps were then injected into the tail vein of nude mice and imaged by micro - pet / ct . results high uptake signals were observed in the right lung following the direct injection of t cells containing 111in - labelled aunps . 
cui college of science , university of shanghai for science and technology , shanghai , china the dynamic biodistribution of t cells containing 64cu - labelled aunps when compared with 64cu - labelled aunps alone . conclusions this study demonstrated the feasibility of the in vivo imaging of t cells loaded with radiolabelled aunps . keywords t cells ( cid : 2 ) gold nanoparticles ( cid : 2 ) in vivo imaging introduction in the human immune system , lymphocytes with cytolytic functions include natural killer ( nk ) cells and cytolytic t cells . 
the basic principle of adoptive immunotherapy involves the separation of lymphocytes from either the peripheral blood of cancer patients or surgically resected tumour tissue . these lymphocytes are then cultured in vitro in the presence of interleukin - 2 ( il - 2 ) , which stimulates lymphocyte [ 1 ]  . proliferation and enhances anti - tumour adoptive transfer of these lymphocytes into cancer patients results in tumour recession and prevents metastasis , thus achieving the therapeutic purpose . 
therefore , tracking the reinfusion of such lymphocytes in vivo is critical . functions t cells play a central role in cell - mediated immunity and can be genetically modied to target specic receptors expressed on tumour cells . 
1 the aunp labelling process radiol med ( 2014 ) 119 : 269276 materials and methods laboratory animals eleven male balb / c - nu / nu nude mice ( aged 6 weeks , 1822 g ) were acquired from the national cancer institute and housed in micro - isolator cages . 
the synthesis and analysis methods of these two aunp types were similar and , therefore , the method used the purposes of for dota alone is described for illustration . bifunctional opss - peg - nhs stable rod - like gold aunps were prepared using the cetyl trimethyl ammonium bromide ( ctab ) method described by sau et al . 
p - nh2 - bn - dota ( s - 2 - ( 4 - aminobenzyl ) - ) was conjugated ( opyrglycol - n - hydroxysuccinimide idyldisulde - polyethylene ester )  . 
p - nh2 - bn - dota and opss - peg - nhs were mixed at a 1 : 1 molar ratio and the mixture was incubated overnight at room temperature . 
the resulting opss - pegdota was then added to the aunps solution in 10 mm phosphate buffer ( ph 7 ) at a 10 , 000 : 1 molar ratio followed by overnight incubation at room temperature . 
solutions were then incubated at 37 ( cid : 3 ) c for 90 min followed by the addition of the peg - sh blocking agent at an approximate 300 , 000 : 1 molar ratio and incubated at room temperature for 1 h . reaction mixtures were then centrifuged to remove unconjugated 64cucl2 and peg . 
labelling efciencies were calculated by the following formula : ( cid : 2 ) activity in pellet = activity in supernatant activity in pellet ( cid : 3 ) ( cid : 3 ) 100 : radiolabelling stability was also investigated by incubating 64cu - nps in pbs and serum at 37 ( cid : 3 ) c for up to 5 h . 
percentages of 64cu remaining on the nps were calculated by the following formula : ( cid : 2 ) activity in pellet = activity in supernatant activity in pellet ( cid : 3 ) ( cid : 3 ) 100 : the control 64cu - dota sample was prepared by mixing 64cucl2 ( 2.0 mci ) with 200 ll 0.20 mm dota solution ( ph 6.5 ) and incubating at 37 ( cid : 3 ) c for 90 mthe 64cu - dota - peg was prepared by mixing 64cucl2 ( 2.0 mci ) with 200 ll 0.20 mm dota - peg solution ( ph 6.5 ) and incubating at 37 ( cid : 3 ) c for 90 mthe formation of 64cu complexes was veried by radio thinlayer chromatography using a mobile phase that consisted of 50 : 50 meoh / 10 % ammonium acetate on silica plates . and incubated on ice for 510 melectroporation was conducted using a btx cm830 device with the following settings : 1 kv / cm , 4 ms duration , single square pulse . subsequently , the electroporation cup was incubated on ice for a further 510 min before the cells were transferred to 1 - ml culture medium containing 10 % calf serum and incubated at 37 ( cid : 3 ) c in an atmosphere containing 5 % co2 for 2 h . 
preliminary spect and ct images were acquired in axial , sagittal and coronal planes and fusion images were obtained on the workstation . analysis of the biodistribution of t cells containing aunps by micro - pet / ct the other ten mice were randomly divided into two groups . in group 1 , t cells ( 0.5 9 106 cells ) transformed with 64cu - aunps were administered intravenously ( iv ) into ve mice and in vivo micro - pet / ct images were acquired at three time points : immediately after injection , 2 and 18 h after injection . 
all mice were anaesthetised , and pet and ct fusion images were acquired as described above . results transferring aunps into t cells via electroporation all cell handling was aseptically performed in a laminar ow hood . 
t cells were separated from the peripheral blood of normal individuals and the trypsinized cell suspension was transferred to 1.5 ml ep tubes containing dmem medium supplemented with 10 % calf serum and centrifuged at 1 , 000 rpm for 5 min at room temperature . 
the cell suspension and synthesised aunps were mixed at a concentration of 2 9 107 / ml in a 4 - mm electroporation cup the maximum absorption wavelength of the aunps was identied as * 740 nm by uvvis spectrophotometry . zetasizer measurements showed that the particle size of the primary aunps was * 25 nm in diameter with a zeta potential of approximately - 50 mv . 
t cells were injected into mice via the tail vein and micro - pet / ct images were acquired . the biodistribution of t cells containing 64cu - labelled aunps was tracked in group 1 mice . 
this technique involves the adoptive transfer of specic immunity in the form of sensitised lymphocytes or the products of these cells into patients lacking some aspects of cellular immune function , thus providing anti - tumour immunity . 
many groups [ 5 , 6 ] are now committed to generate a variety of t cell chimeric antigen receptors ( car ) that render t cells capable of targeting tumours in an antigen - specic manner . 
the ability to observe such lymphocytes in vivo is critical for the real - time monitoring of their biodistribution , viability and the occurrence of rejection and allows the more accurate assessment of adoptive immunotherapy efcacy [ 7 ]  . surface - modied nanoparticles possess controllable biological characteristics and versatility [ 810 ]  . 
these include the amplication of imaging signals that emanate from the encapsulated imaging agent , molecular recognition of specic antigen and receptor interactions of target cells by the coupling of antibodies or ligands , transport of one or more treatment factors , and the avoidance of biobarriers , such as by pegylation to increase their circulation time for the avoidance of macrophage uptake . 
therefore , surface - modied nanoparticles concurrently perform a variety of important functions in disease treatment and diagnosis [ 11 ]  . aunps exhibit many favourable features [ 1214 ] such as controllable shape and size , mild surface chemistry and radiol med ( 2014 ) 119 : 269276 fig . 
3 micro - pet / ct images showing the dynamic biodistribution of t cells carrying 64cu - labelled aunps good biocompatibility , coupled with a unique plasma surface absorption , light scattering and other physical properties . 
to date , the majority are\50 nm in diameter , with uniform size and good colloidal stability . these aunps are spherical , shell - like , rod - like or cage - like and the surface is easily modied with targeting proteins , specic biological markers and aptamers . 
furthermore , gold is easily identied and characterised by commonly used elemental analysis methods , thus enabling the improved validation of imaging data . in this study , a conjugation procedure was developed to label nps with 64cu ( t1 / 2 = 12.7 h ) , using bifunctional opss - peg - nhs and the bifunctional chelating agent , dota - nh2 . 
5 kinetic analysis of imaging agent uptake in the lung and liver tissues of group 1 and group 2 mice showing marked differences in the biodistribution of t cells containing nanoparticles compared with nanoparticles alone radiol med ( 2014 ) 119 : 269276 liver rapid clearance the ability to transfer nanoparticles and a wide range of other materials into t cells via electroporation can be exploited to adapt t cells as biological delivery vehicles capable of targeting specic tissues , such as tumour tissue , and to facilitate the in vivo imaging of these tissues [ 18 ]  . furthermore , aunps can be used to target the delivery of therapeutic genes and chemotherapeutics for tumour therapy [ 19 , 20 ]  . 
this improvement in local retention can also enhance the efcacy of the therapeutic effect [ 21 ]  . electroporation involves the subjection of cells to a controlled electric eld , such as a transient high - intensity electric eld , which results in reversible pore formation in the cell membrane . 
in general , the electroporation transfection efciency and cell viability are affected by factors that include pulse amplitude and duration , temperature , buffer composition , cell status and volume [ 23 , 24 ] , with pulse amplitude being the key parameter . 
in contrast , if the pulse amplitude is too high , the viability of transfected cells is greatly affected , which in turn decreases the transfection efciency . in the initial phase of our experiment , 111in - labelled aunps were transferred into t cells via electroporation , and directly injected into the right lung of mouse 1 . 
after the injection of transfected t cells into the tail vein of group 1 mice , the acquisition of micropet / ct images at three time points clearly showed the dynamic biodistribution of t cells loaded with 64culabelled aunps in the body of normal nude mice . 
control images of 64cu - aunp alone from group 2 mice showed a marked difference in the biodistribution of radiolabelled nanoparticles alone when compared with t cells loaded with 64cu - labelled aunps . these preliminary studies indicated that the in vivo imaging of t cells loaded with radiolabelled aunps was feasible . 
they represent a basis for the further development of imaging protocols that can assess the delivery of multifunctional aunps by genetically - modied t cells into tumour - bearing nude mice [ 25 ]  . 
the clinical and technical characteristics of the rst ten proton beam radiotherapy treatments are reported . materials and methods ten patients , six males and four females ( age range 2773 years , median 55.5 ) , were treated with proton beam radiotherapy . 
after one to two surgical procedures , seven patients received a histological diagnosis of chordoma ( of the skull base in three cases , the cervical spine in one case and the sacrum in three cases ) r . 
prescribed doses were 74 gye for chordoma and 70 gye for chondrosarcoma at 2 gye / fraction delivered 5 days per week . results treatment was well tolerated without toxicityrelated interruptions . 
after 612 months of follow - up , no patient developed tumour progression . conclusions the analysis of the rst ten patients treated with proton therapy at cnao showed that this treatment was feasible and safe . 
currently , patient accrual into these as well as other approved protocols is continuing , and a longer follow - up period is needed to assess tumour control and late toxicity . keywords proton therapy ( cid : 2 ) skull base ( cid : 2 ) spine ( cid : 2 ) chordoma ( cid : 2 ) chondrosarcoma ( cid : 2 ) hadrontherapy introduction the italian national centre for oncological hadrontherapy ( centro nazionale di adroterapia oncologica , cnao ) was established in 2001 by the italian ministry of health , and a project was launched to realise a centre designed for the use of charged particles for cancer treatment . 
the facility is equipped with a synchrotron to accelerate protons and ions and with three treatment rooms , two with xed horizontal and one with both horizontal and vertical beam lines . 
after relevant commissioning tests , clinical activity started with protons in september 2011 and with carbon ions in november 2012 . 278 radiol med ( 2014 ) 119 : 277282 we report the results of the rst ten patients affected by skull base and spine chordoma and chondrosarcoma who have completed proton beam radiotherapy , with an emphasis on the clinical and technical characteristics of the treatment . inclusion into the approved protocols for proton therapy . each patient received in - depth information regarding the potentially expected outcome and side effects and gave their informed consent . materials and methods patient population to start clinical activity , prospective trials for proton beam radiotherapy were designed for established indications as per existing literature and included skull base and spine chordoma and chondrosarcoma and intracranial meningioma . 
they were conducted in agreement with the criteria of the helsinki declaration . we report on the rst ten patients , with a minimum of 6 months follow - up , treated in phase ii trials for skull base and spine chordoma and chondrosarcoma of grade iii . 
the main patients characteristics are shown in table 1 . clinical symptoms and signs were dependent on the site of the disease and included headache , cranial nerve decits , visual and auditory and hypothalamuspituitary dysfunclesions , and mobility tion in patients with intracranial problems and bowel or bladder incontinence for patients with spine tumour locations . five out of ten patients were referred after the rst surgical operation , 3 / 10 were referred after having been reoperated either for gross residual disease or for tumour relapse , and 2 / 10 , deemed unresectable at the time of diagnosis , were referred for proton therapy after undergoing biopsy for diagnostic purposes . 
the ct scan was performed with a slice and interslice thickness of 2 mm . magnetic resonance imaging ( mri ) with a 3.0 t unit ( magnetom verio , siemens , germany ) was also performed in the same position as the simulation ct , using the same immobilisation device . 
the sequences obtained were contrast and noncontrast t1 , t2 images along with fat suppression , flair ( uid - attenuated inversion recovery ) , stir ( short tau inversion recovery ) and adc ( apparent diffusion coefcient ) sequences . 
both ct and mri datasets were transferred via the dicom protocol to the treatment planning system ( tps ) ( syngo vb10 , siemens , germany ) for image fusion prior to segmentation . 
the structures delineated were gross tumour volume ( gtv ) , clinical target volume ( ctv ) , both low dose and high dose , planning target volume ( ptv ) both low and high dose , and organs at risk ( oars )  . 
1 setup verication in a patient with skull base chordoma before treatment delivery radiol med ( 2014 ) 119 : 277282 tumour location and included brainstem , temporal lobes , pituitary , optic chiasm , optic nerves , eyes , cochlea , spinal cord , parotid glands , pharyngeal sphincters , larynx for the skull base region , and rectal wall , sacral nerves , spinal cord , kidneys and small bowel for the spine location ; the skin was delineated as an oar in all cases . 
ctv to ptv expansion was 2 mm for skull base and 4 mm for spine tumours , gures that were obtained after accurate in - house estimation of the patient setup . 
the high - dose ctv values for skull base and spine tumour locations are reported in table 2 . doses were measured in gray equivalent ( gye ) considering a relative biological effectiveness value of 1.1 compared to that of photons . 
in the second phase , the prescribed dose was 20 gye for chordoma and 16 gye for chondrosarcoma at 2 gye per fraction , and sbo was used in two cases and impt in seven cases . 
the maximal acute toxicities recorded are listed in table 3 and consisted of grade 2 oropharyngeal mucositis and nausea and vomiting for skull base tumours , and grade 2 dermatitis for sacral tumours . 
2 relative dose distribution on axial , sagittal and coronal computed tomography ( ct ) slices depicting planning target volume and healthy structures in a case of skull base chordoma 280 radiol med ( 2014 ) 119 : 277282 table 3 maximal acute toxicities during treatment none grade 1 grade 2 grade 3 skull base / cervical spine ( n = 7 ) oropharyngeal mucositis dermatitis alopecia headache nausea vomiting dysphagia dermatitis proctitis dysuria sacrum ( n = 3 ) fully recovered within a few weeks after completion . treatment after a minimum and maximum follow - up interval of 6 and 12 months , all but one patient ( 9 / 10 ) showed sd at mri studies . 
as for subtypes are chondrosarcoma , the usual histological conventional and mesenchymal , which are further classied as grades iiii based on the differentiation [ 14 ]  . grades iii ( low - grade ) are quite indolent and tend to recur locally , while grade iii is more aggressive with a high metastatic potential [ 2 , 3 ]  . 
complete surgical resection offers the best chance of control , but is rarely achievable due to the proximity of nearby critical structures which risk irreversible damage in the case of aggressive resection . consequently , in most cases gross or microscopic residual disease is the norm , which translates into high recurrence rates . 
in our series , only partial resection could be achieved in skull base cases , even though repeat resection was attempted in two out of seven cases . combining surgery with radiation has improved the local control rates in literature studies . 
these tumours are considered to be relatively radioresistant and a minimum useful photon dose is considered to be 6065 gy , or even higher , especially in series where charged particle irradiation was used [ 2 , 3 , 57 ]  . 
in part , these high local recurrence rates in older literature series could be attributed to limitations of imaging for target identication , but even contemporary series reported poor control rates with conventional radiation at dose levels of 5064 gy [ 11 ]  . 
 [ 12 ] , in a study of patient outcome after stereotactic fractionated photon radiotherapy used to treat skull base chordoma and low - grade chondrosarcoma with doses of 66.6 gy ( for chordoma ) and 64.9 gy ( for chondrosarcoma ) , reported 5 - year local control rates of 50 and 100 % , respectively . analysis of predictors for local failure after proton beam radiotherapy by terahara et al . 
this can be achieved by combining adequate surgical resection with protons which can offer a better dose distribution compared to photons . when performing surgery on sacral tumours , care has to be taken to preserve the sacral nerves and cauda equina . chordomas are slow - growing tumours which can reach considerable dimensions in the pelvis before the symptoms appear and the diagnosis can be obtained . 
additionally , in these cases , proton therapy offered a chance to preserve bladder and bowel function while controlling tumour progression . in terms of dose distribution , protons have an edge over photons due to the inherent radiation physics , although radiobiologically they do not differ greatly from photons , having a radiobiological effective value of 1.1 as compared to 1 of photons . 
the characterising feature is the energy deposition in the patient tissues located in the bragg peak that can be opportunely spread out , thereby sparing most of the traversed and the deeper located tissues . 
this high spatial selectivity enables better sparing of the healthy tissues [ 16 , 17 ] and can result in delivery of 1020 % higher doses to the tumour as compared to conventional radiotherapy [ 12 , 18 ]  . 
it has also been reported that protons deliver 1.53 times lower integral dose outside the target volume as compared to x - rays [ 19 ]  . protons can be delivered as either a passive scattered beam or an active spot - scanning technique . 
this way , the high - dose region is limited to the target alone and , unlike the passive scattering systems , there is no extra dose deposition proximal to the target itself [ 20 ]  . 
in the given set of patients , a combination of both sbo and impt techniques was used in most cases . consequent to the superior dose conformation , sparing of normal tissues was possible to a higher extent as compared to conventional radiotherapy , which translated into a low incidence of acute side effects reported in this set of patients , with maximal toxicities being bgrade 2 overall . 
it should be emphasised that , apart from dermatitis , more common in cases of sacral lesions approaching the skin surface , a major proportion of patients had no toxicity at all during the course of treatment . after a minimum of 6 months follow - up , 9 / 10 patients had sd and 1 / 10 was labelled as having pr as per the protocol . 
after radiotherapy , no dramatic shrinkage of the tumour is expected to be seen on imaging studies . accordingly , the general consensus is to dene tumour control as a state of no clinical or radiological signs of tumour progression . late toxicity was assessed in all patients , although the follow - up was limited to 612 months ; two patients were scored as having grade 2 toxicity as per ctcae v 4.0. 
one patient with sacral chordoma had episodic rectal bleeding persisting for 34 weeks that resolved spontaneously , and the other patient , who had skull base chordoma , had an expected hypothalamicpituitary failure and is currently on hormone replacement therapy . 
early toxicity and preliminary ndings of late side effects are in the range of the other literature reports [ 2 , 7 , 14 ]  . conclusion the analysis of the rst ten patients treated with spotscanning proton therapy at cnao showed that this treatment was feasible and could be delivered safely with mild toxicity . 
currently , patient accrual into these as well as other approved protocols is continuing and a longer followup is needed to assess denitive local tumour control rate and late toxicity . the technical and scientic committee , acknowledgments the authors would like to acknowledge the president , the advisory board , the general secretary , the ofce of communications , the department of safety prevention and environment service , department of legal affairs and human resources , the department of radioprotection , the ofce of quality , the accelerator department , the department of infrastructure , the department of administration and finance , the radiation technologist unit and the nursing staff for their contribution towards making it possible to initiate clinical activity at cnao . conict of interest roberto orecchia , v . 
the type of claim was examined in each of the 26 cases , with as many as 15 being related to radiotherapy injury to tissues surrounding the neoplasm , thus confirming this to be the most frequent cause for insurance claims . 
now that the historical causes of error that led to incorrect radiotherapy treatment have been eliminated through strict adherence to protocols , risk management in radiotherapy identifies side effects as the main source of risk for patients and physicians . 
data analysis confirms the need to implement risk management procedures in radiotherapy in which insurance claims ( 15 / 26 cases ) are motivated by side effects of treatment . key words risk management radiotherapy side effects insurance claims riassunto obiettivo . 
si utilizzata unanalisi delle denunce assicurative , nellarco di un periodo congruo di 10 anni , sulla base dei radioterapisti , 256 nel 2004 , assicurati con la societ scientifica . 
stata analizzata la tipologia delle 26 denunce e di queste ben 15 riguardavano danni da radioterapia a tessuti circostanti la neoplasia confermando come tale fattore , analizzato nelle cause di risk management , sia quello pi frequente di denuncia . 
eliminate , con ladesione puntuale ai protocolli , le cause storiche di errore che portavano ad un trattamento radioterapico errato , attualmente il risk management in radioterapia individua negli effetti collaterali la fonte di maggiore rischio per il paziente ed il medico . 
lanalisi dei dati conferma la necessit di attuare norme di risk management in radioterapia nella quale il contenzioso , 15 casi su 26 , riferibile agli esiti collaterali del trattamento radioterapico . parole chiave risk management radioterapia effetti collaterali denunce assicurative f . 
fileni : risk management in radiotherapy introduction introduzione all human activity has associated risk factors , and the awareness of this has led to undertaking measures for protection and prevention . 
risk factors are particularly numerous in medicine and depend on the nature of diseases treated , increasing average patient age , the high number of patients treated each year , the number of professionals involved in treatment and complexity of each individual therapeutic procedure . for a number of years now , awareness has been increasing of the need to assess the various risk factors of hospitalisation , particularly with regard to patient care and treatment , both to implement prevention measures and to reduce the number of litigations and , as a consequence , the amount of insurance premiums , particularly for hospitals that implement forms of risk prevention [ 1 ]  . 
in other words , risk management involves all of the coordinated activities undertaken by a healthcare facility to define work procedures and exclude foreseeable and avoidable risks [ 2 ]  . 
this type of definition and interpretation , which applies to high - risk activities ( above all in aeronautics ) , should also be applied in healthcare , the specific field of action of which involves the patient , treatment of disease and risks the patient may run when treated in a healthcare facility . applying criteria of risk management to medical practice allows identification of all activities carrying an intrinsic risk both those due to the organisation of the healthcare facility and to the actions of healthcare workers themselves and identification of tools necessary for assessing , managing and eliminating those risks . 
these actions are aimed at improving overall healthcare practice since risk management in healthcare means attaining quality and safety in the patients interest [ 3 , 4 ]  . a further aspect of risk management is aimed at specific assessment of medical activity to minimise professional risks related to the various specialties , with the same goal of recognising and preventing thethe concept of safe practice should be seen in the context of clinical governance , considered as healthcare workers monitoring and self - assessment of their practices , which is also aimed at safeguarding the healthcare workers themselves , both physicians and nonphysicians alike , who work within the systeso as to be completely effective , clinical governance must therefore implement risk management programmes within each department or division . 
assessment should therefore include the interaction between risk and clinical governance that is distinctive of the various specialties , thus making all healthcare professionals more responsible for reducing risk . this objective appears to be more ambitious and a greater safeguard for patients than the objective that has been set for several years in the united states , where risk management has the economic - financial aim of reducing economic loss ( incurred by hospitals and physicians ) due to errors and injury to patients , and of reducing insurance premiums as a consequence . ogni attivit umana presenta potenzialmente dei fattori di rischio e la coscienza di ci ha spinto ad intraprendere azioni di tutela e prevenzione . 
in campo medico tali fattori sono particolarmente numerosi : ci dipende dalla natura stessa delle malattie , dallinnalzamento dellet media , dallelevato numero di pazienti trattati ogni anno , dalla pluralit degli operatori coinvolti e dalla complessit ormai raggiunta da ogni singola attivit terapeutica . da diversi anni ci si resi conto della necessit di valutare i diversi fattori di rischio nella ospedalizzazione , specie nella attivit assistenziale e medica , sia per effettuare unopera di prevenzione e sia al fine di ridurre il fenomeno del contenzioso medico - legale e , conseguentemente , anche limporto dei premi assicurativi , specificatamente per gli ospedali che attuavano forme di prevenzione del rischio [ 1 ]  . con il termine risk management si intende quindi linsieme delle attivit con le quali si conosce e gestisce il rischio e grazie alle quali si attuano le procedure per prevenirlo ; rappresenta cio linsieme delle azioni coordinate intraprese in una azienda sanitaria al fine di guidare unorganizzazione lavorativa ad escludere i rischi prevedibili ed evitabili [ 2 ]  . questo tipo di definizione ed interpretazione , valida nelle comuni imprese ed attivit ad alto rischio ( massima in quella aeronautica ) , deve essere applicata anche nellambito sanitario che ha il suo campo specifico di azione verso il paziente , verso il trattamento della malattia , e verso i rischi nei quali il paziente pu incorrere quando trattato in ambito clinico - sanitario . applicare anche nellattivit medica i criteri del risk management consente di evidenziarne tutti gli atti intrinsecamente rischiosi , da parte sia della organizzazione della struttura sia degli atti propri degli operatori , ricercando gli strumenti che ne consentano la valutazione con il fine ultimo di governarli ed eliminarli . 
con tali azioni si persegue il miglioramento dellattivit aziendale nel suo complesso , perch la gestione del rischio clinico in sanit si configura come raggiungimento della qualit e della sicurezza a tutela dei pazienti [ 3 , 4 ]  . un ulteriore aspetto del risk management rivolto anche alla specifica valutazione dellattivit medica per ridurre al minimo i rischi professionali legati alle varie specialit sempre al fine di conoscerli e prevenirli . 
inoltre il concetto di attivit sicura si deve inserire in quello che oggi il governo clinico , inteso anche come controllo ed autovalutazione della propria attivit da parte degli operatori della sanit , e ci a tutela anche degli operatori , medici e non , che in tale sistema operano . il governo clinico , per essere completamente efficace , deve tradurre operativamente allinterno di ogni unit operativa anche il programma di risk management . 
sono quindi da valutare anche gli aspetti di interazione tra rischio e governo clinico ( clinical governance ) che sono peculiari delle varie specialit aumentando la responsabilizzazione di tutti i professionisti e operatori sanitari finalizzata alla diminuzione del rischio . tale obiettivo appare pi ambizioso e tutelante rispetto a quello applicato gi da diversi anni negli usa , nel quale il risk management in radiotherapy radiotherapy has distinctive risk features owing to the invasiveness of radiating techniques used and to the seriousness of neoplastic disease [ 57 ]  . radiotherapy applications in nonneoplastic disease will not be considered here , both because these are numerically more limited and , above all , because the radiotherapists safety margin is much broader since these diseases do not require high radiation doses to control the tumour . 
it is therefore essential to achieve a therapeutic compromise based on appropriateness of radiation treatment required for recovery , personalised for each individual patient affected by a specific type of cancer , and with minimal , even if inevitable , damage to surrounding healthy tissues [ 8 ]  . risk management for the specialist oncological radiotherapist applies to the first assessment of the patient , monitoring the type and course of disease , choice of treatment plan , sharing and acceptance by the patient of both radiotherapy and possible side effects , and during treatment cycles close observation of premonitory symptoms of side effects , all of which is decided on the basis of disease stage and general condition of the patient [ 9 ]  . the considerable changes in the attitude of patients in recent years with regard to their disease , and in particular in the case of cancer , should be borne in mind . 
thanks to the increasing diffusion of news by various media , there is today a much more widespread knowledge of medical topics . just a few decades ago , patients tended to be passively resigned to having cancer and undergoing the necessary treatment whereas today , they are much more informed , or even fully aware , of their disease . 
they are , nonetheless , less well informed regarding discomfort , risks and side effects that treatment may entail , be it surgery , radiotherapy or chemotherapy . increasing survival times and the possibility of complete recovery have , on the one hand , clearly led to increased trust in the positive outcome of treatment while , on the other , they have led to an increasing demand to reduce the toxic effects of treatment and to nonacceptance of their inevitability . 
for decades now , radiotherapy has been performed taking for granted that the diagnosis of cancer , supported by correct clinical , imaging and histological assessment , is certafor this reason , diagnosis of a tumour must be based on definite histological findings . 
this has ( or should have ) led to elimination of the first three types of risk in radiotherapy that were present in the early days of the discipline : ( 1 ) treatment of a healthy patient ; ( 2 ) treatment of an unhealthy patient not suffering from cancer ; ( 3 ) incorrect treatment . given that the conditions have been satisfied for eliminating the risk of inappropriate indication of treatment , the risk inherent in the method of performing treatment , which is still potentially possible , needs to be examined . 
fileni : risk management in radiotherapy risk management ha una finalit economico - finanziaria per ridurre le perdite economiche ( degli ospedali e dei medici ) dovute a errori e danni al paziente nelle cure e , conseguentemente , per ridurre gli importi dei premi assicurativi . il risk management in radioterapia la radioterapia presenta peculiari e specifici aspetti di rischio per linvasivit delle metodiche radianti utilizzate e per la gravit delle patologie neoplastiche trattate [ 57 ]  . non verranno qui considerate le applicazioni della radioterapia in patologie non neoplastiche , sia perch numericamente pi limitate sia soprattutto perch il margine di sicurezza del radioterapista pi ampio non essendo condizionato dalla necessit di erogare una dose elevata per ottenere il controllo della neoplasia . 
in ambito oncologico invece ogni trattamento richiede la ricerca di un equilibrio ottimale determinato dal rapporto tra effetto terapeutico delle radiazioni sulle cellule neoplastiche ed il minor danno ai tessuti sani circostanti la neoplasia . caratteristica fondamentale quindi il raggiungimento di un compromesso terapeutico basato sulladeguatezza del trattamento radiante , al fine della guarigione , personalizzato sul singolo paziente affetto dalla specifica tipologia di cancro , con la minima , anche se inevitabile , compromissione dei tessuti circostanti sani [ 8 ]  . il risk management dello specialista radioterapista oncologo legato alle varie fasi che vanno dal primo approccio con il paziente , al controllo del tipo e decorso della malattia , alla scelta dei percorsi e piani terapeutici , alla condivisione ed accettazione da parte del paziente sia della radioterapia che dei possibili effetti secondari o collaterali , e , durante i cicli di terapia , anche losservazione attenta dei sintomi premonitori degli effetti collaterali ed il tutto sempre deciso in base dello stadio di malattia e alle condizioni generali del paziente [ 9 ]  . bisogna considerare che negli anni latteggiamento dei pazienti nei confronti della malattia , ed in particolare nel caso di tumore , notevolmente mutato . 
solo pochi decenni fa i pazienti manifestavano una rassegnazione passiva nei confronti del cancro e delle necessarie terapie ; oggi invece sono sempre pi informati , se non perfettamente consapevoli , della loro malattia . 
sono tuttavia sicuramente meno informati e consapevoli dei disagi , dei rischi e degli effetti collaterali che qualsiasi trattamento ( chirurgico , radio o chemioterapico ) comporta . evidente che il sempre maggiore allungamento dei tempi di sopravvivenza , se non la guarigione stessa , da un lato , porta ad una maggiore fiducia di risultati positivi da parte dei trattamenti instaurati , dallaltro , rende sempre pi alta la richiesta di ridurre gli effetti tossici del trattamento stesso e la non accettazione della loro inevitabilit . 
ormai da decenni la radioterapia viene attuata dando come fattore acquisito che la diagnosi di cancro , supportata da una corretta valutazione clinico - strumentale ed istologica , sia di certezza e per tale motivo i criteri di diagnosi di neoplasia def . 
fileni : risk management in radiotherapy without the patient having given consent or being correctly informed of the risks and possible ( serious ) side effects ; ( 2 ) correct radiotherapy treatment but not accompanied by a satisfactory therapeutic response in terms of tumour control and symptom reduction or remission ; ( 3 ) incorrect radiotherapy treatment . an example of the first type of possible litigation , which regards informed consent , could be a case of radical radiotherapy of the cervix , which , given the high doses of radiation required for it to be completely effective , can produce more or less serious side effects with possible damage to the small bowel and colon . 
once a methodological error has been ruled out , possible subjective biological factors or unrecognised variables can be considered , which negatively affected the therapeutic response [ 11 ]  . such cases of limited therapeutic response are most commonly attributable to tumour aggressiveness . 
there is , however , the inevitable risk that the patient may compare their own with other situations and be critical of the treatment received ( an attitude supported at times by the physicians tendency to criticise , often in the absence of the necessary information for making a fair judgment )  . the third case incorrect treatment falls into the class of malpractice due to inexperience , carelessness or negligence . 
to prove this , there are methods to analyse a posteriori , independent of the therapeutic result , the correctness of the radiotherapy technique performed and the potential risk factors [ 12 ]  . 
this review is fundamental in that an analysis of real or presumed errors is the basis for implementing risk management . criteria for assessing treatment correctness are the following : ( 1 ) correspondence of the treatment schedule for administration of radiation dose and technical performance by the radiographer ; ( 2 ) identification of the most restricted field of radiation possible taking into consideration the assistance provided by modern diagnostic imaging devices in preparing vono basarsi su dati istologici definitivi . 
ci ha ( o dovrebbe avere ) determinato la scomparsa delle prime tre tipologie di rischio nella attivit radioterapia presenti alla nascita e allo sviluppo della disciplina : ( 1 ) trattare un paziente non malato ; ( 2 ) trattare un paziente malato , ma non di cancro ; ( 3 ) trattare in modo errato . poste le condizioni per eliminare il rischio di inappropriatezza dellindicazione al trattamento , resta da analizzare il rischio inerente alle modalit di esecuzione che ancora potenzialmente possibile . 
questo lattuale risk management radioterapico . la invasivit e tossicit di trattamento pu infatti dare origine a tre tipologie di rischio e di conseguente contenzioso : ( 1 ) trattamento radioterapico corretto , ma senza che il paziente sia consenziente e correttamente informato dei rischi e dei possibili effetti collaterali , anche gravi ; ( 2 ) trattamento radioterapico corretto , ma non accompagnato da una soddisfacente risposta terapeutica in termini di controllo della neoplasia e di riduzione o remissione dei sintomi ; ( 3 ) trattamento radioterapico non corretto . per esemplificare la prima tipologia di possibile contenzioso , che attiene alla sfera del consenso informato , si pu considerare la radioterapia radicale della cervice uterina che , alle dosi radianti necessarie per la sua completa efficacia , produce effetti collaterali pi o meno gravi con possibili danni allintestino tenue ed al colon . 
necessario quindi spiegare sempre al paziente le conseguenze collaterali della terapia radiante , allo scopo di informarlo e discuterne le possibili alternative terapeutiche , e al fine di avere un consenso informato che dovr prudentemente essere documentato con firma di assenso al fine di evitare una fonte pretestuosa di contenzioso [ 10 ]  . sicuramente le condizioni di ansiet del paziente neoplastico possono allungare i tempi di approccio terapeutico , ed anche le alternative proposte possono provocare latenze , pi lunghe anche del dovuto , prima di iniziare il trattamento radioterapico , ma la mancata comunicazione della prevedibilit e non evitabilit dei possibili danni e delle alternative per limitarli , uno dei motivi pi frequenti fra le possibili cause di contenzioso medico - legale . 
in addition , the definition of patient management protocols for tumour type eliminates , or minimises , the possibility of excessive or insufficient dose , in part associated with variations caused by incorrect positioning . 
specific competence of the radiotherapist for the organ or system being treated has become currently accepted among criteria for treatment quality . in this regard , it is unfortunately realistic to state that the radiotherapy culture , particularly linked to specific technological development , hinders absolute understanding of all diseases and the relative optimal treatment plans by a single operator , and as a result , subspecialties have been developed for individual tumours or homogenous groups of tumours . 
if correctly monitored and performed , all the specific points covered enable risk management in radiotherapy . risk assessment in italy through an analysis of insurance claims cases of unsafe behaviour or real or presumed malpractice in radiotherapy are infrequent and little known . 
this is due to the fact that radiotherapists have not overcome the fear that the study of unsafe behaviour is not aimed at identifying causes underlying the behaviour , unsafe action or injury but , rather , at finding the guilty party . a real appreciation of the phenomenon in italy is therefore not possible owing to the absence of national or regional figures regarding such cases . 
nonetheless , we can indirectly gain insight into the phenomenon and type of services most at risk of litigation through analysis of insurance claims made to the insurance company that , according to an agreement , insures a high number of radiotherapists . materials and methods the analysis of litigation through the use of insurance claims has already been performed in radiodiagnostics on a high number of radiologists , accounting for about 50% of italian radiologists , with highly indicative results [ 13 ]  . 
for radiotherapy , data we analysed refer to a 10 - year period , from 1995 to 2004 , with the number of radiotherapists insured increasing from 123 in 1995 to 256 in 2004 ( table 1 )  . results the number of insurance claims made over the 10 years was f . 
per provare ci esistono modalit per analizzare a posteriori , indipendentemente dal risultato terapeutico , la correttezza tecnica di un trattamento radioterapeutico ed i fattori di potenziale rischio [ 12 ]  . 
questa rivalutazione fondamentale , in quanto dallanalisi dei veri o presunti errori che si pu attuare una vera opera di risk management . i criteri per valutare la correttezza del trattamento sono : ( 1 ) la corrispondenza del piano terapeutico elaborato per la somministrazione della dose radiante e la sua esecuzione tecnica da parte del tsrm ; ( 2 ) lindividuazione del campo di irradiazione pi ridotto possibile in considerazione dellaiuto , per lelaborazione del piano di trattamento e di centratura , dato oggigiorno dallutilizzo delle pi moderne apparecchiature di diagnostica per immagine ; ( 3 ) la sicurezza nel controllo di qualit delle apparecchiature e lesattezza della dose erogata , di pertinenza del fisico sanitario . fondamentale definire protocolli organizzativi che indichino le modalit con cui procedere alla verifica costante delle apparecchiature identificando anche il responsabile di ogni processo . 
inoltre , la definizione di protocolli di gestione del paziente per tipologia di neoplasia elimina , o riduce al minimo tollerabile , le possibilit di sovradosaggio o sottodosaggio radiante legato anche a variazioni per errato posizionamento . la competenza specifica per organo o apparato da parte del radioterapista ormai opinione acquisita tra i criteri di qualit dei trattamenti . 
a questo proposito purtroppo realistico affermare che la cultura radioterapica , soprattutto legata allo sviluppo tecnologico specifico , impedisca una conoscenza assoluta di tutte le patologie e dei relativi trattamenti ottimali da parte di un singolo operatore , per cui si sono andate sviluppando nel tempo sottospecializzazioni con indirizzo specifico per singole neoplasie o gruppi omogenei delle stesse . tutti gli specifici punti trattati , se correttamente controllati ed eseguiti , consentono la gestione del risk management in radioterapia . valutazione del rischio in italia tramite analisi del contenzioso assicurativo i casi di comportamento rischioso , o di vera o presunta malpractice , in radioterapia sono occasionali e poco conosciuti . non esiste una raccolta nazionale di dati relativi ad errori o danni in radioterapia . ci dovuto al fatto che non stato superato dagli operatori il timore che lo studio dei comportamenti a rischio non sia finalizzato alla individuazione delle cause che hanno f . 
fileni : risk management in radiotherapy table 1 insured radiotherapists table 2 number and cause of insurance claims in radiotherapy insured , n cause year 1995 1996 1997 1998 1999 2000 2001 2002 2003 2004 anno 1995 1996 1997 1998 1999 2000 2001 2002 2003 2004 tabella 1 radioterapisti assicurati assicurati , n 26 , of which two were made by the same patient for different reasons ( table 2 )  . in five cases , the cause of the claim was unspecified , while in the remaining 21 , motivations were explicit : four cases related to patient death ( three postradiotherapy : one 2 years after treatment and one during the stay in the radiotherapy department ) , and one case regarded a lesion treated that proved not to be a tumour ; in addition to the unmotivated radiotherapy injury , a claim was also made for lack of informed consent to the treatment itself ( dual claim )  . 
the remaining 15 cases related to radiotherapy outcomes of varying nature ( table 3 )  . discussion and conclusions data analysed confirm what was stated above regarding risk management in radiotherapy , that is , risks of radiotherapy treatment ( and therefore risk of litigation ) pertain to the outcome or complications of treatment . 
in addition , the claim made for incorrect treatment of a nontumorous lesion , if shown to be true , demonstrates that there is still the possibility of radiotherapy treatment of a lesion that turns out not to be a tumour ( or caused by incorrect histological diagnosis that led to the unjustified treatment )  . clearly , the insurance claim is a precautionary , but obligatory , act of reporting to the insurance company the beginning of legal action in which the healthcare worker is involved . 
as such , the insurance claim is not an index of guilt or malpractice which can only be confirmed at the various nontumorous lesion death during or after radiotherapy postradiotherapy injury or outcomes not specified failure to obtain consent total cause lesione risultata non tumorale decessi durante o dopo radioterapia danni o esiti post - radioterapia non specificate mancato consenso totale tabella 2 numero e specifica delle denunce assicurative in radioterapia determinato il comportamento , lazione rischiosa o il danno , ma bens a quella di ricercare un colpevole . non vi quindi possibilit di una raccolta di tale casistica in ambito regionale o nazionale per avere la reale dimensione del fenomeno in italia . possiamo , in maniera indiretta , analizzare le denunce assicurative pervenute alla societ assicurativa che , tramite convenzione , assicura un numero elevato di radioterapisti , per avere la percezione del fenomeno e la tipologia delle prestazioni a maggior rischio di denuncia . materiali e metodi lanalisi del contenzioso , utilizzando le denunce assicurative , gi stata effettuata in radiodiagnostica su un elevato numero di radiologi che rappresenta circa il 50% dei radiologi italiani con dati estremamente indicativi [ 13 ]  . 
per la radioterapia , i dati in nostro possesso si riferiscono ad un periodo di 10 anni , dal 1995 al 2004 , con una adesione del numero di radioterapisti che passata dai 123 del 1995 ai 256 del 2004 ( tabella 1 )  . risultati il numero di denunce assicurative pervenute nel decennio di 26 , delle quali due dello stesso paziente per motivi diversi ( tabella 2 )  . 
delle 26 denunce , in 5 non erano specificate le cause mentre nelle restanti 21 , in cui erano specificate le motivazioni , 4 riguardavano decessi di pazienti ( 3 post - radioterapia , dei quali 1 a due anni dal trattamento , ed 1 durante la degenza in radioterapia ) ; unaltra si riferiva a lesione trattata , ma poi risultata non tumorale , e , oltre al danno da radioterapia non motivata , si denunciava anche il mancato consenso informato al trattamento stesso ( denuncia table 3 reasons for insurance claims due to radiotherapy damage doppia )  . 
fileni : risk management in radiotherapy reasons incorrect dose sores or burns bone marrow damage female genital sphere ( vaginal stenosis , sterility ) pulmonary fibrosis retinal damage osteomyelitis total tabella 3 motivazioni delle denunce per danni radioterapici motivazione errato dosaggio piaghe e ustioni danni midollari sfera genitale fem ( stenosi vag . , sterilit ) fibrosi polmonare danni retinici osteomielite totale stages of the hearing right up to the final sentence but does , however , allow one to assess the scale of the phenomenon . only at the end of legal proceedings , if concluded with a conviction , is there the legal certainty of medical malpractice in the radiotherapy procedure due to either inexperience , carelessness or negligence . the slow pace of the italian legal system and the safeguarding of privacy do not allow us to know the outcome of the insurance claims studied . 
we can , however , state that the number of claims is statistically low ( 1.4% of radiotherapists ) compared with the number of insured physicians and the number of claims , but this does confirm the need highlighted by risk management to carefully follow pretreatment radiotherapy protocols to contain the phenomenon . 
with the elimination of historical causes of error that led to incorrect radiotherapy treatment , thanks to careful observance of protocols , risk management in radiotherapy currently identifies the main source of risk for the patient and the healthcare worker to be side effects induced by treatment . 
in addition , the claim made for radiotherapy treatment of a lesion that proves not to be a tumour , if shown to be true , demonstrates that this is still possible , despite being caused by incorrect behaviour of another specialist and probably with no malpractice on the part of the radiotherapist . discussione e conclusioni i dati rilevati confermano quanto osservato in precedenza nel risk management radioterapico ; cio che i rischi dei trattamenti radioterapici ( e quindi anche delle denunce ) riguardano gli esiti del trattamento e / o le complicanze dello stesso . inoltre la denuncia per trattamento di lesione risultata non tumorale , se provata , insegna che ancora esiste la possibilit di trattamento radioterapico in lesione non tumorale ( o causata da diagnosi istologica errata che ha portato al trattamento risultato non giustificato )  . sicuramente la denuncia assicurativa un atto cautelativo , ma obbligatorio , di segnalazione alla compagnia assicurativa dellapertura di un contenzioso nel quale il sanitario risulta coinvolto . come tale la denuncia assicurativa non un indice di colpa o di prestazione errata che dovr eventualmente essere confermata nei vari gradi di giudizio fino a sentenza definitiva ma consente comunque di valutare le dimensioni del fenomeno . solo al termine dei vari gradi di giudizio , se conclusi con sentenza di condanna , si avr la certezza giuridica della colpa del medico nella prestazione radioterapica , per imperizia , negligenza o imprudenza . la lentezza del sistema giudiziario italiano e la tutela della privacy non ci consentono di conoscere lesito di tali denunce assicurative . possiamo affermare che il numero delle denunce statisticamente basso ( 1 , 4% dei radioterapisti ) correlato al numero dei medici assicurati e al numero delle denunce , ma conferma la necessit , evidenziata dallo studio del risk management , di seguire puntualmente i protocolli pre - trattamento radioterapico al fine di contenere il fenomeno . 
lagalla sezione di diagnostica per immagini , dipartimento di biotecnologie mediche e medicina legale , policlinico universitario , via del vespro 127 , i - 90127 palermo , italy , correspondence to : t.v. 
thirteen patients with histologically proven gist ( size : 430 cm ; mean : 9 cm ) underwent 40 - slice mdct after the ingestion of 1 , 000 ml of water . 
seven out of 13 gists were located in the jejunumileum , 3 / 13 in the stomach , 2 / 13 in the rectum and in one case , the origin remained unknown . 
thirteen out of 13 exhibited inhomogeneous enhancement due to areas of necrosis and cystic degeneration . direct invasion to adjacent organs ( n = 3 ) , ascites ( n = 3 ) , and liver ( n = 1 ) and peritoneal ( n = 1 ) metastases were also detected . 
tredici pazienti affetti da tgis ( dimensioni : 430 cm ; media : 9 cm ) istologicamente confermati sono stati sottoposti a tcmd con una unit 40 - strati , previa assunzione per os di 1000 ml di acqua , prima e dopo somministrazione ev di 120 ml di mdc iodato . 
le immagini sono state esaminate in consenso da due esperti radiologi valutando , per ciascuna lesione , sede , dimensioni , margini , densit , tipologia di crescita e aspetto contrastografico , nonch leventuale presenza di ascite , linfadenopatie , invasione loco - regionale e / o a distanza . 
in prevalenza , i tgis presentavano margini netti e regolari ( 10 / 13 ) , sviluppo extraluminale ( 11 / 13 ) ed un aspetto contrastografico disomogeneo ( 13 / 13 )  . 
la tcmd consente un ottimale bilancio preoperatorio dei tgis , fornendo elementi utili per la loro caratterizzazione . parole chiave tumore gastrointestinale stromale tratto gastrointestinale tc tumori introduction introduzione gastrointestinal stromal tumours ( gists ) are relatively uncommon mesenchymal neoplasms ( 0.1%3% of all gastrointestinal neoplasms ) that originate in the muscularis propria [ 1 ]  . 
in particular , they account for 1%3% of gastric tumours , 20% of small - bowel tumours and 0.2%1% of coli tumori stromali del tratto gastro - intestinale ( tgis ) sono neoplasie mesenchimali nel complesso poco frequenti 0 , 1%3% di tutte le neoplasie gastrointestinali che traggono origine dalla tonaca muscolare propria [ 1 ]  . 
among these , mitotic index , size and site of origin are especially important , with prognosis being worse for tumours with intestinal rather than gastric origin [ 3 ]  . 
although small - bowel enema may depict the endoluminal component of the tumour , computed tomography ( ct ) is able to accurately demonstrate both wall involvement and extraparietal growth , including possible invasion of adjacent structures or the presence of metastatic lesions [ 47 ]  . 
recent studies have shown that the introduction of multidetector ct ( mdct ) can be useful both in characterising gist through depiction of the exophytic component and in evaluating extent of disease through detection of possible distant metastasis or vascular invasion [ 7 , 8 ]  . 
the aim of this study was to describe the ct features of gists studied by mdct ( 40 - slice ) and evaluate the contribution of the technique to preoperative assessment . materials and methods patients and lesions after obtaining approval from our institutions ethics committee , we retrospectively reviewed the ct studies of 13 patients , eight men and five women , aged between 25 and 75 ( mean : 54.6 ) years with a diagnosis of gastrointestinal stromal tumour confirmed by surgical excision and / or biopsy and immunohistochemistry . 
twelve patients had a nonspecific clinical presentation with diffuse abdominal pain ( n = 7 ) , sense of weight in the abdomen ( n = 4 ) , palpable mass ( n = 2 ) , anaemia ( n = 5 ) , haematemesis ( n = 1 ) , melaena ( n = 1 ) and retrosternal pyrosis ( n = 1 )  . 
before the ct study , all patients gave their written informed consent . examination technique ct images were available on our institutes pacs ( impax , agfa - gevaert , milan , italy ) and had been obtained with a multidetector ( 40 - slice ) philips brilliance scanner ( royal philips electronics , andover ma , usa ) using the following study technique : after distending the gastrointestinal tract with 1 , 000 ml of oral water to ensure correct visualization of the vascular tree on the three - dimensional ( 3d ) reconstructions , we made volumetric acquisitions before and after intravenous administration of 120 ml of water - soluble iodinated nonionic contrast material ( iomeron 400 , bracco spa , milan , italy ) infused at a rate of 34 ml / s via a 18 - gauge needle cannula in an antecubital vein of the right arm ; scan delay was about 70 s . 
technical parameters were as follows : 120 kev ; 380 mas ; collimation 400.625 ; slice thickness 0.9 mm ; increment 0.7 mm ; pitch 1.2 ; gantry rotation time 420 ms ; matrix 512512 ; reconstruction algorithm 180 . 
sebbene gi il clisma del tenue possa evidenziare la componente endoluminale del tumore , la tomografia computerizzata ( tc ) in grado di dimostrare compiutamente sia il coinvolgimento di parete che laccrescimento extra - parietale , incluse leventuale invasione delle strutture anatomiche contigue o la presenza di localizzazioni metastatiche [ 47 ]  . 
recenti studi hanno indicato come lintroduzione delle unit tc multidetettore ( tcmd ) possa risultare utile ai fini sia della caratterizzazione , mediante il riconoscimento della componente esofitica , sia di un corretto bilancio destensione , valutando leventuale presenza di metastasi a distanza o di invasione vascolare [ 7 , 8 ]  . 
scopo di questo lavoro stato quello di descrivere gli aspetti dei tgis studiati con tc multidetettore ( 40 - strati ) e di valutare il contributo di questultima nel bilancio preoperatorio . materiali e metodi pazienti e lesioni ottenuta lapprovazione da parte del comitato etico istituzionale , sono stati valutati retrospettivamente gli esami tc di 13 pazienti , 8 uomini e 5 donne , con et compresa tra 25 e 75 anni , ( et media 54 , 6 anni ) , giunti alla nostra osservazione presso la sezione di scienze radiologiche delluniversit degli studi di palermo e affetti da neoplasie stromali gastrointestinali , confermate mediante escissione chirurgica e / o biopsia e analisi immunoistochimica . 
dodici pazienti presentavano un quadro clinico aspecifico , caratterizzato da dolore addominale diffuso ( n = 7 ) , senso di peso in sede addominale ( n = 4 ) , massa palpabile ( n = 2 ) , anemia ( n = 5 ) , ematemesi ( n = 1 ) , melena ( n = 1 ) e , infine , pirosi retrosternale ( n = 1 )  . 
prima dellesecuzione dello studio tc tutti i pazienti hanno fornito il loro consenso informato sotto forma scritta . tecnica desame la documentazione tc era disponibile sul sistema pacs in dotazione alla nostra istituzione ( impax , agfa - gevaert , milano , italia ) ed stata ottenuta con apparecchiatura multidetettore ( 40 - strati ) philips brilliance ( royal philips electronics andover , mass . , usa ) mediante la seguente tecnica di studio : previa distensione del tratto gastroenterico con 1000 ml di acqua per os al fine di non interferire con la corretta visualizzazione dellalbero vascolare con le tecniche di ricostruzione tridimensionale , sono state effettuate acquisizioni volumetriche prima e dopo somministrazione endovena ed work station ( royal philips electronics ) to visualise axial , multiplanar reconstruction ( mpr ) , maximum intensity projection ( mip ) and 3d volume rendering ( vr ) images . image analysis images were evaluated in consensus by two expert radiologists ( with over 15 years experience in abdominal radiology ) blinded to the histological diagnoses . 
 clinical , laboratory and histological investigations were saved separately and used for statistical evaluation using the chi - square and fischer exact test , with statistical significance established at p < 0.05. reference standard definitive diagnosis was obtained by surgical excision in 11 cases and biopsy and subsequent histological typing ( cd117 positivity ) in the remaining two cases [ 1 ]  . results results are summarised in table 1 . 
in order of frequency , 7 / 13 gists ( 53.8% ) were located in the jejunum - ileum , 3 / 13 ( 23% ) in the stomach and 2 / 13 ( 15.4% ) in the rectum ; in the remaining case , mdct was unable to identify the site of origtumour size ranged from 4 cm to 30 cm ( mean : 9 cm )  . most gists ( 11 / 13 ) were of medium size ( > 5 cm and < 10 cm ) ; one was larger than 10 cm , and one was smaller than 5 cin 76.9% of cases ( 10 / 13 ) , the gist had well - defined , sharp margins whereas in the remaining 23.1% ( 3 / 13 ) , the margins were ill defined and irregular . 
sono stati utilizzati i seguenti parametri tecnici : 120 kev ; 380 mas ; collimazione 400 , 625 ; spessore di strato 0 , 9 mm ; incremento 0 , 7 mm ; pitch 1 , 2 ; tempo di rotazione 420 ms ; matrice 512512 ; algoritmo di ricostruzione 180 . 
in 3 / 13 ( 23% ) cases , the tumour appeared to be in close contact with adjacent organs , as there was no clear cleavage plane , and in particular with the bladder dome , small - bowel loops , sigmoid colon and uterus . 
the absence of vascular involvement was confirmed at surgery in 11 cases whereas in the remaining two cases both nonresectable , prevalently giuno - ileale , 3 / 13 ( 23% ) in sede gastrica ed 2 / 13 ( 15 , 4% ) in corrispondenza del retto , mentre nel rimanente caso non stato possibile , allo studio tcmd , identificare con esattezza la sede dorigine . 
la maggioranza dei tgis osservati ( 11 / 13 ) presentava dimensioni intermedie ( > 5 cm e < 10 cm ) ; 1 tgis superava i 10 cm , mentre il rimanente era inferiore a 5 cnel 76 , 9% dei casi ( 10 / 13 ) i tgis presentavano margini netti e definiti , mentre , nel rimanente 23 , 1% ( 3 / 13 ) , erano sfumati ed irregolari . 
in condizioni di base tutte le lesioni presentavano densit disomogenea e , in extraluminal tumours analysis was limited to the images obtained in the portal phase only . liver metastases ( n = 9 ) with a diameter of 0.520 mm and hypervascular appearance in the arterial phase were detected in one case whereas 3 / 13 ( 23% ) patients had minimal ascites in perihepatic locations ( two cases ) and the pouch of douglas ( one case )  . 
no statistically significant correlations were identified between onset of gist and clinical , laboratory or histological parameters . discussion gists are rare gastrointestinal mesenchymal tumours made up of spindle , epithelioid or , more rarely , pleomorphic cells that present a tyrosine - kinase receptor for growth factor cd117 or c - kit , which is useful for histological characterisation [ 9 ]  . 
some authors have reported an increased risk of gist in patients with type i neurofibromatosis , in whom the neoplasm tends to be multifocal , whereas no correlation has been demonstrated with race , gender or occupation [ 4 ]  . 
this observation , at least as concerns the last two variables , was confirmed by our experience . reported sites of origin are , in order of frequency , stomach ( 60% ) , small bowel ( 30% ) , colon - rectum ( 5% ) and oesophagus ( < 5% )  . 
in our series , however , the majority of lesions ( 7 / 13 ) originated in the small - bowel loops , few in the stomach or rectum , and none in the colon or oesophagus . 
this discrepancy is probably connected to the relative rarity of the tumour and consequently to the small number of patients that can be investigated in a single - centre study such as ours . moreover , the higher incidence of small - bowel gists in our series may also related to the considerable size ( 610 cm ) of the majority of tumours observed . in most cases , gists are asymptomatic . 
however , the presence of clinical symptoms , even if variable and nonspecific , is often correlated with the finding of large tumours , which carry a poor prognosis and tend to recur after surgical excision [ 3 , 8 ]  . 
the tumours in our series had a mean diameter of 9 cm , and 12 / 13 patients had clinically appreciable symptoms and signs whereas in the remaining patient , the tumour was discovered incidentally during abdominal ultrasound . 
the clinical picture was totally nonspecific and characterised by abdominal pain ( 7 / 13 cases ) ; this was associated with a sense of weight in four cases and correlated with an exophytic growth pattern observed in six patients , two of whom had a palpable abdominal mass . 
in 3 / 13 ( 23% ) casi la massa tumorale assumeva rapporti di stretta contiguit , senza la presenza di sicuri piani di clivaggio , con gli organi adiacenti costituiti , in particolare , dalla cupola vescicale , alcune anse del piccolo intestino , sigma e utero . 
in accordo con i dati di letteratura , secondo i quali i tgis si manifestano pi frequentemente in soggetti di et media compresa tra i 50 e i 60 anni , nella nostra casistica let media risultata pari a 56 anni [ 2 ]  . 
alcuni autori riportano un rischio maggiore di sviluppare un tgis nei pazienti affetti da neurofibromatosi di tipo 1 nei quali , peraltro , tale neoplasia si manifesterebbe in forma multifocale , mentre , di contro , non stata finora dimostrata alcuna correlazione con la razza , il sesso o lattivit lavorativa [ 4 ]  . 
1a - c extraluminal gastric gastrointestinal stromal tumour ( gist ) in a 68 - year - old man with abdominal paa transverse unenhanced computed tomography ( ct ) scan shows a well - defined and homogeneous mass arising from the stomach , with extraluminal growth ( arrows )  . 
a unenhanced axial multidetector computed tomography ( mdct ) scan shows a slightly inhomogeneous intraluminal mass with well - defined borders arising from the inner wall of the greater curvature and extending to the lesser curvature ( arrow )  . 
a scansione assiale precontrastografica dimostrante una massa a sviluppo endofitico , a margini netti e sfumatamente disomogenea , che origina dalla parete della grande curvatura gastrica estendendosi allinterno del lume sino alla piccola curvatura ( freccia )  . 
pi raramente , i tgis possono coinvolgere direttamente lomento , il mesentere o il retroperitoneo [ 4 , 9 , 10 ]  . a differenza di quanto appena riportato , nella nostra serie la maggioranza delle lesioni ( 7 / 13 ) aveva come sede dinsorgenza le anse del piccolo intestino , mentre le sedi gastrica e rettale hanno presentato unincidenza minore . 
tale discrepanza , verosimilmente , da mettere in relazione alla relativa rarit della lesione e , di conseguenza , al limitato numero di pazienti che possibile esaminare in uno studio fig . 
3a - c extraluminal invasive gastrointestinal stromal tumours ( gist ) of unknown origin in a 60 - year - old man with a palpable abdominal mass and suffering from diffuse abdominal paa axial unenhanced multidetector computed tomography ( mdct ) reveals a bulky , irregular and inhomogeneous tumour ( arrows )  . 
b contrast - enhanced mdct shows the mass to be mainly hypodense in comparison with adjacent muscles and in close contact with the left kidney which appears dislocated and some bowel loops . 
b dopo somministrazione di mdc iodato , la massa si presenta ipodensa rispetto ai piani muscolari adiacenti e contrae stretti rapporti di contiguit con il rene sinistro che appare dislocato e alcune anse del piccolo e del grosso intestino . 
inoltre , la maggior frequenza di tgis a sede nel piccolo intestino riscontrata nella nostra casistica pu anche essere posta in relazione alle considerevoli dimensioni ( tra 6 e 10 cm ) della maggior parte dei tumori osservati . nella maggioranza dei casi , i tgis non si associano ad alcun sintomo . 
tuttavia , la presenza di una sintomatologia clinica , ancorch variabile ed aspecifica , risulta spesso correlata al riscontro di eteroplasie voluminose , le quali non godono di una prognosi favorevole e tendono a recidivare dopo escissione chirurgica [ 3 , 8 ]  . 
nella nostra serie , caratterizzata da lesioni con un diametro medio pari a 9 cm , un apprezzabile quadro clinico risultato presente in 12 / 13 pazienti , mentre nel rimanente caso il riscontro della massa tumorale stato del tutto occasionale , essendo avvenuto durante lesecuzione di un esame ecografico addominale . 
il quadro clinico , peraltro del tutto aspecifico , risultato caratterizzato in primo luogo ( 7 / 13 casi ) dal dolore addominale , questultimo associato in quattro casi a senso di peso e correlato ad una modalit di crescita di tipo esofitico , riscontrata in sei di tali pazienti , due dei quali presentavano una massa addominale palpabile . tuttavia , in ulteriori quattro casi a crescita esofitica non era presente alcuna sintomatologia dolorosa . 
tale osservazione potrebbe essere messa in relazione al diametro medio pi piccolo ( 6 , 7 cm ) di questultimo gruppo di lesioni rispetto al precedente ( 11 , 8 cm )  . 
lascite , descritta nella nostra serie in tre casi , un reperto occasionale , suggerendo che , in genere , questi tumori non sono responsabili di una significativa reazione flogistica [ 1 ]  . 
le metastasi sono unevenienza meno infrequente ( fino al 50% dei casi allesordio ) ma , qualora presenti , esse possono presentarsi con aspetto prevalentemente ipervascolare e si localizzano pi frequentemente in sede epatica e peritoneale , come nei casi da noi riportati , mentre raro il loro riscontro in sede retroperitoneale , pleurica , polmonare , ossea e sottocutanea [ 1 , 2 , 6 , 9 , 11 ]  . a tale proposito , mentre alcuni autori ritengono sufficiente lacquisizione delle scansioni tc nella sola fase portale , altri , invece , preferiscono anche lacquisizione di una fase arteriosa epatica perch convinti che possa portare ad un miglioramento nella detezione di quella quota parte di metastasi epatiche che appaiono riccamente vascolarizzate , come nel caso da noi descritto [ 6 ]  . 
in nessun paziente stata da noi evidenziata la presenza di coinvolgimento linfonodale , reperto peraltro a tal punto incostante da non giustificare lesecuzione routinaria di una linfoadenectomia in tali pazienti [ 12 ]  . tuttavia , il coinvolgimento linfonodale , loco - regionale o a distanza , rientra tra i criteri classificativi impiegati per definire la prognosi di tali tumori , tra i quali ricordiamo lindice mitotico , la sede , le dimensioni , i margini , la gi descritta modalit di crescita o il comportamento dopo somministrazione ev di mdc , come ad esempio la dimostrazione di fenomeni degenerativi intralesionali [ 3 , 13 , 14 ]  . 
4a - c peritoneal metastasis from rectal gastrointestinal stromal tumour ( gist ) in a 33 - year - old woman with a palpable abdominal mass and suffering from diffuse abdominal paa contrast - enhanced axial multidetector computed tomography ( mdct ) reveals a huge , well - defined and inhomogeneous mass ( arrows )  . 
a tali fini la tc , grazie alla sua panoramicit e alla possibilit di consentire un pi accurato studio della parete viscerale , rispetto ad esempio al clisma del tenue , si rivelata un mezzo particolarmente utile per poter indirizzare il paziente ad un adeguato trattamento , sia esso chirurgico o chemioterapico [ 15 ]  . limpossibilit , infatti , di definire chiaramente i margini della lesione o la dimostrazione tc dellinvasione degli organi contigui o di metastasi a distanza consentono di indirizzare il trattamento , anzich alla chirurgia , verso una terapia farmacologica con glivec [ 2 , 46 ]  . 
in particolare , la nostra esperienza suggerisce che la qualit delle ricostrumatemesis , melaena and retrosternal pyrosis in two cases . ascites , seen in three cases in our series , is an uncommon finding , suggesting that these tumours do not generally produce a significant inflammatory reaction [ 1 ]  . 
metastases are less uncommon ( up to 50% of cases at presentation ) but , when present , appear prevalently hypervascular and often involve the liver and peritoneum , as seen in our series . 
on this subject , whereas some authors consider portal - phase scans sufficient , others prefer to acquire images in the hepatic arterial phase as well , as they believe this improves detection of richly vascular hepatic lesions , as in the case described in our study [ 6 ]  . 
none of the patients in our series had nodal involvement , a finding that is so inconstant that routine lymphadenectomy is not justified in these patients [ 12 ]  . 
nevertheless , locoregional or distant nodal involvement is one of the criteria for defining the prognosis of these tumours ; others include mitotic index , site , size , margins , growth pattern or behaviour after i.v. 
administration of contrast material , as well as demonstration of internal degenerative changes [ 3 , 13 , 14 ]  . about 30% of tumours smaller than 6 cm cause symptoms and signs and show malignant behaviour [ 8 ]  . 
it follows that early diagnosis and accurate staging are extremely important for planning appropriate treatment and improving prognosis . in this context , the panoramic capabilities of ct and its ability to visualise the visceral wall more accurately than , for example , small - bowel enema , have made the technique particularly useful in selecting the most appropriate treatment , whether that be surgery or chemotherapy [ 15 ]  . 
inability to clearly define lesion margins or the ct demonstration of invasion of adjacent organs or distant metastasis will orient the decision towards pharmacological therapy with glivec rather than surgery [ 2 , 46 ]  . 
our experience suggests that the high - quality mpr , mip and 3d vr images obtained with the recent isotropic mdct scanners enable evaluation of the complete abdominal vascular tree especially the more distal branches with mip while providing concise views that are particularly appreciated by clinicians and surgeons for preoperative planning [ 2 ]  . most tumours observed in our study were well - circumscribed masses , which were found at histology to be confined to the serosa . 
however , even when these tumours do display malignant behaviour , as seen in our experience , they tend to preserve relatively well - defined , lobulated margins or give rise to fingerlike extensions rather than infiltrate the surrounding organs in an irregular fashion . 
however , the patients clinical history and some ct signs may provide useful information , thanks to the ready depiction of exophytic or intraand extraparietal dumbbell growth patterns [ 17 ]  . 
carcinomas , for example , tend to give rise to luminal stenosis or substenosis ; they have irregular margins , strongly inhomogeneous enhancement and marked tendency towards contiguous and distant nodal and visceral invasion . 
lymphomas , like carcinomas , produce concentric stenosis of the lumen or form bulky masses , which become ulcerated , extend to the adjacent mesentery , and often involve locoregional and distant lymph nodes . 
as regards differentiation with other mesenchymal tumours such as leiomyomas , leiomyoblastomas , leiomyosarcomas , schwannomas and neurofibromas useful diagnostic data will generally be provided by immunohistochemistry and electronic microscopy [ 7 ]  . 
however , even in this case , tumour site may provide some indication , given that leiomyomas commonly develop in the oesophagus and remain confined within the wall [ 10 ]  . 
negative attenuation values on nonenhanced ct scans may indicate the presence of fat , suggesting a diagnosis of gastric lipoma [ 18 ]  . there are some limitations to our study . 
tali tumori , tuttavia , anche quando presentino caratteri di invasivit , cos come riscontrato nella nostra esperienza , pi che infiltrare gli organi circostanti in modo irregolare , tendono a mantenere dei margini abbastanza ben definiti , lobulati , o a produrre delle espansioni digitiformi . 
queste caratteristiche , tra laltro , ne rendono pi semplice lescissione chirurgica [ 12 ]  . nella nostra serie , la maggioranza delle lesioni osservate ha mostrato un aspetto contrastografico disomogeneo , attribuibile alla presenza di aree di necrosi , di emorragia o di degenerazione cistica . per quanto attiene la diagnosi differenziale con le altre neoplasie che originano nellapparato gastro - intestinale , essa non infrequentemente risulta difficoltosa e , spesso , di pertinenza dellanatomo - patologo . 
tuttavia , la storia clinica del paziente e alcune caratteristiche semeiologiche dellindagine tc possono fornire utili indicazioni a tale fine , grazie allagevole riconoscimento della modalit di crescita esofitica o intraed extra - parietale a clessidra [ 17 ]  . 
i carcinomi , ad esempio , tendono a determinare pi frequentemente la stenosi o la sub - stenosi del lume , hanno margini irregolari , captazione fortemente disomogenea del mdc , una spiccata tendenza allinvasivit linfonodale e viscerale , contigua e a distanza . i linfomi , cos come i carcinomi , determinano pi frequentemente una stenosi concentrica del lume del viscere o la formazione di masse di dimensioni notevoli che tendono ad ulcerarsi , oltre che ad estendersi al mesentere contiguo , comportando , inoltre , un frequente coinvolgimento linfonodale loco - regionale e a distanza . i carcinoidi si localizzano solitamente in corrispondenza dellileo terminale determinando anche una reazione desmoplasica locale . 
per quanto pi propriamente riguarda , invece , la diagnosi differenziale con le altre neoplasie di origine mesenchimale quali leiomiomi , leiomioblastomi , leiomiosarcomi , schwannomi e neurofibromi sono sostanzialmente limmunoistochimica e la microscopia elettronica a fornire utili elementi diagnostici [ 7 ]  . tuttavia , anche in questo caso la sede del tumore pu fornire qualche indizio , infatti i leiomiomi sono neoplasie pi frequenti a livello esofageo , dove rimangono spesso confinati nello spessore della parete [ 10 ]  . 
valori densitometrici intralesionali negativi in condizioni di base possono testimoniare la presenza di grasso , suggerendo la diagnosi di lipomi gastrici [ 18 ]  . il nostro studio presenta dei limiti e , in particolare , la sua natura retrospettiva ha comportato limpossibilit di analizzare , tranne che in un caso , le immagini in fase arteriosa . 
as a result , vascular invasion was assessed on the basis of the portal - venous phase alone and the absence of a fat plane separating the lesion from the vessel ; in addition , identification of hypervascular liver metastases was limited by the possibility that these appear isodense to the surrounding liver parenchyma in the portal phase and therefore go undetected [ 9 ]  . in conclusion , mdct provides an important contribution to the staging of gists before treatment , as it is able to identify small , typically hypervascular , liver metastases that , together with peritoneal metastases , are crucial for correct staging of the disease . 
zompatori , sezione di diagnostica per immagini , padiglione barbieri , ospedale maggiore di parma , via gramsci 14 , i - 43100 parma , tel . : + 39 - 0521 - 703432 , e - mail : maurizio.zompatori@unipr.it received : 20 january 2006 / accepted : 20 february 2006 / published online : 29 june 2006 abstract up to now , neither chest radiograph nor high - resolution computed tomography ( hrct ) has much to offer to the diagnosis of patients with chronic bronchitis ( cb )  . 
a lot of hrct findings can be observed , but they cannot be regarded as specific for pure cb . their evaluation is often subjective , and measurements are poorly reproducible . 
a better comprehension of the large airways abnormalities is important because it is likely that the same pathophysiologic process that causes small - airway obstruction also takes place in larger airways , where it has less functional effect . key words chronic bronchitis chronic obstructive pulmonary disease smoking emphysema riassunto fino ad ora n la radiografia del torace , n la tomografia computerizzata ad alta risoluzione ( hrtc ) hanno contribuito molto alla diagnosi di bronchite cronica ( bc )  . 
lispessimento delle pareti bronchiali dovrebbe essere considerato un reperto non sensibile oltre che non specifico ; la bc non dovrebbe essere equiparata solamente ad un ispessimento delle pareti bronchiali visto che lo spessore pu variare attraverso i diversi stadi di sviluppo della malattia . usando la tc volumetrica a strato sottile , si possono notare frequentemente delle piccole fossette lungo la superficie interna dei bronchi centrali nei pazienti con bc . 
importante una miglior comprensione delle alterazioni a carico delle grandi vie aeree , poich il processo pato - fisiologico sembra essere lo stesso di quello che causa lostruzione a livello delle piccole vie , anche se con conseguenze ridotte dal punto di vista funzionale . parole chiave bronchite cronica affezione ostruttiva polmonare cronica fumo enfisema chronic bronchitis ( cb ) is a clinical diagnosis characterized by chronic productive cough on most days during at least three consecutive months for not less than two consecutive years , after having excluded other causes of chronic cough , such as bronchiectasis or tuberculosis [ 1 ]  . 
the mucuscontaining exudate produced by inflammatory response la diagnosi di bronchite cronica ( bc ) clinica e si basa sulla presenza di tosse cronica produttiva per pi di tre mesi e per almeno due anni consecutivi , dopo aver escluso altre cause di tosse cronica come le bronchiectasie e la tubercolosi [ 1 ]  . 
cb may precede or accompany pulmonary emphysema . pure cb is not necessarily associated with functional impairment , but reduced expiratory flow is often present , usually increased by the coexistent emphysema and bronchiolitis . 
obstruction , which is usually concentrated in small airways , has both reversible components ( mucous plugging , smooth muscle hypertrophy ) and irreversible ones ( fibrosis and stenosis ) [ 2 ]  . 
the main pathologic changes are always described in the mucus - secreting elements : hypertrophy and hyperplasia of the bronchial glands , which develop enlarged ducts , and goblet - cell hyperplasia . 
the enlargement of mucous glands can be measured histologically using different indexes , such as the time - honoured reid index , which is the ratio of gland thickness to bronchial wall thickness measured from the epithelial basement membrane to the perichondrium [ 4 ]  . 
the reid index correlates rather well with the severity of mucous hypersecretion [ 5 ] , but there is overlap between normal subjects and patients with cb [ 6 ]  . 
the absolute increase in gland thickness is small , and the mean reid index in the unselected adult population is 0.35 mm ( range : 0.260.44 ) and in cb is 0.51 mm ( range : 0.430.59 ) [ 7 ]  . 
 [ 11 ] , using chest x - ray , were able to demonstrate that the wall thickness of the bronchi visualized end - on in the parahilar regions is of limited value in distinguishing patients with cb from normal subjects . 
the increased lung markings give rise to the appearance of so - called dirty lung , though we currently know that it can also be related to other smoking - related diseases , such as respiratory bronchiolitis with interstitial lung disease [ 12 , 13 ]  . 
la bc non necessariamente associata ad una modificazione funzionale , sebbene una alterazione dei test di funzionalit respiratoria di tipo ostruttivo sia di frequente riscontro , incrementata soprattutto dalla concomitante presenza di enfisema e bronchiolite . 
lostruzione , che principalmente causata dalla patologia delle piccole vie aeree , presenta aspetti sia di tipo reversibile ( tappi mucosi , ipertrofia della muscolatura liscia delle pareti bronchiali ) che di tipo irreversibile ( fibrosi e stenosi ) [ 2 ]  . 
specifiche correlazioni patologiche con la sindrome clinica propria della bc sono difficili da reperire . sebbene alcuni pazienti con bc possano non dimostrare alcuna anormalit istologica , la maggior parte di essi presenta modificazioni a carico delle vie aeree di medio - grande calibro ; in alcuni casi di bc il processo infiammatorio si estende fino a coinvolgere anche i bronchioli pi piccoli [ 3 ]  . le principali alterazioni patologiche si osservano a carico degli elementi muco - secernenti : ipertrofia e iperplasia delle ghiandole bronchiali con dilatazione dei dotti e iperplasia delle cellule caliciformi . lingrandimento delle ghiandole mucose pu essere misurato su preparati istologici ricorrendo a diversi indici , il pi noto dei quali lindice di reid che corrisponde al rapporto tra lo spessore della ghiandola bronchiale e lo spessore della parete bronchiale misurato dalla membrana basale al pericondrio [ 4 ]  . 
lindice di reid si correla significativamente con la gravit dellipersecrezione mucoide [ 5 ] , ma esiste una certa sovrapposizione tra i valori riscontrati in individui asintomatici ed in pazienti affetti da bc [ 6 ]  . 
laumento assoluto dello spessore ghiandolare di minima entit e lindice di reid nella popolazione generale in et adulta pari in media a 0 , 35 mm ( range : 0 , 260 , 44 ) mentre , nei bronchitici cronici , in media pari a 0 , 51 mm ( range : 0 , 430 , 59 ) [ 7 ]  . altri reperti patologici includono : infiltrato di cellule infiammatorie croniche a livello della mucosa bronchiale , metaplasia squamosa epiteliale , ipertrofia muscolare liscia delle pareti bronchiali e bronchiolite cronica . 
la presenza di atrofia cartilaginea , di esiti cicatriziali e di tratti stenotici bronchiali alternati ad altri dilatati , pu essere inoltre riscontrata negli stadi pi avanzati della malattia . fino ad ora n la radiografia del torace , n la tomografia computerizzata ad alta risoluzione ( hrtc ) hanno contribuito molto alla diagnosi di bc . 
furthermore , an objective evaluation of bronchial wall thickness is difficult to obtain ; airways measurements are influenced by the angle between the bronchial long axis and the plane of section and by other variables , such as lung volume and window settings . 
dedicated softwares may provide more objective measurements , but they are not widely available and might still overestimate wall thickness , underestimating the luminal area as well as the inner diameter [ 16 , 17 ]  . 
although patients with emphysema had significantly lower mean lung attenuation at 90% of vital capacity than normal subjects or patients with cb , attenuation was the same for normal subjects and patients with cb [ 18 ]  . variable emphysema extents can be seen ( centrilobular and / or paraseptal ) , and emphysema may be the predominant feature in patients with symptoms of cb . 
as would be expected , evidence of air trapping may be identified on expiratory images in patients with cb , mostly due to mast - cell and neutrophil infiltration of the smooth muscle layer in smokers [ 19 ]  . 
in order to better characterise hrct features of cb , further efforts are warranted . firstly , the finding of bronchial wall thickening may even be considered nonsensitive as well as nonspecific ; cb should not only be equated with narrowing of the airway since thickness of the bronchial wall may vary among different stages of development [ 20 , 21 ] : chronic catarrhal bronchitis , chronic catarrhal - fibrotic bronchitis , chronic granulating bronchitis , chronic purulent bronchitis , and chronic fibrotic bronchitis . 
although longitudinal studies are lacking , the bronchial wall might also grow thinner during disease progression , as subjects with more severe emphysema have less airway thickening than those with less severe emphysema [ 16 ]  . although bronchography is almost completely outdated and bronchographic findings are mainly of historic interest , radiologists of the first half of the twentieth century using that technique were able to illustrate a complex and refined set of delle pareti bronchiali ( viste come opacit ad anello o a binario ) e laccentuazione del disegno parenchimale polmonare dovuta alla sovrapposizione delle pareti bronchiali ispessite e alla malattia delle piccole vie aeree [ 8 , 10 ]  . 
 [ 11 ] , utilizzando il radiogramma del torace , furono in grado di dimostrare che la valutazione dello spessore parietale dei bronchi visti di infilata in sede para - ilare scarsamente utile per discriminare tra pazienti normali e pazienti con bc . laccentuazione del disegno parenchimale polmonare nota anche con il termine di polmone sporco , che attualmente sappiamo essere presente anche in pazienti affetti da altre malattie connesse al fumo , come la bronchiolite respiratoria associata a patologia polmonare interstiziale [ 12 , 13 ]  . 
altri segni radiografici associati comprendono : lieve iperinsufflazione polmonare con oligoemia ( usualmente dovuta allenfisema associato ) , trachea a fodero di sciabola , dilatazione del cuore e delle arterie polmonari centrali per ipertensione arteriosa polmonare . non molto si sa dei reperti hrtc riscontrabili nella bc . poich le alterazioni sono localizzate a livello delle vie aeree , le ricerche sono state focalizzate soprattutto sullispessimento delle pareti bronchiali , sebbene questo sia un reperto non specifico [ 14 ]  . 
 [ 14 ] hanno rilevato un ispessimento delle pareti bronchiali in un terzo dei pazienti fumatori , anche se questa alterazione non era comunque specifica , vista la sua presenza nel 18% dei non fumatori . 
inoltre , una misura oggettiva dello spessore delle pareti bronchiali difficile da ottenere ; le misurazioni dipendono dallangolo tra il maggior asse bronchiale ed il piano di scansione assiale e da altre variabili come il volume polmonare e i valori di finestra elettronica . 
alcuni software dedicati potrebbero offrire qualche vantaggio , ma non sono ampiamente diffusi e possono portare a sovrastime dello spessore parietale , sottostimando larea endoluminale ed il diametro interno [ 16 , 17 ]  . misure densitometriche eseguite su esami tc , spirometricamente controllati al 90% e al 10% della capacit vitale , sono state impiegate per distinguere i pazienti con enfisema da quelli con bc ; sebbene i pazienti con enfisema avessero al 90% della capacit vitale valori di attenuazione media polmonare significativamente pi bassi dei pazienti normali o con bc , non vi era differenza tra quelli dei pazienti normali e quelli dei soggetti con bc [ 18 ]  . si possono notare gradi di estensione di enfisema ( centrolobulare e / o parasettale ) variabili , e lenfisema pu essere lalterazione dominante nei pazienti che presentano sintomi di bc . 
come facilmente ci si potrebbe aspettare , la presenza di aree di intrappolamento aereo pu essere evidenziata nelle scansioni espiratorie , soprattutto a causa della infiltrazione infiammatoria di mastociti e neutrofili della muscolatura liscia dei piccoli bronchi dei fumatori [ 19 ] ; questo processo potrebbe progressivamente condurre al rimodellamento permanente delle piccole vie aeree . 
1 la broncografia mostra piccole estroflessioni lungo il bronco lobare medio ( freccia nera ) e superiore di destra ; si osserva inoltre la perdita del nomale affusolamento bronchiale e la dilatazione e lincompleto riempimento delle vie aeree periferiche con terminazioni brusche . 
2 piccola depressione ( freccia nera ) lungo la parete del bronco lingulare in un paziente affetto da bronchite cronica . findings related to cb , which included [ 22 , 23 ] : loss of bronchial tapering , intraluminal secretions ( mucous plugs ) , dilatation or incomplete filling of the peripheral airways with abrupt terminations , excessive collapse during expiration ( or cough ) due to bronchomalacia , accordion - like pattern of the bronchial inner surface due to filling of dilated mucus gland ducts , and pseudodiverticular projections that were analogous to the visualization of paraurethral ducts in cases of urethritis . the latter abnormalities appeared to start as submicroscopic depressions and dilatations of the bronchial gland ducts on the mucosal surface [ 24 ]  . 
3 la ricostruzione coronale a strato sottile mette in evidenza multiple fossette che appaiono come diverticoli lungo il bronco principale di destra . prevalenza della tracheo - broncomalacia non nota ( probabilmente non meno del 10% dei soggetti con bpco )  . 
altri reperti hrtc comprendono : secrezioni endoluminali tracheo - bronchiali , noduli centrolobulari , opacit ad albero in fiore ( tree in bud ) , aree di opacit a vetro smerigliato ( ground - glass ) o zone consolidative dovute alla sovrainfezioni . in sostanza , diversi reperti hrtc possono essere riscontrati , ma essi non possono essere considerati specifici per la diagnosi di bc ; la loro interpretazione spesso soggettiva e le misurazioni sono scarsamente riproducibili . 
innanzitutto , lispessimento delle pareti bronchiali dovrebbe essere considerato un reperto non sensibile oltre che non specifico ; la bc non dovrebbe essere equiparata solamente ad un ispessimento delle pareti bronchiali , visto che lo spessore pu variare attraverso i diversi stadi di sviluppo della malattia [ 20 , 21 ] : bronchite cronica catarrale , bronchite cronica catarrale - fibrotica , bronchite cronica granulomatosa , bronchite cronica purulenta e bronchite cronica fibrotica . 
sebbene manchino studi longitudinali , le pareti bronchiali potrebbero anche assottigliarsi con il progredire della malattia , dato che stato osservato che i soggetti con enfisema pi esteso presentano pareti bronchiali meno spesse di quelli con enfisema meno severo [ 16 ]  . sebbene la broncografia sia ormai quasi completamente dimenticata e i reperti broncografici abbiano un interesse storico , i radiologi operanti nella prima met del xx secolo furono in grado di sviluppare un corpus di segni broncografici collegati alla bc rilevante per raffinatezza e complessit [ 22 , 23 ] : perdita di normale affusolamento bronchiale verso m . 
these signs were observed mostly in the large bronchi of patients with cb although some authors recorded such findings in normal adults as well as in patients affected by tuberculosis and bronchiectasis [ 25 , 26 ]  . 
a better comprehension of large airways abnormalities is important because it is likely that the same pathophysiologic process that causes small - airways obstruction also takes place in larger airways , where it has less functional effect [ 27 ]  . 
although the presence of bronchial pits is rarely challenged , the use of thin - collimations , multiplanar reconstructions and different reconstruction algorithms , such as minimum - intensity projection ( minip ) , are recommended to improve detection of such bronchial abnormalities . 
multiple dilatazioni e depressioni si fondevano fino a creare un diverticolo che erniava attraverso i fasci della muscolatura liscia ; la rottura di questultima determinava quindi la formazione di ampi diverticoli . 
the purpose of this study was to evaluate the efficacy of postoperative radiotherapy in reducing the incidence of prostate carcinoma ( pca ) recurrences after radical prostatectomy ( rp ) , define the importance of the time interval between surgery and radiotherapy for prognosis and the toxicity of the treatment in comparison with radiotherapy or surgery alone . 
the treatment was considered adjuvant if was conducted less than 6 months after rp , if there was no macroscopic residual disease and if there was no progressive increase in serum prostate - specific antigen ( psa ) and salvage if performed more than 6 months after rp , for the presence of macroscopic recurrence or with rising psa . 
the best results are obtained with early postoperative treatment ( adjuvant ) ; adjuvant radiotherapy of high - risk forms yields better results if performed with psa less than or equal to 1 ng / ml . key words prostate carcinoma radical prostatectomy postoperative radiotherapy riassunto obiettivo . 
il trattamento stato considerato adiuvante se condotto meno di 6 mesi dopo pr , se non era presente residuo macroscopico di malattia e in assenza di incremento progressivo dellantigene prostatico specifico ( psa ) serico ; di salvataggio se effettuato pi di 6 mesi dopo pr , per la presenza di malattia macroscopica recidiva o con psa in crescita . 
la sopravvivenza libera da ricadute ( rfs ) a 5 anni e 10 anni risultata rispettivamente pari a 538% e 3214 , 2% per lintera casistica , a 769% e 382 , 7% nel gruppo di pazienti trattati con radioterapia adiuvante e a 3610% e 2810% nei pazienti sottoposti a radioterapia di salvataggio ( p < 0 , 01 )  . 
inoltre , la rfs a 5 anni risultata migliore nel gruppo di pazienti trattati con radioterapia adiuvante e psa inferiore o eguale a 1 ng / ml ( p < 0 , 05 )  . 
i risultati migliori si ottengono con un trattamento precoce dopo chirurgia ( adiuvante ) ; inoltre , la radioterapia adiuvante delle forme ad alto rischio ha migliori risultati se effettuata con psa1 ng / ml . parole chiave carcinoma prostatico prostatectomia radicale radioterapia post - operatoria b . 
however , although radical surgery has proved to be just as effective as radiotherapy alone for intracapsular forms , around 15%40% of patients with stage t1 - t2 prostate cancer develop a recurrence [ 1 , 2 ]  . 
moreover , in about one third of patients with recurrence , the disease progresses to distant metastasis [ 1 , 3 ]  . the risk of local recurrence after prostatectomy alone has been estimated at 15%45% at 5 years in patients with locally advanced prostate carcinoma ( pca ) ( pt3 ) and at 20%60% and 40%65% in the presence of positive margins and involvement of the seminal vesicles . 
it is therefore possible to identify prognostic factors that correlate with a high risk of local recurrence , including preoperative serum prostate - specific antigen ( psa ) , margin positivity , gleason score and clinical and pathological stage . the combination of all of these factors increases the risk of recurrence by around 50% [ 58 ]  . numerous studies have highlighted the efficacy of postoperative radiotherapy in reducing the incidence of local recurrence in high - risk cases [ 911 ]  . 
the timing of radiotherapy is , however , still controversial : is adjuvant or salvage radiotherapy more effective ? adjuvant treatment is generally performed within 6 months of surgery in the presence of positive margins and / or extracapsular spread ; salvage radiotherapy refers to radiotherapy initiated when a macroscopic recurrence appears or with rising psa , generally later than 6 months after surgery . 
 this paper reports the results of a retrospective review carried out on a single - institution case series of 97 patients treated with surgery for pca in order to evaluate the efficacy of postoperative radiotherapy in reducing the incidence of locoregional recurrence , define the best timing for radiotherapy and assess late toxicity of postoperative treatment compared with that seen after radiotherapy alone and after surgery alone . 
it was considered salvage if performed more than 6 months after rp , for the presence of macroscopic disease or progressively rising psa values . patient age was 6070 years in 80% of cases ; 78% of patients had a karnofsky performance status ( ki ) equal to or greater than 80 . 
tuttavia , sebbene la chirurgia radicale si sia dimostrata un trattamento altrettanto efficace della radioterapia esclusiva per le forme intracapsulari , circa il 15%40% dei pazienti portatori di carcinoma prostatico in stadio t1 - t2 sviluppano una recidiva [ 1 , 2 ]  . 
inoltre , circa un terzo dei pazienti con recidiva progrediscono con la comparsa di metastasi a distanza [ 1 , stato stimato che il rischio di ricaduta locale dopo sola prostatectomia pari al 15%45% a 5 anni in pazienti portatori di carcinoma prostatico localmente avanzato ( pt3 ) e rispettivamente al 20%60% ed al 40%65% in presenza di margini positivi e in caso di interessamento delle vescicole seminali . 
possibile , quindi , identificare dei fattori prognostici che si correlano ad un elevato rischio di recidiva locale , tra cui il valore del psa pre - chirurgia , la positivit dei margini , lo score di gleason , lo stadio clinico e patologico . 
lassociazione di tutti questi fattori aumenta il rischio di recidiva di circa il 50% [ 58 ]  . numerosi studi hanno evidenziato lefficacia della radioterapia post - operatoria nel ridurre lincidenza delle recidive locali nei casi ad alto rischio [ 911 ]  . 
risulta , per , ancora controverso il timing radioterapico : pi efficace la radioterapia adiuvante o quella di salvataggio ? il trattamento adiuvante viene in genere effettuato entro sei mesi dalla chirurgia , in presenza di margini positivi e / o di extracapsularit ; mentre considerata di salvataggio la radioterapia iniziata alla comparsa di recidiva macroscopica o con psa in crescita progressiva , in genere oltre i sei mesi dallintervento chirurgico . in questo lavoro vengono riportati i risultati ottenuti dallanalisi retrospettiva di una casistica monoistituzionale di 97 pazienti trattati con chirurgia per carcinoma prostatico , al fine di valutare lefficacia della radioterapia post - operatoria nel ridurre lincidenza delle recidive loco - regionali , definire il timing ottimale della radioterapia e valutare la tossicit tardiva del trattamento post - operatorio , nel confronto con quella che si osserva dopo trattamento radioterapico esclusivo o dopo sola chirurgia . materiali e metodi dal 1980 al 2003 sono stati trattati consecutivamente 97 pazienti portatori di carcinoma prostatico in esiti di prostatectomia radicale ( pr )  . 
il trattamento radioterapico ( rtt ) stato considerato adiuvante se condotto meno di 6 mesi dopo pr e in assenza di malattia macroscopica residua o recidiva locale e di innalzamento progressivo dei valori del psa . 
in 13 patients , this information was not available ( during the first years of the period considered , psa testing was not available at our institution )  . as a result , data analysis for this parameter was done excluding these patients . 
there were no significant differences between the two treatment groups as regards age , ki or gleason score . of the 41 patients treated with adjuvant radiotherapy , only 22% had disease - free surgical margins ; extracapsular spread was present in 80% of cases . 
treatment volume was limited to the surgical bed in 76% of cases , with a total target dose less than 70 gy in 54% of cases . of the 56 patients treated with salvage radiotherapy , 82% had disease - free surgical margins and only 46% had extracapsular spread . 
treatment volume was limited to the surgical bed in 82% of cases , with a total target dose less than 70 gy in 12% of cases only . the main clinical and treatment differences between the two groups undergoing adjuvant and salvage radiotherapy are summarised in table 1 . 
after radiotherapy , patients were followed up by means of psa monitoring and physical examination every 6 months . further investigations ( bone scintigraphy , chest x - ray and prostate ultrasound ) were requested for patients showing rising psa level . 
the appearance of clinically documented disease , local or distant , was considered as the event of interest . comparison between the two groups was carried out with the log - rank test ( cox multivariate analysis being impossible due to the small number of events in the subgroups )  . 
late toxicity of rtt was documented and described according to the radiation therapy oncology group ( rtog ) scale . pi di 6 mesi dopo pr , per la presenza di malattia macroscopica o per innalzamento progressivo del valore del psa . nellintera casistica , let era compresa tra 60 e 70 anni nell80% dei casi ; il 78% dei pazienti presentava un performance status secondo karnosfky ( ik ) maggiore o uguale a 80 . 
in 13 pazienti tale dato non era disponibile ( nei pazienti reclutati nei primi anni del periodo considerato , quando il dosaggio del psa non era disponibile presso la nostra istituzione )  . 
non sono state documentate differenze significative tra i due gruppi terapeutici per ci che concerne et , ik , gleason score . dei 41 pazienti trattati con radioterapia adiuvante , solo il 22% presentava margini chirurgici liberi da malattia ; unestensione extracapsulare era presente nell80% dei casi . la maggior parte dei pazienti ( 68% ) aveva un psa pre - radioterapia inferiore o eguale a 1 ng / ml . 
le principali differenze nella distribuzione dei pazienti nei due gruppi trattati con radioterapia adiuvante e di salvataggio , a seconda delle pi importanti caratteristiche patologiche e terapeutiche sono riassunte nella tabella 1 . 
la grande maggioranza dei casi ( circa l80% ) stata sottoposta anche a trattamento ormonale , senza differenze significative tra i pazienti trattati con radioterapia adiuvante e quelli trattati con radioterapia di salvataggio . 
this finding is more significant if we consider that the total dose was lower in the group treated with adjuvant radiotherapy ( table 1 )  . no significant differences in rfs were observed in relation to gleason score , surgical margin positivity or extracapsular spread either in the series as a whole or in the two subgroups . a preradiotherapy psa level greater than 1 ng / ml was found to correlate significantly with a worse rfs only in the adjuvant radiotherapy group [ 50% vs . 
patients treated with salvage rtt therefore showed table 1 clinical and treatment characteristics of the case series studied analisi statistica lend point principale per lanalisi dei risultati stato la sopravvivenza libera da ricaduta ( rfs ) , calcolata con metodo attuariale di kaplan - meier . 
il confronto tra sottogruppi stato effettuato con il log - rank test ( non essendo possibile impiegare lanalisi multivariata secondo il modello di cox per lesiguit numerica degli eventi nei vari sottogruppi )  . 
la tossicit tardiva del trattamento radioterapico stata documentata e descritta in accordo con la scala del radiation therapy oncology group ( rtog )  . risultati sopravvivenza libera da ricaduta la sopravvivenza attuariale non corretta per altre cause di morte ( os ) a 5 e 10 anni dalla fine della radioterapia e per lintera casistica stata del 75%8% e 26%2% , quella corretta per altre cause di morte ( dss ) dell83%7% e 38%28% , e quella libera da ricadute ( rfs ) del 53%8% e 32%14 , 2% . 
la rfs stata correlata a vari fattori prognostici , tra cui il tipo di radioterapia ( adiuvante o di salvataggio ) , il gleason score , lestensione extracapsulare , la positivit dei margini chirurgici ed il valore del psa pre - radioterapia . 
questo dato assume magadjuvant rtt , % ( n = 41 ) salvage rtt , % ( n = 56 ) rtt , radiotherapy treatment ; psa , prostate - specific antigen ; rt , radiotherapy apsa data available for only 84 / 97 patients ( see text ) tabella 1 caratteristiche cliniche e del trattamento radioterapico della casistica in esame rtt adiuvante , % ( n = 41 ) rtt di salvataggio , % ( n = 56 ) free surgical margins extracapsular spread psa pre - rt 1 ng / mla total dose < 70 gy rtt limited to surgical bed associated hormone therapy margini chirurgici liberi estensione extracapsulare psa pre rt 1 ng / mla dose totale < 70 gy rtt solo letto operatorio ormonoterapia associata rtt , trattamento di radioterapia ; psa , antigene prostatico specifico ; rt , radioterapia ail dato sul psa disponibile solo in 84 / 97 pazienti ( vedi testo ) b . 
only two cases ( 2% ) presented gastrointestinal toxicity ( grade less than or equal to 2 )  . discussion this study evaluated the results of postoperative radiotherapy for prostate cancer and in particular compared adjuvant and salvage radiotherapy . 
non si sono invece osservate differenze significative nella rfs a seconda del gleason score , della positivit dei margini chirurgici , della presenza di malattia extracapsulare , sia nella intera casistica che nei due sottogruppi terapeutici . 
69% , p ( log - rank ) = 0 , 05 ]  . sede e incidenza delle ricadute nellintera casistica si sono verificate 27 ricadute ( 28% ) , cos distribuite : 11 recidive locali , 12 metastasi a distanza , 2 ricadute loco - regionali isolate e 2 associate a metastasi a distanza . 
si osservata una tossicit urinaria in 6 / 97 casi ( 6% ) , in un solo caso ( cistite emorragica ) di grado > 2 secondo la scala rtog . 
solo 2 casi ( 2% ) hanno presentato tossicit gastrointestinale , di grado2 . discussione in questo studio , abbiamo valutato i risultati della radioterapia post - operatoria per il cancro prostatico ed in particolare abbiamo confrontato la radioterapia adiuvante con quella di salvataggio . 
i pazienti sottoposti a radioterapia adiuvante hanno manifestato una miglior rfs rispetto al gruppo di pazienti trattato con radioterapia di salvataggio , con una differenza statisticamente significativa ( p < 0 , 01 )  . 
infatti , nella casistica in esame ( 97 casi ) , abbiamo osservato 27 recidive ( 28% ) : 7 / 41 ( 17% ) nel gruppo della radioterapia adiuvante e 20 / 56 ( 36% ) in quello della radioterapia di salvataggio , nonostante che la dose totale sia stata meno elevata nei pazienti trattati con rtt adiuvante . 
sebbene lanalisi univariata sia stata estesa a tutti gli altri diversi fattori prognostici , anche separatamente nei due diversi sottogruppi terapeutici , la rfs risultata significativamente migliore solo nel gruppo in cui il psa pre - radioterapia era 1 ng / ml , e ci solo nel sottogruppo trattato con radioterapia adiuvante . 
limportanza prognostica del psa pre - rtt stata anche recentemente confermata dalla letteratura [ 12 ] e rappresenta un altro elemento a favore di un precoce inizio della radioterapia post - operatoria nei sottogruppi a rischio . 
our data are therefore in agreement with previous studies that testify to the efficacy of postoperative rtt . these include retrospective studies comparing the results of surgery alone with those of surgery combined with radiotherapy [ 13 ] and , above all , the randomised study of european organisation for research and treatment of cancer ( eortc ) 22911 , which confirms the improvement in biochemical and clinical disease - free survival [ 14 ] with the use of adjuvant postoperative rtt in pt3 cases . 
ours was a retrospective study and therefore suffers some limitations : the groups were not homogeneous , treatment changed over the years and surgical indications have evolved . in our series , radiotherapy was generally well tolerated . late toxicity was acceptable , with only one case of g4 urinary toxicity ( haemorrhagic cystitis )  . there were no major chronic gastrointestinal sequelae . comparison of the late sequelae reported for surgery alone with those observed after postoperative rtt ( in our series and others ) identified no major differences [ 15 ]  . 
likewise , in terms of late sequelae , radiotherapy alone for prostate cancer has similar toxicity to postoperative rtt , as shown by the results of a recent italian multicentre study [ 16 ]  . hormone treatment , with different drugs and duration , was given to the majority of patients receiving either adjuvant or salvage radiotherapy : this precludes any reliable assessment of the therapeutic role of androgen block in our series . 
si tratta sia di studi retrospettivi , in cui si paragonano i risultati della sola chirurgia con quelli in cui si associa al trattamento chirurgico quello radiante [ 13 ] e soprattutto dello studio randomizzato delleortc 22911 , in cui si conferma il miglioramento della sopravvivenza libera da malattia sia biochimica che clinica [ 14 ] con luso della rtt adiuvante postoperatoria nelle forme pt3 . 
il nostro uno studio retrospettivo con tutte le limitazioni correlate : la non omogeneit del gruppo , le modifiche dellapproccio terapeutico in un lungo periodo di tempo e levoluzione delle indicazioni chirurgiche . 
confrontando le sequele tardive della sola chirurgia , documentate in letteratura , con quelle osservate dopo rtt post - operatoria ( in questa come in altre casistiche ) , non si sono osservate differenze sostanziali [ 15 ]  . allo stesso modo , in termini di sequele tardive , il trattamento radioterapico esclusivo del cancro prostatico gravato da una tossicit simile a quella della rtt post - operatoria , come si pu ad esempio osservare considerando i risultati di un recente studio multicentrico italiano [ 16 ]  . 
il trattamento radioterapico adiuvante post - operatorio , tuttavia , trova indicazione solo nelle forme clinicamente intracapsulari che , allesame istologico del pezzo operatorio , risultino extracapsulari o con positivit marginale . 
thirty - two out of 36 patients met the following inclusion criteria : transabdominal and endocavitary ( us ) examination and mr imaging , followed by laparoscopy performed within 2 weeks . 
sensitivity and specificity of the two imaging techniques in the recognition of the different locations were 58% and 25% , respectively , for us and 56% and 50% , respectively , for mr imaging . 
us examination is the primary evaluation in cases of suspected disease and for the rectovaginal septumr examination is recommended for correct classification in doubtful cases and in cases of suspected extrapelvic lesions and adhesions . key words endometriosis magnetic resonance ultrasound riassunto obiettivo . 
sono state studiate consecutivamente 36 pazienti con sospetto o diagnosi clinica di endometriosi . trentadue / 36 pazienti rispondevano ai seguenti criteri di inclusione e sono state comprese in questo studio : esecuzione di indagine eg con approccio sovra - pubico e trans - cavitario , di indagine rm e intervento laparoscopico entro le 2 settimane successive . 
lindagine rm preferibile per la tipizzazione della lesione nei casi dubbi , per lo studio delle localizzazioni extra - pelviche e nel caso di aderenze . parole chiave endometriosi risonanza magnetica ecografia g . 
distinction on the basis of lesion morphology rather than lesion depth justifies the importance that imaging techniques , and in particular magnetic resonance ( mr ) , are assuming in defining different lesion components [ 1 ]  . 
for the same reason , although laparoscopy remains the gold standard in the diagnosis of endometriosis , several recent studies evaluated the role of noninvasive imaging techniques in the attempt to overcome the intrinsic limits of the laparoscopic approach ( evaluation of posterior pelvis ; superficial implants on intestinal loops or the bladder ; localisations in the ureter or rectovaginal septum ; extrapelvic localisations , presence of adhesions ) [ 18 ]  . 
the purpose of this study was to define the real contribution of imaging , in particular ultrasound ( us ) and mr , in diagnosis and local staging of endometriosis by comparing results with those of laparoscopy . materials and methods population between july 2003 and may 2005 ( overall duration 22 months ) , we consecutively evaluated 36 women with suspected or clinically diagnosed endometriosis . 
all patients underwent transabdominal and endocavitary us and mr ( both performed in the preovulatory phase within the 12th day of the menstrual cycle ) and laparoscopy within 15 days from mr without interposition of menstrual cycle . 
patients who did not give informed consent or did not undergo laparoscopy within 2 weeks of the imaging studies were excluded . patients ages ranged from 24 to 51 ( mean 33 ) years ; 18 / 36 patients had previously undergone appendicectomy whereas 17 / 36 had been operated on for endometriosis . 
only 4 / 36 patients had had a pregnancy whereas 4 / 36 were sterile with normal partner spermiogra rectosigmoidoscopy , performed in 21 / 36 patients before surgery , was negative for endometriosis in all cases ; in 7 / 36 patients , it showed hyperaemia of the mucosa due to inflammation , with hyperplastic polyps in two cases . ultrasound us examination was carried out with a transabdominal and lendometriosi una malattia comune nelle giovani donne e si associa a dolore pelvico cronico ed infertilit . 
tale distinzione importante , dal momento che lendometriosi peritoneale e quella ovarica rappresentano lesioni prevalentemente emorragiche , mentre le localizzazioni alla pelvi posteriore , allintestino ed alla vescica rappresentano prevalentemente lesioni di tipo adenomiosico . 
la distinzione delle lesioni sulla base dellaspetto morfologico piuttosto che in relazione alla profondit dellimpianto rende ragione dellimportanza che le metodiche di imaging , in particolare la risonanza magnetica ( rm ) , stanno assumendo nel determinare le componenti lesionali [ 1 ]  . 
 anche per questa ragione , sebbene la laparoscopia rimanga il gold standard nella diagnosi di endometriosi , recentemente numerosi studi hanno valutato il ruolo delle metodiche di imaging non invasivo , nel tentativo di ovviare alle limitazioni intrinseche dellapproccio laparoscopico ( valutazione della pelvi posteriore ; impianti superficiali su anse intestinali o vescicali ; localizzazioni ureterali o nel setto retto - vaginale ; localizzazioni extra pelviche , presenza di adesioni ) [ 18 ]  . scopo di questo studio definire leffettivo contributo dellimaging , in particolare dellecografia ( eg ) e della risonanza magnetica ( rm ) , nella diagnosi e nella valutazione di estensione dellendometriosi , attraverso il confronto dei dati ottenuti mediante tali metodiche con i risultati dellintervento chirurgico laparoscopico cui sono state sottoposte tutte le pazienti considerate . materiali e metodi popolazione in studio nel periodo compreso fra luglio 2003 e maggio 2005 ( durata complessiva 22 mesi ) sono state studiate in maniera consecutiva 36 pazienti giunte alla osservazione con sospetto o diagnosi clinica di endometriosi . 
le pazienti incluse in questo studio sono state sottoposte sia ad indagine eg con approccio sovrapubico e trans - cavitario che ad indagine mr ( espletate nel periodo pre - ovulatorio entro il 12 giorno del ciclo mestruale ) ed a intervento laparoscopico entro 15 giorni dalla esecuzione dello studio mr e senza interposizione di ciclo mestruale . 
i criteri di esclusione sono stati : pazienti che non hanno espresso il consenso informato e pazienti in cui non stato possibile realizzare latto laparoscopico entro 2 settimane dallo studio imaging . le pazienti esaminate avevano et compresa tra 2451 anni ( et media di 33 anni ) ; di queste , 18 / 36 erano state in precedenza sottoposte ad appendicectomia e 17 / 36 ad intervento chirurgico per endometriosi . 
transabdominal us was performed with a realtime unit ( sequoia , acuson , siemens , erlangen , germany ) using convex or sectoral 3to 5 - mhz probes , depending on the patients build . 
in some cases , to better evaluate possible involvement of rectal walls , vaginal fornix and rectovaginal septum , as well as the presence of adhesions , the rectum was distended using a water - filled balloon . 
in some cases , the colour doppler technique , available on both transabdominal and endocavitary probe , was performed to differentiate between endometriotic implants and normal anatomical structures ( vessels )  . magnetic resonance mr imaging was performed with a 1.5 - t superconductive unit ( symphony , siemens , erlangen , germany )  . 
t2 fast spin echo sequences ( tr / te : 6 , 400 / 96 ; etl : 16 ) were acquired with a 256256 matrix in the sagittal , axial and sometimes coronal plane . 
t1 gre breath - hold sequences ( tr / te : 100 / 2.66 ; fa : 70 ) were performed with and without fat saturation in the three spatial planes . 
bolus was reserved for selected patients only when it was necessary to demonstrate the possible neoplastic nature of a solid component detected within the mass ( three cases )  . data analysis in all patients studied with us and mr , we evaluated lesion presence , number , location , dimensions and morphology . results were compared with findings of laparoscopy performed within 2 weeks of the mr examination and without intervening menstrual period . 
four patients were excluded owing to refusal ( n = 1 ) , obesity ( n = 2 ) and excessive time lag between imaging and surgery ( n = 1 )  . 
la rettosigmoidoscopia effettuata in 21 / 36 pazienti prima dellintervento era risultata in tutti i casi negativa per endometriosi ; in 7 / 36 casi era stata rilevata la presenza di iperemia della mucosa per fenomeni flogistici , associata al riscontro di polipi iperplastici in 2 casi . ecografia lindagine ecografica stata realizzata mediante approccio trans - addominale ed endo - cavitario , in particolare endo - rettale e / o endovaginale . 
per lesame ecografico trans - addominale stato utilizzato apparecchio real - time con 512 canali digitali ( sequoia , acuson , siemens , erlangen , germania ) , impiegando sonde convex o settoriali , da 35 mhz , a seconda della costituzione fisica della paziente . 
la preparazione ha richiesto distensione della vescica con il duplice fine di spostare verso lalto le anse intestinali , riducendo lo sbarramento del fascio ad opera del meteorismo , e ridurre la normale antiversione dellutero . a quello trans - addominale stato sempre affiancato lesame ecografico endo - cavitario per via trans - rettale o trans - vaginale , per la visualizzazione della parete rettale e dei suoi rapporti con il setto retto - vaginale , dei parametri e dei legamenti utero - sacrali . 
in alcuni casi , per meglio valutare leventuale coinvolgimento delle pareti rettali , del fornice vaginale o del setto retto - vaginale , nonch la presenza di aderenze , si ottenuta distensione del retto con palloncino pieno dacqua . lo studio stato realizzato sempre dallo stesso operatore particolarmente esperto . 
la tecnica color doppler , disponibile sia sulla sonda trans - addominale che endo - cavitaria , stata utilizzata in alcuni casi al fine di conseguire la diagnosi differenziale fra le localizzazioni endometriosiche e le strutture anatomiche normali ( vasi )  . risonanza magnetica lindagine rm stata realizzata utilizzando un magnete superconduttivo a 1.5 t ( symphony , siemens , erlangen , germania )  . 
la preparazione della paziente ha richiesto clistere di pulizia la mattina dellesame , al fine di limitare la presenza di residui fecali in corrispondenza del retto e del sigma . al momento dellesame stato somministrato farmaco ipotonizzante ( buscopam , 1 fl ev ) al fine di ridurre gli artefatti legati alla peristalsi intestinale . 
lindagine stata condotta impiegando bobine di superficie di tipo phased - array . lesame nel complesso stato realizzato utilizzando spessore di strato di 4 mm ed intervallo di 0 , 10 , 2 mle sequenze t2 fast spin echo ( tr / te : 6400 / 96 ; etl : 16 ) sono state realizzate con matrice 256256 nei piani sagittale , assiale e g . 
in particular , adhesion was considered as a lack of fatty cleavage plane between adjacent organs , with stretching of their walls and / or distortion of an intestinal loop [ 4 ]  . cul - de - sac obliteration was defined as the presence of signs of adhesion , such as stretching of the rectum towards the uterus with or without a fibrous plaque , and elevation of the posterior vaginal fornix [ 4 ]  . 
comparative data analysis provided sensitivity , specificity and predictive values of imaging techniques relative to different disease locations identified at laparoscopy . results ultrasound us examination showed the presence of endometriotic lesions in all 32 patients examined . 
these patients had a total of 101 lesions , with the following anatomical distribution : 31 in the rectovaginal septum , 37 in the ovary , 14 in the rectum , four in the vagina , three in the posterior vaginal fornix , five in the posterior cul - de - sac , two in the salpinx , two in the left uterosacral ligament , one on the bladder wall and one case of cul - de - sac obliteration . 
with regard to number , there were 84 / 101 single lesions and 17 / 101 multiple lesions ; single lesions were most frequent in the ovary ( n = 37 ) and rectovaginal septum ( n = 31 ) whereas multiple lesions were prevalently located in the rectovaginal septum ( n = 10 )  . 
 small nodules ( 43 / 101 ) , with diameter between 3 mm and 18 mm ( mean 6.6 mm ) , were prevalently located in the rectovaginal septum ( 28 / 43 )  . 
laminar lesions ( 13 / 101 ) , which had a greater axis of 1040 mm ( mean diameter , 25 mm ) , were seen in the rectovaginal septum ( two cases ) , rectum wall ( eight cases ) , posterior cul - de - sac ( two cases ) and vaginal fornix ( one case ) and were all hypoechoic . 
of the cystic lesions , 38 / 39 had internal echogenic components whereas 1 / 39 , located in the rectovaginal septum and with a diameter of 3 mm , was thick walled and with low - level internal echoes . 
le sequenze t1 gre breath - hold ( tr / te : 100 / 2 , 66 ; fa : 70 ) sono state espletate senza e con soppressione del grasso nei tre piani spaziali . 
in particolare , stato utilizzato solo in presenza , nellambito della massa , di componente solida al fine di dimostrarne la eventuale natura neoplastica ( 3 casi )  . analisi dei dati in tutte le pazienti esaminate con eg e rm stata valutata la presenza , il numero , la sede , le dimensioni e la morfologia delle lesioni eventualmente presenti . 
pertanto delle 36 pazienti esaminate , ne sono state selezionate e sono oggetto di questo studio 32 pazienti , sottoposte ad indagine eg con approccio sovrapubico e trans - cavitario e a rm , ed infine ad intervento chirurgico . quattro pazienti sono state escluse dallo studio di cui una per rifiuto da parte della paziente , 2 per obesit e una per il ritardo intercorso fra limaging e latto laparoscopico . 
ogni lesione identificata con indagine eg e rm stata classificata in base alla sede anatomica , al numero ( uniche o multiple ) e ad una delle seguenti caratteristiche morfologiche come : piccolo nodulo ( diametro inferiore a 15 mm ) , grande nodulo ( diametro superiore a 15 mm ) , lesione laminare , cisti , neoformazione complessa , adesione e obliterazione del cavo di douglas , sulla base degli aspetti recentemente riportati in letteratura [ 3 , 4 ]  . 
in particolare , abbiamo inteso come adesione la mancata visualizzazione del piano adiposo di clivaggio tra organi adiacenti con stiramento della parete degli stessi e / o distorsione di unansa intestinale [ 4 ]  . inoltre , abbiamo definito obliterazione del cavo di douglas la situazione in cui sono stati visualizzati segni di adesione come stiramento del retto verso lutero con o senza placca fibrotica e innalzamento del fornice vaginale posteriore [ 4 ]  . tale reperto che configura coinvolgimento del cavo di douglas , senza tuttavia lesione occupante spazio , non consente approccio laparoscopico anteriore . 
lanalisi comparativa dei dati ha fornito i valori di sensibilit , specificit e di predittivit delle metodiche di imaging utilizzate , relativamente alle singole localizzazioni di malattia riscontrate alla laparoscopia . risultati ecografia lindagine ecografica ha documentato la presenza di lesioni endometriosiche in tutte le 32 pazienti esaminate . 
finally , cul - de - sac obliteration was visualised as hypoechoic in only one case ( 1 / 101 )  . magnetic resonance mr examination showed the presence of endometriotic lesions in all 32 patients considered . 
overall , it demonstrated 92 lesions with the following anatomical distribution : 23 in the rectovaginal septum , 41 in the ovary ( 16 on the right and 25 on the left ) , nine in the rectum , three in the vagina , two in the posterior cul - de - sac , three in the posterior vaginal fornix , two in the large ligaments , one in the vesicouterine fold , one in the terminal ileum , two in the uterus , one in the bladder wall , two cases of cul - de - sac obliteration and two cases of adhesions . 
the majority of single lesions were seen in the ovary ( n = 18 ) , followed by the rectovaginal septum ( n = 13 ) and rectum ( n = 8 )  . 
all lesions located in the vagina , posterior cul - de - sac , posterior vaginal fornix , large ligaments , vesicouterine fold , ileum , uterus and bladder wall as well as the two cases of cul - de - sac obliteration and adhesions appeared as single . 
the 92 lesions were classified on the basis of their morphology . small nodules ( 40 / 92 ) , with diameter between 3 mm and 15 mm ( mean 8 mm ) , were prevalently seen in the rectovaginal septum ( 20 / 40 observations )  . 
of these , 36 / 40 had homogeneous appearance in t1and t2 - weighted sequences . in particular , 36 lesions were hyperintense in t1 - weighted sequences , 20 / 36 hypointense in t2 - weighted sequences , 14 / 36 hyperintense and 2 / 36 isointense . 
the 4 / 40 small nodules exhibiting inhomogeneous appearance were all hyperintense in t1 - weighted sequences ( one had an isointense marginal halo ) whereas in t2 - weighted sequences , they had a peripheral halo that was hypointense ( two cases ) and hyperintense ( two cases )  . 
 large nodules ( 3 / 92 ) , with diameter between 15 mm and 30 mm ( mean 23 mm ) , were seen in the vaginal fornix ( one case ) , rectovaginal septum ( one case ) and bladder ( one case )  . these lesions were isohypointense in t1 - weighted sequences , with small foci of signal hyperintensity . 
 laminar lesions ( 8 / 92 ) were encountered in the rectovaginal septum , large ligament and posterior cul - de - sac ; the last one was described as haematic paint . 
all these lesions had hyperintense signal in t1 - weighted sequences ; in t2 - weighted sequences , they were poorly detectable because of their isointensity in comparison with adjacent tissues , with the exception of one case that was hyperintense . 
 cystic lesions ( 32 / 92 ) , which had diameter between 4 mm and 80 mm ( mean 29 mm ) , were almost exclusively seen in the ovary ( 31 / 32 observations )  . 
per quanto concerne il numero delle 101 lesioni riscontrate , 84 sono state descritte come singole , con sede di maggiore riscontro in corrispondenza dellovaio ( n = 37 ) , seguita dal setto rettovaginale ( n = 31 )  . 
analizzando le 101 lesioni e suddividendole in rapporto al loro aspetto eg , emerge quanto segue . i piccoli noduli ( 43 / 101 ) , con diametro compreso tra 3 mm e 18 mm ( diametro medio 6 , 6 mm ) , sono risultati localizzati prevalentemente in corrispondenza del setto retto - vaginale ( 28 / 43 )  . 
questa , localizzata in corrispondenza della vescica , possedeva diametro di 30 mm ed aspetto ipoecogeno . le lesioni laminari ( 13 / 101 ) , che presentavano maggior asse compreso tra 10 mm e 40 mm ( diametro medio di 25 mm ) , sono state descritte in corrispondenza del setto retto - vaginale ( 2 casi ) , della parete del retto ( 8 casi ) , del cavo di douglas ( 2 casi ) e del fornice vaginale ( 1 caso ) e mostravano sempre aspetto ipoecogeno . le lesioni cistiche ( 39 / 101 ) , con diametro compreso tra 3 mm e 80 mm ( diametro medio 24 mm ) sono state localizzate prevalentemente a livello dellovaio ( 34 / 39 di cui 14 a destra e 20 a sinistra )  . 
di tutte le lesioni , 38 / 39 possedevano contenuto corpuscolato , mentre 1 / 39 , localizzata in corrispondenza del setto retto - vaginale , con diametro di 3 mm , stata descritta con parete spessa a contenuto finemente ecogeno . 
le neoformazioni complesse ( 4 / 101 ) , con diametro compreso tra 55 e 70 mm ( diametro medio di 64 mm ) erano localizzate in corrispondenza dellovaio ( 3 / 4 ) e del cavo del douglas ( 1 / 4 )  . 
tali lesioni presentavano sempre contenuto corpuscolato ed aspetto ecografico complesso , per la contemporanea presenza di zone ipoed iper - ecogene , per il riscontro di pareti particolarmente spesse o di gettoni solidi allinterno della formazione cistica . 
infine , lobliterazione del cavo di douglas stata visualizzata con aspetto ipoecogeno in un unico caso ( 1 / 101 )  . risonanza magnetica lindagine rm ha documentato la presenza di lesioni endometriosiche in tutte le 32 pazienti . 
nelle pazienti esaminate , sono state complessivamente riscontrate 92 lesioni con la seguente sede anatomica : 23 al setto retto - vaginale , 41 in corrispondenza dellovaio di cui 16 a destra e 25 a sinistra , 9 al retto , 3 alla vagina , 2 al cavo del douglas , 3 al fornice vaginale posteriore , 2 in corrispondenza dei legamenti larghi , 1 alla plica vescico - uterina , 1 allileo terminale , 2 allutero , 1 alla parete vescicale , obliterazione del cavo di douglas in due casi e aderenze in altri 2 casi . 
the latter two lesions showed a peripheral halo of signal hyperintensity , and in t2 weighted sequences , they had a hyperintense signal with a hypointense marginal halo with varying conspicuity . 
 adhesions ( 2 / 92 ) were observed between the rectum , an intestinal loop and the uterus in one case and between the uterus and sigmoid colon in the other case . 
 posterior cul - de - sac obliteration ( 2 / 92 ) was visualised as isointense , with foci of hyperintensity in t1 - weighted sequences and homogeneous hypointensity in t2 - weighted sequences . data analysis after being analysed separately , imaging findings in the 32 patients were compared with the results of laparoscopy in order to define the number of correct diagnoses ( true positives and true negatives ) , underestimated lesions ( false negatives ) and overestimated lesions ( false positives ) in common for the two techniques and separately for each one . among the 101 lesions detected by us and the 92 lesions detected by mr , the total number of lesions in the same anatomical site diagnosed with both us and mr and confirmed by surgery was 67 ( table 1 )  . 
of these 67 true positive findings , 33 were located in the ovaries , 20 in the rectovaginal septum , eight on the rectal wall , two in the vagina , one in the vaginal fornix , one in the posterior cul - de - sac , one in the bladder and one was a cul - de - sac obliteration . 
both us and mr misdiagnosed 38 lesions , most of which involved the large ( ten cases ) and uterosacral ( eight cases ) ligaments ( false negatives for us and mr )  . 
tutte le lesioni con sede anatomica alla vagina , al cavo del douglas , al fornice vaginale posteriore , in corrispondenza dei legamenti larghi , alla plica vescico - uterina , allileo , allutero , alla parete vescicale , lobliterazione del cavo di douglas e le aderenze sono state rilevate come singole . 
trentaquattro lesioni sono state rilevate come multiple e sono state localizzate in corrispondenza del setto retto - vaginale ( 10 casi ) e dellovaio ( 23 casi ) e del retto ( 1 caso )  . 
le 92 lesioni sono state suddivise ed analizzate in rapporto al loro aspetto . i piccoli noduli ( 40 / 92 ) , con diametro compreso tra 3 mm e 15 mm ( diametro medio 8 mm ) , sono stati individuati prevalentemente in corrispondenza del setto retto - vaginale ( 20 / 40 osservazioni )  . 
in particolare 36 lesioni erano iperintense nelle sequenze t1 pesate , 20 / 36 mostravano ipointensit di segnale nelle sequenze t2 pesate , 14 / 36 iperintensit e 2 / 36 isointensit . 
i 4 / 40 piccoli noduli che invece presentavano disomogeneit del segnale apparivano tutti iperintensi nelle sequenze t1 pesate ( 1 di essi mostrava alone marginale di isointensit di segnale ) , mentre nelle sequenze t2 pesate erano caratterizzati da alone periferico , rispettivamente ipointenso ( 2 casi ) ed iperintenso ( 2 casi )  . i grandi noduli ( 3 / 92 ) , che presentavano diametro compreso tra 15 mm e 30 mm ( diametro medio 23 mm ) , sono stati riscontrati in corrispondenza del fornice vaginale ( 1 caso ) , del setto retto - vaginale ( 1 caso ) e della vescica ( 1 caso )  . 
nelle sequenze pesate in t2 solo 1 / 3 dei grandi noduli presentava iperintesit di segnale con alone marginale ipointenso . le lesioni laminari ( 8 / 92 ) , sono state descritte in corrispondenza del setto retto - vaginale , del legamento largo e del cavo del douglas ; questultima era descritta come verniciatura ematica . 
tali lesioni erano tutte caratterizzate da iperintensit di segnale in t1 ; nella sequenza pesata in t2 erano mal riconoscibili in quanto iso - intense rispetto ai tessuti adiacenti ad eccezione di 1 caso , in cui la lesione appariva iperintensa . le lesioni cistiche ( 32 / 92 ) , che presentavano diametro compreso tra 4 mm e 80 mm ( diametro medio 29 mm ) , sono state individuate quasi esclusivamente a carico dellovaio ( 31 / 32 osservazioni )  . 
di queste 25 / 32 presentavano aspetto omogeneo nelle sequenze t1 e t2 pesate , caratterizzato sempre da iperintensit di segnale in t1 , mentre in t2 solo 9 / 25 apparivano iperintense , mostrando le restanti 16 lesioni ipointensit di segnale . 
le stesse lesioni presentavano iperintensit di segnale nelle sequenze pesate in t2 con coesistenza di alone marginale ipointenso pi o meno rappresentato , fino ad apparire come spessa banda . le neoformazioni complesse ( 5 / 92 ) , con diametro compreso tra 20 mm ed 80 mm ( diametro medio 44 mm ) , erano g . 
in contrast , 12 lesions were detected by us but not confirmed by mr or surgery ( table 1 ) localizzate in corrispondenza dellovaio ( 4 casi ) e del douglas ( 1 caso )  . 
nelle sequenze pesate in t2 in tutte le osservazioni sono stati rilevati noduli parietali , mentre il contenuto ha presentato aspetto variabile . le aderenze ( 2 / 92 ) sono state osservate fra retto , ansa table 1 differences in ultrasound ( us ) and magnetic resonance ( mr ) findings by location site of lesions identified at laparoscopy concordant diagnoses us + mr discordant diagnoses tp , true positive ; fn , false negative ; tn , true negative ; fp , false positive tabella 1 differenze dei rilievi alle diverse metodiche , suddivise per sede sede delle lesioni identificate alla lps rectovaginal septum ovary large ligaments uterosacral ligaments rectum vagina and vaginal fornix uterus douglas cul - de - sac vesicouterine fold salpinx lymph node bladder pararectal fossa peritoneum ileum sigmoid colon adhesions cul - de - sac obliteration total setto retto - vaginale ovaio legamenti larghi legamenti utero - sacrali retto vagina e fornice vaginale utero douglas plica vescico - uterina tuba linfonodo vescica fossa para - rettale peritoneo ileo sigma aderenze obliterazione douglas totale diagnosi coincidenti us + rm diagnosi discordanti vp , vero positivo ; fn , falso negativo ; vn , vero negativo ; fp , falso positivo g . 
us had greater accuracy in evaluating the rectovaginal septum , thanks to the endorectal approach that made it possible to identify lesions affecting the rectal wall and vagina . ileale e utero in un caso e fra utero e sigma nellaltro caso . le caratteristiche di segnale in entrambi i casi sono state iperintensit con banda periferica nelle sequenze pesate in t1 e ipodensit di segnale nelle sequenze pesate in t2 . lobliterazione del cavo di douglas ( 2 / 92 ) stata visualizzata con segnale isointenso con focolai di iperintensit nelle sequenze pesate in t1 e con omogenea ipointensit nelle sequenze pesate in t2 . ( cid : 2 ) ( cid : 2 ) fig . 
in this case , a peritoneal lesion was interpreted as bowel content ( white arrow in b ) at mr imaging , but us correctly identified the lesion ( a )  . 
in questa paziente non stata riconosciuta lesione peritoneale ( freccia bianca in b ) , identificata invece dalla indagine ecografica ( a )  . demonstration of lesions of large ligaments and uterosacral ligaments proved difficult , if not impossible , for both techniques ( table 2 )  . 
in particular , although us was more sensitive than mr in demonstrating lesions of the rectovaginal septum , its specificity in this site was lower ( table 2 )  . discussion endometriosis refers to the presence of functioning endometrial tissue in a heterotopic site , more frequently in the ovaries , peritoneum , posterior cul - de - sac , uterosacral ligaments and serous surface of the rectosigmoid flexure or uterus . 
di questi 67 rilievi veri positivi , 33 sono stati identificati a carico delle ovaie , 20 a carico del setto rettovaginale , 8 a livello della parete rettale , 2 in corrispondenza della vagina , 1 a livello del fornice vaginale , 1 in corrispondenza del cavo del douglas , 1 sulla parete della vescica , ed 1 come obliterazione del cavo di douglas . 
entrambe le metodiche non hanno identificato ben 38 lesioni , localizzate in prevalenza nei legamenti larghi ( 10 casi ) ed in quelli uterosacrali ( 8 casi ) ( falsi negativi eg e rm )  . 
leg si dimostrata pi attendibile nello studio del setto retto - vaginale in virt dellapproccio trans - rettale , che peraltro ha favorito anche lidentificazione di lesioni a carico della parete rettale e della vagina . 
lindagine eg ( a ) evidenza una lesione ipoecogena a livello della parete anteriore della ampolla rettale , ma non riconosce lobliterazione del cavo di douglas , identificata dalla rm ( sequenza gre t1 fs ) ( b ) e confermata dalla laparoscopia . 
nel cavo di douglas apprezzabile nodulo ipointenso , stiramento delle anse intestinali e obliterazione dello spazio retto - uterino ( b )  . paroscopic classification of the american fertility society ( afs ) ( 1985 ) based on evaluation of the presence , size and depth of peritoneal or ovarian implants , density of adhesions and degree of cul - de - sac obliteration [ 7 , 12 ]  . 
nevertheless , inspection by physical examination is frequently inadequate for assessing extension of the disease to the posterior pelvis or the presence of adhesions , so that imaging plays a major role in diagnosing endometriosis in the posterior pelvis , bowel and bladder [ 1 , 13 ]  . 
the radiological diagnosis of endometriosis is largely based on the demonstration of endometriotic cysts or endometrioma , consisting of blood degradation products accumulated after repeated bleeding . endocavitary us , particularly with a transvaginal approach , proved to be very useful in diagnosing and differentiating endometriomas from other ovarian masses , with sensitivity of 83%88% and specificity of 89%90% [ 1416 ]  . accuracy of transvaginal us is better in endometriomas larger than 2 cm and in patients with a low risk of recurrent hemorrhagic cysts [ 1 ]  . 
endorectal us had sensitivity of 97% and specificity of 96% in the diagnosis of endometriosis of the rectovaginal septum and of 80% and 97% , respectively , in the assessment of infiltration of the uterosacral ligaments [ 17 ]  . 
a recent study found similar accuracy levels for transvaginal us and endorectal us in the evaluation of rectal endometriosis and proposed using transvaginal us as the firstline examination and endorectal us to investigate suspected intestinal involvement or before surgery [ 18 ]  . 
mr is cheaper than laparoscopy , can be repeated over time [ 19 ] , is not operator delizzazioni a carico dei legamenti larghi e / o utero - sacrali ( tabella 2 )  . la specificit delle due metodiche appare significativamente diversa , nettamente a favore della rm ( 25% eg vs . 50% rm , tabella 2 )  . tali insoddisfacenti risultati , anche per quanto riguarda la rm , trovano giustificazione da un lato nella quota relativamente elevata di falsi positivi e dallaltra nellesiguo numero di veri negativi . 
in particolare leg , dimostratasi pi sensibile della rm nella dimostrazione di localizzazioni nel setto retto - vaginale , risultata meno specifica proprio in questa sede ( tabella 2 )  . discussione con il termine endometriosi si definisce la presenza di tessuto endometriale funzionante in sede eterotopica , pi comunemente a carico delle ovaie , peritoneo , cavo di douglas , legamenti utero - sacrali , superficie sierosa del retto - sigma o dellutero . 
possono essere pur raramente interessati anche altri organi pelvici o extra - pelvici [ 911 ]  . lattuale stadiazione della malattia comunemente accettata quella laparoscopica proposta dallamerican fertility society ( 1985 ) basata su presenza , dimensioni , profondit di penetrazione degli impianti peritoneali e ovarici , sulla estensione delle aderenze , e sul grado di obliterazione del cavo di douglas [ 7 , 12 ]  . tuttavia , lispezione con esame obiettivo si dimostra frequentemente inadeguata per valutare lestensione della malattia alla pelvi posteriore , come anche la presenza di adesioni , perci limaging acquista un ruolo importante per la diagnosi nella pelvi posteriore , nellintestino e nella vescica [ 1 , 13 ]  . 
the left ovarian fossa shows a hyperintense lesion in the t1weighted sequence ( a ) , which is isointense and surrounded by a hypointense peripheral ring in the t2 - weighted sequence ( b )  . 
lindagine rm , meno costosa della laparoscopia , pu essere ripetuta pi volte nel tempo [ 19 ] , non operatore - dipendente , meno invasiva della ecografia con approccio endo - cavitario e non risente dello stato di riempimento vescicale . 
alcuni autori sostengono che il ruolo della rm nella diagnosi di endometriosi dipenda dalla sede degli impianti , riconoscendole ruolo utile nella identificazione di quelli localizzati in corrispondenza dei legamenti utero - sacrali e del setto rettovaginale [ 21 ]  . confrontando la stadiazione della malattia basata sul punteggio afs con la stadiazione proposta con limpiego dello studio rm emerge una concordanza del 89% [ 22 ]  . 
la metodica rm valuta in modo accurato i primi due parametri della stadiazione laparoscopica , ma il limite maggiore dellindagine rm risiede nella valutazione ed estensione delle aderenze [ 2224 ]  . non ci risulta che sino ad oggi siano stati effettuati studi di confronto della metodica rm con quella ecografica , in particolare quella effettuata mediante approccio endocavitario trans - rettale , allo scopo di valutare leffettivo apporto delle due metodiche nel riconoscimento e nella valutazione di estensione della malattia . in questo lavoro si cercato di verificare i risultati di ciascuna metodica nel definire la presenza , la sede e le dimensioni delle singole lesioni , mettendole a confronto fra loro e con la laparoscopia . 
ma tale lesione non confermata dalla indagine rm , sequenza t2 tse nel piano sagittale ( b ) n dallatto laparoscopico . pendent , is less invasive than us with endocavitary approach and is not influenced by degree of filling of the urinary bladder . 
some authors believe the role of mr in the diagnosis of endometriosis depends on the site of the implants and recognise its usefulness in detecting lesions located in the uterosacral ligaments and rectovaginal septum [ 21 ]  . 
mr is accurate in evaluating the first two parameters of the laparoscopic classification but is limited in the assessment of adhesions [ 2224 ]  . to our knowledge , no studies have compared mr and us , and in particular , endocavitary us with the transrectal approach , to evaluate the real contribution of the two techniques to identifying and staging the disease . 
the present study evaluated the results of each technique in assessing presence , location and dimension of each lesion and compared the techniques with each other and with laparoscopy . to this aim , we selected only patients with endometriosis , which limits the statistical value of the data . 
another limitation is that confirmation of the radiological diagnosis was obtained by laparoscopy , which is not a foolproof method . with these limitations , sensitivity and specificity of the two techniques in the diagnosis of disease were of 100% . 
in fact , all patients with a diagnosis of endometriosis were true positive at surgery , but if we consider the detection of single lesions , the results of the two techniques are more disappointing . 
overall , us demonstrated sensitivity of 58% ( table 2 ) , specificity of 25% ( table 2 ) , positive and negative predictive value of 82% and 9% and accuracy of 53% . 
mr demonstrated sensitivity of 56% ( table 2 ) , specificity of 50% ( table 2 ) , positive and negative predictive value of 90% and 16% , respectively , and accuracy of 55% . 
the two techniques therefore have excellent sensitivity for identification of endometriosis , but their performance in assessing disease extent is unsatisfactory owing to the possible misinterpretation of many la validit statistica dei risultati . 
considerando per il riconoscimento delle singole lesioni i risultati delle due metodiche sono meno brillanti . delle 143 lesioni confermate chirurgicamente infatti , ne sono state rilevate solo 83 con eg e 80 con rm . 
pertanto alla eg la sensibilit stata del 58% ( tabella 2 ) , la specificit del 25% ( tabella 2 ) , i valori predittivi positivi e negativi rispettivamente del 82% e del 9% , laccuratezza del 53% . 
alla rm la sensibilit stata del 56% ( tabella 2 ) , la specificit del 50% ( tabella 2 ) , i valori predittivi positivi e negativi rispettivamente del 90% e del 16% , laccuratezza del 55% . si deve pertanto ritenere che le due metodiche abbiano ottima sensibilit nella identificazione della endometriosi , mentre il loro bilancio di estensione della malattia assai meno accurato in quanto molte localizzazioni , identificate laparoscopicamente , possono essere misconosciute . 
endorectal us can in part overcome the field - of - view limitations of the transvaginal approach , as progress of the probe into the pelvis is not hindered by the vaginal fornices . 
at the same time there was a high incidence of false positive results for us in the diagnosis of very small lesions , especially those located in the rectovaginal septu because this site contains no anatomical structures that could resemble small endometriotic foci , it is more likely that they should go undetected during laparoscopy . 
in the rare cases that a single small lesion is detected , it is treated medically rather than surgically ; instead , where such lesions are associated with larger ones , detectable with the gynaecological examination , surgery is required , above all in the presence of pain . false positive us results might also be caused by the misdiagnosis of endometrioma in the presence of a haemorrhagic ovarian cyst , a tuboovarian abscess or an ovarian neoplasia [ 27 ]  . 
the false negativity of mr is accounted for by the very small dimensions of some endometriotic implants ; instead , its false positivity results from vessels and bowel content , both of which cause signal hyperintensity in t1weighted sequences , especially in those with fat suppression . conclusions to date , diagnostic accuracy of endorectal us and mr in the study of endometriosis is not significantly different . 
in contrast , in the case of a diagnostic doubt as to the real nature of the lesion , mr and , in particular , t1 - weighted sequences with fat suppression will prole lesioni pelviche , localizzate nel campo di vista del fascio ultrasonoro , e dalla maggiore esplorabilit e discriminazione tissutale consentita dalla indagine rm . 
lindagine ecografica , con approccio endo - cavitario trans - rettale , pu parzialmente ovviare alle limitazioni di campo di vista intrinseche alla metodica trans - vaginale in rapporto al mancato ostacolo , rappresentato dai fornici vaginali , alla risalita della sonda nello scavo pelvico . 
nel contempo si registrata elevata incidenza di false positivit degli us proprio nella diagnosi di lesioni di assai piccole dimensioni , localizzate soprattutto nello spessore del setto retto - vaginale . 
poich non esistono in tale sede strutture anatomiche che possano presentare aspetto simile ai piccoli focolai endometriosici descritti , parrebbe pi verosimile il loro mancato riconoscimento in corso di laparoscopia . in ogni caso , lesioni di cos piccole dimensioni presentano scarso valore clinico . 
infatti , nei rari casi di localizzazione unica , queste lesioni non sono suscettibili di trattamento chirurgico , ma solo farmacologico ; quando sono associate a lesioni di pi grosse dimensioni , valutabili peraltro con la sola visita ginecologica , comunque si impone il trattamento chirurgico , soprattutto in presenza di dolore . la falsa positivit ecografica pu inoltre derivare dalla errata diagnosi di endometrioma in presenza di cisti emorragica dellovaio , ascesso tubo ovarico o tumore ovarico [ 27 ]  . 
gli errori di falsa negativit della rm trovano il pi delle volte giustificazione nelle assai esigue dimensioni di alcune localizzazioni endometriosiche . per la falsa positivit rm giocano invece ruolo fondamentale i vasi ed il contenuto intestinale responsabili entrambi di iperintensit di segnale nelle sequenze t1 pesate , soprattutto in quelle con soppressione del grasso . conclusioni allo stato attuale leg , per via trans - rettale , e la rm non dimostrano significative differenze di accuratezza diagnostica nello studio della endometriosi . 
in particolare nel caso di documentata lesione pelvica , unica o multipla , con chiare caratteristiche di endometriosi , il ricorso alla rm appare superfluo dovendosi procedere direttamente con la laparoscopia . 
nel caso invece vi siano dubbi diagnostici circa la effettiva natura della lesione identificata , preferibile il ricorso alla rm che consente pi accurata analisi strutturale grazie soprattutto alle sequenze pesate in t1 con soppressione del grasso . 
di radiologia , universit degli studi , ospedale di cattinara , strada di fiume 447 , i - 34149 trieste , italy , tel . : + 39 - 040 - 910947 , fax : + 39 - 040 - 910921 , e - mail : dallap@units.it received : 12 march 2006 / accepted : 25 march 2006 / published online : 29 june 2006 abstract todays radiology is experiencing two major trends , one negative and one positive . 
the first is the so - called turf war , in other words , the progressive invasion of the imaging domain by other specialists such as cardiologists , urologists , gastroenterologists , gynaecologists etc . 
in this process , they are aided by new technologies such as picture archiving and communication systems ( pacs ) and computed - aided diagnosis cad and by radiology technologists who collaborate with them , replacing radiologists . 
the positive aspect is the outstanding technological evolution : the advent of molecular imaging , optical imaging , nanotechnologies , teleradiology and percutaneous gene therapy . while dramatically expanding the diagnostic possibilities down to the subcellular level , these techniques demand new forms of training in radiology and interdisciplinary cooperation . tomorrows radiologist will need to acquire appropriate clinical knowledge , restore contact with the patient to take on a prominent role in the diagnostic process , learn the basic sciences , foster a multidisciplinary approach and finally be able to use the internet for learning and continuing education . 
il primo rappresentato dalla cosiddetta guerra di campo o turf war ovverosia dalla progressiva invasione del campo dellimaging da parte di altri specialisti quali il cardiologo , lurologo , il gastroenterologo , il ginecologo etc . , che si vanno impossessando di varie tecniche , in primis lecografia e via via della tac e della rm . 
in questo sono favoriti dalle nuove tecnologie quali il pacs e le cad e dalla collaborazione con tecnici di radiologia che si sostituiscono , loro fianco , ai radiologi . laspetto positivo rappresentato dalla strepitosa evoluzione tecnologica : lavvento dellimaging molecolare , dellimaging a luce ottica , delle nanotecnologie , della teleradiologia , della terapia genica percutanea le quali se allargano enormemente le possibilit diagnostiche sino a livello subcellulare richiedono peraltro al futuro radiologo una nuova formazione e una collaborazione interdisciplinare . 
egli dovr acquisire una appropriata cultura clinica , ritrovare il contatto con il paziente per acquisire un ruolo preminente nelliter diagnostico , apprendere le scienze di base , favorire lapproccio operativo multidisciplinare e infine saper navigare in internet per favorire lapprendimento e laggiornamento . 
il radiologo del futuro sopravvivr se sapr reinventarsi . key words future radiology turf war imaging new technologies continuing education parole chiave radiologia , futuro guerra di campo nuove tecnologie dimmagini educazione continua introduction introduzione before considering possible future scenarios for radiologists in the new century , i find it useful to describe the current situation , outline recent developments in radiology and predict future developments : with radiology constantly evolving , how will radiologists survive ? my presentation therefore deals with : radiologists today : turf wars the radiology revolution radiologists tomorrow : what future ? trattare il tema di quale potr essere il futuro del radiologo in questo nuovo secolo implica iniziare con la fotografia della situazione attuale dei radiologi , delineare i recenti sviluppi della radiologia e prevedere i successivi per poi entrare nei vivo del tema : in una radiologia in continua evoluzione come sopravvivr il radiologo ? tratterr quindi in successione : il radiologo oggi : la guerra di campo la rivoluzione della radiologia il radiologo domani : quale futuro ? l . 
dalla palma : tomorrows radiologist : what future ? radiologists today : turf wars il radiologo oggi : guerra di campo in a recent article , levin and rao [ 1 ] wrote : we in radiology generally believe that for a number of reasons , we are the ones who should perform imaging on patients . 
we are familiar with all imaging modalities and are thus able to consult with ordering physicians and steer their patients to other studies that may be more appropriate for the clinical questions at hand.... 
and last but not least , we are trained in radiation and magnetic resonance imaging safety . despite the inherent truth and logic of this argument , many of our physician colleagues in other specialties do not agree with it . 
and this interest lies at the heart of the so - called turf battles or wars . the most blatant example is that of cardiologists , who have virtually taken over both coronary angiography and percutaneous coronary interventions ( angioplasty and stenting )  . 
radiologists have progressively abandoned cardioradiology . less striking but equally pressing is the turf war concerning percutaneous angioplasty and peripheral artery stenting . interesting data in this respect have been reported by levin et al . 
the authors evaluated the number of procedures carried out from 1997 to 2002 subdivided by specialists performing the while interventional vascular procedures done by radiologists increased by 29% , those done by cardiologists increased by 181% , those done by vascular surgeons by 398% and those done by other specialists by 195% . 
a clear sign of this is the recent creation of the in un loro recente articolo levin e rao [ 1 ] scrivono : noi in radiologia generalmente crediamo per un insieme di ragioni di essere quelli che dovrebbero acquisire le immagini dei pazienti . 
noi abbiamo familiarit con tutte le tecniche di imaging e siamo quindi nelle condizioni di consultare il medico richiedente e dirottare i loro pazienti ad altri tipi di indagini pi adatte a risolvere i quesiti clinici . 
nasce da questo interesse quella che in inglese viene definita turf battle or war ovverossia battaglia o guerra di campo . lesempio pi clamoroso lo abbiamo con i cardiologi che di fatto si sono impossessati pressoch totalmente sia della coronarografia che degli interventi percutanei coronarici ( angioplastica e stent )  . 
vi stato un progressivo allontanamento dei radiologi dalla cardioradiologia . meno importante , per incalzante , loccupazione di campo per quanto riguarda langioplastica percutanea e la collocazione di stents nelle arterie periferiche . 
mentre il numero di procedure intervenzionali vascolari dei radiologi aumentato del 29% , quello dei cardiologi del 181% , dei chirurghi vascolari del 398% e di altri specialisti del 195% . 
valutando il numero complessivo per specialit nei due anni di osservazione si nota come il numero di procedure eseguite da radiologi si sia abbassato dal 63 , 3% al 49% , quelle dei cardiologi si alzato dal 25 , 2% al 36 , 3% e di pari passo per gli altri specialisti . lavanzamento nel campo cardiovascolare sta profilandosi preoccupante per le tecniche non invasive quali la tc e la rm . 
ne un forte segnale la recente costituzione della society of cardiovascular computed tomography ( scct ) forsociety of cardiovascular computed tomography ( scct ) , composed of cardiologists , radiologists and vascular surgeons but with a predominance of cardiologist . 
the same is happening in mri with the creation of the society for cardiovascular magnetic resonance whose 2005 congress saw an increase in both scientific communications and posters compared with the previous 2 years . 
in europe , the european society of urologic imaging has been set up , with the more - or - less unwitting connivance of some radiologists ; society members so far include experts in ultrasonography ( us ) , ct and mri . a very lively battle is being fought over us , above all in certain fields ; the battle over cardiology has been lost whereas the situation is compromised in other fields such as obstetrics . 
european radiologists have controlled general us ( abdomen , pelvis , soft tissue , breast , etc . ) since the mid - 1970s , but the invasion by nonradiologists is becoming more aggressive on the grounds that sonography refines the clinical assessment . 
on the basis of the data collected , they divided the hospitals into four categories : in group 1 , radiologists performed 96%100% of examinations with an average of 2 , 800 exams per machine / year . 
in group 2 , radiologists performed 60%95% of exams with an average of 2 , 0003 , 000 exams per machine / year ; nonradiologists performed 300400 exams per machine / year . 
in group 3 , radiologists controlled 20%50% of the work with 2 , 5003 , 200 exams per machine / year ; nonradiologists performed an average of 300600 exams per machine / year . 
in group 4 , the authors list the hospitals where the situation is hopeless : at the university hospital of frankfurt , radiologists performed 1 , 500 exams per year on five sonography machines whereas it was assumed that nonradiologists , with 38 sonography machines , performed 35 , 00040 , 000 exams / year . 
according to the authors , this example is not the only one in germany and reflects the tendency to lose control over us , as is also happening in switzerland and austria . data gathered for the usa are also interesting . 
 [ 6 ] used the medicare database to collect data on the number of us examinations done by radiologists , cardiologists and other physicians from 1993 to 2001 per 1 , 000 medicare beneficiaries . 
analogo orientamento gi in atto per la rm con la costituzione della society for cardiovascular magnetic resonance che nel suo congresso del 2005 ha visto un aumento rispetto ai due anni precedenti sia delle comunicazioni scientifiche che dei posters . 
negli stati uniti da tempo pure attiva la north american society of cardiac imaging ( nasci )  . lo stesso fenomeno sta profilandosi in campo urologico . a livello europeo si infatti costituita , con la connivenza pi o meno ingenua di alcuni colleghi radiologi , la european society of urologic imaging che per ora si limita ad annoverare esperti di ecografia e cultori di tc ed rm . molto vivace invece lo scontro per lecografia soprattutto in alcuni campi ; mentre in cardiologia la battaglia perduta , in altri ancora , quali lostetricia , compromessa . con gli urologi la battaglia molto accesa mentre meno accesa con i gastroenterologi . i radiologi in europa hanno preso posizione nellecografia generale ( addome , pelvi , parti molli , mammella etc . ) sin dalla met degli anni 70 ma attualmente nel mondo non radiologico loccupazione di campo sta avanzando alla luce del concetto che la sonda ecografica consente di perfezionare lesame semeiologico clinico . 
su questa base , sulla miglior conoscenza del quadro clinico i medici specialisti autoprescrivono e conducono lesame ecografico : particolarmente aggressivi sono i medici del dipartimento di emergenza ed i gastroenterologi . 
nella categoria 3 i radiologi controllano il 20%50% dellattivit con un numero di esami per apparecchio / anno di 25003200 ; i non radiologi eseguono mediamente tra i 300600 esami apparecchio / anno . 
 [ 6 ] hanno raccolto il numero di esami ecografici eseguiti da radiologi , cardiologi e altri medici negli anni 1993 e 2001 attraverso il servizio medicare calcolando il numero su 1000 utilizzatori del servizio . 
i radiologi sono passati da 132 , 9 a 166 , 3 per mille con un aumento del 25% ; i cardiologi da 190 , 3 e 356 , 1 con un aumento dell85% ( nella grandissima maggioranza si trattava di ecocardiografie ) ; altri medici sono passati da 116 , 9 a 167 con un aumento del 43% . 
dalla palma : tomorrows radiologist : what future ? an 85% increase ( the vast majority were echocardiograms ) ; other physicians increased from 116.9 to 167 , a 43% increase . 
in other words , the number of examinations for nonradiologists ( excluding cardiologists ) grew twice as rapidly as it did for radiologists , a phenomenon driven by self - referrals , which lead to overutilisation and higher costs . 
the situation in italy is even bleaker given that the siumb ( italian society for ultrasonography in medicine and biology ) has also involved general practitioners , and it was facilitated in this by industry , which introduced portable us machines . a turf battle may also be looming for ct and mri at the level of both large hospitals and private practices . 
another example is mobile outsourcing where mri and ct machines are installed on vehicles that travel from hospital to hospital to make up for staff and / or technology shortages . 
here , the competition is not based on examination quality or staff professionalism , both of which have to be above standard in public facilities : the superspecialisation seen in public facilities surely fosters a better clinical - radiological interpretation . 
a typical example of teleradiology reporting centres can be seen in bangalore , india , which does plenty of work for the united states . let us now consider the situation in nonvascular interventional radiology , a domain that has been thoroughly investigated by schnyder et al . 
 in the meantime , radiologists devised new percutaneous drainage techniques , stenting procedures ( mostly biliary ) and balloon dilatation procedures and subsequently new abdommero di esami tra i non radiologi ( esclusi i cardiologi ) cresciuto due volte rispetto a quello dei radiologi , fenomeno sul quale incide lautoprescrizione che porta ad una superutilizzazione e a maggiori costi . 
in italia il fenomeno ancora pi grave dal momento che la siumb ha coinvolto come operatori i medici di medicina generale e lindustria li ha facilitati con la produzione di apparecchi portatili . la battaglia di campo pu profilarsi anche per la tc e rm sia a livello di grandi ospedali sia nellattivit privata . 
tipico lesempio dellimprenditore finanziario che attiva strutture tecnologicamente dotate e gestite da radiologi non sempre allaltezza ; tali strutture si mettono in concorrenza con la struttura pubblica , magari molto qualificata ma non sempre in grado di soddisfare tempestivamente il paziente esterno . 
caratteristico lesempio delloutsourcing mobile basato sullinstallazione di macchine rm e tc che si spostano di ospedale in ospedale per sopperire carenze di organico e / o di struttura . unaltra forma di outsourcing rappresentata dalla possibile creazione di centri di refertazione teleradiologici gestiti da radiologi cui far afferire immagini radiologiche digitali acquisite da colleghi di altre discipline . 
in questo caso la competizione non pu che basarsi sulla qualit dellesame e sulla professionalit dello staff che nella struttura pubblica devono essere di livello superiori : la superspecialit presente in questa struttura favorisce certamente una migliore interpretazione clinico - radiologica . 
un tipico esempio di tali centri lo riscontriamo in india - bangalore che ha unintensa attivit con gli stati uniti . passo ora a descrivere la situazione nel campo della radiologia interventistica non vascolare , aspetto ben analizzato da schnyder et al . 
la radiologia interventistica esplosa attorno agli anni 80 quando venne introdotta laspirazione percutanea di alcuni visceri addominali , di masse e raccolte per esami citologici e batteriologici e successivamente estesa al torace e incrementata con le biopsie con aghi di maggior calibro per esami istologici , attivit facilitate dalla guida con gli us e con la tc . 
pochi anni dopo inizi la battaglia , favorita appunto dallimpiego dellecografia , con i gastroenterologi per le procedure epatiche e biliari , con gli urologi per le nefrostomie e le litotrissie percutanee : questi specialisti stanno progressivamente avanzando . 
nel frattempo i radiologi mettevano a punto nuove tecniche di drenaggio percutaneo , procedure di stenting , prevalentemente biliare , e di dilatazione mediante palloncino ; successivamente a livello addominale altre tecniche apparivano , grazie ai radiologi , quali la tip e il posizionamento di filtri cavali . 
the current situation should be basically unchanged , favoured as we are by the advances in imaging technology such as ct fluoroscopy and open mri , which ensure precise guidance in the insertion of needles , catheters and probes . i end this section by illustrating yet another invasion that is occurring in england where , due to the small number of radiologists and increased workloads , the door has been opened for radiographers to report on chest and skeletal radiographs and carry out and report on contrast - enhanced exams such as barium enemas and urograms . 
the decision has been justified by the need for radiologists to devote their time to more complex and specialised examinations and by the opportunity given to radiographers to increase their motivation and to develop professionally . 
a recent metaanalysis of a homogeneous selection of 12 articles [ 8 ] demonstrated that the reporting accuracy of skeletal radiographs in emergency department patients did not differ between welltrained radiographers and radiologists with varying levels of experience . 
the degree of radiographer training only affected specificity , meaning that the distinction between normal and pathological requires a good level of training . another recent study found that the accuracy of radiographers in reporting on urographic examinations reached 92% compared with an expert uroradiologist [ 9 ]  . 
the trend is undoubtedly alarming as regards what could happen in italy where the law has given the head radiographer management responsibilities and set up degree courses for radiographers . it should also be noted that radiographers are being employed by other specialists , in particular , cardiologists and orthopaedic surgeons [ 11 ] , which broadens the gap between these clinical domains and radiology and turns the turf battle into a real war . the radiology revolution this is the aspect that will most influence the future of radiologists . 
and the magnitude of these advances also emerged in various sections of this excellent congress of our society , which has done admirably well in handling the developments of radiology from congress to congress . 
dalla palma : tomorrows radiologist : what future ? dovrebbe essere molto diversa al giorno doggi favoriti come siamo dallavanzamento della tecnologia di imaging quale la fluorotc e la rm a campo aperto che facilitano la guida precisa nellintroduzione di aghi , di cateteri e di sonde . chiudo questo capitolo segnalando unaltra invasione che in atto soprattutto in inghilterra dove per lo scarso numero di radiologi e laumento dei carichi di lavoro sono state aperte le porte ai tecnici radiologi nella refertazione di esami radiografici del torace e dello scheletro e nellesecuzione e refertazione di esami contrastografici quali il clisma e lurografia . 
questa decisione viene giustificata dalla necessit che hanno i radiologi di dedicarsi ad indagini pi complesse e pi specialistiche e dallopportunit che viene offerta ai tecnici di sentirsi pi motivati e di migliorare la loro professionalit . 
una recente valutazione metaanalitica su 12 articoli selezionati in modo omogeneo [ 8 ] ha documentato che laccuratezza nella refertazione di esami radiografici dello scheletro in pazienti provenienti dal pronto soccorso e dal dipartimento di emergenza non apparsa diversa tra tecnici radiologi ben addestrati e radiologi di varia anzianit . 
il grado di addestramento dei tecnici ha influenzato solamente la specificit per cui la distinzione tra normale e patologico richiede loro un buon training . un altro recente articolo ha riportato che laccuratezza del tecnico nel refertare esami urografici ha raggiunto il 92% messo a confronto con un esperto uroradiologo [ 9 ]  . tale iniziativa in atto anche in alcune universit degli stati uniti [ 10 ]  . 
non c dubbio che il fenomeno allarmante per quanto potrebbe succedere nel nostro paese dove la legge ha responsabilizzato il capotecnico nella gestione del reparto e ha attivato i corsi di laurea per tecnici . va inoltre tenuto presente che i tecnici radiologi vengono arruolati da altri specialisti , in particolare cardiologi ed ortopedici [ 11 ] aggravando il distacco delle rispettive attivit dalla radiologia e trasformando la battaglia in vera e propria guerra di campo . la rivoluzione della radiologia questo il capitolo che condizioner maggiormente il radiologo del futuro . 
in quale direzione stiamo andando ?  . per quanto concerne la radiologia del futuro trovo interessante riportare quanto ha scritto arenson [ 13 ] , chairman del dipartimento di radiologia delluniversit di san francisco , in un articolo dal titolo the practice of medicine and radiology in 2020 dove lautore descrive il futuribile che sintetizzo . 
dalla palma : tomorrows radiologist : what future ? as regards the future of radiology , the predictions made by arenson [ 13 ] , chairman of the department of radiology of the university of san francisco in an article titled the practice of medicine and radiology in 2020 are worth summarising . 
firstly , telemedicine will undergo incredible development with the use of videoconferencing , permitting a variety of interactions , including two - way audio and video communications between patients at home and the medical facilities where they have been examined . 
there will be considerable ageing of the population , with a mean age around 100 years for women and 90 years for men : some will survive until the age of 120 years , so there will be a preponderance of geriatric diseases and a corresponding decrease in paediatric diseases . plain film radiography will be supplanted by ct and mri and digital radiography as the first - line approach in emergency settings and the bedside modality in hospitals and ambulances . 
in interventional radiology , endovascular mri will guide not only catheters but also remote - controlled electronic devices that serve to launch a variety of devices that , like microscopic missiles , travel through vessels to reach organs or tissues adjacent to the vessels . 
picture archiving and communication systems ( pacs ) systems will be so efficient and widespread as to allow the transmission of images , connected to the patients smart card , to any part of the world . 
in this scenario , it is the radiologists who have expertise in electronics and informatics who will control the imaging of the future . as a postscript to my article , i briefly describe what is happening in the united states [ 14 ]  . 
recently , the national institutes of health ( nih ) provided funding for three broad lines of research , one titled new pathways to discovery , within which a number of bioinformatics and computational biology projects were selected . 
one of these is based at the brigham and womens hospital of boston , which operates through the national alliance for medical imaging computinterazioni ivi compreso la comunicazione audio e video a due vie che metter in contatto i pazienti da casa con la struttura medica dove stato esaminato . 
vi sar un invecchiamento notevole della popolazione con unet media attorno ai 100 anni per le donne e 90 anni per gli uomini : alcuni sopravviveranno sino ai 120 anni , per cui vi sar una preponderanza di patologia geriatrica , con una concomitante diminuzione della patologia pediatrica . lesame radiografico ceder il passo allesame con tc ed rm e allesame diretto digitale come primo esame nella patologia durgenza , e quale esame al letto del paziente e nelle ambulanze . 
a livello interventistico , la rm endovascolare guider non solo cateteri ma anche dispositivi elettronici controllabili a distanza e predisposti al lancio di congegni vari che come micromissili viaggiano nei vasi sino a raggiungere organi o comunque strutture tissutali adiacenti ai vasi . 
in questa evoluzione il radiologo che avr una formazione professionale elettronica ed informatica potr tenere sotto controllo limaging del futuro . in appendice a quanto ho scritto nel mio articolo ritengo opportuno aggiornarvi su quanto sta attualmente succedendo negli stati uniti [ 14 ]  . 
il brigham and womens hospital di boston opera attraverso il centro national alliance for medical imaging computing che costituito da un team multi - istituzionale che comprende computer scienziati , ingegneri software e ricercatori medici che si focalizzano sullo sviluppo di metodi computazionali per analizzare e visualizzare i dati di immagini mediche . 
per avanzare la frontiera della conoscenza di questa patologia mentale verranno utilizzati nuovi metodi computazionali , un robusto software integrato con imaging di risonanza magnetica strutturale , funzionale e di diffusione , elettroencefalografia quantitativa e pet . ing , a multiinstitutional team of computer scientists , software engineers and medical investigators who develop computational tools for analysis and visualisation of medical image data . 
focusing on schizophrenia , the research project aims at increasing knowledge about the disease by using new computational methods , a robust software integrated with structural , functional and diffusion mri , quantitative electroencephalography and positron emission tomography ( pet )  . thanks to research by image scientists , radiologists will find themselves handling the diagnosis and treatment of a large part of tomorrows medicine . tomorrows radiologist : what future ? we need to make a distinction between the near future and the distant future in relation to which radiologists will have to change many of their attitudes and rethink their professional training to accommodate the dramatic revolution and evolution of radiology . to face the near future , we need to reconsider our strategy in fighting the various turf wars described above . one of the main reasons why radiologists are losing many turf battles is no doubt their inadequate if not inexistent clinical culture : a high level of technical training is not sufficient for dealing with clinicians and their clinical queries . medical practice is becoming increasingly interdisciplinary due to the vastness of knowledge involved . 
good clinical training will enable radiologists to interact on a par with clinicians , even in view of the fact that clinicians are moving further and further away from the patient , being fascinated by the disease in contrast with the spirit of medicine passed down by hippocrates . 
we have all found ourselves reporting without any clinical data because the patient was referred to the radiology department before being examined . clinicalisation is therefore one of the main steps . 
clearly , this approach entails privileging organ pathology , which should be learned after having acquired a basic grounding . each staff radiologist working in a complex facility will have to be superspecialised in the imaging of a specific organ system ( nervous , musculoskeletal , chest , abdomen ) to be able to take part in an interdisciplinary discussion as a key player rather than merely an image reader unable to tackle a clinical differential diagnosis . 
clinicians will feel the need to seek the opinion of radiologists with good clinical knowledge ; otherwise , pacs and teleradiology will prevail , with images arriving directly in the clinical departments and bypassing the radiologist . 
dalla palma : tomorrows radiologist : what future ? il radiologo quindi , grazie alle ricerche dello scienziato dellimmagine , si trover a gestire diagnosi e terapia di una parte cospicua della medicina del futuro . il radiologo domani : quale futuro ? distinguo anzitutto un futuro immediato e un futuro in proiezione in rapporto ai quali i radiologi devono anzitutto modificare molti dei loro atteggiamenti e in secondo luogo devono reinventarsi una nuova formazione professionale che affronti la eccezionale rivoluzione ed evoluzione della radiologia . il futuro immediato va affrontato riorganizzando la strategia con la quale combattere le varie battaglie di campo che ho ora trattato . 
uno dei fattori principali che trovano i radiologi in ritirata in molte battaglie di campo certamente nella maggior parte dei casi la modesta per non dire assente cultura clinica : una elevata preparazione tecnica infatti non sufficiente per affrontare il collega clinico con i suoi quesiti . 
nellattivit medica che sta diventando sempre pi interdisciplinare per la vastit delle conoscenze che necessario saper dominare , una buona conoscenza della clinica consente un dialogo allo stesso livello con il clinico anche perch questi si sta sempre pi allontanando dal malato affascinato invece dalla malattia in contrasto con lo spirito della medicina tramandato da ippocrate . 
nellorganico di una struttura complessa quindi opportuno che ognuno dei radiologi sia super specializzato nella radiologia di un apparato ( nervoso , muscolo - scheletrico , torace , addome ) in modo da poter partecipare a un dibattito interdisciplinare come una figura di primo piano e non come un semplice lettore di immagini incapace di gestire una diagnostica differenziale clinica . 
un buon esempio di quanto valida sia la preparazione clinica la troviamo nel neuroradiologo la cui conoscenza della neurologia anatomo - clinica di ottimo livello , il che garantisce un ottimo dialogo con il neurologo e con il neurochirurgo . 
un radiologo con buona cultura clinica far sentire la necessit di essere interpellato dal collega ; in caso contrario prender il sopravvento la tecnologia pacs e teleradiologica con le immagini che arrivano direttamente nei reparti clinici bypassando il radiologo : se ci inevitabile per la casistica semplice , non cos avverr per la casistica complessa che non pu prescindere dal dibattito collegiale . 
la clinicizzazione del radiologo sar completa quanto pi egli riprender il contatto con il paziente ; questo si verifica con lecografia quando il radiologo conducendo lesame dialoga con il paziente e si trasforma , nel momento in cui gestisce la sonda , in un vero e proprio semeiologo clinico . 
this is the case in us where the radiologist talks to the patient while performing the examination and becomes , as he or she handles the probe , a true clinical semiologist . 
but for all the other modalities , despite the physicians respect for the radiologist who guides the diagnosis and treatment and documents treatment efficacy through follow - up examinations , patients do not perceive the importance of the role because of the minimal contact they have with the radiologist . 
as a result , the patient is convinced that it is the referring doctor who reads the examination , even more so today as pacs allows him or her to view the image . 
margulis and sostman [ 15 ] , however , state that radiologists need to restore the doctor - patient relationship , take the history and give patients information on the examination results so that patients may perceive they have been dealing with a doctor and not with a technician . 
i have had this experience in my private practice where this approach meant that the patients often wanted to see me before the clinician , who paradoxically devotes increasingly less time to the patient . 
this anecdotal data is confirmed by margulis and sostman [ 15 ] , who mention private ct screening centres in the united states where the radiologist - patient relationship is becoming more and more popular . 
this should not be merely the bureaucratic signing of a form but the signing of a consent based on correct information that justifies performance of the examination despite the risks associated with it and with a view to solving the clinical problem troubling the patient . 
contact with outpatients can be further improved by using internet technology : for example , by putting the report online as soon as it is ready , possibly together with the most significant images . already in place in the united states , this system was found to increase patient satisfaction and foster acknowledgement of the radiologist as the professional actually responsible for the examination and result [ 16 ]  . clinicalisation of radiology will encourage medical graduates to choose radiology as their speciality given that diagnostic radiology is often discarded precisely because it is considered exclusively technical , increasingly complex and without contact with patients , the latter being the most meaningful aspect of medicine . 
exclusively technical radiologists are destined to be progressively replaced by graduate radiographers and / or physicists with a sound medical knowledge . grado il ruolo del radiologo sia rispettato dal medico perch la sua interpretazione guida la diagnosi e la successiva terapia e documenta lefficacia di questultima con il follow - up , ci malgrado il paziente non percepisce questo ruolo proprio per il minimo contatto che ha con il radiologo , affermano margulis e sostman [ 15 ] che documentano questa affermazione sulla base di un questionario cui hanno risposto 42 dipartimenti universitari e 24 centri privati . 
egli invece , sostengono margulis e sostman , deve ritrovare il contatto con il paziente , raccogliere lanamnesi , dargli le prime informazioni sullesito dellesame in modo che abbia la percezione che ha avuto a che fare con un medico e non con un tecnico . 
io ho avuto questa esperienza nella mia attivit privata dove con questa impostazione mi sono trovato molto spesso ad essere richiesto dal paziente prima del clinico che paradossalmente dedica sempre meno tempo al paziente . 
questo dato aneddotico peraltro confermato da margulis e sostman che citano i centri tc di screening privati negli stati uniti dove il contatto paziente - radiologo la regola con un ritorno di popolarit . 
tale rapporto peraltro la regola nei centri senologici . il rapporto con il paziente una delle responsabilit etiche del radiologo , rapporto che nasce al momento del consenso informato : questo non deve essere una semplice firma burocratica su un modulo bens la firma ad un consenso basato su una informazione corretta che giustifica lesame pur con i rischi ad esso connessi , nella logica di risolvere il problema clinico che angoscia il paziente . 
il contatto con il paziente esterno ancora perfezionabile ricorrendo alluso della tecnologia internet e mettendo quindi in linea il referto non appena questo pronto ed eventualmente le immagini pi significative dellesame : tale sistema gi operativo negli stati uniti dove si notato una maggior soddisfazione del paziente che riconosce , fra laltro , nel radiologo , il vero responsabile dellesame e del risultato [ 16 ]  . la clinicizzazione del radiologo favorir la scelta della nostra specialit da parte del medico neolaureato che nel suo orientamento molto spesso scarta la radiologia diagnostica proprio perch considerata esclusivamente tecnica e sempre pi complessa e senza rapporto con il paziente che rappresenta il momento pi pregnante in medicina . 
il radiologo esclusivamente tecnico destinato a essere progressivamente soppiantato dal tecnico radiologo laureato e / o dal fisico con buone conoscenze mediche : questi sono favoriti dallimporsi della tecnologia pacs e della teleradiologia nonch dei computers con software dedicati al riconoscimento automatico dimmagine ( cad )  . 
ovvio che il clinico operante nei grossi complessi ospedalieri in mancanza di un radiologo con cultura clinica sar portato a gestirsi linquadramento diagnostico su immagini acquisite da altre figure tecniche . this is facilitated by pacs technology and teleradiology and by computers with software for automated image detection ( cad )  . 
clearly , the lack of radiologists with clinical knowledge will lead clinicians in large hospitals to make their diagnoses on images acquired by other technical professionals . clinicalised radiology also entails a need to recover the role of interventional radiologists who will need both hospital beds and a follow - up clinic for their work . patients undergoing percutaneous interventional procedures require adequate preparation and aftercare , as well as careful follow - up to check the success of the radiologists intervention . 
even in this case , patients will perceive that the radiologist has been crucial to the solution of their problem and can be relied on for the follow - up ; in other words , the radiologist becomes their treating physician as well . 
it should be noted that radiologists actually have the edge in the turf wars , as they have access to an array of imaging modalities to guide the procedure , and hospital management will consider the concentration of interventional procedures in a single facility devoted full - time to this activity as the economically soundest solution . 
this means that an interventional procedure facility that works part time is underutilised and therefore has higher costs . another limitation of nonradiologist specialists doing interventional procedures is the fact that they generally do not carry out all types of interventional procedures but only those pertaining to their speciality . 
in other words , when modernising the facility , they will have to devote the same attention and effort to locating resources and improving organisation as they do to upgrading diagnostic technologies . in order to survive , the radiologist of the near future will have to face up to the challenge of the dramatic technological revolution of the past few years . 
the advent of clinical spectroscopy , functional techniques in mri and us , quantitative and volumetric analyses with various digital techniques , optical imaging [ 20 ] , molecular imaging [ 21 ] , nanotechnologies [ 22 ] , the internet revolution [ 23 ] , percutaneous gene therapy [ 24 ] and the need for strategic planning [ 25 ] , all this calls for a parallel revolution in professional education and training . 
this is the task of the speciality schools that , to ensure the survival of radiologists , need to foster a diagnostic culture that goes beyond macroscopic anatomy and l . 
dalla palma : tomorrows radiologist : what future ? nel quadro della clinicizzazione si inserisce anche la necessit di recuperare il ruolo del radiologo intervenzionale che per la sua attivit necessita di alcuni letti di degenza e di un ambulatorio per il follow - up : il paziente che deve essere sottoposto ad una procedura intervenzionale percutanea deve essere adeguatamente preparato prima dellintervento e adeguatamente assistito dopo la procedura e tenuto sotto controllo nel follow - up per stabilire lefficacia o meno di quanto il radiologo ha fatto . 
anche in questo caso il paziente avr del radiologo la percezione che stato determinante nella soluzione del suo problema e che pu affidarsi a lui anche per il follow - up successivo : in altre parole diviene anche il suo medico curante . 
ovvio che il radiologo o lo staff radiologico deve essere competente per tutte le procedure intervenzionali vascolari , urologiche , gastroenterologiche , etc . , avere il suo laboratorio cateteri e assicurare un costante controllo di qualit . 
va tenuto presente che nella battaglia di campo il radiologo ha il vantaggio di disporre di varie tecniche di imaging utili a guidare la procedura intervenzionale e pu godere del favore degli amministratori dellospedale che in unattivit concentrata in ununica struttura dedicata full - time vedranno la soluzione pi convincente da un punto di vista economico . 
lattivit infatti condotta da chirurghi vascolari o addominali unattivit part - time perch il maggior tempo dedicato alla sala operatoria e / o al reparto : ne deriva che la struttura per lattivit intervenzionale che lavora part - time sottoutilizzata e comporta quindi un maggior costo di gestione . 
un altro limite degli specialisti non radiologi che eseguono attivit intervenzionale rappresentato dal fatto che in generale questo specialista non esercita tutta lattivit intervenzionale ma si limita a quella specifica del proprio settore di competenza . 
in altre parole nellaggiornamento della struttura il responsabile dovr dedicare alla radiologia interventistica la stessa attenzione e lo stesso impegno nella ricerca delle risorse e nel miglioramento dellorganizzazione che vengono dedicati allaggiornamento della tecnologia diagnostica . il radiologo del futuro oramai alle porte per sopravvivere deve saper affrontare e gestire la strepitosa rivoluzione tecnologica di questi ultimi anni . 
lavvento della spettroscopia clinica , delle tecniche funzionali in risonanza magnetica e in ecografia , delle analisi quantitative e volumetriche con le varie tecniche digitali , dellimaging a luce ottica [ 20 ] , dellimaging molecolare [ 21 ] , delle nanotecnologie [ 22 ] , della rivoluzione elettronica con luso di internet [ 23 ] , lavvento della terapia genica percutanea [ 24 ] , lesigenza di una cultura gestionale strategica [ 25 ] , tutto ci richiede una parallela rivoluzione nella formazione professionale . 
ci compito delle scuole di specializzazione che devono realizzare , per la sopravvivenza del radiologo , una cultura diagnostica che non deve limitarsi allanatomia e patologia macroscopica ma deve allargarsi alle strutture microscopiche e submicroscopiche : limaging molecolare ne un esempio . 
dalla palma : tomorrows radiologist : what future ? pathology to incorporate all microscopic and submicroscopic structures : molecular imaging is one example . this form of diagnostics based on microscopic or submicroscopic images opens the way for diagnosing diseases in the early , asymptomatic stage at the cellular level . 
we therefore need to strengthen the teaching of the basic sciences chemistry , biochemistry , physics , informatics and genetics by relying on experts who cannot limit themselves to teaching theory but will have to help the radiologist apply these new techniques in clinical practice . 
it has been reported that 90% of pet machines sold in europe are pet / ct machines [ 26 ]  . with regard to this technology , there is the problem of reporting , which in most cases is done by the nuclear medicine specialist and the radiologist for their respective competences . 
if most of this activity is currently represented by oncological diagnostics ( detection , staging and follow - up of lesions ) , the most convincing research on molecular imaging has been carried out with pet , as well as with very - high - field mri ( 47 tesla ) for experimental studies . how will the radiologist survive this revolution ? surely by acquiring a new culture but above all by interacting closely with the nuclear physician [ 27 ]  . 
in some countries , such as italy , these new technologies reopen the need to bring together diagnostic imaging and nuclear medicine in the same department , as is already the case in most north american and british hospitals . 
the mere number of modalities available for morphofunctional diagnostic imaging makes the need to combine a basic specialist culture with superspecialist organ - specific knowledge even more pressing . radiology residents need to be involved not only in learning but also in research on the grounds that todays research is tomorrows clinical practice [ 28 ]  . 
until now , research has taken its cue from the advent and evolution of digital technologies and has focused on the creation of a new semiology and on the evaluation of diagnostic accuracy . 
as marano states [ 29 ] , this is research funded by the market rather than by the university and scientific institutions on projects and protocols endorsed by them . there is virtually a complete lack of hypothesis - driven basic research . 
the reasons for this are several , the most important being a lack of specific training in specialty schools and a lack of funds , which have been mostly diverted towards biological , scientific , and clinical centres . 
if we want competitive radiologists capable of driving the development of diagnostic imaging , a field that clinicians find so appealing as to want to invade it , we need to reverse the situation and train ranostro ruolo nella diagnosi precoce mediante tecniche quali ecografia , tac ed rm . 
necessario quindi potenziare linsegnamento delle scienze di base chimica , chimica biologica , fisica , informatica e genetica coinvolgendo gli esperti di queste discipline che non devono limitarsi ad un insegnamento teorico ma devono affiancare il nuovo radiologo nella messa a punto clinica delle nuove tecniche . 
linsegnamento di queste discipline fondamentale ad esempio per una corretta gestione della tomografia ad emissione di positroni ( pet ) oggi sempre pi abbinata alla tomografia computerizzata ( tc )  . si ritiene che in europa il 90% delle macchine pet vendute sia rappresentato da macchine pet / tc [ 26 ]  . 
se al momento la maggior parte di questa attivit rappresentata dalla diagnostica oncologica ( riconoscimento di lesione , stadiazione e follow - up ) , alla pet fanno capo le ricerche pi convincenti di imaging molecolare , cui si affiancano , a livello sperimentale , quelle con rm ad altissimo campo , 47 tesla . 
queste nuove tecnologie riaprono in alcuni paesi come il nostro la necessit di vedere nello stesso dipartimento la radiodiagnostica e la medicina nucleare , organizzazione gi operante nella maggioranza degli ospedali nord - americani ed inglesi . 
il numero delle tecnologie disponibili per la diagnostica dimmagine morfo - funzionale rende ancor pi attuale lesigenza di una cultura specialistica di base affiancata da una cultura superspecialistica dorgano . fondamentale che lo specializzando venga coinvolto oltre che nellinsegnamento anche nella ricerca ricordando che la ricerca oggi pratica clinica domani [ 28 ]  . 
sinora la ricerca ha preso spunto dalla comparsa ed evoluzione delle tecnologie digitali e si basata sulla messa a punto di una nuova semeiotica e sulla valutazione dellaccuratezza nella diagnosi di patologia . 
si tratta nella gran parte dei casi di ricerca sponsorizzata dallindustria e da questa ispirata , e quindi di ricerca finalizzata ad ottenere ricadute socio - economiche a breve e medio termine . 
si tratta quindi , come dice marano [ 29 ] , di una ricerca finanziata dal marketing e non dalluniversit e istituzioni scientifiche su progetti e protocolli da queste avvallati . 
certamente in radiologia abbiamo sofferto questo aspetto per diverse ragioni , anzitutto per la mancanza di training specifico nelle scuole di specializzazione e in secondo luogo per la mancanza di finanziamenti , diretti prevalentemente alle strutture biologiche , scientifiche e cliniche . 
se vogliamo avere radiologi competitivi allaltezza di guidare lo sviluppo della diagnostica per immagini , che sempre pi affascina i nostri colleghi clinici al punto da invadere il campo dellimaging , necessario rovesciare la situazione formando un gruppo di radiologi preparati alla ricerca . 
the research training model devised by arenson , dunnick and hillman in the united states [ 30 ] and discussed and approved by the society of chairmen of academic radiology departments is interesting . 
in this case , residents follow programme 2 of the previous class . after the presentation , the society of chairmen of academic radiology departments drew the following conclusions : 1 . 
nellambito di un programma nazionale di educazione alla ricerca sono state identificate 3 categorie di dipartimento e precisamente : categoria 1 : comprende dipartimenti di radiologia con forte storia di ricerca competitiva e dotati di finanziamenti per supportare lavviamento e la formazione di ricercatori . il programma in questo caso prevede almeno un anno e preferibilmente due anni di ricerca che comprende : 1 . 
insegnamento a preparare richieste di finanziamento per progetti di ricerca . categoria 2 : comprende dipartimenti che hanno annualmente finanziamenti per coprire i costi dello sviluppo , di ricerca e di training di ricerca . 
almeno 3 mesi di esperienza nella ricerca seguiti dalla preparazione di un manoscritto da pubblicare che pu esser pronto 3 mesi dopo aver completato il tirocinio di ricerca ; 2 . 
un ciclo di lezioni , di presentazioni di ricerca ed esercizi di pensiero critico che sottolinea l ' importanza della ricerca nella pratica clinica . categoria 3 : comprende dipartimenti con modeste risorse umane , di ricerca e finanziarie per educare adeguatamente ricercatori competitivi . 
ogni dipartimento viene richiesto di assegnarsi la categoria di appartenenza e si invitano quelli di categoria inferiore ad adoperarsi per un avanzamento . gli autori cos concludono : il futuro della radiologia l . 
dalla palma : tomorrows radiologist : what future ? the authors conclude : the future of radiology depends on the training of a new class of radiologists who are clinicians and scientists . continuing education is extremely important . 
web - based learning is very appealing : education is widely available , inexpensive ( or free ) , always accessible , regularly updated and a huge amount of educational materials are available [ 23 ]  . 
constant technological developments and critical review of knowledge force radiologists to use web sites for their continuing education , but not all web sites undergo quality control and peer review . 
accuracy of the presentation is especially important . the authors also present four broad categories of web sites for radiology : ( 1 ) metalink sites provide a large number of links on a single portal ; ( 2 ) sites with teaching files , similar to our eurorad ; ( 3 ) subspecialty sites , such as those devoted to skeletal radiology , nuclear medicine etc . ; ( 4 ) technique - based sites , such as those devoted to multislice ct . 
the internet provides radiologists with an infinite learning resource that allows them to keep up - to - date with recent developments . in conclusion , to survive the tendency of other specialists to invade and occupy the radiology turf , the radiologist of the very near future will have to live up to the challenge by : 1 . 
becoming familiar with the basic sciences , physics , chemistry , biochemistry , genetics , informatics and nandipende dalla formazione di una nuova categoria di radiologi clinici e scienziati . estremamente importante l ' aggiornamento professionale : oggi una larga parte dei congressi , convegni e corsi sono accreditati e quindi sono la garanzia di un aggiornamento serio . 
l ' apprendimento basato sulla ricerca web molto attraente : l ' aggiornamento disponibile su larga scala , poco costoso ( o gratuito ) , accessibile in ogni momento , regolarmente aggiornato ed disponibile una vasta quantit di materiale educativo [ 23 ]  . 
la costante evoluzione tecnologica e revisione critica del sapere costringe il radiologo ad utilizzare per l ' aggiornamento i siti web che peraltro non hanno tutti un controllo di qualit e quindi un comitato di revisori . 
il radiologo insomma trova in internet una fonte di apprendimento inesauribile che gli consente un aggiornamento costante . in conclusione il radiologo del futuro che gi iniziato se vuole sopravvivere alla tendenza di altri specialisti di invadere ed occupare il campo della diagnostica per immagini deve affrontare nuove realt quali : 1 . 
dalla palma : tomorrows radiologist : what future ? otechnologies to be able to take on board new imaging techniques , such as molecular imaging , and new forms of percutaneous treatment , such as gene therapy 4 . 
fostering a multidisciplinary approach in his or her practice , made increasingly complex by technological advances : interaction with the nuclear physician is one of the first approaches determined by pet technology and pet / ct 5 . 
acquisire la dimestichezza di navigare in internet per favorire l ' apprendimento e l ' aggiornamento su siti web dedicati e disponibili in ogni momento . l ' apprendimento costante in una disciplina in continua evoluzione imperativo . 
salvatore dipartimento di scienze biomorfologiche e funzionali ( dsbmf ) , universit degli studi di napoli federico ii ( unina ) , istituto di biostrutture e bioimmagini ( ibb ) , consiglio nazionale delle ricerche ( cnr ) , napoli , italy correspondence to : s . 
maurea , via raffaele de cesare 7 , i - 80132 napoli , italy , tel . : + 39 - 081 - 7463560 / 2356 , fax : + 39 - 081 - 5457081 / 2296117 , e - mail : simone.maurea.@unina.it received : 26 september 2005 / accepted : 8 march 2006 / published online : 29 june 2006 abstract purpose . 
histology ( n = 19 ) , biopsy ( n = 3 ) or clinical - imaging follow - up ( n = 19 ) demonstrated 29 adenomas , five pheochromocytomas , three cysts and four carcinomas . 
axial and coronal imaging planes were used , with a slice thickness of 35 mmr images were qualitatively assessed for signal intensity of the adrenal mass relative to the liver on t1 , t2 , cs and t1 - gd scans ; diagnostic criteria for adenomas were isointensity or hypointensity on both t1 and t2 scans , out - of - phase cs signal loss and mild transient enhancement after gd . 
analysis of t1t2 signal intensity showed diagnostic accuracy , sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) of 80% , 72% , 100% , 100% and 60% , respectively . 
sono stati arruolati 36 pazienti ( 9 m , 27 f , et media = 51 , 314 , 4 anni ) con tumori surrenalici a sede unilaterale ( n = 31 ) o bilaterale ( n = 5 ) identificati incidentalmente nel corso dellesecuzione di altri esami dimaging ( ecografia , tc ) eseguiti per altre indicazioni cliniche . 
i risultati del nostro studio suggeriscono che la sequenza cs migliora significativamente laccuratezza diagnostica della rm nella identificazione degli adenomi surrenalici in confronto alle sequenze convenzionali t1 e t2 s . 
in particular , adenomas showed signal hypointensity relative to liver parenchyma on both t1 and t2 scans whereas pheochromocytoma , cysts and adrenal metastasis displayed signal hypointensity on t1 scans and hyperintensity on t2 scans . 
quantitative analysis of signal intensity of adrenal lesions compared with that of the liver , fat , muscle and image background was subsequently shown to improve characterisation of adrenal masses compared with qualitative analysis of signal variations [ 15 ]  . 
 the use of gadolinium ( gd ) , an intravenous paramagnetic contrast agent with extracellular distribution , made it possible to assess the enhancement pattern of tumor masses on the basis of signal variations induced by the contrast agent [ 1 , 7 ]  . compared with metastatic lesions , adrenal adenomas showed early arterial - phase enhancement followed by rapid washout [ 1 ]  . 
recently , a new mr imaging sequence known as chemical shift ( cs ) has been proposed , which is based on the different lipid content of adrenal lesions of a different histological nature [ 1 , 2 , 8 , 9 ]  . we report our experience with patients with adrenal masses to assess diagnostic accuracy of the cs sequence in differential diagnosis between adenoma and non adenoma lesions compared with conventional precontrast t1 and t2 scans and t1 scans after the administration of paramagnetic contrast material . materials and methods population a total of 36 patients ( 9 men , 27 women , mean age 51.314.4 years ) with adrenal masses were prospectively studied by mr of the upper abdomen . 
patients with adrenal masses documented by imaging studies were included ; in particular , the masses had been incidentally discovered during ultrasound ( us ) and / or ct performed for other clinical indications ( table 1 )  . 
a total of 41 materiali e metodi popolazione la risonanza magnetica ( rm ) stata proposta come valida alternativa alla tomografia computerizzata ( tc ) come tecnica di diagnostica per immagini per la caratterizzazione delle formazioni espansive a sede surrenalica [ 13 ]  . 
inizialmente , lesecuzione dellesame stata proposta mediante limpiego di sequenze t1 e t2 pesate che consentivano di valutare le variazioni del segnale rm come indice di tipizzazione tessutale [ 1 ] ; in particolare , gli adenomi hanno mostrato una ipointensit di segnale rispetto al parenchima epatico sia in t1 che t2 ; al contrario , il feocromocitoma , la cisti e le metastasi surrenaliche hanno mostrato unipointensit di segnale in t1 associata ad una iperintensit di segnale in t2 . 
successivamente , lanalisi quantitativa dellintensit del segnale rm delle lesioni surrenaliche in rapporto a quella del tessuto epatico , adiposo , muscolare e del fondo dellimmagine stata suggerita come pi valido approccio per la caratterizzazione delle masse surrenaliche rispetto allanalisi qualitativa delle modifiche del segnale [ 15 ] ; tuttavia anche questo tipo di analisi ha mostrato dei risultati non completamente soddisfacenti in quanto sovrapponibili tra lesioni di diversa natura [ 6 ]  . 
lutilizzo del gadolinio , mezzo di contrasto paramagnetico a distribuzione extra - cellulare somministrato per via endovenosa , ha consentito di valutare la dinamica del grado di impregnazione delle formazioni espansive in base alle modifiche del segnale indotte dal mezzo di contrasto [ 1 , 7 ] ; a tale proposito , gli adenomi surrenalici hanno mostrato una precoce impregnazione di gadolinio in fase arteriosa associata ad una rapida dismissione del mezzo di contrasto paramagnetico rispetto alle lesioni metastatiche [ 1 ]  . 
negli ultimi anni , stata proposta una nuova sequenza di acquisizione delle immagini rm , la sequenza chemical - shift ( cs ) , basata sulle differenze nel contenuto lipidico di lesioni surrenaliche di diversa natura istologica [ 1 , 2 , 8 , 9 ]  . 
riportiamo in questo studio la nostra esperienza in pazienti con formazioni espansive a sede surrenalica allo scopo di valutare laccuratezza diagnostica della sequenza cs per la diagnosi differenziale tra lesioni adenomatose e non - adenomatose in confronto alle sequenze convenzionali t1 e t2 pesate eseguite in fase pre - contrastografica e alla sequenza t1 dopo mezzo di contrasto paramagnetico . sono stati studiati prospetticamente con rm delladdome sus . 
in the remaining 19 patients with lesions smaller than 3 cm , clinical - imaging follow - up yielded a diagnosis of adenoma ( n = 17 ) or pheochromocytoma ( n = 2 )  . periore 36 pazienti con formazioni espansive a sede surrenalica ( 9 m , 27 f , et media = 51 , 314 , 4 anni ) , di cui 31 con lesioni a sede monolaterale e 5 con lesioni a sede bilaterale ; il criterio di inclusione dei pazienti nel gruppo di studio consisteva nellevidenza di lesioni espansive a sede surrenalica , documentate dal risultato di esami di diagnostica per immagini ; in particolare , i tumori surrenalici sono stati identificati incidentalmente nel corso di ecografia e / o tc eseguiti per altre indicazioni cliniche ( tabella 1 )  . 
sono state valutate in totale 41 lesioni ( diametro medio 3 , 02 , 2 cm ) e sono stati utilizzati come standard di riferimento per la diagnosi di natura i risultati istologici ( n = 19 ) , bioptici ( n = 3 ) o del follow - up clinico - strumentale ( n = 19 ) ; il follow - up clinicostrumentale comprendeva i dosaggi ormonali specifici della funzione ghiandolare ( corticale e / o midollare ) surrenalica , s . 
all examinations were carried out with 3to 5mm - thick axial and coronal scans ; more specifically , slice thickness was 5 mm for axial scans and 3 mm for coronal scans . 
the studies were integrated with cs t1 - dual - ffe sequences with a tr of 236 ms and double te of 4.6 ms in phase and 2.3 ms out of phase in the axial plane . 
axial t1 - ffe - bh il monitoraggio dimensionale delle lesioni mediante ecografia e / o tc ed esame scintigrafico della zona corticale e / o della zona midollare dei surreni ; in particolare , la mediana della durata del follow - up stata uguale a 5 mesi ( intervallo compreso tra 3 e 8 mesi )  . 
lesame istologico ha mostrato la presenza di adenoma ( n = 10 ) , feocromocitoma ( n = 3 ) , carcinoma ( n = 3 ) e cisti ( n = 3 ) ; lesame bioptico ha dimostrato la presenza di 2 adenomi e 1 carcinoma ; nei rimanenti 19 pazienti , con lesioni di dimensioni inferiori ai 3 cm , il followup clinico - strumentale ha consentito di formulare la diagnosi di adenoma ( n = 17 ) o di feocromocitoma ( n = 2 )  . risonanza magnetica gli esami rm sono stati effettuati utilizzando un apparecs . 
administration of extracellular paramagnetic contrast agent ( gadolinium chelates , 0.1 mmol / kg body weight ) using a dynamic technique with preset scan times and image acquisition in the arterial ( 30 s ) , portal ( 60 s ) and late equilibrium phases ( 180300 s )  . image and data analysis mr images were qualitatively analysed by two radiologists who assessed both the preand postcontrast signal intensity of adrenal lesions relative to that of the liver parenchyma ; for three cases in which there was no agreement , a third radiologist was consulted . 
imaging signs considered diagnostic of adenoma were : t1 and t2 isoor hypointensity , cs signal loss ( definite hypointensity ) on out - of - phase images relative to in - phase images and early enhancement during the postcontrast arterial phase with rapid washout during the following phases [ 13 ]  . results of the qualitative analysis of t1t2 , cs and postcontrast t1 mr images were compared with histological , biopsy and follow - up data defining the nature of the adrenal lesions ( pheochromocytoma , adenoma , cyst , myelolipoma and malignancies )  . 
in particular , we compared the results of t1t2 images , cs in - phase and outof - phase images and postcontrast t1 images . we calculated accuracy , sensitivity and specificity values , as well as positive ( ppv ) and negative predictive values ( npv ) in the three series of images ( t1t2 , in - phase and out - of - phase cs and postcontrast t1 )  . statistical analysis to assess statistical significance of the differences observed in accuracy , sensitivity , specificity , ppv and npv among the three series of mr images ( t1t2 , cs and postcontrast t1 ) , we used the mcnemar test ; a value of p < 0.05 was taken to be statistically significant . results results of qualitative analysis of t1t2 signal intensity performed for each lesion are shown in table 2 . 
gli esami sono stati integrati con sequenza cs t1 - dual - ffe con tr di 236 ms e doppio te di 4 , 6 ms in - fase e 2 , 3 ms in - opposizione di fase secondo il piano assiale . la sequenza t1 - ffe - bh , in piani di scansione assiali stata ripetuta dopo somministrazione endovenosa di mezzo di contrasto ( mdc ) paramagnetico a distribuzione extra - cellulare ( chelati di gadolinio , 0 , 1 mmol / kg di peso corporeo ) con tecnica dinamica a tempi pre - fissati ed acquisizione di immagini in fase arteriosa ( 30 s ) , in fase portale ( 60 s ) e in fase tardiva allequilibrio ( 180300 s )  . analisi delle immagini e dei dati le immagini rm sono state analizzate qualitativamente da due medici radiologi valutando le caratteristiche di intensit del segnale delle lesioni surrenaliche , sia in fase preche post - contrastografica , in rapporto allintensit del segnale del parenchima epatico ; in tre casi in cui si verificata discordanza di interpretazione delle immagini , stato consultato un terzo medico radiologo . 
lintensit del segnale rm delle lesioni surrenaliche in t1 e t2 stata classificata come isointensa , ipointensa , lievemente o nettamente iperintensa rispetto a quella del tessuto epatico . gli studi rm acquisiti con sequenza cs sono stati valutati qualitativamente in base alla variazione di intensit del segnale delle lesioni surrenaliche tra le immagini in - fase e quelle in - opposizione di fase ; stata considerata come significativa una variazione dellintensit del segnale rm in termini di netta ipointensit ( perdita di segnale ) in - opposizione di fase rispetto alle immagini in - fase . 
sono state , inoltre , valutate le modifiche dellintensit di segnale delle lesioni surrenaliche nelle diverse fasi ( arteriosa , portale e tardiva allequilibrio ) post - contrastografiche ; il grado di impregnazione di mdc stato classificato come assente , lieve o netto . sono stati considerati criteri semeiologici diagnostici per adenoma lisoo lipo - intensit sia in t1 che in t2 , la perdita di segnale ( netta ipointensit ) in - opposizione di fase rispetto alle immagini in - fase in sequenza cs e la precoce impregnazione di mdc in fase arteriosa post - contrastografica con rapida dismissione di mdc nelle successive fasi di studio [ 13 ]  . 
one of the aims of medical research in this field is to investigate the possibility of characterising adrenal lesions by using imaging methods so as to avoid the need for biopsies [ 12 ]  . mr is one of the most accurate methods for morphofunctional evaluation of adrenal masses [ 1 ] , and one of its advananalisi statistica allo scopo di valutare la significativit statistica delle differenze osservate nei valori di accuratezza , sensibilit e specificit diagnostica , e dei valori predittivo positivo ( vpp ) e negativo ( vpn ) tra le tre serie di immagini rm ( t1 - t2 , cs e t1 dopo mdc ) stato impiegato il test di mc nemar ; un valore della p < 0 , 05 stato considerato statisticamente significativo . risultati i risultati dellanalisi qualitativa delle intensit di segnale s . 
in addition , qualitative and quantitative analyses of the mr signal , the use of paramagnetic contrast material and cs imaging constitute specific methods that allow characterisation of adrenal masses [ 1 , 48 ]  . 
the cs sequence relies on the different resonance frequencies of the hydrogen protons in tissues with a prevalent water or lipid component as a result of the electron shell around the nucleus . 
by creating a local magnetic field , this electron shell forms a shield that depends on the density and spatial distribution of electrons and interferes with the main magnetic field [ 9 ]  . 
by modifying the te , water and fat protons may be in phase ( longer te ) or out of phase ( shorter te ) , leading to differences in signal intensity that allow identification of prevalently fatty adrenal adenomas out of phase , with significant signal reduction with respect to in - phase images . in our experience , use of the cs sequence or postcontrast t1 sequence succeeded in reducing the rate of false negatives in the identification of adrenal adenomas compared with conventional t1and t2 - weighted sequences . 
in dettaglio , la differente incidenza di risultati falsamente negativi nel confronto tra le immagini rm t1 - t2 , in cs e t1 dopo mdc ha determinato la significativit statistica in termini di accuratezza , sensibilit e vpn tra le tre serie di immagini rm . discussione in pazienti con formazioni espansive a sede surrenalica , laspetto clinico fondamentale rappresentato dal riconos . 
la lesione si presenta isointensa al parenchima epatico sia nelle scansioni assiali ffe t1 pesate ( a ) che in quelle tse t2 pesate ( b ) : risultato t1 - t2 vero positivo . zation of adrenal adenomas and obviates the need for the postcontrast t1 sequence . clinical applications of the cs sequence are based on the different lipid content of benign and malignant adrenal lesions [ 1117 ] ; in particular , adrenal adenomas have a higher lipid concentration than metastases . 
the variability of fat content of adenomas may lead to heterogeneous signal alterations on out - of - phase images relative to in - phase images [ 13 ]  . 
in addition , the possible presence of a lipid component in malignant adrenal lesions may result in reduced out - ofphase signal similar to that seen in adenomas and therefore lead to false positive results at cs imaging [ 14 ]  . 
we had three cases of false positive adenomas at cs imaging ; in these patients , lower fat content might have accounted for the different pattern out of phase [ 13 ]  . 
nonetheless , the low false negative rate of cs imaging led to significantly better accuracy and sensitivity values compared with conventional t1t2 sequence such that the cs sequence increased the diagnostic potential of the mr examination . 
accuracy , sensitivity and specificity values in this study were 94% , 89% and 99% , respectively , resulting in high predictive values for the cs sequence in the characterization of adrenal adenomas . a further possibility offered by the cs sequence is the scimento della natura benigna o maligna di tali lesioni allo scopo di definire la terapia adeguata [ 10 ]  . 
numerose tecniche di diagnostica per immagini possono essere utilizzate nella valutazione morfo - funzionale di tali pazienti , quali la tc , la rm e le metodiche radionuclidiche [ 1 , 6 , 11 ]  . 
uno degli obiettivi della ricerca medica in tale settore rappresentato dalla possibilit o meno di ottenere informazioni per la caratterizzazione tessutale delle lesioni surrenaliche utilizzando queste metodiche strumentali allo scopo di evitare lesecuzione di un esame bioptico [ 12 ]  . 
la rm rappresenta una delle metodiche pi accurate per la valutazione morfofunzionale delle lesioni espansive a sede surrenalica [ 1 ] , in particolare , le scansioni multiplanari rappresentano uno dei vantaggi di questa tecnica rispetto alle altre metodiche ; inoltre lanalisi qualitativa e quantitativa del segnale rm , limpiego del mdc paramagnetico e le sequenze cs costituiscono aspetti tecnici specifici per la caratterizzazione tissutale delle masse surrenaliche [ 1 , 48 ]  . 
la sequenza chemicalshift si basa , in particolare , sulla differente frequenza di risonanza dei protoni di idrogeno nei tessuti a prevalente componente fluida o adiposa in dipendenza della nube elettronica che circonda il nucleo ; tale nube elettronica , creando un campo magnetico locale , determina una schermatura , dipendente dalla densit e dalla distribuzione spaziale degli elettroni , che interferisce con lazione del campo magnetico principale [ 9 ]  . 
i protoni di idrogeno dei tessuti di tipo fluido sono meno schermati verso il campo magnetico esterno rispetto a quelli dei tessuti a componente adiposa ; ci determina che i protoni dei tessuti di tipo fluido hanno una maggiore frequenza di risonanza e , dunque , un segnale pi elevato . 
modificando il tempo di eco ( te ) della sequenza possibile che i protoni dei tessuti di tipo fluido e quelli di un tessuto a prevalente contenuto adiposo siano in - fase ( te pi lungo ) o in - opposizione di fase ( te pi breve ) realizzando delle differenze di intensit tali da poter identificare in - opposizione di fase gli adenomi surrenalici a prevalente componente adiposa e , dunque , con significativa riduzione di segnale rispetto alle immagini in - fase . 
nella casistica riportata ed in base alla nostra esperienza limpiego della sequenza cs o della sequenza t1 dopo mdc ha consentito di ridurre lincidenza dei risultati rm falsamente negativi , rispetto alle immagini convenzionali t1 e t2 pesate , nella corretta identificazione delle lesioni adenomatose delle ghiandole surrenaliche . 
la significativit statistica delle differenze in accuratezza , sensibilit e vpn della sequenza cs e t1 dopo mdc rispetto alle sequenze convenzionali t1 - t2 suggerisce certamente un ruolo clinico diagnostico dellimaging rm in cs per la caratterizzazione degli adenomi surrenalici senza la necessit di ricorrere allimpiego della sequenza t1 post - contrastografica . 
le applicazioni cliniche della sequenza cs si basano sulle differenze del contenuto lipidico tra lesioni surrenaliche benigne e maligne [ 1117 ] ; in particolare , stata osservata una maggiore concentrazione di lipidi negli adenomi surrenalici rispetto alle metastasi . la sequenza cs pu , tuttavia , presentare alcune limitazioni ; infatti , il contenuto lipidico variabile degli adenomi pu determinare una eterogeneit delle modifiche del segnale rm in - opposizione di fase rispetto alle immagini infase [ 13 ]  . 
the index is calculated on the basis of the difference between signal intensity in phase and out of phase divided by signal intensity in phase [ 2 , 16 ]  . 
in more detail , adenomas were shown to have an index of 0.36 , corresponding to 27% fat , whereas metastatic lesions or pheochromocytomas had negative signal - intensity indexes , with values corresponding to 0% fat [ 16 ]  . 
this method for quantitative assessment of signal intensity was found to be more accurate than calculating the differences in signal intensity between adrenal lesions and that of other locoregional tissues , such as liver , spleen and muscle [ 17 ]  . 
i nostri risultati hanno mostrato tre casi falsamente negativi per lesione adenomatose in sequenza cs ; in tali pazienti , la minore concentrazione lipidica potrebbe giustificare il diverso comportamento in - opposizione di fase [ 13 ]  . 
tuttavia la bassa incidenza di risultati falsi negativi in sequenza cs ha determinato valori di accuratezza e sensibilit significativamente superiori rispetto alla sequenza convenzionale t1 - t2 , tali da realizzare un incremento delle potenzialit diagnostiche dellesame rm utilizzando tale sequenza . 
i risultati del nostro studio concordano con quelli di uno studio recentemente pubblicato riguardo un significativo gruppo di pazienti con masse surrenaliche valutate qualitativamente con la sequenza cs [ 15 ] ; in tale esperienza , gli autori hanno studiato 182 pas . 
t1 - fast field echo ( ffe ) axial dynamic scans with fat suppression before gadolinium ( gd ) administration ( a ) , and in arterial ( b ) and delayed ( c ) phases after gd administration . 
scansioni assiali in sequenza dinamica ffe t1 pesata con soppressione del segnale del tessuto adiposo in fase pre - contrastografica ( a ) , in fase arteriosa post - contrastografica dopo gadolinio ( b ) e in fase tardiva post - contrastografica dopo gadolinio ( c )  . 
la lesione mostra precoce impregnazione contrastografica in fase arteriosa ( b ) con associata rapida dismissione contrastografica in fase tardiva ( c ) : risultato rm t1 - gadolinio vero positivo . zienti riportando valori di accuratezza , sensibilit e specificit diagnostica della sequenza cs analoghi a quelli da noi osservati , rispettivamente 94% , 89% e 99% che comportavano elevati valori di predittivit diagnostica della sequenza cs per la caratterizzazione degli adenomi surrenalici . una ulteriore possibilit metodologica della sequenza rm in cs rappresentata dalla valutazione quantitativa delle variazioni dellintensit di segnale in - opposizione di fase rispetto alle immagini in - fase mediante il calcolo dellindice di intensit di segnale di una lesione surrenalica adenomatosa o non - adenomatosa ; tale indice viene calcolato in base alla differenza tra lintensit di segnale in - fase e quella inopposizione di fase diviso lintensit di segnale in - fase [ 2 , 16 ] ; stato dimostrato che tale indice espressione della percentuale in contenuto adiposo della lesione , tale che lindice di intensit di segnale pari a 1 corrisponde ad una quota adiposa di circa il 90% ; in particolare , gli adenomi hanno mostrato un indice pari a 0 , 36 che corrispondeva ad una frazione adiposa di circa il 27% , mentre le lesioni metastatiche o i feocromocitomi mostravano indici di intensit di segnale negativi con valori corrispondenti di percentuale adiposa pari a zero [ 16 ]  . 
questo metodo di valutazione quantitativa dellintensit di segnale risultato essere pi accurato rispetto al calcolo dei rapporti tra lintensit di segnale della lesione surrenalica e quella di altri tessuti loco - regionali , quali il tessuto epatico , splenico e muscolare [ 17 ]  . 
in base ai recenti dati riportati in letteratura [ 18 ] , la rm con sequenza cs ha mostrato un suo ruolo specifico nei casi in cui la tc non consente di caratterizzare con certezza una les . 
da ronch , istituto di radiologia apugd , via colugna 50 , i - 33100 udine , italy , e - mail : tdaronch@sirm.org received : 9 june 2005 / accepted : 17 november 2005 / published online : 29 june 2006 abstract purpose . 
between august 2000 and september 2004 , we conducted a retrospective study of the abdominal ct of 15 patients with histological diagnosis of gist that is , the immunopositivity for c - kit ( cd117 ) on a surgical specimen of the primary disease . 
we used a helical ct single - slice ( toshiba , asteion ; rotation time 0.75 s ) in ten cases and helical ct multislice ( toshiba , aquilion ; 4 slices / rotation ; rotation time 0.5 s ) in five cases . 
size , partial or total extraluminal tumour growth , homogeneous or inhomogeneous lesion enhancement and the eventual presence of calcifications were assumed to be criteria for characterisation of a gist . 
we demonstrated one substantial concordance between radiological and pathological valuation of site , morphology , tumour size and absence of intralesional calcifications of gist . nine of ten gist smaller than 5 cm , the two 510 cm and the three larger than 10 cm presented extraluminal growth . enhancement was inhomogeneous in five of ten lesions smaller than 5 cm and in all cases larger than 5 cat pathological analysis , in all cases of inhomogeneous enhancement , solid , hemorrhagic , necrotic and cystic areas were found . 
of seven tumours of intermediate malignancy , six were smaller than 5 cm and only one larger than 10 cm ; the two 510 cm were of high malignancy and all tumours superior of 10 cm were at intermediate or high malignancy . 
si sono prese in considerazione , mediante studio retrospettivo , le tc addominali di 15 pazienti con diagnosi istologica di gist sul pezzo operatorio in malattia primitiva , in un periodo compreso tra agosto 2000 e settembre 2004 . 
le apparecchiature tc usate sono state una spirale a singolo strato ( tcss ) ( toshiba , asteion ; tempo di rotazione 0 , 75 s ) in 10 casi ed una multistrato ( tcms ) ( toshiba , aquilion ; 4 strati / rotazione ; tempo di rotazione 0 , 5 s ) in 5 . 
in tutti i casi stato utilizzato un mezzo di contrasto ( mdc ) organo - iodato non ionico ad una concentrazione di iodio variabile da 350 a 400 mgi / ml per via endovenosa . 
la sede , la morfologia e le dimensioni ( classificate in tre gruppi : inferiori a 5 cm , comprese tra 5 e 10 cm e superiori a 10 cm ) sono stati considerati parametri per lidentificazione della neoplasia ; le dimensioni , lo sviluppo parzialmente o francamente estrinseco , lenhancement omogeneo o disomogeneo della lesione e leventuale presenza di calcificazioni al suo interno sono stati assunti come criteri di caratterizzazione di un gist ; la presenza di metastasi epatiche , peritoneali e / o linfonodali stata considerata parametro di malignit intermedia o elevata . 
si dimostrata una sostanziale concordanza tra valutazione radiologica ed anatomo - patologica per quanto riguarda la sede , la morfologia , le dimensioni dei gist e lassenza di calcificazioni intralesionali . 
tumour size established with ct was not sufficient to determine the degree of malignancy . metastases at the time of diagnosis were indicative of intermediate or high malignancy , but the absence of metastases did not allow classification of gist in the group of low and very low risk of malignancy . key words gist helical ct stomach bowel liver tutti i casi di enhancement disomogeneo , allanalisi del pezzo operatorio si sono trovate aree sia solide , che necrotiche , emorragiche e / o cistiche . 
delle 7 neoplasie a rischio intermedio di malignit 6 erano inferiori a 5 cm e solo 1 superiore a 10 cm , 2 su 2 di dimensioni tra 5 e 10 cm rientravano nel gruppo a rischio elevato e tutte quelle superiori a 10 cm rientravano nel gruppo a rischio intermedio o in quello a rischio elevato . 
la diagnosi di certezza dei gist richiede la dimostrazione dellimmunopositivit al cd117 , ma la diagnostica per immagini ed , in particolare , la tc spirale svolge un ruolo di primaria importanza . 
da questo studio emerso che la tc si rivelata attendibile nellidentificare la neoplasia , che tutti i tumori di dimensioni superiori a 5 cm presentavano uno sviluppo estrinseco , un enhancement disomogeneo , lassenza di calcificazioni e di interessamento linfonodale e che anche quelli inferiori a 5 cm tendono a presentare uno sviluppo estrinseco ed una densit disomogenea . 
after more than 50 years of controversial classification , the term gist is currently reserved for gists that are immunopositive for c - kit ( cd117 ) , a receptor for the tyrosine - kinase growth factor [ 3 , 5 , 69 , 11 ]  . 
with the exception of the presence of metastasis at diagnosis , an invariably negative prognostic factor , tumour size and mitotic index alone seem to be predictive of the benign or malignant behaviour of gist [ 3 , 8 ] , and these parameters are commonly used by pathologists for prognostic evaluation as proposed by fletcher et al . 
 [ 3 ] ( table 1 )  . gist tends to affect individuals aged over 50 years , without any gender predilection [ 7 , 9 , 12 ]  . 
although they may affect any level of the gastrointestinal tract , the most frequent site is the stomach ( 60%70% ) followed by the small bowel ( 20%30% ) , the anusrectum ( 7% ) , the colon ( 5% ) and the oesophagus ( 2% )  . 
unlike the case with many other neoplasms , the lymph nodes are not the main route of spread [ 1 , 7 , 11 , 1315 , 17 , 18 ]  . the most frequent clinical presentations are haematemesis , melaena and signs of anaemia ; bowel obstruction ; abi tumori stromali gastrointestinali ( gist ) sono le pi comuni neoplasie mesenchimali del tratto gastroenterico . 
attualmente il termine gist , dopo oltre cinquantanni di classificazioni alquanto dibattute , indica esclusivamente i tumori stromali gastrointestinali che presentano limmunopositivit al c - kit ( cd117 ) , un recettore per il fattore di crescita tirosino - kinasi [ 3 , 5 , 69 , 11 ]  . 
eccetto il fattore prognostico invariabilmente sfavorevole della presenza di metastasi al momento della diagnosi , solo le dimensioni della neoplasia ed il tasso di mitosi sembrano essere criteri predittivi di un comportamento benigno o maligno dei gist [ 3 , 8 ]  . 
the use of fast ct scanners allowing thin - slice acquisitions and high - quality multiplanar reconstructions associated with optimisation of iv contrast material enables detailed evaluation of the gastrointestinal tract as well as staging of a tumour in this area . 
in gist in particular , despite the fact that data are few and often imprecise as a result of recent introduction of immunohistochemical classification , there seem to be highly characteristics signs for these neoplasms [ 2 , 4 , 7 , 10 , 14 , 15 , 2224 ]  . as regards treatment , surgical resection when feasible is the procedure of choice given that the response rate to conventional radioand chemotherapy is negligible [ 2 , 11 , 13 ]  . however , sti - 571 [ imatinib ( gleevec ) , novartis basel , switzerland ] has recently been introduced , a drug that acts specifically on the biomolecular change at the origin of the disease by targeting tumour cells exclusively [ 1 , 5 , 7 , 12 , 13 , 2528 ]  . this drug , which appears to make the disease stable in at least 80% of cases [ 1 ] , is used in cases of inoperable gist , whether metastatic or not , and in patients with metastatic disease who have undergone surgery . 
meno frequenti sono lostruzione intestinale , il reperto palpatorio di massa addominale e il riscontro incidentale in corso di indagini eseguite per altri motivi [ 4 , 5 , 7 , 9 , 15 ]  . la diagnosi definitiva di gist istologica , per , la diagnostica per immagini ed , in particolare , la tc spirale di fondamentale importanza . 
infatti , luso di apparecchiature tc con elevata velocit di acquisizione che consentono scansioni di spessore sottile e ricostruzioni multiplanari di notevole qualit , associato allottimizzazione delliniezione endovenosa di mdc , permette una valutazione dettagliata del tratto gastrointestinale oltre che un preciso bilancio destensione di una patologia di tale distretto . 
in particolare , per quanto riguarda i gist , nonostante dati non numerosi e non sempre precisi , in relazione allintroduzione piuttosto recente del criterio immunoistochimico di classificazione , sembrano esserci reperti semeiologici altamente caratteristici di queste neoplasie [ 2 , 4 , 7 , 10 , 14 , 15 , 2224 ]  . in ambito terapeutico , la resezione chirurgica , quando praticabile , la procedura di prima scelta , anche perch il tasso di risposta alla radio e chemioterapia convenzionali insignificante [ 2 , 11 , 13 ]  . 
recentemente , per , stato introdotto il sti - 571 ( imatinib , gleevec , novartis , basel , switzerland ) un farmaco che agisce specificatamente sullalterazione biomolecolare allorigine della neoplasia aggredendo esclusivamente le cellule neoplastiche [ 1 , 5 , 7 , 12 , 13 , 2528 ]  . 
tale farmaco , che sembra stabilizzare la malattia in almeno l80% dei casi [ 1 ] , usato nei pazienti con gist inoperabili sia metastatici che non ed in quelli sottoposti ad intervento chirurgico , ma metastatici . 
essendo la definizione istogenetica dei gist di recente introduzione [ 3 ] , in letteratura non ci sono ancora numerosi studi sulle possibilit offerte dalla tc spirale nella valutazione di queste neoplasie . lo scopo di questo lavoro , pertanto , stato valutare laccuratezza diagnostica della tc spirale nella identificazione , caratterizzazione e nel bilancio destensione dei gist mediante la correlazione con alcuni aspetti anatomo - patologici degli stessi . materiali e metodi si sono prese in considerazione , mediante studio retrospettivo , le tc addominali di 15 pazienti , di cui 8 maschi e 7 femmine di et compresa tra 23 anni e 84 anni ( et media 64 anni ) , con diagnosi istologica di gist sul pezzo operatorio in malattia primitiva , in un periodo compreso tra agosto 2000 e settembre 2004 . 
criteri di esclusione sono stati la diagnosi di gist su prelievo bioptico della neoplasia e / o su lesioni recidivanti ; inoltre , un altro parametro di esclusione stata lesecuzione della tc in altre t . 
the aim of this study was to assess the diagnostic accuracy of spiral ct in detection , characterisation and staging of gist by correlating ct findings with pathology reports . materials and methods we retrospectively reviewed abdominal ct scans of 15 patients ( eight men and seven women , age range 2384 years , mean age 64 years ) with histological diagnosis of primary gist obtained on a surgical specimen . 
all of the patients underwent surgical treatment ; two also underwent medical treatment with sti - 571 but at 8 and 10 months after surgery following the appearance of liver metastasis . since this retrospective study considered ct examinations carried out over a period of 4 years , ct imaging techniques used were different . 
a single - slice spiral ct ( ssct ) scanner ( toshiba , asteion ; rotation time 0.75 s ) was used in ten cases and a multislice ct ( msct ) scanner ( toshiba , aquilion ; 4 slices / rotation ; rotation time 0.5 s ) in five cases . all cases underwent a complete abdominal study ( from the costophrenic angles to the inguinal regions )  . 
ssct studies were performed using a protocol that involved a slice thickness of 7 mm , a table feed of 10 mm ( pitch 1.4 ) and a reconstruction interval of 7 mm with 120 kv and 190 mas . 
the msct study protocol involved a slice thickness of 3 mm with a reconstruction interval of 5 mm in three cases and a slice thickness of 5 mm and reconstruction interval of 7 mm in the other two , with 120 kv and 125200 mas . all studies were carried out after iv administration of nonionic iodinated contrast material with an iodine concentration of 350400 mgi / ml : five patients received 140 ml at a rate of 3.5 ml / s ( for a study including the arterial phase ) or a rate of 2 ml / s ( portal phase only ) whereas in the other cases , such technical data were not available . 
all patients had a portal - phase study ( 70 - s scan delay ) ; eight had a non - contrast - enhanced study ; three had an arterial - phase study ( 30 - s scan delay ) and ten a late study in the equilibrium phase ( 3 min after iv injection of contrast material )  . 
ten patients received oral , water - soluble radiopaque contrast material ( gastrografin ) diluted in water , four received only water ( 500 ml ) whereas one received no contrast material as he was polytraumatised and intubated . 
 two radiologists independently assessed the scans for : site ( stomach , duodenum , small bowel , colon or peritoneum ) , size ( classed into three groups : less than 5 cm , 510 cm , and larger than 10 cm ) , morphology ( rounded or oval , multilobulated or not multilobulated ) , intrinsic or extrinsic growth relative to the organ of origin , homogeneous or inhomogeneous enhancement , possible presence of calcification , presence of liver , peritoneal and / or nodal metastasis and presence of intraabdominal fluid collection . 
tutti i suddetti pazienti sono stati sottoposti a trattamento chirurgico , 2 a terapia medica con sti - 571 , ma a distanza di 8 e 10 mesi dallintervento chirurgico in seguito alla comparsa di lesioni secondarie a livello epatico . essendo questo uno studio retrospettivo su esami eseguiti nellarco di quattro anni , le tecniche dindagine mediante tc utilizzate sono state pi duna . 
le apparecchiature tc usate sono state una spirale a singolo strato ( tcss ) ( toshiba , asteion ; tempo di rotazione 0 , 75 s ) in 10 casi ed una multistrato ( tcms ) ( toshiba , aquilion ; 4 strati / rotazione ; tempo di rotazione 0 , 5 s ) in 5 . 
gli studi condotti con lapparecchiatura tcss sono stati effettuati mediante un protocollo che prevedeva un row - thickness di 7 mm , un avanzamento del lettino di 10 mm ( pitch di 1 , 4 ) ed un intervallo di ricostruzione di 7 mm con 120 kv e 190 mas . 
in quelli condotti con tcms il protocollo prevedeva un row - thickness di 3 mm con un intervallo di ricostruzione di 5 mm in 3 casi e rispettivamente row - thickness di 5 mm e intervallo di ricostruzione di 7 mm in altri 2 , con 120 kv e con valori di mas compresi tra un minimo di 125 ed un massimo di 200 . tutte le indagini sono state eseguite con mezzo di contrasto ( mdc ) per via endovenosa : il mdc utilizzato stato un organo - iodato non ionico ad una concentrazione di iodio variabile da 350 a 400 mgi / ml : in 5 casi la quantit iniettata stata di 140 ml alla velocit di 3 , 5 ml / s ( se effettuato anche uno studio in fase arteriosa ) o alla velocit di 2 ml / s ( per la sola fase portale ) , mentre negli altri casi non stato possibile risalire ai suddetti dati tecnici . 
in tutti i casi stato eseguito lo studio in fase portale ( scan - delay di 70 s ) ; in 8 casi stato eseguito anche lo studio diretto ( senza mdc ) ; in 3 casi anche lo studio in fase arteriosa ( scan - delay di 30 s ) ed in 10 lo studio tardivo nella fase dequilibrio ( a 3 min dalliniezione endovenosa di mdc )  . 
a 10 pazienti stato somministrato per os mdc radiopaco idrosolubile ( gastrografin ) diluito con acqua , a 4 solamente acqua ( 500 ml ) , mentre a 1 paziente nessun mdc , poich politraumatizzato intubato . due radiologi indipendentemente hanno valutato : la sede ( stomaco , duodeno , tenue , colon o peritoneo ) , le dimensioni ( classificate in tre gruppi : inferiori a 5 cm , comprese tra 5 e 10 cm e superiori a 10 cm ) , la morfologia ( rotondeggiante o ovalare , polilobata o non polilobata ) , lo sviluppo intrinseco o estrinseco rispetto allorgano di origine , lenhancement omogeneo o disomogeneo della neoplasia , leventuale presenza al suo interno di calcificazioni , il riscontro di lesioni metastatiche a livello epatico , peritoneale e / o linfonodale e la presenza di versamento endoaddominale . 
la sede , la morfologia e le dimensioni sono stati considerati parametri per lidentificazione della neoplasia ; le dimensioni , lo sviluppo parzialmente o francamente estrinseco , limpregnazione di mdc omogenea o disomogenea della lesione e leventuale presenza di calcificazioni al suo interno sono stati assunti come criteri di caratterizzazione di un gist ; la presenza di metastasi epatiche , peritoneali e / o linfonodali e / o di versamento libero endoaddominale stata considerata parametro di malignit intermedia o elevata . i risultati ottenuti sono stati successivamente correlati phology and size were considered parameters for identification of the neoplasm ; size , partially or frankly extrinsic growth , homogeneous or inhomogeneous enhancement and the possible presence of intralesional calcifications were considered criteria for gist characterisation ; the presence of liver , peritoneal and / or nodal metastasis and / or the presence of free intraabdominal fluid were considered parameters of intermediate or high malignancy . the results obtained were subsequently correlated with some pathological findings obtained on the surgical specimen , in particular , with gross pathology findings such as lesion site , morphology , and size before fixation and with its various tissue components ( solid , haemorrhagic , cystic , ulcerative or calcific )  . 
comparison was based on correspondence between radiological and histopathological assessment of site , morphology and size and some criteria reported in the literature whereby gists are noncalcific lesions that exhibit homogeneous density and a predominantly intrinsic growth pattern if smaller than 5 cm , and inhomogeneous density and a prevalently extrinsic growth pattern in those larger than 5 cin particular , we evaluated whether inhomogeneous density , which was more evident after iv injection of contrast material and characterised by areas of high attenuation in the nonenhanced study and low attenuation in the contrast - enhanced study and areas of fluid or fluid - fluid low attenuation in all phases of the study , correlated with the presence of haemorrhagic , cystic and / or ulcerative areas , respectively . furthermore , we evaluated whether size and the presence of metastasis and / or intraabdominal fluid could be considered indicative of an intermediateor high - grade of malignancy . all malignancy grades are included in the classification proposed by fletcher et al . 
 [ 3 ] ( table 1 ) that , in addition to the macroscopic parameter of size in centimetres , also uses a microscopic parameter such as the number of mitoses per 50 high - power fields ( hpf ) and is currently the only prognostic tool available . 
no multivariate statistical analysis was carried out because patient samples were relatively small . results in the 15 cases considered , at gross pathology , the disease was found to affect the stomach in nine ( 60% ) and the small bowel in six ( 40% ) , of which one was in the duodenum . there were no cases of primary location of gist in other sites of the gastrointestinal systein the four cases of larger lesions ( three larger than 10 cm and one measuring 9 cm ) , at abdominal ct , the site of origin was hypothesised to be the stomach , but the hypothesis was considered uncertain three of these cases , the hypothesis corresponded to the pathology report whereas for the 9 - cm neoplasm , the site of origin was the ileu in the remaining 11 cases ( lesions smaller than 9 cm ) , the site was defined with a good degree of certainty and confirmed by the gross pathology report . as regards lesion morphology and size ten gists smaller than 5 cm , two 510 cm , and three larger than 10 cm ( table 2 ) ct findings essentially agreed with those of gross pathology . 
il confronto si basato sulla corrispondenza tra valutazione radiologica ed anatomo - patologica di sede , morfologia e dimensioni e su alcuni criteri riportati in letteratura secondo cui i gist sarebbero lesioni prive di calcificazioni , a densit omogenea e sviluppo prevalentemente allinterno dellorgano di origine se inferiori a 5 cm , a densit disomogenea e sviluppo preferenzialmente estrinseco se superiori a 5 cin particolare , si valutato se la disomogenea densit , pi evidente dopo iniezione endovenosa di mdc , caratterizzata da aree iperdense in fase diretta ed ipodense dopo mdc ed aree ipodense di tipo liquido o sovraliquido in tutte le fasi di studio , si correlava alla presenza di aree rispettivamente emorragiche e cistiche e / o ulcerative . 
inoltre , si valutato se le dimensioni e la presenza di metastasi e / o di versamento endoaddominale , potessero essere criteri indicativi di un grado di malignit intermedio o elevato . 
nel 2002 [ 3 ] ( tabella 1 ) che , oltre ad un parametro macroscopico come le dimensioni espresse in cm , utilizza anche un parametro microscopico quale il numero di mitosi per 50 campi ad alta risoluzione ( hpf ) e che attualmente lunico strumento in uso per una valutazione prognostica . 
non si effettuata unanalisi statistica multivariata dei risultati , poich il campione dei pazienti stato ritenuto di dimensioni relativamente piccole . risultati nei 15 casi presi in considerazione , allesame anatomo - patologico la localizzazione di malattia risultata lo stomaco in 9 casi ( 60% ) ed il piccolo intestino in 6 ( 40% ) di cui il duodeno in 1 caso . 
nei 4 casi di lesioni di maggiori dimensioni ( di cui 3 superiori a 10 cm e 1 di 9 cm ) alla rivalutazione della tc addominale , la sede dorigine stata ipotizzata essere lo stomaco , ma posta come dubbia . 
nei rimanenti 11 casi ( di dimensioni inferiori a 9 cm ) , invece , la sede stata definita con un certo grado si sicurezza ed effettivamente stata confermata dallanalisi anatomo - patologica . per quanto concerne la morfologia delle lesioni e le loro dimensioni , 10 gist inferiori a 5 cm , 2 gist con dimensioni comprese tra 5 e 10 cm , 3 con dimensioni superiori a 10 cm ( tabella 2 ) , i risultati sono sostanzialmente concordi con quelli dellanatomia patologica . 
in tc , inoltre , nessuna neoplasia presentava calcificazioni intralesionali ed anche questo rilievo stato confermato dallesame istopatologico . per quanto riguarda lo sviluppo della lesione , in 9 casi sui 10 inferiori a 5 cm esso risultato alla tc parzialmente t . 
in all cases of homogeneous density , histopathology revealed the almost exclusive presence of solid areas whereas in all those with inhomogeneous contrast enhancement ( solid , haematic and / or fluid attenuation ) , it revealed solid , haemorrhagic , necrotic and / or cystic areas . the correlation between malignancy size and grade according to the predictive criteria proposed by fletcher et al . [ 3 ] revealed that of the seven tumours with intermediate malignancy grade , six were smaller than 5 cm and only one larger than 10 cm , that two out of two measuring 510 cm were high malignancy grade and that all those larger than 10 cm were intermediate or high malignancy grade ( table 3 )  . ct demonstrated liver metastasis in two cases , peritoneal and / or nodal metastasis in none , and intraabdominal fluid in one . 
in tutti i casi di densit omogenea lanalisi patologica ha rivelato la presenza quasi esclusivamente di aree solide , mentre in tutti quelli con impregnazione di mdc disomogenea per la presenza di aree a densit di tipo solido , ematico e / o liquido sono state riscontrate aree sia solide , che emorragiche , necrotiche e / o cistiche . la correlazione tra dimensioni e grado di malignit , secondo i criteri predittivi proposti da fletcher et al . 
 [ 3 ] , ha messo in evidenza che delle 7 neoplasie a rischio intermedio 6 erano inferiori a 5 cm e solo 1 superiore a 10 cm , che 2 su 2 di dimensioni tra 5 e 10 cm rientravano nel gruppo a rischio elevato e che tutte quelle superiori a 10 cm rientravano , invece , nel gruppo a rischio intermedio o in quello a rischio elevato di malignit ( tabella 3 )  . in 2 casi alla tc si sono individuate metastasi epatiche , in nessun caso peritoneali e / o linfonodali , in 1 versamento endoaddominale . 
negli altri casi di malignit intermedia o elevata non erano presenti metastasi al momento della diagnosi . discussion a final diagnosis of gist requires demonstration of cd117 positivity , but diagnostic imaging and spiral ct in particular la diagnosi di certezza dei gist richiede la dimostrazione dellimmunopositivit al cd117 , ma la diagnostica per immagini ed , in particolare , la tc spirale , svolge comunque un discussione table 2 results of correlation between size , development , enhancement and calcifications size , cm total , n development extrinsic , n intrinsic , n enhancement inhomogeneous , n homogeneous , n no calcifications , n tabella 2 risultati della correlazione tra dimensioni , sviluppo , enhancement e presenza di calcificazioni dimensioni , cm totale , n svilupppo enhancement assenza di calcificazioni , n estrinseco , n intrinseco , n disomogeneo , n omogeneo , n > 5 - < 10 > 5 e < 10 t . 
abdominal computed tomography ( ct ) , axial images : without iv contrast agent , arterial and portal phases , respectively ; a roundish formation , lobate , with partial extraluminal growth . density is inhomogeneous , particularly after contrast agent and particularly in the portal phase . 
abdominal computed tomography ( ct ) , axial images : arterial , portal and late phases , respectively ; oval formation ( arrow ) of inhomogeneous density with extraluminal growth . 
e aspetto macroscopico del gist allanalisi del pezzo operatorio ; presenza di necrosi centrale ( freccia ) ed aree ulcerate ; sviluppo allesterno della parete gastrica ( freccia )  . is nonetheless instrumental in the diagnostic workup [ 10 , 15 , 22 , 29 ]  . 
however , one study [ 20 ] has shown that , thanks to its high - contrast resolution , mri is reliable in depicting the various components of larger gists ( 728 cm ) , and thanks to its multiplanar capabilities , it is effective in assessing the relationship between the lesion and adjacent organs . as regards endoscopy , although in a very small proportion of patients diagnosis is made through biopsy , in the majority of patients , histology is negative owing to the tendent . 
a , b tc delladdome , immagini assiali , fase portale : formazione che mostra enhancement disomogeneo per la presenza di aree a densit di tipo solido ed altre francamente ipodense . 
c , d ricostruzioni sul piano coronale e sagittale che consentono una buona valutazione dellestensione della lesione e dei rapporti con le strutture adiacenti . ruolo fondamentale nelliter diagnostico [ 10 , 15 , 22 , 29 ]  . esami di vario livello sono lendoscopia , lecografia delladdome , lo studio radiologico del tubo digerente con mezzo di contrasto ( mdc ) e la tc addominale . 
comunque , da uno studio riportato in letteratura [ 20 ] , emerge che la rm , grazie allelevata risoluzione di contrasto , attendibile nellevidenziare le varie componenti dei gist di maggiori dimensioni ( da 7 a 28 cm ) e , grazie alla multiplanariet , nel valutare i rapporti tra la lesione neoplastica e gli organi adiacenti . per quanto riguarda lendoscopia , mentre esiste una piccolissima quota di pazienti in cui la diagnosi viene fatta mediante prelievi bioptici , nella maggioranza dei casi listologia negativa a causa della tendenza di queste neoplasie ad avere uno sviluppo estrinseco rispetto alla parete . 
i limiti dellecografia , invece , quali la costituzione fisica del paziente , il meteorismo intestinale , loperatore - dipendenza e la scarsa panoramicit spesso non consentono la caratterizzazione e soprattutto un corretto bilancio destensione di una massa addominale . 
lo studio radiologico del tubo digerente a singolo o doppio contrasto in grado di mettere in evidenza alterazioni parietali e della plicatura e lesioni aggettanti nel lume riferibili ad una neoplasia , consentendo anche di stabilire se essa intrao extra - murale , per , non permette una valutazione extra - luminale della patologia [ 15 ]  . lintroduzione della tc spirale ed , in particolare , di quella multistrato , invece , grazie allelevata velocit desecuzione dellesame , allutilizzo di scansioni con spessore molto sottile con possibilit di sovrapposizione e di ottenere ricostruzioni multiplanari di elevata qualit , ha offerto nuot . 
the limitations of ultrasound instead , such as patient build , intestinal gas , operator dependency and limited field of view , often prevent characterisation and , above all , correct staging of abdominal masses . 
singleor double - contrast barium studies are able to detect changes in the wall and folds and identify exophytic lesions referable to a tumour , even allowing establishment of whether the lesion is intraor extramural ; however , they do not enable an extraluminal evaluation of the disease [ 15 ]  . 
 introduction of spiral ct and in particular msct thanks to the short examination times , the use of very thin slices with the possibility of overlapping slices and obtaining highquality multiplanar reconstructions has provided new opportunities in gastrointestinal imaging , allowing detailed evaluation of the stomach , small and large bowel and relations with adjacent structures . 
spiral abdominal ct has long been used as a routine study in patients with gastrointestinal ve opportunit nello studio per immagini dellapparato gastrointestinale consentendo valutazioni dettagliate di stomaco , piccolo e grande intestino e dei rapporti con le strutture adiacenti . 
la tc spirale delladdome , da tempo , unindagine usata di routine in pazienti con tumori delle vie digestive per il bilancio destensione della malattia , nonch nel follow - up del paziente operato . 
pi recentemente , limpiego della tc , grazie alle innovazioni tecnologiche , stato esteso anche alla identificazione e caratterizzazione di neoplasie dellapparato digerente , in particolari situazioni rappresentate da masse di origine ignota o a partenza da aree del tratto digerente non raggiungibili con lendoscopia . 
inoltre , proprio per quanto riguarda i gist , sembra che queste neoplasie presentino in tc aspetti semeiologici , se non patognomonici , perlomeno altamente caratteristici [ 4 , 7 , 10 , 14 , 15 , 19 , 2124 ]  . 
per consentire risultati validi in tale ambito , va condotta unadeguata tecnica tc che deve prevedere una buona distensione gastrica ed intestinale e unottimizzazione size , cm > 5 < 10 total > 5 e < 10 totale very low medium high molto basso basso intermedio elevato tumours , both for disease staging and follow - up after surgery . 
thanks to the more recent technological innovations , the use of ct has been extended to the identification and characterisation of digestive tract neoplasms in specific situations , such as masses with unknown origin or originating in areas of the digestive tract not amenable to endoscopic techniques . 
in addition , as regards gists in particular , these tumours seem to exhibit highly characteristic , if not pathognomic , ct patterns [ 4 , 7 , 10 , 14 , 15 , 19 , 2124 ]  . 
 for results to be reliable in this field , a correct ct technique is needed that involves good gastric and intestinal distension and optimisation of iv injection of contrast material . adequate distension of the stomach and bowel loops , preferably with low - attenuation agents and possibly water , is essential , as a collapsed wall may mimic a nonexistent alteration or mask existing disease [ 10 , 21 , 22 ]  . 
 with regard to the study phases after iv contrast injection , some authors [ 21 , 22 ] agree on carrying out an arterial - phase study of the abdominal sectors comprising the stomach and liver only on the basis of precise requests for a vascular study and a portal - phase study of the entire abdomen ( from the costophrenic angles to the pubic symphysis ) ; the latter phase is considered indispensable for the diagnosis of gastrointestinal disease and at times sufficient [ 21 , 22 ]  . 
even in our study , arterial - phase scans were not acquired in all cases whereas portal - phase scans were . as concerns ct evaluation of gist , it should be noted that because the immunohistochemical criterion for tumour identification was only recently introduced , the studies published to date have included a relatively small number of patients and not all have paid special attention to tumour size . this information , which can be obtained both at ct and at gross pathology , is the most important prognostic factor currently used , together with the histopathological mitotic count [ 4 ]  . 
 as regards site and growth pattern , since gists originate in the muscularis propria , they commonly have exophytic growth from the wall and therefore appear at ct as a mass prevalently located outside the affected organ . predominantly intraluminal forms are rare and mostly related to small size and wall thickening , which makes this sign uncharacteristic for these tumours [ 4 , 7 , 10 , 14 , 21 ]  . 
in particular , stomach gists , which tend to affect the gastric body and fundus , exhibit extragastric extension in a wide majority of cases ( 86% in the series by levy et al . ) [ 7 ] , and those affecting the small bowel may have primary presentation in extraserous sites ( 22% in the same series )  . 
 [ 4 ] showed that , regardless of site , gists smaller than 5 cm tend to have predominantly intraluminal growth , those measuring 510 cm combined intraand extraluminal growth and those greater than 10 cm prevalently extraluminal growth with a tendency to invade adjacent organs [ 4 ]  . in contrast , in our series , even tumours smaller than 5 cm exhibited prevalently extrinsic growth ( only one case out of ten was contained in the affected organ ) , as did the larger t . 
infatti , unadeguata distensione dello stomaco e delle anse intestinali , preferenzialmente con agenti a bassa attenuazione ed , in particolare lacqua , di fondamentale importanza , poich un lume collassato pu mimare unalterazione inesistente o mascherare una patologia realmente presente [ 10 , 21 , 22 ]  . 
dal punto di vista delle fasi di studio dopo iniezione ev di mdc alcuni autori [ 21 , 22 ] concordano nellesecuzione di una fase di tipo arterioso dei settori delladdome comprendenti stomaco e fegato solo sulla base di precise richieste di uno studio vascolare , e di una fase portale di tutto laddome ( dai seni costofrenici alla sinfisi pubica ) : questultima ritenuta indispensabile per una diagnosi di patologia gastrointestinale , ma talvolta sufficiente [ 21 , 22 ]  . 
per quanto riguarda la valutazione dei gist mediante tc va sottolineato che , essendo recente il criterio immunoistochimico di identificazione di queste neoplasie , gli studi finora pubblicati hanno compreso un numero relativamente basso di pazienti e che non tutti hanno posto particolare attenzione alle dimensioni del tumore : questo elemento , per , ricavabile sia quale reperto semeiologico in tc sia dalla valutazione macroscopica del pezzo operatorio il pi importante fattore prognostico attualmente usato assieme allelemento istopatologico della conta mitotica [ 4 ]  . 
per quanto riguarda la sede ed il tipo di crescita , poich i gist prendono origine nella muscolare propria , molto comunemente hanno uno sviluppo esofitico rispetto alla parete e , quindi , in tc si presentano come massa localizzata prevalentemente allesterno dellorgano interessato . 
le forme principalmente intra - luminali sono rare , per lo pi legate alle piccole dimensioni e lispessimento parietale , dunque , non un reperto semeiologico tipico di questi tumori [ 4 , 7 , 10 , 14 , 21 ]  . 
 [ 4 ] emerso che , indipendentemente dalla sede , i gist inferiori a 5 cm tendono a presentare una crescita preferenzialmente intraluminale , quelli tra 5 e 10 cm una combinata intraed extra - luminale e quelli maggiori di 10 cm una prevalentemente extraluminale con tendenza allinfiltrazione degli organi adiacenti [ 4 ]  . 
nella nostra casistica , invece , anche i tumori inferiori a 5 cm mostrano uno sviluppo prevalentemente estrinseco ( solo in 1 caso su 10 era allinterno dellorgano colpito ) , come quelli di maggiori dimensioni ( 2 su 2 di quelli tra 5 e 10 cm e 3 su 3 di quelli superiori a 10 cm )  . 
 ( 3% ) [ 4 , 7 ] : i risultati del nostro studio sono concordi con tale rilievo , poich in nessuna delle neoplasie in esame si evidenziata la presenza di calcificazioni al suo interno . 
homogeneous enhancement is instead present in a minority of cases only ( 8% ) and is typical of small lesions [ 4 , 7 , 14 , 2124 , 30 ]  . 
in our study , only 50% of tumours smaller than 5 cm ( five cases out of ten ) had homogeneous density whereas the remaining 50% had markedly or slightly inhomogeneous density ; all cases of gist larger than 5 cm exhibited frankly inhomogeneous density , as reported in the literature . 
in all cases of homogeneous enhancement , however , analysis of the surgical specimen demonstrated the presence of solid areas only whereas in all those of inhomogeneous enhancement , it found solid , necrotic , haemorrhagic and / or cystic areas . 
ct differential diagnosis of gastric gist with adenocarcinoma and lymphoma relies on the fact that they have exophytic growth and are almost never associated with perigastric adenopathy [ 7 ]  . 
gist metastasis to the mesentery and / or omentum enter the differential diagnosis with peritoneal carcinomatosis , lymphomatosis and disseminated peritoneal leiomyomatosis [ 4 , 7 , 11 , 16 ]  . 
liver metastasis , typically hypovascular , appear at ct as hypodense areas , at times with a hyperdense rim ( similar to secondary lesions from other neoplasms ) [ 1 , 4 , 7 , 14 ]  . 
the ability of ct to identify recurrences is essential in the decision to initiate treatment with gleevec , as the drug is reserved for patients with inoperable or metastatic gist . conclusions final diagnosis of gist requires demonstration of positivity for cd117 , but spiral ct plays a fundamental role because gists exhibit signs that are strongly characteristic , if not pathognomic , and ct enables correct grading of the disease , which is crucial in deciding upon resection and / or medical dei gist dopo somministrazione endovenosa di mdc , simile indipendentemente dal sito di origine , va data enfasi al fatto che la gran parte dei tumori di maggiori dimensioni ( 92% secondo levy et al . ) tendono ad avere una presa di contrasto periferica e delle zone ipodense centrali espressione dei reperti patologici macroscopici rispettivamente di tumore vitale e di aree di emorragia , necrosi o degenerazione cistica ( per cui si parla di massa complessa al taglio )  . 
unassunzione omogenea di contrasto , invece , presente solo in una minoranza di casi ( 8% ) ed tipica di lesioni piccole [ 4 , 7 , 14 , 2124 , 30 ]  . 
nel nostro studio solo nel 50% dei casi di tumori inferiori a 5 cm ( 5 casi su 10 ) la densit omogenea , mentre nel restante 50% marcatamente o perlomeno lievemente disomogenea ; in tutti i casi di gist superiori a 5 cm essa , invece , francamente disomogenea come riportato in letteratura . 
in tutti i casi , comunque , dimpregnazione omogenea di mdc lanalisi del pezzo operatorio ha rivelato la presenza solamente di aree solide , mentre in tutti quelli dimpregnazione disomogenea sono state riscontrate aree sia solide , che necrotiche , emorragiche e / o cistiche . 
nella quasi totalit dei casi non presente un interessamento metastatico dei linfonodi loco - regionali e / o a distanza [ 4 , 14 , 15 , 30 ] : elemento confermato dal nostro studio nel quale in nessun caso si sono rilevati linfonodi aumentati di volume . 
la diagnosi differenziale dei gist in tc , in ambito gastrico , con ladenocarcinoma ed il linfoma si basa sul fatto che mostrano una crescita esofitica e non sono quasi mai associati ad adenopatie perigastriche [ 7 ]  . 
per quanto riguarda il piccolo intestino anche il linfoma pu presentarsi come massa disomogenea che si estende al mesentere adiacente : ci che permette lipotesi diagnostica di un gist , per , anche in questo caso , lassenza di interessamento linfonodale [ 7 , 30 ]  . 
le metastasi da gist a livello di mesentere e / o omento vanno in diagnosi differenziale con la carcinomatosi peritoneale , la linfomatosi e la leiomiomatosi peritoneale disseminata [ 4 , 7 , 11 , 16 ]  . 
le metastasi epatiche , tipicamente ipovascolarizzate , presentano un aspetto alla tc di aree ipodense talvolta con cercine iperdenso ( caratteristiche comuni a lesioni secondarie ad altri tipi di neoplasie ) [ 1 , 4 , 7 , 14 ]  . tale aspetto era presente anche nei nostri due casi di secondariet epatiche . 
la capacit della tc di individuare lesioni ripetitive fondamentale al fine della scelta del trattamento medico con gleevec in quanto farmaco riservato oltre che ai pazienti con gist inoperabili anche a quelli metastatici . conclusioni la diagnosi di certezza dei gist richiede la dimostrazione dellimmunopositivit al cd117 , ma la tc spirale svolge un ruolo di primaria importanza poich i gist mostrano aspetti semeiologici se non patognomonici perlomeno fortemente caratteristici e poich permette un corretto bilancio destensione , elemento fondamentale per la scelta di resecabilit e / o trattamento medico . 
tumour size , as established by ct , even though not corresponding to the true size of the tumour , is not a sufficient criterion to predict the grade of malignancy . 
while the presence of metastases at the time of diagnosis may be indicative of intermediateor high - grade malignancy , their absence , like the absence of intraabdominal fluid , does not allow one to consider the gist to be low or very low malignancy grade . 
mentre la presenza di metastasi al momento della diagnosi pu essere indicativa di un grado di malignit intermedio o elevato , la loro assenza , come la non evidenziazione di un versamento endoaddominale , non consente di collocare i gist nel gruppo a basso o molto basso rischio . 
at contrastenhanced ct , they were inhomogeneous in 21 cases ( 91.3% ) , with geographic pattern ( 61.9% of cases ) , serpiginous linear areas of enhancement ( intralesional vessels ) ( 23.8% ) , rounded ( 52.4% ) or linear ( 33.3% ) areas of low attenuation ( necrosis )  . 
il sospetto di lesione pleurica comporta una distinzione in base alle sue dimensioni : in presenza di una piccola neoformazione con margini netti , contorni lisci , angoli di raccordo retti / ottusi e densit omogenea , facile ipotizzare la diagnosi di tfsp ; qualora la neoplasia sia pi voluminosa , la presenza di margini netti e contorni lobulati , angoli di raccordo acuti dolci ed enhancement disomogeneo nelle scansioni con contrasto possono permettere di operare una distinzione da una massa di pertinenza polmonare . key words solitary fibrous tumors of the pleura ct pleural neoplasm parole chiave tumore fibroso solitario della pleura tc neoplasie pleuriche introduction introduzione solitary fibrous tumour of the pleura ( sftp ) is a rare neoplasm that accounts for fewer than 5% of all pleural tumours [ 1 ]  . 
over 50% of patients are asymptomatic at presentation , and the lesion is usually discovered inil tumore fibroso solitario della pleura ( tfsp ) una neoplasia rara che rappresenta meno del 5% di tutti i tumori pleurici [ 1 ]  . 
oltre il 50% dei pazienti asintomatico al momento della diagnosi e la lesione riscontrata in cidentally on chest radiographs performed for other reasons [ 1 , 2 , 5 , 7 , 8 ]  . 
patients may , however , also present with nonspecific symptoms ( cough , chest pain , dyspnoea and fatigue ) [ 1 , 2 , 8 ] or a neoplastic syndrome ( digital clubbing , hypertrophic osteoarthropathy and refractory hypoglycaemia ) [ 9 , 10 ]  . 
sftp generally appears as a solid , sharply marginated , well - circumscribed solitary lesion located at the periphery of the chest or close to a fissure ; it can become very large and occupy even the entire hemithorax [ 1 , 7 , 11 , 12 ]  . 
the tumour has benign behaviour in 80% of cases , and prognosis is generally excellent after surgical resection provided that this is radical [ 2 , 4 , 7 , 8 , 12 , 15 ]  . 
despite the use of transthoracic needle biopsy [ fine - needle aspiration ( fna ) ] [ 16 , 17 , 18 ] and fibreoptic bronchoscopy [ 9 , 12 ] , as well as all the imaging modalities , diagnosis is rarely straightforward . 
in some cases , a definite diagnosis may be established preoperatively with a cutting - needle biopsy , but in most , diagnosis is provided by postoperative histology and immunohistochemistry on the surgical specimen [ 3 , 4 ]  . the primary aim of this study was to review computed tomography ( ct ) features of sftp in order to : ( 1 ) identify a specific ct pattern that could allow a diagnosis of sftp ; ( 2 ) search for radiological signs capable of suggesting lesions of pleural origin or , at least , identifying the benign nature of the lesion . materials and methods between november 1989 and january 2005 , 29 consecutive patients with a histological and immunohistochemical diagnosis of sftp underwent surgical resection of the lesion at the thoracic surgery department of our hospital . 
as such lesions grow within the lung parenchyma without projecting into the pleural cavity , they cannot be assimilated to the classic forms and therefore were not considered suitable for the purposes of this study . 
the study was therefore conducted on 26 patients . we collected clinical data of possible radiological relevance , such as mode of lesion discovery ( incidental / symptomatic ) , presence or absence of respiratory symptoms , transthoracic needle biopsy ( fna ) under fluoroscopic or ct guidance and its results , and preoperative clinical diagnosis . data from surgical reports concerning sessile or pedunculated tumour base , gross pathology features , site of origin ( visceral , parietal , mediastinal or diaphragmatic pleura ) , presence of inflammatory adhesions and / or infiltration of adjacent tissues or organs . 
dal punto di vista radiologico , lelemento pressoch patognomonico delle forme peduncolate il cambiamento di forma e posizione durante le fasi della dinamica respiratoria [ 9 , 13 , 14 ]  . il comportamento di tale neoplasia benigno nell80% dei casi e la prognosi generalmente ottima dopo intervento chirurgico di exeresi , purch radicale [ 2 , 4 , 7 , 8 , 12 , 15 ]  . nonostante lutilizzo dellagobiopsia transtoracica ( fna ) [ 1618 ] e della fibrobroncoscopia [ 9 , 12 ] , nonch di tutte le metodiche di imaging , la diagnosi risulta spesso difficoltosa . 
talvolta una diagnosi preoperatoria di certezza pu essere ottenuta con la biopsia ad ago tranciante , ma nella maggior parte dei casi post - chirurgica , frutto dellesame istologico e dellanalisi immuno - istochimica sul pezzo operatorio [ 3 , 4 ]  . lobiettivo primario di questo studio stato la valutazione dei quadri tc allo scopo di ( 1 ) identificare un quadro tomodensitometrico specifico che permetta di porre diagnosi di tfsp ; ( 2 ) ricercare i segni radiologici indicativi di una lesione di origine pleurica o , quanto meno , individuare la natura benigna della lesione in esame . materiali e metodi nel periodo compreso tra novembre 1989 e gennaio 2005 , 29 pazienti consecutivi con diagnosi definitiva , istologica e immunoistochimica , di tfsp sono stati sottoposti ad intervento chirurgico di resezione presso la s.c.d.u. 
dal momento che tali lesioni crescono indovate nel contesto del parenchima polmonare anzich estrinsecarsi nel cavo pleurico , non possono presentare per definizione un aspetto assimilabile alle forme classiche e pertanto non si adattano allo scopo di questo studio . 
pertanto 26 pazienti costituiscono loggetto dellindagine . sono stati desunti i dati anamnestici di possibile interesse radiologico , quali la modalit del riscontro ( occasionale / sintomatico ) , la presenza o meno di sintomi respiratori , lesecuzione di agobiopsia trans - toracica ( fna ) sotto controllo fluoroscopico o tc , la diagnosi clinica pre - operatoria . 
administration of contrast medium and 14 at baseline ( 11 studies were performed before and after contrast - medium administration )  . statistical analysis the data collected ( clinical , surgical , histopathological and radiological ) were entered into an excel spreadsheet for comparative evaluation . 
di mezzo di contrasto e 14 in condizioni basali ( 11 studi sono stati eseguiti prima e dopo somministrazione del contrasto )  . analisi statistica le informazioni ottenute ( cliniche , chirurgiche , anatomopatologiche e radiologiche ) sono state inserite in un foglio di lavoro elettronico excel per le debite valutazioni comparative . 
 stato considerato significativo un valore di p0 , 05 . risultati dati clinici i 26 pazienti oggetto di questo studio , operati nel periodo tra novembre 1989 e gennaio 2005 , presentano unet media di 64 , 9 anni ( mediana 68 anni ; range 4081 anni )  . 
diciotto pazienti ( 69 , 2% ) erano totalmente asintomatici al momento della diagnosi e il tfsp stato riscontrato occasionalmente nella radiografia del torace eseguita per altre ragioni ( routine preoperatoria o esame eseguito in occasione di traumi )  . 
in tutti i pazienti la neoplasia pleurica era evidente nei radiogrammi standard del torace , localizzata a destra in 14 casi ( 53 , 8% ) , a sinistra nei restanti 12 ( 46 , 2% )  . la fibrobroncoscopia stata eseguita in 18 pazienti ( 69 , 2% ) : una compressione estrinseca delle strutture bronchiali , sempre confermata alla tc , era presente in 9 casi ( 50% )  . 
una diagnosi istologica pre - operatoria corretta stata raggiunta in 10 casi ( 38 , 4% ) ; nei restanti 10 casi , il prelievo risultato non diagnostico o suggestivo per mesotelioma maligno . allesplorazione chirurgica , il tumore risultato originare dalla pleura viscerale in 20 pazienti ( 83 , 3% ) : 18 lesioni ( 90% ) sono peduncolate , 2 ( 10% ) sessili . 
presentano pi frequentemente una stretta base dimpianto i tfsp a partenza dalla pleura viscerale , mentre quelli originanti dalla pleura parietale sono pi spesso sessili : tale correlazione risultata significativa dal punto di vista statistico ( p = 0 , 018 )  . 
aderenze di natura flogistica tra il tfsp e le strutture adiacenti sono state riscontrate intraoperatoriamente in 15 ( 57 , 7% ) pazienti ( pleura mediastinica 2 , pleura parietale 8 , pleura viscerale di parenchima polmonare contiguo 12 ) ; in 11 ( 42 , 3% ) la lesione apparsa , invece , ben delimitata e facilmente enucleabile . dati tomodensitometrici la valutazione morfologica - densitometrica dei tfsp stata eseguita sulle 26 tc pre - operatorie disponibili . 
as regards the second parameter , two angles were evaluated for each tumour , and the results are shown in figures 2 and 3 . although 19 / 26 ( 73% ) lesions were found to be pediculated at surgery , there was no ct evidence of the presence of a pedicle . 
an ipsilateral pleural effusion was seen in 5 patients ( 19.2% ) whereas no ct scan demonstrated enlarged hilarmediastinal lymph nodes . analysis of the available unenhanced ct scans ( n = 14 ) alsono pi voluminose ( media 16 , 1 cm ; range 14 , 520 )  . 
i margini delle neoplasie sono risultati a carattere netto in tutti i casi : in 12 ( 46 , 1% ) con contorni lobulati , in 14 ( 53 , 9% ) lisci . 
per quanto riguarda , invece , il secondo parametro , per ogni tumore sono stati valutati due angoli di raccordo , con i risultati riportati nelle figure 2 e 3 . 
in 17 tc ( 65 , 4% ) sono stati rilevati segni di compressione sulle strutture circostanti ; in particolare , leffetto massa si reso evidente sul parenchima polmonare in tutti i casi , associato in due casi a dislocazione mediastinica . 
un versamento pleurico omolaterale associato stato riscontrato in 5 pazienti ( 19 , 2% ) , mentre in nessuna tc sono stati obiettivati linfonodi ilo - mediastinici ingranditi . lanalisi delle scansioni basali disponibili ( 14 tc ) ha permesso di valutare le caratteristiche tomodensitometriche dei tfsp . 
dodici tumori ( 85 , 7% ) dimostrano unattenuazione simile a quella dei muscoli della parete toracica , 2 ( 14 , 3% ) mostrano unipodensit relativa , mentre nessun tfsp risultato iperdenso rispetto ai muscoli . 
all lesions larger than 7 cm showed heterogeneous enhancement after administration of contrast mediuenhancement patterns of sftp after administration of contrast material are summarised in table 3 . certain features of sftp were correlated to the size of the tumour , and the results are shown in table 4 . 
lanalisi delle risultanze derivate dalla clinica , dalle procedure bioptiche e dai referti radiologici originali ha permesso di porre diagnosi di lesione pleurica in 17 pazienti ( n = 26 ; 65 , 4% ) e di identificare con certezza il tfsp in 12 di essi ( n = 17 ; 70 , 6% )  . 
its rarity is confirmed by our experience , as the 26 cases considered were encountered over a period of 16 years , despite the fact that our department of thoracic surgery is a regional referral centre . 
sftp are discovered incidentally on routine chest radiographs performed for other reasons [ 2 , 7 , 8 , 9 ] , and they tend to have an indolent course . 
when possible , definitive diagnosis is made preoperatively on the basis of fna cytology [ 17 , 18 ] and confirmed by the absence of infiltration of the bronchial tree as ascertained by fibreoptic bronchoscopy [ 9 , 12 ]  . 
 on chest radiographs and chest ct scans , sftp appear as well - delineated solitary lesions located in the chest periphery or within a fissure [ 1 , 2 , 9 , 12 , 21 ]  . 
they may become very large and at times occupy an entire hemithorax , giving rise to extensive opacities and causing respiratory problems [ 1 ]  . typically , they present as lesions , with their maximum diameter abutting the chest wall , with which they form obtuse , right or acute angles with a smooth tapering margin [ 22 , 23 ]  . a pathognomic finding in pedunculated lesions is the mobility of the tumour with changes in patient position [ 3 , 9 , 11 , 13 , 14 ]  . 
the usefulness of this finding is , however , limited by the size of the mass : the larger the sftp , the more firmly it is attached to adjacent structures by adherences ( 84.6% of tumours > 10 cm in our series ) , which makes the mass less mobile [ 9 , 20 , 24 ]  . 
in addition , another limitation inherent to the retrospective design of our study is that this sign was never elicited by changing patient position during the ct scans . finally , the right , obtuse or acute angles with smooth tapering contours allowed us to confirm that the origin of the lesion is pleural rather than parenchymal ( 73% of our cases ) [ 1 , 3 , 17 , 25 ]  . 
dal punto di vista clinico , le caratteristiche dei nostri tfsp sono del tutto analoghe a quelle di altri studi [ 4 ]  . noto che spesso i tfsp sono scoperti incidentalmente in radiografie del torace eseguite di routine [ 2 , 79 ] e che il decorso di tali neoplasie in genere indolente . 
la diagnosi di certezza posta , quando possibile , preoperatoriamente grazie allesame citologico sul materiale prelevato in corso di fna [ 17 , 18 ] , corroborata dallassenza di segni di infiltrazione dellalbero bronchiale alla fibrobroncoscopia [ 9 , 12 ]  . 
quando , invece , lfna non sia eseguita o risulti non diagnostica , lanalisi anatomopatologica , istologica ed immunoistochimica sul pezzo operatorio , a confermare la natura della lesione [ 17 ]  . 
al radiogramma ed alla tc del torace , i tfsp appaiono generalmente come lesioni solitarie , a margini netti , situate alla periferia del torace o in relazione ad una scissura [ 1 , 2 , 9 , 12 , 21 ]  . 
talvolta possono raggiungere dimensioni notevoli fino ad occupare un intero emitorace , producendo grossolane opacit e causando disturbi respiratori al paziente [ 1 ]  . caratteristicamente si presentano come lesioni con il diametro massimo a contatto con la parete toracica , con la quale formano angoli di raccordo ottusi , retti o acuti dolci [ 22 , 23 ]  . 
tale aspetto , per , trova un limite alla sua utilizzazione nelle dimensioni della massa : infatti , pi il tfsp voluminoso pi ancorato alle strutture adiacenti per mezzo di tenaci aderenze ( lo l84 , 6% delle neoplasie di dimensioni > 10 cm nella nostra casistica ) e quindi meno risulta essere mobile [ 9 , 20 , 24 ]  . 
a questo si aggiunge un ulteriore limite intrinseco al nostro studio : essendo un lavoro retrospettivo , nessuno ha mai ricercato questo segno con lacquisizione di scansioni tc al variare del decubito dei pazienti . gli angoli di raccordo retti , ottusi o , infine , acuti dolci ci permettono di confermare che tale lesione di origine pleurica e non parenchimale ( 73% dei nostri casi ) [ 1 , 3 , 17 , l . 
at least one acute angle with smooth tapering margins , first described by dedrick et al . [ 1 ] in five out of six lesions examined , was present in 57% of lesions in our series . 
the different incidence of this parameter is , in our opinion , largely due to the small size of the series examined by dedrick et al . evaluation of relationships between the lesion and adjacent structures is another important element . 
tale caratteristica presente in quasi tutte le lesioni di piccole dimensioni ed in una buona percentuale di masse di dimensioni superiori , tenendo conto del fatto che langolo acuto dolce ha , nei tumori pi voluminosi ( diametro massimo medio 13 , 5 cm ) , significato analogo a quello degli angoli retti / ottusi nei pi piccoli ( diametro medio 7 , 25 cm )  . 
inoltre , nel 65 , 4% dei casi stato possibile osservare i segni delleffetto massa sulle strutture circostanti , in particolare sul parenchima polmonare e sul mediastino [ 1 , 26 ]  . 
tale caratteristica , assente in caso di lesioni parenchimali , risente delle dimensioni del tfsp : risulta , infatti , maggiormente evidente con lincremento dimensionale ( 100% delle lesioni di dimensioni > 10 cm )  . la valutazione delle tc a nostra disposizione individua nelle caratteristiche dellenhancement un ulteriore aspetto distintivo dei tfsp . 
il 91 , 3% delle lesioni disomogenea dopo somministrazione del mezzo di contrasto e tale disomogeneit si configura nel 76 , 2% dei casi nei pattern tipici [ 3 , 11 , 21 , 24 , 25 ]  . 
7 woman with dyspnoea and a bulky solitary fibrous tumours of the pleura ( sftp ) occupying almost the entire right hemithorax with lobulated contours , smooth tapering margins and heterogeneous enhancement . 
due to their rich vascularity , the lesions show high attenuation relative to muscle on contrast - enhanced ct scans [ 4 ] , and their enhancement pattern is often heterogeneous with a geographic pattern , with areas of necrosis and depiction of serpiginous vessels [ 3 , 11 , 21 , 24 , 25 ]  . in very large tumours , the discrepancy between the scarcity of clinical findings and the dramatic radiological picture is in itself indicative of a slow - growing lesion ( lung tumours rarely grow so large without causing symptoms )  . absence of lymph node involvement [ 21 ] and preservation of cleavage planes with adjacent structures , despite the fact that these masses may occupy an entire hemithorax , provide confirmation of the benign nature of the lesion . 
when lesion arises from the mediastinal pleura , a suggestive finding is displacement of the thymic space , which does not occur in the presence of thymomas and lymphomas . ct therefore proves to be a very reliable imaging modality , especially when integrated with clinical and biopsy findings . se alle dimensioni , al fine di porre il sospetto diagnostico . 
la densit omogenea , simile a quella della muscolatura adiacente ; ci aiuta nella diagnosi differenziale con lesioni adipose o con raccolte liquide saccate [ 4 , 11 , 27 ]  . 
in virt della ricca vascolarizzazione delle lesioni , la loro densit superiore a quella dei muscoli dopo somministrazione di mezzo di contrasto [ 4 ] e lenhancement pi spesso disomogeneo a carta geografica , con aree di necrosi e immagini di vasi dallaspetto serpiginoso [ 3 , 11 , 21 , 24 , 25 ]  . di fronte a tumori molto voluminosi , inoltre , la discrepanza fra la povert della presentazione clinica e limportanza del quadro radiologico sono gi orientative di una lesione a lenta crescita ( i tumori polmonari raramente raggiungono tali dimensioni in assenza di un corredo sintomatologico )  . 
lassenza di un coinvolgimento linfonodale [ 21 ] e la conservazione di piani di clivaggio con le strutture adiacenti , nonostante le masse possano giungere ad occupare un intero emitorace , sono la conferma della benignit della lesione . 
di chirurgia , universit degli studi dellinsubria , viale borri 57 , i - 21100 varese , italy 3unit operativa di nefrologia , azienda ospedaliera ospedale di circolo e fondazione macchi , varese , italy correspondence to : g . 
over the past 2 years , we have observed 80 patients with stenotic haemodialysis accesses ; 24 of these ( mean age 66.4 years , range 5081 ) with 26 stenoses of 24 accesses ( 21 cimino - brescia fistulas and 3 dialysis loops ) were selected for cutting balloon angioplasty . 
in 11 cases , the cutting balloon device was used after failure to dilate the access with a high - pressure balloon whereas in 15 cases ( 10 focal stenoses and 5 restenoses ) , it was used as a first choice . 
follow - up examinations ( range 324 months , mean 18.2 months ) demonstrated patency of the vascular access and its good functioning during dialysis in 23 / 24 cases ( 95% )  . 
cutting balloon angioplasty is safe and effective in the treatment of haemodialysis access stenosis , especially in cases of severe stenosis , with low restenosis rate both in the short and medium ter key words cutting balloon arteriovenous fistula pta riassunto obiettivo . 
negli ultimi 2 anni sono giunti alla nostra osservazione 80 pazienti con stenosi dellaccesso per emodialisi ; 24 di essi ( et media 66 , 4 anni , range 5081 ) portatori di 26 stenosi di 24 accessi ( 21 fistole di cimino - brescia e 3 loops dialitici ) sono stati selezionati per un trattamento di angioplastica mediante cutting balloon . 
in 11 casi , il cutting balloon stato utilizzato dopo il fallimento della dilatazione con un pallone ad alta pressione , mentre in 15 casi ( 10 stenosi focali e 5 restenosi ) stato utilizzato di prima intenzione . 
langioplastica mediante cutting balloon sicura ed efficace nel trattamento delle stenosi degli accessi vascolari per dialisi , particolarmente nei casi di stenosi severe con bassi tassi di restenosi anche nel medio periodo . parole chiave cutting balloon fistola artero - venosa angioplastica percutanea introduction introduzione g . 
interventional radiology has taken on an increasingly important role in the prevention and treatment of complications affecting vascular haemodialysis accesses ; in particular , percutaneous angioplasty ( pta ) has become the treatment of choice in stenosis of access grafts [ 1 , 2 ]  . 
however , these stenoses , which are caused by intimal hyperplasia and proliferation of fibrous scar tissue , often resist dilatation with conventional angioplasty balloons [ 35 ] and high - pressure balloons [ 6 ]  . 
more recently , new applications in extracardiac vascular surgery have been proposed [ 1013 ] , in particular , in the treatment of stenoses of dialysis access sites [ 3 , 6 , 14 , 15 ]  . 
 materials and methods over the past 2 years , 80 patients were referred to our department for suspected stenosis of vascular haemodialysis accesses on the basis of the following clinical criteria : decreased thrill , increased pulsatility , oedema of the hand or forearm , low arterial pressure during dialysis . 
for this retrospective study , we collected data concerning 24 patients ( mean age 66.4 years , range 5081 ) presenting with 26 stenoses ( double stenosis in two patients ) in 24 haemodialysis accesses ( 21 cimino - brescia fistulae and 3 dialysis loops ) , which were treated by cutting balloon pta as a first choice or after failed conventional balloon angioplasty . 
twenty - three patients had a radiocephalic access and one had a femoral access . all patients had a failing fistula with a flow capacity < 300 ml / min as measured by the dialysis equipment and resulting difficulty in completing the dialysis procedure . before treatment , all patients underwent evaluation by colour doppler ultrasound ( cdus ) ( philips atl 5000 )  . stenosis was considered to be greater than 50% when peak systolic velocity was higher than 4 m / s and if the maximum velocity ratio was greater than 3 : 1 . 
subsequently , all patients underwent preprocedural angiography , with catheterisation of the humeral artery in 23 / 24 patients and of the common femoral artery in one patient ( using a 0.035 terumo hydrophilic guidewire and 4f terumo introducer sheath )  . 
la radiologia interventistica ha assunto negli ultimi anni un ruolo sempre pi importante nella prevenzione e nel trattamento della complicanze degli accessi vascolari per emodialisi ; in particolare langioplastica percutanea ( pta ) diventata il trattamento di scelta in caso di stenosi dei grafts con protesi [ 1 , 2 ]  . 
nellultimo decennio sono stati pubblicati numerosi lavori riguardanti questo device ; la maggior parte delle casistiche riguarda lutilizzo dello stesso in ambito cardiologico [ 8 ] ed endo - urologico [ 9 ]  . 
pi recentemente sono state proposte diverse applicazioni del cutting balloon in ambito vascolare extra - cardiaco [ 1013 ] e in particolare nel trattamento delle stenosi degli accessi dialitici [ 3 , 6 , 14 , 15 ]  . materiali e metodi durante gli ultimi 2 anni sono stati inviati alla nostra osservazione 80 pazienti per sospetta stenosi dellaccesso vascolare per emodialisi sulla base dei seguenti criteri clinici : diminuito thrill , aumentata pulsabilit , edema della mano e dellavambraccio , bassa pressione arteriosa durante la dialisi ; in 10 pazienti non erano presenti stenosi morfologicamente superiori al 30% e pertanto non meritevoli di trattamento percutaneo ; 46 pazienti sono stati trattati con angioplastica con pallone convenzionale ; in questo studio retrospettivo sono stati raccolti i dati relativi a 24 pazienti ( et media 66 , 4 anni , range 5081 ) portatori di 26 stenosi ( duplice stenosi in 2 pazienti ) in 24 accessi per emodialisi ( 21 fistole di cimino - brescia e 3 loops dialitici ) che sono stati trattati mediante cutting balloon pta di prima intenzione o dopo fallimento di angioplastica con pallone convenzionale . ventitr pazienti erano portatori di accesso radio - cefalico e 1 / 24 di accesso femorale . tutti i pazienti presentavano una failing fistula con portata della pompa misurata dallapparecchiatura di dialisi < 300 ml / min e conseguente difficolt allespletamento della procedura dialitica . 
la valutazione pre - trattamento stata effettuata in tutti i casi , con eco - color doppler ( philips atl 5000 ) : si considerato una stenosi superiore al 50% quando il picco di velocit sistolica era superiore a 4 m / s e se il rapporto di massima velocit era superiore a 3 : 1 ; successivamente tutti i pazienti sono stati sottoposti a studio angiografico preliminare alla procedura , espletato mediante cateterismo dellarteria omerale in 23 / 24 pazienti e dellarg . 
lo studio preliminare stato condotto tramite cateterismo arterioso in quanto nella nostra esperienza liniezione di mdc da tale versante consente di visualizzare in maniera ottimale laccesso per emodialisi lungo tutto il suo decorso e non crea intralcio al successivo cateterismo venoso per lespletamento di una eventuale procedura di angioplastica . 
il grado delle stenosi trattate era compreso tra 30% e 90% . previo consenso informato da parte del paziente , abbiamo proceduto allincannulamento del versante venoso con superamento della stenosi che stato conseguito con lutilizzo di guida idrofilica 0 , 035 ( terumo ) e catetere idrofilo ( 4f glidecath / terumo )  . 
successivamente stato posizionato un introduttore 6 / 7f ( terumo ) e si provveduto alla sostituzione della guida 0 , 035 con una guida 0 , 018 ( sv wire / cordis ) mediante catetere retto 5 f ( cordis )  . 
nei pazienti con duplice stenosi abbiamo impiegato lo stesso device per il trattamento di entrambe . la dilatazione stata eseguita mediante siringa dotata di manometro ( medflator ii / medex medical ) con insufflazione fino a 20 atm , mantenuta per 1 minuto , nel caso di un pallone ad alta pressione , e con insufflazione graduale del pallone ( 1 atm / 5 s ) fino ad una pressione di 6 atm ( tranne in 3 casi in cui si raggiunta una pressione di 78 atm determinante rottura del pallone ) con conseguente sgonfiaggio una volta raggiunta la pressione desiderata quando stato impiegato il cutting balloon . 
il follow - up stato pertanto espletato mediante valutazione clinica e con eco - color doppler a 1 , 3 , 6 , 12 , 18 e 24 mesi . risultati il successo tecnico immediato stato documentato in tutte le fig . 
1 cutting balloon : pallone da angioplastica non convenzionale con 3 o 4 aterotomi ( lame microchirurgiche ) montate longitudinalmente sulla superficie esterna ( cortesia boston scientific )  . inary study was carried out using arterial catheterisation because we have found that arterial injection of contrast material allows for optimal visualisation of the entire course of the haemodialysis access and does not interfere with possible subsequent venous catheterisation carried out for angioplasty procedures . 
the degree of stenosis ranged from 30% to 90% . after obtaining the patients informed consent , we proceeded to cannulate the vein crossing the stenosis using a 0.035 terumo hydrophilic guidewire and a 4f hydrophilic catheter ( terumo glidecath )  . 
a 6 / 7f terumo introducer sheath was subsequently inserted , and the 0.035 guidewire was exchanged for a 0.018 guidewire ( sv wire , cordis ) through a straight 5f catheter ( cordis )  . 
in patients with two stenoses , these were both treated using the same device . dilatation was carried out using a syringe equipped with a manometer ( medflator ii , medex medical )  . if high - pressure balloons were used , these were inflated up to a pressure of 20 atm , maintained for 1 min , whereas if the cutting balloon was used , it was inflated gradually ( 1 atm / 5 s ) up to 6 atm ( except for three cases in which a pressure of 78 atm was reached , causing balloon rupture ) g . 
when this was the case , we first negotiated the stenosis with a stiff guidewire ( amplatz super stiff , boston scientific ) and then advanced the balloon through the introducer sheath , which was withdrawn before inflation . there were no minor complications or early thromboses . in 3 cases , the balloon ruptured owing to inflation to 78 atin all 3 cases , the device could be removed in one piece without difficulty or complications . 
 clinical success was achieved in all patients ( 24 / 24 ) , with restored function of the access ( 24 / 24 ) used for dialysis within 2 days of the procedure . 
during follow - up ( mean 18.2 months , range 324 ) there was one case of restenosis which was not haemodynamically significant ( < 20% ) and did not impair access function . 
 discussion a functioning vascular access for haemodialysis is of crucial importance for efficient dialysis procedures and requires accurate monitoring , as it may be affected by a series of problems with patency rates at 1 year of 41%75% [ 16 ]  . 
 fibrotic changes resulting from repeated punctures [ 15 ] and haemodynamic conditions arising above all in the anastomoses and efferent vein through intimal hyperplasia induced by turbulent flow and high pressure applied on the efferent vein underlie the formation of stenoses . this reduction in calibre entails decreased access capacity with resulting impaired efficiency of the access during dialysis , which requires a flow capacity of at least 300 ml / min [ 19 ]  . 
monitoring access flow and prompt treatment of haemodynamically significant stenoses ( > 50% ) are required to increase the life span of an access site and decrease its rate of thrombosis [ 20 , 21 ]  . endovascular treatments have taken on a major role in the management and salvage of vascular dialysis accesses and now constitute the treatment of choice [ 20 ] due to the lower relazione alla rigidit del device e al ridotto calibro della guida portante : in questo caso stato dapprima avanzato lintroduttore oltre la stenosi con lausilio di una guida rigida ( amplatz super stiff , boston scientific ) ; successivamente il pallone stato avanzato allinterno dellintroduttore che stato poi ritirato prima dellinsufflazione . 
in 3 casi si verificata la rottura del pallone quando lo stesso stato insufflato a 78 atm ; in tutti i 3 casi il device stato rimosso integro , senza difficolt e senza complicanze . 
in tutti i pazienti ( 24 / 24 ) si ottenuto anche un successo clinico con ripristino della funzionalit dellaccesso ( 24 / 24 ) che stata utilizzata per la procedura dialitica entro 2 giorni dal trattamento . 
in 23 / 24 pazienti laccesso si pertanto mantenuto pervio e funzionante ed stata utilizzato durante le procedura dialitica con una perviet primaria del 95% . discussione la disponibilit di un accesso vascolare per emodialisi ben funzionante un elemento di grande importanza per lespletamento della procedura dialitica e richiede una gestione molto accurata in quanto gravata da una serie di problemi con tassi di perviet a 1 anno del 41%75% [ 16 ]  . 
la presenza di una stenosi il fattore responsabile del malfunzionamento e della trombosi dello stesso in oltre il 90% dei casi [ 1 , 2 , 17 , 18 ]  . 
le alterazioni fibrotiche dovute ai traumatismi legati alle punture ripetute [ 15 ] e le condizioni emodinamiche che si creano , soprattutto in corrispondenza delle anastomosi e del versante efferente dellaccesso , rappresentano , attraverso liperplasia miointimale indotta dal flusso turbolento e dalle elevate pressioni cui viene esposta la parete della vena efferente , il substrato eziopatogenetico della stenosi . 
tale riduzione di calibro comporta una diminuzione della portata dellaccesso con conseguente compromissione della efficienza dello stesso durante la dialisi che richiede un accesso con portata di almeno 300 ml / min [ 19 ]  . 
il monitoraggio del flusso dellaccesso e il trattamento tempestivo delle stenosi emodinamicamente significative ( > 50% ) sono necessari al fine di aumentare la vita dellaccesso e di diminuirne la percentuale di trombosi [ 20 , 21 ]  . 
i trattamenti endovascolari hanno assunto un ruolo fondamentale nella gestione e nel salvataggio degli accessi vascolari dialitici e rappresentano oggi lapproccio terapeutico di prima scelta [ 20 ] , in quanto gravato da minori tassi di complicanze rispetto alla chirurgia [ 5 ]  . 
la pta la procedura endovascolare di scelta [ 1 , 2 ] per il trattamento delle stenosi degli accessi vascolari con tassi di successo tecnico compresi tra 85% e 94% [ 2224 ]  . 
pta is the endovascular treatment of choice [ 1 , 2 ] for vascular access stenosis , with rates of technical success ranging from 85% to 94% [ 2224 ]  . 
pta nonetheless suffers some limitations , especially as regards anastomotic stenoses [ 3 ] and the high incidence of restenosis with a 2 - year patency rate of 20%30% [ 2224 ]  . the high incidence of post - pta recoil , caused by the pathogenesis of this type of stenosis [ 3 , 4 ] , has stimulated the search for new devices and alterative endovascular procedures [ 19 ]  . 
as regards pta , proposals include the use of high - pressure balloons [ 5 , 6 ] and prolonged inflation with devices that allow simultaneous perfusion of the fistula [ 3 ]  . 
in addition , the presence of the stent increases the incidence of thrombosis limiti legati alle stenosi resistenti , soprattutto in prossimit dellanastomosi [ 3 ] e dallelevata incidenza di restenosi con tasso di perviet a 2 anni del 20%30% [ 2224 ]  . 
lelevata frequenza di recoil post - pta , determinata dalla particolare patogenesi di questo tipo di stenosi [ 3 , 4 ] , ha favorito la ricerca di nuovi devices e di procedure endovascolari alternative [ 19 ]  . 
per quanto riguarda la pta stato proposto lutilizzo di palloni ad alta pressione [ 5 , 6 ] e linsufflazione prolungata con dispositivi che consentono la contemporanea perfusione della fistola [ 3 ]  . 
lintegrazione della pta con lo stenting non sembra migliorare i risultati dellangioplastica [ 25 ] ; inoltre la presenza dello stent aumenta lincidenza di trombosi e riduce larea disponibile per la puntura [ 26 ]  . 
il cutting balloon , device che unisce i principi della microchirurgia e dellangioplastica percutanea , stato proposto per la prima volta nel 1991 da barath per pta coronarica al fine di cong . 
 the cutting balloon , a device that combines the principles of microsurgery with those of percutaneous angioplasty , was first proposed by barath in 1991 to control intimal hyperplasia and decrease restenosis rate in coronary pta [ 7 ]  . 
it consists of a noncompliant balloon equipped with three or four microblades ( atherotomes ) mounted longitudinally on the outer surface of the balloon . balloon expansion exposes the microblades , which cut into the intima in a controlled manner , allowing vessel dilatation without the irregular intimal tears caused by conventional balloons [ 27 ]  . the regular incisions involve minimal exposure of the media with reduced procoagulation and local inflammatory responses and lesser extent of repair process [ 7 , 28 ]  . 
it appears that after cutting balloon dilatation , there is less expression of neutrophil adhesion molecules and the expression of cell growth and proliferation factors is not circumferential but limited to the intimal incisions . 
these factors are apparently responsible for the lower rates of restenosis [ 28 ]  . the cutting action of the microblades creates an area of least resistance in the fibrous strand at the level of the stenosis , enabling balloon inflation . 
the cutting balloon may therefore also enhance the efficacy of conventional pta by allowing greater balloon expansion [ 3 ]  . beginning in 1991 , many papers have addressed the use of the device in coronary arteries [ 8 ]  . 
more recently , other studies have demonstrated its good results in other districts , above all when the stenosis is caused by intimal hyperplasia and fibrosis [ 1013 ]  . applicability of the device to the venous system and in particular to the treatment of stenotic fistulae was demonstrated by vorwerk et al . 
 [ 3 ] published the results achieved in 15 cimino - brescia fistulae and four haemodialytic shunts showing a primary patency of 100% postprocedure of 94% at 6 months and of 64% at 69 months . 
in 2005 , singer - jordan published the interesting results of a prospective study of 29 patients with arteriovenous fistulae for a total of 42 stenoses in which the immediate technical success was 100% , primary patency was 76% at 6 months and secondary patency was 93% [ 29 ]  . a previous paper of ours reported our experience with cutting balloon pta in 21 patients followed up for mean period of 11.1 months [ 30 ]  . 
regular monitoring of these patients allowed us to verify the efficacy of the treatment , even in the medium term ( 18.2 months ) , confirming a primary patency of 95% . at long - term follow - up , we recorded only one case of haemodynamically significant restenosis in a patient in whom vessel diameter had been originally underestimated . the stenosis was treated after 6 months with a repeat cutting balloon pta procedure , which had immediate technical success . 
in all patients , the cutting balloon expanded rapidly to its full diameter without the need for prolonged dilatations , trollare liperplasia intimale e diminuire il tasso di restenosi [ 7 ]  . 
quando questo viene insufflato si realizza lesposizione delle microlame che provocano una incisione controllata dellintima in modo da permettere la dilatazione del vaso evitando le lacerazioni irregolari dellintima causate dai palloni convenzionali [ 27 ]  . 
le incisioni regolari comportano una minima esposizione della media con ridotta risposta procoagulante e infiammatoria locale e minore entit dei processi riparativi [ 7 , 28 ] ; sembra infatti che dopo dilatazione con cutting balloon si verifichi una minore espressione di molecole di adesione per i neutrofili ; inoltre lespressione di fattori di crescita e la proliferazione cellulare non sono circonferenziali , ma limitati alle incisioni dellintima . 
a partire dal 1991 sono stati pubblicati numerosi lavori riguardanti lutilizzo del device a livello coronarico [ 8 ]  . pi recentemente altri studi ne hanno dimostrato i buoni risultati in stenosi resistenti in altri distretti , soprattutto laddove la riduzione di calibro sostenuta da iperplasia intimale e fibrosi [ 1013 ]  . 
lapplicabilit del device al distretto venoso ed in particolare al trattamento delle stenosi delle fistole stata dimostrata da vorwerk nel 1995 [ 15 ] ; successivamente lo stesso vorwerk nel 1996 [ 3 ] ha pubblicato i risultati riguardanti 15 fistole di cimino - brescia e 4 shunts emodialitici con una perviet primaria del 100% alla fine della procedura , del 94% a distanza di 6 mesi e del 64% a 69 mesi ; bittl e feldman [ 6 ] hanno trattato 3 stenosi di graft con successo tecnico immediato del 100% e tasso di restenosi del 16 , 6% durante un follow - up medio di 6 , 7 mesi ; ryan et al . 
nel 2005 singer - jordan ha pubblicato degli interessanti risultati di uno studio prospettico di 29 pazienti con fistola artero - venosa per un totale di 42 stenosi riportando un successo tecnico immediato del 100% , una perviet primaria del 76% a 6 mesi e una perviet secondaria del 93% [ 29 ]  . 
in un precedente lavoro abbiamo gi riportato la nostra esperienza riguardante la pta con cutting balloon in 21 pazienti seguiti in media per 11 , 1 mesi [ 30 ]  . 
durante il follow - up prolungato abbiamo riportato solo un caso di ristenosi emodinamicamente significativa in una paziente in cui avevamo inizialmente sottostimato il diametro del vaso ; la stenosi stata trattata a 6 mesi di distanza con una nuova cutting balloon pta con successo tecnico immediato . 
in tutti i pazienti , il cutting balloon si espanso rapidamente al proprio diametro senza necessit di dilatazione prolungate , tranne nei 3 casi in cui si dovuto sovradilatare fino a 78 atm ( pressione di rottura del pallone ) in quanto a 6 atm la divulsione della stenosi non era iconograficamente soddisfacente : tale comportamento verosimilmente da mettere in relazione al fatto che lincisione g . 
 conclusions on the basis of our experience and previous reports , we can state that cutting balloon angioplasty is a safe and effective procedure for the treatment of haemodialysis - access stenosis with low rates of restenosis in the short and medium term in that it provides excellent results even in focal , tight stenoses that are resistant to dilatation with high - pressure balloons . nonetheless , randomised controlled studies on larger patient populations are required to confirm our encouraging results on the efficacy of the device in prolonging access patency . 
in addition , the economic impact of the use of cutting balloons should be assessed given that , despite having a higher unit cost compared with conventional pta balloons , these devices require fewer maintenance procedures . dellintima riduce il barotrauma sulla parete vasale , richiedendo pressioni di insufflazione minori . 
questo aspetto particolarmente vantaggioso se consideriamo che nella nostra serie i pazienti trattati con palloni convenzionali ad alta pressione avvertono dolore che richiede sedazione o supporto anestesiologico . conclusioni in base a quanto emerge dallesperienza personale e dai dati riportati in letteratura , possibile affermare che langioplastica mediante cutting balloon una procedura sicura ed efficace nel trattamento delle stenosi degli accessi vascolari per emodialisi , in quanto consente di ottenere ottimi risultati anche nelle stenosi focali serrate , resistenti alla dilatazione con palloni ad alta pressione , con bassi tassi di restenosi a breve e medio termine . 
sono comunque necessari ulteriori studi , randomizzati e controllati , numericamente pi consistenti al fine di confermare gli incoraggianti risultati della nostra serie riguardante lefficacia del device nel prolungare la perviet degli accessi . 
solivetti , via citt della pieve 19 , i - 00191 roma , italy , tel . : + 39 - 06 - 52666447 , fax : + 39 - 06 - 52663937 , e - mail : solivetti@tiscalinet.it received : 15 september 2005 / accepted : 17 february 2006 / published online : 29 june 2006 abstract purpose . 
following a review of the relevant literature , we present the results of a retrospective study based on 2 , 000 malignant melanoma patients with complete case records . of these , we selected 600 patients who had a thick melanoma ( > 1 mm ) at presentation but were clinically free of in - transit or satellite melanoma metastases during follow - up . 
a total of 95 lesions were identified . average lesion diameter was 0.7 mm , and only four were larger than 1 call suspected lesions were confirmed by surgery , follow - up or us - guided fine - needle aspiration ( fna ) with 22gauge needles using a freehand technique and exploiting the capillarity principle . 
in this series , there were apparently no false positive or false negative us results although inclusion criteria precluded correct evaluation of possible false negatives . minimum lesion diameter allowing sonographic detection appears to be around 0.4 mus features of in - transit metastases have been well documented . 
dopo revisione della letteratura di pertinenza , gli autori presentano i risultati di uno studio retrospettivo basato su un archivio di dati clinico - radiologici completi relativi a 2000 pazienti . 
nellambito di tale ampia casistica sono stati presi in considerazione 600 casi , riguardanti pazienti che avevano , al momento della valutazione iniziale , una lesione melanomatosa di maggior spessore ( > 1 mm ) , ma riscontrati clinicamente negativi per metastasi in transito o satelliti di melanoma nel follow - up clinico . 
nellambito di tale popolazione di pazienti clinicamente negativi , in 63 casi , il sospetto di metastasi in transito o satellite stato posto ecograficamente , e sono state individuate 95 lesioni , con dimensioni medie di 0 , 7 mm e solo in quattro casi di dimensioni > 1 ctutte le lesioni sospette sono state confermate chirurgicamente , con follow - up o mediante esame cito - aspirativo , eseguendo il prelievo citologico sotto guida ecografica , con aghi da 22 g , sfruttando il principio di aspirazione per capillarit . 
sotto il profilo ecografico le dimensioni minime accettabili per poter identificare una lesione metastatica sembrano essere intorno a 0 , 4 mle caratteristiche ecografiche delle metastasi da melanoma sono ben documentate in letteratura . 
solitamente si tratta di lesioni solide ipoecogene , rispetto al tessuto adiposo sottocutaneo circostante , con margini abbastanza netti e definiti , con una buona trasmissione degli ultrasuoni ( us )  . 
queste caratteristiche ecografiche in ecografia dermatologica sono piuttosto aspecifiche per tutti i tipi di metastasi , ma , tra le patologie benigne , soltanto site of a malignant melanoma should be more widely used and associated with us - guided fna biopsy . key words ultrasound in - transit metastasis cutaneous malignant melanoma f.m. 
gli autori desiderano promuovere ed incoraggiare un pi ampio impiego dellecografia nel follow - up dei tessuti molli circostnati la sede iniziale dei melanomi , associata al prelievo citologico sotto guida ecografica . parole chiave ultrasuoni metastasi in transito melanoma maligno cutaneo introduction introduzione cutaneous malignant melanoma ( mm ) is a relatively common malignancy . 
its incidence is rapidly increasing , with rates doubling every 1020 years [ 1 , 2 ] , and it is the third most frequent cancer to give rise to cutaneous metastases , with an incidence of 24% [ 3 ]  . melanoma recurrences in soft tissue are known as satellite metastases when located within 2 cm from the primary lesion and in - transit metastases when located in the cutaneous or subcutaneous tissues more than 2 cm from the primary tumour . 
in particular , the use of probes with frequencies between 7.5 and 20 mhz has enabled a more accurate differential diagnosis between mm recurrences / metastases and skin metastases from other malignancies and even between mm metastases and other conditions , such as fibromas , lipomas and aberrant scars [ 5 ]  . the aim of this study was to assess the potential of us in detection of in - transit or satellite metastases on the basis of a large case series . il melanoma maligno cutaneo ( mm ) una patologia aggressiva relativamente comune , con frequenza in incremento ; stato osservato che il suo tasso dincidenza raddoppia ogni 1020 anni [ 1 , 2 ] ; esso rappresenta inoltre la terza neoplasia che , in ordine di frequenza , determina metastasi a livello cutaneo , con unincidenza del 24% [ 3 ]  . le recidive di melanoma nei tessuti molli sono chiamate satelliti se sono nel raggio di 2 cm dalla lesione primitiva , mentre quelle cutanee e sottocutanee lontane pi di 2 cm sono definite come metastasi in transito . 
esse si sviluppano lungo la via linfatica tra la lesione primitiva e la stazione linfonodale di drenaggio [ 4 ]  . la diagnosi precoce di queste recidive stata incrementata dalluso dellecografia ( us ) , con sonde ad alta frequenza . 
in particolare , luso di sonde di frequenza compresa tra 7 , 5 e 20 mhz ha reso possibile una pi accurata diagnosi differenziale tra recidive - metastasi da mm e metastasi cutanee da altre patologie maligne od anche tra metastasi da mm ed altre ipotesi diagnostiche , quali fibromi , lipomi e cicatrici aberranti [ 5 ]  . lo scopo del lavoro di verificare le attuali possibilit dellecografia nel riconoscimento di metastasi in transito e satelliti sulla base dei dati di una casistica molto numerosa . materials and methods a total of 600 patients were selected on the basis of the following inclusion criteria : ( 1 ) patients affected by mm with a thickness greater than 1 mm ; ( 2 ) patients who underwent wide surgical excision and assessment of sentinel node , and removal of the draining lymph node station in the case of positive sentinel node . 
during follow - up , all study patients underwent clinical assessment every 6 months , and if the findings were negative , a yearly us examination of the surgical scar and surrounding tissue within a radius of 10 cm from the tumour materiali e metodi nel nostro studio abbiamo selezionato 600 pazienti , sulla base dei seguenti criteri di inclusione : ( 1 ) pazienti affetti da mm di spessore superiore ad 1 mm ; ( 2 ) pazienti trattati chirurgicamente con escissione ampia della lesione , valutazione del linfonodo sentinella ed , in caso di positivit dello stesso , svuotamento della stazione linfonodale di drenaggio . 
i 600 pazienti erano 336 di sesso femminile e 264 di sesso maschile , con et media di 54 anni ; di essi il 60% ha raggiunto i previsti 5 anni di follow - up . 
 all us examinations were carried out with an esaote au5 unit ( genoa , italy ) using a 20 - mhz annular array probe and 13 and 7.5 mhz linear probes ; standard chest radiographs and total - body computed tomography ct scans were also performed , as per protocol . 
colour - doppler us was performed using settings allowing assessment of slowflow conditions ( therefore using the most sensitive low - cut filter and the units highest sensitivity setting ; flow velocities that can be detected are in the order of a few centimetres per second ) and taking multiple samplings in different areas of the lesion ; the sampling volume for pulsed doppler us was chosen in relation to the expected vessel size , below 1 mm . fine - needle aspiration ( fna ) was carried out after obtaining written informed consent and using a freehand technique under sonographic guidance ; samples were taken with 23gauge needles exploiting the capillarity principle thus without applying vacuum and making two passes for each nodule . 
 results out of 600 patients who were clinically free of local recurrence , us examination raised the suspicion of in - transit metastasis ( 39 cases ) or satellite lesion ( 24 cases ) in 63 patients . 
in these patients , the primary lesion had a mean thickness of 2 mm and was located on the limbs in 41 cases and on the trunk in 22 cases . 
the time interval between detection of the new lesion and surgical excision of the primary tumour was about 2 years , with a range of 6 months to 5 years . 
of the 32 patients who underwent fna , cytology provided a definitive diagnosis of metastasottoposti ad esame clinico ogni 6 mesi e , se obbiettivamente negativi , ad ecografia annuale dei tessuti molli dellarea cicatriziale e della zona ad essa circostante , in un raggio di circa 10 cm , intorno alla sede originaria della neoplasia . parte rilevante dei pazienti positivi sono stati trattati senza ulteriori indagini diagnostiche per immagini locoregionali . tutti gli esami ecografici sono stati eseguiti con ecografo esaote au5 ( genova , italia ) , impiegando sonda anular array da 20 mhz e sonda lineare da 13 e 7 , 5 mhz ; sono stati inoltre effettuati radiogrammi toracici standard ed esami tc total body , come da protocollo . lesame color doppler stato eseguito con impostazione dei parametri tale da consentire la valutazione dei flussi pi bassi ( quindi impiegando il filtro taglia - basso pi sensibile e con la sensibilit in ricezione pi alta consentita dallapparecchiatura in uso ; le velocit di flusso rilevabili sono nellordine di pochi cm / s ) ; effettuando inoltre plurimi campionamenti in aree diverse della lesione ; per ci che concerne il doppler pulsato , il volume campione stato scelto in relazione alle dimensioni attese dei vasi , al di sotto del millimetro . per la fna si sempre ottenuto consenso informato preliminare scritto e si impiegata una tecnica a mano libera , sotto assistenza ecografica , con aghi sottili da 23 g , utilizzando il principio della capillarit e senza quindi applicare il vuoto ed effettuando normalmente due successivi prelievi per ogni nodulo . risultati tra questi 600 pazienti , in 63 casi - clinicamente negativi per ricorrenza locale stata posta diagnosi ecografia di sospetta metastasi in transito ( 39 casi ) o lesione satellite ( 24 casi )  . 
in questi 63 pazienti , la lesione primitiva aveva uno spessore medio di 2 mm , era localizzata in 41 casi agli arti ed in 22 casi al tronco ; lintervallo di tempo tra la documentazione della nuova patologia ed il trattamento chirurgico della lesione primitiva era di circa 2 anni , con un minimo di 6 mesi ed un massimo di 5 anni . in questi 63 pazienti stato trovato un totale di 95 lesioni , con un massimo di 4 noduli per paziente . 
le lesioni campionate con fna avevano un diametro medio di 7 mm , con un minimo di 5 mm ed un massimo di 13 mnon vi sono stati casi falsi positivi . discussione la ricerca e la diagnosi di localizzazioni secondarie , in pazienti affetti da mm , rappresentano ovviamente un punto cardine nel percorso terapeutico . 
gi da tempo gli ultrasuoni sono stati utilizzati in questo specifico settore ; in particolare , il primo a proporre il ricorso allecografia per la ricerca di metastasi , satelliti od in transito , stato fornage [ 6 ]  . 
il suo studio , basato su tre casi , descriveva tali lesioni come solide , ipoecogene e con contorni netti ; altri autori [ 7 ] , in seguito , hanno descritto ulteriori caratteristiche ecografiche di tali metastasi quali , ad esempio , la presenza di segnali vascolari allinterno del nodulo , evidenziabili con il color doppler e , assai meglio , con il power doppler , oppure la presenza di piccole aree fluide interne , dovute a fenomeni di necrosi . nella nostra esperienza abbiamo potuto verificare inoltre come la maggior parte di queste lesioni si localizzi in un raggio di 10 cm dalla lesione primitiva e , in riferimento alla nostra casistica , costituita da pazienti con melanoma di spessore superiore ad 1 mm , tale metodologia dindagine ci ha consentito di identificare lesioni metastatiche nel 10% dei casi nel corso del follow - up . abbiamo potuto verificare come le caratteristiche di queste lesioni coincidano con quanto descritto in letteratura ; in particolare : la presenza di aree fluide interne sembra legata a fenomeni di necrosi e quindi pi frequente nelle patologie di maggiori dimensioni , dove il flusso ematico insufficiente ; tali ripetizioni possono inoltre mostrare contorni netti ma leggermente irregolari ; esse possono infine mostrare buona trasmissione del fascio ultrasonoro e rinforzo di parete posteriore , con frequentemente segnali vascolari interni al power doppler . per le modeste dimensioni delle lesioni e per i limiti tecnici delle apparecchiature impiegate , non possibile esprimere un definitivo giudizio circa il vero pattern vascolare di questo tipo di patologia.una corretta stima dei falsi negatifig . 
2 la sonda lineare da 13 mhz documenta la presenza di una formazione nodulare , ipoecogena , a margini lievemente sfumati . sis in 25 and a probable diagnosis of metastasis in seven . 
lesions sampled with fna had a mean diameter of 7 mm , with a range of 513 mthere were no cases of false positive results . discussion in patients with mm , detection and diagnosis of metastases are clearly crucial steps in the therapeutic process , and us has long been used for this purpose . 
fornage was the first to propose us for the search for satellite or in - transit metastases [ 6 ]  . his study , based on three cases , described the lesions as being solid , hypoechoic and well circumscribed . 
3 la sonda lineare da 13 mhz documenta la presenza di una formazione nodulare , modestamente disomogenea , per la presenza di qualche millimetrica area fluida al suo interno . doppler us and especially with power - doppler us or the presence of tiny internal fluid areas due to necrosis . 
in our experience we also found that most of these lesions are located within 10 cm from the primary lesion and , as regards patients with melanoma with a thickness > 1 mm , that us enabled detection of metastasis in 10% of cases during follow - up . sonographic features of the metastatic lesions identified in our study were in agreement with the literature . 
more specifically : the presence of internal fluid areas appears to be related to necrosis and is therefore more common in larger lesions , where blood flow is insufficient metastatic lesions may also exhibit well - defined but slightly irregular contours . metastatic lesions may also show good sound - wave transmission and posterior shadowing , frequently with internal vascular signals at power - doppler imaging . given the small size of the lesions and the technical limitations of the us equipment used , we are unable to express a definitive judgement on the vascular pattern of the disease . 
likewise , correct estimation of sonographic false negatives , despite long - term follow - up , cannot be provided owing to the retrospective nature of the study , the yearly intervals for us followup and the relatively high rate of patients lost to follow - up ; every year , about 8% of our patients fail to attend routine follow - up appointments though they appeared to be in good health at the previous examination . 
it should be recalled that by including patients with mm with a thickness greater than 1 mm and excluding those with a clinical diagnosis of recurrent disease , this retrospective study does not allow assessment of the true incidence of satellite and in - transit metastases . 
for detection of metastatic lesions , it is important to use multiple us probes , from 7.5 up to 20 mhz , or an appropriate multifrequency probe , if possible , because depending on its site and size a lesion may be well visualised at a given frequency but totally invisible at another . 
as regards differential diagnoses in this phase , an abnormal scar shows blurred contours and is often avascular whereas a granuloma often incorporates the foreign body and tends to be hypovascular or avascular at colour imaging . 
on the basis of our experience , given that we detected no lesions smaller than 4 mm , it seems reasonable to consider 4 mm as the threshold value for the identification of such lesions . as previously stated , the characteristics of our study population do not allow us to exclude the existence of false negative results . 
even though some of the lesions identified at the second , third , fourth or fifth us follow - up examination might have been present earlier but were too small to detect , the doubling time of these tumours makes this hypothesis unlikely . 
in our series , 52 patients out of 63 were negative at the first follow - up and became positive during the follow - up period . fornage [ 6 ] was the first to propose us as a modality to guide fna . 
fanelli , tel : + 39 - 06 - 4455602 , fax : + 39 - 06 - 490243 , e - mail : fabrizio.fanelli@uniroma1.it received : 7 july 2005 / accepted : 27 january 2006 / published online : 29 june 2006 abstract transjugular intrahepatic portosystemic shunt ( tips ) is a nonoperative therapeutic option for the management of portal hypertension , variceal bleeding , recurrent ascites , budd - chiari syndrome . 
in view of the many issues surrounding the use of tips , in 1994 the us national digestive diseases advisory board convened a scientific conference to review the current data available and to establish the indications and controindications for this procedure . 
however there are still unsolved problems especially short primary patency of the shunt due to intimal hyperplasia , which causes a reduction of the shunt lumen thus favoring a return of the portal hypertension with recurrent variceal bleeding . 
in our experience more then 100 patients were treated with the viatorr stent - graft . after a follow - up ranging from 1 to 50 months we reported a 1 - year primary patency rate of 83.8%. 
in case of hepatic hencefalopathy refractory to the conventional medical therapy , tips reduction should be performed . key words tips portal hypertension covered stents hepatic encephalopathy viatorr riassunto lo shunt transgiugulare intraepatico portosistemico ( tips ) una procedura terapeutica , non chirurgica , per il trattamento dellipertensione portale , del sanguinamento da varici esofagee , dellascite refrattaria e della sindrome di budd - chiari . dallintroduzione della tips nella pratica clinica , sono state avanzate diverse teorie sullutilizzo di tale metodica . 
per tale motivo , nel 1994 la national digestive diseases advisory board americana si riunita in una conferenza per stabilire , sulla base dei dati disponibili in letteratura , le linee guida con indicazioni e controindicazioni alla procedura . 
tuttavia esistono ancora dei problemi irrisolti correlati principalmente con la ridotta perviet primaria conseguente ad iperplasia neo - intimale con progressiva riduzione del lume dello shunt che favorisce la ricomparsa dei sintomi . 
nella nostra esperienza pi di 100 pazienti sono stati trattati con il viatorr e dopo un follow - up compreso tra 1 e 50 mesi la perviet primaria stata del 83.8%. 
in caso di encefalopatia epatica refrattaria alla terapia medica convenzionale , necessario effettuare una riduzione dello shunt . parole chiave tips ipertensione portale stent ricoperti encefalopatia epatica viatorr introduction introduzione the transjugular intrahepatic portosystemic shunt ( tips ) is a nonoperative therapeutic option for the management of portal hypertension , variceal bleeding , recurrent ascites and budd - chiari syndrome . 
the portal venous system is partially decompressed by the creation of a parenchymal tract between the portal ( pv ) and hepatic ( hv ) veins followed by reinforcement of the tract with a metallic stent . 
from 1969 , when this procedure was used for the first time in dogs lo shunt transgiugulare intraepatico portosistemico ( tips ) una procedura terapeutica , non chirurgica , per il trattamento dellipertensione portale , del sanguinamento da varici esofagee , dellascite refrattaria e della sindrome di budd - chiari . il sistema venoso portale parzialmente decompresso mediante la creazione di un tramite intraparenchimale tra la vena porta e le vene sovraepatiche , rinforzato da uno stent metallico . 
in the 1980s , metallic stents were developed and used by palmaz and rosch , and in 1983 , colapinto performed for the first time this procedure in a human [ 2 ]  . 
however , the initial enthusiasm was subsequently tempered by several complications represented by hepatic encephalopathy ( he ) and shunt stenosis . patient selection in view of the many issues surrounding the use of tips , in 1994 , the us national digestive diseases advisory board convened a scientific conference to review the available data and establish indications and contraindications for this procedure [ 3 , 4 ]  . 
after tips , immediate cessation of bleeding is reported in 73%96% of cases [ 6 ] , with a recurrent variceal bleeding rate of 15%20% at 1 year [ 5 ]  . tips is particularly helpful when bleeding occurs from inaccessible intestinal or gastric varices or is the result of severe portal hypertensive gastropathy [ 3 ]  . 
tips has been found to be valuable in managing patients who have developed rebleeding despite receiving adequate medical or endoscopic therapy [ 3 , 8 ]  . many trials were published comparing tips with endoscopic treatment for the prevention of recurrent oesophageal variceal bleeding . 
a metaanalysis of these trials reported that tips is associated with a 28% reduction in recurrent bleeding compared with endoscopic therapy [ 5 ]  . la prima volta in un cane da rosch , molti studi sono stati effettuati per migliorare la tecnica e la perviet dello shunt . nel 1980 stato impiantato da palmaz e rosch uno stent metallico e , nel 1983 , colapinto effettu la procedura su un uomo per la prima volta [ 2 ]  . finalmente negli ultimi tre anni sono stati introdotti stent ricoperti per prolungare la perviet dello shunt evitando malfunzioni dovute alliperplasia intimale . 
tuttavia lentusiasmo iniziale si gradualmente stemperato a causa delle gravi complicanze rappresentate dallencefalopatia epatica e dalla stenosi dello shunt . selezione dei pazienti dallintroduzione della tips nella pratica clinica , sono state avanzate diverse teorie sullutilizzo di tale metodica . 
dopo tips la scomparsa immediata del sanguinamento riportata nel 73%96% dei casi [ 6 ] , con una percentuale di ricorrenza del sanguinamento ad un anno del 15%20% [ 5 ]  . la tips particolarmente efficace quando il sanguinamento origina da varici intestinali inaccessibili o da varici gastriche o quando il risultato di una severa gastropatia conseguente ad ipertensione portale [ 3 ]  . 
sia la scleroterapia che la terapia farmacologica con - bloccanti sono ben tollerate ed efficaci nel prevenire il sanguinamento ricorrente da varici ma i pazienti che hanno sviluppato un nuovo sanguinamento dopo terapia medica o endoscopica sono da ritenersi candidati alla tips [ 3 , 8 ]  . 
refractory ascites is defined as recurrent tense ascites that cannot be improved by routine medical care , including sodium restriction and diuretics , or that requires frequent paracenteses [ 6 ]  . 
ascites can represent , also , a technical problem because it pushes the liver up and makes the angle between the hepatic and the pvs more acute and more difficult for the needle catheter to traverse . 
the effect of tips in these patients is associated with a marked improvement of sodium and water handling of renal perfusion with a general clinical improvement [ 8 ]  . 
tips has been used successfully in the treatment of hepatic hydrothorax ; this is secondary to refractory ascites due to migration of ascitic fluid into the thoracic cavity along a pressure gradient . 
budd - chiari syndrome ( bcs ) results from obstruction of the hepatic venous outflow tract due to occlusion of hvs and / or inferior vena cava ( ivc )  . tips decreases portal congestion by creating a new hepatic venous outflow tract and improving hepatic blood flow with an increase of arterial blood supply to the liver . technically , tips placement in bcs is frequently challenging due to difficulties in identifying an hv as take - off point for the shunt . 
si definisce ascite refrattaria una ascite tesa che non pu essere migliorata attraverso i comuni accorgimenti medici compresi la restrizione sodica ed i diuretici , o una ascite che richiede frequenti paracentesi [ 6 ]  . 
lascite pu anche rappresentare un problema tecnico durante lesecuzione della tips perch spinge il fegato in alto e crea quindi un angolo pi acuto tra la vena porta e la vena epatica , che rende pi difficoltoso il passaggio dellago . 
per questo , nei pazienti con severa ascite consigliabile effettuare una paracentesi evacuativa , subito prima della procedura , per facilitare il successo tecnico . leffetto della tips in questi pazienti associato ad un marcato miglioramento della ritenzione di sodio e acqua , della perfusione renale , con un miglioramento clinico generale [ 8 ]  . 
la tips in grado di ridurre il gradiente pressorio porto - sistemico del 46%63% , con una risposta al trattamento che varia dal 50% al 92% [ 6 ]  . 
on the other hand , encephalopathy precipitated by acute , uncontrolled haemorrhage may be improved when tips is used to treat active variceal haemorrhage refractory to conventional therapy [ 3 , 6 ]  . 
 tips procedure tips is a multistep procedure that includes four key points : jugular - vein puncture , hepatic - vein incannulation , portalvein puncture and stent selection and position . 
the procedures were performed with the patient under deep sedation using a laryngeal mask with a mixture of o2 , n2o , and isoflurane ( 1%2% ) [ 12 ]  . jugular vein puncture the right internal jugular vein ( jv ) is the preferred access because the path to the liver is straight , with minimal angulation controindicazioni assolute 1 . 
il posizionamento della tips determina dei cambiamenti fisiologici anche sui pazienti in buone condizioni cliniche . la creazione con la tips di un canale intraepatico a bassa resistenza causa un flusso preferenziale attraverso lo stent diretto dalle varici e dai sinusoidi epatici attraverso lo shunt . 
in casi selezionati , viene eseguita una tc spirale per ottenere una migliore valutazione dellanatomia del fegato e delle patologie associate . procedura la tips una procedura multi - fasica che include quattro fasi : la puntura della vena giugulare , lincannulazione della vena epatica , la puntura della vena porta , la selezione dello stent e il suo posizionamento . 
needle guidance with real - time sonography is a very simple method that can be used in difficult cases and can also reduce the risk of haematoma or adverse carotid artery puncture . 
an 18 - gauge needle is directed towards the ipsilateral nipple and approximately to the medial third of the clavicle , performing a single - wall puncture with gentle aspiration . 
a 12 - f introducer sheath ( 35to 40 - cm long , daig , minnetonka , mn , usa ) is advanced into the right atrium for pressure measurement and then into the ivc . 
the hv is then catheterised directly using the curved metallic cannula of the tips set ( angiodynamics , queensberry , ny , usa ) and the glidewire ( terumo )  . 
a venogram is then performed in order to visualise the morphology of the hepatic vegenerally , we prefer to create the shunt from the right hv to the right portal branch . 
however , a short , straight path is preferred because of less trauma to the liver parenchyma . portal - vein puncture this is the most difficult and critical step of the tips procedure and requires special attention to avoid the risk of intraperitoneal haemorrhage secondary to liver capsule perforation . 
the puncture is generally performed through the wall of the hv 13 cm from its origonce the needle is into the hv , it is turned anteriorly and advanced into the liver parenchyma for 45 cit is then slowly retracted while performing a gentle aspiration with a 10 - cc syringe . 
many methods have been proposed to locate the pv : arterial portography , ct , us , and wedge hepatic portal venography with contrast media or with co2 [ 14 , 15 ]  . 
in our experience , a blind puncture was performed in 101 / 105 patients while in four cases ( 3.8% ) , us guidance was necessary to reach the pv . 
we prefer to create the shunt into the right pv 23 cm from its orig however , selection of the left portal branch is sometimes necessary in patients with advance cirrhosis because atrophy of the right hepatic lobe is f . 
il giorno prima della procedura deve essere intrapreso un trattamento antibiotico ev ( ceftriaxone , rocefin , hoffmann - la roche , kaiseraugust , ch ) e continuato per 48 ore . puntura della vena giugulare la principale via di accesso rappresentato dalla vena giugulare interna destra in modo che lago possa effettuare un percorso pi rettilineo possibile durante la puntura della vena porta . 
la vena giugulare interna destra localizzata 0 , 5 cm lateralmente allarteria carotide comune . la puntura viene praticata di solito con tecnica alla cieca , pungendo allapice dellangolo formato dai due capi del muscolo sternoscleidomastoideo . 
quando la giugulare interna destra non accessibile per agenesia , occlusione o legatura chirurgica , devono essere prese in considerazione altre vie di accesso quali la vena giugulare esterna destra , la vena giugulare sinistra o la vena succlavia . una volta punta la vena giugulare , una guida angolata idrofilica 0 , 035 ( terumo co , tokyo , giappone ) viene avanzata allinterno della giugulare fino alla vena cava inferiore . a questo livello la guida deve essere manipolata con cautela onde evitare la comparsa di extrasistoli . 
un introduttore da 12 f ( 3540 cm di lunghezza , daig co , minnesota , usa ) viene avanzato fino allatrio destro per effettuare la misurazione della pressione venosa centrale . 
la vena epatica viene cateterizzata direttamente usando la canula metallica curva del set tips ( angiodynamics inc , queensberry , ny , usa ) e la guida idrofilica ( terumo co , tokyo , giappone )  . 
tuttavia sempre preferibile praticare un tramite corto e diretto cos da ridurre il trauma del parenchima epatico . puntura della vena porta rappresenta la fase pi delicata di tutta la procedura e richiede unattenzione particolare per evitare il rischio di emorragia intraperitoneale secondaria ad uneventuale perforazione della capsula epatica . 
1 puntura della vena porta : dopo lincannulazione della branca principale della vena porta si esegue una flebografia per valutare il sito di puntura e la morfologia della vena porta . 
una volta avanzato lago allinterno della vena epatica , questo viene ruotato anteriormente e avanzato attraverso il parenchima epatico per 45 cm . lago viene quindi lentamente retratto praticando una leggera aspirazione con una siringa da 10 ml . 
sono stati proposti molti metodi per localizzare la vena porta : portografia arteriosa , tc , ecd , venografia portale epatica con mezzo di contrasto o co2 [ 14 , 15 ]  . nella nostra esperienza una puntura alla cieca stata praticata in 101 / 105 pazienti mentre in 4 casi ( 3 , 8% ) stato necessario utilizzare una guida ecografica per individuare la vena porta . 
per evitare complicanze , noi preferiamo creare lo shunt nel ramo destro della vena porta , a 23 cm dalla sua origine . la selezione del ramo sinistro della porta necessaria talvolta nei pazienti con cirrosi avanzata perch latrofia del lobo epatico di destra associato ad una posizione pi mediale del ramo destro che non pu essere raggiunto attraverso la vena epatica di destra . 
dato che il catetere percorre generalmente il tratto pi corto dello shunt , consigliabile selezionare uno stent circa 1 cm pi lungo rispetto alla misura ottenuta con il catetere centimetrato . successivamente , una guida super - stiff ( amplatz , boston scientific co , natick , ma , usa ) inserita nella vena splenica o mesenterica ed il tratto intraepatico viene dilatato con un catetere a palloncino a basso profilo ( wanda , boston scientific co , natick , ma , usa ) delle dimensioni corrispondenti al diametro dello stent . scelta dello stent il diametro dello stent deve essere stabilito in base a vari fattori : gradiente portosistemico , et del paziente , condizioni cliniche , grado di encefalopatia , funzionalit cardiaca . 
 afterwards , a super - stiff guidewire ( amplatz , boston scientific , natick , ma , usa ) is inserted into the splenic or mesenteric vein , and the intrahepatic tract is dilated using a low - profile balloon ( wanda , boston scientific ) of the size corresponding to the stent diameter or , in sicker patients , only to 8 mm . stent - graft selection the diameter of the stent must be tailored to the patients portosystemic gradient , age , clinical condition , preexisting encephalopathy , cardiac function and indication . 
following our experience , in older patients with reduced liver and cardiac functions , a small - calibre stent graft ( 8 mm ) can be used to decrease the incidence of encephalopathy . stent - graft design the viatorr stent graft consists of a self - expanding nitinol fig . 
3 misurazione del tratto intra - epatico : per ottenere la corretta lunghezza del tratto intra - epatico dello shunt viene avanzato in vena porta un catetere centimetrato pig - tail . 
la superficie esterna del rivestimento composta da una pellicola in eptfe modificato , a ridotta permeabilit per bile e mucina , che inibisce la crescita iperplastica di tessuto e permette un rinforzo radiale della superficie interna . 
la superficie interna a contatto con il sangue composta da e - ptfe con propriet meccaniche e microstruttura simile a quella degli stent vascolari prodotti con gore - tex . il viatorr ha un design costituito da una parte rivestita in e - ptfe per il tratto intraepatico e da una porzione scoperta , lunga 2 cm , per la regione portale ; disponibile in commercio in differenti diametri ( 8 , 10 , 12 mm ) e in differenti lunghezze ( 6 , 7 , 8 cm )  . 
in pi un altro piccolo marker in oro incorporato nellestremit prossimale della porzione ricoperta per migliorare limmagine fluoroscopica durante il posizionamento del viatorr . rilascio dello stent il viatorr ( wl gore e associati , flagstaff , az , usa ) rappresenta a tuttoggi lunico stent ricoperto disponibile sul mercato specificatamente progettato per la tips . 
un introduttore da 12 f deve essere avanzato nel sistema portale per almeno 3 c una volta avanzato lo stent al suo interno , fino allestremo distale , in porta , lintroduttore viene retratto delicatamente per permettere il corretto rilascio della porzione non rivestita allinterno della vena porta . va sottolineato che non possibile riposizionare il segmento scoperto della protesi in caso di rilascio non corretto . 
una volta confermato il corretto posizionamento della porzione non ricoperta allinterno della vena porta , lintroduttore viene retratto fino allestremo prossimale della protesi , in corrispondenza della giunzione tra vena epatica e vena cava inferiore , e , tenendo fermo il sistema , la porzione ricoperta viene rilasciata tirando lapposito filo . la protesi viene poi dilatata con il pallone per angioplastica utilizzato precedentemente per la dilatazione del tramite intraepetico . successivamente , viene effettuata una venografia per valutare il corretto funzionamento dello shunt . 
4a - d deployment of the viatorr stent graonce the introducer is advanced into the portal vein ( pv ) for at least 3 cm , the uncovered portion of the stent graft should be deployed by retrieving the introducer ( a )  . 
the device is gently retracted until resistance is felt , thus indicating that the proximal portion of the bare stent has reached the junction of the pv with the intrahepatic tract ( b )  . 
4a - d rilascio dello stent viatorr : una volta che lintroduttore stato avanzato nella vena porta , per almeno 3 cm , la parte non ricoperta dello stent pu essere rilasciata retraendo lintroduttore ( a )  . 
tutto il dispositivo viene retratto delicatamente fino a che non si avverte una resistenza , questa indica che la porzione prossimale del tratto non ricoperto dello stent ha raggiunto la giunzione tra vena porta e tratto intraepatico ( b )  . 
the outer surface of the tube is composed of a modified e - ptfe film that minimises transmural permeation of bile and mucin to inhibit hyperplastic tissue ingrowth and provide radial reinforcement to the inner surface . 
the inner blood - contacting surface is made of e - ptfe and has a microstructure and mechanical properties similar to vascular stent grafts manufactured with gore - tex . the viatorr presents a characteristic structural design composed of an uncovered portion 2 - cm in length for the portal region and an e - ptfe - covered portion for the intrahepatic tract , available in different diameters ( 8 , 10 , 12 mm ) and different lengths ( 48 mm )  . 
dopo la procedura , nei pazienti con parametri della coagulazione normali , per ridurre lincidenza di occlusione dello shunt viene prescritta una terapia anticoagulante con 12500 ui di eparina in 500 ml di soluzione fisiologica per le prime 24 ore e successivamente i pazienti vengono sottoposti a terapia antiagregions . 
the stent graft is mounted on a very low profile 10 fr device where the covered portion is secured with a constraining e - ptfe sleeve while the self - expandable uncovered part is secured with an introducer sleeve . stent - graft deployment deployment of the viatorr can be divided in two parts : 1 . 
the 12 - f introducer sheath should be advanced into the portal system for at least 3 cm and then gently retracted to permit release of the uncovered portion within the pv . 
all patients underwent postimplantation therapy with 12 , 500 ui of heparin diluted in 500 ml of saline for the first 24 h , and thereafter 0.5 mg of low - molecular - weight heparin are administered twice a day for at least 1 week . technical and periprocedural complications the most frequent complications that can occur during tips procedure are represented by [ 11 ] : neck haematoma for inadvertent carotid artery puncture ( 1% ) f . 
i fattori associati ad una prognosi negativa dopo il posizionamento della tips per sanguinamento di varici comprendono liponatremia , lencefalopatia , la cirrosi child c e una procedura urgente di tips per ascite refrattaria , comprendente littero e linsufficienza renale [ 17 ]  . 
le maggiori complicanze che possono accorrere pi frequentemente dopo la tips sono rappresentate dallencefalopatia epatica e dellinsufficienza dello shunt [ 17 ]  . encefalopatia epatica lencefalopatia epatica si manifesta nel 15%30% [ 18 , 19 ] dei pazienti dopo tips effettuata utilizzando stent non ricoperti , mentre con lutilizzo degli stent ricoperti tale incidenza arriva al 47% [ 20 ]  . 
sono stati identificati diversi fattori predittivi , inclusa una storia precedente di encefalopatia epatica , una patologia epatica non alcolica , let maggiore di 60 anni , il diametro dello shunt . 
unanalisi comparativa retrospettiva dei pazienti trattati con stent non ricoperti e dei pazienti trattati con viatorr , ha evidenziato una maggiore perviet a lungo termine dello stent ricoperto con ridotta iperplasia intimale , associata per ad una maggiore incidenza di encefalopatia ( 47 , 7% )  . insufficienza dello stent pneumothorax following too low a puncture site ( < 1% ) hepatic capsula laceration during pv puncture linsufficienza dello shunt pu essere secondaria a stenosi o ad occlusione dello stent dovuta ad iperplasia intimale con f . 
5 lo stent viatorr costituito da due porzioni differenti separate da un anello doro : una parte non ricoperta lunga 2 cm , per la porzione portale dello shunt e una parte ricoperta in e - ptfe per il tratto intraepatico . hepatic - artery puncture secondary to a too anterior direction of the needle ( 1% ) bile - duct puncture ( 10% ) extrahepatic puncture of the pv ( 2% ) thirty - day mortality rates after tips placement range from 3% to 44% , and 1 - year mortality rates range from 10% to 58% [ 17 ]  . 
factors associated with a poor prognosis after tips placement for variceal bleeding include hyponatremia , encephalopathy , childs class c cirrhosis , and urgent tips placement for refractory ascites , including jaundice and renal insufficiency [ 17 ]  . 
the two major complications that can occur more frequently after tips procedure are represented by he and shunt insufficiency [ 17 ]  . hepatic encephalopathy hepatic encephalopathy ( he ) is present in the 15%30% [ 18 , 19 ] of patients after tips performed with conventional bare stents ; using a covered stent , a higher incidence is generally reported ( 47% ) [ 20 ]  . 
in case of severe encephalopathy refractory to conventional medical therapy , a shunt reduction should be performed using a covered stent ( jostent , abbot vascular , rangendingen , germany ) released inside the viatorr with an hourglass shape . 
6 la riduzione della tips : in caso di encefalopatia , refrattaria alla comune terapia medica , necessario ricorrere alla riduzione dello shunt mediante lutilizzo di uno stent ricoperto ( jostent , abbot vascular , rangendingen , germany ) , opportunamente conformato a clessidra , da rilasciare allinterno del viatorr . 
dopo il rilascio dello stent si osserva un aumento immediato del psg con miglioramento delle condizioni cliniche . riduzione del lume dello shunt , che favorisce il ripristino dellipertensione portale ed il sanguinamento da varici . come riportato in letteratura , gli stent non ricoperti presentano una perviet primaria del 40%50% ad un anno e del 15%30% a due anni [ 6 , 21 , 22 ]  . 
tale problema pu richiedere ripetute revisioni della tips , che prolungano certamente la perviet dello shunt , ma incrementano notevolmente il costo della procedura , sottoponendo inoltre il paziente a maggiori complicanze . 
per superare questa importante complicanza , che aveva fatto ridurre il numero delle procedure per anno , molti autori hanno sperimentato lutilizzo di stent ricoperti fatti in casa , prima negli animali e poi nelluomo . 
molti materiali sono stati utilizzati per ricoprire lo stent , come il politetrafluoroetilene ( ptfe ) , il polietilene tereftalato ( pte , commercialemente conosciuto come dacron ) , e poliuretanolo ( pu )  . 
i risultati dei tentativi con dacron e pu non sono stati molto soddisfacenti per lalta incidenza di occlusione precoce , ma gli esperimenti eseguiti con il ptfe hanno evidenziato una alta percentuale di perviet primaria a 12 mesi [ 23 , 24 ]  . valutazione post - procedurale del paziente il successo della tips correlato alla perviet dello shunt . shunt insufficiency shunt insufficiency is secondary to stent stenosis or occlusion . 
this is due to the almost constant presence of progressive increase of pseudointimal hyperplasia , which causes reduction of the shunt lumen , thus favouring return of portal hypertension with recurrent variceal bleeding . 
as reported in the literature , using bare stents , primary patency rates are almost constant at approximately 40%50% at 1 year and 15%30% at 2 years [ 6 , 21 , 22 ]  . the problem can be partially resolved with repeated tips revisions , which certainly prolong stent patency , but they are very expensive and require extended patient compliance . 
various materials have been used to cover the stent , such as ptfe , polyethylene terephthalate ( pte , commercially known as dacron ) , and polyurethanol ( pu )  . 
results of attempts with dacron and pu were not very good because of the high incidence of early occlusions , but attempts made using ptfe were very promising , with a high primary patency rate at 12 months [ 23 , 24 ] postprocedure patient evaluation tips success is correlate with shunt patency . 
shunt function can be assessed by cdus , angiography with pressure measurement or spiral ct angiography ( cta ) [ 11 ]  . cdus is a noninvasive , inexpensive procedure that can be easily performed in intervals of 36 months , with sensitivity of 53%100% and specificity of 62%98% [ 6 , 22 ]  . 
however , this procedure is time consuming , difficult to perform and highly operator dependent [ 22 ]  . angiography with measurement of portal - venous pressure gradient represent the gold standard in the diagnosis of shunt failure . 
however , ionising radiation and relatively high doses of intravascular contrast media can represent a limitation of cta . our experience from january 2000 , 105 consecutive patients with a mean f . 
la funzionalit dello shunt pu essere valutata con eco - color doppler ( ecd ) , angiografia con misurazione della pressione o angio - tc spirale [ 11 ]  . 
lecd una metodica non invasiva , non costosa , che pu essere facilmente praticata con intervalli di 3 e 6 mesi , con una sensibilit del 53%100% e specificit del 62%98% [ 6 , 22 ]  . 
in un recente studio pubblicato da chopra [ 25 ] stata riportata una sensibilit di questa metodica del 97% , una specificit dell89% e unaccuratezza del 94% . tuttavia lutilizzo delle radiazioni ionizzanti e la relativa alta dose di mezzo di contrasto endovenoso possono rappresentare delle limitazione allutilizzo della tc durante il follow - up . la nostra esperienza da gennaio 2000 , 105 pazienti con unet media di 56 , 513 , 8 anni ( range 1675 anni ) sono stati trattati con uno stent viatorr . 
le indicazioni a tale trattamento erano sanguinamento ( n = 56 ) , asciti refrattarie ( n = 44 ) e sindrome budd - chiari ( n = 5 )  . limpianto dello stent viatorr ha avuto successo in tutti i pazienti , con una immediata rifuzione della psg da 23 , 36 , 5 mmhg ( range : 1342 mmhg ) a 7 , 133 , 1 mmhg ( range : 216 mmhg )  . in 4 pazienti ( 3 , 8% ) , un sanguinamento intra - addominale a seguito della puntura della vena porta stato immediatamente arrestato tramite rilascio dello stent . 
in un paziente trattato per sanguinamento delle varici , lo stent viatorr stato impiantato mediante puntura della vena porta sinistra . una settimana dopo limpianto si registrata una ostruzione del dotto biliare sinistro con aumento del livello di billirubina , per compressione causata dallo stent . i sintomi si sono risolti completamente dopo impianto di una endoprotesi biliare ; il paziente tuttavia deceduto dopo 19 mesi . 
three - dimensional ( 3d ) images obtained with maximum intensity projection ( mip ) and vr ( volume - rendering ) algorithms performed at 12 months follow - up showed complete patency of the stent graft , with no signs of intimal hyperplasia . 
 in four patients ( 3.8% ) , extrahepatic pv puncture with intraabdominal extravasation of contrast media was treated with the rapid deployment of the viatorr stent graft , with immediate arrest of intraabdominal bleeding . 
the patient was treated with implantation of a plastic biliary endoprosthesis , and symptoms resolved completely until the patients death 19 months later . after a mean follow - up of 23.89.3 ( range 150 ) months , 72 / 105 ( 68.6% ) patients were in good condition with a patent shunt ; 22 / 105 ( 20.9% ) had died from multiorgan failure while 11 / 105 ( 10.5% ) underwent orthotopic liver transplantation olt without procedural difficulties . 
twelve reinterventions were performed for implantation of too short a viatorr not completely covering the intraparenchymal tract ( n = 7 ) , pv stenosis ( n = 1 ) , hv stenosis ( n = 2 ) and increase of psg value with no evidence of shunt stenosis ( n = 2 )  . 
 the 1 - year primary patency rate was 83.8% , with a secpatency sufficienza sistemica , mentre 11 / 105 pazienti ( 10 , 5% ) sono stati sottoposti a trapianto di fegato senza complicazioni procedurali . 
nove dei 105 patients ( 8 , 6% ) sono stati sottoposti a reimpianto dello shunt a causa di malfunzionamento rilevato tramite ecd , endoscopia o evidenza clinica ( presenza di varici o asciti )  . 
in 7 pazienti stata necessaria una revisione , in un paziente sono state necessarie 2 revisioni e 3 revisioni in un ultimo paziente . dodici reinterventi sono stati effettuati a causa di impianti di stent viatorr troppo corti e non in grado di coprire completamente il tratto intraparenchimale ( n = 7 ) , stenosi della vena porta ( n = 1 ) , stenosi della vena epatica ( n = 2 ) e incremento del psg senza evidenza di stenosi dello shunt ( n = 2 )  . 
se , tuttavia , calcoliamo separatamente la percentuale di perviet per quei pazienti con uno stent della lunghezza adeguata otteniamo una perviet primaria ad 1 anno del 90 , 8% , mentre per il gruppo di pazienti con uno stent troppo corto la percentuale di perviet primaria era 79 , 5% . 
 encefalopatia nella nostra esperienza , durante un periodo di follow - up medio di 23 , 89 , 3 mesi , 49 / 105 pazienti ( 46 , 6% ) trattati con uno stent ptfe ( viatorr ) hanno sviluppato encefalopatia epatica . 
in 13 pazienti , lencefalopatia stata considerata di grado moderato ( grado iii ) e in 12 di grado severo ( grado iiiiv )  . dodici pazienti con encefalopatia sono stati ricoverati . ondary patency rate of 98.1%. 
if , however , we calculate separately the patency rate for those patients with a stent graft of the proper length , we obtain a 1 - year primary patency rate of 90.8% while in the group with too short a stent graft , the primary patency rate was only 79.5%. 
 encephalopathy in our experience , during a mean follow - up of 23.89.3 months , 49 / 105 patients ( 46.6 % ) treated with an e - ptfecovered stent graft ( viatorr ) developed he . 
however , statistical analysis showed no significant correlation between the incidence of encephalopathy , psg values and stent diameter ( ttest , p = 0.27 ; chi square test , p = 0.88 ; with identical values for logistic regression analysis )  . in 37 of 49 patients , encephalopathy was successfully treated medically with lactulose and dietary restriction . 
shunt reduction was required in the remaining 12 cases ( 24.4% ) of severe encephalopathy refractory to medical treatment after a mean period of 6.3 months ( range 6 days to 37 months )  . 
an immediate increase of psg value was observed in all cases , and up to the time of writing of this article , 8 / 12 patients ( 66.6% ) were alive and in good health while three had died . only in one case ( 8.3% ) was redilatation of the reduced shunt performed for rebleeding . orthotopic liver transplantation in our series , 11 patients ( 10.5% ) underwent olt without procedural difficulties . 
an initial belief that longer stents would cause difficulty during surgery was later discarded because the covered portion of the stent graft was not attached to the liver parenchyma and easily displaced for clamping . 
histopathologic analyses of explanted viatorrs showed patent stent grafts lined internally with a thin layer of fibrno signs of endothelialisation or intimal hyperplasia were observed in the covered portion of the viatorrs , and the stents were easily removed from the liver parenchyma . 
una riduzione dello shunt stata necessaria nei rimanenti 12 casi ( 24 , 4% ) che presentavano encefalopatia di grado severo refrattaria a terapia medica dopo 6 , 3 mesi ( range : 6 giorni37 mesi )  . 
in tutti i casi stato osservato un immediato incremento del valore del psg e , al momento in cui questo articolo stato redatto , 8 / 12 pazienti ( 66 , 6% ) erano vivi e in buone condizioni di salute , mentre 3 erano deceduti . 
solo in un caso ( 8 , 3% ) stata necessaria una ri - dilatazione dello shunt a causa di un nuovo episodio di sanguinamento . trapianto di fegato nella nostra casistica , 11 pazienti ( 10 , 5% ) sono stati sottoposti a trapianto di fegato senza complicazioni procedurali . contrariamente a quanto si era creduto inizialmente , gli stent lunghi non sono stati causa di complicazioni chirurgiche , perch la porzione ricoperta dello stent non era adesa al parenchima epatico e pertanto stata facilmente rimossa . lanalisi istopatologica ha mostrato la perviet degli stent viatorr espiantati che erano rivestiti internamente da un sottile strato di fibrina . non sono stati osservati segni di endotelializzazione o iperplasia intimale nella porzione ricoperta degli stent viatorr e gli stent sono stati facilmente rimossi dal parenchima epatico . 
la porzione di stent non ricoperta era invece strettamente adesa alla parete della vena porta e solo in un caso ( 9 , 1% ) risultata troppo lunga e , attraversando la linea di sezione della vena porta , ha complicato la procedura . mortalit a breve termine durante il periodo di follow - up , la mortalit a 30 giorni risultata del 3 , 8% ( 4 / 105 pazienti ) : un paziente deceduto per insufficienza cardiovascolare , uno per sindrome epato - renale e gli altri per insufficienza sistemica . mortalit a lungo termine escludendo gli 11 pazienti sottoposti a trapianto , abbiamo registrato una percentuale di sopravvivenza del 76 , 6% ( 38 / 94 ) e una mortalit del 23 , 4% ( 22 / 94 pazienti ) ad un periodo medio di follow - up di 23 , 82 mesi . 
 excluding the 11 patients who underwent transplantation , we had a survival rate of 76.6% ( 38 / 94 ) and a total mortality of 23.4% ( 22 / 94 patients ) , with a mean of 23.82 months of follow - up . la tips pu essere considerata una modalit particolarmente interessante per il trattamento dellipertensione portale , del sanguinamento da varici , dellascite refrattaria e conclusioni f . 
however , there are still unsolved problems , especially short primary patency of the shunt due to intimal hyperplasia , which causes reduction of the shunt lumen , thus favouring a return of portal hypertension with recurrent variceal bleeding . 
with the use of new ptfe - covered stents , we hope to prolong primary shunt patency and that tips will regain its lost popularity in the treatment of portal hypertension . 
further studies are necessary to compare these two imaging modalities . della sindrome di budd - chiari . sono stati praticati molti studi per valutare lefficacia e il rapporto costo - benificio di questa tecnica in relazione alle altre modalit terapeutiche . 
comunque rimangono ancora alcuni problemi irrisolti , soprattutto per quanto riguarda la breve perviet primaria dello shunt conseguente allo sviluppo delliperplasia intimale , che causa una riduzione del lume dello shunt , favorendo il ripristino dellipertensione portale . con lutilizzo dei nuovi stent ricoperti in ptfe noi auspichiamo di poter prolungare la perviet primaria dello shunt cosicch la tips possa incrementare la sua popolarit per il trattamento dellipertensione portale . lecd rimane la modalit di scelta per il follow - up dei pazienti con tips , mentre langio - tc spirale ritenuta vantaggiosa per la sua elevata sensibilit e specificit . 
an accessory finding devoid of pathological meaning in most cases , it can , however , be a possible cause of voiding disorders in some instances . key words urethra children cowpers ducts and glands riassunto obiettivo . 
due diaframmatiche e due bulbari o accessorie , le ghiandole di cowper sono piccole formazioni lobulate , di tipo tubulo - alveolare composto , disposte ai lati delluretra , tra i foglietti del diaframma urogenitale le prime ; nel corpo spongioso , lungo luretra bulbare g . 
le diaframmatiche ( di cui la destra prevalente sulla sinistra , spesso inesistente ) sono simili ad un pisello , con dimensione di circa 0 , 5 cm , maggiore rispetto a quello delle bulbari , pi piccole . 
i dotti escretori delle ghiandole diaframmatiche hanno lunghezza di circa 3 cm e diametro medio di 0 , 7 mm , attraversano la faccia inferiore del trigono urogenitale e sboccano sulla faccia inferiore delluretra bulbare , mentre quelli delle ghiandole bulbari o accessorie , sottili e brevi , sboccano direttamente nelluretra o si fondono con il dotto escretore principale del lato corrispondente . 
pu essere invece pi frequente in caso di stenosi uretrali o di problemi intrinseci ai dotti stessi che assumono laspetto di dilatazione cistica venendo cos descritti con il termine di siringocele [ 5 , 6 , 1316 ] anche se lo stesso termine non universalmente accettato e considerato causa di confusione [ lebowitz rl ( 2005 ) , cofig . 
diaphragmatic gland ducts are 3 - cm long , with an average diameter of 0.7 mthey run through the inferior side of the urogenital trigonum and open onto the inferior side of the bulbar urethra . 
5a , b dotto di cowper semplice a monte del collare di cobb : a durante la fase minzionale , b alluretrografia . as syringocele [ 5 , 6 , 1316 ] , a definition considered misleading by some authors [ lebowitz rl ( 2005 ) , personal communication ]  . 
lopacizzazione del dotto spesso rapida , transitoria ( per cui importante la ripresa delle immagini con spot - film a cadenza rapida ) e richiede una certa esperienza nella sua dimostrazione ed interpretazione . 
 il dotto di cowper appare come una sottile struttura allungata , a margini netti , parallela al margine inferiore delluretra membranosa / bulbare , che si dirige in senso cefalico risalendo fino al diaframma urogenitale . 
lack of opacification of the corresponding gland can be a source of diagnostic doubt [ 2 , 6 , 20 ]  . the real frequency of cowpers glands and ducts lesions is at present unknown since most of them are asymptomatic , with a reported rate of about 1.5% in paediatric vcu [ 25 ]  . autopsic studies have shown a 2.3% rate of occurrence in males in all age groups [ 26 , 28 ]  . 
a possible association with urethral valves has been reported [ 11 , 13 , 14 ]  . the term syringocele ( from the greek syrinx , tubular formation , and cele , swelling ) was first used by maizels in 1983 [ 13 ] to define the congenital or acquired dilatation of cowpers ducts . 
la reale incidenza delle lesioni dei dotti e delle ghiandole di cowper sconosciuta dal momento che la maggior parte delle stesse asintomatica con unincidenza variabile tra l1 , 5% in corso di esami cisto - uretrografici in et pediatrica [ 25 ] ed il 2 , 3% dei soggetti maschi in tutti i gruppi di et in casi autoptici [ 2628 ]  . 
in tali situazioni si potr avere non solo lopacizzazione del dotto , di calibro superiore a quanto osservabile in condizioni di normalit in funzione della componente ostruttiva , ma anche delle ghiandole . 
il termine siringocele ( da syrinx = formazione tubulare e cele = dilatazione ) stato coniato nel 1983 da maizels per definire la dilatazione , congenita od acquisita , del dotto di cowper [ 13 ]  . 
 [ 14 ] ne stata segnalata una frequenza dello 0 , 065% ( 14 casi in 21.384 pazienti adulti e bambini ) e dello 0 , 18% nella presente ( anche se basata su di una popolazione assai pi ridotta ) , mentre riportion of the duct imperforated or cystic syringocele : the duct orifice is closed causing dilatation of the distal duct , which appears as a filling defect or a mass that compresses the floor of the bulbar urethra , sometimes resulting in urethral stenosis and dilatation of its proximal portion perforated syringocele : the dilated distal duct looks like a diverticulum of the bulbar urethra into which the duct drains through a large opening ; opacification of cowpers glands is possible ruptured syringocele : the bulbar portion of the duct is dilated , like a cyst that has lost connection with its proximal portion ; radiologic images show thin filling defects in the radiolucent bulbar urethra due to remnants of the dilated duct transperineal ultrasound ( us ) in the sagittal and longitudinal scans show an anechoic double - channel tubular structure , the nearest to the probe representing the dilated cowpers duct , the more distal the urethra [ 21 , 22 ]  . 
the most important advantage of mri for patients consists of it being free of ionising radiation ; it is noninvasive and allows multiplanar imaging and precise evaluation of the relationship between the cyst and adjacent tissues and the ventral urethra [ 23 , 24 ]  . 
 [ 14 ] reported the finding in 0.065% of an adult and paediatric population ( 14 cases in 21 , 384 patients )  . this rare occurrence is in accordance with the 0.18% recorded in our population , even if smaller than the previous reports , while according to dewan , it can be found in 1.5% of children [ 25 ]  . 
a possible explanation of the higher percentage of cowpers syringocele in children than in adults may be the greater number of radiological procedures performed to exclude congenital malformations of the urinary tract or vesicoureteric reflux when recurrent urinary tract infections are present . 
considering these facts , it is not easy or even possible to establish clear - cut percentage differences amongst different types of syringocele according to different age groups . results during the past 24 years , 3 , 096 children ( 1 , 676 males , 1 , 420 females , age : newborn to 18 years ) were studied by vcu in our department of paediatric radiology . 
in six of them ( 0.35% ) , aged 6 months to 10 years and undergoing vcu for urinary tract infection , opacification of cowpers ducts appeared as a thin , clear - cut , radiopaque image running parallel to the inferior membranous / bulbar urethral edge . 
la possibile spiegazione del perch il riscontro del siringocele pi elevato nei bambini che nelladulto pu essere determinata dalla frequenza delle indagini eseguite per lesclusione di malformazioni congenite dellapparato urinario o di reflussi vescico - ureterali in caso di infezioni ricorrenti delle vie urinarie nei bambini , mentre nelladulto motivi dello studio sono cause traumatiche o post - infettive [ 2 , 7 ] e perci meno frequenti . 
in vista di ci non facile o possibile stabilire differenze percentuali tra le varie forme in funzione dellet . risultati in 24 anni di attivit della nostra sezione di radiologia pediatrica , sono stati sottoposti a cisto - uretrografia minzionale 3096 bambini ( 1676 maschi , 1420 femmine ; et neonatale18 anni ) per un totale di 4321 indagini di cui 2340 nei maschi e 1981 nelle femmine ed stata osservata in 9 soggetti ( 0 , 53% ) lopacizzazione del dotto di cowper . 
in 6 di questi ( 0 , 35% ) , di et variabile tra i 6 mesi ed i 10 anni , sottoposti ad indagine per infezione delle vie urinarie , si osservata opacizzazione del dotto sotto forma di sottile immagine radiopaca a margini netti , parallela al margine inferiore delluretra membranosa / bulbare . 
la visualizzazione , in proiezione obliqua o laterale , di una immagine canalicolare grossolanamente parallela alluretra , e labituale assenza di opacizzazione del corpo ghiandolare , possono rendere difficile lattribuzione della stessa al dotto della ghiandola di cowper . 
le principali diagnosi differenziali in caso di dubbio sono rappresentate da tragitti fistolosi uretrali , dai margini irregolari e con tendenza espansiva ; da spandimenti e stravasi di mezzo di contrasto ; da false immagini [ 6 ] , da duplicazioni e sovrapposizioni di immagini [ 2 , 14 ] nonch da diverticoli delluretra bulbare , di forma ovalare , dai contorni sottili e netti , ma g . 
one of the two other patients had been treated in the neonatal period due to the presence of posterior urethral valves : at the age of 4 years , he presented haematuria and urinary tract infection ; the second one was admitted at the age of 14 years , being affected by distal urethral stenosis . 
in utero si manifesta sotto forma di ostruzione transitoria o meno della vescica le cui pareti possono essere ispessite con associata idronefrosi quando lostruzione uretrale provocata da un dotto ostruito [ 28 ] ; nel neonato sono frequenti forme francamente ostruttive , con alterazioni del mitto , gocciolamento di urina , an incidental finding during urologic radiological procedures in children and adults , and such finding should not lead to incorrect diagnoses . 
a typical finding in the rare cases of duct opacification due to contrast reflux secondary to stenosis of the distal urethra is an image of the excretory duct and its corresponding glandular structure [ 6 ] , which is easily differentiated from the prostatic canal or from an abnormal course . 
syringocele can cause hydronephrosis in utero [ 28 ] ; in the newborn , there may be frank obstruction often followed by renal insufficiency , as is the case in the presence of posterior urethral valves [ 11 , 15 ]  . 
perforated and ruptured syringocele very often traumatic or postinfectious may rarely lead to dysuria due to local irritative phenomena , haematuria probably due to traumatic local lesions during micturition , posturinary incontinence and urinary tract infections due to bacterial colonisation of mucus and urine stagnating in the syringocele [ 15 16 , 19 , 28 ]  . 
treatment comprises symptomatic medical treatment and , in the case of obstructive syringoceles , endoscopic unroofing as first - choice option or open surgery [ 11 , 15 , 19 ]  . 
9 diverticolo delluretra bulbare in paziente sottoposto a ripetuti interventi di correzione di ipospadia di alto grado . globo vescicale , dilatazioni del tratto urinario superiore e , spesso , insufficienza renale : nel complesso , un quadro assimilabile a quello osservabile in presenza di valvole uretrali [ 11 , 15 ]  . 
nelle altre forme di siringocele , quasi sempre di natura traumatica o post - infiammatoria , sono possibili disuria , attribuibile a fenomeni irritativi locali , ematuria , presumibilmente secondaria a lesione traumatica della fragile parete del siringocele durante la minzione , infezioni urinarie , conseguenti a colonizzazione batterica di muco ed urina ristagnanti nel contesto del siringocele stesso [ 15 ] , piuria ed incontinenza urinaria post - minzionale [ 16 , 19 , 28 ]  . 
sonographic features of 256 histologically confirmed ( 148 benign , 108 malignant ) breast lesions were retrospectively and independently reviewed by three radiologists unaware of mammographic findings and pathology results . 
analysis of the sonographic features predictive of malignant disease , taken as a whole , showed that only irregular margins and marked hypoechogenicity maintain their predictive value independent of lesion size . 
i segni ecografici relativi a 256 lesioni mammarie con verifica istologica ( 148 benigne , 108 maligne ) , sono stati analizzati retrospettivamente e indipendentemente da tre radiologi , che non erano a conoscenza n della mammografia n dei risultati istologici relativi alla lesione in esame . 
i criteri normalmente utilizzati in ecografia a questo scopo presentato una accuratezza significativamente ridotta nella caratterizzazione delle lesioni di piccole dimensioni . parole chiave mammella ecografia segni ecografici carcinoma mammario c . 
with the recent advances in technology and standardisation of sonographic findings , breast us has improved significantly and is now used to characterise solid masses through analysis of their features [ 1 ]  . the remarkable technical improvements of us instrumentation compared with the machines used in the early studies on breast sonography have significantly increased sensitivity and specificity of this diagnostic tool [ 26 ]  . 
the current importance of breast us in characterising breast lesions has also been the result of standardisation of examination technique and evaluation of sonographic findings that may be useful in differentiating benign from malignant lesions . 
the authors compared sonographic findings of 750 solid breast lesions classified by the radiologist as benign , malignant or indeterminate with histological findings , and they analysed the frequency of each finding and its positive and negative predictive values . 
the reproducibility of their findings in routine clinical practice has since been evaluated by several authors [ 810 ] who considered the different us equipment , experience of sonographers and interobserver variability in the classification of findings to show how all these elements affect the final result . 
the purpose of this study was to retrospectively evaluate the accuracy of breast us alone in characterising solid lesions and identify sonographic features that may be predictive of benign or malignant disease . 
we also evaluated interobserver variability in classifying the lesions and the influence of lesion size on the above aspects . materials and methods selection of cases sonographic images of 256 consecutive solid breast lesions , which underwent us - guided core biopsy , were retrospectively examined . 
the reasons for biopsy were : breast imaging reporting and data systems ( birads ) 4 and 5 lesions , birads 2 and 3 lesions in patients with a previous history of breast carcinoma , strong family history of breast carcinoma or highly anxious patients . 
negli anni settanta ed ottanta questa tecnica era utilizzata esclusivamente allo scopo di differenziare le opacit a margini ben definiti , identificate alla mammografia , distinguendo le lesioni cistiche dalle lesioni solide . 
nei recenti anni passati , grazie agli avanzamenti nella tecnologia e alla standardizzazione dei segni ecografici , lecografia mammaria migliorata significativamente , essendo attualmente utilizzata anche nella caratterizzazione delle lesioni grazie allanalisi degli aspetti ecografici [ 1 ]  . i notevoli avanzamenti tecnici ottenuti negli anni recenti per quanto concerne le apparecchiature ecografiche , in confronto con gli ecografi utilizzati nei primi studi eseguiti mediante ecografia mammaria , ha permesso di ottenere un incremento significativo di sensibilit e specificit di questa metodica [ 26 ]  . 
nondimeno , il ruolo fondamentale recentemente ottenuto dallecografia mammaria nella caratterizzazione delle lesioni mammarie , stato ottenuto anche grazie alla standardizzazione dei metodi di esame e alla valutazione dei segni ecografici , che risultano utili nel differenziale le lesioni benigne dalle lesioni maligne . 
gli autori hanno comparato i segni ecografici relativi a 750 lesioni solide mammarie , che erano state classificate dai radiologi come maligne , benigne o indeterminate , correlandoli con listologia e analizzando la frequenza di ogni segno ecografico valutandone il valore predittivo positivo e negativo . 
 [ 7 ] , utilizzando il loro sistema di classificazione , hanno ottenuto valori di sensibilit , specificit , accuratezza , valore predittivo positivo e negativo rispettivamente 98 , 4% , 67 , 8% , 72 , 9% , 38% e 99 , 5% . 
nella routine clinica , considerando differenti apparecchiature , lesperienza degli ecografisti e la variabilit interosservatore nella classificazione dei segni ecografici , dimostrando come tutti questi elementi influenzino il risultato finale . per quanto a noi noto , linfluenza della dimensione delle lesioni nella valutazione di questi segni ecografici utili nella differenziazione tra lesioni benigne e maligne , non stata ancora valutata . 
lobiettivo di questo lavoro stato quello di valutare laccuratezza dellecografia mammaria nella caratterizzazione delle lesioni solide mammarie identificando i segni ecografici potenzialmente utili nella diagnosi di lesione benigna o maligna . 
surgical biopsy was performed in 2% of benign lesions because of patient anxiety or recommendation by the pathologist ; in these cases , the diagnosis of benign lesion was always confirmed . 
all other benign lesions were unchanged at follow - up after at least 24 months . evaluation of sonographic images three radiologists experienced in breast imaging ( 4 , 5 and 8 years of practice , respectively ) retrospectively and independently evaluated sonographic images of the 256 selected cases . 
the radiologists assessed each lesion for shape ( round , ellipsoid , irregular ) , margins ( regular , ill - defined , microlobulated , angular , spiculated , with fewer or more than three well - defined macrolobulations , branch pattern ) , texture ( homogeneous , heterogeneous ) , echogenicity ( mild or marked hypoechogenicity , hyperechogenicity , isoechogenicity , anechogenicity ) , posterior acoustic transmission ( increased , regular , reduced ) and presence or absence of lateral acoustic shadows , pseudocapsule and microcalcification . 
each radiologist expressed a degree of suspicion for each lesion : benign , probably benign , probably malignant and malignant . statistical analysis and study design association between lesion morphological features and histological diagnosis was evaluated using the chi - square test after combining some categories , if necessary . 
finally , we assessed the accuracy of breast us in characterising solid lesions by comparing the degree of radiological suspicion expressed by each reader and the final pathology report . results histological analysis demonstrated that 148 / 256 ( 58% ) lesions were benign and 108 / 256 ( 42% ) were malignant . 
benign lesions were classified as follows : 101 fibroadenomas ( 68% ) , 15 fibrocystic disease ( 10% ) and 32 different benign lesions ( 22% ) such as focal fibrosis , typical ductal hyperplasia , radial scar , sclerosing adenosis , granuloma , lipoma , hamartoma , benign phyllodes tumour , papilloma and adenografiche di 256 consecutive lesioni solide mammarie , sottoposte ad agobiopsia sotto guida ecografica . 
la biopsia chirurgica stata eseguita nel 2% delle lesioni benigne in seguito ad ansiet delle pazienti e a raccomandazione del patologo ; anche in questi casi la diagnosi preliminare dellagobiopsia stata confermata . 
tutte le altre lesioni benigne risultavano invariate al follow - up di ameno 24 mesi . valutazione delle immagini ecografiche tre radiologi , esperti in senologia ( rispettivamente con quattro , cinque e otto anni di esperienza ) , hanno valutato indipendentemente e retrospettivamente , le immagini ecografiche relative ai 256 casi selezionati . 
ogni radiologo ha descritto per ogni lesione la forma ( rotonda , ovalare , irregolare ) , i margini ( regolari , indefiniti , microlobulati , angolati , spiculati , con meno di tre o pi di tre macrolobulazioni , ramificati ) , la tessitura ( omogenea , disomogenea ) , lecogenicit ( ipoecogenicit moderata o marcata , iperecogenicit , isoecogenicit , anecogenicit ) , la trasmissione del segnale acustico posteriore ( aumentata , normale , ridotta ) , e la presenza o assenza delle ombre acustiche laterali , della pseudocapsula e delle microcalcificazioni . 
ogni radiologo ha poi espresso il grado di sospetto relativo ad ogni lesione , classificandole come benigne , probabilmente benigne , probabilmente maligne o maligne . analisi statistica e disegno dello studio lassociazione tra gli aspetti morfologici delle lesioni e la diagnosi istologica stata valutata mediante il test ( cid : 2 ) 2 , dopo aver combinato alcune categorie se ritenuto necessario . 
al fine di analizzare linfluenza della dimensione della lesione sui singoli segni , utili a predire la diagnosi istologica di benignit o malignit , per ogni singolo segno stata identificata la soglia al di sopra della quale esso risulti ancora in grado di esprimec . 
malignant lesions were classified as follows : 85 invasive ductal carcinomas ( 79% ) , eight invasive lobular carcinomas ( 7% ) , two in situ ductal carcinomas ( 2% ) and 13 different neoplastic lesions ( 12% ) such as invasive papillary carcinoma , invasive medullary carcinoma , invasive ductal - lobular carcinoma and mixed in situ invasive carcinoma . 
 the logistic model applied to the features as a whole yielded an odds ratio ( or ) = 2.34 [ 95% confidence interval ( ci ) ( 1.025.40 ) ] for marked hypoechogenicity and an or = 112.29 [ 95% ci ( 37.6334.71 ) ] for irregular margins . impact of lesion size the predictive value of each feature relative to lesion size is shown in table 3 . 
infine , abbiamo calcolato laccuratezza dellecografia mammaria nel caratterizzare le lesioni solide , comparando il sospetto radiologico di ogni lettore con la diagnosi istologica definitiva . risultati lanalisi istologica ha dimostrato che 148 / 256 ( 58% ) lesioni erano benigne , mentre 108 / 256 ( 42% ) lesioni erano maligne . 
le lesioni benigne sono state classificate come di seguito : 101 fibroadenomi ( 68% ) , 15 malattia fibro - cistica ( 10% ) , 32 differenti lesioni benigne ( 22% ) come fibrosi focale , iperplasia duttale tipica , radial scar , adenosi sclerosante , granuloma , lipoma , amartoma , tumore fillode benigno , papilloma , adenoma . 
le lesioni maligne sono state classificate come di seguito : 85 carcinoma duttale infiltrante ( 79% ) , 8 carcinoma lobulare infiltrante ( 7% ) , 2 carcinoma duttale in situ ( 2% ) , e 13 differenti lesioni neoplastiche maligne ( 12% ) quali carcinoma papillare infiltrante , carcinoma midollare infiltrante , carcinoma duttulo - lobulare infiltrante , carcinoma duttale misto invasivo e intraduttale . 
let delle pazienti risulta compresa tra i 18 e gli 88 anni ( et media 53 , 2 anni , mediana 51 anni )  . la dimensione massima delle lesioni risultava compresa tra i 3 ed i 100 mm ( mediana 13 , 79 mm , mediana 12 mm , ds 9 , 09 mm ) ; in particolare , la dimensione delle lesioni benigne era compresa tra i 4 e i 45 mm ( media 13 , 11 mm , mediana 12 mm , ds 6 , 88 mm ) , mentre la dimensione delle lesioni maligne era compresa tra i 3 e i 100 mm ( media 14 , 71 mm , mediana 13 mm , ds 11 , 42 mm )  . la distribuzione dei diversi aspetti ecografici tra lesioni benigne e maligne riportata nella tabella 1 ; peraltro , per lanalisi dei dati stato necessario combinare in categorie alcuni segni ecografici . 
in particolare i segni relativi ai margini sono stati raggruppati come di seguito : margini regolari , o con macrolobulazioni sono stati raggruppati nei margini regolari ; margini indefiniti , microlobulati , angolati , spiculati , ramificati sono stati raggruppati nei margini irregolari . analizzando i dati riportati in tabella 1 relativi alle lesioni benigne , si evince come i segni ecografici pi frequenti per ogni categoria siano la forma ovoidale ( 74 , 3% ) , i margini regolari ( 54 , 7% ) , la moderata ipoecogenicit ( 46 , 6% ) , la presenza di una pseudocapsula ( 67 , 6% ) , una normale trasmissione acustica posteriore ( 62 , 8% ) , e la presenza delle ombre acustiche laterali ( 55 , 4% )  . 
sullaltro versante , per le lesioni maligne , i segni ecografici pi frequenti per ogni categoria sono risultati essere la forma ( 45 , 4% ) , i margini microlobulati ( 43 , 5% ) , la marcata ipoecogenicit ( 75 , 9% ) , e la trasmissione acustica posteriore ridotta ( 53 , 7% )  . 
sia le lesioni benigne che maligne hanno presentato pi frequentemente una tessitura omogenea . il valore di ogni singolo segno , considerato singolarmente , nella predizione della diagnosi istologica di benignit o malignit stato riportato in tabella 2 . 
un assorbimento acustico posteriore , una tessitura disomogenea e la presenza di microcalcificazioni . il modello logistico applicato alla globalit dei segni ecografici ha dimostrato una odds ratio ( or ) = 2 , 34 ( 95% ci ipoecogenicit e una [ 1 , 025 , 40 ] ) per or = 112 , 29 ( 95% ci [ 37 , 67334 , 71 ] ) per i margini irregolari . la marcata influenza delle dimensioni sulla lesione il valore di ogni singolo segno nella predittivit della diagnosi istologica di benignit o malignit , in relazione alle dimensioni delle lesioni , riportato in tabella 3 . 
la presenza di una pseudocapsula risulta associata pi frequentemente con diagnosi di benignit solo per lesioni uguali o maggiori di 7 mconsiderando la trasmissione acustica posteriore normale come riferimento , un assorbimento acustico posteriore in grado di predire la diagnosi di malignit solo per lesioni maggiori o uguali ai 7 mm , mentre un rinforzo acustico posteriore diventa segno di benignit solo per lesioni solide maggiori di 30 mla presenza delle ombre acustiche laterali diventa segno di benignit per lesioni di almeno 6 mm di diametro , mentre una tessitura disomogenea risulta segno predittivo di malignit per lesioni con massimo diametro di almeno 7 mlanalisi relativa alla presenza di microcalcificazioni deve essere interpretata con cautela in relazione al ridotto numero di casi , dal momento che tale reperto risulta difficilmente identificato ecograficamente . 
the lesions measure 3 mm ( a ) and 4 mm ( b ) in diameter , and both present mild hypoechogenicity , ill - defined margins and regular posterior acoustic transmission . 
1a , b vengono messe a confronto le immagini di due lesioni mammarie , riscontrate in due differenti pazienti , del diametro rispettivamente di 3 ( a ) e 4 ( b ) mm , con caratteristiche semeiologiche simili . 
dopo agobiopsia percutanea , la lesione in aa risultata essere un carcinoma duttale infiltrante di grado 1 , mentre la lesione in bb una mastopatia fibrosocistica . with benign diagnoses for lesions equal to or greater than 7 mif we take regular posterior acoustic transmission as a reference , reduced transmission is able to predict malignancy for lesions equal to or larger than 7 mm whereas increased transmission becomes a sign of benign disease for lesions at least 30 mm in diameter . 
the presence of lateral acoustic shadows indicates benign disease in lesions at least 6 mm in size whereas heterogeneous texture indicates malignancy for lesions at least 7 mm in size . 
sensitivity , specificity and positive predictive , negative predictive and accuracy values for each reader and on the lesions as a whole and by size are shown in table 6 . 
these data became particularly interesting when we considered the readers ability to correctly classify the lesions into the four categories ( benign , probably benign , probably malignant and malignant )  . 
the results , shown in tables 7 and 8 , indicate a significantly larger number of lesions classified in the intermediate categories ( probably benign and probably malignant ) in concordanza interosservatore e accuratezza la concordanza interosservatore per quanto concerne il sospetto ecografico attribuito a ogni lesione , quando calcolata indipendentemente dalle dimensioni delle lesioni , risultata essere sempre buona o eccellente , secondo i criteri classificativi di landis e koch [ 11 ] , risultando compresa tra 0 , 71 e 0 , 83 , come dimostrato in tabella 4 . 
considerando invece due gruppi di lesioni con diametro massimo inferiore o uguale ai 7 mm e diametro massimo maggiore di 7 mm , la concordanza interosservatore ha dimostrato risultati sostanzialmente simili come dimostrato in tabella 5 . 
i valori di sensibilit , specificit , valore predittivo positivo e negativo e accuratezza per ogni singolo lettore considerati nella globalit o relativamente alle dimensioni sono riportati in tabella 6 . 
questi dati sono risultati interessanti quando abbiamo preso in considerazione la capacit del lettore in classificare correttamente le lesioni nelle quattro categorie ( benigne , probabilmente benigne , probabilmente maligne e maligne )  . 
 finally , the results of logistic analysis , interobserver agreement and accuracy of breast us show that a maximum diameter of 7 mm is the best threshold beyond which the sonographic features are able to express their predictive value . 
although breast us has not been demonstrated to be an alternative to mammography in breast cancer screening , it can be helpful for detecting a significant number of lesions missed at mammography in patients with dense breasts [ 12 , 13 ]  . differentiation between benign and malignant lesions , on the contrary , has never been considered an indication for breast gnificativamente pi numerose nel gruppo di lesioni con diametro inferiore o uguale ai 7 mm rispetto alle lesioni con diametro maggiore di 7 mal contrario , le lesioni con diametro massimo maggiore di 7 mm sono state classificate pi frequentemente nelle categorie benigne o maligne , con una riduzione della percentuale di lesioni classificate come indeterminate . infine , prendendo in considerazione i risultati dellanalisi logistica , la concordanza interosservatore e laccuratezza dellecografia mammaria , si evinto come la soglia dei 7 mm per il massimo diametro delle lesioni sia quella pi idonea , al di sopra della quale gli aspetti ecografici possano esprimere il loro valore predittivo . discussione lecografia mammaria , nel caso in cui venga eseguita con tecnica ottimizzata , rappresenta la tecnica ancillare pi utile in approfondimento alla mammografia . 
percutaneous biopsy of all solid lesions was therefore recommended in the past [ 1416 ] , with breast us being used to distinguish between solid and cystic lesions detected by mammography . in the 1990s , several studies appeared that demonstrated the ability of us to characterise breast lesions . 
the application of digital compound technology [ sono - computed tomography ( ct ) ] has improved contrast resolution and eliminated several artefacts typical of conventional sonography [ 4 , 5 ]  . sono - ct , for example , allows better definition of margins , pseudocapsule , galactophorous ducts and connective fibres [ 5 ]  . 
it also improves visualisation of low - contrast lesions and of the internal architecture of solid and cystic lesions [ 4 , 5 ]  . microcalcifications are better detected thanks to elimination of the clutter artefact [ 4 ]  . 
 the role of breast us in lesion characterisation has also alla mammografia nello screening del tumore della mammella , pu essere utile nellidentificazione di un numero significativo di lesioni non visualizzabili alla mammografia , in particolare nelle pazienti con seni densi mammograficamente [ 12 , 13 ]  . 
la differenziazione tra lesioni mammarie benigne e maligne , al contrario , per lungo tempo non stata considerata una corretta indicazione per lecografia mammaria , in relazione allampia sovrapposizione tra i vari aspetti e segni ecografici . 
pertanto , in passato , era raccomandata la biopsia percutanea di tutte le lesioni solide mammarie [ 1416 ] , mentre lecografia veniva utilizzata solo al fine di distinguere tra le lesioni identificate mammograficamente , quelle solide da quelle cistiche . 
questo risultato stato ottenuto soprattutto grazie agli avanzamenti tecnologici , allutilizzo di sonde ad ampio spettro , di algoritmi compound , e alla standardizzazione della metodologia ecografica e degli aspetti semeiologici . 
lapplicazione dellalgoritmo compound digitale ( sono - ct ) ha permesso di ottenere un incremento della risoluzione spaziale , eliminando diversi artefatti tipici della ecografia convenzionale [ 4 , 5 ]  . 
essa consente per esempio di ottenere una miglior definizione dei margini delle lesioni , della pseudocapsula , dei dotti galattofori e delle fibre connettivali [ 5 ]  . inoltre risultano meglio visualizzabili le lesioni a basso contrasto , nonch larchitettura interna delle lesioni sia solide che cistiche [ 4 , 5 ]  . 
infine le microcalcificazioni , quando evidenziabili , risultano meglio visibili grazie alleliminazione dellartefatto clutter [ 4 ]  . il ruolo dellecografia mammaria nella caratterizzazione delle lesioni quindi cresciuto nel corso del tempo anche grazie alla chiara identificazione di alcuni segni semeiologici , come riportato da stavros et al . 
successivamente , correlando la classificazione ecografica con i risultati istologici , hanno calcolato dei valori di sensibilit , specificit , valore predittivo positivo e negativo , e accuratezza rispettivamente 98 , 4% , 67 , 8% , 38% , 99 , 5% e 72 , 9% . 
i margini spiculati , angolati o microlobulati , la presenza di microcalcificazioni , la marcata ipoecogenicit , lassorbimento acustico posteriore , la crescita verticale , lestensione intraduttale e laspetto ramificato sono stati considerati segni predittivi di malignit . 
lassenza dei segni predittivi di malignit , la marcata iperecogenicit , la forma ovalare , la presenza di macrolobulazioni ben circoscritte e la presenza di pseudocapsula , sono stati considerati segni predittivi di benignit . 
spiculated , angular or microlobulated margins , microcalcifications , marked hypoechogenicity , shadowing , vertical growth , intraductal extension and branch pattern were considered predictive of malignancy ; the absence of malignant findings , marked hyperechogenicity , ellipsoid shape , presence of wellcircumscribed macrolobulations and presence of a pseudocapsule were considered predictive features for benign lesions ; indeterminate features were lesion size , isoechogenicity , mild hypoechogenicity , regular or increased posterior acoustic transmission and texture ( homogeneous or heterogeneous )  . 
 [ 7 ] was followed by several other papers analysing the same [ 9 ] or largely similar [ 8 , 19 , diverse pubblicazioni su simili argomenti sono seguite al lavoro di stavros et al . 
 [ 7 ] , che hanno preso in considerazione gli stessi segni ecografici [ 9 ] o comunque in gran parte simili [ 8 , 19 , 20 ] ottenendo analoghi risultati [ 8 , 9 , 19 , 20 ]  . 
inoltre , gli autori hanno cercato di quantizzare la capacit di questi segni ecografici nel caratterizzare le lesioni , analizzando la frequenza di presentazione di ogni singolo segno e valutando la variabilit interosservatore relativa a ciascuno di essi . 
 [ 8 ] hanno dimostrato come il segno pi predittivo di benignit , presente frequentemente e affetto da bassa variabilit interosservatore , siano i margini regolari o macrolobulari , nonch la morfologia rotondeggiante o ovalare . 
 [ 9 ] hanno messo in evidenza come la morfologia delle lesioni sia il segno con la maggior concordanza interosservatore , mentre al contrario la presenza della pseudocapsula presenti la pi bassa concordanza interosservatore , rimanendo comunque bassa o modesta anche la concordanza per quanto concerne i margini , lecogenicit e la trasmissione c . 
 [ 8 ] demonstrated that the most predictive findings for benign lesions , with high frequency and low interobserver variability , were regular or macrolobulated margins and round or ellipsoid shape . 
 [ 9 ] identified shape as the finding with the highest interobserver agreement whereas the presence of a pseudocapsule had the lowest interobserver agreement ; interobserver agreement for margins , echogenicity and posterior acoustic transmission was always low or moderate . 
sonographic findings that were found to be most frequent and most strongly predictive of malignant lesions ( or risk factors ) were irregular shape , microlobulated margins , marked hypoechogenicity and reduced posterior acoustic emission . 
the most frequent and most predictive findings for benign lesions ( or protective factors ) were ellipsoid shape , regular margins , presence of a pseudocapsule , regular posterior acoustic transmission and lateral acoustic shadows . 
the only differences between our results and those reported in the literature concern mild hypoechogenicity and regular or increased posterior acoustic transmission , which we classify as protective factors , and heterogeneous texture , which we classify as a risk factor ; these features were not considacustica posteriore . per quanto a noi noto , fino ad oggi , non stata presa in considerazione linfluenza delle dimensioni delle lesioni , sulla frequenza o sul valore predittivo dei diversi segni ecografici presi in esame . 
i segni ecografici che sono risultati essere pi predittivi di malignit ( o cosidetti fattori di rischio ) e pi frequenti , sono la morfologia irregolare , i margini microlobulati , la marcata ipoecogenicit , e lassorbimento acustico ; mentre i segni ecografici che sono risultati essere pi predittivi di benignit ( o fattori protettivi ) nonch pi frequenti , sono la morfologia ovalare , i margini regolari , la presenza di una pseudocapsula , la trasmissione acustica posteriore e la presenza di ombre acustiche laterali . 
lunica differenza tra i nostri risultati e quelli riportati in letteratura , concerne la moderata ipoecogenicit e la trasmissione acustica posteriore regolare o aumentata , che per noi risultano essere fattori protettivi e la tessitura disomogenea , che noi classifichiamo con fattore di rischio ; questi segni in realt non sono stati considerati utili per una caratterizzazione dagli autori precedenti [ 79 ]  . nondimeno , dai nostri dati emerge come correlando questi segni con le dimensioni delle lesioni , il loro valore predittivo diminuisce progressivamente , proporzionalmente alla riduzione del massimo diametro delle lesioni . 
siamo stati quindi in grado di identificare dei valori soglia relativi alle dimensioni , per ogni singolo segno , al di sotto dei quali , esso non risulta pi predittivo . 
other findings , such as the presence of pseudocapsule and lateral acoustic shadows , were instead found to be protective factors only for lesions equal to or larger than 7 mm and 6 mm , respectively , whereas findings such as round or irregular shape , decreased posterior acoustic transmission and heterogeneous texture were risk factors only for lesions equal to or larger than 7 mm , and marked hypoechogenicity for lesions equal to or larger than 11 mm . these results indicate that the distribution of sonographic findings among small lesions , whether benign or malignant , is more homogeneous , making their characterisation more difficult . 
there is a significant difference in the frequency of each finding in lesions larger or smaller than 7 mm , whether benign or malignant , and this was particularly true for shape , echogenicity and texture . 
in detail , the percentage of lesions classified in the more indeterminate , central categories ( probably benign and probably malignant ) is significantly higher for lesions equal to or smaller than 7 mm compared with those larger than 7 mm . consequently , the percentage of lesions correctly classified as benign or malignant was significantly higher for lesions larger than 7 mm compared with smaller ones ( 63% and 73% compared with 44.8% and 48% , respectively )  . 
in conclusion , while confirming the potential of breast us in characterising solid breast lesions , thanks to the definition of features predictive of benign or malignant lesions , our results revealed that the method suffers limitations in characterising small lesions . 
therefore , even in the absence of suspicious findings , solid lesions smaller than 7 mm should be monitored with short - term follow - up or be subjected to percutaneous biopsy ( fine - needle aspiration or core needle biopsy )  . acustiche laterali sono risultati essere predittivi di benignit solo per lesioni con diametro massimo maggiore o uguale rispettivamente a 7 e 6 mm , mentre la morfologia tondeggiante o irregolare , lassorbimento acustico posteriore , la tessitura disomogenea sono risultati essere predittivi di malignit solo per lesioni con diametro massimo maggiore o uguale a 7 mm , mentre la marcata ipoecogenicit solo per lesioni con diametro massimo maggiore o uguale a 11 m questi risultati mettono in evidenza come la distribuzione dei segni ecografici nelle lesioni di piccole dimensioni , sia pi omogenea , sia nelle lesioni benigne che in quelle maligne , rendendone pi difficoltosa la caratterizzazione . 
infatti abbiamo dimostrato come vi sia una significativa differenza di frequenza dei diversi segni ecografici sia nelle lesioni benigne che nelle lesioni maligne , per diametri maggiori o inferiori / uguali ai 7 mm , in particolare per quanto concerne la morfologia , lecogenicit e la tessitura . 
in particolare , la percentuale delle lesioni classificate nelle due categorie centrali pi indeterminate ( probabilmente benigne e probabilmente maligne ) significativamente maggiore per lesioni inferiori o uguali a 7 mm rispetto alle lesioni maggiori di 7 mconseguentemente , la percentuale di lesioni classificate correttamente nelle due categorie benigna e maligna risultata significativamente maggiore nelle lesioni con diametro maggiore ai 7 mm rispetto alle lesioni pi piccole ( 63% e 73% rispetto a 44 , 8% e 48% )  . 
la sua brillante intelligenza e il suo interesse per la medicina e le scienze matematiche gli hanno consentito di conseguire con il massimo dei voti , presso luniversit cattolica di roma , una laurea in medicina e chirurgia e tre specializzazioni in radiologia diagnostica , radioterapia ed oncologia . il suo cruccio fu quello di non potersi laureare in scienze matematiche , ma gi gli argomenti della sua tesi di laurea e di specializzazione in radiologia ( langiografia digitale : sviluppo di una classica metodica e nuove prospettive offerte dalluso del computer ; considerazioni dosimetriche in angiografia digitale ) dimostrano la sua propensione ad affrontare e comprendere immediatamente argomenti che avessero a che fare con numeri . io ho avuto lonore di collaborare , durante la sua formazione sia alluniversit che alla scuola di specializzazione , con un professionista geniale e nello stesso tempo semplice come tutti i grandi . 
ferrero di cambiano 17 , i - 10024 moncalieri ( to ) , italy , tel . : + 39 - 011 - 6615506 , e - mail : ago.depascale@libero.it received : 10 march 2006 / accepted : 7 april 2006 / published online : 11 august 2006 abstract purpose . 
computed tomography ( ct ) is of great value in the evaluation of the mediastinum , which is frequently involved by the disease , but carries a high radiation load . 
x - ray proved to be superior in hilar adenopathies only . us provides qualitative information ( hypoechoic or hyperechoic tissues ) in addition to quantitative data ( maximum diameter of each lymph node ) it shares with ct . 
compared with x - ray , us allows for a better evaluation of the anterior mediastinal regions , showing small , central adenopathies that do not alter the mediastinal lines on x - ray . it is , however , of very limited value in the evaluation of posterior compartments because of their deep location . 
us may have a specific role in monitoring patients with mediastinal adenopathies , providing early indications on possible response to treatment and allowing the frequency of ct follow - up scans to be reduced . 
il mediastino , frequentemente coinvolto dalla patologia , studiabile in modo ottimale con la tc , indagine che utilizza dosi importanti di radiazioni ionizzanti : alcuni autori hanno pertanto proposto di avvalersi anche dellecotomografia per valutare la risposta al trattamento gi dalle prime settimane , in virt dei peculiari vantaggi dellesame , caratterizzato da buona compliance e assenza di rischi per il paziente , bassi costi , agevole ripetibilit , immagini dinamiche che permettono valutazioni multiplanari , criteri qualitativi oltre che quantitativi . 
nel corso del 2005 , in 12 pazienti stato monitorato , in momenti successivi , il coinvolgimento mediastinico mediante radiografia standard del torace in due proiezioni , ecotomografia mediastinica e tc spirale con mdc ( gold standard )  . 
rispetto alla radiografia , lo studio ultrasonografico consente di valutare meglio le regioni del mediastino anteriore , evidenziando adenopatie piccole e centrali , che non modificano le linee mediastiniche sul radiogramma ; le regioni posteriori sono invece scarsamente valutabili a causa della loro maggiore a . 
lecotomografia pu rivestire un ruolo specifico durante il trattamento di pazienti con adenopatie mediastiniche , fornendo indicazioni precoci sul trend di risposta e consentendo di ridurre e distanziare nel tempo i controlli tc , e diventare cos complementare alla stessa tc , pur non potendo sostituirla ( la tc deve infatti continuare ad essere considerata la tecnica gold standard )  . parole chiave linfoma ecotomografia mediastino introduction introduzione lymphomas refer to a wide range of multicentric , solid malignancies of the lymphatic system , which at the thoracic level occur almost exclusively in the mediastinum [ 1 , 2 ]  . 
the mediastinum has been traditionally studied by using different imaging techniques , each of which has a different indication in diagnosis , treatment and follow - up [ 3 ]  . 
at present , the most commonly used diagnostic modalities are standard chest x - ray a firstline examination characterised by a large number of false negatives that does not provide a detailed description of mediastinal masses and computed tomography ( ct ) [ 35 ]  . 
although permitting accurate morphostructural and topographic evaluation in this complex anatomical region , ct involves high exposure to ionising radiation and requires the use of iodinated contrast material , with possible adverse reactions [ 3 , 4 , 6 ]  . 
nuclear imaging provides other very useful diagnostic tools , in particular positron - emission tomography ( pet ) - ct , which combines functional information and precise topographic and morphostructural localisation of the lesion [ 4 , 7 , 8 ]  . 
however , similarly to magnetic resonance imaging ( mri ) ( in which diagnostic detail is nearly identical to ct without the disadvantages ) , this technique is not widely used because of its limited availability [ 4 , 6 , 9 ]  . it has been suggested that these modalities should be integrated with ultrasonography ( us ) , a technique characterised by good compliance , absence of patient risks , low cost , easy reproducibility , multiplanar images and qualitative and quantitative lesion assessment [ 1021 ]  . 
though recognising that the anatomical characteristics of the mediastinum impair penetration of the us beam into all mediastinal districts i linfomi , ampia gamma di neoplasie maligne solide multicentriche del sistema linfatico , a livello toracico si sviluppano quasi esclusivamente nel contesto del mediastino [ 1 , 2 ]  . per la corretta gestione clinica di questi pazienti , spesso giovani , che necessitano di trattamenti articolati , emerge la fondamentale importanza della diagnostica radiologica , il cui impatto non trascurabile si associa agli importanti effetti tossici che gravano le terapie . 
lo studio del mediastino si avvale tradizionalmente di diverse tecniche di imaging , che trovano differente indicazione nel decorso della malattia : in corso di diagnosi , durante il trattamento , nel follow - up successivo [ 3 ]  . 
attualmente le metodiche di diagnostica per immagini pi utilizzate sono la radiografia standard , esame di prima istanza , ma caratterizzato da un elevato numerosi di falsi negativi e che non permette una descrizione dettagliata delle masse mediastiniche , e la tc [ 35 ]  . 
questultima consente unaccurata valutazione morfostrutturale e topografica in un distretto anatomico complesso , ma gravata da unimportante esposizione a radiazioni ionizzanti , oltre a prevedere lutilizzo di mezzo di contrasto organoiodato , non scevro dal rischio di reazioni avverse [ 3 , 4 , 6 ]  . 
di grande ausilio diagnostico sono sicuramente le indagini medico - nucleari , e tra queste in particolare offre notevoli potenzialit di impiego la pet - tc , che associa informazioni di carattere funzionale ad altre di precisa collocazione topografica e morfostrutturali della patologia [ 4 , 7 , 8 ]  . 
tuttavia tale ultima indagine , cos come la rm ( metodica in grado di fornire dettagli diagnostici quasi sovrapponibili alla tc in assenza degli inconvenienti sopramenzionati ) non diffusamente impiegata per la minore disponibilit sul territorio [ 4 , 6 , 9 ]  . alcuni autori hanno suggerito di affiancare alle precedenti metodiche lecotomografia , indagine caratterizzata da a . 
pur riconoscendo le importanti implicazioni negative dovute alle caratteristiche anatomiche del mediastino , che non consente la progressione del fascio ultrasonoro in tutti i distretti e quindi una valutazione diagnostica completa , lo scopo del nostro lavoro rilevare il possibile ruolo di tale metodica come esame integrativo nello studio della risposta al trattamento in corso di terapia di pazienti con localizzazione mediastinica di linfoma . materiali e metodi presso il servizio di ecotomografia della scdu di radiologia dellospedale s . 
luigi di orbassano ( to ) , nel corso del 2005 , sono stati esaminati 12 pazienti , 4 donne e 8 uomini , di et compresa tra 17 e 68 anni , con localizzazione mediastiniche di linfoma ( 4 linfomi di hodgkin , lh , e 8 linfomi nonhodgkin , lnh ) , diagnosi sempre formulata in base allesame istologico seguito da stadiazione mediante tc . 
ogni paziente stato valutato in quattro momenti successivi ( tabella 1 ) , per un totale di 44 esami ecotomografici : prima dellinizio della chemioterapia ; alla fine del primo ciclo di trattamento , quando dovrebbero essere evidenziabili i primi effetti terapeutici ; al termine del quarto ciclo di chemioterapia ( 8 pazienti ) o subito prima dellautotrapianto ( 4 pazienti ) , a seconda dello schema di trattamento impostato ; al termine dellintero percorso terapeutico . 
 solo 10 pazienti sono giunti a completare il follow - up , in and consequently hinder a thorough diagnostic evaluation , we carried out this study to assess the possible role of us as a complementary modality to evaluate response to treatment in patients with mediastinal lymphomas . 
 materials and methods in 2005 , we studied 12 patients ( four women , eight men ; age range : 1768 years ) with mediastinal lymphoma [ four hodgkins lymphomas ( hl ) and eight non - hodgkins lymphomas ( nhl ) ] at the department of ultrasonography of the s.c.d.u. 
each patient was studied on four different occasions ( table 1 ) , for a total of 44 us examinations : before initiating chemotherapy ; after the first treatment cycle ( when the first therapeutic effects should be visible ) ; after the fourth chemotherapy cycle ( eight patients ) or just before autologous transplantation ( four patients ) , depending on the treatment regimen ; and on completion of treatment . 
in the majority of cases , 3040 days elapsed between the first and second follow - up examination , 35 months between the second and third and 12 months between the third and fourth . 
for two patients whose treatment regimen involved longer intervals between cycles , the followup period was longer ( approximately 2 months between the first and second follow - up , 67 months between the second and third and approximately 3 months between the third and fourth )  . 
the radiologist systematically explored the mediastinal regions in search of disease locations and accurately determined size , morphology and structure of each adenopathy , which was then classified based on location . 
us examinations were performed on a sonoline elegra siemens device using 3.5 - mhz convex , 7.5to 10 - mhz linear and 6.5 - mhz sector transducers following the approaches outlined by wernecke et al . 
in the suprasternal approach , the patient lies supine with a cushion under the shoulders to enable full extension of the head ; the transducer is placed in the jugular fossa , and scans are made in the coronal , sagittal and semisagittal planes , providing easy exploration of the aortopulmonary window and supraaortic and paratracheal regions . 
in the parasternal approach , the patient lies in the right and left lateral position ; the transducer is placed in the intercostal spaces , and scans are made in the quanto 2 sono deceduti durante il periodo di osservazione . nella maggior parte dei casi , tra il primo ed il secondo controllo sono intercorsi 3040 giorni , 35 mesi tra il secondo ed il terzo , 12 mesi tra il terzo e lultimo . 
per 2 pazienti , invece , per i quali era stato scelto uno schema di terapia con cicli pi distanti nel tempo , il periodo di follow - up stato pi lungo ( circa 2 mesi tra il primo ed il secondo controllo , 67 mesi tra il secondo ed il terzo e circa 3 mesi tra il terzo e lultimo )  . 
ad ogni controllo , in pochi giorni i pazienti sono stati tutti sottoposti a radiografia standard del torace in proiezione pa e ll , a tc spirale in corso di somministrazione di m.d.c. 
organoiodato ( pitch 1 , 5 , spessore di strato 5 , 5 mm , ritardo di acquisizione delle immagini 3035 s , ricostruzioni ogni 5 scansioni ) e ad ecotomografia mediastinica . gli esami ecotomografici sono stati eseguiti tutti dallo stesso radiologo , non a conoscenza dellesito delle altre due indagini , che ha proceduto ad una sistematica esplorazione delle regioni mediastiniche , alla ricerca di localizzazioni della malattia di base , ed ad unaccurata misurazione dimensionale e valutazione morfostrutturale di ogni adenopatia riscontrata , classificata poi in base alla sede . 
il materiale iconografico rx e tc raccolto per ogni paziente stato poi attentamente rivalutato da due radiologi operanti presso i servizi di radiologia convenzionale e di tc : questi dati sono stati quindi confrontati con quelli preventivamente riscontrati in corso di ecotomografia . 
sono state infine calcolate con metodo statistico le correlazioni diagnostiche di radiologia convenzionale ed ecotomografia rispetto alla tc quale indagine di riferimento ( gold - standard )  . lindagine ecotomografica stata eseguita con attrezzatura sonoline elegra siemens , utilizzando le sonde convex 3 , 5 mhz , lineare 7 , 510 mhz , settoriale 6 , 5 mhz , seguendo gli approcci descritti da wernecke et al . 
per lapproccio sovrasternale , il paziente in posizione supina con un cuscino sotto le spalle per favorire liperestensione del capo ; ponendo la sonda a livello della fossa giugulare , con scansioni lungo i piani coronali , sagittali e semisagittali , sono agevolmente esplorabili la finestra aorto - polmonare e le regioni sovraaortica e paratracheale . 
per lesplorazione parasternale , invece , il paziente deve assumere il decubito laterale , destro e sinistro ; ponendo la sonda a livello degli spazi intercostali , attraverso la nuova finestra acustica che si crea al di sotto dello sterno , con scansioni lungo il piano sagittale e altri pi o meno prossimi al trasversale , si valutano le regioni prevascolare e subcarinale ed il mediastino posteriore . 
prevascular and subcarinal regions are evaluated together with the posterior mediastinum through the acoustic window just beneath the sternumediastinal exploration is easier if the breath is held during forced expiration , as the width of the window changes with respiration . 
us yielded 38 / 41 true positives ( tp ) , 3 / 3 true negatives ( tn ) and three false negatives ( fn ) ; standard radiography yielded 27 / 41 tp , 3 / 3 linfoadenopatie in 41 / 44 casi ( tabella 2 )  . 
con gli ultrasuoni rilevabile una maggior frequenza di esami veri positivi ( vp ) e veri negativi ( vn ) nelle regioni sovraaortica ( vp 28 / 29 e vn 15 / 15 ) , prevascolare ( vp 30 / 31 e vn 13 / 13 ) , paratracheale ( vp 26 / 30 e vn 14 / 14 ) e nella finestra aortopolmonare ( vp 12 / 15 e vn 29 / 29 ) , rispetto allesame radiografico che presenta un numero maggiore di falsi negativi ( fn ) nelle regioni sovraaortica ( 13 / 29 ) , prevascolare ( 19 / 31 ) , nella finestra aortopolmonare ( 15 / 15 ) e nella regione subcarinale ( 19 / 19 )  . 
per quanto riguarda lo studio ultrasonografico delle localizzazioni pi profonde , si osservato 1 / 19 vp per la regione subcarinale e 41 / 41 vn per il mediastino posteriore ; lesame radiografico ha evidenziato 19 / 19 e 3 / 3 fn rispettivamente . i maggiori valori di sensibilit e accuratezza diagnostica ( tabella 5 ) sono stati osservati per lecotomografia a carico delle regioni sovraaortica ( 97% e 98% rispettivamente ) , prevascolare ( 97% e 98% ) , paratracheale ( 87% e 91% ) e della finestra aortopolmonare ( 80% e 93% ) , superiori a quelli calcolati per lesame radiografico . le adenopatie mediastiniche evidenziate sono risultate ipoecogene in 92 / 97 ( 95% ) casi . 
negli altri 5 casi ( 5% ) , invece , lecotomografia mostrava , a livello del mediastino anteriore ( in 2 casi a carico della regione paratracheale ed in 3 della regione prevascolare ) , formazioni solide ad ecogenicit aumentata rispetto ai controlli precedenti e con scarsa delimitazione di vere e proprie lesioni adenopatiche . 
subcarinale mediastino posteriore totale regions supraaortic region , % prevascular region , % paratracheal region , % aortopulmonary window , % 80 subcarinal window , % posterior mediastinum , % total , % regioni r . 
thus , sensitivity and diagnostic accuracy ( da ) of us were both 93% compared with 66% and 68% , respectively , for standard x - ray ( table 3 )  . 
results shown in table 2 were subsequently classified according to due pazienti presentavano un habitus costituzionale sfavorevole allesplorazione ecotomografica : il primo per una conformazione dello stretto toracico superiore priva di adeguate finestre acustiche ultrasonografiche , il secondo per a . 
in tutti gli esami eseguiti stata utilizzata la funzione thi ( tissue harmonic imaging ) , che ha favorito la corretta valutazione delle regioni anatomiche pi superficiali ; lattenuazione del fascio ultrasonoro ha penalizzato lievemente lesplorazione di distretti pi profondi . 
il colordoppler stato di ausilio solo in alcuni casi , per gli inevitabili artefatti legati alla pulsazione vigorosa dei grossi vasi arteriosi . discussione la metodica ecotomografica tradizionalmente considerata non idoneo allo studio del distretto toraco - mediastinico , territorio senza dubbio ostico per lesplorazione con gli ultrasuoni a causa delle numerose strutture anatomiche che ne limitano la progressione . 
tuttavia , grazie allimportante progresso tecnologico , con la commercializzazione di attrezzature pi sofisticate dotate di sonde sempre pi adatte alla valutazione di compartimenti anatomici con finestre acustiche limitate , e al crescente interesse manifestato dallambiente radiologico , negli ultimi anni si assistito ad un ampliamento nellutilizzo della metodica , che sta progressivamente acquisendo un ruolo importante nello studio di patologie del cavo pleurico , del parenchima polmonare , della parete toracica , del diaframma [ 10 , 21 ]  . la letteratura pi comunemente reperibile riporta studi che confrontano lecotomografia unicamente con la radiografia tradizionale e la tc . 
il nostro studio , condotto su una popolazione di pazienti affetti da lh e lnh con localizzazione mediastinica , ha evidenziato il positivo ruolo dellecotomografia come indagine di monitoraggio , e si affianca ad altri eseguiti in passato su pazienti affetti da differenti tipi di tumori mediastinici ; come nel lavoro di wernecke et al . 
 ( 1990 ) [ 12 ] , sono state stimate sensibilit e specificit dellecotomografia e della radiografia standard del torace in ogni regione in cui stato suddiviso il mediastino , assumendo la tc quale esame di riferimento ( gold standard )  . 
dai risultati da noi ottenuti , sensibilit e specificit dellecotomografia ( 93% e 100% ) sono nettamente superiori rispetto alla radiografia ( 66% e 100% ) come mostrato in tabella 3 . 
confluenza delle vene anonime nella vena cava superiore : importanza del color - doppler nel riconoscimento dei vasi mediastinici ( c )  . anatomical region ( table 4 )  . 
by contrast , x - ray had more fn results ( fn ) in the supraaortic ( 13 / 29 ) and prevascular ( 19 / 31 ) regions , in the aortopulmonary window ( 15 / 15 ) and in the subcarinal rea . 
scansione sovrasternale : arco aortico e tessuto iperecogeno ( di verosimile natura fibrosa ) a carico della finestra aortopolmonare ( c )  . gion ( 19 / 19 )  . 
us of deeper mediastinal masses produced 1 / 19 tp in the subcarinal region and 41 / 41 tn in the posterior mediastinum ; x - ray revealed 19 / 19 and 3 / 3 fn , respectively . the highest sensitivity and da values ( table 5 ) were obtained by us in the supraaortic ( 97% and 98% , respectively ) , prevascular ( 97% and 98% ) and paratracheal ( 87% and 91% ) regions and aortopulmonary window ( 80% and 93% )  . 
4a , b adenopatie in sede sovraaortica : scansione sovrasternale ( a ) e tc con mdc ( b )  . sono infatti solo 3 i falsi negativi , con una sensibilit del 80% , presentando una performance diagnostica di poco inferiore , per tale distretto , rispetto alla tc ( ad 93% )  . 
lindagine ecotomografica non offre invece adeguata attendibilit diagnostica nella valutazione di distretti mediastinici pi profondi , quali la regione subcarinale ed il mediastino posteriore ( valori di sensibilit pari a 5% e 0% )  . 
tali risultati , pur di scarsa rilevanza diagnostica , sono comunque superiori a quelli riportati con lo studio radiografico standard ( sensibilit pressoch nulla )  . in accordo con gli studi di wernecke et al . 
 ( 1995 , 1997 ) [ 15 , 23 ] sullaccuratezza e lattuabilit di unindagine ecotomografica del mediastino finalizzata a rilevare la presenza di linfoadenopatie , i dati statistici dello studio da noi condotto mettono in evidenza , in confronto con la tc , una buona sensibilit , specificit e accuratezza diagnostica per lesioni localizzate a livello sovraaortico ( 97% , 100% , 98% ) , prevascolare ( 97% , 100% , 98% ) e paratracheale ( 87% , 100% , 91% ) , con differenze di sensibilit nei confronti dellesame radiografico tradizionale del 10 - 58% a favore dellecotomografia . 
in queste sedi lecotomografia appare dunque pressoch sovrapponibile alla tc . anterior mediastinum ( paratracheal region in two cases and prevascular region in three cases ) demonstrated solid masses with increased echogenicity compared with the previous examinations and poor resemblance to adenopathic lesions . 
 two patients had a body habit that was unfavourable for us : the first due to inadequate acoustic windows in the thoracic outlet and the second due to severe spondyloarthrosis with dorsal kyphosis preventing the head hyperextension needed for suprajugular examination . 
tissue harmonic imaging was performed in all cases , allowing for accurate evaluation of the more superficial anatomical regions ; attenuation of the us beam slightly hindered exploration of the deeper districts . 
si infatti osservata una netta superiorit dellaccuratezza diagnostica dellecotomografia mediastinica rispetto alla radiografia standard del torace : lo studio ultrasonografico del mediastino consente infatti di valutare meglio le diverse regioni e di evidenziare linfoadenopatie pi piccole e centrali , che non determinano alcuna modificazione delle linee mediastiniche sul radiogramma . 
tale lieve discrepanza pu essere legata alla diversa tipologia di studio , con valutazione , nei lavori segnalati , di tumori mediastinici anche non linfomatosi , e quindi caratterizzati da struttura con gradiente di ecogenicit maggiore rispetto ai tessuti circostanti . di notevole interesse , inoltre , il risultato ottenuto per lo studio della finestra aortopolmonare ( sensibilit e specificit pari rispettivamente a 80% e 100% ) , lievemente sopra la media rispetto ai lavori presenti in letteratura . 
i migliori risultati da noi ottenuti in termini di sensibilit sono probabilmente ascrivibili alla migliore qualit delle sonde oggi disponibili e allutilizzo della funzione thi , che consentono una migliore valutazione di questo distretto anatomico , tipifig . 
this modality has acquired an important role in the evaluation of diseases of the pleural cavity , pulmonary parenchyma , chest wall and diaphragm [ 10 , 21 ]  . previous studies have compared us with x - ray and ct only , so the value and potential of us have been analysed in relation to the results obtained with these two imaging modalities . 
our study , conducted on patients with mediastinal hl and nhl , revealed the positive role of us for surveillance and adds to other previous studies on different types of mediastinal malignancies . 
our results indicate that sensitivity and specificity ( 93% and 100% ) of us were higher than those of x - ray ( 66% and 100% ) , as shown in table 3 . 
moreover , us showed remarkable sensitivity in evaluation of the aortopulmonary window , yielding only three false negatives and achieving 80% sensitivity and a da only slightly lower than ct ( da 93% )  . 
us does not have sufficient da in the evaluation of deeper mediastinal regions , such as the subcarinal region and the posterior mediastinum ( sensitivity of 5% and 0% )  . 
on accuracy and feasibility of us in detection of mediastinal lymph nodes [ 14 , 15 , 22 , 23 ] , our statistical data revealed good sensitivity , specificity and da compared with ct for lesions in the supraaortic ( 97% , 100% , 98% ) , prevascular ( 97% , 100% , 98% ) and paratracheal ( 87% , 100% , 91% ) regions , respectively . 
 our data substantially agree with those reported in the studies by wernecke et al . , which evaluated all mediastinal tumours and not only lymphomas [ 12 , 24 , 25 ]  . 
the da of mediastinal us was clearly superior to that of standard chest x - ray : mediastinal us allows better evaluation of the different regions and detection of smaller and more central lymphadenopathies that do not affect the mediastinal lines on radiograms . 
this slight discrepancy may be related to the different study decamente poco esplorabile per la profondit e per la scarsa accessibilit , ma che gode dellottima finestra acustica costituita dallarco aortico che la delimita superiormente . 
per le stesse ragioni di maggiore profondit e scarsa accessibilit , la sensibilit della metodica di molto inferiore se si valutano la regione subcarinale , il mediastino posteriore e le regioni paravertebrali ( sensibilit 0% - 5% )  . 
per quanto riguarda il mediastino posteriore e le regioni paravertebrali , lelevata distanza dalla sonda , con importante assorbimento del fascio ultrasonoro , e le caratteristiche delle finestre acustiche disponibili , di dimensioni ridotte e forma sfavorevole , rendono queste regioni scarsamente accessibili con gli ultrasuoni . 
anche il valore predittivo negativo dellecotomografia , riscontrato pari al 50% , pu essere motivato dalla presenza di regioni pi difficilmente esplorabili con gli ultrasuoni , ed in particolare dal maggior numero di falsi negativi riscontrato a carico di regioni quali la subcarinale . lunica situazione in cui abbiamo constatato una superiorit dallesame radiografico sullecotomografia riguardava linteressamento degli ili polmonari : le stazioni ilari , per le loro peculiari caratteristiche anatomiche di sede e rapporti , sono infatti ben valutabili sul radiogramma , ma non esplorabili con gli ultrasuoni . 
alcuni autori sostengono che la scarsa accessibilit di alcune regioni mediastiniche agli ultrasuoni non debba essere considerata limitante per lutilizzo dellecotomografia , perch il successo del trattamento analogo a livello di tutte le localizzazioni di malattia [ 14 , 18 ]  . 
 ( 1991 ) hanno osservato che tutti i linfonodi non evidenziati con lecotomografia mostravano risposta alla terapia identica a quella delle adenopatie accessibili agli ultrasuoni . un aspetto di notevole importanza legato alla peculiare capacit dellecotomografia di studiare con notevole dettaglio le strutture superficiali . 
in alcuni casi lindagine ultrasonografica stata agevolmente estesa alla valutazione di adenopatie a livello sovraclaveare , latero - cervicale ed ascellare , presenti rispettivamente in 17 , 4 e 2 esami . 
sono tutte possibili localizzazioni della malattia , per la loro sede non facilmente rilevate con altre indagini , che risultano invece di facile esplorazione con gli ultrasuoni , diventando cos reperti aggiuntivi nella valutazione della risposta alla terapia . bench lunico criterio di differenziazione tra linfonodi normali e patologici in tc sia di tipo esclusivamente dimensionale , sono stati osservati casi di linfonodi ingranditi non coinvolti in processi neoplastici n flogistici classificati come patologici dallesame tc e non evidenziati in ecotomografia , e linfonodi invece patologici di dimensioni 1 cm non considerati come tali dalla tc . 
inoltre , il confronto tra le dimensioni di adenopatie mediastiniche misurate mediante tc con quelle ricavate da esame ecotomografico non sempre ugualmente attendibile : molti linfonodi , infatti , sono disposti in senso longitudinale nel mediastino [ 23 ]  . 
our better sensitivity values are probably the result of the improved quality of current transducers and the use of the thi function , which enable better evaluation of this deep and poorly accessible anatomical region in which the aortic arch provides , however , an excellent acoustic window . 
a significant distance from the probe , with intense absorption of the us beam , together with the small and suboptimal acoustic windows , make the posterior mediastinum and paravertebral regions barely amenable to sonography . 
the negative predictive value ( npv ) of sonography ( 50% ) and , in particular , the high number of false negatives at the subcarinal level may be due to the presence of regions that are difficult to explore by us . 
 one site in which chest x - ray proved superior to us was the pulmonary hiludue to their peculiar anatomic characteristics , hilar stations are clearly visualised on x - ray but not on us . 
some authors maintain that the poor accessibility of some mediastinal regions should not limit the use of us since treatment is successful for all disease locations [ 14 , 18 ]  . 
 [ 18 ] noted that all lymph nodes missed by us had identical response to treatment to those that were visible . a very important aspect is the ability of us to visualise superficial structures . 
in some cases , assessment was extended to adenopathies in the supraclavicular , laterocervical and axillary regions , present in 17 , four and two of our patients , respectively . 
 though size is the only ct criterion for discriminating between normal and pathological nodes , enlarged lymph nodes uninvolved by neoplastic or inflammatory processes were classified as pathological on ct but were not visualised on us ; likewise , pathological lymph nodes 1 cm were not classified as such by ct . 
moreover , comparison of the size of mediastinal adenopathies measured on ct and us is not always reliable : many lymph nodes are arranged longitudinally in the mediastinum [ 23 ]  . 
tale discrepanza pu essere oggi superata grazie alle efficaci ricostruzioni multiplanari ottenibili con la tc multislice ( msct ) , metodica per altro meno diffusamente disponibile rispetto alla tc con una o due spirali . la misurazione ultrasonografica , condotta sistematicamente ed in modo dettagliato durante gli esami eseguiti per il nostro studio , correla meglio con le reali dimensioni del conglomerato adenopatico . 
chiaro che la metodica ultrasonografica non pu assolutamente competere , per quanto riguarda laccuratezza diagnostica , con la tc , che infatti nel nostro lavoro viene considerata indagine di riferimento : per sicuramente utile come esame complementare nello studio delle masse linfoadenopatiche in corso di terapia , anche solo per il semplice controllo dimensionale , parametro sempre importante nella valutazione della risposta al trattamento . lecotomografia stata inoltre in grado di aggiungere un criterio di valutazione qualitativo ( lecogenicit ) a quello quantitativo tipico della tc ( il diametro massimo ) [ 13 , 16 ] , che sembra essere un indicatore pi affidabile dellattivit tumorale rispetto alla sola valutazione dimensionale . 
nel nostro lavoro la metodica ultrasonografica risultata in alcuni casi pi precisa e dettagliata rispetto alla tc nella valutazione strutturale di tessuti a livello del mediastino anteriore . nel corso della chemioterapia , si proceduto infatti alla valutazione ultrasonografica della struttura delle linfoadenopatie , che risultata ipoecogena in 92 / 97 ( 95% ) casi . 
negli altri 5 casi ( 5% ) , nei quali la tc rilevava la presenza di formazioni patologiche riferite verosimilmente a linfoadenopatie a livello del mediastino anteriore ( in 2 casi a carico della regione paratracheale ed in 3 della regione prevascolare ) , lecotomografia mostrava formazioni solide ad ecogenicit aumentata rispetto ai controlli precedenti e con scarsa delimitazione di vere e proprie lesioni adenopatiche . tale reperto contrastava con quello tc , che segnalava formazioni di verosimile natura adenopatica con caratteristiche densitometriche non specifiche . 
molti studi confermano infatti la possibilit di differenziare , con lecotomografia , il tessuto adenopatico attivo da residui fibrosi conseguenti alla terapia , distinzione non consentita dalla tc [ 14 , 18 ]  . linfonodi infiltrati da cellule neoplastiche , infatti , appaiono ipoecogeni rispetto al tessuto adiposo ed al connettivo circostanti . 
se rispondenti alla terapia , assumono di nuovo , progressivamente , la loro naturale ecogenicit , fino al punto da non essere pi distinguibili se si ottiene la remissione completa della patologia . 
 us has added a qualitative criterion for evaluation ( echogenicity ) to the quantitative criterion of ct ( maximum diameter ) [ 13 , 16 ] , and echogenicity appears to be a more reliable indicator of tumour activity compared with size . 
in some cases , us proved more precise and detailed than ct in the structural evaluation of tissues within the anterior mediastinu during chemotherapy , us appearance of adenopathic masses was hypoechoic in 92 / 97 cases ( 95% )  . 
in the remaining five cases ( 5% ) in which ct showed the presence of pathological masses in the anterior mediastinum ( in the paratracheal and prevascular regions in two and three cases , respectively ) , us detected solid masses with increased echogenicity compared with the previous follow - up exams and poor resemblance to adenopathic lesions . 
others , such as schulte - altedorneburg et al . , believe that the use of us contrast material does not significantly add to the information obtained with conventional us ( or colour power doppler ) despite the good depiction of intranodal vascularity [ 27 ]  . 
on the basis of our preliminary observations , we believe that the use of sonographic contrast material in mediastinal lymphadenopathies may improve da , above all for evaluating the activity of residual tissue . our study indicates that mediastinal us , a technique requiring regular practice and specific training , offers a number of advantages : it is inexpensive , widely available and reproducible an ideal condition for frequent use during follow - up and is generally characterised by good compliance given that there are no side effects due to ionising radiation or iodinated contrast material . 
us has good da for evaluation of some mediastinal regions only , with deeper lesions being more difficult to distinguish due to the high rate of absorption of the us beam . the uncertain acoustic window prevents exploration of the posterior mediastinal regions . 
 ( 2004 ) , sulla base delle caratteristiche di perfusione osservate , sostengono una maggiore accuratezza diagnostica dellindagine condotta con la somministrazione del mdc [ 26 ]  . si contrappongono coloro che , come schulte - altedorneburg et al . 
 ( 2003 ) , ritengono che lutilizzo del mdc non comporti un incremento significativo delle informazioni fornite dallecotomografia condotta tradizionalmente , eventualmente con lausilio del color - power - doppler , nonostante la buona visualizzazione della vascolarizzazione intranodale [ 27 ]  . nostra opinione , in base ad osservazioni preliminari da noi condotte , che lutilizzo del mdc su linfoadenopatie mediastiniche possa migliorare lattendibilit diagnostica della metodica ecotomografica , soprattutto nella valutazione dellattivit di tessuti residui , evidenziando uno specifico pattern di enhancement . dalla nostra sperimentazione abbiamo inoltre evidenziato come lecotomografia mediastinica , esame che richiede una pratica assidua e una preparazione specifica delloperatore , presenti numerosi vantaggi di carattere generale : un esame poco costoso , facilmente disponibile e ripetibile , condizione ideali per un frequente utilizzo in corso di followup , ed generalmente caratterizzato da una buona compliance , trattandosi di unindagine priva di effetti collaterali in quanto non ricorre allutilizzo di radiazioni ionizzanti n di mdc organoiodato . abbiamo tuttavia osservato alcuni limiti , strettamente legati alla metodica . 
lesame presenta buona attendibilit diagnostica per lo studio solo di alcune regioni mediastiniche , mentre lesioni situate in distretti pi profondi , per lelevato assorbimento del fascio ultrasonoro , risultano difficilmente distinguibili dai tessuti circostanti : la precaria finestra acustica non consente di valutare gli spazi mediastinici posteriori , che risultano cos scarsamente esplorabili . le caratteristiche individuali dei pazienti inoltre influiscono sullesito dellesame : lhabitus costituzionale , la presenza di patologie concomitanti o particolari conformazioni anatomiche possono non consentire unesplorazione ottimale . per la valutazione dei linfomi a localizzazione mediastinica lesame di riferimento resta sicuramente la tc , cui si aggiunge in alcuni casi la pet - tc , nonostante limportante dose di radiazioni ionizzanti cui tali indagini espongono i pazienti ( circa 20 msv la tc spirale , 8 msv la sola tc del torace e 10 - 12 msv la pet - tc )  . 
6a , b ecostruttura linfonodale : linfonodo reattivo ( a ) e linfonodo neoplastico ( b )  . patients characteristics , including body habit , presence of concurrent disease or particular anatomical conformation . 
 ct , integrated by pet - ct in some cases , remains the reference standard for evaluation of mediastinal lymphomas despite the high dose of ionising radiation ( approximately 20 msv for spiral ct , 8 msv for chest ct and 1012 msv for pet - ct )  . 
in order to reduce the frequency of ct follow - up scans during treatment , and consequently total radiation exposure , while closely monitoring the disease , the use of mediastinal us could be extend to include evaluation of mediastinal involvement , with chest x - ray being limited to the study of the hilar regions . 
although conventional x - ray is the first - line examination for diagnosis of mediastinal disease , the gold standard for evaluation of this region is ct despite its suboptimal specificity due to poor characterisation of residual tissue after therapy . 
in this context , us is ideal for evaluating mediastinal adenopathies . advantages include good compliance , absence of patient risks , low cost , easy reproducibility and dynamic imaging with multiplanar capabilities and good qualitative and quantitative information . 
disadvantages include operator dependence , limited accessibility of some mediastinal regions and dependence on the individual patients characteristics . nonetheless , poor accessibility of some mediastinal regions should not be regarded as a limiting factor since treatment has proved successful in all disease locations . 
 our study indicates the essential superiority of us over x - ray , particularly in some anatomical districts such as the supraaortic , prevascular and paratracheal regions and the aortopulmonary window . 
in the future , greater experience with mediastinal us may help reduce the frequency of follow - up ct scans . conclusioni per individuare il trend della patologia , in senso positivo o negativo , ed operare quindi le opportune correzioni terapeutiche , di grande utilit per il clinico rilevare in tempi precoci variazioni a carico delle masse neoplastiche a livello mediastinico . 
nonostante la radiologia tradizionale costituisca un primo livello nella diagnosi delle malattie mediastiniche , il gold standard per la valutazione di questa regione rappresentato tuttora , nella pratica clinica , dalla tc , pur con i limiti di specificit dovuti allinsufficiente caratterizzazione tissutale di formazioni residue dopo terapia . 
sono infatti numerosi i vantaggi della metodica : la buona compliance e lassenza di rischi per il paziente , i bassi costi , lagevole ripetibilit , lo studio diagnostico di tipo dinamico che permette una valutazione multiplanare , gli apprezzabili risultati qualitativi e quantitativi , pur a fronte di limiti quali la dipendenza delle informazioni ottenibili dallesperienza delloperatore , il difficile accesso in alcuni distretti mediastinici e lesplorazione difficoltosa in presenza di sfavorevoli caratteristiche individuali del paziente . 
la scarsa accessibilit di alcune regioni mediastiniche agli ultrasuoni non deve tuttavia essere considerata limitante per lutilizzo dellecotomografia , perch il successo del trattamento analogo a livello di tutte le localizzazioni di malattia . nella nostra casistica si pone laccento sulla sostanziale superiorit dellecotomografia rispetto alla radiografia standard , con particolare riferimento ad alcuni distretti anatomici , quali le regioni sovraaortica , prevascolare e paratracheale e la finestra aortopolmonare . 
tali considerazioni spingono a proporre lindagine ultrasonografica come esame importante nel follow - up in corso di terapia dei pazienti affetti da linfomi con localizzazione mediastinica , da affiancare ai controlli tc programmati , la cui frequenza non incrementabile per le note problematiche legate allesposizione a radiazioni ionizzanti . 
gerardo , via pergolesi 33 , i - 20052 monza , italy 3scuola di specializzazione in fisica sanitaria , universit degli studi di milano , via celoria 16 , i - 20133 milan , italy correspondence to : a . 
the aim of this study was to calibrate monitors used in soft - copy review of diagnostic images in a pictures archiving and communication system ( pacs ) and to assess critical quality assurance ( qa ) parameters through appropriate checks . 
barco [ cathode ray tube ( crt ) and liquid crystal display ( lcd ) ] and eizo ( lcd ) monitors were evaluated . calibration and qa controls were carried out during acceptance tests on the systems and every 6 months according to the task group 18 ( tg18 ) report by the american association of physicists in medicine ( aapm )  . 
la calibrazione e i controlli sono stati effettuati in fase di accettazione e successivamente con cadenza semestrale seguendo le indicazione del report tg18 dellamerican association of physicists in medicine ( aapm )  . alcuni dei parametri considerati sono : luminanza massima , rapporto di contrasto , risposta di luminanza , risoluzione spaziale e risposta angolare . 
comunque assolutamente necessario procedere con i controlli di qualit periodici per garantire il perdurare delle caratteristiche di qualit . parole chiave interpretazione diagnostica soft - copy calibrazione monitor aapm tg18 a . 
international papers strongly recommend periodic checks and suggest reference procedures and values ; among them , the american association of physics in medicine ( aapm ) with its task group 18 ( tg18 ) has exhaustively dealt with the issue , thus becoming de facto the main source of reference [ 3 , 4 ]  . materials and methods simultaneously with the installation of the pacs system ( agfa impax ) , 15 reporting stations were set up , each provided with a low - resolution monitor allowing access to the radiological information system ( ris ) database not considered in this study and two high - resolution monitors displaying medical images . 
crt monitors are provided with conventional crts found in tv sets : a brush of accelerated electrons is run along the entire monitor surface and its intensity modulated to generate the required grey level . 
the lcd technology is based , instead , on the ability of liquid crystals to rotate when voltage is applied : the image is then generated by a matrix of liquid crystals that , based on the angle they form , mitigate the light emitted by the backlighting lamp to a varying degree . 
the reporting stations are currently installed in various hospital departments ( radiodiagnostic , accident and emergency ) and at a hospital a few miles away belonging to the same hospital trust . the aapm tg18 document suggests , in addition to the essential calibration , that a number of parameters should be checked , each with different techniques of varying complexity and accuracy levels . 
the decision about which kind of measurement to perform for every characteristic to evaluate was based on a compromise between quality of result and ease of performance , considering the contingent conditions of reporting rooms , which are always very busy and unable to lay out complex experimental setups [ 5 ]  . allinterno di un sistema pacs , come quello recentemente installato presso lospedale s . 
gerardo di monza , il percorso degli esami radiologici pu ora prescindere dalle pellicole radiografiche e seguire un iter completamente digitale.la visualizzazione delle immagini digitali al momento della refertazione viene affidata ad una coppia di monitor ad elevate prestazioni . 
i monitor di visualizzazione entrano anchessi a far parte della catena delle immagini digitali e bisogna evitare che siano questi ultimi il collo di bottiglia che porti ad un degrado della qualit finale dellesame . 
i monitor crt ( cathode ray tube ) sono dotati dei classici tubi catodici di tipo televisivo : un pennello di elettroni accelerati viene fatto scorrere lungo lintera superficie del monitor e modulato in intensit per generare il livello di grigio richiesto . 
la tecnologia lcd ( liquid crystal display ) si basa invece sulla capacit dei cristalli liquidi di ruotare se percorsi da corrente : limmagine viene quindi generata da una matrice di cristalli liquidi che a seconda dellangolo che formano attenuano in modo maggiore o minore la luce emessa dalla lampada retroilluminante . 
le stazioni di refertazione sono attualmente dislocate sia in diversi reparti dellospedale ( radiodiagnostica , pronto soccorso ) , che in un ospedale situato a qualche chilometro di distanza appartenente alla medesima azienda ospedaliera . il documento aapm tg18 suggerisce , oltre alla indispensabile calibrazione , molteplici parametri da controllare , ognuno con diverse tecniche di varia complessit e livello di accuratezza . 
all monitors included in this study are dedicated to reporting ; therefore , they must meet the tightest tolerances of primary monitors . in order to calibrate monitors and subsequent luminance measurements , the x - rite dtp - 92 colorimeter / photometer was used in combination with the medical pro software package ( barco )  . 
we chose to use mostly the phantoms suggested by aapm tg18 and available in digital imaging and communications in medicine ( dicom ) format on the internet [ 3 ]  . images were displayed on stations with the same software normally used by radiologists for reporting ( agfa impax ) , taking care to use the window and level standard values , without any look - up table ( lut ) that the software might apply . 
the just noticeable difference ( jnd ) is introduced for this purpose [ 7 ]  . si basata su di un compromesso tra la qualit del risultato e la semplicit di esecuzione , tenendo conto della situazione contingente delle sale di refertazione , sempre molto impegnate e senza la possibilit di allestire setup sperimentali complessi [ 5 ]  . i sistemi di visualizzazione vengono classificati in sistemi primari e sistemi secondari [ 3 ] ; si definiscono primari i sistemi di visualizzazione utilizzati per la refertazione , sono secondari invece i sistemi che visualizzano immagini mediche per scopi diversi dalla refertazione , tra cui la visualizzazione su console di unit diagnostiche o la consultazione da parte di medici non radiologi . 
tutti i monitor considerati in questo studio sono dedicati alla refertazione , pertanto devono rispondere alle pi strette tolleranze indicate per i monitor primari . per la calibrazione dei monitor e le successive misure di luminanza stato utilizzato il colorimetro / fotometro x - rite dtp - 92 in combinazione con il pacchetto software medical pro ( barco )  . per alcune misure di luminanza stato utilizzato inoltre il fotometro telescopico hagner s3 , caratterizzato dal fatto di poter misurare la luminanza a distanza . 
si scelto nella maggioranza dei casi di utilizzare i fantocci suggeriti da aapm tg18 e disponibili in formato dicom su internet [ 3 ]  . la visualizzazione delle immagini sulle stazioni stata affidata al medesimo software normalmente in uso ai radiologi per la refertazione ( agfa impax ) , avendo per laccortezza di utilizzare i valori standard di finestra e livello , senza utilizzare nessuna lut ( look up table ) che il software table 1 tolerances suggested by american association of physicists in medicine task group 18 ( aapm tg18 ) for primary and secondary displays primary displays secondary displays geometrical distortion , % maximum luminance , cd / m2 contrast ratio luminance response , % luminance uniformity , % resolution noise veiling glare distorsioni geometriche , % luminanza massima , cd / m2 contrasto risposta di luminanza , % uniformit di luminanza , % risoluzione rumore veiling glare > 170 > 250 0 ( cid : 2 ) cx ( cid : 2 ) 4 3 / 4 inserts ( cid : 3 ) 3 inserts > 170 > 250 0 ( cid : 2 ) cx ( cid : 2 ) 4 3 / 4 inserti ( cid : 3 ) 3 inserti tabella 1 tolleranze indicate da aapm tg18 per sistemi di visualizzazione primari e secondari monitor primari monitor secondari > 100 > 100 0 ( cid : 2 ) cx ( cid : 2 ) 6 2 / 4 inserts ( cid : 3 ) 1 inserts > 100 > 100 0 ( cid : 2 ) cx ( cid : 2 ) 6 2 / 4 inserti ( cid : 3 ) 1 inserto a . 
before calibrating , the x - rite contact photometer must be placed in the middle of the screen . with barco crt monitors , the procedure is repeated for every monitor of the pair . 
eizo monitors are instead controlled by the workstation as if they were a single monitor ( because of software and hardware limitations ) ; hence , the calibration curve applied will be the same for both monitors . 
in this case , the calibration will be performed first on the left then on the right monitor , and the quality of the greyscale curve will be checked to ensure it is within limits . 
the only possible correction is reduction of the brightness setting of the brightest monitor in order to equalize maximum luminance ( lmax ) as much as possible before the actual calibration . 
unfortunately , the user is given no information on the corrections made . geometric distortions deflections of the electron beam along its path often cause geometric distortions to appear on crt monitors that do not maintain the height / width ratios in the different screen areas . this is a known defect , and high - quality monitors usually incorporate appropriate correction circuits . 
partendo dal modello di barten della visione umana definita la curva dicom che associa un valore di luminanza tra 0 , 05 e 4000 cd / m2 a ognuno dei 1023 jnd che si suppongono discernibili dallocchio umano [ 8 ]  . 
la calibrazione fa in modo che , dato un intervallo di luminanza minima - massima , i valori di luminanza dei livelli di grigio intermedi si dispongano su jnd equispaziati , ottenendo quindi la linearizzazione percezionale [ 9 ]  . la procedura di calibrazione gestita in modo automatico dal software medical pro attualmente installato su tutte le stazioni destinate alla refertazione . 
i monitor eizo sono invece pilotati dalla workstation come se fossero un monitor unico ( a causa di limitazioni software e hardware ) , pertanto la curva di calibrazione applicata sar la stessa per entrambi i monitor . 
lunica correzione possibile ridurre limpostazione di luminosit ( brightness ) del monitor pi luminoso in modo da pareggiare lmax il pi possibile prima di procedere alla calibrazione vera e propria . 
i monitor barco lcd dispongono di un sensore incorporato che controlla in tempo reale la luminanza massima in modo da garantire una maggiore stabilit nel tempo di tale parametro . questo sensore anche utilizzato per la calibrazione dal software medical pro al posto del fotometro x - rite . 
purtroppo nessuna informazione viene fornita allutente sulle correzioni effettuate . distorsioni geometriche le deflessioni del pennello elettronico lungo il suo percorso portano spesso i monitor crt a presentare delle distorsioni di tipo geometrico in cui non sono mantenuti i rapporti altezza / larghezza nelle diverse aree dello schermo . 
according to the tg18 , under optimal conditions , the smallest insert observable in total darkness must be the same as can be observed under standard reporting conditions ; i.e. 
light conditions of the room should be adjusted to achieve this condition . however , the measurements were taken in a less - than - optimal reporting situation , with a good number of ambient lights [ 10 ]  . luminance and contrast the lmax and minimum luminance ( lmin ) are measured during the calibration procedure while a preset value can be set in the software . 
secondo il tg18 in condizioni ottimali il minimo inserto visibile in condizioni di buio totale deve essere lo stesso visibile nelle condizioni standard di refertazione ; i riflessi luminosi non devono cio interferire con la visione dei dettagli a basso contrasto . 
nelle misure effettuate stata comunque considerata una situazione di refertazione non ottimale , accendendo un buon numero di luci ambientali [ 10 ]  . luminanza e contrasto la luminanza massima ( lmax ) e quella minima ( lmin ) vengono misurate durante la procedura di calibrazione ed possibile impostare nel software un valore prefissato . 
nei monitor barco come lmax viene impostato un valore corrispondente a quello dichiarato dalla casa costruttrice come valore calibrato ; tale luminanza inferiore alla luminanza massima che il monitor in grado di emettere , in modo che sia possibile nel tempo mantenere la luminanza calibrata nonostante linevitabile decadimento dovuto alluso [ 11 ]  . 
i monitor eizo invece , per poter rispettare i limiti minimi di luminanza richiesti vanno impostati alla massima luminanza possibile ( brightness = 100% nella maggioranza dei casi ) , rendendo cos impossibile compensare il deterioramento che viene inoltre accelerato dagli alti valori di brightness impostati . 
il rapporto di contrasto ( cr ) dipende fortemente dal valore di lmin ; questultimo non pu essere abbassato a piacere poich renderebbe indistinguibili i dettagli a bassa luminanza , fig . 
eizo monitors , on the other hand , must be set to the highest lmax possible ( brightness = 100% in most cases ) to meet lmin requirements , thus making it impossible to compensate for deterioration , which is also accelerated by the high brightness values set . 
the contrast ratio ( cr ) depends largely on the lmin value ; it cannot be decreased at will because it would make the low luminance details vague , blurred by the ambient light reflections . 
these images are made up of 20% luminance background and of a central square of luminance spanning from black to white in 16 intervals with equally spaced grey levels , one per image . 
these measurements are taken by placing the contact photometer in the middle of the image . the luminance interval ( lmin - lmax ) is divided into 16 jnd equally spaced levels , resulting in a luminance vs . 
the same medical pro calibration software can automatically check the calibration following a similar procedure : the result is a percentage value indicating the degree of matching between the response curve and the dicom curve . 
this test is used for the periodic qa checks and , sometimes , to decide whether to recalibrate a monitor if it is out of tolerance . luminance uniformity luminance uniformity is often poor in crt monitors because of the different paths electrons have to travel before reaching the various spots of the screen . 
in barco monitors ( both crt and lcd ) , the evaluation was performed separately for each monitor of the pair while with eizo monitors , the five squares are distributed between both monitors , thus providing an overall uniformity for that pair . 
the tolerance suggested by aapm tg18 is 30% , as the maximum difference . spatial resolution the resolution capability of a monitor is not merely its speciconfusi dai riflessi della luce ambiente . 
le tolleranze indicate da aapm tg18 sono : lmax > 170 cd / m2 e cr > 250 . risposta di luminanza le misure di verifica della calibrazione sono state effettuate utilizzando i 16 fantocci geometrici aapm tg18 - ln ( fig . 3 ) , e il fotometro a contatto x - rite . 
queste immagini sono composte da uno sfondo di luminanza 20% e da un quadrato centrale di luminanza variabile dal nero al bianco in 16 intervalli a livelli di grigio equispaziati , uno per ogni immagine . 
maggiormente significativi sono i valori di risposta di contrasto , cio dl / l vs . jnd , la cui tolleranza consigliata del 10% rispetto al relativo valore nella curva dicom . 
lo stesso software di calibrazione medical pro in grado di effettuare un controllo automatico sulla calibrazione con un sistema analogo : il risultato fornito un valore percentuale indicante la corrispondenza della curva di risposta con la curva dicom . 
tale test viene utilizzato per i controlli di qualit periodici ed eventualmente per decidere di ricalibrare un monitor qualora fosse fuori dalle tolleranze . uniformit di luminanza luniformit di luminanza spesso carente nei monitor crt , a causa del differente percorso che gli elettroni devono percorrere per giungere nelle diverse regioni dello schermo . 
luniformit di luminanza stata misurata utilizzando un fantoccio geometrico incluso nel software medical pro ; composto da uno sfondo con luminanza 20% e da 5 aree quadrate ( centro e 4 angoli ) con luminanza 100% . 
nei monitor barco ( sia crt che lcd ) la valutazione stata effettuata separatamente per i due monitor della coppia , mentre per i monitor eizo i 5 quadrati sono distribuiti sui due monitor , fornendo quindi un valore di uniformit complessivo della coppia . 
la tolleranza proposta da aapm tg18 del 30% come massima differenza . risoluzione spaziale la capacit risolutiva di un monitor non semplicemente la dimensione del pixel dichiarata ma deve includere la capacit di controllare lemissione del singolo pixel indipendentemente da quelli vicini . 
resolution was evaluated through a visual test using the tg18 - cx phantom ( fig . 4 ) composed of a number of graphic inserts , with different levels of grey covering the entire surface of the monitor and showing in the middle a caption reporting the scores to be assigned to the resolution of those inserts . 
the average luminance in the middle of two test objects composed of horizontal and vertical bands , alternatively black and white , at the monitors nominal resolution ( nyquist frequency ) was measured with a hagner telescopic photometer . 
the two objects are expected to have a different average luminance because the electron beam is required to vary extremely quickly from minimum to maximum intensity and vice versa to draw the vertical bands , generating a lower average luminance because the maximum intensity condition has not been reached yet . 
these inserts are located in the middle and in the four corners of the tg18 - qc phantoaccording to aapm tg18 , the percentage difference between the average luminance cannot exceed 30% in the middle of the monitor . 
monitor response at half the frequency ( two black bands and two white bands ) was probed using the inserts contained in the same phantom . noise background noise on screen is one of the possible factors limiting resolution of low - contrast details . 
i punteggi variano da 0 ( perfetto ) a 9 ( gravi problemi di risoluzione ) ; sono presenti anche valori negativi che indicano un problema di funzionamento del monitor . 
con il fotometro telescopico hagner si misurata la luminanza media al centro di due oggetti test , composti da righe orizzontali e verticali alternativamente bianche e nere , alla risoluzione nominale del monitor ( frequenza di nyquist )  . 
ci si aspetta che i due oggetti abbiano luminanza media differente , in quanto al pennello elettronico sono richiesti rapidissimi passaggi dallintensit minima a quella massima e viceversa , per rappresentare le linee verticali , generando una luminanza media inferiore a causa del mancato raggiungimento della condizione di intensit massima . 
stata indagata anche la risposta del monitor a una frequenza dimezzata ( 2 linee nere e 2 linee bianche ) tramite gli inserti presenti nel medesimo fantoccio . rumore il rumore di fondo nella visualizzazione a schermo uno dei fattori che pu limitare la risolvibilit di dettagli a basso contrasto . 
la tolleranza suggerita che siano visibili 3 dettagli su 4 . i riflessi che avvengono allinterno della superficie del monitor producono un aumento della luminanza nelle aree scure adiacenti o circondate da aree ad alta luminanza . 
la luminanza percepita quindi fortemente variabile in funzione dellangolo di visione , provocando una degradazione del contrasto , arrivando perfino a valori negativi ( inversione del contrasto )  . per ovviare a questo problema necessario conoscere le fig . 
therefore , the perceived luminance is a heavily variable as a function of the viewing angle , causing some contrast degradation , even reaching negative values ( contrast inversion )  . 
lmax and lmin were measured with the hagner telescopic photometer aimed at the centre of the tg18 - ln phantoms , considering only the two extreme luminance values ( 0% and 100% )  . 
according to aapm tg18 , the cr for angles other than the perpendicular should not drop by more than 30% below the limit suggested for the contrast ( 250 ) ; hence , the maximum cr value allowed is 175 . anatomical images ten radiologists of different ages and experiences were recruited for this evaluation . 
the tg18 - qc pattern results from the wellknown society of motion picture and television engineers ( smpte ) phantom , which is currently the industrial standard to test television chains ; the use of this pattern is recommended by the international literature for day - to - day qa [ 12 , 13 ]  . results and discussion during acceptance tests , save for a few exceptions , monitors fig . 
6 tg18 - gv : nellangolo rappresentato un dettaglio degli inserti a basso contrasto presenti nel centro del fantoccio . caratteristiche del monitor in modo da definire un intervallo angolare in cui luminanza e contrasto rimangono entro i limiti di accettabilit . 
lmax e lmin sono state misurate con il fotometro telescopico hagner puntato sul centro dei fantocci tg18 - ln limitatamente ai due valori di luminanza estremi ( 0% e 100% )  . 
secondo aapm tg18 , il rapporto di contrasto per angoli diversi dalla normale non deve scendere di oltre il 30% rispetto al limite suggerito per il contrasto ( 250 ) ; quindi il massimo valore di cr consentito 175 . immagini anatomiche per questa valutazione sono stati arruolati dieci medici radiologi con diversa et ed esperienza . 
stato chiesto loro di valutare due immagini di riferimento : una radiografia toracica e una articolazione del ginocchio , in quattro modalit : su pellicola ( gold standard ) , su monitor barco crt , su monitor barco lcd e su monitor eizo lcd . 
nonetheless , the evolution of quality over time was followed by half - yearly checks . geometric distortions by their nature , lcd monitors are not affected by distortions , and this has been confirmed by the measurements always showing a 0% distortion . 
the measurements taken on crt monitors are always well within the 2% tolerance ( fig . 7 ) ; the slightly increasing trend that may be noticed may , in the future , require manually correcting the image geometry with the supplied software . ambient reflections no evident specular reflections were found because of the correct monitor position ; the presence of diffuse reflections caused by the light emitted by the adjacent ris monitor , by any view boxes and by other ambient lights . 
eizo monitors are significantly less sensitive to this effect , owing to the absence of glass protections , which is typical of lcd monitors . as a result , taking into account the presence of ambient light sources is crucial ; when possible , they must be switched off before using monitors for medical purposes . 
the different quality of monitors stands out immediately : medical models feature a high lmax , as well as the ability to keep it constant over a long period . eizo monitors are , instead , pushed to the limit from the very first day to meet the minimum requirements , determining their quick deterioration . 
il pattern tg18 - qc deriva dal ben noto fantoccio smpte che attualmente lo standard industriale per la verifica delle catene televisive ; lutilizzo di tale pattern raccomandato dalla letteratura internazionale come controllo di qualit giornaliero [ 12 , 13 ]  . risultati e discussione nel corso delle prove di accettazione , salvo piccole eccezioni , i monitor sono risultati entro le tolleranze consigliate . 
si comunque proceduto a seguire landamento nel tempo della qualit grazie allesecuzione di controlli con cadenza semestrale . distorsioni geometriche i monitor lcd per loro natura non risentono di distorsioni e ci stato confermato dalle misure che indicano una distorsione sempre pari allo 0% . 
this shows that calibration is crucial and requires a number of conditions to be met : the photometer must be in a correct position , the screen must be sufficiently clean and sufficient monitor warm up is necessary . 
the quality factor of the curve did not deteriorate much over time , and only occasionally did the monitor need to be recalibrated after the tolerances were no longer met . 
nel giro di un anno la luminanza massima di molti di questi calata al di sotto del valore di tolleranza di 170 cd / m2 , fatto che ne ha resa necessaria la sostituzione . 
i rapporti di contrasto dei monitor barco , sia crt che lcd si mantengono invece stabili su valori decisamente alti . risposta di luminanza in fase di accettazione stata acquisita la curva di luminanza e di contrasto per ogni monitor . 
8a , b andamento temporale della luminanza massima , aa monitor barco , bb monitor eizo . left monitor dicom right monitor left monitor dicom right monitor gray level / livello di grigio , jnd gray level / livello di grigio , jnd fig . 
luminance decay against time is consequently independent of the single monitor . spatial resolution visual test of spatial resolution confirmed the excellent resolution capability of the monitors in question , also over time . values measured on lcd monitors are constantly 0 , and on crt monitors , they stay within the tolerance range without decreasing over time . 
the luminance method was applied to crt monitors only during the acceptance to probe even more deeply the actual spatial resolution . the monitor proved scarcely able to represent pairs of lines at the nominal resolution along the horizontal axis . 
this realisation and the success of the tg18 - cx visual test let us assume that a structure such as the pairs of vertical lines can push the monitor to its limits but under perfectly theoretical conditions , which cannot be repeated in clinical usage . 
those frequencies cannot be distinguished by the average observer , who can always rely on software instruments to magnify the area of interest . noise on barco monitors , three inserts out of four are visible while on eizo monitors , only two are visible . 
no variations of this parameter were observed over time . the test is strongly affected by contrast resolution , which is lower on eizo monitors because of a lower maximum luminance . 
the noise generated by monitors , especially lcds , is predictably negligible ; hence , the inability to view the third insert , needed to meet tolerances , is really due to poor contrast . dal documento aapm tg18 , riportata sul grafico quale riferimento . 
ci indice della criticit della calibrazione che richiede molte accortezze , quali un corretto posizionamento del fotometro , una buona pulizia dello schermo e un sufficiente tempo di preaccensione del monitor . il fattore di qualit della curva non ha subito decadimenti particolari nel tempo e solo occasionalmente stato necessario ricalibrare il monitor a seguito di un mancato rispetto delle tolleranze . 
ovviamente il monitor finir per lavorare su di un range di jnd molto inferiore . uniformit di luminanza le misure di uniformit sono risultate sempre contenute nel 30% di tolleranza indicata . 
il degrado della luminanza in funzione del tempo risulta quindi indipendente dal singolo monitor . risoluzione spaziale il test visuale di risoluzione spaziale ha confermato lottima capacit risolutiva dei monitor in oggetto , anche nel corso del tempo . 
questa constatazione , unita al buon risultato ottenuto dal test visuale tg18 - cx , inducono a pensare che una struttura come le coppie di linee verticali siano in grado di portare il monitor ai suoi limiti , ma in condizioni del tutto teoriche e non presenti nellutilizzo clinico . 
tali frequenze infatti non sono neppure discernibili da un osservatore medio che potr sempre contare sullutilizzo di strumenti software per magnificare larea di interesse . veiling glare angular response all monitors were found to be within tolerance values , allowing three inserts to be distinguished . rumore table 2 shows the maximum angles from the perpendicular that maintain the luminance values acceptable . 
si pu quindi sconsigliare lutilizzo diagnostico dei monitor per angoli superiori a 30 per gli eizo e 50 per i barco . with eizo and greater than 50 with barco monitors is not to be recommended . immagini anatomiche anatomical images radiologists evaluations were analysed using students t test for paired samples , comparing the scores obtained with the different types of monitors with those obtained on film ( table 3 )  . 
eizo monitors were judged better than film , but in nearly all cases , the score was comparable although the test was carried out with highresolution images , which are not usually reported on these workstations . conclusions measurements taken confirm the good quality of the system and its suitability to that specific application [ 14 , 15 ]  . 
the quality of the greyscale curve declines over time , making it essential to repeat the le valutazioni dei radiologi sono state analizzate utilizzando il test t di student per campioni appaiati , confrontando i punteggi ottenuti dai diversi tipi di monitor con quelli del film ( tabella 3 )  . 
solo in pochi casi la qualit del monitor stata giudicata inferiore a quella della pellicola e neppure sono mancati casi in cui i monitor barco venissero valutati meglio del gold standard . 
i monitor eizo non sono mai risultati migliori del film , ma nella quasi totalit dei casi il giudizio risultato equivalente , anche se il test effettuato riguarda immagini ad alta risoluzione che solitamente non vengono refertate su queste stazioni di lavoro . conclusioni le misure effettuate confermano la buona qualit del sistema e ladeguatezza allutilizzo specifico [ 14 , 15 ]  . 
the measurements taken also enabled us to use the monitors in tasks suitable for their potential : eizo monitors , for instance , are not used in the reporting of high - resolution examinations while barco monitors showed their high quality even in the most critical applications . 
the periodic 6 - monthly checks are currently assigned to the medical physics expert , but it is not to be ruled out , that in the future , part of them could be performed by the radiographer . misurazioni effettuate hanno inoltre permesso di assegnare i monitor a compiti adeguati alle loro potenzialit : i monitor eizo ad esempio non vengono utilizzati per la refertazione di esami ad alta risoluzione . 
de cicco2 1unit operativa di radiologia domenico noto , azienda ospedali civili riuniti giovanni paolo ii , sciacca , italy 2unit operativa di neuroriabilitazione intensiva , fondazione salvatore maugeri , azienda ospedali civili riuniti giovanni paolo ii , sciacca , italy correspondence to : f . 
barbiera , via lanza 2 , i - 92019 sciacca , italy , tel . : + 39 - 0925 - 962203 , fax : + 39 - 0925 - 962316 , e - mail : radiologia@ospedaledisciacca.it * authors contributed equally to this study / * gli autori hanno contribuito in parti uguali alla realizzazione di questo studio received : 8 february 2006 / accepted : 22 march 2006 / published online : 11 august 2006 abstract purpose . 
in 1 year ( march 2004march 2005 ) 47 patients with oropharyngeal dysphagia due to different types of neurological deficit and who required rehabilitation were studied . all patients underwent : ( 1 ) clinical history assessment , ( 2 ) speech therapy assessment and ( 3 ) vfss using digital fluoroscopy ( 25 frames per second )  . 
patients were divided according to the waxman classification into seven levels of dysphagia , and the most suitable type of feeding was selected ( normal diet , restricted diet , artificial nutrition )  . 
in 13 / 47 ( 28% ) patients , vfss identified changes at the oral ( three patients ) or pharyngeal stage ( three patients ) or both ( seven patients ) but with no signs of silent aspiration . 
our experience shows that vfss precisely classifies the degree of dysphagia that conditions the dietary management of each neurologically compromised patient . key words dysphagia videofluorography swallow study rehabilitation riassunto obiettivo . 
tutti i pazienti sono stati sottoposti a : ( 1 ) valutazione clinico - anamnestica ; ( 2 ) valutazione logopedica ; ( 3 ) studio videofluorografico della deglutizione attraverso un sistema di fluoroscopia digitale ( 25 frame per secondo )  . 
tutti i pazienti sono stati classificati secondo la classificazione di waxmann in 7 livelli di disfagia e su questa base stata scelta la tipologia di nutrizione pi appropriata ( dieta libera , dieta con limitazione , nutrizione non orale )  . 
la videofluorografia ha confermato la presenza di aspirazione in 21 / 47 pazienti ( 44% ) di cui 4 ( 8% ) non sospettabili sulla base della valutazione clinico - logopedica in 13 / 47 ( 28% ) pazienti la videofluorografia ha dimostrato la presenza di alterazioni della fase orale ( 3 pz ) o della fase faringea ( 3 pz ) o di entrambe ( 7 pz ) ma senza segni di aspirazione silente . 
la nostra esperienza dimostra che attraverso lesame videofluorografico della deglutizione si pu ottenere una precisa classificazione della entit della disfagia e , su questa base , scegliere la dieta pi opportuna per ogni singolo paziente . parole chiave disfagia videofluorografia riabilitazione introduction introduzione f . 
the incidence of dysphagia following cerebral infarct varies from 25% to 45% [ 13 ] while it has been estimated that around 50% of patients with parkinsons disease are dysphagic [ 4 ]  . 
in these patients , the videofluorography swallow study ( vfss ) is crucial , given its ability to study disruptions in the swallowing process and , above all , to identify the presence of aspiration of food , which may cause aspiration pneumonia or choking [ 5 , 6 ]  . 
the aim of this study was to demonstrate the important role played by vfss in the management of dysphagic patients and especially in the selection of the type of diet the patient can maintain ( oral , artificial or mixed ) when they are admitted to the neurorehabilitation ward and after rehabilitative and speech therapy . materials and methods the study was based on a series of 47 patients observed during the period march 2004march 2005 suffering neurological deficit varying in nature ( table 1 ) and varying degrees of oropharyngeal dysphagia . 
lincidenza di disfagia dopo infarto cerebrale stata stimata in percentuali variabili da 25% al 45% [ 13 ] , mentre si calcola che circa il 50% dei pazienti con malattia di parkinson presentino disfagia [ 4 ]  . in questi pazienti lesame videofluorografico della deglutizione considerato di fondamentale importanza in quanto consente di studiare lalterazione della dinamica deglutitoria e soprattutto di identificare la presenza di aspirazione del materiale alimentare che pu causare polmonite ab - ingestis o soffocamento [ 5 , 6 ]  . scopo del presente lavoro quello di dimostrare il ruolo centrale dellesame videofluorografico della deglutizione nel management del paziente disfagico ed in particolare nella selezione del tipo di alimentazione che il paziente pu mantenere ( orale o artificale o mista ) al momento dellammissione nel reparto di neuroriabilitazione e dopo terapia riabilitativa e logopedica . materiali e metodi il presente lavoro si basa su una casistica di 47 pazienti osservati nel periodo compreso tra marzo 2004 e marzo 2005 e con deficit neurologici di vario tipo ( tabella 1 ) e differente grado di disfagia orofaringea . i pazienti , 27 maschi e 20 femmine , presentavano et compresa tra 16 e 80 anni e venivano inviati per un programma di riabilitazione neuromotoria . 
in realt il numero di pazienti disfagici , osservati nellarco di tempo considerato nel presente lavoro , stato di 62 su un totale di 270 pazienti ricoverati : di questi 62 pazienti , 3 sono stati esclusi in quanto non valutabili dal punto di vista logopedico e radiologico per il grave deficit cognitivo ; in altri 12 pazienti stata fatta la valutazione logopedica , ma non stato possibile eseguire lo studio videofluorografico con sufficiente attendibilit diagnostica ( pazienti irrequieti , con postura del capo non adeguata o impossibilitati a trattenere anche minime quantit di mdc nel cavo orale )  . tutti i 47 soggetti sono giunti alla nostra osservazione entro i primi 6 - 12 mesi dallesordio della disfagia e sono stati sottoposti a : 1 . 
valutazione logopedica con lanalisi di : livello di vigilanza , prassie bucco - linguo - facciale , sensibilit e motricit dellapparato linguo - buccale , attuazione di prove di deglutizione , ricerca di eventuali segni di inalazione e riflessi di protezione , studio delle funzioni correlate con la deglutizione ( fonazione e respirazione )  . sulla base della valutazione clinica e logopedica si sono suddivisi i pazienti in : f . 
speech assessment with analysis of the level of awareness , oral - buccal - lingual apraxia , sensitivity and motility of the lingual - buccal apparatus , swallowing trials , search for possible signs of aspiration and protection reflexes and study of functions correlated with swallowing ( phonation and breathing )  . 
to correlate the clinical data with the speech assessment and vfss findings , we used the dysphagia severity rating scale proposed by waxman et al [ 7 ] ( table 2 ) in which each patient has a different degree of dysphagia ( 7 points ) based on clinical findings ( more - or - less severe dysphagia , lengthening of meal times , nutritional state ) , speech assessment ( presence / absence of cough reflex , presence and degree of voluntary cough , ability to learn swallowing techniques and compensatory strategies ) and the findings of vfss ( presence / absence of aspiration , aspiration of one or more consistencies , amount of material aspirated , presence of cough reflex )  . 
on this basis , all patients were classified using the 7 - point scale , and as a result , the most appropriate type of diet was selected , as follows : free diet restricted diet ( semisolid homogenised with liquid restrictions ; semiliquid with a higher water content than the first ) nothing - by - mouth diet [ percutaneous endoscopic gastrostomy ( peg ) or nasogastric tube ] during their hospital stay , patients underwent speech therapy and a rehabilitation programme aimed , among other things , at regaining correct posture and in some cases ( patients with aspiration ) , a second vfss . 
on the basis of clinical course and degree of recovery obtained , modification to the hospital diet was assessed at the time of discharge . results results of the speech assessment showed suspected dysphagia with aspiration ( cough , gurgly voice , desaturation , low - grade fever , feeling of choking ) in 29 / 47 patients ( 61.7% ) while in the remaining cases , alterations to the oral and pharyngeal phases of swallowing were present but signs indicating aspiration were absent . 
in 13 / 47 patients ( 28% ) , vfss demonstrated the presence of alterations to the oral phase ( three cases ) or the pharyngeal phase ( three cases ) or both ( seven cases ) but without silent aspiration . 
in the remaining 13 patients ( 28% ) , vfss showed no swallowing alterations . on the basis of clinical and radiological findings , the patients were classified according to the waxman dysphagia dellesame videofluorografico il radiologo non era a conoscenza del risultato della valutazione logopedica ( studio in cieco )  . al fine di correlare il dato clinico con quello logopedico e videfluorografico abbiamo utilizzato la classificazione della disfagia di waxmann [ 7 ] ( tabella 2 ) nella quale ogni paziente ha un grado differente di disfagia ( 7 livelli ) a seconda di dati clinici ( disfagia pi o meno grave , allungamento del tempo del pasto , stato nutrizionale ) , valutazioni logopediche ( presenza / assenza del riflesso della tosse , presenza e entit della tosse volontaria , capacit di apprendimento delle tecniche di deglutizione e possibilit di compenso ) e risultati dellesame videofluorografico ( presenza / assenza di aspirazione , aspirazione di una o pi consistenze , entit del materiale aspirato , presenza del riflesso tussigeno )  . 
su questa base tutti i pazienti sono stati classificati in 7 livelli di disfagia e , di conseguenza , si selezionata la tipologia di nutrizione pi opportuna suddivisa come segue : dieta libera ; dieta con limitazioni ( dieta semisolida omogenea con restrizione di liquidi ; dieta semiliquida a maggiore contenuto idrico rispetto alla prima ) ; nutrizione non orale ( peg o sondino naso - gastrico )  . durante il ricovero i pazienti sono stati sottoposti a training logopedico oltre che a programma riabilitativo mirato anche al recupero della postura e in alcuni casi ( pazienti con aspirazione ) a rivalutazione videofluorografia . 
sulla base dellevoluzione clinica e del grado di recupero ottenuto si valutata , allatto della dimissione , la possibilit di modificare lapproccio nutrizionale avuto durante il ricovero . risultati i risultati della valutazione logopedica hanno fatto rilevare il sospetto di disfagia con aspirazione ( tosse , voce gorgogliante , desaturazione , rialzo termico , senso di soffocamento ) in 29 / 47 pazienti ( 61 , 7% ) mentre nei restanti casi erano presenti alterazioni della fase orale e faringea della deglutizione in assenza di segni che facessero sospettare la presenza di aspirazione . la videofluorografia ha confermato la presenza di aspirazione in 21 / 47 pazienti ( 44% ) : il confronto fra i dati della videofluorografia e quelli della valutazione clinico - logopedica ha fatto rilevare che solo in 17 casi il sospetto clinico di aspirazione stato confermato , mentre in 4 casi ( 8% ) lesame radiologico ha dimostrato la presenza di aspirazione non sospettata clinicamente . 
in 13 / 47 ( 28% ) pazienti la videofluorografia ha dimostrato la presenza di alterazioni della fase orale ( 3 pz ) o della fase faringea ( 3 pz ) o di entrambe ( 7 pz ) , ma senza segni di aspirazione silente . 
nei restanti 13 / 47 ( 28% ) pazienti la videofluorografia non presentava alterazioni della dinamica deglutitoria . sulla base della valutazione clinica e radiologica alla ammissione stata effettuata la classificazione waxmann del grado di disfagia dei pazienti e si sono adottate le seguenti strategie nutrizionali : 1 . 
in 1 / 13 patients , despite the lack of vfss evidence of significant swallowing alterations , the presence of cognitive alterations and the minimal autonomy related to psychophysical deficit suggested placing the patient on a semisolid diet with restrictions on solids ; at the end of the rehabilitation period , with the return of a certain degree of autonomy , the patient was placed on a free diet . 
two other patients , one of whom admitted with an in situ tracheostomy cannula and the other with a peg , followed a diet with a restriction of some consistencies ( in the patient with tracheostomy cannula ) and mixed ( via the peg and oral with restrictions ) during their hospital stay as a precautionary measure and to enable their return to an adequate nutritional state . 
the 13 patients with alterations of the oral and / or pharyngeal phase of swallowing but without silent aspiration were classified as grades 2 ( nine patients ) and 3 ( four patients ) and placed on a diet with restrictions of some consistencies . 
22 penetrazione laringea sub - epiglottica con presenza di mezzo di contrasto anche nel ventricolo di morgagni ( rischio di aspirazione ) ; ristagno di mdc in faringe . classificazione di waxmann sono stati trattati come segue : 10 / 13 pazienti sono stati lasciati in dieta libera . 
in 1 / 13 pazienti - pur non essendovi evidenza videofluorografica di alterazioni deglutitorie significativela presenza di alterazioni dello stato cognitivo e la scarsa autonomia legata al deficit psico - fisico ha suggerito di porre il paziente a dieta semisolida omogenea con limitazione dei solidi ; al termine del periodo riabilitativo , con il recupero di un certo grado di autonomia il paziente stato posto a dieta libera . 
altri 2 pazienti erano portatori di cannula endotracheale e peg al momento della ammissione ; durante la degenza si effettuata una alimentazione con limitazione di alcune consistenze ( nella paziente con cannula endotacheale ) e mista ( attraverso la peg e orale con limitazione ) a scopo precauzionale e per consentire il recupero dello stato nutrizionale . 
i 13 pazienti che presentavano alterazione della fase orale e / o faringea della deglutizione ma senza fenomeni di aspirazione silenziosa sono stati classificati nei livelli 2 ( 9 pz ) e 3 ( 4 pz ) della classificazione di waxmann e posti in dieta con limitazione di alcune consistenze . 
i 21 pazienti con aspirazione silenziosa venivano classificati come segue : 1 pazienti venivano classificati nei livelli 5 ( 4 pz ) ( fig . 2 ) e 4 ( 7 pz ) della classificazione di waxmann ; 10 di questi pazienti venivano posti allatto del ricovero a dieta con limitazione e alla dimissione 2 venivano posti a dieta libera . 
44 aspirazione di mezzo di contrasto con opacizzazione della trachea . stay while one patient had the peg removed after rehabilitation and at discharge was placed on a diet with restrictions . 
interrupting artificial feeding in the remaining six patients , even after rehabilitation , was not possible . discussion the role of videofluorography in identifying swallowing alterations has been codified in a number of studies [ 46 , 8 ] , which also demonstrated how the examination is crucial for revealing aspiration , particularly aspiration not followed by the cough reflex ( silent aspiration )  . 
a relatively large case series also recently demonstrated how the risk of developing pneumonia is closely correlated with the degree of swallowing dysfunction appreciable at vfss ; in fact , the risk of contracting pneumonia in such patients was calculated to be four times greater than in patients with normal swallowing in the event of laryngeal penetration , ten times greater in the event of aspiration and 13 times greater in the event of silent aspiration [ 9 ]  . 
this is why the type of dysphagia needs to be classified on the basis of degree and type of penetration or aspiration of contrast material so as to identify the type of diet the patient should maintain to avoid severe respiratory complications . over the years , a number of different scales have been developed to assess the degree of dysphagia , which take into account the findings of videofluorography : the waxman scale [ 7 ] , the rosenbek penetration - aspiration scale [ 10 ] ; the ott scale , which distinguishes four levels of dysphagia ( 03 ) [ 11 ] ; and the daniels scale , with five increasing levels of dysphagia ( 05 ) [ 12 ]  . 
of all of these , the waxman scale [ 7 ] appeared to be the most useful in that it correlates vfss findings to the degree of dysphagia and then to the type of diet the patient can maintaindeed , careful classification of the patients enabled us to place the clinical and vfss findings in one of the seven waxman degrees of dysphagia and zienti come il rischio di sviluppare polmoniti sia strettamente correlato al grado di disfunzione della deglutizione apprezzabile alla valutazione videofluorografica ; in particolare il rischio di polmonite stato quantizzato , rispetto ai pazienti con deglutizione normale , in 4 volte superiore in caso di penetrazione laringea , 10 volte superiore in caso di aspirazione e 13 volte superiore in caso di aspirazione silenziosa [ 9 ]  . da quanto sopra deriva la necessit di classificare il tipo di disfagia sulla base della entit ed il tipo di penetrazione o aspirazione del mdc cos da individuare correttamente il tipo di alimentazione che il paziente deve mantenere per evitare gravi complicanze respiratorie . 
 da questo punto di vista nel corso degli anni sono nate diverse scale di valutazione del grado di disfagia che tengono conto dei reperti videofluorografici : la scala penetrazione - aspirazione di rosenbek [ 10 ] , la scala di ott che distingue quattro livelli di disfagia ( 03 ) [ 11 ] e la scala di daniels in cinque livelli crescenti di disfagia ( 05 ) [ 12 ]  . tra tutte , la scala elaborata da waxmann [ 7 ] ci sembrata pi utile in quanto correla i reperti videofluorografici al grado di disfagia e , successivamente , al tipo di alimentazione possibile . 
lattenta classificazione dei pazienti ci ha consentito , infatti , di inquadrare i reperti videofluorografici e clinici in una delle sette categorie di waxmann e di impiegare le indicazioni dietetiche previste , in quasi tutti i casi . dalla nostra esperienza risulta chiaro che il ruolo dellesame videofluorografico fondamentale nel management del paziente disfagico in quanto consente un preciso grading dellalterazione il che influenza strettamente la gestione nutrizionale e la scelta tra alimentazione orale e non orale . si possono , inoltre , trarre alcune considerazioni : 1 . 
 our findings clearly demonstrate the crucial role of vfss in the management of the dysphagic patient in that the study enables precise staging of the alteration , which directly influences dietary management and the choice between an oral or artificial diet . 
vfss enabled patients with aspiration to be identified with extreme certainty and greater accuracy than the clinical assessment ( 17 aspirations out of the 29 suspected ) ; our data confirm the findings in the literature [ 46 ] with regard to the ability to identify aspirations in the absence of clinical suspicion , as occurred in four patients in our study . 
the possibility of radiologically reassessing the patient before discharge and thus monitoring the degree of recovery from dysphagia offers promise in identifying the type of diet the patient will be able to maintain at home at the end of rehabilitation . conclusions we feel that our findings demonstrate the central role of vfss in classifying the degree of dysphagia , the knowledge of which influences dietary management of the patient affected by neurological deficit . 
nonetheless , since complex patients are involved , at times with severe cognitive deficit and a limited degree of autonomy , the dietary and rehabilitative approach needs to be carried out ad hoc through the assessment of a multidisciplinary team in which the radiologist is a vital member . 
tuttavia in alcuni casi lapproccio suggerito stato modificato sulla base del grado di deficit cognitivo generale del paziente , del grado di autonomia nella gestione complessiva dellalimentazione e dello stato nutrizionale complessivo al momento della ammissione in reparto . 3 la possibilit di rivalutare radiologicamente il paziente prima della dimissione e monitorare cos il grado di recupero della disfagia appare uninteressante potenzialit ai fini della individuazione della tipologia di nutrizione che il paziente potr mantenere al domicilio al termine del trattamento riabilitativo . conclusioni riteniamo che la nostra esperienza sia dimostrativa del ruolo centrale dellesame videofluorografico della deglutizione nella classificazione della entit della disfagia il che condiziona la gestione nutrizionale del paziente affetto da deficit neurologico . tuttavia , poich si tratta di pazienti complessi , con a volte grave deficit cognitivo e limitazione del grado di autonomia , lapproccio nutrizionale - riabilitativo dovr a volte essere fatto ad hoc tramite valutazione di una equipe multidisciplinare di cui il radiologo deve assolutamente fare parte . 
berletti minerva medica , torino ( 2006 ) isbn 88 - 7711 - 525 - 4 published online : 8 september 2006 scrivere il referto di un esame radiologico una vera arte , un compito certamente pi difficile di quanto possa sembrare . 
in effetti possiamo dire che oggi pi che mai il referto il vero atto medico del radiologo . gli autori , e in particolare schiavon , si sono resi conto di questa importanza e da anni hanno dedicato allargomento interventi , pubblicazioni varie e hanno anche organizzato un congresso . 
dalla palma , presidente della sirm , e con una breve nota di ringraziamento , nella quale impressiona il gran numero di personalit e strutture intervistate e coinvolte nella redazione del testo : esponenti del mondo della filosofia , della psicologia , della scienza delle formazioni , un italianista di fama nazionale e televisiva , esperti di fisica , di medicina legale e un buon numero di esponenti del mondo manageriale . 
naturalmente sono quelli che maggiormente attirano lattenzione , linteresse e la curiosit del lettore , il quale improvvisamente si accorge di essere completamente coinvolto e intento a cercar di capire dove , quale , di che tipo lerrore , e... 
dalla modalit di impostazione del referto , dallimpiego di alcune espressioni si pu , ad esempio , riconoscere un radiologo veneto discendente dal mitico lenarduzzi e differenziarlo da un radiologo lombardo discendente dal maestro ratti o da un ligure discendente dallancor pi mitico vallebona vi sono espressioni , create e care ai nostro maestri , che , con tutta la buona volont non si riescono a sradicare . 
e cos riaffiorano ( anche nel testo che leggiamo ) le ombre ( lombra cardiaca , lombra mediastinica , lombra renale , lombra dellilo ) o gli emidiametri destro e sinistro del cuore . 
le ombre andavano bene ai tempi di busi e di balli , quando il radiologo , immerso nel buio pi completo della sala , scrutava sullo schermo radioscopico e vedeva soltanto e veramente delle ombre . 
quelle che abbiamo oggi sono splendide immagini chiarissime , spesso multiplanari o addirittura tridimensionali , che ci portano in un mondo completamente diverso da quello del bellissimo libro dei cacciatori di ombre di donizetti . 
e i diametri ! i diametri ci riconducono ai tempi fumosi , complicatissimi e spesso inconcludenti di alcuni dei grandi maestri come perona , palmieri o cignolini , in cui il radiologo era costretto a basarsi su queste misurazioni complesse e difficili , che non portavano mai a qualche cosa di clinicamente sicuro . 
oggi , che sul cuore sappiamo praticamente tutto , un buon radiologo deve avere il coraggio di parlare di ventricolo , di atrio , di aorta , di arteria polmonare . questopera inoltre ricca di dati ed elementi utili , di osservazioni critiche , di spunti che costringono a riflettere e a pensare , esposti sempre in maniera chiara e originale . 
non v dubbio che la conoscenza dei dati clinici e degli essenziali elementi anamnestici con un chiaro quesito da parte del medico possono influenzare e orientare in maniera determinante la stesura del referto e il giudizio diagnostico finale . 
gli autori riportano da schopenhauer che : non vi nulla di pi facile che scrivere in modo che nessuno possa capire , come nulla pi difficile che esprimere pensieri significativi in modo che ognuno possa comprenderli e da calvino che parlare oscuramente lo sa fare ognuno , ma chiaro pochissimi . 
opportuno avere sempre presente il referto deve essere chiaro , corretto , conciso , completo , coerente e competente , alle quali aggiungono una settima c , condiviso . nel testo che segue ognuno di questi punti viene analizzato , criticato , commentato ed esemplificato in maniera esauriente e originale . 
facile comprendere lestrema importanza di questo capitolo e la grande utilit che pu avere la sua analisi e la conoscenza di ogni risvolto che pu avere nellesercizio della nostra professione . 
attraverso una serie di utili consigli vengono esposti e analizzati problemi medicolegali che possono riguardare lattivit del radiologo , espressa proprio nella sua manifestazione pi importante : la refertazione dellesame . si deve sottolineare che tutto quanto fin qui esposto riguarda non soltanto gli esami radiologici tradizionali , ma anche le nuove metodiche , come lecografia , la tc e la rm . alla fine del libro viene proposto un capitolo di suggerimenti , nel quale i diversi principi esposti vengono book review riassunti e considerati in senso generico . 
auflage ( volume della serie rrr referenz - reihe radiologie ) gabriele benz - bohm ( ed ) georg thieme verlag , stuttgart , new york ( 2005 ) isbn 3 - 13 - 107492 - 2 published online : 8 september 2006 questo volume della serie rrr referenz - reihe radiologie ( collana di riferimenti radiologici ) giunto alla sua seconda edizione e , da quanto precisato nell ' introduzione da parte della curatrice , risulta molto ampliato rispetto alla prima . 
diviso in 10 capitoli ( caratteristiche della tecnica e delle radiazioni ; anatomia speciale del prematuro ; scheletro ; torace e mediastino ; apparato digerente ; apparato urinario ; ecografia speciale ; rmn ; tac ; angiografia ed interventistica ) , scritti dalla " crema " dei radiologi pediatrici tedeschi , il volume affronta i vari temi di questo delicato settore della radiologia , offrendo al lettore una descrizione precisa e sintetica della materia e divenendo cos opera di riferimento giornaliero , che evita spesso il ricorso a trattati pi ampi dedicati alla materia . il testo , nella sua sinteticit in grado di fornire con grande precisione i cardini dell ' argomento , correlato da tabelle di sintesi e da incisi a lato della pagina , ben indicati da frecce e caratteri evidenziati in blu , in cui vengono sintetizzati i punti fondamentali relativi all ' argomento trattato . di grande utilit pratica risultano le tre pagine in cui vengono raccolte , prima dellindice del volume , tutte le abbreviazioni utilizzate successivamente nel testo , evitando cos il rompicapo che le stesse possono provocare nel loro riscontro . le immagini sono riprodotte con la precisione e bellezza spettacolare , di cui si fa vanto la casa editrice , siano esse in bianco e nero o a colori : molto belli e dettagliati anche i disegni , esplicativi o di sintesi di particolari situazioni , nonch le tavole anatomiche . ogni capitolo correlato da una bibliografia sintetica , che consente di ulteriormente ampliare quanto descritto nello stesso . l ' indice analitico , infine , permette di individuare con immediatezza gli argomenti ricercati . questo volume pu essere considerato un testo di riferimento e pertanto denominarlo bigino risulterebbe termine assai riduttivo . 
ad esempio , delle 100 pagine in cui viene trattato lo scheletro , ben 17 si occupano del grave e sempre pi ricorrente problema del bambino maltrattato , in tutte le sue sfaccettature . notevole parte , inoltre , dedicata , non solo all ' ecografia , ma soprattutto alla rm , in particolare nello studio dell ' encefalo . 
sono sicuro che , qualora tradotto in italiano o inglese , la diffusione dello stesso sarebbe veramente significativa , proprio per le sue caratteristiche di sintesi , precisione e corretta spiegazione della materia . 
passariello1 1dipartimento di scienze radiologiche , 2dipartimento di chirurgia toracica , universit degli studi la sapienza , viale regina elena 324 , i - 00161 roma , italy correspondence to : f . 
nine patients with emphysema were studied by low - dose chest mdct ( 64 - slice somatom sensation cardiac , siemens ) with a collimation of 64x0.6 mm and a slice thickness of 1 mafter treatment , mdct scans were repeated at 7 and 30 days . 
volume assessment at 30 days showed a 29% reduction in rul volume in patient a , a 15% reduction in patient b , a < 1% reduction in patient c and a 30% reduction in patient d . 
in patients undergoing endobronchial valve placement , mdct with dedicated software allows for a better evaluation of volume reduction of a single lobe and of the whole lung . key words lung volumetric assessment endobronchial valve placement mdct emphysema riassunto obiettivo . 
nove pazienti con enfisema sono stati sottoposti a un esame tcms a bassa dose , ( somatom sensation cardiac , siemens , 64 strati ) : collimazione 64x0 , 6mm ; spessore di strato 1 mdopo il trattamento , lindagine tc stata ripetuta a distanza di 7 e 30 gg . 
quattro pazienti , ( a - d ) , in cui la tc ha evidenziato una maggior condizione enfisematica a carico del lobo superiore di destra ( lsd ) , sono stati sottoposti a sve . 
la valutazione volumetrica con tcms , in pazienti sottoposti a sve , effettuata con software dedicato , consente di valutare leffettiva rvp sia globale che per singolo lobo . parole chiave volumetria polomonare by - pass valvolari endobronchiali tcms enfisema f . 
its pathophysiology is characterised by dilatation of air spaces distal to the terminal bronchioles , and it is determined by irreversible , destructive changes in the alveolar walls [ 13 ]  . 
lung transplant provides better long - term results , but the number of organ donors is inadequate , and the selection of suitable candidates is problematic ( advanced age or concomitant disease ) [ 79 ]  . 
lung - volume reduction surgery ( lvrs ) aims to reduce total lung volume by 20%30% , thus improving chestwall elastic recoil ; however , this method presents the obvious limitation of subjecting patients , who are often elderly and with evident restrictive ventilatory defects , to a major surgical operation [ 4 ]  . 
more recently , several authors have suggested a less invasive procedure known as bronchoscopic lung - volume reduction ( blvr ) , which involves the placement of valves inside the bronchi leading to the most affected lobe . this procedure is both highly reliable , with low intraand postoperative morbidity and mortality , and reversible in that the valves may be removed at any time [ 10 ]  . 
it is thought that the implantation of one - way endobronchial valves allows the air to flow out but not to flow in , resulting in collapse of the nonventilated parenchyma [ 11 , 12 ]  . 
the aim of our study was to assess with a 64 - slice ct scanner lung - volume changes in patients undergoing blvr and to correlate these data with spirometric tests in order to confirm the true clinical benefits of the procedure . 
 materials and methods patient selection between june and september 2005 , nine men aged 6070 years referred to us from the department of thoracic surgery and respiratory medicine were studied by low - dose multislice chest computed tomography ( ct )  . 
the reason for referral was to evaluate the extent of emphysema to assess eligibility for endobronchial - valve placement ( emphasys endobronchial valve , redwood city , ca , usa )  . 
selection criteria for valve placement were severe limitation in daily activities despite adequate medical therapy , severe dyspnoea , radiological evidence of heterogeneous emphysema , forced expiratory volume in 1 s ( fev1 ) < 35% after administration of bronchodilators , residual volume ( rv ) > 180% and age lenfisema polmonare rappresenta una delle principali cause dinvalidit e di mortalit del mondo occidentale ; la fisiopatologia caratterizzata dalla dilatazione degli spazi aerei posti distalmente ai bronchioli terminali e determinata da alterazioni distruttive irreversibili delle pareti alveolari [ 13 ]  . 
ne consegue una riduzione della compliance polmonare e del ritorno elastico della parete toracica , che si manifesta con uniperinflazione aerea e un allungamento della fase espiratoria . il trattamento per via chirurgica principalmente rappresentato dal trapianto polmonare e dalla riduzione volumetrica del lobo maggiormente affetto [ 46 ]  . 
entrambe le metodiche presentano dei limiti ; il trapianto garantisce migliori risultati a lungo termine , ma subordinato allinadeguato numero di donatori di organi e alla difficolt di selezionare dei possibili candidati allintervento ( et avanzata o patologie concomitanti ) [ 79 ]  . 
la riduzione volumetrica polmonare per via chirurgica , ha come intento quello di poter ridurre il volume polmonare totale di circa il 20%30% , migliorando in tal modo il ritorno elastico della parete toracica ; tuttavia essa presenta lovvio limite di dover sottoporre un paziente , spesso anziano e con una evidente patologia restrittiva polmonare , ad un severo intervento chirurgico [ 4 ]  . recentemente diversi autori hanno proposto un intervento meno invasivo , rappresentato dallo stenting valvolare per via endobronchiale , eseguito con posizionamento di valvole allinterno dei bronchi del lobo maggiormente affetto . 
tale intervento si presenta molto affidabile , con bassa morbilit e mortalit intra e post operatoria e in pi reversibile , dal momento che le valvole possono essere rimosse in qualsiasi momento [ 10 ]  . 
ipoteticamente lapplicazione per via endobronchiale di valvole unidirezionali ( blvr , bronchoscopic lung volume reduction ) , consente allaria di uscire , ma non di entrare , determinando un collabimento del parenchima disventilato [ 11 , 12 ]  . 
lo scopo del nostro studio stato quindi di valutare , utilizzando una apparecchiatura tc a 64 strati , le modificazioni volumetriche nei pazienti trattati e di correlare tali dati con le prove spirometriche , per poter verificare il reale beneficio clinico . materiali e metodi selezione dei pazienti nel periodo compreso tra giugno e settembre 2005 , 9 pazienti , tutti uomini di et compresa tra i 60 e 70 anni , provescanning protocol procedura chirurgica between 35 and 75 years . 
exclusion criteria included radiological evidence of homogeneous emphysema and isolated bullae , being a smoker , paco2 > 50 mmhg , dlco < 20% , productive cough , and small airway disease . 
efficacy of the intervention was assessed by multidetector - row ct ( mdct ) scans repeated 7 and 30 days after the procedure to evaluate lung - volume reduction , and by spirometry and the 6 - min walking test , to evaluate clinical improvement . 
correct positioning was then checked by fibreoptic bronchoscopy . examinations were performed with a 64 - slice ct scanner ( somatom sensation cardiac 64 , siemens ag , forchheim , germany ) with 32 detectors and a gantry rotation speed of 33 ms . 
images were then reconstructed with the combi ( combined reconstruction ) protocol : one with a 1 - mm slice thickness , 1 - mm reconstruction interval and the b70 reconstruction algorithm to assess lung parenchyma , and the other with a 5 - mm slice thickness , 5 - mm reconstruction interval , and the b30 algorithm to study the mediastinuthe raw data sets were all saved on our pacs ( lifeweb ferrania imaging technologies ) for further processing , if needed . image analysis and volume assessment axial images were analysed on a dedicated workstation by a radiologist experienced in chest pathology . 
the preoperative evaluation took into account the presence and distribution of emphysema , establishing : site ( topographic location within the lobes and identification of the most affected lobe ) , features ( centrilobular , panlobular , or paraseptal ) , presence of isolated bullae and possible presence of focal alterations suspicious for malignancy . 
the volume of the most affected lobe and of the entire right and left lung was then calculated . postprocessing was carried out on a dedicated workstation ( vitrea 2.8 , vital images )  . 
il motivo della richiesta era la valutazione della patologia enfisematosa di cui erano affetti , al fine di valutare lidoneit allintervento di posizionamento di valvole endobronchiali ( emphasys endobronchial valve , redwood city , ca )  . 
i criteri di inclusione per lo stenting valvolare prevedevano una severa riduzione dello svolgimento delle attivit quotidiane , nonostante una adeguata terapia medica , dispnea severa , valutazione radiologica di enfisema eterogeneo , fev1 < 35% dopo somministrazione di broncodilatatori , vr > 180% , et compresa tra 35 e 75 anni . 
i criteri di esclusione prevedevano evidenza radiologica di enfisema omogeneo e di bolle aeree isolate , lessere fumatore , paco2 > 50 mmhg , dlco < 20% , tosse produttiva , malattia delle piccole vie aeree . lo stesso esame era poi eseguito a distanza di 7 e 30 giorni dopo lintervento , contemporaneamente a test clinici , quali la spirometria e il test del cammino in 6 min , per verificare lefficacia dellintervento , valutabili a livello radiologico con una riduzione del volumi polmonari e a livello clinico con un miglioramento della sintomatologia . il protocollo per lintervento di stenting valvolare per via endobronchiale stato precedentemente approvato dal comitato etico . 
i pazienti sono stati informati adeguatamente e in anticipo sulla possibilit , che se la procedura per via endobronchiale fosse fallita , la riduzione volumetrica per via chirurgica sarebbe rimasta come ultima scelta . 
tutti i pazienti sono stati sedati con lidocaina per prevenire linsorgenza della tosse . attraverso il broncoscopio sono stati individuati i bronchi segmentali target , su cui attraverso un catetere guida , sono state posizionate le valvole . 
il paziente , al momento dellesame , stato invitato a sdraiarsi in posizione supina sul lettino con le braccia dietro la testa ed stato informato sulla necessit di dover mantenere unapnea respiratoria per pochi secondi . 
i parametri tecnici di acquisizione dello studio utilizzati sono stati su tutti i pazienti : collimazione 64x0 , 6 mm , spessore di strato 1 mm ; al fine di ridurre le radiazioni ionizzanti stata eseguita una scansione care dose , per la modulazione automatica della dose in base alla diversa attenuazione corporea . 
1a axial computed tomography ( ct ) image : postprocessing on the dedicated workstation ( vitrea 2.8 , vital images ) to evaluate right upper lobe volume by manual tracing of the lobe profile ( arrow )  . 
1a immagine assiale tc , fase di postprocessing eseguita su workstation dedicata ( vitrea 2.8 , vital images ) ; elaborazione del volume polmonare del lobo superiore del polmone destro , con traccia manuale del profilo del lobo ( freccia )  . 
in ogni caso i dati grezzi sono stati salvati sul nostro sistema pacs ( lifeweb ferrania imaging technologies ) , per successive eventuali elaborazioni . analisi delle immagini e valutazione volumetrica le immagini assiali sono state analizzate su una workstation dedicata , da un radiologo esperto di patologia toracica . 
la valutazione pre - operatoria ha preso in considerazione la presenza e la distribuzione dellenfisema in maniera qualitativa , distinguendo : sede ( localizzazione topografica nei lobi e lobo maggiormente colpito ) , caratteristiche ( centrolobulare , panlobulare e parasettale ) ; presenza di bolle isolate ; eventuale presenza di alterazioni focali sospette per essere di natura eteroplasica . 
successivamente stato effettuato il calcolo della volumetria per il lobo maggiormente affetto dallenfisema e per lintero polmone destro e sinistro . la fase di postprocessing stata eseguita su una workstation dedicata ( vitrea 2.8 , vital images )  . 
la valutazione post operatoria stata eseguita a distanza di 7 e 30 giorni ed ha preso in considerazione la valutazione della riduzione volumetrica ed eventuali patologie infiammatorie , secondarie allintervento ( processi broncopneumonici ) , oltre che la presenza di pneumotorace . risultati nella valutazione pre - operatoria lindagine tc ha confermato la presenza di enfisema in tutti i pazienti . 
in 6 la distribuzione stata prevalente a carico del lobo superiore del polmone di destra ; in 2 a livello del lobo superiore di sinistra , in 1 a livello del lobo inferiore destro . 
in 7 pazienti le caratteristiche morfologiche hanno evidenziato un tipo di enfisema di natura panlobulare ; in 1 paziente il riscontro prevalente stato di tipo parasettale ( anche se con alcune aree a carattere panlobulare ) ; in 1 paziente lenfisema stato definito come centrolobulare . 
in 3 pazienti sono state identificate bolle isolate ; in due pazienti localizzate a livello controlaterale rispetto il polmone maggiormente affetto ed in 1 paziente a livello del lobo inferiore , mentre la maggiore fig . 
isolated bullae were identified in three patients : in two , they were contralateral to the most affected lung ; in one , they were in the lower lobe whereas the emphysema was prevalently distributed in the ipsilateral upper lobe . in one patient , a spiculated nodular formation was detected , which was considered to be suspicious for malignancy . 
 in agreement with the thoracic surgeons , only five patients were considered eligible for treatment ; in four of them , preoperative evaluation indicated panlobular emphysema , with prevalent distribution in the right upper lobe ; in one patient , image analysis identified paraseptal emphysema , most prominent in the left upper lobe . 
in un paziente si riscontrata una formazione nodulare a margini spiculati , considerata sospetta per essere di natura eteroplasica . in accordo con i chirurghi toracici , in base ai criteri di inclusione precedentemente esposti , sono stati cos sottoposti a trattamento unicamente 5 pazienti ; in quattro la valutazione pre - operatoria ha dimostrato un enfisema con caratteristiche di tipo panlobulare e con maggior estensione a carico del lobo superiore di destra , cos sottoposto a trattamento ; in un paziente lanalisi delle immagini ha messo in evidenza un enfisema di tipo parasettale , pi evidente a livello del lobo superiore di sinistra . 
non si sono riscontrate invece modificazioni volumetriche per lintero polmone e per il polmone controlaterale . negli stessi pazienti stato rilevato un miglioramento delle condizioni cliniche , del fev1 , del volume residuo ( vr ) e della capacit polmonare totale ( cpt )  . 
i risultati dei dati volumetrici ed il confronto con i risultati spirometrici del pre e post trattamento sono riportati in tabella 2 e nella figura 4 . discussione lintroduzione nella pratica clinica della tc multistrato consente di ottenere in ununica apnea respiratoria informazioni su tutto il parenchima polmonare , con una alta qualit di immagine e con possibilit di un imaging isotropico e volumetrico . 
lelevata risoluzione spaziale con strati contigui consente , infatti , di delineare lanatomia polmonare e di poter ottenere informazioni volumetriche con eccellente dettaglio anatomico fornendo al radiologo ed al clinico importanti informazioni aggiuntive rispetto allutilizzo delle immagini 2d . 
la possibilit inoltre con le apparecchiature di ultima generazione di modulare la dose , ottenendo valori di esposizione poco pi alti di un esame radiografico standard , pone lindicazione per un utilizzo routinario della tc in molte applicazioni e nella valutazione dellenfisema [ 15 ]  . diversi autori hanno , infatti , valutato lutilizzo della tc nella identificazione , caratterizzazione e valutazione preoperatoria dei pazienti con enfisema [ 5 , 16 ]  . 
3a , b axial computed tomography ( ct ) images a before and b after endobronchial valve placement in a patient with severe emphysema predominant in the right upper lobe . 
3a , b immagini assiali tc : prima ( a ) e dopo 7 gg ( b ) dallintervento di inserimento di valvole endobronchiali in paziente con enfisema pi evidente in corrispondenza del lobo superiore destro . 
possibile evidenziare il progressivo collasso del lobo superiore ( punta di freccia ) , con relativo spostamento anteriore della grande scissura ( freccia )  . 2500 2000 1500 1000 fev 1 ( l / s ) cv ( l ) vt6m vol ( cc ) paz a paz b paz c paz d paz a paz b paz c paz d fig . 
4a , b rappresentazione grafica dellandamento del fev1 , della cv ( a ) , del walking test e del volume polmonare ( b ) nei pazienti sottoposti a trattamento valvolare endobronchiale . tire lung or contralateral lung was observed . the patients showed improved clinical condition , fev1 , rv and total lung capacity ( tlc )  . 
results of lung volume assessment and correlation with spirometric tests before and after treatment are shown in table 2 and in figure 4 . discussion the introduction of mdct into clinical practice enables us to study the entire lung parenchyma during a single breathhold with good image quality and the possibility of obtaining isotropic and 3d images . 
the high spatial resolution with lavori in letteratura abbiano dimostrato limportanza di una misurazione volumetrica e funzionale dellenfisema prima e dopo un trattamento di resezione polmonare , poca attenzione stata posta nelle modificazioni volumetriche successive ad un intervento di riduzione volumetrica del lobo affetto eseguita per via endobronchiale [ 4 , 17 , 18 ]  . linnovazione tecnologica nel campo della chirurgia toracica ha consentito , infatti , la creazione di valvole unidirezionali , introdotte per via endobronchiale , che consentono allaria di uscire durante lespirazione , ma non di entrare . lo scopo del nostro studio stato quindi quello di validare la tesi empirica di un collasso parziale del lobo , in cui sono posizionate le valvole con una conseguente riespansione anche del lobo contiguo , non pi sottoposto alleffetto massa di iperinflazione del parenchima trattato . 
nei pazienti sottoposti allintervento stato individuato a distanza di 7 gg una riduzione volumetrica del lobo superiore pari a 26% per a , 24% per b , < 3% per c e 22% per d ; a distanza di 30 gg a ha ottenuto una riduzione totale del lobo superiore di destra table 1 functional assessment before and after bronchoscopic volume lung reduction patient / evaluation f . 
furthermore , the capability of latest - generation devices to modulate the dose so that exposure is only slightly higher than that delivered by standard radiographic equipment supports the routine use of ct in many applications , including the assessment of emphysema [ 15 ]  . several authors have evaluated the use of ct in the identification , characterisation and preoperative assessment of emphysema [ 5 , 16 ]  . 
although recent reports demonstrated the importance of volumetric and functional measurements of emphysema before and after lung - reduction surgery , little pari al 29% , b del 15% , c < 1% e d pari al 30% . 
la valutazione volumetrica del polmone di destra e di sinistra , non ha invece mostrato apprezzabili modificazioni ; ci potrebbe confermare lipotesi di una migliore compliance elastica della parete toracica , conseguenza di una riduzione della compressione locale da parte di parenchima disventilato sul tessuto circostante [ 19 ]  . 
la correlazione con i dati spirometrici ha confermato una evidente riduzione del fev1 , della cv e dei valori del walking test , sia dopo sette , ma soprattutto nel controllo a distanza di 30 gg . non necessariamente come dimostrato dai dati del nostro studio si assiste ad un miglioramento contemporaneo dei parametri di funzionalit respiratoria . 
 technological advances in thoracic surgery have led to the development of one - way endobronchial valves , which allow air to flow out during expiration , but not to flow the aim of our study was to validate the empirical hypothesis that valve placement leads to partial collapse of the affected lobe and consequently to an increase in volume of the contiguous lobe , which is no longer compressed by the hyperinflated parenchyma . 
seven days after the procedure , upper - lobe volumes were found to be reduced by 26% in patient a , 24% in patient b , < 3% in patient c and 22% in patient d ; at 30 days , overall volume reduction of the right upper lobe was 29% for patient a , 15% for patient b , < 1% for patient c and 30% for patient d . volume assessments of the right and left lung did not reveal significant changes ; this could validate the hypothesis that chest - wall compliance improves as a result of the reduction in local compression by the nonventilated parenchyma [ 19 ]  . 
correlation with the spirometric data confirmed a marked reduction in fev1 and vc , and an improvement in the 6 - min walking test results after 7 days and especially after 30 days . 
there is still no certainty of a real and coincident correlation between radiological and clinical data ; for example , a minimal volume change of the right upper lobe in patient c corresponded to a effective clinical response , quantified as a 9% improvement in fev1 , a 70% improvement in vc and an over 90% increase in the distance covered in 6 m however , the actual volume changes and the fact that symptoms , in particular subjective breathlessness , improved confirms the clinical benefit of the technique and supports the use of ct for both the preoperative and postoperative evaluation of patients . 
in our experience , ct allowed for accurate patient selection in terms of not only assessment of emphysema but also detection of concurrent disease that , although decisive for patient selection , may be missed on standard chest radiograph . 
furthermore , the preoperative ct study lazione tra i dati radiologici ed i dati clinici , dal momento che , come dimostrato nel paziente ( c ) alla minima variazione radiologica volumetrica del lobo superiore del polmone di destra , a livello clinico corrisponde una efficace risposta , valutabile con un miglioramento del fev1 pari al 9% , della cv del 70% ed un incremento superiore al 90% nella distanza percorsa nel test del cammino . 
tuttavia il miglioramento sintomatologico , in particolare con una riduzione soggettiva della dispnea , conferma il reale beneficio clinico di questa tecnica , associato alla reale modificazione volumetrica conseguente al trattamento e propongono lutilizzo della tc non solo nella valutazione preoperatoria dei pazienti , ma anche nel post operatorio . nella nostra esperienza personale la tc ha consentito una accurata selezione dei pazienti , sia in termini di enfisema , che di eventuali patologie correlate , spesso non diagnosticate dal semplice esame standard del torace e che invece rappresentano criteri decisionali nellinclusione dei pazienti al trattamento . lo studio preoperatorio con tc ha inoltre permesso di definire con un maggiore grado di sicurezza rispetto al semplice esame radiografico standard le caratteristiche dellenfisema [ 20 ] , il lobo maggiormente colpito e leventuale presenza di bolle aeree isolate o diffuse , anchesse criteri di selezione del paziente al trattamento . in tutti i pazienti il protocollo di studio ha previsto lesecuzione di una tc del torace a bassa dose , sia nella valutazione pre - operatoria , che in quella postoperatoria . 
lutilizzo di un basso dosaggio , cos come riportato da altri autori , limita la qualit di immagine , con conseguente perdita di informazioni in particolare quando si vuol studiare linterstizio polmonare [ 21 ]  . 
sebbene nel nostro studio non sia stata eseguita una valutazione quantitativa sulla qualit di immagine , lutilizzo di un sistema di modulazione automatica della dose , possibile sulla nostra apparecchiatura , ha permesso di acquisire immagini ad alta risoluzione , considerate dal radiologo di buona qualit e comunque adeguata per was more accurate than the chest radiograph in defining the extent of emphysema [ 20 ] , the most affected lobe and the possible presence of isolated or diffuse bullae , which are also selection criteria for treatment . for all patients , the study protocol involved low - dose chest ct both in the preoperative and in postoperative assessment . 
use of low doses , as reported by other authors , reduces image quality , causing loss of data , especially in the study of the pulmonary interstitium [ 21 ]  . 
although our study did not include a quantitative evaluation of image quality , the use of our scanners automatic dose - modulation option made it possible to acquire high - resolution images , which our radiologist judged to be of good diagnostic quality . 
these high - performing scanners are able to acquire images with high spatial resolution during a single 4 - s breath - hold , an especially important consideration in patients with severe emphysema . 
several commercially available systems can now provide immediate volumetric information on lung parenchyma and offer the possibility of automatic segmentation without requiring manual tracing . the application of these systems may prove essential for the assessment of postoperative respiratory function in candidates for surgical or endobronchial volume reduction and in patients undergoing more - extensive lung resections , such as cancer patients . 
few clinical and radiological studies have dealt with this topic , and all of them were conducted on small series ; nonetheless , the results were encouraging not only in terms of surgical and clinical response but also as regards the correlation between mdct and respiratory function tests . 
a second limitation is that , unlike previous authors [ 2224 ] , we made no quantitative evaluation of the extent of emphysema ; however , our patients lung function tests had already revealed a restrictive disorder for which the patients were receiving medication ; in addition , the main aim of our study was to demonstrate the reduction in lung volume following treatment and the advantages of mdct in preand postoperative evaluation of these patients . 
possibile che il progresso tecnologico in termini di apparecchiature consentir , tramite lintroduzione di filtri di convoluzione sempre pi sofisticati , di ridurre ulteriormente la dose , fino a quella di un semplice esame radiografico . 
ultimo punto riguarda il ridotto tempo di scansione ottenibile con una apparecchiatura a 64 detettori e con tempo di rotazione di 0 , 33 secondi . proprio in pazienti con una importante dispnea , lutilizzo di una apparecchiatura cos performante , consente di ottenere immagini in singola apnea di circa 4 secondi , e con elevata risoluzione spaziale . 
allo stato attuale diversi sistemi commerciali consentono di ottenere informazioni immediate volumetriche sul parenchima polmonare , con possibilit di una segmentazione automatica , senza il bisogno di una segmentazione manuale come eseguita nel nostro caso ; lapplicazione di tali sistemi appare essenziale nel calcolo della funzionalit respiratoria post operatoria sia in pazienti che andranno incontro a riduzione volumetrica per via chirurgica o endobronchiale , sia , come gi dimostrato , nei pazienti da sottoporre a resezioni polmonari pi ampie , come nei pazienti con neoplasia . al nostro studio bisogna riconoscere dei limiti ; primo fra tutti la ridotta numerosit della popolazione in studio , che non ha permesso di affrontare una analisi statistica . 
pochi studi clinici e radiologici hanno affrontato largomento ed ognuno con casistiche limitate ; nonostante comunque il piccolo campione studiato , i risultati ottenuti sono stati incoraggianti , sia per la risposta chirurgica e quindi sintomatologica del paziente , sia per la correlazione tra tc multistrato e test respiratori . probabile che un follow - up pi lungo ed un campione pi ampio di soggetti consentir una miglior comprensione fisiopatologica delle modificazioni che si riscontrano nel polmone in corso di enfisema e dopo il trattamento . un secondo limite riguarda la mancanza di valutazione quantitativa del grado di enfisema , cos come riportato da precedenti lavori [ 2224 ] ; tuttavia i pazienti gi presentavano test funzionali che evidenziavano una patologia di tipo ostruttivo , per la quale erano in trattamento medico ; inoltre lo scopo dello studio prevedeva principalmente la dimostrazione della tesi di riduzione volumetrica conseguente al trattamento ed i vantaggi della tecnica di tc multistrato nellimaging pree post - operatorio di questi pazienti . 
anche in questo caso dato il limitato numero di pazienti incluso e quindi la limitata correlazione statistica , un secondo giudizio , peraltro su dati in cui lelaborazione viene effettuata da un software dedicato , non avrebbe probabilmente aggiunto sostanziali modifiche . conclusions technological advances , in particular , 64 - slice scanners , in le innovazioni tecnologiche delle nuove apparecchiature tc in particolare a 64 strati , consentono una accurata definiconclusioni f . 
lung - volume assessment by means of dedicated software , used in addition to spirometry , enables the radiologist to calculate the volume of a single lobe or lung region and to determine the real improvement both in general terms as indicated by spirometry and in the treated parenchyma . 
larger patient populations and longterm follow - up are needed to determine the real benefit of bronchoscopic lung - volume reduction and the real correlation between ct findings and clinical tests . zione pree post - operatoria nei pazienti con enfisema trattati con un nuovo approccio di valvole endobronchiali . 
la valutazione volumetrica effettuata su software dedicati consente inoltre , in aggiunta alla spirometria , di poter effettuare un calcolo per singolo lobo , o regione polmonare , con possibilit di valutare leffettivo miglioramento sia in termini globali , cos come emerge dalla spirometria , ma anche sul parenchima trattato . 
un maggior numero di pazienti ed un follow - up a lungo termine consentir di valutare leffettivo beneficio del trattamento endobronchiale , cos come una pi reale correlazione tra tc e test clinici . radiol med ( 2006 ) 111 : 878 doi 10.1007 / s11547 - 006 - 0084 - 6 ecografia clinica p . 
nei due capitoli dedicati ai mezzi di contrasto in ecografia , vengono trattati i principi fisici , le tecnologie e le metodiche di visualizzazione dei mezzi di contrasto . larticolazione dei capitoli che segue quindi divisa per distretti anatomici . il primo volume dedicato alla testa , al collo e al torace ; in questo volume compreso anche lapparato locomotore . 
nella parte testa , collo e torace sono trattati i capitoli dedicati alle ghiandole salivari , alle malattie diffuse della tiroide , alle neoplasie della tiroide , alle paratiroidi ed ai linfonodi . 
la trattazione del rene , separata dalladdome superiore , nella parte dedicata allapparato urinario , consente una valutazione dinsieme delle patologie delle vie urinarie . nel terzo volume sono trattati lapparato genitale femminile , la pediatria , lapparato vascolare . 
muzzio1 1dipartimento di scienze medico diagnostiche e terapie speciali , 2dipartimento di scienze mediche e chirurgiche , clinica chirurgica 3 , universit degli studi di padova , istituto oncologico veneto , via giustiniani 2 , i - 35128 padova , italy 3dipartimento di radioterapia e medicina nucleare , azienda ospedaliera di padova , istituto oncologico veneto , padova , italy correspondence to : d . 
prognosis and treatment of esophagus and cardia cancer ( ecc ) depend on the precision with which the disease is staged according to the american joint committee of cancer ( ajcc ) criteria . 
imaging modalities normally used in clinical staging are esophagography , esophagoscopy , endoscopic ultrasound ( eus ) , computed tomography ( ct ) and positron emission tomographyct fusion ( ct - pet )  . 
fifty - six patients with ecc diagnosed by x - ray of the upper digestive tract , endoscopy and biopsy were staged using eus , chest and abdomen ct scan , and ct - pet . thirty - four patients in stage ii and 18 patients in stage iii underwent surgery after neoadjuvant chemotherapy ; four patients in stage iv were treated with the positioning of an endoprosthesis after chemoradiotherapy . 
in the 52 patients who had surgery , follow - up included digestive tract x - ray , endoscopy and ct of the chest and abdomen every 68 months for the first 3 years . 
in all 56 patients , endoscopy , eus , ct and ct - pet in combination were crucial in determining the site of disease , locoregional extent and depth of esophageal wall penetration ( t ) , and any involvement of the mediastinal lymph nodes ( n1 ) , extrathoracic lymph nodes ( m1 ) or hepatic metastases . 
in the locoregional staging of ecc before chemotherapy , we were able to differentiate t2t3 from t4 in 40 patients ; t4 disease was found in 12 potentially resectable cases . 
the specificity of ct in detecting small lymph nodes in the mediastinum was less than 50% while for ctpet , it was more than 80% ; eus revealed sensitivity higher than 90% but a low specificity in seven cases . 
le tecniche di imaging in uso nella pratica clinica sono : lesofagografia , lendoscopia , lecoendoscopia ( eus ) , la tomografia computerizzata ( tc ) e la tomografia ad emissione di positroni fusa con la tc ( tc - pet )  . queste metodiche combinate tra loro sono determinanti non soltanto per la diagnosi , ma soprattutto per la stadiazione ed il follow - up dopo trattamenti multimodali . 
cinquantasei pazienti portatori di cec , diagnosticato con esame radiologico del tubo digerente prime vie e con endoscopia con biopsia , sono stati stadiati mediante eus , tc toraco - addominale e tc - pet . 
trentaquattro in stadio ii e 18 in stadio iii hanno eseguito chemioterapia neoadiuvante e poi sono stati operati ; 4 in stadio iv sono stati sottoposti a posizionamento di endoprotesi dopo chemio - radioterapia . 
la endoscopia , la eus , la tc e la tc - pet combinate ci hanno permesso di determinare in tutti i 56 casi la sede , lestensione locoregionale e il grado di infiltrazione della parete dellesofago ( t ) , la presenza di metastasi linfonodali mediastiniche ( n1 ) , extratoraciche ( m1 ) e / o epatiche . 
nella stadiazione loco - regionale del cec prima della chemioterapia si differenziato il t2 - t3 dal t4 in 40 casi ; si evidenziato un t4 in 12 casi solo potenzialmente resecabili . 
per quanto riguarda i piccoli linfonodi metastatici nel mediastino la tc ha dimostrato specificit inferiore al 50% , la tc - pet specificit maggiore dell80% , la eus sensibilit di oltre il 90% ma bassa specificit in 7 casi . 
x - ray of the upper digestive tract and chest and abdomen ct scan are useful in preliminary evaluation of ecc . endoscopy is particularly indicated for evaluating tumour morphology , taking biopsies for a histological diagnosis and the early diagnosis of anastomotic recurrences . 
ct - pet is extremely useful in identifying small mediastinal metastatic lymph nodes ( n1 ) or extrathoracic lymph nodes ( m1 ) and hepatic metastases ( 1 cm ) , which may escape multislice ct . 
pet alone is useful for identifying residual or recurrent tumour in the esophageal wall when an endoprosthesis is in place . key words esophagus and cardia cancer x - ray upper digestive tract endoscopy endoscopic ultrasound computed tomography positron emission tomography ct fusion effettuata mediante endoscopia , eus , tc toraco - addominale e tc - pet nei casi dubbi ha posto la indicazione allintervento chirurgico . 
la tc - pet consente di identificare le piccole metastasi linfonodali intramediastiniche ( n1 ) ed extratoraciche ( m1 ) e le lesioni epatiche di dimensioni 1 cm , non sempre identificabili con la tc anche con la tecnica multistrato . 
la pet da sola trova indicazione nellidentificare persistenza o ripresa di malattia nella parete dellesofago sede di endoprotesi . parole chiave tumore dellesofago e del cardias tubo digerente , prime vie endoscopia eco - endoscopia tomografia computerizzata tomografia ad emissione di positroni - tc introduction introduzione esophagus and cardia cancer ( ecc ) is relatively rare and has a predilection for the male gender . 
in the last 20 years , there have been signs of a considerable increase in the incidence of ecc [ 7 , 8 ] associated with a decline in the epidermoid type ( which tends to affect the median and lower third of the esophagus and is related to alcohol abuse , smoking and vitamin and mineral dietary deficiencies ) and an increase in the proportion of adenocarcinomas , localised mainly in the distal portion and cardia , which develop mainly in barretts epithelium [ 912 ]  . there is no consensus concerning treatment protocols and survival curves for patients suffering from this disease . while patients operated for early squamous cell carcinoma can reach perfectly acceptable 5 - year survival rates of between 57% and 78% , patients with locally advanced disease have a far lower survival rate , ranging from 6% to 14% at 5 years [ 2 , 1315 ]  . 
this is partly due to the fact that more than a third of patients have extensive disease already at diagnosis ( involving the tracheal - bronchial tree , laryngeal nerves , vascular structures and / or regional or remote lymph nodes ) , which usually rules out any radical or even palliative surgery [ 16 ]  . 
after postoperative chemoradiotherapy or neoadjuvant chemotherapy , these patients survive a median of 9 months or so , with 5 - year survival rates of between 20% and 30% in those who have undergone surgery [ 13 , 14 , 1721 ]  . 
negli ultimi 20 anni si notato un notevole aumento dellincidenza del cec [ 7 , 8 ] associato ad una diminuzione del tipo epidermoide ( che interessa preferenzialmente il terzo medio e inferiore dellesofago , legato allabuso di alcol , tabacco e a deficit nutrizionali di vitamine e minerali ) e ad un aumento delladenocarcinoma localizzato principalmente nel tratto distale e nel cardias , che insorge sopratutto su lesione di barrett [ 912 ]  . in letteratura non vi uniformit sui protocolli terapeutici e sulle curve di sopravvivenza dei pazienti affetti da tale patologia . 
se da un lato i carcinomi squamosi early stage operati , possono raggiungere tassi di sopravvivenza accettabili tra il 57% e il 78% a 5 anni , dallaltro pazienti con malattia localmente avanzata hanno bassa sopravvivenza , con un range a 5 anni , che varia dal 6% all14% [ 2 , 1315 ]  . ci in parte dovuto al fatto che oltre un terzo dei pazienti si presenta alla diagnosi oramai con malattia estesa ( interessamento dellalbero tracheo - bronchiale , dei nervi laringei , delle strutture vascolari o dei linfonodi regionali o a distanza ) e non pu essere sottoposto ad un trattamento chirurgico radicale o palliativo [ 16 ]  . 
in questi pazienti , dopo chemio - radioterapia postoperatoria o dopo solo chemioterapia neoadiuvante viene riportata una sopravvivenza mediana intorno ai 9 mesi , con tassi di sopravvivenza a 5 anni d . 
thus , despite significant improvements in diagnostic imaging techniques [ 2232 ] , the advent of new surgical strategies [ 21 ] and new chemotherapeutic preparations [ 3339 ] , the survival rate remains low . 
 this paper discusses the indications for endoscopic ultrasonography ( eus ) , computed tomography ( ct ) , positron emission tomography ( pet ) and ct - pet fusion in pretreatment staging of ecc and in the follow - up after multimodality treatment . 
 materials and methods from january 2002 to september 2005 , 56 patients with ecc came under our observation for a joint surgical and oncological assessment ; 47 were men and nine were women , with an age ranging between 39 and 74 ( mean 63 ) years . 
the ecc was first diagnosed by barium - swallow upper - digestive - tract x - ray ; in the more severe cases with major dysphagia for solid and liquid foods , upper digestive tract x - ray with gastrografin was preferred . 
in all cases , ecc was staged using eus , chest - abdomen ct and ctpet before deciding the type of treatment . eus was performed using 7.5 mhz or 20 mhz probes capable of producing an excellent representation of the five layers of the esophageal wall . 
for ct , we used the spiral technique and 5 - mm slab thicknesses , 5 - mm increments , 3to 2 - mm reconstructions and a pitch of 1.5 after intravenous administration with an automatic injector of 100 ml of iopamiro 370 at a rate of 3 ml / s . 
the last 12 cases were evaluated using a multislice ( 16 - slice ) ct apparatus with the following acquisition parameters : thickness 3 mm , reconstruction index 1 mm , pitch 1.5. 
ct - pet images were acquired after injecting a dose of 710 mci ( 240370 mbq ) of 18 - fluorodeoxyglucose ( fdg ) at intervals of 6090 min with an acquisition time of 4 min / bed , using a ct voltage of 80110 kev , depending on the thickness of the adipose layer . 
image processing and fusion were done automatically using a specific clinical programme . patients were staged as follows : 34 in stage ii , 28 of them in stage iia ( t3 n0 ) and six in stage iib ( t2 n1 ) ; 18 in stage iii ( six t3 n1 and 12 t4 n0 ) ; four in stage iv ( m1 )  . 
the 34 patients ( 61% ) who underwent esophagectomy and the 18 ( 32% ) patients with advanced but potentially resectable disease were given neoadjuvant chemotherapy before surgery . postoperative radiotherapy was provided in 12 cases ( 18 stage iii and four stage ii ) in which there was some doubt as to surgical radicality . 
four patients ( 7% ) were treated with chemoradiotherapy and subsequently fitted with an endoprosthesis because they had hepatic metastases ( three cases ) and extracompartmental lymph node metastases ( three cases ) ; the follow - up tra il 20% e 30% in quelli operati [ 13 , 14 , 1721 ]  . 
la reale efficacia di tali strategie terapeutiche combinate o no non ancora supportata da validi e certi risultati e le linee guida terapeutiche non sono standardizzate [ 14 ]  . 
nonostante , quindi , i significativi miglioramenti delle tecniche diagnostiche di immagine [ 2232 ] , di nuove strategie di approccio chirurgico [ 21 ] e lutilizzo di nuovi preparati chemioterapici [ 3339 ] , la sopravvivenza rimane comunque mediamente bassa . scopo di questo lavoro quello di puntualizzare le indicazioni alla eco - endoscopia ( eus ) , alla tomografia computerizzata ( tc ) , alla tc associata alla tomografia ad emissione di positroni ( tc - pet ) sia nella stadiazione pre - trattamento del cec sia nel follow - up dopo trattamento multimodale . materiali e metodi da gennaio 2002 a settembre 2005 56 pazienti affetti da cancro dellesofago e del cardias , sono occorsi alla nostra osservazione nellambito di una valutazione collegiale chirurgico - oncologica . 
di questi 47 sono maschi e 9 femmine , di et compresa tra 39 e 74 anni con et mediana di 63 anni . il cec stato diagnosticato preliminarmente mediante esame radiologico del tubo digerente dopo assunzione di sospensione di solfato di bario ; nei casi di grave ed importante disfagia per i cibi solidi e liquidi si ritenuto di eseguire lesame radiologico delle prime vie del tubo digerente mediante gastrograf successivamente i pazienti sono stati sottoposti ad endoscopia per la valutazione morfologica del tumore e la diagnosi istologica mediante ago - biopsia . 
in tutti i casi il cec stato stadiato mediante eus , tc toraco - addominale e tc - pet prima di decidere il tipo di terapia . lindagine eus si avvalsa dellutilizzo di sonde da 7 , 5 mhz o 20 mhz in grado di produrre una ottimale rappresentazione dei 5 strati della parete dellesofago . 
la tc si avvalsa della tecnica a spirale con spessore dello strato di 5 mm , con avanzamento di 5 mm e ricostruzioni a 23 mm e con pitch di 1 , 5 , dopo somministrazione endovenosa mediante iniettore automatico di 100 ml di iopamiro 370 alla velocit di 3 ml / s . 
gli ultimi 12 casi sono stati valutati mediante apparecchio tc multistrato ( 16 strati ) con i seguenti parametri di acquisizione : spessore di 3 mm , indice di ricostruzione 1 mm , pitch 1 , 5 . 
le immagini tc - pet sono state acquisite dopo avere iniettato una dose di 710 mci ( 240370 mbq ) di 18 - fdg a distanza di 6090 minuti con un tempo di acquisizione di 4 min / bed , servendosi di un voltaggio della tc di 80110 kv in base allo spessore del pannicolo adiposo . lelaborazione e la fusione delle immagini sono state ottenute in automatico mediante lutilizzo di programma clinico specifico . 
chemotherapy was administered according to the following protocol : 5 - fluorouracil 1 , 000 mg / m2 in continuous infusion on days 1 and 5 ; 100 mg / m2 cisplatin on day 1 , for each cycle of treatment . 
radiotherapy was given in a dose of 45 gy / 25 fr . follow - up involved 52 operated patients and involved endoscopy and chest - abdomen ct every 68 months for the first 3 years . 
ct - pet was performed in 12 cases with a clinical picture and / or morphological signs on ct suspicious of recurrence ( small nodular formations in the intramediastinal lymph nodes , structural irregularities in the liver )  . results in all 56 cases , combining eus , ct and ct - pet enabled us to accurately establish site and locoregional extent of the ecc , degree of infiltration of the esophageal wall and involvement of the mediastinal and / or extracompartmental lymph nodes , as well as identifying any small hepatic metastases all fundamental factors in determining the most suitable treatment and an accurate prognosis . as for cancer site , it was located at the esophagogastric junction in 23 patients ( 41% of the total ) , in the middle thoracic portion of the esophagus in 14 ( 25% of the total ) , the upper thoracic portion in 16 ( 29% of the total ) and in the cervical esophagus in three ( 5% of the total )  . 
in the nodal staging , we differentiated n0 from n1 ( 12 cases ) ; although n1 cases are operable , their prognosis is not good . using ct - pet , we found four cases of small hepatic metastases 0.51.5 cm in size ( three cases ) and extrathoracic lymph node metastases in the subdiaphragmatic region ( three cases )  . 
at the time of reassessment 4 weeks after completing the treatment , three of these patients had persistent esophageal - wall disease demonstrated by pet ( two cases ) and ct - pet ( one case )  . 
 as for the presence of small metastatic lymph nodes in the mediastinum , in 12 n1 cases , ct demonstrated specificity of less than 50% ( five cases ) while ct - pet had a specificity higher than 80% ( ten cases ) ; eus sensitivity was higher than 90% ( 11 cases ) , even for periesophageal lymph nodes less than 1 cm , but its specificity was limited in seven cases ( less than 60% )  . 
quattro pazienti ( 7% ) sono stati trattati con chemio - radioterapia e successivamente sottoposti a posizionamento di endoprotesi in quanto presentavano metastasi epatiche ( 3 casi ) e metastasi linfonodali extracompartimentali ( 3 casi ) ; il follow - up stato eseguito in 2 casi solo mediante pet . 
la chemioterapia stata somministrata secondo il seguente schema : 5 - fluorouracile : 1000 mg / m2 in infusione continua dai giorni 1 e 5 e cisplatino : 100 mg / m2 nel giorno 1 , per ogni ciclo di terapia . 
la radioterapia con il seguente dosaggio : 45 gy / 25 fr . il follow - up stato effettuato nei 52 pazienti operati mediante endoscopia e tc toraco - addominale ogni 68 mesi per i primi 3 anni . 
la tc - pet stata eseguita in 12 casi in rapporto al quadro clinico sospetto e / o allaspetto morfologico alla tc dubbio per recidiva ( piccole formazioni nodulari linfonodali intramediastiniche , disomogeneit della struttura del fegato )  . risultati la eus , la tc e la tc - pet combinate hanno permesso di determinare in tutti i 56 casi con precisione la sede e lestensione loco - regionale del cec , il grado di infiltrazione della parete dellesofago , il coinvolgimento dei linfonodi mediastinici e / o extracompartimentali e di evidenziare anche piccole metastasi epatiche , tutti fattori determinanti per la scelta del trattamento pi idoneo e per una prognosi accurata . per quanto riguarda la sede del cancro in 23 pazienti ( 41% del totale ) la localizzazione era a livello della giunzione esofago - gastrica , in 14 ( 25% del totale ) della porzione toracica media , in 16 pazienti ( 29% del totale ) dellesofago toracico superiore ed in 3 ( 5% del totale ) dellesofago cervicale . 
nella stadiazione delln , abbiamo differenziato ln0 dalln1 ( 12 casi ) ; pur essendo ln1 operabile , la prognosi non buona . abbiamo riscontrato mediante tc - pet la presenza in 4 casi sia di piccole metastasi epatiche 0 , 51 , 5 cm ( 3 casi ) sia di metastasi ai linfonodi extratoracici della regione sottodiaframmatica ( 3 casi )  . 
 preoperative restaging of the 18 patients in stage iii given neoadjuvant chemotherapy ( performed a mean 40 days after completing the treatment ) using endoscopy , eus and ct of the chest and abdomen associated with ct - pet in dubious cases demonstrated good response to chemotherapy in all cases , so this group of patients also underwent surgery . 
 discussion prognosis and treatment of ecc relies on accurate staging according to the criteria of the american joint committee on cancer ( ajcc ) system based on the use of endoscopy , eus , ct and ct - pet [ 1 , 40 ]  . 
the first layer corresponds to the boundary echo and superficial mucosa ; the second to the mucosa , including the muscularis mucosae ; the third to the submucosa ; the fourth to the muscularis propria and the fifth to the adventitia [ 29 , 41 , 42 ]  . 
 ct scan of the chest and abdomen , especially using multislice techniques , was the basic imaging method we used not only for global staging of the tumour ( remote metastases ) but also for an assessment of its spread into the mediastinum . obliteration of the layers of mediastinal fat prior to any neoadjuvant treatment is an important predictor of spread of ecc beyond the esophageal wall . 
mediastinal fat is particularly abundant at the level of the lower third of the esophagus and cardia , where it acts as a sort of barrier to tumour aggression on adjacent anatomical structures , i.e. 
in addition to tumour spread into mediastinal fat , another ( albeit less reliable ) criterion to consider is the craniocaudal extension of the esophageal mass : the greater the extension of the tumour in the sagittal direction , the more likely it is to be a case of t4 ( 12 cases observed )  . even with modern multislice ct techniques , it is not always possible to evaluate infiltration of the vascular structures , and the aorta in particular , with any certainty since endolumento della rivalutazione eseguita a distanza di quattro settimane dalla fine dei trattamenti , persistenza di malattia intraparietale dimostrata con la pet ( 2 casi ) e con la tc - pet ( 1 caso )  . per quanto riguarda la presenza di piccoli linfonodi metastatici nel mediastino , la tc ha dimostrato , su 12 casi n1 , specificit inferiore al 50% ( 5 casi ) , la tc - pet una specificit maggiore dell80% ( 10 casi ) , la eus elevata sensibilit oltre il 90% ( 11 casi ) per i linfonodi periesofagei anche di dimensioni inferiori ad 1 cm , ma bassa specificit in 7 casi ( < 60% )  . 
in 2 casi nel tempo prechirurgico si ottenuta la diagnosi di metastasi linfonodale peritumorale mediante ago - biopsia eus mirata . per quanto riguarda i 3 casi di cec in cui erano presenti linfonodi extracompartimentali metastatici sottodiaframmatici , la tc ha evidenziato piccoli linfonodi ( diametro inferiore a 15 mm ) ma non stata in grado di dimostrare la presenza di eventuali metastasi ben evidenti alla tc - pet . la ristadiazione pre - operatoria dei 18 pazienti in stadio iii sottoposti a chemioterapia neoadiuvante effettuata dopo 40 giorni mediamente dalla fine del trattamento , con endoscopia , con eus e con tc toraco - addominale , associata a tc - pet nei casi dubbi , ha dimostrato in tutti una buona risposta alla chemioterapia per cui anche questo gruppo di pazienti stato sottoposto a intervento chirurgico . la recidiva a livello della anastomosi esofago - gastrica stata identificata in 16 dei 52 pazienti mediante endoscopia associata alla biopsia in un arco di tempo compreso tra i 3 e i 12 mesi . 
il gran vantaggio delleus la sua capacit di evidenziare i singoli strati che compongono la parete esofagea : si ottenuta infatti , nei nostri casi , una precisa rappresentazione dei 5 strati della parete dellesofago . 
va ricordato che il primo corrisponde al limite tra lo strumento e la superficie mucosa , il secondo strato alla mucosa inclusa la muscolaris mucosae , il terzo strato alla sottomucosa , il quarto alla muscolaris propria e il quinto strato allavventizia [ 29 , 41 , 42 ]  . 
so we have to rely on nonspecific signs , such as the degree of deformity in the circumference of the descending aorta or more than 90 of contact between the neoplastic solid tissue and the vessel wall . any involvement of the trachea and / or left main bronchus is ascertained by endoscopy in the absence of endoluminal non solo per una stadiazione complessiva del tumore ( metastasi a distanza ) , ma anche per una valutazione della sua estensione nel mediastino . 
in fact , ct very clearly identified the esophageal mass but failed to distinguish any involvement of peritumoural lymph nodes because , in the absence of planes of cleavage , it was incapable of discriminating neoplastic solid tissue from lymph nodes , which had the same densitometric values . 
any lymph node and hepatic micrometastases less than 1 cm in size of a dubious nature on the ct scan , even using the multislice technique , were easily detected by ct - pet , ruling out surgery for four patients who were treated with chemoradiotherapy alone . 
oltre allo spread tumorale nel grasso mediastinico , un criterio anche se meno valido , potrebbe essere quello della estensione cranio - caudale della massa esofagea : tanto pi esteso in senso sagittale il tumore tanto pi probabile che si tratti di un t4 ( 12 casi osservati )  . 
anche con le moderne tecniche tc multistrato non sempre possibile valutare con certezza la infiltrazione delle strutture vascolari , soprattutto laorta , in quanto non si mai in presenza , come avviene per i vasi venosi , di proliferazioni trombotiche endoluminali . 
bisogna quindi basarsi su segni aspecifici come per esempio il grado di deformazione della circonferenza dellaorta discendente o un contatto superiore ai 90 tra il tessuto solido neoplastico e la parete del vaso . 
il coinvolgimento della trachea e / o del bronco principale di sinistra di pertinenza della endoscopia in assenza di proliferazioni endoluminali , che sono bene evidenziate dalla tc , anche con il concorso della endoscopia virtuale . valutazioni diagnostiche delln leus lunica tecnica in grado di distinguere il tessuto tumorale esofageo dalla linfoadenopatia mediastinica contigua alla massa ( n1 )  . 
diagnostic certainty can come only from direct morphological examination and / or biopsy using endoscopy [ 43 ]  . evaluation of locoregional recurrence identification of locoregional recurrence in the operated cases posed problems of interpretation . 
la tc , infatti , ha evidenziato molto bene la massa esofagea , ma non ha distinto il coinvolgimento dei linfonodi contigui al tumore , in quanto non stata in grado di discriminare , in assenza di piani di clivaggio , il tessuto solido tumorale dai linfonodi che presentavano eguali valori densitometrici . 
piccole metastasi linfonodali e lesioni epatiche inferiori al centimetro , di natura dubbia alla tc anche con la tecnica multistrato , sono state individuate facilmente con la tc - pet , escludendo dalla terapia chirurgica 4 pazienti , sottoposti esclusivamente alla chemio - rafig . 
la certezza diagnostica deriva solo dallaccertamento morfologico diretto e / o bioptico mediante endoscopia [ 43 ]  . valutazione della recidiva locoregionale la identificazione della recidiva locoregionale nei casi operati ha offerto delle problematiche di interpretazione . 
nella nostra casistica quando la recidiva si localizzata a livello della anastomosi ( 16 casi ) , la sua identificazione e valutazione avvenuta prevalentemente per via endoscopica con ago - biopsia anche di piccole irregolarit della superficie mucosa . 
b fluorodeoxyglucose - positron emission tomography ( fdg - pet ) shows gross recurrence of the ecc , with a nodular appearance in the sagittal direction , metastatic lymph nodes in the left clavicular region and small ( 1 - cm ) metastases in the liver ( arrows )  . 
bb la fdg - pet mostra grossolana recidiva del cec con aspetti nodulari in senso sagittale , linfonodi metastatici in regione clavicolare sinistra e piccole metastasi epatiche ( 1 cm ) ( frecce )  . 
bb la fdg - pet rileva piccolo iperaccumulo del tracciante metabolico in corrispondenza della parete laterale destra del tratto esofageo sede dellendoprotesi ( frecce )  . first imaging methods to use for preliminary evaluation of ecc . 
endoscopy is indispensable for a direct view of the tumour , for taking biopsies and thus establishing a histological diagnosis and ensuring early detection of small recurrences at sione diretta del tumore , per il campionamento bioptico e quindi per la diagnosi istologica e per lidentificazione precoce di piccole recidive in sede di anastomosi dopo la chirurgia ; leus per differenziare il t2 - t3 dal t4 , per evidend . 
ct - pet provides morphological and functional information that enables even very small recurrences to be identified and located both in iatrogenic fibrotic periesophageal areas and in lymph nodes and intraand extrathoracic organs . even using the multislice technique , even when ct revealed liver lesions of 1 cm or more , it was unable to determine their benign or malignant nature with certainty . 
each imaging modality has its advantages and limitations , but in combination , they are crucial in determining the most appropriate treatment for patients with ecc . ziare piccoli linfonodi peritumorali e per biopsie mirate . lendoscopia , leus , la tc e la tc - pet combinate trovano indicazione per una precisa stadiazione pre - operatoria , essendo lintervento chirurgico altamente demolitivo . 
la tc - pet infatti , offre informazioni morfologiche e funzionali che consentono di evidenziare e localizzare anche piccole recidive sia nelle aree fibrotiche iatrogene periesofagee sia nei linfonodi e negli organi intra ed extratoracici . la tc , anche nei pazienti valutati con la tecnica multistrato , quando ha dimostrato la presenza di lesioni epatiche del diametro 1 cm non stata in grado di determinare con certezza la natura benigna - maligna di queste . 
the test , consisting of 17 screendetected cancer cases and 133 negative controls , was validated by a panel of expert readers defining a minimum standard as to sensitivity for cancer and recall rate of negative controls . 
radiologist training needs to be considered a priority , at least in those screening programmes that are still to be implemented in one third of the country . key words mammography screening diagnosis proficiency test riassunto obiettivo . 
il test , costituito da 17 casi di carcinomi diagnosticati allo screening e da 133 controlli negativi , stato validato da lettori esperti e prevede di superare uno standard relativo alla sensibilit e al tasso di richiamo a approfondimento tra i controlli negativi . 
laccuratezza misurata al test funzione della esperienza , rilievo non inaspettato , che suggerisce che limpiego corrente in screening di radiologi generalisti , con scarsa esperienza in mammografia e senza un congruo addestramento , dovrebbe essere riconsiderato . laccuratezza al test migliora sensibilmente con laddestramento ( stage formativi e consultazione di casistiche didattiche ) : molti programmi di screening in italia sono stati varati senza che si provvedesse a una adeguata formazione dei radiologi : almeno per i programmi che ancora devono iniziare in un terzo del territorio nazionale auspicabile che la formazione sia un punto di forza . parole chiave mammografia screening diagnosi test di accuratezza s . 
several such tests have been developed over time at the centro per lo studio e la prevenzione oncologica ( cspo ) of florence , and a large number of italian radiologists have been tested , either as a measure of quality control of ongoing national screening programmes , within courses held at cspo or on individual request for self - evaluation purposes [ 13 ]  . the aim of the present study was to review the series of tests taken to assess the success rate and its association to a variety of indicators of reader experience defined at the time of the test . 
however , because requests for the test have been increasing in recent years , probably as a result of the large number of organised screening programmes implemented on a national basis [ 4 ] , the series available for review has grown much larger , allowing for more stable estimates , and deserved a new evaluation . nella istruzione di un nuovo programma e tra i controlli di qualit di un servizio di screening mammografico , uno dei problemi quello di valutare laccuratezza diagnostica dei radiologi . 
diversi test del genere sono stati realizzati nel tempo presso il centro per lo studio e la prevenzione oncologica ( cspo ) di firenze , e ad essi si sono sottoposti nel tempo molti radiologi italiani , sia nellambito di programmi di controllo di qualit di programmi di screening nazionali , sia nel corso di tirocini pratici presso il cspo , sia per autoverifica personale [ 13 ]  . 
scopo dello studio qui riportato stato quello di rivedere la casistica dei test sostenuti , per verificare il tasso di superamento degli stessi , e la correlazione tra superamento e una serie di indicatori di esperienza dei lettori , raccolti in occasione del test . 
dato il notevole incremento della richiesta di sottoporsi al test negli anni pi recenti , verosimilmente in concomitanza della diffusione nazionale di programmi organizzati di screening di popolazione [ 4 ] , la casistica oggi disponibile molto pi ampia ed per questo stata rivalutata , consentendo stime assai pi stabili . materials and methods materiali e metodi the proficiency test was developed at cspo in 1996 . 
it consists of a set of 150 cases of bilateral , two - view screening mammography : a consecutive series of 133 negative cases ( diagnosed as negative within the florence province programme that screens women aged 5069 years and confirmed negative for at least one further screening round ) was seeded with 17 consecutive cancer cases detected by screening during the same year and confirmed by histology . 
the test was validated by a panel of four expert radiologists ( at least 20 , 000 mammograms read ) who were invited , as in current screening practice , to provide a report of : ( a ) negativity or ( b ) referral for further diagnostic assessment . 
average panel results ( sensitivity = 95% , range 88%100% ; referral rate = 8% , range 3%14% ) were lowered to make the test easier and were taken as reference standards . referral rate was determined only on negative controls . 
a test was passed when sensitivity was 80% and the referral rate was 15% . information on previous experience in mammography reading was available for most radiologists taking the test . experience was expressed as : ( a ) years of experience in mammography reading , ( b ) overall number of mammograms read and ( c ) number of mammograms read over the last year . after the test , radiologists were given their overall result and sensitivity and referral rate results , but not the results for the il test oggetto di questo studio stato sviluppato al cspo nel 1996 . 
esso consta di 150 casi di mammografia bilaterale in due proiezioni : una serie consecutiva di 133 casi negativi ( diagnosticati come tali nellambito del programma di screening della provincia di firenze , che invita le donne residenti dai 50 ai 69 anni , e rimasti tali almeno a un controllo biennale ) stata arricchita con 17 casi consecutivi di carcinoma , diagnosticati in occasione dello screening durante lo stesso anno e istologicamente confermati . 
dalla casistica consecutiva sono stati esclusi casi con radiogrammi di cattiva qualit ( cattiva esposizione , sfumature da movimento , artefatti , posizionamento inadeguato ) e carcinomi sintomatici o in categoria t2 o superiore . 
il test stato validato da 4 radiologi esperti ( almeno 20.000 mammografie lette ) ai quali stato richiesto , come nella pratica di screening , di formulare un giudizio alternativo tra un referto negativo o di indicazione a un ulteriore accertamento diagnostico . 
i risultati medi ( sensibilit media = 95% , range 88%100% ; tasso di richiamo medio = 8% , range 3%14% , questultimo calcolato escludendo i casi di carcinoma ) ottenuti da questo panel di esperti sono stati scontati per facilitare il superamento del test e hanno costituito lo standard di riferimento del test , che si ritiene superato solo quando siano raggiunti sia lo standard di sensibilit ( 80% ) che il tasso di richiamo ( 15% )  . 
the digital version was validated by a panel of four radiologists who confirmed the previously adopted reference standards . the study analysed the results obtained , their association with indicators of experience and the results of repeat tests taken by radiologists who had failed the first attempt . 
statistical analysis of the differences observed was based on the chi - square test ( 2 ) , statistical significance being set at p < 0.05. results during 19972005 , 537 first tests were taken by volunteering radiologists . 
only one third reported having > 10 years experience , approximately one third had read < 5 , 000 mammograms overall and one third had read < 1 , 000 mammograms during the previous year . test results are reported in table 2 . 
tests were usually repeated after a period of training , mostly after consulting a teaching dvd atlas provided by cspo , with several thousand mammography cases visible as an atlas or as an interactive test . 
 discussion use of a standard set to test diagnostic accuracy is definitely simpler , faster , and more feasible compared with conventional methods for measuring diagnostic accuracy , such as determining cancer detection rate or interval cancer frequency . 
on the contrary , a proficiency test is almost immediate , may be easily repeated and , if in sia come anni di esperienza in mammografia , che ( b ) come numero di mammografie totali lette , che ( c ) numero di mammografie lette nellultimo anno . 
i radiologi che hanno sostenuto il test sono stati informati solo sui valori si sensibilit e tasso di richiamo raggiunti e sulleventuale superamento del test , ma non sono stati rivelati i risultati nei singoli casi , il che ha consentito la ripetizione del test , a richiesta . 
data la grande richiesta di sostenere il test da parte dei radiologi italiani , piuttosto voluminoso e difficilmente decentrabile , esso stato trasposto in versione digitale ( fotografia digitale dei casi analogici ) su dvd , il che ha consentito il sostenimento del test al computer , e anche linvio a distanza . 
lo studio analizza i test sostenuti , in particolare confrontando il tasso di superamento con i diversi indicatori di esperienza raccolti , e valutando landamento del test nel tempo per i radiologi che lo hanno sostenuto pi volte , non avendolo superato . 
lanalisi statistica delle differenze osservate si basata sul test chi - quadrato ( 2 ) : la significativit statistica stata posta ad un valore di p < 0 , 05 . risultati dal settembre 1997 al dicembre 2005 sono stati sostenuti 537 primi test di screening , da parte di radiologi volontari , per la gran parte gi con esperienza di refertazione in mammografia , generalmente clinica . 
solo un terzo dei soggetti riferisce una esperienza da oltre 10 anni , circa il 30% riferisce a pi di 5000 mammografie totali lette , circa un terzo ha letto pi di 1000 mammografie nellultimo anno . 
il test stato superato al primo tentativo da 176 radiologi ( 32 , 7% ) , e non stato superato da 361 radiologi , dei quali da 220 per insufficiente sensibilit ( 60 , 9% ) , da 57 per eccessivo tasso di richiamo ( 15 , 7% ) e da 84 per entrambe le ragioni ( 23 , 2% )  . 
il superamento del test risultato essere correlato con lesperienza , quando questa misurata in base agli anni di esperienza di mammografia ( cut - off 5 anni : 2 per trend = 4 , 17 , p = 0 , 04 ) , o in termini di mammografie totali lette ( 2 per trend = 11 , 8 , p = 0 , 002 ) , o in termini di mammografie lette per anno ( 2 per trend = 6 , 27 , p = 0 , 04 )  . 
la ripetizione del test avvenuta per lo pi dopo un periodo di addestramento , in particolare dopo la consultazione di un dvd didattico , fornito dal cspo , contenente diverse migliaia di casi consultabili in forma di atlante o come test interattivo . 
la tabella 3 mostra i risultati di questi test ripetuti : un chiaro e significativo miglioramento della prestazione evidente sia al secondo ( 2 = 15 , 1 , p < 0 , 0001 ) che al terzo ( 2 = 10 , 2 , p < 0 , 01 ) tentativo . discussione luso di set standard in forma di test per la valutazione s . 
such an attitude is common in a clinical setting where excess investigations are not a major problem ( the presence of the woman allows immediate further investigation ) , and missing a cancer , often a symptomatic one , is unacceptable . 
on the contrary , in a screening setting , specificity is extremely imdellaccuratezza diagnostica certamente pi semplice e agile di misurazioni reali della sensibilit , basate sul tasso diagnostico di carcinoma , o sul tasso di carcinomi di intervallo . queste ultime misure , infatti , richiedono casistiche assai voluminose , difficili da ottenere per singoli operatori , e che comunque richiedono un lungo periodo di osservazione , mentre un test pressoch istantaneo , ripetibile , fruibile in qualsiasi momento e , specie in formato digitale , in qualsiasi luogo . la condizione del test , peraltro , introduce spesso una deformazione psicologica in chi lo sostiene , che spesso adotta una soglia di sospetto pi bassa , nel tentativo di aumentare al massimo la sensibilit . 
an excess referral rate increases economic and psychological costs ( reading is not immediate , and women have to be recalled , which is a major cause of anxiety ) , which may be unacceptable . 
in a scenario with a cancer prevalence < 1% , raising sensitivity by 10% detects one additional cancer every 2 , 000 screened cases whereas a 10% increase in referral rate implies 200 additional referrals per each additional cancer detected [ a referral positive predictive value ( ppv ) of 0.5% compared with 10%20% , as currently observed in screening ]  . 
the psychological effect associated with taking the test is almost unavoidable , and the observed sensitivity and referral rates are likely to be different from those obtained in current practice . 
thus , observed test results have no absolute value but are useful for comparison between tested subjects or to evaluate the same operator over time . the series examined is fairly large , and if we consider the total number of italian radiologists and the small minority involved in reporting mammography , a sample of over 500 cases is sufficiently representative of the national situation . although access to the test is on a voluntary basis , which might suggest a selection of less experienced but more strongly motivated radiologists , a large proportion of tests was taken by all radiologists working in the same radiology department or local health trust or even region . 
the option of employing properly trained general radiologists might turn out to be an acceptable and more feasible policy compared with the implementation of independent screening units on a national basis . rore falso negativo , che a un falso positivo : questo un atteggiamento tipico dello scenario clinico , ove un approfondimento diagnostico in pi non riveste un problema ( anche perch la donna presente e lapprofondimento immediato ) , mentre un errore diagnostico in un carcinoma , spesso sintomatico , decisamente da evitare . 
in uno scenario di screening , invece , la specificit ha una importanza molto maggiore , e un tasso di richiamo eccessivo , che comporta un aumento dei costi economici e psicologici ( la lettura differita e il richiamo causa un notevole stress alla donna ) pu risultare inaccettabile . 
in un contesto dove la prevalenza di carcinoma inferiore all1% , un aumento della sensibilit del 10% comporta lidentificazione aggiuntiva di un carcinoma ogni 2000 esami circa , mentre un aumento del 10% del tasso di richiamo comporta 200 richiami in pi per ogni carcinoma aggiuntivo diagnosticato ( un valore predittivo positivo dello 0 , 5% , rispetto al 10%20% comunemente osservato nello screening )  . 
leffetto psicologico del test su chi lo sostiene quasi inevitabile , e i valori di sensibilit e di tasso di richiamo ottenuti non saranno uguali a quelli che loperatore ha nella pratica corrente . 
considerato il numero generale di radiologi e il fatto che una piccola minoranza di essi referta la mammografia nella propria pratica professionale , un campione di oltre 500 casi risulta abbastanza rappresentativo della realt nazionale . 
anche se laccesso al test formalmente volontario , il che potrebbe suggerire una selezione tra i meno esperti ma certo i pi volonterosi , buona parte dei test sono stati sostenuti dallinsieme dei radiologi di una unit operativa di radiologia diagnostica , o di una asl , o addirittura di una regione . 
assumendo che il campione abbia una sua significativit , colpisce subito il dato dellesperienza in mammografia . soprattutto il dato relativo alle mammografie lette nellultimo anno , con oltre un terzo dei radiologi che leggono meno di 1000 , e poco meno di un terzo meno di 2000 mammografie lanno , rende ragione della realt italiana , peraltro ben nota , che vede la mammografia non affidata a centri senologici dedicati , ma a radiologi generalisti , nellambito delle varie metodologie diagnostiche afferenti a una unit operativa ospedaliera o territoriale standard , senza che questi radiologi siano stati previamente sottoposti ad un adeguato addestramento . 
questa una realt , pi che una scelta , che peraltro , come si vede dallanalisi dei risultati , potrebbe dover essere riconsiderata , per lo meno nel senso di garantire a tutti gli operatori addetti un congruo periodo di addestramento specifico . 
limpiego di radiologi generalisti propriamente addestrati potrebbe essere una soluzione accettabile e pi facilmente realizzabile su scala nazionale rispetto alla creazione di unit di screening indipendenti . nonostante il test sia stato creato con lintento di non renderlo troppo difficile ( i carcinomi erano stati effettivamente diagnosticati nella pratica corrente , i livelli di sensibilit e tasso di richiamo ottenuti dagli esperti sono stati ragionevolmente scontati ) , il tasso di superamento stato effettivamente modesto ( 32 , 7% )  . 
the number of mammograms read in the previous year is probably a better indicator of experience compared with number of years of experience or total mammograms read , as it accounts for recent intensive experience . 
consulting an interactive teaching atlas containing a large number of cases ( which would require decades to be seen in current practice ) allowed most radiologists to pass the test : the cumulative rate of success was 32.7% after one test , 66.7% after two and 89.3 % after three attempts . overall , with the limits inherent to the artificial nature of the test , the study suggests that : 1 . 
training is still possible , however , particularly if we consider that one third of italy has still to be covered by organised screening [ 4 ]  . rare il test dipende assai di pi dallesperienza che non dalla sua difficolt intrinseca . 
il numero di mammografie lette nellultimo anno un indicatore migliore degli anni di esperienza o delle mammografie totali lette , in quanto rende ragione di una esperienza recente e concentrata nel tempo : i radiologi di minore esperienza ( < 1000 mammografie / anno ) hanno risultati ( superamento del test nel 22 , 7% ) decisamente inferiori a radiologi di non tanto maggior esperienza ( > 2000 mammografie / anno ) che ottengono risultati pi che doppi ( superamento del test nel 54 , 8% )  . il ruolo fondamentale dellesperienza ribadito dallevidenza relativa a chi ripete il test , non avendolo superato , dopo un periodo ( in genere breve ) di addestramento su un supporto didattico congruo . 
la visione in un atlante interattivo di un numero elevato di casi , cosa che nella realt professionale avrebbe richiesto decenni o non si sarebbe mai avverata , ha consentito alla maggioranza dei radiologi di superare il test . 
se si generalizzano i risultati di chi ha ripetuto il test alla totalit della casistica , il tasso di superamento complessivo del test del 36 , 7% con un tentativo , del 66 , 7% con due tentativi , dell89 , 3% con tre . 
arrigo , via venezia 16 , i - 15100 alessandria , italy 2dipartimento di medicina sperimentale , sezione di diagnostica per immagini e radioterapia , universit di genova , largo rosanna benzi 10 , i - 16132 genova , italy correspondence to : f . 
zandrino , corso volpini 111 , i - 14057 isola dasti ( at ) , italy , tel . : + 39 - 0131 - 206481 , fax : + 39 - 0131 - 206682 , e - mail : zandrino@libero.it received : 17 october 2005 / accepted : 31 march 2006 / published online : 11 august 2006 abstract purpose . 
at mammography , five were not detected , three presented as spiculated masses , two as masses with irregular margins , two as spiculated masses with microcalcifications , two as distortions , one as a cluster of microcalcifications and one as asymmetric density . 
in three , core biopsy was made : in the first , a complex sclerosing lesion with atypical cells was suggested , in the second differential diagnosis between tubular carcinoma and sclerosing adenosis was proposed and in the third a tubular carcinoma . 
alla mammografia 5 non erano visibili , 3 si presentavano come masse spiculate , 2 come masse con contorni irregolari , 2 come masse spiculate con microcalcificazioni , 2 come distorsioni , 1 come gruppo di microcalcificazioni ed 1 come densit asimmetrica . 
in 3 stato fatto un prelievo bioptico mediante core - biopsy con le seguenti diagnosi : lesione sclerosante complessa con cellule atipiche ; lesione con diagnosi differenziale da porsi tra carcinoma tubulare ed adenosi sclerosante ; carcinoma tubulare . 
this particular subtype of invasive ductal carcinoma occurs with a prevalence of 1%10% of all mammary adenocarcinomas [ 26 ] , with a reported mortality of 2% [ 7 ]  . since prognosis is better than for other histological types [ 4 , 5 , 8 ] , it seems to be useful to improve the detection and presurgical characterisation of this type of lesion [ 9 ]  . 
the purpose of this paper is to present the histopathological , clinical , mammographic and ultrasonographic ( us ) features of a series of 16 cases of tubular carcinoma and to review the current literature . il carcinoma tubulare della mammella un adenocarcinoma invasivo , relativamente raro , ben differenziato . 
la prevalenza dell1%10% di tutti gli adenocarcinomi della mammella [ 26 ] , e la mortalit del 2% [ 7 ]  . essendo la prognosi pi favorevole rispetto agli altri tipi istologici [ 4 , 5 , 8 ] , utile , in fase pre - chirurgica , identificare e caratterizzare questo tipo di lesione [ 9 ]  . 
lo scopo del nostro lavoro presentare gli aspetti istopatologici , clinici , mammografici ed ecografici di una serie di 16 casi di carcinoma tubulare e analizzare la letteratura disponibile su tale lesione . materials and methods a retrospective review of 560 consecutive histologically proven breast carcinomas was made . 
in this series of patients , whenever a suspicious lesion was detected on mammography , us or supplementary projections were done . mammographic examinations were performed with dmr ( ge medical systems , milwaukee , wi , usa ) and mammomat 2000 ( siemens , erlangen , germany ) units . 
us was also performed in patients with a dense mammographic pattern . us - guided fine - needle aspiration cytology ( fnac ) was made for us - detectable lesions while stereotactic - guided biopsy ( 14 - gauge core biopsy ) was performed for lesions not detected with us . 
 materiali e metodi stata effettuata una revisione di 560 casi consecutivi di carcinoma della mammella , tutti con diagnosi istologica , osservati nel periodo compreso tra gennaio 2000 e gennaio 2005 . 
le mammografie sono state eseguite con apparecchiature dmr ( ge medical systems , milwaukee , wi , u.s.a. ) e mammomat 2000 ( siemens , erlangen , germania )  . lecografia veniva inoltre eseguita in pazienti con quadro mammografico di tipo denso . 
lagoaspirato ecoguidato stato eseguito sulle lesioni visibili allecografia , mentre nei casi di lesioni non identificabili allecografia veniva eseguita una core - biopsy sotto guida stereotassica con ago tranciante da 14 gauge . 
in tutti i casi di carcinoma tubulare sono stati registrati ed analizzati i dati clinici delle pazienti , cos come i reperti mammografici , ecografici ed istopatologici . results sixteen pure tubular carcinomas were found ( 2.86% ) in 14 women ( age 5510 years , meanstandard deviation )  . 
a nonspecific diagnosis positive for carcinoma was made in 11 cases without identification of the histological type while atypical cells were found in two cases ( table 1 )  . 
in three patients , core biopsy was made : in the first , a complex sclerosing lesion with atypical cells was suggested ; in the second , differential diagnosis between tubular carcinoma and sclerosing adenosis was proposed ; in the third , a tubular carcinoma was diagnosed . lesions associated with tubular carcinoma found at histology and the results of fnac and core biopsy in our series are listed in table 2 . 
1a - c craniocaudal ( a ) and mediolateral oblique ( b ) views demonstrate an irregularly shaped density in the upper - external quadrant of the left breast ( arrows )  . 
1a - c le proiezioni cranio - caudale ( a ) e medio - laterale oblique ( b ) dimostrano un addensamento con contorni irregolari nel quadrante supero - esterno della mammella sinistra ( frecce )  . 
in 11 lesioni stata fatta una diagnosi generica di carcinoma , senza identificazione del tipo istologico , mentre in 2 la diagnosi stata cellule atipiche ( tabella 1 )  . 
in 3 pazienti stata fatta una core - biopsy con le seguenti diagnosi micro - istologiche : lesione sclerosante complessa con cellule atipiche ; lesione con diagnosi differenziale da porsi tra carcinoma tubulare ed adenosi sclerosante ; carcinoma tubulare . 
adenosi sclerosanteb dcis , atypical hyperpalsia papillary hyperplasia , sclerosing adenosis , lcis sclerosing adenosis atypical lobular hyperplasia , lcis cribriform intraductal carcinoma dcis , atypical ductal hyperplasia atypical ductal hyperplasia cribriform intraductal carcinoma papillary intraductal carcinoma radial scar cribriform invasive carcinoma sclerosing adenosis cdis , iperplasia atipica iperplasia papillare , adenosi sclerosante , clis adenosi sclerosante iperplasia lobulare atipica , clis carcinoma cribriforme intraduttale cdis , iperplasia duttale atipica iperplasia duttale atipica carcinoma cribriforme intraduttale carcinoma papillare intraduttale radial scar carcinoma cribriforme invasivo adenosi sclerosante dcis , ductal carcinoma in situ ; lcis , lobular carcinoma in situ afine - needle aspiration cytology ; bcore biopsy tabella 1 risultati clinici ed istopatologici nella nostra casistica di 16 carcinomi tubulari puri in 14 pazienti paziente chirurgia linfonodi reperti istopatologici associati cdis , carcinoma duttale in situ ; clis , carcinoma lobulare in situ acitologia ; bcore biopsy discussion histopathology diagnosis of tubular carcinoma with fnac is often difficult . 
although not pathognomonic , some distinctive cytological features of tubular carcinoma can be identified : increased cellularity , angular cellular clusters with sharp borciate ai carcinomi tubulari identificate allesame istopatologico ed i risultati dellesame citologico e micro - istologico pre - operatori sono elencate in tabella 2 . le dimensioni dei carcinomi tubulari allesame istopatologico sono state di 9 , 74 , 9 mm ( da 4 , 9 a 20 , 0 mm )  . 
l ' ingrandimento ( b ) evidenzia un nodulo con contorni irregolari . all ' esame ecografico ( c ) questo piccolo carcinoma tubulare si presenta come una lesione ipoecogena , con contorni irregolari , senza attenuazione del fascio ultrasonoro . 
quadro citologico ( d ) ed istologico ( e )  . ders , oval cells perpendicularly arranged along the edges of the clusters , dispersed single epithelial cells with minimal atypia and few bare oval nuclei in the background [ 10 ]  . 
in the report by mitnick and coworkers , fnac was performed in 36 tubular carcinomas , with positive results for tubular carcinoma in 15 ( 42% ) , suspicion in three , atypia in ten and false negative discussione istopatologia la diagnosi citologica di carcinoma tubulare in genere difficile . 
found , in fnac of 15 tubular carcinomas , ten carcinomas and five cases with atypia [ 5 ]  . histological characteristics of tubular carcinoma are an orderly distribution of branched angular tubules in a loose , fibrous stroma , with low nuclear grade and no evidence of vascular or lymphatic invasion [ 10 ]  . 
core biopsy is recommended when tubular carcinoma is considered to be a possible diagnosis since fewer lesions are diagnosed as atypia and fewer false negatives can occur [ 5 , 9 ]  . 
nevertheless , in our series , a correct diagnosis of tubular carcinoma was made in only one case . other histological types of carcinoma can be found in association with tubular carcinoma , with a prevalence of ductal carcinoma in situ [ 13 , 7 , 9 ]  . 
the high frequency of ductal carcinoma in situ ( 12.5% in our series ) and cribriform carcinoma ( 19% ) associated with tubular carcinoma raised the question about a possible relationship among these lesions [ 4 ]  . 
calcifications , which are usually seen in intraductal carcinoma , are found on microscopy in 50% of tubular carcinomas [ 3 ] : this association suggests a correlation of tubular carcinoma and intraductal carcinoma [ 9 ]  . associated benign lesions are fibrocystic changes , atypical ductal hyperplasia , sclerosing adenosis and radial scar [ 9 ]  . 
radial sclerosing lesions ( radial scar , a central area of sclerosis composed of collagen and elastic tissue surrounded by stellate duct proliferation ) , presenting in many cases as spiculated masses , often mimic tubular carcinoma on histopathology . 
some authors have discussed the potential malignancy of radial scar and suggest progression from radial scar to tubular carcinoma [ 11 , 12 ]  . the age of our population is close to the mean age reported in other similar studies [ 4 , 5 , 8 ]  . 
the mean size of tubular clinical features aumentata cellularit , clusters cellulari con morfologia angolata e contorni netti , cellule ovalari disposte perpendicolarmente lungo i bordi dei clusters , cellule epiteliali sparse con minime atipie , rari nuclei ovali sullo sfondo [ 10 ]  . 
 [ 9 ] , la citologia stata effettuata in 36 carcinomi tubulari , con risultato positivo per carcinoma tubulare in 15 , sospetto in 3 , diagnosi di atipia in 10 e diagnosi falsamente negativa in 8 ( 22% )  . 
 [ 5 ] sono stati sottoposti ad esame citologico 15 carcinomi tubulari , con diagnosi di carcinoma in 10 e di atipia in 5 . le caratteristiche istologiche sono quelle di una serie di strutture tubulari angolate e ramificate disposte in modo ordinato allinterno di uno stroma connettivale lasso , con basso grado nucleare ; non presente invasione di vasi sanguigni o linfatici [ 10 ]  . 
alcuni autori raccomandano la core - biopsy nel caso si sospetti un carcinoma tubulare , in quanto con esame micro - istologico possibile evitare diagnosi generiche di atipia e sono rari i falsi negativi [ 5 , 9 ]  . 
ciononostante nella nostra casistica , solo in 1 caso stata fatta una diagnosi corretta di carcinoma tubulare . accanto al carcinoma tubulare vengono descritti altri tipi istologici , prevalentemente il carcinoma duttale in situ [ 13 , 7 , 9 ]  . 
lelevata incidenza di associazione con il carcinoma in situ ( 12 , 5% nella nostra casistica ) ed il carcinoma cribriforme ( 19% ) hanno fatto supporre un possibile rapporto tra queste lesioni [ 4 ]  . 
le calcificazioni , generalmente presenti nel carcinoma intraduttale , sono identificate allesame microscopico nel 50% dei carcinomi tubulari [ 3 ] : questa associazione fa supporre una relazione tra carcinoma tubulare e carcinoma intraduttale [ 9 ]  . si associano al carcinoma tubulare anche lesioni benigne quali alterazioni di tipo fibrocistico , iperplasia duttale atipica , adenosi sclerosante e radial scar [ 9 ]  . 
le lesioni radiali sclerosanti ( radial scar , unarea di sclerosi centrale costituita da tessuto collagene ed elastico e circondata da proliferazione cellulare con forma stellata ) , che si presentano in genere alla mammografia come masse spiculate , simulano spesso allesame istopatologico il carcinoma tubulare . alcuni autori hanno discusso sulla potenziale malignit della radial scar , ipotizzando un passaggio da radial scar a carcinoma tubulare [ 11 , 12 ]  . aspetti clinici let media delle nostre pazienti con carcinoma tubulare poco si discosta da quella riportata in studi simili [ 4 , 5 , 8 ]  . la dimensione media dei carcinomi tubulari allesame istopatologico descritta in letteratura di circa 1 cm [ 2 , 4 , 5 , 9 , 1315 ]  . 
nella nostra casistica stata di 9 , 7 mla maggior parte dei carcinomi tubulari non sono palpabili per le piccole dimensioni [ 4 , 9 ]  . lincidenza delle metastasi linfonodali va dallo 0% al 29% [ 2 , 48 , 14 ]  . 
moreover , the very low incidence of lymph node involvement is likely related to the low invasiveness of the primary lesion rather than the small size of most tubular carcinomas at the time of diagnosis [ 4 ]  . 
l ' ecografia dimostra un piccolo nodulo ipoecogeno con attenuazione posteriore ( d )  . all ' esame istologico carcinoma tubulare associato a radial scar . bassa incidenza sarebbe correlabile pi alla scarsa invasivit del tumore primitivo che alle piccole dimensioni della maggior parte dei carcinomi tubulari alla diagnosi [ 4 ]  . 
suggested no axillary nodal dissection in patients with a tubular component > 90% [ 16 ]  . no difference in presentation or clinical outcome of pure tubular carcinoma is observed in comparison with mixed forms [ 7 ]  . 
due to the low invasiveness of tubular carcinoma , breast preservation therapy , with or without radiotherapy , is probably the best approach [ 4 , 17 ] , in particular when no nodal metastasis is found [ 18 ]  . 
in a series of tubular carcinomas sized 3 cm or less , a low rate of recurrence was observed ( 4% ; 5.4 years mean follow - up ) after only lesion excision without radiotherapy [ 19 ]  . mammography the sensitivity of mammography in detecting tubular carcinoma ranges from 65% to 100% [ 2 , 5 , 9 , 15 ]  . 
according to most authors , the small size of the lesions on mammography is not specific enough to differentiate tubular carcinoma from other small carcinomas [ 2 , 4 ]  . 
only one case in our series presented as a cluster of microcalcifications without a mass . according to mitnick et al . , the presence of microcalcifications alone is the rarest mammographic pattern of tubular noma tubulare [ 4 , 17 ] , in particolare quando non sono presenti localizzazioni linfonodali [ 18 ]  . 
in carcinomi tubulari di dimensioni uguali o inferiori a 3 cm stata osservata una percentuale di recidiva bassa ( 4% , follow - up medio di 5 , 4 anni ) anche dopo semplice escissione della lesione senza radioterapia [ 19 ]  . mammografia la sensibilit della mammografia nellidentificazione del carcinoma tubulare varia dal 65% al 100% [ 2 , 5 , 9 , 15 ]  . 
come osservato nella nostra casistica , la maggior parte dei lavori descrivono il carcinoma tubulare come una piccola lesione spiculata senza microcalcificazioni ( tabella 2 ) [ 2 , 4 , 10 ]  . 
 [ 5 ] hanno identificato microcalcificazioni con aspetto radiologico maligno nel 24% delle lesioni . questo risultato potrebbe dipendere dallutilizzo dellingrandimento radiologico , effettuato nella maggior parte delle pazienti [ 5 ]  . 
not available afour lesions with microcalcifications ; bfour cases with calcifications suggestive of malignancy ; ctwo lesions with microcalcifications tabella 2 aspetti clinici e mammografici del carcinoma tubulare della mammella : dati estratti dalla letteratura carcinomi tubulari , n [ voce bibliografica ] palpabili mx negativa masse con contorni densit mal definiti / spiculati noduli microcalcificazioni / asimmetriche , rotondeggianti / masse con distorsioni ovali microcalcificazioni mx , mammografia ; n.a. , dato non disponibile aquattro lesioni con microcalcificazioni ; bquattro casi con microcalcificazioni ; cdue lesioni con mirocalcificazioni carcinoma [ 9 ]  . 
the only report suggesting typical radiological and clinical features of tubular carcinoma argued that a small , nonpalpable , spiculated mass is distinctive enough to differentiate tubular carcinoma from other malignancies [ 14 ]  . 
as in our series , all authors describe most tubular carcinomas as hypoechoic masses with ill - defined margins and posterior acoustic shadowing [ 5 , 9 , 15 ]  . 
the two missed lesions were 6 mm and 8 mm on histopathology [ 5 ]  . differential diagnosis a precise differential diagnosis between tubular carcinoma and other histological subtypes cannot be reached with mammography . 
small size and spiculated margins , the most frequent pattern of tubular carcinoma on mammography , are nonspecific characteristics that do not allow differentiation from other small - sized malignant lesions . 
the appearance of tubular carcinoma at colour - doppler us was not systematically evaluated in our series , and data were not recorded ; moreover , no large series of tubular carcinomas studied with colour - doppler us are available in the literature . 
 on magnetic resonance imaging ( mri ) , some authors observed enhancement patterns that could help to differentiate tubular carcinoma from other histological subtypes [ 2123 ]  . the most frequently observed is a thin rim of delayed peripheral enhancement [ 22 , 23 ]  . cytological diagnosis is difficult due to the possible occurrence of false negatives or nonspecific results [ 4 , 24 , 25 ] , also observed in our series , and for the sometimes difficult differential diagnosis with radial scar [ 24 , 26 ]  . 
notwithstanding the larger amount of material that allows a microhistological assessment , core biopsy , did not give , in our series , a definite diagnosis in two out of three patients . 
 [ 5 ] , in un tentativo di caratterizzare il carcinoma tubulare , hanno osservato come spicule lunghe , frequentemente associate alla radial scar , sono identificabili in circa la met dei carcinomi tubulari . ecografia sono rare le pubblicazioni in cui stato descritto laspetto ecografico dei carcinomi tubulari [ 5 , 9 , 20 ]  . 
le due lesioni non visualizzate misuravano , allesame istopatologico , 6 e 8 mm [ 5 ]  . diagnosi differenziale la mammografia non permette una sicura diagnosi differenziale tra carcinoma tubulare ed altri tipi istologici . 
le piccole dimensioni ed i contorni spiculati , che sono laspetto mammografico di buona parte dei carcinomi tubulari , sono caratteristiche aspecifiche , che non ne consentono la differenziazione da altre lesioni maligne di piccole dimensioni . 
anche la possibile associazione con la radial scar rappresenta una caratteristica aspecifica , non essendo state riscontrati aspetti radiologici particolari nelle radial scars associate a carcinoma tubulare [ 11 ]  . 
le caratteristiche dei carcinomi tubulari al color - doppler non sono state valutate in modo sistematico nella nostra casistica , e non sono al momento disponibili in letteratura descrizioni su ampie casistiche . 
dal punto di vista citologico la diagnosi di carcinoma tubulare complessa , per la possibile presenza di false negativit o di diagnosi aspecifiche [ 4 , 24 , 25 ] , osservate anche nella nostra casistica , e per la diagnosi differenziale talora difficile con la radial scar [ 24 , 26 ]  . 
la core - biopsy , nonostante la maggior quantit di materiale prelevato che consente una diagnosi micro - istologica , non ha fornito , nella nostra casistica , risultati sicuri in 2 casi su 3 . 
pertanto probabile che nella diagnosi pre - operatoria solo la vacuum - assisted biopsy possa consentire un prelievo sufficientemente accurato . conclusioni in conclusione , si pu affermare come la prognosi favorevole con possibilit di un approccio terapeutico minimamente invasivo al carcinoma tubulare rendono necessaria una vaf . 
this can probably only be obtained with histological sampling ( if possible , vacuum - assisted biopsy ) , allowing precise differential diagnosis between tubular carcinoma and other histological subtypes and benign associated lesions . lutazione pre - operatoria il pi possibile accurata . 
bruschi , institute of radiology pugd , via colugna 50 , i - 33100 udine , italy , tel . : + 39 - 043 - 2559266 , fax : + 39 - 043 - 2559867 , e - mail : radiologia.segr@med.uniud.it received : 7 september 2005 / accepted : 1 april 2006 / published online : 11 august 2006 abstract purpose . 
in a blind in vitro analysis , 28 great saphenous veins , obtained after stripping surgery from 28 patients with chronic venous insufficiency , were examined with a digital us scanner atl - hdi5000 , linear 5 to 12 - mhz broadband probe , compound imaging technique and analogic - digital zooming . 
the samples , fixed in formalin , were sent to the pathology laboratory : sections were obtained at the same level of the sonographic planes , and images were obtained by digital camera mounted on an optical microscope . measurements obtained at histology were considered as the gold standard . 
if these preliminary data are confirmed in vivo , sonography could be used to discriminate patients eligible for conservative treatment instead of surgery . key words ultrasound parietal thickness varicose veins endovenous laser treatment riassunto obiettivo . 
in una analisi in cieco sono stati esaminati in vitro 28 pezzi operatori di grande safena , provenienti da altrettanti pazienti affetti da insufficienza venosa cronica e sottoposti a stripping chirurgico . 
stato utilizzato un ecografo digitale atl - hdi 5000 , con sonda ecografica lineare broadband con frequenza variabile da 5 a 12 mhz , tecnica compound imaging e tecnica zoom ad , ottenendo sia scansioni assiali che longitudinali . 
nella nostra esperienza preliminare , lo studio in vitro delle vene varicose permette un riconoscimento almeno morfologico delle pareti ipotrofiche , ponendo le basi per lo studio in vivo nella selezione dei pazienti candidati a trattamento conservativo , piuttosto che chirurgico . parole chiave ecografia spessore parietale vene varicose trattamento laser endovascolare introduction introduzione e . 
it has been widely demonstrated that vascular morphology depends on general factors , such as age , and on particular factors , such as variations in resistance , pressure and flow strictly depending on local haemodynamics [ 2 ]  . 
 [ 3 ] noted that hypertrophy may be caused by derangement of smooth muscle cells ( due to mutation from a contractile phenotype to a less elastic phenotype ) and extracellular matrix accumulation , as well as by increased vasa vasorum due to hypoxia and some growth factors ( tgf )  . 
 [ 6 ] suggest that changes in the cellular matrix of the vein wall can be considered the first cause of varicosity while valve failure would be merely a consequence of these modifications . 
 histological remodelling phenomena account for cellular proliferation , cellular migration , and extracellular matrix biosynthesis due to biochemical factors produced by mural cells ( endothelial cells , smooth muscle cells , fibroblasts ) and by circulation elements ( platelets , leucocytes ) [ 2 ]  . 
therefore , the hyperdynamic flow , related more frequently in vivo to incontinence of the saphenofemoral junction of the great saphenous vein ( gsv ) , may induce parietal changes , which result in a succession of atrophic and clearly hypertrophic segments in the same vein wall [ 3 ]  . 
 the wall of normal veins displays , on histological section with masson 's trichrome , regular arrangement in three layers : intima ( thin and regular ) , muscularis ( which supports the vein wall and is made up of smooth muscle cells clustered in circular bundles or surrounded by extracellular matrix ) and adventitia ( outermost layer , at times interrupted by vasa vasorum )  . the intima and muscularis are usually involved in veinwall remodelling , and these two tunicae present an overall normal thickness ranging from 460 m to 690 m [ 3 ]  . 
this ultrastructural normal aspect , according to some authors , correlates with a three - layer pattern at sonographic imaging [ 7 , 8 ] : the adventitia appears hyperechoic ; the media hypoechoic ; the intima hyperechoic [ 7 ]  . 
initially , the wall reacts with an accumulation of smooth muscle cells and fibrous tissue , which causes disappearance of the typical three - layer pattern due to loss of separation between intima and media [ 2 ] and causes a thickening of these two layers , ranging from 800 to 1 , 380 m [ 3 ]  . 
 subsequently , ischaemia due to insufficient flow from vasa vasorum leads to a progressive loss of smooth muscle cells and matrix , which causes a reduction of wall thickness ( 115350 m ) [ 3 ]  . 
a hypotrophic vein wall is two times thinner than a regular le vene varicose colpiscono circa un quarto della popolazione adulta dei paesi occidentali , rappresentando una causa considerevole di morbidit e di accesso ai servizi di assistenza medica . 
stato largamente dimostrato che la morfologia vascolare strettamente legata a fattori generali come let e a fattori particolari che possono mostrare modificazioni legate a variazioni emodinamiche locali che comprendono la resistenza , la pressione e il flusso [ 2 ]  . 
 [ 3 ] hanno posto lattenzione sullipertrofia dovuta alla disorganizzazione delle cellule muscolari lisce ( con mutazione da un fenotipo contrattile verso un fenotipo meno elastico ) e allaccumulo di matrice extracellulare , nonch sullincremento dei vasa vasorum sotto lo stimolo ipossico e sotto lo stimolo di alcuni fattori di crescita ( tgf )  . 
altri autori [ 4 , 5 ] hanno enfatizzato come possa essere importante laumento della produzione di collagene di tipo i a scapito di quella di tipo iii e v e la diminuzione dellelastina . 
 [ 6 ] sostengono che i cambiamenti della matrice cellulare della parete della vena possono essere considerati come la prima causa delle varicosit e linsufficienza valvolare come lesito di tali cambiamenti . 
sicuramente i principali fenomeni di rimodellamento da un punto di vista istologico possono essere riassunti in : proliferazione cellulare , migrazione cellulare , biosintesi di matrice extracellulare , dovuti a fattori biochimici prodotti da cellule parietali ( cellule endoteliali , cellule muscolari lisce , fibroblasti ) e da elementi circolanti ( piastrine , leucociti ) [ 2 ]  . 
possibile quindi affermare che la parete di una vena che viene sottoposta ad un regime iperdinamico ( condizione pi frequente in vivo il caso della vena grande safena a monte della quale si instauri una incontinenza della crosse safeno - femorale ) va incontro ad una serie di trasformazioni parietali compensatorie costituite da una alternanza di segmenti atrofici ad altri pi francamente ipertrofici [ 3 ]  . 
la parete della vena sana presenta , alla sezione istologica con colorazione tricromica di masson , una regolare tristratificazione : lintima ( sottile e regolare ) , la muscolare ( che fa da struttura portante della parete ed costituita da cellule muscolari lisce disposte a bande circolari o impacchettate con matrice extracellulare ) e lavventizia ( la pi esterna )  . 
pi esternamente , lavventizia disposta a nastri viene interrotta talora dai vasa vasoruintima e muscolare sono di solito coinvolte nel rimodellamento della parete della vena e nel complesso queste due tuniche raggiungono uno spessore complessivo massimo di 460690 m [ 3 ]  . 
almeno inizialmente la parete risponde con un accumulo di cellule muscolari lisce e tessuto fibroso , che porta alla scomparsa della caratteristica tristratificazione , per la perdita della netta separazione fra intima e media [ 2 ] e un complessivo aumento dello spessore parietale a carico di intima e e . 
the succession of alternating hypertrophic and atrophic segments probably explains the typical tortuosity of varicose veins . analysis of wall features and thickness has never been considered really relevant until now , mainly for two reasons : first , because the only available treatment up to now was radical saphenectomy ; and second , because a presurgical histological study after percutaneous biopsy is probably too invasive a procedure for a low - risk disease . the advent of digital sonography with a high - frequency , high - resolution broadband probe has introduced many important advantages in clinical practice , such as decreased noise , absence of signal distortion and optimal focusing of the ultrasound ( us ) beathe quality of the resulting sonographic image is usually better than conventional us with regard to axial and lateral resolution , contrast , absence of noise and artefacts [ 10 ] , permitting the evaluation of submillimetric structures , such as vein walls , until now never really considered by sonography . the thickness of pathological vein walls is potentially very relevant for the surgeon , who may consider the option of conservative treatment , e.g. 
in fact , surgical excision of varicose portions characterised by parietal hypoplasia may be very difficult due to their fragility . on the contrary , a thick muscle wall makes evlt ineffective , increasing the risk of recurrences [ 11 ]  . 
 successivamente fenomeni ischemici dovuti allinsufficiente apporto dei vasa vasorum , portano alla perdita di cellule muscolari lisce e matrice con assottigliamento complessivo della parete ( 115350 m ) [ 3 ] , mentre le cellule muscolari lisce e la componente extracellulare sono quasi completamente scomparse . 
allo studio delle caratteristiche e dello spessore parietale , non mai stata data la giusta importanza , sia perch lunico trattamento proposto era quello della safenectomia radicale , con leliminazione del tronco venoso superficiale principale , sia perch presupponeva uno studio istologico preoperatorio , improponibile nellinquadramento di una patologia che rarissimamente mette a rischio la vita del paziente . 
la recente introduzione degli ecografi digitali con sonde ad alta frequenza , larga banda ed alta risoluzione , ha permesso nella pratica clinica una serie di vantaggi non indifferenti , tra cui la riduzione del rumore di fondo , la mancata distorsione del segnale , lottimale focalizzazione del fascio di ultrasuoni . 
la qualit dellimmagine definitiva di solito nettamente superiore allimmagine ecografica convenzionale in termini di risoluzione spaziale assiale e laterale , di contrasto , di annullamento del rumore di fondo e di eliminazione degli artefatti [ 10 ] , cos da poter valutare strutture submillimetriche , come la parete delle vene , finora mai considerata in ecografia . 
la conoscenza dello spessore della parete delle vene un dato potenzialmente interessante sia per lecografista , che si trova alle prese con misurazione submillimetriche , che per il chirurgo che abbia optato per il trattamento conservativo e nella fattispecie per il trattamento laser endovascolare ( evlt ) di recente introduzione . 
infatti i tratti varicosi caratterizzati da spiccata ipoplasia parietale risultano difficilmente asportabili con le tecniche invasive , proprio a causa della loro fragilit . per contro , lassenza di una spessa parete muscolare rende efficace il trattamento endovascolare , riducendo al minimo il rischio di recidive [ 11 ]  . 
during postprocessing with appropriately calibrated software , we were able to perform further sonographic measurements , extending our assessment to other segments not considered at the beginning . the formalin - fixed samples were sectioned by the pathologist axially and longitudinally , at the same level of the sonographic planes . 
the samples were embedded in paraffin and cut at a thickness of 5 m , then stained with hematoxylin - eosin and masson 's trichrome to better visualise wall layers . 
histological measures were calculated using dedicated software ( olympus dp soft version 3.2 ) with magnification of a digital camera olympus mounted on an optical microscope ( axioscop , zeiss , ag , germany )  . 
su queste ultime sono state effettuate da 1 a 3 misurazioni progressive ( con un massimo di 3 misurazioni nelle vene pi lunghe e con un valore medio di 2 , 39 misurazioni su ciascuna vena , per un totale di 67 spessori parietali )  . 
in accordo con quanto riportato in letteratura [ 3 ] , abbiamo considerato come normale una vena con spessore parietale compreso tra 0 , 4 e 0 , 7 mm , ipertrofica una con valori superiori a 0 , 8 mm e ipotrofica una con spessore inferiore a 0 , 35 mle misurazioni lungo il tratto safenico sono state riferite al collega anatomopatologo come distanza , espressa in centimetri , dal filo chirurgico legato a monte , in corrispondenza della crosse safeno - femorale ( punto 0 )  . 
in post - processing con lutilizzo di un software dedicato , opportunamente calibrato , abbiamo potuto compiere ulteriori misurazioni ecografiche , estendendo le nostre valutazioni ad altri tratti non considerati in un primo momento . 
i reperti , fissati in formalina , sono poi stati inviati presso il laboratorio di anatomia patologica , dove sono stati sottoposti a sezione in corrispondenza delle riferite scansioni ecografiche , secondo una direzione longitudinale e assiale . 
i prelievi sono stati inclusi in paraffina e sezionati ad uno spessore di 5 m e quindi sottoposti a colorazione con ematossilina - eosina e tricromica di masson , in modo da evidenziare con maggiore contrasto la parete e lavventizia . 
complete agreement was demonstrated in hypotrophy when the central hypoechoic layer only was considered us with the two hyperechoic lines us with central hypoechoic line only histology tabella 1 ecografia versus istologia : risultati . 
stata verificata una totale concordanza nei casi di ipotrofia quando stata considerata la sola linea ipoecogena centrale spessore ecografico con le due linee iperecogene spessore ecografico della sola linea centrale ipoecogena istologia diagnosis hypotrophy , n normotrophy , n hypertrophy , n total , n diagnosi ipotrofia , n normotrofia , n ipertrofia , n totale , n essa compresa e quindi non realmente parte dello spessore parietale , abbiamo diagnosticato 32 tratti safenici come ipotrofici ( valore medio di 0 , 28 mm ) , contro i 29 diagnosticati nelle corrispondenti sezioni istologiche ( valore medio di 0 , 279 mm )  . 
lecografia ha fatto diagnosi di normotrofia in 23 casi ( valore medio di 0 , 52 mm ) , mentre listologia ne ha diagnosticati 22 ( valore medio di 0 , 56 mm ) , confermando 19 dei casi individuati allecografia ( 86% ) , mentre 4 / 23 furono dimostrati poi essere ipertrofici allistologia , rappresentando una sottostima ecografica . 
lecografia ha permesso la diagnosi di 12 casi di ipertrofia ( valore medio di 0 , 86 mm ) , mentre lesame istologico ne ha riconosciuti 16 ( valore medio di 0 , 99 mm )  . 
the graphic shows , on the basis of measurements considering the hypoechoic layer only , higher dispersion of measurements in normotrophy and hypertrophy relative to hypotrophy even though for some authors , the values in hypotrophy are too small to be evaluated . 
sonography classified 23 segments as normotrophic ( mean value 0.52 mm ) as against 22 identified at histology ( mean value 0.56 mm ) ; 19 / 23 cases ( 86% ) considered normotrophic by sonography were confirmed by histology whereas 4 / 23 were hypertrophic at histology ( sonographic underestimation )  . 
the k - test statistic demonstrated excellent agreement ( 0.91 ) for the diagnosis of hypotrophy , good agreement ( 0.7 ) for the diagnosis of hypertrophy and fair - to - good agreement ( 0.47 ) for the diagnosis of normotrophy . 
furthermore , the more - or - less irregular morphology of vein walls and their inhomogeneous echogenicity , not distinguishable from surrounding tissue , do not always allow in vivo measurements of parietal thickness . 
3a , b histologically normal structure of a venous wall stained with masson 's trichrome ( a ) showing the different tunicae : intima ( i ) , media ( m ) and adventitia ( a )  . 
3a , b immagine istologica di normale struttura di parete venosa colorata con tricromica di masson ( a ) che mostra le differenti tuniche : lintima ( i ) , la media costituita da cellule muscolari lisce disposte a bande circolari o impacchettate con matrice extracellulare ( m ) e lavventizia ( a )  . 
secondo la nostra interpretazione , limmagine ecografica di un normale spessore parietale mostra una linea centrale ipoecogena ( i + m ) compresa da due linee iperecogene ( cfr doppia freccia ) : la pi interna che corrisponde allinterfaccia sangue - parete ( punte di freccia ) , la pi esterna che corrisponde allinterfaccia gel - avventizia ( a )  . pi o meno irregolare , e lecogenicit disomogenea , non sempre distinguibile dai tessuti circostanti , rendono agevole , in vivo , la sua misurazione . 
lautore , in particolare , ha dimostrato che il thi migliora la risoluzione spaziale laterale e lo spessore di fetta in funzione della profondit , mentre il compound quella di contrasto ed il riconoscimento dei bersagli anecogeni , infine che lhsonoct migliora la risoluzione spaziale laterale . 
ci nonostante la risoluzione spaziale massima per un trasduttore da 512 mhz , , sia pure con limpiego di tali algoritmi , sempre e comunque superiore a 0 , 4 mm , valore limite nel nostro studio tra una parete normotrofica ed una ipotrofica . 
daltra parte nel nostro studio basato sul confronto istologico , abbiamo constato che , anche se spessori inferiori a tale limite sono di difficile misurazione , possibile riconoscere perlomeno morfologicamente interfacce e . 
quindi , pur non essendo possibile effettuare attendibilmente misure quantitative al di sotto del limite di risoluzione del sistema , abbiamo potuto dimostrare in modo abbastanza chiaro che interfacce ad intervalli minori possono essere evidenziate . 
un ulteriore limite nella valutazione sperimentale rappresentato dalle difficolt nel far coincidere le misurazioni ecografiche con quelle effettuate nel preparato istologico , a causa delleterogeneit parietale , in particolare nei segmenti ipertrofici e normotrofici . 
lo studio ha messo inoltre in evidenza che la misura nellimmagine ecografica della parete venosa , comprendendo le due interfacce ecogene , non correla con la misura istologica , dato che produce una netta sovrastima globale . 
4a , b longitudinal histological sections ( a ) of a hypertrophic vein wall . derangement of the layers , mostly due to accumulation of smooth muscle cells and fibrous tissue green on masson 's trichrome corresponds to a thickened hypoechoic central line ( double arrow ) at ultrasound ( b )  . 
la disorganizzazione delle tuniche , in gran parte dovuta allaccumulo di cellule muscolari lisce e tessuto fibroso riconoscibile come verde alla colorazione tricromica , corrisponde nellimmagine ecografica ( b ) ad una linea centrale ispessita ( doppia freccia )  . 
this process , produced by haematic vaporisation , is presumably caused by the chromophore role of haemoglobin , which absorbs all of the laser 's beam energy [ 15 ] and consequently generates steam bubbles . 
furthermore , this procedure has fewer serious side effects than closure with radiofrequency ( molecular agitation produced by radiofrequency waves ) , which is associated in 16% of cases with major skin paraesthesias due to injury to surrounding nervous structures [ 16 ]  . 
in addition , evlt can be used in association with other treatments . nevertheless the first experiences with these procedures have demonstrated some limits . some authors have noted one the one hand the possibility of incomplete endothelial coagulations and early reopening of a treated venous portion and , on the other , the possibility of undesirable perforations causing haematoma and pain [ 16 , 17 ]  . 
it is even possible to assume that the knowledge of parietal thickness could be useful to sura che debba essere effettivamente considerata . oggi possiamo quindi ipotizzare una capacit dei nuovi ecografi digitali di riconoscere non solo la dilatazione del lume della vena grande safena , ma anche di potere correttamente riconoscerne lo spessore della parete . 
laffacciarsi di nuove tecniche terapeutiche che mirano a un trattamento conservativo , cio a sigillare la vena patologica , pi che a eliminarla , presupporrebbe , infatti , una corretta conoscenza della sua parete . 
gi noto infatti , fin dagli anni 80 , presso i sostenitori della terapia sclerosante [ 12 ] che le iniezioni endovasali di sostanze sclerosanti sono pi efficaci nei cosiddetti vecchi varicosi , proprio in relazione alla loro fibrosi cronica parietale , che esita in una ipotrofia parietale , piuttosto che nei giovani varicosi che , specie se donne in et fertile , vanno preferenzialmente indirizzati alla chirurgia tradizionale . 
 [ 13 ] hanno proposto un nuovo sistema conservativo per il trattamento delle varici dei tronchi safenici , utilizzando lenergia fornita dal laser attraverso una fibra ottica introdotta da una guida allinterno del vaso ( evlt )  . 
tale sottile fibra laser introdotta fino al punto di patologia , con linvio di flussi laser in tutte le direzioni , provoca un surriscaldamento del contenuto e quindi del contenente . 
 [ 14 ] hanno sottolineato come sia proprio la presenza del sangue allinterno del vaso che contribuisce alla dispersione omogenea del calore allinterno del vaso e sulle sue pareti , ottenendo cos , attraverso una vaporizzazione ematica , presumibilmente per la presenza dellemoglobina che si comporta come un cromoforo in grado di assorbire tutta lenergia del fascio laser [ 15 ] e di conseguenza di produrre bolle di vapore , una fotosclerosi dei due endoteli contrapposti e quindi una fibrosi da contatto connettivale tra le due pareti . 
carbonizzazioni e perforazioni dello strato connettivale sono stati dimostrati in vitro da proebstle in un recente lavoro [ 15 ] che distingueva , utilizzando un modello sperimentale , la trombosi del sangue vaporizzato dal danno parietale esercitato dal fascio laser diretto , in grado di penetrare fino a 0 , 3 mm di spessore . 
tale procedura , ha recentemente destato un notevole interesse , poich , unisce i vantaggi della scleroterapia ( poco invasiva e meno traumatica della chirurgia , brevi tempi di ospedalizzazione e anestesia locale ) a un minor numero di recidive . 
inoltre , essa gravata da meno effetti collaterali gravi rispetto al trattamento che utilizza radiofrequenze ( agitazione molecolare da onde a radiofrequenza ) , che si associa nel 16% dei casi a importanti parestesie cutanee da danno delle strutture nervose circostanti [ 16 ] e pu essere utilizzata in combinazione ad altri trattamenti . 
diversi autori hanno evidenziato le possibilit di incomplete coagulazioni endoteliali e ricanalizzazione precoce del tratto venoso trattato e per contro le possibilit di complicanze , soprattutto le indesiderate perforazioni , causa di ematomi e dolore [ 16 , 17 ]  . 
the digital us scanner used as a microscope in vivo would allow one to measure the thickness of pathological veins before treatment in order to distinguish patients with marked hypertrophy more frequent in young people suitable for surgery or longer exposition times with laser therapy from those with parietal atrophy caused by chronic disease . 
the second group of patients can be treated conservatively with evlt , reducing laser exposition time proportionally to the thickness of the hypotrophic wall . da a radiofrequenza , che pur utilizzando un principio differente dallevlt ( agitazione molecolare prodotta da onde a radiofrequenza ) , produce una embolizzazione del vaso e la pi antica scleroterapia che potrebbe utilizzare una quantit di sostanza sclerosante adeguata al vaso da trattare . 
bellelli , via ombrone 4 , i - 00198 rome , italy , tel . : + 39 - 06 - 6837243 , fax : + 39 - 06 - 6837346 , e - mail : abellelli@libero.it received : 8 april 2006 / accepted : 9 may 2006 / published online : 11 august 2006 abstract purpose . 
the mri exam was performed on a 0.2 - tesla ( t ) magnet and a 1.5 - t magnet using t1 - weighted spin echo ( se ) , t2 - weighted se and fat - suppression scans [ short - tau inversion recovery ( stir ) ] in axial , sagittal and coronal planes . 
out of 77 patients , 35% of the whole sample , 37 had a tear of the posteromedial fascicle ( type ii lesion ) , and the remaining 40 had anterolateral fascicle tears ( type iii )  . 
l ' esame rm stato eseguito con magnete permanente 0 , 2 tesla e superconduttivo 1 , 5 tesla , con sequenze se t1 e t2 pesate , e sequenze ottenute con la soppressione del segnale del tessuto adiposo ( stir ) , su piani assiali , sagittali e coronali . 
in 77 pazienti , che rappresentavano il 35% dei pazienti riesaminati , 37 mostravano una lesione del fascio postero - mediale ( ii grado di lesione )  . i restanti 40 pazienti mostravano una lesione del fascio anterolaterale , lesione di iii grado . 
l ' esame rm permetterebbe cos di qualificare il tipo di danno a livello del lcp e quindi come incida sulla stabilit articolare . key words posterior cruciate ligament injury mri knee stability parole chiave lesione del legamento crociato posteriore rm stabilit di ginocchio introduction introduzione many studies have reported that the posterior cruciate ligament ( pcl ) has biomechanical and neurosensory features that make it the main stabiliser in internal rotation and flexion of the knee . 
as with the anterior cruciate ligament ( acl ) , the pcl is composed of two molti studi in letteratura hanno sottolineato che il legamento crociato posteriore ( lcp ) ha delle caratteristiche biomeccaniche e neurosensoriali tali da renderlo il principale stabilizzatore nei movimenti di rotazione interna e flessione di ginocchio . 
in particular , studies on ligament strength show that the al is stronger than the pm portion ( 70% versus 30% ) and has the main role until knee flexion reaches 90 [ 79 ]  . in 1992 , for the first time , gross et al . 
the main limitation of t1 - weighted mri scans lies in their low contrast resolution , which does not allow one to distinguish between intraligament oedema and haematoma , the sign of a ruptured ligament . 
moreover , the gross classification does not consider the anatomical site of the injury , an important factor , especially in view of the different roles that the al and pm fascicles play in knee biomechanics . 
 this study proposes a new anatomical classification of acute traumatic pcl injuries using morphological t1weighted mri scans and high - contrast signal sequences , such as se t2 - weighted and fat - suppression images [ shorttau inversion recovery ( stir ) ]  . 
by using mri , we aimed to distinguish the more significant ligament injuries from those which are biomechanically less important . materials and methods we conducted a retrospective study of 4 , 000 mri scans carried out between june 2000 and june 2003 and selected 220 patients with acute pcl traumatic injury after car or sport accidents . 
ages ranged from 14 to 64 , with a mean age of 32.7. out of 220 patients , 125 underwent a new mri exam 1 - 3 months after sustaining the injury . 
la principale limitazione delle sequenze se t1 pesate dovuta alla bassa risoluzione di contrasto , che non permette di distinguere l ' edema intra - legamentoso della lesione , dall ' ematoma , segno di rottura a livello del legamento . 
inoltre , la classificazione di gross non considera la sede anatomica di lesione , dato di fondamentale importanza , in modo particolare in considerazione delle differenti caratteristiche biomeccaniche dei fasci al e pm . l ' obiettivo del nostro studio di proporre una nuova classificazione delle lesioni acute traumatiche del lcp , utilizzando sia sequenze morfologiche se t1 pesate , sia sequenze ad alto contrasto come le sequenze se t2 pesate e le sequenze ottenute con la soppressione del segnale del tessuto adiposo . 
attraverso l ' esame rm il nostro intento quello di poter distinguere le lesioni legamentose meno significative , da quelle che lo sono di pi da un punto di vista biomeccanico . materiali e metodi abbiamo condotto uno studio retrospettivo su 4000 risonanze magnetiche di ginocchio , da giugno 2000 a giugno 2003 . abbiamo preso in considerazione nel nostro studio 220 pazienti , 157 maschi e 63 femmine , con lesione traumatica acuta del lcp dopo incidente stradale o sportivo , con et compresa tra 14 e 64 anni , con una media di 32 , 7 anni . 
i 220 pazienti in cui stata evidenziata la lesione a carico del lcp erano stati precedentemente valutati clinicamente e classificati come pazienti con instabilit posteriore . abbiamo incluso nello studio sia pazienti con lesione isolata di lcp , che pazienti con lesione complessa , associata a patologia meniscale , osteocondrale o capsulare . l ' esame rm stato eseguito a pazienti supino , con ginocchio flesso tra 0 e 15 , con magnete permanente 0 , 2 tesla ( artoscan , esaote , genova , italia ) e superconduttivo 1 , 5 tesla ( simphony siemens , erlangen , germania ) , usando sequenze se t1 e se t2 pesate e sequenze ottenute con la soppresione del grasso ( stir ) , su piani assiali , sagittali e coronali . 
lo spessore di strato stato compreso tra 3 e 5 mm , con gap di 0 mm e fov variabile tra 170200 mm ; la matrice stata di 256x256 sul magnete 0 , 2 tesla , mentre era di 512x512 su magnete 1 , 5 tesla . 
the thin area with intermediate signal intensity appearing within the pcl on t1 - weighted images but not on t2 - weighted scans was considered to be due to the magic angle effect . 
we did not take into account the high - intensity signal within the ligament due to eosinophil degeneration in arthritic knees . results fifty - five of the 220 patients ( 25% of cases ) had an area of increased signal intensity within the pcl on both t1and t2 - weighted images ; the edges appeared homogeneously continuous and hypointense ( gross type i )  . 
in the last 22 patients ( 10% ) , we detected complete tear of the pcl , which presented no continuity of the remaining ligament fibres on high - contrast images . on the basis of our results , we propose a new classification of pcl traumatic injuries , which takes in consideration the extent of remaining fibres and the exact anatomical site of the lesion . 
this way , we can distinguish between posteromedial pcl ligament injuries on the dorsal aspect from those of the anterolateral fascicle ( ventral aspect )  . discussion the mri classification of posterior ligament injuries was first published by gross et al [ 10 ]  . 
il piano assiale stato posizionato parallelo al piano tibiale o meniscale , mentre il piano coronale stato allineato alla tangente bicondiloidea posteriore . in rm stata considerata come lesione del lcp il caso in cui la banda a bassa intensit del segnale , che rappresenta il legamento , appariva discontinua , con un ' area di alta intensit del segnale che coinvolgeva uno dei due versanti del legamento . 
abbiamo escluso dallo studio l ' iperintensit del segnale intra - legamentosa , nelle ginocchia artrosiche , dovuta alla degenerazione eosinofila . risultati il nostro studio ha condotto ai segmenti risultati . 
cinquantacinque dei 220 pazienti , ( il 25% dei casi ) ha mostrato nelle immagini rm un ' area di iperintensit del segnale all ' interno del legamento , sia nelle immagini t1 che in quelle t2 pesate , con margini omogeneamente continui e ipointensi ( di i grado secondo gross )  . 
sebbene in questi casi lo spessore del legamento risultato lievemente aumentato , il decorso intraarticolare del legamento apparso normale , cos come la rappresentazione del tessuto adiposo all ' interno della gola inter - condiloidea . 
il legamento appariva continuo nelle sequenze se t2 pesate ed in quelle ottenute con la soppressione del segnale del tessuto adiposo . lo spessore del legamento era lievemente aumentato , tuttavia i margini risultavano continui , anche se modicamente disomogenei . 
in accordo con la classificazione di gross , le lesioni del lcp appartenenti al iii grado , ossia lesioni complete , sono state individuate in 77 pazienti ( 35% )  . 
nella nostra esperienza abbiamo confrontato le sequenze se t1 pesate con le sequenze ad alto contrasto in rm e abbiamo notato che le lesioni del legamento sul versante ventrale ( sede del fascio al ) sono state evidenziate in 40 casi , poco pi della met , mentre quelle sul versante dorsale ( sede del fascio pm ) , sono state osservate in 37 casi . 
nei rimanenti 22 pazienti ( il 10% ) abbiamo identificato una lesione completa del lcp , con soluzione di continuo completa del legamento , senza evidenza di fibre residue nelle sequenze ad alto contrasto . quindi , in relazione a quanto stato evidenziato nel nostro studio , abbiamo deciso di proporre una nuova classifitable 1 magnetic resonance imaging ( mri ) grading of posterior cruciate ligament ( pcl ) injuries on spin - echo ( se ) t1 - weighted images [ 10 ] a . 
both edges of the ligament show homogeneously low signal intensity the high signal intensity is within the ligament and in one of two edges ; partial lesion the high signal intensity involves the entire ligament ; complete lesion tabella 1 gradi di lesione in rm delle lesioni del lcp , con sequenze se t1 - pesate [ 10 ] grado immagine rm il legamento crociato posteriore mostra omogenea bassa intensit del segnale ed continuo iperintensit del segnale all ' interno del legamento . 
type ii includes partial lesions , in which high signal intensity is seen in the central portion within the ligament as well as one of the two ventral or dorsal margins of the ligament . 
type iii injury is described as high signal intensity extending to the entire ligament and including both the dorsal and the ventral aspects ; this situation has been classified by gross as a complete injury . 
the gross classification presents some important limitations , in particular , the lack of comparison between t1weighted se images and high - contrast sequences , such as t2 - weighted se or stir scans . 
mri techniques with fat suppression and t2 se can make the diagnosis easier because the intact fascicle which shows high signal intensity on the t1 - weighted scan displays low signal intensity on t2 - weighted images , as the signal of the intraligament oedema is abated by the contrast of the sequence . 
in questo modo possiamo distinguere tra lesioni del fascio pm del lcp , sul versante dorsale , da quelle del versante ventrale , sede del fascio al . discussione la classificazione delle lesioni traumatiche del lcp , basata sui dati rm , stata pubblicata per la prima volta da gross et al . 
in questo modo sono stati distinti tre differenti gradi di lesione ( tabella 1 )  . nel i grado , gli autori hanno incluso le lesioni intra - legamentose , dove il lcp era continuo , normale e a bassa intensit del segnale sia sul versante dorsale che su quello ventrale . 
nel ii grado sono state catalogate le lesioni parziali , in cui l ' iper - intensit del segnale interessava la porzione interna del legamento ed uno dei due versanti , ventrale o dorsale . 
secondo gross questa rappresentava una lesione completa . la classificazione di gross ha , per , alcune importanti limitazioni , prima tra tutte l ' assenza di comparazione tra le sequenze se t1 pesate e le sequenze ad alto contrasto , come le se t2 o le sequenze stir . 
in accordo con quanto ottenuto dai nostri studi ed in altre recenti esperienze descritte in letteratura [ 1115 ] , l ' integrazione ed il confronto tra due differenti sequenze a diverso contrasto di fondamentale importanza . 
nelle sequenze se t1 pesate l ' edema , l ' ematoma e la soffusione siero - ematica hanno la stessa intensit del segnale sia nelle lesioni acute che nelle lesioni subacute . 
b rappresentazione del lcp da cadavere durante l ' estensione . ion , a correct classification of pcl injuries needs to take into account the anatomical site of injury on mri . 
for this reason , our new classification of traumatic pcl injuries considers four different types of acute lesion ( table 2 ) : type i : the high signal intensity is within the ligament in both sequences . 
le tecniche di rm ad alto contrasto , ( se t2 pesate e stir ) , possono essere d ' aiuto per una diagnosi migliore , per il fatto che il fascio legamentoso non interessato dalla lesione , che comunque table 2 anatomical classification of acute posterior cruciate ligament ( pcl ) injuries [ 11 ] type magnetic resonance imaging normal pcl : homogeneously low signal intensity on all sequences intraligament lesion : high signal intensity within the ligament . 
the ventral and dorsal ligament edges have homogeneously low signal intensity partial lesion : high intensity signal on the dorsal edge of the ligament , which is the anatomical site of the posteromedial ( pm ) fascicle . 
the anterolateral ( al ) fascicle shows low signal intensity partial lesion : high signal intensity on the ventral edge of the ligament , which is the anatomical site of the anterolateral ( al ) fascicle ( the main one in knee biomechanics )  . 
il fascio al mostra bassa intensit del segnale normale lesione parziale : iperintensit del segnale sul versante ventrale del legamento , sede anatomica del fascio al ( prevalente nella biomeccanica di ginocchio )  . 
4a - c type ii : high signal intensity involves the internal portion of the ligament and its dorsal border [ posteromedial ( pm ) fascicle ] on the t1 - weighted scan ( a )  . 
4a - c ii grado : iperintensit del segnale in sede intralegamentosa e con coinvolgimento del margine dorsale ( fascio pm ) nelle sequenze se t1 pesate ( a )  . 
in questi casi infatti le sequenze se t2 pesate o fat sat sono in grado di abbattere il segnale dell ' edema intra - legamentoso . al momento attuale non stata ancora ben sottolineata l ' importanza della biomeccanica e della sede anatomica di lesione . 
il legamento , da un punto di vista anatomico , composto da due differenti gruppi di fasci fibrosi , il fascio al ed il fascio pm , distinti per la loro inserzione su tibia e femore . 
il fascio al situato sul versante ventrale del lcp , mentre il fascio pm si trova sul versante dorsale . secondo noi , la corretta classificazione delle lesioni del lcp deve prendere in considerazione la reale sede anatomica del danno in rm . 
per questo motivo la nuova classificazione anatomica delle lesioni del lcp descrive 4 tipi differenti di lesione traumatica acuta ( tabella 2 )  . i grado : l ' alta intensit del segnale si trova all ' interno del legamento , in entrambe le sequenze . 
5a , b type iii : high signal intensity involves the internal portion of the ligament and its ventral border [ anterolateral ( al ) fascicle ] on t1and t2 - weighted images ( a )  . 
5a , b iii grado : nelle sequenze se t1 pesate l ' iperintensit del segnale evidente sull ' interno del legamento e nel versante ventrale ( fascio al ) ( a )  . 
mri detection of a traumatic injury affecting the ventral edge of the pcl , the anatomical site of the al fascicle , denotes more severe damage in relation to clinical - arthrometric and stress radiography data [ 21 ]  . 
we are strongly convinced it is clinically and prognostically important to be able to recognise on the first mri examination injuries that are very likely to develop into serious knee instability . 
questo causa un incremento nell ' instabilit di ginocchio che , nell ' arco di poco tempo , portano ad un precoce danneggiamento delle altre strutture articolare . in questi casi il chirurgo ortopedico ha maggiori difficolt nel ripristinare l ' assetto articolare corretto con la sola ricostruzione isolata del lcp . 
per questo motivo molto importante essere in grado definire quale sia il reale danno a carico del lcp nella fase acuta e sub - acuta . , ed eventuali lesioni capsulari associate . 
nel caso in cui in rm si osserva una lesione del fascio ventrale del legamento , sede anatomica del lcp , questa ha una gravit maggiore , in relazione ai dati clinico - artrometrici e alle radiografie in stress [ 21 ]  . siamo convinti che essere in grado di riconoscere al primo esame rm il tipo di lesione che svilupper nel tempo una grave instabilit di ginocchio da quelle meno significative da un punto di vista biomeccanico rappresenta una fattore clinico e prognostico importante . 
la rm ha evidenziato 26 traumi minori e 55 maggiori . la rm e l ' ecografia hanno mostrato una concordanza completa in 71 pazienti ( sede , tipo , entit della lesione )  . 
sono stati riportati 10 falsi negativi all ' ecografia , di cui 6 lesioni minori e 4 maggiori . la sensibilit dell ' ecografia nell ' identificare correttamente i traumi muscolari risultata dell ' 87 , 65% . 
la rm rileva le lesioni misconosciute all ' ecografia e valuta con maggiore precisione l ' entit e la sede del danno muscolare . parole chiave muscoli lesioni muscolari ecografia risonanza magnetica introduction introduzione acute muscle injuries are frequently observed in both amateur and professional athletes . 
the risk of injury is increased by poor preparation , inadequate warmup , excessive fatigue , slippery or hard playing surfaces , exposure to cold , muscle tension due to emotional factors ( performance anxiety ) and previous muscle injuries le lesioni muscolari acute sono di frequente osservazione nelle discipline sportive praticate sia a livello amatoriale che agonistico . 
le discipline pi a rischio sono il calcio , l ' atletica leggera e tutti gli sport in cui la muscolatura viene sollecitata in maniera massimale anche se per brevi periodi . i fattori di rischio sono l ' inadeguata preparazione , lo scarso riscaldamento , l ' eccessivo affaticamento , i terreni di gioco scivolosi o pesanti , l ' eccessiva esposizione al freddo , la tentable 1 classification of muscle injuries minor traumas major traumas indirect delayed - onset muscle soreness , traumas lengthenings , contractures strains direct traumas mild contusions severe contusions ( haematomas ) ttaabbeellllaa 11 classificazione dei traumi muscolari traumi minori traumi maggiori traumi indiretti traumi diretti doms elongazioni contratture contusioni lievi distrazioni contusioni gravi ( ematomi ) [ 1 , 2 ]  . 
in sports such as football or athletics , the posterior thigh muscles [ 3 , 4 ] , adductors [ 1 ] , femoral quadriceps [ 1 , 5 ] and sural triceps [ 1 , 3 , 5 ] are most commonly involved . muscle injuries can be distinguished into minor or major injuries [ 6 ]  . 
they may also be classified according to mechanism of injury into muscle strains , the origins of which are internal and triggered by exaggerated or untimely contraction ; and contusions , the causes of which are external . 
major injuries comprise first - , secondor third - degree strains produced by an indirect trauma and severe contusions resulting in the formation of a haematoma [ 7 , 8 ] ( table 1 )  . diagnostic imaging is indispensable for classifying the type of muscle injury , estimating the extent of the lesion , predicting possible complications and establishing recovery times . 
magnetic resonance imaging ( mri ) allows for correct diagnosis of even small muscle injuries and enables detection of even minimal muscle alterations that are not macroscopically detectable [ 815 ]  . the aim of our study was to analyse and compare the sensitivity of ultrasound ( us ) in relation to mri and define a diagnostic algorithm for the study of muscle injuries . materials and methods between june 2003 and june 2004 , we studied 81 professional and amateur football players with a mean age of 26.2 ( range 1832 years ) who presented with lower - limb muscle injuries ( 27 lower - leg and 54 thigh injuries )  . 
thirteen patients reported intense muscle pain developing within hours or 1 day of exercise , but they could not remember the kind of trauma sustained and the time of occurrence . 
negli sport come il calcio o l ' atletica leggera i muscoli maggiormente colpiti sono quelli posteriori della coscia [ 3 , 4 ] , gli adduttori [ 1 ] , il quadricipite femorale [ 1 , 5 ] e il tricipite surale [ 1 , 3 , 5 ]  . le lesioni traumatiche muscolari si possono distinguere , in relazione alla loro gravit , in traumi minori e traumi maggiori [ 6 ]  . 
un altro criterio classificativo considera il meccanismo lesivo e consente di differenziare i traumi di tipo distrattivo , la cui causa intrinseca al muscolo stesso sottoposto ad una contrazione esagerata o mal collocata nel tempo , dai traumi di tipo contusivo , la cui causa esterna . 
i traumi minori comprendono la contrattura , l ' elongazione , la doms ( delayed onset muscle soreness ) , indotti da un meccanismo indiretto , e la contusione lieve , indotta da un agente lesivo che agisce dall ' esterno . 
i traumi maggiori consistono , in relazione alla gravit , in distrazioni di primo , secondo e terzo grado , conseguenza di un trauma indiretto , e in contusioni gravi che comportano la formazione di un ematoma [ 7 , 8 ] ( tabella 1 )  . la diagnostica per immagini delle lesioni muscolari indispensabile per classificare il tipo di trauma , valutare l ' entit del danno , l ' eventuale insorgenza di complicanze e stabilire i tempi di recupero . 
la risonanza magnetica ( rm ) permette una diagnosi corretta nelle lesioni muscolari traumatiche , anche di piccole dimensioni , e permette di rilevare le minime alterazioni muscolari non macroscopicamente obiettivabili [ 815 ]  . lo scopo del nostro lavoro di analizzare e confrontare il valore diagnostico , in termini di sensibilit , dell ' ecografia ( us ) rispetto alla risonanza magnetica e di definire un algoritmo diagnostico nello studio dei traumi muscolari . materiali e metodi nel periodo tra giugno 2003 e giugno 2004 sono stati studiati 81 calciatori professionisti e dilettanti con et media di 26 , 2 anni ( range 1832 anni ) che presentavano un quadro clinico suggestivo di lesione muscolare traumatica , localizzata all ' arto inferiore ( 27 traumi della gamba e 54 della coscia )  . 
tredici pazienti riferivano la comparsa di un dolore muscolare intenso poche ore dopo o il giorno successivo rispetto allo svolgimento dell ' attivit sportiva , non ricordavano il momento e il tipo di trauma . 
ventisei pazienti riferivano la comparsa di un dolore muscolare acuto , violento , comparso durante lo svolgimento dell ' attivit sportiva in assenza di un trauma diretto ; 10 atleti non avevano sospeso l ' attivit , mentre negli altri 16 il dolore era stato cos intenso da costringerli a sospendere la gara o l ' allenamento . 
trentadue pazienti riferivano con precisione un trauma diretto , come lo scontro con un avversario o l ' impatto con il terreno , in seguito al quale era insorto il dolore muscolare . 
thirty - two patients reported having sustained direct traumas , such as collisions or falls , which had brought on the paof these , 29 had suspended their activity immediately after the trauma . 
physical examination was carried out to assess the site of pain , muscle tenderness , muscular hypertonia , functional impotence , reduced muscle strength , increased muscle volume , subcutaneous swelling and ecchymosis . all patients underwent us shortly after the injury ( 672 hours afterwards ) and mri within 5 days . 
to correctly evaluate lesion size , additional scans were performed in all planes and with various sequences , depending on the extent and anatomical characteristics of the lesions . diagnostic sensitivity of us was compared with that of mri , which was considered the gold standard . 
the study group was subdivided on the basis of patient history and clinical findings , physical examination and subsequent diagnostic investigations ( table 1 )  . results mri detected 26 minor and 55 major traumas in the 81 patients examined . 
 the seven patients with doms ( three in the medial head of the gastrocnemius , four in the rectus femoris ) , all of whom had a poor level of fitness , had diffuse pain in the affected muscle , which had typically appeared the day after athletic activity . 
con l ' esame obiettivo sono stati valutati la sede del dolore spontaneo , la dolorabilit alla palpazione del muscolo interessato , l ' eventuale presenza di ipertono muscolare , l ' impotenza funzionale , la riduzione della forza muscolare , l ' aumento del volume del muscolo leso , la tumefazione del tessuto sottocutaneo e l ' eventuale presenza di un ' ecchimosi sottocutanea . tutti i pazienti sono stati sottoposti ad ecografia nelle ore successive al trauma ( da 6 ad un massimo di 72 ore ) e a risonanza magnetica entro cinque giorni dal trauma . 
l ' ecografia stata condotta con apparecchio technos ( esaote biomedica , genova , italia ) , utilizzando transduttori lineari con frequenze comprese tra 7 , 5 e 13 mhz . 
sono state eseguite scansioni assiali e longitudinali del muscolo leso e dei muscoli adiacenti ; sono stati inoltre valutati la fascia muscolare , i tendini , le aponeurosi ed il tessuto sottocutaneo nella regione anatomica in esame . 
sono state effettuate sequenze assiali se t1pesate ( tr 400 ms , te 20 ms ; spessore di strato 8 mm , intervallo tra gli strati 0 , 8 mm ) , assiali se t2 - pesate ( tr 3000 ms , te 100 ms ; spessore di strato 8 mm , intervallo tra gli strati 0 , 8 mm ) e coronali stir ( short time inversion recovery ) ( tr 3600 ms , te 20 ms , ti 90 ms ; spessore di strato 7 mm , intervallo tra gli strati 0 , 7 mm )  . 
abbiamo considerato come falsi negativi sia i casi in cui l ' ecografia non ha evidenziato alcuna lesione dimostrata dalla risonanza magnetica sia i casi nei quali l ' ecografia ha sottostimato il grado della lesione . 
sulla base dei dati clinico - anamnestici , dell ' esame obiettivo e delle successive indagini diagnostiche , abbiamo suddiviso il gruppo di pazienti secondo la classificazione riportata in tabella 1 . risultati la risonanza magnetica , negli 81 pazienti , ha evidenziato 26 traumi minori e 55 maggiori . 
fra i traumi minori sono state evidenziate 7 doms , 5 elongazioni , 6 contratture e 8 contusioni lievi ; 26 traumi maggiori sono risultati distrazioni mentre 29 erano ematomi ( tabella 2 )  . 
 the five patients with lengthening ( rectus femoris in four patients , medial head of the gastrocnemius in one ) had acute localised muscle pain during exercise that was exacerbated by contraction or stretching . 
mri revealed a similar pattern to that seen in patients with doms ; us agreed with mri in terms of both lesion site and extent in four cases whereas it failed to detect any alteration in a fifth patient . the six patients with contractures ( medial head of gastrocnemius in four patients , rectus femoris in two patients ) had diffuse muscle pain that developed within hours or days of physical exercise and was brought on by muscle contraction against resistance . 
in all these patients , mri showed slight signal hyperintensity in axial se t2 - weighted and coronal stir sequences whereas us revealed vague echostructural inhomogeneity in five patients and was negative in one case ( one false negative )  . among the eight patients in whom mri revealed mild contusions ( signal hyperintensity in se t1 - weighted sequences , se t2 - weighted and stir sequences ) , five suffered intense pain in the affected muscle but had no history of a direct trauma whereas three suffered pain in the area of the contusion . 
la risonanza magnetica mostrava iperintensit di segnale del muscolo dolorante nelle sequenze se t2 - pesate assiali e nelle stir coronali , dovuta unicamente all ' edema e nessuna alterazione dell ' intensit del segnale nelle sequenze se t1 - pesate assiali . 
l ' ecografia era risultata negativa in 3 atleti ( falsi negativi ) , mentre negli altri 4 permetteva di rilevare una ipoecogenicit disomogenea , dovuta all ' edema , della struttura muscolare in esame . nei 5 pazienti con elongazione ( in 4 localizzata nel muscolo retto femorale ed in 1 nel muscolo gemello mediale ) , il quadro clinico era caratterizzato da un dolore muscolare acuto insorto durante l ' attivit sportiva , ben localizzato , esacerbato dalla contrazione o dall ' allungamento muscolare ; tutti i pazienti ricordavano con precisione il momento dell ' insorgenza del dolore . 
la risonanza magnetica mostrava un quadro del tutto simile a quello dei pazienti con doms ; l ' ecografia concordava con la risonanza magnetica sia per quanto riguardava la sede che per l ' entit della lesione in 4 pazienti , mentre in un altro paziente non dimostrava alcuna alterazione del muscolo . i 6 pazienti con contrattura ( 4 pazienti con localizzazione a livello del gemello mediale e 2 a livello del retto femorale ) riferivano un dolore muscolare mal localizzato , insorto a distanza di qualche ora o qualche giorno dall ' attivit sportiva , che compariva durante la contrazione muscolare contro resistenza . 
in tutti questi pazienti , la risonanza magnetica mostrava una lieve iperintensit di segnale nelle sequenze se t2 - pesate assiali e nelle stir coronali ; l ' ecografia mostrava una sfumata disomogeneit ecostrutturale muscolare in 5 pazienti , mentre risultava negativa in uno ( 1 falso negativo )  . degli 8 pazienti con quadro rm di piccola contusione ( iperintensit del segnale nelle sequenze se t1 - pesate , se t2 - pesate e stir ) , 5 lamentavano dolore intenso al muscolo interessato , ma senza il ricordo anamnestico di trauma diretto e 3 riferivano dolore nella sede del trauma contusivo ; l ' ecografia , eseguita dopo poche ore dal trauma , aveva confermato il quadro contusivo in 7 pazienti evidenziando una zona di ipoecogenicit associata a piccole aree iperecogene a livello del muscolo dolente ; in 1 paziente , invece , l ' ecografia era risultata negativa . 
la sede delle piccole contusioni era il muscolo retto femorale in 3 pazienti , il muscolo vasto intermedio in 2 pazienti , il muscolo gemello mediale in 2 pazienti ed il muscolo bicipite femorale in 1 paziente . ventisei pazienti mostravano un quadro clinico caratterizzato da dolore acuto insorto durante l ' attivit sportiva , impotenza funzionale e riduzione della forza . 
l ' esame obiettivo evidenziava impotenza funzionale e riduzione di forza in alcuni casi di grado lieve ( i grado ) , in altri moderato ( ii grado ) o grave ( iii grado )  . 
us and mri provided the following results : in 22 subjects , the two techniques were perfectly concordant in identifying and estimating the extent of the lesions and detecting discontinuity of tertiary bundles , reactive muscle oedema , interstitial haemorrhage and / or haematoma . 
in another four patients , mri produced the same results as those described above whereas us was negative in two patients and detected only discontinuity of muscle fibres in the other two , thus underestimating the degree of the lesion . 
 twenty - nine subjects with a history of severe direct trauma had functional impotence , strength reduction , muscle hypertonia and increased muscle volume proportional to pain intensity ; five patients had evidence of extensive subcutaneous ecchymosis distal to the lesion . 
in all these patients , both us and mri correctly detected a haematoma , with varying characteristics depending on stage of development . the sites of muscle injury were as follows : 11 in the rectus femoris , nine in the medial head of the gastrocnemius , four in the vastus lateralis , three in the vastus intermedius and two in the biceps femoris . 
us sensitivity by type of trauma was 57% for doms , 80% for lengthening , 83% for contracture , 84% for muscle strain , 87.5% for mild contusion and 100% for severe contusion ( table 3 )  . no fornito i seguenti risultati : in 22 pazienti le due tecniche sono state perfettamente concordi nell ' identificare e stimare l ' entit della lesione evidenziando discontinuit dei fasci terziari , edema muscolare reattivo , emorragia interstiziale e / o un ematoma . 
in altri 4 pazienti la risonanza magnetica aveva fornito gli stessi risultati sopra descritti , mentre l ' ecografia era risultata negativa in 2 pazienti , mentre negli altri 2 aveva mostrato soltanto una discontinuit delle fibre muscolari , sottostimando il grado della lesione . 
la localizzazione delle lesioni muscolari era la seguente : 11 nel muscolo retto femorale , 9 nel muscolo gemello mediale , 4 nel muscolo vasto laterale , 3 nel muscolo vasto intermedio e 2 nel muscolo bicipite femorale . in sintesi , la risonanza magnetica e l ' ecografia hanno mostrato una concordanza completa in 71 pazienti circa la sede , il tipo e l ' entit della lesione . 
non stato possibile calcolare i valori di specificit e di accuratezza diagnostica poich i pazienti non sintomatici ed ecograficamente negativi non sono stati sottoposti alla risonanza magnetica , per ovvii motivi di costi e tempi di attesa . 
sono stati calcolati i valori di sensibilit dell ' ecografia nei 2 sottogruppi di pazienti con lesioni maggiori ( 55 casi ) e con lesioni minori ( 26 casi ) , ottenendo un valore di sensibilit del gruppo con lesioni maggiori del 92 , 72% e di quello con lesioni minori del 76 , 92% . 
stata , inoltre , calcolata la sensibilit dell ' ecografia in considerazione del tipo di trauma , ottenendo valori del 57% per le doms , dell ' 80% per le elongazioni , del l ' 83% per le contratture , dell ' 84% per le distrazioni , dell ' 87 , 5% per le contusioni lievi , del 100% per le contusioni gravi ( tabella 3 )  . discussione traumatic muscle lesions are particularly common in football players and mainly affect the lower limbs , particularly the thigh and calf . 
the most frequently affected muscles are the posterior thigh muscles [ 3 , 4 ] , the adductors [ 1 ] , femoral quadriceps [ 1 , 5 ] and sural triceps [ 1 , 3 , 5 ]  . 
the decision whether to treat conservatively or surgically is crucial given that appropriate treatment can reduce recovery times and increase the chances le lesioni traumatiche muscolari sono particolarmente ricorrenti nei calciatori e interessano prevalentemente l ' arto inferiore , la coscia e il polpaccio . 
i muscoli pi frequentemente interessati sono quelli posteriori della coscia [ 3 , 4 ] , gli adduttori [ 1 ] , il quadricipite femorale [ 1 , 5 ] e il tricipite surale [ 1 , 3 , 5 ]  . 
in our experience , only a combination of imaging and accurate clinical examination makes it is possible to achieve correct diagnosis . in our study , we observed only 26 minor traumas out of a total of 81 traumas ( 32% )  . 
in letteratura non esiste una classificazione univoca dei traumi muscolari e risulta ancora pi complessa quella dei traumi minori , i quali presentano quadri di imaging sovrapponibili . nella nostra esperienza , soltanto attraverso l ' integrazione dell ' esame strumentale con un accurato esame clinicoanamnestico possibile formulare una diagnosi esatta . nel nostro studio abbiamo osservato solo 26 traumi minori su 81 traumi complessivi ( 32% )  . 
 [ 22 ] hanno osservato , in un gruppo di 40 pazienti con doms , che l ' ecografia ha una bassa sensibilit nell ' individuare le alterazioni muscolari della doms . nei sette pazienti con doms da noi studiati , la risonanza magnetica ha correttamente individuato l ' edema muscolare , ma il pattern aspecifico e per un suo corretto inquadramento necessaria l ' integrazione con dati di laboratorio , quali il dosaggio della creatin - chinasi [ 19 ]  . 
de smet [ 4 ] sostiene che la risonanza magnetica attendibile solo se preceduta da un valido inquadramento clinico che permetta di scegliere le sequenze pi adatte e orientare correttamente le scansioni ed ha osservato valori di specificit e sensibilit rispettivamente del 80% e del 83% nella diagnosi delle contratture e delle elongazioni . 
questo dato da ricondurre all ' edema muscolare di grado elevato che facilita l ' identificazione della lesione . in queste situazioni l ' ecografia dimostra una diffusa ipoecogenicit con dislocazione dei fasci terziari . 
in seven of our patients with doms , although mri correctly detected the muscle oedema , the pattern was nonspecific and the correct diagnosis required integration with laboratory findings such as creatine - kinase assay [ 19 ]  . de smet [ 4 ] states that mri is reliable only if it is preceded lit della ecografia sale ancora , seppur di pochi punti percentuali , nelle contusioni di lieve entit . 
nella nostra esperienza , l ' imaging ecografico delle piccole contusioni non si differenzia considerevolmente da quello degli altri traumi minori ; in tutti i casi , infatti , il quadro caratterizzato da imbibizione by a thorough clinical assessment that enables selection of the most appropriate sequences and scan planes and has observed specificity and sensitivity values of 80% and 83% , respectively , for diagnosis of contractures and lengthening . this may also be correlated to the presence of considerable muscle oedema , which facilitates lesion identification . 
in our experience , the us imaging pattern of small contusions does not differ much from that of other minor traumas ; in all cases , it shows muscle oedema without interruption of the continuity of muscle fibres . 
differentiation was only possible on the basis of the patient 's history . as regards major traumas , us had an 84% sensitivity in identifying muscle strathe extent of tissue alterations affects the us pattern . 
the reason for such underestimation was that both lesions were located deep in the femoral quadriceps and therefore less amenable to us . us examination enables identification of typical lesions of muscle strains : discontinuity of tertiary bundles , reactive oedema and haematoma . 
in first - degree strains , the involvement of a small number of myofibrils can make it difficult to recognise the lesion with us so that the use of mri is necessary . 
more - severe lesions ( second and third degree ) with involvement of a larger number of myofibrils , will exhibit a hypoechoic or anechoic haematoma , which can remain localised or extend along the bundles . 
immediately after a trauma , the true extent of a lesion may be masked by a hyperechoic haemorrhage whereas us done 4872 h afterwards will reveal the evolution of the haematoma and the extent of the area affected [ 7 , 10 , 23 , 24 ]  . 
in cases of complete tears of the muscle belly , the retracted muscle bundles have the typical us appearance of a bell clapper surrounded by a hypoechoic haematoma [ 7 , 25 ]  . 
a dynamic examination is fundamental in all cases and particularly in first - degree strains , as it enables detection of the separation and dislocation of tertiary bundles and evaluation of the effective extent of the lesion [ 7 , 24 , 26 ]  . muscle strains are recognised at mri by changes in muscle volume and composition , variations in signal intensity and pathological alterations of surrounding tissues [ 1 , 27 , 28 ]  . 
coronal or sagittal images along the muscle belly axis make it possible to define the extent of the lesion [ 3 , 4 , 15 ]  . an important finding of our study was that in all patients with severe contusion , the haematoma was detected by both us and mri , leading to a sensitivity of 100% for us . 
la differenziazione stata possibile solo sulla base dei dati anamnestici . per quanto riguarda i traumi maggiori , l ' ecografia ha ottenuto un valore di sensibilit dell ' 84% nell ' individuazione delle distrazioni . 
l ' entit delle alterazioni tissutali condiziona l ' aspetto del quadro ecografico ; in effetti , abbiamo notato differenze significative tra le distrazioni di iii grado , sempre individuabili , e quelle di i grado . 
in 2 atleti , considerati come dei falsi negativi , l ' ecografia , pur sottostimandone l ' entit , aveva effettivamente localizzato la lesione , valutata poi alla risonanza magnetica come di ii grado . 
la sottostima da imputarsi al fatto che tutte e due le lesioni si trovavano in regioni profonde del quadricipite femorale e quindi pi difficilmente esplorabili con la tecnica ecografia . lo studio ecografico consente di evidenziare le lesioni caratteristiche delle distrazioni muscolari : la discontinuit dei fasci terziari , l ' edema reattivo e l ' ematoma . 
nelle lesioni di maggiore gravit ( ii e iii grado ) , in cui coinvolto un numero maggiore di miofibrille , si evidenzia un ematoma ipoo anecogeno che pu rimanere localizzato o estendersi lungo le fasce . 
nel periodo immediatamente successivo al trauma , lo spandimento emorragico iperecogeno pu mascherare l ' entit reale della lesione ; un ' ecografia eseguita dopo 4872 ore rivela l ' evoluzione dell ' ematoma e l ' estensione dell ' area lesa [ 7 , 10 , 23 , 24 ]  . 
in caso di rottura completa del ventre muscolare , i fasci muscolari retratti appaiono all ' ecografia con la tipica immagine a batacchio di campana , circondati dall ' ematoma ipoecogeno [ 7 , 25 ]  . 
l ' esame dinamico fondamentale in tutti i casi e particolarmente nelle distrazioni di primo grado , dal momento che consente di rilevare l ' allontanamento e la dislocazione dei fasci terziari e di valutare l ' effettiva estensione della lesione [ 7 , 24 , 26 ]  . 
le distrazioni sono riconoscibili alla risonanza magnetica per i cambiamenti del volume e dell ' architettura muscolare , per le variazioni dell ' intensit del segnale , per le alterazioni patologiche a carico dei tessuti circostanti [ 1 , 27 , 28 ]  . 
le immagini coronali o sagittali , lungo l ' asse del ventre muscolare , permettono di definire l ' estensione della lesione [ 3 , 4 , 15 ]  . 
un dato importante , rilevato dal nostro studio , che in tutti i pazienti con contusione grave , l ' ematoma stato evidenziato sia dall ' ecografia che dalla risonanza magnetica : abbiamo ottenuto quindi un valore di sensibilit dell ' ecografia pari al 100% . 
secondo peetrons [ 12 ] possibile una classificazione ecografica delle lesioni muscolari maggiori in 4 tipi , in base alla percentuale di muscolo coinvolto , ma essenziale operare una distinzione tra lesioni che hanno provocato un ematoma e lesioni che hanno provocato solo una lacerazione delle fibre muscolari . 
questo un criterio fondamentale per stabilire il periodo di inattivit dell ' atleta che sar di 12 settimane per le lesioni senza ematoma e di almeno 4 settimane per i traumi con ematoma . nel nostro studio abbiamo osservato 29 atleti con contua . 
this is a fundamental criterion when establishing the length of the recovery period , which is usually 12 weeks for lesions without haematoma and at least 4 weeks for those with haematoma . in our study , there were 29 patients with severe contusion , and us was able not only to locate the haematoma but also to evaluate its extent in total agreement with mri . 
in contrast , in the study of deeper muscles , kolouris and connell [ 31 ] identified a discrepancy between us and mri in the evaluation of hamstring injuries and observed that mri is more accurate in assessing the extent of injury . these studies confirm that us is limited in the study of muscle injury in that its resolution is limited to the tertiary bundle , it is unable to identify pathological alterations to the secondary and primary bundles and myofibrils and cannot evaluate deep muscle planes [ 17 , 23 ]  . conclusions us is the first - line technique in the study of muscle traumas , as it is readily available , has a good cost - benefit profile , enables assessment of muscle dynamics and provides reliable assessment of the extent of damage . 
disadvantages of us are that its resolution is limited to the tertiary bundle , it is unable to identify alterations to secondary and primary bundles and myofibrils and cannot visualise deep muscle planes . 
 mri has many advantages , including multiplanar capabilities , panoramic views , ability to evaluate deep muscle planes and to detect lesions missed by us . sione grave , l ' ecografia stata in grado non solo di localizzare l ' ematoma , ma anche di valutarne l ' estensione in perfetto accordo con la risonanza magnetica . 
l ' ecografia mostra una sensibilit per i traumi maggiori molto pi elevata rispetto a quella per i traumi minori , ci deriva dal fatto che la capacit dell ' ecografia nella valutazione di questi ultimi limitata ai casi in cui l ' edema muscolare importante . 
in queste situazioni , si pu valutare con maggiore accuratezza l ' estensione della lesione , la percentuale di muscolo coinvolto , la grandezza della cicatrice e le eventuali complicanze [ 7 , 12 , 29 ]  . 
 [ 30 ] hanno esaminato 17 pazienti con lesione acuta del retto femorale , valutandola sia con la risonanza magnetica che con ecografia : in tutti i casi le due tecniche si sono rivelate concordi nel localizzare la lesione e nel valutarne l ' entit . 
nella valutazione di muscoli pi profondi , invece , kolouris e connell [ 31 ] hanno evidenziato una certa discrepanza fra la valutazione delle lesioni dei muscoli hamstring con l ' ecografia e con la risonanza magnetica , osservando che quest ' ultima fornisce una stima pi corretta dell ' entit del danno . 
questi studi confermano che l ' ecografia ha dei limiti nello studio della patologia muscolare : il potere di risoluzione limitato al fascio terziario , l ' incapacit di identificare le alterazioni patologiche del fascio secondario , del fascio primario e delle miofibrille , la difficolt nel valutare i piani muscolari profondi [ 17 , 23 ]  . conclusioni l ' ecografia rappresenta la tecnica di prima istanza nello studio dei traumi muscolari per la facile accessibilit , per il favorevole rapporto costo - beneficio , per la possibilit di valutare la dinamica del muscolo e per l ' affidabilit nella stima dell ' entit del danno . 
questa tecnica presenta alcuni svantaggi : il potere di risoluzione limitato al fascio terziario , l ' incapacit di identificare le alterazioni del fascio secondario , primario e delle miofibrille , la difficolt nel valutare i piani muscolari profondi . 
mri provided additional information , identifying the possible absence of cochlear nerve and excluding other central nervous system ( cns ) diseases . key words cochlear implants auditory brainstem implants cochlear nerve magnetic resonance imaging computed tomography riassunto obiettivo . 
inoltre la rm ha permesso di ottenere informazioni aggiuntive valutando leventuale assenza della componente cocleare dellviii nervo cranico ed escludendo altre patologie del snc . parole chiave impianti cocleari impianti acustici al tronco nervo cocleare risonanza magnetica tomografia computerizzata introduction introduzione r . 
sensorineural hearing loss has constituted both a diagnostic and surgical challenge , only in part overcome by computed tomography ( ct ) , which has allowed identification of congenital cochleovestibular abnormalities and indirectly of cochlear nerve agenesis , but it is unable to detect abnormalities affecting the central nervous system ( cns ) [ 1 ]  . 
following the development of abis for direct stimulation of cochlear nuclei in patients with sensorineural hearing loss , magnetic resonance imaging ( mri ) became crucial to confirm inner ear alterations demonstrated by ct and verify the integrity of the auditory pathways up to the temporal cortex [ 2 ]  . 
when the cochlear nerve is aplastic or hypoplastic , there is no possibility of restoring hearing by direct stimulation of the organ of corti or of the auditory nerve fibres using traditional cochlear implants . 
 materials and methods we examined ct and mri studies of 17 patients ( 12 females and five males ) aged between 2 and 34 years ( mean age 14 years ) with congenital inner ear disease and abnormalities of the cochleovestibular systethe presence of disorders constituting exclusion criteria for surgery , in particular , dysmetabolic disease and cortical malformations , had already been ruled out ( even by means of preliminary mri ) in all these candidates for abi . 
all patients had undergone preliminary audiometric testing ( tympanometry and impedance audiometry ) that excluded middle ear disorders ; they were then subjected to electrocochleography to assess function of the cells of the organ of corti and promontory electrostimulation to check the presence of stimulable neuronal fibres . 
all patients selected for abi were then studied by ct ( siemens , somatom plus 4 , germany ) and mri ( siemens , symphony maestro , germany )  . 
ct was performed to obtain a detailed study of the petrous bone using a bone algorithm in the axial and coronal planes ( sequential technique , slice thickness 1 mm , 140 kv , 77 ma )  . 
mri was performed with proton - density ( pd ) and t2 - weighted axial turbo spin echo ( tse ) scans ( tr 2800 te 24 / 121 , thickness 5 mm ) ; coronal t2 - weighted , ( tr 4850 , te 108 , thickness 4 mm ) and sagittal t1weighted scans ( tr 440 , te 12 , thickness 4.5 mm ) to confirm the absence of other cns diseases that could contraindicate the use of abi . 
inner ear structures were examined in the lanacusia congenita o la grave ipoacusia legata ad alterazioni dellorecchio rappresentano unimportante causa di disabilit che , fino a non molti anni fa , aveva come unico trattamento la logoterapia , che consentiva ai pazienti solo una limitata capacit di inserimento sociale . 
lipoacusia neurosensoriale ha infatti rappresentato un problema diagnostico oltre che chirurgico , solo in parte risolto dallavvento della tomografia computerizzata ( tc ) ; questa metodica ha consentito di evidenziare le alterazioni congenite vestibolo - cocleari , ed in maniera indiretta lagenesia del nervo cocleare , ma non le alterazioni a livello del sistema nervoso centrale ( snc ) [ 1 ]  . 
per le protesi elettriche impiantabili a livello cocleare , la metodica tc ha rappresentato lindagine essenziale per escludere la presenza di malformazioni a livello delle strutture cocleari ed in particolare per verificarne la regolare perviet . 
in seguito allapprontamento di protesi impiantabili a livello del tronco encefalico , per stimolare direttamente i nuclei cocleari nei pazienti affetti da ipoacusia neurosensoriale , la risonanza magnetica ( rm ) divenuta metodica radiologica fondamentale sia per confermare eventuali alterazioni gi documentate da indagine tc , a livello delle strutture dellorecchio interno , che per verificare lintegrit delle vie acustiche fino alla corteccia temporale [ 2 ]  . 
quando il nervo cocleare aplasico o ipoplasico , infatti , non vi alcuna possibilit di ripristinare la percezione uditiva con la stimolazione diretta dellorgano del corti delle fibre del nervo acustico mediante i tradizionali impianti cocleari . 
in questo lavoro sono state esaminate le indagini tc ed rm di pazienti affetti da sordit congenita sottoposti ad impianto di protesi al tronco encefalico ( auditory brainstem implants : abi ) , al fine di verificarne laffidabilit nellindividuare le cause del deficit acustico . materiali e metodi nel nostro studio sono state esaminate le indagini tc ed rm di 17 pazienti ( 12 femmine e 5 maschi ) di et compresa tra i 2 ed i 34 anni ( et media 14 anni ) , affetti da patologia congenita dellorecchio interno , aventi anomalie riscontrate a carico del sistema cocleo - vestibolare . 
per tutti questi pazienti candidati ad abi per anacusia erano gi state escluse ( anche tramite indagine rm preliminare ) patologie che rappresentavano criterio di esclusione per il trattamento chirurgico , in particolare la patologia dismetabolica e la malformativa corticale . 
tutti i pazienti hanno eseguito test audiometrici preliminari ( timpanometria e limpedenzometria ) che hanno escluso patologie a carico dellorecchio medio ; sono stati quindi sottoposti ad elettrococleografia per valutare la funzionalit delle cellule dellorgano del corti e ad elettrostimolazione del promontorio per verificare la eventuale presenza di fibre neuronali stimolabili . 
in agreement with the literature , among the inner ear malformations eligible for abi , we considered the following cochlear deformities : michel deformity , cochlear aplasia , common cavity , cochlear hypoplasia , type i incomplete partition ( ip - i ) and type ii incomplete partition ( ip - ii , mondini deformity ) [ 3 , 4 ]  . 
lindagine tc stata espletata per lo studio di particolare delle rocche con algoritmo per osso secondo i piani assiale e coronale ( tecnica sequenziale , spessore di strato 1 mm , kv 140 , ma 77 )  . 
lindagine rm stata eseguita mediante scansioni assiali tse , dp e t2 pesate ( tr 2800 te 24 / 121 , spessore 5 mm ) ; coronale t2 pesata , ( tr 4850 , te 108 , spessore 4 mm ) e sagittale t1 pesata ( tr 440 , te 12 , spessore 4 , 5 mm ) allo scopo di confermare lassenza di altre patologie del snc che potrebbero rappresentare controindicazione allutilizzo degli abi . 
le strutture dellorecchio interno sono state esaminate secondo il piano assiale , con sequenza 3dft - ciss ( constructive interference in steady state ) : 28 slices , tr 17 , 3 , te 6 , 9 , spessore 0 , 65 , flip angle 70 , matrice 358512 * ( interp ) , nex 2 , fov 100100 ; queste ultime sequenze sono state esaminate anche mediante algoritmo di ricostruzione volumetrico mip ( maximum intensity projection ) , per ottenere la migliore visualizzazione globale delle strutture labirintiche . 
the straight line corresponds to the parasagittal mr scan ( c ) to identify the components of the cochleo - vestibulo - facial nerve bundle . three dimensional reconstruction of ( 3d ) fig . 
the internal implant converts the code into electrical signals such as those produced by the organ of corti , which are sent to the abi electrodes adjacent to the cochlear nuclei in order to stimulate the nerve fibres ; at this point the brain recognises the signals as sounds , producing an auditory sensation [ 11 , 1518 ]  . 
axial magnetic resonance ( mr ) scan ( a ) : the straight line corresponds to the left parasagittal mr scan ( b ) that demonstrates the absence of the cochlear nerve ( arrow )  . 
in accordo con i dati presenti in letteratura , nellinsieme delle malformazioni dellorecchio interno passibili di intervento per impianto acustico al tronco , abbiamo considerato le seguenti malformazioni cocleari : deformit di michel , aplasia cocleare , cavit comune , ipoplasia cocleare , incompleta partizione di tipo i ( ip - i ) ed incompleta partizione di tipo ii ( ip - ii , deformit di mondini ) [ 3 , 4 ]  . 
i pazienti sono stati quindi sottoposti ad intervento chirurgico di impianto al tronco ( auditory brainsteam implant : abi ; cochlear ltd , australia ) [ 57 ] , nel periodo compreso tra il febbraio 2000 ed il marzo 2005 [ 5 , 710 ]  . 
tale impianto fornito di una componente esterna , costituita da un microfono posizionato in sede retroauricolare , in grado di ricevere le onde sonore dellambiente e di inviarle , dopo averle trasformate in segnale digitale , ad un elaboratore del linguaggio con un trasmettitore collocato nel tessuto sottocutaneo in sede temporale superficiale ; il trasmettitore invia il codice attraverso la pelle allimpianto interno collocato in una nicchia ossea immediatamente al di sotto del r . 
limpianto interno converte il codice in segnali elettrici , simili a quelli prodotti dallorgano del corti , che sono inviati agli elettrodi posizionati a livello dei nuclei cocleari al fine di stimolare le fibre nervose ; a questo punto i segnali vengono riconosciuti come suoni dal cervello producendo una sensazione uditiva [ 11 , 1518 ]  . 
3a - d mr findings ( a ) : unique cavity , in parasagittal left reconstruction in which is impossible to distinguish the cochlear and vestibular components ( b ) and right reconstruction with regular findings of vii ( arrow ) and viii nerve ( black arrow ) ( c )  . 
3a - d paziente studiato mediante rm ( a ) : cavit unica , nelle ricostruzioni parasagittali sinistra senza differenziazione delle componenti cocleare e vestibolare ( b ) , e destra con riconoscimento del vii ( freccia ) e viii n.c. 
abi is contraindicated in cases of enlarged lateral recess of the fourth ventricle , a possible cause of electrode instability ; in the case of cochlear nuclei ischaemia ; and radiation exposure ( gamma - knife or stereotactic irradiation ) , which may have damaged the floor of the risultati tutti i 17 pazienti inviati dalla clinica otorinolaringoiatrica con sospetto clinico di malformazione a carico dellorecchio interno hanno trovato conferma delle loro anomalie congenite mediante tc e / o rm . 
in particolare la rm ha permesso di ottenere informazioni aggiuntive per la corretta valutazione dei nervi cocleari in 10 pazienti su 17 . discussione il sistema abi fornisce a pazienti con grave compromissione della funzionalit uditiva lopportunit di ricevere informazioni uditive mediante una stimolazione diretta dei nuclei cocleari [ 57 , 9 ] ; da ci ne consegue la necessit di reperire per mezzo della rm eventuali controindicazioni allintervento . 
limpianto abi risulta infatti controindicato nel caso in cui ci si trovi di fronte ad un recesso laterale del quarto ventricolo allargato , possibile causa di instabilit degli elettrodi , in caso di sequele ischemiche dei nuclei cocleari , ed in caso di esposizione a radiazioni ( gamma - knife o irradiazione stereotassica ) che potrebbero aver lesionato il pafourth ventricle . 
cochlear aplasia , a relatively rare malformation ( bilateral in 50% of cases ) , may be recognised as a bony vesicle on the ventral surface of the internal auditory canal ( iac ) a malformation due to arrested development before the fourth week of gestation which has been equally well documented on ct and mri [ 1 , 3 , 4 ]  . 
similarly , patients with common cochleovestibular cavity a malformation due to developmental arrest at the fourth week had normal recognition of the components of the vii and viii cranial nerves but without separation of the cochlear and vestibular components , the latter well documented on mri only . 
the common cavity , generally containing fluid , is instead readily depicted by ct and mri . in ip - i or cystic cochleovestibular deformity arising from developmental arrest at the fifth week the cochlea lacked the entire modiolus and cribriform area , resulting in a cystic formation that was well visualised with both techniques ; in this case the cochleovestibular dimensions are normal , but the internal architecture is completely deranged . 
nella sezione parasagittale si evidenzia lassenza della componente cocleare dellviii nervo cranico ( b )  . lated and cystic and might , according to some authors , represent a subsequent and therefore more differentiated form of the common cavity deformity [ 19 ]  . 
in the only patient examined by us , the iacs were within normal limits . ip - ii or mondini deformity is due to a developmental arrest arising later than in ip - i , generally at the seventh week , since the dimensions of the cochlea and vestibule are normal and the internal architecture is less deranged . 
the cochlea presents only one and a half turns , and the defect in the interscalar septum is located between the middle turn and the apical turn , which are fused and appear as an apical cystic formation . 
the basal portion of the modiolus and the basal turn are present with a normal iac in 60% of cases [ 1 , 68 ] ; this implies that the spiral ganglion is more likely to be present and more abundant than in ip - i . 
in all cases of ip - ii ( mondini deformity ) , the vestibular aqueduct appears dilated and symmetric given that embryonic development of this passage occurs at a later stage than the previous deformity . ip - ii was well demonstrated on both ct and mri although mri was also able to recognise agenesis of the right cochlear nerve in one patient . 
laplasia cocleare , malformazione piuttosto rara ( bilaterale nel 50% dei casi ) , pu essere riconosciuta come una vescicola di osso compatto sulla superficie ventrale del condotto uditivo interno ( cui ) malformazione che pu essere ricondotta ad un arresto dello sviluppo embrionario prima della quarta settimana di vita intrauterina stata altrettanto bene documentata sia mediante indagine tc che rm [ 1 , 3 , 4 ]  . 
analogamente , i pazienti che presentavano una cavit comune cocleo - vestibolare che rappresenta entrambe le strutture malformazione riconducibile ad un arresto della differenziazione embrionale generalmente nella quarta settimana di gestazione presentavano regolare riconoscimento delle componenti del vii e viii nervo cranico di cui per non risultavano separate le componenti cocleare e vestibolare , queste ultime ben valutabili solo con rm ; la cavit comune , generalmente a contenuto liquido , invece facilmente riconoscibile sia alla tc che alla rm . 
 nella ip - i o malformazione cocleo - vestibolare cistica che si verifica per arresto della differenziazione alla quinta settimana la coclea era sprovvista dellintero modiolo e dellarea cribriforme , esitando quindi in una formazione cistica , ben visualizzata da entrambe le metodiche ; in questo caso le dimensioni cocleovestibolari sono regolari , ma larchitettura interna completamente sovvertita . nellunico paziente che presentava ip - i , la rm ha documentato la presenza di un nervo vestibolare senza la componente cocleare . 
analogamente in entrambe le metodiche il vestibolo risultava dilatato , anchesso di forma cistica , e potrebbe , secondo alcuni autori , rappresentare una fase successiva e quindi pi differenziata della cavit comune [ 19 ] ; nellunico paziente da noi esaminato i cui risultavano nei limiti . 
 lip - ii o deformit di mondini rappresenta un arresto dello sviluppo pi tardivo rispetto alla ip - i , generalmente alla settima settimana , in quanto le dimensioni della coclea e del vestibolo sono normali e larchitettura interna pi organizzata . 
la coclea presenta solo un giro e mezzo , il difetto del setto interscalare tra il giro medio ed il giro apicale che risultano fusi tra loro e si presentano come una formazione cistica apicale . 
la porzione basale del modiolo ed il giro basale sono presenti con cui regolare nel 60% dei casi [ 1 , 68 ] ; da ci deriva la maggior probabilit che il ganglio spirale sia presente ed in maggior quantit rispetto alla ip - i . 
in tutti i casi di ip - ii ( deformit di mondini ) lacquedotto vestibolare si presenta dilatato e simmetrico , poich lo sviluppo embriologico di tale condotto avviene in tempi successivi alla malformazione precedente . 
in the two patients with cochlear hypoplasia in our study , well depicted on both ct and mri , mri documented the absence of the cochlear component of the eighth cranial nerve . in our experience ct was able to provide immediate visualisation of malformations of the bony labyrinth ; mri , performed with 3d acquisitions with a slice thickness less than 1 mm was able to provide similar information on bony structures , as described in the literature [ 20 , 21 ]  . 
mri is therefore fundamental for assessing the cochlear nerve ( with function demonstrated by clinical and laboratory tests ) in patients with malformed cochlea complete in its basal and middle turn only as the patients can undergo surgical treatment with a less invasive but equally effective procedure , such as the cochlear implant . 
 conclusions our study confirms mri as the primary imaging method in patients with hearing loss , as it is more complete than ct in recognising inner ear malformations eligible for treatment with auditory brainstem implant and in assessing deaf patients for central causes such as neoplastic diseases ( typically neurofibromatosis ) or metabolic - demyelinating diseases . ct is nonetheless useful and should be used to assess abnormalities of the middle and external ear , which can be effectively visualised by this modality only . vano ipoplasia cocleare , ben evidente in tc e rm , si documentata mediante rm lassenza della componente cocleare dellviii nervo cranico . nella nostra esperienza la tc si dimostrata la metodica in grado di fornire immediata visualizzazione delle malformazioni del labirinto osseo ; la rm se eseguita con studio 3d acquisita con spessore della sezione inferiore ad 1 mm , stata in grado di fornire analoghe informazioni riguardo le strutture ossee , cos come in letteratura [ 20 , 21 ]  . 
la rm risulta quindi di fondamentale importanza per i pazienti con coclea malformata completa solo del giro basale ed intermedio per il riconoscimento del nervo cocleare ( con funzionalit documentata dai test clinico - laboratoristici ) , perch possono essere trattati chirurgicamente con un intervento meno invasivo , ma altrettanto efficace , come limpianto cocleare . conclusioni lo studio della nostra casistica ha permesso di confermare la rm come metodica principale di imaging nei pazienti affetti da anacusia , in quanto pi completa della tc nel riconoscere le malformazioni dellorecchio interno che indirizzino al trattamento con impianto protesico al tronco , e nel valutare pazienti anacusici per cause di tipo centrale , come patologie neoplastiche ( tipicamente la neurofibromatosi ) o metabolico - dismielizzanti . 
post - traumatic adrenal contusion / haematoma may arise not only because of a direct trauma but also as a consequence of a sudden increase in the pressure in the inferior vena cava system - adrenal veins . 
this is why adrenal haemorrhage is not directly proportional to the trauma : compression of the inferior vena cava leads to increased pressure in the adrenal venous circulation , which supports the parenchymal lesion . 
the right adrenal gland is more frequently injured than the left gland : it can be easily compressed between the liver , spine and kidney , and its venous drainage flows directly into the inferior vena cava . key words adrenal injuries blunt abdominal trauma pediatrics riassunto le lesioni pediatriche della ghiandola surrenale , in seguito a traumi chiusi toraco - addominali , sono rare e frequentemente associate a lesioni epato - renali . 
di fatto , questa patologia pu non essere direttamente proporzionale allentit del trauma stesso : la vena cava inferiore , se compressa , pu causare un incremento della pressione venosa retrograda intrasurrenalica con conseguente danno ghiandolare . parole chiave lesioni surrenali traumi chiusi toracoaddominali pediatria introduction introduzione thoracoabdominal trauma in children rarely causes isolated adrenal injuries : the adrenal glands are anatomically protected and their involvement is usually linked to multiorgan trauma [ 15 ]  . 
the aim of this paper is to present imaging findings and possible direct and indirect adrenal [ 6 ] involvement in children with blunt abdominal trauma [ 2 , 3 ]  . nei bambini i traumi toraco - addominali chiusi causano raramente lesioni surrenaliche isolate : il surrene un organo anatomicamente protetto e , nella maggior parte dei casi , il suo coinvolgimento legato ad un traumatismo toraco - addominale multiorgano [ 15 ]  . 
scopo del lavoro di sottolineare come nel politrauma la lesione surrenalica associata debba sempre essere presa in considerazione [ 2 , 3 ] anche perch il danno surrenalico pu avere una genesi indiretta legata allimprovviso aumento della pressione intra - addominale [ 6 ]  . three patients , ages ranging from 3 to 11 years , came to our hospital after sustaining a blunt abdominal trauma in a car crash in two cases and a household accident in one case . all patients had regular haemodynamic status . 
on admismateriali e metodi sono stati esaminati tre pazienti , 2 politraumatizzati della materials and methods sion , the first patient had multiple skin lesions and pain in the right hypochondriu neurological examination was negative . 
the third patient presented sternal and epigastric trauma with anterior thoracic pain . all ultrasound ( us ) examinations were performed with a us scanner ( atl 5000 , philips , eindhoven , netherlands ) equipped with multifrequency probes ( 57.5 mhz ) and doppler parameters set to the highest sensitivity . 
computed tomography ( ct ) examination with contrast medium injection was performed in one case only with a single - slice scanner ( aquilon , toshiba , tokyo , japan ) and using specific paediatric settings . 
the contrast medium ( iomeron 300 ) was administered as a 2 ml / kg bolus infused at a rate of 2 ml / s . two patients underwent magnetic resonance imaging ( mri ) using a 1.5 - t magnet ( edge , philips , eindhoven , netherlands ) , with 16mt gradient and a phased - array coil . 
us follow - up showed a cystic evolution ( typical of a focal haemorrhagic lesion ) of a nodule that disappeared in 5 months . the third patient underwent us and mri examri was performed because of vanilmandelic acid in the urine . 
la seconda paziente , politraumatizzata della strada , con trauma cranico e contusione toraco - addominale destra , presentava esami clinico - laboratoristici di base nei limiti della norma ; lo stick urinario era negativo per ematuria . 
il terzo paziente presentava contusione sternale ed epigastrica . gli esami ecografici sono stati eseguiti con apparecchiatura ( atl 5000 , philips , eindhoven , olanda ) dotata di trasduttori multi - frequenza da 5 a 7 , 5 mhz , e utilizzando parametri doppler impostati al massimo della sensibilit . 
lesame stato effettuato senza e con mezzo di contrasto ( iomeron 300 ) somministrato alla dose di 2 ml / kg con una velocit di iniezione di 2 ml / s . 
gli esami di rm sono stati effettuati con apparecchiatura da 1 , 5 t ( edge , philips , eindhoven , olanda ) , gradienti da 16 mt e bobina phased - array . 
i quadri us e di rm erano orientativi per emorragia surrenalica . discussione le lesioni della ghiandola surrenale , nei traumi chiusi toraco - addominali , sono rare e frequentemente associate a lesioni epato - renali . 
gli esiti , che si consolidano entro un termine massimo di 6 mesi dallevento traumatico , variano dalla restitutio ad integrum , come nei nostri tre casi , fino allesito calcifico [ 6 ]  . in letteratura non sono descritte lesioni traumatiche bilaterali e di fatto non sono riportate sequele di insufficienza funzionale . nel i caso la diagnosi non presentava difficolt per laumento volumetrico omogeneo della ghiandola . 
il nodulo permane ipointenso e senza ce ; il segnale intracistico verosimilmente ascrivibile ad un contenuto spurio . unilateral , no endocrine consequences have been reported in the literature . in the first case described here , the diagnosis of contusion was straightforward due to the homogeneous increase in gland volume . 
this is why adrenal haemorrhage is not directly proportional to the trauma : compression of the inferior vena cava leads to an increase in the pressure of the adrenal venous circulation , which supports the parenchymal lesion [ 6 ]  . 
the right adrenal gland is more frequently injured than the left gland , as it can be easily pressed between the liver , spine and kidney , and its venous drainage flows directly into the inferior vena cava . differential diagnosis between adrenal hemorrhage and other paediatric adrenal masses , especially neuroblastoma , is based upon both temporal criteria ( volume and structural changes of the lesion over time ) and doppler findings : intraparenchymal flow is not present in the adrenal haemorrhage whereas it is usually appreciable in neuroblastoma . 
iodine - 131 - metaiodobenzylguanidine ( mibg ) scintigraphy is required in cases of doubt . tica non legata alla sola contusione diretta , ma verosimilmente anche ad un improvviso aumento pressorio del sistema vena cava inferiore - vene surrenaliche . 
di fatto , questa patologia pu non essere direttamente proporzionale allentit del trauma stesso : la vena cava inferiore , se compressa , pu causare un incremento della pressione venosa retrograda intrasurrenalica con conseguente danno ghiandolare [ 6 ]  . 
inoltre la lesione traumatica del surrene quasi esclusivamente a destra : sia perch pi facilmente compresso tra fegato , rachide e rene , sia perch il drenaggio venoso del surrene destro stesso sbocca direttamente nella vena cava inferiore . la diagnostica differenziale con il neuroblastoma e si basa sia sul criterio temporale ( evoluzione lacunare e dimensionale riduttiva ) sia sui rilievi doppler : nella emorragia surrenalica non presente flusso al cd , mentre nel neuroblastoma la velocit di flusso ben evidente . 
garlaschi springer verlag italia ( 2006 ) isbn 88 - 470 - 0518 - 3 published online : 11 october 2006 il volume ecografia dellapparato osteoarticolare focalizzato sullimpatto dellecografia in campo muscoloscheletrico con particolare riferimento alla patologia in ambito reumatologico . come noto , infatti , significativi sono limpatto sociale delle malattie reumatiche , in costante aumento e causa spesso di alterazioni altamente invalidanti , e limportanza clinica di una diagnosi precoce . 
il ricorso a tecniche ecografiche sempre pi sofisticate ed avanzate ha reso possibile la definizione di importanti aspetti iniziali di malattia , quali il coinvolgimento sinoviale , conformazione del panno e il danno cartilagineo articolare . 
luso poi , sempre pi frequente , di metodiche contrastografiche ha consentito , inoltre , lacquisizione di parametri di significativa importanza , sia in campo clinico che terapeutico , di valutazione oggettiva ( grado di iperemia e qualit dei flussi ) delle fasi di attivit e di quiescenza delle patologie infiammatorie croniche articolari . lopera si articola in tre sezioni ben distinte : nella prima ( capitoli 1 - 3 ) vengono considerati i principali aspetti tecnologici e le molteplici procedure di esame con i relativi rilievi anatomici sia in condizioni basali che con le tecniche doppler . 
la seconda sezione ( capitoli 4 - 5 ) rappresenta senza dubbio , per la rigorosa e puntuale analisi della semeiotica ecografica dellapparato locomotore e per i molteplici quadri patologici presentati , resi ancora pi preziosi da uneccellente iconografia quanto mai dimostrativa e scelta con rigorosa cura , il punto pi innovativo e didattico di tutta la monografia , a cui contribuisce in maniera decisamente significativa il ruolo dellecografia nel monitoraggio della terapia in corso di malattie infiammatorie croniche articolari ( capitolo 6 )  . 
nellultima sezione , infine , ( capitolo 7 ) sono trattate , soprattutto in chiave prospettica , alcune interessanti applicazioni dellecografia in campo terapeutico che , se opportunamente affinate , potranno rappresentare in un prossimo futuro un prezioso ed insostituibile complemento per una sempre pi precisa ed essenziale programmazione terapeutica . in conclusione , si tratta di un testo chiaro , caratterizzato da una bibliografia precisa e aggiornata e da una iconografia curata nei minimi particolari , da cui traspaiono lesperienza e lelevata capacit didattica degli autori . 
lesions were found along the posteromedial wall of the proximal gastric pouch and ranged in size from 10 to 25 monly two patients were symptomatic at the time of diagnosis ; in most cases , diverticula were discovered during studies performed as part of the standard follow - up protocol . 
we do not believe these lesions to be clinically important ; at present , our patients are no longer followed up for this problem and undergo diagnostic examinations only if and when they develop symptoms . key words morbid obesity vertical - banded gastroplasty diverticula riassunto obiettivo . 
i diverticoli erano localizzati lungo la parete postero - mediale della tasca prossimale dello stomaco operato e avevano diametro variabile tra 10 e 25 msolo due pazienti erano sintomatici al momento della diagnosi ; nella maggior parte dei casi i diverticoli vennero riscontrati durante un follow - up routinario . 
riteniamo che queste lesioni siano da considerare non clinicamente importanti ; attualmente , i nostri pazienti non sono pi sottoposti a follow - up per questo problema e vengono controllati solo se e quando insorge sintomatologia . parole chiave obesit patologica gastroplastica verticale diverticoli introduction introduzione vertical - banded gastroplasty ( vbg ) is a gastric restriction procedure that is commonly used to control excessive weight in morbidly obese patients , the recently established laparoscopic feasibility of which has greatly contributed to increase diffusion , especially in europe [ 1 , 2 ]  . 
although generally regarded as a safe operation , vbg is not free from postoperative complications , and a variety of problems , such as leaks , staple - line disruptions , band erosion , reflux oesophagitis and pouch dilatations , with or without stenosis , have been described in the literature [ 3 , 4 ]  . 
diverticula arising from the la gastroplastica verticale ( vertical banded gastroplasty , vbg ) una tecnica chirurgica utilizzata nei pazienti con obesit patologica al fine di ridurre leccessivo introito di cibo che ha avuto , soprattutto in relazione alla possibilit di esecuzione mediante accesso laparoscopico , una notevole diffusione , specialmente in europa [ 1 , 2 ]  . 
non esiste consenso in letteratura sul meccanismo con cui queste alterazioni vengono a crearsi , sul loro significato clinico e sulla necessit o meno di un trattamento delle stesse [ 47 ]  . scopo di questo lavoro descrivere i reperti radiografici osservati in un gruppo di pazienti operati di vbg che hanno sviluppato diverticoli della tasca gastrica prossimale e riportare le variazioni degli stessi durante il follow - up clinicoradiologico . tecnica chirurgica nella gastroplastica verticale secondo mclean [ 2 ] , lo stomaco viene diviso in due parti , creando una piccola tasca prossimale lungo la piccola curva , in comunicazione con lo stomaco distale attraverso uno stretto stoma . 
il peso medio al momento dellintervento era di 103 kg ( range 90130 kg ) ; lindice di massa corporea ( body mass index , bmi ) era di 40 ( range 3550 ) kg / m2 . 
due pazienti erano state sottoposte alla vbg dopo complicanze insorte a seguito di un intervento di bendaggio gastrico per via laparoscopica . gli esami radiografici sono stati eseguiti come parte di un programma standard di follow - up postoperatorio : un primo controllo era effettuato in terza giornata , utilizzando mezzo di contrasto iodato idrosolubile ; studi baritati erano quindi ottenuti a 1 , 4 e 12 mesi dallintervento , o ogniqualvolta si sospettavano complicanze . 
allinizio dellindagine venivano somministrati al paziente 3060 ml di una sospensione liquida di bario 125% p / v per identificare eventuale dilatazione esofagea , reflusso gastroesofageo , e analizzare volume e forma della tasca gastrica prossimale , valutando anche il diametro del passaggio allo stomaco distale . stato possibile sottoporre a follow - up radiografico 7 / 12 pazienti per un periodo variabile tra 14 e 53 mesi ; quattro pazienti sono state esaminate due volte . 
viene creata una piccola tasca verticale lungo la piccola curva dello stomaco usando una suturatrice meccanica . proximal gastric pouch are an additional possible finding that has been reported in a few papers only [ 46 ]  . 
no consensus exists regarding the possible mechanism causing these lesions , their clinical significance and the need for treatment [ 47 ]  . the purpose of this paper is to describe the radiographic findings we observed in a series of patients with vbg who developed diverticula of the proximal gastric pouch and to describe changes observed during clinical and radiological follow - up . surgical technique in vbg , according to mclean [ 2 ] , the stomach is divided into two parts , creating a proximal pouch by two applications of an endovascular gastrointestinal anastomosis ( endo - gia ) 60 stapler from an end - to - end anastomosis window 7 cm below the angle of his along the lesser curvature against a 12mm ewald tube . 
the examination involved swallowing 3060 ml of a liquid barium suspension at 125% w / v to detect possible oesophageal dilatation and gastrooesophageal reflux and to evaluate pouch volume , size and shape , as well as the outlet diameter . radiological follow - up of the diverticula was possible in 7 / 12 cases ( range 1152 months ) ; four patients were examined twice during this period . 
images were reviewed by two radiologists who evaluated size and location of the diverticula and , although it was not possible to evaluate precisely dimensional changes due to different radiological projections and patient sizes , formulated a consensus opinion about enlargement of these lesions over time . correlation of the presence of diverticula with symptoms , postoperative weight loss and clinical history was obtained in all cases . 
le immagini radiografiche sono state quindi esaminate retrospettivamente da due radiologi che hanno valutato grandezza e posizione dei diverticoli e , bench non fosse possibile effettuare una misurazione precisa di eventuali modificazioni volumetriche dei diverticoli nel tempo , hanno cercato di esprimere , in consenso tra loro , una opinione su questo argomento . abbiamo correlato la presenza dei diverticoli con i sintomi del paziente , la perdita di peso postoperatoria , e la storia clinica . 
i diverticoli sono stati identificati in terza giornata postoperatoria in 6 pazienti ; sono stati dimostrati al controllo a 1 mese in 3 casi , e allesame effettuato a 4 mesi dallintervento nei 3 soggetti rimanenti . 
2a , b patient 2 : a anteroposterior ( ap ) radiograph obtained 1 month after vertical - banded gastroplasty ( vbg ) showing a diverticulum about 16 mm in largest diameter arising from the proximal gastric pouch . 
2a , b paziente 2 : a radiogramma ap ottenuto 1 mese dopo lintervento dimostra la presenza di un diverticolo di circa 16 mm di diametro massimo a partenza dalla tasca gastrica prossimale . 
one patient ( patient 1 ) presented with dysphagia at the first follow - up study at 34 months , when the diverticulum appeared unchanged ; symptoms had subsided at the second follow - up study , when the diverticulum was slightly enlarged . 
la maggior parte dei pazienti era del tutto asintomatica ; solo due soggetti ( le pazienti n 6 e 12 della tabella 1 ) avevano episodi ricorrenti di vomito al momento della diagnosi . 
stenosi del passaggio tra la parte prossimale dello stomaco e la parte distale dello stesso venne dimostrata in uno dei due casi ( paziente 12 ) al primo esame di follow - up , a 7 mesi di distanza . 
una paziente ( paziente 1 ) si present al primo esame di follow - up a 34 mesi accusando disfagia , e il diverticolo appariva immodificato rispetto allesame precedente ; i sintomi erano scomparsi al secondo follow - up , mentre il diverticolo appariva lievemente aumentato di volume . 
due pazienti ( caso 4 e caso 7 ) svilupparono reflusso gastroesofageo a 29 e 19 mesi dopo lintervento : in una ( paziente 4 ) il diverticolo non aveva subito modificazioni rispetto al primo esame ; nellaltra ( paziente 7 ) si osserv lieve aumento di volume . 
abbiamo osservato sviluppo di diverticoli della tasca prossimale lungo tutta la nostra esperienza di 79 interventi di vbg , e non solo allinizio della nostra casistica ( tabella 1 )  . quattro pazienti sono state sottoposte a nuovo intervento chirurgico . 
in two of them ( patients 2 and 4 ) , the diverticulum was unchanged from its first demonstration while it was slightly enlarged in the remaining one ( patient 7 )  . 
development of pouch diverticula was observed in all 79 patients who underwent vga and not only in the early cases ( see table 1 )  . four patients underwent a second surgical procedure . two were converted to biliopancreatic diversion : one because of new weight gain ( patient 5 ) ; the other for outlet stenosis ( patient 12 )  . 
two ( patients 8 and 11 ) requested restoration because of intolerance to the operation ; both underwent gastrogastrostomy ( one at our institution , the other at another hospital )  . 
the diverticula were not immediately visible , nor were they specifically searched for during surgery . creatica : una per aumento di peso ( paziente 5 ) ; laltra per la stenosi dello stoma ( paziente 12 )  . 
due ( pazienti 8 e 11 ) hanno richiesto una nuova operazione per intolleranza allintervento ; entrambe sono state sottoposte a gastrostomia ( una nel nostro reparto ; una in un altro ospedale )  . 
agli interventi , i diverticoli non erano immediatamente visibili n sono stati specificatamente ricercati . non abbiamo dimostrato correlazione tra presenza dei diverticoli , sintomi , perdita di peso postoperatoria e storia clinica delle pazienti . 
nella nostra casistica abbiamo avuto 2 / 12 pazienti con vomito ( 16 , 7% ) , 2 / 12 con reflusso gastroesofageo ( 16 , 7% ) , e 1 / 12 con stenosi dello stoma ( 8 , 3% )  . 
lanalisi statistica non ha dimostrato table 1 summary of clinical and radiographic findings following vertical - banded gastroplasty ( vbg ) diagnosis symptoms approximate first diameter , follow - up , months diameter , second follow - up , months symptoms approximate symptoms approximate diameter , no . 
no. in the series 1 month 1 month 4 months no 4 months no 3 days vomiting 3 days 4 months no 1 month 3 days 3 days 3 days vomiting 3 days go , gastrooesophageal reflux ; = , no changes tabella 1 riassunto dei reperti clinici e radiologici diagnosi nella serie operatoria 1 mese 1 mese 4 mesi 4 mesi 3 giorni 3 giorni 4 mesi 1 mese 3 giorni 3 giorni 3 giorni 3 giorni vomito vomito g - e , gastroesofageo ; = , referti invariati dysphagia go reflux go reflux > ( 28 ) go reflux vomiting > ( 16 ) > ( 15 ) disfagia riflusso g - e = vomito riflusso g - e > 28 riflusso g - e = no . 
no. sintomi diametro sintomi approssimativo , primo follow - up , mesi diametro approssimativo , secondo follow - up , mesi sintomi diametro approssimativo , there was no statistical correlation between the presence of diverticula and symptoms , postoperative weight loss and clinical history . 
they are considered to be a consequence of excessive pressure within the proximal gastric pouch that develops after surgery or , according to mason , due to a too narrow stoma between the proximal pouch and the distal stomach [ 7 ]  . 
although suturing was always performed against a 12 - mm ewald tube to ensure correct placement , this was probably not the case in all patients , thus leading to the development of diverticula at the crossing of the staple lines . 
moreover , at least in two patients , the fact that the vbg was done after a previous gastric banding could explain difficulties in obtaining correct alignment of the staple lines . 
however , it must be said that we encountered this kind of complication throughout our experience with this kind of operation , not only at the beginning , and this stands against this hypothesis . 
another possible explanation could be the follow - up protocol we adopted : in fact , all patients in our series underwent four radiographic studies in the first postoperative year even if they were symptom free . this closer follow - up strategy than that followed in most published series could possibly lead to demonstration of nonsymptomatic changes , as diverticula were demonstrated in most of our patients . the second point to discuss is the clinical significance of these lesions . 
vengono considerati conseguenza dellaumento della pressione allinterno della tasca gastrica prossimale che si sviluppa dopo lintervento o , secondo linterpretazione di mason , il risultato di uno stoma troppo ristretto tra la tasca prossimale e lo stomaco distale [ 7 ]  . 
bench le stesse siano state sempre effettuate lungo un tubo di ewald da 12 mm per garantire un corretto posizionamento , questo non stato , verosimilmente , possibile in tutti i casi , consentendo quindi il formarsi dei diverticoli allincrocio delle linee di sutura . 
inoltre , almeno in due pazienti , il fatto che lintervento di vbg sia stato effettuato dopo un precedente intervento di bendaggio gastrico pu spiegare ulteriori difficolt al corretto posizionamento delle linee di sutura . 
possibile inoltre ipotizzare che i diverticoli siano il risultato della doppia curva di apprendimento affrontata dai chirurghi ( quella durante lapprendimento della tecnica laparotomica di intervento e , in un secondo momento , quella per lapprendimento della tecnica laparoscopica )  . 
tuttavia , il fatto che i diverticoli si siano presentati in pazienti operati durante tutto larco della nostra esperienza , e non solo allinizio , sembra contrastare con questa possibilit . 
unaltra possibile spiegazione sta nel tipo di protocollo di follow - up radiologico utilizzato nei nostri casi : infatti , tutti i pazienti sono stati sottoposti a quattro indagini radiologiche nel primo anno dopo lintervento , anche se asintomatici . 
questa una strategia di controllo molto pi serrata di quella seguita nella maggioranza degli altri centri che pu aver portato alla dimostrazione di reperti non sintomatici , come si sono dimostrati essere i diverticoli nella maggior parte dei nostri casi . il secondo punto da discutere il significato clinico di queste lesioni . 
three other patients developed symptoms during follow - up ( one dysphagia and two gastrooesophageal reflux ) , but diverticula were unchanged in two of them and only slightly increased in the remaining one . 
more in detail , patient 1 , who had dysphagia , had an unchanged diverticulum at the first follow - up examination whereas the lesion was slightly enlarged at follow - up after about 1 year , when her symptom had disappeared . 
in addition , no differences were observed between frequency and type of long - term complications in vbg patients with diverticula and those without them . to conclude , our results show that , in our series , diverticula of the proximal pouch in patients who undergo vbg are a relatively common finding . 
the cause of diverticula were , most probably , problems in obtaining good alignment of the suture lines along the lesser curvature of the stomach at surgery while demonstration of diverticula was related to the strict follow - up protocol adopted . 
from a clinical point of view , we do not believe these lesions to be important ; at present , our patients are no longer followed up for this problem and undergo diagnostic examinations only if and when they develop symptoms . tra la sintomatologia osservata nei soggetti con diverticoli rispetto a quella dei pazienti senza questo tipo di lesioni . inoltre , non abbiamo osservato alcuna correlazione tra storia clinica e variazioni volumetriche dei diverticoli nel tempo . 
in uno dei due pazienti sintomatici il vomito scomparve dopo pochi mesi , mentre laltro ebbe persistenza dei sintomi a fronte di mancato incremento volumetrico della lesione . tre ulteriori soggetti hanno sviluppato sintomi durante il follow - up ( uno disfagia e due reflusso gastroesofageo ) , ma i diverticoli rimasero immodificati in due e solo lievemente aumentato nel rimanente . 
specificatamente , la paziente 1 , che aveva disfagia aveva il diverticolo immodificato al primo controllo , mentre lo stesso era lievemente ingrandito allindagine successiva , a circa un anno , ma con scomparsa della sintomatologia . per concludere , i nostri risultati mostrano che , nella nostra casistica , i diverticoli della tasca prossimale nei pazienti operati per vbg sono un reperto relativamente comune . lo sviluppo di queste lesioni stato in relazione , verosimilmente , a difficolt ad ottenere un corretto allineamento delle linee di sutura lungo la piccola curva durante lintervento chirurgico , e la loro dimostrazione stata il risultato dello stretto programma di follow - up da noi utilizzato . 
lagalla sezione di diagnostica per immagini , dipartimento di biotecnologie mediche e medicina legale , policlinico universitario , via del vespro 127 , i - 90127 palermo , italy , correspondence to : t.v. 
 + 39 - 091 - 6552335 / 6552336 , fax + 39 - 091 - 6552337 , e - mail : tv.bartolotta@unipa.it received : 14 february 2006 / accepted 11 april 2006 / published online : 11 october 2006 abstract purpose . 
however , the growing use of us in the study of the neck and thyroid has markedly increased the detection rate of nonpalpable thyroid nodules , with values reaching almost 70% of the study sample in some series [ 25 ]  . 
most thyroid incidentalomas are of no clinical significance since thyroid cancer is rare , accounting for 1.5% of all malignancies and 0.23% of all cancer deaths in the usa in 2001 [ 6 ]  . moreover , surgical and autoptic studies have demonstrated that occult thyroid cancers are more frequent than clinically manifest forms reaching 36% of the population studied in some countries which confirms the limited biological significance of this cancer [ 7 , 8 ]  . a new sonographic technique real - time spatial compound sonography ( cs ) has recently been introduced that uses electronic beam steering of a transducer array to acquire several ( three to nine ) partially overlapping scans of an object from different view angles [ 9 ]  . 
the application of this technique to the study of the thyroid has been shown to improve image quality compared with conventional sonography , mainly thanks to the reduction in background noise , spurious echoes and other acoustic artefacts [ 10 ]  . the primary aim of this study was to assess the incidence and sonographic patterns with both greyscale and colour doppler us of thyroid nodules detected by neck sonography in an adult population with no suspicion of thyroid disease . 
the secondary aim was to evaluate the possible benefit of cs technology in terms of improved image quality . materials and methods patients and lesions between january and october 2003 , after obtaining approval from the ethics committee , we carried out hrus and cs of the thyroid on 704 consecutive patients ( 400 women and 304 men ; age range 1793 years ; mean : 60.615 years ) who had been referred to us for colour doppler us of the epiaortic trunks and had no history , symptoms or signs of thyroid disease . 
all patients were inhabitants of the province of palermo ( northern sicily ) , an area with a low iodine intake ( mean daily urinary iodine excretion less than 50 - 100 g / g of creatinine )  . 
in order of frequency , the clinical indications for colour doppler us of the carotids were : vertigo ( 211 ) , previous cerebral stroke ( 181 ) or tia ( 157 ) , generalised atherosclerosis ( 130 ) , type i or ii diabetes mellitus ( 126 ) , headache ( 58 ) and previous trauma ( 15 )  . 
informed consent was obtained from all patients before the us study . lecografia ad alta risoluzione in scala di grigi ( us ) e limpiego dei moduli color e power - doppler consentono unaccurata valutazione delle strutture anatomiche della tiroide , fornendo , al contempo , informazioni di carattere funzionale sulla ghiandola normale e su quella patologica , con particolare riguardo alla sua vascolarizzazione [ 1 ]  . tuttavia , in diretta conseguenza del sempre crescente utilizzo dellus nello studio del collo e della tiroide , si registrato un netto incremento del riscontro di noduli tiroidei non palpabili , fino a valori che , in alcune casistiche , raggiungono quasi il 70% della popolazione in studio [ 25 ]  . 
la maggioranza degli incidentalomi tiroidei , infatti , non riveste significato clinico di rilievo , in quanto il cancro della tiroide poco frequente , rappresentando l1 , 5% di tutte le neoplasie maligne e lo 0 , 23% di tutte le morti per cancro nel 2001 negli stati uniti damerica [ 6 ]  . 
inoltre , studi chirurgici e autoptici hanno messo in evidenza come il cancro occulto della tiroide sia pi frequente di quello clinicamente manifesto raggiungendo in alcuni paesi anche il 36% della popolazione presa in esame a conferma della sua limitata rilevanza biologica [ 7 , 8 ]  . recentemente , stata introdotta una nuova tecnica ecografica real time spatial compound sonography ( cs ) la quale sfrutta la possibilit di angolare elettronicamente il fascio ultrasonoro generato dalla linea di elementi trasduttori al fine di effettuare diverse ( da tre a nove ) scansioni in parte sovrapposte di un oggetto da diversi angoli di vista [ 9 ]  . 
lapplicazione di tale tecnica allo studio ecografico della tiroide ha mostrato una migliore qualit dellimmagine rispetto allecografia convenzionale , principalmente grazie alla riduzione del rumore di fondo , degli echi spuri e di altri artefatti acustici [ 10 ]  . lobiettivo primario di questo lavoro stato quello di valutare lincidenza e gli aspetti ecografici sia in scala dei grigi che color - doppler dei noduli tiroidei riscontrati in una popolazione adulta , senza sospetto clinico di malattia tiroidea , sottoposta a studio ecografico del collo . 
quale obiettivo secondario , stato valutato leventuale apporto fornito dalla tecnologia cs in termini di qualit dellimmagine . materiali e metodi pazienti e lesioni tra gennaio e ottobre 2003 , ottenuta lapprovazione da parte del comitato etico , 704 pazienti consecutivi ( 400 donne e 304 uomini ; 1793 anni ; media : 60 , 615 anni ) inviati presso il nostro istituto per essere sottoposti ad uno studio ecocolor - doppler dei tronchi epiaortici e i quali non presentavano anamnesi , sintomi o segni clinici di patologia tiroidea sono stati sottoposti ad hrus e cs della tiroide . 
tutti i pazienti erano cittadini della provincia di palermo , nella sicilia settentrionale , che costituisce unarea a bassa increzione iodica ( escrezione media giornaliera di iodio con le urine inferiore a 50100 g / g di creatinina )  . 
once adjusted , the technical parameters remained unchanged throughout the us study . for each nodule detected , the study was completed with the acquisition of two images , one with conventional us and the other with the cs technique . 
both images were saved on the units hard disk and then transferred as raw data to a personal computer ( pc ) connected to the us unit via an ethernet connection . on - site analysis at the end of each examination , the radiologists , who were unaware of the final diagnosis , determined the number , size ( measured in three diameters ) , site , echogenicity ( hyper - , isoor hypoechoic ) , echostructure ( solid , cystic , mixed ) , margins ( well - defined , irregular , ill - defined ) and the presence of hyperechoic spots ( coarse calcification or microcalcifications ) in all nodules detected [ 11 ]  . 
in detail , the following were considered malignant sonographic characteristics on greyscale us : ( a ) punctate microcalcifications defined as hyperechoic spots less than 2 mm with or without acoustic shadows , ( b ) markedly hypoechoic echostructure ( increased hypoechogenicity relative to adjacent muscle ) , ( c ) irregular or microlobulated margins and ( d ) anteroposterior diameter greater than longitudinal diameter [ 12 ]  . 
the presence and pattern of flow at colour and power doppler imaging were assessed and classified as follows : type i , no flow ; type ii , perinodular flow only ; type iii , intranodular flow only ( iiia ) or intraand perinodular flow ( iiib ) [ 13 ]  . 
clinical , sonographic and cytological results were filed separately and used for statistical evaluation using the chi - square and fisher exact tests , with statistical significance set at p < 0.05. off - site analysis digital images stored on the pc were reviewed by two expert radiologists who had not taken part in the us examinations and were blinded to the final diagnosis and examination technique . 
la regolazione relativa al guadagno colore stata effettuata innalzando lamplificazione fino ad ottenere , in ogni singolo paziente , la comparsa di segnali casuali di natura artefattuale e poi abbassando lievemente lamplificazione fino alla loro scomparsa . 
una volta regolati , i parametri tecnici sono stati mantenuti invariati per tutta la rimanente durata dellindagine ecografica . ogni studio stato completato , per ogni nodulo individuato , con lacquisizione di due immagini , la prima ottenuta con metodica ecografica convenzionale e la seconda con tecnica compound . 
entrambe le immagini sono state archiviate sul disco rigido in dotazione allunit ecografica e poi inviati , sotto forma di dati grezzi , ad un personal computer ( pc ) collegato allecografo attraverso una connessione in standard ethernet . analisi on - site al termine di ogni indagine ecografica gli esaminatori , non a conocenza della diagnosi finale , hanno valutato consensualmente numero , dimensioni ( misurate in 3 diametri ) , sede , ecogenicit ( iper - , isoo ipo - ecogena ) , ecostruttura ( solida , cistica , mista ) , margini ( ben definiti , irregolari o sfumati ) e la presenza di spots iperecogeni ( calcificazioni grossolane o microcalcificazioni ) in tutti i noduli individuati [ 11 ]  . 
the two radiologists expressed their evaluation in consensus and graded image quality on a 5 - point scale ; statistical analysis was performed using the t test for paired samples . reference standard nodules displaying at least one criterion of malignancy at us or colour doppler us underwent fna . 
aspirates were fixed in alcohol and stained with papanicolaou staall cytological samples were examined and graded according to papanicolaou into classes from 0 to 5 : class 0 indicates inadequate sample ; class 1 absence of atypical or abnormal cells ; class 2 atypical cytological findings but no evidence of malignancy ; class 3 cytological findings suggestive of , but not conclusive for , malignancy ; class 4 strongly suggestive of malignancy ; and class 5 conclusive for malignancy . results we detected 711 thyroid nodules in 233 patients ( 33.1% ) , with an age range of 1793 years and a mean age of 59.415.3 years ( table 1 )  . 
no statistically significant difference was found between the number of nodules located in the right so ; tipo ii , flusso esclusivamente perinodulare ; tipo iii , flusso esclusivamente intranodulare ( iiia ) o intra e perinodulare ( iiib ) [ 13 ]  . 
gli accertamenti clinici , ecografici e citologici sono stati archiviati separatamente e utilizzati per valutazioni statistiche tramite i test chi - quadro ed esatto di fisher con livello di significativit statistica fissato a p inferiore a 0 , 05 . analisi off - site le immagini digitali archiviate allinterno della stazione di lavoro basata su pc sono state retrospettivamente riesaminate da due esperti radiologi , non coinvolti negli esami ecografici e tenuti alloscuro riguardo la diagnosi finale e la tecnica utilizzata per ogni esame . 
agli esaminatori stato chiesto di valutare , per ciascuna immagine , la qualit complessiva in relazione alla presenza o meno di artefatti , quali : ( a ) la granulosit dellimmagine artefatto anche noto con il termine di coherent wave interface o speckle e riconducibile ad un eccessivo rumore di fondo ; ( b ) la presenza di echi spuri o clutter ; ( c ) le ombre acustiche laterali e altri artefatti acustici ; ( d ) il grado di evidenza delle lesioni ( visibilit e chiarezza dei noduli rispetto al parenchima ghiandolare adiacente ) [ 15 ]  . 
i due radiologi hanno espresso , in consenso , la loro valutazione graduandola su una scala di cinque livelli e lanalisi statistica stata effettuata utilizzando il t test per campione doppio . standard di riferimento nei noduli con almeno un criterio di malignit positivo allecografia e / o al color - doppler stato effettuato laspirato con ago sottile ( fna )  . 
in accordo con questa classificazione , la classe 0 indica women : no nodules women : detected nodules men : no nodules men : detected nodules donne : noduli assenti donne : noduli presenti uomini : noduli assenti uomini : noduli presenti age range / fasce det fig . 
2a high - resolution ultrasonography ( hrus ) axial image in a 31 - year - old woman shows a slightly hypoechoic , ill - defined , 6 - mm nodule ( large arrow ) on the anterior aspect of the right lobe ; artefactual shadowing is clearly appreciable on the common carotid ( small arrows ) , as is speckle ( grainy appearance ) ( large arrow )  . 
2a immagine assiale in scala di grigi convenzionale in una donna di 31 anni che evidenzia , nel lobo destro in sede anteriore , un nodulo lievemente ipoecogeno a margini mal definiti del diametro di 6 mm ( freccia grande ) ; la presenza di ombre acustiche laterali chiaramente apprezzabile in corrispondenza del tronco carotideo comune ( frecce piccole ) cos come laspetto complessivamente granuloso dellimmagine . 
type ii colour doppler pattern was statistically more common in nodules less than 10 mm in diameter ( p < 0.001 ) ( table 5 )  . none of the nodules had microcalcifications , irregular or microlobulated margins , marked hypoechogenicity or longitudinal diameter greater than anteroposterior diameter . 
416 / 711 noduli sono stati rilevati in 143 donne ( 58 , 5% ) e 295 / 711 noduli in 90 uomini ( 41 , 5% ) ( p < 0 , 001 )  . 67 / 233 ( 28 , 7% ) pazienti presentavano un singolo nodulo mentre i rimanenti 166 / 233 ( 72 , 3% ) avevano multiple formazioni nodulari . 
non sono state , di contro , osservate differenze statisticamente significative tra il numero dei noduli localizzati nel lobo destro e quelli localizzati nel lobo sinistro : 372 / 711 ( 52 , 3% ) nel lobo destro , 336 / 711 ( 47 , 4% ) nel sinistro e i restanti 3 ( 0.4% ) noduli in sede istmica . lintervallo dimensionale dei noduli individuati stato di 0 , 184 , 1 cm ( media : 1 , 1 cm )  . 
in clinical practice , us is increasingly regarded as an extension of the physical examination of the thyroid and , as a result , the number of endocrinologist referrals for incidentally discovered thyroid nodules is likely to reach epidemic proportions , raising several concerns as to the management of these patients [ 6 ]  . 
the low malignancy and mortality rates associated with thyroid neoplasms and the fact that benign nodules tend to remain so for a long time call for a thorough assessment of the costbenefit ratio of the use of different diagnostic tools in nodular thyroid pathology [ 16 ]  . in agreement with the literature , the incidence of thyroid nodules observed in our series is high approximately one third of the population examined with a higher incidence in women and in old age . 
however , the incidence in the general population is most probably even higher , given that our study excluded patients with a positive history or clinical signs and symptoms of thyroid pathology . 
a study on us screening for thyroid nodules in 101 middle - aged women without previous thyroid disease living in southern finland detected thyroid nodules or echostructural abnormalities in 35.6% of subjects [ 17 ] , and the same authors reported the presence of sonographic thyroid abnormalities in 69 / 253 risultato statisticamente pi frequente nei noduli di diametro inferiore a 10 mm ( p < 0 , 001 ) ( tabella 5 )  . 
in nessuno dei noduli presi in esame stata riscontrata la presenza di microcalcificazioni , margini irregolari o microlobulati , ipoecogenicit marcata o diametro longitudinale maggiore di quello antero - posteriore . 
nella pratica clinica , lecografia assume sempre pi la valenza di vera e propria estensione dellesame obiettivo della tiroide e , per questo , verosimile che il numero di soggetti che si rivolgono agli endocrinologi per noduli tiroidei scoperti in maniera incidentale tenda progressivamente ad aumentare , assumendo proporzioni di vera e propria epidemia e sollevando non poche preoccupazioni in relazione alla gestione di tali pazienti [ 6 ]  . 
infatti , alla luce dei bassi tassi sia di malignit che di morte per neoplasie tiroidee nonch della constatazione che noduli tiroidei benigni tendono a rimanere tali a lungo , appare necessaria una corretta valutazione del rapporto costo / beneficio nellimpiego dei diversi presidi diagnostici nella patologia nodulare tiroidea [ 16 ]  . in accordo con quanto riportato in letteratura , lincidenza di noduli tiroidei osservata nella nostra serie elevata , pari a circa un terzo del campione in esame , con una maggiore incidenza nel sesso femminile ed in et avanzata . 
tuttavia , lincidenza nella popolazione generale da ritenersi , con tutta probabilit , ancora maggiore , dal momento che dal nostro studio sono stati esclusi i pazienti con anamnesi positiva o sintomi e segni clinici di patologia tiroidea . 
unindagine ecografica eseguita nella finlandia meridionale in 101 donne det media senza precedenti patologie tiroidee , ha dimostrato noduli tiroidei o anomalie ecostrutturali nel 35 , 6% dei soggetti [ 17 ] mentre gli stessi autori hanno rivelato la presenza di anomalie ecografiche della tiroide in 69 / 253 ( 27 , 3% ) soggetti selezionati casualmente [ 2 ]  . 
infine , una valutazione ecografica di eventuali anomalie tiroidee , condotta su 547 soggetti sovrappeso in unarea cittadina con introito giornaliero di iodio relativamente basso , ha evidenziato la presenza di alterazioni tiroidee nel 56% dei soggetti [ 18 ]  . in particolare , nella nostra casistica circa i due terzi dei noduli riscontrati misurava meno di 10 mm e la grande maggioranza ( 93% ) misurava meno di 20 mm , a conferma del fatto che i noduli tiroidei non palpabili sono di frequente riscontro allo studio ecografico della tiroide , anche in una popolazione non a rischio per patologia tiroidea . 
tuttavia , nonostante uno studio abbia dimostrato come lecografia convenzionale modifichi la gestione clinica nel 63% dei pazienti , lutilit della stessa nel predire la malignit dei noduli tiroidei risulta tuttora controversa , soprattutto se raffrontata con la biopsia ad ago sottile [ 19 ]  . 
finally , a sonographic assessment of possible thyroid abnormalities in 547 overweight individuals from an urban area with relatively low daily iodine intake found thyroid alterations in 56% of subjects [ 18 ]  . 
 in our series , about two thirds of the nodules detected were smaller than 10 mm , and the large majority ( 93% ) were smaller than 20 mm , confirming the fact that nonpalpable thyroid nodules are a common finding on thyroid sonography , even in a population not at risk of thyroid pathology . nonetheless , although it has been demonstrated that conventional us affects clinical management in 63% of patients , its usefulness in predicting the malignancy of thyroid nodules is still controversial , above all when compared with fna [ 19 ]  . indeed , as regards the relative risk of malignancy attributable to the various us findings in nonpalpable thyroid nodules both greyscale and colour doppler it has been shown that there is considerable overlap between benign and malignant lesions [ 14 , 2022 ]  . 
in particular , whereas some authors found that greyscale sonography findings had no value in predicting malignancy [ 23 ] , other more recent studies have suggested a positive predictive role for the presence of irregular or ill - defined margins , microcalcifications , marked hypoechogenicity and anteroposterior diameter greater than longitudinal diameter [ 14 ]  . 
no malignant lesions were found in our series , which indirectly confirms the high specificity of the findings of greyscale sonography and the very low rates of malignant thyroid nodules in the general adult population [ 12 , 16 , 2428 ]  . as regards colour doppler analysis , our series exhibited all the different vascular patterns described in the literature , with a statistically significantly higher prevalence of perinodular flow , the most common flow pattern especially in nodules smaller than 10 mbecause intranodular vascularity was reported as an independent risk factor for malignancy in one study , we decided to regard as suspicious all lesions with intralesional vascularity ( patterns iiia and iiib ) [ 13 , 14 ]  . 
this finding is essentially in agreement with previous reports and confirms that the colour doppler patterns , similar to the greyscale us findings mentioned above , are not highly predictive of malignancy when considered individually [ 22 ]  . 
it should also be noted that the availability of increasingly efficient colour doppler techniques has improved sensitivity in detecting intranodular flow but has also decreased , in terms of specificity , the possibility of characterising thyroid nodules using the colour mode only . 
 a technique described by whittingham in 1997 , spatial cs , has led to improvements in overall image definition , which some studies have reported to be useful for diagnostic purposes , for example , in the field of rotator - cuff imaging [ 2931 ]  . 
although some authors expressed concern about the possible elimination of potentially il rischio relativo di malignit attribuibile ai diversi reperti ecografici sia in scala di grigi che color - doppler nei noduli tiroidei non palpabili , stata dimostrata una non trascurabile sovrapposizione tra le lesioni benigne e quelle maligne [ 14 , 2022 ]  . 
in particolare , nonostante alcuni lavori non abbiano dimostrato la validit dei reperti ecografici in scala di grigi in quanto elementi predittivi di malignit [ 23 ] , altri e pi recenti studi suggeriscono un ruolo predittivo positivo per la presenza rispettivamente di margini irregolari o sfumati , microcalcificazioni , ipoecogenicit marcata e , infine , per la presenza di un diametro antero - posteriore del nodulo maggiore di quello longitudinale [ 14 ]  . 
nella nostra casistica non sono state riscontrate lesioni maligne , il che indirettamente conferma lalta specificit attribuita ai reperti ecografici in scala di grigi , cos come il tasso molto basso , riportato da svariati autori , di neoplasie maligne fra i noduli tiroidei nella popolazione generale adulta [ 12 , 16 , 2428 ]  . per quanto attiene lanalisi color - doppler , nella nostra serie sono stati osservati tutti i differenti pattern di vascolarizzazione descritti in letteratura , con una prevalenza pi alta e statisticamente significativa per il flusso perinodulare , che si rivelato molto pi frequente soprattutto nei noduli di diametro inferiore a 10 mpoich in uno studio la presenza di vascolarizzazione intranodulare era stato riportato come un fattore di rischio indipendente di malignit , ai fini di questo studio si deciso di considerare sospetta ogni lesione che presentasse vascolarizzazione intralesionale ( pattern iiia e iiib ) [ 13 , 14 ]  . 
tale osservazione risulta sostanzialmente in accordo con alcuni dati precedentemente pubblicati , confermando come i pattern color - doppler , allo stesso modo dei gi considerati reperti ecografici in scala di grigi , quando considerati isolatamente , non risultino altamente predittivi di malignit [ 22 ]  . 
in particolare , andrebbe osservato come la diffusione di tecniche color - doppler sempre pi efficaci abbia consentito un incremento della sensibilit nel rilevamento del flusso intranodulare ma , al contempo , abbia condotto ad un decremento , in termini di specificit , della possibilit di caratterizzazione dei noduli tiroidei con il semplice modulo colore . la cs una tecnica ultrasonografica le cui basi sono state descritte da whittingham nel 1997 e la cui applicazione ha condotto ad un miglioramento della definizione dellimmagine che alcuni studi hanno riportato essere utile anche ai fini diagnostici , ad esempio in ambito muscolo - scheletrico ed in particolare nel distretto anatomico della cuffia dei rotatori [ 2931 ]  . 
anche uno studio della ghiandola tiroidea condotto con tale tecnica , ha riportato una minore presenza di artefatti ed una pi alta capacit di evidenziare noduli rispetto allecografia convenzionale [ 10 ]  . 
tuttavia , alcuni autori hanno sollevato alcune perplessit riguardo la possibile eliminazione di artefatti di potenziale rilevanza diagnostica , come , ad esempio , lombra acustica posteriore , segno suggestivo di malignit nelle lesioni mammarie [ 32 ]  . 
anche nella nostra esperienza la cs ha fornito una qualit delle imdiagnostic artefacts such as the posterior shadow , a sign suggestive of malignancy in breast lesions [ 32 ] it has recently been shown that the use of spatial cs does not significantly affect the radiologists assessment of solid breast lesions [ 33 ]  . 
even in our experience , spatial cs of thyroid nodules provided an image quality that was subjectively judged to be better than that of conventional us , and the technique is routinely used at our institution . 
on the other hand , better image quality does not necessarily and immediately translate into a higher detection rate or better diagnostic efficacy , and therefore , further studies are required to assess these aspects . 
although reflecting clinical management , this approach may have led to a slight underestimation of the true number of thyroid cancers even if the number is expected to be extremely small . 
finally , a double - blind review of cases would have enabled us to calculate intraand interobserver variability even if this was only a secondary aim of our study . in conclusion , our series of incidentally discovered thyroid nodules exhibited a high incidence of nodules 1 cm or less in size that were hypoechoic , with exclusively peripheral vascularity and a benign nature . 
daltra parte , anche una migliore qualit dellimmagine pu non tradursi necessariamente ed immediatamente , nella pratica clinica , in un pi elevato tasso di identificazione di noduli tiroidei o in una maggiore efficacia diagnostica e , pertanto , ulteriori studi saranno necessari al fine di valutare tali aspetti . il nostro studio presenta alcune limitazioni . 
in primo luogo , nella nostra casistica non stata disponibile la verifica istologica , anche in relazione al fatto che nei pazienti presi in esame non era presente alcuna indicazione allintervento chirurgico . 
tale approccio , per quanto conforme alla pratica della gestione clinica , pu tuttavia lievemente sottostimare il numero reale di tumori della tiroide , sebbene ci si aspetti che tale cifra sia estremamente bassa . 
una revisione dei casi in doppio cieco , infine , avrebbe consentito il calcolo della variabilit intraed inter - osservatore , anche se questa era una finalit solo secondaria del nostro lavoro . in conclusione , nella nostra casistica di noduli della tiroide riscontrati incidentalmente , risultata elevata lincidenza di noduli di dimensioni pari o inferiori al centimetro , ipoecogeni , con vascolarizzazione esclusivamente periferica e di natura benigna . 
tali reperti suggeriscono , operativamente , un approccio conservativo per questo tipo di noduli , a meno che non siano presenti evidenti segni di malignit allo studio ecografico in scala dei grigi . 
pilon2 1dipartimento di scienze medico - diagnostiche e terapie speciali , sezione di radiologia , 2istituto di clinica chirurgica i , 3istituto di clinica chirurgica ii , universit di padova , italy correspondence to : g . 
barbiero , via fogarine 59 , i - 30030 foss ( ve ) , italy , tel . : + 39 - 0424 - 888795 , fax : + 39 - 0424 - 888791 , e - mail : giuliobarbiero@katamail.com received : 14 january 2006 / accepted : 10 may 2006 / published online : 11 october 2006 abstract purpose . 
the aim of the study was to evaluate quantitatively the main morphological changes of the abdominal aortic aneurysm ( aaa ) - endograft ( eg ) complex following endovascular repair of infrarenal aaa and to evaluate the functional consequences of these changes in terms of rate of complications ( endoleaks and thrombosis )  . 
eighty - five patients ( m / f = 82 / 3 ; mean age at time of operation 70.53.5 years , range 49.989.6 years ) who underwent endovascular treatment of infrarenal aaa between april 1997 and october 2004 with a follow - up of at least 1 month were considered . 
morphological and dimensional changes involved the diameter ( six cases ) and length ( 14 cases ) of aaa proximal neck , diameter ( 36 cases ) and length ( 51 cases ) of the aneurysm sac and shape of the stent - graft ( 47 cases )  . 
aaa growth was correlated with the diameter of the aneurysm sac while shrinkage was correlated with the eg used . during follow - up after endovascular repair , patients require careful evaluation of the morphological and dimensional features of the aaa and eg to promptly identify any changes that can anticipate major complications and even conversion to conventional surgery . 
valutare quantitativamente le principali modificazioni morfologiche del complesso aneurisma ( aaa ) - endoprotesi ( ep ) dopo trattamento endoluminale degli aaa infrarenali , e le loro conseguenze funzionali in termini di incidenza di complicanze ( endoleak e trombosi )  . 
sono stati considerati 85 pazienti consecutivi ( m / f = 82 / 3 ; et media al momento dellimpianto 70 , 53 , 5 anni , range 49 , 989 , 6 anni ) portatori di aaa infrarenale sottoposti fra aprile 1997 e ottobre 2004 a posizionamento di ep per via transfemorale con follow - up post - procedurale di almeno 1 mese . sono stati riesaminati criticamente 408 esami angio - tc eseguiti sia in fase preoperatoria che postoperatoria . 
modificazioni morfodimensionali significative hanno interessato il diametro ( 6 casi ) e la lunghezza ( 14 casi ) del colletto prossimale dellaaa , il diametro ( 36 casi ) e la lunghezza ( 51 casi ) della sacca aneurismatica , e la morfologia dello stentgraft ( 47 casi )  . 
nel follow - up dei pazienti trattati necessaria unaccurata valutazione dei parametri morfodimensionali sia dellaaa che dellep allo scopo di coglierne precocemente eventuali modificazioni che possano precedere importanti conseguenze funzionali , fino alla necessit di conversione laparotomica . parole chiave aneurisma aortico addominale trattamento endovascolare endograft endoleak c . 
after endoluminal treatment , the proximal neck , the major site of fixation of the eg to the aortic wall [ 4 , 5 ] , may become progressive dilated [ 6 , 7 ] , facilitating the development of a secondary type - 1 endoleak ( el ) , that is , persistence of perigraft blood flow ( table 1 ) [ 8 , 9 ] , with resulting expansion of the aaa and increased risk of rupture [ 1012 ]  . 
after complete endoluminal exclusion , the aneurysm sac shrinks progressively , especially in larger aaa and with certain types of eg , sometimes to the point of complete reabsorption of perigraft thrombotic material [ 1321 ]  . 
in some cases , however , the aaa enlarges after eg implantation , an indication of persistent pressurisation of the aneurysm sac , even in the absence of endotension dopo esclusione di un aneurisma dellaorta addominale ( aaa ) dal torrente circolatorio mediante endoprotesi ( ep ) [ 13 ] , si verifica un rimodellamento del complesso aaa - ep nel tempo , che interessa il colletto sottorenale , la sacca aneurismatica e lep stessa . 
il colletto prossimale , sito principale di fissazione dellep alla parete aortica [ 4 , 5 ] , dopo trattamento endoluminale pu subire una progressiva dilatazione [ 6 , 7 ] , che favorisce linsorgenza di endoleak ( el ) , ossia persistenza di flusso sanguigno periprotesico ( tabella 1 ) [ 8 , 9 ] , di tipo i secondario , con conseguente espansione dellaaa e , quindi , aumentato rischio di rottura [ 1012 ]  . 
la sacca aneurismatica , dopo esclusione endoluminale completa , generalmente subisce una progressiva contrazione ( shrinkage ) nel tempo , specie negli aaa pi grandi e con certi tipi di ep , talvolta fino al completo riassorbimento del materiale trombotico periprotesico [ 1321 ]  . 
talvolta , per , si verifica unespansione dellaaa post - ep , indice di pressurizzazione persistente della sacca aneurismatica , anche in assenza di el ( endotension ) [ 2224 ]  . 
lep , infine , pu presentare distorsioni ed table 1 classification based on aetiology of the endoleak ( adapted from [ 36 ] ) endoleak cause of the perigraft blood flow insufficient seal at the graft ends at the proximal end at the distal end insufficient seal of an iliac occlusion device retrograde blood flow from aortic branches ( lumbar arteries , inferior mesenteric artery , hypogastric arteries , accessories renal arteries ) graft disconnection or graft disintegration graft disconnection fabric tears minor ( < 2 mm ) major ( 2 mm ) type 4 type 5 endoleak of undefined origin unknown cause graft wall porosity ( within 30 days after endovascular repair ) persistent aneurysm sac pressurisation with no evidence of the source of leakage ( endotension ) tabella 1 classificazione eziologica degli endoleak ( da [ 36 ] , modificata ) endoleak causa del flusso periprotesico incompleto contatto della protesi con la parete vascolare a livello delle sue estremit dellestremit prossimale dellestremit distale da inefficienza di un dispositivo di occlusione iliaca da flusso retrogrado attraverso vasi viscerali ( arterie lombari , mesenterica inferiore , ipogastriche , renali accessorie ) per disconnessione dei moduli protesici o per rottura della protesi per disconnessione dei moduli protesici per rottura del tessuto protesico : minore ( < 2 mm ) maggiore ( 2 mm ) tipo iv tipo v endoleak di origine indeterminata visualizzazione dellendoleak senza determinazione della sua origine da porosit del tessuto protesico ( nei primi 30 giorni dopo il posizionamento dellendoprotesi ) pressurizzazione persistente della sacca aneurismatica senza rifornimento dimostrabile ( endotension ) type 1 type 2 type 3 tipo i tipo ii tipo iii c . 
finally , the eg may develop distortions and kinking [ 2528 ] and in some cases structural disintegration , with a risk of type - 3 el and a need for repeat endovascular procedures or surgical conversion . 
alternatively , it may migrate distally , resulting in type - 1 el secondary to loss of proximal seal [ 2934 ]  . the aim of this study was to quantitatively evaluate the main morphological changes affecting the aaa - eg complex after endovascular treatment and the functional consequences of these changes in terms of rate of complications ( in particular , el and thrombosis )  . 
in addition , we assessed whether the morphological and structural changes could be related to the preprocedural size of the aaa and to the type of eg used . angolazioni nel tempo [ 2528 ] , fino ad arrivare in certi casi ad un cedimento strutturale , che pu determinare la comparsa di un el di tipo iii e , quindi , la necessit di procedure endovascolari secondarie o conversione chirurgica , oppure pu presentare una migrazione distale con conseguente el di tipo i secondario da perdita del sealing prossimale [ 2934 ]  . scopo di questo lavoro valutare quantitativamente le principali modificazioni morfologiche del complesso aaa - ep dopo trattamento endoluminale , e le loro conseguenze funzionali in termini di incidenza di complicanze ( in particolar modo el e trombosi )  . 
inoltre si intende valutare se tali modificazioni morfofunzionali possano essere messe in relazione alle dimensioni preprocedurali dellaaa e al tipo di ep impiegato . materials and methods we studied 85 consecutive patients with infrarenal aaa ( m / f = 82 / 3 ; mean age at time of operation 70.53.5 years , range 49.989.6 years ) who underwent transfemoral eg placement between april 1997 and october 2004 and were followed up for at least 1 month . 
seven eg models from different manufacturers were used ( table 2 ) , of which one ( 1.2% ) was a straight aortoaortic tubular eg and 84 ( 98.8% ) were bifurcated aortobiiliac eg . 
the follow - up included a colour - doppler ultrasound ( us ) scan at discharge or a ct angiography scan on day 7 , followed by periodic ct angiography studies at 1 , 3 , 6 and 12 months and yearly thereafter . 
in 10 pazienti ( 11 , 8% ) il trattamento endovascolare stato eseguito pur non rispettando completamente i criteri suggeriti dalla letteratura [ 5 ] in quanto vi era controindicazione assoluta allintervento chirurgico tradizionale e laaa era ad alto rischio ( 4 pazienti con colletto sottorenale breve , 1 paziente con colletto prossimale ampio , 1 paziente con diametro dellaaa > 7 cm e infine 4 pazienti con esili arterie renali accessorie originanti dal colletto prossimale o dalla sacca aneurismatica )  . 
sono stati utilizzati 7 modelli di ep di case costruttrici diverse ( tabella 2 ) , di cui solo una ( 1 , 2% ) di tipo tubulare retto aorto - aortico , e 84 ( 98 , 8% ) di tipo biforcato aorto - bisiliaco . 
il follow - up dei pazienti trattati prevedeva un controllo mediante eco - color - doppler alla dimissione o lesecuzione di un angio - tc in settima giornata , seguita da controlli periodici mediante angio - tc a 1 , 3 , 6 , 12 mesi e quindi annualmente . 
di ogni esame tc sono stati valutati : diametro e lunghezza del colletto prossimale aortico , diametri anteroposteriore ( ap ) , laterolaterale ( ll ) e trasverso massimo ( mtr ) dellaaa ( che corrisponde al diametro trasverso minimo in una sezione ellittica del vaso ) , lunghezza dellaaa , morfologia e lunghezza ed eventuale dislocazione longitudinale dellep , presenza di el e / o trombosi endoprotesica . 
eg migration was evaluated by comparison to the first postprocedural ct scan by measuring the length of the infrarenal aorta not covered by the stent - grael and endoluminal thrombosis were assessed by comparing the ct scans before and after contrast administration and by performing densitometric measurements in equivocal cases [ 35 ]  . 
in acquiring the data , we followed the standards proposed by the ad hoc committee for standardized reporting practices in vascular surgery of the society for vascular surgery / 1nternational society for cardiovascular surgery ( svs / iscs ) [ 36 ]  . 
changes in diameter or length of at least 5 mm relative to preprocedural values were considered significant , in part to minimise intraand interobserver differences in measurement , as suggested by svs / iscs [ 36 ]  . statistical analysis a log - rank test was used to measure the relationship between changes in aaa size relative to preprocedural size , considering all 85 patients divided into two groups on the basis of a 50 - mm cut - off transverse diameter of the aaa . 
la dislocazione dellep stata valutata rispetto alla prima tc post - procedurale , misurando la lunghezza della porzione aortica sottorenale non ricoperta dallo stent - gralel e la trombosi endoluminale sono stati valutati confrontando le scansioni tc pree post - mdc e mediante misurazioni densitometriche nei casi dubbi [ 35 ]  . nellacquisizione dei dati si sono seguiti gli standard proposti dal ad hoc committee for standardized reporting practices in vascular surgery of the society for vascular surgery / international society for cardiovascular surgery ( svs / iscs ) [ 36 ]  . si considerata significativa una variazione di diametro e / o lunghezza di almeno 5 mm rispetto ai valori preposizionamento , anche allo scopo di minimizzare le differenze di misurazione intraed inter - osservatore , come suggerito dalla svs / iscs [ 36 ]  . analisi statistica stata valutata , mediante log - rank test , la relazione fra le modificazioni dimensionali dellaaa rispetto alle dimensioni pre - procedurali , considerando tutti gli 85 pazienti suddivisi in 2 gruppi in base a un diametro trasverso soglia dellaaa di 50 m stata valutata , sempre mediante log - rank test , anche la relazione fra le modificazioni dimensionali dellaaa rispetto al tipo di ep impiegato , considerando un sottogruppo di 75 pazienti cui era stato impiantato uno dei 3 modelli di ep maggiormente utilizzati ( aneurx , talent ed excluder )  . 
statistical significance was set at p < 0.05. risultati table 4 available follow - up data follow - up patients repair 1 month 3 months 6 months 1 year 2 years 3 years 4 years 5 years 6 years 7 years follow - up procedura 1 mese 3 mesi 6 mesi 1 anno 2 anni 3 anni 4 anni 5 anni 6 anni 7 anni le caratteristiche morfodimensionali preprocedurali degli aaa trattati sono presentate in tabella 3 . 
la durata media della procedura in sala operatoria stata di circa 120 minuti , con un tempo medio di scopia di 15 , 41 , 4 min ( range 558 min )  . 
la durata media del follow - up risultata di 34 , 459 , 3 mesi ( range 189 mesi )  . modificazioni morfodimensionali del colletto prossimale si verificato un aumento significativo ( > 5 mm ) del diametro del colletto prossimale in 2 pazienti ( 2 , 4% ) e un aumento ai limiti della significativit ( 5 mm ) in altri 4 pazienti ( 4 , 7% ) , di cui 2 con discesa e angolazione dellep e un caso con rottura dello stent prossimale ( vanguard )  . 
non vi sono state variazioni significative ( > 5 mm ) della lunghezza del colletto prossimale nei controlli tc effettuati . un aumento significativo ( > 5 mm ) del diametro trasverso massimo ( mtr ) dellaaa si verificato in 7 pazienti ( 8 , 2% ) nel corso del follow - up ( range 718 mm ) , ed era sempre associato ad aumento significativo ( > 5 mm ) anche del diametro trasverso ap e / o ll dellaaa . 
the mean duration of the repair procedure was 120 min , with a mean fluoroscopy time of 15.41.4 ( range 558 ) mavailability of follow - up data at the time of the analysis ( 31 october 2004 ) is shown in table 4 . 
mean duration of follow - up was 34.459.3 ( range 189 ) months . changes in size and shape of the proximal neck a significant increase ( > 5 mm ) in proximal neck diameter was seen in two patients ( 2.4% ) and an almost significant increase ( 5 mm ) in another four ( 4.7% ) , two of whom had caudal migration and kinking of the eg and one with disintegration of the proximal stent ( vanguard )  . 
 changes in shape and size of the aneurysm sac a significant increase ( > 5 mm ) in the maximum transverse ( mtr ) diameter of the aaa was observed during follow - up in seven patients ( 8.2% ) ( range 718 mm ) , and it was constantly associated with a significant increase ( > 5 mm ) in the ap and / or ll transverse diameter of the aaa . 
the significant reduction in one of the three transverse diameters of the aaa was associated with absence of el in 25 cases and presence of type - 2 el in four cases . 
la velocit media di riduzione della lunghezza dellaaa fu di 22 , 5 mm / anno ( range 2 , 160 , 0 mm / anno )  . modificazioni morfologiche e dislocazioni dellendoprotesi modificazioni morfologiche dellep , da minime a rilevanti , sono state osservate in 47 pazienti ( 55 , 3% ) , di cui 24 in cui la modificazione morfologica era gi presente entro il 1 mese dallimpianto dellep ( comprese 5 virgin position )  . le modificazioni morfologiche potevano interessare il corpo principale ( 15 casi ) , una o entrambe le branche iliache ( 23 casi ) o tutte le componenti dellep ( 9 casi )  . 
alterazioni morfologiche dellasse longitudinale dellep ( concavit , convessit , angolazioni , rettilineizzazioni ) erano presenti in 37 casi ( 43 , 5% ) , mentre alterazioni morfologiche dellasse trasversale ( restringimenti , allargamenti ) erano presenti , invece , in 10 casi ( 11 , 8% )  . 
le alterazioni morfologiche risultarono associate in 12 casi ( 14 , 1% ) a trombosi endoprotesica di grado variabile ( da minima apposizione trombotica endoluminale fino allocclusione di branca ) e in 15 casi ( 17 , 6% ) ad el ( 2 el di tipo i , 10 el di tipo ii e 3 el di tipo iii )  . 
in 4 casi ( 4 , 7% ) di alterazione morfologica dellep si rese necessaria la conversione laparotomica : 2 casi per el di tipo ia , 1 caso per el di tipo iii da rottura dello stent pi craniale ( vanguard ) e 1 caso per eccessiva angolazione delle componenti protesiche ( anaconda )  . 
le valutazioni della lunghezza dellep sono state escluse dallo studio , essendo risultate le misure assai variabili nei controlli tc e , pertanto , giudicate non sufficientemente attendibili . si sono verificati 13 casi ( 15 , 3% ) di dislocazione caudale significativa ( > 5 mm ) dellep rispetto al 1 controllo tc post - procedurale , dei quali 4 con associato allargamento del colletto prossimale aortico , e 6 con discesa dellep particolarmente marcata ( > 15 mm ) e conseguente angolazione pi o meno accentuata delle sue componenti ( 2 aneurx , 2 talent , 1 vanguard e 1 anaconda )  . 
evaluations of eg length were excluded from the study because ct measurements were extremely variable and therefore not considered sufficiently reliable . there were 13 cases ( 15.3% ) of significant downward migration ( > 5 mm ) of the eg relative to the first postprocedural ct study ; four of these were associated with enlarged proximal aortic neck and six with particularly marked downward slippage of the eg ( > 15 mm ) and resulting angulation of its components ( two aneurx , two talent , one vanguard and one anaconda )  . 
in addition , there was one case ( 1.2% ) of significant upward migration ( > 5 mm ) of the eg ( talent ) at 3 months , with resulting exclusion of the ostium of a main renal artery and reduction in renal perfusion . 
 endoleaks a total of 36 el occurred in 32 patients ( 37.6% ) , with four ( 4.7% ) having two el of a different type ( types 1 and 2 )  . 
in detail , there were six type - 1 el ( four primary and two secondary ; two proximal and four distal ) and 26 type - 2 el ( 16 primary and ten secondary ; 11 el resolved spontaneously , seven remained essentially unchanged and eight worsened ) due to retrograde flow from the inferior mesenteric artery ( ten cases ) , lumbar arteries ( seven cases ) , hypogastric arteries ( six cases ) or mixed origin ( three cases )  . 
inoltre vi furono 3 el di tipo iii ( 2 primari e 1 secondario ) e un caso di verosimile el di tipo iv con scomparsa spontanea in 12 giornata post - procedurale . trombosi endoprotesica trombosi endoprotesica di qualsiasi entit ( da minima a occludente ) stata riscontrata in 23 pazienti ( 27 , 1% ) : a livello del corpo dellep in 7 pazienti , a livello di una singola branca iliaca protesica in 11 pazienti , a livello di entrambe le branche iliache dellep in 2 pazienti , e a livello sia di corpo che di branca iliaca dellep in 3 pazienti . 
kaplan - meier curves for freedom from aaa growth > 5 mm in relation to the diameter of the aaa sac [ 85 patients with follow - up 1 month , grouped according to aaa diameter < 50 mm ( n = 49 ) or 50 mm ( n = 46 ) ]  . 
confronto delle curve di kaplan - meier per la libert da riduzione dellaaa > 5 mm in relazione al diametro massimo trasverso iniziale dellaaa ( 85 soggetti con follow - up di almeno 1 mese , ripartiti in 2 gruppi : gruppo 1 , n = 49 , aaa < 50 mm ; gruppo 2 , n = 46 , aaa ( cid : 2 ) 50 mm )  . tion in sample size , which prevents accurate assessment of morphological changes in the aaa - eg complex and the incidence of the long - term complications of endovascular repair . 
moreover , the suggested anatomical and morphological criteria for selecting candidates to eg implantation were not always applied because the risk - benefit analysis indicated a clear advantage of endovascular repair compared with the risk of surgical conversion . proximal neck despite six cases ( 7.1% ) of increased proximal neck diameter , none of which were associated with type - 1a el , in most cases , proximal - neck diameter ( 79 cases , 92.9% ) and length ( 85 cases , 100.0% ) remained essentially stable , in agreement with the literature [ 7 ] , the proximal neck is the transition between the extraaneurysmal aorta ( healthy ) and the aneurysmal aorta ( diseased ) and , despite there not being any significant reduction in radial forces after repair , it is subjected to the additional centrifugal force exerted by the eg itself . 
 aneurysm sac changes in shape and size of the aneurysm sac involved the three transverse diameters ( maximum , ap and ll ) and the length of the aaa even though the most frequently used parameter for evaluating morphological changes of the sac is the mtr , which corresponds to the minimal transverse diameter in an elliptical section of the vessel . 
changes in ap and / or ll diameter were always associated with changes in mtr , but not vice versa , a sign that mtr is a more sensitive index of variations in the size of the aneurysm sac . there were 36 cases ( 42.4% ) of significant mtr changes , metro trasverso minimo in una sezione ellittica del vaso . 
infatti unalterazione del diametro ap e / o ll dellaaa era sempre associata ad alterazione del mtr , ma non viceversa , segno , quindi , che il mtr rappresenta un indice pi sensibile di variazione dimensionale della sacca aneurismatica . si ebbero 36 casi ( 42 , 4% ) di modificazioni significative del mtr , 30 dei quali ( 83 , 3% ) entro i primi 30 mesi di follow - up , e 51 casi ( 60 , 0% ) di modificazioni significative della lunghezza dellaaa , 38 dei quali ( 74 , 5% ) entro i primi 30 mesi di follow - up , dati che sembrerebbero confermare , come affermato dalla letteratura , che le variazioni dimensionali dellaaa , per lo meno quelle in senso riduttivo , si osservano prevalentemente nei primi mesi di follow - up , per poi assestarsi in una sorta di plateau , perch i fenomeni di rimodellamento di un aaa completamente escluso avvengono in tempi relativamente brevi . il riscontro relativamente precoce di crescita significativa del mtr e / o della lunghezza dellaaa , invece , verosimilmente dovuto allassociazione con el ( 100 , 0% dei casi di aumento del mtr e 80 , 0% dei casi di aumentata lunghezza dellaaa ) , il quale el si evidenzi piuttosto precocemente ( 100 , 0% degli el di tipo ii e iv , 71 , 4% degli el di tipo i e 66 , 7% degli el di tipo iii comparvero entro i primi 30 mesi )  . da questi dati si deduce che la maggior parte dei pazienti trattati ha presentato una riduzione del volume totale dellaaa ( anche se tale parametro non stato direttamente calcolato ) , in virt della diminuzione dei diametri trasversi e / o della lunghezza dellaaa stesso e , quindi , una diminuzione del rischio di rottura . 
tale progressiva riduzione volumetrica dellaaa spiegabile con il rimodellamento dello stesso alle nuove condizioni createsi dopo la sua esclusione endoluminale , che hanno portato ad una riduzione della pressione endoluminale , e quindi della forza radiale esercitata sulle pareti della sacca stessa . la stragrande maggioranza degli aaa in crescita significativa ( 11 / 13 , 84 , 6% ) era associata a persistenza di flusso c . 
 the relatively early finding of a significant increase in mtr and / or aaa length is , instead , probably due to the associated el ( 100.0% of cases of increased mtr and 80.0% of cases of increased aaa length ) , which developed relatively early ( 100.0% of types 2 and 4 , 71.4% of type 1 and 66.7% of type 3 el developed within 30 months )  . it can be inferred that the majority of patients experienced a reduction in the total volume of the aaa ( even though this parameter was not calculated directly ) given that the transverse diameters and / or length of the aaa were reduced , and therefore a lower risk of rupture . 
this progressive decrease in aaa volume can be explained by the aneurysm remodelling to adapt to the new conditions resulting from its exclusion , which led to reduced endoluminal pressure and radial pressure on the sac walls . the vast majority of aaa that enlarged significantly ( 11 / 13 , 84.6% ) were associated with persistent perigraft flow after eg implantation . 
the only two cases ( 2 / 13 , 15.4% ) without el were significant increases in length ( 1 and 4 months postprocedure , respectively ) , both of which were followed by equally significant shortening . 
even these cases could be accounted for by transient persistent pressurisation of the aaa during the early phases of follow - up , which was related to the transmission of pressure from the eg to the mural thrombus and aortic walls . 
these data seem to confirm the presence of el as the main risk factor for significant aaa growth even though only type - 1 and type - 3 el have been shown to be associated with aaa growth [ 3742 ]  . 
only types 1 , 2 and 3 were associated with significant aaa growth ; the only case of type - 4 el had disappeared at ct follow - up on day 12 , so its relatively short life did not allow any significant increase in aaa size . 
the controversial role of type - 2 el is discussed below . endograft over a period of 7 years , seven different types of eg were implanted , with heterogeneous distribution : some of them are no longer available ( vanguard , endologix , anaconda , passager ) , and others have undergone major redesign over the years ( talent )  . 
for this reason and because our experience with other models was too limited , our evaluation of the morphological and functional changes of the aaa in relation to type of eg was based on the three most commonly used models ( aneurx , talent , excluder )  . sanguigno periprotesico dopo limpianto di ep e gli unici 2 casi ( 2 / 13 , 15 , 4% ) osservati in assenza di el erano precoci aumenti significativi di lunghezza ( rispettivamente ad 1 e a 4 mesi dallimpianto dellep ) , seguiti , poi , entrambi da accorciamento altrettanto significativo . 
anche tali casi potrebbero essere spiegati con una transitoria persistente pressurizzazione dellaaa nelle prime fasi di follow - up , legata a trasmissione di pressione dallep al trombo murale e , quindi , sulle pareti aortiche . 
questi dati confermerebbero , pertanto , la presenza di endoleak quale fattore di rischio principale per la crescita significativa dellaaa , anche se dalla letteratura risulta che soltanto gli el di tipo i e iii sono statisticamente associati a crescita dellaaa [ 3742 ]  . 
soltanto i tipi i , ii e iii di el risultarono associati a crescita significativa dellaaa , poich lunico caso osservato di el di tipo iv scomparve al controllo tc in 12a giornata e quindi la sua durata relativamente breve non permise un significativo aumento delle dimensioni dellaaa . 
il ruolo controverso degli el di tipo ii , invece , discusso pi avanti . endoprotesi nellarco di 7 anni sono stati impiantati ben 7 tipi differenti di endoprotesi , con una distribuzione non omogenea : alcuni di essi sono stati ormai ritirati dal commercio ( vanguard , endologix , anaconda , passager ) , altri hanno subito delle modificazioni importanti nel corso degli anni ( talent )  . 
tutto ci riflette la continua evoluzione tecnica dei device disponibili e rappresenta un grosso problema nella valutazione dei risultati poich , ovviamente , rende assai difficili i confronti tra pazienti portatori di ep diverse . 
per questo nella valutazione delle modificazioni morfofunzionali degli aaa in rapporto al tipo di ep abbiamo considerato soltanto i 3 modelli da noi maggiormente utilizzati ( aneurx , talent , excluder ) in quanto le nostre esperienze con gli altri modelli erano numericamente troppo esigue . quanto alle modificazioni morfologiche dellep , in 5 pazienti ( 5 , 9% ) stato adottato volontariamente un posizionamento dellep con incrocio delle branche iliache ( virgin position ) allo scopo di preservare la perviet di una o entrambe le arterie ipogastriche . 
infatti , nonostante la grande disponibilit di misure diverse per ciascun tipo di ep , vi sono certe situazioni ( origine precoce di una o entrambe le arterie ipogastriche , marcata tortuosit di uno o entrambi gli assi iliaci ) in cui la scelta del tipo di ep risulta difficile e non priva di rischi . 
pertanto , in mancanza di misure adeguate dellep , allo scopo di ridurne la lunghezza sullasse longitudinale , pu venire eseguita tale procedura , che sfrutta la rotazione di 180 sul piano trasversale delle branche iliache allinterno della sacca aneurismatica per far atterrare lestremo distale delle branche iliache stesse a monte dellemergenza delle arterie ipogastriche . oltre a queste modificazioni morfologiche indotte , ci sono tutta una serie di altre alterazioni della morfologia dellep che possono influenzare negativamente la funzione del device , quali concavit , convessit , angolazioni , restringimenti , etc . 
despite the wide availability of different sizes for each eg model , there are some situations ( early origin of one or both hypogastric arteries , marked tortuosity of one or both iliac axes ) where the choice of eg is difficult and not free of risks . 
as a result , when adequate eg sizes are lacking , eg length can be reduced by applying this procedure , which exploits the 180 transverse rotation of the iliac branches inside the aneurysm sac to place the distal end of the iliac branches above the emergence of the hypogastric arteries . in addition to these induced morphological changes , there are changes in eg morphology that may negatively affect device function , such as concavity , convexity , kinking , narrowing , etc . 
according to virchows triad , one factors responsible for thrombosis is slow flow , which arises when the flow changes from laminar to turbulent , as occurs at bifurcations or just below vessel strictures . 
in one of our cases , there was complete thrombosis of an iliac branch of the eg , ascribable to inadequate expansion 1 month after implantation , which was successfully treated by percutaneous transluminal angioplasty ( pta )  . 
most morphological changes observed were , however , minimal and not associated with endoluminal thrombosis . even the el , and especially graft - related el ( types 1 and 3 ) , might have been promoted by a preexisting morphological change in the eg extremities or at the junction between the main body and the contralateral iliac branch in modular models : the first situation facilitates detachment of the eg from the vessel walls ; the second may lead to separation of the graft components . 
in particular , there was one case of proximal stent disintegration ( vanguard ) 51 months after implantation in a patient who had never shown changes in graft morphology or significant variations in the aaa or the proximal neck ; loss of adherence between the eg and the aorta wall resulted in a massive type - 3 el and the patient had to undergo late surgical conversion . it is interesting to note that some morphological changes of the eg could also have affected the adjacent vessel segments not covered by the graft , leading to sharp angulations or kinking . 
although not directly addressed in our study in part because of lack of adequate 3d ct reconstructions [ maximum intensity projection ( mip ) and volume rendering technique ( vrt ) ] for some patients this phenomenon occurred in at least three cases ( 3.5% ) and could have been due to remodelling not only of the aaa but also of the uncovla trombosi endoprotesica poteva essere favorita dallalterazione morfologica quando questa comportava una significativa alterazione del flusso endoprotesico , tale da favorire il deposito di materiale trombotico sulle pareti interne dellep , come in caso di angolazioni e / o restringimenti del calibro luminale . 
secondo la triade di virchow , infatti , uno dei fattori responsabili della trombosi rappresentato dal rallentamento del flusso , che si verifica laddove il regime di flusso , normalmente di tipo laminare , diventa di tipo vorticoso , come in corrispondenza delle biforcazioni o subito a valle dei restringimenti del calibro vasale . 
in un caso , poi , si verific la trombosi completa di una branca iliaca protesica , attribuibile alla scarsa espansione della stessa ad 1 mese dallimpianto , trattata poi con successo mediante pta . 
la maggior parte delle alterazioni morfologiche osservate , tuttavia , era di minima entit e non si associava a trombosi endoluminale . anche gli endoleak , specie i cosiddetti el graft - correlati ( tipi i e iii ) , potevano essere favoriti da una preesistente alterazione della morfologia dellep , quando questa interessava uno degli estremi dellep , oppure il sito di embricazione fra corpo principale e branca iliaca controlaterale nei modelli modulari , perch favorisce il distacco dellep dalle pareti vasali nel primo caso , o dei singoli elementi protesici nel secondo . 
in particolare si verific un caso di rottura dello stent prossimale dellep ( vanguard ) a 51 mesi dallimpianto in una paziente che non aveva mai mostrato prima alterazioni della morfologia del graft , n variazioni significative dellaaa o del colletto prossimale ; la perdita di ancoraggio fra lep e la parete aortica determin , di conseguenza , un el di tipo iii massivo e la paziente fu pertanto sottoposta a conversione chirurgica tardiva . interessante notare che talune alterazioni morfologiche dellep potevano talvolta ripercuotersi anche nei segmenti vasali adiacenti non ricoperti dal graft determinando brusche angolazioni o kinking vasali a stretto raggio di curvatura . 
tale fenomeno , pur non essendo stato affrontato direttamente nello studio , anche per la mancata disponibilit di adeguate ricostruzioni tc tridimensionali ( soprattutto mip e vrt ) per alcuni pazienti , si verific in almeno 3 casi ( 3 , 5% ) e potrebbe essere spiegato con il rimodellamento non solo dellaaa , ma anche dei segmenti aortici e iliaci non ricoperti adiacenti allep e sottoposti a brusche forze longitudinali e / o torsionali da parte del graft . la presenza di importanti alterazioni morfologiche dellep stata considerata fattore di indicazione sufficiente per la conversione laparotomica , come in un caso ( 1 , 2% ) di espianto dellep ( anaconda ) a 17 mesi di follow - up . 
un altro caso simile , con severa angolazione ( < 90 ) a livello del corpo principale dellep , tuttora sotto stretto follow - up . riteniamo che i casi di marcata alterazione morfologica dellep debbano essere tenuti sotto stretta osservazione , in quanto a rischio di rottura , anche se lunico caso riportato di rottura dellep non aveva mai presentato prima alterazioni della morfologia del graft . la valutazione delle alterazioni di lunghezza dellep non stata presa in considerazione a causa dellalta variabilit delle misure , legata sia alla variabilit intraed inter - osservatore , che alla non disponibilit di adeguate ricostruzioni tc tridimensionali per alcuni pazienti . interessanti , infine , sono le dislocazioni longitudinali c . 
we believe that cases of marked eg morphological change should be closely monitored due to the risk of rupture even if the only case of eg failure never showed alterations in graft morphology . changes in eg length were not evaluated due to the wide variation in measurements related both to intraand interobserver variability and to the lack of adequate 3d ct reconstructions for some patients . finally , longitudinal migrations of the eg were interesting . 
on release , the eg is usually positioned with the covered proximal portion just beneath the ostium of the more caudad renal artery so as to cover almost completely the infrarenal neck of the aaa and exploit the entire length available for eg fixation . 
however , even though eg deployment was technically correct , 13 cases ( 15.3% ) showed significant caudal migration ( > 5 mm ) , with marked downward slippage ( > 15 mm ) of the stent - graft in six ( 46.2% ) during follow - up . 
increased length of the infrarenal aorta not covered by the eg could be related to the physiological lengthening of the aortic walls as a result of progression of atherosclerotic disease . 
by increasingly weakening vessel walls , atherosclerosis induces both a lengthening and widening of the vessel whereas in most patients , the increase in length of this uncovered segment of the aorta was not matched by an increase in diameter , meaning that the lengthening was only apparent and most probably due to distal migration of the eg . 
therefore , an isolated lengthening of the uncovered infrarenal portion of the aorta can be considered an indirect sign of caudal migration of the eg and should be carefully assessed in relation to the length measured at early postprocedural ct follow - up , which becomes crucial . the six cases ( 7.1% ) of marked downward slippage ( > 15 mm ) of the eg were associated with more or less marked angulations of the device due to loss of proximal fixation and resulting distal migration ; in the presence of stable distal fixation , this caudal migration led to shortening and kinking inside the aneurysm sac with possible haemodynamic consequences , especially at the level of the iliac branches , and eg thrombosis ( three cases )  . the only case of significant upward migration ( > 5 mm ) of the eg at 3 months led to occlusion of the origin of one of the renal arteries . 
generalmente , al momento del rilascio , lep viene collocata posizionandone la parte prossimale ricoperta subito al di sotto dellostio dellarteria renale pi caudale , in modo da ricoprire pressoch completamente il colletto sottorenale dellaaa , allo scopo di sfruttare tutta la lunghezza disponibile per il fissaggio dellep . 
tuttavia , anche se il posizionamento endoprotesico stato tecnicamente corretto , in 13 casi ( 15 , 3% ) si verificata una migrazione caudale significativa ( > 5 mm ) dellep con marcata discesa ( > 15 mm ) dello stent - graft in 6 di essi ( 46 , 2% ) nel corso del follow - up . laumentata lunghezza della porzione aortica sottorenale non ricoperta dallep potrebbe essere legata al fisiologico allungamento delle pareti vasali aortiche in rapporto alla naturale progressione della malattia aterosclerotica . 
generalmente il processo aterosclerotico , determinando un progressivo sfiancamento delle pareti vasali , provoca sia un allungamento che un allargamento del calibro del vaso , mentre nella maggior parte dei pazienti allaumento di lunghezza di tale segmento aortico non ricoperto non corrispondeva un altrettanto aumento del suo diametro , segno che lallungamento , solo apparente , era dovuto , pi probabilmente , a migrazione distale dellep . 
pertanto , un allungamento isolato della porzione aortica sottorenale non ricoperta pu essere considerato un segno indiretto di dislocazione caudale dellep e , quindi , deve essere valutato attentamente comparandolo sempre con il valore al precoce controllo tc postimpianto , che assume cos unimportanza cruciale . nei 6 casi ( 7 , 1% ) di marcata discesa ( > 15 mm ) dellep si associarono , poi , angolazioni pi o meno accentuate del device , dovute a perdita dellancoraggio prossimale del graft , con conseguente migrazione distale dellep ; in presenza di un ancoraggio distale stabile , tale dislocazione caudale dellep determinava un accorciamento della sua lunghezza sullasse longitudinale e , pertanto , la formazione di kinking allinterno della sacca aneurismatica con possibili conseguenze emodinamiche per alterazione dei regimi di flusso , specialmente a livello delle branche iliache , con possibile trombosi endoprotesica ( 3 casi )  . lunico caso di risalita significativa ( > 5 mm ) dellep a 3 mesi dallimpianto ha portato a occlusione dellorigine di unarteria renale . 
tale fenomeno , assai inconsueto per la pi facile possibilit di migrazione distale del device a causa della direzione centrifuga del flusso ematico , potrebbe , tuttavia , essere spiegato con un ancoraggio distale stabile dellep subito a monte delle biforcazioni iliache , per cui il riequilibrio delle forze in gioco avrebbe potuto determinare una spinta risultante verso lalto e , quindi , la risalita dellep stessa . trombosi endoprotesica la trombosi endoprotesica ( 27 , 1% dei pazienti trattati ) complicanza abbastanza frequente nel trattamento endovascolare degli aaa . 
a livello delle branche iliache , essendo minore il calibro e per fattori emodinamici , pu portare a ostruzione completa e , quindi , a necessit di ulteriori procedure di ricanalizzazione , che comportano un rischio aggiuntivo per il paziente e non sempre risultano efficaci ( 4 casi di occlusione trombotica , 2 dei quali esitati in conversione chirurgica )  . 
interessante notare che la trombosi endoluminale si rese evidente alla tc entro i primi 2 anni dallimpianto in 18 / 23 pazienti ( 78 , 3% ) ed entro i primi 3 anni dallimc . 
at the level of the iliac branches , due to the smaller calibre and to haemodynamic factors , it may result in complete occlusion and in the need for further recanalisation procedures that , as well as being an additional risk , are not always successful ( four cases of thrombotic occlusion , two of which requiring surgical conversion )  . 
it is interesting to note that the thromboses became manifest at ct within the first 2 years of implantation in 18 / 23 patients ( 78.3% ) and within the first 3 years in 22 / 23 patients ( 95.7% ) and that the four cases of complete iliac branch occlusion all occurred within the first year of implantation . 
these data underline the importance of a close follow - up of patients treated with eg , above all during the first year of follow - up , even if a certain degree of risk of eg thrombosis remains . 
whereas it is accepted that types 1 and 3 require prompt treatment since they are associated with significant aaa growth and increased risk of rupture , the management of type - 2 el is more challenging , partly because they tend to resolve spontaneously . 
this would seem to indicate that early appearance is predictive of spontaneous el thrombosis and that the spontaneous closure is rare after more than 12 months , as has been reported in the literature [ 38 ]  . 
as regards the decision whether or not to treat type - 2 el , treatment is only indicated in the presence of aaa growth whereas a watchful , waiting approach is indicated in all other cases [ 3942 ]  . 
the presence of type - 2 el may be associated with stability or even reduction in aaa volume : we had 20 cases ( 76.9% ) of mtr stability and two ( 7.7% ) of significant mtr reduction ( > 5 mm ) despite the presence of type - 2 el , which confirms that the association pianto in 22 / 23 pazienti ( 95 , 7% ) , e che i 4 casi di trombosi completa di branca iliaca si verificarono tutti entro i primi 12 mesi dallimpianto . 
questi dati sottolineano , pertanto , limportanza di una stretta sorveglianza dei pazienti trattati con ep , specie nel 1 anno di follow - up , anche se , tuttavia , un certo rischio di trombosi endoluminale persiste sempre , essendosi verificata la comparsa di sottile apposizione trombotica endoprotesica in un paziente a 45 mesi di follow - up . endoleak la complicanza pi frequente ( 37 , 6% ) osservata dopo trattamento endovascolare di aaa infrarenale costituita dallendoleak ( incidenza media variabile in letteratura compresa fra 2 , 4% e 45 , 5% a seconda delle varie casistiche ) [ 9 , 37 ] , che stato definito come la comparsa di iperdensit nel materiale trombotico periprotesico alla tc in fase arteriosa e / o tardiva , espressione di persistente flusso sanguigno allinterno dellaaa , ma allesterno dellep . gli el primari ( entro 30 giorni dallimpianto ) di tipo i furono 4 / 6 ( 66 , 7% ) , il 75% dei quali scomparve dopo pta ( 2 casi ) o posizionamento di unestensione iliaca ( 1 caso )  . 
si ebbero , invece , soltanto 2 / 6 casi ( 33 , 3% ) di el secondari ( oltre 30 giorni dallimpianto ) di tipo i , confermando la necessit di uno stretto follow - up dei pazienti trattati , specie nel 1 mese dopo il posizionamento dellep , poich i difetti di adesione delle estremit dello stent - graft alle pareti vasali sono precoci a comparire . gli el di tipo ii furono i pi frequenti ( 26 / 36 el , 72 , 2% ) e il loro significato clinico rimane tuttora controverso [ 37 ]  . 
infatti , mentre un dato consolidato che gli el di tipo i e iii richiedono un trattamento obbligatorio e tempestivo in quanto associati ad un significativo aumento delle dimensioni dellaaa e , quindi , ad aumentato rischio di rottura , quelli di tipo ii costituiscono un problema di pi difficile gestione , anche perch spesso evolvono nella risoluzione spontanea . 
gli 11 casi ( 42 , 3% ) di risoluzione spontanea osservati si verificarono in un intervallo di tempo compreso fra 3 giorni e 7 mesi dalla comparsa dellel ed erano tutti el primari , ossia a comparsa precoce dallimpianto dellep . 
questo dato , perci , sembrerebbe indicare che un fattore predittivo per la trombosi spontanea dellel potrebbe essere la sua comparsa precoce nel post - impianto , e che la chiusura spontanea di un el rara dopo pi di 12 mesi dalla sua persistenza , in accordo con quanto gi descritto in letteratura [ 38 ]  . 
quanto al problema dellopportunit o meno del trattamento degli el di tipo ii , esso viene invocato solamente in caso di crescita dimensionale dellaaa , riservando un atteggiamento di sorveglianza negli altri casi [ 3942 ]  . 
noto che la presenza di el di tipo ii possa essere associata a stabilit o addirittura a riduzione volumetrica dellaaa : si verificarono , infatti , 20 casi ( 76 , 9% ) di stabilit e 2 casi ( 7 , 7% ) di riduzione significativa ( > 5 mm ) del mtr pur in presenza di el di tipo ii , a conferma che lassociazione fra crescita dellaaa e presenza di el non sempre valida per gli el di tipo ii . 
pertanto , di fronte ad un el di tipo ii , sembra essere giustificato un atteggiamento attendistico , a meno che non si associ un incremento significativo delle dimensioni dellaaa . vi furono 3 / 36 casi ( 8 , 3% ) di el di tipo iii , di cui 2 primari alla giunzione corpo - branca iliaca protesica , e 1 secondario dovuto alla rottura dello stent pi craniale a 51 c . 
consequently , in the presence of a type - 2 el , a watchful , waiting approach appears to be justified unless there is significant growth of the aaa . there were 3 / 36 cases ( 8.3% ) of type - 3 el . 
of these , two were primary , at the junction between body and iliac branch , and one was secondary due to failure of the cranial stent after 51 months ; the latter required surgical conversion and occurred with an eg model ( vanguard ) that is no longer on the market , a sign of the constant evolution of materials and devices . the only case of likely type - 4 el seen at postprocedure ct and no longer present on day 12 was probably related to graft - wall porosity ( talent ) and did not require treatment . there were no demonstrated cases of type - 5 el or endotension . 
mtr is therefore an important predictor of aaa growth , and aaa with a diameter < 50 mm are those that respond better to endovascular repair , in agreement with previous reports [ 4345 ]  . 
in fact , the three types of eg considered in the statistical analysis ( aneurx , talent and excluder ) all have a nitinol skeleton , and the talent and aneurx models , which showed a strongly significant difference in aaa shrinkage ( p = 0.0004 ) , are both covered with a dacron membrane . 
therefore , to understand such differences in aaa behaviour during follow - up , the structure of the stent - graft might be more important than the covering material . mesi di follow - up , esitato in conversione chirurgica , e associato a un modello di ep ( vanguard ) gi ritirato dal commercio , a conferma della continua evoluzione tecnica dei materiali e dei modelli di device disponibili . lunico caso di verosimile el di tipo iv osservato al controllo post - procedurale e scomparso in 12a giornata postimpianto era probabilmente legato a porosit del tessuto protesico dellep ( talent ) e non richiese alcun tipo di trattamento . 
non ci fu nessun caso dimostrabile di el di tipo v o endotension , ma si segnala un paziente portatore di un piccolo el di tipo ii da rifornimento retrogrado attraverso unarteria ipogastrica , trattato con successo mediante posizionamento di unestensione iliaca omolaterale a 12 mesi dallimpianto , che tuttavia present un ulteriore lieve incremento del mtr dellaaa ai limiti della significativit ( 5 mm ) nei controlli tc successivi , e che potrebbe essere spiegabile o con una persistenza dellel precedente ma con flusso assai ridotto ( inferiore alla soglia di sensibilit della tc ) , oppure con una pressurizzazione persistente della sacca aneurismatica ( endotension )  . analisi statistica dallanalisi statistica effettuata mediante log - rank test risultato , innanzitutto , che la crescita dimensionale dellaaa significativamente correlata con le sue dimensioni pre - procedurali ( p = 0 , 002 ) , ma non con il tipo di ep impiegato ( p = 0 , 97 )  . 
pertanto il mtr rappresenta un importante fattore predittivo per la crescita dellaaa , e gli aaa che meglio rispondono al trattamento endovascolare sono risultati quelli con diametro inferiore a 50 mm , in accordo con altri studi effettuati in letteratura [ 4345 ]  . 
resta aperta , tuttavia , la questione se trattare o meno aaa di diametro inferiore a 50 mm , poich attualmente il diametro limite per il trattamento chirurgico tradizionale degli aaa infrarenali varia proprio tra 5 , 0 e 5 , 5 cm [ 10 , 4648 ]  . lo shrinkage , invece , non sembra correlato con il diametro iniziale dellaaa ( p = 0 , 85 ) , mentre risulta significativamente correlato al tipo di stent - graft impiantato ( p = 0 , 0005 ) , in accordo con quanto descritto in letteratura , secondo cui , appunto , la riduzione volumetrica dellaaa maggiore con certi modelli di ep , in rapporto al tipo di materiale di rivestimento ( dacron o ptfe ) [ 1921 ]  . 
in realt , i 3 tipi di ep su cui stata effettuata lanalisi statistica ( aneurx , talent ed excluder ) , possiedono tutti uno scheletro in nitinol , e i modelli talent ed aneurx , fra i quali esiste una differenza marcatamente significativa di contrazione volumetrica dellaaa ( p = 0 , 0004 ) , sono entrambi rivestiti da una membrana in dacron . 
pertanto , per giustificare una tale differenza di comportamento dellaaa nel follow - up , potrebbe essere importante non tanto il materiale della membrana di rivestimento , quanto piuttosto la sua struttura , anche se questa soltanto unipotesi . conclusions despite its limitations , this study allows us to draw at least two conclusions : conclusioni da questo studio , pur con tutte le sue limitazioni , possiamo tuttavia tentare di trarre almeno 2 conclusioni : laaa e lep non sono 2 componenti separati , ma sono 2 elementi strettamente associati dal punto di vista spaziale e c . 
ct angiography is the ideal modality for the follow - up of patients after endovascular positioning of an aortobiiliac eg , as it allows accurate assessment of all morphological and functional parameters of the aaa - ep complex : the first postprocedure , ct examination , is fundamental , as it provides important quantitative data ( in particular , mtr and length of the proximal neck and aaa ) , which will serve as a reference standard for all subsequent follow - up examinations . interdipendenti da quello funzionale , e sono soggetti ad un processo di rimodellamento nel tempo anche molto significativo ; tale rimodellamento , statisticamente correlato al diametro dellaaa e al tipo di ep , interessa tanto laaa ( alterazioni dimensionali del colletto e della sacca ) quanto lep ( modificazioni di forma e dimensioni , migrazioni , rotture ) , e si pu accompagnare a conseguenze funzionali importanti ( el , trombosi endoprotesica ) che possono comportare la necessit di ulteriori procedure endovascolari e / o chirurgiche fino alla conversione laparotomica [ 49 ]  . a causa di questo processo di rimodellamento del complesso aaa - ep , e delle sue conseguenze funzionali , si rende necessario il rispetto di un rigoroso follow - up nei pazienti trattati , nel breve ma anche nel lungo termine . 
infatti alcune complicanze ( el , trombosi endoluminale ) sono pi frequenti nei primi tempi dallimpianto dellep , specie nel 1 anno , per cui questo richiede un follow - up particolarmente stretto in tale fase delicata ; tuttavia altre complicanze possono manifestarsi anche a distanza di diversi anni dallimpianto dellep , tanto da poter richiedere una conversione chirurgica tardiva . 
piga1 1medicina nucleare , policlinico universitario , universit degli studi , cagliari , italy 2unit operativa territoriale di nefrologia e dialisi , azienda usl 8 , cagliari , italy 3chirurgia generale , policlinico universitario , universit degli studi , cagliari , italy correspondence to : m . 
sixteen patients ( 11 women and five men ; age range 3580 years ) with severe hyperparathyroidism ( hp ) ( ten php , six shp ) were studied by ultrasound ( us ) , and , after i.v. 
double phase parathyroid scintigraphy identified 14 probable parathyroid glands , spect 23 ( 14 ectopic and nine eutopic ) and spect / ct confirmed all 23 probable parathyroid lesions , offering more precise localisation and an evident improvement in diagnostic accuracy . 
we believe 99mtc - sestambi spect / ct to be a more reliable presurgical method to study a patient subgroup affected by php or shp in whom conventional us and other scintigraphic methods have failed for intrinsic reasons due to the concomitant presence of multinodular goitre or ectopic parathyroid gland . 
in fact , anatomical information provided by ct enables precise localisation of the functional abnormalities highlighted by spect , and both are essential to a correct surgical approach . key words parathyroid scintigraphy spect / ct hyperparathyroidism riassunto obiettivo . 
sono stati sottoposti ad indagine spect / tc per lidentificazione e localizzazione prechirurgica delle paratiroidi 16 pazienti , 11 femmine e 5 maschi det compresa tra i 35 e 80 anni , affetti da iperparatiroidismo . 
nel raffronto tra accuratezza diagnostica delle spect e spect / tc la prima metodologia stata in grado di localizzare correttamente il 61% ( 14 / 23 ) delle formazioni patologiche mentre la spect / tc ha localizzato con precisione tutte le 23 formazioni nodulari captanti il radiofarmaco . 
si ritiene che la spect / tc rappresenti un approccio prechirurgico essenziale in tutti i pazienti affetti da iperparatiroidismo , primitivo o secondario , quando le altre metodologie tradizionali , ecografia e scintigrafia planare non possano essere dirimenti per la contemporanea presenza di gozzo multinodulare o di paratiroidi ectopiche . 
la singola metodologia spect , infatti , pur essendo in grado di identificare la ghiandola responsabile del quadro clinico risulta essere meno accurata dellindagine spect / tc nella sua precisa localizzazione e quindi meno affidabile per il chirurgo che deve pianificare lintervento . parole chiave scintigrafia parotidea spect / ct iperparatiroidismo introduction introduzione the recent introduction of hybrid scanners [ 1 ] in the field of diagnostic imaging procedures has provided a marked improvement in diagnostic methodologies compared with those offered by the use of single , uncoupled devices [ 2 ]  . 
over the last few years , clinical use of positron emission tomography computed tomography ( pet - ct ) scanners [ 4 ] has increased significantly because of its important advantages compared with pet alone in the diagnostic / prognostic evaluation of a variety of cancers in determining their real extension , response to chemotherapy and / or radiotherapy and precise delineation of target volumes to be irradiated . 
their use could be even more frequent than pet - ct for the widespread diffusion of scanners utilising gamma - emitting radiopharmaceuticals , especially if the added value of the fusion procedure in assuring clinical improvement in the interpretation of functional imaging was known [ 6 ]  . 
the aim of our study was to define the role and diagnostic accuracy of spect / ct as a methodology of choice in presurgical imaging of patients with primary ( php ) and secondary hyperparathyroidism ( shp ) with undetectable , dubious or ectopic parathyroid glands according to the recent report by gayed et al . 
in patients affected by php alone [ 7 , 21 ]  . la recente introduzione in diagnostica per immagini delle apparecchiature ibride [ 1 ] ha permesso un notevole affinamento delle metodiche diagnostiche rispetto a quelle ottenibili dalle singole macchine disaccopiate [ 2 ]  . 
in particolare ha avuto grande incremento limpiego dei tomografi pet - tc [ 4 ] di grande impatto clinico sia nella valutazione diagnostico / prognostica delle neoplasie che nel loro follow - up oltre che per la precisa delineazione dei volumi bersaglio nellapprontamento dei piani di trattamento radioterapico . 
il loro utilizzo potrebbe essere ancora pi capillare rispetto alla pet - tc , in funzione della pi estesa presenza della diagnostica medico - nucleare utilizzante radionuclidi gamma emittenti , ove fosse chiaro il valore aggiunto che tale procedura pu garantire alla diagnostica funzionale [ 6 ]  . 
lo scopo del presente studio stato quello di definire il ruolo e laccuratezza diagnostica della spect / tc come metodologia di scelta nella diagnostica pre - intervento chirurgico di pazienti affetti da iperparatiroidismo ( ip ) primitivo ( ipp ) e secondario ( ips ) con sede della lesione paratiroidea non precisata , dubbia od ectopica secondo le tecniche convenzionali in considerazione di quanto recentemente dimostrato da altri aa nellipp [ 7 , 21 ]  . materiali e metodi materials and methods between october 2004 and october 2005 , 94 patients with hyperparathyroidism ( hp ) were studied in our department . sixteen ( 11 women and five men , age range 3580 years , mean age 51 ) were selected for the study . 
 i criteri dinclusione nello studio comprendevano i seguenti requisiti : indicazione clinica alla paratiroidectomia in ip con paratiroidi ad incerta identificazione ecografica per concomitante patologia tiroidea multinodulare o in ip con ecografia negativa per ricerca di paratiroide / i in presenza di tiroide indenne o in ip con paratiroide ectopica dimostrata alla scintigrafia paratiroidea planare . diagnostic protocol esami tradizionali e spect / tc preliminarily , all patients underwent thyroid / parathyroid cdus exploration and subsequent thyroid scintigraphy after i.v. 
the ct scanner is a third - generation system with a lowpower x - ray tube and linear detector array located on the opposite side of the gamma camera slip gantry . spect acquisition parameters matrix size was 128128 over a 360 arc with a 3 step , 25 - s duration per frame and a zoom factor of 1 . 
total acquisition time was approximately 25 min . ct acquisition parameters tutti i pazienti sono stati preliminarmente sottoposti ad eco - color doppler della regione del collo ed a scintigrafia tiroidea dopo somministrazione e.v. 
lacquisizione tomografica emissiva stata eseguita dopo la prima ora dalla somministrazione con successiva rilevazione tomografica trasmissiva . acquisizione spect lindagine stata effettuata mediante impiego del sistema ibrido infinia - hawkeye ( general electric medical system , milwaukee , wi ) comprendente una gamma camera a doppia testa ed uno scanner tc . 
nellacquisizione spect sono stati adottati i seguenti i parametri : matrice dacquisizione 128128 pixel , zoom 1 , con proiezioni ottenute su campionamento angolare di 3 su 360 per un totale di 120 immagini . 
la ricostruzione delle immagini stata fatta mediante luso dalgoritmi matematici ( retroproiezione filtrata ) con filtro hann ottenendo delle sezioni secondo i tre assi dello spazio assiale , sagittale e coronale . acquisizione tc slice step was 5 mm , slice time 14 s , voltage 140 kv and current 2.5 ma , which gives a smaller patient radiation dose than conventional ct ( < 3 mgy )  . 
forty translo scanner tc un sistema di terza generazione dotato di un tubo a raggi x di bassa energia e con detettore lineare situato in situazione opposta rispetto al gantry della gamma camera . 
nella tomografia trasmissiva sono stati utilizzati i seguenti parametri : dimensione della slice di 5 mm e slice / time di 14 secondi , valori di tensione di 140 kv e valori di cor1001 a . 
total acquisition time was approximately 10 min ( table 2 )  . methodological problems the coregistration of spect / ct , particularly of the neck - thorax regions , can produce artefacts caused by possible patient movement . 
this issue must be clear to both nuclear medicine physicians and surgeons to avoid or reduce the possibility of topographic errors in parathyroid localisation . the radiation exposure caused by the coregistered spect / ct was respectively 3.3 and 3 msv ( icrp 80 , 2000 ) [ 10 ]  . 
in three patients with mng , a large calcific nodule ( 40 mm ) , as well as other nodularities , was located in the upper right thyroid lobe ( patient 1 ) and in the other two ( patients 8 and 13 ) were probable hyperplastic parathyroids . double - phase planar parathyroid scintigraphy showed 14 probable hyperfunctioning parathyroid glands , 12 in eutopic and two in ectopic sites , but these anatomic localisations were not certatwenty - three probable hyperfunctioning parathyroids were shown by spect , 14 in ectopic and nine in normotopic sites . 
la considerazione che la spect / tc della regione cervico - toracica deve essere eseguita per localizzare con precisione le paratiroidi al fine esclusivo di un intervento chirurgico pone un ulteriore problema . 
il paziente , infatti , posizionato sul tavolo chirurgico in estensione del collo tale da poter falsare i rapporti anatomici della ghiandola rispetto ai piani circostanti , ed ossei in particolare , ove anche lindagine scintigrafica non venisse condotta , nei limiti del possibile , nella medesima postura . 
tale evidenza deve essere ben chiara sia al medico nucleare sia alloperatore per minimizzare possibili misinterpretazioni topografiche . la dose di esposizione del paziente dovuta alla coregistrazione dellindagine spect / tc rispettivamente di 3 , 3 e 3 msv ( icrp 80 , 2000 ) [ 10 ]  . 
stato attuato in ogni paziente il controllo intraoperatorio dei livelli ematici di paratormone intatto ( ipth ) ed stata eseguita lindagine istologica di tutte le paratiroidi ablate . risultati lecografia rilevava la presenza di gozzo multinodulare ( gmn ) in 12 / 16 pazienti e risultava negativa negli altri 4 . 
case 1 , who underwent thyroidectomy for parathyroid carcinoma inside a calcific cyst located in the right thyroid lobe and for a concomitant follicular carcinoma in the eutopiche e 2 ectopiche , ma con insufficienti informazioni circa la loro reale posizione anatomica . la spect evidenziava la presenza di 23 sospette paratiroidi iperfunzionanti di cui 14 in sede ectopica e 9 normotopica . 
di queste va segnalata la presenza ( caso n 1 ) di una vasta area diperfissazione right parathyroid carcinoma + left thyroid follicular carcinoma hyperplastic parathyroid hyperplastic parathyroids parathyroid adenoma parathyroid adenoma parathyroid adenoma parathyroid adenoma hyperplastic parathyroids parathyroid adenoma hyperplastic parathyroids hyperplastic parathyroid hyperplastic parathyroids hyperplastic parathyroid hyperplastic parathyroid hyperplastic parathyroids hyperplastic parathyroids 1003 a . 
worthy of note is the fact that in shp patients , another five parathyroid glands negative at all scintigraphic and cdus procedures were resected . these negative parathyroid glands were virtually identical in size to those positive to spect / ct and were all located in normotopic sites . 
after parathyroidectomy , the intraoperative ipth measurements confirmed normal values in all patients . the histological report of resected lesions identified 16 hyperplastic glands , five adenomatous glands , one parathyroid carcinoma and one thyroid carcinoma ( table 3 )  . 
da segnalare lesecuzione di tiroidectomia totale ( caso n 1 ) per gmn affetto da k paratiroideo interno a cisti calcifica del lobo destro e concomitante carcinoma tiroideo 1004 a . 
2a , b paziente femmina di 60 anni affetta da iperpartiroidsmo primitivo . la spect / tc evidenzia la presenza di unarea di iperaccumulo del sestamibi situata sul mediastino antero - superiore retrostante il manubrio sternale destro . 
in patients affected by shp , sensitivity was 43% for planar scintigraphy and 64% for both spect and spect / ct . nevertheless , in comparison between diagnostic accuracy of spect and spect / ct , the first method was able to localise correctly 61% ( 14 / 23 ) of pathological lesions while spect / ct localised all 23 sestamibi - positive lesions with extreme precision . 
however , in the other spect - positive lesions , subsequent spect / ct provided surgeons with imporfollicolare del lobo sva tuttavia precisato che nei casi di pazienti affetti da ipt secondario sono state identificate ed asportate al tavolo operatorio altre 5 paratiroidi non evidenziate dalla scintigrafia perch non captanti il radioindicatore . tali ghiandole avevano di norma una dimensione sovrapponibile a quelle circostanti evidenziate sia dalla spect che dalla spect / tc ed erano tutte situate in sedi eutopiche . 
il reperto istologico delle ghiandole ablate ha permesso di identificare 16 iperplasie paratiroidee , 5 adenomi paratiroidei oltre ai citati carcinoma paratiroideo interno alla cisti calcifica e carcinoma follicolare della tiroide nello stesso paziente ( tabella 3 )  . 
tutte le altre ghiandole asportate , scintigraficamente fredde , erano paratiroidi iperplasiche . nella forme di ipt primitivo la sensibilit della scintigrafia planare nel rilevare le formazioni patologiche stata del 57% mentre la sensibilit della spect e della spect / tc stata in entrambe del 100% . 
nel raffronto tra laccuratezza diagnostica delle spect e spect / tc la prima metodologia stata in grado di localizzare correttamente il 61% ( 14 / 23 ) delle formazioni patologiche fissanti il sestamibi mentre la spect / tc ha localizzato con precisione tutte le 23 formazioni nodulari captanti . 
comunque anche per le formazioni correttamente localizzate dalla sola spect lindagine con macchina ibrida stata in grado di fornire al chirurgo pi precisi e preziosi dettagli topografici facilitanti il compito ablativo . 
ha inoltre sicuramente mutato lapproccio chirurgico nei tre pazienti con localizzazione retrotracheale . discussione nel campo della diagnostica preoperatoria del paziente affetto da iperparatiroidismo del tutto evidente che la certez1005 a . 
3a , b a 63 - year - old woman with primary hyperparathyroidism ( php ) and multinodular goitre with a large calcified cyst on the right upper lobe of the thyroid gland . 
single - photon computed tomography / computed tomography ( spect / ct ) shows an extensive area of sestamibi uptake within the cyst , which was diagnosed at histology as a parathyroid carcinoma . 
3a , b paziente femmina di 63 anni , affetta da iperparatiroidismo primario e gozzo multinodulare con voluminosa cisti a pareti calcifiche sul polo superiore del lobo destro della tiroide . 
la spect / tc dimostra la presenza di una vasta area di fissazione del sestamibi allinterno della cisti che lesame istologico ha rilevato essere un carcinoma paratiroideo . tant additional information concerning the precise localisation of lesions , thereby simplifying resection . 
this method certainly changed the surgical approach in three patients with parathyroid glands located in the retrotracheal space . discussion in the preoperative diagnosis of hp , it is evident that precise localisation of the glands responsible for the clinical picture is fundamental both for surgeon and patient . 
prior to clinical introduction of hybrid devices , the most accurate method for identifying and localising parathyroid glands was represented by pinhole spect [ 11 , 12 ]  . the recent development of new devices with the ability to acquire functional and anatomical information in a single scheduled examination has provided diagnostic imaging with a new procedure . 
in a selected group of patients in whom for intrinsic methodological causes us cannot be the main point of reference , this value has been taken on by scintigraphic methodologies . cervical - thorax planar scintigraphy has been confirmed as a suboptimal technique , with positive results in only 61% of cases and an inability to identify posterior or small - size lesions in thyroids affected by mng . spect performed in the same regions improved sensitivity of planar scintigraphy , as it was able to identify the pres1006 za di localizzazione delle paratiroidi responsabili del quadro clinico rappresenta un elemento di assoluto interesse ed importanza sia per il chirurgo sia , in ultima analisi , per il paziente . 
infatti , i precisi correlati topografici della ghiandola da ablare , facilitando il compito del chirurgo , implicano tempi pi brevi dintervento con ricadute positive sia sul paziente sia sulla gestione complessiva delle risorse . 
fino allavvento delle nuove macchine ibride , la metodologia pi accurata nellidentificare e localizzare le paratiroidi stata quella legata allimpiego del pinhole spect [ 11 , 12 ]  . la attuale procedura di fusione di immagini sta ormai identificando un nuovo settore di imaging offrendo la possibilit di potenziare , sommando , le varie tecnologie . 
nella selezionata casistica presentata e caratterizzata da pazienti nei quali lecografia non poteva rappresentare per motivi intrinseci alla metodica il punto di riferimento diagnostico principale le indagini scintigrafiche hanno assunto tale valore . 
la scintigrafia planare della regione cervico - toracica si rilevata positiva nel 61% dei casi non riuscendo ad identificare formazioni patologiche posteriori o di modeste dimensioni in un contesto tiroideo di gmn . 
solo le immagini di fusione hanno correttamente permesso di localizzare , in maniera inattesa , al suo interno la presenza della paratiroide responsabile del quadro clinico di iperparatiroidismo , peraltro , dovuto ad un a . 
spect / ct provided additional information concerning anatomical characterisation of lesions , important for surgical resection , in 39% of patients examined . the case of a patient affected by a large calcific thyroid nodule located in the upper pole of the right lobe was particularly interesting . 
in fact , abundant mitochondria - rich oxyphil cells present in thyroid oxyphil adenoma [ 13 , 14 ] or thyroid carcinoma [ 15 ] seem to assume a relevant mechanism of sestamibi uptake . 
 in our previous report , we hypothesised that in shp - positive parathyroid , scintigraphy exclusively identifies hyperfunctioning autonomous parathyroid glands refractory to vitamin d therapy and therefore the glands responsible for the so - called tertiary hp [ 16 ]  . 
subsequently , other authors confirmed this observation by demonstrating that supplementation with calcium and vitamin d in patients affected by shp inhibits parathyroid cells and , at same time , reduces sestamibi uptake by influencing the parathyroid membrane potential [ 17 , 18 ]  . 
furthermore , cell membrane expression of p - glycoprotein encoded by the human multiple drug resistant ( mdr ) gene certainly plays a relevant role in parathyroid uptake of lipophilic cationic complex [ 19 , 20 ]  . 
in conclusion , a large series of biological / molecular variable factors can influence sestamibi uptake , in particular in shp , contributing to the discussed false negative results that are , however , independent of size and site of the parathyroid glands . 
 conclusions spec / ct might currently represent the state of the art in the diagnostic flowchart to localise parathyroid glands when these are not in normotopic sites or , at any rate , undetectable at carcinoma paratiroideo . 
lo stesso caso presentava unulteriore piccolo focolaio di iperfissazione stabile del sestamibi sul polo inferiore controlaterale che allindagine istologica risultato essere un carcinoma tiroideo follicolare di 7 mm di diametro . 
tale ultima osservazione appare utile per precisare che lindagine scintigrafica con il sestamibi certamente molto sensibile nellindividuare le paratiroidi responsabili di un quadro clinico di iperparatiroidismo primitivo , ma non offre al pari unelevata specificit . 
cellularit in cui vi sia alto contenuto mitocondriale quali ladenoma a cellule ossifile [ 13 , 14 ] od i carcinomi tiroidei [ 15 ] risultano parimenti iperfissare il radiocatione . 
nei tre casi con paratiroidi ectopiche in tale sede , infatti , solo la spect / tc si dimostrata in grado di offrire un valido e risolutivo contributo preliminare allintervento chirurgico . 
certamente non rappresenta un difetto intrinseco della metodica quanto piuttosto la documentazione in immagini di un differente comportamento biologico / molecolare delle cellule paratiroidee stesse . in un precedente lavoro del nostro gruppo si prospettata lipotesi che la scintigrafia paratiroidea identifichi nellipt secondario esclusivamente quelle paratiroidi a pi elevata attivit funzionale ed autonome dallazione della terapia supplementare con vitamina d , quindi le paratiroidi responsabili dellipt terziario [ 16 ]  . 
altri autori hanno successivamente confermato tale ipotesi dimostrando che la terapia supplementare con calcio e vitamina d in grado di inibire la funzione delle cellule paratiroidee ed in concomitanza luptake del sestamibi [ 17 , 18 ]  . 
in aggiunta , lespressione a livello di membrana della p - glicoproteina codificata dal gene mdr sicuramente gioca un ruolo rilevante nella fissazione del complesso lipofilico allinterno delle cellule paratiroidee [ 19 , 20 ]  . 
in conclusione , una larga serie di variabili biologico / molecolari concorre probabilmente alla creazione di falsi negativi . certamente , comunque , non rappresentano fattori discriminanti n la dimensione delle ghiandole n la loro posizione . conclusioni la spec / tc rappresenta attualmente lo stato dellarte nella diagnostica per immagini delle paratiroidi quando esse non siano eutopiche od indocumentabili con ecografia . 
in our experience , lesion localisation improved in 39% of cases , with consequent and implicit additive value for the surgical approach . the practical result of this new method confirms its importance in surgery , as it identifies and locates parathyroid lesions not only in php , as recently reported by gayed et al . 
in this subtype of hp , despite the wellknown low sensitivity of spect / ct , it is fundamental to resect all sestamibi - positive hyperfunctioning parathyroid glands during surgical exploration and not only the larger and more conspicuous ones , which may also be negative to sestamibi . in conclusion , a wider diffusion of the spect / ct hybrid system should be encouraged given its usefulness not only in presurgical hp but also in all clinical events when the precise correlation between radionuclide signals and anatomical position is important for the correct diagnostic and therapeutic approach . za riportata la localizzazione delle lesioni migliora nel 39% dei casi con la conseguente implicita valenza positiva nei confronti dellapproccio chirurgico . 
in tali forme , infatti , nonostante il riconosciuto modesto livello si sensibilit della metodica , appare fondamentale che allatto chirurgico vengano sicuramente ablate le paratiroidi iperfissanti il radiocatione , quindi sicuramente iperfunzionanti , e non solo quelle iperplastiche , che per le loro stesse dimensioni sono facilmente reperite dal chirurgo ma che possono essere anche fredde . 
olivetti masson editore ( 2005 ) isbn 88 - 214 - 2729 - 3 published online : 11 october 2006 il nuovo libro si propone come un punto di riferimento nella diagnostica per immagini del fegato e delle vie biliari . larticolazione dei capitoli prevede infatti un progressivo passaggio delle nozioni di base per arrivare alla parte fondamentale del libro dedicata agli aspetti semeiologici delle varie patologie del fegato e delle vie biliari . a questo proposito il libro si divide in 8 parti e 25 capitoli . la prima parte dedicata allanatomia , dapprima normale , macro e microscopica , e successivamente radiologica , con particolare riferimento allecografia , alla tc e alla rm . 
una attenzione particolare viene riservata allanatomia vascolare e allanatomia segmentaria del fegato . la seconda parte dedicata alla clinica delle malattie epatiche e delle vie biliari , con una ulteriore distinzione tra le malattie epatiche focali nel paziente epatopatico e non epatopatico . la terza parte entra nel merito delle tecniche di immagine e la relativa semeiotica ed dedicata allecografia , alla tc , alla rm , alla medicina nucleare e alla colangio - pancreatografia retrograda endoscopia e rm . 
in questa parte vengono inoltre trattati i mezzi di contrasto in tc e rm . nella quarta , quinta e sesta parte viene estesamente trattata la patologia epatica e biliare , con grande ricchezza sia di informazioni sia di iconografia . nella settima parte viene trattata la radiologia interventistica del fegato con particolare riguardo alla chemioembolizzazione e alle tecniche ablative percutanee dellepatocarcinoma e delle metastasi epatiche , nonch alla tips e ai drenaggi biliari . lultima parte , infine , a testimoniare la completezza dellopera , dedicata al fegato trapiantato . il libro rappresenta un testo molto aggiornato e completo sulla diagnostica per immagini del fegato e delle vie biliari . riccardo manfredi istituto di radiologia policlinico g.b. 
passariello1 1dipartimento di scienze radiologiche , 2dipartimento di scienze cliniche , divisione di gastroenterologia , 3polo didattico pontino di latina , dipartimento di scienze radiologiche , universit di roma la sapienza , policlinico umberto i , viale regina elena 324 , i - 00166 roma , italy correspondence to : v . 
functional mri sequences acquired during the administration of oral contrast material can evaluate oesophageal transit , providing information on motility and morphology ; furthermore , this modality can properly visualise the typical functional and morphological alterations of motility disorders . key words oesophagus functional mri oesophageal motility riassunto obiettivo . 
la valutazione del transito esofageo con rm funzionale utilizzando sequenze turbo flash acquisite durante la somministrazione di mezzo di contrasto orale fattibile ed in grado di fornire informazioni valide sui dati morfologici e funzionali dell ' esofago ; inoltre , risultata essere metodica promettente nello studio delle alterazioni della funzionalit , gi oggetto di nostri altri studi . parole chiave esofago rm funzionale motilit esofagea v . 
currently , the main field of application is cardiac imaging [ 4 ] , a sector in which high - performing , state - of - the - art equipment is particularly needed . 
gastrointestinal imaging is , on the other hand , a relatively unexplored field : the study of gastrointestinal function requires levels of spatial and temporal resolution that have long remained a prerogative of videofluoroscopic techniques . 
current experience with fmri of the gastrointestinal tract is limited to some preliminary [ 57 ] and clinical studies [ 8 , 9 ] on deglutition and other more recent reports on the evaluation of gastric motility [ 10 ] ; only manabe et al . 
 [ 11 ] have investigated the use of fmri for the evaluation of oesophageal motility , introducing an optimised protocol based on t1 - weighted fast - field - echo ( ffe ) sequences . 
the aim of our study was to use fmri with t1 - weighted turbo fast low - angle shot ( flash ) sequences in the evaluation of oesophageal motility to define mri morphofunctional patterns of normality in healthy subjects and to gain preliminary experience in the study of patients with oesophageal motility disorders . materials and methods population sample thirty healthy volunteers ( 18 men and 12 women ; mean age 307 years ) with no history of oesophageal motility disorders or previous functional radiological or manometric investigation and seven patients ( three men and four women ; mean age 587 years ) with a radiological and manometric diagnosis of oesophageal motility disorder were enrolled in the study . 
subjects with general contraindications to mri were excluded ( one patient with a pacemaker and one with a metallic crystalline implant , and one healthy volunteer with claustrophobia )  . contrast material to obtain a suitable contrast agent for the examination , we tried to reproduce the physical properties of barium while ensuring that the mri signal would be good . 
we therefore tested different combinations of foods ( water , semolina and yoghurt ) mixed with gadolinium - diethylene triamine pentaacetic acid ( gd - dtpa ) 0.5 m ( 1 : 100 ) [ 8 , 9 ]  . 
although the mixture of semolina and gd - dtpa and that of yoghurt and gd - dtpa both had adequate physical properties and optimal mr signal intensity , we opted for the yoghurt - based medium because it was more palatable and easier to handle ( preparation and preservation )  . la risonanza magnetica ( rm ) funzionale ha costituito una delle principali sfide nel campo della diagnostica per immagini sin dalla seconda met degli anni ottanta [ 13 ] grazie al progressivo miglioramento in termini di risoluzione temporale e di risoluzione spaziale via via offerti dalle nuove apparecchiature . 
di contro , il campo gastroenterologico permane sostanzialmente inesplorato ; lo studio della funzionalit gastrointestinale richiede , infatti , livelli di risoluzione spazio - temporale che sono rimasti a lungo esclusiva prerogativa delle tecniche videofluoroscopiche . 
lattuale esperienza nel campo della rm funzionale del tratto gastrointestinale limitata ad alcuni studi preliminari [ 57 ] e clinici [ 8 , 9 ] sulla funzionalit della deglutizione e ad altri pi recenti articoli sulla valutazione della motilit gastrica [ 10 ] ; solo manabe et al . 
 [ 11 ] , nel 2004 , hanno proposto uno studio sullimpiego della rm funzionale nella valutazione della motilit esofagea , introducendo lottimizzazione di un protocollo basato su sequenze fast field echo t1 - pesate . 
lo scopo del nostro studio stato quello di utilizzare la rm funzionale con sequenze turbo flash t1 - pesate nella valutazione della motilit esofagea definendo dei pattern morfofunzionali rm di normalit in soggetti sani e di acquisire unesperienza nello studio di pazienti affetti da patologie della motilit esofagea . materiali e metodi popolazione campione trenta volontari sani ( 18 maschi e 12 femmine ; et media = 307 anni ) , con anamnesi negativa per la presenza di disturbi della motilit esofagea e non precedentemente sottoposti ad alcunindagine per lo studio funzionale radiologico e manometrico , e 7 pazienti ( 3 maschi e 4 femmine ; et media = 587 anni ) con diagnosi radiologica e manometrica positiva per patologia della motilit esofagea sono stati arruolati nella popolazione campione . 
sono stati esclusi dallo studio tutti i soggetti che presentavano controindicazioni generali allesecuzione di un esame rm ( 1 portatore di pace - maker ed 1 di protesi metallica del cristallino tra i soggetti patologici , un volontario sano con claustrofobia )  . mezzo di contrasto allo scopo di ottenere un mezzo di contrasto adeguato a questo tipo di esame , si cercato di emulare le propriet fisiche del bario e di ottenere , allo stesso tempo , un adeguato segnale rm . 
sono state quindi testate differenti miscele di sostanze alimentari ( acqua , semolino e yoghurt ) addizionate con gd - dtpa 0 , 5 m ( 1 : 100 ) [ 8 , 9 ]  . 
il mezzo di contrasto a base di acqua , pur presentando eccellenti caratteimaging protocol all examinations were performed on a 1.5 - t magnet ( magnetom vision , siemens , erlangen , germany ; gradients 25 mt / m2 , slew rate 800 t / m per second , rise time 400 s )  . the subjects had fasted for at least 4 h before the examination to obtain a baseline assessment of oesophageal motility . during the scan , the subjects lay prone inside the magnet with a four - channel phased - array coil positioned on their back . 
la miscela di semolino e gd - dtpa e quella di yoghurt e gd - dtpa presentavano entrambe propriet fisiche adeguate ed un ottimale intensit di segnale rm , tuttavia si optato per lutilizzo del contrasto a base di yoghurt per la miglior gradevolezza e facilit di gestione riscontrate ( modalit di preparazione e conservazione della miscela )  . protocollo di imaging tutti gli esami sono stati eseguiti utilizzando un magnete da 1 , 5 t ( magnetom vision , siemens , erlangen , germania ; gradienti 25 mt / m2 , slew rate 800 t / m / s , rise time 400 micro / s )  . 
i parametri tecnici delle sequenze dynamic tfl sono stati adeguatamente modificati in modo da ottenere una corretta visualizzazione dinamica della motilit esofagea : il numero di acquisizioni stato aumentato da 1 a 45 per ottenere un campionamento ripetuto nel tempo del lume esofageo , lo spessore della singola fetta stato aumentato a 20 mm per coprire le curvature dellesofago lungo il suo passaggio attraverso il torace e laddome . 
la quantit di contrasto somministrata per ogni sequenza dinamica non stata superiore a 1015 ml ed i soggetti sono stati istruiti ad effettuarne la deglutizione in un unico atto , sincronizzandosi con gli impulsi sonori che segnano linizio dellacquisizione di ogni sequenza . 
images show bolus progression in the oesophageal lumen in the sagittal plane 3 s ( a ) , 6 s ( b ) and 9 s ( c ) after the start of acquisition . 
le immagini dimostrano la progressione del bolo nel lume esofageo sul piano sagittale dopo 3 ( a ) , 6 ( b ) e 9 ( c ) secondi dallinizio dellacquisizione . 
si noti la continua e regolare progressione del mezzo di contrasto lungo lesofago e la completa apertura della giunzione gastroesofagea ( freccia ) al suo passaggio ( d )  . be synchronised with the sound signalling the beginning of the acquisition of each sequence . 
to formulate the normality patterns , the observers assessed healthy volunteer images for a predetermined set of morphofunctional parameters based on those commonly used in the main oesophageal motility studies , manometry and barium fluoroscopy [ 11 ]  . 
per elaborare i pattern di normalit , gli osservatori hanno valutato in tutti i volontari un insieme prestabilito di parametri morfofunzionali , con riferimento a quelli che sono i dati comunemente acquisiti con i principali esami utilizzati nello studio della motilit esofagea , ovvero la manometria e la fluoroscopia con bario [ 11 ]  . 
3a - d dynamic t1 - weighted turbo fast low - angle shot ( flash ) sequence acquired in the oblique axial plane during contrast medium transit through the gastrooesophageal junction . 
4a - d morphofunctional measurements on images obtained with dynamic t1 - weighted turbo fast low - angle shot ( flash ) sequences : oesophageal length is measured from the cricopharyngeal sphincter to the gastrooesophageal junction ( goj ) using images showing a completely opacified lumen ( a , line ) ; calibre is measured on the anteroposterior diameter of the oesophagus ( b , arrows ) ; transit time is calculated from the first appearance of the bolus in the lumen to when it reaches and crosses the goj . 
4a - d misurazioni morfofunzionali su immagini ottenute con sequenze dynamic turbo - flash t1 pesate : la lunghezza dellesofago misurata dallo sfintere cricofaringeo alla giunzione gastroesofagea impiegando le immagini in cui il lume risulta completamente opacizzato ( a , linea ) ; il calibro viene valutato misurando il diametro antero - posteriore dellesofago ( b , frecce ) ; il tempo di transito calcolato dal momento iniziale in cui il mezzo di contrasto appare nel lume al momento in cui raggiunge ed oltrepassa la giunzione gastroesofagea . 
i pattern di normalit ottenuti dagli esami effettuati nei volontari sani sono stati successivamente utilizzati come parametro di confronto nei pazienti con alterazioni della motilit esofagea ; in questultimo gruppo di pazienti la diagnosi rm stata raggiunta in consenso con quella radiologica e manometrica , permettendo una preliminare valutazione della validit diagnostica della metodica che sar oggetto di studi futuri . results the fmri study of oesophageal morphology and function with dynamic tfl sequences was possible in all subjects , providing satisfactory image quality . 
la durata media dellesame stata di 155 mil tratto di esofago compreso tra lo sfintere cricofaringeo e la gge stato correttamente visualizzato in tutti i soggetti . pattern di normalit i parametri morfologici sono stati correttamente valutati grazie alladeguata risoluzione spaziale della sequenza utilizzata ; per ogni parametro stato calcolato il valore medio ( m ) e la deviazione standard ( ds ) : lunghezza dellesofago : m = 22 , 8 cm , ds = 2 , 7 cm ; calibro dellesofago : m = 21 mm , ds = 1 , 8 mm . la risoluzione temporale ottenibile attraverso i valori di tr , te e flip angle impiegati stata di circa 2 , 5 frames per secondo . 
none of the patients with a diagnosis of oesophageal motility disorder had mri findings referable to hiatal hernia or gastrooesophageal reflux . discussion the study of oesophageal morphology and motility currently relies on a combined radiological and manometric saggio del bolo . alterazioni della motilit nei pazienti con diagnosi di alterazione della motilit esofagea stato possibile evidenziare reperti patologici corrispondenti a quelli riscontrati allesame videofluoroscopico convenzionale : la rm ha potuto correttamente diagnosticare 3 casi di acalasia ( di cui uno in fase precoce e due in fase avanzata ) e 4 casi di spasmo esofageo diffuso . 
limmagine a 4 secondi ( a ) evidenzia un rapido riempimento del lume esofageo ; il normale transito del mezzo di contrasto tuttavia interrotto da contrazioni terziarie intermittenti ( b ) che ne ostacolano la progressione , creando un tipico aspetto a cavaturaccioli ( freccia nellingrandimento )  . esofagea si sono evidenziate immagini riferibili ad ernia iatale n a reflusso gastroesofageo . discussione attualmente lo studio della morfologia e della motilit esofagea si basa su un approccio combinato radiologico e manometrico : se infatti lo studio della morfologia e delle sue variazioni durante gli eventi fisiologici stretta pertinenza della fluoroscopia con bario [ 12 , 13 ] , lanalisi dettagliata della motilit viene effettuata attraverso limpiego della manometria , metodica strumentale in grado di misurare con estrema precisione parametri difficilmente valutabili con tecniche differenti , quali lintensit della singola onda peristaltica o la pressione di apertura dello sfintere esofageo inferiore [ 14 , 15 ]  . 
tecniche alternative di studio funzionale , quale la valutazione con radionuclidi del transito esofageo , sono state proposte con discreto successo [ 16 ] ; tuttavia non esiste ad oggi alcuna metodica di imaging alternativa che risulti sufficientemente affidabile rispetto allapproccio radiologico tradizionale . 
il protocollo da noi proposto introduce una tecnica rm in grado di offrire unadeguata risoluzione spazio - temporale nella visualizzazione degli eventi fisiologici che si producono durante la peristalsi esofagea . 
la sequenza dynamic tfl impiegata nel nostro protocollo soddisfa in maniera soddisfacente i requisiti tecnici necessari ad un esame dinamico : i bassi valori di flip angle ( 8 ) e di tr ( 416 ms ) utilizzati in combinazione con il mezzo di contrasto orale a base di gd - dtpa , permettono la visualizzazione in tempo reale della motilit esofagea con unadeguata risoluzione di contrasto a livello del lume . 
i risultati ottenuti con la metodica hanno permesso la formulazione di pattern morfofunzionali rm di normalit in accordo con i reperti manometrici e radiologici riscontrati in letteratura [ 17 , 18 ] in soggetti sani ; lutilizzo dei pattern di normalit come parametro comparativo costituisce , inoltre , presupposto fondafig . 
whereas oesophageal morphology and its changes during physiological events is studied with the barium swallow [ 12 , 13 ] , motility is investigated by manometry , a technique able to provide precise measurements of parameters not assessable with other methods , such as intensity of the single peristaltic wave or the opening pressure of the lower oesophageal sphincter [ 14 , 15 ]  . alternative techniques proposed for functional studies , such as radionuclide assessment of oesophageal transit , have met with moderate success [ 16 ] ; nonetheless , no alternative imaging method has proved sufficiently reliable compared with conventional radiology . 
the protocol proposed by us introduces an mri technique able to offer adequate spatial and temporal resolution in visualising physiological events occurring during oesophageal peristalsis . the dynamic tfl sequence adequately fulfils the technical requirements of a dynamic study : the low flip angle ( 8 ) and tr ( 416 ms ) values used in combination with oral gddtpa - based contrast material allows real - time visualisation of oesophageal motility with adequate contrast resolution in the lumen . 
in these subjects , mri proved able to identify morphofunctional alterations typical of the conditions being studied , in agreement with findings of conventional videofluoroscopy . compared with conventional radiology , fmri of the oesophagus has several major advantages : multiplanar imaging capabilities with visualisation of the oesophagus and intrathoracic soft tissues in the different spatial planes , the possibility of making acquisitions with dedicated sequences and possible use of contrast material targeted to specific diagnostic queries and higher contrast resolution . 
with fmri , it would be possible to repeat examinations over time ( for example , in the follow - up before and after dilatation and / or myotomy in patients with achalasia ) and to study patients , such as pregnant women and younger subjects , in whom radiation exposure is contraindicated . the technique presented does , however , suffer some limitations : first , the spatial resolution of the sequences used , although adequate for assessing oesophageal function , is still too low to study alterations of the wall profile , as can be done with videofluoroscopy ; we should , however , add that the typical filling defect pattern ( as seen in one case of leiomyoma of the distal third ) and / or marked wall thickening at the level of the goj ( as in the case of cardia cancer ) could raise the suspicion of pseudoachalasia . 
second , the maximum temporal resolution [ 2.5 frames per second ( fps ) ] is still far below the standards currently obtainable with conventional radiology ( 2530 fps )  . 
a further technical limitation might be the possibility of imaging patients in the clinostatic position only , especially if we consider the range of positions and projections used in videofluoroscopy and manometry ; however , in the light of the results of our preliminary experience we can state that even the information obtained with the patients in the clinostatic position may be valuable for diagnosis . 
our next study , which is being conducted on patients with motility disorders , already involves double acquisitions with patients in the prone and supine position . mentale per la valutazione diagnostica dei pazienti con alterazioni della motilit . 
 rispetto allapproccio radiologico tradizionale , lesame rm funzionale dellesofago presenta alcuni importanti vantaggi : capacit di imaging multiplanare con visualizzazione dellesofago e dei tessuti molli endotoracici sui diversi piani dello spazio , possibilit di effettuare acquisizioni con sequenze dedicate ed eventuale impiego del mezzo di contrasto sulla base di precise richieste diagnostiche , superiore risoluzione di contrasto . 
il vantaggio maggiore tuttavia rappresentato dalla possibilit di esplorare la funzionalit dellesofago senza limpiego di radiazioni ionizzanti : lesposizione alle radiazioni [ 19 ] rimane ad oggi , nonostante lavvento delle apparecchiature digitali e la sensibile riduzione della dose di esposizione , la principale controindicazione allesame fluoroscopico ; al contrario , la rm funzionale potrebbe consentire esami ripetibili nel tempo ( richiesti ad esempio nei programmi di follow - up pre e post dilatazione e / o miotomia nei pazienti acalasici ) , permettendo inoltre lo studio di quei pazienti nei quali lesposizione alle radiazioni sconsigliata , quali le donne in gravidanza ed i soggetti pi giovani . 
 la tecnica da noi presentata non tuttavia priva di limiti : in primo luogo la risoluzione spaziale delle sequenze impiegate , seppur adeguata per la valutazione della funzionalit esofagea , risulta ancora troppo bassa per lo studio delle alterazioni del profilo della parete esofagea cosi come ottenibile con la videofluoroscopia ; bisogna , tuttavia , aggiungere che il tipico aspetto da difetto di riempimento ( come ad esempio riscontrabile in un caso di leiomioma del terzo distale ) e / o un evidente ispessimento parietale a livello della giunzione gastro - esofagea ( come nel caso di un tumore del cardias ) potrebbero porre il sospetto per pseudoacalasia . 
potrebbe risultare tecnicamente opinabile la possibilit di eseguire gli esami nel solo clinostatismo soprattutto considerando le differenti posizioni e proiezioni utilizzate negli studi videofluoroscopico e manometrico ; alla luce dei risultati acquisiti nella nostra esperienza preliminare possiamo ritenere , tuttavia , che anche le informazioni ottenute in posizione clinostatica possano comunque risultare valide ai fini diagnostici . 
lesperienza successiva gi in corso su una popolazione di pazienti patologici , gi prevede la duplice acquisizione in posizione prona e supina . conclusioni conclusions our study demonstrated that the evaluation of oesophageal transit with fmri using tfl sequences during the administration of oral contrast material is feasible and able to provide valuable morphological and functional information on the oesophagus ; in addition , this method is able to correctly identify alterations of oesophageal function and morphology in subjects with motility disorders . in conclusione il nostro studio dimostra che la valutazione del transito esofageo con rm funzionale utilizzando sequenze turbo flash acquisite durante la somministrazione di mezzo di contrasto orale fattibile ed in grado di fornire informazioni valide sui dati morfologici e funzionali dellesofago ; inoltre , questa metodica in grado di evidenziare correttamente le alterazioni della funzionalit e della morfologia esofagea presenti in soggetti affetti da disordini della motilit . 
even though the technique , above all in terms of performance of the equipment , is still far from being state - of - the - art and suffers some significant technical limitations , we believe this diagnostic approach to be feasible and to hold significant future prospects for the study of subjects with oesophageal disorders , whom we are currently studying with state - of - the - art equipment . rm funzionale risultato rapido , facilmente riproducibile , del tutto non invasivo e privo di disagio per il paziente . 
magnavita2 1istituto nazionale di riposo e cura dellanziano ( inrca ) , sede di roma , via cassia 1167 , i - 00189 roma , italy 2istituto di medicina del lavoro delluniversit cattolica del sacro cuore , roma , italy correspondence to : a . 
lastly , radiologists were frequently named as one of multiple defendants , together with medical ( or surgical ) doctors , in cases of patient death in roughly 6% of all cases . 
strict adherence to radiological standards may be a means of reducing the risk of legal action and obviating litigation . key words malpractice radiology liability error clinical risk management riassunto obiettivo . 
in altri termini , il 44% della coorte , rappresentativa dei radiologi italiani , ha ricevuto o ricever una citazione in giudizio riferita alla propria attivit professionale degli ultimi 10 anni . 
a questo riguardo la prima causa di errore in ordine di frequenza ancora la mancata diagnosi di lesioni dello scheletro immediatamente seguita , in ordine di frequenza , dalla mancata diagnosi di neoplasia , soprattutto della mammella . 
magnavita : a 12 - year follow - up study of malpractice claims against radiologists in italy introduction introduzione legal action taken against physicians for presumed malpractice is an increasing problem in all countries and in all specialties . 
radiological malpractice in italy has recently been the subject of a number of papers , including qualitative investigations in mammography [ 1 ] , methodological proposals [ 2 ] , and the presentation of case series [ 3 ]  . there is therefore the need to analyse the epidemiology of the phenomenon , which would also help to identify the most effective measures in terms of clinical risk management . this is the aim of the present study , which is based on the examination of a cohort of more than 4 , 000 radiologists accounting for over half of the members of the italian society of medical radiology ( sirm ) and who were studied over a period of 12 years . le denunce contro i medici per presunta malapratica ( malpractice nella letteratura anglosassone ) sono un problema di crescente gravit in tutti i paesi e in tutte le specialit . 
al tema della malapratica radiologica nel nostro paese sono state recentemente dedicate verifiche qualitative nel settore mammografico [ 1 ] e proposte metodologiche [ 2 ] , oltre naturalmente a segnalazioni casistiche [ 3 ]  . 
la popolazione di riferimento , costituita da tutti i radiologi che hanno stipulato lassicurazione , sensibilmente aumentata nel periodo di osservazione ( da 1400 iscritti nel 1993 a 4007 al 1 / 1 / 04 con incremento del 286% )  . 
essa si riferisce attualmente al 53% dei radiologi iscritti alla sirm e pu essere quindi ritenuta sufficientemente rappresentativa dellinsieme dei radiologi italiani ( tabella 1 )  . le denunce sono state classificate in ragione della causa che le aveva prodotte , come : ( 1 ) da presunto errore diagnostico ; ( 2 ) da presunto errore nella conduzione dellesame ; ( 3 ) da omissione di indicazioni diagnostiche e / o terapeutiche ; ( 4 ) da terapie con radiazioni ionizzanti e / o non ionizzanti ; ( 5 ) da responsabilit civile per infortuni subiti dal paziente durante lesecuzione dellesame ( per urti , cadute ecc . ) ; ( 6 ) da applicazione dellart . 
in questultima categoria sono stati compresi anche tutti i casi nei quali il radiologo non ha specificato la causa della denuncia , riservandosi di farlo in un secondo tempo ; nei casi in cui entro il 31 / 12 / 2005 stato possibile conoscere le specificazioni di tipologia e sede del sinistro si provveduto a correggere la relativa classificazione . i dati sono stati analizzati mediante statistiche descrittive , utilizzando lo statistical package for social sciences ( spss / pc 11 , 5 )  . per ottenere la stima delle denunce riferibili al periodo in esame , ma che perverranno allente assicuratore entro i termini di prescrizione delle denunce di responsabilit civile ( dieci anni dallevento lesivo ) , si proceduto nel modo seguente : ( 1 ) stata formulata lipotesi che la propensione a a . 
magnavita : a 12 - year follow - up study of malpractice claims against radiologists in italy materials and methods all malpractice claims regarding the professional activity of radiologists received by the insurance company from 1 january 1993 ( the beginning of the convention with sirm ) to 31 december 2004 were examined . 
the study population , made up of all sirm radiologists insured with the company , noticeably increased over the study period ( from 1 , 400 members in 1993 to 4 , 007 on 1 january 2004 , an increase of 286% )  . 
the population currently accounts for 53% of sirm members and can therefore be considered a sufficiently representative sample of all italian radiologists ( table 1 )  . claims were classified according to the cause that produced them , such as : ( 1 ) presumed diagnostic error ; ( 2 ) presumed error in performing the examination ; ( 3 ) failure to provide diagnostic and / or therapeutic indications ; ( 4 ) treatment with ionising and / or nonionising radiation ; ( 5 ) civil liability due to accidents suffered by the patient during the examination ( slip - and - fall accidents , etc . ) ; and ( 6 ) application of articles 589 of the italian penal code ( manslaughter ) and 590 ( culpable lesions ) and other articles of the penal or civil codes . 
the last of these categories also includes all of those cases in which the radiologist fails to specify the cause of the claim , deciding to do so at a later time ; cases in which the cause of the claim could be verified by 31 december 2005 were reclassified accordingly . 
in other words , since only 22% of claims relating to the 19931995 period were filed within 1 year of the event , we estimated that the claims filed in 2004 made up only 22% of all claims referring to 2004 , which will be filed within the prescribed ( 10 - year ) time period . 
in a similar way , we performed calculations for 2003 , 2002 , and so on , until 1995 . using similar reasoning , we estimated the cause of claims yet to be filed by examining frequency according to cause of claims filed at least 1 year after the alleged harmful event and applying those percentages to the number of claims expected to be filed . results in the study period , radiologists covered by insurance policies received 990 claims for alleged malpractice . 
the claims prevalently concerned radiologists working in the public hospital system ( 714 cases ; 72.1% ) whereas radiologists working in private facilities were subject to about a quarter of all denunciare i medici radiologi sia costante nel tempo ; ( 2 ) di conseguenza , stato assunto che landamento delle denunce nei primi anni di osservazione , tra il 1993 ed il 1995 , una volta esaurito leffetto delle denunce tardive , esprima landamento costante delle denunce nella coorte ; ( 3 ) stata calcolata la percentuale cumulativa delle denunce pervenute dopo uno , due , tre o pi anni nel periodo di osservazione anteriore al 1995 ; ( 4 ) tali percentuali cumulative sono state applicate come coefficienti alle osservazioni attuali . 
in altri termini , poich nel periodo 19931995 solo il 22% delle denunce pervenuta entro lanno di accadimento , si stimato che le denunce pervenute nel 2004 siano solo il 22% di quello che sar il numero totale di denunce riferibili al 2004 che perverranno entro i termini di prescrizione . 
in modo analogo si proceduto per gli anni 2003 , 2002 e precedenti , fino al 1995 . con lo stesso procedimento logico si proceduto a stimare la causa delle denunce non ancora pervenute , esaminando la frequenza per causa delle denunce pervenute dopo almeno un anno dallevento lesivo ed applicando tali percentuali agli eventi attesi . risultati nel periodo esaminato i medici radiologi coperti da polizze assicurative hanno ricevuto 990 denunce per presunta responsabilit civile . 
le denunce hanno riguardato prevalentemente medici operanti nelle strutture pubbliche ( 714 casi , 72 , 1% ) , mentre i radiologi che lavorano in strutture private hanno subito circa un quarto delle denunce ( 244 casi , 24 , 6% )  . 
i danni allegati consistevano prevalentemente in lesioni personali ( 661 casi , 66 , 8% ) , ma significativamente elevata la quota di decessi ( 329 casi , 33 , 2% )  . 
il numero pi elevato di denunce perviene dopo un anno dallevento lesivo ( 311 denunce , 31 , 4% ) , mentre quasi met perviene negli anni ancora successivi , in alcuni casi anche dopo oltre otto anni ( tabella 4 )  . lanalisi delle cause delle denunce ( tabella 5 ) consente di osservare che nella maggior parte dei casi ( 660 casi , 66 , 7% ) limputazione di errata diagnosi , in quanto si ipotizza incapacit o negligenza del radiologo nellinterpretazione dellesame radiologico . 
il presunto errore diagnostico del radiologo non solo la principale causa di contenzioso , ma anche quella che registra il maggior incremento percentuale rispetto allanalisi dei primi dati italiani da noi analiz1011 a . 
alleged diagnostic error is not only the main cause of legal action but also registers the greatest percentage increase with respect to the zati , quando tale categoria rappresentava un terzo delle denunce [ 4 ]  . 
va considerato inoltre che ad un presunto errore diagnostico del radiologo si riferiscono molte delle denunce provvisoriamente classificate nella categoria miscellanea , nelle quali spesso il radiologo viene citato per omicidio colposo o lesioni assieme a tutti gli altri medici che hanno avuto a che fare con il paziente , sulla base di presunta imperizia o negligenza nellesecuzione degli accertamenti radiologici ( tabella 5 )  . la sede pi frequente degli errori diagnostici lapparato scheletrico ( 44 , 5% ) ; seguono in ordine di frequenza la mammella ( 25 , 9% ) , il torace ( 11 , 4% ) , laddome ( 8 , 3% ) ( tabella 6 )  . 
tra le cause di errore , si conferma al primo posto la mancata o errata diagnosi di lesioni dellapparato osteoarticolare ( 279 casi ) , ma le denunce per mancata o ritardata diagnosi delle neoplasie ( 265 casi ) risultano ormai quasi altrettanto numerose , e laumento rispetto alle precedenti rilevazioni fa ritenere che in un prossimo futuro lordine abbia ad invertirsi . 
nellambito delle neoplasie , gli errori riguardano in primo luogo la mammella ( 171 casi , pari al 64% di tutte le neoplasie ) e , in minor misura , tumori polmonari o di altre sedi ( tabella 7 )  . 
le denunce per neoplasie mammaria registrano anche il maggiore incremento nume1012 percentuale cumulativa 23 , 3 54 , 7 71 , 9 85 , 6 93 , 2 98 , 0 99 , 3 99 , 8 100 , 0 percentuale totale a . 
it should also be borne in mind that alleged misdiagnosis accounts for many of claims provisionally classified in the miscellaneous category , in which legal action is often taken against the radiologist , along with all other physicians who came into contact with the patient , for manslaughter or culpable lesions on the basis of alleged inability or negligence in interpreting radiological findings ( table 5 )  . 
 the most common site of diagnostic errors was the skeletal system ( 44.5% ) , followed by the breast ( 25.8% ) , the chest ( 11.4% ) and the abdomen ( 8.3% ) ( table 6 )  . 
once again , the most common cause of error was misdiagnosis or failure to diagnose lesions to the osteoarticular system ( 279 cases )  . however , the number of claims made for misdiagnosis or failure to diagnose cancer ( 265 cases ) has almost reached the same level . 
with regard to cancer , the most common site of claims was the breast ( 171 cases , or 64% of all cancers ) followed to rico dalle prime osservazioni da noi condotte [ 4 ] , quando erano stati denunciati solo due casi . 
gli errori nelle tecniche e procedure radiologiche rappresentano percentualmente solo il 10 , 3% delle denunce ( 112 casi ) , circa la met dei quali ( 59 casi ) da attribuirsi a tecniche di radiologia interventistica . la latenza tra evento lesivo e denuncia varia nei diversi gruppi di eventi causali ( tabella 8 )  . 
mentre le lesioni conseguenti a presunti errori di tecnica o infortuni occorsi nella sala radiologica danno luogo a denuncia spesso entro lo stesso anno di accadimento e comunque entro il secondo anno solare dallevento , i procedimenti per malapratica si attivano a distanza maggiore dallevento . 
errors in radiological techniques and procedures accounted for only 10.3% of claims ( 112 cases ) , almost half of which ( 59 cases ) involved interventional radiological techniques . latency between the alleged error event and the filed claim varies according to cause ( table 8 )  . 
whereas lesions due to alleged technical errors or accidents in the radiology room are often associated with claims filed in the same year or at least within the second calendar year from the alleged event , malpractice claims tend to be filed at a greater distance from the alleged event . 
in particular , claims for failure per ottenere una stima del numero di denunce che si riferiranno a tutti gli eventi radiologici occorsi nel periodo di osservazione , possiamo tenere conto dellandamento dei tempi di latenza relativi agli anni pi lontani , anteriori al 1995 , per i quali si pu ormai ritenere estinto il diritto al risarcimento civile ( dieci anni )  . 
lesame di questi dati rafforza quanto sopra affermato circa la maggiore latenza delle denunce per neoplasia , che negli eventi pi remoti , sono di circa quattro anni ( tabella 9 )  . 
tenendo conto della latenza delle denunce , e facendo lipotesi che la propensione a denunciare i radiologi sia costante negli anni a venire , si pu stimare che verranno sporte almeno 1370 denunce per eventi riferiti ai dodici anni di osservazione , con un incremento del 38% ( 380 casi ) rispetto alle 990 denunce sinora perve1014 a . 
the significant latency of claims complicates assessment of the phenomenon overall and makes assessment of the incidence of risk particularly difficult since the number of claims in the study period is still incomplete . to obtain an estimate of the number of future claims relating to all radiological events that occurred during the study period , we examined the trend of latency times with regard to the earliest years of the study period ( prior to 1995 ) for which the right to civil compensation has expired ( 10 years )  . 
analysis of these data reinforces the observation that claims regarding cancer have a greater latency , which in some cases extends to around 4 years ( table 9 )  . 
il metodo di stima da noi applicato ci induce a ritenere che le denunce per errata diagnosi di neoplasia rappresenteranno la principale causa di contenzioso , una volta esaurita la latenza dei tempi di denuncia ( tabella 11 )  . sempre sulla base dellipotesi che la propensione a denunciare i radiologi si mantenga costante , il rischio di denuncia risulta superiore al 44 per mille ( tabella 10 )  . 
ci corrisponde al rischio di una denuncia ogni 22 , 7 anni di lavoro , ovvero , in altri termini , alla certezza statistica , per il radiologo medio , di essere denunciato almeno una volta nel corso della propria vita lavorativa . 
magnavita : a 12 - year follow - up study of malpractice claims against radiologists in italy verse analisi della coorte da noi effettuate in anni precedenti induce a ritenere che la propensione a denunciare i radiologi nel nostro paese sia in aumento . stant in the future , we estimated that at least 1 , 370 claims will be lodged for events occurring in the 12 - year study period , with an increase of 38% ( 380 cases ) compared with the 990 claims lodged to date ( table 10 )  . 
the method of estimation we employed suggests that claims for cancer misdiagnosis is the main cause of legal action once the latency cut - off period for claims has been reached ( table 11 )  . while maintaining the hypothesis that the tendency for legal action against radiologist remains constant , the risk of being sued is greater than 44 per 1 , 000 subjects ( table 10 )  . this figure corresponds to a risk of being sued every 22.7 working years or , in other words , statistical certainty that the average radiologist will be sued at least once in his or her working life . 
this estimate is once again higher than the values we calculated in this cohort in previous studies [ 47 ]  . progressive increase in the rate of claims lodged in the various analyses of the cohort we carried out in previous years suggests that the tendency to take legal action against radiologists in italy is increasing . discussion the most significant finding of our study was the high risk of being sued for malpractice . 
our estimate , which is based on the conservative hypothesis that there is no increase in the tendency of patients to sue physicians and therefore probably underestimates the phenomenon , suggests that half of the radiologists in our cohort have received or will receive a request for compensation or be taken to court in relation to the previous 10 years of their professional activity . 
in one third of cases , claims pertain to events in which the patient died , thus involving requests for very high amounts of compensation and possible severe criminal proceedings . further analysis suggests that the risk of legal complications for italian radiologists is progressively approaching that of the united states where it is estimated that 40% of radiologists are taken to court on average once every 5 years [ 8 ]  . 
in the united states , malpractice suits filed against radiologists account for 10%15% of the total charges against physicians for inability or negligence even though in the united states radiologists overall are less exposed to the risk of legal action than are surgeons but much more exposed than are internists and specialists [ 9 ]  . even though not all legal action ends with the physician being sentenced since in most cases there is insufficient evidence to convict the radiologist and an out - of - court settlement is reached the burden of worry , legal expense and time that each case inevitably causes the radiologist should be borne in mind . 
in a significant number of cases , the stress connected to legal action can cause alterations of a physical , psychological and behavioural nature [ 10 ] , prompting the radiologist to adopt a defensive attitude ( so - called defensive medicine ) [ 11 ] or an aggressive defensive approach [ 12 ]  . these are situations that were practically unknown to the preceding generation of radiologists and that have suddenly become inevitable and innate to our professional activity . an epidemiological analysis of malpractice suits filed discussione il dato di maggiore rilievo nella nostra indagine lelevato rischio di essere denunciati per malapratica . 
la nostra stima , che basata sullipotesi prudenziale che non ci sia un aumento della tendenza a denunciare i medici da parte dei pazienti e che pertanto verosimilmente sottostima il fenomeno , induce a ritenere che la met dei radiologi della nostra coorte abbia ricevuto o stia per ricevere una richiesta di risarcimento o una citazione penale relativa allattivit professionale svolta nellultimo decennio . 
in un terzo dei casi le denunce si riferiscono ad eventi nei quali si verificato il decesso del paziente ; ci determina richieste di risarcimento di importo molto elevato e possibili pesanti ripercussioni penale nostre successive analisi della coorte di radiologi italiani assicurati ci inducono a ritenere che il rischio di complicazioni giudiziarie per i radiologi italiani tenda progressivamente ad avvicinarsi a quello degli stati uniti dove si stima che il 40% dei radiologi sia citato in giudizio mediamente una volta ogni 5 anni [ 8 ]  . 
sempre negli usa le denunce contro i radiologi rappresentano il 10%15% del totale delle denunce contro i medici per imperizia o negligenza anche se , in quel paese , i radiologi risultano nel complesso meno esposti al rischio di citazioni rispetto ai chirurghi , ma molto pi esposti dei medici internisti e specialisti [ 9 ]  . anche se non tutte le denunce si concludono con la condanna del medico , in quanto nella maggior parte dei casi possibile raggiungere un accordo extragiudiziale , ovvero non risultano sussistere elementi di colpa da parte del sanitario , occorre considerare il carico di preoccupazioni , spese legali e tempo che ciascuna di queste denunce inevitabilmente comporta per il medico radiologo . 
in non pochi casi lo stress connesso con la denuncia pu determinare alterazioni sul piano fisico , psicologico e comportamentale [ 10 ] , inducendo nel radiologo atteggiamenti di difesa ( la cosiddetta medicina difensiva ) [ 11 ] o attivi ( di difesa aggressiva ) [ 12 ]  . 
si tratta , in ogni caso , di esperienze quasi sconosciute ai colleghi della generazione che ci ha preceduto , ed improvvisamente diventate inevitabili e connaturate allattivit professionale . lanalisi epidemiologica delle denunce sporte contro i radiologi italiani consente di individuare , accanto ad aspetti analoghi a quelli gi segnalati nei paesi anglosassoni , alcune peculiarit strettamente legate al nostro sistema giuridico e sociale . 
tra gli aspetti di analogia con le esperienze dei colleghi statunitensi possiamo annoverare la prevalenza delle denunce per errori diagnostici e , allinterno di questi , il sempre maggiore peso delle denunce per mancata identificazione di neoplasie . 
magnavita : a 12 - year follow - up study of malpractice claims against radiologists in italy against italian radiologists enables identification of a number of features unique to the italian legal and social system , as well as others similar to those already reported in englishspeaking countries . 
in contrast , the high latency period of claims is atypical and can only be partly explained by the time required to gather the medical documentation required for formulating a malpractice suit . in more than two thirds of cases , legal action is taken against the radiologist due to incorrect diagnosis . 
this trend is in line with the tendency already noted in series in the united states [ 8 , 1315 ]  . errors are inevitably linked to radiological and medical practice in general , just as they are to all other human activities . 
there is , however , a need to question the possible causes of errors in order to formulate the most appropriate preventive measures ( clinical risk management ) [ 16 , 17 ]  . 
since the relationship between errors and claims is not biunique in that there can be errors not followed by legal action and legal action not substantiated by errors , there is also the need to question the factors that promote legal action . one of the main causes of diagnostic errors in radiology is undoubtedly the increase in the number of examinations . 
in the united states , it has been estimated that the number of examinations and images produced has increased by 40% in the last 5 years , and a further increase of 28% is expected by 2008 [ 18 ]  . 
review studies show that the performance of radiologists ( reduction of false negatives and false positives ) is correlated neither with the increase in the number of examinations interpreted nor the level of professional experience [ 19 ]  . 
it is therefore likely that an increase in the number of examinations interpreted , without a similar increase in the time available for their interpretation , produces a reduction in performance . 
in contrast , it has been shown that when double reading is possible , for example for mammograms , the number of errors can be reduced [ 2022 ]  . the risk of legal action due to delayed diagnosis is also associated with the spread of screening programmes , such as those for breast cancer [ 23 , 24 ] , in which the retrospective diagnosis of disease on previous radiographs is often possible or suspected . 
this tends to falsely undervalue the difficulty of reaching the correct diagnosis at the time of the first examination . the group of alleged misdiagnosis includes most of the claims originating from manslaughter and serious bodily injury charges . 
in these cases , the radiologist is invariably involved due to objective responsibility with all the other physicians who came into contact with the patient in very 1018 in oltre due terzi dei casi il radiologo citato per errore di diagnosi . 
tra questi errori , lomessa diagnosi di neoplasia si appresta a divenire anche nel nostro paese la prima causa di denuncia , seguita dallomessa diagnosi di fratture , secondo la tendenza gi osservata nelle serie storiche negli stati uniti [ 8 , 1315 ]  . lerrore inevitabilmente legato alla pratica radiologica e medica in generale , cos come ad ogni altra attivit umana . 
poich tra errori e denunce la relazione non biunivoca , in quanto possono esservi sia errori non seguiti da denunce che denunce non sostanziate da errori , occorre anche interrogarsi sui motivi che favoriscono le denunce contro i medici . tra le cause degli errori diagnostici in radiologia , una delle principali senza dubbio laumento del numero degli esami . 
negli stati uniti si stima che il numero delle indagini e delle immagini prodotte sia aumentato del 40% negli ultimi 5 anni , ed un ulteriore aumento del 28% atteso per il 2008 [ 18 ]  . 
in italia non vi sono dati di questo genere , ma riteniamo che la tendenza sia similare . lincremento di produttivit richiesto in questi ultimi anni ai servizi di radiologia ha senzaltro ridotto il tempo che il radiologo pu dedicare sia al colloquio con il paziente sia alla refertazione e questo fatto , associato al ridotto tempo da dedicare allaggiornamento professionale , pu giustificare laumento del numero degli errori . 
studi di revisione dimostrano che la performance del radiologo ( riduzione dei falsi positivi e dei falsi negativi ) non correlata n con lincremento del numero di esami refertati , n con lesperienza professionale [ 19 ]  . 
al contrario , stato dimostrato che , laddove sia possibile una doppia lettura , come ad esempio per gli esami mammografici , possibile ridurre il numero di errori [ 2022 ]  . il rischio di denunce per ritardata diagnosi inoltre associato al diffondersi dei controlli sanitari periodici a fini preventivi quali quelli per il tumore della mammella [ 23 , 24 ] nei quali la diagnosi retrospettiva di malattia su radiogrammi precedenti spesso possibile o sospettabile , e questo porta falsamente a sottostimare la difficolt di porre la diagnosi corretta allepoca del primo esame . tra gli errori diagnostici presunti rientrano la maggior parte delle denunce originate da avvisi di garanzia per omicidio o lesioni colpose . 
in questi casi il radiologo viene invariabilmente coinvolto per responsabilit oggettiva assieme a tutti gli altri sanitari che hanno avuto contatti con il paziente , nei casi , invero molto frequenti , in cui il paziente , pervenuto in condizioni critiche in un dipartimento di urgenza o emergenza , sia stato sottoposto ad accertamenti radiologici . 
questo meccanismo ha causato anni addietro unepidemia di denunce contro i radiologi in francia [ 25 ] e negli stati uniti , tanto da rendere necessaria una riforma legislativa [ 9 ]  . un altro aspetto finora episodico , ma comunque allarmante rappresentato da denunce per mancato riconoscia . 
magnavita : a 12 - year follow - up study of malpractice claims against radiologists in italy common cases in which the patient arrives at the emergency department in critical conditions and undergoes radiological examinations . 
some years ago , this mechanism led to such an epidemic of malpractice suits against radiologists in france [ 25 ] and the united states that legislative reform was required [ 9 ]  . another feature to date episodic but nonetheless alarming is the malpractice claim for failure to diagnose a lesion in panoramic examinations , such as computed tomography ( ct ) , in the case of lesions outside the clinical setting that motivated and justified the examination or after review of examinations that were reassessed with modified reconstruction parameters in search of a lesion that only became apparent later . malpractice claims for failure to order further diagnostic examinations are still rather rare in italy and are generally associated with missed cancer diagnosis . 
this has led to a change in the main reason for radiological malpractice suits in the united states in recent years : whereas in the past , the radiologist was sued above all for having done something wrong , today they are sued for not having done something right [ 26 ]  . the number of malpractice claims filed against physicians for not having ordered radiological examinations has in fact increased , and in parallel , so , too , have the claims against radiologists for not having ordered further imaging examinations . 
nor can it be ruled out that in italy in the near radiologists will be sued for not having made use of new and promising diagnostic techniques , such as computer - assisted detection ( cad ) and teleradiology , or for not having called for a second opinion from an expert colleague [ 26 ]  . 
the fears shown by american physicians appear to be finding ground even in the italian situation . in our cohort , the frequency of claims for lesions caused by radiological procedures themselves ( such as contrastmedium reactions , organ rupture during barium enema , etc . ) account for only one tenth of the total . 
the cause of this type of problem may be attributed to the diffusion of interventional radiology and more in general to the need to administer drugs or contrast media during radiodiagnostic procedures . interventional radiology is in all countries a field with a high risk of litigation [ 27 ]  . 
a recent american study , the medmarx data report [ 28 ] based on the voluntary reporting of errors occurring between 2000 and 2004 in 314 hospitals , reported that medication errors in radiology departments cause harm to the patient with a frequency seven times higher than in other hospital departments . 
questa caratteristica differenzia sostanzialmente il nostro paese dagli stati uniti , dove questo tipo di denuncia ha avuto negli ultimi anni il maggiore aumento , rispetto alle altre cause di denuncia , anche a causa dellintroduzione di provvedimenti che , allo scopo di frenare la spesa sanitaria , obbligano i medici a limitare le prescrizioni [ 9 ]  . 
in questo modo si assistito , negli ultimi anni , ad un cambiamento della motivazione principale per le denunce di malapratica negli usa : se in passato il radiologo veniva denunciato soprattutto per aver fatto qualcosa di sbagliato , oggi lo si denuncia soprattutto per non avere fatto qualcosa di appropriato [ 26 ]  . 
sono infatti fortemente aumentate le denunce contro i medici per non avere ordinato esami radiografici , e parallelamente anche quelle contro i radiologi , per non avere prescritto ulteriori accertamenti radiografici o strumentali . 
non si pu escludere che , in un prossimo futuro anche in italia , i radiologi possano essere denunciati anche per non avere fatto ricorso a nuove , promettenti tecniche di ausilio alla diagnosi , come la computer assisted detection ( cad ) o la teleradiologia , o per non avere richiesto un secondo parere da parte di un collega esperto [ 26 ]  . 
i timori dei medici statunitensi non sembrano privi di fondamento neppure nella situazione italiana . nella nostra coorte , la frequenza di denunce per lesioni causate dalle stesse procedure radiologiche ( quali ad es . reazioni al mdc , rottura del viscere nel clisma opaco , etc . ) rappresenta solo un decimo del totale . 
la causa di questo tipo di problemi va attribuita alla diffusione delle tecniche di radiologia interventistica e pi in generale alla necessit di somministrare farmaci o mezzi di contrasto nel corso delle procedure radiodiagnostiche . le tecniche di radiologia interventistica rappresentano in tutti i paesi una branca ad elevato rischio di liti legali [ 27 ]  . una recente indagine statunitense , il medmarx data report [ 28 ] , basato sulla segnalazione volontaria degli errori verificatisi tra il 2000 e il 2004 in 314 ospedali , ha segnalato come la frequenza di errori nella somministrazione di farmaci nel reparto radiologico determini conseguenze dannose per il paziente con una frequenza sette volte maggiore che negli altri reparti dellospedale . 
anche se lamerican college of radiology ha formalmente protestato contro le conclusioni dellinchiesta [ 28 ] , ritenuta eccessivamente allarmante per il paziente ( i duemilatrenta errori censiti , a fronte di due milioni e mezzo di procedure radiologiche condotte nel periodo in esame , rappresentano un rischio pari allo 0 , 00008% ) , losservazione che gran parte degli errori di somministrazione o di prescrizione di farmaci avrebbe potuto essere eliminata con un migliore collegamento tra il dipartimento di radiologia e quello di provenienza del paziente merita una 1019 a . 
improved communications between radiologists and clinicians is at the same time desirable and imperative for overcoming the ambiguity that is often the origin of radiological errors [ 29 ]  . 
policies available on the italian market can be the loss occurrence type , with coverage for claims lodged for events that occurred in the insured year and up to the 10 - year cut - off period , or the claims made type , with coverage only for claims lodged in the insured year and with reference to it . 
claims made policies do allow for coverage of a prior period as part of an expressly requested additional clause but is limited to 2 or , at most , 4 years . 
it is worth bearing in mind when signing this type of contract that in radiology , a certain amount of malpractice claims are nonetheless beyond its contractual guarantees . the high frequency of claims in relation to deceased patients or patients suffering severe harm and the correlated onset of criminal liability should induce the radiologist to the strictest adherence of professional best practice at all times . 
it is therefore not superfluous to say that the radiologist must pay close attention to the information provided by the patient prior to performing the examination and always ask for a document of informed consent to be signed , especially in the case of contrast - enhanced or invasive examinations . 
the radiologist should inform the clinician of any problems arising in relation to the examination . maximum care should be dedicated to technique , devices and environmental characteristics of the radiology room in relation to which the law prescribes the precise safety features , for which the radiologist is responsible in his or her role as employer ( in a facility of his or her own property ) or as director ( if working in a public facility or a private facility of anothers ownership )  . 
il miglioramento della comunicazione tra il radiologo ed i clinici al tempo stesso desiderabile e imperativa per risolvere le ambiguit che sono spesso allorigine di errori radiologici [ 29 ]  . 
 responsabilit del clinico trasmettere al radiologo le informazioni rilevanti in modo chiaro ed adeguato ; compito del radiologo scegliere la procedura corretta , in base alla conoscenza della storia clinica del paziente . infine le nostre osservazioni confermano che altre cause di denunce , come gli infortuni subiti dai pazienti mentre si trovano allinterno della sala radiologica , limperizia nella esecuzione di terapie radianti , o altri problemi episodici ( raccolti nella categoria miscellanea ) hanno una prevalenza ridotta ( 7 , 8% )  . un aspetto molto rilevante per le sue conseguenze pratiche la latenza tra evento lesivo e denuncia . 
le polizze disponibili sul mercato italiano possono essere del tipo loss occurrence , con copertura delle denunce per sinistri avvenuti nellanno assicurato e fino alla prescrizione decennale , ovvero claims made , con copertura delle sole denunce pervenute nellanno assicurato e ad esso riferite . 
le polizze claims made prevedono , come clausola aggiuntiva da richiedere espressamente , la copertura di un periodo pregresso , per limitato a due o al massimo a quattro anni . 
bene sapere , sottoscrivendo questo tipo di contratti , che in radiologia una quota di sinistri rimane comunque al di fuori delle garanzie contrattuali . lelevata frequenza di denunce riferite a pazienti deceduti o con lesioni gravi , e la correlata insorgenza di responsabilit penali , devono indurre il radiologo alla pi scrupolosa adesione alle buone pratiche professionali in ogni momento della propria attivit . 
non sembri quindi pleonastico ricordare che il medico radiologo dovr quindi porre sempre la massima attenzione alle notizie fornite dal paziente prima dellesecuzione dellesame , e richiedere sempre la sottoscrizione di un valido consenso informato soprattutto nel caso di esecuzione di esami contrastografici o invasivi . 
la massima cura dovr essere dedicata alla tecnica , alle apparecchiature e alle caratteristiche ambientali della sala radiologica ; si ricordi , al proposito , che la legge prevede precise caratteristiche di sicurezza degli ambienti radiologici , delle quali il radiologo responsabile nella sua veste di datore di lavoro ( in una struttura di sua propriet ) o di dirigente ( se opera in una struttura pubblica o di altrui propriet )  . 
magnavita : a 12 - year follow - up study of malpractice claims against radiologists in italy should be performed with the necessary care and possibly integrated with reviews and comparisons of interpretations of other colleagues . 
in formulating the findings , the radiologist should indicate any unexpected or relevant data , as well as all limitations to interpretation and any further examinations that would be required to clarify the diagnostic query . the radiologist - patient relationship should also be given significant attention , especially since many malpractice claims are prompted by inadequate information flows regarding diagnostic possibilities and results . 
unfortunately , precisely this aspect , which is highly qualifying for the radiologist and reassuring for patients in relation to the level of attention and professionalism with which they will be examined , is increasingly impeded and sacrificed by the need for productivity imposed by radiology departments . 
yet paradoxically in the healthcare setting , and especially in radiology characterised by rapid technological development , the best defence for facing the phenomenon of legal action seems to be the improvement of those human characteristics that lie at the heart of the medical vocation . zione e possibilmente integrata da revisioni e confronti con linterpretazione di altri colleghi . 
nel formulare il referto il radiologo avr cura di segnalare eventuali dati inaspettati o rilevanti , cos come tutti i limiti interpretativi e gli eventuali ulteriori accertamenti che dovessero essere necessari per chiarire il quesito diagnostico . si raccomanda in particolare di curare al massimo il rapporto tra il medico radiologo ed il paziente , giacch molte denunce scaturiscono proprio da una inadeguatezza dei flussi informativi circa le possibilit diagnostiche ed i risultati raggiunti . 
purtroppo proprio questo aspetto , che quanto mai qualificante per il radiologo e rassicurante per il paziente circa lattenzione e la professionalit con cui verr esaminato , sempre pi ostacolato e sacrificato dalle esigenze di produttivit poste ai servizi di radiologia . 
gortenuti1 1dipartimento di radiologia , 2divisione di chirurgia clinicizzata , 3servizio di anatomia patologica , azienda ospedaliera di verona , p.le stefani 1 , i - 37126 verona , italy correspondence to : g . 
nineteen patients ( 13 men and six women ) scheduled for cea between march and august 2004 were imaged on a 1.5 - t scanner ( magnetom symphony , siemens , erlangen , germany )  . 
the protocol included four types of sequences [ t1 , t2 , proton density ( pd ) and three - dimensional time of flight ( 3d - tof ) ]  . 
therefore , it may be useful in evaluating and guiding the treatment of haemodynamically nonsignificant stenoses with a potential embolic risk and , in the future , to assess coronary plaque . key words magnetic resonance atherosclerosis carotid arteries atherosclerotic plaque riassunto obiettivo . 
19 pazienti ( 13 maschi e 6 femmine ) , programmati per intervento di tea , sono stati sottoposti ad esame rm ( 1 , 5 t magnetom symphony , siemens , erlangen , germania ) nel periodo compreso tra marzo e agosto 2004 . 
la rm ha identificato la presenza del core lipidiconecrotico con sensibilit e specificit del 91 , 6% e del 95 , 0% , rispettivamente , mentre la sola emorragia intraplacca con sensibilit e specificit rispettivamente del 91 , 6% e del 100% . 
la rm in grado di identificare i segni di instabilit delle placche carotidee con elevata sensibilit e specificit . potrebbe quindi essere utile nella valutazione delle stenosi emodinamicamente non significative con un potenziale rischio emboligeno , in modo di scegliere il miglior trattamento e nel futuro per la valutazione delle placche a livello coronarico . parole chiave risonanza magnetica aterosclerosi arterie carotidi placche aterosclerotiche g . 
randomised trials have demonstrated the efficacy of thromboendarterectomy ( tea ) compared with medical therapy in symptomatic patients with stenosis > 70% [ north american symptomatic carotid endarterectomy trial ( nascet ) 1991 ] [ 2 , 3 ]  . 
asymptomatic patients with stenoses greater than 60% treated with surgery have been shown to be less likely to develop ipsilateral transient ischaemic attacks ( tia ) at 5 years compared with medically treated patients [ 4 , 5 ]  . 
a number of studies [ 614 ] have demonstrated that magnetic resonance imaging ( mri ) has a high sensitivity and specificity for characterising atherosclerotic plaque composition in vivo and ex vivo . 
 [ 13 ] were the first to use three - dimensional time of flight ( 3d - tof ) bright - blood sequences for evaluating the fibrous cap whereas yuan et al . 
 [ 9 ] were the first to assess the in vivo accuracy of mri in identifying the presence of a soft core composed of a lipid - rich acellular region and / or the presence of haemorrhage . 
 this paper presents an mri - histology correlation study of the morphological features of carotid plaque , with special reference to the presence of lipid - rich core and intraplaque haemorrhage , in symptomatic patients with stenosis greater than 70% undergoing tea . materials and methods the study is based on the evaluation of tissue contrast features at mri . 
 between march and august 2004 , we prospectively studied 19 patients with symptomatic carotid disease ( 13 men and six women , mean age 72.5 years , age range 5981 ) using mri and mr angiography . 
patients had carotid stenosis greater than 70% diagnosed with doppler sonography and were symptomatic for the presence of at least one tia or minor stroke during the 3 months before surgery . 
we first assessed plaque morphology and then performed mr angiography of the neck veslaterosclerosi caratterizzata dal progressivo accumulo , a livello dellintima della parete arteriosa , di lipidi , proteine ed esteri del colesterolo con conseguente formazione di placche che possono ostruire il lume vasale o fissurarsi determinando occlusione acuta del vaso o provocare disseminazione emboligena [ 1 ]  . 
attualmente vivo linteresse per la valutazione delle lesioni a livello carotideo in considerazione dellalto impatto socio - economico che rappresenta lo stroke ( circa 4 , 5 milioni di morti allanno e 5 disabili su 1000 persone , nel mondo )  . 
trials randomizzati hanno dimostrato lefficacia della trombo - endo - arterectomia ( tea ) rispetto alla terapia medica nei pazienti sintomatici con stenosi > 70% ( nascet 1991 ) [ 2 , 3 ]  . 
in questi ultimi stato riportato che le stenosi superiori al 60% trattate chirurgicamente presentano una minor possibilit di sviluppare tia omolaterale a distanza di 5 anni , rispetto ai pazienti trattati farmacologicamente [ 4 , 5 ]  . studi autoptici hanno mostrato come il rischio clinico dellaterosclerosi non correli solo con il grado di stenosi , ma anche con le caratteristiche morfologiche delle placche . recentemente numerose pubblicazioni [ 614 ] hanno dimostrato che la rm in grado di caratterizzare in vivo ed ex vivo la composizione delle placche aterosclerotiche con alta sensibilit e specificit . 
in particolare hatsukami [ 13 ] stato il primo ad utilizzare le sequenze 3d tof bright - blood per la valutazione del cappuccio fibroso , mentre il gruppo di yuan [ 9 ] ha valutato per primo in vivo laccuratezza della rm nellidentificare la presenza di un core soffice composto da una regione acellulare ricca di lipidi e / o con presenza di emorragia . lo scopo di questo lavoro descrivere la nostra esperienza nella valutazione comparata rm / istologia , delle caratteristiche morfologiche delle placche carotidee , in particolare riguardo la presenza di core lipidico ed emorragia intraplacca , in pazienti sintomatici , con stenosi superiore al 70% , sottoposti ad intervento di tea . materiali e metodi lo studio si basa sulla valutazione delle caratteristiche di contrasto tissutale delle immagini rm . 
listologia stata considerata come gold standard . nel periodo compreso tra marzo e agosto 2004 abbiamo studiato prospetticamente 19 pazienti ( 13 maschi , et media 72 , 5 anni , range 5981 anni ) con sintomatologia suggestiva di patologia carotidea , mediante rm e angio - rm , che successivamente sono stati sottoposti a intervento di tea . tutti i pazienti presentavano una stenosi carotidea superiore al 70% diagnosticata mediante eco - doppler , sintomatica per la presenza di almeno un tia o un minor stroke nei 3 mesi precedenti lintervento chirurgico . lindagine rm stata condotta con un magnete da 1 , 5 t g . 
si utilizzato un protocollo desame standard come segnalato in letteratura , ottenendo immagini in 4 differenti pesature ( time of flight - tof , t1 , densit protonica e t2 pesate )  . 
dalla parte centrale di una fetta macroscopica dello spessore di 3 mm corrispondente alla scansione rm , sono state ricavate sezioni istologiche da 5 micron colorate con ematossilina - eosina . 
tutti i pazienti sono stati preventivamente informati del tipo di procedura e di studio al quale venivano sottoposti . per ogni tipo di sequenza abbiamo effettuato 4 scansioni ( immagini ) della placca , dello spessore e con intervallo di 3 mm , che poi sono state correlate con le corrispondenti sezioni istologiche derivanti dal pezzo operatorio . 
le immagini rm sono state analizzate da due radiologi , i quali congiuntamente hanno valutato tutte le sequenze ed espresso un parere comune in merito alla presenza di core lipidico / necrotico ed emorragia intraplacca.il muscolo sternocleidomastoideo stato preso come riferimento relativamente allintensit del segnale , per linterpretazione delle immagini . 
il core lipidico necrotico si individua come unarea di iperintensit di segnale nelle sequenze t1 , di segnale intermedio ( isointenso ) nelle sequenze 3d tof e di intensit variabile nelle sequenze t2 e dp . 
surgical specimens were fixed in formaldehyde , decalcified and embedded in parafffrom the central portion of a 3 - mm section corresponding to the mri slab , 5 - micron histological sections were obtained and stained with haematoxylin and eosin ( h&e )  . 
all patients were informed beforehand of the type of procedure and study they would undergo . for each sequence , we obtained four scans ( images ) of the plaque , with a thickness and interval of 3 mm , which were then correlated with the corresponding histological sections . 
the lipid - rich necrotic core appears as an area of high signal intensity on t1 , intermediate signal intensity ( isointense ) on 3d - tof and variable intensity on t2 and pd . 
in four patients , we evaluated three histological sections . mri identified the presence of a lipid - rich necrotic core and / or intraplaque haemorrhage in 45 / 56 regions as against 48 / 56 detected at histology , resulting in three false negatives and no false positives . 
sensitivity and specificity of mri were thus high , 91.6% and 100% , respectively , with a k value of 0.945 ( one false negative and no false positives )  . histology identified calcifications in 40 / 56 sections whereas mri detected them in 32 / 40 , showing a sensitivity and specificity of 80% and 93.7% , respectively , with a k value of 0.652 ( eight false negatives and one false positive )  . comparative mri and histological evaluation of the fibrous cap was possible in 23 / 41 cases only ; three sections showed cap ulceration , all of which were identified by mri . there were no false negatives and four false positives . 
un valore di k > 0 , 75 indica una buona concordanza ; k compreso fra 0 , 40 e 0 , 75 indica concordanza media [ 16 ]  . risultati due pazienti sono stati esclusi dallo studio a causa di artefatti da movimento durante lesecuzione della rm . 
in 4 pazienti sono state valutate 3 sezioni istologiche . la presenza di core lipidico - necrotico e / o emorragia intraplacca stata rilevata alla rm in 45 / 56 regioni , 48 / 56 invece il riscontro allistologia ; 3 quindi i falsi negativi mentre table 3 correlation between magnetic resonance imaging ( mri ) and histology lipid - rich core intraplaque haemorrhage calcifications disrupted fibrous cap g . 
previous reports indicate , however , that vulnerable plaque is characterised by a lipid - rich necrotic core and / or haemorrhagic focus and separated from the vessel lumen by an unstable fibrous cap [ 18 , 21 , 22 ]  . 
studies on the coronary arteries [ 2325 ] have demonstrated that progression of atherosclerosis is sporadic and related to the fissuring or rupture of plaque composed of an acellular core separated from the lumen by a thin fibrous cap . 
given the histological similarity of carotid and coronary plaque , we can assume that similar phenomena of plaque instability underlie tias that arise in patients with haemodynamically nonsignificant stenoses but vulnerable plaque . conventional angiography , such as ct and mr angiography , are unable to assess the morphological characteristics of plaque other than the presence of ulcerations ; in addition , the degree of stenosis does not correlate with plaque composition . as a consequence , an imaging method is needed that is able to provide this type of information . 
moreover , it can also provide information regarding the stage of the plaque : in early stages the lipid - rich necrotic core is surrounded by a fibrous cap with or without calcification whereas in later stages , the plaque may grow and become complex , with loss of continuity of its surface ( fibrous cap disruption ) and presence of haemorrhage or thrombus ; finally , it may calcify and become chronic . 
il core lipidico - necrotico stato riscontrato da solo in 34 / 56 regioni alla rm , mentre istologicamente in 36 / 56 sezioni con sensibilit e specificit rispettivamente del 91 , 6% e del 95 , 0% , con valore di k = 0 , 848 ( 3 falsi negativi e 1 falso positivo )  . 
la rm ha identificato la sola emorragia intraplacca in 11 / 56 sezioni , listologia in 12 / 56 sezioni , con elevate sensibilit e specificit , rispettivamente del 91 , 6% e del 100% ( valore di k 0 , 945 ) ( 1 falso negativo e nessun falso positivo )  . istologicamente le calcificazioni sono state riscontrate in 40 / 56 sezioni ; la rm le ha individuate in 32 / 40 , con sensibilit e specificit rispettivamente dell80% e del 93 , 7% con valore di k = 0 , 652 ( 8 falsi negativi e 1 falso positivo )  . la valutazione comparata rm / istologia del cappuccio fibroso stata possibile solamente in 23 / 41 casi ; 3 sezioni presentavano ulcerazione del cappuccio , tutte identificate dalla rm . 
quindi anche le stenosi lievi e medie possono determinare un infarto del miocardio : non solo il grado di stenosi a determinare levento , ma anche le caratteristiche della placca . 
a lr - nc is identified by hiper - isotense signal on t1 - weighted image ( arrow ) , and b hipo - isotense signal on time - of - flight ( tof ) image ( arrow )  . 
la rm inoltre pu fornire informazioni riguardo lo stadio evolutivo della placca : negli stadi precoci si osserva la presenza del core lipidico e / o necrotico circondato da un cappuccio fibroso con o meno delle calcificazioni , successivamente la placca pu crescere e diventare complessa con possibile difetto della sua superficie ( interruzione del cappuccio fibroso ) e presenza di emorragia o trombo ; infine pu calcificare e cronicizzarsi . noi abbiamo valutato pazienti con stenosi superiore al 70% sintomatici , quindi concettualmente 2 volte a rischio , con alta possibilit di riscontrare placche complesse . 
infatti nell85 , 7% delle sezioni istologiche abbiamo riscontrato segni di vulnerabilit ( core lipidico - necrotico ed emorragia ) individuati con alta sensibilit ( 93 , 7% ) e specificit ( 100% ) dalla rm , senza nessun falso positivo . 
il core , considerato separatamente , il componente pi rappresentato ( 64 , 3% delle sezioni ) mentre lemorragia da sola si rileva in circa 1 / 5 delle sezioni . 
la rm ha dimostrato alta specificit e sensibilit nellidentificazione di entrambi i componenti . valutazione a parte merita il frequente riscontro di calcificazioni ( 40 / 56 sezioni istologiche )  . 
esse non sono certo marker di vulnerabilit , ma indicano piuttosto lo stadio evolutivo avanzato ( cronico ) delle placche in esame : il dato spiegabile con il criterio di selezione scelto per la popolazione in studio e cio la presenza di una stenosi superiore al 70% . 
da sottolineare lalto numero di falsi negativi [ 8 ] nel riconoscimento delle calcificazioni , giustificabile con i limiti intrinseci della metodica . analogamente a quanto riportato in letteratura [ 9 , 26 , 27 ] , confermiamo che la distinzione tra core lipidico ed emorragia intraplacca si effettua fondamentalmente tramite la valutazione combinata delle sequenze t1 e tof . 
come illustrato nelle figure 1 e 2 sia il core lipidico che lemorragia appaiono iperintense in t1 , ma lemorragia pu essere distinta dal core lipidico in quanto appare iperintensa anche nelle sequenze tof , le quali rappresentano quindi le sequenze discriminanti . 
mri proved to have high specificity and sensitivity in the identification of both components . the high frequency of calcifications observed ( 40 / 56 histological sections ) requires separate analysis . 
worthy of note is the high number of mri false negatives [ 8 ] in recognising calcifications , which is explained by the methods intrinsic limits . in agreement with the literature [ 9 , 26 , 27 ] , our study confirms that the distinction between lipid core and intraplaque haemorrhage essentially relies on the combined assessment of t1 and tof sequences . 
adjacent sternocleidomastoid ( scm ) muscle both on t1 - weighted ( a ) ( arrow ) and time - of - flight ( tof ) ( b ) ( arrow ) sequences but isointense on pdw ( c ) ( arrow )  . 
this is fundamental in that fresh and recent haemorrhage could represent the real sign of vulnerability . placca fresca , recente e vecchia , con alta sensibilit utilizzando le quattro diverse sequenze , enfatizzando per , in particolare , il ruolo delle t2 e dp [ 28 ]  . 
questo dato fondamentale perch lemorragia fresca e recente , a differenza di quella vecchia , potrebbe rappresentare il vero segno di vulnerabilit . la scelta del trattamento di questi pazienti , dovrebbe quindi tener conto non solo del grado di stenosi , ma anche della composizione della placca : di fronte ad una placca vulnerabile , anche in assenza di una stenosi significativa , si potrebbe prospettare lipotesi di un atteggiamento interthe choice of treatment in these patients should therefore take into account not only the degree of stenosis but also plaque composition : vulnerable plaque , even without significant stenosis , could prompt an interventional approach rather than medical therapy alone . 
in addition , the information on plaque morphology could be used to choose between open or endovascular surgery on the basis of embolism risk , which can also influence the choice of the cerebral protection device to be used . 
possiamo inoltre sfruttare le informazioni derivate dallo studio della placca per scegliere fra la chirurgica classica piuttosto che lapproccio endovascolare sulla base del rischio emboligeno , che pu influenzare anche la scelta del dispositivo di protezione cerebrale da utilizzare . 
un limite dello studio rappresentato dal numero limitato di pazienti , tutti sintomatici , quindi con placche prevalentemente complesse . lutilizzo di bobine di superficie dedicate , aumentando il potere risolutivo , dovrebbe consentire una miglior accuratezza nella discriminazione delle diverse componenti tissutali . 
pensiamo inoltre che quando gli sviluppi tecnologici lo permetteranno , interessante sar lapplicazione di questa metodica allo studio delle placche coronariche . conclusioni conclusions the results of our study are in agreement with the literature data and confirm that mri has good sensitivity and specificity in identifying the various components of atherosclerotic plaque and , in particular , markers of plaque vulnerability . further studies are , however , needed to validate the method and allow mri to be increasingly used in clinical practice . i risultati del nostro studio sono in linea con i dati riportati in letteratura e hanno confermato che la rm presenta buona sensibilit e specificit nellidentificazione delle varie componenti della placca aterosclerotica , in particolare dei markers di vulnerabilit . 
biondetti1 1department of radiology , 2department of surgery zonda , 3department of hematology and bone transplantation , 4department of surgery beretta est , fondazione irccs , ospedale maggiore policlinico , mangiagalli e regina elena , via f . 
lamarmora 18 , i - 20122 milan , italy , e - mail : alemos@sirm.org received : 27 march 2006 / accepted : 15 june 2006 / published online : 11 october 2006 abstract purpose . 
sedation was required in 31 / 88 ( 35% ) ct examinations in group 1 and in 6 / 46 ( 13% ) in group 2 . conventional angiography was performed in 20 / 88 ( 22% ) cases in group 1 and in 6 / 46 ( 13% ) in group 2 . 
mdct can reduce the need for sedation and conventional angiography in children after liver transplantation . there is no effect on patient motion artefacts . key words multidetector ct hepatic transplantation motion artefacts riassunto obiettivo . 
nel periodo antecedente a settembre 2000 , abbiamo utilizzato la tc a singolo detettore ( sdtc ) , dopo questo periodo , la tc a detettori multipli ( tcmd )  . 
centoventisei bambini di et inferiore ai 6 anni , sono stati sottoposti a 134 tc addominali , 88 eseguite con sdtc ( 65% ; gruppo 1 ) e 46 con tcmd ( 35% ; gruppo 2 )  . 
nel gruppo 1 , la sedazione era necessaria in 31 delle 88 ( 35% ) tc effettuate , mentre nel gruppo 2 in 6 delle 46 ( 13% )  . 
gli artefatti da movimento sono stati individuati in 8 su 88 tc effettuate nel gruppo 1 ( 9% ) e in 4 su 46 nel gruppo 2 ( 8% )  . 
the introduction of multidetector ct ( mdct ) has again created a wealth of new imaging opportunities [ 35 ]  . the ability to acquire multiple projections of raw data with each gantry rotation permits thinner slices with higher resolution and shorter scanning times . 
further advantages of mdct versus single - detector row ct ( sdct ) include more consistent contrast enhancement and higher quality of angiographic reconstructions . the increased speed of mdct , the resulting shorter scan times and the increased ability for vascular reconstructions should decrease the need for sedation and conventional angiography studies as well as the frequency of motion artefacts in infants and younger children . 
the aim of this retrospective study was to address the question of whether or not mdct compared with sdct can decrease sedation needs , the frequency of conventional angiograms and patient motion artefacts in paediatric imaging . 
 materials and methods patients between january 1993 and june 2005 , 126 children 6 years of age or younger underwent 134 ct studies for evaluation of suspected postoperative complications after liver transplantation on the basis of abnormal clinical and sonographic findings . 
 con lintroduzione della tc a detettore singolo ( tcsd ) e successivamente con lintroduzione della tc spirale , alla fine degli anni 80 , luso di questa metodica nei pazienti in et pediatrica notevolmente aumentato [ 1 , 2 ]  . 
inoltre , lavvento della tcmd ha determinato un pi consistente enhancement vascolare ed una pi elevata qualit delle ricostruzioni tridimensionali . lincremento della velocit di scansione ed il risultante breve tempo di acquisizione , nonch la capacit di ottenere ricostruzioni vascolari tri - dimensionali , dovrebbe portare ad una riduzione del bisogno di sedazione , del numero di angiografie convenzionali e degli artefatti da movimento nei pazienti pediatrici . 
precedenti lavori hanno evidenziato che la frequenza di sedazione nei pazienti pediatrici sottoposti a tcmd era inferiore al 5% , rispetto al 30% ottenuto con la tcsd [ 68 ]  . 
quindi , noi abbiamo realizzato questo studio retrospettivo per rispondere alla domanda se limpiego della tcmd , confrontata con la tcsd , pu determinare una riduzione del bisogno di sedazione , della frequenza della angiografie convenzionali e degli artefatti da movimento nei pazienti pediatrici . materiali e metodi pazienti da gennaio 1993 a giugno 2005 , 126 pazienti pediatrici di et inferiore ai 6 anni , sono stati sottoposti a 134 tc delladdome per la valutazione di eventuali complicanze post - trapianto epatico , sulla base dei risultati clinici e di laboratorio e sulla base dei quadri ecografici . 
la tc viene utilizzata quando lecografia e / o la risonanza magnetica non sono diagnostiche , oppure quando richiesta una ulteriore valutazione . abbiamo retrospettivamente rivisto gli esami tc ed i dati clinici del gruppo di pazienti inclusi nel nostro studio . 
inoltre , abbiamo scelto i pazienti con trapianto epatico , in quanto la popolazione studiata nei due periodi era molto simile . questi pazienti avevano simili indicazioni per lesame tc e simili indicazioni per langiografia . 
inoltre , abbiamo utilizzato let di 6 anni come et massima , in quanto eravamo interessati nel valutare il bisogno di sedazione in questo gruppo di pazienti , in quanto solitamente i pazienti pi grandi non hanno bisogno di essere sedati . 
eighty - eight of the 134 studies ( 65% ) were performed with a sdct scanner ( group 1 ) whereas the remaining 46 studies ( 35% ) were performed with a mdct scanner ( group 2 )  . 
in order to reduce patient agitation resulting from venipuncture performed just prior to the administration of contrast material , an intravenous catheter was in place when the child arrived in the ct suite . 
nonionic contrast material ( iopamidolo bioindustria 300 mg / ml , l.i.m , bologna , italy ) was administered at a dose of 2.0 ml / kg by using a power injector ( envision ct , medrad , indianola , pa , usa )  . 
patients examined with an sdct or mdct scanner received intravenous contrast material by means of power injection , using a flow rate of 1.52 ml / s for a 22 - gauge intravenous catheter and 23 ml / s for a 20 - gauge intravenous catheter . 
for the arterial phase , the empiric delay ranged from 12 to 30 s whereas for the portal venous phase , the empiric delay ranged from 60 to 80 s after the start of the intravenous contrast injection . tube current and kilovoltage were adjusted according to body weight [ 9 ]  . 
with the sdct scanner , images were acquired with 5 - mm collimation , 5 - mm reconstruction interval , 10 - mm / s table speed and gantry rotation of 1s . 
mdct examinations were acquired with 0.8 - s gantry rotation , 2.5 - mm collimation , 2.5 - mm reconstruction interval and a table speed of 15 mm / s . 
ct scans were obtained during breath holding at suspended inspiration in cooperative patients and during quiet respiration in children who were unable to comply with breath - holding instructions and in patients who were sedated . for the study and analysis of complex vascular structures and anastomoses , we used multiplanar reformation ( mpr ) and three - dimensional ( 3d ) reconstructions images . 
considerata la natura retrospettiva dello studio , il consenso informato non stato necessario . esami tc durante un periodo complessivo di 12 anni , centoventisei pazienti di et inferiore a 6 anni , sono stati sottoposti a 134 esami tc delladdome . 
in quanto 8 pazienti sono stati ritrapiantati , ciascuno di essi stato sottoposto a 2 esami tc . ottantotto delle 134 tc ( 65% ) sono state effettuate con tcsd ( gruppo 1 ) , mentre le rimanenti 46 sono state effettuate con una tcmd ( gruppo 2 )  . 
lintervallo di tempo medio tra trapianto epatico ed esecuzione della tc stato di 47 giorni ( range , 7 giorni - 3 mesi )  . nel gruppo 1 , tutti gli esami tc sono stati effettuati con limpiego di una tc spirale ad una singola filiera di detettori ( highspeed ct / i , ge medical systems , milwaukee , wi , usa ) , mentre nel gruppo 2 , mediante lutilizzo di una tc a 4 file di detettori ( lightspeed q / xi , ge medical system , milwaukee , wi , usa )  . 
allo scopo di ridurre lagitazione dei piccoli pazienti , che altrimenti si avrebbe se lago cannula per linfusione del mezzo di contrasto fosse posizionato nella sala tc , lago cannula viene posizionato prima che il paziente arrivi alla sala tc . 
stato utilizzato mezzo di contrasto non - ionico ( iopamidolo bioindustria , 300 mg / ml , lim , bologna , italia ) , alla dose di 2 , 0 ml / kg , somministrato mediante una pompa automatica di iniezione ( envision ct , medrad , indianola , pa , usa )  . 
indipendentemente dal tipo di tc utilizzata ( singolo o multi - detettore ) , abbiamo utilizzato un flusso di iniezione pari a 1 , 52 ml / s con un ago cannula di 22 - gauge e di 23 ml / s con un ago cannula di 20 - gauge . 
tutti gli esami tc sono stati eseguiti allo scopo di evidenziare eventuali complicanze vascolari , per questo motivo abbiamo utilizzato una fase tc arteriosa ed una venosa . abbiamo utilizzato un ritardo empirico per iniziare la scansione nei pazienti che pesavano meno di 10 kg ( n = 23 ) , mentre per i pazienti pi grandi abbiamo utilizzato un sistema di sincronizzazione automatico ( smart prep , ge medical systems , milwaukee , wi , usa )  . 
per la fase arteriosa , il ritardo empirico stato dai 12 ai 30 secondi dallinizio dellinfusione del mezzo di contrasto , mentre per la fase portale dai 60 agli 80 secondi . la corrente del tubo ed il voltaggio sono stati aggiustati in base al peso del paziente [ 9 ]  . 
con la tcsd , le immagini sono state acquisite a 5 mm di collimazione , 5 mm di intervallo di ricostruzione e 10 mm / s di velocit di scorrimento del tavolo , con una rotazione del gantry di 1 secondo . 
con la tcmd , le immagini sono state acquisite a 2 , 5 mm collimazione , 2 , 5 mm di intervallo di ricostruzione , 15 mm / s di velocit di scorrimento del tavolo , con una rotazione del gantry di 0 , 8 secondi . 
 oral chloral hydrate ( major pharmaceuticals , rosemont , il , usa ) at a dose of 50100 mg / kg was administered for infants 18 months of age or younger , and intravenous pentobarbital sodium ( farmotal , farmacia spa , milan , italy ) at a dose of 6 mg / kg was administered for children older than 18 months [ 10 , 11 ]  . 
explanation of the procedure and reassurance by both staff and parents was used in nonsedated patients . angiography to assess the frequency of conventional angiography after the introduction of mdct , two paediatric radiologists retrospectively and independently reviewed records from our computerised database . 
 before the introduction of the mdct scanner at our institution , conventional angiography was performed in all cases in which vascular complications were suspected on sdct . since mdct became available , conventional angiography has been performed only to confirm positive mdct angiography findings . 
negative findings are confirmed by sonography . patient motion artefacts motion - related artefacts were randomly assessed in sedated and nonsedated patients by two paediatric radiologists who were blinded to each others reading with respect to sedation and sdct or mdct technology . 
an artefact was considered present if it degraded visualisation of major vascular structures , including hepatic veins , hepatic artery , portal vein , celiac axis and splenic vein on one or more images . 
a consensus was also obtained to determine whether diagnostic quality was good enough to avoid ct repetition . records of every patient were reviewed for any repeated exzienti collaboranti , e durante respirazione libera nei pazienti che non erano in grado di collaborare o che non erano in grado di apprendere le istruzioni per mantenere lapnea , e nei pazienti sedati . per lo studio e lanalisi di strutture vascolari complesse e delle anastomosi , abbiamo utilizzato le ricostruzioni multiplanari ( mpr ) e le ricostruzioni 3d . 
dopo lacquisizione dei dati , i dati grezzi sono stati retro - ricostruiti a 1 , 25 mm di collimazione e 1 , 25 mm di intervallo di ricostruzione ed inviati alla workstation ( advantage windows 3.1 , ge medical systems , milwaukee , wi , usa ) per le riformattazioni in immagini 3d . 
abbiamo usato 2 algoritmi di ricostruzione 3d : volume rendering ( vr ) e maximum intensity projection ( mip )  . sedazione per la valutazione della frequenza di sedazione , due radiologi pediatrici , retrospettivamente ed indipendentemente hanno valutato i dati clinici relativi ai pazienti inclusi nello studio . 
i pazienti sedati ed intubati , provenienti dalla terapia intensiva , non sono stati inclusi nello studio . nei bambini di 18 mesi di et e nei pazienti pi piccoli , abbiamo utilizzato idrato di cloro per os ( major pharmaceuticals , rosemont , ill , usa ) , per la sedazione , alla dose di 50100 mg / kg , mentre per i bambini pi grandi abbiamo utilizzato pentobarbitale sodico ( farmotal , farmacia spa , milano , italia ) , alla dose di 6 mg / kg [ 10 , 11 ]  . 
nei pazienti non sedati , si proceduto alla spiegazione della procedura e a riassicurarli , con laiuto del personale e dei genitori . angiografie convenzionali per la valutazione della frequenza delle angiografie convenzionali , dopo lintroduzione della tcmd , due radiologi pediatrici , retrospettivamente e indipendentemente hanno rivisto la frequenza delle angiografie eseguite prima e dopo lintroduzione della tcmd , estraendo i dati dal nostro database . 
i pazienti sottoposti ad angiografia allo scopo di eseguire procedure interventistiche , non sono stati inclusi nella stima della frequenza delle angiografie . prima dellintroduzione della tcmd nel nostro istituto , langiografia stata eseguita in tutti i casi sospetti per complicanze vascolari . 
the total time required for interpretation for all images was approximately 3 h for reader 1 and 3 h 20 min for reader 2 . statistical analysis students t test was used to compare mean patient ages in groups 1 and 2 . 
all statistical calculations were performed by using software package of spss version 11.00 ( spss , chicago , il , usa )  . results clinical the patient population consisted of 74 boys and 52 girls . clinical findings that prompted ct scanning after us and / or mri examination included abnormal liver function tests , abdominal pain , fever and gastrointestinal signs , including distension , vomiting and diarrhoea . 
un artefatto da considerarsi presente se esso degrada la visualizzazione delle maggiori strutture vascolari , incluse le vene sovra - epatiche , larteria epatica , la vena porta , il tronco celiaco o la vena splenica , su una o pi scansioni . 
gli artefatti non relativi al movimento ( ad esempio , volume parziali , artefatti da scalini ) sono stati ignorati nella valutazione delle immagini . le immagini tc sono state valutate alla work station ( advantage windows 3.1 , ge medical systems , milwaukee , wi , usa )  . 
il tempo totale necessario per linterpretazione di tutte le immagini stato di 3 ore per losservatore 1 e di 3 ore e 20 minuti per losservatore 2 . analisi statistica abbiamo utilizzato il test t di student per confrontare le medie delle et dei pazienti nel gruppo 1 e 2 . 
il test di pearson ( 2 test ) stato utilizzato per confrontare la frequenza di sedazione , il numero di angiografie e gli artefatti da movimento , tra i gruppi 1 e 2 . 
una terza misurazione stata effettuata per lanalisi degli artefatti da movimento . per esprimere la variabilit inter - osservatore nella valutazione degli artefatti da movimento , abbiamo determinato la concordanza complessiva e quella chance - correlata ( cohen statistico )  . 
tutti i calcoli statistici sono stati effettuati mediante limpiego di un software package spss versione 11.0 ( spps , chicago , il , usa )  . risultati clinica la popolazione dei pazienti consisteva in 74 maschi e 52 femmine . 
the overall agreement between the two readers in the assessment of patient motion artefacts was 100% whereas the chance - corrected agreement was expressed as almost perfect for both groups : = 0.83 ( 95% ci = 0.7550.912 ) for group 1 , and = 0.84 ( 95% ci = 0.7340.946 ) for group 2 . 
nei pazienti di et inferiore ad 1 anno , la sedazione stata necessaria in 21 su 28 ( 75% ) delle tcsd eseguite ( due pazienti sono stati sottopoti a 2 tc ciascuno ) ed in 4 su 8 delle tcmd ( 50% ) eseguite ( due pazienti sono stati sottoposti a due tc ciascuno ) ( p < 0 , 001 )  . 
nei pazienti fra 1 e 6 anni di et la sedazione stata necessaria in 10 su 62 tcsd eseguite ( 16% ) e in 2 su 38 ( 5% ) tcmd ( quattro pazienti sono stati sottoposti a 2 tc ciascuno )  . 
1 motion artefacts detected in a 5 - year - old boy with situs inversus following split - liver transplantation by using single - detector computed tomography ( sdct )  . 
non abbiamo ottenuto una differenza statisticamente significativa riguardo la frequenza dellangiografia in relazione allet e al bisogno di sedazione ( p > 1 )  . artefatti da movimento 8 delle 88 tc effettuate nel gruppo 1 ( 9% ) e 4 delle 46 tc effettuate nel gruppo 2 ( 8% ) , presentavano artefatti da movimento . 
la concordanza complessiva tra i due osservatori nellindividuare gli artefatti da movimento era del 100% , mentre la concordanza chance - correlata stata espressa come quasi perfetta per entrambi i gruppi : = 0 , 83 ( 95% ic = 0 , 755 a 0 , 912 ) per il gruppo 1 , e = 0 , 84 ( 95% ic = 0 , 734 a 0 , 946 ) , per il gruppo 2 . 
il ruolo delle ricostruzioni tri - dimensionali ( 3d ) nella valutazione delle strutture vascolari continua ad evolvere diventando sempre pi importante sia per quanto riguarda la valutazione delle complicanze vascolari che per quanto riguarda la cura del paziente . 
le principali applicazioni della tcmd nella valutazione dei pazienti pediatrici dopo trapianto epatico , includono le stenosi vascolari , le trombosi ed i difetti di perfusione del fegato trapiantato . nel nostro studio , nei pazienti da 0 a 6 anni di et , il bisogno di sedazione passato dal 35% con la tcsd , al 13% con la tcmd . 
b le ricostruzioni arteriografiche 3d ottenute dopo dilatazione ed il posizionamento di uno stent , dimostrano perviet del by - pass aorto - epatico ( frecce ) e perviet dellarteria epatica ( teste di freccia )  . discussion mdct plays an important role in the evaluation of vascular complications after liver transplantation . 
the role of 3d volume imaging in the evaluation of vascular structures continues to evolve , with this technique becoming increasingly important in the detection of vascular complications as well as in decisions about patient care . 
the principal clinical applications of mdct in the evaluation of children following liver transplantations include vascular stenoses , thromboses and perfusion defects of the transplanted liver . in our study , for patients in the 06 age range , the sedation rate changed from 35% with single - detector ct to 13% with the mdct scanners . 
pappas et al also reported that they did not need to sedate any patients aged 26 years when mdct was performed whereas in the 16 age group , we had a sedation rate of 5% . 
following surgery , liver transplant recipients are often anxious and agitated , and they are more likely to need sedation than is a random population consisting of some patients who are acutely ill and some who are asymptomatic or relatively asymptomatic . 
decreasing sedation rates would reduce the incidence of potential complications in addition to decreasing parental anxiety , increasing patient throughput and decreasing costs . conventional angiography has remained the standard of reference for the evaluation of vascular complications in liver transplant recipients , but given its invasiveness and cost , a noninvasive alternative technique for evaluating postoperative complications would be of clinical value . 
the advantages of reducing or obviating the need for conventional angiography include decreased frequency of complications such as haematoma formation and vascular injuries [ 13 , 14 ]  . other advantages of ct over conventional angiography include shorter acquisition times , superior 3d rendering and greater range of coverage , which increase detection of vascular and nonvascular abnormalities [ 15 , 16 ]  . 
 in addition to better 3d technology for vascular reconstructions and increased operator ability , we believe that the reduction of angiography rates did not depend on a different fixed protocol used after the advent of mdct at our institution . rather , this reduction simply reflects a different diagnostic aperano estremamente agitati . 
nei risultati ottenuti da pappas et al . , non ci sono stati pazienti che hanno avuto bisogno di sedazione nella fascia di et compresa fra i 2 ed i 6 anni , quando sono stati sottoposti a tcmd , mentre nella fascia di et fra 1 e 6 anni , noi abbiamo avuto una percentuale di sedazione pari al 5% . 
dopo un importante intervento chirurgico , quale il trapianto epatico , i piccoli pazienti sono spesso ansiosi ed agitati e perci necessitano maggior sedazione rispetto ad una popolazione random di pazienti , caratterizzata da alcuni pazienti nella fase acuta della malattia ed altri asintomatici o relativamente asintomatici . 
diminuendo il bisogno di sedazione , si reduce lincidenza di potenziali complicanze , oltre a diminuire lansiet dei genitori , il tempo di ricovero ed i costi . langiografia convenzionale rappresenta il gold standard nella valutazione delle complicanze vascolari dopo trapianto epatico , ma considerata la sua invasivit , ed i costi , una modalit alternativa non - invasiva sarebbe necessaria per la valutazione delle complicanze vascolari nei pazienti pediatrici dopo trapianto epatico . 
tali vantaggi consentono di valutare sia le complicanze vascolari che quelle non - vascolari del fegato trapiantato [ 15 , 16 ]  . oltre ad una miglior tecnologia 3d e ad una maggiore abilit delloperatore nelleffettuare le ricostruzioni vascolari , noi crediamo che la riduzione del numero di angiografie dopo lintroduzione della tcmd nel nostro istituto , non sia dipesa da un differente protocollo fisso utilizzato , ma da un differente approccio diagnostico . 
infatti , prima dellavvento della tcmd tutti i pazienti con sospette complicanze vascolari sono stati sottoposti ad ecografia e successivamente ad angiografia , mentre dopo lavvento della tcmd tutti i pazienti con sospette complicanze vascolari sono stati sottoposti ad ecografia e successivamente a tcmd . 
langiografia veniva effettuata solo per confermare i quadri tc positivi . sebbene la tc , come langiografia , richiedano luso di radiazioni ionizzanti , la dose al paziente della tc pi bassa rispetto a quella di un esame angiografico convenzionale ( 6 msv per una tc bifasica delladdome contro 12 msv per un esame angiografico convenzionale della vascolarizzazione epatica )  . 
per minimizzare la dose di radiazioni abbiamo seguito i criteri alara ( as low as reasonable achievable ) per i pazienti pediatrici sottoposti ad esame tc [ 17 , 18 ]  . 
la tcmd dovrebbe essere effettuata con parametri di acquisizione che provvedano proach : before the advent of mdct , all patients with suspected vascular complications underwent sonography and subsequently conventional angiography whereas after the advent of mdct , all patients with suspected vascular complications underwent sonography and mdct . 
conventional angiography was performed only to confirm positive mdct findings . although ct , like conventional angiography , requires the use of ionising radiation , the dose from mdct is still several times lower than that from conventional angiography ( 6 msv for a double mdct acquisition of the upper abdomen vs 12 msv for a conventional angiogram of the liver vasculature )  . 
these acquisition parameters should include the use of low milliamperage and kilovoltage settings ( a higher kilovoltage will be needed in patients with larger body habitus : > 50 kg ) , appropriate section thickness and a faster table speed [ 4 , 5 , 19 , 20 ]  . 
mdct has the advantage over mri of shorter acquisition times , which means a reduced need for sedation and the ability to scan extremely ill patients who cannot tolerate the long imaging times for mri examinations . 
 in our study , the difference between sedation and angiography rates was statistically significant ( p0.001 ) whereas the difference with regard to patient motion artefacts was not ( p ( cid : 2 ) 1 )  . 
one explanation is the small sample size . the relatively small number of patients is due to the fact that we limited our study to patients with liver transplantations rather than studying all patients who had ct scans . 
before and after the introduction of mdct , we aggressively used restraining straps and blankets in infants and young children and verbal reassurance and explanation of the procedure in older children . 
finally , another possible explanation for the lack of difference in motion artefacts between sdct and mdct may be the correlation between patient movements and scanning speed : in a faster scanner , patient motion may potentially create artefacts on more slices than on a slower scanner . 
questi parametri di acquisizione dovrebbero includere luso di un basso amperaggio e voltaggio ( un voltaggio pi alto necessario nei pazienti con maggiore abito corporeo : > 50 kg ) , appropriati spessori di collimazione e unalta velocit di scorrimento del tavolo [ 4 , 5 , 19 , 20 ]  . 
anche le acquisizioni multifasiche non sono utilizzate nella routine nei pazienti pediatrici e non dovrebbero essere eseguite se non c una specifica indicazione clinica ( es , studio vascolare )  . la tcmd ha anche guadagnato una larga approvazione come alternative alla risonanza magnetica ( rm ) nella diagnosi delle anomalie vascolari nei pazienti pediatrici . 
la tcmd ha il vantaggio rispetto alla rm di minori tempi di acquisizione , che significa un ridotto bisogno di sedazione e labilit di esaminare pazienti estremamente malati che non possono tollerare i lunghi tempi di acquisizione della rm . esiste il rischio di esposizione alle radiazioni con la tcmd , ma il rischio di una prolungata sedazione maggiore rispetto a quello delle radiazioni [ 5 ]  . nel nostro studio , la differenza fra la frequenza di sedazione ed il numero di angiografie convenzionali stata statisticamente significativa ( p0 , 001 ) , mentre quella degli artefatti da movimento non lo stata ( p ( cid : 2 ) 1 )  . 
una pu essere dovuta al limitato campione di pazienti , in quanto abbiamo limitato il nostro studio a pazienti pediatrici dopo trapianto epatico , piuttosto che a tutti i pazienti pediatrici che hanno effettuato un esame tc . 
prima e dopo lintroduzione della tcmd , abbiamo utilizzato in maniera piuttosto aggressiva fasce di contenimento e coperte , nonch la riassicurazione verbale nei pazienti pi piccoli e la spiegazione della procedura nei pazienti pi grandi . 
infine , unaltra possibile spiegazione per la mancanza di una differenza statisticamente significativa negli artefatti da movimento , fra tcsd e tcmd pu essere la correlazione tra i movimenti del paziente e la velocit di scansione : in una tc veloce , i movimenti del paziente possono potenzialmente creare artefatti su pi immagini rispetto a quelli creati in una tc pi lenta . il maggior limite di questo lavoro rappresentato dal fata.a. 
 to che il criterio per sedare o no il paziente stato definito dal radiologo insieme allanestesista e alla nurse della tc , e quindi soggetto ad una certa variabilit . conclusions the higher performance of mdct compared with sdct , the capability of 3d arteriographic reconstructions , better contrast enhancement as well as the speed of the examinations have allowed a reduction in the need for sedation and the number of conventional angiograms . 
a larger population is necessary to determine a significant effect on patient motion artefacts . conclusioni la capacit di effettuare ricostruzioni tri - dimensionali , il migliore enhancement vascolare , cos come la maggior velocit di acquisizione delle immagini , della tcmd rispetto alla tcsd , ha determinato come conseguenza una riduzione della frequenza di sedazione e del numero di angiografie . non c un apparente effetto sugli artefatti da movimento . con il continuo sviluppo della tecnologia tc , realistico sperare in unulteriore riduzione della frequenza di sedazione e delle angiografie convenzionali . 
volpe3 1diagnostica per immagini di euganea medica , via colombo 13 , i - 35020 albignasego ( pd ) , italy 2servizio di radiologia , ospedale civile , monselice ( pd ) , italy 3unit operativa di chirurgia del piede e della caviglia , casa di cura abano terme ( pd ) , italy correspondence to : l . 
the aim of this paper is to demonstrate the efficacy of the dynamic study of the forefoot during lateral compression of the metatarsal heads ( mulders manoeuvre ) in the visualisation of mortons neuroma . 
clinical evaluation , which is fundamental for accurate diagnosis , can make use of dynamic us in the first instance in order to confirm clinical signs and identify the correct site and number of masses . 
in our opinion , mr maintains a primary role in differential diagnosis with other diseases ( mainly stress fractures , bursitis , ganglion cysts or tendon tumour sheaths )  . key words foot ultrasound magnetic resonance , neuroma mortons neuroma riassunto obiettivo . 
nei 40 avampiedi esaminati lecografia dinamica ha permesso di riconoscere 37 formazioni espansive intermetatarsali ( 2 doppie localizzazioni ) , dimostrandosi maggiormente efficace rispetto alla sola valutazione statica che ne ha dimostrate solo 25 . negli avampiedi studiati con rm si avuta la conferma del sospetto ecografico di formazione espansiva in 16 su 22 rilievi ecografici con valutazione dinamica ; uno dei 6 casi non confermati alla rm stato successivamente operato ottenendo il riscontro chirurgico del neuroma . 
la valutazione clinica , fondamentale ai fini della diagnosi , pu giovarsi dellecografia dinamica come metodica strumentale di primo impiego per la verifica del sospetto clinico , lidentificazione della sede e del numero di localizzazioni ; la rm a nostro parere mantiene un ruolo determinante nella diagnosi differenziale con altre patologie ( principalmente fratture da stress , borsiti , ganglio sinoviale o tumore gigantocellulare delle guaine tendinee )  . parole chiave piede , ecografia piede , risonanza magnetica neuroma di morton l . 
the aim of our study was to compare clinical , surgical and magnetic resonance ( mr ) findings with results obtained from examination of the intermetatarsal spaces with both static and dynamic ultrasound ( us )  . 
 la sindrome di morton una metatarsalgia neuralgica causata dallintrappolamento del nervo digitale comune nel canale metatarsale ; il traumatismo continuo determina un processo flogistico perineurale che a sua volta induce proliferazione connettivale endo - perineurale e degenerazione ialina dellendonevrio [ 1 ]  . 
la diagnostica per immagini viene impiegata per confermare il sospetto clinico , la sede ed il numero di localizzazioni e nella diagnosi differenziale con altre patologie [ 24 ]  . 
scopo del nostro lavoro stato quello di comparare i dati clinici , i rilievi chirurgici ed i riscontri rm con i risultati ottenuti dallesame degli spazi intermetatarsali con ecografia sia statica che dinamica , questultima ottenuta valutando ecograficamente gli effetti della compressione laterale delle teste metatarsali , in pazienti con sospetto clinico di neuroma di morton . materials and methods a total of 40 forefeet were studied in 38 patients ( 29 women and nine men , age range 2574 years ) , all with a clinical picture of interdigital neuritis ( table 1 )  . 
 following us assessment , mr was performed on 26 / 40 forefeet using dedicated low - field equipment ( esaote artoscan ) to obtain spin echo ( se ) t1 sequences ( tr / te 400 / 20 ms ) , se t2 sequences ( tr / te 2 , 600 / 90 ms ) and short - tau inversion recovery ( stir ) sequences ( tr / te / ti 1 , 580 / 22 / 65 ms ) , with a slice thickness of 4 mm in the sagittal , coronal and axial planes . a total of 20 intermetatarsal spaces were surgically explored in 18 forefeet ( two spaces were examined simultaneously in two cases )  . 
surgical treatment consisted of neurecmateriali e metodi sono stati studiati con ecografia in tutto 40 avampiedi in 38 pazienti ( 29 femmine e 9 maschi , di et compresa tra i 25 ed i 74 anni ) , con quadro clinico riferibile a neurite intermetatarsale ( tabella 1 )  . 
alla valutazione statica si associata lanalisi dinamica ottenuta con la compressione laterale delle teste dei metatarsi eseguita manualmente come nella manovra di mulder ; simultaneamente si registrato il quadro ecografico in sequenze di video - clip . alla valutazione ecografica seguita una rm di 26 / 40 avampiedi , utilizzando un apparecchio dedicato a basso campo ( esaote artoscan ) , ottenendo acquisizioni se t1 ( tr / te 400 / 20 ms ) , se t2 ( tr / te 2600 / 90 ms ) e stir ( tr / te / ti 1580 / 22 / 65 ms ) secondo i piani sagittale , coronale e assiale , con spessore di strato di 4 mm . table 1 summary of all cases forefeet , n tabella 1 sintesi della casistica in esame avampiedi , n clinical evaluation static and dynamic sonography surgery chirurgia valutazione clinica ecografia statica e dinamica l . 
lesplorazione chirurgica dei 20 spazi intermetatarsali ha rilevato in 19 la presenza di un neuroma di morton ; in un caso si riscontrato un ganglio sinoviale in continuit con la guaina del tendine flessore del 4 dito . complessivamente sono state identificate con ecografia nei 40 avampiedi esaminati ( tabella 2 ) 37 formazioni espansive di cui 36 formazioni nodulari solide ed 1 a contenuto fluido ( in 4 pazienti erano presenti 2 localizzazioni : in 2 pazienti nello stesso avampiede mentre negli altri due erano localizzate una per ciascun avampiede )  . 
a paziente supino si esplora il versante plantare con lieve inclinazione caudo - craniale della sonda ; la mano libera dellesaminatore esegue la manovra di compressione dei metatarsi . tomy through the intermetatarsal dorsal approach , with excision of the nerve at least 1 cm above the proximal margin of the deep transverse metatarsal ligament and repositioning of the nerve stump in the oblique adductor muscle . 
 results correlazione ecografia statica , ecografia dinamica , rm all patients had symptoms of intermetatarsal neuritis characterised by episodic pain in the distal metatarsal region , nei 40 avampiedi esplorati erano riconoscibili con ecografia statica ( es ) 25 / 37 ( 67 , 6% ) delle formazioni espansive ritable 2 correlation of data between static sonography , dynamic sonography and magnetic resonance ( mr ) in all cases investigated lesions / forefeet , n 25a / 40 37b / 40 static sonography dynamic sonography aone forefoot with double localisation btwo forefeet with double localisation tabella 2 confronto tra i dati relativi alla ecografia statica , ecografia dinamica e rm nel riscontro di formazioni espansive intermetatarsali in tutti i pazienti considerati nello studio lesioni / avampiedi , n 25a / 40 37 b / 40 ecografia statica ecografia dinamica aun avampiede con duplice localizzazione bdue avampiedi con duplice localizzazione 16a / 26 16 a / 26 l . 
in one case , a synovial ganglion was found in continuity with the flexor tendon sheath of the fourth toe . us identified 37 masses in the 40 forefeet examined ( table 2 )  . 
thirty - six were solid nodular formations , and one had a fluid content ( two localisations were present in four patients : two on the same forefoot in two patients , and one on each forefoot in the other two )  . 
in all cases , there was correlation between the site of the us finding and clinical examination ( pain on compression of the site )  . correlation between static us , dynamic us and mr in the 40 forefeet examined , static us ( sus ) detected 25 / 37 ( 67.6% ) of masses identified by us : 24 of these were small hypoechoic masses , with a diameter ranging from 4 mm to 9 mm , prominent on the plantar side at the level of the intermetatarsal space . 
sequenza di immagini ottenute prima ( a ) , e nel corso ( b , c ) della compressione laterale dei metatarsi che evidenzia il neuroma ( frecce ) riconoscibile solo nella fase dinamica , protrudere dallo spazio intermetatarsale per effetto della spremitura . scontrate complessivamente con ecografia : di esse 24 erano masserelle solide ipoecogene rispetto ai tessuti circostanti , con diametro variabile da 4 a 9 mm , prominenti sul versante plantare in corrispondenza dello spazio intermetatarsale . altre 12 formazioni ( 32 , 4% ) con analoghe caratteristiche ecografiche sono risultate riconoscibili solo con ecografia dinamica ( ed )  . 
3a sonography shows a fluid - filled mass , with mild inner echoes , protruding onto the plantar aspect at the third intermetatarsal space ( arrows ) and fixed during the dynamic manoeuvre related to the synovial cyst . 
b axial magnetic resonance ( mr ) t1 - weighted and coronal short - tau inversion recovery ( stir ) images confirm the presence of a fluid - filled mass in the intermetatarsal space ( arrows )  . 
3a scansione ecografica che dimostra una formazione a contenuto liquido con echi interni prominenti sul versante plantare tra le teste del 3 e 4 metatarso , immobile alla valutazione dinamica , compatibile con ganglio sinoviale . 
b acquisizioni rm assiale t1 e coronale stir confermano la presenza di formazione a contenuto fluido nel terzo spazio intermetatarsale . sonographic features were detected by dynamic us ( dus ) only . 
quindici di esse corrispondevano a formazioni solide nello spazio intermetatarsale , ipointense nelle acquisizioni t1 e t2 pesate con i caratteri del neuroma ( in un paziente era presente duplice localizzazione nello stesso avampiede ) ; in 8 di esse si associava il rilievo di una fig . 
4a , b longitudinal ultrasound ( us ) scan ( a ) in correspondence with the third metatarsal head showing thickening of the capsular structures on the plantar aspect related to capsulitis . 
fifteen of these were solid masses in the intermetatarsal space and hyperintense in the t1and t2 - weighted images with the appearance of neuroma ( one patient had two localisations on the same forefoot ) ; in eight of these , the finding was associated with fluid distension of the intermetatarsal bursa . 
 one of the six lesions seen on us and not confirmed on mr was later identified by surgical exploration , which identified a 5 - mm diameter neuromatous mass ; the other five received conservative treatment . 
1 , legamento trasverso metatarsale profondo e superficiale ; 2 , fascio neurovascolare ; 3 , muscolo e tendine lombricale ; 4 , tendini flessori delle dita ; 5 , borse intermetatarsali ; 6 , muscoli interossei . sistently confirmed the presence of a mass , with identification of 20 masses in 18 forefeet ( in two cases , there were two localisations on the same forefoot ) : 13 / 20 ( 65% ) were recognised using sus whereas 7 / 20 ( 35% ) were only seen on dus . among patients who underwent surgery , mr assessments were available for ten forefeet : mr correctly identified 8 / 11 lesions ( 72.7 % ) ( one patient had double localisation on the same forefoot ) ; in 2 / 11 ( 18.2% ) , results were uncertain , even on retrospective analysis ; in 1 / 11 ( 9.1% ) , results were negative . 
the neurovascular bundle and lumbrical muscle pass through the lower compartment immersed in abundant fat tissue whereas in the higher level , also immersed in fat , we can find the tendons of the interosseous muscles and the intermetatarsal bursa . 
in its relationship with the deep transverse metatarsal ligament , the latter is most prominent distal to the level of the second or third space beyond which it comes into contact with the neurovascular bundle [ 5 ]  . ( 9 , 1% )  . 
nella loggia inferiore decorre il fascio neurovascolare ed il muscolo lombricale immersi in unatmosfera adiposa , mentre nella loggia superiore , immersi anchessi nel tessuto adiposo , si trovano i tendini dei muscoli interossei e la borsa intermetatarsale ; questultima nel suo rapporto con il ligamento trasverso metatarsale profondo si dimostra maggiormente prominente distalmente a livello del 2 e 3 spazio ove , superandolo , giunge a contatto con il fascio neurovascolare [ 5 ]  . la metatarsalgia neuralgica nella sindrome di morton dunque da considerarsi una sindrome da impingement del nervo digitale comune nello spazio intermetatarsale legata a dislocamento dorsale del nervo tra le teste metatarsali a seguito della pressione plantare e successivamente pinzato tra le teste stesse , in associazione o meno a concomitante borsite . 
il continuo traumatismo determina un processo flogistico perineurale che induce proliferazione connettivale endo - perineurale e degenerazione ialina dellendonevrio [ 1 ] con ingrossamento del nervo che alimenta il meccanismo di impinl . 
 mulders manoeuvre is important in the diagnosis of the neuroma and consists of lateral compression of the metatarsal heads in alternation with plantar pressure , which tends to induce plantar dislocation of the intermetatarsal mass provoking a clicking sensation ( mulders click )  . 
 in our series , the efficacy of us in identifying intermetatarsal masses improved with the use of dynamic assessment , the sensitivity in the group with surgical correlation being 65% for sus and 100% for dus . 
these results seem to be inferior to those reported in the literature in terms of static assessment but are aligned with the best results obtained by dynamic assessment in the most recent series [ 69 ]  . 
one justification for the different sensitivity values of static us in our series may be its limited use , with only the plantar approach and without using the usual manual interdigital compression . 
dynamic assessment with lateral compression of the metatarsal heads , in our opinion , increases us sensitivity , allowing recognition of the neuroma as it is expelled from the intermetatarsal canal , which it entered due to plantar pressure or attraction by neighbouring structures , such as the intermetatarsal bursa ( which at surgery is often indistinguishable from the nerve )  . 
 in our series , mr had a sensitivity of 72.7% in the examination of intermetatarsal masses , which is lower than that found in studies using high - field equipment [ 10 ]  . 
in our experience , in particular , the most effective sequences for recognising the neuroma proved to be se t1 and t2 in the axial and coronal planes whereas identification with stir sequences was affected by oedema of plantar soft tissue that can mask the neuroma [ 10 ]  . 
in the five cases that did not undergo surgery , mr was nonetheless able to account for the clinical picture , with findings compatible with mechanical support capsulitis in three cases and a stress fracture of the third metatarsal in two . 
tale entit anatomo - patologica comunemente conosciuta come neuroma di morton . la manovra di mulder , importante manovra semeiologica nella diagnosi del neuroma , consiste nella compressione laterale delle teste metatarsali alternata a pressione plantare , che tende a provocare la lussazione plantare della massa intermetatarsale evocando una sensazione di scatto ( click di mulder ) ; tale meccanismo rende maggiormente evidente allecografia la massa stessa durante la spremitura dallo spazio intermetatarsale apparendo questa maggiormente prominente sul versante plantare . nella nostra casistica lecografia si rilevata maggiormente efficace nel riscontro di formazioni espansive intermetatarsali , quando si utilizzata la valutazione dinamica con una sensibilit nel campione con verifica chirurgica del 65% per la es e del 100% per la ed ; tali risultati appaiono inferiori a quanto riportato in letteratura per quello che riguarda la valutazione statica mentre si allineano ai migliori risultati ottenuti nelle casistiche della letteratura anche pi recente considerando la valutazione ecografica dinamica [ 69 ]  . 
una giustificazione alla discrepanza nei valori di sensibilit della ecografia statica pu essere ricercata nelluso limitato di tale metodo considerando nella nostra casistica il solo approccio plantare senza lutilizzo delle usuali tecniche di compressione manuale interdigitale . 
la valutazione dinamica con compressione laterale delle teste metatarsali aumenta a nostro giudizio comunque la sensibilit della metodica , consentendo il riconoscimento della masserella neuromatosa nella sua espulsione dal canale intermetatarsale , ove la stessa risalita a causa della pressione plantare o per attrazione da parte di strutture limitrofe come la borsa intermetatarsale ( che al tavolo operatorio risulta spesso indissociabile dal nervo )  . lindagine rm ha dimostrato nella nostra serie una sensibilit del 72 , 7% nel riscontro di formazioni espansive intermetatarsali ; tale dato risulta inferiore a quanto riportato in letteratura con indagini eseguite peraltro utilizzando apparecchiature ad alto campo [ 10 ]  . 
in particolare nella nostra esperienza le sequenze pi efficaci nel dimostrare il neuroma sono risultate le se t1 e t2 nei piani assiale e coronale , mentre le sequenze stir hanno presentato maggiori problemi nellidentificazione della massa neuromatosa in relazione alla presenza concomitante di edema dei tessuti molli plantari che pu mascherarla [ 10 ]  . 
in 5 casi non operati infine la rm ha potuto comunque giustificare il quadro clinico riscontrando in 3 di essi un quadro compatibile con una capsulite meccanica da appoggio ed in 2 una frattura da durata del 3 metatarso . conclusioni diagnosis of neuroma remains prevalently based on clinical findings , partly in consideration of the high incidence of la diagnosi di neuroma resta legata prevalentemente ai rilievi clinici , anche in considerazione dellelevata incidenza di riscontro di formazioni compatibili con neuromi tanto alconclusions l . 
diagnostic imaging ( us and mr ) is used to confirm the clinical diagnosis , site and number of localisations and in differential diagnosis with other conditions [ 6 , 10 , 12 ]  . in our experience , us remains the initial modality for assessing the forefoot of the patient with neuralgic metatarsalgia ; dynamic assessment allows easy identification of intermetatarsal masses . 
mr should be left as a second - level investigation to be carried out after us has failed to justify the clinical findings ; when other conditions need to be ruled out , such as stress fractures , bursitis or synovitis ; or to better characterise capsulitis , a synovial ganglion or a giant cell tumour of the tendon sheath . la ecografia che alla rm in pazienti asintomatici [ 11 , 12 ]  . la diagnostica per immagini ( ecografia e rm ) , viene impiegata per confermare il sospetto clinico , la sede ed il numero di localizzazioni e nella diagnosi differenziale con altre patologie [ 6 , 10 , 12 ]  . lecografia nella nostra esperienza resta metodica di primo impiego nella valutazione dellavampiede del paziente con metatarsalgia neuralgica consentendo con la valutazione dinamica il facile riscontro di processi espansivi intermetatarsali . 
da pozzo , istituto di radiologia , via giustiniani 5 , i - 35128 padova , italy , e - mail : spoxius@libero.it received : 24 february 2006 / accepted : 28 june 2006 / published online : 11 october 2006 abstract purpose . 
progressive multifocal leukoencephalopathy ( pml ) is a serious disorder that primarily affects individuals with a suppressed immune systefew semiological elements help clearly distinguish pml from other diseases included in the differential diagnosis . 
the purpose of this study was to confirm the diagnostic value of conventional mri sequences combined with diffusion - weighted imaging ( dwi ) in pml to identify those patients with worst prognosis . 
dwi permits more accurate differentiation of the disease progression front , which exhibits low signal intensity in apparent diffusion coefficient ( adc ) maps , from the central gliotic area of demyelinisation , characterised by high adc values . 
the addition of dwi sequences to conventional mri seems to be a valid method for accurately diagnosing pml and establishing the degree of disease progression . key words progressive multifocal leukoencephalopathy diffusion - weighted magnetic resonance imaging riassunto obiettivo . 
le sequenze pesate in diffusione permettono pi accuratamente di differenziare il fronte di progressione della malattia che appare ipointenso nelle mappe adc , dalla porzione centrale di demielinizzazione con riparazione gliotica ( elevati valori adc )  . 
le sequenze convenzionali associate alle nuove sequenze pesate in diffusione sembrano in grado di porre diagnosi di pml e di fornire indicazioni sul grado di progressione della malattia . parole chiave leucoencefalopatia multifocale progressiva risonanza magnetica diffusion - weighted s . 
among these disorders , progressive multifocal leukoencephalopathy ( pml ) is caused by the reactivation of human polyomavirus jc ( jcv ) , which remains latent in the organism and becomes pathogenic and aggressive in conditions of serious iatrogenic immunodeficiency as in leukaemia and lymphoma or of immunodepression mediated by other pathogens influencing the immune system directly as in patients with acquired immunodeficiency syndrome ( aids )  . 
jcv selectively affects oligodendrocytes , causing their cytolysis and consequent demyelination [ 2 ]  . the clinical presentation of pml is usually characterised by a progressive decline in mental status ( cognitive function ) often associated with neurological focal , motor and visual deficits ( homonymous hemianopsia )  . cerebral magnetic resonance imaging ( mri ) permits a noninvasive study of the brain and accurately reveals multifocal lesions of the white matter , which are hypointense on t1 - weighted sequences and hyperintense on t2 , often located in the grey / white interface with involvement of u - fibres [ 3 ]  . the most affected area is the semioval centre although the posterior cranial fossa is involved in about one third of all cases [ 4 ]  . 
in particular , reaction to contrast agents at the lesion margins seems to be related to improvement in the patients immunocompetence and the presence of mass effect to particularly aggressive forms [ 5 ]  . neuropathological studies have identified areas with different stages of white matter demyelination in the same lesion . 
older lesions and the central portion of more recent ones are characterised by almost total breakdown of the myelin sheath and axonal damage , with an increase in extracellular space . 
other studies [ 6 ] have recently discovered some interesting peculiarities of pml lesions in diffusionweighted sequences : although homogeneous on t1 and t2 , these lesions are characterised by different signal intensity on diffusion - weighted sequences and different apparent diffusion coefficient ( adc ) values . the aim of this paper is to illustrate the differences between gliotic and necrotic components and active disease elements in order to help establish the diagnosis and assess disease progression in response to treatment . pazienti immunocompromessi presentano spesso disturbi neurologici [ 1 ] dovuti ad malattie opportunistiche o neoplastiche la cui diagnosi differenziale affidata , oltre che alla neuroimmagine , anche ad esami laboratoristici del liquor e del sangue , alla risposta alle terapie e alla evoluzione nel tempo delle lesioni.fra queste malattie la pml legata alla riattivazione di un virus jc che , ubiquitario nellorganismo , diventa patogeno ed aggressivo in condizioni di grave immunodepressione iatrogena , come nelle leucemie e nei linfomi , o mediata da altri agenti patogeni che agiscono direttamente sul sistema immunitario , come nei pazienti aids . 
la presentazione clinica caratterizzata da un declino progressivo delle funzioni cognitive spesso associato a deficit neurologici focali motori o visivi ( emianopsia omonima )  . la rm cerebrale permette lo studio non invasivo dellencefalo riconoscendo con elevata sensibilit lesioni multifocali della sostanza bianca che appaiono ipointense nelle sequenze t1 pesate , iperintense in t2 , spesso localizzate a livello dellinterfaccia fra sostanza grigia e bianca con coinvolgimento delle fibre ad u [ 3 ]  . 
in particolare , la risposta al mezzo di contrasto ai margini delle lesioni sembra in relazione al miglioramento della immunocompetenza del soggetto mentre la presenza di effetto massa sembra essere correlata a forme particolarmente aggressive [ 5 ]  . studi neuropatologici hanno evidenziato allinterno della stessa lesione aree con differenti stadi di demielinizzazione della sostanza bianca . 
le lesioni pi datate cos come la porzione centrale delle lesioni recenti sembrano caratterizzate da una quasi totale perdita di mielina e da un danno assonale con allargamento degli spazi extracellulari . 
recentemente alcuni autori [ 6 ] hanno rilevato alcune specificit delle sequenze pesate in diffusione nellanalisi delle lesioni della pml evidenziando come esse , pur apparendo omogenee in t1 e t2 , siano invece caratterizzate da diverse intensit di segnale nella sequenza pesata in diffusione e da diversi valori di adc . lo scopo di questo studio di sottolineare le differenze fra componenti gliotiche o necrotiche e componenti in fase attiva di malattia al fine di aiutare a porre diagnosi e per valutare la progressione della malattia in risposta alle terapie effettuate . materials and methods we examined four men aged between 40 and 50 years affected by pml with identification by polymerase chain reaction ( pcr ) of jcv sequences in csf . 
in two patients , ( dl and tp ) , the disease rapidly led to death while the other two patients ( cm and ad ) presented a chronic course and are sono stati esaminati 4 pazienti , tutti di sesso maschile , con et compresa tra 40 e 50 anni , affetti da pml e con identificazione nel liquor cerebrospinale delle sequenze del jcv . 
the study protocol included axial single - shot echoplanar diffusion images [ 5 , 871 / 99 / 1 ( tr / te / excitation ) ] , fov = 24 cm , matrix 128128 , b - value of 0 and 1 , 000 s / ( mm ) ^2 in each cardinal plane . case 1 dl , a 53 - year - old man treated in 1989 for chronic lymphatic leukaemia ( cll ) with chemotherapy ( fludarabine + cyclophosphamide ) and splenic radiotherapy , presented in february 2004 with slowly progressive motor deficits in the right upper limb and language disorder with onset 1 week previously . 
tutti i pazienti sono stati esaminati mediante uno scanner marconi picker medical system 1 , 0 t polaris con sequenze sagittali ed assiali t1 spin echo ( 434 / 12 / 2 [ tr / te / excitation ] ) , axial dual echo fast spin echo ( fse , etl = 4 ) ( 3473 / 20 and 120 / 2 [ tr / te / excitation ] ) , axial fluid attenuated inversion recovery ( flair ) fast spin echo ( fse , etl = 8 ) ( 2100 / 6000 / 80 / 1 [ ti / tr / te / excitation ] )  . 
il paziente progressivamente peggiorato e successivi controlli rm condotti dopo 7 e 24 gg rispetto al primo esame confermano una progressione delle lesioni senza comparsa di contrast enhancement ; un successivo controllo liquorale tramite pcr evidenzia positivit per jc virus . 
lobiettivit neurologica allingresso evidenziava : parziale disorientamento s / t , anosognosia , deficit di attenzione , comprensione , denominazione , ripetizione , memoria , calcolo , ragionamento astratto e tendenza alla confabulazione ed alla perseverazione . 
the patient refused further examination and died 2 months later . case 2 tp , a 55 - year - old man , was accompanied to the emergency room in a state of agitation after knocking down a pedestrian proceeding from the left while aboard his moped . 
approximately 2 weeks later , an outpatient brain mri was performed , disclosing lesions in the right occipitaltemporal and left occipital white matter that did not react to contrast mediuthe patient was admitted to the neurology department . 
neurological examination performed on admission showed partial s / t disorientation ; anosognosia , cognitive impairment with deficits in attention , comprehension , denomination , repetition , memorisation , calculation , abstract reasoning and a tendency to confabulate and perseverate . brain ct revealed an extensive hypodense lesion in the right temporoparietooccipital subcortical region and , less markedly , in the left occipital region . 
biohumoral tests showed moderate pancytopenia [ white blood cell count ( wcc ) 2.70109 / l ( nv 4.411 ) , neutrophils 33% , red blood cell count ( rcc ) 3.191 , 012 / l ( nv 4.55.9 ) , haemoglobin ( hb ) 103g / l ( nv 140175 ) , haematocrit ( ht ) 32% ( nv 4150 ) , platelets ( plt ) 139109 / l ( nv 150450 ) ] , with an increase in erythrocyte sedimentation rate ( esr ) [ 80 mm / h ( nv 228 ) ] and normal fibrinogen , c - reactive protein ( crp ) and a - 2 globulin values . 
a follow - up brain mri performed roughly 1 month after the previous one showed an increase in lesion dimensions , which had extended to the right parietal and insularfrontal and left temporal regions . 
the patient underwent lumbar puncture , which proved positive for jcv . the patient rapidly deteriorated and died 1 month later . case 3 cm , a 42 - year - old man admitted to hospital due to dimmed eyesight lasting about 15 min with inability to distinguish surrounding objects , reported having experienced progressive decline in eyesight over the previous 2 months . 
in view of a selective fall in cd4 lymphocytes ( approximately 90 ) and a diminished cd4 / cd8 ratio ( 01 ) , human immunodeficiency virus ( hiv ) - acquired immunodeficiency syndrome associated with chronic hepatitis c virus ( hcv ) - related hepatopathy was suspected and diagnosed . 
la biopsia ossea risult positiva per linfoma non - hodgkuna rmn di controllo eseguita ad un mese dimostr un ingrandimento delle lesioni che si estendevano ora alle regioni parietale ed insulo - frontale destre e alla temporale dell altro lato . 
alla luce di un calo selettivo dei linfociti cd4 ( circa 90 ) con ridotto rapporto cd4 / cd8 ( 01 ) venne fatta sospettata e quindi confermata la diagnosi di sindrome da immunodeficienza acquisita da hiv con epatopatia cronica hcv correlata . 
fluid - attenuated inversion recovery ( flair ) , t1 - weighted and diffusion - weighted ( dw ) images and apparent diffusion coefficient ( adc ) maps show an area ( arrows ) of reduced adc values in the anterior portion of the right occipitotemporal lesion , consistent with active progression front not seen in the previous examination ( not shown )  . 
la rmn celebrale eseguita 12 giorni dopo mostr plurime aree di alterato segnale in sede iuxta - corticale , ipointense in t1 ed iperintense in t2 , con aspetto a stampo per coinvolgimento delle fibre ad u in sede fronto - occipitale , prive di effetto massa ed areagenti al mdc . 
anche in questo caso le immagini pesate in diffusione risultarono di scarso significato . discussione lo stato di immunodepressione predispone allinsorgenza di infezioni opportunistiche del sistema nervoso centrale ( snc ) , quali lencefalite da cytomegalovirus , le infezioni da toxoplasma e da jc virus . 
tra queste il quadro rm della pml ben conosciuto , caratterizzato da lesioni della sostanza bianca multifocali , povere di elementi specifici [ 79 ] tanto che la diagnosi rimane basata sul riconoscimento mediante pcr delle sequenze virali nel liquor . gli studi neuropatologici identificano allinterno delle lesioni aree con differenti stadi di demielinizzazione della sostanza bianca : le lesioni pi datate cos come la porzione fig . 
3 paziente 3 : immagini flair , t1w , dwi e mappe adc del primo esame e dei successivi controlli a 12 e 16 mesi ; le molteplici lesioni della sostanza bianca sottocorticale non mostrano significativi margini di accrescimento e le immagini evidenziano sfumati segni di atrofia cerebrale . region and occipital region bilaterally . 
brain mri , performed 12 days later , showed multiple areas of altered signal in the juxtacortical region , hypointense on t1 and hyperintense on t2 images , with a punched - out appearance due to involvement of u - shaped fibres in the frontooccipital region , with no mass effect and no reaction to contrast mediu since the findings were highly suggestive of pml , a lumbar puncture was performed and tested positive for jcv . 
diffusion - weighted images ( dwis ) were of little significance . case 4 ad , a 55 - year - old hiv - positive man with left pml - related hemiplegia , was hospitalised due to onset of recurrent seizures that failed to respond to medication . 
brain mri showed extensive signal alteration in the white matter of the semioval centre , with thinning of the corpus callosuin this case , too , dwis were of little significance . baseline 7th day 22th day discussion fig . 
accordingly , the diagnosis of pml is based on identification by pcr of viral sequences in the csf . neuropathological studies have detected some areas within the lesions with different stages of white matter demyelination : older lesions and the central portion of more recent ones are characterised by almost total breakdown of the myelin sheath and by axonal damage , with an increase in extracellular space ; conversely , the most medial portion of lesions consists of oligodendrocytes with nuclear inclusions and partially destroyed myelin , with relative sparing of axons . despite histopathological heterogeneity , mri signal alterations that characterise pml in conventional sequences seem to show homogeneous low signal intensity on t1weighted images and hyperintensity on t2 - weighted images , irrespective of the lesions progression and as a consequence of the altered ratio between myelin content and water . 
some authors have recently reported that analysis of the evolution of a lesion with diffusion - weighted mri can supply important new semiological elements [ 3 , 6 ]  . 
comparison of dwi sequences and adc maps shows different signal behaviour between the lesion centre and the extending margin particular , dwi presents some signal features that are similar to flair , i.e. 
margin hyperintensity and central hypointensity . on adc maps , signal intensity is elevated in the central area ( values : 1 , 710125 ) whereas at the lesion margins , it seems to further distinguish the more recent portion ( growth margin ) with reduced water diffusibility compatible with cytotoxic oedema ( values : 561135 ) from less recent portions that have intermediate values ( 940135 )  . 
in particular , adc maps show an elevated signal in the centre of the lesion and low signal intensity at the edge of the lesions expansion towards the white matter . 
 [ 10 ] correlated lesion stage with dwi / adc signal and interpreted these findings as both increased water diffusibility in the central areas of glial repair and reduced diffusibility because of cytotoxic oedema within active viral infectious areas . 
 [ 3 ] also described this peculiar pattern of development of pml using diffusion tensor imaging ( dti ) without , however , considering the relationship between findings obtained with dwi sequences and adc maps . our study confirms signal heterogeneity of lesions on adc maps : although lacking in neuropathological correlation , close comparison of lesions serially and temporally suggests that the alterations detected on adc maps strictly centrale delle lesioni recenti sono caratterizzate da una quasi totale perdita di mielina e da un danno assonale con allargamento degli spazi extracellulari ; la parte pi mediale delle lesioni invece sembra costituita da oligodendrociti con inclusioni intranucleari e mielina parzialmente distrutta , con relativo risparmio degli assoni . 
 a dispetto della eterogeneit istopatologica , le alterazioni di segnale rm che caratterizzano la pml nelle sequenze standard appaiono omogeneamente ipointense in t1 ed iperintense in t2 indipendentemente dalla fase evolutiva della lesione , come conseguenza dellalterato rapporto tra contenuto in mielina e acqua . alcuni autori hanno recentemente segnalato che nella pml le sequenze pesate in diffusione possono fornire nuovi ed utili elementi semeiologici [ 3 , 6 ]  . 
il confronto delle immagini rm nei pazienti con un decorso aggressivo della malattia evidenzia un progressivo aumento delle dimensioni delle lesioni che risultano sostanzialmente omogeneamente iperintense in t2 ed ipointense in t1 . 
nelle mappe adc il segnale elevato nella porzione centrale ( valori : 1710125 ) mentre , in corrispondenza dei margini delle lesioni , sembra ulteriormente differenziare la porzione pi recente ( margine di accrescimento ) , caratterizzata da ridotti valori di diffusibilit dellacqua compatibili con edema citotossico ( valori : 561135 ) , da porzioni meno recenti che presentano valori intermedi ( 940135 )  . 
 [ 10 ] hanno correlato lo stadio della lesione con il segnale in dwi / adc e hanno interpretato tali reperti come unaumentata diffusibilit dellacqua nelle aree centrali di riparazione gliotica e come una ridotta diffusibilit per presenza di edema citotossico nelle aree di infezione attiva del virus . 
 [ 3 ] hanno sottolineato questo caratteristico sviluppo della pml , grazie allutilizzo del tensore ( dti ) , senza porre per attenzione al confronto tra i risultati ottenuti con le sequenze in diffusione e le mappe adc . il nostro studio conferma leterogeneit di segnale delle lesioni nelle mappe adc : il confronto seriato e temporalmente ravvicinato delle lesioni , sebbene privo di correlato neuropatologico , sembra dimostrare che le alterazioni rilevate nelle mappe adc corrispondono strettamente alla maturit delle lesioni . 
in particular , the areas of lesion extension , initially characterised by a low adc signal ( cytotoxic oedema ) will evolve at subsequent examinations into high adc signal areas typical of vasogenic oedema and glial repair , and new cytolysis regions will emerge peripherally to the previous ones . 
these dwi features , which characterise the acute stages of the disease , were not detectable in patients 3 and 4 , whose lesions progressed very little over time , with a prevalence of atrophic degeneration . 
in these cases , the progression front was probably too tenuous , if not absent , and could not , therefore , be detected on mri . our results highlight the importance of all information provided by dwi and related adc maps and , together with previous findings , introduce new , early semiological and neuroradiological elements that are specific for this disease . mente caratterizzate da basso segnale adc ( edema citotossico ) evolvono , nei successivi controlli , ad aree ad alto segnale adc tipico delledema vasogenico e della riparazione gliotica e che nuove aree di citolisi si aggiungono perifericamente alle precedenti . 
questi aspetti nelle sequenze in diffusione , che caratterizzano le fasi acute della malattia , non sembrano essere evidenti nei pazienti 3 e 4 , in cui le lesioni presentano una lenta evolutivit , con prevalenza di aspetti degenerativo - atrofici . 
in questi casi il fronte di accrescimento troppo sfumato , se non assente , quindi non apprezzabile nelle immagini rmn . i nostri risultati confermano limportanza delle informazioni ottenibili con la sequenza pesata in diffusione e le relative mappe adc e , assieme alle segnalazioni gi presenti in letteratura , introducono un elemento semeiologico neuroradiologico nuovo , precoce e specifico di questa patologia . conclusions conclusioni diffusion - weighted sequences add new semiological elements in the neuroradiological diagnosis of pml and seem to correctly identify disease progression , which is not otherwise detectable on conventional sequences . 
further studies are needed to assess the clinical impact and reliability of these new elements in evaluating response to treatment in future clinical and pharmacological trials . le sequenze pesate in diffusione aggiungono nuovi elementi semeiologici nella diagnosi neuroradiologica di pml e sembrano in grado di riconoscere il fronte di progressione della malattia altrimenti non apprezzabile nelle sequenze convenzionali . 
fugazzola1 1vascular and interventional radiology , department of radiology , 2vascular surgery , 3anesthesiology , university of insubria , viale borri 57 , i - 21100 varese , italy correspondence to : d . 
we selected 19 patients ( mean age 66.3 years , range 4580 ) : five with complete occlusion of the infrarenal aorta and both common iliac arteries ( cias ) , four of which were associated with occlusion of the external iliac arteries ( eias ) ; three with complete occlusion and three with severe stenosis of the distal aorta with occlusion or stenosis of the cias and eias ; and eight with focal severe stenosis of the infrarenal aorta . 
immediate technical success was 94.7% ( 18 / 19 cases )  . we observed two cases of distal embolism treated with thrombolysis , one case of mild renal failure and one case of transient angina abdominis . 
during the follow - up ( mean 19.6 months ; range 648 ) , 2 / 18 ( 11.1% ) occlusions of an iliac stent occurred 1 and 3 months after the procedure ( treated with local intra - arterial thrombolysis )  . 
direct stenting is a feasible and safe option for the treatment of infrarenal abdominal aortic steno - occlusions , especially in patients at high surgical risk , with good early and late clinical results . key words aorta stent endovascular riassunto obiettivo . 
abbiamo selezionato 19 pazienti ( et media 66 , 3 anni , range 4580 ) : 5 con occlusione completa dellaorta addominale sottorenale e delle arterie iliache comuni ( aics ) , associata in 4 casi ad occlusione delle arterie iliache esterne ( aies ) ; 3 occlusioni e 3 stenosi severe dellaorta distale con occlusione o stenosi delle aics e aies ; 8 stenosi focali severe dellaorta sottorenale . 
si sono verificate 2 embolie distali , 1 insufficienza renale moderata e 1 angina abdominis transitoria . durante il follow - up ( medio 19 , 6 mese ; range 648 ) , abbiamo osservato 2 / 18 ( 11 , 1% ) occlusioni di uno stent iliaco a 1 e 3 mesi dalla procedure ( trattate con fibrinolisi loco - regionale )  . 
soprattutto in pazienti ad elevato rischio chirurgico , con buoni risultati a breve e medio termine . parole chiave aorta stent endovascolare introduction introduzione infrarenal aortic occlusive disease is an uncommon consequence of atherosclerosis and mainly affects middleaged women with dyslipidaemia and a history of smoking [ 1 ]  . 
usual management involves endarterectomy for focal lesions or surgical bypass for more extensive aortoiliac disease and is characterised by established and favourable long - term results ( 90% 5 - year and 75% 10year patency rates ) [ 2 , 3 ] even if burdened by a nonnegla malattia occlusiva dellaorta sottorenale una infrequente sequela dellaterosclerosi e colpisce soprattutto soggetti di sesso femminile di et media , con dislipidemia e anamnesi di tabagismo [ 1 ]  . 
il trattamento convenzionale prevede lendoarterectomia , per le lesioni focali , o il by - pass chirurgico per la patologia aorto - iliaca estesa , ed caratterizzato da buoni risultati a lungo termine ( perviet del 90% a 5 anni e del 75% a 10 anni ) [ 2 , 3 ] , anche se gravato da d . 
its limited invasiveness , lower morbidity and costs in comparison to surgery and favourable early and long - term results [ 712 ] have subsequently established the role of pta as the first - choice strategy in the management of focal infrarenal aortic stenosis [ 11 ]  . in most literature reports , indications for stenting have been unsuccessful or complicated pta , such as elastic recoil of the wall and stenosing or occluding flap ( secondary stenting ) [ 4 , 5 , 1322 ]  . 
subsequent data on primary or direct stenting ( stenting with or without balloon predilation , respectively ) in the elective management of focal lesions [ 4 , 13 , 1727 ] , infrarenal aortic occlusions [ 13 , 2528 ] or aortoiliac lesions [ 20 , 23 , 26 , 27 ] were more limited and conflicting . 
the aim of this paper is to present our experience in the elective management of steno - occlusive abdominal aortic disease with direct stenting . materials and methods over the past 4 years , we treated 19 patients ( 12 men and seven women ; mean age 66.3 years , range 4580 ) with leriche syndrome ( claudication and femoral pulselessness associated in some cases with impotence ) who were unfit for open conventional repair owing to poor cardiorespiratory function . 
five patients had complete occlusion of the infrarenal aorta and both common iliac arteries ( cia ) [ in four cases associated with bilateral occlusion of the external iliac arteries ( eia ) ; in three cases the aorta was occluded immediately below the origin of renal artery and in two cases at level of the middle aorta ; in four cases , a rich collateral circulation recanalised the common femoral arteries and in one case the eias ]  . 
eight cases had severe focal stenosis ( > 70% ) of the infrarenal aorta due to a calcified eccentric plaque , which was ulcerated in two . none of the patients had a history of previous surgical or endovascular intervention in the aortic or iliac vessels . risk factors included smoking ( n = 11 ) , hypertension ( n = 9 ) , cardiac disease ( n = 12 ) , hyperlipidaemia ( n = 6 ) , diabetes ( n = 4 ) and pulmonary disease ( n = 7 )  . 
symptoms were classified according to the classification of the society of vascular surgery and the international society of cardiovascular surgery ( svs / iscs ) : four patients were class 2 ( moderate claudication ) , eight were class 3 ( severe claudication ) and seven were class 4 ( ischaemic rest pain )  . 
 preprocedural assessment was performed in all patients with multislice computed tomography ( ct ) angiography ( mscta ) ( lightspeedplus , ge , milwaukee , wi , usa e aquilion 64 , toshiba , tokio , japan ) , with scans obtained at baseline and in un tasso non trascurabile di complicanze maggiori ( 5%10% dei casi ) [ 2 , 3 ]  . dalle prime esperienze riportate in letteratura a partire dal 1980 , riguardanti il trattamento percutaneo di stenosi focali dellaorta sottorenale mediante angioplastica ( pta ) in pazienti ad elevato rischio chirurgico [ 46 ] , lapproccio endovascolare stato proposto come alternativa alla chirurgia . 
la mini - invasivit , la riduzione della morbidit e dei costi rispetto alla chirurgia e i buoni risultati immediati e a distanza [ 712 ] hanno consolidato il ruolo della pta come approccio di prima scelta nel trattamento delle stenosi focali dellaorta sottorenale [ 11 ]  . in letteratura , nella maggior parte delle casistiche , le indicazione allo stent sono state linsuccesso o le complicanze della pta , quali il ritorno elastico di parete e il flap stenosante o occludente ( secondary stenting ) [ 4 , 5 , 1322 ]  . successivamente sono stati pubblicati dati pi limitati e contraddittori relativi al primary stenting o al direct stenting ( stenting rispettivamente con o senza pre - dilatazione ) nel trattamento endovascolare delle lesioni focali [ 4 , 13 , 1727 ] , e al trattamento delle occlusioni complete dellaorta sottorenale [ 2226 ] e delle lesioni aorto - iliache [ 20 , 23 , 26 , 27 ]  . 
scopo di questo lavoro presentare la nostra esperienza nel trattamento endovascolare della malattia stenoocclusiva dellaorta sottorenale mediante direct stenting . materiali e metodi negli ultimi 4 anni abbiamo selezionato 19 pazienti ( 12 maschi e 7 femmine ; et media 66 , 3 anni , range 4580 ) , sintomatici per sindrome di leriche ( claudicatio e assenza dei polsi femorali , associati in alcuni casi a impotenza ) , ad elevato rischio chirurgico per patologie cardio - respiratorie . 
i pazienti erano portatori delle seguenti lesioni : 5 occlusioni complete dellaorta sottorenale e di entrambe le aics in 4 casi associate allocclusione bilaterale delle aies , in 3 casi laorta era occlusa subito a valle dellorigine delle arterie renali e in 2 casi a livello del tratto intermedio , in 4 casi ricchi circoli collaterali ricanalizzavano le arterie femorali comuni ( afcs ) e in 1 caso le aies ; 3 occlusioni complete e 3 stenosi severe ( > 70% ) dellaorta distale con occlusione bilaterale delle aics e delle aies ; 8 stenosi focali severe ( > 70% ) dellaorta sottorenale da placca eccentrica calcifica , in 2 casi ulcerata . 
nessun paziente era stato sottoposto in precedenza a trattamenti chirurgici o endovascolari a livello aorto - ilaco . i pazienti presentavano i seguenti fattori di rischio : tabagismo ( n = 11 ) , ipertensione ( n = 9 ) , patologie cardiache ( n = 12 ) , iperlipidemia ( n = 6 ) , diabete ( n = 4 ) e patologie polmonari ( n = 7 )  . 
i pazienti sono stati classificati in base alla severit dei sintomi in accordo con la classificazione svs / iscvs ( society of vascular surgery and international society of cardiovascular surgery ) : 4 pazienti categoria 2 ( claudicatio moderata ) , 8 categoria 3 ( claudicatio severa ) e 7 categoria 4 ( dolore a riposo )  . la valutazione pre - trattamento stata effettuata in tutti i d . 
all patients underwent cardiac and pulmonary monitoring during the procedure and received antithrombotic prophylaxis consisting of heparin ( 5 , 000 iu ) followed by light - molecular - weight heparin in prophylactic doses for 30 days after the procedure and life - long antiplatelet or anticoagulant therapy . 
procedures were performed in 14 cases in the vascular suite under local anaesthesia ( 10 ml 2% carbocaine at the site of arterial access ) and in five cases ( all total occlusions of the infrarenal aorta ) in the operating theatre with surgical stand - by . all patients underwent percutaneous access of the common femoral artery using a 5 - f introducer sheath ( cordis , miami , fl , usa ) and a 0.035 ( 300 - cm ) hydrophilic curved guidewire ( glidewire , terumo , tokyo , japan ) unilaterally in eight cases with focal stenosis and bilaterally in the remaining cases . 
before stent implantation , the hydrophilic guidewire was exchanged with a 0.035 ( 300cm ) stiff wire ( amplatz , boston scientific , ratingen , germany ) , and the lesion was crossed with a 12 - f , 30 - cm - long sheath ( cook , bloomington , in , usa ) in order to enable the protected advancement of the hand - crimped stent and thus avoid dislodgement . 
the stents were first dilated to the minimum diameter enabling sealing to the vessel wall ( 12 - mm powerflex , cordis , miami ) and progression along the 12 - f sheath . postdilation by in - stent pta [ using balloons with a diameter ranging between 16 and 18 mm ( powerflex , cordis , miami ) ] was then performed in order to achieve an adequate vessel diameter and sufficient stent shortening , stopping the postdilation when the patient reported pa for lesions involving the bifurcation and the iliac vessels , direct kissing stenting of the cias was performed with self - expandable stents ( 1012 mm in diameter , 60 mm in length ) ( smart , cordis , miami )  . 
in tutti i casi durante la procedura stato effettuato il monitoraggio cardio - respiratorio ; stata inoltre effettuata la profilassi antitrombotica con somministrazione di eparina ( 5000 iu ) ; successivamente eparina a basso peso molecolare in dosi profilattiche per 30 giorni seguita da terapia antiaggregante o anticoagulante . 
le procedure sono state effettuate in 14 casi in sala angiografica in anestesia locale ( 10 ml di carbocaina 2% nel sito di accesso arterioso ) e in 5 casi ( tutti i pazienti con occlusione completa dellaorta sottorenale ) in sala operatoria con stand - by chirurgico . in tutti i pazienti stato effettuato un cateterismo percutaneo dellafc , utilizzando un introduttore vascolare 5 fr ( cordis , miami , usa ) e una guida idrofilica curva 0 , 035 ( glidewire terumo , tokyo , giappone ) , monolaterale in 8 casi con stenosi focale e bilaterale nei restanti casi . 
prima dello stenting la guida idrofilica stata sostituita con guida rigida 0 , 035 ( amplatz , boston scientific , ratingen , germania ) e le lesioni sono state superate con introduttore 12 fr lungo 30 cm ( cook , bloomington , in , usa ) , al fine di garantire lavanzamento protetto dello stent crimpato su pallone ed evitarne dislocazioni . 
gli stents sono stati dapprima dilatati al minimo diametro necessario a garantirne lancoraggio alla parete aortica ( 12 mm powerflex , cordis , miami , usa ) e la progressione lungo lintroduttore 12 fr . 
successivamente stata effettuata una pta intra - stent ( mediante palloni con diametro compreso tra 16 e 18 mm powerflex , cordis , miami , usa ) finalizzata a raggiungere un calibro sufficiente del vaso e a ottenere un adeguato accorciamento dello stent , arrestando la post - did . 
1a - f a 59 - year - old patient with a complete occlusion of the infrarenal aorta and both common iliac arteries ( cias ) and external iliac arteries ( eias )  . 
a preprocedural multislice computed tomography angiography ( mscta ) , volume rendering ( vr ) reconstruction ; mscta clearly shows the collateral circulation that , through deep iliac circumflex arteries ( black arrows ) and inferior epigastric arteries ( white arrows ) allows recanalisation of the common femoral arteries . 
e , f mscta , maximum intensity projection ( mip ) ( e ) and vr ( f ) reconstruction 1 year after the procedure confirms the patency of the aorta and iliac arteries . fig 1a - f paziente di 59 anni con occlusione completa dellaorta sottorenale e di entrambe le aics e aies . 
a atcms pre - procedura , ricostruzioni vr : occlusione completa dellaorta sottorenale con circoli collaterali che , attraverso le arterie circonflesse iliache profonde ( frecce nere ) e epigastriche superficiali ( frecce bianche ) ricanalizzano le arterie femorali comuni ; b angiografia pre - procedura espletata dopo superamento dellocclusione ; c direct stenting con posizionamento di 2 stents espandibili su pallone in aorta ( frecce bianche ) e di 3 stents autoespandibili in entrambi gli assi iliaci ( frecce nere ) ; d langiografia espletata dopo il trattamento , mostra la completa ricanalizzazione dellaorta sottorenale , delle aics e aies . 
2a - c a 70 - year - old patient with a complete occlusion of the infrarenal aorta and both common iliac arteries ( cias ) and external iliac arteries ( eias )  . 
a preprocedural multislice computed tomograph angiography ( mscta ) , curved multiplanar reconstruction ( mpr ) : occlusion of the abdominal aorta just below the origin of renal arteries ( bilaterally 2 renal arteries are present )  . 
c angiography performed after the direct stenting shows complete recanalisation of the infrarenal aorta , cias and eias and patency of renal arteries . fig 2a - c paziente di 70 anni con occlusione completa dellaorta sottorenale e di entrambe le aics e aies ; a angio - tcms , ricostruzioni mpr curve dellorigine delle arterie renali ( bilateralmente sono presenti 2 arterie renali ) ; b angiografia pre - procedura espletata dopo superamento dellocclusione , con guida angiografica che guadagna il lume vero dellaorta ; c angiografia espletata dopo il direct stenting che mostra la completa ricanalizzazione dellaorta sottorenale , delle aics e delle aies e la perviet delle arterie renali . lesions involving the eias , two additional stents ( 9 - mm diameter , 60 - mm long ) ( smart , cordis , miami ) were deployed to completely reconstruct the iliac vessels . 
in all nine cases in whom the lesion involved the origin of the inferior mesenteric artery ( which was patent before the procedure in 4 / 9 cases ) , the stent covered its ostium . immediate postprocedure results were assessed with angiography ( anteroposterior and lateral views ) in order to assess stent patency and deployment as well as the lumen of the target vessel , and angiograms of the distal leg vessels were also obtained to exclude complications such as distal embolis follow - up was performed with colour - doppler ultrasound ( cdus ) and clinical assessment 1 , 3 , 6 and 12 months after the procedure and yearly thereafter . 
1d , 2c latazione quando il paziente riferiva la comparsa di dolore . per le lesioni che coinvolgevano la biforcazione aortica e i vasi iliaci stato effettuato un direct kissing stenting delle aics , mediante stents autoespandibili ( diametro 1012 mm , lunghezza 60 mm ) ( smart , cordis , miami , usa )  . 
in 5 pazienti con lesioni che coinvolgevano le aies , sono stati embricati altri 2 stents ( diametro 9 mm , lunghezza 60 mm ) ( smart , cordis , miami , usa ) per completare la ricostruzione degli assi iliaci . 
nei 9 casi in cui la lesione coinvolgeva lemergenza dellarteria mesenterica inferiore ( che risultava pervia prima della procedura in 4 / 9 casi ) lostio stato coperto dallo stent . il risultato immediato stato controllato mediante angiografia ( in proiezione antero - posteriore e latero - laterale ) al fine di valutare lapertura e la perviet degli stents e il calibro vasale raggiunto ; stata inoltre effettuata unangiografia degli arti inferiori per escludere complicanze emboliche distali . 
in nine cases , the ostium of the inferior mesenteric artery was covered by the stent , with ensuing total occlusion of the artery in all cases ( in five patients , the artery was already occluded ) ; no patient experienced major complications due to inferior mesenteric artery occlusion with the exception of one case of transient angina abdominis . patients were discharged after a mean of 3.2 ( range 37 ) days . 
during the follow - up performed in the 18 patients achieving immediate procedural success ( mean 19.6 months ; range 648 ) , 2 / 18 ( 11.1% ) occlusions of the iliac stent occurred 1 and 3 months after the procedure . 
 discussion endovascular treatment of infrarenal aortic stenosis has been proposed [ 28 , 29 ] as a viable alternative to surgical revascularisation since the 1980s , and data available have established the safety and effectiveness of pta , with an 85% primary and a 90% secondary patency rate [ 712 ] together with a low ( 3% ) risk of major complications , such as vessel - wall rupture and distal and visceral embolism [ 21 ]  . 
on the other hand , data on aortic stenting mainly focus on its use for the management of unsuccessful or complicated pta procedures [ 4 , 5 , 1318 , 23 , 30 , 31 ]  . primary or direct stenting has been proposed as a result of the favourable results obtained in the iliac arteries , including its higher patency rates in comparison with pta [ 6 , 32 ] and has been employed selectively in complex stenotic lesions ( ulcerated , eccentric , irregular and / or calcific plaques ) [ 4 , 13 , 1727 ] and , more rarely , in total occlusions [ 20 , 2326 ]  . the rationale for direct stenting is based on the frequent early post - pta elastic recoil due to the extensive presence of elastic fibres in the aortic wall [ 13 ] and on the risk of rupture due to the large diameter of the aorta , according to the laplace law [ 19 ] ; the more uniform distribution of radial forces during stenting should decrease the risk of rupture in comparison to balloon pta [ 20 , 22 , 24 ]  . 
in un caso con occlusione completa dellaorta sottorenale e di entrambe le aics e aies non stato possibile valicare locclusione , nonostante plurimi tentativi retrogradi e anterogradi e il paziente stato trattato , durante la stessa seduta con by - pass axillo - bifemorale . non si sono verificate rotture di arteria ; abbiamo osservato 2 / 18 ( 11 , 1% ) embolie distali , trattate con successo mediante fibrinolisi loco - regionale e 1 lieve insufficienza renale dovuta a microembolia a livello dellarteria renale destra ( in questo caso lecd ha dimostrato una ridotta perfusione del parenchima renale )  . 
in 9 casi lostio dellarteria mesenterica inferiore stato coperto dallo stent con conseguente occlusione dellarteria in tutti i casi ( in 5 / 9 pazienti larteria era gi precedentemente occlusa ) ; non abbiamo osservato complicanze severe legate allocclusione dellarteria mesenterica inferiore con eccezione di una angina abdominis transitoria . 
peraltro i dati riguardanti lo stenting sono per la maggior parte focalizzati sul suo utilizzo nelle complicanze e negli insuccessi della pta [ 4 , 5 , 1318 , 23 , 30 , 31 ]  . lo stenting , primario o diretto , stato proposto alla luce dei favorevoli risultati ottenuti a livello iliaco con maggiori tassi di perviet rispetto alla sola pta [ 6 , 32 ] ed stato utilizzato di prima intenzione nelle lesioni stenosanti complesse ( placche ulcerate , eccentriche , irregolari e / o calcifiche ) [ 4 , 13 , 1727 ] e pi raramente nelle occlusioni complete [ 20 , 2326 ]  . il razionale del direct stenting basato sullalta frequenza del ritorno elastico di parete post - pta , dovuto allelevata presenza di fibre elastiche a livello della parete aortica [ 13 ] , e sul rischio di rottura dovuto al grosso calibro dellaorta , in accordo con la legge di laplace , [ 19 ] ; la pi uniforme distribuzione delle forze di dilatazione radiale durante lo stenting potrebbe diminuire il rischio di rottura rispetto alla sola dilatazione con pallone [ 20 , 22 , 24 ]  . 
inoltre , il posizionamento dello stent senza pre - dilatazione ( direct stenting ) , metodica applicata in questo studio e in alcuni altri riportati in letteratura , riduce il rischio di embolizzad . 
in our study , at an overall average follow - up of 17.4 ( range 148 ) months , we observed two occlusions ( 11.1% ) successfully treated with thrombolysis and pta . our choice of a balloon - expandable stent for aortic lesions is based on its superior radial force and the fact that it can be further dilated after the initial expansion in order to achieve a haemodynamically satisfying diameter [ 33 ]  . dilatation must be carefully guided by the patients symptoms , as the occurrence of pain during dilation is mostly due to the initial rupture of the intima and media . 
moreover , it is well known that balloon - expandable stents enable a quicker , more precise and accurate deployment than self - expandable stents given their reproducible shortening [ 24 ]  . 
to date , the availability of large - size stents ( with diameters up to 25 mm ) enables the management of a larger number of patients whereas in the past , only subjects with a small aorta could be treated [ 13 ]  . among the complications , the most feared aortic wall rupture is quite rare , and only sporadic cases have been reported after pta [ 34 ] and stenting [ 35 ]  . 
other reported complications , excluding those at the access site due to large diameter of the devices , may include distal or visceral embolisation [ 13 , 20 , 21 , 27 ]  . 
in any case , a careful preprocedural evaluation is of crucial importance in order to assess the patency of all relevant splanchnic vessels ( coeliac trunk , superior mesenteric artery , hypogastric arteries )  . among the causes of late clinical failure , with recurzione distale [ 1927 ]  . 
inoltre , la forza radiale dello stent in acciaio medicale consente una dilatazione uniforme e simmetrica della parete arteriosa , anche in vasi calcifici , evitando , soprattutto in caso di lesioni eccentriche , che la dilatazione interessi solo la porzione sana della parete . stato riportato il trattamento mediante primary o direct stenting dellaorta addominale in circa 100 casi ( nel 75% si trattava di stenosi focali ) con un successo clinico del 96% , definito come risoluzione o miglioramento dei sintomi , e come risultato emodinamico , e con tassi di perviet primaria del 90% e secondaria del 100% [ 4 , 13 , 1927 ]  . nella nostra casistica abbiamo ottenuto il successo tecnico in 18 / 19 casi ( 94 , 7% )  . 
nel nostro studio ad un follow - up medio di 17 , 4 mesi ( range 148 ) abbiamo osservato 2 occlusioni ( 11 , 1% ) di stents trattate con successo mediante fibrinolisi loco - regionale e pta . la nostra scelta di stents espandibili su pallone per le lesioni aortiche basato sulla loro superiore forza radiale e sul fatto che possono essere ulteriormente dilatati dopo lespansione iniziale , al fine di raggiungere un calibro del vaso emodinamicamente significativo [ 33 ]  . 
attualmente la disponibilit di stents di grosso calibro ( con diametro fino a 25 mm ) permette il trattamento di un maggior numero di pazienti , mentre in passato potevano essere sottoposti a stenting solo pazienti con small aorta [ 13 ]  . tra le complicanze , la pi temuta la rottura della parete aortica che in realt piuttosto rara e sono riportati in letteratura solo casi sporadici dopo pta [ 34 ] o stenting [ 35 ]  . inoltre , attualmente tale complicanza gestibile per via endovascolare con stents ricoperti . 
inoltre nel bypass chirurgico larteria mesenterica inferiore quasi sempre sacrificata , con un 2% di incidenza di ischemia intestinale [ 36 ]  . nella nostra esperienza abbiamo osservato solo 1 caso di angina abdominis transitoria . 
however , in - stent neointimal hyperplasia is less frequent in the aorta than in other vascular districts , as this is a high - flow vessel [ 1 ]  . 
accordingly , in most cases , restenotic lesions can be treated with a percutaneous approach , with secondary patency rates approaching 100% [ 13 , 23 , 27 ]  . 
such favourable results of endovascular treatment of aortic atherosclerotic occlusive disease are complemented by its advantages over open surgical revascularisation , basically due to its limited invasiveness , avoidance of general anaesthesia and use of laparotomy , with the consequent reductions in mortality and morbidity [ 19 ]  . 
similarly , the endovascular approach does not interfere with sexual function [ 26 ] , which , especially in men , may be compromised in up to 30% of cases after surgery [ 37 ]  . finally , the endovascular strategy does not preclude open surgical management in case of procedural failure or disease progression and , for total occlusions of the aortoiliac vessels , endovascular recanalisation of the aorta and even only one of the two iliac vessels may reduce the invasiveness of the subsequent surgical procedure ( femorofemoral crossover instead of aortobifemoral bypass )  . in conclusion , on the basis of the present study and the current literature , endovascular treatment , and in particular , direct stenting , may be considered the treatment of choice for steno - occlusive lesions of the abdominal aorta , as it provides excellent early and late clinical results with very low complication rates . 
the treatment of total occlusions of the abdominal aorta and lesions involving the bifurcation and the iliac vessels is feasible and safe but warrants additional studies , with larger series and longer follow - up . tra le cause di insuccesso clinico a distanza , con recidiva o peggioramento dei sintomi , oltre alla progressione prossimale o distale della patologia aterosclerotica [ 19 , 20 ] o alla insufficiente espansione dello stent [ 18 ] , va ricordata liperplasia intimale , la quale pu causare , quando determina una stenosi critica , anche locclusione trombotica dello stent [ 13 , 20 , 23 , 27 ]  . 
la maggior parte dei casi di restenosi pu comunque essere trattata con approccio percutaneo con tassi di perviet secondaria che raggiungono il 100% [ 13 , 23 , 27 ]  . tali favorevoli risultati del trattamento endovascolare nella patologia aterosclerotica occlusiva dellaorta addominale sono supportati anche dai vantaggi nei confronti dellapproccio chirurgico , legati alla minore invasivit e alla possibilit di evitare lanestesia generale con conseguente riduzione della morbidit e mortalit [ 19 ]  . 
peraltro lapproccio endovascolare non interferisce con la funzione sessuale [ 26 ] la quale , sopratutto nei maschi pu essere compromessa in pi del 30% dei casi dopo chirurgia [ 37 ]  . infine , la strategia endovascolare non preclude il trattamento chirurgico in caso di insuccesso o di progressione della patologia e , per le occlusioni complete dellaorta e delle arterie iliache , la ricanalizzazione dellaorta e anche di un solo asse iliaco , pu ridurre linvasivit della procedura chirurgica ( cross - over femoro - femorale anzich by - pass aorto - bifemorale )  . in conclusione , sulla base dei risultati di questo studio e dei dati della letteratura , il trattamento endovascolare , e in particolare il direct stenting , pu essere considerato la terapia di prima scelta per la patologia steno - occlusiva dellaorta addominale , con buoni risultati clinici immediati e a medio termine , con bassi tassi di complicanze . 
fugazzola1 1vascular and interventional radiology , department of radiology , 2vascular surgery , 3surgery , 4anesthesiology , university of insubria , viale borri 57 , i - 21100 varese , italy correspondence to : d . 
in 23 haemodynamically stable patients , computed tomography ( ct ) angiography was performed before treatment , and aaa exclusion was carried out as an urgent procedure ; 15 patients with haemorrhagic shock were examined by ultrasound ( us ) only in the emergency room whereas the procedure was carried out in emergency and planned using angiography . 
endovascular treatment of aaas is a good therapeutic alternative even in urgency and emergency conditions where correct planning ensures technical results comparable with those obtained under elective conditions . key words abdominal aortic aneurysm rupture endovascular treatment stent - grafts riassunto obiettivo . 
in 23 pazienti , emodinamicamente stabili , stata eseguita unangio - tc pre - trattamento e la procedura stata effettuata in urgenza ; 15 pazienti , in shock emorragico , sono stati valutati con la sola ecografia e la procedura stata effettuata in emergenza e pianificata mediante angiografia . 
il trattamento endovascolare una valida alternativa terapeutica per gli aaa anche in urgenza e emergenza , dove un corretto planning consente di ottenere risultati tecnici comparabili a quelli in elezione . parole chiave aneurisma aorta addominale rottura trattamento endovascolare stent - grafts d . 
although significant progress has been made in the fields of diagnosis , surgery and anaesthesiology , mortality among patients with aaa rupture who arrive at the hospital alive is 45%70% [ 2 ]  . 
since 1990 , the year of the first aortic stentgraft implanted by parodi , an alternative treatment , which is less invasive especially for patients at high surgical risk , has emerged [ 3 ]  . 
over the last decade , elective endovascular treatment of aaas has continuously spread , with shortand middle - term results comparable , according to some authors , to open surgery [ 4 ]  . 
improvements in devices and growing experience have led to suggestions for the use of endovascular treatment instead of surgery even in emergency settings , with the aim of reducing mortality [ 5 ]  . 
we describe our centres experience in urgency and emergency endovascular treatment of aaas . le emergenze dellaorta addominale costituiscono la terza causa di morte nei paesi industrializzati e il 95% di queste legato alle rotture di aaa . 
nonostante importanti progressi in campo diagnostico , chirurgico e anestesiologico , la percentuale di mortalit tra i pazienti con rottura di aaa che arrivano vivi in ospedale del 45%70% [ 2 ]  . 
dal 1990 , data della prima endoprotesi aortica impiantata da parodi si aperta una nuova alternativa al trattamento degli aaa , meno invasiva specialmente nei pazienti ad alto rischio chirurgico [ 3 ]  . 
nel corso dellultimo decennio si assistito ad una costante diffusione del trattamento endovascolare degli aaa in elezione con buoni risultati a breve e medio termine , secondo alcuni , comparabili con lesperienza di chirurgia open [ 4 ]  . 
il perfezionamento dei devices e la crescente esperienza degli operatori ha consentito di proporre il trattamento endovascolare come alternativa terapeutica alla chirurgia , anche in emergenza , con lo scopo di ridurre la mortalit [ 5 ]  . 
questo lavoro si propone di presentare lesperienza del nostro centro nella gestione e nel trattamento endovascolare in urgenza e emergenza degli aaa . materials and methods materiali e metodi between july 2001 and october 2005 , 193 patients underwent aaa exclusion with stent - grafts at our centre . 
the patients presented with the following comorbidities : hypertension ( 19 cases ) , ischaemic cardiac disease ( 17 cases ) , chronic obstructive pulmonary disease ( 16 cases ) , chronic kidney failure ( five cases ) and diabetes ( five cases )  . 
on the basis of the severe comorbidities and urgency of the disease , 23 patients were classified american society of anesthesiology ( asa ) 4e ( urgent cases with severe systemic disease that is a constant threat to life ) whereas 15 patients with symptomatic aaa and thrombus fissure were classed asa 3e ( urgent cases with moderate or severe systemic disease with functional limitations )  . 
more specifically , the studies were conducted with multislice ct ( lightspeedplus , ge , milwaukee , wi , usa ; aquilion 64 , toshiba , tokyo , japan ) with unenhanced , arterialand venous - phase durante il periodo compreso tra luglio 2001 e ottobre 2005 , presso il nostro centro sono stati trattati 193 pazienti con endoprotesi per esclusione di aaa . 
i pazienti presentavano le seguenti comorbidit : ipertensione ( 19 casi ) ; cardiomiopatia ischemica ( 17 casi ) ; broncopneumopatia cronica ostruttiva ( 16 casi ) ; insuffucienza renale cronica ( 5 casi ) e diabete ( 5 casi )  . 
in relazione alle severe comorbidit e allurgenza della patologia , 23 pazienti sono stati classificati grado e4 di rischio operatorio ( pazienti trattati in urgenza con patologia sistemica severa in costante pericolo di vita ) in accordo con la classificazione della american society of anesthesiologist ( asa ) e 15 pazienti , con aaa sintomatico e fissurazione del trombo , grado e3 ( pazienti trattati in urgenza , con moderata o severa patologia sistemica limitante lattivit )  . 
pi specificatamente gli studi sono stati eseguiti con tc multistrato ( lightspeedplus , ge , milwaukee , usa ; aquilion 64 , toshiba , tokyo , giappone ) attraverso scansioni ottenute in condizioni basali , fase arteriosa , venosa e rid . 
b , c enhanced ct , arterial phase : haemorrhage in the mural thrombus with compression of the true lumen ( b , arrow ) and penetration of contrast medium into the thrombus ( c , arrow )  . 
b , c tc con mdc , fase arteriosa : lematoma del trombo causa compressione del vero lume ( b , freccia ) ; mdc penetra il trombo ( c , freccia )  . 
the venous - phase study is done to identify any increase in density of the retroperitoneal haematoma to determine whether it is fed ; in addition , leakage of contrast material is better visualised in this phase . 
in patients with haemorrhagic shock ( 15 / 38 patients ) , the diagnosis was established by ultrasonography ( us ) ( atl 5000 , philips medical systems , best , the netherlands ) performed in the emergency room , and the costruzioni mip ( maximum intensity projection ) e vr ( volume rendering )  . 
la fase venosa stata effettuata in relazione alla possibilit di individuare lincremento di densit dellematoma retroperitoneale per stabilire se rifornito ; inoltre lo stravaso attivo di mdc viene meglio evidenziato in fase venosa . 
nei casi di shock emorragico ( 15 / 38 pazienti ) , la diagnosi stata ottenuta con ecotomografia ( atl 5000 , philips medical systems , best , olanda ) eseguita in pronto soccorso e la procedura stata realizzata in emergenza efd . 
a , b computed tomography ( ct ) : a unenhanced phase ; b arterial phase : abdominal aortic aneurysm ( aaa ) rupture due to posterior sac tear resulting from conflict with the lumbar spine ( black arrow ) , with penetration of the contrast agent into the thrombus ( white arrow )  . 
a , b tc ( senza mdc : a ; fase arteriosa : b ) aaa rotto tamponato per lacerazione posteriore della sacca da conflitto con il rachide ( freccia nera ) ; mdc penetra il trombo ( freccia bianca )  . 
in these cases , evaluation of neck size and stent - graft selection was carried out by angiography with software allowing measurements starting from a precise calibre , such as that of the catheter , and using a ruled catheter to measure length . 
mean aneurysm diameter was 85 mm ( range 45120 mm ) , mean length of the proximal neck was 20 mm ( range 1030 mm ) and mean neck diameter was 25 mm ( range 1830 mm )  . 
in 21 patients , the aneurysm involved the abdominal aorta only ; in ten , both the common iliac arteries ; and in seven , the abdominal aorta and one common iliac artery . 
il diametro medio degli aneurismi era di 85 mm ( range 45120 mm ) , la lunghezza media del colletto prossimale di 20 mm ( range 1030 mm ) e il diametro medio dello stesso di 25 mm ( range 1830 mm )  . 
in 5 / 15 cases treated as emergencies , we used a catheter with a latex occlusive balloon ( equalizer , boston scientific , ratingen , germany ) ( diameter : 2733 mm ) placed in juxtarenal position with transfemoral percutaneous access because of the patient rapidly deteriorating haemodynamic status . 
in 2 / 5 cases , this allowed us to complete the procedure with positioning of a bifurcated stent - grathirty - two bifurcated stent - grafts [ 27 excluder ( gore , flagstaff , az , usa ) and five zenith ( cook , bloomington , in , usa ) ] and six aortouniiliac devices ( zenith ) were implanted . 
in selecting stent - grafts , we chose devices 23 mm larger than the diameter of the aneurysm neck and the calibre of the common iliac arteries for proximal and distal fixation , respectively . 
 our operating room is equipped with the following devices for the emergency / urgency treatment of aneurysms : two aortouniiliac kits with occluders ( diameters : 30 and 32 mm ) and four bifurcated endografts , including two for infrarenal fixation ( diameters : 28 and 30 mm with two leg measuring 12 cm and 14 cm in length ) and two endografts for suprarenal fixation ( diameters : 30 and 32 mm )  . 
endograft extensions are also available and are also interchangeable , if necessary . the main body of the device was introduced through the common femoral artery that had been isolated surgically . transfemoral access for placement of the contralateral leg of bifurcated devices was percutaneous in 29 patients and surgical in three owing to the small calibre of the iliofemoral axis . 
le procedure sono state espletate da un team di radiologi interventisti , chirurghi vascolari e anestesisti in sala operatoria con angiografo portatile . tutte le procedure sono state realizzate in anestesia generale . in 5 / 15 casi trattati in emergenza stato utilizzato un catetere fornito di pallone occlusore in lattice ( equalizer , boston scientific , ratingen , germania ) , con diametro di 2733 mm , posizionato in sede iuxta - renale mediante accesso percutaneo transfemorale poich le condizioni emodinamiche del paziente erano in rapido peggioramento allarrivo in sala operatoria . 
sono state impiantate 32 endoprotesi biforcate ( 27 excluder - gore , flagstaff , az , usa e 5 zenith - cook , bloomington , in , usa ) e 6 devices aorto - uni - iliaci ( zenith - cook , bloomington , in , usa )  . 
sono state adottate per la scelta dellendoprotesi dimensioni superiori di 23 mm rispetto al diametro del colletto dellaneurisma e al calibro delle arterie iliache comuni per lancoraggio rispettivamente prossimale e distale . presso il nostro centro , per il trattamento degli aneurismi in emergenza / urgenza sono disponibili in sala operatoria i seguenti device : 2 kit aorto - monoiliaci con rispettivo occlusore ( diametri 30 e 32 mm ) e 4 protesi biforcate , di cui 2 ad ancoraggio sottorenale ( diametri 28 e 30 cm con 2 bracci protesici lunghi 12 e 14 cm ) e 2 protesi ad ancoraggio sovrarenale ( diametri 30 e 32 mm con i rispettivi bracci protesici )  . 
laccesso transfemorale per il posizionamento del braccio protesico controlaterale del device biforcato stato percutaneo in 29 pazienti e chirurgico in 3 casi , in relazione al ridotto calibro dellasse iliaco - femorale . 
successivamente stata avanzata una guida superstiff 0 , 035 300 cm ( back - up meier , boston scientific , ratingen , germania ) e il corpo principale dellendoprotesi stato posizionato attraverso un introduttore da 18 f ( cook , bloomington , in , usa )  . 
in the 32 / 38 cases treated with bifurcated stent - grafts , the contralateral leg was positioned through a 12 - f introducer ( cook ) and a 0.035 - ( 185 - cm ) super - stiff guide ( back - up meier , boston scientific ) in the common femoral artery . 
use of a catheter with a low - pressure latex balloon ( diameter : 2733 mm ) ( equalizer , boston scientific ) allowed sealing of the endograft at the proximal and distal fixation sites and at the points of junction of the graft segments . 
in 6 / 38 patients , additional endovascular procedures on the iliac axis were necessary to advance the device [ percutaneous transluminal angioplasty ( pta ) in five cases , pta and stenting in one case ]  . 
nonionic isosmolar contrast material ( iodixanol , visipaque , amersham , saluggia , italy ) was administered to all patients ( range : 80160 ml , mean 100 ml )  . 
antithrombotic prophylaxis consisted of intraprocedural heparin ( 5 , 000 iu i.v. ) and low - molecularweight heparin in prophylactic doses for 30 days followed by antiaggregants or anticoagulants ( depending on the clinical data )  . 
an ultra - short term antibiotic prophylaxis was administered during induction of anaesthesia with the aim of achieving a reasonable concentration during endograft positioning ( vancomycin , abbott , latina , italy ; 1 g i.v. ) ; in patients with kidney failure or a history of intolerance , ciprofloxacin and cefazolin were used . 
in all patients , follow - up was performed with ct angiography according to the european collaborators on stent - graft techniques for abdominal aortic aneurysm repair ( eurostar ) protocol at 1 , 3 , 6 and 12 months and yearly thereafter [ 6 ]  . 
 trattati con device aorto - uni - iliaco ( zenith - cook , bloomington , in , usa ) , in 5 / 6 casi la procedura stata completata con il posizionamento di un dispositivo occlusore ( cook , bloomington , in , usa ) nellarteria iliaca comune controlaterale ; in 1 / 6 casi in urgenza la procedura stata completata con lutilizzo di spirali metalliche embolizzanti ( vortex - 35 , boston scientific , ratingen , germania , 78 mm ) nella arteria iliaca comune controlaterale steno - occlusa , al fine di preservare la perviet dellarteria iliaca interna . 
in 32 / 38 casi trattati con endoprotesi biforcata , la gamba controlaterale stata posizionata mediante introduttore 12 f ( cook , bloomington / in / usa ) e guida superstiff 0 , 035 185cm ( back - up meier , boston scientific , ratingen , germania ) attraverso larteria femorale comune ; quando stata utilizzata lendoprotesi zenith , lintroduttore era parte integrante del device . 
lutilizzo di un catetere fornito di pallone in lattice ( 2733 mm di diametro ) a bassa pressione ( equalizer , boston scientific , ratingen , germania ) ha consentito di sigillare lendoprotesi a livello degli ancoraggi prossimale e distale e le connessioni dei segmenti protesici . 
in 6 / 38 pazienti sono state necessarie procedure endovascolari aggiuntive a livello dellasse iliaco al fine di consentire lavanzamento del device ( pta in 5 casi , pta e stenting in 1 caso )  . il successo tecnico immediato stato dimostrato dallo studio angiografico eseguito al termine della procedura . 
 stato utilizzato in tutti i pazienti un mezzo di contrasto nonionico , isoosmolare ( iodixanolo , visipaque , amersham , saluggia , italia ) ( range 80160 ml , media 100 )  . 
la profilassi antitrombotica durante la procedura stata praticata con somministrazione di eparina ( 5000 ui endovena ) , seguita da eparina a basso peso molecolare in dosi profilattiche nei 30 giorni successivi , e successivamente con antiaggregante o anticoagulante ( in base ai dati clinico - anamnestici del paziente )  . 
la profilassi antibiotica stata realizzata secondo un protocollo ultra breve al momento dellinduzione dellanestesia per ottenere unadeguata concentrazione del farmaco al momento del posizionamento dellendoprotesi ( vancomicina , abbott , lt , italia ; 1 g ev ) ; in pazienti con insufficienza renale o pregressa intolleranza stata utilizzata ciprofloxacina e cefazoline . 
in tutti i pazienti il follow - up stato realizzato mediante angio - tc in accordo al protocollo eurostar a 1 , 3 , 6 , 12 mesi e in seguito annualmente [ 6 ]  . una angio - tc pre - dimissione stata eseguita nei 15 pazienti che , emodinamicamente instabili allingresso , erano giunti a diagnosi mediante la sola ecotomografia . results mean procedure time was 105 min ( range : 65235 )  . 
abbiamo osservato 7 lievi rialzi ( > 2 mg / dl ) dei livelli di creatinina sierica ( 2 / 7 pazienti con preesistente insufficienza renale cronica sono stati trattati con dialisi temporanea ) e 2 infezioni di d . 
there were 4 / 38 deaths ( 10.5% ) , one on the first postoperative day due to arrhythmia , two on the second and one on the fourth postoperative day due to multiorgan failure . 
mean postoperative hospital stay was 7.7 ( range : 230 ) days ; 11 / 38 patients required admission to the intensive care unit ( mean hospital stay 13 days , range : 230 days )  . 
five endoleaks were identified during follow - up ( 12% ) : four type - 2 endoleaks were identified at 3 months ( one arising from the inferior mesenteric artery , which thrombosed after 8 months ; three from the iliolumbar arteries , of which one thrombosed after 6 months and two were under observation at the time of writing ) ; one type - 3 endoleak ( detected at 12 months ) due to disjunction of the contralateral leg , which was corrected by positioning an extension . 
the total percentage of types - 1 and 3 endoleaks related to technical failure was 2.9% , which is comparable with the percentage measured under elective conditions ( 4% )  . 
in one patient , the endograft leg occluded after 6 months and was treated with femorofemoral bypass surgery . during follow - up , shrinkage of the aneurysm sac was observed in 10 / 34 cases whereas the remaining 24 / 34 cases showed no change in size ; no cases of aneurysm sac growth ( endotension ) were observed . discussion despite major progress in the fields of surgery , radiology , anaesthesia and intensive care , morbidity and mortality of ruptured aaas have remained high over the past 10 years as a result of the advanced age and frequent cardiorespiratory comorbidity of patients affected by this disease [ 7 ]  . 
the development of increasingly versatile devices and growing operator experience have extended the clinical and morphological indications for endovascular treatment , which is now being proposed as an alternative to open surgery , even in emergency settings [ 2 , 7 , 928 ]  . endovascular treatment presents some analogies with the modern approach to patients with severe haemorrhage . 
the primary goal is to use the least invasive procedure to rapidly control the source of bleeding and reduce the risk of prolonged hypoperfusion , hypothermia , coagulopathy and acidosis [ 29 ]  . 
abbiamo osservato 4 / 38 decessi ( 10 , 5% ) : uno nella i giornata post - operatoria a causa di un aritmia cardiaca , due in ii e uno in iv giornata post - operatoria a causa di una insufficienza multiorgano . 
la degenza post - operatoria media stata 7 , 7 giorni ( range 230 giorni )  . il ricovero in terapia intensiva stato necessario in 11 / 38 pazienti ( degenza media 13 giorni , range 230 giorni )  . 
durante il follow - up si sono osservati 5 endoleaks ( 12% ) : 4 di tipo ii documentati 3 mesi dopo la procedura ( 1 dallarteria mesenterica inferiore trombizzato in 8 mesi ; 3 dalle arterie ileo - lombari di cui uno trombizzato in 6 mesi e 2 sotto osservazione ) ; 1 di tipo iii ( dimostrato 12 mesi dopo la procedura ) dovuto alla sconnessione della gamba protesica controlaterale e corretto con il posizionamento di una prolunga protesica . non abbiamo osservato endoleak di tipo i . 
la percentuale totale di endoleaks di tipo i e iii direttamente correlate allinsuccesso tecnico della procedura stata del 2 , 9% , comparabile con quella riscontrata nella nostra esperienza in elezione ( 4% )  . 
durante il follow - up abbiamo osservato una riduzione della sacca aneurismatica in 10 / 34 casi e dimensioni invariate in 24 / 34 casi ; non abbiamo osservato casi di incremento volumetrico della sacca ( endotension )  . discussione nonostante gli importanti progressi nel campo di chirurgia , imaging , anestesia e metodiche di terapia intensiva , negli ultimi dieci anni la percentuale di morbilit e mortalit tra i pazienti con rottura di aaa rimane ancora elevata , soprattutto in considerazione dellet avanzata e della frequente comorbidit cardio - respiratoria dei pazienti con questo tipo di patologia [ 7 ]  . 
il trattamento chirurgico in elezione degli aaa in centri specializzati ha attualmente una mortalit di poco inferiore al 5% , che raggiunge il 50%65% in emergenza [ 8 ]  . 
lo sviluppo di devices sempre pi versatili e la crescente esperienza degli operatori ha esteso le indicazioni clinico - morfologiche del trattamento endovascolare permettendo allo stesso di proporsi come possibile alternativa terapeutica alla chirurgia open anche in emergenza [ 2 , 7 , 928 ]  . lalternativa endovascolare presenta alcune analogie con il moderno approccio al paziente con emorragia severa . lobiettivo primario infatti il rapido controllo della fonte di sanguinamento , attraverso la procedura meno invasiva , per ridurre il conseguente rischio di prolungata ipoperfusione e quindi di ipotermia , coagulopatia e acidosi [ 29 ]  . 
in haemodynamically stable patients ( arterial pressure > 80100 mmhg ) , ct angiography can be performed to identify the signs of aaa rupture and assess feasibility of the endovascular approach , and planning of the procedure is done in urgent conditions [ 30 ]  . 
in patients with haemorrhagic shock ( arterial pressure < 80 mmhg ) who have a us diagnosis of aaa rupture and are ineligible for open surgery , planning of the endovascular procedure is done in emergency conditions with angiography only [ 11 , 14 , 23 ]  . 
 selection criteria for urgent endovascular treatment are clinical and radiological : lumbar pain and / or hypotension ( systolic pressure < 100 mmhg ) or haemorrhagic shock ( systolic pressure < 80 mmhg ) , and pulsatile abdominal masses were considered clinical signs of symptomatic or ruptured aaa . 
radiological criteria were evidence of retroperitoneal haematoma or signs of impending rupture on ct angiography ( precontrast hyperdense thrombus , crescent sign and / or contrast penetration in the thrombus ) or on us ( inhomogeneous and stratified structure of the thrombus )  . 
in our experience , we used aortouniiliac stent - grafts in urgent conditions in patients with anatomy precluding placement of a bifurcated device only : occlusion of an iliofemoral axis ; small aortic bifurcation preventing placement of two endograft leg . 
vascular reconstruction afforded by the stentgraft is less anatomical ; furthermore , use of a uniiliac device in emergency conditions guarantees that the bleeding stops after deployment of the iliac occluder , which is definitely faster than that of an endograft leg , to be used in cases of severe haemodynamic instability [ 29 ]  . 
 some authors [ 31 , 32 ] have analysed outcomes to identify the variables most frequently associated with high mortality . variables identified were age over 80 years , preoperative cardiac arrest , loss of consciousness and shock ( systolic pressure < 91 mmhg , haemoglobin < 8 g / dl , haematocrit < 25% )  . 
this may be an ethically and professionally correct approach that spares the patient unnecessary suffering , avoid raising unjustified hopes in the relatives and reduce unnecessary healthcare costs [ 31 , 32 , 33 ]  . 
as also reported by other authors , we found the time required for placement of the contralateral leg of a bifurcated endograft to be shorter than that needed to perform a surgical femorofemoral crossover , with reduction in operative times [ 10 , 28 ]  . 
however , in haemodynamically unstable patients , placement of an aortouniiliac stent - graft is faster and safer . stabilisation of the patients haemodynamic conditions after tamponade and resuscitation procedures may provide the tre nei pazienti con sospetto di rottura di aaa essenziale seguire liter diagnostico meno time consuming . 
nel paziente emodinamicamente stabile ( pressione arteriosa > 80100 mmhg ) possibile eseguire unangio - tc per individuare i segni di rottura dellaaa e valutare la fattibilit dellapproccio endovascolare e il planning della procedura viene effettuato in urgenza [ 30 ]  . 
nel paziente con shock emorragico ( pressione arteriosa < 80 mmhg ) allorquando viene effettuata diagnosi di aaa rotto mediante ecografia e stabilito che il paziente non possiede gli estremi per lintervento di chirurgia open , il planning della procedura endovascolare viene effettuato in emergenza con la sola angiografia [ 11 , 14 , 23 ]  . 
 i criteri utilizzati per selezionare i pazienti per il trattamento endovascolare in urgenza sono clinici e radiologici . dolore lombare e / o ipotensione ( pressione sistolica < 100 mmhg ) o shock emorragico ( pressione sistolica < 80 mmhg ) e massa addominale pulsante sono stati considerati segni clinici di aaa sintomatico o rotto . 
i criteri radiologici utilizzati sono stati la presenza di ematoma retroperitoneale o segni di imminente rottura alla valutazione mediante angio - tc ( iperdensit del trombo in fase pre - contrastografica crescent sign e / o penetrazione del mezzo di contrasto nel contesto del trombo ) o mediante ecografia ( disomogeneit e stratificazione dellecostruttura del trombo )  . 
nella nostra esperienza le endoprotesi aorto - uni - iliache sono stati utilizzate , in urgenza , solamente in casi dove lanatomia non ha permesso il posizionamento di un device biforcato : occlusione di un asse iliaco - femorale , biforcazione aortica di diametro ridotto tale da non poter allogare due bracci protesici . 
questa endoprotesi consente una ricostruzione vascolare meno anatomica ; inoltre luso di un device monoiliaco in emergenza garantisce larresto del sanguinamento dopo il posizionamento dellocclusore iliaco , sicuramente pi veloce del posizionamento di un braccio protesico , da utilizzare in casi di severa instabilit emodinamica [ 29 ]  . 
tali variabili sono state identificate in : et superiore a 80 anni , arresto cardiaco preoperatorio , perdita di coscienza , shock ( pressione sistolica < 91 mmhg , emoglobina < 8 g / dl , ematocrito < 25% )  . 
questo potrebbe essere un atteggiamento corretto dal punto di vista etico e professionale al fine di evitare inutili sofferenze al paziente ed infondere inutili speranze nei suoi familiari , oltre che evitare costi assistenziali assolutamente inutili [ 3133 ]  . come riportato da alcuni autori in letteratura , nella nostra esperienza il tempo necessario al posizionamento della gamba controlaterale dellendoprotesi biforcata minore rispetto a quello richiesto per realizzare il cross - over chirurgico femoro - femorale , con una riduzione dei tempi operatori [ 10 , 28 ]  . 
the catheter was placed percutaneously and transfemorally by fixing it to a juxtarenal site through a 30 - cmlong 12 - f introducer to prevent any caudal displacement of the occlusive balloon caused by the arterial pressure . 
transfemoral access was preferred to brachial access owing to catheter calibre ( 7 f ) and the fact that attempting a third arterial access would have been too time consuming [ 24 ]  . 
although a number of studies have proposed local anaesthesia because of the small rate of cardiorespiratory complications [ 10 , 21 ] , our experience and that of other authors [ 15 , 16 ] make us inclined to use general anaesthesia to prevent unwanted movements and achieve better control of the patients haemodynamic conditions . use of muscle relaxants is , however , contraindicated since relaxation of the retroperitoneal musculature prevents control of the retroperitoneal haematoma [ 7 ]  . 
it should be noted that with uncontrolled haemorrhage , excessive fluid infusion may be dangerous and increase the bleeding ; controlled hypotension , on the other hand , slows the haemorrhage and can therefore facilitate the formation of a local clot . 
in emergency procedures , it reaches 28% , which can be explained by the need to cover the renal arteries in the absence of a neck in nonsurgical patients undergoing emergency endovascular treatment [ 10 ]  . 
exclusion of the inferior mesenteric artery ( and hence of the hypogastric artery ) in a hypoperfused patient can cause colonic ischaemia , in part as a result of a reduced compensation capacity of the other splanchnic vessels . 
la decisione anche in relazione allesperienza degli operatori . nella nostra casistica in accordo con lesperienza riportata in letteratura , il catetere fornito di pallone occlusore in lattice stato utilizzato solo in 5 / 15 casi di instabilit emodinamica del paziente appena arrivato in sala operatoria [ 16 ]  . 
il catetere stato posizionato per via percutanea transfemorale ancorandolo in sede iuxtarenale mediante un introduttore 12 f lungo 30 cm per prevenire dislocazioni caudali del pallone occlusore dovute alla pressione arteriosa . 
laccesso transfemorale stato preferito al brachiale in relazione al calibro del catetere di 7 f e perch il tentare il terzo accesso arterioso avrebbe comportato un eccessivo dispendio di tempo [ 24 ]  . 
malgrado molti studi suggeriscano luso dellanestesia locale in relazione alla bassa percentuale di complicanze cardio - respiratorie [ 10 , 21 ] , la nostra esperienza e quella di altri autori [ 15 , 16 ] propende per la scelta dellanestesia generale . 
bene sapere che , in presenza di un emorragia incontrollata , uneccessiva infusione di liquidi pu essere pericolosa causando un incremento del sanguinamento ; una ipotensione controllata invece rallentando lemorragia pu agevolare la formazione di un coagulo locale . le possibili complicanze del trattamento endovascolare sono sovrapponibili a quelle incontrate nel trattamento in elezione . particolare attenzione andrebbe inoltre riservata alla funzionalit renale e alleventuale ischemia splancnica nel caso del trattamento in emergenza . 
lo shock emorragico con ipoperfusione renale , la prolungata ipotensione e la sindrome compartimentale da ematoma retroperitoneale sono tutti fattori che contribuiscono al deterioramento della funzione renale connesso anche alluso del mezzo di contrasto . 
lincidenza dellinsufficienza renale post - operatoria varia tra il 2 , 5% e l8 , 3% per il trattamento in urgenza , in accordo con i dati eurostar e non differisce significativamente dal trattamento chirurgico . 
nelle emergenze raggiunge il 28% e questo pu essere anche giustificato dalla necessit di coprire le arterie renali in assenza di colletto in paziente non chirurgico che effettua lalternativa endovascolare in emergenza [ 10 ]  . 
lesclusione dellarteria mesenterica inferiore ( e in definitiva dellarteria ipogastrica ) in un paziente ipoperfuso pu causare unischemia colica anche in relazione alla minore capacit di compenso degli altri vasi splancnici . 
the frequency of type - 1 and type - 3 endoleaks , directly related to technical failure , is 3.7% , similar to that observed in elective procedures in our experience ( 4% ) and to that reported in the literature [ 26 ]  . 
review of the literature and consideration of the different techniques used by the various centres for planning the procedure ( from device selection to choice of anaesthesia ) shows that endovascular treatment is feasible and carries a high rate of shortand medium - term technical success , with only a few cases requiring surgical conversion [ 2 , 7 , 928 ]  . 
furthermore , reports comparing endovascular and surgical treatment have demonstrated that endovascular treatment significantly reduces mortality in addition to providing the benefits of a minimally invasive procedure ( less blood loss , shorter stays in intensive care units ) [ 2 , 12 , 17 , 18 ]  . 
 on the basis of our personal experience and the literature , we can conclude that the endovascular approach is a promising alternative for the treatment of aaas , under both urgency and emergency conditions . 
the use of bifurcated grafts , when possible , allows for better reconstruction of the vascular anatomy with shorter overall operative times compared with the placement of an aortouniiliac device and subsequent femorofemoral bypass . 
further studies with longer follow - up periods and larger series are required to evaluate the long - term results of endovascular treatment and compare it with surgical treatment in terms of morbidity , mortality and long - term success . sere trattata con una decompressione extraperitoneale translombare nei pazienti con segni di insufficienza dorgano correlata allaumento della pressione intra - addominale [ 7 , 11 ]  . la frequenza di endoleak tipo iiii direttamente correlata al fallimento tecnico della procedura del 3 , 7% , comparabile con quella riscontrata nella nostra esperienza nel trattamento in elezione ( 4% ) e con quella riportata in letteratura [ 26 ]  . 
dalla revisione della letteratura e considerando le differenti tecniche usate nei differenti centri per pianificare la procedura ( dalla scelta del device al tipo di anestesia ) , lapproccio endovascolare fattibile con unalta percentuale di successo tecnico immediato e a medio termine e in pochi casi richiede la conversione chirurgica [ 2 , 7 , 928 ]  . 
 inoltre le casistiche che comparano il trattamento endovascolare con la chirurgia rivelano una significativa riduzione in mortalit nel primo gruppo in aggiunta ai vantaggi correlati alla mini - invasivit della procedura ( minori perdite ematiche , riduzione dei tempi di degenza in unit di cura intensiva ) [ 2 , 12 , 17 , 18 ]  . 
in conclusione , da quanto si evince dallesperienza personale e dalla revisione della letteratura , possibile affermare che lapproccio endovascolare una promettente alternativa terapeutica per il trattamento sia in urgenza che in emergenza degli aaa . 
la scelta del tipo di protesi , biforcata o aorto - uni - iliaca , in urgenza e in emergenza dipende dalle condizioni emodinamiche del paziente , dallesperienza degli operatori e dalladeguato approvvigionamento di materiali . 
luso dellendoprotesi biforcata , dove possibile , permette una migliore ricostruzione dellanatomia vascolare con minori tempi operatori complessivi , rispetto al posizionamento di un device aorto - uni - iliaco con successivo bypass femoro - femorale . 
gandini1 1ospedale san giovanni battista , via genova 3 , i - 10126 torino , italy 2struttura complessa fisica sanitaria i , 3scdu di endocrinologia e malattie del metabolismo , istituto di radiologia , universit di torino , torino , italy correspondence to : c . 
at baseline and at 6 months follow - up , 290 male patients aged between 18 and 37 ( average age 27.3 years ) with left ( 266 cases ) or bilateral ( 24 cases ) varicocele underwent clinical assessment , doppler ultrasonography ( us ) , laboratory testing of free and total serum testosterone , leutenising hormone ( lh ) and follicle stimulating hormone ( fsh ) gonadotropins , inhibin b and spermiograin 223 cases , selective catheterisation of the spermatic vein was performed with a right transfemoral approach . 
technical success was achieved in 206 / 223 cases ; two phlebographic examinations ( immediately following administration of the sclerosing agent and after 1520 min ) showed prethrombotic endoluminal alterations of the internal spermatic veat 6 months follow - up , 172 / 206 patients ( 83.49% ) showed complete resolution of the varicocele whereas 34 / 206 ( 16.5% ) had only partial disengorgement of the pampiniform plexus . 
the following minor procedural complications were recorded : two cases of acute abdominal pain , three of vagal crisis during administration of sclerosing agent that resolved spontaneously and two of spermatic cord inflammation that resolved within days after medical therapy . we recorded no statistically significant differences with regard to riassunto obiettivo . 
in condizioni basali e ad un follow - up di 6 mesi 290 pazienti maschi di et compresa tra 18 e 37 anni ( vm 27 , 3 ) con varicocele sinistro ( 266 casi ) o bilaterale ( 24 casi ) sono stati valutati con esame clinico , esame doppler , dosaggio su siero di testosterone libero e totale , delle gonadotropine lh ed fsh e dellinibina b e con lo spermiogramma . 
duecentosei su 223 pazienti sono stati sottoposti a trattamento radiologico del varicocele ; in 194 casi stato utilizzato esclusivamente lhydroxy - poliethoxy - docanol ( atossisclerol ) , mentre in 12 casi ( 5 , 8% ) in aggiunta ad esso sono stati impiegati 5 ml di alcol assoluto ed una spirale di gianturco ( cook 10 mmx50 mm da 0 , 038 pollici )  . 
nei 206 pazienti trattati stato ottenuto il successo tecnico immediato ; due successivi controlli flebografici ( immediatamente dopo ed a 1520 minuti dalla somministrazione degli agenti scleroembolizzanti ) hanno dimostrato le alterazioni pretrombotiche endoluminali della vena spermatica interna . 
il follow - up a 6 mesi dal trattamento radiologico percutaneo ha rilevato la scomparsa del varicocele in 172 / 206 pazienti ( 83 , 49% ) , mentre in 34 / 206 pazienti ( 16 , 5% ) la detensione del plesso pampiniforme stata soltanto parziale . 
sono stati registrati i seguenti piccoli effetti collaterali del trattamento : 2 casi di algia addominale acuta e 3 casi di crisi vagale durante liniezione dello sclerosante , regrediti spontaneamente , e 2 casi di flogosi irritativa c . 
the principal technical limitation to percutaneous treatment is related to difficult selective catheterisation of the spermatic vein due to anatomic alterations , spasms and intimal dissection of the vemoreover , when the cremasteric vein is incontinent , inguinal surgical ligation provides better results . 
in the majority of cases , administration of at least 3 ml sclerosing agent at 3% ensures occlusion of the gonadic vein above the abdominal collaterals , which are responsible for long - term recurrence if not treated . 
 key words varicocele sclerotherapy seminal parameters dosimetry del funicolo spermatico risolta in pochi giorni con terapia medica . non sono state registrate differenze statisticamente significative per quanto concerne la volumetria testicolare ed i dosaggi ormonali sierici tra il gruppo di pazienti trattati e non trattati . 
la somministrazione di almeno 3 ml di sclerosante concentrato al 3% assicura nella gran parte dei pazienti locclusione della vena gonadica a monte dei circoli collaterali addominali , responsabili , se non trattati , di recidiva a distanza ; negli altri casi , possono essere utilizzati a completamento terapeutico lalcol assoluto e le spirali metalliche . 
riteniamo , infine , che le manovre radiologiche siano controindicate ed ingiustificate nei casi in cui si rendano necessari prolungati cateterismi con elevata irradiazione delle gonadi . parole chiave varicocele scleroterapia parametri seminali dosimetria introduction introduzione varicocele , a varicose dilatation of the pampiniform plexus veins , is a very common disorder that is clinically relevant in 5%20% of males and often associated with dyspermia ( 30%45% ) and infertility ; hence , the indication for treatment of paediatric patients and / or adolescents [ 1 ]  . 
the disorder is caused by inversion of blood flow within the internal spermatic vein , which drains into the renal vein on the left side and , in 90% of cases , directly into the inferior vena cava on the right side . 
primary varicocele is due to valve incompetence and favoured by the retroperitoneal location of the internal spermatic vein ( absence of contiguous muscles facilitating centripetal blood flow ) and by renal - vein abnormalities ; it is associated with factors related to the vessel wall . symptomatic varicocele is rare and secondary to expansile processes of the retroperitoneum , kidney and pancreas . due to the above - mentioned anatomical factors , varicocele is more common on the left side . 
venous reflux occurs more frequently through the internal spermatic vein or via aberrant collateral branches originating from the renal vein , intraor perirenal branches , inferior vena cava , lumbar veins or iliac vein and anastomosed caudally with the internal spermatic vediagnostic imaging is instrumental in the diagnosis and staging of varicocele . 
ultrasonography is highly sensitive in detecting subclinical forms , and il varicocele , dilatazione varicosa del plesso pampiniforme , unaffezione molto frequente che ha rilevanza clinica nel 5%20% della popolazione maschile ed spesso associata a dispermia ( 30%45% ) ed infertilit ; di qui lindicazione al trattamento di pazienti pediatrici e / o adolescenti [ 1 ]  . 
questa patologia dovuta allinversione di flusso nella vena spermatica interna , che a sinistra sbocca nella vena renale e , a destra , nel 90% dei casi direttamente nella vena cava inferiore . 
la forma primitiva dovuta ad incontinenza valvolare , favorita dalla sede retroperitoneale della vena spermatica interna ( assenza di muscoli contigui favorenti la progressione centripeta del sangue ) e da alterazioni anatomiche della vena renale , ed associata a fattori costituzionali della parete vasale . 
il reflusso venoso avviene pi spesso attraverso la vena spermatica interna o in alternativa lungo collaterali venosi aberranti con essa anastomizzati caudalmente originanti dalla vena renale , da rami intrao peri - renali , dalla vena cava inferiore , dalle vene lombari o dalle vene iliache . la diagnostica per immagini ha un ruolo fondamentale nella diagnosi e nella stadiazione del varicocele e si avvale delle seguenti tecniche : flussimetria doppler , eco - tomografia e flebografia . 
selective phlebography of the renal vein or internal spermatic vein enables identification of incompetent valves at the ostial level , determination of degree of reflux of contrast medium as well as mapping of the venous drainage system , which serves to distinguish among the different types of varicocele ( table 1 )  . 
 percutaneous treatment , which can be performed as an outpatient procedure and involves a moderate radiation dose [ 4 ] , is always indicated in types i and iii but only indicated in types ii and iv if the catheter can be advanced above the collaterals close to the inguinal ligament . 
in advanced cases , with associated ectasia of the posterior pampiniform plexus draining into the iliac system , surgery is the only feasible treatment due to impossibility of selectively catheterising the relevant veins . 
 the through a right transfemoral or brachial rarely jugular is selectively internal spermatic vein approach , catheterised using simmons or cobra catheters , depending on whether the right or left side is being treated . 
the use of detachable balloons and metallic coils reduces embolisation time but is not recommended in the presence of a rich network of collaterals due to possible risk of early recurrence ; in such cases , sclerosing agents should be used . 
 complications secondary to percutaneous therapy are relatively rare and unimportant ; the most serious include development of phlebothrombosis of the pampiniform plexus and of the venous districts connected to the internal spermatic vein and the possible migration of embolisation material , or parts thereof , into the systemic circulation . current legislation on radiation protection [ 5 ] requires compliance with the principle of justification for medical extable 1 types of left - sided varicocele based on anatomical variants c . 
schematicamente , i metodi attualmente utilizzati nella terapia percutanea del varicocele sono locclusione meccanica con spirali di gianturco o palloncini staccabili e la sclerosi con un agente chimico . con approccio femorale destro o brachiale , raramente giugulare , si cateterizza selettivamente la vena spermatica interna , utilizzando per lo pi cateteri di tipo cobra se il trattamento da effettuare a sinistra e di tipo simmons se a destra . 
sulla base della preventiva flebografia , eseguita facendo compiere al paziente la manovra di valsalva , si decide il trattamento pi idoneo in base al tipo di variante anatomica dimostrata . 
luso dei palloncini staccabili e delle spirali metalliche riduce il tempo di trombizzazione , ma non indicato nei casi in cui sia presente una ricca rete di collaterali per la possibile insorgenza di recidiva precoce ; in questi casi opportuno limpiego di farmaci sclerosanti . le complicanze conseguenti alla terapia percutanea sono relativamente poco frequenti e di scarsa importanza ; tra le pi gravi , vi sono lassai rara comparsa di flebotrombosi del plesso pampiniforme e dei distretti venosi anastomizzati con la vena spermatica interna e la possibile migrazione nel cirsingle testicular vein without valves afferent collateral retroperitoneal vessels to the ascendant lumbar vein and / or retroaortic vessels adjacent to the lumbar vessels tributary of the inferior vena cava duplication of internal spermatic vein into parallel main branches with communicating cross - connecting branches afferent collaterals to renal and / or perirenal veins bifurcation of renal vein showing preand retroaortic course tabella 1 tipologie di varicocele sinistro secondo le varianti anatomiche vena testicolare singola senza valvole circoli collaterali retroperitoneali afferenti alla vena lombare ascendente e / o vasi retroaortici contigui alle vene lombari tributari della vena cava inferiore suddivisione della vena spermatica interna in due rami principali paralleli ampiamente anastomizzati tra loro circoli collaterali afferenti alle vene renali e / o perirenali vena renale biforcata a decorso antero e retro - aortico c . 
 materials and methods clinical and seminal evaluation two hundred and ninety patients aged 1837 years ( mean age 27 years ) referred to our division of andrology for low fertility or testicular pain were diagnosed with varicocele . all patients were assessed on entry and 6 months later after associated urogenital , endocrine and internal disorders had been excluded . 
serum concentrations of total ( radioimmunoassay , sorin biomedica , saluggia , italy ) and free ( radioimmunoassay , diagnostic products corporation , los angeles , ca , usa ) testosterone , follicle stimulating hormone ( fsh ) and leutenising hormone ( lh ) gonadotropin ( immunoradiometric assay , radim s.p.a. , rome , italy ) and inhibin b ( enzyme - linked immunosorbent assay , oxford bio - innovation ltd , upper heyford , uk ) were measured . 
seminal examinations were carried out in accordance with the world health organisation ( who ) criteria [ 9 ]  . sperm concentration was obtained using a makler chamtable 2 doppler - based grading system according to dubin [ 8 ] modest and transitory reflux during a valsalva manoeuvre ( normal report ) persistent reflux finishing before the end of a valsalva manoeuvre reflux persisting during a valsalva manoeuvre baseline reflux not changing during a valsalva manoeuvre tabella 2 grading doppler del varicocele secondo dubin [ 8 ] modesto e transitorio reflusso venoso durante la manovra di valsalva ( quadro fisiologico ) reflusso venoso persistente che si esaurisce prima del termine della manovra di valsalva reflusso venoso persistente durante lintera manovra di valsalva reflusso venoso presente in condizioni basali che non muta durante la manovra di valsalva grade 0 grade 1 grade 2 grade 3 grado 0 grado 1 grado 2 grado 3 colo sistemico dei mezzi embolizzanti o delle loro parti . lattuale normativa di radioprotezione [ 5 ] impone losservanza del principio di giustificazione per le esposizioni mediche attraverso la valutazione dei potenziali vantaggi diagnostici o terapeutici complessivi prodotti rispetto al danno alla persona che lesposizione potrebbe causare . lefficacia tecnico - clinica del trattamento radiologico del varicocele deve essere quindi valutata alla luce di misure dosimetriche . 
alcuni studi presenti in letteratura [ 6 , 7 ] riportano valori di dose alle gonadi che permettono di escludere linduzione di danni di tipo deterministico e valori di dose efficace che , pur rientrando nellordine di grandezza proprio di altre indagini diagnostiche , meritano una particolare attenzione nei confronti del rischio probabilistico . materiali e metodi valutazione clinico - seminale in 290 pazienti di et compresa tra 18 e 37 anni ( vm 27 anni ) , giunti al servizio di andrologia del nostro ospedale per ipofertilit o dolenza testicolare , stata posta diagnosi di varicocele . 
sono state quindi dosate le concentrazioni sieriche di testosterone totale ( radioimmunoassay sorin biomedica , saluggia , italia ) e libero ( radioimmunoassay diagnostic products corporation , los angeles , usa ) , delle gonadotropine fsh ed lh ( immunoradiometricassay radim s.p.a. , roma , italia ) e di inibina b ( enzyme - linked immunosorbent assay oxford bio - innovation ltd . , upper heyford , uk )  . 
gli esami seminali sono stati effettuati secondo i criteri del who [ 9 ]  . la concentrazione degli spermatozoi stata determinata utilizzando la camera di makler , mentre la loro morfologia stata valutata con colorazione di papanicolaou ; il grado di motilit stato stimato soggettivamente . duecentosei pazienti sono stati sottoposti a scleroembolizzazione radiologica della vena spermatica interna , mentre in 17 pazienti stata effettuata la sola flebografia spermatica . 
treatment effectiveness was assessed by two consecutive postprocedure phlebographic examinations and subsequently by doppler examination of the spermatic cord ; in particular , partial regression of the varicocele by at least one grade was defined as a reduction in the degree of incompetence . 
 radiological procedure this procedure was carried out using an angio diagnost 3 dvi ( philips medical systems , best , the netherlands ) radiological device . following local anaesthesia ( 5 ml of 2% lidocaine ) , the right common femoral vein was accessed and a 5f vascular introducer positioned . 
selective catheterisation of the renal vein with 5f cobra catheter and 0.035hydrophilic guidewire ( terumo corporation , tokyo , japan ) was performed using the seldinger technique . contrast medium ( ultravist 370 , schering ag , berlin , germany ) was administered with the patient performing a valsalva manoeuvre to demonstrate valve incompetence of the internal spermatic vein . subsequently , selective analysis of the internal spermatic vein was performed with the catheter tip positioned just above the inguinal ligament ; morphology of the collateral circulation and incontinence of the cremasteric vein were accurately evaluated [ 10 ]  . a simmons 5f hydrophilic catheter was used for rightsided selective spermatic phlebography ; in these patients , the ipsilateral transfemoral approach made it difficult to achieve deep catheterisation , which was only possible with the more expensive coaxial technique . following digital massage of the testis to drain the opacified veins of the pampiniform plexus , occlusion of the internal spermatic vein was obtained by administering a 50% mixture of hydroxy - poliethoxy - docanol ( atoxysclerol ) at 2% or 3% and contrast material via the catheter placed with the tip caudal to the origin of the collaterals just above the inguinal ligament . during treatment , the patient was instructed to compress the internal spermatic vein to avoid thrombosis of the testicular circulation and to perform a valsalva manoeuvre to prevent reflux of the sclerosing agent into the renal vein . the same technique was performed on right - sided varicoceles . 
at the end of the procedure , two successive phlebographic examinations were performed at 1520 min 12 cases of persistent patency of the spermatic vein , 5 ml of alcohol and a 0.038 - ( 10 mmx50 mm ) metallic coil were also used . 
following removal of the angiographic catheter and vascular introducer , the puncture site was briefly compressed ; the patient was then sent to the day hospital for 34 h of clinical observation . 
in anestesia locale ( 5 ml di lidocaina al 2% ) stata eseguita la puntura della vena femorale comune destra con successivo posizionamento di introduttore vascolare di 5f . con tecnica di seldinger stato eseguito il cateterismo selettivo della vena renale con catetere cobra di 5f e guida idrofila di 0 , 035 pollici ( terumo corporation , tokyo , japan )  . 
per dimostrare lincontinenza valvolare della vena spermatica interna stata eseguita uniniezione di mdc ( ultravist 370 , shering ag , berlin , germany ) in corso di manovra di valsalva . 
stato quindi effettuato lo studio selettivo della vena spermatica interna , sospingendo in tutti i casi lapice del catetere appena al di sopra del legamento inguinale ; stato possibile valutare precisamente lanatomia dei circoli collaterali e lincontinenza della vena cremasterica [ 10 ]  . 
a destra , per la flebografia spermatica selettiva , stato impiegato un catetere idrofilo tipo simmons di 5f ; in questi pazienti lapproccio vascolare transfemorale omolaterale ha reso difficoltoso in molti casi il cateterismo profondo , che stato reso possibile solo grazie alla pi costosa tecnica coassiale . 
previo massaggio digitale del proprio testicolo da parte del paziente , volto a drenare le vene del plesso pampiniforme opacizzate , stata ottenuta locclusione della vena spermatica interna somministrando una miscela al 50% di hydroxy - poliethoxy - docanol ( atossisclerol ) al 2% o 3% e contrasto attraverso il catetere posizionato con apice caudalmente allorigine dei circoli collaterali , poco al di sopra del legamento inguinale . 
durante il trattamento il paziente effettuava contemporaneamente una compressione occlusiva della vena spermatica interna allinguine , per evitare la trombosi del circolo testicolare , e la manovra di valsalva per evitare il reflusso dellagente sclerosante in vena renale . la stessa tecnica stata applicata ai varicoceli di destra . 
al termine della procedura sono stati eseguiti 2 successivi controlli flebografici a distanza di 1520 min 12 casi di persistente perviet della vena spermatica sono stati utilizzati anche 5 ml di alcol ed una spirale metallica da 0 , 038 pollici di 10 mmx50 mprevia rimozione del catetere angiografico e dellintroduttore vascolare stata effettuata una breve compressione del sito di puntura ; il paziente stato quindi rinviato in day hospital per unosservazione clinica di 34 ore . 
alla dimissione sono stati consigliati riposo a letto per 48 ore ed astensione da attivit fisica gravosa per almeno 30 giorni . analisi statistica sono stati utilizzati il t - test e c2 test . valutazione dosimetrica sono state effettuate misure in vivo nel corso di 20 procedure . 
per le misure stata utilizzata una camera trasmissiva diamentor m4kdk a doppio canale ( ptw , freiburg ) con misura simultanea del kerma in aria ( kair ) sullasse centrale del fascio ( area di misura di 13x13 mm ) e del dap ( area di misura di 140x140 mm )  . 
a double diamentor m4kdk transmission chamber ( ptw - freiburg ) was used to measure simultaneously the air kerma ( kair ) on the central beam axis ( field size 13x13 mm2 ) and the dose area product ( dap ) ( field size 140x140 mm2 )  . 
the chamber was positioned at the x - ray tube window during the procedures after checking that it did not interfere with beam characteristics and actions required for the interventional procedure . 
appropriately calibrated singlepack kodak x - omat v films ( 25.4x30.5 cm2 ) positioned between the bed and the patient were used to measure entrance surface dose ( esd ) and effective dose ( ed )  . 
film optical density , correlated to the dose according to the calibration curve used , was read using a densitometer for point measurements ( pehamed densoquick 2 ) and an agfa arcus ii scanner . 
complete distribution of the esd obtained in this way can be used to derive a reliable estimate of effective dose by defining an equivalent configuration of static exposures and using the ods - 60 calculation software ( distributed by rti electronic ) , which measures organ dose in a phantom for conventional radiological examinations ( thus with rectangular fields and based on dap ) on the basis of data obtained with monte carlo simulations . 
1 rappresentazione schematica della disposizione della strumentazione di misura utilizzata per le valutazioni di dose in corso di procedura angiografica . rificato la totale assenza di interferenza con le caratteristiche del fascio e con le azioni necessarie per lo svolgimento dellintervento . 
per le valutazioni della dose in ingresso ( di ) e per la stima della dose efficace ( de ) sono state utilizzate pellicole kodak tipo x - omat v impacchettate in busta singola di dimensioni 25 , 4x30 , 5 cm , opportunamente calibrate e posizionate tra il lettino e il paziente . 
la lettura dei valori di densit ottica delle pellicole , correlati alla dose secondo la curva di taratura realizzata , stata effettuata con un densitometro a punto ( pehamed densoquick 2 ) e con uno scanner agfa arcus ii . la distribuzione completa della dose in ingresso superficiale cos ottenuta pu essere utilizzata per effettuare una stima attendibile della dose efficace , attraverso la definizione di una configurazione equivalente di esposizioni statiche e lutilizzo del programma di calcolo ods - 60 distribuito dalla rti electronic , che determina la dose assorbita dagli organi di un fantoccio virtuale per esami radiologici tradizionali ( quindi con campi rettangolari e in base al dap ) , sulla base di dati ottenuti da simulazioni monte carlo . 
le calibrazioni e le letture dei dosimetri sono state effettuate dalla ditta x - gammaguard di saronno , con valori espressi in termini di equivalente di dose personale hp ( 0 , 07 )  . 
tali valori sono stati convertiti in kerma in aria utilizzando i coefficienti di conversione tabulati [ 12 ] e riferendosi al fascio di taratura utilizzato di energia media 58 kev . 
i valori di kerma in aria sono stati a loro volta convertiti in equivalente di dose alle gonadi tramite lopportuno coefficiente di conversione [ 12 ] pari a 1 , 6 , considerando che la tensione media di lavoro di 80 kv per lapparecchio utilizzato corrisponde ad unenergia media di 44 kev . risultati non sono state registrate differenze statisticamente significative per quanto concerne la volumetria testicolare ( 1825 cc ) ed i dosaggi ormonali sierici nei 2 gruppi studiati . 
in 206 / 223 pazienti ( 92 , 37% ) stato possibile effettuare con successo il trattamento radiologico percutaneo del varicocele ; i controlli flebografici hanno dimostrato le incipienti alterazioni pretrombotiche endoluminali della vena spermatica interna . 
in 17 / 223 pazienti ( 7 , 6% ) ci si limitati ad eseguire la flebografia selettiva diagnostica della vena spermatica a causa di dissezioni intimali invalicabili accidentalmente indotte o per la presenza nel letto da occludere di grossi collettori venosi comunicanti con il circolo sistemico . la durata media della procedura percutanea stata di 30 min ; il secondo controllo flebografico ha comportato un ulteriore impegno di 20 min della sala angiografica . 
il tempo medio di radioscopia continua stato 6 , 3 minuti ( range : 510 min )  . locclusione stata ottenuta mediamente con 3 fiale di atossisclerol ; in 12 pazienti , data la persistente opacizzazioc . 
air kerma values were in turn converted into gonad dose equivalent using the appropriate conversion coefficient of 1.6 [ 12 ] , considering that the mean working current 80 kv for the device used corresponds to a mean energy of 44kev . 
 results there were no significant differences regards testicular volume ( 1825 cc ) and serum hormone levels in the two groups . in 206 / 223 patients ( 92.37% ) , percutaneous treatment of the varicocele was successful ; postprocedural phlebography showed incipient endoluminal prethrombotic alterations of the internal spermatic vein 17 / 223 patients ( 7.6% ) , only diagnostic selective phlebography of the spermatic vein was performed due to either accidental intimal dissections or the presence of large venous vessels communicating with systemic circulation . 
mean duration of the percutaneous procedure was 30 min whereas the second phlebographic examination entailed a further 20 min in the angiography suite . mean duration of continuous fluoroscopy was 6.3 min ( range 510 min )  . 
 occlusion was obtained with an average of three vials of aetoxysclerol ; in 12 patients , treatment was completed with a metallic coil ( 0.038cook coil , 10 mmx50 mm ) and 5 ml of absolute alcohol due to persistent opacification of the varicocele during phlebography . 
in all 206 patients , follow - up at 6 months showed a significant increase in sperm concentration and motility , with negligible morphological changes ( table 3 )  . 
2 distribuzione e collocazione sul fantoccio virtuale della dose superficiale dingresso . ne del varicocele al controllo flebografico , sono stati impiegati a completamento terapeutico una spirale metallica ( cook di 10x50 mm da 0 , 038 pollici ) e 5 ml di alcol assoluto . 
because the procedures did not involve radiography , fluoroscopy time was the most significant exposure parameter ; variability in fluoroscopy time was relatively low , with a standard deviation of 24% . 
figure 2 shows an example of the entrance dose distribution obtained from radiographic films and an indication of its position on the phantom , which we used to calculate the effective dose by defining an equivalent configuration of four static fields . in particular , the gonad doses calculated by the ods - 60 programme corresponded to the direct readings of the thermoluminescent dosimeters , with a 20% tolerance . 
 discussion and conclusions varicocele is a disorder characterised by dilatation of the pampiniform plexus veins secondary to hypertension of the left renal vein ; the presence of circulation between the two gonadal veins may cause increased contralateral pressure with development of milder varicocele on the right side as well . 
27 / 206 , 13 , 1% ; p < 0 , 001 ]  . il trattamento percutaneo ha indotto complicanze minori in 5 pazienti : 2 algie addominali acute di pochi minuti in corso di iniezione di alcol , 2 flogosi del funicolo spermatico trattate con successo mediante terapia medica ed 3 brevi crisi vagali risoltesi spontaneamente . 
nei pazienti che costituivano il gruppo di controllo dello studio e nei 17 pazienti non trattati in corso di follow - up non si sono verificate variazioni significative n dal punto di vista clinico , n per quanto concerne i parametri seminali . 
poich le procedure effettuate non prevedevano lutilizzo della modalit grafia , il tempo di fluoroscopia stato il parametro di esposizione pi significativo per caratterizzare la complessit dellintervento ; la variabilit di tale grandezza risultata essere piuttosto bassa , con un valore di deviazione standard percentuale del 24% . la figura 2 mostra un esempio di distribuzione di dose in ingresso ottenuta dalle pellicole radiografiche e unindicazione della sua collocazione sul fantoccio virtuale utilizzato per il calcolo della dose efficace , attraverso lutilizzo di una configurazione equivalente di quattro campi statici . 
in particolare si verificata la corrispondenza dei valori di dose alle gonadi ricavate dal programma di calcolo ods - 60 con quelli ottenuti dalle misure dirette tramite dosimetri a termoluminescenza , entro una tolleranza del 20% . discussione e conclusioni il varicocele unaffezione caratterizzata dallectasia del plesso pampiniforme secondaria ad uno stato ipertensivo della vena renale sinistra ; lesistenza di circoli tra le 2 vene gonadiche spiega il possibile incremento pressorio controlaterale con insorgenza di varicocele anche a destra , seppur di grado inferiore . 
la possibile associazione tra varicocele ed infertilit ha suggerito di intraprendere sulla popolazione adolescenziale programmi di diagnosi preventiva e di terapia precoce . il trattamento percutaneo del varicocele una procedura paragonabile per efficacia alla correzione chirurgica [ 13 ] ; nellanalisi della giustificazione alla procedura e del rapporto costi / benefici vanno tuttavia considerati il rischio di danno probabilistico radio - indotto , la giovane et dei pazienti ed il basso grado di gravit della patologia . 
nella popolazione in studio , assume quindi una particolare rilevanza radioprotezionistica valutare la dose di esposizione , la dose efficace e la dose equivalente ; per calcolare queste grandezze in corso di procedure interventistiche ( ad elevata dinamicit , non standardizzabili e condotte per lo pi in fluoroscopia ) , si preferito utilizzare un metodo sperimentale in quanto pi preciso del metodo monte carlo . nel campione considerato , significativo seppur limitato , le dosi rilevate rientrano nellordine di grandezza di alcune cation of the procedure and cost - benefit ratio , one has to consider probabilistic risks , patients young age and limited severity of varicocele . 
in the population examined , it was therefore important to evaluate exposure dose , effective dose and equivalent dose ; in order to calculate these doses during interventional procedures ( highly dynamic , nonstandardised and performed using fluoroscopy ) , we opted for an experimental method as it is more accurate than the monte carlo method . 
 in our study population , which was small but significant , doses obtained were within the range of other diagnostic procedures , such as computed tomography , nuclear medicine , etc . 
although definitely below the lower threshold corresponding to the deterministic effect of temporary sterility ( 150 msv ) , gonad dose values recorded ( always lower than 1 msv ) were slightly higher than those previously reported , probably because of the short time of direct exposure of the inguinal region during some phases of the procedure . 
to optimise exposure during the angiographic procedure , we adopted adequate field - limiting measures , never used radiography and limited fluoroscopy time to a maximum of 10 m the principal technical limitation to percutaneous treatment of varicocele is related to the difficulty in achieving selective catheterisation of the internal spermatic vein due to anatomical factors , vasospasm or intimal dissections . 
in cases of incontinence of the cremasteric vein demonstrated by phlebography , in which selective radiological treatment is rarely achievable and which presents a high incidence of recurrences [ 10 , 14 ] , the patient was referred for surgical ligation . 
 in agreement with other authors [ 15 ] , we believe administration of at least 3 ml of sclerosing agent at 3% to be the most effective therapy , allowing occlusion of the pelvic segment of the gonadal vein and simultaneous treatment of abdominal collaterals , at times responsible for long - term recurrence . unlike other authors [ 16 , 17 ] , we used large - calibre metallic coils to rapidly complete the treatment of very large gonadal veins only . 
direct fluoroscopic control during injection of sclerosing agent allowed us to minimise complications associated with possible migration of the embolising agent in the pampiniform plexus and / or systemic circulation . despite the encouraging results obtained in the seminal parameters ( significantly increased sperm concentration and motility ) , fertility of the patients treated cannot be guaranteed [ 1823 ] ; as demonstrated by numerous studies , this depends on several female and male variables related to spermatogenesis and ovulation . 
i valori di dose equivalente alle gonadi registrati ( sempre inferiori al msv ) , pur essendo nettamente al di sotto della prima soglia corrispondente alleffetto deterministico di sterilit temporanea ( 150 msv ) , risultano lievemente superiori a quelli riportati in altri lavori , probabilmente a causa della breve esposizione diretta della regione inguinale durante alcune fasi della procedura . durante le manovre angiografiche , per ottimizzare le esposizioni sono sempre state effettuate opportune diaframmature del campo , non mai stata utilizzata la grafia e si deciso di limitare i tempi di fluoroscopia ad un massimo di 10 min . le difficolt al cateterismo selettivo della vena spermatica interna , correlate a problematiche anatomiche , fenomeni di vasospasmo o a dissezioni intimali , rappresentano la principale limitazione tecnica alla terapia radiologica percutanea del varicocele . nei casi di incontinenza della vena cremasterica dimostrata alla flebografia , in cui come suggerito dalla letteratura [ 10 , 14 ] il trattamento radiologico pu essere assai di rado condotto selettivamente e presenta una considerevole incidenza di recidiva , si preferito inviare il paziente al chirurgo per la legatura inguinale . nella nostra esperienza e secondo altri autori [ 15 ] la condotta terapeutica che garantisce i migliori risultati la somministrazione di almeno 3 ml di sclerosante concentrato al 3% , che consente di occludere la vena gonadica nella porzione pelvica e di trattare contemporaneamente i circoli collaterali addominali , responsabili talvolta di recidiva a distanza . a differenza di quanto descritto in altri lavori [ 16 , 17 ] le spirali metalliche di grande calibro sono state impiegate esclusivamente per completare rapidamente il trattamento di vene gonadiche assai voluminose . 
il controllo fluoroscopico diretto durante liniezione dello sclerosante ha consentito di ridurre al minimo le complicanze correlabili ad indesiderate migrazioni del farmaco nel plesso pampiniforme e / o nel circolo sistemico . gli incoraggianti risultati seminali ottenuti ( significativo incremento di concentrazione e motilit degli spermatozoi ) non ci consentono tuttavia di fare sicure valutazioni circa la fertilit dei pazienti trattati [ 1823 ] ; essa infatti , cos come dimostrato da numerosi studi , dipende da molte variabili maschili e femminili che influenzano la spermatogenesi e lovulazione . ipotizzabile infine che significative variazioni morfologiche delle cellule germinali si rendano apprezzabili solo in corso di follow - up pi estesi nel tempo . il trattamento percutaneo del varicocele si conferma tecnica affidabile , efficace , mininvasiva ed economica attuabile in regime ambulatoriale . 
muzzio1 1dipartimento di scienze medico diagnostiche e terapie speciali , universit degli studi di padova , via giustiniani 2 , i - 35128 padova , italy 2dipartimento di radioterapia e medicina nucleare , azienda ospedaliera di padova , padova , italy correspondence to : d . 
computed tomography ( ct ) , magnetic resonance ( mr ) and positron emission tomography ( pet ) have a very important role in the diagnosis of malignant pleural mesothelioma ( mpm ) in the choice of chemoradiotherapy alone or in combination with surgery and in evaluating possible recurrence . 
we considered 28 patients suffering from mpm whose mean survival after diagnosis was 1518 months . sixteen of these patients had radiotherapy or chemoradiotherapy alone , according to standard protocols , while 12 also underwent surgery . 
nine of the 12 patients who underwent pleuropneumonectomy had no significant survival advantage over the mean survival in the 16 who were not operated whereas the other three lived 13 years longer . 
ct , pet and ct - pet are indicated for diagnosis and , above all , for staging of mpm , in the selection of patients who might benefit from surgery after neoadjuvant therapy and also in identifying small recurrences and / or remote metastases . being highly specific , pet is essential in the follow - up of patients undergoing chemoradiotherapy alone and / or surgery . 
la tomografia computerizzata ( tc ) , la risonanza magnetica ( rm ) e la tomografia per emissione di positroni ( pet ) hanno un ruolo molto importante nella diagnosi del mesotelioma pleurico maligno ( mpm ) , nella scelta del trattamento chemioradioterapico semplice o combinato , eventualmente associato alla chirurgia , e nella identificazione di eventuali recidive . 
in 3 pazienti lincremento della sopravvivenza stato compreso tra 1 e 3 anni rispetto alla media . a questo proposito vengono riportati 2 casi sottoposti a terapia chirurgica dopo una risposta ottimale ai trattamenti chemioradio . 
la tc , la pet e la tc - pet hanno indicazioni nella diagnosi e soprattutto nella stadiazione del mpm , nella accurata selezione dei pazienti da sottoporre alla chirurgia dopo terapia neoadiuvante e nellidentificare la presenza di eventuali piccole recidive e / o di metastasi a distanza . 
mpm has a multifocal origin in a single district and advances by contiguity to serous membranes and adjacent tissues , metastasising only at a late stage . this particular clinical - biological behaviour makes careful staging essential . 
the international mesothelioma interest group ( imig ) [ 4 , 5 ] has recently developed a new staging system based on the traditional tnm staging system , with a view to obtaining a reliable prediction of survival according to tumour extension ( local or distant ) and lymph node involvement , so as to identify patients with a similar prognosis and thus select candidates for surgery . current imaging techniques play a fundamental role in evaluating mpm not only for diagnostic purposes , but also for ensuring a precise tumour staging [ 6 ]  . 
opinions differ in the literature as regards mean survival of patients after multimodal treatment , in the absence of nodal involvement or involvement of the contralateral hemithorax , of pulmonary metastases or subdiaphragmatic spread [ 7 , 8 ]  . materials and methods we reviewed a series of 28 patients with mpm who had been treated over the past 3 years and who survived 1518 months after treatment : 16 were treated with radiotherapy alone ( generally for palliative purposes ) or with chemotherapy and radiotherapy according to specific , partly standardised protocols . in addition to chemoradiotherapy , the other 12 patients also underwent demolitive surgery ( pleural decortication or pleuropneumonectomy with diaphragmatic and at pericardial reconstruction )  . 
all patients underwent ct , which revealed the following findings : relapsing unilateral pleural effusion nodes or plaques of pleural thickening nodosity of the interlobar pleura ring coarctation of the hemithorax calcific plaques obliteration of extrapleural fat planes foci of costal osteolysis hemidiaphragmatic encasement subdiaphragmatic nodosity although suggestive of the disease , these tomographic signs are not specific to the diagnosis of mpm . 
diagnosis was a lungo si discusso sulla eziologia e sulla epidemiologia del mesotelioma pleurico maligno ( mpm ) [ 1 , 2 ] e delle sue correlazioni radiologiche e anatomopatologiche [ 3 ]  . 
recentemente infatti linternational mesothelioma interest group ( imig ) [ 4 , 5 ] ha formulato un nuovo metodo di stadiazione basato sul tradizionale tnm . lobiettivo quello di ottenere informazioni certe sulla sopravvivenza a seconda della estensione del tumore ( locale o a distanza ) e del coinvolgimento linfonodale ; si possono cos inserire i pazienti nellambito di prestabilite categorie che hanno prognosi simile , al fine di identificare con maggiore accuratezza i soggetti potenzialmente resecabili . le tecniche di imaging attualmente disponibili nella valutazione del mpm sono fondamentali non solo per la corretta diagnosi , ma anche per una precisa stadiazione del tumore [ 6 ]  . 
lo scopo di questo lavoro quello di evidenziare : ( 1 ) il ruolo che le metodiche di imaging radiologico , la tomografia computerizzata ( tc ) , la risonanza magnetica ( rm ) , la tomografia per emissione di positroni ( pet ) e la tc - pet hanno nella diagnosi e nella valutazione complessiva del mpm , alla luce della scelta del trattamento terapeutico pi idoneo ( di tipo conservativo o di tipo altamente demolitivo , come la pleuropneumonectomia ) ; ( 2 ) leventuale beneficio che tale intervento pu apportare alla sopravvivenza del paziente . per quanto riguarda la sopravvivenza media dei pazienti sottoposti a trattamento multimodale , in assenza di coinvolgimento linfonodale , dellemitorace controlaterale , di metastasi polmonari e di estensione sottodiaframmatica della malattia , i pareri in letteratura sono discordanti [ 7 , 8 ]  . materiali e metodi abbiamo rivisitato 28 casi di mpm occorsi alla nostra osservazione negli ultimi 3 anni , la cui sopravvivenza media stata di 1518 mesi . 
sedici di questi pazienti sono stati sottoposti a semplici modalit di trattamento : soltanto terapia radiante generalmente usata per una terapia palliativa , chemioterapia e radioterapia secondo precisi schemi in parte standardizzati . 
dodici di questi pazienti sono stati sottoposti a terapia multimodale che oltre ai trattamenti di chemio - radioterapia prevede un approccio chirurgico aggressivo ( decorticazione pleurica o pleuropneumonectomia associata a ricostruzione del diaframma e a volte del pericardio )  . 
tutti i nostri pazienti sono stati valutati mediante tc che complessivamente ha evidenziato i seguenti elementi semeiologici : versamento recidivante monolaterale ; ispessimento nodulare o a placca della pleura ; nodulazioni della pleura interlobare ; coartazione ad anello di un emitorace ; placche calcifiche ; obliterazione dei piani di grasso extrapleurici ; d . 
d micronodulazioni pleuriche diffuse di diametro inferiore ai 5 mm . table 1 characteristics of pleural thickening pleural thickening morphology plaque nodular focal mass simple uni - bilateral calcific micro < 5 mm macro 520 mm > 3 cm tabella 1 caratteristiche dellispessimento pleurico ispessimento pleurico morfologia a placca nodulare massa focale semplice mono - bilaterale calcificata micro < 5 mm macro 520 mm > 3 cm focolai di osteolisi costale ; encasement dellemidiaframma ; nodulazioni sottodiaframmatiche . questi segni tomografici messi in evidenza indirizzano verso un sospetto diagnostico , ma non sono tuttavia specifici per la diagnosi di mpm . 
our study has attempted to highlight the numerous and in some cases unusual morphological patterns of mpm detectable by ct and underline the need for accurate staging of the disease to ensure a correct prognostic and therapeutic approach . 
 despite careful clinical and radiological assessment of our 12 mpm patients subjected to pleuropneumonectomy or pleural decortication , nine had no significant benefit in terms of survival [ 5 , 6 , 1618 ] compared with the mean survival of the 16 patients who did not undergo surgery . 
in un caso infine , abbiamo osservato una formazione nodulare in sede intrascissurale a sinistra senza , tuttavia , segni di versamento pleurico loco - regionale , la cui diagnostica differenziale col fibroma pleurico non stata possibile ( la diagnosi stata posta esclusivamente allintervento chirurgico )  . discussione numerose sono le casistiche di mpm riportate in letteratura [ 5 , 6 , 918 ] con risultati spesso sconfortanti ai fini dellincremento della media della sopravvivenza sia nei pazienti d . 
on this issue , it is worth noting two particularly unfortunate cases of very short survival after surgery despite the fact that surgery was absolutely indicated given the patients positive response to chemotherapy and radiotherapy . 
nel nostro lavoro abbiamo cercato di sottolineare i numerosi e a volte inusuali aspetti morfologici del mpm con la tc e la necessit di una precisa stadiazione ai fini di un corretto approccio prognostico e terapeutico . 
nonostante la valutazione clinico - radiologica estremamente accurata dei 12 pazienti con mpm , sottoposti ad intervento chirurgico di pleuropneumonectomia o di decorticazione pleurica , in 9 di questi d . 
8 la tc dimostra la presenza di placca pleurica nodulare in sede intrascissurale sinistra di mpm ( freccia ) , con minimo versamento . non si sono ottenute significative variazioni dellincremento della sopravvivenza in rapporto alla media dei 16 pazienti non operati [ 5 , 6 , 1618 ]  . 
paziente di 57 anni deceduta dopo 5 mesi . treatment for mpm make us sceptical as to the genuine efficacy of pleuropneumonectomy : although three of our operated patients lived a little longer , the survival gain ( 13 years ) was too limited to justify such aggressive treatment . pet and ct - pet are important in staging disease and identifying recurrences , providing important information on : active pleural nodulation for well - aimed biopsy mediastinal lymph node involvement metastases ( intrathoracic and / or distant ) clearly , the poor spatial resolution of pet is overcome by fusion with ct anatomical images . va , inoltre , ricordata limportanza della pet e della tcpet sia nella stadiazione sia nella identificazione delle recidive . 
tale metodica fornisce , inoltre , importanti informazioni su : nodulazioni pleuriche attive ai fini di una biopsia mirata ; coinvolgimento dei linfonodi mediastinici ; metastasi ( toraciche e / o a distanza )  . naturalmente la insufficiente risoluzione spaziale della pet compensata dalle tecniche di fusione con le immagini anatomiche della tc . conclusions ct , pet and ct - pet have an important , combined role in conclusioni la tc , la pet e la tc - pet trovano nel mpm , prima e dopo terapia semplice o multimodale , un uso combinato che ha come importantissimo scopo sia la selezione di pazienti nel d . 
10a , b pleuropneumectomia sinistra con scomparsa in b delle estese placche pleuriche , evidenti alla tc nel versante mediastinico in a ( frecce )  . paziente di anni 51 deceduto dopo 8 mesi dallintervento . evaluating mpm before and after treatment , in selecting patients potentially eligible for surgery and in detecting recurrences after surgery . 
being highly specific , pet proves helpful for accurate tumour staging and is also essential in the follow - up of patients after chemoradiotherapy both to identify residual neoplastic foci or thoracic recurrences and to detect remote metastasis . it is important to emphasise that thoracic recurrences are often hidden at ct by anatomical structures ( hila , diaphragm , etc . ) or by major anatomical disruption resulting from surgery . each imaging modality has its advantages and limitations , and we recommend their combined use in order to select the most appropriate treatment options . periodo pre - chirurgico , sia la evidenziazione di eventuali recidive nel periodo post - chirurgico . 
per la sua elevata specificit la pet indicata ai fini di una accurata stadiazione del tumore ed indispensabile nel monitoraggio dei pazienti sottoposti a chemio - radioterapia per identificare foci neoplastici residui , recidive intratoraciche ed eventuali metastasi extra - compartimentali . 
 importante sottolineare che le recidive intratoraciche spesso sono nascoste alla stessa tc o dalle strutture anatomiche ( ili , diaframma , etc . ) o dagli importanti sovvertimenti anatomici dovuti alla chirurgia . 
patients with primary mediastinal masses and cysts will usually undergo surgical resection ; radiological and clinical features should prompt limited biopsy specimens followed by oncologic consultation , and chemotherapy or radiotherapy when appropriate . 
the objective of this review was to examine the role of diagnostic imaging in the management of masses of the anterior mediastinum . key words anterior mediastinum thymus neoplasm germcell tumours mesenchymal tumours cysts riassunto i tumori del mediastino sono frequentemente asintomatici e riscontrati incidentalmente ad una radiografia del torace di routine . 
in relazione con il gruppo neoplastico , i tumori primitivi del mediastino anteriore pi comuni sono il timoma , il teratoma ed il linfoma ; tutte le altre lesioni sono rare . 
i pazienti con masse primitive mediastiniche e cisti andranno in genere incontro a resezione chirurgica ; le caratteristiche radiologiche e cliniche dovrebbero suggerire una biopsia limitata della lesione seguita da consulenza oncologica e chemioterapia o radioterapia quando opportune . 
scopo di questa revisione esaminare il ruolo dellimaging diagnostico nella gestione di una massa del mediastino anteriore . parole chiave mediastino anteriore timo , tumore tumori a cellule germinali tumori mesenchimali cisti introduction introduzione a wide spectrum of conditions can present as a space - occupying lesion in the anterior mediastinuthese may be divided into two groups : inflammatory processes and expansile lesions . 
the latter include heterogeneous groups : neoplasms ( primary or secondary ) and nonneoplastic congenital - dysembryoplastic or acquired lesions . unampia variet di condizioni pu presentarsi come lesione occupante spazio nel mediastino anteriore . 
si distinguono processi flogistici e lesioni espansive ; tra queste ultime si riconoscono gruppi eterogenei : condizioni neoplastiche ( primitive o secondarie ) e lesioni , congenite - disembriogenetiche o acquisite , non tumorali . inflammation flogosi mediastinitis and mediastinal abscesses mediastiniti ed ascessi mediastinici a.m. 
more often , the infection reaches the anterior compartment via locoregional spread ( from other mediastinal compartments , from the cervical region or from the lung and pleural cavity )  . 
infections may be classified into diffuse mediastinitis and mediastinal abscesses on the basis of their extension [ 2 ] ; they may be acute or chronic . acute infections are caused by bacteria and in some cases become organised into abscesses ; they are accompanied by symptoms and signs ( retrosternal pain , fever ) and are often fulminant and fatal . 
chronic infection results from mycosis or tubercular processes ; although chronic mediastinitis typically has insidious onset and is not associated with clinical manifestations , some patients show symptoms and signs of obstruction or compression of one or more mediastinal structures . 
in addition to chronic inflammation of infectious origin , there is also a group of mediastinal diseases of unknown origin characterised by accumulation of dense fibrous tissue ( at times systemic ) consisting of granulomatous inflammation . the major radiographic manifestation of acute mediastinitis is mediastinal widening , generally more evident in the upper portions ; the affected region is smoothly marginated . air may be seen in the mediastinum and in the soft tissues of the neck ; there may be pneumoor hydrothorax and multiple abscesses [ 4 ]  . 
the main signs are oesophageal thickening , obliteration and increased density of fat planes , areas of perioesophageal hypodensity , localised fluid collections , single or multiple abscesses , presence of extraluminal gas or contrast material [ 2 , 5 , 6 ] , pleural or pericardial effusion and lymphadenopathy . 
stenosis or occlusion of the superior vena cava may be demonstrated with ct . in rapporto agli altri distretti mediastinici , le flogosi con origine nel mediastino anteriore sono relativamente rare . 
pi spesso il compartimento anteriore raggiunto per diffusione loco - regionale dallevento infettivo ( da altre sezioni del mediastino , dalla regione cervicale oppure dal polmone e dal cavo pleurico )  . 
nella loggia anteriore possono avere origine mediastiniti da causa chirurgica , sequele di interventi di cardiochirurgia o chirurgia esofagea [ 2 ] : in particolare , le mediastiniti postoperatorie si verificano approssimativamente nello 0 , 5%1% dei pazienti sottoposti a sternotomia mediana per interventi di cardiochirurgia [ 3 ]  . 
le infezioni acute sono causate da batteri e talvolta si organizzano in ascessi : si accompagnano a segni e sintomi ( dolore retrosternale , febbre ) e , spesso , sono fulminanti e letali . 
linfezione cronica deriva da micosi o processi tubercolari ; sebbene le mediastiniti croniche siano caratteristicamente insidiose nella comparsa e non associate a manifestazioni cliniche , alcuni pazienti presentano sintomi e segni correlati allostruzione o compressione di una o pi strutture mediastiniche . 
in aggiunta ai casi di infiammazione cronica di origine infettiva , esiste inoltre un gruppo di mediastinopatie ad eziologia sconosciuta caratterizzate dallaccumulo di tessuto denso fibroso ( talvolta a carattere sistemico ) , che consiste in una infiammazione granulomatosa . la maggiore manifestazione radiografica delle mediastiniti acute costituita da un allargamento del mediastino , in genere pi pronunciato negli ambiti superiori ; la regione alterata si presenta con margini lisci e netti . 
la stenosi / occlusione della vena cava superiore pu essere dimostrata con la tc . space - occupying lesions table 1 illustrates the nosography of space - occupying lesions of the anterior mediastinuprimary tumours account la tabella 1 descrive la nosografia delle lesioni occupanti lesioni occupanti spazio a.m. 
in relazione alla clinica , il 75% delle masse mediastiniche in soggetti asintomatici risulta benigno , mentre nei pazienti sintomatici quasi i 2 / 3 sono maligne ; inoltre , l85% dei pazienti affetti da un tumore maligno sintomatico , mentre solo il 46% dei casi di natura benigna si associa a sintomi [ 8 ]  . 
globalmente , il 60% delle lesioni espansive del mediastino presenta sintomi correlati alla compressione o allinvasione diretta delle strutture circostanti , o a sindromi paraneoplastiche ( tabella 2 )  . i pi comuni sintomi da compressione sono dolore toracico , tosse e dispnea ; sindrome della vena cava superiore , sindrome di horner , raucedine e deficit neurologici sono pi frequentemente associati a patologie maligne [ 8 ]  . 
i tumori metastatici sono pi comuni rispetto alle neoplasie primitive e , nel caso del mediastino anteriore , rappresentano pi frequentemente il coinvolgimento linfatico da parte di tumori della mammella e del polmone . tumori le neoplasie del mediastino sono rare , si possono presentare ad ogni et , ma prevalentemente nel iii e iv decennio di vita [ 8 , 9 ]  . 
lincidenza dei tumori primitivi del mediastino , valutata su 1900 pazienti , risultata del 25 , 3% per i tumori neurogenici , 23 , 3% per il timoma , 15 , 3% per i linfomi , 12 , 2% per i tumori a cellule germinali [ 8 ]  . 
oesophagogram reveals an oesophageal tear and a massive leak of barium into the mediastinuc computed tomography ( ct ) scan shows a perioesophageal mediastinal abscess with bilateral pleural effusion and air . 
della componente epiteliale sono stati distinti , nel timo a maturazione , sei sottotipi cellulari ; uno di questi ( tipo vi ) forma i corpuscoli di hassall , caratteristici del timo . 
questi ultimi , localizzati nella zona midollare dei lobuli timici , sono fortable 1 space - occupying lesions benign hyperplasia follicular or lymphoid hyperplasia thymolipoma cysts : congenital , acquired ( inflammation ) lymphoepithelial thymoma ( benign ) mature teratoma immature teratoma ( age < 15 years ) mature teratoma with immature component less than 50% of volume a.m. 
with regard to clinical presentation , 75% of mediastinal masses in asymptomatic subjects are benign whereas almost 2 / 3 of those in symptomatic patients are malignant ; in addition , 85% of patients with a malignancy are symptomatic whereas only 46% of cases of benign disease are associated with symptoms [ 8 ]  . 
overall , 60% of expansile mediastinal lesions are associated with symptoms related to compression or direct invasion of neighbouring structures or paraneoplastic syndromes ( table 2 )  . the most common symptoms resulting from compression are chest pain , cough and dyspnoea . 
metastatic tumours are more common than primary tumours , and those involving the anterior mediastinum are more frequently related to lymphatic involvement by breast or lung cancers . tumours mediastinal tumours are rare , and they may present at any age although predominantly in the third and fourth decades [ 8 , 9 ]  . 
sino allet di 20 anni , pi dell80% della ghiandola costituita da tessuto linfoide : successivamente il suo volume si riduce e lorgano va incontro ad involuzione adiposa , che dopo i 60 anni diviene completa . 
inoltre , tessuto timico ectopico pu essere riscontrato in ogni compartimento mediastinico e nel collo , e spesso risulta indistinguibile dal grasso mediastinico : questa distribuzione giustifica la presentazione dei timomi al di fuori del mediastino anteriore e la possibile persistenza di sintomatologia miastenica dopo timectomia [ 10 ]  . la patologia timica la causa pi comune di allargamento del mediastino anteriore ; laumento di volume del timo riconosce cause molteplici : iperplasia , timoma , carcinoma , carcinoide , timolipoma , cisti , linfomi , seminoma , lesioni secondarie . 
in children , percentages are 43% , 18% and 39% , respectively [ 9 ]  . these differences are justified by a higher incidence of thymic tumours and lymphomas in adults and neurogenic tumours in children . 
therefore , both the subjects age and the site of presentation will help establish a tentative diagnosis . masses of thymic origin thymus the thymus arises from the ventral portion of the third branchial pouch , as do the parathyroid glands . 
six cellular subtypes of the epithelial component have been identified in the mature thymus ; one of these ( type vi ) forms hassall bodies , which are characteristic of the thymus . these are located in the thymic medulla and are formed by concentrically arranged , involuted epithelial cells ; the core cells are keratinized , calcific or necrotic and may undergo lysis with the consequent formation of cysts . 
its weight at birth is on average 22 g , increasing to 35 g at puberty . until the age of 20 years , more than 80% of the gland is made up of lymphoid tissue ; subsequently , it shrinks and undergoes fatty involution , which is complete after the age of 60 years . various events can cause its enlargement ( stress ) or shrinkage . 
in addition , ectopic thymic tissue may be found in every mediastinal compartment and in the neck and is often indistinguishable from mediastinal fat . this distribution accounts for the fact that thymomas may present outside the anterior mediastinum and the possible persistence of myasthenia , even after thymectomy [ 10 ]  . thymic disease is the most common cause of widening of the anterior mediastinuthymic enlargement may have a variety of causes : hyperplasia , thymoma , carcinoma , carcinoid tumour , thymolipoma , cysts , lymphoma , seminoma or secondary lesions . although lymphoma , carcinoid tumours and germ - cell tumours may develop within the thymus , only thymomas , thymic carcinomas and thymolipomas arise from thymic precursors . cellule germinali possano svilupparsi nel timo , soltanto i timomi , i carcinomi del timo ed i timolipomi derivano da precursori timici . iperplasia timica vera liperplasia timica vera , contrapposta alliperplasia linfoide associata alla miastenia gravis , definita come incremento nella dimensione della ghiandola in presenza di una normale architettura istologica [ 11 ]  . 
possibile il riscontro anamnestico di eventi causa di stress , quali la sepsi o le ustioni massive . la maggior parte dei soggetti , alla diagnosi , sono bambini o giovani adulti [ 11 ] : in genere asintomatica . 
anche la rm ha un valore limitato [ 17 ]  . timolipoma un tumore infrequente a lenta crescita , benigno , costituito da una commistione di tessuto adiposo maturo e di tessuto timico linfoepiteliale ; rappresenta l1%10% di tutti i tumori del timo [ 18 ]  . 
sono state formulate diverse ipotesi patogenetiche : potrebbe rappresentare un lipoma che insorge nel timo , un tumore misto ( lipoma e timoma ) o uniperplasia timica vera che successivamente regredisce per involuzione aditrue thymic hyperplasia true thymic hyperplasia , as opposed to the lymphoid hyperplasia associated with myasthenia gravis , is defined as enlargement of the gland in the presence of normal histological architecture [ 11 ]  . 
it may result from atrophy due to antiblastic chemotherapy ( generally for lymphoma or germ - cell tumour ) [ 13 ] or from hypercortisolism [ 14 ] ; more frequently , however , there is no correlation with other conditions and the finding is incidental . 
there may be a history of stressful events , such as sepsis or massive burns . at diagnosis , most subjects are children or young adults [ 11 ] , and the condition is usually asymptomatic . 
in children , the radiological finding , which is often incidental , is sufficient for diagnosis , and the condition requires no treatment . in adults , a tentative diagnosis may be made in the presence of a history of anticancer treatment ; without this , biopsy is mandatory . 
microscopicamente , i centri germinativi sono assenti ( anche in presenza di miastenia gravis ) , le calcificazioni e la degenerazione cistica dei corpuscoli di hassall sono comuni [ 20 ]  . 
laspetto radiografico consiste di una massa del mediastino anteriore con forma a campana [ 7 , 18 , 19 ] , con estensione in uno o entrambi gli emitoraci ; pu simulare cardiomegalia o elevazione del diaframma , mentre , quando di piccole dimensioni , ha forma rotonda o ovale . 
per la consistenza molle pu modificare forma ( che si adegua alle strutture circostanti ) e posizione in relazione al diverso decubito del paziente [ 19 ]  . alla tc mostra caratteristicamente lattenuazione del grasso , o densit equivalente a grasso e tessuti molli . 
spesso la massa connessa al timo da un piccolo peduncolo [ 19 ]  . la rm dimostra lelevata intensit di segnale , tipica del grasso , nella sequenza se t1 pesata ed aree di segnale intermedio correlate ai tessuti molli [ 21 ]  . 
le caratteristiche peculiari del timolipoma evidenti alla radiografia ed alla tc consentono la diagnosi differenziale nella maggior parte dei casi ; quando la componente adiposa predominante pu essere confuso con un lipoma mediastinico . cisti timiche le cisti del timo sono infrequenti e rappresentano solo il 3% di tutte le masse del compartimento anteriore [ 8 ]  . 
le masse si proiettano sul lato destro del mediastino . con alcune condizioni neoplastiche ( linfoma di hodgkin , seminoma , carcinoma timico ) , per una parte dopo trattamento ( radioterapia , toracotomia ) [ 22 , 23 ]  . 
la maggior parte deriva probabilmente dai residui del dotto timofaringeo fetale e possono , pertanto , essere riscontrate in qualsiasi punto , dal collo sino al mediastino anteriore , lungo il percorso di migrazione embriologica del timo [ 24 ]  . circa la met delle cisti congenite sono di riscontro occasionale nei primi due decenni di vita [ 24 ] , mentre le cisti reattive si presentano in soggetti adulti asintomatici . 
nella parete cistica pu essere identificato focalmente tessuto timico normale e questo riscontro necessario per la diagnosi e per la diagnosi differenziale con alcune condizioni neoplastiche ( timoma , linfoma di hodgkin , tumori a cellule germinali ) che possono presentare un aspetto cistico dominante [ 25 ]  . il quadro radiologico , al radiogramma del torace , consiste in un espanso del mediastino antero - superiore a margini lisci , ben circoscritto [ 26 ] ; quando ha dimensioni cospicue pu simulare una cardiomegalia . 
presenta una bassa intensit di segnale nelle sequenze rm t1 pesate , che diviene alta sulle immagini t2 [ 21 ] , se non complicata ( emorragia intracistica , contenuto proteinaceo )  . timoma linfoepiteliale le neoplasie del timo costituiscono il 30% di tutte le masse del mediastino anteriore in et adulta [ 27 ] , mentre sono meno comuni nel bambino , dove rappresentano solo il 15% degli espansi di questa sede [ 28 ]  . 
tuttavia , dal momento che il timoma evolutivo privo delle caratteristiche citologiche ed istologiche di malignit e dal punto di vista microscopico identico al timoma capsulato , la dizione di timoma invasivo da preferirsi a timoma maligno [ 29 ]  . 
inoltre , in presenza di atipia citologica ed elevato indice mitotico sono pi propriamente definiti carcinomi timici . il timoma il tumore primitivo pi comune del mediastino anteriore : rappresenta circa il 20% di tutti i tumori del mediastino . 
ha una lieve predilezione per il sesso femminile , con et media di incidenza nel v - vi decennio di vita [ 30 ] , mentre di raro riscontro nellinfanzia e nelladolescenza . la variabilit istologica ha suggerito diverse classificatomy [ 15 ]  . 
even magnetic resonance imaging ( mri ) is of limited value [ 17 ]  . thymolipoma this is an uncommon , slow - growing , benign tumour made up of a mixture of mature adipose tissue and lymphoepithelial thymic tissue ; it accounts for 1%10% of all thymic tumours [ 18 ]  . 
it may be a lipoma arising in the thymus , a mixed tumour ( lipoma and thymoma ) or a true thymic hyperplasia that subsequently regresses due to fatty involution . 
there is no gender predilection , and although it may manifest at any age , young adults seem to be most commonly affected by the disease [ 19 ]  . 
microscopically , it has no germinal centres ( even in the presence of myasthenia gravis ) , and calcification and cystic degeneration of the hassall bodies are common [ 20 ]  . the radiographic pattern consists of a bell - shaped mass within the anterior mediastinum [ 7 , 18 , 19 ] extending to one or both hemithoraces ; it may mimic cardiomegaly or diaphragmatic elevation . 
given the soft texture of these tumours , they may vary in shape ( adapting to the surrounding structures ) and location , depending on the patients position [ 19 ]  . at ct , they typically have fat attenuation or density of fat and soft tissue . 
mri reveals high signal intensity , typical of fat , in the t1 - weighted spin - echo ( se ) sequence and areas of intermediate signal related to soft tissues [ 21 ]  . the peculiar radiographic and ct features of thymolipoma allow differential diagnosis in most cases ; when the fatty component prevails , the condition may be mistaken for a mediastinal lipoma . thymic cysts thymic cysts are uncommon , accounting for only 3% of all anterior mediastinal masses [ 8 ]  . 
they may be congenital or acquired . the latter are due to inflammation or are associated with certain neoplasms ( hodgkins lymphoma , seminoma , thymic carcinoma ) , in some cases after treatment ( radiotherapy , thoracotomy ) [ 22 , 23 ]  . acquired cysts are thought to derive from dilatation of the epithelial component due to inflammation of the thymic parenchyma . 
most cysts probably derive from remnants of the foetal thymopharyngeal duct and may therefore be found anywhere between the neck and the anterior mediastinum along the embryological migration route of the thymus [ 24 ]  . 
in ambito clinico la classificazione anatomo - chirurgica di masaoka , che distingue iv stadi ( i , macroscopicamente capsulato senza invasione microscopica della capsula ; ii , invasione macroscopica nel tessuto adiposo circostante o a livello della pleura mediastinica o invasione microscopica della capsula ; iii , invasione macroscopica negli organi adiacenti pericardio , grossi vasi , polmone ; iva , disseminazione pleurica o pericardica , ivb , metastasi linfatiche o ematogene ) , condiziona leventuale integrazione terapeutica ( radioterapia e chemioterapia adiuvanti ) ed ha dimostrato una valida correlazione prognostica [ 31 ]  . circa la met di questi tumori sono asintomatici e di riscontro casuale alla radiografia del torace . 
nei pazienti sintomatici , il 40% presenta miastenia gravis , mentre in altri casi lamentano dolore toracico e sintomi da emorragia acuta intralesionale o compressione delle strutture mediastiniche [ 30 ]  . la maggior parte ( 90% dei casi ) origina nella porzione superiore del mediastino anteriore , che corrisponde alla sede usuale del timo , situata in prossimit della giunzione tra il cuore ed i grossi vasi ( pu tuttavia presentarsi in ogni altra sede , dal collo allangolo cardiofrenico ) ; ben capsulata ed ha forma rotonda o lievemente lobulata , di dimensioni in genere variabili tra 5 e 15 cm di diametro [ 32 ]  . 
generalmente si presenta come lesione solida , talvolta ha aspetto cistico [ 25 ] : fino ad 1 / 3 dei casi mostra necrosi , emorragia , calcificazioni ed aree di colliquazione cistica . 
nonostante questa difficolt chirurgica , laspetto citologico rimane benigno [ 32 ]  . linvasivit documentata dal riscontro istologico , sul pezzo operatorio , di cellule tumorali oltre il confine della capsula : indipendentemente dalla dimensione , almeno 1 / 3 dei timomi presenta infiltrazione della capsula con conseguente estensione nel grasso mediastinico [ 32 ]  . 
a seconda delle casistiche [ 29 , 32 , 33 ] , nel 30%50% dei casi viene documentata linfiltrazione della pleura , del polmone , della parete toracica , del pericardio , dei grossi vasi mediastinici , dellatrio destro o del diaframma : la prognosi correla con linvasione extracapsulare . 
inoltre , si pu verificare lestensione attraverso il diaframma in addome o nel retroperitoneo e linsemenzamento metastatico loco - regionale della pleura omolaterale e del pericardio [ 29 ]  . 
la diffusione linfonodale e sistemica sono evenienze rare [ 32 ] e possono verificarsi sia nella forma invasiva sia , eccezionalmente , nella variante capsulata . sebbene la stadiazione chirurgico - patologica proposta da masaoka sia universalmente accettata , alcuni punti di controversia rimangono : in particolare , molti timomi capsulati presentano una tendenza a recidivare localmente nonostante unexeresi radicale . 
by contrast , cysts associated with a neoplasm are frequently symptomatic . most congenital cysts are smaller than 6 cm , spherical , unior multilobulated and have thin walls without an inflammatory component . 
cyst walls may show foci of normal thymic tissue , a finding necessary for diagnosis and differentiating these cysts from neoplasms ( thymoma , hodgkins lymphoma , germ - cell tumours ) presenting with a predominantly cystic appearance [ 25 ]  . chest radiography shows a smoothly marginated , wellcircumscribed expansile mass of the anterosuperior mediastinum [ 26 ] ; when large , it may mimic cardiomegaly . 
thymomas are the most frequent neoplasms of the thymic epitheliuthey may have benign or malignant behaviour . however , because malignant thymomas do not display the cytological and histological features of malignancy and fig . 
in alcuni casi , la bassa attenuazione non assoluta , ma i valori di attenuazione sono analoghi a quelli dei tessuti molli a causa del contenuto mucoso o calcio . includendo anche il concetto di adesivit oltre quello di invasivit locale . 
alcuni timomi , infatti , presentano una reazione fibrosa pericapsulare priva di cellule neoplastiche , che si manifesta microscopicamente sotto forma di aderenze fibrose con la pleura parietale o con il pericardio : queste aumentano il rischio di recidiva locale . radiologicamente il timoma ha forma rotonda od ovale ed i margini sono lisci o lobulati , ben demarcati . 
si presenta nel mediastino antero - superiore , origina da uno dei lobi timici e , nella presentazione pi usuale , cresce verso un lato della linea mediana ; pu , peraltro , protrudere da entrambi i lati del mediastino ( lestensione bilaterale comunque meno comune ) e dislocare il cuore ed i grossi vasi posteriormente . le calcificazioni , non molto frequenti ( 20% nella nostra esperienza ) , sono pi spesso a grano di sale ( a differenza del teratoma dove in genere sono laminari ) [ 35 ]  . 
la densit omogenea [ 35 ] , tranne nelle lesioni di maggior dimensione nelle quali la presenza di emorragia , necrosi o formazioni cistiche produce aree focali di ipodensit [ 26 ]  . 
anche la tc non consente una distinzione preoperatoria attendibile del carattere di invasivit , a meno di grossolani reperti , suggestivi di infiltrazione , a carico dei grossi vasi , della pleura o di irregolarit delle interfacce con il polmone [ 35 ]  . 
lintensit di segnale rm intermedia ( equivalente o superiore a quella del muscolo scheletrico ) nella sequenza t1 pesata ed incrementata ( prossima a quella del tessuto adiposo ) nella t2 . 
la rm particolarmente utile nel dirimere un dubbio di invasione di strutture vascolari . alla diagnosi la met dei timomi risulta sintomatica : si rivelano per sintomi locali ( compressione ed invasione di strutture toraciche in 1 / 3 dei pazienti : dolore toracico , tosse , dispnea , disfagia ; sindrome della vena cava superiore ) o sistemici ( sindromi paraneoplastiche )  . 
la miastenia gravis la condizione paraneoplastica pi frequente : circa il 10%15% dei soggetti miastenici ha il timoma e circa il 35%40% dei pazienti affetti da timoma presenta la miastenia [ 32 ]  . lasportazione del timo migliora la clinica del paziente in molte delle condizioni morbose paraneoplastiche ; in particolare , circa il 70% dei pazienti miastenici con timoma mostra un graduale miglioramento dei sintomi in seguito alla timectomia [ 33 ] ; la remissione completa varia dal 7% al are microscopically identical to the encapsulated forms , the term invasive thymoma is preferred to malignant thymoma [ 29 ]  . 
moreover , in the presence of cytological atypia with high mitotic index , these thymomas are more appropriately referred to as thymic carcinomas . thymoma is the most common primary tumour of the anterior mediastinum and accounts for about 20% of all mediastinal tumours . 
in clinical practice , masaokas surgical - pathological classification into four stages ( i encapsulated tumour without gross or microscopic invasion of the capsule ; ii macroscopic invasion into the mediastinal fat or pleura or microscopic invasion into the capsule ; iii gross invasion of the adjacent organs : pericardium , great vessels , lung ; iva pleural or pericardial spread , ivb lymphatic or haematogenous metastases ) affects adjuvant treatment ( adjuvant radiotherapy and chemotherapy ) and has proved to correlate well with prognosis [ 31 ]  . about half of these tumours are asymptomatic and incidentally discovered at chest radiography . 
the others complain of chest pain and symptoms of acute intralesional haemorrhage or compression of mediastinal structures [ 30 ]  . most tumours ( 90% ) originate in the upper portion of the anterior mediastinum , which corresponds to the usual location of the thymus , near the junction between the heart and the great vessels ( they may , however , arise anywhere between the neck and the cardiophrenic angle )  . 
tumours are well encapsulated , have rounded or slightly lobular shape and are generally between 5 cm and 15 cm in diameter [ 32 ]  . they usually manifest as a solid lesion , and in some cases they have cystic appearance [ 25 ]  . 
up to 1 / 3 show necrosis , haemorrhage , calcification and areas of cystic colliquation . they may be encapsulated , more or less adherent to the surrounding structures , or frankly invasive [ 32 ]  . 
irrespective of size , at least 1 / 3 of thymomas show capsular infiltration with extension into the mediastinal fat [ 32 ]  . depending on the case series [ 29 , 32 , 33 ] , 30%50% of cases show evidence of infiltration of the pleura , lung , chest wall , pericardium , great mediastinal vessels , right atrium or diaphragprognosis is correlated with extracapsular invasion . 
in addition , the tumour may extend through the diaphragm into the abdomen or retroperitoneum , or there may be locoregional metastatic seeding of the ipsilateral pleura and pericardium [ 29 ]  . 
quasi il 15% dei pazienti con timoma sviluppa un secondo tumore : sarcoma di kaposi , chemodectoma , mieloma multiplo , leucemia acuta e carcinomi ( polmone , colon )  . una resezione chirurgica completa considerata il trattamento di scelta . 
in generale , una terapia complementare di associazione ( radioterapia , chemioterapia ) prescritta in tutti i casi dopo resezione chirurgica , ad eccezione dei timomi ben capsulati , che allesame istologico non presentano invasione microscopica e senza aderenze mediastiniche al tempo operatorio [ 38 ]  . 
per il rischio di persistenza / recidiva , indispensabile un programma di controlli radiologici seriati a lungo termine . carcinoma timico questa dizione riservata a quei tumori epiteliali maligni del timo che possiedono caratteristiche citologiche ed istologiche patognomoniche di malignit : atipia nucleare / citologica , elevata attivit mitotica , necrosi [ 39 ]  . 
in genere si presentano come massa bulky ( 515 cm ) del mediastino anteriore , dai margini lobulati o poco definiti [ 40 ] ed alla diagnosi invadono i piani adiposi circostanti e le strutture adiacenti . 
la distinzione tra carcinoma primitivo e metastatico pu essere difficile sulla base del solo esame istologico : lassenza di un tumore polmonare lelemento discriminativo di maggiore affidabilit ( essendo infrequente la presenza di secondariet di origine extrapolmonare ) [ 41 ]  . alla tc possono presentare una attenuazione omogenea da tessuti molli o eterogenea per la presenza di necrosi ; come il timoma , pu avere aspetto cistico [ 25 ] ; sono presenti calcificazioni nel 10%40% dei casi . 
linfoadenopatie mediastiniche sono presenti nel 40% dei casi [ 42 ]  . dal punto di vista clinico , la maggior parte dei pazienti sono asintomatici alla diagnosi ; al confronto con il timoma , non sono comuni le manifestazioni paraneoplastiche . 
la prognosi infausta , condizionata da una crescita intratoracica progressiva ( metastasi pleuriche , polmonari ed ai linfonodi mediastinici , cervicali ed ascellari ) e dalla metastatizzazione a distanza ( osso , fegato ) nella maggior parte dei pazienti . 
quando si riscontri alla tc una massa timica bulky con invasione dei grossi vasi , coinvolgimento linfonodale , paralisi del nervo frenico o metastasi ematogene , dovrebbe essere considerata lipotesi diagnostica del carcinoma timico piuttosto che il timoma invasivo [ 43 ]  . neoplasie neuroendocrine del timo comprendono diverse variet , con caratteristiche comuni sotto laspetto istologico e immunoistochimico : verosimile che rappresentino uno spettro di differenziazione , piuttosto che entit nosografiche specifiche . 
listotipo pi frequente il carcinoide ( tipico e atipico ) , identico nellistologia e nella clinica ( sindromi paraneoplastiche ) ad ogni altra presentazione extratimica . interessano ogni fascia di et , con media alla diagnosi di a.m. 
allo studio coronale rm fast spin - echo t1 - pesata , il timoma capsulato si manifesta come una massa del mediastino anteriore omogenea , lobulata . although masaokas surgical - pathological staging system is universally accepted , there are still some controversial points : in particular , many encapsulated thymomas tend to recur locally despite radical resection . 
to shed light on this controversial aspect , in 1996 , a japanese team [ 34 ] revised masaokas classification to include the notion of adhesiveness as well as local invasiveness . 
some thymomas , in fact , have a fibrous pericapsular reaction free of tumour cells , which manifests microscopically in the form of fibrous adhesions to the parietal pleura or pericardiu these adhesions increase the risk of local recurrence . radiologically , thymomas have a rounded or oval shape and smooth or lobulated , well - defined margins . 
possono , altre volte , essere presenti segni e sintomi di compressione e invasione locale , o sindromi paraneoplastiche , queste ultime presenti in circa 1 / 3 dei pazienti [ 44 ]  . 
contrast - enhanced computed tomography ( ct ) scan demonstrates an inhomogeneous anterior mediastinal mass with focal areas of calcification , nodular left pleural thickening and a left pleural effusion ; the mass is associated with focal obliteration of fat planes in close relationship to the aortic arch and main pulmonary artery . 
una scansione tc dopo mezzo di contrasto dimostra una massa disomogenea del mediastino anteriore con aree focali di calcificazione , ispessimento nodulare pleurico sinistro e versamento pleurico sinistro ; la massa associata con obliterazione focale dei piani adiposi , in stretta prossimit con larco aortico e larteria polmonare . 
computed tomography ( ct ) scan : large , well - defined mass adjacent to ascending aorta and superior vena cava contains solid component . it presents inhomogeneous attenuation with foci of calcification . 
at surgery , a thymoma was found , with solid areas surrounded by a thick , fibrous capsule . right posterior mediastinal thymic tissue is present due to lobulated pleural implants , without pleural effusion . 
tc : una grossa massa a margini ben definiti adiacente al tratto ascendente dellaorta ed alla vena cava superiore ha contenuto solido : mostra attenuazione disomogenea per presenza di focali calcificazioni . 
the common denominator of disorders associated with thymoma is a condition of autoimmunity neuromuscular syndromes haematological disorders autoimmune diseases endocrine disorders miscellaneous myasthenia gravis eaton - lambert syndrome paraneoplastic polyneuropathy limbic encephalopathy stiff - person syndrome pure erythrocyte aplasia aplastic anaemia low platelet count hypogammaglobulinaemia t lymphocytosis t - cell deficiency syndrome agranulocytosis hyperthyroidism hyperparathyroidism addisons disease panhypopituitarism cushings syndrome thyroiditis hypertrophic osteoarthropathy nephrotic syndrome primary glomerulonephritis with minimal lesions polymyositis systemic lupus erythematosus hashimoto thyroiditis rheumatoid arthritis pernicious anaemia scleroderma graves disease sjgrens syndrome sarcoidosis tabella 3 sindromi paraneoplastiche e condizioni associate a timoma . 
la funzione del timo la produzione di linfociti t immunocompetenti , per proliferazione e maturazione di linfociti immaturi del midollo osseo : nellambito della patologia il comune denominatore delle condizioni associate a timoma rappresentato da un carattere di autoimmunit sindromi neuromuscolari disordini ematologici malattie autoimmuni disordini endocrini miscellanea miastenia gravis sindrome di eaton - lambert polineuropatia paraneoplastica encefalopatia limbica sindrome di stiff - person aplasia eritrocitaria pura anemia aplastica piastrinopenia ipogammaglobulinemia linfocitosi t sindrome da deficienza di cellule t agranulocitosi polimiosite lupus erythematosus sistemico tiroidite hashimoto artrite reumatoide anemia perniciosa sclerodermia malattia di graves sindrome di sjgren sarcoidosi ipertiroidismo iperparatiroidismo morbo di addison panipopituitarismo sindrome di cushing tiroidite osteoartropatia ipertrofica sindrome nefrosica glomerulonefrite primitiva a lesioni minime sent in the anterosuperior mediastinum , originate from one of the thymic lobes and typically project onto one side of the midline . 
more rarely , however , they may extend on either side of the mediastinum and displace the heart and great vessels posteriorly . calcifications , which are relatively infrequent ( 20% in our experience ) , are often salt - grain calcifications ( unlike teratoma , where they are usually laminar ) [ 35 ]  . 
density is homogeneous [ 35 ] except in larger lesions in which the presence of haemorrhage , necrosis or cysts produces focal areas of low density [ 26 ]  . 
nonetheless , ct is not capable of reliably identifying invasiveness prior to surgery unless there are evident signs of infiltration of the great vessels or pleura or irregularities of the interfaces with the lung [ 35 ]  . 
signal intensity at mri is intermediate ( equal to or higher than that of skeletal muscle ) in t1 - weighted sequences and increased ( approaching that of fat ) in t2 . 
cystic areas with fluid la radiografia del torace pu risultare anche normale , evenienza plausibile in caso di sindrome di cushing ; invece , tumori non secernenti o men si presentano pi frequentemente come grosse masse del mediastino anteriore [ 45 ]  . alla tc la densit omogenea o , pi frequentemente , eterogenea per necrosi , emorragia e calcificazioni puntiformi e distrofiche [ 7 ] ; possono assumere il mezzo di contrasto . 
le metastasi ossee sono tipicamente osteoblastiche . tumori con origine da cellule staminali : neoplasie a cellule germinali il termine si riferisce ad un gruppo di tumori identici per aspetto istologico ad alcune neoplasie del testicolo e dellovaio , che nellinsieme si ritiene derivino da elementi germinali primitivi comuni . 
costituiscono un insieme eterogeneo di lesioni , benigne e maligne , a localizzazione mediastinica come conseguenza di un errore disembriogenetico per interruzione della migrazione , per la colonizzazione delle gonadi , di elementi staminali lungo la cresta urogenitale . si riscontrano pertanto lungo la linea mediana del corpo , dalla ghiandola pineale allarea presacrale , poich questa linea direttiva corrisponde alla cresta urogenitale embrionale . 
il mediastino rappresenta la sede pi comune delle localizzazioni extragonadiche e , in particolare , il compartimento anteriore il pi frequentemente interessato : infatti , content show hypointense signal in t1 and hyperintense in t2 . 
symptoms may be local ( compression and invasion of thoracic structures in 1 / 3 of patients : chest pain , cough , dyspnoea , dysphagia ; superior vena cava syndrome ) or systemic ( paraneoplastic syndromes )  . 
about 10%15% of myasthenic subjects have thymoma , and about 35%40% of patients with thymoma have myasthenia [ 32 ]  . thymic resection improves the clinical picture in many paraneoplastic syndromes . 
almost 15% of patients with thymoma develop a second tumour : kaposis sarcoma , chemodectoma , multiple myeloma , acute leukaemia and carcinomas ( lung , colon )  . complete surgical resection is the treatment of choice . 
in general , adjuvant therapy ( radiotherapy , chemotherapy ) is prescribed in all cases after resection , except for well - encapsulated thymomas not showing microscopic invasion at histology and mediastinal adhesions at surgery [ 38 ]  . 
due to the risk of persistence and recurrence , long - term radiological follow - up is mandatory . thymic carcinoma features the term thymic carcinoma is reserved for those malignant epithelial tumours of the thymus that have cytological and histological of malignancy : nuclear / cytological atypia , high mitotic index , necrosis [ 39 ]  . they form a diverse group of rare and aggressive epithelial tumours with a strong tendency towards early local invasion and metastatic spread . pathognomic there are no distinctive radiological features . 
thymic carcinomas generally present as a bulky mass ( 515 cm ) of the anterior mediastinum , with lobulated or poorly defined margins [ 40 ] , which at diagnosis are found to invade surrounding fat planes and adjacent structures . 
as in the case of thymoma , it may have a cystic appearance [ 25 ] ; calcification is present in 10%40% of cases . mediastinal lymphadenopathy is seen in 40% of cases [ 42 ]  . most patients are clinically asymptomatic at presentation . compared with thymoma , paraneoplastic manifestations are rare . 
prognosis is poor as a result of progressive intrathoracic growth ( metastases to the pleura and lungs and mediastinal , cervical and axillary lymph nodes ) and distant metastasis ( bone , liver ) in most patients . 
nella maggior parte dei casi , la neoplasia diviene manifesta nel giovane adulto , con et media alla diagnosi tra iii e v decennio [ 47 ]  . sono classificati in forme benigne ( 80% dei casi ) e maligne . 
i tumori maligni comprendono i seminomi , i tumori non seminomatosi ed una parte dei teratomi ( teratomi immaturi in et superiore a 15 anni ; teratomi con trasformazione maligna )  . 
in et pediatrica , invece , si presentano con uguale distribuzione per sesso . i tumori benigni sono in genere asintomatici ; al contrario , quasi la totalit dei pazienti affetti da neoplasie maligne manifesta sintomi : dolore toracico , dispnea , tosse , febbre o manifestazioni da compressione ed invasione delle strutture mediastiniche circostanti . tra le forme benigne listotipo pi comune il teratoma maturo , che rappresenta il 45%75% dei casi [ 48 ]  . 
inoltre , i tumori a cellule germinali del mediastino hanno propensione a sviluppare una componente di malignit non germinale ( rabdomiosarcoma , adenocarcinoma , tumori neuroectodermici ) che pu diventare listologia prevalente . 
stata descritta la relazione tra queste neoplasie e la sindrome di klinefelter ( cariotipo 47 , xxy ) , con unassociazione pari a quasi l8% dei casi [ 49 ]  . 
pi del 95% dei radiogrammi sono alterati , per la presenza di una massa localizzata il pi delle volte in mediastino anteriore ( solo 3%8% in mediastino posteriore ) [ 50 ]  . 
sebbene debba essere sempre effettuato lesame obiettivo del testicolo , incluso lapprofondimento ecotomografico , la presenza di una massa isolata in mediastino anteriore senza coinvolgimento retroperitoneale non suggestiva per lorigine primitiva testicolare . 
the most frequent histological type is carcinoid tumour ( typical and atypical ) , which is histologically and clinically ( neoplastic syndromes ) identical to all other extrathymic presentations . these tumours can affect all age groups , with a mean age at diagnosis of 45 years . 
half are well circumscribed or encapsulated ; the others invade the pleura , pericardium , diaphragm and mediastinal structures . chest radiography may even be normal , which is understandable in the case of cushings syndrome ; in contrast , nonsecreting tumours or men more frequently appear as large masses of the anterior mediastinum [ 45 ]  . ct attenuation is homogeneous or , more often , heterogeneous due to necrosis , haemorrhage and punctuate and dystrophic calcification [ 7 ]  . 
bone metastases are typically osteoblastic . tumours originating from stem cells : germ - cells neoplasms the term refers to a group of tumours with identical histology to some neoplasms of the testicle and ovary , all of which are believed to derive from common primary germ cells . they form a diverse group of benign and malignant lesions that develop in the mediastinum as a consequence of an embryogenic error interrupting the migration of stem cells along the urogenital ridge to the gonads . they therefore arise along the midline between the pineal gland and the presacral area , as this line corresponds to the embryonic urogenital ridge . 
la tc pu , inoltre , dimostrare la presenza di metastasi polmonari o lirregolarit dellinterfaccia con il polmone segno di infiltrazione per contiguit , oltre allestensione alla parete toracica , il coinvolgimento linfonodale mediastinico e le metastasi a distanza [ 40 , 51 ]  . la valutazione sierologica di - fetoproteina ( - fp ) e gonadotropina corionica umana ( - hcg ) utile nella gestione del paziente con sospetto clinico - radiologico di tumore maligno a cellule germinali , sia nella diagnosi sia nel follow - up . 
lelevazione di questi marcatori , singola o congiunta , si riscontra nell80%85% dei tumori non seminomatosi ; la sola - fp alterata nel 60%80% dei casi , mentre dal 30% al 50% di questi tumori presenta un incremento di hcg [ 52 ]  . 
i seminomi puri possono associarsi ad una alterazione della - hcg ( a bassi livelli ) con - fp mai mossa . teratoma un tumore rappresentato da tessuto derivante da uno o tutti e tre i foglietti embrionali germinali : queste linee non costituiscono una struttura organizzata . 
riconosce tre tipi istologici : ( 1 ) maturo , ( 2 ) immaturo e ( 3 ) con trasformazione maligna . i teratomi maturi costituiscono la variante pi comune : rappresentano il 70% dei tumori a cellule germinali del mediastino in et pediatrica ed il 60% nelladulto [ 46 , 50 ]  . sono ben delimitati rispetto alle strutture mediastiniche circostanti e sono uni o multicistici ; le forme solide sono di riscontro raro [ 53 ]  . 
alla diagnosi il paziente in genere asintomatico , e la diagnosi dunque incidentale al radiogramma del torace , ma , poich presentano dimensioni cospicue ( 810 cm ) , possono causare sintomi locali [ 53 ]  . 
dal punto di vista istologico , sono costituiti da tessuti adulti ben differenziati , arrangiati in modo irregolare , di derivazione ectodermica ( cute e suoi annessi quali denti , peli , ghiandole sudoripare e sebacee ) , mesodermica ( cartilagine , osso , grasso , tessuto muscolare liscio ) ed endodermica ( epitelio bronchiale , intestinale e tessuto pancreatico )  . 
altri tessuti relativamente comuni includono : cartilagine , grasso , tessuto muscolare liscio e mucosa respiratoria ; osso , denti , tessuto gliale e mucosa enterica sono di meno frequente riscontro . 
moeller [ 54 ] ha riportato la frequenza delle componenti a maggiore rappresentazione : liquido 88% , grasso 76% , calcificazioni 53% , i tre elementi of thymic tissue at the periphery of some of these tumours suggests that they originate in the thymus . 
in most cases , the tumour becomes manifest in the young adult , with an age range at diagnosis between the third and fifth decade [ 47 ]  . these tumours are classified into benign ( 80% of cases ) and malignant forms . 
benign tumours include mature teratomas and those mature teratomas with an immature component less than 50% of the volume . malignant tumours include seminomas , nonseminomatous tumours and some teratomas ( immature teratomas in subjects older than 15 years ; teratomas with malignant transformation )  . 
in children , instead , they are equally distributed between genders . benign tumours are generally asymptomatic whereas nearly all patients with malignant disease report symptoms : chest pain , dyspnoea , cough , fever or signs of compression and invasion of the surrounding mediastinal structures . among benign forms , the most frequent histological type is mature teratoma , which accounts for 45%75% of cases [ 48 ]  . 
moreover , germ - cell tumours of the mediastinum tend to develop a non - germ - cell malignant component ( rhabdomyosarcoma , adenocarcinoma , neuroectodermal tumours ) , which may become the predominant histological component . 
at diagnosis , a primary tumour of the gonads must be excluded even though a single metastatic localisation in the anterior mediastinum is rare . a correlation has been reported between these tumours and klinefelters syndrome ( karyotype 47 , xxy ) in 8% of cases [ 49 ]  . 
haematological malignancies ( commonly nonlymphoid leukaemia and occasionally malignant histiocytosis ) have also been found to be associated , in particular , with teratomas . germ - cell tumours of the mediastinum are more frequently identified at standard chest radiography . 
although physical and sonographic evaluation of the testicle should always be carried out , presence of an isolated mass in the anterior mediastinum without retroperitoneal involvement is not suggestive of a primary testicular origradiological presentation of malignant nonseminomatous tumours is generally of a large mass of the anterior mediastinum with smooth , lobulated or irregular margins . 
at ct , they have inhomogeneous attenuation with extensive areas of low density ; there may be focal calcification . contiguous fat planes are usually infiltrated ; pleural and pericardial effusion are common . 
ct can also reveal the presence of lung metastases or irregularity of the interface with the lung , a sign of invasion via contiguous spread , as well as extension to the chest wall , involvement of mediastinal lymph nodes and distant metastases [ 40 , 51 ]  . testing of serum - fetoprotein ( - fp ) and - human choria.m. 
il tessuto pancreatico presenta unincidenza relativamente alta [ 55 ] e pu indurre complicanze da rottura spontanea ( per autodigestione da fluidi pancreatici ) con spandimento negli organi cavi vicini : bronchi , pleura , pericardio o polmone [ 46 , 53 ]  . i teratomi immaturi sono costituiti dagli stessi tessuti differenziati della variet matura in associazione a tessuto poco organizzato di tipo fetale : il tessuto neuroepiteliale primitivo il pi comune . 
hanno comportamento variabile , in relazione allet del paziente : nellinfanzia la prognosi favorevole ( in et inferiore a 15 anni sono assimilabili alla controparte matura ) ; nelle altre et della vita hanno frequentemente comportamento aggressivo ( recidiva locoregionale o ripresa a distanza ) , che conduce allexitus il paziente . i teratomi con trasformazione maligna o teratomi maligni o teratocarcinomi contengono una componente francamente maligna , pi frequentemente sarcoma ( angiosarcoma , rabdomiosarcoma ) , in associazione a tessuto fetale o a tessuti adulti ben differenziati ; altre variet sono ladenocarcinoma , il carcinoma a cellule squamose , il carcinoma indifferenziato o una variante mista in associazione ad un tumore maligno a cellule germinali . 
sono aggressivi e causano la morte entro pochi mesi dalla diagnosi per diffusione locale , metastasi a distanza o come conseguenza di entrambe [ 47 ]  . la maggior parte dei teratomi del mediastino dimostrata sul radiogramma standard del torace come massa localizzata a livello del compartimento anteriore , in stretta prossimit allorigine dei grossi vasi ed al cuore [ 7 , 54 ] ; in genere protrudono da un lato della linea mediana e possono raggiungere dimensioni ragguardevoli . 
alla radiologia tradizionale , in una percentuale variabile sino al 26% dei casi , si possono evidenziare calcificazioni prevalentemente laminari e , raramente , osso strutturato o denti [ 53 ]  . 
in particolare , quando siano dimostrate strutture ossee o denti nellambito di una massa riscontrata alla radiologia tradizionale o la combinazione di grasso , fluido , tessuti molli e calcificazioni alla tc consentita la diagnosi nella maggior parte dei teratomi cistici maturi , con un elevato grado di confidenza . 
le complicanze , che possono risultare evidenti sia al radiogramma standard sia alla tc , includono latelectasia , come conseguenza dellostruzione bronchiale , la polmonite ostruttiva o da rottura [ 51 , 54 ] ed il versamento secondario a rottura spontanea nello spazio pleurico o pericardico [ 57 ]  . 
pure seminomas may be associated with altered - hcg ( at low levels ) with unchanged - fp . teratoma this tumour is made up of tissue arising from one or all three of the germ - cell layers of the embryo . 
at diagnosis , patients are generally asymptomatic , so these tumours tend to be incidentally discovered at chest radiography ; however , because they can reach a remarkable size ( 810 cm ) , they may give rise to local symptoms [ 53 ]  . in addition , an abrupt increase in size leading to sudden retrosternal pain is not necessarily an indication of malignancy , as it may be caused by intracystic haemorrhage . histologically , these tumours consist of irregularly arranged , well - differentiated adult tissues of ectodermal ( skin and annexes such as teeth , hairs , sweat and sebaceous glands ) , mesodermal ( cartilage , bone , fat , smooth muscle tissue ) and endodermal origin ( bronchial and intestinal epithelium and pancreatic tissue )  . 
of these , the ectodermal elements prevail , in particular , skin and annexes . other relatively common tissues include cartilage , fat , smooth muscle tissue and respiratory mucosa ; bone , teeth , glial tissue and intestinal mucosa are less frequent . moeller [ 54 ] reported the frequency of the most common components : fluid 88% , fat 76% , calcification 53% and a combination of the three elements 39% . 
ginecomastia ed incremento dei valori ematici di estradiolo e - hcg sono stati descritti raramente [ 61 ] : circa il 10% dei pazienti affetti da seminoma puro pu presentare un incremento sierologico dei livelli di - hcg , ma non mai presente lelevazione della - fp . radiograficamente si manifestano , per lo pi , come masse bulky , lobulate , che protrudono da uno o ambo i lati del mediastino anteriore . 
le metastasi pi frequenti hanno sede polmonare e intratoracica , ai linfonodi regionali ; quelle extratoraciche interessano in genere losso [ 7 , 59 ]  . raccomandato un vigile protocollo di osservazione , senza chirurgia , per le masse residue dopo chemioterapia , a meno che se ne dimostri la crescita . disembriomi non seminomatosi comprendono il tumore del seno endodermico o del sacco vitellino , il coriocarcinoma ed il carcinoma embrionario o , infine , la variante mista [ 62 ]  . 
circa l85% dei casi interessa gli uomini , con et media di 29 anni ; si associa la sindrome di klinefelter sino nel 20% dei pazienti [ 50 ]  . 
frequente il riscontro di valori elevati della lattato deidrogenasi ( ldh ) e di marcatori sierici : - fp nel 60%80% dei pazienti e - hcg nel 30%50% dei casi [ 63 ]  . 
teratomas with malignant transformation , malignant teratomas or teratocarcinomas contain a frankly malignant component , most commonly sarcoma ( angiosarcoma , rhabdomyosarcoma ) , associated with foetal tissue or welldifferentiated adult tissue . 
they are aggressive and lead to death within months of diagnosis as a result of local spread , distant metastasis or both [ 47 ]  . most mediastinal teratomas are depicted by standard chest radiography as a localised mass in the anterior compartment close to the heart and the origin of the great vessels [ 7 , 54 ]  . in general , they extend to one side of the midline and may reach a large size . 
at ct , they have well - defined , smooth or lobulated margins . mature teratomas are encapsulated and display heterogeneous attenuation due to the combination of soft tissue , fluid , fat and calcific components . 
in particular , a finding of bone structures or teeth within a mass at conventional radiology or of a combination of fat , fluid , soft tissue and calcification at ct will allow a confident diagnosis in most mature cystic teratomas . complications visible at both conventional radiology and ct include atelectasia resulting from bronchial obstruction , pneumonia due to obstruction or rupture [ 51 , 54 ] and effusion due to spontaneous rupture of the pleural or pericardial space [ 57 ]  . 
some teratomas may be complicated by synchronous or metachronous leukaemia , which may condition prognosis . seminoma this is the second most frequent germ - cell tumour of the the most common teratoma and mediastinum after ( 35%40% ) among the pure forms [ 59 ]  . 
sono frequentemente invasivi alla diagnosi , con quasi il 90% dei pazienti che presenta sintomi . radiologicamente assumono laspetto di grosse masse irregolari del mediastino anteriore , spesso con densit disomogenea alla tc per la presenza di estese aree centrali ipodense dovute a necrosi , emorragia e degenerazione cistica . pu essere presente invasione delle strutture adiacenti , compresa la parete toracica , diffusione ai linfonodi loco - regionali ed a distanza . 
alla diagnosi l85%95% dei pazienti presenta metastasi evidenti , a distanza ; le sedi pi comuni includono polmone , pleura , linfonodi , fegato e , meno frequentemente , losso [ 59 ]  . espansi linfonodali i linfonodi del mediastino anteriore possono essere interessati da eventi loco - regionali e sistemici . 
la patologia sistemica ( linfomi ) vede coinvolti spesso i linfonodi del mediastino anteriore e , contestualmente , il timo che organo linfatico . i linfonodi normalmente non sono visibili alla radiografia del torace per le piccole dimensioni e perch indovati nel tessuto adiposo . 
il loro ingrandimento pu dislocare la pleura producendone una bozzatura visibile : questo reperto pu risultare evidente , qualora coinvolga le catene mammarie interne , determinando una alterazione della linea extrapleurica anteriore ( lea )  . 
lecotomografia , pur se non consente di esaminare tutte le sezioni del mediastino , condivide la sensibilit della tc nella valutazione del mediastino anteriore , con elevata specificit nello studio delle linfoadenopatie . quando le linfoadenopatie sono associate ad una massa polmonare centrale , ad una lesione cavitaria od infiltrativa , essenziale la diagnosi di natura di tale lesione , ottenibile con broncoscopia a fibre ottiche , con biopsia endobronchiale , transbronchiale o fna . 
infine , quando non siano accessibili n per via broncoscopica , n percutanea , o quando i campioni siano inadeguati o non diagnostici , pu essere indicata la mediastinoscopia con biopsia escissionale . il trattamento delle linfoadenopatie mediastiniche legato alla malattia di base . linfoma primitivo mediastinico il linfoma un tumore mediastinico piuttosto comune e pu a.m. 
contrast - enhanced computed tomography ( ct ) of an 11 - year - old girl , large , complex mass containing multiple cysts , fat and dystrophic calcification displaces the mediastinum to leit contains fatty fluid , debris and focal fatty density ( mean attenuation 96 hounsfield units )  . 
invasion of adjacent structures is very rare [ 46 ] , but distant metastases are possible . the most frequent sites for metastasis are lung , chest and regional lymph nodes ; extrathoracic metastases usually involve bone [ 59 , 7 ]  . 
residual masses after chemotherapy should undergo close monitoring without surgery unless their growth has been documented . nonseminomatous dysembryomas these include tumours of the endodermal sinus or yolk sac , choriocarcinomas , embryonal carcinomas or the mixed variant [ 62 ]  . 
these are malignant tumours , which are symptomatic and affect young adults [ 46 ]  . about 85% of cases occur in men with a mean age of 29 years ; klinefelters syndrome is associated in up to 20% of patients [ 50 ]  . 
patients usually have elevated lactate dehydrogenase ( ldh ) and serum markers : - fp in 60%80% of patients and - hcg in 30%50% [ 63 ]  . essere riscontrato nel compartimento anteriore , medio e posteriore [ 64 ]  . 
rappresenta circa il 20% di tutti i tumori del mediastino nelladulto ed il 50% nel bambino ; nel 5% dei casi il mediastino lunica sede di malattia ed in questo caso la diagnosi differenziale pu essere difficile sulla base del solo reperto radiologico . 
in genere , la diagnosi conseguente allescissione di una linfoadenopatia periferica palpabile , qualora sia presente , ed il coinvolgimento toracico accertato dagli esami di diagnostica per immagini . molti dei linfomi primitivi del mediastino originano nel timo , alternativamente da linfonodi : si tratta per lo pi di linfomi di hodgkin , o , meno comunemente , di linfomi nonhodgkinfrequentemente sono confinati nel mediastino al momento della diagnosi : il 50%70% dei pazienti affetti da malattia linfomatosa di altra sede con coinvolgimento mediastinico presenta la malattia di hodgkin e solo nel 15%25% un linfoma non - hodgkin [ 65 ]  . 
tra i linfomi non - hodgkin , le varianti pi frequenti , che possono interessare primariamente il mediastino anteriore , sono il linfoma a grandi cellule b ed il linfoma linfoblastico . 
 la scintigrafia con gallio e soprattutto la fdg - pet sono utili nella stadiazione e nel follow - up dopo trattamento . linfoma di hodgkin si presenta con distribuzione bimodale , con picco di incidenza nelladolescenza e nella giovane et adulta , e dopo il vi decennio . 
i sintomi sistemici ( che identificano la categoria b : febbre , calo ponderale superiore al 10% del peso corporeo negli ultimi 6 mesi , sudorazioni notturne , prurito ) sono evidenti nel 20%30% dei casi , mentre la maggior parte dei soggetti non mostra una sintomatologia n sistemica n locale ed il riscontro pertanto incidentale alla radiografia del torace . talvolta , tuttavia , pu essere presente dolore toracico , tosse , dispnea , disfagia da invasione o da effetto massa sulle strutture mediastiniche . 
dal punto di vista macroscopico si manifesta come conglomerato linfonodale o come massa polilobulata a nonseminomatous germ - cell tumours of the mediastinum more commonly occur in the anterior compartment and appear as lobulated masses enclosed by a thin capsule . 
they are frequently invasive at diagnosis , with almost 90% of patients reporting symptoms . the radiological appearance is of a bulky irregular mass in the anterior mediastinum , often with inhomogeneous density at ct due to the presence of large hypodense central areas related to necrosis , haemorrhage and cystic degeneration . there may be invasion of adjacent structures , including the chest wall , as well as spread to the locoregional lymph nodes and distant metastasis . 
at diagnosis , 85%95% of patients have distant metastasis ; the most common sites include lung , pleura , lymph nodes , liver and , less commonly , bone [ 59 ]  . lymph node masses lymph nodes of the anterior mediastinum may be affected by locoregional and systemic events . 
systemic diseases ( lymphomas ) often involve nodes of the anterior mediastinum and thymus , a lymphatic organ . lymph nodes are not normally visible on chest radiographs due to their small size and the fact that they are embedded in fat . 
ultrasonography , though not allowing inspection of all sections of the mediastinum , has the same accuracy as ct in evaluation of the anterior mediastinum and high specificity in the study of lymphadenopathy . when node enlargement is associated with a central pulmonary mass , cavitary or infiltrative disease , it is mandatory to determine the nature of the lesion by fibreoptic bronchoscopy , endobronchial or transbronchial biopsy or fineneedle aspiration ( fna )  . 
finally , if the nodes are not amenable to bronchoscopic or percutaneous techniques , or in the event of inadequate or nondiagnostic sampling , mediastinoscopy with excisional biopsy may be indicated . 
 treatment of mediastinal lymphadenopathy depends on the underlying disease . primary mediastinal lymphoma lymphoma is a relatively common mediastinal tumour , which may be seen in the anterior , middle or posterior compartment [ 64 ]  . 
quando ha sede timica possono essere presenti , prima o dopo trattamento , aree cistiche [ 25 ]  . in circa il 70% dei casi la radiografia del torace patologica : di questi , il 90% presenta un interessamento linfonodale bilaterale . 
la diffusione per stazioni linfonodali contigue , linteressamento di un singolo gruppo segnalato solo nel 15% dei casi : il mediastino anteriore ed i linfonodi paratracheali rappresentano le sedi pi usuali . 
la variante pi comune ( scleronodulare ) si presenta tipicamente come massa lobulata ben delimitata nel mediastino antero - superiore [ 65 ]  . nel 12% dei pazienti si osserva invasione polmonare , che quasi sempre associata con linteressamento adenopatico ilare . 
alla tc , dal 71% all85% delle nuove diagnosi di linfoma di hodking presenta localizzazione toracica [ 67 ] : la massa mediastinica pu essere costituita da formazioni multiple arrotondate con densit dei tessuti molli ( linfoadenopatie ) , da una massa bulky ( conglomerati adenopatici ) o da una lesione solida ( e pi raramente cistica ) timica [ 25 ]  . 
alla rm rappresentato da una massa relativamente omogenea , con bassa intensit di segnale nella sequenza t1 , analoga al tessuto muscolare , e segnale intermedio o alto nelle immagini in t2 , come da tessuto adiposo . 
nelle sequenze in t2 liperintensit di segnale pu essere in relazione con edema , infiammazione , fibrosi precoce o tessuto granulomatoso , mentre il tessuto fibroso denso ( dopo trattamento ) ha bassa intensit . 
alle lesioni bulky dopo terapia spesso residuano masse fibrose che non possono essere distinte dalle persistenze tumorali alla tc : in questi casi le sequenze t2 di rm possono segnalare un incremento diffuso dellintensit o aree focali iperintense , che correlano con la malattia recidiva [ 68 ]  . infine , deve essere ricordato che una massa mediastinica in progressione o di nuova presentazione dopo trattamento pu rappresentare una recidiva tumorale , o in alternativa uniperplasia timica o una cisti del timo . linfoma non - hodgkin alla presentazione generalmente gi malattia diffusa ; la classificazione istopatologica ha un valore prognostico superiore allestensione anatomica di malattia . 
l85% dei pazienti presenta , alla diagnosi , uno stato di malattia avanzato che generalmente si accompagna a sintomi sistemici ( categoria b ) , linfoadenopatie generalizzate o malattia extranodale . il linfoma a grandi cellule b interessa primitivamente il mediastino , nella fascia di et del giovane adulto ed occasionalmente nel bambino , con prevalenza del sesso femminile in entrambi i casi . 
in general , diagnosis is achieved through excision of a palpable peripheral node , when present , and chest involvement is established by diagnostic imaging . many primary mediastinal lymphomas arise in the thymus rather than in lymph nodes . 
they may cause bulky enlargement of mediastinal nodes , at times associated with ipsilateral interstitial oedema due to lymphatic or venous obstruction . gallium scintigraphy and especially fluorodeoxyglucose positron emission tomography ( fdg - pet ) are useful in disease staging and follow - up after treatment . hodgkins lymphoma hodgkins lymphoma has a bimodal age distribution , with an incidence peak in adolescence and early adulthood and after the sixth decade of life . 
systemic symptoms ( which identify category b : fever , weight loss more than 10% of body weight during the previous 6 months , night sweats , itching ) are present in 20%30% of cases whereas most subjects have no systemic or local symptoms , and the disease is incidentally discovered at chest radiography . 
the most common variant ( nodular sclerosing ) typically presents as a well - circumscribed lobulated mass in massa tumorale , con possibile infiltrazione della vena cava superiore , delle vie aeree , della parete toracica o di altre strutture adiacenti . 
la diffusione extratoracica , alla presentazione , un reperto inusuale . anche i linfomi linfoblastici sono altrettanto aggressivi nella presentazione : si tratta di forme ad alto grado che si presentano nei primi due decenni di vita , pi spesso nelladolescente di sesso maschile . 
il linfoma linfoblastico condivide molte caratteristiche cliniche con la leucemia linfoblastica associata a massa mediastinica : questultima presentazione ne pu rappresentare la fase leucemica . entrambi gli istotipi si manifestano come massa bulky , non capsulata , con franco atteggiamento invasivo che interessa il timo e pu infiltrare le strutture adiacenti . le caratteristiche radiologiche sono varie . 
quasi il 50% ha un coinvolgimento linfonodale tipicamente a salto e non interessa le stazioni mediastiniche anteriori e paratracheali : infatti , a differenza del linfoma di hodgkin , interessa meno elettivamente il compartimento mediastinico anteriore ed ha una maggiore predilezione per la diffusione linfonodale a stazioni non contigue ed ematogena . pu verificarsi infiltrazione polmonare ( in meno del 5% dei pazienti in fase tardiva , indifferentemente dallassociazione con unadenopatia ilare ) , pleurica o pericardica [ 68 ]  . 
the mediastinal mass may consist of multiple rounded formations with soft tissue density ( lymphadenopathy ) , a bulky mass ( nodal conglomerates ) or a solid thymic lesion ( less commonly cystic ) [ 25 ]  . 
calcification is typically present after treatment [ 65 ]  . at mri , the mass is relatively homogeneous , with low signal intensity similar to muscle in t1 and intermediate or high signal intensity similar to fat in t2 . 
the high t2 signal intensity may be related to oedema , inflammation , early fibrosis or granulomatous tissue whereas the dense fibrous tissue ( after treatment ) has low signal intensity . 
in these cases , mri t2 sequences may reveal a diffuse increase in signal intensity or focal areas of hyperintensity , which are correlated with disease recurrence [ 68 ]  . finally , it should be remembered that a progressing or new mediastinal mass after treatment may represent tumour recurrence , thymic hyperplasia or a thymic cyst . non - hodgkins lymphoma at presentation , the disease is already diffuse ; histopathological classification has greater prognostic significance than anatomical extension of disease . 
at presentation , 85% of patients have advanced disease , usually with systemic symptoms ( category b ) , generalised lymphadenopathy or extranodal disease . large b - cell lymphoma is a primary mediastinal lymphoma seen in young adults and occasionally children , with prevalence in females in both cases . 
i soggetti affetti da carcinoma mammario , in particolar modo coloro che sviluppano una recidiva a livello della parete toracica in sede parasternale , dovrebbero essere indagati ponendo attenzione allarea retrosternale poich queste recidive possono rappresentare una diretta estensione dai linfonodi della catena mammaria interna . la diagnosi differenziale si pone con la malattia linfoproliferativa ( linfoma o leucemia ) , che pu coinvolgere questa catena linfonodale ; in genere , per , per tali patologie ematologiche non si verifica il loro interessamento in assenza di coinvolgimento delle stazioni in sede toracica . lindagine radiologica ricopre un importante ruolo nella detezione di linfoadenopatie della catena mammaria interna , dal momento che questo gruppo linfonodale non pu essere indagato attraverso la mediastinoscopia . un ingrandimento dei linfonodi di questa stazione rappresenta una delle cause di alterazione della lea , che in questo caso presenta margine dentellato o lobulato . 
enlargement of sternal or internal mammary chain nodes these nodes , especially those located in the first three intercostal spaces , tend to be involved by metastatic spread from breast cancer . 
subjects with breast cancer , in particular , those who develop a recurrence in the parasternal chest wall , should undergo careful investigation of the retrosternal region , as these recurrences may represent a direct extension from nodes of the internal mammary chain . differential diagnosis should consider lymphoproliferative diseases ( lymphoma or leukaemia ) , which may affect the internal mammary chain general , however , involvement by these diseases does not occur without involvement of the thoracic node groups . imaging is instrumental in the detection of internal mammary chain lymphadenopathy , which cannot be investigated with mediastinoscopy . 
enlargement of this node group is one of the causes of an altered ael , which in this case displays a serrated or lobulated margless frequently , the interface may appear linear , with a band of increased density separating the lung from the anterior chest wall . 
enlargement of diaphragmatic nodes ( anterior and middle ) or cardiophrenic angle nodes these lymph nodes cannot be visualised at radiography unless they are massively enlarged since they are surrounded by areolar tissue and fat , which mask minimal enlargement . when they become visible at the level of the cardiophrenic angle , they produce a mass with lateral convexity on frontal views and posterior convexity on laterolateral ( ll ) views . 
in the case of suspected lymphadenopathy , a ct ( or us ) examination may be useful in differentiating involvement of the diaphragmatic nodes from a pericardial fat pad . mesenchymal abnormalities mesenchymal abnormalities include cystic and solid lesions . mediastinal mesenchymal masses originate from the mediastinal connective tissue , account for about 5% of all mediastinal masses and include benign and malignant lesions originating from fat , fibrous tissue , smooth and striated muscle , blood and lymphatic vessels , bone and nerve tissue [ 69 ]  . around 55% are malignant ; there is no gender predilection [ 70 ]  . 
in caso di sospetta linfoadenopatia , lindagine tc ( ovvero con us ) risulta utile al fine di differenziare un interessamento dei linfonodi diaframmatici da un cuscinetto adiposo pericardico . anomalie mesenchimali le anomalie mesenchimali comprendono lesioni cistiche e lesioni solide . 
gli espansi mesenchimali mediastinici originano dagli elementi di tessuto connettivo del mediastino . rappresentano circa il 5% di tutte le masse mediastiniche ed includono lesioni benigne e maligne ad origine dal tessuto adiposo , fibroso , dal muscolo liscio e striato , dai vasi sanguigni e linfatici , da osso e da tessuto nervoso [ 69 ]  . 
circa il 55% maligno ; non si riscontra predilezione di sesso [ 70 ]  . possono presentarsi in qualunque compartimento , con leccezione delle formazioni nervose ( a sede elettiva paravertebrale ) , ma il mediastino anteriore rappresenta la sede pi frequente . 
tuttavia , la localizzazione mediastinica meno comune rispetto alle sedi extratoraciche . espansi ad origine dal tessuto adiposo il riscontro di tessuto adiposo nel mediastino frequente e ben documentabile soprattutto dallo studio tc , che , per intrinseche caratteristiche , ne permette una precisa dimostrazione . 
nonetheless , mediastinal location is less common than extrathoracic sites . masses originating from adipose tissue adipose tissue is frequently found in the mediastinum and is particularly well documented by ct thanks to the intrinsic properties of this technique . 
adipose tissue may be seen in a wide spectrum of conditions some nonpathological ( lipomatosis , fat pads ) , others expressing local disease ( lipomas , well - differentiated liposarcoma ) , and others expressing frankly progressive disease ( undifferentiated liposarcoma )  . lipomatosis is a diffuse and excessive accumulation fat in typical sites of the mediastinum ; it is seen in obesity and associated with hypercortisolism , as in cushings syndrome , ectopic adrenocorticotropic hormone ( acth ) production and as a side effect of treatment ( long - term steroids )  . 
the posteroanterior ( pa ) view shows symmetrical widening , with homogenous appearance , of the supra - aortic and supra - azygotic mediastinal portions , with normal and smoothly marginated appearance ( at times lobulated ) of the anterior junction line ( ajl )  . 
the finding may be confirmed by mri , which will reveal marked t1 hyperintensity with classical suppression in the fat - suppressed short tau inversion recovery ( stir ) sequences . pericardial fat pads are the most common mediastinal fat depositions . 
on pa and ll chest radiographs , they appear as faint triangular opacities of the cardiophrenic angles , more frequently on the lethe interface they form with the lung may have convex or concave shape . on the lateral radiogram , they appear as an extrapleural triangular opacity at the level of the anterior cardiophrenic angle . 
often , radiography is unable to discern the adipose nature of the pericardial pad , but this can be readily demonstrated by ct [ 40 , 71 ] , which provides differential diagnosis with pericardial cyst , thymolipoma and morgagnis hernia . extrathymic lipoma is the most common nonneurogenic mesenchymal tumour of the mediastinum and accounts for 2% of all mediastinal masses [ 28 ]  . 
at standard chest radiography , they appear as poorly radiopaque masses ( due to the typical low density of fat ) ; at times bulky , they are multilobulated and change their shape according to the patients position . the pliable nature of these masses accounts for the lack of symptoms , even in the presence of very large masses . 
nella proiezione pa visibile uno slargamento , simmetrico , di aspetto omogeneo , delle porzioni sovra - aortica e sovra - azygotica del mediastino , con aspetto regolare ed a margini lisci ( talvolta lobulati ) della linea di giunzione anteriore ( lga )  . 
nei casi dubbi , la tc diagnostica : si evidenzia un diffuso incremento del tessuto cellulo - adiposo mediastinico ; il dato pu essere confermato alla rm dal riscontro di marcata iperintensit nella sequenza t1 con classica soppressione nelle scansioni inversion recovery con soppressione ( stir )  . i cuscinetti adiposi paracardiaci sono i pi frequenti accumuli adiposi del mediastino . 
spesso la natura adiposa del cuscinetto pericardico non viene definita con sicurezza dallindagine radiografica , ma facilmente dimostrata dalla tc [ 40 , 71 ] , che discrimina la diagnosi differenziale con : cisti pericardica , timolipoma , ernia di morgagni . il lipoma extratimico il pi comune tumore mesenchimale non neurogenico a localizzazione mediastinica e rappresenta il 2% di tutte le masse del mediastino [ 28 ]  . 
al radiogramma standard del torace appaiono come masse poco radioopache ( per la tipica ipodensit del grasso ) , anche voluminose , polilobulate che modificano la forma con il decubito del paziente . 
la presenza di aree eterogenee , con valori di densit tipici dei tessuti molli , dovrebbe suggerire lipotesi diagnostica del liposarcoma . i liposarcomi sono molto rari ; in alcuni casi lorigine nel timo , ma la sede pi frequente il mediastino posteriore . la diagnosi avviene in et adulta ( v decennio )  . 
in many cases , the disease is locally advanced at presentation and manifests with the signs and symptoms of compression ( dyspnoea , chest pain , cough ) ; vena cava syndrome is uncommon . 
the well - differentiated forms show areas with fat density associated with areas of soft tissue density whereas the poorly differentiated forms have the typical homogenous density of soft tissue . 
less frequent , the other form is seen in adults and mostly affects the lower anterior mediastinum away from the neck [ 73 ]  . mediastinal cystic lymphangioma or cystic hygroma is a histologically benign proliferation of lymphatic vessels , which may have an infiltrative growth pattern . 
pathogenic hypotheses include a developmental abnormality or a hamartomatous or neoplastic origit is a typical childhood tumour : in 50% of cases it is present at birth , and 90% are diagnosed by the time the individual is 2 years old . 
they tend to enlarge as the child develops , in particular during puberty . a total of 95% of lymphangiomas affect the neck or axilla , and 10% extend in the anterosuperior mediastinum or , less commonly , in other mediastinal compartments . 
it is located in the anterior mediastinum in 37% of cases but may occur as gensegni e sintomi da compressione ( dispnea , dolore toracico , tosse ) ; la sindrome della vena cava rara . 
alla tc le forme ben differenziate presentano zone a densit adiposa associate ad aree dalla attenuazione dei tessuti molli , mentre le varianti scarsamente differenziate hanno la caratteristica densit omogenea dei tessuti molli . raramente si osservano metastasi extratoraciche . espansi ad origine dai vasi sanguigni i tumori vascolari del mediastino includono emangiomi , emangioendoteliomi , emangiopericitomi benigni e maligni ed angiosarcoma [ 70 ]  . 
la diagnosi conseguita con tc o rm : nel 30% dei casi si riconoscono fleboliti . langiografia utile per lembolizzazione prima della resezione chirurgica completa [ 72 ]  . espansi ad origine dai vasi linfatici sono nel complesso rari . 
si distinguono del linfangioma a sede mediastinica due variet clinicopatologiche : la prima , igroma cistico , nel mediastino alto , a prevalente presentazione nellinfanzia ( la diagnosi occorre in genere entro i 2 anni di et ) ; laltra forma , meno frequente , di riscontro in et adulta , per lo pi nel mediastino anteriore basso a distanza dal collo [ 73 ]  . il linfangioma cistico mediastinico o igroma cistico una proliferazione istologicamente benigna di vasi linfatici che pu assumere una crescita infiltrativa . 
raramente ( 17% dei casi ) , il linfangioma si presenta come tumore primitivo del mediastino in et adulta , ed in questa evenienza nel 37% dei casi ha sede nel mediastino anteriore , o come linfangiomatosi generalizzata con interessamento multifocale estensivo di diversi apparati [ 74 ]  . 
it may infiltrate tissue cleavage planes , but more frequently , it surrounds and displaces mediastinal structures and adjacent vessels [ 74 ]  . the most common ct finding , seen in around 60% of cases , is a smoothly marginated cystic mass with homogeneous fluid attenuation ; multilobulated cystic dilatations , which represent wide lymphatic vascular spaces and vary in diameter from a few millimetres ( 12 mm ) to several centimetres , are present in around 1 / 3 of cases [ 75 ] and have thin or thick septa that may show mild contrast enhancement . less frequent findings include calcification , homogeneous soft tissue density and spiculated margins . 
other lymphatic tissue tumours include lymphangiosarcoma and lymphangiopericytoma . pericardial mesothelial cysts these are congenital developmental abnormalities that derive from the persistence and fusion of anterior pericardial recesses ( ventral and parietal ) of the coelomic cavity . 
they have fluid content and a thin wall of connective tissue lined by a thin layer of mesothelial - like cells , are spherical or ovoid in shape and mostly unilobulated . these cysts are rare [ 8 ] , typically asymptomatic and therefore tend to be discovered incidentally at chest radiography . they occur in adulthood in the fourth and fifth decade . at chest radiography , they appear as rounded , unilobular , smoothly marginated and well - defined homogeneous masses at the level of the cardiophrenic angles , above all on the right . 
if the patients position is modified , they tend to take up a gravity - dependent position , and if there is communication with the pericardium , their fluid content can be seen to move . ct can demonstrate their benign nature : they appear as well - defined unilobulated masses with fluid density and a thin peripheral rim ; they do not enhance [ 65 ]  . 
alla tc , laspetto pi comune , che si riscontra circa nel 60% dei casi , di una massa cistica a margini lisci che ha densit omogenea , prossima a quella dellacqua ; le dilatazioni cistiche multiloculate , che rappresentano ampi spazi vascolari linfatici , variano di diametro da pochi millimetri ( 12 mm ) a diversi centimetri , sono presenti circa in 1 / 3 dei casi [ 75 ] e mostrano setti sottili o spessi che possono assumere debolmente il mezzo di contrasto . 
la resezione parziale pu essere causa di un chilotorace . altri tumori del tessuto linfatico includono il linfangiosarcoma ed il linfangiopericitoma . cisti mesoteliali pericardiche sono anomalie congenite di sviluppo che derivano dalla persistenza e fusione dei recessi pericardici anteriori ( ventrale e parietale ) della cavit celomatica . 
si presentano in et adulta , nel iv e v decennio di vita . al radiogramma del torace appaiono come masse uniloculate a margini lisci , ben definite , rotondeggianti , omogenee , a livello degli angoli cardiofrenici , soprattutto a destra . possibile la presentazione atipica in sede di mediastino superiore . 
modificando la postura del paziente , tendono ad assumere la posizione declive e , peraltro , qualora esista una comunicazione con il pericardio , pu aversi lo spostamento del contenuto liquido . 
alla tc ne viene documentata la natura benigna : risultano masse ben definite , uniloculate che presentano densit di tipo fluido ed un fine cercine periferico ; non assumono il mezzo di contrasto [ 65 ]  . 
talora la densit disomogenea o tipica dei tessuti molli per la presenza di un contenuto viscoso : in tal caso difficile la diagnosi differenziale con un processo neoplastico [ 40 ]  . 
diagnosis can also be confirmed by us [ 78 ] , which will demonstrate the hypoechoic nature and low - grade absorption of ultrasound waves . pericardial cysts can undergo clinical and radiological monitoring . 
in fact , detection of a space - occupying lesion in the anterior mediastinum is often coincidental to chest radiography performed for other purposes whereas in other cases , examination is carried out due to local ( and sometimes systemic ) clinical symptoms . ct is the modality that yields diagnosis in most cases ( more easily in differentiated forms ) while providing reliable assessment of disease extent . 
the remaining imaging techniques currently have a complementary role . integration of imaging with clinical findings ( signs and symptoms of myasthenia gravis , hyperparathyroidism , paraneoplastic syndromes ) and laboratory data ( autoantibodies against postsynaptic acetylcholine receptors , - fp , - hcg , ldh , thyroid hormones , pth , acth ) is nonetheless fundamental in the diagnostic work - up . 
infatti , la diagnosi di processi occupanti spazio nel mediastino anteriore spesso incidentale ad un radiogramma eseguito per altre ragioni , mentre in altri casi lindagine conseguente ad una sintomatologia clinica locale ( e talvolta sistemica )  . la tc la metodica che consente , nella larga maggioranza dei casi , di conseguire la diagnosi ( pi semplice nel caso delle forme differenziate ) , al contempo di un valido bilancio di estensione della malattia . 
le altre tecniche di imaging rivestono , attualmente , ruoli complementari . nelliter diagnostico comunque fondamentale lintegrazione con i dati clinici ( segni e sintomi di miastenia gravis , iperparatiroidismo , sindromi paraneoplastiche ) e di laboratorio ( autoanticorpi contro i recettori post - sinaptici dellacetilcolina , - fp , - hcg , ldh , ormoni tiroidei , pth , acth )  . 
in ogni caso , ove indicato , la tc offre unutile guida allaccertamento bioptico . ringraziamenti gli autori ringraziano , per gli importanti e competenti suggerimenti , i colleghi : f . 
for qualitative evaluation , one experienced reader graded the opacification of renal arteries as excellent , good or poor ; for quantitative evaluation , mdct and dsa were independently evaluated for the number of renal arteries and the presence , location and degree of stenosis in random order by three readers . 
on the basis of consensus readings , calculations of sensitivity , specificity , accuracy , positive predictive value ( ppv ) and negative predictive value ( npv ) for detection of degree of stenosis were made by using dsa findings as the standard of reference . 
although 72 of these were also classified as normal with ct angiography , one was overestimated by one grade ; at dsa , 16 arteries were classified as moderately stenotic ; in two arteries , there was an overestimation of one grade . 
in two patients , all three readers detected multiple severe stenoses on both modalities , with a string - of - beads appearance typical of fibromuscular dysplasia . accessory arteries were correctly identified as such by all three readers on either dsa or mdct . 
la valutazione quantitativa stata effettuata in modo indipendente da tre lettori che hanno determinato , sia con langio - tc che con la dsa , il numero delle arterie renali , la presenza , la localizzazione e il grado di eventuali stenosi . sensibilit , specificit , accuratezza , ppv e npv , per la valutazione del grado di stenosi , sono stati calcolati sulla base di una lettura consensuale usando i risultati della dsa come gold standard . 
per quanto riguarda la valutazione quantitativa 73 arterie sono state classificate come normali con la dsa ; 72 di queste sono state classificate come normali anche con langio - tc , in 1 caso la tc ha sovrastimato la stenosi di un grado . 
i valori di sensibilit , specificit , e accuratezza per quanto riguarda il grado di stenosi sono stati rispettivamente del : 100% , 98 , 6% , e 96 , 9% , con un ppv e npv del 97 , 6% e 100% . 
mdct angiography is very accurate and robust , even for the assessment of renal artery stenosis , and has the potential to become a viable substitute , in most cases , for diagnostic catheter - based dsa . key words computed tomography angiography comparative studies renal arteries stenosis hypertension fibromuscular dysplasia rispettivamente del : 100% , 97 , 3% , e 97 , 8% , con un ppv e un npv del 98 , 2% e 97 , 8% . 
langio tcms una metodica accurata e valida nella valutazione delle stenosi delle arterie renali e possiede le potenzialit per diventare un valido sostituto della dsa diagnostica . parole chiave tomografia computerizzata angiografia , studi comparativi arterie renali stenosi ipertensione displasia fibromuscolare introduction introduzione renal artery stenosis is the most common cause of secondary hypertension [ 1 ] , and its detection is an important goal for the physician since the condition is potentially treatable [ 2 ]  . although still considered the standard modality in the evaluation of stenosis of renal arteries , digital subtraction angiography ( dsa ) is not free of risks , and less invasive techniques such as magnetic resonance ( mr ) angiography and computed tomography ( ct ) angiography have been suggested as possible alternatives for assessment of renal artery disease , with very promising results . 
mr angiography , in view of the absence of ionising radiation and the possibility of using nonnephrotoxic contrast media , is widely accepted for detection of diseases of renal arteries and aorta [ 3 ]  . 
single - slice spiral ct , in particular with thin collimations , has proved to provide accurate assessment of renal artery stenoses [ 47 ]  . the limitation of single - slice ct lies in the obvious compromise : thin collimation / long scan time ( with resulting opacification of renal veins and venous structures and possible breathing artefacts affecting the quality of the examination ) , thicker collimation / short scan time ( therefore excellent arterial enhancement but limited spatial resolution and resulting poor depiction of accessory arteries )  . 
the advent of multislice ct ( msct ) has made it possible to acquire large body volumes with high spatial resolution and very short scan times and , therefore , to have excellent depiction of small vessels , including accessory arteries and segmental branches [ 810 ] without opacification of the renal veins . the aim of our study was to determine the utility of msct angiography in identifying and quantifying stenoses of renal arteries . 
 materials and methods during a period of 8 months , 50 patients , who had been studied by dsa following color doppler ultrasonography indication , underwent ct angiography of the abdominal aorta . the study was approved by the ethics committee , and informed consent was given by all patients . 
indications for angiography included vascular disorders , such as stenosis of renal arteries , abdominal aorta aneurysms and steno - occlusive disease of the aortoiliac axis . in all 50 patients , renal arteries were evaluated with both techniques , with dsa and ct angiography being performed within 7 days of each other ( 27 days : mean interval 4.3 days ) and dsa being performed first in all cases . 
for each injection , 20 ml nonionic contrast medium was administered ( iomeprol 350 mgi / ml : iomeron 350 , bracco , milan , italy ) at a rate of 20 ml / s . 
the ct examination was performed after administration of 80 ml contrast material injected at a rate of 4 ml / s with an automatic injector ( envision ct , medrad , indianola , pa , usa )  . 
a high - concentration nonionic iodinated contrast agent was used ( iomeron 400 , bracco , milan , italy ) followed by 20 ml saline injected at a flow rate of 4 ml / s via a second injector connected to the intravenous cannula with a y - shaped adaptor . 
scan parameters were as follows : collimation 4x1 mm , table speed 10 mm / s , gantry rotation time 0.5 s , 120 kvp , 80 mas , ctdiw ( weighted ct dose index ) 7.9 mgy ; reconstruction interval 1 mm , matrix 512x512 with a slice thickness of 1.25 mvoxel size was therefore 0.60.7x0.60.7x1.25 min all patients , scan delay was calculated using the bolus test : 20 ml of contrast material was injected at a flow rate of 4 ml / s followed by f . 
i pazienti ( 39 uomini , 11 donne ) di et compresa tra 43 e 79 anni ( et media 63 anni ) sono stati selezionati per lo studio in base ad una storia di ipertensione secondaria ( pressione arteriosa superiore a 160 / 90 mmhg , in trattamento con farmaci anti - ipertensivi )  . 
tutti i pazienti presentavano una funzionalit renale normale ( creatinemia media di 0 , 97 mg / dl )  . lindicazione ad eseguire lesame angiografico comprendeva disordini vascolari quali : stenosi delle arterie renali , aneurismi dellaorta addominale e patologia steno - occlusiva dellasse aorto iliaco . in tutti i cinquanta pazienti le arterie renali sono state valutate con entrambe le tecniche ; dsa e angio - tc sono state eseguite nellarco di 7 giorni ( 27 giorni : intervallo medio 4 , 3 giorni ) e la dsa stata eseguita come primo esame in tutti i casi . 
stato utilizzato un approccio transfemorale ( 36 punture dellarteria femorale destra e 14 sinistra ) per posizionare un catetere di 5f pigtail a livello delle arterie renali . per ogni iniezione sono stati utilizzati 20 ml di contrasto non ionico ( iomeprol 350 mgi / ml : iomeron 350 , bracco , milano , italia ) con un flusso di 20 ml / s . 
le immagini sono state ottenute inizialmente nella proiezione antero - posteriore ; successivamente sono state eseguite proiezioni oblique ( 15 sinistra e destra anteriore )  . se ritenuta necessaria dal radiologo , stata effettuata anche una cateterizzazione selettiva dellarteria renale . tomografia computerizzata multistrato ( tcms ) langio - tc stata eseguita in tutti i pazienti usando una tc spirale a 4 detettori ( siemens volume zoom , forcheim , germania ) con un tempo di rotazione del gantry di 0 , 5 s . 
this was followed by a series of lowdose scans ( 120 kvp , 10 ma ) at the same level ( coeliac trunk ) every 2 s from 12 s and up to 35 s after bolus administration . 
 image analysis all images were analysed on a dedicated console ( kayak xu 800 , hewlett - packard ) using three - dimensional ( 3d ) reconstruction software ( vitrea 2.6 , vital images inc , plymouth , mn , usa ) , which the radiologists had been using for at least 6 months . 
the 3d image analysis was done directly by the readers without using predefined reconstructions : analysis of each case took approximately 510 malthough not considered necessary for diagnostic purposes , bone segmentation was carried out to provide the vascular surgeons with easy - to - read images . 
the readers also noted the level of the stenosis : 1 , ostium ; 2 , proximal renal artery ; 3 , segmental renal arteries ; 4 , accessory renal artery . 
sensitivity , specificity , accuracy , 80 ml di mezzo di contrasto ad una velocit di flusso di 4 ml / s , con un iniettore automatico ( envision ct , medrad , indianola , pa , usa )  . 
stato utilizzato un mezzo di contrasto iodato non ionico ad alta concentrazione ( iomeron 400 , bracco , milano , italia ) seguito da 20 ml di soluzione salina iniettata con una velocit di flusso di 4 ml / s con un secondo iniettore connesso con una valvola ad y alla cannula endovenosa . del voxel la collimazione usata stata di 4x1 mm , la velocit del tavolo di 10 mm / s , il tempo di rotazione del gantry di 0 , 5 secondi ; i kvp impiegati sono stati 120 , i mas 80 , il ctdiw ( weighted ct dose index ) di 7 , 9 mgy ; lintervallo di ricostruzione utilizzato stato di 1 mm ; le dimensioni della matrice di 512x512 con uno spessore di strato di 1 , 25 mm : le dimensioni 0 , 60 , 7x0 , 60 , 7x1 , 25 min tutti i pazienti il tempo di ritardo per una corretta somministrazione del mezzo di contrasto , stato calcolato con il bolus test che ha previsto una preliminare iniezione di 20 ml di mezzo di contrasto con velocit di flusso di 4 ml / s seguita da 20 ml di soluzione salina . sono state conseguentemente effettuate una serie di scansioni a bassa dose ( 120 kvp , 10 ma ) allo stesso livello ( tronco celiaco ) ogni 2 secondi a partire da 12 e fino a 35 secondi dopo la somministrazione del bolo . risultate quindi sono analisi delle immagini tutte le immagini sono state analizzate su una console dedicata ( kayak xu 800 , hewlett - packard ) utilizzando un software di ricostruzione 3 - d ( vitrea 2.6 , vital images inc , plymouth , mn , usa ) , con il quale i tre radiologi avevano unesperienza di utilizzo di almeno 6 mesi . 
the confidence interval for each sample was also assessed . results on the basis of the qualitative analysis , arterial opacification was considered excellent in 39 patients and good in the remaining 11 . 
the renal veins were opacified in six cases but did not , however , affect correct evaluation of the renal arteries from their origin to their intraparenchymal branches : choice of a correct window and use of different 3d reconstructions permitted correct interpretation and differentiation of arterial and venous vessels , in particular at the level of the distal intraparenchymal branches where superimposition often occurs . in five patients with cardiac insufficiency , image quality was considered good , with limited arterial enhancement . in the 50 patients considered , all readers correctly identified the 99 main renal arteries and all 15 accessory arteries ( six for the right kidney and nine for the left kidney )  . 
perfect interobserver agreement was achieved with regard to location of the stenosis in all cases , with excellent correlation with dsa : 19 stenoses located at the ostium of the main artery , two in the proximal main renal artery and two in both the proximal main renal artery and the segmental branches ( fibromuscular dysplasia ) ; there were no cases of stenosis of accessory renal arteries . 
in two patients , all table 1 digital subtraction angiography ( dsa ) and multidetector - row computed tomography ( mdct ) findings : interobserver agreement ( k values ) a , 1st observer ; b , 2nd observer ; c , third observer tabella 1 concordanza tra gli osservatori tra dsa e tcms . 
gli osservatori hanno descritto anche il punto di stenosi coinvolto : 1 , lostio ; 2 , larteria renale prossimale ; 3 , le arterie renali segmentarie ; 4 , larteria renale accessoria . 
il grado di stenosi stato classificato come : 1 , normale ; 2 , malattia moderata ( 0%50% di stenosi ) ; 3 , stenosi di grado severo ( > 50% ) ; 4 , occlusione . analisi statistica i risultati dellanalisi quantitativa sono stati raccolti in un database ( excel per office 2000 ; microsoft corporation ; redmond , washington ) e analizzati per calcolare la concordanza tra gli osservatori mediante un test statistico di cohen ( spss 8.0 per windows ; spss ; chicago , iii ) : scarsa concordanza ( k < 0 , 01 ) , bassa concordanza ( k = 0 , 010 , 20 ) , discreta concordanza ( k = 0 , 210 , 40 ) , buona concordanza ( k = 0 , 410 , 60 ) , sostanziale concordanza ( k = 0 , 610 , 80 ) , concordanza quasi perfetta ( k = 0 , 811 , 00 ) [ 11 ]  . nove arterie sono state valutate di grado diverso da tutti e tre i radiologi che hanno successivamente raggiunto un consensus . 
sono stati calcolati i valori di sensibilit , specificit , accuratezza , valore predittivo positivo ( ppv ) e valore predittivo negativo ( npv ) nellidentificazione del grado di tutte le stenosi e delle stenosi significative ( > 50% ) , rispetto alla dsa che invece stata considerata come gold standard . 
stata inoltre effettuata la valutazione dellintervallo di confidenza per ogni campione . risultati in base allanalisi qualitativa , lopacizzazione arteriosa stata considerata eccellente in 39 pazienti , buona nei restanti 11 : in nessun caso stata considerata scarsa . 
le vene renali sono risultate opacizzate in 6 casi , senza tuttavia determinare limitazioni per la corretta valutazione delle arterie renali nella loro interezza , dallorigine sino alle diramazioni intraparenchimali : la scelta di una corretta finestra e luso di differenti ricostruzioni 3d hanno , infatti , permesso una corretta interpretazione e differenziazione dei vasi arteriosi da quelli venosi , in particolare a livello delle diramazioni distali intraparenchimali dove la sovrapposizione spesso presente . 
in 5 pazienti con insufficienza cardiaca , la qualit delle immagini stata considerata buona con un limitato enhancement arterioso . nei 50 pazienti studiati , tutti i lettori hanno correttamente identificato le 99 arterie renali principali e tutte le 15 arterie accessorie ( 6 per il rene di destra e 9 per il rene di sinistra )  . 
per tutti gli osservatori , laccordo per le due tecniche stato quasi perfetto ( k = 0 , 811 ) , con un valore di k compreso tra 0 , 82 e 0 , 95 . 
mean time for analysis of dsa images was approximately 5 ( range 46 ) min with readings performed on hard copy . discussion stenosis of renal arteries is one of the most common causes fig . 
angio - tcms con ricostruzioni mip ( a ) e dsa ( b ) : presenza di una stenosi severa bilaterale ( frecce ) delle arterie renali dovuta ad una placca dellostio parzialmente calcifica . lettori nella localizzazione della stenosi stato ottenuto in tutti i casi , con unottima correlazione con la dsa : 19 stenosi localizzate allostio dellarteria principale , due nella porzione prossimale dellarteria renale principale e due sia nella porzione prossimale sia nei rami segmentari ( displasia fibro - muscolare ) ; non stato trovato nessun caso di stenosi a livello delle arterie renali accessorie . 
i valori di sensibilit , specificit , e accuratezza rispetto al grado della stenosi sulla base della lettura consensuale sono stati del 100% ( ic 95% : 91 , 4100 ) , of secondary hypertension . 
detection and , above all , correct quantification of the degree of renal artery stenosis is fundamental for planning appropriate treatment : antihypertensive drugs , angioplasty or , more rarely , surgical treatment [ 12 ]  . noninvasive diagnostic techniques such as ultrasonography , fig . 
multidetector - row computed tomography ( mdct ) axial curved multiplanar reconstruction and coronal thin maximum intensity projection ( mip ) ( a , b ) show a < 50% stenosis of the proximal left renal artery due to a calcified plaque ( arrow )  . 
le ricostruzioni delle curve assiali multiplanari e coronali mip a spessore sottile evidenziano una stenosi inferiore al 50% della porzione prossimale dellarteria renale sinistra determinata da una placca calcifica ( freccia ) ( c )  . 
nellidentificazione e nella valutazione del grado delle stenosi severe ( restringimento del lume del 50100% ) la sensibilit , la specificit e laccuratezza sono state del 100% ( ic 95% : 86 , 3100 ) , 97 , 3% ( ic 95% : 92 , 199 , 7 ) e 97 , 8% ( ic 95% : 95 , 8100 ) , rispettivamente , con un valore predittivo positivo e negativo del 98 , 2% ( ic 95% : 8199 , 9 ) e 97 , 8% ( ic 95% : 95 , 9100 )  . le arterie renali accessorie sono state identificate correttamente dai tre lettori sia con la dsa che con langio - tc . il tempo medio per la valutazione delle immagini di tcms su stazioni di lavoro dedicate stato di 12 minuti circa ( compreso tra 10 e 15 minuti ) per i tre lettori . 
il tempo medio di lettura per lanalisi delle immagini di dsa stato di circa 5 minuti ( compreso tra 4 e 6 minuti ) con lanalisi eseguita su pellicola . discussione la stenosi delle arterie renali rappresenta la pi comune causa di ipertensione secondaria . 
la sua identificazione , ed in particolare una corretta quantificazione del grado di stenosi delle arterie renali risulta di fondamentale importanza per una corretta pianificazione del trattamento : terapia farmacologia antiipertensiva , angioplastica o , raramente , trattamento chirurgico [ 12 ]  . 
tecniche diagnostiche non invasive , come lecografia , langio - rm e langio - tc , si sono dimostrate accurate nella valutazione dellipertensione nefrovascolare con lo scopo di ridurre il numero delle angiografie diagnostiche [ 3 , 5 , 7 , 1317 ]  . lecografia di solito utilizzata come tecnica di prima istanza per la valutazione della stenosi delle arterie renali [ 13 ]  . 
il limite principale della ecografia rappresentato dalla difficile finestra acustica in un ampio numero di pazienti e da una relativa bassa sensibilit e specificit nella visualizzazione delle arterie renali accessorie [ 15 ]  . langio - rm una tecnica valida che offre risultati eccellenti nella valutazione delle arterie renali [ 3 , 14 , 15 ] ; il suo limite principale tuttavia limpossibilit di visualizzare i rami segmentari delle arterie renali principali e in alcuni casi le arterie renali accessorie che possono essere responsabili , anche se in un limitato numero di pazienti , di ipertensione nefrovascolare [ 16 ]  . la tc spirale singolo strato stata proposta da molti autori per la valutazione delle arterie renali con risultati promettenti , ma con molte limitazioni ; infatti il rapporto tra il volume da analizzare e la risoluzione spaziale lungo lasse z non permette , in molti casi , la visualizzazione dellorigine delle arterie renali principali e delle arterie accessorie . 
multidetector - row computed tomography ( mdct ) angiography ( a ) demonstrates irregular appearance of the ventral branch of the right renal artery with a string - of - beads morphology typical of fibromuscular dysplasia . 
il quadro tc confermato dalla dsa ( b )  . mr angiography and ct angiography have proved to be accurate in assessment of secondary hypertension and provide valuable alternatives to diagnostic angiography [ 3 , 5 , 7 , 1317 ]  . ultrasonography is normally used as a first - line approach in evaluation of renal artery stenoses [ 13 ]  . 
its main limitations are a difficult acoustic window in a large number of patients and relatively low sensitivity and specificity in depicting accessory renal arteries [ 15 ]  . mr angiography is a valuable technique that offers excellent results in assessment of renal arteries [ 3 , 14 , 15 ] ; its main limit is an inability to depict segmental branches of main renal arteries and in some cases accessory renal arteries , which may be responsible of secondary hypertension in a small number of patients [ 16 ]  . 
 single - slice spiral ct has often been proposed for evaluation of renal arteries with promising results , but it also suffers many limitations since the ratio between the volume to be analysed and spatial resolution in the z axis often does not allow visualisation of the origin of main renal arteries and accessory arteries . 
in addition , long scan times result in enhancement of the renal veins and possible breathing artefacts in patients with limited breath - hold capabilities , with resulting poor quality of 3d reconstructions , which have become integral to diagnosis for both clinicians and radiologists . the recent introduction of mdct has considerably shortened acquisition times of increasingly large volumes , with excellent longitudinal resolution and near - isotropic voxels , which allow for high - quality multiplanar and volume rendered reconstructions , reduced contrast material , excellent arterial enhancement without venous - system interference and fewer motion artefacts . 
in view of these advantages , this study toria , con una conseguente relativa limitata qualit delle ricostruzioni tridimensionali , che sono diventate parte integrante della diagnostica sia per i radiologi che per i clinici . la recente introduzione della tcms ha incrementato notevolmente la velocit di acquisizione di volumi sempre pi ampi , con una eccellente risoluzione longitudinale e con voxels pressoch isotropici , che permettono ricostruzioni multiplanari e volume rendering di alta qualit , una riduzione nella somministrazione di mezzo di contrasto , una ottima opacizzazione arteriosa , scevra da sovrapposizione del sistema venoso ed una riduzione degli artefatti da movimento . in virt dei suddetti vantaggi della tcms lo scopo di questo studio stato di verificare la capacit diagnostica della angio - tcms nella valutazione delle arterie renali . nella maggior parte dei pazienti del nostro studio , la qualit delle immagini stata considerata eccellente e con un ottimo enhancement anche nei pazienti con associate altre patologie cardio - vascolari , senza sovrapposizioni da parte del sistema venoso . 
nei pochi casi di sovrapposizione stata comunque possibile una ottima visualizzazione del sistema arterioso grazie alle ricostruzioni 3d . nellanalisi quantitativa , laccordo tra gli osservatori stato quasi perfetto sia per langio - tc che per la dsa ; nella valutazione del grado di stenosi , langio - tc ha mostrato unelevata specificit ( 97 , 8% ) , anche quando ristretta a stenosi severe ( > 50% )  . un caso considerato come stenosi di primo grado con dsa stato considerato di secondo grado con la tcms : questo errore diagnostico non ha modificato il programma terapeutico n i valori di sensibilit o specificit per le stenosi di grado severo ( > 50% )  . 
al contrario , in altri due pazienti , langio - tcms ha sovrastimato la stenosi di un grado aimed at evaluating the diagnostic capabilities of mdct angiography in assessment of renal arteries . in the majority of the patients examined , image quality was considered excellent , with optimal enhancement , even in patients with other associated cardiovascular disorders , without overlapping venous enhancement . 
in quantitative analysis , interobserver agreement was almost perfect for both mdct and dsa ; in evaluating degree of stenosis , mdct angiography had high specificity ( 97.8% ) , even when restricted to severe stenoses ( > 50% )  . 
one case assessed as a grade 1 stenosis with dsa was considered a grade 2 stenosis with mdct : this diagnostic error did not change treatment or sensitivity or specificity for severe stenoses ( > 50% )  . 
moreover , the use of protocols with thin collimations , which are routinely adopted with the latest generations of mdct ( 16 , 64 slices ) , may further improve spatial resolution and allow more accurate distinction between wall calcifications and residual lumen in severe stenosis . 
in addition , in order to limit diagnostic errors in the case of wall calcification , use of a soft window will allow differentiation between residual lumen and calcific atherosclerotic plaque . 
on the other hand , visualisation of vessel walls is a major advantage of ct not only over dsa but also over other noninvasive modalities , as it allows evaluation both of plaque components and , in particular , wall calcification and also of the residual lumen . there are two important limitations of mdct angiography : the use of ionising radiation , and iodinate contrast material . 
as regards nonionic iodinated contrast material , it should be noted that it is less nephrotoxic compared with ionic contrast agents and that it is well tolerated even by high - risk patients [ 18 ]  . 
it has recently been demonstrated that nonionic iodinated contrast agents can be used , even in patients with impaired renal function , without significant risk of nephrotoxic effects [ 19 ]  . 
the advent of new and faster ct scanners ( 16 , 64 slices ) means that even less contrast material is required to obtain good assessment of renal arteries , and use of saline solution injected immediately after the contrast bolus allows further reduction in volume to be injected and greater bolus uniformity . 
as regards the use of ionising radiation , we need to consider that the dose used in ct is significantly lower than that used for dsa and that the protocol used in this study was optimised with respect to previous studies , maintaining , however , a high diagnostic quality [ 20 ]  . 
recent studies have demonstrated the possibility of using low - dose protocols for other body districts , with excellent results in terms of image quality and diagnostic capabilities [ 21 , 22 ]  . one limitation of our study is the small number of patients f . 
inoltre , luso di protocolli con collimazioni sottili , che sono impiegati routinariamente con le ultime generazioni di tcms ( 16 , 64 strati ) possono ulteriormente migliorare la risoluzione spaziale e permettere una pi accurata distinzione tra calcificazioni parietali e lume residuo nel caso di stenosi severe ; inoltre , per limitare errori diagnostici nel caso di calcificazioni parietali , lutilizzo di una finestra morbida consente la differenziazione tra lume residuo e placca aterosclerotica calcifica . 
daltra parte , la visualizzazione delle pareti dei vasi un importante vantaggio della tc , nei confronti non solo della dsa , ma anche delle altre metodiche non invasive , in virt della capacit di valutare sia i costituenti della placca ed in particolare le apposizioni calcifiche parietali , sia il lume residuo . ci sono due importanti limitazioni dellangio - tc : luso di radiazioni ionizzanti e di mezzo di contrasto iodato . 
per quanto riguarda il mezzo di contrasto iodato non ionico bisogna ricordare che la sua nefrotossicit limitata rispetto ai mezzi di contrasto ionici , e che ben tollerato anche in pazienti ad alto rischio [ 18 ]  . nella nostra popolazione di studio non stato rilevato nessun incremento dei livelli sierici di creatinina dopo lesecuzione dellesame . 
 stato recentemente dimostrato come anche nei pazienti con una funzionalit renale compromessa i mezzi di contrasto iodati non ionici possono essere somministrati senza significativi rischi di nefrotossicit [ 19 ]  . 
inoltre la quantit di mezzo di contrasto utilizzata con la tcms inferiore rispetto a quella utilizzata con la tc spirale a singolo strato , grazie allincremento di velocit nellacquisizione delle immagini . 
lintroduzione di nuove e pi veloci tc ( 16 , 64 strati ) permette inoltre di ridurre ancor di pi la quantit di mezzo di contrasto necessario per ottenere una buona valutazione delle arterie renali . inoltre , luso di una soluzione salina iniettata subito dopo il bolo di mezzo di contrasto permette una ulteriore riduzione del volume da iniettare ed una maggior uniformit del bolo . 
per quanto riguarda luso di radiazioni ionizzanti , bisogna tener presente che la dose utilizzata in tc significativamente inferiore rispetto a quella utilizzata per la dsa e che il protocollo utilizzato in questo studio stato ottimizzato rispetto agli studi precedentemente pubblicati mantenendo tuttavia una elevata qualit diagnostica [ 20 ]  . 
sono stati ultimamente pubblicati degli studi che hanno dimostrato la possibilit di utilizzare protocolli a bassa dose di radiazioni ionizzanti per altre parti del corpo con risultati eccellenti in termini di qualit di immagini e di capacit diagnostiche [ 21 , 22 ]  . una limitazione del nostro studio rappresentata dal basso numero di pazienti con stenosi significative ( 50%100% ) e leterogeneit della nostra popolazione che includeva pazienti con patologie diverse : ipertensione nefrovascolare , malattia occlusiva aorto - iliaca , patologia dilatativa . 
a further major advantage of mdct is the possibility of visualising the entire aortoiliac axis , including the renal arteries , in a single examination without loss of enhancement or superimposition of the venous system using thin collimations and high spatial resolution . 
in conclusion , this study demonstrated that mdct angiography is very accurate and reproducible in evaluation of renal arteries and stenosis and has the potential to replace digital angiography . tato dalla possibilit di visualizzare in un unico esame lintero asse aorto - iliaco , comprese le arterie renali senza perdita di enhancement o senza sovrapposizione del sistema venoso , usando collimazioni sottili ed elevata risoluzione spaziale . difficile determinare quale sar il ruolo dellangiotcms rispetto allangio - rm . 
villari1 1sezione di radiodiagnostica , dipartimento di fisiopatologia clinica , universit degli studi , azienda ospedaliero - universitaria di careggi , viale morgagni 85 , i - 50134 firenze , italy 2sezione di radiodiagnostica , universit degli studi , azienda ospedaliero - universitaria senese , policlinico le scotte , siena , italy 3unit clinica operativa di radiologia , universit degli studi , ospedale di cattinara , trieste , italy correspondence to : s . 
 + 39 - 055 - 4377673 , fax : + 39 - 055 - 431970 , e - mail : s.colagrande@dfc.unifi.it received : 23 june 2005 / accepted : 23 july 2005 / published online : 11 april 2006 abstract diffusion - weighted ( dw ) imaging has for a number of years been a diagnostic tool in the field of neuroradiology , yet only since the end of the 1990s , with the introduction of echoplanar imaging ( epi ) and the use of sequences capable of performing diffusion studies during a single breath hold , has it found diagnostic applications at the level of the abdomen . 
the inherent sensitivity to motion and the magnetic susceptibility of dw sequences nonetheless still create problems in the study of the abdomen due to artefacts caused by the heartbeat and intestinal peristalsis , as well as the presence of various parenchymal - gas interfaces . 
with regard to focal liver lesions , a review of the literature reveals that dw imaging is able to differentiate lesions with high water content ( cysts and angiomas ) from solid lesions . 
with regard to the latter , although there are differences between benign forms [ focal nodular hyperplasia ( fnh ) , adenoma ] and malignant forms [ metastasis , hepatocellular carcinoma ( hcc ) ] in their apparent diffusion coefficient ( adc ) in the average values for histological type , there is a significant overlap in values when lesions are assessed individually , with the consequent problem of their correct identification . 
one promising aspect is the possibility of quantifying the degree of fibrosis in patients with chronic liver disease and cirrhosis given that the deposit of collagen fibres restricts the motion of water molecules and therefore reduces adc values . 
here it is possible to differentiate mucin - producing tumours of the pancreas from pseudocystic forms on the basis of adc values even though the limited spatial resolution of dw imaging does not enable the identification of small lesions . 
in addition , given that renal parenchyma has significantly variable adc values on the basis of the anatomic section and physiological conditions , the possibility of assessing functional alterations is currently being studied . 
with regard to musculoskeletal applications , the absence of riassunto in ambito neuroradiologico , limaging pesato in diffusione pu essere considerato una realt diagnostica da vari anni , mentre a livello addominale , soltanto verso la fine degli anni 90 , quindi con lintroduzione delle tecniche eco - planari ( epi ) , si sono rese disponibili sequenze tali da consentire studi di diffusione a respiro sospeso . 
lintrinseca sensibilit al movimento e alla suscettivit magnetica delle sequenze diffusione - pesate ( diffusion - weighted , dw ) rende tuttavia problematico , ancora oggi , lo studio delladdome superiore , per gli artefatti secondari allattivit cardiaca e alla peristalsi intestinale , nonch per la presenza di varie interfacce parenchimi - gas . 
per quanto riguarda la patologia epatica focale , una revisione della letteratura indica che limaging dw permette di differenziare le lesioni ad elevato contenuto acquoso ( cisti ed angiomi ) da quelle solide . 
fra queste ultime , pur esistendo differenze di coefficiente apparente di diffusione ( adc ) , nei valori medi per tipo istologico , fra forme benigne ( fnh , adenoma ) e maligne ( metastasi , hcc ) , si rileva anche unampia sovrapposizione di valori fra le lesioni valutate singolarmente , con conseguenti problemi in termini di caratterizzazione . 
interessanti le possibilit di quantificare il grado di fibrosi nei pazienti con epatopatia cronica e cirrosi , dal momento che la deposizione di fibre collagene , restringendo i movimenti molecolari dellacqua , comporta una riduzione dei valori di adc ; anche in questo settore , gli studi sono tuttavia da considerare preliminari , lontani da una reale applicazione in ambito clinico . 
nel retroperitoneo , distretto meno interessato da artefatti da movimento , altrettanto degna dattenzione risulta la possibilit di differenziare fra neoplasie pancreatiche mucinose e forme pseudocistiche , in funzione dei valori di adc , anche se la limitata risoluzione spaziale propria delle immagini dw , non permette il rilievo di lesioni di piccole dimensioni . 
inoltre , dal momento che il parenchima renale presenta valori di adc molto variabili in funzione della porzione anatomica e delle condizioni fisiologiche , allo studio la possibilit di valutare le alterazioni della funzione ; ad oggi stata riscontrata una buona correlazione tra i valori di adc e lentit del filtrato glomerulare . 
greater agreement has been found regarding sensitivity of the technique in assessing response of these tumours to chemotherapy : tumour necrosis is thought to increase adc whereas the persistence of vital neoplastic tissue tends to lower it . one of the most promising applications of dw imaging is without doubt the assessment of vertebral collapse where a high adc has been shown to be associated with an osteoporotic cause and a low adc with a neoplastic cause . 
in particular , no significant difference in adc is noted between normal hypercellular bone marrow and hypercellular bone marrow secondary to lymphomatous infiltration whereas this difference is significant between hypocellular , normocellular and haematopoietic hypercellular bone marrow . 
with regard to the study of joints , the limited structure dimensions , particularly cartilage , creates technical difficulties related to spatial resolution and an adequate signal - to - noise ratio , problems that can only be solved by further technological developments . 
si cos tentato di utilizzare limaging dw nella caratterizzazione delle neoplasie dei tessuti molli , anche se con risultati per il momento controversi . maggiore accordo vi invece sulla sensibilit di tale tecnica nella valutazione della risposta di questi tumori alla chemioterapia : la necrosi tissutale determinerebbe , infatti , un aumento delladc , diminuito viceversa al permanere di tessuto neoplastico vitale . una delle applicazioni pi promettenti dellimaging dw senza dubbio la valutazione dei crolli vertebrali , nei quali si dimostrato un adc elevato ove la causa sia porotica e ridotto ove neoplastica ; anche in questo caso si riscontra tuttavia un discreto overlap fra gli adc delle due popolazioni . 
in particolare non si rileva significativa differenza di adc tra il midollo ipercellulare normale e quello secondario ad infiltrazione linfomatosa , mentre tale differenza significativa tra il midollo ipocellulare , quello normocellulare e lipercellulare emopoietico . 
in ambito articolare , le ridotte dimensioni delle strutture di interesse e in particolare delle cartilagini , determinano difficolt tecniche inerenti la risoluzione spaziale ed un adeguato rapporto s / r , problemi che impongono ulteriori sviluppi della tecnologia . 
the main field of application of the earliest studies in molecular diffusion was neuroradiological [ 1 ] , where diffusion - weighted ( dw ) sequences play an important part in the diagnosis of cerebral ischaemia in the hyperacute phase ( 06 h )  . 
at the same time , other applications were developed regarding both the characterization of brain tumours ( with the possibility of differentiating the cystic / oedematous lesions from solid forms ) and more recently the assessment of demyelinating diseases . from applications limited to neuroradiology , steps have progressively been taken in other body regions , such as the abdomen [ 24 ] and musculoskeletal system [ 57 ] both in adults and paediatric patients . 
this interest is justified by the potential of dw imaging to qualitatively and quantitatively assess molecular motion on the basis of microstructural organization of the region being studied . i recenti avanzamenti tecnologici nel settore delle apparecchiature a risonanza magnetica ( rm ) hanno portato allo sviluppo di macchine commerciali con prestazioni sempre pi elevate , sia per quanto riguarda lintensit / omogeneit di campo magnetico , che le caratteristiche dei gradienti , rendendo possibili studi con tecniche avanzate , come la valutazione del parametro diffusione ( d )  . 
i primi studi sulla diffusione molecolare hanno avuto come principale campo dapplicazione lambito neuroradiologico [ 1 ] , ove le sequenze diffusione - pesate ( diffusion - weighted , dw ) rappresentano un momento importante nella diagnostica dellischemia cerebrale in fase iperacuta ( 06 ore )  . 
parallelamente , sono state sviluppate altre applicazioni riguardanti sia la caratterizzazione delle lesioni neoplastiche encefaliche ( con la possibilit di differenziare le forme cistiche / edematose dalle solide ) sia , pi di recente , la valutazione delle malattie demielinizzanti . da tali applicazioni circoscritte allambito neuroradiologico si progressivamente passati allo studio di altri distretti corporei , come laddome [ 24 ] e lapparato muscolo scheletrico [ 57 ] sia nelladulto che nel piccolo paziente . tale interesse risulta giustificato dalle potenzialit dellimas . 
the following summary is limited to the main technical problems related to the region being studied . in the abdomen the study of the diffusion parameter became possible with the development of ultrafast sequences . this enabled the entire acquisition to be made in a single breath hold , thus eliminating respiratory artefacts and reducing those resulting from vascular pulsation and intestinal peristalsis , which lower the signal - to - noise ratio ( snr ) and create difficulties for quantitative analysis . those ultrafast sequences were echoplanar imaging ( epi ) sequences , which , thanks to acquisition of around 3060 ms per image , reduce artefacts due to macroscopic physiological motion . the high acquisition speed , however , does have its limits , especially with regard to spatial resolution . 
the abdominal organs and their relative focal lesions do not possess a characteristic structural organization like the fibres of white matter . the sequences adopted for the study of the abdomen , therefore , are very similar to those used for the study of ischaemic disease in the brain . technically speaking , based on our experience and in line with other studies on the subject [ 24 ] , the mr examination should be performed with a high - field superconductive magnet ( 1.5 t ) equipped with 2330 mt / m intensity gradients , a slew rate of 150 mt / m per second and phased - array surface coils . 
all sequences are acquired in breath hold to reduce respiratory artefacts . after a preliminary conventional study with t1and t2weighted sequences , dw images are acquired using a variation of the spin - echo sequence ( stejskal and tanner sequence ) performed with the single - shot echoplanar technique ( se - epi - ssh )  . this entails a classic spin - echo sequence characterized by two successive radiofrequency impulses at 90 and 180 , to which two additional gradients known as motion - probing gradients ( mpgs ) equal in breadth and duration but opposite in direction are added immediately before and after the 180 impulse . the amount of weighting in diffusion of the sequence is ging dw nella valutazione quali - quantitativa del movimento molecolare in funzione dellorganizzazione microstrutturale del distretto esaminato . scopo di questa rassegna quello di presentare le principali esperienze maturate con lacquisizione in diffusione in ambito addominale e muscolo - scheletrico , compresi alcuni cenni sulla patologia pediatrica . note di tecnica per quanto riguarda i fondamenti dellimaging dw dal punto di vista fisico , tecnico e semeiotico si rimanda ad una precedente nota [ 8 ]  . 
di seguito ci limitiamo a ricordare i principali problemi di natura tecnica , in funzione del distretto da esaminare . a livello addominale lo studio del parametro diffusione stato permesso dallo sviluppo di sequenze ultraveloci che consentono lintera acquisizione in una singola apnea , in modo da eliminare gli artefatti respiratori e ridurre quelli secondari a pulsatilit vascolare e peristalsi intestinale , che diminuiscono il rapporto segnale / rumore ( s / r ) e rendono problematica lanalisi quantitativa . 
tali sequenze ultraveloci sono rappresentate dalle sequenze eco - planari ( echo - planar imaging , epi ) che , grazie a tempi di acquisizione dellordine di 3060 ms per immagine , riducono gli artefatti dovuti ai movimenti fisiologici macroscopici . 
pertanto le sequenze adottate in ambito addominale possono essere assimilate a quelle che si utilizzano per lo studio delle malattie ischemiche encefaliche . dal punto di vista tecnico , sulla base della nostra esperienza ed in accordo con quanto riportato dagli autori che si sono occupati dellargomento [ 24 ] , necessario eseguire lesame rm con un magnete superconduttivo ad alto campo ( 1 , 5 t ) , dotato di gradienti di intensit pari a 2330 mt / m e slew rate di 150 mt / m / s , e con bobine di superficie del tipo phased - array . 
tutte le sequenze sono acquisite a respiro sospeso ( breath - hold , bh ) per ridurre gli artefatti secondari ai movimenti respiratori . dopo un preliminare studio tradizionale tramite sequenze t1 e t2 - pesate , vengono acquisite le immagini dw , avvalendosi di una variante della sequenza spin eco ( sequenza di stejskal e tanner ) assunta con tecnica eco - planare del tipo single - shot ( se - epi - ssh ) : sullo schema di una classica spin eco , caratterizzata da due impulsi di radiofrequenza in sucs . 
a field lines in the air ( 1 ) and in the context of the object immersed in the magnetic field ( 2 ) with the consequent deviation of the magnetic field itself . 
b single - shot echoplanar ( se - epi ) image with b = 0 of a cylindrical phantom containing water ; three smaller cylinders containing ultrasound gel are placed around it . 
c note deformation of the cylinder in the se - epi image weighted in diffusion ( b = 800 s / mm2 ) without the presence of the cylinders , which already shows the sequence sensitivity to magnetic susceptibility . 
c notare la deformazione del cilindro nella immagine se - epi pesata in diffusione ( b = 800 s / mm2 ) senza la presenza dei cilindri , che gi evidenzia la sensibilit della sequenza alla suscettibilit magnetica . 
d dopo riposizionamento dei cilindri tale reperto pi accentuato a livello dellinterfaccia tra cilindro di acqua e cilindro di gel ( freccia nera ) come deformazione focale del profilo del fantoccio nella direzione della codifica di fase . defined by the factor b [ expressed in seconds per millimetre squared ( s / mm2 ) ] , which summarizes gradient characteristics according to the formula b = 2g22 ( - / 3 ) where is the gyromagnetic constant , g and are the breadth and the duration of the diffusion gradients , respectively , and is the time interval between their application [ 8 ]  . 
diffusion produces a reduction in cessione a 90 e 180 , vengono applicati , immediatamente prima e dopo limpulso a 180 , due gradienti aggiuntivi uguali per ampiezza e durata , ma contrari per verso , detti gradienti di diffusione ( motion probing gradients , mpgs )  . lentit della pesatura in diffusione della sequenza definita dal fattore b ( espresso in s / mm2 ) , che riassume le caratteristiche dei gradienti , secondo la formula : b = 2g22 ( - / 3 ) dove la costante giromagnetica , g e sono rispettivas . 
adc is usually measured by linear regression analysis with the following formula : adc = ln ( s0 / s ) / b the other parameters of the sequence generally used are : tr 1 , 8005 , 000 ms , 60 < te < 120 , matrix 128x128256 , number of measurements 1 , indicative band width 2 , 080 hz / pixel , number of sections acquired 1220 , slice thickness 58 mm , and field of view ( fov ) variable based on the build of the patient . chemical - shift artefacts are reduced by systematically using fat presaturation . 
in addition , where possible the use of parallel imaging can be an advantage , a technique capable of reducing acquisition time or increasing the matrix and therefore the spatial resolution without altering the acquisition time and without significant loss in image quality ( sensitivity encoding , sense ) [ 9 ]  . in the postprocessing phase , the various dw images are used to obtain the respective adc maps on which quantitative analysis of the signal is performed by positioning a region of interest ( roi ) on the structure being studied . as we shall see , the choice of the b value and therefore the degree of weighting in diffusion is a problem that cannot be overlooked and for which no solution has yet been found . various studies using different b values have yielded different results of these , we would like to draw particular attention to the significant differences reported in the literature between adc values of the normal and cirrhotic liver as well as focal hepatic lesions . 
the current tendency is to use a superconductive magnet with a field intensity of 1.5 t , gradients of 30 mt / m , slew rate of 150 mt / m per second and a 4channel phased - array coil [ 10 ]  . 
various sequences have been proposed to reduce sensitivity to magnetic susceptibility typical of epi and improve spatial resolution in acquisitions that require an fov smaller than those used for the abdomen . the first attempts were made with conventional spin - echo sequences , which have a high snr and very low magnetic susceptibility , but acquisition times were calculated in minutes , with a consequent increase in sensitivity to motion artefacts [ 1 ]  . mente lampiezza e la durata dei gradienti di diffusione e lintervallo di tempo intercorrente fra la loro applicazione [ 5 ]  . 
la diffusione produce una riduzione dellintensit di segnale in ogni pixel data da : s = s0e - bxadc dove s rappresenta lintensit di segnale nel pixel dopo lapplicazione dei gradienti di diffusione per un dato valore di b , s0 lintensit di segnale con b pari a 0 , mentre adc il coefficiente di diffusione apparente ( espresso in mm2 / s )  . ladc viene di solito misurato per mezzo dellanalisi della regressione lineare calcolata sulla base della seguente formula : adc = ln ( s0 / s ) / b gli altri parametri della sequenza generalmente utilizzati sono i seguenti : tr 18005000 ms , 60 < te < 120 ms , matrice 128x128256 , numero di misure 1 , ampiezza di banda indicativa 2080 hz / pixel , numero di sezioni acquisite 1220 , spessore di strato 58 mm , fov variabile in funzione della corporatura del paziente . 
inoltre , ove disponibile , pu essere vantaggioso utilizzare una tecnica di acquisizione parallela delle immagini ( parallel imaging ) che consente di ridurre il tempo di acquisizione o , alternativamente , di aumentare la matrice e quindi la risoluzione spaziale a parit di tempo di acquisizione , senza significativo degrado della qualit delle immagini ( sensitivity encoding , sense ) [ 9 ]  . 
in fase di postprocessing , dalle varie acquisizioni diversamente pesate in diffusione vengono ottenute le rispettive mappe adc sulle quali possibile eseguire lanalisi quantitativa del segnale posizionando una regione di interesse ( region of interest , roi ) sulla struttura in esame . come vedremo , la scelta del valore di b e quindi il grado di pesatura in diffusione un problema non trascurabile e non ancora risolto ; se osserviamo la letteratura riguardante largomento , infatti , vari autori utilizzando valori diversi di b , sono giunti a risultati non sovrapponibili . 
fra tutti vogliamo ricordare le notevoli differenze riportate in letteratura fra i valori di adc del fegato normale e cirrotico , nonch delle lesioni focali epatiche . in ambito retroperitoneale i problemi legati ai movimenti respiratori , cardiaci e peristaltici si rendono meno evidenti . attualmente la tendenza quella di utilizzare un magnete superconduttivo con intensit di campo di 1 , 5 t , gradienti pari a 30 mt / m , velocit di raggiungimento del picco di 150 mt / m / s , con limpiego di una bobina phased - array a 4 canali [ 10 ]  . 
le immagini di diffusione vengono acquisite utilizzando una sequenza se - epi - ssh ( tr = 2883 , te = 61 , flip angle = 90 , fov variabile , matrice = 128x256 ) , con valori di b pari a 0 e a 500 s / mm2 ( comunque possibile acquisire con pi alti valori di b ) ; viene impiegata inoltre una tecnica di acquisizione parallela delle immagini . table 1 summary of results of most cited studies . 
numero di pazienti studiati , valori di fattore b utilizzati ( in ordine crescente ) e valori di adc delle principali lesioni focali epatiche riportati dagli autori citati nel testo . 
other sequences commonly reported in the literature , especially for the study of cartilage , are based on steady - state free precession ( ssfp )  . these sequences have relatively short acquisition times although they are not directly comparable with epi - dw sequences , as well as a high snr . 
however , performing quantitative assessments of diffusion is not a simple matter : the b value in this type of sequence , required to calculate adc , is not clearly definable without knowing the t1 and t2 relaxation times [ 12 ]  . most studies in the literature , however , reveal that currently , the most commonly used sequences are se - epi - ssh [ 13 ] , with a configuration not unlike that presented above with regard to the study of the abdomen and retroperitoneu the use of dedicated coils , a slice thickness of 46 mm , fov relative to the segment being studied and a matrix of 128x128256 are obviously required . the most important parameter is still the b value , which , as noted earlier , determines the real weighting in diffusion of the sequence . 
in letteratura sono state proposte sequenze di vario tipo al fine di ridurre la sensibilit alla suscettibilit magnetica , propria della tecnica epi , e di migliorare la risoluzione spaziale in acquisizioni che necessitano di fov inferiori a quelli usati per laddome . i primi tentativi sono stati effettuati con sequenze spin eco convenzionali , che presentano elevato rapporto s / r e scarsa suscettibilit magnetica , ma tempi di acquisizione calcolabili in minuti , con incremento conseguente della sensibilit agli artefatti da movimento [ 1 ]  . 
per ovviare a tale inconveniente sono state pertanto usate da alcuni autori sequenze single - shot multi - eco ( rapid acquisition with relaxation enhancement , rare , o half - fourier acquired single - shot turbo spin - eco , haste ) , anche se i dati in proposito sono ancora scarsi [ 11 ]  . 
altre sequenze frequentemente riportate in letteratura , soprattutto nella valutazione delle cartilagini , sono quelle basate sulla steady - state free precession ( ssfp ) : esse presentano tempi di acquisizione relativamente brevi , anche se non sovrapponibili a quelli delle epi - dw , ed elevato rapporto s / r . 
non tuttavia semplice eseguire valutazioni quantitative della diffusione ; in questo tipo di sequenze , infatti , il valore del fattore b , necessario per il computo delladc , non chiaramente definibile senza conoscere i tempi di rilassamento t1 e t2 [ 12 ]  . attualmente , come si evince dalla maggior parte degli s . 
one of the promising applications in the study of the liver involves characterization of focal hepatic lesions following the demonstration of differences in mean adc values measured in hepatocellular carcinoma ( hcc ) , metastases and hepatic angiomas studi presenti in letteratura , vengono utilizzate sequenze seepi - ssh [ 13 ] , configurate in modo non dissimile da quanto gi riportato in precedenza a proposito del distretto addominale e retroperitoneale . ovviamente necessario lutilizzo di bobine dedicate , spessore di strato compreso tra 4 e 6 mm , fov relativo al segmento in esame e matrice 128x128256 . 
b , c in diffusion - weighted ( dw ) images with b = 0 and 1 , 000 s / mm2 , the signal remains high even with elevated weighting in diffusion . 
 [ 15 ] studied 74 hepatic lesions ( 48 hcc , 15 metastases and 11 angiomas ) ( table 1 ) using the sequences and the protocol mentioned above [ 15 ] , with some minor variations . since high b values ( > 400 s / mm2 ) reduce the signal intensity of the liver with resulting poor image quality , the authors chose to use b values equal to 1.6 , 16 and 55 s / mm2 , thus obtaining three sets of differently weighted dw images , even though with such low b values the image proves to be more influenced by phenomena of perfusion and t2 relaxation time ( shine through ) than by diffusion . 
all types of lesions ( hcc , metastases and angiomas ) showed mean adc values higher than those of normal and cirrhotic liver except for some cases of metastases . the mean adc value of angiomas was the highest , followed by that of hcc and metastases ( table 1 )  . 
ad esempio , la milza ha basso adc , che sta ad indicare ridotta mobilit delle molecole di acqua , mentre la corticale renale presenta valori di adc estremamente alti . lutilit clinica delle immagini dw a livello addominale non ancora chiara , sebbene esistano potenziali applicazioni nello studio del fegato , del pancreas e dei reni . 
hanno studiato 74 lesioni epatiche ( 48 hcc , 15 metastasi ed 11 angiomi ) ( tabella 1 ) avvalendosi , a parte piccole variazioni , delle sequenze e del protocollo ricordato nel paragrafo precedente [ 15 ]  . 
a turbo spin echo ( tse ) t2 - weighted image ( te = 80 ms ) showing degenerative nodule of about 3 cm in diameter in the iii hepatic segment , which has induced thrombosis in the portal branch of the left lobe . 
b , c single - shot echoplanar diffusion - weighted ( se - epi - dw ) images obtained with b = 0 and 1 , 000 s / mm2 in which the solid malignant lesion is clearly visible with a necrotic component at its centre ; the surrounding parenchyma has a relatively hyperintense signal owing to reduced diffusion of water molecules induced by the thrombosis . 
a immagine tse t2 pesata ( te = 80 ms ) nella quale si apprezza nodulo degenerativo del diametro di circa 3 cm nel iii segmento epatico , inducente trombosi nella diramazione portale per il lobo sinistro . 
b , c immagini se - epi - dw ottenute con b = 0 e 1000 s / mm2 nelle quali si rende ben evidente la lesione solida maligna che presenta al centro una componente necrotica ; il circostante parenchima presenta segnale relativamente iperintenso , in relazione alla diminuita diffusivit protonica indotta dalla trombosi . 
d mappa adc : il valore di adc dellepatocarcinoma risulta pari a 1 , 130 , 18x10 - 3 mm2 / s . the problem of the correct choice of the b value therefore appears vital , and in those years , it was tackled most convincingly by yamada et al . 
this microscopic motion in biological tissue includes not only molecular diffusion of water but also microcirculation of blood ( perfusion )  . due to the random organization of the capillary network at the level of the voxel , even the microcirculation of blood can be considered incoherent motion . 
this corresponds to the true diffusion coefficient ( d ) only when diffusion is the only type of motion present ( as occurs in a test tube containing distilled water )  . 
 [ 17 ] performed a thorough analysis of the phenomenon , showing that adc values calculated withmagine , tali autori hanno ritenuto di utilizzare valori di b pari a 1 , 6 , 16 e 55 s / mm2 ottenendo tre set di immagini diversamente pesate in diffusione , anche se , con valori di b cos bassi , limmagine risulta maggiormente influenzata da fenomeni di perfusione e dal tempo di rilassamento t2 ( shine through ) piuttosto che dalla diffusione . 
tutti i tipi di lesioni ( hcc , metastasi ed angiomi ) hanno evidenziato valori medi di adc superiori a quelli del fegato normale e cirrotico a parte alcuni casi di metastasi ; in particolare ladc medio degli angiomi risultato il pi alto , seguito da quelli dellhcc e delle metastasi ( tabella 1 )  . 
examinations with low b values suffer significantly from t2 effects ( shine through ) , and calculation of adc on the maps obtained contains a significant amount of nondiffusional ivim , often derived from perfusion . it would therefore be fair to say that such examinations are little weighted in d and heavily weighted in t2 and perfusion , and the same authors suggest it is worthwhile assessing the effective d and the perfusion fraction f with multiple measurements and an increasing b value ( up to 1 , 100 s / mm2 ) ( table 1 )  . it should be borne in mind , however , that measurements performed with b > 1 , 000 s / mm2 provide low - quality images , with an unfavourable snr and low spatial resolution . 
in addition , repeated measurements with increasing b values lengthens acquisition times , creating problems of repeatability , particularly with less - than - cooperative patients . other relevant considerations can be found in a thoroughly conducted study [ 18 ]  . 
the authors made acquisitions with varying b values on a phantom containing two liquids with known adc values ( of course , adc = d in these cases ) , namely , water ( 2.29x10 - 3 mm2 / s ) and acetone ( 3.98x10 - 3 mm2 / s )  . the aim was to obtain a definite reference parameter for the measurements performed . 
the acquisitions demonstrate significant differences between normal and cirrhotic liver ( table 1 ) and between benign and malignant hepatic lesions . with a threshold of 1.6x10 - 3 mm2 / s and a maximum b value < 846 s / mm2 , a sensitivity of 98% and a specificity of 80% are achieved in differentiating malignant from benign lesions . a revision of the subject was recently performed in a particularly interesting manner , both from the technical and conceptual point of view [ 4 ]  . 
the study involved 66 patients affected by 52 cystic , angiomatous , solid benign and malignant focal hepatic lesions with diameters between 1 and 15 cm ( table 1 )  . assessment was also extended to the normal and cirrhotic parenchyma . 
the study showed there is no statistically significant difference between adc values ( of normal parenchyma , cirrhotic parenchyma and focal hepatic lesions ) measured in the three directions , unlike in the brain and kidneys . 
a causa dellorganizzazione casuale della rete capillare a livello del voxel , infatti , anche la microcircolazione del sangue pu essere considerata un movimento incoerente . pertanto , ladc include tanto gli effetti della diffusione propriamente detta o vera , quanto quelli della perfusione ( pseudodiffusione ) ; corrisponde al coefficiente di diffusione vero ( d ) soltanto quando la diffusione lunico tipo di movimento presente ( come avviene nella provetta contenente acqua distillata )  . 
yamada ha effettuato unanalisi approfondita del fenomeno , dimostrando che i valori di adc , calcolati senza tener conto degli effetti della perfusione , risultano poco utili per differenziare le lesioni epatiche [ 17 ]  . 
la valutazione con bassi valori di fattore b risente infatti fortemente degli effetti del t2 ( shine through ) ed il calcolo delladc sulle mappe cos ottenute contiene una quota importante di ivim non diffusionali , specie derivanti da perfusione : si potrebbe dunque affermare che queste valutazioni sono poco pesate in d e molto in t2 e in perfusione , mentre secondo gli stessi autori viceversa utile valutare la d effettiva e la frazione di perfusione f tramite multiple misure con b crescenti ( fino a 1100 s / mm2 ) ( tabella 1 )  . 
 tuttavia da ricordare che le misure con b > 1000 s / mm2 comportano immagini di bassa qualit con rapporto s / r sfavorevole e bassa risoluzione spaziale ; inoltre , le misure ripetute a b crescenti allungano i tempi di acquisizione con problemi di ripetibilit , in particolare in pazienti non completamente collaboranti . altre considerazioni interessanti si possono trovare in un lavoro condotto in modo molto rigoroso [ 18 ] : questi autori hanno provato acquisizioni a vari b , sempre con presenza di un fantoccio contenente due liquidi con valori noti di adc ( naturalmente in questi casi adc = d ) , ovvero acqua ( 2 , 29x10 - 3 mm2 / s ) e acetone ( 3 , 98x10 - 3 mm2 / s ) ; questo al fine di ottenere un parametro di riferimento certo per le misure effettuate . 
essi hanno dimostrato differenze significative fra il fegato normale e quello cirrotico ( tabella 1 ) e fra lesioni epatiche benigne e maligne ; ponendo un valore soglia a 1 , 6x10 - 3 mm2 / s con b massimo < 846 s / mm2 , essi hanno ottenuto una sensibilit del 98% ed una specificit del 80% nel differenziare le lesioni maligne dalle benigne . recentemente stata operata una revisione della materia in modo particolarmente interessante , sia dal punto di vista tecnico che concettuale [ 4 ]  . 
nella maggior parte dei lavori precedenti , i valori di adc venivano misurati in una sola direzione , assumendo implicitamente che , a differenza dellencefalo e del rene , la diffusione a livello epatico fosse isotropica . 
questo studio ha coinvolto 66 pazienti portatori di 52 lesioni focali epatiche cistiche , angiomatose , solide benigne e maligne con diametri compresi fra 1 e 15 cm ( tabella 1 ) ; la valutazione stata estesa anche ai parenchimi normale e s . 
b , c in the single - shot echoplanar diffusion - weighted ( se - epi - dw ) images obtained with b = 0 and 1 , 000 s / mm2 , lesions are identifiable . 
b , c nelle scansioni se - epi - dw ottenute con b = 0 e 1000 s / mm2 le lesioni risultano percepibili . d mappa adc : il valore di adc della lesione di maggiori dimensioni risulta pari a 1 , 50 , 07x10 - 3 mm2 / s . lastly the study showed that malignant lesions ( hcc and metastases ) have the lowest adc values , benign hepatocellular lesions have intermediate adc values whereas angiomas and cysts have the highest adc values . 
lesions with adc between 1 and 2x10 - 3 mm2 / s may be either benign or malignant , with a considerable amount of overlap . this fact tends to invalidate , at least in part , the usefulness of dw images for characterizing focal hepatic lesions if the possibility of differentiating cysts and angiomas is excluded . in fact , hepatic cysts have the highest adc values owing to their fluid content , with unrestricted movement of water molecules , whereas angiomas have high adc values owing to their rich vascular component . to summarize , a number of significant limitations to dw images need to be recognized with reference to the sequences used . the se - epi - ssh has limited spatial resolution and low snr and therefore cannot be used to assess lesions with a diameter less than 1 cseveral studies suggest the possibility that new fast sequences will improve image quality and reduce artefacts associated with echoplanar acquisitions [ 19 ]  . in addition , the use of magnets with a 3t field intensity could improve the signal in diffusion [ 20 ]  . 
moreover , if on the one hand very high b values reduce image quality , then the mid - range values usually used ( 300500 s / mm2 ) lead to cirrotico . 
questi autori dimostrano che non esistono differenze statisticamente significative fra i valori di adc ( del parenchima epatico normale , cirrotico e delle lesioni focali epatiche ) misurati nelle tre direzioni , al contrario di quanto avviene nellencefalo e nel rene . 
pertanto , il fegato ha un pattern di diffusione isotropico , probabilmente per la sua organizzazione strutturale casuale , e non risulta quindi necessaria ladozione di gradienti di diffusione multi - direzionali , ovvero lungo le tre direzioni dello spazio . 
si dimostra inoltre che le misure dei valori di adc sono tanto pi accurate , quanti pi valori di b vengono utilizzati lungo la direzione della selezione dello strato ( quattro valori di b crescenti : 0 , 134 , 267 e 400 s / mm2 )  . 
infine risultato che le lesioni maligne ( hcc e metastasi ) presentano i pi bassi valori di adc , le epatocellulari benigne valori di adc intermedi , mentre angiomi e cisti i valori di adc pi alti . pi precisamente le lesioni con adc superiore a 2x10 - 3 mm2 / s risultano benigne , mentre quelle con valori inferiori a 1x10 - 3 mm2 / s , maligne . 
questo fatto inficia dunque , almeno in parte , lutilit delle immagini dw nella caratterizzazione delle lesioni focali epatiche , se si esclude la possibilit di differenziare cisti ed angiomi . 
le cisti epatiche presentano infatti i pi alti valori di adc per il loro contenuto fluido , the risk of overestimating the values due to inclusion of the perfusion fraction f . 
the interstitial deposit of collagen fibres within the lobule modifies the content and motility of water molecules ; this may be considered the expression of mr diffusion , probably causing a restriction of the movement of water molecules , which is evident by the reduction of adc values with respect to healthy parenchyma . 
the same study also showed a correlation between serum levels of hyaluronic acid ( a marker of hepatic fibrosis ) , the child - pugh classification and adc values . in the retroperitoneum and with regard to the pancreas , epi - dw sequences can be useful in differentiating mucinproducing tumours from other histological types [ 23 . 
alcuni studi suggeriscono la possibilit che le nuove sequenze rapide possano migliorare la qualit dellimmagine e ridurre gli artefatti correlati alle acquisizioni eco - planari [ 19 ] ; inoltre , ladozione di magneti con intensit di campo pari a 3t , potrebbe potenzialmente migliorare il segnale in diffusione [ 20 ]  . 
inoltre , se da un lato valori molto alti di fattore b comportano riduzione della qualit di immagine , i valori medi solitamente utilizzati ( pari a 300500 s / mm2 ) comportano il rischio della sovrastima dei valori per inclusione della frazione di perfusione f . 
tale reperto da ascrivere allaccumulo progressivo di matrice fibrillare extracellulare ( prevalentemente collagene di tipo i e iii ) che caratterizza le epatopatie croniche di qualunque etiologia e che raggiunge il suo massimo grado di espressione nella cirrosi ( epatopatia cronica sclerogena ) , contraddistinta dalla formazione di noduli rigenerativi , circondati da setti fibrotici , che sovvertono larchitettura del parenchima epatico . 
la deposizione interstiziale di fibre collagene nel contesto del lobulo epatico modifica il contenuto e la mobilit delle molecole di acqua , delle quali pu essere considerata espressione la diffusione rm , determinando verosimilmente una restrizione del movimento molecolare dellacqua che si rende evidente con la riduzione dei valori di adc rispetto al parenchima sano . 
la possibilit di quantificare in maniera non invasiva , senza cio il ricorso alla biopsia epatica , il grado di fibrosi , ha spinto recentemente alcuni autori a valutare lutilit dellimaging rm pesato in diffusione nella diagnosi di cirrosi e nella quantificazione della fibrosi epatica nei soggetti affetti da epatopatia cronica e da cirrosi . 
in particolare , si cercato di definire se sia possibile distinguere i vari gradi di fibrosi ed infiammazione nei pazienti con epatite cronica c , acquisendo sequenze dw bh con cinque valori di fattore b crescenti , compresi tra 50 e 250 s / mm2 , applicati lungo i tre assi [ 21 ]  . 
questi autori riferiscono di non aver trovato nessuna correlazione tra i valori di adc e i gradi di fibrosi ed infiammazione / attivit di malattia , determinati istologicamente tramite biopsia epatica , indicando che le modificazioni tissutali indotte dallepatite c non sembrano poter essere quantificate con dwi . 
unfortunately the limited spatial resolution obtained with epi sequences precludes assessment of small masses . therefore , small peripheral mucin - producing tumours ( situated near the peripheral ductal branches ) cannot be visualized . the kidney is a good candidate for dw imaging given the relative hypomotility of water molecules within the organ . recent studies [ 2529 ] report adc values of normal renal parenchyma to be higher than those of other abdominal parenchyma in relation to high blood flow and function of fluid transportation performed by the kidney . the first mean adc value of normal renal parenchyma reported in the literature was 3.54x10 - 3 mm2 / s [ 26 ]  . 
an experimental study on animals assessed the effect of intravenous administration of high - viscosity nonionic contrast material on flow in the renal cortex and medulla , showing that following administration , there is a transitory reduction in adc values both in the cortex and medulla . this is explained by a reduction in perfusion induced by the contrast material itself . 
the study showed an adc value at the upper pole significantly higher than at the central portion using low b values whereas no significant differences were obtained with high b values . this is explained by anisotropic diffusion in that structures in the polar regions are oriented parallel to the gradients whereas in the central portion , they are perpendicular . 
furthermore , there is a greater amount of cortex than medulla in the renal poles , and it should be borne in mind that blood flow in the cortex is about ten times greater than in the medulla . 
high adc values at the poles are therefore justified by the greater perfusion , an effect noted when low b values are used whereas with high b values , that effect is almost entirely eliminated [ 25 ]  . 
in fact , it has already been mentioned that as b increases , the weighting in d increases , and the effects secondary to nondiffusional ivim , such as perfusion , are almost entirely eliminated . it should be borne in mind that the findings presented so far refer to studies published in the last 10 years obtained with different devices ( some commercially available , others dedicated to experimental studies ) and using different examination techniques ( different b values , hydrated and dehydi fibrosi epatica ) , la classificazione di child - pugh ed i valori di adc . in ambito retroperitoneale , per quel che riguarda il pancreas , le epi - dw possono essere utili per differenziare i tumori mucinosi dalle altre variet istologiche [ 23 , 24 ]  . 
usando un fattore di diffusione b massimo pari a 300 s / mm2 , ladc medio del fluido viscoso ( contenuto sia nelle cavit cistiche che nei dotti pancreatici principali ) dei tumori mucinosi risultato sostanzialmente pi basso di quello dei tumori sierosi e del liquido cerebrospinale , ma con valori prossimi a quelli delle pseudocisti pancreatiche . 
tuttavia , dal momento che queste ultime non sono associate alla presenza di materiale viscoso allinterno del wirsung , il calcolo delladc effettuato allinterno della lesione cistica e del dotto principale potrebbe essere utile per differenziare le pseudocisti ( wirsung con segnale relativamente elevato , maggiore della lesione cistica ) dai tumori mucinosi ( wirsung con segnale relativamente ridotto , comunque uguale a quello della lesione cistica )  . 
pertanto piccoli tumori mucinosi periferici ( localizzati in prossimit dei rami duttali periferici ) non possono essere apprezzati . il rene si presta ad essere studiato con limaging in d per lipomobilit relativa alla sede . 
nella letteratura recente sono riportati valori di adc del parenchima renale normale [ 2529 ] superiori a quelli degli altri parenchimi addominali , in relazione allelevato flusso sanguigno e alla funzione di trasporto di fluidi del rene . 
questo dato confermato da altri autori [ 25 ] che hanno misurato i valori di adc al polo superiore , inferiore e in sede mesorenale , utilizzando diversi valori di b , compresi tra 317 e 932 s / mm2 . 
risultato che , a tutti i livelli indagati , utilizzando b elevati si ottengono valori di adc significativamente pi bassi ( 1 , 361 , 51x10 - 3 mm2 / s )  . 
c apparent diffusion coefficient ( adc ) map : adc value measured at the middle portion of the right kidney is 2.290.13x10 - 3 mm2 / s . ( se - epi - dw ) fig . 
questo pu essere spiegato dalla diffusione anisotropica , in quanto nelle regioni polari le strutture renali sono orientate in modo parallelo alla direzione dei gradienti , mentre in regione mesorenale risultano perpendicolari . 
inoltre , a livello dei poli renali esiste prevalenza della corticale rispetto alla midollare e deve essere ricordato che il flusso ematico nella corticale circa 10 volte superiore rispetto a quello nella midollare . 
gli alti valori di adc ai poli sono pertanto giustificati dalla maggior perfusione , effetto che si risente quando si utilizzano valori bassi di fattore b , mentre quando si utilizzano valori di b elevati tale contributo pressoch totalmente eliminato [ 25 ]  . 
infatti gi stato ricordato che allincremento del fattore b , aumenta la pesatura in d e si riducono gli effetti secondari ai cosiddetti ivim non diffusionali , quali la perfusione . importante sottolineare che i dati fin qui riportati fanno riferimento a lavori pubblicati negli ultimi 10 anni ottenuti con differenti apparecchiature ( alcune disponibili in commercio , altre dedicate solo a studi sperimentali ) ed utilizzando tecniche desame diverse ( diversi valori di b , pazienti idratati o disidratati , differente sede di posizionamento della roi )  . 
da sottolineare che , in tale studio , la roi stata posizionata in sede mesorenale a livello della giunzione cortico - midollare e non selettivamente a sede midollare e corticale in quanto , come gi evidenziato da altri autori [ 25 ] , risulta difficile posizionare la roi separatamente nelle due sedi , a causa della scarsa risoluzione spaziale delle epi e della presenza , seppur modesta , di artefatti da movimento . le potenzialit dellimaging in diffusione sono state valutate anche in varie situazioni patologiche , quali le alterazioni della funzione , le infezioni renali , la idro / pionefrosi e le masse tumorali [ 10 , 2532 ]  . nello studio della funzione renale [ 27 , 29 ] si dimostrata una buona correlazione tra i valori di adc e lentit del filtrato glomerulare ( gfr ) [ 29 ]  . 
limaging in diffusione potrebbe pertanto rappresentare un metodo nuovo e non invasivo per valutare linsufficienza renale acuta ( ira ) e cronica ( irc ) , e il parenchima in pazienti con stenosi dellarteria renale ( ras )  . 
nella irc i valori di adc risultano ridotti , rispetto al rene sano , sia nella corticale che nella midollare , a seguito della perdita di nefroni , con conseguente riduzione della mobilit dellacqua . 
si ipotizzato che la riduzione dei valori di adc sia secondaria allischemia renale e alledema intracellulare a cui consegue , a sua volta , la riduzione del movimento delle molecole dacqua . 
d apparent diffusion coefficient ( adc ) map : adc value measured at the level of the hydronephrotic pelvis is 3.140.24x10 - 3 mm2 / s . ( se - epi - dw ) fig . 
d mappa adc : il valore di adc misurato a livello della pelvi idronefrotica pari a 3 , 140 , 24x10 - 3 mm2 / s . the potential of dw imaging has also been assessed in a variety of pathological situations , such as functional alterations , kidney infections , hydro / pyonephrosis and tumours [ 10 , 2532 ]  . 
dw imaging might therefore be a useful noninvasive technique for assessing acute and chronic kidney failure and the parenchyma in patients with renal artery stenosis . adc values in chronic kidney failure are lower than those in the normal kidney , both in the cortex and medulla , owing to loss of nephrons and the consequent reduction in water motility . adc values in acute kidney failure are lower than those in the normal kidney , both in the cortex and medulla , but higher than those measured in chronic kidney failure . 
adc values in renal artery stenosis are lower than those in the normal kidney due to reduction in perfusion , which is particularly evident in perfusione particolarmente evidente a livello corticale [ 25 ]  . altri autori confermano valori di adc significativamente minori sia nel parenchima dei pazienti con insufficienza renale acuta e cronica , che a livello della corticale dei reni con stenosi dellarteria renale [ 28 ]  . 
le flogosi sembrano determinare riduzione dei valori di adc : questo riscontrato sia nei casi di pielonefrite , che di ascesso o cisti renale ascessualizzata [ 10 , 31 ]  . 
another study has confirmed significantly lower adc values both in the parenchyma of patients with acute and chronic kidney failure and in the renal cortex in patients with renal artery stenosis [ 28 ]  . 
in fact , in the pyonephrotic kidney , the collecting system is full of high viscosity and high cellularity purulent material , which produces reduction in diffusion , high dw signal and low adc values . dw imaging may also play a part in the assessment of kidney masses . 
further studies , however , are required to determine the possible differences in adc values between cystic and / or necrotic renal tumours and complex renal cysts . the use of dw sequences for the study of thoracoabdominal districts in paediatric patients is often hindered by motion artefacts secondary to free - breathing acquisitions in the case of uncooperative or sedated patients . 
a recent study examined the abdomen of eight paediatric patients with no clinical / humoural evidence of diffuse disease of the abdominal parenchyma ( se - epi - ssh with b set to 300 , 600 and 800 s / mm2 ) [ 33 ]  . 
values obtained with maximum b value were in line with those reported in the literature in adult patients with sequences acquired in breath hold or with respiratory triggering [ 16 , 18 , 34 ]  . 
if these findings are confirmed by further studies , the possibility of performing dw imaging in paediatric and sedated patients would have significant developments in the multimodal approach to abdominal paediatric disease . 
using a similar sequence to the one described above , a low value of adc was found in neuroblastomas ( 1.1x10 - 3 mm2 / s ) , suggestive of restricted diffusion [ 35 ]  . 
the study justifies this figure by suggesting that cellular barriers in a tissue characterized by significantly high cellular density with a high nucleus / cytoplasm ratio has a limiting effect on water molecule diffusion . 
the study of kidney diseases caused by reflux or stenosis of the pyeloureteral junction might also benefit from dw imaging if the existence of a correlation between parenchymal adc and biohumoural pas . 
sono tuttavia necessari ulteriori studi , per determinare le possibili differenze nei valori di adc tra i tumori renali cistici e / o necrotici e le cisti renali complesse . luso delle sequenze dw per lo studio dei distretti toracoaddominali in pediatria frequentemente gravato da artefatti da movimento secondari ad acquisizioni a respiro libero in caso di pazienti poco collaboranti o sedati . 
i valori ottenuti con b massimo sono risultati sovrapponibili a quelli riportati in letteratura in pazienti adulti con sequenze acquisite a respiro sospeso o con trigger respiratorio [ 16 , 18 , 34 ]  . 
utilizzando una sequenza analoga a quella descritta precedentemente , stato riscontrato un basso valore di adc nei neuroblastomi ( 1 , 1x10 - 3 mm2 / s ) , secondo un quadro di diffusione ristretta [ 35 ]  . 
per giustificare tale dato , gli autori , hanno ipotizzato leffetto limitante , sulla diffusivit protonica , delle barriere cellulari , in un tessuto caratterizzato da una notevole densit cellulare , ad alto rapporto nucleo / citoplasma . 
markedly hyperintense cyst with b = 0 appears isointense to renal parenchyma with increased weighting in diffusion ( b = 500 s / mm2 ) ; had the image been obtained with b = 1 , 000 s / mm2 , the cyst would have had a low signal . 
la cisti , marcatamente iperintensa a b = 0 , risulta isointensa al parenchima renale allaumentare del peso in diffusione ( b = 500 s / mm2 ) ; ove fosse stato acquisito b = 1000 la cisti sarebbe risultata a basso segnale . 
d mappa adc : il valore di adc misurato a livello della cisti 3 , 010 , 16x10 - 3 mm2 / s . fisico , dimostrando un aumento di tale parametro in condizioni di stress fisico , probabilmente in relazione ad un aumento della microcircolazione ( pseudodiffusione ) , oltre che della componente extra - cellulare [ 5 ]  . anche in questo distretto ha suscitato interesse la possibilit di discriminare le lesioni benigne dalle maligne . 
alcuni autori riportano un valore medio di adc significativamente maggiore nelle lesioni benigne ( 1 , 71x10 - 3 mm2 / s ) , rispetto alle maligne ( 1 , 08x10 - 3 mm2 / s ) [ 38 ]  . 
questi risultati sono tuttavia contraddetti da una recente pubblicazione in cui , basandosi su una limitata casistica ( 29 lesioni , di cui 16 benigne e 13 maligne ) , non si riscontrata una significativa differenza tra questi due gruppi ; infatti le lesioni benigne hanno presentato un adc compreso tra 1 e 2 , 9x10 - 3 mm2 / s , mentre le maligne fra 0 , 9 e 2 , 3x10 - 3 mm2 / s [ 41 ]  . 
altri ancora giungono a conclusioni intermedie : in una casistica pi ampia ( 60 lesioni ) , utilizzando b = 1000 s / mm2 , stato rilevato come solo nel caso di lesioni mixomatose il dwi non perrameters of renal function is confirmed [ 28 ]  . musculoskeletal applications in recent years , a number of advanced mr acquisition techniques have been proposed [ 37 ] , including dw imaging sequences , particularly for the study of soft tissue [ 38 ] , bone marrow [ 7 ] and joints ( effusion and cartilage ) [ 6 , 39 ]  . 
b single - shot echoplanar diffusion - weighted ( se - epi - dw ) image obtained with b = 0 s / mm2 : the lesion is moderately hypointense . 
one study [ 38 ] reports a mean adc value significantly higher in benign lesions ( 1.71x10 - 3 mm2 / s ) than in malignant lesions ( 1.08x10 - 3 mm2 / s )  . 
yet another study [ 42 ] came to an intermediate conclusion : based on a larger case series ( 60 lesions ) and using a b value of 1 , 000 s / mm2 , dw imaging was unable to successfully differentiate myxomatous lesions only whereas it was particularly effective in differentiating cartilaginous lesions . 
infine da ricordare , a proposito dellelevato valore di adc delle lesioni benigne , che stato sottolineato come gli alti valori riscontrati negli angiomi dei tessuti molli siano dovuti ad una significativa componente di pseudodiffusione o sloshing effect ( perfusione ovvero ivim non diffusionali ) , prodotta dal flusso ematico allinterno della lesione [ 43 ]  . se la caratterizzazione tumorale non ha offerto finora dati univoci , vi maggiore accordo sullefficacia del dwi nel follow - up post - chemio e radioterapia . 
secondo alcuni studi il dwi sarebbe infatti in grado di caratterizzare i tessuti neoplastici e di differenziare le aree di necrosi ( ad elevato adc ) dai residui tumorali ( a basso adc ) [ 44 , 45 ]  . 
sono stati inoltre riscontrati valori di adc significativamente superiori ( p < 0 , 0019 ) nelledema dei tessuti muscolari perilesionali e negli igromi , rispetto alle recidive tumorali [ 46 ]  . la rm presenta unelevata sensibilit nella valutazione delle alterazioni ossee , che nella maggior parte dei casi determinano una riduzione del segnale nelle sequenze t1 ed un aumento in quelle t2 - pesate ; la specificit della metodica s . 
b - d immagini a b crescenti pari a 300 , 600 , 800 s / mm2 . tipico artefatto da suscettibilit magnetica a livello della bolla gastrica ( punte di freccia bianche )  . 
progressivo calo del segnale degli organi parenchimali allaumentare di b , pi evidente a livello del parenchima renale ( frecce bianche ) , in relazione alla maggior diffusivit protonica . while findings regarding tumour differentiation have not been unequivocal to date , there is greater consensus regarding the effectiveness of dw imaging in postchemotherapy and radiotherapy follow - up . 
studies have shown that dw imaging is capable of characterizing neoplastic tissue and differentiating areas of necrosis ( high adc ) from tumour residue ( low adc ) [ 44 , 45 ]  . 
in addition , significantly higher adc values have been found ( p < 0.0019 ) in the oedema of perilesional muscular tissue and in hygromas than in relapsed tumour [ 46 ]  . mr has high sensitivity in assessment of bone alterations , which in most cases cause a signal decrease in t1 and an increase in t2 although its specificity in distinguishing oedema from inflammation or tumours is low . 
assessment of normal adc values in bone obviously refers to bone marrow , given the absence of diffusion in the compact component of bone . values reported in the literature vary according to intrinsic factors ( yellow marrow has a lower diffusible water component than red marrow ) and technical factors , such as sequences and , above all , b values used . 
i valori riportati in letteratura variano in relazione a fattori intrinseci ( il midollo giallo ha una componente di acqua diffusibile inferiore al midollo rosso ) e a fattori tecnici , come le sequenze utilizzate e soprattutto i valori di b adottati . 
il midollo osseo normale presenta un adc inferiore a 0 , 5x10 - 3 mm2 / s , con valori compresi tra 0 , 15 e 0 , 35x10 - 3 mm2 / s [ 4749 ] ; in particolare il midollo rosso avrebbe un adc superiore rispetto al midollo giallo [ 47 ]  . valori di adc pi elevati sono stati rilevati da nonomura et al . 
che hanno valutato il midollo a livello della cresta iliaca , distinguendo tre gradi di normalit midollare : ipocellulare ( 0 , 31 mm2 / s ) , normocellulare ( 0 , 82 mm2 / s ) e ipercellulare ( 1 , 29 mm2 / s ) , questultimo presente nei bambini [ 7 ]  . 
a turbo spin echo ( tse ) t2 - weighted axial image showing moderately hyperintense homogenous mass ( white arrows ) originating from the posterior mediastinum ; some axillary lymphonodal packets are also present ( black arrowheads )  . 
b single - shot echoplanar diffusion - weighted ( se - epi - dw ) sequence with fat signal suppresion and b = 0 ( tr 6 , 890 , te 95 , epi factor 88 ) confirms the presence of the formation described and the right axillary lymphonodal packet ; both appear with elevated signal intensity . 
c with the application of a diffusion gradient of 800 s / mm2 , there is a significant loss of axillary lymph node signal but not of the mediastinal mass , which maintains high signal intensity . 
d apparent diffusion coefficient ( adc ) map : high lymph node signal as a consequence of high diffusion ( ) at that level , most likely due to colliquative phenomena . 
a immagine tse t2 sul piano assiale che mostra una massa omogenea e modicamente iperintensa ( frecce bianche ) che origina dal mediastino posteriore ; sono presenti anche dei pacchetti linfonodali ascellari ( punte di freccia nere )  . 
b la sequenza seepi - dw con soppressione del grasso a b = 0 ( tr 6890 , te 95 , epi factor 88 ) conferma la presenza della formazione descritta e del pacchetto linfonodale ascellare destro ; entrambe appaiono ad elevata intensit di segnale . 
c con lapplicazione di un gradiente di diffusione di 800 s / mm2 si ottiene una notevole perdita di segnale dei linfonodi ascellari , ma non della massa mediastinica che mantiene elevata intensit di segnale . 
 [ 7 ] , who assessed marrow at the level of the iliac crest , distinguishing three degrees of marrow normality : hypocellular ( 0.31x10 - 3 mm2 / s ) , normocellular ( 0.82x10 - 3 mm2 / s ) and hypercellular ( 1.29x10 - 3 mm2 / s ) , the last of which was measured in paediatric patients . 
su questo presupposto si basata la valutazione con dwi dei crolli vertebrali , nel tentativo di distinguere quelli su base osteoporotica da quelli secondari , soprattutto qualora sia presente edema dellintero soma e / o dei peduncoli vertebrali [ 51 ]  . 
acquisition of single - shot echoplanar diffusion - weighted ( se - epi - dw ) images using orthogonal diffusion gradients oriented along the anteroposterior axis ( ap , corresponding to the phase code ) , laterolateral ( ll , corresponding to the read code ) and craniocaudal ( crc , corresponding to the slice selection ) direction , respectively . 
axial dw slice image , obtained along the longitudinal axis of the soleus muscle and the lateral belly of the triceps sura , shows greater hypointensity ( white arrowhead ) than shown by dw images acquired along the other two directions in space . 
acquisizione di immagini se - epi - dw utilizzando gradienti di diffusione orientati rispettivamente lungo lasse antero - posteriore ( ap , corrispondente alla codifica di fase : phase ) , latero - laterale ( ll , corrispondente alla codifica di lettura : read ) e lungo la direzione cranio - caudale ( crc , corrispondente alla selezione di strato : slice ) , tra loro ortogonali . 
this is the basis for using dw imaging to assess vertebral collapse in the attempt to distinguish those due to osteoporosis and those secondary in nature , especially when oedema is present in the entire vertebral body and / or peduncles [ 51 ]  . 
when assessed with the same sequence , vertebral collapse due to osteoporosis tends to have a hypointense signal in dw sequences ( i.e. high diffusion high adc ) while vertebral collapse due to metastasis has a hyperintense signal in dw ( low diffusion low adc ) [ 53 ]  . 
il crollo vertebrale su base osteoporotica tende inoltre , se valutato con la stessa sequenza , a presentare ipointensit di segnale nelle sequenze dw ( ossia elevata diffusione alto adc ) , mentre il cedimento vertebrale secondario a metastasi presenta iperintensit di segnale nelle dw ( bassa diffusione basso adc ) [ 53 ]  . 
ricordando che le sequenze se - epi - ssh permettono di quantificare ladc , nelle casistiche con b sovrapponibili e tendenzialmente elevati ( 8801000 s / mm2 ) , tale valore varia tra 1 , 61 e 1 , 94 nei crolli osteoporotici e tra 0 , 69 e 0 , 82x10 - 3 mm2 / s in quelli su base sostitutiva [ 49 , 54 ]  . infine , castillo et al . 
riportano dati contraddittori rispetto a quanto fin qui descritto [ 55 ] , anche se in tale studio erano presenti ben 9 / 15 mestastasi sclerotiche note , nelle quali la scarsa presenza di protoni diffusibili determina un basso segnale sia nellimmagine di riferimento ( b = 0 ) che nellimmagine dw ; il rischio di falsi negativi nelle lesioni ripetitive osteosclerotiche stato riportato anche da altri autori [ 49 ]  . 
a single - shot echoplanar diffusion - weighted ( se - epi - dw ) image with fat signal suppression in the sagittal plane with b = 0 s / mm2 . 
 [ 55 ] , however , report findings contradictory to the above even though in the study there were as many as 9 / 15 known sclerotic metastases , in which the limited presence of diffusible water molecules produces a low signal in both reference images ( b = 0 ) and dw images . 
it should also be borne in mind that this limitation is , in part , linked to the use of sequences in the studies mentioned that do not enable calculation of adc . we have already noted that adc of bone marrow may vary in healthy subjects on the basis of the degree of adipose involution . 
this would justify the higher adc value in haematopoietic marrow in the paediatric population , particularly those under 5 years of age , when both axial and appendicular skeletons ( with the exception of phalanxes ) are hypercellular [ 56 ]  . 
dw imaging is able to distinguish those different characteristics of the marrow [ 7 ] since areas of high cellularity have a higher adc value than hypocellular areas . abbiamo gi accennato in precedenza a come ladc midollare possa variare nei soggetti sani in funzione del grado di involuzione adiposa ; tale dato giustificherebbe il valore pi alto di questo indice nel midollo ematopioetico e nella popolazione infantile , in special modo al di sotto dei 5 anni , quando sia lo scheletro assile che quello appendicolare ( ad eccezione delle falangi ) ipercellulare [ 56 ]  . 
in particolare stato dimostrato come non vi sia una significativa differenza di adc tra il normale midollo ipercellulare e quello con ipercellularit secondaria ad infiltrazione linfomatosa , mentre tale differenza significativa tra il midollo ipocellulare , quello normocellulare e lipercellulare emopoietico [ 7 ]  . 
d mappa adc : larea edematosa presenta adc superiore a quello del circostante midollo osseo . it has been shown that there is no significant difference in adc between normal hypercellular marrow and marrow with hypercellularity resulting from lymphomatous infiltration while the difference is significant between hypocellular marrow , hypercellular haematopoietic marrow [ 7 ]  . 
tali valori sono in linea con quanto riportato da baur [ 11 ] : utilizzando b di 750 s / mm2 , vengono riferiti valori di adc pari a circa 1 , 37 e 0 , 95x10 - 3 mm2 / s in caso di edema midollare e metastasi , rispettivamente . 
a in the single - shot echoplanar ( se ) t1 - weighted image at the time of diagnosis , an extensive area of bone marrow hypointensity at the level of the posterior portion of the ankle is evident ( black arrowhead )  . 
b single - shot echoplanar diffusion - weighted ( se - epi - dw ) image obtained with b = 300 s / mm2 : diffuse medullary hyperintensity ( white arrowheads )  . 
a nella se t1 pesata al momento della diagnosi evidente una estesa area di ipointensit della midollare ossea a livello della porzione posteriore del calcagno ( punte di freccia nere )  . 
there have been no clinical studies regarding the use of dw imaging in bone tumours , with the exception of the above - mentioned work on vertebral metastasis and the relatively few studies regarding lymphomatous infiltration . 
however , thanks to a number of experimental studies , including the above - mentioned study by lang et al . [ 44 ] , we know that adc can be a sensitive indicator of the response of those tumours to treatment ( given the progressive increase in adc in the necrotic component )  . 
in a study performed on patients affected by vertebral metastasis and in a time interval ranging from 1 to 6 months following radioallutilizzo del dwi nelle neoplasie ossee , ad eccezione di quanto gi riportato a proposito delle metastasi vertebrali e dei pochi lavori sulla valutazione dellinfiltrazione linfomatosa . 
 [ 44 ] , sappiamo tuttavia che ladc pu essere un sensibile indicatore della risposta di tali neoplasie ai trattamenti ( dato il progressivo aumento delladc della componente necrotica )  . 
in uno studio condotto su pazienti affetti da metastasi vertebrali , in un intervallo di tempo compreso tra 1 e 6 mesi dopo terapia radiante , gli autori [ 58 ] hanno riscontrato , sulle immagini dw , una iperintensit di segnale delle metastasi nella valutazione pre - terapeutica , in relazione ai bassi valori di adc delle lesioni ripetitive ( 0 , 78x10 - 3 mm2 / s )  . 
nelle successive indagini in corso di terapia si evidenziata progressiva perdita di segnale , per laumento di diffusivit causato dallincremento dellacqua extra - cellulare e dalla diminuzione della componente cellus . 
 [ 58 ] found in dw images a hyperintense signal of the metastasis in the pretreatment assessment in relation to the low adc values of repetitive lesions ( 0.78x10 - 3 mm2 / s )  . 
examinations performed during therapy revealed progressive loss of signal owing to the increase in diffusivity caused by the increase in extracellular water and the decrease in the cellular component ( 1.22x10 - 3 mm2 / s )  . these changes first appeared 1 month after the beginning of therapy , which , if confirmed , would place dw imaging at a distinct advantage over bone scintigraphy , which cannot be performed prior to 6 months due to the false hyperfixation produced in that period by bone repair . 
in the same way , using a b value of 1 , 000 s / mm2 , an adc value was shown at the peak effectiveness of treatment to be about three times higher than the value when treatment began [ 59 ]  . cartilaginous structures have the potential to be well assessed by dw imaging thanks to their high water content [ 39 ]  . 
however , only in recent years and thanks to the development of new acquisition techniques have targeted studies been performed in this respect . the technical limitation regards the short t2 of cartilage , which necessitates dw sequences with a relatively low te and appropriate spatial resolution . 
in this sense , the se - epissh sequences , despite having a very short te , are unable to provide high resolution images while ssfp sequences , as stated above , have the disadvantage of not enabling the calculation of adc . 
the patellar cartilage showed a progressive reduction in signal intensity with an increasing b value while the signal for synovial fluid was totally absent due to high diffusion [ 61 ]  . 
this finding appears to vary in relation to the nature of the effusion : a significant difference between adc of effusion of a degenerative and inflammatory nature was found ( 2.4x10 - 3 mm2 / s and 3.1x10 - 3 mm2 / s , respectively ) [ 6 ]  . the authors of the study explain this finding as the result of hyaluronidase activity present in inflammatory forms , which causes reduction in hyaluronic acid concentration , with a consequent decrease in viscosity . the dependence of dw images on diffusivity of water molecules and the possibility of quantifying their movement therefore hold great promise for increasing the global ability of mr to distinguish benign from malignant lesions . 
in some cases , as in assessment of vertebral fractures and follow - up of soft tissue tumours or lymphomas undergoing adjuvant treatment , a large number of studies have been published , and the preliminary results obtained to date appear encouraging . 
work done to date regarding use of dw imaging to asses cartilage , although limited to in vitro studies , seems to offer developments in the near future in line with technological progress in hardware ( coils with a higher snr ) and software ( new sequences ) in response to clinical and therapeutic needs of increasingly molecular imaging techniques . nonetheless , an increase in spatial resolution will be relare ( 1 , 22x10 - 3 mm2 / s )  . 
tali modificazioni sono comparse un mese dopo linizio della terapia e questo rappresenterebbe , se confermato da altri studi , un vantaggio rispetto alla scintigrafia ossea , che non pu essere eseguita prima di 6 mesi a causa della falsa ipercaptazione prodotta in tale periodo dallattivit osteoriparativa . 
allo stesso modo , si dimostrato , utilizzando b = 1000 s / mm2 , un aumento delladc di circa 3 volte rispetto al valore di partenza nella fase di massima efficacia terapeutica [ 59 ]  . le strutture cartilaginee sono potenzialmente ben valutabili con dwi , a causa del loro contenuto idrico [ 39 ] : alcuni autori hanno stabilito una correlazione tra la perdita di proteoglicani che avviene nei processi degenerativi e laumento delladc cartilagineo [ 60 ]  . 
in questo senso le sequenze se - epi - ssh , pur con te brevissimo , non consentono immagini ad elevata risoluzione , mentre quelle ssfp presentano , come accennato in precedenza , lo svantaggio di non permettere il calcolo delladc . 
stata recentemente utilizzata una sequenza steady - state dw a cui stato applicato un eco - navigatore per ridurre gli artefatti da movimento ed aumentare la risoluzione spaziale : la cartilagine rotulea ha presentato progressiva riduzione dellintensit di segnale allaumentare del valore di b , mentre il liquido sinoviale risultato completamente privo di segnale per lelevata diffusione [ 61 ]  . 
tale reperto sembra variare in relazione alla natura del versamento : stata riscontrata una significativa differenza tra adc dei versamenti di natura degenerativa ed infiammatoria ( rispettivamente 2 , 4x10 - 3 mm2 / s e 3 , 1x10 - 3 mm2 / s ) [ 6 ]  . 
questo dato stato spiegato dagli autori come il prodotto dellattivit della ialuronidasi presente nelle forme infiammatorie , che determina una riduzione della concentrazione dellacido ialuronico con conseguente decremento della viscosit . la dipendenza dellimmagine dw dalla diffusivit dei protoni dellacqua e la possibilit di quantificarne il movimento risulta quindi molto promettente nellaumentare la capacit globale della rm nel distinguere le lesioni benigne da quelle maligne . in alcuni casi , come nella valutazione delle fratture vertebrali e nel follow - up delle neoplasie dei tessuti molli o dei linfomi in corso di terapia adiuvante , la letteratura offre unampia casistica ed i risultati preliminari ottenuti ad oggi sembrano incoraggianti . 
quanto riportato nella valutazione con dwi delle cartilagini , sebbene limitato a studi in vitro , sembra poter avere sviluppo nel prossimo futuro parallelamente ai progressi tecnologici sia nel campo del hardware ( bobine di quadratura a pi elevato s / r ) che del software ( nuove sequenze ) , rispondendo alle esigenze cliniche e terapeutiche di un imaging sempre pi molecolare . 
sar comunque necessario aumentare la risoluzione spaziale ed eliminare linfluenza del flusso capillare sulla genesi del segnale di diffusione , in modo da poter stabilire valori di adc quired along with elimination of the effects of capillary flow on the genesis of the diffusion signal to establish reliable adc values that are reproducible in the various districts and individual pathologies . 
dw sequences also need to be validated on a broad number of cases in an attempt to define sequences and b values that guarantee optimal results in the musculoskeletal district . recently , a number of studies were performed on animals using a diffusion sequence with steady - state sequential acquisitions known as line scan , both before and after induction of femoral ischaemia [ 62 ]  . 
the study showed a variation of adc values in the epiphysis characterized by an initial reduction ( 26% in the first 3 h ) followed by progressive increase ( + 27% after 5 h ; + 75% after 96 h )  . 
these findings are suggestive of early cytotoxic oedema , which would justify the initial restricted diffusion and consequent cellular lysis , which , in contrast , would tend to increase water molecule diffusion . these findings may have a significant impact in paediatrics regarding treatment of legg - calv - perthes disease , in which knowledge of the extension of ischaemia and its duration is vital for establishing the most appropriate treatment . the results seem to confirm anecdotal evidence : medullary oedema with a mean adc of 1.22x10 - 3 mm2 / s compared with a normal value of 0.56x10 - 3 mm2 / s [ 50 ]  . 
however , dw imaging does not appear to be able to differentiate between an increase in adc present in inflammatory foci and an increase due to medullary oedema and osteochondritis [ 63 ]  . 
appare necessaria la validazione delle sequenze dw su pi ampie casistiche , nel tentativo di definire le sequenze ed i valori di b che garantiscano i migliori risultati nel distretto muscolo - scheletrico . recentemente sono stati condotti alcuni studi su animali , utilizzando una sequenza di diffusione ad acquisizioni sequenziali in steady - state , nota come line - scan , prima e dopo induzione di ischemia femorale [ 62 ]  . 
gli autori hanno riscontrato nellepifisi una variazione dei valori di adc caratterizzata da una iniziale diminuzione ( 26% nelle prime 3 ore ) , seguita da un progressivo aumento ( + 27% dopo 6 ore , + 75% dopo 96 ore ) , tali risultati sono stati posti in relazione ad un precoce edema citotossico , che giustificherebbe la iniziale diffusione ristretta , e ad una successiva lisi cellulare , che , al contrario , determinerebbe laumento della diffusivit protonica . questi risultati potrebbero avere un significativo impatto in pediatria , sul trattamento della malattia di legg - calvperthes , nella quale importante conoscere lestensione dellischemia e la sua durata , al fine di stabilire la terapia pi appropriata . 
questi risultati sembrano confermati , ad ora , da riscontri aneddotici : edema midollare con adc medio di 1 , 22x10 - 3 mm2 / s , rispetto a valori di normalit di 0 , 56x10 - 3 mm2 / s [ 50 ]  . 
un aumento della diffusione rilevabile anche nelle osteomieliti , a causa verosimilmente delliperemia , dellaumento dello spazio extracellulare e della presenza di foci necrotici ; non sembra tuttavia che il dwi permetta di differenziare laumento delladc presente nei focolai flogistici da quello delledema midollare e delle osteocondriti [ 63 ]  . 
orsola malpighi , azienda ospedaliero - universitaria di bologna , via massarenti 9 , i - 40138 bologna , italy 2servizio sanit pubblica , direzione generale sanit e politiche sociali , regione emilia - romagna , via a . 
the italian decree of law 187 / 2000 provides for many fulfilments relevant to justification and optimisation of medical exposures that can complicate the daily work of radiology departments if considered as mere legal requirements . 
to this end , the emiliaromagna region carried out an initial assessment of medical exposures to its population in 2001 followed by a second survey taking into account new dosimetric evaluations . 
study of distribution of the entrance skin dose for different examinations in single hospitals showed no systematic differences in kilovoltage settings versus dose whereas the number of examinations tended to be inversely proportional to dose . 
these trends could be explained by the fact that in hospitals where many examinations of the same type are performed , operators , equipment and procedures are well integrated , leading to a level of specialisation that allows efficient interaction in order to deliver an optimal dose . 
the evaluations performed in this study show that this type of analysis heavily relies not only on the cooperation of all professionals responsible for patient radiation protection but riassunto obiettivo . 
il decreto legislativo 187 / 2000 prevede numerosi adempimenti relativi alla giustificazione ed alla ottimizzazione delle esposizioni mediche che , se vissuti come meri obblighi di legge , possono appesantire il lavoro quotidiano delle unit operative di radiologia . 
al contrario , la normativa dovrebbe essere unutile occasione per analizzare ed ottimizzare le modalit operative adottate : in questa ottica la regione emilia - romagna ha effettuato nel 2001 una prima valutazione di dose alla popolazione regionale dovuta alle esposizioni a scopo medico e , successivamente , una seconda raccolta dati che tenesse conto delle nuove valutazioni dosimetriche eseguite . 
si sono innanzitutto definite le tipologie di esame che si volevano prendere in considerazione : in radiodiagnostica convenzionale e tomografia computerizzata si sono identificati dodici differenti esami distinti in macroaggregati e facilmente identificabili . 
nello studio delle distribuzioni delle dosi di ingresso per i vari esami nelle singole aziende sanitarie in generale non si evidenziano differenze sistematiche dei kv impostati in funzione della dose , mentre si pu notare che il numero di prestazioni eseguite tende ad essere inversamente proporzionale alla dose erogata . 
questi andamenti potrebbero essere spiegati con il fatto che , laddove si eseguono molti esami appartenenti ad una medesima tipologia , gli operatori , le apparecchiature e le procedure sono ben integrati tra di loro e raggiungono una specializzazione che permette di interagire in maniera ideale per erogare una dose ottimale . 
le valutazioni effettuate dimostrano che in questa tipologia di analisi sono fondamentali sia la collaborazione tra tutte le figure professionali che si occupano della radioprotezione del paziente sia lesperienza maturata nel corso delle varie campagne di raccolta dati , in quanto la fase di censimento dei dati molto delicata e pu inficiare , se non condotta accuratamente , tutte le elaborazioni posteriori . parole chiave dosimetria misura esposizione radioprotezione paziente introduction introduzione by supplying regulatory tools to verify whether the principles of justification and optimisation are effectively implemented in clinical practice , decree of law no . 
in this context , studies investigating the doses delivered to patients , clearly in conjunction with analysis of image quality , are becoming increasingly important at both the national [ 25 ] and international level [ 610 ]  . it is therefore hoped that the many requirements provided for by this decree will not merely be seen as legal duties but as an opportunity to analyse , or reanalyse , our working practices : in particular , article 12 of the decree requires that regions carry out assessments of medical exposures as regards the regions population and specific reference groups in the region , that such assessments be carried out periodically and that the results be sent to the ministry of health . 
187 / 2000 richiede che le regioni provvedano a valutare le esposizioni a scopo medico con riguardo alla popolazione regionale e a gruppi di riferimento della stessa e che tale valutazione sia effettuata periodicamente ed inviata al ministero della salute . 
per ottemperare al citato obbligo di legge la regione emilia - romagna ha effettuato una prima valutazione di dose nel 2001 , relativa allanno 2000 [ 11 ] e , anche se non espressamente richiesto dalla legislazione , ha effettuato una nuova raccolta dei dati relativa allanno 2002 , sfruttando il fatto che entro il 31 / 12 / 2002 i responsabili degli impianti radiologici avvalendosi degli esperti in fisica medica dovevano verificare il rispetto dei livelli diagnostici di riferimento ( ldr ) e quindi potessero rendere disponibili dati dosimetrici pi attendibili . 
in questo lavoro sono illustrati i risultati di questa seconda raccolta dati , per evidenziare la variabilit che si pu riscontrare tra le dosi correlate ad esami di radiologia diagnostica anche in una regione come lemilia - romagna , in cui il livello quali - quantitativo delle prestazioni sanitarie erogate si presenta omogeneo a livello territoriale ; sono stati inoltre effettuati un confronto ed una analisi dei dati raccolti rispetto a quanto riscontrato in analoghe indagini riportate in letteratura . materials and methods the first pitfall in analysing the radiation dose imparted by the various imaging procedures is of a lexical nature and related to the possible ambiguity of terms such as radiological examination of the head , chest , spine , etc : even european un primo rischio che si presenta nellaffrontare la problematica delle dosi da radiazioni ionizzanti impartite nelle varie prestazioni diagnostiche di tipo lessicale e consiste nel riscontramateriali e metodi g . 
the first problem when planning our dose survey among the 19 emilia - romagna region hospitals was therefore to specify the types of examinations we intended to consider . as regards conventional radiology and computed tomography ( ct ) , we selected 12 easily identifiable examinations divided into macroaggregates , which are shown in the first column of table 1 . 
the survey on the number of examinations was carried out by asking each hospital for their list of examinations divided by type and grouped by the ministry of health nomenclature code : examination types and codes are shown in the second column of table 1 . if incomplete , data provided by a given hospital were extrapolated and completed on the basis of means or proportions derived from the other hospitals . 
with regard to private healthcare facilities under contract with the regional health system , we extrapolated frequencies of ambulatory services from data of the regional specialised ambulatory healthcare . as concerns dosimetry , considering that all radiological equipment undergoes regular quality control tests as part of quality assurance programmes implemented by equipment holders and medical physics experts , each hospital was asked to provide , for each of the examinations in table 1 , some technical parameters related to both the examination protocol and the equipment . the hospitals were also invited to supply the numerical value of dosimetric measurements made by the medical physics experts : entrance skin dose ( esd ) for conventional and paediatric imaging , ct dose index ( ctdi ) and doselength product ( dlp ) for ct . in particular , they were asked to supply the mean of these values as measured on all x - ray tubes performing a given examination , weighted for the number of exams performed on each equipment . 
il primo problema che si dovuto affrontare quando si pianificata la rilevazione delle dosi nelle 19 aziende sanitarie dellemilia - romagna ( as ) stato quindi specificare quali erano le tipologie di esame che si volevano prendere in considerazione . 
per quanto riguarda la radiodiagnostica convenzionale e la tomografia computerizzata ( tc ) si sono identificati dodici differenti esami distinti in macroaggregati e facilmente identificabili , che sono riportati nella prima colonna della tabella 1 . 
la raccolta dei dati relativi al numero di prestazioni stata effettuata richiedendo direttamente alle as il dettaglio del numero di esami suddivisi per tipologia e raggruppati per codice del nomenclatore ministeriale : tali tipologie e codici sono riportati nella seconda colonna della tabella 1 . 
i dati forniti da una determinata as , qualora siano risultati incompleti , sono stati estrapolati e completati in base a medie o a proporzioni effettuate sui dati delle altre as . 
relativamente alle strutture sanitarie che operano in regime di convenzione con il servizio sanitario regionale , si sono ottenute le frequenze delle prestazioni ambulatoriali tramite unestrapolazione della banca dati dellassistenza specialistica ambulatoriale regionale . 
per quanto attiene al discorso pi propriamente dosimetrico , premesso che regolari controlli di qualit sulle apparecchiature radiologiche vengono eseguiti allinterno dei programmi di garanzia della qualit predisposti dai responsabili degli impianti radiologici congiuntamente con gli esperti in fisica medica , ad ognuna delle as sono stati richiesti , per gli stessi esami descritti nella tabella 1 , alcuni parametri tecnici relativi sia al protocollo di esecuzione dellesame sia allapparecchiatura . 
le as sono state altres invitate a fornire il valore numerico delle grandezze dosimetriche misurate dagli esperti in fisica medica : dose di ingresso ( entrance skin dose , esd ) per la radiodiagnostica convenzionale e pediatrica , indice di dose tc ( computed tomography dose index , ctdi ) e prodotto dose - lunghezza ( dose - length product , dlp ) per la tc . 
in particolare , stata richiesta la media di queste grandezze effettuata su tutti i tubi radiogeni che eseguivano un dato esame , pesata in base al numero di esami effettuati su ogni apparecchiatura . 
ad esempio , la grandezza esdaddome relativa allesame addome in radiodiagnostica convenzionale stata calcolata per ogni as in base alla formula : esdaddome = n i = 1 ( ni / p ) ( esdaddome ) i dove : n = numero di tutte le apparecchiature radiologiche di quella as su cui viene eseguito lesame addome ; ni = numero di prestazioni ( cio di esami addome ) eseguite con lapparecchiatura radiologica i - esima ; ( esdaddome ) i = esd valutata ai sensi dellart . 
figures 1 and 2 show , for the various examinations , esd distributions ( in adult conventional radiology ) among single hospitals , versus a significant technical parameter ( kvp ) and the number of procedures performed , respectively . 
it should be noted that in both figures data are shown in increasing order of esd so that the order of the hospitals changes in each figure and is not the same as that shown in the tables . 
lordine da 1 a 19 il medesimo per entrambe le tabelle ed stato attribuito casualmente alle singole as . nelle figure 1 e 2 sono mostrate , per i vari esami , le distribuzioni delle esd ( nella radiologia convenzionale adulti ) tra le singole as in relazione , rispettivamente , a un parametro tecnico significativo ( kv impostati ) ed al numero di prestazioni eseguite . 
si fa notare che in entrambe le figure i dati sono sempre stati ordinati per esd crescente e quindi lordine delle singole as varia in ogni grafico e non lo stesso di quello riportato nelle tabelle . nella tabella 4 , infine , sono mostrati i rapporti esdmassima / esdminima per le varie proiezioni e tra le varie as , confrontandoli con valori di letteratura [ 13 , 14 ]  . discussion discussione data collected lend themselves to different possible analyses and interpretations , but two aspects will be discussed here : the first is related to the characteristics of each hospital and the second concerns the variability of examinations among all hospitals . to analyse the first aspect , figure 1 shows , for the various examinations , esd distributions in single hospitals in relation to a significant technical parameter ( kvp )  . 
to see if there is a more significant variable influencing esds , figure 2 shows , for the various examinations , esd distributions in single hospitals in relation to the number of examinations performed . 
it can be noted that the number of examinations tends to be inversely related to esd ( in other words , the dose imparted in a given examination tends to be lower in hospitals performing many examinations of the same type )  . 
this could be accounted for by the fact that where many examinations of the same type are performed , there is excellent integration among radiologists , equipment and procedures , enabling a level of specialisation that allows delivery of an optimal dose , that is , a dose which , associated with a correctly optimised and justified radiological procedure [ 15 ] , is the lowest possible dose compatible with a good quality image . 
this statement is consistent with the concept of clinical competence , whereby quantity may help attain a greater competence : the statistical significance of this trend will be studied more in depth when we have all data from our next survey , which are expected to be collected more accurately by single hospitals . as regards variability of examinations among all hospitals , table 4 illustrates the esdmax / esdmin ratio . 
because all hospitals perform the same examinations , we coni dati che sono stati raccolti si prestano a diverse possibili analisi ed interpretazioni : in questa sede verranno discussi essenzialmente due aspetti , il primo pi legato alle caratteristiche della singola as , il secondo riguardante la variabilit degli esami tra tutte le as . per analizzare il primo aspetto , nella figura 1 sono mostrate per i vari esami le distribuzioni delle esd nelle singole as in relazione a un parametro tecnico significativo ( kv impostati ) : come si pu notare dai vari grafici , in generale non si evidenziano differenze sistematiche di questo parametro tra le diverse realt della regione in funzione della dose . 
per vedere se esiste una variabile pi significativa nellinfluenzare le dosi in ingresso , nella figura 2 sono state riportate , per i vari esami , le distribuzioni delle esd nelle singole as in relazione al numero di prestazioni eseguite : in questo caso si pu notare che il numero di prestazioni tende ad essere inversamente proporzionale alla esd erogata ( cio la dose per un dato esame tende ad essere pi bassa nelle as in cui vengono effettuati molti esami di quel tipo )  . 
questi andamenti potrebbero essere spiegati con il fatto che , laddove si eseguono molti esami appartenenti ad una medesima tipologia , gli operatori , le apparecchiature e le procedure sono ben integrati tra di loro e raggiungono una specializzazione che permette di interagire in maniera ideale per erogare una dose ottimale , intesa come quella dose che , associata ad una procedura radiologica correttamente ottimizzata e giustificata [ 15 ] , risulta la pi bassa possibile e fornisce unimmagine di buona qualit . 
questa affermazione risulta peraltro coerente con il concetto di competenza clinica , secondo il quale la quantit pu aiutare a raggiungere una maggiore competenza : la significativit statistica di questo andamento verr studiata in maniera pi approfondita quando si avranno a disposizione i dati relativi alla successiva indagine , che dovrebbero essere raccolti in maniera pi accurata dalle singole as . per quanto riguarda la variabilit degli esami considerati tra tutte le as , nella tabella 4 si esamina il parametro rapporto esdmassima / esdminima : questo un indicatore gi utilizzato in letteratura [ 13 , 14 ] per valutare lampiezza delle differenze tra diverse strutture di radiologia . 
2 distribuzioni delle dosi in ingresso ( esd ) tra le singole aziende sanitarie regionali ( as ) in relazione al numero di prestazioni eseguite per i vari esami . sidered correct to analyse those with the lowest and highest esd values . the esdmax / esdmin ratios obtained for the various projections and hospitals were compared with those reported in the literature : in urography and abdomen examinations these ratios were found to be similar to those previously reported for a large italian hospital [ 13 ] , which has more than one radiology department and where one would expect ratios to be lower as a result of greater uniformity among departments . 
in the chest lat ( lateral ) , lumbar spine ap ( anteroposterior ) , pelvis ap , skull ap / pa ( posteroanterior ) and skull lat projections , ratios observed in the present study were almost double those reported in the italian study [ 13 ] ; in the chest pa , lumbar spine lat and lumbosacral spine views , ratios obtained in this study were definitely higher . 
the cause of this greater dispersion could be a physiological scale factor in that , as stated above , it is natural there are greater differences in clinical protocols and radiological equipment among hospitals of a region than there are within a single hospital , and it is just as natural that these differences will be reflected in broader esd ranges . 
 [ 14 ] for lumbar spine ap , pelvis ap , skull ap / pa , skull lat and abdomen views but highi rapporti esdmassima / esdminima ottenuti in questo studio per le varie proiezioni e tra le varie as sono confrontati con quelli riportati in letteratura : si nota che , negli esami urografia e addome , questi rapporti sono dello stesso ordine di grandezza di quanto riscontrato in uno studio italiano in un grande ospedale [ 13 ] dove sono presenti pi unit operative di radiologia e dove ci si aspetta effettivamente che tali rapporti siano minori , in quanto dovrebbe esserci pi uniformit tra le varie unit operative ; nelle proiezioni torace lat , rachide lombare ap , pelvi ap , cranio ap / pa e cranio lat i rapporti riscontrati nel presente lavoro sono circa il doppio di quanto riportato nello studio italiano [ 13 ] ; nelle proiezioni torace pa , rachide lombare lat e rachide lombosacrale , infine , i rapporti riscontrati in questo lavoro sono decisamente pi elevati rispetto allo studio italiano citato . la causa di questa maggiore dispersione potrebbe risiedere in un fisiologico fattore di scala , in quanto , come sopra accennato , inevitabile che allinterno di una regione siano presenti , rispetto a quanto avviene in un ospedale seppure grande , maggiori differenze nei protocolli clinici e nelle apparecchiature radiologiche tra le diverse as ed altrettanto inevitabile che queste differenze si riflettano in pi ampi intervalli di esd . 
per verificare se questa ipotesi di un fattore di scala potesse essere considerata valida , si esteso il confronto ad un altro studio effettuato su una dimensione a scala nazionale [ 14 ] : in effetti si riscontrato , come riportato nella tabella 4 , che nelle proiezioni rachide lombare ap , pelvi ap , cranio ap / pa , cranio lat e addome i rapporti esdmassima / esdminima sono inferiori a quanto riportato nello studio della realt nazionale , mentre nelle proiezioni torace lat , torace pa e rachide lombare lat i rapporti riscontrati nel nostro studio sono superiog . 
this finding might have been expected , as it is known [ 16 ] that the chest is a physically complex radiographic object , partly in view of the many different diseases that may affect it , and that therefore there may be many differences in clinical protocols even in a relatively uniform territory such as our region . 
although the esds imparted by single chest examinations are low , widespread use of this examination ( in terms of number of examinations , it accounts for approximately 50% of all conventional radiography studies ) urgently calls for its homogenisation and optimisation . 
questi confronti , pur con tutti i limiti connessi ad una analisi semi - quantitativa come quella qui presentata , sembrano dimostrare che il fattore di scala abbia comunque un ruolo fondamentale nella variabilit dei valori di esd tra le varie as e che soprattutto lesame torace quello pi critico , nel senso che presenta le maggiori differenze nelle esd . 
questo risultato del resto era abbastanza prevedibile in quanto ben noto [ 16 ] che il torace un oggetto radiografico fisicamente complesso anche per le molte e diverse patologie che possono riscontrarsi e quindi possono essere presenti molte differenze a livello di protocollo clinico pur in un ambito territorialmente abbastanza omogeneo come quello della nostra regione : sicuramente vero che le esd del singolo esame toracico sono basse , per la sua diffusione alquanto ampia ( infatti come numero di prestazioni rappresenta circa il 50% di tutte le indagini radiografiche tradizionali ) rende importante una sua omogeneizzazione ed ottimizzazione . it is hoped that the numerous duties provided for by decree auspicabile che i numerosi adempimenti previsti dal d . 
lgs. 187 / 2000 non vengano interpretati come un mero assolvimento conclusioni conclusions table 3 average dose - length product ( dlp ) values ( mgy cm ) for computed tomography ( ct ) examinations provided by emilia - romagna region hospitals tabella 3 valori di dlp medi ( in mgy cm ) per gli esami tc forniti dalle varie aziende sanitarie della regione emilia - romagna g . 
evaluations performed in our study demonstrate that both cooperation of all professionals involved in patient radiation protection and experience gained in the various surveys are fundamental in this type of study in that data collection is a very delicate phase which , if not accurately conducted , can invalidate all subsequent data processing . 
a new survey of the same hospitals for the years after 2002 will allow us to make a more accurate quantitative evaluation of the issues addressed in this study . di obblighi di legge , ma contribuiscano a migliorare realmente le prestazioni di radiologia diagnostica . 
in particolare , il monitoraggio della dose alla popolazione pu essere un utile strumento di ottimizzazione in quanto permette di effettuare valutazioni pragmatiche e non teoriche , usando dati raccolti sul campo , senza appesantire le normali attivit lavorative : le regioni infatti possono raccogliere i dati in maniera efficiente , nel senso di usare valutazioni che devono essere comunque effettuate dal responsabile dellimpianto radiologico e dallesperto in fisica medica . 
most mediastinal abnormalities are initially suspected following chest radiography ; the need for further investigation and the most appropriate imaging modality are largely dictated by the tentative diagnosis made on this examination . 
although routine chest radiography initiates the evaluation of mediastinal disorders , it is rarely diagnostic : notable exceptions are teeth or bones within a mass , which are diagnostic of a teratoma ; air / fluid levels suggest an oesophageal origin , hernia , cyst , or abscess . 
however , even sct with contrast material is occasionally diagnostic ( a confident diagnosis can be made of some lesions such as mature teratoma and mediastinal goiter ) but is usually sufficient for preoperative evaluation before mediastinotomy or mediastinoscopy : it is instrumental in planning further diagnostic workup . 
thyroid scanning with radioactive iodine is useful in identifying and evaluating masses of suspected thyroid origthe role of fluorodeoxyglucose positron emission tomography ( fdg - pet ) in mediastinal diseases continues to be evaluated : it has potential for differentiating between benign and malignant disease and is expected to play a more extensive role in the imaging of mediastinal neoplasms in the future . 
in this paper , the radiological features of masses located in the anterior mediastinum are discussed , with particular reference to radiographic and ct patterns useful to the clinicians everyday practice . key words anterior mediastinum standard radiography computed tomography magnetic resonance imaging positron emission tomography sonography riassunto il mediastino suddiviso in compartimenti ( anteriore , medio , posteriore ) sulla base della radiografia del torace in proiezione laterale . 
la maggior parte delle alterazioni mediastiniche sono sospettate alla radiografia del torace ; lopportunit di ulteriori indagini e la metodica ottimale di imaging sono dettate dalla diagnosi presuntiva formulata con tale esame . 
sebbene un radiogramma standard del torace inizi la valutazione delle malattie del mediastino , raramente diagnostico : fanno eccezione denti o osso entro una massa , che sono patognomonici per teratoma ; livelli aria - fluido suggeriscono lorigine esofagea , unernia , cisti o ascessi . 
tuttavia , anche la stc con mezzo di contrasto occasionalmente diagnostica ( possono essere formulate diagnosi presuntive di alcune lesioni , come il teratoma maturo e lo struma ) , ma in genere sufficiente per una valutazione preoperatoria prima di una mediastinotomia o di una mediastinoscopia : utile nella programmazione di ulteriori indagini diagnostiche . 
il ruolo della fdg - pet nelle malattie del mediastino in corso di valutazione : ha un valore potenziale nella diagnosi differenziale tra malattia benigna e maligna ed in futuro rivestir un ruolo pi estensivo nellimaging delle neoplasie mediastiniche . in questo lavoro , vengono enfatizzate le caratteristiche radiologiche delle masse localizzate nel mediastino anteriore , con particolare riferimento alla semeiotica radiologica , alla radiografia del torace ed alla tomografia computerizzata , utili nella pratica clinica quotidiana . parole chiave mediastino anteriore radiologia tradizionale tomografia computerizzata risonanza magnetica tomografia ad emissione di positroni ecotomografia s.m. 
to fully understand the nosography of this region , it is therefore indispensable to make some considerations on its contents and semantics , which are functional to the study techniques and their signs . il mediastino anteriore uno spazio del torace pressoch virtuale che , tuttavia , pu essere sede di numerose condizioni patologiche . 
sono dunque indispensabili , ai fini della piena comprensione della nosografia , alcune premesse sul contenuto e sulla semantica topografica , funzionali alla analisi delle tecniche di studio ed allapprendimento della semeiotica ad esse relative . contents of the anterior mediastinum different structures are present in the anterior mediastinum : containing structures ( muscles , ligaments , fat tissue ) , vessels , lymphatic tissue , parenchymatous organs : the transversus thoracis or triangularis sterni , which is located on the inner side of the anterior chest wall , delimits the mediastinum anteriorly , but its thickness is not sufficient to produce a corresponding radiological pattern . 
the inner aspect of the muscle is lined by the endothoracic fascia . the sternopericardial ligaments , upper and lower , extend between the pericardium and the sternal manubrium and xiphoid process , respectively . the internal thoracic artery or internal mammary artery originates from the first portion of the subclavian artery , descends behind the first six costal cartilages and ends at the sixth intercostal space giving rise to the musculophrenic artery and the superior epigastric artery ; it is accompanied by a chain of lymph nodes and by two satellite veins . the anterior mediastinal arteries ( which distribute to the areolar tissue and anterior mediastinum lymph nodes to the remains of the thymus and to the pericardium ) and the sternal branches ( for the transversus thoracis and the posterior aspect of the sternum ) are collateral branches of the internal mammary artery . the lymph node stations of the anterior mediastinum are the parietal lymph nodes of the internal mammary chains and the diaphragmatic chains , and the visceral lymph nodes of the anterior mediastinum chains . the lymph nodes of the internal mammary chain or sternal lymph nodes may vary from six to ten in number . 
they are located deep in the thoracic cavity on the endothoracic fascia in the intercostal spaces ivi between the costal cartilages , adjacent to the medial or lateral margin of the internal mammary vessels . 
the efferent collectors flow into a single trunk , which reaches the internal jugular vein directly at its confluence with the subclavian vein or the thoracic duct on the left and the subclavian trunk on the right . the anterior mediastinum lymph nodes form different clusters : right and left anterior mediastinum lymph nodes , lymph nodes of the transverse chain , and diaphragmatic nodes ; they receive lymphatic collectors from the diaphragm , pleura , heart , pericardium , lung , thymus , thyroid and trachea . 
they are connected to the sternal lymph contenuto del mediastino anteriore nel mediastino anteriore si descrivono diverse entit : strutture di contenimento ( muscoli , legamenti , tessuto adiposo ) , vasi , tessuto linfatico , organi parenchimatosi . il muscolo trasverso del torace o triangolare dello sterno , che situato sulla faccia interna della parete toracica anteriore , limita anteriormente il mediastino , ma il suo spessore non sufficiente a dare un corrispettivo reperto radiografico . 
la faccia interna del muscolo rivestita dalla fascia endotoracica . i legamenti sternopericardici , distinti in superiore ed inferiore , sono tesi tra pericardio e , rispettivamente , manubrio sternale e processo xifoideo . larteria toracica interna o mammaria interna origina dalla prima porzione dellarteria succlavia , discende in basso , dietro le prime sei cartilagini costali , e termina al vi spazio intercostale dando larteria muscolofrenica e larteria epigastrica superiore ; accompagnata da una catena di linfonodi e da due vene satelliti . le arterie mediastiniche anteriori ( che si distribuiscono al tessuto areolare ed ai linfonodi del mediastino anteriore , ai residui del timo ed al pericardio ) ed i rami sternali ( per il muscolo trasverso del torace e la faccia posteriore dello sterno ) sono rami collaterali dellarteria mammaria interle stazioni linfonodali del mediastino anteriore sono rappresentate da linfonodi parietali , delle catene mammarie interne e delle catene diaframmatiche , e da linfonodi viscerali , delle catene del mediastino anteriore . i linfonodi della catena mammaria interna o linfonodi sternali variano da sei a dieci . 
sono situati in profondit alla parete toracica , sulla fascia endotoracica negli spazi intercostali i - vi , tra le cartilagini costali , adiacenti al margine mediale o laterale dei vasi mammari interni . 
i collettori efferenti confluiscono in un tronco unico che raggiunge direttamente la vena giugulare interna alla sua confluenza con la vena succlavia oppure a sinistra il dotto toracico e a destra il tronco succlavio . i linfonodi mediastinici anteriori costituiscono diversi raggruppamenti : linfonodi mediastinici anteriori di destra , di sinistra , della catena trasversa , diaframmatici ; ricevono collettori linfatici che provengono dal diaframma , dalla pleura , dal cuore , dal pericardio , dal polmone , dal timo , nodes , and they send efferent collectors to the bronchomediastinal trunks . the anterior mediastinum also contains , at its lower boundary , the anterior and middle diaphragmatic lymph nodes or cardiophrenic angle nodes . 
the anterior diaphragmatic lymph nodes are situated on the diaphragm dome in front of the anterior leaflet of the central tendon behind the xiphoid process and the cartilage of the seventh rib . 
the middle diaphragmatic lymph nodes are found close to the point of innervation of the diaphragm by the phrenic nerve ; they are often missing on the left side . the thymus is a lymphoepithelial organ located for the most part in the anterior mediastinum with a small portion in the neck . 
it is a transient organ that is considerably developed in the foetus and during the early years of life ; in the young adult it undergoes fatty involution , with wide individual variability . occasionally , the anterior mediastinum may contain the lower pole of the thyroid or an ectopic parathyroid that has migrated with the thymus . topography of the anterior mediastinum to map its contents , the anterior mediastinum may schematically be divided into two regions : upper and lower . 
at this level , behind the anterior chest wall and lateral to the sternum , lie the parietal nodes of the internal mammary chain ( or sternal nodes ) , arranged along the course of the mammary vessels and , at a deeper level , three prevascular chains of the anterior mediastinum ( anterior mediastinal lymph nodes )  . 
finally , the anterior mediastinum communicates widely with the neck , middle mediastinum and , through the sternal fasciae of the diaphragm , with the preperitoneal lax connective tissue of the anterior abdominal wall . radiological anatomy of the anterior mediastinum . compartment definitions : anatomical and radiological classification the mediastinum extends from the sternum to the spine in an anteroposterior direction and from the thoracic inlet to the diaphragm in a craniocaudal direction . 
sono connessi con i linfonodi sternali ed inviano collettori efferenti ai tronchi broncomediastinici . il mediastino anteriore contiene anche , al suo limite inferiore , i linfonodi diaframmatici anteriori e medi o dellangolo cardiofrenico . i linfonodi diaframmatici anteriori sono posti sulla convessit del muscolo al davanti della fogliola anteriore del centro tendineo , dietro il processo xifoideo e la cartilagine costale della vii costa . 
i collettori efferenti si connettono con i linfonodi mediastinici e con i linfonodi sternali . i linfonodi diaframmatici medi sono prossimi al punto di innervazione del diaframma da parte del nervo frenico ; sono spesso assenti dal lato sinistro . il timo un organo linfoepiteliale localizzato , per la maggior parte , nel mediastino anteriore e , per una piccola porzione , nel collo . 
un organo transitorio , notevolmente sviluppato nel feto e nei primi anni della vita postnatale : va incontro ad involuzione adiposa nel giovane adulto , peraltro con un notevole grado di variabilit individuale . occasionalmente , nel mediastino anteriore pu localizzarsi il polo inferiore della tiroide o una paratiroide ectopica migrata con il timo . topografia del mediastino anteriore per collocare topograficamente il contenuto , per ragioni di semplicit , il mediastino anteriore pu , del tutto schematicamente , essere distinto in due distretti : superiore ed inferiore . superiormente rappresentato dalla loggia timica . 
a questo livello si localizzano , a ridosso della parete toracica anteriore e di lato allo sterno , i linfonodi parietali della catena mammaria interna ( o linfonodi sternali ) , disposti lungo il decorso dei vasi mammari e , pi profondamente , tre catene linfonodali prevascolari del mediastino anteriore ( linfonodi mediastinici anteriori )  . 
inferiormente rappresentato dal tessuto adiposo extra - pericardico con lestensione laterale , pi o meno pronunciata , dei cuscinetti adiposi paracardiaci . agli angoli cardiofrenici , si localizzano alcuni gruppi dei linfonodi parietali delle catene diaframmatiche ( linfonodi diaframmatici anteriori e medi o dellangolo cardiofrenico )  . infine , il mediastino anteriore comunica ampiamente con collo , mediastino medio e , attraverso i fasci sternali del diaframma , con il tessuto lasso preperitoneale della parete addominale anteriore . anatomia radiologica del mediastino anteriore . 
definizioni di compartimento : classificazione anatomica e radiologica il mediastino si estende , in senso antero - posteriore , dallo sterno alla colonna vertebrale e , in senso cranio - caudale , s.m. 
the mediastinum may be divided into three compartments on the basis of the lateral chest radiograph : anterior , central or middle and posterior [ 3 , 4 ]  . 
the anterior mediastinum lies behind the sternum and in front of the great vessels and pericardiuit is laterally bounded by the mediastinal pleurae in contact with the anteromedial portion of each lung . 
inferiorly it extends to the diaphragm whereas its upper boundary is arbitrarily considered the plane extending from the inferior margin of the manubrium to the lower edge of the fourth dorsal vertebra . 
however , because the anterior edge of the ascending aorta and brachiocephalic veins are difficult to visualise radiologically and the anterior mediastinal masses often project onto the heart , felsons classification [ 2 ] included among the disorders affecting this compartment lesions predominantly located in the region bounded posteriorly by a fig . 
anatomicamente suddiviso in superiore ( al di sopra del piano che passa per larticolazione manubrio - corpo sternale e la superficie inferiore della iv vertebra dorsale ) ed inferiore ( ulteriormente distinto nei compartimenti anteriore o prevascolare , medio o cardiovascolare e posteriore o postvascolare )  . 
tuttavia , sussistono molti punti criticabili in questa classificazione , come sottolineato da heitzman [ 1 ] e felson [ 2 ] : , in realt , basata solo parzialmente sullanatomia del mediastino , dal momento che lunica struttura di riferimento per la sepimentazione il pericardio , anche perch non esistono piani anatomici o fasciali che suddividano il mediastino in compartimenti definiti ; pertanto , una suddivisione anatomica ha un corrispettivo radiologico modesto . radiologicamente , nonostante lesistenza di numerose classificazioni , nessuna tra queste ha trovato unanime consenso . 
il mediastino pu essere distinto , sulla base del radiogramma del torace in proiezione laterale , in tre compartimenti : anteriore , centrale o medio e posteriore [ 3 , 4 ]  . 
infine , pi di recente , fraser ha definito compartimento mediastinico anteriore la regione situata al davanti di una linea tracciata , sempre sul radiogramma laterale del torace , lungo il margine anteriore della silhouette cardiaca ed i vasi brachiocefalici [ 4 ]  . line passing through the anterior edge of the trachea and the posterior margin of the heart . 
more recently , fraser defined the anterior mediastinal compartment as the region situated in front of a line drawn on the lateral chest radiograph along the anterior margin of the cardiac silhouette and the brachiocephalic vessels [ 4 ]  . in conclusion , although the best classification is still a matter of debate , alternative classifications to that proposed by heitzman appear to have limited clinical utility . study techniques and semeiotics chest imaging offers two main possibilities to study this region : conventional radiology ( cr ) and computed tomography ( ct )  . 
cr has an important role given that the first step in identifying a mediastinal disorder is standard chest radiography , the semeiotics of which relies on the assessment of mediastinal lines . 
in addition , sonography and nuclear medicine functional imaging are useful tools for further investigation in selected cases and in some instances may even become the examinations of choice ( endocrine disorders , diseases of the thyroid and parathyroid , ectopic glands )  . standard radiography pathological processes affecting the anterior mediastinum are frequently silent , and consequently , their radiological detection is incidental : around 40% of mediastinal masses are asymptomatic [ 5 ]  . 
radiographs with posteroanterior ( pa ) and laterolateral ( ll ) views represent the basic imaging modality in the study of the chest and mediastinuchest radiography allows localisation of the pathological process : orthogonal projections can demonstrate site , size and density and the presence of calcifications , thereby narrowing the range of differential diagnoses . 
moreover , fluoroscopic examination and opacification of the oesophagus will provide valuable complementary information . a mediastinal mass may : be directly visible and protrude unior bilaterally from the mediastinum and have varying degrees of lobulation ; cause an increase in the density of part of the mediastinum ; change the appearance of the mediastinal lines . 
in particular , judging normality on a radiograph presupposes adequate knowledge of the pattern formed by the mediastinal lines the interfaces between lung and mediastinum that can be observed in specific conditions . 
it should be recalled that radiologically , a line is formed when certain conditions are met : there is a difference in density between two adjacent tissues ; the two tissues are separated by a curved surface ; the beam hits this surface tangentially . these conditions occur often in chest radiography where the s.m. 
il ruolo della rt importante , poich il primum movens alla identificazione di una patologia mediastinica la radiografia standard del torace , la cui semeiologia affidata alla valutazione delle linee mediastiniche . la comprensione anatomica stata , peraltro , enormemente facilitata dallavvento delle tecniche di imaging tc e di risonanza magnetica ( rm ) che consentono la precisa localizzazione delle varie strutture mediastiniche . 
inoltre , lecotomografia e limaging funzionale di medicina nucleare costituiscono , in casi selezionati , utili strumenti informativi di approfondimento diagnostico , talvolta rappresentando persino esami di elezione ( patologia endocrina , tiroidea e paratiroidea , in ghiandole ectopiche )  . radiogramma standard i processi patologici del mediastino anteriore sono frequentemente silenti nella sintomatologia ed il riscontro radiologico pertanto incidentale : infatti circa il 40% delle masse mediastiniche asintomatico [ 5 ]  . 
le radiografie in proiezione pa e ll rappresentano lindagine radiologica base nello studio del torace , in generale , e del mediastino , nello specifico . la rt consente , in prima istanza , di localizzare il processo patologico : le proiezioni ortogonali definiscono la sede , la dimensione , la densit , la presenza di calcificazioni restringendo il ventaglio delle diagnosi differenziali . 
inoltre , lesame radioscopico e la opacizzazione dellesofago offrono valide informazioni complementari . la massa mediastinica pu essere direttamente visibile e protrudere monoo bilateralmente dal mediastino con contorni pi o meno polilobulati , determinare un aumento di densit di un distretto del mediastino o modificare la morfologia delle linee mediastiniche . in particolare , il giudizio di normalit dellimmagine radiografica presuppone una adeguata conoscenza della semeiotica basata sulle linee mediastiniche , rappresentate dalle interfacce polmone - mediastino osservate in particolari condizioni . 
it is therefore possible , based on the knowledge of the plane to which the mediastinal lines belong , to have a provisional three - dimensional ( 3d ) analysis of the mediastinum in a single view . 
normal morphology of these lines is a reliable indication of normality of the single mediastinal compartments : the presence of space - occupying lesions will , instead , cause their displacement or cancellation . 
 pa radiogram : anterior junction line or anterior commissure as the two lungs approximate anteromedially , they are separated by four layers of pleura and a variable amount of fat , giving rise to a septum of varying thickness : the anterior junction line ( ajl ) or anterior mediastinal line or anterior commissure . 
this line is present when there is apposition of the pleurae behind the sternusince the anterior portions of the lungs join only from the sternal manubrium downwards , the ajl ends superiorly at the sternal angle of louis ( notch for second rib )  . 
2 una radiografia del torace in proiezione postero - anteriore mostra sia la linea di giunzione anteriore sia la linea di giunzione posteriore . tessuti siano separati da una superficie curva , il fascio incidente colga tangenzialmente tale superficie . 
queste condizioni si verificano spesso nellosservazione radiografica delle riflessioni dei polmoni ( aerati e quindi radiotrasparenti ) sul mediastino ( radiopaco ) : da qui la formazione di numerose linee , definite linee mediastiniche . 
nel mediastino anteriore riconosciamo linee in proiezione frontale ( linea di giunzione anteriore ) e laterale ( linea retrosternale ) [ 1 , 3 ]  . risulta cos possibile , avvalendosi della conoscenza del piano di appartenenza delle linee mediastiniche , una analisi presuntiva tridimensionale del mediastino in una sola vista . una regolare morfologia di tali linee affidabilmente indicativa della normalit dei singoli compartimenti mediastinici : la presenza di lesioni occupanti spazio determina invece un loro spostamento o la loro cancellazione . radiogramma in proiezione pa : linea di giunzione anteriore o commissura anteriore nellaccostarsi antero - medialmente , i due polmoni restano separati da quattro strati di pleura e da una certa quantit di tessuto adiposo interposto , venendosi a formare un setto di spessore variabile : la linea di giunzione anteriore ( lga ) o linea mediastinica anteriore o commissura anteriore . 
questa presente nel caso si realizzi il mutuo contatto delle pleure in sede retrosternale . dal momento che le porzioni anteriori dei polmoni si congiungono solo dal manubrio sternale in gi , la lga ha , come suo limite superiore , langolo sternale del luys ( ii incisura costale )  . 
in basso , si estende , per una lunghezza variabile ( 58 cm ) , sino al punto di contatto del cuore con i tessuti molli retrosternali . si apre verso lalto per delimitare la loggia timica . 
al contrario , lincapacit di visualizzare una lga precedentemente presente ( con ampliamento dellombra mediastinica anteriore o superiore ) , su indagini radiografiche seriate , suggerisce linterposizione di un espanso tra i margini anteriori dei due polmoni e induce il sospetto di malattia mediastinica . 
by contrast , the inability to see an ajl that was previously present ( with widening of the anterior or superior mediastinal shadow ) on serial radiographs suggests the interposition of a mass between the anterior margins of the two lungs and raises the suspicion of mediastinal disease . 
at the caudate end of the ajl , the presence of fat pads produces simple marginal lines at the paracardiac level , which are due to creation of the interface conditions described above . ll radiograph : retrosternal line or anterior extrapleural line in front of the ajl , behind the sternum , the pleural interfaces diverge as they create each pleural cavity . 
in normal individuals , the anterior portion of the lungs reaches the anterior chest wall , and therefore , the retrosternal area in front of the heart is completely radiolucent in the true lateral view . 
the opaque line with soft - tissue density ( the retrosternal line or anterior extrapleural line , ael ) , which evenly follows the profile of the sternum , is made up of retrosternal fat , internal s.m. 
inoltre , da sottolineare che , poich lo spessore della lga variabile , la sua valutazione non affidabile a meno di un suo grossolano ispessimento . allestremo caudale della lga , per effetto della presenza di cuscinetti adiposi , si possono riscontrare , a livello paracardiaco , linee semplici marginali , dovute allinstaurarsi delle condizioni di interfaccia precedentemente descritte . radiogramma in proiezione ll : linea retrosternale o linea extrapleurica anteriore al davanti della lga , dietro lo sterno , le interfacce pleuriche divergono nel costituire ciascuna cavit pleurica . 
negli individui normali la porzione anteriore dei polmoni raggiunge la parete toracica anteriore e , pertanto , larea retrosternale , al davanti del cuore , interamente radiotrasparente in proiezione laterale vera . la banda opaca , della densit delle parti molli ( che rappresenta la linea retrosternale o linea extrapleurica anteriore , lea ) uniformemente addossata al profilo dello sterno , costituita da tessuto adiposo retrosternale , vasi e linfatici mammari interni , nervi intercostali . 
inferiormente , in sede paracardiaca , la presenza di un cuscinetto adiposo pu determinare un analogo scostamento della linea . inoltre , anche nella proiezione laterale , come gi nella frontale , la presenza di cuscinetti pu determinare la formazione di linee semplici . frequente nei soggetti brachitipi obesi la presenza di opacit triangolari con apice al processo xifoideo e base verso il parenchima , sostenute dai triangoli opachi parasternali , che corrispondono a cuscinetti adiposi particolarmente sviluppati . il cuscinetto adiposo prepericardico pu raggiungere notevoli dimensioni ( 35 cm in altezza , 10 cm in lunghezza ) e pu protrudere su ambo i lati del mediastino , pi frequentemente a sinistra . 
3 radiografia laterale del torace con evidenza della linea retrosternale normale . in sintesi , le formazioni del mediastino anteriore determinano lo slargamento della lga , mentre nel radiogramma in proiezione ll si possono apprezzare come opacit che occupano lo spazio chiaro retrosternale , con ondulazioni della s.m. 
inferiorly , the presence of a fat pad at the paracardiac level may produce similar displacement of the line . in addition , in the lateral view as well as in the frontal view , the presence of fat pads may cause the formation of simple lines . 
a frequent finding in endomorph obese subjects is the presence of triangular opacities with the apex at the xiphoid process and the base towards the parenchyma ; these are related to opaque parasternal triangles corresponding to particularly developed fat pads . 
i dati rilevabili dalla radiografia del torace permettono pertanto , quasi sempre , di accertare la presenza e la sede di una patologia mediastinica , ma , tranne poche eccezioni , non consentono di definirne natura , organo di origine e presenza di eventuali caratteri infiltrativi . 
la rt per queste ragioni raramente diagnostica , con poche eccezioni : calcificazioni linfonodali a guscio duovo , se pur rare , sono fortemente suggestive di silicosi , linfoma trattato e sarcoidosi ; il riscontro di denti o osso o di un livello grasso / fluido nel contesto di una massa sono patognomonici di teratoma ; la presenza di livelli idro - aerei suggerisce lorigine esofagea , unernia , lesioni cistiche o ascessi [ 7 ]  . 
le immagini assiali eliminano il problema relativo alla sovrapposizione dei tessuti a densit simile : la dimostrazione degli spazi mediastinici e delle stazioni linfonodali in essi contenute ed il rapporto con le strutture circostanti ed i vasi sanguigni costituiscono lapporto qualitativamente pi importante della tc . le indicazioni comprendono la caratterizzazione , sulla base dei valori di attenuazione , di lesioni ( cistiche / solide , densit adiposa / calcificazioni ) individuate sul radiogramma standard e la valutazione del mediastino in pazienti con sospetto clinico e radiografia standard negativa [ 8 , 9 ]  . i vantaggi di questa procedura possono essere raggruppati in due categorie generali : ( 1 ) la descrizione fine e analitica del dettaglio anatomico , garantita dalla rappresentazione per strati , associata alla acquisizione volumetrica spirale ed alla fruibilit di nuovi punti di vista ( mpr ) e di tecniche innovative di post processing ; ( 2 ) lanalisi densitomefig . 
4 una radiografia laterale del torace evidenzia una linea retrosternale anomala ( banda retrosternale ) dovuta a lipomatosi . from a few exceptions , it cannot define its nature , organ of origin or the presence of possible infiltrative features . 
for these reasons , chest radiography is seldom diagnostic , with few exceptions : although uncommon , egg - shell lymph node calcifications are strongly suggestive of silicosis , treated lymphoma and sarcoidosis ; the finding of teeth , bone or a fat / fluid level within a mass are diagnostic of teratoma ; the presence of air / fluid levels suggests an oesophageal origin , a hernia , cystic lesions or abscesses [ 7 ]  . 
axial imaging avoids the problem of overlapping tissues with similar density : demonstration of mediastinal spaces with their lymph nodes , relations with surrounding structures and blood vessels represent the most important contributions of ct . 
indications include characterisation of lesions ( cystic / solid , adipose density / calcification ) previously identified on standard x - ray based on attenuation values and assessment of the mediastinum in patients with a clinical suspicion of disease but negative standard x - ray [ 8 , 9 ]  . advantages of ct fall into two major categories : ( 1 ) a fine analytical depiction of anatomical detail guaranteed by cross - sectional imaging associated with volumetric spiral acquisition and availability of new points of view [ multiplanar reformatting ( mpr ) ] and innovative postprocessing techniques ; ( 2 ) densitometric analysis ( with good preservation of spatial resolution ) and enhancement patterns . 
with its higher contrast resolution compared with chest radiography , ct allows distinction between the different mediastinal organs and visualises the lesion directly ; this leads to better localisation of a mediastinal mass , allows assessment of its extension and relations with neighbouring organs and determination of attenuation values of mass content , which , if integrated with data on the site of origin , often allows the nature of the mass to be defined . 
 most masses involving the anterior mediastinum and most cystic lesion , even when benign , require surgical resection . the choice among the various options [ video - assisted thoracic surgery ( vats ) , standard cervical mediastinoscopy , anterior mediastinotomy , thoracoscopy , thoracotomy ] is dictated by the nature of the lesion as demonstrated by ct , by whether a biopsy or resection is required and by the surgeons ability and experience . 
in sintesi , la tc per la sua superiore risoluzione di contrasto rispetto alla rt permette di distinguere i differenti organi mediastinici visualizzando direttamente la lesione ; ci porta ad una migliore definizione topografica ( localizzazione ) delle alterazioni mediastiniche , a valutare lestensione , i rapporti con gli organi vicini e a rilevare dati di attenuazione del contenuto della massa stessa che , integrati con la sede di origine , consentono non di rado di definirne la natura . 
la tc inoltre importante per il conseguimento dellaccertamento bioptico . la maggior parte delle masse a localizzazione mediastinica anteriore e delle lesioni cistiche , anche quando benigne , richiede una resezione chirurgica . 
la scelta tra le diverse opzioni ( video assisted thoracic surgery - vats , mediastinoscopia cervicale standard , mediastinotomia anteriore , toracoscopia , toracotomia ) indirizzata dai riscontri alla tc , evocativi della natura della lesione , dallintento perseguito di biopsia o resezione e dalla abilit ed esperienza del chirurgo . 
la diagnosi definitiva delle lesioni a sede nel mediastino anteriore , comunque , pi spesso ottenuta con lago - aspirato ( fine needle aspiration biopsy - fnab ) percutaneo sotto guida tc . 
tuttavia , lindagine tc in genere sufficiente per la valutazione preoperatoria ( esame di diagnostica per immagini di ultimo livello ) , prima di indirizzarsi verso una procedura invasiva per laccertamento della diagnosi , poich utile nella visualizzazione delle eventuali linfoadenopatie mediastiniche o ilari , nella diagnosi differenziale con anomalie vascolari e nella discriminazione di varianti anatomiche [ 7 ]  . semeiotica tc la diagnosi differenziale delle patologie mediastiniche alla tc avviene sulla base di numerose osservazioni , che includono la localizzazione , lidentificazione della struttura di origine , la definizione della unicit , multifocalit o del carattere di processo diffuso , la dimensione e la forma , lattenuazione ( grasso , fluido , tessuto molle o una combinazione di questi ) , la presenza di calcificazioni ed il contrast enhancement . 
gli espansi mediastinici possono presentare attenuazione bassa , alta o pari a quella del grasso ; le lesioni a bassa attenuazione hanno densit superiore a quella del grasso , ma inferiore a quella del muscolo , mentre lalta attenuazione contraddistingue una densit superiore a quella del muscolo . 
le lesioni con la densit del grasso includono : lipomatosi e cuscinetti adiposi , timolipoma , teratoma , lipoma e liposarcoma , ernie di tessuto adiposo [ 10 ]  . 
low - attenuation lesions are generally cystic and include congenital or acquired cysts , cystic thymoma , germ - cell tumours , lymphangioma and haemangioma , mediastinal abscesses , mediastinitis , haematoma , cystic struma , and primary or secondary necrotic tumours [ 11 ]  . high - density masses contain calcium or are rich in iodine or blood . 
they include : calcific lymphadenopathy ( granulomatous infections , sarcoidosis , silicosis ; adenocarcinoma and sarcoma metastasis ; treated lymphoma ) , partially calcific primary tumours ( germ - cell tumours , thymoma ) , struma ( calcific or rich in iodine ) , vascular atheroma and mediastinal haematoma [ 12 ]  . finally , after administration of contrast material , enhancing masses are strongly vascular [ 13 ] and include thyroid and parathyroid , carcinoid tumour , lymphangiomas and haemangiomas , partially necrotic inflammatory and neoplastic lesions . in conclusion , diagnostic accuracy of ct is higher than that of conventional chest radiography : in a study of 128 patients , the correct diagnosis was achieved in 48% of cases with ct and in only 36% of cases with chest radiography [ 14 ]  . magnetic resonance imaging mri has not been as extensively used as ct in the study chest pathology . 
the reason is that it has suffered from certain technical limitations mainly artefacts caused by respiratory and cardiac movements but technological progress has made gating systems available and allowed the acquisition of fast sequences that are virtually free of artefacts and are used in cardiovascular imaging . 
considering its multiplanar capabilities and excellent depiction of musculoskeletal structures , mri is generally suitable for studying processes located near the lung apex and spine and in the chest wall , as well as disorders of the mediastinal vessels and peridiaphragmatic regions . 
 however , its high capacity for tissue differentiation allows discrimination , in a single examination , between pleural involvement and parenchymal consolidation and mediastinal and chest - wall involvement , which may be associated . 
in addition , it can distinguish atelectasia within an area of increased parenchymal density [ 15 ]  . le masse ad alta densit contengono calcio , ovvero hanno un alto contenuto di iodio oppure sono in relazione con un elevato tenore ematico ; includono : linfoadenopatie calcifiche ( infezioni granulomatose , sarcoidosi , silicosi ; metastasi da adenocarcinoma e sarcoma ; linfoma dopo trattamento ) , tumori primitivi parzialmente calcifici ( tumori a cellule germinali , timoma ) , struma ( calcifico o ad alto contenuto di iodio ) , ateromasie in lesioni vascolari , ematoma mediastinico [ 12 ]  . infine , dopo somministrazione di mezzo di contrasto , le masse con enhancement hanno alto tenore vascolare [ 13 ] ed includono tiroide e paratiroidi , carcinoidi , linfangiomi ed emangiomi , lesioni infiammatorie e neoplastiche parzialmente necrotiche . in conclusione , laccuratezza diagnostica di questa metodica risulta superiore alla radiografia tradizionale del torace : in uno studio su 128 pazienti , la diagnosi corretta stata conseguita nel 48% dei casi sulla base della tc e solo nel 36% dei casi al radiogramma toracico [ 14 ]  . risonanza magnetica a causa di alcuni limiti tecnici , la rm non stata utilizzata in modo estensivo nello studio della patologia toracica al contrario della tc . 
sussistevano infatti alcuni svantaggi nelle sue applicazioni al distretto toracico , principalmente gli artefatti generati dai movimenti respiratorio e cardiaco , sebbene oggi i progressi tecnologici abbiano reso disponibili sistemi gating e permesso lacquisizione di sequenze veloci , quasi del tutto prive di artefatti , utilizzate nella dimostrazione della patologia cardiovascolare . in considerazione della possibilit di rappresentazione multiplanare e della eccellente dimostrazione delle strutture muscoloscheletriche , la rm , in termini generali , idonea alla valutazione di processi localizzati in prossimit dellapice del polmone , della colonna vertebrale , nella parete toracica ed , infine , adeguata allo studio di patologie che coinvolgano i vasi mediastinici e le regioni peridiaframmatiche . 
ha , invece , applicazioni pi limitate nella valutazione della patologia del parenchima polmonare , a meno che sia associato un interessamento pleurico . tuttavia , a suo favore , lelevata capacit di differenziazione tessutale consente , in un unico esame , la discriminazione dellinteressamento pleurico dal consolidamento parenchimale , dal coinvolgimento mediastinico e della parete toracica , che possono essere associati . 
consente , inoltre , di distinguere nel contesto di un addensamento parenchimale la componente atelectasica [ 15 ]  . le indicazioni a questa modalit di imaging multiplanare sono , dunque , nellambito del distretto toracico limitate : pu essere utilizzata come indagine di terzo livello , complementare alla tc , ma senza che rivesta un carattere routinario [ 16 , 17 ]  . solo in casi selezionati si dimostra superiore alla tc e potrebbe , pertanto , rappresentare lindagine di seconda istanza , nello specifico di : valutazione di lesioni vascolari ; definizione del coinvolgimento vascolare da parte di processi patologici estrinseci ; studio della parete toracica e del mediastino posteriore ; imaging delle regioni paravertebrali , indications for mri are therefore limited : it may be used as a third - level investigation to complement ct but not as a routine study [ 16 , 17 ]  . 
these cases are assessment of vascular lesions ; definition of vascular involvement by extrinsic pathological processes ; study of the chest wall and posterior mediastinum ; imaging of the paravertebral regions , nerve plexuses and neurogenic tumours ; recognition , within the mediastinal structures and heart , cleavage planes and their invasion by tumours , particularly when the ct findings are doubtful ; and differential diagnosis between fibrous tissue and persistence or recurrence of neoplasm after radiation therapy . 
it is therefore useful when there is a contraindication to iodinated contrast agents , in imaging of the posterior mediastinum and to assess invasion of tissues , vessels and the heart . 
its limitations on the other hand are : claustrophobia , compliance of debilitated patients , examination times , high cost and limited availability . in conclusion , where mri provides the same diagnostic information as ct , ct should be preferred . 
the gas was directly insufflated into the anterior mediastinum through a curved needle inserted just above the throat and pushed along the posterior surface of the sternum for a few centimetres [ 19 ]  . 
on the other hand , it gave clear depiction of contours of a normal or pathological thymus thereby providing useful topographic information for planning surgical thymectomy . sonography transthoracic ultrasound imaging of the mediastinum is not very commonly used although its convenience and low cost make it a useful and rapid complement to radiography in selected cases [ 20 ]  . 
it has sensitivity close to that of ct , in particular in the study of certain regions ( supra - aortic , pericardiac , prevascular , paratracheal ) [ 20 ] ; in the study of mediastinal lymphadenopathy , its specificity is higher . 
questultimo aspetto di particolare rilievo per il monitoraggio dei pazienti affetti da linfoma , dopo trattamento [ 18 ]  . inoltre , nel confrontare questa metodica con la tc , lutilizzo del mezzo di contrasto in rm consentito anche nei pazienti con ridotta funzionalit renale . 
pertanto utile quando vi sia controindicazione alla somministrazione di mezzo di contrasto iodato , nellimaging del mediastino posteriore e per la valutazione dellinvasione dei tessuti , dei vasi e del cuore . 
ha inoltre il vantaggio di non utilizzare radiazioni ionizzanti . tuttavia presenta alcuni limiti : claustrofobia , compliance del paziente debilitato , tempi di esecuzione , costi e disponibilit sul territorio . in conclusione , qualora la rm offra informazioni diagnostiche equivalenti a quelle della tc , questultima rappresenta lo studio pi appropriato . 
lossigeno insufflato negli spazi del mediastino in quantit di 200300 cm3 , avvolgeva gli organi mediastinici , rendendone possibile lesatta delimitazione radiologica . il gas era direttamente insufflato nel mediastino anteriore attraverso un ago ricurvo , infisso subito al di sopra del giugulo e la cui punta veniva sospinta per qualche centimetro lungo la faccia posteriore dello sterno [ 19 ]  . 
possedeva peraltro il merito di dimostrare con chiarezza i contorni del timo , normale o patologico , fornendo utili informazioni di topografia preliminari ad uneventuale procedura chirurgica di timectomia . ecotomografia lo studio ecotomografico del mediastino per via transtoracica non molto diffuso , ma per la praticit ed il basso costo , costituisce , in situazioni selezionate , un utile e rapido esame complementare alla radiografia [ 20 ]  . consente una agile chiarificazione di reperti radiologici dubbi , senza richiedere unulteriore esposizione a radiazioni ionizzanti . presenta una sensibilit prossima a quella della tc nello studio , in particolare , di alcuni distretti ( sovraaortico , pericardico , prevascolare , paratracheale ) [ 20 ] ; per lo studio delle linfoadenopatie mediastiniche la sua specificit sembra superiore . tuttavia non consente di esaminare tutte le sezioni del mediastino . 
la finestra acustica per laccesso al mediastino ottenuta con approccio sovrasternale ( al giugulo ) [ 21 ] o parasternale [ 20 ] ; sporasonographic anatomy of the mediastinum has already been described in the literature [ 21 ]  . 
the acoustic window for access to the mediastinum is obtained with a suprasternal ( jugulum ) [ 21 ] or parasternal [ 20 ] approach ; in rare cases , an infrasternal approach may be useful [ 21 ]  . 
6a - d sonographic access to the mediastinum is obtained via the suprasternal ( a ) and parasternal ( b , c ) approach , though occasionally also the infrasternal ( d ) path is chosen . 
the great vessels and their position relative to the heart on the various levels serve as landmarks in the mediastinu suprasternal examination is carried out with the patient lying supine . 
6a - d laccesso ecografico al mediastino ottenuto attraverso lapproccio soprasternale ( a ) e parasternale ( b , c ) , sebbene venga scelta occasionalmente anche la via infrasternale ( d )  . 
b lo stesso giovane paziente , con malattia di hodgkin scleronodulare , dopo trattamento ( chemioterapia e radioterapia ) : lecotomografia dimostra unevidente riduzione della massa bulky . in a nonpathological context , lymph nodes , fat and connective tissue are depicted as homogeneous hypoechoic structures . 
the main conditions are : emphysema ( it reduces suprasternal , parasternal and aortopulmonary windows ) ; presence of fibrous tissue ( due to inflammation , surgery , radiotherapy ) ; skeletal deformations of the spine ( which may affect the patients decubitus or insonation ) , movement artefacts . 
as a result , in the event of systemic disease , sonography is penalised by its exploration limits . quality of the examination is strictly operator dependent ( adequate knowledge of mediastinal anatomy and considerable experience in image interpretation are required ) and depends on patient compliance . 
also , because the ultrasound wave is progressively attenuated as it penetrates tissue , deep lesions might not be differentiated from surrounding structures , with resulting false negative results . despite these limitations , sonography of the anterosuperior mediastinum may yield good results . 
according to the literature , sonography in expert hands is almost as reliable as ct and may therefore take on an intermediate role between chest radiography and ct [ 22 ]  . 
lindagine inoltre resa pi informativa con lintegrazione del segnale color doppler , che migliora la qualit e laccuratezza dellimaging b - mode . in un contesto non patologico , i linfonodi ed il tessuto adiposo e connettivo sono rappresentati come strutture ipoecogene a segnale omogeneo . 
le principali condizioni sono rappresentate da : enfisema ( riduce le finestre sovrasternale , parasternale ed aortopolmonare ) ; presenza di tessuto fibroso ( conseguente ad infiammazione , chirurgia , radioterapia ) ; deformazioni scheletriche del rachide ( che possono condizionare il decubito del paziente o linsonazione ) ; artefatti da movimento . 
pertanto , nellevenienza di una patologia sistemica , il limite di esplorabilit penalizza la metodica ultrasonografica . la qualit dellesame strettamente operatore dipendente ( indispensabile una adeguata conoscenza dellanatomia mediastinica ed richiesta una considerevole esperienza nella interpretazione delle immagini ) , oltre ad essere condizionata dalla compliance del paziente . 
finally , anterior mediastinal masses may be biopsied under sonographic guidance , especially if located at the edges of the sternum ; sonography minimises the risk of bleeding , as vessels are readily recognised without any need for contrast material ; complications are rare [ 25 ]  . nuclear medicine thyroid and parathyroid scintigraphy having excluded disorders affecting endocrine glands ( thyroid and parathyroid ) from the discussion , this section does not describe in detail the relevant nuclear medicine function investigations that are requested in conditions of ectopia . positron emission tomography : pet the role of fluorodeoxyglucose positron emission tomography ( fdg - pet ) in assessment of mediastinal pathology is controversial . 
8 la sezione assiale di un esame pet - ct di un uomo con tumore del polmone dimostra accumulo di fdg nei linfonodi del mediastino anteriore , che successivamente stato dimostrato essere metastatico . lapproccio soprasternale consente unaccessibilit soddisfacente nel 90%95% dei casi [ 20 ]  . lecotomografia , da quanto riportato in letteratura , a discrezionalit di un operatore esperto , quasi altrettanto affidabile della tc e , pertanto , potrebbe assumere una posizione intermedia tra radiografia del torace e tc [ 22 ]  . 
stato anche descritto luptake fisiologico , in assenza di patologia intrinseca , da parte del timo [ 2931 ] , che si verifica frequentemente in et pediatrica . non noto , in quanto sono descritti in letteratura dati contraddittori , leffetto della terapia ( chemioterapia , radioterapia a fasci esterni , radioterapia metabolica ) sulluptake da parte del timo : questultimo pu essere riscontrato prima o dopo trattamento e si verifica nei soggetti pi giovani con ghiandole pi voluminose . 
in one series , the mean differential uptake ratio for fdg by the normal thymus was 1.47 , which is considerably lower than the 2.5 associated with malignancy [ 29 ] ; this was confirmed by another study that concluded that physiological uptake of fdg by the thymus is substantially lower than that seen in the presence of disease [ 31 ]  . fdg uptake by thymic malignancies has , in fact , been reported [ 2628 ]  . 
quantitative analysis could potentially be very useful in those cases in which location and gross morphological features of the lesion at radiological imaging do not allow qualitative differentiation between physiological and pathological uptake [ 31 ]  . fdg - pet is indicated both for diagnosis and monitoring response to treatment [ 31 ]  . 
it has also been used to characterise thymoma and thymic hyperplasia , but its usefulness in this clinical context is still to be validated [ 27 ]  . in conclusion , fdg - pet has potential in the differential diagnosis between benign and malignant lesions and is expected to have a role in imaging mediastinal diseases in the future . invasive procedures : diagnostic confirmation histological diagnosis of mediastinal expansile processes is nearly always necessary to plan the most appropriate treatment . 
traditional exploratory surgery is no longer required , thanks to the development of radiological and nonradiological minimally invasive techniques and improved immunohistochemistry and electron microscopy techniques [ 3336 ]  . ct - guided percutaneous needle biopsy , whether fnab for cytological diagnosis or core - needle biopsy for histological definition , is currently standard procedure in initial assessment of most mediastinal masses . 
although fnab is generally appropriate for recognising carcinomatous lesions , coreneedle biopsy in indicated in the majority of cases , in particular when lymphoma or thymoma are suspected [ 34 , 37 , 38 ]  . guidance with ct or colour doppler us prevents puncturing vascular structures , so complications are rare . surgical procedures are still required in select cases [ 33 , 39 ]  . 
in una casistica , il differential uptake ratio medio per fdg uptake da parte del timo normale era di 1 , 47 , un valore considerevolmente inferiore al minimo di 2 , 5 associato con il riscontro di malignit [ 29 ] ; il dato stato confermato da un ulteriore studio , che ha concluso che luptake timico fisiologico di fdg consistentemente inferiore rispetto allassunzione in presenza di malattia [ 31 ]  . 
lanalisi quantitativa potrebbe potenzialmente essere molto utile nei casi in cui non fosse possibile , sulla sola base della localizzazione e dei caratteri macroscopici morfologici della lesione allimaging radiologico , differenziare qualitativamente luptake fisiologico dal patologico [ 31 ]  . fdg - pet indicata sia nella diagnosi sia nel monitoraggio della risposta alla terapia [ 31 ]  . 
in particolare , senzaltro utile nella stadiazione whole - body dei linfomi e nella valutazione , dopo trattamento , della malattia residua nei tumori a cellule germinali [ 26 ]  . 
stata inoltre utilizzata nella caratterizzazione del timoma e delliperplasia timica , ma la sua utilit in questo contesto clinico rimane da validare [ 27 ]  . in conclusione , fdg - pet ha potenzialit nella diagnosi differenziale tra lesioni benigne e maligne e , verosimilmente , guadagner un ruolo nellimaging delle patologie mediastiniche . procedure invasive per laccertamento della diagnosi laccertamento della diagnosi istologica dei processi espansivi del mediastino quasi sempre indispensabile per la pianificazione del trattamento adeguato . 
oggigiorno non sono pi necessarie procedure chirurgiche tradizionali esplorative per limplementazione di tecniche radiologiche e non - radiologiche mini - invasive e di metodiche di immunoistochimica e di microscopia elettronica pi efficaci [ 3336 ]  . lagobiopsia percutanea sotto guida tc , sia con aspirato con ago sottile ( fine needle aspiration biopsy - fnab ) per laccertamento citologico , sia con tecnica agobioptica ( core needle biopsy ) per la definizione istologica , rappresenta attualmente lo standard nella valutazione iniziale della maggior parte delle masse mediastiniche . 
sebbene la fnab sia in genere idonea nel riconoscimento delle lesioni carcinomatose , lagobiopsia indicata nella maggioranza dei casi , in particolare nel sospetto di linfoma e di timoma [ 34 , 37 , 38 ]  . 
la toracoscopia , in anestesia generale , una procedura miniinvasiva che garantisce unaccuratezza diagnostica pari a quasi il 100% nella maggior parte dei compartimenti mediastinici [ 40 ] : tuttavia dovrebbe essere riservata agli accertamenti bioptici che non possono essere conseguiti con la mes.m. 
finally , thoracotomy is almost never required for diagnosis and is indicated in select cases for exploratory purposes . diagnostic integration : laboratory tests some mediastinal lesions release substances into the bloodstream that may be measured using laboratory techniques . these markers can confirm a diagnostic suspicion , evaluate response to treatment , or indicate disease persistence or recurrence . 
some germ - cell tumours produce - fetoprotein ( fp ) , - human chorionic gonadotropin ( - hcg ) and lactate dehydrogenase ( ldh ) ; assessment of their serum levels is indispensable in evaluation of anterior mediastinal masses in males [ 4 ]  . 
in addition , in the appropriate clinical setting , evaluation of thyroid hormones , of adrenocorticotropic hormone ( acth ) and parathyroid hormone ( pth ) may help establish the nature of the lesion ( table 1 )  . conclusions diseases of the mediastinal comprise a wide spectrum of benign and malignant entities that share the same anatomical location within the chest . 
this division , which is based on the lateral chest x - ray , allows a rational , topographic approach to the differential diagnosis and helps plan further imaging studies and clinical investigations to select the definitive cytohistological procedure and the most appropriate treatment strategy . knowledge of pathology , demographics , clinical presentations , imaging patterns and treatment options is indispensable for correct management of anterior mediastinal masses , which often require a multidisciplinary approach . 
infine , la toracotomia non quasi mai necessaria per laccertamento diagnostico e , a titolo esplorativo , indicata in casi selezionati . integrazioni diagnostiche : esami di laboratorio alcune lesioni del mediastino rilasciano sostanze in circolo che possono essere misurate mediante tecniche di laboratorio . 
alcuni tumori a cellule germinali producono - fetoproteina ( - fp ) , - gonadotropina corionica umana ( - hcg ) e lattato deidrogenasi ( ldh ) : il loro dosaggio sierico indispensabile nella valutazione di masse del mediastino anteriore in soggetti di sesso maschile [ 4 ]  . inoltre , la valutazione degli ormoni tiroide , di acth e del pth pu , in casi selezionati sulla base dei dati clinici , indirizzare la diagnosi di natura ( tabella 1 )  . conclusioni le malattie del mediastino comprendono diverse entit nosografiche , di natura benigna e maligna , che condividono la stessa localizzazione anatomica nel torace . 
questa divisione , basata sul radiogramma laterale del torace , consente di stabilire razionalmente lambito delle diagnosi differenziali , di pianificare le ulteriori indagini di diagnostica per immagini e gli approfondimenti clinici per delineare laccertamento cito / istologico definitivo e la strategia terapeutica pi appropriata . la conoscenza della patologia , della demografia , delle presentazioni cliniche , dei dati di imaging e delle opzioni di trattamento indispensabile per una corretta gestione delle masse del mediastino anteriore , che spesso richiede un approccio multidisciplinare . 
in particolare , con il miglioramento delle tecniche di imaging nellindirizzare la diagnosi e nel guidare le procedure bioptiche , la maggior parte dei pazienti non richiede pi una toracotomia esplorativa prima della pianificazione del trattamento . ringraziamenti gli autori ringraziano , per gli importanti e competenti suggerimenti , i colleghi : f . 
of radiology , azienda ospedaliera universitaria , parma , italy 3dibimel , sezione di scienze radiologiche , universit di palermo , palermo , italy 4irccs santa lucia , roma , italy 5u.o. 
cademartiri , viale rustici 2 , i - 43100 parma , italy , tel . : + 39 - 052 - 1961833 , fax : + 39 - 052 - 1703381 , e - mail : filippocademartiri@hotmail.com received : 28 august 2004 / accepted : 5 march 2005 / published online : 11 april 2006 abstract conventional coronary angiography is the gold standard for the diagnosis of coronary artery anomalies . 
recently , the increasing performance of diagnostic techniques , such as electron beam tomography ( ebt ) , magnetic resonance ( mr ) and , more recently , multislice computed tomography ( msct ) , has enabled their application to cardiac imaging . 
we report the incidence and pathophysiology of coronary artery anomalies based on the capabilities of recent diagnostic tools with the aim of improving an accurate and noninvasive diagnostic approach . key words multislice computed tomography coronary artery anomalies magnetic resonance angiography electron beam tomography riassunto la coronarografia convenzionale rappresenta la tecnica di scelta per la diagnosi delle anomalie delle arterie coronarie . 
il loro riscontro , anche se in una percentuale molto bassa di individui , , nella maggior parte dei casi , occasionale durante lesecuzione di una coronarografia diagnostica nei pazienti con sospetta malattia coronarica ostruttiva . 
questultima , ricopre un ruolo importante nellimaging diagnostico coronarico grazie allelevata risoluzione temporale e spaziale raggiunte ed alla capacit di visualizzare in modo tridimensionale la complessa anatomia dei vasi epicardici . 
riportiamo lincidenza e la fisiopatologia specifica delle anomalie coronariche alla luce delle moderne tecniche diagnostiche , al fine di privilegiare , ove possibile , un approccio diagnostico accurato e non invasivo . parole chiave tomografia computerizzata multistrato anomalie delle arterie coronarie angiografia con risonanza magnetica tomografia ad emissione di elettroni introduction introduzione from the beginning of the 1990s , a variety of techniques other than conventional coronography ( cc ) have been used in diagnostic imaging of the coronaries [ 16 ]  . 
recently , multislice computed tomography ( msct ) has rapidly gained credibility thanks to the quality of the results obtained and its reproducibility in dallinizio degli anni novanta , diverse tecnologie , alternative alla coronarografia convenzionale ( cc ) , si sono affiancate nellimaging diagnostico delle coronarie [ 16 ]  . 
di recente , la tomografia computerizzata multistrato ( tcms ) ha rapidamente guadagnato credibilit per la qualit dei risultati ottenuti e per la loro rithe morphological assessment of coronary arteries [ 712 ]  . one of the strengths of msct of the coronaries is the threedimensional ( 3d ) visualisation of the epicardial vessels [ 13 ]  . for this reason , there has been much interest in the application of msct to assess coronary artery anomalies ( caas )  . the anatomical details and the physiopathological characteristics of most caas are not well known . 
although the medical community and the general public are increasingly aware that in special cases , caas can be fatal ( typically among young athletes under physical stress ) [ 14 ] , there are very few studies in the literature regarding their clinical significance , possible diagnostic protocol and the possibility of treatment and follow - up . 
the anatomical landmark shows the region of interest in an axial section at the level of the coronary artery origins from the left sinus of valsalva . the right coronary artery ( acd ) arises from the right sinus of valsalva and passes anteriorly in the right atrioventricular groove . 
the left coronary artery arises from the left sinus of valsalva and divides into the left anterior descending artery ( ada ) in the interventricular groove and the circumflex artery ( acx ) in the posterior atrioventricular groove . 
larteria coronaria sinistra ( acs ) , che origina dal seno di valsalva sinistro , dopo un breve tratto , si divide in arteria discendente anteriore ( ada ) , che si porta anteriormente , seguendo il decorso del solco interventricolare e arteria circonflessa ( acx ) che , invece , segue il decorso del solco atrio - ventricolare posteriore . 
per questa ragione , la tcms ha suscitato interesse nellapplicazione alla valutazione delle anomalie coronariche ( ac )  . i dettagli anatomici e le caratteristiche fisiopatologiche di gran parte delle ac non sono ben conosciute . 
sebbene la comunit medica e la popolazione siano sempre pi consapevoli che le anomalie coronariche possono , in casi particolari , essere fatali ( tipicamente nei giovani atleti durante sforzo fisico ) [ 14 ] , esistono solo pochi dati in letteratura sulla loro rilevanza clinica , sulleventuale protocollo diagnostico e sulle possibilit di trattamento e follow - up . 
 [ 15 ] , secondo la quale lac rappresenta un pattern coronarico con una caratteristica ( origine , numero , numero di ostii , decorso , etc . ) , che viene raramente riscontrata nella popolazione generale . epidemiologia in accordo con i dati riportati in letteratura , che si basano su reperti di angiografie eseguite per sospetta malattia ostruttiva coronarica , le ac coinvolgono circa l1 , 3% della popolazione generale [ 1618 ]  . 
i reperti autoptici , invece , forniscono unincidenza pi bassa : in 18.950 autopsie , alexander e griffith [ 19 ] hanno riscontrato solo 54 anomalie coronariche ( 0 , 3% )  . bisogna per considerare che le autopsie negli stati uniti non sono eseguite routinariamente , ma quasi esclusivamente per motivi medico - legali : dopo una morte violenta o avvenuta in ambiente non ospedaliero . 
inoltre , dal 1960 , il numero di autopsie per le morti in ospedale diminuito dal 50% al 10% [ 20 ] , motivo per cui , lincidenza delle ac fornita dagli studi autoptici risulterebbe poco affidabile [ 15 ]  . secondo uno studio effettuato da barriales villa et al . , che hanno rivalutato 13.500 coronarografie , riscontrando 75 pazienti con 75 anomalie coronariche , il sesso maggiormente interessato dalle ac sarebbe quello maschile ( 54 maschi vs 21 femmine ) [ 3 , 21 ]  . 
 [ 15 ] , which states that a caa is a coronary pattern with a characteristic ( origin , number , number of ostia , course , etc . ) which is rarely encountered in the general population . epidemiology according to data present in the literature , which are based on angiographic findings performed for suspected coronary obstructive disease , caas affect about 1.3% of the general population [ 1618 ]  . 
it should be borne in mind , however , that autopsies are not performed routinely in the united states but almost exclusively for medicallegal purposes after a violent death or death not in the hospital environment . 
in addition , since 1960 , the number of autopsies following death in hospital has fallen from 50% to 10% [ 20 ] , a reason for which the incidence of coronary anomalies provided by postmortem studies is somewhat unreliable [ 15 ]  . 
although they are rare , caas may be frequently present in association with other congenital heart diseases ( tetralogy of fallot [ 23 ] , transposition of the great arteries [ 24 ] , pulmonary atresia with intact ventricular septum [ 25 ] , rubella syndrome , hurlers syndrome and friedrichs ataxia [ 2630 ] )  . 
haemodynamically significant anomalies may induce angina pectoris , syncope , arrhythmia , myocardial infarct and sudden death and promote the onset and progression of coronary atherosclerosis [ 31 ]  . 
the study examining the largest number of cases , performed in north america at the cleveland clinic on 126 , 595 patients who underwent coronary angiography , reported a 1.3% incidence of caas ( 1 , 686 ) [ 18 ]  . 
while the cleveland study reported an 87% incidence for anomalies in the origin and course of the coronary arteries and 13% for coronary fistulas , the hunsottoposti ad angiografia coronarica per sospetta malattia ischemica , le ac sono pi comuni nelle donne ( 7 , 6% ) rispetto agli uomini ( 4 , 8% ) [ 15 , 22 ]  . sebbene rare , le ac possono frequentemente presentarsi in associazione con altre malattie congenite del cuore ( tetralogia di fallot [ 23 ] , trasposizione completa dei grossi vasi [ 24 ] , atresia della polmonare con setto interventricolare intatto [ 25 ] , sindrome della rubeola , sindrome di hurler e sindrome di friedrich [ 2630 ] )  . 
le anomalie che risultano emodinamicamente significative possono indurre : angina pectoris , sincope , aritmia , infarto miocardico , morte improvvisa e favorire linsorgenza e la progressione della malattia aterosclerotica coronarica [ 31 ]  . lo studio pi consistente dal punto di vista numerico , effettuato nel 1990 in nord america presso la cleveland clinic su 126.595 pazienti sottoposti ad angiografia coronarica , riporta una incidenza di ac dell1 , 3% ( 1.686 ) [ 18 ]  . 
mentre , nello studio della cleveland clinic lincidenza per le anomalie di origine e decorso delle arterie coronarie dell87% e per le fistole coronariche del 13% , in quello ungherese vengono riportati valori differenti , rispettivamente , del 95% e 5% [ 18 , 32 ]  . questa differenza nella frequenza e distribuzione delle anomalie congenite delle arterie coronarie pu essere attribuita ad un fattore genetico , come topaz et al . 
suggeriscono [ 33 ] : unarteria del cono indipendente pu essere identificata nel 27% dei pakistani , nel 38% dei britannici e nel 50% degli americani . nella popolazione giapponese , la frequenza di una origine separata dellarteria coronaria destra dal seno aortico di valsalva ( ad esempio , una dallarteria del cono e laltra dal tronco comune dellarteria coronaria destra ) solo del 10% [ 34 ]  . 
il 90% della popolazione cinese e di quella americana hanno nel circolo coronarico una dominanza destra [ 35 , 36 ]  . questi sono i risultati di due studi anatomo - patologici riportati da cheng ed effettuati da un gruppo di cardiologi cinesi a pechino e shanghai [ 36 ]  . 
 [ 32 ] , che hanno identificato , nel 52% dei casi valutati , una origine separata dellarteria coronaria discendente sinistra e dellarteria circonflessa nel seno coronarico sinistro ( ad esempio , assenza del tronco comune sinistro ) , mentre velican et al . 
 [ 42 , 43 ]  . classe i : ac benigne quelle pi frequenti di questo gruppo sono in genere silenti dal punto di vista clinico [ 18 ] e non sono state correlate allischemia miocardica o alla morte improvvisa , sebbene sia stata spesso riscontrata una loro associazione con diversi gradi di malattia aterosclerotica [ 31 , 44 ]  . 
il chirurgo , infatti , potrebbe erroneamente reciderla non conoscendone il decorso anomalo [ 38 ]  . la comunicazione intercoronarica una rara anomalia che si pu confondere con un vaso collaterale pervio , indicativo di una probabile ostruzione dellarteria coronaria . unorigine indipendente della discendente anteriore sinistra e della circonflessa pu essere relativamente frequente [ 15 ]  . 
la sua incidenza aumenta in caso di coesistenza di malattia valvolare aortica o dominanza sinistra . la pi frequente tra le ac considerata lorigine ectopica dellarteria circonflessa dallarteria coronaria destra o dal seno di valsalva destro . la sua rilevanza clinica correlabile alla possibilit di compressione durante un intervento chirurgico di sostituzione valvolare . 
 [ 45 ] in differenti sottotipi ( tipo iiv ) , in base alla distribuzione e al decorso nel solco interventricolare dei rami settali e diagonali , non associabile ad eventi sfavorevoli se non coesiste una malattia aterosclerotica [ 46 ]  . i ponti miocardici ( i.e. , myocardial bridges ) sono suddivisi in 5 gruppi ( da 1 a 5 ) a seconda della loro lunghezza ( < o > 1 cm ) e della riduzione di calibro durante la contrazione cardiaca ( < 25% , 50% o > 75% )  . 
varianti : acd che origina dal seno aortico anteriore sinistro , con decorso anomalo ( passando tra ap ed ao o posteriormente ) : acs che origina dal seno aortico anteriore destro , con decorso anomalo ( passa anteriormente o posteriormente allaorta o tra aorta ed arteria polmonare o presenta un decorso intramiocardico ) : arteria coronaria unica : la potenziale compressione di un singolo vaso coronarico se passa tra aorta ed arteria polmonare , pu provocare episodi ischemici , infarto miocardico e morte improvvisa acx che origina dal seno aortico anteriore destro o dal tratto prossimale della acd , con decorso anomalo ( posteriormente al decorso della ao ) : non emodinamicamente significativa . 
pu essere incidentalmente compressa durante una sostituzione valvolare acd , arteria coronaria destra ; acs , arteria coronaria sinistra ; acx , arteria coronaria circonflessa ; ada , arteria discendente anteriore ; ao , aorta ; ap , arteria polmonare f . 
right ventricle , right atrium , coronary sinus , superior vena cava , pulmonary artery , left atrium , left ventricle , multiple ( right and / or left ventricle ) rca , right coronary artery ; lca , left coronary artery ; lad , left anterior descending coronary artery ; lcx , left circumflex artery tion of congenital anomalies of the coronary arteries may be due to genetic factors , as topaz et al . 
multiple ostia in the right aortic sinus can be identified in another 10% of the same population ( 6% with three ostia and 4% with four )  . ninety percent of the chinese and american population have a right dominant coronary circulation [ 35 , 36 ]  . 
nelladulto questanomalia si pu associare ad ischemia miocardica , ad un pi elevato rischio di malattia coronarica e ad un sovraccarico cardiaco [ 50 ]  . la presenza di ununica arteria coronaria , distinta in diversi sottotipi r o l ( i - ii - iii ) , si associa ad ischemia miocardica per la inadeguata capacit di sostenere adeguatamente la normale circolazione coronarica [ 29 ]  . unulteriore ac da considerarsi benigna , sebbene in grado di provocare ischemia miocardica , latresia coronarica che , di solito , si associa ad altre malformazioni congenite tabella 3 anomalie dellanatomia intrinseca e della terminazione tipo di anomalia coronarica reperto anatomico rilevanza clinica anomalie dellanatomia intrinseca episodi ischemici miocardici a riposo f . 
if only the physiopathological and clinical consequences of caas are taken into account , this classification proves to be incomplete [ 41 ]  . there are a number of classifications in the literature that propose an anatomical and physiopathological approach to caas . 
this classification divides caas into four classes based on their clinical relevance ( table 1 ) , thus facilitating management and clinical follow - up . below is a summary of the main features of this classification . 
 [ 42 , 43 ]  . nei bambini con sindrome da rubeola , di hurler e di friederich [ 26 , 27 ]  . classe iii : associazione tra malattie coronariche e morte improvvisa le ac in quanto ad origine , decorso e distribuzione sono state , recentemente , ritenute la principale causa del 5%35% di morti improvvise nei giovani [ 50 ] , mentre una brusca ed acuta angolazione nel tratto prossimale di unarteria coronaria e la presenza di setti simili a delle valvole in prossimit del suo ostio , in assenza di malattia coronarica , possono essere la causa di una morte improvvisa [ 5153 ]  . 
il 19% delle morti improvvise nei giovani atleti sono da considerare imputabili alla presenza di una ac [ 43 ] , infatti , in presenza di una ac , un intenso sforzo fisico pu essere causa di morte improvvisa . i sottotipi di arterie coronarie uniche rappresentano una rara condizione nella quale la perfusione cardiaca totalmente affidata ad unarteria coronaria destra che origina f . 
its incidence increases with concomitant aortic valvular disease or left coronary artery dominance . the most common caa is probably the ectopic origin of the lcx from the rca or the right sinus of valsalva . 
quando presente questa ac il rischio di un evento fatale per il soggetto portatore elevato [ 54 , 55 ]  . il significato clinico dellorigine ectopica dellarteria coronaria sinistra dal seno di valsalva destro , dipende dalla sua posizione e dal decorso anatomico rispetto allaorta e allarteria polmonare . 
multiplanar reconstruction in an oblique coronal plane parallel to the long axis of the right coronary artery ( acd ) and the ectopic origin of the circumflex artery ( acx ) ( a )  . 
the acx first passes between the aortic root ( ao ) and the right atrium ( ad ) , and then passes between the ao and the left atrium ( as ) to enter the left atrioventricular groove ( b , arrowhead ) and to follow the lateral wall of the left ventricle . 
nelle immagini si pu anche apprezzare il tratto distale dellarteria circonflessa anomala che seguendo il decorso del solco atrio - ventricolare sinistro ( b , punta di freccia ) , subito dopo , si porta sulla parete laterale del ventricolo sinistro ( vs )  . 
panoramic three - dimensional ( 3d ) volume - rendering reconstruction of the heart shows the left anterior descending coronary artery ( ada ) that follows the anterior interventricular groove . 
the 3d volume - rendering and magnified multiplanar reconstructions in an orthogonal plane at the ada long axis ( 13 ) show the intramyocardial course of the artery ( 2 )  . 
vd , ventricolo destro ; vs , ventricolo sinistro ; ada , arteria coronaria discedente anteriore . basis of the distribution and course within the interventricular groove of the septal and diagonal branches , is not associated with unfavourable events in the absence of atherosclerosis [ 46 ]  . 
myocardial bridges are divided into five groups ( from 1 to 5 ) on the basis of their length ( < 1 or > 1 cm ) and their reduction in diameter during cardiac contraction ( < 25% , 50% or > 75% )  . 
the presence of a single coronary artery , which may be classified into subtypes r or l ( i - iiiii ) , is associated with myocardial ischaemia owing to the inability to adequately sustain normal coronary circulation [ 29 ]  . 
multiplanar reconstruction in a para - axial plane at the level of the origin of the right ( acd ) and left ( acs ) coronary arteries ( a )  . 
ricostruzione multiplanare sul piano assiale obliquo allemergenza ed al tratto prossimale delle arterie coronarie destra ( acd ) e sinistra ( acs ) dai rispettivi seni coronarici di valsalva ( a ) e ricostruzione 3d volume rendering panoramica del cuore ( b )  . 
hanno per primi suggerito che unarteria circonflessa anomala presenta un maggiore grado di stenosi rispetto alle arterie normali , ma la localizzazione ed il grado di stenosi nellarteria anomala non influenzano la sopravvivenza del soggetto [ 17 ]  . allo stesso modo , garg et al . 
 [ 33 ] , hanno rilevato unincidenza del 28%33% di malattia coronarica nelle arterie anomale e , soprattutto , unincidenza di malattia coronarica in pazienti con ac pari al 66%68% , suggerendo che queste due condizioni sono indipendenti . imaging non invasivo e metodi di screening sin ad oggi , la coronarografia convenzionale ha rappresentato la tecnica di scelta per la diagnosi delle anomalie coronariche [ 28 , 64 , 65 ]  . la diagnosi di ac stabilita , molto spesso , sulla base dellimpossibilit di trovare la coronaria nella normale sede anatomica e , quindi , di cateterizzarne lostio . negli ultimi anni si sono sviluppate altre tecniche nellimaging diagnostico cardiologico come , ad esempio , lecocardiografia transtoracica ( ett ) e transesofagea ( ete ) , langio - rm coronarica , la electron beam tomography ( ebt ) e la tcms [ 1 , 2 , 64 , 6669 ]  . ecocardiografia trans - esofagea e trans - toracica lett , che trova indicazione soprattutto in campo pediatrico , non sempre fornisce risultati diagnostici affidabili . 
caas are believed to be responsible for 19% of sudden death in young athletes [ 43 ] since intense physical activity in the presence of a caa may lead to sudden death . 
subtypes of single coronary arteries are a rare condition in which cardiac perfusion is performed entirely by a single rca , which arises from a normal left coronary artery , usually passing between the pulmonary artery and aorta . 
the clinical significance of the ectopic origin of the lad from the right sinus of valsalva depends on its position and anatomical course with respect to the aorta and the pulmonary artery . the septal subtype of these caas is the most commonly encountered whereas the between variety is rare but more dangerous [ 56 ]  . 
 [ 42 ] , patients with this anomaly have a high risk of malignant ventricular arrhythmias and require prompt treatment . the anomalous origin of the rca from the pulmonary artery is rare , and its clinical course is generally benign although it may be associated with sudden death , particularly after physical exertion [ 59 , 60 ]  . class iv : association between coronary artery anomalies and superimposed coronary artery disease there have been no studies to date that show that caas are more susceptible to coronary artery disease . 
 [ 61 ] found that an anomalous circumflex artery has an earlier and greater degree of atherosclerosis than a nonanomalous vessel . this predilection has been observed only in vessels arising from the right side with a retroaortic course [ 61 ]  . 
 [ 17 ] were the first to suggest that an anomalous circumflex artery has a greater degree of stenosis than normal arteries although the location and degree of stenosis in the anomalous artery do not influence survival of the subject . 
5 three - dimensional ( 3d ) volume - rendering reconstruction of the heart shows the anomalous origin and course of the right coronary artery ( acd )  . the anomalous artery arises as a separate vessel from the left sinus of valsalva . 
it then has an interarterial course between the aortic root ( ao ) and right ventricular outflow tract ( tevd ) to enter the right atrioventricular groove ( arrowhead )  . the anatomic landmark shows the coronary artery anomaly . 
5 anomalia coronaria destra ad origine dal seno coronario sinistro . ricostruzione 3d volume rendering del cuore nella quale si osserva lanomala emergenza dellarteria coronaria destra ( acd ) ed il suo anomalo decorso . 
lanomala arteria coronaria destra ( acd ) origina dal seno coronario sinistro e , passando tra aorta ascendente ( ao ) e tratto di efflusso del ventricolo destro ( tevd ) , segue il decorso del solco atrio - ventricolare destro ( punta di freccia )  . in basso a sinistra schematizzata lanomalia descritta . 
tevd , tratto di efflusso del ventricolo destro ; ao , aorta ascendente ; ad , atrio destro ; as , atrio sinistro ; vs , ventricolo sinistro . riportiamo lesperienza di davis et al . 
the diagnosis of a caa is often established on the impossibility of finding the coronary arteries in their normal anatomical position and therefore to catheterise the ostiu in recent years , other techniques in cardiologic diagnostic imaging have been developed , such as transthoracic echocardiography ( tte ) , transoesophageal echocardiography ( tee ) , magnetic resonance angiography ( mra ) , electron beam tomography ( ebt ) and msct [ 1 , 2 , 64 , 6669 ]  . transthoracic and transoesophageal echocardiography tte , which is used mainly in paediatric radiology , does not always provide reliable diagnostic results . 
although this technique is able to identify the course of and territory supplied by caas , and after colour doppler integration supply information regarding the direction of blood flow [ 70 , 71 ] , it has some important shortcomings . 
when performed on adult patients , it proves difficult to obtain diagnostic images owing to the interposition of the bones of the ribcage ( ribs and sternum ) , pulmonary parenchyma and subcutaneous adipose tissue [ 5 , 72 ]  . 
nella ricerca e valutazione dellorigine delle arterie coronarie , la rm pu fornire informazioni pi complete rispetto allangiografia convenzionale , specialmente nei pazienti con altre anomalie cardiache congenite concomitanti [ 1 , 7577 ]  . 
la maggiore limitazione dellangio - rm consiste nellincompleta visualizzazione dei vasi coronarici , in particolar modo dei loro tratti distali . questo ne limita lutilizzo a scopo diagnostico per la valutazione delle fistole , dellorigine delle arterie coronarie diversa dai seni aortici ( i.e. , da un ventricolo o dallarteria polmonare ) e dei vasi collaterali . electron beam tomography la electron beam tomography ( ebt ) , utilizzata estensivamente per la valutazione del calcio coronarico [ 7881 ] , sfrutta una elevata risoluzione temporale ( 50100 ms ) e la sincronizzazione prospettica della scansione in apnea con lecg . 
questo permette di ridurre gli artefatti da movimento cardio - respiratorio e la dose assorbita dal paziente [ 2 ]  . sulla base di queste caratteristiche stato riconosciuto il razionale per limpiego clinico nellimaging vascolare cardiaco [ 82 , 83 ]  . uno dei primi gruppi a studiare la possibilit di valutare le anomalie coronariche ed il loro decorso mediante ebt stato quello di ropers et al . 
le maggiori limitazioni allutilizzo dellebt nella pratica clinica sono lelevato costo dellapparecchiatura e la limitata diffusione sul territorio nazionale ( si contano ad oggi circa 150 scanner ebt nel mondo , due terzi dei quali negli stati uniti )  . coronary magnetic resonance angiography tomografia computerizzata multistrato mra [ 1 , 7577 ] is a highly promising technique since no ionising radiation is used . 
in the study of the origin of the coronary arteries , mra can provide more complete information than conventional angiography , particularly in patients with other concomitant congenital cardiac anomalies [ 1 , 7577 ]  . the main limitation of mra is incomplete visualisation of the coronary vessels , particularly their distal tracts . 
laccuratezza diagnostica di questa metodica ed il suo verosimile utilizzo estensivo consentiranno di apprezzare la prevalenza delle ac nelle differenti popolazioni . i vantaggi della tcms risiedono essenzialmente nellelevata accuratezza diagnostica ed anatomica . 
these characteristics reduce cardiac - respiratory motion artefacts and the dose absorbed by the patient [ 2 ]  . this has been the basis for the techniques clinical use in cardiac vascular imaging [ 82 , 83 ]  . one of the first groups to study the possibility of assessing caas and their course with ebt was ropers et al . 
ebt therefore has a relatively high diagnostic accuracy in the study of caas with a limited radiation exposure estimated at 1.1 msv [ 84 ]  . the main limitations to the use of ebt in clinical practice are the high costs of equipment and the limited number of scanners in italy ( there are approximate 150 in the world , two thirds of which are in the united states )  . multislice computed tomography in a few short years , msct has revolutionised coronary diagnostics by highlighting the feasibility of a noninvasive approach . 
the diagnostic accuracy of the technique and its likely widespread use excellently place it to appreciate the prevalence of caas in different populations . the advantages of msct lie primarily in its high level of diagnostic and anatomical accuracy . 
the complex and tortuous coronary anatomy can be readily visualised with msct [ 13 ]  . despite the excellent results , even this technique suffers from a series of limitations . 
multiplanar reconstructions with maximum intensity projections ( mip ) of the anomalous left coronary artery ( acs ) in a para - axial ( a ) and coronal oblique ( b ) plane . 
the anomalous acs then runs anteriorly and on the left , passing below the right ventricular outflow tract ( tevd ) within the myocardium ( a , b , arrowheads )  . 
ricostruzioni multiplanari con proiezione di massima intensit ( mip ) dellarteria coronaria sinistra ( acs ) anomala su un piano para - assiale ( a ) e coronale obliquo ( b )  . 
la acs nasce dal seno coronario di destra e si porta anteriormente e verso sinistra , passando al di sotto del tratto di efflusso del ventricolo destro ( tevd ) , nel contesto del muscolo cardiaco ( punte di freccia in a e b )  . 
knowledge of the characteristics and consequences of different types of anomalies enables the radiologist to appropriately assess the finding . the indication of performing a noninvasive coronographic examination for suspected caa or to exclude the presence of a caa must be carefully considered in cooperation with the clinic in order to avoid exposing young patients to excessive ionising radiation . conclusioni le anomalie coronariche sono un reperto relativamente frequente nel contesto dellimaging diagnostico non invasivo coronarico . la conoscenza delle caratteristiche e delle conseguenze dei differenti tipi di anomalie permette al medico radiologo di giudicare in modo adeguato il reperto . 
passariello1 1dipartimento di scienze radiologiche , universit degli studi di roma la sapienza , viale regina elena 324 , i - 00161 roma , italy 2sezione di statistica , 3oncologia medica , dipartimento di medicina sperimentale e patologia , universit degli studi di roma la sapienza , roma , italy correspondence to : f . 
the aim of this study was to assess the efficacy of a computer - aided detection ( cad ) system in the identification of lung metastases and to compare the volumetric cad measurements with unidimensional observer measurements in the evaluation of treatment response in oncology patients . 
multislice ct scans were performed before and after the injection of contrast material with a high - resolution protocol ( collimation 4x1 mm , 100 mas , 120 kv )  . 
tutti gli esami sono stati eseguiti prima della somministrazione di mdc , con un protocollo di tc multistrato ( tcms ) ad alta risoluzione del torace ( collimazione 4x1 mm , 100 mas , 120 kv )  . 
successivamente , i noduli , identificati come lesioni target ( noduli pi significativi presenti sia prima che dopo chemioterapia ) , sono stati rivalutati mediante un sistema computerizzato in grado di effettuare il calcolo del volume della lesione . 
ventiquattro noduli ( dt : 518 mm nel primo studio e 420 mm nel follow - up ) sono stati inclusi in questa valutazione . gli osservatori hanno espresso un giudizio di risposta alla terapia sovrapponibile in 21 noduli : 8 considerati aumentati e 13 stabili . le misurazioni degli osservatori e le misurazioni automatiche fornite dal sistema cad differivano in 3 noduli : due considerati stabili dai radiologi e aumentati dal cad e uno considerato aumentato dai radiologi e stabile dal cad . 
computed tomography ( ct ) and , in particular , multislice technology , has long been considered a highly sensitive method for identification of lung metastases and evaluation of response to therapy during oncologic follow - up examinations ; in fact , its high spatial resolution and high contrast resolution at the level of the lung parenchyma make it an essential diagnostic tool in oncologic patients undergoing chemotherapy . the international criteria that define oncologic response were initially established in the 1980s by the world health organisation ( who ) [ 3 ] and recently modified as response evaluation criteria in solid tumours ( recist ) criteria [ 4 ]  . recist criteria only take into consideration the largest diameter of the significantly more important lesions ( five for each organ ; up to ten per patient in the case of multiorgan secondary lesions ) and subdivide response to therapy into four categories : stable disease , when there is a < 30% reduction or < 20% increase in maximum diameter or in the sum of diameters of more than one lesion ; partial response , when there is a > 30% reduction ; progressive disease , when there is a > 20% increase ; complete response , in the case of complete tumour disappearance [ 4 ]  . although they are simple and easy to use , these criteria present some limitations in clinical practice , namely : difficulty in measuring the lesion ( extremes of the lesion in the axial plane ) ; different slice thickness used in successive exams ( often performed in different facilities or with different devices ) ; ill - defined lesion margins ; type of measurement performed ( manual or electronic ) ; selection of the target lesions . 
a consequence of these limitations is often high intraand interobserver variability , with a highly variable judgement of response to therapy both between the different observers who evaluate follow - up studies and for the same observer reevaluating previous exams [ 58 ]  . 
in science , this variability is often avoided by consensus : readings by two or more observers , and calculation of the mean among all readings ( or , in this case , among measurements ) ; in practice , however , this is often not possible . one alternative proposed in identification of lung nodules and their measurement is the utilisation of computerised reading devices , which map the lesions and measure their volume . 
at present , these computer - aided detection ( cad ) il ruolo della diagnostica per immagini in oncologia andato ampliandosi negli ultimi anni , sia per lidentificazione e stadiazione della neoplasia primitiva , sia nella rivalutazione dei pazienti in corso di trattamenti chemioo radioterapici [ 1 , 2 ]  . 
la tc , ed in particolare la nuova tecnologia multistrato , gi da tempo considerata tecnica di elevata sensibilit nella identificazione delle metastasi polmonari e nella valutazione della risposta alla terapia nel corso dei follow - up oncologici ; infatti , lelevata risoluzione spaziale , associata alla elevata risoluzione di contrasto a livello del parenchima polmonare , ne consentono un essenziale strumento diagnostico in pazienti oncologici in corso di chemioterapia . i criteri internazionali che definiscono la risposta oncologica sono stati inizialmente definiti negli anni 80 dalla who [ 3 ] e recentemente modificati come criteri recist [ 4 ]  . 
i criteri recist prendono in considerazione unicamente il diametro maggiore delle lesioni significativamente pi importanti ( 5 per organo ; fino ad un massimo di 10 per paziente , nel caso in cui le lesioni secondarie siano multiorgano ) , suddividendo la risposta alla terapia in 4 differenti categorie : stabilit di malattia , nel caso in cui vi sia una riduzione inferiore al 30% o un incremento inferiore al 20% del diametro massimo o della somma dei diametri di pi lesioni ; risposta parziale , nel caso in cui la riduzione sia superiore al 30% ; progressione di malattia , nel caso di un incremento superiore al 20% ; risposta totale , nel caso di scomparsa totale della lesione [ 4 ]  . sebbene semplici e di facile utilizzo , i limiti di applicabilit nella pratica clinica sono rappresentati dalla difficolt di misurazione ( estremi massimi di lesione sul piano assiale ) , dal diverso spessore di strato utilizzato tra esami successivi ( spesso eseguiti in strutture o con apparecchiature diverse ) , dai margini di lesione non ben definibili , dal tipo di misurazione effettuata ( manuale o elettronica ) , dalla scelta delle lesioni target . 
conseguenza di tali limiti spesso rappresentata da unalta variabilit intraed interosservatore , con un giudizio di risposta alla terapia ampiamente variabile sia tra diversi osservatori che valutano studi successivi , sia nellosservatore stesso quando si trovi a rivalutare esami precedenti [ 58 ]  . 
during a 14 - month period ( january 2004 to march 2005 ) , 67 oncologic patients from the department of clinical oncology ( age range : 3562 years ) undergoing chemotherapy were evaluated using a four - detector - row multislice ct ( msct ) scanner ( volume zoom , forcheim , germany )  . to create a database , we included only patients undergoing chemotherapy with a diagnosis of lung metastasis on the first examination and a ct scan performed during the two chemotherapy cycles . 
exclusion criteria were : patients with studies performed with different acquisition protocols ; patients who did not have lung metastases at the first study ; those who did not have a complete response at the second study ( absence of nodular formations within the lung parenchyma )  . 
thus , nine patients with breast cancer were selected for our database . the acquisition protocol we used was the so - called combi - mode , with the following technical features : 4x1 - mm collimation , 100 mas , 120 kv . 
a una delle alternative proposte nella identificazione dei noduli polmonari e nella loro misurazione lutilizzo di sistemi di lettura computerizzati ; essi forniscono , infatti , una mappa delle lesioni ed una loro misurazione volumetrica . allo stato attuale , tali sistemi , denominati cad , vengono applicati principalmente alla valutazione dei noduli polmonari , sia nella loro identificazione , sia per la quantificazione del tempo di crescita in studi successivi [ 911 ]  . lo scopo del nostro studio stato provare a integrare tali sistemi nella valutazione dei pazienti oncologici , identificando eventuali differenze tra una lettura effettuata da diversi osservatori ed una valutazione volumetrica effettuata con il nostro sistema computerizzato . materiali e metodi popolazione di pazienti e protocollo di acquisizione lo studio da noi proposto uno studio retrospettivo ; per la raccolta dati e per lelaborazione degli stessi stata comunque richiesta lautorizzazione da parte del comitato etico . durante un periodo di 14 mesi ( gennaio 2004 , marzo 2005 ) , 67 pazienti oncologici ( et compresa tra 35 e 62 anni ) , provenienti dal dipartimento di oncologia clinica ed in corso di trattamento chemioterapico , sono stati valutati utilizzando un apparecchiatura di tc multistrato ( tcms ) a 4 banchi di detettori ( volume zoom , forcheim , germany )  . nella creazione del database sono stati inclusi nello studio unicamente i pazienti in corso di chemioterapia , con una diagnosi di metastasi polmonari al primo controllo e con una tc eseguita durante due cicli di chemioterapia . 
criteri di esclusione sono stati : pazienti con studi effettuati con protocolli di acquisizione diversi ; pazienti che non presentavano metastasi polmonari nel primo studio o con una risposta completa nel secondo studio ( assenza di formazioni nodulari nel parenchima polmonare )  . 
lobiettivo per linclusione stato di valutare sia lutilizzo di un sistema computerizzato , sia la risposta ad un determinato chemio farmaco per i pazienti oncologici . sono stati cos selezionati , nel nostro database , 9 pazienti con tumore della mammella . il protocollo di acquisizione stato condotto utilizzando una tecnica definita combi con le seguenti caratteristiche tecniche : collimazione 4x1 mm , 100 mas , 120 kv . 
lo spessore di strato utilizzato stato di 1 , 25 mm con un intervallo di ricostruzione di 1 mm ed algoritmo di ricostruzione b60 per lo studio del parenchima ; la valutazione del mediastino stata effettuata utilizzando ricostruzioni con spessore di strato di 5 mm e con algoritmo b30 . la scansione iniziale sul parenchima polmonare stata effettuata nelle sole condizioni basali ; successivamente le pazienti sono state valutate per un follow - up completo con un esame tc completo di torace - addome - pelvi e , dove richiesto , del cranio , dopo iniezione di mezzo di contrasto organo iodato non ionico . 
in order to reduce any intraand interobserver variability , nodule images were enlarged by 150%200% . the third radiologist then measured ( based on the numerical measurement provided by each observer ) the percentage difference between the single lesions , using the recist criteria , and providing a general opinion on disease improvement , worsening or stability , considering both response of the single nodules and response for each patient , summing the size of every single nodule . 
thus , 24 metastases were considered in the first reading and 24 in the second . statistical analysis in the evaluation of response to treatment , the recist criteria were taken into consideration ( both for single nodules and for each patient )  . 
in agreement with volumetric measurements , partial response was defined as > 65% reduction ; progressive disease was defined as one having > 73% volume increase ; stable disease was defined as one having < 73% increase and < 65% reduction ( table 1 ) [ 12 ]  . 
reading table 1 treatment response categories state trasferite sul nostro sistema di archiviazione pacs ( lifeweb , ferrania imaging technologies )  . selezione delle metastasi tutti i casi selezionati sono stati trasferiti su una console dedicata fornita di un sistema computerizzato di identificazione dei noduli polmonari ( lungcheck , r2 technology , inc )  . 
in un primo momento la lettura dei casi avvenuta in consensus tra due radiologi , ponendo a confronto su un doppio monitor il primo studio ed il follow - up , per identificare le lesioni target su cui successivamente effettuare le misurazioni.un terzo radiologo , non incluso nella valutazione dei casi , ha creato il database , registrando su una tabella la sede delle lesioni target scelte dai radiologi . successivamente , a distanza di una settimana , i due radiologi , singolarmente , hanno valutato le dimensioni delle lesioni prescelte secondo lasse massimo trasversale di ogni lesione ; per ridurre leventuale variabilit di misurazione intra ed interosservatore , le immagini dei noduli sono state ingrandite del 150%200% . il terzo radiologo ha quindi calcolato ( sulla risposta numerica di misurazione fornita da ciascun osservatore ) la percentuale di differenza tra le singole lesioni , utilizzando i criteri recist e fornendo quindi un giudizio complessivo di miglioramento , peggioramento e stabilit di malattia , considerando sia la risposta per singoli noduli , sia la risposta per paziente , effettuando la somma delle dimensioni di ogni singolo nodulo . 
nei casi di disaccordo nella valutazione della risposta stata effettuata una seconda lettura in consensus . category unidimensional criteriaa volumetric criteriab complete response tumour disappearance tumour disappearance partial response stable disease > 30% reduction in diameter > 65% reduction in volume size between that for partial and progressive disease size between that for partial and progressive disease progressive disease > 20% increase in in diameter > 73% increase in volume abased on response evaluation criteria in solid tumours ( recist ) guidelines . 
in patients with multiple lesions , individual maximum diameters were summed bbased on recist guidelines tabella 1 categorie di risposta al trattamento categorie criteri unidimensionalia criteri volumetricib risposta completa scomparsa delle lesioni scomparsa delle lesioni risposta parziale riduzione > 30% del diametro massimo riduzione > 65% del volume stabilit di malattia dimensioni comprese tra risposta parziale e progressione di malattia dimensioni comprese tra risposta parziale e progressione di malattia progressione di malattia aumento > 20% del diametro massimo aumento > 73% del volume asecondo i criteri recist . 
thus , kappa - type statistics were used to determine very poor ( k < 0.01 ) , poor ( k 0.010.20 ) , moderate ( k 0.210.40 ) , good ( k 0.410.60 ) , very good ( k 0.610.80 ) and excellent ( k 0.811.00 ) agreement [ 13 ]  . 
considering results for each patient , there was one case of disagreement between the radiologists , who stated the patient was stable , and cad , which revealed disease progression . 
consensus results between the observers and between cad and the observers are shown in table 4 . discussion an objective evaluation of response to therapy in oncologic patients is an important goal in routine radiological activity both concerning clinical decisions on patient treatment and trials on new chemotherapeutic agents [ 2 ]  . 
in the past few years , assessment and follow - up of oncologic patients has successivamente , i tre radiologi in consensus hanno valutato le dimensioni volumetriche effettuate dal sistema computerizzato ed hanno valutato la risposta alla terapia , anche in questo caso sia per nodulo che per paziente . 
sono state cos prese in considerazione 24 metastasi nella prima lettura e 24 nella seconda lettura . analisi statistica nella valutazione della risposta al trattamento sono stati presi in considerazione i criteri recist ( sia per i noduli singoli , sia per paziente )  . 
in accordo con le misurazioni volumetriche , la risposta parziale stata definita come una riduzione superiore al 65% ; la progressione di malattia come aumento del volume superiore al 73% ; la stabilit di malattia come aumento inferiore al 73% e diminuzione inferiore al 65% ( tabella 1 ) [ 12 ]  . i risultati delle letture sono stati inseriti in un foglio di lavoro excel e valutati , utilizzando un programma statistico ( spss 8.0 per windows ; spss ; chicago , iii ) , in termini di accordo inter - osservatore e di concordanza tra le misurazioni del singolo osservatori con i criteri recist e le misurazioni volumetriche del cad . bassa ( k < 0 , 01 ) , ( k = 0 , 010 , 20 ) , stata cos utilizzata una statistica k per determinare scarsa discreta ( k = 0 , 210 , 40 ) , buona ( k = 0 , 410 , 60 ) , sostanziale concordanza ( k = 0 , 610 , 80 ) e concordanza quasi perfetta ( k = 0 , 811 , 00 ) [ 13 ]  . 
per ogni test statistico effettuato stato definito come parametro di significativit un limite di p < 0 , 005 . risultati ventiquattro noduli sono stati inclusi in questa valutazione . il diametro dei noduli valutati risultato compreso tra 5 e 18 mm nel primo studio e 4 e 20 mm nel follow - up . 
considerando i risultati per paziente , in un caso si avuta una discordanza di valutazione tra i radiologi , per i quali il paziente era stabile , e il cad , per il quale cera stata una progressione di malattia . 
1a , b metastatic lung nodule in right upper lobe , evaluated with two multislice computed tomography ( msct ) studies before and after chemotherapy . agreement between the first ( a ) and second observer ( b ) in evaluation of therapy response . 
based on response evaluation criteria in solid tumours ( recist ) criteria , both radiologists considered the disease as stable . fig 1a , b nodulo polmonare di natura secondaria localizzato a livello del lobo superiore del polmone di destra , valutato con due esami tcms prima e dopo chemioterapia . 
a case of disagreement between the two observers : the first ( a ) considered the nodule decreased in size while the second ( b ) considered the nodule as stable after therapy . 
il consensus , effettuato in un secondo momento , ha classificato il nodulo come stabile dopo terapia . marked improvement in survival and quality of life ; second , greater availability of increasingly sophisticated ct scanners , which results in a rise in requests for radiological examinations . 
these fundamentals result in a need to evaluate an increasing number of ct exams and in particular to study , even at short time intervals , exams of oncologic patients undergoing chemotherapy or actinic therapy . in spite of the growing diagnostic reliability of latest - generation scanners in diagnosis and staging , the large number of exams to be read and compared with previous exams often performed with different imaging techniques raises the issue of objective variability of opinions [ 7 ]  . 
nevertheless , as revealed in clinical practice and reported in our study , interobserver variability , even on a limited number of patients and with readers asked to define a response to therapy , proved to be wide and , in our study , involved two out of nine patients . 
in fact , according to recist criteria , measurement of the greatest transverse diameter of a lesion involves the obvious limitation of selecting the slice on which to perform the measurement [ 5 ] ; furthermore , although metastatic lung diseases generally consist of often spherical nodular masses , eccentric growth in the tra le molteplici ragioni di questo incremento nel numero di esami vi sono certamente due fondamenti . 
primo , terapie pi aggressive , con farmaci antiblastici di maggior successo nelle forme secondarie , con una prognosi per il paziente maggiormente favorevole ed un netto miglioramento della durata e della qualit di vita . 
il risultato che ne deriva rappresentato dalla necessit di valutare un numero crescente di esami tc ed in particolare di valutare , spesso a distanze ravvicinate , esami di pazienti oncologici in corso di terapie chemioterapiche o attiniche . 
nonostante la sempre maggior affidabilit diagnostica delle apparecchiature di ultima generazione nella diagnosi e stadiazione , lelevato numero di esami da dover giornalmente valutare , ponendo a confronto esami precedenti , peraltro spesso eseguiti con tecniche di studio diverse , pone il radiologo di fronte ad una oggettiva variabilit di giudizio [ 7 ]  . uno dei sistemi adottati nel nostro dipartimento per la valutazione di tutti i pazienti oncologici e per ridurre la variabilit intra ed interosservatore di utilizzare protocolli standard , e quindi riproducibili e confrontabili negli studi successivi . nonostante ci , cos come evidenziato nella pratica clinif . 
questi sistemi hanno dimostrato una ampia affidabilit diagnostica , con valori di sensibilit superiori al 90% e superiori alla valutazione dello stesso radiologo [ 911 ]  . una della caratteristiche tecniche di questi sistemi la valutazione automatica delle dimensioni del nodulo in termini di volume , consentendo quindi di comparare studi diversi ; lutilizzo di tali sistemi computerizzati allo stato attuale stato limitato alla identificazione dei noduli polmonari e alla valutazione del tempo di crescita . 
both observers agreed in classifying the nodule as progressive disease according to response evaluation criteria in solid tumours ( recist ) criteria ( a , b ) ; computer - aided detection ( cad ) volumetric measurements classified the disease as stable ( c )  . fig 3a - c metastasi polmonare localizzata a livello del lobo medio del polmone di destra . 
i due radiologi ( a , b ) concordavano , in accordo con i criteri recist , sulla progressione di malattia , mentre le misurazioni volumetriche effettuate dal cad consideravano stabile la patologia secondaria dopo terapia ( c )  . longitudinal plane is not uncommon [ 2 ]  . 
this leads to interobserver variability among measurements and , therefore , an overor underestimation of response to therapy according to recist criteria . several authors have evaluated the role of three - dimensional ( 3d ) measurements of lung nodules and liver metastases ; results provided by volumetric measurements present , in some cases , considerable differences from uniand bidimensional measurements , in particular when the lesion margins are ill defined [ 12 , 14 ]  . 
nonetheless , one limitation of using a method for volumetric measurement is the long time needed to calculate the volume , mainly due to the manual drawing of the lesion edges ; furthermore , small or ill - defined lesions are often associated with manual errors in volume calculation [ 15 ]  . the aim of our study was to apply a computerised system capable of automatically performing a volumetric measurement of a lesion to the evaluation of oncologic patients with f . 
one technical features of these systems is automatic assessment of nodule size in terms of volume , which allows for comparison between different studies ; at present , use of these techniques is limited to identification of lung nodules and assessment of their growth pattern . 
this role has proved to be extremely significant , providing better evaluation of volumetrically increased nodules that remain stable in the transverse plane [ 16 ]  . in our study , we took into consideration interobserver consensus , thus obtaining fair agreement between the response to therapy assessed by the observers and that assessed through the measurement ; nevertheless , the observers recorded three cases in which images had to be reevaluated to reach a consensus . 
this means that interobserver variability plays an important role in establishing therapy success . on the other hand , other authors have shown that volume measurement by a computerised system is reliable and reproducible among different studies [ 17 ]  . 
thus , the possibility of evaluating response to therapy using a computerised technique able to provide volumetric results represents valuable support for the radiologist , as it reduces reading times and provides more objective evaluation , even for lung metastases . conclusions cad volumetric measurements easily allow for objective , reproducible and automated volume measurement , thus limiting interobserver variability in evaluation of response to treatment of oncologic patients . 
furthermore , a different selection of more spherical or irregular metastases could modify results of our volumetric measurement , leading to greater agreement or disagreement between observers and cad . thus , our study only presents preliminary results and aimed at assessing the possibility of using computerised techniques even in the evaluation of response to treatment of oncologic patients . 
a second limitation found in the daily application of these systems is the need to use thin - collimation protocols , indispensable for cad image processing , which lead to difficult comparisons with exams performed in other centres and with different protocols . 
for this reason , our study had to be retrospective , performed only on patients who had undergone high - resolution exams that could be analysed by cad . two considerations need to be made about this limitation : first is that the need to use thin - slice protocols for correct evaluation of lung nodules has recently been demonstrated gliorare la valutazione di noduli cresciuti volumetricamente , ma stabili su un piano di misurazione trasversale [ 16 ]  . nel nostro studio , prendendo in considerazione il consensus tra gli osservatori , si ottenuta una buona concordanza tra la risposta alla terapia dei lettori e quella fornita da una misurazione volumetrica ; nonostante ci , tra gli osservatori vi sono stati 3 casi in cui le immagini sono state rivalutate per raggiungere un accordo . ne consegue che la variabilit interosservatore gioca un ruolo importante nello stabilire il corretto andamento di una terapia . di contro , la valutazione del volume di un sistema computerizzato stata dimostrata da altri autori essere invece una misura affidabile e quindi riproducibile nella comparazione tra i diversi studi [ 17 ]  . la possibilit di valutare la risposta alla terapia utilizzando un sistema computerizzato , in grado di fornire risultati volumetrici , rappresenta , quindi , un valido ausilio per il radiologo , riducendo il tempo di lettura e fornendo una valutazione maggiormente oggettiva anche per le metastasi polmonari . conclusioni le misurazioni volumetriche effettuate dal cad consentono con facilit una misurazione oggettiva , riproducibile ed automatica in termini volumetrici , riducendo , quindi , la variabilit interosservatore nella valutazione della risposta al trattamento dei pazienti oncologici . il nostro studio presenta alcune limitazioni , prima fra tutte il limitato numero di pazienti e di metastasi valutate . 
 [ 5 ] ; the second consideration concerns the increasing use of multislice ct scanners , with collimations that are either fixed or variable to less than 1 mm , that allow for storage on increasingly sophisticated pacs systems of submillimetre raw data that can thus be used by cad systems . the final limitation is that cad could be unable to identify all nodules chosen as target lesions . 
in our study , this did not happen , as cad identified all nodules selected as target lesions ; however , it is still possible to manually add a lesion not identified by cad on which the system can perform the same volumetric measurement . integration of new systems capable of automatically comparing two studies on different screens and providing the percentage of variation of a lesion paves the way for routine use of cad systems , even in evaluation of lung metastases , as well as representing a valuable second reading in screening programmes and identification of lung nodules . mm , con possibilit di archiviare su sistemi pacs sempre pi performanti i dati grezzi submillimetrici , utilizzabili quindi anche dai sistemi cad . infine , unultima limitazione che il cad potrebbe non identificare tutti i noduli scelti come lesioni target . 
nel nostro studio ci non si verificato , avendo il cad identificato tutte le formazioni nodulari prescelte come lesioni target ; nonostante ci , possibile aggiungere manualmente una lesione non identificata dal cad , su cui viene eseguita dal sistema la stessa misurazione volumetrica . 
lupattelli3 1dipartimento di patologia umana ed oncologia , sezione di radiologia oncologica , medicina nucleare e radioterapia , universit degli studi di siena , policlinico santa maria alle scotte , viale bracci 2 , i - 53100 siena ( si ) , italy 2radiologia universitaria , azienda ospedaliera universitaria senese , italy 3dipartimento di scienze chirurgiche , radiologiche , odontoiatriche e medico - legali , universit degli studi di perugia , italy 4ge healthcare , italy correspondence to : l . 
the purpose of this study was to test the reproducibility of the three - dimensional ( 3d ) advanced lung analysis software ( 3d - ala , ge healthcare ) in the estimation of pulmonary nodule volume . 
we retrospectively reviewed the unenhanced multislice ct scans ( lightspeed pro 16 ge ) of 77 patients with a solitary pulmonary nodule ( n = 71 ) or metastatic pulmonary disease ( n = 6 )  . 
the following acquisition parameters were used : slice thickness 0.625 mm , reconstruction interval 0.4 mm , pitch 0.562 : 1 , 140 kv , 300 mas , field of view 13 cm , bone kernel . for each of the 103 nodules three , 3d volume measurements were obtained by the 3d - ala software . 
the reproducibility of nodule segmentation was evaluated according to a visual score ( 1 = optimal , 95% ; 2 = fair , 9095% ; 3 = poor , 90% ) by three observers working in consensus . 
ala - 1 software allowed segmentation in all nodules ( type 1 segmentation n = 43 , type 2 n = 35 , type 3 segmentation n = 25 )  . 
sono stati analizzati retrospettivamente gli esami tc multistrato ( lightspeed pro 16 ge ) , senza mdc per vena di 77 pazienti ( 71 con noduli polmonari solitari e 6 con noduli secondari )  . 
i parametri di acquisizione utilizzati per il calcolo volumetrico sono stati i seguenti : spessore di strato 0 , 625 mm , intervallo di ricostruzione 0 , 4 mm , pitch 0 , 562 : 1 , 140 kv , 300 mas , fov 13 cm , algoritmo di ricostruzione ad elevata risoluzione spaziale . 
per ciascun dei 103 noduli , impiegando il software ala1 , sono state effettuate tre misurazioni volumetriche . tre osservatori in consensus , in ogni misurazione , hanno assegnato alla segmentazione dei contorni di ciascun nodulo , un punteggio visivo ( 1 = ottimo , 95% ; 2 = discreto , 9095% ; 3 = scarso , 90% )  . 
tale software ha consentito una segmentazione di tipo 1 in 43 noduli , una segmentazione di tipo 2 in 35 noduli ed una segmentazione di tipo 3 in 25 noduli . 
il calcolo volumetrico risultato identico , nelle tre misurazioni consecutive , in 62 dei 103 noduli : 16 dei 19 noduli circoscritti ( 84 , 2% ) , 31 dei 45 noduli iuxta - vascolari ( 68 , 8% ) e 15 dei 39 noduli iuxta - pleurici ( 38 , 4% )  . ala1 non ha effettuato una ricostruzione riproducibile in termini di volume in 41 dei 103 noduli , di cui 3 dei 19 ( 15 , 7% ) circoscritti , 14 dei 45 ( 31 , 1% ) iuxta - vascolari , 24 dei 39 ( 61 , 5% ) iuxta - pleurici e dei quali 2 su 41 ( 4 , 8% ) sono stati segmentati dal software con qualit 1 , 15 su 41 ( 36 , 5% ) con qualit 2 ed infine 24 su 41 ( 58 , 5% ) con qualit di segmentazione pari a 3 . 
il calcolo volumetrico con il software ala1 riproducibile per tutti i noduli in riferimento alle dimensioni e al tipo . il software ala1 ha consentito un calcolo volumetrico affidabile e riproducibile nei noduli circoscritti e nella maggior parte dei noduli iuxta - vascolari . 
relativamente ai noduli iuxta - pleurici , in particolare quelli adiacenti alla pleura diaframmatica , la riproducibilit del calcolo volumetrico non ancora sufficiente e necessita di miglioramenti tecnici . parole chiave tomografia computerizzata multistrato nodulo polmonare solitario introduction introduzione characterisation of pulmonary nodules , above all those measuring 510 mm , is difficult if not impossible with positron emission tomography ( pet ) , multiphasic dynamic computed tomography ( ct ) or percutaneous needle biopsy [ 13 ]  . 
with the exception of completely calcified nodules and / or fat - containing nodules , which are considered benign , all other nodules are to be considered potentially malignant , and it is crucial to monitor their possible growth which , if demonstrated , calls for a histological diagnosis with percutaneous biopsy , video - assisted thorascopy or surgical intervention . 
currently , ct is instrumental in evaluating the growth parameter of a pulmonary nodule , as it allows two - dimensional ( 2d ) comparison of diameters in the axial plane . 
however , the asymmetrical or minimal growth of some malignant nodules may be missed if a manual , and therefore nonreproducible , ct measurement is used [ 4 ]  . 
the aim of this study was to demonstrate the reproducibility of volume measurement of pulmonary nodules using the advanced lung analysis software ( ala - 1 , ge healthcare )  . materials and methods patient selection our series comprised 77 nonconsecutive patients ( 42 men , 35 women ) aged 4582 years ( mean age 65 years ) studied by ct between january and december 2004 . 
inclusion criteria were solid , noncalcific pulmonary nodules according to the definition reported in the literature [ 5 ] , solitary pulmonary nodules ( spn ) with peripheral ground - glass attenuation and central cavitation . 
in six patients , oncological follow - up revealed multiple repetitive lesions . overall , we retrospectively evaluated 103 nodules ranging in size between 3.8 mm and 30 mm , 19 of which were well cirla caratterizzazione di un nodulo polmonare , specie di quelli con dimensioni comprese tra 5 mm e 10 mm , difficile se non impossibile con metodiche quali la tomografia computerizzata ad emissione di positroni ( pet ) , la tc dinamica multifasica o lagobiopsia percutanea [ 13 ]  . ad eccezione di alcuni noduli polmonari completamente calcifici e / o contenenti tessuto adiposo e pertanto considerati benigni , tutti gli altri sono da considerarsi potenzialmente maligni e perci diventa cruciale la valutazione delleventuale aumento delle loro dimensioni che , se dimostrato , impone una diagnosi istologica con biopsia percutanea , videotoracoscopia oppure lintervento chirurgico . allo stato attuale , la tc riveste un ruolo fondamentale nella valutazione del parametro crescita di un nodulo polmonare , poich consente una comparazione bidimensionale dei diametri su piani di scansione assiali . 
tuttavia , la crescita asimmetrica o di lieve entit di alcuni noduli maligni pu essere misconosciuta , impiegando un tipo di misurazione manuale con tc e quindi non ripetibile [ 4 ]  . obiettivo del nostro studio quello di dimostrare la ripetibilit del calcolo volumetrico dei noduli polmonari utilizzando un software automatico advanced lung analysis ( ala1 , ge healthcare )  . materiali e metodi selezione dei pazienti la serie comprende 77 pazienti ( 42 maschi e 35 femmine ) non consecutivi di et compresa tra 45 e 82 anni ( media 65 anni ) , sottoposti a tc nel periodo compreso tra gennaio 2004 e dicembre 2004 . criteri di inclusione : noduli polmonari solidi non calcifici secondo la definizione riportata in letteratura [ 5 ] , noduli polmonari solitari con ground - glass periferico e con cavitazione centrale . 
criteri di esclusione : noduli con diametro > 30 mm , noduli con atelectasia adiacente , noduli calcifici ed a componente mista ( solido - liquida )  . settantasette pazienti presentavano un nodulo polmonare solitario ( nps ) riscontrato casualmente in corso di un esame radiologico del torace o tc del torace effettuati per altri cumscribed , 45 juxtapleural and 39 juxtavascular ( table 1 )  . acquisition parameters examinations were conducted with a 16 - detector - row multislice ct ( msct ) scanner ( lightspeed pro 16 ge healthcare , milwaukee , wi , usa )  . 
the study to identify the pulmonary nodules was carried out with an unenhanced lowdose ct scan of the chest with volumetric caudocranial acquisition from the costophrenic sulci to the thoracic inlet and with a single inspiratory breath - hold . 
the study to measure nodule volume was performed by including the single nodule in the acquisition and using the following acquisition parameters : slice thickness 0.625 mm , reconstruction interval 0.4 mm , pitch 0.562 : 1 , 140 kv , 300 mas , field of view 13 cm and high spatial resolution reconstruction algorith ala software the ala software segments the pulmonary nodule by combining watershed segmentation and shape analysis techniques . 
different shape - analysis algorithms are used depending on the type of nodule ( which is recognised automatically ) : ( a ) well - circumscribed ( no or minimal connections with vessels or pleura ) ; ( b ) juxtavascular ( adhering to vascular structures ) ; ( c ) juxtapleural ( adhering to pleural structures )  . 
in 6 pazienti , in follow - up oncologico , sono state rilevate lesioni ripetitive multiple . complessivamente sono stati valutati retrospettivamente 103 noduli con dimensioni variabili da 3 , 8 mm a 30 mm e di cui 19 circoscritti , 45 iuxta - pleurici e 39 iuxta - vascolari ( tabella 1 )  . parametri di acquisizione lesame stato condotto con apparecchiatura tc multistrato a 16 banchi di detettori ( lightspeed pro 16 ge healthcare , milwaukee , usa )  . 
per la ricerca dei noduli polmonari stato effettuato un esame tc del torace a bassa dose con acquisizione volumetrica senza mdc per via endovenosa , dagli sfondati costo - frenici allo stretto toracico superiore , in senso caudo - craniale , in singola apnea inspiratoria . 
lo studio per il calcolo volumetrico del nodulo stato effettuato includendo nel volume di acquisizione il singolo nodulo ed utilizzando i seguenti parametri di acquisizione : spessore di strato 0 , 625 mm , intervallo di ricostruzione 0 , 4 mm , pitch 0 , 562 : 1 , 140 kv , 300 mas , campo di vista ( field of view ) 13 cm ed algoritmo di ricostruzione ad elevata risoluzione spaziale . software ala il software da noi utilizzato segmenta il nodulo polmonare mediante un sistema combinato di segmentazione spartiacque e di tecnica di analisi della forma . 
il concetto di segmentazione la chiave del funzionamento del software advanced lung analysis ( ala )  . il risultato di una segmentazione automatica , ottenuta dopo che loperatore ha posto un repere di identificazione sul nodulo , fornisce una calcolo , anchesso automatico , del volume del nodulo stesso . 
after the radiologist has placed a marker on the nodule , the segmentation process starts with automatic display of a region of interest around the nodule that includes surrounding anatomic structures such as vessels , pleural surface and mediastinuthis box is oversampled to obtain isotropic voxels for more accurate volume estimation . 
lultimo step lanalisi della forma , che applica la giusta segmentazione per isolare il nodulo dai vasi e / o dalla pleura circostanti . and retrospectively analysed on a workstation ( advantage windows 4.2 , ge healthcare ) and were classified based on type and algorithm used by the software into well circumscribed ( n = 19 ) , juxtavascular ( n = 45 ) and juxtapleural ( n = 39 ) if in contact with the mediastinal , diaphragmatic pleura , fissures or chest wall . 
of the 103 nodules studied , ten ( 9.7% ) had a diameter < 5 mm , 25 ( 24.27% ) had a diameter of 5 mm and < 10 mm , 41 ( 39.8% ) had a diameter of 10 mm to < 15 mm , 14 ( 13.6% ) had a diameter of 15 to < 18 mm and 13 ( 12.62% ) had a diameter 18 and < 30 mm . the case series comprised 98 solid nodules , three excavated nodules ( two juxtavascular and one juxtapleural ) , one well - circumscribed excavated nodule with peripheral ground - glass attenuation , and one well - circumscribed solid nodule with peripheral ground - glass attenuation . 
accuracy and reproducibility of nodule contour segmentation over three consecutive measurements was evaluated in consensus by three radiologists ( lv , ms , mam ) with different levels of experience in chest ct ( 25 , 16 , 5 years )  . 
on the basis of the softwares ability to outline the nodule contours as accurately as possible , a visual score was assigned ( 1 = optimal , 95% ; 2 = fair , 9095% ; 3 = poor , 90% )  . 
reproducibility of volume measurement was assessed by comparing the values in mm3 estimated in the three measurements obtained for each nodule . statistical analysis correlations were made between the three measurements and between each measurement and diameters . 
repeatability of the calculation of mean volume mm3 in the three measurements obtained for each nodule ( well circumscribed , juxtavascular and juxtapleural ) was determined by simple variance analysis ( anova test )  . 
standard deviation in parentheses measurement nodules anova test 1 , 422.69 ( 1 , 678.68 ) 1 , 451.23 ( 1 , 702.76 ) 1 , 411.00 ( 1 , 650.18 ) p > 0.05 tabella 2 volume medio ( in mm3 ) dei noduli i nelle tre misurazioni . 
i numeri in parentesi indicano la deviazione standard misurazione noduli anova test 1422 , 69 ( 1678 , 68 ) 1451 , 23 ( 1702 , 76 ) 1411 , 00 ( 1650 , 18 ) p > 0 , 05 l . 
dei 103 noduli studiati , 10 ( 9 , 7% ) presentavano un diametro < 5 mm , 25 noduli ( 24 , 27% ) 510 mm , 41 ( 39 , 8% ) 1015 mm , 14 ( 13 , 6% ) 1518 mm ed infine 13 ( 12 , 62% ) 1830 mm . nella casistica sopradescritta sono compresi 98 noduli solidi , 3 noduli escavati ( 2 iuxta - vascolari ed 1 nodulo iuxtapleurico ) , 1 nodulo escavato con ground - glass periferico , circoscritto , ed 1 nodulo solido con ground - glass periferico , anchesso circoscritto . impiegando il software ala1 sono state effettuate tre misurazioni volumetriche automatiche consecutive per ciascuno dei 103 noduli studiati . 
laccuratezza e la riproducibilit nella segmentazione dei contorni di ogni nodulo , in tre misurazioni consecutive , stata valutata , in consensus da tre radiologi ( lv , ms , mam ) con diversa esperienza in tc del torace ( 25 , 16 , 5 anni )  . in base alla capacit del software di delineare i contorni del nodulo nel modo pi fedele possibile , stato assegnato un punteggio visivo ( 1 = ottimo , 95% ; 2 = discreto , 90%95% ; 3 = scarso , 90% )  . 
la riproducibilit nel calcolo del volume stata valutata confrontando i valori in mm3 stimati nelle tre misurazioni ottenute per ciascun nodulo . analisi statistica stata effettuata la correlazione tra le tre misurazioni e tra ciascuna misurazione e i rispettivi diametri . 
la riproducibilit nel calcolo del volume medio in mm3 nelle tre misurazioni ottenute per ciascun nodulo ( circoscritto , iuxta - vascolare e iuxtapleurico ) stata determinata con lanalisi della varianza semplice ( anova test )  . 
un valore p inferiore a 0 , 05 stato considerato statisticamente significativo . risultati la segmentazione stata possibile in tutti i noduli analizzacon il software ala1 stata ottenuta una segmentazione di tipo 1 in 43 noduli , una segmentazione di tipo 2 e 3 rispettivamente in 35 e 25 noduli . 
il software ala1 ha consentito una segmentazione ottima ( tipo 1 ) separando correttamente il nodulo dalla parete toracica . table 3 mean volume ( in mm3 ) of nodules after dimension classification in three measurements . 
standard deviation in parentheses measurement circumscribed ( n = 19 ) juxtapleural ( n = 39 ) juxtavascular ( n = 45 ) tabella 4 volume medio ( in mm3 ) dei noduli , dopo stratificazione per tipo , nelle tre misurazioni . 
the size distribution of the 41 nodules in which ala - 1 failed to provide a repeatable volume reconstruction was : 0 nodules < 5 mm , 11 nodules 5 to < 10 mm , 19 nodules 10 to < 15 mm , two nodules 15 to < 18 mm and nine nodules 18 to < 30 mm . of the 41 nodules with nonreproducible volume reconstruction , 22 showed a difference , expressed in mm3 , over the three measurements < 5% , nine 5% to < 10% and ten 10% . 
these 41 nodules included one excavated nodule ( juxtapleural ) and the solid nodule with peripheral groundglass attenuation ( well circumscribed ) , for which the difference , expressed in mm3 , over the consecutive measurements was < 5% . in the nodules for which ala - 1 yielded identical volume calculation , repeatability of the three measurements correlated with repeatability of the segmentation ; in contrast , in the nodules without repeatable volume calculation , none of the three measurements correlated with segmentation repeatability . 
the mean volume ( in mm3 ) of the well - circumscribed , juxtavascular and juxtapleural in the three measurements is shown in table 2 . figures 6 and 7 show the correlation between nodule volume and diameter , respectively . 
 discussion the introduction of singleand multislice ct scanners in clinical practice has substantially increased detection rates of pulmonary nodules [ 6 ] , and it has been reported that in 23%66% of subjects participating in screening programmes , at least one solitary pulmonary nodule is discovered , most with a diameter of 510 mm [ 7 , 8 ]  . previous reports have highlighted the potential utility of computer - aided detection ( cad ) in increasing sensitivity of misu misu misu misu misu misu itlineformisu misu itlineformisu misu itlineformisu misu qinear qinear qinear fig . 
nei 41 noduli sopradetti rientrano 1 nodulo escavato ( iuxtapleurico ) ed il nodulo solido con ground - glass periferico ( circoscritto ) che presentavano comunque una differenza , espressa in mm3 , tra le tre misurazioni consecutive < 5% . nei noduli in cui ala1 consentiva un identico calcolo del volume , la riproducibilit delle tre misurazioni si correlava con una riproducibilit di segmentazione ; viceversa nei noduli senza riproducibilit nel calcolo del volume , ciascuna delle tre misurazioni non si correlava , in nessun caso , con una riproducibilit di segmentazione . il volume medio ( in mm3 ) dei noduli circoscritti , iuxtavascolari e iuxta - pleurici nelle tre misurazioni riportato nella tabella 2 . nelle figure 6 e 7 riportata rispettivamente la correlazione tra volume e diametro del nodulo . 
lanalisi statistica non ha dimostrato una differenza statistica significativa tra i volumi dei noduli riscontrando quindi una forte correlazione ( p < 0 , 01 )  . measure 1 / misurazione 1 diameter / diametro measure 2 / misurazione 2 diameter / diametro measure 3 / misurazione 3 volume volume volume diameter / diametro fig . 
gli atti della letteratura , infatti , riportano che dal 23% al 66% di soggetti inclusi in un programma di screening presentano almeno un nodulo polmonare solitario nella maggior parte con diametro compreso tra i 5 ed i 10 mm [ 7 , 8 ]  . alcuni autori hanno sottolineato la potenziale utilit del cad ( computer - aided detection ) nel consentire un incremento della sensibilit nella identificazione dei noduli polmonari con tcms e nel ridurre il tasso di falsi positivi , con possibilit di rimpiazzare nella doppia lettura il secondo radiologo [ 9 , 10 ]  . 
 because lung cancer often presents as an spn and treatment at an early stage ( ia ) is associated with relatively good outcomes ( 5 - year survival around 60%70% ) , the current tendency is to overdiagnose and treat even very small nodules [ 11 ]  . 
moreover , hospitalisation for surgical removal of an spn costs around us$ 25 , 000 [ 15 ] , so that the aim of treatment is to find a balance between early and unnecessary resections . the main objective in the management of an spn is therefore twofold : ( a ) achieve early resection of malignant forms , and ( b ) minimise the number of benign nodules that are surgically removed . 
characterisation of an spn often relies on morphological criteria ( dimensions , shape , contours , internal characteristics ) of high - resolution ct , which is far more sensitive than the standard ct technique in evaluating features typically associated with benignity or malignancy [ 16 ]  . 
to date , however , only three such criteria have been widely accepted as indicators of benignity : ( a ) intralesional calcification with benign pattern ; ( b ) presence of intralesional fat ; ( c ) absence of volume increase for over two years . 
have , however , reported that the likelihood of a small noncalcified nodule ( 4 mm ) displaying perceptible growth at ct follow - up after 1 year is 1% ; they therefore recommend that nodules 4 mm in patients with no previous history of malignancy should undergo a first ct follow - up scan after 12 months at least rather than 36 months and be followed up for at least 2 years thereafter to ascertain the nodule is stable [ 17 ]  . 
 [ 4 ] reported a case of a nodule with an asymmetrical growth that was considered to have a doubling time compatible with benignity on the basis of 2d measurements but compatible with malignancy on the basis of 3d measurements , thus underlining that some malignant nodules may have an asymmetrical growth that may be missed with conventional 2d measurements . moreover , manual measurements may prove extremely imprecise and nonreproducible , especially when carried out on small nodules with only minimal growth [ 18 ] even if done with standard window and level values . 
the possibility of assessing the growth of an spn by means of automatic a tuttoggi , tuttavia , solo tre criteri radiologici tc sono largamente accettati come indice di benignit : ( a ) calcificazioni intralesionali con pattern benigno ; ( b ) presenza di tessuto adiposo intralesionale ; ( c ) assenza di crescita volumetrica per un periodo superiore a due anni . la valutazione delle caratteristiche morfologiche di un nps con tc ad alta risoluzione pu aiutare il radiologo nel differenziare forme benigne da forme maligne ed evitare ulteriori , costosi approfondimenti diagnostici . 
hanno comunque riportato che esiste una probabilit 1% che un piccolo nodulo non calcifico ( 4 mm ) possa presentare una crescita percettibile in un follow - up con tc entro 12 mesi e raccomandano quindi nei noduli con dimensioni 4 mm , in pazienti con anamnesi negativa per patologia neoplastica , un primo controllo tc ad almeno 12 mesi di distanza piuttosto che 36 mesi ed un follow - up con durata di almeno due anni per accertarne la stabilit [ 17 ]  . il follow - up mediante tc , basato sul rilievo della crescita del nodulo , si realizza con la misurazione comparativa bidimensionale del diametro su piani di scansione assiali . 
tuttavia poich la crescita di un nodulo un fenomeno tridimensionale , il calcolo diretto del volume , pu essere estremamente pi accurato della misurazione bidimensionale dei suoi diametri . a tal proposito , yankelevitz et al . 
 [ 4 ] hanno riportato un nodulo con crescita asimmetrica il cui tempo di raddoppiamento era stato considerato compatibile con un pattern benigno sulla base delle misurazioni bidimensionali e che invece presentava un tempo di raddoppiamento compatibile con un pattern maligno sulla base delle misurazioni volumetriche , sottolineando cos che alcuni noduli maligni possono presentare una crescita asimmetrica che pu essere misconosciuta dalle misurazioni bidimensionali convenzionali . inoltre leffettuazione di misurazioni manuali pu essere estremamente imprecisa e non ripetibile sopratutto su noduli di piccole dimensioni e con modesto incremento dimensionale [ 18 ] anche se effettuata con valori standard di finestra e di livello . la possibilit di valutare la crescita dimensionale di un nps mediante il calcolo volumetrico automatico , piuttosto che tramite il confronto manuale di due successive misurazioni della lesione sul piano assiale , una tecnica di recente introduzione e non ancora validata su ampie casistiche [ 1820 ]  . attualmente , sono in commercio alcuni software che consentono il calcolo volumetrico delle lesioni nodulari parenchimali polmonari con tcms . 
le problematiche concernenti , il calcolo automatico 3d di un nodulo , con tali software , sono essenzialmente legate a : ( a ) modalit destrazione del volume ; ( b ) posizionamento del marker o repere che individua il nodulo . lelevata riproducibilit o ripetibilit di un software 3d dipende dal fatto che lestrazione del volume viene eseguita automaticamente mediante lutilizzo di differenti algoritmi volume estimation rather than by manually comparing two successive measurements of cross - sectional diameter is a recent technique that has not yet been validated on a wide scale [ 1820 ]  . 
in particular , ala - 1 had higher reproducibility in volume calculation of well - circumscribed nodules compared with juxtavascular and juxtapleural nodules and higher reproducibility in volume calculation in nodules with type 1 segmentation compared with those with type 2 and 3 segmentation . the close correlation between volumes demonstrates the extreme reproducibility of ala - 1 unlike diameter measurements , which do not correlate with volume . 
 as regards nodule size in relation to nodule type in the various subgroups , variance analysis demonstrated that no statistically significant difference exists ( p > 0.05 ) between mean volumes in the three measurements relative to nodule type or there is no correlation between reproducibility of volume calculation and nodule type . 
mentre ala1 non ha effettuato una ricostruzione riproducibile in termini di volume in 41 su 103 noduli , di cui il 15 , 7% rappresentati da noduli circoscritti , il 31 , 1% da noduli iuxta - vascolari , il 61 , 5% da noduli iuxtapleurici . 
dei 41 noduli con segmentazione non riproducibile il 4 , 8% sono stati segmentati dal software con qualit 1 , il 36 , 5% con qualit 2 ed infine il 58 , 5% con qualit di segmentazione pari a 3 . 
i risultati ottenuti evidenziano lesistenza di una correlazione tra riproducibilit volumetrica e qualit di segmentazione e tra riproducibilit volumetrica e tipo di nodulo . in particolare ala1 presenta una percentuale di riproducibilit nel calcolo volumetrico pi elevata nei noduli circoscritti rispetto a quelli iuxta - vascolari e iuxta - pleurici ed una percentuale di riproducibilit nel calcolo del volume pi elevata nei noduli con qualit di segmentazione pari ad 1 rispetto a quelli con segmentazione di tipo 2 e 3 . 
la stretta correlazione tra i volumi dimostra che ala1 estremamente riproducibile differentemente dalla misurazione dei diametri che non correlano con il volume . relativamente alle dimensioni in relazione al tipo di nodulo nei vari sottogruppi , lanalisi della varianza ha dimostrato che non esiste alcuna differenza statistica significativa ( p > 0 , 05 ) tra le medie dei volumi nelle tre misurazioni in relazione alle dimensioni e al tipo di nodulo , ovvero non esiste una correlazione tra riproducibilit del calcolo volumetrico e dimensioni in relazione al tipo di nodulo . i dati della nostra serie , confermano la affidabilit e la riproducibilit del software . 
la riproducibilit del software stata valutata nel calcolo volumetrico di una singola acquisizione tc e non prende in considerazione due differenti acquisizioni tc ( ad esempio , eventuale controllo a distanza ) che potrebbero inficiare la comparazione del volume ; 2 . 
volume calculation with ala - 1 has therefore the potential to enter decision - making algorithms for management of spn and replace the less accurate 2d measurement in the ct follow - up of indeterminate or benign - appearing nodules . 
ciatto2 1ambulatori oncologici raphael , via vittorio emanuele ii , i - 25011 calcinato ( bs ) , italy 2centro per lo studio e la prevenzione oncologica , firenze , italy correspondence to : v . 
after evaluation by internal and external reviewers of cancers detected by ultrasonography performed to confirm negative mammography , we determined the additional cancer detection rate of ultrasonography and the cost of the protocol . 
the evidence is insufficient to recommend this policy in routine screening practice but suggests that , at least in current clinical practice , adding ultrasonography in dense breasts may be useful despite the substantial costs . key words breast cancer diagnosis screening ultrasonography dense breast riassunto obiettivo . 
levidenza ancora insufficiente per poter raccomandare lintroduzione di questa procedura nella corrente pratica di screening , in attesa dei risultati degli studi controllati in corso , ma suggerisce che , almeno nella pratica clinica corrente , lintegrazione ecografica nei seni densi pu essere utile , sia pure associata a costi non trascurabili . parole chiave carcinoma mammario diagnosi screening ecografia seno denso introduction introduzione v . 
this limit is evident in both clinical [ 1 ] and screening practice : dense breast tissue is considered the major determinant of reduced screening sensitivity in women younger than 50 years and is significantly associated with the risk of interval cancer at any age [ 25 ]  . 
the accuracy of ultrasonography is not dependent on age [ 6 ] , and ultrasonographic diagnosis of cancer occult to mammography due to the masking effect of dense breasts is not a rare event . 
routine association of ultrasonography and mammography in women with dense breasts has been advocated although clinical studies on this policy [ 4 , 711 ] do not allow for a reliable evaluation of its cost effectiveness , and specifically designed prospective controlled studied on this subject are ongoing [ 12 , 13 ]  . 
at the raphael clinic , a centre for cancer prevention and early diagnosis , multimodal breast diagnosis has been employed on women self referring for symptoms or screening since 1986 . 
in the present study , we reviewed a consecutive series of 17 , 883 subjects undergoing the protocol and evaluated the results of routine ultrasonography of dense breasts . materials and methods the study analyses a consecutive series of 17 , 883 women aged between 25 and 96 years undergoing breast palpation and mammography from january 2000 to september 2004 . four reporting radiologists classified breast density according to the volume occupied by fibroglandular opacity [ breast imaging reporting and data system ( bi - rads ) d1 = 025 , d2 = 2650 , d3 = 5175 , d4 = 76100 ]  . 
subjects with negative mammography and in the d3 - d4 classes underwent bilateral ultrasonography using an aloka pro sound ssd - 5500 echograph with a linear multifrequency 5to 10 - mhz probe . 
in order to confirm the negativity of mammography , cancer cases diagnosed by ultrasonography alone were first reviewed by four internal reviewers and thereafter by an expert external reviewer with more than 20 years mammography experience and more 200 , 000 mammograms read ( sc )  . 
cancer cases reviewed as even minimally suspicious at mammography ( bi - rads 35 ) were excluded from evaluation of the benefits of association of ultrasonography , as their la densit radiologica della mammella costituisce un limite notevole per la sensibilit della mammografia . 
questo limite ben evidente sia in ambito clinico [ 1 ] che di screening : il seno denso considerato il principale movente della ridotta sensibilit ed efficacia dello screening mammografico al di sotto dei 50 anni e si associa significativamente al rischio di carcinoma di intervallo a qualsiasi et [ 25 ]  . 
laccuratezza della ecografia mammaria non risente dellet [ 6 ] e la diagnosi ecografica di carcinomi non evidenziati alla mammografia per leffetto mascherante del seno denso un evento non raro . 
lassociazione sistematica dellecografia mammaria alla mammografia in donne con seno denso proposta da molti , ma gli studi clinici che riportano simili esperienze [ 4 , 711 ] non consentono una valutazione precisa dei costi e dei benefici di una simile procedura , per cui sono in corso studi controllati appositamente disegnati [ 12 , 13 ]  . presso gli ambulatori raphael , un centro di prevenzione e diagnosi precoce delle patologie oncologiche , in atto dal 1986 una attivit di diagnostica senologica integrata su donne che accedono spontaneamente per sintomi o con finalit preventive . 
nel presente studio abbiamo rivisto una serie consecutiva di 17.883 casi e valutato i risultati dellassociazione sistematica dellecografia nei casi con seno denmateriali e metodi lo studio considera una serie consecutiva di 17.883 donne di et compresa fra i 25 e i 96 anni sottoposte a esame senologico e mammografia dal gennaio 2000 al settembre 2004 . i 4 radiologi che hanno interpretato i radiogrammi hanno definito la densit del seno in base alla percentuale di volume mammario occupato da densit fibroghiandolare ( birads d1 = 025 , d2 = 2650 , d3 = 5175 , d4 = 76100 )  . i soggetti con mammografia negativa classificati nelle categorie d3 e d4 sono stati esaminati con ecografia mammaria bilaterale : liter diagnostico stato completato con altri accertamenti ( esami radiologici mirati , citologia , core biopsy , biopsie chirurgiche ) in base alle eventuali alterazioni evidenziate su base clinico - ecografica . 
la revisione avvenuta in cieco , attraverso la valutazione dei casi di carcinoma mescolati a controlli negativi , selezionati in modalit casuale tra casi con seno denso approfonditi e risultati effettivamente negativi , in un rapporto cancri / controlli di 1 : 1 per la revisione interna e di v . 
as far as surgical biopsy is concerned , two alternatives were considered , namely : ( a ) outpatient procedure under local anaesthesia , or ( b ) hospitalisation . results out of 17 , 883 mammographies performed between january 2000 and september 2004 , 167 cancers were detected , with a detection rate of 0.93% ( 167 / 17 , 883 ) in the overall series . suspicious mammographies were 257 and diagnosed cancers 138 : negative mammography was reported in 11 , 177 cases ; 6 , 449 were classified as d3 - 4 ( 36.5% of the total mammographies performed and classified as not suspicious : 6 , 449 / 17 , 626 ) and ultrasonography was performed . 
il revisore , oltre a indicare le alterazioni sospette per le quali avrebbe richiesto un approfondimento diagnostico , ha espresso secondo la classificazione bi - rads [ 14 ] sia il livello di sospetto che la densit radiologica del seno . 
i casi di carcinoma identificati dal revisore come portatori di alterazioni con livello anche minimo di sospetto ( bi - rads 35 ) sono stati esclusi dalla valutazione dei vantaggi dellecografia e la loro diagnosi stata attribuita alla mammografia che , per queste categorie diagnostiche , condiziona correntemente un completamento ecografico . i risultati dellassociazione dellecografia alla mammografia negativa in seno denso sono stati espressi in termini di tasso diagnostico di carcinoma : stata anche verificata la percentuale di approfondimenti diagnostici ( citologia , core biopsy , biopsia chirurgica ) richiesti a seguito di sospetto ecografico , ma con esito negativo . 
il costo della biopsia chirurgica stato computato in base a due alternative : ( a ) biopsia escissionale ambulatoriale in anestesia locale e ( b ) biopsia in regime di ricovero ospedaliero con breve anestesia generale . risultati su un totale di 17.883 mammografie eseguite dal gennaio 2000 al settembre 2004 sono stati diagnosticati 167 carcinomi , con un tasso diagnostico di carcinoma di 0 , 93% ( 167 / 17.883 ) nella serie complessiva . 
the remaining 18 cancers were mixed with 72 negative controls and were examined by the external reviewer , who identified three cancers as radiologically suspicious ( birads r3 = 2 , r4b = 1 ) and also reported abnormalities in 15 negative controls ( bi - rads r3 = 10 , r4a = 4 , r4b = 1 )  . 
overall , after excluding symptomatic cases and cases reviewed as suspicious at mammography , the cancers for which mammography was confirmed to be negative at review and diagnosis could be attributed to ultrasonography only were 15 , accounting for a detection rate of 0.23% ( 15 of 6 , 449 cases ) and for 8.9% of total cancers detected . 
table 2 shows the distribution of cancers detected by ultrasonography alone by age , stage , morphology ( mass , calcifications ) and radiological density according to the external reviewer . 
a seguito di tale approfondimento sono stati diagnosticati altri 29 carcinomi , con una prevalenza di 0 , 44% ( 29 / 6.449 ) , pari al 17 , 3% dei carcinomi totali diagnosticati . 
i dati dettagliati per classi di et sono riportati nella tabella 1 . dei 29 carcinomi diagnosticati dallecografia in casi con mammografia negativa , le mammografie originali erano disponibili in 25 casi . 
i restanti 18 casi , mescolati a 72 controlli negativi , sono stati valutati dal revisore esterno , che ha identificato altri 3 carcinomi effettivamente sospetti alla mammografia ( bi - rads r3 = 2 , r4b = 1 ) , formulando un sospetto anche in 15 controlli ( bi - rads r3 = 10 , r4a = 4 , r4b = 1 )  . 
a setable 2 distribution of cancers detected by ultrasonography alone in mammographically negative dense breasts , according to age , density at external review , morphology , staging ( ptnm ) and histological type case no . density morphology histological type mass mass mass mass mass mass mass mass mass mass mass mass mass mass mass nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo nodulo 1 ( i + ) 1 ( i + ) nos , not otherwise specified tabella 2 distribuzione dei carcinomi identificati dallecografia in mammografie negative con seno denso , in funzione dellet , densit radiologica alla revisione , morfologia , stadio ( ptnm ) e istotipo caso densit morfologia istotipo ductal nos ductal nos ductal nos ductal nos ductal nos lobular tubular papillary mucinous lobular ductal nos medullary lobular ductal nos ductal nos duttale duttale duttale duttale duttale lobulare tubulare papillare mucinoso lobulare duttale midollare lobulare duttale duttale v . 
cost analysis details are reported in table 3 . discussion ultrasonography is often employed in both clinical and screening settings for further investigation of cases with negguito di questa revisione , i carcinomi la cui diagnosi stata effettivamente attribuita allecografia , escludendo quelli sintomatici o identificati come sospetti dai revisori , sono rimasti 15 , pari ad un tasso diagnostico di 0 , 23% ( 15 su 6.449 casi sottoposti ad ecografia di principio per seno denso ) , corrispondenti all 8 , 9% dei carcinomi totali diagnosticati . la tabella 2 riporta la distribuzione di questi carcinomi per et , stadio , morfologia ( massa , calcificazioni ) e densit radiologica alla revisione . 
la categoria pt risultata pt1a in 3 casi , pt1b in 8 casi , pt1c in 3 casi e pt2 in 1 caso . lapprofondimento ecografico ha generato in totale 405 esami citologici , 15 core biopsy , 66 biopsie chirurgiche . 
most published studies ( summarised in table 4 ) although poorly comparable due to differences in age distribution , criteria to define a dense breast , ultrasonographic equipment and accuracy [ 15 , 16 ] report a strikingly similar detection rate of mammographically occult cancers ( 0.3%0.4% ) and a false positive rate ranging between 1% and 3% . 
in our experience , the detection rate at initial analysis of crude data was 0.44% and the false positive rate was 1.25%. unfortunately , these series are not drawn from current screening practice but are based on subjects self referring to mammography , not necessarily in the screening age range ( 5069 )  . 
thus , it is difficult to evaluate from these clinical series ( for which the underlying risk and expected incidence are uncertain ) what might be the benefit of adding ultrasonography for dense breasts in screening practice in terms of additional cancer detection rate . 
to answer this question we will have to wait for the results of ongoing prospective controlled trials [ 12 , 13 ]  . the present consecutive series , although based on self referring subjects in a wide age range , is rather large and may provide some information , at least in a clinical scenario , of the likelihood of ultrasonography detecting mammographically occult breast cancer in dense breasts . 
on the other hand , it is a retrospective study , which is unable to provide definitive evidence to recommend the use of ultrasonography in current practice in cases of negative mammography and dense breasts . 
i dati dettagliati della analisi dei costi sono riportati nella tabella 3 . discussione lecografia frequentemente impiegata , sia in ambito clinico che di screening , per il completamento diagnostico in casi sostanzialmente negativi alla mammografia , ma ad elevato rischio di errore mammografico per la presenza di seno denso . 
la gran parte delle esperienze pubblicate ( le principali , assieme al presente studio , sono indicate nella tabella 4 ) , nonostante la discutibile comparabilit delle casistiche per la diversa composizione in et , la variabilit nella definizione di seno denso e nella accuratezza diagnostica ecografica [ 15 , 16 ] , riportano un tasso diagnostico di carcinoma occulto alla mammografia sorprendentemente simile , variabile tra lo 0 , 3% e lo 0 , 4% , e un tasso di falsi positivi variabile tra l1% e il 3% . 
nella presente esperienza il tasso diagnostico in prima analisi stato di 0 , 44% , con un tasso di falsi positivi di 1 , 25% . purtroppo queste esperienze non si riferiscono a casistica di screening , ma a casistica ad accesso spontaneo e spesso in et diversa da quella in cui lo screening correntemente raccomandato ; nel presente studio in particolare il 45 , 1% della popolazione esaminata aveva et inferiore ai 50 anni . quindi difficile valutare in base ai risultati di queste casistiche ( a rischio di malattia e prevalenza incerti ) quale possa essere il vantaggio relativo , in termini di tasso diagnostico di carcinoma , dellintroduzione del completamento ecografico nei seni densi nella routine dello screening . 
per tale motivo auspicabile che siano completati gli studi controllati in corso [ 12 , 13 ] , disegnati in un contesto di screening , che sono gli unici a poter rispondere al quesito . la casistica in esame , una serie clinica con afferenza spontanea di ogni et , comunque piuttosto ampia e pu fornire interessanti elementi quanto alla probabilit , sia pure in un contesto clinico , di diagnosi ecografica di carcinoma occulto alla mammografia . 
si tratta comunque di uno studio retrospettivo e , come tale , non pu costituire elemento definitivo per sostenere che lecografia in caso di mammografia negativa con seno denso radiologico sia una procedura raccomandabile di routine . 
quindi doveroso sottolineare i limiti di questa analisi , al fine di evitare che il lettore giunga a conclusioni affrettate . a tal fine , oltre a fornire il dato osservazionale grezzo , si operata una accurata revisione radiologica , che non risulta essere stata condotta nella maggioranza degli altri studi citati . 
inadequate interpretation or inaccurate reporting ( negative instead of suspicious ) of mammograms in cases selected for ultrasonography might bias the results when analysis is based on the original report . 
in the present study , review identified eight of 25 cancers that turned out to be suspicious at mammography . this peculiar aspect of our study , together with a different age distribution , may at least partially account for the lower cancer detection rate at ultrasonography observed with respect to other literature reports . 
it must be noted that the review process , though blind and with cancers mixed with negative controls , is likely to influence the reader , who is aware of reviewing a series with a high cancer prevalence , and might therefore lower the threshold for suspicion to maximise sensitivity at the expense of specificity : in fact , in our study , the external reviewer had a recall rate of 20.8% ( 15 / 72 ) among negative controls , definitely higher compared with the usual recall rate in screening , although suspicion was mild in most cases ( 14 / 15 < r4b , no r4c - r5 )  . 
external review does not discount that mammography was actually reported as negative or the benefit of ultrasonography but suggests that this benefit might also be obtained , to some extent , by improving the accuracy of mammography , particularly if this is suboptimal . 
the aim of external review is not to minimise the advantages of ultrasonography but to suggest caution in drawing definitive conclusions , and we believe that review may be useful for such a purpose . 
in agreement with previous literature reports , ultrasonography detected at least 15 additional cancers , a detection rate of 0.23% among subjects undergoing ultrasonography , or 8.98% of all cancers detected in the study cohort . 
detection rate was age dependent , being highest in the 50to 59 - year age group ( 0.32% ) ; this finding is interesting , as screening is currently recommended in this age group . 
the benefits of ultrasonography are further underlined by the limited stage of cancers detected , with 11 of 15 cases measuring less than 1 cm in size , a sign of a favourable prognosis . 
because ultrasonography is not highly specific , its extensive use implies unnecessary diagnostic procedures leading to a negative final diagnosis [ 9 , 10 , 15 ]  . grafie precedenti un carcinoma di intervallo . 
una insufficiente qualit della lettura mammografica , infatti , o una non accurata codifica ( negativo anzich sospetto ) dei casi avviati allecografia , potrebbe falsare i dati ove la valutazione prenda come riferimento la refertazione originale della mammografia . 
questa caratteristica dello studio , oltre alla diversa composizione in et , pu almeno in parte spiegare il minor tasso diagnostico di carcinoma allecografia osservato in questa , rispetto alle altre serie della letteratura ( tabella 4 )  . 
opportuno considerare che la conduzione di una revisione , sia pure cieca e con aggiunta di controlli negativi , modifica comunemente latteggiamento del revisore che , consapevole dello scopo della revisione , pu abbassare il livello di sospetto nellintento di aumentare la sensibilit a spese della specificit : nel presente studio il revisore esterno , infatti , ha avuto un tasso di falsi positivi tra i controlli del 20 , 8% ( 15 / 72 ) , sia pure con livelli di sospetto prevalentemente bassi ( 14 / 15 < r4b , nessun r4c - r5 )  . 
la revisione nulla toglie al fatto che quella mammografia stata di fatto considerata negativa e al beneficio conseguente allecografia , ma avverte che i benefici dellecografia potrebbero essere ottenuti , almeno in parte , anche da un miglioramento della accuratezza diagnostica mammografica . 
lintento della revisione non di sminuire i meriti dellecografia , ma di indurre cautela nelle conclusioni , e ci sembrato utile adottare questo controllo , preferendo presentare , oltre al dato osservazionale grezzo , una stima pi prudenziale dei benefici dellecografia . il contributo diagnostico dellecografia in questo studio non stato trascurabile . 
confermando i risultati della letteratura , lecografia ha diagnosticato 15 carcinomi aggiuntivi , pari ad un tasso del 0 , 23% nei soggetti sottoposti ad ecografia e al 8 , 98% dei carcinomi diagnosticati complessivamente nella coorte in esame . 
il tasso diagnostico dipende dallet , con il valore pi elevato nella fascia det 5059 anni ( 0 , 32% ) ; il dato appare significativo , se si considera che tale popolazione rientra fra quella a cui si rivolge lo screening . 
il beneficio dellecografia ulteriormente valorizzato dal fatto che le neoplasie diagnosticate hanno una distribuzione per stadio molto favorevole , con ben 11 casi su 15 di diametro inferiore ai 10 mm , foriera di una buona prognosi . la non assoluta specificit dellecografia implica ovviamente che un suo uso esteso comporti un certo numero di accertamenti inutili , non esitanti in diagnosi di carcinoma [ 9 , 10 , 15 ]  . 
lanalisi dei costi relativa a questo carico diagnostico addizionale stata necessariamente condotta in base a un preciso tariffario , pur consapevoli che una simile stima solo indicativa , in quanto non tiene conto di una notevole variabilit dei tempi e dellorganizzazione di lavoro nei diversi contesti . 
this is definitely higher compared with the average cost ( around euro 5 , 000 ) reported per cancer detected at screening [ 17 ] , but a higher cost was indeed expected , as ultrasonography was looking for cancers missed at mammography , which are likely to be difficult to detect and to have a low prevalence . 
it is impossible to compare costs to prognostic benefit obtained by additional cancer detection at ultrasonography , as we ignore whether and to what extent mortality was affected by the earlier diagnosis by ultrasonography . 
it is difficult to draw any conclusion concerning a screening scenario from the present experience , as the study population is selected ( self referring ) and is likely not representative of a general screening population in terms of breast cancer risk and dense - breast frequency . 
the proportion of subjects with dense breast over age 50 and thus sent for ultrasonography were 25.7% : assuming the cost subsequent to ultrasonography to be independent of age , the cost per woman examined would be around euro 15 , 00 . 
this is a substantial increase ( + 30% ) of screening costs , the most recent reliable published report being around euro 50 , 00 per woman in 1995 [ 17 ] , which may be presently estimated to be around euro 60 , 00 ( adjusted for devaluation )  . 
on the other hand , additional cancers detected by ultrasonography in women over age 50 were seven , compared with 112 detected at mammography , thus accounting for a relative sensitivity increase of 6.2%. 
overall , the present experience confirms the possibility of ultrasonography detecting mammographically occult cancer in dense breasts [ 1 , 18 ] although we agree with kopans [ 1922 ] that this does not constitute sufficient evidence to support the introduction of this policy in current screening practice . 
tale costo decisamente pi elevato del costo per carcinoma diagnosticato ( intorno ad euro 5000 ) comunemente riportato in esperienze di screening [ 17 ] , ma un costo pi elevato ovviamente atteso quando si ricerchino carcinomi aggiuntivi , sfuggiti alla mammografia , verosimilmente pi difficili da identificare e a bassa prevalenza . 
 impossibile quantificare il beneficio della diagnosi ecografica in termini prognostici , in quanto non possibile stimare se , ed eventualmente quanto , lanticipazione diagnostica ottenuta abbia influenzato di fatto la mortalit . assai difficile trarre da questa esperienza indicazioni valide per uno scenario di screening , dato che la popolazione in esame autoselezionata e ha verosimilmente una prevalenza di seno denso e un rischio di carcinoma diverso da una popolazione di screening . 
pu essere comunque utile , a solo fine speculativo , tentare un confronto approssimativo . se si considerano le donne di 50 anni ed oltre , i soggetti avviati allecografia per seno denso sono stati il 25 , 7% : assumendo che il costo dellintegrazione con ecografia sia omogeneo per et , il costo per donna esaminata risulterebbe di circa euro 15 , 00 e configurerebbe un aumento consistente ( + 30% ) dei costi dello screening , la cui ultima stima attendibile in letteratura , risalente al 1995 , intorno a euro 50 , 00 per donna esaminata [ 17 ] , stimabile attualmente intorno a euro 60 , 00 ( correzione in base al tasso di svalutazione )  . 
di contro , i carcinomi aggiuntivi diagnosticati dalla sola ecografia in et di 50 o pi anni sono stati 7 rispetto a 112 sospettati dalla mammografia , pari ad un aumento relativo di sensibilit del 6 , 2% . complessivamente la presente esperienza conferma la possibilit che lecografia identifichi neoplasie maligne occulte alla mammografia in seni densi [ 1 , 18 ] , anche se , come ripetutamente stigmatizzato da kopans a distanza di anni [ 1922 ] , non costituisce una evidenza sufficiente a raccomandare lintroduzione di questa procedura nella corrente pratica di screening . 
il disegno di studio , con lattenta revisione critica dei radiogrammi originalmente refertati come negativi , ha ridimensionato in parte il contributo dellecografia , ma non si deve dimenticare che nella realt clinica ( in assenza di una revisione ) i carcinomi occulti alla mammografia , asintomatici e sospettati grazie alla sola integrazione ecografica sono stati ben 27 ( 16 , 1% )  . 
the aim of this study was to determine the spin - lattice relaxation or t1 time constant of phosphocreatine in the human gastrocnemius muscle , both at rest and during aerobic exercise , when a clinical nuclear magnetic resonance ( nmr ) scanner is available . 
protocols and models were tested on a phantom containing 1 kg of distilled water in which were dissolved 5.88 g sodium chloride , 1 cm3 phosphoric acid and 7.58 g sodium phosphate dodecahydrate . 
tutti i protocolli ed entrambi i modelli sono stati testati su un fantoccio contenente 1 kg dacqua distillata in cui erano disciolti 5 , 88 g di cloruro di sodio , 1 cm3 di acido fosforico e 7 , 58 g di fosfato di sodio dodecaidrato . 
sul fantoccio , i valori medi di t1 sono risultati molto diversi per i protocolli ed i modelli matematici utilizzati , variando da 0 , 61 s a 7 , 20 s . 
correggendo il valore di t1 ottenuto sui volontari , mediante i risultati del fantoccio , si ricava un valore di t1 pari a 5 , 73 s , confrontabile con quello riportato in letteratura per la sola condizione di riposo . key words t1 time constant progressive saturation muscle , exercise phosphocreatine parole chiave costante di tempo t1 saturazione progressiva muscolo , esercizio fosfocreatina introduction introduzione clinical nuclear magnetic resonance ( nmr ) devices are often also used for research purposes after appropriate software and hardware has been added . 
1h - mrs is used to diagnose brain masses [ 1 ] or in oncology [ 2 , 3 ] whereas 31p or 13c spectroscopy is used in the diagnosis and follow - up of epilepsy and other neuropsychile apparecchiature di risonanza magnetica nucleare per uso clinico sono spesso utilizzate anche a scopo di ricerca , aggiungendo opportuni software ed hardware . 
ci avviene , in particolare , per quelle unit rmn ampliate per rendere possibili anche indagini di spettroscopia in vivo ( mrs ) , tecnica che negli ultimi anni sta ricevendo sempre maggiore attenzione . 
finally , 31p spectroscopy is used to study muscle function and / or metabolism both in healthy volunteers [ 7 ] and in patients [ 810 ]  . in 31p spectra obtained from muscle tissue , the prevailing lines are those of inorganic phosphate ( pi ) , phosphocreatine ( pcr ) and three phosphoric groups of adenosine triphosphate ( - atp , - atp , and - atp )  . 
furthermore , the absolute position of the pi peak depends on intracellular ph , which can thus be determined by measuring the chemical shift of pi relative to a fixed line ( typically the pcr line )  . 
in the absence of disease , at the start of moderate exercise , the pcr is hydrolysed to provide part of the energy needed for contraction ; consequently , the intensity of its peak drops , only to stabilise as soon as aerobic metabolic processes are able to produce all the necessary energy . 
 these phenomena can be observed clearly only with a good signal - to - noise ratio , obtained by adding as many spectra as possible although within an inevitably limited time . 
as a consequence , short repetition times ( trs ) are used , which , however , make the spectra partially saturated and therefore require the peak intensity to be corrected to obtain information on the absolute concentrations of metabolites . 
to this end , with the muscle at rest , the ratio between the area subtended by a spectrum acquired with a long tr and that of a spectrum acquired with a short tr is calculated . 
this ratio is then used to correct the areas of all the spectra acquired with a short tr during the experimental stage [ 15 , 17 , 18 ]  . 
application of this method must , however , take into account the intrinsic characteristics of the material being studied , quantised through the spin - lattice relaxation or t1 time constant . 
the t1 values reported in the literature have been obtained both on isolated muscles [ 13 , 19 ] and in vivo [ 20 , 21 ] but only during isometric exercises without doing any mechanical work [ 22 ] and , sometimes , with varying intracellular ph [ 21 ]  . the purpose of our work was to estimate , with the saturation recovery technique , the apparent t1 [ 23 ] on humans by using a clinical scanner adapted for 31p spectroscopy studies . 
in particular , the possible variations of the apparent t1 of phosphocreatine ( t1 ) between rest and moderate aerobic exercise were investigated . materials and methods the experiment was conducted with a 1.5 tesla magnetic resonance ( mr ) scanner ( magnetom sp 4000 , siemens , erlangen , germany ) equipped with a 5 - cm surface coil that can be tuned to detect both hydrogen ( 1h ) and phosphorus nuclei ( 31p )  . 
the spectroscopy sequence available on the nmr unit , provided by the manufacturing company , merely excited the spettroscopie al 31p o al 13c sono utilizzate nella diagnosi e nel follow - up di epilessia ed altre patologie neuro - psichiatriche [ 46 ]  . 
infine , la spettroscopia al 31p utilizzata per studiare la funzione e / o il metabolismo muscolare , sia in volontari sani [ 7 ] che in pazienti [ 810 ]  . negli spettri al 31p ottenuti dal tessuto muscolare , le righe che predominano sono quelle del fosforo inorganico ( pi ) , della fosfocreatina ( pcr ) e dei tre gruppi fosforici delladenosintrifosfato ( - atp , - atp e - atp )  . 
inoltre , la posizione assoluta del picco del pi dipende dal ph intracellulare , che quindi pu essere determinato misurando il chemical shift del pi rispetto ad una riga fissa ( tipicamente quella della pcr )  . 
in assenza di patologie , allinizio di un esercizio moderato , la pcr viene idrolizzata per fornire una parte dellenergia necessaria per la contrazione e quindi lintensit del suo picco si riduce , per stabilizzarsi appena i processi metabolici di tipo aerobico sono in grado di produrre tutta lenergia necessaria . 
il picco del fosforo inorganico presenta lo stesso andamento , ma speculare , mentre le dimensioni dei rimanenti picchi rimangono invariate , risultando quindi indipendenti dal lavoro muscolare . questi fenomeni sono chiaramente osservabili solo con un buon rapporto segnale - rumore , ottenuto sommando il maggior numero possibile di spettri , anche se in un tempo necessariamente limitato . 
di conseguenza , sono utilizzati tempi di ripetizione ( tr ) brevi che , per , rendono gli spettri parzialmente saturati e quindi , volendo ottenere informazioni sulle concentrazioni assolute dei metaboliti , lintensit dei picchi deve essere corretta . 
a tal fine , sul muscolo a riposo , viene calcolato il rapporto tra larea sottesa da uno spettro acquisito con un tempo di ripetizione lungo e quella di uno spettro acquisito con il tr breve , che poi viene utilizzato per correggere le aree di tutti gli spettri acquisiti con il tr breve in fase sperimentale [ 15 , 17 , 18 ]  . 
lapplicazione di questo metodo , per , non pu prescindere dalle caratteristiche intrinseche del materiale in studio , quantizzate dalla costante di tempo di rilassamento spin - reticolo o t1 . 
i valori di t1 finora riportati dalla letteratura sono stati ottenuti sia su muscoli isolati [ 13 , 19 ] che in vivo [ 20 , 21 ] , ma effettuando solamente esercizi di tipo isometrico , ovvero senza compimento di lavoro meccanico [ 22 ] e , a volte , con variazione di ph intracellulare [ 21 ]  . scopo del presente lavoro stimare , applicando la tecnica della saturazione progressiva , il t1 apparente [ 23 ] in vivo sulluomo utilizzando un tomografo per uso clinico adattato agli studi di spettroscopia al 31p . 
in particolare , sono state indagate le possibili variazioni del t1 apparente della fosfocreatina ( t1 ) tra le condizioni di riposo e di esercizio aerobico moderato . materiali e metodi la sperimentazione stata condotta con un tomografo rmn ( magnetom sp 4000 , siemens , erlangen , germania ) da 1 , 5 v . 
the time required for each measurement ( tmis ) included : a first waiting interval lasting one tr the time required by the prescans ( nps ) , namely , the number of excitations of the tissue caused by radiofrequency ( rf ) pulses with homogeneous tr intervals without collecting the mr signal the time required to excite the tissue and record the mr signal for a certain number of acquisitions ( nacq ) , each one tr apart . 
having to automatically acquire nmis spectra , the nmr unit operated for a ta time equal to ta = nmis tmis to which the time required for software reconstruction and saving of the spectra on the scanners computer ( about 1 s for each spectrum ) had to be added . the entire experiment involved a first set of in vitro measurements followed by the in vivo experiments . 
the parameters of the different acquisition protocols were selected in order to acquire of all spectra under saturation conditions , assuming that t1 = 6 s [ 22 ]  . in vitro experimental protocols a first set of measurements was made by placing the surface coil over a phantom consisting of a plexiglas cylinder containing 1 kg of distilled water in which 5.88 g nacl , 1 cm3 h3po4 and 7.58 g na3po412h2o were dissolved . 
the first measurement protocol ( long protocol ) was aimed at determining the t1 time constant of the solution contained in the phantom and was repeated six times on different days . 
the tr , initially set at 601 ms , was increased by 500 ms for every set whereas the number of the spectra acquired for each set was reduced from 24 in the first to 19 in the 13th set . 
the parameters of the three short protocols were fixed so as to be very different from one another although meeting the following conditions : total time of each protocol had to be less than 8 min information on the greatest number of trs had to be acquired within the available time tesla , dotato di una bobina di superficie del diametro di 5 cm , sintonizzabile sia per i nuclei di idrogeno ( 1h ) che per quelli di fosforo ( 31p )  . 
non era possibile controllare esattamente alcuni parametri cruciali , come ad esempio il flip angle . il software di gestione permetteva lacquisizione automatica di una serie di spettri ( misure ) , tutti acquisiti con lo stesso tr . 
il tempo necessario per ogni misura ( tmis ) comprendeva : un primo intervallo di attesa , della durata di un tempo di ripetizione ( tr ) ; il tempo impiegato dai pre - scans , ovvero dal numero nps di eccitazioni del tessuto con impulsi rf ad intervalli temporali omogenei tr , senza la raccolta del segnale rm ; il tempo impiegato per leccitazione del tessuto e la registrazione del segnale rm per un certo numero di acquisizioni nacq , tutte distanziate di un tempo tr . 
 conseguentemente tmis era pari a : tmis = tr + npstr + nacqtr + = tr ( 1 + spn + nacq ) + dove lintervallo di tempo aveva una durata di circa 1 , 26 s . 
dovendo acquisire automaticamente nmis spettri , lunit rmn veniva impegnata per un tempo ta pari a : ta = nmis tmis a cui si aggiungeva il tempo necessario per la ricostruzione software ed il salvataggio degli spettri sul computer del tomografo ( circa 1 secondo per ogni spettro )  . lintera sperimentazione ha previsto una prima serie di misure effettuate in vitro , alle quali hanno fatto seguito gli esperimenti in vivo . 
i parametri dei diversi protocolli di acquisizioni sono stati selezionati imponendo che tutti gli spettri fossero acquisiti in condizioni di saturazione , ipotizzando un t1 = 6 s [ 22 ]  . protocolli sperimentali in vitro una prima serie di misure stata effettuata posizionando la bobina di superficie su un fantoccio formato da un cilindro di plexiglass contenente 1 kg dacqua distillata in cui erano disciolti 5 , 88 g di nacl , 1 cm3 di h3po4 e 7 , 58 g di na3po412h2o . 
il primo protocollo di misura ( protocollo lungo ) ha avuto lo scopo di determinare il t1 della soluzione contenuta nel fantoccio ed stato ripetuto 6 volte in giorni diversi . 
il tr , inizialmente fissato a 601 ms , stato incrementato di 500 ms ad ogni serie , mentre il numero di spettri acquisiti per ciascuna serie stato ridotto da 24 nella prima a 19 nella tredicesima . per ciascun tr sono stati considerati solamente gli ultimi 16 spettri acquisiti . successivamente , sono stati effettuati 3 protocolli corti , v . 
the number of prescans fell from 25 in the first to three in the sixth measurement whereas the tr increased in each measurement from 601 ms to 5 , 601 ms with 1 - s increments . 
in the third protocol ( protocol c ) , 65 spectra were acquired with seven separate sets , all with three acquisitions and no prescan ; the first two sets supplied ten spectra , the remaining sets nine . 
for this protocol , only the last six spectra were taken into consideration for every tr . in vivo experimental protocol the protocol on volunteers was aimed at estimating the t1 time constant of muscle tissue both at rest and during moderate aerobic exercise . 
each subject was adequately informed on the experimental protocol and gave written informed consent to the spectroscopic examination . the subjects lay in a supine position on an ergometer made of nonferromagnetic materials and consisting of a support table upon which two independent pedals are hinged [ 25 ]  . 
power output was measured with appropriate force and position transducers applied to the ergometer . in the spectroscopy measurements , the surface coil was applied to the subjects right leg at the level of the medial gastrocnemius muscle . 
the protocol involved repeating the rest / exercise sequence three times , with an interval of at least 5 min between the repetitions , each phase lasting about 7 min measured using a chronometer . 
in the exercise phases , acquisition of the spectra was started at least 10 s after the beginning of the exercise . data processing after acquisition , the spectra were transferred to a workstation ( o2 , silicon graphics , usa )  . 
i parametri dei 3 protocolli corti sono stati fissati in modo che essi fossero molto diversi fra loro , pur soddisfacendo le seguenti condizioni : il tempo totale di ciascun protocollo doveva essere inferionel tempo a disposizione dovevano essere acquisite le informazioni per il maggior numero possibile di tr ; per ogni diverso valore di tr dovevano essere acquisiti alre a 8 minuti ; meno 16 fid . con il primo protocollo ( protocollo a ) sono stati acquisiti 6 spettri raccolti con misure distinte , tutte aventi nacq = 16 . il numero di pre - scans diminuiva da 25 per la 1a a 3 per la 6a misura , mentre il tr aumentava , per ciascuna misura , da 601 ms a 5601 ms con incrementi di 1 s . il secondo protocollo ( protocollo b ) ha consentito di raccogliere 107 spettri con 5 serie diverse , tutte effettuate con 1 acquisizione e nessun pre - scan . 
solamente gli ultimi 16 spettri di ciascun tr sono stati utilizzati . con il terzo protocollo ( protocollo c ) sono stati acquisiti 65 spettri con 7 serie distinte , tutte aventi 3 acquisizioni e nessun pre - scan ; le prime due serie hanno fornito 10 spettri , le altre 9 . 
per questo protocollo sono stati considerati solo gli ultimi 6 spettri di ogni tr . protocollo sperimentale in vivo il protocollo sui volontari aveva lo scopo di stimare la costante di tempo t1 del tessuto muscolare sia in condizioni di riposo che durante esercizio aerobico moderato . 
 stato scelto a priori di utilizzare il protocollo di acquisizione c in quanto presentava caratteristiche simili ai parametri di acquisizione utilizzati per gli studi sulla funzione muscolare nelluomo . alla sperimentazione hanno partecipato 4 soggetti sani ( 3 maschi e 1 femmina , di et , massa corporea ed altezza medi rispettivamente di : 25 , 33 , 1 anni , 73 , 511 , 6 kg e 1775 cm ( ds ) ) nessuno dei quali svolgeva attivit fisica abituale e / o con intenti sportivi . 
ogni soggetto stato adeguatamente informato sul protocollo sperimentale ed ha sottoscritto il consenso informato allindagine spettroscopica . i soggetti erano distesi supini su un apposito ergometro costruito con materiali non ferro - magnetici , formato da una tavola , che funge da supporto , sulla quale sono imperniati due pedali indipendenti [ 25 ]  . 
con i piedi vincolati ai pedali , i volontari effettuano un lavoro compiendo delle flessioni plantari che estendono gli elastici applicati sullergometro . per la presente sperimentazione le flessioni erano sincrone , alla frequenza di 50 battute al minuto e per unestensione di circa 30 gradi . 
la potenza istantanea sviluppata stata misurata attraverso appositi trasduttori di forza e di posizione applicati sullergometro . per le misure di spettroscopia , la bobina di superficie stata applicata sulla gamba destra dei soggetti , a livello del muscolo gastrocnemio mediale . 
the area under a precise spectrum peak , and its position were determined with the time - domain varpro fitting routine of the mrui software [ 26 ] using the appropriate starting values and without any prior conditions . the single peak for both 1h and 31p was considered for the spectra obtained on the phantom whereas the water ( for 1h ) and phosphocreatine and inorganic phosphate peaks ( for 31p ) were evaluated for the spectra obtained in vivo . 
for protocol c , considering the greater temporal complexity of the sequence used , the s values were interpolated with two modified models : s ( tr ) = s0 ( cid : 2 ) 1 - b e 2tr + ( cid : 3 ) + 2s0 ( cid : 2 ) 1 - b e tr ( cid : 3 ) data acquired for every volunteer were processed separipetere tre volte , con un intervallo di attesa di almeno 5 minuti tra luna e laltra , la successione riposo - esercizio della durata di circa 7 minuti ciascuno , controllato mediante un cronometro . 
nei periodi di esercizio la registrazione degli spettri iniziata almeno 10 s dopo linizio dellesercizio . trattamento dei dati dopo lacquisizione , gli spettri sono stati trasferiti su una stazione di lavoro ( o2 , silicon graphics , usa )  . 
successivamente , lintensit di segnale s , ovvero larea sottesa da un preciso picco spettrale e la sua posizione sono state determinate nel dominio temporale tramite il sottoprogramma di fitting varpro del software mrui [ 26 ] , utilizzando gli appropriati valori iniziali e senza limposizione di condizioni a priori . 
per gli spettri ottenuti sul fantoccio stato considerato lunico picco presente sia per l1h che per il 31p , mentre per gli spettri ottenuti in vivo sono stati valutati il picco dellacqua ( per l1h ) e quelli della fosfocreatina e del fosforo inorganico ( per il 31p )  . 
la distanza ( in p.p.m. ) fra il picco della pcr ed il picco del pi ha consentito di calcolare il valore del ph utilizzando la seguente formula [ 14 , 27 ] : ph = 6 , 75 + log 3 , 27 5 , 69 i diversi valori di s calcolati per il 31p allo scopo di determinare il t1 apparente sono stati approssimati , per tutti i protocolli , attraverso due modelli matematici , in funzione del parametro temporale t specifico del protocollo in esame : s ( t ) = s0 ( cid : 2 ) 1 - bet t1 ( cid : 3 ) il primo modello ha interpolato i valori secondo una curva esponenziale semplice , imponendo b = 1 , e quindi restavano da determinare i parametri s0 e t1 . 
il secondo modello , al fine di compensare il fatto che limpulso rf di eccitazione non investe uniformemente il campione indagato , ha utilizzato una funzione esponenziale saturata , in cui era da stimare anche il coefficiente di correzione di saturazione b , che dovrebbe risultare compreso tra 0 e 1 [ 22 ]  . per il protocollo lungo eseguito sul fantoccio , le 13 intensit di segnale s sono state interpolate con i due modelli matematici , assumendo come tempo t il tempo di misura di ciascuno spettro ( t = tmis = 2tr + ) , variabile da 2 , 46 s a 14 , 46 s con incrementi di 1 s . 
per confronto , la stessa metodologia di analisi stata applicata utilizzando solamente le intensit di segnale s acquisite con i 5 tr pi piccoli . i dati raccolti con i tre protocolli corti sono stati elaborati mediante analisi specifiche per ciascuno di essi . 
il segnale di ogni spettro acquisito con il protocollo a per ciascuno dei 6 diversi valori di tr stato diviso per il numero di acquisizioni ( n = 16 )  . 
 all statistical evaluations and interpolations were carried out with the spss software ( spss inc . , chicago , il , usa )  . the probability value p = 5% was assumed to indicate statistical significance . 
per il protocollo b , i valori s sono stati interpolati con i due modelli matematici assumendo come tempo t il tempo di misura di ciascuno spettro ( t = tmis = 2tr + ) , variabile da 2 , 46 s a 3 , 66 s con incrementi di 0 , 2 s . 
per il protocollo c , considerando la maggiore complessit temporale della sequenza utilizzata in questo test per lacquisizione degli spettri , i valori di s sono stati interpolati con due modelli modificati : s ( tr ) = s0 ( cid : 2 ) 1 - b e 2tr + ( cid : 3 ) + 2s0 ( cid : 2 ) 1 - b e tr ( cid : 3 ) results in vitro estimation of t1 the values of signal s obtained with the 13 different trs during a repetition are illustrated in figure 1 , which also depicts the curves described by the two different mathematical models , using as parameters t1 , s0 , and b those obtained by the nonlinear regression estimation on the same data . 
t1 and s0 values obtained with the two mathematical models were significantly different ( wilcoxon test , n = 6 , p < 0.05 ) , using both the complete set of values and only five values . 
the estimation performed by applying the simple exponential model to just five data gave significantly lower results ( wilcoxon test , n = 6 , p < 0.05 ) than by applying the same model to 13 values . i dati acquisiti su ogni volontario sono stati elaborati separatamente per ciascuna ripetizione del protocollo , mantenendo distinte le informazioni ottenute durante i periodi di riposo e di esercizio , ottenendo quindi per ciascun soggetto 6 set di spettri . 
 tutte le valutazioni statistiche e le interpolazioni sono state effettuate tramite il software spss ( spss inc , il , usa )  . il valore di probabilit p = 5% stato assunto come soglia di significativit statistica . 
sono riassunti i risultati ottenuti applicando entrambi i modelli matematici , utilizzando , per le stime , tutti i 13 valori a disposizione oppure solamente i 5 dati acquisiti con minore tr stima su 13 dati stima su 5 dati v . 
see text for details tabella 2 valori medi ( ds ) del tempo impiegato per una successione completa di misure e parametri t1 , s0 , r2 e b ( quando opportuno ) , stimati applicando i due modelli matematici ai dati ottenuti sul fantoccio con i tre diversi protocolli corti di acquisizione ( a , b e c ) protocollo a protocollo b protocollo c a valori medi di 3 sole ripetizioni . 
vedi testo per i dettagli una ripetizione sono illustrati nella figura 1 , in cui sono rappresentate anche le curve descritte dai due diversi modelli matematici , utilizzando come parametri t1 , s0 e b quelli ottenuti dalle stime per regressione non lineare sugli stessi dati . 
la tabella 1 riporta i valori medi dei parametri stimati con entrambi i modelli matematici , utilizzando tutti i 13 valori a disposizione oppure solamente quelli corrispondenti ai cinque tr pi piccoli . i valori di t1 e quelli di s0 ottenuti con i due modelli matematici sono risultati significativamente diversi ( test di wilcoxon , n = 6 , p < 0 , 05 ) , sia utilizzando lintera serie di valori che solamente 5 dati . 
le stime effettuate applicando il modello esponenziale semplice su 5 soli dati hanno fornito risultati significativamente inferiori ( test di wilcoxon , n = 6 , p < 0 , 05 ) rispetto allo stesso modello applicato su 13 valori . la tabella 2 riassume i tempi medi di esecuzione dei tre diversi protocolli corti ( a , b e c ) ed i parametri t1 , s0 e b ottenuti applicando i due modelli matematici , oltre al valore medio dei coefficienti di determinazione r2 . 
la curva continua e quella spezzata sono rispettivamente quelle predette attraverso il modello esponenziale semplice ed esponenziale saturato applicati agli stessi dati . table 2 summarises the mean time required for the three different short protocols ( a , b , and c ) and the parameters t1 , v . 
the t1 constant and the s0 values estimated with the simple exponential model are significantly smaller for protocol c ( kruskal - wallis test , n = 18 ; p < 0.005 for both parameters )  . 
 for protocol a , both the t1 constant and the s0 values estimated through the simple exponential are significantly lower than those predicted with the saturated exponential model ( wilcoxon test , n = 6 , p < 0.05 for both parameters )  . 
indeed , the nonlinear regression procedure succeeded in concluding the estimation of the saturated exponential model parameters in a finite number of iterations ( < 300 ) in only one case for protocol b ( for which , however , the value of coefficient b is meaningless : b = 7.96 ) and in only three out of six repetitions of protocol c . in vivo experimentation figure 2 illustrates , for a typical subject , the mean spectra obtained with different tr values during one of the three repetitions , both at rest ( a ) and during exercise ( b )  . 
it can be seen that compared to rest , the spectra obtained during exersui dati dei protocolli b e c non stato effettuato alcun test statistico di confronto , data la bassa numerosit dei risultati ottenuti con lesponenziale saturata . 
si pu notare che rispetto al riposo , gli spettri ottenuti durante esercizio presentano il picco della fosfocreatina pi piccolo e quello del fosforo inorganico pi grande , mentre le righe spettrali dellatp sono rimaste pressoch invariate . 
la stima dei parametri con il modello esponenziale saturata si conclusa con valori accettabili ( b1 ) solamente in 2 prove su 12 sia per i dati acquisiti a riposo che per quelli registrati durante esercizio . 
la stessa tabella riassume anche i valori di potenza e ph intratable 3 average values ( sd ) of parameters t1 , s0 and r2 obtained with the simple exponential model on volunteers . 
summary of average power developed by the right leg during exercises and intracellular ph calculated for the two conditions tabella 3 valori medi ( ds ) di t1 , s0 e r2 ottenuti con il modello esponenziale semplice sui volontari . 
2a , b spettri medi ricavati dagli ultimi 6 spettri acquisiti da un soggetto in funzione dei 7 tempi di ripetizione utilizzati : a a riposo , b durante esercizio . cise have a lower phosphocreatine peak and a higher inorganic phosphate peak whereas the atp spectrum lines are virtually unchanged . 
table 3 shows the mean t1 and s0 values obtained for phosphocreatine with the simple exponential model in resting and exercise conditions . the estimation of parameters with the saturated exponential model ended with acceptable values ( b1 ) in only two tests out of 12 for data acquired during both rest and exercise . 
table 3 also summarises power and intracellular ph values in both conditions . the kruskall - wallis test revealed that there were no significant differences in t1 and ph values between rest and exercise ( n = 24 , p = ns for both parameters )  . 
furthermore , for each tr , the first spectra collected were discarded for an overall time more than three times the hypothetical t1 = 6 s [ 22 ] , this to ensure that all data came from a sample under saturated conditions . the two mathematical models used to estimate the t1 are based on different physical interpretations of the systethe saturated exponential model describes better the phenomecellulare nelle due condizioni . 
al contrario , il valore di s0 durante esercizio risultato significativamente inferiore rispetto a quello a riposo ( test di kruskall - wallis a 1 coda , n = 24 , p < 0 , 05 ) , con una differenza , in media , dell11 , 3% . discussione stima del t1 in vitro una stima attendibile del t1 possibile solamente se le informazioni sono state ottenute su un ampio range di valori di tr e se , per ciascuno di essi , stato raccolto un numero sufficiente di spettri , tale da garantire le condizioni di saturazione ed un buon rapporto segnale - rumore . 
inoltre , sono stati scartati , per ciascun tr , i primi spettri raccolti , per un tempo complessivo superiore a 3 volte il t1 presunto di 6 s [ 22 ] , a garanzia che tutti i dati provenissero da un campione in condizioni saturate . 
i valori di t1 stimati con questo modello sono risultati circa doppi rispetto allesponenziale semplice , mentre i valori di s0 sono risultati simili , anche se quelli ottenuti con lesponenziale semplice sono sistematicamente minori ( tabella 1 )  . 
t1 values estimated with this model were almost double compared with the simple exponential whereas the s0 values were similar , even though those obtained with the simple exponential are systematically lower ( table 1 )  . 
furthermore , we tried to obtain the same signal - to - noise ratio as with the long protocol by having at least 16 readings of the relaxation signal for every tr value . the t1 and s0 values calculated by applying the simple exponential model to the data obtained with all three protocols ( a , b , and c ) are smaller than the corresponding parameters obtained with the long protocol . 
this result may be partially explained by the lower extension and lower maximum values of the trs under study with these protocols . furthermore , protocol c , despite the use of a modified version of the mathematical models allowing for the greater complexity of the acquisition , provided decidedly lower parameters than those obtained with protocols a and b . 
estimation of parameters , through saturated regression , on the data of protocol a gave higher values than those obtained with the simple exponential curve ( table 2 ) , similarly to what has been observed for the long protocol , in which the tr extension was larger . 
moreover , the power developed by the subjects with their right legs alone was lower than that reported by other authors as being the threshold for lactate production , namely 4.84.6 w [ 12 , 28 ]  . it should be noted that the time constant t1 during exercise can be estimated only if pcr - splitting processes which occur at the beginning of the exercise are no longer underway , i.e. 
anche per i protocolli corti stata garantita la condizione di saturazione , inserendo un adeguato numero di pre - scan o scartando degli spettri , nonostante i limiti di tempo imposti . 
inoltre , si cercato di ottenere lo stesso rapporto segnale - rumore del protocollo lungo , mantenendo ad almeno 16 il numero di letture del segnale di diseccitazione per ogni valore di tr . i valori di t1 e di s0 , calcolati applicando il modello esponenziale semplice ai dati ottenuti con tutti e tre i protocolli ( a , b e c ) , sono pi piccoli dei corrispondenti parametri ottenuti dal protocollo lungo . 
questo risultato pu essere parzialmente spiegato dalla minore estensione e dai valori massimi pi piccoli dei tr indagati con questi protocolli . inoltre il protocollo c , nonostante lutilizzazione di una versione modificata dei modelli matematici che tenga conto della maggiore complessit dellacquisizione , ha fornito parametri decisamente inferiori rispetto ai protocolli a e b . 
ci pu essere un indice del fatto che , in sequenze rm di acquisizione temporalmente pi complesse , altri fattori , oltre al t1 , possono essere importanti nel determinare lintensit del segnale raccolto . la procedura di stima dei parametri dellesponenziale saturata non riuscita a terminare correttamente per tutte le ripetizioni del protocollo b e per la met delle ripetizioni del protocollo c . 
la stima dei parametri , mediante regressione saturata , sui dati del protocollo a ha fornito valori superiori a quelli ottenuti tramite lesponenziale semplice ( tabella 2 ) , analogamente a quanto gi osservato per il protocollo lungo , in cui lestensione di tr indagata era maggiore . sperimentazione in vivo gli esperimenti condotti sui volontari sono stati eseguiti in modo da ottenere le informazioni relative alla costante di tempo t1 del muscolo gastrocnemio sia in condizioni di riposo che durante esercizio aerobico . 
questultima condizione stata raggiunta , in quanto non c stata variazione nei valori di ph fra la condizione di riposo e quella di esercizio . inoltre , la potenza sviluppata dai soggetti con la sola gamba destra risultata minore della potenza riportata da altri autori come soglia di produzione del lattato , pari a 4 , 84 , 6 w [ 12 , 28 ]  . va sottolineato che la stima della costante di tempo t1 in corso di esercizio possibile esclusivamente se non sono pi in atto i processi di scissione della pcr che avvengono allinizio dellesercizio , cio la concentrazione della pcr deve rimanere costante . 
precedenti studi [ 11 , 2931 ] hanno descritto il processo di scissione della pcr con un andamento esponenziale , la cui costante di tempo risulta di circa 20 s . assumendo tale costante di tempo e che il segnale della pcr durante esercizio aerobico diminuisca al massimo del 20% v . 
assuming such a time constant and that the pcr signal during aerobic exercise drops by a maximum of 20% compared with the rest phase [ 12 , 28 ] , after 30 s from the start of the process , the remaining signal will be around 85% of the rest signal instead of 80% . 
the 10 - s wait before beginning acquisitions and the time required for acquisition of the spectra to be discarded ensured an interval from the beginning of the exercise of at least 30 s . the relative decline of the s0 value of pcr between rest and exercise , estimated with the simple exponential model , is around 11.3%. 
moreover , during exercise , the signal comes from spectra collected during movement of the limb , a source of noise due to the noncomplete homogeneity of the main magnetic field b0 or to morphological changes of the muscle . 
this value is comparable with the value reported at rest by newcomer ( 5.6 s ) under the same acquisition conditions ( b0 = 1.5 t with surface coil [ 22 ] )  . rispetto al riposo [ 12 , 28 ] , dopo 30 s dallinizio del processo il segnale residuo sar circa l85% di quello a riposo , invece dell80% . 
i 10 s di attesa prima di iniziare le acquisizioni , assieme al tempo impiegato per lacquisizione degli spettri da scartare , hanno garantito un intervallo dallinizio dellesercizio di almeno 30 s . la diminuzione relativa del valore di s0 della pcr fra riposo ed esercizio , stimato con il modello esponenziale semplice , di circa 11 , 3% . 
inoltre , durante esercizio , il segnale proviene da spettri raccolti durante il movimento dellarto , che fonte di rumore dovuto alla non perfetta omogeneit del campo magnetico principale b0 od a modifiche morfologiche del muscolo . 
il valore di probabilit del test statistico ( p = 0 , 722 ) e la relativamente piccola deviazione standard , rassicurano sul fatto che la costante di tempo effettivamente non cambia tra le due condizioni . 
di conseguenza , negli studi di quantizzazione della pcr , appropriato utilizzare lo stesso coefficiente di correzione sia per il riposo che per lesercizio . la costante spin - reticolo misurata sul muscolo in vivo con la presente sperimentazione stata ottenuta con una sequenza rm complessa , risultando essere di 0 , 91 s . 
supponendo che le procedure di analisi abbiano introdotto gli stessi errori sistematici sia nei dati acquisiti in vivo che in quelli ottenuti in vitro , si pu calcolare il valore teorico ottenibile in condizioni ideali , a parit di modello esponenziale semplice . 
utilizzando la costante di tempo t1 ottenuta in vitro con il protocollo lungo ( 3 , 84 s ) ed il valore di t1 ottenuto in vitro a parit di protocollo di acquisizione ( protocollo c ; 0 , 61 s ) , il valore vero del t1 apparente della pcr in vivo pu essere calcolato come : 0 , 91 ( 3 , 84 / 0 , 61 ) = 5 , 73 s . 
tale valore sovrapponibile a quello riportato da newcomer a riposo ( 5 , 6 s ) nelle stesse condizioni di acquisizione ( b0 = 1 , 5 t con bobina di superficie [ 22 ] )  . conclusions conclusioni the main purpose of our work was to estimate the time constant t1 during aerobic exercise using a clinical mr scanner . lo scopo principale del presente lavoro era di stimare la costante di tempo t1 durante esercizio aerobico , utilizzando un v . 
franchi maggi 5 , i - 27100 pavia , italy , tel . : + 39 - 038 - 5022838 , fax : + 39 - 038 - 5028597 , e - mail : g.beluffi@smatteo.pv.it received : 11 july 2005 / accepted : 18 october 2005 / published online : 11 april 2006 abstract purpose . 
among the 16 , 326 patients who underwent x - ray study of the hands , nine ( six males and three females , 0.055% of the total ) presented the typical radiological features of kirners deformity ; no patient had a family history of the disorder except for one , in whom the suspicion of familiarity could not be verified radiologically . 
although rare , as also shown by our study , kirners deformity must be recognised and properly diagnosed in order to spare the subject unnecessary surgical procedures . key words kirners deformity dystelephalangy nail phalanx riassunto obiettivo . 
il portatore non lamenta generalmente n dolore n impotenza funzionale delle dita : al massimo denunciata una difficolt a compiere particolari movimenti . allesame radiologico la falange ungueale del v dito ( quasi sempre bilateralmente ) composta da una epifisi la cui porzione distale , di solito dal lato palmare , pu presentare un piccolo sprone osseo . 
la diafisi pi piccola che di norma , incurvata in senso palmare , deviata di 1050 dallasse normale in senso radiale , e non saldata con lepifisi , con possibile e frequente aumento dello spazio epifisometafiso - diafisario . la struttura ossea in corrispondenza della zona epifiso - metafisaria presenta talvolta segni di sclerosi , in particolare in corrispondenza della porzione metafisaria ungueale . 
distal phalanx bilateral changes are more pronounced on the left side where the shaft is more bent towards the palm ( a , b ) than on the right side ( c , d ) in relation to the dysmorphic epiphysis . 
alterazione bilaterale della falange ungueale con aspetto pi angolato della diafisi dal lato sinistro ( a , b ) , meno evidente a destra ( c , d ) con aspetto tozzo dellepifisi basale . 
fiori : clinical and radiological findings in kirners deformity patients and methods pazienti e metodi at our paediatric radiology section , an average of 1 , 040 wrist and hand x - ray films are taken each year , not only to study bone age but also to assess morphologic and pathologic changes in the presence of trauma , haematological disorders , bone syndromes and dysplasias , dysmorphic features , rheumatic disorders , etc . 
over a period of 23.5 years a total of 23 , 996 such procedures were performed with an average of 36% follow - up examinations without significant differences between males and females . 
ba : a boy aged 13 years and 5 months , karyotype 46 xy , with hypophyseal dwarfism , referred for radiological assessment of bone age , which corresponded to 10.5 years according to greulich and pyle ( g&p ) [ 10 ] standards . 
hm : a boy aged 9 years and 11 months , karyotype 46 xy , referred for bone - age evaluation ( equal to 9.5 years according to g&p ) for suspected fetal alcohol syndrome . 
sf : a girl with turners syndrome , karyotype 46 xo , seen for the first time at the age of 2 years and 3 months for evaluation of bone age ( 1 year and 10 months )  . 
a very small epiphysis appeared at the age of 5 years and 1 month , and the presumptive diagnosis of kirners deformity was confirmed when the girl was 8 years and 2 months . 
in 23 anni e mezzo sono stati eseguiti 23.966 radiogrammi di questo tipo con una percentuale di controlli nel tempo del 36% , senza significative differenze tra maschi e femmine . 
s.f. , femmina affetta da sindrome di turner , con cariotipo 46 xo , che allet di 2 anni e 3 mesi esegue il primo radiogramma del carpo per la determinazione dellet scheletrica ( pari ad 1 anno e 10 mesi )  . 
sin dal primo controllo si osserva dismorfia della falange ungueale del v dito che spiccatamente ipoplasica rispetto a quella delle altre dita , lievemente incurvata in senso radiale , con comparsa della epifisi ( puntiforme ) al controllo eseguito allet di 5 anni e 1 mese e definizione certa della anomalia di kirner al controllo intorno agli 8 anni e 2 mesi di vita ed in quelli successivi . 
3a - h changes over time of kirners deformity between age 2 years and 3 months and 13 years and 4months in a patient affected by turners syndrome . the first x - ray film shows lack of the epiphysis and a dysmorphic , hypoplastic phalanx shaft slightly bent towards the radial side ( a )  . 
follow - up x - ray films show the appearance of a small epiphysis at the age of 5 years and 1 month ( b ) , which slowly enlarges ( c ) , becoming stubby and dysmorphic with the typical appearance of kirners deformity at the age of 8 years and 2 months ( d )  . 
3a - h evoluzione nel tempo della anomalia di kirner dallet di 2 anni e 3 mesi a quella di 13 anni e 4 mesi in portatrice di sindrome di turner . 
comparsa di una piccola epifisi a 5 anni e 1 ese ( b ) con successivo ingrandimento della stessa ( c ) , tozza e dismorfica , che assume laspetto tipico dellanomalia di kirner allet di 8 anni e 2 mesi ( d ) con aspetto sempre pi evidente nei successivi controlli ( e , f ) , fino allultimo allet di 13 anni e 4 mesi ( g , h ) in cui lepifisi tozza , con sprone al suo margine infero - superiore e la diafisi angolata . 
affected by acute lymphatic leukaemia ( all ) , he first underwent an x - ray study of his left hand at the age of 14 years in order to establish bone age ( equal to 12 years ) as a follow - up in the treatment protocol of his disease . 
r.a. , maschio , cariotipo 46 xy , dellet attuale di 17 anni , portatore di lla stato sottoposto per la prima volta allet di 14 anni allo studio rx per la determinazione dellet scheletrica ( pari a 12 anni ) , quale controllo nel contesto del protocollo terapeutico della emopatia da cui era affetto . 
la falange distale del v dito appariva corta e tozza con deviazione volare e presentava una unghia dismorfica a vetrino dorologio . il controllo radiologico dimostr una epifisi falangea regolare g . 
the same findings were detected in the right hand . in all nine patients , the distal phalanges of the little fingers had a stubby , dysmorphic appearance with palmar and radial bending and showed dysmorphic , eagle - claw - like nails . 
in contrast , the x - ray findings in the other eight patients were typical for kirners deformity : bending of nail - phalanx shaft , irregular diaphyseal thickening with loss of normal bone texture and straight epiphysis with a spur on the volar surface projecting towards the shaft where it fits into a groove . ed una diafisi piccola e deviata medialmente con aspetto quasi ad uncino , tipico della anomalia di kirner . 
in tutti e 9 i pazienti le falangi distali del v dito della mano presentano un aspetto tozzo , deviazione in senso palmare e radiale ed unghia corta e dismorfica . 
nei rimanenti 8 pazienti , il quadro radiologico risultava essere quello tipico della anomalia di kirner documentato da : incurvamento della falange ungueale , irregolare addensamento struttura ossea diafisaria , epifisi mai incurvata , ma dotata di sprone ( becco ) , al quale corrisponde una incisura metafisaria , scavata quasi a colpo dunghia e con aspetto chiaramente dismorfico dellunghia . discussion and conclusions in all nine cases ( one of which was already reported [ 9 ] ) , there were no doubts about the diagnosis . 
all nine displayed the typical clinical and radiological features of kirners deformity ( dysmorphic , painless deformity of nail phalanges with bent shafts ) associated with delayed bone age , except in case 2 . 
both the clinical and especially radiological diagnosis in these cases , as well as in the other cases reported in the literature , are straightforward and can usually be made between 8 and 14 years of age ( 6 and 14 in the present series ) [ 18 , 10 , 1228 ]  . discussione e conclusioni in tutti e nove i casi da noi osservati ( di cui uno gi descritto ) [ 9 ] non possono sorgere dubbi sulla diagnosi . 
sono infatti riscontrabili clinicamente e radiologicamente le alterazioni gi descritte e tipiche della sindrome di kirner ( dismorfia della falange ungueale del v dito non accompagnata da sintomatologia dolorosa , incurvamento , malformazione radiologica tipica ) , associate ad un ritardo , pi o meno evidente , della maturazione scheletrica , ad eccezione del caso n . 
4 paziente affetto da lla : evoluzione nel corso di 3 anni ( dallet di 14 a quella di 17 anni ) della anomalia di kirner con progressiva riduzione della cartilagine di coniugazione e persistente deviazione mediale della diafisi , dallaspetto quasi ad uncino . even though kirners deformity involves swelling and a stubby appearance of the little fingers , it is usually painless . 
in only four cases reported in the literature were symptoms present : two , reported by staheli [ 18 ] had dull , aching pain and progressive myositis ossificans ; and two , reported by dykes [ 23 ] had pain for a few months and nail phalanx redness . the deformity is usually sporadic but may be inherited as an autosomal dominant trait [ 17 , 29 ] with scarce or incomplete penetrance [ 22 ]  . it affects females more frequently than males with a 2 : 1 ratio and is often associated with delayed bone age . 
dystelephalangy changes were reported in some members of the mothers family but not in the fathers , so the girl has to be considered heterozygous for the deformity [ 30 ]  . there is no agreement about the aetiopathogenesis of kirners deformity , which is still unknown and controversial [ 17 , 2931 ] , with hypotheses being : juvenile osteomalacia [ 5 ] ; aseptic necrosis on the basis of biopsy findings , which showed lysis between the diaphysis and epiphysis of the terminal phalanx with diminished trabecular bone and decreased thickness of the zone of provisional calcification [ 15 ] ; osteochondrosis of possible vascular origin [ 7 ]  . 
recently , it has been suggested that kirners deformity is a congenital defect of growth - cartilage to be classified among the genotypic osteochondrodysplasias ( such as a epiphyso - metaphyseal acrodysplasia ) [ 4 , 26 , 31 ]  . in the only case in the literature studied by magnetic resonance imaging ( mri ) , it has been suggested that a chronic inflammatory disorder or vascular dysfunction of the soft tissues of the distal phalanges could be the cause of the deformity [ 30 ]  . this hypothesis has been criticised on the grounds of technical artefacts during mri examination [ 32 , 33 ]  . 
our cases provide no information to confirm or refute the above hypotheses , nor do they suggest an alternative hypothesis . the apparently positive family history in one ( case 3 ) suggests the hereditary nature of the deformity . significant reports from the point of view of heredity are g . 
fiori : clinical and radiological findings in kirners deformity di osservazione variabile tra gli 8 ed i 14 anni ( nei nostri pazienti tra i 6 ed i 14 anni ) semplice e non dovrebbe far sorgere dubbi [ 18 , 10 , 1228 ]  . 
 [ 18 ] erano presenti disturbi clinici e soggettivi : in uno , in forma di marcata dolorabilit , nellaltro associata ad una miosite ossificante progressiva , ed in due di quelli descritti da dykes arrossamento e dolore per brevi periodi di tempo [ 23 ]  . 
lanomalia presenta in genere caratteri di sporadicit o di familiarit secondo una modalit di trasmissione autosomica dominante [ 17 , 29 ] a bassa od incompleta penetranza [ 22 ] e colpisce pi frequentemente le femmine dei maschi , con un rapporto di 2 : 1 , associandosi in genere ad un ritardo della maturazione scheletrica . 
di raro riscontro in america ed in europa ( 0 , 055% nella nostra casistica ) , con la sola eccezione dellinghilterra , ove raggiunge una incidenza dello 0 , 25% [ 29 ]  . 
lo stesso autore ha descritto un caso di distelefalangia esteso a quasi tutte le dita ( esclusi i pollici e lindice della mano destra ) come possibile espressione di uno stato omozigote del gene responsabile , poich verificatosi in una paziente in cui genitori ed il nonno materno ( nonch un fratello ) risultavano portatori di deformit di kirner bilaterale [ 8 ]  . un altro caso di distelefalangia politopica di tutte le dita ( una bambina con iniziale interessamento delle falangi distali allet di 2 mesi ed espressione completa dellalterazione a 5 anni ) stato descritto recentemente da brune [ 30 ]  . 
circa leziopatogenesi della anomalia , ancora oscura e fonte di discussione [ 17 , 29 , 30 , 31 ] , sono state fatte alcune ipotesi : da una osteomalacia giovanile [ 5 ] , ad una necrosi asettica [ 15 ] , giustificata da un reperto istopatologico post - bioptico , che ha dimostrato solo unirregolarit della zona di passaggio tra cartilagine e zona diafisaria con riduzione dellosso trabecolare ed in particolare con ridotto spessore della zona di calcificazione provvisoria ; ad una osteocondrosi di natura vascolare [ 7 ]  . 
attualmente lorientamento della letteratura che si tratti di una alterazione congenita della cartilagine di accrescimento nel contesto generale delle ostecondrodisplasie genotipiche ( acrodisplasia epifiso - metafisaria ) [ 4 , 26 , 31 ]  . 
stata avanzata anche lipotesi , nellunico caso studiato con rm , che un processo infiammatorio cronico od una alterazione della vascolarizzazione siano la causa della anomalia [ 30 ]  . 
non vi sono dati utili , nei casi osservati , per confermare o negare una di tali ipotesi , n siamo in grado di poter avanzare una nostra ipotesi eziopatogenetica . 
fiori : clinical and radiological findings in kirners deformity those by blank and girdany [ 17 ] , who described seven cases ( four males and three females ) , all belonging to the same family , and sugiura [ 8 ] , which suggest homozygosity of the deformity ; on the contrary , the case of brune et al . 
per quanto riguarda invece la percentuale pi elevata di manifestazione nelle femmine rispetto ai maschi , con un rapporto 2 : 1 ( addirittura di 5 : 1 nella casistica di dykes ) [ 23 ] , con interessamento quasi sempre bilaterale , mentre nei maschi spesso monolaterale ( lato destro pi del sinistro ) [ 29 ] , non possibile esprimere un giudizio , data lesiguit nel numero dei nostri pazienti , in cui anzi si potrebbe parlare di rapporto invertito maschi / femmine , pari infatti a 6 : 3 ( sei maschi e tre femmine ) e con riscontro bilaterale in tutti i casi . 
lanomalia stata invece segnalata in associazione con una grande variet di malformazioni sia dellapparato scheletrico , quali cifosi e ginocchio valgo [ 1 ] , deformit del dito indice e della metafisi radiale [ 12 ] , aspetto mongoloide [ 2 ] , piede cavo [ 3 ] , osteomielite [ 7 ] e miosite ossificante progressiva [ 18 ] , nonch di quello cardiovascolare ( difetto settale interventricolare , dotto arterioso pervio , difetto settale atriale tipo ostium secundum , stenosi valvolare polmonare [ 29 ] )  . 
nellet adulta la forma evolve con fusione delle due porzioni della falange , lasciando come reliquato solo un danno estetico dovuto allincurvamento od una lieve difficolt ad eseguire quei movimenti che richiedono luso del v dito , come suonare strumenti tipo pianoforte o violino e scrivere a macchina . 
the encouraging results , if validated by larger series , support the use of pet / ct in patients with carcinoma of unknown primary origin and negative conventional imaging results . key words metastatic cancer occult primary cancer 18f - fdgpet / ct riassunto obiettivo . 
la popolazione in studio costituita da 38 pazienti consecutivi con malattia tumorale metastatica provata istologicamente in cui le tecniche di diagnostica per immagini convenzionale erano risultate negative o non conclusive nella identificazione della lesione primitiva . 
the site of the occult primary tumour often remains unidentified after common imaging investigations ( chest x - ray , abdominal and pelvic ct , mammography in women ) ( 20%27% of cases ) [ 1 , 2 ] or autopsy ( 30%82% ) [ 24 ]  . 
reasons for the low rate of detection of the primary cancer include a lesion size smaller than the spatial and contrast resolution of the technique used or involution of the primary mass due to limited angiogenic competence [ 5 ]  . 
conventional contrast studies of the upper and lower digestive tract , for example , have a low diagnostic yield , and mammography , although routinely ordered , is often unhelpful because very few patients with cup have a primary mass in the breast [ 6 ]  . recent papers have reported that the median survival for patients with cup is approximately 12 months and that detection of the primary tumour and initiation of therapy can prolong survival to 23 months [ 7 ]  . 
the aim of this study was to assess the role of 18f - fdg - pet / ct in the identification of occult primary tumours . materials and methods the patient population consisted of 38 consecutive patients ( 22 men , 16 women ; mean age 5911 years , range 4177 years )  . 
the uptake period was 6090 meach patient then underwent a pet / ct scan with a dedicated hybrid scanner ( discovery ls , general electric ; biograph sensation 16 , siemens ) and whole - body scans ; attenuation correction was la sindrome del tumore primitivo occulto ( cup ) consiste nella presenza di una malattia tumorale metastatica per la quale sia impossibile identificare la sede primitiva della neoplasia dopo una attenta indagine anamnestica , esame obbiettivo negativo , negativi gli esami clinico - diagnostici ( emocromo completo , funzionalit renale , epatica , pancreatica , test delle urine , radiogramma del torace , tc addominale e pelvica e mammografia nelle donne , psa negli uomini ) [ 1 ]  . 
nella maggior parte dei casi , impossibile identificare la sede del tumore primitivo occulto con altri esami ( 20%27% ) di diagnostica per immagini pi diffusi ( radiografia del torace , tc addominale e pelvica , mammografia nelle donne ) [ 1 , 2 ] o allautopsia ( 30%82% ) [ 24 ]  . le motivazioni alla base dello scarso potere di identificazione della sede del tumore primitivo comprendono le dimensioni al di sotto del potere di risoluzione , sia spaziale che di contrasto , delle tecniche utilizzate o linvoluzione della massa primitiva a causa di uno scarso potere angiogenetico [ 5 ]  . 
la mammografia , nonostante sia utilizzata nella routine diagnostica , spesso non utile in quanto un limitato numero di pazienti con cup hanno una massa primitiva a livello mammario [ 6 ]  . recenti lavori riportano come la sopravvivenza mediana dei soggetti con cup sia attorno ai 12 mesi e che la identificazione della sede primitiva di malattia con la possibilit di intraprendere un iter terapeutico sposti la sopravvivenza mediana a 23 mesi [ 7 ]  . 
successivamente ogni soggetto stato sottoposto a scansione pet - tc con tomotabella 1 dati clinici , istopatologici e di diagnostica per immagini dei casi con tumore primitivo a livello toracico caso n sesso et , anni biopsia pet / tc tumore occulto dopo pet / tc dimensioni lesione , mm brain metastasis adenocarcinoma supraclavicular node metastasis mediastinal and neck node metastasis adenocarcinoma adenocarcinoma supraclavicular node metastasis sacral vertebra metastasis melanoma adenocarcinoma left humerus metastasis squamous cell carcinoma area of increased uptake in left lung area of increased positive mediastinal and neck nodes , area in right lung positive neck nodes , area of uptake on chest skin multiple areas of uptake in bone and left lung multiple metastases to bone , right adrenal gland , right lung lymph nodes , lung left lung left lung right lung melanoma left lung right lung lung lung laterocervical node spinous cell metastasis brain metastasis carcinoma epithelial carcinoma bone , lung diangostica convenzionale metastasi cerebrale metastasi linfonodo sovraclaveare metastasi linfonodali ( mediastinici e cervicali ) metastasi linfonodo sovraclaveare metastasi ossea vertebra sacrale adenocarcinoma adenocarcinoma adenocarcinoma area di aumentato uptake polmonare sx area di aumentato uptake polmonare sx linfonodi mesiatinici e cervicali , area polmone dx polmone sx polmone sx polmone dx melanoma linfonodi cervicali , area cute torso melanoma adenocarcinoma metastasi omero carcinoma squamocellulare metastasi linfonodali laterocervicali metastasi cerebrale carcinoma spinocellulare carcinoma epiteliale multiple aree captanti a livello osseo e polmonare sx multiple meta . 
the low rate of detection of the primary tumour site has two main causes . first , the size of the primary lesion may be smaller than the resolution power of conventional imaging procedures ( such as ct or gastrointestinal contrast studies ) , or the lesions may be located in sites such as the abdomen , pelvis , head and neck . 
epatiche , area positiva gastrica negativa carcinoma a cellule transizionali adenocarcinoma carcinoma a cellule fusate carcinoma squamocellulare carcinoma squamocellulare negativa linfonodi adiacenti mammella sx area mediastinica ignoto linfonodi cervicali dx ignoto ignoto ignoto ignoto ignoto ignoto carcinoma epiteliale linfonodo ascellare sx ignoto carcinoma epiteliale linfonodo pelvico ignoto adenocarcinoma surrene dx , linfonodi ignoto adenocarcinoma adenocarcinoma mucoide adenocarcinoma mucoide carcinoma epiteliale mano sx area mediastinica ed ossea cute ignoto ignoto cute peritoneo fegato ignoto carcinoma epiteliale cute carcinoma indifferenziato linfonodo mediastinico ignoto ignoto ignoto na , non applicabile suggested that the primary tumour may disappear after having given rise to metastasis because of its angiogenic incompetence , which leads to marked apoptosis and cell turnover [ 5 ]  . whereas no diagnostic procedures can identify a primary lesion that has disappeared due to marked apoptosis , it has been demonstrated that fdg - pet can improve primary - site detection in patients with cup and a negative diagnostic workup . 
although the number of patients in our study was small , our preliminary results show that pet / ct is more sensitive than pet alone , with a 53% detection rate for occult cancers missed by other techniques discussione la cup una sindrome caratterizzata da una prognosi infausta . 
la identificazione della sede primitiva di neoplasia , comunque , pu essere importante in quanto permette di impostare una terapia specifica , migliorando significativamente la prognosi ( 1 anno vs 2 anni ) [ 7 ]  . 
le dimensioni delle lesioni primitive possono essere inferiori al potere di risoluzione delle procedure diagnostiche ( tc o studi contrastografici del tratto gastrointestinale ) o trovarsi in sedi quali laddome , la pelvi , la testa - collo . 
la pet - tc ( sezioni transassiali della pet , tc e immagine di fusione pet - tc ) ha evidenziato unarea di patologico accumulo a livello dellipofaringe ( indicata da freccia nella immagine mip )  . nari di piccole dimensioni [ 1 ]  . 
laltro motivo dipende dalle caratteristiche biologiche del tumore primitivo : stato ipotizzato che la massa tumorale primitiva possa scomparire dopo aver dato luogo a metastatizzazione a causa di uno scarso potere angiogenetico che porta a marcata apoptosi e turn over cellulare [ 5 ]  . mentre nessuna procedura diagnostica pu identificare una lesione primitiva che scomparsa per marcata apoptosi , stato dimostrato come la pet con fdg possa migliorare la identificazione della sede primitiva della lesione in pazienti con cup e una flow - chart diagnostica peraltro negativa . 
al momento presente , sono pochi gli studi che hanno valutato il valore aggiunto della pet - tc rispetto alla fdgpet convenzionale per lidentificazione della sede del tumore occulto [ 810 ]  . 
i nostri risultati preliminari , nonostante il campione sia limitato , mostrano che la pet - tc pi sensibile della pet convenzionale , rilevando il 53% dei tumori occulti che non erano stati evidenziati con le altre tecniche [ 1113 ]  . 
le limitate informazioni morfologiche fornite dalla pet da sola , rendono necessaria lintegrazione con i dati anatomici forniti dalla tc per migliorare la definizione anatomica delle aree di aumentata captazione del tracciante . 
the limited morphological information provided by pet alone requires integration with the anatomical data supplied by ct in order to improve the anatomical definition of the areas of increased tracer uptake . 
pet / ct scanners capture anatomical and functional data in a single registration [ 14 ] , overcoming the limitations of patient repositioning and time interval between scans when the images are fused a posteriori [ 15 ]  . 
the primary tumour was identified in 7 / 29 cases ( two carcinomas of the nasopharynx , one plasmocytoma of the tongue base , one lung carcinoma , two breast cancers ) , showing 24% sensitivity . 
this result is not , however , comparable with our findings because alberini included 22 patients with another positive conventional test : this means that pet provided additional information in 4 / 44 cases only . 
although the population was not selected ( in contrast to our study population ) , the sensitivity of pet was 37.8% , which is significantly lower than that reported in our study . although the heterogeneity of patients could be seen as a potential limitation to our study , with patients referred from different centres and affected by different types of tumours , this fact does not undermine the value of our study , as the diagnostic - therapeutic approach to unknown primary tumours has not yet been codified by international guidelines . 
the head and neck , abdomen and pelvis are highly complex anatomical districts and are characterised by areas of physiological tracer uptake ( for example , by the tonsils , lymphatic tissue , stomach , bowel and ureters )  . small areas of increased uptake due to a small primary tumour may be mistaken for areas of physiological uptake . the careful comparison of metabolic and anatomical information , made possible by pet / ct , considerably improves the sensitivity of the procedure , allowing visualisation of even small areas of asymmetrical tracer distribution or areas of increased focal uptake that would otherwise be considered physiological . 1154 dallintervallo di tempo tra gli scans quando le immagini sono fuse a posteriori [ 15 ]  . 
la sede del tumore primitivo stata identificata in 7 / 29 ( 2 carcinomi del nasofaringe , 1 plasmocitoma della base della lingua , 1 carcinoma polmonare , 2 carcinomi della mammella ) con una sensibilit del 24% . 
questo risultato , comunque , non confrontabile con il nostro studio in quanto alberini ha incluso nel campione 22 soggetti che avevano un altro test convenzionale positivo : questo significa che la pet ha fornito indicazioni aggiuntive solamente in 4 / 44 casi . 
nonostante la popolazione non fosse stata selezionata , al contrario di quella descritta nel nostro studio , la sensibilit della pet risultata del 37 , 8% , che sensibilmente inferiore a quella da noi riportata . sebbene un potenziale limite al presente studio sia rappresentato dal fatto che il campione preso in esame eterogeneo in quanto costituito da pazienti provenienti da centri diversi e portatori di neoplasie di diverso tipo , tuttavia questo non toglie valore allo studio in quanto lapproccio diagnostico - terapeutico in casi di tumore primitivo ignoto non ancora codificato da norme internazionali . 
alcune sedi quali il capo - collo , laddome e la pelvi , sono anatomicamente molto complesse e caratterizzate da varie sedi di fisiologico uptake del tracciante ( per esempio le tonsille , il tessuto linfatico , lo stomaco , lintestino , gli ureteri )  . 
the main cause of acute chest pain , which accounts for 6.5% of urgent medical examinations in emergency rooms in italy , is acute coronary syndrome ( acs )  . 
we performed this prospective study to evaluate the diagnostic accuracy of a 16 - channel computed tomography ( ct ) scanner with dedicated software in a group of patients with chest pain and medium to low risk of acs materials and methods . 
this study involved a selected group of 31 patients reporting chest pain with a medium to low probability of acs , defined on the basis of preliminary tests [ electrocardiogram ( ecg ) and serum cardiac markers ]  . 
msct identified the presence of occlusions and significant ( > 50% ) or nonsignificant stenoses in the main coronary segments , with a sensitivity of 65% , a specificity of 98.8% , a positive predictive value ( ppv ) of 81.2% , a negative predictive value ( npv ) of 97.3% and an accuracy of 96.4%. 
in patients with a medium to low coronary risk , msct is a more accurate indicator of the need for coronary angiography than is exercise stress testing , which is less expensive but has lower predictive values . key words coronary arteries coronarography ct angiography multislice ct riassunto obiettivo . 
causa predominante del dolore toracico acuto , che motiva il 6 , 5% delle visite mediche urgenti effettuate nei pronto soccorso italiani , la sindrome coronarica acuta ( sca )  . 
lo studio analizza laccuratezza diagnostica della tc multistrato ( tc - ms ) a 16 canali in un gruppo selezionato di 31 pazienti con dolore toracico a medio - bassa probabilit di sca , cos definiti in base agli accertamenti preliminari ( elettrocardiogramma e markers biochimici )  . 
utilizzando come gold standard la coronarografia , eseguita nelle 24 ore successive allesame tomodensitometrico , la tc - ms ha identificato nei segmenti coronarici principali la presenza di occlusioni , stenosi significative ( > 50% ) e non ( < 50% ) con sensibilit : 65% ; specificit : 98 , 8% , vpp : 81 , 2% ; vpn : 97 , 3% , accuratezza : 96 , 4% . 
le stenosi significative e le occlusioni sono state invece accertate con sensibilit : 71 , 4% ; specificit : 99 , 6% ; vpp : 93 , 7% ; vpn : 97 , 7% ; accuratezza : 97 , 5% . 
the predominant cause is acute coronary syndrome ( acs ) , the management of which has le visite per dolore toracico acuto rappresentano circa il 6 , 5% di tutte le prestazioni effettuate nei pronto soccorso ( ps ) italiani cos come nelle emergency room statunitensi ; tale percentuale in costante aumento : nel 2000 si attestava al 5 , 1% . 
it has been calculated that in the united states 1 , 200 , 000 coronary angiography examinations are performed each year , 35% of which are followed by a revascularisation procedure . 
even though the morbidity and mortality rates of coronary catheterisation are very low ( 1% and 0.1% , respectively ) , there is a keen interest in alternative , less invasive and less expensive procedures possessing the same diagnostic accuracy in detecting or ruling out acute myocardial infarction ( ami ) and unstable angina . electrocardiogram ( ecg ) , serum cardiac markers and echocardiography can identify subjects with ami , for whom immediate reperfusion is indicated , and those with unstable angina . 
a proportion of patients presenting with chest pain are , however , considered at medium to low risk due to the absence of ischaemic st - segment abnormalities and negative serum markers , and these patients require additional investigations , such as exercise testing [ 1 ]  . 
because the advent of multidetector technology has considerably expanded the diagnostic potential of computed tomography ( ct ) , we performed this prospective study to evaluate the diagnostic accuracy of a 16 - channel ct scanner with dedicated software in a group of patients with chest pain and medium to low risk of acs . materials and methods between november 2004 and october 2005 , we recruited 31 subjects ( 19 men , 12 women ; mean age 59 years , age range 2670 years ) who presented to the emergency department with chest pain that was defined as medium to low probability of acs on the basis of first - line investigations ( ecg , and ischaemia markers : troponin , creatine phosphokinase and myoglobin ) but for whom a clinical suspicion of myocardial ischaemia persisted . 
subjects who had undergone previous myocardial revascularisation procedures or coronary angioplasty , with or without stent placement , were excluded . within 24 h of presentation , all patients ( who had given their informed consent for inclusion ) were studied by multislice ct ( msct ) and coronary angiography . 
further exclusion criteria for the ct study were heart rate > 70 bpm ( even after heart - rate - lowering drugs ) ; arrhythmia ; severe cardiac insufficiency ; pacemaker , defibrillators or valve implants ; history of adverse reactions to contrast material ; renal or respiratory insufficiency ; and pregnancy . the risk factors of the 31 patients selected for the study were hypertension ( 17 ) , cigarette smoking ( 6 ) , dyslipidaemia ( 6 ) , family history of ami ( 4 ) and diabetes ( 2 )  . 
all patients with heart rate higher than 65 bpm were treated with a heartrate - lowering agent ( metoprolol 100 mg / day ) whereas those with borderline heart rates around or just above 65 bpm received a - blocker ( metoprolol tartrate 5 mg ) intravenously 15 min before the examination . the ct study was performed with a 16 - channel multidetector scanner ( sensation cardiac , siemens ) using the following parameters : collimation 0.75 mm , voltage 120 kvp , rotation time 375 ms , slice thickness 0.75 mcardiac acacuta ( sca ) , nei cui confronti da una gestione attendista si passati ad una strategia aggressiva che prevede limmediata esecuzione di unindagine coronarografica e di uneventuale angioplastica . 
ancorch il cateterismo coronarico comporti una morbilit ed una mortalit assai ridotte ( rispettivamente nellordine dell1% e dello 0 , 1% ) permane alto linteresse per procedure alternative che assicurino non - invasivit e riduzione dei costi economici , identificando o escludendo con equivalente accuratezza diagnostica linfarto miocardico acuto ( ima ) e langina instabile . elettrocardiogramma , markers biochimici , ecocardiogramma consentono di individuare sia i soggetti con ima , nei quali generalmente indicata una terapia immediata di riperfusione , sia quelli con angina instabile . 
esiste , tuttavia , una quota di pazienti con dolore toracico definiti a mediobasso rischio , per lassenza di alterazioni ischemiche del tratto st dellelettrocardiogramma e la negativit dei markers biochimici , nei quali si rende necessaria lesecuzione di altre indagini , che attualmente consistono in test da stress [ 1 ]  . 
poich lintroduzione della tecnologia multidetettore ha comportato un incremento notevole delle potenzialit diagnostiche della tc , ci siamo proposti , in questo studio prospettico , di valutare laccuratezza diagnostica di una apparecchiatura a 16 canali e software dedicato in un gruppo di pazienti con dolore toracico a medio - basso rischio di sca . materiali e metodi nel periodo compreso tra novembre 2004 e ottobre 2005 , sono stati reclutati 31 soggetti ( 19 maschi , 12 femmine ; et media 59 anni con range : 2670 anni ) pervenuti allosservazione in ps per dolore toracico definito a medio - bassa probabilit di sca in base alle indagini di prima istanza ( tracciato elettrocardiografico e markers di ischemia : troponina , creatinfosfochinasi e mioglobina ) ma nei quali persisteva il sospetto clinico di ischemia miocardia . 
nellarco di 24 ore dalla presentazione in ps , tutti i pazienti ( dai quali era stato ottenuto il preventivo consenso informato per linserimento nel presente studio ) sono stati sottoposti a esame tc multidetettore ( tc - md ) e coronarografia . 
ai fini dellindagine tomodensitometrica altri criteri di esclusione sono stati : frequenza cardiaca ( fc ) > 70 bpm ( anche dopo bradicardizzazione farmacologia ) ; aritmia ; insufficienza cardiaca grave ; presenza di pacemaker , defibrillatori o protesi valvolari ; pregresse reazioni avverse al mezzo di contrasto ; insufficienza renale o respiratoria ; stato di gravidanza . nel gruppo selezionato di 31 soggetti i fattori di rischio 1055 l . 
coronary angiography images were obtained with volume rendering ( vr ) and curvilinear multiplanar reconstruction ( mpr ) three - dimensional ( 3d ) techniques . in the comparison between msct and coronary angiography , the latter being considered the gold standard , we evaluated 16 coronary segments according to the american heart association classification [ 3 ]  . 
two operators , one radiologist and one cardiologist , independently evaluated each segment for assessability and image quality ( excellent , fair and poor ) and the presence of occlusions and stenoses , which they ranked as nonsignificant ( 50% ) or significant ( 51%99% ) based on a subjective visual judgement for msct and a quantitative judgement for coronary angiography [ 4 ]  . results at msct , 383 ( 81.7% ) of the 469 segments visualised by coronary angiography were considered assessable ; the intermediate branch was present in four subjects only ( table 1 )  . if only the main segments were considered right coronary erano ipertensione ( 17 ) , fumo di sigaretta ( 6 ) , dislipidemia ( 6 ) , familiarit per ima ( 4 ) e diabete ( 2 )  . 
per coloro invece che presentavano una frequenza borderline e cio intorno o di poco superiore ai 65 bpm si optato per la somministrazione endovena di un - bloccante ( metoprololo tartrato 5 mg ) 15 minuti prima dellesecuzione dellesame . lindagine tc stata effettuata con una apparecchiatura multidetettore a 16 canali ( sensation cardiac , siemens ) , utilizzando i seguenti parametri : collimazione 0 , 75 mm , voltaggio 120 kvp , tempo di rotazione 375 ms , spessore di strato 0 , 75 mlattivit cardiaca stata costantemente monitorata durante lindagine mediante tracciato elettrocardiografico in singola derivazione . per liniezione di mezzo di contrasto ( mdc ) organo - iodato non ionico ( concentrazione 350400 mgi / ml ) si utilizzato un iniettore automatico collegato ad unagocannula da 1820 gauge inserita in una vena antecubitale del braccio . utilizzando la tecnica del bolus tracking con roi nellaorta ascendente sono stati iniettati 100 ml di mdc , seguiti da 40 ml di soluzione fisiologica , ad una velocit di infusione di 4 ml / s . la ricostruzione delle immagini stata effettuata mediante gating cardiaco retrospettivo , individuando la finestra temporale ottimale per ogni ramo coronarico ( solitamente 400 , 350 o 300 ms prima del successivo complesso qrs elettrocardiografico ) [ 2 ]  . 
sono state ricostruite sezioni assiali dello spessore effettivo di 0 , 75 mm con overlapping di 0 , 5 mle immagini coronarografiche sono state ottenute con tecnica 3d volume rendering ( vrt ) e multiplanare ( mpr ) curvilinea . ai fini del confronto tra tcmd e coronarografia , assunta quale gold standard , sono stati considerati 16 segmenti coronarici secondo la classificazione dellamerican table 1 number and percentage of coronary artery segments considered assessable on computed tomography ( ct ) in 31 patients tabella 1 numero e percentuale dei segmenti coronarici giudicati valutabili alla tc in 31 pazienti segments assessable , n ( % ) segmenti variabili , n ( % ) 1 . 
di ogni segmento due operatori , un radiologo e un cardiologo , hanno considerato in maniera indipendente la valutabilit e la qualit iconografica ( eccellente , discreta e scadente ) nonch la presenza di occlusioni o di stenosi classificate in non significative ( 50% ) e significative ( 51%99% ) in base ad un giudizio visuale soggettivo per la tc - md e quantitativo per la coronarografia [ 4 ]  . risultati alla tc - md sono stati giudicati valutabili 383 ( 81 , 7% ) dei 469 segmenti visualizzati alla coronarografia , essendo il ramo intermedio presente solo in 4 soggetti ( tabella 1 )  . 
considerando esclusivamente i segmenti principali e cio arteria coronaria destra ( segmenti 1 , 2 , 3 ) , tronco comune ( segmento 5 ) , arteria discendente anteriore ( segmenti 6 , 7 , 8 ) , arteria circonflessa ( segmenti 11 , 13 ) e , laddove presente , ramo intermedio ( segmento 16 ) , i segmenti considerati valutabili sono stati 277 di 283 ( 97 , 9% ) : in 4 / 31 ( 12 , 9% ) pazienti si avuto un segmento non valutabile , pi frequentemente il 13 ; in 1 paziente ( 3% ) i segmenti non esaminabili sono stati due . 
la tabella 3 mostra i risultati del confronto tc - coronarografia limitatatotal total tc , n positiva negativa totale , n tc , n positive negative totale , n fig . 
1a - c a 40 - year - old man , a heavy smoker with a family history of coronary disease , admitted to the emergency room with precordial chest pain ; sinusal rhythm with 60 bpm at electrocardiogram ( ecg ) , myocardial ischaemia markers negative , no regional wall motion abnormalities at echocardiography . 
computed tomography ( ct ) ( a , b ) shows about 50% tubular stenosis with focal , severe narrowing of the lumen of the anterior descending artery ( ada ) , segment 1 ( arrowheads )  . 
alla coronaro - tc ( a , b ) : stenosi tubulare di circa il 50% , cui segue focale serrato restringimento del lume dellarteria discendente anteriore ( ada ) prossimale , segmento 1 ( punta di freccia )  . 
2a - c a 70 - year - old woman with hypertension admitted to the emergency room with precordial chest pain radiating to the neck ; sinusal rhythm with 63 bpm and minimal st depression at electrocardiogram ( ecg ) , absence of serum cardiac markers , normal ventricular wall motion at echocardiography . 
paziente maschio , et 56 anni , diabete mellito nid , iperteso , con scintigrafia miocardica da sforzo ( eseguita 3 mesi prima ) dubbia per coronaropatia ; pervenuto in ps con dolore toracico retrosternale . 
4a , b a 70 - year - old man with hypertension and hypercholesterolaemia admitted to the emergency room with precordial chest pain ; sinusal rhythm with 58 bpm , absence of ischaemic signs at electrocardiogram ( ecg ) ; absence of serum cardiac markers . 
computed tomography ( ct ) ( a ) shows eccentric calcific plaque of the middle circumflex artery ( segment 13 ) ( arrow )  . the vessel lumen is not well assessable , but a > 50% stenosis ( arrow ) is suggested . 
alla tc ( a ) : placca eccentrica calcifica dellarteria circonflessa , tratto medio , segmento 13 ( freccia ) ; il lume non ben valutabile ma si ipotizza una stenosi > 50% . 
alla coronarografia ( b ) : stenosi della lunghezza di circa 15 mm e del 90% circa nel punto critico ( freccia )  . particular , it reports the number of subjects with at least one occlusion or stenosis > 50% identified by ct with respect to the number of those identified by coronary angiography . 
inoltre , la coronarografia documenta come in 3 di 6 segmenti ( 50% ) vi sia una riopacizzazione da circolo collaterale del tratto distale alla stenosi . la tabella 5 presenta , infine , unanalisi della casistica che considera il singolo paziente piuttosto che i segmenti coronarici ; in particolare , riporta il numero dei soggetti con almeno una occlusione o una stenosi > 50% identificati alla tc rispetto a quanti individuati dalla coronarografia . 
nei pazienti ( 16 / 31 ) , nei quali la qualit dimmagine risultata eccellente per tutti i segmenti , i valori di sensibilit , specificit , valore predittivo positivo e negativo , accuratezza sono pari al 100% . discussione lesame dei pazienti che si presentano in ps per dolore toracico acuto richiede tempo e risorse economiche finalizzati allaccertamento di una sca che risulta , al termine di tutte le indagini , inesistente in una percentuale tuttaltro che trascurabile di casi . 
la valutazione clinica ( intensit , irradiazione , durata ) del dolore toracico , daltra parte , facilmente soggetta ad errori interpretativi e insufficiente per la diagnosi ; ne consegue che lapproccio tradizionale a tali pazienti preveda lelettrocardiogramma e il dosaggio dei markers biochimici . 
lalterazione di questi ultimi unitamente allelevazione elettrocardiografica del tratto st corrobora il sospetto clinico di infarto miocardico , che comunque diagnosticabile anche in assenza di precoci alterazioni elettrocardiografiche qualora vi sia innalzamento di troponina , creatinfosfochinasi e mioglobina . 
quando anche tali markers siano negativi , i pazienti definiti a medio - basso rischio di sca debbono essere avviati a test da stress elettrocardiografici , ecocardiografici o scintigrafici per evidenziare la presenza o lassenza di malattia coronarica significativa [ 5 , 6 ]  . 
5a - c a 58 - year - old woman with hypertension and a previous history of smoking admitted to the emergency room with precordial chest pain and dyspnoea ; absence of ischemic alterations at electrocardiogram ( ecg ) , absence of serum cardiac markers . 
although poor quality of computed tomography ( ct ) image ( a ) should have induced the reader to avoid any judgement , a severe stenosis ( arrow ) of the right coronary artery ( segment 2 ) is suggested . 
si ipotizza comunque lesistenza di una stenosi critica da placca calcifica del segmento 2 , sottovalutando erroneamente lipotesi di una occlusione con riopacizzazione a valle da parte dellemisistema coronarico sinistro , come invece dimostrato dalla coronarografia ( punte di freccia ) ( b , c )  . partment with acute chest pain in order to identify an acs that very often turns out to be nonexistent . 
the clinical assessment ( intensity , radiation , duration ) of chest pain is , on the other hand , often prone to misinterpretation and is inadequate for the diagnosis , with the result that the conventional approach to these patients includes an ecg and serum cardiac markers . abnormal serum cardiac markers associated with st elevation supports the clinical suspicion of myocardial infarction , which can , however , be diagnosed even without early electrocardiographic alterations if the troponin , creatine phosphokinase and myoglobin levels are high . 
where these markers are negative , patients considered at medium to low risk of acs must proceed to electrocardiographic , echocardiographic or nuclear stress testing to determine the presence or absence of significant coronary disease [ 5 , 6 ]  . 
the diagnostic reference standard for the assessment of vascular anatomy and the detection of stenosing lesions is coronary angiography , which , in addition to a diagnostic phase , allows immediate myocardial reperfusion by means of angioplasty . 
the invasiveness and high cost of this examination have , however , promoted research into alternative , noninvasive diagnostic techniques . the technological evolution of spiral ct has made available multislice scanners with 4 , 8 , 16 and , recently , 64 detector rows that offer a temporal and spatial resolution that enable analysis of the coronary arteries with a high level of anatomical detail . 
linvasivit e lelevato costo di tale indagine hanno indirizzato tuttavia gli sforzi della ricerca verso tecniche diagnostiche alternative non invasive . levoluzione tecnologica della tc spirale ha reso disponibili apparecchiature multistrato a 4 , 8 , 16 e , recentemente , 64 file di detettori caratterizzate da risoluzione spaziale e temporale tali da consentire lanalisi delle coronarie con elevato dettaglio anatomico . 
in letteratura , dallanno 2000 ad oggi , sono stati pubblicati diversi studi sullidentificazione di placche coronariche mediante tc - md a 4 o 16 canali [ 711 ]  . 
nella quasi totalit dei lavori sono state prese in considerazione le stenosi che comportano riduzione > 50% o occlusione del lume coronarico ; attualmente , con lutilizzo di scanner a 64 slice , si iniziano a valutare anche stenosi < 50% [ 1214 ]  . 
peraltro , in questa classe di pazienti che presentano angina instabile , due o pi fattori di rischio , incremento della troponina sierica , slivellamento st > 1 mm , aritmie o instabilit emodinamica , le pi recenti linee - guida cardiologiche suggeriscono lesecuzione in prima istanza dellangiografia coronarica e della rivascolarizzazione , se indicata [ 16 , 17 ]  . la presente casistica considera esclusivamente soggetti giunti allosservazione in ps con un dolore toracico acuto 1061 l . 
in this class of patients with unstable angina , two or more risk factors , increased serum troponin , st deviation > 1 mm , arrhythmias or haemodynamic instability , the most recent cardiological guidelines recommend coronary angiography and revascularisation , if indicated , as the first - line approach [ 16 , 17 ]  . our study included only subjects presenting to the emergency department for acute chest pain and at medium to low risk for acs associated with one , two or more risk factors for coronary disease ( age , smoking , dyslipidaemia , arterial hypertension , diabetes mellitus ) but with ischaemia markers and ecg not indicative of q and non - q ami . 
in the 31 patients enrolled , all of the 15 ( or 16 if the intermediate branch was present ) segments were analysed ; subsequently , the main coronary branches only were considered , that is , the right coronary artery ( segments 1 , 2 , 3 ) , left main branch ( segment 5 ) , anterior descending or interventricular artery ( segments 6 , 7 , 8 ) , circumflex artery ( segments 11 and 13 ) and , where present , the intermediate branch ( segment 16 )  . 
 compared with the interesting statistical results of previous reports , the sensitivity of msct ( 71.4% for occlusions and stenoses > 50% ) identified in our study is among the lowest reported in the literature [ 18 , 19 , 2125 ] and higher only than the value reported by hoffmann et al . 
the false negatives are due to underestimation of the degree of stenosis in poor - quality images or to misinterpretation in cases of revascularisation of the branch below the stenosis due to collateral circulation ; in particular , the latter situation led to three stenoses being interpreted as significant rather than as occlusions . 
msct therefore takes on an important role in the diagnostic workup of this class of cardiological patients , as it guides towards coronary angiography more accurately than does exercise stress testing which , though definitely less expensive , has decidedly lower predictive values [ 2628 ]  . 
si sono esclusi i pazienti portatori di bypass aorto - coronarico o pace - maker e i soggetti sottoposti in passato ad interventi di angioplastica , con o senza posizionamento di stents coronarici . 
nei 31 pazienti arruolati , sono stati analizzati tutti i 15 ( o 16 in presenza di ramo intermedio ) segmenti ; successivamente sono stati presi in considerazione solo i rami coronarici principali , ovverosia arteria coronaria destra ( segmenti 1 , 2 , 3 ) , tronco comune ( segmento 5 ) , arteria discendente anteriore o interventricolare ( segmenti 6 , 7 , 8 ) , arteria circonflessa ( segmenti 11 e 13 ) e , qualora presente , il tronco intermedio ( segmento 16 )  . 
il dato in linea con quanto emerge da altri studi effettuati con tc - md a 12 e 16 canali [ 1820 ]  . rispetto a precedenti interessanti risultati statistici , nel presente studio emerge una sensibilit della tc - md ( 71 , 4% per le occlusioni e le stenosi > 50% ) che si posiziona ai limiti inferiori del range dei valori riportati in letteratura [ 18 , 19 , 2125 ] , risultando superiore soltanto a quella ( 63% ) di hoffmann et al . 
essi sono dovuti a sottostima dellentit della stenosi in immagini di qualit scadente o ancora ad errore interpretativo in casi di riabitazione del ramo a valle della stenosi per fenomeni di collateralit : in particolare , questultima evenienza responsabile di tre stenosi interpretate come significative e non , in realt , come occlusioni . 
per quanto concerne invece la specificit per le occlusioni e le stenosi > 50% , il nostro dato ( 99 , 6% ) appare incoraggiante essendo il range delle percentuali fino ad oggi riportate oscillante fra l86% ed il 98% . i valori predittivi negativo ( 97 , 7% ) e positivo ( 93 , 7% ) , superiori a quanto mediamente riportato in letteratura [ 18 , 19 , 2125 ] , implicano che un paziente , pervenuto in ps per dolore toracico con media - bassa probabilit di sca e tc - md negativa per stenosi significativa , abbia solo il 2 , 3% di probabilit di avere in realt una coronaropatia significativa ; allopposto , un soggetto con stenosi giudicata emodinamicamente significativa alla tc ha una probabilit superiore al 93% di conferma coronarografica . 
in questa classe cardiologica di pazienti la tc - md assume quindi un ruolo rilevante nellalgoritmo diagnostico indirizzando verso un approfondimento coronarografico pi correttamente di quanto non possa un test da sforzo , sicuramente meno costoso , ma caratterizzato da valori predittivi decisamente inferiori [ 2628 ]  . 
inoltre se , meno dettagliatamente ma in maniera clinicamente pi congrua , non si considerino i rami coronarici principali bens i singoli pazienti si ottiene una predittivit positiva del 100% . 
of the 467 patients examined by cdus , 159 ( 34% ) showed no signs of renal artery stenosis ( ras ) or nephropathy and were therefore started on medical therapy . 
nel periodo 20002004 sono giunti alla nostra osservazione 467 pazienti ( 205 donne e 262 uomini , range 2096 anni ) , per essere sottoposti ad indagine ecd , in quanto presentavano ipertensione arteriosa resistente alla terapia e / o segni di insufficienza renale . 
dei 467 pazienti esaminati mediante ecd , 159 ( 34% ) non presentavano indici di stenosi delle arterie renali n segni ecografici di nefropatia , ed hanno proseguito un iter terapeutico medico . 
dai risultati ottenuti e alla luce dei dati della letteratura , si riconferma il ruolo fondamentale svolto dallecd nei pazienti con sospetta o accertata patologia nefro - vascolare , fornendo dati importanti sullemodinamica renale di insostituibile utilit per un corretto approccio clinico - terapeutico . parole chiave eco color doppler ipertensione nefrovascolare arterie renali introduction introduzione atherosclerotic renal artery stenosis ( ras ) is associated with two common clinical syndromes , renovascular hypertension and ischaemic nephropathy , which imply a significant worsening of renal function in the presence of stenosis [ 13 ]  . the exact prevalence of ras is unknown , but many data indicate that it is high among elderly , chiefly caucasian , subjects and those with diabetes , diffuse atherosclerosis and rela stenosi aterosclerotica dellarteria renale ( sar ) si associa a due comuni sindromi cliniche : lipertensione nefro - vascolare e la nefropatia ischemica , intendendo per questultima una significativa riduzione della funzione renale in presenza della stenosi [ 13 ]  . lesatta prevalenza della stenosi aterosclerotica dellarteria renale non nota , ma molti dati fanno ritene1115 g.c. 
renal angiography and renal colour - doppler ultrasound ( cdus ) studies performed during coronary angiography or peripheral arteriography have demonstrated that ras is present in 20%30% of more than 10 , 000 investigations [ 1 ]  . 
a large number of patients with serum creatinine higher than 1.7 mg / dl have been found to have ras in prospective and retrospective studies , and ras has been demonstrated in 5%10% of patients with acute renal failure [ 1 ]  . 
this prevalence becomes higher when other clinical signs of atherosclerosis coexist , with rates of 12%24% in patients undergoing coronary angiography , 11% in stroke patients and 40% in patients with peripheral vascular disease [ 3 ]  . 
few studies have assessed atherosclerotic ras in patients with abdominal aorta aneurysm ( aaa ) , another manifestation of atherosclerotic disease . the high prevalence of atherosclerotic ras has raised the need to identify a noninvasive , inexpensive modality with high diagnostic accuracy in order to reduce the use of invasive investigations , such as arteriography , which nonetheless remains the gold standard in the diagnosis of ras [ 2 , 4 , 5 ]  . diagnostic imaging offers several noninvasive methods for selecting patients for angiography : cdus , captopril renal scintigraphy , spiral computed tomography ( ct ) angiography , and magnetic resonance ( mr ) angiography [ 2 , 3 , 511 ]  . cdus of the renal arteries is currently the main screening tool for ras , and many international studies have demonstrated a sensitivity of 83%96% , a specificity of 76%98% , a positive predictive value ( ppv ) of 81%92% and a negative predictive value ( npv ) of 94%98% [ 58 , 1115 ]  . 
the advantages of cdus are that it is inexpensive , reproducible , noninvasive and has good npv when performed in selected populations ; its known disadvantages , on the other hand , are operator dependence , patient preparation and cooperation , scars , obesity , bowel gas and vascular abnormalities , in particular , the presence of anatomical variants of the renal artery [ 2 , 4 , 6 , 1517 ]  . the primary aim of our study was to evaluate the role and usefulness of cdus in analysing overall renal morphology and haemodynamics in patients with hypertension and nephropathy ; the secondary aim was to assess the association between atherosclerotic ras and aaa . materials and methods between 2000 and 2004 , 467 patients ( 205 women and 262 men , age range 2096 years ) with refractory hypertension and / or signs of renal failure ( serum creatinine > 2.5 mg / dl ) were referred to our department for renal cdus . the patients were examined by a single radiologist on a philips ssd 800 and hitachi h21 scanner using a 3.5 - mhz convex - array transducer and colourand power - doppler mode . 
sonograms were assessed for renal morphology , overall renal blood flow and abdominal aorta . 1116 re che essa sia assai frequente nei soggetti anziani , specie di razza caucasica , diabetici , con patologia aterosclerotica polidistrettuale e con insufficienza renale . 
studi angiografici renali e di eco color doppler ( ecd ) renale , eseguiti in corso di coronarografia o di arteriografia periferica , hanno documentato una frequenza di sar nel 20%30% di oltre 10000 indagini [ 1 ]  . 
analisi retrospettive o prospettiche in pazienti con creatininemia superiore a 1 , 7 mg / dl dimostrano presenza di sar in molti casi , cos come in casi di insufficienza renale acuta si ha la sua dimostrazione nel 5%10% dei casi [ 1 ]  . 
poich la stenosi aterosclerotica dellarteria renale pu indurre un danno renale progressivo , in alcune casistiche essa causa di ingresso in dialisi nel 15%30% dei pazienti uremici [ 1 ]  . 
in pazienti anziani non selezionati stata dimostrata mediante ecd una prevalenza del 6 , 6% ; la prevalenza maggiore quando coesistono altre manifestazioni cliniche dellaterosclerosi : nei pazienti sottoposti a coronarografia la prevalenza varia dal 12% al 24% , nei pazienti con ictus dell11% , nei pazienti con malattia vascolare periferica intorno al 40% [ 3 ]  . 
esistono pochi dati che valutino levidenza della sar nei pazienti portatori di aneurisma dellaorta addominale , che rappresenta altra manifestazione di patologia aterosclerotica . lelevata prevalenza di tale patologia ha sollevato la necessit di individuare una metodica non invasiva , a basso costo e con elevata accuratezza diagnostica al fine di limitare il ricorso ad unindagine strumentale invasiva , quale larteriografia che rimane , comunque , la metodica gold standard nella diagnosi della stenosi delle arterie renali [ 2 , 4 , 5 ]  . 
limaging attualmente ha a disposizione alcune metodiche non invasive , come indagini di screening e selezione per la successiva angiografia : lecd , la scintigrafia renale con captopril , langio - tc spirale , langiorm [ 2 , 3 , 511 ]  . 
attualmente lecd delle arterie renali risulta la principale metodica di screening nella diagnosi di stenosi delle arterie renali con numerosi lavori in ambito internazionale che attribuiscono a tale metodica valori di sensibilit pari all83%96% , di specificit 76%98% , valore predittivo positivo 81%92% e valore predittivo negativo 94%98% [ 58 , 1115 ]  . 
in tutti i pazienti , per una pi ampia e corretta valutazione vascolare , stata esaminata laorta addominale , valutandone calibro , morfologia e flusso ( diametro normale < 2 , 5 cm , ectasia 2 , 53 cm , aneurisma > 3 cm )  . risultati dei 467 pazienti esaminati mediante ecd , 159 ( 34% ) non presentavano indici di stenosi delle arterie renali n segni ecografici di nefropatia , ed hanno proseguito un iter terapeutico medico ; in particolare uno di questi pazienti era portatore di protesi aorto - renale pervia . 
i restanti 308 pazienti ( 66% ) mostravano invece segni ecografici di stenosi emodinamicamente significativa o di nefropatia . in particolare , 174 pazienti ( 37 , 2% ) mostravano solo segni di nefropatia , con riduzione del flusso ematico in sede ilare ed ostiale ed un aumento dell ir ; in 123 pazienti ( 26 , 3% ) era presente nefropatia severa con ir 0 , 80 e tra questi un paziente presentava aneurisma dellarteria renale ed un paziente necrosi corticale acuta , confermati successivamente con esame tc ; 51 ( 10 , 9% ) invece presentavano nefropatia moderata con ir di 0 , 75 . in 134 pazienti ( 28 , 7% ) veniva evidenziata una sar emodinamicamente significativa ; 58 dei 134 pazienti ( 12 , 4% ) con sar presentavano segni di nefropatia associata ; in 2 di questi era gia stato posizionato stent , 2 hanno eseguito an1117 fig . 
to obtain a more exhaustive and correct vascular assessment , the calibre , morphology and flow pattern of the abdominal aorta were also evaluated in all patients ( normal diameter < 2.5 cm , ectasia 2.53 cm , aneurysm > 3 cm )  . results of the 467 patients examined with cdus , 159 ( 34% ) had no indices of ras or sonographic signs of nephropathy and were started on medical therapy ; in particular , one of them had a patent aortorenal stent . 
the remaining 308 patients ( 66% ) had sonographic evidence of haemodynamically significant stenosis or nephropathy . in detail , 174 patients ( 37.2% ) showed signs of nephropathy only , with reduced hilar and ostial flow and increased ri . nephropathy was severe in 123 patients ( 26.3% ) , with ri 0.80 ; among them , one had renal artery aneurysm and one had acute cortical necrosis , later confirmed by ct . 
altri 22 pazienti non hanno eseguito angiografia ; in particolare , 1 aveva gi posizionato stent renale , 1 presentava iperplasia mio - intimale , 10 pazienti avevano gi una completa occlusione dellarteria renale , mentre 10 pazienti sono al momento in attesa di eseguire angiografia ed eventuale intervento di rivascolarizzazione . 
in totale , quindi , 33 pazienti , con sar e senza segni di nefropatia ( 7% del totale e 44% dei pazienti con segni ecd di stenosi ) non hanno eseguito esame angiografico . quarantre pazienti ( 9 , 2% del totale e 56% dei positivi per stenosi allecd ) hanno invece eseguito angiografia che ha confermato la diagnosi in 39 dei 43 pazienti . 
di questi , 24 ( 5 , 1% del totale e 55 , 8% dei positivi per stenosi ) hanno posizionato stent con ripristino ottimale della vascolarizzazione renale nel 92% dei casi ( solo in 2 casi erano presenti dopo la procedura interventistica segni clinico - laboratoristici e bioptici di ateroembolismo colesterinico , con quadro di severa compromissione dellemodinamica renale allecd in entrambi i casi )  . diciannove pazienti ( 4% del totale e 44 , 2% dei positivi per stenosi ) invece non hanno posizionato stent : di questo ultimo gruppo 7 avevano gi posizionato stent ( 2 completamente chiusi e 5 restenosi ) , in 3 sussistevano problemi anatomici con biforcazione precoce dellarteria renale , 1 paziente presentava middle aortic syndrome , in 1 caso si era verificata complicanza ( dissezione in corso di procedura ) , in 1 un caso langiografista non riusciva a superare la stenosi , 1 paziente presentava dissezione aortica , in 1 caso si trattava di stenosi lieve - moderata e 2 erano falsi positivi . in particolare , lecd ha permesso di svelare in una giovane paziente una grave situazione anatomica , verosimilmente su base congenita , definita come middle aortic syndrome o coartazione aortica sottodiaframmatica . 
dopo una gestosi , nella paziente era insorta una severa ipertensione arteriosa e , dopo unindagine ecografia risultata negativa per alterazioni morfologiche renali , era stata sottoposta ad indagine ecd che rilevava marcato decremento degli ir arteriosi intraparenchimali ( ir = 0 , 45 ) con polso parvus et tardus in sede ilare e segni di stenosi emodinamicamente significative di entrambe le arterie renali . 
this was associated with signs of nephropathy in 58 patients ( 12.4% ) ; two had already had a stent implanted , two underwent angiography and one had polycystic kidneys , whereas the remaining 56 were excluded from angiography because of signs of severe nephropathy ( longitudinal diameter < 8 cm , ri > 0.80 and poor parenchymal perfusion on cd and pd imaging )  . 
a further 22 patients did not undergo angiography , as one had a renal stent , one had myointimal hyperplasia , ten had complete occlusion of the renal artery , whereas ten were on the waiting list for angiography and possible revascularisation at the time of this writing . 
therefore , a total of 33 patients with ras and without evidence of nephropathy ( 7% of the total and 44% of patients with cd signs of stenosis ) did not undergo angiography . forty - three patients ( 9.2% of the total and 56% of those with ras on cdus ) underwent angiography , which confirmed the diagnosis in 39 . 
of these , 24 ( 5.1% of the total and 55.8% of those with stenosis ) underwent renal stenting , with optimally restored renal perfusion in 92% of cases ( only two had clinical , laboratory and biopsy evidence of cholesterol atheroembolism , with severely impaired renal haemodynamics on cdus , after the interventional procedure )  . nineteen patients ( 4% of the total and 44.2% of those with stenosis ) did not undergo stent implantation : seven of these already had stents ( two of which completely occluded and five with restenosis ) , three patients presented early bi1118 g.c. 
b indagine tc con mdc : assenza di opacizzazione in sede corticale renale bilaterale ( c )  . furcation of the renal artery , one patient had middle aortic syndrome , one developed a complication ( dissection during the procedure ) , in one , the operator could not negotiate the stenosis , one had aortic dissection , one had mild to moderate stenosis and two were false positives . 
following a gestosis , the patient developed severe arterial hypertension and , after a negative sonography for morphological renal alterations , was studied by cdus , which revealed marked reduction of intraparenchymal arterial ri ( ri = 0.45 ) with parvus - tardus pulse in the hilum and signs of haemodynamically significant stenoses of both renal arteries . 
il 56% di questi presentava una marcata riduzione del flusso a livello delle arterie renali e nel 30% erano presenti stenosi emodinamicamente significative delle arterie renali ed in un caso ( 6% ) unarteria renale era occlusa . per quanto riguarda la presenza di aneurisma dellaorta addominale ( aaa ) operato e non , i dati raccolti sono i seguenti : laaa era presente in 19 pazienti dei 333 senza segni di sar ( 5 , 7% ) con netta prevalenza nei pazienti con nefropatia ( 16 casi ) rispetto ai pazienti senza nefropatia ( 3 casi ) mentre laaa era presente in 15 dei 134 pazienti con segni 1119 g.c. 
this translates into a marked clinical benefit for the patient as well as considerable economic savings , given that out of the 467 patients studied by cdus , 88% did not undergo angiography as against 22% who did undergo angiography . 
if we exclude patients who underwent angiography before cdus ( cdus follow - up ) and those with a previously implanted stent , the remaining 65% underwent stent revascularisation , with excellent outcome in all patients except two , one of whom develop cholesterol atheroembolism after the procedure . in some cases , cdus revealed severe impairment of renal circulation in patients with poor renal compensation who showed only minor laboratory alterations ( serum creatinine 1.62.5 mg / dl )  . 
in addition to being valuable for analysing renal morphology and volume and assessing blood flow on cdus and pdus , evaluation of the ri proved to be reliable for determining renal function 1120 di sar ( 11 , 2% ) ; la presenza di aaa operato stata di 5 pazienti tra i 333 senza segni di sar ( 1 , 5% ) ed in particolare pi frequente tra i pazienti nefropatici ( 4 casi ) che nei non nefropatici ( 1 caso ) mentre la presenza di aaa operato nei pazienti con segni di sar stata di 10 pazienti sui 134 ( 7 , 46% )  . discussione dai risultati ottenuti si riconferma lutilit dellecd nellesaminare i pazienti con ipertensione e nefropatia ; lo studio dellemodinamica renale con ecd si rilevata in alcuni casi indagine insostituibile per un corretto approccio clinico - terapeutico [ 2 , 5 , 7 , 9 , 15 ]  . lecd ha evitato langiografia nei pazienti negativi e in quelli con stenosi occlusiva dellarteria renale e con segni di grave nefropatia , nei quali lintervento avrebbe potuto aggravare il deficit renale ( tossicit del mdc , ateroembolismo colesterinico , ecc . ) con indubbio vantaggio clinico per il paziente e risparmio economico . 
infatti del totale dei 467 pazienti esaminati allecd l88% non stato sottoposto ad esame angiografico e solo il 22% ha eseguito angiografia . escludendo i pazienti che hanno eseguito lindagine angiografica prima dellecd ( monitoraggio ecd ) e i pazienti con pregresso posizionamento di stent , i restanti 65% sono stati sottoposti ad intervento di rivascolarizzazione con stent con ottimi risultati in tutti i pazienti ( ad eccezione di 2 casi , uno dei quali presentava ateroembolismo colesterinico dopo la procedura )  . lindagine ecd ha rilevato in diversi casi una compromissione del circolo renale di diversa entit in pazienti con labile compenso renale che presentavano modeste alterazioni laboratoristiche ( creatininemia 1 , 62 , 5 mg / dl ) ; in questi casi il corretto approccio terapeutico ha sicuramente ritardato lesaurimento della funzionalit renale ed il ricorso al trattamento dialitico con il miglioramento della qualit della vita  . 
si tratta di una sindrome non comune in letteratura , descritta in giovane et ( 628 anni ) come variet rara di coartazione aortica ( 0 , 2%2% delle coartazioni aortiche ) , associata ad aneurisma dellaorta addominale e a stenosi della arteria renale . 
rarely reported in the literature , the syndrome has been described in young subjects ( 628 years old ) as a rare variant of aortic coarctation ( 0.2%2% of aortic coarctations ) and to be associated with aaa and ras . 
multiple causes have been recognised , including congenital and secondary to takayasus syndrome , von recklinghausens neurofibromatosis , coeliac disease and autoimmune disorders ( dermatitis herpetiformis , insulindependent diabetes ) , and clinical onset is usually renovascular hypertension and claudication [ 2224 ]  . in 16 patients with a clinical and laboratory diagnosis of cholesterol atheroembolism , the results of cdus provided a good indication of the severity of their clinical condition : in 12 patients , the condition arose after interventional procedures ( five after angiography , four after coronary angiography , one after coronary artery stenting , one after subclavian artery stenting and one after left renal artery stenting ) and in four patients following administration of coumadall patients had signs of severely impaired parenchymal flow due to cholesterol emboli clogging the small arteries and causing inflammatory reactions , intimal proliferation , vessel fibrosis and luminal obliteration . 
despite being nonspecific findings on cdus , these alterations translate into increased resistive index in the intrarenal arteries and reduced parenchymal and hilar flow in the renal arteries . in nine cases , cdus diagnosed renal artery occlusion in patients with modest chronic renal failure whose renal function had rapidly declined ; thus , it avoided the need for further investigations and enabled selection of patients for medical therapy . 
the study of the renal artery should not be limited to the ostial region ( where the majority of stenoses are present ) but should include an overall assessment of renal arterial circulation to detect possible alterations and evaluate the feasibility of an appropriate revascularisation procedure . 
patients with severe impairment of renal haemodynamics who were unlikely to benefit from revascularisation were therefore excluded from angiography [ 17 , 25 ]  . our experience highlights the association between aaa and ras , an important factor for vascular surgeons and angiographers considering endovascular treatment for aortic aneurysms and for selecting the most appropriate strategy when the two diseases coexist [ 2630 ]  . this study reconfirms the crucial role of cdus in monitoring patients who have undergone stent revascularisation procedures [ 25 ]  . 
in addition , it raises the problem of contrast medium toxicity in patients with poor renal function . cdus consistently revealed haemodynamically significant stenosis of the stent site with parvus - tardus pulse below the stenosis , in most cases due to the presence of fibrointimal celiaco e malattie autoimmuni ( dermatite erpetiforme , diabete insulino dipendente ) ; spesso ad esordio clinico con ipertensione nefrovascolare e claudicatio [ 2224 ]  . in 16 pazienti con diagnosi clinico - laboratoristica di ateroembolismo colesterinico , lecd ha fornito risultati che ben rispecchiano la gravit del quadro clinico : in 12 pazienti il quadro insorto dopo manovre interventistiche ( 5 dopo angiografia , 4 dopo coronarografia , 1 dopo posizionamento di stent in arteria carotide , 1 in arteria succlavia e 1 in arteria renale sinistra ) e in 4 pazienti dopo somministrazione di coumadin tutti i pazienti sono stati rilevati segni di grave compromissione del circolo parenchimale dovuto agli emboli di colesterolo il cui impianto nelle piccole arterie seguito da una reazione infiammatoria , proliferazione dellintima , fibrosi dei vasi colpiti e obliterazione del lume vasale . 
tali alterazioni , pur essendo aspecifiche allecd , si traducono con lincremento dellindice di resistenza arterioso intrarenale e con riduzione del flusso parenchimale e ilare nelle arterie renali . in 9 casi lecd ha diagnosticato locclusione di unarteria renale , in pazienti con modesta insufficienza renale cronica che avevano presentato rapido aggravamento della funzionalit renale evitando in questi ulteriori indagini e sottoponendoli alla sola terapia medica . 
lo studio dellarteria renale non deve esaurirsi alla sede ostiale ( ove presente la maggior parte delle stenosi ) ma deve valutare globalmente il circolo arterioso renale per evidenziare eventuali alterazioni e per valutare la possibilit di proporre al paziente un corretto intervento di rivascolarizzazione . 
sono pertanto stati esclusi dallangiografia i pazienti che presentavano severa compromissione dellemodinamica renale , che probabilmente non avrebbero tratto beneficio dal trattamento di rivascolarizzazione [ 17 , 25 ]  . la nostra esperienza mette in risalto lassociazione fra la patologia aneurismatica dellaorta addominale e la stenosi dellarteria renale , dato sicuramente molto importante per il chirurgo vascolare e per langiografista , alla luce del trattamento endovascolare degli aneurismi aortici e sulla scelta strategica pi opportuna in presenza contemporanea delle due patologie [ 2630 ]  . in questo studio viene riaffermato linsostituibile ruolo svolto dallecd nel monitoraggio dei pazienti che hanno subito interventi di rivascolarizzazione con stent [ 25 ]  . 
in questi pazienti lindagine angio - tc ha fornito , nella nostra esperienza , informazioni sul corretto posizionamento dello stent ma risultato difficile lo studio della perviet dello stent stesso , senza tener conto della tossicit del mdc in questi pazienti dalla gi labile funzionalit renale . lesame ecd ha rilevato stenosi emodinamicamente significative in corrispondenza dello stent con presenza di polso parvus et tardus nel tratto a valle la stenosi in tutti i pazienti , nella maggior parte dovuto alla presenza di iperplasia fibrointimale o a placche aterosclerotiche site prossimalmente o distalmente rispetto allo stent . 
cdus identified patients with restenosis ( seven cases ) , all of which were confirmed by angiography and subsequently treated by repeat revascularisation ( placement with another co - axial stent or with the use of a cutting balloon )  . conclusioni di rivascolarizzazione ( posizionando un altro stent coassiale o con lutilizzo del cutting ballon )  . conclusions on the basis of our results and data from previous reports , we confirm that cdus plays a fundamental role in patients with suspected or known renovascular disease , as it provides important information on renal haemodynamics and guides the clinician towards the most appropriate clinical and therapeutic approach [ 2 , 57 , 1416 ]  . our results indicate that cdus , with appropriate selection criteria , is able to discriminate between patients who should or should not undergo angiography , leading to considerable economic savings and benefits for the patient , who can thus be directed to the most appropriate treatment plan [ 16 ]  . 
in addition , our findings point to a close association between the presence of aaa and ras and confirm the need for close collaboration between the vascular surgeon , the interventional radiologist and the nephrologist in planning the most appropriate treatment approach in these patients with associated diseases [ 2630 ]  . cdus proved its value in confirming the diagnosis of cholesterol embolism suspected on the basis of clinical and laboratory findings . 
these patients carry a poor prognosis , with 1 - year mortality rates between 64% and 87% , and monitoring by imaging may certainly help the clinician deal with this complex disease given that angiography is strongly contraindicated both because it is an interventional manoeuvre and because it requires heparin administration [ 3133 , 34 ]  . in the patient with middle aortic syndrome , cdus revealed the alteration in renal haemodynamics , thus justifying the use of a more panoramic modality , such as ct angiography , which shed light on the patients complex anatomical situation [ 2224 ]  . another important contribution of cdus was to substantiate the clinical and laboratory suspicion of acute renal failure in a septic patient with cortical necrosis . 
use of contrast medium , justified by the need to shed light on what was clearly a very critical clinical situation , enabled prompt treatment ( haemodialysis and plasmapheresis ) , with partial recovery of renal function [ 35 ]  . cdus confirmed its value in monitoring nephropathic patients and those who have undergone renal artery revascularisation procedures [ 17 , 25 ]  . 
our experience also highlights the importance of cdus in monitoring patients in whom renal artery occlusion or stenosis has been diagnosed at angiography : in these patients , clinical and laboratory monitoring should be combined with follow - up by cdus , which is able to effectively reveal disease progression and provide the clinician with the data required for a more appropriate treatment strategy . 1122 dai risultati ottenuti e alla luce dei dati della letteratura , si riconferma il ruolo fondamentale svolto dallecd nei pazienti con sospetta o accertata patologia reno - vascolare , fornendo dati importanti sullemodinamica renale di insostituibile utilit per un corretto approccio clinico - terapeutico [ 2 , 57 , 1416 ]  . dai nostri risultati si evince come ecd , alla luce dei criteri adottati , possa essere metodica in grado di discriminare i pazienti che devono o non devono essere sottoposti ad esame agiografico , con risparmio dei costi e beneficio per il paziente che potr quindi essere indirizzato al pi opportuno iter terapeutico [ 16 ]  . 
i nostri dati mettono inoltre in risalto unelevata associazione fra la presenza dellaaa e la sar : questo vuole riconfermare lutilit di una stretta collaborazione fra il chirurgo vascolare , il radiologo interventista e il nefrologo nel programmare la strategia terapeutica pi opportuna in questi pazienti con patologia associata [ 2630 ]  . lecd si dimostrata metodica utile nel confermare la diagnosi di ateroembolismo colesterinico , gi prospettata in base ai dati clinico - laboratoristici . 
questi sono pazienti a prognosi infausta con mortalit ad 1 anno variabile dal 64% all87% in cui il monitoraggio strumentale pu essere certamente di ausilio al clinico nellaffrontare una cos complessa patologia , dal momento che in tali pazienti fortemente controindicata langiografia , sia perch manovra interventistica sia per la somministrazione di eparina [ 3133 , 34 ]  . nella paziente con la middle aortic syndrome lecd ha svelato lalterazione emodinamica a livello renale , giustificando il ricorso a metodiche pi panoramiche come langiotc che ha rilevato la complessa situazione anatomica da cui era affetta [ 2224 ]  . occorre senzaltro rimarcare limportanza dellecd nel confermare lipotesi clinico - laboratoristica di insufficienza renale acuta in corso di sepsi nella paziente affetta da necrosi corticale ; lutilizzo del mdc , giustificato dalla necessit di chiarire una situazione che allesordio era molto critica , ha consentito la tempestiva terapia ( emodialisi e plasmaferesi ) con parziale recupero della funzione renale [ 35 ]  . la metodica ecd si dunque riconfermata di indubbio valore nel monitoraggio dei pazienti nefropatici e di quelli sottoposti ad intervento di rivascolarizzazione allarteria renale [ 17 , 25 ]  . 
souza de oliveira ir , widman a , molinar lj et al ( 2000 ) color doppler ultrasound : a new index improves the diagnosis of renal artery stenosis . ultrasound med biol 26 : 4147 12 . 
frauchiger b , zierler r , bergelin ro et al ( 1996 ) prognostic significance of intrarenal resistance indices in patients with renal artery interventions : a preliminary duplex sonographic study . cardiovasc surg 4 : 324330 18 . 
mehta m , darling rc 3rd , roddy sp et al ( 2004 ) outcome of concomitant renal artery reconstructions in patients with aortic aneurysm and occlusive disease . vascular 12 : 381386 29 . 
tali caratteri radiografici non sono correlati ad alcun tipo istologico particolare . parole chiave lesioni non palpabili linfonodi intra - mammari carcinoma della mammella introduction introduzione intramammary lymph nodes are the most common cause of nonpathological masses seen on conventional mammography , being detected in about 30% of breasts , mostly in the upper - outer quadrants [ 1 ]  . 
the typical mammographic features of intramammary lymph nodes ( size smaller than 15 mm , round or oval shape , regular margins , low density , association with a vascular branch and , frequently , a radiolucent centre ) have been clearly established [ 17 ] , and their detection does not warrant further diagnostic investigation i linfonodi intra - mammari costituiscono la causa pi frequente di formazione espansiva con significato non patologico riscontrata allesame mammografico convenzionale : sono infatti presenti in circa il 30% delle mammelle , prevalentemente nei quadranti supero - esterni [ 1 ]  . 
i caratteri mammografici tipici dei linfonodi intra - mammari ( dimensioni inferiori a 15 mm , morfologia rotondeggiante od ovalare , contorni regolari , bassa densit , associazione con una diramazione vascolare e frequente area centrale di maggiore radio - trasparenza ) sono chiaramente codificati da lungo tempo in letteratura [ 17 ] ed il 1078 e . 
however , in rare cases , breast cancers may exhibit mammographic features compatible with intramammary lymph nodes [ 1 , 2 , 9 , 11 ]  . the aim of this study was to verify the existence of mammographic criteria justifying a suspicion of atypical intramammary lymph node , assess whether certain histological types of breast cancer are more likely to display the radiographic features of intramammary lymph nodes , and consider the most appropriate diagnostic strategy in women with node - like mammographic findings . materials and methods we retrospectively reviewed the previous mammograms of women who received a diagnosis of breast cancer between january 1997 and december 2004 . 
the mammograms had been performed 6 months to 3 years before the diagnosis and depicted findings morphologically similar to intramammary lymph nodes at the site where the cancer was subsequently detected . 
the imaging equipment consisted of a dedicated conventional radiology unit ( mammomat 3000 , siemens , erlangen , germany ) combined with a high - spatialresolution detector , gadolinium screen ( kodak min r 2000 ) and single - coated film ( kodak m35 series x - omat processor )  . 
examinations performed with different equipment and techniques were excluded from the study . during the examination that aroused the suspicion of a neoplastic lesion , all lesions were studied by fine - needle cytology ( 2023 gauge ) under sonographic guidance ( seven cases ) or stereotactic guidance ( in one case in which the lesion was poorly visualised on ultrasound )  . 
all lesions subsequently underwent surgical excision and histological examination . loro riscontro non richiede approfondimenti diagnostici , che si rendono necessari solo in caso di incremento volumetrico in un controllo mammografico successivo [ 813 ]  . 
sebbene raramente , tumori della mammella in fase iniziale possono presentare caratteri mammografici sovrapponibili a quelli tipici dei linfonodi intra - mammari [ 1 , 2 , 9 , 11 ]  . scopo di questo lavoro ricercare se esistano criteri di semeiotica mammografica che consentano di porre il sospetto di linfonodo intra - mammario atipico , valutare se alcuni istotipi tumorali si manifestino preferenzialmente con caratteri radiografici simili a quelli dei linfonodi intra - mammari ed esaminare quale sia la strategia diagnostica pi opportuna quando si riscontrino reperti di aspetto compatibile con quello dei linfonodi intra - mammari . materiali e metodi sono stati retrospettivamente valutati i radiogrammi espletati in un periodo compreso tra i sei mesi e tre anni prima della diagnosi di tumore della mammella , posta tra gennaio 1997 e dicembre 2004 nei quali , nella sede in cui sarebbe stata in seguito identificata la neoplasia , era presente un reperto con i caratteri morfologici di un linfonodo intra - mammario . 
tutte le pazienti considerate hanno eseguito un esame mammografico standard , con almeno due proiezioni ( cranio - caudale e medio - laterale obliqua ) per mammella ; lindagine stata espletata con apparecchiatura radiologica convenzionale dedicata ( mammomat 3000 , siemens , erlangen , germania ) associata a detettore ad alta risoluzione spaziale , con schermo di rinforzo in gadolinio ( kodak min r 2000 ) e pellicola monoemulsionata ( kodak m35 series x - omat processor )  . 
le indagini espletate con modalit differenti da quella citata sono state escluse dallo studio . tutte le lesioni , nel corso dellindagine in cui ne stata sospettata la natura neoplastica , sono state sottoposte ad esame citologico con ago sottile ( calibro 2023 g ) , espletato sotto guida ecografica ( 7 casi ) o stereotassica ( nel singolo caso in cui la lesione non risultava chiaramente riconoscibile allesame ecografico )  . 
it is difficult to identify any lesion at all at the site of interest ( arrow and arrowhead ) on the mediolateral oblique mammogram ( a )  . only the craniocaudal view ( b ) shows an 8 - mm , faint , round opacity in the upper - outer quadrant that can be evaluated as an intramammary lymph node ( arrows )  . 
sul radiogramma in proiezione medio - laterale obliqua ( a ) risulta difficilmente identificabile , nel punto di interesse ( freccia e testa di freccia ) , una qualsiasi lesione . 
solo la proiezione cranio - caudale ( b ) dimostra nel versante supero - esterno tenue opacit rotondeggiante di 8 mm valutabile come linfonodo intra - mammario ( freccia )  . 
in the craniocaudal view ( b ) , an oval opacity with regular margins can be seen ( arrow ) projecting along a vascular branch , with a radiolucent central area ( 8 mm )  . 
in fase pre - diagnostica la proiezione medio - laterale obliqua ( a ) non consente di identificare lesioni sospette nellarea di interesse ( freccia e testa di freccia )  . 
in proiezione cranio - caudale ( b ) si identifica tenue opacit ovalare a contorni regolari ( freccia ) proiettatesi su diramazione vascolare , con nucleo radio - trasparente ( 8 mm )  . 
mediolateral oblique mammogram shows an 8 - mm , faint , round opacity in the upper quadrant ( arrow ) , with multilobular margins and radiolucent centre ( a ) interpreted as an intramammary lymph node . 
radiogramma in proiezione medio - laterale obliqua che dimostra nel versante superiore tenue opacit rotondeggiante di 8 mm ( freccia ) a contorni pluriciclici e nucleo radiotrasparente ( a ) interpretata come linfonodo intra - mammario . 
a minute ( 4 mm ) , round opacity with a radiolucent central area projecting along a small vascular branch can be seen in the upper - outer quadrant on both views ( arrows in a , b )  . 
minuta ( 4 mm ) opacit rotondeggiante con nucleo radiotrasparente , proiettantesi su piccola diramazione vascolare , riconoscibile nel versante supero - esterno in entrambe le proiezioni ( frecce in a , b )  . 
il controllo effettuato a distanza di 24 mesi ( c , d ) dimostra lieve incremento volumetrico ( 6 mm ) con densit lievemente aumentata . at baseline mammography , all masses showed round or oval shape and low density , with well - defined margins in seven cases ( two of which lobulated ) , and one case showed slightly indistinct margins . 
le dimensioni delle formazioni erano comprese fra 4 e 8 mm ( tabella 1 )  . lindagine in cui stata riconosciuta la reale natura neoplastica delle neoformazioni stata espletata da 6 a 36 mesi dopo la prima . 
a small ( 5 mm ) , faint , round opacity with radiolucent central area projecting along a vascular branch is seen in the upper - outer quadrant on the mediolateral oblique view ( arrow in a ) , which is even more evident on the craniocaudal view ( arrow in b )  . 
piccola ( 5 mm ) e tenue opacit rotondeggiante con nucleo radiotrasparente , proiettantesi sul decorso di diramazione vascolare nel versante supero - esterno , apprezzabile in proiezione medio - laterale obliqua ( freccia in a ) e meglio in proiezione cranio - caudale ( freccia in b )  . 
in the prediagnostic phase , the minute ( 6 mm ) , faint opacity visible in the upper - outer quadrants on both views ( arrows in a , b ) could easily be interpreted as an intramammary lymph node because of its site , density , radiolucent centre and proximity to vascular structures . 
in fase pre - diagnostica , la minuta ( 6 mm ) e tenue opacit apprezzabile in entrambe le proiezioni ( frecce in a , b ) nel versante supero - esterno facilmente interpretabile come linfonodo intramammario , in virt della sede , delle densit , del nucleo radiotrasparente e delle prossimit con le strutture vascolari . 
dopo 24 mesi ( c , d ) la lesione presenta contorni sfumati ; sensibilmente aumentata di volume ( 20 mm ) e di densit , questultima disomogenea . discussion discussione the radiographic features traditionally ascribed to intramammary lymph nodes [ 17 ] still hold good , as they are based on pathology findings and experience : the finding of small round or oval masses with regular margins and low density ( especially if located along a vascular branch and relatively radiolucent in their central portion ) does not justify a suspicion of neoplastic disease . 
a number of benign conditions can cause lymph nodal eni caratteri radiografici tradizionalmente attribuiti ai linfonodi intra - mammari [ 17 ] , in quanto fondati su dati anatomopatologici e condizionati dalla esperienza , rimangono validi a tuttoggi : il riscontro di formazioni espansive rotondeggianti od ovalari di piccole dimensioni , a margini regolari e dotate di bassa densit ( specie se situate lungo una diramazione vascolare e relativamente radio - trasparenti nella porzione centrale ) non autorizza a porre il sospetto di patologia neoplastica . 
the prediagnostic mediolateral oblique view shows , in the area in question ( arrow in a ) , an almost imperceptible , very small ( 4 mm ) and faint opacity , marked with an arrow on the craniocaudal view ( b )  . 
in fase pre - diagnostica , nella proiezione medio - laterale obliqua pressoch impercettibile nella zona di interesse ( freccia in a ) la minuta ( 4 mm ) e tenue opacit contrassegnata con freccia nella proiezione cranio - caudale ( b )  . 
a distanza di 36 mesi ( c , d ) la lesione risulta sensibilmente aumentata di volume ( 10 mm ) e densit , presentando contorni sfumati . largement and increased radiographic density , for example , inflammation of the breast skin ( at times related to implants ) or systemic inflammation ( rheumatoid arthritis )  . 
lymph nodal enlargement and increased density may also result from lymphoproliferative disease or from metastasis from cancers located in other parts of the breast , or rarely , elsewhere in the body ( melanomas , pulmonary , gastric and ovarian cancers ) [ 9 ]  . 
 inoltre causare nel tempo incremento nelle dimensioni e nella densit radiografica dei veri linfonodi intra - mammari , come avviene in caso di flogosi cutanee proprie della ghiandola mammaria ( anche sostenute dalla presenza di protesi ) o su base sistemica ( quali lartrite reumatoide ) ; analogo reperto pu essere causato da malattie infettive fra cui la tubercolosi . 
infine , possono ingrandirsi ed aumentare in densit i linfonodi intra - mammari sede di localizzazione di malattia linfoproliferativa o di metastasi , a partire da tumori primitivi posti in altre porzioni della mammella o , raramente , altrove ( melanomi ; tumori polmonari , gastrici ed ovarici ) [ 9 ]  . to our knowledge , the possibility that early primary secondo i dati a nostra disposizione , la possibilit che 1083 e . 
the retrospective review of our small case series did not reveal any correlation between histological type of cancer and node - like radiographic patterns , nor did it indicate the existence of new semiological criteria . 
it did , however , highlight a need for careful assessment of the known semiological criteria . owing to their small size , initial cancers with misleadingly similar features to intramammary lymph nodes may exhibit suspicious features in one radiographic view only . 
in addition , it should be noted that slight blurring of tumori primitivi della mammella esordiscano con quadri mammografici simili a quelli dei linfonodi intra - mammari non stata trattata in letteratura , sebbene sia noto che i carcinomi mucinosi possono presentare margini netti [ 7 ]  . la valutazione retrospettiva di questa casistica per quanto numericamente limitata non ha evidenziato correlazioni fra specifici istotipi tumorali e caratteri radiografici simil - linfonodali . 
non sono inoltre emersi criteri semeiologici nuovi ma la necessit di dedicare estrema attenzione a quelli gi noti . in conseguenza delle loro esigue dimensioni , lesioni tumorali in fase precoce e con caratteri ingannevolmente simili a quelli dei linfonodi intra - mammari possono mostrare segni sospetti in una sola proiezione radiografica . 
gists were located in the stomach in 18 / 27 patients , in the small bowel in seven , in the oesophagus in one and in the rectum in one . 
in 15 / 27 cases , the lesions exhibited extramural growth , and in 17 / 27 cases , they were homogeneous after contrast medium injection . the borders were regular in 17 cases . 
in 1983 , in - depth studies recognised gists as discrete entities , which allowed them to be differentiated from smooth con il termine di tumori stromali gastrointestinali ( gist , dallinglese gastro - intestinal stromal tumor ) si comprende attualmente un eterogeneo gruppo di neoplasie mesenchimali del tratto gastroenterico , che sono state a lungo oggetto di controversie riguardanti la loro nomenclatura , istogenesi , diagnosi e prognosi . 
fino al 1983 , infatti , erano inclusi in questa categoria di tumori anche i leiomiomi , leiomioblastomi , leiomiosarcomi , schwannomi e neurofibromi . nel 1983 studi pi approfonditi hanno conferito a questi tu1103 c . 
histological and immunohistochemical characteristics of gists are well defined and include the presence of spindle cells ( less commonly epithelioid cells and rarely both ) and positivity for the cd117 membrane protein [ 113 ]  . despite being the most common type of gastrointestinal mesenchymal tumour [ 1 , 2 , 5 , 9 , 10 ] , gists are rare and account for only 0.1%3% of all gastrointestinal neoplasms [ 8 , 1416 ]  . 
gists generally affect individuals over the age of 50 years and are rare in subjects younger than 40 years [ 2 , 5 , 10 , 12 ] , with a slight , though debated , predilection for males [ 2 , 4 , 5 , 17 , 18 ]  . 
gists arise in the stomach in 60%70% of cases , in the small bowel in 20%25% , in the rectum in 5% and very rarely in the oesophagus , colon and appendix [ 25 , 8 , 9 , 12 , 16 , 1925 ]  . 
regardless of the location and in the absence of haemorrhagic complications related to mucosal ulcerations , the clinical symptoms of gist are nonspecific and tend to develop late , when the tumour has reached a large size . diagnostic imaging and especially computed tomography ( ct ) are instrumental in the detection and staging of gist , as has been reported in the literature [ 1 , 5 , 8 , 9 , 12 , 13 , 19 , 23 , 24 , 26 , 27 ]  . 
the aim of this study was to evaluate the potential of multislice ct ( msct ) in the identification and characterisation of gist . materials and methods we retrospectively evaluated the ct images of 27 patients ( 15 men and 12 women , aged 3774 years ) studied between april 2001 and may 2004 and found to be affected by gist . the definitive diagnosis was provided by histological examination of the surgical specimen . 
given the retrospective design of the study , approval by the ethics committee was not required . in 15 cases , ct was carried out to investigate submucosal disease suspected at endoscopy and involving the oesophagus in one case , the stomach in 13 cases , and the rectum in one case . 
in genere interessano soggetti che hanno oltre 50 anni di et e sono di raro riscontro in pazienti di et inferiore ai 40 anni [ 2 , 5 , 10 , 12 ] , con una discussa lieve predominanza per il sesso maschile [ 2 , 4 , 5 , 17 , 18 ]  . 
indipendentemente dalla loro localizzazione ed in assenza di complicanze emorragiche legate ad ulcerazioni della mucosa , la sintomatologia clinica dei gist aspecifica e tardiva e compare soltanto quando i tumori raggiungono considerevoli dimensioni . la diagnostica per immagini e soprattutto la tomografia computerizzata ( tc ) hanno un ruolo fondamentale nel riconoscimento e nella stadiazione dei gist come riportato in letteratura [ 1 , 5 , 8 , 9 , 12 , 13 , 19 , 23 , 24 , 26 , 27 ]  . 
scopo del presente lavoro valutare le possibilit della tc multistrato ( tc - ms ) nella identificazione e caratterizzazione di tali tumori . materiali e metodi sono state valutate retrospettivamente le immagini tc di 27 pazienti ( 15 uomini e 12 donne ) , di et compresa tra 37 e 74 anni , studiati tra aprile 2001 e maggio 2004 e risultati affetti de gist . 
trattandosi di uno studio retrospettivo non stato necessario richiedere il consenso alla commissione etica per il suo svolgimento . lesame tc era stato eseguito in 15 casi per lo studio di una patologia sottomucosa sospettata con endoscopia in 1 caso a livello esofageo , in 13 casi a livello dello stomaco , in 1 caso a livello del retto . 
all patients received contrast material for the study of the bowel loops : two sachets of negative contrast material ( duogas , bracco , milan , italy ) for the study of the oesophagus ( one case ) 400600 cc of water or duogas for the study of the stomach ( 13 cases ) 400600 ml diluted methylglucamine diatrizoate ( gastrografin ) in the remaining 13 cases the data acquired were retrospectively transferred to a workstation ( hp kayak xu800 , hewlett packard , palo alto , ca , usa ) running dedicated reconstruction software ( vitrea 2.6 , vital images , minneapolis , mn , usa )  . 
multiplanar ( coronal , sagittal and oblique ) and three - dimensional ( 3d ) reconstructions were obtained with multiplanar reformatting ( mpr ) and volume rendering ( vr ) techniques . 
two cases of disagreement about the possible origin of large masses were resolved by consensus . the images were assessed for : morphological changes to the intestinal wall caused by the presence of a recognisable , expansile mass in the wall portion of the gastrointestinal tract involved by the tumour ( oesophagus , stomach , duodenum , jejunum , ileum , colon and rectum ) tumour size origin and growth pattern relative to the affected organ ( defined as intraor extraluminal , depending on whether more or less than half of the tumour lay inside or outside the lumen ) attenuation , defined as homogeneous or heterogeneous according to enhancement characteristics margin morphology of both mucosal and extramural components ( regular if smooth or lobular ; irregular if finely jagged ) presence of mucosal ulcerations at the lesion site relationship with adjacent structures or organs ; infiltration was hypothesised in the absence of a clear cleavage plane presence of distant metastases evidence of lymph nodes ; any node detected on the scans was considered pathological , regardless of diameter presence of ancillary findings , such as intestinal occlusion or ascites additional information provided by the mpr and vr reconstructions aiding identification and characterisation of the tumour and definition of its growth pattern and relationship with adjacent structures c . 
il mdc uroangiografico non - ionico ( iopromide , ultravist 370 , schering , berlino , germania ) stato iniettato nella vena cubitale attraverso un ago da 1618 gauge , utilizzando un iniettore automatico ( mk - iv , medrad , pittsburgh , pennsylvania , usa ) con i seguenti parametri : volume 1 , 5 ml / kg di peso corporeo ( fino ad un massimo di 130 ml ) , velocit di iniezione 3 , 5 ml / s . 
in tutti i casi stato somministrato mezzo di contrasto per lo studio delle anse intestinali : due bustine di mezzo di contrasto negativo ( duogas , bracco , milano , italia ) per lo studio dellesofago ( 1 caso ) ; 400600 ml di acqua o duogas per lo studio dello stomaco ( 13 casi ) ; 400600 ml di soluzione diluita di diatrizoato e metilglucamina ( gastrografin ) nei restanti 13 casi . i dati acquisiti sono stati trasferiti retrospettivamente ad una workstation ( hp kayak xu800 , hewlett packard , palo alto , california , usa ) dotata di un software di ricostruzione dedicato ( vitrea 2 , 6 , vital images , minneapolis , minnesota , usa )  . 
i programmi applicativi utilizzati sono stati il multiplanar reformatting ( mpr ) e il volume rendering ( vr ) che hanno consentito di ottenere ricostruzioni multiplanari ( coronali , sagittali e oblique ) e tridimensionali . 
la durata complessiva del postprocessing stata di 15 minuti . tutte le immagini assiali e le ricostruzioni sono state valutate in cieco da due radiologi esperti , non coinvolti direttamente nellesecuzione dellesame tc . 
in due casi divergenze collegate alla possibile origine di voluminose neoformazioni sono state risolte in consenso . nella valutazione delle immagini sono stati considerati : alterazioni morfologiche della parete intestinale determinate dalla presenza di un riconoscibile processo espansivo nel suo contesto ; tratto dellapparato gastroenterico ( esofago , stomaco , duodeno , digiuno , ileo , colon e retto ) interessato dalla patologia ; dimensioni del tumore ; origine e sviluppo del tumore rispetto alla parete del viscere interessato ( considerato intrao extraluminale a seconda che pi o meno di met lesione si sviluppasse allinterno o allesterno del lume del viscere ) ; densitometria del tumore , differenziata in omogenea o disomogenea a seconda delle caratteristiche di impregnazione ; morfologia dei margini sia sul versante mucoso che extraparietale ( regolari , se lisci o lobulati ; irregolari , se finemente frastagliati ) ; presenza di ulcerazioni mucose nella sede della lesione ; 1105 c . 
in tutti i casi esaminati la lesione neoplastica era unica . le dimensioni del tumore variavano da un diametro minimo di 1 , 5 cm ad un massimo di 21 cm ( dimensione media di 7 , 4 cm )  . 
in particolare in 10 dei 18 gist gastrici ( 55% ) lindagine tc ha mostrato una crescita di tipo endofitico mentre nei restanti 8 / 18 casi ( 45% ) lo sviluppo era prevalentemente ex1107 fig . 
presenza di profonda ulcerazione mucosa ( freccia vuota )  . results ct findings in the 27 patients with gist are reported in table 1 . the most frequently affected site was the stomach ( 18 / 27 , 67% ) , and in particular , the cardias in one case , the fundus in one case , the body in 13 cases and the antrum in three cases . in seven cases ( 26% ) , the disease involved the small bowel , and specifically , the jejunum in four cases , the duodenum in one case and the ileum in two cases . 
in detail , gastric lesions ranged from 1.5 cm to 15 cm ( mean 5.3 cm ) , intestinal lesions from 4 cm to 21 cm ( mean 12 cm ) , the oesophageal lesion was 12 cm and the rectal lesion was about 10 cm . in 23 out of 27 cases , an extramucosal origin was suggested by the presence of raised mucosa at the lesion site c . 
tutte le lesioni dopo iniezione del mezzo di contrasto hanno mostrato un persistente incremento di densit , che si manifestato in maniera omogenea in 17 / 27 casi e disomogenea in 10 casi . 
in nessun caso sono state evidenziate calcificazioni intralesionali . i margini sono risultati regolari in 18 / 27 casi ( 67% ) ed irregolari nei restanti 9 casi ( 33% )  . 
i margini delle lesioni gastriche si sono dimostrati regolari sia sul versante mucoso che extraparietale in 14 / 18 casi , in particolare in 6 / 8 gist a sviluppo extraparietale e in 8 / 10 a sviluppo endoluminale . 
in nessun caso stata evidenziata uninfiltrazione delle strutture vascolari o degli organi contigui alla neoplasia . lesioni metastatiche , in tutti i casi localizzate a livello epatico , erano gi evidenti al momento della diagnosi in 5 / 27 pazienti ( 18% )  . 
in particular , 10 / 18 gastric gists ( 55% ) showed an endophytic growth pattern whereas the remaining 8 / 18 cases ( 45% ) had a prevalently extragastric growth pattern . 
the intestinal gists exhibited extramural growth pattern in 5 / 7 cases ( 71% ) , a constant feature in lesions larger than 11 cthe remaining two lesions had intraluminal growth . 
a in correspondence with the posterior wall of the gastric body , there is a small , high - attenuation mass showing regular borders and intraluminal growth ( arrowheads )  . 
b , c nel lobo sinistro del fegato presente una metastasi che appare tenuemente iperdensa nelle scansioni precoci ( b ) ed ipodensa nelle scansioni tardive ( c ) ( frecce vuote )  . the lesions could always be detected on the precontrast scans , and they showed homogeneous appearance in 23 cases , and there was a heterogeneous appearance in four cases of large tumours . 
in no case was infiltration of vascular structures or adjacent organs observed . metastatic lesions , involving the liver in all cases , were detected at presentation in 5 / 27 patients ( 18% )  . 
the primary tumours ranged in size from 1.5 cm to 11 cm . lymph node enlargement was detected in only one gist of the gastric fundus , and the lesions were located in the perigastric node stations . 
il tumore primitivo aveva diametro compreso tra 1 , 5 e 11 cm . la presenza di linfonodi aumentati di volume stata riscontrata soltanto in 1 gist del fondo gastrico e le lesioni erano localizzate nelle stazioni perigastriche . 
per differenziare i gist da altri tumori mesenchimali sono comunemente utilizzati altri markers immunochimici come ls100 tipico degli schwannomi , e lactina e desmina caratteristiche dei veri tumori a cellule muscolari lisce , i leiomiomi ed i leiomiosarcomi [ 1 ]  . lesatta prevalenza dei gist sconosciuta e secondo miettinem e lasota [ 2 ] di 1020 casi per milione di persone , senza alcuna associazione geografica , etnica , razziale o occupazionale [ 1 , 2 , 14 ]  . tali tumori possono originare dalla parete di qualunque segmento del tratto gastroenterico , dallesofago the mpr and vr reconstructions were of no help in diagnosing the tumour , which was always appreciable on the axial scans , or in characterising it . 
other markers that are commonly used to differentiate gists from other mesenchymal tumours include s100 for schwannomas and actin and desmin for true smooth muscle tumours , leiomyomas and leiomyosarcomas [ 1 ]  . the exact prevalence of gist is unknown , but according to miettinem and lasota [ 2 ] , it is 1020 cases per million people , without any geographic , ethnic , racial or occupational association [ 1 , 2 , 14 ]  . gists can arise from the wall of any portion of the gastrointestinal tract , from the oesophagus to the anus [ 5 , 28 ] , and represent the most common type of mesenchymal tumour , if we exclude the oesophagus , where 25% are gists and 75% are leiomyomas [ 5 , 28 ]  . 
the gist locations found in our study ( stomach 67% ; small intestine 26% ; oesophagus 4% ; rectum 4% ) reflect the data reported in the literature [ 15 , 9 , 12 , 13 ]  . the size of these tumours varies widely , from several millimetres , in which case they are generally an incidental finding , to 30 cm or more [ 1 , 5 ]  . 
the gastric tumours in our series ranged in size from 1.5 cm to 15 cm ( mean 5 cm ) , the oesophageal gist was 12 cm , the intestinal gists were 421 cm ( mean 12 cm ) and the rectal gist was 10 cm . gists often originate in muscularis propria ( outer wall layers ) ; those arising in the muscularis mucosae ( deeper wall layers ) are rare and more frequently involve the colon [ 5 ]  . according to some authors , tumour origin from the muscularis propria or muscularis mucosae will influence its exophytic growth pattern , which was seen in 15 / 27 of our cases , or intraluminal growth pattern , which was seen in the remaining 12 cases . clinical presentation depends on lesion site and size . small tumours are generally asymptomatic and discovered incidentally during surgery , endoscopy or imaging studies . symptomatic gists tend to be large and , depending on location , can give rise to dysphagia , nausea , vomiting , abdominal pain and a palpable mass [ 1 , 5 , 28 ]  . 
whatever the site , erosion of the mucosa overlying the lesion may lead to gastrointestinal bleeding . biologically , gist are considered potential malignancies with different degrees of risk ( very low , low , intermediate , high ) on the basis of size and mitotic rate [ 3 , 2931 ] ; thus , all gists require surgical treatment . diagnostic imaging is instrumental in the detection of gists and relies on conventional radiology , ultrasound ( us ) , ct , magnetic resonance ( mr ) and positron emission c . 
in rapporto allorigine dagli strati pi esterni della parete ( muscolaris propria ) o dagli strati pi interni ( muscolaris mucosae ) , secondo alcuni autori si determinerebbe uno sviluppo esofitico riscontrato nella nostra casistica in 15 / 27 casi o endoluminale riscontrato nei 12 restanti casi . la presentazione clinica di questi tumori variabile a seconda della sede e dimensione della patologia . 
indipendentemente dalla loro localizzazione lerosione della mucosa sovrastante il tumore pu generare emorragie gastrointestinada un punto di vista biologico i gist sono considerati tumori potenzialmente maligni con differente grado di rischio ( molto basso , basso , intermedio , alto ) valutato in base alle dimensioni e tasso mitotico [ 3 , 2931 ] , pertanto tutti necessitano di una terapia chirurgica . nel riconoscimento dei gist la diagnostica per immagini ha un ruolo fondamentale e si basa su : radiologia tradizionale , ultrasonografia ( us ) , tomografia computerizzata ( tc ) , risonanza magnetica ( rm ) , tomografia ad emissione di positroni ( pet )  . 
il ruolo della tc nello studio dei gist stato ampiamente sottolineato in letteratura [ 1 , 5 , 8 , 9 , 12 , 13 , 19 , 23 , 24 , 26 , 27 ] e la metodica interviene nel riconoscimento del tumore e nel valutare la sua estensione o eventuale disseminazione metastatica . 
la morfologia tc dei gist nella nostra esperienza risultata priva di specificit ed i tumori apparivano come processi espansivi a partenza extramucosa , con modesto enhancement dopo iniezione di mezzo di contrasto . 
le lesioni di piccole dimensioni avevano aspetto omogeneo , quelle voluminose pi spesso disomogeneo in rapporto ad emorragie e necrosi intratumorali . nellambito delle diagnosi differenziali , in presenza di un sospetto gist riconosciuto alla tc devono essere consi1111 c . 
the role of ct in the study of gist has been widely emphasised in the literature [ 1 , 5 , 8 , 9 , 12 , 13 , 19 , 23 , 24 , 26 , 27 ] and consists of recognising the tumour and assessing its extension and possible metastatic spread . 
in our experience , the ct appearance of gist was found to lack specificity , with the tumours manifesting as expansile masses with extramucosal origin and moderate enhancement after contrast medium injection . 
small lesions appeared homogeneous whereas larger lesions were more often heterogeneous due to intralesional haemorrhage and necrosis . the differential diagnosis of a suspected gist detected on ct should include both benign lesions , such as lipomas , cystic duplications , leiomyomas , schwannomas or neurofibromas , and malignant lesions , such as leiomyosarcomas , lymphomas or adenocarcinomas [ 32 ]  . 
lymphomas cause varying degrees of wall thickening , which may be diffuse , often multiple , with a hypodense appearance of the submucosal infiltrates , and often associated with lymphadenopathy . 
carcinomas may exhibit broad - based intraluminal vegetations or varying degrees of concentric or eccentric wall thickening , always associated with mucosal alterations and frequently with lymphadenopathy [ 32 , 33 ]  . in a study by dematteo et al . 
only 18% of gists in our series ( three gastric and two ileal ) showed secondary liver lesions at presentation , and no correlation was found between tumour size and metastasis , which was also seen in a gist measuring 1.5 cthis finding supports the view that metastatic spread is influenced by mitotic rate rather than tumour size . in agreement with previous reports [ 1 , 5 , 12 ] finding limited evidence of nodal spread associated with sarcomas , only one out of 27 patients in our series had metastatic lymphadenopathy . use of multislice ct with mpr and vr reconstructions proved particularly useful in the study of large gists , as it enabled better definition of tumour origin and relationships with adjacent organs . 
conversely , the technique appears to offer no additional contribution to disease characterisation compared with conventional modalities . derate lesioni benigne come lipomi , duplicazioni cistiche , leiomiomi , schwannomi o neurofibromi e lesioni maligne come leiomiosarcomi , linfomi o adenocarcinomi [ 32 ]  . 
una diagnosi differenziale tra gist ed altri tumori sottomucosi come leiomiomi , schwannomi , neurofibromi e leiomiosarcomi impossibile in base alla morfologia tc ed a tale fine indispensabile lesame istologico . 
la diagnosi differenziale con altre forme maligne come linfomi ed adenocarcinomi in genere possibile . i linfomi determinano ispessimenti parietali di vario grado , diffusi , spesso multipli , con aspetto in genere ipodenso degli infiltrati sottomucosi , associati spesso a linfoadenopatie . 
nei carcinomi possono riscontrarsi vegetazioni endoluminali a larga base dimpianto o ispessimenti parietali concentrici o eccentrici di vario grado , sempre con alterazione della mucosa e frequenti linfoadenopatie [ 32 , 33 ]  . in uno studio di dematteo et al . 
le lesioni epatiche apparivano ipo - isodense rispetto al parenchima nelle scansioni di base e mostravano dopo iniezione di mdc un enhancement disomogeneo per la presenza di aree centrali necroticocolliquative . 
solo il 18% dei gist nella nostra casisitica ( tre tumori a sede gastrica e due a sede ileale ) presentavano al momento della diagnosi lesioni secondarie epatiche e non stata trovata alcuna correlazione tra dimensioni del tumore e presenza di metastasi , che sono state infatti riconosciute anche in un gist di 1 , 5 c tale dato depone per un rischio di disseminazione metastatica in rapporto al tasso mitotico piuttosto che alle dimensioni della lesione . in accordo con la letteratura [ 1 , 5 , 12 ] che sottolinea la scarsa evidenza di diffusione linfonodale associata a sarcomi , nei nostri risultati in un solo caso su 27 pazienti erano presenti linfoadenopatie metastatiche . limpiego della tc multistrato , per la possibilit di fornire ricostruzioni mpr ed in vr , risultato particolarmente utile nello studio dei gist voluminosi per meglio definire lorigine del tumore ed i rapporti con gli organi contigui . 
gallo dipartimento integrato dei servizi diagnostici e per immagini , struttura complessa di radiologia ii , azienda policlinico , via del pozzo 71 , i - 41100 modena , italy correspondence to : m.g. 
with regard to lesion site , virtual endoscopy proved to be as informative as real endoscopy . the virtual endoscope was able to cross severe stenoses with a residual lumen of 3 mfollow - up studies were performed in 15 patients treated with laser and cryotherapy . 
the technique , with the integration of mpr images , can be proposed as a preliminary study to obtain accurate characterisation of stenoses , to shorten the time required for the subsequent endoscopic procedure and to plan the most appropriate treatment . key words tracheobronchial stenosis virtual bronchoscopy fiberoptic bronchoscopy riassunto obiettivo . 
lendoscopio virtuale stato in grado di superare stenosi serrate con lume residuo fino a 3 mm . il follow - up stato eseguito in 15 pazienti sottoposti a laser e crio - terapia . 
essa , integrata dalle immagini mpr , pu essere proposta come indagine preliminare per una accurata caratterizzazione della patologia stenotica , per abbreviare i tempi di esecuzione della successiva procedura endoscopica e per la pianificazione del trattamento terapeutico pi appropriato . parole chiave stenosi tracheobronchiale broncoscopia virtuale fibrobroncoscopia 1064 m.g. 
in these patients , a reproducible and objective noninvasive technique could prove useful , not only for a correct diagnosis , but also for guiding towards the most appropriate treatment and for evaluating response to treatment during follow - up [ 2 , 3 ]  . the standard diagnostic procedures used in stenotic lesions of the central airway include computed tomography ( ct ) and flexible bronchoscopy [ 24 ]  . 
although these techniques are highly precise and reliable , they both suffer some technical limitations that could lead to inaccurate characterisation of the airway disease [ 3 ]  . multidetector spiral ct allows the acquisition of thin - slice axial sections of entire body volumes during a single breathhold [ 57 ] , thus eliminating respiratory artefacts [ 8 ] even in poorly cooperating patients with severe airway disease [ 9 ]  . the possibility of obtaining multiplanar and three - dimensional ( 3d ) images has enabled the demonstration of focal airway stenoses and the localisation of lesions in endobronchial , peribronchial or submucosal sites [ 10 , 11 ]  . furthermore , 3d techniques have led to virtual bronchoscopy , a reconstruction technique that exploits the natural contrast between endoluminal air and surrounding tissue [ 9 , 12 ] , allowing navigation through the tracheobronchial tree [ 10 ] with the same endoluminal perspective as real endoscopy [ 13 , 14 ]  . 
virtual bronchoscopy is not operator dependent [ 14 ] , and reports have demonstrated a 63%100% sensitivity and a 61%99% specificity for the identification of central stenoses [ 1 , 3 , 9 , 12 ]  . 
these include the inability to perform biopsies for histological assessment [ 1 , 3 , 9 , 15 ] and to provide a chromatic distinction between normal mucosa and pathological tissue [ 1 , 8 ] and to determine its texture [ 10 , 16 ]  . conventional endoscopy therefore remains the gold standard for the identification and characterisation of airway lesions of any size [ 10 ]  . endoscopy , on the other hand , may fail to provide sufficient information owing to the lesion completely obstructing a bronchus and preventing the study of branches beyond , because of the presence of severe bleeding following a biopsy attempt , or because some concomitant condition ( advanced age , tracheomalacia , etc . ) advises against its use where not absolutely needed [ 10 ]  . 
in addition , it is an uncomfortable , poorly tolerated procedure that requires local sedation [ 8 , 9 ] and is associated with a 0.8% morbidity [ 3 , 10 , 17 ] and occasionally with well - known complications ( oxygen desaturation and tachycardia ) caused by the procedure itself or by the anaesthetic [ 8 , 9 ]  . 
nonetheless , the indisputable diagnostic and therapeutic value of the technique justifies its relative invasiveness and the risk of complications [ 9 , 18 , 19 ]  . le patologie ostruenti le vie respiratorie centrali , che siano di natura benigna o maligna , sono unimportante causa di mortalit e morbilit [ 1 , 2 ]  . le principali cause di compromissione locale delle vie aeree includono : neoplasie intraluminali , compressioni estrinseche , tracheomalacia , tessuto granulomatoso aberrante e fibrosi [ 1 ]  . spesso , soggetti con lesioni di questo tipo , coinvolgenti il tratto respiratorio prossimale , esordiscono con un quadro di ostruzione bronchiale parziale o completa [ 2 ]  . 
in tali pazienti un metodo non invasivo , riproducibile ed oggettivo potrebbe rivelarsi utile non solo per una corretta diagnosi , ma anche per indirizzare verso unappropriata terapia e ad una successiva valutazione della risposta al trattamento [ 2 , 3 ]  . le procedure diagnostiche standard a cui vengono sottoposti i pazienti con patologie del torace , determinanti stenosi delle vie aeree centrali , includono la tc e lendoscopia con broncoscopio flessibile [ 24 ]  . 
sebbene queste metodiche siano altamente precise ed attendibili , entrambe presentano dei limiti tecnici che potrebbero essere causa di una inaccurata caratterizzazione della patologia aerea [ 3 ]  . la tc spirale multidetettore ha permesso lacquisizione di sezioni assiali a spessore sottile di interi volumi corporei , nel tempo di una singola breve apnea [ 57 ] , eliminando gli artefatti da respiro [ 8 ] anche in pazienti con gravi patologie aeree e , conseguentemente , con ridotta capacit collaborativa [ 9 ]  . la possibilit di ottenere immagini multiplanari e tridimensionali ha consentito di dimostrare stenosi focali delle vie aeree e di localizzare la lesione in sede endobronchiale , peribronchiale o sottomucosa [ 10 , 11 ]  . le tecniche 3d , inoltre , hanno permesso un tipo di ricostruzione , la broncoscopia virtuale , che , sfruttando il naturale contrasto tra il contenuto aereo endoluminale e il tessuto circostante [ 9 , 12 ] , consente di navigare allinterno dellalbero tracheo - bronchiale [ 10 ] , riproducendo la stessa prospettiva endoluminale del reale esame endoscopico [ 13 , 14 ]  . 
la broncoscopia virtuale non un esame operatore - dipendente [ 14 ] e numerosi lavori in letteratura ne hanno dimostrato una sensibilit nella individuazione di stenosi centrali del 63%100% e una specificit del 61%99% [ 1 , 3 , 9 , 12 ] ; ci nonostante , lindagine virtuale attualmente non pu sostituire quella convenzionale , in quanto non scevra da limiti . 
limite intrinseco alla metodica lincapacit di eseguire prelievi bioptici per lanalisi isto - citologica del tessuto [ 1 , 3 , 9 , 15 ] e di operare una distinzione cromatica tra la mucosa normale e il tessuto patologico [ 1 , 8 ] n tanto meno di valutare la sua consistenza [ 10 , 16 ]  . attualmente lendoscopia reale rimane lesame goldstandard nellindividuazione e tipizzazione delle lesioni delle vie aeree anche di piccole dimensioni [ 10 ]  . a volte la broncoscopia non d informazioni sufficienti , in quanto la lesione ostruisce completamente un bronco e di conseguenza non possono essere valutati i rami a valle 1065 m.g. 
furthermore , we believe that it may be suggested as a valuable tool both for planning treatment and for evaluating response to treatment during the follow - up of patients with cancer and those with severe stenosis , whose clinical conditions are severely compromised . materials and methods between december 2004 and october 2005 , 25 patients ( 16 men and nine women , age range 6083 years ) underwent virtual endoscopy at our radiology department . 
si aggiunga che lendoscopia convenzionale una procedura scomoda e poco tollerata dai pazienti , motivo per cui richiesta la sedazione locale [ 8 , 9 ] ; inoltre associata ad una morbilit dello 0 , 8% [ 3 , 10 , 17 ] e , in rari casi , a ben note complicanze ( desaturazione di ossigeno e tachicardia ) , intrinseche alla procedura stessa , nonch allanestesia [ 8 , 9 ]  . 
lindiscutibile valore diagnostico e terapeutico della procedura , tuttavia , ne giustifica la relativa invasivit ed il rischio di complicanze [ 9 , 18 , 19 ]  . in considerazione a ci , quindi , possiamo ritenere le due tecniche non antagoniste tra loro , bens indagini complementari [ 9 , 20 ] , che , integrando le loro informazioni , sono in grado di fornire unaccurata caratterizzazione pre - operatoria delle patologie tracheo - bronchiali , che si potr poi tradurre in un aumento dellefficacia terapeutica delle stesse [ 11 ]  . lo scopo del nostro studio non quello di proporre la broncoscopia virtuale come alternativa a quella reale , ma come indagine preliminare nellabbreviare i tempi di esecuzione della successiva procedura endoscopica . 
crediamo , inoltre , possa essere proposta sia come valido strumento per pianificare il trattamento terapeutico pi appropriato nel post - operatorio come follow - up per la valutazione della risposta al trattamento in pazienti oncologici e nei pazienti con gravi patologie stenosanti , le cui condizioni cliniche siano molto compromesse . materiali e metodi nel periodo compreso tra dicembre 2004 e ottobre 2005 sono stati sottoposti a broncoscopia virtuale , presso la struttura complessa di radiologia ii dellazienda ospedalierouniversitaria di modena , 25 pazienti ( 16 uomini e 9 donne , di et compresa tra i 60 e gli 83 anni ) , con sospetta patologia steno - ostruttiva tracheo - bronchiale , dopo preliminare valutazione radiologica tradizionale e clinica . 
diffusione extrabronchiale della lesione stenosante 1 ( stenosi < 25% ) ; 2 ( 25% < stenosi > 50% ) ; 3 ( 50% < stenosi > 75% ) ; 4 ( stenosi > 75% )  . about 500 hu for optimal representation of the airmucosa interface , a bronchoscopic study of the tracheobronchial tree was performed . the endoscopic images obtained were mounted as a sequence to simulate endoscopic navigation . 
this confirmed the presence of a lesion , the degree of obstruction and the patency and accessibility of the airway beyond the obstruction , as shown in table 1 . image processing and interpretation took 15 min on average , providing the endoscopist with the data needed to guide conventional bronchoscopy . 
this reduced bronchoscopy times by almost 10 min , with increased patient comfort . images obtained with virtual bronchoscopy before and after treatment were then compared with the findings of fiberoptic bronchoscopy . 
 conventional bronchoscopy conventional bronchoscopy was performed by an experienced pneumologist with a videobronchoscope ( epk - 1000 ; pentax , tokyo , japan ) and with the patient under local anaesthesia . before conventional endoscopy , the virtual bronchoscopy images were made available to the bronchoscopist to provide guidance on the examination path and the precise position of the region of interest . the conventional bronchoscopy images of the stenoses were then compared with those obtained with virtual bronchoscopy . 1068 diametro delle vie aeree normali adiacenti , in : grado 1 : restringimento del lume fino al 25% ; grado 2 : dal 25% al 50% ; grado 3 : fino al 75% ; grado 4 : superiore al 75% . in seguito , utilizzando il programma di endoscopia virtuale , con algoritmo di ricostruzione volume rendering e valore soglia di rappresentazione dellinterfaccia aria - mucosa intorno a 500 uh , stato condotto uno studio broncoscopico attraverso lalbero tracheobronchiale . le immagini endoscopiche cos realizzate sono state montate in sequenza , realizzando in tal modo la simulazione della visione endoscopica in movimento . 
 results concordance of the virtual bronchoscopy and fiberoptic bronchoscopy was evaluated with regard to identification , localisation and characterisation of the tracheobronchial stenoses before and after treatment . results before treatment the quality of the virtual endoscopy images was excellent for all patients , who were able to maintain the breath - hold for the entire duration of scan ( 68 s ) , even in cases of severe respiratory failure . among the 25 patients with proximal airway obstruction studied by chest ct with image processing followed by conventional bronchoscopy , four had benign lesions and 21 had malignant lesions ( table 2 )  . 
 a patient with a finding of aortic arch aneurysm had been referred for virtual bronchoscopy to confirm a suspicion of mediastinal mass , possibly causing extrinsic compression of table 2 tracheobronchial obstructive lesions lesion patients , n malignant lesion : squamocellular carcinoma small cell cancer adenocarcinoma mesothelioma benign lesion : sarcoidosis tracheomalacia endobronchial lipoma right aortic arch aneurysm patologia patologie maligne : squamocellulare microcitoma adenocarcinoma mesotelioma patologie benigne : sarcoidosi tracheomalacia lipoma endobronchiale aneurisma dellarco aortico destro - posto tabella 2 patologie ostruttive tracheo - bronchiali pazienti , n risultati pre - trattamento la qualit delle immagini endoscopiche virtuali stata eccellente in tutti i pazienti , che sono stati in grado di mantenere lapnea per lintera durata della scansione ( 68 s ) , anche nei casi di grave insufficienza respiratoria . dei 25 pazienti con patologia ostruente le vie aeree prossimali , sottoposti a tc del torace con elaborazione delle immagini e successiva broncoscopia reale , 4 hanno presentato lesioni di natura benigna e 21 di natura maligna ( tabella 2 )  . 
 nel caso del riscontro dellaneurisma dellarco aortico , il paziente ci stato inviato per lesecuzione dellindagine virtuale nel sospetto di massa mediastinica quale causa di compressione estrinseca delle vie aeree prossimali , in un quadro di insufficienza respiratoria e radiografia del torace apparentemente negativa . 
in questo caso , il paziente aveva gi eseguito fibrobroncoscopia che aveva rivelato un bomb in corrispondenza della parete posteriore della trachea , con riduzione del lume di circa il 50% . 
si trattava , infatti , di un aneurisma dellaorta toracica con arco destro - posto che , anzich localizzarsi anteriormente rispetto alla trachea e passare a ponte al di sopra del bronco principale sinistro , si dirigeva posteriormente alla trachea e allesofago , con normale decorso nel restante tratto discendente . per quanto riguarda la sede delle stenosi , la broncoscopia virtuale ha fornito informazioni sovrapponibili a quelle della broncoscopia reale . 
in particolare sono state riscontrate 4 stenosi della trachea , 5 del bronco principale destro , 4 del bronco intermedio , 12 nel bronco principale sinistro , 6 del bronco lobare superiore sinistro , 4 del bronco lobare inferiore sinistro . 
sono state riscontrate : 1 stenosi di grado i ; 5 di grado ii ; 2 di grado iii ; 18 di grado iv . tali dati sono risultati sovrapponibili alla valutazione semiquantitativa descritta in broncoscopia reale . 
in un unico caso lesame fibrobroncoscopico non ha confermato lesistenza di una stenosi di grado i , documentata allindagine virtuale , al iii medio della trachea , attribuibile alla presenza di secrezioni viscose , con una concordanza pari al 96% . lendoscopio virtuale stato in grado di passare oltre stenosi di grado iv , con lume residuo fino a 3 mm , riuscendo ad esplorare zone inaccessibili al broncoscopio flessibile . con lausilio delle immagini assiali e delle mpr , abbiamo documentato lestensione intraed extra - bronchiale , la perviet o meno delle vie aeree a valle ed il coinvolgimento delle strutture mediastiniche da parte della lesione stenosante . 
ct with mpr and virtual bronchoscopy demonstrated the presence of the stenosis and its vascular origthe stenosis was in fact caused by a thoracic aorta aneurysm with a right - sided aortic arch that , instead of lying anterior to the trachea and passing over the left main bronchus , ran posterior to the trachea and oesophagus , with an otherwise normal course in the remaining descending branch . as concerns the site of stenosis , virtual bronchoscopy provided identical data to those yielded by conventional bronchoscopy . 
in detail , there were four stenoses of the trachea , five of the right main bronchus , four of the intermediate bronchus , 12 of the left main bronchus , six of the left upper lobar bronchus and four of the left lower lobar bronchus . stenoses involving the left upper lobar bronchus and the left lower lobar bronchus were seen in cases with obstruction of the main bronchi . 
degree of stenosis was as follows : one grade - 1 stenosis five grade - 2 stenoses two grade - 3 stenoses eighteen grade - 4 stenoses these data were very similar to those obtained from the semiquantitative evaluation at conventional bronchoscopy . only in one case did fiberoptic bronchoscopy fail to confirm a grade - 1 stenosis of the middle third of the trachea that the virtual study had detected , possibly as a result of the presence of viscous secretions ; agreement was 96% . the virtual endoscope was able to pass through grade - 4 stenoses , with a residual lumen of 3 mm , thus succeeding in table 3 follow - up of benign lesions sarcoidosis tracheomalacia endobronchial lipoma therapy drug conservative surgical resection stenosis degree pretherapy posttherapy * the patient underwent follow - up , without treatment tabella 3 follow - up lesioni benigne terapia grado di stenosi pretrattamento posttrattamento farmacologica sarcoidosi tracheomalacia conservativa lipoma endobrochiale resenzione chirurgica * la paziente non stata sottoposta a terapia , ma solo a follow - up strumentale 1070 risultati post - trattamento il follow - up con broncoscopia virtuale dopo trattamento stato eseguito su 15 dei 25 pazienti ; 9 sono deceduti alcune settimane dallinizio della terapia . tra le lesioni stenosanti di natura benigna ( tabella 3 ) il caso dellaneurisma aortico non stato compreso nel programma di controllo a distanza . 
esso consente : visualizzazione diretta del lume e della mucosa dellalbero tracheo - bronchiale con la possibilit di individuare eventuali alterazioni quali tumori o lesioni granulomatose ; biopsia di lesioni endobronchiali evidenti o sospette ; spazzolamento , lavaggio o biopsia di parti del polmone per la coltura e lesame citologico [ 19 ]  . la broncoscopia in grado di visionare e valutare cambiamenti della mucosa relativi a qualsiasi patologia : infiammazioni acute e croniche , lesioni endoluminali , compressioni ab - estrinseco , etc . il broncoscopio flessibile attualmente in grado di identificare e tipizzare le lesioni delle vie aeree centrali con una percentuale di falsi positivi molto bassa ( 0 , 8% ) e unaccurata diagnosi istologica nel 94% dei casi [ 10 ]  . ci sono casi per in cui la broncoscopia non in grado di fornire informazioni sufficienti ; ci si verifica quando la massa neoplastica ostruisce completamente un bronco . 
sn 4 intermedio indagine tc 0 main bronchus 4 upper lobar bronchus 1 left main bronchus 4 upper lobar bronchus 4 left main bronchus 2 intermediate bronchus bronchus 4 lower lobar bronchus post - trattamento 0 br . 
the data obtained were provided to the endoscopist before conventional bronchoscopy , resulting in reduced examination times ( approximately 10 min )  . results after treatment follow - up virtual bronchoscopy was performed on 15 of the 25 patients ; nine had died a few weeks after beginning treatment . 
the patient affected by tracheomalacia , with stenoa partire dagli anni 90 levoluzione tecnologica ha consentito di produrre apparecchiature tc che permettono lo studio di un intero volume anatomico con una singola acquisizione in apnea respiratoria [ 22 ] , grazie alla possibilit di associare la rotazione continua del sistema tubo - detettori alla consensuale traslazione longitudinale del tavolo porta paziente [ 23 , 24 ]  . la tc multistrato rappresenta unevoluzione della tc spirale , con importanti innovazioni per quel che riguarda la composizione dei detettori ; soprattutto lutilizzo di multiple file di detettori , invece che di ununica fila , ha aumentato di molto non solo laccuratezza diagnostica , ma anche la qualit delle immagini e delle ricostruzioni tridimensionali , gra1071 m.g. 
3a - g pretreatment evaluation of left hilar lesion ( a ) causing a grade - 4 stenosis of the ipsilateral main bronchus , at a distance of 40 mm from the carina , and upper - lobe subatelectasis ( be )  . 
3a - g valutazione pre - trattamento di lesione ilare sinistra ( a ) che provoca stenosi di grado 4 del bronco principale omolaterale ad una distanza di 40 mm dalla carena e subatelettasia del lobo superiore ( b - e )  . 
the technique in fact , allows : direct visualisation of the lumen and mucosa of the tracheobronchial tree , with the possibility of detecting alterations such as tumours or granulomatous lesions biopsy of evident or suspicious endobronchial lesions brushing , lavage or biopsy of parts of the lung for cytologic analysis [ 19 ] bronchoscopy is able to detect and assess mucosal changes resulting from any disease : acute and chronic inflammations , endoluminal lesions , extrinsic compression , etc . the flexible bronchoscope can currently identify and characterise central airway lesions with very few false positive results ( 0.8% ) and provide an accurate histological diagnosis in 94% of cases [ 10 ]  . however , in some cases , bronchoscopy is unable to provide sufficient information , such as when a bronchus is completely obstructed by a neoplastic mass . 
there are very few absolute contraindications to bronchoscopy : unstable cardiovascular status , severe cardiac arrhythmia , very severe refractory hypoxaemia , congestive heart failure and bronchial spasm [ 18 , 21 ]  . la tc spirale multistrato ha inoltre aperto interessanti prospettive nellinterpretazione di peculiari aspetti della patologia bronco - polmonare , con lausilio dei software di ricostruzione e lo sviluppo della tecnica endoscopica virtuale [ 24 ]  . 
sono inoltre in grado di fornire preziose informazioni sui rapporti che la lesione contrae con le strutture mediastiniche adiacenti [ 11 ]  . ct imaging broncoscopia virtuale beginning in the 1990s , technological progress has led to the production of ct scanners permitting the study of an entire anatomical volume during a single breath - hold [ 22 ] , thanks to the association of the constant rotation of the tube - detector system with the simultaneous longitudinal translation of the patient table [ 23 , 24 ]  . la broncoscopia virtuale con tomografia computerizzata spirale rappresenta una tecnica complementare sul piano diagnostico a quella tradizionale , con interessanti risultati nella individuazione delle lesioni endobronchiali [ 24 , 26 ]  . 
4a - e after chemotherapy , multiplanar reconstructions ( mpr ) demonstrate patency of the left main bronchus , which appears to have reduced calibre ( grade - 3 stenosis ) and to be stretched anteriorly ( ac )  . 
in particular , the use of multiple rows of detectors instead of a single row has significantly improved not only diagnostic accuracy but also the quality of images and 3d reconstructions . 
these scanners can , in fact , acquire up to 64 slices per rotation , with a tube rotation time equal to or less than 0.5 s , which results in faster scans compared with single - slice spiral ct and the possibility of studying large volumes with thin slices [ 24 ]  . the advantages are many and include improved temporal resolution , resulting from reduced acquisition time for each rotation and fewer voluntary and involuntary motion artefacts ( peristalsis , breathing , etc . ) , and reduced volumetric acquisition time [ 24 ]  . 
furthermore , they provide valuable information on the relationships between the lesion and the surrounding mediastinal structures [ 11 ]  . virtual bronchoscopy spiral ct virtual bronchoscopy is a complementary diagnostic technique to conventional bronchoscopy , which has shown interesting results in the detection of endobronchial lesions [ 24 , 26 ]  . 
by exploiting the natural contrast between luminal content and surrounding tissue [ 2 , 3 ] , the 3d reconstruction software allows the user to navigate through the tracheobronchial tree [ 10 ] with same endoluminal perspective as conventional endoscopy [ 13 , 14 ]  . the bronchoscopic images are displayed on the monitor alongside the multiplanar ct axial , sagittal and coronal oblique reference sections , on which the position and direction of the virtual bronchoscope is marked with a cursor . 
this makes it possible to explore the tracheobronchial tree from the inside by moving the cursor on the reference ct sections or by navigating the airway with a kind of virtual airplane , whose direction and speed are controlled through a mouse [ 27 ]  . virtual endoscopy images have a strong visual impact and provide a more complete and panoramic view not only of the 1074 naturale contrasto tra il contenuto aereo endoluminale e il tessuto circostante [ 2 , 3 ] , consente di navigare allinterno dellalbero tracheo - bronchiale [ 10 ] , riproducendo la stessa prospettiva endoluminale del reale esame endoscopico [ 13 , 14 ]  . tali visioni broncoscopiche vengono rappresentate su monitor consensualmente alle sezioni tc multiplanari sul piano assiale , sagittale e coronale obliquo di riferimento , sulle quali vengono evidenziate , mediante un cursore , la posizione e lorientamento del broncoscopio virtuale . 
possibile in tal modo esplorare linterno dellalbero tracheobronchiale spostando il cursore sulle sezioni tc di riferimento o navigando al suo interno utilizzando una sorta di aeroplano virtuale , la cui direzione e velocit vengono regolate utilizzando il mouse [ 27 ]  . lendoscopia virtuale fornisce immagini di grande impatto visivo e fornisce una visione pi panoramica e completa non solo dellalbero tracheo - bronchiale ma anche di tutti gli organi e strutture circostanti [ 28 ]  . 
la adeguata selezione di questo parametro assume una notevole rilevanza in considerazione del fatto che le dimensioni apparenti di una lesione e la sua stessa morfologia , variano nella rappresentazione endoscopica virtuale in funzione del valore soglia prescelto . 
in particolare , quanto pi il valore negativo , tanto pi le dimensioni della lesione risulteranno sovrastimate . la possibilit di percezione delle lesioni molto piccole dipende strettamente dal pitch e dalla collimazione , in un rapporto ormai noto , e cio quanto pi bassi sono tanto pi alta sar la capacit di individuare piccole lesioni [ 24 ]  . 
nel nostro studio stato scelto un protocollo che prevedeva collimazione di 1 , 25 mm con sovrapposizione di 0 , 6 mm , tempo di rotazione di 0 , 6 secondi e noise index di 11 . 
tuttavia , nonostante lottimizzazione dei parametri di scansione , ricostruzione e visualizzazione finalizzata alla riduzione degli artefatti ed al miglioramento della definizione dellimmagine , si avr sempre una certa distorsione dellimmagine correlata alleffetto della rappresentazione prospettica [ 24 ]  . 
da ci deriva come la misura delle dimensioni di una lesione sia maggiormente attendibile sulle ricostruzioni assiali trasverse o multiplanari ( mpr ) bidimensionali che non sulle ricostruzioni broncoscopiche virtuali [ 24 ]  . vantaggi la broncoscopia virtuale ha senzaltro una migliore tolleranza da parte del paziente rispetto a quella convenzionale , risultando un metodo non invasivo , privo delle controindicazioni e delle complicanze proprie della fibrobroncoscopia e affidabile nella valutazione delle patologie delle vie aeree [ 12 , 26 ]  . 
in our study , we used a value of 500 hu as the threshold for optimal representation of the air - mucosa interface , based on our experience and the data reported in the literature . correct selection of this parameter is very important in view of the fact that in the virtual endoscopic representation , the apparent size and morphology of a lesion will change depending on the threshold value selected . 
in particular , the more negative the value , the greater the overestimation of lesion size . the conspicuity of very small lesions closely depends on pitch and collimation , with lower values improving the ability to identify small lesions [ 24 ]  . 
however , despite optimisation of the scan , reconstruction and visualisation parameters to reduce artefacts and improve image resolution , some image distortion will always occur as a result of the perspective rendering effect [ 24 ]  . 
for this reason , measurement of lesion size is more reliable on 2d transverse or axial mpr than on virtual bronchoscopy reconstructions [ 24 ]  . advantages virtual bronchoscopy is no doubt better tolerated by patients than is conventional endoscopy , as it is noninvasive , does not have the contraindications or complications of fiberoptic bronchoscopy , and is very reliable in the assessment of airway disease [ 12 , 26 ]  . 
as a consequence , this technique has become the modality of choice to evaluate response to medical or surgical treatment in cancer patients or to follow up patients who have undergone self - expanding stent placement as a palliative procedure [ 5 , 13 ]  . 
in addition , unlike conventional bronchoscopy [ 14 ] , virtual bronchoscopy is not operator dependent and can be performed in patients in poor clinical condition or in subjects with severe airway stenosis that precludes endoscopic investigation [ 1 ]  . 
in these cases , during the endoscopic simulation , segments can be explored that are not accessible to the bronchoscope , such as those distal to nonnegotiable stenoses or to segmental occlusions , allowing one to establish an indication for procedures that would never have been proposed ( endoscopic laser therapy , stent placement ) [ 6 , 27 ]  . a further major advantage of virtual bronchoscopy is the simultaneous visualisation of both the airway lumen and the mediastinal and hilar structures . 
this is made possible by the display , alongside each virtual image , of the axial and multiplanar ( sagittal and coronal oblique ) reference images that not only enable the correct localisation of endobronchial disease but also provide anatomical and pathological information on structures outside the airway , thereby allowing easier distinction between stenosis and extrinsic compression [ 12 , 26 ]  . 
the images displayed on the monitor can be rotated in different directions to visualise the relationships between mediastinal structures and the airway [ 5 , 12 ]  . the main indication for virtual bronchoscopy is the study of tracheobronchial stenoses , as the technique enables the precise evaluation of the site , size and degree of obstruction , with the possibility of studying the inner surface of the tracheobronchial tree even beyond a subtotal stenosis [ 12 , 29 ]  . risposta ad eventuali terapie o procedure chirurgiche o nel follow - up di pazienti a cui sono stati posizionati stent autoespandibili a scopo palliativo [ 5 , 13 ]  . 
in aggiunta , la broncoscopia virtuale ha come vantaggio , rispetto allendoscopia reale , di non essere una procedura operatore - dipendente [ 14 ] e di poter essere eseguita in pazienti in cattive condizioni cliniche o in soggetti con stenosi severe delle vie aeree , tali per cui non sarebbe possibile lesecuzione dellindagine endoscopica [ 1 ]  . 
in tali casi , durante la simulazione endoscopica , quindi possibile esplorare segmenti non raggiungibili dal broncoscopio , come quelli a valle delle stenosi non superabili o delle occlusioni segmentarie , consentendo di porre lindicazione a procedure altrimenti non proponibili ( laserterapia endoscopica , stent ) [ 6 , 27 ]  . un ulteriore grande vantaggio diagnostico della tecnica virtuale dato dalla possibilit di visualizzare simultaneamente sia il lume delle vie respiratorie che le strutture extra luminali mediastiniche ed ilari . 
questo grazie alla disponibilit , accanto ad ogni immagine virtuale , di immagini assiali e multiplanari ( sagittali e coronali oblique ) di riferimento che consentono non solo una esatta localizzazione di eventuali patologie endobronchiali , ma anche di avere informazioni anatomiche e patologiche sulle strutture esterne alle vie aeree , distinguendo , in tal modo , pi facilmente una stenosi endoluminale da una compressione estrinseca [ 12 , 26 ]  . 
le immagini sul monitor possono essere ruotate secondo diverse angolazioni , aiutando nella visualizzazione dei rapporti tra le strutture mediastiniche e le vie aeree [ 5 , 12 ]  . la principale indicazione della broncoscopia virtuale rappresentata dallo studio delle stenosi dellalbero tracheo - bronchiale , in quanto tale tecnica consente di definire esattamente la sede di ostruzione , lentit ed il grado con possibilit di visualizzare e studiare dallinterno lalbero tracheo - bronchiale oltre una stenosi anche subtotale [ 12 , 29 ]  . 
tali informazioni risultano piuttosto preziose in caso di stenosi neoplastica , nella pianificazione preoperatoria o in previsione del posizionamento di stent endobronchiali per prevenire la completa chiusura del lume bronchiale [ 12 ]  . 
virtual bronchoscopy may precede conventional studies and provide a map of the patients airway anatomy , thus reducing the time needed for bronchoscopic investigation of obstructing lesions [ 1 , 16 ]  . limitations partial volume artefacts , difficulties in visualising bronchial branches with complex orientation , and the differential diagnosis between vegetative lesions and mucosal irregularities on the one hand , and endoluminal pseudolesions related to the presence of mucus , secretions and mucosal sloughing ( responsible for partial volume artefacts ) on the other hand , are the main limitations of the technique [ 24 ]  . another important clinical and diagnostic pitfall is the inability to detect early mucosal changes ( small surface lesions , such as ulcers or plaques ) or the submucosal lymphatic permeation seen in some neoplasms [ 1 , 2 ]  . in addition , data provided by virtual bronchoscopy images alone do not allow distinction between stenoses due to endobronchial masses or to extrinsic compression ; the analysis of surrounding tissues and the study of the length of the stenosis requires simultaneous visualisation of the mpr [ 24 ]  . further limitations include the inability to biopsy the tissue for histological examination [ 1 , 3 , 9 , 15 ] and the fact that , although virtual bronchoscopy can assess the shape of a lesion [ 3 ] , it is unable to distinguish the colour of normal mucosa and pathological tissue [ 1 , 8 ] or to show their texture [ 10 , 16 ]  . conclusions ct and fiberoptic endoscopy are highly sensitive techniques for the evaluation of stenoses of the tracheobronchial tree , although they both present technical limitations that may lead to inaccurate characterisation [ 3 ]  . the introduction of volumetric spiral ct , including mpr and virtual bronchoscopy , has dramatically improved accuracy in establishing the site , extension and severity of endobronchial abnormalities [ 1 ] , thus providing important information for treatment planning . 
virtual bronchoscopy cannot , however , be regarded as an alternative to conventional bronchoscopy but , rather , as its integration , given that the two techniques are complementary [ 27 ]  . our study , performed on obstructive disease of the proximal airway , has demonstrated the high diagnostic accuracy of virtual bronchoscopy , which , when integrated with mpr images , provides data for the detailed classification of tracheobronchial diseases before and after treatment . 
anche la diffusione linfatica sottomucosa presente in alcune forme neoplastiche difficilmente identificabile [ 1 , inoltre , con il solo apporto di informazioni fornite dalle immagini di broncoscopia virtuale non si in grado di distinguere tra stenosi determinate da masse a sviluppo endobronchiale o sottomucoso da compressione ab - estriseco ; la valutazione dei tessuti vicini e la stima dellestensione in lunghezza di una stenosi richiede la simultanea visualizzazione di immagini di ricostruzione multiplanare [ 24 ]  . limite intrinseco alla metodica inoltre lincapacit di eseguire prelievi bioptici per lanalisi isto - citologica del tessuto [ 1 , 3 , 9 , 15 ] e , sebbene riesca a valutare la forma lesionale [ 3 ] , non in grado di distinguere il colore tra la mucosa normale e il tessuto patologico [ 1 , 8 ] n la sua consistenza [ 10 , 16 ]  . conclusioni la tc e lendoscopia a fibre ottiche sono tecniche altamente sensibili per la valutazione delle stenosi dellalbero tracheo - bronchiale , ma entrambe non scevre da limiti tecnici che possono essere causa di una inaccurata caratterizzazione della patologia aerea [ 3 ]  . con lintroduzione della tc spirale volumetrica , inclusa lmpr e la broncoscopia virtuale , sono stati fatti passi avanti nellaccuratezza con cui viene determinata la sede , lestensione e la severit delle anomalie endobronchiali [ 1 ] , fornendo , in tal modo , preziose informazioni per la successiva decisione sul trattamento pi appropriato da intraprendere . 
tuttavia lapproccio virtuale non pu essere considerato come alternativo alla valutazione broncoscopica convenzionale , bens integrativo , ritenendo le due tecniche complementari tra loro [ 27 ]  . il nostro studio , condotto su patologie ostruenti le vie aeree prossimali , ha dimostrato una elevata capacit diagnostica della broncoscopia virtuale che , integrata con immagini mpr , ha fornito utili informazioni per una classificazione dettagliata della patologia tracheo - bronchiale prima e dopo trattamento . 
in considerazione di ci , le ricostruzioni multiplanari e di broncoscopia virtuale possono essere proposte come indagini preliminari per una accurata caratterizzazione della lesione stenotica , per abbreviare i tempi di esecuzione della successiva procedura endoscopica e per la pianificazione del trattamento terapeutico pi appropriato . la broncoscopia virtuale , oltre che utile nel pre - operatorio , pu essere considerata un eccellente metodo riproducibile ed oggettivo per la successiva valutazione della risposta al trattamento in soggetti con stenosi severe delle vie aeree ed in condizioni cliniche tali per cui non sia possibile lesem.g. 
sofia 78 , 95123 catania , italy correspondence to : luca macarini , ab : via conte giusso 3 , 70125 bari , italy , tel : + 39 - 88 - 1736089 , fax : + 39 - 88 - 1733866 e - mail : l.macarini@unifg.it received : 27 december 2005 / accepted : 20 april 2006 / published online : 20 december 2006 abstract purpose . 
the study was performed with a 1.5 - tesla device and characterised by three phases : the first phase without contrast material ( unenhanced mri ) , the second after the administration of ferumoxides ( spio - mri ) , and the third , a double - contrast study following the injection of a bolus of paramagnetic contrast material ( dc - mri )  . 
the sensitivity of unenhanced mri , spiomri and dc - mri in identifying and characterising hepatic focal lesions was assessed , together with the diagnostic increment of one technique with respect to the others . 
lo studio rm stato effettuato con apparecchiatura da 1 , 5 tesla ed consistito di tre fasi : la prima senza mdc ( rm - base ) , la seconda dopo infusione di mdc spio , a contrasto singolo ( rm - spio ) e la terza dopo iniezione a bolo di mdc paramagnetico , a doppio contrasto ( rm - dc )  . 
sono stati valutati la sensibilit della rmbase , della rm - spio e della rm - dc nellidentificazione e nella caratterizzazione delle lesioni focali epatiche e lincremento diagnostico di una metodica rispetto alle altre . 
su 67 pazienti in 14 casi ( 20 , 8% ) erano presenti alterazioni della captazione e della distribuzione del mdc spio di tipo acde che limitavano lesame rm - spio . 
in 5 casi si trattava di fibrosi confluente , in 2 casi di cirrosi scompensata , in 1 caso di trombosi vascolare e in 1 caso di esiti cicatriziali di un paziente operato di 1087 l . 
twenty - three patients had a total of 68 lesions , which consisted of 37 dysplastic nodules ( dn ) , 19 hcc nodules , two relapses of hcc following chemoembolisation , two hcc associated with portal thrombosis , one cancer - cirrhosis , two angiomas and five small cysts . 
spio - luda were the result of vascular thrombosis in one case and fibrosis in four cases . in all of these cases , dc - mri proved useful for diagnosis . 
in our study , the combined use of two contrast agents , negative and positive , provided greater diagnostic confidence and caused no side effects in the patients . key words mr liver cirrhosis contrast medium resezione epatica per hcc . 
ventitre pazienti erano portatori di 68 lesioni rappresentate da : 37 noduli displasici , 19 noduli hcc , 2 recidive di hcc dopo chemioembolizzazione , 2 hcc associati a trombosi portale , 1 cancrocirrosi , 2 angiomi e 5 piccole cisti . 
la sensibilit nellidentificazione delle lesioni stata per la rm - base , la rm - spio e la rm - dc rispettivamente del 57 , 3% , 67 , 6% e 75% . 
lutilizzo combinato dei due mezzi di contrasto , negativi e positivi , consente una migliore confidenza diagnostica e nella nostra esperienza non ha determinato reazioni secondarie nei pazienti . parole chiave rm fegato cirrosi mezzi di contrasto introduction introduzione liver - specific superparamagnetic iron oxide ( spio ) contrast agents are used in the identification and characterisation of focal hepatic lesions and have been proposed for use in the staging of patients undergoing surgical procedures for focal hepatic malignancies [ 18 ]  . 
the use of ferumoxides has been proposed in the follow - up of patients with liver cirrhosis for the detection of hepatocellular carcinoma ( hcc ) , with excellent results [ 911 ]  . 
a number of studies claim that the dynamic study with the injection of a bolus of paramagnetic gadolinium - diethylenetriaminepentaacetic acid ( gd - dtpa ) contrast material is more effective , particularly in detecting small ( < 1.5 cm ) hcc [ 1215 ]  . 
other studies , in contrast , report better results with spio - enhanced imaging , [ 16 , 17 ] while still others have found increased diagnostic accuracy with the combined use of the two contrast agents [ 1822 ]  . reservations regarding the use of spio agents in liver cirrhosis are based on the possibility that the significant subversion of liver structure and function , intrahepatic vascular alterations , presence of inflammatory processes , and steatosis can alter the action of ferumoxides and reduce their effectiveness and that well - differentiated hcc can take up spio in the same way as regenerative nodules ( rn ) and dysplastic nodules ( dn ) , thus making their differentiation difficult [ 2329 ]  . 
the alterations in liver uptake and distribution of spio that can oc1088 i mezzi di contrasto ( mdc ) superparamagnetici epatospecifici a base di particelle di ossido di ferro ( spio ) sono utilizzati per lidentificazione e la caratterizzazione delle lesioni focali epatiche e il loro uso stato proposto per lo staging di pazienti da sottoporre a trattamenti chirurgici o loco - regionali per lesioni focali epatiche maligne [ 18 ]  . luso di mdc spio stato proposto anche nel follow - up dei pazienti portatori di cirrosi epatica per lidentificazione dellepatocarcinoma ( hcc ) con ottimi risultati [ 911 ]  . 
alcuni autori sostengono la superiorit dello studio dinamico dopo iniezione a bolo di mdc paramagnetico gd - dtpa soprattutto nellidentificazione dei piccoli ( 1 , 5 cm ) hcc [ 1215 ] , altri invece hanno rilevato migliori risultati con i mdc spio [ 16 , 17 ] ed altri infine hanno verificato un miglioramento diagnostico nellutilizzo combinato dei due mezzi di contrasto [ 1822 ]  . le riserve sulluso dei mdc spio nella cirrosi epatica si basano sulla possibilit che in tale patologia il notevole sovvertimento della struttura e delle funzioni epatiche , le alterazioni vascolari intraepatiche , la presenza di processi flogistici e la steatosi possano alterare il meccanismo dazione dei mdc spio , riducendone lefficacia e che gli hcc ben differenziati possano captare i mdc spio come i noduli di rigenerazione ( nr ) e i noduli displasici ( nd ) rendendone difficile lidentificazione e la caratterizzazione [ 2329 ]  . 
spio - luda appear on the mr images either as areas of hyperintense signal in which the contrast medium is absent or as areas of hypointense signal in which the contrast medium is more concentrated . 
nonetheless , spio - luda are an expression of changes to the liver parenchyma that occur in cirrhosis , and their recognition helps in understanding the causes of disease and provides useful information regarding its stage [ 30 ]  . as the survival of patients with cirrhosis is related to timely and appropriate treatment of hcc and its recurrences [ 31 , 32 ] , in cirrhotic patients with spio - luda or problems of focal lesion characterisation on spio - mri , completion of the mr examination with an injectable paramagnetic contrast medium having extracellular distribution could prove useful . 
to this end , several studies have proposed the sequential use during the same examination of spio contrast media and gadolinium chelates to exploit the increased contrast obtained with the simultaneous use of negative superparamagnetic and positive paramagnetic contrast media [ 2022 , 33 ]  . the aim of our study was to assess the role of doublecontrast mri ( dc - mri ) in the study of the cirrhotic liver with the sequential use of negative superparamagnetic spio and gadolinium - based positive paramagnetic contrast media and to compare the findings with unenhanced mri and spio - mri , paying special attention to those cases in which spio - luda were present on spio - mri . materials and methods sixty - seven patients affected by liver cirrhosis and scheduled for liver transplant underwent dc - mri . 
the screening protocol for all patients involved liver ultrasound ( us ) and alpha - fetoprotein testing every 6 months , and mri every 12 months or , in the presence of a hepatic nodule at us or elevated alpha - fetoprotein levels , every 6 months . 
the mri study was performed with a 1.5 - tesla device and consisted of three phases : the first without the use of contrast medium ( unenhanced mri ) ; the second , the single - contrast phase , after spio administration ( spio - mri ) ; and the third , the double - contrast study , after the injection of paramagnetic contrast medium ( dc - mri )  . 
sulle immagini rm le acde sono rappresentate da aree di segnale iperintenso in cui assente mdc o aree di segnale ipointenso in cui il mdc pi concentrato , possono simulare la presenza di lesioni focali o impedirne il riconoscimento , rendere difficoltosa la loro caratterizzazione o la valutazione delle loro dimensioni . 
in ogni caso le acde sono espressione di alterazioni del parenchima epatico che si verificano nella cirrosi e il loro riconoscimento permette la comprensione delle cause che le hanno determinate fornendo utili informazioni sullo stadio della malattia [ 30 ]  . siccome la sopravvivenza dei malati di cirrosi legata al trattamento tempestivo e adeguato dellepatocarcinoma e delle sue recidive [ 31 , 32 ] nei casi di cirrosi epatica in cui lesame rm eseguito con mdc spio presenti alterazioni del tipo delle acde o problemi di caratterizzazione di lesioni focali , potrebbe risultare utile completare lesame rm con limpiego di un mdc paramagnetico a distribuzione extracellulare , iniettabile a bolo . 
a tal fine alcuni autori hanno proposto lutilizzo sequenziale , nella stessa seduta di rm , dei mdc spio e dei chelati del gadolinio , per sfruttare lincremento di contrasto che si ottiene dallazione contemporanea di mezzi di contrasto superparamagnetici negativi e paramagnetici positivi [ 2022 , 33 ]  . scopo del nostro lavoro stato quello di valutare il contributo nello studio del fegato cirrotico della tecnica rm a doppio contrasto ( rm - dc ) , con impiego sequenziale di mdc superparamagnetici negativi spio e paramagnetici positivi a base di gadolinio , confrontandolo con gli esami rm di base e con mdc spio , con particolare attenzione a quei casi in cui allesame rm - spio si verificano alterazioni del comportamento contrastografico del tipo delle acde . materiali e metodi abbiamo studiato con rm - dc 67 pazienti affetti da cirrosi epatica in lista dattesa per trapianto epatico . 
in tutti i pazienti il protocollo di screening prevedeva lesecuzione semestrale di un esame ecografico del fegato , il dosaggio dellalfa - feto - proteina e lesecuzione annuale , o in seguito allidentificazione con lecografia di un nodulo epatico da caratterizzare o a un rialzo dellalfa - feto - proteina , dellesame rm . 
lo studio rm stato effettuato con apparecchiatura da 1 , 5 tesla ed consistito di tre fasi : la prima senza mdc ( rm - base ) , la seconda dopo infusione di mdc spio , a contrasto singolo ( rm - spio ) e la terza dopo iniezione a bolo di mdc paramagnetico , a doppio contrasto ( rm - dc )  . 
the slice thickness in all sequences was 8 mm with a 1 mm gap , the matrix was 128256 , and the field of view ( fov ) was 380450 mm with reconstruction algorithm of the matrix ( rfov ) of 3 / 4 . 
 we assessed the sensitivity of unenhanced mri , spiomri and dc - mri in detecting and characterising focal hepatic lesions , as well as the diagnostic increment of one technique with respect to the others . 
to assess the detection rate , we considered the number of lesions identified by unenhanced mri , spio - mri and dc - mri and calculated the sensitivity of the various techniques . 
to assess lesion characterisation , we evaluated three groups of images : the first group consisted of the unenhanced mr images , the second group consisted of the unenhanced mr images plus the spio - mr images , and the third group consisted of the images from the second group plus the dc - mr images . 
the following lesion parameters were considered : signal intensity ( si ) on the unenhanced mr images , rate of signal loss ( rsl ) on the spio - mr images compared with the unenhanced - mr images , and type of contrast enhancement ( ce ) on the dc - mr images . 
the structural characteristics of lesions , as revealed by the double - contrast technique , and in particular , vascularity and the presence of areas of necrosis or a pseudocapsule , were also assessed . the final diagnosis for lesion identification was made by radiologists working in consensus on the basis of the overall assessment of radiological examinations before and after mri and clinical - radiological follow - up in all cases . 
with regard to lesion characterisation , the definitive diagnosis was made on the basis of histological findings in 38 cases , lipiodol - ct in 13 cases , multidetector ct in 17 cases and clinical - radiological follow - up in all cases . 
liver and kidney function tests , blood tests and urinalysis were performed in all patients in the 2448 h before and after the mr study . results 1090 focal lesions were absent in 44 / 67 patients and present in 23 / 67 patients . 
in tutte le sequenze lo spessore di strato stato di 8 mm con gap di 1 mm , la matrice di 128256 , il campo di vista ( fov ) 380450 mm , con algoritmo di ricostruzione della matrice ( rfov ) di 3 / 4 . 
per lidentificazione stato considerato il numero delle lesioni identificate dalla rm - base , dalla rm - spio e dalla rm - dc calcolando rispettivamente la sensibilit delle varie metodiche . 
per la caratterizzazione sono stati valutati separatamente tre gruppi di immagini : il primo gruppo stato quello delle immagini ottenute dalla rm - base , il secondo da quello delle immagini della rm - base insieme a quelle della rm - spio ed il terzo da quello delle immagini della rm - base insieme a quelle della rm - spio e della rm - dc . 
sono stati considerati i seguenti parametri delle lesioni : sulle immagini rm di base le caratteristiche dintensit di segnale ( si ) ; in quelle dopo mdc spio la percentuale di perdita di segnale ( pps ) delle lesioni rispetto allesame di base ; in quelle a doppio contrasto il tipo di enhancement contrastografico ( ce ) dopo iniezione a bolo . 
sono state rilevate , inoltre , le caratteristiche strutturali delle lesioni che la tecnica a doppio contrasto ha permesso di evidenziare ed in particolare la vascolarizzazione , la presenza di aree di necrosi o di una pseudocapsula . la diagnosi finale per lidentificazione di lesione stata posta da un consenso di radiologi sulla base della valutazione complessiva delle indagini radiologiche pree post - rm e del follow - up clinico - radiologico in tutti i casi . 
per quanto riguarda la caratterizzazione delle lesioni la diagnosi definitiva stata fatta sulla base di accertamenti istologici in 38 casi , della lipiodol - tc in 13 casi , della tc multi - detettore in 17 casi e del follow - up clinico - radiologico in tutti i casi . in tutti i pazienti sono stati controllati prima e dopo 2448 h l . 
unenhanced magnetic resonance imaging ( mri ) ( a ) with t1 - weighted fast low - angle shot ( flash ) sequence reveals an irregular , multinodular appearance suspicious for recurrence at the site of resection ( arrows )  . 
la rm di base ( a ) , con sequenza flash t1w , dimostra un aspetto irregolarmente pluri - nodulare a livello della sede del pregresso intervento sospetto per recidiva locale ( frecce )  . 
these cases exhibited focal or diffuse areas of lack of spio uptake , which either simulated the presence of lesions or reduced the ability of spio to identify the in particular , in the case of decompensated cirrhosis , there was failure to absorb the contrast medium by the entire liver . 
in the patient with vascular thrombosis , dc - mri identified two hcc within an area of lack of spio uptake due to reduced blood flow , from which the two hcc could not be dissociated . 
in 14 casi ( 20 , 8% ) erano presenti alterazioni della captazione e della distribuzione del mdc spio tipo acde , di cui 9 in pazienti privi di lesioni e 5 in pazienti con lesioni focali . acde in pazienti privi di lesioni focali in 44 pazienti la rm non ha evidenziato le lesioni focali epatiche e tale dato stato confermato dal follow - up clinico - radiologico a 1 anno . 
in questi casi erano presenti aree focali o diffuse di mancata captazione del mdc spio che potevano simulare la presenza di lesioni o ne riducevano la capacit di identificazione del mdc spio . 
in tutti questi casi il completamento dellesame rm con la tecnica a doppio contrasto ha chiarito il quadro rm , confermando lassenza di lesioni focali . acde in pazienti con lesioni focali in 23 pazienti con lesioni focali epatiche erano presenti acde in 5 casi ( 21 , 7% )  . 
nel paziente con trombosi vascolare la rm - dc ha identificato due hcc allinterno di unarea di assenza di captazione del mdc spio per ridotto apporto vascolare e dalla quale i due hcc non erano dissociabili . 
contrast - enhanced computed tomography ( ct ) ( a ) demonstrates slight enhancement at the level of the right - lobe nodule ( arrows ) , suspicious for recurrence . 
unenhanced magnetic resonance imaging ( mri ) ( b ) with a spinecho ( se ) t2 - weighted sequence shows slight hyperintensity at the level of the nodule in the right lobe ( arrows )  . 
2a - d ripresa di malattia in paziente sottoposto a chemioembolizzazione di un hcc del lobo destro e piccolo hcc consensuale del lobo sinistro . la tc ( a ) con mdc dimostra un tenue ce a livello del nodulo del lobo destro trattato con chemioembolizzazione ( frecce ) sospetta per recidiva di malattia . 
la rm - spio ( c ) dimostra unassenza di captazione di mdc spio a livello della sede del nodulo sottoposto a chemioembolizzazione ( frecce ) e unaltra lesione nodulare del lobo sinistro ( punta di frecce )  . 
non sono stati identificati con tutte le tre metodiche rm 17 nd , riscontrati allesame istologico effettuato sui pezzi operatori dei pazienti sottoposti ad intervento chirurgico di resezione epatica , in quanto i nd presentavano caratteristiche di segnale e contrastografiche simili a quelle del parenchima epatico cirrotico limitrofo . identificazione delle lesioni in 23 / 67 pazienti sono state identificate 68 lesioni del diametro medio di 2 , 8 cm ( range 0 , 710 cm )  . 
le lesioni erano rappresentate da : 37 nd , 19 hcc , 2 recidive di hcc dopo chemio - embolizzazione , 2 hcc associati a trombosi portale , 1 cancro - cirrosi , 2 angiomi e 5 piccole cisti . 
la sensibilit nellidentificazione di lesione focale di diametro minimo di 1 cm circa stata rispettivamente per la rm - base , la rm - spio e la rmdc del 57 , 3% , 66 , 1% e 75% ( tabella 1 )  . 
la rm di base non ha identificato 7 hcc , 17 nd , le 2 recidive hcc dopo chemio - embolizzazione , i 2 hcc associati a trombosi portale e la cancro - cirrosi . 
unenhanced magnetic resonance imaging ( mri ) with fast low - angle shot ( flash ) t1 - weighted ( a ) and spin - echo ( se ) t2weighted ( b ) sequences reveals a slightly hyperintense nodule on the t2weighted images ( arrows )  . 
superparamagnetic iron oxide ( spio ) - mri ( c ) reveals an uptake of ferumoxide , which is barely distinguishable from the surrounding liver parenchyma ( arrows )  . 
lesame rm di base , con sequenze flash t1w ( a ) e se t2w ( b ) , dimostra una lesione nodulare discretamente iperintensa in nelle immagini t2w ( frecce )  . allesame rm - spio ( c ) la lesione presenta una captazione di mdc spio ed mal differenziabile dal parenchima epatico limitrofo ( frecce )  . 
4a - d massive cancer - cirrhosis of the left lobe with portal thrombosis . unenhanced magnetic resonance imaging ( mri ) ( a ) performed with t1weighted sequence shows a diffuse signal alteration in the left lobe , which appears inhomogeneously hypointense ( arrows )  . 
superparamagnetic iron oxide ( spio ) - mri ( b ) performed with t2 * - weighted sequence reveals lack of spio uptake by the left lobe ( arrows )  . 
4a - d cancro - cirrosi massiva del lobo sinistro con trombosi portale . lesame rm di base ( a ) , con sequenza t1w , dimostra una diffusa alterazione di segnale del lobo sinistro del fegato che appare disomogeneamente ipointenso ( frecce )  . 
lesame rm - spio ( b ) , con sequenza t2 * w , dimostra lassenza di captazione di mdc spio da parte del lobo sinistro epatico ( frecce )  . 
all three mri techniques missed 17 dn identified at histology of the resected liver specimens in that dn present signal and enhancement characteristics similar to those of the surrounding cirrhotic liver parenchyma . lesion identification in 23 / 67 patients , a total of 68 lesions with a mean diameter of 2.8 cm ( range 0.710.0 cm ) were identified . 
la rm - dc non ha identificato 17 nd . caratterizzazione delle lesioni i risultati ottenuti sul piano della caratterizzazione delle lesioni sono stati rispettivamente per la rm di base del 20 , 5% , per la rm - spio del 63 , 2% e per la rm - dc del 73 , 5% ( tabella 2 )  . 
la rm - base non ha caratterizzato nessun nd , nessuna recidiva hcc dopo chemio - embolizzazione , i due hcc associati a trombosi portale e la cancro - cirrosi , mentre ha caratterizzato solo 8 noduli hcc , e 1 angioma ; la rm - spio non ha caratterizzato 2 noduli hcc , 2 riprese di malattia in hcc trattati con chemio - embolizzazione , 1 angioma , i 2 hcc associati a trombosi portale e la cancro - cirrosi , mentre la rm - dc ha caratterizzato correttamente tutte le lesioni ad eccezione dei 17 nd , che non erano stati identificati , e di un angioma che stato erroneamente interpretato come un hcc . 
le formazioni cistiche sono state valutate correttamente con tutte tre le metodiche ma erano di difficile interpretazione con la rm - spio , se questa non era confrontata con le immagini di base senza mdc . incremento diagnostico lincremento diagnostico della rm - spio sulla rm base e della rm - dc sulla rm - spio stato rispettivamente nellidentificazione del 9% e del 8 , 9% ( tabella 1 ) e nella caratterizzazione del 42 , 7% e del 10 , 3% ( tabella 2 )  . reazioni avverse in nessun caso abbiamo registrato effetti collaterali indesiderati a seguito della somministrazione sequenziale dei due mdc , n si sono verificate alterazioni dei parametri bioumorali nei controlli a 2448 h . discussione i mezzi di contrasto superparamagnetici hanno migliorato notevolmente laccuratezza diagnostica della rm nello studio delle lesioni focali epatiche consentendo di identificare lesioni di dimensioni al di sotto del cm con elevata accuratezza diagnostica [ 35 , 3436 ]  . 
anche per quanto riguarda la caratterizzazione delle lesioni la rm - spio risultata valida e competitiva con la rm eseguita con mezzi di contrasto paramagnetici iniettabili a bolo [ 17 ]  . 
tuttavia ancora oggi non esistono risultati definitivi su quale sia il mdc e la tecnica di studio rm migliore per lo studio della cirrosi epatica e per lidentificazione e caratterizzazione degli hcc [ 10 , 1214 , 18 , 19 , 37 ]  . 
le due tecniche di studio rm pi utilizzate sono rappresentate da quella dinamica dopo iniezione a bolo di mdc paramagnetico gd - dtpa e da quella con mdc spio epatospecifico . 
i dati della letteratura che riguardano queste due metodiche sono discordanti . lo studio dinamico dopo iniezione a bolo di mdc gd - dtpa secondo alcuni presenta una maggiore sensibilit 1093 l . 
la rm - base ( a ) dimostra una piccola lesione nodulare tenuemente iperintensa ( frecce )  . la rm - spio ( b ) dimostra una mancata captazione della lesione ( frecce )  . 
la rm - dc ( c ) dimostra un marcato ce del piccolo hcc in fase arteriosa . consisted of 37 dn , 19 hcc , two hcc recurrences after chemoembolisation , two hcc associated with portal thrombosis , one cancer - cirrhosis , two angiomas and five small cysts . 
unenhanced mri failed to identify seven hcc , 17 dn , the two hcc recurrences following chemoembolisation , the two hcc associated with portal thrombosis and the cancer - cirrhosis . 
spiomri failed to identify two hcc , 17 dn , the two hcc recurrences following chemoembolisation and the two hcc nellidentificazione di piccoli hcc di diametro inferiore al cm [ 12 ]  . 
innanzitutto in tutti i lavori pubblicati su tale argomento la maggior parte dei piccoli hcc identificati come aree di enhancement vascolare in fase arteriosa non hanno avuto una conferma istologica [ 16 ]  . 
inoltre alcuni autori hanno dimostrato che oltre il 52% di queste aree di enhancement vascolare in fase arteriosa nel fegato cirrotico sono da riferire a shunt artero - venosi o a nd e non a hcc e che quindi lo studio con gd - dtpa altafig . 
unenhanced mri failed to characterise the dn , the hcc recurrences following chemoembolisation , the two hcc associated with portal thrombosis and the cancer - cirrhosis , whereas it correctly characterised only eight hcc and one angioma . 
spio - mri failed to characterise two hcc , the two hcc recurrences following chemoembolisation , one angioma , the two hcc associated with portal thrombosis and the cancer - cirrhosis . 
la rm - dc ( b ) dimostra un piccolo hcc ( freccia ) che presenta ce dopo iniezione di mdc paramagnetico . mente sensibile ma molto poco specifico [ 16 , 37 ]  . 
hanno rilevato che le piccole aree di enhancement vascolare in fase arteriosa con i mdc gd - dtpa che non presentano captazione di mdc spio sono sempre hcc e quindi nel loro lavoro hanno concluso che lutilizzo di entrambi i mdc migliora laccuratezza diagnostica della metodica [ 19 ]  . anche lo studio rm del fegato cirrotico con mdc spio pu presentare delle limitazioni in relazione alla presenza di acde causate con meccanismi patogenetici diversi daltable 1 identification of focal lesions : sensitivity of unenhanced magnetic resonance imaging ( mri ) , superparamagnetic iron oxide ( spio ) - mri and double - contrast ( dc ) - mri in 23 patients histological type no . 
with regard to lesion characterisation , spio - mri has also proved a valid technique , which is competitive with mri performed with injectable paramagnetic contrast media [ 17 ]  . 
nonetheless there are still no definitive findings as to which contrast medium and mri technique is best suited for studying liver cirrhosis and identifying and characterising hcc [ 10 , 13 , 14 , 18 , 19 , 37 ]  . 
the two most widely used techniques are dynamic mri following a bolus injection of paramagnetic gd - dtpa , and mri with liver - specific spio . the literature data on these two techniques are in disagreement . 
according to some studies , dynamic mri following a bolus injection of gd - dtpa has greater sensitivity in the identification of small hcc with a diameter less than 1 cm [ 12 ]  . 
firstly , in all the studies on the subject , the majority of small hcc identified as areas of arterial - phase enhancement were not confirmed histologically [ 16 ]  . 
in addition , some studies have shown that more than 52% of these areas of arterial - phase enhancement in the cirrhotic liver are caused by arteriovenous shunts or dn and not hcc , such that the study with gd - dtpa is highly sensitive but poorly specific [ 16 , 37 ]  . 
found that the small areas of arterial - phase enhancement with gd - dtpa that fail to take up spio are always hcc , leading the authors to conclude that the use of both contrast media increases diagnostic accuracy [ 19 ]  . spio - mri of the cirrhotic liver also suffers some limitations due to the presence of spio - luda caused by a variety of pathogenetic mechanisms , including fibrosis , vascular thrombosis , hepatitis and steatosis [ 20 ]  . 
such alterations may mimic the presence of focal lesions , prevent their detection or affect the assessment of lesion size or the results of lo1096 la fibrosi , dalle trombosi vascolari , delle epatiti e dalla steatosi [ 20 ]  . 
tali alterazioni possono simulare la presenza di lesioni focali , impedirne lidentificazione , alterare la valutazione delle loro reali dimensioni o dei risultati dei trattamenti loco - regionali con importanti risvolti clinici [ 2426 , 28 , 38 ]  . 
il meccanismo dazione dei mezzi di contrasto spio si basa sulla captazione selettiva delle nanoparticelle di ossido di ferro da parte delle cellule del sistema reticolo - endoteliale , in particolare dalle cellule di kupffer epatiche , presenti nel fegato normale e in alcune lesioni focali benigne e assenti nelle lesioni maligne [ 34 , 36 ]  . 
perch il mezzo di contrasto spio agisca sono fondamentali la presenza di un numero adeguato di cellule di kupffer con normale attivit macrofagica e la presenza di un normale flusso vascolare epatico per garantire un sufficiente apporto di mdc . 
le varie patologie alla base delle acde nel fegato cirrotico determinano , con meccanismi patogenetici differenti , alterazioni che agiscono direttamente sul funzionamento del mdc spio e quindi sulla sua captazione intracellulare e sulla sua distribuzione nel parenchima epatico . la fibrosi epatica non presenta al suo interno cellule di kupffer e allesame rm - spio rappresentata da aree iperintense di mancata captazione di mdc , di aspetto reticolare o focale , localizzate pi frequentemente in sede sottodiaframmatica , associate spesso a retrazione della superficie parenchimale . 
la fibrosi epatica assume un aspetto confluente nel 14% dei pazienti con cirrosi avanzata , con problemi di diagnosi differenziale con la cancro - cirrosi [ 28 , 39 ]  . le alterazioni vascolari , e in particolare la riduzione di afflusso vascolare conseguenti alle trombosi , possono determinare zone di ridotta o assente captazione di mdc spio , che assumono una morfologia legata al territorio tributario della struttura vascolare interessata e a volte possono simulare la presenza o impedire il riconoscimento di lesioni focali . 
alcuni autori , in particolare , hanno sottolineato la comparsa di pseudo - lesioni in pazienti studiati con mezzi di contrasto spio in sede peritumorale [ 29 , 40 ]  . tali pseudo - lesioni sarebbero determinate da riduzione del flusso vascolare conseguente a shunt vascolari peritumorali o da riduzione dellazione macrofagica per sofferenza l . 
the mechanism by which spio contrast agents act is based on the selective uptake of iron oxide nanoparticles by the cells of the reticuloendothelial system , especially the kupffer cells , which are present in the normal liver and in some benign focal lesions but absent in malign lesions [ 34 , 36 ]  . 
for the spio contrast agents to act , a sufficient number of kupffer cells with normal macrophagic activity must be present together with normal liver blood flow to guarantee a sufficient supply of contrast medium . the various conditions responsible for spio - luda in the cirrhotic liver cause changes that act directly on the functioning of the spio agent and therefore on its intracellular uptake and its distribution in the liver parenchyma . kupffer cells are not present within hepatic fibrosis so that at spio - mri , fibrosis appears as hyperintense areas of lack of spio uptake , with reticular or focal appearance , most frequently located directly below the diaphragm and often associated with retraction of the parenchymal surface . 
hepatic fibrosis has a confluent appearance in 14% of patients with advanced cirrhosis , thus complicating the differential diagnosis with cancer - cirrhosis [ 28 , 39 ]  . vascular changesand in particular , reduced blood supply due to thrombosiscan lead to areas of reduced or abdelle cellule di kupffer e si localizzano caratteristicamente in sede periferica , a valle della lesione neoplastica . 
gli esami bioptici di tali pseudo - lesioni hanno dimostrato parenchima epatico normale , ma anche aree di linfangite carcinomatosa e di flogosi peri - tumorale [ 40 ]  . 
sulle immagini rm dopo iniezione di mezzo di contrasto spio tali aree creano un alone peri - tumorale di assenza di mdc che non distinguibile dalla lesione neoplastica e ne impedisce la definizione dei margini . 
tale sovradimensionamento rende lesame non utilizzabile per una corretta valutazione topografica e volumetrica della lesione , soprattutto quando si voglia eseguire un trattamento locale di termoablazione o alcolizzazione in cui necessario stabilire con certezza i margini della lesione da trattare . 
such pseudolesions are thought to be caused by a reduction in blood flow resulting from peritumoural vascular shunts or a reduction in macrophage activity due to kupffer - cell damage , and they are characteristically found peripherally and distal to the neoplastic lesion . biopsy of pseudolesions has revealed normal liver parenchyma but also areas of carcinomatous lymphangitis and peritumoural inflammation [ 40 ]  . 
on spio - mr images , the areas of reduced or absent uptake produce a peritumoural halo of nonenhancement , which is indistinguishable from the neoplastic lesion and prevents definition of its margins . 
this size overestimation makes the examination useless for the correct assessment of lesion position and size , especially when planning local treatments such as thermoablation or alcohol ablation , which require precise definition of lesion margins . 
indeed , a reduction in spio uptake has been reported in areas of liver parenchyma that have undergone radiotherapy of a tumour and where there is a resulting postactinic hepatitis [ 41 ]  . decompensated cirrhosis in the acute phase may also exhibit reduced spio uptake due to inflammatory processes hampering the macrophagic activity of kupffer cells . 
in acute hepatitis , reduced spio uptake translates into an 11% signal loss compared with a 75% signal loss in normal liver parenchyma and a 52% loss in cirrhotic tissue [ 25 ]  . 
in hepatitis , there is a reduction in the function of the kupffer cells and a reduction in their number per gram of tissue [ 25 , 34 ]  . 
in addition , reduced hepatic clearance of spio is thought to be the result of reduced opsonisation , which is found in hepatitis and cirrhosis , because plasma fibronectin , an opsonin believed to enhance the phagocytic activity of kupffer cells , is reduced [ 25 ]  . in all of these cases where enhancement patterns may give rise diagnostic uncertainty , it might be worthwhile to assess not only intracellular spio uptake but also the dynamic vascular enhancement patterns after administration of gadolinium - based media . 
one study has proposed the combined use of two - positive and negative - contrast media , reporting better contrast - to - noise ratio between the liver and the lesion using the double - contrast technique [ 42 ]  . 
this approach enables the two contrast media to be administered in the same session without significant lengthening of examination times and with the summing of the different enhancement effects of the two media [ 20 ]  . 
moreover , the double - contrast technique can be seen as the completion of the spio - mr examination , and therefore the administration of gd - dtpa is optional and should be used only when diagnostic uncertainties are present . 1098 sentare una mancata o ridotta captazione del mdc spio per linibizione su base flogistica dellattivit macrofagica delle cellule di kupffer . 
nelle epatiti acute si ha una ridotta captazione di spio che si traduce in una perdita di segnale dell11% , rispetto alla perdita di segnale del 75% riscontrata nel parenchima epatico normale e del 52% in quello cirrotico [ 25 ]  . 
nellepatite , infatti , si ha una riduzione della funzionalit delle cellule di kupffer ed una loro riduzione numerica per grammo di tessuto [ 25 , 34 ] ; inoltre la ridotta clearance epatica di spio sarebbe imputabile anche ad una ridotta opsonizzazione , riscontrabile nelle epatiti come anche nella cirrosi , poich la fibronectina plasmatica , unopsonina che potenzierebbe lattivit fagocitaria delle cellule di kupffer , ridotta [ 25 ]  . in tutti questi casi in cui il comportamento contrastografico pu determinare delle incertezze diagnostiche pu essere utile valutare , oltre che la captazione del mdc spio intra - cellulare , anche il comportamento vascolare dinamico delle lesioni dopo somministrazione a bolo di mdc paramagnetici a base di gadolinio . 
a tale proposito alcuni autori hanno proposto luso combinato di due mezzi di contrasto , positivi e negativi , dimostrando un incremento del rapporto c / n tra fegato e lesione con la tecnica a doppio contrasto [ 42 ]  . 
tale metodologia consente la somministrazione di due mdc nella stessa seduta , senza un significativo allungamento del tempo desame e con sommazione degli effetti contrastografici differenti dei due mdc [ 20 ]  . 
 [ 21 ] hanno evidenziato con la tecnica a doppio contrasto una migliore definizione della caratteristiche strutturali interne delle lesioni , che ha consentito una diagnosi di natura pi agevole . 
 [ 22 ] hanno rilevato che la rm - dc pi accurata nellidentificazione delle lesioni rispetto alla rm - spio , mentre non hanno riscontrato differenze statisticamente significative nella caratterizzazione , pur segnalando una pi agevole confidenza diagnostica . tale autore , tuttavia , non ha utilizzato nel suo studio sequenze ge t2 * w in apnea , che si sono dimostrate successivamente le pi sensibili nellidentificazione delle lesioni quando utilizzato mdc spio [ 7 , 11 ]  . 
 [ 33 ] hanno rilevato , invece , una maggiore sensibilit della rmspio rispetto alluso combinato dei due mezzi di contrasto nellidentificazione delle lesioni ed hanno concluso che luso del doppio mezzo di contrasto non necessario nello studio del fegato cirrotico . nella nostra esperienza su pazienti con cirrosi epatica i maggiori vantaggi della doppia somministrazione di mdc si sono ottenuti quando erano presenti alterazioni della captazione e della distribuzione del mdc spio del tipo delle acde conseguenti a fibrosi , trombosi vascolare , cirrosi scompensata , trattamenti di chemio - embolizzazione o quando erano necessarie ulteriori informazioni per caratterizzare una lesione focale . 
in their study , however , the authors did not use ge t2 * - weighted breath - hold sequences , which have since proved to be more sensitive for lesion detection with spio - mri [ 7 , 11 ]  . 
in cases exhibiting spio - luda , the action of spio was reduced , creating difficulties in lesion detection and characterisation . completion of the mr study with a bolus injection of paramagnetic contrast material proved crucial for obtaining information useful for the diagnosis . 
this was done during the same mr session , immediately after the assessment of the spio - mr images , without having the patient leave the mri room and therefore without further time delays and logistic problems of rescheduling an mr examination . in lesion identification , the greater enhancement obtained with the sequential administration of two contrast media improved the diagnostic confidence of dc - mri with respect to spio - mri by 8.9%. 
in most cases , spio - luda were caused by fibrosis or vascular thrombosis , and the administration of gd - dtpa facilitated the recognition and delimitation of the focal lesions in the areas of nonuptake of spio . the sensitivity values in identifying focal lesions for the three techniques , and in particular the contrast - enhanced examinations , were not particularly high due to the failure to identify 17 low - grade dn , which were identified only at histology of the surgical specimen . 
these dn could not even be identified on review of the unenhanced and contrast - enhanced mr images in that they were not distinguishable from cirrhotic liver parenchyma or regenerative nodules . even in cases without focal lesions , dc - mri proved useful in the event of spio - luda preventing definitive exclusion of focal lesions . in lesion characterisation , administration of the two contrast media enabled the study of the lesions vascular dynamics , thus adding information that produced a diagnostic increment of 10.3% with respect to spio - mri . 
the additional information regarded the lesions structural characteristics , such as the presence of areas of necrosis or a pseudocapsule or the type of vascular enhancement , which permitted better assessment of the hcc and the two cases of hcc recurrence after chemoembolisation and differentiation from dn . 
with regard to characterisation of focal lesions , there may be problems differentiating between hcc and dn because both can display a hyperintense signal in the nonenhanced t1 - weighted sequences whereas they diserano presenti acde lazione del mdc spio era ridotta con difficolt di identificazione e caratterizzazione delle lesioni . 
stato possibile effettuare ci nella stessa seduta rm , immediatamente dopo la valutazione delle immagini ottenute con mdc spio , senza far uscire il paziente dalla sala di rm e , quindi , senza ulteriore perdita di tempo e senza problemi organizzativi relativi alla riprogrammazione dellesame nellidentificazione delle lesioni il maggior contrasto ottenuto dalla doppia somministrazione ha migliorato la confidenza diagnostica della rm - dc rispetto alla rmspio dell8 , 9% . 
nella maggior parte di questi casi erano presenti acde determinate da fibrosi o da trombosi vascolari in cui lapporto del mdc gd - dtpa iniettato a bolo ha consentito di riconoscere e delimitare meglio le lesioni focali nellambito di aree di mancata captazione di mdc spio . 
i valori di sensibilit nella identificazione delle lesioni focali delle tre metodiche di studio rm , in particolare di quelle contrastografiche , non sono risultati particolarmente elevati per la mancata identificazione di 17 nd a basso grado , che sono stati rilevati solo dallesame istologico su pezzo operatorio . 
questi nd non sono stati identificati neanche in una rivalutazione a posteriori delle immagini rm di base e contrastografiche , in quanto non erano differenziabili dal parenchima epatico cirrotico o dai noduli di rigenerazione . 
anche nei casi in cui non erano presenti lesioni focali la rm - dc stata utile quando alla rm - spio erano presenti alterazioni del tipo delle acde che non consentivano di escludere con certezza la presenza di lesioni focali . nella caratterizzazione delle lesioni , la doppia somministrazione di mdc permette di studiare la dinamica vascolare delle lesioni aggiungendo informazioni diagnostiche che hanno determinato un incremento diagnostico rispetto alla rm - spio del 10 , 3% . 
si sono aggiunte informazioni sulle caratteristiche strutturali delle lesioni , come la presenza di aree di necrosi o di una pseudocapsula o il tipo di enhancement vascolare , che hanno consentito una migliore valutazione degli hcc , della ripresa di malattia nei due casi di hcc sottoposti ad intervento di chemio - embolizzazione e della diagnosi differenziale con i nd . 
nellambito della caratterizzazione delle lesioni focali esistono in alcuni casi problemi di diagnosi differenziale tra i nd e gli hcc , poich possono apparire entrambi di segnale iperintenso nelle sequenze pesate in t1 senza mdc , mentre mostrano un comportamento di segnale variabile nelle sequenze pesate in t2 [ 43 ]  . 
tale comportamento contrastografico stato tipico in tutti i nd da noi evidenziati , successivamente sottoposti a controllo istologico , e differisce in maniera sostanziale da quello dei noduli di hcc , che non presentano captazione di mdc . 
these enhancement patterns were seen in all dn we encountered , which were later confirmed histologically , and differed substantially from those of hcc nodules , which presented no uptake of the contrast mediuthe greater uptake of spio by dn could be due to increased activity of the kupffer cells [ 44 ] and the different vascularisation , which is portal in dn but prevalently arterial in hcc [ 45 ]  . 
in the case of angiomas , however , the dc - mri examination failed to demonstrate the typical centripetal enhancement pattern after the bolus injection of gd - dtpa due to the hyperintensity of the signal typical of angiomas in t1 - weighted sequences after spio administration , which tends to mask the subsequent action of the paramagnetic contrast mediuin angiomas , spio remains in the extracellular space within the vascular sinusoids in a nonbonded forin this form , spio presents paramagnetic characteristics , with a hyperintense signal in t1 - weighted sequences known as t1 effect , characteristics that are typical of angiomas . 
this was , however , one of the first cases studied , and a more careful assessment of the images before and after contrast enhancement would have avoided the error . in our study there were no side effects or changes in biohumoural parameters after the administration of the contrast media . 
this time interval does not compromise the contrast features of spio in that its maximum liver concentration occurs within the fourth hour whereas its plasma half - life of about 10 min enables the delayed administration of gd - dtpa without pharmacological interaction of the two contrast media [ 42 , 46 ]  . 
in addition , the distribution and elimination of the two contrast media have completely different pathways , and pharmacological studies have demonstrated no interactions between the two contrast media in vitro [ 21 , 42 ]  . conclusions the combined sequential use of two - negative and positivecontrast media improves diagnostic confidence and in our study caused no side effects in patients . 
nonetheless , the technique can be useful to complete the spio - mr examination in cases of diagnostic uncertainty and in the presence of spioluda , increasing the diagnostic accuracy of the method . 1100 il differente tipo di vascolarizzazione che nei nd di tipo portale mentre negli hcc di tipo prevalentemente arterioso [ 45 ]  . 
nella nostra esperienza tutti gli hcc hanno presentato un enhancement vascolare arterioso tipico ed un wash - out in fase portale , mentre i nd non hanno presentato enhancement vascolare . 
negli angiomi invece , con la tecnica a doppio contrasto , non stato possibile dimostrare il comportamento vascolare tipico di enhancement centripeto dopo iniezione a bolo di gd - dtpa a causa delliperintensit di segnale tipico degli angiomi nelle sequenze pesate in t1 dopo iniezione di mdc spio che mascherava la successiva azione del mdc paramagnetico . 
in questa forma il mdc spio ha un comportamento paramagnetico , presenta un segnale iperintenso nelle sequenze pesate in t1 , denominato t1 effetto , e tale comportamento contrastografico tipico appunto degli angiomi . 
si trattava peraltro di uno dei primi casi studiati ed una pi attenta valutazione delle immagini prima e dopo contrasto avrebbe consentito di non incorrere in tale errore . nel nostro studio non si sono verificate reazioni secondarie o alterazioni dei parametri bio - umorali dopo somministrazione dei due mezzi di contrasto . 
tale distanza di tempo non pregiudica leffetto contrastografico del mdc spio , in quanto questultimo presenta la massima concentrazione epatica entro la 4a h , mentre la sua emivita plasmatica di circa 10 min consente la somministrazione ritardata di gd - dtpa senza interazione farmacologica dei due mdc [ 42 , 46 ]  . 
la distribuzione e leliminazione dei due mdc segue peraltro strade completamente diverse e studi farmacologici non hanno rilevato interazioni tra i due mdc in vitro [ 21 , 42 ]  . conclusioni lutilizzo sequenziale - combinato dei due mezzi di contrasto , negativi e positivi , consente una migliore confidenza diagnostica e nella nostra esperienza non ha determinato reazioni secondarie nei pazienti . 
carriero published online : 20 december 2006 ours is a life marked by fortune ; we have had the luck to be born in a country kissed by the sun and embraced by the sea , protected by the mountains and , above all , enriched with well - being . 
 its in this land whose very name italia suggests elegance , historical respect and reverence for ardent intelligence , an unusual coexistence in the imagination that we have our big family of more than 8 , 000 people united under the banner of sirm . 
 in todays world where alliances always have an archaic flavour or unbridled interests , in which the driving element is for ones own selfish means with the philosophy that theres no such thing as a free lunch , being united by a ray is a story of other times . 
if it were a ray of sunshine , there might be some justification , but that an invisible ray that doesnt heat or illuminate , and which is even hidden behind the unidentified x , can be the link for 8 , 000 people could be nothing short of a miracle . it was therefore spontaneous to ask to whose merit do we owe these 50 years of familiar militancy in the rm ? it brings to mind the words of my teacher , when trying desperately to make me grow up , who told me that when battles are lost , its always the fault of the generals and not the soldiers . from here we can use the opposite logic that the success of sirm is the result of the general presidents , members of the directive council and secretaries who conceptualised it , realized it and made the organisation grow in tune with the times . but wars arent won without soldiers , and in addition to the infinite recognition to our generals , its possible that the merit of this large organisation is due to the daily work of the 8 , 000 people of sirm . 
its a group of big - hearted professionals who , with ever - increasing difficulty , and in silence , support the radiology departments , which are , like it or not , the heart of the italian public and private health services . 
in this way , when one day my students at the school of specialisation in novara were in a discussional mood , something occurred to me like a bolt out of the blue our radiologists in sirm are , among other equally great things , a group of very generous people . 
in so doing , i was at the same time expanding my own personal efforts for humanitarian causes . it always happens that dreams are the first hope of man , also because dreaming doesnt cost anything and opens new horizons , allowing us to sail on a sea of optimism and to help those burnt by the aridness of daily life . 1170 la nostra una vita nel marchio della fortuna ; abbiamo avuto la fortuna di nascere in un paese baciato dal sole , accarezzato dal mare , protetto dalle montagne ma soprattutto ricco del suo benessere . ed in questo paese , che anche nel suo nome italia impone eleganza , rispetto storico , riverenza per le fervide intelligenze , nella coesistenza inusuale della fantasia , la nostra una grande famiglia di pi di 8000 persone unite nel segno della sirm . nel mondo doggi in cui le coalizioni hanno sempre il sapore dellarcaico o dellinteresse sfrenato , in cui lelemento conduttore il proprio torna conto nella filosofia che nulla debba essere fatto senza un immediato ritorno , sentirsi uniti da un raggio una storia daltri tempi . 
fosse un raggio di sole pur avrebbe una giustificazione ma che un raggio invisibile che non riscalda e non illumina e che addirittura nascosto dietro allignota x , fosse il filo dunione di 8000 persone non pu che essere un miracolo . stato spontaneo quindi domandarsi in questi cinquantanni di militanza familiare nella rm , di chi fosse il merito . 
allora vengono alla mente le frasi del mio maestro quando un giorno , nel tentativo disperato di farmi crescere , mi disse che quando si perdono le battaglie la colpa sempre dei generali e non dei soldati ; da qui la deduzione opposta che la realt sirm merito dei vari generali - presidenti membri del consiglio direttivo , segretari che lhanno pensata , voluta , realizzata , fatta crescere e proiettata al passo con i tempi . ma senza i soldati le guerre non si vincono e cos , oltre alla infinita riconoscenza ai nostri generali , forse il merito di questa grande societ sta anche nel lavoro quotidiano di 8000 radiologi : il popolo della sirm . 
un popolo di professionisti , dal cuore grande , che nel silenzio e in difficolt sempre maggiori regge i reparti di radiologia che sono , piaccia o no , il cuore della sanit pubblica e privata italiana . 
johns catholic school di watamu , kenya . between telephone calls , work dinners , congresses and days spent among scans and x - rays , this dream of coming together in the name of that unknown ray called x , to help whoever came knocking on our door , was born . so in that way , partly as a joke , and partly as a bet , the idea radiology for life was born . 
im not so sure yet what it will become , but i know that this group of people who are willing to support humanitarian efforts have been diffused all over italy , so much so that my e - mail inbox is full of mail every day from the people who have made sirm great , wanting to tell me of their availability . 
in 2006 , radiology for life adopted st . johns catholic school in the watamu area of kenya ; all of this resulted from a humanitarian trip to watamu that i had previously made . 
johns school was seriously incomplete and lacking in materials . two classrooms were missing ( 80 children were forced to have their lessons under a tree , even during the rainy season )  . 
it needed all the necessary furniture for the classrooms ( desks , blackboards , chairs etc . ) , all manner of sanitation was missing and it also needed an office , which could be used as a refectory when needed . 
i exchanged tra una telefonata e una cena di lavoro , tra un congresso ed una giornata tra risonanze tac e radiografie nato il sogno di mettersi insieme nel nome di quel raggio , incognita x , per aiutare chi bussa alla nostra porta . cos , un po per scherzo e un po per scommessa , nata a novara unidea , la radiologia per la vita : non so bene ancora cosa sia , so solo che la voce di questo gruppo che vuole essere di supporto ad iniziative umanitarie , si sparsa a macchia dolio nelle radiologie di tutta italia , tanto che la mia e - mail piena ogni giorno di disponibilit da parte di quel popolo radiologico che ha fatto grande la sirm . 
john era gravemente carente ed incompiuta : mancavano due classi ( 80 bambini erano costretti a far lezione sotto un albero anche durante il periodo delle piogge ) , mancavano quindi tutti gli arredi relativi alle classi ( banchi , lavagne , sedie , ecc . ) , mancavano tutti i servizi sanitari , mancava un office che potesse essere usato alloccorrenza come refettorio . 
the 400 little children probably wont ever ask themselves what these letters stand for and wont ever know what radiology for life is , but a little piece of the hearts of italian radiologists now beats in watamu . the man who doesnt dream is finished , and so id like to continue dreaming of the idea to build an entire school totally sustained by radiology for life , and who knows , maybe the unknown x can bring luck again . mio amico frate agapius , responsabile della scuola , bastato uno sguardo e cos dopo appena un anno la scuola cattolica di st . 
john ha tutto ci di cui necessitava ( classi , servizi igienici , refettorio ) e tutto grazie al grande cuore degli amici radiologi italiani . quello che mi preme per sottolineare che per realizzare tutto questo , su un budget complessivo necessario di 13000 euro , il presidente della sirm e tutto il consiglio direttivo ha deliberato di contribuire come societ alla costruzione della scuola donando una cifra sino a 5000 euro , ma ne sono bastati solo 3000 , al resto ci ha pensato il popolo della sirm . cos a fine dicembre sar a watamu ad inaugurare le nuove strutture della scuola di st . 
fortuna amirsys inc , salt lake city , utah ( 2005 ) isbn 1 - 4160 - 2333 - x ; isbn 0 - 8089 - 2324 - 2 ( international english edition ) published online : 20 december 2006 this volume is part of a series dedicated to diagnostic imaging in the various fields of radiology . 
it is made up of 1043 pages and 3000 illustrations some of which dealing with macroscopic and micro pathology specimens , often supplemented with beautiful explicative and very precise drawings . 
tali caratteri radiografici non sono correlati ad alcun tipo istologico particolare . parole chiave lesioni non palpabili linfonodi intra - mammari carcinoma della mammella introduction introduzione intramammary lymph nodes are the most common cause of nonpathological masses seen on conventional mammography , being detected in about 30% of breasts , mostly in the upper - outer quadrants [ 1 ]  . 
the typical mammographic features of intramammary lymph nodes ( size smaller than 15 mm , round or oval shape , regular margins , low density , association with a vascular branch and , frequently , a radiolucent centre ) have been clearly established [ 17 ] , and their detection does not warrant further diagnostic investigation i linfonodi intra - mammari costituiscono la causa pi frequente di formazione espansiva con significato non patologico riscontrata allesame mammografico convenzionale : sono infatti presenti in circa il 30% delle mammelle , prevalentemente nei quadranti supero - esterni [ 1 ]  . 
i caratteri mammografici tipici dei linfonodi intra - mammari ( dimensioni inferiori a 15 mm , morfologia rotondeggiante od ovalare , contorni regolari , bassa densit , associazione con una diramazione vascolare e frequente area centrale di maggiore radio - trasparenza ) sono chiaramente codificati da lungo tempo in letteratura [ 17 ] ed il 1078 e . 
however , in rare cases , breast cancers may exhibit mammographic features compatible with intramammary lymph nodes [ 1 , 2 , 9 , 11 ]  . the aim of this study was to verify the existence of mammographic criteria justifying a suspicion of atypical intramammary lymph node , assess whether certain histological types of breast cancer are more likely to display the radiographic features of intramammary lymph nodes , and consider the most appropriate diagnostic strategy in women with node - like mammographic findings . materials and methods we retrospectively reviewed the previous mammograms of women who received a diagnosis of breast cancer between january 1997 and december 2004 . 
the mammograms had been performed 6 months to 3 years before the diagnosis and depicted findings morphologically similar to intramammary lymph nodes at the site where the cancer was subsequently detected . 
the imaging equipment consisted of a dedicated conventional radiology unit ( mammomat 3000 , siemens , erlangen , germany ) combined with a high - spatialresolution detector , gadolinium screen ( kodak min r 2000 ) and single - coated film ( kodak m35 series x - omat processor )  . 
examinations performed with different equipment and techniques were excluded from the study . during the examination that aroused the suspicion of a neoplastic lesion , all lesions were studied by fine - needle cytology ( 2023 gauge ) under sonographic guidance ( seven cases ) or stereotactic guidance ( in one case in which the lesion was poorly visualised on ultrasound )  . 
all lesions subsequently underwent surgical excision and histological examination . loro riscontro non richiede approfondimenti diagnostici , che si rendono necessari solo in caso di incremento volumetrico in un controllo mammografico successivo [ 813 ]  . 
sebbene raramente , tumori della mammella in fase iniziale possono presentare caratteri mammografici sovrapponibili a quelli tipici dei linfonodi intra - mammari [ 1 , 2 , 9 , 11 ]  . scopo di questo lavoro ricercare se esistano criteri di semeiotica mammografica che consentano di porre il sospetto di linfonodo intra - mammario atipico , valutare se alcuni istotipi tumorali si manifestino preferenzialmente con caratteri radiografici simili a quelli dei linfonodi intra - mammari ed esaminare quale sia la strategia diagnostica pi opportuna quando si riscontrino reperti di aspetto compatibile con quello dei linfonodi intra - mammari . materiali e metodi sono stati retrospettivamente valutati i radiogrammi espletati in un periodo compreso tra i sei mesi e tre anni prima della diagnosi di tumore della mammella , posta tra gennaio 1997 e dicembre 2004 nei quali , nella sede in cui sarebbe stata in seguito identificata la neoplasia , era presente un reperto con i caratteri morfologici di un linfonodo intra - mammario . 
tutte le pazienti considerate hanno eseguito un esame mammografico standard , con almeno due proiezioni ( cranio - caudale e medio - laterale obliqua ) per mammella ; lindagine stata espletata con apparecchiatura radiologica convenzionale dedicata ( mammomat 3000 , siemens , erlangen , germania ) associata a detettore ad alta risoluzione spaziale , con schermo di rinforzo in gadolinio ( kodak min r 2000 ) e pellicola monoemulsionata ( kodak m35 series x - omat processor )  . 
le indagini espletate con modalit differenti da quella citata sono state escluse dallo studio . tutte le lesioni , nel corso dellindagine in cui ne stata sospettata la natura neoplastica , sono state sottoposte ad esame citologico con ago sottile ( calibro 2023 g ) , espletato sotto guida ecografica ( 7 casi ) o stereotassica ( nel singolo caso in cui la lesione non risultava chiaramente riconoscibile allesame ecografico )  . 
it is difficult to identify any lesion at all at the site of interest ( arrow and arrowhead ) on the mediolateral oblique mammogram ( a )  . only the craniocaudal view ( b ) shows an 8 - mm , faint , round opacity in the upper - outer quadrant that can be evaluated as an intramammary lymph node ( arrows )  . 
sul radiogramma in proiezione medio - laterale obliqua ( a ) risulta difficilmente identificabile , nel punto di interesse ( freccia e testa di freccia ) , una qualsiasi lesione . 
solo la proiezione cranio - caudale ( b ) dimostra nel versante supero - esterno tenue opacit rotondeggiante di 8 mm valutabile come linfonodo intra - mammario ( freccia )  . 
in the craniocaudal view ( b ) , an oval opacity with regular margins can be seen ( arrow ) projecting along a vascular branch , with a radiolucent central area ( 8 mm )  . 
in fase pre - diagnostica la proiezione medio - laterale obliqua ( a ) non consente di identificare lesioni sospette nellarea di interesse ( freccia e testa di freccia )  . 
in proiezione cranio - caudale ( b ) si identifica tenue opacit ovalare a contorni regolari ( freccia ) proiettatesi su diramazione vascolare , con nucleo radio - trasparente ( 8 mm )  . 
mediolateral oblique mammogram shows an 8 - mm , faint , round opacity in the upper quadrant ( arrow ) , with multilobular margins and radiolucent centre ( a ) interpreted as an intramammary lymph node . 
radiogramma in proiezione medio - laterale obliqua che dimostra nel versante superiore tenue opacit rotondeggiante di 8 mm ( freccia ) a contorni pluriciclici e nucleo radiotrasparente ( a ) interpretata come linfonodo intra - mammario . 
a minute ( 4 mm ) , round opacity with a radiolucent central area projecting along a small vascular branch can be seen in the upper - outer quadrant on both views ( arrows in a , b )  . 
minuta ( 4 mm ) opacit rotondeggiante con nucleo radiotrasparente , proiettantesi su piccola diramazione vascolare , riconoscibile nel versante supero - esterno in entrambe le proiezioni ( frecce in a , b )  . 
il controllo effettuato a distanza di 24 mesi ( c , d ) dimostra lieve incremento volumetrico ( 6 mm ) con densit lievemente aumentata . at baseline mammography , all masses showed round or oval shape and low density , with well - defined margins in seven cases ( two of which lobulated ) , and one case showed slightly indistinct margins . 
le dimensioni delle formazioni erano comprese fra 4 e 8 mm ( tabella 1 )  . lindagine in cui stata riconosciuta la reale natura neoplastica delle neoformazioni stata espletata da 6 a 36 mesi dopo la prima . 
a small ( 5 mm ) , faint , round opacity with radiolucent central area projecting along a vascular branch is seen in the upper - outer quadrant on the mediolateral oblique view ( arrow in a ) , which is even more evident on the craniocaudal view ( arrow in b )  . 
piccola ( 5 mm ) e tenue opacit rotondeggiante con nucleo radiotrasparente , proiettantesi sul decorso di diramazione vascolare nel versante supero - esterno , apprezzabile in proiezione medio - laterale obliqua ( freccia in a ) e meglio in proiezione cranio - caudale ( freccia in b )  . 
in the prediagnostic phase , the minute ( 6 mm ) , faint opacity visible in the upper - outer quadrants on both views ( arrows in a , b ) could easily be interpreted as an intramammary lymph node because of its site , density , radiolucent centre and proximity to vascular structures . 
in fase pre - diagnostica , la minuta ( 6 mm ) e tenue opacit apprezzabile in entrambe le proiezioni ( frecce in a , b ) nel versante supero - esterno facilmente interpretabile come linfonodo intramammario , in virt della sede , delle densit , del nucleo radiotrasparente e delle prossimit con le strutture vascolari . 
dopo 24 mesi ( c , d ) la lesione presenta contorni sfumati ; sensibilmente aumentata di volume ( 20 mm ) e di densit , questultima disomogenea . discussion discussione the radiographic features traditionally ascribed to intramammary lymph nodes [ 17 ] still hold good , as they are based on pathology findings and experience : the finding of small round or oval masses with regular margins and low density ( especially if located along a vascular branch and relatively radiolucent in their central portion ) does not justify a suspicion of neoplastic disease . 
a number of benign conditions can cause lymph nodal eni caratteri radiografici tradizionalmente attribuiti ai linfonodi intra - mammari [ 17 ] , in quanto fondati su dati anatomopatologici e condizionati dalla esperienza , rimangono validi a tuttoggi : il riscontro di formazioni espansive rotondeggianti od ovalari di piccole dimensioni , a margini regolari e dotate di bassa densit ( specie se situate lungo una diramazione vascolare e relativamente radio - trasparenti nella porzione centrale ) non autorizza a porre il sospetto di patologia neoplastica . 
the prediagnostic mediolateral oblique view shows , in the area in question ( arrow in a ) , an almost imperceptible , very small ( 4 mm ) and faint opacity , marked with an arrow on the craniocaudal view ( b )  . 
in fase pre - diagnostica , nella proiezione medio - laterale obliqua pressoch impercettibile nella zona di interesse ( freccia in a ) la minuta ( 4 mm ) e tenue opacit contrassegnata con freccia nella proiezione cranio - caudale ( b )  . 
a distanza di 36 mesi ( c , d ) la lesione risulta sensibilmente aumentata di volume ( 10 mm ) e densit , presentando contorni sfumati . largement and increased radiographic density , for example , inflammation of the breast skin ( at times related to implants ) or systemic inflammation ( rheumatoid arthritis )  . 
lymph nodal enlargement and increased density may also result from lymphoproliferative disease or from metastasis from cancers located in other parts of the breast , or rarely , elsewhere in the body ( melanomas , pulmonary , gastric and ovarian cancers ) [ 9 ]  . 
 inoltre causare nel tempo incremento nelle dimensioni e nella densit radiografica dei veri linfonodi intra - mammari , come avviene in caso di flogosi cutanee proprie della ghiandola mammaria ( anche sostenute dalla presenza di protesi ) o su base sistemica ( quali lartrite reumatoide ) ; analogo reperto pu essere causato da malattie infettive fra cui la tubercolosi . 
infine , possono ingrandirsi ed aumentare in densit i linfonodi intra - mammari sede di localizzazione di malattia linfoproliferativa o di metastasi , a partire da tumori primitivi posti in altre porzioni della mammella o , raramente , altrove ( melanomi ; tumori polmonari , gastrici ed ovarici ) [ 9 ]  . to our knowledge , the possibility that early primary secondo i dati a nostra disposizione , la possibilit che 1083 e . 
the retrospective review of our small case series did not reveal any correlation between histological type of cancer and node - like radiographic patterns , nor did it indicate the existence of new semiological criteria . 
it did , however , highlight a need for careful assessment of the known semiological criteria . owing to their small size , initial cancers with misleadingly similar features to intramammary lymph nodes may exhibit suspicious features in one radiographic view only . 
in addition , it should be noted that slight blurring of tumori primitivi della mammella esordiscano con quadri mammografici simili a quelli dei linfonodi intra - mammari non stata trattata in letteratura , sebbene sia noto che i carcinomi mucinosi possono presentare margini netti [ 7 ]  . la valutazione retrospettiva di questa casistica per quanto numericamente limitata non ha evidenziato correlazioni fra specifici istotipi tumorali e caratteri radiografici simil - linfonodali . 
non sono inoltre emersi criteri semeiologici nuovi ma la necessit di dedicare estrema attenzione a quelli gi noti . in conseguenza delle loro esigue dimensioni , lesioni tumorali in fase precoce e con caratteri ingannevolmente simili a quelli dei linfonodi intra - mammari possono mostrare segni sospetti in una sola proiezione radiografica . 
the main cause of acute chest pain , which accounts for 6.5% of urgent medical examinations in emergency rooms in italy , is acute coronary syndrome ( acs )  . 
we performed this prospective study to evaluate the diagnostic accuracy of a 16 - channel computed tomography ( ct ) scanner with dedicated software in a group of patients with chest pain and medium to low risk of acs materials and methods . 
this study involved a selected group of 31 patients reporting chest pain with a medium to low probability of acs , defined on the basis of preliminary tests [ electrocardiogram ( ecg ) and serum cardiac markers ]  . 
msct identified the presence of occlusions and significant ( > 50% ) or nonsignificant stenoses in the main coronary segments , with a sensitivity of 65% , a specificity of 98.8% , a positive predictive value ( ppv ) of 81.2% , a negative predictive value ( npv ) of 97.3% and an accuracy of 96.4%. 
in patients with a medium to low coronary risk , msct is a more accurate indicator of the need for coronary angiography than is exercise stress testing , which is less expensive but has lower predictive values . key words coronary arteries coronarography ct angiography multislice ct riassunto obiettivo . 
causa predominante del dolore toracico acuto , che motiva il 6 , 5% delle visite mediche urgenti effettuate nei pronto soccorso italiani , la sindrome coronarica acuta ( sca )  . 
lo studio analizza laccuratezza diagnostica della tc multistrato ( tc - ms ) a 16 canali in un gruppo selezionato di 31 pazienti con dolore toracico a medio - bassa probabilit di sca , cos definiti in base agli accertamenti preliminari ( elettrocardiogramma e markers biochimici )  . 
utilizzando come gold standard la coronarografia , eseguita nelle 24 ore successive allesame tomodensitometrico , la tc - ms ha identificato nei segmenti coronarici principali la presenza di occlusioni , stenosi significative ( > 50% ) e non ( < 50% ) con sensibilit : 65% ; specificit : 98 , 8% , vpp : 81 , 2% ; vpn : 97 , 3% , accuratezza : 96 , 4% . 
le stenosi significative e le occlusioni sono state invece accertate con sensibilit : 71 , 4% ; specificit : 99 , 6% ; vpp : 93 , 7% ; vpn : 97 , 7% ; accuratezza : 97 , 5% . 
the predominant cause is acute coronary syndrome ( acs ) , the management of which has le visite per dolore toracico acuto rappresentano circa il 6 , 5% di tutte le prestazioni effettuate nei pronto soccorso ( ps ) italiani cos come nelle emergency room statunitensi ; tale percentuale in costante aumento : nel 2000 si attestava al 5 , 1% . 
it has been calculated that in the united states 1 , 200 , 000 coronary angiography examinations are performed each year , 35% of which are followed by a revascularisation procedure . 
even though the morbidity and mortality rates of coronary catheterisation are very low ( 1% and 0.1% , respectively ) , there is a keen interest in alternative , less invasive and less expensive procedures possessing the same diagnostic accuracy in detecting or ruling out acute myocardial infarction ( ami ) and unstable angina . electrocardiogram ( ecg ) , serum cardiac markers and echocardiography can identify subjects with ami , for whom immediate reperfusion is indicated , and those with unstable angina . 
a proportion of patients presenting with chest pain are , however , considered at medium to low risk due to the absence of ischaemic st - segment abnormalities and negative serum markers , and these patients require additional investigations , such as exercise testing [ 1 ]  . 
because the advent of multidetector technology has considerably expanded the diagnostic potential of computed tomography ( ct ) , we performed this prospective study to evaluate the diagnostic accuracy of a 16 - channel ct scanner with dedicated software in a group of patients with chest pain and medium to low risk of acs . materials and methods between november 2004 and october 2005 , we recruited 31 subjects ( 19 men , 12 women ; mean age 59 years , age range 2670 years ) who presented to the emergency department with chest pain that was defined as medium to low probability of acs on the basis of first - line investigations ( ecg , and ischaemia markers : troponin , creatine phosphokinase and myoglobin ) but for whom a clinical suspicion of myocardial ischaemia persisted . 
subjects who had undergone previous myocardial revascularisation procedures or coronary angioplasty , with or without stent placement , were excluded . within 24 h of presentation , all patients ( who had given their informed consent for inclusion ) were studied by multislice ct ( msct ) and coronary angiography . 
further exclusion criteria for the ct study were heart rate > 70 bpm ( even after heart - rate - lowering drugs ) ; arrhythmia ; severe cardiac insufficiency ; pacemaker , defibrillators or valve implants ; history of adverse reactions to contrast material ; renal or respiratory insufficiency ; and pregnancy . the risk factors of the 31 patients selected for the study were hypertension ( 17 ) , cigarette smoking ( 6 ) , dyslipidaemia ( 6 ) , family history of ami ( 4 ) and diabetes ( 2 )  . 
all patients with heart rate higher than 65 bpm were treated with a heartrate - lowering agent ( metoprolol 100 mg / day ) whereas those with borderline heart rates around or just above 65 bpm received a - blocker ( metoprolol tartrate 5 mg ) intravenously 15 min before the examination . the ct study was performed with a 16 - channel multidetector scanner ( sensation cardiac , siemens ) using the following parameters : collimation 0.75 mm , voltage 120 kvp , rotation time 375 ms , slice thickness 0.75 mcardiac acacuta ( sca ) , nei cui confronti da una gestione attendista si passati ad una strategia aggressiva che prevede limmediata esecuzione di unindagine coronarografica e di uneventuale angioplastica . 
ancorch il cateterismo coronarico comporti una morbilit ed una mortalit assai ridotte ( rispettivamente nellordine dell1% e dello 0 , 1% ) permane alto linteresse per procedure alternative che assicurino non - invasivit e riduzione dei costi economici , identificando o escludendo con equivalente accuratezza diagnostica linfarto miocardico acuto ( ima ) e langina instabile . elettrocardiogramma , markers biochimici , ecocardiogramma consentono di individuare sia i soggetti con ima , nei quali generalmente indicata una terapia immediata di riperfusione , sia quelli con angina instabile . 
esiste , tuttavia , una quota di pazienti con dolore toracico definiti a mediobasso rischio , per lassenza di alterazioni ischemiche del tratto st dellelettrocardiogramma e la negativit dei markers biochimici , nei quali si rende necessaria lesecuzione di altre indagini , che attualmente consistono in test da stress [ 1 ]  . 
poich lintroduzione della tecnologia multidetettore ha comportato un incremento notevole delle potenzialit diagnostiche della tc , ci siamo proposti , in questo studio prospettico , di valutare laccuratezza diagnostica di una apparecchiatura a 16 canali e software dedicato in un gruppo di pazienti con dolore toracico a medio - basso rischio di sca . materiali e metodi nel periodo compreso tra novembre 2004 e ottobre 2005 , sono stati reclutati 31 soggetti ( 19 maschi , 12 femmine ; et media 59 anni con range : 2670 anni ) pervenuti allosservazione in ps per dolore toracico definito a medio - bassa probabilit di sca in base alle indagini di prima istanza ( tracciato elettrocardiografico e markers di ischemia : troponina , creatinfosfochinasi e mioglobina ) ma nei quali persisteva il sospetto clinico di ischemia miocardia . 
nellarco di 24 ore dalla presentazione in ps , tutti i pazienti ( dai quali era stato ottenuto il preventivo consenso informato per linserimento nel presente studio ) sono stati sottoposti a esame tc multidetettore ( tc - md ) e coronarografia . 
ai fini dellindagine tomodensitometrica altri criteri di esclusione sono stati : frequenza cardiaca ( fc ) > 70 bpm ( anche dopo bradicardizzazione farmacologia ) ; aritmia ; insufficienza cardiaca grave ; presenza di pacemaker , defibrillatori o protesi valvolari ; pregresse reazioni avverse al mezzo di contrasto ; insufficienza renale o respiratoria ; stato di gravidanza . nel gruppo selezionato di 31 soggetti i fattori di rischio 1055 l . 
coronary angiography images were obtained with volume rendering ( vr ) and curvilinear multiplanar reconstruction ( mpr ) three - dimensional ( 3d ) techniques . in the comparison between msct and coronary angiography , the latter being considered the gold standard , we evaluated 16 coronary segments according to the american heart association classification [ 3 ]  . 
two operators , one radiologist and one cardiologist , independently evaluated each segment for assessability and image quality ( excellent , fair and poor ) and the presence of occlusions and stenoses , which they ranked as nonsignificant ( 50% ) or significant ( 51%99% ) based on a subjective visual judgement for msct and a quantitative judgement for coronary angiography [ 4 ]  . results at msct , 383 ( 81.7% ) of the 469 segments visualised by coronary angiography were considered assessable ; the intermediate branch was present in four subjects only ( table 1 )  . if only the main segments were considered right coronary erano ipertensione ( 17 ) , fumo di sigaretta ( 6 ) , dislipidemia ( 6 ) , familiarit per ima ( 4 ) e diabete ( 2 )  . 
per coloro invece che presentavano una frequenza borderline e cio intorno o di poco superiore ai 65 bpm si optato per la somministrazione endovena di un - bloccante ( metoprololo tartrato 5 mg ) 15 minuti prima dellesecuzione dellesame . lindagine tc stata effettuata con una apparecchiatura multidetettore a 16 canali ( sensation cardiac , siemens ) , utilizzando i seguenti parametri : collimazione 0 , 75 mm , voltaggio 120 kvp , tempo di rotazione 375 ms , spessore di strato 0 , 75 mlattivit cardiaca stata costantemente monitorata durante lindagine mediante tracciato elettrocardiografico in singola derivazione . per liniezione di mezzo di contrasto ( mdc ) organo - iodato non ionico ( concentrazione 350400 mgi / ml ) si utilizzato un iniettore automatico collegato ad unagocannula da 1820 gauge inserita in una vena antecubitale del braccio . utilizzando la tecnica del bolus tracking con roi nellaorta ascendente sono stati iniettati 100 ml di mdc , seguiti da 40 ml di soluzione fisiologica , ad una velocit di infusione di 4 ml / s . la ricostruzione delle immagini stata effettuata mediante gating cardiaco retrospettivo , individuando la finestra temporale ottimale per ogni ramo coronarico ( solitamente 400 , 350 o 300 ms prima del successivo complesso qrs elettrocardiografico ) [ 2 ]  . 
sono state ricostruite sezioni assiali dello spessore effettivo di 0 , 75 mm con overlapping di 0 , 5 mle immagini coronarografiche sono state ottenute con tecnica 3d volume rendering ( vrt ) e multiplanare ( mpr ) curvilinea . ai fini del confronto tra tcmd e coronarografia , assunta quale gold standard , sono stati considerati 16 segmenti coronarici secondo la classificazione dellamerican table 1 number and percentage of coronary artery segments considered assessable on computed tomography ( ct ) in 31 patients tabella 1 numero e percentuale dei segmenti coronarici giudicati valutabili alla tc in 31 pazienti segments assessable , n ( % ) segmenti variabili , n ( % ) 1 . 
di ogni segmento due operatori , un radiologo e un cardiologo , hanno considerato in maniera indipendente la valutabilit e la qualit iconografica ( eccellente , discreta e scadente ) nonch la presenza di occlusioni o di stenosi classificate in non significative ( 50% ) e significative ( 51%99% ) in base ad un giudizio visuale soggettivo per la tc - md e quantitativo per la coronarografia [ 4 ]  . risultati alla tc - md sono stati giudicati valutabili 383 ( 81 , 7% ) dei 469 segmenti visualizzati alla coronarografia , essendo il ramo intermedio presente solo in 4 soggetti ( tabella 1 )  . 
considerando esclusivamente i segmenti principali e cio arteria coronaria destra ( segmenti 1 , 2 , 3 ) , tronco comune ( segmento 5 ) , arteria discendente anteriore ( segmenti 6 , 7 , 8 ) , arteria circonflessa ( segmenti 11 , 13 ) e , laddove presente , ramo intermedio ( segmento 16 ) , i segmenti considerati valutabili sono stati 277 di 283 ( 97 , 9% ) : in 4 / 31 ( 12 , 9% ) pazienti si avuto un segmento non valutabile , pi frequentemente il 13 ; in 1 paziente ( 3% ) i segmenti non esaminabili sono stati due . 
la tabella 3 mostra i risultati del confronto tc - coronarografia limitatatotal total tc , n positiva negativa totale , n tc , n positive negative totale , n fig . 
1a - c a 40 - year - old man , a heavy smoker with a family history of coronary disease , admitted to the emergency room with precordial chest pain ; sinusal rhythm with 60 bpm at electrocardiogram ( ecg ) , myocardial ischaemia markers negative , no regional wall motion abnormalities at echocardiography . 
computed tomography ( ct ) ( a , b ) shows about 50% tubular stenosis with focal , severe narrowing of the lumen of the anterior descending artery ( ada ) , segment 1 ( arrowheads )  . 
alla coronaro - tc ( a , b ) : stenosi tubulare di circa il 50% , cui segue focale serrato restringimento del lume dellarteria discendente anteriore ( ada ) prossimale , segmento 1 ( punta di freccia )  . 
2a - c a 70 - year - old woman with hypertension admitted to the emergency room with precordial chest pain radiating to the neck ; sinusal rhythm with 63 bpm and minimal st depression at electrocardiogram ( ecg ) , absence of serum cardiac markers , normal ventricular wall motion at echocardiography . 
paziente maschio , et 56 anni , diabete mellito nid , iperteso , con scintigrafia miocardica da sforzo ( eseguita 3 mesi prima ) dubbia per coronaropatia ; pervenuto in ps con dolore toracico retrosternale . 
4a , b a 70 - year - old man with hypertension and hypercholesterolaemia admitted to the emergency room with precordial chest pain ; sinusal rhythm with 58 bpm , absence of ischaemic signs at electrocardiogram ( ecg ) ; absence of serum cardiac markers . 
computed tomography ( ct ) ( a ) shows eccentric calcific plaque of the middle circumflex artery ( segment 13 ) ( arrow )  . the vessel lumen is not well assessable , but a > 50% stenosis ( arrow ) is suggested . 
alla tc ( a ) : placca eccentrica calcifica dellarteria circonflessa , tratto medio , segmento 13 ( freccia ) ; il lume non ben valutabile ma si ipotizza una stenosi > 50% . 
alla coronarografia ( b ) : stenosi della lunghezza di circa 15 mm e del 90% circa nel punto critico ( freccia )  . particular , it reports the number of subjects with at least one occlusion or stenosis > 50% identified by ct with respect to the number of those identified by coronary angiography . 
inoltre , la coronarografia documenta come in 3 di 6 segmenti ( 50% ) vi sia una riopacizzazione da circolo collaterale del tratto distale alla stenosi . la tabella 5 presenta , infine , unanalisi della casistica che considera il singolo paziente piuttosto che i segmenti coronarici ; in particolare , riporta il numero dei soggetti con almeno una occlusione o una stenosi > 50% identificati alla tc rispetto a quanti individuati dalla coronarografia . 
nei pazienti ( 16 / 31 ) , nei quali la qualit dimmagine risultata eccellente per tutti i segmenti , i valori di sensibilit , specificit , valore predittivo positivo e negativo , accuratezza sono pari al 100% . discussione lesame dei pazienti che si presentano in ps per dolore toracico acuto richiede tempo e risorse economiche finalizzati allaccertamento di una sca che risulta , al termine di tutte le indagini , inesistente in una percentuale tuttaltro che trascurabile di casi . 
la valutazione clinica ( intensit , irradiazione , durata ) del dolore toracico , daltra parte , facilmente soggetta ad errori interpretativi e insufficiente per la diagnosi ; ne consegue che lapproccio tradizionale a tali pazienti preveda lelettrocardiogramma e il dosaggio dei markers biochimici . 
lalterazione di questi ultimi unitamente allelevazione elettrocardiografica del tratto st corrobora il sospetto clinico di infarto miocardico , che comunque diagnosticabile anche in assenza di precoci alterazioni elettrocardiografiche qualora vi sia innalzamento di troponina , creatinfosfochinasi e mioglobina . 
quando anche tali markers siano negativi , i pazienti definiti a medio - basso rischio di sca debbono essere avviati a test da stress elettrocardiografici , ecocardiografici o scintigrafici per evidenziare la presenza o lassenza di malattia coronarica significativa [ 5 , 6 ]  . 
5a - c a 58 - year - old woman with hypertension and a previous history of smoking admitted to the emergency room with precordial chest pain and dyspnoea ; absence of ischemic alterations at electrocardiogram ( ecg ) , absence of serum cardiac markers . 
although poor quality of computed tomography ( ct ) image ( a ) should have induced the reader to avoid any judgement , a severe stenosis ( arrow ) of the right coronary artery ( segment 2 ) is suggested . 
si ipotizza comunque lesistenza di una stenosi critica da placca calcifica del segmento 2 , sottovalutando erroneamente lipotesi di una occlusione con riopacizzazione a valle da parte dellemisistema coronarico sinistro , come invece dimostrato dalla coronarografia ( punte di freccia ) ( b , c )  . partment with acute chest pain in order to identify an acs that very often turns out to be nonexistent . 
the clinical assessment ( intensity , radiation , duration ) of chest pain is , on the other hand , often prone to misinterpretation and is inadequate for the diagnosis , with the result that the conventional approach to these patients includes an ecg and serum cardiac markers . abnormal serum cardiac markers associated with st elevation supports the clinical suspicion of myocardial infarction , which can , however , be diagnosed even without early electrocardiographic alterations if the troponin , creatine phosphokinase and myoglobin levels are high . 
where these markers are negative , patients considered at medium to low risk of acs must proceed to electrocardiographic , echocardiographic or nuclear stress testing to determine the presence or absence of significant coronary disease [ 5 , 6 ]  . 
the diagnostic reference standard for the assessment of vascular anatomy and the detection of stenosing lesions is coronary angiography , which , in addition to a diagnostic phase , allows immediate myocardial reperfusion by means of angioplasty . 
the invasiveness and high cost of this examination have , however , promoted research into alternative , noninvasive diagnostic techniques . the technological evolution of spiral ct has made available multislice scanners with 4 , 8 , 16 and , recently , 64 detector rows that offer a temporal and spatial resolution that enable analysis of the coronary arteries with a high level of anatomical detail . 
linvasivit e lelevato costo di tale indagine hanno indirizzato tuttavia gli sforzi della ricerca verso tecniche diagnostiche alternative non invasive . levoluzione tecnologica della tc spirale ha reso disponibili apparecchiature multistrato a 4 , 8 , 16 e , recentemente , 64 file di detettori caratterizzate da risoluzione spaziale e temporale tali da consentire lanalisi delle coronarie con elevato dettaglio anatomico . 
in letteratura , dallanno 2000 ad oggi , sono stati pubblicati diversi studi sullidentificazione di placche coronariche mediante tc - md a 4 o 16 canali [ 711 ]  . 
nella quasi totalit dei lavori sono state prese in considerazione le stenosi che comportano riduzione > 50% o occlusione del lume coronarico ; attualmente , con lutilizzo di scanner a 64 slice , si iniziano a valutare anche stenosi < 50% [ 1214 ]  . 
peraltro , in questa classe di pazienti che presentano angina instabile , due o pi fattori di rischio , incremento della troponina sierica , slivellamento st > 1 mm , aritmie o instabilit emodinamica , le pi recenti linee - guida cardiologiche suggeriscono lesecuzione in prima istanza dellangiografia coronarica e della rivascolarizzazione , se indicata [ 16 , 17 ]  . la presente casistica considera esclusivamente soggetti giunti allosservazione in ps con un dolore toracico acuto 1061 l . 
in this class of patients with unstable angina , two or more risk factors , increased serum troponin , st deviation > 1 mm , arrhythmias or haemodynamic instability , the most recent cardiological guidelines recommend coronary angiography and revascularisation , if indicated , as the first - line approach [ 16 , 17 ]  . our study included only subjects presenting to the emergency department for acute chest pain and at medium to low risk for acs associated with one , two or more risk factors for coronary disease ( age , smoking , dyslipidaemia , arterial hypertension , diabetes mellitus ) but with ischaemia markers and ecg not indicative of q and non - q ami . 
in the 31 patients enrolled , all of the 15 ( or 16 if the intermediate branch was present ) segments were analysed ; subsequently , the main coronary branches only were considered , that is , the right coronary artery ( segments 1 , 2 , 3 ) , left main branch ( segment 5 ) , anterior descending or interventricular artery ( segments 6 , 7 , 8 ) , circumflex artery ( segments 11 and 13 ) and , where present , the intermediate branch ( segment 16 )  . 
 compared with the interesting statistical results of previous reports , the sensitivity of msct ( 71.4% for occlusions and stenoses > 50% ) identified in our study is among the lowest reported in the literature [ 18 , 19 , 2125 ] and higher only than the value reported by hoffmann et al . 
the false negatives are due to underestimation of the degree of stenosis in poor - quality images or to misinterpretation in cases of revascularisation of the branch below the stenosis due to collateral circulation ; in particular , the latter situation led to three stenoses being interpreted as significant rather than as occlusions . 
msct therefore takes on an important role in the diagnostic workup of this class of cardiological patients , as it guides towards coronary angiography more accurately than does exercise stress testing which , though definitely less expensive , has decidedly lower predictive values [ 2628 ]  . 
si sono esclusi i pazienti portatori di bypass aorto - coronarico o pace - maker e i soggetti sottoposti in passato ad interventi di angioplastica , con o senza posizionamento di stents coronarici . 
nei 31 pazienti arruolati , sono stati analizzati tutti i 15 ( o 16 in presenza di ramo intermedio ) segmenti ; successivamente sono stati presi in considerazione solo i rami coronarici principali , ovverosia arteria coronaria destra ( segmenti 1 , 2 , 3 ) , tronco comune ( segmento 5 ) , arteria discendente anteriore o interventricolare ( segmenti 6 , 7 , 8 ) , arteria circonflessa ( segmenti 11 e 13 ) e , qualora presente , il tronco intermedio ( segmento 16 )  . 
il dato in linea con quanto emerge da altri studi effettuati con tc - md a 12 e 16 canali [ 1820 ]  . rispetto a precedenti interessanti risultati statistici , nel presente studio emerge una sensibilit della tc - md ( 71 , 4% per le occlusioni e le stenosi > 50% ) che si posiziona ai limiti inferiori del range dei valori riportati in letteratura [ 18 , 19 , 2125 ] , risultando superiore soltanto a quella ( 63% ) di hoffmann et al . 
essi sono dovuti a sottostima dellentit della stenosi in immagini di qualit scadente o ancora ad errore interpretativo in casi di riabitazione del ramo a valle della stenosi per fenomeni di collateralit : in particolare , questultima evenienza responsabile di tre stenosi interpretate come significative e non , in realt , come occlusioni . 
per quanto concerne invece la specificit per le occlusioni e le stenosi > 50% , il nostro dato ( 99 , 6% ) appare incoraggiante essendo il range delle percentuali fino ad oggi riportate oscillante fra l86% ed il 98% . i valori predittivi negativo ( 97 , 7% ) e positivo ( 93 , 7% ) , superiori a quanto mediamente riportato in letteratura [ 18 , 19 , 2125 ] , implicano che un paziente , pervenuto in ps per dolore toracico con media - bassa probabilit di sca e tc - md negativa per stenosi significativa , abbia solo il 2 , 3% di probabilit di avere in realt una coronaropatia significativa ; allopposto , un soggetto con stenosi giudicata emodinamicamente significativa alla tc ha una probabilit superiore al 93% di conferma coronarografica . 
in questa classe cardiologica di pazienti la tc - md assume quindi un ruolo rilevante nellalgoritmo diagnostico indirizzando verso un approfondimento coronarografico pi correttamente di quanto non possa un test da sforzo , sicuramente meno costoso , ma caratterizzato da valori predittivi decisamente inferiori [ 2628 ]  . 
inoltre se , meno dettagliatamente ma in maniera clinicamente pi congrua , non si considerino i rami coronarici principali bens i singoli pazienti si ottiene una predittivit positiva del 100% . 
the encouraging results , if validated by larger series , support the use of pet / ct in patients with carcinoma of unknown primary origin and negative conventional imaging results . key words metastatic cancer occult primary cancer 18f - fdgpet / ct riassunto obiettivo . 
la popolazione in studio costituita da 38 pazienti consecutivi con malattia tumorale metastatica provata istologicamente in cui le tecniche di diagnostica per immagini convenzionale erano risultate negative o non conclusive nella identificazione della lesione primitiva . 
the site of the occult primary tumour often remains unidentified after common imaging investigations ( chest x - ray , abdominal and pelvic ct , mammography in women ) ( 20%27% of cases ) [ 1 , 2 ] or autopsy ( 30%82% ) [ 24 ]  . 
reasons for the low rate of detection of the primary cancer include a lesion size smaller than the spatial and contrast resolution of the technique used or involution of the primary mass due to limited angiogenic competence [ 5 ]  . 
conventional contrast studies of the upper and lower digestive tract , for example , have a low diagnostic yield , and mammography , although routinely ordered , is often unhelpful because very few patients with cup have a primary mass in the breast [ 6 ]  . recent papers have reported that the median survival for patients with cup is approximately 12 months and that detection of the primary tumour and initiation of therapy can prolong survival to 23 months [ 7 ]  . 
the aim of this study was to assess the role of 18f - fdg - pet / ct in the identification of occult primary tumours . materials and methods the patient population consisted of 38 consecutive patients ( 22 men , 16 women ; mean age 5911 years , range 4177 years )  . 
the uptake period was 6090 meach patient then underwent a pet / ct scan with a dedicated hybrid scanner ( discovery ls , general electric ; biograph sensation 16 , siemens ) and whole - body scans ; attenuation correction was la sindrome del tumore primitivo occulto ( cup ) consiste nella presenza di una malattia tumorale metastatica per la quale sia impossibile identificare la sede primitiva della neoplasia dopo una attenta indagine anamnestica , esame obbiettivo negativo , negativi gli esami clinico - diagnostici ( emocromo completo , funzionalit renale , epatica , pancreatica , test delle urine , radiogramma del torace , tc addominale e pelvica e mammografia nelle donne , psa negli uomini ) [ 1 ]  . 
nella maggior parte dei casi , impossibile identificare la sede del tumore primitivo occulto con altri esami ( 20%27% ) di diagnostica per immagini pi diffusi ( radiografia del torace , tc addominale e pelvica , mammografia nelle donne ) [ 1 , 2 ] o allautopsia ( 30%82% ) [ 24 ]  . le motivazioni alla base dello scarso potere di identificazione della sede del tumore primitivo comprendono le dimensioni al di sotto del potere di risoluzione , sia spaziale che di contrasto , delle tecniche utilizzate o linvoluzione della massa primitiva a causa di uno scarso potere angiogenetico [ 5 ]  . 
la mammografia , nonostante sia utilizzata nella routine diagnostica , spesso non utile in quanto un limitato numero di pazienti con cup hanno una massa primitiva a livello mammario [ 6 ]  . recenti lavori riportano come la sopravvivenza mediana dei soggetti con cup sia attorno ai 12 mesi e che la identificazione della sede primitiva di malattia con la possibilit di intraprendere un iter terapeutico sposti la sopravvivenza mediana a 23 mesi [ 7 ]  . 
successivamente ogni soggetto stato sottoposto a scansione pet - tc con tomotabella 1 dati clinici , istopatologici e di diagnostica per immagini dei casi con tumore primitivo a livello toracico caso n sesso et , anni biopsia pet / tc tumore occulto dopo pet / tc dimensioni lesione , mm brain metastasis adenocarcinoma supraclavicular node metastasis mediastinal and neck node metastasis adenocarcinoma adenocarcinoma supraclavicular node metastasis sacral vertebra metastasis melanoma adenocarcinoma left humerus metastasis squamous cell carcinoma area of increased uptake in left lung area of increased positive mediastinal and neck nodes , area in right lung positive neck nodes , area of uptake on chest skin multiple areas of uptake in bone and left lung multiple metastases to bone , right adrenal gland , right lung lymph nodes , lung left lung left lung right lung melanoma left lung right lung lung lung laterocervical node spinous cell metastasis brain metastasis carcinoma epithelial carcinoma bone , lung diangostica convenzionale metastasi cerebrale metastasi linfonodo sovraclaveare metastasi linfonodali ( mediastinici e cervicali ) metastasi linfonodo sovraclaveare metastasi ossea vertebra sacrale adenocarcinoma adenocarcinoma adenocarcinoma area di aumentato uptake polmonare sx area di aumentato uptake polmonare sx linfonodi mesiatinici e cervicali , area polmone dx polmone sx polmone sx polmone dx melanoma linfonodi cervicali , area cute torso melanoma adenocarcinoma metastasi omero carcinoma squamocellulare metastasi linfonodali laterocervicali metastasi cerebrale carcinoma spinocellulare carcinoma epiteliale multiple aree captanti a livello osseo e polmonare sx multiple meta . 
the low rate of detection of the primary tumour site has two main causes . first , the size of the primary lesion may be smaller than the resolution power of conventional imaging procedures ( such as ct or gastrointestinal contrast studies ) , or the lesions may be located in sites such as the abdomen , pelvis , head and neck . 
epatiche , area positiva gastrica negativa carcinoma a cellule transizionali adenocarcinoma carcinoma a cellule fusate carcinoma squamocellulare carcinoma squamocellulare negativa linfonodi adiacenti mammella sx area mediastinica ignoto linfonodi cervicali dx ignoto ignoto ignoto ignoto ignoto ignoto carcinoma epiteliale linfonodo ascellare sx ignoto carcinoma epiteliale linfonodo pelvico ignoto adenocarcinoma surrene dx , linfonodi ignoto adenocarcinoma adenocarcinoma mucoide adenocarcinoma mucoide carcinoma epiteliale mano sx area mediastinica ed ossea cute ignoto ignoto cute peritoneo fegato ignoto carcinoma epiteliale cute carcinoma indifferenziato linfonodo mediastinico ignoto ignoto ignoto na , non applicabile suggested that the primary tumour may disappear after having given rise to metastasis because of its angiogenic incompetence , which leads to marked apoptosis and cell turnover [ 5 ]  . whereas no diagnostic procedures can identify a primary lesion that has disappeared due to marked apoptosis , it has been demonstrated that fdg - pet can improve primary - site detection in patients with cup and a negative diagnostic workup . 
although the number of patients in our study was small , our preliminary results show that pet / ct is more sensitive than pet alone , with a 53% detection rate for occult cancers missed by other techniques discussione la cup una sindrome caratterizzata da una prognosi infausta . 
la identificazione della sede primitiva di neoplasia , comunque , pu essere importante in quanto permette di impostare una terapia specifica , migliorando significativamente la prognosi ( 1 anno vs 2 anni ) [ 7 ]  . 
le dimensioni delle lesioni primitive possono essere inferiori al potere di risoluzione delle procedure diagnostiche ( tc o studi contrastografici del tratto gastrointestinale ) o trovarsi in sedi quali laddome , la pelvi , la testa - collo . 
la pet - tc ( sezioni transassiali della pet , tc e immagine di fusione pet - tc ) ha evidenziato unarea di patologico accumulo a livello dellipofaringe ( indicata da freccia nella immagine mip )  . nari di piccole dimensioni [ 1 ]  . 
laltro motivo dipende dalle caratteristiche biologiche del tumore primitivo : stato ipotizzato che la massa tumorale primitiva possa scomparire dopo aver dato luogo a metastatizzazione a causa di uno scarso potere angiogenetico che porta a marcata apoptosi e turn over cellulare [ 5 ]  . mentre nessuna procedura diagnostica pu identificare una lesione primitiva che scomparsa per marcata apoptosi , stato dimostrato come la pet con fdg possa migliorare la identificazione della sede primitiva della lesione in pazienti con cup e una flow - chart diagnostica peraltro negativa . 
al momento presente , sono pochi gli studi che hanno valutato il valore aggiunto della pet - tc rispetto alla fdgpet convenzionale per lidentificazione della sede del tumore occulto [ 810 ]  . 
i nostri risultati preliminari , nonostante il campione sia limitato , mostrano che la pet - tc pi sensibile della pet convenzionale , rilevando il 53% dei tumori occulti che non erano stati evidenziati con le altre tecniche [ 1113 ]  . 
le limitate informazioni morfologiche fornite dalla pet da sola , rendono necessaria lintegrazione con i dati anatomici forniti dalla tc per migliorare la definizione anatomica delle aree di aumentata captazione del tracciante . 
the limited morphological information provided by pet alone requires integration with the anatomical data supplied by ct in order to improve the anatomical definition of the areas of increased tracer uptake . 
pet / ct scanners capture anatomical and functional data in a single registration [ 14 ] , overcoming the limitations of patient repositioning and time interval between scans when the images are fused a posteriori [ 15 ]  . 
the primary tumour was identified in 7 / 29 cases ( two carcinomas of the nasopharynx , one plasmocytoma of the tongue base , one lung carcinoma , two breast cancers ) , showing 24% sensitivity . 
this result is not , however , comparable with our findings because alberini included 22 patients with another positive conventional test : this means that pet provided additional information in 4 / 44 cases only . 
although the population was not selected ( in contrast to our study population ) , the sensitivity of pet was 37.8% , which is significantly lower than that reported in our study . although the heterogeneity of patients could be seen as a potential limitation to our study , with patients referred from different centres and affected by different types of tumours , this fact does not undermine the value of our study , as the diagnostic - therapeutic approach to unknown primary tumours has not yet been codified by international guidelines . 
the head and neck , abdomen and pelvis are highly complex anatomical districts and are characterised by areas of physiological tracer uptake ( for example , by the tonsils , lymphatic tissue , stomach , bowel and ureters )  . small areas of increased uptake due to a small primary tumour may be mistaken for areas of physiological uptake . the careful comparison of metabolic and anatomical information , made possible by pet / ct , considerably improves the sensitivity of the procedure , allowing visualisation of even small areas of asymmetrical tracer distribution or areas of increased focal uptake that would otherwise be considered physiological . 1154 dallintervallo di tempo tra gli scans quando le immagini sono fuse a posteriori [ 15 ]  . 
la sede del tumore primitivo stata identificata in 7 / 29 ( 2 carcinomi del nasofaringe , 1 plasmocitoma della base della lingua , 1 carcinoma polmonare , 2 carcinomi della mammella ) con una sensibilit del 24% . 
questo risultato , comunque , non confrontabile con il nostro studio in quanto alberini ha incluso nel campione 22 soggetti che avevano un altro test convenzionale positivo : questo significa che la pet ha fornito indicazioni aggiuntive solamente in 4 / 44 casi . 
nonostante la popolazione non fosse stata selezionata , al contrario di quella descritta nel nostro studio , la sensibilit della pet risultata del 37 , 8% , che sensibilmente inferiore a quella da noi riportata . sebbene un potenziale limite al presente studio sia rappresentato dal fatto che il campione preso in esame eterogeneo in quanto costituito da pazienti provenienti da centri diversi e portatori di neoplasie di diverso tipo , tuttavia questo non toglie valore allo studio in quanto lapproccio diagnostico - terapeutico in casi di tumore primitivo ignoto non ancora codificato da norme internazionali . 
alcune sedi quali il capo - collo , laddome e la pelvi , sono anatomicamente molto complesse e caratterizzate da varie sedi di fisiologico uptake del tracciante ( per esempio le tonsille , il tessuto linfatico , lo stomaco , lintestino , gli ureteri )  . 
of the 467 patients examined by cdus , 159 ( 34% ) showed no signs of renal artery stenosis ( ras ) or nephropathy and were therefore started on medical therapy . 
nel periodo 20002004 sono giunti alla nostra osservazione 467 pazienti ( 205 donne e 262 uomini , range 2096 anni ) , per essere sottoposti ad indagine ecd , in quanto presentavano ipertensione arteriosa resistente alla terapia e / o segni di insufficienza renale . 
dei 467 pazienti esaminati mediante ecd , 159 ( 34% ) non presentavano indici di stenosi delle arterie renali n segni ecografici di nefropatia , ed hanno proseguito un iter terapeutico medico . 
dai risultati ottenuti e alla luce dei dati della letteratura , si riconferma il ruolo fondamentale svolto dallecd nei pazienti con sospetta o accertata patologia nefro - vascolare , fornendo dati importanti sullemodinamica renale di insostituibile utilit per un corretto approccio clinico - terapeutico . parole chiave eco color doppler ipertensione nefrovascolare arterie renali introduction introduzione atherosclerotic renal artery stenosis ( ras ) is associated with two common clinical syndromes , renovascular hypertension and ischaemic nephropathy , which imply a significant worsening of renal function in the presence of stenosis [ 13 ]  . the exact prevalence of ras is unknown , but many data indicate that it is high among elderly , chiefly caucasian , subjects and those with diabetes , diffuse atherosclerosis and rela stenosi aterosclerotica dellarteria renale ( sar ) si associa a due comuni sindromi cliniche : lipertensione nefro - vascolare e la nefropatia ischemica , intendendo per questultima una significativa riduzione della funzione renale in presenza della stenosi [ 13 ]  . lesatta prevalenza della stenosi aterosclerotica dellarteria renale non nota , ma molti dati fanno ritene1115 g.c. 
renal angiography and renal colour - doppler ultrasound ( cdus ) studies performed during coronary angiography or peripheral arteriography have demonstrated that ras is present in 20%30% of more than 10 , 000 investigations [ 1 ]  . 
a large number of patients with serum creatinine higher than 1.7 mg / dl have been found to have ras in prospective and retrospective studies , and ras has been demonstrated in 5%10% of patients with acute renal failure [ 1 ]  . 
this prevalence becomes higher when other clinical signs of atherosclerosis coexist , with rates of 12%24% in patients undergoing coronary angiography , 11% in stroke patients and 40% in patients with peripheral vascular disease [ 3 ]  . 
few studies have assessed atherosclerotic ras in patients with abdominal aorta aneurysm ( aaa ) , another manifestation of atherosclerotic disease . the high prevalence of atherosclerotic ras has raised the need to identify a noninvasive , inexpensive modality with high diagnostic accuracy in order to reduce the use of invasive investigations , such as arteriography , which nonetheless remains the gold standard in the diagnosis of ras [ 2 , 4 , 5 ]  . diagnostic imaging offers several noninvasive methods for selecting patients for angiography : cdus , captopril renal scintigraphy , spiral computed tomography ( ct ) angiography , and magnetic resonance ( mr ) angiography [ 2 , 3 , 511 ]  . cdus of the renal arteries is currently the main screening tool for ras , and many international studies have demonstrated a sensitivity of 83%96% , a specificity of 76%98% , a positive predictive value ( ppv ) of 81%92% and a negative predictive value ( npv ) of 94%98% [ 58 , 1115 ]  . 
the advantages of cdus are that it is inexpensive , reproducible , noninvasive and has good npv when performed in selected populations ; its known disadvantages , on the other hand , are operator dependence , patient preparation and cooperation , scars , obesity , bowel gas and vascular abnormalities , in particular , the presence of anatomical variants of the renal artery [ 2 , 4 , 6 , 1517 ]  . the primary aim of our study was to evaluate the role and usefulness of cdus in analysing overall renal morphology and haemodynamics in patients with hypertension and nephropathy ; the secondary aim was to assess the association between atherosclerotic ras and aaa . materials and methods between 2000 and 2004 , 467 patients ( 205 women and 262 men , age range 2096 years ) with refractory hypertension and / or signs of renal failure ( serum creatinine > 2.5 mg / dl ) were referred to our department for renal cdus . the patients were examined by a single radiologist on a philips ssd 800 and hitachi h21 scanner using a 3.5 - mhz convex - array transducer and colourand power - doppler mode . 
sonograms were assessed for renal morphology , overall renal blood flow and abdominal aorta . 1116 re che essa sia assai frequente nei soggetti anziani , specie di razza caucasica , diabetici , con patologia aterosclerotica polidistrettuale e con insufficienza renale . 
studi angiografici renali e di eco color doppler ( ecd ) renale , eseguiti in corso di coronarografia o di arteriografia periferica , hanno documentato una frequenza di sar nel 20%30% di oltre 10000 indagini [ 1 ]  . 
analisi retrospettive o prospettiche in pazienti con creatininemia superiore a 1 , 7 mg / dl dimostrano presenza di sar in molti casi , cos come in casi di insufficienza renale acuta si ha la sua dimostrazione nel 5%10% dei casi [ 1 ]  . 
poich la stenosi aterosclerotica dellarteria renale pu indurre un danno renale progressivo , in alcune casistiche essa causa di ingresso in dialisi nel 15%30% dei pazienti uremici [ 1 ]  . 
in pazienti anziani non selezionati stata dimostrata mediante ecd una prevalenza del 6 , 6% ; la prevalenza maggiore quando coesistono altre manifestazioni cliniche dellaterosclerosi : nei pazienti sottoposti a coronarografia la prevalenza varia dal 12% al 24% , nei pazienti con ictus dell11% , nei pazienti con malattia vascolare periferica intorno al 40% [ 3 ]  . 
esistono pochi dati che valutino levidenza della sar nei pazienti portatori di aneurisma dellaorta addominale , che rappresenta altra manifestazione di patologia aterosclerotica . lelevata prevalenza di tale patologia ha sollevato la necessit di individuare una metodica non invasiva , a basso costo e con elevata accuratezza diagnostica al fine di limitare il ricorso ad unindagine strumentale invasiva , quale larteriografia che rimane , comunque , la metodica gold standard nella diagnosi della stenosi delle arterie renali [ 2 , 4 , 5 ]  . 
limaging attualmente ha a disposizione alcune metodiche non invasive , come indagini di screening e selezione per la successiva angiografia : lecd , la scintigrafia renale con captopril , langio - tc spirale , langiorm [ 2 , 3 , 511 ]  . 
attualmente lecd delle arterie renali risulta la principale metodica di screening nella diagnosi di stenosi delle arterie renali con numerosi lavori in ambito internazionale che attribuiscono a tale metodica valori di sensibilit pari all83%96% , di specificit 76%98% , valore predittivo positivo 81%92% e valore predittivo negativo 94%98% [ 58 , 1115 ]  . 
in tutti i pazienti , per una pi ampia e corretta valutazione vascolare , stata esaminata laorta addominale , valutandone calibro , morfologia e flusso ( diametro normale < 2 , 5 cm , ectasia 2 , 53 cm , aneurisma > 3 cm )  . risultati dei 467 pazienti esaminati mediante ecd , 159 ( 34% ) non presentavano indici di stenosi delle arterie renali n segni ecografici di nefropatia , ed hanno proseguito un iter terapeutico medico ; in particolare uno di questi pazienti era portatore di protesi aorto - renale pervia . 
i restanti 308 pazienti ( 66% ) mostravano invece segni ecografici di stenosi emodinamicamente significativa o di nefropatia . in particolare , 174 pazienti ( 37 , 2% ) mostravano solo segni di nefropatia , con riduzione del flusso ematico in sede ilare ed ostiale ed un aumento dell ir ; in 123 pazienti ( 26 , 3% ) era presente nefropatia severa con ir 0 , 80 e tra questi un paziente presentava aneurisma dellarteria renale ed un paziente necrosi corticale acuta , confermati successivamente con esame tc ; 51 ( 10 , 9% ) invece presentavano nefropatia moderata con ir di 0 , 75 . in 134 pazienti ( 28 , 7% ) veniva evidenziata una sar emodinamicamente significativa ; 58 dei 134 pazienti ( 12 , 4% ) con sar presentavano segni di nefropatia associata ; in 2 di questi era gia stato posizionato stent , 2 hanno eseguito an1117 fig . 
to obtain a more exhaustive and correct vascular assessment , the calibre , morphology and flow pattern of the abdominal aorta were also evaluated in all patients ( normal diameter < 2.5 cm , ectasia 2.53 cm , aneurysm > 3 cm )  . results of the 467 patients examined with cdus , 159 ( 34% ) had no indices of ras or sonographic signs of nephropathy and were started on medical therapy ; in particular , one of them had a patent aortorenal stent . 
the remaining 308 patients ( 66% ) had sonographic evidence of haemodynamically significant stenosis or nephropathy . in detail , 174 patients ( 37.2% ) showed signs of nephropathy only , with reduced hilar and ostial flow and increased ri . nephropathy was severe in 123 patients ( 26.3% ) , with ri 0.80 ; among them , one had renal artery aneurysm and one had acute cortical necrosis , later confirmed by ct . 
altri 22 pazienti non hanno eseguito angiografia ; in particolare , 1 aveva gi posizionato stent renale , 1 presentava iperplasia mio - intimale , 10 pazienti avevano gi una completa occlusione dellarteria renale , mentre 10 pazienti sono al momento in attesa di eseguire angiografia ed eventuale intervento di rivascolarizzazione . 
in totale , quindi , 33 pazienti , con sar e senza segni di nefropatia ( 7% del totale e 44% dei pazienti con segni ecd di stenosi ) non hanno eseguito esame angiografico . quarantre pazienti ( 9 , 2% del totale e 56% dei positivi per stenosi allecd ) hanno invece eseguito angiografia che ha confermato la diagnosi in 39 dei 43 pazienti . 
di questi , 24 ( 5 , 1% del totale e 55 , 8% dei positivi per stenosi ) hanno posizionato stent con ripristino ottimale della vascolarizzazione renale nel 92% dei casi ( solo in 2 casi erano presenti dopo la procedura interventistica segni clinico - laboratoristici e bioptici di ateroembolismo colesterinico , con quadro di severa compromissione dellemodinamica renale allecd in entrambi i casi )  . diciannove pazienti ( 4% del totale e 44 , 2% dei positivi per stenosi ) invece non hanno posizionato stent : di questo ultimo gruppo 7 avevano gi posizionato stent ( 2 completamente chiusi e 5 restenosi ) , in 3 sussistevano problemi anatomici con biforcazione precoce dellarteria renale , 1 paziente presentava middle aortic syndrome , in 1 caso si era verificata complicanza ( dissezione in corso di procedura ) , in 1 un caso langiografista non riusciva a superare la stenosi , 1 paziente presentava dissezione aortica , in 1 caso si trattava di stenosi lieve - moderata e 2 erano falsi positivi . in particolare , lecd ha permesso di svelare in una giovane paziente una grave situazione anatomica , verosimilmente su base congenita , definita come middle aortic syndrome o coartazione aortica sottodiaframmatica . 
dopo una gestosi , nella paziente era insorta una severa ipertensione arteriosa e , dopo unindagine ecografia risultata negativa per alterazioni morfologiche renali , era stata sottoposta ad indagine ecd che rilevava marcato decremento degli ir arteriosi intraparenchimali ( ir = 0 , 45 ) con polso parvus et tardus in sede ilare e segni di stenosi emodinamicamente significative di entrambe le arterie renali . 
this was associated with signs of nephropathy in 58 patients ( 12.4% ) ; two had already had a stent implanted , two underwent angiography and one had polycystic kidneys , whereas the remaining 56 were excluded from angiography because of signs of severe nephropathy ( longitudinal diameter < 8 cm , ri > 0.80 and poor parenchymal perfusion on cd and pd imaging )  . 
a further 22 patients did not undergo angiography , as one had a renal stent , one had myointimal hyperplasia , ten had complete occlusion of the renal artery , whereas ten were on the waiting list for angiography and possible revascularisation at the time of this writing . 
therefore , a total of 33 patients with ras and without evidence of nephropathy ( 7% of the total and 44% of patients with cd signs of stenosis ) did not undergo angiography . forty - three patients ( 9.2% of the total and 56% of those with ras on cdus ) underwent angiography , which confirmed the diagnosis in 39 . 
of these , 24 ( 5.1% of the total and 55.8% of those with stenosis ) underwent renal stenting , with optimally restored renal perfusion in 92% of cases ( only two had clinical , laboratory and biopsy evidence of cholesterol atheroembolism , with severely impaired renal haemodynamics on cdus , after the interventional procedure )  . nineteen patients ( 4% of the total and 44.2% of those with stenosis ) did not undergo stent implantation : seven of these already had stents ( two of which completely occluded and five with restenosis ) , three patients presented early bi1118 g.c. 
b indagine tc con mdc : assenza di opacizzazione in sede corticale renale bilaterale ( c )  . furcation of the renal artery , one patient had middle aortic syndrome , one developed a complication ( dissection during the procedure ) , in one , the operator could not negotiate the stenosis , one had aortic dissection , one had mild to moderate stenosis and two were false positives . 
following a gestosis , the patient developed severe arterial hypertension and , after a negative sonography for morphological renal alterations , was studied by cdus , which revealed marked reduction of intraparenchymal arterial ri ( ri = 0.45 ) with parvus - tardus pulse in the hilum and signs of haemodynamically significant stenoses of both renal arteries . 
il 56% di questi presentava una marcata riduzione del flusso a livello delle arterie renali e nel 30% erano presenti stenosi emodinamicamente significative delle arterie renali ed in un caso ( 6% ) unarteria renale era occlusa . per quanto riguarda la presenza di aneurisma dellaorta addominale ( aaa ) operato e non , i dati raccolti sono i seguenti : laaa era presente in 19 pazienti dei 333 senza segni di sar ( 5 , 7% ) con netta prevalenza nei pazienti con nefropatia ( 16 casi ) rispetto ai pazienti senza nefropatia ( 3 casi ) mentre laaa era presente in 15 dei 134 pazienti con segni 1119 g.c. 
this translates into a marked clinical benefit for the patient as well as considerable economic savings , given that out of the 467 patients studied by cdus , 88% did not undergo angiography as against 22% who did undergo angiography . 
if we exclude patients who underwent angiography before cdus ( cdus follow - up ) and those with a previously implanted stent , the remaining 65% underwent stent revascularisation , with excellent outcome in all patients except two , one of whom develop cholesterol atheroembolism after the procedure . in some cases , cdus revealed severe impairment of renal circulation in patients with poor renal compensation who showed only minor laboratory alterations ( serum creatinine 1.62.5 mg / dl )  . 
in addition to being valuable for analysing renal morphology and volume and assessing blood flow on cdus and pdus , evaluation of the ri proved to be reliable for determining renal function 1120 di sar ( 11 , 2% ) ; la presenza di aaa operato stata di 5 pazienti tra i 333 senza segni di sar ( 1 , 5% ) ed in particolare pi frequente tra i pazienti nefropatici ( 4 casi ) che nei non nefropatici ( 1 caso ) mentre la presenza di aaa operato nei pazienti con segni di sar stata di 10 pazienti sui 134 ( 7 , 46% )  . discussione dai risultati ottenuti si riconferma lutilit dellecd nellesaminare i pazienti con ipertensione e nefropatia ; lo studio dellemodinamica renale con ecd si rilevata in alcuni casi indagine insostituibile per un corretto approccio clinico - terapeutico [ 2 , 5 , 7 , 9 , 15 ]  . lecd ha evitato langiografia nei pazienti negativi e in quelli con stenosi occlusiva dellarteria renale e con segni di grave nefropatia , nei quali lintervento avrebbe potuto aggravare il deficit renale ( tossicit del mdc , ateroembolismo colesterinico , ecc . ) con indubbio vantaggio clinico per il paziente e risparmio economico . 
infatti del totale dei 467 pazienti esaminati allecd l88% non stato sottoposto ad esame angiografico e solo il 22% ha eseguito angiografia . escludendo i pazienti che hanno eseguito lindagine angiografica prima dellecd ( monitoraggio ecd ) e i pazienti con pregresso posizionamento di stent , i restanti 65% sono stati sottoposti ad intervento di rivascolarizzazione con stent con ottimi risultati in tutti i pazienti ( ad eccezione di 2 casi , uno dei quali presentava ateroembolismo colesterinico dopo la procedura )  . lindagine ecd ha rilevato in diversi casi una compromissione del circolo renale di diversa entit in pazienti con labile compenso renale che presentavano modeste alterazioni laboratoristiche ( creatininemia 1 , 62 , 5 mg / dl ) ; in questi casi il corretto approccio terapeutico ha sicuramente ritardato lesaurimento della funzionalit renale ed il ricorso al trattamento dialitico con il miglioramento della qualit della vita  . 
si tratta di una sindrome non comune in letteratura , descritta in giovane et ( 628 anni ) come variet rara di coartazione aortica ( 0 , 2%2% delle coartazioni aortiche ) , associata ad aneurisma dellaorta addominale e a stenosi della arteria renale . 
rarely reported in the literature , the syndrome has been described in young subjects ( 628 years old ) as a rare variant of aortic coarctation ( 0.2%2% of aortic coarctations ) and to be associated with aaa and ras . 
multiple causes have been recognised , including congenital and secondary to takayasus syndrome , von recklinghausens neurofibromatosis , coeliac disease and autoimmune disorders ( dermatitis herpetiformis , insulindependent diabetes ) , and clinical onset is usually renovascular hypertension and claudication [ 2224 ]  . in 16 patients with a clinical and laboratory diagnosis of cholesterol atheroembolism , the results of cdus provided a good indication of the severity of their clinical condition : in 12 patients , the condition arose after interventional procedures ( five after angiography , four after coronary angiography , one after coronary artery stenting , one after subclavian artery stenting and one after left renal artery stenting ) and in four patients following administration of coumadall patients had signs of severely impaired parenchymal flow due to cholesterol emboli clogging the small arteries and causing inflammatory reactions , intimal proliferation , vessel fibrosis and luminal obliteration . 
despite being nonspecific findings on cdus , these alterations translate into increased resistive index in the intrarenal arteries and reduced parenchymal and hilar flow in the renal arteries . in nine cases , cdus diagnosed renal artery occlusion in patients with modest chronic renal failure whose renal function had rapidly declined ; thus , it avoided the need for further investigations and enabled selection of patients for medical therapy . 
the study of the renal artery should not be limited to the ostial region ( where the majority of stenoses are present ) but should include an overall assessment of renal arterial circulation to detect possible alterations and evaluate the feasibility of an appropriate revascularisation procedure . 
patients with severe impairment of renal haemodynamics who were unlikely to benefit from revascularisation were therefore excluded from angiography [ 17 , 25 ]  . our experience highlights the association between aaa and ras , an important factor for vascular surgeons and angiographers considering endovascular treatment for aortic aneurysms and for selecting the most appropriate strategy when the two diseases coexist [ 2630 ]  . this study reconfirms the crucial role of cdus in monitoring patients who have undergone stent revascularisation procedures [ 25 ]  . 
in addition , it raises the problem of contrast medium toxicity in patients with poor renal function . cdus consistently revealed haemodynamically significant stenosis of the stent site with parvus - tardus pulse below the stenosis , in most cases due to the presence of fibrointimal celiaco e malattie autoimmuni ( dermatite erpetiforme , diabete insulino dipendente ) ; spesso ad esordio clinico con ipertensione nefrovascolare e claudicatio [ 2224 ]  . in 16 pazienti con diagnosi clinico - laboratoristica di ateroembolismo colesterinico , lecd ha fornito risultati che ben rispecchiano la gravit del quadro clinico : in 12 pazienti il quadro insorto dopo manovre interventistiche ( 5 dopo angiografia , 4 dopo coronarografia , 1 dopo posizionamento di stent in arteria carotide , 1 in arteria succlavia e 1 in arteria renale sinistra ) e in 4 pazienti dopo somministrazione di coumadin tutti i pazienti sono stati rilevati segni di grave compromissione del circolo parenchimale dovuto agli emboli di colesterolo il cui impianto nelle piccole arterie seguito da una reazione infiammatoria , proliferazione dellintima , fibrosi dei vasi colpiti e obliterazione del lume vasale . 
tali alterazioni , pur essendo aspecifiche allecd , si traducono con lincremento dellindice di resistenza arterioso intrarenale e con riduzione del flusso parenchimale e ilare nelle arterie renali . in 9 casi lecd ha diagnosticato locclusione di unarteria renale , in pazienti con modesta insufficienza renale cronica che avevano presentato rapido aggravamento della funzionalit renale evitando in questi ulteriori indagini e sottoponendoli alla sola terapia medica . 
lo studio dellarteria renale non deve esaurirsi alla sede ostiale ( ove presente la maggior parte delle stenosi ) ma deve valutare globalmente il circolo arterioso renale per evidenziare eventuali alterazioni e per valutare la possibilit di proporre al paziente un corretto intervento di rivascolarizzazione . 
sono pertanto stati esclusi dallangiografia i pazienti che presentavano severa compromissione dellemodinamica renale , che probabilmente non avrebbero tratto beneficio dal trattamento di rivascolarizzazione [ 17 , 25 ]  . la nostra esperienza mette in risalto lassociazione fra la patologia aneurismatica dellaorta addominale e la stenosi dellarteria renale , dato sicuramente molto importante per il chirurgo vascolare e per langiografista , alla luce del trattamento endovascolare degli aneurismi aortici e sulla scelta strategica pi opportuna in presenza contemporanea delle due patologie [ 2630 ]  . in questo studio viene riaffermato linsostituibile ruolo svolto dallecd nel monitoraggio dei pazienti che hanno subito interventi di rivascolarizzazione con stent [ 25 ]  . 
in questi pazienti lindagine angio - tc ha fornito , nella nostra esperienza , informazioni sul corretto posizionamento dello stent ma risultato difficile lo studio della perviet dello stent stesso , senza tener conto della tossicit del mdc in questi pazienti dalla gi labile funzionalit renale . lesame ecd ha rilevato stenosi emodinamicamente significative in corrispondenza dello stent con presenza di polso parvus et tardus nel tratto a valle la stenosi in tutti i pazienti , nella maggior parte dovuto alla presenza di iperplasia fibrointimale o a placche aterosclerotiche site prossimalmente o distalmente rispetto allo stent . 
cdus identified patients with restenosis ( seven cases ) , all of which were confirmed by angiography and subsequently treated by repeat revascularisation ( placement with another co - axial stent or with the use of a cutting balloon )  . conclusioni di rivascolarizzazione ( posizionando un altro stent coassiale o con lutilizzo del cutting ballon )  . conclusions on the basis of our results and data from previous reports , we confirm that cdus plays a fundamental role in patients with suspected or known renovascular disease , as it provides important information on renal haemodynamics and guides the clinician towards the most appropriate clinical and therapeutic approach [ 2 , 57 , 1416 ]  . our results indicate that cdus , with appropriate selection criteria , is able to discriminate between patients who should or should not undergo angiography , leading to considerable economic savings and benefits for the patient , who can thus be directed to the most appropriate treatment plan [ 16 ]  . 
in addition , our findings point to a close association between the presence of aaa and ras and confirm the need for close collaboration between the vascular surgeon , the interventional radiologist and the nephrologist in planning the most appropriate treatment approach in these patients with associated diseases [ 2630 ]  . cdus proved its value in confirming the diagnosis of cholesterol embolism suspected on the basis of clinical and laboratory findings . 
these patients carry a poor prognosis , with 1 - year mortality rates between 64% and 87% , and monitoring by imaging may certainly help the clinician deal with this complex disease given that angiography is strongly contraindicated both because it is an interventional manoeuvre and because it requires heparin administration [ 3133 , 34 ]  . in the patient with middle aortic syndrome , cdus revealed the alteration in renal haemodynamics , thus justifying the use of a more panoramic modality , such as ct angiography , which shed light on the patients complex anatomical situation [ 2224 ]  . another important contribution of cdus was to substantiate the clinical and laboratory suspicion of acute renal failure in a septic patient with cortical necrosis . 
use of contrast medium , justified by the need to shed light on what was clearly a very critical clinical situation , enabled prompt treatment ( haemodialysis and plasmapheresis ) , with partial recovery of renal function [ 35 ]  . cdus confirmed its value in monitoring nephropathic patients and those who have undergone renal artery revascularisation procedures [ 17 , 25 ]  . 
our experience also highlights the importance of cdus in monitoring patients in whom renal artery occlusion or stenosis has been diagnosed at angiography : in these patients , clinical and laboratory monitoring should be combined with follow - up by cdus , which is able to effectively reveal disease progression and provide the clinician with the data required for a more appropriate treatment strategy . 1122 dai risultati ottenuti e alla luce dei dati della letteratura , si riconferma il ruolo fondamentale svolto dallecd nei pazienti con sospetta o accertata patologia reno - vascolare , fornendo dati importanti sullemodinamica renale di insostituibile utilit per un corretto approccio clinico - terapeutico [ 2 , 57 , 1416 ]  . dai nostri risultati si evince come ecd , alla luce dei criteri adottati , possa essere metodica in grado di discriminare i pazienti che devono o non devono essere sottoposti ad esame agiografico , con risparmio dei costi e beneficio per il paziente che potr quindi essere indirizzato al pi opportuno iter terapeutico [ 16 ]  . 
i nostri dati mettono inoltre in risalto unelevata associazione fra la presenza dellaaa e la sar : questo vuole riconfermare lutilit di una stretta collaborazione fra il chirurgo vascolare , il radiologo interventista e il nefrologo nel programmare la strategia terapeutica pi opportuna in questi pazienti con patologia associata [ 2630 ]  . lecd si dimostrata metodica utile nel confermare la diagnosi di ateroembolismo colesterinico , gi prospettata in base ai dati clinico - laboratoristici . 
questi sono pazienti a prognosi infausta con mortalit ad 1 anno variabile dal 64% all87% in cui il monitoraggio strumentale pu essere certamente di ausilio al clinico nellaffrontare una cos complessa patologia , dal momento che in tali pazienti fortemente controindicata langiografia , sia perch manovra interventistica sia per la somministrazione di eparina [ 3133 , 34 ]  . nella paziente con la middle aortic syndrome lecd ha svelato lalterazione emodinamica a livello renale , giustificando il ricorso a metodiche pi panoramiche come langiotc che ha rilevato la complessa situazione anatomica da cui era affetta [ 2224 ]  . occorre senzaltro rimarcare limportanza dellecd nel confermare lipotesi clinico - laboratoristica di insufficienza renale acuta in corso di sepsi nella paziente affetta da necrosi corticale ; lutilizzo del mdc , giustificato dalla necessit di chiarire una situazione che allesordio era molto critica , ha consentito la tempestiva terapia ( emodialisi e plasmaferesi ) con parziale recupero della funzione renale [ 35 ]  . la metodica ecd si dunque riconfermata di indubbio valore nel monitoraggio dei pazienti nefropatici e di quelli sottoposti ad intervento di rivascolarizzazione allarteria renale [ 17 , 25 ]  . 
souza de oliveira ir , widman a , molinar lj et al ( 2000 ) color doppler ultrasound : a new index improves the diagnosis of renal artery stenosis . ultrasound med biol 26 : 4147 12 . 
frauchiger b , zierler r , bergelin ro et al ( 1996 ) prognostic significance of intrarenal resistance indices in patients with renal artery interventions : a preliminary duplex sonographic study . cardiovasc surg 4 : 324330 18 . 
mehta m , darling rc 3rd , roddy sp et al ( 2004 ) outcome of concomitant renal artery reconstructions in patients with aortic aneurysm and occlusive disease . vascular 12 : 381386 29 . 
manenti , tel : + 39 - 06 - 20902401 , fax : + 39 - 06 - 20902404 , e - mail : guggi@tiscali.it received : 9 november 2005 / accepted : 30 march 2006 / published online : 20 december 2006 abstract purpose . 
morphological imaging was obtained with t2 - weighted turbo spin - echo ( tse ) sequences with and without fat suppression [ spectral presaturation with inversion recovery ( spir ) ] and an axial dynamic t1 - weighted spir fast - field echo ( ffe ) sequence during intravenous administration of contrast material . 
our preliminary results indicate that dwi is useful for characterising tissue in the different regions of the prostate gland and in distinguishing normal from cancerous tissues , given its ability to detect early changes in the structural organisation of prostate tissue . key words prostate mr diffusion adc value of prostate tumours 1124 riassunto obiettivo . 
la diffusione un processo fisico basato sul movimento casuale delle molecole dacqua noto come moto browniano . limaging pesato in diffusione ( dwi ) quindi una tecnica di risonanza magnetica ( rm ) che fornisce indirettamente informazioni sulle propriet biofisiche dei tessuti come la densit , lorganizzazione cellulare e la microstruttura , che determinano la diffusibilit delle molecole dacqua . 
limaging morfologico stato condotto mediante sequenze tse t2 - pesata con e senza tecnica di soppressione del segnale del grasso ( spir ) ed una sequenza dinamica ffe assiale t1 - pesata spir durante somministrazione ev di mdc . 
il valore medio di adc della porzione centrale della ghiandola ( 1512 , 07124 , 8510 - 3 mm2 / s ) risultato significativamente pi basso del valore di adc della porzione periferica ( 1984 , 11226 , 2310 - 3 mm2 / s ) ( p < 0 , 01 )  . 
currently , mri is the only technique able to assess molecular diffusion in vivo and provide information about such biophysical properties of tissue as cell organisation , density and microstructure [ 1 ]  . rapid changes in diffusion properties can be identified by calculating the diffusion coefficient ( dc )  . 
however , in biological systems , this coefficient is known as apparent diffusion coefficient ( adc ) because its value is influenced not only by the brownian motion of water molecules , but also by other polluting factors , including perfusion and t2 tissue signals [ 2 ]  . diffusion mri techniques have been mainly used in the field of neuroradiology to evaluate cerebral ischaemia , stroke and multiple sclerosis , and to differentiate normal from cancerous tissue . 
all patients received ten punctures according to the division of the prostate into octants ( one puncture each for apex , intermediate zone and base , and two punctures on each side for the lateral zones )  . 
at least two samples were obtained from zones presenting abnormal features on mri and trus . mri study the mri examination was performed using a 1.5 - tesla magnet ( philips gyroscan intera ; best , the netherlands ) equipped with a master dynamic gradient system ( 30 mt / m maximum power and 150 mt / m / ms slew rate ) using a multichannel surface coil . le immagini di risonanza magnetica ( rm ) pesate in diffusione ( dwi ) sono sensibili alla diffusione molecolare dovuta ai movimenti casuali delle molecole dacqua in grado di produrre in un gradiente di campo magnetico unalterazione incoerente della fase che determina unattenuazione dellintensit di segnale . 
attualmente la rm la sola tecnica in grado di valutare il processo di diffusione molecolare in vivo e consente di ottenere quindi informazioni sulle propriet biofisiche dei tessuti come lorganizzazione , la densit cellulare e la microstruttura [ 1 ]  . rapidi cambiamenti nelle caratteristiche di diffusione possono essere identificati calcolando il coefficiente di diffusione ( dc )  . 
tuttavia , nei sistemi biologici si deve parlare di coefficiente apparente di diffusione ( adc ) poich il valore del coefficiente misurato determinato non solo dal moto browniano delle molecole dacqua , ma anche da altri fattori inquinanti , fra cui la perfusione del microcircolo e la componente t2 tissutale [ 2 ]  . finora le tecniche di diffusione rm sono state abitualmente utilizzate nel campo della neuroradiologia per la valutazione dellischemia cerebrale , dello stroke , della sclerosi multipla e per differenziare tessuto sano da quello tumorale . 
per lo studio degli organi addominali le sequenze pesate in diffusione non sono ancora entrate nella pratica clinica soprattutto per motivi di natura tecnica : movimenti respiratori , suscettibilit magnetica dellaria nei polmoni e nellintestino , e artefatti da pulsatilit e da movimento rappresentano le cause pi comuni della scarsa qualit delle immagini pesate in diffusione anche a livello addominale . lavvento delle sequenze eco - planari a singolo impulso ultraveloci ( epi ) in associazione con le tecniche di acquisizione in una singola apnea , hanno consentito la fattibilit delle sequenze pesate in diffusione anche a livello addominale [ 3 , 4 ]  . lo scopo del nostro studio stato quello di valutare laffidabilit del dwi nella valutazione delladc delle differenti regioni anatomiche della ghiandola prostatica e di testare la possibilit di eseguire una differenziazione fra tessuto sano e maligno sulla base del valore di adc . materiali e metodi pazienti sono stati studiati 10 volontari ( et media 56 anni , range : 4072 anni ; psa totale medio 4 , 65 , range 2 , 86 , 5 ng / ml ) e 19 pazienti ( et media 65 anni , range : 4585 anni ; psa totale medio 25 , 15 , range 4 , 346 ng / ml ) con tumore prostatico , precedentemente diagnosticato con esame ecotomografico trans - rettale ( trus ) e successivamente confermato con biopsia trus - guidata eseguita entro un mese dopo lesecuzione dellesame rm . 
in tutti i pazienti sono stati effettuati 10 prelievi secondo suddivisione in ottanti della prostata ( 1 prelievo per apice , zona intermedia , basale e 2 per la zona laterale per ciascun lato )  . 
le immagini pesate in diffusione sono state ottenute prima delliniezione di mezzo di contrasto con una sequenza single - shot spin - echo epi inversion recovery ( te 64 , tr 2500 , fa 90 , fov 140 mm , matrice 6464 , spessore di sezione 3 mm , intervallo 1 mm , 15 slice , valore b = 0 , 125 , 250 , 375 and 500 s / mm2 ) , nsa 6 e tempo di acquisizione 4 minuti e 22 secondi , orientata sul piano assiale e con lutilizzo della tecnica di codifica del segnale sense . misurazione adc la mappa di adc stata ottenuta per ogni slice calcolando il valore di adc dei singoli pixel utilizzando un algoritmo illustrato dalla seguente equazione : adc ( mm2 / s ) = 1 / 1000ln [ is ( b0 ) / is ( bx ) ] dove is ( b0 ) rappresenta lintensit del segnale nelle acquisizioni con fattore b uguale a 0 e is ( bx ) rappresenta lintensit del segnale nelle acquisizioni con fattore b uguale ad ognuno dei valori utilizzati . 
sulle immagini assiali della sequenza pesata in diffusione con valore b = 0 , che non contengono dati sulla diffusione molecolare , ma sono caratterizzate da una pesatura t2 , sono state posizionate roi ( regioni di interesse ) bilaterali e simmetriche , di forma ellittica e con area equivalente ad 8 pixel , a livello della zona centrale , della periferia e dellarea tumorale ( area focale di ipointensit relativa rispetto al parenchima circostante ) , quando presente , avendo cura di evitare calcificazioni e cisti . 
in particolare stato adottato il paired students t test per valutare le differenze statistiche fra i valori di adc delle differenti aree prostatiche sane e malate allinterno dei due gruppi separatamente ; mentre stato adottato lunpaired students t test per valutare le differenze statistiche dei valori di adc delle singole aree prostatiche fra i due gruppi . 
on the axial dwis with b = 0 , which do not contain data on molecular diffusion but are characterised by t2 weighting , we positioned symmetrical elliptical regions of interest ( rois ) measuring 8 pixels bilaterally in the central and peripheral zone and in the tumour area ( a relatively hypointense focal area compared with the surrounding parenchyma ) , when present , taking care to avoid calcifications and cysts . 
data were processed using the statistical package for social sciences , version 12 ( spss , chicago , il , usa )  . results 1128 all examinations were diagnostic , and no case was excluded from the study . nei 19 pazienti il valore medio del coefficiente apparente di diffusione ( adc ) della zona centrale della ghiandola prostatica ( 1512 , 07124 , 8510 - 3 mm2 / s ) risultato statisticamente pi basso del valore medio di adc della zona periferica sana ( 1984 , 11226 , 2310 - 3 mm2 / s ) e il valore medio di adc dei tumori ( 958 , 97168 , 9810 - 3 mm2 / s ) risultato statisticamente pi basso del valore medio di adc della zona periferica sana ( p < 0 , 01 )  . 
la variabilit dei risultati ottenuti legata soprattutto alla differente pesatura in diffusione delle immagini , rappresentata dal valore del fattore b che racchiude le principali caratteristiche dei gradienti di diffusione ( ampiezza , durata e intervallo di tempo ) [ 1 , 58 ]  . la pesatura in diffusione ideale di una sequenza epi rappresenta ancora un problema irrisolto . 
se vengono utilizzati valori bassi di fattore b ( 30100 s / mm2 ) pu risultare una sovrastima del valore di adc per laggiunta della componente t2 tissutale e della perfusione del microcircolo al valore puro di diffusione delle molecole dacqua . 
 [ 9 ] hanno proposto una sequenza pesata in diffusione con fattore b di 0 e 1000 ed elevata risoluzione spaziale , acquisita mediante bobina di superficie : contrariamente agli altri lavori apparsi in letteratura sullutilizzo delle sequenze pesate di diffusione nella diagnosi del tumore prostatico , il tessuto neoplastico stato in questo caso individuato grazie al suo segnale iperintenso nelle immagini con fattore b 1000 , senza la costruzione di mappe di adc a causa della riduzione del rapporto segnale / rumore e quindi della qualit delle immagini , determinati dalla forte pesatura in diffusione [ 9 ]  . nel nostro lavoro , al fine di ottenere una valutazione quantitativa della restrizione del coefficiente di diffusione apparente , abbiamo deciso di utilizzare un valore massimo di fattore b pari a 500 e di costruire mappe di adc grazie al buon rapporto segnale / rumore . 
4 valore medio adc ( 10 - 3 mm2 / s ) con relativo valore di deviazione standard nella zona periferica ( zp ) , nella zona centrale ( zc ) e nelle aree tumorali dei 19 pazienti esaminati . discussion mri is currently the only technique capable of measuring molecular diffusion in vivo . 
la mappa di adc stata ottenuta dai dati acquisiti con i singoli valori di fattore b . la difficolt aggiuntiva nella valutazione dei valori di adc nella ghiandola prostatica risiede nella disomogeneit del suo parenchima , soprattutto per quanto riguarda la porzione centrale sia essa normale che adenomatosa , spesso sede di alterazioni di natura sia cistica che fibro - calcifica le2350 2150 1950 1750 1550 1350 1150 2350 2150 1950 1750 1550 1350 1150 1130 g . 
if low b - values ( 30100 s / mm2 ) are used , the adc value can be overestimated owing to the t2 tissue component and perfusion adding to the pure diffusion value of water molecules . 
conversely , the use of high b - values ( > 1 , 000 s / mm2 ) produces extremely noisy images due to the short t2 value of abdominal tissues . a recent paper by shimofusa et al . 
unlike other reports investigating the use of dwi for prostate cancer detection , the study identified cancerous tissue based on its hyperintense signal on images with b - value = 1 , 000 , without the production of adc maps because of the lower signal - tonoise ratio ( snr ) and poorer image quality generated by the high diffusion weighting [ 9 ]  . in our study , in order to quantitatively evaluate the reduction in apparent diffusion coefficient , we decided to use a maximum b - value = 500 and to produce adc maps based on the good snr . 
a useful expedient to obtain good - quality images with high diffusion weighting was to acquire the sequence with different b - values ( 0 , 125 , 250 , 375 and 500 )  . the adc map was obtained from the data acquired with the individual b - values . an additional problem in assessing prostate adc values lies in the heterogeneity of its parenchyma ; this is especially true of its central portion , which , whether normal and adenomatous , is often the site of cystic and fibrotic - calcific changes related to inflammation . 
the peripheral zone may also undergo structural fibrotic changes related to chronic inflammation ; the differential diagnosis between these changes and cancer is not easy with noninvasive imaging techniques , and often biopsy is required although a radiated rather than nodular appearance and slow wash - in and wash - out following contrast administration are strongly indicative of fibrotic disease . 
to measure the adc values of different portions of the gland , we carefully selected the areas to be sampled and avoided positioning the roi on tissues with calcifications or cysts , whose signals in t2 - weighted sequences are necessarily altered . our series revealed a statistically significant difference between the adc values of the central zone and those of the healthy peripheral zone and , more importantly , a dramatic reduction in the adc values in focal malignant lesions compared with the healthy peripheral zone . 
zonal differentiation within the prostate based on t2 signal intensity and adc values was confirmed by the histological sections exhibiting larger luminal spaces in the peripheral zones , which accounts for the greater concentration and freedom of movement of water molecules in the periphery compared with the centre [ 10 ]  . 
conversely , the marked reduction of adc values in cancerous areas is explained with the replacement of normal tissue , composed of water - rich acinar structures , by cancerous tissue , usually consisting of small components packed into a small amount of stroma : derangement of normal tissue structure is associated with the presence of cellular elements with increased nucleus - to - cytoplasm ratio , resulting in extremely reduced motility of water molecules [ 11 ]  . gate essenzialmente a fenomeni flogistici . 
anche la porzione periferica pu essere sede di alterazioni strutturali di natura prevalentemente fibrotica , legate anchesse a fenomeni flogistici cronici , la cui diagnosi differenziale con lesioni di natura neoplastica non cos agevole con le tecniche di imaging non invasive , risolvendosi spesso solo con il prelievo bioptico , anche se un aspetto radiato piuttosto che nodulare e un comportamento contrastografico con wash - in e washout lenti sono fortemente indicativi di patologia fibrotica . per la misurazione dei valori di adc nelle differenti porzioni della ghiandola , stata quindi posta particolare attenzione nella scelta delle aree campionabili evitando di posizionare la roi su tessuto interessato da calcificazioni o cisti , il cui segnale nelle sequenze t2 - pesate risulta inevitabilmente alterato . dalla nostra casistica si riscontrata una differenza statisticamente significativa fra i valori di adc dellarea centrale e della zona periferica sana , ma ancora pi importante la netta riduzione dei valori di adc nelle lesioni focali maligne rispetto alla zona periferica sana . 
la differenziazione regionale allinterno della ghiandola prostatica in base allintensit di segnale nelle sequenze t2 - pesate e ai valori di adc stata confermata nello studio delle sezioni istologiche dalla dimostrazione di spazi luminali di maggiori dimensioni a livello della porzione periferica , che rende ragione della maggiore concentrazione e libert di movimento delle molecole dacqua in questa zona rispetto alla zona centrale [ 10 ]  . 
viceversa , la netta riduzione del valore di adc allinterno di unarea tumorale trova giustificazione nella sostituzione delle strutture acinari ricche di acqua del tessuto normale da parte di tessuto neoplastico , costituito comunemente da un pattern cellulare a piccoli elementi fittamente stipati allinterno di una esigua quantit di stroma : alla perdita della normale architettura tissutale , si associa anche la presenza di elementi cellulari con rapporto nucleo / citoplasma aumentato , quindi con motilit delle molecole dacqua estremamente limitata [ 11 ]  . gi alcuni lavori pubblicati negli ultimi hanno dimostrato la capacit di distinguere tessuto neoplastico sano e canceroso nella regione periferica e di transizione della ghiandola prostatica da parte del dwi con sequenze epi sulla base del valore di adc [ 12 , 13 ]  . 
per aumentare la capacit delle sequenze pesate in diffusione di differenziare regioni distinte , sane e patologiche , della ghiandola prostatica stato fondamentale lutilizzo di sequenze epi con risoluzione spaziale elevata , ottenuta con ladozione di spessori di strato sottili ( 3 mm ) e di fov di piccole dimensioni ( 140 mm2 ) seppur con una matrice di acquisizione ridotta ( 6464 )  . 
per lacquisizione di tale sequenza , stato preferito lutilizzo della bobina di superficie multicanale in sostituzione della bobina endorettale , che abbiamo deciso di non utilizzare a causa degli inevitabili artefatti gi codificati in letteratura oltre che per ridurre il disconfort del soggetto sottoposto allesame [ 14 ]  . la maggiore differenza statistica fra i valori di adc delle lesioni cancerose e del tessuto sano della zona periferica della ghiandola prostatica risultante dalla nostra casistica rispetto a lavori apparsi recentemente in letteratura 1131 g . 
however , to enhance the ability of dwi to differentiate between healthy and cancerous regions of the prostate gland , the use of epi sequences with high spatial resolution , obtained with thin sections ( 3 mm ) and small fov ( 140 mm2 ) , albeit with a reduced acquisition matrix ( 6464 ) , proved essential . 
for this sequence , we decided to use a multichannel surface coil instead of an endorectal coil to avoid the inevitable artefacts already described in the literature and to minimise the subjects discomfort [ 14 ]  . the greater statistical difference between the adc values of cancerous lesions and those of healthy tissue of the peripheral zone observed in our study is likely to be related to the higher spatial resolution of the sequence ( 13.23 - mm3 voxel ) and resulting reduction in partial volume effects when measuring the adc value : sato et al . 
the higher spatial resolution did , however , require a increased number of acquisition averages in the diffusion - weighted sequence , with a resulting time of 4 min 22 s , that is , 1 min 16 s and 1 min longer than the sequences used by sato et al . 
and by hosseinzadeh et al . , respectively , but causing in no case the appearance of motion artefacts in the prostate gland . conclusions our preliminary results suggest that thin - slice diffusionweighted mri can be used to acquire data on tissue characterisation of the different anatomical zones of the prostate gland . 
diffusion - weighted mri also proved to be reliable and reproducible in differentiating normal and cancerous tissue , allowing detection of early changes in the structural organisation of prostatic tissue . 
comparative studies on adc values of cancer tissue with fibrotic areas or with localised , especially granulomatous , prostatitis will be of great assistance in understanding the real value and possible role of diffusion - weighted sequences in the noninvasive characterisation of structural alterations in the peripheral zone . 
although larger series are needed to confirm the difference between the adc values of benign and malignant lesions , our study suggests that diffusion - weighted mri could be used to integrate the standard prostate imaging protocol , adding only a few minutes to the total mri examination time . 1132 verosimilmente legata alla maggiore risoluzione spaziale della sequenza utilizzata ( voxel di 13 , 23 mm3 ) , e alla conseguente riduzione degli effetti di volume parziale durante la misurazione del valore di adc : sato et al . 
 [ 12 ] per differenziare il tessuto sano da quello canceroso mediante il valore di adc hanno proposto una sequenza con fattore b di 0 - 300 - 600 , matrice di 119192 e fov di 250 mm2 , ma uno spessore di strato di 7 mm con voxel risultante di 2 , 11 , 37 mm ( 19 , 11 mm3 ) , utilizzando una bobina di superficie [ 12 ] ; mentre hosseinzadeh et al . 
 [ 13 ] per lo stesso fine hanno proposto una sequenza con fattore b di 0 - 1000 , matrice di 8080 , fov di 200 mm2 e spessore di strato di 3 mm con voxel risultante di 2 , 52 , 53 mm ( 18 , 75 mm3 ) , utilizzando una bobina trans - rettale insieme ad una bobina di superficie per la pelvi per aumentare il rapporto segnalerumore e consentire la costruzione di mappe di adc con lutilizzo di sequenze maggiormente pesate in diffusione [ 13 ]  . 
la maggiore risoluzione spaziale ha comportato tuttavia la necessit di aumentare il numero delle medie di acquisizione della sequenza pesata in diffusione con un tempo risultante di 4 minuti e 22 secondi , nettamente superiore a quello delle sequenze utilizzate da sato et al . 
 [ 12 , 13 ] , rispettivamente di 1 minuto e 16 secondi e di 1 minuto , senza tuttavia determinare in nessun caso la comparsa di artefatti da movimento a livello della ghiandola prostatica . conclusioni i nostri risultati preliminari indicano la possibilit di poter utilizzare le sequenze rm di diffusione a strato sottile per acquisire dati sulla caratterizzazione tissutale delle differenti regioni anatomiche della ghiandola prostatica . 
la diffusione in rm inoltre risultata essere una metodica affidabile e riproducibile per differenziare il tessuto prostatico normale da quello neoplastico , riuscendo a distinguere cambiamenti precoci nellorganizzazione strutturale del tessuto prostatico . 
studi comparativi sui valori di adc del tessuto neoplastico con aree fibrotiche o con localizzazioni di prostatite , soprattutto nella sua variante granulomatosa , saranno di grande ausilio per capire leffettiva utilit e il possibile ruolo delle sequenze pesate in diffusione nella diagnostica non invasiva di natura delle alterazioni strutturali della porzione periferica . 
inches2 1dipartimento di scienze oncologiche e chirurgiche , sezione di senologia , universit degli studi di padova , via gattamelata 64 , i - 35128 padova , italy 2dipartimento di scienze medicodiagnostiche e terapie speciali , universit degli studi di padova , via giustiniani 2 , i - 35128 padova , italy correspondence to : l . 
practical aspects with psychological and clinical involvement are discussed with tree diagrams . key words human error perception interpretation system riassunto viene proposto un approccio sistematico allerrore umano nella diagnostica per immagini ( di ) , riconoscendo la sua collocazione nelle attivit personali della percezione e della interpretazione e nelloperativit globale del sistema . 
nellinquadramento che si sviluppa secondo ramificazioni ad albero sono discussi gli aspetti pratici alla luce di contributi provenienti dagli studi psicologici e dalla evoluzione della realt clinica e sanitaria . parole chiave errore umano percezione interpretazione sistema introduction introduzione the approach to the study of human error in diagnostic imaging ( di ) requires a preliminary introduction regarding the concept of error in modern medicine . human error is always placed inevitably in relation with truth [ 1 , 2 ] , which in a strictly scientific field should be considered , as the epistemologist blandino states , as only probable and approximate , connected to theories which change and at times crumble , to be replaced by other , more valid ones . 
it can safely be said that there is currently such a huge quantity of knowledge in medicine and biology that the medical practitioner is increasingly exposed to a great number and variety of errors . traditionally two relevant aspects have been indicated : errors in medicine , considered as the collection of theories regarding health and the state of disease in humans ; for the scientific representation of errors in medicine the statistics and theory of bayes [ 3 ] are used medical practitioners errors , in that as humans . 
they are subject to making mistakes according to a distinction made by epistemologists , the term mistake is more accurate for errors related to the activity in which theoretical notions are applied whereas errors in the lapproccio allo studio degli errori commessi dalluomo nella diagnostica per immagini ( di ) impone una preliminare introduzione sulle connotazioni che il concetto di errore assume nella moderna attivit medica . lerrore da sempre messo inevitabilmente in rapporto con la verit [ 1 , 2 ] che in ambito strettamente scientifico da intendersi , come indica lepistemologo blandino , come soltanto probabile e approssimata , connessa a teorie che si modificano e talora crollano , sostituite da altre pi valide : anche le verit diagnostiche sono quindi relative e commisurate al sapere di un determinato tempo . 
non vi dubbio che allo stato attuale via sia una tale mole di conoscenze in medicina e biologia che si pu tranquillamente affermare che loperato del medico sempre pi esposto ad errori , molteplici e di varia natura . tradizionalmente se ne indicano due aspetti rilevanti : gli errori della medicina , considerata come insieme di teorie che riguardano la salute e lo stato di malattia delluomo , per la rappresentazione scientifica dei quali ci si avvale soprattutto della statistica e del teorema di bayes [ 3 ] ; gli errori dei medici , in quanto essere umani e come tali soggetti a sbagliare . secondo una distinzione degli epistemologi , proprio il termistrict sense regard science as such . 
in this paper , the term error will be used for simplicity , even if in reference to mistakes . medical tradition also commonly makes a distinction between two reference errors : cognitive : concerning diagnosis and prognosis operative : concerning decision making and therapy di is slightly removed from this picture , as the use of perception is particularly relevant but also because given the progressive expansion of the discipline , the search for errors needs to be placed in an organized and technologically advanced context , with a much broader range of devices than in the early days of the first applications of the coolidge tube when medicine was almost totally reliant on the personal abilities of the practitioners . like other fields , such as nuclear engineering or aviation [ 4 , 5 ] , a radiology department stands out for its organizational and operative peculiarities as a system , with features similar to any company such as logistics , finance and the hiring and training of personnel . 
some errors may be present in the planning and organizational phase such that reason and rasmussen [ 6 ] classifies them as latent errors with delayed effects and differentiates them from active errors in which there is a momentary and welldefined participation by the operator . 
seeking out these remote errors is an important feature of the modern management of the radiology department because when they appear , the operator is in fact programmed to make a mistake . 
the operator is the victim of a mediocre project , insufficient maintenance , inappropriate materials and managerial decisions which create situations of risk , such as unrealistic workloads , inappropriate training or exasperating turnaround times . 
since the error appears with the last operator , whether he or she is the direct or indirect cause , all errors should be considered human error and in di the radiologists error . in this context the aim of this study was to unify the problems and the causes of errors , taking into consideration the crucial moment of image assessment in radiology when the radiologist utilizes the characteristics of his or her personality , culture and training [ 7 ]  . characteristics of the radiologists activities the radiological act as it currently stands can be defined as a technical - methodological procedure performed on a patient in an organizational and decision - making system , the outcome of which is the image obtained to achieve diagnosis . 
it is here , in fact , that to reach a decision , the radiologist makes use of a process of perception and cognition , features which occur simultaneously and are interdependent , and yet , as wood [ 8 ] notes , are separate mental activities . 
inches : systematic approach to human error in radiology ne sbaglio pi corretto ad indicare gli errori inerenti alle attivit in cui le nozioni teoriche sono applicate , mentre gli errori in senso stretto riguardano la scienza come tale . nellelaborato il termine errore sar usato per comodit e consuetudine , anche se riferito agli sbagli . ancora nella tradizione medica si soliti configurare due errori di riferimento : cognitivo : concerne la diagnosi e la prognosi ; operativo : concerne gli aspetti decisionali e la terapia . la di se ne discosta parzialmente essendo per essa rilevante lapporto della percezione , ma anche perch , nella progressiva espansione della disciplina , la ricerca dellerrore va inquadrata in un contesto organizzato e tecnologicamente avanzato , che prospetta tipologie pi ampie rispetto allepoca artigianale delle prime applicazioni del tubo di cooledge , coeve ad una medicina legata alle pressoch assolute capacit personali dei medici . la radiologia , intesa quale servizio o unit operativa che dir si voglia , analogamente ad altre strutture di lavoro , come lingegneria nucleare o laviazione [ 4 , 5 ] , si identifica allo stato attuale per peculiarit gestionali e operative come sistema , al quale sono attribuiti analogamente a qualsiasi azienda almeno gli ambiti organizzativi della logistica , della finanza , dellassunzione e della preparazione del personale . il sistema come tale pu essere sottoposto ad analisi e verifica ai fini della ricerca degli errori e della loro correzione mediante procedure adatte . alcuni errori possono essere gi insiti in fase di progettazione e organizzazione , tanto che reason [ 6 ] li classifica come errori latenti , con effetti ritardati , differenziandoli dagli errori attivi in cui vi una partecipazione momentanea e bene circostanziata delloperatore . 
la ricerca di questi errori remoti rappresenta allora uno dei punti notevoli della moderna conduzione del reparto , perch , quando compaiono , loperatore in realt stato programmato per sbagliare : egli vittima ultima di un progetto mediocre , di una manutenzione insufficiente , di materiali inidonei , di decisioni della dirigenza che si esplicano in situazioni di rischio , quali ad esempio gli irrealistici carichi di lavoro , laddestramento non adeguato o i tempi di produzione esasperati . 
poich di fatto lerrore si manifesta nelle circostanze con lultimo operatore , ne sia egli la causa diretta o indiretta , tutti gli errori in definitiva debbono essere considerati riferiti alluomo : per la di al radiologo . sotto questo profilo lo scopo del lavoro di unificare problematiche e cause di errore prendendo in considerazione nella di il momento cruciale della valutazione del documento , allorquando il radiologo partecipa mettendo in campo le proprie caratteristiche di personalit , cultura e preparazione [ 7 ]  . caratteristiche dellattivit del radiologo latto radiologico allo stato attuale pu essere definito come procedura tecnico - metodologica condotta sul paziente , avvenuta in un sistema organizzativo - decisionale , che si esprime nel documento dimmagine ottenuto per conseguire il fil . 
inches : systematic approach to human error in radiology mental phenomena at play is required : the phenomenon of perception the perceptual process transforms retinal stimulation at the higher centres into conscious perception , allowing images to be extracted and translated in conscious assessment by simplifying and organizing the information from the peripheral regions . 
according to attneave , quoted by wood [ 8 ] , this process is limited , not being sufficiently capable in the sense of capacity to transmit all information which reaches the retina . 
hake , also cited by wood [ 8 ] , instead believes that perception is governed by the centre in that it is linked to the search for a meaning connecting the fragmentary retinal images . 
in fact , the meaning and even the writing of a sentence itself may be considered absolutely precise even though obvious errors may be found when the text is carefully revised [ 9 ]  . 
lastly , it is worth noting that perception is substantially different from simple vision , in which only the peripheral activities of the observer take part in relation to the nervous system . the phenomenon of cognition the cognitive part of diagnostic decision making is less well known yet fascinating , given the models proposed for explaining the mental stages which lead to a conclusion . 
qui , infatti , che il radiologo si avvale di un procedimento percettivo e conoscitivo , simultanei e interdipendenti , da considerare tuttavia con wood e tuddenham [ 8 ] come attivit psichiche separate , per giungere ad una decisione . 
per rendere comprensibile e al tempo stesso unitaria la classificazione a seconda della tipologia e delle cause di errore indispensabile un richiamo sintetico alle conoscenze dei fenomeni psichici in gioco . il fenomeno della percezione il processo percettivo trasforma in percezione cosciente i modelli della stimolazione retinica ai centri superiori ; consente di estrarre immagini e di tradurle in valutazione conscia , mediante una semplificazione e organizzazione delle informazioni provenienti dalla periferia . 
secondo atteneave , citato da wood [ 8 ] il processo limitato , non essendo sufficientemente capace , nel senso proprio di capiente , per trasmettere tutte le informazioni che raggiungono la retina . hake , pure citato da wood [ 8 ] ritiene invece che la percezione sia diretta dal centro in quanto legata alla ricerca di un significato che colleghi le frammentarie immagini retiniche . 
per la lettura ; i rettangoli indicano le conoscenze che dallalto in basso divengono via via pi profonde ; in un caso clinico linterprete potrebbe trascurare leziologia di un broncogramma , ad esempio metastasi polmonari , se lattivazione particolarmante frequente per le cause infettive . pointed out that classic cognitivism recognizes the diagnostic process as inductive reasoning aimed at identifying rules and categories , beginning with concrete examples : the dialogue between the areas of research of concrete examples ( variable features ) and rules ( fixed features ) leads to the selection of facts , to remembering the theories based on the facts and to test the hypotheses . 
the classic model , however , has the defect , particularly for medical applications , of overlooking the concrete and pragmatic aspects , in essence , situations such as emergencies in which the examinations are necessarily limited owing to time constraints . 
 the most complete and appropriate model for our purposes which explains the relationship between real facts and the examination of the mind is the model proposed by raufaste and eyrolle [ 10 , 11 ] in 1998 . 
long - term memory has an enormous capacity for storage and contains declarative knowledge ( theory ) and procedural knowledge ( know - how ) interconnected by various types of logical systems in an active for for example , the processes of classification of part / whole relations become increasingly rapid in acquisition times as the knowledge is implemented and interconnected . 
generally speaking , by bringing ones attention to a certain level of knowledge , that level is activated , and once more overcoming a certain threshold , awareness is achieved . working memory involves a variety of aspects , including phonological , visual and spatial . 
infine da osservare come la percezione si differenzi in modo sostanziale dalla semplice visione , al cui fenomeno partecipano solo le attivit periferiche dellosservatore in rapporto alle caratteristiche del sistema nervoso . il fenomeno cognitivo la parte cognitiva della decisione diagnostica meno conosciuta , affascinante per i modelli proposti a spiegare le tappe mentali che portano alla conclusione . 
premesso che lambito mentale molto ampio e a margini poco definiti , doveroso accennare come il cognitivismo classico riconosca il procedimento diagnostico come ragionamento induttivo teso ad identificare regole e categorie partendo da esempi concreti : il dialogo fra gli spazi di ricerca degli esempi concreti ( tratti variabili ) e delle regole ( tratti fissi ) conduce a selezionare i fatti , a ricordare le teorie a partire dai fatti e a verificare le ipotesi . 
il modello classico ha per il difetto , soprattutto per le applicazioni mediche , di trascurare gli aspetti concreti e pragmatici , in sostanza le situazioni , ad esempio le emergenze , in cui le indagini sono necessariamente limitate per motivi di tempo . 
per spiegare meglio il rapporto tra fatti reali e lindagine della mente risulta pi completo e adatto alle nostre esigenze , perch dedicato alla radiologia , il modello del francese roufaste del 1998 [ 10 , 11 ]  . 
la memoria a lungo termine ha vasta possibilit di stoccaggio ed duratura nel tempo : contiene le conoscenze dichiarative ( del sapere teorico ) e procedurali ( del saper fare ) interconnesse da diversi tipi di sistemi logici in forma attiva . 
cos ad esempio i processi di classificazione o di relazione parte / tutto divengono sempre pi rapidi nei tempi di acquisizione mano a mano che tali conoscenze sono implementate e interconnesse . 
unlike long - term memory , which is activated autonomously and without the intervention of the conscious , working memory highly depends on the attention system capable of authorizing the implementation of higher functions , such as symbolic calculations or the decision to implement or inhibit automatisms [ 10 , 11 ]  . 
 analysis of radiographs involves the fundamental function of working memory , that is , the maintenance of a representation constructed from empirical data , in our case from the characteristics of the radiographs , and from information recalled from long - term memory , which we could call experience . 
la memoria di lavoro ha apporti differenti , anche fonologici , visivi e spaziali ; permette di stoccare un numero piccolo di informazioni ( da 3 a 7 indipendenti una dallaltra )  . 
la risoluzione di problemi complessi , come quello della valutazione dei radiogrammi , abbisogna di parametri molto pi numerosi : il problema risolto con lassociazione nella memoria di lavoro di pi sottoinsiemi , che sono trattati come singole unit . 
contrariamente alla memoria a lungo termine , che attivata autonomamente e senza lintervento della coscienza , la memoria di lavoro dipende fortemente dal sistema attenzionale in grado di autorizzare la messa in opera di funzioni superiori come il calcolo simbolico , la decisione di una gestione o linibizione degli automatismi [ 10 , 11 ]  . 
ai fini dellosservazione dei radiogrammi interviene la funzione fondamentale della memoria di lavoro ovvero il mantenimento di una rappresentazione , costruita a partire dai dati empirici , nel caso nostro dalle caratteristiche dei radiogrammi , e da informazioni recuperate dalla memoria a lungo termine , che in modo arbitrario , ma di immediata acquisizione potremmo chiamare esperienza . 
knowledge - based activity : the diagnostic process is guided by analytical reasoning , in the awareness of already stored knowledge , to tackle new situations , which require a considerable application effort . human error in diagnostic imaging : types and causes having introduced the areas of human activity where errors may occur , the causes may now be sought in the three major groups of error : ( 1 ) perceptual errors , ( 2 ) cognitive errors and ( 3 ) system errors . 
these are summarised in figure 3 . the scientific principle of assessment is also valid for human error , that is to say , that similar to the bayes formula , errors are either false positives or false negatives . 
la diagnostica orientata da un ragionamento analitico , nella consapevolezza di un bagaglio di conoscenze gi immagazzinate , per far fronte a situazioni nuove , che richiedono quindi uno sforzo applicativo non comune . according to berlin [ 12 ] , 70% of lawsuits brought against radiologists are related to the non - identification of radiological signs , 60% of which are due to perceptual errors . with regard to the causes , a distinction is made between errori umani nella di : tipologie e cause introdotti gli ambiti delle attivit umane in cui avviene lerfig . 
inches : systematic approach to human error in radiology rore , possibile ricercarne le cause nei tre grandi insiemi : ( 1 ) linsieme degli errori percettivi , ( 2 ) linsieme degli errori cognitivi , ( 3 ) linsieme degli errori del sistema . 
per gli errori di sistema o latenti qui ribadito che lerrore umano di ripercussione , essendo la causa antecedente al momento dellavvenimento , gi radicata nel sistema organizzativooperativo . errori percettivi secondo berlin il 70% [ 12 ] delle pratiche legali contro i radiologi connesso ad una non identificazione di segni radiologici , con un contributo del 60% degli errori percettivi . quanto alle cause , si distinguono errori di identificazione con errata attribuzione ed errori di non identificazione . errori di identificazione con errata attribuzione sono errori poco frequenti : si verificano allorquando il radiologo segnala una lesione che non sussiste , scambiando ad esempio un reperto normale con uno patologico . 
barbaum [ 13 ] riporta , ad esempio , che nella ricerca di un corpo estraneo per la presunta ingestione di un bottone da parte di un bimbo di 1 anno in un radiogramma standard del torace , un radiologo ha malamente interpretato un nucleo di ossificazione sternale attribuendolo al bottone . 
le verifiche endoscopiche e il pasto opaco hanno dimostrato linconsistenza dellaffermazione . come gi osservato sono gli errori pi frequenti : il riconoscimento postumo di un nodo polmonare sul radiogramma del torace la situazione pi nota . 
questa possibilit di errore risulta chiara se ci si cimenta con i disegni paradossali di esher o con il libro per bambini di handford the great waldo [ 14 ]  . 
nellultimo libro , i bambini sono sfidati a trovare il mostriciattolo waldo nascosto tra mille disegni : difficile da riconoscere , ma una volta scoperto o rifugiatisi nelle soluzioni , alla fine la sua inconfondibile sagoma e la relativa posizione risultano ovvie . 
nellesempio la percezione fortemente influenzata dalle aspettative ; perci trovare waldo pi semplice che vedere un piccolo nodo polmonare sul radiogramma toracico , perch waldo sicuramente c , mentre per il nodo polmonare non abbiamo indizi . 
 [ 13 ] report an example in the search for a foreign body in a standard chest x - ray due to the presumed ingestion of a button by a 1 - year - old child . 
endoscopic examinations and an opaque bolus proved the affirmation incorrect . non - identification errors these are the most frequent kinds of errors , with the late recognition of a pulmonary node on a chest x - ray being the most common situation . 
the possibility of making this kind of error is clear if one tests oneself with the paradoxical drawings of escher or with the childrens books by handford wheres wally ? [ 14 ]  . 
in one of the most recent books , children are challenged to find wally hidden among hundreds of figures ; he is extremely difficult to recognize , but once identified his , unmistakable outline and his position are in the end obvious . 
in this example , perception is strongly influenced by expectations , so that finding wally is much easier than identifying a small pulmonary nodule on a chest x - ray because wally is definitely there while a pulmonary nodule may or may not be present . 
with regard to errors in this activity , kopans and daniel [ 15 , 16 ] note cases reported by psychologists of the difficulty and frustration of contingent situations often present in daily life , such as the fruitless search for a bunch of keys which we are unable to see but need to get into our house . 
the example can easily be related to a mammographic sign indicated by a colleague or recognized at a later time . specific causes as well as non - describable factors , the erroneous perception that leads to the non - identification on radiographs is connected to specific , numerous and heterogeneous causes . 
indeed , the final error is perceptual , but the complexity of mental behaviour is such that causal factors which are a part of technical and cognitive features play a part . 
with reference to berlin [ 18 ] , in one case of non - identified pulmonary nodule , the judicial assessment commission admitted that the lesion was difficult to diagnose since the x - rays were overexposed , thus suggesting the responsible error . 
the difficulty of diagnosing lesions at the level of the last cervical and first thoracic vertebrae is also well known , particularly in trauma patients , unless an optimal patient position is found . 
berlin [ 18 ] reports the case of a patient who fell from a ladder and underwent radiography of the cervical vertebrae on three separate occasions owing to the persistence of symptoms . 
unfortunately , the lesion identified on a later occasion in another hospital was a fracture / luxation of c6 - c7 , with the patient ending up a permanent quadriplegic . 
inches : systematic approach to human error in radiology screening : in quello mammografico infatti notevole la variabilit anatomica , spesso la struttura di difficile analisi , e il numero di casi da interpretare pu essere enorme . 
per gli errori in questa attivit kopans [ 15 , 16 ] ricorda , su segnalazione degli psicologi , le difficolt e le frustrazioni delle situazioni contingenti spesso presenti nella vita quotidiana , come la ricerca infruttuosa di un mazzo di chiavi , che non siamo in grado di vedere , ma che sono necessarie per entrare in casa . 
lesempio si ricollega con facilit ad un segno mammografico indicato da un altro operatore o riconosciuto in tempi successivi . cause specifiche oltre a fattori non descrivibili , lerrata percezione che porta alla non identificazione sui radiogrammi connessa a cause specifiche , numerose ed eterogenee . 
le tipologie sono indicate in figura 4 . gli errori tecnici [ 17 ] sono bene esemplificati dalla lesione non vista per sovra o sottoesposizione o per errato posizionamento del paziente . 
con riferimento a berlin [ 18 ] , in un caso di nodulo polmonare non visto , la commissione di valutazione giudiziaria ammise che era difficile diagnosticare la lesione perch le radiografie erano sottoesposte , sottintendendo cos lerrore responsabile . 
sempre berlin riporta il caso di un paziente , caduto dalle scale di casa e sottoposto a radiografie della colonna cervicale in tre fasi diverse , a causa di una persistente sintomatologia : il primo esame identific le prime 4 vertebre cervicali , il secondo dimostr anche c5 con sole note artrosiche . 
the anomalies outside the privileged area of the examination are not infrequent and include thoracic lesions identified during an abdominal examination ; or pleural , pulmonary or mediastinal lesions incidentally encountered during a radiological study of the spine , thoracic bones or shoulder girdle . 
in a litigation caused by lack of identification of an arteriovenous malformation of the bone marrow , berlin [ 19 ] underlines the difficulty of establishing whether the error was due to non - perception or lack of knowledge by the radiologist , and such difficulties can be extended to other cases . the attempt to explain non - identification with other causes dates back to the 1960s and the work of several authors , such as smith and tuddenham , which was later commented by wood , and raufaste and eyrolle [ 8 , 10 , 11 ] : several lesions were not identified owing to another lesion present in the image which had caught the attention of the radiologist . 
following the same line of research , berbaum [ 20 ] investigated the phenomenon on his own colleagues , introducing an artificial nodular lesion in chest x - rays already marked by original lesions . 
he defined this perceptual error satisfaction of search , thus recognizing the argument of cognitive psychologists who note that radiologists tend to be satisfied after finding a lesion , and if they continue the assessment of the image , it is only to restrict the field of study to what they have identified . the quantity of perceptual errors varies according to the examination in question . 
 [ 21 ] , in an interval of 16to 40 - mm nodules , recognized a minimum error of 20% ! in a specific study on the efficiency of health services , watcher et al . 
 [ 22 ] reports similar types of errors in other organs and systems recognized by other researchers : the errors in emergency situations have a low percentage of 3%6% ( robin ) , the sensitivity of identifying ureteral stones , many of which are recognizable a posteriori , is 46% ( levine ) and the error rate in contrast enema is 15% ( wesses )  . a first critical examination of perceptual errors , in the light of case series and studies which go beyond the individual case with legal implications , demonstrates that the real difficulty is the error without specific cause . 
it should be toracica individuata in corso di addome diretto , o ancora le lesioni pleuriche , polmonari o mediastiniche incidentalmente comparse in corso di studio radiografico della colonna vertebrale , delle ossa del torace o del cingolo scapolare . 
berlin in un suo articolo , in un caso di contenzioso per la mancata individuazione alla mielografia di una malformazione arterovenosa del midollo spinale [ 19 ] , sottolinea che vi sono concrete difficolt a stabilire se nel caso lerrore fosse dovuto alla non percezione o alla scarse conoscenze del radiologo e che tali perplessit sono da estendere ad altre evenienze . il tentativo di spiegare la non identificazione con ulteriori cause risale agli anni 60 con le osservazioni di alcuni autori , quali smith e tuddenham , raccolte e commentate successivamente da wood e raufaste [ 8 , 10 , 11 ] : alcune lesioni potevano non essere individuate a causa di unaltra lesione presente nel documento che aveva catturato lattenzione del radiologo . 
berbaum [ 20 ] nello stesso filone di ricerca ha indagato il fenomeno con i propri collaboratori , introducendo una lesione nodulare artificiale nei radiogrammi del torace gi interessati da altre lesioni originali : lidentificazione di queste ultime , per il disturbo delle altre , diminuiva in modo significativo . 
egli ha chiamato un tale errore percettivo satisfaction of search , riconoscendo la tesi degli psicologi cognitivisti che notano che i radiologi tendono ad essere soddisfatti dopo la ricerca di una lesione e proseguono semmai oltre solo restringendo il campo dindagine su ci che hanno visto . in termini applicativi la quantit di errori percettivi varia a seconda delle indagini in questione . 
interessante notare come in una revisione della casistica personale di radiogrammi del torace e nel confronto con altri autori , quekel [ 21 ] riconosca in un intervallo da 16 a 40 mm delle dimensioni dei noduli un errore minimo del 20% ! in uno studio specifico sullefficienza delle prestazioni sanitarie watcher [ 22 ] riporta analoghe tipologie di errore relative ad altri organi ed apparati riconosciute da altri ricercatori : gli errori in emergenza hanno percentuali minime del 3%6% ( robin ) ; la sensibilit di rilevamento dei calcoli ureterali , molti dei quali riconoscibili a posteriori , del 46% ( levine ) ; la quota derrore nel clisma opaco del 15% ( wesses )  . una prima considerazione critica sugli errori percettivi , alla luce di casistiche e studi che esulano dal caso singolo con risvolti giudiziari , mette in evidenza come il vero rebus sia lerrore senza specifica causa . 
 [ 23 ] hanno studiato gli effetti della doppia e tripla lettura su un campione di 60 casi di clisma opaco a doppio contrasto , in cui erano presenti 46 lesioni . 
the radiologist is aware of the routine and surrounding working conditions ; a temporary loss of attention causes the slip , which may be considered a small monitoring error . a ( perceptual ) error caused by capture occurs when the radiologists attention is attracted by a sign and is satisfied by this first finding , using a more common working framework rather than a less common one . alongside this type of slip is one in which the error is so obvious that it is known as a description error . 
it is an error characteristic of reporting when a semantic field related to one technique is used to describe another , for example , a ct study described with echogenicity - based terminology , or an ultrasound described with density - based terminology . other slips , such as associative activation ( answering the telephone when the doorbell rings ) or loss of activation , described as the temporary loss of memory while performing a precise task ( the search for an object ) , appear to be circumstantial , more common with the use of high - tech equipment or procedures , and can immediately be made up for . 
therefore , performing tasks without disturbances or distractions is the best prevention for this type of error . in contrast , a series of factors of various natures may help create situations which foster the occurrence of slips . 
the most common psychological elements include fatigue , loss of sleep , alterations caused by alcohol or drugs , or emotional states such as boredom , frustration , fear , anxiety or anger all conditions which cause concern and distract ones atl . 
inches : systematic approach to human error in radiology errori cognitivi gli errori della fase cognitiva sono stati classificati da reason e rasmussen [ 6 ] con il riferimento ad ogni livello attenzionale come basati sulla capacit intellettiva ( skill based ) , sul metodo cognitivo ( rule based ) e sulla conoscenza ( knowledge based )  . 
errore caratteristico nella refertazione quando si utilizzi una semantica relativa ad una metodica per descriverne unaltra : ad esempio , un referto con terminologia basata sullecogenicit per unindagine tc o invece sulla densit per unecografia . altre sviste quali lattivazione di associazioni ( associative activation ) come rispondere al telefono quando suona il campanello o la mancanza dattivazione ( loss of activation ) ovvero la temporanea perdita di memoria in corso di unazione ben precisa , come la ricerca di un oggetto , appaiono circostanziali , pi frequenti nel corso dimpiego di tecnologie o procedure , e di solito dimmediato recupero . tuttavia va sottolineato come le sviste sono spesso causate da interruzioni di precedenti attivit che erano in atto . pertanto lo svolgimento dellattivit senza disturbi e distrazioni la migliore prevenzione per tali tipologie derrore . per contro , una serie di fattori di diversa natura pu innescare situazioni favorevoli alle sviste . 
gli elementi psicologici pi frequenti comprendono la fatica , la perdita di sonno , le alterazioni da alcool o droghe oppure stati emozionali , quali la noia , la frustrazione , la paura , lansia , la collera , tutte condizioni che conducono alla preoccupazione che distrae lattenzione . a queste condizioni possono contribuire altri fattori esterni quali leccesso di lavoro e le relazioni interpersonali difficili o ambientali come il rumore , la calura , stimoli visivi eccessivi . 
in addition to these conditions , there may also be external factors , such as an excessive workload , difficult interpersonal relations or an unfavourable working environment characterised by excessive noise , heat or visual stimuli . in di , therefore , a large number of slips can be the result of working environments inappropriate for the study of radiographic images , excessive workloads , difficult conditions in the department and so on . rule - based and knowledge - based errors errors related to the two cognitive activities , commonly known as psychological errors , have been studied less than others and are more difficult to assess . 
these errors are due to an erroneous assessment of a contingent situation for which an incorrect procedure is applied . figure 5 shows how those errors , more correctly defined mistakes , are both recognition and decision making in nature . 
mistakes are therefore specifically cognitive errors , distinct from the more general term errors , which includes all types and therefore perceptual and system errors as well . figure 5 also shows how recognition errors are usually based on the most commonly used reasoning , adopted due to mental laziness on the part of the radiologist who has trouble breaking from known and repeated implementation models . included with this mental laziness or preconceived positions are mistaken choices , which piattelli - palmarini [ 24 ] defines deadly sins and which are summarized in figure 5 and outlined here below : biased memory leads to overgeneralizations of the ordinary or undergeneralizations of facts due to emotive reactions connected with personal success or contradictory experiences . heuristic availability prompts us to use only the primary information which comes to mind . confirmation bias supports our working hypotheses , causing us to ignore all contradictory information . overconfidence leads us to overestimate ourselves and our own abilities . anchoring highlights the influence that our first impression , or first judgement , has and how it becomes impossible to completely suppress it in later revisions . probability blindness refers to the mental procedure incapable of taking into consideration probabilistic estimates . it is so dangerous that piattelli - palmarini warns that any probabilistic intuition of any person not specifically versed in probability calculations has more than 50% probability of being incorrect [ 24 ]  . reconsideration under suitable scripts , lastly , is the seventh of the mental procedures which lead to cognitive errors . 
it is thought that a type of event or situation is judged all the more frequently the easier it is to mentally imagine and the greater the emotional impact it has as well as the more our judgement of probability is biased by the scripts . together with these seven deadly sins of the mind are two inevitable corollaries , situations contingent to the work phases : errori nellambito dellattivit basata sulle regole ( ruled based activity ) e dellattivit basata sulla conoscenza ( knowlodge based activity ) gli errori inerenti le due attivit cognitive , denominati comunemente psicologici , sono i meno studiati e i pi difficili da inquadrare : spesso sono identificabili pi cause che insieme contribuiscono allerrore . 
la figura 5 evidenzia ancora come lerrore di riconoscimento si basi di solito sul ragionamento usato pi frequentemente , cui si ricorre a causa della pigrizia mentale del radiologo , che stenta a staccarsi da schemi applicativi noti e ripetuti . 
clinical information may play a determining role in this assessment . before taking into consideration this aspect , which is fundamental in daily practice , it is worth noting the three main types of error in di associated with mental tunnels , as proposed by fitzgerald [ 26 ] : availability bias : the ease of remembering a diagnosis specific to the case compromises the possibility of making a correct diagnosis . regret bias : a distorted probability of diagnosis influences the correctness in the unconscious desire that something regrettable occurs . framing bias : the frame of the examination ( the request , case history , etc . ) unduly influences the report . a study in 1992 by norman et al . 
the first phase of the experiment involved 50 radiologists called on to assess 50 radiographs 25 from patients affected by bronchiolitis and 25 from normal patients with the radiologists being asked to search for signs of disease such as hyperinsufflation , bronchiolar thickening and perihilar opacities . the signs were found in both diseased and healthy patients in compliance with the suggested provisional diagnosis . 
in the second phase of the experiment , the radiographs were accompanied with a brief clinical history of normality or pathology , and three radiologists were specifically asked what the real probability of bronchiolitis was . the experiment showed the consistent effect of the clinical history on both attribution of a diagnostic category and the radiological signs on uncertain radiographs . 
at any rate , there is no doubt that knowledge of clinical history and signs regarding physical examination increase the possibility of radiological interpretation . further useful information can be gleaned from a comparison of previous radiological studies performed on a patient , as studied by berbaum et al . 
 [ 28 ] and berlthe american college of radiology has included the procedure among the published quality standards , stating that comparison with relevant previous examinations and reports should be part of the radiologic consultation and report when appropriate and available . 
inches : systematic approach to human error in radiology centrarsi su una sola fonte dinformazione ; il capovolgimento sotto affaticamento ( reversion under stress ) il fenomeno nel quale i comportamenti appresi di recente sono sostituiti con altri pi vecchi , ma pi familiari anche se inadatti al problema in esame . 
gli errori di riconoscimento avvengono quando una anomalia vista dal radiologo , ma non apprezzata come tale ; in realt riconoscere unanomalia richiede pi una memoria visiva che unacuit visiva . 
le informazioni cliniche possono giocare un ruolo determinante in questo giudizio . prima di prendere in considerazione tale aspetto , fondamentale nella pratica quotidiana , vale la pena di riportare da fitzgerald [ 26 ] i tre principali tipi di errore nella di connessi ai tunnel mentali : influenza della memoria ( avaibility bias ) : la facilit di ricordare una diagnosi specifica al caso pregiudica la possibilit della diagnosi corretta ; influenza emotiva ( regret bias ) : una distorta probabilit di diagnosi influenza la correttezza , nellinconscio desiderio che avvenga qualcosa che dispiace ; influenza del contorno ( framing bias ) : la cornice dellesame ( richiesta , anamnesi etc ) influenza eccessivamente il referto . a tale riguardo uno studio di norman del 1992 [ 27 ] dimostra empiricamente limportanza delle informazioni cliniche . 
lesperimento riguarda 50 radiologi esperti chiamati a valutare in una prima fase 50 radiogrammi , 25 di pazienti affetti da bronchiolite e 25 normali , chiedendo loro di ricercare i segni della malattia quali iperinsufflazione , ispessimento bronchiolare , opacit perilari . 
in una seconda fase stato chiesto esplicitamente ai tre radiologi quale fosse in ogni radiogramma , cui era stata aggiunta una breve storia clinica di normalit o di patologia , la probabilit reale di bronchiolite . 
a livello operativo nessuno osa in ogni caso mettere in dubbio che la conoscenza della storia clinica e dei segni relativi allesame obiettivo aumentino le possibilit dinterpretazione radiologica . altre informazioni utili possono ancora essere desunte dal confronto con i precedenti studi radiografici eseguiti sul paziente , come sperimentato da berbaum e berlin [ 28 ]  . lamerican college of radiology ha posto la procedura tra gli standard di qualit pubblicati affermando che il confronto con gli esami precedentemente eseguiti dal paziente , quando possibile , parte integrante dellindagine radiologica l . 
inches : systematic approach to human error in radiology space and time can be resolved with the picture archiving communication system ( pacs ) [ 29 ] which with the storage of digital data ( and therefore not analogical images ) could nonetheless give rise to revisions and evaluations after the fact , both regarding the use of the same in the broadest possible sense and the perception and interpretation of the derived images . if knowledge of the history and a comparison of previous data are valid methods for eliminating the radiologists decision - making errors , then reading previous radiological reports could also prove useful . 
this proposal , however , opens up an important debate regarding alliterative errors [ 30 ] , defined as an erroneous and reiterated diagnosis by several radiologists on the basis of the report of the first radiologist . the first such case reported by berlin [ 30 ] of a case of lung cancer , which on several occasions was labelled as bronchopneumonia , was followed by an important debate . 
the theory of berlin [ 31 ] which states that if a radiologist fails to recognize an anomaly or incorrectly interprets its meaning , then the possibility of the next radiologist repeating the same error is noticeably increased is supported by smith , cited by berlin [ 31 ] , who states that radiologists are induced to read the report of a colleague before assessing the radiograph . 
laspetto relativo allarchiviazione , di difficile applicazione nello spazio e nel tempo , potr essere risolto dai sistemi digitali pacs [ 29 ] , che tuttavia con la memorizzazione dei dati numerici ( non immagini analogiche quindi ) potranno dare luogo a revisioni e giudizi postumi , sia sullutilizzazione degli stessi in tutta la loro ampiezza che sulla percezione e interpretazione delle immagini ricavate . se la conoscenza della storia e il confronto con i dati precedenti sono metodi validi per eliminare gli errori decisionali del radiologo , anche la lettura dei referti precedenti allegati potrebbero rientrare in questa ottica . laffermazione apre tuttavia limportante dibattito relativo allerrore alliterativo [ 30 ] , individuando in questo unerronea e reiterata diagnosi da parte di pi radiologi sulla base del referto del primo radiologo . 
alla prima segnalazione di berlin su un caso di tumore polmonare , in pi circostanze etichettato come broncopolmonite [ 30 ] segu un importante dibattito . la teoria di berlin [ 31 ] che , se un radiologo non vede unanomalia o le attribuisce un significato sbagliato , la possibilit che il successivo radiologo ripeta il medesimo errore notevolmente aumentata sostenuta anche da smith , citato da berlin [ 31 ] , il quale afferma che i radiologi sono portati a leggere il riscontro del collega prima dellapproccio al radiogramma . tuttavia lamerican college of radiology nello standard for communication mette in evidenza che il paragone con precedenti esami e referti , dove possibile , parte integrante dellanalisi radiologica . 
in una successiva revisione berlin [ 32 ] riporta da autori diversi analisi sperimentali in contraddizione , riconoscendo che hunter e boyle dimostrano lutilit nel leggere i precedenti referti nel 60% dei casi e un considerevole aiuto nel 22%24% dei casi , mentre white segnala solo 1 , 5% di utilit e un 48% di inutilit . 
scelta della soglia del sospetto . ferred to for the following discussion . in the strategy outlined in model 1 , the threshold of suspicion would lead to a high specificity for the test and a good level of sensitivity but with 19% more false negatives than model 2 . 
on the other hand , the threshold of suspicion is lower in model 2 , thus introducing more recognizable minimal signs , even in healthy breasts , and therefore reducing the specificity of the test to the point of increasing false positives by 4 , 110 cases ( out of a total of 17 , 000 )  . 
so a diagnostic gain of 19% ( no small thing ! ) is counterbalanced by the anxiety of being called for follow - up multiplied by ten times and the implementation of invasive procedures multiplied by five . 
on the basis of current knowledge and experience , since in both cases the radiologist knows in advance the nature of the error , either false positive or false negative , and plans his or her work activity on the basis of this assessment , the error may be defined as strategic , especially if the choice is shared in the context of coordinated decision making and operations . 
as a result , in the implementation phase of breast screening , the error becomes operatively present , with a meaning similar to that codified by federspil and vettor [ 1 , 2 ] in clinical activity , when there is a choice of two alternative therapies . prevedere la diversa distribuzione degli errori : la figura 7 , di facile comprensione nei passaggi dai valori assoluti a quelli percentuali [ 39 ] , funge da riferimento per le successive argomentazioni . 
nellipotesi di una scelta strategica che si uniformi al modello 1 la soglia del sospetto comporterebbe unelevata specificit del test ed una buona sensibilit , ma con una quota di falsi negativi del 19% in pi rispetto al modello operativo 2 . 
daltro canto nel modello operativo 2 , ove la soglia del sospetto si abbassa , introducendo quindi molti segni minimi riconoscibili anche in mammelle sane , la specificit del test si riduce al punto di aumentare di ben 4410 casi ( su 17000 donne ! ) i falsi positivi . 
poich , sulla base delle attuali conoscenze ed esperienze , in entrambi i casi il radiologo conosce preventivamente il versante dellerrore , falso positivo o falso negativo , e anche in base a tale valutazione progetta la sua attivit , lerrore pu essere definito strategico , a maggior ragione se la scelta condivisa nellambito di un coordinamento operativo - decisionale . 
inches : systematic approach to human error in radiology system errors it has already been mentioned how system errors have repercussions in the end on the final medical assessment , with the characteristic connotations of human error [ 7 ]  . 
it has been recognized that the system as such has peculiarities in which the cause of errors is to be found . generally speaking , we would intuitively expect a wellconstructed system to be equipped with defences , barriers and mechanisms which reduce the risk of errors to a minimu nonetheless , those mechanisms , which reason and rasmussen [ 6 ] liken to barriers filled with holes , are extremely vulnerable when the holes line up on the same trajectory . the inevitable error is accompanied by the personal application , which is not able to correct the error owing to a series of preexisting causes , such as those summarized in figure 6 . system errors are therefore prevented above all by adopting a safety system which renders their occurrence difficult for individual work and by performing constant research which is accompanied by daily efficiency [ 40 ]  . there are numerous suggestions for achieving this in di . 
those which draw on applicative criteria include protocols for reducing reliance on memory , improvement of access to information through the patients case history , use of systems impermeable to errors to avoid homonymy , and training . measures more specifically related to the department include maintenance of quality standards , systematic control of equipment , revision of reports and appropriate instructions to users . federspil e vettor [ 1 , 2 ] nellattivit clinica , allorch si mettano in alternativa due scelte terapeutiche . errori di sistema gi stato dato risalto a come gli errori di sistema si ripercuotano alla fine sulla valutazione medica conclusiva , con le connotazioni caratteristiche dellerrore umano [ 7 ]  . 
allerrore inevitabile si aggiunge lapplicazione personale , che non in grado di correggerlo per una serie di concause tra le quali si riconoscono in modo immediato quelle raccolte in figura 6 . 
la prevenzione degli errori di sistema si attua quindi sopratutto mediante un apparato di sicurezza che li renda di difficile evenienza per il lavoro individuale e mediante una costante ricerca che proceda di pari passo con lefficienza giornaliera [ 40 ]  . nella di molti sono i suggerimenti in questo senso . 
tra quelli che si rifanno ai criteri applicativi generali si citano i protocolli per ridurre la fiducia nella memoria , il miglioramento allaccesso dellinformazione mediante la cartella clinica del paziente , luso di sistemi impermeabili agli errori ad evitare omonimie , laddestramento . 
per quanto riguarda pi specificamente il reparto si ricordano il mantenimento degli standard di qualit , il controllo sistematico delle attrezzature , la revisione dei referti , le idonee segnalazioni agli utenti . conclusions considerazioni conclusive error is a characteristic feature of human activity . 
the latin saying errare humanum est may be applied to all activity , and di is no exception . perhaps less well known is the medieval addition to the saying attributed to saint bernard sed perseverare diabolicum indicating that errors upset our balance and therefore need to be corrected or , better still , prevented . to achieve these aims in a complex system such as di , simple recognition of the error does not appear to be sufficient . preliminary knowledge of the types and causes of errors relating to human activity and the system is required , as well as their application in a daily analysis to improve both standards of service and personal satisfaction . lerrore rappresenta una connotazione caratteristica delle azioni umane . 
de vargas macciucca , via alberico albricci 28 , i - 00194 roma , italy , tel . : + 39 - 338 - 5924034 , fax : + 39 - 06 - 49970212 , e - mail : marinadevargasm@hotmail.com received : 2 february 2005 / accepted : 7 november 2005 / published online : 3 march 2006 abstract purpose . 
we retrospectively reviewed 35 patients ( 23 men and 12 women ; mean age 66.6 years ) presenting with acute cholecystitis who were assessed by emergency ultrasonography ( us ) ( 30 / 35 cases ) and spiral ct ( 12 / 35 cases ) ; all patients underwent emergency surgery . 
the us signs were analysed and classified as major criteria ( wall thickening and stratification , distension , murphys sign ) , minor criteria ( bile stones , sludge , and biliary tract dilatation ) , and complication signs ( gas collections , aerobilia , fluid collection , difficult or missed identification of the gallbladder )  . 
imaging results were compared with histological findings ( gold standard ) , and accuracy , sensitivity , specificity , and positive and negative predictive values ( ppvs and npvs ) were assessed for each modality . 
if more than two major signs associated with one minor sign or at least one sign of complication are present at us , ct is mandatory to recognise and thoroughly evaluate the type of complication and indicate appropriate treatment . key words acute cholecystitis complicated cholecystitis us spiral ct riassunto scopo . 
sono stati esaminati retrospettivamente 35 pazienti ( 23 uomini e 12 donne ; et media 66 , 6 anni ) affetti da colecistite acuta , valutati in urgenza con esame ecografico ( 30 / 35 casi ) e tc ( 12 casi ) e sottoposti a intervento chirurgico urgente . 
i parametri ecografici sono stati analizzati e classificati come criteri maggiori ( ispessimento parietale , stratificazione parietale , sovradistensione , segno di murphy ecografico ) , minori ( calcoli o sedimenti nella colecisti o nelle vie biliari , dilatazione delle vie biliari ) e segni di complicazione ( raccolte gassose , aerobilia , raccolte fluide , difficile o mancato riconoscimento della colecisti )  . i risultati dellimaging sono stati confrontati con quelli dellesame istologico ( gold standard ) e sono state valutate accuratezza , sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) delle rispettive metodiche . 
lecografia ha dimostrato una accuratezza del 66 , 6% , una sensibilit del 37 , 5% , una specificit del 70% , un vpp del 100% e un vpn del 58 , 3% . 
in presenza di pi di due segni maggiori e uno minore o di almeno un segno di complicazione allecografia , lesame tc raccomandabile per il riconoscimento e la completa valutazione del tipo di complicazione , fornendo la giusta indicazione allintervento chirurgico urgente . parole chiave colecistite acuta colecistite complicata ecografia tc - spirale m . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis introduction introduzione the clinical suspicion of acute cholecystitis is one of the most frequent conditions facing the radiologist in emergency settings , as well as being the fourth cause of hospitalisation in patients presenting with acute abdomen [ 1 ] and the chief indication for emergency cholecystectomy [ 2 , 3 ]  . 
women under the age of 50 years are up to three times more frequently affected by cholecystitis than men whereas after this age , the incidence is the same in both genders . 
the most common cause of cholecystitis is lithiasis with cystic duct obstruction ( 90%95% )  . mucosal hypersecretion due to irritation resulting from increased bile concentration leads to oedema associated with wall thickening , followed by increased intraluminal pressure , wall distension , and stretching of the thin wall vessels with subsequent ischaemia and necrosis of the parietal mucosa . bacterial superinfection , which develops in 50%70% of cases , can lead to complications of acute cholecystitis such as empyema , gangrene , necrosis , and perforation [ 46 ]  . 
a patient without a history of biliary symptoms will rarely develop acute cholecystitis , whereas fewer than 15% of patients with gallstones present symptoms and fewer than 5% develop acute cholecystitis [ 7 ]  . in 5%10% of cases , cholecystitis is non - calculous . 
this situation mainly occurs in patients who have suffered serious injuries or burns , debilitated patients , patients with long - term hospitalisation in icu , or those undergoing prolonged parenteral feeding ; in these patients , systemic shock or the continued use of vasoconstrictors apparently causes ischaemia of the gallbladder wall mucosa , which is characterised by terminal blood supply and insufficient collateral circuits . 
according to another theory , however , non - calculous cholecystitis is due to mechanical obstruction of the cystic duct ( already narrowed by oedematogenic events ) by bile that has become dense and viscous following prolonged biliary stasis [ 8 , 9 ]  . 
other risk factors include overeating , diabetes , sepsis , cardiac arrest , atherosclerosis , aids , and chemotherapy via the hepatic artery [ 10 ]  . because symptoms are non - specific , it is difficult to clinically differentiate biliary colic from acute inflammation , but differential diagnosis is fundamental for establishing the correct therapeutic approach . 
treatment of acute cholecystitis is a matter of debate due to the different therapeutic options : emergency surgery ( laparotomy or laparoscopy ) , or delayed surgery after antibiotic treatment [ 11 , 12 ]  . 
further diagnostic investigation using imaging studies is therefore necessary for early diagnosis and timely treatment , above all when there is a suspicion of complications of acute cholecystitis . ultrasonography ( us ) is usually the first - choice modality [ 13 ] : the association of hepatobiliary us alone with clinical assessment allows accurate diagnosis in the majority of cases of calculous cholecystitis thanks to its very high sensitivity in the detection of cholelithiasis ( 95% ) [ 14 ] ; in addition , this examination has a low cost , is reproducible , and allows recognition and exclusion of numerous other causes of abdominal pain . both computed tomography ( ct ) and magnetic resonance il sospetto clinico di colecistite acuta rappresenta uno dei quesiti pi frequentemente sottoposti al radiologo in urgenza nonch la quarta causa di ricovero ospedaliero per pazienti che si presentano con addome acuto [ 1 ] ed la principale indicazione alla colecistectomia eseguita in urgenza [ 2 , 3 ]  . al di sotto dei 50 anni le donne sono fino a 3 volte pi colpite degli uomini , mentre oltre tale et lincidenza uguale nei due sessi . 
lipersecrezione mucosa determinata da fenomeni irritativi per iperconcentrazione della bile alla base del conseguente edema con ispessimento delle pareti , cui segue laumento della pressione intraluminale e la distensione delle pareti , con stiramento dei sottili vasi parietali , fenomeni alla base della successiva ischemia e poi della necrosi della mucosa parietale ; la sovrainfezione batterica , che si verifica solo nel 50%70% dei casi , invece causa delle possibili complicanze della colecistite acuta quali lempiema , la gangrena , la necrosi e la perforazione [ 46 ]  . 
raro che un paziente senza storia di sintomatologia biliare possa sviluppare una colecistite acuta , mentre al contrario meno del 15% dei pazienti con colelitiasi presentano sintomi clinici e meno del 5% sviluppano una colecistite acuta [ 7 ]  . nel 5%10% dei casi la colecistite invece alitiasica . questa evenienza si verifica essenzialmente in pazienti che hanno subito gravi traumi , defedati , ustionati , ricoverati a lungo in reparti di rianimazione o con alimentazione per via parenterale protratta nel tempo , nei quali lo shock sistemico o luso prolungato di vaso - costrittori indurrebbero unischemia della mucosa parietale della colecisti , che possiede una irrorazione di tipo terminale , con scarsi circoli collaterali ; tuttavia , secondo unaltra teoria le colecistiti alitiasiche sarebbero causate dallostruzione meccanica del dotto cistico ( gi ridotto di calibro per fenomeni edemigeni ) da parte di bile divenuta densa e vischiosa in seguito a prolungata stasi biliare [ 8 , 9 ]  . 
altri fattori di rischio includono liperalimentazione , il diabete , la sepsi , larresto cardiaco , laterosclerosi , laids e la chemioterapia attraverso larteria epatica [ 10 ]  . a causa dellaspecificit dei sintomi difficile differenziare clinicamente una colica biliare da una infiammazione acuta , ma la diagnosi differenziale fondamentale per una corretta pianificazione terapeutica . 
il trattamento delle colecistiti acute oggetto di discussione in quanto esistono differenti opzioni terapeutiche : lintervento chirurgico ( per via laparotomica o laparoscopica ) eseguito in urgenza o differito dopo terapia antibiotica [ 11 , 12 ]  . 
pertanto , specie quando si sospettino le complicanze della colecistite acuta , al fine di una precoce diagnosi e di un tempestivo trattamento terapeutico , si impone la necessit di approfondimenti diagnostici con esami strumentali . generalmente lecografia lindagine strumentale di prima istanza [ 13 ] : associando la sola ecografia epato - biliare alla valutazione clinica possibile una diagnosi accurata nella maggior parte dei casi , specie se la colecistite su base litiasica , grazie alla elevatissima sensibilit di questa metodica nel rilievo di colelitiasi ( 95% ) [ 14 ] ; inoltre tale esame presenta un basso costo , riproducibile e permette il riconoscimento e lesclusione di numerose altre cause di dolore m . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis ( mr ) normally add a small amount of information to the evaluation of acute cholecystitis but can be very useful in the case of subacute manifestations , in the presence of palpable pseudo - masses in the right hypochondrium , of clinical us discrepancy , and in the case of complications such as empyemic cholecystitis , abscesses , emphysematous cholecystitis , necrotic - gangrenous cholecystitis , perforation , biliary - enteric fistula or biliary ileus [ 2 , 6 , 7 , 15 , 16 ]  . the aim of this study was to review cases seen over 1 year of complicated acute cholecystitis evaluated by emergency us and ct and treated with emergency surgery in order to recognise specific and non - specific signs of complication and compare them with those reported in the literature . another aim was to define a correct diagnostic protocol involving the use of ct in selected cases . materials and methods in this study , we retrospectively examined the cases of 35 patients ( 12 women and 23 men ) aged between 27 and 99 years ( mean age 66.6 years ) suffering from acute cholecystitis who underwent imaging examinations between april 2003 and april 2004 . all patients underwent surgery and histological examination was considered the gold standard . 
patients whose diagnostic examinations performed at other sites were not available , patients who did not undergo emergency surgery due to medical contraindications , and patients whose operation was delayed for more than 48 h after presentation were excluded . clinical signs ( pain , murphys sign , fever , palpable swelling , jaundice ) and laboratory signs ( neutrophilic leukocytosis , bilirubinaemia , transaminasemia , glycaemia ) at the time of diagnosis were considered . 
ct spiral examinations ( siemens somatom plus 4 , erlangen , germany ) were performed before and after iv injection of contrast agent , with scans during the venous phase ( 60to 70 - s delay ) without oral contrast agent . 
in one case , ct was performed without iv injection of contrast agent due to reported allergy to iodinated contrast agents . the parameters analysed in ultrasonographic examinations were the following : focal or diffuse wall thickening ( more than 3 mm ) ; stratification or double parietal profile ; distension ( maximum transverse diameter greater than 5 cm ) ; stones in the gallbladder or biliary tract ; sludge or endoluminal aggregates ; parietal , endoluminal or extra - parietal gas collections ; aerobilia ; free or sacculated pericholecystic or abdominal fluid collections ; intraand extra - hepatic biliary tract dilatation ; presence of ultrasonographic murphys sign ; and possible associated findings . 
difficulty or inability to recognise the gallbladder was also evaluated . ultrasonographic signs were divided into three groups : major criteria of simple acute cholecystitis ( msac ) , minor criaddominale . sia la tc che la rm generalmente aggiungono un numero esiguo di informazioni alla valutazione delle colecistiti acute , ma possono essere molto utili in caso di manifestazioni subacute , in presenza di pseudomasse palpabili in ipocondrio destro , in caso di discrepanza clinico - ecografica e nei casi di complicazioni quali la colecistite empiematosa , lascessualizzazione , la colecistite enfisematosa , la colecistite necrotico - gangrenosa , la perforazione , la fistola bilioenterica o lileo biliare [ 2 , 6 , 7 , 15 , 16 ]  . questo studio si propone di esaminare i casi di colecistite acuta complicata , valutati in urgenza con ecografia e tc e sottoposti ad intervento chirurgico in urgenza nel corso di un anno , al fine di riconoscere i segni specifici ed aspecifici di complicanza da noi riscontrati e confrontarli con una revisione della letteratura . 
ci proponiamo inoltre di definire un corretto iter diagnostico che preveda limpiego della tc in casi selezionati . materiali e metodi in questo studio sono stati esaminati retrospettivamente 35 pazienti ( 12 donne e 23 uomini ) di et compresa tra 27 e 99 anni ( et media 66 , 6 anni ) affetti da patologia acuta della colecisti e sottoposti ad esami strumentali nel periodo compreso tra laprile 2003 e laprile 2004 . 
sono stati pertanto esclusi i casi in cui non sono risultati disponibili gli esami diagnostici eseguiti in altre sedi , i pazienti non sottoposti ad intervento chirurgico in urgenza per controindicazioni mediche e quelli il cui intervento chirurgico stato differito oltre le 48 ore dalla diagnosi . sono stati considerati i segni clinici ( dolore , manovra di murphy , febbre , tumefazione palpabile e ittero ) e laboratoristici ( leucocitosi neutrofila , bilirubinemia , transaminasemia , glicemia ) al momento della diagnosi . 
per gli esami ecografici sono state utilizzate due differenti apparecchiature ( au5 esaote , italia e logiq 400 , ge medical system , milwaukee , wi , usa ) con sonda convex da 3 , 55 mhz . 
per riferita allergia al mdc iodato . i parametri analizzati negli esami ecografici sono stati i seguenti : ispessimento parietale diffuso o focale ( considerando ispessita la parete quando superiore a 3 mm ) , stratificazione o doppio contorno parietale , sovradistensione ( diametro traverso massimo maggiore di 5 cm ) , calcoli nella colecisti o nelle vie biliari , presenza di sedimenti o aggregati endoluminali , raccolte gassose parietali , endoluminali o extraparietali , aerobilia , raccolte fluide pericolecistiche o endo - addominali libere o saccate , dilatazione delle vie biliari intraed extra - epatiche , presenza di segno di murphy ecografico ed eventuali reperti associati . 
msac , major criteria of simple acute cholecystitis ; msac , minor criteria of simple acute cholecystitis ; cc , complication criteria msac msac wall thickening > 3 mm wall stratification overdistension > 5 cm ultrasonographic murphys sign biliary sludge or stones biliary tract dilatation calculous cholecystitis biliary lithiasis pericholecystic or abdominal fluid collections parietal , endoluminal or extraparietal gas collections aerobilia difficult or missed recognition of the gallbladder tabella 1 segni ecografici di colecistite . 
mcas , criteri maggiori di colecistite acuta semplice ; mcas , criteri minori di colecistite acuta semplice ; cc , criteri di complicanza mcas mcas ispessimento parietale > 3 mm stratificazione parietale sovradistensione > 5 cm murphy ecografico sedimenti o aggregati biliari dilatazione delle vie biliari litiasi della colecisti litiasi delle vie biliari raccolte fluide pericolecistiche o endoaddominali raccolte gassose parietali , endoluminali o extraparietali aerobilia difficile o mancato riconoscimento della colecisti teria of simple acute cholecystitis ( msac ) , and complication criteria ( cc ) ( table 1 )  . 
for ct in addition to the us parameters , with the exception of murphys sign , we evaluated the presence of free air and alterations to vascularisation of the liver parenchyma adjacent to the gallbladder , both being signs of complication . 
the final histological examinations , considered as the gold standard , were compared with us and ct results , and accuracy , sensitivity , specificity , ppv , and npv for each modality were measured . 
the association with neutrophilia was observed in 28 / 35 ( 80% ) of cases ; in 11 / 35 cases , patients had elevated bilirubinaemia ( 31.4% ) and in 9 / 35 cases increased transaminases ( 25.7% ) ; 21 / 35 patients ( 60% ) had hyperglycaemia on admission , and four of them had a history of diabetes mellitus . 
in the selected group , hepatobiliary us was performed as the first - choice diagnostic examination in 30 / 35 patients , followed by ct in seven cases ; in five cases presenting with acute abdomen , ct was performed as the first - choice examination . 
on the whole , 30 patients were studied with us and 12 by ct ; in 7 / 35 cases , both us and ct were performed . us findings us revealed diffuse thickening of the gallbladder wall in gni ecografici sono stati inoltre suddivisi in tre gruppi : criteri maggiori di colecistite acuta semplice ( mcas ) , criteri minori di colecistite acuta semplice ( mcas ) e criteri di complicanza ( cc ) ( tabella 1 )  . 
per la tc oltre agli stessi parametri utilizzati per lecografia , fatta eccezione per il segno di murphy ecografico , stata valutata la presenza di aria libera e le alterazioni della vascolarizzazione del parenchima epatico adiacente alla colecisti , entrambi segni di complicazione . in base ai reperti riscontrati negli esami diagnostici sono stati distinti due gruppi di patologie : colecistiti acute semplici e colecistiti acute complicate . 
gli esami istologici definitivi , considerati il gold standard , sono stati confrontati con i risultati degli esami ecografici e tc e sono state misurate accuratezza , sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) delle rispettive metodiche . 
nei casi sottoposti sia ad ecografia che a tc stata inoltre valutata la concordanza tra le due metodiche e lentit dei dati aggiuntivi forniti da una metodica rispetto allaltra . risultati i pazienti presentavano clinicamente dolore in ipocondrio destro o epigastrio in 32 / 35 casi ( 91 , 4% ) , manovra di murphy positiva in 22 / 35 casi ( 62 , 8% ) , febbre in 18 / 35 casi ( 51 , 4% ) , tumefazione palpabile in 6 / 35 casi ( 17 , 1% ) , ittero in 2 / 35 casi ( 5 , 7% )  . 
si associava leucocitosi neutrofila in 28 / 35 casi ( 80% ) ; in 11 / 35 casi i pazienti presentavano un innalzamento dei valori di bilirubinemia ( 31 , 4% ) e in 9 / 35 casi si rilevava un incremento dei valori delle transaminasi ( 25 , 7% ) ; 21 / 35 pazienti ( 60% ) avevano iperglicemia al momento del ricovero e 4 di questi pazienti presentavano storia di diabete mellito . 
nel gruppo selezionato , lecografia epatobiliare stata eseguita come primo esame diagnostico in 30 / 35 pazienti , seguita dalla tc in 7 casi ; in 5 casi la tc stata eseguita come esame di prima istanza , trattandosi di gravi quadri di addome acuto . 
ct also revealed three cases of acute pancreatitis ( 25% ) characterised by pancreatic enlargement , with peripancreatic fat tissue hyperdensity in two of these cases . in one patient with suspected thoracic aortic dissection , the detection of cholecystitis was an occasional finding revealed by ct . 
ct allowed the detection of three cases of simple acute cholecystitis and nine cases of complicated acute cholecystitis ( table 2 )  . surgical treatment and histology all patients underwent laparotomic or laparoscopic cholecystectomy within 2448 h of diagnosis . 
in addition to cholecystectomy , the following procedures were performed : three viscerolyses , two hepatic resections , one intestinal resection , one abdominoplasty for laparocele , one umbilical hernial repair , one peritoneal lavage , three abdominal collection drainages , one main biliary tract drainage , one duodenal fistula repair , and one choledochoplasty with kehr tube positioning . 
la tc ha inoltre individuato 3 casi di pancreatite acuta ( 25% ) caratterizzata da aumento volumetrico del pancreas con iperdensit del tessuto adiposo peripancreatico in 2 di questi casi . in un paziente con sospetta dissecazione dellaorta toracica il riscontro di colecistite stato un reperto occasionale rilevato allesame tc . 
la tc ha permesso di distinguere 3 casi di colecistite acuta semplice e 9 casi di colecistite acuta complicata ( tabella 2 )  . interventi chirurgici ed istologia tutti i pazienti sono stati sottoposti a colecistectomia per via laparotomica o laparoscopica nelle 2448 ore successive alla diagnosi . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis table 2 comparison between ultrasonography ( us ) , computed tomography ( ct ) , and histological findings * acute and recurrent cholecystitis are included in the group of simple cholecystitis tabella 2 confronto tra i risultati dellecografia , della tc e dellesame istologico simple cholecystitis * complicated cholecystitis neoplasms colecistiti semplici * colecistiti complicate neoplasie 24 / 30 ( 80% ) 6 / 30 ( 20% ) ecografia 24 / 30 ( 80% ) 6 / 30 ( 20% ) * il gruppo di colecistiti semplici comprende le acute e le croniche riacutizzate table 3 ultrasonographic signs in simple cholecystitis 3 / 12 ( 25% ) 9 / 12 ( 75% ) 3 / 12 ( 25% ) 9 / 12 ( 75% ) histology 14 / 35 ( 40% ) 20 / 35 ( 57.1% ) 1 / 35 ( 2.8% ) istologia 14 / 35 ( 40% ) 20 / 35 ( 57 , 1% ) 1 / 35 ( 2 , 8% ) patient thickening stratification distension murphys sign sludge biliary tract dilatation lithiasis tabella 3 segni ecografici riscontrati nelle colecistiti non complicate paziente ispessimento stratificazione sovradistensione murphy sedimenti dilatazione vvbb litiasi three cases of acute calculous cholecystitis ; 11 cases of recurrent chronic cholecystitis ( with inflammatory infiltrates associated with fibrosis ) , ten of which were calculous and one non - calculous ; and 20 complicated cases of cholecystitis ( 14 calculous and six non - calculous )  . 
the final histological examination revealed one case of undifferentiated carcinoma epatiche , 1 resezione intestinale , 1 addominoplastica per laparocele , 1 riduzione di ernia ombelicale , 1 lavaggio peritoneale , 3 drenaggi di raccolte addominali , 1 drenaggio della via biliare principale , 1 sutura di fistola duodenale e 1 coledoco - plastica con posizionamento di tubo di kehr . 
of the 20 complicated forms , histology diagnosed 13 cases of phlegmonous cholecystitis , two cases of empyema , two cases of necrotic and gangrenous cholecystitis , two cases of abscess , and one case of duodeno - cholecystic fistula . 
us had a sensitivity of 37.5% , a specificitable 4 ultrasonographic signs in complicated acute cholecystitis colecistite acuta litiasica , 11 casi di colecistite cronica riacutizzata ( con infiltrati flogistici associati a fibrosi ) , 10 delle quali su base litiasica e 1 alitiasica , 20 colecistiti complicate ( 14 litiasiche e 6 alitiasiche )  . in 1 caso lesame istologico definitivo ha dimostrato la presenza di un carcinoma indifferenziato della colecisti associato a litiasi . 
delle 20 forme complicate 13 sono risultate allesame istologico come colecistiti flemmonose , 2 casi di empiema , 2 casi di colecistite acuta necrotica e gangrenosa , 2 casi di ascesso e 1 caso di fistola colecisto - duodenale . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis ty of 70% , an accuracy of 66.6% , a ppv of 100% , and an npv of 58.3%. 
in the seven cases studied by both modalities , us and ct yielded similar results as regards the presence of complications ; however , ct provided additional information compared with us , as it detected the presence of fluid in four cases , identified the gallbladder in two cases in which it was not recognizable by us , and demonstrated the presence of intraparietal air in one case , endoluminal air in three cases and free air in one case . 
it also demonstrated biliary tract dilatation in two cases , a biliary - enteric fistula in one case , and intrahepatic fluid and gas due to cholecystitis in one case . 
unlike us , ct also permitted identification of three cases of oedematous pancreatitis . discussion considering that more than 20% of cases clinically classified as cholecystitis correspond to other diseases , the role of emergency diagnostic imaging is to support the clinical diagnosis of acute cholecystitis and to identify the complications of cholecystitis , thus indicating the correct therapeutic approach [ 7 ]  . 
in cases of simple cholecystitis , surgical treatment is normally delayed , and the patient is treated with antibiotics during the acute phase ; emergency surgery within 2448 h , however , prevents the formation of adhesions , which may complicate laparoscopic surgery and increase the rate of conversion into laparotomy [ 12 , 17 , 18 ]  . 
emergency surgery , especially when laparoscopic , therefore implies shorted hospitalisation and reduced post - operative complications and overall hospitalisation costs [ 11 , 12 , 17 , 1824 ]  . clinically , three quarters of patients suffering from acute cholecystitis have a history of biliary colic and pain in the right hypochondrium , which may irradiate to the right shoulder and to the epigastric region , accompanied by nausea , vomiting , and dyspepsia . 
con la tc sono stati identificati 3 vn , 9 vp , nessun fp e nessun fn . lecografia ha dimostrato una sensibilit del 37 , 5% , una specificit del 70% , una accuratezza del 66 , 6% , un vpp del 100% e un vpn del 58 , 3% . 
la tc ha invece presentato una sensibilit del 100% , una specificit del 100% , una accuratezza del 100% ( tabella 5 )  . nei 7 casi sottoposti sia ad ecografia che a tc le due metodiche sono risultate concordi per la presenza di complicanze , ma la tc ha fornito in ogni caso maggiori informazioni rispetto allecografia rilevando la presenza di versamento fluido in 4 casi , identificando la colecisti in 2 casi in cui allecografia non era riconoscibile , diagnosticando la presenza di aria intraparietale in 1 caso , endoluminale in 3 casi , di aria libera in 1 caso , ha mostrato la presenza di dilatazione delle vie biliari in 2 casi , la fistola bilio - enterica in 1 caso , la presenza di raccolta fluido - gassosa intraepatica ad origine dalla colecisti in 1 caso . 
la tc ha inoltre consentito rispetto allecografia lidentificazione di 3 casi di pancreatite edematosa . discussione il ruolo della diagnostica per immagini in emergenza nella patologia acuta della colecisti quello di supportare la diagnosi clinica , considerando che oltre il 20% dei casi classificati clinicamente come colecistite corrispondono a unaltra patologia , e di identificare le complicanze indicando il corretto approccio terapeutico [ 7 ]  . 
generalmente se la colecistite non risulta complicata , il trattamento chirurgico viene differito , sottoponendo il paziente in fase acuta a terapia antibiotica ; tuttavia , lintervento chirurgico in emergenza entro 2448 ore previene la formazione di aderenze che possono complicare lintervento chirurgico laparoscopico aumentandone la percentuale di conversione in laparotomia [ 12 , 17 , 18 ]  . 
in our study , fewer patients underwent ct than us , and the majority of them had complicated cholecystitis suspected at us or on the basis of clinical findings ; therefore , it was not possible to accurately assess the major and minor criteria using ct in simple cholecystitis . forty percent of patients with acute cholecystitis develop complications such as empyema , pericholecystic abscesses , necrotic - gangrenous cholecystitis , emphysematous cholecystitis , haemorrhagic cholecystitis , perforation , cholecysticenteric fistula , and biliary ileus [ 3638 ]  . 
 we also detected one case of duodeno - cholecystic fistula . in this case , the gallbladder was not recognisable at us whereas both aerobilia and a coarse calcification ( 3 cm ) between the liver and the pancreatic head were well visible in the second duodenal portion ; also , ct had some difficulties in that the stone could not be precisely localised in the intestinal lumen , and neither free air or endoperitoneal fluid collection could be seen . 
however , the presence of aerobilia guito in laparoscopia , comporta riduzione dei tempi di ospedalizzazione , delle complicanze post - operatorie e dei costi complessivi del ricovero [ 11 , 12 , 17 , 1824 ]  . clinicamente tre quarti dei pazienti affetti da colecistite acuta presentano una storia di coliche biliari , dolore in ipocondrio destro , che si pu irradiare alla spalla destra ed in sede epigastrica , accompagnato da nausea , vomito e dispepsia . 
il segno di murphy generalmente positivo e vi possono essere reperti di laboratorio aspecifici ( leucocitosi , iperbilirubinemia , iperamilasemia e aumento dei livelli di transaminasi ) [ 25 , 26 ]  . 
nel nostro studio i pazienti sottoposti a tc sono stati in numero ridotto rispetto ai casi sottoposti ad ecografia ed erano quasi tutti casi di colecistiti complicate sospettate allesame ecografico o in base al quadro clinico , pertanto non stato possibile valutare con accuratezza i criteri maggiori e minori con tale metodica nelle colecistiti semplici . 
nel 40% dei pazienti con colecistite acuta si sviluppano complicanze quali lempiema , gli ascessi pericolecistici , la colecistite necrotico - gangrenosa , la colecistite enfisematosa , la colecistite emorragica , la perforazione , la fistola colecisto - enterica e lileo bilare [ 3638 ]  . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis and inability to identify the gallbladder , perforated and collapsed , correctly prompted towards emergency surgery during which and a duodeno - cholecystic fistula with a stone impacted in the second duodenal portion was detected . 
in our study , no cases of haemorrhagic cholecystitis or biliary ileus were observed . the fundamental aim of diagnostic imaging , especially in emergency settings , is to differentiate simple and complicated cholecystitis in order to plan laparoscopic or laparotomic surgery within 48 h . 
to detect the complicated forms , we suggest a classification that takes into account the main us signs divided into major criteria ( wall thickening > 3 mm , wall stratification , positive sonographic murphys sign , and distension ) , minor criteria ( biliary sludge , calculous cholecystitis and biliary tract dilatation ) and criteria for complicated forms ( aerobilia , fluid and gas collections , or missed recognition of the gallbladder ) ( table 1 )  . 
this classification differs from mirviss classification [ 9 ] ( table 6 ) first of all because it takes into consideration sonographic criteria but also because the presence of stones and biliary sludge is considered a minor criteria ; this depends on the fact that , despite being a frequent sonographic finding , biliary sludge is not specific for cholecystitis . 
the analysis of associations between major and minor signs , on the other hand , did not show a significant difference between the two groups of simple and complicated cholecystitis . 
indeed , in 5 / 16 cases ( 31.2% ) of complicated cholecystitis and in 10 / 14 cases ( 71.4% ) of simple cholecystitis , an association of at least two major criteria and one minor was found . 
in 4 / 16 cases ( 25% ) of complicated cholecystitis and in 4 / 14 cases ( 28.5% ) of simtable 6 computed tomography ( ct ) signs of acute cholecystitis ( mirviss classification ) ct signs of acute cholecystitis [ mirvis et al . 
in questo caso allesame ecografico non risultava riconoscibile la colecisti , mentre erano ben evidenti sia laerobilia che la presenza di una struttura calcifica grossolana ( 3 cm ) situata tra il fegato e la porzione cefalica pancreatica , nella sede della seconda porzione duodenale ; anche la tc ha presentato alcune difficolt diagnostiche in quanto la formazione litiasica non risultava localizzabile con certezza nel lume intestinale e non erano visibili aria libera n versamento fluido endoperitoneale ; tuttavia la presenza di aerobilia e il mancato riconoscimento della colecisti , in quanto perforata e collassata , hanno indirizzato correttamente la paziente al trattamento chirurgico urgente ed stata riscontrata una fistola colecisto - duodenale con calcolo indovato a livello della seconda porzione duodenale . 
nella nostra casistica non sono stati riscontrati casi di colecistite emorragica n di ileo biliare . lobiettivo fondamentale che si propone la diagnostica per immagini soprattutto in emergenza quello di distinguere le colecistopatie semplici dalle complicate al fine di poter programmare lintervento chirurgico per via laporoscopica o laparotomica , entro le 48 ore . 
a tal fine per poter individuare le forme complicate proponiamo una classificazione che tiene conto dei principali segni ecografici suddivisi in criteri maggiori ( ispessimento parietale > 3 mm , aspetto stratificato della parete , segno ecografico di murphy positivo e sovradistensione ) , criteri miniori ( sedimenti biliari , litiasi della colecisti o delle vie biliari e dilatazione delle vie biliari ) e criteri riconducibili a forme complicate ( areobilia , raccolte fluide , raccolte gassose o mancato riconoscimento della colecisti ) ( tabella 1 )  . 
una classificazione basata su tali criteri differisce da quella di mirvis riportata in letteratura [ 9 ] ( tabella 6 ) , innanzitutto perch prende in considerazione dei criteri ecografici , ma anche perch la presenza di calcoli e sedimenti biliari considerata un criterio minore poich , sebbene con tale metodica sia molto frequentemente riscontrata , non specifica di colecistite : nel nostro studio calcoli e aggregati biliari erano presenti quasi sempre ( 98% della popolazione esaminata ) sia nelle forme complicate che in quelle semplici . nella nostra esperienza lecografia ha riscontrato segni sicuri di complicanza in 6 / 16 casi ( 37 , 5% )  . 
tra le colecistiti semplici i segni di complicazione non sono mai stati rilevati . lanalisi delle associazioni tra segni maggiori e minori invece non ha dimostrato una significativa differenza tra i due gruppi di colecistiti , semplici e complicate . 
infatti in 5 / 16 casi ( 31 , 2% ) di colecistite complicata e in 10 / 14 casi ( 71 , 4% ) di colecistite semplice stata riscontrata lassociazione di almeno 2 criteri maggiori e uno minore . 
in 4 / 16 casi ( 25% ) di colecistite complicata e in 4 / 14 casi ( 28 , 5% ) di colecistite semplice erano presenti allecografia meno di due criteri maggiori . 
 these data indicate that us can distinguish complicated and simple cholecystitis only in the presence of definite signs of complication ; in the majority of cases , however , these signs are not present . 
we believe that ct would have provided the correct diagnosis of complication in many of these cases given its higher accuracy and sensitivity . indeed , ct yielded no fp or fn results . 
because the majority of complications revealed by us showed at least two major criteria associated with at least one minor criterion or at least one criterion for complication ( overall 68.7% ) , further ct investigation after us is justified under these circumstances . numerous cases of phlegmonous cholecystitis were present ( 9 / 16 cases ) among the cases assessed as simple cholecystitis by us and as complicated cholecystitis by histological examination . although this form is not regarded as a complicated form in the literature , we decided to include these cases in the group of complications because involvement of the entire thickness of the organ causes serositis with peritoneal effusion in the majority of cases . 
if the emergency approach is based on medical treatment with delayed surgery , the peritoneal reaction may lead to the formation of synechia and fibrosis , with development of adhesions . 
phlegmonous cholecystitis therefore requires immediate surgical treatment because adhesions hinder possible surgical treatment during quiescence and increase the incidence of complications ; there is also a higher risk of laparoscopy being converted into laparotomy [ 12 ]  . conclusions assessment of acute cholecystitis in an emergency department requires careful analysis of the clinical findings and relies on us as first - choice examination . us allows the recognition of signs which , taken singularly , are poorly specific ; this directs the patient to further investigation by ct , which is indispensable for the complete recognition and evaluation of complicated forms . 
trenta , radiologists at the emergency department of policlinico umberto i , rome , for their help in collecting the case series . solo in presenza di segni certi di complicanza , ma nella maggior parte dei casi questi non sono presenti ; infatti , nella nostra casistica , allecografia sono risultati falsi negativi ( fn ) un terzo dei casi e la maggior parte di tali pazienti non stata sottoposta ad ulteriori indagini . 
poich allecografia la maggior parte delle complicanze presentavano almeno due criteri maggiori associati ad almeno uno minore oppure almeno un criterio di complicanza ( globalmente il 68 , 7% ) , si pu considerare giustificato in tali circostanze approfondire lesame ecografico con un esame tc . 
sebbene la letteratura non tratti questa forma come complicata , abbiamo ritenuto di includere tali casi nel gruppo delle complicazioni in quanto linteressamento a tutto spessore del viscere determina comunque una sierosite con presenza nella maggior parte dei casi di versamento peritoneale . 
in tali pazienti , se la scelta terapeutica in urgenza il trattamento medico e lintervento chirurgico viene differito , la reazione peritoneale nel tempo pu determinare la formazione di sinechie e fibrosi con lo sviluppo di briglie aderenziali . 
le colecistiti flemmonose necessitano pertanto di un trattamento chirurgico immediato , in quanto le aderenze rendono leventuale intervento in fase di quiescenza pi difficoltoso e aumentano lincidenza di complicanze ; in questi casi inoltre pi elevato il rischio di conversione dellintervento da laparoscopico a laparotomico [ 12 ]  . conclusioni la valutazione in un dipartimento di emergenza della patologia acuta della colecisti necessita di una attenta analisi dei dati clinici e si avvale dellutilizzo dellecografia come metodica di prima istanza . 
lecografia permette il riconoscimento di alcuni segni che sono poco specifici singolarmente , indirizzando il paziente allapprofondimento con tc che risulta indispensabile per riconoscere e valutare in maniera completa le forme complicate . 
in particolare , quando allecografia sono identificati almeno due segni maggiori e uno minore e quando sono presenti i segni specifici di complicanza , lapprofondimento con tc imprescindibile in quanto permette di selezionare i pazienti candidati ad intervento in urgenza rispetto a quelli da trattare con terapia antibiotica ed intervento differito ; inoltre la distinzione tra le diverse forme di colecistite aiuta il chirurgo nella scelta della tecnica operatoria pi indicata ( laparoscopica o laparotomica )  . ringraziamenti si ringraziano per la collaborazione nel reperimento della casistica il dott . 
gargiulo2 1dipartimento integrato dei servizi diagnostici e per immagini , azienda policlinico , via del pozzo 71 , i - 41100 modena , italy 2cattedra di chirurgia vascolare , azienda policlinico , modena , italy correspondence to : m.g. 
 + 39 - 059 - 4222238 , fax : + 39 - 059 - 4224349 , e - mail : amorico.mariagrazia@policlinico.mo.it received : 27 june 2005 / accepted : 18 october 2005 / published online : 3 march 2006 abstract purpose . 
magnetic resonance angiography ( mra ) has recently become instrumental in the diagnosis of arterial disease in various body districts and is gaining an increasingly important role in the study of peripheral vascularisation . 
mra was performed with a philips intera 1.5 t , with acquisitions from the coeliac trunk to the feet . for acquisitions of the feet and ankles we used unenhanced timeof - flight ( tof ) sequences with a head coil . 
digital subtraction angiography ( dsa ) remains the reference standard for planning treatment and for the follow - up of these patients , but it is invasive and potentially harmful as the iodinated contrast larteriopatia occlusiva periferica degli arti inferiori una patologia cronica e progressiva con unincidenza negli uomini con pi di 55 anni che va dal 4 , 5% al 8 , 8% [ 1 , 2 ]  . 
la diagnosi solitamente ottenuta mediante un accurato esame clinico , ma la scelta di uneventuale terapia non pu prescindere da precise informazioni morfologiche dellalbero arterioso ottenibili esclusivamente attraverso la diagnostica strumentale . 
because peripheral arterial occlusive disease is an increasingly common chronic condition , a large number of mostly elderly patients would have to undergo numerous angiographic examinations and endovascular procedures , both of which carry a high risk of complications , such as puncture of the arteries , iodinated contrast agent toxicity , and protracted exposure to radiation [ 3 ]  . 
for these reasons , it has become necessary to identify an alternative modality that is less invasive than dsa and able to evaluate the number and severity of lesions in order to plan treatment . 
recent technological innovations , such as continuous table movement and very fast three - dimensional ( 3d ) sequences [ contrast - enhanced mr angiography ( ce - mra ) ] [ 2 , 5 ] , have enabled the study of the arteries from the abdominal aorta to the foot with a single injection of contrast material . 
these improvements have overcome the limitations of the previous time - of - flight ( tof ) and phasecontrast sequences , such as long acquisition times ( ats ) and flow and movement artefacts . 
the aim of this study was to assess the reliability of mra in the evaluation of lesions caused by peripheral arterial occlusive disease , using intraarterial dsa as the reference standard . materials and methods patients from november 2003 to august 2004 , a total of 30 patients ( 11 women and 19 men ; age range , 4984 years ; mean age , 72 years ) underwent digital subtraction angiography and mra of the lower limbs . 
two patients had concurrent renal artery stenosis ( one on the right and one on the left ) , and another two had aneurysm of the infrarenal aorta , one of whom with concurrent aneurysm of the left popliteal artery . 
two patients were excluded after dsa because they had a pacemaker , and another was excluded due to a history of surgery with insertion of artificial crystalline made of non - mr - compatible material . 
poich larteriopatia periferica una patologia cronica in aumento , un numero elevato di pazienti , la maggior parte anziani , dovrebbe essere sottoposto a numerose angiografie e procedure endovascolari che comportano un elevato rischio di complicanze sia legate alla procedura , come la puntura dei vasi arteriosi , che alla tossicit del mezzo di contrasto ed allesposizione prolungata alle radiazioni ionizzanti [ 3 ]  . 
per tutti questi motivi si sentita lesigenza di una metodica di studio delle arterie degli arti inferiori meno invasiva e che possa essere utilizzata come valutazione del numero e della severit delle lesioni in previsione di un trattamento . la risonanza magnetica una tecnica di indagine non invasiva che non impiega radiazioni ionizzanti n mezzo di contrasto potenzialmente nefrotossico [ 4 ]  . 
recentemente sono state introdotte innovazioni tecnologiche come , per esempio , il movimento automatico del lettino porta - paziente e sequenze tridimensionali molto veloci ( ce - mra ) [ 2 , 5 ] che rendono possibile lo studio dellalbero arterioso dal tripode celiaco ai vasi del piede con ununica iniezione di mezzo di contrasto . 
ci ha permesso di superare le limitazioni delle precedenti sequenze time - of - flight e phase - contrast come i lunghi tempi di acquisizione , gli artefatti da flusso e da movimento . 
scopo di questo lavoro analizzare quale sia la reale affidabilit della angio - rm nella valutazione delle lesioni causate dallarteriopatia occlusiva periferica , utilizzando come standard di riferimento langiografia digitale a sottrazione ( dsa )  . materiali e metodi pazienti dal novembre 2003 allagosto 2004 , 30 pazienti di et compresa tra i 49 ed gli 84 anni ( 11 donne e 19 uomini ; et media 72 anni ) sono stati sottoposti ad angiografia digitale e ad angio - rm degli arti inferiori . 
due casi , inoltre , mostravano la presenza concomitante di stenosi dellarteria renale ( 1 a destra ed 1 a sinistra ) , in 2 casi un aneurisma dellaorta sottorenale in uno dei quali era concomitante un aneurisma dellarteria poplitea sinistra . 
the disease staging classification adopted by us was the following : mild stenosis ( not haemodynamically significant ) with less than 50% reduction in vessel lumen ; moderate stenosis ( haemodynamically significant ) with 50%90% reduction in lumen ; severe stenosis with a reduction in vessel lumen greater than 90% . the percentage of stenosis was automatically calculated by software present in the image - processing work stations connected to the angiographic and mr instruments ( viewforum , philips )  . patients included in the study underwent dsa performed with digital equipment ( philips integris allura , philips medical system , the netherlands ) , following a pre - established procedure . 
the examination procedure involved positioning of a 4 - french universal flash ( uf ) catheter into the abdominal aorta through a retrograde , generally right - sided , transfemoral approach , or a brachial approach according to the seldinger technique , after the local administration of 10 cc of lidocaine hydrochloride 200 mg ( bioindustria , italy )  . 
the catheter was positioned in the external or common iliac artery to perform selective arteriography of the limb , with anteroposterior ( ap ) projections for the thigh and leg vessels , and both ap and laterolateral ( ll ) projections for the feet vessels . 
images of the lower limb vessels , from the femoral artery to those of the feet , were obtained sequentially with separate injections of contrast material delayed relative to acquisition , on the basis of the level of study and the speed of flow . 
the mean dose of contrast agent injected was approximately 200 cc ( iomeprol 300 mg / i / ml , iomeron bracco , or iopamidol 300 mg / i / ml , iopamiro bracco ; iodixanol 270 mg / i / ml , visipaque nycomed amersham in selected subjects ) , with a range from 160 to 300 cc according to the diagnostic requirements of the single case . 
the entire examination had a mean duration of 60 min . mra was performed by using a 1.5 - t whole - body mri unit ( intera philips gyroscan 1.5 tesla , philips medical system )  . for each patient , a complete history was taken to exclude the presence of contraindications . 
the patient was positioned supine with both feet inside the coil usually used for the study of the head ( head coil ) for a preliminary evaluation of the foot arteries with an unenhanced 3d - tof sequence . 
due pazienti sono stati esclusi dallo studio dopo lesecuzione della dsa , perch portatori di pace - maker ed uno per presenza di anamnesi positiva per intervento con inserimento di cristallino artificiale di materiale non rm - compatibile . 
tre pazienti erano gi stati precedentemente sottoposti a procedure di rivascolarizzazione ( 1 by - pass femorofemorale destro - sinistro con bypass femoro - popliteo bilaterale , 1 by - pass femoro - popliteo destro , 1 endoprotesi hemoban in femorale superficiale destra ) e tre pazienti avevano subito lamputazione di uno o pi dita di un piede . la classificazione da noi seguita distingue : stenosi lievi ( non emodinamicamente significative ) con riduzione del lume vasale inferiore al 50% ; stenosi moderate ( emodinamicamente significative ) con riduzione del lume vasale superiore al 50% , ma inferiore al 90% ; stenosi gravi con riduzione del lume vasale superiore al 90% . la percentuale di stenosi stata calcolata automaticamente da un programma di calcolo presente nelle stazioni di elaborazione delle immagini correlate allangiografo philips allura ed allapparecchio di rm ( viewforum , philips medical systems , olanda )  . angiografia digitale i pazienti inclusi nello studio sono stati sottoposti a dsa con tecnica di sottrazione dimmagine eseguita con angiografo digitale ( integris allura philips , philips medical systems , olanda ) , seguendo una procedura prestabilita . 
lesecuzione dellesame prevede il posizionamento di un catetere uf ( universal flash ) di 4 f nellaorta addominale per mezzo di un approccio transfemorale retrogrado , generalmente destro , o brachiale , con ago munito di mandrino secondo la tecnica seldinger , ovviamente dopo aver eseguito nella sede lanestesia locale con 10 cc di lidocaina cloridrato 200 mg . 
il catetere viene posizionato in arteria iliaca esterna o comune per lesecuzione di unarteriografia darto selettiva ; si effettuano riprese dei vasi di coscia e di gamba in a - p e del piede sia in a - p che in ll . 
le immagini del riempimento degli arti inferiori dallarteria femorale a quelle del piede sono state ottenute sequenzialmente con iniezioni separate di mezzo di contrasto ritardate rispetto allacquisizione in base al livello di studio ed alla velocit del flusso . 
la dose media di mezzo di contrasto iniettato per via endoarteriosa di 200 cc circa ( iomeprolo 300 mg i / ml , iomeronr bracco oppure iopamidolo 300 mg i / ml , iopamiror bracco ; iodixanolo 270 mg i / ml , visipaquer , amersham , in soggetti selezionati ) , con un range variabile da 160 a 300 cc a seconda delle esigenze diagnostiche del singolo caso . 
the parameters used were : tr 23 ms , te 9.2 ms , flip angle 20 , thickness 0.7 mm , matrix 304x258 , field of view ( fov ) 30 c the sequence yielded around 150 images , which were processed in 3d at the workstation view forum 3.1 ( philips medical systems )  . 
subsequently , the head coil was replaced with a body coil , with mobytrack , a specific attachment for this type of study which supports and immobilises the legs at the level of the knees and holds the feet perpendicular to the legs . 
positioning of the entire lower limb in the same plane is important , as the coronal acquisition might otherwise miss arterial segments not perfectly included in the field of view . 
the arterial study was performed with three 40to 45 - cm acquisitions , with 3d coronal sequences from the coeliac trunk to the feet , each lasting around 3035 s , with an overlap of 13 c automatic table movement means the examination can be performed in a time compatible with the persistence of the paramagnetic contrast agent in the arterial vessels . first , a 2d fast - field - echo centring sequence was performed in the three planes in all three positions , on which the following sequences were planned . 
the parameters of this sequence were : tr 6.1 ms , te 1.5 ms , flip angle 35 , thickness 1.5 mm , matrix 512x384 , fov 43 cthen , circulation time ( ct ) , or bolus timing , was evaluated by injecting 2 cc of contrast agent followed by 15 cc of saline solution with a special mr - compatible injector ( spectris mr injector , medrad )  . 
this was followed by a fast - field - echo sequence ( tr 7 , te 0.87 , flip angle 40 , thickness 80 mm , matrix 256x256 , fov 53 cm ) in which a single coronal image at the level of the abdominal aorta and its bifurcation was acquired at intervals of 1 s for about 50 times , repeating the same image at regular intervals until the contrast agent was visualised . 
scan delay ( sd ) was obtained by subtracting half of the at from the ct plus half of the injection time ( it ) : sd = ct + ( it / 2 ) - ( at / 2 )  . an initial unenhanced 3d sequence serving as a mask was performed from the feet to the abdomen . 
around 40 - 50 cc of paramagnetic contrast agent ( gadodiamide ; omniscan nycomed amersham ) [ 15 ] was then injected as a bolus divided in two fractions : 50% was injected at a speed of 1 ml / s and 50% at a speed of 0.5 ml / s , followed by 15 ml of saline solution injected at a speed of 1 ml / s . 
this part of the examination lasted 2025 mparameters used in this sequence were : tr 6.1 ms , te 1.5 ms , flip angle 35 , thickness 1.5 mm , matrix 512x384 , fov 43 cthe 3d sequence used by us was designed to acquire a centric k space , the centre of the k space being acquired during the enhancement peak , which provides the best contrast between blood and static tissue . 
approximately 200 images were obtained , which were reconstructed with 3d maximum image projecte superconduttivo ( philips gyroscan intera 1 , 5 tesla , olanda ) dotato di gradienti con intensit massima di 30 mtesla / m ed una rapidit di salita ( slew rate ) di 150 mtesla / m / ms . 
il paziente viene posizionato supino , con entrambi i piedi allinterno della bobina solitamente usata per lo studio dellencefalo ( head ) , per eseguire una preliminare valutazione delle arterie del piede attraverso un sequenza 3d - tof senza mezzo di contrasto . 
la sequenza viene eseguita su un piano coronale obliquo perpendicolare allasse maggiore del piede e la banda di presaturazione necessaria per impedire il contemporaneo rilevamento del flusso venoso posta caudalmente alla acquisizione . 
successivamente si effettua un cambio di bobina : si sostituisce la bobina head e si utilizza la bobina body per la trasmissione e la ricezione del segnale ed un supporto dedicato per lo studio degli arti inferiori , moby - track , che sostiene ed immobilizza le gambe a livello delle ginocchia , che sono leggermente sollevate , e mantiene i piedi su uno stesso piano perpendicolare a quello delle gambe . 
il posizionamento di tutto larto inferiore su uno stesso piano un accorgimento importante poich altrimenti lacquisizione nel piano coronale potrebbe non includere segmenti arteriosi non perfettamente compresi nel campo di vista . 
lo studio arterioso viene eseguito in 3 acquisizioni da 4045 cm con sequenze 3d coronali dal tripode ai piedi , ognuna della durata di circa 3035 secondi , con sovrapposizione di 13 cil movimento automatizzato del letto porta - paziente permette di eseguire questo tipo di esami in un tempo compatibile con la permanenza del mezzo di contrasto paramagnetico nei vasi arteriosi . 
si esegue inizialmente una sequenza di centratura 2d turbo field echo sui 3 piani in tutte le 3 posizioni sulla quale verranno pianificate tutte le sequenze successive con i seguenti parametri : tr 6 , 1 ms , te 1 , 5 ms , flip angle 35 , spessore 1 , 5 mm , matrice 512x384 , campo di vista 43 csi procede poi ad una valutazione del tempo di circolo o bolus timing iniettando 2 cc di contrasto seguiti da 15 cc di soluzione fisiologica con un apposito iniettore rm - compatibile ( spectris mr injector , medrad , indianola , pa )  . 
si esegue una sequenza fast field echo ( tr 7 , te 0 , 87 , flip angle 40 , spessore 80 mm , matrice 256x256 , campo di vista 53 cm ) , in cui una singola immagine coronale , a livello dellaorta addominale e della sua biforcazione acquisita ad intervalli di 1 secondo per circa 50 volte ripetendo la stessa immagine ad intervalli costanti fino alla visualizzazione del mezzo di contrasto a quel livello . 
il tempo di ritardo scansione ( trs ) si ottiene sottraendo al tempo di circolo ( tc ) la met del tempo di acquisizione ( ta ) , dopo avervi sommato la met del tempo di iniezione table 1 evaluation form right left m . 
the total time spent by the patient inside the mr room , which included examination time , technical time for sequence formulation , and coil changing , was about 4045 min . data collection and analysis mra and dsa examinations were independently evaluated by three radiologists who used grading sheets to assess vessel state : no stenosis , or obstruction . 
the vessel being studied was drawn with parallel lines along a segment that includes the vessel above and below the stenosis and stenotic segment ; the computer analyses the segment and calculates the percentage of stenosis . 
conventional angiography examinations were evaluated by another radiologist blinded to the patients clinical history and results of mra . table 2 patent arteries with regular lumen artery common iliac external iliac internal iliac common femoral superficial femoral deep femoral popliteal anterior tibial posterior tibial peroneal dorsalis pedis plantaris pedis total mra , magnetic resonance ; dsa , digital subtraction angiography tabella 2 arterie pervie di calibro regolare vaso angio - rm angiografia a . 
si iniettano poi circa 4050 cc di contrasto paramagnetico ( gadodiamide omniscanner amersham , uppsala ) in un unico bolo suddiviso in due frazioni : il 50% viene iniettato ad una velocit di 1 ml / s , il restante ad una velocit di 0 , 5 ml / s ; seguito da 15 ml di fisiologica iniettata ad una velocit di 1 ml / s . 
la seconda sequenza con contrasto ha uno start - delay calcolato in base al bolus timing e viene eseguita dal tripode celiaco ai piedi . lapnea richiesta solo durante lacquisizione a livello addominale ed ha una durata di circa 25 s . 
il software della macchina sottrae automaticamente la sequenza con contrasto alla maschera per eliminare il segnale del tessuto adiposo e si ottiene unimmagine angio - rm delle arterie degli arti inferiori . 
la durata di questa parte dellesame di circa 2025 m i parametri utilizzati per eseguire questa sequenza sono : tr 6 , 1 ms , te 1 , 5 ms , flip angle 35 , spessore 1 , 5 mm , matrice 512x384 , campo di vista 43 cla sequenza 3d da noi utilizzata impostata per acquisire lo spazio k in senso centrico , grazie infatti allopzione centra , per cui viene acquisito il centro dello spazio k durante il passaggio del picco di contrasto massimo , che fornisce il contrasto migliore tra sangue e tessuto stazionario . 
il tempo totale che il paziente trascorre allinterno della stanza del magnete , che comprende il tempo desame , il tempo tecnico di impostazione delle sequenze e di cambio delle bobine di circa 4045 minuti . raccolta ed analisi dei dati gli esami di angio - rm e di angiografia sono stati valutati da 3 medici radiologi in modo indipendente attraverso la compilazione di schede , in cui si richiede di valutare lo stato del vaso : pervio , stenosi , ostruzione . 
la percentuale di stenosi stata ottenuta tramite un programma di calcolo inserito in speciali stazioni di elaborazione delle immagini , in cui viene disegnato con linee parallele il vaso in esame per un tratto che comprende il vaso a valle e a monte della stenosi ed il segmento stenotico ; il computer analizza il segmento in esame e calcola la percentuale di stenosi . 
langio - rm stata valutata da 2 medici radiologi in doppio cieco , senza conoscere la storia clinica del paziente ed i risultati dellangiografia tradizionale , utilizzando le rielaborazioni 3d delle immagini e le immagini originarie . 
si sono ottenute due schede ( tabella 1 ) per ogni paziente , una per la rm ed una per la angiografia , che sono state poi confrontate per valutare il livello di corrispondenza . 
i vasi arteriosi esaminati sono : aorta sottorenale , iliaca comune , iliaca esterna , iliaca interna , femorale comune , femorale superficiale , femorale profonda , poplitea , tibiale anteriore , tibiale posteriore , interossea , dorsale e plantare del piede . 
nei 2 pazienti con bypass se ne valutata anche la perviet , lo stato degli stessi e dei territori a valle . thus , two tables were obtained ( table 1 ) for each patient : one for mra and one for dsa , which were compared in order to evaluate the level of concordance . 
arterial vessels examined were : infrarenal aorta ; common iliac artery ; external and internal iliac arteries ; common , superficial , and deep femoral arteries ; popliteal artery ; anterior and posterior tibial arteries ; peroneal artery ; and dorsalis and plantaris pedis arteries . 
in the two patients with bypass , we also evaluated the patency and state of the bypass grafts and territories downstream . results mra was easy to perform and well tolerated although patients with trophic lesions , especially of the heels , had some difficulty staying motionless in the supine position because of pa this problem concerned above all the tof sequences , in which both feet have to be kept motionless inside the head coil for about 7 mas a result , because this sequence requires a very high level of patient cooperation , it was only performed in 15 . 
however , it did not yield important additional information compared with the contrast - enhanced study , except in one case . table 3 occlusions artery common iliac external iliac internal iliac common femoral superficial femoral deep femoral popliteal anterior tibial posterior tibial peroneal dorsalis pedis plantaris pedis total mra , magnetic resonance ; dsa , digital subtraction angiography tabella 3 occlusioni a . 
questo problema ha riguardato soprattutto lesecuzione delle sequenze tof , in cui entrambi i piedi devono rimanere immobili allinterno della bobina per circa 7 min . questa sequenza infatti non stata eseguita in tutti i pazienti , ma solo in 15 , in quanto necessita di estrema collaborazione e non ha dato informazioni rilevanti o aggiuntive rispetto allo studio con mezzo di contrasto , tranne in un singolo caso . 
sono stati visualizzati 552 vasi di calibro regolare con langio - rm e 547 con la dsa ( tabella 2 )  . si ottenuta una corretta visualizzazione di tutti i vasi fino alla caviglia , mentre per quanto riguarda le arterie del piede , in 3 casi , il precoce ritorno venoso ha reso difficile linterpretazione dellesame , ma grazie alla rielaborazione delle immagini alla workstation siamo sempre riusciti ad espritable 4 stenoses artery < 50% > 50% > 90% < 50% > 50% > 90% common iliac external iliac internal iliac common femoral superficial femoral deep femoral popliteal anterior tibial posterior tibial peroneal dorsalis pedis plantaris pedis total mra , magnetic resonance angiography ; dsa , digital subtraction angiography tabella 4 stenosi a . 
correct visualisation of all vessels was obtained up to the ankle whereas in the foot arteries , early venous return in three cases made interpretation of the examination difficult ; nonetheless , image processing enabled a judgement on the vessel to be expressed in all cases . 
discordances regarded the infrapopliteal arteries , with mra visualising the obstruction of 28 anterior tibial arteries , 35 posterior tibial , 14 peroneal , and 23 dorsalis pedis as against the 30 anterior tibial , 33 posterior tibial , 18 peroneal , and 22 dorsalis pedis visualised by dsa . 
in the cases of obstruction , the visibility of the collateral circulations was better with dsa , which was able to depict even tiny branches , but was also judged good with mra , which depicts the larger vessels only . 
evaluation of the foot arteries was more difficult : the tof sequences , if correctly performed , give information on the larger vessels perpendicular to the acquisition plane ; the contrast - enhanced sequences are also informative but they have a smaller field of view . 
as regards the nine ( 1.25% ) discordant segments , mra overestimated two ( 0.3% ) ( two occlusions of the posterior tibial arteries ) and underestimated six ( 1% ) ( two anterior tibial and four peroneal arteries )  . 
mra documented one occlusion of dorsalis pedis artery not visualised by dsa . overall , in the cases studied , mra had a specificity of 99.6% and a sensitivity of 96% ( table 5 )  . 
there was absolute concordance between the two imaging procedures in il numero di occlusioni valutato in angio - rm stato 140 e con la dsa 143 ( tabella 3 )  . 
le discordanze sono nelle arterie infrapoplitee , in particolare langio - rm ha riconosciuto lostruzione di 28 arterie tibiali anteriori , 35 tibiali posteriori , 14 interossee , 23 dorsali del piede contro le 30 tibiali anteriori , 33 tibiali posteriori , 18 inter - ossee , 22 dorsali del piede della dsa . 
nelle stenosi inferiori al 50% langio - rm ne ha riconosciute 13 , la dsa 14 : con questultima stata riconosciuta una stenosi dallarteria femorale profonda che risultava pervia alla angio - rm . 
nei casi di ostruzione la visibilit dei circoli collaterali stata migliore con la dsa , che stata in grado di evidenziare tutti i rami anche di piccolissimo calibro , ma stata giudicata buona con langio - rm , che mette in evidenza solo vasi di calibro maggiore . con entrambe le metodiche comunque possibile evidenziare il punto di ricanalizzazione del vaso . 
la valutazione pi difficoltosa stata quella dei vasi del piede : le sequenze tof danno informazioni , se correttamente eseguite , sui vasi di maggior calibro e perpendicolari al piano dacquisizione ; le sequenze con contrasto danno buone informazioni , ma hanno un campo di vista inferiore . 
dei 9 ( 1 , 25% ) segmenti discordanti , 2 ( 0 , 3% ) sono stati sovrastimati con langio - rm ( 2 occlusioni delle tibiali posteriori ) e 6 ( 1% ) sono stati sottostimati ( 2 tibiali anteriori e 4 inter - ossee )  . 
la permanenza totale del paziente nella sala del magnete stata in media di 45 mil tempo necessario alla rielaborazione ed alla stampa delle immagini alla workstation philips stato di 2030 mcome gi detto in caso di importante contaminazione venosa stato necessario un tempo maggiore . 
non si sono avute reazioni ai mezzi di contrasto in nessuno dei pazienti . discussione la tecnica di angio - rm da noi utilizzata , basata sullacquisizione di 3 volumi lievemente sovrapposti , iniettando il contrasto con uniniezione bifasica , ha permesso unaccurata valutazione dellalbero arterioso dal tripode celiaco alle arterie del piede . 
rispetto allangiografia , la rm offre importanti vantaggi nello studio di pazienti anziani con patologia arteriosa periferica , in quanto si possono evitare i rischi associati alla puntura arteriosa , al mezzo di contrasto iodato ed alle radiazioni ionizzanti . 
none of the patients experienced reactions to the contrast agent . discussion mra , based on the acquisition of three slightly overlapping volumes with two - phase injection of contrast agent , allowed table 6 data from the literature m . 
nellesecuzione dellangiorm si pu incorrere in alcuni pitfalls soprattutto perch per ottenere un esame angio - rm di elevata qualit con contrasto fondamentale la perfetta coordinazione tra linizio dellacquisizione e larrivo del mezzo di contrasto nella regione da studiare . 
non si sono avute comunque sostanziali discordanze tra angio - rm e dsa nella rilevazione della perviet dei vasi e nella valutazione della presenza di malattia aterosclerotica in tutti i territori esaminati . 
nello 0 , 3% dei casi si rilevata una sovrastima della gravit delle lesioni in angio - rm rispetto alla dsa [ 6 ]  . la sovrastima causata dal defasamento degli spin prodotto dal flusso turbolento che si crea nelle stenosi e da effetti di volume parziale . 
questo effetto risulta accentuato nelle ricostruzioni mip in cui non sempre si riesce a distinguere il ridotto calibro della porzione stenotica del vaso dal segnale di fondo [ 7 ]  . 
1 occlusione dellarteria iliaca esterna sinistra ( freccia ) e stenosi in serie di entrambe le arterie femorali superficiali . an accurate evaluation of the arterial tree from the coeliac trunk to the foot arteries . 
in comparison with conventional angiography , mr offers important advantages in the study of elderly patients with peripheral arterial disease , enabling one to avoid the risks associated with arterial puncture , iodinated contrast material , and radiation . 
this effect increases in the mip reconstructions , in which it is not always possible to distinguish the reduced calibre of the stenotic portion of the vessel from the background signal [ 7 ]  . 
la causa principale della sottostima nei casi da noi esaminati stata data da effetti di volume parziale , anche in questo caso dovuti alla difficolt di rilevare attraverso strati sottili i ridotti calibri dei vasi stenotici [ 6 , 8 ]  . 
langio - rm si rivelata una metodica dotata di alta specificit , ma di inferiore sensibilit , quindi praticamente sovrapponibile alla dsa nella valutazione dei vasi di calibro regolare , mentre in caso di lesione steno - ostruttiva la dsa pi accurata , anche se nel nostro studio abbiamo rilevato una buona concordanza . nessuno dei pazienti ha avuto reazioni alla somministrazione della gadodiamide [ 9 ]  . 
non ci sono stati artefatti da materiale metallico in quanto un solo paziente aveva uno stent hemoban ( nitinolo ) in femorale superficiale destra che per non ha causato alterazioni del segnale . 
alcuni pazienti di questo studio , tutti arteriopatici allo stadio iii e iv di la fontaine ( tranne due ) , hanno avuto difficolt a tollerare limmobilit a causa del dolore , ma questo problema si presentato sia durante lesecuzione dellangio - rm sia durante la dsa . 
per quanto riguarda la sequenza tof , ha fornito una discreta valutazione dei vasi del piede , ma come tipo di sequenza mostra alcune limitazioni : i vasi non perfettamente perpendicolari al piano di acquisizione possono avere una bassa intensit di segnale e simulare una patologia [ 10 ] ; la pulsatilit del flusso pu produrre artefatti se non si utilizza un gating cardiaco ; il flusso retrogrado di alcuni vasi collaterali o ricostruiti pu essere anchesso saturato e mascherare di conseguenza il vero livello dellostruzione o sovrastimare la lunghezza del segmento stenotico [ 11 , 12 ]  . solo 15 dei pazienti esaminati ha potuto eseguire questo tipo di sequenza a causa dei gi citati problemi legati allimmobilit in posizione supina . 
mra proved to have higher specificity but lower sensitivity and is therefore practically identical to dsa in the evaluation of normal vessels ; however , in the case of steno - obstructive lesions , dsa is more accurate , even if we recorded a good agreement in our study . 
no patient had a reaction to gadodiamide [ 9 ]  . there were no artefacts due to metallic material , as only one patient had a hemoban stent ( nitinol ) in the right superficial femoral artery , which did not cause signal alterations . a non - negligible limitation of this examination is the immobility requested of the patient . 
some patients in our study , all but two with fontaine stage iii and iv disease , had difficulty keeping immobile because of pain , but this problem arose during both mra and dsa . as regards the tof sequence , despite providing a discrete evaluation of the foot vessels , it does suffer some limitations : vessels not perfectly perpendicular to the acquisition plane may have low signal intensity and simulate disease [ 10 ]  . flow pulsatility can produce artefacts if cardiac gating is not used . 
 the retrograde flow of some collateral or reconstructed vessels can also be saturated and disguise the true level of obstruction or overestimate the length of the stenotic segment [ 11 , 12 ]  . only 15 of our patients could be studied with this sequence because of difficulty lying motionless in the supine position . 
it does , however , have some limitations , some of which will be eliminated by technological advances with fast gradients and specific contrast agents for vascular studies whereas others will remamra may be proposed for selected indications : screening asymptomatic patients with a family history of diabetes or risk factors for atherosclerosis , patients with renal insufficiency , elderly patients , and for surveillance of bypass grafts . conclusions in our experience based on a limited number of patients , mra can be considered an alternative modality to dsa in the management of patients with steno - occlusive disease of the peripheral arteries , as it allows screening of candidates for interventional [ percutaneous angioplasty ( pta ) or stent ] or surgical procedures ( bypass graft )  . the pre - requisite for this is to optimise the injection time on the basis of each patients cardio - circulatory parameters , as also shown by westenberg et al . 
da quanto detto si evince che , nonostante la metodica si sia rivelata sicura , affidabile e sopportabile per la maggior parte dei pazienti , presenta pur sempre dei limiti , alcuni dei quali saranno eliminati dallavanzamento della tecnologia con gradienti ancora pi veloci e mezzi di contrasto dedicati allo studio vascolare , mentre altri invece resteranno invalicabili . 
tutto questo rende langio - rm un esame proponibile solo ad alcuni pazienti : screening nei pazienti asintomatici con familiarit diabetica o con fattori di rischio per aterosclerosi , insufficienza renale , pazienti anziani , controllo di bypass . conclusioni nella nostra esperienza , limitata al numero di casi da noi studiati , langio - rm pu essere considerata una metodica alternativa alla dsa nel management dei pazienti con patologia steno - ostruttiva del circolo arterioso periferico , selezionando i candidati a procedura interventistica ( pta o stent ) o chirurgica ( bypass )  . la condizione imprescindibile su cui si fonda questa affermazione lottimizzazione del tempo di iniezione ad ogni singolo paziente , in base ai suoi parametri cardio - circolatori come dimostrato anche da westenberg et al . 
bacci1 1sezione di chemioterapia , 2servizio di radiologia , dipartimento di oncologia muscoloscheletrica , istituti ortopedici rizzoli , via pupilli 1 , i - 40136 bologna , italy correspondence to : a . 
between march 1997 and december 2001 at our department of musculoskeletal oncology , 231 patients with peripheral osteosarcoma received a central venous catheter to allow infusion therapy and blood sampling . 
in ten cases ( 4.3% ) , radiology showed damage to the alveolar interstitium typical of inflammatory forms , whereas in the remaining three ( 1.3% ) it depicted nodular opacities , which required differentiation between lung metastases and septic emboli . 
the most common complications of the use of central venous catheters include infection and venous thrombosis whereas pulmonary septic emboli are rare . key words osteosarcoma pulmonary metastases pulmonary nodules differential diagnosis riassunto obiettivo . 
da marzo 1997 a dicembre 2001 , presso il nostro dipartimento di oncologia muscoloscheletrica stato inserito un catetere venoso centrale per permettere terapia infusionale e prelievi ematici a 231 pazienti affetti da osteosarcoma periferico . 
in 10 casi ( 4 , 3% ) il quadro radiologico era di impegno interstizio alveolare tipico delle forme flogistiche , mentre nei restanti 3 ( 1 , 3% ) si osservarono delle opacit nodulari che posero problemi di diagnosi differenziale fra metastasi polmonari ed emboli settici . 
le complicanze pi frequenti dellutilizzo del catetere venoso centrale sono le infezioni e le trombosi venose , mentre gli emboli settici polmonari sono rari . parole chiave osteosarcoma metastasi polmonari noduli polmonari diagnosi differenziale introduction introduzione the use of hickman , broviac and groshong indwelling central venous catheters ( cvcs ) , which remain in place for months or years , is highly important for cancer patients who require prolonged chemotherapy and support infusion therapies . 
venous catheters connected with their port to a central venous line , such as infuse - a - port or port - a - cath , have also been used with success . 
vein perforation , generally caused by the insertion of the catheter or its incorrect positioning , is fortunately an uncommon immediate or early complication . the most frequent late complications are venous thrombosis of the vessel in which the catheter is positioned and infections . 
the incidence of thrombosis varies between 12% and 74% and is higher in cancer patients [ 1 ]  . the thrombosis may be located in the vessel or in the catheter lumen ; only one - third of thromboses are symptomatic . 
a number of studies [ 24 ] have demonstrated that thrombosis is one of the main risk factors for catheter infection whereas infections occur in 15%20% of cases [ 5 , 6 ]  . septic emboli resulting from catheter infection are a wellknown but uncommon complication , even in children and adolescents [ 6 , 7 ]  . the central venous line is a very important tool for delivering chemotherapy , especially in children . 
many studies have demonstrated the usefulness and feasibility of prolonged use , up to years , of a cvc even in children , with an acceptable incidence of complications : displacement , occlusion and infection [ 710 ]  . 
the aim of this study was to highlight the problems of differential diagnosis and the possible solutions using conventional radiography and computed tomography ( ct )  . materials and methods between march 1997 and december 2001 , the division of chemotherapy of our institution treated 253 patients with adjuvant chemotherapy for primitive bone sarcomas . 
anche i cateteri venosi collegati con la propria porta ad un catetere venoso centrale tipo infuse - a - porth o port - a - cath sono impiegati con successo . entrambi i tipi di cateteri sono associati a possibili complicazioni sia precoci che tardive . 
alcuni studi [ 24 ] hanno dimostrato che la trombosi uno dei principali fattori di rischio per linfezione del catetere venoso centrale , mentre le infezioni sono una complicanza che si verifica in circa il 15%20% dei casi [ 5 , 6 ]  . 
gli emboli settici conseguenti a infezioni del catetere sono una complicanza ben conosciuta , pur se non frequente , anche nei pazienti pediatrici od adolescenti [ 6 , 7 ]  . il catetere venoso centrale uno strumento molto importante per la somministrazione della chemioterapia in particolare nei bambini . 
molti studi hanno dimostrato lutilit e la fattibilit di un uso prolungato , talora per anni , del catetere venoso centrale anche in pazienti pediatrici con una percentuale accettabile di complicanze : dislocazioni , occlusioni ed infezioni [ 710 ]  . 
lo scopo del lavoro di evidenziare le problematiche di diagnosi differenziale e le possibilit di soluzione mediante radiologia tradizionale e tomografia computerizzata ( tc )  . materiali e metodi dal marzo 1997 al dicembre 2001 , presso lunit operativa di chemioterapia del nostro istituto sono stati trattati con chemioterapia adiuvante per osteosarcoma primitivo 253 pazienti ; 34 di questi pazienti presentavano metastasi alla diagnosi : 31 al polmone e 3 in altri segmenti ossei ; in 219 pazienti la lesione era localizzata . 
a 231 pazienti fu inserito un catetere venoso centrale : 228 cvc tipo broviac e 3 port - a - cath ; 22 pazienti tutti adulti rifiutarono il posizionamento del catetere . 
a second radiological assessment of the primary cancer with ct and mri , and chest ct was performed at the end of preoperative chemotherapy ( lasting four to six cycles , depending on the protocol ) , and before surgery . 
given the prolonged anticancer treatment typical of osteosarcoma ( 3643 weeks , depending on the protocol ) , conventional chest radiography was performed every 2 months to exclude the development of metastasis . in order to prevent catheter occlusions , 5 cc of heparin solution ( 20 cc of saline plus 3 cc of sodium heparin equal to 5 , 000 iu diluted in 100 cc of saline ) was injected into the central venous line every other day . 
patients with neutropoenia ( neutrophils < 500 / mm3 ) received granulocyte colony stimulating factors ( gcsf ) , together with a broad - spectrum antibiotic such as trimethoprim , sulfamethoxazole or ceftriaxone , at a dose of 5 g / kg per day until the white blood cell count ( wbc ) reached a concentration of at least 10 , 000 / mm3 . 
he received neoadjuvant chemotherapy from july 1998 to june 1999 after a broviac central venous catheter had been positioned in the left subclavian veone week after the last chemotherapy cycle ( cisplatin ) , the patient developed chills and fever ( 39c ) while at home . 
central and peripheral blood cultures were performed , both of which were positive for staphylococcus aureus and , on the basis of the antibiogram , antibiotic therapy with 200 mg / day teicoplanin was started , leading to remission of the fever . 
three weeks , later the patient was admitted for removal of the cvc and final staging with lung ct . the material sampled from the catheter after removal showed colonies of s . 
ct , performed on the same day ( 20 july 1999 ) , revealed the presence of a nodular opacity in the posterior segment of the lower right lobe that was suggestive of pulmonary metastasis from osteosarcoma teteri , usati sia per la somministrazione della chemioterapia che per prelievi ematici , furono posizionati prima dellinizio dei cicli di chemioterapia , previo consenso informato . tutti i pazienti ricevettero chemioterapia secondo i protocolli in uso al momento , ior / os - n4 o ior / os - n5 , impiegati dal 1997 al 2001 con i seguenti farmaci : adriamicina , cisplatino , ifosfamide , pi metotrexate nei pazienti al di sotto dei 40 anni ( precedentemente riportati in dettaglio [ 11 , 12 ] )  . la stadiazione radiologica di base comprendeva tc e rm del tumore primitivo osseo , scintigrafia ossea e tc del torace per escludere lesioni sostitutive secondarie polmonari . una seconda valutazione radiologica con tc ed rm del tumore primitivo e tc del torace stata eseguita al termine della chemioterapia preoperatoria ( durata 46 cicli a seconda del protocollo ) , prima dellintervento chirurgico . 
dato il prolungato trattamento antiblastico tipico dellosteosarcoma ( da 36 a 43 settimane a seconda del protocollo ) uno studio radiologico tradizionale del torace veniva eseguito ogni 2 mesi per escludere la comparsa di metastasi . a scopo profilattico , per evitare occlusioni del catetere , a giorni alterni si iniettavano nel catetere venoso centrale 5 cc di soluzione eparinata ( 20 cc di soluzione fisiologica pi 3 cc di eparina sodica pari a 5000 ui diluiti in 100 cc di soluzione fisiologica )  . 
in caso di neutropenia ( neutrofili inferiori o uguali a 500 / mm3 ) fattori stimolanti la crescita di colonie ( gcsf ) , congiuntamente ad un antibiotico ad ampio spettro tipo trimethoprim , sulfametoxazolo o cefriaxone , venivano somministrati ai pazienti alla dose di 5g / kg / die fino a che la concentrazione dei globuli bianchi ( wbc ) non raggiungeva il valore di 10000 / mm3 . tredici pazienti su 231 ( 5 , 6% ) svilupparono uninfezione del catetere venoso centrale . 
in 10 pazienti ( 4 , 3% ) lindagine radiologica tradizionale e / o la tc del torace evidenziarono un impegno interstizio - alveolare tipico delle forme flogistiche e nei restanti 3 ( 1 , 3% ) opacit nodulari , alcune delle quali a margini regolari che posero problemi di diagnosi differenziale con lesioni metastatiche . caso 1 maschio , 7 anni , con osteosarcoma osteoblastico localizzato allomero destro . 
una settimana dopo lultimo ciclo di chemioterapia ( cisplatino ) , il paziente ebbe , a domicilio , un episodio di febbre ( 39c ) con brividi ; esegu due emocolture : una da prelievo centrale e una da prelievo periferico . 
although the patient was asymptomatic , the recent cvc infection was thought to have caused the spread of a septic embolus to the lung , so antibiotic therapy with teicoplanin ( 200 mg / day ) was administered for a further 15 days . 
shortly after the end of the last cycle of postoperative chemotherapy , he developed a fever ( 40c ) and was treated at home with a broad - spectrum antibiotic that failed to resolve the fever . two - view chest radiography performed at the patients home was negative . 
on june 15 , the patient was admitted , and the cultures of material sampled from the central venous line and a peripheral vein both revealed the presence of pseudomonas fluorescens sensitive to piperacillthe central venous line was removed . 
poco dopo il termine dellultimo ciclo di chemioterapia postoperatoria , ebbe febbre ( 40c ) e inizi a domicilio terapia antibiotica a largo spettro che non ne determin la remissione . il radiogramma tradizionale del torace eseguito in due proiezioni al domicilio del paziente era negativo . 
il 15 giugno il paziente fu ricoverato e le emocolture del materiale prelevato dal catetere centrale a da vena periferica evidenziarono entrambe la presenza di psudomonas fluorescens sensibile alla piperacillina . 
nello stesso giorno il paziente esegu , come da protocollo , tc del torace di fine cura , che evidenzi la presenza di tre opacit nodulari nel polmone destro : la prima nel segfig . 
1a , b the first computed tomography ( ct ) study shows a nodular opacity measuring 15 mm in diameter with slight irregular margins in the posterobasal segment of the right lower lobe ( a )  . 
1a , b il primo esame evidenzia una opacit nodulare di 15 mm di diametro a margini leggermente irregolari nel segmento posterobasale del lobo inferiore di destra ( a )  . 
2a - d the first computed tomography ( ct ) study shows three subpleural nodular opacities ( arrows ) , two measuring a few millimetres : the first has paracardiac location in the middle lobe and no feeding vessel sign ; the second is in the laterobasal segment of the right lower lobe ( a ) ; the third is larger and located in the posterobasal segment of the right lower lobe ( b )  . 
2a - d il primo esame tc evidenzia tre opacit nodulari subpleuriche ( frecce ) di cui due millimetriche : la prima localizzata in sede paracardiaca a livello del lobo medio senza il segno del vaso che nutre , la seconda nel segmento laterobasale del lobo inferiore destro ( a ) , la terza opacit , di dimensioni superiori , nel segmento posterobasale del lobo inferiore di destra ( b )  . 
dopo somministrazione di terapia specifica , il secondo esame tc eseguito tre mesi dopo , non evidenzia pi alcuna lesione ( c , d )  . case 3 a 17 - year - old girl with fibroblastic osteosarcoma of the right femur . 
chest radiography demonstrated two nodular opacities in the middle third of the right lung field , both of which where strongly suspicious for metastases . chest ct performed immediately confirmed the presence of the lesions , which were subpleural and with slightly irregular margins , one in the anterior segment and the other in the posterior segment of the lower lobe . 
chemioterapia neoadiuvante dal dicembre 2000 attraverso un catetere centrale tipo broviac . terminato il nono ciclo di chemioterapia , la paziente ebbe un episodio di neutropenia febbrile risoltosi con somministrazione di terapia antibiotica a largo spettro e di fattori stimolanti la crescita . 
la tc del torace eseguita immediatamente conferm la presenza delle due lesioni entrambe subpleuriche e con margini lievemente irregolari , una nel segmento anteriore e laltra nel segmento posteriore del lobo inferiore . 
la paziente a tuttoggi viva , senza lesioni sostitutive . discussione losteosarcoma un tumore osseo estremamente maligno tipico dei bambini e degli adolescenti con un picco tra i 15 ai 25 anni [ 13 ]  . 
il polmone rappresenta , infatti , la pi frequente sede ( 90% di tutte le sedi di metastasi ) di metastasizzazione di questo tumore alla diagnosi e durante il follow - up [ 17 ]  . 
3a - c the first computed tomography ( ct ) study shows two subpleural nodular opacities ( arrows ) : the first in the apical segment of the right lower lobe ; the second , clearly inflammatory , in the lateral segment of the middle lobe ( a )  . 
the second ct study performed after 20 days shows disappearance of the two opacities , with moderate residual subpleural fibrosis in the middle lobe and the presence of a new opacity with irregular and fluffy margins contiguous with a pulmonary vessel in the posterolateral segment of the right lower lobe ( b )  . 
3a - c il primo esame tc evidenzia due opacit nodulari subpleuriche ( frecce ) : la prima nel segmento apicale del lobo inferiore destro , la seconda chiaramente flogistica nel segmento laterale del lobo medio ( a )  . 
il secondo esame tc , eseguito a 20 giorni di distanza , mostra la scomparsa delle due opacit con modesto esito fibrotico subpleurico nel lobo medio e la presenza di unaltra opacit , a contorni irregolari e sfrangiati in continuit con un vaso polmonare nel segmento posterolaterale del lobo inferiore destro ( b )  . 
the lung is often the first site of metastatic spread of many solid tumours [ 16 ] , and this is particularly true for osteosarcoma . the lung is the most frequent site of metastasis ( 90% of all metastasis sites ) of this tumour at presentation and during follow - up [ 17 ]  . osteosarcoma of the extremities tends to metastasize within the first 5 years of diagnosis in 30%40% of cases [ 13 ]  . 
early diagnosis of such lesions may in some cases dramatically increase the survival of patients after appropriate treatment : thoracic surgery and / or chemotherapy . all osteosarcoma protocols require ct scans at baseline and after treatment and conventional chest radiography every 2 months during chemotherapy . 
despite not having the same reliability as ct in detecting metastasis , conventional chest radiography in two views anteroposterior ( ap ) and laterolateral ( ll ) is just as effective in identifying metastatic lesions with a diameter of 1 cm or more , it is easy to perform and it is inexpensive . 
in addition , entrance dose and absorbed dose are much lower than in ct : 1.9 mgy / msi versus 30 mgy / msi , ctdiw / 650 mgy / msi - cm dlp . development of lung metastases during treatment is a rare but possible occurrence . 
mediastinal lymph nodes are rarely involved [ 13 ]  . oncological patients who are free of disease may , however , develop pulmonary nodules of varying size , shape and location , as has been reported by many studies [ 1824 ]  . 
almost all of cases reported were treated either with drugs with minimal bone marrow toxicity and high pulmonary toxicity or drugs and radiotherapy [ 19 ]  . many underwent segmental or lobar resection . 
histology revealed not only metastatic nodules but also the presence of nodular lesions of other natures : nodular nonspecific intersitial pneumonia or fibrosis in patients with peripheral infusion of drugs with high pulmonary toxicity , such as bleomycin [ 2024 ] or nodular lesions caused by infection by opportunistic organisms ( cryptococcus neoformans , aspergillus fumigatus , or others ) in patients treated with radiotherapy who became immunocompromised . infectious processes may also include septic emboli developing inside the cvc or migrating there from other sites . 
the finding of areas of pulmonary consolidation of varying shape on ct scans of cancer patients represents a challenge , and the differential diagnosis is one of the radiologists routine tasks . 
 lung nodules identified in our three patients were both subpleural and parenchymal ; they had similar density but ri metastatici osservati su un radiogramma del torace e / o una tc del torace in pazienti con tumore primitivo extrapolmonare da considerarsi segno prognostico infausto . 
una diagnosi precoce di lesioni sostitutive pu talora dare lopportunit di una lunga sopravvivenza al paziente dopo adeguata terapia : chirurgia toracica e / o chemioterapia . tutti i protocolli per gli osteosarcomi richiedono una tc di base allinizio del trattamento , unaltra alla fine e radiogrammi tradizionali del torace ogni due mesi durante il lungo periodo della chemioterapia . 
il radiogramma tradizionale del torace in due proiezioni ( p - a e l - l ) pur non avendo la stessa affidabilit della tc nel rilevare metastasi egualmente efficace nellevidenziare lesioni sostitutive di diametro pari o superiore al centimetro , di facile esecuzione , poco costoso , inoltre la dose allingresso / dose assorbita sono di molto inferiori a quelle di una tc : 1 , 9 mgy / msi versus 30 mgy / msi , ctdiw / 650 mgy / msi - cm dlp . 
i linfonodi mediastinici sono raramente coinvolti [ 13 ]  . tuttavia in pazienti neoplastici liberi da malattia possibile osservare la comparsa di noduli polmonari di dimensioni , forma e sede variabile ; tale comparsa stata descritta in molti lavori [ 1824 ]  . 
quasi tutti questi pazienti sono stati trattati o solo con farmaci a minima tossicit midollare ed ad alta tossicit polmonare o con farmaci e radioterapia [ 19 ]  . molti di questi pazienti furono sottoposti a resezione chirurgica segmentaria o lobare . 
lesame istologico rivel non solo la presenza di noduli metastatici , ma anche la presenza di lesioni nodulari di differente natura : polmoniti interstiziali nodulari aspecifiche e fibrosi polmonare interstiziale nodulare in pazienti con infusione periferica di farmaci ad alta tossicit polmonare come la bleomicina [ 2024 ] o lesioni nodulari di natura infettiva provocate da organismi opportunisti ( criptococcus neoformans , aspergillus fumigatus o altri ) in pazienti precedentemente trattati con radioterapia e divenuti ospiti immunocompromessi . 
i sintomi clidifferent shape , being rounded or lobulated but never reticular ; their margins were smooth and regular or fluffy and irregular , but never hazy ; size varied between 3 mm and 25 mthe two patients in whom the catheter was removed immediately and s . 
lung metastases from any primary cancer are well - marginated nodular opacities that are at times very calcific ( especially in osteosarcoma ) ; they tend to have peripheral location but have no predilection for the upper , middle or lower lobes [ 25 ]  . in our three cases , all pulmonary nodules simulating metastases appeared during chemotherapy in patients with broviac cvcs positioned in the subclavian vein for the delivery of chemotherapy , transfusions or blood sampling . 
none of the three patients had symptoms of pulmonary embolism . three cases of pulmonary septic embolism out of 231 patients with cvc is indeed a small percentage ( 1.3% ) , in agreement with other studies [ 6 ]  . 
pulmonary infection could have been the cause rather than the consequence of cvc infection but , given that culture of material retrieved from the distal lumen of the catheter was positive in two out of three cases , the cause of the haematopulmonary infection was far more likely to have been the cvc . the three cases described demonstrate that cvc infection can cause pulmonary septic embolism with variable imaging features . 
le metastasi polmonari , qualunque sia lorigine del tumore primitivo , sono opacit nodulari a margini netti , ben definiti , talora molto calcifiche ( specialmente nellosteosarcoma ) ; sono generalmente localizzate perifericamente ma senza predilezione di sede tra lobo superiore , medio od inferiore [ 25 ]  . nei nostri tre pazienti tutti i noduli polmonari che simulavano metastasi apparvero in corso di chemioterapia in pazienti con catetere venoso centrale tipo broviac inserito in una vena succlavia ed utilizzato per chemioterapia , trasfusioni o prelievo ematico . 
tre casi di emboli settici polmonari su 231 pazienti portatori di cvc una piccola percentuale ( 1 , 3% ) , in accordo coi risultati di altri studi [ 6 ]  . 
la flogosi polmonare potrebbe essere stata la causa e non la conseguenza dellinfezione del catetere venoso centrale , ma dal momento che lesame colturale effettuato sul materiale prelevato dal lume distale del catetere fu positivo in due dei tre casi , sembr estremamente pi probabile che la causa dellinfezione emato - polmonare fosse il catetere venoso centrale . 
nondimeno , aree polmonari di aumentata densit , in soggetti neutropenici e portatori di catetere venoso centrale deve suggerire , tra le altre ipotesi diagnostiche , la possibilit di unembolizzazione settica nodulare secondaria alla presenza ed allinfezione del catetere venoso centrale . 
in addition , the specificity of ct in evaluating the nature of a pulmonary nodule , especially when small , is still limited , and only biopsy or nodule excision are able to reveal the benign or malignant nature of the nodule through histological examination whereas evolution of the radiological finding can only guide the diagnosis between benign or malignant nodular opacities [ 26 ]  . conclusions correct diagnosis of a pulmonary opacity is fundamental for the prognosis and choice of treatment ( surgical ) in a patient with a doubtful lung lesion . 
 in the presence of a cvc , any change in shape ( rounded , lobulated , irregular , fluffy ) in relationship with a vessel ( contiguous , distal ) and in location ( apical , medial , basal ) of an area of lung consolidation seen on serial ct scans , both during and after chemotherapy , is an important clue for pulmonary septic embolism secondary to cvc infection regardless of antibiotic treatment . catheter replacement , central and peripheral blood cultures , administration of specific antibiotic treatment based on blood cultures and ct follow - up of nodular opacities must always be given priority with respect to surgical treatment . mento che possono essere normali o non specifici [ 22 ] come pure laspetto radiologico di noduli polmonari a differente eziologia . 
inoltre la specificit della tc , nella valutazione di natura , benigna o maligna , di un nodulo polmonare , specialmente se questo di piccole dimensioni , ancora limitata e solo la biopsia o lasportazione del nodulo sono in grado di rivelare la vera natura della lesione permettendone lesame istologico , mentre levoluzione del reperto radiologico pu unicamente orientare la diagnosi tra opacit nodulare benigna o maligna [ 26 ]  . conclusioni la corretta diagnosi di una opacit polmonare di vitale importanza per la prognosi ed il differente trattamento terapeutico ( chirurgico ) nel caso di paziente con lesione polmonare dubbia per metastasi . 
simonetti1 1dipartimento di diagnostica per immagini e radiologia interventistica , universit degli studi di roma tor vergata , roma , italy 2sezione di medicina nucleare , universit degli studi di roma tor vergata , roma , italy correspondence to : g . 
sergiacomi , policlinico tor vergata , viale oxford 81 , i - 00133 roma , italy , tel . : + 39 - 06 - 20902372 , fax + 39 - 06 - 20902404 , e - mail : sergiacomigianluigi@tin.it received : 22 march 2005 / accepted : 23 august 2005 / published online : 3 march 2006 abstract purpose . 
the purpose of this study was to evaluate efficacy of multislice computed tomography ( msct ) and single photon emission computed tomography ( spect ) - ct with tc - 99m sestamibi in the assessment of solitary pulmonary nodules of uncertain significance . 
between september 2003 and august 2004 , 23 patients with a solitary pulmonary nodule detected on ct underwent spect - ct using tc - 99m sestamibi as a radiotracer . nodules with positive scintigraphy were immediately subjected to biopsy or surgical resection . 
scopo del nostro studio valutare lefficacia diagnostica dellutilizzo della tomografia computerizzata multistrato ( tcms ) e della spect - tc con tc - 99m sestamibi nella gestione di lesioni nodulari polmonari di incerto significato . 
ventitre pazienti , nel periodo tra settembre 2003 e agosto 2004 , con un nodulo polmonare solitario sospetto , hanno eseguito una tcms del torace e successiva spect - tc utilizzando come radiotracciante il tc - 99m sestamibi . 
ci potrebbe permettere di anticipare la tipizzazione istologica e leventuale trattamento chirurgico in pazienti con nps riscontrato allesame tc del torace . parole chiave tc multistrato nodulo polmonare sestamibi spect g . 
this technique can now perform thinslice imaging of the lung parenchyma , and it employs software providing information on size , volume , density and contrast enhancement of pulmonary nodules as well as calculating automatically and accurately any change in size by comparing studies conducted at different times . a few nodules can be defined as probably benign ( presence of fat or benign calcification ) and not requiring further investigation ; others are highly suspicious for malignancy ( spiculated margins , malignant calcification , diameter > 2 cm ) and require immediate surgical excision or biopsy [ 1 ]  . 
the majority of pulmonary nodules ( 70% ) , however , cannot be characterised with certainty , even after a ct scan . encouraging results in lung cancer diagnosis have been obtained with single photon emission computed tomography ( spect ) using 99mtc - hexakis - 2 - methoxy - isobutyl - isonitrile ( sestamibi ) , a lipophilic cation used in myocardial perfusion scintigraphy [ 24 ]  . this technique currently makes use of new devices equipped with an x - ray tube - detector system for ct scans . scintigraphy is carried out using a hybrid g - camera allowing acquisition of spect and ct images during the same session . 
preliminary results of the clinical application of this new diagnostic tool in the study of different neoplasms , including thoracic applications , have been very interesting [ 5 , 6 ]  . 
this allows for a more effective and accurate preclinical diagnosis of disease , given that the early diagnosis of lung cancer is still the only means to improve patient survival [ 7 , 8 ]  . 
our aim was to correlate the results of msct and sestamibi spect - ct in the early diagnosis of lung cancer and to assess their concordance with histological examination . materials and methods between september 2003 and august 2004 , we selected 23 patients ( 17 men and six women ) aged between 40 and 82 years ( mean age 63.2 ) with an spn ranging from 0.8 cm to 2 cm in size ( mean size 1.3 cm ) discovered at ct performed to investigate a chest radiography finding or as a diagnostic examination for another condition . our study excluded nodules with tomodensitometric characteristics highly suggestive of either benign or malignant disease . 
the examinations were conducted with a lightspeed 16 msct scanner ( ge medical systems , milwaukee , wi , usa ) capable of obtaining slice thicknesses between 10 mm and 0.625 mthe examination was performed durla diagnostica per immagini ha raggiunto , grazie agli imponenti progressi tecnologici , importanti risultati nella valutazione del nodulo polmonare solitario ( nps ) con lausilio della tomografia computerizzata multistrato ( tcms )  . 
attualmente tale tecnica in grado di poter eseguire esami sul parenchima polmonare a strato sottile e si avvale di software in grado di fornire informazioni su dimensioni , volume , densit e contrast enhancement delle nodularit polmonari nonch di calcolarne automaticamente in modo accurato le modificazioni dimensionali , comparando esami eseguiti in tempi diversi . 
alcuni noduli possono essere definiti come benigni con alta probabilit ( presenza di grasso o calcificazioni benigne ) e non richiedere ulteriori approfondimenti ; altri risultano altamente sospetti per malignit ( margini spiculati , calcificazioni maligne , diametro superiore a 2 cm ) e richiedono immediata escissione chirurgica o biopsia [ 1 ]  . 
ciononostante la maggior parte dei noduli polmonari ( 70% ) non sono caratterizzabili con certezza anche dopo un esame tc . incoraggianti risultati nella diagnostica della neoplasia polmonare sono stati ottenuti con la tomografia computerizzata ad emissione di singolo fotone ( spect ) con lutilizzo di tc - 99m - hexakis - 2 - metossi - isobutil - isonitrile ( sestamibi ) , un catione lipofilico in uso nella diagnostica scintigrafica miocardica perfusionale [ 24 ]  . 
i risultati preliminari dellimpiego clinico di questa nuova apparecchiatura diagnostica nello studio di diverse neoplasie , comprendendo alcune applicazioni anche a livello toracico , si sono dimostrati molto interessanti [ 5 , 6 ]  . 
tutto ci ci consente di fare una diagnosi pre - clinica di malattia molto pi efficace e accurata , dato che la diagnosi precoce delle neoplasie del polmone rimane lunico mezzo per aumentare la sopravvivenza dei pazienti affetti [ 7 , 8 ]  . il nostro studio incentrato sulla caratterizzazione di lesioni nodulari solitarie di incerto significato rinvenute allesame radiografico del torace , o incidentalmente durante lesecuzione di esami tc , integrando lesame scintigrafico con le informazioni fornite dalla tcms . 
lo scopo correlare i risultati forniti dalla tcms e dalla spect - tc con sestamibi nella diagnosi precoce del cancro polmonare e valutarne la concordanza con lesame istologico . materiali e metodi nel periodo compreso tra settembre 2003 e agosto 2004 sono stati selezionati 23 pazienti di cui 17 uomini e 6 donne di et compresa tra i 40 e 82 anni ( et media 63 , 2 anni ) , con un nps di dimensioni comprese fra 0 , 8 e 2 cm ( dimensioni medie 1 , 3 cm ) , individuato mediante esame tc , eseguito come approfondimento diagnostico di una precedente radiografia del torace o come accertamento diagnostico per altra patologia . 
images were processed on an advantage w 4.1 workstation supplied by the same company using multiplanar reconstructions ( mpr ) , volume rendering ( vr ) and automatic segmentation software ( ala ) , which provides an accurate assessment of size , shape and density once the operator has selected the region of interest and performed three - dimensional ( 3d ) segmentation with removal of adjacent structures . volume and morphology data obtained at the first measurement were compared with those of the follow - up examinations . 
risk assessment was not performed on 2d criteria , such as changes in lesion diameter , but on 3d criteria , so that when the volume doubles , the lesion diameter actually increases by only 26% . all patients then underwent ( within 5 days ) lung scintigraphy with positive indicator using a vg millennium ( ge medical systems ) dual - head gamma camera equipped with an x - ray tube - detector system similar to a third - generation ct [ 9 ]  . 
this hybrid system has shown to improve the diagnostic accuracy of a large number of spect examinations [ 5 ]  . twenty minutes after the iv administration of about 740 mbq of tc - 99m sestamibi , spect - ct of the chest was performed . 
after prefiltering with a metz filter , the spect images were reconstructed in a ramp filter in order to produce transaxial sections from which coronal and sagittal images were derived . patients with positive nodules at scintigraphy underwent invasive procedures for histological characterisation ( ctguided or bronchoscopic biopsy , video - assisted thoracoscopic excision )  . patients with negative nodules at scintigraphy underwent repeat ct after 34 months with reassessment of volume by means of ala software and subsequent histological characterization ( ct - guided or bronchoscopic biopsy , video - assisted thoracoscopic excision )  . in these cases , follow - up ct was always performed with the same acquisition parameters as the first examinacon caratteristiche tomodensitometriche altamente probanti per benignit o malignit . 
gli esami sono stati condotti con una tc multistrato light - speed 16 ( ge medical systems , milwakee , wi , usa ) in grado di ottenere spessori di strato variabili da 10 mm a 0 , 625 mlesame stato effettuato in ununica apnea prima e dopo somministrazione di mezzo di contrasto organo - iodato non ionico ( 80100 ml , flusso di 34 ml / s , ritardo di 2530 s dallinizio della somministrazione ) previo consenso informato del paziente , con i seguenti parametri tecnici di acquisizione : spessore di strato pari a 5 mm ( retroricostruibile fino a 0 , 625 mm ) , velocit di avanzamento 11 , 25 mm / rotazione , tempo di rotazione di 0 , 5 s , tempo complessivo di acquisizione pari a 1215 s , 120140 kv , 200240 ma . 
le immagini sono state successivamente rielaborate su una workstation advantage w 4.1 fornita dalla stessa ditta mediante ricostruzioni multiplanari ( mpr ) , volumetriche ( vr ) e software di segmentazione automatica ( ala ) che permette , selezionando la regione di interesse ed effettuando una segmentazione tridimensionale con eliminazione delle strutture adiacenti , di ottenere una corretta valutazione di dimensioni , forma e densitometria . 
i valori ottenuti con le prime rilevazioni sono stati confrontati con quelli dei follow - up successivi , utilizzando come elemento di comparazione il criterio volumetrico accanto a quello morfologico . 
laccertamento del rischio non viene effettuato sulla base di elementi bidimensionali , come le modificazioni del diametro della lesione , ma si fonda su criteri tridimensionali , cos quando il volume raddoppia , il suo diametro aumenta in realt solo del 26% . tutti i pazienti sono stati successivamente ( entro 5 giorni ) sottoposti a tomoscintigrafia polmonare con indicatore positivo , impiegando una gamma camera a doppia testata vg millenium ( ge medical systems , milwakee , wi , usa ) equipaggiata con un complesso tubo radiogeno - detettori analogo ad una tc di iii generazione [ 9 ]  . 
per la spect sono state acquisite 120 immagini planari ( una ogni 3 ) della durata di 25 s ognuna su un arco di rotazione di 360 , utilizzando una matrice 128x128 . 
subito dopo , senza muovere il paziente dal lettino della gamma camera , stata effettuata una tc a bassa risoluzione del torace , su un campo di vista di 40 cm , esattamente uguale a quello acquisito dalla spect . 
i parametri utilizzati da questa tc sono fissi e non modificabili dalloperatore : spessore di strato di 1 cm , tempo di acquisizione pari a circa 14 s per sezione , 140 kv e 2 , 5 ma . 
le immagini spect e tc ottenute sono state elaborate in una workstation dedicata ( integra , ge medical system ) che permette in maniera rapida di ottenere una fusione precisa delle corrispondenti sezioni dei due studi , funzionale ( spect ) ed anatomico ( tc )  . 
dopo una pre - filtrazione con un filtro di metz , le immagini spect sono state ricostruite in un filtro a rampa per produrre sezioni transassiali , dalle quali sono state poi ottenute le immagini coronali e sagittali . 
ct computed tomography , spect single photon emission computed tomography patient size ( spn ) , cm site ( spn ) spect histology age , years a + / - , indeterminate ; - , doubt about its benignity ; + , doubt about its malignancy r , right ; l , left lower r lobe lingula lower r lobe lower r lobe upper l lobe upper l lobe upper l lobe lower r lobe l hilar lower r lobe lingula lower r lobe lower r lobe lower r lobe upper l lobe upper r lobe upper r lobe middle lobe upper l lobe upper r lobe upper r lobe middle lobe lower l lobe negative negative negative negative positive negative positive positive positive positive negative positive positive negative positive positive negative negative negative positive negative positive negative fibrous lesion adenocarcinoma fibrous lesion fibrous lesion adenocarcinoma fibrous lesion adenocarcinoma metastasis adenocarcinoma undifferentiated carcinoma fibrous lesion gi granuloma squamous cell carcinoma hamartoma adenocarcinoma adenocarcinoma hamartoma hamartoma granuloma adenocarcinoma granuloma adenocarcinoma granuloma tabella 1 caratteristiche riassuntive dei 23 pazienti con nodulo polmonare solitario : dato radiologico , scintigrafico ed istopatologico paziente dimensioni ( nps ) , cm sede ( nps ) aspetto tca spect istologia et , anni 1 , 5 0 , 8 1 , 1 1 , 0 1 , 5 1 , 5 1 , 0 0 , 9 1 , 2 2 , 0 1 , 0 1 , 2 1 , 4 1 , 3 2 , 0 1 , 5 1 , 4 2 , 0 1 , 0 1 , 1 1 , 1 0 , 9 1 , 3 a + / - , indeterminato ; - , dubbio sulla benignit ; + , dubbio sulla malignit dx , destro ; sn , sinistro lobo inf . 
the smallest lesion ( 0.8 cm ) , this adenocarcinoma , measured 1 cm at ct followup after 3 months , with a significant increase in volume and therefore suspicious for malignancy . table 1 summarises the characteristics of the 23 patients in our study . 
ct indicators of suspected benignity are well - defined contour , nonspiculated margins , fat tissue or calcification in more than 10% of the nodule and contrast enhancement < 20 hu . 
ct indicators of suspected malignancy are blurred contour , spiculated margins , eccentric microcalcifications and contrast enhancement > 20 hu . nodules were considered doubtful as to benignity or malignancy when they showed a prevalence of no more than two criteria whereas they were considered indeterminate when they displayed no prevalence of any of the classification criteria . on the basis of the correlation between the scintigraphic and histological results , the sestamibi spect - ct scan had 90.9 % sensitivity ( se ) , 91.6 % specificity ( sp ) , diagnostic accuracy of 91.3 % with positive predictive value ( ppv ) of 90.9 % and negative predictive value ( npv ) of 91.6 % ( table 2 )  . in evaluating the scintigraphic scan , the simultaneous ct acquisition was always decisive in identifying nodular lesions with no uptake and contributed to the differential diagnosis in nodules with uptake located in perihepatic sites . spect acquisition alone without the aid of the anatomical ct images was decisive in all enhancing lung lesions other than those with perihepatic distribution . 
the ct scan with volumetric evaluation after 34 months showed absolute concordance with the histological findings ( table 3 )  . i pazienti portatori di noduli non captanti alla tomoscintigrafia sono stati sottoposti ad un nuovo controllo tc a distanza di 34 mesi con rivalutazione volumetrica mediante software ala e successiva tipizzazione istologica ( biopsia tc guidata o broncoscopica , escissione videotoracoscopica )  . 
in questi casi lesame tc di controllo stato sempre eseguito rispettando gli stessi parametri di acquisizione dellesame precedente ( kv , ma , spessore di strato , intervallo di ricostruzione , ecc ) al fine di ottenere una comparazione attendibile . 
tutti i pazienti , anche quelli portatori di lesioni non captanti rivalutati a 34 mesi , hanno optato , previo consenso informato , per la definitiva caratterizzazione istologica piuttosto che sottoporsi ad ulteriori controlli per un lungo periodo di tempo . risultati dei 23 noduli polmonari solitari rinvenuti allesame tc , 11 sono risultati positivi allesame scintigrafico , 12 sono risultati negativi . 
questultimo , risultata la lesione pi piccola ( 0 , 8 cm ) della nostra casistica , al successivo controllo tc a 3 mesi , presentava dimensioni pari a 1 cm , con un incremento volumetrico significativo e pertanto sospetto per malignit . 
dopo lasportazione chirurgica il referto istologico ha confermato la natura maligna della lesione ( carcinoma anaplastico )  . localizzata nel lobo diagnostic investigation based on standard chest radiography and sputum cytology failed to deliver the expected results in reducing mortality [ 1113 ]  . over the last few years , the concept of early diagnosis of lung cancer has been reconsidered as a following the encouraging results obtained with multidetector computed tomography ( mdct ) [ 8 , 14 , 15 ] and the use complementary nuclear medicine methods . 
indici tc di sospetta benignit sono la presenza di limiti ben definiti , margini non spiculati , presenza di tessuto adiposo o metaplasia calcifica in pi del 10% del nodulo , un contrast enhancement < 20 uh . 
abbiamo classificato le formazioni nodulari come dubbie per benignit o malignit quando presentavano una prevalenza di non oltre 2 criteri , mentre quelle definibili come indeterminate quando non era possibile evidenziare una prevalenza dei criteri classificativi utilizzati . 
extremely rapidly growing masses are probably inflammatory while slowgrowing masses fall under the category of so - called pseudodiseases , a term indicating diseases that never progress over a lifetime either because they do not increase in size and may in fact regress naturally ( type i pseudodiseases ) or bepari a 91 , 6% ( tabella 2 )  . 
la consensuale acquisizione tc nella valutazione dellesame scintigrafico risultata sempre determinante nellindividuazione delle lesioni nodulari non captanti ed ha orientato verso una diagnosi differenziale nei casi di nodularit captanti localizzate in sede peri - epatica . la sola registrazione spect non adiuvata dallimmagine anatomica tc risultata determinante in tutte le lesioni polmonari captanti a distribuzione diversa da quella peri - epatica . 
lo studio tc , mediante valutazione volumetrica a 34 mesi , ha presentato una concordanza assoluta con il dato istologico ( tabella 3 )  . discussione il convenzionale esame radiografico del torace , primo ed essenziale momento diagnostico per tutta la patologia polmonare , non si dimostrato sufficientemente sensibile e specifico per assicurare una diagnosi precoce [ 10 ]  . 
in passato , esami diagnostici basati sulla radiografia standard del torace e sullesame citologico dellescreato non hanno dato i risultati sperati nella riduzione della mortalit [ 1113 ]  . negli ultimi anni si sta assistendo ad una profonda revisione del concetto di diagnosi precoce del cancro del polmone grazie agli incoraggianti risultati ottenuti con la tomografia computerizzata multistrato [ 8 , 14 , 15 ] , ed a tecniche complementari di medicina nucleare . 
nella differenziazione tra lesioni benigne e maligne in tc sono stati individuati criteri qualitativi , basati sulla morfologia del nodulo e quantitativi , rappresentati dalla densit , caratteristiche di enhancement dopo somministrazione di mdc organoiodato e dalla velocit di crescita della lesione nei casi sottoposti a controllo . 
in particolare lassenza di crescita in un periodo di almeno 2 anni un indicatore attendibile di benignit [ 16 ]  . luso del tempo di raddoppio , che per le lesioni sferiche definito come un incremento del 26% del diametro , si basa sullosservazione che le lesioni benigne raddoppiano il proprio volume in un tempo inferiore a 30 gg e superiore a 450 gg . 
infatti , le formazioni a rapidissimo accrescimento sono di probabile significato infiammatorio , mentre quelle a lenta crescita rientrano nel novero della cos detta pseudomalattia ove con tale termine si intenda una malattia che non progredir mai in senso negativo nel corso della vita , o perch non aumenta mai di dimensioni , potendo regredire naturalmente ( pseudomalattia di tipo i ) o perch progredisce cos lentamente che non si svilupperanno mai i sintomi nel corso della vita ( pseudomalattia di tipo ii ) [ 17 ]  . 
un nps che cresca ad una velocit tale che il suo tempo di raddoppio volumetrico previsto si collochi tra i 30 ed i 450 gg deve essere sottoposto ad ulteriori accertamenti in quanto sospetto per malignit . 
the mechanism through which the uptake occurs in cancer cells is still uncertain , and some studies [ 19 ] have suggested a role for the negative potential of cell and mitochondrial membranes , passive diffusion , and the lipophilic nature of methoxyisobutyl isonitrile ( mibi )  . 
in agreement with the literature [ 21 , 22 ] , in all cases examined and subsequently subjected to histopathology , the use of spect with tc - 99m sestamibi often provided support for radiological suspicion , but in selected highly suspicious cases , it prompted surgical excision rather than follow - up . 
the results suggest , consistent with the literature data [ 21 , 22 ] , that sestamibi has a high specificity in the identification of malignant lung lesions . although our preliminary data are based on a small case series and require confirmation by larger studies , they suggest that spect - ct can detect true positive cases at an early stage . 
therefore , the possible inclusion of scintigraphy in the characterisation of spns might lead to ct being reserved for the follow - up of scintigraphically negative lesions only . with regard to sensitivity , spect yielded one false negative result , in an 8 - mm lesion ( the smallest in our series )  . however , even biological factors such as cancer aggressiveness and the possible presence of multidrug resistance may affect results . 
the mechanism for the uptake of tc - 99m sestamibi a lipophilic cation that is taken up by cancer cells is related to regional blood flow and to the activity of mitochondria , where it is almost exclusively concentrated [ 23 , 20 ]  . 
it has also been observed that cancer cells , characterised by chemoresistance , show a rapid washout of tc - 99m sestamibi , which is linked to increased expression of certain membrane p - glycoproteins [ 24 , 25 ]  . the main benefit of spect - ct fusion imaging was , in our experience , the correct characterisation of perihepatic lesions affected by the normal uptake of the radiopharmaceutical by the liver . 
our work , although based on a limited number of patients , confirms preliminary results on the potential of this new technique in the differentiation of lung lesions with lipophilic cationic radiopharmaceuticals based on technetium [ 5 ]  . 
the use of this radiotracer would also assist in cost - benefit decision making for pamibi un radiofarmaco impiegato solitamente nello studio della perfusione miocardica , ma dimostratosi efficace nella diagnostica oncologica . 
il meccanismo attraverso il quale avviene lup - take nella cellula neoplastica ancora incerto ed alcuni studi [ 19 ] suggeriscono il ruolo del potenziale negativo delle membrane cellulari e mitocondriali , della diffusione passiva , e della natura lipofilica del mibi . 
nellambito del nostro studio lapplicazione della spect - tc con tc - 99m sestamibi , sulla base di precedenti in letteratura [ 21 , 22 ] , in tutti i casi da noi esaminati e successivamente sottoposti a diagnosi anatomo - patologica , ha fornito da un lato spesso un conforto al sospetto radiologico , dallaltro , in casi selezionati fortemente sospetti , ha fatto optare per lescissione chirurgica piuttosto che per il follow - up . 
i nostri dati preliminari , ottenuti in una casistica limitata , se confermati in studi successivi con linclusione di un numero maggiore di pazienti , suggeriscono che la spect - tc in grado di identificare precocemente i casi veri positivi . 
per quanto riguarda la sensibilit della spect - tc , va sottolineato che lunico caso risultato falso negativo stato osservato in una lesione di 8 mm ( la pi piccola dimensionalmente nella nostra casistica )  . 
infatti il meccanismo di accumulo del tc - 99m sestamibi , che un catione lipofilico che viene captato dalle cellule neoplastiche , in relazione al flusso ematico distrettuale ed alla attivit mitocondriale , dove si concentra quasi esclusivamente [ 23 , 20 ]  . stato poi osservato che nelle cellule neoplastiche , caratterizzate da chemioresistenza , si ha un rapido wash - out del tc - 99m sestamibi , legato ad unaumentata espressione di alcune p - glicoproteine di membrana [ 24 , 25 ]  . 
il vantaggio pi importante della fusione delle immagini spect - tc , nella nostra esperienza , si avuto nella corretta caratterizzazione delle lesioni peri - epatiche , condizionate dal normale up - take del radiofarmaco da parte del fegato . 
il nostro lavoro , anche se basato su un numero non elevato di pazienti , conferma le acquisizioni preliminari circa le potenzialit di questa nuova tecnica nella diagnostica differenziale delle lesioni polmonari con radiofarmaci cationici lipofilici tecneziati [ 5 ]  . 
lutilizzo di questo radiotracciante sarebbe inoltre di ausilio nellottica decisionale costo - beneficio , nei pazienti che , per la compromessa funzionalit cardio - polmonare , risulterebbero ad alto rischio per una toracotomia . 
another important aspect is that spect is more widely available and less expensive than positron emission tomography - fluorodeoxyglucose ( pet - fdg ) , an examination that is sensitive and specific in diagnosis and staging of lung cancer [ 27 , 28 ] but currently limited by its cost and poor availability . 
pet - fdg , however , has an accuracy of 90% and sensitivity and specificity of 91% and 68% , respectively , in the differential diagnosis of spns [ 29 ]  . 
 ritorio delle apparecchiature ed il basso costo dellesame , se confrontato con la pet - fdg , esame dimostratosi sensibile e specifico nella diagnosi e nella stadiazione delle neoplasie polmonari [ 27 , 28 ] , ma attualmente limitato dai costi e dalla scarsa reperibilit su territorio . 
bazzocchi istituto di radiologia , policlinico universitario a gestione diretta , universit degli studi di udine , via colugna 50 , i - 33100 udine , italy correspondence to : r.m. 
fifty patients with 111 hcc foci ( 61 confirmed histologically , 46 confirmed by percutaneous interventional procedures , four confirmed by ct follow - up of at least 6 months ) underwent mdct with a double arterial phase and a portal venous phase after administration of contrast material with a high iodine concentration ( 400 mgi / ml , 2 ml / kg , 5 ml / s )  . two radiologists independently evaluated the images in three distinct reading sessions ( early arterial phase ( eap ) , late arterial phase ( lap ) and double arterial phase ) to determine presence , number and degree of suspicion of hcc . 
sensitivity and ppv increase progressively when passing from eap to lap to double - arterial - phase images obtained with contrast material with a high iodine concentration . however , the difference in sensitivity between lap and the double arterial phase was not statistically significant . 
cinquanta pazienti con 111 foci di hcc ( 61 confermati istologicamente , 46 tramite procedure intervenzionali percutanee , 4 confermati mediante un follow - up in tc di almeno 6 mesi ) hanno eseguito una tc con una doppia fase arteriosa ed una fase venosa portale con un apparecchio multidetettore dopo somministrazione di mdc ad elevata concentrazione di iodio ( 400 mgi / ml , 2 ml / kg , 5 ml / s )  . 
due radiologi hanno valutato indipendentemente le immagini in tre sessioni di lettura separate ( fase arteriosa precoce ( fap ) , tardiva ( fat ) ed entrambe le fasi arteriose combinate ) per determinare la presenza , il numero ed il livello di sospetto di hcc . 
la sensibilit media ed il vpp per lidentificazione dellhcc sono risultati rispettivamente 83 , 8% e 93 , 5% per la fap , 90 , 5% e 94 , 8% per la fat , 94 , 1% e 95 , 1% per le due fasi arteriose combinate . 
la sensibilit ed il vpp incrementano progressivamente passando dallanalisi delle immagini della fap , a quelle della tardiva e delle due fasi arteriose combinate ottenute con mdc ad elevata concentrazione di iodio . 
as a result , it has only been possible to study the characteristics of the phenomenon since the advent of spiral computed tomography ( ct ) scanners , which permit analysis of the passage of cm in the liver vasculature within seconds of its arrival in the hepatic artery ( during the so - called arterial phase ) [ 39 ]  . 
with the introduction of multidetector ct ( mdct ) scanners , the passage of cm can even be studied by acquiring two arterial phases , one very early [ early arterial phase ( eap ) ] and one immediately after [ late arterial phase ( lap ) ] [ 1013 ]  . 
over the last few years , several studies have attempted to determine whether the contribution of the two arterial phases to the identification of hcc was the same as that of a single arterial phase or whether it improved ct sensitivity in diagnosing hcc [ 11 , 13 ] , or , again , whether either of the two phases was better than the other , making the other redundant . 
some studies found that lap yields a higher sensitivity than eap in identifying hcc [ 13 ] although the use of the two phases in combination improves the final result . 
while there is some agreement on the importance of administering the cm with a sufficiently high flow rate [ 1417 ] , there is no agreement on the optimal concentration and amount of iodine allowing the best visualisation of hcc in the two different phases . 
recently , various studies have compared aortic and hepatic enhancement obtained with cm at different iodine concentrations [ 1822 ] , emphasising the benefits linked to the use of higher iodine concentrations not only to determine a more intense and earlier aortic enhancement but also improved contrast difference between hypervascular lesions and the liver parenchyma [ 19 , 20 , 22 ]  . the purpose of our study was to evaluate whether mdct with double arterial phase and high - iodine - concentration cm increases the techniques sensitivity in the identification of hepatocellular carcinoma . materials and methods the study included 50 consecutive patients ( 32 men , 18 women , aged between 38 and 81 years ; mean age : 68 years ) referred for ct for the suspicion of at least one hcc based on ultrasound findings . 
forty - three patients had histologically confirmed chronic liver disease ( 23 with hepatitis c , 12 with hepatitis b , one with hepatitis b and c , one with primary biliary cirrhosis , six with a toxic - dysmetabolic liver disease ) ; seven patients had a sonographically suspicious lesion without known chronic liver disease . 
all patients gave their informed consent , and the study was approved by our ethics lepatocarcinoma ( hcc ) presenta generalmente una ricca vascolarizzazione arteriosa in seguito a fenomeni di neoangiogenesi intratumorale , direttamente proporzionale al grado di malignit della lesione [ 1 ]  . 
in queste lesioni vi pertanto uninversione del bilancio artero - portale a favore di un incremento dellinput arterioso [ 2 ] , che fa s che il mezzo di contrasto ( mdc ) , giunto attraverso larteria epatica , arrivi molto precocemente allinterno dellhcc ed altrettanto precocemente ne venga dismesso . 
la precocit del fenomeno tale che solo lavvento delle tc spirali , che hanno permesso lanalisi del passaggio del mdc nel fegato e nei suoi vasi nei primi secondi dallarrivo in arteria epatica ( durante cio la cosiddetta fase arteriosa ) , ha consentito di analizzarne le caratteristiche [ 39 ]  . 
lintroduzione delle tc multidetettore ha consentito di poter studiare il passaggio del mdc addirittura mediante lacquisizione di due fasi arteriose , una molto precoce ( fase arteriosa precoce ) ed una immediatamente successiva ( fase arteriosa tardiva ) [ 1013 ]  . 
negli ultimi anni diversi lavori hanno cercato di stabilire se lapporto delle due diverse fasi arteriose nellidentificazione dellhcc fosse sovrapponibile a quello di una singola fase arteriosa , oppure se migliorasse la sensibilit della tc nella diagnosi dellhcc [ 11 , 13 ] ; oppure , ancora , se una sola delle due fasi fosse migliore e rendesse superfluo lapporto dellaltra . 
alcuni lavori hanno sottolineato che la fase arteriosa tardiva fornisce una sensibilit maggiore rispetto a quella precoce nellidentificazione dellhcc [ 13 ] , anche se lassociazione delle due migliora il risultato finale . 
mentre vi un certo accordo nel sottolineare limportanza dellintroduzione del mdc ad un flusso sufficientemente elevato [ 1417 ] , non vi sufficiente accordo nel ritenere quali siano le concentrazioni e la quantit di iodio ottimali per la migliore visualizzazione dellhcc nelle due diverse fasi . 
recentemente , in letteratura sono comparsi diversi studi che hanno confrontato lenhancement aortico ed epatico ottenuto con mdc a differenti concentrazioni di iodio [ 1822 ] , sottolineando i vantaggi nellimpiego di maggiori concentrazioni di iodio non solo nel determinare un enhancement aortico pi intenso e precoce , ma conseguentemente anche una migliore differenza di contrasto tra lesioni ipervascolari e parenchima epatico [ 19 , 20 , 22 ]  . 
lo scopo del nostro lavoro stato valutare se lo studio mediante tc multidetettore con doppia fase arteriosa e mdc ad elevata concentrazione di iodio determini un miglioramento in termini di sensibilit nellidentificazione dellepatocarcinoma . materiali e metodi in questo studio sono stati inclusi 50 pazienti consecutivi ( 32 maschi , 18 femmine ; et compresa tra 38 ed 81 anni ; et media , 68 anni ) inviati allesame tc per il sospetto di almeno un hcc sulla base di reperti ecografici . 
in patients with biopsy - proven hcc , only one nodule was biopsied ; consequently , those patients presenting with other lesions with the same imaging characteristics as the biopsied lesion were considered to be affected by multifocal hcc . 
forty - six nodules in 15 patients were confirmed by response to interventional percutaneous procedures such as chemoembolization , radiofrequency , and alcoholization ( meant as a reduction in size and / or total or partial absence of arterial vascularity at ct follow - up 1 month after the procedure and every 6 months for at least 1 year )  . 
four lesions in four patients were confirmed by ct follow - up alone ( size increase of the lesion and / or increase of the number of nodules at 3 , 6 , 9 and 12 months ) , as the patients poor clinical condition precluded surgery or percutaneous procedures . 
in ten patients without focal hepatic lesions on ct ( suspected at previous ultrasonography ) , absence of the tumour was confirmed by ct follow - up at 6 months from the first examination and negative - fetoprotein test . 
acquisition parameters were as follows : collimation 3 mm , slice thickness 5 mm , reconstruction interval 5 mm , pitch 5.5 ( table feed 33 mm / s ) ; 135 kv ; 175 mas . iodine concentration administered before examination , all patients received 500 ml of water orally and a non - ionic water - soluble contrast agent with a high intravenously ( 400 mgi / ml iomeprol ) ( iomeron 400 , bracco , milan , italy ) at a 5 - ml / s flow rate and a 2 - ml / kg volume ( volume range 100160 ml ; mean 138.5 ml ) using an automatic injector ( envision ct injector , medrad , indianola , pa , usa )  . 
to determine the best time to start the ct scan after administering the cm , we used contrast tracking software ( sure start , toshiba , tokyo , japan ) : a region of interest ( roi ) , which calculates blood density before the cm , is positioned within the abdominal aorta at the level of a plane passing through the diaphragm ; the operator establishes a density threshold in hounsfield units ( hu )  . 
the contrast bolus is then administered and , as soon as the established density threshold is reached , the ct scan starts automatically . three scans of the entire liver were performed with an acquisition time of 710 s ( 9 s on average ) , depending on the craniocaudal diameter of the liver . 
the first scan ( eap ) was obtained in the craniocaudal direction , the second ( lap or portal inflow phase ) in the caudocranial direction with a 5s delay between the two acquisitions . 
tutti i pazienti hanno firmato il consenso informato ; lo studio stato approvato dal nostro comitato etico ed ha seguito i principi della dichiarazione di helsinki [ 23 ]  . in 40 pazienti su 50 stato riscontrato almeno un hcc , per un totale di 111 lesioni ( con un numero medio di lesioni per paziente pari a 2 , 77 )  . 
la conferma istologica di hcc stata ottenuta per 61 noduli in 21 pazienti ( mediante trapianto di fegato per 16 lesioni in 8 pazienti , mediante resezione parziale per 8 lesioni in 4 pazienti , mediante biopsia percutanea con ago da 18 gauge per 37 noduli in 9 pazienti )  . nei pazienti con conferma bioptica di hcc , un unico nodulo stato sottoposto a biopsia ; pertanto sono stati considerati portatori di hcc multifocale quei pazienti che presentavano altre lesioni con le medesime caratteristiche allimaging della lesione sottoposta a biopsia . 
la conferma per i rimanenti 50 noduli in 19 pazienti stata ottenuta con un follow - up , che teneva conto di dati di laboratorio ( ad esempio , test per la funzionalit epatica e dosaggio dell - fetoproteina ) e radiologici . quarantasei noduli in 15 pazienti sono stati confermati grazie alla risposta a terapie percutanee intervenzionali come chemioembolizzazione , radiofrequenza ed alcolizzazione ( intesa come riduzione delle dimensioni e / o assenza completa / parziale di vascolarizzazione arteriosa al controllo tc ad 1 mese dalla procedura ed ogni 6 mesi per un periodo medio di almeno 1 anno )  . quattro lesioni in 4 pazienti sono state confermate solamente mediante un follow - up con tc ( aumento dimensionale della lesione e / o del numero di noduli a 3 , 6 , 9 e 12 mesi ) , in quanto non suscettibili di intervento chirurgico n di terapie percutanee a causa delle scadenti condizioni cliniche del paziente . 
nei 10 pazienti privi di lesioni focali epatiche allesame tc ( sospettate ad un precedente esame ecografico ) , la conferma di assenza di patologia neoplastica stata ottenuta mediante tc di controllo a 6 mesi di distanza dal primo esame e valori negativi di - fetoproteina . 
tutti gli esami tc sono stati eseguiti mediante un apparecchio multidetettore a 4 canali di acquisizione ( data acquisition system , das , aquilion , toshiba , tokio , giappone ) , a matrice asimmetrica di detettori e tempo di rotazione del gantry di 0 , 5 s . 
i parametri di acquisizione sono stati i seguenti : collimazione , 3 mm ; spessore di visualizzazione , 5 mm ; intervallo di ricostruzione , 5 mm ; pitch , 5 , 5 ( avanzamento del lettino , 33 mm / s ) ; 135 kv ; 175 mas . prima dellesame a tutti i pazienti sono stati somministrati per os 500 ml di acqua e per via endovenosa un mdc non ionico idrosolubile ad elevata concentrazione di iodio ( iomeprolo 400 mgi / ml ) ( iomeron 400 , bracco , milano , italia ) ad un flusso di 5 ml / s e con un volume pari a 2 ml / kg ( volume compreso tra 100160 ml ; media , 138 , 5 ml ) , mediante iniettore automatico ( envision ct injector , medrad , indianola , pennsylvania , usa )  . 
per determinare il momento ideale in cui iniziare lacquisizione tc dopo la somministrazione di mdc stato impiegato un software di contrast tracking ( sure start , toshiba , tokio , giappone ) : una region of inter.m. 
la fase arteriosa precoce evidenzia un voluminoso hcc caratterizzato da un disomogeneo enhancement ( a ) ; in fase arteriosa tardiva sono ben evidenti sia un incremento della sua cospicuit che la comparsa di una piccola lesione ipervascolare ( freccia ) ( b )  . 23 s on average ( range , 1925 s )  . 
fifteen seconds after the end of lap , the third scan was performed ( portal venous phase ) in the craniocaudal direction , with a mean delay of 62 s ( range , 5075 s )  . 
in the 12 patients undergoing surgery ( transplantation or partial resection ) , data obtained in eap were used for rest , roi , che calcola la densit ematica prima del mdc , viene posizionata allinterno dellaorta addominale , a livello di un piano passante per il diaframma ; loperatore fissa un valore di densit soglia in unit hounsfield , hu ; quindi si somministra il bolo di mdc e , dopo il raggiungimento del valore soglia di densit preimpostato , la scansione tc inizia automaticamente . sono state effettuate 3 scansioni sullintero fegato con un tempo di acquisizione di 710 s ( media , 9 s ) , a seconda del diametro cranio - caudale del fegato . 
la prima scansione ( fase arteriosa precoce ) stata ottenuta con direzione craniocaudale , la seconda ( fase arteriosa tardiva o portal inflow phase ) con direzione caudo - craniale ed un ritardo tra le due acquisizioni di 5 s . 
il ritardo medio dallinizio della somministrazione di mdc stato di 21 s ( range , 1635 s ) per la fase arteriosa precoce e di 34 s ( range , 2850 s ) per la fase arteriosa tardiva . 
dopo 15 s dal termine della fase arteriosa tardiva , stata effettuata la terza scansione ( fase venosa portale ) con direzione cranio - caudale ed un ritardo medio di 62 s ( range , 5075 s )  . nei 12 pazienti sottoposti ad intervento chirurgico ( trapianto o resezione parziale ) i dati ottenuti durante la fase arteriosa precoce sono stati utilizzati per ricostruzioni vascolari tridimensionali ( maximum intensity projection e / o volume rendering )  . le immagini della fase arteriosa precoce , tardiva e delle due fasi arteriose combinate ( double arterial phase ) sono state valutate separatamente ed indipendentemente da due radiologi esperti . 
per ogni paziente sono state impiegate da entrambi i lettori tre sessioni di lettura separate : per evitare bias da apprendimento nelle prime due venivano proposte in modo randomizzato le immagini della fase arteriosa precoce e tardiva ; nellultima sessione venivano proposte le immagini delle due fasi arteriose combinate . 
tra ogni sessione di lettura trascorso un periodo di tempo pari a due settimane . la valutazione delle immagini stata eseguita su una workstation dedicata ( anet , toshiba , tokio , giappone ) impiegando un livello della finestra pari a 100 hu ed unampiezza pari a 250 hu . 
i due lettori erano a conoscenza che la maggior parte dei pazienti avevano unepatopatia medica cronica ed erano soggetti a rischio di hcc , ma non conoscevano ulteriori informazioni cliniche ( ad esempio , livelli di - fetoproteina ) n riscontri ecografici . 
per ogni fase ciascun lettore ha indicato dimensioni , posizione e numero delle lesioni ed ha fornito in modo soggettivo un grado di sospetto per la presenza di hcc mediante una scala a 5 punti : punteggio 0 , assenza di hcc ; punteggio 1 , hcc probabilmente assente ; punteggio 2 , hcc possibilmente presente ; punteggio 3 , hcc probabilmente presente ; punteggio 4 , hcc sicuramente presente . 
una lesione veniva definita hcc quando nelle immagini delle fasi arteriose appariva come un nodulo di enhancement focale , omogeneo o disomogeneo , privo dei criteri tipici per una lesione benigna . 
the readers used three separate reading sessions for each patient : in order to avoid learning bias in the first two , eap and lap images were submitted to their judgement at random ; in the last session , images of the two arterial phases combined were examined . 
two weeks elapsed between each reading session . image assessment was carried out on a dedicated workstation ( anet , toshiba , tokyo , japan ) with a window level of 100 hu and width of 250 hu . 
if the two readers disagreed , images were re - assessed with a third reader to reach a consensus . all lesions , subsequently confirmed to be hcc , with a degree of suspicion > 2 were considered true positives . 
 table 1 k values for degree of agreement between the two readers as to presence ( score 24 ) or absence ( score 01 ) of lesions reading session reader 1 vs . 
lettore 2 tutte le lesioni , con successiva conferma di hcc , con un grado di sospetto superiore o uguale a 2 sono state considerate veri positivi ; tutte quelle con punteggio da 0 a 1 , con conferma di hcc , sono state considerate falsi negativi . 
un valore di p inferiore a 0 , 05 con un test a due code stato considerato significativo . risultati in 40 pazienti su 50 arruolati stato riscontrato almeno un hcc , per un totale di 111 lesioni . 
trentanove tumori su 111 presentavano un diametro maggiore o uguale a 20 mm , 72 / 111 presentavano un diametro inferiore ai 20 mm ( range , 5220 mm ; media , 22 mm )  . 
i valori k dei due lettori hanno mostrato una concordanza moderata nellanalisi della fase arteriosa precoce ( k = 0 , 49 ) , ed elevata nella valutazione sia della fase arteriosa tardiva ( k = 0 , 62 ) che delle due fasi arteriose combinate ( k = 0 , 78 ) ( tabella 1 )  . 
la sensibilit ed il valore predittivo positivo medi nellidentificazione di hcc sono risultati rispettivamente pari a 83 , 8% e 93 , 5% per le immagini della fase arteriosa precoce , 90 , 5% e 94 , 8% per la fase arteriosa tardiva , 94 , 1% e 95 , 1% per la double arterial phase . 
lanalisi delle immagini della sola fase arteriosa tardiva e di quelle delle due fasi arteriose combinate ha consentito lidentificazione di un numero significativamente superiore di hcc , rispetto alla valutazione della sola fase arteriosa precoce ( p < 0 , 05 )  . 
la valutazione delle immagini della double arterial phase ha evidenziato valori di sensibilit e valore predittivo positivo superiori rispetto a quelli della sola fase arteriosa tardiva , anche se entrambi con differenza non statisticamente significativa ( p > 0 , 05 ) ( entrambi i lettori hanno identificato 4 lesioni in 4 pazienti perse nella fase arteriosa tardiva ) ( tabella 2 e 3 )  . 
in lap , the two readers identified 12 tumours in six patients , which had a seguito di fenomeni di neoangiogenesi intratumorale nellhcc si riscontrano vasi tumorali , spesso irregolari e tortuosi , con un apporto vascolare prevalentemente arterioso rispetto al fegato sano circostante ( arterializzazione ) [ 2 ]  . 
per la corretta identificazione di tale neoplasia necessaria pertanto lacquisizione di una fase arteriosa , durante la quale vi unelevata quantit di mdc allinterno dei vasi arteriosi , oltre che lacquisizione di una fase venosa portale pi tardiva , in cui la neoplasia ha gi dismesso il mdc apparendo quindi ipodensa rispetto al parenchima circostante [ 2426 ]  . negli ultimi anni molti autori hanno riconosciuto come la fase arteriosa migliori la sensibilit nellidentificazione table 2 sensitivity and positive predictive value ( ppv ) of the two readers in the three reading sessions . 
evaluation of double arterial phase images had higher sensitivity and positive predictive value than achieved with lap alone although the difference was not statistically significant ( p > 0.05 ) ( both readers identified four missed lesions in four patients in lap ) ( tables 2 and 3 )  . 
the two readers mean degree of suspicion was higher with images of lap and the double arterial phase as compared with eap alone ( 3.48 in eap ; 3.67 in lap ; 3.63 in double arterial phase )  . 
 discussion following intratumoral neoangiogenesis phenomena , often irregular and tortuous tumour vessels are present within hccs , leading to predominantly arterial supply relative to the surrounding healthy liver ( arterialization ) [ 2 ]  . 
as a consequence , correct ct identification of this tumour requires acquisition of an arterial phase during which a large amount of cm is contained in the arteries , as well as acquisition of a later portal venous phase during which the neoplasm has already eliminated the cm and appears hypodense against the surrounding parenchyma [ 2426 ]  . 
over the last few years , several authors have recognised that the arterial phase improves sensitivity of ct in the identification of hcc , both with single - slice [ 3 , 59 ] and multislice scanners [ 1113 ] ; others have reported that higher iodine concentrations increase aortic endellhcc , sia con tc a singolo strato [ 3 , 59 ] , sia con apparecchi multidetettore [ 1113 ] ; altri hanno descritto come maggiori concentrazioni di iodio determinino un incremento in particolar modo dellenhancement aortico , risultando in una migliore differenza di contrasto tra strutture iperdense , come vasi arteriosi e tumori ipervascolari ( ad esempio , hcc ) , ed il parenchima epatico [ 1822 , 27 , 28 ]  . in questo studio abbiamo eseguito un esame tc in modalit trifasica con un apparecchio multidetettore , come gi descritto da altri autori [ 10 , 12 , 13 ] , per aumentare la capacit di identificare le lesioni ipervascolari . abbiamo acquisito due fasi arteriose ( precoce e tardiva ) in ununica apnea inspiratoria ed una fase venosa portale . a differenza di laghi et al . 
 [ 12 , 13 ] , in questo studio abbiamo deciso di valutare solamente il contributo delle immagini ottenute nelle due fasi arteriose , anche se la fase venosa portale stata acquisita in tutti i pazienti . 
sulla base di osservazioni della letteratura , che evidenziavano lefficacia delle alte concentrazioni dei mdc [ 22 , 29 ] , si scelto di utilizzare un mdc ad alta concentrazione per valutare se questo migliori lidentificazione dellhcc , che notoriamente , nella maggior parte dei casi , una neoplasia ipervascolarizzata . 
per ovviare ai problemi legati alla velocit di circolo dei pazienti abbiamo impiegato un software di contrast - tracking . i nostri risultati hanno evidenziato unelevata sensibilit per lidentificazione dellhcc in fase arteriosa precoce ( 83 , 8% ) , tardiva ( 90 , 5% ) e nella double arterial phase ( 94 , 1% ) , sebbene non vi fosse una differenza statisticamente significativa tra la fase arteriosa tardiva e la double arterial phase , come peraltro gi riscontrato da laghi et al . 
our study used a three - phase mdct examination , as already reported by other authors [ 10 , 12 , 13 ] , to increase our ability to detect hypervascular lesions . 
 [ 12 , 13 ] , we decided to evalli e valutabili durante la fase arteriosa tardiva , probabilmente a causa di un intervallo di tempo necessario affinch il sangue arterioso contrastato , proveniente dallarteria epatica , si distribuisca allinterno dellinterstizio della lesione [ 10 ]  . 
va inoltre sottolineato che dai nostri dati sono emersi valori di sensibilit maggiori , se paragonati a quelli ottenuti in altri studi in cui siano state valutate le due fasi arteriose [ 11 , 13 ] , e questa differenza risulta pi marcafig . 
2a - d computed tomography ( ct ) images of a 52 - year - old patient with hepatitis - c - virus - related liver disease , with a transjugular intrahepatic portosystemic shunt ( tips ) , candidate for liver transplantation . 
in early arterial phase , a 25 - mm hepatocellular carcinoma ( hcc ) nodule can be clearly seen near the hepatic hilum , characterised by early enhancement ( a ) and increased conspicuity in the late arterial phase ( b )  . 
in fase arteriosa precoce evidente un nodulo di hcc di 25 mm in prossimit dellilo epatico caratterizzato da un precoce enhancement ( a ) , la cui cospicuit risulta maggiore in fase arteriosa tardiva ( b )  . 
on the basis of literature reports , which showed the effectiveness of high concentrations of cm [ 22 , 29 ] , we decided to use a high - concentration cm to determine whether it can improve identification of hcc , which is known to be a hypervascular tumour . 
our results indicated a high sensitivity in the identification of hccs in eap ( 83.8% ) , in lap ( 90.5% ) and in the double arterial phase ( 94.1% ) although there was no statistically significant difference between lap and the double arterial phase , as already noted by laghi et al . 
it should be noted that our study found higher sensitivity values compared with those obtained by other studies assessing both arterial phases [ 11 , 13 ] , and that this difference is more dramatic in eap . 
in our view , this greater sensitivity may be due to the higher concentration of contrast agent employed since high - concentration cm administered at a high flow rate leads to an earlier and more intense arterial enhancement peak [ 27 , 30 ]  . 
since the hepatic artery is one of the main branches of the aorta , concentration of cm in the hepatic artery , and consequently in the hcc , is thought to be equivalent to concentration in the aorta . 
therefore , it can be assumed that during the arterial phase , the contrast difference between a hypervascular lesion and the liver is comparable to that between the aorta and the liver [ 18 ]  . 
thus , lesions such as hcc , which is supplied by the hepatic artery , have a more intense and earlier enhancement during the arterial phase when a high - concentration contrast agent is used . 
the above may also explain the greater increase in sensitivity in hcc identification during eap as compared with the late phase when our results are compared with those reported in the literature . 
 [ 18 ] , who found greater aortic enhancement and a more dramatic contrast difference between lesion and liver during eap using higher concentrations of cm ( 370 mgi / ml )  . 
 [ 20 ] , who studied patients with chronic liver disease , even though only one arterial phase was used in these studies . finally , our results agree with those of a recent pilot study by marchiano et al . 
nevertheless , as suggested by other reports [ 11 , 13 , 22 ] , we used other methods to obtain confirmation , such as clinical history , ct follow - up and response ta nella fase arteriosa precoce . 
secondo noi questa maggiore sensibilit potrebbe essere dovuta alla maggiore concentrazione del mdc impiegato , in quanto mdc ad elevata concentrazione , somministrati con elevata velocit , determinano un picco di enhancement arterioso pi precoce e pi intenso [ 27 , 30 ]  . 
dato che larteria epatica rappresenta uno dei principali rami dellaorta , si suppone che la concentrazione di mdc in arteria epatica , e quindi nellhcc , sia equivalente a quella aortica . 
si pu allora presumere che in fase arteriosa la differenza di contrasto tra una lesione ipervascolare e fegato sia paragonabile a quella tra aorta e fegato [ 18 ]  . quindi lesioni come lhcc , vascolarizzato dallarteria epatica , presentano verosimilmente un enhancement pi intenso e precoce in fase arteriosa quando si impieghi un mdc ad elevata concentrazione . quanto sopra pu spiegare anche il pi marcato incremento di sensibilit nellidentificazione dellhcc in fase arteriosa precoce rispetto a quella tardiva , quando si confrontano i nostri risultati con quelli medi riscontrati in letteratura . peraltro altri studi confermerebbero la nostra ipotesi , come quello di awai et al . 
 [ 18 ] , che hanno evidenziato un maggiore enhancement aortico ed una pi marcata differenza di contrasto tra lesione e fegato in fase arteriosa precoce utilizzando concentrazioni di mdc pi elevate ( 370 mgi / ml )  . conclusioni simili sono emerse anche in lavori di sultana et al . 
execution of a single arterial phase followed by a portal venous phase would imply considerable dose savings for each examination ( 6.03 msv ) , an important aspect if we consider that these patients undergo periodic ct scans during follow - up . 
we believe that further studies are needed to compare different concentrations of cm with the same amounts of iodine administered to the same subject , especially in hcc candidates for liver transplantation , with the possibility of establishing the precise number of lesions on the explanted liver . conclusions the use of high - iodine - concentration cm ( 400 mgi / ml ) produces an increase in the number of hccs identified during the arterial phase , both early and late . 
in ct studies of patients with more or less known chronic liver disease and suspected hcc , we suggest that high - iodine - concentration cm should be used ( 400 mgi / ml )  . 
considering that these patients undergo periodic follow - up examinations , and considering the dose delivered by a double arterial phase acquisition , we believe acquisition of lap alone , followed by the portal venous phase , to be indicated . 
 riteniamo siano necessari ulteriori studi per paragonare differenti concentrazioni di mdc con medesime quantit di iodio somministrate allo stesso soggetto , soprattutto in pazienti con hcc candidati a trapianto di fegato , con la possibilit quindi di calcolare il numero esatto di lesioni sul fegato espiantato . conclusioni limpiego di mdc ad elevata concentrazione di iodio ( 400 mgi / ml ) consente di incrementare il numero di hcc identificati in fase arteriosa sia precoce che tardiva . 
negli studi tc di pazienti con epatopatia medica cronica nota o meno e sospetto di hcc , suggeriamo lutilizzo di un mdc ad elevata concentrazione di iodio ( 400 mgi / ml )  . tenuto conto del fatto che questi pazienti sono sottoposti a frequenti controlli e della dose a cui sarebbero esposti in caso di acquisizione di una doppia fase arteriosa , riteniamo che sia indicata lacquisizione della sola fase arteriosa tardiva seguita dalla fase venosa portale . 
bassiano , via dei lotti 14 , i - 36061 bassano del grappa ( vi ) , italy 2istituto di radiologia , ospedale cattinara , universit di trieste , strada di fiume , i - 34100 trieste , italy 3u.o. 
typical computed tomography ( ct ) pattern has been widely described and consists of peripheral parenchymal consolidations with air bronchogram with or without surrounding ground - glass - like opacities . 
the purpose of this article is to describe the less frequent imaging pattern of this disease represented by single or multiple focal lesions ( nodules or masses that place diagnostic problems with malignancy ) , bronchocentric pattern ( parenchymal consolidations with peribronchovascular distribution ) , atoll sign ( central area of ground - glass - like density and peripheral area of consolidation ) , nodular lesions ( poorly defined micronodular pattern ) , linear and band - like opacities ( subpleural linear opacities that can have disposition parallel or perpendicular in relation to the pleura ) , perilobular pattern ( thickening of the interlobular septa with reticular pattern ) and progressive fibrotic pattern ( irregular thickening of the interlobular septa with associated ground - glasslike appearance and consolidations )  . key words organizing pneumonia hrct cryptogenic organizing pneumonia idiopathic interstitial pneumonias boop riassunto la polmonite organizzata ( op ) unentit clinico - patologica che , se idiopatica , fa parte delle polmoniti interstiziali secondo la classificazione ats / ers del 2002 ( 50% dei casi , chiamata polmonite organizzata criptogenetica o cop )  . 
op is a relatively common condition accounting for approximately half la polmonite organizzata ( op ) unentit clinico - patologica descritta per la prima volta da davison e collaboratori nel 1983 [ 1 ]  . 
il termine op , recentemente entrato nelluso comune , da preferire perch meglio descrive gli aspetti anatomopatologici ed evita confusione diagnostica con altre patologie delle vie aeree ( per esempio , la bronchiolite obliterante ) [ 3 ]  . 
according to the new classification introduced by he american thoracic society / european respiratory society ( ats / ers ) in 2002 [ 5 ] , the idiopathic form of op falls within the idiopathic interstitial pneumonias and is called cryptogenic organizing pneumonia ( cop )  . 
op may , however , also be secondary to several conditions since it represents the lungs reaction to different pathogenic noxae ( op reaction pattern ) ( table 1 )  . over the years , many papers have appeared in the radiological literature that describe new high - resolution computed tomography ( hrct ) patterns of op [ 6 , 7 ]  . 
the aim of this paper is to review the recent literature data describing typical and atypical clinical , pathological and especially ct and hrct aspects of op . za frequente , rappresentando circa la met dei casi diagnosticati di malattia delle piccole vie aeree , ed idiopatica nel 50% dei casi [ 4 ]  . 
secondo la nuova classificazione dellats / ers del 2002 [ 5 ] , la forma idiopatica della op fa parte delle polmoniti interstiziali idiopatiche e denominata cop ( polmonite organizzata criptogenetica )  . la polmonite organizzata pu essere tuttavia anche secondaria , associata cio a molte situazioni rappresentando una peculiare modalit di risposta del polmone a diverse noxae patogene ( op reaction - pattern ) ( tabella 1 )  . 
scopo di questo lavoro quindi di proporre i dati recenti della letteratura , descrivendone gli aspetti clinici , anatomopatologici , ma soprattutto tc ad alta risoluzione ( hrct ) , sia tipici sia quelli meno comuni . clinical presentation the frequency of the disease is identical in men and women and , even though no sure relation exists with cigarette smoking , it is prevalent in non - smokers , with a 2 : 1 ratio [ 8 ]  . 
there may also be weight loss , mild fever and myalgia . they will usually have been treated with one or more courses of antibiotics without symptom resolution or improvement [ 9 ]  . 
although a definitive diagnosis of op cannot be made on the sole basis of clinical findings , the combination of a compatible clinical history and adequate hrct signs may enable diagnosis in 80% of cases . 
transbronchial biopsy and bronchoalveolar lavage can confirm the diagnosis , but imaging alone may be sufficient for a diagnostic hypothesis of op [ 6 ]  . histology histologically , op presents with polyps of lax connective tissue within the terminal or respiratory bronchioles , alveolar ducts and the alveoli , with patchy distribution , usually without changes in pulmonary architecture and with temporal homogeneity . 
the bronchiolar component may be lacking , and there may be signs of chronic interstitial inflammation , but istologia clinica la frequenza della malattia sovrapponibile tra maschi e femmine e , anche se non esiste una sicura relazione con il fumo di sigaretta , prevalente nei non fumatori , con un rapporto 2 : 1 [ 8 ]  . 
i pazienti presentano caratteristicamente un quadro clinico di infezione delle basse vie aeree con malessere di recente insorgenza ( di solito da meno di 3 mesi ) , con grado variabile di tosse e dispnea . 
in alcuni casi si pu osservare una rapida evoluzione verso la fibrosi , ma esiste anche la possibilit di una polmonite organizzata sovrapposta alla fibrosi polmonare idiopatica ( fpi )  . 
non possibile porre una diagnosi di certezza di op solo in base al quadro clinico , ma lassociazione di una storia clinica compatibile e i segni hrct adeguati possono porre diagnosi nell80% dei casi . 
la biopsia transbronchiale e il lavaggio bronchiolo - alveolare possono confermare la diagnosi , anche se in alcuni casi limaging radiologico pu essere da solo sufficiente nellipotesi diagnostica di questa malattia [ 6 ]  . il quadro istologico della op rappresentato da polipi di r . 
miscellaneous inflammatory bowel disease primary biliary cirrhosis polyarteritis nodosa haematological malignancies myelodysplastic syndrome t - cell leukaemia lymphoma radiotherapy exposure to toxic substances aspiration syndrome extrinsic allergic alveolitis acute and chronic eosinophilic pneumonia wegeners disease a . 
varie malattie infiammatorie intestinali cirrosi biliare primitiva poliarterite nodosa tumori ematologici sindrome mielodisplasica leucemia a cellule t linfoma radioterapia esposizione a sostanze tossiche sindrome da aspirazione alveolite allergica estrinseca polmonite eosinofila acuta e cronica malattia di wegener d . 
finally , it should be noted that foci of intraluminal op typical of op are also seen in association with inflammation and fibrosis in about half of the cases of non - specific interstitial pneumonia ( nsip ) [ 12 ]  . typical hrct pattern the typical pattern is present in 60%90% of cases [ 13 , 14 ] and characterised by bilateral patchy areas of consolidation , often triangular or polygonal in shape , in the peripheral subpleural regions , but also peribronchial , and often located in the lower lobes . 
in 60% of cases scattered ground - glass opacities are associated and at times ( 10%50% ) small ill - defined centrinodular lobules that are often peribronchial [ 13 , 15 ]  . 
the prevalently subpleural location of op calls for a differential diagnosis with chronic eosinophilic pneumonia [ 9 , 16 ]  . other diseases may display similar radiological patterns and , in particular , bronchioloalveolar carcinoma , lymphoma , vasculitis , and infections ( above all tuberculous and atypical mycobacteriosis )  . 
even the symptoms may be suggestive of cancer due to the presence of haemoptysis if the lesions are cavitated , a relatively common occurrence in this type of op . some hrct signs may , however , help in differentiating the two diseases : peripheral location , predominant oval or trapezoidal shape ( unlike cancer , which is usually rounded ) and the frequent presence of satellite lesions are suggestive of op [ 15 , 1822 ]  . 
nel 60% dei casi coesistono aree sparse di ground - glass e talvolta ( 10%50% ) piccoli noduli centrolobulari a margini mal definiti , spesso peribronchiali [ 13 , 15 ]  . le lesioni tendono a progredire e a cambiare sede nel tempo e sono stati descritti casi di remissione spontanea . 
la localizzazione prevalente subpleurica pone la op in diagnosi differenziale con la polmonite eosinofila cronica [ 9 , 16 ]  . altre malattie possono manifestarsi con aspetti radiologici simili ed in particolare , il carcinoma bronchiolo - alveolare , il linfoma , le vasculiti , e le infezioni ( soprattutto tubercolari e le micobatteriosi atipiche )  . in tali casi la diagnosi certa si ottiene solo con manovre invasive ( biopsia transbronchiale ) [ 5 , 16 ]  . 
 da ricordare che gli addensamenti presenti in caso di op secondaria ad amiodarone , hanno la particolarit di essere iperdensi per la presenza di iodio nel farmaco [ 17 ] ; tale aspetto rende la diagnosi certa . pattern hrct atipico lesione focale ( unica o multipla ) la op pu presentarsi come unica lesione parenchimale , frequentemente localizzata nei lobi superiori , a contatto con la pleura e le scissure ( pleural tags , nel 38% dei casi ) ( fig . 2 ) o lungo il fascio bronco - vascolare . queste caratteristiche radiologiche sono pressoch sovrapponibili a quelle del cancro del polmone e la diagnosi definitiva richiede il ricorso alla biopsia o allasportazione chirurgica . anche la sintomatologia pu a volte far pensare alla neoplasia per la presenza di emoftoe nel caso in cui le lesioni siano cavitate , evento non raro in questo tipo di op . 
1a , b bilateral peripheral air - space consolidation , more evident on the right , with air bronchogram in a patient with typical organizing pneumonia ( a )  . 
1a , b addensamento parenchimale bilaterale , pi esteso a destra , in sede mantellare posteriore , con broncogramma aereo ( a ) in paziente con forma tipica di op . 
in the presence of multiple lesions , the differential diagnosis is complex and includes metastasis , lymphoma , infections ( including septic emboli ) , wegeners disease and kaposis sarcoma . 
although uncommon as a single sign ( about one - third of cases ) , it is seen in association with the classical form in 33% of patients [ 6 , 14 ]  . 
this presentation raises problems in the differential diagnosis with other lung diseases with a similar hrct pattern , in particular , vasculitis ( churg - strauss syndrome and wegeners disease ) , diffuse bronchiolo - alveolar carcinoma and chronic eosinophilic pneumonia . 
 [ 16 ] have , however , noted that patients with op are more likely to have bronchocentric lesions associated with ground - glass - like opacity than are those with chronic eosinophilic pneumonia . 
the association of bronchocentric op with polymyositis and dermatomyositis has been frequently reported , such that the finding of areas of bronchocentric consolidation in patients with these diseases may be sufficient for a diagnosis of op [ 18 , 24 , 25 ]  . atoll sign in 1996 , voloudaki et al . 
this presentation is exactly the opposite to that of nodules with a halo sign and has therefore been called reversed halo sign [ 14 ] , or atoll sign [ 27 ]  . 
described it in about 19% of patients in their series [ 14 ]  . micronodular lesions the predominant feature of this rare presentation of op is the presence of micronodular lesions ( smaller than 1 cm ) , with ill - defined margins and often peribronchial location . the micronodules represent areas of op around the mucusfilled bronchioles , surrounded by relatively healthy lung . they are seen in around one third of patients with op in association with other signs but constitute the only sign in 9% of cases only [ 15 ]  . the presence of such nodules may be the only clue for the differential diagnosis with chronic eosinophilic pneumonia , in which nodules are rare [ 28 ]  . linear and band - like opacities this is a rare presentation which is possible both in isolation or combined with other more common patterns . 
two types have been described , usually in association with parenchymal consolidation . the first type is characterised by linear opacities extending in a radial manner along the bronchi towards the pleura , measuring 24 cm in length and 12 mm in width , located in the lower lobes and bilaterally in 50% of cases . 
6 segno dellatollo : lesione nodulare nel lobo inferiore sinistro in cui il quadro a vetro smerigliato disposto centralmente e la parte consolidativa periferica , patognomonico per op . ma classica [ 6 , 14 ]  . 
questo tipo di presentazione pone dei problemi di diagnosi differenziale con altre malattie del polmone che hanno un quadro hrct simile , in particolare le vasculiti ( sindrome di churg - strauss e malattia di wegener ) , il carcinoma bronchiolo - alveolare diffuso e la polmonite eosinofila cronica . arakawa e collaboratori [ 16 ] hanno comunque constatato una frequenza maggiore di lesioni broncocentriche associate a vetro smerigliato nei pazienti con op rispetto a quelli con polmonite eosinofila cronica . stata descritta la frequente associazione di questa forma nelle polimiositi e dermatomiositi , al punto che la presenza di addensamenti broncocentrici in pazienti con queste malattie pu essere sufficiente per la diagnosi di op [ 18 , 24 , 25 ]  . segno dellatollo voloudaki e collaboratori [ 26 ] hanno descritto nel 1996 due casi di op con aree di vetro smerigliato centrale circondato da un alone addensativo conformato ad anello . 
tale presentazione esattamente lopposto di quella dei noduli con halo sign ed stata quindi denominata reversed halo sign [ 14 ] o , per limmagine che ricorda , segno dellatollo [ 27 ]  . 
questo segno tipico della op poich , fino ad ora lunica malattia in cui stato segnalato ; kim e collaboratori lo descrivono in circa il 19% dei pazienti della loro casistica [ 14 ]  . lesioni micronodulari in questa rara forma di presentazione dellop , laspetto prevalente rappresentato dalle lesioni microdulari ( inferiori al centimetro ) e a margini mal definiti , spesso peribronchiali . i micronoduli rappresentano aree di polmonite organizzata attorno ai bronchioli ripieni di muco , circondati da polmone relativamente sano . 
la presenza di noduli di questo tipo pu essere lunico elemento di diagnosi differenziale con la polmonite eosinofila cronica dove i noduli sono poco frequenti [ 28 ]  . opacit lineari e a banda presentazione rara , possibile sia come quadro isolato che in combinazione con gli altri aspetti pi comuni . 
ne sono stati descritti 2 tipi , di solito in associazione con gli addensamenti parenchimali . il primo tipo caratterizzato da opacit lineari che si estendono in modo radiale lungo i bronchi e verso la pleura , lunghe 24 cm , con spessore di 12 mm , localizzate nei lobi inferiori , bilaterali nel 50% dei casi . 
they are related to inflammation along the segmental bronchial branches , and there is no fibrosis [ 6 ]  . perilobular lesions this pattern was first described by murata et al . 
in 1989 [ 30 ] as disease localisation in the peripheral portions of the secondary pulmonary lobule ; it is related to the accumulation of exudate of op along the walls of the peripheral alveoli adjacent to the interlobular septa . at hrct , there may be apparent thickening of the septa themselves due to their proximity with the site of the inflammation , contributing to a coarse reticular pattern with polygil secondo tipo costituito da opacit lineari subpleuriche , senza relazioni con i bronchi , parallele alla superficie pleurica , con lunghezza di 34 cm e spessore di 12 mm , a volte conformate ad arco o con broncogramma aereo allinterno , bilaterali e prevalenti nei lobi inferiori , anche se possono essere presenti nei lobi superiore e medio [ 29 ]  . 
sono determinate da flogosi localizzata lungo i rami bronchiali segmentari e non presente fibrosi [ 6 ]  . lesioni perilobulari questo quadro stato descritto per la prima volta da murata e collaboratori nel 1989 [ 30 ] come localizzazione della malattia a livello delle porzioni periferiche del lobulo polmonare secondario ; esso cio determinato dallaccumulo di essudato della polmonite organizzata lungo la parete degli alveoli periferici , adiacenti ai setti interlobulari . 
in hrct vi pu essere un apparente ispessimento dei setti stessi per la loro vicinanza alla sede della flogosi con realizzazione di un quadro di tipo reticolare sfumato a morfologia poligonale . 
the distribution of these findings corresponds to the typical subpleural and peripheral distribution of op , and this presentation is usually associated with the use of nitrofurantoin and tends to progress to fibrosis [ 3133 ]  . fibrosi progressiva pica della op , con sede mantellare e periferica e di solito questa presentazione associata alluso di nitrofurantoina e presenta unevoluzione verso la fibrosi [ 3133 ]  . progressive fibrosis this radiological pattern was first described in 1973 by gosink et al . 
it is important to bear in mind these different appearances to be able to consider , among the various possible differential diagnoses and in an appropriate clinical setting , even the possibility of a primary or secondary op not presenting with a conventional pattern . pur essendo ormai conosciute da lungo tempo le alterazioni tipiche della op , sempre pi numerose sono le descrizione dei differenti patterns di presentazione di questa malattia . 
ospedali civili riuniti , sciacca ( agrigento ) , italy 4servizio di radiologia , ospedale san massimo , penne ( pescara ) , italy 5facolt di medicina e chirurgia , dipartimento di internistica clinica e sperimentale f . 
stanzione 18 , i - 80129 napoli , italy , tel . : + 39 - 348 - 3738149 , fax : + 39 - 081 - 5584521 , e - mail : roberto.grassi@libero.it received : 27 october 2004 / accepted : 11 july 2005 / published online : 3 march 2006 abstract this paper examines the diagnostic potential of multislice computed tomography enteroclysis ( msct - e ) to detect and assess different diseases affecting the small bowel , emphasising the increasingly important role assumed by the technique in the study of this anatomical region . 
after a short summary of the technical aspects , we discuss the different findings that can be observed during an msct - e study and that enable detection of small - bowel disease and , if necessary , assessment of the extent and stage of disease . key words small bowel multidetector - row ct enteroclysis malabsorption crohns disease bowel neoplasms riassunto gli autori in questo lavoro esaminano le potenzialit diagnostiche della enteroclisi tc multistrato ( e - msct ) nella identificazione e nella valutazione di estensione delle differenti patologie dellintestino tenue , sottolineando il ruolo sempre pi importante che tale tecnica assume nello studio di differenti condizioni morbose che interessano tale distretto anatomico . 
dopo un breve richiamo delle nozioni di tecnica vengono esaminati i differenti rilievi osservabili e da ricercare nel corso di un esame e - msct al fine di ottenere lidentificazione della patologia e , nel caso sia necessario , lestensione e la stadiazione delle differenti patologie del piccolo intestino . parole chiave intestino tenue enteroclisi - tc multistrato malassorbimento morbo di crohn neoplasie intestinali introduction introduzione despite the widespread diffusion and technological evolution of endoscopy , the small bowel is still the only portion of the gastrointestinal tract that cannot be completely explored with endoscopic techniques . 
as a consequence , the diagnosis of small - bowel disease is still mostly established by radiology , which enables the study of both the bowel lumen and wall as well as of extraparietal structures . 
singleor double - contrast enteroclysis has high levels of sensitivity and specificity in the diagnosis of small - bowel disease , as has been widely documented over the past decades . 
forced bowel loop distension through naso - intestinal intubation allows a more accurate study compared with that obtained nonostante la diffusione e levoluzione tecnologica della endoscopia , lintestino tenue rimane , attualmente , lunica parte del tratto gastro - enterico non esplorabile completamente con le metodiche endoscopiche . 
di conseguenza , la diagnosi delle malattie del piccolo intestino ancora affidata in gran parte alla radiologia che offre uno studio sia del versante endoluminale , sia della parete , nonch del versante extraparietale . le metodiche pi utilizzate per lo studio di gran parte delle malattie gastro - intestinali sono la radiologia tradizionale , lecografia ( us ) e la tomografia computerizzata ( tc )  . 
volumetric acquisition can rapidly explore , in a single inspiratory breath - hold , the entire abdomino - pelvic region , almost completely eliminating artefacts due to respiration and intestinal peristalsis . 
multislice ct enteroclysis ( msct - e ) is a recent technique in small - bowel imaging , which combines the advantages of bowel distension with naso - intestinal intubation with those of spiral ct [ 68 ]  . 
the aim of the present review was to define the indications for msct - e in the most common clinical settings and to illustrate the diagnostic gains provided by msct - e compared with other imaging modalities . accurato rispetto a quello ottenibile con lopacizzazione per os del piccolo intestino [ 4 , 5 ]  . 
lacquisizione volumetrica in grado di esplorare rapidamente , in unica apnea inspiratoria , tutto il distretto addomino - pelvico , eliminando quasi completamente gli artefatti respiratori e da peristalsi intestinale . 
lenteroclisi - tc multistrato ( e - tcms ) una recente metodica di studio dellintestino tenue , che somma i vantaggi della distensione intestinale , ottenuta con lintubazione naso - enterica , a quelli propri della tc spirale [ 68 ]  . 
scopo del presente articolo definire le indicazioni della e - tcms nelle pi frequenti situazioni cliniche e di precisare il guadagno diagnostico di tale metodica rispetto alle altre metodiche di imaging . malabsorption malassorbimento the diagnosis of malabsorption is essentially based on clinical and laboratory findings . 
in some cases , the radiologist is called upon to demonstrate the intestinal disorder causing the malabsorption [ 9 , 10 ]  . the intestinal conditions most commonly responsible for malabsorption include : parasite infection ; small - bowel diverticular disease ; short bowel syndromes ( both post - surgical and due to reduced mucosal surface , such as diffuse chronic enteritis , chronic intestinal ischaemia , radiation enteritis ) ; jejuno - colic fistulae ; and adult coeliac disease ( acd )  . 
tra le malattie intestinali di interesse radiologico pi frequentemente causa di malassorbimento ricordiamo : le parassitosi ; la diverticolosi del tenue ; le sindromi da intestino corto ( sia post - chirurgico che da riduzione della superficie mucosa utile allassorbimento , come le enteriti croniche diffuse , la ischemia intestinale cronica , lenterite da radiazioni ) ; le fistole digiuno - coliche ; la malattia celiaca delladulto ( mca )  . 
frequentemente si tratta di malattie croniche e note da tempo ; pertanto non esiste indicazione elettiva allo studio radiologico dellintestino tenue e le alterazioni dimostrabili radiologicamente hanno in genere unimportanza marginale [ 912 ]  . 
infatti , i linfonodi mesenterici e la irregolarit delle pliche digiunali residue sono reperti frequentemente riscontrabili anche in pazienti con mca scompensata , ma non complicata ; talvolta , un breve follow - up clinico contribuisce a risolvere il problema diagnostico [ 21 ]  . small - bowel occlusion mechanical occlusion of the small bowel ( sbo ) , a very common clinical condition , may be complete or partial . 
conventional ct has high levels of sensitivity in both the diagnosis of locclusione meccanica dellintestino tenue ( sbo ) , condizione clinica molto frequente , pu essere completa oppure parziale . 
ben evidente la riduzione del numero delle valvole conniventi nelle anse prossimali dellintestino tenue ( a ) , ed il relativo incremento delle pliche nelle anse pelviche ( b ) , che presentano anche aspetto ipotonico e diffusamente digiunizzato . 
inoltre , non si rende necessaria la somministrazione di contrasto endoluminale perch la distensione intestinale , provocata dallo stato occlusivo , consente gi uno studio ottimale delle anse , grazie al contrasto naturale tra il lume ipodenso ( per il contenuto liquido della stasi ) e la parete resa iperdensa dal mdc iodato e.v. 
spiral computed tomography with iv iodinated contrast agent without further opacification of the bowel loops , which appear distended ( a ) ; normal parietal contrast enhancement ; small collection due to perihepatic ascites . 
esame tc spirale con mdc iodato e.v , senza ulteriore opacizzazione delle anse intestinali , che appaiono distese ( a ) ; regolare ce parietale ; piccola falda di ascite periepatica . 
reperti suggestivi per sbo da aderenze ; conferma chirurgica . of sbo , above all in the case of complex adherence syndromes [ 8 , 22 ]  . in partial sbo , the diagnosis may prove challenging . 
there may also be an indication for mr enteroclysis or convenmultiplanari possono , talvolta , rendere pi agevole la diagnosi di sbo , soprattutto nel caso di sindromi aderenziali complesse [ 8 , 22 ]  . in caso di sbo parziale , la diagnosi pu essere impegnativa . 
consente di escludere problemi di perfusione parietale e permette anche un giudizio accurato sul mesentere ( a )  . ben apprezzabile la transizione tra le anse distese a monte della ostruzione e lintestino vuoto a valle . 
il contrasto endoluminale positivo consente una dimostrazione ottimale della natura estrinseca della patologia ostruente . tional enteroclysis , which allow progression of the endoluminal contrast material to be followed through the bowel loops [ 2 , 22 , 27 , 28 ]  . possono trovare indicazione anche la rm - enteroclisi o il clisma del tenue tradizionale , che permettono di seguire la progressione del mdc endoluminale attraverso le anse intestinali [ 2 , 22 , 27 , 28 ]  . crohns disease crohns disease was and still is the most common field of application of all small - bowel imaging techniques . 
total parenteral nutrition and new effective drugs , even non - conventional drugs such as infliximab ( anti - alpha tnf ) , have changed the role of surgery ; surgery now tends to be used less frequently and as an elective procedure . 
 all imaging modalities provide a fundamental contribution to the correct diagnosis and staging of crohns disease . patients with the disease do not form a clinically homogeneous group , and they may be very different from one another , with different clinical situations influenced by individual expression of the disease and possible previous surgical procedures ; this does not always allow a uniform and reproducible clinical and radiological standardisation of the disease [ 37 ]  . 
msct - e is usually used immediately after us or even as a first - line examination and is therefore gradually replacing conventional enteroclysis [ 38 , 39 ]  . 
luminal distension with neutral contrast material and iv administration of iodinated contrast macampo di studio e di applicazione pi frequente di tutte le metodiche di imaging dellintestino tenue . una malattia infiammatoria cronica , ancora oggi ad ezio - patogenesi sconosciuta , che pu interessare qualsiasi parte del tratto gastro - enterico , prediligendo lileo e il colon . 
la storia naturale della malattia caratterizzata da fasi di riacutizzazione alternate a periodi di remissione clinica [ 2936 ]  . la nutrizione parenterale totale e nuovi farmaci efficaci , anche non convenzionali come linfliximab ( anti - alfa tnf ) , hanno modificato il ruolo della chirurgia ; si tende ad intervenire chirurgicamente sempre meno , in elezione , e sono sempre pi praticate stricturoplastiche , dilatazioni pneumatiche delle stenosi , drenaggi percutanei di raccolte ascessuali . per una corretta diagnosi e stadiazione della malattia risulta fondamentale lapporto di tutte le metodiche di imaging . 
i pazienti con malattia di crohn non costituiscono , infatti , una entit clinica omogenea e possono essere molto differenti tra loro , con situazioni cliniche polimorfe , influenzate dalla espressivit individuale della malattia e da eventuali precedenti terapie chirurgiche ; ci non sempre permette una standardizzazione clinico - strumentale uniforme e riproducibile [ 37 ]  . 
follow - up of patients with known crohns disease , even those with good response to medical therapy , is mostly carried out by ultrasound so as to exclude the appearance of complications with insidious course [ 4042 ]  . 
recurrence of crohns disease requires a similar diagnostic workup to that used for the initial diagnosis since lesion course in recurring disease is known to mimic the course at initial onset . however , it should be recalled that crohns disease is not the only cause of bowel - wall thickening . 
attualmente , la e - tcms viene di solito utilizzata subito dopo lesame ecografico od addirittura in prima istanza , sostituendo cos gradualmente il clisma del tenue tradizionale [ 38 , 39 ]  . la distensione del lume con mdc neutro e la somministrazione di mdc iodato e.v. 
il follow - up del paziente con malattia di crohn gi nota affidato oggi prevalentemente allesame ecografico , anche in caso di buona risposta al trattamento medico , allo scopo di escludere la comparsa di complicanze a sviluppo insidioso [ 4042 ]  . 
noto , infatti , che la naturale evoluzione delle lesioni in caso di recidiva mimi il decorso della malattia allesordio . comunque opportuno ricordare che la malattia di crohn non lunica causa di ispessimento delle pareti intestinali . 
nei casi in cui clinica e rilievi tc non siano concordi , pu risultare opportuno ricorrere allintegrazione diagnostica ( eventualmente in follow - up ) con le metodiche di contrastografia baritata . esse permettono uno studio morfologico accurato del rilievo mucoso , la cui semeiotica , consolidata da pluriennale esperienza , risulta senzaltro pi ricca di elementi diagnostici [ 49 ]  . lenteroclisi - rm una metodica emergente , ancora in via di sviluppo . 
essa sta fornendo ottimi risultati nello studio delle malattie del piccolo intestino , grazie alla sua eccellente risoluzione di contrasto ed alla possibilit di ottenere immagini sia statiche che dinamiche . 
transverse ultrasound scan ( a ) and spiral computed tomography ( ct ) ( b , c ) with intestinal opacification with positive contrast material in a patient with crohns disease in the descending colon , which shows thickened walls and narrowed lumen ( a , c )  . 
a hypoechoic fistula ( a ) originating in the colon and directed posteriorly feeds a large abscess collection with mixed content ( even gaseous ) in adjacent soft tissues , with involvement of the ileo - psoas muscle and reaching as far as the gluteal region . 
esame ecografico in scansione trasversale ( a ) e tc spirale ( b , c ) con opacizzazione intestinale con mdc positivo in paziente con localizzazione di malattia al colon discendente , che presenta pareti ispessite e lume ristretto ( a , c )  . 
tramite fistoloso ipoecogeno ( a ) a partenza colica e diretto posteriormente ; alimenta ampia raccolta ascessuale a contenuto misto ( anche gassoso ) nei tessuti molli contigui , con coinvolgimento del muscolo ileo - psoas e sconfinamento fino alla regione glutea . 
spiral computed tomography enteroclysis with negative endoluminal contrast material ( methylcellulose ) ; the intubation catheter is clearly visible in the jejunum ( a , b ) ; administration of iv iodinated contrast material . 
e - tc spirale con mdc endoluminale negativo ( metilcellulosa ) ; visibile il catetere da intubazione in sede digiunale ( a , b ) ; somministrazione di mdc iodato e.v. 
demonstration of extraluminal fistulas by spiral computed tomography after injection of iodinated contrast material through the outer opening of the fistulas ( a ) and after intestinal opacification with positive oral contrast material ( b )  . 
dimostrazione dei tramiti fistolosi extraluminali con esami tc spirale eseguiti dopo iniezione di mdc iodato attraverso lorifizio esterno delle fistole ( a ) , e dopo opacizzazione intestinale con mdc positivo per os ( b )  . 
there are , however , no definite findings allowing differential diagnosis with other forms of enteritis or crohns disease even if the wall enhancement is more intense at the mucosal level ( a )  . 
non ci sono comunque elementi sicuri che permettano una diagnosi differenziale con altre enteriti e con la malattia di crohn , anche se il ce parietale pi intenso lungo il versante della mucosa ( a )  . 
la paziente stata controllata successivamente ( dopo guarigione clinica ) con un altro esame radiografico , che ha dimostrato la regressione delle alterazioni in precedenza visibili . cy between clinical and ct findings , it may be useful to resort to diagnostic integration ( even during the follow - up ) with barium studies . 
these allow an accurate morphological study of the mucosa which , as years of experience have shown , is undoubtedly richer in diagnostic clues [ 49 ]  . mr - enteroclysis is an emerging technique that is still developing . 
the absence of ionising radiation and encouraging initial results herald a growing clinical role for mr enteroclysis [ 2 , 5057 ]  . intestinal bleeding in acute bleeds , endoscopy , nuclear medicine , and angiography preserve their fundamental role in both diagnostic and therapeutic terms [ 5860 ]  . 
however , in this field , we should recall the emerging role of capsule endoscopy [ 62 ]  . intestinal ischaemia mesenteric ischaemia is a complex disease [ 6365 ]  . 
in the acute phase , there is no indication for msct - e , and the method should be regarded as contraindicated until the intestinal distress and consequent risk of infarction and / or perforation is overcome . 
in addition , multiplanar reconstructions can provide impressive angiography - like images of the vascular arches [ 58 ]  . intestinal neoplasms small - bowel neoplasms are rare and often manifest with non - specific symptoms and signs , such as nausea , abdominal pain , occult blood , and weight loss . 
inoltre , le ricostruzioni multiplanari possono offrire suggestive immagini simil - angiografiche delle arcate vascolari [ 58 ]  . neoplasie intestinali i tumori dellintestino tenue sono rari e spesso si presentano con segni e sintomi aspecifici , come nausea , dolore addominale , sanguinamento occulto , dimagrimento . 
la scarsa incidenza di queste malattie e lintroduzione recente della metodica e - tcms non hanno ancora consentito lacquisizione di una casistica ampia e valida , dalla quale attingere aspetti di semeiotica utili per linquadramento diagnostico . 
i rilievi della e - tcms sono quasi sempre aspecifici , cos come lo sono , daltronde , anche quelli dellesame baritato . la diagnosi viene posta solo con lintegrazione dei dati clinico - polistrumentali . 
in reality , our experience has shown that patients with systemic mesenchymal diseases have a greater incidence of intestinal involvement , such as crohns enteritis , in that there is probably a common autoimmune basis . 
after years of experience with the technique , we feel we can propose msct - e as the examination of choice studying the small bowel , in particular , in partial occlusions , crohns disease , chronic occult bleeds , chronic ischaemia , and tumours . 
la e - tcms ( a ) dimostra la presenza di lesioni infiltranti a livello di alcune anse digiunali , in un paziente studiato per follow - up di neoplasia gi nota , nel quale erano presenti inoltre lesioni secondarie di pertinenza linfonodale a livello dei linfonodi inguinali ( b )  . gangrenoso , in letteratura descritta una incidenza minima di enteriti sincrone alla patologia mesenchimale principale . in realt , nella nostra esperienza abbiamo verificato che i pazienti portatori di mesenchimopatie sistemiche hanno una frequenza maggiore di coinvolgimento intestinale , come lenterite di crohn , in quanto hanno verosimilmente una comune base autoimmune . 
le nuove apparecchiature tc spirale multidetettore consentono scansioni veloci e collimazioni sempre pi sottili con conseguente miglioramento delle ricostruzioni multiplanari e 3d . attualmente , la nostra esperienza , ormai pluriennale , ci consente di proporre le - tcms come esame di scelta nello studio del piccolo intestino , in particolare nellocclusione parziale , nella malattia di crohn , nei sanguinamenti occulti cronici , nellischemia cronica e nelle neoplasie . la metodica non oggi proponibile nei pazienti in cui necessaria unanalisi accurata del rilievo mucoso intestinale e questo senza ombra di dubbio costituisce una limitazione importante della metodica , specie nelle patologie nelle quali sia richiesta unaccurata valutazione della integrit dello strato mucoso del piccolo intestino . se questa rappresenta lunica limitazione dal punto di vista diagnostico , non va dimenticato che esistono anche degli svantaggi , che si estrinsecano prevalentemente in alcune limitazioni tecniche , che non sono solo costituite dalla intubazione , indispensabile , naso - intestinale , ma anche dal fatto che molto spesso , quando non adeguatamente standardizzata , la metodica pu risultare limitata nella definizione diagnostica in relazione alla distensione sub - ottimale dellileo , legata alla impossibilit di seguire fluoroscopicamente la progressione del mezzo di contrasto neutro fino al colon destro . accanto allalto costo globale dellesame esistono , infine , secondo alcuni autori , problematiche relative alla probabile maggiore invasivit biologica della metodica . tuttavia unanalisi accurata della dose totale assorbita durante un esame baritato del piccolo intestino e durante un esame msct per lo studio del tenue fornisce risultati sorprendenti . 
baseline spiral computed tomography , with intestinal opacification with iodinated contrast mediu clear demonstration of the segment of pelvic ileum with diffusely and evenly thickened walls and stenotic lumen , responsible for the patients occlusive symptoms . 
although this is the techniques only diagnostic limitation , it should be recalled that there are also some disadvantages , prevalently due to technical shortcomings : as well as requiring naso - intestinal intubation , the technique , when not adequately standardised , may very often suffer diagnostic limitations as a fig . 
however , a careful analysis of the total dose absorbed during a barium study and an msct study of the small bowel provides surprising results . considering that the total absorbed dose during a radiographic study of the small bowel consists not only of the dose delivered while acquiring the radiograms but also that delivered during fluoroscopy , total absorbed dose is represented by the sum of the dose delivered during naso - intestinal intubation , the dose absorbed during fluoroscopic assessment of the passage of the contrast agent , and the dose absorbed while acquiring the radiograms , with a mean absorbed dose in depth of around 24.48 mgy for each procedure . 
as regards ct enteroclysis , total absorbed dose is represented by the sum of the dose delivered during fluoroscopy for naso - jejunal intubation and the dose delivered during a single volumetric scan from the diaphragm to the pelvis , with a mean absorbed dose in depth of around 11.2 mgy for each procedure if a single - slice spiral scanner is used . 
even if this figure is multiplied by the number of detector rows used in msct , the total absorbed dose during msct - e will be similar to , if not lower than , that delivered by conventional small - bowel enteroclysis . experience has taught us that modalities performed with naso - intestinal intubation allow a more accurate assessment of the small bowel compared with examinations requiring oral administration of contrast material . 
in this sense , even msct - e confirms that the luminal distension obtained with direct administration of suitable contrast material allows better assessment not only of the bowel wall but of all structures surrounding hollow abdominal organs and is undoubtedly an important diagnostic tool . 
rollandi ga , curone pf , biscaldi e et al ( 1999 ) spiral ct of the abdomen after distention of small bowel loops with transparent enema in patients with crohns disease . 
dallapiccola 962 pp , 835 illustrazioni springer - verlag berlin , heidelberg ( 2005 ) isbn 3 - 540 - 67997 - 9 published online : 10 march 2006 ricordo che dellintenzione e desiderio di scrivere un volume sullargomento , ne sentii parlare dal castriotascanderbeg nel lontano 1994 , durante una delle pause del congresso annuale della european society of paediatric radiology in corso di svolgimento a bruxelles . 
da allora ho seguito la progressiva evoluzione del progetto e la sua gestazione nel corso di 12 anni , come specificato nella prefazione , le difficolt incontrate nella sua preparazione e nel reperimento del materiale da utilizzare , fino al compimento di questo , che considero il tipico miracolo italiano , frutto di una perseveranza e di una dedizione totale allopera da parte del castriota - scanderbeg , autore di buona parte del testo . lopera veramente monumentale divisa in due parti : la prima , in 9 capitoli ( di cui uno solo a due mani ) , dedicata alla trattazione delle anomalie di cranio , torace , rachide , pelvi , ossa lunghe , mani , piedi , articolazioni ed anomalie generalizzate dello scheletro ; la seconda , alla trattazione e descrizione di 111 sindromi . 
la base concettuale della prima parte costituita dalla descrizione dei singoli segni o alterazioni morfologiche dei componenti ossei della porzione di scheletro interessata ed in studio , segni che possono rientrare in un pi vasto quadro di alterazioni e lesioni e che , proprio per il loro aspetto , talvolta anche sfumato , devono o dovrebbero far sospettare , allosservatore attento , la presenza di una peculiare patologia . 
ad esempio , il primo capitolo , dedicato al cranio , suddiviso in 6 sezioni ( anomalie di forma e / o dimensioni del cranio ; anomalie dello sviluppo e dellossificazione ; anomalie della base cranica ; anomalie delle ossa facciali e dei seni paranasali ; anomalie della mandibola ; calcificazioni endocraniche ) , a loro volta comprendenti diverse sottosezioni , quali : microcefalia , macrocefalia , craniosinostosi , per la sezione dedicata alle anomalie di forma e / o dimensioni del cranio ; oppure difetti dellossificazione , ritardata chiusura e / o incompleta ossificazione delle suture e delle fontanelle , ossa wormiane , ispessimento del cranio , per la sezione dedicata alle anomalie dello sviluppo e dellossificazione . 
tale impostazione si ripete nei capitoli successivi , risultando pi o meno ampia , ma sempre esauriente , a seconda della porzione di scheletro in studio . ciascuna parte comprende la descrizione del quadro clinico e radiologico di base ; quello delle sindromi , displasie o malattie in cui lalterazione pu esser rintracciata [ ciascuna riportata con la relativa classificazione omim ( on line mendelian inheritance in man ) e mappatura genica , ove conosciuta ] ; una sinossi radiologica delle proiezioni necessarie per lo studio della parte e dei segni in base ai quali porre la diagnosi ; un elenco delle associazioni con malattie , sindromi , displasie , anomalie cromosomiche , per finire con una bibliografia aggiornata , nonostante la tumultuosa evoluzione delle conoscenze e delle scoperte , soprattutto in campo genetico . la seconda parte , scritta in collaborazione con il prof . dallapiccola , uno dei massimi genetisti italiani , che con il suo contributo rende lopera completa da un punto di vista clinico , dedicata alla descrizione di 111 sindromi , displasie ed anomalie cromosomiche : di ciascuna vengono elencate sinteticamente eponimi od altre denominazioni , frequenza , genetica , sintesi analitica delle caratteristiche cliniche e radiologiche , diagnosi differenziale e bibliografia : il tutto corredato da immagini cliniche e radiografiche significative e dimostrative . 
questa parte non comprende le possibili sindromi o displasie , ritrovabili in altri testi e a cui si fa preciso riferimento nellintroduzione . le immagini , sia cliniche che radiologiche , sono riprodotte con notevole fedelt , ad eccezione di alcune non originali , riprese da altri testi . 
esse forniscono una rappresentazione completa per giungere , in modo relativamente semplice , ad una interpretazione di quadri talvolta se non spesso tenui od oscuri e rari e perci non facilmente apprezzabili ed interpretabili sia dal radiologo generale che dal clinico . forniscono inoltre la possibilit di un apprendimento esaustivo a coloro che desiderano approfondire o illustrare correttamente tali aspetti . il testo infine completato da un minuzioso ed esaustivo indice analitico . 
simonetti1 1dipartimento di diagnostica per immagini e radiologia interventistica , universit degli studi di roma tor vergata , viale oxford 81 , i - 00133 roma , italy 2dipartimento di neuroscienze , universit degli studi di roma tor vergata , roma , italy correspondence to : f . 
the regions of interest were manually positioned on rcbf maps over the caudate nucleus , the putamen , the external and internal globus pallidus , and over the ventrolateral nucleus of the thalamus . 
our study suggests that pw - mri is a valuable tool for assessing haemodynamic changes in pd patients . haemodynamic change pattern may be useful in the early diagnosis of pd . key words parkinsons disease perfusion - weighted magnetic resonance imaging basal ganglia riassunto obiettivo . 
sono state posizionate manualmente delle regioni di interesse ( roi ) sulle mappe di rcbf a livello del caudato , putamen , pallido interno / esterno e a livello del nucleo ventrolaterale del talamo . 
 diagnosis of pd is currently a clinical diagnosis only based on history , disease course , and finding of at least two of the three basic symptoms of the disease , i.e. 
on the other hand , in the early stages of disease , it is impossible to arrive at a firm differential diagnosis between idiopathic pd and atypical vascular or degenerative parkinsonisms on the sole basis of clinical data and initial response to treatment . 
indeed , early pd , when symptoms are extremely mild and blurred , may show only a subtle , if any , response to dopaminergic therapy , just as subjects with atypical parkinsonism may exhibit a limited response to therapy , which can persist for 12 years . 
diagnosis based only of such criteria was found to be incorrect in 25% of cases subjected to post - mortem histological examination at the united kingdom brain bank in london [ 2 ]  . 
interest in such a differential diagnosis lies mainly in the different course of these diseases and in the significant difference in how they respond to treatment . the neuroimaging techniques that have been used in the differential diagnosis mainly rely on nuclear medicine methods , such as single proton emission computed tomography ( spect ) and positron emission tomography ( pet ) [ 38 ]  . although these methods are extremely sensitive in the early detection of depleted nigrostriatal nerve endings and useful in the follow - up [ 911 ] , their limited availability ( in particular in the case of pet ) , high costs , limited supply of tracers , and poor spatial resolution make them unsuitable as a routine aid in the early diagnosis of pd . for instance , pet is unable to distinguish , within the basal nuclei , the putamen from the globus pallidus and even less the lateral from the medial pallidus . 
current theories on the pathogenesis of pd assign often diametrically opposed functions to these structures . an examination comprising them without differentiation [ 12 , 13 ] carries a risk of underestimating those alterations . the reduced metabolism of the external pallidus should correspond to increased activity of the internal pallidus without affecting total activity [ 14 ]  . the purpose of this study was to use perfusion - weighted magnetic resonance imaging ( pw - mri ) as a diagnostic method to identify a specific perfusion pattern in the basal ganglia of pd subjects . il morbo di parkinson ( mdp ) una patologia neurodegenerativa caratterizzata da una preferenziale degenerazione dei neuroni dopaminergici a livello della pars compacta della sostanza nigra ( sn ) [ 1 ] e di altri pigmenti tronco - encefalici , nonch dalla comparsa , nei neuroni coinvolti nel processo degenerativo , di inclusioni citoplasmatiche note come corpi di levy . la diagnosi di morbo di parkinson attualmente una diagnosi clinica basata solo sulla anamnesi , sul decorso della malattia e sul riscontro obiettivo di almeno due dei tre sintomi cardine della patologia , vale a dire della rigidit , di una ipo - bradicinesia e del tremore a riposo con caratteristica asimmetria tra i lati corporei in termini di epoca di comparsa ed intensit dei sintomi ; inoltre di estrema rilevanza , sempre ai fini diagnostici , la risposta ai farmaci dopaminergici nel tempo . 
daltro canto , in fase iniziale del tutto impossibile arrivare a porre una diagnosi differenziale certa tra il morbo di parkinson idiopatico ed i parkinsonismi atipici su base vascolare o degenerativa , sulla sola base dei dati clinici e della risposta farmacologica iniziale ; infatti , nei pazienti con parkinson iniziale ( early pd ) il cui quadro clinico sia quindi estremamente lieve e sfumato , la risposta alla terapia dopaminergica pu non essere eclatante anche quando presente , cos come in soggetti affetti da parkinsonismi atipici si pu osservare una risposta alla terapia farmacologica che , ancorch ridotta , perdura per uno - due anni . una diagnosi effettuata esclusivamente sulla base di tali criteri , ha portato ad errore nel 25% dei casi sottoposti postmortem ad esame autoptico - istologico presso la brain bank di londra [ 2 ]  . 
linteresse per una tale diagnosi differenziale risiede principalmente nella differente evoluzione delle patologie sopra citate e nella notevole differenza della rispettiva risposta ai farmaci . fino ad oggi le tecniche di neuroimaging utilizzate per la valutazione di tale diagnosi differenziale si sono basate principalmente sulla utilizzazione di metodiche di medicina nucleare quali la spect e la pet [ 38 ]  . 
pur essendo tali metodiche altamente sensibili nel rilevare precocemente una deplezione delle terminazioni nervose nigro - striatali e utili nel follow - up della malattia [ 911 ] , la loro ridotta disponibilit ( in particolare della pet ) , gli alti costi , la ridotta disponibilit di traccianti e la scarsa risoluzione spaziale le rendono inadatte come supporto routinario alla clinica nella diagnosi precoce di mdp . 
infatti , ad esempio , la pet non permette di distinguere allinterno dei nuclei della base il putamen dal globo pallido e tanto meno il pallido laterale da quello mediale . molti degli studi effettuati con pet nel mdp hanno in effetti studiato le variazioni di densit recettoriale , fibre dopaminergiche o le variazioni di metabolismo nel nucleo lenticolare . 
in order to avoid any interferences caused by the effect of dopaminergic drugs on the basal ganglia flow [ 16 ] , the subjects were studied after at least 20 days withdrawal of dopaminergic treatment . 
a sagittal t2 - tse sequence ( slice thickness 3 mm , number of averages 3 ) was used to identify the two commissures on which we performed an axial t1 - se sequence , a t2 - weighted sequence using cerebral spinal fluid ( csf ) suppression [ axial fluid attenuated inversion recovery ( flair ) ] with a fov 230 mm , te 150 ms , tr 6 , 000 ms , ti 2 , 000 ms , slice thickness 5 mm , gap 1 mm , matrix 256x256 , number of averages 1 , acquisition time approximately 3 m the pw - mri study was carried out using a gradient echo ( ge ) , t2 * - weighted sequence with tr 620 ms , te 30 ms , al diminuito metabolismo del pallido esterno dovrebbe corrispondere un aumento di attivit in quello interno con una somma dei due probabilmente invariata [ 14 ]  . lo scopo di questo studio stato quello di utilizzare la rm perfusionale come metodica diagnostica per identificare uno specifico pattern di perfusione a livello dei gangli della base nei soggetti affetti da mdp . materiali e metodi sono stati studiati 20 soggetti affetti da parkinson idiopatico ( 11 maschi , 9 femmine ; et media 683 , 2 anni ) secondo i criteri della brain bank [ 15 ] , con una durata di malattia variabile tra i 52 , 4 anni . 
sono stati esclusi da questo gruppo di pazienti in studio , soggetti che presentavano altre patologie neurologiche e che non rispondevano alla terapia acuta . per evitare interferenze possibili dovute allazione dei farmaci dopaminergici sul flusso dei gangli della base [ 16 ] , i soggetti sono stati studiati dopo un periodo di interruzione del trattamento dopaminergico di almeno venti giorni . 
finally , the axial t1 sequence was repeated after administration of gadoliniu gadolinium diethylene triamine pentaacetate ( g - dtpa ) paramagnetic contrast material ( magnevist , schering , berlin , germany ) was injected as a bolus , 0.4 mmol / kg , while the subjects held their eyes closed , via an 18 - gauge needle cannula inserted into an antecubital vein of the arm using an automatic injector with a 4 ml / s flow rate . perfusion data were processed by dedicated software on an independent console to obtain perfusion maps to calculate cerebral blood flow ( rcbf ) according to the technique previously reported by apruzzese et al . 
then , ten - pixel regions of interest ( rois ) were manually placed on the rcbf maps in the following regions : head of the caudate nucleus ( cn ) , putamen ( pu ) , external and internal globus pallidus ( egp / igp ) separately , and ventrolateral nucleus of the thalamus ( th )  . 
perfusion data were calculated as the average of every roi positioned on the basal nuclei and powm on every side and values obtained were transformed into logarithms and normalised as a percentage of the value obtained with the ipsilateral powm . in order to determine asymmetries ( contrast effect ) , the normalised data of each nucleus were expressed as the ratio between the nucleus being studied and the corresponding contralateral nucleus according to the formula : ( r nucleus l nucleus ) / ( r nucleus + l nucleus ) * 100 . 
in pd patients , the formula was expressed as : [ ( less affected side more affected side ) / ( less affected side + more affected side ) * 100 ] based on their clinical asymmetry . 
we used the third section of the unified parkinsons disease rating scale ( updrs ) as a score of pd motor disability , ranging from 0 ( normal ) to 180 ( maximum disability ) [ 18 ]  . 
in order to compare contrast data in the two groups , the factors group and nuclei were used . results all patients with pd showed a significant ( f ( 1 / 37 ) = 7.98 ; p < 0.01 ) difference in the average rcbf on the better side ( bs ) 1 , 5 tesla ( philips medical - system , best , olanda ) con intensit di gradiente di 30 mt con profilo sinusoidale e con una bobina in quadratura standard dedicata per lo studio dellencefalo . abbiamo eseguito una sequenza t2 tse sul piano sagittale ( spessore di strato 3 mm , numero di medie 3 ) per la individuazione delle due commessure sulle quali abbiamo impostato una sequenza t1 se assiale , una sequenza t2 pesata con la tecnica della soppressione liquorale ( flair assiale ) con fov 230 mm , te di 150 ms , tr = 6000 ms , ti = 2000 ms , spessore di strato 5 mm gap di 1 mm , matrice 256x256 , numero di medie 1 con un tempo di acquisizione di 3 minuti circa . lo studio rm perfusionale stato effettuato utilizzando una sequenza gradient echo ( ge ) t2 * pesata con un tr = 620 ms , te = 30 ms , spessore di strato = 7 , gap = 0 mm , numero di medie 1 , flip angle = 40 , matrice = 128x128 , tempo di acquisizione = 1 , 17 min , al fine di ottenere una serie di immagini dinamiche a suscettibilit di contrasto t2 pesate acquisite durante il passaggio di mdc . 
il mdc paramagnetico gadolinio - dtpa ( magnevist , shering , berlino , germania ) stato iniettato a bolo , 0 , 4 mmol / kg mentre i soggetti tenevano gli occhi chiusi , mediante iniettore automatico con una velocit di flusso pari a 4 ml / s ed attraverso un ago - cannula del calibro di 18 gauge posizionato in una vena antecubitale del braccio . 
i dati di perfusione sono stati elaborati tramite software dedicato su consolle indipendente , ottenendo quindi mappe di perfusione per il calcolo del flusso ematico cerebrale ( rcbf ) , in accordo a quanto gi descritto da apruzzese et al . 
in un precedente lavoro [ 17 ]  . sono state quindi posizionate manualmente sulle mappe dellrcbf delle roi di 10 pixel a livello della testa del nucleo caudato ( cn ) , a livello del putamen ( pu ) , a livello del globo pallido esterno ed interno ( gpe / gpi ) separatamente , ed a livello del nucleo ventrolaterale del talamo ( th )  . 
i dati della perfusione sono stati calcolati come la media di ogni roi posizionata a livello dei nuclei della base e di quelle posizionate a livello della wpom di ogni lato , i valori ottenuti sono stati trasformati in logaritmo , e quindi normalizzati come percentuale del valore ottenuto con la wpom omolaterale . 
per la determinazione delle asimmetrie ( effetto contrasto ) le normalizzazioni dei dati relativi a ciascun nucleo sono stati espresse come rapporto tra il nucleo in esame ed il corrispondente controlaterale , secondo la formula : ( nucleo dx - nucleo sn ) / ( nucleo dx + nucleo sn ) * 100 . 
nei pazienti con morbo di parkinson la formula stata espressa come : [ ( lato meno affetto - lato pi affetto ) / ( lato meno affetto + lato pi affetto ) * 100 ] in accordo con la loro asimmetria clinica . 
abbiamo usato la sezione iii dellupdrs ( unified parkinsons disease rating scale ) come score di disabilit motoria nel parkinson che va da 0 ( normale ) a 180 ( massimo livello di disabilit ) [ 18 ]  . 
seven patients with pd had abnormal contrast values in all nuclei under study whereas these were normal in all control subjects . traendo lo score del lato meno affetto da quello del lato pi affetto . per lanalisi dei dati stato utilizzato un software statistica per windows . 
la correzione di greenghouse geisser stata utilizzata quando necessario . in caso di significativit di un fattore con pi di due livelli od in caso di significativit di interazioni tra fattori stato utilizzato il tukey test come post hoc . per comparare i dati contrasto , nei due gruppi sono stati usati i seguenti fattori : gruppo , nuclei . discussion the diagnosis of pd remains largely clinical and is based on the presence of the three characteristic pathognomonic symptoms . 
pet and spect are still , however , very costly methods , use of which is restricted to a small number of highly specialised centres ; hence , they cannot be proposed as screening tests . 
over the last few years , various researchers have used pw - mri to measure cbf in several diseases of neuroradiological concern . the literature does not provide information on possible altered flow values detected in degenerative diseases such as pd with pd patients controls fig . 
2 il grafico evidenzia una asimmetria interemisferica dei valori di rcbf nei gangli della base nei pazienti con mdp non presente nei soggetti controllo . risultati nella totalit dei pazienti con mdp si dimostrato una significativa ( f ( 1 / 37 ) = 7 , 98 ; p < 0 , 01 ) differenza dellrcbf medio nel lato migliore ( bs ) vs . 
la differenza risulta essere simile in tutti i nuclei studiati cos che nessuna interazione significativa gruppox nuclei stata riscontrata . sedici dei 20 pazienti con mdp hanno mostrato un anormale indice di contrasto nel putamen e 13 hanno mostrato la stessa anormalit nel talamo . solamente 5 soggetti controllo hanno mostrato valori anormali nel putamen e nessuno nel talamo . 
sette pazienti con mdp hanno mostrato valori anormali di contrasto in tutti i nuclei studiati , mentre in nessuno dei soggetti controllo si evidenziato tale riscontro . discussione la diagnosi di morbo di parkinson rimane prevalentemente clinica e si basa sulla presenza della caratterizzazione della triade sintomatologia patognomonica . 
a possible explanation of this result might be the loss of dopamine in the affected side , which could result in a maximum increase in the baseline rcbf on this side , an asymmetry that was never observed in control subjects . 
wolfson conducted a cerebral perfusion study using pet on patients affected by mild - to - moderate forms of unilateral and bilateral pd , finding blood flow asymmetry in the basal ganglia on both sides and with respect to controls . 
other pet studies , on the other hand , did not find any asymmetry between homologous basal ganglia regions but only when the rcbf in basal ganglia was compared with the flow in critical cortical areas [ 19 ]  . 
we were also able to detect a perfusion asymmetry in most pd patients ( 65%80% ) by analysing homologous sub - regions of basal nuclei , thanks to the higher resolution of mri relative to pet . we believe that future studies analysing the ratio between cortical areas and basal ganglia might be useful to better demonstrate the abnormalities found in our investigation . pochi centri ad elevata specializzazione , non quindi proponibile il loro impiego come esame di screening . la rm , al contrario , una metodica molto pi diffusa , meno dispendiosa e disponibile in numerosi centri di diagnostica per immagini . 
tuttavia , a tuttoggi , non sono riportati dati in letteratura circa la possibilit di evidenziare alterati valori di flusso nellambito di patologie degenerative come la mdp mediante la rm perfusionale . il nostro lavoro , unico nel suo genere , si propone di valutare alterazioni perfusionali a livello dei nuclei della base , nei soggetti con mdp . i nostri dati mostrano una notevole asimmetria dellrcbf tra il lato pi affetto ed il lato meno affetto nei nuclei della base dei pazienti con mdp . 
una possibile spiegazione di tale risultato , a nostro giudizio , potrebbe essere dovuta alla maggior perdita di dopamina nel lato affetto , che potrebbe indurre un incremento massimale del rcbf in questo lato in condizioni basali . 
tale asimmetria non stata , infatti , mai osservata nei soggetti controllo . una relativa asimmetria dellrcbf nei gangli della base , stata riportata anche in altri studi con pet nei pazienti con mdp unilaterale o bilaterale . 
wolfson ha condotto uno studio di perfusione cerebrale , valutata con la pet , su pazienti affetti da forme lievi / moderate di mdp mono e bilaterale ed ha evidenziato una asimmetria del flusso a livello dei gangli della base di entrambi i lati e rispetto ai controlli . 
altri studi con pet , invece , non hanno mostrato asimmetria tra regioni dei gangli della base omologhe , ma solamente se lrcbf dei nuclei della base erano comparati con quelli di aree corticali critiche [ 19 ]  . il nostro studio conferma in parte questi dati , come precedentemente descritto , attraverso una metodica molto meno dispendiosa quale la risonanza magnetica perfusionale . 
stato inoltre possibile , grazie alla pi alta risoluzione della rm rispetto alla pet , rivelare unasimmetria perfusionale nella maggioranza dei pazienti con mdp ( 65%80% ) esaminando subregioni omologhe dei nuclei della base . 
riteniamo che studi futuri , che analizzeranno la ratio tra le aree corticali ed i gangli della base , potrebbero essere utili per dimostrare ancor meglio le anormalit evidenziate nel nostro lavoro . conclusioni conclusions pw - mri appears to be a valid method in the diagnosis of pd since it can identify blood flow asymmetry in the basal nuclei in both hemispheres . 
the low cost of this method , its wide availability , and its higher resolution compared with other functional imaging modalities ( pet , spect ) make pw - mri extremely useful and expedient as a support tool for the early diagnosis of pd . la rm perfusionale sembra essere una metodica valida per la diagnosi di mdp , essendo in grado di individuare unasimmetria di flusso a livello dei nuclei della base dei due emisferi . 
bacci1 1sezione di chemioterapia , 2servizio di radiologia , dipartimento di oncologia muscoloscheletrica , istituti ortopedici rizzoli , via pupilli 1 , i - 40136 bologna , italy correspondence to : a . 
between march 1997 and december 2001 at our department of musculoskeletal oncology , 231 patients with peripheral osteosarcoma received a central venous catheter to allow infusion therapy and blood sampling . 
in ten cases ( 4.3% ) , radiology showed damage to the alveolar interstitium typical of inflammatory forms , whereas in the remaining three ( 1.3% ) it depicted nodular opacities , which required differentiation between lung metastases and septic emboli . 
the most common complications of the use of central venous catheters include infection and venous thrombosis whereas pulmonary septic emboli are rare . key words osteosarcoma pulmonary metastases pulmonary nodules differential diagnosis riassunto obiettivo . 
da marzo 1997 a dicembre 2001 , presso il nostro dipartimento di oncologia muscoloscheletrica stato inserito un catetere venoso centrale per permettere terapia infusionale e prelievi ematici a 231 pazienti affetti da osteosarcoma periferico . 
in 10 casi ( 4 , 3% ) il quadro radiologico era di impegno interstizio alveolare tipico delle forme flogistiche , mentre nei restanti 3 ( 1 , 3% ) si osservarono delle opacit nodulari che posero problemi di diagnosi differenziale fra metastasi polmonari ed emboli settici . 
le complicanze pi frequenti dellutilizzo del catetere venoso centrale sono le infezioni e le trombosi venose , mentre gli emboli settici polmonari sono rari . parole chiave osteosarcoma metastasi polmonari noduli polmonari diagnosi differenziale introduction introduzione the use of hickman , broviac and groshong indwelling central venous catheters ( cvcs ) , which remain in place for months or years , is highly important for cancer patients who require prolonged chemotherapy and support infusion therapies . 
venous catheters connected with their port to a central venous line , such as infuse - a - port or port - a - cath , have also been used with success . 
vein perforation , generally caused by the insertion of the catheter or its incorrect positioning , is fortunately an uncommon immediate or early complication . the most frequent late complications are venous thrombosis of the vessel in which the catheter is positioned and infections . 
the incidence of thrombosis varies between 12% and 74% and is higher in cancer patients [ 1 ]  . the thrombosis may be located in the vessel or in the catheter lumen ; only one - third of thromboses are symptomatic . 
a number of studies [ 24 ] have demonstrated that thrombosis is one of the main risk factors for catheter infection whereas infections occur in 15%20% of cases [ 5 , 6 ]  . septic emboli resulting from catheter infection are a wellknown but uncommon complication , even in children and adolescents [ 6 , 7 ]  . the central venous line is a very important tool for delivering chemotherapy , especially in children . 
many studies have demonstrated the usefulness and feasibility of prolonged use , up to years , of a cvc even in children , with an acceptable incidence of complications : displacement , occlusion and infection [ 710 ]  . 
the aim of this study was to highlight the problems of differential diagnosis and the possible solutions using conventional radiography and computed tomography ( ct )  . materials and methods between march 1997 and december 2001 , the division of chemotherapy of our institution treated 253 patients with adjuvant chemotherapy for primitive bone sarcomas . 
anche i cateteri venosi collegati con la propria porta ad un catetere venoso centrale tipo infuse - a - porth o port - a - cath sono impiegati con successo . entrambi i tipi di cateteri sono associati a possibili complicazioni sia precoci che tardive . 
alcuni studi [ 24 ] hanno dimostrato che la trombosi uno dei principali fattori di rischio per linfezione del catetere venoso centrale , mentre le infezioni sono una complicanza che si verifica in circa il 15%20% dei casi [ 5 , 6 ]  . 
gli emboli settici conseguenti a infezioni del catetere sono una complicanza ben conosciuta , pur se non frequente , anche nei pazienti pediatrici od adolescenti [ 6 , 7 ]  . il catetere venoso centrale uno strumento molto importante per la somministrazione della chemioterapia in particolare nei bambini . 
molti studi hanno dimostrato lutilit e la fattibilit di un uso prolungato , talora per anni , del catetere venoso centrale anche in pazienti pediatrici con una percentuale accettabile di complicanze : dislocazioni , occlusioni ed infezioni [ 710 ]  . 
lo scopo del lavoro di evidenziare le problematiche di diagnosi differenziale e le possibilit di soluzione mediante radiologia tradizionale e tomografia computerizzata ( tc )  . materiali e metodi dal marzo 1997 al dicembre 2001 , presso lunit operativa di chemioterapia del nostro istituto sono stati trattati con chemioterapia adiuvante per osteosarcoma primitivo 253 pazienti ; 34 di questi pazienti presentavano metastasi alla diagnosi : 31 al polmone e 3 in altri segmenti ossei ; in 219 pazienti la lesione era localizzata . 
a 231 pazienti fu inserito un catetere venoso centrale : 228 cvc tipo broviac e 3 port - a - cath ; 22 pazienti tutti adulti rifiutarono il posizionamento del catetere . 
a second radiological assessment of the primary cancer with ct and mri , and chest ct was performed at the end of preoperative chemotherapy ( lasting four to six cycles , depending on the protocol ) , and before surgery . 
given the prolonged anticancer treatment typical of osteosarcoma ( 3643 weeks , depending on the protocol ) , conventional chest radiography was performed every 2 months to exclude the development of metastasis . in order to prevent catheter occlusions , 5 cc of heparin solution ( 20 cc of saline plus 3 cc of sodium heparin equal to 5 , 000 iu diluted in 100 cc of saline ) was injected into the central venous line every other day . 
patients with neutropoenia ( neutrophils < 500 / mm3 ) received granulocyte colony stimulating factors ( gcsf ) , together with a broad - spectrum antibiotic such as trimethoprim , sulfamethoxazole or ceftriaxone , at a dose of 5 g / kg per day until the white blood cell count ( wbc ) reached a concentration of at least 10 , 000 / mm3 . 
he received neoadjuvant chemotherapy from july 1998 to june 1999 after a broviac central venous catheter had been positioned in the left subclavian veone week after the last chemotherapy cycle ( cisplatin ) , the patient developed chills and fever ( 39c ) while at home . 
central and peripheral blood cultures were performed , both of which were positive for staphylococcus aureus and , on the basis of the antibiogram , antibiotic therapy with 200 mg / day teicoplanin was started , leading to remission of the fever . 
three weeks , later the patient was admitted for removal of the cvc and final staging with lung ct . the material sampled from the catheter after removal showed colonies of s . 
ct , performed on the same day ( 20 july 1999 ) , revealed the presence of a nodular opacity in the posterior segment of the lower right lobe that was suggestive of pulmonary metastasis from osteosarcoma teteri , usati sia per la somministrazione della chemioterapia che per prelievi ematici , furono posizionati prima dellinizio dei cicli di chemioterapia , previo consenso informato . tutti i pazienti ricevettero chemioterapia secondo i protocolli in uso al momento , ior / os - n4 o ior / os - n5 , impiegati dal 1997 al 2001 con i seguenti farmaci : adriamicina , cisplatino , ifosfamide , pi metotrexate nei pazienti al di sotto dei 40 anni ( precedentemente riportati in dettaglio [ 11 , 12 ] )  . la stadiazione radiologica di base comprendeva tc e rm del tumore primitivo osseo , scintigrafia ossea e tc del torace per escludere lesioni sostitutive secondarie polmonari . una seconda valutazione radiologica con tc ed rm del tumore primitivo e tc del torace stata eseguita al termine della chemioterapia preoperatoria ( durata 46 cicli a seconda del protocollo ) , prima dellintervento chirurgico . 
dato il prolungato trattamento antiblastico tipico dellosteosarcoma ( da 36 a 43 settimane a seconda del protocollo ) uno studio radiologico tradizionale del torace veniva eseguito ogni 2 mesi per escludere la comparsa di metastasi . a scopo profilattico , per evitare occlusioni del catetere , a giorni alterni si iniettavano nel catetere venoso centrale 5 cc di soluzione eparinata ( 20 cc di soluzione fisiologica pi 3 cc di eparina sodica pari a 5000 ui diluiti in 100 cc di soluzione fisiologica )  . 
in caso di neutropenia ( neutrofili inferiori o uguali a 500 / mm3 ) fattori stimolanti la crescita di colonie ( gcsf ) , congiuntamente ad un antibiotico ad ampio spettro tipo trimethoprim , sulfametoxazolo o cefriaxone , venivano somministrati ai pazienti alla dose di 5g / kg / die fino a che la concentrazione dei globuli bianchi ( wbc ) non raggiungeva il valore di 10000 / mm3 . tredici pazienti su 231 ( 5 , 6% ) svilupparono uninfezione del catetere venoso centrale . 
in 10 pazienti ( 4 , 3% ) lindagine radiologica tradizionale e / o la tc del torace evidenziarono un impegno interstizio - alveolare tipico delle forme flogistiche e nei restanti 3 ( 1 , 3% ) opacit nodulari , alcune delle quali a margini regolari che posero problemi di diagnosi differenziale con lesioni metastatiche . caso 1 maschio , 7 anni , con osteosarcoma osteoblastico localizzato allomero destro . 
una settimana dopo lultimo ciclo di chemioterapia ( cisplatino ) , il paziente ebbe , a domicilio , un episodio di febbre ( 39c ) con brividi ; esegu due emocolture : una da prelievo centrale e una da prelievo periferico . 
although the patient was asymptomatic , the recent cvc infection was thought to have caused the spread of a septic embolus to the lung , so antibiotic therapy with teicoplanin ( 200 mg / day ) was administered for a further 15 days . 
shortly after the end of the last cycle of postoperative chemotherapy , he developed a fever ( 40c ) and was treated at home with a broad - spectrum antibiotic that failed to resolve the fever . two - view chest radiography performed at the patients home was negative . 
on june 15 , the patient was admitted , and the cultures of material sampled from the central venous line and a peripheral vein both revealed the presence of pseudomonas fluorescens sensitive to piperacillthe central venous line was removed . 
poco dopo il termine dellultimo ciclo di chemioterapia postoperatoria , ebbe febbre ( 40c ) e inizi a domicilio terapia antibiotica a largo spettro che non ne determin la remissione . il radiogramma tradizionale del torace eseguito in due proiezioni al domicilio del paziente era negativo . 
il 15 giugno il paziente fu ricoverato e le emocolture del materiale prelevato dal catetere centrale a da vena periferica evidenziarono entrambe la presenza di psudomonas fluorescens sensibile alla piperacillina . 
nello stesso giorno il paziente esegu , come da protocollo , tc del torace di fine cura , che evidenzi la presenza di tre opacit nodulari nel polmone destro : la prima nel segfig . 
1a , b the first computed tomography ( ct ) study shows a nodular opacity measuring 15 mm in diameter with slight irregular margins in the posterobasal segment of the right lower lobe ( a )  . 
1a , b il primo esame evidenzia una opacit nodulare di 15 mm di diametro a margini leggermente irregolari nel segmento posterobasale del lobo inferiore di destra ( a )  . 
2a - d the first computed tomography ( ct ) study shows three subpleural nodular opacities ( arrows ) , two measuring a few millimetres : the first has paracardiac location in the middle lobe and no feeding vessel sign ; the second is in the laterobasal segment of the right lower lobe ( a ) ; the third is larger and located in the posterobasal segment of the right lower lobe ( b )  . 
2a - d il primo esame tc evidenzia tre opacit nodulari subpleuriche ( frecce ) di cui due millimetriche : la prima localizzata in sede paracardiaca a livello del lobo medio senza il segno del vaso che nutre , la seconda nel segmento laterobasale del lobo inferiore destro ( a ) , la terza opacit , di dimensioni superiori , nel segmento posterobasale del lobo inferiore di destra ( b )  . 
dopo somministrazione di terapia specifica , il secondo esame tc eseguito tre mesi dopo , non evidenzia pi alcuna lesione ( c , d )  . case 3 a 17 - year - old girl with fibroblastic osteosarcoma of the right femur . 
chest radiography demonstrated two nodular opacities in the middle third of the right lung field , both of which where strongly suspicious for metastases . chest ct performed immediately confirmed the presence of the lesions , which were subpleural and with slightly irregular margins , one in the anterior segment and the other in the posterior segment of the lower lobe . 
chemioterapia neoadiuvante dal dicembre 2000 attraverso un catetere centrale tipo broviac . terminato il nono ciclo di chemioterapia , la paziente ebbe un episodio di neutropenia febbrile risoltosi con somministrazione di terapia antibiotica a largo spettro e di fattori stimolanti la crescita . 
la tc del torace eseguita immediatamente conferm la presenza delle due lesioni entrambe subpleuriche e con margini lievemente irregolari , una nel segmento anteriore e laltra nel segmento posteriore del lobo inferiore . 
la paziente a tuttoggi viva , senza lesioni sostitutive . discussione losteosarcoma un tumore osseo estremamente maligno tipico dei bambini e degli adolescenti con un picco tra i 15 ai 25 anni [ 13 ]  . 
il polmone rappresenta , infatti , la pi frequente sede ( 90% di tutte le sedi di metastasi ) di metastasizzazione di questo tumore alla diagnosi e durante il follow - up [ 17 ]  . 
3a - c the first computed tomography ( ct ) study shows two subpleural nodular opacities ( arrows ) : the first in the apical segment of the right lower lobe ; the second , clearly inflammatory , in the lateral segment of the middle lobe ( a )  . 
the second ct study performed after 20 days shows disappearance of the two opacities , with moderate residual subpleural fibrosis in the middle lobe and the presence of a new opacity with irregular and fluffy margins contiguous with a pulmonary vessel in the posterolateral segment of the right lower lobe ( b )  . 
3a - c il primo esame tc evidenzia due opacit nodulari subpleuriche ( frecce ) : la prima nel segmento apicale del lobo inferiore destro , la seconda chiaramente flogistica nel segmento laterale del lobo medio ( a )  . 
il secondo esame tc , eseguito a 20 giorni di distanza , mostra la scomparsa delle due opacit con modesto esito fibrotico subpleurico nel lobo medio e la presenza di unaltra opacit , a contorni irregolari e sfrangiati in continuit con un vaso polmonare nel segmento posterolaterale del lobo inferiore destro ( b )  . 
the lung is often the first site of metastatic spread of many solid tumours [ 16 ] , and this is particularly true for osteosarcoma . the lung is the most frequent site of metastasis ( 90% of all metastasis sites ) of this tumour at presentation and during follow - up [ 17 ]  . osteosarcoma of the extremities tends to metastasize within the first 5 years of diagnosis in 30%40% of cases [ 13 ]  . 
early diagnosis of such lesions may in some cases dramatically increase the survival of patients after appropriate treatment : thoracic surgery and / or chemotherapy . all osteosarcoma protocols require ct scans at baseline and after treatment and conventional chest radiography every 2 months during chemotherapy . 
despite not having the same reliability as ct in detecting metastasis , conventional chest radiography in two views anteroposterior ( ap ) and laterolateral ( ll ) is just as effective in identifying metastatic lesions with a diameter of 1 cm or more , it is easy to perform and it is inexpensive . 
in addition , entrance dose and absorbed dose are much lower than in ct : 1.9 mgy / msi versus 30 mgy / msi , ctdiw / 650 mgy / msi - cm dlp . development of lung metastases during treatment is a rare but possible occurrence . 
mediastinal lymph nodes are rarely involved [ 13 ]  . oncological patients who are free of disease may , however , develop pulmonary nodules of varying size , shape and location , as has been reported by many studies [ 1824 ]  . 
almost all of cases reported were treated either with drugs with minimal bone marrow toxicity and high pulmonary toxicity or drugs and radiotherapy [ 19 ]  . many underwent segmental or lobar resection . 
histology revealed not only metastatic nodules but also the presence of nodular lesions of other natures : nodular nonspecific intersitial pneumonia or fibrosis in patients with peripheral infusion of drugs with high pulmonary toxicity , such as bleomycin [ 2024 ] or nodular lesions caused by infection by opportunistic organisms ( cryptococcus neoformans , aspergillus fumigatus , or others ) in patients treated with radiotherapy who became immunocompromised . infectious processes may also include septic emboli developing inside the cvc or migrating there from other sites . 
the finding of areas of pulmonary consolidation of varying shape on ct scans of cancer patients represents a challenge , and the differential diagnosis is one of the radiologists routine tasks . 
 lung nodules identified in our three patients were both subpleural and parenchymal ; they had similar density but ri metastatici osservati su un radiogramma del torace e / o una tc del torace in pazienti con tumore primitivo extrapolmonare da considerarsi segno prognostico infausto . 
una diagnosi precoce di lesioni sostitutive pu talora dare lopportunit di una lunga sopravvivenza al paziente dopo adeguata terapia : chirurgia toracica e / o chemioterapia . tutti i protocolli per gli osteosarcomi richiedono una tc di base allinizio del trattamento , unaltra alla fine e radiogrammi tradizionali del torace ogni due mesi durante il lungo periodo della chemioterapia . 
il radiogramma tradizionale del torace in due proiezioni ( p - a e l - l ) pur non avendo la stessa affidabilit della tc nel rilevare metastasi egualmente efficace nellevidenziare lesioni sostitutive di diametro pari o superiore al centimetro , di facile esecuzione , poco costoso , inoltre la dose allingresso / dose assorbita sono di molto inferiori a quelle di una tc : 1 , 9 mgy / msi versus 30 mgy / msi , ctdiw / 650 mgy / msi - cm dlp . 
i linfonodi mediastinici sono raramente coinvolti [ 13 ]  . tuttavia in pazienti neoplastici liberi da malattia possibile osservare la comparsa di noduli polmonari di dimensioni , forma e sede variabile ; tale comparsa stata descritta in molti lavori [ 1824 ]  . 
quasi tutti questi pazienti sono stati trattati o solo con farmaci a minima tossicit midollare ed ad alta tossicit polmonare o con farmaci e radioterapia [ 19 ]  . molti di questi pazienti furono sottoposti a resezione chirurgica segmentaria o lobare . 
lesame istologico rivel non solo la presenza di noduli metastatici , ma anche la presenza di lesioni nodulari di differente natura : polmoniti interstiziali nodulari aspecifiche e fibrosi polmonare interstiziale nodulare in pazienti con infusione periferica di farmaci ad alta tossicit polmonare come la bleomicina [ 2024 ] o lesioni nodulari di natura infettiva provocate da organismi opportunisti ( criptococcus neoformans , aspergillus fumigatus o altri ) in pazienti precedentemente trattati con radioterapia e divenuti ospiti immunocompromessi . 
i sintomi clidifferent shape , being rounded or lobulated but never reticular ; their margins were smooth and regular or fluffy and irregular , but never hazy ; size varied between 3 mm and 25 mthe two patients in whom the catheter was removed immediately and s . 
lung metastases from any primary cancer are well - marginated nodular opacities that are at times very calcific ( especially in osteosarcoma ) ; they tend to have peripheral location but have no predilection for the upper , middle or lower lobes [ 25 ]  . in our three cases , all pulmonary nodules simulating metastases appeared during chemotherapy in patients with broviac cvcs positioned in the subclavian vein for the delivery of chemotherapy , transfusions or blood sampling . 
none of the three patients had symptoms of pulmonary embolism . three cases of pulmonary septic embolism out of 231 patients with cvc is indeed a small percentage ( 1.3% ) , in agreement with other studies [ 6 ]  . 
pulmonary infection could have been the cause rather than the consequence of cvc infection but , given that culture of material retrieved from the distal lumen of the catheter was positive in two out of three cases , the cause of the haematopulmonary infection was far more likely to have been the cvc . the three cases described demonstrate that cvc infection can cause pulmonary septic embolism with variable imaging features . 
le metastasi polmonari , qualunque sia lorigine del tumore primitivo , sono opacit nodulari a margini netti , ben definiti , talora molto calcifiche ( specialmente nellosteosarcoma ) ; sono generalmente localizzate perifericamente ma senza predilezione di sede tra lobo superiore , medio od inferiore [ 25 ]  . nei nostri tre pazienti tutti i noduli polmonari che simulavano metastasi apparvero in corso di chemioterapia in pazienti con catetere venoso centrale tipo broviac inserito in una vena succlavia ed utilizzato per chemioterapia , trasfusioni o prelievo ematico . 
tre casi di emboli settici polmonari su 231 pazienti portatori di cvc una piccola percentuale ( 1 , 3% ) , in accordo coi risultati di altri studi [ 6 ]  . 
la flogosi polmonare potrebbe essere stata la causa e non la conseguenza dellinfezione del catetere venoso centrale , ma dal momento che lesame colturale effettuato sul materiale prelevato dal lume distale del catetere fu positivo in due dei tre casi , sembr estremamente pi probabile che la causa dellinfezione emato - polmonare fosse il catetere venoso centrale . 
nondimeno , aree polmonari di aumentata densit , in soggetti neutropenici e portatori di catetere venoso centrale deve suggerire , tra le altre ipotesi diagnostiche , la possibilit di unembolizzazione settica nodulare secondaria alla presenza ed allinfezione del catetere venoso centrale . 
in addition , the specificity of ct in evaluating the nature of a pulmonary nodule , especially when small , is still limited , and only biopsy or nodule excision are able to reveal the benign or malignant nature of the nodule through histological examination whereas evolution of the radiological finding can only guide the diagnosis between benign or malignant nodular opacities [ 26 ]  . conclusions correct diagnosis of a pulmonary opacity is fundamental for the prognosis and choice of treatment ( surgical ) in a patient with a doubtful lung lesion . 
 in the presence of a cvc , any change in shape ( rounded , lobulated , irregular , fluffy ) in relationship with a vessel ( contiguous , distal ) and in location ( apical , medial , basal ) of an area of lung consolidation seen on serial ct scans , both during and after chemotherapy , is an important clue for pulmonary septic embolism secondary to cvc infection regardless of antibiotic treatment . catheter replacement , central and peripheral blood cultures , administration of specific antibiotic treatment based on blood cultures and ct follow - up of nodular opacities must always be given priority with respect to surgical treatment . mento che possono essere normali o non specifici [ 22 ] come pure laspetto radiologico di noduli polmonari a differente eziologia . 
inoltre la specificit della tc , nella valutazione di natura , benigna o maligna , di un nodulo polmonare , specialmente se questo di piccole dimensioni , ancora limitata e solo la biopsia o lasportazione del nodulo sono in grado di rivelare la vera natura della lesione permettendone lesame istologico , mentre levoluzione del reperto radiologico pu unicamente orientare la diagnosi tra opacit nodulare benigna o maligna [ 26 ]  . conclusioni la corretta diagnosi di una opacit polmonare di vitale importanza per la prognosi ed il differente trattamento terapeutico ( chirurgico ) nel caso di paziente con lesione polmonare dubbia per metastasi . 
de vargas macciucca , via alberico albricci 28 , i - 00194 roma , italy , tel . : + 39 - 338 - 5924034 , fax : + 39 - 06 - 49970212 , e - mail : marinadevargasm@hotmail.com received : 2 february 2005 / accepted : 7 november 2005 / published online : 3 march 2006 abstract purpose . 
we retrospectively reviewed 35 patients ( 23 men and 12 women ; mean age 66.6 years ) presenting with acute cholecystitis who were assessed by emergency ultrasonography ( us ) ( 30 / 35 cases ) and spiral ct ( 12 / 35 cases ) ; all patients underwent emergency surgery . 
the us signs were analysed and classified as major criteria ( wall thickening and stratification , distension , murphys sign ) , minor criteria ( bile stones , sludge , and biliary tract dilatation ) , and complication signs ( gas collections , aerobilia , fluid collection , difficult or missed identification of the gallbladder )  . 
imaging results were compared with histological findings ( gold standard ) , and accuracy , sensitivity , specificity , and positive and negative predictive values ( ppvs and npvs ) were assessed for each modality . 
if more than two major signs associated with one minor sign or at least one sign of complication are present at us , ct is mandatory to recognise and thoroughly evaluate the type of complication and indicate appropriate treatment . key words acute cholecystitis complicated cholecystitis us spiral ct riassunto scopo . 
sono stati esaminati retrospettivamente 35 pazienti ( 23 uomini e 12 donne ; et media 66 , 6 anni ) affetti da colecistite acuta , valutati in urgenza con esame ecografico ( 30 / 35 casi ) e tc ( 12 casi ) e sottoposti a intervento chirurgico urgente . 
i parametri ecografici sono stati analizzati e classificati come criteri maggiori ( ispessimento parietale , stratificazione parietale , sovradistensione , segno di murphy ecografico ) , minori ( calcoli o sedimenti nella colecisti o nelle vie biliari , dilatazione delle vie biliari ) e segni di complicazione ( raccolte gassose , aerobilia , raccolte fluide , difficile o mancato riconoscimento della colecisti )  . i risultati dellimaging sono stati confrontati con quelli dellesame istologico ( gold standard ) e sono state valutate accuratezza , sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) delle rispettive metodiche . 
lecografia ha dimostrato una accuratezza del 66 , 6% , una sensibilit del 37 , 5% , una specificit del 70% , un vpp del 100% e un vpn del 58 , 3% . 
in presenza di pi di due segni maggiori e uno minore o di almeno un segno di complicazione allecografia , lesame tc raccomandabile per il riconoscimento e la completa valutazione del tipo di complicazione , fornendo la giusta indicazione allintervento chirurgico urgente . parole chiave colecistite acuta colecistite complicata ecografia tc - spirale m . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis introduction introduzione the clinical suspicion of acute cholecystitis is one of the most frequent conditions facing the radiologist in emergency settings , as well as being the fourth cause of hospitalisation in patients presenting with acute abdomen [ 1 ] and the chief indication for emergency cholecystectomy [ 2 , 3 ]  . 
women under the age of 50 years are up to three times more frequently affected by cholecystitis than men whereas after this age , the incidence is the same in both genders . 
the most common cause of cholecystitis is lithiasis with cystic duct obstruction ( 90%95% )  . mucosal hypersecretion due to irritation resulting from increased bile concentration leads to oedema associated with wall thickening , followed by increased intraluminal pressure , wall distension , and stretching of the thin wall vessels with subsequent ischaemia and necrosis of the parietal mucosa . bacterial superinfection , which develops in 50%70% of cases , can lead to complications of acute cholecystitis such as empyema , gangrene , necrosis , and perforation [ 46 ]  . 
a patient without a history of biliary symptoms will rarely develop acute cholecystitis , whereas fewer than 15% of patients with gallstones present symptoms and fewer than 5% develop acute cholecystitis [ 7 ]  . in 5%10% of cases , cholecystitis is non - calculous . 
this situation mainly occurs in patients who have suffered serious injuries or burns , debilitated patients , patients with long - term hospitalisation in icu , or those undergoing prolonged parenteral feeding ; in these patients , systemic shock or the continued use of vasoconstrictors apparently causes ischaemia of the gallbladder wall mucosa , which is characterised by terminal blood supply and insufficient collateral circuits . 
according to another theory , however , non - calculous cholecystitis is due to mechanical obstruction of the cystic duct ( already narrowed by oedematogenic events ) by bile that has become dense and viscous following prolonged biliary stasis [ 8 , 9 ]  . 
other risk factors include overeating , diabetes , sepsis , cardiac arrest , atherosclerosis , aids , and chemotherapy via the hepatic artery [ 10 ]  . because symptoms are non - specific , it is difficult to clinically differentiate biliary colic from acute inflammation , but differential diagnosis is fundamental for establishing the correct therapeutic approach . 
treatment of acute cholecystitis is a matter of debate due to the different therapeutic options : emergency surgery ( laparotomy or laparoscopy ) , or delayed surgery after antibiotic treatment [ 11 , 12 ]  . 
further diagnostic investigation using imaging studies is therefore necessary for early diagnosis and timely treatment , above all when there is a suspicion of complications of acute cholecystitis . ultrasonography ( us ) is usually the first - choice modality [ 13 ] : the association of hepatobiliary us alone with clinical assessment allows accurate diagnosis in the majority of cases of calculous cholecystitis thanks to its very high sensitivity in the detection of cholelithiasis ( 95% ) [ 14 ] ; in addition , this examination has a low cost , is reproducible , and allows recognition and exclusion of numerous other causes of abdominal pain . both computed tomography ( ct ) and magnetic resonance il sospetto clinico di colecistite acuta rappresenta uno dei quesiti pi frequentemente sottoposti al radiologo in urgenza nonch la quarta causa di ricovero ospedaliero per pazienti che si presentano con addome acuto [ 1 ] ed la principale indicazione alla colecistectomia eseguita in urgenza [ 2 , 3 ]  . al di sotto dei 50 anni le donne sono fino a 3 volte pi colpite degli uomini , mentre oltre tale et lincidenza uguale nei due sessi . 
lipersecrezione mucosa determinata da fenomeni irritativi per iperconcentrazione della bile alla base del conseguente edema con ispessimento delle pareti , cui segue laumento della pressione intraluminale e la distensione delle pareti , con stiramento dei sottili vasi parietali , fenomeni alla base della successiva ischemia e poi della necrosi della mucosa parietale ; la sovrainfezione batterica , che si verifica solo nel 50%70% dei casi , invece causa delle possibili complicanze della colecistite acuta quali lempiema , la gangrena , la necrosi e la perforazione [ 46 ]  . 
raro che un paziente senza storia di sintomatologia biliare possa sviluppare una colecistite acuta , mentre al contrario meno del 15% dei pazienti con colelitiasi presentano sintomi clinici e meno del 5% sviluppano una colecistite acuta [ 7 ]  . nel 5%10% dei casi la colecistite invece alitiasica . questa evenienza si verifica essenzialmente in pazienti che hanno subito gravi traumi , defedati , ustionati , ricoverati a lungo in reparti di rianimazione o con alimentazione per via parenterale protratta nel tempo , nei quali lo shock sistemico o luso prolungato di vaso - costrittori indurrebbero unischemia della mucosa parietale della colecisti , che possiede una irrorazione di tipo terminale , con scarsi circoli collaterali ; tuttavia , secondo unaltra teoria le colecistiti alitiasiche sarebbero causate dallostruzione meccanica del dotto cistico ( gi ridotto di calibro per fenomeni edemigeni ) da parte di bile divenuta densa e vischiosa in seguito a prolungata stasi biliare [ 8 , 9 ]  . 
altri fattori di rischio includono liperalimentazione , il diabete , la sepsi , larresto cardiaco , laterosclerosi , laids e la chemioterapia attraverso larteria epatica [ 10 ]  . a causa dellaspecificit dei sintomi difficile differenziare clinicamente una colica biliare da una infiammazione acuta , ma la diagnosi differenziale fondamentale per una corretta pianificazione terapeutica . 
il trattamento delle colecistiti acute oggetto di discussione in quanto esistono differenti opzioni terapeutiche : lintervento chirurgico ( per via laparotomica o laparoscopica ) eseguito in urgenza o differito dopo terapia antibiotica [ 11 , 12 ]  . 
pertanto , specie quando si sospettino le complicanze della colecistite acuta , al fine di una precoce diagnosi e di un tempestivo trattamento terapeutico , si impone la necessit di approfondimenti diagnostici con esami strumentali . generalmente lecografia lindagine strumentale di prima istanza [ 13 ] : associando la sola ecografia epato - biliare alla valutazione clinica possibile una diagnosi accurata nella maggior parte dei casi , specie se la colecistite su base litiasica , grazie alla elevatissima sensibilit di questa metodica nel rilievo di colelitiasi ( 95% ) [ 14 ] ; inoltre tale esame presenta un basso costo , riproducibile e permette il riconoscimento e lesclusione di numerose altre cause di dolore m . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis ( mr ) normally add a small amount of information to the evaluation of acute cholecystitis but can be very useful in the case of subacute manifestations , in the presence of palpable pseudo - masses in the right hypochondrium , of clinical us discrepancy , and in the case of complications such as empyemic cholecystitis , abscesses , emphysematous cholecystitis , necrotic - gangrenous cholecystitis , perforation , biliary - enteric fistula or biliary ileus [ 2 , 6 , 7 , 15 , 16 ]  . the aim of this study was to review cases seen over 1 year of complicated acute cholecystitis evaluated by emergency us and ct and treated with emergency surgery in order to recognise specific and non - specific signs of complication and compare them with those reported in the literature . another aim was to define a correct diagnostic protocol involving the use of ct in selected cases . materials and methods in this study , we retrospectively examined the cases of 35 patients ( 12 women and 23 men ) aged between 27 and 99 years ( mean age 66.6 years ) suffering from acute cholecystitis who underwent imaging examinations between april 2003 and april 2004 . all patients underwent surgery and histological examination was considered the gold standard . 
patients whose diagnostic examinations performed at other sites were not available , patients who did not undergo emergency surgery due to medical contraindications , and patients whose operation was delayed for more than 48 h after presentation were excluded . clinical signs ( pain , murphys sign , fever , palpable swelling , jaundice ) and laboratory signs ( neutrophilic leukocytosis , bilirubinaemia , transaminasemia , glycaemia ) at the time of diagnosis were considered . 
ct spiral examinations ( siemens somatom plus 4 , erlangen , germany ) were performed before and after iv injection of contrast agent , with scans during the venous phase ( 60to 70 - s delay ) without oral contrast agent . 
in one case , ct was performed without iv injection of contrast agent due to reported allergy to iodinated contrast agents . the parameters analysed in ultrasonographic examinations were the following : focal or diffuse wall thickening ( more than 3 mm ) ; stratification or double parietal profile ; distension ( maximum transverse diameter greater than 5 cm ) ; stones in the gallbladder or biliary tract ; sludge or endoluminal aggregates ; parietal , endoluminal or extra - parietal gas collections ; aerobilia ; free or sacculated pericholecystic or abdominal fluid collections ; intraand extra - hepatic biliary tract dilatation ; presence of ultrasonographic murphys sign ; and possible associated findings . 
difficulty or inability to recognise the gallbladder was also evaluated . ultrasonographic signs were divided into three groups : major criteria of simple acute cholecystitis ( msac ) , minor criaddominale . sia la tc che la rm generalmente aggiungono un numero esiguo di informazioni alla valutazione delle colecistiti acute , ma possono essere molto utili in caso di manifestazioni subacute , in presenza di pseudomasse palpabili in ipocondrio destro , in caso di discrepanza clinico - ecografica e nei casi di complicazioni quali la colecistite empiematosa , lascessualizzazione , la colecistite enfisematosa , la colecistite necrotico - gangrenosa , la perforazione , la fistola bilioenterica o lileo biliare [ 2 , 6 , 7 , 15 , 16 ]  . questo studio si propone di esaminare i casi di colecistite acuta complicata , valutati in urgenza con ecografia e tc e sottoposti ad intervento chirurgico in urgenza nel corso di un anno , al fine di riconoscere i segni specifici ed aspecifici di complicanza da noi riscontrati e confrontarli con una revisione della letteratura . 
ci proponiamo inoltre di definire un corretto iter diagnostico che preveda limpiego della tc in casi selezionati . materiali e metodi in questo studio sono stati esaminati retrospettivamente 35 pazienti ( 12 donne e 23 uomini ) di et compresa tra 27 e 99 anni ( et media 66 , 6 anni ) affetti da patologia acuta della colecisti e sottoposti ad esami strumentali nel periodo compreso tra laprile 2003 e laprile 2004 . 
sono stati pertanto esclusi i casi in cui non sono risultati disponibili gli esami diagnostici eseguiti in altre sedi , i pazienti non sottoposti ad intervento chirurgico in urgenza per controindicazioni mediche e quelli il cui intervento chirurgico stato differito oltre le 48 ore dalla diagnosi . sono stati considerati i segni clinici ( dolore , manovra di murphy , febbre , tumefazione palpabile e ittero ) e laboratoristici ( leucocitosi neutrofila , bilirubinemia , transaminasemia , glicemia ) al momento della diagnosi . 
per gli esami ecografici sono state utilizzate due differenti apparecchiature ( au5 esaote , italia e logiq 400 , ge medical system , milwaukee , wi , usa ) con sonda convex da 3 , 55 mhz . 
per riferita allergia al mdc iodato . i parametri analizzati negli esami ecografici sono stati i seguenti : ispessimento parietale diffuso o focale ( considerando ispessita la parete quando superiore a 3 mm ) , stratificazione o doppio contorno parietale , sovradistensione ( diametro traverso massimo maggiore di 5 cm ) , calcoli nella colecisti o nelle vie biliari , presenza di sedimenti o aggregati endoluminali , raccolte gassose parietali , endoluminali o extraparietali , aerobilia , raccolte fluide pericolecistiche o endo - addominali libere o saccate , dilatazione delle vie biliari intraed extra - epatiche , presenza di segno di murphy ecografico ed eventuali reperti associati . 
msac , major criteria of simple acute cholecystitis ; msac , minor criteria of simple acute cholecystitis ; cc , complication criteria msac msac wall thickening > 3 mm wall stratification overdistension > 5 cm ultrasonographic murphys sign biliary sludge or stones biliary tract dilatation calculous cholecystitis biliary lithiasis pericholecystic or abdominal fluid collections parietal , endoluminal or extraparietal gas collections aerobilia difficult or missed recognition of the gallbladder tabella 1 segni ecografici di colecistite . 
mcas , criteri maggiori di colecistite acuta semplice ; mcas , criteri minori di colecistite acuta semplice ; cc , criteri di complicanza mcas mcas ispessimento parietale > 3 mm stratificazione parietale sovradistensione > 5 cm murphy ecografico sedimenti o aggregati biliari dilatazione delle vie biliari litiasi della colecisti litiasi delle vie biliari raccolte fluide pericolecistiche o endoaddominali raccolte gassose parietali , endoluminali o extraparietali aerobilia difficile o mancato riconoscimento della colecisti teria of simple acute cholecystitis ( msac ) , and complication criteria ( cc ) ( table 1 )  . 
for ct in addition to the us parameters , with the exception of murphys sign , we evaluated the presence of free air and alterations to vascularisation of the liver parenchyma adjacent to the gallbladder , both being signs of complication . 
the final histological examinations , considered as the gold standard , were compared with us and ct results , and accuracy , sensitivity , specificity , ppv , and npv for each modality were measured . 
the association with neutrophilia was observed in 28 / 35 ( 80% ) of cases ; in 11 / 35 cases , patients had elevated bilirubinaemia ( 31.4% ) and in 9 / 35 cases increased transaminases ( 25.7% ) ; 21 / 35 patients ( 60% ) had hyperglycaemia on admission , and four of them had a history of diabetes mellitus . 
in the selected group , hepatobiliary us was performed as the first - choice diagnostic examination in 30 / 35 patients , followed by ct in seven cases ; in five cases presenting with acute abdomen , ct was performed as the first - choice examination . 
on the whole , 30 patients were studied with us and 12 by ct ; in 7 / 35 cases , both us and ct were performed . us findings us revealed diffuse thickening of the gallbladder wall in gni ecografici sono stati inoltre suddivisi in tre gruppi : criteri maggiori di colecistite acuta semplice ( mcas ) , criteri minori di colecistite acuta semplice ( mcas ) e criteri di complicanza ( cc ) ( tabella 1 )  . 
per la tc oltre agli stessi parametri utilizzati per lecografia , fatta eccezione per il segno di murphy ecografico , stata valutata la presenza di aria libera e le alterazioni della vascolarizzazione del parenchima epatico adiacente alla colecisti , entrambi segni di complicazione . in base ai reperti riscontrati negli esami diagnostici sono stati distinti due gruppi di patologie : colecistiti acute semplici e colecistiti acute complicate . 
gli esami istologici definitivi , considerati il gold standard , sono stati confrontati con i risultati degli esami ecografici e tc e sono state misurate accuratezza , sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) delle rispettive metodiche . 
nei casi sottoposti sia ad ecografia che a tc stata inoltre valutata la concordanza tra le due metodiche e lentit dei dati aggiuntivi forniti da una metodica rispetto allaltra . risultati i pazienti presentavano clinicamente dolore in ipocondrio destro o epigastrio in 32 / 35 casi ( 91 , 4% ) , manovra di murphy positiva in 22 / 35 casi ( 62 , 8% ) , febbre in 18 / 35 casi ( 51 , 4% ) , tumefazione palpabile in 6 / 35 casi ( 17 , 1% ) , ittero in 2 / 35 casi ( 5 , 7% )  . 
si associava leucocitosi neutrofila in 28 / 35 casi ( 80% ) ; in 11 / 35 casi i pazienti presentavano un innalzamento dei valori di bilirubinemia ( 31 , 4% ) e in 9 / 35 casi si rilevava un incremento dei valori delle transaminasi ( 25 , 7% ) ; 21 / 35 pazienti ( 60% ) avevano iperglicemia al momento del ricovero e 4 di questi pazienti presentavano storia di diabete mellito . 
nel gruppo selezionato , lecografia epatobiliare stata eseguita come primo esame diagnostico in 30 / 35 pazienti , seguita dalla tc in 7 casi ; in 5 casi la tc stata eseguita come esame di prima istanza , trattandosi di gravi quadri di addome acuto . 
ct also revealed three cases of acute pancreatitis ( 25% ) characterised by pancreatic enlargement , with peripancreatic fat tissue hyperdensity in two of these cases . in one patient with suspected thoracic aortic dissection , the detection of cholecystitis was an occasional finding revealed by ct . 
ct allowed the detection of three cases of simple acute cholecystitis and nine cases of complicated acute cholecystitis ( table 2 )  . surgical treatment and histology all patients underwent laparotomic or laparoscopic cholecystectomy within 2448 h of diagnosis . 
in addition to cholecystectomy , the following procedures were performed : three viscerolyses , two hepatic resections , one intestinal resection , one abdominoplasty for laparocele , one umbilical hernial repair , one peritoneal lavage , three abdominal collection drainages , one main biliary tract drainage , one duodenal fistula repair , and one choledochoplasty with kehr tube positioning . 
la tc ha inoltre individuato 3 casi di pancreatite acuta ( 25% ) caratterizzata da aumento volumetrico del pancreas con iperdensit del tessuto adiposo peripancreatico in 2 di questi casi . in un paziente con sospetta dissecazione dellaorta toracica il riscontro di colecistite stato un reperto occasionale rilevato allesame tc . 
la tc ha permesso di distinguere 3 casi di colecistite acuta semplice e 9 casi di colecistite acuta complicata ( tabella 2 )  . interventi chirurgici ed istologia tutti i pazienti sono stati sottoposti a colecistectomia per via laparotomica o laparoscopica nelle 2448 ore successive alla diagnosi . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis table 2 comparison between ultrasonography ( us ) , computed tomography ( ct ) , and histological findings * acute and recurrent cholecystitis are included in the group of simple cholecystitis tabella 2 confronto tra i risultati dellecografia , della tc e dellesame istologico simple cholecystitis * complicated cholecystitis neoplasms colecistiti semplici * colecistiti complicate neoplasie 24 / 30 ( 80% ) 6 / 30 ( 20% ) ecografia 24 / 30 ( 80% ) 6 / 30 ( 20% ) * il gruppo di colecistiti semplici comprende le acute e le croniche riacutizzate table 3 ultrasonographic signs in simple cholecystitis 3 / 12 ( 25% ) 9 / 12 ( 75% ) 3 / 12 ( 25% ) 9 / 12 ( 75% ) histology 14 / 35 ( 40% ) 20 / 35 ( 57.1% ) 1 / 35 ( 2.8% ) istologia 14 / 35 ( 40% ) 20 / 35 ( 57 , 1% ) 1 / 35 ( 2 , 8% ) patient thickening stratification distension murphys sign sludge biliary tract dilatation lithiasis tabella 3 segni ecografici riscontrati nelle colecistiti non complicate paziente ispessimento stratificazione sovradistensione murphy sedimenti dilatazione vvbb litiasi three cases of acute calculous cholecystitis ; 11 cases of recurrent chronic cholecystitis ( with inflammatory infiltrates associated with fibrosis ) , ten of which were calculous and one non - calculous ; and 20 complicated cases of cholecystitis ( 14 calculous and six non - calculous )  . 
the final histological examination revealed one case of undifferentiated carcinoma epatiche , 1 resezione intestinale , 1 addominoplastica per laparocele , 1 riduzione di ernia ombelicale , 1 lavaggio peritoneale , 3 drenaggi di raccolte addominali , 1 drenaggio della via biliare principale , 1 sutura di fistola duodenale e 1 coledoco - plastica con posizionamento di tubo di kehr . 
of the 20 complicated forms , histology diagnosed 13 cases of phlegmonous cholecystitis , two cases of empyema , two cases of necrotic and gangrenous cholecystitis , two cases of abscess , and one case of duodeno - cholecystic fistula . 
us had a sensitivity of 37.5% , a specificitable 4 ultrasonographic signs in complicated acute cholecystitis colecistite acuta litiasica , 11 casi di colecistite cronica riacutizzata ( con infiltrati flogistici associati a fibrosi ) , 10 delle quali su base litiasica e 1 alitiasica , 20 colecistiti complicate ( 14 litiasiche e 6 alitiasiche )  . in 1 caso lesame istologico definitivo ha dimostrato la presenza di un carcinoma indifferenziato della colecisti associato a litiasi . 
delle 20 forme complicate 13 sono risultate allesame istologico come colecistiti flemmonose , 2 casi di empiema , 2 casi di colecistite acuta necrotica e gangrenosa , 2 casi di ascesso e 1 caso di fistola colecisto - duodenale . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis ty of 70% , an accuracy of 66.6% , a ppv of 100% , and an npv of 58.3%. 
in the seven cases studied by both modalities , us and ct yielded similar results as regards the presence of complications ; however , ct provided additional information compared with us , as it detected the presence of fluid in four cases , identified the gallbladder in two cases in which it was not recognizable by us , and demonstrated the presence of intraparietal air in one case , endoluminal air in three cases and free air in one case . 
it also demonstrated biliary tract dilatation in two cases , a biliary - enteric fistula in one case , and intrahepatic fluid and gas due to cholecystitis in one case . 
unlike us , ct also permitted identification of three cases of oedematous pancreatitis . discussion considering that more than 20% of cases clinically classified as cholecystitis correspond to other diseases , the role of emergency diagnostic imaging is to support the clinical diagnosis of acute cholecystitis and to identify the complications of cholecystitis , thus indicating the correct therapeutic approach [ 7 ]  . 
in cases of simple cholecystitis , surgical treatment is normally delayed , and the patient is treated with antibiotics during the acute phase ; emergency surgery within 2448 h , however , prevents the formation of adhesions , which may complicate laparoscopic surgery and increase the rate of conversion into laparotomy [ 12 , 17 , 18 ]  . 
emergency surgery , especially when laparoscopic , therefore implies shorted hospitalisation and reduced post - operative complications and overall hospitalisation costs [ 11 , 12 , 17 , 1824 ]  . clinically , three quarters of patients suffering from acute cholecystitis have a history of biliary colic and pain in the right hypochondrium , which may irradiate to the right shoulder and to the epigastric region , accompanied by nausea , vomiting , and dyspepsia . 
con la tc sono stati identificati 3 vn , 9 vp , nessun fp e nessun fn . lecografia ha dimostrato una sensibilit del 37 , 5% , una specificit del 70% , una accuratezza del 66 , 6% , un vpp del 100% e un vpn del 58 , 3% . 
la tc ha invece presentato una sensibilit del 100% , una specificit del 100% , una accuratezza del 100% ( tabella 5 )  . nei 7 casi sottoposti sia ad ecografia che a tc le due metodiche sono risultate concordi per la presenza di complicanze , ma la tc ha fornito in ogni caso maggiori informazioni rispetto allecografia rilevando la presenza di versamento fluido in 4 casi , identificando la colecisti in 2 casi in cui allecografia non era riconoscibile , diagnosticando la presenza di aria intraparietale in 1 caso , endoluminale in 3 casi , di aria libera in 1 caso , ha mostrato la presenza di dilatazione delle vie biliari in 2 casi , la fistola bilio - enterica in 1 caso , la presenza di raccolta fluido - gassosa intraepatica ad origine dalla colecisti in 1 caso . 
la tc ha inoltre consentito rispetto allecografia lidentificazione di 3 casi di pancreatite edematosa . discussione il ruolo della diagnostica per immagini in emergenza nella patologia acuta della colecisti quello di supportare la diagnosi clinica , considerando che oltre il 20% dei casi classificati clinicamente come colecistite corrispondono a unaltra patologia , e di identificare le complicanze indicando il corretto approccio terapeutico [ 7 ]  . 
generalmente se la colecistite non risulta complicata , il trattamento chirurgico viene differito , sottoponendo il paziente in fase acuta a terapia antibiotica ; tuttavia , lintervento chirurgico in emergenza entro 2448 ore previene la formazione di aderenze che possono complicare lintervento chirurgico laparoscopico aumentandone la percentuale di conversione in laparotomia [ 12 , 17 , 18 ]  . 
in our study , fewer patients underwent ct than us , and the majority of them had complicated cholecystitis suspected at us or on the basis of clinical findings ; therefore , it was not possible to accurately assess the major and minor criteria using ct in simple cholecystitis . forty percent of patients with acute cholecystitis develop complications such as empyema , pericholecystic abscesses , necrotic - gangrenous cholecystitis , emphysematous cholecystitis , haemorrhagic cholecystitis , perforation , cholecysticenteric fistula , and biliary ileus [ 3638 ]  . 
 we also detected one case of duodeno - cholecystic fistula . in this case , the gallbladder was not recognisable at us whereas both aerobilia and a coarse calcification ( 3 cm ) between the liver and the pancreatic head were well visible in the second duodenal portion ; also , ct had some difficulties in that the stone could not be precisely localised in the intestinal lumen , and neither free air or endoperitoneal fluid collection could be seen . 
however , the presence of aerobilia guito in laparoscopia , comporta riduzione dei tempi di ospedalizzazione , delle complicanze post - operatorie e dei costi complessivi del ricovero [ 11 , 12 , 17 , 1824 ]  . clinicamente tre quarti dei pazienti affetti da colecistite acuta presentano una storia di coliche biliari , dolore in ipocondrio destro , che si pu irradiare alla spalla destra ed in sede epigastrica , accompagnato da nausea , vomito e dispepsia . 
il segno di murphy generalmente positivo e vi possono essere reperti di laboratorio aspecifici ( leucocitosi , iperbilirubinemia , iperamilasemia e aumento dei livelli di transaminasi ) [ 25 , 26 ]  . 
nel nostro studio i pazienti sottoposti a tc sono stati in numero ridotto rispetto ai casi sottoposti ad ecografia ed erano quasi tutti casi di colecistiti complicate sospettate allesame ecografico o in base al quadro clinico , pertanto non stato possibile valutare con accuratezza i criteri maggiori e minori con tale metodica nelle colecistiti semplici . 
nel 40% dei pazienti con colecistite acuta si sviluppano complicanze quali lempiema , gli ascessi pericolecistici , la colecistite necrotico - gangrenosa , la colecistite enfisematosa , la colecistite emorragica , la perforazione , la fistola colecisto - enterica e lileo bilare [ 3638 ]  . 
de vargas macciucca et al . : ultrasonographic and spiral ct evaluation of simple and complicated acute cholecystitis and inability to identify the gallbladder , perforated and collapsed , correctly prompted towards emergency surgery during which and a duodeno - cholecystic fistula with a stone impacted in the second duodenal portion was detected . 
in our study , no cases of haemorrhagic cholecystitis or biliary ileus were observed . the fundamental aim of diagnostic imaging , especially in emergency settings , is to differentiate simple and complicated cholecystitis in order to plan laparoscopic or laparotomic surgery within 48 h . 
to detect the complicated forms , we suggest a classification that takes into account the main us signs divided into major criteria ( wall thickening > 3 mm , wall stratification , positive sonographic murphys sign , and distension ) , minor criteria ( biliary sludge , calculous cholecystitis and biliary tract dilatation ) and criteria for complicated forms ( aerobilia , fluid and gas collections , or missed recognition of the gallbladder ) ( table 1 )  . 
this classification differs from mirviss classification [ 9 ] ( table 6 ) first of all because it takes into consideration sonographic criteria but also because the presence of stones and biliary sludge is considered a minor criteria ; this depends on the fact that , despite being a frequent sonographic finding , biliary sludge is not specific for cholecystitis . 
the analysis of associations between major and minor signs , on the other hand , did not show a significant difference between the two groups of simple and complicated cholecystitis . 
indeed , in 5 / 16 cases ( 31.2% ) of complicated cholecystitis and in 10 / 14 cases ( 71.4% ) of simple cholecystitis , an association of at least two major criteria and one minor was found . 
in 4 / 16 cases ( 25% ) of complicated cholecystitis and in 4 / 14 cases ( 28.5% ) of simtable 6 computed tomography ( ct ) signs of acute cholecystitis ( mirviss classification ) ct signs of acute cholecystitis [ mirvis et al . 
in questo caso allesame ecografico non risultava riconoscibile la colecisti , mentre erano ben evidenti sia laerobilia che la presenza di una struttura calcifica grossolana ( 3 cm ) situata tra il fegato e la porzione cefalica pancreatica , nella sede della seconda porzione duodenale ; anche la tc ha presentato alcune difficolt diagnostiche in quanto la formazione litiasica non risultava localizzabile con certezza nel lume intestinale e non erano visibili aria libera n versamento fluido endoperitoneale ; tuttavia la presenza di aerobilia e il mancato riconoscimento della colecisti , in quanto perforata e collassata , hanno indirizzato correttamente la paziente al trattamento chirurgico urgente ed stata riscontrata una fistola colecisto - duodenale con calcolo indovato a livello della seconda porzione duodenale . 
nella nostra casistica non sono stati riscontrati casi di colecistite emorragica n di ileo biliare . lobiettivo fondamentale che si propone la diagnostica per immagini soprattutto in emergenza quello di distinguere le colecistopatie semplici dalle complicate al fine di poter programmare lintervento chirurgico per via laporoscopica o laparotomica , entro le 48 ore . 
a tal fine per poter individuare le forme complicate proponiamo una classificazione che tiene conto dei principali segni ecografici suddivisi in criteri maggiori ( ispessimento parietale > 3 mm , aspetto stratificato della parete , segno ecografico di murphy positivo e sovradistensione ) , criteri miniori ( sedimenti biliari , litiasi della colecisti o delle vie biliari e dilatazione delle vie biliari ) e criteri riconducibili a forme complicate ( areobilia , raccolte fluide , raccolte gassose o mancato riconoscimento della colecisti ) ( tabella 1 )  . 
una classificazione basata su tali criteri differisce da quella di mirvis riportata in letteratura [ 9 ] ( tabella 6 ) , innanzitutto perch prende in considerazione dei criteri ecografici , ma anche perch la presenza di calcoli e sedimenti biliari considerata un criterio minore poich , sebbene con tale metodica sia molto frequentemente riscontrata , non specifica di colecistite : nel nostro studio calcoli e aggregati biliari erano presenti quasi sempre ( 98% della popolazione esaminata ) sia nelle forme complicate che in quelle semplici . nella nostra esperienza lecografia ha riscontrato segni sicuri di complicanza in 6 / 16 casi ( 37 , 5% )  . 
tra le colecistiti semplici i segni di complicazione non sono mai stati rilevati . lanalisi delle associazioni tra segni maggiori e minori invece non ha dimostrato una significativa differenza tra i due gruppi di colecistiti , semplici e complicate . 
infatti in 5 / 16 casi ( 31 , 2% ) di colecistite complicata e in 10 / 14 casi ( 71 , 4% ) di colecistite semplice stata riscontrata lassociazione di almeno 2 criteri maggiori e uno minore . 
in 4 / 16 casi ( 25% ) di colecistite complicata e in 4 / 14 casi ( 28 , 5% ) di colecistite semplice erano presenti allecografia meno di due criteri maggiori . 
 these data indicate that us can distinguish complicated and simple cholecystitis only in the presence of definite signs of complication ; in the majority of cases , however , these signs are not present . 
we believe that ct would have provided the correct diagnosis of complication in many of these cases given its higher accuracy and sensitivity . indeed , ct yielded no fp or fn results . 
because the majority of complications revealed by us showed at least two major criteria associated with at least one minor criterion or at least one criterion for complication ( overall 68.7% ) , further ct investigation after us is justified under these circumstances . numerous cases of phlegmonous cholecystitis were present ( 9 / 16 cases ) among the cases assessed as simple cholecystitis by us and as complicated cholecystitis by histological examination . although this form is not regarded as a complicated form in the literature , we decided to include these cases in the group of complications because involvement of the entire thickness of the organ causes serositis with peritoneal effusion in the majority of cases . 
if the emergency approach is based on medical treatment with delayed surgery , the peritoneal reaction may lead to the formation of synechia and fibrosis , with development of adhesions . 
phlegmonous cholecystitis therefore requires immediate surgical treatment because adhesions hinder possible surgical treatment during quiescence and increase the incidence of complications ; there is also a higher risk of laparoscopy being converted into laparotomy [ 12 ]  . conclusions assessment of acute cholecystitis in an emergency department requires careful analysis of the clinical findings and relies on us as first - choice examination . us allows the recognition of signs which , taken singularly , are poorly specific ; this directs the patient to further investigation by ct , which is indispensable for the complete recognition and evaluation of complicated forms . 
trenta , radiologists at the emergency department of policlinico umberto i , rome , for their help in collecting the case series . solo in presenza di segni certi di complicanza , ma nella maggior parte dei casi questi non sono presenti ; infatti , nella nostra casistica , allecografia sono risultati falsi negativi ( fn ) un terzo dei casi e la maggior parte di tali pazienti non stata sottoposta ad ulteriori indagini . 
poich allecografia la maggior parte delle complicanze presentavano almeno due criteri maggiori associati ad almeno uno minore oppure almeno un criterio di complicanza ( globalmente il 68 , 7% ) , si pu considerare giustificato in tali circostanze approfondire lesame ecografico con un esame tc . 
sebbene la letteratura non tratti questa forma come complicata , abbiamo ritenuto di includere tali casi nel gruppo delle complicazioni in quanto linteressamento a tutto spessore del viscere determina comunque una sierosite con presenza nella maggior parte dei casi di versamento peritoneale . 
in tali pazienti , se la scelta terapeutica in urgenza il trattamento medico e lintervento chirurgico viene differito , la reazione peritoneale nel tempo pu determinare la formazione di sinechie e fibrosi con lo sviluppo di briglie aderenziali . 
le colecistiti flemmonose necessitano pertanto di un trattamento chirurgico immediato , in quanto le aderenze rendono leventuale intervento in fase di quiescenza pi difficoltoso e aumentano lincidenza di complicanze ; in questi casi inoltre pi elevato il rischio di conversione dellintervento da laparoscopico a laparotomico [ 12 ]  . conclusioni la valutazione in un dipartimento di emergenza della patologia acuta della colecisti necessita di una attenta analisi dei dati clinici e si avvale dellutilizzo dellecografia come metodica di prima istanza . 
lecografia permette il riconoscimento di alcuni segni che sono poco specifici singolarmente , indirizzando il paziente allapprofondimento con tc che risulta indispensabile per riconoscere e valutare in maniera completa le forme complicate . 
in particolare , quando allecografia sono identificati almeno due segni maggiori e uno minore e quando sono presenti i segni specifici di complicanza , lapprofondimento con tc imprescindibile in quanto permette di selezionare i pazienti candidati ad intervento in urgenza rispetto a quelli da trattare con terapia antibiotica ed intervento differito ; inoltre la distinzione tra le diverse forme di colecistite aiuta il chirurgo nella scelta della tecnica operatoria pi indicata ( laparoscopica o laparotomica )  . ringraziamenti si ringraziano per la collaborazione nel reperimento della casistica il dott . 
inches2 1dipartimento di scienze oncologiche e chirurgiche , sezione di senologia , universit degli studi di padova , via gattamelata 64 , i - 35128 padova , italy 2dipartimento di scienze medicodiagnostiche e terapie speciali , universit degli studi di padova , via giustiniani 2 , i - 35128 padova , italy correspondence to : l . 
practical aspects with psychological and clinical involvement are discussed with tree diagrams . key words human error perception interpretation system riassunto viene proposto un approccio sistematico allerrore umano nella diagnostica per immagini ( di ) , riconoscendo la sua collocazione nelle attivit personali della percezione e della interpretazione e nelloperativit globale del sistema . 
nellinquadramento che si sviluppa secondo ramificazioni ad albero sono discussi gli aspetti pratici alla luce di contributi provenienti dagli studi psicologici e dalla evoluzione della realt clinica e sanitaria . parole chiave errore umano percezione interpretazione sistema introduction introduzione the approach to the study of human error in diagnostic imaging ( di ) requires a preliminary introduction regarding the concept of error in modern medicine . human error is always placed inevitably in relation with truth [ 1 , 2 ] , which in a strictly scientific field should be considered , as the epistemologist blandino states , as only probable and approximate , connected to theories which change and at times crumble , to be replaced by other , more valid ones . 
it can safely be said that there is currently such a huge quantity of knowledge in medicine and biology that the medical practitioner is increasingly exposed to a great number and variety of errors . traditionally two relevant aspects have been indicated : errors in medicine , considered as the collection of theories regarding health and the state of disease in humans ; for the scientific representation of errors in medicine the statistics and theory of bayes [ 3 ] are used medical practitioners errors , in that as humans . 
they are subject to making mistakes according to a distinction made by epistemologists , the term mistake is more accurate for errors related to the activity in which theoretical notions are applied whereas errors in the lapproccio allo studio degli errori commessi dalluomo nella diagnostica per immagini ( di ) impone una preliminare introduzione sulle connotazioni che il concetto di errore assume nella moderna attivit medica . lerrore da sempre messo inevitabilmente in rapporto con la verit [ 1 , 2 ] che in ambito strettamente scientifico da intendersi , come indica lepistemologo blandino , come soltanto probabile e approssimata , connessa a teorie che si modificano e talora crollano , sostituite da altre pi valide : anche le verit diagnostiche sono quindi relative e commisurate al sapere di un determinato tempo . 
non vi dubbio che allo stato attuale via sia una tale mole di conoscenze in medicina e biologia che si pu tranquillamente affermare che loperato del medico sempre pi esposto ad errori , molteplici e di varia natura . tradizionalmente se ne indicano due aspetti rilevanti : gli errori della medicina , considerata come insieme di teorie che riguardano la salute e lo stato di malattia delluomo , per la rappresentazione scientifica dei quali ci si avvale soprattutto della statistica e del teorema di bayes [ 3 ] ; gli errori dei medici , in quanto essere umani e come tali soggetti a sbagliare . secondo una distinzione degli epistemologi , proprio il termistrict sense regard science as such . 
in this paper , the term error will be used for simplicity , even if in reference to mistakes . medical tradition also commonly makes a distinction between two reference errors : cognitive : concerning diagnosis and prognosis operative : concerning decision making and therapy di is slightly removed from this picture , as the use of perception is particularly relevant but also because given the progressive expansion of the discipline , the search for errors needs to be placed in an organized and technologically advanced context , with a much broader range of devices than in the early days of the first applications of the coolidge tube when medicine was almost totally reliant on the personal abilities of the practitioners . like other fields , such as nuclear engineering or aviation [ 4 , 5 ] , a radiology department stands out for its organizational and operative peculiarities as a system , with features similar to any company such as logistics , finance and the hiring and training of personnel . 
some errors may be present in the planning and organizational phase such that reason and rasmussen [ 6 ] classifies them as latent errors with delayed effects and differentiates them from active errors in which there is a momentary and welldefined participation by the operator . 
seeking out these remote errors is an important feature of the modern management of the radiology department because when they appear , the operator is in fact programmed to make a mistake . 
the operator is the victim of a mediocre project , insufficient maintenance , inappropriate materials and managerial decisions which create situations of risk , such as unrealistic workloads , inappropriate training or exasperating turnaround times . 
since the error appears with the last operator , whether he or she is the direct or indirect cause , all errors should be considered human error and in di the radiologists error . in this context the aim of this study was to unify the problems and the causes of errors , taking into consideration the crucial moment of image assessment in radiology when the radiologist utilizes the characteristics of his or her personality , culture and training [ 7 ]  . characteristics of the radiologists activities the radiological act as it currently stands can be defined as a technical - methodological procedure performed on a patient in an organizational and decision - making system , the outcome of which is the image obtained to achieve diagnosis . 
it is here , in fact , that to reach a decision , the radiologist makes use of a process of perception and cognition , features which occur simultaneously and are interdependent , and yet , as wood [ 8 ] notes , are separate mental activities . 
inches : systematic approach to human error in radiology ne sbaglio pi corretto ad indicare gli errori inerenti alle attivit in cui le nozioni teoriche sono applicate , mentre gli errori in senso stretto riguardano la scienza come tale . nellelaborato il termine errore sar usato per comodit e consuetudine , anche se riferito agli sbagli . ancora nella tradizione medica si soliti configurare due errori di riferimento : cognitivo : concerne la diagnosi e la prognosi ; operativo : concerne gli aspetti decisionali e la terapia . la di se ne discosta parzialmente essendo per essa rilevante lapporto della percezione , ma anche perch , nella progressiva espansione della disciplina , la ricerca dellerrore va inquadrata in un contesto organizzato e tecnologicamente avanzato , che prospetta tipologie pi ampie rispetto allepoca artigianale delle prime applicazioni del tubo di cooledge , coeve ad una medicina legata alle pressoch assolute capacit personali dei medici . la radiologia , intesa quale servizio o unit operativa che dir si voglia , analogamente ad altre strutture di lavoro , come lingegneria nucleare o laviazione [ 4 , 5 ] , si identifica allo stato attuale per peculiarit gestionali e operative come sistema , al quale sono attribuiti analogamente a qualsiasi azienda almeno gli ambiti organizzativi della logistica , della finanza , dellassunzione e della preparazione del personale . il sistema come tale pu essere sottoposto ad analisi e verifica ai fini della ricerca degli errori e della loro correzione mediante procedure adatte . alcuni errori possono essere gi insiti in fase di progettazione e organizzazione , tanto che reason [ 6 ] li classifica come errori latenti , con effetti ritardati , differenziandoli dagli errori attivi in cui vi una partecipazione momentanea e bene circostanziata delloperatore . 
la ricerca di questi errori remoti rappresenta allora uno dei punti notevoli della moderna conduzione del reparto , perch , quando compaiono , loperatore in realt stato programmato per sbagliare : egli vittima ultima di un progetto mediocre , di una manutenzione insufficiente , di materiali inidonei , di decisioni della dirigenza che si esplicano in situazioni di rischio , quali ad esempio gli irrealistici carichi di lavoro , laddestramento non adeguato o i tempi di produzione esasperati . 
poich di fatto lerrore si manifesta nelle circostanze con lultimo operatore , ne sia egli la causa diretta o indiretta , tutti gli errori in definitiva debbono essere considerati riferiti alluomo : per la di al radiologo . sotto questo profilo lo scopo del lavoro di unificare problematiche e cause di errore prendendo in considerazione nella di il momento cruciale della valutazione del documento , allorquando il radiologo partecipa mettendo in campo le proprie caratteristiche di personalit , cultura e preparazione [ 7 ]  . caratteristiche dellattivit del radiologo latto radiologico allo stato attuale pu essere definito come procedura tecnico - metodologica condotta sul paziente , avvenuta in un sistema organizzativo - decisionale , che si esprime nel documento dimmagine ottenuto per conseguire il fil . 
inches : systematic approach to human error in radiology mental phenomena at play is required : the phenomenon of perception the perceptual process transforms retinal stimulation at the higher centres into conscious perception , allowing images to be extracted and translated in conscious assessment by simplifying and organizing the information from the peripheral regions . 
according to attneave , quoted by wood [ 8 ] , this process is limited , not being sufficiently capable in the sense of capacity to transmit all information which reaches the retina . 
hake , also cited by wood [ 8 ] , instead believes that perception is governed by the centre in that it is linked to the search for a meaning connecting the fragmentary retinal images . 
in fact , the meaning and even the writing of a sentence itself may be considered absolutely precise even though obvious errors may be found when the text is carefully revised [ 9 ]  . 
lastly , it is worth noting that perception is substantially different from simple vision , in which only the peripheral activities of the observer take part in relation to the nervous system . the phenomenon of cognition the cognitive part of diagnostic decision making is less well known yet fascinating , given the models proposed for explaining the mental stages which lead to a conclusion . 
qui , infatti , che il radiologo si avvale di un procedimento percettivo e conoscitivo , simultanei e interdipendenti , da considerare tuttavia con wood e tuddenham [ 8 ] come attivit psichiche separate , per giungere ad una decisione . 
per rendere comprensibile e al tempo stesso unitaria la classificazione a seconda della tipologia e delle cause di errore indispensabile un richiamo sintetico alle conoscenze dei fenomeni psichici in gioco . il fenomeno della percezione il processo percettivo trasforma in percezione cosciente i modelli della stimolazione retinica ai centri superiori ; consente di estrarre immagini e di tradurle in valutazione conscia , mediante una semplificazione e organizzazione delle informazioni provenienti dalla periferia . 
secondo atteneave , citato da wood [ 8 ] il processo limitato , non essendo sufficientemente capace , nel senso proprio di capiente , per trasmettere tutte le informazioni che raggiungono la retina . hake , pure citato da wood [ 8 ] ritiene invece che la percezione sia diretta dal centro in quanto legata alla ricerca di un significato che colleghi le frammentarie immagini retiniche . 
per la lettura ; i rettangoli indicano le conoscenze che dallalto in basso divengono via via pi profonde ; in un caso clinico linterprete potrebbe trascurare leziologia di un broncogramma , ad esempio metastasi polmonari , se lattivazione particolarmante frequente per le cause infettive . pointed out that classic cognitivism recognizes the diagnostic process as inductive reasoning aimed at identifying rules and categories , beginning with concrete examples : the dialogue between the areas of research of concrete examples ( variable features ) and rules ( fixed features ) leads to the selection of facts , to remembering the theories based on the facts and to test the hypotheses . 
the classic model , however , has the defect , particularly for medical applications , of overlooking the concrete and pragmatic aspects , in essence , situations such as emergencies in which the examinations are necessarily limited owing to time constraints . 
 the most complete and appropriate model for our purposes which explains the relationship between real facts and the examination of the mind is the model proposed by raufaste and eyrolle [ 10 , 11 ] in 1998 . 
long - term memory has an enormous capacity for storage and contains declarative knowledge ( theory ) and procedural knowledge ( know - how ) interconnected by various types of logical systems in an active for for example , the processes of classification of part / whole relations become increasingly rapid in acquisition times as the knowledge is implemented and interconnected . 
generally speaking , by bringing ones attention to a certain level of knowledge , that level is activated , and once more overcoming a certain threshold , awareness is achieved . working memory involves a variety of aspects , including phonological , visual and spatial . 
infine da osservare come la percezione si differenzi in modo sostanziale dalla semplice visione , al cui fenomeno partecipano solo le attivit periferiche dellosservatore in rapporto alle caratteristiche del sistema nervoso . il fenomeno cognitivo la parte cognitiva della decisione diagnostica meno conosciuta , affascinante per i modelli proposti a spiegare le tappe mentali che portano alla conclusione . 
premesso che lambito mentale molto ampio e a margini poco definiti , doveroso accennare come il cognitivismo classico riconosca il procedimento diagnostico come ragionamento induttivo teso ad identificare regole e categorie partendo da esempi concreti : il dialogo fra gli spazi di ricerca degli esempi concreti ( tratti variabili ) e delle regole ( tratti fissi ) conduce a selezionare i fatti , a ricordare le teorie a partire dai fatti e a verificare le ipotesi . 
il modello classico ha per il difetto , soprattutto per le applicazioni mediche , di trascurare gli aspetti concreti e pragmatici , in sostanza le situazioni , ad esempio le emergenze , in cui le indagini sono necessariamente limitate per motivi di tempo . 
per spiegare meglio il rapporto tra fatti reali e lindagine della mente risulta pi completo e adatto alle nostre esigenze , perch dedicato alla radiologia , il modello del francese roufaste del 1998 [ 10 , 11 ]  . 
la memoria a lungo termine ha vasta possibilit di stoccaggio ed duratura nel tempo : contiene le conoscenze dichiarative ( del sapere teorico ) e procedurali ( del saper fare ) interconnesse da diversi tipi di sistemi logici in forma attiva . 
cos ad esempio i processi di classificazione o di relazione parte / tutto divengono sempre pi rapidi nei tempi di acquisizione mano a mano che tali conoscenze sono implementate e interconnesse . 
unlike long - term memory , which is activated autonomously and without the intervention of the conscious , working memory highly depends on the attention system capable of authorizing the implementation of higher functions , such as symbolic calculations or the decision to implement or inhibit automatisms [ 10 , 11 ]  . 
 analysis of radiographs involves the fundamental function of working memory , that is , the maintenance of a representation constructed from empirical data , in our case from the characteristics of the radiographs , and from information recalled from long - term memory , which we could call experience . 
la memoria di lavoro ha apporti differenti , anche fonologici , visivi e spaziali ; permette di stoccare un numero piccolo di informazioni ( da 3 a 7 indipendenti una dallaltra )  . 
la risoluzione di problemi complessi , come quello della valutazione dei radiogrammi , abbisogna di parametri molto pi numerosi : il problema risolto con lassociazione nella memoria di lavoro di pi sottoinsiemi , che sono trattati come singole unit . 
contrariamente alla memoria a lungo termine , che attivata autonomamente e senza lintervento della coscienza , la memoria di lavoro dipende fortemente dal sistema attenzionale in grado di autorizzare la messa in opera di funzioni superiori come il calcolo simbolico , la decisione di una gestione o linibizione degli automatismi [ 10 , 11 ]  . 
ai fini dellosservazione dei radiogrammi interviene la funzione fondamentale della memoria di lavoro ovvero il mantenimento di una rappresentazione , costruita a partire dai dati empirici , nel caso nostro dalle caratteristiche dei radiogrammi , e da informazioni recuperate dalla memoria a lungo termine , che in modo arbitrario , ma di immediata acquisizione potremmo chiamare esperienza . 
knowledge - based activity : the diagnostic process is guided by analytical reasoning , in the awareness of already stored knowledge , to tackle new situations , which require a considerable application effort . human error in diagnostic imaging : types and causes having introduced the areas of human activity where errors may occur , the causes may now be sought in the three major groups of error : ( 1 ) perceptual errors , ( 2 ) cognitive errors and ( 3 ) system errors . 
these are summarised in figure 3 . the scientific principle of assessment is also valid for human error , that is to say , that similar to the bayes formula , errors are either false positives or false negatives . 
la diagnostica orientata da un ragionamento analitico , nella consapevolezza di un bagaglio di conoscenze gi immagazzinate , per far fronte a situazioni nuove , che richiedono quindi uno sforzo applicativo non comune . according to berlin [ 12 ] , 70% of lawsuits brought against radiologists are related to the non - identification of radiological signs , 60% of which are due to perceptual errors . with regard to the causes , a distinction is made between errori umani nella di : tipologie e cause introdotti gli ambiti delle attivit umane in cui avviene lerfig . 
inches : systematic approach to human error in radiology rore , possibile ricercarne le cause nei tre grandi insiemi : ( 1 ) linsieme degli errori percettivi , ( 2 ) linsieme degli errori cognitivi , ( 3 ) linsieme degli errori del sistema . 
per gli errori di sistema o latenti qui ribadito che lerrore umano di ripercussione , essendo la causa antecedente al momento dellavvenimento , gi radicata nel sistema organizzativooperativo . errori percettivi secondo berlin il 70% [ 12 ] delle pratiche legali contro i radiologi connesso ad una non identificazione di segni radiologici , con un contributo del 60% degli errori percettivi . quanto alle cause , si distinguono errori di identificazione con errata attribuzione ed errori di non identificazione . errori di identificazione con errata attribuzione sono errori poco frequenti : si verificano allorquando il radiologo segnala una lesione che non sussiste , scambiando ad esempio un reperto normale con uno patologico . 
barbaum [ 13 ] riporta , ad esempio , che nella ricerca di un corpo estraneo per la presunta ingestione di un bottone da parte di un bimbo di 1 anno in un radiogramma standard del torace , un radiologo ha malamente interpretato un nucleo di ossificazione sternale attribuendolo al bottone . 
le verifiche endoscopiche e il pasto opaco hanno dimostrato linconsistenza dellaffermazione . come gi osservato sono gli errori pi frequenti : il riconoscimento postumo di un nodo polmonare sul radiogramma del torace la situazione pi nota . 
questa possibilit di errore risulta chiara se ci si cimenta con i disegni paradossali di esher o con il libro per bambini di handford the great waldo [ 14 ]  . 
nellultimo libro , i bambini sono sfidati a trovare il mostriciattolo waldo nascosto tra mille disegni : difficile da riconoscere , ma una volta scoperto o rifugiatisi nelle soluzioni , alla fine la sua inconfondibile sagoma e la relativa posizione risultano ovvie . 
nellesempio la percezione fortemente influenzata dalle aspettative ; perci trovare waldo pi semplice che vedere un piccolo nodo polmonare sul radiogramma toracico , perch waldo sicuramente c , mentre per il nodo polmonare non abbiamo indizi . 
 [ 13 ] report an example in the search for a foreign body in a standard chest x - ray due to the presumed ingestion of a button by a 1 - year - old child . 
endoscopic examinations and an opaque bolus proved the affirmation incorrect . non - identification errors these are the most frequent kinds of errors , with the late recognition of a pulmonary node on a chest x - ray being the most common situation . 
the possibility of making this kind of error is clear if one tests oneself with the paradoxical drawings of escher or with the childrens books by handford wheres wally ? [ 14 ]  . 
in one of the most recent books , children are challenged to find wally hidden among hundreds of figures ; he is extremely difficult to recognize , but once identified his , unmistakable outline and his position are in the end obvious . 
in this example , perception is strongly influenced by expectations , so that finding wally is much easier than identifying a small pulmonary nodule on a chest x - ray because wally is definitely there while a pulmonary nodule may or may not be present . 
with regard to errors in this activity , kopans and daniel [ 15 , 16 ] note cases reported by psychologists of the difficulty and frustration of contingent situations often present in daily life , such as the fruitless search for a bunch of keys which we are unable to see but need to get into our house . 
the example can easily be related to a mammographic sign indicated by a colleague or recognized at a later time . specific causes as well as non - describable factors , the erroneous perception that leads to the non - identification on radiographs is connected to specific , numerous and heterogeneous causes . 
indeed , the final error is perceptual , but the complexity of mental behaviour is such that causal factors which are a part of technical and cognitive features play a part . 
with reference to berlin [ 18 ] , in one case of non - identified pulmonary nodule , the judicial assessment commission admitted that the lesion was difficult to diagnose since the x - rays were overexposed , thus suggesting the responsible error . 
the difficulty of diagnosing lesions at the level of the last cervical and first thoracic vertebrae is also well known , particularly in trauma patients , unless an optimal patient position is found . 
berlin [ 18 ] reports the case of a patient who fell from a ladder and underwent radiography of the cervical vertebrae on three separate occasions owing to the persistence of symptoms . 
unfortunately , the lesion identified on a later occasion in another hospital was a fracture / luxation of c6 - c7 , with the patient ending up a permanent quadriplegic . 
inches : systematic approach to human error in radiology screening : in quello mammografico infatti notevole la variabilit anatomica , spesso la struttura di difficile analisi , e il numero di casi da interpretare pu essere enorme . 
per gli errori in questa attivit kopans [ 15 , 16 ] ricorda , su segnalazione degli psicologi , le difficolt e le frustrazioni delle situazioni contingenti spesso presenti nella vita quotidiana , come la ricerca infruttuosa di un mazzo di chiavi , che non siamo in grado di vedere , ma che sono necessarie per entrare in casa . 
lesempio si ricollega con facilit ad un segno mammografico indicato da un altro operatore o riconosciuto in tempi successivi . cause specifiche oltre a fattori non descrivibili , lerrata percezione che porta alla non identificazione sui radiogrammi connessa a cause specifiche , numerose ed eterogenee . 
le tipologie sono indicate in figura 4 . gli errori tecnici [ 17 ] sono bene esemplificati dalla lesione non vista per sovra o sottoesposizione o per errato posizionamento del paziente . 
con riferimento a berlin [ 18 ] , in un caso di nodulo polmonare non visto , la commissione di valutazione giudiziaria ammise che era difficile diagnosticare la lesione perch le radiografie erano sottoesposte , sottintendendo cos lerrore responsabile . 
sempre berlin riporta il caso di un paziente , caduto dalle scale di casa e sottoposto a radiografie della colonna cervicale in tre fasi diverse , a causa di una persistente sintomatologia : il primo esame identific le prime 4 vertebre cervicali , il secondo dimostr anche c5 con sole note artrosiche . 
the anomalies outside the privileged area of the examination are not infrequent and include thoracic lesions identified during an abdominal examination ; or pleural , pulmonary or mediastinal lesions incidentally encountered during a radiological study of the spine , thoracic bones or shoulder girdle . 
in a litigation caused by lack of identification of an arteriovenous malformation of the bone marrow , berlin [ 19 ] underlines the difficulty of establishing whether the error was due to non - perception or lack of knowledge by the radiologist , and such difficulties can be extended to other cases . the attempt to explain non - identification with other causes dates back to the 1960s and the work of several authors , such as smith and tuddenham , which was later commented by wood , and raufaste and eyrolle [ 8 , 10 , 11 ] : several lesions were not identified owing to another lesion present in the image which had caught the attention of the radiologist . 
following the same line of research , berbaum [ 20 ] investigated the phenomenon on his own colleagues , introducing an artificial nodular lesion in chest x - rays already marked by original lesions . 
he defined this perceptual error satisfaction of search , thus recognizing the argument of cognitive psychologists who note that radiologists tend to be satisfied after finding a lesion , and if they continue the assessment of the image , it is only to restrict the field of study to what they have identified . the quantity of perceptual errors varies according to the examination in question . 
 [ 21 ] , in an interval of 16to 40 - mm nodules , recognized a minimum error of 20% ! in a specific study on the efficiency of health services , watcher et al . 
 [ 22 ] reports similar types of errors in other organs and systems recognized by other researchers : the errors in emergency situations have a low percentage of 3%6% ( robin ) , the sensitivity of identifying ureteral stones , many of which are recognizable a posteriori , is 46% ( levine ) and the error rate in contrast enema is 15% ( wesses )  . a first critical examination of perceptual errors , in the light of case series and studies which go beyond the individual case with legal implications , demonstrates that the real difficulty is the error without specific cause . 
it should be toracica individuata in corso di addome diretto , o ancora le lesioni pleuriche , polmonari o mediastiniche incidentalmente comparse in corso di studio radiografico della colonna vertebrale , delle ossa del torace o del cingolo scapolare . 
berlin in un suo articolo , in un caso di contenzioso per la mancata individuazione alla mielografia di una malformazione arterovenosa del midollo spinale [ 19 ] , sottolinea che vi sono concrete difficolt a stabilire se nel caso lerrore fosse dovuto alla non percezione o alla scarse conoscenze del radiologo e che tali perplessit sono da estendere ad altre evenienze . il tentativo di spiegare la non identificazione con ulteriori cause risale agli anni 60 con le osservazioni di alcuni autori , quali smith e tuddenham , raccolte e commentate successivamente da wood e raufaste [ 8 , 10 , 11 ] : alcune lesioni potevano non essere individuate a causa di unaltra lesione presente nel documento che aveva catturato lattenzione del radiologo . 
berbaum [ 20 ] nello stesso filone di ricerca ha indagato il fenomeno con i propri collaboratori , introducendo una lesione nodulare artificiale nei radiogrammi del torace gi interessati da altre lesioni originali : lidentificazione di queste ultime , per il disturbo delle altre , diminuiva in modo significativo . 
egli ha chiamato un tale errore percettivo satisfaction of search , riconoscendo la tesi degli psicologi cognitivisti che notano che i radiologi tendono ad essere soddisfatti dopo la ricerca di una lesione e proseguono semmai oltre solo restringendo il campo dindagine su ci che hanno visto . in termini applicativi la quantit di errori percettivi varia a seconda delle indagini in questione . 
interessante notare come in una revisione della casistica personale di radiogrammi del torace e nel confronto con altri autori , quekel [ 21 ] riconosca in un intervallo da 16 a 40 mm delle dimensioni dei noduli un errore minimo del 20% ! in uno studio specifico sullefficienza delle prestazioni sanitarie watcher [ 22 ] riporta analoghe tipologie di errore relative ad altri organi ed apparati riconosciute da altri ricercatori : gli errori in emergenza hanno percentuali minime del 3%6% ( robin ) ; la sensibilit di rilevamento dei calcoli ureterali , molti dei quali riconoscibili a posteriori , del 46% ( levine ) ; la quota derrore nel clisma opaco del 15% ( wesses )  . una prima considerazione critica sugli errori percettivi , alla luce di casistiche e studi che esulano dal caso singolo con risvolti giudiziari , mette in evidenza come il vero rebus sia lerrore senza specifica causa . 
 [ 23 ] hanno studiato gli effetti della doppia e tripla lettura su un campione di 60 casi di clisma opaco a doppio contrasto , in cui erano presenti 46 lesioni . 
the radiologist is aware of the routine and surrounding working conditions ; a temporary loss of attention causes the slip , which may be considered a small monitoring error . a ( perceptual ) error caused by capture occurs when the radiologists attention is attracted by a sign and is satisfied by this first finding , using a more common working framework rather than a less common one . alongside this type of slip is one in which the error is so obvious that it is known as a description error . 
it is an error characteristic of reporting when a semantic field related to one technique is used to describe another , for example , a ct study described with echogenicity - based terminology , or an ultrasound described with density - based terminology . other slips , such as associative activation ( answering the telephone when the doorbell rings ) or loss of activation , described as the temporary loss of memory while performing a precise task ( the search for an object ) , appear to be circumstantial , more common with the use of high - tech equipment or procedures , and can immediately be made up for . 
therefore , performing tasks without disturbances or distractions is the best prevention for this type of error . in contrast , a series of factors of various natures may help create situations which foster the occurrence of slips . 
the most common psychological elements include fatigue , loss of sleep , alterations caused by alcohol or drugs , or emotional states such as boredom , frustration , fear , anxiety or anger all conditions which cause concern and distract ones atl . 
inches : systematic approach to human error in radiology errori cognitivi gli errori della fase cognitiva sono stati classificati da reason e rasmussen [ 6 ] con il riferimento ad ogni livello attenzionale come basati sulla capacit intellettiva ( skill based ) , sul metodo cognitivo ( rule based ) e sulla conoscenza ( knowledge based )  . 
errore caratteristico nella refertazione quando si utilizzi una semantica relativa ad una metodica per descriverne unaltra : ad esempio , un referto con terminologia basata sullecogenicit per unindagine tc o invece sulla densit per unecografia . altre sviste quali lattivazione di associazioni ( associative activation ) come rispondere al telefono quando suona il campanello o la mancanza dattivazione ( loss of activation ) ovvero la temporanea perdita di memoria in corso di unazione ben precisa , come la ricerca di un oggetto , appaiono circostanziali , pi frequenti nel corso dimpiego di tecnologie o procedure , e di solito dimmediato recupero . tuttavia va sottolineato come le sviste sono spesso causate da interruzioni di precedenti attivit che erano in atto . pertanto lo svolgimento dellattivit senza disturbi e distrazioni la migliore prevenzione per tali tipologie derrore . per contro , una serie di fattori di diversa natura pu innescare situazioni favorevoli alle sviste . 
gli elementi psicologici pi frequenti comprendono la fatica , la perdita di sonno , le alterazioni da alcool o droghe oppure stati emozionali , quali la noia , la frustrazione , la paura , lansia , la collera , tutte condizioni che conducono alla preoccupazione che distrae lattenzione . a queste condizioni possono contribuire altri fattori esterni quali leccesso di lavoro e le relazioni interpersonali difficili o ambientali come il rumore , la calura , stimoli visivi eccessivi . 
in addition to these conditions , there may also be external factors , such as an excessive workload , difficult interpersonal relations or an unfavourable working environment characterised by excessive noise , heat or visual stimuli . in di , therefore , a large number of slips can be the result of working environments inappropriate for the study of radiographic images , excessive workloads , difficult conditions in the department and so on . rule - based and knowledge - based errors errors related to the two cognitive activities , commonly known as psychological errors , have been studied less than others and are more difficult to assess . 
these errors are due to an erroneous assessment of a contingent situation for which an incorrect procedure is applied . figure 5 shows how those errors , more correctly defined mistakes , are both recognition and decision making in nature . 
mistakes are therefore specifically cognitive errors , distinct from the more general term errors , which includes all types and therefore perceptual and system errors as well . figure 5 also shows how recognition errors are usually based on the most commonly used reasoning , adopted due to mental laziness on the part of the radiologist who has trouble breaking from known and repeated implementation models . included with this mental laziness or preconceived positions are mistaken choices , which piattelli - palmarini [ 24 ] defines deadly sins and which are summarized in figure 5 and outlined here below : biased memory leads to overgeneralizations of the ordinary or undergeneralizations of facts due to emotive reactions connected with personal success or contradictory experiences . heuristic availability prompts us to use only the primary information which comes to mind . confirmation bias supports our working hypotheses , causing us to ignore all contradictory information . overconfidence leads us to overestimate ourselves and our own abilities . anchoring highlights the influence that our first impression , or first judgement , has and how it becomes impossible to completely suppress it in later revisions . probability blindness refers to the mental procedure incapable of taking into consideration probabilistic estimates . it is so dangerous that piattelli - palmarini warns that any probabilistic intuition of any person not specifically versed in probability calculations has more than 50% probability of being incorrect [ 24 ]  . reconsideration under suitable scripts , lastly , is the seventh of the mental procedures which lead to cognitive errors . 
it is thought that a type of event or situation is judged all the more frequently the easier it is to mentally imagine and the greater the emotional impact it has as well as the more our judgement of probability is biased by the scripts . together with these seven deadly sins of the mind are two inevitable corollaries , situations contingent to the work phases : errori nellambito dellattivit basata sulle regole ( ruled based activity ) e dellattivit basata sulla conoscenza ( knowlodge based activity ) gli errori inerenti le due attivit cognitive , denominati comunemente psicologici , sono i meno studiati e i pi difficili da inquadrare : spesso sono identificabili pi cause che insieme contribuiscono allerrore . 
la figura 5 evidenzia ancora come lerrore di riconoscimento si basi di solito sul ragionamento usato pi frequentemente , cui si ricorre a causa della pigrizia mentale del radiologo , che stenta a staccarsi da schemi applicativi noti e ripetuti . 
clinical information may play a determining role in this assessment . before taking into consideration this aspect , which is fundamental in daily practice , it is worth noting the three main types of error in di associated with mental tunnels , as proposed by fitzgerald [ 26 ] : availability bias : the ease of remembering a diagnosis specific to the case compromises the possibility of making a correct diagnosis . regret bias : a distorted probability of diagnosis influences the correctness in the unconscious desire that something regrettable occurs . framing bias : the frame of the examination ( the request , case history , etc . ) unduly influences the report . a study in 1992 by norman et al . 
the first phase of the experiment involved 50 radiologists called on to assess 50 radiographs 25 from patients affected by bronchiolitis and 25 from normal patients with the radiologists being asked to search for signs of disease such as hyperinsufflation , bronchiolar thickening and perihilar opacities . the signs were found in both diseased and healthy patients in compliance with the suggested provisional diagnosis . 
in the second phase of the experiment , the radiographs were accompanied with a brief clinical history of normality or pathology , and three radiologists were specifically asked what the real probability of bronchiolitis was . the experiment showed the consistent effect of the clinical history on both attribution of a diagnostic category and the radiological signs on uncertain radiographs . 
at any rate , there is no doubt that knowledge of clinical history and signs regarding physical examination increase the possibility of radiological interpretation . further useful information can be gleaned from a comparison of previous radiological studies performed on a patient , as studied by berbaum et al . 
 [ 28 ] and berlthe american college of radiology has included the procedure among the published quality standards , stating that comparison with relevant previous examinations and reports should be part of the radiologic consultation and report when appropriate and available . 
inches : systematic approach to human error in radiology centrarsi su una sola fonte dinformazione ; il capovolgimento sotto affaticamento ( reversion under stress ) il fenomeno nel quale i comportamenti appresi di recente sono sostituiti con altri pi vecchi , ma pi familiari anche se inadatti al problema in esame . 
gli errori di riconoscimento avvengono quando una anomalia vista dal radiologo , ma non apprezzata come tale ; in realt riconoscere unanomalia richiede pi una memoria visiva che unacuit visiva . 
le informazioni cliniche possono giocare un ruolo determinante in questo giudizio . prima di prendere in considerazione tale aspetto , fondamentale nella pratica quotidiana , vale la pena di riportare da fitzgerald [ 26 ] i tre principali tipi di errore nella di connessi ai tunnel mentali : influenza della memoria ( avaibility bias ) : la facilit di ricordare una diagnosi specifica al caso pregiudica la possibilit della diagnosi corretta ; influenza emotiva ( regret bias ) : una distorta probabilit di diagnosi influenza la correttezza , nellinconscio desiderio che avvenga qualcosa che dispiace ; influenza del contorno ( framing bias ) : la cornice dellesame ( richiesta , anamnesi etc ) influenza eccessivamente il referto . a tale riguardo uno studio di norman del 1992 [ 27 ] dimostra empiricamente limportanza delle informazioni cliniche . 
lesperimento riguarda 50 radiologi esperti chiamati a valutare in una prima fase 50 radiogrammi , 25 di pazienti affetti da bronchiolite e 25 normali , chiedendo loro di ricercare i segni della malattia quali iperinsufflazione , ispessimento bronchiolare , opacit perilari . 
in una seconda fase stato chiesto esplicitamente ai tre radiologi quale fosse in ogni radiogramma , cui era stata aggiunta una breve storia clinica di normalit o di patologia , la probabilit reale di bronchiolite . 
a livello operativo nessuno osa in ogni caso mettere in dubbio che la conoscenza della storia clinica e dei segni relativi allesame obiettivo aumentino le possibilit dinterpretazione radiologica . altre informazioni utili possono ancora essere desunte dal confronto con i precedenti studi radiografici eseguiti sul paziente , come sperimentato da berbaum e berlin [ 28 ]  . lamerican college of radiology ha posto la procedura tra gli standard di qualit pubblicati affermando che il confronto con gli esami precedentemente eseguiti dal paziente , quando possibile , parte integrante dellindagine radiologica l . 
inches : systematic approach to human error in radiology space and time can be resolved with the picture archiving communication system ( pacs ) [ 29 ] which with the storage of digital data ( and therefore not analogical images ) could nonetheless give rise to revisions and evaluations after the fact , both regarding the use of the same in the broadest possible sense and the perception and interpretation of the derived images . if knowledge of the history and a comparison of previous data are valid methods for eliminating the radiologists decision - making errors , then reading previous radiological reports could also prove useful . 
this proposal , however , opens up an important debate regarding alliterative errors [ 30 ] , defined as an erroneous and reiterated diagnosis by several radiologists on the basis of the report of the first radiologist . the first such case reported by berlin [ 30 ] of a case of lung cancer , which on several occasions was labelled as bronchopneumonia , was followed by an important debate . 
the theory of berlin [ 31 ] which states that if a radiologist fails to recognize an anomaly or incorrectly interprets its meaning , then the possibility of the next radiologist repeating the same error is noticeably increased is supported by smith , cited by berlin [ 31 ] , who states that radiologists are induced to read the report of a colleague before assessing the radiograph . 
laspetto relativo allarchiviazione , di difficile applicazione nello spazio e nel tempo , potr essere risolto dai sistemi digitali pacs [ 29 ] , che tuttavia con la memorizzazione dei dati numerici ( non immagini analogiche quindi ) potranno dare luogo a revisioni e giudizi postumi , sia sullutilizzazione degli stessi in tutta la loro ampiezza che sulla percezione e interpretazione delle immagini ricavate . se la conoscenza della storia e il confronto con i dati precedenti sono metodi validi per eliminare gli errori decisionali del radiologo , anche la lettura dei referti precedenti allegati potrebbero rientrare in questa ottica . laffermazione apre tuttavia limportante dibattito relativo allerrore alliterativo [ 30 ] , individuando in questo unerronea e reiterata diagnosi da parte di pi radiologi sulla base del referto del primo radiologo . 
alla prima segnalazione di berlin su un caso di tumore polmonare , in pi circostanze etichettato come broncopolmonite [ 30 ] segu un importante dibattito . la teoria di berlin [ 31 ] che , se un radiologo non vede unanomalia o le attribuisce un significato sbagliato , la possibilit che il successivo radiologo ripeta il medesimo errore notevolmente aumentata sostenuta anche da smith , citato da berlin [ 31 ] , il quale afferma che i radiologi sono portati a leggere il riscontro del collega prima dellapproccio al radiogramma . tuttavia lamerican college of radiology nello standard for communication mette in evidenza che il paragone con precedenti esami e referti , dove possibile , parte integrante dellanalisi radiologica . 
in una successiva revisione berlin [ 32 ] riporta da autori diversi analisi sperimentali in contraddizione , riconoscendo che hunter e boyle dimostrano lutilit nel leggere i precedenti referti nel 60% dei casi e un considerevole aiuto nel 22%24% dei casi , mentre white segnala solo 1 , 5% di utilit e un 48% di inutilit . 
scelta della soglia del sospetto . ferred to for the following discussion . in the strategy outlined in model 1 , the threshold of suspicion would lead to a high specificity for the test and a good level of sensitivity but with 19% more false negatives than model 2 . 
on the other hand , the threshold of suspicion is lower in model 2 , thus introducing more recognizable minimal signs , even in healthy breasts , and therefore reducing the specificity of the test to the point of increasing false positives by 4 , 110 cases ( out of a total of 17 , 000 )  . 
so a diagnostic gain of 19% ( no small thing ! ) is counterbalanced by the anxiety of being called for follow - up multiplied by ten times and the implementation of invasive procedures multiplied by five . 
on the basis of current knowledge and experience , since in both cases the radiologist knows in advance the nature of the error , either false positive or false negative , and plans his or her work activity on the basis of this assessment , the error may be defined as strategic , especially if the choice is shared in the context of coordinated decision making and operations . 
as a result , in the implementation phase of breast screening , the error becomes operatively present , with a meaning similar to that codified by federspil and vettor [ 1 , 2 ] in clinical activity , when there is a choice of two alternative therapies . prevedere la diversa distribuzione degli errori : la figura 7 , di facile comprensione nei passaggi dai valori assoluti a quelli percentuali [ 39 ] , funge da riferimento per le successive argomentazioni . 
nellipotesi di una scelta strategica che si uniformi al modello 1 la soglia del sospetto comporterebbe unelevata specificit del test ed una buona sensibilit , ma con una quota di falsi negativi del 19% in pi rispetto al modello operativo 2 . 
daltro canto nel modello operativo 2 , ove la soglia del sospetto si abbassa , introducendo quindi molti segni minimi riconoscibili anche in mammelle sane , la specificit del test si riduce al punto di aumentare di ben 4410 casi ( su 17000 donne ! ) i falsi positivi . 
poich , sulla base delle attuali conoscenze ed esperienze , in entrambi i casi il radiologo conosce preventivamente il versante dellerrore , falso positivo o falso negativo , e anche in base a tale valutazione progetta la sua attivit , lerrore pu essere definito strategico , a maggior ragione se la scelta condivisa nellambito di un coordinamento operativo - decisionale . 
inches : systematic approach to human error in radiology system errors it has already been mentioned how system errors have repercussions in the end on the final medical assessment , with the characteristic connotations of human error [ 7 ]  . 
it has been recognized that the system as such has peculiarities in which the cause of errors is to be found . generally speaking , we would intuitively expect a wellconstructed system to be equipped with defences , barriers and mechanisms which reduce the risk of errors to a minimu nonetheless , those mechanisms , which reason and rasmussen [ 6 ] liken to barriers filled with holes , are extremely vulnerable when the holes line up on the same trajectory . the inevitable error is accompanied by the personal application , which is not able to correct the error owing to a series of preexisting causes , such as those summarized in figure 6 . system errors are therefore prevented above all by adopting a safety system which renders their occurrence difficult for individual work and by performing constant research which is accompanied by daily efficiency [ 40 ]  . there are numerous suggestions for achieving this in di . 
those which draw on applicative criteria include protocols for reducing reliance on memory , improvement of access to information through the patients case history , use of systems impermeable to errors to avoid homonymy , and training . measures more specifically related to the department include maintenance of quality standards , systematic control of equipment , revision of reports and appropriate instructions to users . federspil e vettor [ 1 , 2 ] nellattivit clinica , allorch si mettano in alternativa due scelte terapeutiche . errori di sistema gi stato dato risalto a come gli errori di sistema si ripercuotano alla fine sulla valutazione medica conclusiva , con le connotazioni caratteristiche dellerrore umano [ 7 ]  . 
allerrore inevitabile si aggiunge lapplicazione personale , che non in grado di correggerlo per una serie di concause tra le quali si riconoscono in modo immediato quelle raccolte in figura 6 . 
la prevenzione degli errori di sistema si attua quindi sopratutto mediante un apparato di sicurezza che li renda di difficile evenienza per il lavoro individuale e mediante una costante ricerca che proceda di pari passo con lefficienza giornaliera [ 40 ]  . nella di molti sono i suggerimenti in questo senso . 
tra quelli che si rifanno ai criteri applicativi generali si citano i protocolli per ridurre la fiducia nella memoria , il miglioramento allaccesso dellinformazione mediante la cartella clinica del paziente , luso di sistemi impermeabili agli errori ad evitare omonimie , laddestramento . 
per quanto riguarda pi specificamente il reparto si ricordano il mantenimento degli standard di qualit , il controllo sistematico delle attrezzature , la revisione dei referti , le idonee segnalazioni agli utenti . conclusions considerazioni conclusive error is a characteristic feature of human activity . 
the latin saying errare humanum est may be applied to all activity , and di is no exception . perhaps less well known is the medieval addition to the saying attributed to saint bernard sed perseverare diabolicum indicating that errors upset our balance and therefore need to be corrected or , better still , prevented . to achieve these aims in a complex system such as di , simple recognition of the error does not appear to be sufficient . preliminary knowledge of the types and causes of errors relating to human activity and the system is required , as well as their application in a daily analysis to improve both standards of service and personal satisfaction . lerrore rappresenta una connotazione caratteristica delle azioni umane . 
gargiulo2 1dipartimento integrato dei servizi diagnostici e per immagini , azienda policlinico , via del pozzo 71 , i - 41100 modena , italy 2cattedra di chirurgia vascolare , azienda policlinico , modena , italy correspondence to : m.g. 
 + 39 - 059 - 4222238 , fax : + 39 - 059 - 4224349 , e - mail : amorico.mariagrazia@policlinico.mo.it received : 27 june 2005 / accepted : 18 october 2005 / published online : 3 march 2006 abstract purpose . 
magnetic resonance angiography ( mra ) has recently become instrumental in the diagnosis of arterial disease in various body districts and is gaining an increasingly important role in the study of peripheral vascularisation . 
mra was performed with a philips intera 1.5 t , with acquisitions from the coeliac trunk to the feet . for acquisitions of the feet and ankles we used unenhanced timeof - flight ( tof ) sequences with a head coil . 
digital subtraction angiography ( dsa ) remains the reference standard for planning treatment and for the follow - up of these patients , but it is invasive and potentially harmful as the iodinated contrast larteriopatia occlusiva periferica degli arti inferiori una patologia cronica e progressiva con unincidenza negli uomini con pi di 55 anni che va dal 4 , 5% al 8 , 8% [ 1 , 2 ]  . 
la diagnosi solitamente ottenuta mediante un accurato esame clinico , ma la scelta di uneventuale terapia non pu prescindere da precise informazioni morfologiche dellalbero arterioso ottenibili esclusivamente attraverso la diagnostica strumentale . 
because peripheral arterial occlusive disease is an increasingly common chronic condition , a large number of mostly elderly patients would have to undergo numerous angiographic examinations and endovascular procedures , both of which carry a high risk of complications , such as puncture of the arteries , iodinated contrast agent toxicity , and protracted exposure to radiation [ 3 ]  . 
for these reasons , it has become necessary to identify an alternative modality that is less invasive than dsa and able to evaluate the number and severity of lesions in order to plan treatment . 
recent technological innovations , such as continuous table movement and very fast three - dimensional ( 3d ) sequences [ contrast - enhanced mr angiography ( ce - mra ) ] [ 2 , 5 ] , have enabled the study of the arteries from the abdominal aorta to the foot with a single injection of contrast material . 
these improvements have overcome the limitations of the previous time - of - flight ( tof ) and phasecontrast sequences , such as long acquisition times ( ats ) and flow and movement artefacts . 
the aim of this study was to assess the reliability of mra in the evaluation of lesions caused by peripheral arterial occlusive disease , using intraarterial dsa as the reference standard . materials and methods patients from november 2003 to august 2004 , a total of 30 patients ( 11 women and 19 men ; age range , 4984 years ; mean age , 72 years ) underwent digital subtraction angiography and mra of the lower limbs . 
two patients had concurrent renal artery stenosis ( one on the right and one on the left ) , and another two had aneurysm of the infrarenal aorta , one of whom with concurrent aneurysm of the left popliteal artery . 
two patients were excluded after dsa because they had a pacemaker , and another was excluded due to a history of surgery with insertion of artificial crystalline made of non - mr - compatible material . 
poich larteriopatia periferica una patologia cronica in aumento , un numero elevato di pazienti , la maggior parte anziani , dovrebbe essere sottoposto a numerose angiografie e procedure endovascolari che comportano un elevato rischio di complicanze sia legate alla procedura , come la puntura dei vasi arteriosi , che alla tossicit del mezzo di contrasto ed allesposizione prolungata alle radiazioni ionizzanti [ 3 ]  . 
per tutti questi motivi si sentita lesigenza di una metodica di studio delle arterie degli arti inferiori meno invasiva e che possa essere utilizzata come valutazione del numero e della severit delle lesioni in previsione di un trattamento . la risonanza magnetica una tecnica di indagine non invasiva che non impiega radiazioni ionizzanti n mezzo di contrasto potenzialmente nefrotossico [ 4 ]  . 
recentemente sono state introdotte innovazioni tecnologiche come , per esempio , il movimento automatico del lettino porta - paziente e sequenze tridimensionali molto veloci ( ce - mra ) [ 2 , 5 ] che rendono possibile lo studio dellalbero arterioso dal tripode celiaco ai vasi del piede con ununica iniezione di mezzo di contrasto . 
ci ha permesso di superare le limitazioni delle precedenti sequenze time - of - flight e phase - contrast come i lunghi tempi di acquisizione , gli artefatti da flusso e da movimento . 
scopo di questo lavoro analizzare quale sia la reale affidabilit della angio - rm nella valutazione delle lesioni causate dallarteriopatia occlusiva periferica , utilizzando come standard di riferimento langiografia digitale a sottrazione ( dsa )  . materiali e metodi pazienti dal novembre 2003 allagosto 2004 , 30 pazienti di et compresa tra i 49 ed gli 84 anni ( 11 donne e 19 uomini ; et media 72 anni ) sono stati sottoposti ad angiografia digitale e ad angio - rm degli arti inferiori . 
due casi , inoltre , mostravano la presenza concomitante di stenosi dellarteria renale ( 1 a destra ed 1 a sinistra ) , in 2 casi un aneurisma dellaorta sottorenale in uno dei quali era concomitante un aneurisma dellarteria poplitea sinistra . 
the disease staging classification adopted by us was the following : mild stenosis ( not haemodynamically significant ) with less than 50% reduction in vessel lumen ; moderate stenosis ( haemodynamically significant ) with 50%90% reduction in lumen ; severe stenosis with a reduction in vessel lumen greater than 90% . the percentage of stenosis was automatically calculated by software present in the image - processing work stations connected to the angiographic and mr instruments ( viewforum , philips )  . patients included in the study underwent dsa performed with digital equipment ( philips integris allura , philips medical system , the netherlands ) , following a pre - established procedure . 
the examination procedure involved positioning of a 4 - french universal flash ( uf ) catheter into the abdominal aorta through a retrograde , generally right - sided , transfemoral approach , or a brachial approach according to the seldinger technique , after the local administration of 10 cc of lidocaine hydrochloride 200 mg ( bioindustria , italy )  . 
the catheter was positioned in the external or common iliac artery to perform selective arteriography of the limb , with anteroposterior ( ap ) projections for the thigh and leg vessels , and both ap and laterolateral ( ll ) projections for the feet vessels . 
images of the lower limb vessels , from the femoral artery to those of the feet , were obtained sequentially with separate injections of contrast material delayed relative to acquisition , on the basis of the level of study and the speed of flow . 
the mean dose of contrast agent injected was approximately 200 cc ( iomeprol 300 mg / i / ml , iomeron bracco , or iopamidol 300 mg / i / ml , iopamiro bracco ; iodixanol 270 mg / i / ml , visipaque nycomed amersham in selected subjects ) , with a range from 160 to 300 cc according to the diagnostic requirements of the single case . 
the entire examination had a mean duration of 60 min . mra was performed by using a 1.5 - t whole - body mri unit ( intera philips gyroscan 1.5 tesla , philips medical system )  . for each patient , a complete history was taken to exclude the presence of contraindications . 
the patient was positioned supine with both feet inside the coil usually used for the study of the head ( head coil ) for a preliminary evaluation of the foot arteries with an unenhanced 3d - tof sequence . 
due pazienti sono stati esclusi dallo studio dopo lesecuzione della dsa , perch portatori di pace - maker ed uno per presenza di anamnesi positiva per intervento con inserimento di cristallino artificiale di materiale non rm - compatibile . 
tre pazienti erano gi stati precedentemente sottoposti a procedure di rivascolarizzazione ( 1 by - pass femorofemorale destro - sinistro con bypass femoro - popliteo bilaterale , 1 by - pass femoro - popliteo destro , 1 endoprotesi hemoban in femorale superficiale destra ) e tre pazienti avevano subito lamputazione di uno o pi dita di un piede . la classificazione da noi seguita distingue : stenosi lievi ( non emodinamicamente significative ) con riduzione del lume vasale inferiore al 50% ; stenosi moderate ( emodinamicamente significative ) con riduzione del lume vasale superiore al 50% , ma inferiore al 90% ; stenosi gravi con riduzione del lume vasale superiore al 90% . la percentuale di stenosi stata calcolata automaticamente da un programma di calcolo presente nelle stazioni di elaborazione delle immagini correlate allangiografo philips allura ed allapparecchio di rm ( viewforum , philips medical systems , olanda )  . angiografia digitale i pazienti inclusi nello studio sono stati sottoposti a dsa con tecnica di sottrazione dimmagine eseguita con angiografo digitale ( integris allura philips , philips medical systems , olanda ) , seguendo una procedura prestabilita . 
lesecuzione dellesame prevede il posizionamento di un catetere uf ( universal flash ) di 4 f nellaorta addominale per mezzo di un approccio transfemorale retrogrado , generalmente destro , o brachiale , con ago munito di mandrino secondo la tecnica seldinger , ovviamente dopo aver eseguito nella sede lanestesia locale con 10 cc di lidocaina cloridrato 200 mg . 
il catetere viene posizionato in arteria iliaca esterna o comune per lesecuzione di unarteriografia darto selettiva ; si effettuano riprese dei vasi di coscia e di gamba in a - p e del piede sia in a - p che in ll . 
le immagini del riempimento degli arti inferiori dallarteria femorale a quelle del piede sono state ottenute sequenzialmente con iniezioni separate di mezzo di contrasto ritardate rispetto allacquisizione in base al livello di studio ed alla velocit del flusso . 
la dose media di mezzo di contrasto iniettato per via endoarteriosa di 200 cc circa ( iomeprolo 300 mg i / ml , iomeronr bracco oppure iopamidolo 300 mg i / ml , iopamiror bracco ; iodixanolo 270 mg i / ml , visipaquer , amersham , in soggetti selezionati ) , con un range variabile da 160 a 300 cc a seconda delle esigenze diagnostiche del singolo caso . 
the parameters used were : tr 23 ms , te 9.2 ms , flip angle 20 , thickness 0.7 mm , matrix 304x258 , field of view ( fov ) 30 c the sequence yielded around 150 images , which were processed in 3d at the workstation view forum 3.1 ( philips medical systems )  . 
subsequently , the head coil was replaced with a body coil , with mobytrack , a specific attachment for this type of study which supports and immobilises the legs at the level of the knees and holds the feet perpendicular to the legs . 
positioning of the entire lower limb in the same plane is important , as the coronal acquisition might otherwise miss arterial segments not perfectly included in the field of view . 
the arterial study was performed with three 40to 45 - cm acquisitions , with 3d coronal sequences from the coeliac trunk to the feet , each lasting around 3035 s , with an overlap of 13 c automatic table movement means the examination can be performed in a time compatible with the persistence of the paramagnetic contrast agent in the arterial vessels . first , a 2d fast - field - echo centring sequence was performed in the three planes in all three positions , on which the following sequences were planned . 
the parameters of this sequence were : tr 6.1 ms , te 1.5 ms , flip angle 35 , thickness 1.5 mm , matrix 512x384 , fov 43 cthen , circulation time ( ct ) , or bolus timing , was evaluated by injecting 2 cc of contrast agent followed by 15 cc of saline solution with a special mr - compatible injector ( spectris mr injector , medrad )  . 
this was followed by a fast - field - echo sequence ( tr 7 , te 0.87 , flip angle 40 , thickness 80 mm , matrix 256x256 , fov 53 cm ) in which a single coronal image at the level of the abdominal aorta and its bifurcation was acquired at intervals of 1 s for about 50 times , repeating the same image at regular intervals until the contrast agent was visualised . 
scan delay ( sd ) was obtained by subtracting half of the at from the ct plus half of the injection time ( it ) : sd = ct + ( it / 2 ) - ( at / 2 )  . an initial unenhanced 3d sequence serving as a mask was performed from the feet to the abdomen . 
around 40 - 50 cc of paramagnetic contrast agent ( gadodiamide ; omniscan nycomed amersham ) [ 15 ] was then injected as a bolus divided in two fractions : 50% was injected at a speed of 1 ml / s and 50% at a speed of 0.5 ml / s , followed by 15 ml of saline solution injected at a speed of 1 ml / s . 
this part of the examination lasted 2025 mparameters used in this sequence were : tr 6.1 ms , te 1.5 ms , flip angle 35 , thickness 1.5 mm , matrix 512x384 , fov 43 cthe 3d sequence used by us was designed to acquire a centric k space , the centre of the k space being acquired during the enhancement peak , which provides the best contrast between blood and static tissue . 
approximately 200 images were obtained , which were reconstructed with 3d maximum image projecte superconduttivo ( philips gyroscan intera 1 , 5 tesla , olanda ) dotato di gradienti con intensit massima di 30 mtesla / m ed una rapidit di salita ( slew rate ) di 150 mtesla / m / ms . 
il paziente viene posizionato supino , con entrambi i piedi allinterno della bobina solitamente usata per lo studio dellencefalo ( head ) , per eseguire una preliminare valutazione delle arterie del piede attraverso un sequenza 3d - tof senza mezzo di contrasto . 
la sequenza viene eseguita su un piano coronale obliquo perpendicolare allasse maggiore del piede e la banda di presaturazione necessaria per impedire il contemporaneo rilevamento del flusso venoso posta caudalmente alla acquisizione . 
successivamente si effettua un cambio di bobina : si sostituisce la bobina head e si utilizza la bobina body per la trasmissione e la ricezione del segnale ed un supporto dedicato per lo studio degli arti inferiori , moby - track , che sostiene ed immobilizza le gambe a livello delle ginocchia , che sono leggermente sollevate , e mantiene i piedi su uno stesso piano perpendicolare a quello delle gambe . 
il posizionamento di tutto larto inferiore su uno stesso piano un accorgimento importante poich altrimenti lacquisizione nel piano coronale potrebbe non includere segmenti arteriosi non perfettamente compresi nel campo di vista . 
lo studio arterioso viene eseguito in 3 acquisizioni da 4045 cm con sequenze 3d coronali dal tripode ai piedi , ognuna della durata di circa 3035 secondi , con sovrapposizione di 13 cil movimento automatizzato del letto porta - paziente permette di eseguire questo tipo di esami in un tempo compatibile con la permanenza del mezzo di contrasto paramagnetico nei vasi arteriosi . 
si esegue inizialmente una sequenza di centratura 2d turbo field echo sui 3 piani in tutte le 3 posizioni sulla quale verranno pianificate tutte le sequenze successive con i seguenti parametri : tr 6 , 1 ms , te 1 , 5 ms , flip angle 35 , spessore 1 , 5 mm , matrice 512x384 , campo di vista 43 csi procede poi ad una valutazione del tempo di circolo o bolus timing iniettando 2 cc di contrasto seguiti da 15 cc di soluzione fisiologica con un apposito iniettore rm - compatibile ( spectris mr injector , medrad , indianola , pa )  . 
si esegue una sequenza fast field echo ( tr 7 , te 0 , 87 , flip angle 40 , spessore 80 mm , matrice 256x256 , campo di vista 53 cm ) , in cui una singola immagine coronale , a livello dellaorta addominale e della sua biforcazione acquisita ad intervalli di 1 secondo per circa 50 volte ripetendo la stessa immagine ad intervalli costanti fino alla visualizzazione del mezzo di contrasto a quel livello . 
il tempo di ritardo scansione ( trs ) si ottiene sottraendo al tempo di circolo ( tc ) la met del tempo di acquisizione ( ta ) , dopo avervi sommato la met del tempo di iniezione table 1 evaluation form right left m . 
the total time spent by the patient inside the mr room , which included examination time , technical time for sequence formulation , and coil changing , was about 4045 min . data collection and analysis mra and dsa examinations were independently evaluated by three radiologists who used grading sheets to assess vessel state : no stenosis , or obstruction . 
the vessel being studied was drawn with parallel lines along a segment that includes the vessel above and below the stenosis and stenotic segment ; the computer analyses the segment and calculates the percentage of stenosis . 
conventional angiography examinations were evaluated by another radiologist blinded to the patients clinical history and results of mra . table 2 patent arteries with regular lumen artery common iliac external iliac internal iliac common femoral superficial femoral deep femoral popliteal anterior tibial posterior tibial peroneal dorsalis pedis plantaris pedis total mra , magnetic resonance ; dsa , digital subtraction angiography tabella 2 arterie pervie di calibro regolare vaso angio - rm angiografia a . 
si iniettano poi circa 4050 cc di contrasto paramagnetico ( gadodiamide omniscanner amersham , uppsala ) in un unico bolo suddiviso in due frazioni : il 50% viene iniettato ad una velocit di 1 ml / s , il restante ad una velocit di 0 , 5 ml / s ; seguito da 15 ml di fisiologica iniettata ad una velocit di 1 ml / s . 
la seconda sequenza con contrasto ha uno start - delay calcolato in base al bolus timing e viene eseguita dal tripode celiaco ai piedi . lapnea richiesta solo durante lacquisizione a livello addominale ed ha una durata di circa 25 s . 
il software della macchina sottrae automaticamente la sequenza con contrasto alla maschera per eliminare il segnale del tessuto adiposo e si ottiene unimmagine angio - rm delle arterie degli arti inferiori . 
la durata di questa parte dellesame di circa 2025 m i parametri utilizzati per eseguire questa sequenza sono : tr 6 , 1 ms , te 1 , 5 ms , flip angle 35 , spessore 1 , 5 mm , matrice 512x384 , campo di vista 43 cla sequenza 3d da noi utilizzata impostata per acquisire lo spazio k in senso centrico , grazie infatti allopzione centra , per cui viene acquisito il centro dello spazio k durante il passaggio del picco di contrasto massimo , che fornisce il contrasto migliore tra sangue e tessuto stazionario . 
il tempo totale che il paziente trascorre allinterno della stanza del magnete , che comprende il tempo desame , il tempo tecnico di impostazione delle sequenze e di cambio delle bobine di circa 4045 minuti . raccolta ed analisi dei dati gli esami di angio - rm e di angiografia sono stati valutati da 3 medici radiologi in modo indipendente attraverso la compilazione di schede , in cui si richiede di valutare lo stato del vaso : pervio , stenosi , ostruzione . 
la percentuale di stenosi stata ottenuta tramite un programma di calcolo inserito in speciali stazioni di elaborazione delle immagini , in cui viene disegnato con linee parallele il vaso in esame per un tratto che comprende il vaso a valle e a monte della stenosi ed il segmento stenotico ; il computer analizza il segmento in esame e calcola la percentuale di stenosi . 
langio - rm stata valutata da 2 medici radiologi in doppio cieco , senza conoscere la storia clinica del paziente ed i risultati dellangiografia tradizionale , utilizzando le rielaborazioni 3d delle immagini e le immagini originarie . 
si sono ottenute due schede ( tabella 1 ) per ogni paziente , una per la rm ed una per la angiografia , che sono state poi confrontate per valutare il livello di corrispondenza . 
i vasi arteriosi esaminati sono : aorta sottorenale , iliaca comune , iliaca esterna , iliaca interna , femorale comune , femorale superficiale , femorale profonda , poplitea , tibiale anteriore , tibiale posteriore , interossea , dorsale e plantare del piede . 
nei 2 pazienti con bypass se ne valutata anche la perviet , lo stato degli stessi e dei territori a valle . thus , two tables were obtained ( table 1 ) for each patient : one for mra and one for dsa , which were compared in order to evaluate the level of concordance . 
arterial vessels examined were : infrarenal aorta ; common iliac artery ; external and internal iliac arteries ; common , superficial , and deep femoral arteries ; popliteal artery ; anterior and posterior tibial arteries ; peroneal artery ; and dorsalis and plantaris pedis arteries . 
in the two patients with bypass , we also evaluated the patency and state of the bypass grafts and territories downstream . results mra was easy to perform and well tolerated although patients with trophic lesions , especially of the heels , had some difficulty staying motionless in the supine position because of pa this problem concerned above all the tof sequences , in which both feet have to be kept motionless inside the head coil for about 7 mas a result , because this sequence requires a very high level of patient cooperation , it was only performed in 15 . 
however , it did not yield important additional information compared with the contrast - enhanced study , except in one case . table 3 occlusions artery common iliac external iliac internal iliac common femoral superficial femoral deep femoral popliteal anterior tibial posterior tibial peroneal dorsalis pedis plantaris pedis total mra , magnetic resonance ; dsa , digital subtraction angiography tabella 3 occlusioni a . 
questo problema ha riguardato soprattutto lesecuzione delle sequenze tof , in cui entrambi i piedi devono rimanere immobili allinterno della bobina per circa 7 min . questa sequenza infatti non stata eseguita in tutti i pazienti , ma solo in 15 , in quanto necessita di estrema collaborazione e non ha dato informazioni rilevanti o aggiuntive rispetto allo studio con mezzo di contrasto , tranne in un singolo caso . 
sono stati visualizzati 552 vasi di calibro regolare con langio - rm e 547 con la dsa ( tabella 2 )  . si ottenuta una corretta visualizzazione di tutti i vasi fino alla caviglia , mentre per quanto riguarda le arterie del piede , in 3 casi , il precoce ritorno venoso ha reso difficile linterpretazione dellesame , ma grazie alla rielaborazione delle immagini alla workstation siamo sempre riusciti ad espritable 4 stenoses artery < 50% > 50% > 90% < 50% > 50% > 90% common iliac external iliac internal iliac common femoral superficial femoral deep femoral popliteal anterior tibial posterior tibial peroneal dorsalis pedis plantaris pedis total mra , magnetic resonance angiography ; dsa , digital subtraction angiography tabella 4 stenosi a . 
correct visualisation of all vessels was obtained up to the ankle whereas in the foot arteries , early venous return in three cases made interpretation of the examination difficult ; nonetheless , image processing enabled a judgement on the vessel to be expressed in all cases . 
discordances regarded the infrapopliteal arteries , with mra visualising the obstruction of 28 anterior tibial arteries , 35 posterior tibial , 14 peroneal , and 23 dorsalis pedis as against the 30 anterior tibial , 33 posterior tibial , 18 peroneal , and 22 dorsalis pedis visualised by dsa . 
in the cases of obstruction , the visibility of the collateral circulations was better with dsa , which was able to depict even tiny branches , but was also judged good with mra , which depicts the larger vessels only . 
evaluation of the foot arteries was more difficult : the tof sequences , if correctly performed , give information on the larger vessels perpendicular to the acquisition plane ; the contrast - enhanced sequences are also informative but they have a smaller field of view . 
as regards the nine ( 1.25% ) discordant segments , mra overestimated two ( 0.3% ) ( two occlusions of the posterior tibial arteries ) and underestimated six ( 1% ) ( two anterior tibial and four peroneal arteries )  . 
mra documented one occlusion of dorsalis pedis artery not visualised by dsa . overall , in the cases studied , mra had a specificity of 99.6% and a sensitivity of 96% ( table 5 )  . 
there was absolute concordance between the two imaging procedures in il numero di occlusioni valutato in angio - rm stato 140 e con la dsa 143 ( tabella 3 )  . 
le discordanze sono nelle arterie infrapoplitee , in particolare langio - rm ha riconosciuto lostruzione di 28 arterie tibiali anteriori , 35 tibiali posteriori , 14 interossee , 23 dorsali del piede contro le 30 tibiali anteriori , 33 tibiali posteriori , 18 inter - ossee , 22 dorsali del piede della dsa . 
nelle stenosi inferiori al 50% langio - rm ne ha riconosciute 13 , la dsa 14 : con questultima stata riconosciuta una stenosi dallarteria femorale profonda che risultava pervia alla angio - rm . 
nei casi di ostruzione la visibilit dei circoli collaterali stata migliore con la dsa , che stata in grado di evidenziare tutti i rami anche di piccolissimo calibro , ma stata giudicata buona con langio - rm , che mette in evidenza solo vasi di calibro maggiore . con entrambe le metodiche comunque possibile evidenziare il punto di ricanalizzazione del vaso . 
la valutazione pi difficoltosa stata quella dei vasi del piede : le sequenze tof danno informazioni , se correttamente eseguite , sui vasi di maggior calibro e perpendicolari al piano dacquisizione ; le sequenze con contrasto danno buone informazioni , ma hanno un campo di vista inferiore . 
dei 9 ( 1 , 25% ) segmenti discordanti , 2 ( 0 , 3% ) sono stati sovrastimati con langio - rm ( 2 occlusioni delle tibiali posteriori ) e 6 ( 1% ) sono stati sottostimati ( 2 tibiali anteriori e 4 inter - ossee )  . 
la permanenza totale del paziente nella sala del magnete stata in media di 45 mil tempo necessario alla rielaborazione ed alla stampa delle immagini alla workstation philips stato di 2030 mcome gi detto in caso di importante contaminazione venosa stato necessario un tempo maggiore . 
non si sono avute reazioni ai mezzi di contrasto in nessuno dei pazienti . discussione la tecnica di angio - rm da noi utilizzata , basata sullacquisizione di 3 volumi lievemente sovrapposti , iniettando il contrasto con uniniezione bifasica , ha permesso unaccurata valutazione dellalbero arterioso dal tripode celiaco alle arterie del piede . 
rispetto allangiografia , la rm offre importanti vantaggi nello studio di pazienti anziani con patologia arteriosa periferica , in quanto si possono evitare i rischi associati alla puntura arteriosa , al mezzo di contrasto iodato ed alle radiazioni ionizzanti . 
none of the patients experienced reactions to the contrast agent . discussion mra , based on the acquisition of three slightly overlapping volumes with two - phase injection of contrast agent , allowed table 6 data from the literature m . 
nellesecuzione dellangiorm si pu incorrere in alcuni pitfalls soprattutto perch per ottenere un esame angio - rm di elevata qualit con contrasto fondamentale la perfetta coordinazione tra linizio dellacquisizione e larrivo del mezzo di contrasto nella regione da studiare . 
non si sono avute comunque sostanziali discordanze tra angio - rm e dsa nella rilevazione della perviet dei vasi e nella valutazione della presenza di malattia aterosclerotica in tutti i territori esaminati . 
nello 0 , 3% dei casi si rilevata una sovrastima della gravit delle lesioni in angio - rm rispetto alla dsa [ 6 ]  . la sovrastima causata dal defasamento degli spin prodotto dal flusso turbolento che si crea nelle stenosi e da effetti di volume parziale . 
questo effetto risulta accentuato nelle ricostruzioni mip in cui non sempre si riesce a distinguere il ridotto calibro della porzione stenotica del vaso dal segnale di fondo [ 7 ]  . 
1 occlusione dellarteria iliaca esterna sinistra ( freccia ) e stenosi in serie di entrambe le arterie femorali superficiali . an accurate evaluation of the arterial tree from the coeliac trunk to the foot arteries . 
in comparison with conventional angiography , mr offers important advantages in the study of elderly patients with peripheral arterial disease , enabling one to avoid the risks associated with arterial puncture , iodinated contrast material , and radiation . 
this effect increases in the mip reconstructions , in which it is not always possible to distinguish the reduced calibre of the stenotic portion of the vessel from the background signal [ 7 ]  . 
la causa principale della sottostima nei casi da noi esaminati stata data da effetti di volume parziale , anche in questo caso dovuti alla difficolt di rilevare attraverso strati sottili i ridotti calibri dei vasi stenotici [ 6 , 8 ]  . 
langio - rm si rivelata una metodica dotata di alta specificit , ma di inferiore sensibilit , quindi praticamente sovrapponibile alla dsa nella valutazione dei vasi di calibro regolare , mentre in caso di lesione steno - ostruttiva la dsa pi accurata , anche se nel nostro studio abbiamo rilevato una buona concordanza . nessuno dei pazienti ha avuto reazioni alla somministrazione della gadodiamide [ 9 ]  . 
non ci sono stati artefatti da materiale metallico in quanto un solo paziente aveva uno stent hemoban ( nitinolo ) in femorale superficiale destra che per non ha causato alterazioni del segnale . 
alcuni pazienti di questo studio , tutti arteriopatici allo stadio iii e iv di la fontaine ( tranne due ) , hanno avuto difficolt a tollerare limmobilit a causa del dolore , ma questo problema si presentato sia durante lesecuzione dellangio - rm sia durante la dsa . 
per quanto riguarda la sequenza tof , ha fornito una discreta valutazione dei vasi del piede , ma come tipo di sequenza mostra alcune limitazioni : i vasi non perfettamente perpendicolari al piano di acquisizione possono avere una bassa intensit di segnale e simulare una patologia [ 10 ] ; la pulsatilit del flusso pu produrre artefatti se non si utilizza un gating cardiaco ; il flusso retrogrado di alcuni vasi collaterali o ricostruiti pu essere anchesso saturato e mascherare di conseguenza il vero livello dellostruzione o sovrastimare la lunghezza del segmento stenotico [ 11 , 12 ]  . solo 15 dei pazienti esaminati ha potuto eseguire questo tipo di sequenza a causa dei gi citati problemi legati allimmobilit in posizione supina . 
mra proved to have higher specificity but lower sensitivity and is therefore practically identical to dsa in the evaluation of normal vessels ; however , in the case of steno - obstructive lesions , dsa is more accurate , even if we recorded a good agreement in our study . 
no patient had a reaction to gadodiamide [ 9 ]  . there were no artefacts due to metallic material , as only one patient had a hemoban stent ( nitinol ) in the right superficial femoral artery , which did not cause signal alterations . a non - negligible limitation of this examination is the immobility requested of the patient . 
some patients in our study , all but two with fontaine stage iii and iv disease , had difficulty keeping immobile because of pain , but this problem arose during both mra and dsa . as regards the tof sequence , despite providing a discrete evaluation of the foot vessels , it does suffer some limitations : vessels not perfectly perpendicular to the acquisition plane may have low signal intensity and simulate disease [ 10 ]  . flow pulsatility can produce artefacts if cardiac gating is not used . 
 the retrograde flow of some collateral or reconstructed vessels can also be saturated and disguise the true level of obstruction or overestimate the length of the stenotic segment [ 11 , 12 ]  . only 15 of our patients could be studied with this sequence because of difficulty lying motionless in the supine position . 
it does , however , have some limitations , some of which will be eliminated by technological advances with fast gradients and specific contrast agents for vascular studies whereas others will remamra may be proposed for selected indications : screening asymptomatic patients with a family history of diabetes or risk factors for atherosclerosis , patients with renal insufficiency , elderly patients , and for surveillance of bypass grafts . conclusions in our experience based on a limited number of patients , mra can be considered an alternative modality to dsa in the management of patients with steno - occlusive disease of the peripheral arteries , as it allows screening of candidates for interventional [ percutaneous angioplasty ( pta ) or stent ] or surgical procedures ( bypass graft )  . the pre - requisite for this is to optimise the injection time on the basis of each patients cardio - circulatory parameters , as also shown by westenberg et al . 
da quanto detto si evince che , nonostante la metodica si sia rivelata sicura , affidabile e sopportabile per la maggior parte dei pazienti , presenta pur sempre dei limiti , alcuni dei quali saranno eliminati dallavanzamento della tecnologia con gradienti ancora pi veloci e mezzi di contrasto dedicati allo studio vascolare , mentre altri invece resteranno invalicabili . 
tutto questo rende langio - rm un esame proponibile solo ad alcuni pazienti : screening nei pazienti asintomatici con familiarit diabetica o con fattori di rischio per aterosclerosi , insufficienza renale , pazienti anziani , controllo di bypass . conclusioni nella nostra esperienza , limitata al numero di casi da noi studiati , langio - rm pu essere considerata una metodica alternativa alla dsa nel management dei pazienti con patologia steno - ostruttiva del circolo arterioso periferico , selezionando i candidati a procedura interventistica ( pta o stent ) o chirurgica ( bypass )  . la condizione imprescindibile su cui si fonda questa affermazione lottimizzazione del tempo di iniezione ad ogni singolo paziente , in base ai suoi parametri cardio - circolatori come dimostrato anche da westenberg et al . 
conte3 1fisica sanitaria , 2radiologia , ospedale di circolo e fondazione macchi , viale borri 57 , i - 21100 varese , italy 3dipartimento di scienze cliniche e biologiche , universit dellinsubria , i - 21100 varese , italy correspondence to : s . 
la dose efficace media in un esame angio - tc varia da 18 , 8 msv a 28 , 8 msv , secondo il protocollo adottato . lottimizzazione ha portato alla stesura di una tabella che riporta i valori di corrente al tubo da utilizzare in funzione della corporatura del paziente in fase arteriosa . 
le procedure per esami angio - tc impartiscono dosi rilevanti al paziente ; tuttavia possibile ottenere una riduzione delle stesse senza influenzare la qualit dellimmagine . parole chiave tomografia computerizzata multistrato dose efficace introduction introduzione during the last few years , multislice computed tomography ( msct ) has spread rapidly and is now widely used as a diagnostic technique . 
 negli ultimi anni la tomografia computerizzata multistrato ( tcms ) si rapidamente diffusa nei differenti centri e ormai largamente impiegata come tecnica diagnostica , quindi necessario approfondire sia lottimizzazione dei protocolli di acquisizione , sia laspetto radioprotezionistico inevitabilmente collegato . 
assessment of the computed tomography dose index ( ctdiw ) was performed on polymethylmethacrylate ( pmma ) cylindrical phantoms with diameters of 1632 cstatistical data analysis was performed using the programme statistica 6.1 produced by statsoft , italia s.r.l. four different protocols used in angio - ct were considered : the thoracic aorta protocol , the thoracic - abdominal aorta protocol , the abdominal aorta protocol and the endoprosthesis protocol . 
each ct examination consisted of a digital projection radiograph ( topogram ) and two or three series ( baseline , arterial , venous ) , depending on the clinical query . 
the algorithm uses the monte carlo dosimetric data of the national radiological protection board ( nrpb ) , uk , described in the report sr250 [ 1 , 2 ]  . 
calculation of organ dose is based on the nctdiair value , measured on the scanners rotation axis and multiplied by an international commission on radiation units ( icru ) factor that provides soft - tissue dose di acquisizione , in modo tale da ridurre la dose al paziente , garantendo allo stesso tempo una buona qualit dellimmagine . 
lottimizzazione stata eseguita dapprima su un paziente di corporatura standard e in un secondo momento estesa a pazienti con differenti corporature . materiali e metodi il presente studio stato effettuato su un apparecchio lightspeed plus 4 - slice ct scanner ( general electric , milwaukee , wi , usa ) ; per le misure dosimetriche stato impiegato un elettrometro rti solidose 400 con camera a ionizzazione capintec pc4p da 10 cle valutazioni dellindice di dose in tomografia computerizzata ( ctdiw ) sono state eseguite con fantocci cilindrici in polimetilmetacrilato ( pmma ) da 16 cm e 32 cm di diametro . 
lanalisi statistica dei dati stata effettuata col programma statistica 6.1 prodotto da statsoft italia srl . sono stati considerati quattro differenti protocolli impiegati in esami angio - tc : protocollo aorta toracica , protocollo aorta toraco - addominale , protocollo aorta addominale , protocollo endoprotesi . 
ogni esame tc costituito da una proiezione digitale radiografica ( topogramma ) e da due o tre serie ( basale , arteriosa , venosa ) , secondo il quesito clinico . 
x - ray tube voltage is 120 kv , pitch is 1.5 and rotation time is 0.8 s for all protocols thoracic aorta abdominal - thoracic aorta abdominal aorta endoprosthesis 160 ; 184a ; 232 ; 240 5 ; 10 ; 20a 184a ; 240 5 ; 10 ; 15 ; 20a 160 ; 184a ; 224 10 ; 20a 184a ; 200 ; 224 ; 240 10 ; 15 ; 20a tube load , mas nominal beam collimation , mm aparameters relating to baseline series only tabella 1 parametri tecnici dei differenti protocolli di acquisizione . 
la tensione del tubo radiogeno di 120 kv , il pitch di 1 , 5 e il tempo di rotazione del tubo di 0 , 8 s per tutti i protocolli aorta toracica aorta toraco - addominale aorta addominale endoprotesi 160 ; 184a ; 232 ; 240 5 ; 10 ; 20a 184a ; 240 5 ; 10 ; 15 ; 20a 160 ; 184a ; 224 10 ; 20a 184a ; 200 ; 224 ; 240 10 ; 15 ; 20a carico del tubo , mas larghezza nominale del fascio , mm aparametri relativi solo alla serie basale s . 
dosimetric calculations were performed using the monte carlo data set number 19 ; for each patient , scan length and position were evaluated on the basis of the topogram . the arterial series of each protocol was optimised for a standard patient ( weighing 70 kg ) , following the procedure shown in figure 1 . 
during the arterial phase , a series was obtained with the minimum number of images on the liver ; parameters of additional series initially coincide with those of the clinical protocol . 
the process is repeated and allows identification of the lowest tube current value needed to obtain good image quality for each protocol . this value will correspond to the maximum acceptable image noise . 
in boones study , tube current values are adapted to the patients abdominal diameter ; fantoccio utilizzato per generare il data set permette la selezione interattiva del punto di inizio e di fine della scansione . il foglio di calcolo contiene una lista di nctdiair e nctdiw per specifici modelli di scanner in differenti condizioni ( ad esempio , tensione del tubo , collimazioni del fascio )  . 
il calcolo della dose al singolo organo basato sul valore di nctdiair , misurato sullasse di rotazione dello scanner , moltiplicato per un fattore icru che permette di ottenere la dose nei tessuti molli [ 3 ]  . 
la dose efficace in una serie ( dserie ) si ottiene sommando tutte le dosi agli organi , ciascuna moltiplicata per il relativo fattore di peso wt [ 4 ]  . 
i calcoli dosimetrici sono stati effettuati con il data set monte carlo numero 19 ; per ogni paziente la lunghezza e la posizione della scansione sono state valutate dal topogramma . la serie arteriosa di ogni singolo protocollo stata ottimizzata , per paziente standard ( peso 70 kg ) , seguendo la procedura descritta in figura 1 . 
se la serie di immagini giudicata di buona qualit quella sul paziente successioriginal protocol protocollo di acquisizione originale images on the liver immagini sul fegato noise evaluation image quality evaluation va lutazione rumore va lutazione qualit dellimmagine other patient lower ma altro paziente riduzione ma previous step noise and ma values are considered optimal considero rumore e ma del passo precedente come valori ottimali fig . 
 the equation that best interpolates the data is the following : deq = - 0.003 x weight2 + 0.58 x weight + 1.8 ( r2 = 0.809 ) where deq is the patients equivalent diameter , i.e. 
in boone [ 6 ] i valori di corrente al tubo vengono adattati al diametro addominale del paziente ; tale lavoro si riferisce a pazienti pediatrici , ma possibile estrapolare i dati per diametri maggiori . 
as before , the equivalent diameter is a function of the patients weight and is obtained experimentally . equation 2 shows that optimal tube load ( mas ) is a function of optimal noise value , of patient weight and of tube table 3 tube current values related to patient weight weight , kg tube current , ma tabella 3 valori di corrente al tubo da impostare in base al peso del paziente peso , kg corrente al tubo , ma dove : k una costante di proporzionalit ; = ( kv ) il coefficiente di attenuazione lineare a un dato valore di tensione del tubo , questo valore stato ricavato da [ 8 ] ; deq il diametro equivalente . 
come in precedenza il diametro equivalente funzione del peso del paziente ed ricavato sperimentalmente . dalla ( 2 ) si evidenzia che il valore ottimale di carico al tubo ( mas ) funzione del valore ottimale di rumore , del peso del paziente e della tensione al tubo attraverso il coefficiente di attenuazione  . in breve : rumore peso il valore ottimale di carico al tubo pu essere calcolato quindi dalla seguente formula : rumore peso peso dove k1 una costante di proporzionalit scelta in base ai valori relativi al paziente standard . 
il valore di carico al tubo determina automaticamente la corrente in ma poich il tempo di rotazione del tubo stato giudicato adeguato . risultati risultati delle valutazioni dosimetriche in tabella 2 sono riportati i valori di dose efficace per i differenti protocolli . 
la dose efficace media per una serie ( dserie ) effettuata con protocollo toracico pari a 14 , 9 msv , con protocollo toraco - addominale 9 , 4 msv , con protocollo addominale 10 , 9 msv e con protocollo endoprotesi 12 , 4 msv . la dose efficace media per un esame effettuato con protocollo toracico pari a 28 , 5 msv , con protocollo toraco - addominale 18 , 8 msv , con protocollo addominale 24 , 4 msv e con protocollo endoprotesi 28 , 8 msv . risultati dellottimizzazione i parametri di acquisizione della serie arteriosa dei protocolli angio - tc ottimizzati per un paziente standard sono i seguenti : tensione al tubo 120 kv ; tempo di rotazione 0 , 8 sec ; modalit spirale ; larghezza nominale del fascio 10 mm ; spessore di fetta 2 , 5 mm ; 15 mm / rot ; pitch 1 , 5 ; corrente al tubo 235 ma . 
tube load value automatically determines the current in ma because tube rotation time has been considered appropriate . 24 , 0 26 , 0 30 , 0 32 , 0 34 , 0 28 , 0 de q [ cm ] fig . 
 optimisation arterial series acquisition parameters of optimised angio - ct protocols for a standard patient are as follows : tube voltage 120 kv , rotation time 0.8 s , ; spiral acquisition , nominal beam width 10 mm , slice thickness 2.5 mm ; 15 mm / rotation , 1.5 pitch and tube current 235 ma . 
3 relazione tra rumore e diametro equivalente ( deq ) dopo la procedura di ottimizzazione . esame non ottimizzato aveva portato al valore di dose efficace media di 14 , 9 msv . 
la riduzione di dose ottenuta in fase arteriosa quindi dellordine del 45% . la figura 3 e la figura 4 riportano i dati di rumore e di diametro equivalente nel campione dei pazienti esaminati con protocollo ottimizzato e nel campione dei pazienti esas . 
dose reduction obtained during the arterial phase is therefore about 45% . figures 3 and 4 show noise and equivalent diameter values in the study patients examined using the optimised protocol and the original protocol , respectively . 
il test per la correlazione dei ranghi di spearman ha , infatti , dato un valore di r uguale a 0 , 43 nel caso del protocollo ottimizzato e a 0 , 86 nel caso del protocollo non ottimizzato . 
questo significa che il rumore ottenuto sulle immagini dipende dal diametro del paziente se i parametri di acquisizione non vengono adattati alle dimensioni del paziente , mentre questa correlazione viene persa nel caso del protocollo ottimizzato . 
sui grafici di figura 3 e figura 4 sono inoltre riportate le rette interpolanti i dati , che confermano come il rumore ( e quindi la qualit dellimmagine ) nel protocollo ottimizzato indipendente dal diametro del paziente ( r2 = 0 , 24 )  . 
la metodologia proposta di facile applicabilit e pu essere estesa anche ad altre tipologie di esame . secondo la tipologia di esame considerato , e del quesito clinico cui deve rispondere , il livello ottimale di rumore dellimmagine sar differente . 
cova1 1unit clinica operativa di radiologia , universit degli studi , ospedale di cattinara , strada di fiume , 447 , i - 34149 trieste , italy 2unit clinica operativa di neurologia , universit degli studi , ospedale di cattinara , trieste , italy 3brain center for neuroscience , trieste , italy 4dipartimento di fisica , universit degli studi di trieste , italy correspondence to : m . 
sono stati studiati 7 pazienti ( 6 di sesso maschile e 1 di sesso femminile ) affetti da una forma di morbo di parkinson lateralizzata acinetico - rigida , sottoposti ad un esame di risonanza magnetica funzionale . 
inoltre , stata riscontrata in alcuni casi lassenza di attivazione a livello delle aree premotoria e supplementare motoria ; quando invece presente , lattivazione era caratterizzata da intensit superiore durante il movimento della mano sana . 
le alterazioni osservate riflettono verosimilmente una riorganizzazione corticale secondaria al deficit sottocorticale allorigine della malattia . parole chiave risonanza magnetica risonanza magnetica funzionale encefalo morbo di parkinson introduction introduzione parkinsons disease is a neurological disorder characterised by progressive loss of dopaminergic neurons from the subcortical circuit of the basal nuclei , which presents clinically with four cardinal signs : tremor at rest , bradykinesia , rigidity and postural instability . 
the prevalence of the disease is approximately 120180 cases in 100 , 000 individuals per il morbo di parkinson un disordine neurologico caratterizzato da una progressiva perdita di neuroni dopaminergici del circuito sottocorticale dei nuclei della base e si manifesta clinicamente con quattro segni cardinali : tremore a riposo , bradicinesia , rigidit ed instabilit posturale . 
the diagnosis is mainly clinical although morphologicalfunctional brain imaging , with both radiological and nuclear medicine techniques , may be of particular assistance despite the lack of specificity and the variability of imaging signs . although the disease has always been considered to affect subcortical ganglia , the effects of dopamine depletion are widespread and also involve non - dopaminergic neurons in areas of the brain crucial for motor control . only a few published reports have investigated functional magnetic resonance imaging ( mri ) in the assessment of cortical activation in patients with parkinsons disease . 
in particular , the studies focused on cortical activation during simple motor tasks , prevalently evaluating the primary sensory - motor area , the supplementary motor area and the pre - motor area , with only limited information on parietal lobes . 
this study aimed to assess cortical activation patterns with functional mri in patients with lateralised parkinsons disease during a relatively complex motor task in order to better understand pathophysiological mechanisms of the disease and detect possible clinical effects of functional mri on these subjects . materials and methods this study assessed two groups of subjects : the first included 11 healthy volunteers ( six men and five women ) aged between 23 and 37 with no neurological disease ; the second consisted of seven patients ( six men and one woman ) aged between 56 and 82 years with parkinsons disease . 
 patients were receiving a mean l - dopa dose of 42064.54 mg / day , and none of them was taking dopamine agonists : all were continuing their normal work activities . both the healthy volunteers and patients received adequate information about the functional study , which they underwent only after giving their consent . 
volunteers were univocally identified by a number : numbers from 1 to 7 identified lanno nella popolazione caucasica [ 1 ] , ma considerando la prevalenza nei soggetti di oltre 65 anni di et si arriva all1% e al 2% oltre gli 80 anni . leziologia multifattoriale , in particolare correlata sia a fattori genetici che ambientali . 
la diagnosi principalmente clinica , anche se le metodiche di imaging cerebrale morfo - funzionale , sia radiologiche che di medicina nucleare , possono fornire un notevole ausilio nonostante lestrema aspecificit ed incostanza dei segni riscontrabili . 
nonostante tale patologia sia sempre stata considerata di pertinenza ganglionare , nettamente sottocorticale , gli effetti della perdita di dopamina sono diffusi e coinvolgono anche i neuroni non - dopaminergici in regioni encefaliche che costituiscono elementi cruciali per il controllo motorio . 
in letteratura sono stati pubblicati pochi lavori riguardanti lattivazione corticale valutata con risonanza ( rm ) funzionale in pazienti affetti da morbo di parkinson . in particolare , in questi studi stata posta lattenzione sullattivazione corticale durante lesecuzione di compiti motori semplici , valutando prevalentemente larea sensitivo - motoria primaria , larea supplementare motoria e larea premotoria , con solo pochi dati riguardanti i lobi parietali . con questo studio abbiamo voluto valutare i pattern di attivazione corticale in rm funzionale in soggetti affetti da morbo di parkinson lateralizzato durante lo svolgimento di un compito motorio relativamente complesso con lobiettivo di comprendere meglio i meccanismi fisiopatologici di tale malattia ed in secondo luogo di ricavare una possibile ricaduta clinica della rm funzionale in questi soggetti . materiali e metodi in questo studio sono stati valutati due gruppi di soggetti : il primo comprendeva 11 volontari sani ( 6 maschi e 5 femmine ) di et compresa tra i 23 ed i 37 anni , non affetti da patologie neurologiche , mentre il secondo gruppo comprendeva sette pazienti ( 6 maschi e 1 femmina ) di et compresa tra i 56 e gli 82 anni , affetti da morbo di parkinson . 
tutti i pazienti presentavano una sindrome ad esordio asimmetrico , acinetico - rigida , ipertonica , atremorigena cui si associava una bradicinesia importante ed ipomimia : il tempo medio di diagnosi di malattia di parkinson era di 12 , 82 , 37 mesi . nella tabella 1 sono riportate le caratteristiche di lateralizzazione riscontrate clinicamente per ciascun paziente . 
i pazienti assumevano una quantit di l - dopa media di 42064 , 54 mg / die e nessuno era in terapia con farmaci dotable 1 lateralisation detected clinically in each patient with parkinsons disease tabella 1 lateralizzazione riscontrata clinicamente in ciascun paziente affetto da morbo di parkinson patient lateralisation paziente lateralizzazione right left right right left right left destra sinistra destra destra sinistra destra sinistra m . 
lattivazione viene espressa in variazione percentuale del contrasto bold tra fase di attivazione e di riposo soggetto no . mano destra mano sinistra m1 omolaterale m1 controlaterale m1 omolaterale m1 controlaterale the healthy volunteers who performed the motor task with both hands , volunteers 810 performed it with their right hand only whereas volunteer 11 performed it with the left hand only . 
likewise , parkinsons disease patients were identified by a progressive number from 1 to 7 , and all performed the motor task with both hands . the examinations were conducted on a standard clinical mri unit with a 1.5 - t intera master super - conductive magnet ( philips , gyroscan intera 1.5 t master , best , the netherlands )  . 
an echo planar fast field echo ( ffe ) sequence ( tr / te : 3 , 200 / 45 ms , slice thickness 4 mm , gap 0 , fov 200 mm , matrix 64x64 ) was used for functional acquisition , with evaluation of cortical activation exploiting the blood oxygen level dependent ( bold ) contrast . finger tapping was selected as the activation test : in this test , the subject is asked to tap the thumb on the pulp of each of the other fingers in turn , and then start over again particular , during the whole sequence , made up of 150 trs lasting a total of 8 min , the subject was asked to alternate a phase of rest and a phase of activity for three consecutive times with the same hand . 
in particular , we chose an inversion recovery sequence ( tr / te / ti : 1 , 786 / 15 / 350 ) characterised by fov , slice thickness and gaps similar to those used for the functional sepaminoagonisti : tutti continuavano la loro normale attivit lavorativa . 
i volontari sono stati individuati univocamente da un numero : i numeri da 1 a 7 individuano i volontari sani che hanno eseguito il compito motorio con entrambe le mani , i volontari 8 , 9 , 10 con la sola mano destra mentre il volontario 11 con la sola mano sinistra . 
 gli esami sono stati condotti su un tomografo clinico standard dotato di un magnete superconduttivo da 1 , 5 t ( philips , gyroscan intera 1 , 5 t master , best , olanda )  . 
per lacquisizione funzionale stata utilizzata una sequenza echo planar ffe ( tr / te : 3200 / 45 ms , spessore di strato = 4 mm , gap = 0 , fov = 200 mm , matrice 64x64 ) , con valutazione dellattivazione corticale sfruttando il contrasto bold ( blood oxygen level dependent )  . 
per quanto riguarda la prova di attivazione stato scelto il finger tapping : cio stato chiesto al soggetto di toccare con il polpastrello del primo dito , in successione , il polpastrello del secondo , terzo , quarto e quinto dito e , quindi , ricominciare da capo . 
activation is expressed as a percentage change of the blood oxygen level dependent ( bold ) contrast between activity and rest phases tabella 3 risultati relativi allattivazione dellarea motoria supplementare e dellarea premotoria nei volontari sani : confronto tra movimento della mano destra e sinistra . 
activation is expressed as a percentage change of the blood oxygen level dependent ( bold ) contrast between activity and rest phases subject no . affected hand healthy hand m1 ipsilateral m1 contralateral m1 ipsilateral m1 contralateral tabella 5 risultati relativi allattivazione dellarea motoria primaria ( m1 ) nei pazienti parkinsoniani : confronto tra movimento della mano sana e della mano malata . 
a p value of 0.01 was considered to indicate statistical significance . in all subjects , the presence or absence of activation was evaluated at the level of the primary motor area , the pre - motor area and supplementary motor area of the parietal and occipital lobes . 
each area was studied as a cluster if voxels were contiguous and made the structure identifiable or as a spherical volume if the voxels were separate but could be related to the same brodmann area . 
graphically , pixels corresponding to cortical activation were overlaid onto the anatomic sequence to enable more accurate localisation . results tables 2 , 3 and 4 show numerical results for each healthy volunteer and each area . 
in all patients considered , we observed activation of the primary motor area contralateral la durata complessiva di 8 minuti , stato chiesto al soggetto di alternare una fase di riposo ad una fase di attivit e questo per tre volte consecutive con la stessa mano . 
successivamente stata acquisita una sequenza anatomica , in particolare abbiamo scelto una sequenza inversion recovery ( tr / te / ti = 1786 / 15 / 350 ) caratterizzata da fov , spessore di strato e gap analoghi a quelli utilizzati per la sequenza funzionale . 
in tutti i soggetti stata valutata la presenza o assenza di attivazione in corrispondenza dellarea motoria primaria , dellarea premotoria e supplementare motoria , dei lobi parietali e dei lobi occipitali . 
ciascuna area stata studiata come cluster , se i voxels erano contigui e dunque rendevano individuabile la struttura , oppure come volume sferico , se i voxels erano separati , ma riconducibili alla stessa area di brodmann . 
da un punto di vista grafico i pixels relativi allattivazione corticale sono stati sovrapposti alla sequenza anatomica , di modo da consentire una loro pi corretta localizzazione . risultati nelle tabelle 2 , 3 e 4 sono riportati i risultati numerici relam . 
intensity of the activation signal was higher , on average , in the primary motor area contralateral to the moving hand , as compared with the ipsilateral primary motor area . 
signal intensity of the primary ipsilateral and contralateral motor areas was higher during movement of the affected hand as compared with the healthy tivi a ciascun volontario sano e ciascuna area . 
accanto a queste attivazioni stata rilevata unattivazione a livello dellarea motoria omolaterale e a livello dei lobi parietali . nelle tabelle 5 , 6 e 7 sono riportati i risultati relativi ai pazienti parkinsoniani . 
in tutti i pazienti studiati stata osservata la presenza di attivazione in corrispondenza dellarea motoria primaria controlateralmente al lato in esame e in 6 pazienti su 7 lattivazione delle aree motoria supplementare e premotoria . table 6 results concerning activation of the supplementary motor area and pre - motor area in parkinsons patients : comparison between movement of the healthy hand and affected hand . 
activation is expressed as a percentage change of the blood oxygen level dependent ( bold ) contrast between activity and rest phases tabella 6 risultati relativi allattivazione dellarea motoria supplementare e dellarea premotoria nei pazienti parkinsoniani : confronto tra movimento della mano sana e della mano malata . 
activation of the supplementary motor and pre - motor areas was observed in six patients out of seven during movement of the healthy hand and in five patients out of seven during movement of the affected hand . 
in the remaining two cases , activation of the parietal cortex ipsilateral to the moving hand and activation of the parietal cortex were observed , respectively , bilaterally when the task was performed with the healthy hand , and contralateral when performed with the affected hand . 
the disease has always been regarded as gangliar and subcortical , but , despite the neurochemical lesion being mainly located in the nigrostriatal dopaminergic system , the effects of dopamine depletion are widespread and also affect neuronal pathways that are not strictly dopaminergic but more like bridges to areas of the brain crucial for motor control [ 3 ]  . 
with this study , we aimed at evaluating cortical acaccanto a queste attivazioni stata rilevata unattivazione a livello dellarea motoria omolaterale al movimento , della corteccia parietale e della corteccia occipitale . il segnale proveniente dallarea motoria primaria omolaterale stato osservato in 5 pazienti su 7 durante il movimento della mano sana e in 6 pazienti su 7 durante il movimento della mano malata : lintensit del segnale di attivazione mediamente maggiore in corrispondenza dellarea motoria primaria controlaterale alla mano in movimento rispetto allarea motoria primaria omolaterale . 
nei restanti due casi stata osservata rispettivamente unattivazione della corteccia parietale omolaterale alla mano in movimento e lattivazione della corteccia parietale bilateralmente quando il compito stato svolto con la mano sana e controlateralmente se stato svolto con la mano malata . 
tale affezione sempre stata considerata di pertinenza ganglionare , nettamente sottocorticale ma , anche se la lesione neurochimica localizzata prevalentemente a livello del sistema dopaminergico nigrostriatale , gli effetti della perdita di dopamina sono diffusi e coinvolgono vie neuronali anche non strettamente dopaminergiche , trait - dunion con regioni encefaliche cruciali per il controllo motorio [ 3 ]  . 
con questo studio , pertanto , abbiamo voluto valutare le caratteristiche dellattivazione corticale in soggetti affetti da morbo di parkinson durante lo svolgimento di un compito motorio relativamente complesso , confrontandole con quelle osservate in un gruppo di controllo costituito da volontari sani e , avendo i pazienti un morbo di parkinson lateralizzato , stato possibile effettuare un confronto tra le attivazioni ottenute con la mano sana e quella malata . in condizioni normali , con il semplice finger tapping , si osserva lattivazione della corteccia pree post - rolandica controlaterale , legate , la prima al movimento della mano , la seconda principalmente al contatto intrinseco interfalangeo . spesso si riconosce inoltre lattivazione in sede frontale delle aree supplementare motoria e premotoria : generalmente lattivazione dellarea motoria supplementare si distingue in una parte anteriore bilaterale simmetrica ed una posteriore , controlateralmente alla mano che esegue il compito motorio fig . 
2 marcata attivazione bilaterale della corteccia parietale durante il movimento della mano malata . tivation characteristics in patients with parkinsons disease during a relatively complex motor task , comparing them with those observed in a control group consisting of healthy volunteers . 
under normal conditions , simple finger tapping activates the preand post - rolandic contralateral cortex , the former being linked to hand movement , the latter mainly to intrinsic contact between phalanges . 
furthermore , frontal activation of the supplementary motor and pre - motor areas is often detected : activation of the supplementary motor area is generally subdivided into a symmetrical , bilateral , anterior portion and a posterior portion , contralateral to the hand performing the motor task [ 4 ]  . 
in healthy volunteers , the expected activation pattern was confirmed , but other areas were also activated , in particular , the ipsilateral primary motor cortex and the parietal cortex . activation corresponding to the primary motor cortex ipsilateral to the moving hand is neurologically justified by the partial hemilateral non - specificity of motor operations . 
when the task becomes slightly more complex and sequential , as with finger tapping , the ipsilateral primary motor cortex and parietal lobes , which are involved in the perception of movement in space , are also activated [ 6 ]  . before evaluating the results obtained in parkinsons patients , it should be noted that any differences between patients and healthy volunteers might be related not only to the disease but also to age . 
in this respect , it is important to note that the healthy volunteers age range was 2337 years whereas patients age range was 5682 years and that there were no functional mri investigations of brain activation induced by finger tapping performed under the same conditions by healthy subjects of different ages . 
nonetheless , the only published study contrasting the extent of activation of primary motor areas during a motor task , as assessed by spectroscopy in subjects of different ages , showed no statistically significant difference in activation among the different age groups [ 7 ]  . 
this hyperactivity of the contralateral primary motor area has already been described in the literature [ 8 , 9 ] and could represent the neural substrate for the difficulty experienced by the patient with parkinsons disease to perform the movement . 
it could therefore be assumed that this hyperactivity reflects the cortical re - organisation , which compensates for the subcortical deficit causing the disease . activation of the primary motor cortex ipsilateral to the hand examined has been also observed in parkinsons patients , but [ 4 ]  . 
nei volontari sani stato confermato il pattern di attivazione atteso , ma stata rilevata unattivazione a livello di altre aree , in particolare a livello della corteccia motoria primaria ipsilaterale e della corteccia parietale . la presenza di attivazione in corrispondenza della corteccia motoria primaria omolaterale alla mano in movimento giustificata , neurologicamente , dalla parziale aspecificit emilaterale delle operazioni motorie : infatti , a ciascuna mano sono affidate differenti abilit e le istruzioni per eseguire un determinato movimento possono in parte risiedere nelluno o nellaltro emisfero ed essere richiamate con la stessa modalit che implica lattivazione dellarea motoria supplementare . 
ovviamente , essendo ridotto il feed - back tattile , il segnale omolaterale riguarda la sola area rolandica deputata al controllo del movimento [ 5 ]  . altra ipotesi per spiegare tale attivazione legata al tipo di compito motorio : nel caso di un movimento molto semplice ( ad es . , apertura e chiusura della mano ) si osserva generalmente lattivazione della sola area motoria primaria controlaterale . 
quando il compito diviene modestamente pi complesso e sequenziale , come accade con il finger tapping , si pu osservare lattivazione anche della corteccia motoria primaria omolaterale e dei lobi parietali , che sono coinvolti nella percezione del movimento nello spazio [ 6 ]  . prima di valutare i risultati ottenuti nei pazienti parkinsoniani , va sottolineato come eventuali differenze rispetto ai volontari sani potrebbero essere legate non solo alla malattia , ma anche al fattore et . 
riguardo a questultimo aspetto , va ricordato come la fascia det dei volontari sani sia 2337 anni , mentre quella dei pazienti 5682 anni e come non esistano in letteratura studi di rm funzionale sullattivazione cerebrale indotta da finger tapping , eseguito nelle medesime condizioni da soggetti sani , ma di et diverse . 
va comunque sottolineato come lunico lavoro pubblicato , nel quale stata messa a confronto lentit di attivazione delle aree motorie primarie durante un compito motorio , valutata con spettroscopia , in soggetti di diverse fasce di et , non ha dimostrato una differenza di attivazione statisticamente significativa tra i diversi gruppi [ 7 ]  . 
in tutti i parkinsoniani stata osservata la presenza dellattivazione della corteccia motoria primaria controlateralmente alla mano in esame . ma , mediamente , a tale livello lintensit di segnale superiore rispetto a quanto osservato nei volontari sani : questa iperattivit dellarea motoria primaria controlaterale gi stata descritta in letteratura [ 8 , 9 ] e potrebbe rappresentare il substrato neurale della difficolt del paziente con morbo di parkinson nellesecuzione del movimento . 
moreover , taking into account the hemispheric dominance and equal distribution of parkinsons disease between the dominant and non - dominant hand , the correlation between observations and the disease seems plausible . 
 an explanation of our results might be that there is a recovery of the activity of the ipsilateral motor cortex , compensating for the contralateral deficit , as demonstrated by two positron emission tomography ( pet ) studies on patients with central , lateralised and ischaemic deficits [ 10 , 11 ]  . 
in addition to the contralateral motor cortex , the ipsilateral cortex appears to undergo a process of compensatory functional re - organisation . another phenomenon has been described that could account for this asymmetry in activation , which is also seen in subjects with motor deficits : the presence of associated movement of the hand contralateral to the one being studied [ 12 ]  . 
although this was not done in our study , we did carefully monitor the subjects visually during image acquisition , and no movement of the contralateral hand in either volunteers or patients was detected . as regards activation of the supplementary motor and premotor cortices , these were activated in six parkinsonian patients , with asymmetric activation ( more intensely during the movement of the healthy hand )  . 
this could be explained by the speed of movement . a recent study observed that the intensity of activation of the pre - motor and supplementary motor areas in healthy volunteers is directly proportional to the speed of the hand movement [ 2 ]  . 
this aspect has already been observed in the literature [ 2 , 79 ] and is explained in the following manner : the parietal cortex integrates different sensory , motivational and attentional inputs and can therefore provide the basis for the generation of sensory - guided movements in parkinsons patients without requiring circuitry between the basal ganglia and frontal cortex , which are altered in these patients . as a consequence , hyperactivity of the parietal lobes , along with activation of the pre - motor and supplementary motor areas , would be a compensatory mechanism for the hypoactivity of striatofrontal projections , thus creating an intact alternative pre - motorparietal circuit . 
in this respect , we found no difference in the activation of the parietal lobes between movement of the affected and healthy hands in parkinsons patients , and this suggests that these alterations entrambe le mani . 
inoltre , tenendo conto della dominanza emisferica , e dellequa distribuzione del morbo di parkinson , alla mano dominante e non , la correlazione possibile tra quanto osservato e la patologia sembra plausibile . 
una spiegazione dei nostri risultati pu essere data dal fatto che vi sia un recupero dellattivit della corteccia motoria ipsilaterale , compensatoria al deficit controlaterale , come dimostrato in due studi eseguiti con tecnica pet su pazienti con deficit centrale , lateralizzato , ischemico [ 10 , 11 ]  . 
in letteratura stato descritto un ulteriore fenomeno che potrebbe essere alla base di questa asimmetria di attivazione che presente anche nei soggetti con deficit motorio : la presenza di movimento associato della mano opposta a quella in esame [ 12 ]  . 
esso non ha messo in evidenza movimenti della mano controlaterale , n nei volontari , n nei parkinsoniani . riguardo allattivazione delle cortecce motoria supplementare e premotoria , nei parkinsoniani si dimostrata la loro attivazione in sei casi , con attivazione asimmetrica ( maggiore intensit di attivazione durante il movimento della mano sana )  . 
in un recente studio si osservato come in volontari sani lintensit di attivazione delle aree premotoria e supplementare motoria sia direttamente proporzionale alla velocit del movimento della mano [ 2 ]  . 
questo aspetto gi stato osservato in letteratura [ 2 , 79 ] ed giustificato dal fatto che la corteccia parietale viene ritenuta un integratore di diversi input sensitivi , motivazionali ed attenzionali che possa pertanto fornire le basi per la genesi di movimenti guidati da stimoli sensoriali nei pazienti affetti da morbo di parkinson senza la necessit dei circuiti tra gangli della base e corteccia frontale , che sono alterati in questi pazienti . 
pertanto liperattivazione dei lobi parietali , insieme allattivazione delle aree premotoria e supplementare motoria , rappresenterebbe un meccanismo di compenso per lipofunzione delle proiezioni striato - frontali , creando un circuito alternativo integro premotorio - parietale . 
a tale riguardo , non abbiamo rilevato una differenza di attivazione dei lobi parietali tra movimento della mano malata e movimento della mano sana nei parkinsoniani , e questo suggerisce come tali alterazioni possano essere rilevabili anche in una fase preclinica . 
another hypothesis is that the impairment of the connections between basal nuclei and cortex , responsible for parietal cortical hyperactivity , changes the perception of movement in space in patients during the movement of both the healthy and affected hands . another observation concerns the activation of the occipital lobes . 
this was absent in healthy volunteers . these results are certainly interesting from a neuropathological point of view but might also have clinical relevance , in particular , in the differential diagnosis between the different types of parkinsonism , and suggest an anatomical - physiological basis for the rehabilitation of these patients . 
more precisely , functional mri could be used in the differential diagnosis of parkinsons disease and cortico - basal degeneration , which has been shown to have a different activation pattern [ 13 ]  . 
consequently , the technique could be useful in the initial stages of the disease , when the cortico - basal degeneration may be impossible to distinguish clinically from parkinsons disease although the therapeutic approach and prognosis are completely different . the main limitation of our study , shared by all studies of this kind , concerns the small number of patients studied , which precludes a statistical analysis of the results . 
however , the problems in finding patients with a lateralised akineticrigid form of parkinsons who can endure a functional mri examination should be considered . rattivit corticale parietale , determini nei pazienti una alterata percezione del movimento nello spazio , presente sia durante il movimento della mano sana che della mano malata . altra osservazione quella relativa allattivazione dei lobi occipitali : un primo commento riguarda il fatto che non stato chiesto n ai volontari sani n ai pazienti di tenere gli occhi chiusi durante lacquisizione delle immagini . 
questa spiegazione trova ulteriore conferma dallosservazione sperimentale della presenza di ampi movimenti del capo nei parkinsoniani allinizio del compito motorio , movimenti eseguiti involontariamente per permettere il controllo visivo del movimento . conclusioni con questo lavoro abbiamo descritto i patterns di attivazione corticale durante un compito motorio in pazienti affetti da morbo di parkinson lateralizzato confrontandoli con quelli nei volontari sani e inoltre , nellambito dello stesso paziente , abbiamo confrontato lattivazione ottenuta con la mano sana con quella della mano malata . 
inoltre stata riscontrata , in alcuni casi , lassenza di attivazione a livello delle aree premotoria e supplementare motoria , verosimilmente secondarie allimpaccio motorio . dove , invece , tali zone si attivavano lo facevano con intensit superiore durante il movimento della mano sana . 
infine , si osservata una spiccata tendenza di questi pazienti al controllo visivo del movimento con conseguente attivazione dei lobi occipitali , assente nei volontari sani . questi risultati sono sicuramente interessanti da un punto di vista neurofisiopatologico , ma potrebbero anche rivestire un ruolo nellambito clinico , in particolare nella diagnosi differenziale tra i diversi parkinsonismi e suggerire una base anatomo - fisiologica per il recupero fisiatrico di questi pazienti . 
pi precisamente la rm funzionale potrebbe essere impiegata nella diagnosi differenziale tra morbo di parkinson e degenerazione cortico - basale , nella quale si dimostrato un diverso pattern di attivazione [ 13 ]  . 
pertanto tale tecnica potrebbe risultare utile nelle fasi iniziali di malattia , quando la degenerazione cortico - basale pu essere clinicamente indistinguibile dal morbo di parkinson , ma il suo approccio terapeutico e la prognosi sono completamente diverse . il principale limite del nostro lavoro , comune a tutti i lavori simili pubblicati , riguarda la non elevata numerosit dei pazienti che non consente una valutazione statistica dei risultati . 
simonetti dipartimento di diagnostica per immagini e radiologia interventistica , universit di roma tor vergata , policlinico , viale oxford 81 , i - 00133 rome , italy correspondence to : e . 
magnetic resonance imaging ( mri ) and mrsi were performed on 39 patients with prostate - specific antigen ( psa ) levels greater than 4 ng / ml and suspicious findings at trans - rectal ultrasound ( trus )  . 
at mrsi , cancer was defined as possible if the ratio of choline plus creatine to citrate exceeded mean normal peripheral zone values by two standard deviations ( sd ) or as definite if that ratio exceeded the normal value by three sd . 
mri and mrsi alone had sensitivity , specificity , positive and negative predictive values and diagnostic accuracy in the detection of prostate cancer equal to 85% , 75% ; 53% , 89% ; 65% , 88% ; 77% , 74% ; and 69% , 79% , respectively . 
trentanove pazienti con valori di antigene specifico prostatico ( psa ) superiori a 4 ng / ml e reperti sospetti allecografia transrettale ( trus ) sono stati sottoposti ad imaging morfologico con risonanza magnetica ( rm ) e a rmsp . 
alla rmsp la presenza di tumore stata definita come possibile se il rapporto tra colina pi creatina su citrato era maggiore di 2 ds rispetto al valore medio della zona periferica normale o certa se tale rapporto superava di 3 ds quello normale . 
la rm e la rmsp singolarmente hanno evidenziato sensibilit , specificit , valore predittivo positivo e negativo e accuratezza diagnostica per lindividuazione del cancro prostatico del 85% , 75% e 53% , 89% e 65% , 88% e 77% , 74% e 69% , 79% rispettivamente . 
laggiunta della rmsp alla rm permette una significativa pi alta specificit nellindividuazione del tumore rispetto alla sola rm e pu essere indicata come modalit risolutiva prima della biopsia nei pazienti con elevati valori di psa ed ecografia transrettale ( trus ) sospetta . key words prostate prostatic neoplasm biopsy magnetic resonance imaging magnetic resonance spectroscopy imaging parole chiave prostata neoplasia prostatica biopsia risonanza magnetica spettroscopia con risonanza magnetica introduction introduzione the growing incidence of prostate cancer , together with an increasing ageing population in the western world , has made prostate tumour an acute medical and socioeconomic problein 2004 in the united states , the american cancer society estimated 230 , 000 new cases of prostate carcinoma as well as 29 , 900 cases of deaths related to this disease [ 1 ]  . screening with digital rectal examination associated with evaluation of serum prostate - specific antigen ( psa ) and trans - rectal ultrasound ( trus ) , possibly complemented by biopsy [ 2 ] , has enabled physicians to identify cancers at an earlier stage than in the past , drawing attention to the possibility of using treatments ( brachytherapy , radiotherapy , thermoablation and cryosurgery ) that have less aggressiveness and morbidity than radical prostatectomy . hence , locating and staging the cancer accurately as well as assessing its biological aggressiveness have become crucial . magnetic resonance imaging ( mri ) improves the evaluation of zonal morphology and prostate anatomy although there is still no agreement over diagnostic accuracy of mri in identifying prostate cancer lesions . studies conducted to date have shown extreme variations in accuracy levels , with values ranging from 75% to 90% , with peaks of 97% [ 3 ] in locating known lesions , but showing a remarkable drop with lesions < 5 mm [ 4 ]  . 
however , morphologic evaluation alone had poor specificity ( 55% ) [ 5 ] because of a high number of false positives . these can be attributed to several conditions ( post - biopsy haemorrhage , the effects of conservative treatments ) or diseases ( prostatitis ) affecting the prostate tissue , which can mimic cancer and its typical t2 appearance as an area of low signal intensity against a background of relatively hyperintense normal peripheral zone . 
the introduction of proton mr spectroscopic imaging ( mrsi ) has enabled direct correlation of anatomical and morphological findings with functional information on tissue metabolism . initial studies show the potential of combined mri and mrsi in determining the presence of prostate cancer with higher accuracy , view its extension and estimate its biological aggressiveness [ 6 ]  . 
therefore , the purpose of our study was to compare the diagnostic performance of mrsi and morphological imaging alone in the identification and localisation of prostate tumours by comparing it prospectively with histopathologic findings . materials and methods patients between april and october 2004 , 39 patients underwent , after giving informed consent , mri of the prostate with associated spectroscopic evaluation at our department . 
lamerican cancer society ha stimato negli stati uniti , nel 2004 , 230.000 nuovi casi di carcinoma prostatico e 29.900 casi di decesso ad esso correlati [ 1 ]  . 
lo screening con esplorazione digito - rettale associato alla valutazione dellantigene prostatico specifico ( psa ) sierico e allo studio con ecografia transrettale ( trus ) , eventualmente completato dalla biopsia [ 2 ] ha consentito lindividuazione delle neoplasie ad uno stadio pi precoce rispetto al passato , richiamando inoltre lattenzione sulla possibilit di utilizzare degli strumenti terapeutici ( brachiterapia , radioterapia , termoablazione e criochirurgia ) meno aggressivi e gravati da minore morbilit rispetto alla prostatectomia radicale . 
diviene in tal modo di fondamentale importanza la precisa localizzazione e stadiazione della neoplasia e la valutazione della sua aggressivit biologica . limaging con risonanza magnetica ( rm ) consente una migliore valutazione della morfologia e dellanatomia zonale della prostata sebbene riguardo al valore di accuratezza diagnostica della rm nellidentificazione delle lesioni prostatiche neoplastiche non vi sia ancora accordo tra i vari autori . 
gli studi finora effettuati hanno mostrato unampia variabilit dei risultati di accuratezza con valori che vanno dal 75% al 90% , raggiungendo il 97% [ 3 ] nella localizzazione di lesioni gi note , ma mostrando una sensibile flessione per lesioni di diametro inferiore ai 5 mm [ 4 ]  . 
la sola valutazione morfologica , per , si rilevata scarsamente specifica ( 55% ) [ 5 ] , a causa di un elevato numero di falsi positivi , i quali possono essere attribuiti alla presenza di alcune condizioni ( emorragia post - bioptica , effetti delle terapie conservative ) o patologie ( prostatiti ) che interessano il tessuto prostatico e che sono in grado di mimare la lesione neoplastica con il tipico aspetto di area a bassa intensit di segnale nelle sequenze t2 pesate nel contesto della relativa iperintensit della zona periferica normale . lintroduzione della spettroscopia dellidrogeno con rm ( rmsp ) ha permesso di correlare il dato anatomico e morfologico direttamente con informazioni di tipo funzionale relative al metabolismo tissutale . 
studi iniziali mostrano la potenzialit della combinazione del rm e rmsp nel determinare in maniera pi accurata la presenza del carcinoma prostatico , visualizzarne lestensione e stimarne laggressivit biologica [ 6 ]  . 
lo scopo del nostro studio stato , pertanto , verificare la performance diagnostica della spettroscopia dellidrogeno rispetto al solo imaging morfologico nella individuazione e localizzazione della patologia tumorale prostatica , confrontandola prospetticamente con il dato istopatologico . materiali e metodi pazienti da aprile ad ottobre 2004 , 39 pazienti si sono recati presso il nostro dipartimento per essere sottoposti , previo consenso g . 
for the morphological study , t2 - weighted turbo spin echo ( tse ) images with high spatial resolution were acquired in the transverse plane ( using the spir fat - suppression technique as well ) and in the coronal plane , including the entire prostate and seminal vesicles in the acquisition volume . 
acquisition parameters were the following : tr 4 , 000 ms , te 130 ms ( tr 4 , 750 ms , te 90 ms in the spir sequence ) , 2.5 - mm slice thickness without gap between the slices , four excitations , 190 mm field of view ( fov ) and acquisition and reconstruction matrices of 240 and 256 , respectively . the morphological study was completed with the acquisition of ten t1 - weighted fast - field echo ( ffe ) spir post - contrast dynamic sequences ( tr 20 ms , te 5 m , 20 flip angle , 3 - mm slice thickness )  . the volume to be studied by spectroscopy was selected on the basis of the axial t2 morphological images , trying to include the prostate parenchyma and exclude as much periglandular fat as possible . 
to this end , a double spin - echo point - resolved spatially localized spectroscopic ( press ) sequence was used , along with a te ( 136 ms ) optimised for quantitative evaluation of citrate and choline with multivoxel analysis . 
let media dei pazienti esaminati di 68 , 5 aa ( range 5582 anni ) con un valore medio di psa sierico di 24 , 15 ng / ml ( range 4 , 344 ng / ml )  . tecnica rm le immagini sono state acquisite con unapparecchiatura ad elevata intensit di campo ( 1 , 5 t ) ( philips gyroscan intera , best , netherlands ) equipaggiata con gradienti da 30 mt / m , utilizzando la bobina del corpo per la trasmissione degli impulsi e una bobina di superficie ( c1 ) , posizionata a livello della pelvi , per la ricezione del segnale . 
allo scopo di ridurre la motilit intestinale e migliorare cos la qualit delle immagini sono stati somministrati per via i.glucagone o nbutilbromuro di ioscina ( buscopan fl 20 mg / ml )  . 
per lo studio morfologico sono state acquisite immagini tse t2 pesate ad alta risoluzione spaziale sul piano trasversale ( utilizzando anche la tecnica della soppressione del grasso spir ) e su quello coronale includendo nel volume dacquisizione lintera prostata e le vescicole seminali . 
i parametri di acquisizione sono stati i seguenti : tr 4000 ms , te 130 ms ( tr 4750 ms , te 90 ms nella sequenza spir ) , spessore di sezione 2 , 5 mm senza intervallo tra le sezioni , 4 eccitazioni , fov di 190 mm e una matrice di acquisizione e di ricostruzione rispettivamente di 240 e 256 . 
lo studio morfologico stato completato con lacquisizione di 10 sequenze dinamiche post - contrastografiche ffe t1w spir ( tr 20 msec , te 5 msec , flip angle 20 , spessore di sezione 3 mm )  . il volume sottoposto ad analisi spettroscopica stato selezionato , sulla base delle immagini assiali t2 morfologiche , cercando di includere il parenchima prostatico e di escludere il pi possibile il grasso perighiandolare . 
a tal fine stata utilizzata una sequenza press ( double spin - echo point - resolved spatially localized spectroscopic sequence ) con un te ( 136 ms ) ottimizzato per la valutazione quantitativa del citrato e della colina con analisi multivoxel . 
sono stati utilizzati i seguenti parametri di acquisizione : tr 1.600 ms , te 136 ms , ampiezza spettrale 1.000 hz , con risoluzione spettrale nominale del voxel di 0 , 24 cm3 . 
il tempo di acquisizione della sequenza spettroscopica stato di 18 minuti . le sequenze post - contrastografiche sono state utilizzate nella valutazione di rapidi potenziamenti di segnale , in particolare della porzione periferica della ghiandola , sincroni con la normale omogeneizzazione della porzione adenomiomatosa , suggestivi di lesione produttiva con neoangiogenesi anarchica nel contesto . image analysis was carried out by an experienced radiologist ( es ) in mri of abdominal - pelvic structures . 
1a - d dynamic t1 - weighted fast - field ( ffe ) sequence : the acquisitions at time 0 ( a ) and 20 s after contrast medium infusion ( b ) show a focal early wash - in ( arrow ) in the middle - left peripheral portion . 
acquisizione a 20 s dalla somministrazione del mezzo di contrasto che evidenzia precoce wash - in focale ( freccia ) a carico della porzione periferica paramediana sinistra ( b )  . 
presence of a rounded homogeneously hypointense area esperto ( es ) nellimaging rm delle strutture addomino - pelviche il quale era a conoscenza del fatto che i pazienti avevano lesioni sospette per neoplasia alla trus . 
i confini della zona periferica sono stati definiti grazie alla visualizzazione delle bande di bassa intensit di segnale nelle immagini t2 dipendenti riferibili alla capsula e alla pseudocapsula prostatica [ 7 ]  . 
by using dedicated software for spectroscopic analysis , values of the integral of the areas underlying citrate , choline and creatine peaks were calculated . to detect the presence of cancer , the ratio between the integral of choline plus creatine and the integral of citrate was calculated for each voxel . 
la presenza di unarea omogeneamente ipointensa a margini rotondeggianti e limiti sfumati stata considerata come sospetta per neoplasia . i singoli voxel del volume selezionato nella sequenza spettroscopica sono stati rappresentati bidimensionalmente in forma grafica di griglia sovrapposta alle corrispondenti immagini traverse t2 pesate . 
in tutti i pazienti sono stati effettuati 10 prelievi secondo suddivisione in ottanti della prostata ( 1 prelievo per apice , zona intermedia , basale e 2 per la zona laterale per ciascun lato )  . almeno 2 campionamenti sono stati ottenuti dalle zone che presentavano caratteristiche patologiche alla rm ed alla rmsp . 
in all patients , ten samples were taken according to the subdivision of the prostate into octants ( one sample from the apical , intermediate and basal areas and two samples for the lateral area on each side )  . at least two samples were taken from the areas that presented pathological features at mri and mrsi . 
samples were classified based on the sampling site , and histological analysis was carried out for each site . every biopsy sample was analysed by a single pathologist specialized in prostatic diseases . statistical analysis findings were processed with the statistical package for social sciences , version 12 ( spss , chicago , il , usa )  . 
results obtained with mri and mrsi used separately and in combination and with biopsy were analysed in terms of sensitivity , specificity , positive ( ppv ) and negative predictive value ( npv ) and accuracy values . statistically significant differences in the comparison between mri and mrsi and mri and mrsi combined versus biopsy were processed through an c2 test according to pearson , assuming a value of p0.05 , to indicate a significant correlation . 
although images had been classified as normal , equivocal or suspicious for cancer , in the statistical analysis , results were divided into two groups only : positive ( suspicious and equivocal , > 3 sd and < 23 sd > ) and negative ( normal and < 2 sd )  . results findings of the dynamic post - contrast acquisitions were not used in statistical evaluation of the selected sample . 
twentysix out of 39 patients ( 66% ) showed focal and / or unilateral or bilateral signal hypointensity in the t2 - weighted images whereas the remaining 13 ( 33% ) showed no pathological signal alterations . 
in particular , as regards location within the gland , mri detected five suspicious areas at the apical level ( three on the right , two on the left ) , eight at the intermediate level ( three on the right , five on the left ) , nine at the lateral level ( five on the right , four on the left ) and four at a basal level ( two on the right , two on the left )  . of the 26 patients in whom mri was suggestive of a neoplastic lesion , histology confirmed adenocarcinoma in 17 [ 65% true positive ( tp ) ] but diagnosed benign lesions in nine [ 35% false positive ( fp ) ]  . 
ciascun campione bioptico stato analizzato da un unico anatomo - patologo specialista nella patologia prostatica . analisi statistica i dati sono stati elaborati utilizzando lo statistical package for social sciences , versione 12 ( spss , chicago , illinois )  . 
i risultati ottenuti rispettivamente dalla rm , dalla rmsp , dalla combinazione rm - rmsp e dalla biopsia sono stati tabulati calcolando i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) ed accuratezza . i valori di significativit statistica nel confronto tra i risultati della rm e della rmsp e della combinazione rm - rmsp rispetto alla biopsia sono stati elaborati mediante test c2 secondo pearson , assumendo un valore di p0 , 05 indicante una correlazione significativa . sebbene le immagini fossero state classificate come normali , equivoche o sospette per neoplasia , ai fini dellanalisi statistica i risultati sono stati suddivisi in due soli gruppi ovvero positivi ( sospetti ed equivoci , > 3 ds e < 23 ds > ) e negativi ( normali , < 2 ds )  . risultati i dati relativi alle acquisizioni dinamico - contrastografiche non sono stati utilizzati nella valutazione statistica del campione selezionato . ventisei pazienti dei 39 totali ( 66% ) presentavano ipointensit di segnale di tipo focale e / o diffusa mono o bilateralmente nelle immagini t2 dipendenti , mentre i rimanenti 13 ( 33% ) non mostravano alterazioni di segnale di carattere patologico . in particolare , in riferimento alla localizzazione a livello della ghiandola , con la rm sono state attribuite 5 aree sospette a livello dellapice ( 3 a destra , 2 a sinistra ) , 8 in regione intermedia ( 3 a destra , 5 a sinistra ) , 9 in sede laterale ( 5 a destra , 4 a sinistra ) e 4 in regione basale ( 2 a destra , 2 a sinistra )  . dei 26 pazienti con rm suggestiva per lesione discariocinetica , 17 ( 65% vp ) hanno trovato conferma istologica di adenocarcinoma , mentre 9 ( 35% fp ) hanno avuto diagnosi di lesione benigna , in 5 casi di natura flogistica ( prostatiti acute o croniche ) nei rimanenti 4 di iperplasia nodulare benigna . 
of the 13 patients without suspicious findings for cancer , histology confirmed the absence of neoplastic lesions in ten [ 77% true negative ( tn ) : seven cases of benign nodular hyperplasia and three of granulomatous prostatitis ] but detected adenocarcinoma in 3three [ 23% false negative ( fn ) ] ( table 1 )  . based on these results , mri had a 85% sensitivity , 53% specificity , with 65% ppv and 77% npv and 69% accuracy with a p = 0.013 ( table 2 )  . 
mrsi identified pathological spectra ( cho + cr / cit ratio > 3 sd or < 23 sd > ) in 17 patients ( 43% ) whereas spectrum analysis was normal ( cho + cr / cit ratio < 2 sd ) in the remaining 22 ( 57% )  . 
la rmsp ha individuato spettri di tipo patologico ( rapporto cho + cr / cit > 3 ds o < 23 ds > ) in 17 pazienti ( 43% ) , mentre nei restanti 22 ( 57% ) lanalisi spettrale risultata nei limiti della normalit ( rapporto cho + cr / cit < 2 ds )  . 
in base alla suddivisione in ottanti 2 erano le aree sospette a livello dellapice prostatico , 7 in regione intermedia ( 3 a destra , 4 a sinistra ) , 7 in sede laterale ( 4 a destra , 3 a sinistra ) 1 in regione basale destra . 
la rmsp ha dimostrato una sensibilit del 75% con specificit del 89% , un vpp del 88% , un vpn del 74% con unaccuratezza del 87% con un valore di p = 0 , 000 ( tabella 2 )  . combinando i risultati della rm con quelli della rmsp abbiamo avuto una sensibilit del 70% con una specificit del 89% , vpp 88% , vpn 74% , unaccuratezza del 79% e un valore di p = 0 , 000 ( tabella 2 )  . riguardo alla localizzazione delle lesioni non si evidenziata una significativa correlazione tra i risultati ottenuti ai prelievi bioptici e quelli evidenziati alla rm e alla rmsp , se non per quanto riguarda i risultati dellistologia e della rmsp nella zona intermedia e laterale ( p = 0 , 003 e p = 0 , 002 rispettivamente )  . table 1 correlation of magnetic resonance imaging ( mri ) , mr spectroscopic imaging ( mrsi ) and biopsy findings tabella 1 correlazione tra rm , rmsp e reperti bioptici biopsy findings mrsi risultati biopsia rmsp negative positive negative positive negativi positivi negativi positivi negative positive total negativi positivi totale table 2 sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) , and accuracy of magnetic resonance imaging ( mri ) , mr spectroscopic imaging ( mrsi ) and combined mri / mrsi tabella 2 sensibilit , specificit , vpp , vpn , accuratezza della rm , rmsp e rm / rmsp combinate mri , % mrsi , % mri / mrsi , % rm , % rmsp , % rm / rmsp , % sensibilit specificit accuratezza sensitivity specificity accuracy g . 
3a - d ipointensit focale nelle immagini assiali t2pesate nella zona periferica in sede mediana sinistra . lo spettro ottenuto dallarea di alterata intensit di segnale ha evidenziato unelevazione della colina e una riduzione del citrato compatibile con la presenza di cancro ( d )  . 
4a - d diffusa alterata intensit di segnale nella zona periferica a destra nelle immagini t2 - pesate ( piano assiale , a e c e piano coronale , b )  . 
in contrast , our study aimed at assessing the ability of mri and mrsi to identify and localise prostate cancer by prospectively correlating findings of single techniques with biopsy results . the decision to use a surface coil was dictated by the need to obviate the poor tolerability of the examination carried out with an intracavitary coil and to improve the quality of images corrupted by specific artefacts of endorectal coils ( coil flare , straight line , glandular distortion ) [ 18 ]  . as regards the morphological evaluation alone , mri had 85% sensitivity and 53% specificity in the detection of lesions values in line with those reported in the literature . il carcinoma prostatico rappresenta a tuttoggi unimportante causa di morte per cancro nella popolazione maschile [ 1 ]  . 
di contro a questa rilevante mortalit , ci sono molti casi di tumore a decorso subclinico rilevati casualmente al solo esame autoptico [ 9 ]  . le tecniche diagnostiche non invasive correntemente disponibili presentano delle forti limitazioni nel discriminare forme latenti da forme aggressive e progressive [ 10 , 11 ]  . la trus ha dimostrato di non essere in grado di individuare fino al 30% delle lesioni palpabili allesplorazione rettale e di avere unelevata percentuale di falsi positivi in quanto solo il 20% delle lesioni ipoecogene ( principale caratteristica ecografia di malignit ) sono realmente maligne [ 12 ] ; la biopsia ecoguidata inoltre presenta unelevata percentuale di errori nel campionamento per il fatto che solo una piccola parte della ghiandola prostatica viene effettivamente analizzata cosicch molti pazienti che presentano valori di psa alterati ( > 4 ng / ml ) e che sono sottoposti ad un campionamento sistematico lungo i sestanti prostatici hanno esito negativo allesame bioptico e sono candidati ad un ulteriore prelievo [ 13 , 14 ]  . con lemergere di nuove strategie terapeutiche meno invasive rispetto alla prostatectomia radicale , si sente , inoltre , maggiormente lesigenza di una precisa localizzazione e valutazione dellestensione della malattia , per eseguire una terapia mirata che incrementi lefficacia del trattamento , riducendone la morbilit . 
le esperienze sinora pubblicate , aggiungendo al dato morfologico quello metabolico mediante limaging spettroscopico 3d , evidenziano un miglioramento nellindividuazione della neoplasia e nella definizione della stadiazione , volume e grado di aggressivit [ 8 , 16 , 17 ]  . 
 la maggior parte dei dati in letteratura deriva per da studi di tipo retrospettivo , in cui laccuratezza diagnostica della rm e della rmsp stata valutata facendo riferimento al dato istopatologico ottenuto dopo prostatectomia radicale . 
nel nostro studio abbiamo voluto invece valutare la capacit della rm e della rmsp nellindividuazione e localizzazione del tumore prostatico , correlando prospetticamente i risultati ottenuti dalle singole tecniche con quelli bioptici . la scelta di utilizzare una bobina di superficie si imposta per ovviare alla scarsa tollerabilit dellesame eseguito con bobina endocavitaria e per migliorare la qualit dellimmagine corrotta da artefatti specifici delle bobine endorettali ( coil flar , straight line , distorsione ghiandolare ) [ 18 ]  . per quanto riguarda la sola valutazione morfologica la rm ha mostrato , nellidentificazione delle lesioni , una sensibilit del 85% e una specificit del 53% , valori questi sostanzialmente sovrapponibili a quelli riportati in letteratura . la rmsp , con laggiunta del dato metabolico ha mostrato mrsi , with the addition of metabolic data , proved to be significantly more specific in identifying tumours as compared with mri alone ( 89% versus 53% )  . 
a positive result at mri and mrsi indicates the likely presence of cancer ( ppv 88% ) whereas a negative result excludes it with a slightly lower likelihood ( npv 77% )  . 
presumably , this is affected by the number of false negatives , which are likely due to limitations of the current multivoxel technology , with a nominal voxel value that is still high ( 0.24 cm3 ) , and is typical of 1.5t magnetic fields , with a possible summation of the tumour 's metabolic findings with those of surrounding healthy tissue in the sampled volume . 
another possible explanation of the failed identification of tumour lesions by mrsi may be the low biological aggressiveness of some cancers . some authors [ 19 ] have already reported that small , lowgrade tumours ( gleason scores 4 and 5 ) may be missed owing to slight alterations of citrate and choline . 
il valore nominale del voxel infatti ancora elevato ( 0 , 24 cm3 ) , caratteristico per campi magnetici di 1 , 5t , e ci potrebbe determinare un effetto di sommazione del dato metabolico tumorale con quello del tessuto sano circostante nel volume campionato . unaltra possibile spiegazione della non avvenuta identificazione delle lesioni tumorali da parte la rmsp pu essere correlata alla scarsa aggressivit biologica di alcune neoplasie . infatti , gi stato riportato da alcuni autori [ 19 ] come piccoli tumori a basso grado ( gleason 4 e 5 ) possono non essere rilevati per le lievi alterazioni del citrato e della colina . 
iniziali studi clinici , che vedono lapplicazione di campi magnetici ad alta intensit ( 3t ) , dimostrano come sia possibile aumentare sensibilmente la risoluzione spettrale , con un sostanziale incremento di accuratezza nellidentificazione spaziale del dato metabolico [ 20 ]  . la scarsa correlazione complessiva tra i risultati della rm e della rmsp e quelli istopatologici , riguardo la localizzazione spaziale delle lesioni , fa s che il nostro studio non sia in grado di rispondere alla domanda se la localizzazione del tumore prostatico influenzi la capacit delle due tecniche di rilevare il tumore stesso . 
in realt , per lintrinseca difficolt della biopsia ecoguidata di garantire una precisa corrispondenza tra il sito del prelievo e le aree sospette alla rm e alla rmsp , solo lanalisi istologica dopo prostatectomia radicale in grado di rispondere realmente a tale quesito . conclusions conclusioni although ours was a preliminary study carried out on a small sample of patients and larger series are needed to confirm our findings , we can reasonably conclude that the combination of mri and mrsi also considering the greater tolerability of an examination that avoids the use of endorectal coils may be indicated as a problem - solving modality for two categories of patients : those whose high serum psa and suspicious trus finding , which make them candidates for biopsy ; and those who have already undergone multiple biopsies , all with a negative outcome but persistent serum psa alterations , and are therefore candidates for further biopsy . 
identification of suspicious areas on mri and mrsi also provides the possibility of performing targeted biopsies of those areas , under direct mri guidance , and to remove the error inherent in correlating mri with trus findings [ 21 ]  . in conclusione , sebbene il nostro sia certamente uno studio iniziale , realizzato su di una piccola popolazione campione e che siano necessarie pi ampie serie di pazienti per confermare quanto da noi evidenziato , ragionevole ritenere che lassociazione rm / rmsp , anche in relazione alla maggiore tollerabilit di un esame che evita lutilizzo della bobina endorettale , possa essere indicata come modalit problem - solving in quei pazienti che , con elevati valori di psa sierico e trus sospetta per lesione neoplastica , sono candidati al prelievo bioptico oppure in coloro che , gi sottoposti a biopsie multiple con esito negativo , per il persistere delle alterazioni sieriche del psa , rientrano in una zona di incertezza e sono candidati ad unulteriore biopsia . 
cova1 1unit clinica operativa di radiologia , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , i - 34149 trieste , italy 2unit operativa di radiologia , ospedale umberto i , mestre , venezia , italy 3dipartimento di economia e tecnica aziendale , universit degli studi di trieste , trieste , italy correspondence to : f . 
the sum of equipment costs ( amortisation and service contract ) , variable costs ( supplies and related services ) and personnel costs ( radiologist , radiographer and nurse ) was determined . 
intra - arterial dsa costs more than mra , mainly because of the higher costs of supplies used during the procedure and higher personnel costs ( as a result of the longer duration of intra - arterial dsa )  . 
mra provides good diagnostic accuracy in the evaluation of arteries of the lower extremities , and its biological cost is far lower than that of intra - arterial dsa ( mra is noninvasive , it does not use ionising radiation , and the contrast medium is safe )  . 
its lower cost is another argument in favour of the use of mra instead of intra - arterial dsa in the evaluation of lower - extremity arterial disease . key words magnetic resonance angiography intra - arterial digital subtraction angiography cost analysis peripheral vascular disease riassunto obiettivo . 
stato calcolato il costo differenziale delle due indagini , ovvero la somma dei costi delle apparecchiature ( ammortamenti e manutenzione ) , dei costi variabili ( materiali e servizi connessi ) e dei costi del personale ( medico , tecnico e infermieristico )  . 
il costo differenziale dellangio - rm risultato di 186 , 14 euro ( costi delle apparecchiature 50 , 80 euro , costi variabili 75 , 04 euro , costi del personale 60 , 30 euro ) , mentre quello dellangiografia digitale risultato di 238 , 18 euro ( costi delle apparecchiature 57 , 60 euro , costi variabili 90 , 13 euro , costi del personale 90 , 45 euro )  . 
langiografia digitale ha un costo superiore allangio - rm , determinato essenzialmente dal maggior costo del materiale utilizzato durante la procedura e dal maggior costo del personale ( legato , a parit di figure professionali coinvolte , alla maggior durata dellesame angiografico )  . 
langio - rm fornisce una buona accuratezza diagnostica nella valutazione delle arterie degli arti inferiori ed ha un costo biologico nettamente inferiore allangiografia digitale ( assenza di invasivit , assenza di radiazioni ionizzanti , mezzo di contrasto con pi elevato margine di sicurezza )  . 
il minor costo dellangio - rm costituisce un ulteriore elemento che porta a preferire questa indagine allangiografia digitale nella diagnostica delle arteriopatie degli arti inferiori . parole chiave angio - rm angiografia digitale intra - arteriosa analisi dei costi arteriopatia periferica f . 
technological advancements have allowed this technique to provide high levels of sensitivity and specificity as compared with digital subtraction angiography ( dsa ) as the gold standard even though the reported ranges are extremely wide ( sensitivity : 71%100% , specificity : 63%100% ) [ 111 ]  . 
most papers have , therefore , considered its diagnostic contribution and emphasised its advantages of having a negligible biological cost . by contrast , this study analyses and compares the costs of mra and intra - arterial dsa in the evaluation of lower - limb arteries . 
it should be noted that activities and costs related to these two examinations pertain largely to the radiology department even if some aspects , particularly related to dsa , concern other departments as well . 
the costs were also analysed from the point of view of the producer ( the hospital ) , whose aim it is to provide the patient with the best and most cost - effective clinical approach . 
our study presents a cost - identification analysis , namely , a partial assessment of the two examinations in question , concentrating on their effect on costs ( input ) [ 12 ]  . 
clinical consequences of the two different approaches have , instead , been excluded from our study ( output )  . langiografia mediante risonanza magnetica ( angio - rm ) ha trovato negli ultimi anni applicazione sempre pi ampia nella valutazione delle arteriopatie degli arti inferiori . 
i progressi tecnologici hanno fatto s che tale indagine possa garantire una sensibilit ed una specificit elevate , utilizzando langiografia digitale come gold standard , pur se i lavori pubblicati riportano un range di percentuali assai ampio ( sensibilit tra il 71% e il 100% , specificit tra il 63% e il 100% ) [ 111 ]  . 
molti lavori hanno preso quindi in considerazione il suo apporto diagnostico ed hanno sottolineato i suoi benefici , per il trascurabile costo biologico . in questo lavoro abbiamo ritenuto opportuno analizzare invece i costi dellangio - rm nella valutazione delle arterie degli arti inferiori , raffrontati a quelli dellangiografia digitale per via arteriosa . 
va rilevato come attivit e costi relativi a queste due indagini sono in larga misura di pertinenza dei servizi di radiologia , ma per talune , langiografia digitale in particolare , riguardano anche altri reparti . 
i costi sono inoltre stati considerati dal punto di vista del produttore ( lospedale ) che ha lobiettivo di fornire al paziente lapproccio clinico migliore e con il miglior rapporto costo - efficacia . 
lanalisi dei costi effettuata del tipo cost - identification , ovvero una valutazione parziale con lobiettivo di valutare , analizzando le due indagini considerate , gli effetti sui costi ( input ) [ 12 ]  . 
non sono invece state considerate le conseguenze cliniche dei due diversi approcci ( output )  . materials and methods examination technique magnetic resonance angiography mra examinations were performed using a 1.5 - t intera master superconductive magnet ( philips medical systems , eindhoven , the netherlands ) with 30 mt / m power gradients and 150 mt / m per millisecond rise time . 
the use of automated table movement ( mobitrack , philips ) allowed us to study the aorto - iliac , femoral - popliteal and popliteal - tibial vascular regions in a sequence . 
for evaluation of each vascular region , we used three - dimensional ( 3 - d ) fast spin echo ( fse ) t1 - weighted sequences with the following parameters : tr = 6 ms , te 1.5 ms , flip angle 35 , slice thickness 1.5 mm ( 3 mm with 1.5 - mm overlap ) , field of view 430 mm , matrix 512512 , number of slices 70 and acquisition time 28 s . 
overall acquisition time of successive sequences , including the time needed for two table movemateriali e metodi tecnica desame angio - rm gli esami di angio - rm sono stati eseguiti utilizzando un magnete superconduttivo da 1 , 5 t intera master ( philips medical systems , eindhoven , olanda ) con gradienti di potenza pari a 30 mt / m e velocit di raggiungimento del picco di 150 mt / m / ms . 
limpiego dello spostamento automatico del tavolo ( mobitrack ; philips ) ha consentito di studiare in successione il distretto vascolare aorto - iliaco , quello femoropopliteo e quello popliteo - tibiale . 
sono state impiegate per la valutazione di ciascun distretto vascolare sequenze 3d fse t1 pesate utilizzando i seguenti parametri : tr = 6 ms , te 1 , 5 ms , flip angle = 35 , spessore di strato pari ad 1 , 5 mm ( 3 mm con sovrapposizione di 1 , 5 mm ) , campo di vista = 430 mm , matrice = 512x512 , numero di strati = 70 , tempo di acquisizione paf . 
this was followed by injection of 0.2 mmol / kg of 0.5 m paramagnetic contrast agent ( gadobenate dimeglumine , multihance , bracco , milan , italy ) with a 0.5 - ml / s flow rate . 
post - processing included subtraction of images acquired before and after the contrast agent injection and 3 - d reconstructions based on the maximum intensity projection ( mip ) algorithm . dsa ( intra - arterial ) dsa examinations were carried out using the integris allura system for diagnostic angiography and interventional radiology ( philips medical systems , eindhoven , the netherlands )  . 
examinations were performed with intra - arterial catheterisation , usually after puncture of the femoral artery and insertion of the distal end of the catheter into the infrarenal abdominal aorta . 
straight - end or pigtail catheters , which can endure high flows of contrast material , were employed . intra - arterial examinations were performed using two different methods : the bolus - chasing technique ( in which synchronised table movement during injection of the contrast agent allows passage of the contrast through the aorto - iliacfemoral - popliteal region to be monitored ) , and the successive fields technique . 
choice of technique was based on the result of the preliminary test to determine the knee arrival time ( kat ) or the number of seconds it takes for a small amount of injected contrast agent to reach the popliteal artery at the knee joint . we noted that when the kat is very short ( 46 in . ) , image quality , especially at the abdominal level , is affected by blurring of the vessel caused by the table moving too fast . hence , the bolus - chasing technique is only used when the kat exceeds 7 s whereas for shorter kats , the classical multiple - fields technique is adopted . 
in the bolus - chasing technique , the examination is carried out with a single injection of 80 ml of non - ionic monomeric contrast medium ( 350370 mgi / ml ) with a 79 ml / s flow rate through an automatic injector , and the table moves automatically at a speed determined by result of the preliminary test . 
stato preliminarmente valutato con liniezione di 2 ml di mezzo di contrasto ( mdc ) ( 0 , 5 ml / s ) in una vena del braccio il tempo necessario per iniziare ad ottenere lopacizzazione dellaorta addominale . 
sono state quindi effettuate con spostamento del tavolo le sequenze maschera ( senza somministrazione del mdc ) sui tre tratti a partire da quello popliteo - tibiale . sono stati poi iniettati 0 , 2 mmol / kg di un mdc paramagnetico 0 , 5 m ( gadobenato dimeglumina , multihance , bracco , milano , italia ) con flusso di 0 , 5 ml / s . 
sono state quindi acquisite le sequenze dopo iniezione di mdc a partire dal distretto aorto - iliaco , secondo il tempo di ritardo calcolato mediante il bolo preliminare di 2 ml . 
il post processing prevedeva la sottrazione di immagine tra quelle acquisite prima e dopo iniezione di mdc e ricostruzioni 3d secondo lalgoritmo mip ( maximun intensity projection )  . angiografia digitale ( accesso arterioso ) gli esami sono stati effettuati utilizzando il sistema per angiografia diagnostica e radiologia interventistica integris allura ( philips medical systems , eindhoven , olanda )  . 
sono stati utilizzati cateteri ad estremit diritta o pig tail in grado di sostenere flussi elevati di mdc . gli esami con accesso arterioso sono stati eseguiti con due diverse modalit : tecnica bolus chasing ( che grazie al movimento sincronizzato del tavolo durante liniezione del mdc consente di seguire lavanzamento del bolo di mdc nel distretto aorto - iliaco - femoro - popliteo ) o tecnica per campi successivi . 
la diversa tecnica di esecuzione si basata sul risultato del preliminare test per determinare il kat ( knee arrival time ) che stabilisce , una volta iniettato un piccolo quantitativo di mdc , quanti secondi esso impiega a giungere nellarteria poplitea a livello della rima articolare del ginocchio . 
si verificato che quando il kat molto breve ( 46 s ) la qualit delle immagini soprattutto a livello addominale risulta essere subottimale per la presenza di sfumatura del vaso causata dalleccessiva velocit del movimento di avanzamento del tavolo . 
nella tecnica bolus chasing lesame viene effettuato con ununica iniezione di 80 ml di un mdc monomero non ionico ( 350370 mgi / ml ) ad un flusso di 79 ml / s eseguita mediante apposito iniettore automatico e il tavolo scorre automaticamente ad una velocit che si basa sul risultato del test preliminare . 
if motion artefacts are present , images can be processed with pixel shift software so as to minimise them . if motion artefacts are more substantial , images can be visualised at any rate without subtracting the skeletal structures . 
an automatic injector is again used to administer 30 ml of contrast agent at a 15 - ml / s flow rate for each field , for a total of 150 ml . 
the full cost of the two studies was thus obtained ( the sum of differential and common costs )  . equipment cost was calculated based on the time it was used ; when analysing the cost of technology , the purchase price of the various machines ( which can be strongly affected by substantial discounts ) and the adequacy of the system for calculating amortisation are clearly important . 
purchase prices were derived from hospital administration records . amortisation was calculated on a time basis based on a constant annual value . the lifetime of the radiological units was estimated as 8 years , i.e. 
procedure duration was estimated based on times envisaged by the radiology information system ( ris ) in use at our unit . in evaluating the differential cost , we merely considered the technical act , disregarding any other costs related to patient management , as inclusion of the latter would have required an explicit description of the relations between the radiology department and other cost centres of the hospital and the part played by radiological examinations in inpatient treatment . therefore , our analysis was restricted to costs incurred by the radiology unit . 
this made it possible to draw comparisons over time ( with respect to budget targets ) and space ( with respect to other hospitals : independent , with separate accounting , or private ) [ 13 ]  . 
 the cost of fixed - asset utilisation ( technology ) was related to their time of use , and the cost of radiologists , technologists and nurses was related to their specific activity meadelliniezione del mdc e la seconda durante liniezione del mdc , ottenendo quindi due serie di 15 immagini ciascuna . 
ad ogni campo desame vengono iniettati , sempre mediante iniettore automatico , 30 ml di mdc con un flusso di 15 ml / s , per un totale di 150 ml . analisi economica stato calcolato il " costo differenziale " ( definito come la somma dei costi delle apparecchiature , dei costi variabili e dei costi del personale ) delle due indagini . 
 stato inoltre calcolato il " costo comune " , il quale raggruppa quelle componenti del costo che risultano sovrapponibili per ogni tipo di esame svolto allinterno dellunit clinico operativa di radiologia . 
stato cos possibile ottenere il " costo pieno " delle due indagini ( somma del costo differenziale e di quello comune )  . il costo delle apparecchiature stato calcolato in base al tempo di utilizzo delle stesse ; nel valutare il costo della tecnologia emerge limportanza del costo dacquisto delle diverse attrezzature ( che pu essere influenzato notevolmente da sconti significativi ) e della congruit del sistema di calcolo dellammortamento . 
la durata della vita lavorativa delle apparecchiature radiologiche stata considerata di otto anni , il loro tempo tecnologico massimo . sono poi stati valutati i costi variabili , relativi ai materiali impiegati e ai servizi legati a tale impiego . 
la durata delle procedure stata stimata facendo riferimento ai tempi previsti nel sistema informativo radiologico ( ris ) in uso presso la nostra struttura . nella valutazione del costo differenziale ci siamo limitati a considerare latto tecnico , ignorando tutti gli altri costi legati alla gestione del paziente . 
ci infatti avrebbe comportato lesplicitazione di tutti i rapporti tra la radiologia e gli altri centri di costo dellazienda ospedaliero - universitaria e , per i pazienti ricoverati , anche del ruolo che le indagini radiologiche hanno sul processo di cura . 
they are therefore not decisive for comparing costs but play a role in determining the full cost of the two methods . the sections below provide a detailed analysis of the differential costs of mra and dsa , with the methods in use at our radiology unit . 
as stated above , three components of the differential cost were considered , namely : ( 1 ) equipment costs ( amortisation and service contract ) ; ( 2 ) variable costs ( supplies and related services ) ; ( 3 ) personnel costs . it should be noted that every patient undergoing dsa must have a blood test to evaluate serum glucose and creatinine levels and coagulation profile [ quick time , international normalised ratio ( inr ) and platelets ]  . in addition , patients with a history of allergy ( 1% of cases ) require pre - medication with steroids associated with antih1 and anti - h2 . the cost of these procedures does not pertain to the radiology unit however , because the procedures are mandatory before contrast - enhanced angiography and because their cost is not negligible , they will be briefly discussed . finally , it should be recalled that costs of supplies and equipment are inclusive of 20% vat . results differential costs magnetic resonance angiography 1 . 
we took into account the cost of a 1.5 - t intera master mri device ( philips medical systems , eindhoven , the netherlands ) with 30 - mt / m power gradients and a rise time of 150 mt / m per millisecond . 
there follows an annual cost of 3 , 021.25 euro considering 8 years of amortisation . then the cost of the dry printer ( kodak dryview 8700 laser imager ) was included . 
come gi evidenziato , sono state prese in considerazione 3 componenti del costo differenziale , e precisamente : ( 1 ) costi delle apparecchiature ( ammortamenti e manutenzione ) ; ( 2 ) costi variabili ( materiali e servizi connessi ) ; ( 3 ) costo del personale . va rilevato che ogni paziente sottoposto ad angiografia digitale deve eseguire preliminarmente un prelievo ematico per valutare i livelli sierici di glucosio e creatinina e il suo assetto emocoagulativo ( tempo di quick , inr e piastrine )  . nell1% dei casi inoltre , essendoci unanamnesi allergica positiva , si esegue anche una preparazione farmacologica ( basata sullimpiego di cortisonici associati ad anti - h1 ed anti - h2 )  . 
i costi legati a tali procedure non sono di pertinenza dellunit clinico operativa di radiologia ; tuttavia queste sono fondamentali ai fini dellesecuzione dellesame angiografico con mezzo di contrasto ed avendo comunque un certo rilievo economico verranno in seguito brevemente prese in considerazione . si ricorda infine che i costi di materiali ed apparecchiature sono comprensivi di iva al 20% . risultati costi differenziali angio - rm 1 . 
abbiamo preso in considerazione il costo di un apparecchio di rm da 1 , 5 t intera master con gradienti di potenza pari a 30 mt / m e velocit di raggiungimento del picco di 150 mt / m / ms . 
by estimating the average annual cost of a radiologist , technologist and nurse ( totalling 158 , 744 euro ) and subtracting the time off work for ordinary , special and sick leave ( 30% on average ) from the annual hourly debt , the actual work time amounted to 35 weeks / year , which results in a daily cost of 905 euro and an hourly cost of 120.73 euro for these three professionals taken together . 
valutando il costo medio annuo per un medico , per un tecnico sanitario di radiologia medica ( tsrm ) e per un membro del pool infermieristico ( complessivamente 158.744 euro ) e sottraendo al debito orario annuo le assenze per congedo ordinario , straordinario e malattie ( 30% in media ) , risulta un tempo lavorativo effettivo pari a 35 settimane / anno , da cui si deriva il costo giornaliero ( 905 euro ) e orario ( 120 , 73 euro ) di queste tre figure professionali considerate assieme . 
limpegno temporale del medico legato alle diverse attivit che egli deve svolgere in prima persona , ovvero : presenza fisica in fase di acquisizione dellesame , analisi delle immagini alla consolle , refertazione , correzione e sigla del referto . 
va inoltre preso in considerazione il tempo preliminare allesame ; in particolare , il paziente deve sottoscrivere un apposito questionario mediante il quale se ne verifica lidoneit allaccesso al magnete . 
perci , in base alla nostra esperienza , il tempo medico previsto per un angio - rm degli arti inferiori di 30 minuti . ogni indagine di angio - rm per lo studio degli arti inferiori comporta un impegno temporale del tsrm e dellinfermiere anchesso stimabile in 30 minuti . 
ne risulta quindi un costo personale per esame di 60 , 30 euro . da quanto esposto risulta come , sommando tutti i parametri considerati , il costo differenziale di unangio - rm degli f . 
the cost of the contrast agent injector ( mark 4 , medrad , indianola , usa ) , 8 , 374.29 euro , corresponds to 1 , 046.78 euro per year for 8 years of amortisation . 
the following factors were taken into account : supplies used prior to the procedure ( sterile gloves , disinfection material , sterile cloth , sterile cloths without slit , a sheet with slit for femoral access ) : total cost of preparatory supplies was 1.10 euro supplies used during the procedure ( surgical gauzes , 10 - cc luerlock syringe , 20 - cc syringe , needle for arterial puncture , lidocaine , guidewire , introducer , catheter )  . 
essa viene utilizzata dallunit clinico operativa di radiologia con contratto daffitto triennale comprensivo di installazione , interfacciamento ai sistemi di archiviazione delle immagini e manutenzione , per un costo pari a 13.785 , 00 euro annui . 
alla stampante a secco confluiscono peraltro le due apparecchiature tc in uso nellunit clinico operativa di radiologia ; nel nostro caso langiografo digitale utilizza la stampante per circa il 30% della sua attivit ; ne deriva quindi un costo annuo di 4135 , 50 euro . 
va inoltre considerato il costo delliniettore del mezzo di contrasto ( mark 4 , medrad , indianola , usa ) pari a 8.374 , 29 euro , il che corrisponde a 1.046 , 78 euro annui per 8 anni di ammortamento . 
vanno presi in considerazione i seguenti fattori : materiale preparatorio allesecuzione dellesame ( guanti sterili , materiale per disinfezione , telino sterile , teli sterili senza spacco , lenzuolo con taglio accesso femorale )  . 
il costo totale del materiale preparatorio di 1 , 10 euro . materiale utilizzato durante la procedura ( garze sterili , siringa luerlock da 10 cc , siringa da 20 cc , ago da puntura arteriosa , lidocaina , guida , introduttore , catetere )  . 
estimating the overall average annual cost for a radiologist , a technologist and a nurse at 158 , 744 euro and subtracting ordinary , special and sick leaves ( 30% on average ) from the annual hourly debt , the actual work time is 35 weeks / year , with a daily cost of 905 euro and an hourly cost of 120.73 euro for these three professionals taken together . the radiologists time commitment depends on the different activities he / she has to perfor in the case of an angiographic examination , the radiologists time includes performing the procedure from the end of patient preparation to positioning the catheter into the aorta , as well as being physically present during the acquisition phase , assessing images on screen , removing the catheter , performing the compression , reporting , correcting and signing the written report . hence , based on our experience , intra - arterial lower limb angiography involves 45 min of the radiologists time . 
these costs are unaffected by variations in the total number of yearly examinations . common costs are those associated with support staff and support materials . we were unable to conduct a detailed analysis of support activities to quantify the contribution of these production factors to the different procedures ( random principle ) , but we could , as an alternative , use the means method , assuming that each radiological procedure uses these services to the same extent , i.e. 
that the specific features of each procedure do not affect the common costs . support staff costs were calculated considering all professionals not described so far . they consist of one consultant , one chief technologist , three technologists , three auxiliary staff , four file clerks and seven assistants and administrative assistants . 
per ogni esame se ne impiegano in media 120 ml ( diaco , sodio cloruro 0 , 9% ) usando flaconi da 250 ml ( al costo di 0 , 25 euro per flacone ) , con un costo per esame di 0 , 10 euro . pellicole : nella documentazione delle angiografie degli arti inferiori previsto luso di una pellicola 3543 cm ( dvb kodak ) , per un costo di 2 , 97 euro ( le confez ioni da 500 hanno un costo di 1489 , 40 euro )  . 
valutando il costo medio annuo complessivo di un medico , un tsrm e un infermiere in 158.744 euro e sottraendo al debito orario annuo le assenze per congedo ordinario , straordinario e malattie ( in media 30% ) , risulta un tempo lavorativo effettivo pari a 35 settimane / anno , da cui si deriva un costo giornaliero di 905 euro e orario di 120 , 73 euro di queste tre figure professionali considerate assieme . 
nel caso dellesame angiografico il tempo medico prevede lesecuzione della procedura dal termine della preparazione del paziente fino al posizionamento del catetere in aorta , la presenza fisica in fase di acquisizione dellesame , la verifica a monitor delle immagini acquisite , la rimozione del catetere , la compressione , la refertazione dellesame , la correzione e la sigla del referto . 
ne risulta quindi un costo personale per esame di 90 , 45 euro . da quanto esposto risulta come , sommando tutti i parametri considerati , il costo differenziale di una indagine angiografica degli arti inferiori risulti presso il nostro istituto di 238 , 18 euro . costi comuni abbiamo indicato con lespressione costi comuni i costi dei fattori produttivi , interni allunit clinico operativa di radiologia , che garantiscono unattivit di supporto a tutti gli atti diagnostici svolti nellunit operativa . 
non siamo in grado di effettuare unanalisi dettagliata delle attivit di supporto per quantizzare il contributo di questi fattori produttivi alle diverse procedure ( criterio causale ) , per cui rimane lalternativa di ricorrere al metodo della media , ipotizzando che ciascuna indagine radiologica usufruisca in pari misura di tali servizi , vale a dire che le specificit di ciascuna indagine non siano una determinante dei costi di cui stiamo trattando . 
non riteniamo che il loro lavoro sia influenzato dalla tipologia degli esami svolti e quindi il loro costo complessivo stato ripartito proporzionalmente su tutte le indagini eseguite presso lunit clinico operativa di radiologia . i materiali di supporto comprendono computer , stampanti , registratori , materiale elettrico e di rete , materiale di cancelleria e materiale di pulizia . 
ne risulta un costo comune aggiuntivo per esame di 5 , 62 euro . costo pieno sommando i costi differenziali con i costi comuni , stato calcolato il costo pieno di ciascuna indagine ( tabella 1 ) , ovvero : 1 . 
angio - rm : 186 , 14 euro + 5 , 62 euro = 191 , 76 euro ; 2 angiografia digitale : 238 , 18 euro + 5 , 62 euro = 243 , 8 euro . in tutti i pazienti che vengono sottoposti ad indagini contrastografiche che prevedono limpiego di un mezzo di contrasto organo iodato ( in questo caso si tratta dellesame angiografico ) viene effettuato un prelievo ematico per valutarne i livelli sierici di glucosio e creatinina a cui vengono aggiunti i parametri emocoagulativi ( inr , assetto piastrinico ) per un costo complessivo di 7 , 50 euro per esame . 
questo costo non rientra tra i costi differenziali dellesame , per riteniamo non scorretto sottolineare come langiografia venga cos a pesare maggiormente sui costi allesterno della struttura radiologica rispetto allangio - rm . 
opportuno infine ricordare , come gi precedentemente accennato , che circa nell1% dei pazienti che vanno sottoposti ad esami angiografici , essendoci unanamnesi allergica positiva , si esegue anche una preparazione farmacologica ( basata sullimpiego di cortisonici associati ad anti - h1 ed anti - h2 ) , per un costo di 4 euro , in media 0 , 04 euro in pi per ogni esame . 
 complessivamente , questi costi esterni alla radiologia ammontano a 7 , 54 euro . discussione e conclusioni lanalisi dei costi ha dimostrato un costo superiore del 27 , 1% dellangiografia digitale rispetto allangio - rm nella valutazione delle arterie degli arti inferiori ( 243 , 8 versus 191 , 76 euro )  . 
factors with the highest impact are supplies used in the procedure and personnel costs ( owing to the longer examination time )  . decisions concerning the treatment to be pursued after ascertaining that treatment is indeed required will also affect overall cost calculation [ 1417 ]  . indeed , mra may or may not evidence lesions requiring surgical treatment with percutaneous transluminal angioplasty ( pta ) and / or stent placement . 
in this event , the cost of the mra examination should be subsequently added to the costs of intra - arterial angiography and the costs for 1 day in hospital after the interventional procedure ( however , costs of hospitalisation are not included in our analysis , which assesses only costs incurred by the radiology unit )  . it would also be possible to perform angiography first , combining the diagnostic and therapeutic parts in one session , thereby avoiding mra examination . this approach would have to take into account an additional hypothetical , non - predictable workload for the section and delays or cancellations of scheduled examinations because of possible complications arising during the procedure . in our personal experience , however , diagnostic and interventional procedures are usually performed separately . it should also be noted that after diagnostic angiography with arterial catheterisation , the patient is usually hospitalised to monitor possible complications such as bleeding . therefore , external costs of hospitalisation need to be considered . on the other hand , an alternative to manual compression and hospitalisation is to apply an intra - vasal haemostatic device ( angio - seal ) [ 18 ]  . if the device is applied at the end of the procedure , the patient can be mobilised immediately without serious complications or longer examination times [ 19 ]  . 
however , the use of this device entails a cost of 139.44 euro , which , although cheaper than 1 day in hospital , directly weighs on our units budget . 
if it were used , it would then have considerable impact on the full costs of dsa . hospitalisation may also be avoided by monitoring the patient for 5 h after a 15 - min compression and then conducting a telephone follow - up up to the seventh day [ 20 , 21 ]  . 
a further alternative to avoid hospitalisation may be to perform the diagnostic examination with a brachial as opposed to femoral access . the cost analysis we conducted employed a technique often applied in industry , which ensures a rigour that reduces fattori che incidono maggiormente sono rappresentati dal costo del materiale utilizzato durante la procedura e dal costo del personale ( questultimo legato , a parit di figure professionali coinvolte , alla maggior durata dellesame angiografico )  . 
vi infatti la possibilit che langio - rm non evidenzi lesioni passibili di trattamento interventistico mediante pta e / o posizionamento di stent , oppure al contrario che dimostri lesioni suscettibili di tali trattamenti . 
in questo secondo scenario , al costo dellesame angio - rm andrebbero successivamente aggiunti i costi relativi allesame angiografico eseguito mediante accesso arterioso e i costi relativi ad un giorno di degenza post - procedura interventistica ( i costi di degenza non rientrano peraltro nella nostra analisi che valuta i costi allinterno dellunit clinico operativa di radiologia )  . vi sarebbe peraltro la possibilit di eseguire in primis langiografia , effettuando cos in ununica seduta sia la parte diagnostica che la parte terapeutica , evitando in tal modo lesame di angio - rm . 
tale atteggiamento dovrebbe tenere in considerazione il carico di lavoro ipotetico aggiuntivo non prevedibile della sezione e eventuali ritardi o annullamento di esami programmati a causa di eventuali complicanze insorte in corso di procedura . 
esso tuttavia presenta un costo di 139 , 44 euro che , pur essendo inferiore al costo di un giorno di degenza , grava direttamente sul budget dellunit clinico operativa di radiologia . qualora utilizzato , esso graverebbe quindi considerevolmente sui costi pieni dellangiografia digitale . la degenza ospedaliera pu anche essere evitata eseguendo al termine di una compressione di 15 minuti un monitoraggio temporaneo del paziente per 5 ore e successivamente un follow - up telefonico fino alla 7a giornata [ 20 , 21 ]  . 
 unulteriore alternativa per evitare la degenza pu essere costituita da un esame diagnostico eseguito con accesso brachiale anzich femorale . lanalisi dei costi da noi condotta fa riferimento a una tecnica ampiamente utilizzata in campo industriale che garantisce un rigore che riduce le approssimazioni dei metodi tradizionali di calcolo dei costi [ 22 ]  . 
they reflect the situation in our department at a certain moment in time , but costs in other radiology departments may be extremely different to assess , either owing to different costs of equipment used or simply because of different organisation , which can affect variable costs ( different materials used ) or personnel costs ( possible different roles )  . 
in our view , this does not detract from the validity of our analysis , but it emphasises its value in suggesting a model that can be easily applied to other settings rather than for reported cost data . this can therefore be a stimulus for similar cost evaluations of these two techniques , possibly considered within more complex diagnostic protocols or in comparison with other techniques , such as ct angiography . clearly , a cost analysis is only the first step towards a cost - effectiveness analysis , which considers both the diagnostic benefits , including impact on therapy , and biological costs . the high diagnostic accuracy of mra in the evaluation of lower - limb arteries is an established fact [ 111 ]  . 
in addition , mra no doubt offers clear advantages over angiography if biological costs are considered since it is non - invasive , involves no ionising radiation and makes use of a paramagnetic contrast agent , which is safer than organic iodinated products . 
these elements led to a quick transition from dsa to mra in the diagnosis of lower - limb arterial disease in our department . in 2004 , mra was carried out on all patients with this clinical condition , reserving dsa to a mere 4% of cases , i.e. those with contraindications to mri . tuata in questo campo applicativo risulta comparabile ad un solo lavoro in letteratura [ 23 ] , mentre negli altri [ 14 , 24 ] si fa riferimento alle tariffe di angio - rm ed angiografia digitale e non ad una valutazione dei costi reali . 
vi sono soprattutto differenze operative che giustificano questa diversit , tra le altre il computo del costo del mantenimento del paziente sorvegliato per 34 ore in un letto predisposto nel servizio di radiologia dopo leffettuazione dellangiografia e il minimo coinvolgimento del medico radiologo ( stimato in soli 7 minuti ) per leffettuazione e la refertazione dellangio - rm . 
essi rappresentano una fotografia della situazione nella nostra struttura in un certo momento storico , ma evidente che in altre strutture i costi possono essere estremamente diversi , vuoi per il costo diverso delle apparecchiature utilizzate o semplicemente per diverse scelte organizzative che possono incidere ad esempio sui costi variabili ( per diversi materiali utilizzati ) o sui costi del personale , qualora ne sia previsto un diverso impiego . 
ci non toglie a nostro giudizio validit a tale analisi , ma sottolinea il suo valore non tanto per i dati grezzi di costo riportati quanto per il suggerimento di un modello facilmente applicabile in altre realt operative . ci pu quindi essere stimolo per analoghe valutazioni dei costi di queste due tecniche , eventualmente inserite anche in protocolli diagnostici pi articolati o in raffronto ad altre indagini , quale langio - tc . 
chiaro che unanalisi dei costi rappresenta solo un primo tassello per giungere ad unanalisi costo - efficacia , che consideri quindi da un lato i benefici diagnostici , includendo le ricadute terapeutiche , e dallaltro i costi biologici . 
lelevata accuratezza diagnostica dellangio - rm nella valutazione delle arterie degli arti inferiori un dato acquisito [ 111 ]  . non vi dubbio inoltre che , per quanto riguarda i costi biologici , langio - rm offre chiari vantaggi rispetto allangiografia , per lassenza di invasivit , lassenza di radiazioni ionizzanti e lutilizzo di un mezzo di contrasto paramagnetico , pi sicuro di un prodotto organo - iodato . 
the purpose of this study was to investigate supraspinatus tendon sonographic morphology in a population of young overhead athletes in correlation with main pathologic models of secondary shoulder impingement syndrome . 
between april and may 2004 , 20 subjects ( ten professional basketball players and ten non - athlete controls of the same age , weight and height ranges ) underwent bilateral , standardised , sonographic sholulder examination to evaluate supraspinatus echotexture , supraspinatus and subacromial bursa thickness , subacromial space width ( cutoff of 7 mm ) and dynamic anterior impingement beneath the acromial marg results . 
despite the study limitations , ultrasonography ( us ) is able to detect subacromial space narrowing in young overhead athletes as early shoulder impingement sign , according to the continuum impingement - instability pathologic model . key words sport lesions sonographic examination of shoulder sonographic examination of tendons subacromial impingement syndrome shoulder instability riassunto obiettivo . 
quattro giocatori mostravano segni e sintomi di instabilit di spalla atraumatica destra ( 2 casi ) o di impingement del sovraspinato con dolore anteriore di spalla ( 1 spalla destra ed 1 spalla sinistra )  . 
nonostante i limiti dello studio , lecografia in grado di individuare il restringimento dello spazio subacromiale in atleti overhead giovani come segno precoce di impingement del sovraspinato , in accordo con il modello patogenetico del continuum impingement - instabilit . parole chiave lesioni da sport spalla , ecografia tendini , ecografia sindrome di impingement subcromiale instabilit introduction introduzione r . 
among shoulder pathologies , secondary supraspinatus impingement syndrome frequently affects so - called overhead sports players , sometimes with the risk of compromising athletic careers [ 1 ]  . during the last few years , increasing understanding and subtler classification of pathologic mechanisms responsible for this condition have enabled more appropriate orthopaedic treatments than in the past , leading to more acceptable clinical and functional results [ 2 ]  . 
all subjects underwent preliminary clinical examination as previously described [ 7 ] , including neer and hawkins tests for anterior and posterior impingement and apprehension and relocation tests for instability . standardised morphological study of the supraspinatus tendon was performed by a senior sonographer with 10 - years experience in musculoskeletal radiology targeted to tendon il movimento overhead , caratterizzato dalla elevazione del braccio al di sopra dei 90 associato ad abduzione ed extrarotazione , caratteristico di diverse discipline sportive e la sua biomeccanica ed i riflessi patologici sullarticolazione di spalla sono stati ampiamente studiati negli ultimi anni [ 1 ]  . fra le patologie di spalla la sindrome da impingement secondario del tendine sovraspinato affligge di frequente i giocatori di sport cosiddetti overhead , comportando il rischio di compromettere la carriera atletica [ 1 ]  . 
negli ultimi anni una comprensione progressiva ed una classificazione pi approfondite dei meccanismi patogenetici responsabili di questa condizione hanno permesso trattamenti ortopedici pi appropriati rispetto al passato con risultati pi accettabili in termini clinici e di recupero funzionale [ 2 ]  . 
il tendine del sovraspinato coinvolto elettivamente nei disordini secondari della cuffia dei rotatori , indipendentemente dalla loro etiologia [ 3 ]  . lecografia , specialmente in mani di operatori esperti , considerata attualmente indagine di primo livello nella diagnosi di impingement o di lesioni del sovraspinato , in virt della elevata risoluzione spaziale , del buon contrasto tissutale e della multiplanariet , con risultati sovrapponibili a quelli della rm specie nellindividuazione e nella quantificazione delle lesioni tendinee [ 4 ]  . 
i criteri di esclusione erano rappresentati da alterazioni muscolari dovute a precedenti traumi di spalla , malattie sistemiche muscoloscheletriche e / o assunzione corrente di fans o di steroidi . tutti i soggetti sono stati sottoposti in via preliminare ad una visita clinica come precedentemente descritto [ 7 ] , comprendente i test di neer e di hawkins per limpingement anteriore e posteriore ed i test di apprensione e di relocation per linstabilit . 
lo studio morfologico standardizzato del tendine sovraspinato stato eseguito da un ecografista esperto con 10 anni di esperienza nel settore muscoloscheletrico , mirato ai siti tendinei ed extra - tendinei tipicamente coinvolti nella sindrome da impingement [ 8 ]  . 
lo spessore del tendine stato misurato in prossimit dellinserzione sulla testa omerale , fra la superficie inferiore della borsa ed il margine inferiore visibile della struttura fibrillare . and extra - tendon sites of typical involvement in impingement syndrome [ 8 ]  . 
examination starts with the probe placed parallel to the longitudinal tendon axis ( paracoronal plane ) with the shoulder internally rotated and extended by positioning the arm behind the back in order to increase the extent of supraspinatus lateral to the acromial shadow [ 9 ]  . 
lo spessore del tendine stato misurato dalla sutable 1 tendon echotexture was interpreted based on a division into grades , following neers classification of tendon tears [ 10 ] tendon echotexture fibrillar hypoechoic hyperechoic iiia partial tear iiib full - thickness tear tabella 1 lecostruttura del tendine stata interpretata in base ad una suddivisione in gradi , operata sulla falsariga della classificazione di neer delle lesioni tendinee [ 10 ] ecostruttura del tendine fibrillare ipoecogena iperecogena iiia iiib lesione parziale lesione a tutto spessore table 2 criteria for interpretation of the other sonographic parameters considered [ 9 , 10 ] increased reduced tendon thickness , mm bursal thickness , mm subacromial space , mm anterior impingement spazio subacromiale , mm impingement anteriore normal present normale presente absent assente tabella 2 criteri di interpretazione degli altri parametri ecografici considerati [ 9 , 10 ] spessore del tendine , mm spessore della borsa subacromiale , mm aumentato ridotto r . 
dynamic passive abduction of the arm from this position assesses tendon integrity and the presence or absence of tendon impingement beneath the acromial margrepositioning the arm in the original posiperficie inferiore della borsa perpendicolarmente fino al margine inferiore dove lecostruttura fibrillare risulta chiaramente visibile . 
la sonda successivamente posizionata perpendicolarmente al maggior asse tendineo ( piano parasagittale ) , con lavambraccio flesso a 90 sul braccio , a sua volta addotto al tronco con la mano poggiata sulla spalla controlaterale . la successiva abduzione passiva del braccio volta a stabilire lintegrit del tendine e la presenza od assenza di impingement del tendine al di sotto del margine dellacromion . 
none of the sonographic measurements is pathological in relation to the criteria selected mean bursal thickness , mm tendon thickness , mm subacromial space , mm impingement echotexture spessore borsa , mm spessore tendine , mm spazio subacromiale , mm impingement ecostruttura dx , spalla destra ; sx , spalla sinistra ; ds , deviazione standard r , right shoulder ; l , left shoulder ; sd , standard deviation tabella 4 reperti ecografici nei soggetti di controllo non - atleti . 
4a , b player with right shoulder paon the basis of the selected cut - off , the width of the right subacromial space is moderately reduced ( a ) whereas the contralateral space ( b ) is normal . 
measurement of the subacromial space in the parasagittal scan , lateral to the acromion shadow cone , between the point of entry of the tendon at dynamic abduction and the humeral - head cortical fig . 
misurazione dello spazio subacromiale in scansione parasagittale , effettuato lateralmente al cono dombra dellacromion fra il punto di ingresso del tendine alla manovra dinamica di abduzione e la corticale della testa omerale r . 
imaging was interpreted following criteria reported in tables 1 and 2 , according to expected clinical and sonographic patterns previously described [ 9 , 10 ] and choosing a cut - off of 7 mm for subacromial space width . 
statistical analysis on measurements lacking a definite cut - off for pathology ( tendon and bursal thicknesses ) was based on a two - tailed u mann - whitney test whereas the one - tailed fisher exact test was used for the other parameters . 
four players showed symptoms and positive clinical signs of secondary supraspinatus impingement syndrome at an early stage : two right shoulder atraumatic instability ( previous spontaneous subluxation episode in one case ) , and anterior shoulder pain in one right assenza di restringimento per lampiezza dello spazio subacromiale . 
lanalisi statistica sulle misure che difettavano di un cut - off patologico definito ( spessori del tendine e della borsa ) si avvalsa di un test u di mann - whitney a due code , mentre per gli altri parametri stato utilizzato il test esatto di fisher ad una coda ; in entrambi i casi il livello di significativit era fissato al 5% ( p < 0 , 05 )  . risultati tutti i soggetti erano destrimani . 
quattro giocatori mostravano sintomi e test clinici positivi suggestivi di impingement secondario del sovraspinato ad uno stadio iniziale : 2 instabilit atraumatiche di spalla destra ( episodio di sublussazione spontanea in 1 caso ) e dolore anteriore di spalla a carico di 1 spalla destra e di 1 spalla sinistra ( con scrosci articolari nel primo caso )  . 
i rilievi ecografici sono riportati neltabella 6 classificazione secondo belling srensen e jrgensen dellimpingement della cuffia dei rotatori secondo il modello del continuum impingement - instabilit ( modificata da [ 2 ] ) r . 
no significant sonographic differences were found between players and controls in tendon echotexture ( all cases classified as grade 0 ) and in dynamic anterior impingement testing ( absent in all cases )  . 
gli spessori del tendine e della borsa subacromiale non mostrano significativa differenza fra le spalle di destra e di sinistra allinterno dello stesso gruppo e fra i 2 gruppi ( p > 0 , 05 ) ( tabella 5 )  . 
lo spazio subacromiale risulta ridotto in ampiezza sia a destra ( a ) che a sinistra ( b ) , pur in assenza di alterazioni ecostrutturali a carico del tendine sovraspinato e della borsa subacromiale . discussion basketball is considered an overhead sport due to repeated shooting and passing , throwing - like movements , studied in the throwing model , characterised by typical elevation - abduction - extrarotation of the arm , which lead to functional overload and mechanical stress of the supraspinatus [ 11 ]  . 
neers pathogenic model , which explains primary supraspinatus impingement as a consequence of a primitive narrowing of the subacromial space , cannot alone explain the association of supraspinatus lesions with shoulder instability in overhead players [ 12 ] , as demonstrated by the fact that surgical intervention on instability does provide symptom relief and acceptable functional recovery whereas acromionplasty and / or surgical - cuff decompression fails this goal in most cases [ 13 ]  . 
a supraspinatus tendon can be damaged , primarily as a consequence of an eccentric tensile overload responsible of tears [ 15 ] or when chronically impinged during throwing movement between the humeral head and the postero - superior capsular labrum in the so - called postero - superior impingement ( or internal impingement ) [ 13 , 16 ]  . 
according to the continuum impingement - instability pathologic and clinical model , supraspinatus impingement in overhead athletes would be a consequence of a primary narrowing of the subacromial space that occurs in a spectrum of clinical conditions , which vary from pure impingement as described by neer , usually more frequent in older athletes ( > 35 years ) , to pure instability , prevailing in young athletes ( 1835 years )  . 
in our series , in comparison to a control group of ten non - athlete subjects with no clinical or sonographic evidence of supraspinatus impingement , 6 / 10 modello del lancio , caratterizzati dalla tipica elevazione - abduzione - extrarotazione del braccio e responsabili di sovraccarico funzionale e di stress meccanico del tendine sovraspinato [ 11 ]  . 
il modello patogenetico di neer , che riconduce limpingement primario del sovraspinato ad un restringimento primitivo dello spazio subacromiale , non in grado di spiegare da solo lassociazione delle lesioni tendinee con linstabilit di spalla [ 12 ] , come dimostrato dal fatto che la correzione chirurgica dellinstabilit determina un beneficio sintomatico ed un recupero funzionale accettabili , mentre lacromionplastica e / o la decompressione chirurgica della cuffia perlopi falliscono questo obiettivo [ 13 ]  . in pi , stata riportata una caratteristica prevalenza di lesioni tendinee del versante articolare piuttosto che di quello bursale negli atleti overhead giovani con spalla dolorosa [ 14 ]  . 
il danno tendineo pu essere primitivo , come conseguenza di un sovraccarico tensivo ( eccentric tensile overload ) responsabile di lacerazioni [ 15 ] o di un impingement cronicamente ripetuto , durante il movimento di lancio , fra la testa omerale ed il labbro capsulare postero - superiore , nel cosiddetto impingement postero - superiore ( o impingement interno ) [ 13 , 16 ]  . secondo il modello patogenetico e clinico del continuum impingement - instabilit limpingement del sovraspinato negli atleti overhead sarebbe conseguenza di una primitiva riduzione in ampiezza dello spazio subacromiale nel contesto di uno spettro continuo di condizioni cliniche variabili dal puro impingement come descritto da neer , di solito pi frequente negli atleti vecchi ( > 35 anni ) , fino allinstabilit pura , prevalente negli atleti giovani ( 1835 anni ) , passando attraverso una serie di condizioni intermedie con caratteristiche miste , ciascuna delle quali richiede un trattamento adeguato ( tabella 6 ) [ 2 , 14 ]  . nella nostra esperienza in confronto ad un gruppo di controllo di 10 soggetti non atleti senza evidenza clinica od ecografica di impingement del sovraspinato , 6 giocatori di basket su 10 hanno mostrato un significativo restringimento dello spazio subacromiale allecografia : di quello destro ( spalla dominante ) in 2 casi asintomatici ed in 1 caso di spalla dolorosa , di quello sinistro ( spalla non dominante ) in 1 caso di r . 
6 the subacromial space of the right shoulders ( dominant ) in the players group is reduced in a significant number of cases compared with the control group ( no reduction )  . 
6 lo spazio subacromiale delle spalle di destra ( dominanti ) nel gruppo dei giocatori ridotto in un numero significativo di casi rispetto al gruppo di controllo ( non riduzione )  . 
us + , spazio subacromiale < 7 mm ; us - , spazio subacromiale 7 msullasse delle ordinate riportato il numero di spalle osservate . basketball players showed sonographic subacromial space narrowing : right dominant in two asymptomatic cases and in one case of painful shoulder , left non - dominant in one case of painful shoulder and bilaterally in two cases of right atraumatic instability . 
because of the insufficient accuracy of this sonographic measurement , despite the fact that reliability comparable to standard radiography has been reported [ 19 ] , we preferred a lower cut - off to be sure of effective space narrowing . 
in particular , no tendon thickness measurements were considered pathologic because of its high interobserver variability reported to be as high as 56% in one study on asymptomatic subjects [ 20 ]  . the same considerations were extended to subacromial bursa thickness . 
the data obtained are in agreement with the concept of a primitive space narrowing in athletes as a cause of supraspinatus impingement , independently from clinical onset and before the sonographic evidence of tendon damage becomes visible . meanwhile , a study [ 21 ] on subject , affected by impingement syndrome undergoing rehabilitation demostrated a significant association between progressive increase of subacromial space ( initially reduced ) and functional recovery . spalla dolorosa e bilateralmente in 2 casi di instabilit destra atraumatica . 
stato scelto un cut - off di ampiezza dello spazio subacromiale di 7 , 0 mm come compromesso fra i valori medi ottenuti nel corso della nostra esperienza clinica ( 6 , 0 mm ) [ de candia , presentato allecr 2002 ] e quelli di soggetti normali misurati in rm con il braccio in posizione neutra abdotto di 30 in due diversi studi ( rispettivamente di 7 + / 1 , 6 mm e di 8 , 18 + / 1 , 0 mm ) [ 17 , 18 ]  . dato lampio margine di inaccuratezza di questa misurazione in ecografia , nonostante essa sia risultata sovrapponibile a quella radiografica utilizzata come standard [ 19 ] , abbiamo preferito un cut - off abbastanza basso per essere sicuri di una effettiva riduzione dello spazio . 
in particolare , nessuna misurazione dello spessore tendineo stata ritenuta anormale , considerato la sua notevole variabilit interosservatore , riportata del 56% in uno studio condotto su soggetti asintomatici [ 20 ]  . analoga considerazione vale per lo spessore bursale . i dati ottenuti sono in accordo con lipotesi di un restringimento primitivo dello spazio subacromiale quale causa di impingement del sovraspinato , indipendentemente dalla manifestazione clinica e prima che si renda evidente allecografia un danno del tendine . ulteriore conferma fornita da uno studio [ 21 ] condotto su soggetti con sindrome da impingement sottoposti a riabilitazione nel quale stata dimostrata una significativa associazione fra lincremento progressivo dello spazio subacromiale ( inizialmente ridotto ) ed il recupero funzionale , suggerendo che la misurazione dello spazio subacromiale possa aiutare ad identificare i soggetti in grado di trarre beneficio dalla riabilitazione . lo studio soffre di alcune limitazioni . 
statistical power is low due to the small population studied , so further studies are required on larger groups of overhead athletes to confirm our results and establish the accuracy of us in detecting early morphological changes in the subacromial space . della variabilit interosservatore ed intra - soggetto delle misurazioni ecografiche , parzialmente compensata dalla stretta aderenza ai criteri di misurazione stabiliti . 
a second - generation us contrast agent was utilised with a high - frequency transducer and a contrast - specific algorithm ( low acoustic pressure cnti )  . the enhancement characteristics of all lesions were analysed using qualitative and quantitative parameters obtained from timeintensity curves with the different imaging modalities . 
the correct assessment of biological behaviour was achieved in all cases by angiosonography ( sensitivity of 100% ; specificity of 91% ) and colour doppler us ( 45% sensitivity ; 78% specificity )  . 
angiosonography is more accurate than colour doppler us in the correct assessment of biological behaviour of suspicious breast lesions . key words breast , neoplastic lesions breast focal lesions power doppler us angiosonography riassunto obiettivo . 
la valutazione del comportamento biologico stata ottenuta con la metodica angiosonografica ( sensibilit del 100% , specificit del 91% ) e con la metodica eco power doppler ( sensibilit 45% , specificit 78% )  . 
langiosonografia rispetto alleco power doppler una metodica pi precisa e affidabile nella corretta valutazione del comportamento biologico delle lesioni mammarie sospette . parole chiave mammella , neoplasie mammella , lesioni focali power doppler us angiosonografia introduction introduzione the past few years have seen a development of ultrasonographic imaging , with refining of power doppler ultrasonography ( us ) and , recently , the use of contrast material . 
angiogenesis is the basis of tumour growth [ 13 ]  . new intravascular contrast agents known as second - generation agents have recently been introduced , which have the in questi ultimi anni si assistito ad uno sviluppo della metodica ecografica , con perfezionamento della tecnica eco power doppler e , pi recentemente , dellutilizzo del mezzo di contrasto ( mdc )  . 
the setting used for power doppler us was optimised to obtain a higher sensitivity for small slow - flow vessels : low wall filter 50 hz , dynamic range 55 db , pulse repetition frequency ( prf ) 7001 , 000 hz . 
lesion vascularity was evaluated on the basis of the number of vessels identified according to the criteria reported in the literature [ 9 ] avascular ( no vascular poles ) , hypovascular ( presence of one or two vascular poles ) , hypervascular ( presence of three or more poles ) and enhancement patterns . 
integration of data and hypothesis of the nature of the lesion ( table 1 ) were obtained on the basis of the literature criteria [ 1012 ] by assigning a score from 0 to 2 to each finding considered : 0 for findings suggestive of benign lesion , 1 for findings present in both benign and malignant lesions , and 2 for findings suggestive of malignant lesion . 
contrast - enhanced sonography was performed with a technos mpx ( cnti technology ) unit and dedicated lineararray probe ( 7.5 mhz la 532 ) with low mechanical index ( less than 0.2 ) and low acoustic power ( 16 kpa )  . 
as a contrast agent , we used the second - generation agent sonovue ( bracco , milan , italy ) [ 13 ] ; biochemically , it consists of sulphur hexafluoride surrounded by phospholipid molecules . 
 the protocol involved pre - setting of the acoustic pressure data ( derate pressure , or dp ) , frequency , mechanical index ( im ) , gains , focuses and depths , injection of rapid bolus of contrast medium ( 2.4 ml in 2 s ) followed by a saline flush ( 4 ml ) , activation of the dedicated software for viewing of the time - intensity curves ( acquisition time set at 2 min ) [ 14 ] and digital storage of all the examination phases and threedimensional ( 3 - d ) reconstruction ( post - processing time 3 min )  . 
total time to carry out the contrast - enhanced examination was approximately 10 min . lesion vascularity was evaluated on the basis of the numgenerazione " che presentano i requisiti chimico - fisici necessari per un loro efficace impiego nella diagnostica ultrasonografica [ 48 ]  . 
il confronto stato fatto con la metodica di eco power doppler . materiali e metodi sono state studiate 20 pazienti di sesso femminile det compresa tra i 28 e 73 anni ( et media di 46 , 25 anni )  . 
ogni paziente presentava una lesione mammaria con caratteristiche mammografiche e / o ecografiche sospette gi sottoposta a fnac ( fine needle aspiration citology ) risultata inadeguata ; in particolare 6 / 20 erano inadeguati ( c1 ) , 9 / 20 presentavano atipie probabilmente benigne ( c3 ) ; 5 / 20 atipie probabilmente maligne ( c4 )  . lo studio stato effettuato in modo prospettico ed in doppio cieco da due osservatori . 
ogni lesione stata sottoposta a diagnosi istologica e valutazione immunoistochimica con marcatore anticorpale endoteliale cd34 . il setting utilizzato per leco power doppler stato ottimizzato per ottenere una maggiore sensibilit ai vasi piccoli con flussi lenti : basso filtro di parete 50 hz , range dinamico 55 db , frequenza di ripetizione degli impulsi ( prf 7001000 hz )  . lacquisizione stata limitata alla lesione sospetta ed a parte ( 10 mm ) del tessuto circostante . 
la vascolarizzazione della lesione stata valutata in base al numero dei vasi identificabili secondo i criteri riportati in letteratura [ 9 ] ( avascolare assenza di poli vascolari , ipovascolarizzata presenza duno o due poli vascolari , ipervascolarizzata presenza di pi di tre poli ) ed al pattern di enhancement . 
lintegrazione dei dati e lipotesi di natura ( tabella 1 ) sono state ottenute sulla base dei criteri della letteratura [ 1012 ] , affiancando ad ogni aspetto considerato un punteggio da 0 a 2 : 0 agli aspetti ritenuti suggestivi per lesione benigna , 1 agli aspetti presenti sia nelle lesioni benigne che maligne , 2 agli aspetti suggestivi per lesione maligna . se il punteggio minore di 3 la lesione probabilmente benigna ; se maggiore di 3 la lesione probabilmente maligna . lecografia con mdc stata effettuata con ecotomografo technos mpx ( tecnologia cnti ) e sonda lineare dedicata ( modello la 532 da 7 , 5 mhz ) multibanda con basso indice meccanico ( minore di 0 , 2 ) e bassa potenza acustica ( 16 kpa )  . 
il mdc utilizzato stato il sonovue ( bracco , milano , italia ) , mezzo di contrasto ecografico di seconda generazione [ 13 ] ; dal punto di vista biochimico si tratta di esafluoruro di zolfo circondato da molecole di fosfolipidi . 
il protocollo utilizzato ha previsto la regolazione dei dati di pressione acustica ( derate pressure o dp ) , frequenza , indice meccanico ( mi ) , guadagni , fuochi e profondit che sono stati pre - impostati e non modificati per tutta la durata dellesame , liniezione in bolo rapido di mdc ( 2 , 4 ml in 2 s ) seguito da flush di soluzione fisiologica ( 4 ml ) , lattivazione di software dedicato per la visualizzazione di curve intensit / tempo ( tempo dacquisizione fissato a due minuti ) [ 14 ] ed infine larchiviazione digitale di tutte le fasi dellesame e ricostruzione 3d , tempo di post - processing 3 minuti . 
peak intensity was evaluated in percent using the formula ( [ post - contrast signal pre - contrast signal ] / precontrast signal ) 100 [ % ] [ 1517 ] : < 50% no or slight increase , 50%100% moderate , over 100% marked . 
the curve pattern after the peak allowed us to identify three types of curves : type 1 with maximum signal intensity after 60 s and slow washout , type 2 with maximum intensity after 30 s and rapid washout , type 3 with maximum intensity after 30 s and multiple peaks during washout . 
integration of data and hypotheses as to the nature [ 10 ] ( table 2 ) were obtained by assigning a score from 0 to 2 to each of the aspects considered . 
each patient underwent surgical biopsy for a histological diagnosis ; microvessel density was obtained for histological sections of the most representative portion of the lesion stained with cd34 using the standard avidin - biotin - peroxidase procedure [ 3 , 15 , 18 , 19 ]  . 
 [ 2 ] with some changes : in the histological sections , the area with the highest concentration of vessels was identified and a subjective score assigned on a scale from + 1 to + 4 ; the highest count and the mean of the areas analysed were then recorded as maximum and mean microvessel density . 
both the vessel count and the subjective evaluation ( from + 1 to + 4 ) of the lesion were carried out by a single pathologist unaware of the results of the imaging examinations . con mezzo di contrasto stato di 10 minuti circa . la vascolarizzazione della lesione stata valutata in base al numero dei poli vascolari identificati , al pattern di enhancement intenso ed omogeneo , intenso e disomogeneo , assente [ 14 ] ed alla valutazione delle curve intensit / tempo ottenute posizionando delle roi nelle regioni giudicate da ciascun osservatore di maggior enhancement . 
le curve sono state classificate come benigne e maligne in base al tempo di comparsa del picco dintensit del segnale ed allandamento della curva dopo il picco . lintensit di picco stata valutata in percentuale usando la formula ( [ segnale post - contrasto segnale pre - contrasto ] / segnale pre - contrasto ) x100 [ % ] [ 1517 ] : < 50% , nessuno o debole incremento , 50%100% , moderato , oltre 100% , marcato . landamento della curva dopo il picco ha permesso di identificare tre tipi di curve : tipo 1 , con massima intensit di segnale dopo 60 secondi e lento wash - out ; tipo 2 , con massima intensit dopo 30 secondi e rapido decremento ; tipo 3 , con massima intensit dopo 30 secondi e multipli picchi in fase di wash - out . ogni lesione stata valutata per forma ( ovale , rotondeggiante e spiculata ) e per margini ( netti , sfumati )  . 
lintegrazione dei dati e lipotesi di natura [ 10 ] ( tabella 2 ) sono state ottenute , come per la metodica precedente , affiancando ad ogni aspetto un punteggio da 0 a 2 . 
ciascuna paziente stata sottoposta a biopsia chirurgica per la diagnosi istologica ; la densit microvascolare stata ottenuta da sezioni istologiche della parte pi rappresentativa della lesione colorata con cd34 con metodo standard avidina - biotina - perossidasi [ 3 , 15 , 18 , 19 ]  . 
sia la conta dei vasi che la procedura di valutazione soggettiva su base graduale ( da + 1 a + 4 ) della lesione stata effettuata dallo stesso patologo che non era a conoscenza dei risultati delle indagini radiologiche . results eleven out of 20 lesions were benign at histology and nine out of 20 were malignant . 
at fnac , the 20 lesions were distributed as follows ( table 3 ) : c1 ( inadequate sample ) 6 / 20 , of which there were two fibroadenomas , one adenosis , two nos infiltrating ductal carcinomas and one ductal carcinoma in situ c3 ( probably benign ) 9 / 20 , of which there were four fibroadenomas , one adenosis , one fibrocystic disease , two nos infiltrating ductal carcinomas and one infiltrating lobular carcinoma c4 ( suspicious of malignancy ) 5 / 20 , of which there were one fibroadenoma , one fibrocystic disease , two nos infiltrating ductal carcinomas and one recurrence on a scar of infiltrating ductal carcinoma . at power doppler us , analysis of lesion vascularity revealed the presence of ten avascular lesions , six hypovascular lesions , and four hypervascular lesions . 
this result was correlated with the histological findings ( table 4 ) : 6 / 9 of malignant lesions were found to be avascular ( four lesions ) or hypovascular ( two lesions )  . 
these results were compared with those obtained with power doppler us and correlated with the histological diagnosis : none of the malignant lesions was avascular after administration of contrast material , and the hypovascular lesions ( 1 / 9 ) proved to be malignant istologico , di natura benigna e 9 su 20 di natura maligna , in particolare , 7 erano dei fibroadenomi , 2 delle adenosi e 2 delle lesioni riconducibili ad un quadro di mastopatia fibrocistica ; 6 erano carcinomi duttali infiltranti di tipo nas , 1 carcinoma lobulare infiltrante , 1 recidiva su cicatrice di carcinoma duttale infiltrante e 1 carcinoma duttale in situ . allindagine fnac le 20 lesioni erano state cos distribuite ( tabella 3 ) : c1 ( inadeguato ) 6 / 20 di cui 2 fibroadenomi , 1 adenosi , 2 carcinomi duttali infiltranti di tipo nas e 1 carcinoma duttale in situ ; c3 ( verosimilmente benigno ) 9 / 20 di cui 4 fibroadenomi , 1 adenosi , 1 mastopatia fibrocistica , 2 carcinomi duttali infiltranti di tipo nas e 1 carcinoma lobulare infiltrante ; c4 ( sospetto maligno ) 5 / 20 di cui 1 fibroadenoma , 1 mastopatia fibrocistica , 2 carcinomi duttali infiltranti tipo nas e 1 recidiva su cicatrice di carcinoma duttale infiltrante . allesame eco power doppler la vascolarizzazione delle lesioni , determinata in base ai criteri puntualizzati nei materiali e metodi , ha dimostrato la presenza di 10 lesioni avascolari , 6 ipovascolarizzate , e 4 ipervascolarizzate . 
tale risultato stato correlato con il reperto istologico ( tabella 4 ) : 6 / 9 delle lesioni maligne sono risultate avascolari ( 4 lesioni ) o ipovascolarizzate ( 2 lesioni )  . il giudizio complessivo , considerando gli altri parametri analizzati ( pattern radiale o periferico ; analisi spettrale ) , stato di 13 lesioni benigne e 7 maligne . 
la metodica ha dimostrato una sensibilit del 45% ed una specificit del 78% . lo studio della vascolarizzazione delle lesioni con metodica angiosonografica ha permesso l ' identificazione di 3 lesioni avascolari , 8 ipovascolarizzate e 9 ipervascolarizzate . 
tali risultati sono stati confrontati con quelli ottenuti dallo studio eco power doppler e correlati con la diagnosi istologica : nessuna delle lesioni maligne risultata avascolare dopo somministrazione di mdc e le lesioni ipovascolarizzate ( 1 / 9 ) sono risultate maligne ( tabella 4 )  . le curve ottenute dopo studio angiosonografico hanno morfologia diversa nelle lesioni benigne rispetto a quelle malif . 
nos not otherwise specified cytology histology angiosonography : vascularity angiosonography : final evaluation after scoring notes * 3 benign * 3 malignant * 3 benign 1 hypervascular * 6 benign * 3 malignant * 5 benign * 4 malignant * 2 benign * 3 malignant * 2 benign * 3 malignant 2 fibroadenomas 1 adenosis 2 nos infiltrating ductal carcinomas 1 ductal carcinoma in situ 4 fibroadenomas 1 adenosis 1 fibrocystic disease 2 nos infiltrating ductal carcinomas 1 infiltrating lobular carcinoma 1 fibroadenoma 1 fibrocystic disease 2 nos infiltrating ductal carcinoma 1 carcinoma 2 fibroadenomi 1 adenosi 2 carcinomi duttali infiltranti tipo nas 1 carcinoma duttale in situ 4 fibroadenomi 1 adenosi 1 mastopatia fibrocistica 2 carcinomi duttali infiltranti nas 1 carcinoma lobulare infiltrante 1 fibroadenoma 1 mastopatia fibrocistica 2 carcinomi duttali infiltranti nas 1 carcinoma 2avascular 1 hypovascular 2 hypervascular 4 hypovascular 1 hypovascular 1 hypovascular 2 hypervascular 1 hypervascular 1 avascular 1 hypovascular 2 hypervascular 1 hypervascular 2 avascolari 1 ipovascolare 2 ipervascolari 1 ipervascolare 4 ipervascolari 1 ipovascolare 1 ipovascolare 2 ipervascolari 1 ipervascolare 1 avascolare 1 ipovascolare 2 ipervascolari 1 ipervascolare * 3 benigni * 3 maligni * 3 benigni * 3 maligni * 6 benigni * 3 maligni * 5 benigni * 4 maligni * 2 benigni * 3 maligni * 2 benigni * 3 maligni angiosonography : all lesions detected correctly cytology : inadequate * 3 malignant angiosonography : 8 / 9 lesions interpreted correctly , 1 false positive cytology : 6 / 9 lesions truly benign angiosonography : all lesions detected correctly cytology : 3 / 5 lesions identified correctly angiosonografia : ha identificato correttamente tutte le lesioni citologia : inadeguata angiosonografia : 8 / 9 lesioni giustamente interpretate , 1 falso positivo cytology : 6 / 9 lesioni realmente benigne angiosonografia : tutte le lesioni correttamente identificate citologia : 3 / 5 lesioni identificate correttamente tabella 3 confronto tra i risultati ottenuti con fnac e angiosonografia citologia istologia angiosonografia : vascolarizzazione angiosonografia : valutazione finale dopo score note ( table 4 )  . 
for all of masses analysed , there was a significant correlation between cd34 microvessel density and the results of angiosonography ; in particular , there was correlation between the vascular density index obtained at histology and the area under the curve . 
 precoce , di intensit pi elevata rispetto a quanto ottenuto nella patologia benigna , con wash - out ad andamento progressivo ma irregolare . il giudizio prognostico , considerando il pattern di enhancement e lo studio delle curve intensit / tempo , stato di 10 lesioni benigne e 10 lesioni maligne . 
la metodica ha mostrato una sensibilit del 100% ed una specificit del 91% . per tutte le masse analizzate si evidenziata una significativa correlazione tra la densit microvascolare con cd34 ed i risultati dellangiosonografia ; in particolare stata valutata la correlazione tra lindice di densit vascolare ottenuto dallesame istologico e larea sotto la curva . il mezzo di contrasto si rilevato sicuro , solo una paziente ha manifestato una cefalea della durata di un paio dore verosimilmente correlata con lindagine angiosonografica . the formation of new blood vessels in neoplastic disease is of fundamental importance for tumour growth and spread [ 13 ]  . 
power doppler us and the use of contrast material offer the possibility of studying the vascularity of a lesion in order to establish its nature ( benign or malignant lesion )  . 
power doppler us proved to have low sensitivity ( 45% ) and specificity ( 78% ) compared with angiosonography , which had a sensitivity of 100% and a specificity of 91% . 
despite the care taken in setting the sonographic parameters and reducing movement artefacts , power doppler us proved to be unreliable in identifying neoplastic lesions with slow flow and abundant fibrotic component ( four malignant lesions were found to be avascular )  . 
in addition , two hypervascular lesions interpreted as malignant even after quantitative assessment [ radiation intensity ( ri ) greater than 0.7 ] turned out to be benign at histology ; this finding was in agreement with previous reports [ 911 ] , which consider flow velocity and resistive index to be less reliable parameters than the morphological assessment of vessels . 
only one case in group c3 ( made up of nine lesions ) was overestimated and considered malignant by angiosonography ( one false positive ) whereas in the same group , fnac had assigned probably benign atypias to three malignant lesions ( three false negatives : two nos infiltrating ductal carcinomas and one infiltrating lobular carcinoma )  . 
few papers have been published that investigate time - intensity curves obtained with us with second - generation contrast agent [ 20 , 21 ] , so the criteria used to classify the types of curve ( intensity and appearance of the enhancement peak ; curve pattern after the peak , washout ) refig . 
tipo 1 con massima intensit di segnale dopo 60 secondi e lento wash - out , tipo 2 con massima intensit dopo 30 secondi e rapido decremento , tipo 3 con massima intensit dopo 30 secondi e multipli picchi in fase di wash - out . stica di fondamentale importanza per la crescita e la disseminazione tumorale [ 13 ]  . le cellule neoplastiche producono fattori di crescita endoteliali specifici quali bfgf ( basic fibroblastic growth factors ) e il vegf ( vascular endoteliar growth factor ) in grado di formare i capillari e gli shunt artero - venosi necessari per la crescita tumorale [ 19 ]  . lesame ecografico con tecnica power doppler e lutilizzo di mdc offrono la possibilit di studiare la vascolarizzazione della lesione al fine di caratterizzarne la natura ( lesione benigna versus lesione maligna )  . 
lesame eco power doppler ha dimostrato una bassa sensibilit 45% e specificit 78% , rispetto alla metodica angiosonografica che ha presentato una sensibilit del 100% ed una specificit del 91% . 
nonostante la massima cura nel settare i parametri ecografici e nel ridurre gli artefatti da movimento , lindagine eco power doppler risultata poco affidabile nellidentificare alcune lesioni neoplastiche con flussi lenti ed abbondante componente fibrotica ( 4 lesioni maligne sono risultate avascolari )  . 
inoltre 2 lesioni ipervascolarizzate interpretate anche dopo la valutazione quantitativa ( ir maggiore di 0 , 7 ) , come maligne , sono risultate allesame istologico benigne ; tale dato concorda con quanto riportato in letteratura [ 911 ] che ritiene la velocit di flusso e lindice di resistenza elementi meno affidabili rispetto alla valutazione morfologica dei vasi . lutilizzo del mdc invece ha ridotto drasticamente il numero delle lesioni identificate come avascolari o ipovascolari definendo correttamente come maligne tutte le lesioni neoplastiche . questi risultati , nonostante la casistica ancora limitata , fanno ben sperare per un ruolo di rilievo dellangiosonografia nelliter diagnostico di lesioni mammarie dubbie o sospette . 
un solo caso appartenente al gruppo c3 ( composto di 9 lesioni ) era stato sovrastimato dallangiosonografia ( 1 falso positivo ) e dato come maligno , mentre nello stesso gruppo fnac aveva assegnato atipie probabilmente benigne a 3 lesioni maligne ( 3 falsi negativi : 2 carcinomi duttali infiltranti di tipo nas e 1 carcinoma lobulare infiltrante )  . 
la differenza di vascolarizzazione tra lesioni benigne e maligne risultata statisticamente significativa solo dopo utilizzo del mdc ( significativit per dati appaiati calcolata con test di mc nemar per c2 con p = 0 , 031 )  . in letteratura sono presenti pochi lavori dedicati alle curve intensit / tempo ottenute dallo studio ecografico con mezzo di contrasto di seconda generazione [ 20 , 21 ] , quindi i criteri utilizzati per classificare i tipi di curva ( intensit e comparsa del picco di enhancement ; andamento della curva dopo il picco wash - out ) rispecchiano quanto codificato in risonanza magnetica con mezzo di contrasto ( cerm ) [ 18 , 2225 ] e negli studi ecof . 
il posizionamento di roi ( d ) permette levidenziazione di curve intensit / tempo di tipo benigno ( e )  . diagnosi istologica : fibroadenoma ( f ) a ricca componente vascolare . 
time - intensity curves obtained after positioning a region of interest ( roi ) ( d ) show a multiphasic malignant pattern ( e ) with rapid wash - in and washout with several peaks . 
le curve intensit / tempo ottenute dopo posizionamento di roi ( d ) presentano morfologia maligna polifasica ( e ) con rapido incremento del segnale e decremento a pi picchi . 
b - mode ultrasonography ( us ) shows a hypoechoic nodule with irregular margins measuring about 1 cm in greatest diameter ( a ) ; power doppler us reveals a major vascular pole ( b ) with mainly peripheral distribution . 
the time - intensity curves obtained after positioning of a region of interest ( roi ) ( d ) have a malignant multiphasic pattern ( e ) with rapid wash - in and wash - out with several peaks . 
le curve intensit / tempo ottenute dopo posizionamento di roi ( d ) presentano morfologia maligna polifasica ( e ) con rapido incremento del segnale e decremento a pi picchi . linterpretazione finale per tutte le metodiche stata di lesione maligna . 
the different shape of the curves seen in benign and malignant lesions after administration of contrast material is explained by the different vascularity of malignant lesions ( presence of arteriovenous shunts ; greater number of anarchically arranged capillaries ) versus benign lesions ( regular vessels even if more than one vascular pole is present )  . 
at power doppler us , this lesion was hypervascular whereas histology revealed areas of capillary invasion by hyperplastic cells with angiogenesis ; such a finding is present in 10% of reported cases of adenosis [ 19 ]  . 
the results obtained definitely support contrast - enhanced us over power doppler us given that the use of contrast material affords greater accuracy in identifying vascularity . grafici con mezzi di contrasto di prima generazione [ 2628 ]  . la diversa morfologia delle curve nelle lesioni benigne versus quelle maligne ottenute dopo somministrazione di mdc da mettere in relazione alla diversa vascolarizzazione delle lesioni maligne ( presenza di shunt artero - venosi ; maggiore quantit di capillari a disposizione anarchica ) versus quelle benigne ( vasi regolari pur nella presenza di pi poli vascolari )  . 
allindagine eco power doppler tale lesione si presentava come ipervascolarizzata mentre , istologicamente , si sono rilevate aree di invasione capillare da parte delle cellule iperplastiche con fenomeni di angiogenesi ; tale rilievo presente in letteratura nel 10% delle adenosi [ 19 ]  . i risultati ottenuti sono sicuramente a favore dellecografia con mdc rispetto a quella di eco power doppler e ci comprensibile vista la maggior accuratezza nellidentificazione vascolare permessa dallutilizzo del mezzo di contrasto . conclusions conclusioni contrast - enhanced us allows the characterisation of suspicious breast lesions and is more sensitive and specific that power doppler us . 
analysis of the time - intensity curves provides a good quantification of microcirculation of a tumour , an essential parameter for evaluating its aggressiveness , and shows a good correlation with the histological data on microvessel density . lecografia con mdc consente di approfondire lo studio ecografico ai fini della caratterizzazione delle lesioni mammarie sospette e risulta essere pi sensibile e specifica dellindagine eco power doppler . 
fugazzola1 1cattedra di radiologia , universit degli studi dellinsubria , viale borri 57 , i - 21100 varese , italy 2oncoematologia , ospedale niguarda c granda , milano , italy 3anatomia patologica , ospedale niguarda c grande , milano , italy 4radiologia , ospedale niguarda c grande , milano , italy 5radiologia , ospedale fatebenefratelli ed oftalmico , milano , italy correspondence : g . 
between 1997 and 2003 , 18 haematologically immunodeficient patients with suspected filamentous fungi infection and negative bronchoalveolar lavage ( bal ) underwent percutaneous pulmonary biopsy to diagnose the nature of the infection . 
in 3 cases , biopsy was not specific , and in one case , the tissue sample was inadequate for a diagnosis ; however , clinical course and response to drugs were compatible with fungal infection . 
tra il 1997 e il 2003 , 18 pazienti ematologici con sospetta infezione da funghi filamentosi , con bal negativo , sono stati sottoposti a biopsia polmonare percutanea per raggiungere una diagnosi di natura dellinfezione . 
in 3 casi , la biopsia risultata non specifica e in un caso il materiale era insufficiente per la diagnosi ; tuttavia , il decorso clinico e la risposta alla terapia erano compatibili con infezione fungina . 
la differenziazione istologica tra aspergillo e mucor importante per pianificare i corretti protocolli terapeutici in quanto il mucor solitamente resistente agli azoli . key words pulmonar fine - needle aspiration biopsy aspergillosis mucor immunodepression parole chiave agobiopsia polmonare aspergillosi mucor immunodepressione g . 
mortality of angioinvasive pulmonary aspergillosis ( apa ) is high , varying from over 50% in leukaemia patients to over 90% in patients undergoing bone marrow transplantation [ 3 ] , despite the availability of new antifungal drugs . 
to reduce significantly the rate of mortality in these patients , diagnosis of the agent responsible for the infection should not only be early but be specific to allow rapid implementation of treatment with the suitable antifungal drug . in neutropenic haematological patients , the finding of persistent fever resistant to broad - spectrum antibiotic therapy or the re - appearance of fever in patient on antibiotic therapy are highly suggestive for mycotic infection [ 4 ]  . 
a proven diagnosis is established only when there is histoor cytopathological evidence of tissue invasion ; otherwise , the diagnosis can only be defined as probable or possible according to european organization for research and treatment of cancer ( eortc ) / national institute of allergy and infectious diseases ( niaid ) mycoses study groups criteria [ 5 ]  . 
in fact , diagnosis is difficult because culture for fungi are often negative ; bronchoalveolar lavage ( bal ) is usually performed in these patients , but sensitivity of the procedure in the detection of aspergillosis is only 50% [ 6 , 7 ]  . 
 some reports have attributed to computed tomography ( ct ) a more reliable diagnostic role than standard chest radiography and clinical and laboratory investigations thanks to the recognition of the halo sign and crescent sign [ 1 , 7 , 912 ]  . 
the purpose of our study was to evaluate the utility of ct and percutaneous ct - guided biopsy in the early and specific diagnosis of fungal pulmonary infections , particularly those due to aspergillus and mucor , in patients with malignant haematological diseases receiving chemotherapy . 
 materials and methods we retrospectively reviewed the results of 18 percutaneous lung biopsies performed from august 1997 to august 2003 in 18 neutropenic haematological patients ( neutrophils < 0.5x109 / l ) with clinical symptoms and radiological findings suggestive of opportunistic infection by filamentous fungi . lincidenza delle infezioni da funghi filamentosi ( aspergillus e mucor ) in aumento nei pazienti ematologici immunodepressi , soprattutto durante la fase di granulocitopenia indotta dal trattamento chemioterapico e nei pazienti sottoposti a trapianto di midollo [ 1 , 2 ]  . 
la mortalit dellaspergillosi polmonare angioinvasiva ( apa ) rimane elevata , variando da oltre il 50% nei pazienti leucemici ad oltre il 90% nei pazienti sottoposti a trapianto di midollo osseo [ 3 ] , nonostante la disponibilit di nuovi farmaci antifungini . 
al fine di ridurre in maniera significativa il tasso di mortalit in questi pazienti necessaria non solo una diagnosi precoce , ma anche di specificit dellagente eziologico responsabile dellinfezione per procedere tempestivamente con il trattamento antimicotico mirato . 
il riscontro , nei pazienti ematologici neutropenici , di febbre persistente , resistente alla terapia antibiotica a largo spettro , o la ricomparsa di febbre in pazienti in terapia antibiotica , sono altamente suggestivi per infezione micotica [ 4 ]  . la diagnosi di certezza viene posta solamente in presenza di evidenza citologica o istologica di invasione tissutale , altrimenti la diagnosi pu solo essere definita come probabile o possibile secondo i criteri eortc / niaid mycoses study groups [ 5 ]  . 
la diagnosi infatti difficile , in quanto le colture per miceti sono spesso negative ; il liquido di lavaggio bronchiolo - alveolare ( bal ) di solito espletato in questi pazienti , ma la sensibilit della metodica nella identificazione di aspergillosi solo del 50% [ 6 , 7 ]  . 
il radiogramma standard del torace rappresenta la metodica di imaging di primo approccio da impiegare nei soggetti con sospetto di patologia polmonare opportunistica ; ci da mettere in relazione alla ubiquitaria disponibilit della metodica ed al miglior rapporto costo / beneficio . 
taluni contributi della letteratura hanno attribuito alla tomografia computerizzata ( tc ) un ruolo diagnostico pi attendibile di quello fornito dal radiogramma standard del torace e dalle valutazioni clinico - laboratoristiche attraverso il riconoscimento dellhalo sign e del crescent sign [ 1 , 7 , 912 ]  . 
scopo del nostro lavoro valutare lutilit della tc nella diagnosi precoce e la sensibilit della biopsia percutanea tc - guidata nella diagnosi specifica delle infezioni polmonari micotiche , in particolare da aspergillus e mucor , nei pazienti affetti da malattie ematologiche maligne e sottoposti a trattamento chemioterapico . materiali e metodi abbiamo revisionato retrospettivamente il risultato di 18 biopsie percutanee polmonari espletate dallagosto 1997 allagosto 2003 in 18 pazienti ematologici neutropenici ( neutrofili < 0 , 5x109 / l ) con sintomatologia clinica e reperti radiografici indicativi di infezione opportunistica da funghi filamentosi . 
dei 18 pazienti , 12 femmine e 6 maschi , con et compresa tra 27 e 64 anni ( et media 49 , 7 anni ) , 13 ( 72 , 2% ) erano affetti da leucemia acuta mieloide , 2 ( 11 , 1% ) in all patients , the main site of infection was the lung ; in one patient , central nervous system ( cns ) involvement was also present . 
of the 18 patients , 12 women and 6 men , with age ranging between 27 and 64 ( mean 49.7 ) years , 13 ( 72.2% ) had acute myeloid leukaemia , 2 ( 11.1% ) had acute lymphoid leukaemia , 2 ( 11.1% ) had non - hodgkins lymphoma and 1 ( 5.6% ) had aplastic anaemia . 
all patients were receiving chemotherapy and had had neutropoenia from 1 to 28 days . clinical symptoms at onset included fever , dyspnoea , nonproductive cough and thoracic pleuritic - like pa all patients were receiving antifungal prophylaxis with nystatin ( n = 7 ) , amphotericin b ( n = 3 ) , itraconazole subcutaneously ( s.c ) ( n = 7 ) or itraconazole per os ( po ) plus nystatin ( n = 1 )  . all patients underwent sputum culture , nose swab exam , anti - aspergillus precipitin evaluation and blood culture for fungi . 
 in all patients , a standard chest x - ray was obtained and subsequently a high - resolution ( hr ) ct exam using ct scanner somatom plus ( siemens medical system , germany )  . 
these exposure parameters , despite increasing the dose to the patient , provided highquality images , reducing the quantic noise due to both technical factors ( reconstruction algorithm , kv and ma , scan time ) and patient factors . 
 patients underwent percutaneous needle biopsy when the platelet count was > 50x109 / l ; time from the beginning of treatment to the biopsy therefore varied from 0 to 172 days . ct - guided biopsy was performed with a 19to 22 - gauge needle for fine needle aspiration after local anaesthesia with 2% lidocaine , preferably on peripheral lesions and limiting the number of passages to two to reduce the risk of pneumothorax . 
a histological diagnosis of aspergillosis was made when biopsy specimens showed typical septate hyphae of uniform calibre with acute - angle dichotomous branches whereas mucormycosis was diagnosed when irregular , broad , non - septate hyphae with rare branches usually at right angles were found [ 13 ]  . 
i pazienti sono stati posti in terapia profilattica con nistatina ( n = 7 ) , con amfotericina b ( n = 3 ) , con itraconazolo s.c. ( n = 7 ) , con itraconazolo cp + nistatina ( n = 1 )  . 
dieci pazienti sono stati sottoposti anche allesame del bal . in tutti i pazienti stato eseguito dapprima un radiogramma standard del torace e successivamente un esame hrtc utilizzando unapparecchiatura tc somaton plus ( siemens medical system , germania )  . 
sono state effettuate scansioni contigue dagli apici alle basi , con spessore di strato ( collimazione ) di 1 mm , ottenendo , cos , una pi elevata risoluzione spaziale . 
per ridurre il pi possibile gli artefatti da movimento , particolarmente evidenti nei pazienti non collaboranti , sono stati utilizzati tempi di scansione molto brevi ( 1 s )  . 
questi dati di esposizione , pur incrementando la dose al paziente , hanno consentito di ottenere immagini di elevata qualit , riducendo il rumore quantico riconducibile sia a fattori tecnici ( algoritmo di ricostruzione , kv e ma , tempo di scansione ) sia costituzionali del paziente . 
i pazienti sono stati sottoposti ad agobiopsia percutanea quando la conta piastrinica era > 50x109 / l ; il tempo intercorso dallinizio della terapia allespletamento della biopsia variava quindi da 0 a 172 giorni . 
la biopsia tc - guidata stata effettuata con ago sottile per agoaspirato 1922 g , previa anestesia locale con lidocaina al 2% , preferibilmente su lesioni periferiche e limitando a due il numero di passaggi , al fine di ridurre il rischio di pneumotorace . il materiale aspirato stato subito analizzato al microscopio da un anatomopatologo ( cg ) per giudicarne ladeguatezza e successivamente fissato in una soluzione di formalina al 10% . 
la diagnosi istologica di aspergillosi stata posta quando nei campioni erano visibili ife settate , sottili , di calibro uniforme con ramificazioni dicotomiche ad angolo acuto , mentre la mucormicosi stata diagnosticata quando le ife erano irregolari , ampie , non settate , con ramificazioni scarse , di solito ad angolo retto [ 13 ]  . risultati le infezioni polmonari , allesordio , si sono sempre manifestate con tosse e con il persistere di una febbre resistente alla terapia antibiotica ad ampio spettro , con emocolture negative . 
pleural alterations were associated with the pulmonary lesions : moderate pleural effusion was present in 44.4% of cases ( 8 / 18 ) , predominantly unilateral and to the right . 
in 3 / 18 patients ( 16.7% ) , the result was non - specific ; in 1 / 18 cases ( 5.6% ) , the biopsy sample was inadequate . in these cases , clinical course and response to therapy confirmed the diagnosis of mycosis . 
radiological follow - up of the lesions , performed at the end of therapy , allowed us to evaluate lesion excavation and therefore the appearance of the crescent air sign , a finding with a favourable prognostic significance . 
la distribuzione dei noduli nellambito dei due emitoraci risultata la seguente : in 5 / 13 pazienti ( 38 , 5% ) a destra , in 3 / 13 ( 23% ) a sinistra , in 5 / 13 ( 38 , 5% ) bilaterali . 
le consolidazioni parenchimali riscontrate in 8 pazienti erano singole in 3 pazienti ( 38% ) e multiple in 5 ( 63% ) ; erano localizzate a destra in 5 / 8 pazienti ( 63% ) e a sinistra in 3 pazienti ( 38% )  . 
esse si presentavano sotto forma di addensamenti singoli o multipli , pi spesso di forma triangolare con la base rivolta verso la pleura e con aspetto a vetro smerigliato del parenchima circostante . alle lesioni polmonari si associavano alterazioni pleuriche : il versamento pleurico , di media entit , era presente nel 44 , 4% delle osservazioni ( 8 / 18 ) , prevalentemente monolaterale destro . 
in 3 / 18 pazienti ( 16 , 7% ) il reperto risultato non specifico , in 1 / 18 casi ( 5 , 6% ) la quantit di materiale prelevato risultata insufficiente ; in questi casi il decorso clinico e la risposta alla terapia hanno confermato la diagnosi di micosi . 
il paziente con riscontro bioptico di carcinoma bronchiolo - alveolare non stato trattato con antifungini . solo in 1 caso si verificato uno pneumotorace dopo la biopsia che ha richiesto il posizionamento di un drenaggio pleurico ; non abbiamo riscontrato soffusione emorragica o altre complicanze . 
al primo controllo clinico effettuato al termine della terapia ( durata media 30 giorni ) si registrata la guarigione in 7 pazienti ( 38 , 9% ) , un miglioramento in altri 7 pazienti ( 38 , 9% ) , stabilit della malattia in 2 pazienti ( 11 , 1% ) e in altri 2 ( 11 , 1% ) lexitus . 
il monitoraggio radiologico delle lesioni effettuato al termine della terapia ha consentito di valutare lescavazione delle stesse e quindi la comparsa del segno della falce daria , reperto che riveste un significato prognostico favorevole . 
at follow - up , one patient ( 6.3% ) showed stable condition , 4 ( 25% ) had improved , 9 ( 56.3% ) had recovered , and 2 ( 12.5% ) had died because of progression of the underlying disease . 
 il follow - up dei rimanenti 16 pazienti stato effettuato in un tempo variabile da 1 a 7 anni ( tempo medio di 2 , 6 anni )  . al follow - up 1 paziente ( 6 , 3% ) presentava un quadro stabile , 4 pazienti ( 25% ) miglioramento , 9 ( 56 , 3% ) pazienti guarigione . 
successivamente in un paziente si registrata una recidiva della malattia di base , in seguito alla quale deceduto . discussion discussione patients with haematological malignancies are susceptible to fungal infections as result of the phase of granulocytopenia induced by chemotherapy . 
aspergillus and , to a lesser extent , mucor , are the i pazienti con malattie ematologiche maligne sono suscettibili alle infezioni da funghi e batteri come risultato della fase di granulocitopenia indotta dal trattamento chemioterapico . 
la neutropenia prolungata , infatti , rappresenta uno dei maggiori fattori di rischio per le infezioni da funghi filamenmost common infectious agents , and they have a high probability of becoming pathogens in immunocompromised patients . 
peribronchial extension of aspergillus infection can reach the wall of the pulmonary arteries by contiguity , leading to haemorrhagic infarctions , which usually develop in the same territories as the initial round opacity [ 2 ]  . 
the high mortality rate is due to the biological aggressiveness of the pathogens , which grow 12 mm / h , as well as to diagnostic and therapeutic delay . the diagnosis of fungal infection may be difficult because even in appropriate cultures , the pathogens grow with difficulty : sputum culture is positive in less than 10% of cases [ 1 ] , and since aspergillus is a common airways saprophyte , a positive culture is not proof of infection ; serology is not always reliable , and the sensitivity of bal is less than 50% [ 14 ]  . 
ct is a non - invasive diagnostic method that is highly useful for the early diagnosis of pulmonary infections by filamentous fungi [ 10 ] : it is a useful examination to identify probable pulmonary aspergillosis and to guide tissue sampling to obtain a definitive and specific diagnosis and initiate appropriate treatment . 
the presence of wedgeshaped parenchymal consolidation areas requires the differential diagnosis with bronchopneumonic infections of bacterial origa fungal - like infection could be suspected when the presence of a ground - glass attenuation surrounding the initial opacity ( halo sign ) is observed [ 1 ]  . 
this halo is the result of the angioinvasion of aspergillus that causes a coagulative central necrosis with a peripheral rim due to haemorrhage and inflammatory reaction ; this sign would herald the subsequent onset of necrosis and excavation . 
 it is well known that this finding is not pathognomonic for aspergillosis only , as it is also seen in candidosis and in noninfectious pathologies such as wegener granulomatosis as well as in primary neoplastic lesions and haemorrhage g . 
lestensione peribronchiale dellinfezione da aspergillus pu raggiungere per contiguit la parete delle arterie polmonari , determinando di conseguenza degli infarti emorragici che , abitualmente , si sviluppano negli stessi territori dellopacit rotonda iniziale [ 2 ]  . 
la diagnosi di infezione funginee in effetti pu essere difficoltosa , perch gli agenti patogeni crescono con difficolt anche in terreni di coltura appropriati : le colture su escreato sono positive in meno del 10% dei casi [ 1 ] e , poich laspergillo un comune saprofita delle vie aeree , una coltura positiva non una prova di infezione ; gli studi sierologici non sono sempre attendibili e la sensibilit del bal inferiore al 50% [ 14 ]  . 
la radiografia del torace negativa nel 10% dei pazienti che mostrano tuttavia una tc positiva [ 8 ]  . secondo i criteri eortc [ 5 ] il gold standard diagnostico rimane levidenza citologica o istologica dellinvasione tissutale . 
la tc una metodica diagnostica non invasiva di elevata utilit per la diagnosi precoce delle infezioni polmonari da funghi filamentosi [ 10 ] : un esame utile per identificare una probabile aspergillosi polmonare e per guidare il prelievo di materiale per una diagnosi di certezza e di specificit al fine di intraprendere il trattamento terapeutico appropriato . 
in accordo con quanto riportato in letteratura , anche nella esperienza personale abbiamo ritrovato come reperti caratteristici delle infezioni da funghi filamentosi la presenza di noduli e / o masse ( 55 , 6% dei casi ) , di opacit parenchimali ( 27 , 8% dei casi ) o la combinazione di questi due reperti ( 16 , 7% dei casi )  . 
nella nostra casistica le consolidazioni parenchimali tendevano ad essere multiple ( 61 , 5% ) piuttosto che singole ( 38 , 4% ) , con una prevalenza nel polmone destro ( 38 , 5% )  . la presenza di addensamenti parenchimali , spesso di forma triangolare , deve essere posta in diagnosi differenziale con focolai broncopneumonici di origine batterica . 
una infezione di tipo fungino pu essere sospettata quando si osserva la presenza di unimmagine interstiziale a vetro smerigliato , definita come halo sign , che circonda lopacit iniziale [ 1 ]  . questo alone il risultato dellangioinvasione dellaspergillo che provoca una necrosi coagulativa centrale con un bordo periferico dovuto alla reazione emorragica ed infiammatoria ; questo segno annuncerebbe la successiva insorgenza della necrosi e dellescavazione . 
 noto come tale reperto non sia patognomonico solo dellaspergillosi , potendosi , peraltro , riscontrare nelle candidosi , nelle patologie non infettive quali la granulomatosi di wegener , nonch nelle lesioni neoplastiche primitive e g . 
in patients with fever resistant to antibiotic therapy and with the presence of prolonged neutropoenia , the finding of the halo sign is nearly always pathognomonic for aspergillosis [ 16 ]  . 
in our experience , chest ct can guide diagnosis by revealing the halo sign and the crescent air sign . in addition , it documents the position of fungal lesions with respect to vessels and bronchi and their diffusion . 
it is usual to begin antifungal therapy in febrile neutropenic patients in the post - chemotherapy aplastic phase because fungal infections in such patients are aggressive , and mortality is high . 
biopsy has a high sensitivity also in these patients even though there is a risk of false negative results , which have , however , also been reported in open - lung biopsy . 
moreover , fnab is a safe technique : in our experience , no major complications occurred . mucormycosis infection is not rare , and probably , it is underestimated because the clinical picture is very similar to aspergillosis . 
the preparation of cytological and histological samples is important for the differential diagnosis because mucor is usually resistant to azoles and echinocandins , so only amphotericin b can be used for treatment and secondary prophylaxis . 
nella nostra esperienza la tc del torace indispensabile per orientare la diagnosi mostrando il segno dellalone e il crescent sign ; inoltre permette di localizzare la sede delle lesioni rispetto ai vasi e ai bronchi e la loro diffusione ; infine utile per scegliere lapproccio percutaneo per la biopsia . 
 prassi incominciare una terapia antifungina in pazienti neutropenici e febbrili nella fase aplastica post - chemioterapica , dal momento che le infezioni funginee in questi pazienti sono aggressive e la mortalit elevata . 
la biopsia mostra sensibilit elevata anche in questi pazienti , con la possibilit , tuttavia , di ottenere risultati falsi - negativi che sono riportati anche per la biopsia a cielo aperto . 
linfezione da mucormicosi non rara e probabilmente sottostimata perch il quadro clinico molto simile a quello dellaspergillosi . lallestimento di preparati citologici e istologici importante per la diagnosi differenziale dal momento che il mucor solitamente resistente agli azoli e alle echinocandine , quindi solo lamfotericina b pu essere utilizzata per il trattamento e la profilassi secondaria . conclusions conclusioni ct is a valuable diagnostic tool that enables the early detection of lesions suggestive of filamentous fungi infection . when compared with standard chest radiography , ct can better evaluate the number of the lesions , sometimes identifying nodules that are small or located in sites not visible on radiograms . 
amphotericin b total dose varied from 26 mg to 5 , 920 mg and amphotericin b lipid formulation dose from 210 mg to 21 , 100 mg . la tc risulta un valido aiuto diagnostico , in quanto consente di evidenziare precocemente lesioni che fanno sospettare una infezione da funghi filamentosi . 
in definitiva , la tc rispetto alla radiografia standard del torace pu valutare meglio il numero delle lesioni , identificando talvolta noduli piccoli o in posizione tale da non essere visibili nel radiogramma ; permette di delimitare lestensione del coinvolgimento pleurico rispetto al parenchima ed , inoltre , pi sensibile nel rilevare piccoli pneumotoraci , versamenti e ispessimenti pleurici . 
la fnab semplice , di facile esecuzione , affidabile , non comporta complicanze e permette di ottenere materiale utile sia per la diagnosi certa di conferma , sia per la tipizzazione dellagente eziologico al fine di intraprendere la terapia appropriata . nota 1amfotericina b ( 7 / 18 pazienti ) ( 38 , 9% ) ; amfotericina b liposolubile ( 2 / 18 ) ( 11 , 1% ) ; itraconazolo cp ( 3 / 18 ) ( 16 , 7% ) ; amfotericina b + amfotericina b liposolubile ( 4 / 18 ) ( 22 , 2% ) ; itraconazolo cp e successivamente con amfotericina b liposolubile ( 1 / 18 ) ( 5 , 6% )  . 
fifteen men and 16 women with planned arthroscopy for chronic ( n = 17 ) or traumatic tear of the rotator cuff ( n = 8 ) , congenital atraumatic ( n = 1 ) or traumatic glenohumeral instability ( n = 2 ) , traumatic tear of the rotator cuff with glenohumeral instability ( n = 1 ) , or frozen shoulder ( n = 2 ) underwent plain helical ct in neutral position and intra - articular ct - guided injection of a mixture of iodinated and paramagnetic contrast agents ( gadodiamide at 1 : 250 and iobitridol 350 at 1 : 5 in 20 ml of saline solution )  . 
cta and mra can be performed as a one - shot exacta - mra seems to give more information than cta or mra separately . key words shoulder computed tomography arthrography magnetic resonance arthrography ct contrast media mr contrast media riassunto obiettivo . 
sono stati arruolati 15 pazienti maschi e 16 femmine per i quali era programmata unartroscopia per lesione cronica ( n = 17 ) o traumatica ( n = 8 ) della cuffia dei rotatori , per instabilit gleno - omerale non traumatica congenita ( n = 1 ) o traumatica ( n = 2 ) , per lesione traumatica della cuffia dei rotatori associata a instabilit gleno - omerale ( n = 1 ) , o per spalla congelata ( n = 2 )  . 
tali pazienti sono stati sottoposti a tc elicoidale diretta in posizione neutra e a iniezione intra - articolare tc - guidata di una mistura di mezzi di contrasto diluiti in 20 ml di soluzione fisiologica ( gadodiamide a 1 : 250 e iobitridolo 350 a 1 : 5 )  . 
le immagini artro - tc e artro - rm sono state valutate separatamente e congiuntamente ( artro - tc - rm ) in tre differenti sessioni di lettura , in cieco . 
these two imaging procedures are definitely better than plain ct or mri of the shoulder because of the contrast resolution due to the presence of intra - articular diluted paramagnetic contrast or iodinated agent , respectively , and to the distension of the of the joint capsule [ 16 ]  . 
the evaluation of site , type , grade , and extent of the disease is more reliable , in particular for rotator cuff tears [ 2 , 7 , 8 ] and congenital or traumatic glenohumeral instability [ 911 ]  . 
the two techniques give different information due to a higher ct sensitivity for calcifications and bone injuries [ 11 , 12 ] and an optimal mr contrast resolution for soft tissue abnormalities [ 2 , 3 , 7 , 11 , 13 ]  . the stability of the mixture of gd - chelates and iodinated contrast agents is well known [ 14 , 15 , 16 ] while its clinical safety has been reported for performing cta and mra of the ankle as a one - shot exam ( cta - mra ) [ 17 ]  . on this basis , our aim was to perform cta and mra of the shoulder as a one - shot exam using a mixture of iodinated and paramagnetic contrast agents and to test the value of this cta - mra exam compared with each of the two modalities used separately , using arthroscopy as a standard of reference . materials and methods thirty - one patients ( 15 men and 16 women , age range 2376 years ) with planned arthroscopy for a clinical diagnosis of chronic ( n = 17 ) or traumatic ( n = 8 ) rotator cuff tear , congenital atraumatic ( n = 1 ) or traumatic glenohumeral instability ( n = 2 ) , traumatic rotator cuff tear and glenohumeral instability ( n = 1 ) , and frozen shoulder ( n = 2 ) were enrolled . 
informed consent for one - shot cta - mri of the shoulder was obtained . a mixture of contrast agents was prepared using gd - dtpa - bma ( omnniscan , amersham health , oslo , norway ) at 1 : 250 and iobitridol 350 ( xenetix , guerbet , rome , italy ) at 1 : 5 in 20 ml of saline solution for a total mixture of 24 ml . all patients underwent plain helical ct of the shoulder using a prospeed sx power unit ( general electric , milwaukee , il , usa ) with the following technical parameters : x - ray beam thickness 3 mm , pitch 1 : 1 , 120 kv , 250 mas , field of view 160180 mm , and reconstruction of 3 - mm axial slices . 
the scan covered a body length from the acromioclavicular joint to the inferior capsular recess , defined on the basis of a scanogra lartrografia a rm ( artro - rm ) e lartrografia tc ( artro - tc ) sono considerate le metodiche per immagini pi affidabili nella diagnosi delle lesioni della spalla se comparate prospetticamente con i reperti artroscopici e chirurgici . 
queste due indagini sono effettivamente superiori alle corrispondenti valutazioni tc o rm dirette , ovvero eseguite senza somministrazione di mezzo di contrasto ( mdc ) , grazie alla risoluzione di contrasto e alla distensione della capsula articolare ottenute mediante somministrazione intraarticolare di mdc paramagnetico o iodato opportunamente diluiti in soluzione fisiologica [ 16 ]  . 
la valutazione della sede , del tipo e dellestensione delle alterazioni pi attendibile , in particolare in presenza di lesioni della cuffia dei rotatori [ 2 , 7 , 8 ] e dellinstabilit gleno - omerale congenita o traumatica [ 911 ]  . 
le due indagini forniscono uninformazione non sovrapponibile in virt della pi alta sensibilit della tc per le calcificazioni e le alterazioni ossee [ 11 , 12 ] e dellottimale risoluzione di contrasto della rm per le lesioni dei tessuti molli [ 2 , 3 , 7 , 11 , 13 ]  . la stabilit delle misture di chelati del gd e mdc iodati nota [ 1416 ] e la loro innocuit stata segnalata per lartrotc e lartro - rm della caviglia eseguite in unica sessione ( artro - tc - rm ) [ 17 ]  . su tali basi il nostro obiettivo stato realizzare lartro - tc e lartro - rm della spalla in unica seduta mediante la somministrazione intra - articolare di una mistura di mdc paramagnetico e iodato e valutarne laccuratezza diagnostica rispetto a ciascuna delle due indagini considerata separatamente , utilizzando un gold standard artroscopico . materiali e metodi sono stati arruolati 31 pazienti ( 15 maschi e 16 femmine , di et compresa tra 23 e 76 anni ) per i quali era stata programmata unartroscopia di spalla sulla base della diagnosi clinica di lesione cronica ( n = 17 ) o traumatica ( n = 8 ) della cuffia dei rotatori , instabilit gleno - omerale non traumatica congenita ( n = 1 ) o traumatica ( n = 2 ) , di lesione traumatica della cuffia dei rotatori associata a instabilit gleno - omerale ( n = 1 ) , o di spalla congelata ( n = 2 )  . 
ciascuno dei pazienti ha fornito consenso informato allesecuzione dellindagine artro - tc e artro - rm in unica seduta . stata preparata una mistura di mdc diluiti in 20 ml di soluzione fisiologica , composta di gadodiamide ( gd - dtpa - bma , omnniscan , amersham health , oslo , norway ) a 1 : 250 e iobitridolo 350 ( xenetix , guerbet , rome , italy ) a 1 : 5 , per un totale di 24 ml . tutti i pazienti sono stati sottoposti a tc elicoidale diretta della spalla con apparecchiatura prospeed sx power ( general electric , milwaukee , illinois , usa ) con i seguenti parametri tecnici : collimazione 3 mm , pitch 1 : 1 , 120 kv , 250 mas , campo di vista 160180 mm , ricostruzioni assiali di 3 mm di spessore . il paziente era in posizione supina con larto superiore indagato addotto in posizione neutra e laltro braccio addotto intorno al capo . 
la scansione comprendeva il tratto corporeo esteso dallarticolazione acromio - clavicolare al recesso capsulare inferiore , in base alla valutazione dello scanogramma . portato il paziente fuori dal gantry , un ago di chiba ( lunghezza 90 mm ) veniva introdotto in sede immediatamente infethe patient was moved out of the gantry , and a 90 - mm chiba needle ( 20 gauge ) was introduced below and lateral to the apex of the coracoid process . 
mra scans with spin - echo ( se ) and gradient - echo ( ge ) t1 - weighted sequences were obtained using the following technical parameters : axial , coronal oblique , and sagittal oblique planes ; slice thickness , 4 mm ; gap interslice , 1 mm ; field of view , 1618 cse sequences were acquired with a tr / te = 600 / 20 ms and a 90 flip angle and ge sequences with a tr / te = 500 / 10 ms and 70 flip angle adding a chemical fat - saturating pulse ( fat - sat )  . cta images were printed with two different ct windows : plain scans , level 120 and width 750 hounsfield units ( hu ) and contrast - enhanced scans , 650 and 2 , 100 uh , respectively . 
mra images were printed with the usual operator - dependent windowing . cta and mra images were evaluated separately and jointly ( cta - mra ) in three different blinded sessions ( with a time interval of at least 1 month ) by two radiologists by consensus . 
finally , a radiologist and an orthopedist assigned a 03 score to the agreement between cta and arthroscopy , mra and arthroscopy , and cta - mra and arthroscopy by consensus ( 0 , no agreement ; 1 , low agreement ; 2 , high agreement ; 3 , total agreement )  . 
wilcoxon matched - pairs signedranks test was used . results the mean injected volume of the mixture of contrast agents was 19.22.3 ml , ranging from 10 ml in a case of adhesive capsulitis to 24 ml in a case of congenital atraumatic multidirection instability . 
no side effects in possible correlation with the intra - articular injection of the mixture of agents were observed . mean examination time was about 25 min for cta ( including contrast injection ) , 5 min for moving the patient from the ct to the mr room , and 30 min for mra ; about 1 h for the whole procedure . 
the mra scans started about 15 min after the intra - articular injection of the mixture of contrast agents . cta had an agreement mean score with arthroscopy of 2.330.62 , mra of 2.470.52 , and cta - mra of a . 
sono state quindi realizzate scansioni elicoidali artro - tc in intraed extra - rotazione dellarto con gli stessi parametri tecnici descritti precedentemente . il paziente era quindi trasferito dalla sala diagnostica tc a quella rm dello stesso servizio e riposizionato supino , con larto da esaminare addotto in posizione neutra . 
le scansioni artro - rm sono state realizzate mediante sequenze spinecho ( se ) e gradient - echo ( ge ) t1 - pesate con i seguenti parametri tecnici : piani assiali , coronali obliqui e sagittali obliqui ; spessore 4 mm ; interspazio 1 mm ; campo di vista 1618 cle sequenze se sono state acquisite con tr / te = 600 / 20 ms e flip angle di 90 ; le sequenze ge con tr / te = 500 / 10 ms , flip angle di 70 e impulso di saturazione spettrale del grasso ( fat - sat )  . le immagini tc sono state stampate utilizzando due differenti finestre : livello di 120 e ampiezza 750 uh per le scansioni dirette ; 650 e 2100 uh per le scansioni artro - tc , rispettivamente . 
le immagini artro - rm sono state stampate con usuale finestra operatore - dipendente . le immagini artro - tc e artro - rm sono state valutate separatamente e congiuntamente ( artro - tc - rm ) in tre differenti sessioni , in cieco , in ordine casuale , da due radiologi per consenso , con un intervallo di tempo di almeno un mese tra una sessione e laltra . 
a fini statistici stato utilizzato il testi di wilcoxon . risultati il volume della mistura di agenti di contrasto mediamente iniettato stato di 19 , 22 , 3 ml , con un minimo di 10 ml in un caso di capsulite adesiva al massimo di 24 mm in un caso di instabilit congenita atraumatica multidirezionale . 
non abbiamo osservato alcun effetto collaterale in possibile correlazione con liniezione intra - articolare della mistura di mdc . il tempo - esame stato mediamente intorno a 25 min per lartro - tc ( inclusa liniezione intra - articolare di mdc ) , 5 min per lo spostamento dalla diagnostica tc a quella rm e 30 min per lartro - rm ; lintera procedura stata quindi effettuata in circa unora . 
le scansioni artro - rm sono iniziate circa 15 minuti dopo liniezione intraarticolare della mistura di mdc . lartro - tc ha ottenuto uno score medio di accordo con lartroscopia di 2 , 330 , 62 , lartro - rm di 2 , 470 , 52 e lartro - tcrm di 2 , 670 , 49 . 
non stata osservata differenza significativa tra lo score ottenuto dallartro - tc e quello ottenuto dallartrorm , mentre differenze significative sono state osservate per la comparazione artro - tc - rm versus artro - tc ( p = 0 , 0281 ) e per a . 
a t1 - weighted coronal oblique image shows both tears : the subacromial bursitis appears as a low signal area under the acromioclavicular joint ( white asterisk ) instead of the regular adipose interface . 
a limmagine artro - rm t1 - pesata mostra entrambe le lesioni : la borsite subacromiale come unarea a basso segnale sottostante larticolazione acromio - clavicolare ( asterisco bianco ) invece della normale interfaccia adiposa ; lerosione tendinea come irregolarit del profilo inferiore dello stesso tendine ( frecce )  . 
 [ 17 ] recently reported the clinical safety of a mixture of 1 : 1 diluted ( 4 mmol / l ) gd chelate ( gadoteridol ) and nonionic iodinated contrast agent ( iopamidol 300 mg i / ml ) for mr and cta of the ankle . our 1 : 250 dilution of 0.5 - m gadodiamide ( 2 mmol / l ) is in agreement with the report by schulte - altedorneburg et al . [ 6 ] who judged this dilution to be the best concentration for intra - articular administration of gadopentetate dimeglumine  . after passive complete diffusion from the joint within 624 h , complete and rapid renal elimination after intra - articular injection was observed [ 6 ]  . 
the 1 : 5 dilution of the iodinated contrast agent in saline solution is a routine procedure for cta at our department , even if higher concentrations have been reported [ 17 ]  . 
mra of the shoulder is usually performed with a maximum required volume of 15 ml for rotator cuff lesions and 20 ml for instability [ 2 , 6 , 18 ]  . 
in order to obtain a marked distension of the capsule with optimal visualization of normal and abnormal anatomical structures , we stopped the intra - articular injection only when the distention became uncomfortable [ 19 ] , reaching in such a way a higher mean of injected volumes compared with the literature [ 6 ]  . the cta - mra exam did not create any particular problems in scheduling , performing , and reading the images . the two exams were scheduled with mra starting 30 min after cta , considering that the two rooms are located near each other . 
in our department , mr scans are now reduced to 1012 min using a new mr unit , with a total of 4045 min for the whole cta - mra . 
thirty minutes could be enough for cta - mra of the shoulder if a multidetector ct unit is used . la comparazione artro - tc - rm versus artro - rm ( p = 0 , 0277 )  . tre casi di maggior valore diagnostico dellartro - rm sono illustrati nelle figure 13 , due casi di maggior valore diagnostico dellartro - tc sono illustrati nelle figure 4 e 5 e un caso di valore diagnostico equivalente dellartro - tc e dellartro - rm illustrato in figura 6 . discussione il presente lavoro dimostra la possibilit di effettuare artro - tc e artro - rm di spalla in unica sessione mediante liniezione intraarticolare di una mistura di mdc iodato e paramagnetico diluiti in soluzione fisiologica . con la presente esperienza confermiamo linnocuit di tale mistura , come gi dimostrato sia in studi sperimentali che clinici [ 1417 ]  . 
inoltre , schmid et al . [ 17 ] hanno recentemente riportato linnocuit di una mistura di una diluizione 1 : 1 ( 4 mmol / l ) di un chelato del gd ( gadoteridolo ) con un mdc iodato nonionico ( iopamidolo 300 mg / ml ) nelluso clinico per lartro - tc e artro - rm della caviglia . la diluizione 1 : 250 di gadodiamide 0 , 5 - m ( 2 mmol / l ) , da noi utilizzata , in accordo con lesperienza riportata da schulte - altedorneburg et al . 
 [ 6 ] , i quali giudicano questa diluizione ottimale per la somministrazione intra - articolare di gd - dtpa . dopo completa diffusione passiva dallarticolazione in circa 624 ore , si ha una totale e rapida eliminazione renale [ 6 ]  . 
la diluizione 1 : 5 del mdc iodato in soluzione fisiologica utilizzata di routine per lartro - tc nel nostro servizio , anche se alcuni autori hanno riportato lutilizzo di concentrazioni pi elevate [ 17 ]  . nella presente esperienza noi abbiamo iniettato una media di circa 19 ml della mistura dei due mdc , con un range tra 10 e 24 ml . 
lartro - rm di spalla usualmente realizzata con un volume massimo di circa 15 ml per le lesioni della cuffia dei rotatori e di circa 20 ml per linstabilit gleno - omerale [ 2 , 6 , 18 ]  . al fine di ottenere una marcata distensione della capsula con ottimale visualizzazione delle strutture anatomiche normali e patologiche abbiamo interrotto liniezione intra - articolare solo quando la distensione capsulare provocava dolore soggettivamente riferito dal paziente [ 19 ] , raggiungendo in tal modo un pi alto volume medio di iniezione intra - articolare rispetto a quanto riportato in letteratura [ 6 ]  . lartro - tc - rm in unica sessione non ha creato alcun particolare problema di programmazione , esecuzione o refertazione . considerando che nel nostro servizio le due diagnostiche sono collocate una accanto allaltra , lartro - rm era programmata mezzora dopo lartro - tc . 
riteniamo , infatti , che potrebbe essere sostanzialmente ridotto come infatti gi accade attualmente nel nostro servizio : le scansioni artro - rm sono infatti ottenute in 1012 min con la nuova unit rm recentemente installata , con un tempo totale per lartro - tcrm di circa 4045 m utilizzando unapparecchiatura tc multidetettore il tempo totale potrebbe ridursi a circa 30 minuti . i nostri risultati confermano lelevata accuratezza dellartrorm nella diagnosi delle lesioni del cercine glenoideo [ 1 , 4 , 7 ] e our results confirm the high accuracy of mra in diagnosing labral lesions [ 1 , 4 , 7 ] as well as the value of cta in detecting calcifications of tendon and ligaments and cortical bone damage [ 11 , 12 ]  . 
in spite of the significant difference in favor of cta - mra for the level of correspondence with arthroscopy , the number of cases is too small to draw a final conclusion , and the one - shot ctamra of the shoulder should be still regarded as a work in progress . 
this modality could be used in order to combine the advantages of mri for capsular damage , partial tendon tears , and labrum tears with those of cta for detecting calcifications of tendons and ligaments and cortical bone damage . 
if we do not take into account the problem of radiation exposure , the two techniques are probably equivalent in evaluating full - thickness tendon tears . a not fully understood increase of signal intensity in t1weighted images obtained after intra - articular injection of iodinated contrast agents compared with saline solution only was reported and was more pronounced for ionic agents [ 6 , 14 ]  . 
in our mra images , we did not notice any clinically relevant reduction of intra - articular signal intensity , as opposed to the experiences reported by kopka et al . [ 14 , 15 ] , probably due to the combination of several factors in our study : ( 1 ) low concentration of iodinated contrast agent , ( 2 ) short time interval between injection and mr scans ( about 15 min ) , the ( 3 ) high volume of solution injected . 
in our cta , the amount of gd chelate added to the diluted iodinated agent was too low to give a detectable increase of electron density [ 20 ]  . 
we should take into account that the diagnostic information of cta could be increased by the higher - quality multiplanar reconstructions with multidetector equipment [ 21 , 22 ] , making ct really comparable with mr multiplanar imaging . 
finally , if mr and ct acquisitions were coregistered , an image fusion postprocessing would superimpose the bone and calcium analysis of ct on the soft tissue contrast resolution of mr [ 23 ]  . an alternative method of obtaining a one - shot cta - mra could be to inject only diluted iodinated contrast agent and to perform t2or t2 * - weighted mr sequences with high signal of the water , as reported for mra of the shoulder with only saline or ringer solution as intra - articular contrast agent [ 2427 ]  . 
tuttavia , nonostante la significativit statistica di tale guadagno fornito dallartro - tc - rm in confronto con il gold standard artroscopico , il numero di casi della nostra sede troppo ridotto per ottenere una conclusione affidabile . 
se ne delinea un possibile utilizzo mirante a coniugare i vantaggi dellartro - rm nei casi di lesioni capsulari , lesioni parziali dei tendini e del cercine glenoideo con quelli dellartro - tc nella valutazione delle lesioni dellosso corticale e delle calcificazioni . 
al di l di considerazioni radioprotezionistiche , le due tecniche appaiono pressoch equivalenti nella valutazione delle lesioni tendinee a tutto spessore . in letteratura stato riportato ( e non completamente spiegato ) un incremento del segnale rm nelle immagini t1 - pesate dopo iniezione intraarticolare di mdc iodato in comparazione con liniezione di sola fisiologica , incremento pi pronunciato allorquando sono utilizzati mdc ionici [ 6 , 14 ]  . 
 [ 14 , 15 ] , verosimilmente a causa di diversi fattori operanti nel nostro studio in modo combinato : ( 1 ) bassa concentrazione del mdc iodato ; ( 2 ) ridotto intervallo di tempo tra liniezione intra - articolare e le scansioni rm ( circa 15 minuti ) ; ( 3 ) elevato volume di soluzione iniettata . 
peraltro , nelle nostre immagini artro - tc la quantit di gd aggiunta al mdc iodato diluito troppo bassa per dare luogo a un incremento di densit elettronica rilevabile [ 20 ]  . segnale ovviamente , dobbiamo considerare che linformativit diagnostica dellartro - tc potrebbe essere nettamente incrementata dallelevata qualit delle ricostruzioni multiplanari ottenibili con apparecchiature tc multidetettore [ 21 , 22 ] , rendendo in tal senso la tc realmente comparabile con limaging multiplanare a rm . 
infine , qualora le immagini rm e tc siano coregistrate , un post - processing che fonda le due immagini potrebbe sommare la sensibilit della tc per losso e il calcio con la risoluzione di contrasto della rm per i tessuti molli [ 23 ]  . una modalit alternativa per ottenere artro - tc e artro - rm in unica sessione potrebbe essere iniettare in sede intraarticolare soltanto mdc iodato diluito ed eseguire , oltre alle scansioni artro - tc , sequenze rm t2o t2 * - pesate , come riportato per lartro - rm di spalla con iniezione intra - articolare di soluzione fisiologica o di ringer [ 2427 ]  . 
si tratta di una modalit interessante , perch configura lartro - rm come una possibile , ma non obbligatoria , seconda fase dopo lartro - tc , in casi selezionati . conclusions conclusioni our experience confirms the safety of the intra - articular administration of a mixture of iodinated and paramagnetic contrast agent and demonstrates the feasibility of cta and mra in conclusione , la nostra esperienza conferma linnocuit della somministrazione intraarticolare di una mistura di mdc iodato e paramagnetico e dimostra la fattibilit dellartro - tc e artroa . 
roger b , skaf a , hooper aw et al ( 1999 ) imaging findings in the dominant shoulder of throwing athletes : comparison of radiography , arthrography , ct arthrography , and mr arthrography with arthroscopic correlation . 
kopka l , funke m , fischer u et al ( 1994 ) signal characteristics of x - ray contrast media and their interaction with gadolinium - dtpa in mrt . 
kopka l , funke m , fischer u et al ( 1994 ) mr arthrography of the shoulder with gadopentetate dimeglumine : influence of concentration , iodinated contrast material , and time on signal intensity . ajr am j roentgenol 163 : 621623 16 . 
brown rr , clarke dw , daffner rh ( 2000 ) is a mixture of gadolinium and iodinated contrast material safe during mr arthrography ? ajr am j roentgenol 175 : 10871090 17 . 
berg bc , lecouvet fe , poilvache p et al ( 2002 ) spiral ct arthrography of the knee : technique and value in the assessment of internal derangement of the knee . 
handels h , ehrhardt j , plotz w , poppl sj ( 2001 ) three - dimensional planning and simulation of hip operations and computer - assisted construction of endoprostheses in bone tumor surgery . 
willemsen uf , wiedemann e , brunner u et al ( 1998 ) prospective evaluation of mr arthrography performed with highvolume intraarticular saline enhancement in patients with recurrent anterior dislocations of the shoulder . 
binkert ca , zanetti m , gerber c et al ( 2001 ) mr arthrography of the glenohumeral joint : two concentrations of gadoteridol versus ringer solution as the intraarticular contrast material . 
martino e cliniche universitarie convenzionate , genova , italy 3divisione di radiologia , istituto europeo di oncologia e istituto di scienze radiologiche , universit degli studi , milano , italy 4istituto di scienze radiologiche c . 
stanzione 18 , i - 80129 napoli ( na ) , italy , tel . : + 39 - 348 - 3738149 , fax : + 39 - 081 - 5584521 , e - mail : roberto.grassi@libero.it received : 27 october 2004 / accepted : 18 march 2005 abstract the authors illustrate the technique for small - bowel imaging using enteroclysis with multidetector - row computed tomography ( mdct ) , underscoring the important role played by ct in the assessment of the small bowel thanks to the advent of first the spiral and later the multidetector technique . 
the paper makes a detailed comparison of the various methods that have been used in ct study of the small bowel and proposes a standardised technique to achieve correct distension of bowel loops and adequate evaluation of bowel wall vascularity , making reference to the well - consolidated experiences of the various italian research groups . 
the paper accurately describes the different procedures required for ct assessment of the small bowel , from nasojejunal intubation to the selection of the most appropriate acquisition phases for assessment of bowel wall vascularity . 
 key words small bowel msct enteroclysis msct enterography riassunto viene illustrata in questo lavoro la metodologia di studio dellintestino tenue mediante limpiego delle enteroclisi con tc multistrato , sottolineando il ruolo importante che la tc , grazie allavvento della tecnologia spirale prima e multistrato successivamente , svolge nell ' analisi dellintestino tenue . 
viene proposto un accurato confronto tra le differenti metodiche di studio fin qui adottate per lo studio dellintestino tenue con tc , proponendo una tecnica standardizzata per la corretta distensione delle anse intestinali e per ladeguata valutazione della vascolarizzazione parietale , facendo riferimento alle esperienze ormai consolidate di differenti gruppi di studio italiani . 
si descrivono infine le differenti procedure indispensabili per la valutazione con tc multistrato dellintestino tenue , dalla intubazione naso - digiunale , fino alla scelta delle pi opportune fasi di acquisizione per la corretta valutazione della vascolarizzazione di parete . parole chiave piccolo intestino enteroclisi con tcms transito dal tenue con tcms introduction introduzione gastrointestinal radiology has drastically changed over the last two decades . 
in the study of the small bowel , volumetric ct , single - slice first and multislice later , has eliminated the presence of movement artefacts due to peristalsis and allowed the adequate assessment of intestinal - wall enhancement with the possibility of obtaining excellent - quality multiplanar reconstructions ( mpr )  . 
lo studio radiologico convenzionale dellintestino , basato su sistemi analogici e dominato dalla contrastografia baritata , a singolo e doppio contrasto , stato gradualmente affiancato ed a volte sostituito da metodiche digitali , quali gli ultrasuoni ( us ) , la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm )  . 
the attention of radiologists , previously limited to the parenchyma , can now also focus on assessing the bowel loops , which are no longer considered a source of disturbance . 
the earliest literature reports to this effect date back to 1992 - 1993 and were written by german investigators [ 1 , 2 ]  . the investigators combined standard abdominal ct with adequate distension of the small bowel by nasointestinal intubation , defining the method ct - sellink . 
the first contribution came from the genoa group , which promoted this innovative method at both national and international congresses [ 58 ] and through published reports [ 9 , 10 ]  . 
in 2000 , the neapolitan school reported a case of multiple jejunal angiodysplasia detected using this method [ 11 ] while the roman group presented their experience at the international congress of gastroenterology [ 12 ]  . in 2002 , di mizio published a book on crohns disease of the small bowel , which was extensively illustrated with images obtained both with double - contrast barium and air enteroclysis and with ct enteroclysis . the volume deals in depth with the technical aspects and the new ct semiotics , making clear the advantages of the method . 
the book was convincing , it was well - received by the us teams [ 13 , 14 ] and it helped to promote the method definitively . the recent availability of multislice ct ( msct ) scanners has allowed the technique to be further refined , leading to a wider spread of ct enteroclysis in the study of the small bowel ; an increasing number of contributions have appeared in the literature on both sides of the atlantic . 
other european groups have followed the lead of the italians : the french school , which suggests the use of water as an intraluminal contrast agent [ 15 , 16 ] , the swiss and austrian schools , which use an almost identical protocol to that used in italy [ 1719 ] and the german school [ 2022 ]  . today , thanks to the frequent opportunities for contact and exchange provided by european and american congresses and , above all , to the commitment of the societ italiana di radiologica medica ( sirm ) study section on gastrointestinal and abdominal radiology , the consensus on the study technique is almost unanimous . attualmente , il ruolo della tc nello studio dellintestino tenue indiscusso . 
lattenzione del radiologo , dapprima limitata ai parenchimi , si rivolge ora anche alla valutazione delle anse , finalmente non considerate pi come elementi di disturbo . nellultimo decennio , si sviluppato e diffuso il tentativo di riunire in una sola metodica i vantaggi dellindagine tc con quelli dellenteroclisi convenzionale . a tal proposito , i primi contributi apparsi in letteratura sono del biennio 19921993 ad opera di autori tedeschi [ 1 , 2 ]  . 
per la distensione delle anse utilizzano un mezzo di contrasto ( mdc ) positivo , una sospensione di solfato di bario opportunamente diluita . tale esperienza viene ripresa oltreoceano e nel triennio 19961998 compaiono alcuni contributi di autori nord americani . 
essi utilizzano un mdc iodato idrosolubile per la distensione delle anse . la loro esperienza si basa prevalentemente sullo studio delle occlusioni parziali dellintestino tenue [ 3 , 4 ]  . 
essi impiegano un mdc endoluminale neutro , lacqua oppure la metilcellulosa ( mc ) allo 0 , 5% in soluzione acquosa , e , contemporaneamente , un mdc positivo iodato endovena ( ev )  . nella seconda met degli anni novanta la scuola radiologica italiana particolarmente attiva . il primo contributo della scuola genovese , che si fa portavoce di questa metodica innovativa , sia in sedi congressuali nazionali ed internazionali [ 58 ] sia con contributi in letteratura [ 9 , 10 ]  . 
essa per prima suggerisce dimpiegare lenteroclisitc ( e - tc ) , o clisma - tc del tenue , nello studio delle varie patologie dellintestino tenue . nel 2000 , la scuola napoletana descrive un caso di angiodisplasia digiunale multipla identificata con tale metodica [ 11 ] , mentre quella romana presenta la sua esperienza al congresso internazionale di gastroenterologia [ 12 ]  . nel 2002 , di mizio pubblica un volume sul morbo di crohn del tenue , dove viene presentata unampia iconografia , ottenuta sia con lenteroclisi a doppio contrasto con bario ed aria , sia con la e - tc . in questo volume vengono esaminati in dettaglio gli aspetti tecnici e la nuova semeiotica tc , esplicitando i vantaggi della metodica . 
il libro convince , trova consensi nei cultori doltreoceano [ 13 , 14 ] e contribuisce a promuovere definitivamente la metodica . la recente commercializzazione delle apparecchiature tc multistrato ha ulteriormente migliorato gli aspetti tecnici , consentendo una pi ampia diffusione dello studio dellintestino tenue tramite e - tc ; sono sempre pi numerosi , infatti , i contributi apparsi in letteratura , su entrambe le sponde delloceano atlantico . anche altre scuole europee fanno eco alla scuola italiana : la francese , che suggerisce limpiego di acqua quale mdc endoluminale [ 15 , 16 ] , quella svizzera e austriaca , quasi perfettamente assonanti con quella italiana [ 1719 ] e tedesca [ 2022 ]  . oggi , grazie alle frequenti occasioni di confronto nei congressi europei ed americani e grazie , soprattutto , allimpegno della sezione di studio di radiologia gastroenterologica ed addominale della sirm , si raggiunto un consenso quasi unanime sullesecuzione dellesame . definition definizione msct enteroclysis ( invasive ct enterography , multidetector - row helical ct enteroclysis ) is an imaging method that involves distension of the small bowel with intraluminal contrast material administered via a nasointestinal tube , bowel hypotonia and the infusion of iv iodinated contrast material . the aim of msct enteroclysis is to combine all the advantages of conventional enteroclysis and abdominal spiral ct into a single modality . 
forced distension and luminal hypotonia : ( 1 ) avoid diagnostic errors caused by collapsed and contracted loops ; failure to achieve adequate loop distension may result in both false positive results mimicking abscesses , masses , enlarged lymph nodes and false negative results due to non - distended loops masking lesions ; ( 2 ) highlight deformations and alterations in loop profile as well as the possible pathological reduction of wall elasticity ; ( 3 ) improve the identification and assessment of strictures as a consequence , in the study of the small bowel , ct enteroclysis provides greater diagnostic gains compared to ct with oral contrast material ( ct enterography or non invasive peroral ct enterography ) [ 2325 ]  . materials and methods the method involves eight steps : 1 . 
in our experience , bowel preparation is indispensable in that a clean colon facilitates the intraluminal flow of contrast material through the small bowel , avoids the reflux of faecal matter into the terminal ileum and reduces patient discomfort due to loop distension . 
ct exaonce intubated , the patient is transferred to the ct roothe scout view is then performed , the correct position of the tube is checked and the volumetric scan is r . 
obiettivo delle - tcms di riunire in una sola metodica i vantaggi dellenteroclisi convenzionale e dellesame tc spirale delladdome . la distensione forzata e lipotonizzazione del lume : ( 1 ) evitano che anse collabite e contratte possano essere fonte di errore diagnostico ; la mancata od insufficiente distensione delle anse pu essere causa sia di rilievi falsi positivi , simulando ascessi , masse , linfoadenomegalie sia di rilievi falsi negativi , poich le anse non distese possono nascondere delle lesioni ; ( 2 ) mettono in risalto le deformazioni e le alterazioni del profilo delle anse nonch leventuale riduzione patologica dellelasticit parietale ; ( 3 ) migliorano lidentificazione e la valutazione delle stenosi . di conseguenza , le - tcms offre un maggiore guadagno diagnostico nello studio del tenue rispetto allesame tc ottenuto dopo assunzione di mdc per os ( per gli anglosassoni ctenterography oppure non invasive peroral ct - enterography ) [ 2325 ]  . materiali e metodi la metodica prevede otto fasi : 1 . 
secondo la nostra esperienza , la preparazione intestinale risulta indispensabile in quanto un colon pulito facilita il flusso del mdc endoluminale nel tenue , evita il reflusso di materiale fecale nellileo terminale e riduce il disagio del paziente determinato dalla distensione delle anse . 
clistere di pulizia da effettuare presso il servizio di radiologia table 2 patient preparation before multislice computed tomography ( msct ) enteroclysis ( method 2 ) tabella 2 preparazione del paziente per leffettuazione della enteroclisi ( metodo 2 ) the afternoon before the exam : 1 . 
before infusing the intraluminal contrast material , small - bowel hypotonia is induced with 20 mg of iv hyoscine n - butylbromide ( buscopan )  . this serves to lessen patient discomfort and reduce intestinal peristalsis and the resulting segmentation of the loops so that the entire small bowel is adequately and uniformly distended during the volumetric scan . 
a the scout view shows that despite inflation of the balloon ( arrow ) , the nasointestinal tube has reached the jejunal loops , which project at the level of the left iliac crest . 
a sulla scout view si osserva che la sonda naso - intestinale , nonostante il palloncino gonfiato ( freccia ) , avanzata fino alle anse digiunali che si proiettano allaltezza della cresta iliaca di sinistra . 
3 errore di tecnica : il precoce ed erroneo arresto dellinfusione della metilcellulosa prima della effettuazione della scansione ha permesso lingestione successiva di aria da parte del paziente , disturbando notevolmente lanalisi di unansa digiunale . some investigators induce hypotonia before the infusion of intraluminal contrast material [ 26 ] whereas others wait until at least 1 , 000 ml have been infused [ 9 , 27 ]  . 
mc is a well - known contrast agent that is safe , well tolerated and not absorbed . because this solution has a ct density similar to water , it is capable of creating a significant difference in contrast between the lumen and the wall enhanced by the iodinated contrast mediuconsidering that mc is hardly absorbed at the intestinal level , it is preferred to water in patients with precarious cardiocirculatory compensation so as to avoid a dangerous blood volume overload resulting from the rapid absorption of water by the intestinal mucosa . 
according to some investigators , intraluminal infusion should be done at a steady flow rate of 100 ml / m for the entire duration of the exaothers have proposed a more complex infusion pattern ( table 3 ) whereby the first 500 ml is introduced at a rate of 120 ml / min , followed by 1 , 000 ml at a rate of 240 ml / min , and a further 300 ml at 120 ml / s . 
the faster infusion rate serves to force distension of the loops and increase the vis a tergo in order to advance the previously infused contrast as far as the right colon . 
il momento della ipotonizzazione controverso : alcuni autori la effettuano prima dellinfusione del mdc endoluminale [ 26 ] , altri dopo averne infuso almeno 1000 ml [ 9 , 27 ]  . 
la mc un mdc ben conosciuto , sicuro , ben tollerato , scarsamente assorbibile . tale soluzione presenta una densit pressoch simile a quella dellacqua , idonea a creare una differenza di contrasto significativa tra il lume e la parete intestinale impregnata di mdc iodato . 
in considerazione dello scarso assorbimento a livello intestinale della mc , essa viene preferita allacqua nei pazienti in fase di compenso cardio - circolatorio precario , onde evitare un pericoloso sovraccarico di volume ematico , reso possibile dal rapido assorbimento dellacqua da parte della mucosa intestinale . si somministrano senza interruzione 1800 ml circa di mdc intraluminale , alla temperatura di 37c . 
quantit totale di mdc somministrato = 1800 ml circa table 4 diagram for biphasic infusion of iv iodinated contrast medium tabella 4 modalit di infusione bifasica del mdc iodato ev 1 . 
quantit totale di mdc infuso = 130 ml as an alternative to neutral contrast agents , some investigators have proposed hypodense and hyperdense agents [ 15 ]  . the use of oil - based substances as a negative intraluminal contrast agent allows a faster manual injection but does not provide any substantial benefit in terms of image . 
in italy , these substances are not authorised as contrast agents , and they are particularly expensive . positive intraluminal contrast agents hinder the assessment of wall lesions as their hyperdensity is confused with the hyperdensity of the intestinal wall enhanced by the iv iodinated contrast medium [ 13 ]  . 
administration of iv iodinated contrast mediu once about 1 , 500 ml of intraluminal contrast material has been infused , the iodinated contrast medium , heated to 37c , is injected intravenously with a common ct mechanical injector . it is advisable not to exceed the dose of 1 mg of iodine per kilo of body weight . 
according to most authors , the iv injection of iodinated contrast material is given as a single bolus at a rate of 34 ml / s with different scan delay times . some perform the classic arterial and portal venous phase scans , obtaining similar images in the two acquisitions . 
until now , the study of the parenchyma has influenced the way iodinated contrast agents have been administered , with various phases being required to identify and characterise parenchymal lesions . 
in our view , the study of bowel loops requires a different approach to the use of contrast media . the intestinal wall enhances with an adequate bolus of iv iodinated contrast material . 
in this method , 130 ml of iv iodinated contrast medium at a concentration of 400 mg iodine per millilitre ( iomeprol , iomeron 400 , bracco , italy ) is injected , with a scan delay of 80 s . 
during the first 40 s , the contrast medium is injected at a rate of 1 ml / s whereas during the next 30 s , it is administered at a rate of 3 ml / s ( table 4 )  . ten seconds after the infusion of iv iodinated contrast medium has been completed , the ct scan is started . 
this infusion protocol allows opacification of the arteries and enhancement of the mucosa ( provided by the bolus at 3 ml / s ) as well as slight opacification of the veins and intestinal wall la velocit pi lenta ha lo scopo di evitare al paziente lo stress da distensione improvvisa , ridurre la sensazione di nausea ed evitare il vomito . 
la velocit pi elevata serve a forzare la distensione delle anse e ad aumentare la vis a tergo al fine di spingere in avanti fino al colon destro il contrasto gi introdotto . linfusione di mdc deve continuare durante tutto il tempo della scansione per evitare lingestione eccessiva di aria da parte del paziente . 
luso di sostanze lipidiche , come mdc endoluminale negativo , permette una pi rapida iniezione manuale , ma non presenta sostanziali vantaggi iconografici . in italia , queste sostanze non risultano autorizzate come mdc e sono particolarmente costose . 
introdotta la quantit di circa 1500 ml circa di mdc intraluminale , si inietta il mdc iodato ev , riscaldato a 37 , con un comune iniettore meccanico da tc . 
secondo la maggior parte degli autori , liniezione del mdc iodato ev viene fatta con un bolo unico alla velocit di 34 ml / s con differenti tempi di ritardo di scansione . alcuni eseguono le scansioni classiche in fase arteriosa e venosa portale con risultati iconografici sostanzialmente sovrapponibili nelle due acquisizioni . altri hanno suggerito leffettuazione di una acquisizione singola , ma con tempi diversi di ritardo : 25 , 35 , 40 , 45 , 50 s . 
a nostro avviso , lo studio della parete delle anse richiede un diverso approccio alluso del mdc . la parete intestinale , infatti , si amplifica dopo un adeguato bolo di mdc iodato ev . 
vari autori hanno verificato che lenhancement mucoso ottimale nelle fasi arteriosa tardiva e venosa portale precoce . partendo da questi presupposti , alcuni autori hanno standardizzato una nuova modalit bifasica di infusione del mdc . vengono iniettati 130 ml di mdc iodato ev , alla concentrazione di 400 mg iodio / ml ( iomeprolo , iomeron 400 , bracco , italia ) , con ritardo di scansione di 80 s . 
durante i primi 40 s , il mdc iniettato alla velocit di 1 ml / s , mentre nei successivi 30 s il mdc somministrato alla velocit di 3 ml / s ( tabella 4 )  . 
this way , the abdomen lights up as a result of the simultaneous enhancement of the loop walls , vascular network and parenchyma , allowing analysis of the various components of the abdomen and intestine . 
it is often laborious and at times impossible in the axial images . instead , the use of mpr facilitates the anatomo - topographic location of the lesions and allows greater potential for assessing extension . 
the overall level of diagnostic confidence is significantly higher when the analysis of the axial scans is carried out with the aid of mpr . disadvantages of the method in addition to the undoubted advantages , msct enteroclysis also presents some disadvantages : the need for nasointestinal intubation the impossibility of checking the progression of the neutral intraluminal contrast as far as the right colon by fluoroscopy the possible suboptimal distension of the distal ileum the inability to identify superficial mucosal lesions the lack of functional information the high overall cost of the exam the high dose of ionising radiation r . 
when the lumen is well distended , wall thickness ranges from 1 to 2 mthe diameter of the lumen is pathological if it is greater than 4.5 cm in the proximal jejunum , 4 cm in the mid - bowel or 3 cm in the ileu the mesentery , at the centre of the abdomen , appears homogeneously hypodense due to its abundant fat component , and it is crossed by hyperdense vascular structures . a typical feature is the fan - shaped arrangement of the mesentery and the vessels contained in it . 
the omentum , located just underneath the anterior abdominal wall , lateral and anterior to the small bowel , appears as a homogenous structure , with the attenuation of fat , crossed by vessels . 
 conclusions loop distension achieved by nasointestinal intubation is excellent and valid for any imaging method selected for the study of the small bowel . loop distension achieved by oral contrast medium will never equal that obtained with intubation . 
criteria for establishing that the exam has been correctly performed are the identification of the methylcellulose in the right colon , which attests to its passage through the small bowel , and the uniform distension of all bowel segments . 
in definitiva , il livello di confidenza diagnostica globale significativamente pi elevato quando lanalisi delle scansioni assiali viene affiancata ed arricchita dalle mpr . svantaggi della metodica accanto agli indubbi vantaggi della metodica e - tcms , devono essere ricordati alcuni svantaggi : la necessit dellintubazione naso - intestinale ; limpossibilit di controllare fluoroscopicamente la progressione del mdc intraluminale neutro fino al colon destro ; la possibile distensione subottimale dellileo distale ; la mancata identificazione delle lesioni superficiali della mucosa ; lassenza di informazioni sugli aspetti funzionali ; lalto costo globale dellesame ; lelevata dose di radiazioni ionizzanti . 
quando il lume ben disteso , lo spessore della parete compreso tra 1 e 2 mil diametro del lume patologico se supera 4 , 5 cm nel digiuno prossimale , 4 cm nellintestino medio , 3 cm nellileo . 
lomento , situato giusto allinterno della parete addominale anteriore , lateralmente ed anteriormente rispetto allintestino tenue , appare come struttura omogenea , ad attenuazione di tipo adiposo , attraversata da vasi . conclusioni la distensione delle anse , ottenuta tramite intubazione naso - intestinale , risulta ottimale e valida per qualsiasi metodica dimaging scelta per lapproccio diagnostico al piccolo intestino . 
the current indications of msct enteroclysis are essentially inflammatory diseases of the small bowel and intestinal bleeding that cannot be defined by other means [ 2325 , 2730 ]  . new prospects have been opened up by the possibility of using mri in the study of the small bowel , as reported in the recent literature [ 3133 ]  . 
the current challenge is to publicise these modalities and disseminate a higher degree of diagnostic confidence in the assessment of the small bowel by ct and mri . rapida esecuzione , standardizzabile e ripetibile [ 1822 ]  . 
le attuali indicazioni della e - tcms sono rappresentate essenzialmente dalla malattia infiammatoria del piccolo intestino , ma anche dai sanguinamenti intestinali non altrimenti definibili [ 2325 , 2730 ]  . 
simonetti dipartimento di diagnostica per immagini e radiologia interventistica , universit degli studi di roma tor vergata , policlinico tor vergata , viale oxford 81 , i - 00133 roma , italy correspondence to : e . 
the development of new operative techniques in oral and maxillofacial surgery within the last few years has led to an increasing demand for dentascan examination , also in paediatric patients . 
dosimeters were applied to the eyes , mouth , parotid glands , thyroid and back of the neck of an anthropomorphic plexiglas phantom that underwent multidetector computed tomography ( mdct ) dentascan examinations . 
la quantit di esami dentascan eseguiti su richiesta specialistica aumentata drasticamente negli ultimi anni sia per una valutazione preimplantologica che per un approfondimento diagnostico di lesioni ossee focali a carico dei mascellari . 
 stato utilizzato un fantoccio antropomorfo testa - collo in plexiglass al quale stato applicato un dosimetro a lettura immediata nelle sedi corrispondenti agli occhi , alla bocca , alle parotidi , alla tiroide ed al collo posteriormente . 
il nostro studio , confortato da una iniziale applicazione clinico - diagnostica , vuole fornire una valida proposta per un protocollo dentascan che riduca sostanzialmente la quantit di dose fornita alle strutture anatomiche esposte senza inficiare il valore diagnostico dellesame . parole chiave dosimetria tomografia computerizzata dentascan introduction introduzione the increasing use of diagnostic imaging for dental implant planning justifies the growing interest in dosimetric estimates concerning the various imaging techniques . 
in particular , with the introduction of the dentascan reconstruction programme , the use of computed tomography ( ct ) in odontostomatology has gained increasing attention of both radiologists and dental surgeons [ 13 ]  . during the past few years , dentascan , initially limited to the management of problems concerning implantology , has been used in the study of all jaw diseases . 
during a tomographic evaluation of the jaw bones , the anatomic structures of the head and neck are irradiated . in the literature , several dosimetric studies have been undertaken in the field of odontostomatologic imaging diagnostics [ 46 ] , and the results are often inconsistent as a consequence of the evolution and type of device used . 
recently , a new dedicated machine has been introduced for extraoral digital imaging of the dental arches , based on the use of a radiant cone beam ( cone beam computed tomography , cbct )  . this technique was developed as an alternative to conventional ct in volumetric dental studies in order to reduce operating costs and the radiation dose administered to the patient [ 7 ]  . 
di recente introduzione un nuovo strumento dedicato per limaging digitale extraorale delle arcate dentarie basato sullutilizzo di un fascio radiante conico ( cone beam computer tomography , cbct )  . 
questa tecnologia si sviluppata come alternativa alla tc convenzionale nello studio volumetrico dentale al fine di ridurre i costi operativi e la dose di radiazioni fornita al paziente [ 7 ]  . 
lo scopo del nostro studio quello di dimostrare come , riducendo il voltaggio in un esame dentascan eseguito con tc spirale multistrato , sia possibile , senza modificare gli altri parametri di acquisizione , ottenere una sostanziale riduzione della dose fornita alle principali strutture anatomiche della testa e del collo , senza alterare la validit diagnostica dellimmagine ottenuta . 
il fine quello di proporre un protocollo di studio dentascan che riduca sostanzialmente la dose rispetto ai dati forniti dalla letteratura . materiali e metodi per le misurazioni stato utilizzato un fantoccio testa - collo in plexiglass riempito di acqua con le stesse caratteristiche antropomorfe di una testa umana . 
le successive scansioni sono state acquisite con uno spessore di strato di 1 , 25 mm , intervallo 0 , 6 mm , velocit di avanzamento 11 , 25 mm / rotazione , tempo di rotazione del tubo pari a 0 , 6 s , 200 ma , fov 13 , 7 cm , matrice 512 x 512 , inclinazione del gantry di 0 . 
the dosimeter was a directreading tema model set in micrograys , sensitive to xand gamma rays , dip.62 model , equipped with an energy - compensated gm detector ( model zp1313 ) and with a memory for storage of data regarding the absorbed dose . 
dose absorbed unit : milligrays tabella 3 misure dosimetriche riassuntive della nostra esperienza e confronto con i dati presenti in letteratura espressi come minimo e massimo per un esame tc mascellare / mandibola . 
nella tabella 1 , le dosi lette in micrograys ( mgy ) sul dosimetro sono trascritte in milligrays ( mgy ) per avere la stessa unit di misura con i dati raccolti dalla letteratura . 
the scanning technique consisted in a preliminary scan performed in the anteroposterior ( ap ) and laterolateral ( ll ) projections , with the following acquisition parameters : 120 kv or 80 kv , with 20 ma . the subsequent scans were taken with a 1.25 - mm slice thickness , 0.6 - mm interval , 11.25 - mm table speed / rotation , 0.6 - s rotation time , 200 ma , 13.7 - cm fov , 512x512 matrix , and 0 gantry angle . 
after each scan , the dose was read and the dosimeter was set to zero , each time considering the amount of dose absorbed during the preliminary scan in the ap and ll projections . results measurements taken with the dosimeter in the positions corresponding to the eyes , mouth , parotid glands , thyroid and back of the neck ( c3 / c4 ) are reported in tables 2 and 3 , which illustrate in detail the results achieved with all values obtained , with a comparison with those reported in the literature . in table 1 , doses read in micrograys on the dosimeter are reported in milligrays so as to have the same unit of measurement as that reported in the literature . 
6 limmagine acquisita secondo il piano assiale documenta una disodontiasi a carico di 38 ( inclusione e mesioangolazione ) e 48 ( inclusione e mesio - linguoangolazione )  . ments at each site were taken at 120 kv and 80 kv , respectively , in two separate imaging protocols , while the remaining acquisition parameters were identical . each item reported is the mean value of 11 measurements taken with the dosimeter in the same position , with scans taken separately at the level of the upper jaw bone and the mandible , taking into account the dose absorbed during the preliminary scan . mente a 120 kv e 80 kv in due corrispondenti protocolli di studio che prevedono valori identici per i restanti parametri tecnici di acquisizione . 
ciascun dato trascritto la media di 11 misurazioni effettuate con la stessa posizione del dosimetro ed eseguendo separatamente in tempi distinti lesame a livello del mascellare superiore e della mandibola considerando il contributo di dose dovuto al preliminare scanogramma . 
dalle ricostruzioni contigue risultano ben evidenti i rapporti tra lelemento dentario incluso e i denti contigui . 120 kv e 80 kv confrontati con i dati riportati in letteratura espressi come minimo e massimo [ 8 ]  . discussione mantenendo i mas costanti , la quantit di radiazioni in uscita da un tubo a raggi x incrementa con laumentare dellenergia dei raggi x cio con il voltaggio imposto . 
parallelamente , al diminuire dellenergia dei raggi x ( voltaggio ) , aumenta il contrasto tra le diverse strutture attraversate dal fascio di radiazioni [ 9 , 10 ]  . questo dato stato utilizzato nella nostra esperienza per determinare una sostanziale riduzione di dose senza alterare la qualit dellimmagine ottenuta . 
in letteratura numerosi studi si sono interessati della dosimetria nella radiologia odontostomatologica , spesso proponendo il confronto tra la tomografia computerizzata , le apparecchiature tomografiche a fascio radiante conico ( cbct ) e lortopantomografia . 
tali valori sono sostanzialmente comparabili , tenuto conto del progresso tecnologico delle apparecchiature utilizzate e delle diverse tecniche dosimetriche , con studi pi recenti [ 6 , 7 ]  . 
nella nostra esperienza i valori dosimetrici ottenuti e descritti riassuntivamente nella tabella 3 risultano abbondantemente inferiori ai valori minimi espressi in letteratura . anche quando confrontati con i valori di dose registrati sulle fascio radiante conico apparecchiature ( cbct ) , i risultati ottenuti nel nostro studio , con le ovvie approssimazioni legate alla diversa tecnologia e metodologia di analisi dosimetrica , sono sovrapponibili ; in alcune sedi anatomiche i valori di dose assorbita registrati nella nostra esperientomografiche a table 3 summarises the values obtained for the different anatomic structures , examined at 120 kv and 80 kv , respectively , compared with the data reported in the literature , and indicated as minimum and maximum [ 8 ]  . discussion when milliamperes are kept constant , the radiation dose delivered by an x - ray tube increases as the x - ray energy , that is the kilovoltage , increases . this effect is largely exploited in diagnostic imaging performed on babies or children , where a low radiation dose is required [ 9 , 10 ]  . as x - ray energy ( kilovoltage ) decreases the contrast between the structures crossed by the x - ray beam increases [ 9 , 10 ]  . 
 [ 8 ] reported the doses absorbed by anatomical sites studied using a ct scan in the pre - operative assessment of a dental implant . considering the technological progress of the devices and the different dosimetric techniques , these results are very close to those obtained by more recent studies [ 6 , 7 ]  . 
even when compared with the doses reported for cbct , with the obvious approximations linked to the different dosimetric techniques , our results were comparable , and the absorbed dose measured in our study was e . 
12 ricostruzioni panorex del caso esposto nella figura 9 . even lower in some anatomical sites [ 11 ]  . the eleven measurements taken for each examination all proved to be in the same order of dose , which confirms the reliability of the values obtained . a 50% to ten - fold reduction of the radiation dose was seen in the 80 - kv protocol compared with what is reported in the literature . 
this principle has been fully adopted by the italian law , article 2 of legislative decree 230 / 95 , which regulates all activities carrying a risk of ionizing radiation . 
therefore , our study continues this line of research [ 1315 ] by suggesting a protocol that significantly reduces the dose administered to the anatomical structures involved by a dentascan exam without affecting diagnostic accuracy . in our department of diagnostic imaging , all dentascan exams are currently performed with the 80 - kv protocol , with excellent results in terms of image quality . 
i tomografi a fascio radiante conico ( cbct ) , caratterizzati da una dose relativamente bassa di radiazioni , sono indicati solo nella diagnostica dellimplantologia di base e dei traumi . 
inoltre , lutilizzo di tali apparecchiature , limitato esclusivamente allimaging del distretto maxillo - facciale , ne giustifica , in termini di rapporto costo beneficio , un impiego esclusivo nei reparti di chirurgia orale e maxillo - facciale . 
dai dati ottenuti si evidenzia inoltre come parotidi , tiroide e bocca siano le strutture anatomiche pi esposte a radiazioni durante un esame tc dentascan sia del mascellare superiore che dellinferiore , in linea con quanto documentato in precedenti studi [ 5 ]  . 
la sempre maggiore richiesta di esami dentascan a fini implantologici e la sempre pi estesa applicazione di questa tecnica sulla popolazione pediatrica impone una maggiore attenzione su questo tipo di attivit diagnostica , al fine di ottimizzare la tecnica e ridurre la dose ai livelli pi bassi ragionevolmente ottenibili . 
il nostro studio si inserisce pertanto in questo filone di ricerca [ 1315 ] , fornendo una proposta di protocollo che riduca sostanzialmente la quantit di dose fornita alle strutture anatomiche esposte durante un esame dentascan senza inficiare il valore diagnostico dellesame . 
attualmente presso il nostro dipartimento di diagnostica per immagini tutti gli esami dentascan vengono eseguiti con il protocollo a 80 kv con risultati ottimali per quanto riguarda la qualit dellimmagine ottenuta . 
ulteriori studi potranno essere utili per dimostrare che risultati diagnostici validi sono raggiungibili con una ulteriore riduzione del voltaggio nonch dellintensit di corrente e levoluzione tecnologica e dei software render possibile ci nel futuro prossimo venturo . acknowledgements we thank valerio valeri ( trm ) for the valuable collaboration . ringraziamenti si ringrazia per la collaborazione il sig . 
in order to define the optimal radiological procedure , kerma - area product ( kap ) measurements and evaluations of image quality in fluoroscopy and fluorography mode were made using dedicated phantoms . 
with the defined radiological procedure , the obtained kap values are lower than recorded doses in interventional radiology , and the corresponding values of entrance skin dose are lower than the threshold dose for deterministic effects . 
considering the effective dose at the median kap value , the probability for stochastic effects is shown to be low , at approximately 1 in 39 , 000 . key words swallow videofluoroscopy kerma - area product effective dose riassunto obiettivo . 
utilizzando specifici fantocci , sono stati misurati i valori del prodotto kerma per area ( kap ) ed stata valutata la qualit dellimmagine nelle diverse modalit di esposizione fluoroscopica e fluorografica , al fine di definire la procedura da impiegare in ambito clinico . 
stato quindi costituito un campione di studio di 22 pazienti , di ciascuno dei quali sono stati registrati il kap , il tempo totale di acquisizione e la tensione media impostata . 
la mediana , il primo e il terzo quartile della distribuzione dei valori di kap sono risultati rispettivamente uguali a 2 , 1 , 1 , 5 e 2 , 7 gy cm2 , corrispondenti a un valore di dose efficace di 0 , 35 , 0 , 26 e 0 , 46 msv . 
i valori di kap ottenuti impiegando la procedura radioscopica definita sono significativamente inferiori a quelli tipicamente registrati per le procedure di radiologia interventistica e i corrispondenti valori della dose in ingresso alla superficie del paziente ( esd ) sono minori del primo valore soglia per i danni di natura deterministica . 
considerando il valore della dose efficace corrispondente alla mediana del kap , si ricava infine che la probabilit di insorgenza di effetti stocastici significativamente basso , approssimativamente 1 su 39.000. parole chiave deglutizione videofluoroscopia prodotto kerma per area dose efficace l . 
performing periodic dosimetric assessments is therefore advisable for this type of examination , on the basis of which the necessary corrective measures may be taken to reduce the dose to the patient while obtaining sufficient diagnostic information . the aim of this study was to optimise the technique by defining optimal exposure parameters as well as estimate the associated radiological risk in terms of both effective and organ dose . lo studio dinamico mediante tecnica radioscopica della regione oro - faringea viene spesso impiegato per la valutazione funzionale dellatto deglutitorio [ 1 ] , perch consente la diagnosi delle alterazioni patologiche della deglutizione e costituisce un valido strumento per la programmazione e la verifica delle tecniche riabilitative . 
tuttavia , sebbene non vi siano indicazioni per includere lo studio radioscopico della deglutizione tra le procedure comportanti alte dosi di radiazione [ 25 ] , il paziente suscettibile di ricevere una dose di radiazione indebita qualora la tecnica e i parametri di esposizione non vengano ottimizzati . 
quindi opportuno che anche per questo tipo di esami vengano eseguite periodiche valutazioni dosimetriche , sulla base delle quali adottare eventuali misure correttive necessarie a ridurre la dose al paziente , compatibilmente con lottenimento di adeguate informazioni diagnostiche . scopo del presente lavoro stato quello di ottimizzare la tecnica , attraverso la definizione dei parametri di esposizione ottimali , e di stimare il rischio radiologico associato in termini di dose efficace e di dose agli organi . materials and methods materiali e metodi the dosimetric assessments were performed with an rti electronics system ( molndal , sweden ) made up of a doseguard 100 connected to a vacutec - 70157 ionization chamber with a sensitive surface of 145x145 mm and a filtration less than 0.5 mm al capable of measuring the kerma - area product ( kap ) and the total exposure time . 
the unit of measure is the grays per centimetre squared ( gycm2 )  . calibration of the dosimetric system was verified with a model 96020c ionization chamber connected to a 35050a dosimeter ( keithley instruments , cleveland , oh , usa )  . values of both the effective dose and the dose to the organs were calculated from kap values using the winods calculation program ( rti electronics , molndal , sweden ) [ 6 ] , which determines the distribution of the dose as a function of the area and filtration of the incident beam of radiation on the patient , simulated using a phantom modifiable in size and gender . 
i valori della dose efficace e della dose agli organi sono stati calcolati a partire dai valori di kap utilizzando il programma di calcolo winods ( rti electronics , molndal , svezia ) [ 6 ] , il quale determina la distribuzione della dose in funzione dellarea e della filtrazione del fascio di radiazione incidente sul paziente simulato da un fantoccio virtuale antropomorfo regolabile in dimensione e sesso . 
al fine di fornire una stima rappresentativa della dose alla popolazione in generale , stato considerato un paziente adulto normotipo , con peso e altezza pari a 70 kg e a 173 cm [ 6 ]  . tutti gli esami sono stati effettuati utilizzando un apparecchio telecomandato digitale prestige vh ( ge medical systems , milwaukee , usa ) dotato di intensificatore di brillanza da 12 pollici , tubo rx con macchia focale da 0 , 6 e da 1 , 25 , tensione massima pari a 150 kv in grafia e 120 kv in scopia , in grado di eseguire esami funzionali in modalit sia fluoscopica che fluorografica . 
to optimise diagnostic quality of the examination and dose to the patient in both modes , the operator may choose between three contrast curves that automatically regulate the exposure parameters . 
on the basis of the curve chosen , three different values of current to the tube are associated to the same voltage value . to define the optimal exposure technique in terms of dose to the patient , the kap was measured during a series of dynamic acquisitions with an rs - 230t phantom ( rsd , long beach , ca , usa ) in fluorography and fluoroscopy with the three contrast scales . 
image quality obtained in the two modes was assessed by exposing a tor 18fg phantom ( faxil , leeds , uk ) positioned on a 15 - cm block of perspex placed on the radiological table 100 cm from the focus . a group of 22 patients ( 15 men and seven women ) obtained in conditions of routine activity and aged between 39 and 84 years who presented with acute ( stroke , head injury and brain tumours ) or chronic ( parkinsons disease , multiple sclerosis and amyotrophic lateral sclerosis ) pathological neurological conditions underwent the optimised fluoroscopic examination . kap , total fluoroscopy time and mean voltage were recorded for each patient . 
since swallowing alterations were significantly different , examinations were not performed with a standard protocol but , rather , with individual settings . in general , the study was performed with the patient seated about 1 m from the x - ray tube in the lateral projection , with a field of view having a 20 - cm diameter centred on the pharyngeal region during the swallowing of a bolus of contrast material in the form of a paste , which , according to patient conditions , was either liquid , semi - liquid , semi - solid or solid . 
the boluses were prepared using a small quantity ( 510 ml ) of iopamidol ( 61.2% weight volume , gastromiro , bracco , milan , italy ) in the pure state or mixed with a thickening substance ( resource thickenup , novartis medical nutrition , fremont , mi , usa ) or with dry biscuits . 
in special cases , the examination was preceded by a short acquisition in anteroposterior ( ap ) projection during the production of the sound eee to assess motility of vocal cords and the larynx . none of the patients required assistance during the period of irradiation , allowing operators to remain within the shielded control room . results dose values and level of image quality with respect to fluoroscopic and fluorographic modes given the same field of irl . 
per ottimizzare la qualit diagnostica dellesame , nonch la dose al paziente in entrambe le modalit , loperatore pu scegliere fra tre curve di contrasto , che regolano automaticamente i parametri di esposizione . 
per definire la tecnica di esposizione ottimale in termini di dose al paziente , stato misurato il prodotto kerma per area durante una serie di acquisizioni dinamiche con un fantoccio antropomorfo rs - 230t ( rsd , long beach , usa ) nelle due modalit fluorografica e fluoroscopica al variare delle tre scale di contrasto . 
la qualit dellimmagine ottenuta con le diverse modalit stata valutata esponendo a 100 cm dal fuoco un fantoccio tor 18fg ( faxil , leeds , uk ) posto sopra un blocco di perspex da 15 cm , a sua volta appoggiato sul tavolo radiologico . un campione di 22 pazienti ( 15 maschi e 7 femmine ) ottenuto in condizioni di attivit routinaria , di et compresa tra 39 e 84 anni , che presentavano esiti di patologie neurologiche acute ( ictus , trauma cranico e tumori cerebrali ) o croniche ( parkinson , sclerosi multipla e sclerosi laterale amiotrofica ) , stato sottoposto allesame fluoroscopico ottimizzato . 
dal momento che i pazienti presentavano stati di alterazione della deglutizione molto diversi tra loro , gli esami non sono stati eseguiti secondo un protocollo standardizzato , ma sono stati impostati individualmente . 
in generale , lo studio stato effettuato con il paziente seduto a circa 1 metro dal tubo rx , in proiezione laterale , con un campo di vista di 20 cm di diametro centrato sulla regione faringea , durante la deglutizione di un bolo di mezzo di contrasto sotto forma di pasto che , a seconda delle condizioni del paziente , era di tipo liquido , semiliquido , semisolido o solido . 
per la preparazione dei boli sono state impiegate piccole quantit ( 510 ml ) di iopamidolo ( 61 , 2% pesovolume , gastromiro , bracco , milano , italia ) allo stato puro oppure mescolato con una sostanza addensante ( resource thickenup , novartis medical nutrition , fremont , mi , usa ) o con biscotti secchi . 
in alcuni casi particolari , lesame stato preceduto da una breve acquisizione in proiezione antero - posteriore durante la fonazione del suono iii per la verifica della motilit delle corde vocali e della laringe . 
tutti i pazienti esaminati non hanno richiesto assistenza durante il tempo di irradiazione , consentendo agli operatori presenti di rimanere allinterno della sala comandi schermata . risultati i valori di dose e di qualit dellimmagine relativi alle diverse modalit fluoroscopiche e fluorografiche , a parit di campo di irradiazione , sono riportati nella tabella 1 , insieme con i relativi parametri di esposizione selezionati dallapparecchiatura in modo automatico . 
in terms of radiation dose , the fluoroscopic technique with the least exposure to the patient is indicated with the letter c , which on average uses high doses of voltage but relatively low current . 
this choice does not significantly affect image quality in terms of spatial resolution and contrast threshold in that the results obtained are comparable with those regarding the other contrast curves and are compatible with the acceptability criteria indicated in annex v of the legislative decree 187 / 00 [ 2 ]  . results obtained with the fluorographic technique , while on the one hand provide greater image quality sharper images with improved contrast , on the other hand involve high and , in our opinion , unjustifiable exposure to the patient . 
per facilitare il confronto , riportato il rateo del kap , ovvero il valore del prodotto kerma per area per unit di tempo . dal punto di vista dosimetrico , la tecnica fluoroscopica che comporta la minor esposizione del paziente quella indicata con la lettera c , che utilizza valori mediamente elevati di tensione associati , per , a correnti relativamente basse . 
questa scelta non penalizza sostanzialmente la qualit dellimmagine , in termini di risoluzione spaziale e soglia di contrasto , in quanto i risultati ottenuti sono confrontabili con quelli relativi alle altre curve di contrasto e sono comunque conformi ai criteri di accettabilit indicati nellallegato v al d . 
i risultati ottenuti con la tecnica fluorografica , se da un lato consentono di ottenere immagini qualitativamente migliori , ovvero pi nitide e con un miglior contrasto , comportano unelevata e , a nostro giudizio , inopportuna esposizione del paziente . 
the major salivary glands were also considerably included within the field of irradiation during the entire exposure time , with the median dose value absorbed by these glands , depending on their position , ranging from 5 to 7 mgy . 
the dose absorbed by the eyes , which were situated on the edge of the field , depended significantly on the centring of the beam and inclination of the patients head , varying between less than 1 and several mgy . 
sono ampiamente comprese allinterno del campo di irradiazione durante tutto il tempo di esposizione anche le ghiandole salivari maggiori ed stato calcolato che il valore mediano della dose assorbita da queste ghiandole varia , in base alla loro posizione , tra 5 e 7 mgy . 
la dose assorbita dagli occhi , che si trovano invece in corrispondenza del bordo del campo , dipende fortemente dalla centratura del fascio e dallinclinazione della testa del paziente e pu variare da meno di 1 a qualche mgy . 
i valori relativi al tempo di esposizione sono compresi nellintervallo da 84 a 306 secondi . lanalisi dei dati mostra che esiste una relazione lineare tra landamento del tempo di esposizione e i valori del kap . 
nella tabella 2 sono riportati per esteso i risultati ottenuti . discussion the dynamic swallow study with radioscopic examination is widely used to assess swallowing disorders in the oral and pharyngeal phase and provides useful information for assessing treatment results . for these reasons , many patients undergo this type of examination , even several times in as many weeks , during which they may receive unjustifiably high doses of radiation if a radiological procedure analysis and an assessment of dose and associated radiological risk are not performed . 
the european atomic energy community ( euratom ) directive 97 / 43 [ 4 ] regarding medical exposure requires that reference levels of doses be established and used to optimise the carrying out of radiodiagnostic examinations . 
a useful tool for assessing the risk associated with a radiological prodiscussione lo studio dinamico della deglutizione mediante esame radioscopico largamente impiegato per la valutazione dei disordini disfagici nella fase orale e faringea del meccanismo deglutitorio e fornisce elementi utili per la verifica dei risultati del trattamento riabilitativo . 
per queste ragioni , sono numerosi i pazienti sottoposti a questo particolare tipo di esame , anche pi volte nel giro di poche settimane , i quali possono ricevere dosi indebite qualora non si effettui unanalisi della pratica radiologica e una contestuale valutazione della dose e del rischio radiologico associato . 
la direttiva 97 / 43 euratom [ 4 ] sulle esposizioni mediche richiede inoltre di stabilire e impiegare livelli di dose di riferimento ai fini dellottimizzazione dellesecuzione degli esami radiodiagnostici . 
this is a highly practical technique in that it enables the dose of each patient to be recorded , particularly in the case of complex procedures , which require the simultaneous use of radiographic and fluoroscopic techniques and which are often associated with constant changes to exposure parameters , size of radiation field and anatomical region involved . the chamber is connected in front of the window of the xray tube and is transparent to both the light of the centring device and radiation and therefore does not interfere with the diagnostic procedure and enables measurement to be performed during examination . results reveal that the fluoroscopic technique provides good diagnostic quality and significantly reduces the dose to the patient with respect to the acquisition of a series of digital images obtained with the fluorographic technique . 
although management of digital images is undoubtedly much simpler with respect to images stored on vhs , avoiding the high levels of radiation exposure associated with fluorography is also recommended [ 7 ]  . once fluoroscopy had been established as the optimal technique , we recorded kap values for each patient available for the dynamic swallow study , without setting conditions regarding their size , to establish a typical dose value for this type of examination . 
the limited number of subjects in the group did not enable a diagnostic reference level to be established with a reasonable degree of accuracy for this procedure , but it was enough to define an estimate of dose at the local level [ 5 ]  . although total fluoroscopy time is not always a reliable indicator of the dose to the patient in interventional radiological procedures [ 8 ] , in the dynamic swallow study , the calculations performed showed a statistically significant correlation with the kap . 
in fact , for this particular fluoroscopic examination , the anatomical regions involved , exposure parameters and geometrical factors , including the irradiated area , do not vary significantly from patient to patient . fluoroscopy time , therefore , is a practical tool for the assessment of dose to the patient for this particular examination , even in the absence of the ionization chamber . variation in dosimetric results obtained depends on the inability to utilise a standard acquisition protocol , given the need to tailor the number of contrast boluses and the duration of exposures to the physical state and level of cooperation of each individual patient . the distribution of kap values is therefore asymmetrical , tailing out towards the high doses , with the mean higher than the median . 
the results show that kap values obtained with the defined radioscopic procedure are significantly lower than those recorded for interventional radiological procedures [ 8 , 9 ] , thus confirming the findings of prior studies [ 10 , 11 ] , and the entrance surface dose of the patient is such to exclude the possibility of this medical exposure producing deterministic damage to the skin [ 3 ]  . prodotto kerma per area ( kap ) per mezzo di una camera a ionizzazione a trasmissione . 
il principale vantaggio che deriva dal suo impiego lestrema praticit , in quanto consente di registrare la dose per ciascun paziente , soprattutto nel caso di interventi complessi , i quali comportano il contemporaneo utilizzo della tecnica radiografica e fluoroscopica , spesso associati a continue variazioni dei parametri di esposizione , delle dimensioni del campo di radiazione e della regione anatomica di interesse . 
la camera , infatti , collocata nellapposita guida porta - accessori davanti alla finestra del tubo radiogeno e risulta trasparente sia alla luce del centratore luminoso , sia alla radiazione , non interferendo con le procedure diagnostiche e rendendo cos possibile la misura contestualmente allesecuzione dellesame . stato verificato che la modalit fluoroscopica consente di ridurre sensibilmente la dose al paziente , conservando una buona qualit diagnostica , rispetto allacquisizione di una serie di immagini digitali ottenute con la tecnica fluorografica . 
indubbio che la gestione delle immagini digitali risulta assai pi semplice rispetto alle immagini registrate su nastro vhs , ma altres raccomandabile evitare gli elevati valori di dose associati alla modalit fluorografica [ 7 ]  . una volta definita la modalit fluoroscopica ottimale , stato registrato il valore del kap relativo a tutti i pazienti disponibili per lo studio dinamico della deglutizione , senza porre condizioni sulla loro corporatura , in modo da determinare un valore di dose tipico per questo tipo di esame . 
il campione numericamente limitato non consente di stabilire con un buon grado di accuratezza un livello diagnostico di riferimento ( ldr ) per questa procedura , ma sufficiente per definire una stima di dose a livello locale [ 5 ]  . sebbene il tempo totale di fluoroscopia non risulti sempre un indicatore attendibile della dose al paziente nelle procedure di radiologia interventistica [ 8 ] , nel caso dello studio dinamico della deglutizione i calcoli effettuati evidenziano una correlazione statisticamente significativa con il kap . per questo particolare esame fluoroscopico , infatti , i distretti anatomici interessati , i parametri di esposizione e i fattori geometrici , compresa larea irradiata , non variano significativamente da paziente a paziente . 
la variabilit dei risultati dosimetrici ottenuti dipende invece dallimpossibilit di attenersi a un protocollo di acquisizione standard , dovendo necessariamente adeguare il numero dei boli di contrasto e la durata delle esposizioni allo stato fisico e al grado di collaborazione del singolo paziente . 
the purpose of this study was to investigate supraspinatus tendon sonographic morphology in a population of young overhead athletes in correlation with main pathologic models of secondary shoulder impingement syndrome . 
between april and may 2004 , 20 subjects ( ten professional basketball players and ten non - athlete controls of the same age , weight and height ranges ) underwent bilateral , standardised , sonographic sholulder examination to evaluate supraspinatus echotexture , supraspinatus and subacromial bursa thickness , subacromial space width ( cutoff of 7 mm ) and dynamic anterior impingement beneath the acromial marg results . 
despite the study limitations , ultrasonography ( us ) is able to detect subacromial space narrowing in young overhead athletes as early shoulder impingement sign , according to the continuum impingement - instability pathologic model . key words sport lesions sonographic examination of shoulder sonographic examination of tendons subacromial impingement syndrome shoulder instability riassunto obiettivo . 
quattro giocatori mostravano segni e sintomi di instabilit di spalla atraumatica destra ( 2 casi ) o di impingement del sovraspinato con dolore anteriore di spalla ( 1 spalla destra ed 1 spalla sinistra )  . 
nonostante i limiti dello studio , lecografia in grado di individuare il restringimento dello spazio subacromiale in atleti overhead giovani come segno precoce di impingement del sovraspinato , in accordo con il modello patogenetico del continuum impingement - instabilit . parole chiave lesioni da sport spalla , ecografia tendini , ecografia sindrome di impingement subcromiale instabilit introduction introduzione r . 
among shoulder pathologies , secondary supraspinatus impingement syndrome frequently affects so - called overhead sports players , sometimes with the risk of compromising athletic careers [ 1 ]  . during the last few years , increasing understanding and subtler classification of pathologic mechanisms responsible for this condition have enabled more appropriate orthopaedic treatments than in the past , leading to more acceptable clinical and functional results [ 2 ]  . 
all subjects underwent preliminary clinical examination as previously described [ 7 ] , including neer and hawkins tests for anterior and posterior impingement and apprehension and relocation tests for instability . standardised morphological study of the supraspinatus tendon was performed by a senior sonographer with 10 - years experience in musculoskeletal radiology targeted to tendon il movimento overhead , caratterizzato dalla elevazione del braccio al di sopra dei 90 associato ad abduzione ed extrarotazione , caratteristico di diverse discipline sportive e la sua biomeccanica ed i riflessi patologici sullarticolazione di spalla sono stati ampiamente studiati negli ultimi anni [ 1 ]  . fra le patologie di spalla la sindrome da impingement secondario del tendine sovraspinato affligge di frequente i giocatori di sport cosiddetti overhead , comportando il rischio di compromettere la carriera atletica [ 1 ]  . 
negli ultimi anni una comprensione progressiva ed una classificazione pi approfondite dei meccanismi patogenetici responsabili di questa condizione hanno permesso trattamenti ortopedici pi appropriati rispetto al passato con risultati pi accettabili in termini clinici e di recupero funzionale [ 2 ]  . 
il tendine del sovraspinato coinvolto elettivamente nei disordini secondari della cuffia dei rotatori , indipendentemente dalla loro etiologia [ 3 ]  . lecografia , specialmente in mani di operatori esperti , considerata attualmente indagine di primo livello nella diagnosi di impingement o di lesioni del sovraspinato , in virt della elevata risoluzione spaziale , del buon contrasto tissutale e della multiplanariet , con risultati sovrapponibili a quelli della rm specie nellindividuazione e nella quantificazione delle lesioni tendinee [ 4 ]  . 
i criteri di esclusione erano rappresentati da alterazioni muscolari dovute a precedenti traumi di spalla , malattie sistemiche muscoloscheletriche e / o assunzione corrente di fans o di steroidi . tutti i soggetti sono stati sottoposti in via preliminare ad una visita clinica come precedentemente descritto [ 7 ] , comprendente i test di neer e di hawkins per limpingement anteriore e posteriore ed i test di apprensione e di relocation per linstabilit . 
lo studio morfologico standardizzato del tendine sovraspinato stato eseguito da un ecografista esperto con 10 anni di esperienza nel settore muscoloscheletrico , mirato ai siti tendinei ed extra - tendinei tipicamente coinvolti nella sindrome da impingement [ 8 ]  . 
lo spessore del tendine stato misurato in prossimit dellinserzione sulla testa omerale , fra la superficie inferiore della borsa ed il margine inferiore visibile della struttura fibrillare . and extra - tendon sites of typical involvement in impingement syndrome [ 8 ]  . 
examination starts with the probe placed parallel to the longitudinal tendon axis ( paracoronal plane ) with the shoulder internally rotated and extended by positioning the arm behind the back in order to increase the extent of supraspinatus lateral to the acromial shadow [ 9 ]  . 
lo spessore del tendine stato misurato dalla sutable 1 tendon echotexture was interpreted based on a division into grades , following neers classification of tendon tears [ 10 ] tendon echotexture fibrillar hypoechoic hyperechoic iiia partial tear iiib full - thickness tear tabella 1 lecostruttura del tendine stata interpretata in base ad una suddivisione in gradi , operata sulla falsariga della classificazione di neer delle lesioni tendinee [ 10 ] ecostruttura del tendine fibrillare ipoecogena iperecogena iiia iiib lesione parziale lesione a tutto spessore table 2 criteria for interpretation of the other sonographic parameters considered [ 9 , 10 ] increased reduced tendon thickness , mm bursal thickness , mm subacromial space , mm anterior impingement spazio subacromiale , mm impingement anteriore normal present normale presente absent assente tabella 2 criteri di interpretazione degli altri parametri ecografici considerati [ 9 , 10 ] spessore del tendine , mm spessore della borsa subacromiale , mm aumentato ridotto r . 
dynamic passive abduction of the arm from this position assesses tendon integrity and the presence or absence of tendon impingement beneath the acromial margrepositioning the arm in the original posiperficie inferiore della borsa perpendicolarmente fino al margine inferiore dove lecostruttura fibrillare risulta chiaramente visibile . 
la sonda successivamente posizionata perpendicolarmente al maggior asse tendineo ( piano parasagittale ) , con lavambraccio flesso a 90 sul braccio , a sua volta addotto al tronco con la mano poggiata sulla spalla controlaterale . la successiva abduzione passiva del braccio volta a stabilire lintegrit del tendine e la presenza od assenza di impingement del tendine al di sotto del margine dellacromion . 
none of the sonographic measurements is pathological in relation to the criteria selected mean bursal thickness , mm tendon thickness , mm subacromial space , mm impingement echotexture spessore borsa , mm spessore tendine , mm spazio subacromiale , mm impingement ecostruttura dx , spalla destra ; sx , spalla sinistra ; ds , deviazione standard r , right shoulder ; l , left shoulder ; sd , standard deviation tabella 4 reperti ecografici nei soggetti di controllo non - atleti . 
4a , b player with right shoulder paon the basis of the selected cut - off , the width of the right subacromial space is moderately reduced ( a ) whereas the contralateral space ( b ) is normal . 
measurement of the subacromial space in the parasagittal scan , lateral to the acromion shadow cone , between the point of entry of the tendon at dynamic abduction and the humeral - head cortical fig . 
misurazione dello spazio subacromiale in scansione parasagittale , effettuato lateralmente al cono dombra dellacromion fra il punto di ingresso del tendine alla manovra dinamica di abduzione e la corticale della testa omerale r . 
imaging was interpreted following criteria reported in tables 1 and 2 , according to expected clinical and sonographic patterns previously described [ 9 , 10 ] and choosing a cut - off of 7 mm for subacromial space width . 
statistical analysis on measurements lacking a definite cut - off for pathology ( tendon and bursal thicknesses ) was based on a two - tailed u mann - whitney test whereas the one - tailed fisher exact test was used for the other parameters . 
four players showed symptoms and positive clinical signs of secondary supraspinatus impingement syndrome at an early stage : two right shoulder atraumatic instability ( previous spontaneous subluxation episode in one case ) , and anterior shoulder pain in one right assenza di restringimento per lampiezza dello spazio subacromiale . 
lanalisi statistica sulle misure che difettavano di un cut - off patologico definito ( spessori del tendine e della borsa ) si avvalsa di un test u di mann - whitney a due code , mentre per gli altri parametri stato utilizzato il test esatto di fisher ad una coda ; in entrambi i casi il livello di significativit era fissato al 5% ( p < 0 , 05 )  . risultati tutti i soggetti erano destrimani . 
quattro giocatori mostravano sintomi e test clinici positivi suggestivi di impingement secondario del sovraspinato ad uno stadio iniziale : 2 instabilit atraumatiche di spalla destra ( episodio di sublussazione spontanea in 1 caso ) e dolore anteriore di spalla a carico di 1 spalla destra e di 1 spalla sinistra ( con scrosci articolari nel primo caso )  . 
i rilievi ecografici sono riportati neltabella 6 classificazione secondo belling srensen e jrgensen dellimpingement della cuffia dei rotatori secondo il modello del continuum impingement - instabilit ( modificata da [ 2 ] ) r . 
no significant sonographic differences were found between players and controls in tendon echotexture ( all cases classified as grade 0 ) and in dynamic anterior impingement testing ( absent in all cases )  . 
gli spessori del tendine e della borsa subacromiale non mostrano significativa differenza fra le spalle di destra e di sinistra allinterno dello stesso gruppo e fra i 2 gruppi ( p > 0 , 05 ) ( tabella 5 )  . 
lo spazio subacromiale risulta ridotto in ampiezza sia a destra ( a ) che a sinistra ( b ) , pur in assenza di alterazioni ecostrutturali a carico del tendine sovraspinato e della borsa subacromiale . discussion basketball is considered an overhead sport due to repeated shooting and passing , throwing - like movements , studied in the throwing model , characterised by typical elevation - abduction - extrarotation of the arm , which lead to functional overload and mechanical stress of the supraspinatus [ 11 ]  . 
neers pathogenic model , which explains primary supraspinatus impingement as a consequence of a primitive narrowing of the subacromial space , cannot alone explain the association of supraspinatus lesions with shoulder instability in overhead players [ 12 ] , as demonstrated by the fact that surgical intervention on instability does provide symptom relief and acceptable functional recovery whereas acromionplasty and / or surgical - cuff decompression fails this goal in most cases [ 13 ]  . 
a supraspinatus tendon can be damaged , primarily as a consequence of an eccentric tensile overload responsible of tears [ 15 ] or when chronically impinged during throwing movement between the humeral head and the postero - superior capsular labrum in the so - called postero - superior impingement ( or internal impingement ) [ 13 , 16 ]  . 
according to the continuum impingement - instability pathologic and clinical model , supraspinatus impingement in overhead athletes would be a consequence of a primary narrowing of the subacromial space that occurs in a spectrum of clinical conditions , which vary from pure impingement as described by neer , usually more frequent in older athletes ( > 35 years ) , to pure instability , prevailing in young athletes ( 1835 years )  . 
in our series , in comparison to a control group of ten non - athlete subjects with no clinical or sonographic evidence of supraspinatus impingement , 6 / 10 modello del lancio , caratterizzati dalla tipica elevazione - abduzione - extrarotazione del braccio e responsabili di sovraccarico funzionale e di stress meccanico del tendine sovraspinato [ 11 ]  . 
il modello patogenetico di neer , che riconduce limpingement primario del sovraspinato ad un restringimento primitivo dello spazio subacromiale , non in grado di spiegare da solo lassociazione delle lesioni tendinee con linstabilit di spalla [ 12 ] , come dimostrato dal fatto che la correzione chirurgica dellinstabilit determina un beneficio sintomatico ed un recupero funzionale accettabili , mentre lacromionplastica e / o la decompressione chirurgica della cuffia perlopi falliscono questo obiettivo [ 13 ]  . in pi , stata riportata una caratteristica prevalenza di lesioni tendinee del versante articolare piuttosto che di quello bursale negli atleti overhead giovani con spalla dolorosa [ 14 ]  . 
il danno tendineo pu essere primitivo , come conseguenza di un sovraccarico tensivo ( eccentric tensile overload ) responsabile di lacerazioni [ 15 ] o di un impingement cronicamente ripetuto , durante il movimento di lancio , fra la testa omerale ed il labbro capsulare postero - superiore , nel cosiddetto impingement postero - superiore ( o impingement interno ) [ 13 , 16 ]  . secondo il modello patogenetico e clinico del continuum impingement - instabilit limpingement del sovraspinato negli atleti overhead sarebbe conseguenza di una primitiva riduzione in ampiezza dello spazio subacromiale nel contesto di uno spettro continuo di condizioni cliniche variabili dal puro impingement come descritto da neer , di solito pi frequente negli atleti vecchi ( > 35 anni ) , fino allinstabilit pura , prevalente negli atleti giovani ( 1835 anni ) , passando attraverso una serie di condizioni intermedie con caratteristiche miste , ciascuna delle quali richiede un trattamento adeguato ( tabella 6 ) [ 2 , 14 ]  . nella nostra esperienza in confronto ad un gruppo di controllo di 10 soggetti non atleti senza evidenza clinica od ecografica di impingement del sovraspinato , 6 giocatori di basket su 10 hanno mostrato un significativo restringimento dello spazio subacromiale allecografia : di quello destro ( spalla dominante ) in 2 casi asintomatici ed in 1 caso di spalla dolorosa , di quello sinistro ( spalla non dominante ) in 1 caso di r . 
6 the subacromial space of the right shoulders ( dominant ) in the players group is reduced in a significant number of cases compared with the control group ( no reduction )  . 
6 lo spazio subacromiale delle spalle di destra ( dominanti ) nel gruppo dei giocatori ridotto in un numero significativo di casi rispetto al gruppo di controllo ( non riduzione )  . 
us + , spazio subacromiale < 7 mm ; us - , spazio subacromiale 7 msullasse delle ordinate riportato il numero di spalle osservate . basketball players showed sonographic subacromial space narrowing : right dominant in two asymptomatic cases and in one case of painful shoulder , left non - dominant in one case of painful shoulder and bilaterally in two cases of right atraumatic instability . 
because of the insufficient accuracy of this sonographic measurement , despite the fact that reliability comparable to standard radiography has been reported [ 19 ] , we preferred a lower cut - off to be sure of effective space narrowing . 
in particular , no tendon thickness measurements were considered pathologic because of its high interobserver variability reported to be as high as 56% in one study on asymptomatic subjects [ 20 ]  . the same considerations were extended to subacromial bursa thickness . 
the data obtained are in agreement with the concept of a primitive space narrowing in athletes as a cause of supraspinatus impingement , independently from clinical onset and before the sonographic evidence of tendon damage becomes visible . meanwhile , a study [ 21 ] on subject , affected by impingement syndrome undergoing rehabilitation demostrated a significant association between progressive increase of subacromial space ( initially reduced ) and functional recovery . spalla dolorosa e bilateralmente in 2 casi di instabilit destra atraumatica . 
stato scelto un cut - off di ampiezza dello spazio subacromiale di 7 , 0 mm come compromesso fra i valori medi ottenuti nel corso della nostra esperienza clinica ( 6 , 0 mm ) [ de candia , presentato allecr 2002 ] e quelli di soggetti normali misurati in rm con il braccio in posizione neutra abdotto di 30 in due diversi studi ( rispettivamente di 7 + / 1 , 6 mm e di 8 , 18 + / 1 , 0 mm ) [ 17 , 18 ]  . dato lampio margine di inaccuratezza di questa misurazione in ecografia , nonostante essa sia risultata sovrapponibile a quella radiografica utilizzata come standard [ 19 ] , abbiamo preferito un cut - off abbastanza basso per essere sicuri di una effettiva riduzione dello spazio . 
in particolare , nessuna misurazione dello spessore tendineo stata ritenuta anormale , considerato la sua notevole variabilit interosservatore , riportata del 56% in uno studio condotto su soggetti asintomatici [ 20 ]  . analoga considerazione vale per lo spessore bursale . i dati ottenuti sono in accordo con lipotesi di un restringimento primitivo dello spazio subacromiale quale causa di impingement del sovraspinato , indipendentemente dalla manifestazione clinica e prima che si renda evidente allecografia un danno del tendine . ulteriore conferma fornita da uno studio [ 21 ] condotto su soggetti con sindrome da impingement sottoposti a riabilitazione nel quale stata dimostrata una significativa associazione fra lincremento progressivo dello spazio subacromiale ( inizialmente ridotto ) ed il recupero funzionale , suggerendo che la misurazione dello spazio subacromiale possa aiutare ad identificare i soggetti in grado di trarre beneficio dalla riabilitazione . lo studio soffre di alcune limitazioni . 
statistical power is low due to the small population studied , so further studies are required on larger groups of overhead athletes to confirm our results and establish the accuracy of us in detecting early morphological changes in the subacromial space . della variabilit interosservatore ed intra - soggetto delle misurazioni ecografiche , parzialmente compensata dalla stretta aderenza ai criteri di misurazione stabiliti . 
simonetti dipartimento di diagnostica per immagini e radiologia interventistica , universit di roma tor vergata , policlinico , viale oxford 81 , i - 00133 rome , italy correspondence to : e . 
magnetic resonance imaging ( mri ) and mrsi were performed on 39 patients with prostate - specific antigen ( psa ) levels greater than 4 ng / ml and suspicious findings at trans - rectal ultrasound ( trus )  . 
at mrsi , cancer was defined as possible if the ratio of choline plus creatine to citrate exceeded mean normal peripheral zone values by two standard deviations ( sd ) or as definite if that ratio exceeded the normal value by three sd . 
mri and mrsi alone had sensitivity , specificity , positive and negative predictive values and diagnostic accuracy in the detection of prostate cancer equal to 85% , 75% ; 53% , 89% ; 65% , 88% ; 77% , 74% ; and 69% , 79% , respectively . 
trentanove pazienti con valori di antigene specifico prostatico ( psa ) superiori a 4 ng / ml e reperti sospetti allecografia transrettale ( trus ) sono stati sottoposti ad imaging morfologico con risonanza magnetica ( rm ) e a rmsp . 
alla rmsp la presenza di tumore stata definita come possibile se il rapporto tra colina pi creatina su citrato era maggiore di 2 ds rispetto al valore medio della zona periferica normale o certa se tale rapporto superava di 3 ds quello normale . 
la rm e la rmsp singolarmente hanno evidenziato sensibilit , specificit , valore predittivo positivo e negativo e accuratezza diagnostica per lindividuazione del cancro prostatico del 85% , 75% e 53% , 89% e 65% , 88% e 77% , 74% e 69% , 79% rispettivamente . 
laggiunta della rmsp alla rm permette una significativa pi alta specificit nellindividuazione del tumore rispetto alla sola rm e pu essere indicata come modalit risolutiva prima della biopsia nei pazienti con elevati valori di psa ed ecografia transrettale ( trus ) sospetta . key words prostate prostatic neoplasm biopsy magnetic resonance imaging magnetic resonance spectroscopy imaging parole chiave prostata neoplasia prostatica biopsia risonanza magnetica spettroscopia con risonanza magnetica introduction introduzione the growing incidence of prostate cancer , together with an increasing ageing population in the western world , has made prostate tumour an acute medical and socioeconomic problein 2004 in the united states , the american cancer society estimated 230 , 000 new cases of prostate carcinoma as well as 29 , 900 cases of deaths related to this disease [ 1 ]  . screening with digital rectal examination associated with evaluation of serum prostate - specific antigen ( psa ) and trans - rectal ultrasound ( trus ) , possibly complemented by biopsy [ 2 ] , has enabled physicians to identify cancers at an earlier stage than in the past , drawing attention to the possibility of using treatments ( brachytherapy , radiotherapy , thermoablation and cryosurgery ) that have less aggressiveness and morbidity than radical prostatectomy . hence , locating and staging the cancer accurately as well as assessing its biological aggressiveness have become crucial . magnetic resonance imaging ( mri ) improves the evaluation of zonal morphology and prostate anatomy although there is still no agreement over diagnostic accuracy of mri in identifying prostate cancer lesions . studies conducted to date have shown extreme variations in accuracy levels , with values ranging from 75% to 90% , with peaks of 97% [ 3 ] in locating known lesions , but showing a remarkable drop with lesions < 5 mm [ 4 ]  . 
however , morphologic evaluation alone had poor specificity ( 55% ) [ 5 ] because of a high number of false positives . these can be attributed to several conditions ( post - biopsy haemorrhage , the effects of conservative treatments ) or diseases ( prostatitis ) affecting the prostate tissue , which can mimic cancer and its typical t2 appearance as an area of low signal intensity against a background of relatively hyperintense normal peripheral zone . 
the introduction of proton mr spectroscopic imaging ( mrsi ) has enabled direct correlation of anatomical and morphological findings with functional information on tissue metabolism . initial studies show the potential of combined mri and mrsi in determining the presence of prostate cancer with higher accuracy , view its extension and estimate its biological aggressiveness [ 6 ]  . 
therefore , the purpose of our study was to compare the diagnostic performance of mrsi and morphological imaging alone in the identification and localisation of prostate tumours by comparing it prospectively with histopathologic findings . materials and methods patients between april and october 2004 , 39 patients underwent , after giving informed consent , mri of the prostate with associated spectroscopic evaluation at our department . 
lamerican cancer society ha stimato negli stati uniti , nel 2004 , 230.000 nuovi casi di carcinoma prostatico e 29.900 casi di decesso ad esso correlati [ 1 ]  . 
lo screening con esplorazione digito - rettale associato alla valutazione dellantigene prostatico specifico ( psa ) sierico e allo studio con ecografia transrettale ( trus ) , eventualmente completato dalla biopsia [ 2 ] ha consentito lindividuazione delle neoplasie ad uno stadio pi precoce rispetto al passato , richiamando inoltre lattenzione sulla possibilit di utilizzare degli strumenti terapeutici ( brachiterapia , radioterapia , termoablazione e criochirurgia ) meno aggressivi e gravati da minore morbilit rispetto alla prostatectomia radicale . 
diviene in tal modo di fondamentale importanza la precisa localizzazione e stadiazione della neoplasia e la valutazione della sua aggressivit biologica . limaging con risonanza magnetica ( rm ) consente una migliore valutazione della morfologia e dellanatomia zonale della prostata sebbene riguardo al valore di accuratezza diagnostica della rm nellidentificazione delle lesioni prostatiche neoplastiche non vi sia ancora accordo tra i vari autori . 
gli studi finora effettuati hanno mostrato unampia variabilit dei risultati di accuratezza con valori che vanno dal 75% al 90% , raggiungendo il 97% [ 3 ] nella localizzazione di lesioni gi note , ma mostrando una sensibile flessione per lesioni di diametro inferiore ai 5 mm [ 4 ]  . 
la sola valutazione morfologica , per , si rilevata scarsamente specifica ( 55% ) [ 5 ] , a causa di un elevato numero di falsi positivi , i quali possono essere attribuiti alla presenza di alcune condizioni ( emorragia post - bioptica , effetti delle terapie conservative ) o patologie ( prostatiti ) che interessano il tessuto prostatico e che sono in grado di mimare la lesione neoplastica con il tipico aspetto di area a bassa intensit di segnale nelle sequenze t2 pesate nel contesto della relativa iperintensit della zona periferica normale . lintroduzione della spettroscopia dellidrogeno con rm ( rmsp ) ha permesso di correlare il dato anatomico e morfologico direttamente con informazioni di tipo funzionale relative al metabolismo tissutale . 
studi iniziali mostrano la potenzialit della combinazione del rm e rmsp nel determinare in maniera pi accurata la presenza del carcinoma prostatico , visualizzarne lestensione e stimarne laggressivit biologica [ 6 ]  . 
lo scopo del nostro studio stato , pertanto , verificare la performance diagnostica della spettroscopia dellidrogeno rispetto al solo imaging morfologico nella individuazione e localizzazione della patologia tumorale prostatica , confrontandola prospetticamente con il dato istopatologico . materiali e metodi pazienti da aprile ad ottobre 2004 , 39 pazienti si sono recati presso il nostro dipartimento per essere sottoposti , previo consenso g . 
for the morphological study , t2 - weighted turbo spin echo ( tse ) images with high spatial resolution were acquired in the transverse plane ( using the spir fat - suppression technique as well ) and in the coronal plane , including the entire prostate and seminal vesicles in the acquisition volume . 
acquisition parameters were the following : tr 4 , 000 ms , te 130 ms ( tr 4 , 750 ms , te 90 ms in the spir sequence ) , 2.5 - mm slice thickness without gap between the slices , four excitations , 190 mm field of view ( fov ) and acquisition and reconstruction matrices of 240 and 256 , respectively . the morphological study was completed with the acquisition of ten t1 - weighted fast - field echo ( ffe ) spir post - contrast dynamic sequences ( tr 20 ms , te 5 m , 20 flip angle , 3 - mm slice thickness )  . the volume to be studied by spectroscopy was selected on the basis of the axial t2 morphological images , trying to include the prostate parenchyma and exclude as much periglandular fat as possible . 
to this end , a double spin - echo point - resolved spatially localized spectroscopic ( press ) sequence was used , along with a te ( 136 ms ) optimised for quantitative evaluation of citrate and choline with multivoxel analysis . 
let media dei pazienti esaminati di 68 , 5 aa ( range 5582 anni ) con un valore medio di psa sierico di 24 , 15 ng / ml ( range 4 , 344 ng / ml )  . tecnica rm le immagini sono state acquisite con unapparecchiatura ad elevata intensit di campo ( 1 , 5 t ) ( philips gyroscan intera , best , netherlands ) equipaggiata con gradienti da 30 mt / m , utilizzando la bobina del corpo per la trasmissione degli impulsi e una bobina di superficie ( c1 ) , posizionata a livello della pelvi , per la ricezione del segnale . 
allo scopo di ridurre la motilit intestinale e migliorare cos la qualit delle immagini sono stati somministrati per via i.glucagone o nbutilbromuro di ioscina ( buscopan fl 20 mg / ml )  . 
per lo studio morfologico sono state acquisite immagini tse t2 pesate ad alta risoluzione spaziale sul piano trasversale ( utilizzando anche la tecnica della soppressione del grasso spir ) e su quello coronale includendo nel volume dacquisizione lintera prostata e le vescicole seminali . 
i parametri di acquisizione sono stati i seguenti : tr 4000 ms , te 130 ms ( tr 4750 ms , te 90 ms nella sequenza spir ) , spessore di sezione 2 , 5 mm senza intervallo tra le sezioni , 4 eccitazioni , fov di 190 mm e una matrice di acquisizione e di ricostruzione rispettivamente di 240 e 256 . 
lo studio morfologico stato completato con lacquisizione di 10 sequenze dinamiche post - contrastografiche ffe t1w spir ( tr 20 msec , te 5 msec , flip angle 20 , spessore di sezione 3 mm )  . il volume sottoposto ad analisi spettroscopica stato selezionato , sulla base delle immagini assiali t2 morfologiche , cercando di includere il parenchima prostatico e di escludere il pi possibile il grasso perighiandolare . 
a tal fine stata utilizzata una sequenza press ( double spin - echo point - resolved spatially localized spectroscopic sequence ) con un te ( 136 ms ) ottimizzato per la valutazione quantitativa del citrato e della colina con analisi multivoxel . 
sono stati utilizzati i seguenti parametri di acquisizione : tr 1.600 ms , te 136 ms , ampiezza spettrale 1.000 hz , con risoluzione spettrale nominale del voxel di 0 , 24 cm3 . 
il tempo di acquisizione della sequenza spettroscopica stato di 18 minuti . le sequenze post - contrastografiche sono state utilizzate nella valutazione di rapidi potenziamenti di segnale , in particolare della porzione periferica della ghiandola , sincroni con la normale omogeneizzazione della porzione adenomiomatosa , suggestivi di lesione produttiva con neoangiogenesi anarchica nel contesto . image analysis was carried out by an experienced radiologist ( es ) in mri of abdominal - pelvic structures . 
1a - d dynamic t1 - weighted fast - field ( ffe ) sequence : the acquisitions at time 0 ( a ) and 20 s after contrast medium infusion ( b ) show a focal early wash - in ( arrow ) in the middle - left peripheral portion . 
acquisizione a 20 s dalla somministrazione del mezzo di contrasto che evidenzia precoce wash - in focale ( freccia ) a carico della porzione periferica paramediana sinistra ( b )  . 
presence of a rounded homogeneously hypointense area esperto ( es ) nellimaging rm delle strutture addomino - pelviche il quale era a conoscenza del fatto che i pazienti avevano lesioni sospette per neoplasia alla trus . 
i confini della zona periferica sono stati definiti grazie alla visualizzazione delle bande di bassa intensit di segnale nelle immagini t2 dipendenti riferibili alla capsula e alla pseudocapsula prostatica [ 7 ]  . 
by using dedicated software for spectroscopic analysis , values of the integral of the areas underlying citrate , choline and creatine peaks were calculated . to detect the presence of cancer , the ratio between the integral of choline plus creatine and the integral of citrate was calculated for each voxel . 
la presenza di unarea omogeneamente ipointensa a margini rotondeggianti e limiti sfumati stata considerata come sospetta per neoplasia . i singoli voxel del volume selezionato nella sequenza spettroscopica sono stati rappresentati bidimensionalmente in forma grafica di griglia sovrapposta alle corrispondenti immagini traverse t2 pesate . 
in tutti i pazienti sono stati effettuati 10 prelievi secondo suddivisione in ottanti della prostata ( 1 prelievo per apice , zona intermedia , basale e 2 per la zona laterale per ciascun lato )  . almeno 2 campionamenti sono stati ottenuti dalle zone che presentavano caratteristiche patologiche alla rm ed alla rmsp . 
in all patients , ten samples were taken according to the subdivision of the prostate into octants ( one sample from the apical , intermediate and basal areas and two samples for the lateral area on each side )  . at least two samples were taken from the areas that presented pathological features at mri and mrsi . 
samples were classified based on the sampling site , and histological analysis was carried out for each site . every biopsy sample was analysed by a single pathologist specialized in prostatic diseases . statistical analysis findings were processed with the statistical package for social sciences , version 12 ( spss , chicago , il , usa )  . 
results obtained with mri and mrsi used separately and in combination and with biopsy were analysed in terms of sensitivity , specificity , positive ( ppv ) and negative predictive value ( npv ) and accuracy values . statistically significant differences in the comparison between mri and mrsi and mri and mrsi combined versus biopsy were processed through an c2 test according to pearson , assuming a value of p0.05 , to indicate a significant correlation . 
although images had been classified as normal , equivocal or suspicious for cancer , in the statistical analysis , results were divided into two groups only : positive ( suspicious and equivocal , > 3 sd and < 23 sd > ) and negative ( normal and < 2 sd )  . results findings of the dynamic post - contrast acquisitions were not used in statistical evaluation of the selected sample . 
twentysix out of 39 patients ( 66% ) showed focal and / or unilateral or bilateral signal hypointensity in the t2 - weighted images whereas the remaining 13 ( 33% ) showed no pathological signal alterations . 
in particular , as regards location within the gland , mri detected five suspicious areas at the apical level ( three on the right , two on the left ) , eight at the intermediate level ( three on the right , five on the left ) , nine at the lateral level ( five on the right , four on the left ) and four at a basal level ( two on the right , two on the left )  . of the 26 patients in whom mri was suggestive of a neoplastic lesion , histology confirmed adenocarcinoma in 17 [ 65% true positive ( tp ) ] but diagnosed benign lesions in nine [ 35% false positive ( fp ) ]  . 
ciascun campione bioptico stato analizzato da un unico anatomo - patologo specialista nella patologia prostatica . analisi statistica i dati sono stati elaborati utilizzando lo statistical package for social sciences , versione 12 ( spss , chicago , illinois )  . 
i risultati ottenuti rispettivamente dalla rm , dalla rmsp , dalla combinazione rm - rmsp e dalla biopsia sono stati tabulati calcolando i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) ed accuratezza . i valori di significativit statistica nel confronto tra i risultati della rm e della rmsp e della combinazione rm - rmsp rispetto alla biopsia sono stati elaborati mediante test c2 secondo pearson , assumendo un valore di p0 , 05 indicante una correlazione significativa . sebbene le immagini fossero state classificate come normali , equivoche o sospette per neoplasia , ai fini dellanalisi statistica i risultati sono stati suddivisi in due soli gruppi ovvero positivi ( sospetti ed equivoci , > 3 ds e < 23 ds > ) e negativi ( normali , < 2 ds )  . risultati i dati relativi alle acquisizioni dinamico - contrastografiche non sono stati utilizzati nella valutazione statistica del campione selezionato . ventisei pazienti dei 39 totali ( 66% ) presentavano ipointensit di segnale di tipo focale e / o diffusa mono o bilateralmente nelle immagini t2 dipendenti , mentre i rimanenti 13 ( 33% ) non mostravano alterazioni di segnale di carattere patologico . in particolare , in riferimento alla localizzazione a livello della ghiandola , con la rm sono state attribuite 5 aree sospette a livello dellapice ( 3 a destra , 2 a sinistra ) , 8 in regione intermedia ( 3 a destra , 5 a sinistra ) , 9 in sede laterale ( 5 a destra , 4 a sinistra ) e 4 in regione basale ( 2 a destra , 2 a sinistra )  . dei 26 pazienti con rm suggestiva per lesione discariocinetica , 17 ( 65% vp ) hanno trovato conferma istologica di adenocarcinoma , mentre 9 ( 35% fp ) hanno avuto diagnosi di lesione benigna , in 5 casi di natura flogistica ( prostatiti acute o croniche ) nei rimanenti 4 di iperplasia nodulare benigna . 
of the 13 patients without suspicious findings for cancer , histology confirmed the absence of neoplastic lesions in ten [ 77% true negative ( tn ) : seven cases of benign nodular hyperplasia and three of granulomatous prostatitis ] but detected adenocarcinoma in 3three [ 23% false negative ( fn ) ] ( table 1 )  . based on these results , mri had a 85% sensitivity , 53% specificity , with 65% ppv and 77% npv and 69% accuracy with a p = 0.013 ( table 2 )  . 
mrsi identified pathological spectra ( cho + cr / cit ratio > 3 sd or < 23 sd > ) in 17 patients ( 43% ) whereas spectrum analysis was normal ( cho + cr / cit ratio < 2 sd ) in the remaining 22 ( 57% )  . 
la rmsp ha individuato spettri di tipo patologico ( rapporto cho + cr / cit > 3 ds o < 23 ds > ) in 17 pazienti ( 43% ) , mentre nei restanti 22 ( 57% ) lanalisi spettrale risultata nei limiti della normalit ( rapporto cho + cr / cit < 2 ds )  . 
in base alla suddivisione in ottanti 2 erano le aree sospette a livello dellapice prostatico , 7 in regione intermedia ( 3 a destra , 4 a sinistra ) , 7 in sede laterale ( 4 a destra , 3 a sinistra ) 1 in regione basale destra . 
la rmsp ha dimostrato una sensibilit del 75% con specificit del 89% , un vpp del 88% , un vpn del 74% con unaccuratezza del 87% con un valore di p = 0 , 000 ( tabella 2 )  . combinando i risultati della rm con quelli della rmsp abbiamo avuto una sensibilit del 70% con una specificit del 89% , vpp 88% , vpn 74% , unaccuratezza del 79% e un valore di p = 0 , 000 ( tabella 2 )  . riguardo alla localizzazione delle lesioni non si evidenziata una significativa correlazione tra i risultati ottenuti ai prelievi bioptici e quelli evidenziati alla rm e alla rmsp , se non per quanto riguarda i risultati dellistologia e della rmsp nella zona intermedia e laterale ( p = 0 , 003 e p = 0 , 002 rispettivamente )  . table 1 correlation of magnetic resonance imaging ( mri ) , mr spectroscopic imaging ( mrsi ) and biopsy findings tabella 1 correlazione tra rm , rmsp e reperti bioptici biopsy findings mrsi risultati biopsia rmsp negative positive negative positive negativi positivi negativi positivi negative positive total negativi positivi totale table 2 sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) , and accuracy of magnetic resonance imaging ( mri ) , mr spectroscopic imaging ( mrsi ) and combined mri / mrsi tabella 2 sensibilit , specificit , vpp , vpn , accuratezza della rm , rmsp e rm / rmsp combinate mri , % mrsi , % mri / mrsi , % rm , % rmsp , % rm / rmsp , % sensibilit specificit accuratezza sensitivity specificity accuracy g . 
3a - d ipointensit focale nelle immagini assiali t2pesate nella zona periferica in sede mediana sinistra . lo spettro ottenuto dallarea di alterata intensit di segnale ha evidenziato unelevazione della colina e una riduzione del citrato compatibile con la presenza di cancro ( d )  . 
4a - d diffusa alterata intensit di segnale nella zona periferica a destra nelle immagini t2 - pesate ( piano assiale , a e c e piano coronale , b )  . 
in contrast , our study aimed at assessing the ability of mri and mrsi to identify and localise prostate cancer by prospectively correlating findings of single techniques with biopsy results . the decision to use a surface coil was dictated by the need to obviate the poor tolerability of the examination carried out with an intracavitary coil and to improve the quality of images corrupted by specific artefacts of endorectal coils ( coil flare , straight line , glandular distortion ) [ 18 ]  . as regards the morphological evaluation alone , mri had 85% sensitivity and 53% specificity in the detection of lesions values in line with those reported in the literature . il carcinoma prostatico rappresenta a tuttoggi unimportante causa di morte per cancro nella popolazione maschile [ 1 ]  . 
di contro a questa rilevante mortalit , ci sono molti casi di tumore a decorso subclinico rilevati casualmente al solo esame autoptico [ 9 ]  . le tecniche diagnostiche non invasive correntemente disponibili presentano delle forti limitazioni nel discriminare forme latenti da forme aggressive e progressive [ 10 , 11 ]  . la trus ha dimostrato di non essere in grado di individuare fino al 30% delle lesioni palpabili allesplorazione rettale e di avere unelevata percentuale di falsi positivi in quanto solo il 20% delle lesioni ipoecogene ( principale caratteristica ecografia di malignit ) sono realmente maligne [ 12 ] ; la biopsia ecoguidata inoltre presenta unelevata percentuale di errori nel campionamento per il fatto che solo una piccola parte della ghiandola prostatica viene effettivamente analizzata cosicch molti pazienti che presentano valori di psa alterati ( > 4 ng / ml ) e che sono sottoposti ad un campionamento sistematico lungo i sestanti prostatici hanno esito negativo allesame bioptico e sono candidati ad un ulteriore prelievo [ 13 , 14 ]  . con lemergere di nuove strategie terapeutiche meno invasive rispetto alla prostatectomia radicale , si sente , inoltre , maggiormente lesigenza di una precisa localizzazione e valutazione dellestensione della malattia , per eseguire una terapia mirata che incrementi lefficacia del trattamento , riducendone la morbilit . 
le esperienze sinora pubblicate , aggiungendo al dato morfologico quello metabolico mediante limaging spettroscopico 3d , evidenziano un miglioramento nellindividuazione della neoplasia e nella definizione della stadiazione , volume e grado di aggressivit [ 8 , 16 , 17 ]  . 
 la maggior parte dei dati in letteratura deriva per da studi di tipo retrospettivo , in cui laccuratezza diagnostica della rm e della rmsp stata valutata facendo riferimento al dato istopatologico ottenuto dopo prostatectomia radicale . 
nel nostro studio abbiamo voluto invece valutare la capacit della rm e della rmsp nellindividuazione e localizzazione del tumore prostatico , correlando prospetticamente i risultati ottenuti dalle singole tecniche con quelli bioptici . la scelta di utilizzare una bobina di superficie si imposta per ovviare alla scarsa tollerabilit dellesame eseguito con bobina endocavitaria e per migliorare la qualit dellimmagine corrotta da artefatti specifici delle bobine endorettali ( coil flar , straight line , distorsione ghiandolare ) [ 18 ]  . per quanto riguarda la sola valutazione morfologica la rm ha mostrato , nellidentificazione delle lesioni , una sensibilit del 85% e una specificit del 53% , valori questi sostanzialmente sovrapponibili a quelli riportati in letteratura . la rmsp , con laggiunta del dato metabolico ha mostrato mrsi , with the addition of metabolic data , proved to be significantly more specific in identifying tumours as compared with mri alone ( 89% versus 53% )  . 
a positive result at mri and mrsi indicates the likely presence of cancer ( ppv 88% ) whereas a negative result excludes it with a slightly lower likelihood ( npv 77% )  . 
presumably , this is affected by the number of false negatives , which are likely due to limitations of the current multivoxel technology , with a nominal voxel value that is still high ( 0.24 cm3 ) , and is typical of 1.5t magnetic fields , with a possible summation of the tumour 's metabolic findings with those of surrounding healthy tissue in the sampled volume . 
another possible explanation of the failed identification of tumour lesions by mrsi may be the low biological aggressiveness of some cancers . some authors [ 19 ] have already reported that small , lowgrade tumours ( gleason scores 4 and 5 ) may be missed owing to slight alterations of citrate and choline . 
il valore nominale del voxel infatti ancora elevato ( 0 , 24 cm3 ) , caratteristico per campi magnetici di 1 , 5t , e ci potrebbe determinare un effetto di sommazione del dato metabolico tumorale con quello del tessuto sano circostante nel volume campionato . unaltra possibile spiegazione della non avvenuta identificazione delle lesioni tumorali da parte la rmsp pu essere correlata alla scarsa aggressivit biologica di alcune neoplasie . infatti , gi stato riportato da alcuni autori [ 19 ] come piccoli tumori a basso grado ( gleason 4 e 5 ) possono non essere rilevati per le lievi alterazioni del citrato e della colina . 
iniziali studi clinici , che vedono lapplicazione di campi magnetici ad alta intensit ( 3t ) , dimostrano come sia possibile aumentare sensibilmente la risoluzione spettrale , con un sostanziale incremento di accuratezza nellidentificazione spaziale del dato metabolico [ 20 ]  . la scarsa correlazione complessiva tra i risultati della rm e della rmsp e quelli istopatologici , riguardo la localizzazione spaziale delle lesioni , fa s che il nostro studio non sia in grado di rispondere alla domanda se la localizzazione del tumore prostatico influenzi la capacit delle due tecniche di rilevare il tumore stesso . 
in realt , per lintrinseca difficolt della biopsia ecoguidata di garantire una precisa corrispondenza tra il sito del prelievo e le aree sospette alla rm e alla rmsp , solo lanalisi istologica dopo prostatectomia radicale in grado di rispondere realmente a tale quesito . conclusions conclusioni although ours was a preliminary study carried out on a small sample of patients and larger series are needed to confirm our findings , we can reasonably conclude that the combination of mri and mrsi also considering the greater tolerability of an examination that avoids the use of endorectal coils may be indicated as a problem - solving modality for two categories of patients : those whose high serum psa and suspicious trus finding , which make them candidates for biopsy ; and those who have already undergone multiple biopsies , all with a negative outcome but persistent serum psa alterations , and are therefore candidates for further biopsy . 
identification of suspicious areas on mri and mrsi also provides the possibility of performing targeted biopsies of those areas , under direct mri guidance , and to remove the error inherent in correlating mri with trus findings [ 21 ]  . in conclusione , sebbene il nostro sia certamente uno studio iniziale , realizzato su di una piccola popolazione campione e che siano necessarie pi ampie serie di pazienti per confermare quanto da noi evidenziato , ragionevole ritenere che lassociazione rm / rmsp , anche in relazione alla maggiore tollerabilit di un esame che evita lutilizzo della bobina endorettale , possa essere indicata come modalit problem - solving in quei pazienti che , con elevati valori di psa sierico e trus sospetta per lesione neoplastica , sono candidati al prelievo bioptico oppure in coloro che , gi sottoposti a biopsie multiple con esito negativo , per il persistere delle alterazioni sieriche del psa , rientrano in una zona di incertezza e sono candidati ad unulteriore biopsia . 
cova1 1unit clinica operativa di radiologia , universit degli studi , ospedale di cattinara , strada di fiume , 447 , i - 34149 trieste , italy 2unit clinica operativa di neurologia , universit degli studi , ospedale di cattinara , trieste , italy 3brain center for neuroscience , trieste , italy 4dipartimento di fisica , universit degli studi di trieste , italy correspondence to : m . 
sono stati studiati 7 pazienti ( 6 di sesso maschile e 1 di sesso femminile ) affetti da una forma di morbo di parkinson lateralizzata acinetico - rigida , sottoposti ad un esame di risonanza magnetica funzionale . 
inoltre , stata riscontrata in alcuni casi lassenza di attivazione a livello delle aree premotoria e supplementare motoria ; quando invece presente , lattivazione era caratterizzata da intensit superiore durante il movimento della mano sana . 
le alterazioni osservate riflettono verosimilmente una riorganizzazione corticale secondaria al deficit sottocorticale allorigine della malattia . parole chiave risonanza magnetica risonanza magnetica funzionale encefalo morbo di parkinson introduction introduzione parkinsons disease is a neurological disorder characterised by progressive loss of dopaminergic neurons from the subcortical circuit of the basal nuclei , which presents clinically with four cardinal signs : tremor at rest , bradykinesia , rigidity and postural instability . 
the prevalence of the disease is approximately 120180 cases in 100 , 000 individuals per il morbo di parkinson un disordine neurologico caratterizzato da una progressiva perdita di neuroni dopaminergici del circuito sottocorticale dei nuclei della base e si manifesta clinicamente con quattro segni cardinali : tremore a riposo , bradicinesia , rigidit ed instabilit posturale . 
the diagnosis is mainly clinical although morphologicalfunctional brain imaging , with both radiological and nuclear medicine techniques , may be of particular assistance despite the lack of specificity and the variability of imaging signs . although the disease has always been considered to affect subcortical ganglia , the effects of dopamine depletion are widespread and also involve non - dopaminergic neurons in areas of the brain crucial for motor control . only a few published reports have investigated functional magnetic resonance imaging ( mri ) in the assessment of cortical activation in patients with parkinsons disease . 
in particular , the studies focused on cortical activation during simple motor tasks , prevalently evaluating the primary sensory - motor area , the supplementary motor area and the pre - motor area , with only limited information on parietal lobes . 
this study aimed to assess cortical activation patterns with functional mri in patients with lateralised parkinsons disease during a relatively complex motor task in order to better understand pathophysiological mechanisms of the disease and detect possible clinical effects of functional mri on these subjects . materials and methods this study assessed two groups of subjects : the first included 11 healthy volunteers ( six men and five women ) aged between 23 and 37 with no neurological disease ; the second consisted of seven patients ( six men and one woman ) aged between 56 and 82 years with parkinsons disease . 
 patients were receiving a mean l - dopa dose of 42064.54 mg / day , and none of them was taking dopamine agonists : all were continuing their normal work activities . both the healthy volunteers and patients received adequate information about the functional study , which they underwent only after giving their consent . 
volunteers were univocally identified by a number : numbers from 1 to 7 identified lanno nella popolazione caucasica [ 1 ] , ma considerando la prevalenza nei soggetti di oltre 65 anni di et si arriva all1% e al 2% oltre gli 80 anni . leziologia multifattoriale , in particolare correlata sia a fattori genetici che ambientali . 
la diagnosi principalmente clinica , anche se le metodiche di imaging cerebrale morfo - funzionale , sia radiologiche che di medicina nucleare , possono fornire un notevole ausilio nonostante lestrema aspecificit ed incostanza dei segni riscontrabili . 
nonostante tale patologia sia sempre stata considerata di pertinenza ganglionare , nettamente sottocorticale , gli effetti della perdita di dopamina sono diffusi e coinvolgono anche i neuroni non - dopaminergici in regioni encefaliche che costituiscono elementi cruciali per il controllo motorio . 
in letteratura sono stati pubblicati pochi lavori riguardanti lattivazione corticale valutata con risonanza ( rm ) funzionale in pazienti affetti da morbo di parkinson . in particolare , in questi studi stata posta lattenzione sullattivazione corticale durante lesecuzione di compiti motori semplici , valutando prevalentemente larea sensitivo - motoria primaria , larea supplementare motoria e larea premotoria , con solo pochi dati riguardanti i lobi parietali . con questo studio abbiamo voluto valutare i pattern di attivazione corticale in rm funzionale in soggetti affetti da morbo di parkinson lateralizzato durante lo svolgimento di un compito motorio relativamente complesso con lobiettivo di comprendere meglio i meccanismi fisiopatologici di tale malattia ed in secondo luogo di ricavare una possibile ricaduta clinica della rm funzionale in questi soggetti . materiali e metodi in questo studio sono stati valutati due gruppi di soggetti : il primo comprendeva 11 volontari sani ( 6 maschi e 5 femmine ) di et compresa tra i 23 ed i 37 anni , non affetti da patologie neurologiche , mentre il secondo gruppo comprendeva sette pazienti ( 6 maschi e 1 femmina ) di et compresa tra i 56 e gli 82 anni , affetti da morbo di parkinson . 
tutti i pazienti presentavano una sindrome ad esordio asimmetrico , acinetico - rigida , ipertonica , atremorigena cui si associava una bradicinesia importante ed ipomimia : il tempo medio di diagnosi di malattia di parkinson era di 12 , 82 , 37 mesi . nella tabella 1 sono riportate le caratteristiche di lateralizzazione riscontrate clinicamente per ciascun paziente . 
i pazienti assumevano una quantit di l - dopa media di 42064 , 54 mg / die e nessuno era in terapia con farmaci dotable 1 lateralisation detected clinically in each patient with parkinsons disease tabella 1 lateralizzazione riscontrata clinicamente in ciascun paziente affetto da morbo di parkinson patient lateralisation paziente lateralizzazione right left right right left right left destra sinistra destra destra sinistra destra sinistra m . 
lattivazione viene espressa in variazione percentuale del contrasto bold tra fase di attivazione e di riposo soggetto no . mano destra mano sinistra m1 omolaterale m1 controlaterale m1 omolaterale m1 controlaterale the healthy volunteers who performed the motor task with both hands , volunteers 810 performed it with their right hand only whereas volunteer 11 performed it with the left hand only . 
likewise , parkinsons disease patients were identified by a progressive number from 1 to 7 , and all performed the motor task with both hands . the examinations were conducted on a standard clinical mri unit with a 1.5 - t intera master super - conductive magnet ( philips , gyroscan intera 1.5 t master , best , the netherlands )  . 
an echo planar fast field echo ( ffe ) sequence ( tr / te : 3 , 200 / 45 ms , slice thickness 4 mm , gap 0 , fov 200 mm , matrix 64x64 ) was used for functional acquisition , with evaluation of cortical activation exploiting the blood oxygen level dependent ( bold ) contrast . finger tapping was selected as the activation test : in this test , the subject is asked to tap the thumb on the pulp of each of the other fingers in turn , and then start over again particular , during the whole sequence , made up of 150 trs lasting a total of 8 min , the subject was asked to alternate a phase of rest and a phase of activity for three consecutive times with the same hand . 
in particular , we chose an inversion recovery sequence ( tr / te / ti : 1 , 786 / 15 / 350 ) characterised by fov , slice thickness and gaps similar to those used for the functional sepaminoagonisti : tutti continuavano la loro normale attivit lavorativa . 
i volontari sono stati individuati univocamente da un numero : i numeri da 1 a 7 individuano i volontari sani che hanno eseguito il compito motorio con entrambe le mani , i volontari 8 , 9 , 10 con la sola mano destra mentre il volontario 11 con la sola mano sinistra . 
 gli esami sono stati condotti su un tomografo clinico standard dotato di un magnete superconduttivo da 1 , 5 t ( philips , gyroscan intera 1 , 5 t master , best , olanda )  . 
per lacquisizione funzionale stata utilizzata una sequenza echo planar ffe ( tr / te : 3200 / 45 ms , spessore di strato = 4 mm , gap = 0 , fov = 200 mm , matrice 64x64 ) , con valutazione dellattivazione corticale sfruttando il contrasto bold ( blood oxygen level dependent )  . 
per quanto riguarda la prova di attivazione stato scelto il finger tapping : cio stato chiesto al soggetto di toccare con il polpastrello del primo dito , in successione , il polpastrello del secondo , terzo , quarto e quinto dito e , quindi , ricominciare da capo . 
activation is expressed as a percentage change of the blood oxygen level dependent ( bold ) contrast between activity and rest phases tabella 3 risultati relativi allattivazione dellarea motoria supplementare e dellarea premotoria nei volontari sani : confronto tra movimento della mano destra e sinistra . 
activation is expressed as a percentage change of the blood oxygen level dependent ( bold ) contrast between activity and rest phases subject no . affected hand healthy hand m1 ipsilateral m1 contralateral m1 ipsilateral m1 contralateral tabella 5 risultati relativi allattivazione dellarea motoria primaria ( m1 ) nei pazienti parkinsoniani : confronto tra movimento della mano sana e della mano malata . 
a p value of 0.01 was considered to indicate statistical significance . in all subjects , the presence or absence of activation was evaluated at the level of the primary motor area , the pre - motor area and supplementary motor area of the parietal and occipital lobes . 
each area was studied as a cluster if voxels were contiguous and made the structure identifiable or as a spherical volume if the voxels were separate but could be related to the same brodmann area . 
graphically , pixels corresponding to cortical activation were overlaid onto the anatomic sequence to enable more accurate localisation . results tables 2 , 3 and 4 show numerical results for each healthy volunteer and each area . 
in all patients considered , we observed activation of the primary motor area contralateral la durata complessiva di 8 minuti , stato chiesto al soggetto di alternare una fase di riposo ad una fase di attivit e questo per tre volte consecutive con la stessa mano . 
successivamente stata acquisita una sequenza anatomica , in particolare abbiamo scelto una sequenza inversion recovery ( tr / te / ti = 1786 / 15 / 350 ) caratterizzata da fov , spessore di strato e gap analoghi a quelli utilizzati per la sequenza funzionale . 
in tutti i soggetti stata valutata la presenza o assenza di attivazione in corrispondenza dellarea motoria primaria , dellarea premotoria e supplementare motoria , dei lobi parietali e dei lobi occipitali . 
ciascuna area stata studiata come cluster , se i voxels erano contigui e dunque rendevano individuabile la struttura , oppure come volume sferico , se i voxels erano separati , ma riconducibili alla stessa area di brodmann . 
da un punto di vista grafico i pixels relativi allattivazione corticale sono stati sovrapposti alla sequenza anatomica , di modo da consentire una loro pi corretta localizzazione . risultati nelle tabelle 2 , 3 e 4 sono riportati i risultati numerici relam . 
intensity of the activation signal was higher , on average , in the primary motor area contralateral to the moving hand , as compared with the ipsilateral primary motor area . 
signal intensity of the primary ipsilateral and contralateral motor areas was higher during movement of the affected hand as compared with the healthy tivi a ciascun volontario sano e ciascuna area . 
accanto a queste attivazioni stata rilevata unattivazione a livello dellarea motoria omolaterale e a livello dei lobi parietali . nelle tabelle 5 , 6 e 7 sono riportati i risultati relativi ai pazienti parkinsoniani . 
in tutti i pazienti studiati stata osservata la presenza di attivazione in corrispondenza dellarea motoria primaria controlateralmente al lato in esame e in 6 pazienti su 7 lattivazione delle aree motoria supplementare e premotoria . table 6 results concerning activation of the supplementary motor area and pre - motor area in parkinsons patients : comparison between movement of the healthy hand and affected hand . 
activation is expressed as a percentage change of the blood oxygen level dependent ( bold ) contrast between activity and rest phases tabella 6 risultati relativi allattivazione dellarea motoria supplementare e dellarea premotoria nei pazienti parkinsoniani : confronto tra movimento della mano sana e della mano malata . 
activation of the supplementary motor and pre - motor areas was observed in six patients out of seven during movement of the healthy hand and in five patients out of seven during movement of the affected hand . 
in the remaining two cases , activation of the parietal cortex ipsilateral to the moving hand and activation of the parietal cortex were observed , respectively , bilaterally when the task was performed with the healthy hand , and contralateral when performed with the affected hand . 
the disease has always been regarded as gangliar and subcortical , but , despite the neurochemical lesion being mainly located in the nigrostriatal dopaminergic system , the effects of dopamine depletion are widespread and also affect neuronal pathways that are not strictly dopaminergic but more like bridges to areas of the brain crucial for motor control [ 3 ]  . 
with this study , we aimed at evaluating cortical acaccanto a queste attivazioni stata rilevata unattivazione a livello dellarea motoria omolaterale al movimento , della corteccia parietale e della corteccia occipitale . il segnale proveniente dallarea motoria primaria omolaterale stato osservato in 5 pazienti su 7 durante il movimento della mano sana e in 6 pazienti su 7 durante il movimento della mano malata : lintensit del segnale di attivazione mediamente maggiore in corrispondenza dellarea motoria primaria controlaterale alla mano in movimento rispetto allarea motoria primaria omolaterale . 
nei restanti due casi stata osservata rispettivamente unattivazione della corteccia parietale omolaterale alla mano in movimento e lattivazione della corteccia parietale bilateralmente quando il compito stato svolto con la mano sana e controlateralmente se stato svolto con la mano malata . 
tale affezione sempre stata considerata di pertinenza ganglionare , nettamente sottocorticale ma , anche se la lesione neurochimica localizzata prevalentemente a livello del sistema dopaminergico nigrostriatale , gli effetti della perdita di dopamina sono diffusi e coinvolgono vie neuronali anche non strettamente dopaminergiche , trait - dunion con regioni encefaliche cruciali per il controllo motorio [ 3 ]  . 
con questo studio , pertanto , abbiamo voluto valutare le caratteristiche dellattivazione corticale in soggetti affetti da morbo di parkinson durante lo svolgimento di un compito motorio relativamente complesso , confrontandole con quelle osservate in un gruppo di controllo costituito da volontari sani e , avendo i pazienti un morbo di parkinson lateralizzato , stato possibile effettuare un confronto tra le attivazioni ottenute con la mano sana e quella malata . in condizioni normali , con il semplice finger tapping , si osserva lattivazione della corteccia pree post - rolandica controlaterale , legate , la prima al movimento della mano , la seconda principalmente al contatto intrinseco interfalangeo . spesso si riconosce inoltre lattivazione in sede frontale delle aree supplementare motoria e premotoria : generalmente lattivazione dellarea motoria supplementare si distingue in una parte anteriore bilaterale simmetrica ed una posteriore , controlateralmente alla mano che esegue il compito motorio fig . 
2 marcata attivazione bilaterale della corteccia parietale durante il movimento della mano malata . tivation characteristics in patients with parkinsons disease during a relatively complex motor task , comparing them with those observed in a control group consisting of healthy volunteers . 
under normal conditions , simple finger tapping activates the preand post - rolandic contralateral cortex , the former being linked to hand movement , the latter mainly to intrinsic contact between phalanges . 
furthermore , frontal activation of the supplementary motor and pre - motor areas is often detected : activation of the supplementary motor area is generally subdivided into a symmetrical , bilateral , anterior portion and a posterior portion , contralateral to the hand performing the motor task [ 4 ]  . 
in healthy volunteers , the expected activation pattern was confirmed , but other areas were also activated , in particular , the ipsilateral primary motor cortex and the parietal cortex . activation corresponding to the primary motor cortex ipsilateral to the moving hand is neurologically justified by the partial hemilateral non - specificity of motor operations . 
when the task becomes slightly more complex and sequential , as with finger tapping , the ipsilateral primary motor cortex and parietal lobes , which are involved in the perception of movement in space , are also activated [ 6 ]  . before evaluating the results obtained in parkinsons patients , it should be noted that any differences between patients and healthy volunteers might be related not only to the disease but also to age . 
in this respect , it is important to note that the healthy volunteers age range was 2337 years whereas patients age range was 5682 years and that there were no functional mri investigations of brain activation induced by finger tapping performed under the same conditions by healthy subjects of different ages . 
nonetheless , the only published study contrasting the extent of activation of primary motor areas during a motor task , as assessed by spectroscopy in subjects of different ages , showed no statistically significant difference in activation among the different age groups [ 7 ]  . 
this hyperactivity of the contralateral primary motor area has already been described in the literature [ 8 , 9 ] and could represent the neural substrate for the difficulty experienced by the patient with parkinsons disease to perform the movement . 
it could therefore be assumed that this hyperactivity reflects the cortical re - organisation , which compensates for the subcortical deficit causing the disease . activation of the primary motor cortex ipsilateral to the hand examined has been also observed in parkinsons patients , but [ 4 ]  . 
nei volontari sani stato confermato il pattern di attivazione atteso , ma stata rilevata unattivazione a livello di altre aree , in particolare a livello della corteccia motoria primaria ipsilaterale e della corteccia parietale . la presenza di attivazione in corrispondenza della corteccia motoria primaria omolaterale alla mano in movimento giustificata , neurologicamente , dalla parziale aspecificit emilaterale delle operazioni motorie : infatti , a ciascuna mano sono affidate differenti abilit e le istruzioni per eseguire un determinato movimento possono in parte risiedere nelluno o nellaltro emisfero ed essere richiamate con la stessa modalit che implica lattivazione dellarea motoria supplementare . 
ovviamente , essendo ridotto il feed - back tattile , il segnale omolaterale riguarda la sola area rolandica deputata al controllo del movimento [ 5 ]  . altra ipotesi per spiegare tale attivazione legata al tipo di compito motorio : nel caso di un movimento molto semplice ( ad es . , apertura e chiusura della mano ) si osserva generalmente lattivazione della sola area motoria primaria controlaterale . 
quando il compito diviene modestamente pi complesso e sequenziale , come accade con il finger tapping , si pu osservare lattivazione anche della corteccia motoria primaria omolaterale e dei lobi parietali , che sono coinvolti nella percezione del movimento nello spazio [ 6 ]  . prima di valutare i risultati ottenuti nei pazienti parkinsoniani , va sottolineato come eventuali differenze rispetto ai volontari sani potrebbero essere legate non solo alla malattia , ma anche al fattore et . 
riguardo a questultimo aspetto , va ricordato come la fascia det dei volontari sani sia 2337 anni , mentre quella dei pazienti 5682 anni e come non esistano in letteratura studi di rm funzionale sullattivazione cerebrale indotta da finger tapping , eseguito nelle medesime condizioni da soggetti sani , ma di et diverse . 
va comunque sottolineato come lunico lavoro pubblicato , nel quale stata messa a confronto lentit di attivazione delle aree motorie primarie durante un compito motorio , valutata con spettroscopia , in soggetti di diverse fasce di et , non ha dimostrato una differenza di attivazione statisticamente significativa tra i diversi gruppi [ 7 ]  . 
in tutti i parkinsoniani stata osservata la presenza dellattivazione della corteccia motoria primaria controlateralmente alla mano in esame . ma , mediamente , a tale livello lintensit di segnale superiore rispetto a quanto osservato nei volontari sani : questa iperattivit dellarea motoria primaria controlaterale gi stata descritta in letteratura [ 8 , 9 ] e potrebbe rappresentare il substrato neurale della difficolt del paziente con morbo di parkinson nellesecuzione del movimento . 
moreover , taking into account the hemispheric dominance and equal distribution of parkinsons disease between the dominant and non - dominant hand , the correlation between observations and the disease seems plausible . 
 an explanation of our results might be that there is a recovery of the activity of the ipsilateral motor cortex , compensating for the contralateral deficit , as demonstrated by two positron emission tomography ( pet ) studies on patients with central , lateralised and ischaemic deficits [ 10 , 11 ]  . 
in addition to the contralateral motor cortex , the ipsilateral cortex appears to undergo a process of compensatory functional re - organisation . another phenomenon has been described that could account for this asymmetry in activation , which is also seen in subjects with motor deficits : the presence of associated movement of the hand contralateral to the one being studied [ 12 ]  . 
although this was not done in our study , we did carefully monitor the subjects visually during image acquisition , and no movement of the contralateral hand in either volunteers or patients was detected . as regards activation of the supplementary motor and premotor cortices , these were activated in six parkinsonian patients , with asymmetric activation ( more intensely during the movement of the healthy hand )  . 
this could be explained by the speed of movement . a recent study observed that the intensity of activation of the pre - motor and supplementary motor areas in healthy volunteers is directly proportional to the speed of the hand movement [ 2 ]  . 
this aspect has already been observed in the literature [ 2 , 79 ] and is explained in the following manner : the parietal cortex integrates different sensory , motivational and attentional inputs and can therefore provide the basis for the generation of sensory - guided movements in parkinsons patients without requiring circuitry between the basal ganglia and frontal cortex , which are altered in these patients . as a consequence , hyperactivity of the parietal lobes , along with activation of the pre - motor and supplementary motor areas , would be a compensatory mechanism for the hypoactivity of striatofrontal projections , thus creating an intact alternative pre - motorparietal circuit . 
in this respect , we found no difference in the activation of the parietal lobes between movement of the affected and healthy hands in parkinsons patients , and this suggests that these alterations entrambe le mani . 
inoltre , tenendo conto della dominanza emisferica , e dellequa distribuzione del morbo di parkinson , alla mano dominante e non , la correlazione possibile tra quanto osservato e la patologia sembra plausibile . 
una spiegazione dei nostri risultati pu essere data dal fatto che vi sia un recupero dellattivit della corteccia motoria ipsilaterale , compensatoria al deficit controlaterale , come dimostrato in due studi eseguiti con tecnica pet su pazienti con deficit centrale , lateralizzato , ischemico [ 10 , 11 ]  . 
in letteratura stato descritto un ulteriore fenomeno che potrebbe essere alla base di questa asimmetria di attivazione che presente anche nei soggetti con deficit motorio : la presenza di movimento associato della mano opposta a quella in esame [ 12 ]  . 
esso non ha messo in evidenza movimenti della mano controlaterale , n nei volontari , n nei parkinsoniani . riguardo allattivazione delle cortecce motoria supplementare e premotoria , nei parkinsoniani si dimostrata la loro attivazione in sei casi , con attivazione asimmetrica ( maggiore intensit di attivazione durante il movimento della mano sana )  . 
in un recente studio si osservato come in volontari sani lintensit di attivazione delle aree premotoria e supplementare motoria sia direttamente proporzionale alla velocit del movimento della mano [ 2 ]  . 
questo aspetto gi stato osservato in letteratura [ 2 , 79 ] ed giustificato dal fatto che la corteccia parietale viene ritenuta un integratore di diversi input sensitivi , motivazionali ed attenzionali che possa pertanto fornire le basi per la genesi di movimenti guidati da stimoli sensoriali nei pazienti affetti da morbo di parkinson senza la necessit dei circuiti tra gangli della base e corteccia frontale , che sono alterati in questi pazienti . 
pertanto liperattivazione dei lobi parietali , insieme allattivazione delle aree premotoria e supplementare motoria , rappresenterebbe un meccanismo di compenso per lipofunzione delle proiezioni striato - frontali , creando un circuito alternativo integro premotorio - parietale . 
a tale riguardo , non abbiamo rilevato una differenza di attivazione dei lobi parietali tra movimento della mano malata e movimento della mano sana nei parkinsoniani , e questo suggerisce come tali alterazioni possano essere rilevabili anche in una fase preclinica . 
another hypothesis is that the impairment of the connections between basal nuclei and cortex , responsible for parietal cortical hyperactivity , changes the perception of movement in space in patients during the movement of both the healthy and affected hands . another observation concerns the activation of the occipital lobes . 
this was absent in healthy volunteers . these results are certainly interesting from a neuropathological point of view but might also have clinical relevance , in particular , in the differential diagnosis between the different types of parkinsonism , and suggest an anatomical - physiological basis for the rehabilitation of these patients . 
more precisely , functional mri could be used in the differential diagnosis of parkinsons disease and cortico - basal degeneration , which has been shown to have a different activation pattern [ 13 ]  . 
consequently , the technique could be useful in the initial stages of the disease , when the cortico - basal degeneration may be impossible to distinguish clinically from parkinsons disease although the therapeutic approach and prognosis are completely different . the main limitation of our study , shared by all studies of this kind , concerns the small number of patients studied , which precludes a statistical analysis of the results . 
however , the problems in finding patients with a lateralised akineticrigid form of parkinsons who can endure a functional mri examination should be considered . rattivit corticale parietale , determini nei pazienti una alterata percezione del movimento nello spazio , presente sia durante il movimento della mano sana che della mano malata . altra osservazione quella relativa allattivazione dei lobi occipitali : un primo commento riguarda il fatto che non stato chiesto n ai volontari sani n ai pazienti di tenere gli occhi chiusi durante lacquisizione delle immagini . 
questa spiegazione trova ulteriore conferma dallosservazione sperimentale della presenza di ampi movimenti del capo nei parkinsoniani allinizio del compito motorio , movimenti eseguiti involontariamente per permettere il controllo visivo del movimento . conclusioni con questo lavoro abbiamo descritto i patterns di attivazione corticale durante un compito motorio in pazienti affetti da morbo di parkinson lateralizzato confrontandoli con quelli nei volontari sani e inoltre , nellambito dello stesso paziente , abbiamo confrontato lattivazione ottenuta con la mano sana con quella della mano malata . 
inoltre stata riscontrata , in alcuni casi , lassenza di attivazione a livello delle aree premotoria e supplementare motoria , verosimilmente secondarie allimpaccio motorio . dove , invece , tali zone si attivavano lo facevano con intensit superiore durante il movimento della mano sana . 
infine , si osservata una spiccata tendenza di questi pazienti al controllo visivo del movimento con conseguente attivazione dei lobi occipitali , assente nei volontari sani . questi risultati sono sicuramente interessanti da un punto di vista neurofisiopatologico , ma potrebbero anche rivestire un ruolo nellambito clinico , in particolare nella diagnosi differenziale tra i diversi parkinsonismi e suggerire una base anatomo - fisiologica per il recupero fisiatrico di questi pazienti . 
pi precisamente la rm funzionale potrebbe essere impiegata nella diagnosi differenziale tra morbo di parkinson e degenerazione cortico - basale , nella quale si dimostrato un diverso pattern di attivazione [ 13 ]  . 
pertanto tale tecnica potrebbe risultare utile nelle fasi iniziali di malattia , quando la degenerazione cortico - basale pu essere clinicamente indistinguibile dal morbo di parkinson , ma il suo approccio terapeutico e la prognosi sono completamente diverse . il principale limite del nostro lavoro , comune a tutti i lavori simili pubblicati , riguarda la non elevata numerosit dei pazienti che non consente una valutazione statistica dei risultati . 
cova1 1unit clinica operativa di radiologia , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , i - 34149 trieste , italy 2unit operativa di radiologia , ospedale umberto i , mestre , venezia , italy 3dipartimento di economia e tecnica aziendale , universit degli studi di trieste , trieste , italy correspondence to : f . 
the sum of equipment costs ( amortisation and service contract ) , variable costs ( supplies and related services ) and personnel costs ( radiologist , radiographer and nurse ) was determined . 
intra - arterial dsa costs more than mra , mainly because of the higher costs of supplies used during the procedure and higher personnel costs ( as a result of the longer duration of intra - arterial dsa )  . 
mra provides good diagnostic accuracy in the evaluation of arteries of the lower extremities , and its biological cost is far lower than that of intra - arterial dsa ( mra is noninvasive , it does not use ionising radiation , and the contrast medium is safe )  . 
its lower cost is another argument in favour of the use of mra instead of intra - arterial dsa in the evaluation of lower - extremity arterial disease . key words magnetic resonance angiography intra - arterial digital subtraction angiography cost analysis peripheral vascular disease riassunto obiettivo . 
stato calcolato il costo differenziale delle due indagini , ovvero la somma dei costi delle apparecchiature ( ammortamenti e manutenzione ) , dei costi variabili ( materiali e servizi connessi ) e dei costi del personale ( medico , tecnico e infermieristico )  . 
il costo differenziale dellangio - rm risultato di 186 , 14 euro ( costi delle apparecchiature 50 , 80 euro , costi variabili 75 , 04 euro , costi del personale 60 , 30 euro ) , mentre quello dellangiografia digitale risultato di 238 , 18 euro ( costi delle apparecchiature 57 , 60 euro , costi variabili 90 , 13 euro , costi del personale 90 , 45 euro )  . 
langiografia digitale ha un costo superiore allangio - rm , determinato essenzialmente dal maggior costo del materiale utilizzato durante la procedura e dal maggior costo del personale ( legato , a parit di figure professionali coinvolte , alla maggior durata dellesame angiografico )  . 
langio - rm fornisce una buona accuratezza diagnostica nella valutazione delle arterie degli arti inferiori ed ha un costo biologico nettamente inferiore allangiografia digitale ( assenza di invasivit , assenza di radiazioni ionizzanti , mezzo di contrasto con pi elevato margine di sicurezza )  . 
il minor costo dellangio - rm costituisce un ulteriore elemento che porta a preferire questa indagine allangiografia digitale nella diagnostica delle arteriopatie degli arti inferiori . parole chiave angio - rm angiografia digitale intra - arteriosa analisi dei costi arteriopatia periferica f . 
technological advancements have allowed this technique to provide high levels of sensitivity and specificity as compared with digital subtraction angiography ( dsa ) as the gold standard even though the reported ranges are extremely wide ( sensitivity : 71%100% , specificity : 63%100% ) [ 111 ]  . 
most papers have , therefore , considered its diagnostic contribution and emphasised its advantages of having a negligible biological cost . by contrast , this study analyses and compares the costs of mra and intra - arterial dsa in the evaluation of lower - limb arteries . 
it should be noted that activities and costs related to these two examinations pertain largely to the radiology department even if some aspects , particularly related to dsa , concern other departments as well . 
the costs were also analysed from the point of view of the producer ( the hospital ) , whose aim it is to provide the patient with the best and most cost - effective clinical approach . 
our study presents a cost - identification analysis , namely , a partial assessment of the two examinations in question , concentrating on their effect on costs ( input ) [ 12 ]  . 
clinical consequences of the two different approaches have , instead , been excluded from our study ( output )  . langiografia mediante risonanza magnetica ( angio - rm ) ha trovato negli ultimi anni applicazione sempre pi ampia nella valutazione delle arteriopatie degli arti inferiori . 
i progressi tecnologici hanno fatto s che tale indagine possa garantire una sensibilit ed una specificit elevate , utilizzando langiografia digitale come gold standard , pur se i lavori pubblicati riportano un range di percentuali assai ampio ( sensibilit tra il 71% e il 100% , specificit tra il 63% e il 100% ) [ 111 ]  . 
molti lavori hanno preso quindi in considerazione il suo apporto diagnostico ed hanno sottolineato i suoi benefici , per il trascurabile costo biologico . in questo lavoro abbiamo ritenuto opportuno analizzare invece i costi dellangio - rm nella valutazione delle arterie degli arti inferiori , raffrontati a quelli dellangiografia digitale per via arteriosa . 
va rilevato come attivit e costi relativi a queste due indagini sono in larga misura di pertinenza dei servizi di radiologia , ma per talune , langiografia digitale in particolare , riguardano anche altri reparti . 
i costi sono inoltre stati considerati dal punto di vista del produttore ( lospedale ) che ha lobiettivo di fornire al paziente lapproccio clinico migliore e con il miglior rapporto costo - efficacia . 
lanalisi dei costi effettuata del tipo cost - identification , ovvero una valutazione parziale con lobiettivo di valutare , analizzando le due indagini considerate , gli effetti sui costi ( input ) [ 12 ]  . 
non sono invece state considerate le conseguenze cliniche dei due diversi approcci ( output )  . materials and methods examination technique magnetic resonance angiography mra examinations were performed using a 1.5 - t intera master superconductive magnet ( philips medical systems , eindhoven , the netherlands ) with 30 mt / m power gradients and 150 mt / m per millisecond rise time . 
the use of automated table movement ( mobitrack , philips ) allowed us to study the aorto - iliac , femoral - popliteal and popliteal - tibial vascular regions in a sequence . 
for evaluation of each vascular region , we used three - dimensional ( 3 - d ) fast spin echo ( fse ) t1 - weighted sequences with the following parameters : tr = 6 ms , te 1.5 ms , flip angle 35 , slice thickness 1.5 mm ( 3 mm with 1.5 - mm overlap ) , field of view 430 mm , matrix 512512 , number of slices 70 and acquisition time 28 s . 
overall acquisition time of successive sequences , including the time needed for two table movemateriali e metodi tecnica desame angio - rm gli esami di angio - rm sono stati eseguiti utilizzando un magnete superconduttivo da 1 , 5 t intera master ( philips medical systems , eindhoven , olanda ) con gradienti di potenza pari a 30 mt / m e velocit di raggiungimento del picco di 150 mt / m / ms . 
limpiego dello spostamento automatico del tavolo ( mobitrack ; philips ) ha consentito di studiare in successione il distretto vascolare aorto - iliaco , quello femoropopliteo e quello popliteo - tibiale . 
sono state impiegate per la valutazione di ciascun distretto vascolare sequenze 3d fse t1 pesate utilizzando i seguenti parametri : tr = 6 ms , te 1 , 5 ms , flip angle = 35 , spessore di strato pari ad 1 , 5 mm ( 3 mm con sovrapposizione di 1 , 5 mm ) , campo di vista = 430 mm , matrice = 512x512 , numero di strati = 70 , tempo di acquisizione paf . 
this was followed by injection of 0.2 mmol / kg of 0.5 m paramagnetic contrast agent ( gadobenate dimeglumine , multihance , bracco , milan , italy ) with a 0.5 - ml / s flow rate . 
post - processing included subtraction of images acquired before and after the contrast agent injection and 3 - d reconstructions based on the maximum intensity projection ( mip ) algorithm . dsa ( intra - arterial ) dsa examinations were carried out using the integris allura system for diagnostic angiography and interventional radiology ( philips medical systems , eindhoven , the netherlands )  . 
examinations were performed with intra - arterial catheterisation , usually after puncture of the femoral artery and insertion of the distal end of the catheter into the infrarenal abdominal aorta . 
straight - end or pigtail catheters , which can endure high flows of contrast material , were employed . intra - arterial examinations were performed using two different methods : the bolus - chasing technique ( in which synchronised table movement during injection of the contrast agent allows passage of the contrast through the aorto - iliacfemoral - popliteal region to be monitored ) , and the successive fields technique . 
choice of technique was based on the result of the preliminary test to determine the knee arrival time ( kat ) or the number of seconds it takes for a small amount of injected contrast agent to reach the popliteal artery at the knee joint . we noted that when the kat is very short ( 46 in . ) , image quality , especially at the abdominal level , is affected by blurring of the vessel caused by the table moving too fast . hence , the bolus - chasing technique is only used when the kat exceeds 7 s whereas for shorter kats , the classical multiple - fields technique is adopted . 
in the bolus - chasing technique , the examination is carried out with a single injection of 80 ml of non - ionic monomeric contrast medium ( 350370 mgi / ml ) with a 79 ml / s flow rate through an automatic injector , and the table moves automatically at a speed determined by result of the preliminary test . 
stato preliminarmente valutato con liniezione di 2 ml di mezzo di contrasto ( mdc ) ( 0 , 5 ml / s ) in una vena del braccio il tempo necessario per iniziare ad ottenere lopacizzazione dellaorta addominale . 
sono state quindi effettuate con spostamento del tavolo le sequenze maschera ( senza somministrazione del mdc ) sui tre tratti a partire da quello popliteo - tibiale . sono stati poi iniettati 0 , 2 mmol / kg di un mdc paramagnetico 0 , 5 m ( gadobenato dimeglumina , multihance , bracco , milano , italia ) con flusso di 0 , 5 ml / s . 
sono state quindi acquisite le sequenze dopo iniezione di mdc a partire dal distretto aorto - iliaco , secondo il tempo di ritardo calcolato mediante il bolo preliminare di 2 ml . 
il post processing prevedeva la sottrazione di immagine tra quelle acquisite prima e dopo iniezione di mdc e ricostruzioni 3d secondo lalgoritmo mip ( maximun intensity projection )  . angiografia digitale ( accesso arterioso ) gli esami sono stati effettuati utilizzando il sistema per angiografia diagnostica e radiologia interventistica integris allura ( philips medical systems , eindhoven , olanda )  . 
sono stati utilizzati cateteri ad estremit diritta o pig tail in grado di sostenere flussi elevati di mdc . gli esami con accesso arterioso sono stati eseguiti con due diverse modalit : tecnica bolus chasing ( che grazie al movimento sincronizzato del tavolo durante liniezione del mdc consente di seguire lavanzamento del bolo di mdc nel distretto aorto - iliaco - femoro - popliteo ) o tecnica per campi successivi . 
la diversa tecnica di esecuzione si basata sul risultato del preliminare test per determinare il kat ( knee arrival time ) che stabilisce , una volta iniettato un piccolo quantitativo di mdc , quanti secondi esso impiega a giungere nellarteria poplitea a livello della rima articolare del ginocchio . 
si verificato che quando il kat molto breve ( 46 s ) la qualit delle immagini soprattutto a livello addominale risulta essere subottimale per la presenza di sfumatura del vaso causata dalleccessiva velocit del movimento di avanzamento del tavolo . 
nella tecnica bolus chasing lesame viene effettuato con ununica iniezione di 80 ml di un mdc monomero non ionico ( 350370 mgi / ml ) ad un flusso di 79 ml / s eseguita mediante apposito iniettore automatico e il tavolo scorre automaticamente ad una velocit che si basa sul risultato del test preliminare . 
if motion artefacts are present , images can be processed with pixel shift software so as to minimise them . if motion artefacts are more substantial , images can be visualised at any rate without subtracting the skeletal structures . 
an automatic injector is again used to administer 30 ml of contrast agent at a 15 - ml / s flow rate for each field , for a total of 150 ml . 
the full cost of the two studies was thus obtained ( the sum of differential and common costs )  . equipment cost was calculated based on the time it was used ; when analysing the cost of technology , the purchase price of the various machines ( which can be strongly affected by substantial discounts ) and the adequacy of the system for calculating amortisation are clearly important . 
purchase prices were derived from hospital administration records . amortisation was calculated on a time basis based on a constant annual value . the lifetime of the radiological units was estimated as 8 years , i.e. 
procedure duration was estimated based on times envisaged by the radiology information system ( ris ) in use at our unit . in evaluating the differential cost , we merely considered the technical act , disregarding any other costs related to patient management , as inclusion of the latter would have required an explicit description of the relations between the radiology department and other cost centres of the hospital and the part played by radiological examinations in inpatient treatment . therefore , our analysis was restricted to costs incurred by the radiology unit . 
this made it possible to draw comparisons over time ( with respect to budget targets ) and space ( with respect to other hospitals : independent , with separate accounting , or private ) [ 13 ]  . 
 the cost of fixed - asset utilisation ( technology ) was related to their time of use , and the cost of radiologists , technologists and nurses was related to their specific activity meadelliniezione del mdc e la seconda durante liniezione del mdc , ottenendo quindi due serie di 15 immagini ciascuna . 
ad ogni campo desame vengono iniettati , sempre mediante iniettore automatico , 30 ml di mdc con un flusso di 15 ml / s , per un totale di 150 ml . analisi economica stato calcolato il " costo differenziale " ( definito come la somma dei costi delle apparecchiature , dei costi variabili e dei costi del personale ) delle due indagini . 
 stato inoltre calcolato il " costo comune " , il quale raggruppa quelle componenti del costo che risultano sovrapponibili per ogni tipo di esame svolto allinterno dellunit clinico operativa di radiologia . 
stato cos possibile ottenere il " costo pieno " delle due indagini ( somma del costo differenziale e di quello comune )  . il costo delle apparecchiature stato calcolato in base al tempo di utilizzo delle stesse ; nel valutare il costo della tecnologia emerge limportanza del costo dacquisto delle diverse attrezzature ( che pu essere influenzato notevolmente da sconti significativi ) e della congruit del sistema di calcolo dellammortamento . 
la durata della vita lavorativa delle apparecchiature radiologiche stata considerata di otto anni , il loro tempo tecnologico massimo . sono poi stati valutati i costi variabili , relativi ai materiali impiegati e ai servizi legati a tale impiego . 
la durata delle procedure stata stimata facendo riferimento ai tempi previsti nel sistema informativo radiologico ( ris ) in uso presso la nostra struttura . nella valutazione del costo differenziale ci siamo limitati a considerare latto tecnico , ignorando tutti gli altri costi legati alla gestione del paziente . 
ci infatti avrebbe comportato lesplicitazione di tutti i rapporti tra la radiologia e gli altri centri di costo dellazienda ospedaliero - universitaria e , per i pazienti ricoverati , anche del ruolo che le indagini radiologiche hanno sul processo di cura . 
they are therefore not decisive for comparing costs but play a role in determining the full cost of the two methods . the sections below provide a detailed analysis of the differential costs of mra and dsa , with the methods in use at our radiology unit . 
as stated above , three components of the differential cost were considered , namely : ( 1 ) equipment costs ( amortisation and service contract ) ; ( 2 ) variable costs ( supplies and related services ) ; ( 3 ) personnel costs . it should be noted that every patient undergoing dsa must have a blood test to evaluate serum glucose and creatinine levels and coagulation profile [ quick time , international normalised ratio ( inr ) and platelets ]  . in addition , patients with a history of allergy ( 1% of cases ) require pre - medication with steroids associated with antih1 and anti - h2 . the cost of these procedures does not pertain to the radiology unit however , because the procedures are mandatory before contrast - enhanced angiography and because their cost is not negligible , they will be briefly discussed . finally , it should be recalled that costs of supplies and equipment are inclusive of 20% vat . results differential costs magnetic resonance angiography 1 . 
we took into account the cost of a 1.5 - t intera master mri device ( philips medical systems , eindhoven , the netherlands ) with 30 - mt / m power gradients and a rise time of 150 mt / m per millisecond . 
there follows an annual cost of 3 , 021.25 euro considering 8 years of amortisation . then the cost of the dry printer ( kodak dryview 8700 laser imager ) was included . 
come gi evidenziato , sono state prese in considerazione 3 componenti del costo differenziale , e precisamente : ( 1 ) costi delle apparecchiature ( ammortamenti e manutenzione ) ; ( 2 ) costi variabili ( materiali e servizi connessi ) ; ( 3 ) costo del personale . va rilevato che ogni paziente sottoposto ad angiografia digitale deve eseguire preliminarmente un prelievo ematico per valutare i livelli sierici di glucosio e creatinina e il suo assetto emocoagulativo ( tempo di quick , inr e piastrine )  . nell1% dei casi inoltre , essendoci unanamnesi allergica positiva , si esegue anche una preparazione farmacologica ( basata sullimpiego di cortisonici associati ad anti - h1 ed anti - h2 )  . 
i costi legati a tali procedure non sono di pertinenza dellunit clinico operativa di radiologia ; tuttavia queste sono fondamentali ai fini dellesecuzione dellesame angiografico con mezzo di contrasto ed avendo comunque un certo rilievo economico verranno in seguito brevemente prese in considerazione . si ricorda infine che i costi di materiali ed apparecchiature sono comprensivi di iva al 20% . risultati costi differenziali angio - rm 1 . 
abbiamo preso in considerazione il costo di un apparecchio di rm da 1 , 5 t intera master con gradienti di potenza pari a 30 mt / m e velocit di raggiungimento del picco di 150 mt / m / ms . 
by estimating the average annual cost of a radiologist , technologist and nurse ( totalling 158 , 744 euro ) and subtracting the time off work for ordinary , special and sick leave ( 30% on average ) from the annual hourly debt , the actual work time amounted to 35 weeks / year , which results in a daily cost of 905 euro and an hourly cost of 120.73 euro for these three professionals taken together . 
valutando il costo medio annuo per un medico , per un tecnico sanitario di radiologia medica ( tsrm ) e per un membro del pool infermieristico ( complessivamente 158.744 euro ) e sottraendo al debito orario annuo le assenze per congedo ordinario , straordinario e malattie ( 30% in media ) , risulta un tempo lavorativo effettivo pari a 35 settimane / anno , da cui si deriva il costo giornaliero ( 905 euro ) e orario ( 120 , 73 euro ) di queste tre figure professionali considerate assieme . 
limpegno temporale del medico legato alle diverse attivit che egli deve svolgere in prima persona , ovvero : presenza fisica in fase di acquisizione dellesame , analisi delle immagini alla consolle , refertazione , correzione e sigla del referto . 
va inoltre preso in considerazione il tempo preliminare allesame ; in particolare , il paziente deve sottoscrivere un apposito questionario mediante il quale se ne verifica lidoneit allaccesso al magnete . 
perci , in base alla nostra esperienza , il tempo medico previsto per un angio - rm degli arti inferiori di 30 minuti . ogni indagine di angio - rm per lo studio degli arti inferiori comporta un impegno temporale del tsrm e dellinfermiere anchesso stimabile in 30 minuti . 
ne risulta quindi un costo personale per esame di 60 , 30 euro . da quanto esposto risulta come , sommando tutti i parametri considerati , il costo differenziale di unangio - rm degli f . 
the cost of the contrast agent injector ( mark 4 , medrad , indianola , usa ) , 8 , 374.29 euro , corresponds to 1 , 046.78 euro per year for 8 years of amortisation . 
the following factors were taken into account : supplies used prior to the procedure ( sterile gloves , disinfection material , sterile cloth , sterile cloths without slit , a sheet with slit for femoral access ) : total cost of preparatory supplies was 1.10 euro supplies used during the procedure ( surgical gauzes , 10 - cc luerlock syringe , 20 - cc syringe , needle for arterial puncture , lidocaine , guidewire , introducer , catheter )  . 
essa viene utilizzata dallunit clinico operativa di radiologia con contratto daffitto triennale comprensivo di installazione , interfacciamento ai sistemi di archiviazione delle immagini e manutenzione , per un costo pari a 13.785 , 00 euro annui . 
alla stampante a secco confluiscono peraltro le due apparecchiature tc in uso nellunit clinico operativa di radiologia ; nel nostro caso langiografo digitale utilizza la stampante per circa il 30% della sua attivit ; ne deriva quindi un costo annuo di 4135 , 50 euro . 
va inoltre considerato il costo delliniettore del mezzo di contrasto ( mark 4 , medrad , indianola , usa ) pari a 8.374 , 29 euro , il che corrisponde a 1.046 , 78 euro annui per 8 anni di ammortamento . 
vanno presi in considerazione i seguenti fattori : materiale preparatorio allesecuzione dellesame ( guanti sterili , materiale per disinfezione , telino sterile , teli sterili senza spacco , lenzuolo con taglio accesso femorale )  . 
il costo totale del materiale preparatorio di 1 , 10 euro . materiale utilizzato durante la procedura ( garze sterili , siringa luerlock da 10 cc , siringa da 20 cc , ago da puntura arteriosa , lidocaina , guida , introduttore , catetere )  . 
estimating the overall average annual cost for a radiologist , a technologist and a nurse at 158 , 744 euro and subtracting ordinary , special and sick leaves ( 30% on average ) from the annual hourly debt , the actual work time is 35 weeks / year , with a daily cost of 905 euro and an hourly cost of 120.73 euro for these three professionals taken together . the radiologists time commitment depends on the different activities he / she has to perfor in the case of an angiographic examination , the radiologists time includes performing the procedure from the end of patient preparation to positioning the catheter into the aorta , as well as being physically present during the acquisition phase , assessing images on screen , removing the catheter , performing the compression , reporting , correcting and signing the written report . hence , based on our experience , intra - arterial lower limb angiography involves 45 min of the radiologists time . 
these costs are unaffected by variations in the total number of yearly examinations . common costs are those associated with support staff and support materials . we were unable to conduct a detailed analysis of support activities to quantify the contribution of these production factors to the different procedures ( random principle ) , but we could , as an alternative , use the means method , assuming that each radiological procedure uses these services to the same extent , i.e. 
that the specific features of each procedure do not affect the common costs . support staff costs were calculated considering all professionals not described so far . they consist of one consultant , one chief technologist , three technologists , three auxiliary staff , four file clerks and seven assistants and administrative assistants . 
per ogni esame se ne impiegano in media 120 ml ( diaco , sodio cloruro 0 , 9% ) usando flaconi da 250 ml ( al costo di 0 , 25 euro per flacone ) , con un costo per esame di 0 , 10 euro . pellicole : nella documentazione delle angiografie degli arti inferiori previsto luso di una pellicola 3543 cm ( dvb kodak ) , per un costo di 2 , 97 euro ( le confez ioni da 500 hanno un costo di 1489 , 40 euro )  . 
valutando il costo medio annuo complessivo di un medico , un tsrm e un infermiere in 158.744 euro e sottraendo al debito orario annuo le assenze per congedo ordinario , straordinario e malattie ( in media 30% ) , risulta un tempo lavorativo effettivo pari a 35 settimane / anno , da cui si deriva un costo giornaliero di 905 euro e orario di 120 , 73 euro di queste tre figure professionali considerate assieme . 
nel caso dellesame angiografico il tempo medico prevede lesecuzione della procedura dal termine della preparazione del paziente fino al posizionamento del catetere in aorta , la presenza fisica in fase di acquisizione dellesame , la verifica a monitor delle immagini acquisite , la rimozione del catetere , la compressione , la refertazione dellesame , la correzione e la sigla del referto . 
ne risulta quindi un costo personale per esame di 90 , 45 euro . da quanto esposto risulta come , sommando tutti i parametri considerati , il costo differenziale di una indagine angiografica degli arti inferiori risulti presso il nostro istituto di 238 , 18 euro . costi comuni abbiamo indicato con lespressione costi comuni i costi dei fattori produttivi , interni allunit clinico operativa di radiologia , che garantiscono unattivit di supporto a tutti gli atti diagnostici svolti nellunit operativa . 
non siamo in grado di effettuare unanalisi dettagliata delle attivit di supporto per quantizzare il contributo di questi fattori produttivi alle diverse procedure ( criterio causale ) , per cui rimane lalternativa di ricorrere al metodo della media , ipotizzando che ciascuna indagine radiologica usufruisca in pari misura di tali servizi , vale a dire che le specificit di ciascuna indagine non siano una determinante dei costi di cui stiamo trattando . 
non riteniamo che il loro lavoro sia influenzato dalla tipologia degli esami svolti e quindi il loro costo complessivo stato ripartito proporzionalmente su tutte le indagini eseguite presso lunit clinico operativa di radiologia . i materiali di supporto comprendono computer , stampanti , registratori , materiale elettrico e di rete , materiale di cancelleria e materiale di pulizia . 
ne risulta un costo comune aggiuntivo per esame di 5 , 62 euro . costo pieno sommando i costi differenziali con i costi comuni , stato calcolato il costo pieno di ciascuna indagine ( tabella 1 ) , ovvero : 1 . 
angio - rm : 186 , 14 euro + 5 , 62 euro = 191 , 76 euro ; 2 angiografia digitale : 238 , 18 euro + 5 , 62 euro = 243 , 8 euro . in tutti i pazienti che vengono sottoposti ad indagini contrastografiche che prevedono limpiego di un mezzo di contrasto organo iodato ( in questo caso si tratta dellesame angiografico ) viene effettuato un prelievo ematico per valutarne i livelli sierici di glucosio e creatinina a cui vengono aggiunti i parametri emocoagulativi ( inr , assetto piastrinico ) per un costo complessivo di 7 , 50 euro per esame . 
questo costo non rientra tra i costi differenziali dellesame , per riteniamo non scorretto sottolineare come langiografia venga cos a pesare maggiormente sui costi allesterno della struttura radiologica rispetto allangio - rm . 
opportuno infine ricordare , come gi precedentemente accennato , che circa nell1% dei pazienti che vanno sottoposti ad esami angiografici , essendoci unanamnesi allergica positiva , si esegue anche una preparazione farmacologica ( basata sullimpiego di cortisonici associati ad anti - h1 ed anti - h2 ) , per un costo di 4 euro , in media 0 , 04 euro in pi per ogni esame . 
 complessivamente , questi costi esterni alla radiologia ammontano a 7 , 54 euro . discussione e conclusioni lanalisi dei costi ha dimostrato un costo superiore del 27 , 1% dellangiografia digitale rispetto allangio - rm nella valutazione delle arterie degli arti inferiori ( 243 , 8 versus 191 , 76 euro )  . 
factors with the highest impact are supplies used in the procedure and personnel costs ( owing to the longer examination time )  . decisions concerning the treatment to be pursued after ascertaining that treatment is indeed required will also affect overall cost calculation [ 1417 ]  . indeed , mra may or may not evidence lesions requiring surgical treatment with percutaneous transluminal angioplasty ( pta ) and / or stent placement . 
in this event , the cost of the mra examination should be subsequently added to the costs of intra - arterial angiography and the costs for 1 day in hospital after the interventional procedure ( however , costs of hospitalisation are not included in our analysis , which assesses only costs incurred by the radiology unit )  . it would also be possible to perform angiography first , combining the diagnostic and therapeutic parts in one session , thereby avoiding mra examination . this approach would have to take into account an additional hypothetical , non - predictable workload for the section and delays or cancellations of scheduled examinations because of possible complications arising during the procedure . in our personal experience , however , diagnostic and interventional procedures are usually performed separately . it should also be noted that after diagnostic angiography with arterial catheterisation , the patient is usually hospitalised to monitor possible complications such as bleeding . therefore , external costs of hospitalisation need to be considered . on the other hand , an alternative to manual compression and hospitalisation is to apply an intra - vasal haemostatic device ( angio - seal ) [ 18 ]  . if the device is applied at the end of the procedure , the patient can be mobilised immediately without serious complications or longer examination times [ 19 ]  . 
however , the use of this device entails a cost of 139.44 euro , which , although cheaper than 1 day in hospital , directly weighs on our units budget . 
if it were used , it would then have considerable impact on the full costs of dsa . hospitalisation may also be avoided by monitoring the patient for 5 h after a 15 - min compression and then conducting a telephone follow - up up to the seventh day [ 20 , 21 ]  . 
a further alternative to avoid hospitalisation may be to perform the diagnostic examination with a brachial as opposed to femoral access . the cost analysis we conducted employed a technique often applied in industry , which ensures a rigour that reduces fattori che incidono maggiormente sono rappresentati dal costo del materiale utilizzato durante la procedura e dal costo del personale ( questultimo legato , a parit di figure professionali coinvolte , alla maggior durata dellesame angiografico )  . 
vi infatti la possibilit che langio - rm non evidenzi lesioni passibili di trattamento interventistico mediante pta e / o posizionamento di stent , oppure al contrario che dimostri lesioni suscettibili di tali trattamenti . 
in questo secondo scenario , al costo dellesame angio - rm andrebbero successivamente aggiunti i costi relativi allesame angiografico eseguito mediante accesso arterioso e i costi relativi ad un giorno di degenza post - procedura interventistica ( i costi di degenza non rientrano peraltro nella nostra analisi che valuta i costi allinterno dellunit clinico operativa di radiologia )  . vi sarebbe peraltro la possibilit di eseguire in primis langiografia , effettuando cos in ununica seduta sia la parte diagnostica che la parte terapeutica , evitando in tal modo lesame di angio - rm . 
tale atteggiamento dovrebbe tenere in considerazione il carico di lavoro ipotetico aggiuntivo non prevedibile della sezione e eventuali ritardi o annullamento di esami programmati a causa di eventuali complicanze insorte in corso di procedura . 
esso tuttavia presenta un costo di 139 , 44 euro che , pur essendo inferiore al costo di un giorno di degenza , grava direttamente sul budget dellunit clinico operativa di radiologia . qualora utilizzato , esso graverebbe quindi considerevolmente sui costi pieni dellangiografia digitale . la degenza ospedaliera pu anche essere evitata eseguendo al termine di una compressione di 15 minuti un monitoraggio temporaneo del paziente per 5 ore e successivamente un follow - up telefonico fino alla 7a giornata [ 20 , 21 ]  . 
 unulteriore alternativa per evitare la degenza pu essere costituita da un esame diagnostico eseguito con accesso brachiale anzich femorale . lanalisi dei costi da noi condotta fa riferimento a una tecnica ampiamente utilizzata in campo industriale che garantisce un rigore che riduce le approssimazioni dei metodi tradizionali di calcolo dei costi [ 22 ]  . 
they reflect the situation in our department at a certain moment in time , but costs in other radiology departments may be extremely different to assess , either owing to different costs of equipment used or simply because of different organisation , which can affect variable costs ( different materials used ) or personnel costs ( possible different roles )  . 
in our view , this does not detract from the validity of our analysis , but it emphasises its value in suggesting a model that can be easily applied to other settings rather than for reported cost data . this can therefore be a stimulus for similar cost evaluations of these two techniques , possibly considered within more complex diagnostic protocols or in comparison with other techniques , such as ct angiography . clearly , a cost analysis is only the first step towards a cost - effectiveness analysis , which considers both the diagnostic benefits , including impact on therapy , and biological costs . the high diagnostic accuracy of mra in the evaluation of lower - limb arteries is an established fact [ 111 ]  . 
in addition , mra no doubt offers clear advantages over angiography if biological costs are considered since it is non - invasive , involves no ionising radiation and makes use of a paramagnetic contrast agent , which is safer than organic iodinated products . 
these elements led to a quick transition from dsa to mra in the diagnosis of lower - limb arterial disease in our department . in 2004 , mra was carried out on all patients with this clinical condition , reserving dsa to a mere 4% of cases , i.e. those with contraindications to mri . tuata in questo campo applicativo risulta comparabile ad un solo lavoro in letteratura [ 23 ] , mentre negli altri [ 14 , 24 ] si fa riferimento alle tariffe di angio - rm ed angiografia digitale e non ad una valutazione dei costi reali . 
vi sono soprattutto differenze operative che giustificano questa diversit , tra le altre il computo del costo del mantenimento del paziente sorvegliato per 34 ore in un letto predisposto nel servizio di radiologia dopo leffettuazione dellangiografia e il minimo coinvolgimento del medico radiologo ( stimato in soli 7 minuti ) per leffettuazione e la refertazione dellangio - rm . 
essi rappresentano una fotografia della situazione nella nostra struttura in un certo momento storico , ma evidente che in altre strutture i costi possono essere estremamente diversi , vuoi per il costo diverso delle apparecchiature utilizzate o semplicemente per diverse scelte organizzative che possono incidere ad esempio sui costi variabili ( per diversi materiali utilizzati ) o sui costi del personale , qualora ne sia previsto un diverso impiego . 
ci non toglie a nostro giudizio validit a tale analisi , ma sottolinea il suo valore non tanto per i dati grezzi di costo riportati quanto per il suggerimento di un modello facilmente applicabile in altre realt operative . ci pu quindi essere stimolo per analoghe valutazioni dei costi di queste due tecniche , eventualmente inserite anche in protocolli diagnostici pi articolati o in raffronto ad altre indagini , quale langio - tc . 
chiaro che unanalisi dei costi rappresenta solo un primo tassello per giungere ad unanalisi costo - efficacia , che consideri quindi da un lato i benefici diagnostici , includendo le ricadute terapeutiche , e dallaltro i costi biologici . 
lelevata accuratezza diagnostica dellangio - rm nella valutazione delle arterie degli arti inferiori un dato acquisito [ 111 ]  . non vi dubbio inoltre che , per quanto riguarda i costi biologici , langio - rm offre chiari vantaggi rispetto allangiografia , per lassenza di invasivit , lassenza di radiazioni ionizzanti e lutilizzo di un mezzo di contrasto paramagnetico , pi sicuro di un prodotto organo - iodato . 
violante1 1uos di angiografia e radiologia interventistica , ente ecclesiastico , ospedale regionale miulli , via maselli campagna , i - 70021 acquaviva delle fonti , bari , italy 2uo di chirurgia vascolare , clinica salus , brindisi , italy correspondence to : s . 
the contralateral approach allows greater control over the entire procedure , with a reduction in potential risks in relation to the saphenofemoral junction given that , unlike in the technique proposed by min et al . 
the tip of the laser is directed at all times towards the saphenous vein and never towards the femoral vethis more radical procedure offers a significant reduction in the possibility of relapse of varicose disease of the saphenofemoral junction . key words saphenous vein endovenous therapy laser riassunto obiettivo . 
la nostra tecnica prevede il cateterismo superselettivo , eseguito radioscopicamente , della vgs con accesso venoso controlaterale eseguendo il cross - over iliaco . si realizza quindi esame fleboscopico retrogrado , ma anche fleboscopia anterograda da una ago - cannula posizionata al dorso del piede . 
lapproccio controlaterale consente un maggior controllo di tutta la procedura con potenziali minori rischi operativi in corrispondenza della crosse safeno - femorale , in quanto la punta dello strumento , rispetto alla tecnica descritta in letteratura , appare sempre rivolta verso la safena e mai verso la vena femorale ; ne consegue maggiore radicalit con significativa riduzione anche di possibili varici recidive di crosse . parole chiave vena safena trattamento endovascolare laser introduction introduzione superficial venous insufficiency of the lower limbs has an incidence of 25% among women and 15% among men [ 1 ] and often appears with insufficiency of the great saphenous vein ( gsv ) and varicosities of the thigh and lower leg . 
the clinical presentation of severe insufficiency of both superficial and deep venous systems is much more complicated . according to the criteria proposed by hach [ 2 , 3 ] , varicose syndrome of the gsv is subdivided into four grades while the syndrome of the small saphenous vein ( ssv ) is subdilinsufficienza venosa superficiale degli arti inferiori presenta una incidenza del 25% nelle donne e del 15% negli uomini [ 1 ] e spesso si manifesta con linsufficienza della vena grande safena ( vgs ) e con le varici di coscia e di gamba . pi complesso appare , invece , il quadro clinico in corso di grave insufficienza sia del sistema venoso superficiale che profondo , che si estrinseca nella cosiddetta malattia ad elevata portata . 
second - grade truncal varicosity is characterised by valvular insufficiency of the gsv for a section approximately 15 cm from the junction up to the middle third of the thigh . 
both the lateral accessory vein and the suprapatellar superficial branch may be involved , with varicosities only of the thigh and the knee region [ 2 , 3 ]  . 
in this case , there may also be involvement of the may and cockett iiiii perforating veins , lateral perforators , and the boyd and sherman veins [ 2 , 3 ]  . 
the perforating veins involved in this case are the cockett iiiii and may perforators . the traditional surgical approach depends principally on this grading and involves surgical ligation of the saphenofemoral junction ( sfj ) with stripping of the gsv and exclusion of any branches , and revision and ligation of incompetent perforating veins [ 4 ]  . 
the most common surgical complications are haematoma , lesion of the saphenous nerve , infection and telangiectasis ; cases of arterial lesion and pulmonary embolism have also been reported [ 5 ]  . in recent years new , less invasive and totally endovascular techniques have been successfully used , namely radiofrequency [ 6 ] and laser [ 7 , 8 ]  . 
 [ 79 ] who perform photothermolysis of the gsv using a 810 - nm laser fibre . this technique , which we have defined as classic laser photothermolysis , involves the direct puncture under ultrasound ( us ) guidance of the gsv a little above the knee and the running the laser diode up to about 2 cm from the sfj , where it is activated and withdrawn up to the entrance , causing vessel photothermolysis . we present our experience with regard to the endovascular treatment of varicose insufficiency of the gsv using endovascular laser treatment , with a modified technique using a contralateral percutaneous venous approach . materials and methods between june 2003 and june 2004 , 52 patients ( 12 men and 40 women , age range 4075 ) underwent endovascular treatment with laser photothermolysis . 
the group included four patients with post - surgical relapse of the gsv , all of whom suffering from revascularisation of the lateral accessory vein . all patients were selected following a precise preliminary examination , including echo doppler analysis , which congradi , mentre quella della piccola safena ( vps ) in tre , in base allanatomia e alla sede dellinsufficienza [ 2 , 3 ]  . il primo grado molto prossimale essendo coinvolta solo la prima valvola con minimo interessamento tronculare ( 13 cm )  . 
in questo caso pu coesistere , in fase conclamata , anche linteressamento delle vene perforanti di cockett iii - ii , may , vene perforanti laterali , vene di boyd e sherman [ 2 , 3 ]  . 
la varicosi tronculare di iv grado o completa prevede linteressamento varicoso della vgs in toto e di tutti i possibili rami collaterali ; le vene perforanti pi frequentemente coinvolte , in questo caso , sono quelle di cockett iii - ii e di may [ 2 , 3 ] lapproccio tradizionale chirurgico dipende in gran parte da questa stadiazione e prevede la legatura chirurgica della crosse safenofemorale con lo stripping della vgs , esclusione delle eventuali ramificazioni con revisione e legatura di eventuali perforanti incontinenti [ 4 ]  . 
le complicanze chirurgiche pi frequenti sono caratterizzate dallematoma , dalla lesione del nervo safeno , ma anche da eventuali infezioni e teleangectasie ; sono stati descritti anche casi di lesioni arteriose ed embolia polmonare [ 5 ]  . negli ultimi anni sono state sperimentate con successo nuove tecniche meno invasive e totalmente endovascolari in riferimento alla radiofrequenza [ 6 ] ed al laser [ 7 , 8 ]  . 
in particolare , abbiamo rivolto la nostra attenzione ai lavori di min e di navarro [ 79 ] che eseguono la fototermolisi della vgs utilizzando una fibra laser da 810 ntale tecnica , che noi abbiamo definito come fototermolisi laser classica prevede la puntura diretta , sotto guida ecografica , della safena magna poco sopra il ginocchio , facendo scorrere la sonda laser da 810 nm sino a circa 2 cm dalla crosse safenofemorale , dove viene attivata e retratta sino allingresso causando la fototermolisi vasale . 
viene presentata lesperienza personale in merito al trattamento endovascolare dellinsufficienza varicosa della vgs mediante trattamento endovascolare laser , con tecnica modificata , mediante approccio venoso percutaneo controlaterale . materiali e metodi da giugno 2003 a giugno 2004 sono stati sottoposti a trattamento endovascolare con fototermolisi laser 52 pazienti di cui 12 uomini e 40 donne di et compresa tra 40 e 75 anni . tra questi pazienti sono state trattate , inoltre , quattro recidive post - chirurgia della vgs che presentavano tutte rivas . 
an 18to 20 - gauge needle cannula is inserted on the dorsum of the foot homolateral to the gsv to be treated , thus enabling venous mapping and monitoring of the procedure with a series of direct phlebographies generally two to three repeated injections with a portable angiograph ( philips bv300 ) and an angiographic injector ( flows of 25 cc of iopamiro , bracco , 300 at 3 ml / s )  . at this stage , the 600 - m laser fibre ( 15 - watt diode laser with a 810 - nm wavelength ) is inserted into the introducer and advanced until about 1 cm of it extends beyond the tip of the catheter . 
dopo cross - over iliaco si cateterizza la vena femorale comune dal lato da trattare e si procede al cateterismo superselettivo , per via retrograda , della vgs insufficiente con lausilio di una guida terumo 0 , 035 dritta da 260 cm , su cui si fa scorrere un catetere multipurpose 110 cm da 6f ( mp a1 cordis )  . 
a questo punto attraverso il catetere guida si inserisce la fibra laser da 600 micron ( laser 15 w a diodi , con lunghezza donda di 810 nm ) facendola sporgere 1 cm circa dalla punta del catetere . 
the fibre tip is directed upwards in the direction of the common femoral vein , thus requiring a safety distance of 2 cm from the saphenous ostium , with the possible recurrences from the free stump by collateral veins . 
after the iliac crossover , the fibre tip is at all times directed towards the great saphenous vein ( gsv ) , even during the final phase of the procedure . 
la punta della fibra rivolta in alto , in direzione della vena femorale comune ; ci comporta il limite di 2 cm di distanza di sicurezza dallostio safenico con possibili recidive dal moncone libero da parte delle collaterali . 
b crosse safeno - femorale tecnica modificata . la punta della fibra , dopo cross - over iliaco , sempre rivolta verso la grande safena , anche nella fase conclusiva della procedura . di conseguenza la fibra viene spenta esattamente in corrispondenza dellostio safenico . 
c visualisation of the superficial venous system with phlebographic examination performed with a needle cannula positioned on the dorsum of the foot , with visualisation of the pathological perforating veins ( arrow )  . 
c visualizzazione del sistema venoso superficiale di gamba mediante esame fleboscopico eseguito contestualmente con ago - cannula posizionata al dorso del piede con visualizzazione anche delle perforanti patologiche ( freccia )  . 
e dopo trattamento si osserva la completa occlusione della recidiva varicosa di crosse ( freccia )  . results risultati we successfully treated 52 patients using the modified technique without the advent of shortor long - term complications . 
il follow - up , che nel nostro gruppo di pazienti stato eseguito mediante valutazione clinica ed eco - doppler , ha mostrato ricanalizzazione nel 5 , 7% di pazienti a sei mesi e il 7 , 5% a un anno . discussion discussione in contrast to the technique presented by min et al . 
 [ 710 ] , our modified technique has the clear advantage of a better approach to the sfj in that the laser tip is always directed towards the gsv during the procedure and never towards the common femoral vein , as occurs in the classic technique . la tecnica modificata , rispetto a quella descritta da min et al . 
 [ 710 ] , presenta il notevole vantaggio di potersi approcciare meglio nei confronti della crosse safeno - femorale , in quanto , durante la procedura di fototermolisi laser , la punta laser sempre rivolta verso la vgs e mai in direzione della vena femorale comune come invece avviene durante la s . 
phlebographic examinations performed prior to and during photothermolysis enable not only identification with certainty of vessels responsible for relapse but also panoramic assessment of the general haemodynamics of the venous flows of the limb , thus enabling the laser tip to be guided with near absolute precision to the level of the venous segment to be treated . we observed no major complication in our series , apart from a case of ecchymosis at the site of photothermolysis accompanied by mild pain , which nonetheless cleared up in a few days . the use of 18 - mmhg elastic stockings for about 10 days resolved symptoms of pain in all cases . 
the percentage of recanalisation at 12 months in our series of patients using the new technique was lower ( 7.5% ) than case series of classic photothermolysis ( about 10% ) [ 9 , 10 ] but higher than consolidated surgical case series ( 3%6% ) [ 11 ]  . compared with surgery involving ligation and stripping of the gsv , photothermolysis is less invasive , better tolerated and , above all , without significant complications , both in our case series and in other studies . 
in special cases , in the presence of large , autonomous varicosities of the leg , combined treatment ( laser and phlebectomy ) may be indicated . conclusions this preliminary study demonstrates that the 810to 980 - nm laser is an excellent device for endovascular treatment of gsv insufficiency . 
use of fluoroscopy is necessary in order to perform superselective catheterisation of the gsv and to perform direct phlebographies to obtain precise vascular mapping . by using the laser fibre and particularly long angiographic guides , we were able to treat complex varicose syndromes ( hach stages iii and iv ) in which even deep perforating veins below the knee ( cockett , boyd and sherman ) were involved . 
with regard to post - surgical relapse of the gsv , we propose this laser technique as first choice . the higher percentage of post - laser relapse of the gsv ( 7.5% ) with respect to classic surgery could be attributable to our natural learning curve , as this occurred in our first group tecnica classica . 
ci consente una maggiore radicalit nei confronti della crosse stessa e sue collaterali , minor rischio di trombosi accidentale della vena femorale comune e maggiore possibilit di eradicare eventuali collaterali , anche sottogenicolari , in casi di insufficienza di iii e iv tipo di hach , risultando pi agevole anche la revisione di eventuali vene perforanti di coscia . la procedura endovascolare laser da noi proposta pu diventare il trattamento di scelta per ci che concerne le recidive chirurgiche di coscia a livello della crosse safeno - femorale , laddove un reintervento potrebbe esser gravato da un maggior rischio di complicanze . 
lesame fleboscopico preliminare , e in corso di fototermolisi , permette non solo di individuare con certezza gli assi venosi responsabili della recidiva , ma anche di valutare panoramicamente lemodinamica generale dei flussi venosi dellarto , in modo da guidare con precisione pressoch assoluta la punta della fibra laser a livello del segmento venoso da trattare . 
non abbiamo osservato alcuna complicanza maggiore nella nostra serie personale , a parte una ecchimosi nella sede della fototermolisi accompagnata da una modesta sintomatologia algica peraltro regredita in pochi giorni . una terapia sintomatica associata ad uso di calze elastiche da 18 mmhg per circa 10 giorni stata sempre risolutiva . 
la percentuale di ricanalizzazione a 12 mesi nella nostra serie di pazienti , utilizzando questa nuova tecnica , stata comunque pi bassa ( 7 , 5% ) rispetto alle casistiche di fototermolisi classica ( circa il 10% ) [ 9 , 10 ] , ma superiore di qualche punto percentuale rispetto a casistiche chirurgiche consolidate ( circa il 3%6% ) [ 11 ]  . rispetto alla chirurgia , mediante legatura e stripping della vgs , la fototermolisi appare , per , meno invasiva , meglio tollerata e soprattutto priva di complicanze rilevanti sia nella nostra serie personale , sia in quella degli altri autori . 
in casi particolare in presenza di grosse varicosit autonome di gamba pu essere indicato il trattamento combinato ( laser e flebectomia )  . conclusioni da questa preliminare esperienza ci sembra di poter affermare che il laser da 810980 nm un ottimo strumento per il trattamento endovascolare dellinsufficienza della vgs . 
lausilio scopico , a nostro avviso , necessario per poter effettuare il cateterismo superselettivo della grande safena e per poter eseguire fleboscopie dirette ai fini di un preciso mappaggio vascolare . usufruendo di sonde laser e guide angiografiche particolarmente lunghe stato possibile anche il trattamento di sindromi varicose pi complesse ( iii e iv stadio di hach ) , in cui erano coinvolte anche vene perforanti sottofasciali sottogenicolari ( cockett , boyd e sherman )  . per ci che concerne le recidive della vgs post - chirurgia riteniamo oggi , questa tecnica laser , una indicazione di prima scelta . 
segnaliamo che la maggiore percentuale di recidive della vgs post - laser ( 7 , 5% in un anno ) , rispetto alla chirurgia classica , essendosi verificata nel primo gruppo di paziens . 
il costo della procedura in termini di apparecchiature , personale e materiali appare sostanzialmente contenuto rispetto al relativo drg ( 3500 euro circa ) , considerato anche che il peso maggiore della spesa sicuramente dovuto allacquisto dellangiografo , ma ci diventa irrilevante se tale procedura si aggiunge a tutta linterventistica endovascolare eseguita in una sala di radiologia interventistica . la tecnica classica non in grado , a nostro avviso , di trattare la vgs al di sotto del ginocchio a meno di un nuovo accesso percutaneo della vgs alla caviglia con tutte le difficolt che questo comporta . 
in recent years , the number of patients treated with evar has steadily risen as a result of increased physician experience , availability of new and more versatile devices and improvements in noninvasive imaging techniques . 
sono stati valutati retrospettivamente tutti gli esami angio - tc eseguiti dal gennaio 2002 al giugno 2003 , presso il nostro dipartimento di radiodiagnostica , in 182 pazienti con sospetto aneurisma dellaorta addominale . 
su un totale di 182 pazienti con sospetto aneurisma dellaorta addominale sottoposti ad esame angio - tc , previa valutazione combinata radiologica - chirurgica , stata posta lindicazione al trattamento chirurgico o endovascolare in 130 pazienti ( 71 , 4% )  . 
si posta lindicazione al trattamento , endovascolare in 51 pazienti ( 39 , 3% , gruppo a ) e chirurgico in 79 pazienti ( 60 , 7% , gruppo b )  . 
negli ultimi anni il numero di pazienti sottoposti a tale trattamento in continuo aumento , in rapporto sia alla crescente esperienza degli operatori che alla disponibilit di protesi pi versatili , sia al miglioramento di metodiche di imaging vascolare non invasive . 
the natural history of the aneurysm involves progressive growth ( 4 mm / year ) until rupture , which is associated with high mortality rates ( 80%90% ) [ 3 ] and the risk of which increases with the size of the aneurysm sac [ 4 ]  . a less invasive alternative to open surgery has recently been devised that consists of positioning a covered stentgraft intraluminally under imaging guidance . 
the success of endovascular treatment , in terms of exclusion of the aneurysm and absence of perioperative and postoperative complications , is closely dependent on accurate selection of patients to ensure that only aneurysms with morphology meeting well - defined requirements are treated [ 57 ]  . 
on the other hand , indications for endovascular repair based on both clinical and radiological criteria are continuously evolving as a result of the growing experience of operators , who tend to use the procedure in an increasing number of patients , and the more versatile and usable models of stent - grafts now available . 
the imaging modality of reference in the evaluation and selection of patients for endovascular abdominal aortic aneurism repair ( evar ) is multislice computed tomography ( msct ) angiography , which allows detailed and accurate study of the abdominal aorta and visceral vessels . 
 the purpose of our study was to evaluate in a large population studied by ct angiography for abdominal aortic aneurysm the percentage of patients eligible for evar on the basis of clinical - radiological criteria and to identify the main reasons for exclusion from treatment . materials and methods population laneurisma dellaorta addominale rappresenta una patologia di notevole rilevanza clinica , con unincidenza stimata in 2040 casi / 100000 abitanti per anno ed inoltre responsabile dell1 , 7% delle morti in soggetti tra 65 e 74 anni [ 1 , 2 ]  . la storia naturale dellaneurisma prevede un suo progressivo accrescimento ( 4 mm / anno ) sino alla rottura , che si associa ad unelevata percentuale di mortalit ( 80%90% ) [ 3 ] ed il cui rischio aumenta allaumentare delle dimensioni della sacca aneurismatica [ 4 ]  . negli ultimi anni stata messa a punto una tecnica alternativa alla chirurgia tradizionale , meno invasiva , che consiste nel posizionamento imaging - guidato per via endoluminale di uno stent - graft ricoperto , che ha mostrato risultati estremamente soddisfacenti . 
il successo del trattamento endovascolare , in termini di assenza di complicanze perie post - operatorie e , soprattutto , di esclusione dellaneurisma , strettamente correlato ad una accurata selezione dei pazienti al fine di trattare esclusivamente i casi nei quali le caratteristiche morfologiche dellaneurisma siano perfettamente rispondenti ad indicazioni ben codificate [ 57 ]  . 
daltra parte , le indicazioni al trattamento endovascolare , basate su criteri sia clinici che radiologici , sono in continua evoluzione , sia per la crescente esperienza degli operatori , che tendono a trattare con questa procedura una quota sempre maggiore di pazienti , sia per la disponibilit di nuovi modelli di endoprotesi con migliori caratteristiche di versatilit ed applicabilit . 
la metodica di riferimento nella valutazione e selezione dei pazienti candidati al trattamento endovascolare rappresentata dallangio - tc con tecnica multistrato , che consente una dettagliata ed accurata analisi dellaorta addominale e dei vasi viscerali . gli obiettivi del nostro lavoro sono stati quelli di identificare , in unampia popolazione sottoposta ad esame angiotc per aneurisma dellaorta addominale , la percentuale di pazienti candidati al trattamento endovascolare sulla base di criteri clinico - radiologici e di individuare le principali cause di esclusione a tale trattamento . the study involved 182 consecutive patients ( 121 men and 61 women ; mean age : 69.9 years ; age range : 5992 years ) who underwent ct angiography of the abdominal aorta for assessment of aortic aneurysm based on findings of a preliminary colour doppler ultrasound ( us ) study . materiali e metodi popolazione ct angiography ct angiography was carried out with the multislice technique ( somatom plus 4 volume zoom , siemens , erlangen , germany ) before and during infusion of a 120 - ml bolus of contrast medium ( 300 mgi / ml ; 3 ml / s flow rate )  . 
precontrast acquisition was performed with the following parameters : collimation 4x2.5 mm , pitch 6 , gantry rotation 0.5 s , slice thickness and reconstruction interval 5 mm , field of view 240 mm on average and volume of interest from d12 to the pubic symphysis . 
postcontrast acquisition was carried out with collimation 4x1 mm , sono stati inclusi 182 pazienti consecutivi ( 121 maschi e 61 femmine ; et media : 69 , 9 anni ; range et : 5992 anni ) sottoposti presso il nostro dipartimento di radiodiagnostica ad esame angio - tc dellaorta addominale per patologia aneurismatica aortica , su indicazione di un preliminare studio mediante eco - color - doppler . esame angio - tc lesame angio - tc stato eseguito con tecnica multistrato ( somatom plus 4 volume zoom , siemens , erlangen , germania ) prima e durante infusione a bolo di 120 ml di mdc ( 300 mgi / ml ; flusso 3 ml / s )  . 
lacquisizione senza somministraziopitch 6 , gantry rotation 0.5 s , slice thickness 1.25 mm , and reconstruction interval 1 mthe volume of interest extended from a plane passing through the celiac trunk to a plane through the common femoral arteries , with a mean acquisition time of 25 s . 
scan delay for each patient was determined by using an automatic bolus tracking system ( care bolus , siemens ) and defining a region of interest ( roi ) in the suprarenal abdominal aorta . evaluation criteria indication for treatment ( surgical or endovascular ) was decided upon by a team of vascular surgeons and interventional radiologists on the basis of clinical and morphological - dimensional data of the aneurysm provided by ct angiography following the italian transfemoral endovascular aneurysm management ( team ) guidelines produced by italian medical radiology society ( sirm ) vascular and interventional radiology study group [ 8 ]  . 
in particular , inclusion criteria used for endovascular repair were : age 65 years , aneurysm sac diameter < 7 cm , proximal neck length 15 mm , proximal neck diameter < 30 mm , proximal neck angulation > 120 , proximal neck with wall calcification extending to less than half of its circumference without significant thrombus apposition , iliac artery angulation > 90 ( < 90 without diffuse calcification ) and external iliac artery diameter > 7 mm and < 14 mendovascular treatment was also indicated for patients at high risk for surgery on the basis of the following criteria : age 80 years , diabetes mellitus , serious cardiac conditions ( severe coronary heart disease and / or marked ventricular function alterations ) , recent acute myocardial infarction ( ami ) , chronic lung disease , impaired kidney function ( creatinine > 2.0 mg / dl ) , hostile abdomen , american society of anesthesiologists ( asa ) iii and iv and obesity [ body mass index ( bmi ) > 30 ] [ 914 ]  . 
absolute contraindications to endovascular repair were : aneurysm involving both iliac arteries , or a hypogastric artery in the case of contralateral occlusion , marfan syndrome or acute inflammatory aaa . 
patients who underwent endovascular repair were followed up by ct angiography at 1 , 6 , 12 and 18 months in order to assess technical success and rate of intra - , periand postprocedural complications in the short and intermediate tercomplication rate was compared with the rate reported in the recent literature in order to justify and validate our inclusion rate . results out of a total of 182 patients studied by ct angiography of the abdominal aorta , 52 ( 28.6% ) were excluded from both surgical and endovascular treatment owing to the presence of an aneurysm with a maximum axial diameter < 44.5 cm without complications or because of normal caliber of the abdominal aorta . 
in the remaining 130 patients ( 71.4% ) , endovascular repair was indicated in 51 ( 39.3% , group a ) and open surgery in the remaining 79 ( 60.7% , group b )  . 
la durata media dellacquisizione stata di 12 s . lacquisizione con mdc stata eseguita con collimazione di 4x1 mm , pitch 6 , velocit di rotazione del sistema tubo radiogeno - detettori di 0 , 5 s , spessore dello strato di 1 , 25 mm ed intervallo di ricostruzione di 1 mil voi stato esteso da un piano passante per il tripode celiaco sino ad un piano passante per le arterie femorali comuni , con un tempo di acquisizione medio di 25 s . 
il ritardo di scansione stato individuato per ogni paziente mediante un sistema automatico di bolus tracking ( care bolus , siemens ) e posizionamento di una ragione di interesse ( roi ) in aorta addominale soprarenale . criteri di valutazione lindicazione al trattamento ( chirurgico o endovascolare ) stata posta da unequipe mista di chirurghi vascolari e radiologi interventisti considerando i criteri clinici e morfo - dimensionali dellaneurisma , desumibili dallesame angio - tc , sulla base delle linee giuda proposte dal team ( transfemoral endovascular aneurysm management ) italiano , a cura della sezione di studio di radiologia vascolare ed interventistica della sirm [ 8 ]  . 
colletto prossimale < 15 mm ; escluso dal trattamento endovascolare . risultati su un totale di 182 pazienti , sottoposti ad angio - tc dellaorta addominale , 52 pazienti ( 28 , 6% ) sono stati esclusi sia dal trattamento chirurgico che da quello endovascolare o per presenza di aneurisma con diametro assiale massimo < 44 , 5 cm , in assenza di complicanze , o per normale calibro dellaorta addominale . 
nei restanti 130 pazienti ( 71 , 4% ) stata posta indicazione al trattamento , endovascolare in 51 pazienti ( 39 , 3% , gruppo a ) e chirurgico nei restanti 79 casi ( 60 , 7% , gruppo b )  . 
tali pazienti erano stati inizialmente esclusi dal trattamento endovascolare per motivi di et in 3 casi ( < 65 anni ) , per le dimensioni della sacca aneurismatica in 2 casi ( > 7 cm ) e per colletto prossimale corto in 11 casi ( 1 paziente : < 0 , 5 cm ; 4 pazienti : 0 , 51 cm ; 6 pazienti : 11 , 5 cm )  . 
non si sono registrate significative complicanze durante la permanenza in ospedale tali da richiedere ulteriori trattamenti medico - chirurgici o endovascolari . follow - up il follow - up con controlli periodici angio - tc ad 1 , 6 , 12 e 18 mesi stato completato in 49 / 51 pazienti : 1 paziente deceduto per infarto acuto del miocardio ( ima ) entro 30 giorni dalla procedura ed 1 paziente che aveva sviluppato una paraplegia post - procedura si presentato solo al primo controllo . risultati a breve termine ( < 6 mesi ) il tasso di reintervento a distanza , conversione chirurgica e migrazione caudale della protesi risultato pari allo 0% . 
72 anni ( f ) : angio - tc , immagine assiale ( a ) e 3d ( b )  . aneurisma sacciforme dellaorta addominale sottorenale escluso per le dimensioni della sacca aneurismatica ( > 7 cm )  . short - term results ( < 6 months ) the rate of reintervention , surgical conversion and caudal migration of the stent - graft was 0% . 
endoleaks were observed in 11 patients ( 21.5% ) : three distal , type i ( 5.9% ) ; seven type ii ( 17% ) and one type iii caused by altered junctable 1 endovascular abdominal aortic aneurysm repair ( evar ) exclusion criteria unfavourable anatomy of the infrarenal neck length < 1.5 cm diameter > 30 mm tortuous course ( < 120 ) significant calcific atheromatosis parietal thrombus apposition age < 65 years aneurysm sac diameter > 7 cm tortuous / dilated iliac axis patient refusal tabella 1 cause di esclusione evar anatomia ostile del colletto sottorenale lunghezza < 1 , 5 cm diametro > 30 mm decorso tortuoso ( < 120 ) presenza di significativa ateromasia calcifica apposizione parietale trombotica et < 65 anni diametro della sacca aneurismatica > 7 cm asse iliaco tortuoso / ectasico rifiuto del paziente 51.9% ( 41 / 79 ) 24.1% ( 19 / 79 ) 6.3% ( 5 / 79 ) 13.9% ( 11 / 79 ) 7.6% ( 6 / 79 ) 21.5% ( 17 / 79 ) 16.4% ( 13 / 79 ) 7.6% ( 6 / 79 ) 2.5% ( 2 / 79 ) 51 , 9% ( 41 / 79 ) 24 , 1% ( 19 / 79 ) 6 , 3% ( 5 / 79 ) 13 , 9% ( 11 / 79 ) 7 , 6% ( 6 / 79 ) 21 , 5% ( 17 / 79 ) 16 , 4% ( 13 / 79 ) 7 , 6% ( 6 / 79 ) 2 , 5% ( 2 / 79 ) di tipo iii da alterata giunzione tra le branche protesiche ( 2% )  . 
nei primi 6 mesi di osservazione non si sono verificate in alcun paziente significative modificazioni delle dimensioni della sacca aneurismatica , nemmeno nel paziente in cui era comparso endoleak di tipo iii . risultati a medio termine ( 18 mesi ) nel follow - up a 18 mesi 7 / 49 pazienti hanno presentato un endoleak : di tipo i distale ( n = 1 , 2% ) e di tipo ii ( n = 6 , 12 , 2% )  . due di questi 7 endoleak non erano presenti nei precedenti controlli . due endoleak di tipo i e 3 endoleak di tipo ii si sono risolti spontaneamente . 
le dimensioni della sacca aneurismatica esclusa sono diminuite di pi di 5 mm in 19 pazienti ( 38 , 8% ) mentre sono rimaste invariate in 29 pazienti ( 59 , 2% )  . 
in 1 solo paziente si registrato un aumento della sacca aneurismatica ( > 4 mm , 2% ) , sostenuto da un endoleak di tipo i distale . tale complicanza stata corretta con la tecnica del bending , che consiste nel posizionamento chirurgico di una fascia protesica attorno allarteria in corrispondenza dellestremit distale della branca iliaca in modo da favorire il miglior ancoraggio di questultima allarteria nativa , eliminando cos la fonte di riperfusione . 
in one patient only did the aneurysm sac increase in size ( > 4 mm , 2% ) , which was the result of a distal type - i endoleak . 
this complication was corrected using the banding technique , which involves surgically placing a prosthetic band around the artery in correspondence with the distal end of the iliac branch so as to improve fixation to the native artery and remove the source of reperfusion . 
none of the patients with type - ii endoleak showed increase in size of the excluded aneurysm sac , and none experienced caudal migration of the stent - graft or the need for surgical conversion with removal of the stent - graft . reintervention rate was 2% ( 1 / 49 : banding for distal type - i endoleak )  . follow - up of the subgroup of patients with high surgical risk in the subgroup of 16 high - surgical - risk patients , one died of ami within 30 days of the procedure ( 6.25% ) and four ( 25% ) developed type - ii endoleaks , of which two resolved spontaneously within 6 months and two remained unchanged throughout the follow - up period . 
the rate of caudal migration of the stent - graft at 12 months is between 0% and 8% depending on the kind of endograft used , with a higher rate for first - generation devices with infrarenal attachment [ 28 , 29 ]  . 
reintervention rate is higher than 15% ( in studies with follow - up > 2 years ) , with a rate of 16% in becquemins study [ 30 ] involving 125 patients followed up for 18 months [ 25 , 26 ]  . 
over the past few years , the use of endovascular repair of abdominal aortic aneurysms has increased progressively , and the technique now represents an alternative that is less invasive and burdened by fewer comfollow - up sottogruppo pazienti ad alto rischio chirurgico nel sottogruppo dei 16 pazienti ad elevato rischio chirurgico si registrato 1 decesso per ima entro 30 giorni dalla procedura ( 6 , 25% ) e la comparsa di endoleak in 4 pazienti ( 25% ) , tutti di tipo ii , di cui 2 risoltisi spontaneamente entro 6 mesi e 2 immodificati in tutti i controlli . 
in nessun caso si osservato un leak di tipo i , n migrazione caudale della protesi . discussione secondo i dati della letteratura recente , il trattamento endovascolare degli aneurismi dellaorta addominale gravato da un tasso di mortalit e morbilit entro 30 giorni pari allo 02 , 6% e al 3 , 217% , rispettivamente [ 1523 ]  . 
la percentuale di conversione chirurgica compresa tra l1 , 4% e il 6 , 3% con un tasso di rottura aortica tardiva > 0 , 3% ; questultima risultata pari allo 0 , 4% e al 2 , 3% in lavori con follow - up inferiori al nostro ( rispettivamente 12 e 17 mesi ) [ 5 , 2427 ]  . 
il tasso di migrazione caudale dellendoprotesi entro 12 mesi dallimpianto compreso tra lo 0% e l8% , in base al tipo di protesi utilizzata , con maggior percentuale per le protesi di i generazione ad aggancio sottorenale [ 28 , 29 ]  . 
il tasso di reintervento a distanza , infine , risulta superiore al 15% ( in studi con follow - up > 2 anni ) con una percentuale pari al 16% nello studio di becquenim [ 30 ] eseguito su 125 pazienti con un follow - up di 18 mesi [ 25 , 26 ]  . negli ultimi anni si assistito ad una sempre maggiore diffusione del trattamento endovascolare dellaneurisma dellaorta addominale , che rappresenta oggi una terapia alternativa , meno invasiva e gravata da minori complicanze rispetto alla chirurgia . 
questa tendenza allaumento di procedure endovascolari da correlarsi principalmente alla crescente esperienza degli operatori e alla disponibilit di endoprotesi con maggiori caratteristiche di versatilit ed applicabilit quali : aggancio soprarenale , maggior diametro sia del corpo principale che delle branche iliache , minor profilo . 
inoltre , lintroduzione della tc spirale multistrato permette di ottenere unanalisi sempre pi dettagliata ed accurata dellaorta addominale e dei vasi viscerali [ 3137 ] , tale da consentire una corretta selezione dei pazienti e delle caratteristiche del device pi adatto caso per caso . 
alcuni autori pongono come limite il 25%30% di tutti gli aneurismi dellaorta addominale trattabili mentre allestremo opposto altri dati della letteratura riportano la possibilit di estendere tale trattamento sino all80% dei casi [ 7 , 38 ]  . 
the increasing use of endovascular procedures is mainly related to the growing experience of operators and the availability of more versatile and usable endografts , characterised by : suprarenal attachment , increased diameter of both the main body and the iliac branches and reduced profile . 
furthermore , the introduction of msct has resulted in increasingly detailed and accurate studies of the abdominal aorta and visceral vessels [ 3137 ] , allowing the correct selection of patients and of the most appropriate device for each case . 
despite the many proposals of well - defined inclusion criteria , no common data exist as to the true percentage of candidates to endovascular repair . some authors consider 25%30% of all treatable abdominal aortic aneurysms to be eligible whereas others report that up to 80% can be treated [ 7 , 38 ]  . 
studies with high rates of inclusion show definitely higher complication rates and a higher incidence of endograft migration , increased size of aneurysm sac and late reintervention / surgical conversion [ 34 ]  . 
of our population of 182 patients , only 39.3% were candidates for endovascular repair on the basis of clinical - radiological criteria and following selection by a team of interventional radiologists and vascular surgeons . correctness of this selection was validated by a short - and mid - term complication rate equal to or less than reported in the recent literature , with a technical success of 100% . 
furthermore , in 98% of patients , the excluded aneurysm sac had shrunk or remained unchanged at the 18 - month follow - up , therefore reducing the risk of rupture . 
in agreement with the literature [ 3941 ] , the most common criterion for exclusion , observed in 51% of patients with treatable abdominal aortic aneurysm , was unfavourable anatomy of the proximal neck , based on such morphostructural characteristics as length , diameter , course and the existence of parietal thrombus appositions and coarse calcification . 
the recent introduction of endografts with suprarenal attachment has certainly allowed indications to be extended to patients with more unfavourable proximal necks while maintaining an adequate safety margin for the procedure . 
in the group of patients at high risk for surgery , 11 had a < 1.5 - cm - long proximal neck . none of those patients , all treated with grafts with suprarenal attachment , recorded an increase in intra - , perior postoperative complications , caudal migration of the endograft or type - i leaks . 
verhoeven [ 42 ] and greenberg [ 43 ] reported their positive initial experience with this kind of endograft used in 18 high - risk patients with unfavourable necks ( length < 15 mm ) ( absence of intraand per - operative mortality and of proximal type - i endoleaks ) and in 32 patients deened unacceptable candidates for open surgical repair with proximal neck length < 10 mm ( 22 patients ) or < 15 mm with a compromising morphology ( 10 patients ) ( one death and one type - i endoleak )  . 
however , before routine use is proposed , these innovative stent - grafts need to be tested in studies conducted on larger patient populations and with intermediateand long - term follow - up . exclusion due to age ( 21.5% of patients ) is related to etha.r. 
la correttezza di tale selezione stata validata dal tasso di complicanze a breve - medio termine risultato uguale o inferiore rispetto ai dati della letteratura recente , con un successo tecnico pari al 100% . 
inoltre nel 98% dei pazienti la sacca aneurismatica esclusa risultata ridotta o immodificata al controllo a 18 mesi , con conseguente riduzione del rischio di rottura . in accordo con i dati della letteratura [ 3941 ] , nella nostra esperienza il criterio di esclusione pi comune , osservato nel 51% dei pazienti con aneurisma dellaorta addominale da trattare , risultato essere lanatomia ostile del colletto prossimale , basata su caratteristiche morfo - strutturali , quali la lunghezza , il calibro , il decorso e la presenza di apposizioni parietali trombotiche e di grossolane calcificazioni . 
lintroduzione negli ultimi anni di endoprotesi con aggancio soprarenale ha sicuramente consentito di ampliare le indicazioni anche in pazienti con colletto prossimale pi sfavorevole , pur mantenendo un adeguato margine di sicurezza della procedura . nel gruppo di pazienti considerati ad alto rischio chirurgico , 11 presentavano un colletto prossimale di lunghezza < 1 , 5 cin questi pazienti , trattati tutti con protesi ad aggancio soprarenale , non si registrato un aumento delle complicanze intra - , perio post - procedurali , in assenza di migrazione caudale della protesi o di leak di tipo i . 
verhoeven [ 42 ] e greenberg [ 43 ] hanno riportato una loro positiva ed iniziale esperienza con questo tipo di protesi impiantate rispettivamente in 18 pazienti ad elevato rischio chirurgico con colletto ostile ( lunghezza < 15 mm ) ( assenza di mortalit intra - perioperatoria e di endoleak di tipo i prossimale ) e in 32 pazienti ( 1 decesso ed 1 endoleak di tipo i )  . 
tali innovative endoprotesi , tuttavia , per essere utilizzate routinariamente necessitano di trials su pi ampie popolazioni di pazienti e di follow - up a medio - lungo termine . il criterio di esclusione basato sullet anagrafica ( 21 , 5% dei pazienti ) legato a motivi etici in quanto ad oggi mancano follow - up a lungo termine sufficienti per verificare levoluzione e lo stato dellendoprotesi nel tempo e quindi quantizzare il rischio di lesioni che necessitano di un nuovo trattamento / conversione chirurgica a distanza : difetti strutturali , quali rottura delle maglie metalliche e dei punti di sutura , soluzioni di continuo del tessuto o distacco di componenti modulari , deformazioni del device con inginocchiamento e trombosi , migrazione caudale per alterazione dellanatomia dellaorta od inadeguatezza dei sistemi di ancoraggio . 
tale dato sembra avvalorato dai risultati riportati in letteratura in casistiche con follow - up a lungo termine , con un tasso di reintervento a distanza pari a circa il 49% in follow - up superiori a 5 anni e un tasso di migrazione caudaa.r. 
these data seem to be supported by the results of case series with long - term follow - up , with a late reintervention rate of around 49% in follow - up periods longer than 5 years and a caudal migration rate between 29% and 50% with the use of first - generation stent - grafts associated with possible structural damage linked to the use of firstand second - generation endografts . 
this criterion for exclusion is justified by the literature , which indicates that treatment of large abdominal aortic aneurysms ( > 7 cm ) might prove ineffective , even in cases meeting the remaining morphological inclusion criteria , owing to presumed inevitable evolution of parietal disease . 
data from the european collaborators on stent - graft techniques for abdominal aortic aneurysm ( eurostar ) data registry centre , based on a population of 4392 patients treated by stent - graft placement because of abdominal aortic aneurysms with a follow - up period of 6 years , show a higher mortality rate and a higher risk of late rupture for aneurysms larger than 6.5 cm before treatment , with a consequent need for surgical conversion [ 5 , 44 ]  . 
in the study by arko et al . [ 39 ] , 15% of large aneurysms showed significant neck angulation at follow - up whereas 27% of cases exhibited reduced neck length , with a potential greater risk of caudal migration of the stent - grain 7.6% of our patients , exclusion was due to morphological characteristics of the iliac axis : excessive diameter , tortuosity , significant thrombus apposition and coarse wall calcification . 
 in conclusion , our experience indicates that careful and accurate selection of patients made by a team of interventional radiologists and vascular surgeons and the use of adequate clinical - radiological criteria permits the placement of stent - grafts in nearly 40% of patients with abdominal aortic aneurysms , with acceptable complication rates in terms of type and severity . 
the presence of an unfavourable neck proved to be the most common criterion for exclusion from endovascular repair . undoubtedly , neck morphology is the most challenging technological problem , as the possibility of using specially shaped stent - grafts will increase the number of patients with abdominal aortic aneurysms eligible for endovascular repair . 
 le variabile tra il 29% ed il 50% con lutilizzo di protesi di prima generazione associato alla presenza di possibili danni strutturali connessi con lutilizzo di protesi di prima e seconda generazione . il 16 , 4% dei pazienti , sottoposti a trattamento chirurgico tradizionale dai chirurghi vascolari del nostro gruppo , stato escluso dal trattamento endovascolare per le eccessive dimensioni della sacca aneurismatica . 
tale criterio di esclusione appare giustificato dai dati della letteratura secondo i quali il trattamento di aneurismi dellaorta addominale di dimensioni cospicue ( > 7 cm ) potrebbe risultare inefficace anche nei casi in cui fossero rispettati e presenti i restanti criteri morfologici di inclusione , per una presunta ineluttabile evolutivit della malattia di parete . 
i dati delleurostar ( eurostar data registry center ) , basati su una popolazione di 4392 pazienti sottoposti a posizionamento di endoprotesi per aneurisma dellaorta addominale con un follow - up di 6 anni , riportano per gli aneurismi di dimensioni pre - trattamento superiori a 6 , 5 cm un maggior tasso di mortalit ed un maggior rischio di rottura della sacca aneurismatica a distanza , con conseguente necessit di conversione chirurgica [ 5 , 44 ]  . nello studio di arko et al . 
 [ 39 ] il 15% degli aneurismi di grosse dimensioni hanno mostrato nel follow - up una significativa angolazione del colletto , mentre una riduzione della sua lunghezza si registrata nel 27% dei casi , con conseguente maggior rischio potenziale di migrazione caudale della protesi . 
nel 2% dei casi , infine , si registrato il rifiuto del paziente a sottoporsi a questa relativamente nuova procedura . in conclusione , la nostra esperienza ci consente di affermare che , attraverso unattenta ed accurata selezione dei pazienti eseguita da unequipe mista di radiologi interventisti e chirurghi vascolari e utilizzando adeguati criteri clinico - radiologici , il posizionamento di endoprotesi pu essere eseguito in quasi il 40% dei pazienti con aneurisma dellaorta addominale , con unaspettativa di complicanze accettabile per entit e gravit . un rispetto rigoroso dei criteri di inclusione rappresenta il presupposto fondamentale al fine di ottenere un elevato successo tecnico della procedura e di ridurre il tasso di complicanze a breve - medio termine . 
chest us was found to be a valuable diagnostic tool in pneumothorax diagnosis , with diagnostic effectiveness well beyond x - rays and similar to ct . key words ultrasound utilisation - thorax , us comparative study ultrasound pneumothorax riassunto obiettivo . 
sono stati esaminati con lecografia 184 pazienti consecutivi ( 130 maschi e 54 femmine ) , di et compresa tra 26 ed 82 anni , sottoposti ad agobiopsia polmonare transtoracica . 
lecografia del torace si dimostrata un valido strumento per la diagnosi di pneumotorace , con una accuratezza diagnostica superiore a quella della radiologia tradizionale . parole chiave ecografia ecografia toracica studio ecografico comparativo pneumotorace introduction introduzione pneumothorax represents a very important diagnostic problem , above all in emergency medicine and intensive care settings [ 1 ]  . 
on the one hand , excessive suspicion may sometimes be due to equivocal clinical or radiographic findings ; on the other , this condition may be missed , with dangerous treatment delays . the reported sensitivity of conventional radiography in the diagnosis of pneumothorax is between 50% and 70% , depending both on its severity and the projection method used [ 2 ]  . computed tomography ( ct ) , which is considered the gold standard in the diagnosis of pneumothorax , is not readily available in centres located far from hospitals ; moreover , the transfer and stay of critical patients in the ct service cause several clinical and management problems , above all lo pneumotorace rappresenta un problema diagnostico non indifferente , soprattutto in determinati contesti clinici quali la medicina durgenza e la terapia intensiva [ 1 ]  . 
se da un lato il sospetto talvolta evocato per eccesso sulla base di reperti clinici o radiografici equivoci , altre volte tale patologia pu risultare misconosciuta , con pericoloso ritardo terapeutico . la sensibilit della radiografia tradizionale nella diagnosi di pneumotorace stimata , secondo studi eseguiti nel corso degli anni , tra il 50% ed il 70% , in relazione sia allentit di questultimo , sia al metodo di proiezione usato [ 2 ]  . 
la tc , ritenuta il gold standard nella diagnosi di pneumotorace , non rapidamente disponibile in sedi lontane da strutture ospedaliere ; inoltre , il trasporto e la permanenza di pazienti in condizioni critiche al servizio tc crea notevoli difor emergency departments and resuscitation units , as well as high risks for patients . 
1a scansione ecografica longitudinale lungo la parete addominale anteriore ; la linea pleurica ( frecce ) ben riconoscibile come sottile banda iperecogena al di sotto delle strutture della parete toracica . 
le procedure agobioptiche sono state eseguite , a seconda delle caratteristiche della lesione bersaglio e delle esigenze diagnostiche , con ago sottile di chiba da 21 g , con ago spinale da 18 g o con ago tranciante da 18 g . 
alle scansioni tc preliminari , eseguite a scopo di centratura , nessun paziente risultava affetto da preesistente pneumotorace . alla fine della procedura bioptica , ogni paziente stato sottoposto ad una scansione tc di controllo , per escludere la presenza di pneumotorace ; tale scansione stata utilizzata come esame di riferimento per la valutazione dei risultati dello studio . tutti gli esami ecografici sono stati eseguiti dallo stesso operatore , entro 15 minuti dal termine della biopsia , utilizzando lo stesso apparecchio ecografico ( siemens sonoline elegra ) con una sonda convex da 3 , 5 mhz . 
gli artefatti a coda di cometa , bande iperecogene originanti dalla linea pleurica e dirette verso la profondit della scansione , escludono la presenza di pneumotorace al pari dello scorrimento polmonare . materials and methods between march 2002 and january 2005 , 184 consecutive patients ( 130 men and 54 women ) aged 2682 ( mean 66 ) years who had just undergone ct - guided percutaneous lung biopsy were studied by chest us . 
needle - biopsy procedures were performed , depending on lesion characteristics and diagnostic needs , with a 21 - gauge chiba needle , an 18 - gauge spinal needle or an 18 - gauge cutting needle . 
this scan was used as the reference standard to evaluate the results of our study . all us examinations were performed within 15 min of the biopsy by the same operator using the same sonographic fig . 
in the absence of either sign , we ran the probe over the intercostal spaces to look for the lung - point sign to lalgoritmo diagnostico , utilizzato per definire la diagnosi ecografica di pnx rappresentato nella figura 5 . 
in assenza di entrambi i segni , scorrendo con la sonda lungo gli spazi intercostali , si poi ricercato il segno del punto polmonare , al fine di confermare la diagnosi . in presenza di punto polmonare , stata posta diagnosi di pneumotorace lieve , moderato o grave a seconda del punto di proiezione del segno ( vedi sotto )  . 
lo pneumotorace stato arbitrariamente classificato in : lieve : punto polmonare situato medialmente allascellare grave : punto polmonare situato posteriormente allascellare posteriore ; completo ( sospetto ) : punto polmonare assente . infine , ogni paziente stato sottoposto ad esame radiografico del torace da supino : tutti i radiogrammi sono stati valutati da un terzo radiologo per la ricerca dei segni di pneumotorace , anche in tal caso allinsaputa dei risultati di tc ed esame ecografico . 
i risultati dellesame ecografico e di quello radiografico sono stati confrontati tra di loro e quindi con la routinaria scansione tc post - biopsia , considerata quale gold standard . risultati tutti gli esami ecografici eseguiti sono risultati tecnicamente soddisfacenti , e pertanto ritenuti diagnostici ai fini della g . 
if the lung - point sign was detected , a diagnosis of mild , moderate or severe pneumothorax was made depending on the point of projection of the sign ( see below )  . 
pneumothorax was arbitrarily classified mild : lung point located medial to the anterior axillary line moderate : lung point located between the anterior and mesevere : lung point located posterior to the posterior axillary dial axillary lines line complete ( suspected ) : absent lung point finally , each patient underwent chest radiography in the supine position . all radiograms were checked for signs of pneumothorax by a third radiologist blinded to ct results and us examinations . 
results of sonographic and radiographic examinations were compared with one another as well as with the routine postbiopsy ct scan , considered the gold standard . results all sonographic examinations were technically satisfactory and therefore regarded as diagnostic for the detection of pneumothorax . 
the average time required for chest sonography was about 4 mconsidering that normal lung sliding was clearly identified in all 184 healthy hemithoraces ( not considered in the statistical analysis ) , results of sonographic examinations of the 184 hemithoraces that underwent biopsy compared with those of chest x - ray and ct , can be summarised as follows : in 139 hemithoraces , the lung - sliding sign was clearly recognised ; in one case , lung sliding was not clearly recognised but comet - tail artefacts were present ; in all these cases ( 140 ) , the diagnosis of pneumothorax could therefore be excluded . 
in these cases , the search for the lung point sign yielded 28 lung points medial to the anterior axillary line and 15 between the anterior and medial axillary lines ; in one case , it was not recognised . us therefore enabled the diagnosis of 28 cases of mild pneumothorax and 15 of moderate pneumothorax ; in one case , massive pneumothorax was suspected and later confirmed by ct and radiography . at chest radiography , 19 pneumothoraces were recognised . 
according to the criteria described above ( see materials and methods ) , 30 were classified as mild , 15 as moderate and one as complete . the two cases of disagreement , both sonographic false negative results , were a thin anterior pneumothorax and a minimal posterior pneumothorax . according to these results , us demonstrated sensitivity of 95.65% , specificity of 100% and diagnostic accuracy of ricerca di pneumotorace . 
premesso che in tutti i 184 emitoraci sani ( non considerati a fini statistici ) stato chiaramente riconosciuto uno scorrimento pleurico quale segno di normalit , i risultati ottenuti dallesame ecografico dei 184 emitoraci sottoposti ad agobiopsia seguendo lalgoritmo diagnostico descritto , comparati con quelli di rx e tc , possono essere riassunti come segue : in 139 emitoraci esaminati , stato chiaramente riconosciuto lo scorrimento polmonare ; in 1 caso non stato riconosciuto con certezza lo scorrimento polmonare , ma erano presenti artefatti a coda di cometa ; in tutti questi casi ( 140 ) stata pertanto esclusa la diagnosi di pneumotorace . in 44 casi risultavano assenti sia lo scorrimento polmonare , sia gli artefatti a coda di cometa ed stata quindi posta diagnosi di pneumotorace . in tali ultimi stato ricercato il segno del punto polmonare , che risultato riconoscibile in 28 casi medialmente alla linea ascellare anteriore , in 15 tra ascellare anteriore e media , in 1 non stato riconosciuto . pertanto complessivamente sono stati diagnosticati con lecografia 28 pneumotoraci lievi , 15 pneumotoraci moderati ; in un caso stato posto il sospetto di pneumotorace massivo , confermato poi radiograficamente . allesame radiografico del torace , sono state riconosciute 19 falde di pneumotorace . al controllo tc post - bioptico , 46 pazienti ( 25% ) presentavano una falda di pneumotorace ; secondo i criteri sopra definiti ( vedi materiali e metodi ) , 30 sono stati classificati come lievi , 15 come moderati e 1 come completo . i due casi discordanti , entrambi falsi negativi ecografici , sono risultati una sottile falda anteriore e una minima falda di pneumotorace saccato posteriore . alla luce di tali risultati , lecografia ha dimostrato sensibilit pari a 95 , 65% , specificit pari a 100% , accuratezza diagnostica del 98 , 91% . 
il vpp risultato pari a 100% , e il vpn pari al 98 , 57 . pur considerando larbitrariet e lapprossimazione del metodo , vi comunque una concordanza totale tra us e tc nella quantificazione dellentit della falda di pneumotorace . lesame radiografico del torace eseguito a paziente supino ha mostrato una sensibilit del 42% . discussione i risultati esposti confermano la validit dellecografia nella diagnosi di pneumotorace . il principale vantaggio di questa metodica , oltre allinnocuit biologica ed al basso costo , quello di essere facilmente e prontamente disponibile direttamente al letto del paziente . per questo , essa risulta generalmente preziosa in tutte quelle situazioni ( medicina pre - ospedaliera , medicina durgenza , terapia intensiva , medicina aerospaziale ) nelle quali 98.91%. 
the main advantage of this modality , besides biological safety and inexpensiveness , is that it is readily available directly at the patients bedside . for these reasons , it proves invaluable in all situations ( prehospital medicine , emergency medicine , intensive care , aerospace medicine ) in which diagnosis with other modalities cannot be obtained rapidly or because of unavailability or lack of reliability . although sonography is traditionally considered a secondary modality in the study of the chest , new , less common indications are progressively being added to the few well - established ones ( study of chest - wall lesions , pleural effusions , peripheral parenchymal lesions )  . 
for these reasons , several emergency centres have been using chest sonography for years to supplement focused abdominal sonography for trauma ( fast ) in the search for haemothorax , haemopericardium , lung contusions and pneumothorax [ 17 ]  . several sonographic signs , which enable recognition of the presence of gas in the pleural cavity , have been identified and described . after the report by rantanen [ 3 ] published in a veterinary journal , wernecke et al . 
 [ 4 ] were the first to suggest the possibility of sonographic diagnosis of pneumothorax in humans based on the simultaneous absence of lung sliding and comet - tail artefacts ; the value of such signs was later confirmed by numerous other authors [ 515 ]  . the diagnostic algorithm chosen for this study is similar in many respects to the one proposed by lichtenstein et al . [ 12 ] , who reported high values of sensitivity ( 100% ) , ppv ( 100% ) and specificity ( 96.5% ) with use of the simultaneous absence of lung sliding and comet - tail artefacts as a criterion to exclude complete pneumothorax . the same authors reported the lung point sign to be reasonably sensitive ( 75% ) but highly specific ( 100% ) in the identification of the radio - occult pneumothorax . 
considering the distribution of pneumothorax [ 18 ] , we studied patients in the supine position , selecting the anteriormost portion of the anterior wall as the point of study . 
 [ 4 ] ad affermare la possibilit della diagnosi ecografica di pneumotorace nelluomo per la contemporanea assenza di scorrimento pleurico e di artefatti a coda di cometa ; la validit di tali segni stata successivamente confermata da numerosi altri autori [ 515 ]  . lalgoritmo diagnostico scelto per questo studio simile per molti aspetti a quello proposto da lichtenstein et al . [ 12 ] , il quale riferisce elevati valori di sensibilit ( 100% ) , vpn ( 100% ) e specificit ( 96 , 5% ) utilizzando la combinata assenza di scorrimento polmonare ed artefatti a coda di cometa come criterio di esclusione di pneumotorace completo ; lo stesso autore ha descritto successivamente nel punto polmonare un segno discretamente sensibile ( 75% ) ma altamente specifico ( 100% ) nellidentificazione delle falde di pneumotorace radio - occulte . considerando le modalit di distribuzione delle falde di pneumotorace [ 18 ] , il paziente stato esaminato in posizione supina , scegliendo quale sede di studio la parete anteriore nel punto pi antideclive . la popolazione di pazienti reclutati simile a quelle in precedenza proposte , in numeri pi esigui ( rispettivamente 29 e 97 ) , da goodman et al . 
tutti gli esami sono risultati diagnostici : infatti in nessuno dei nostri pazienti si sono verificate situazioni quali lesioni cutanee , bendaggi o altri presidi diagnostici o terapeutici ( elettrodi , drenaggi , etc ) , enfisema sottocutaneo , frammenti di proiettili , la cui presenza rende il pi delle volte inattendibile lindagine ecografica . 
la prevalenza di falde lievi ( 28 / 44 ) , quelle pi frequentemente radio - occulte , rappresenta un aspetto rilevante . la sensibilit globale dellecografia nellidentificare la presenza di falde di pneumotorace anche minime ( 95 , 65% ) si conferma nettamente superiore a quella della radiografia del torace ( 42% ) , in accordo con quanto precedentemente rilevato [ 10 , 14 , 15 , 17 ]  . 
it is precisely in such settings that chest us deserves to be proposed as a complementary , if not alternative , modality to chest radiography . the low sensitivity values of us reported by sistrom et al . 
 [ 15 ] ( 73% and 80% , respectively ) are at least partially ascribable to the method used , which involved deferred instead of real - time diagnoses . the discordant cases in our case series were two false negatives . 
in the first case , it was only a thin anterior pneumothorax , recognised at postbiopsy ct but not at the following us scan . considering its small size , we can assume that it had already been reabsorbed at the time of the us scan . 
the second discordant case was a limited posterior pneumothorax , obviously missed at the us scan , which was performed on the anterior surface only due to our methodological choice . the possibility of this error occurring has already been reported [ 4 ]  . 
in both cases , the following radiographs ( 4 h after biopsy ) were negative , and the patient did not require treatment . specificity and ppv ( 100% ) , although in line with those previously reported [ 13 , 14 ] , deserve some critical considerations . the relative homogeneity of the type of patients examined excluded many potential causes of diagnostic error . 
several situations exist , at least in theory , which can give rise to false positive results , thereby reducing diagnostic accuracy of the modality . previous studies have underlined the fact that lung sliding may be absent or difficult to recognise in cases of bullous emphysema [ 4 ] , paralysis of the phrenic nerve and pachypleuritis [ 7 ] , thereby leading to falsely positive diagnoses when absent lung sliding is considered sufficient for the diagnosis . moreover , this sign can be scarcely appreciable in the upper chest quadrants in normal patients as well [ 7 ]  . in all these cases , the presence of comet - tail artefacts originating from the pleural line is decisive for excluding pneumothorax . rienza personale sia nei precedenti contributi citati , si riferiscono al radiogramma eseguito esclusivamente in proiezione antero - posteriore a paziente supino . 
tale difetto di sensibilit pu essere sicuramente colmato , almeno parzialmente , mediante manovre aggiuntive ( radiogrammi in ortostatismo e massima espirazione , manovra di hessen , etc . ) , le quali peraltro richiedono un grado di collaborazione da parte del paziente difficilmente ottenibile in determinate situazioni cliniche ( paziente traumatizzato , terapia intensiva , etc . ) ; ed proprio in tali situazioni che lecografia toracica merita di essere proposta quale metodica complementare , se non alternativa , al radiogramma toracico . i bassi valori di sensibilit dellecografia ( rispettivamente 73% e 80% ) riportati da sistrom et al . 
 [ 15 ] sono almeno in parte attribuibili al metodo adottato , che prevedeva la diagnosi differita anzich in tempo reale . i casi discordanti della nostra casistica sono rappresentati da due falsi negativi . nel primo caso si trattava di una sottile falda di pneumotorace proclive , riconosciuta al controllo tc post - bioptico , ma non al controllo ecografico successivo ; considerandone lesiguit possibile supporre che essa si fosse gi riassorbita al momento del controllo ecografico . il secondo caso discordante rappresentato da una limitata falda di pneumotorace saccato posteriore , non apprezzata ovviamente al controllo ecografico , eseguito esclusivamente sulla superficie anteriore per scelta metodologica . 
la possibilit di tale errore gi stata riferita in precedenza [ 4 ]  . probabilmente , studiando il paziente direttamente nella sede di biopsia , secondo il metodo adottato da goodman et al . 
in entrambi i casi , il controllo radiografico successivo ( 4 ore dopo la biopsia ) risultava comunque negativo , ed il paziente non ha necessitato di alcun trattamento . i valori di specificit e vpp ( 100% ) , pur allineandosi ad alcuni precedenti [ 13 , 14 ] , necessitano di alcune considerazioni critiche : la relativa omogeneit della tipologia di pazienti da noi esaminati non ha consentito di affrontare molte delle potenziali cause di errore diagnostico . infatti esistono , almeno sul piano teorico , numerose situazioni che possono causare falsi positivi , riducendo laccuratezza diagnostica della metodica . 
6a scansione tc dopo biopsia transtoracica destra ; si apprezza assenza di pneumotorace ; sono presenti segni di enfisema parasettale anteriore a destra . b lecografia m - mode a sinistra documenta normale scorrimento polmonare . 
in our series , the high sensitivity of the sign ( 97.7% ) is surely to be ascribed to the small number of severe or massive pneumothoraces ( 1 / 46 ) , in which the sign is more difficult to appreciate . the sign could not be recognised in one case only , a complete pneumothorax that was , however , easily diagnosed at the radiographic examination . 
us is unable to provide direct quantitative evaluation of the volume of the pneumothorax or thickness of the air collection between the pleural layers except for cases of hydropneumothorax [ 7 ]  . 
it has , however , been noted that the extent of the collection can be derived from the site of lung - point projection [ 4 , 7 , 12 ]  . 
in our series , the sign proved useful for rough quantification of the severity of the collection , with almost total correspondence with ct findings . condo lo stesso autore , il punto polmonare risulterebbe scarsamente sensibile ( 80% considerando solo le falde di pneumotorace radio - occulto )  . 
nella casistica personale , lelevata sensibilit del segno ( 97 , 7% ) sicuramente da attribuire allesiguo numero di falde di pneumotorace grave o massivo ( 1 / 46 ) , nelle quali il segno pi difficilmente apprezzabile . in un solo caso , il segno non risultato riconoscibile , trattandosi di uno pneumotorace completo , peraltro facilmente diagnosticato allesame radiografico . 
i nostri risultati in termini di sensibilit e specificit attribuiscono a questo segno unutilit indiscutibile soprattutto nellidentificazione di minime falde di pneumotorace , pi difficilmente apprezzabili allesame radiografico a paziente supino . 
lecografia non in grado di dare una valutazione quantitativa diretta del volume dello pneumotorace o dello spessore della falda gassosa interposta ai foglietti pleurici , tranne che in caso di idropneumotorace [ 7 ]  . 
stato fatto notare , per , che possibile definire lentit della falda , considerando la sede di proiezione del punto polmonare [ 4 , 7 , 12 ] : in breve , un punto polmonare anteriore indica uno pneumotorace lieve o moderato , mentre un punto polmonare assente sospetto per uno pneumotorace completo . 
nella nostra casistica , il segno risultato utile per una quantificazione approssimativa dellentit della falda , con una corrispondenza pressoch totale rispetto alla tc . conclusions although unable to replace chest radiography owing to its inability to provide a panoramic view of the respiratory system , chest us is a reliable examination in the pure diagnosis of pneumothorax , above all , minimal pneumothoraces that are frequently radio occult . considering the well - known advantages of us , it is hoped that the method will be increasingly used in every situation where chest radiography is not readily available , where it is technically unreliable for recognition of minimal pneumothoraces or not strictly necessary . conclusioni ben lontano dal poter sostituirsi allesame radiografico del torace per limpossibilit di fornire una visione panoramica dellapparato respiratorio , lecografia si dimostra esame affidabile nella diagnosi pura di pneumotorace , soprattutto in caso di falde di minima entit frequentemente radio - occulte . 
romano1 1unit operativa a struttura complessa di radiologia generale e di pronto soccorso , dipartimento di diagnostica per immagini e 2unit operativa a struttura complessa di endoscopia bronchiale , dipartimento di pneumologia , azienda ospedaliera di rilievo nazionale a . 
pinto , via posillipo 168 / d , i - 80123 napoli , italy , tel . : + 39 - 335 - 6762755 , fax : + 39 - 081 - 2466150 , e - mail : antopin1968@libero.it received : 23 june 2005 / accepted : 12 september 2005 / published online : 25 may 2006 abstract purpose . 
during a 5 - year period , 31 patients ( 18 men and 13 women ; age range 6 months to 85 years ) were referred to our observation for clinical suspicion of foreign - body aspiration . 
plain chest radiography showed the presence of a foreign body in the tracheobronchial tree in 7 / 31 ( 22.6% ) patients , who subsequently underwent successful bronchoscopy in all cases . foreign bodies included tooth fragment ( three cases ) , nail ( two cases ) , metallic spiral of a ball - point pen ( one case ) and an earring ( one case )  . 
in the remaining 24 / 31 patients , plain chest radiography was positive in 14 cases , showing atelectasis ( seven cases ) , pneumonia ( six cases ) , pulmonary hyperinflation ( one case ) and pneumomediastinum ( one case )  . 
moreover , three of the remaining ten patients with negative plain chest radiograph were submitted to msct of the chest , which required in 1 case tracheobronchial aspiration of a foreign body that was subsequently removed by means of bronchoscopy . 
overall , plain chest radiography showed the presence of foreign - body aspiration and / or pleuroparenchymal lesions in 21 / 31 patients ( 67.7% ) ; bronchoscopy was positive in 23 / 27 patients ( 85.2% ) , localising the foreign body in the right main bronchus in 16 / 27 patients riassunto obiettivo . 
in un periodo di 5 anni , 31 pazienti ( 18 maschi e 13 femmine , et compresa tra 6 mesi e 85 anni ) sono giunti alla nostra osservazione con il sospetto clinico - anamnestico di corpo estraneo aspirato , presentando i seguenti sintomi : tosse in 27 / 31 casi ( 87 , 1% ) , reperti patologici allascoltazione del torace in 22 / 31 ( 71% ) , sensazione di soffocamento in 18 / 31 ( 58 , 1% ) , febbre in 7 / 31 ( 22 , 6% ) , e cianosi in 5 / 31 ( 16 , 1% )  . 
tutti i pazienti , entro 2 ore dal ricovero , sono stati sottoposti a esame radiografico del torace eseguito in ortostasi nelle due proiezioni ortogonali in 10 / 31 pazienti ( 32 , 3% ) , e in clinostasi in decubito supino nei rimanenti 21 ( 67 , 7% )  . 
lesame radiografico del torace ha consentito di individuare la presenza di corpo estraneo aspirato nellalbero tracheobronchiale in 7 / 31 ( 22 , 6% ) pazienti , successivamente sottoposti ad esame broncoscopico che ha consentito la rimozione del corpo estraneo in tutti i casi . 
i corpi estranei erano rappresentati da : elemento dentario ( 3 casi ) , chiodo ( 2 casi ) , spiralina metallica di penna sfera ( 1 caso ) , orecchino ( 1 caso )  . nei restanti 24 / 31 pazienti , lesame radiologico del torace risultato positivo in 14 casi , evidenziando : aree di atelettasia ( 7 casi ) , focolai broncopneumonici ( 6 casi ) , iperinsufflazione polmonare e pneumomediastino ( 1 caso )  . 
inoltre , 3 dei rimanenti 10 pazienti con esame radiografico del torace negativo sono stati sottoposti ad esame tcms del torace risultato positivo in un caso , successivamente sottoposto a broncoscopia terapeutica . 
nevertheless , in the case of negative chest radiography and a clinical suspicion of foreign - body aspiration , msct possibly integrated with virtual bronchoscopy should be considered in order to avoid unnecessary bronchoscopy . key words foreign bodies aspiration chest radiography lesame radiografico del torace ha evidenziato la presenza di corpo estraneo aspirato e / o di lesioni pleuro - parenchimali in 21 / 31 casi ( 67 , 7% ) ; lesame broncoscopico risultato positivo in 23 / 27 ( 85 , 2% ) , evidenziando il corpo estraneo localizzato a livello di : bronco principale destro in 16 / 27 casi ( 59 , 3% ) , bronco principale sinistro in 7 / 27 ( 25 , 9% ) , bronco intermedio 2 / 27 ( 7 , 4% ) e bronco lobare inferiore destro in 2 / 27 ( 7 , 4% )  . 
lesame radiologico del torace conserva il ruolo di indagine diagnostica di prima istanza in pazienti con sospetta aspirazione di corpo estraneo nellalbero tracheo - bronchiale . tuttavia , in caso di negativit dellesame radiografico del torace e di elevato sospetto clinico di aspirazione di corpo estraneo , giustificato il ricorso allesame tcms del torace ( anche integrato da broncoscopia virtuale ) il cui esito negativo , nella maggioranza dei casi , esclude il ricorso a esame broncoscopico . parole chiave corpi estranei aspirazione esame radiografico del torace introduction introduzione aspiration of foreign bodies in the tracheobronchial tree is relatively common in children [ 1 ] but rare in adults [ 24 ] , in whom it is often associated with specific pathological conditions such as mental retardation , seizures , parkinsons disease and brain tumours . therapeutic dental procedures performed with patients under local anaesthesia and in the supine position represent a further risk factor for the aspiration of foreign bodies into the airways [ 5 ]  . inhaled foreign bodies may be either inorganic or organic . the most common inorganic bodies are plastic objects ( toy fragments , pen caps , dental prostheses ) or metallic objects ( hairpins , pins , steel filaments )  . the most common organic bodies include peanuts , seeds and nuts , blades of grass or bone fragments [ 68 ]  . 
foreignbody aspiration may result in fatal acute asphyxia if not promptly diagnosed and treated , or it may manifest with symptoms of chronic respiratory failure leading to long - term complications [ 9 ]  . clinical suspicion of foreign - body aspiration usually requires immediate admission to hospital where the patient is initially studied by chest radiography to assess the presence of the foreign body or possible pleuroparenchymal and / or mediastinal changes . recent radiological literature has highlighted the diagnostic contribution of bronchoscopy [ 10 ] , computed tomography ( ct ) [ 5 ] , high - resolution ct [ 11 ] , spiral ct [ 12 ] and virtual bronchoscopy with multislice ct ( msct ) [ 13 , 14 ] in the evaluation of patients with suspected tracheobronchial aspiration of foreign bodies , leading to reconsideration of the role traditionally attributed to chest radiography [ 15 ]  . the diagnostic capabilities of magnetic resonance imaging mri in detecting peanuts inhaled into the tracheobronchial tree have also been described [ 16 , 17 ]  . this study investigates the current indications for chest laspirazione di corpi estranei nellalbero tracheobronchiale costituisce evento non infrequente nei bambini [ 1 ] , mentre raro negli adulti [ 24 ] nei quali spesso si associa a particolari condizioni patologiche quali ritardo mentale , crisi convulsive , morbo di parkinson e neoplasie cerebrali . 
gli atti terapeutici eseguiti in ambiente odontoiatrico su pazienti in posizione supina , in anestesia locale , costituiscono un ulteriore fattore predisponente laspirazione di corpi estranei nelle vie aeree [ 5 ]  . i corpi estranei aspirati possono essere inorganici oppure organici : tra quelli inorganici , i pi frequenti sono rappresentati da oggetti di materiale plastico ( frammenti di giocattoli , tappi di penne , protesi dentarie ) oppure di metallo ( forcine per capelli , spilli , filamenti di acciaio )  . 
tra quelli di natura organica , i pi frequenti sono i semi di arachidi o di altri frutti , le spighe di alcune graminacee e frammenti di tessuto osseo [ 68 ]  . 
laspirazione di corpi estranei pu rappresentare una condizione gravata da rischio immediato di asfissia acuta mortale se non rapidamente diagnosticata e terapeuticamente risolta , oppure pu manifestarsi con sintomi di insufficienza respiratoria cronica e comportare complicanze anche a lungo termine [ 9 ]  . 
il sospetto clinico di aspirazione di corpo estraneo nelle vie aeree implica generalmente il rapido ricovero del paziente in ambiente ospedaliero , ove viene praticato , quale prima indagine diagnostica , lesame radiografico del torace allo scopo di evidenziare la presenza del corpo estraneo oppure di eventuali alterazioni pleuro - parenchimali e / o mediastiniche . 
negli ultimi anni , in letteratura radiologica , stato sottolineato il contributo diagnostico offerto dalla broncoscopia [ 10 ] , dalla tomografia computerizzata [ 5 ] , dalla tomografia computerizzata ad alta risoluzione [ 11 ] , dalla tomografia computerizzata spirale [ 12 ] e dalla broncoscopia virtuale con tomografia computerizzata multistrato [ 13 , 14 ] nella valutazione dei pazienti con sospetta aspirazione di corpi estranei nellalbero traradiography in the emergency evaluation of patients with suspected foreign - body aspiration . 
sono state infine descritte le possibilit diagnostiche della risonanza magnetica nella individuazione delle arachidi aspirate nellalbero tracheobronchiale [ 16 , 17 ]  . nel presente contributo sono ricercate le indicazioni attuali dellesame radiografico del torace nella valutazione in urgenza di pazienti con sospetta aspirazione di corpo estraneo . materiali e metodi nel periodo maggio 1999maggio 2004 , 31 pazienti ( 18 di sesso maschile e 13 di sesso femminile ) , di et compresa tra 6 mesi e 85 anni ( et media 9 , 3 anni , 23 / 31 pazienti di et inferiore a 8 anni ) sono giunti alla nostra osservazione con il sospetto clinico - anamnestico di corpo estraneo aspirato , presentando i seguenti sintomi : tosse in 27 / 31 casi ( 87 , 1% ) reperti patologici allascoltazione del torace in 22 / 31 ( 71% ) , sensazione di soffocamento in 18 / 31 ( 58 , 1% ) , febbre in 7 / 31 ( 22 , 6% ) e cianosi in 5 / 31 ( 16 , 1% )  . 
tutti i pazienti , entro 2 ore dal ricovero , sono stati sottoposti a esame radiografico del torace eseguito in ortostasi nelle due proiezioni ortogonali in 10 / 31 pazienti latero - laterale postero - anteriore e ( 32 , 3% ) , e in clinostasi in decubito supino ( unico radiogramma in proiezione antero - posteriore ) nei rimanenti 21 ( 67 , 7% )  . 
lesame radiografico del torace stato successivamente integrato da tomografia computerizzata multistrato ( tcms ) del torace in 3 / 31 pazienti ( 9 , 7% ) e da esame broncoscopico in 27 / 31 pazienti ( 87 , 1% ) eseguiti entro 14 ore dallesame radiografico del torace . 
lindagine tcms ( aquilion 16 , toshiba , tokyo , giappone ) del torace stata eseguita in tutti i 3 casi senza perfusione di mdc ev utilizzando i seguenti parametri di acquisizione : collimazione 1 mm , intervallo di ricostruzione 0 , 8 mm , pitch 1 , 4 . 
le immagini acquisite sono state trasferite su una stazione di lavoro ( vitrea 3.5 , plymouth , minnesota , usa ) ove oltre alle immagini assiali sono state realizzate e visualizzate simultaneamente ricostruzioni multiplanari sui piani sagittale e coronale . risultati lesame radiografico del torace ha consentito di individuare la presenza di corpo estraneo aspirato nellalbero tracheobronchiale in 7 / 31 pazienti ( 22 , 6% ) , successivamente sottoposti ad esame broncoscopico che ha consentito la rimozione del corpo estraneo in tutti i casi . 
1a - c esame radiografico del torace in proiezione postero - anteriore ( a ) e latero - laterale ( b ) : presenza di elemento dentario inalato ( freccia ) localizzato nel bronco principale destro . 
3a - c esame radiografico del torace in proiezione postero - anteriore ( a ) e latero - laterale ( b ) : presenza di orecchino inalato localizzato nel bronco principale destro . 
4a , b plain chest radiograph in anteroposterior projection ( a ) showing left - side atelectasis with ipsilateral mediastinal shift due to bronchial obstruction following inhalation of a small nut ( b ) , which was removed by means of bronchoscopy . 
five patients with negative radiography underwent bronchoscopy : this was negative in four cases and positive in one case ( resolved with extraction of the foreign body )  . the remaining two patients were discharged after 24 h of observation , as the symptoms suggesting foreign - body aspiration did not persist . 
 discussion the term aspiration refers to a variety of clinical conditions characterised by the introduction of fluid or particulate matter into the airways [ 18 ]  . tracheobronchial foreign - body aspiration is a potentially dramatic emergency situation that affects children younger than 3 years in 50% of cases [ 19 , 20 ]  . the nature of the aspirated foreign bodies may differ based on life style and dietary habits [ 21 , 22 ] : the most commonly aspirated foreign bodies are nuts and peanuts in children and particulate matter ( mainly in polytrauma patients in the intensive care unit ) [ 23 ] and denture fragments in adults [ 24 ]  . the aspirated foreign body may be retained in the larynx giving rise to symptoms of glottic obstruction , or reach the main bronchi and their branches where it causes partial or total obstruction . 
 although the clinical picture may be suggestive of foreign - body inhalation , there may be no reference to this susestraneo aspirato nelle vie aeree . complessivamente , lesame radiografico del torace ha evidenziato la presenza di corpo estraneo aspirato e / o di lesioni pleuro - parenchimali in 21 / 31 casi ( 67 , 7% ) ; lesame broncoscopico risultato positivo in 23 / 27 ( 85 , 2% ) , evidenziando il corpo estraneo localizzato a livello di : bronco principale destro in 16 / 27 casi ( 59 , 3% ) , bronco principale sinistro in 7 / 27 ( 25 , 9% ) , bronco intermedio 2 / 27 ( 7 , 4% ) e bronco lobare inferiore destro in 2 / 27 ( 7 , 4% )  . 
inoltre lesame tcms del torace risultato positivo in 1 / 3 casi ( 33 , 3% )  . nessuna complicanza stata osservata nei successivi sei mesi dalla dimissione dallambiente ospedaliero . discussione il termine aspirazione indica una variet di condizioni cliniche caratterizzate dalla immissione di materiale solido oppure liquido nelle vie aeree [ 18 ]  . laspirazione di corpi estranei nellalbero tracheobronchiale rappresenta unemergenza , talvolta drammatica , che colpisce , in circa il 50% dei casi , bambini di et inferiore a 3 anni [ 19 , 20 ]  . sebbene la natura dei corpi estranei aspirati nelle vie aeree differisca in base allo stile di vita e alle abitudini alimentari [ 21 , 22 ] , nei bambini i corpi estranei pi frequentemente aspirati sono rappresentati da noci e noccioline , mentre negli adulti da materiale solido ( prevalentemente nei politraumatizzati ricoverati in rianimazione ) [ 23 ] e da elementi di protesi dentaria [ 24 ]  . 
il corpo estraneo inalato pu essere ritenuto in laringe , dando sintomi di ostruzione glottica , oppure raggiungere i bronchi principali e le loro diramazioni , ove determina ostruzione parziale o totale . 
 non sempre , di fronte a quadri clinici compatibili con corpo estraneo aspirato , vi riferimento anamnestico di sospetta inalazione di corpo estraneo . la sintomatologia , caratterizzata in fase iniziale da sensazione di soffocamento con tosse spasmodica , non produttiva , sibili inspiratori ed espiratori udibili , e dispnea ingravescente , conduce al sospetto clinico di corpo estraneo inalato pi facilmente nei bambini e meno frequentemente negli adulti , soprattutto se affetti da patologia respiratoria cronipicion in the patients history . 
initial symptoms such as a choking with paroxysmal nonproductive cough , inspiratory and expiratory wheezes and worsening dyspnoea may raise the clinical suspicion of foreign - body aspiration more frequently in children than in adults , above all in those with chronic respiratory diseases . moreover , many cases of tracheobronchial foreign - body aspiration in children are misdiagnosed as asthma or bronchiolitis , and the correct diagnosis is achieved within 24 h in 50% of children only [ 25 ]  . delay in diagnosis of foreign - body aspiration is common in adults , above all in those admitted for severe polytrauma [ 23 ]  . 
 the histopathological picture related to bronchial aspiration of a foreign body is characterised by lesions at the point of contact as well as in the lower bronchopulmonary segments . lesions at the point of contact may be traumatic or inflammatory . 
traumatic lesions ( oedema , haemorrhagic suffusion , cutting or piercing wound , lacerated and contused wound , decubitus ulcer ) may develop instantly or after some time , especially if the foreign body is small and changes position when the patient coughs . these lesions are closely related to the physical properties of the foreign body and , by allowing the entry of bacteria , they pave the way for the later development of inflammatory lesions , which tend to have a similar morphohistological profile to any other form of nonspecific bronchial inflammation [ 26 ]  . bronchopulmonary alterations located below the aspirated foreign body include acute emphysema , simple atelectasis and pyosclerosis [ 26 ]  . if the foreign body causes mild alterations on the bronchial wall and its size is such that it occludes the bronchial branch during expiration only , a valve mechanism develops in the air current dynamics . intra - alveolar hypertension , which increases with each expiration , causes abrupt marked dilation of all the acini and lobules distal to the occluded bronchus . 
gross examination reveals a white area that is increased in volume and appears as one or more air bubbles delimited by the overdistended pleura ( acute emphysema )  . in contrast , if the foreign body permanently occludes the bronchial branch due to its size or oedema and fibrin deposits , the entire tributary parenchymal district ( segment , lobe or entire lung ) becomes distended ; in this case , gross examination reveals retraction , redness and thickening of the affected parenchyma . the majority of aspirated foreign bodies in children are found in the proximal airways , probably as a result of bronchial diameter ; the right bronchial branch is more commonly involved owing to its more vertical course . 
 in suspected tracheobronchial foreign - body aspiration , chest radiography is performed in the upright posteroanterior and laterolateral projections or , when this is not possible , in the supine position in the anteroposterior projection . comparison of the inspiratory and expiratory chest radiographs may help detect signs of air trapping [ 3 ]  . 
inoltre , molti casi di aspirazione di corpo estraneo nellalbero tracheo - bronchiale nei bambini sono erroneamente diagnosticati come asma o bronchiolite e la diagnosi di corpo estraneo inalato correttamente formulata nelle prime 24 ore solo nel 50% dei piccoli pazienti [ 25 ]  . 
negli adulti frequente una diagnosi ritardata di corpo estraneo aspirato soprattutto se ricoverati in seguito a grave politrauma [ 23 ]  . il quadro anatomopatologico determinato dalla penetrazione di un corpo estraneo nelle vie bronchiali caratterizzato da lesioni nel punto di contatto e da lesioni dei distretti broncopolmonari a valle . 
le lesioni traumatiche ( edema , soffusioni emorragiche , ferite da punta o taglio , ferite lacero - contusive , ulcere da decubito ) a volte si realizzano immediatamente , altre volte si producono in tempi successivi , specie se , per le sue modeste dimensioni , il corpo estraneo cambia sede in conseguenza dei colpi di tosse . 
queste lesioni sono strettamente correlate con le caratteristiche fisiche del corpo estraneo e , spesso , aprendo la porta allinsediamento batterico , condizionano linsorgenza successiva delle lesioni di tipo infiammatorio , le quali , da un punto di vista macroscopico , assumono nella maggioranza dei casi un profilo morfoistologico simile a quello di tutte le flogosi bronchiali aspecifiche [ 26 ]  . le alterazioni broncopolmonari nei territori a valle rispetto alla sede del corpo estraneo inalato , sono rappresentate da : enfisema acuto , atelettasia semplice , piosclerosi [ 26 ]  . 
se il corpo estraneo provoca modeste alterazioni sulla parete bronchiale e le sue dimensioni sono tali da occludere il ramo bronchiale interessato solo in fase espiratoria , si realizza nella dinamica delle correnti aeree un meccanismo a valvola . 
il regime ipertensivo endoalveolare , che si accresce progressivamente ad ogni espirazione , determina la dilatazione , brusca e marcata , di tutte le unit acinari e lobulari tributarie del bronco occluso . 
macroscopicamente il territorio interessato si presenta pallido , aumentato di volume , e con laspetto di una o pi bolle aeree , delimitate dal foglietto pleurico iperdisteso ( enfisema acuto )  . 
se il corpo estraneo , invece , per le sue dimensioni o perch favorito dalledema e dalle deposizioni fibrinose , realizza locclusione permanente di un ramo bronchiale , tutto il territorio parenchimale tributario ( segmento , lobo o intero polmone ) va in atelettasia . 
allesame macroscopico , il parenchima interessato appare retratto , di colorito rosso , di consistenza aumentata.la maggioranza dei corpi estranei aspirati nei bambini si localizza nelle vie aeree prossimali , probabilmente a causa del diametro dei bronchi ; maggiormente coinvolto appare lalbero bronchiale di destra a causa della sua disposizione pi verticale rispetto al controlaterale : questa sede risultata la pi frequente anche nella nostra casistica . nel sospetto clinico di aspirazione di corpo estraneo nellalbero tracheobronchiale , si esegue lesame radiografico del torace nelle due proiezioni ortogonali postero - anteriore e latero - laterale in ortostasi , mentre , quando non possibile , in decubito supino in proiezione antero - posteriore . il confronto tra il radiogramma del torace in inspirazione e quello in espirazione facilita lindividuazione di segni di ina . 
 negative chest radiography in patients with a strong clinical suspicion of foreign - body aspiration requires subsequent bronchoscopy , which was performed in 27 / 31 ( 87.1% ) of our patients . ct is clearly more accurate than chest radiography in detecting radiolucent foreign bodies [ 3335 ] , and in our opinion , it should be performed in patients with a low level of clinical suspicion of foreign - body aspiration in whom chest radiography is negative . in our series , ct was performed in three patients only , two of whom were discharged without undergoing bronchoscopy on the basis of consistent clinical and ct findings . moreover , several authors have reported that ct may be burdened by false positive results ( calcified lymph nodes misread as endobronchial foreign bodies ) [ 5 ] and that it therefore should not be routinely used as the initial diagnostic approach . we believe that the indication for ct remains valid in the case of atypical presentations or discrepancy between clinical and radiological findings . in these cases , the differential diagnosis includes tracheobronchial obstruction due to external airway compression ( due to enlarged lymph nodes , mediastinal neoplasms , cardiomegaly ) or intraluminal tracheobronchial obstruction ( due to bronchiolitis , neoplasm , granulation tissue as in tuberculosis , mucus plugs and secretions as in bacterial bronchopneumonia , cystic fibrosis , asthma , pulmonary abscess , acute laryngotracheobronchitis ) [ 20 ]  . 
 in patients with suspected foreign - body aspiration , bronchoscopy can also be performed in the presence of negative chest radiography or doubtful clinical findings . only four patients in our series were not subjected to bronchoscopy : two had negative radiography and ct , and the other two had negative radiography , negative 24 - h clinical observation and no persistence of suggestive clinical symptoms . 
 trappolamento aereo [ 3 ] , cos come losservazione fluoroscopica conserva in tali circostanze una delle sue ormai limitatissime indicazioni , poich consente di rilevare asimmetrie della ventilazione e movimenti paradossi del mediastino e del diaframma [ 19 ]  . 
allesame radiologico del torace si possono osservare nella maggioranza dei casi i seguenti reperti : dimostrazione diretta del corpo estraneo , ipertrasparenza lobare o segmentaria secondaria ad intrappolamento aereo , atelettasia , addensamenti parenchimali di possibile natura flogistica [ 20 ]  . 
la visibilit diretta del corpo estraneo allesame radiografico del torace legata ai fattori che regolano la penetrazione dei raggi x nella materia ( spessore , grandezza , peso specifico , peso atomico ) per cui corpi estranei metallici vengono facilmente identificati , mentre frammenti di legno o di vetro si reperiscono , in linea generale , con maggior difficolt [ 30 ]  . 
la percentuale di esami radiografici negativi , in pazienti con corpo estraneo aspirato , varia dal 5 al 30% nei bambini [ 31 ] e dall8 all80% [ 21 , 22 , 32 ] negli adulti . 
la negativit dellesame radiologico del torace in pazienti con elevato sospetto clinico di inalazione di corpo estraneo implica la successiva esecuzione di indagine broncoscopica , che nella nostra casistica stata eseguita in 27 / 31 pazienti ( 87 , 1% )  . lindagine tc ovviamente pi accurata dellesame radiologico del torace nellidentificare i corpi estranei radiotrasparenti inalati [ 3335 ] : a nostro giudizio , tale esame dovrebbe essere eseguito in pazienti con basso sospetto clinico di inalazione di corpo estraneo , nei quali lesame radiologico del torace sia risultato negativo . 
nella nostra serie , lindagine tc stata eseguita in soli tre pazienti , due dei quali dimessi senza aver praticato la broncoscopia in base ai reperti clinici e tc negativi concordi . 
alcuni autori hanno inoltre segnalato che lindagine tc pu essere gravata da falsi positivi ( linfonodi calcifici erroneamente interpretati quali corpi estranei endobronchiali ) [ 5 ] , non consigliandone lesecuzione di routine quale prima indagine diagnostica . 
mazziotti , via consolare pompea 1871 , i - 98165 messina , italy , tel . : + 39 - 090 - 2212941 , fax : + 39 - 090 - 221 3720 , e - mail : smazziotti@unime.it received : 22 march 2005 / accepted : 7 december 2005 / published online : 25 may 2006 abstract purpose . 
all examinations were performed on a multislice ct ( msct ) scanner ( sensation 16 , siemens , erlangen , germany ) with axial volumetric acquisition and completed with reformations of coronal and coronal - oblique images . 
finally , in all cases , it was possible to identify the facial nerve canal and main vascular structures and to measure the distance between these and the sinus tympani , pyramidal eminence and hypotympanuthe coronal oblique ct reformation was of no advantage in the evaluation of the fossa of the oval window and the niche of the round window . 
sono stati studiati 30 pazienti per un totale di 60 rocche petrose normali con et variabile da 18 a 79 anni . lesame stato condotto con apparecchio tc multidetettore ( sensation 16 , siemens , enlargen , germania ) eseguendo unacquisizione volumetrica assiale , integrata da ricostruzioni coronali e paracoronali oblique . 
in tutti i casi , infine , stata possibile la documentazione della sede del canale del faciale e delle principali strutture vascolari e la quantificazione della distanza tra queste ultime e strutture anatomiche quali il seno timpanico , leminenza piramidale e lipotimpano . 
il piano di ricostruzione paracoronale , oggetto del presente lavoro , non deve essere considerato unalternativa allesame standard , ma pu rappresentare una valida integrazione dello stesso , in grado di fornire informazioni aggiuntive su distretti particolarmente cruciali per il loro frequente coinvolgimento in corso di patologia infiammatoria e / o espansiva e per il loro approccio endoscopico , talvolta difficile . 
recent technological improvements , such as multidetector ct ( mdct ) and , particularly , isotropic pixel , allow high - quality multiplanar reconstruction ( mpr ) reformations oriented in all spatial planes to be obtained from thin axial data ; this is also possible in a complex anatomical district characterised by structures smaller than 1 mm , such as the petrous bone . we describe the normal anatomy as observable in a coronal oblique ct reformation oriented towards the major axis of the rocca petrosa and parallel to the basal turn of the cochlea . 
moreover , we assessed the potential adjunctive information deriving from this technical expedient with special reference to some anatomical areas , such as the retroand hypotympanum , which are not satisfactorily visualised on standard axial and ct images . 
we also analysed the possibility of evaluating spatial relationships between the abovementioned anatomical regions and vasculonervous structures with the objective of optimising surgical planning [ 13 ]  . axial and coronal ct normal anatomy the middle ear is an aerated cavity with irregular morphology located in the rocca petrosa of the temporal bone . 
on the basis of its anatomical position , it can be subdivided into [ 46 ] : epitympanum ( superior ) protympanum ( anterior ) mesotympanum retrotympanum ( posterior ) hypotympanum ( inferior ) the retrotympanum and hypotympanum are characterised by a particularly complex anatomy in which it is possible to identify many recesses and bony ridges , which , moreover , introduce a wide anatomical variability [ 7 ]  . retrotympanum the retrotympanum represents the majority ( more than half ) of the tympanic cavity . 
the anatomical transition towards the hypotympanum is represented by an ideal plane passing through the styloid eminence ( or eminence of politzer ) , which is a bony prominence corresponding to the base of the styloid process and situated somewhat inferiorly relative to sinus tympani [ 4 ]  . 
conversely , descriptions of extremely inconstant and / or of anatomical nella pratica clinica la valutazione tc della rocca petrosa dellosso temporale si basa fondamentalmente sulle informazioni deducibili dallacquisizione diretta sia nel piano assiale che coronale e ci per la mediocre risoluzione spaziale che caratterizza le immagini di ricostruzione post - processing , anche se ottenute con tc spirale . le pi recenti innovazioni tecnologiche quali la tc multidetettore e , soprattutto , la possibilit di disporre del voxel isotropico , permettono oggi di poter ottenere immagini di elevata qualit secondo piani di ricostruzione orientati in tutte le direzioni dello spazio , anche in un distretto dotato di estrema complessit e caratterizzato da dettagli anatomici con dimensioni millimetriche e sub - millimetriche quale la rocca petrosa . lo scopo del presente lavoro quello di descrivere lanatomia tc normale secondo un piano di ricostruzione coronale obliquo orientato lungo lasse maggiore della rocca , parallelo al giro basale della coclea . 
saranno , pertanto , valutate le possibili informazioni aggiuntive derivabili da tale accorgimento metodologico con particolare riguardo ad alcune aree anatomiche , quali il retro e lipotimpano , che risultano analizzabili in maniera non del tutto esaustiva nellesame tc limitato ai due classici piani di acquisizione ( assiale e coronale )  . la suddetta modalit dapproccio sar anche analizzata nellottica della valutazione dei reciproci rapporti spaziali tra le summenzionate regioni anatomiche e le strutture vascolo - nervose ad esse limitrofe , e ci soprattutto nellottica relativa alle varie modalit di pianificazione chirurgica [ 13 ]  . cenni di anatomia tc normale assiale e coronale lorecchio medio una cavit aerata di morfologia piuttosto irregolare , scavata nella rocca petrosa dellosso temporale che , in considerazione della disposizione anatomica , possibile suddividere in [ 46 ] : epitimpano ( superiore ) prototimpano ( anteriore ) mesotimpano retrotimpano ( posteriore ) ipotimpano ( inferiore ) il retrotimpano e lipotimpano sono caratterizzati da unanatomia particolarmente complessa nella quale possibile identificare numerosi recessi e salienze ossee le quali , peraltro , presentano unampia variabilit anatomica [ 7 ]  . retrotimpano il retrotimpano rappresenta la gran parte ( oltre la met ) della cavit timpanica ; esso si situa al di sotto dellantro mastoideo e il suo limite anteriore dato dal promontorio . 
this is a small bony relief with triangular morphology located laterally to the sinus tympani . from its apex emerges the tendon of the stapedius muscle [ 7 , 8 ]  . 
this is an osseous protuberance of the upper part of the retrotympanum , formed by the facial nerve canal running between the oval window and the eminence of the semicircular lateral canal . 
molti di essi non sono visualizzabili mediante tc , sia per il loro estremo polimorfismo , sia perch non sempre caratterizzati da un sufficiente grado di ossificazione . per tale motivo nella presente descrizione verranno trattate soltanto quelle salienze ossee ed i relativi recessi dotati di una certa costanza e pi facilmente riconoscibili . 
leminenza piramidale un piccolo rilievo osseo con morfologia triangolare che si localizza lateralmente al seno timpanico e dal cui apice emerge il tendine del muscolo stapedio [ 7 , 8 ]  . 
leminenza del tratto mastoideo del nervo faciale una salienza ossea nella porzione alta del retrotimpano determinata dal canale del nervo faciale nel suo decorso tra la finestra ovale e la salienza del canale semicircolare laterale . 
il ponticulus un incostante rilievo osseo situato tra leminenza piramidale ed il margine postero - superiore del promontorio e separa la finestra ovale dal seno timpanico del quale , come diremo pi avanti , costituisce il limite superiore . 
la fossetta della finestra ovale una depressione relativamente ampia in cui si apre la finestra omonima , occupata dalla staffa e i cui limiti anatomici sono rappresentati in basso dal promontorio e dal ponticulus , che posteriormente dal promontorio raggiunge leminenza piramidale . 
the first , at the top , is separated from the sinus tympani by the ponticulus ; the second , inferiorly , is delimited from the sinus tympani by the subiculuthe medial limit of the sinus tympani is represented by the promontory , and the lateral one corresponds to the pyramidal eminence and crest . 
la fossetta della finestra rotonda una nicchia in cui si apre la finestra rotonda ; essa caratterizzata da una morfologia cilindrica ed situata sotto lestremit libera del giro basale della coclea rispetto al quale presenta una inclinazione postero - laterale . 
la seconda , a sede inferiore , delimitata dal seno timpanico dal subiculuil limite mediale del seno timpanico rappresentato dal promontorio , mentre il suo limite laterale individuato dalleminenza e dalla cresta piramidale . 
in tutti i casi , losso temporale stato compreso nel volume di acquisizione per un totale di 60 rocche petrose normali esaminate . lesame stato condotto con apparecchio tc multidetettore ( sensation 16 , siemens , enlargen , germania ) eseguendo unacquisizione volumetrica assiale , integrata da ricostruzioni coronali e paracoronali oblique . 
le ricostruzioni sono state effettuate con spessore 0 , 7 mm , indice di ricostruzione di 0 , 5 mm e filtro ad alta risoluzione per losso . le immagini assiali sono state orientate secondo un piano parallelo al palato duro . 
durante la valutazione delle immagini stato fondamentale utilizzare una finestra per osso che fosse abbastanza ampia , in modo da poter valutare strutture che avessero densit inferiore allosso ( ricordiamo che alcune strutture possono non essere completamente ossificate e pertanto non facilmente identificabili con valori di finestra molto stretti )  . risultati sono state analizzate le modalit e la frequenza di rappresentazione , oltrecch i relativi rapporti anatomici , delle strutture anatomiche del retro e dellipotimpano analizzate nei piani assiale e coronale . 
lincidenza coronale ha consentito in tutti i casi la individuazione del seno timpanico ma non ha permesso una accurata valutazione delle sue dimensioni sul piano frontale in ragione della distorsione geometrica legata allandamento del piano di ricostruzione . 
all examinations were performed using a 16 - row multislice ct ( msct ) scanner ( sensation 16 , siemens , erlangen , germany ) with axial volumetric acquisition parallel to the hard palate . 
axial images were reconstructed at 0.7 - mm thickness and with a reconstruction increment of 0.5 mm using a high - resolution bone algorithm . coronal images perpendicular to the axial scans were also reconstructed . 
an adequately wide window was used for image visualisation to identify structures with a density lower than bone ( some structures could be not completely ossified and therefore were difficult to recognise with a narrow window setting )  . results axial and coronal images were analysed to establish the modalities and frequency of visualisation , as well as anatomical relationships , of the retroand hypotympanuresults were compared with information obtained with coronal oblique ct reformations . 
the following anatomical structures were taken into consideration : sinus tympani ponticulus subiculum fossa of the oval window niche of the round window pyramidal eminence canal of the facial nerve s . 
in all cases , it was possible to table 1 measurement of the craniocaudal ( cc ) and laterolateral ( ll ) length of the sinus tympani ( st ) and the distance between st and facial canal ( fc ) obtained with coronal oblique reconstruction minimum length , mm maximum length , mm mean length , mm st ( cc ) st ( ll ) st - fc distance tabella 1 misurazione della estensione cranio - caudale ( cc ) e laterolaterale ( ll ) del seno timpanico ( st ) e della distanza intercorrente tra seno timpanico e canale del faciale ( cf ) ottenuta con la ricostruzione paracoronale lunghezza minima , mm lunghezza lunghezza massima , mm media , mm st ( cc ) st ( ll ) distanza st - cf fig . 
subiculula identificazione del subiculum stata estremamente difficoltosa sia nelle scansioni assiali che in quelle coronali e ci in relazione allandamento anatomico della struttura che non consente mai la rappresentazione della stessa in un unico piano di scansione . 
lipotimpano stato ben documentato in tutti i casi con le ricostruzioni assiali e coronali sia pure in maniera parcellare in un numero variabile di immagini . la ricostruzione paracoronale , per converso , in tutti i cas . 
10a ricostruzione paracoronale : 1 giro basale della coclea , 2 canale carotico , 3 golfo della giugulare , 4 ipotimpano ; b 1 canale semicircolare laterale , 2 canale del faciale , 3 ipotimpano . deformed by the projection and partially represented in at least three 0.75 - mm contiguous scans . 
conversely , it was incompletely represented in oblique coronal scans due to its spatial orientation . zione ha consentito in tutti i casi anche la osservazione dei rapporti esistenti tra lipotimpano e la tuba faringea . discussione lipotimpano ed il retrotimpano si configurano come aree anatomiche caratterizzate da notevole complessit e da aspetti critici sia nei confronti di eventi patologici , soprattutto flogistici sia per quanto attiene alla pianificazione di eventuali interventi chirurgici [ 13 , 11 ]  . sulla base dei risultati ottenuti emergono le seguenti considerazioni in merito allimpiego delle immagini derivanti table 2 measurement of the distance between pyramidal eminence ( pe ) and facial canal ( fc ) obtained with coronal oblique reconstruction minimum length , mm maximum length , mm mean length , mm pe - fc tabella 2 misurazione della distanza tra eminenza piramidale ( ep ) e canale del faciale ( cf ) ottenuta con la ricostruzione paracoronale intercorrente lunghezza minima , mm lunghezza lunghezza massima , mm media , mm ep - cf s . 
our oblique paracoronal plane also consistently allowed observation of the relationships between the hypotympanum and pharyngeal tube . discussion the hypotympanum and retrotympanum are anatomical structures characterised by remarkable complexity and critical implications mainly regarding inflammatory diseases and surgical planning [ 13 , 11 ]  . 
it enables estimations of the real dimensions of the sinus tympani , in particular , of its craniocaudal and laterolateral diameters , which are difficult to evaluate at endoscopy [ 4 , 5 , 11 , 12 ]  . 
no advantage was yielded by analysis of the fossa of the oval window and the niche of the round window . it is evident that this approach can be considered a useful complement to the study of the temporal bone performed in the two standard observation planes [ 1316 ] for the study of pathological events localised in the retrotympanum and hypotympanum . it can also play an important role in surgical planning , in particular , in cochlear implant procedures [ 17 ] where presurgical information on the reciprocal anatomical relations between aerial cavities of the tympanum and mastoid and the surrounding vascular , nervous and labyrinthal structures are fundamental . in conclusion , we encourage the routine use of this integration of the standard examination of the temporal bone and also in consideration of the absence of radiation dose increment made possible by multislice technology . table 3 measurement of the distance of hypotympanum with carotid canal and jugular fossa obtained with coronal oblique reconstruction minimum length , mm maximum length , mm mean length , mm hypotympanum carotid canal hypotympanum jugular fossa ipotimpano canale carotideo ipotimpano golfo della giugulare tabella 3 misurazione della distanza tra ipotimpano e canale carotideo e tra ipotimpano e golfo della giugulare lunghezza lunghezza lunghezza minima , mm massima , mm media , mm dallutilizzo del piano di ricostruzione paracoronale obliquo : 1 . 
secondo tale piano di ricostruzione pertanto possibile valutare le reali dimensioni del seno timpanico segnatamente ai suoi diametri cranio - caudale e latero - laterale , informazioni che come noto sono sovente di difficile valutazione endoscopica [ 4 , 5 , 10 , 12 ] ; sono sempre risultate molto ben misurabili , inoltre , le distanze esistenti nei confronti del canale del faciale oltre la valutazione dei rapporti anatomici esistenti tra il seno timpanico ed il canale semicircolare laterale ; 3 . 
algarotti 8 , i - 00137 roma , italy , tel . : + 39 - 349 - 1946942 , e - mail : stepieri@excite.it received : 7 june 2005 / accepted : 18 october 2005 / published online : 25 may 2006 abstract purpose . 
from a retrospective review of 3229 patients treated percutaneously between 1988 and 2003 , we extrapolated the phlebographic images of patients with incontinence of the right internal spermatic vein only . 
contrast medium was injected into both the inferior vena cava and the renal vein . selective catheterisation of the internal spermatic vein was then performed to assess the radiological characteristics of the vessels prior to sclerosis . 
in the first group of patients ( seven cases , 7.5% ) , the right internal spermatic vein drained exclusively into the renal vein ; the injection of contrast medium during a valsalva manoeuvre allowed visualisation of the vein almost as far as the iliac level . 
in the second group ( 21 cases , 22.5% ) , the vein drained into both the renal vein and the inferior vena cava , with one branch showing functional predominance over the other : selective catheterisation was easier to perform on the first branch . 
in most patients , ( 65 cases , 69.8% ) , the internal spermatic vein drained into the inferior vena cava ; the confluence was double in five patients and single in 60 patients . 
da una analisi retrospettiva su 3229 pazienti , trattati con metodica percutanea nellarco temporale tra il 1988 ed il 2003 , sono stati estrapolati i radiogrammi dellanatomia flebografica dei pazienti con incontinenza della sola vena spermatica interna destra . 
lindicazione al trattamento era stata data dalla presenza di una sintomatologia dolorosa nella regione inguinale destra , in assenza di precedenti anamnestici per traumi e / o per alterazioni del liquido seminale . 
in un primo gruppo di pazienti ( 7 casi , 7 , 5% ) , lo sbocco della vena spermatica interna destra avveniva esclusivamente a livello della vena renale ; liniezione di mezzo di contrasto , eseguito durante la manovra di valsalva ne aveva consentito la visualizzazione fin quasi a livello iliaco . 
in un secondo gruppo ( 21 casi , 22 , 5% ) , la confluenza della vena avveniva tanto a livello della vena renale che a livello della vena cava inferiore , con la prevalenza funzionale di un ramo sullaltro : nel primo era pi facile eseguire il cateterismo selettivo . 
interventional radiologists must have a thorough knowledge of anatomic variants of the right internal spermatic vein to be able to perform the procedure within a reasonable amount of time and reduce radiation exposure . 
 key words varicocele right internal spermatic vein phlebography presentava lo sbocco della vena spermatica interna a livello della vena cava inferiore : in 5 pazienti la confluenza dello sbocco era duplice , in 60 era a ramo unico . 
il trattamento interventistico una delle soluzioni terapeutiche nel varicocele maschile ; uno dei limiti di tale metodica rappresentato dalla presenza di varianti anatomiche o di rifornimenti aberranti , che rendono complessa o impossibile la cateterizzazione e la sclerosi della vena spermatica interna . 
la conoscenza delle varianti anatomiche della presentazione della vena spermatica interna destra deve far parte del bagaglio culturale di un radiologo interventista , per poter condurre a termine la procedura , in tempi contenuti , per ridurre lesposizione radiologica . parole chiave varicocele vena spermatica interna destra flebografia introduction introduzione varicocele is dilation of the pampiniform venous plexus caused by pathological venous reflux resulting primarily from valve incontinence of the internal spermatic vein [ 1 ]  . interventional treatment of male varicocele is generally considered an effective treatment option [ 2 ] that can be used as an alternative to the various surgical procedures [ 39 ]  . 
in interventional treatment , knowledge of anatomic variants of the internal spermatic vein confluence is fundamental to both reduce radiation exposure for the patient and radiologist and to ensure technical success of the procedure . clinically , varicocele is more commonly left sided , and numerous authors have investigated this clinical entity in an attempt to define its causes and provide anatomic classification of the various phlebographic patterns of the left internal spermatic vein [ 1013 ]  . 
 the aim of our study was to bridge this gap by providing classification of right internal spermatic vein variants , which has important practical implications in the field of vascular and interventional radiology . 
for phlebographic classification of incontinence of the right internal spermatic vein , we selected cases in which the diagnostic and / or interventional procedure was performed on the right side only , thereby excluding patients il varicocele definito come una dilatazione delle vene del plesso pampiniforme , secondaria alla presenza di un reflusso venoso patologico , causato principalmente da unincontinenza valvolare della vena spermatica interna [ 1 ]  . 
la conoscenza delle varianti anatomiche dello sbocco della vena spermatica interna di fondamentale importanza nellopzione interventistica , sia per ridurre i tempi di esposizione radiologica del paziente e delloperatore , che per la buona riuscita dellatto interventistico . nella pratica clinica , il varicocele riscontrato prevalentemente a sinistra : numerosi sono gli autori che hanno dedicato particolare attenzione a tale entit clinica , alla ricerca di una fattore eziopatogenetico e alla classificazione anatomica dei vari reperti flebografici della vena spermatica interna sinistra [ 1013 ]  . 
non altrettanto interesse stato dedicato alla classificazione anatomica della confluenza della vena spermatica interna controlaterale . scopo del nostro lavoro stato quello di tentare di colmare questo vuoto , contribuendo ad arricchire un bagaglio culturale di nozioni anatomiche , in un particolare campo della radiologia vascolare ed interventistica , con importanti risvolti pratici . materiali e metodi il nostro lavoro si basato sulla analisi retrospettiva delle 3229 flebografie effettuate negli anni 19882003 . 
dallo studio delle singole schede radiologiche , il reclutamento dei pazienti era avvenuto sulla base di motivazioni differenti ( dolore , dispermia , infertilit ) , isolate o in combinazione tra treated initially for bilateral varicocele as well as those treated for left - sided varicocele first and then for right - sided varicocele . 
if the origin of the right internal spermatic vein could not be visualised , phlebography was repeated by placing the catheter tip into the right renal ve in this case , 15 ml of contrast medium was injected at 6 ml / s . 
 right internal spermatic veins were considered incompetent when the reflux of contrast medium during diagnostic phlebography allowed their direct visualisation as far as the iliac level or when , following phlebographic demonstration of incontinence of the first 5 cm , selective catheterisation s . 
la popolazione esaminata presentava unet media di 26 , 4 ( 1446 anni )  . ai fini della classificazione flebografica di una incontinenza della vena spermatica interna destra , sono stati selezionati quei casi clinici , dove la procedura diagnostica e / o interventistica era stata orientata solo ed esclusivamente a destra : abbiamo quindi volutamente escluso sia i pazienti trattati inizialmente per un varicocele bilaterale , sia quelli che , trattati prima a sinistra , sono ritornati in un secondo tempo alla nostra osservazione per essere trattati anche a destra . in tutti i casi , la flebografia era stata eseguita secondo un metodo precedentemente descritto [ 2 ] , che qui riportiamo sommariamente . 
su un tavolo radiologico ribaltabile ( siregraph cf / lx50 , siemens , erlangen , germania ) , con lausilio di un iniettore automatico ( medrad ) , stata eseguita la flebografia , dopo aver ottenuto il consenso informato . 
liniezione di mezzo di contrasto dal catetere angiografico multipurpose , la cui estremit distale situata a livello di l1l2 , durante la contemporanea manovra di valsalva , consente di opacizzare il fisiologico sbocco della vena spermatica interna sul versante antero - mediale della vena cava inferiore . tra le 3229 flebografie esaminate , sono risultati positivi per incontinenza della sola vena spermatica interna destra 93 pazienti ( 2 , 8% )  . 
 results out of 3229 phlebograms examined , 93 ( 2.8% ) showed incontinence of the right internal spermatic vein 7 / 93 cases ( 7.5% ) , the right internal spermatic vein drained caudally into the renal vein only . 
measurements showed calibres constantly > 3 mthis group of right internal spermatic veins were classed as group a on the basis of their confluence into the renal vein ( table 1 )  . in 21 / 93 patients ( 22.5% ) , phlebography demonstrated a double confluence of the internal spermatic veone branch drained caudally into the right renal vein while the other drained into the inferior vena cava . 
nei rimanenti 18 / 93 pazienti ( 19 , 35% ) con duplice sbocco della vena spermatica , il ramo confluente in vena cava inferiore era nettamente superiore a quello confluente in s . 
contrast medium injection during valsalva manoeuvre via a multipurpose angiographic catheter , the tip of which is positioned at the level of the middle - distal segment of the right renal vein , allows for opacification of the possible anomalous confluence of the right internal spermatic vein at this level ( a )  . 
in this patient , the vein has a single branch , with uniformly dilated calibre , draining into the inferior aspect of the right renal vein . selective catheterisation and contrast medium administration ( b ) allowed detailed morphological and functional evaluation ; dilated calibre ( > 34 mm ) and absence of valves are confirmed . 
liniezione di mezzo di contrasto , durante la contemporanea manovra di valsalva , dal catetere angiografico multipurpose , la cui estremit distale situata a livello del tratto medio - distale della vena renale destra , consente di opacizzare leventuale anomalo sbocco della vena spermatica interna destra a questo livello ( a )  . 
il cateterismo selettivo e liniezione di mezzo di contrasto ( b ) consentono lo studio morfologico e funzionale dettagliato : non solo sar confermato il calibro dilatato , oltre i 34 mm , ma anche lassenza degli apparati valvolari . 
sar possibile inoltre misurare la quantit di liquido sclerosante da iniettare allinterno della vena . renal vein , had a markedly larger calibre than the one flowing into the inferior vena cava . 
this group of right internal spermatic veins was classed as group b based on the double simultaneous confluence into two different venous branches ( table 1 )  . in 65 / 93 ( 69.8% ) patients , the internal spermatic vein drained into the inferior vena cava only 12 cm from the origin of the right renal vein on the anterolateral surface of the inferior vena cava . 
3 double confluence of the right internal spermatic ve the first branch , which is morphologically and functionally predominant , drains directly into the caudal margin of the right renal vein ; the second branch , significantly smaller , drains into the inferior vena cava . 
un ramo , preponderante dal punto di vista morfologico e funzionale , sbocca direttamente nel margine caudale della vena renale destra ; laltro , molto pi piccolo , va a confluire nella vena cava inferiore . 
4 double confluence of the right internal spermatic vethe right internal spermatic vein has two separate outlets : the first drains into the renal vein and the second drains into the inferior vena cava . 
despite the presence of a normal calibre , the appearance of a small amount of contrast medium just below the seemingly continent valve prompted selective catheterisation , which confirmed significant dilatation of the spermatic vein and absence of other continent valves . 
 discussion although diagnosis of male varicocele is relatively straightforward , even on the basis of the physical examination alone , and recent technological advances have improved the demonstration of venous reflux [ 14 ] , no consensus has been reached as regards the best treatment . 
the different treatment options developed over the years for varicocele confirm the difficulties in selecting a treatment option that provides both the highest success rate and the lowest rate of recurrences or discussione sebbene la diagnosi di varicocele maschile sia relativamente facile anche solo allesame obiettivo e le pi recenti acquisizioni tecnologiche hanno consentito una pi precisa definizione delle condizioni di reflusso venoso [ 14 ] , non altrettanta uniformit di vedute esiste sul tipo di trattamento da effettuare . infatti , le diverse modalit di trattamento del varicocele che si sono sviluppate nel tempo stanno a confermare le difficolt che sincontrano nel selezionare una opzione terapeutica , in grado di conseguire contemporaneamente la pi alta percentuale di risultati positivi con il minor numero di recidive o persistenze e di complicanze [ 15 ]  . il trattamento radiologico stato introdotto negli anni 80 , da iaccarino [ 16 ] e lima [ 17 ]  . 
5 double confluence of the right internal spermatic vethe right internal spermatic vein has two outlets : the branch draining into the inferior vena cava has a larger calibre but may not be easily identified on cavography due to the presence of a valve system , which could still guarantee its continence either permanently or intermittently . 
anche in questo caso lo sbocco della vena spermatica interna destra duplice : il ramo che confluisce in vena cava inferiore di calibro aumentato , ma pu non essere agevolmente identificato durante la cavografia per la presenza di un apparato valvolare che ne potrebbe garantire ancora la continenza , permanente o intermittente . 
il ramo che drena in vena renale destra filiforme , presenta una valvola parzialmente continente , sufficiente a consentire la visualizzazione dellaltro ramo durante la flebografia renale , consentendo di guidarne e agevolarne il successivo cateterismo selettivo . persistence and complications [ 15 ]  . 
radiological treatment was introduced in the 1980s by iaccarino [ 16 ] and lima [ 17 ] , and the procedure has made much progress towards being accepted as a valuable therapeutic option for varicocele , not only in men . 
despite the advantages offered by these last two approaches in aiding craniocaudal progression of the angiographic catheter , the main technical limitation to the success of all three types of interventional procedures has been the presence of anatomical variants or aberrant feeding vessels , which have hindered selective catheterisation of the internal spermatic vemost anatomical studies have therefore focused on the different characteristics of the confluence of internal spermatic veins [ 23 , 24 ] and / or aberrant feeding vessels of left varicocele [ 25 ] , which is the most frequent for considering the lower incidence of rightsided varicocele , it is not surprising that no studies have appeared in the international literature investigating the phlebographic anatomy of the right internal spermatic vein , with the exception of kadirs report [ 26 ]  . 
entrambi i rami per sono facilmente cateterizzabili ; anche in questo caso il calibro aumentato e non c traccia degli apparati valvolari . confermato il ruolo di valida alternativa allopzione chirurgica [ 1820 ]  . il trattamento interventistico si sviluppato con differenti accessi percutanei : il transfemorale ( il pi diffuso ) , il transgiugulare [ 21 ] e il transbrachiale [ 22 ]  . nonostante i vantaggi offerti da questi due ultimi approcci alla progressione cranio - caudale del catetere angiografico , in tutti e tre i tipi di metodica interventistica il maggior limite tecnico per un buon successo della soluzione terapeutica stato rappresentato dalla presenza di varianti anatomiche o da rifornimenti aberranti , che limitavano la possibilit di cateterizzare selettivamente la vena spermatica interna . il maggior numero di studi anatomici stato quindi orientato alla descrizione dei vari aspetti della confluenza delle vene spermatiche interne [ 23 , 24 ] e / o dei rifornimenti aberranti del varicocele sinistro [ 25 ] , che ritenuto il pi frequente . in virt della minore incidenza , risulta comprensibile come nella letteratura internazionale risulti praticamente assente un lavoro che focalizzi lattenzione sullanatomia flebografica della vena spermatica interna destra , ove si eccettui il testo di kadir [ 27 ]  . la revisione della nostra esperienza ultradecennale su unelevata casistica ha consentito di estrapolare 93 casi di s . 
in un piccolo gruppo di pazienti ( 7 / 93 casi , 7 , 5% ) , lo sbocco della vena spermatica interna era esclusivamente a livello del margine inferiore della vena renale : in 5 / 93 casi si trattato di un ramo unico , in 1 / 93 caso di una duplicazione della vena , mentre in 1 / 93 paziente la confluenza della vena spermatica interna destra avveniva a carico della vena renale controlaterale . nei primi 6 / 93 casi , il cateterismo selettivo e liniezione di mezzo di contrasto ne hanno consentito uno studio dettagliato delle caratteristiche : il vaso venoso si presentava con un calibro uniforme , era privo di apparati valvolari e presentava dimensioni superiori ai 3 mm di diametro trasverso , con lieve incremento distale , in prossimit della confluenza delle vene del plesso pampiniforme . questo gruppo di pazienti presentava un varicocele destro palpabile , con un franco reflusso alleco - color - doppler ; in virt delle caratteristiche della loro confluenza , grazie alla progressione cranio - caudale del catetere angiografico multipurpose , garantito dallapproccio transbrachiale e allangolazione favorevole tra lestremit del catetere e lemergenza delle vene renali e spermatiche , stato agevole procedere alla loro cateterizzazione e alla scleroterapia . pi complesso ed indaginoso stato il trattamento dellunico paziente con unorigine anomala della vena spermatica interna destra , a partenza dalla vena renale sinistra : la discrepanza tra lassente visualizzazione di un ramo incontinente a destra e il reperto eco - doppler di franco reflusso destro , oltre ad unalterazione del liquido seminale , ci ha indotto ad una ricerca dellincontinenza anche dalla vena renale di sinistra . anche in questo caso la progressione cranio - caudale del catetere angiografico ha consentito un agevole cateterismo selettivo . 
7 normal confluence of the right internal spermatic ve during cavography , the right internal spermatic vein drains into the anterolateral margin of the inferior vena cava slightly below the junction with the right renal ve the valve system is partially continent . 
durante la cavografia , si evidenzia la confluenza della vena spermatica interna destra a livello del margine antero - laterale della vena cava inferiore , poco al di sotto della unione con la vena renale destra . 
lapparato valvolare parzialmente continente : lo sbuffo di mezzo di contrasto al di sotto dellapparato valvolare testimonia un grado di normale incontinenza della vena spermatica , parzialmente nascosto dal fisiologico spasmo causato dallansia dellevento cui sottoposto il paziente . group of patients ( 7 / 93 cases , 7.5% ) , the internal spermatic vein drained into the inferior margin of the renal vethe confluence was single in 5 / 93 cases and double in 1 / 93 cases , but in 1 / 93 patients , the right internal spermatic vein drained into the contralateral renal vein the first 6 / 93 cases , selective catheterisation and contrast medium injection allowed for a detailed study of the vein characteristics . 
the vein had a uniform calibre with no valve systems and a transverse diameter > 3 mm that was slightly increased distally in proximity to the confluence of the pampiniform plexus veins . 
characteristics of their confluence , craniocaudal progression of the multipurpose angiographic catheter guaranteed by the transbrachial approach and the favourable angle between catheter tip and emergence of the spermatic and renal veins made catheterisation and sclerotherapy easy to perforfar more complex and laborious was the treatment of the single patient with abnormal origin of the right internal spermatic vein from the left renal vebesides the alteration of the seminal fluid , the discrepancy between the failure to visualise an incontinent branch on the right side and the doppler us finding of marked right reflux prompted a search for incontinence in the left renal vein as well . 
in a larger group of patients ( 21 / 93 cases , 22.5% ) , phlebography demonstrated a double confluence of the internal spermatic ve one branch drained caudally into the right renal vein while the other drained into the inferior vena cava . 
in the remaining 18 patients with double spermatic vein confluence , the vessel draining into the inferior vena cava was significantly larger than the one draining into the right renal veinjection of contrast medium through the renal vein , besides confirming the absence of an anomalous branch draining into this vein , enabled indirect visualisation and subsequent catheterisation by demonstrating opacification of the collaterals feeding the internal spermatic ve the selective study confirmed that the calibre was significantly increased in all cases . 
in the largest group of patients ( 65 / 93 cases , 69.8% ) , the internal spermatic vein drained exclusively into the inferior vena cava ( 69.8% ) at 12 cm from the origin of the right renal vein on the anterolateral surface of the inferior vena cava , as reported in many studies of normal human anatomy [ 27 , 28 ]  . the confluence was double in 5 / 93 patients and single in 60 / 93 patients . 
despite normal venous calibre , the appearance of a small amount of contrast medium below the seemingly continent valve led us to perform selective catheterisation of the vein , which confirmed the significantly increased calibre of the spermatic vein and absence of other competent valves . 
as with the left internal spermatic vein , contralateral spermatic veins might have undergone changes during embryologic development . the lesser variability of anatomic variants on the right side may be due to fewer changes affecting the right - sided venous system during the developmental period [ 29 ]  . 
the normal course of the right renal vein might explain the absence of aberrant feeding vessels of the right internal spermatic veby contrast , on the left side , the course of the left renal vein between the aorta and the superior mesenteric artery produces an increase in venous pressure , which progressively causes the veins to collapse , directly or as a result of aberrant vessel remnants of embryologic development . 
on the basis of the phlebographic anatomy , we propose a classification of right internal spermatic vein variants ( table 1 )  . knowledge of these variants can guide the percutaneous liniezione di mezzo di contrasto dalla vena renale , oltre a confermare lassenza di un ramo anomalo con confluenza in questa vena , attraverso lopacizzazione dei rami collaterali di rifornimento della vena spermatica interna , ne consentiva la indiretta visualizzazione e la successiva cateterizzazione . 
lo studio selettivo ha confermato che il denominatore comune in tutti i casi era il calibro nettamente aumentato , mentre della primitiva esistenza degli apparati valvolari , precedentemente funzionanti , rimaneva solo unimpronta sul margine laterale del vaso . mentre nei primi 3 pazienti era stato diagnosticato un varicocele palpabile , negli altri 18 era stato evidenziato la presenza del varicocele solo con leco - color - doppler . nel gruppo pi numeroso di pazienti ( 65 / 93 casi , 69 , 8% ) lo sbocco della vena spermatica interna era esclusivamente a livello della vena cava inferiore ( 69 , 8% ) , a 12 cm dallemergenza della vena renale destra , sulla superficie antero - laterale della vena cava inferiore , come viene riportato in molti testi di anatomia umana normale [ 26 , 28 ]  . mentre solo in 5 / 93 pazienti lo sbocco era duplice , negli altri 60 / 93 la confluenza era a ramo unico . 
in 52 / 93 casi il reflusso di mezzo di contrasto arrivava ad opacizzare il decorso della vena spermatica interna destra fino a livello lombare ; dopo il cateterismo selettivo dei primi 10 cm della vena , liniezione di mezzo di contrasto confermava lassenza degli apparati valvolari e il calibro nettamente aumentato . in 13 / 93 pazienti lopacizzazione della vena spermatica interna non superava i primi 5 cm dalla confluenza in vena cava superiore : pur in presenza di un calibro venoso non aumentato , la evidenza di un piccolo sbuffo di mezzo di contrasto , subito al di sotto dellapparato valvolare , apparentemente continente , ci ha portato ad effettuare il cateterismo selettivo della vena , confermando il calibro notevolmente aumentato della vena spermatica e lassenza di altri apparati valvolari continenti . erano presenti in oltre 50 pazienti le impronte della primitiva esistenza degli apparati valvolari , ormai incontinenti . come per la vena spermatica interna sinistra , anche per le vene spermatiche controlaterali ipotizzabile una loro alterazione durante lo sviluppo embriologico : la minore variabilit delle varianti anatomiche sul lato destro comprensibile con il minor rimaneggiamento che il sistema venoso di destra subisce durante la crescita [ 29 ]  . il regolare decorso della vena renale destra potrebbe fornire la spiegazione sullassenza di rifornimenti aberranti della vena spermatica interna di questo lato , a differenza di quanto accade a sinistra dove , il passaggio della vena renale sinistra tra laorta e larteria mesenterica superiore crea i presupposti per lincremento pressorio venoso , che alla base del progressivo sfiancamento venoso , diretto o mediato da vasi aberranti , residui dello sviluppo embriologico . sulla base della presentazione anatomica alla flebografia viene proposta una classificazione della vena spermatica interna destra ( tabella 1 ) , la cui conoscenza ha il vantaggio pratico di orientare metodologicamente il trattamento percutaneo per un varicocele destro , effettuato con approccio transbrachiale , iniziando dalla flebografia renale destra , proseguendo poi con la cavografia e con la ricerca manuale della confluenza della vena spermatica interna destra , per s . 
none of the three anatomical presentations preclude percutaneous treatment , especially if done with the transbrachial approach . visualisation of the internal spermatic veins at diagnostic phlebography during valsalva manoeuvre , regardless of their confluence , makes selective catheterisation a matter of patience and manual dexterity only . 
the ab subtype should be considered when a major clinical and imaging finding does not correspond to a phlebographic pattern suggestive of incontinence of the spermatic vecb is the only subtype that might create some technical difficulties during selective catheterisation due to the small proximal sizes of the venous branches . 
with an emphasis on ultrasound david wilson ( ed ) 95 pp , 88 figure , 142 illustrazioni , 3 tabelle springer berlin , heidelberg , new york ( 2005 ) isbn 3 - 540 - 66828 - 4 published online : 29 may 2006 questo agile volume della serie medical radiology / diagnostic imaging a cura di a.l. 
ogni capitolo inoltre corredato di una dettagliata e aggiornata bibliografia , utile ai fini di un approfondimento dellargomento trattato . le immagini utilizzate per illustrare il testo sono di grande qualit , estremamente esplicative e dimostrative . tra i vari capitoli , vorrei porre allattenzione dei lettori quello preparato dai colleghi di genova , maestri della disciplina ecografica , che con sapiente eloquenza dimostrano limportanza delluso delle sonde ad alta frequenza nello studio sia dei tendini che dei legamenti . 
il testo corredato da immagini molto belle , ben integrate con quelle rx , color - doppler e di rm . credo che il volume in questione sia di grande utilit sia per chi si accinga ad intraprendere questo tipo di indagini , sia per chi gi utilizza lecografia in pediatria , metodica che , spesso e senza impiego di radiazioni ionizzanti ( caveat in pueris ! ) , permette di porre diagnosi corrette e rapide , evitando iter diagnostici spesso lunghi e fuorvianti . 
schoepf2 1dipartimento di radiologia , universit cattolica del sacro cuore , roma , italy 2department of radiology , medical university of south carolina , 169 ashley avenue , charleston , sc 29425 , usa 3istituto di radiologia diagnostica e interventistica , university j.w. 
the purpose of this study was to evaluate contrastenhanced electrocardiogram ( ecg ) - gated 64 - slice computed tomography ( ct ) angiography of the thorax as a triage tool in patients with acute equivocal chest pa material and methods . 
technical principles and diagnostic algorithms for using a single ecg - gated 64 - slice ct scan for triple rule - out of acute pulmonary embolism , aortic dissection , acute coronary syndromes and other diseases of the chest are introduced . 
the total length of hospitalisation and charges for emergency department care at the time of discharge were compared with a matched control population that underwent catheter angiography for emergent cardiac workup . 
of the 23 patients , 11 presented without pathological findings , two with extensive pulmonary embolism , two with definite coronary artery disease ( cad ) but stenosis < 50% and eight with significant cad ( > 50% stenosis )  . 
our initial experience shows that ecg - gated 64slice ct angiography of the entire thorax is technically feasible and enables rapid triage of patients to determine underlying cardiac and noncardiac reasons for chest pathis test may thus help to significantly reduce costs and length of hospitalisation . prospective studies involving larger groups of patients are required to confirm these findings . 
si riferiscono i principi tecnici e lalgoritmo diagnostico per lutilizzo dellesame tc 64 - strati del torace che consente con ununica scansione la triplice possibilit di diagnosi di esclusione di dolore toracico acuto , differenziando la sindrome coronarica acuta dalla dissezione aortica e dalla embolia polmonare , e di riscontrare patologie aggiuntive . 
il tempo totale di ospedalizzazione e le spese sostenute nel dipartimento di emergenza sono stati confrontati con quelli di un analogo gruppo di controllo in cui si eseguito il cateterismo cardiaco nel workup cardiologico demergenza . 
dei 23 pazienti , 11 sono stati dimessi senza il riscontro di reperti patologici , 2 con embolia polmonare massiva , 2 con evidente malattia coronarica ( cad ) ma stenosi < 50% ed 8 con malattia coronarica significativa ( stenosi > 50% )  . 
la nostra esperienza iniziale dimostra che lesame angio - tc con gating cardiaco dellintero torace tecnicamente eseguibile e consente una rapida ed accurata valutazione delle principali cause cardiache e non cardiache di dolore toracico . pertanto questo esame potrebbe determinare una significativa riduzione nei costi e nelle spese di ospedalizzazione . 
this approach has high specificity ( 90% ) but inadequate sensitivity ( < 50% ) , above all during the first hours [ 3 ]  . hospitalisation is compulsory for patients with typical signs of unstable angina ( ua ) or ami [ 4 , 5 ] whereas those without risk factors for coronary heart disease ( chd ) , without typical cardiac chest pain and with a normal electrocardiogram ( ecg ) , are usually discharged . diagnostic uncertainty arises , however , for a substantial number of people who are usually subjected to coronarography , an expensive and invasive procedure that is unable to identify other causes of chest pain such as aortic dissection or pulmonary embolisa large number of patients require further imaging investigations , with the result of longer hospitalisation , higher costs and increased exposure to ionising radiation . the possibility of differentiating cardiac and noncardiac causes of chest pain without the use of invasive procedures would be of considerable benefit for both the patients and the hospital [ 68 ]  . the advent of multidetector computed tomography ( mdct ) scanners and cardiac - gating techniques has made it possible to perform a noninvasive study of the heart and coronary tree in selected groups of patients . 
the latest 64slice mdct scanners can acquire images of thoracic vessels with high resolution and retrospective gating , thus allowing evaluation of coronary arteries , aorta and pulmonary arteries . because the high prognostic value of ct angiography in excluding significant coronary artery disease ( cad ) is unanimously accepted [ 8 ] , the negative findings of a diagnosticquality ct angiography scan would allow ruling out cardiac and noncardiac causes of chest pain [ 9 ]  . 
per la diagnosi di infarto miocardico acuto ( ima ) viene ancora ampiamente utilizzato lalgoritmo proposto dalla world health organization ( who ) nel 1979 , che sebbene recentemente modificato [ 1 ] , rimane ancora un punto di riferimento [ 2 ]  . tale approccio consente di avere unalta specificit ( 90% ) ma una sensibilit inadeguata ( < 50% ) , soprattutto nelle prime ore [ 3 ]  . 
lospedalizzazione obbligata per i pazienti con i segni tipici dellangina instabile ( ai ) o ima [ 4 , 5 ] , mentre quelli che non hanno fattori di rischio per cardiopatia coronarica ( cad ) , non hanno un dolore toracico tipicamente cardiaco ed hanno un ecg normale , vengono solitamente dimessi . lincertezza diagnostica si pone tuttavia per un sostanziale numero di soggetti che sono in genere sottoposti ad un esame coronarografico , una procedura onerosa ed invasiva , che non in grado di identificare altre cause di dolore toracico , come la dissezione aortica o lembolia polmonare . 
la possibilit di differenziare cause cardiache e non cardiache di dolore toracico senza lutilizzo di procedure invasive apporterebbe notevoli benefici sia per i pazienti che per le spese delle strutture ospedaliere [ 68 ]  . con lavvento delle apparecchiature tc multidetettore ( tcmd ) e le tecniche di cardiosincronizzazione , divenuto possibile lo studio non invasivo del cuore e dellalbero coronarico in gruppi selezionati di pazienti . 
le ultime tcmd a 64 strati , consentono lacquisizione ad alta risoluzione , con sincronizzazione retrospettiva dei vasi del torace , permettendo la valutazione delle arterie coronarie , dellaorta e delle arterie polmonari . pertanto , poich lalto valore prognostico negativo dellangio - tc per lesclusione di malattia coronarica significativa unanimemente riconosciuto [ 8 ] , un esame angio - tc di sufficiente qualit diagnostica risultato negativo permetterebbe di escludere cause cardiache e non cardiache di dolore toracico [ 9 ]  . scopo di questo lavoro discutere il razionale e descrivere le premesse tecniche per lesecuzione dellangio - tc a 64 strati nel triage dei pazienti con dolore toracico atipico , valutandone limpatto nella gestione del malato e delle aziende ospedaliere . materiali e metodi lo studio stato condotto previa approvazione dellinstitutional review board . 
 stato valutato mediante studio angiografico del torace con tcmd a 64 strati , per la triplice esclusione di coronaropatia , dissezione aortica ed embolia polmonare , un gruppo di 23 pazienti ( 14 maschi , 9 femmine ) g . 
in equivocal cases , a negative ct scan can avoid electrocardiograph ( ecg ) and markers monitoring and a positive examination can orientate the appropriate therapy . adapted from braunwald et al . 
lesame tc , nel paziente con elevata probabilit pre - test ( sopraslivellamento st e / o marker cardiaci positivi ) di risultare positivo per sindrome coronarica acuta ( sca ) non apporta alcun beneficio . 
2 ridefinizione di ima secondo un comitato congiunto di esperti dellamerican college of cardiology e della european society of cardiology pubblicato nel settembre 2000 sia sul jacc [ 1 ] che sullo european heart journal . ical acute chest pain and were treated with conventional procedures , including catheter angiography : 14 men and 9 women aged 3785 years ( mean 5812 )  . 
given the small number of subjects and the variability in costs and length of hospitalisation in patients undergoing different interventional procedures , a subanalysis was performed for patients who did not undergo specific intervention ( stenting , bypass , fibrinolysis ) : 18 patients in the study group and 15 in the control group . statistical analysis was performed using students t test ( for independent data ) and the mann - whitney rank sum test for variables without equal variance . finally , the number and relative percentage of imaging tests requested and performed during hospitalisation were compared for the two complete groups and for subgroups . 
considerato il numero esiguo dei soggetti e la variabilit in termini di costi e tempi di ricovero nei pazienti sottoposti a differenti procedure interventistiche , una subanalisi stata inoltre eseguita per i pazienti non sottoposti ad interventi terapeutici specifici ( stenting , bypass , fibrinolisi ) : 18 pazienti del gruppo di studio e 15 del gruppo di controllo . lanalisi statistica stata effettuata mediante students t test ( per dati indipendenti ) ; un test di mann - whitney ( somma dei ranghi ) stato inoltre eseguito per le variabili con varianza diseguale . 
in two ( 9% ) , examination demonstrated mild stenoses of one or more coronary branches , in four ( 18% ) moderate lesions and in four ( 18% ) critical stenoses or complete occlusion . 
distribution of pathological findings is shown in figure 4 . of the eight cases with moderate cad , only one was treated with immediate interventional procedure ( angioplasty and positioning of an intracoronary stent ) ; the remaining were treated with aggressive medical therapy and modification of risk factors in view of their age and clinical condition , and two were scheduled for surgical placement of an aortocoronary bypass during hospitalisation . the two cases of pulmonary embolism were treated with fibrinolytic therapy . 
 il mezzo di contrasto non ionico utilizzato , isovue 370 mgi / ml , ( bracco diagnostics , princeton , nj , usa ) , stato somministrato per via endovenosa con accesso antecubitale destro con agocannula da 18 g , tramite iniettore automatico a doppia testa stellant d ( medrad , pittsburgh , pa , usa )  . 
sono stati somministrati 510 mg ev di metoprololo prima della scansione ai pazienti con frequenza cardiaca uguale o superiore a 70 bpm . risultati dei 23 pazienti del gruppo di studio in 11 casi ( 48% ) lesame risultato completamente negativo per arteropatia coronarica , embolia polmonare e dissezione aortica . 
in 2 casi ( 9% ) sono state identificate stenosi di lieve entit a carico di uno o pi rami coronarici , in 4 casi ( 18% ) lesioni significative , in 4 casi ( 18% ) stenosi critiche o completa occlusione . le lesioni stenosanti significative ( 50% ) sono state tutte confermate dalla successiva coronarografia ( tabella 2 )  . 
b esami di imaging eseguiti nei due gruppi con lesclusione dei pazienti sottoposti a procedutre interventistiche . ment , further imaging studies were ordered and performed . overall , the study group underwent 17 chest x - ray examinations ( 74% of patients ) , five single photon emission ct ( spect ) studies for myocardial perfusion ( 22% ) , eight doppler ecg studies ( 35% ) and one ultrasound ( us ) study of the lower limbs ( 4% )  . 
catheter angiography was carried out in eight patients ( 35% ) , and mdct of the chest was performed in all patients . in the control group , there were 22 chest x - ray examinations ( 96% ) and one radiographic study of the left hand ( 4% ) ; five spect studies for myocardial perfusion ( 22% ) ; two chest ct scans for suspected pulmonary embolism ( 9% ) and one chest ct for suspected aortic dissection ( 4% ) ( in total , 13% ) and eight doppler echocardiography studies ( 35% )  . 
catheter angiography was performed in all patients . figures 4 and 5 show the differences in the number of examinations , as percentages , between the two groups as a whole , considering only subgroups without indications for specific treatment ( stenting , bypass , fibrinolysis )  . for the study group , the relative percentages in the no - intervention subgroup were : chest x - ray 72% , spect 22% , doppler ecg 27% ; catheter angiography was done in five patients ( 27% ) and chest mdct in all patients . 
ecg is estimated to be nondiagnostic in around 50% of all subjects presenting to the emergency department with chest pain ; even patients with acute or evolving infarction may initially not manifest the typical ecg changes , or the ecg tracing may be impossible to interpret ( treatment with digitalis , left - bundle - branch block , ventricular preexcitation , left ventricular hypertrophy with systolic overload , intracavitary ventricular pacemaker )  . moreover , routinely performed enzyme tests do not have adequate diagnostic accuracy within the first 48 h of symptom onset . in effect , measurement of creatine kinase isoenzyme - mb ( ck - mb ) , which has long been the reference standard for diagnosis of patient with chest pain , has a sensitivity of 30% within 3 h of onset , 46.5% within 6 h and 82.3% at 69 h , reaching maximum sensitivity after 912 h . 
moreover , specificity is low , as the enzyme is widely represented not only in the heart but also in skeletal muscle , similar to myoglobin . the more recent cardiac troponins ( ctni and ctnt ) are specific for cardiac damage but are unable to discriminate the underlying mechanism ( their concentration may also be elevated as a result of myocarditis , pericarditis , dilated cardiomyopathy , etc . ) and are characterised by an initial release mechanism similar to that of ck - mb so that they achieve acceptable sensitivity levels only 48 h after onset of symptoms . 
despite the higher costs , specific chest pain observation units ( cpous ) [ 10 , 11 ] use ischaemia provocation tests ( usually stress test on exercise bicycle ) in addition to ecg monitoring and cardiac enzyme tests to improve diagnostic sensitivity in unstable angina . 
 in consideration of the high percentage of patients with equivocal clinical presentation who are found to be free of cad but who may be affected by other causes of acute chest pain ( pulmonary embolism , aortic dissection and also pericarditis , neoplasm , pneumonia ) , there is clearly a need for a rapid and reliable diagnostic tool to detect both cardiac and noncardiac disease . 
with the introduction of the newer generations of mdct scanners , diagnostic imaging has made huge steps in this direction . the quality of thoracic images and above all of the thoracic vasculature is greatly affected by cardiac pulsation . movement artefacts can prevent assessment of coronary arteries but may also make it difficult to evaluate the root and ascending segment of the aorta and pulmonary artery branches . 
retrospective synchronisation of spiral ct acquisition entrambi i parametri nel gruppo di studio ( valori medisd ) : us $11841 , 719161 e 1 , 72 , 3 giorni nel gruppo di studio versus us $20289 , 310258 , 4 e 32 , 3 giorni nel gruppo di controllo , con p < 0 , 001 e p = 0 , 009 rispettivamente . 
si stima , infatti , che lelettrocardiogramma non sia diagnostico in circa il 50% di tutti i soggetti che si presentano al dipartimento di emergenza con dolore toracico ; anche nei pazienti con infarto acuto o in evoluzione , possono inizialmente mancare le tipiche modificazioni del tracciato , o questo pu non essere interpretabile ( terapia digitalica , blocco di branca sinistro , preeccitazione ventricolare , ipertrofia ventricolare sinistra con sovraccarico sistolico , presenza di pace - maker endocavitario ventricolare )  . 
inoltre , i test enzimatici routinariamente eseguiti non raggiungono unaccuratezza diagnostica adeguata entro le prime 48 ore dallinsorgenza dei sintomi . effettivamente la misura della ck - mb ( isoenzima mb della creatinchinasi ) , che da tempo il gold standard per la diagnosi del paziente con dolore toracico , mostra una sensibilit del 30% circa entro tre ore dallesordio clinico , del 46 , 5% entro sei ore , dell82 , 3% tra sei e nove ore , e raggiunge il valore massimo tra le nove e le dodici ore . 
le troponine ( ctni e ctnt ) , di pi recente utilizzo , sono specifiche per danno miocardico , ma non ne discriminano il meccanismo ( la loro concentrazione pu aumentare anche in conseguenza di miocarditi , pericarditi , cardiopatia dilatativa , etc . ) e sono caratterizzate da uniniziale cinetica di rilascio simile a quella della ck - mb , per cui raggiungono livelli accettabili di sensibilit soltanto quattro - otto ore dopo linizio dei sintomi . 
dal momento che i pazienti in genere giungono allosservazione molto prima di questo intervallo di tempo , inevitabile un periodo di osservazione che prolunga il tempo di ospedalizzazione . in unit specifiche di osservazione per il dolore toracico ( cpou ) [ 10 , 11 ] per migliorare la sensibilit diagnostica dellangina instabile , a spese per di un costo di gestione pi elevato , si utilizzano test provocativi di ischemia ( di solito la prova da sforzo su cicloergometro ) unitamente al monitoraggio elettrocardiografico ed ai test enzimatici . 
considerata lalta percentuale di pazienti con presentazione clinica ambigua che risultano poi esenti da patologia steno - ostruttiwith ecg ( ecg gating ) enables visualisation of the coronary tree while preventing doubling and blurring artefacts , which often lead to major diagnostic errors [ 1216 ]  . 
the advent of mdct scanners has allowed coverage of a large anatomic volume with retrospective gating with high resolution , even in the longitudinal plane , during a single breathhold [ 17 ]  . 
 thanks to these technological features , we can now avail ourselves of a tool enabling noninvasive overall evaluation of the entire arterial system for the diagnosis of atherosclerosis and other vascular diseases with adequate anatomical detail . 
however , the maximum z - axis spatial resolution obtainable with ecg gating with 4 - , 8 - , or 16 - detector - row scanners is limited by the relatively long acquisition time due to data oversampling . these scanners therefore allow only small volumes to be acquired with high - resolution and ecg - gated protocols ( e.g. the heart for the study of the coronary tree ) , but they cannot cover the entire chest anatomy in a single scan . 
the state - ofthe - art in ct angiography in the study of cad involves acquisition of submillimetre sections [ 18 ] , which cannot be obtained in the study of large anatomical volumes . 
despite the excellent performance of the above - mentioned mdct scanner generations , a large proportion of patients require the use of beta blockers for heart - rate control if this is fast or irregular . 
6 retrospectively electrocardiograph ( ecg ) - gated 64 - slice computed tomography ( ct ) angiography of the entire thorax in a patient with acute chest pavolume rendered images unequivocally demonstrate aortic dissection of the descending aorta with intimal flap and true and false lumen , without thrombosis . 
diagnostic quality display of the coronary arteries [ left main ( lma ) , left anterior descending ( lad ) , circumflex ( cx ) , right coronary artery ( cdx ) ] and their branches ( d1 , d2 , d3 ) is achieved from the same data set . 
con lintroduzione delle successive generazioni di apparecchiature tc multidetettore la diagnostica per immagini ha compiuto enormi progressi in questo senso . la qualit delle immagini toraciche e soprattutto delle strutture vascolari toraciche influenzata in maniera sostanziale dalla pulsazione cardiaca . 
gli artefatti da movimento rendono di fatto invalutabili le arterie coronarie , ma possono anche rendere difficoltosa la valutazione della radice e del tratto ascendente dellaorta e delle diramazioni delle arterie polmonari . 
lutilizzo della sincronizzazione retrospettiva dellacquisizione tc spirale con il tracciato elettrocardiografico simultaneamente registrato ( ecg - gating ) , permette da una parte la visualizzazione dellalbero coronarico , e dallaltra di evitare gli artefatti da sdoppiamento e da sfocamento , responsabili spesso di importanti errori diagnostici [ 1216 ]  . lavvento degli scanner tc multidetettore ( tcmd ) ha consentito di coprire un sostanziale volume anatomico con gating retrospettivo , ad elevata risoluzione anche sul piano longitudinale , durante una singola apnea [ 17 ]  . grazie a queste caratteristiche tecnologiche per la prima volta si potuto disporre di uno strumento per la valutazione globale non invasiva dellintero sistema arterioso per la diagnosi della patologia aterosclerotica e di altre patologie vascolari con un dettaglio anatomico adeguato . 
comunque , con apparecchi tcmd a 4 , 8 o a 16 file di detettori , la massima risoluzione spaziale ottenibile sullasse z con tecnica ecg - gated , limitata dal tempo di acquisizione relativamente lungo , in relazione al sovracampionamento dei dati . con queste apparecchiature quindi , possibile acquisire con protocolli ad alta risoluzione e cardiosincronizzazione , soltanto volumi relativamente piccoli , come per esempio quello cardiaco per lo studio dellalbero coronarico , ma non possibile coprire con ununica scansione lintera anatomia toracica . lattuale stato dellarte per langio - tc delle arterie coronarie nella valutazione di dettaglio della malattia coronarica , prevede lacquisizione di sezioni anatomiche submillimetriche [ 18 ] , difficilmente ottenibili nello studio di ampi volumi anatomici . 
nonostante le elevate performance delle suddette generazioni di scanner tcmd , necessario , in una sostanziale percentuale di pazienti , lutilizzo di farmaci beta - bloccanti per il controllo della frequenza cardiaca , quando questa elevata o irregolare . 
i tempi di apnea richiesti sono relativamente lunghi , specialmente nel caso di malati critici e quindi poco collaboranti . analogamente , i tempi di scansione sono proibitivi per la valutazione simultanea del circolo arterioso polmonare e sistemico in ununica apnea , con protocolli che prevedono lalta risoluzione con gating cardiaco . 
further , a gantry rotation time equal to 330 ms significantly improves temporal resolution in cardiac studies , allowing an acquisition time of 165 ms for all rates , which can be reduced to 83 ms with the use of multisegment reconstruction algorithms . the need to use these algorithms , which are dependent on heart rate and can produce artefacts , is , however , definitely reduced . 
con lapparecchiatura utilizzata nel nostro studio , per esempio , si raggiunge una risoluzione spaziale isotropica inferiore a 0 , 4 mm , che migliora notevolmente la visualizzazione di dettaglio delle piccole strutture vascolari . il tempo di rotazione del gantry pari a 330 ms inoltre , migliora significativamente la risoluzione temporale nellesecuzione di esami cardiaci , permettendo un tempo di acquisizione dei dati di 165 ms per tutte le frequenze , che pu essere abbassato fino ad 83 ms con lutilizzo degli algoritmi di ricostruzione multisegmentaria . la necessit di utilizzare questi algoritmi , che invece sono dipendenti dalla frequenza cardiaca e possono produrre artefatti , risulta comunque decisamente ridotta . 
questo comporta un notevole aumento di qualit delle acquisizioni cardiache per frequenze elevate ed irregolari , una minor esigenza di controllo del ritmo cardiaco , e di conseguenza aumenta significativamente la percentuale di pazienti per cui possibile ottenere un esame completamente diagnostico . 
i tempi di apnea richiesti inoltre ( in media 15 s per la sola acquisizione cardiaca e 18 , 5 s per lintero torace ) , anche questi ridotti rispetto alle precedenti generazioni di tcmd , consentono una migliore gestibilit anche di quei pazienti in condizioni instabili o poco collaboranti . 
7a , b a 59 - year - old woman presenting to the emergency department with acute chest pacontrast - enhanced , retrospectively electrocardiograph ( ecg ) gated 64 - slice study of the entire chest with 0.6 - mm collimation was acquired within 19 s total scan time . 
lo studio con mezzo di contrasto dellintero torace stato acquisito con apparecchiatura a 64 strati , con gating retrospettivo , collimazione di 0 , 6 mm e tempo totale di scansione di 19 secondi . 
compared with prospective gating , which implies a smaller radiation dose but a greater susceptibility to artefacts due to heart - rate disturbances , retrospective gating allows more flexibility in temporal reconstruction of images ( reconstruction can be synchronised , a posteriori , with any moment in the cardiac cycle and consequently the best temporal window can be obtained for each of the vessels being studied )  . 
in addition , it allows evaluation of image quality both with and without the multisegment reconstruction algorithm , but more importantly , it allows more rapid acquisition of the entire chest anatomy and reconstruction of images with overlapping sections , providing a longitudinal resolution around 20% less than the slice thickness itself . 
although the clinical utility of ct angiography has not been routinely and officially recognised in many countries , the technique is widespread in the united states , and its use by radiology and cardiology departments has led to its inclusion in routine clinical practice , at least as a tool for early diagnosis to discriminate between the different classes of cad : mild , moderate , severe or occlusive . for these reasons , the use of 64 - slice ct angiography of the chest in the diagnostic workup of equivocal chest pain is technically feasible and able to guarantee rapid triage of g . 
rispetto alla sincronizzazione prospettica che implica una minor dose di esposizione dei pazienti ma una maggior suscettibilit agli artefatti dovuti alle turbe del ritmo cardiaco , quella retrospettiva garantisce una maggior flessibilit nella ricostruzione temporale delle immagini ( possibile , a posteriori , sincronizzare la ricostruzione con qualsiasi istante del ciclo cardiaco , e di conseguenza si pu ottenere la migliore finestra temporale di ricostruzione per ogni vaso in esame ) , permette di valutare la qualit delle immagini con e senza lalgoritmo di ricostruzione multisegmentaria ma soprattutto di acquisire lintera anatomia toracica in minor tempo e di ricostruire le immagini con sovrapposizione di strato , in modo da ottenere una risoluzione spaziale longitudinale di circa il 20% inferiore allo spessore di strato stesso . sebbene langio - tc coronarica non abbia ancora un riscontro clinico routinariamente ed ufficialmente riconosciuto in molti paesi , negli stati uniti la sua diffusione ed il suo utilizzo nei dipartimenti di diagnostica per immagini e di cardiologia ne hanno portato allintegrazione nella pratica clinica quotidiana se non altro come strumento di diagnosi precoce , per discriminare le differenti classi di malattia coronarica : lieve , moderata , severa , occlusiva . 
8a - c a 57 - year - old man presenting to the emergency department with acute chest pain : nondiagnostic electrocardiogram ( ecg ) ; initial cardiac blood markers negative for acute myocardial ischaemia . 
contrast - enhanced , retrospectively ecg - gated 64 - slice study of the entire chest with 0.6 - mm collimation was acquired within 21 s total scan time , ruling out acute pulmonary embolism as a reason for chest pain ( a )  . 
lo studio tc a 64 strati dellintero torace durante somministrazione di mezzo di contrasto , con gating cardiaco e spessore di strato pari a 0 , 6 mm , acquisito in 21 secondi , consente lesclusione dellembolia polmonare tra le cause del dolore toracico ( a ) per questo paziente . 
multiplanar reconstruction ( mpr ) images in oblique anterior perspective ( a , b ) along the left and right main pulmonary arteries demonstrate massive pulmonary embolism ( pe ) with embolus extending into lobar and segmental branches , especially of the lower lobes . 
volume rendered display of the heart and curved mpr ( c ) along the left anterior descending coronary artery shows diffuse atherosclerotic disease , with calcified and noncalcified plaques but without critical stenosis . 
le ricostruzioni mpr secondo piani anteriori obliqui ( a , b ) lungo le arterie polmonari principali di destra e sinistra mostrano la presenza di ep massiva con grossolani difetti di riempimento endoluminali nel tratto distale di queste ed estensione del materiale trombo - embolico nei rami lobari e segmentari , prevalentemente dei lobi inferiori . 
 definition of appropriate clinical indications still needs , however , careful consideration . clearly , patients with a very low likelihood of acute cad , with frankly benign symptoms suggesting early discharge from the emergency department , are unlikely candidates for the examination . 
even in cases eligible for hospitalisation , with ecg and enzyme monitoring the examination may prove beneficial . results obtained with our small but adequate study population , although only first experiences , appear to support our discussion so far . 
in one case , a moderate stenosis estimated to be 50% by mdct turned out to be 80% , and therefore severe , in the angiographic study , and in another case , a severe stenosis ( 90% ) was reported as a complete occlusion . 
statistical analysis of the comparison between the study group and a similar group managed with the conventional protocol , and the subanalysis carried out after excluding from both groups patients who underwent specific treatments , such as stenting , aortocoronary bypass and fibrinolysis , to eliminate the resulting variability in terms of hospitalisation costs and length also provided interesting results . 
in either case , both total hospitalisation time and charges for emergency department care showed significant reduction in the group undergoing 64 - slice ct as part of the diagnostic work - up . 
naturalmente , i pazienti con una probabilit pre - test molto bassa di coronaropatia acuta , con sintomi francamente benigni che lascino presupporre una rapida dimissione dal dipartimento di emergenza , difficilmente saranno candidati allesecuzione dellesame . 
i pazienti per cui , invece , in assenza delle classiche alterazioni ecg ed inizialmente enzimatiche , persista incertezza diagnostica tale da giustificare un esame coronarografico durgenza , o da pianificarne leventuale esecuzione durante il ricovero , possono essere considerati idonei allo studio tc . 
anche nei casi candidati ad ospedalizzazione con monitoraggio elettrocardiografico ed enzimatico , lesame pu risultare vantaggioso . i risultati ottenuti con ladeguata ma esigua popolazione di studio selezionata , per quanto iniziali , sembrano confortare quanto fin ora discusso . lalta percentuale di esami completamente negativi , pari al 48% , il riscontro di due casi di embolia polmonare ( fig . 9 ) come causa extra - cardiaca di dolore toracico ( 9% ) , e lottima correlazione nella stima delle stenosi coronariche tra angio - tc e coronarografia tradizionale ( tabella 2 ) , sono tutti elementi che possono giustificare lutilizzo della tcmd a 64 strati come strumento di triage nei dipartimenti di emergenza . 
in particolare tutte le lesioni stenosanti significative ( 50% ) identificate sono state confermate dalla coronarografia come tali ; in un caso una stenosi significativa definita del 50% con lo studio mdct e risultata dell80% , quindi severa , secondo lo studio angiografico , ed in un altro caso una stenosi severa ( 90% ) stata poi riferita come completa occlusione . lanalisi statistica nel confronto tra il gruppo di studio ed unanaloga popolazione seguita con il protocollo convenzionale , e la subanalisi effettuata escludendo da entrambi i gruppi i pazienti sottoposti a terapie specifiche quali stenting , bypass aorto - coronarico e fibrinolisi , per eliminare la variabilit da queste derivante in termini di costi e tempi totali di ospedalizzazione , hanno anchesse fornito elementi interessanti . 
in entrambi i casi infatti , sia il tempo totale di ospedalizzazione che le spese derivanti dalla gestione dei pazienti nel dipartimento di emergenza con le differenti strategie diagnostiche , hanno mostrato una riduzione signig . 
contrast - enhanced 64 - slice multidetector computed tomography ( mdct ) angiography of the entire thorax with a gantry rotation time of 330 ms and retrospective electrocardiograph ( ecg ) gating rules out acute pulmonary embolism as a reason for chest pain ( a )  . 
maximum intensity projection in a right anterior oblique perspective of the left anterior descending ( lad ) coronary artery shows atherosclerotic plaque in the inferior , anteromedial wall of the lad . 
langiografia toracica con tcmd a 64 strati , con tempo di rotazione del gantry di 330 ms e gating cardiaco retrospettivo permette di escludere lembolia polmonare come causa del dolore ( a )  . 
la ricostruzione mirata per le arterie coronarie evidenzia patologia aterosclerotica diffusa ( b )  . la ricostruzione con proiezione di massima intensit ( mip ) secondo un piano anteriore , obliquo , destro , dellarteria discendente anteriore ( lad ) , evidenzia una placca nella parete inferiore , antero - mediale del vaso . 
lanalisi con la finestra per il parenchima polmonare dellintero torace documenta incidentalmente un carcinoma a cellule squamose ( d ) del lobo polmonare superiore sinistro ficativa nel gruppo in cui langio - tc a 64 strati del torace stata introdotta nellalgoritmo diagnostico . questa riduzione si basa sulla possibilit di escludere accuratamente la presenza di patologie cardio - toraciche in tempi brevi , in un maggior numero di pazienti . 
this provides further indication of the techniques diagnostic potential and relative impact on patient management in the presence or absence of a specific cause of chest pa conclusions chest ct with a 64 - slice multidetector scanner allows clear identification of different causes of chest pain and helps establish an accurate early diagnosis of chd . 
our initial experience suggests that its use in emergency departments for triage of patients with chest pain and atypical clinical presentation would lead to shorter hospital stays and reduced costs combined with better risk - benefit ratio for patients . 
in effetti , mentre per i pazienti ricoverati perch realmente necessitanti di procedure terapeutiche specifiche si rendono spesso utili ulteriori indagini diagnostiche e controlli seriati , nel caso in cui si deve solo escludere la presenza di patologia toracica significativa , la disponibilit di un esame tc dellintero torace risulta spesso definitivamente esaustiva . 
la nostra iniziale esperienza suggerisce che il suo utilizzo nei dipartimenti di emergenza per il triage dei pazienti con dolore toracico a presentazione clinica atipica porterebbe ad una riduzione dei tempi e dei costi di ospedalizzazione , in associazione ad una migliore gestione del rapporto rischio / beneficio per i malati . 
di guglielmo published online : 29 may 2006 istituto di radiologia , irccs policlinico san matteo , universit di pavia , pavia , italy , fax : + 39 - 0382 - 527970 , e - mail : istirad@smatteo.pv.it looking through the pages of a prestigious international radiology journal , i was struck by a small photograph with two lively , penetrating eyes peering out at me and smiling gently . 
plinio ( as we informally call him and as he is known by radiologists worldwide ! ) is about to receive a gold medal from the society of interventional radiology ( sir ) in the united states . 
it recalls his original technical contributions to interventional radiology ( transluminal angioplasty , transhepatic biliary drainage ) and emphasises his extensive research in the field , with over 400 scientific publications to his credit . 
the article also recalls that he gave rise to a true school a large , strong , very active and combative school to which we can only add that it is one of the most beautiful schools of italian radiology . i think that this international award and reward won by an italian radiologist is an honour for all italian radiologists , and for this reason , it should also be announced in the official journal of our radiology society , the italian society of medical radiology ( sirm )  . 
and this not only to extend our warmest congratulations to plinio rossi but also that it may encourage and spur the young and very young generations of italian radiologists . congratulations plinio ! scorrendo le pagine di una prestigiosa rivista internazionale di radiologia siamo stati colpiti da una piccola fotografia dalla quale due occhi penetranti e vivaci ci guardavano con un dolce sorriso . 
plinio ( cos lo chiamiamo noi familiarmente , ma cos conosciuto in tutto il mondo radiologico ! ) ricever a giorni , in america , una medaglia d ' oro dalla society of interventional radiology , sir . nella lunga e circostanziata motivazione che segue , il prof . plinio rossi viene presentato come uno dei padri fondatori della radiologia interventistica e come co - fondatore della societ americana di neuroradiologia . 
vengono ricordati i suoi contributi tecnici originali apportati nella disciplina interventistica ( angioplastica transluminale , drenaggio biliare transepatico ) e sottolineata l ' importanza della sua produzione scientifica , forte di oltre 400 pubblicazioni . 
ma viene dato particolare rilievo alle sue doti di umanit e di signorilit che lo hanno reso stimato e benvoluto da tutti . viene ancora ricordato che ha saputo creare una vera scuola . una scuola numerosa , forte , attivissima , battagliera e noi possiamo aggiungere una delle pi belle scuole della radiologia italiana . abbiamo pensato che questo riconoscimento internazionale dato a un radiologo italiano vada a onore di tutta la radiologia italiana e che per questo sia giusto darne notizia anche sulla rivista ufficiale della nostra sirm . 
all patients were examined prior to treatment with us - cpd study and then with contrast - enhanced power doppler ( cepd ) examination ( cepd ) with the use of us contrast agent ( sonovue , bracco ) , together with clinical assessment and laboratory tests . 
after initial us , cpd and cepd were performed to assess enhancement of the thickened bowel wall with the use of a reference box and a semiquantitative scoring syste results . 
this study demonstrates the importance of us - cpd in the follow - up of patients with crohns disease and suggests systematic use of the us contrast agent , which can improve diagnostic performance of abdominal us study . 
it also provides more information about patients both in the acute phase and during follow - up , thus improving treatment planning and better monitoring of treatment efficacy . key words ultrasonography contrast media crohns disease riassunto obiettivo . 
sono stati studiati 15 pazienti con diagnosi di mc ileale , 12 dei quali esaminati in fase acuta e successivamente dopo impostazione terapeutica a 3060 giorni ; 3 pazienti sono invece stati valutati durante la fase di quiescenza clinica . 
lo studio conferma limportanza delletg - pd nel follow - up dei pazienti affetti da mc e suggerisce il sistematico impiego di mdc ecografico che si dimostrato in grado di migliorare la performance diagnostica nellesplorazione ecografia addominale e di fornire informazioni diagnostiche pi dettagliate in pazienti con mc in fase acuta e nel corso di followup per una corretta scelta terapeutica e per il monitoraggio dellefficacia del trattamento . parole chiave ecografia mezzi di contrasto malattia di crohn a . 
in some cases , surgery may be inevitable due to the possible stenotic or inflammatory complications with a very high percentage of postsurgery relapse . correct clinical management of the patient requires assessment of disease activity to monitor treatment efficacy , implement different or alternative treatments where necessary and assess the prognosis and onset of complications . 
crohns disease activity index ( cdai ) , harvey bradshaw index , etc . ] , but these have been hotly debated , being based purely on clinical and at times subjective criteria . 
however , the most important clinical trials in cd have used cdai [ 1 ] as an indicator of disease activity in terms of clinical parameters , together with biohumoural markers [ leukocyte count , erythrocyte sedimentation rate ( esr ) , c - reactive protein ( crp ) , alpha - 1 - antitrypsin , alpha - 1 - glycoprotein acid , etc . ] , which nonetheless have low specificity [ 2 , 3 ]  . two - dimensional ultrasonography ( us ) , which is able to demonstrate indirect signs of inflammation , has undergone a natural diagnostic evolution with the use of the colour power doppler ( cpd ) module , which in turn is able to identify an increase in parietal vascularity . 
the use of us with administration of the recently introduced contrast media consisting of encapsulated microbubbles ( second - generation contrast media ) , which remain for a lengthy period in intestinal wall microcirculation , seems to provide accurate mapping of the intraparietal vasculature , even identifying low - velocity flows in small - diameter vessels . the aim of this study was to demonstrate the role of us examination performed with contrast media as an integration to standard us and conventional cpd in the study of disease activity in cd for early detection of changes indicating remission or acute exacerbation . materials and methods la malattia di crohn ( mc ) una patologia molto complessa caratterizzata da innumerevoli problematiche dal punto di vista eziopatogenetico , clinico , anatomo - patologico , diagnostico e terapeutico . 
il decorso variabile : periodi pi o meno lunghi di remissione sono interrotti da riacutizzazioni ; talora inevitabile il ricorso alla chirurgia a causa delle possibili complicanze stenotiche o flogistiche con percentuale di recidiva post - intervento molto alta . 
ai fini della corretta gestione clinica del paziente , risulta di fondamentale importanza la valutazione dello stato di attivit della malattia per monitorare lefficacia del trattamento , instaurare eventualmente presidi terapeutici differenti o alternativi e valutare la prognosi e linsorgenza di complicanze . 
sono stati proposti negli anni numerosi metodi clinici di valutazione dello stato di attivit con sistemi a punteggio ( es cdai , harvey bradshaw index , etc . ) , oggetto di controversie perch improntati su criteri puramente clinici e talora soggettivi . 
tuttavia i pi importanti trials clinici sullargomento hanno utilizzato il cdai [ 1 ] come indicatore dello stato di malattia dal punto di vista clinico , e parametri bioumorali ( leucociti , ves , proteina c reattiva , lalfa - 1 - antitripsina , lalfa - 1 - glicoproteina acida , etc . ) per scarsamente specifici [ 2 , 3 ]  . lecotomografia bidimensionale , in grado di dimostrare segni indiretti di flogosi , ha trovato una naturale evoluzione diagnostica con lutilizzo del modulo color power doppler ( cpd ) , capace di rilevare lincremento della vascolarizzazione parietale . 
tuttavia i risultati di questa metodica non sono ottimali soprattutto nel definire precocemente linsorgenza di recidive o nel valutare il viraggio verso linattivit . lavvento dellecografia con somministrazione di mezzi di contrasto ecografici di recente introduzione , costituiti da microbolle gassose stabilizzate ( mdc di seconda generazione ) che permangono per lungo tempo nel microcircolo tissutale della parete intestinale , sembra permettere un accurato studio della mappa vascolare intraparietale evidenziando anche flussi a bassa velocit in vasi di piccolo calibro . lo scopo di questo lavoro dimostrare il ruolo dellesame etg con mdc ( pdce ) come indagine integrativa allesame ecotomografico standard e color power doppler convenzionale nello studio dello stato di attivit della mc evidenziando precocemente il viraggio verso fasi di remissione o di riacutizzazione . between january and may 2004 , we examined 15 patients ( nine females , six males ) between the ages of 17 and 61 years suffering from ileal cd diagnosed with small - bowel enema and endoscopic examinations with biopsy . 
twelve patients were examined in the acute phase with follow - up at predetermined intervals of 2030 and 6080 days while the remaining three were examined during clinical quiescence . in total , 39 segments of diseased bowel loops were examined , 25 of which were classified to be in the active phase materiali e metodi nel periodo gennaio - maggio 2004 , presso il s.c.d.u. 
di radiologia dellospedale san luigi di orbassano ( to ) sono stati esaminati 15 pazienti ( 9 donne , 6 uomini ) di et compresa tra i 17 e i 61 anni , affetti da mc con localizzazione ileale , dimostrata con clisma del tenue ed esami endoscopici associati a biopsia . 
di questi 15 pazienti , 6 erano gi stati sottoposti a resezione ileale con anastomosi ileocolica . dodici pazienti sono stati esaminati in fase acuta e successivamente ad intervalli predeterminati a 2030 e 6080 and the remaining 14 in the inactive phase according to the cdai scoring systeon the same day as the us examination , the patients underwent clinical assessment and targeted laboratory tests ( leukocyte count , crp , esr , alpha - 1 - glycoprotein - acid )  . 
patients with a score between 100 and 150 underwent additional laboratory tests , with 4 points assigned for crp , 3 for alpha - 1 - glycoprotein - acid , 2 for leukocyte count and 1 for esr . 
in this cdai grey zone ( 100150 ) patients with a laboratory score 4 were classified as active . on the same day , patients underwent a standard b - mode us examination , a conventional cpd examination and lastly a contrast - enhanced power doppler ( cepd ) examination , with the use of us contrast material ( sonovue , bracco )  . 
the b - mode examination was performed with a sonoline elegra device ( siemens , erlangen , germany ) using a convex 3.5 - mhz probe and then a linear 7.5to 10 - mhz probe with tissue harmonic imaging ( thi ) , which improves contrast resolution . 
the colour signal within the box was measured and converted into a score based on the number of spots : score 0 = no signal ; score 1 = 12 signals ; score 2 = 35 signals ; score 4 = more than 5 signals . 
i pazienti sono stati sottoposti nello stesso giorno dellindagine ultrasonografica a una valutazione clinica e ad esami di laboratorio mirati ( conta dei globuli bianchi , pcr , ves , alfa - 1 - glicoproteina - acida )  . 
i pazienti con lindice clinico cdai > 150 sono stati classificati attivi ; coloro con un punteggio compreso tra 100 e 150 sono stati sottoposti a ulteriore valutazione laboratoristica a punteggio assegnando 4 punti alla pcr , 3 punti allalfa - glicoproteina - acida , 2 punti alla conta dei globuli bianchi ed 1 punto alla ves . 
in questa zona grigia ( cdai 100150 ) sono stati considerati attivi i pazienti con punteggio laboratoristico superiore o uguale a 4 punti . nello stesso giorno i pazienti sono stati sottoposti ad indagine ecotomografica in b - mode standard ( etg ) , con eco color power doppler convenzionale ( cpd ) ed infine con power doppler contrast enhancement ( pdce ) , con utilizzo di mdc ecografico ( sonovue , bracco )  . 
lecografista non era a conoscenza del risultato clinico - laboratoristico . lindagine ecotomografica stata eseguita con attrezzatura sonoline elegra , siemens , utilizzando la sonda convex 3 , 5 mhz e successivamente la sonda lineare 7 , 510 mhz , con la funzione di armonica tissutale ( thi ) , che consente una migliore risoluzione di contrasto . 
3 alla valutazione power doppler evidenza di uno scarso numero di segnali intraparietali ( score 01 ) in ansa con pareti ispessite ( inattiva )  . the second - generation sonovue us contrast agent . 
the us transmission frequency was kept at the lowest level possible ( about 3.3 mhz ) capable of balancing the resonance frequency of the contrast material , which reacts in an optimal manner to this method of insonation by emitting selective harmonic signals . 
the acoustic power is kept low ( 10%15% ) , with a mechanical index ( mi ) of 0.20.3 , so as not to rupture the microbubbles , which would otherwise undergo elastic deformations with the generation of harmonics , with a considerably long halflife in the order of several minutes . 
4 alla valutazione power doppler evidenza di numerosi segnali intraparietali ( score 3 ) in anse con pareti ispessite . ottimizzate su livelli idonei alla rilevazione di flussi lenti ( pulse repetition frequence , prf , a 600800 hz )  . 
stata quindi posizionata una finestra di studio ( color box ) delle dimensioni di 1 , 5 cm2 nel contesto della parete dellansa patologica ; allinterno stato rilevato il segnale colore successivamente sottoposto a valutazione a punteggio sulla base del numero degli spots : score 0 = nessun segnale ; score 1 = 12 segnali ; score 2 = 35 segnali ; score 3 = pi di 5 segnali . 
la frequenza di trasmissione ultrasonora stata regolata al livello pi basso possibile ( circa 3 , 3 mhz ) in grado di centrare la frequenza di risonanza del mdc che , con tale modalit di insonazione , reagisce in maniera ottimale emettendo segnali armonici selettivamente rilevati in ricezione . 
la potenza acustica viene mantenuta a basso livello ( 10%15% ) , con indice meccanico , mi , 0 , 20 , 3 in modo da non evocare la rottura delle microbolle che invece andranno incontro a deformazioni elastiche con produzione di armoniche , con una emivita nel circolo piuttosto lunga , di diversi minuti . 
stato iniettato il mdc in una vena antidecubitale del gomito ( ago 1921 g ) in due boli da 2 , 5 cc aspettando la dissoluzione delle microbolle compartment , thus facilitating identification of the microvascular network , which is richer in the active phase of disease . the contrast agent was injected into an antecubital vein of the elbow ( 19to 21 - gauge needle ) in two 2.5 - cc boluses , the second bolus being injected once the microbubbles of the first had dissolved . 
when the injection is performed and subject to insertion of the chronometer to measure the time of maximum enhancement , the power doppler function is set with prf to the lowest level possible so as to optimise visualisation of the vessels with slow blood flow and with colour gain set so as to prevent blooming artefacts , which are inevitably present in the early phases of maximum enhancement . 
at this point , dynamic reduction of the colour gain ( to about 3040 db ) is required to obtain an image without artefacts . the cepd signal was also examined in a 1.5 - cm2 colour box positioned at the thickened bowel wall , which is small in size so as to optimise signal sensitivity and reduce the frame rate which , if high , hinders correct real - time assessment of the image . 
the video - recorded procedure then undergoes detailed semiquantitative analysis of the number of colour spots : score 1 = poor or absent signal ; score 2 = low signal ( 78 spots ) ; score 3 = moderate signal ( > 78 spots ) ; score 4 = marked score . 
al momento delliniezione , previo inserimento del cronometro per il rilevamento del tempo di massima presa di contrasto , si imposta la funzione power doppler settata con prf a livello pi basso possibile per ottimizzare la visualizzazione di vasi con flusso ematico lento e con guadagno - colore regolato in modo da evitare artefatti da saturazione del segnale ( blooming ) , peraltro inevitabilmente presenti nelle prime fasi di massimo enhancement ; si rende perci necessaria a questo punto la riduzione dinamica del guadagno - colore ( a circa 3040 db ) per ottenere unimmagine priva di artefatti . 
anche il segnale pdce viene esaminato in un box di interesse del diametro massimo di 1 , 5 cm2 , posizionato nello spessore parietale , che di piccole dimensioni al fine di ottimizzare la sensibilit del segnale e di ridurre il frame - rate che , se alto , non consente una corretta valutazione real - time dellimmagine . 
il segnale - colore nel box di rilevazione viene valutato a punteggio sulla base della qualit e del numero degli spots - colore : score 1 = segnale scarso o assente ; score 2 = segnale modesto ( 78 spots ) ; score 3 = segnale moderato ( > 78 spots ) ; score 4 = segnale marcato . 
cepd examination was in line with clinicallaboratory findings in 96% of segments in that 24 / 25 segments presented moderate - to - marked enhancement following administration of the contrast material . 
cpd examination of the same segments showed agreement with the risultati lesame ecotomografico condotto su 25 segmenti ileali ritenuti attivi dalla preliminare valutazione clinico - laboratoristica ( tabella 1 ) ha messo in evidenza una maggiore sensibilit del pdce rispetto al cpd ; nel 96% dei segmenti si rilevata concordanza pdce - clinico - laboratoristica in quanto 24 / 25 segmenti presentavano un enhancement parietale moderato - marcato dopo somministrazione di mdc . 
lesame cpd degli stessi segmenti attivi si dimostra in accordo con il quadro clinico - laboratoristico in 22 / 25 segmenti , con sensitable 2 subgroup of segments classified as inactive at crohn 's disease activity index ( cdai ) and positive at contrast - enhanced power doppler ( cepd ) , which developed relapse table 3 subgroup of segments classified as inactive : sensitivity values of the parameters wall thickness , contrast - enhanced power doppler ( cepd ) and colour power doppler ( cpd ) tabella 2 sottogruppo di segmenti ritenuti inattivi al cdai e positivi al pdce che hanno sviluppato recidiva tabella 3 sottogruppo di segmenti ritenuti inattivi : valori di sensibilit dei parametri spessore di parete , pdce e cpd 1 / 4 : wall thickness 5 mm 3 / 4 : wall thickness < 5 mm 4 / 4 : cepd + 0 / 4 : cepd1 / 4 : cpd + 3 / 4 : cpd1 / 4 : spessore di parete 5 mm 3 / 4 : spessore di parete < 5 mm 4 / 4 : pdce + 0 / 4 : pdce1 / 4 : cpd + 3 / 4 : cpd3 / 10 ( 30% ) : wall thickness 5 mm 7 / 10 ( 70% ) : wall thickness < 5 mm 1 / 10 ( 10% ) : cepd + 9 / 10 ( 90% ) : cepd2 / 10 ( 20% ) : cpd + 8 / 10 ( 80% ) : cpd3 / 10 ( 30% ) : spessore di parete 5 mm 7 / 10 ( 70% ) : spessore di parete < 5 mm 1 / 10 ( 10% ) : pdce + 9 / 10 ( 90% ) : pdce2 / 10 ( 20% ) : cpd + 8 / 10 ( 80% ) : cpda . 
the parameter thickened wall considered the most sensitive of those assessed with standard us had a sensitivity of 80% and was greater than 5 mm in 20 / 25 cases . disease activity was accompanied by a wall thickness of less than 5 mm in 20% ( 5 / 25 ) of cases . 
in one case , cepd and cpd examinations were both negative whereas clinical findings were suggestive of disease activity and the wall thickness was greater than 5 mm . the 14 ileal segments considered inactive at cdai - laboratory assessment included a subgroup of four segments , two of which showed slightly higher biohumoural parameters while maintaining a negative cdai index ( table 2 )  . 
in three of these four segments , there was agreement between clinicallaboratory indices and both the parameter wall thickness ( less than 5 mm ) and cpd ( negative )  . 
il parametro spessore parietale ritenuto pi sensibile tra quelli valutati in corso di etg standard ha una sensibilit dell80% ed risultato superiore a 5 mm in 20 casi su 25 ; lattivit di patologia si accompagna in circa il 20% dei casi ( 5 / 25 ) a uno spessore di parete inferiore a 5 min 1 caso il pdce ed il cpd sono entrambi negativi a fronte di una valutazione clinica ritenuta di attivit e con spessore di parete maggiore di 5 mm . tra i 14 segmenti ileali ritenuti inattivi allesame cdailaboratoristico , si riconosce un primo sottogruppo da 4 segmenti , 2 dei quali hanno presentato un leggero rialzo di 12 parametri bioumorali , pur mantenendo un indice cdai negativo ( tabella 2 )  . 
in 3 di questi 4 segmenti si ha concordanza con gli indici clinico - laboratoristici sia per il parametro spessore di parete ( inferiore a 5 mm ) sia con il cpd ( negativo )  . 
tutti i 4 pazienti portatori di segmenti patologici inattivi sono stati monitorati dal punto di vista clinico - laboratoristico e hanno sviluppato recidiva di malattia entro tre mesi dalla prima osservazione , con intervallo variabile da 30 a 80 giorni . 
sempre tra i 14 segmenti ileali ritenuti inattivi allesame cdai - laboratoristico stato isolato un secondo sottogruppo da 10 segmenti ( tabella 3 ) nel quale in 9 casi su 10 si osservata una corrispondenza clinico - laboratoristica - strumentale con il pdce , in 8 su 10 con il cpd e in 7 su 10 valutando solo lo spessore di parete . 
all four patients with inactive diseased segments were monitored with clinical - laboratory examinations , and they developed disease recurrence within 3 months of initial observation , with an interval varying from 30 to 80 days . 
the 14 ileal segments classified as inactive at the cdai - laboratory assessment included a second subgroup of ten segments ( table 3 ) in which there was agreement between clinical - laboratory findings and cepd in 9 / 10 cases , cpd in 8 / 10 cases and wall thickness alone in 7 / 10 cases . 
in the three segments with wall thickness greater than 5 mm , cepd examination was in agreement with clinical - laboratory findings . in the subgroup of segments classified as inactive ( cdai negative ) , two cases stand out . 
in the first , cpd was positive , cepd negative and wall thickness less than 5 m in the second , cepd was negative , with moderate enhancement following administration of contrast material , cpd was negative and wall thickness was less than 5 mm . table 4 summarizes sensitivity , specificity , positive predictive vale ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy of the three techniques . discussion clinical management of patients with cd is considerably facilitated by identification of the active phases of the disease . many studies [ 49 ] have concentrated on the optimal use of imaging examinations capable of objectively and reliably showing pathological changes resulting from disease activity . 
obtaining information regarding response to treatment is therefore useful , as is differentiating a thickening of the intestinal wall secondary to transmural fibrosis a situation that would inevitably require surgery from inflammation , which may respond to appropriate medical treatment . 
during the active phase , pathological changes include an increase in splanchnic blood flow , mesenteric vascularisation and neoangiogenesis in the intestinal wall , with an increase in flow in the dilated arteriolar and venular districts . b - mode examination is proposed as the main examination for identifying some of the indirect signs of disease activity [ 8 ]  . 
increase in wall thickness greater than 4 mm , particularly when accompanied by other parameters such as hypertrophy of the mesenteric adipose tissue , has a sensitivity of 80% [ 7 , 10 ] whereas specificity is lower ( 65%75% )  . these findings are in agreement with the results of our study ( sensitivity 80% , specificity 70% ) , in which a cutoff value of wall thickness of 5 mm was imposed to obtain adequate specificity . 
patients with wall thickness between 4 and 5 mm usually undergo further us monitoring 34 months later . the problem is related to the possibility that parietal thickening , in addition to being secondary to inflammation , may also be caused by fibrosis and scarring . 
in this instance , the cpd module comes into its own , given its ability to provide information on vascular density , which is higher during the active phase of the disease . 
risulta quindi rilevante ottenere informazioni sulla risposta alla terapia oppure differenziare ispessimenti della parete intestinale secondari a fibrosi transmurale , situazione che richiede inevitabilmente una soluzione chirurgica , da fenomeni flogistici sensibili a terapie mediche appropriate . 
durante la fase di attivit le modificazioni anatomo - patologiche sono rappresentate da un incremento del flusso ematico splancnico , della vascolarizzazione mesenterica e della neoangiogenesi nel contesto della parete intestinale con aumento del flusso in distretti arteriolari e venulari vasodilatati . 
lincremento dello spessore di parete oltre i 4 mm , specie se in presenza di altri parametri come lipertrofia del tessuto adiposo mesenteriale , dotato di valori di sensibilit di circa l80% [ 7 , 10 ] ma il valore di specificit risulta pi basso ( 65%75% )  . 
tali risultati della letteratura sono in linea con quelli rilevati nel nostro studio ( sensibilit 80% , specificit 70% ) ove , per , per ottenere unadeguata specificit stato considerato un cut - off dello spessore parietale di 5 m i pazienti con ispessimento di parete compreso tra 4 e 5 mm sono solitamente sottoposti nuovamente ad altro controllo etg dopo 34 mesi . 
si pertanto posto in primo piano lutilizzo del modulo color power doppler ( cpd ) , in grado di fornire informazioni sulla densit vascolare che , come noto , risulta incrementata durante la fase di attivit della malattia . 
 [ 11 ] hanno riportato una corrispondenza clinico - laboratoristica - strumentale ( cpd ) molto alta per il gruppo di pazienti attivi ( 40 su 44 ) mentre su 35 segmenti ritenuti inattivi secondo la valutazione cdai - laboratoristica solo in 14 casi non stato riscontrato il segnale - colore . 
 [ 12 ] hanno enfatizzato limportanza dellaccoppiamento dei due parametri ispessimento parietale - cpd in grado di ottenere risultati molto interessanti soprattutto in pazienti attivi ( vpp 94% )  . la valutazione dello stato di attivit stato oggetto di importanti studi anche con la tc spirale e clisma - tc che hana . 
 [ 11 ] reported very high clinical - laboratory imaging agreement for the group of active patients ( 40 / 44 ) whereas the colour signal was encountered in only 14 of 35 segments classified as inactive according to the cdailaboratory assessment . 
 [ 12 ] underlined the importance of combining the two parameters of wall thickness and cpd , as this provides very interesting results , particularly in active patients ( ppv 94% )  . assessment of the degree of activity has also been the focus of some important studies using spiral computed tomography ( ct ) and ct enteroclysis , which showed significant correlation between wall enhancement displaying a stratified appearance associated with the comb sign of mesenteric vessels and disease activity [ 13 , 14 ]  . 
diagnostic accuracy of this examination ( 75%85% ) is in part constrained by difficulty in obtaining adequate distension of the lumen , a situation that does not allow for correct measurement of the visceral wall , and by the subjective nature of the assessment of parietal enhancement , which is significantly correlated to the degree of disease activity only when it is intense and evident . associated with this in many cases is the difficulty in distinguishing inactive segments from segments in the initial phase of activity or barely active . 
lastly , it should be borne in mind that spiral ct and ct enteroclysis involve the use of ionising radiation ( absorbed dose 7.813.3 msv ) and are therefore not indicated for patient follow - up , particularly in young patients of fertile age affected by chronic intestinal diseases and who must undergo frequent monitoring [ 15 ]  . magnetic resonance ( mr ) currently uses fast sequences dedicated to the study of organs in motion , such as the small bowel together , with oral and intravenous contrast media , which promote correct distension of the intestinal lumen and optimal study of the parietal vasculature . 
many studies have shown significant correlation between the degree of activity and parameters such as wall thickness , wall enhancement and length of the diseased segment [ 1619 ]  . 
recent studies have emphasised the correlation between disease activity and wall enhancement following administration of gadolinium , disease activity and wall t2 - weighted signal , and disease activity and the t2 - weighted signal of fibrofatty proliferation on fat - suppressed images [ 20 , 21 ]  . 
 [ 16 ] , reported sensitivity of 92% and specificity of 75% in identifying the degree of activity , taking into consideration the study per patient and not per diseased segment . 
when considering this parameter , findings proved to be markedly different ( sensitivity 59% and specificity 93% ) in that there was a high number of false negatives owing to difficulty in identifying in the same patient activity of all intestinal localisations , parno dimostrato una correlazione significativa tra lenhancement murale con aspetto stratificato associato ad opacizzazione a pettine dei vasi mesenterici e lattivit di malattia [ 13 , 14 ]  . 
laccuratezza diagnostica di tale indagine ( 75%85% ) comunque in parte limitata dalla difficolt ad ottenere unadeguata distensione del lume ( tc spirale ) , situazione che non permette la corretta misurazione della parete viscerale , e dalla soggettivit nel valutare il grado di enhancement parietale che significativamente correlato ad uno stato di attivit di malattia solo quando intenso ed evidente . 
infine non bisogna sottovalutare che la tc spirale e il clisma - tc comportano lutilizzo di radiazioni ionizzanti ( dose assorbita 7 , 813 , 3 msv ) e pertanto risultano controindicati nel follow - up di pazienti , spesso giovani ed in et fertile , affetti da patologie croniche intestinali , che si devono sottoporre a frequenti controlli [ 15 ]  . 
la rm attualmente si avvale di sequenze veloci e dedicate allo studio di organi in movimento come lintestino e dellimpiego di mdc orali ed ev che favoriscono la corretta distensione del lume intestinale e lottimale studio della vascolarizzazione murale . 
molti lavori hanno rilevato una significativa correlazione tra lo stato di attivit ed il prodotto di pi parametri : ispessimento di parete , enhancement di parete e lunghezza del segmento patologico [ 1619 ]  . 
recenti studi hanno sottolineato la corrispondenza attivit - enhancement murale dopo gadolinio - iperintensit murale in t2 con fs ( fat suppression ) - iperintensit in t2 fs del grasso periviscerale ipertrofico [ 20 , 21 ]  . 
 [ 16 ] hanno riportato una sensibilit del 92% e una specificit del 75% nel rilevare lo stato di attivit considerando lo studio per paziente e non per singolo segmento patologico . 
considerando questultimo parametro i risultati si sono rivelati nettamente differenti ( sensibilit 59% e specificit 93% ) in quanto si ha un elevato numero di falsi negativi per la difficolt di rilevare nello stesso paziente lattivit di tutte le localizzazioni intestinali specie se a livello del colon e con spessore parietale ridotto . 
considerando che i presidi terapeutici vengono comunque adottati sul paziente e non sul singolo segmento , quindi pi corretto dare maggiore importanza ai dati per paziente , caratterizzati da alta sensibilit e da discreta specificit ( 92% e 75% )  . 
in questo studio il segno considerato pi accurato lenhancement stratificato di parete , espressione inoltre di stati di attivit anche di recente insorgenza dove si verifica dapprima lispessimento e linfarcimento cellulare flogistico della sottomucosa . 
attualmente molti autori osservano il fenomeno della presa di contrasto valutandone lentit e le modalit di distribuzione nella parete ricaticularly if they were at colon level and with reduced wall thickness . 
however , given that treatment is performed on the patient and not on the individual segment , it is therefore more correct to emphasise findings per patient , characterised by high sensitivity and reasonable specificity ( 92% and 75% )  . 
in this study , the most accurate sign appears to be stratified wall enhancement , which is also the expression of activity of even recent onset where there is first thickening and inflammatory - cell infiltration of the submucosa . 
in addition , as noted for ct , there is still the problem of the numerous false positives associated with quantification of parietal enhancement , which may be difficult to interpret in borderline cases . in this scenario , the use of contrast - enhanced us is finding increasing acceptance . 
most studies currently concentrate on the phenomenon of contrast enhancement , assessing extent and distribution within the wall , thus obtaining patterns that prove to be in correlation or not with the degree of activity [ 23 ]  . our study uses a different kind of approach based on identification in an area of interest ( colour box ) of the harmonic signal originating from the microbubbles and using power doppler with dedicated contrast - specific software ( eci ) , which can be very easily compared with data provided by conventional cpd performed shortly before administration of contrast material . 
this provides objective assessment of signal quantity , which can be considered an expression of parietal vascular density . with regard to the cepd study using first - generation contrast media , kratzer et al . 
 [ 25 ] used a semiquantitative assessment similar to the one we used , relying on a chromaticnumerical study of the power doppler signal in the reference colour box rather than morphological observation of intensity and extent of parietal enhancement , which is probably more open to subjective interpretation . 
the overall results of our study ( table 4 ) , which considers all statistical parameters , show that cepd is diagnostically superior to cpd and , of course , wall thickness in assessing the degree of activity of bowel segments affected by cd [ 2628 ]  . 
according to our findings , cepd is significantly superior diagnostically to cpd and the parameter wall thickness measured during the b - mode study ( diagnostic accuracy 94% for cepd compared with 86% for cpd and 77% for b - mode us ) , thanks to its increased ability to measure the signal generated by the microbubbles in small vessels and with slow flow . 
in particular , cepd has 96% sensitivity and ppv in active diseased segments , which overall indicate greater reliability in defining disease activity and demonstrating increased parietal vascularity linked to neoangiogenesis at an early stage . 
ne deriva una valutazione oggettiva della quantit del segnale espressione della densit vascolare parietale . per quanto concerne la modalit di studio pdce utilizzando il mdc di prima generazione , kratzer et al . 
 [ 25 ] , nelle loro esperienze , si sono avvalsi di una valutazione semiquantitativa simile a quella da noi utilizzata affidandosi ad uno studio cromatico - numerico del segnale power doppler nel box colore di riferimento piuttosto che allosservazione morfologica dellentit e dellestensione dellenhancement murale , probabilmente pi soggetto ad interpretazioni soggettive . dai risultati complessivi emersi dal nostro studio ( tabella 4 ) , considerando la totalit dei parametri statistici , si apprezza una sostanziale superiorit diagnostica del pdce , rispetto al cpd e naturalmente allo spessore parietale , nel valutare lo stato di attivit di segmenti patologici affetti da mc [ 2628 ]  . 
questultimo , secondo i dati ottenuti , presenta una sostanziale superiorit diagnostica rispetto al cpd ed al parametro spessore di parete rilevato in corso di etg standard ( accuratezza diagnostica 94% del pdce vs 86% del cpd e 77% delletg standard ) in virt della maggiore capacit di rilevare il segnale generato dalle microbolle in vasi di piccolo calibro e con flusso lento . 
in particolare il pdce , in segmenti patologici attivi , presenta il 96% di sensibilit e vpp che nel complesso indicano una maggiore affidabilit nel definire lattivit della malattia dimostrando precocemente lincremento della vascolarizzazione parietale legata alla neoangiogenesi . 
lalta specificit ( 90% ) e vpn ( 90% ) sono parametri che rappresentano i valori pi significativi tra le indagini del panorama diagnostico suggerendo limportante ruolo della metodica nel monitoraggio dei pazienti attivi , con la possibilit di valutare correttamente la risposta alla terapia , individuando eventualmente il viraggio verso una fase di inattivit . nella nostra casistica esiste un sottogruppo di 4 casi in cui stato rilevato un aspetto che potrebbe aprire prospettive diagnostiche significative . 
in questi pazienti con segmenti ritenuti inattivi al cdai , talora con lieve alterazione di indici bioumorali , ma positivi al pdce si verificata , in corso di stretto controllo clinico - laboratoristico , linsorgenza di una ripresa di malattia . tale risultato , che necessita di ulteriori conferme , potrebbe avere un significato di notevole valore . 
 infatti ipotizzabile un importante ruolo premonitore del pdce , maggiormente sensibile nel dimostrare precocemente il viraggio verso lattivit dei segmenti inizialmente ritenuti inattivi e quindi nello svelare linsorgenza di recidive . 
cepd , which is more sensitive in demonstrating the colour change towards the activity of segments initially classified as inactive , may play an important early warning role and therefore reveal the onset of relapse . 
the possibility of such forewarning could enable more appropriate management of inactive patients with doubtful biohumoural markers as well as inactive postsurgery patients . within the group of segments classified as inactive , there was a single case where there was discordance between clinical - laboratory and cepd findings . 
if this were so , this case would be a part of the subgroup of four segments in which there was a discrepancy between cdai ( negative ) and cepd ( positive ) , which could be justified by the ability of the imaging examination to identify relapse at an early stage . analysis of the findings also reveals two cases characterised by particular situations . 
in the first , cepd and cpd were negative whereas classification of the clinical examination was active ( cdai positive ) and wall thickness was greater than 5 mm , most likely due to fibrotic scarring , which erroneously affects the cdai score whereas cpd and , better still , cepd are thought to be capable of demonstrating the real pathological modification . 
in the second case , cdai was negative , cpd positive and cepd negative , with wall thickness less than 5 ma later cpd examination of the segment proved to be negative , suggesting an initial setting error , a situation that is more likely to occur at cpd than at cepd . in some cases , findings seem to cast doubt on cdai , and it is commonly held that an imaging parameter such as cepd , particularly if equipped with quantitative assessment , is more reliable than cdai , even when the latter is associated with specific biohumoural markers . 
evidence of greater sensitivity of cepd with respect to cdai in the four cases of disease recurrence within the following 3580 days therefore is not unexpected . in terms of specificity , diagnostic performance of cepd seems to be higher than that of cpd and , above all , of the parameter wall thickness in assessing the importance of wall thickening . 
in three specific cases in our study , in segments classified by cdai as inactive and with wall thickness greater than 5 mm , cepd was negative , suggesting the increase in wall thickness was due to fibrosis . 
it can therefore be stated that contrast - enhanced us examination , if performed as a supplementary examination to the standard us study , is highly reliable , even more so than cpd , in differenmo reperto risulta peraltro descritto anche nella casistica di alcuni lavori scientifici di recente pubblicazione [ 25 ]  . importante possibile significato premonitore questo potrebbe consentire una pi adeguata gestione dei pazienti inattivi con un quadro bioumorale dubbio e dei pazienti inattivi post - chirurgici . allinterno del gruppo dei segmenti considerati inattivi , si osserva un unico caso che presenta discordanza clinico - laboratoristica - pdce , in cui si rileva moderato enhancement dopo somministrazione di sonovue peraltro associato a spessore di parete inferiore a 5 mm e a cpd negativo . 
in questultima evenienza entrerebbe a far parte del sottogruppo da 4 segmenti in cui si verificata una discrepanza cdai ( negativo ) - pdce ( positivo ) , giustificata eventualmente dalla maggiore precocit dellindagine strumentale nel rilevare la riaccensione della malattia . dallanalisi dei risultati emergono infine due casi caratterizzati da situazioni particolari . 
il primo presenta pdce e cpd negativi a fronte di una valutazione clinica ritenuta di attivit ( cdai positivo ) e spessore di parete maggiore di 5 mm , attribuibile in prima ipotesi a fenomeni fibrotico - cicatriziali che erroneamente condizionano la valutazione clinica a punteggio cdai , mentre il cpd ed ancor meglio il pdce sarebbero in grado di dimostrare la reale modificazione anatomo - patologica . 
il secondo , cdai negativo con cpd positivo , pdce negativo e spessore di parete inferiore a 5 mm , ha mostrato negativit allesame cpd ad un controllo successivo di tale segmento , inducendo quindi ad ipotizzare un iniziale errore di settaggio , situazione che pi facilmente si pu verificare in corso di esame cpd rispetto al pdce . i risultati ottenuti sembrano , in alcuni casi , mettere in discussione lindice a punteggio di riferimento ed opinione comune che un parametro strumentale come il pdce , specialmente se dotato di valutazione quantitativa , risulti pi attendibile del cdai stesso seppur associato a specifici parametri bioumorali . 
non quindi un dato inatteso levidenza di una maggior sensibilit del pdce rispetto al cdai - laboratorio nei 4 casi precedentemente descritti in cui si verificata una recidiva di malattia entro 3580 giorni . la performance diagnostica del pdce , in termini di specificit , sembra essere migliore rispetto a quella del cpd e soprattutto del parametro spessore parietale nella valutazione del significato dellispessimento di parete . 
in order to confirm this finding , a study on a much broader patient population is required . a further boost to diagnostic reliability of cepd is expected from technological improvements , which together with dedicated software are expected to provide quantitative , numerical and objective assessment of the parietal area of interest for a more detailed study of parietal enhancement . conclusions our study , which was performed on patients with ileal cd , confirms the important role of us in the study of this disease , particularly during follow - up . 
intuibile che , a conferma di tale significativo dato , sia necessario uno studio su una popolazione di pazienti numericamente pi rilevante . un ulteriore impulso per incrementare lattendibilit diagnostica del pdce atteso dai miglioramenti tecnologici in grado di fornire , con software dedicati , valutazioni quantitative , numeriche e oggettive nellarea parietale di interesse per un pi dettagliato studio dellenhancement parietale . conclusioni il nostro studio , condotto su pazienti con mc ileale , ha confermato limportante ruolo dellecotomografia nello studio di questa patologia , soprattutto in corso di follow - up . 
morana1 1istituto di radiologia , ospedale cafoncello , treviso , italy 2istituto di radiologia , cro , aviano , italy 3istituto di radiologia , universit di verona , policlinico g.b. 
the studies were evaluated for the following parameters : site of obstruction ( hilar , proximal or distal ) , presence of intraor extrahepatic dilation of bile ducts , morphology of ductal stenosis ( gradual tapering or abrupt ending ) , morphology of the lesion ( mass like or circumferential ) , dimension , signal intensity before contrast medium administration and lesion enhancement after administration of contrast mediufinally , we assessed the most useful sequence for the diagnosis . 
in order to evaluate mr accuracy in the diagnosis of malignant obstruction of extrahepatic bile ducts , we prospectively reviewed mr examinations of 74 patients affected by obstructive jaundice ( 55 malignant lesions and 19 inflammatory lesions )  . 
fifty - six percent of the lesions appeared as a circumferential thickening ( infiltrative growth ) ; the remaining lesions had a mass - like appearance ( expansile growth )  . 
most lesions were hypo ( 49% ) or isointense ( 49% ) in t1 - weighted sequences and hyper ( 49% ) or isointense ( 51% ) in t2 - weighted sequences . 
i parametri valutati sono stati : sede di ostruzione ( ilare , prossimale o distale ) ; presenza di dilatazione delle vie biliari intraed extra - epatiche ; morfologia della stenosi duttale ( progressivo affinamento o stop brusco ) ; aspetto morfologico della neoplasia ( mass like o circonferenziale ) ; dimensioni ; intensit del segnale in fase precontrastografica e tipo di enhancement dopo mdc . 
la maggior parte delle lesioni risultata ipo ( 49% ) o iso - intensa ( 49% ) nelle sequenze pesate in t1 e iper ( 49% ) o isointensa ( 51% ) nelle sequenze pesate in t2 . 
la rm ha dimostrato buona sensibilit ( 91% ) ma scarsa specificit ( 47% ) nel caratterizzare la stenosi come maligna giudicando un elevato numero di lesioni benigne appearance ( extraductal or growing into the choledochus )  . 
on the other hand , lesions with parietal thickening , particularly if smaller than 1 cm , require endoscopic cytology or histology because of the high risk of unnecessary procedures for benign lesions . key words mr cholangiopancreatography bile ducts cholangiocarcinoma stenosis obstruction a . 
la rm consente quasi sempre di identificare la causa della stenosi e di ipotizzarne la natura neoplastica qualora sia riconoscibile la presenza di formazione mass - like ( extraduttale o vegetante nel coledoco )  . 
al contrario , nelle forme di ispessimento parietale , soprattutto se inferiore al centimetro , necessario il completamento diagnostico cito - istologico per via endoscopica a causa dellelevato rischio di portare al tavolo operatorio lesioni benigne . parole chiave colangiowirsung - rm dotti biliari colangiocarcinoma stenosi ostruzione introduction introduzione the diagnostic workup of patients with obstructive jaundice generally starts with ultrasound ( us ) and computed tomography ( ct ) , which are able to identify the obstruction site in almost all cases . 
however , because these modalities have relatively low accuracy in determining the cause of the stenosis not exceeding 78% for ct [ 17 ] and far lower for us [ 8 , 9 ] many jaundiced patients were subjected to invasive cholangiographic methods , such as endoscopic retrograde cholangiopancreatography ( ercp ) or percutaneous transhepatic cholangiography ( ptc ) , to confirm the site of obstruction and determine its nature to guide treatment . 
the spread of magnetic resonance imaging ( mri ) has drastically changed diagnostic management of obstructive jaundice as a result of the ability of mr cholangiopancreatography ( mrcp ) sequences to provide a cholangiographic map of the bile ducts . moreover , integration of the information provided by these sequences with that of t2 and t1 sequences obtained before and after contrast medium administration can suggest the nature of the obstruction with an accuracy that varies depending on the site . in addition , postcontrast dynamic acquisition obtained with three - dimensional ( 3d ) sequences enables angiographic evaluation of the hepatic vasculature . 
the all - in - one diagnostic role of mri therefore allows us to limit the use of ercp and ptc to doubtful cases requiring further cytohistological diagnostic investigation or to cases needing interventional palliative treatment . the aims of this study were to : ( 1 ) evaluate the efficacy of mri in identifying the presence and site of the obstruction , ( 2 ) define mri signs that are most strongly suggestive of extrahepatic cholangiocarcinoma , ( 3 ) identify lesions with similar mri features to those of extrahepatic cholangiocarcinomas and define possible criteria for the differential diagnosis and ( 4 ) establish the prospective diagnostic accuracy of mri in determining the malignant nature of the extrahepatic biliary obstruction . liter diagnostico del paziente con ittero ostruttivo prevede generalmente che vengano svolte , in prima battuta , ecografia ( us ) e tomografia computerizzata ( tc ) , le quali permettono di identificare la sede di ostruzione nella quasi totalit dei casi . 
tuttavia queste metodiche presentano accuratezza piuttosto bassa nel determinare la causa della stenosi , non superiore al 78% per la tc [ 17 ] e molto inferiore per gli us [ 8 , 9 ] , quindi molti pazienti itterici in passato venivano sottoposti a metodiche colangiografiche invasive , come la colangiografia per via endoscopica ( ercp ) o per via trans - cutanea ( ptc ) , per confermare la sede della ostruzione e formulare una diagnosi di natura indispensabile per indirizzare la terapia . 
la diffusione dellimpiego della risonanza magnetica ( rm ) ha determinato una drastica modifica delliter diagnostico del paziente con ittero ostruttivo , a motivo della capacit delle sequenze colangiowirsung - rm ( cwrm ) di ottenere una mappa simil - colangiografica delle vie biliari . 
inoltre , integrando le informazioni cos ottenute con quelle provenienti dalle sequenze t2 e t1 pesate , espletate sia prima che dopo la somministrazione di mdc , possibile ipotizzarne la natura , con accuratezza variabile a seconda delle sedi dellostruzione . 
il ruolo diagnostico all in one della rm consente pertanto di limitare limpiego di ercp e ptc ai casi dubbi che richiedano nel contempo approfondimento diagnostico cito - istologico o qualora sia indicato il trattamento palliativo interventistico . 
in 27 / 39 pazienti lindagine rm stata completata con studio colangiografico tradizionale , in 18 con ercp , in 9 con ptc , in 6 con ercp e ptc . 
i pazienti , giunti alla nostra osservazione nellarco temporale di 4 anni , sono stati esaminati utilizzando un magnete da 1 , 5 tesla ( simphony , siemens , erlangen , germania ) procedendo ad acquisizione sia di immagini cwrm che a studio rm convenzionale . 
le immagini cwrm sono state ottenute con sequenze haste ( tr : infinito , te : 60 ms ) multislice ( spessore di fetta : 4 mm senza gap ) nei diversi piani spaziali e con acquisizione proiettiva coronale thick slab ( spessore di fetta : 70 mm ) , utilizzando sequenze turbo spin echo ( tse ) fortemente pesate in t2 ( te : 1100 ms ) con acquisizioni multiple ( 68 ) ad incrementi progressivi di circa 15 . 
lo studio rm convenzionale ha previsto lesecuzione in fase pre - contrastografica di sequenze t1 gre con saturazione del grasso ( tr : 140 ms , te : 4 , 2 ms ) nei piani assiale e coronale e di sequenze t2 stir ( tr : 6000 ms , te : 66 ms ) nel piano assiale ; dopo la somministrazione di mdc ( gadolinio dtpa : 20 ml ; 2 ml / s ) , utilizzando la tecnica trifasica , sono state acquisite sequenze t1 gre fat - sat ( tr : 140 ms , te : 4 , 2 ms ) nei piani assiale o coronale ( spessore di fetta : 5 mm ; gap : 0 , 1 mm ) seguite da una acquisizione tardiva a circa 10 minuti dallinfusione di mdc ev ( gadolinio - dtpa , magnevist , schering , berlino , germania )  . in 10 pazienti , lacquisizione dinamica post - contrastografica stata espletata con sequenza t1 gre 3d ( vibe ; tr : 4 , 6 ms ; te : 1 , 8 ms )  . 
a tutti i pazienti , 10 minuti prima dellesame , sono stati somministrati per os 100 ml di mdc superparamagnetico ( lumirem , guerbet , parigi , francia )  . 
i due osservatori che hanno valutato retrospettivamente le indagini rm , procedendo a consenso in caso di disaccordo , hanno analizzato : sede ( ilare : dalla confluenza al dotto cistico ; prossimale : coledoco sovra - pancreatico ; distale : coledoco intrapancreatico e papilla ) ; eventuale dilatazione delle vie biliari intraed extra - epatiche ; morfologia della stenosi duttale ( progressivo affinamento o stop brusco ) ; aspetto morfologico della neoplasia : mass like o circonferenziale ( a seconda del tipo di crescita rispettivamente espansivo o infiltrativo - stenosante ) ; dimensioni ; intensit di segnale in fase pre - contrastografica ; tipo di enhancement dopo somministrazione di mdc . 
per valutare laccuratezza diagnostica prospettica della rm nel definire la natura maligna di ostruzione delle vie biliari extra - epatiche , sono stati considerati 74 esami rm di pazienti con ittero ostruttivo . 
in addition , in 9 / 23 ( 39% ) hilar cholangiocarcinomas and 1 / 6 ( 16% ) cholangiocarcinomas of the proximal choledochus , mri documented the presence of intrahepatic bile table 1 tumour morphology related to topographic distribution aone lesion involved both the hilum and the distal choledochus bone lesion involved both the proximal and distal choledochus tabella 1 morfologia del tumore in relazione alla distribuzione topografica location hilara proximal choledochusb distal choledochusa , b total sede ilarea coledoco prossimaleb coledoco distalea , b totale auna lesione localizzata sia in sede ilare che al coledoco distale buna lesione localizzata sia al coledoco prossimale che al coledoco distale valutazione retrospettiva delle caratteristiche del tumore lanalisi retrospettiva delle 41 lesioni accertate cito - istologicamente nei 39 pazienti affetti da colangiocarcinoma ha fornito i seguenti risultati . 
in 6 / 41 ( 15% ) colangiocarcinomi di cui 2 del coledoco prossimale e 4 del coledoco distale stata identificata la lesione nonostante lassente dilatazione delle vie biliari a monte . 
nei rimanenti casi , 35 / 41 ( 85% ) , sempre stata rilevata dilatazione delle vie biliari a monte della stenosi , ed in particolare tutti i 23 colangiocarcinomi localizzati in sede ilare si associavano a dilatazione delle vie biliari intra - epatiche . 
in this phase , diffuse parietal thickening of the intrahepatic bile ducts is appreciable ( arrowheads ) , which is better visualised on t1 gradient - echo fat - saturated ( gre - fs ) coronal image ( e )  . 
ben visibili nelle sequenze t2 pesate assiali ( a ) e coronali ( b ) le vie biliari intraepatiche marcatamente dilatate ; in sede ilare nodulo rotondeggiante moderatamente iperintenso ( freccia )  . 
il diametro maggiore medio delle lesioni di tipo espansivo stato 22 mm ( range 360 mm ) , mentre per le lesioni di tipo infiltrativo lo spessore parietale medio riscontrato stato di 7 mm ( range 315 mm )  . 
la maggior parte dei colangiocarcinomi ( 20 / 41 ) sono risultati ipo ( 49% ) o iso - intensi ( 49% ) nelle sequenze pesate in t1 e iper ( 49% ) o iso - intensi ( 21 / 41 ) ( 51% ) nelle sequenze pesate in t2 . 
dopo somministrazione di mdc , in fase tardiva nei piani coronali ( b , c ) apprezzabile manicotto di enhancement che avvolge il dotto epatico comune ( freccia ) con estensione allinfundibolo della colecisti ( frecce ) ed al dotto cistico ( d )  . mean maximum diameter of expansile lesions was 22 mm ( range 360 mm ) whereas mean wall thickness of infiltrative lesions was 7 mm ( range 315 mm )  . 
most cholangiocarcinomas ( 20 / 41 ) appeared hypo ( 49% ) or isointense ( 49% ) in t1 weighted and hyper ( 49% ) or isointense ( 21 / 41 ) ( 51% ) in t2 weighted sequences . 
most lesions ( 39 / 41 ; 95% ) failed to show significant enhancement in the arterial phase whereas almost all ( 40 / 41 ; 98% ) enhanced in the late phase ( 10 min )  . in this phase , enhancement tended to be homogeneous ( 26 / 41 ; 65% ) ( table 2 )  . the best diagnostic cospicuity was obtained , in 76% of cases , with the axial and / or coronal t1 - weighted gre sequence with fat suppression in the late phase . 
in particular , the coronal rather than the axial acquisition enabled identification of both the cholangiocarcinoma and possible vascular involvement . forms with circumferential appearance , generally unrecognisable using t2 - weighted haste sequences alone , were identified on t1 weighted images thanks to the typical maggior parte dei casi ( 39 / 41 : 95% ) non hanno dimostrato significativo enhancement nella fase contrastografica arteriosa , mentre quasi tutti ( 40 / 41 : 98% ) hanno dimostrato impregnazione nella fase tardiva ( 10 min )  . 
la sequenza a maggior cospicuit diagnostica stata , nel 76% dei casi , la t1 pesata gre con soppressione del grasso acquisita in fase post - contrastografica tardiva nei piani assiale e / o coronale . in particolare , la proiezione coronale , meglio di quella assiale , ha permesso di identificare sia il colangiocarcinoma che leventuale coinvolgimento vascolare . 
le forme con aspetto circonferenziale , generalmente non riconoscibili con la sola sequenza t2 pesata tipo haste , sono state identificate nella sequenza t1 pesata grazie al caratteristico manicotto di enhancement tardivo ( tabella 3 )  . nellinsieme dei 74 pazienti esaminati , le lesioni responsabili di ostruzione biliare sono state sempre identificate e correttamente localizzate . 
nelle immagini t1 pesate , espletate dopo somministrazione di mdc ( a , b ) riconoscibile ispessimento neoplastico circonferenziale del dotto epatico comune con estensione prevalente al dotto principale di destra ( freccia )  . peripheral enhancement in the late phase ( table 3 )  . 
mri proved to have good sensitivity ( 91% ) in characterising malignant stenoses due to both cholangiocarcinomas and other neoplasms that infiltrated the bile duct whereas its specificity was very low ( 47% ) given the high number of benign lesions ( 10 / 19 ) that were considered neoplastic ; the positive predictive value ( ppv ) was 83% , and the negative predictive value ( npv ) was 64% . with regard to cholangiocarcinomas only ( 39 lesions ) , mri sensitivity in characterising the lesion was 87% , specificity 51% , ppv 67% and npv 78% . 
the group of 17 false positive results included nine inflammatory lesions , five pancreatichead adenocarcinomas , one duodenal adenocarcinoma , one pancreatic neuroendocrine tumour and one metastasis from breast cancer . 
nine of 11 distal cholangiocarcinomas were correctly characterised thanks to the typical late - phase enhancement ( 10 min )  . comparison between mri and conventional cholangiographic techniques comparison was possible in 27 patients , 18 of whom underwent ercp and nine ptc . 
there was diagnostic agreement in 23 / 27 cases ( 85% ) and disagreement in 2 / 27 ( 7% ) cases : in one case , mri failed to identify a small ampulloma , which was readily visualised on ercp ; in the other case , ercp interpreted as inflammatory a neoplastic stenosis , which mri had classified correctly . 
in 2 / 27 cases , ercp was not diagsibilit ( 91% ) nel caratterizzare le stenosi maligne sia da colangiocarcinoma che da altre neoplasie infiltranti secondariamente la via biliare , mentre la specificit risultata assai bassa ( 47% ) a causa dellelevato numero di lesioni benigne ( 10 / 19 ) considerate neoplastiche ; il valore predittivo positivo risultato del 83% , il valore predittivo negativo del 64% . 
facendo riferimento ai soli colangiocarcinomi ( 39 lesioni ) , la sensibilit dellindagine rm nel caratterizzare la lesione risultata del 87% ; la specificit del 51% ; il valore predittivo positivo del 67% ; il valore predittivo negativo del 78% . 
nove su 11 colangiocarcinomi a sede distale sono stati correttamente tipizzati grazie alla caratteristica impregnazione in fase tardiva ( 10 min )  . confronto tra rm e metodiche colangiografiche tradizionali il confronto stato possibile in 27 pazienti di cui 18 sottoposti ad ercp e 9 a ptc . 
in the t1 - w sequence , the cholangiocarcinoma appears as a round mass with irregular margins , hypointense before contrast medium administration ( b ) and strongly hyperintense after contrast medium administration ( c , d )  . 
alla cwrm ( a ) si evidenzia marcata dilatazione del dotto epatico sinistro e dei suoi rami di divisione ; nella sequenza t1 pesata , il colangiocarcinoma si apprezza come lesione rotondeggiante , a margini irregolari , ipointensa in fase precontrastografica ( b ) e marcatamente iperintensa dopo mdc ( c , d ) ; la lesione meglio visualizzabile nelle immagini coronali t1 pesate ( c )  . 
alcuni rami biliari intraepatici dimostrano , analogamente alla lesione principale , discreto enhancement parietale ( teste di freccia )  . nostic due to failure to cannulate the choledochus . discussione discussion extrahepatic cholangiocarcinomas account for 65% of primary neoplasms of the biliary tract : the most common location is hilar ( about 60% ) , followed by the middle and distal third ( 15% respectively ) and diffuse forms affecting the whole extrahepatic biliary system ( 10% )  . in all cases , clinical manifestation ( jaundice ) occurs relatively early , given that even very small lesions are obstructive . 
in patients presenting with symptoms and signs of biliary obstruction , the aims of diagnostic imaging are to identify the stenosis , provide precise localisation and characterisation , and define locoregional extension to determine rei colangiocarcinomi extra - epatici costituiscono il 65% delle neoplasie primitive della via biliare : tra questi risulta prevalente la localizzazione ilare ( circa 60% ) , pi rare le localizzazioni al iii medio e iii distale ( 15% rispettivamente ) , e le forme diffuse a tutta la via biliare extra - epatica ( 10% )  . 
in tutti i casi , la manifestazione clinica ( ittero ) in genere abbastanza precoce , in quanto anche lesioni molto piccole hanno carattere ostruente . nei pazienti che presentano sintomi e segni di ostruzione biliare , i quesiti che si pongono allimaging sono la identificazione della stenosi , la precisa localizzazione e caratterizzazione ; infine il bilancio destensione loco - regionale costituisce criterio indispensabile per il giudizio di resecabilit [ 1015 ]  . 
magnetic resonance cholangiopancreatography ( mrcp ) ( a , b ) shows mild dilation of the common bile duct , which presents a mouse - tail morphology in its distal tract ( arrow )  . 
nelle immagini di cwrm ( a , b ) riconoscibile lieve dilatazione della via biliare principale che presenta stenosi con morfologia a coda di topo ( freccia ) in corrispondenza del suo tratto distale . 
nella sequenza t1 gre ( b ) espletata dopo somministrazione di mdc apprezzabile manicotto circonferenziale di enhancement ( freccia ) , compatibile con stenosi flogistica , rivelatosi colangiocarcinoma allesame istologico . sectability of the lesion [ 1015 ]  . mri enables identification of the primary lesion but , more importantly , thanks to postcontrast sequences , it allows precise evaluation of periductal soft tissue infiltration , appreciation of possible vascular infiltration and the study of metastatic involvement of the lymph nodes , liver and peritoneum . it therefore allows a complete preoperative lesion assessment and determination of its resectability . 
 mitiva , ma soprattutto , grazie alle sequenze post - contrastografiche , di valutare con precisione lo sconfinamento della neoplasia nei tessuti molli peri - duttali , di apprezzare leventuale infiltrazione vascolare e di studiare il coinvolgimento metastatico linfonodale , epatico e peritoneale . 
ad unanalisi della letteratura risulta che la rm ha sensibilit estremamente elevata ( 90%100% ) nellidentificare le stetable 2 signal and enhancement pattern related to tumour morphology hypo hyper 20 / 41 ( 49% ) 20 / 41 ( 49% ) 1 / 41 ( 2% ) 21 / 41 ( 51% ) hypo late - phase enhancement hyper homogeneous dishomogeneous 20 / 41 ( 49% ) 26 / 41a ( 65% ) 14 / 41a ( 35% ) iso , isointense ; hypo hypointense ; hyper , hyperintense aone exam performed without contrast medium tabella 2 segnale e caratteristiche di enhancement in relazione alla morfologia del tumore iper 20 / 41 ( 49% ) 20 / 41 ( 49% ) 1 / 41 ( 2% ) 21 / 41 ( 51% ) enhancement in fase tardiva disomogeneo omogeneo iper 20 / 41 ( 49% ) 26 / 41a ( 65% ) 14 / 41a ( 35% ) appearance mass like circumferential thickeninga total aspetto mass - like ispessimento circonferenzialea totale iso , isointenso ; ipo , ipointenso ; iper , iperintenso auna indagine eseguita senza mdc a . 
with regard to characterisation , mri is reported to have an accuracy of 66%85% in defining the malignant nature of the biliary stenosis [ 7 , 16 , 17 , 2023 ]  . our experience has shown that mri is almost constantly able to identify both the presence and site of the obstruction . its sensitivity in characterising the malignant nature of the stenosis was excellent ( 91% ) whereas its specificity was relatively poor ( 47% )  . 
the high sensitivity in characterising the malignant nature of biliary obstruction is due to the constant acquisition of late postcontrast images . however , if on the one hand contrast enhancement allows one to suspect the malignant nature of the stenosis , on the other , it leads to false positive errors , more commonly in distal locations , since the scar reaction of an inflammatory stenosis has the same appearance as the typical desmoplastic component of cholangiocarcinomas . in our experience , 10 / 19 benign lesions were considered neoplastic , an overestimation that accounts for the low specificity of the technique . the main criterion enabling differentiation between benign and malignant strictures was lesion morphology : when the lesion displays a mass - like appearance , the diagnosis of malignancy is correct whereas when the lesion appears as a circumferential thickening , it is very difficult to distinguish inflammatory from neoplastic lesions . the 5 - mm cutoff value for discriminating benign and manosi della via biliare extra - epatica . 
per quanto riguarda la sede di stenosi delle vie biliari extra - epatiche , i dati raccolti in letteratura indicano per la rm una sensibilit oscillante tra 85% e 96% , lievemente inferiore rispetto alle metodiche colangiografiche invasive , dotate di maggiore risoluzione spaziale [ 7 , 1620 ]  . 
la rm , tuttavia , pi precisa nel valutare lestensione della stenosi in quanto visualizza la componente neoplastica che si sviluppa lungo la parete del dotto ed in sede extra - duttale [ 7 , 1620 ]  . 
per quando riguarda la caratterizzazione , in letteratura riportata per la rm una accuratezza compresa tra 66% e 85% nel definire la natura maligna di stenosi biliare [ 7 , 16 , 17 , 2023 ]  . nella nostra esperienza emerso che la rm in grado , nella pressoch totalit dei casi , di identificare sia la presenza che la sede dellostruzione . 
la sensibilit nel caratterizzare la natura maligna della stenosi si dimostrata ottima ( 91% ) , mentre la specificit risultata piuttosto scadente ( 47% )  . lelevata sensibilit ottenuta nel caratterizzare la natura maligna dellostruzione biliare dovuta alla costante acquisizione di immagini post - contrastografiche tardive . 
tuttavia , se da un lato lenhancement consente di sospettare la natura maligna della stenosi , dallaltro induce errori di falsa positivit , pi frequentemente in sede distale , in quanto la reazione cicatriziale di una stenosi flogistica ha lo stesso aspetto della componente desmoplastica tipica dei colangiocarcinomi . 
tale sovrastima giustifica la bassa specificit dellindagine . il principale criterio che ha consentito di differenziare stenosi benigne e maligne la morfologia della lesione : quando sostenuta da una lesione con aspetto mass - like risulta corretta la diagnosi di malignit , mentre quando assume aspetto di ispessimento circonferenziale molto difficile distinguere la natura infiammatoria da quella neoplastica . 
in questi casi utile ricorrere alle immagini cwrm che , qualora dimostrino dilatazione duttale cospicua , discrepante rispetto alle esigue dimensioni della lesione , orientano la diagnosi verso forme neoplastiche piuttosto che infiammatorie . 
la maggior parte dei tumori con aspetto mass - like ( 13 / 18 : 72% ) identificabile gi nelle immagini pre - contrastografiche essendo ipointensi rispetto al parenchima epatico nelle sequenze t1 pesate e tenuemente iperintensi in quelle pesate in t2 . 
al contrario , la maggior parte dei colangiocarcinomi cosiddetti circonferenziali sono misconosciuti allindagine pre - contrastografica in quanto isointensi rispetto alla parete duttale sia nelle sequenze pesate in t1 che in quelle pesate in t2 . 
mentre nei colangiocarcinomi ilari le informazioni fornite dalla rm sono nella maggior parte dei casi bastevoli nellindirizzare la diagnosi , quando localizzati nella porzione intrapancreatica del coledoco , dove pi strutture sono anatomicamente congiunte e lincidenza di fenomeni flogistici primitivi ( pancreatite cronica ostruttiva ) o secondari al passaggio di calcoli o a manovre endoscopiche maggiore , la possibilit di errore diagnostico pi elevata . 
in questi casi , segni secondari quali limpronta eccentrica sulla via biliare principale , la dislocazione dei dotti collaterali del pancreas ed il segno del doppio dotto , orientano verso lorigine pancreatica della lesione . 
tuttavia , sia ercp che ptc presentano il limite di non visualizzare la via biliare a monte ( ercp ) o a valle ( ptc ) di stenosi serrate , ma soprattutto sono gravate da complicanze gravi ( pancreatite , sepsi , emobilia , perforazione intestinale ) in una percentuale non trascurabile di casi dal 5 al 9% [ 18 , 20 ]  . 
dopo somministrazione di mdc ( b ) in sede pi caudale si evidenzia metastasi sottocutanea ( asterisco ) da colonizzazione neoplastica da trasporto conseguente a colangiografia transcutanea ( ptc )  . 
riconoscibile il tramite dellago con morfologia tubulare ( asterisco ) , ipointenso rispetto alla lesione . conclusions conclusioni mri correctly identifies stenosis site and suggests its neoplastic origin when it visualises an expansile extraductal mass or a mass growing into the choledochus . 
it is exhaustive in providing the surgeon with all the information needed to best manage the patient . in contrast , in the forms exhibiting parietal thickening , particularly if less than one centimeter and located in the distal third of the choledochus , further cytohistological investigation by endoscopy or endoscopic ultrasound ( eus ) is required owing to the high risk of unnecessary surgery for benign lesions [ 24 , 25 ]  . la rm consente di identificare con precisione la sede della stenosi e di ipotizzarne la natura neoplastica qualora sia riconoscibile formazione espansiva extra - duttale o neoformazione vegetante nel coledoco , risultando esaustiva nel fornire tutte le informazioni necessarie al chirurgo per decidere il miglior management terapeutico per il paziente . 
soldati servizio di pronto soccorso , medicina e chirurgia di accettazione e di urgenza , asl 2 lucca , ospedale della valle del serchio , lucca , italy correspondence to : g . 
soldati , via nazionale 22 , i - 55036 pieve fosciana , lucca , italy , tel . : + 39 - 0583 - 669841 / + 39 - 0583 - 666763 , fax : + 39 - 0583 - 669618 , e - mail : soldati@katamail.com received : 31 august 2005 / accepted : 11 november 2005 / published online : 25 may 2006 abstract lung sonography , generally not thought to be diagnostic , is currently being reconsidered and is developing into an interesting clinical possibility . 
 key words lung ultrasound diagnosis riassunto lecografia polmonare , ritenuta in genere minimamente diagnostica , sta subendo un processo di sviluppo e di revisione delle sue interessanti possibilit di applicazione clinica . attraverso lesperienza personale , confrontata con i dati della letteratura , vengono descritti i principali segni ecografici della patologia polmonare esaminabile con ecografia . parole chiave polmone ecografia diagnosi introduction introduzione it was not so long ago that sonographers considered the airfilled lungs to constitute an insurmountable obstacle , a barrier that could hinder accurate visualisation of the heart and acceptable imaging of the thoracic aorta , the mediastinum or the diaphragmatic domes from above . that the pleural line is a fundamental landmark in the study of the chest and , above all , that its movement synchronous with breathing accurately identifies the contact between the lungs and the chest wall has , only recently , been understood [ 1 , 2 ]  . 
the observation of a motionless pleural line without the characteristic gliding or sliding movement , which even a moderately trained eye can identify in the normal chest , almost inevitably led to the possibility of diagnosing pneumothorax rapidly and accurately . 
since the observation of pneumothorax followed by cases of dyspnoea , fever , chest pain , embolism and trauma , increasingly convincing reports have appeared on sonographic identification of lung consolidation [ 3 ] and different lung - field artefacts useful for diagnosing a variety of conditions , including pneumonia , pulmonary infarction , interstitial disease , pulmonary oedema and contusions [ 46 ]  . 
it is therefore not unreasonable to state that a sonographic semiology of the lung can be defined , intended as a set of sonographic signs that are useful in formulating diagnostic hypotheses of lung disease . 
 the aim of this paper is to illustrate the main sonographic signs of lung disease , highlight their morphological , dynamnon lontano il periodo in cui lecografista riteneva insormontabile lostacolo agli ultrasuoni offerto dai polmoni ripieni di aria : uno sbarramento che impedisce talvolta uno studio accurato del cuore , unimmagine accettabile dellaorta toracica , del mediastino o delle cupole diaframmatiche dallalto . 
solamente in epoca relativamente recente si capito che la linea pleurica rappresenta un repere essenziale nello studio del torace e , soprattutto , che il suo movimento sincrono con gli atti del respiro identifica con accuratezza il contatto del polmone con la parete toracica [ 1 , 2 ]  . la possibilit di diagnosticare con precisione e rapidit il pneumotorace derivata quindi in modo consequenziale e quasi inevitabilmente dallosservazione di una linea pleurica immobile e dallassenza di un gliding o sliding che anche un occhio solo modestamente addestrato pu individuare su ogni torace normale . partendo dallosservazione di soggetti con pneumotorace prima , con dispnea , febbre , dolore toracico , embolia , trauma poi , nellultimo decennio sono apparse in letteratura segnalazioni sempre pi convincenti sulla possibilit di identificare gli addensamenti del polmone [ 3 ] e diverse modificazioni artefattuali dei campi polmonari , utili per la diagnosi di patologie varie : polmoniti , infarti polmonari , interstiziopatie , edema del polmone , contusioni [ 46 ]  . non pertanto azzardato oggi affermare che pu essere descritta una semeiotica ecografica del polmone , intesa cog . 
most of the data are derived from personal observations compared with the experience gained in this field by daniel lichtenstethe remaining data have been gleaned from the literature . me compendio di segni rilevati con luso degli ultrasuoni , utili per porre ipotesi diagnostiche di patologia polmonare . scopo del presente articolo illustrare i principali segni ecografici delle malattie del polmone , mettendone in risalto le caratteristiche morfologiche , dinamiche e artefattuali e table 1 definition of sonographic lung findings sonographic finding definition tabella 1 definizione dei reperti ecografici polmonari reperto ecografico definizione lung gliding or sliding lung point lung pulse a lines z lines b lines e lines interstitial syndrome alveolar syndrome bronchograms static bronchogram lung gliding o sliding lung point lung pulse linee a linee z linee b linee e sindrome interstiziale sindrome alveolare broncogrammi broncogramma statico indicates a lung region in contact with the chest wall indicates the point in which a partially collapsed lung is in contact with the chest wall . on the sonogram , gliding is only present in part of the pleural line minimal gliding synchronous with cardiac systoles , especially at the level of the paracardiac lung . 
they help define a possible obstructive origin of the consolidation immobile and bundled bronchograit indicates atelectasis indica una regione polmonare a contatto con la parete toracica indica il punto in cui un polmone parzialmente collassato contatta la parete toracica . nell ' immagine ecografica presente il gliding solo a livello di una parte della linea pleurica minimo gliding sincrono con le sistoli cardiache , specialmente a livello del polmone paracardiaco . 
sindrome interstiziale ( edema , interstiziopatie ) artefatti verticali , da aria , a partenza dal sottocute e proiettati sui campi polmonari . enfisema sottocutaneo variazione del pattern polmonare da quadro artefattuale orizzontale ( linee a ) a verticale ( linee b ) , settoriale o diffuso ( interstiziopatia , ground glass o kerley b radiografici ) organizzazione ( epatizzazione ) di un campo polmonare . 
indica atelettasia because i believe there is a need to simplify the terminology in this field , in the absence of other proposals , i shall refer to the lung artefacts , which are fundamentally diagnostic , using the terms recently suggested by lichtenstein ( [ 7 ] , personal communication )  . 
soldati : sonographic findings in pulmonary diseases indicandone lutilit in un contesto integrato di diagnosi ( tabella 1 )  . gran parte di questi dati derivano da osservazioni personali , confrontate con lesperienza maturata in questo specifico campo da daniel lichtenste il rimanente fa riferimento ai dati della letteratura disponibili . per quanto concerne la nomenclatura , ritengo che questa vada opportunamente semplificata : pertanto , in assenza di ulteriori proposte , verr fatto riferimento alle componenti artefattuali polmonari , che sono fondamentalmente diagnostiche , utilizzando le notazioni recentemente proposte da questo autore [ 7 , d . 
by contrast , it remains evident in the case of emphysema or parenchymal bullae . another sign related to pleural gliding and having equal significance is the lung pulse : the rhythmic millimetric movement of the pleura produced by cardiac systoles [ 10 ]  . lung pulse rules out pneumothorax . 
tipicamente il rinforzo acustico verticale non oscura le linee b . re ed il gliding sign scompare in caso di pneumotorace e di atelettasia [ 9 ]  . da notare comunque che il gliding poco evidente a livello degli apici polmonari , fisiologicamente meno mobili . di contro ancora evidente in caso di enfisema o di bolle parenchimali . correlato al gliding pleurico e dotato del medesimo significato il lung pulse : il ritmico e millimetrico movimento della pleura indotto dalle sistoli cardiache [ 10 ]  . 
at times , fixed vertical echoic shadows that do not mask the a lines appear against the typical pulmonary background . these findings are of unclear origin and should not be confused with other vertical artefacts ( b lines , see below ) ; fig . 
lung points che si collocano , col paziente supino , anteriormente alla linea ascellare media , indicano raccolte aeree relativamente piccole , mentre lung points mediali alle linee mammillari indicano pneumotoraci minimi , spesso invisibili alla radiografia col paziente in posizione supina ( pneumotoraci occulti )  . il polmone normale il polmone normale identificabile come un campo artefattuale al di sotto della linea pleurica . 
scattered b lines are likely to represent thickened , high - impedance , reverberating subpleural interlobular septa , which are typically situated about 7 mm apart . coalescent b lines probably derive , as suggested by avruch and cooperberg [ 12 ] , from alveolar structures similar to air microbubbles resonating in a predominantly fluid context ( the expanded interstitium )  . these two hypotheses are confirmed by ultrasound ( us ) computed tomography ( ct ) correlations , which show that multiple b lines in pulmonary oedema or interstitial fibrosis indicate expansion of the subpleural interlobular septa and areas of ground - glass ct attenuation , respectively . interstitial syndrome should not be confused with the presence of multiple reverberation artefacts of varying morphology that originate from subcutaneous emphysema and lie external to the pleural line , which is masked by them , as is the costal plane . these artefacts are known as e lines . 
a conferma delle due ipotesi vi sono le correlazioni tra reperti eco e tc che , nelle circostanze in cui compaiono multiple linee b in caso di edema polmonare o fibrosi interstiziale , rispettivamente indicano lespansione dei setti interlobulari subpleurici ed i reperti tomografici di ground glass . 
non va confusa con la sindrome interstiziale la presenza di multipli , difformi artefatti di riverbero che originano da enfisema sottocutaneo e che si situano esternamente alla linea pleurica mascherandola assieme al piano costale . 
diffuse sui campi polmonari , le linee b identificano con unaccuratezza superiore al 90% ledema polmonare cardiogenico ( hanno il significato delle linee b di kerley radiografiche ) , probabilmente fin dalle fasi preradiografiche . 
analogamente indicano anche tutte quelle situazioni in cui vi incremento dellacqua extravasale polmonare ( edemi lesionali , ards ) e nel giusto contesto clinico permettono una differenziazione delle dispnee [ 1316 ]  . 
se localizzate , le linee b indicano un incremento locale dellacqua extravascolare interstiziale , come dato di vedere nelle polmoniti interstiziali , nelle fasi preaddensanti dei focolai polmonitici , attorno agli addensamenti polmonari e nei focolai contusivi del polmone . la sindrome alveolare laddensamento polmonare , inteso come allagamento alveolare ( epatizzazione ) da parte di essudato , trasudato , sangue , fibrina o quantaltro sostituisca laria , se raggiunge la may be present segmentally or diffusely in all diseases that change the interstitium - to - airspace ratio in favour of the interstitiudiffuse b lines over the lung fields correspond to radiographic kerley b lines and identify cardiogenic pulmonary oedema with an accuracy greater than 90% , probably already in the preradiographic phase . similarly , they are also an indication of all those situations of increased extravascular pulmonary fluid ( lesional oedema , acute respiratory distress syndrome , ards ) , and in the appropriate clinical setting , they enable differentiation among forms of dyspnoea [ 1316 ]  . 
when localised , b lines indicate a local increase in interstitial extravascular fluid , as can be seen in interstitial pneumonia , in the preconsolidative stages of pneumonia , around areas of pulmonary consolidation and in lung contusions . 
tipicamente la linea pleurica dellarea addensata appare interrotta ( alveologramma superficiale ) ed allinterno della regione addensata possibile dimostrare ecograficamente , contrariamente al normale , bronchi aerati , bronchi occlusi e vasi . 
questi reperti sono suggestivi di focolai pneumonitici , di foci di embolizzazione , di contusioni organizzate e di atelettasie ( che tipicamente appaiono retrattili )  . i broncogrammi i broncogrammi , al pari dei vasi , appaiono in ecografia nelle regioni polmonari addensate . 
these findings are suggestive of foci of pneumonia , embolism , organised contusions and atelectasis ( typically retractile )  . bronchograms sonography can demonstrate bronchograms as well as vessels within regions of lung consolidation . 
because a fluid bronchogram indicates absence of ventilation of the consolidated area , it should prompt the search for bronchial obstruction , which is at times found in the major lobar bronchi or towards the lung hilu in addition , a bronchogram may appear dynamic , if it moves with respiration , or static , with the bronchi fixed in their position and often bundled . a static bronchogram is an indication of atelectasis , as are the absence of gliding sign , the presence of lung pulse and lung hepatisation . 
a dynamic bronchogram usually correlates with pleural gliding and a nonretractile nature of the lung consolidation [ 19 ]  . consolidation as an acoustic window just as pleural effusions enhance the pleural surface at sonography , every lung consolidation produces an acoustic window , which enables visualisation of the deep lung tissue . this is why it is possible to appreciate the bronchi as well as the veins and arteries , which can be differentiated into bronchial and pulmonary on the basis of their doppler - us haemodynamic indices . likewise , images of the heart and thoracic aorta are enhanced by left - sided consolidations . 
finally , even hilar masses can be identified through portions of lung atelectasis . cardiac window normally , the parasternal and apical cardiac window exists as a result of the contact between the heart pericardium and the chest wall . an interposed portion of lung with its artefacts partially or completely masks the image of the heart . 
in cases of minimal left pneumothorax , with the patient supine , the air collects in the paracardiac regions ( deep sulcus sign ) , abolishing both the image of the heart and pleural sliding [ 20 ] fig . 
la dinamicit del broncogramma di solito si correla invece con il gliding pleurico e con una natura non retrattile delladdensamento [ 19 ]  . laddensamento come finestra acustica al pari del versamento pleurico che allindagine ultrasonora esalta la superficie pleurica , ogni addensamento polmonare crea una finestra acustica che consente una valutazione del tessuto polmonare in profondit . 
questa la ragione per cui si rendono evidenti bronchi , vasi venosi e arteriosi , questi ultimi studiabili e differenziabili con eco doppler in bronchiali e polmonari in base agli indici emodinamici . 
infine anche masse ilari vengono identificate attraverso porzioni di polmone atelettasico . la finestra cardiaca normalmente la finestra cardiaca parasternale ed apicale esiste per il contatto del cuore - pericardio con la parete toracica . un lembo polmonare interposto con i suoi artefatti maschera parzialmente o completamente limmagine del cuore . 
in caso di pneumotoraci minimi sinistri , col paziente supino , laria viene a raccogliersi nelle regioni paracardiache ( deep sulcus sign ) abolendo sia limmagine del cuore che lo sliding pleurico [ 20 ]  . conclusioni allo stato attuale delle conoscenze utile cominciare ad imconclusions given our current state of knowledge , we can start applying some concepts of sonographic semiology of the lung in our clinical practice , as the signs can no doubt assist in the diagnosis and follow - up of several lung diseases . 
chest sonography is particularly relevant in emergency settings , austere contexts and when the patients critical condition precludes transfer from protected environments ( emergency department , intensive care unit , operating theatre )  . 
a further application could be the follow - up of chest disease when there is a need to limit radiation exposure ( paediatrics , obstetrics )  . it is equally important to standardise the terminology in this field , with terms unequivocally identifying given sonographic signs of the lung , which are essentially dynamic or artefactual in nature [ 21 ]  . 
soldati : sonographic findings in pulmonary diseases piegare in un contesto clinico alcuni concetti di semeiotica ecografica del polmone che indubbiamente sono utili per affinare diagnosi o nel follow - up di determinate patologie respiratorie . 
ci particolarmente rilevante in situazioni di urgenza , in contesti austeri o quando il paziente , per la sua criticit , non pu abbandonare ambienti protetti ( pronto soccorso , rianimazioni , sale operatorie )  . 
unaltra utile applicazione pu essere il follow - up di patologie toraciche in casi in cui necessario limitare lesposizione radiante ( pediatria , ostetricia )  . parimenti essenziale in questo campo lutilizzo di una terminologia codificata che identifichi inequivocabilmente certi segni ecografici del polmone , che in sostanza sono di tipo dinamico o artefattuale [ 21 ]  . 
lacquisizione , laggiornamento e la condivisione dei concetti esposti possono pertanto contribuire allo sviluppo di un settore particolare , in rapido progresso , dellecografia . acknowledgements i wish to thank d . 
while there is a general consensus on immediate surgical repair when the ascending aorta is involved , the optimal treatment strategy for type b aortic dissection ( b - ad ) remains controversial . 
recently , endovascular treatment with percutaneous stent - graft implantation , originally used for aortic aneurysm exclusion , has acquired an important role in the treatment of b - ad . 
imaging techniques such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) and angiography have a fundamental role in the search for the anatomic details necessary to tailor the stent graft and in evaluating the most suitable anatomy for stent graft . transesophageal echocardiography is fundamental during the procedure to monitor the correct release of the stent graft and evaluate the result of the procedure expressed by immediate thrombosis out of the stent - graagain , imaging techniques , more notably ct , have a fundamental role in the postoperative followup after stent - graft placement . 
according to the investigators , new therapeutic indications are likely to emerge also in uncomplicated b - ad . key words aortic dissection endovascular treatment riassunto la dissezione aortica tuttora uno degli eventi cardiovascolari pi gravi . 
mentre esiste un accordo unanime sullindicazione allintervento chirurgico immediato , qualora sia coinvolta laorta ascendente , la strategia terapeutica ottimale per la dissezione aortica tipo b ( da - b ) ancora controversa , per lelevata mortalit sia spontanea sia del trattamento chirurgico . 
in questo scenario recentemente ha trovato una precisa collocazione limpianto percutaneo di endoprotesi ( stent - graft )  . originariamente impiegate per lesclusione degli aneurismi aortici , nel trattamento della da - b hanno dato ottimi risultati . 
le metodiche di immagine hanno un ruolo assolutamente fondamentale nella ricerca dei dettagli anatomici necessari per identificare quale paziente pu avvalersi di questo trattamento e per selezionare la misura adatta di endoprotesi . lecocardiografia transesofagea invece fondamentale nel corso della procedura per monitorare il corretto posizionamento dellendoprotesi e verificare limmediato attuarsi del processo di trombosi del falso lume che testimonia lefficacia della procedura . le metodiche di immagine , in modo particolare la tc , svolgono di nuovo un ruolo fondamentale nel follow - up , considerando che il rischio di endoleak pu essere determinante nel rischio di rottura aortica . 
attualmente in corso uno studio randomizzato di confronto tra la procedura di impianto di endoprotesi e la terapia medica da cui possono derivare nuove indicazioni terapeutiche anche nella da - b non complicata . parole chiave dissezione aortica trattamento endovascolare p . 
while there is a general consensus on immediate surgical repair when the ascending aorta is involved , the optimal treatment strategy for type b aortic dissection ( b - ad ) remains controversial . 
because of the high morbidity and mortality of surgery of the descending aorta , medical treatment is generally advocated for uncomplicated cases . however , about 30% of acute b - ad at clinical presentation is complicated by peripheral vascular ischaemia or haemodynamic instability , which results in a high risk of spontaneous death . 
 at present , the most frequent attitude is medical antihypertensive treatment as the primary therapy , reserving surgery for recurrent pain or life - threatening complications such as critical malperfusion syndrome or impending rupture . 
with aggressive antihypertensive therapy , up to 85% of patients may survive their initial hospital stay , with an estimated 50% mortality at 5 years and late expansion of the false lumen in about 25% of patients at 4 years . 
in the longterm , b - ad outcome is unsatisfactory even after successful initial stabilisation and optimal medical therapy . five - year survival rates between 32% and 72% have been reported [ 17 ] because medical therapy alone cannot prevent the evolving nature of the disease . several reports in the literature have analysed the longterm outcome in patients with type b dissection , comparing medical with surgical therapy . 
the long - term survival after surgery reported by fann and colleagues [ 7 ] for patients with acute type b dissections were 56% , 48% , 29% and 11% at 1 , 5 , 10 and 15 years , respectively . a large retrospective analysis by umaa and colleagues [ 1 ] has recently focused on long - term outcome comparison between medical and surgical therapy in 189 patients after acute type b dissection . 
survivals free of dissection - related complications at 5 and 10 years were 82% and 62% , respectively , in the medical group and 68% and 68% , respectively , among surgical patients . 
actuarial survival estimates for all patients were 71% , 60% , 35% and 17% at 1 , 5 , 10 and 15 years , respectively , and were similar for medical and surgical patients . the difference in survival free of reoperation also failed to reach statistical significance , indicating that medical therapy appears to confer some survival advantage only in the short term but fails to demonstrate any significant advantage in the long term . in the past few years , endovascular treatment of the thoracic aorta has been increasingly applied , revolutionizing the clinical approach to thoracic aortic diseases . 
more notably than in abdominal aortic aneurysm , in which endovascular techniques compare with low - risk surgery , stent - graft repair la dissezione aortica tuttora uno degli eventi cardiovascolari pi gravi . 
mentre esiste un accordo unanime sullindicazione allintervento chirurgico immediato , qualora sia coinvolta laorta ascendente , la strategia terapeutica ottimale per la dissezione aortica tipo b ( da - b ) ancora controversa . 
circa il 30% delle da - b acute si presentano invece , alla valutazione clinica , complicate da ischemia periferica o instabilit emodinamica ed un elevato rischio di morte se non trattati . 
nonostante i progressi delle tecniche anestesiologiche e chirurgiche e nella gestione post - operatoria la mortalit nellintervento chirurgico in urgenza per da - b varia dal 29% al 50% [ 17 ]  . 
inoltre si possono verificare sanguinamenti maggiori , ictus , eventi cardiaci e sepsi . attualmente lapproccio pi diffuso si fonda sulla terapia medica anti - ipertensiva come trattamento di base e riserva la chirurgia solo in caso di dolore intrattabile e complicanze letali , quali la sindrome da malperfusione o limminente rottura . 
con una terapia anti - ipertensiva aggressiva fino all85% dei pazienti possono sopravvivere nella degenza ospedaliera con una mortalit stimata a 5 anni del 50% ed unespansione tardiva del falso lume in circa il 25% dei pazienti a 4 anni . 
la percentuale di sopravvivenza a 5 anni riportata varia tra il 32% ed il 72% [ 17 ] poich la sola terapia medica non pu impedire la tendenza ad evolvere della patologia . 
 [ 1 ] ha recentemente messo a fuoco la differenza di prognosi a lungo termine ( 36 anni ) tra la terapia medica e chirurgica in 189 pazienti con da - b acuta . 
la sopravvivenza attuariale stimata per tutti i pazienti stata 71% , 60% , 35% e 17% a 1 , 5 , 10 e 15 anni rispettivamente , senza notevoli differenze tra il gruppo medico e chirurgico . 
in particolare analizzando i dati a lungo termine la terapia medica apporta un vantaggio di sopravvivenza solo nei primi anni , mentre non determina alcun miglioramento di sopravvivenza nel lungo periodo . il trattamento endovascolare dellaorta toracica discendente stato impiegato in modo progressivamente crescente in questi anni , rivoluzionando lapproccio clinico alla patologia dellaorta toracica . 
rispetto allaneurisma dellaorta for thoracic aortic diseases represents a low - invasive technique able to offer a therapeutic option even to high - risk patients who could not be considered candidates for surgery . even though the first thoracic implant was performed in 1986 in russia by volodos and colleagues , the history of endovascular treatment of the thoracic aorta begins in stanford in 1992 [ 8 ] with a clinical trial that included 103 patients affected by various aortic diseases such as atherosclerotic aneurysm , ad , penetrating ulcers and posttraumatic injuries . the availability of commercially manufactured stent grafts in 1997 has brought the endovascular techniques into clinical practice , allowing the growth of technical skill and knowledge of aortic disease in many centres . 
 [ 10 ] compared 12 patients with chronic bad and aneurysmal degeneration ( > 5.5 cm ) treated with commercial stent - graft devices to 12 concurrent patients treated with conventional open surgical repair . 
no patient in the endovascular group died during the 12 - month study and there was not a single instance of spinal cord ischemia whereas 33% of the surgical patients died . after this initial experience , several single - centre reports have shown technical feasibility and clinical safety of endovascular techniques in b - ad [ 1129 ] the concept of endovascular reconstruction in ad was propelled by the desire to induce aortic remodelling by sealing the proximal entry tear , at the same time avoiding the risks associated with open surgery . this rationale was originally based on evidence in the literature [ 30 , 31 ] of the protective effect of false lumen thrombosis against false lumen expansion and on the clinical observation that patients with spontaneous thrombosis of the false lumen have a better long - term prognosis than those without . conversely , persistent perfusion of the false lumen has been identified as an independent predictor of progressive aortic enlargement and adverse long - term outcome . 
closure of the entry tear of a type b dissection is essential to reduce aortic diameter and promote both depressurisation and shrinkage of the false lumen , which could lead to thrombosis , fibrous transformation and subsequent remodelling and stabilisation of the aorta . 
in russia nel 1986 , la storia del trattamento endovascolare dellaorta toracica comincia a stanford nel 1992 con un trial clinico di 103 pazienti [ 8 ] con diverse patologie aortiche tra cui aneurismi aterosclerotici , dissezioni aortiche , ulcere penetranti e lesioni post - traumatiche . lintroduzione di endoprotesi a produzione commerciale nel 1997 ha portato le tecniche endovascolari nella pratica clinica , favorendo una crescita tecnica e culturale nelle malattie aortiche in molti centri . il primo report sul trattamento con endoprotesi nella dab stato pubblicato nel 1999 in due serie di pazienti acuti e cronici . 
 [ 9 ] ha riportato una serie di 19 pazienti con da - b acuta trattati con endoprotesi con un successo tecnico del 100% e mortalit a 30 giorni del 13% . 
eventi severi si sono verificati in 3 ( 20% ) su un totale di 15 pazienti . tre pazienti hanno mantenuto flusso nel falso lume che si risolto al controllo tc ad 1 mese . 
 [ 10 ] hanno comparato 12 pazienti affetti da da - b cronica ed evoluzione aneurismatica ( > 5 , 5 cm ) trattati con endoprotesi e 12 pazienti con terapia chirurgica convenzionale . 
dopo questa esperienza iniziale molti report monocentrici hanno dimostrato la fattibilit e la sicurezza clinica della tecnica endovascolare nella da - b [ 1129 ]  . il concetto di ricostruzione endovascolare nella da stato basato sul tentativo di indurre un rimodellamento aortico chiudendo il foro di ingresso prossimale . 
questa ipotesi si basa sullevidenza in letteratura [ 30 , 31 ] di un effetto protettivo della trombosi del falso lume rispetto alla sua espansione e sullosservazione che i pazienti con trombosi spontanea del falso lume presentavano una migliore prognosi a lungo termine rispetto ai pazienti con falso lume pervio . 
identification of the entry and reentry tears , the relationship between true and false lumen and visceral vessels and involvement of the iliac arteries are all crucial information for patient and stent - graft selection . 
 tecniche di immagine nella valutazione pre - trattamento nel percorso diagnostico di un paziente candidato a trattamento endovascolare per da - b limaging ad alta risoluzione fondamentale al fine di definire i dettagli anatomici essenziali , in quanto il successo della procedura strettamente legato alla definizione anatomica . 
lidentificazione dei fori di ingresso e di rientro , il rapporto tra vero e falso lume e vasi viscerali ed il coinvolgimento delle arterie iliache sono tutte informazioni essenziali per la selezione dei pazienti e dellendoprotesi . computed tomography tomografia computerizzata ct technology has recently evolved with the advent of multidetector ct ( mdct ) becoming one of the most suitable imaging modalities for evaluation of ad . 
these advances significantly modified the possibility of evaluating ad . imaging of dissection requires a volume of coverage from supra - aortic branches superiorly to femoral arteries inferiorly , and mdct in a few seconds can acquire this extent . 
due to cardiac gating and high temporal resolution , entry and reentry sites can be displayed as focal interruption of the intimal flap in axial images or in software reconstruction in any plane and thickness . 
the slender linear areas of low attenuation that occasionally appear in the false lumen on ct images , known as the cobweb sign , are specific to the false lumen and may aid in its recognition . 
measurements for sizing the stent graft should be assessed in maximum intensity projection ( mip ) reconstruction or on axial images orthogonal to the longitudinal axis in order to avoid mistakes in measurements due to partial volumes . magnetic resonance imaging magnetic resonance imaging ( mri ) is a very accurate tool in the detection of ad because of its high sensitivity and specificity that approximate 100% in published series [ 3235 ]  . conventional spin - echo t1 - weighted imaging provides the best anatomic detail of aortic wall tissue and is still the basis of any aortic study . 
similarly to ct , visualisation of dissected media remnants ( aortic cobwebs ) may la tecnologia tc si recentemente evoluta con lavvento della tc multidetettore ed diventata una della tecniche di imaging pi adatte alla valutazione della da . 
a differenza del suo predecessore a singolo detettore , la tc multidetettore ( mdct ) consente la copertura di volumi maggiori sul piano cranio - caudale con una risoluzione spaziale e temporale pi elevate che minimizzano leffetto degli artefatti da movimento . 
limaging della dissezione richiede un ampio volume di acquisizione , dai tronchi sovra - aortici superiormente fino alle arterie femorali inferiormente e la mdct pu eseguire questa acquisizione in pochi secondi . 
grazie al gating cardiaco ed allelevata risoluzione temporale , i fori di ingresso e rientro possono essere visualizzati come interruzioni del flap intimale nelle immagini assiali oppure nelle ricostruzioni volumetriche . 
le aree di attenuazione triangolare che si trovano nel falso lume alla tc , noti come segno del cobweb , quando presenti , sono specifici del falso lume ed aiutano nel suo riconoscimento . 
le misure per stabilire le dimensioni dello endoprotesi da impiegare dovrebbero essere eseguite nelle sequenze mip o nelle immagini assiali prese perpendicolarmente allasse longitudinale allo scopo di evitare errori di volume parziale . risonanza magnetica la rm uno strumento molto accurato per la diagnosi di da in quanto ha uneccellente sensibilit e specificit che si approssimano al 100% in numerosi lavori [ 3235 ]  . 
un mappaggio anatomico dettagliato della da deve includere il tipo e lestensione della dissezione e anche distinguere lorigine e la perfusione dei rami collaterali ( rami dellarco , tripode celiaco , mesenterica superiore , arterie renali e coronarie ) dal vero o dal falso lume . la tecnica gradient - echo fornisce informazioni dinamiche e funzionali [ 36 ]  . 
lintensit del segnale viene ridotta se il flusso lento e quindi fornisce elementi che differenziano il vero lume ( elevata intensit ) dal falso lume ( bassa intensit )  . 
il flusso turbolento determina un segnale vuoto e questo fenomeno permette di identificare turbolenze anomale come comunicazioni tra il vero ed il falso lume . il terzo punto della valutazione pre - operatoria di una da e del suo dettaglio anatomico si basa sullimpiego della angio - rm . 
il foro di ingresso e di rientro appaiono come uninterruzione del flap intimale alle immagini assiali e nelle ricostruzioni mip e volume rendering . angiografia per pi di 20 anni laortografia stata lunica metodica di imaging per lo studio della patologia aortica . 
a detailed anatomic map of ad must indicate the type and extension of dissection but must also distinguish origin and perfusion of branch vessels ( arch branches , celiac , superior mesenteric , renal arteries , coronary arteries ) from the true or false channels . gradient - echo techniques provide dynamic and functional information [ 36 ]  . 
the signal can be reduced if the flow is low , providing elements for differentiating true lumen ( high signal intensity ) from false lumen ( low signal intensity )  . 
turbulent flow produces a signal void , and this phenomenon makes it possible to detect anomalous turbulence such as communications between the true and the false lumen . the third step in preoperative assessment of ad and definition of its anatomic detail relies on the use of gadoliniumenhanced three - dimensional ( 3d ) magnetic resonance angiography ( mra )  . 
because 3d mra is rapidly acquired without any need for electrocardiograph ( ecg ) triggering , it may be used even in severely ill patients and also in patients with renal failure or low cardiac output . 
entry and reentry sites appear as a segmental interruption of the linear intimal flap on axial or sagittal images or in mip and volume rendering reconstruction . angiography for more than 20 years , aortography has been the unique imaging modality for studying aortic pathology and considered to be the diagnostic standard by which to evaluate patients with ad . 
this information is very useful during the endovascular procedure , as tee provides real - time guidance for safe advancement and positioning of the stent - graft device in the true lumen [ 37 , 38 ]  . 
after stent deployment , tee with colour doppler is more sensitive than angiography in identifying endoleaks . pulsed doppler velocity permits distinction of dacron porosity ( usually with a slow velocity < 50 cm / s ) from the faster flow of true persistent leaks ( usually around 100 cm / s )  . 
therefore , tee guidance provides several types of information that can potentially lead to optimal outcome . post - treatment evaluation the goal of endovascular treatment in b - ad is to provide false lumen thrombosis and aortic remodelling with false lumen expansion . 
attualmente , data lelevata capacit diagnostica delle metodiche non invasive , langiografia dovrebbe essere riservata solo ai pazienti nei quali le altre metodiche non siano riuscite a fornire i dettagli anatomici necessari . imaging intraoperatorio : ecocardiografia transesofagea la guida dellimpianto di endoprotesi aortica nella da - b e nellaneurisma toracico richiede sia langiografia che lecocardiogramma transesofageo ( ecote )  . 
le dinamiche di flusso possono essere precisamente evidenziate con il color - doppler differenziando il vero dal falso lume ed i fori di ingresso senza impiego di mezzi di contrasto . queste informazioni sono molto utili durante la procedura endovascolare in quanto lecote una guida in tempo reale del corretto avanzamento e posizionamento dellendoprotesi nel vero lume [ 37 , 38 ]  . 
inoltre , in condizioni di emergenza quando il rischio di rottura non consente di eseguire una tc oppure una rm pre - procedura , pu fornire misurazioni molto precise sulle dimensioni aortiche e del colletto . dopo il posizionamento dellendoprotesi lecote con il color - doppler pi sensibile dellangiografia nellidentificare gli endoleak . 
la velocit al doppler pulsato permette di distinguere tra la porosit del dacron ( bassa velocit < 50 cm / s ) e il veloce flusso di un vero leak peri - stent ( generalmente attorno ai 100 cm / s )  . 
pertanto il monitoraggio ecote fornisce una serie di diverse informazioni che consentono unottimizzazione dei risultati . valutazione dopo trattamento lobiettivo del trattamento endovascolare nella da - b di generare una trombosi del falso lume ed un rimodellamento aortico con espansione del vero lume . 
dopo la procedura obbligatorio un rigido followup di imaging poich lendoleak pu causare unespansione del falso lume ed aumentare il rischio di rottura [ 3943 ]  . una prima valutazione basale post - procedura viene eseguita prima della dimissione oppure entro un mese . 
on the basis of the results of imaging findings , subsequent 3 - , 6and 12 - month imaging follow - up is usually planned in the first postoperative year . 
both mri and ct are reliable techniques even if on mri the metallic component of the stent graft provides artefacts , thus limiting evaluation of the aortic wall . particular attention should be given to identifying a possible endoleak , expressed by reperfusion of the false lumen from flow deriving from the proximal part of the stent graft ( type i ) or from the distal part of the stent graft ( type ii )  . there are no reports about type ii endoleaks from flow deriving from intercostal arteries whereas it is possible to find even at long term a type iii endoleak at the junction of two different stent grafts . 
accurate measurement of true and false lumen dimension are also important for indirect assessment of procedural success because aortic remodelling with false lumen shrinkage and true lumen expansion is an indirect sign of the absence of endoleak . results from the literature at present , there are several reports in the literature attesting to the feasibility of endovascular treatment of b - ad . 
sia la tc che la rm sono metodiche affidabili anche se le componenti metalliche dello endoprotesi non sono valutabili con la rm e determinano artefatti che limitano la valutazione della parete aortica . 
lattenzione maggiore va nella ricerca di eventuali endoleak , evidenziati dalla riperfusione del falso lume da parte della porzione prossimale dello endoprotesi ( tipo i ) oppure da quella distale ( tipo ii )  . 
endoleak tipo ii da riperfusione del falso lume attraverso arterie intercostali sono scarsamente riportati in letteratura , mentre sempre possibile anche a lungo termine un endoleak tipo iii , alla giunzione tra 2 segmenti protesici . 
anche la misurazione accurata delle dimensioni del vero e del falso lume molto importante per una valutazione indiretta del successo procedurale , in quanto il rimodellamento aortico dopo il collasso del falso lume e lespansione del vero lume sono un segno indiretto di assenza di endoleak . risultati della letteratura attualmente ci sono diverse casistiche disponibili in letteratura che dimostrano la fattibilit del trattamento endovascolare nella da - b . 
lincidenza di complicanze maggiori risultata del 10 , 6% ed in particolare le complicanze neurologiche si sono presentate nel 3 , 1% dei pazienti , distribuiti in uno 1% dei pazienti che ha presentato paraplegia ed un fig . 
twentyeight patients died during hospital stay so that we can assume an in - hospital mortality rate of 6.8% even if it is not possible to distinguish which percentage of death was related to the procedure . 
as concerns the subsequent follow - up period , there was a rate of late aortic rupture of 2.5% linked to a late mortality of 3.9%. nowadays , few trials report on endovascular treatment of the thoracic aorta . 
based on observational evidence of potential better outcome of endovascular therapy for ad , the investigation of stent grafts in patients with type b aortic dissection ( instead ) trial was designed as a multicentre , randomised trial that is ongoing in europe . 
the purpose of the study is to compare the outcomes of b - ad subjected to interventional thoracic stent grafting combined as an adjunct with tailored antihypertensive treatment ( stent - graft group ) to those of tailored antihypertensive treatment alone ( medical treatment group )  . according to the results , it will be possible to rule out whether asymptomatic patients are suitable for stent - graft treatment . 
the combined experience of the european collaborators on stent graft techniques for thoracic aortic aneurysm and dissection repair ( eurostar ) and the united kingdom thoracic endograft registries has been recently published [ 44 ]  . the initial and 1 - year outcome of endovascular treatment of thoracic aneurysms and dissections on 443 patients is reported . 
in 89% of patients , primary technical success was achieved ; the remaining 11% had either incomplete covering of the entry tear , persistent flow without thrombosis of the largest portion of the false lumen , no expansion of the true lumen or endoleak . 
late death occurred in 1.5% of patients , and the cumulative survival rate after 1 year was 90% . percutaneous treatment of malperfusion aortic branch - vessel obstruction is one of the most important causes of morbidity and mortality in type b dissection and constitutes a challenge for medical and surgical treatment of the disease . 
the incidence of aortic branch - vessel compromise in association with ad ranges from 25% to 50% [ 45 ]  . ischaemic complications can arise when the dissection compromises blood flow by either extrinsic compression of the true lumen by the false channel or an intimal flap occluding p . 
ventotto pazienti sono deceduti durante il ricovero ospedaliero cosicch si determina una mortalit intra - ospedaliera del 6 , 8% , anche se non possibile differenziare precisamente in quale percentuale la mortalit sia da correlare alla procedura . 
per quanto riguarda il periodo di follow - up successivo , risulta unincidenza di rottura tardiva dellaorta del 2 , 5% con una mortalit a distanza del 3 , 9% . 
basato sullevidenza osservazionale di una prognosi potenzialmente migliore della terapia endovascolare per dissezione aortica , attualmente in corso il trial europeo instead , raccolta dati comparativa multicentrica , prospettica e randomizzata . 
lo scopo del trial di confrontare la prognosi della da - b trattata con impianto di endoprotesi aortica toracica associata a terapia antiipertensiva ( gruppo endoprotesi ) con quella gestita con la sola terapia medica ( gruppo terapia medica )  . 
stata recentemente pubblicata lesperienza combinata del registro eurostar ( european collaborationon on stent graft techniques for thoracic aortic aneurysm and dissection repair ) e del registro united kingdom thoracic endograft [ 44 ]  . 
il successo tecnico primario stato ottenuto nell89% dei pazienti ; il rimanente 11% presentava chiusura incompleta del foro di ingresso , persistenza di flusso senza trombosi del falso lume , mancata espansione del vero lume oppure endoleak . 
nel follow - up a 1 anno eseguito nel 94% dei pazienti , nuovi endoleak sono stati riscontrati nel 2 , 8% dei pazienti e mortalit nel 1 , 5% con un indice di sopravvivenza cumulativo a 1 anno del 90% . trattamento percutaneo della malperfusione lostruzione dei rami collaterali dellaorta una delle cause di morbilit e mortalit nella da - b e costituisce una limitazione nella terapia medica e chirurgica della malattia . lincidenza di compromissione vascolare dei collaterali aortici associata a da - b varia tra il 25% ed il 50% [ 45 ]  . 
le complicanze ischemiche possono presentarsi quando la dissezione compromette il flusso sanguigno o attraverso una compressione estrinseca del vero lume da parte del falso lume oppure per occlusione del collaterale da parte del flap intimale . 
the main mechanisms may involve a static narrowing of the vessel lumen by means of haematoma , or dynamic obstruction of the vessel origin by means of the dissection flap prolapsing into the vessel origalthough peripheral pulse deficit is the most frequent indicator of ischaemia , renal and mesenteric ischaemia and infarction are major causes of morbidity and mortality in patients with acute ad . renal malperfusion syndrome consists of acute renal failure , anuria , uncontrollable hypertension despite full medical therapy , flank pain and haematuria . asymmetrical opacification of renal parenchyma on contrast - enhanced ct or mri is the most significant imaging finding of renal malperfusion . 
however , despite the reperfusion success , the dissected aorta showed progressive enlargement , necessitating thoracoabdominal aortic replacement 6 weeks later . since then , several small series have been reported using a variety of techniques in different indications although there are limited long - term outcome and follow - up data . 
the stanford group [ 8 ] reported their initial experience with the use of aortic branch - vessel stenting in the management of patients with vascular complications from acute and chronic ad . 
 [ 48 ] recently reported their endovascular experience with 24 patients with peripheral vascular complications from ad . they reported a 92% success rate at restoring flow into compromised branch vessels . 
il meccanismo principale pu coinvolgere un restringimento statico del lume del vaso a causa dellematoma oppure unostruzione dinamica dellorigine del vaso a causa del flap intimale che prolassa nel lume del vaso . 
per quanto il deficit dei polsi periferici sia il pi frequente indicatore di ischemia , linfarto e lischemia renale e mesenterica sono le cause maggiori di morbilit e mortalit nella da acuta . 
si pu anche riscontrare il reperto radiologico di sofferenza ischemica delle anse intestinali alla tc . la malperfusione degli arti inferiori si manifesta con dolori agli arti inferiori , assenza di polsi periferici e mancata visualizzazione delle arterie iliache e femorali alla tc o allangio - rm . 
da allora sono state riportate diverse casistiche con numero di pazienti ridotto che valutavano diverse tecniche e diverse indicazioni , anche se non esistono molti dati riguardo la prognosi a lungo termine ed il follow - up . 
 [ 48 ] hanno recentemente documentato la propria esperienza endovascolare con 24 pazienti con complicanze vascolari periferiche da da . viene riportato una percentuale di successo del 92% nel ripristino della perfusione viscerale nei collaterali . 
usually , stent - graft occlusion of the entry site results in thrombosis of the false channel and flow increase in the true lumen , therefore normalising vessel perfusion and restoring branch - vessel patency . 
therefore , immediate relief of malperfusion syndrome may be the first results of endovascular stent graft treatment of ad . trombosi del falso lume ed un aumento di flusso del vero lume con normalizzazione della perfusione del vaso e ripristino della perviet dei vasi viscerali . 
langioplastica dei vasi viscerali o delle arterie iliache pu rendersi saltuariamente necessaria in caso di stenosi fibrotica localizzata nei vasi maggiori o di meccanismo a valvola da prolasso del flap intimale allinterno del lume . 
quindi il recupero immediato della perfusione potrebbe essere il primo risultato del trattamento endovascolare con impianto di endoprotesi della da . conclusions endovascular treatment of b - ad may represent a true advance in the difficult management of this catastrophic disease . 
however , follow - up data and results of randomised trials are necessary to confirm longterm reliability and improvement in prognosis . conclusioni il trattamento endovascolare della da - b pu rappresentare un vero progresso nella difficile gestione di questa temibile malattia . 
fugazzola1 1radiologia vascolare e interventistica cattedra di radiologia , 2cattedra di statistica , universit degli studi dellinsubria , viale borri 57 , i - 21100 varese , italy 3servizio di anestesia e cure palliative , 4divisione di urologia , ospedale di circolo , varese , italy correspondence to : g . 
in the last 3 years , 299 procedures of nephrostomy were performed on 201 patients ( 93 women , 108 men ; mean age 65.7 years , range 32102 years ) at our institute ; all patients were affected by malignancy . 
access to the pyelocalyceal system ( intermediate or lower calices ) was performed by using a seldinger technique in 255 / 299 cases , or a one - step technique ( ost ) in 44 procedures when grade 4 hydronephrosis was present . 
we observed 43 / 299 ( 14.4% ) dislodgements : 32 / 255 ( 10.70% ) with the seldinger technique and 11 / 44 ( 3 , 68% ) with ost . 
from the statistical analysis , we conclude that the examination technique modifies the percentage of complications ; in particular , it significantly ( p < 0.05 ) influences complications connected with the catheter but not minor complications . 
negli ultimi 3 anni , sono state eseguite , presso il nostro istituto , 299 procedure di nefrostomia in 201 pazienti ( 93 donne , 108 uomini ; et media 65 , 7 anni , range 32102 anni ) ; tutti i pazienti erano affetti da patologia neoplastica . 
in 44 casi ( 14 , 72% ) , i pazienti presentavano idronefrosi di iv grado , nelle restanti 255 procedure ( 85 , 28% ) idronefrosi di ii - iii grado . 
laccesso al sistema pelvi - caliciale ( calici intermedi o del gruppo inferiore ) stato effettuato usando la tecnica di seldinger in 255 / 299 casi o one - step technique ( ost ) nelle 44 procedure in cui era concomitante idronefrosi di iv grado . 
non si sono osservate complicanze maggiori . complessivamente il tasso di complicanze minori risultato del 3 , 01% ( 9 / 299 casi ) ; 8 / 255 ( 3 , 13% ) casi con tecnica di seldinger ; 1 / 44 ( 2 , 27% ) casi con ost . 
si sono verificate 4 / 299 ( 1 , 33% ) rotture del catetere e 2 / 299 ( 0 , 67% ) kinking ( tutti i casi con ost )  . dallanalisi statistica dei risultati si deduce che la tecnica di esame modifica le percentuali di complicanze ; in particolare , influenza significativamente ( p < 0 , 05 ) le complicanze legate al catetere , ma non le complicanze minori . 
la tecnica ost indicata nel caso di imponente idronefrosi e nei casi in cui la permanenza del catetere sia di breve durata ; la tecnica di seldinger eseguibile in pazienti con idronefrosi di grado ii e iii e in previsione di un g . 
since its first application , this interventional procedure has been performed on a large series of patients , with high success rates and low complication rates [ 228 ]  . 
the purpose of our paper is to present our experience concerning the complications associated with pcn performed in the last 3 years at our institution . negli ultimi anni , linterventistica urologica ha assunto un ruolo importante nella gestione delluropatia ostruttiva , a partire dal posizionamento della prima nefrostomia percutanea ( npc ) , effettuata nel 1955 da goodwin et al [ 1 ]  . 
dalla sua prima applicazione , tale procedura interventistica stata eseguita in un grande numero di pazienti , associata ad alte percentuali di successo e a bassi tassi di complicanze [ 228 ]  . lo scopo di questo studio presentare la nostra esperienza riguardante le complicanze associate alle npc effettuate negli ultimi 3 anni presso il nostro centro . materials and methods patients in the last 3 years , 299 pcn procedures have been performed on 201 patients ( 93 women , 108 men ; mean age 65.7 years , range 32102 years ) ; all patients were affected by malignancy . 
in 44 / 299 ( 14.72% ) cases , ultrasound performed prior to the procedure showed the presence of severe hydronephrosis ( grade iv ) whereas in 255 / 299 ( 85.28% ) cases , hydronephrosis was grade iiiii . 
sixty - eight ( 23.07% ) procedures were carried out under emergency conditions because of the rapid worsening of renal function related to ureteral obstruction . all in all , 149 pcns on the right side and 88 on the left side were performed ; 31 patients underwent bilateral pcn . technique all patients had normal preprocedure coagulation and platelet ( plt ) estimation [ international normalised ratio ( inr ) > 1.3 ; and plt < 30 , 000 / dl were considered as a contraindications ]  . 
all procedures were carried out in a dedicated interventional room under ultrasound and fluoroscopic guidance , with haemodynamic monitoring facilities ( continuous measurement of oxygen saturation and pulse rate with blood pressure recorded every 5 min )  . 
in 271 / 299 , only local anaesthetic was used ( 10 ml carbocaine 2% ) at the site of puncture ; in 28 / 299 cases , intravenous sedoanalgesia was necessary because of lack of collaboration or excessive pain according to the principles of monitored anaesthesia care ( mac ) ( by using a combination of propofol , midazolam and fentanyl in doses adequate to patient weight and procedure length )  . 
access to the pelvicalyceal system ( intermediate or lower pole calyces ) , usually located under ultrasound guidance , was attempted using a seldinger technique in 255 / 299 cases or a one - step technique ( ost ) in 44 / 299 cases ; the latter was used only when the excretory system was very dilated ( grade iv hydronephrosis )  . 
for both techniques , the pamateriali e metodi pazienti durante gli ultimi 3 anni , sono state eseguite 299 procedure di npc in 201 pazienti ( 93 donne , 108 uomini ; et media 65 , 7 anni , range 32102 anni ) ; tutti i pazienti erano affetti da patologia di natura neoplastica . in 44 / 299 casi ( 14 , 72% ) , lesame ecografico espletato prima della procedura ha mostrato la presenza di idronefrosi di grado severo ( iv ) , mentre in 255 / 299 ( 85 , 28% ) di idronefrosi di ii - iii . 
the seldinger technique involves an ultrasound - guided puncture of the dilated collecting system with a sheathed 19 - gauge needle ( tla needle sheath , boston scientific )  . 
after injection of 10 ml of iodinated contrast medium ( iopamiro 300 , bracco ) to opacify the cavity , under fluoroscopy , we insert a 0.035hydrophilic guide wire ( terumo ) , and upon this wire , we advance the needle sheath . 
we then change the hydrophilic wire with a 0.035super - stiff guide wire ( amplatz , boston scientific ) to insert an 8 fr glidex pigtail catheter ( flexima , boston scientific )  . 
the ost involves a puncture , under ultrasound / fluoroscopic guidance , by using an 8 fr catheter mounted on a hollow 18 - gauge needle ( inter - v , pbn medicals )  . 
under ultrasound guidance , the tip of the needle is inserted into the pelvicalyceal system , and then the catheter slides over the needle into the collecting systein 272 / 299 procedures ( 91% ) , only one puncture was performed to gain access to pelvicalyceal system ; in 18 / 299 procedures ( 6.02% ) two punctures were necessary , and another 9 / 299 procedures ( 3% ) required more than two punctures . 
all patients received a prophylactic antibiotic regimen with a thirdgeneration cephalosporin and gentamicin beginning immediately before the procedure and continuing for the following 4 days . analysis of results statistical analysis of the results was performed by using bilateral tests on proportions as well as 2 test of independence for contingency tables . results results were analysed separately for the seldinger technique and for the ost . 
evaluation of complications was achieved using the following classifications [ 19 , 20 , 25 , 29 , 30 ] : ( 1 ) major complications ( death during or soon after the interventional procedure for causes related to the procedure ; haematuria requiring surgical management or blood transfusion ; vascular laceration , pseudoaneurysm or arteriovenous fistula ; infection requiring surgical management ; sepsis ; puncture of adjacent organs such as colon , spleen , lung ) ; ( 2 ) minor complications ( urine leakage ; macroscopic haematuria with clot formation ; infection treated with medical therapy ; subcapsular or perirenal haematoma not requiring surgical intervention or blood transfusion ) ; ( 3 ) tube complications ( displacement , occlusion , kinking , fracture )  . 
sotto guida ecografica , la punta dellago introdotta nel calice ; successivamente il catetere viene fatto scivolare sullago e avanzato nelle cavit renali . in 272 / 299 procedure ( 91% ) stato effettuato un solo passaggio con lago per accedere ai calici , in 18 / 299 procedure ( 6 , 02% ) sono stati necessari 2 passaggi e in 9 / 299 procedure ( 3% ) pi di 2 passaggi . per il fissaggio del catetere stata utilizzata una sutura alla cute con filo ( 2 / 0 daflon blue b / braun , aesculap ) in 92 / 299 casi ( 31% ) ; in 111 / 299 ( 37% ) stato utilizzato un device adesivo ( drain - fix , unomedical ltd ) e in 96 / 299 ( 32% ) sono stati associati entrambi i sistemi . a tutti i pazienti stata somministrata una profilassi antibiotica con cefalosporina di terza generazione associata a gentamicina , immediatamente prima della procedura e per i 4 giorni successivi . analisi dei risultati lanalisi statistica dei risultati stata effettuata utilizzando test bilaterali sulle proporzioni e test 2 quadrato di indipendenza per tabelle di contingenza . risultati i risultati sono stati analizzati separatamente per la tecnica di seldinger e per la tecnica one - step . 
1 pielografia transnefrostomica che conferma il corretto posizionamento del catetere nefrostomico con approccio dal gruppo dei calici inferiori . served no major complications ; no patient died for causes related to the procedure . 
catheter dislodgement rates were then analysed based on the fixation system to the skin : 6 / 43 ( 13.9% ) in cases fixed with suture ; 35 / 43 ( 81.4% ) in cases fixed with an adhesive device ; 2 / 43 ( 4.6% ) when both systems were used ( table 2 )  . ( 3 , 7% ) con one - step technique ; 4 / 299 ( 1 , 3% ) rotture del catetere ( tutte con one - step technique ) , 2 / 299 ( 0 , 7% ) kinking del catetere ( entrambi conone - step technique )  . 
i tassi di sposizionamento del catetere sono stati poi analizzati in base al sistema di fissaggio alla cute utilizzato : 6 / 43 ( 13 , 9% ) sposizionamenti del catetere si sono verificati in caso di catetere fissato con sutura ; 35 / 43 ( 81 , 4% ) con catetere fissato con device adesivo ; 2 / 43 ( 4 , 6% ) in casi dove erano stati utilizzati entrambi i sistemi ( tabella 2 )  . complessivamente abbiamo osservato un tasso di complicanze del 19 , 4% ( 58 / 299 )  . 
b il controllo pielografico espletato 3 giorni dopo la procedura documenta la risoluzione del leak urinoso con assenza di spandimenti di mezzo di contrasto perirenali . inoltre , il sistema di fissaggio non influenza la percentuale di sposizionamenti . discussione nonostante i notevoli progressi delle tecniche chirurgiche e del trattamento radioterapico e chemioterapico dei tumori urogenitali , ginecologici e intestinali , queste neoplasie , in fase avanzata , spesso provocano uropatia ostruttiva , per invasione locale o diffusione metastatica [ 3138 ]  . la decompressione palliativa del sistema urinario ostruito , mediante nefrostomia e stent ureterale , una metodica ampiamente utilizzata per preservare la funzionalit renale [ 3336 ] in elezione e in urgenza [ 24 ]  . i dati riportati in letteratura [ 3 , 5 , 6 , 9 , 12 , 1521 , 23 , 25 ] dimostrano lefficacia della metodica ( 13 , 7% complicanze ) che , in relazione alla sua mini - invasivit , presenta bassi tassi di mortalit e morbilit sia in elezione che in urgenza [ 25 , 19 ] ( tabella 3 )  . nel nostro studio abbiamo riportato una mortalit correlata alla procedura dello 0% , con tasso di complicanze minori del 3% , significativamente pi basso di quanto riportato in letteratura . dalle esperienze riportate in letteratura risulta che uno dei fattori principali che determina lincidenza delle complicanze lesperienza delloperatore : secondo le linee guida scvir e quanto riportato da alcuni autori [ 4 , 39 ] , necessario eseguire non meno di 1020 procedure / anno al fine di mantenere un livello sufficiente di abilit e di famigliarit nelluso dei devices necessari . la sicurezza della procedura inoltre legata al rispetto delle indicazioni cliniche ed in particolare alla valutazione fig . 
statistical analysis indicates that the technique used modifies the percentage of complications ; particularly , it significantly influences technical ( p < 0.05 ) tube - related complications but not minor complications . 
palliative decompression of the obstructed urinary system by means of a nephrostomy catheter and ureteral stent is a widely used method for preserving renal function [ 3336 ] in both elective and emergency settings [ 24 ]  . 
data reported in the literature [ 3 , 5 , 6 , 9 , 12 , 1521 , 23 , 25 ] show the effectiveness of the technique ( 13.7% complications ) that , thanks to its minimal invasiveness , presents low morbidity and mortality rates in elective and emergency settings [ 25 , 19 ] ( table 3 )  . 
exdei parametri della coagulazione e al grado di idronefrosi presente ( nella nostra casistica tutti i pazienti presentavano idronefrosi di ii - iv grado )  . necessario poi prendere in considerazione una serie di parametri tecnici che determinano la frequenza di insorgenza di complicanze . 
in addition , safety of the procedure is related to adhesion to clinical indications and , in particular , to evaluation of coagulation parameters and hydronephrosis grade ( in our experience , all patients had grade iiiv hydronephrosis )  . 
with regard to the correct technical execution of the procedure , first , good anatomic - topographic knowledge of the kidney and surrounding structures is required in order to select safe access to perform pcn [ 4044 ]  . 
the 12th rib , the iliac crest and the posterior axillary line are important cutaneous landmarks , and the path of calyx branches ideally should be projected by the physician on the dorsolumbar access site . 
direct puncture of the renal pelvis should be avoided in connection with the risk of urinary leakage and proximity of vascular hilar structures that could be harmed during the procedure [ 45 ]  . 
the ideal approach should be performed in posterolateral projection , at the joining of anterior two thirds of the renal parenchyma with posterior one third by pricking a calyx of the inferior group , as this is a relatively avascular area [ 16 , 45 ]  . 
as a matter of fact , the renal artery divides into two major branches , ventral and dorsal , and its division creates an avascular zone known as brdels line , which lies between the vascular districts of the ventral and dorsal branch of the renal artery [ 41 , 42 ]  . 
the use of this area for renal puncture should lower the risk of bleeding complications [ 16 , 41 , 42 , 4549 ]  . in our study ultrasound was used to perform the procedure ( it confirms the correctness of the approach , locates the calyx of the lower group to be pricked and visualises needle position and advancement in real time ) together with fluoroscopy ( which allows checking needle position and following catheter progression )  . 
data reported in the literature show that the percentage of success by using fluoroscopy alone or fluoroscopy combined with sonography ranges from 98% to 100% [ 40 , 42 , 50 ]  . 
thanks to the availability of nephrostomic catheters fitted with tapered tip and good pushability and of stiff guide wires , the use of track dilators could be reserved to obese patients only , in which subcutaneous tissue dilation is necessary . 
among tube - related complications , dislodgement is the most frequent , and it depends more on the system of fixing to the skin than on the type of catheter used and on its system of securement ( pigtail or balloon )  . 
in our experience , a minor rate of dislodgements occurred in patients for whom adhesive devices together with suture stitchdi poter selezionare un accesso sicuro per effettuare la npc [ 4044 ]  . 
la xii costa , la cresta iliaca e la linea ascellare posteriore sono reperi di orientamento cutaneo e il decorso delle diramazioni caliciali deve essere idealmente proiettato dalloperatore sulla zona daccesso dorso - lombare . 
la puntura diretta della pelvi renale deve essere evitata in relazione al rischio di stravaso di urina e alla vicinanza delle strutture vascolari ilari che possono essere lese durante la procedura [ 45 ]  . lapproccio ideale dovrebbe essere effettuato in proiezione postero - laterale , al congiungimento dei 2 / 3 anteriori del parenchima renale con il 1 / 3 posteriore , pungendo un calice del gruppo inferiore , essendo questa regione relativamente avascolare [ 16 , 45 ] ; infatti , larteria renale si divide in 2 rami maggiori , ventrale e dorsale , e la loro suddivisione crea una regione avascolare ; tale zona nota come linea di brdel ( brdels line ) ed localizzata al confine tra i territori vascolari del ramo ventrale e del ramo dorsale dellarteria renale [ 41 , 42 ]  . 
lutilizzo di tale area per la puntura renale ridurrebbe il rischio di complicanze emorragiche [ 16 , 41 , 42 , 4549 ]  . per lespletamento della procedura , nella nostra esperienza stata utilizzato il controllo ecografico ( che consente di confermare la correttezza dellapproccio , di individuare il calice del gruppo inferiore da pungere e di visualizzare la posizione e lavanzamento dellago in tempo reale ) associato a quello fluoroscopico ( che permette il controllo del posizionamento dellago e di seguire la progressione del catetere ) ; dati riportati in letteratura dimostrano che la percentuale di successo utilizzando unicamente la fluoroscopia o lassociazione del controllo scopico e sonografico , varia tra il 98 e il 100% [ 40 , 42 , 50 ] ; tali percentuali sono lievemente pi basse quando usato il solo controllo ecografico [ 40 , 42 , 50 ]  . grazie alluso di cateteri nefrostomici dotati di punte rastremate e di buona pushability e di guide rigide , lutilizzo dei dilatatori fasciali pu essere riservato ai soli pazienti obesi , nei quali necessaria la dilatazione del tessuto sottocutaneo ; nella nostra esperienza lastensione dallutilizzo di tali devices in pazienti non obesi riduce il traumatismo a carico del parenchima renale e il numero di complicanze emorragiche . infatti , tale approccio , inoltre , ha il vantaggio di ridurre il tempo complessivo della procedura e di esposizione del paziente ai raggi x . tra le complicanze legate al catetere nefrostomico , lo sposizionamento il problema pi frequente e , pi che al tipo di catetere utilizzato e al suo sistema di ancoraggio ( pig - tail o palloncino ) , appare correlato al sistema di fissaggio dello stesso alla cute ; nella nostra esperienza il minore tasso di sposizionamenti si avuto nei pazienti nei quali stata utilizzata lassociazione del device adesivo e dei punti di sutura . inoltre molto importante istruire il paziente e i familiari riguardo alla manutenzione del catetere , e soprattutto svuotare periodicamente la sacca di raccolta connessa , il cui peso spesso causa di sposizionamento . 
in addition , it is very important to teach the patient and his or her relatives how to maintain the catheter and , above all , to periodically empty the connecting bag , the weight of which is often a cause of dislodgement . 
nephrostomic catheter replacement should be performed every 23 months because a span longer than 3 months almost always involves its obstruction [ 27 ]  . conclusions pcn is a widely used technique , with a high technical success rate and low rate of complications . 
safety of the procedure is strictly related to correct indications and technical procedures ( reduced risk of bleeding and vascular lesions ) , adequate antibiotic prophylaxis ( reduced risk of sepsis ) and proper maintenance of the catheter and drainage bag , associated with catheter fixation catheter to the skin with adhesive plaque and suture stitches ( low risk of dislodgements )  . 
therefore , the ost technique should be proposed only in patients with grade 4 hydronephrosis and in patients for whom persistence of a drainage catheter is not necessary for an extended period due to the high number of tube - related complications ( dislodgements , fractures and kinking )  . 
on the other hand , the seldinger technique could be proposed in all patients even if the catheter is necessary for a long period . la sostituzione del catetere nefrostomico deve essere effettuata ogni 23 mesi , poich un intervallo pi lungo di 3 mesi quasi invariabilmente comporta lostruzione dello stesso [ 27 ]  . conclusioni la npc una tecnica estesamente utilizzata , con una percentuale di successo tecnico elevato e bassi tassi di complicanze . la sicurezza della procedura strettamente correlata al rispetto delle indicazioni e alla corretta esecuzione tecnica ( ridotto rischio di sanguinamenti e di lesioni vascolari ) ad una adeguata profilassi antibiotica ( ridotto rischio di sepsi ) ed infine alla corretta manutenzione del catetere e della sacca di raccolta associati al fissaggio del catetere alla cute , con placca adesiva e punti di sutura ( riduzione del rischio di sposizionamento del catetere )  . 
colavita1 1unit operativa di diagnostica per immagini , 2unit operativa di broncopneumologia , 3unit operativa di medicina 2 , ospedale generale provinciale di rieti , rieti , italy correspondence to : t . 
cosentini , via riposati 19 , i - 02100 rieti , italy , e - mail : tcosentini@sirm.org received : 22 february 2005 / accepted : 18 october 2005 / published online : 25 may 2006 abstract purpose . 
the aim of this study was to evaluate bone marrow reconversion in patients with obstructive sleep apnoea syndrome ( osas ) by means of magnetic resonance imaging ( mri )  . 
during a 35 - month period , 33 patients with a clinical diagnosis of osas , obese but without restrictive or obstructive ventilatory defects , were evaluated with mri during wakefulness in all patients with t1 - , pdand t2 - weighted sequences in the sagittal and axial plane within 1 week after polysomnography . 
patients with bone marrow reconversion showed higher mean haematocrit ( ht ) values , lower mean nocturnal oxyhaemoglobin saturation , higher percentage of sleep time with oxygen saturation ( sao2 ) < 90% , lower nadir , as well as greater neck adiposity and soft - palate lengthening compared with patients without bone marrow reconversion . 
in patients with osas , bone marrow reconversion is probably correlated with the severity of nocturnal desaturation . as bone marrow reconversion is , for unknown reasons , greater in adults younger than 40 years , mri evidence of bone marrow reconversion could be useful in young individuals for the early diagnosis of sleep - disordered breathing and prevention of associated cardiovascular diseases . 
i pazienti con riconversione midollare hanno rilevato in media valori pi elevati di ematocrito ( ht ) , una saturazione ossiemoglobinica media della notte pi bassa , una percentuale di tempo trascorsa al di sotto del 90% pi elevata ed un nadir pi basso , rispetto a quelli senza riconversione midollare , oltre ad un maggior allungamento del palato molle ed un aumento del tessuto adiposo del collo . 
poich la capacit di riconversione midollare , per ragioni sconosciute , maggiore per gli adulti pi giovani , di et inferiore ai 40 anni , levidenza in rm di riconversione midollare in questi pazienti potrebbe essere utile ai fini di una diagnosi precoce e di una prevenzione delle patologie cardiovascolari associate allosas . parole chiave osas risonanza magnetica orofaringe midollo osseo introduction introduzione t . 
osas is associated with cardiorespiratory diseases ( pulmonary hypertension [ 2 ] , systemic hypertension [ 3 ] , cardiac arrhythmias [ 4 ] , cardiac ischaemia [ 5 ] ) , cerebral ischaemia [ 6 ] and decreased survival [ 7 ]  . 
diagnostic imaging plays a primary role in grading the disease and determining the site of obstruction and coexistence of airway disorders , all of which will guide the clinician in planning the most appropriate treatment [ 8 , 9 ]  . 
 morphological appearance and signal of tissues under examination were considered together with some quantitative parameters for evaluation of the site and extent of obstruction . in particular , we evaluated axial scans perpendicular to the posterior oropharyngeal wall to identify areas of greater airway narrowing and determine site ( retropalatal and / or retrolingual ) and surface in square millimetres and shape ( rounded , oval with greater sagittal axis , oval with greater transverse axis )  . 
 stata documentata associazione fra osas e danni a carico dellapparato cardiorespiratorio ( ipertensione polmonare [ 2 ] , ipertensione sistemica [ 3 ] , aritmie cardiache [ 4 ] , ischemia cardiaca [ 5 ] ) , ischemia cerebrale [ 6 ] ed infine riduzione della sopravvivenza [ 7 ]  . tale sindrome determina inoltre generalmente alterazioni delle concentrazioni di gas ematici nel senso dellipossiemia e dellipercapnia . la diagnostica per immagini ( nellambito della quale sono state e sono tuttora variamente utilizzate la radiologia tradizionale , la tomografia computerizzata e la risonanza magnetica ) gioca un riconosciuto ruolo di primo piano per il grading della malattia , la determinazione del livello dellostruzione , la coesistenza di patologia delle vie aeree , che sono di guida al clinico per la scelta e la modulazione della terapia pi appropriata [ 8 , 9 ]  . 
questo lavoro ha lo scopo di aggiungere alle informazioni sopra menzionate quella riguardante lo stato di attivazione del midollo osseo ottenibile con risonanza magnetica , non essendo stata finora , a nostra conoscenza , segnalata in letteratura una esplicita correlazione fra tale parametro ed osas . materiali e metodi nel periodo gennaio 2001novembre 2003 sono stati esaminati con risonanza magnetica 33 pazienti con diagnosi clinica di osas ( 31 maschi e 2 femmine )  . 
let dei pazienti era compresa fra 26 e 79 anni ( mediasd , 5412 anni )  . lo studio di risonanza magnetica stato condotto con apparecchio picker eclipse 1 , 5 t presso lospedale generale provinciale di rieti mediante sequenze se t1 dipendenti condotte sul piano sagittale ( tr / te 430 / 12 ms , spessore di strato 4 mm , gap 1 mm , fov 22 cm , matrice 192256x256 ) ed assiale ( tr / te 690 / 12 ms , spessore di strato 45 mm , gap 1 mm , fov 24 cm , matrice 256x256 ) e fse pesate in dp e t2 condotte secondo il piano assiale ( tr / te 3000 / 1296 , spessore di strato 5 mm , gap 1 mm , fov 24 cm , matrice 256x256 ) ; le scansioni assiali sono state eseguite dalla volta epifaringea al piano glottico . stata impiegata bobina in quadratura . 
la valutazione degli esami rm stata effettuata da parte di un lettore non a conoscenza dei parametri clinicostrumentali . sono stati presi in considerazione laspetto morfologico ed il segnale dei tessuti componenti la regione esaminata ed alcuni fra i parametri quantitativi espressi in letteratura per la valutazione della sede e del grado dellostruzione . 
for evaluation of mouth - floor lowering we preferred to measure , on the midline sagittal scan , the angle formed by the geniohyoid muscle and the perpendicular line to the longitudinal oropharyngeal axis , which we believe to be geometrically less dependent on the degree of patients neck flexion inside the magnet and on individual conformation of the splanchnocranial elements . 
osas diagnosis was made by clinical - anamnestic evaluation ( chronic snoring with witnessed apnoea , daytime sleepiness evaluated according to the epworth scale ) and polysomnography ( somnostar 4100 , sensormedics ) [ apnoea / hypopnoea index ( ahi ) > 10 ]  . 
mri findings were correlated with the following parameters : body mass index ( bmi ) , ahi , haematocrit ( ht ) , arterial oxygen partial pressure ( pao2 ) at room air during wakefulness , arterial carbon dioxide partial pressure ( paco2 ) during wakefulness and at rest , average nocturnal oxyhaemoglobin saturation ( percent sao2 ) , percentage of total sleep time with sao2 lower than 90% ( tst% ) , forced vital capacity ( fvc% ) , maximum forced expiratory volume in 1 s ( fev1% ) , fev1 / fvc% ratio , minimum oxygen saturation ( nadir )  . 
no statistically significant difference was observed between the group of patients with bone marrow activation and the group without bone marrow activation as regards mean age , bmi , respiratory functional parameters ( fvc% , fev1% , fev1 / vc ) , pao2 and paco2 during wakefulness and at rest and ahi . 
on the contrary , the difference was statistically significant for ht , sleeping - time percentage with average oxyhaemoglobin saturation below 90% ( %tst ) , average nocturnal oxyhaemoglobin saturation ( %sao2 ) and nadir . 
no statistically significant difference was found as regards mean minimal area surface , geniohyoid muscle length and geniohyoid / oropharyngeal perpendicular angle ; by contrast , the difference was statistically evident with regard to soft - palate length . ticolare sono state valutate le scansioni assiali , perpendicolari alla parete posteriore dellorofaringe e , individuate su queste le aree di maggior ristrettezza del lume aereo , ne sono state considerate la sede ( retropalatale e / o retrolinguale ) , la superficie in millimetri quadrati e la forma ( rotondeggiante , ovale a maggior asse sagittale , ovale a maggior asse trasverso )  . 
la presenza di macroglossia stata considerata sulla base dellaspetto arcuato a convessit esterna , nelle scansioni assiali , del complesso muscolare iostiloglosso e dellaumento dellasse trasverso linguale che di norma non supera i 5 c sono stati valutati soggettivamente lincremento di tessuto adiposo del collo ( con particolare riguardo alla presenza , nelle scansioni assiali , di cuscinetti adiposi in sede perifaringea postero - laterale ) e la dislocazione posteriore della lingua ( sulla base del contatto della lingua con il margine anteriore dellepiglottide )  . la lunghezza del palato molle e la lunghezza del muscolo genioioideo sono state misurate in millimetri sulla scansione sagittale mediana . 
per la valutazione del grado di depressione del pavimento orale abbiamo ritenuto preferibile misurare , sulla scansione sagittale mediana , langolo compreso fra il muscolo genioioideo e la linea perpendicolare allasse longitudinale orofaringeo , che a nostro avviso geometricamente meno dipendente dal grado di flessione del collo che il singolo paziente assume allinterno del magnete e dalla conformazione individuale degli elementi dello splancnocranio . stato valutato retrospettivamente il midollo osseo del clivus e della porzione di rachide cervicale compresa nel piano di studio sulle sequenze sagittali se t1 - pesate , considerando segno di riattivazione midollare la presenza di riduzione dellintensit di segnale pi o meno diffusa rispetto a quanto da attendersi nelle relative fasce det dei pazienti esaminati . la diagnosi di osas stata eseguita tramite valutazione clinico - anamnestica ( russamento cronico con apnee testimoniate , sonnolenza diurna valutata con scala di epworth ) e polisonnografica ( somnostar 4100 , sensormedics ) ( indice di apnea / ipopnea , ahi > 10 )  . 
i parametri rm sono stati correlati con i seguenti parametri : body mass index ( bmi ) , indice di apnea / ipopnea ( ahi ) , ematocrito ( ht ) , pressione parziale di o2 arteriosa in aria ambiente e veglia ( pao2 ) e pressione parziale di co2 ( paco2 ) in veglia ed a riposo , saturazione ossiemoglobinica media della notte ( percentuale sao2 ) , e percentuale di tempo di sonno trascorso con una percentuale sao2 al di sotto del 90% ( % tst ) , capacit vitale forzata ( fvc% ) , volume massimo espiratorio al secondo ( fev1% ) , rapporto fev1 / fvc% , saturazione di o2 minima raggiunta ( nadir )  . la significativit statistica stata indagata con i seguenti test : test t di student , indice di correlazione , test del 2 . 
 stato considerato significativo un valore del p < 0 , 05 . risultati dei 33 soggetti studiati ( m 31 , f 2 ; et media 5412 anni ) , rappresentati in prevalenza da soggetti affetti da grave sint . 
a a 58 - year - old patient with obstructive sleep apnoea syndrome ( osas ) showing decrease of signal intensity in bone marrow of the clivus and cervical vertebrae . 
tra i due gruppi di pazienti che presentavano e non presentavano attivazione del midollo osseo nessuna differenza statisticamente significativa stata rilevata tra le medie di : et , bmi , ( fvc% , fev1% , i parametri fev1 / vc ) , la pao2 e la paco2 in veglia ed a riposo e lindice di apnea / ipopnea ( ahi ) , mentre una differenza statisticamente significativa stata rilevata tra lht , la percentuale di tempo di sonno trascorso con una saturazione ossiemoglobinica media al di sotto del 90% ( % tst ) , la saturazione ossiemoglobinica media della notte ( % sao2 ) ed il nadir . 
nessuna differenza statisticamente significativa stata rilevata tra le medie della superficie dellarea minima , la lunghezza del genioioideo e langolo genioioideo / perpendicolare orofaringe ; mentre una differenza statisticamente significativa stata rilevata con la lunghezza del palato molle . i pazienti con evidenza di midollo osseo attivato hanno dimostrato una maggior presenza di adiposit del collo ( p < 0 , 05 ) , mentre nessuna differenza statisticamente significativa stata rilevata tra i due gruppi rispetto alla presenza o meno di macroglossia e dislocazione posteriore della lingua . 
nei soggetti senza attivazione del midollo la sede dellarea minima stata rilevata in sede retropalatale nel 100% dei casi : 16 come unica sede ( 72 , 7% ) , 5 con associazione in sede retrolinguale ( 22 , 7% )  . 
nei soggetti con attivazione midollare la sede dellarea minima stata retropalatale nel 100% dei casi : 7 come unica sede ( 63 , 6% ) , 4 con associazione in sede retrolinguale ( 36 , 4% )  . 
paziente di 53 anni affetto da osas : abbastanza uniforme riduzione del segnale del midollo osseo del clivus e della colonna cervicale . patients with bone marrow activation showed increased neck adipose tissue ( p < 0.05 ) whereas no statistically significant difference was observed between the two groups with regard to the presence of macroglossia and posterior dislocation of the tongue . 
data are averagesd parameter nonactive bone marrow active bone marrow statistical significance n.s. , not significant ; bmi , body mass index ; fvc , forced vital capacity ; fev1 , forced expiratory volume in 1 s ; pao2 , arterial oxygen partial pressure ; paco2 , arterial carbon dioxide partial pressure ; ht , haematocrit ; ahi , apnoea / hypopnoea index ; tst , total sleep time with sao2 lower than 90% ; sao2 , oxygen saturation tabella 1 caratteristiche cliniche e funzionali dei pazienti . 
 it is interesting to note that in patients with rounded minimal area shape , there is no statistically significant difference in ht , bmi , minimal area surface , pao2 , paco2 , nel 31 , 8% dei casi rotondeggiante ( 7 ) , nel 4 , 5% dei casi sagittale ( 1 ) , nel 31 , 8% dei casi traversa ( 7 ) e nel 31 , 8% dei casi mista ( 7 )  . 
nei soggetti con attivazione midollare la forma dellarea minima invece risultata nel 54 , 5% dei casi rotondeggiante ( 6 ) , nel 9 , 1% dei casi sagittale ( 1 ) , nel 27 , 3% dei casi traversa ( 3 ) e nel 9 , 1% dei casi mista ( 3 )  . 
la presenza di forma dellarea minima rotonda e sagittale si dimostrata collegata ad una superficie dellarea minima significativamente pi piccola rispetto alla forma trasversale ( 2812 versus 4719 , p < 0 , 01 )  . 
una differenza statisticamente significativa stata anche rilevata tra i valori della pao2 in veglia ed a riposo ( 736 versus 806 , p < 0 , 02 ) , la percentuale di sao2 media ( 885 versus 922 , p < 0 , 05 ) ed il nadir ( 6613 versus 776 , p < 0 , 02 ) , ma non per la percentuale di tst , lht , la paco2 in veglia ed a riposo , lahi ed il bmi . interessante losservazione che allinterno del gruppo dei soggetti con area minima rotondeggiante non esistono differenze statisticamente significative nei seguenti parametri : ht , bmi , superficie dellarea minima , pao2 , paco2 , percentuale di tst , percentuale di sao2 e nadir , tra i soggetti con midollo attivato e non attivato . 
i soggetti con area table 2 differences in patients with active or nonactive bone marrow and magnetic resonance imaging ( mri ) parameters mri parameters nonactive bone marrow active bone marrow statistical significance t . 
le differenze tra le medie di diversi parametri divengono invece statisticamente significative quando analizziamo i soggetti con area minima rotonda e sagittale con attivazione midollare e quelli con area minima trasversa senza attivazione midollare , come indicato nella tabella 3 . nel totale del campione lindice di apnea / ipopnea ( ahi ) risultato correlato positivamente al bmi ( r = 0 , 6786 , p < 0 , 0001 ) , allematocrito ( r = 0 , 3829 , p < 0 , 05 ) , alla paco2 in veglia ed a riposo ( r = 0 , 5154 , p < 0 , 01 ) ed alla percentuale di tempo di sonno trascorso con saturazione ossiemoglobinica al di sotto del 90% ( r = 0 , 7763 , p < 0 , 001 ) e correlato negativamente alla pao2 in aria ambiente ed in veglia ( r = 0 , 5611 , p < 0 , 001 ) , alla saturazione ossiemoglobinica media della notte ( r = 0 , 6309 , p < 0 , 001 ) ed al nadir ( r = 0 , 5124 , p < 0 , 001 )  . 
nessuna correlazione statisticamente significativa stata rilevata con il bmi e lo ht . nei soggetti con evidenza di midollo osseo attivato nessuna correlazione stata rilevata tra ahi e superficie dellarea minima e tra ahi , ematocrito e nadir , mentre si mantenevano le correlazioni con gli altri parametri ( bmi r = 0 , 7559 , p < 0 , 001 ; pao2 r = 0 , 6612 , p < 0 , 02 ; paco2 r = 0 , 6356 , p < 0 , 02 , percentuale di tst < 90% r = 0 , 7730 , p < 0 , 001 ; percentuale di sao2 media r = 0 , 6383 , p < 0 , 02 )  . in questo gruppo di pazienti la superficie dellarea minima non risultata correlata con nessun parametro . nel totale del campione , inoltre , i pazienti con adiposit del collo presentavano un bmi pi elevato ( 356 versus 293 , p < 0 , 02 ) , una sao2% media della notte pi bassa ( 886 versus 932 , p < 0 , 05 ) ed una percentuale di tempo di sonno trascorso con una saturazione ossiemoglobinica pi bassa del 90% significativamente pi bassa ( 4235 versus 119 , p < 0 , 02 ) rispetto a quelli senza evidenza di depositi adiposi del collo . nessuna differenza statisticamente significativa invece risultata tra lo ahi ( 6736 versus 4726 , p = 0 , 1 ) , la pao2 e la paco2 in veglia ed a riposo ( 739 versus 794 , p = 0 , 17 ; 425 versus 393 , p = 0 , 15 ) , lht ( 433 versus 454 ) , la superficie dellarea minima ( 433 versus 454 p = 0 , 7 ) , la table 3 differences between patients with nonactive bone marrow and transverse minimal area and patients with active bone marrow and rounded or sagittal minimal area . 
data are meansd parameter nonactive bone marrow and transverse minimal area shape active bone marrow and rounded and sagittal minimal area shape statistical significance n.s. , not significant ; ahi , apnoea / hypopnoea index ; bmi , body mass index ; pao2 , arterial oxygen partial pressure ; paco2 , arterial carbon dioxide partial pressure ; ht , haemocrit ; tst , total sleep time with sao2 lower than 90% ; sao2 , oxygen saturation tabella 3 differenze tra pazienti con midollo osseo non attivato ed area minima trasversale e pazienti con midollo osseo attivato ed area minima rotonda o sagittale . 
data are meansd parameter active bone marrow with neck fat tissue nonactive bone marrow without neck fat tissue statistical significance ahi , apnoea / hypopnoea index ; bmi , body mass index ; ht , haematocrit ; pao2 , arterial oxygen partial pressure ; paco2 , arterial carbon dioxide partial pressure ; tst , total sleep time with sao2 lower than 90% ; sao2 , oxygen saturation tabella 4 differenze tra pazienti con midollo osseo attivato ed adiposit del collo e pazienti con midollo osseo non attivato senza adiposit del collo . 
statistically significant differences were observed among patients with neck adipose tissue and bone marrow activation with regard to a few parameters as opposed to those without neck adipose tissue or bone marrow activation , as reported in table 4 . 
the latter encloses the medullary cavities that are filled with bone marrow , a loose connective tissue consisting lunghezza del palato molle ( 446 versus 416 , p = 0 , 25 ) , la lunghezza del muscolo genioioideo ( 466 versus 424 , p = 0 , 09 ) e langolo genioioideo / perpendicolare orofaringe , ( 418 versus 367 , p = 0 , 08 )  . 
un importante aumento del tessuto adiposo del collo stato rilevato nel 54 , 5% dei pazienti con evidenza di midollo osseo attivato , contro il 13 , 6% dei pazienti senza evidenza di midollo osseo attivato ( p < 0 , 05 )  . 
nei soggetti con adiposit del collo e midollo osseo attivato sono state rilevate differenze statisticamente significative in alcuni parametri , rispetto ai soggetti senza adiposit del collo e senza attivazione midollare , come mostrato in tabella 4 . 
anche la superficie del lume aereo orofaringeo , inizialmente significativamente ridotta ( c ) ( 18 mm2 ) , appare ampliata nel controllo dopo terapia ( d ) ( 105 mm2 )  . mainly of adipocytes ( yellow bone marrow ) or mature and immature blood cells and the stem cells producing them ( red bone marrow )  . 
the two distinct types of bone marrow have a different chemical composition : red marrow is composed of approximately 40% water , 40% fat and 20% protein whereas yellow bone marrow is composed of approximately 80% fat , 15% water and 5% protein [ 10 ]  . 
this influences the choice of mri as the primary imaging methodology for the study of bone marrow given its optimal contrast resolution capabilities in differentiating fat from other tissues . for correct evaluation , it is necessary to know that the bone marrow changes with age . 
the conversion from red to yellow marrow begins in the periphery of the appendicular skeleton and proceeds centrally , according to a regular and well - known pattern [ 11 ]  . 
anatomicamente esistono due tipi di tessuto osseo : losso compatto ( esterno ) e losso spugnoso ( interno ) ; questultimo circonda cavit midollari che contengono midollo osseo , un tessuto connettivo lasso in cui possono prevalere adipociti ( midollo giallo ) o cellule ematiche mature ed immature e le cellule staminali che le producono ( midollo rosso ) ; questultimo la principale sede di produzione delle cellule ematiche nelladulto . i due tipi di midollo osseo sono caratterizzati da una diversa composizione chimica : il midollo rosso composto approssimativamente per il 40% di acqua , 40% di grasso e 20% di proteine ; il midollo giallo contiene approssimativamente 80% di grasso , 15% di acqua e 5% di proteine [ 10 ]  . ci condiziona la scelta della risonanza magnetica ( rm ) quale metodica per immagini principale per lo studio del midollo osseo , possedendo unottima capacit di risoluzione tern is reached around 25 years of age , when the red marrow is present in the skull , vertebral bodies , sternum , ribs , pelvis , calcaneus and proximal metaphyses of the humerus and femur . 
when there is a demand for additional haematopoiesis due to stress , chronic anaemia , cardiac decompensation or extensive bone marrow replacement [ 10 ] , conversion of yellow to red marrow is initiated . 
it may occur diffusely , or focal areas of red marrow may appear in a background of yellow marrow [ 11 ]  . neither conventional radiology ( cr ) nor ct , despite their different sensitivities in the study of the changes in compact and spongy bone tissue , are sensitive in detecting the distinct qualities of the bone marrow and may be indicative of pathology only indirectly , when changes occur in the bone tissue composition . 
in particular , cr reveals bone marrow replacement disorders only in the case trabecular bone involvement greater than 50% [ 12 ]  . ct is the best technique to evaluate cortical bone ; nonetheless , it cannot be used to distinguish normal from pathological bone marrow unless a significant amount of trabecular bone is involved [ 12 ]  . 
similarly , nuclear medicine studies are not always sensitive in differentiating normal from pathological bone marrow nor do they have optimal anatomical resolution [ 12 ]  . mri is the only diagnostic imaging modality able to distinguish red marrow from yellow marrow without the use of contrast medium in the anatomical sites they occupy based on the different tissue composition and therefore to detect not only changes of pathological bone marrow ( metastases , haematological malignant tumours , infiltrating disorders such as granulomatous diseases and polycythaemia vera ) [ 1315 ] but also the process of marrow reconversion . 
proton density images contribute little to bone marrow imaging because there is very little difference in proton densities of the various tissues [ 16 ]  . fat has a short t2 relaxation time and shows a decrease in signal intensity on t2 - weighted images compared with water ; therefore , red marrow has a slightly greater hyperintensity compared with yellow marrow [ 16 ] ; however , yellow marrow is not easily distinguishable from red marrow on t2weighted sequences [ 10 ]  . these sequences are more useful for distinguishing bone marrow lesions from normal bone marrow as they have a significantly longer t2 . 
the small differences in signal intensity are virtually eliminated in fse [ turbo spin echo ( tse ) ] sequences , which present a natural increase in the fat - tissue signal . therefore , when a bone marrow disease is suspected , it is advisable to associate additional fat saturation techniques with these sequences [ 17 ]  . 
fat has a short t1 relaxation time and is hyperintense on t1 - weighted images ; yellow marrow also appears hyperintense , with a signal intensity similar to that of subcutaneous fat . 
quando c una richiesta di aumento dellemopoiesi per stress , anemia cronica , scompenso cardiaco , estesa sostituzione midollare [ 10 ] , si innesca un processo di riconversione da midollo giallo in midollo rosso , che progredisce in senso inverso a quello di conversione ; esso pu avvenire in forma diffusa o con la comparsa di aree focali di midollo rosso su uno sfondo di midollo giallo [ 11 ]  . la radiologia tradizionale ( rt ) e la tomografia computerizzata ( tc ) , pur possedendo sensibilit diverse per lo studio delle alterazioni del tessuto osseo compatto e spongioso , sono entrambe insensibili nella dimostrazione delle diverse qualit di midollo osseo e possono essere indicative di una patologia solo indirettamente , allorch si producono ripercussioni sulla composizione del tessuto osseo . 
anche la tc , pur essendo la tecnica migliore per lo studio della corticale ossea , non pu essere impiegata per distinguere midollo osseo normale o patologico finch non sia coinvolta una significativa quantit di osso trabecolare [ 12 ]  . 
anche gli studi medico - nucleari , non sono sempre sensibili a differenziare midollo osseo normale e patologico e comunque non hanno una ottimale risoluzione anatomica [ 12 ]  . tra le metodiche di diagnostica per immagini , la rm lunica in grado di riconoscere , in virt della diversa composizione tissutale , il midollo rosso ed il midollo giallo e di visualizzali , senza necessit di mezzo di contrasto , nelle sedi anatomiche in cui si trovano e quindi di riconoscere non solo le alterazioni del midollo osseo patologico ( metastasi , tumori maligni ematologici , processi infiltrativi come la malattie granulomatose , e la policitemia vera ) [ 1315 ] ma anche i fenomeni di riconversione midollare . 
le immagini in densit protonica contribuiscono poco allimaging del midollo osseo poich la densit protonica dei vari tipi di tessuto differisce poco [ 16 ]  . nelle immagini t2 - dipendenti il grasso ( che ha un breve tempo di rilassamento t2 ) presenta un segnale ridotto rispetto allacqua ( che ha un elevato tempo di rilassamento t2 ) : pertanto il midollo rosso presenta rispetto al midollo giallo una lieve maggiore iperintensit [ 16 ] ; tuttavia il midollo giallo non facilmente distinguibile nelle sequenze t2dipendenti dal midollo rosso [ 10 ]  . 
in people older than 50 years of age , women have slightly longer t1 and t2 relaxation times in the vertebral bodies compared with men , apparently due to a faster and more extensive process of bone demineralisation associated with menopause [ 18 ]  . 
infiltrative diseases of the bone marrow , and more frequently haematological malignancies , manifest with three different patterns of signal alterations : localised areas of abnormal bone marrow , diffuse pattern and variegated pattern [ 16 ]  . 
the diffuse pattern , in which bone marrow is completely replaced by the pathological process ( typical of acute leukaemia ) , lends itself best to a differential diagnosis with bone marrow reconversion . 
t1 images show a diffuse decrease in signal , which can be very difficult to distinguish from red bone marrow , especially in young adults . on the other hand , t2 signal intensity may be difficult to detect , as there is no depiction of normal bone marrow for comparison ; these cases may be solved by using contrast medium , as abnormal bone marrow will enhance [ 19 ] whereas enhancement of normal bone marrow is barely perceptible . 
we therefore believe that evaluation of bone marrow status should be a further clinical parameter for better staging of osas , in addition to those already reported in the literature . 
however , knowledge of temporal physiological evolution and distribution of bone marrow is necessary for correct interpretation of normal or abnormal bone marrow pattern on mri . factors thought to affect bone marrow conversion include changes in local temperature , blood supply and oxygen tension [ 11 ]  . 
in adults , bone marrow reconversion occurs as a consequence of prolonged physiological stress or when the bone marrow is not able to satisfy the demand for additional haematopoiesis [ 11 , 15 ]  . 
the known ones include chronic anaemia ( falciform anaemia , thalassaemia , thrombotic thrombocytopenic purpura ) , polycythaemia , cardiac decompensation and anaemia complicating chemotherapy or radiotherapy [ 11 , 20 ]  . 
the distinction between normal and abnormal heterogeneous signals , evaluated on the clivus only , may be problematic : studies in the adult have demonstrated that the inhomogeneous pattern was present in more than a third of healthy individuals , with a pattern similar to that of patients with haematological diseases [ 12 ]  . 
however , other studies have shown that normal signal hyperintensity is utili per distinguere le lesioni patologiche midollari dal midollo normale , avendo un t2 significativamente pi lungo . le piccole differenze di segnale sono peraltro pressoch annullate quando si utilizzano sequenze fse ( tse ) che presentano naturale incremento del segnale del tessuto adiposo . pertanto nel sospetto di patologia midollare opportuno associare a tali sequenze impulsi aggiuntivi per la saturazione del grasso [ 17 ]  . nelle immagini t1 - dipendenti il grasso ( che ha un breve tempo di rilassamento t1 ) iperintenso e cos appare il midollo giallo , che presenta intensit di segnale vicina a quella del grasso sottocutaneo . 
lacqua ( che ha un lungo tempo di rilassamento t1 ) ipointensa ed il midollo rosso , che ha una percentuale di acqua superiore al midollo giallo , appare con intensit di segnale uguale o lievemente pi alta rispetto a quella dei muscoli . 
in soggetti di et superiore ai 50 anni , le donne hanno tempi di rilassamento t1 e t2 lievemente maggiori nei loro corpi vertebrali rispetto agli uomini : ci sarebbe dovuto ad un pi rapido ed esteso processo di demineralizzazione ossea associato alla menopausa [ 18 ]  . le malattie infiltrative del midollo osseo , e pi frequentemente le neoplasie maligne ematologiche si manifestano con alterazioni di segnale con tre pattern diversi : aree localizzate di midollo anormale , pattern diffuso e pattern variegato [ 16 ] : il pattern diffuso in cui il midollo osseo completamente rimpiazzato dal processo patologico ( tipico della leucemia acuta ) quello che maggiormente si presta ad una diagnosi differenziale con la riconversione midollare : in t1 c un diffuso decremento del segnale e , soprattutto nei giovani adulti , tale aspetto pu essere difficile da distinguere dal midollo rosso . daltra parte lintensit di segnale in t2 pu essere difficile da apprezzare perch manca la rappresentazione del midollo osseo normale per confronto ; in tali casi luso del mezzo di contrasto pu essere talvolta risolutivo per lenhancement che coinvolge il midollo osseo anormale [ 19 ] , essendo invece lenhancement del normale midollo osseo difficilmente percepibile . nello studio che noi eseguiamo per la valutazione rm delle apnee ostruttive del sonno compresa una sequenza sagittale se t1 - pesata che comprende , oltre alle prime vie aeree , il clivus e parte dei metameri ossei del tratto rachideo cervicale ; abbiamo ritenuto pertanto che la valutazione dello stato del midollo osseo debba essere un ulteriore parametro da riferire al clinico per una pi completa stadiazione dellosas , in aggiunta a quelli gi codificati in letteratura . tuttavia , per un corretto giudizio sulla normalit o anormalit di un determinato pattern midollare in rm necessaria la conoscenza della fisiologica evoluzione temporale e distribuzione del midollo osseo . gi conosciuto da tempo che tra i fattori che si pensa influenzino la conversione midollare si includono variazioni della temperatura locale , rifornimento vascolare e tensione di ossigeno [ 11 ]  . 
negli adulti la riconversione midollare avviene per prolungati stress fisiologici o allorch la richiesta di ematopoiesi eccede la capacit del midollo a venire incontro alla domanda [ 11 , 15 ]  . tale stress fisiologico pu essere causato da molte condit . 
quelle note e descritte in letteratura includono : anemie croniche ( anemia falciforme , talassemia , porpora trombotica trombocitopenica ) , policitemia , scompenso cardiaco , anemia complicante chemio o radioterapia [ 11 , 20 ]  . 
la distinzione tra segnale eterogeneo normale ed anormale valutata solo sul clivus pu essere problematica : nelladulto alcuni studi hanno dimostrato che il pattern disomogeneo era presente in pi di un terzo degli individui sani , con un pattern simile a quella dei soggetti con malattie ematologiche [ 12 ]  . 
altri studi hanno per dimostrato come dopo i 24 anni si raggiunge nel 95% dei casi una normale iperintensit di segnale [ 25 ]  . si concorda in genere nel considerare che un basso segnale omogeneo in un adulto suggerisce la presenza di unanormalit [ 20 , 25 , 26 ]  . 
bisogna sottolineare comunque che nel rachide cervicale , fino ai 40 anni il pattern pi frequente quello caratterizzato da omogenea distribuzione di midollo rosso , nella quinta decade di tipo transizionale ( con aree di midollo giallo parallele alle vene basivertebrali o a livello degli spigoli vertebrali ) , mentre nella maggior parte dei soggetti oltre i 50 anni vi una pi omogenea conversione midollare [ 27 ]  . conclusioni non stata ancora a nostra conoscenza segnalata in letteratura la possibilit che losas determini delle modificazioni del midollo osseo . 
a 26 - year - old patient with obstructive sleep apnoea syndrome ( osas ) showing areas of hypointensity in the clivus ascribable to the presence of red bone marrow . 
tale aspetto riferibile allomogenea distribuzione di midollo emopoietico . reached in 95% of cases after 24 years of age [ 25 ]  . it is generally agreed that a low homogeneous signal in an adult is suggestive of an abnormality [ 20 , 25 , 26 ]  . 
it should , however , be noted that the most frequent pattern in the cervical spine up to the age of 40 is characterised by homogeneous distribution of red marrow . in the fifth decade , it is transitional ( with areas of yellow marrow parallel to the basivertebral veins or at the level of vertebral edges ) whereas in most patients over 50 years of age , marrow conversion is more homogeneous [ 27 ]  . conclusions to our knowledge , no previous study has reported the possibility that osas may induce bone marrow changes . 
in contrast , mri detection of signs of bone marrow reconversion during examinations performed for other reasons , which include bone components mainly of the axial skeleton in the field of view , might suggest osas in addition to the known causes of bone marrow reconversion , especially when there are no clinical or laboratory findings of haematological disease . 
surgical pathologies were pnet ( n 42 ) , microcystic serous cystadenomas ( m - scn , n 12 ) and solid pseudopapillary epithelial neoplasms ( spen , n 20 )  . 
using a combination of morphological patterns and enhancement features , pnet was identified with 88% sensitivity and 81% specificity , m - scn was identified with 83% sensitivity and 94% specificity , and spen was identified with 90% sensitivity * hua - dan xue bjdanna95@hotmail.com 1 department of radiology , peking union medical college hospital , shuaifuyuan no . 
pnet could be differentiated from its mimics with high accuracy . keywords pancreatic neoplasms multidetector computed tomography ca19 - 9 diagnosis introduction multidetector ct ( mdct ) of the abdomen has been widely used for the evaluation and characterization of focal pancreatic lesions [ 13 ]  . 
nevertheless , the 1 3 338 radiol med ( 2017 ) 122 : 337344 cystic nature of microcystic serous cystadenoma ( m - scn ) could not always be well appreciated , as they often have a hypervascular solid - dominant appearance , which could be mistaken for more malignant solid tumours [ 10 , 1316 ]  . 
surgeries could be avoided if the benign nature of the lesion is confidently diagnosed based on radiological findings . therefore , the aim of this study is to investigate mdct features of enhancing pancreatic mass with normal serum ca19 - 9 level , and to determine key features that characterize pnet from its mimics . materials and methods patients this retrospective study was approved by the institutional review board , and written informed consent was waived . 
patients were recruited in this study based on the following inclusion criteria : patient received pre - treatment multiphase mdct and demonstrated pancreatic lesion with enhancement ; patient had blood tumour biomarker test within one month of mdct imaging , and serum ca19 - 9 level was within normal range ; patient received pancreatic surgery at our institution . exclusion criteria were enhancing pancreatic mass with a histological diagnosis different from pnet , m - scn and spen ( n 6 , including two focal autoimmune pancreatitis , two pancreatic acinar cell carcinoma , one pancreatic lymphoma and one pancreatic squamous cell carcinoma ) ; patients with known familial history of von hippellindau syndrome ( vhl , n 1 ) and multiple endocrine neoplasia syndrome type 1 ( men1 , n 5 )  . 
the mean time interval between mdct and pancreatic surgery was 17 days ( range 171 days )  . imaging technique ct examinations were performed on 128 - detector ct scanners ( siemens somatom definition flash , siemens healthcare , forchheim , germany )  . 
the scanning parameters were as follows : tube voltage , 120 kvp ; effective amperage settings , 150 mas ; gantry rotation time , 0.5 s ; table increment , 46.8 mm per rotation ; matrix 512 512 . 
thin slice images with 1.0 mm section thickness / 1.0 mm interval were also reconstructed for post - processing purposes . non - ionic contrast media ( ultravist , 370 mg of iodine per milliliter , schering , berlin , germany ) were injected with 1.5 ml per kilogram of body weight , at a rate of 3.0 ml / s using an automatic power injector . 
the equilibrium phase ( ep ) was initiated 90 s after the pap phase . 1 3 radiol med ( 2017 ) 122 : 337344 image analysis mdct images were independently evaluated by two radiologists ( 13 and 12 years experience in interpreting abdominal ct / mr , respectively ) on the picture archiving and communication system ( pacs , centricity , ge )  . 
 both readers were blinded to the surgical and pathological information . the location of the lesion ( head , body or tail of the pancreas ) was documented and lesion size measured . 
secondary changes of the pancreas due to tumour compression were also recorded , including upstream dilatation of the main pancreatic duct and side branches , and distal pancreatic parenchymal atrophy . 
honeycomb pattern was characterized by multiple small chambers of hypoor non - enhancing area , separated by hyper - enhancing fine septumelting icecream pattern denoted lesion with inhomogeneous faint enhancement and partial non - enhancing area within the tumour which melts away from the solid enhancing part . 
lesion - parenchyma attenuation difference was compared in each phase , and lesions were classified into hypo - attenuating in all phases or hyper - attenuating in one or more phases . 
inter - observer agreement of the ct features was determined by calculating kappa values ( 0.210.40 , fair agreement ; 0.410.60 , moderate ; 0.610.80 , good ; 0.811.00 , excellent agreement )  . 
melting icecream pattern ( c ) was characterized by partial non - enhancing area which melts away with the solid - appearing enhancing part of the tumour results mdct findings for each disease entity were summarized in table 2 . 
on the contrary , lesion location , size , calcification and secondary changes to the pancreas ( upstream pancreatic duct dilatation and distal parenchyma atrophy ) were not significantly different for these three pathologies . 
an enhancing mass was seen in the pancreatic head ( arrow ) , which enhanced avidly in pancreatic arterial phase ( pap , a ) , with multiple small chambers of non - enhancing area . 
the honeycomb morphological pattern was better appreciated on later phase ( b ) , as the condense septa within the tumour enhanced less intensely and the microcysts remains non - enhancing . 
using a combination of morphological pattern and one enhancement feature ( enhancement peak of the lesion or lesion - parenchyma contrast ) , pnet could be differentiated from the other lesions with 88% sensitivity and 78% specificity . 
m - scn could be identified with 83% sensitivity and 94% specificity , and spen could be identified with 90% sensitivity and 91% specificity . 1 3 radiol med ( 2017 ) 122 : 337344 in young women ; however , a trend towards decreasing tumour size was noted , as the accessibility of cross - sectional imaging is increasing and more incidental tumours are detected at earlier stage [ 9 ]  . 
although spen was known to have predilection in female patients of younger age , it is noted that in our patient cohort , male patients and older patients were also encountered , adding to the difficulty of characterization . 
 awareness of the key ct features of the above - mentioned pathologies is mandatory , since pancreatic surgeries are associated with substantial risk of morbidity and should only be performed for overt or latent malignant lesions . 
 a thorough understanding of the ct findings is helpful to avoid incorrect or inconclusive mdct diagnosis , which leads to unnecessary surgeries or additional diagnostic procedures , with increased cost and invasiveness to the patient . in our study , a combination of morphological patterns and enhancement features improves diagnostic accuracy for lesion characterization , and the inter - observer agreement for these ct findings was good to excellent . 
this result suggested that pnet could be well characterized from its mimics using key mdct features . to evaluate the key features leading to a correct diagnosis , we focused on the morphological patterns of the lesions , calcification and secondary change of the pancreas . 
cells near the vessel remain intact , whereas cells distant from the vessel underwent degenerative change , which gave its typical look of solid friable tumour , and its melting icecream pattern , as reflected in this study [ 20 ]  . 
surgical pathology confirmed solid pseudopapillary epithelial neoplasm discussion when an enhancing pancreatic mass is detected and patient has normal ca19 - 9 level , characterization of the lesion becomes an important issue . 
the frequency ofpresence of calcification , and the morphology of calcification were not significantly different among thesethree pathologies , and thus not key features for lesion characterization . enhancement patterns of the lesions were also investigated . 
in our study of 20 spen , 2 were less than 3 cm and 8 were less than 4 c progressive filling - in pattern was observed in most spen , which is in accordance with their study . 
 it has been suggested that the imaging features of spen differ between male and female gender , and male patients tend to have larger tumours with more solid component , and a lobulated margin [ 23 ]  . 
 awareness of key mdct features for lesion characterization is mandatory for clinical decision - making . in conclusion , morphological features and enhancement patterns on mdct are key features for characterizing enhancing pancreatic mass with normal serum ca199 . 
 the purpose of this article is to suggest a flow - chart to evaluate the placement of uvc , testing it in young radiologists - in - training . method we developed a simple flow - chart to asses , steps by step , uvc placement considering its course and tip location ( ideally placed in the atriocaval junction )  . 
we tested the flow - chart impact asking to 20 residents to evaluate the placement of 10 uvc before and after they familiarized with the flow - chart and the anatomical findings of a newborn . 
dalessandro , university of palermo , palermo , italy keywords flow - chart frontal radiogram radiology resident umbilical venous catheter introduction since the introduction of intravascular catheters and the use of the umbilical vein for exchange transfusions , umbilical venous catheters ( uvc ) have been routinely used in premature infants to administer parenteral alimentation or antibiotics ( according to the different pathological conditions ) [ 1 ]  . they can be easily detected on frontal abdominal radiograms , indeed normally uvc enters on the anterior abdominal wall at umbilicus , and predominantly follow an anterior and cephalad course ( following the left umbilical vein course )  . 
the wilcoxon matched - pairs sign rank test was used to assess if the number of correct characterizations of uvc position was significantly different before and after the administration of the flow - chart . 
 then , we splitted the data according to the different residency years . the chi - square test was calculated to assess the homogeneity of the evaluations of uvc placement executed by the 20 radiology residents before and after the 1 3 radiol med ( 2017 ) 122 : 386391 388 fig . 
d3 3rd dorsal vertebra ; d4 4th dorsal vertebra ; d5 5th dorsal vertebra ; d9 9th dorsal vertebra ; d10 10th dorsal vertebra ; d12 12th dorsal vertebra ; ivc inferior vena cava ; la left atrium ; l2 2nd lumbar vertebra ; l3 3rd lumbar vertebra ; pv pulmonary vein ; ra right atrium ; svc superior vena cava ; uvc umbilical venous catheter their simplicity makes them useful tools for communicating how processes work and provide key - points in a simple and concise manner . 
 it could be used to define and analyze processes , communicate steps to other people involved in a process , standardize a process , improve a process , identify bottlenecks or troubleshoot a proble moreover , drawing a flow diagram , you can zoom in each individual stage , without feeling overwhelmed by the rest of the process [ 913 ]  . some academic programs and many individual faculty members have tried applying techniques to facilitate learning in their work . 
furthermore , joint commission and important medical societies , proposed flow - charts and other support decision tools for a simple understanding of surgical procedures , management of several diseases or 1 3 radiol med ( 2017 ) 122 : 386391 fig . 
3 fetal circulation anatomy table shown to residents to identify critical points of vulnerability in hospital organization , with excellent results [ 1416 ]  . some authors proposed diagnostic flow - charts for the evaluation and management of different pathologies [ 17 , 18 ] ; for example , colombi et al . 
 [ 17 ] offered a flow - chart with the attempt to support the less experienced clinician in stringently recognizing joint hypermobility syndrome / ehlers - danlos syndrome hypermobility type ; polsfuss et al . 
the ductus venosus is 12 cm long and ends in the left or middle hepatic vein , very close to the junction with the inferior vena cava [ 19 , 20 ]  . as previously described , when a uvc is inserted , it follows the path of the umbilical vein , and in a standard frontal abdomen radiogram , it is placed on the right of lumbar spinous processes ( lumbar vertebrae l3l4 ) , it courses posteriorly through the liver ( closely to the dorsal vertebrae d10d12 ) to the left portal vein and then to ductus venosus and ivc ( d9 level ) fig . 
other recent paper suggest a simple method to assess the precise position of uvc using morphometric measurement of the new born before placement ; however , this method do not avoid misplacement that could be only assessed in plain film [ 21 ]  . our flow - chart summarizes these key - points to evaluate uvc placement , in particular it describes its course and tip location . 
according to the standard / normal position of the uvc using that is possible to judge a correct positioning of the uvc . the students have considered the flow - chart simple and easy to understand . 
according to our results , the number of correct characterizations of uvc position was significantly different after the administrations of the simplified flow - chart : indeed on a first evaluation there were only 106 / 200 ( 53% ) correct assessments of correct or uncorrect positioning of the uvcs evaluated , this number switched to 196 / 200 ( 98% ) correct assessments after the administration of the flow - chart . this result does not surprise , considering the limited experience of younger students ; otherwise they are usually more familiar to support decision tools . 
we have not found significant difference in determination of correct and malposition of uvc in all residents , with similar performance independently from the residents year course ; so the real difference in performance was determined by the use of the flow chart as observed among the twenty radiology residents . however , after the evaluation of flow - chart , there were significant performance improvement both in first year course and successive year courses residents , and the difference was statistically significant . 
hence , the flow - chart improved the results in all students and it could be considered to prove that the flow - charts can became useful tools for teaching improvement programs . 
so , in our case , flow - chart improved the results in the whole sample , becoming an useful tool to teach residents to easily understand the correct placement of uvc . this algorithm is accurate , simple , easy to use , inexpensive , and therefore , applicable in the standard routine radiological evaluation . 
obviously , these techniques are tools that complete and help an extensive study , that of course , cannot be replaced only by flow - chart . the flow - chart could became an useful tool to accompany the daily reporting of the radiologist , especially on issues to them lesser known . compliance with ethical standards funding none . conflict of interest all authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . ethical standards this article does not contain any studies with animals performed by any of the authors . 
from september 2011 to october 2014 , 102 patients who had undergone 1.5 tesla mra of the shoulder , including conventional 2d - fse and iw - 3d and hy - 3d images were included in our study . 
supraspinatus tendon ( sst ) , infraspinatus tendon ( ist ) and subscapularis tendon ( sct ) tears , as well as antero - inferior , superior and posterior labral lesions were assessed , using surgery as the reference standard . 
the sensitivity , specificity , positive predictive values ( ppv ) , negative predictive values ( npv ) and accuracy ( acc ) for all types of rotator cuff tears and labral lesions were calculated . 
used a 3d isotropic t1 - weighted fast spin echo ( fse ) with 6 min acquisition time to study 49 patients who had undergone direct or indirect shoulder mra , evaluating both rc and labral lesions . 
in this paper , using a 6 min 38 s axial 3d dataset ; sensitivity , specificity , and inter - observer reliability were similar to conventional 2d mr arthrography for evaluation of the acetabular labrum [ 15 ]  . 
iw sequence is characterized by good spatial and contrast resolution on both tendons and glenoid labrum ; moreover , double - echo steady - state sequence may allow a further reduction in imaging time . the purpose of this study was to compare the diagnostic accuracy of isotropic 3d intermediate - weighted fse ( iw3d ) and hybrid double - echo steady - state t1 - weighted ( hy3d ) sequences and the conventional two - dimensional fse sequences ( 2d - fse ) in the evaluation of rotator cuff ( rc ) radiol med ( 2017 ) 122 : 353360 and glenoid labrum tears at shoulder mra , using surgical results as the reference standard . patients and methods patient population institutional review board approval was obtained and informed consent was waived for this retrospective study . 
 from september 2011 to october 2014 , 124 patients who had shoulder mra , including conventional 2d - fse , iw - 3d and hy - 3d images , and who subsequently had surgery , were considered for inclusion in our study . 
exclusion criteria included previous shoulder surgery ( n 14 ) , insufficient articular cavity distension ( n 2 ) , insufficient quality of datasets analyzed ( n 6 )  . 
hy - 3d images were obtained using a double - echo steady - state sequence increasing the t2 - weighting of fast imaging with steady - state precession ( fisp ) images , allowing improved delineation of fat , joint fluid , and cartilage . 
a score of 02 was considered negative , and a score of 34 was deemed positive . image analysis images were retrospectively and independently reviewed by two experienced radiologists ( gf , lr ; 11 and 21 years of experience in musculoskeletal radiology , respectively ) blinded to clinical and surgical data . 
to reduce recall bias , the datasets were analyzed separately , in three different reading sessions : 2d images were reviewed first ; iw - 3d and hy - 3d datasets were analyzed during the second ( 4 weeks delay ) and third ( 8 weeks delay ) reading sessions , respectively . 
supraspinatus tendon ( sst ) , infraspinatus tendon ( ist ) and subscapularis tendon ( sct ) tears , as well as antero - inferior , superior and posterior labral lesions were assessed . 
intra - substance tears were not included in our analysis because they could not be correlated with surgical results [ 13 ]  . diagnosis of a full - thickness tear was based on the presence of a complete defect from the articular to the bursal surface with or without retraction of the tendon . 
a partialthickness tear was represented by the visualization of a partial defect of tendon fibers along the articular or bursal surface [ 17 ]  . labral partial - thickness tears were represented by the visualization of a partial defect of the labrum , enhanced by the passage of contrast material , or by the presence of abnormal morphology or partial dislocation . 
an arthroscopic approach was adopted in 98 patients , whereas in four cases an open approach was needed for repairing large glenoid bone fracture following anterior dislocation . statistical analysis the distribution of continuous variables was reported as mean and range ( minimum to maximum values )  . 
each readers performance in assessing rotator cuff and labrum abnormalities was evaluated using the area under the receiver operating characteristic curve ( auc ) and 95% confidence intervals ( cis )  . 
the sensitivity , specificity , positive predictive values ( ppv ) , negative predictive values ( npv ) and accuracy ( acc ) for all types of rotator cuff tears and labral lesions were calculated . 
1 34 - year - old man with shoulder pa a t1 - weighted coronal 2d mr image ; b hy - 3d 1 - mm reformatted image on coronal plane ; c iw - 3d 1 - mm reformatted image on coronal plane . 
four fn were pointed out by reader 1 using 2d images , with six fn and eight fn at iw and hy - 3d images ; also , an increase in fn rate was obtained by reader 2 using 2d ( six fn ) , iw ( seven fn ) and hy - 3d images ( 11 fn )  . among 68 lesions of glenoid labrum , four fp were pointed out by reader 1 using 2d images , with three fp at iw and hy - 3d images , respectively ; reader 2 pointed out three fp at 2d and hy - 3d and four fp at iw - 3d sequences , respectively ; four fn were pointed out by reader 1 using 2d and hy - 3d images , with only three fn at iw images ; six fn were pointed out by reader 2 using 2d and iw - 3d , with eight fn at hy - 3d images , respectively . 1 3 radiol med ( 2017 ) 122 : 353360 fig . 
a t1 - weighted axial 2d mr image ; b hy - 3d 1 - mm reformatted image on axial plane ; c iw - 3d 2 - mm reformatted image on coronal plane . 
antero - inferior labral tear ( arrow ) can be depicted on axial images ; the presence of irregular glenoid bone ( arrow ) , with labral tear extending antero - superiorly ( short arrow ) , can be demonstrated on 1 - mm coronal reformatted iw - 3d image . 
3 17 - year - old woman with shoulder pa a t1 - weighted axial 2d mr image ; b hy - 3d 2 - mm reformatted image on axial plane ; c iw - 3d 2 - mm reformatted image on axial plane . 
although conventional 2d fse images are characterized by high contrast resolution , multiple sequences on different planes are needed to cover all anatomic structures of the shoulder : our 2d imaging protocol , including t1 - weighted , pd and t2 - weighted fat saturated images on multiple planes , takes on average 20 mmoreover , the possibility to miss tiny lesions because of thick slices and small gaps between slices or , because of partial volume averaging have been described [ 20 , 21 ]  . 
previously introduced high - performance mr gradients allowed the radiologists to optimize 3d imaging for the evaluation of the musculoskeletal system , without a significant increase of scanning times [ 712 ]  . 
among rc partial - thickness tears , two fn cases were correlated to the presence of tiny bursal surface sst tears , which were missed using 2d and 3d images . 
a possible explanation is that hy - 3d dataset is characterized by an intrinsic low contrast in depicting tendons , so that tears are well visualized when the articular cavity is adequately distended with contrast material . 
iw - 3d allowed us to obtain the highest sensitivity in identifying labral tears for reader 1 ( 95.6% ) ; a small defect of posterior labrum was missed at 2d and hy - 3d , but identified at iw - 3d . 
as regards labral defects , fn findings were correlated with tiny labral tears considered as large sub - labral recess ( n 2 ) or not adequately opacified with contrast material ( n 1 ) for each image dataset . 
hy - 3d images and iw - 3d allowed us to better evaluate bony lesions frequently associated to labral disorders in case of 1 3 radiol med ( 2017 ) 122 : 353360 anterior shoulder dislocation [ 22 ] ; these datasets allowed us to correctly image all bony bankart lesions , diagnosed in eight patients enrolled , but missed using 2d images in three cases . 
conversely , accurate values for reader 2 were higher in evaluating rc lesions ( 92.2% for iw - 3d dataset and 88.2% for hy - 3d dataset , respectively ) , without any difference as regards the evaluation of labral tears ( 90% of accuracy using both sequences )  . 
although the acquisition time of iw - pd dataset is longer than a single sequence in the 2d series ( 6 min vs 3 or 4 min on average ) , motion artifacts were limited , thanks to optimized position of the patient within gantry . 
our data showed this sequence could be used instead of pd and / or t1 - weighted sequences on multiple planes both in case rc or labral lesions are suspected : as previously reported in the study of park et al . 
 [ 15 ] , it may be more difficult to detect increased water content within edematous bone marrow when compared with the highly fluid - sensitive fat - suppressed t2 - weighted fse sequences because of potential weakness of the iw tissue contrast . 
for these reasons , we believe coronal t2 - weighted fs sequence is still necessary to adequately assess bone marrow edema ; a fast 10 min protocol , including iw - 3d and cor t2 fs is now under evaluation at our institution in clinical practice . this study had some limitations . 
second , other imaging findings , including bony bankart and hillsachs lesions and articular cartilage defects were not considered in our statistical analysis , even though they were relatively uncommon in our study population . 
furthermore , the surgeons were aware of mri findings . in conclusion , at 1.5 tesla shoulder mra , the accuracy of iw - 3d and hy - 3d images was not significantly higher than the 2d sequences in diagnosing rc and labral abnormalities . 
while iw sequence may have the potential to substitute conventional 2d sequences for diagnosing rotator cuff and labral tears , hy - 3d images could be considered an additional tool for evaluating tiny labral lesions suspected on the basis of clinical findings or on the basis of 2d imaging . compliance with ethical standards conflict of interest the scientific guarantor , corresponding author of this publication is giovanni foti . 
also , none of the study subjects or cohorts has been previously published . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent since this was a retrospective study , formal consent was not required . 
age , dose , treatment time , and adc values were compared between the two groups ( group 1 : local control ; group 2 : relapse / persistence of disease ) using the student t test two - tailed unpaired . 
 moreover , the identification of non - responder patients , in the pre - treatment staging or the early phases of treatment , could permit the change of the therapeutic regimen or improve the selection for surgery as further treatment . the radiological evaluation by pet - ct or magnetic resonance ( mr ) in the early post - treatment period is often suboptimal due to the presence of false positives . 
therefore , it would be advantageous to find an imaging marker that predicts response to treatment or identifies possible tumor residues during the early post - treatment period . the clinical use of imaging techniques , such as petct or mr with diffusion weighted sequences , to predict the response in head - and - neck cancer patients treated with chemotherapy is still unprecedented . 
several studies showed the role of standardized uptake value ( suv ) of pre - treatment pet as a prognostic factor in non - smallcell lung carcinomas ( nsclc ) and in cervical cancers [ 2 , 3 ]  . 
 other authors demonstrated that the suv value calculated on lymph nodes is a predictor of disease - free survival [ 5 ]  . the apparent diffusion coefficient ( adc ) was proposed as a marker of the early response for brain , breast , and cervix tumors [ 68 ]  . 
the accuracy of pre - treatment adc in predicting an early response in patients with head - and - neck tumors was never reported , while some studies demonstrated that pre - treatment adc could be used as a potential marker in predicting locoregional recurrences : other studies did not identify any association [ 9 ]  . the goal of this study was to evaluate the prognostic and predictive role of pretreatment adc in patients with head and neck cancer under radiotherapy and chemotherapy . materials and methods patients and variables radiol med ( 2017 ) 122 : 345352 chemotherapy in our radiotherapy department between february 2010 and june 2014 . 
out of the 57 patients , three were excluded due to the small size of the primary tumor that hindered the accurate evaluation of the adc values , and seven were excluded due to the poor quality of the diffusion - weighted images ( dwi )  . 
therefore , the study included 47 patients , whose primary tumor site was in the nasopharynx ( 23 ) , oropharynx ( 19 ) , and hypopharynx ( 5 )  . all patients received radiotherapy with a conformational external beam radiation , with a daily fractionation dose of 1.82.0 gy for 5 days a week and a total dose at the gross tumor volume ( gtv ) varying between 54 and 74 gy . of the 47 patients , 39 received a concomitant chemoradiotherapy , while eight patients also had neoadjuvant chemotherapy . 
the follow - up was based on both clinical and radiological evaluations : 33 patients showed a local control of the disease , 6 patients a persistence of the disease after the treatment , and 8 patients subsequently had a histologically confirmed local recurrence . 
the followup time varied between 3 and 20 months for the patients with local recurrence or persistence and between 10 and 36 months for the patients with local control of the disease . the demographic , clinical , and radiological variables analyzed in the study are shown in table 1 . informed consent was obtained from all participants . 
 as the study was retrospective , approval of the local ethics committee was not sought . magnetic resonance the pre - treatment mr was performed on a 1.5 tesla scanner ( achieva , philips medical system , best , holland ) with 33 mt / m gradient , using a 16 - channel head - and - neck coil . 
all patients received radioand ( 1 ) a manual roi ( roi 1 ) obtained by manually drawing a roi along the lesion contours on the adc map , table 2 mri sequences and parameters sequence weighted tse t2 fov ( mm ) thickness ( mm ) gap ( mm ) matrix tr ( ms ) te ( ms ) weighted tfe t1 with contrast agent ( thrive ) 280 x 280 x 157 none 400 x 400 250 x 195 x 199 256 x 157 3805 124 x 125 5103 diffusion - weighted epi 250 x 250 x 220 1 3 radiol med ( 2017 ) 122 : 345352 fig . 
for each roi , the mean , minimum , and maximum adc values were calculated . all statistical calculations were performed with the medcalc software version 15.2.2 ( medcalc software bvba , ostend , belgium ) and the p - values were considered statistically significant if less than 0.05. age , dose , treatment time , and adc value were compared between the two groups ( group 1 : local control ; group 2 : disease recurrence / persistence ) using the two - tailed , unpaired students t test . 
2 mr images of squamous cell carcinoma of hypopharynx : tse t2 weighted sequences in the axial plane ( a ) ; post - contrast tfe t1 sequence adc maps with the histogram of the adc values obtained from the rois ( b ) roi 1 ( c ) , roi 2 ( d ) the intra - observer agreement on rois positioning and drawing was assessed by mean of cohens k statistics . 
comparison of the minimum adc 2 values between the two groups ( group 1 local control ; group 2 relapse / persistence of disease ) 1 3 350 radiol med ( 2017 ) 122 : 345352 with loco - regional control , but only modifications of the adc value during therapy have a significant correlation . in our work , the role of adc was evaluated as a predictive factor of response to chemo - radiotherapy in headand - neck sccs . 
therefore , a correlation between t staging and therapy response was observed . in this study , the dose of the radiotherapy was the only clinical variable statistically different between the two groups . 
it has to be considered , however , that the patients who received a lower dose did not reach the prescribed dose due to complications or worsening of the clinical condition during the treatment . furthermore , hatakenaka et al.s study [ 11 ] showed a correlation between the adc value of the primary tumor and the response to chemo - radiotherapy : patients with recurrence had pre - treatment adc values higher 3 vs . 
several factors can explain these discrepancies , such as the histological heterogeneity of the headand - neck tumors , sample numbers , and different treatment protocols [ 10 ]  . 
the decrease of the adc value was connected to tumor regrowth , and this is supported by studies in animals showing that adc reduction is caused by repopulation of tumor cells [ 15 , 16 ]  . 
more studies are needed to determine the optimal number and timing of the serial evaluations with adc to detect the onset of resistance to therapy . conclusions in our study , the pre - treatment adc value in patients with local control of the disease is lower than that of patients with disease persistence or recurrence . 
since a negative correlation between adc and cell density was reported [ 17 ] , it looks as if the tumor vital cells with active proliferation and low adc respond better to chemo - radiotherapy as compared to tumors with low cell density and high adc , probably due to the presence of necrotic areas . 
this hypothesis is supported by diffusion and perfusion studies [ 18 , 19 ] that showed that the regions with contrast - enhancement of high - grade gliomas have larger blood volume and smaller adc value as compared to low - grade gliomas . this study has some limitations . 
the first one is the low number of patients with persistent or recurrent disease , as compared to the number of patients with local control . the evaluation of the adc value of the primary tumor could not always be accurate . 
moreover , the interface air - tissue increases the susceptibility of the diffusion - weighted sequence to artifacts . another limitation is that it was not always possible to exclude the necrotic / cystic areas from the manual roi for the inhomogeneities of some tumors . in addition , there is now new evidence suggesting that sccs can have biological differences due to differences in alcohol consumption and smoking , to molecular alterations , such as egfr expression , and to hpv infections , which we did not take into account [ 20 , 21 ]  . 
therefore , as many factors can influence the clinical history of patients with sccs , in our view , more studies , prospective with large samples , taking into account multiple clinical variables , are needed to evaluate the real predictive / prognostic role of adc values . compliance with ethical standards conflict of interest all authors declares that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the purpose of this study was to evaluate the feasibility and ability of rvs to assess adenomyosis since literature shows us itself has a reduced diagnostic accuracy compared to mri . materials and methods this study was conducted over a 4 - month period ( marchjune 2015 )  . 
radiologist was asked to report all three examinations separately . results on a total of 52 patients , on standard endovaginal us , adenomyosis was detected in 27 cases : of these , 21 presented diffuse adenomyosis , and 6 cases focal form of adenomyosis . 
mri detected adenomyosis in 30 cases : 22 * lucia manganaro lucia.manganaro@uniroma1.it 1 department of radiological oncological and anatomopathological sciences , umberto i hospital , sapienza university of rome , viale regina elena 324 , 00161 rome , italy 2 department of obstetrics and gynecology , university roma tor vergata , rome , italy 3 department of obstetrics and gynecology , umberto i hospital , sapienza university of rome , viale regina elena 324 , 00168 rome , italy of these appeared as diffuse form and 8 as focal form , such as adenomyoma and adenomyotic cyst , thus resulting in 3 misdiagnosed cases on us . 
rvs confirmed all 22 cases of diffuse adenomyosis and all 8 cases of focal adenomyosis . conclusions thanks to information from both us and mri , fusion imaging allows better identification of adenomyosis and could improve the performance of ultrasound operator thus to implement the contribution of tvus in daily practice . keywords rvs adenomyosis mri introduction adenomyosis is a common benign condition , frequently occurring in the 4th decade , characterized by the presence of endometrial glands within the myometrium [ 1 ]  . 
when comparing the two techniques , there are contrasting and limited results ; in fact , [ 4 , 6 ] the majority of the studies demonstrate a higher accuracy in favour of mri [ 7 ] , while few investigators demonstrated an overlap of the two techniques [ 8 , 9 ] ; however , in cases of enlarged uterus or coexisting myomas , mri has been proved to have higher sensitivity [ 10 ] than us in discriminating adenomyosis and fibromatosis . these us limits seem to be exceeded by the introduction of three - dimensional technique which allows , above all , a better visualization of the junctional zone and helps the diagnosis of adenomyosis [ 11 ]  . the possibility to have a combined real - time evaluation mri - us with the recent real - time virtual sonography ( rvs ) technology may be helpful to understand the limits and potentiality of us examination . in recent years , in fact , this technology has been particularly used for the diagnosis of tumours , especially in image - guided procedures for liver nodules [ 12 , 13 ]  . it has been suggested that rvs has a potential for training purposes to improve the operators accuracy in both tvs and mri , because it allows easier recognition of anatomical structures thanks to the point - to - point image fusion of volume data [ 15 ]  . the aim of the study was to evaluate diagnostic accuracy of rvs for the detection of adenomyosis in comparison with mri and standard us . mri protocol is shown in table 1 . prior to the us fusion technique a standard tv exam was performed on the ultrasound machine and the report recorded . 
this study was performed after approval of the protocol from our institutional review board . as for the us fusion technique a hitachi aloka ascendus ultrasound system was used with a two - dimensional tv probe . 
the dicom from the previous mri examination was loaded prior to the us exams ; t2 - weighted tse sequences oriented on sagittal , coronal and axial plane were used . 
before starting the fusion imaging , the radiologist selected the sagittal view and plane on mri loaded images and choose the plane were all the sagittal profile of the uterus could be seen as well as the endometrium at least in the fundus where the single pointer was located . 
it is not necessary to consider the body axis of patient . transverse and sagittal planes were used during the examinations as well as oblique when indicated . materials and methods this prospective study was conducted over a 4 - month period ( marchjune 2015 ) in a referral centre ; a single radiologist with a high level of expertise in gynaecological ultrasonography ( 30 years of referral practice ) analysed 52 women with us fusion imaging . 
a is an mri t2 wi and shows asymmetry of the myometrium ( white oval shape ) with inhomogeneous signal ; b is the corresponding sagittal us view and shows linear striation with shadowing effect within the myometrium ( fan - shaped shadowing ) fig . 
also evaluated its use in the evaluation of deep infiltrating endometriosis ( die ) , where it was more accurate than both us and mri in detecting the endometriotic implants [ 15 ]  . to our knowledge , this is the first study to compare the accuracy of mri , us and us - fusion in the detection of both focal and diffuse forms of adenomyosis and to demonstrate that the combination of both the imaging tools may guide the evaluation of the disease . 
ultrasound , both trans abdominal ( taus ) and transvaginal ( tvus ) , is used as the initial imaging modality in the assessment of patients with pelvic pain , menorrhagia and infertility . 
in terms of infertility it has been suggested that the presence of adenomyosis represents a relevant cause of infertility because it prevents the normal implantation of the embryo [ 2 , 18 ]  . 
however , expert sonographers are needed to perform tvs ; screening and follow - up in patients affected by adenomyosis requires a lot of experience and the learning curve may be long . 
in agreement with data literature , in our study , the coexistence of uterine fibroids affected the diagnostic accuracy of tvus in two cases of focal forms of adenomyosis due to the overlapping imaging features , whereas this did not affect the performance of rvs thanks to the simultaneous mri evaluation . 
when comparing ultrasound and mri , an advantage of mri is its high contrast resolution , high reproducibility and the standardized images obtained , which acquire importance in case of follow - up during therapy . 
rvs , combining the strengths of the two techniques , allows to have a standard examination ( mri ) for the evaluation of the progress of the disease , using a technique that is immediate and far less expensive than mri , which would be used only at the beginning of the diagnostic process of the patient for a more complete assessment of the extent of the disease . 1 3 radiol med ( 2017 ) 122 : 361368 fig . 
b and d are the corresponding us images and show the two myomas ( white star and arrow ) and an hypoechoic ill - defined area which was not assessed on us as adenomyotic cyst results from our study demonstrate an overlapping performance of mri and rvs ; therefore , we suggest a baseline exam with mri to provide a better evaluation of the extent and morphologic features of the disease , as well as of associated pathologies , and follow - up with rvs to compare the evolution of the disease on us with the baseline mri . although the results from our study are promising , several limitations must be considered . a main limitation of our study was that radiologists did not use 3d us approach , which was not provided with the machine , although it has been widely demonstrated to be a useful additional tool during us examination for the detection of adenomyosis [ 15 ]  . another limit is represented by the use of mri as gold standard because of the lack of histopathological diagnosis ; for this reason , statistical analysis could not be performed . 1 3 368 radiol med ( 2017 ) 122 : 361368 at last , another potential use of us fusion could be as a teaching tool for radiologist already trained on mri . 
in fact , it may speed up the learning process of tvus , which could be an interesting feature in a residency contest ; further studies are needed in this regard . this study demonstrates that fusion imaging improves us detection of adenomyosis . 
from september 2011 to october 2014 , 102 patients who had undergone 1.5 tesla mra of the shoulder , including conventional 2d - fse and iw - 3d and hy - 3d images were included in our study . 
supraspinatus tendon ( sst ) , infraspinatus tendon ( ist ) and subscapularis tendon ( sct ) tears , as well as antero - inferior , superior and posterior labral lesions were assessed , using surgery as the reference standard . 
the sensitivity , specificity , positive predictive values ( ppv ) , negative predictive values ( npv ) and accuracy ( acc ) for all types of rotator cuff tears and labral lesions were calculated . 
used a 3d isotropic t1 - weighted fast spin echo ( fse ) with 6 min acquisition time to study 49 patients who had undergone direct or indirect shoulder mra , evaluating both rc and labral lesions . 
in this paper , using a 6 min 38 s axial 3d dataset ; sensitivity , specificity , and inter - observer reliability were similar to conventional 2d mr arthrography for evaluation of the acetabular labrum [ 15 ]  . 
iw sequence is characterized by good spatial and contrast resolution on both tendons and glenoid labrum ; moreover , double - echo steady - state sequence may allow a further reduction in imaging time . the purpose of this study was to compare the diagnostic accuracy of isotropic 3d intermediate - weighted fse ( iw3d ) and hybrid double - echo steady - state t1 - weighted ( hy3d ) sequences and the conventional two - dimensional fse sequences ( 2d - fse ) in the evaluation of rotator cuff ( rc ) radiol med ( 2017 ) 122 : 353360 and glenoid labrum tears at shoulder mra , using surgical results as the reference standard . patients and methods patient population institutional review board approval was obtained and informed consent was waived for this retrospective study . 
 from september 2011 to october 2014 , 124 patients who had shoulder mra , including conventional 2d - fse , iw - 3d and hy - 3d images , and who subsequently had surgery , were considered for inclusion in our study . 
exclusion criteria included previous shoulder surgery ( n 14 ) , insufficient articular cavity distension ( n 2 ) , insufficient quality of datasets analyzed ( n 6 )  . 
hy - 3d images were obtained using a double - echo steady - state sequence increasing the t2 - weighting of fast imaging with steady - state precession ( fisp ) images , allowing improved delineation of fat , joint fluid , and cartilage . 
a score of 02 was considered negative , and a score of 34 was deemed positive . image analysis images were retrospectively and independently reviewed by two experienced radiologists ( gf , lr ; 11 and 21 years of experience in musculoskeletal radiology , respectively ) blinded to clinical and surgical data . 
to reduce recall bias , the datasets were analyzed separately , in three different reading sessions : 2d images were reviewed first ; iw - 3d and hy - 3d datasets were analyzed during the second ( 4 weeks delay ) and third ( 8 weeks delay ) reading sessions , respectively . 
supraspinatus tendon ( sst ) , infraspinatus tendon ( ist ) and subscapularis tendon ( sct ) tears , as well as antero - inferior , superior and posterior labral lesions were assessed . 
intra - substance tears were not included in our analysis because they could not be correlated with surgical results [ 13 ]  . diagnosis of a full - thickness tear was based on the presence of a complete defect from the articular to the bursal surface with or without retraction of the tendon . 
a partialthickness tear was represented by the visualization of a partial defect of tendon fibers along the articular or bursal surface [ 17 ]  . labral partial - thickness tears were represented by the visualization of a partial defect of the labrum , enhanced by the passage of contrast material , or by the presence of abnormal morphology or partial dislocation . 
an arthroscopic approach was adopted in 98 patients , whereas in four cases an open approach was needed for repairing large glenoid bone fracture following anterior dislocation . statistical analysis the distribution of continuous variables was reported as mean and range ( minimum to maximum values )  . 
each readers performance in assessing rotator cuff and labrum abnormalities was evaluated using the area under the receiver operating characteristic curve ( auc ) and 95% confidence intervals ( cis )  . 
the sensitivity , specificity , positive predictive values ( ppv ) , negative predictive values ( npv ) and accuracy ( acc ) for all types of rotator cuff tears and labral lesions were calculated . 
1 34 - year - old man with shoulder pa a t1 - weighted coronal 2d mr image ; b hy - 3d 1 - mm reformatted image on coronal plane ; c iw - 3d 1 - mm reformatted image on coronal plane . 
four fn were pointed out by reader 1 using 2d images , with six fn and eight fn at iw and hy - 3d images ; also , an increase in fn rate was obtained by reader 2 using 2d ( six fn ) , iw ( seven fn ) and hy - 3d images ( 11 fn )  . among 68 lesions of glenoid labrum , four fp were pointed out by reader 1 using 2d images , with three fp at iw and hy - 3d images , respectively ; reader 2 pointed out three fp at 2d and hy - 3d and four fp at iw - 3d sequences , respectively ; four fn were pointed out by reader 1 using 2d and hy - 3d images , with only three fn at iw images ; six fn were pointed out by reader 2 using 2d and iw - 3d , with eight fn at hy - 3d images , respectively . 1 3 radiol med ( 2017 ) 122 : 353360 fig . 
a t1 - weighted axial 2d mr image ; b hy - 3d 1 - mm reformatted image on axial plane ; c iw - 3d 2 - mm reformatted image on coronal plane . 
antero - inferior labral tear ( arrow ) can be depicted on axial images ; the presence of irregular glenoid bone ( arrow ) , with labral tear extending antero - superiorly ( short arrow ) , can be demonstrated on 1 - mm coronal reformatted iw - 3d image . 
3 17 - year - old woman with shoulder pa a t1 - weighted axial 2d mr image ; b hy - 3d 2 - mm reformatted image on axial plane ; c iw - 3d 2 - mm reformatted image on axial plane . 
although conventional 2d fse images are characterized by high contrast resolution , multiple sequences on different planes are needed to cover all anatomic structures of the shoulder : our 2d imaging protocol , including t1 - weighted , pd and t2 - weighted fat saturated images on multiple planes , takes on average 20 mmoreover , the possibility to miss tiny lesions because of thick slices and small gaps between slices or , because of partial volume averaging have been described [ 20 , 21 ]  . 
previously introduced high - performance mr gradients allowed the radiologists to optimize 3d imaging for the evaluation of the musculoskeletal system , without a significant increase of scanning times [ 712 ]  . 
among rc partial - thickness tears , two fn cases were correlated to the presence of tiny bursal surface sst tears , which were missed using 2d and 3d images . 
a possible explanation is that hy - 3d dataset is characterized by an intrinsic low contrast in depicting tendons , so that tears are well visualized when the articular cavity is adequately distended with contrast material . 
iw - 3d allowed us to obtain the highest sensitivity in identifying labral tears for reader 1 ( 95.6% ) ; a small defect of posterior labrum was missed at 2d and hy - 3d , but identified at iw - 3d . 
as regards labral defects , fn findings were correlated with tiny labral tears considered as large sub - labral recess ( n 2 ) or not adequately opacified with contrast material ( n 1 ) for each image dataset . 
hy - 3d images and iw - 3d allowed us to better evaluate bony lesions frequently associated to labral disorders in case of 1 3 radiol med ( 2017 ) 122 : 353360 anterior shoulder dislocation [ 22 ] ; these datasets allowed us to correctly image all bony bankart lesions , diagnosed in eight patients enrolled , but missed using 2d images in three cases . 
conversely , accurate values for reader 2 were higher in evaluating rc lesions ( 92.2% for iw - 3d dataset and 88.2% for hy - 3d dataset , respectively ) , without any difference as regards the evaluation of labral tears ( 90% of accuracy using both sequences )  . 
although the acquisition time of iw - pd dataset is longer than a single sequence in the 2d series ( 6 min vs 3 or 4 min on average ) , motion artifacts were limited , thanks to optimized position of the patient within gantry . 
our data showed this sequence could be used instead of pd and / or t1 - weighted sequences on multiple planes both in case rc or labral lesions are suspected : as previously reported in the study of park et al . 
 [ 15 ] , it may be more difficult to detect increased water content within edematous bone marrow when compared with the highly fluid - sensitive fat - suppressed t2 - weighted fse sequences because of potential weakness of the iw tissue contrast . 
for these reasons , we believe coronal t2 - weighted fs sequence is still necessary to adequately assess bone marrow edema ; a fast 10 min protocol , including iw - 3d and cor t2 fs is now under evaluation at our institution in clinical practice . this study had some limitations . 
second , other imaging findings , including bony bankart and hillsachs lesions and articular cartilage defects were not considered in our statistical analysis , even though they were relatively uncommon in our study population . 
furthermore , the surgeons were aware of mri findings . in conclusion , at 1.5 tesla shoulder mra , the accuracy of iw - 3d and hy - 3d images was not significantly higher than the 2d sequences in diagnosing rc and labral abnormalities . 
while iw sequence may have the potential to substitute conventional 2d sequences for diagnosing rotator cuff and labral tears , hy - 3d images could be considered an additional tool for evaluating tiny labral lesions suspected on the basis of clinical findings or on the basis of 2d imaging . compliance with ethical standards conflict of interest the scientific guarantor , corresponding author of this publication is giovanni foti . 
also , none of the study subjects or cohorts has been previously published . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent since this was a retrospective study , formal consent was not required . 
surgical pathologies were pnet ( n 42 ) , microcystic serous cystadenomas ( m - scn , n 12 ) and solid pseudopapillary epithelial neoplasms ( spen , n 20 )  . 
using a combination of morphological patterns and enhancement features , pnet was identified with 88% sensitivity and 81% specificity , m - scn was identified with 83% sensitivity and 94% specificity , and spen was identified with 90% sensitivity * hua - dan xue bjdanna95@hotmail.com 1 department of radiology , peking union medical college hospital , shuaifuyuan no . 
pnet could be differentiated from its mimics with high accuracy . keywords pancreatic neoplasms multidetector computed tomography ca19 - 9 diagnosis introduction multidetector ct ( mdct ) of the abdomen has been widely used for the evaluation and characterization of focal pancreatic lesions [ 13 ]  . 
nevertheless , the 1 3 338 radiol med ( 2017 ) 122 : 337344 cystic nature of microcystic serous cystadenoma ( m - scn ) could not always be well appreciated , as they often have a hypervascular solid - dominant appearance , which could be mistaken for more malignant solid tumours [ 10 , 1316 ]  . 
surgeries could be avoided if the benign nature of the lesion is confidently diagnosed based on radiological findings . therefore , the aim of this study is to investigate mdct features of enhancing pancreatic mass with normal serum ca19 - 9 level , and to determine key features that characterize pnet from its mimics . materials and methods patients this retrospective study was approved by the institutional review board , and written informed consent was waived . 
patients were recruited in this study based on the following inclusion criteria : patient received pre - treatment multiphase mdct and demonstrated pancreatic lesion with enhancement ; patient had blood tumour biomarker test within one month of mdct imaging , and serum ca19 - 9 level was within normal range ; patient received pancreatic surgery at our institution . exclusion criteria were enhancing pancreatic mass with a histological diagnosis different from pnet , m - scn and spen ( n 6 , including two focal autoimmune pancreatitis , two pancreatic acinar cell carcinoma , one pancreatic lymphoma and one pancreatic squamous cell carcinoma ) ; patients with known familial history of von hippellindau syndrome ( vhl , n 1 ) and multiple endocrine neoplasia syndrome type 1 ( men1 , n 5 )  . 
the mean time interval between mdct and pancreatic surgery was 17 days ( range 171 days )  . imaging technique ct examinations were performed on 128 - detector ct scanners ( siemens somatom definition flash , siemens healthcare , forchheim , germany )  . 
the scanning parameters were as follows : tube voltage , 120 kvp ; effective amperage settings , 150 mas ; gantry rotation time , 0.5 s ; table increment , 46.8 mm per rotation ; matrix 512 512 . 
thin slice images with 1.0 mm section thickness / 1.0 mm interval were also reconstructed for post - processing purposes . non - ionic contrast media ( ultravist , 370 mg of iodine per milliliter , schering , berlin , germany ) were injected with 1.5 ml per kilogram of body weight , at a rate of 3.0 ml / s using an automatic power injector . 
the equilibrium phase ( ep ) was initiated 90 s after the pap phase . 1 3 radiol med ( 2017 ) 122 : 337344 image analysis mdct images were independently evaluated by two radiologists ( 13 and 12 years experience in interpreting abdominal ct / mr , respectively ) on the picture archiving and communication system ( pacs , centricity , ge )  . 
 both readers were blinded to the surgical and pathological information . the location of the lesion ( head , body or tail of the pancreas ) was documented and lesion size measured . 
secondary changes of the pancreas due to tumour compression were also recorded , including upstream dilatation of the main pancreatic duct and side branches , and distal pancreatic parenchymal atrophy . 
honeycomb pattern was characterized by multiple small chambers of hypoor non - enhancing area , separated by hyper - enhancing fine septumelting icecream pattern denoted lesion with inhomogeneous faint enhancement and partial non - enhancing area within the tumour which melts away from the solid enhancing part . 
lesion - parenchyma attenuation difference was compared in each phase , and lesions were classified into hypo - attenuating in all phases or hyper - attenuating in one or more phases . 
inter - observer agreement of the ct features was determined by calculating kappa values ( 0.210.40 , fair agreement ; 0.410.60 , moderate ; 0.610.80 , good ; 0.811.00 , excellent agreement )  . 
melting icecream pattern ( c ) was characterized by partial non - enhancing area which melts away with the solid - appearing enhancing part of the tumour results mdct findings for each disease entity were summarized in table 2 . 
on the contrary , lesion location , size , calcification and secondary changes to the pancreas ( upstream pancreatic duct dilatation and distal parenchyma atrophy ) were not significantly different for these three pathologies . 
an enhancing mass was seen in the pancreatic head ( arrow ) , which enhanced avidly in pancreatic arterial phase ( pap , a ) , with multiple small chambers of non - enhancing area . 
the honeycomb morphological pattern was better appreciated on later phase ( b ) , as the condense septa within the tumour enhanced less intensely and the microcysts remains non - enhancing . 
using a combination of morphological pattern and one enhancement feature ( enhancement peak of the lesion or lesion - parenchyma contrast ) , pnet could be differentiated from the other lesions with 88% sensitivity and 78% specificity . 
m - scn could be identified with 83% sensitivity and 94% specificity , and spen could be identified with 90% sensitivity and 91% specificity . 1 3 radiol med ( 2017 ) 122 : 337344 in young women ; however , a trend towards decreasing tumour size was noted , as the accessibility of cross - sectional imaging is increasing and more incidental tumours are detected at earlier stage [ 9 ]  . 
although spen was known to have predilection in female patients of younger age , it is noted that in our patient cohort , male patients and older patients were also encountered , adding to the difficulty of characterization . 
 awareness of the key ct features of the above - mentioned pathologies is mandatory , since pancreatic surgeries are associated with substantial risk of morbidity and should only be performed for overt or latent malignant lesions . 
 a thorough understanding of the ct findings is helpful to avoid incorrect or inconclusive mdct diagnosis , which leads to unnecessary surgeries or additional diagnostic procedures , with increased cost and invasiveness to the patient . in our study , a combination of morphological patterns and enhancement features improves diagnostic accuracy for lesion characterization , and the inter - observer agreement for these ct findings was good to excellent . 
this result suggested that pnet could be well characterized from its mimics using key mdct features . to evaluate the key features leading to a correct diagnosis , we focused on the morphological patterns of the lesions , calcification and secondary change of the pancreas . 
cells near the vessel remain intact , whereas cells distant from the vessel underwent degenerative change , which gave its typical look of solid friable tumour , and its melting icecream pattern , as reflected in this study [ 20 ]  . 
surgical pathology confirmed solid pseudopapillary epithelial neoplasm discussion when an enhancing pancreatic mass is detected and patient has normal ca19 - 9 level , characterization of the lesion becomes an important issue . 
the frequency ofpresence of calcification , and the morphology of calcification were not significantly different among thesethree pathologies , and thus not key features for lesion characterization . enhancement patterns of the lesions were also investigated . 
in our study of 20 spen , 2 were less than 3 cm and 8 were less than 4 c progressive filling - in pattern was observed in most spen , which is in accordance with their study . 
 it has been suggested that the imaging features of spen differ between male and female gender , and male patients tend to have larger tumours with more solid component , and a lobulated margin [ 23 ]  . 
 awareness of key mdct features for lesion characterization is mandatory for clinical decision - making . in conclusion , morphological features and enhancement patterns on mdct are key features for characterizing enhancing pancreatic mass with normal serum ca199 . 
 the purpose of this article is to suggest a flow - chart to evaluate the placement of uvc , testing it in young radiologists - in - training . method we developed a simple flow - chart to asses , steps by step , uvc placement considering its course and tip location ( ideally placed in the atriocaval junction )  . 
we tested the flow - chart impact asking to 20 residents to evaluate the placement of 10 uvc before and after they familiarized with the flow - chart and the anatomical findings of a newborn . 
dalessandro , university of palermo , palermo , italy keywords flow - chart frontal radiogram radiology resident umbilical venous catheter introduction since the introduction of intravascular catheters and the use of the umbilical vein for exchange transfusions , umbilical venous catheters ( uvc ) have been routinely used in premature infants to administer parenteral alimentation or antibiotics ( according to the different pathological conditions ) [ 1 ]  . they can be easily detected on frontal abdominal radiograms , indeed normally uvc enters on the anterior abdominal wall at umbilicus , and predominantly follow an anterior and cephalad course ( following the left umbilical vein course )  . 
the wilcoxon matched - pairs sign rank test was used to assess if the number of correct characterizations of uvc position was significantly different before and after the administration of the flow - chart . 
 then , we splitted the data according to the different residency years . the chi - square test was calculated to assess the homogeneity of the evaluations of uvc placement executed by the 20 radiology residents before and after the 1 3 radiol med ( 2017 ) 122 : 386391 388 fig . 
d3 3rd dorsal vertebra ; d4 4th dorsal vertebra ; d5 5th dorsal vertebra ; d9 9th dorsal vertebra ; d10 10th dorsal vertebra ; d12 12th dorsal vertebra ; ivc inferior vena cava ; la left atrium ; l2 2nd lumbar vertebra ; l3 3rd lumbar vertebra ; pv pulmonary vein ; ra right atrium ; svc superior vena cava ; uvc umbilical venous catheter their simplicity makes them useful tools for communicating how processes work and provide key - points in a simple and concise manner . 
 it could be used to define and analyze processes , communicate steps to other people involved in a process , standardize a process , improve a process , identify bottlenecks or troubleshoot a proble moreover , drawing a flow diagram , you can zoom in each individual stage , without feeling overwhelmed by the rest of the process [ 913 ]  . some academic programs and many individual faculty members have tried applying techniques to facilitate learning in their work . 
furthermore , joint commission and important medical societies , proposed flow - charts and other support decision tools for a simple understanding of surgical procedures , management of several diseases or 1 3 radiol med ( 2017 ) 122 : 386391 fig . 
3 fetal circulation anatomy table shown to residents to identify critical points of vulnerability in hospital organization , with excellent results [ 1416 ]  . some authors proposed diagnostic flow - charts for the evaluation and management of different pathologies [ 17 , 18 ] ; for example , colombi et al . 
 [ 17 ] offered a flow - chart with the attempt to support the less experienced clinician in stringently recognizing joint hypermobility syndrome / ehlers - danlos syndrome hypermobility type ; polsfuss et al . 
the ductus venosus is 12 cm long and ends in the left or middle hepatic vein , very close to the junction with the inferior vena cava [ 19 , 20 ]  . as previously described , when a uvc is inserted , it follows the path of the umbilical vein , and in a standard frontal abdomen radiogram , it is placed on the right of lumbar spinous processes ( lumbar vertebrae l3l4 ) , it courses posteriorly through the liver ( closely to the dorsal vertebrae d10d12 ) to the left portal vein and then to ductus venosus and ivc ( d9 level ) fig . 
other recent paper suggest a simple method to assess the precise position of uvc using morphometric measurement of the new born before placement ; however , this method do not avoid misplacement that could be only assessed in plain film [ 21 ]  . our flow - chart summarizes these key - points to evaluate uvc placement , in particular it describes its course and tip location . 
according to the standard / normal position of the uvc using that is possible to judge a correct positioning of the uvc . the students have considered the flow - chart simple and easy to understand . 
according to our results , the number of correct characterizations of uvc position was significantly different after the administrations of the simplified flow - chart : indeed on a first evaluation there were only 106 / 200 ( 53% ) correct assessments of correct or uncorrect positioning of the uvcs evaluated , this number switched to 196 / 200 ( 98% ) correct assessments after the administration of the flow - chart . this result does not surprise , considering the limited experience of younger students ; otherwise they are usually more familiar to support decision tools . 
we have not found significant difference in determination of correct and malposition of uvc in all residents , with similar performance independently from the residents year course ; so the real difference in performance was determined by the use of the flow chart as observed among the twenty radiology residents . however , after the evaluation of flow - chart , there were significant performance improvement both in first year course and successive year courses residents , and the difference was statistically significant . 
hence , the flow - chart improved the results in all students and it could be considered to prove that the flow - charts can became useful tools for teaching improvement programs . 
so , in our case , flow - chart improved the results in the whole sample , becoming an useful tool to teach residents to easily understand the correct placement of uvc . this algorithm is accurate , simple , easy to use , inexpensive , and therefore , applicable in the standard routine radiological evaluation . 
obviously , these techniques are tools that complete and help an extensive study , that of course , cannot be replaced only by flow - chart . the flow - chart could became an useful tool to accompany the daily reporting of the radiologist , especially on issues to them lesser known . compliance with ethical standards funding none . conflict of interest all authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . ethical standards this article does not contain any studies with animals performed by any of the authors . 
the aim of this study is to compare the differences between cyberknife ( ck ) and tomotherapy ( ht ) treatment plans of rs of single brain metastasis ( bm ) to define when ht should be used in cases beyond cyberknifewhen both systems are readily available for the radiation oncologist . methods and materials nineteen patients with single brain metastasis treated with ck were re - planned for radiosurgery using tomotherapy hi - art syste two planning approaches have been used for tomotherapy plans : the classical one ( ht ) and the improved conformity ( icht ) that produces dose distributions more similar to those of rs plans . 
ptv coverage , conformity index ( ci ) , paddick conformity index ( nci ) , homogeneity index ( hi ) , gradient index ( gi ) , and beam on time of ck , ht , and icht plans were evaluated and compared . results a good coverage was found for ck , ht , and icht plans . 
better dose gradients compared to both icht and ht modalities were observed in ck * daniela greto daniela.greto@gmail.com 1 radiotherapy unit , azienda ospedaliero universitaria careggi , university of florence , largo brambilla 3 , 50141 florence , italy 2 medical physics unit , azienda ospedaliero universitaria careggi , university of florence , florence , italy 3 medical physics unit , i.f.c.a. , florence , italy 4 molecular and nutritional epidemiology unit , ispo ( cancer research and prevention institute ) , florence , italy plans . 
icht modality showed improved mean ci respect to ht modality , similar to that obtained in ck plans . conclusions ck plans show higher conformity and lower gi than icht and ht plans . 
cyberknife and tomotherapy are both optimal rs devices , the choice to use one over another has to be clinically guided . keywords brain metastasis cyberknife tomotherapy radiosurgery dosimetric comparison background brain metastases are the most frequent intracranial neoplasms in adults . 
in patients suffering of cancer , bms will appear in 2040% of cases , and in 1015% , bms are present at the first diagnosis [ 1 ]  . considering the longer survival of cancer patients related to the early detection of disease and treatment improvements , the incidence of brain metastatic disease will increase . 
for this reason , the interest to control the brain disease , to preserve functions , to enhance the quality of life , and to avoid the death due to neurologic causes and not only palliate the symptoms is becoming a clinical priority . the treatment options for brain metastatic patients are whole brain radiotherapy ( wbrt ) , surgical resection , and stereotactic radiosurgery ( rs )  . 
the choice of a local treatment alone or in association to whole brain radiotherapy is usually done depending on performance status , number of bms , controlled systemic disease , and histology [ 2 ]  . 
 recently , two large randomized studies have shown similar 1 3 radiol med ( 2017 ) 122 : 392397 survival benefits and functional independence between patients with 13 bms treated with rs alone and rs plus wbrt [ 3 , 4 ]  . rs may result in a better local control in patients with radioresistant histology , and it can delay wbrt , such as salvage treatment . 
the use of rs as the exclusive treatment of bms is affirmed in emerging studies employing this approach ; recently , a japanese prospective observational study reported that the outcome of patients with five to ten bms treated with rs without wbrt is non - inferior to that of patients with two to four bms in terms of overall survival [ 8 ]  . rs treatments were originally performed with gammaknife , a device equipped with hundreds of 60co sources focused to a single point , and after few years also with linear accelerators . 
while , in the first case , invasive stereotactic frames are used for both target localization and patient immobilization ; in the second one , thermoplastic mask coupled with imaging techniques as cbct is usually employed . 
in the last few years , new systems , such as cyberknife ( accuray incorporated , sunnyvale , ca , usa ) and helical tomotherapy ( accuray incorporated , sunnyvale , ca , usa ) , capable of delivering highly conformed dose distribution to targets with complex shapes have been proposed and used to deliver rs treatments non - invasively . 
cyberknife plans are , in fact , characterized by inhomogeneous highly conformal dose distribution to the target , while tomotherapy plans can provide both homogeneous and typical radiosurgery dose distributions [ 9 ] to the target . in both cases , no invasive head frame is used as patients are immobilized with thermoplastic masks and targets are localized using images : a couple of orthogonal kilovoltage ( kv ) x - ray images in cyberknife treatments and megavoltage ct images in helical tomotherapy cases . the localization and the high dose conformity immobilization approaches , together with that both cyberknife and helical tomotherapy are capable to deliver , make them suitable to perform radiosurgery treatments . 
to understand if one device shall be preferred to the other and to analyze possible advantages of one modality over the other , we performed a dosimetric comparison between the plans of 19 single brain metastases , originally treated with cyberknife , and subsequently re - planned for helical tomotherapy . 
the same planning target volume ( ptv ) used for cyberknife , obtained adding a further 1 - mm uniform margin to ctv , was also employed in tomotherapy planning . 
we are aware that due to the image guidance [ 11 ] , 1 - mm margin is considered safe for cyberknife brain treatments and not for tomotherapy treatment unless more invasive patient immobilization devices are employed [ 12 ]  . 
a detailed description of the parameters used to 1 3 394 radiol med ( 2017 ) 122 : 392397 index the treatment plan conformity and dose fall - off outside the treatment volume is given in the following session . 
the treatment planning optimization resulted in an arrangement of non - isocentric non - coplanar beams of various sizes : a trade - off was accepted between the total beam number ( which is correlated to the plan delivery time ) and the plan conformity and dose gradient , obtaining on average 141 beams ( range 99160 )  . tomotherapy planning results performed using the wilcoxon signed rank test . 
the statistical package for the social sciences ( ibm corporation , new york , usa ) was used . two planning strategies have been followed to prepare tomotherapy plans : the classical one ( ht ) , which consists in delivering a highly homogeneous dose distribution to the target and the improved conformity which , on the contrary , forces the system to deliver higher doses inside the target to obtain the steepest dose gradient outside it . 
 [ 9 ] , creates a dose distribution comparable to that of rs plans using additional non - anatomic planning structures , both internal and external with respect to ptv , according to a specific prescription . 
in the icht mode , the 125% of the prescription dose was required to cover an inner non - anatomic planning structure , while the maximum dose to the ptv was released . 
for this purpose , 19 plans of single brain metastasis planned with cyberknife and re - planned with tomotherapy were compared evaluating the conventional index used to score rs plans , namely ci , hi , gi , and beam on time . 
in ck , the irradiation is performed using nonisocentric non - coplanar beams coming from different angles , while in helical tomotherapy treatments , dose is delivered by a collimated fan beam along an helical pattern . 
moreover , when a helical tomotherapy system with fixed jaws is considered ( as the one here used ) , additional doses superior and inferior to the target volume are observed [ 14 ]  . the same behavior we observed for ci is pointed out in gi analysis . 
 [ 15 ] evaluated 551 plans of both malignant and benign brain lesions treated with gammaknife reporting a median ci of 1.24. a median ci of 1.67 was reported by nakamura et al . 
considering that the volume of the target could limit the use of radiosurgery , ht could be advantageous in cases of multiple bms that have to be treated in the same rs session or in case of wbrt with integrated boost to the lesions [ 18 ]  . 
 [ 20 ] , hotspots inside targets could not necessarily result in a significant risk of complications compared to more homogenous dose distribution . the importance of homogeneity in radiosurgery plans is still controversial ; in fact , if the heterogeneity is considered from some authors , a factor that could influence the local control [ 21 ] in particular in radioresistant metastasis [ 22 ] ; on the other hand , the heterogeneity could be related with higher probability of toxicities [ 23 ]  . 
it is worthwhile to mention that besides dose heterogeneity , other important predictors of radionecrosis are : prescription dose , tumor size , and location , and the brain volume that receive at least 12 gy ( v12 ) [ 2426 ]  . conclusions in the last few years , an improvement in clinical outcome of brain metastatic patients , not correlated to radiotherapy devices used to perform rs , was observed . 
for this reason , considering also the impressive diffusion of new technologies , such as cyberknife and tomotherapy , it is important to guide the use of a specific device keeping into account its characteristic performances . 
four complications of the ipsilateral group were classified as major group c and 1 as major group d , while 1 complication of the contralateral group was classified as minor group b and 1 as major group c according to society of interventional radiology ( sir ) classification . 
no statistical significant difference was seen between complication rates of two groups in regard to sir classification . conclusions spc related complications do not differ in regard to ipsilateral or contralateral side selection on mastectomized patients with breast cancer and lymph node dissection . 
spcs can be implanted on ipsilateral or contralateral sides of the operation in these patients . keywords breast cancer contralateral ipsilateral society of interventional radiology subcutaneous port catheter introduction subcutaneous port catheters ( spcs ) have become an increasingly used technique in the treatment of oncology patients . 
venous access during spc implantation can be challenging in oncology patients , especially in patients with history of breast cancer surgery and / or radiotherapy ( rt ) [ 2 ]  . lymphedema can develop on ipsilateral upper extremity in patients with the history of modified radical mastectomy ( mrm ) or lumpectomy and lymph node dissection . 
although a scientific proof is not present , general opinion is to avoid all venous interventions ( from a simple intravenous cannulation to spc implantation ) in the ipsilateral extremity that lymph node dissection has been done . 
lymphatic drainage can be made partially through alternative ways like internal mammarian nodes in patients with mastectomy and lymph node dissection [ 2 ]  . the aim of this study is to evaluate long - term clinical follow - up results and complication rates of implanting spcs on ipsilateral or contralateral side of the chest with mastectomy side in patients with axillary lymph node dissection . materials and methods protocol inclusion criteria for patients were : female gender , history of breast surgery for breast cancer and eligible for the port implantation procedure ( international normalized ratio [ inr ] below 1.5 , platelet count higher than 75 , 000 / mm3 and good performance status )  . 
spcs were implanted to 73 patients with breast cancer in our department between march 2012 and september 2014 , of which 34 were on the ipsilateral and 39 were on the contralateral side with the operation . 
all of the patients were women and have been treated with breast - sparing surgery ( lumpectomy ) or mrm and lymph node dissection . patients were divided into two groups : ipsilateral group ( 34 patients ) and contralateral group ( 39 patients )  . 
classification of complications according to sir criteria was : minor complications , ( a ) no therapy , no consequence , ( b ) required nominal therapy , no consequence ; included overnight admission for observation ; major complications , ( c ) required therapy , minor hospitalization ( < 48 h ) , ( d ) required major therapy , unplanned increase in level of care , prolonged hospitalization ( > 48 h ) , ( e ) permanent adverse sequelae , ( f ) death . 
local anesthesia alone ( prilocaine 20 mg / ml , citanest , astrazeneca and lidocaine 20 mg / ml epinephrine 0.025 mg / ml , jetokain , adeka ) was adequate for the procedure in most of patients . 
spcs were single lumen catheters and were implanted under the guidance of a monoplane , flat panel angiography unit ( artis zee , siemens , erlangen , germany ) by an experienced interventional radiologist . 
types and characteristic of spcs used are given in table 1 . surgical skin cleansing was made by applying the antiseptic solution ( povidone iodine 10% , batticon , adeka ) to the operation side from mandibular level to lower border of the breast and middle axillary line under sterile conditions in the operation rooa single - wall puncture needle ( 18g ) was introduced into the internal jugular vein under ultrasound ( us ) guidance . 
the port catheter 1 3 474 port table 1 types and characteristics of the implanted ports radiol med ( 2017 ) 122 : 472478 catheter number of patients ( ipsilateral group ) number of patients ( contralateral group ) port - a - cath ii low - profile ( sims deltec , st paul , mn ) pro - fuse ct power injectable low profile ( medcomp , harleysville , pa ) infu - kt titanium standard intravenous access ( fb medical , france ) polysite adult standard ( perouse medical , france ) polysite adult standard ( perouse medical , france ) focus titanium & polysulfone ( promecon gmbh , germany ) 7.8 f , polyurethane 8 f , polyurethane 7.8 f , silicone 7.2 f , polyurethane 9.5 f , polyurethane 10.5 f , polyurethane was introduced into the tunnel by the help of a trocar and it was attached to the reservoir with locking technique . 
functionality of the spc was controlled by injecting 100 u / ml heparinized saline through the port reservoir . patients were followed for 2 h after the procedure in the observation room in regard to hemorrhage and pneumothorax risk . 
the level of significance was determined to be 0.05. results median ages of 34 patients in the ipsilateral group and 39 patients in the contralateral group was 47.3 ( 2866 years ) and 50 ( 3468 years ) , respectively ( table 2 )  . 
group characteristics similar in two groups were : evaluation was retrospective , spc indication was ct , the nature of ct was curative , all patients were outpatient , lymph node dissection history was present in all patients , procedures were technically successful , spcs were implanted under sterile conditions with full dressing in a single session , the procedure was made under fluoroscopy and us guidance , spcs were controlled with heparinized saline injection after the procedure , complete wound closure was ensured , control fluoroscopic images were obtained , there was no malfunction per 100 catheter days and no revision per access site / per 100 catheter days . 
tumor was on the right breast in 31 patients ( 31 / 34 ; 91.2% ) , on the left in 3 patients ( 3 / 34 ; 8.8% ) in the ipsilateral group . 
in ipsilateral group , thrombus was present in jugular vein of three patients ( 3 / 5 ) , in vena cava superior and brachiocephalic vein of one patient ( 1 / 5 ) and in vena cava superior of one patient ( 1 / 5 )  . 
2 findings suggestive of thrombosis on a fluoroscopic image after contrast media injection into the catheter 13 months after implantation of a right sided port catheter in a patient with lumpectomy history in her right breast : contrast media is not passing from superior vena cava into the right atrium and there is pericatheter leakage of the contrast media is to axillary and internal mammary lymph nodes . 
there was no statistical difference between two groups in regard to infections per 1000 days . early ( within 30 days of the procedure ) and late ( after 30 days of the procedure ) complications can happen after spc placement . 
1 axial ( a ) and coronal ( b ) computed tomography angiography images : thrombosis in the catheter and superior vena cava leading to occlusion 11 months after implantation a right sided port catheter in a patient with lumpectomy history in her right breast ( black arrows port catheter , star thrombus ) can be implanted successfully by us and fluoroscopy guidance and procedure related and infective complication rates are low when imaging guidance is used [ 5 , 6 ]  . 
the standard access for spcs is through the subclavian / internal jugular vein or cephalic vein , but a femoral vein access may be preferable in patients with history of breast surgery and / or rt [ 7 ]  . 
we preferred the chest approach and spcs have been implanted with imaging guidance in our interventional radiology unit . lymphatic drainage of the upper extremity is to axillary lymph nodes [ 5 , 10 ] while drainage of the chest wall 1 3 radiol med ( 2017 ) 122 : 472478 fistula , pneumothorax , hemothorax and hematoma are early complications seen within 24 h . 
thrombus most commonly forms at the entrance site of catheter into the vein or with the contact of catheter and wall of the ve it is usually asymptomatic and can lead to infection and pulmonary embolis the effect of type of catheters on thrombus formation is controversial [ 12 ]  . 
 however , this situation did not affect the randomization of the study , because no statistical correlations were observed between complication rates and dimensions / materials of catheters for both groups . one limitation of our study is its retrospective nature . 
it is a potential route for embolic transit from the systemic venous circulation to the brain [ 5 ] , and its prevalence is higher in young patients with cryptogenic stroke than in those with a known stroke etiology [ 6 ]  . 
it is considered small if it has a diameter of 25 mm , and large if its diameter 610 mm [ 7 ] , but it is also possible to quantify its size by measuring right - to - left shunt ( rls ) [ 8 ]  . the most frequent mechanism explaining an increased risk of recurrent stroke is paradoxical embolism due to the systemic passage of venous thrombi through an inter - atrial conduit . 
demonstrated a greater involvement of the vertebro - basilar ( vb ) system in pfo - related stroke ( pfostroke ) , which is usually identified as a cortical ischemic lesion in the vb circle , whereas af - related stroke ( afstroke ) is associated with the presence of cortico - subcortical ischemic lesions involving multiple vascular territories [ 15 ]  . the aim of this study was to map the specific ischemic lesion patterns of distribution of pfo - stroke and af - stroke in our study population . materials and methods inclusion criteria and imaging we retrospectively reviewed the medical records of 750 patients admitted to our hospital with a clinical suspicion of acute ischemic stroke between january 2008 and february 2016 . all patients underwent ct scan of the brain in the emergency department and 534 patients underwent magnetic resonance ( mr ) brain scan during the admission in neurology department . by diagnostic test , including both laboratoristic and instrumental , the patient subtypes were classified using the five categories of the toast classification system [ 2 , 3 ]  . 
when mr studies were not available on pacs , we used all films found in patients records . finally , analysis of the background data of all of the patients identified two groups with different pre - existing diseases : 128 with pfo and 43 with af . 
in few patients of the pfo - group ( 18 ) , imaging was not available and it was considered only radiologic reports . we evaluated the patients symptoms ( headache ) , demographics characteristics ( gender , age ) and risk fig . 
pfo patent foramen ovale , af atrial fibrillation , c - tcd transcranial color doppler ultrasonography with contrast , tee transthoracic echocardiography , ct computed tomography , mri magnetic resonance imaging 1 3 414 radiol med ( 2017 ) 122 : 412418 factors ( hypertension , smoke , dyslipidemic disorders ) , and the presence / absence of an atrial septal aneurysm 10 mm of phasic septal excursion into ( defined as 15 mm durthe atrium or a sum total excursion of ing the cardiorespiratory cycle with base 15 mm as measured using m - mode ) [ 1 ] and rls . 
the entity of the shunt after c - tcd and tee with saline solution was evaluated because these have been considered sensitive methods of detecting a pfo [ 8 ] , which is defined as the passage of > 3 micro - bubbles from the right to the left atrium through the gap during the three cardiac cycle following the complete opacification of the right atrium [ 1 ]  . rls was detected through c - tcd and tte in all patients affected by pfo . 
 respectively , the cardiologist analyzed the count of the maximum number of micro - bubbles seen in left atrium in basal condition and after valsalva maneuver , while the neurologist analyzed the count of the maximum number of micro - bubbles detected in the spectral display of the insonated internal carotid arteries and in the mcas . 
 suggest [ 18 ] , the number of micro - bubbles detected through mca - doppler measurement it could be useful to quantify the rls , so it was possible to classify rls in small ( < 10 bubbles ) , large shunt in shower ( > 25 bubbles ) and curtain ( uncountable signals ) [ 8 ]  . moderate ( 620 bubbles ) , and grade 3 the dwi and flair sequences were used to confirm the ischemic lesions , which were classified in cortical , subcortical and cortical / subcortical . 
only 153 patients were enrolled for this analysis because imaging for 18 was not available . as in other studies , the affected vascular territories were divided into the anterior cerebral artery ( aca ) , mca , vb including pca ( posterior cerebral artery ) , brainstem , and cerebellar [ 19 ]  . 
all 171 patients were considered for this analysis , because also the reports of 18 patients with imaging not available described the sites of ischemia of the brain . two neuroradiologists , with , respectively , 6 and 20 years of experience , made these analyses . this type of work does not require approval by ethics committee , because of the retrospective nature of the study , but before all diagnostic exams patients received and signed informed consent . statistical analysis the differences in the frequency of lesion patterns and the corresponding vascular territory of the lesion between the patients with pfoand af - stroke were compared using pearsons 2 test . 
the size of the pfo was determined in the patients with pfo - stroke , and the correlation between the c - tcd and tee finding were assessed using the index of inter - rater reliability ( cohens k )  . 
age , gender , and risk factors were compared using students t test or pearsons 2 test as appropriate , and the frequency of a history of headache in the pfo - stroke group was analyzed . 
the statistical analyses were made using xlstats ( rodney carr 19972004 ) and graph pad instat software ( 19922009 by graphpad software )  . results 74 were males and n of 171 patients , n females . 
the causes of cryptogenetic stroke comprehend paradoxical af , arterial dissection , vasospasm , migraine - induced stroke , and pfo [ 21 ]  . patients with known causes , evaluated by clinical , laboratoristic , and instrumental findings , were excluded . 
it could be related to a selection bias due to the fact that medical records were from neurologic department . in our study , we did not find lesions in aca territories known and undetermined etiology ( cryptogenic ) [ 2 , 5 ]  . 1 3 416 radiol med ( 2017 ) 122 : 412418 pfo and af are sources of cardio - embolism because they generate arterial occlusions presumably due to an embolus resulting from the heart [ 2 ]  . embolism of cardiac origin is caused by three mechanisms : blood stasis and thrombus formation in an enlarged heart left chamber ( or with intracavitary abnormal structures or aneurysm of the left ventricle ) , supravalvular presence of material , and abnormal passage of venous blood to the arterial circulation ( paradoxical embolism ) [ 22 ]  . one of the most accredited etiopathogenic mechanism of cerebral ischaemia due to pfo is the paradoxical embolism in departure from peripheral venous district . 
this hypothesis assumes the association between venous thromboembolism and rls in the heart , as in the case of pfo [ 18 ]  . stroke in pfo - group involved a younger population than af in our study . 
in hommas metanalysis , several studies described the correlation of pfo with cryptogenic stroke in younger patient populations , however , the association with older patients is still controversial [ 23 , 24 ]  . sathasivam and sathasivam demonstrated the association between pfo and headache , we analyzed the anamnestic background of our study population and we noticed that the majority ( 58% ) of patients with pfo had recurrent episodes of headache [ 25 ]  . 
 [ 1 , 13 ]  . atrial septal aneurysm , an abnormal prolapse of atrial tissue , which protrudes in both or left or right atrium , was present in 16 patients of pfo - group . 
mechanisms of stroke in patients with those abnormalities may include direct embolization from thrombi formed within the aneurysm and also formation of thrombus as a result of atrial arrhythmias , this one was not present in our patients [ 31 ]  . considering that the hemodynamic of the circle of willis is determined by the confluence of flow of the two internal carotid arteries and of the basilar artery , and by the blood flow direction from vessels with high pressure to vessels with low pressure [ 24 , 32 ] , we hypothesized the possible correlation between frequent involvement of the vb territory and an anatomical variance of the pca , such as its embryonic origfrom our preliminary study , we did not achieve a statistically significant correlation ; these results could have been strongly influenced by the low number of patients who had a diagnostic angiographic mr and / or ct in their background . 
4 pattern of cortical involvement of pfo - stroke : left frontal cortical involvement on flair ( a ) and dwi ( b ) images 1 3 radiol med ( 2017 ) 122 : 412418 present embryonic origin of pca ( table 1 ) ; this result probably was obtained because of the limited number of the candidates who underwent angiographic studies ( only 51 patients on a record of 128 )  . 
in spite of the low number of patients with this anatomical variant , a positive association could be found with furthermore studies , because few articles concerning this argument are available in the literature [ 24 , 33 ]  . our study is limited by three factors : at first time , it is a retrospective study . 
we sought to evaluate prevalence and distribution of cn in carotid arteries in correlation with clinical symptoms . methods 178 consecutive patients with unilateral ischemic 2 mm by duplex ultrasound stroke and carotid plaques underwent a carotid - black - blood - 3t - mri with fat - saturated preand post - contrast t1w - , pdw - , t2wand tof images using dedicated surface - coils . 
prevalence of cn was determined in common carotid artery ( cca ) and internal carotid artery ( ica ) in consensus by two reviewers blinded to clinical information . results thirty seven cn in 28 arteries of 26 patients were identified . 
20 , 80336 munich , germany conclusion cn were found in 7.9% of arteries with carotid - plaques 2 mm by duplex - ultrasound ; prevalence was significantly higher in symptomatic arteries with 30% stenosis compared to asymptomatic with < 30% stenosis , suggesting that cn play a role in pathogenesis of ischemic stroke in a small subset of patients . keywords calcified nodules carotid arteries prevalence stroke purpose in western industrial countries atherosclerosis and its thrombotic cardiovascular complications , including myocardial infarction , sudden cardiac death and stroke , are among the most frequent causes of death as well as longterm disability [ 1 , 2 ]  . 
approximately , 2025% of ischemic strokes are due to large artery atherosclerosis and the majority of those are caused by ruptured atherosclerotic plaques at or close to the carotid bifurcation [ 3 ]  . 
therefore , it seems to be of paramount importance to get accurate information about the morphology and the composition , and thus the vulnerability of an atherosclerotic plaque , ideally before an ischemic event can occur . based on studies of culprit plaques [ 4 ] major and minor criteria were defined to assess a plaques vulnerability ( active inflammation , stenosis > 90% , endothelial dysfunc tion , intra - plaque hemorrhage , thin caps with large lipid / necrotic core , fissured plaque , endothelial denudation with or without superficial platelet aggregation and fibrin depo sition , glistening yellow plaques in angioscopy , cn , and outward remodeling )  . 
the pathobiology of atherosclerosis and its clinical consequences varies within the vascular tree , although the disease is a systemic one , that can 1 3 450 radiol med ( 2017 ) 122 : 449457 involve various vascular beds simultaneously [ 4 , 5 ]  . 
hence , markers of plaque vulnerability might not necessarily be identical between distinct vascular beds such as the coronary and carotid arteries . several recent histopathological and in vivo mri studies have confirmed an association of intraplaque hemorrhage [ 6 ] , thin / ruptured fibrous cap and necrotic core size [ 7 ] , thrombus formation and active inflammation with cerebrovascular symptoms in the carotid arteries . 
for other criteria of the vulnerable plaque , such as stenosis > 90% , positive remodeling and calcified nodules the significance of its presence in the carotid arteries has yet to be determined . although calcified nodules are defined as a minor criteria for vulnerable plaques and are known to cause 5% of coronary infarcts [ 8 ] only little data is actual available on the association of these nodules with cerebrovascular events in the carotid arteries . 
consequently calcified nodules are known to be a convex shaped hypointense area in white - blood ( tof ) and black - blood ( t1w , pdw and t2w ) images protruding into the lumen . therefore , the aim of this study is to identify the prevalence , distribution and clinical outcome of patients with calcified nodules in the carotid arteries . materials and methods study population this prospective study was conducted at our department between august 2008 and august 2015 . 
inclusion criteria were the presence of atherosclerotic plaques with 2 mm plaque thickness near or at the carotid bifurcation as determined by duplex ultrasound and ischemic symptoms in the territory of the anterior or middle cerebral artery . 
the subjects were considered to be symptomatic if they had an episode of a transient ischemic attack ( tia ) , stroke or amaurosis fugax in the right or left anterior circulation . 
stroke was defined as an acute dwi lesion and corresponding acute neurological deficit of > 24 h duration , tia was defined as an acute neurological deficit in the anterior circulation of < 24 h duration without dwi lesion on brain mri . 
exclusion criteria were bilateral infarcts on cmri , standard contraindications against mri , allergy to contrast agent , reduced renal function ( gfr glomerular filtration rate < 30 ml / min ) , former radiation therapy to head and / or neck and a surgery within 24 h prior to the carotid mri . the clinical data included age , gender and symptom status . 
in addition presence / absence of cardiovascular disease risk factors ( diabetes , hypercholesterolemia , smoking , arterial hypertension , coronary heart disease , positive family history of cardioor cerebrovascular events ) was documented . mri protocol patients with unilateral ischemic stroke underwent a carotid black - blood 3t - mri ( magnetom verio or magnetom trio , siemens healthcare , erlangen , germany ) with fat - saturated pre - contrast and post - contrast pdw - , t2wt1w - , and tof images using dedicated surface coils according to a previously published protocol [ 9 ]  . 
for improving the signal - to - noise performance and optimizing the spatial resolution , a dedicated 4 - channel surface coil ( machnet b.v. , eelde , netherlands ) for bilateral carotid scans was used . 
for tof slice thickness was 1 mm and for the remaining sequences 2 mm . image review satpoor , 2 sufficient , 3 good and 5 before the review two radiologists rated the image quality by a scale with 5 points ( 1 excellent )  . 
images with a quality isfying , 4 in t1w , t2w or tof 2 were excluded ( indicating a low signal - to - noise ratio or severe blurring that was adjusted to a motion of the subject )  . 
to assess intra - reader reproducibility of the presence / absence of calcified nodules , the initial independent review of the two reviewers was used for analysis , and one of the reviewers re - reviewed 62 arteries of 31 randomly selected patients 3 months after the initial review . 1 3 radiol med ( 2017 ) 122 : 449457 mr criteria for the identification of calcifications , calcified nodules and american heart association ( aha ) lesion type ( please see table 3 ) have been previously reported [ 10 , 11 ]  . 
to compare clinical demographics between patients with and without calcified nodules , we used the fishers exact test for categorical variables , and the unpaired t test with equal or unequal variances ( as appropriate ) for continuous variables . 
2 mr images of the right common carotid artery ( cca ) of an 81 - year - old female with ipsilateral ischemic stroke with 70% stenosis in the internal carotid artery . 
the calcified nodule ( arrowhead ) , which is protruding into the lumen is best seen on tof images although it is clearly visible on all other sequences as well [ asterisk infolding artifact ; tof ( a ) , t1w ( b ) , pd ( c ) and t2w ( d ) ] prevalence and distribution of calcified nodules detailed results of the distribution of calcified nodules in different patient subgroups are shown in table 2 . 
of the 37 calcified nodules , 22 ( 59% ) were found in the common and 15 ( 41% ) were found in the internal carotid artery . the majority of calcified nodules were found near or at the carotid bifurcation . 
figure 4 shows the distribution of calcified nodules in regard to their distance to the carotid bifurcation . calcified nodules , aha lesion types and symptomatic carotid stenosis in 31 out of 37 plaques ( 83.4% ) with calcified nodules the underlying lesion type according to the american heart association ( aha ) was classified as a type vii lesion , 3 underlying lesion types were classified as type iv / v with a large necrotic core covered by an intact fibrous cap and 3 underlying lesions were classified as complicated type vi plaques , with thrombus , hemorrhage and / or rupture of the fibrous cap . 
3 mr images of a calcified nodule in the left internal carotid artery ( ica ) of an 73 - year - old male with contralateral ischemic stroke without luminal stenosis . 
in total we were able to identify 37 calcified nodules in 28 distinct arteries of 26 distinct patients , resulting in a prevalence of 7.9% on an arterial level and of 14.5% on a patient based level . 
we found a higher prevalence of calcified nodules in the common compared to the internal carotid artery and a significantly higher prevalence of calcified nodules in arteries with 30% stenosis ipsilateral to ischemic stroke compared to the contralateral side . 
in addition we found a higher prevalence of calcified nodules in patients with hypercholesterolemia and hypertension . frequency and distribution of calcified nodules to the best of our knowledge there is no published data describing the frequency and distribution of calcified nodule in the carotid arteries and most of our knowledge fig . 
4 distance of calcified nodules ( cn ) to bifurcation in mm ( proximal of bifurcation ; 0 , bifurcation ; , distal of bifurcation ) of calcified nodules , its distribution and its clinical significance are based on histopathological and intravascular ultrasound ( ivus ) studies of the coronary arteries . 
 [ 13 ] found 314 calcified nodules in 250 distinct coronary arteries in table 3 american heart association ( aha ) lesion type and mr criteria for the identification of calcifications , calcified nodules conventional aha lesion type classification modified aha lesion type classification for mri type i : initial lesion with foam cells type iii : near - normal wall thickness , no calcification type ii : fatty streak with multiple foam cell layers type iii : preatheroma with extracellular lipid pools type iii : diffuse intimal thickening or small eccentric plaque with no type iv : atheroma with a confluent extracellular lipid core type v : fibroatheroma type ivv : plaque with a lipid or necrotic core surrounded by fibrous tissue with possible calcification type vi : complex plaque with possible surface defect , hemorrhage , or type vi : complex plaque with possible surface defect , hemorrhage , or thrombus type vii : calcified plaque type viii : fibrotic plaque without lipid core type viii : fibrotic plaque without lipid core and with possible small calcification thrombus type vii : calcified plaque calcifications 1 3 radiol med ( 2017 ) 122 : 449457 697 distinct patients , resulting in a prevalence of calcified nodules of 30% per patient 17% and per artery . 
the lower prevalence of cn in the carotid arteries on a per - patient basis might be due to the fact that we did not image the whole internal and common carotid artery , thus calcified nodules in the proximal common or distal internal carotid artery would have been missed . 
however , in the vast majority of patients carotid atherosclerosis is centered at the carotid bifurcation and therefore it is unlikely that a large number of calcified nodules have been missed due to the limited coverage available in our study . 
another possible reason for the lower prevalence of calcified nodules might have been that we used in vivo mri to visualize calcified nodules ; therefore , very small calcified nodules might have been missed . 
however , we used a similar minimal size for a calcification to be classified as a calcified nodule ( minimum diameter 1 mm ) and previous mr studies have suggested that a spatial reso0.5 mm2 is usually sufficient to identify callution of 0.5 cifications with an area > 1 mm 2 with good correlation to histopathology . there is no precise information about the pathogenesis of calcified nodules . 
based on histological data calcified nodules haveamong the subtypes of vulnerable plaques the greatest relative amount of calcification compared to the total plaque area and are thought to be associated with a healed fibroatheroma and / or recurrent intraplaque hemor rhage [ 8 ]  . 
we found no association of calcified nodules with plaque hemorrhage , since the calcified nodules in our study did not have an area of early or late subacute plaque hemorrhage in its vicinity , suggesting a minor role of recurrent plaque hemorrhage in the pathogenesis of calcified nodules in the carotid arteries . 
however , it has to be pointed out that old hemorrhages are hypointense on all pulse sequences [ 15 ] and , therefore , it is very difficult to distinguish old hemorrhages from calcified tissues by mri , leaving the door open for a role of old hemorrhages in the pathogenesis of these lesions . in our study , we found the highest prevalence of calcified nodules in arteries ipsilateral to ischemic stroke with 30% stenosis , suggesting that calcified nodules could play a role in the pathogenesis of ischemic stroke in a subset of patients . 
overall , 75% of symptomatic arteries with carotid stenosis exhibited features of vulnerable plaques by standard mr criteria and an additional 7.5% of atherosclerotic lesions would have been classified as such if presence of calcified nodules would have been taken into account . 
to date , the impact of this finding remains unclear and larger prospective studies are needed to evaluate whether calcified nodules provide additional value for the characterization of vulnerable plaques . furthermore , we found a higher prevalence of calcified nodules in patients with arterial hypertension and hypercholesterolemia . 
they observed , that there were consistently fewer non - culprit lesions major adverse cardiac events in the patient group with calcified nodules than in the non - calcified nodule group on a follow - up of 1 , 2 or 3 years , suggesting a minor role of calcified nodules on ischemic coronary events . 
to date , no data of the impact of calcified nodules in the carotid arteries on recurrent events is available . several recent cta studies have examined the role of carotid calcification and cardiovascular events . 
another retrospective study with 96 patients who underwent both cta and carotid mra found that adventitial calcification pattern in combination with maximum soft - plaque thickness by cta were highly predictive of plaque hemorrhage by mra [ 17 ]  . 
thus , several studies have examined the role of hard plaque thickness , speckled and adventitial calcification but to the best of our knowledge no study has looked into the role of calcified nodules in the carotid arteries by cta . as a limitation the number of calcified nodules identified in this study is relatively low and consequently no 1 3 456 radiol med ( 2017 ) 122 : 449457 definite association between calcified nodules and ischemic symptoms can be established . 
heber1 corinna storz1 fabian bamberg1 received : 9 june 2016 / accepted : 28 august 2016 / published online : 9 september 2016 italian society of medical radiology 2016 abstract advances of computational sciences over the last decades have enabled the introduction of novel methodological approaches in biomedical research . 
this so - called big data approach has recently found entrance into medical imaging and numerous epidemiological studies have been implementing advanced imaging to identify imaging biomarkers that provide information about physiological processes , including normal development and aging but also on the development of pathological disease states . 
the purpose of this article is to present existing epidemiological imaging studies and to discuss opportunities , methodological and organizational aspects , and challenges that population imaging poses to the field of big data research . keywords epidemiology imaging mri big data introduction technical developments over the past decades have enabled us to obtain abundant biological and socioeconomic information about single individuals and whole populations of interest . 
importantly , it has been realized that genetic data alone may not be sufficient to describe biological processes but that it has to be combined with phenotypic information to come to valid scientific conclusions . in this context , medical imaging can play a crucial role by providing detailed phenotypic data about an individuals anatomy and physiology as well as the early manifestation of morphological and functional disease states . 
one longterm goal is to achieve a detailed biological characterization of single individuals that can be used as a basis for preventive or therapeutic measures within the context of individualized medicine . 
however , to understand the biomedical significance of imaging phenotypes , it is necessary to have access to standardized and well - characterized data of a large number of individuals , ideally combined with relevant non - imaging data including genetic and metabolic information . implementation of imaging techniques in prospective , population - based cohort studies has been pursued early on and has resulted in improved understanding of complex disease processes as well as identification of novel imaging biomarkers as a precursor for overt disease states [ 2 ]  . 
prominent examples include the rotterdam study [ 3 ] , the framingham heart study ( fhs ) [ 4 ] , the multi ethnic study of atherosclerosis ( mesa ) [ 5 ] , the heinz nixdorf recall study [ 6 ] , the study of health in pomerania ( ship ) [ 7 ] , and the atherosclerosis risk in communities study ( aric ) [ 8 ]  . 
examples of novel imaging - based markers of risk include coronary calcification by computed tomogra phy ( ct ) [ 9 , 10 ] , assessment of left ventricular function / fibrosis or hepatic steatosis by magnetic resonance imaging ( mri ) [ 11 , 12 ] , and intima - media - thickness by ultrasound [ 13 ]  . 1 3 radiol med ( 2017 ) 122 : 430436 at the same time , magnetic resonance ( mr ) technology has progressed so rapidly that it offers non - ionizing , highresolution visualization of morphologic and functional processes without the need to administer contrast agent . 
its capability to perform examiner - independent , multi - region and whole - body mr scanning in clinical routine is a recent development [ 14 , 15 ] with a potentially high value for comprehensive phenotyping in a population - based imaging setting [ 2 ]  . utilizing these achievements for advanced , high - resolution , whole - body phenotyping , a number of epidemiological imaging studies have recently been initiated with the objective to create large imaging biobanks . 
in a recent position paper by the european society of radiology , imaging biobanks are defined as organised databases of medical images and associated imaging biomarkers ( radiology and beyond ) shared among multiple researchers , and linked to other biorepositories [ 16 ]  . the purpose of this article is to present existing epidemiological imaging studies implementing advanced , whole - body mr imaging and to discuss methodological and organizational aspects as well as challenges of these approaches . methodological requirements for large imaging studies in contrast to clinical imaging studies which focus on single individuals with specific questions , epidemiological imaging studies aim to collect imaging data from a large representative population using a broad protocol to establish the database that is statistically required for the extraction of meaningful information . 
to achieve this goal , imaging modalities used in such studies should meet certain requirements . primarily , safety aspects have to be considered as many epidemiological studies enroll representative samples from the general , primarily healthy population . 
finally , and most importantly for the data quality and thus scientific value , reproducibility , and standardization are main criteria for choosing the appropriate modality . taking into account these aspects , mri has emerged as the modality - of - choice for the majority of large , population - based imaging studies . 
the lack of ionizing radiation , the relatively good accessibility , and especially the combination of high anatomical detail and functional imaging techniques are advantages of mri compared to alternative techniques including computed tomography ( ct ) and sonography . 
the main drawback of mri in the context of population - based imaging studies is the relatively long examination time that limits the throughput of participants and thus results in comparably high cost . 
furthermore , standardization of mr examinations is a challenge and specific measures should be taken to guarantee comparable and constant image content . large epidemiological studies furthermore pose a challenge concerning data storage and distribution . 
data distribution is then performed either by a centralized system where participating researchers only have indirect access on the centrally stored data or a decentralized system where image data can be retrieved and stored at the individual research sites . 
table 1 shows an overview of these studies . table 1 characteristics of large epidemiological imaging studies using whole - body mr imaging epidemiological set up cohort size acquired data imaging studies ship cross - sectional / longitudinal ~10 , 000 biometric , clinical , biochemical , genetic whole - body mri , ultrasound cross - sectional biometric , clinical , biochemical , genetic whole - body mri ( in 30 , 000 participants ) uk biobank cross - sectional biometric , clinical , biochemical , genetic whole - body mri , ultrasound , dxa 200 , 000 100 , 000 1 3 432 the ship study the ship study ( study of health in pomerania ) was one of the first large - scale epidemiological studies that systematically included whole - body mri as part of the study protocol [ 16 ]  . 
in contrast to many other studies , the ship study provides not only cross - sectional but also longitudinal information of follow - up studies in part of the included cohorts . 
 experiences that were gained in the ship study strongly influenced the design of recent studies including the gnc study and uk biobank . several hundreds of studies and publications have been published using data from the ship study . 
among others , associations between imaging phenotypes and cardiometabolic risk could be demonstrated [ 21 , 22 ]  . the gnc study the gnc ( german national cohort ) study is a largescale epidemiological study aiming to identify genotypic and phenotypic features associated with health and disease [ 23 ]  . 
over 20 mio biological samples are expected to be collected in the course of the study that will be stored in a dedicated biobank in southern germany . as part of the gnc study , whole - body mr examinations will be performed in a sub - cohort of 30 , 000 participants beginning in 2015 [ 19 ]  . 
the mr imaging protocol consists of neuroradiological , cardiovascular , musculoskeletal , and whole - body studies that are acquired within one hour of examination time . in a dedicated pre - study that examined the influence of different scanner types on image - derived parameters , it was found that variations were considerably lower when using a single scanner type compared to a multi - scanner multivendor approach [ 24 ]  . 
over a long time period of approximately 25 years about 500 , 000 volunteers will be examined in a cross - sectional setting acquiring demographic , biometric , and functional data as well as biological samples [ 26 ]  . 
the imaging protocol includes ultrasound examinations , dual energy x - ray absorptiometry , and a whole - body mri scan covering neuroradiological , cardiovascular , and musculoskeletal aspects [ 18 , 27 ]  . access to acquired data is granted to researchers meeting the criteria of scientific quality and public interest . 
similar studies will also be possible combining imaging data and genetic data in the future using a radiogenomic approach . data analysis a major challenge of population - based imaging studies is the analysis and interpretation of acquired data . 
this challenge is not only caused by the enormous amount of acquired data but also by the high complexity of acquired multidimensional and multimodal imaging data ( big data ) [ 31 ]  . in general , imaging protocols are not optimized for a specific question but rather aim to provide a general anatomic and physiologic phenotypization of participating individuals . 
as an alternative , non - enhanced sequences have to be used for the purpose of assessing vascular morphology and the validity of such an approach should be examined in comparison to established contrast - enhanced sequences in a small population , potentially outside the main study . in contrast to conventional clinical imaging studies , where patient populations are relatively small , the extent of many epidemiological studies in terms of included participants reaches a magnitude where manual or visual analysis by human readers becomes very time - consuming or even impossible . 
to this end , fully automated or semi - automated algorithms have been developed for the analysis of specific image contents including organ segmentation [ 32 , 33 ] , assessment of adipose tissue distribution [ 34 ] or automated assessment of image quality [ 35 ]  . 
still , further developments in the field of automated image analysis are necessary to be able to fully harvest the large treasure of information that may be hidden in the acquired imaging biobanks . furthermore , it is of utmost importance to include nonimaging biomarkers into the process of analysis to create a frame of reference and to put imaging data in the correct context of interpretation . 
especially in cross - sectional studies , where no follow - up data are available for the assessment of outcomes , non - imaging markers can help to understand the physiological significance of identified patterns in the respective imaging studies . 
this requires a close collaboration between experts in numerous fields including radiologists , biologists , epidemiologist , and statisticians . as a side - effect , the demands on data analysis in epidemiological imaging studies will potentially initiate the development and application of novel research strategies and data extraction tools that can be used not only within these studies but also in routine clinical studies for the benefit of single patients . 
for example , the emerging methods of radiomics and radiogenomics are already conceptually incorporated in epidemiological studies [ 36 ] and may open new perspectives on imaging data . harmonization between studies as already mentioned above , data homogeneity and standardization plays a central role for the assurance of good data quality that guarantees valid , reliable , and reproducible results . 
to overcome this problem and to identify geographical and ethnic factors influencing imaging phenotypes , it would be of great interest to compare the results of different studies that are performed in different populations . 
this is specifically important for imaging studies that are generally not standardized in the same way as genetic or laboratory tests . imaging international population - based as a solution to this problem , it would be important to harmonize imaging protocols between the major national and studies . 
 challenges of populationbased imaging due to their enormous size , epidemiological studies come with many challenges , especially concerning infrastructure , data acquisition , and data handling . as already mentioned above , standardization of data is a specific challenge of population - based imaging studies , especially when mri is used as the main modality . 
 depicted are cine ssfp sequences ( top left three - chamber view , top right four - chamber view , bottom left two - chamber view , bottom right axial orientation )  . 
these sequences are part of the imaging protocol in the ship study , uk biobank and the gnc study evenly important , continuous data quality assurance is a prerequisite for the generation of valid data and thus useful scientific results . 
current approaches for quality control in imaging studies mostly combine statistical analyses of image properties ( such as signal homogeneity , noise , etc . ) with quality analysis by human observers , either technicians at the acquisition sites or radiologists [ 25 ]  . 
first attempts have been made to automate quality assurance by replacing human observers with machine - learning algorithms [ 35 ]  . another specific challenge of epidemiological imaging studies is the process of dealing with incidental findings . 
to provide a prompt report of severe findings , all acquired images have to be analyzed within a short time frame after acquisition , which is timeconsuming and organizationally challenging . 
again , automated analysis tools may help to optimize this process in the future . 1 3 radiol med ( 2017 ) 122 : 430436 conclusion large - scale population - based imaging studies have introduced a novel scientific approach in medical imaging by acquiring and analyzing large amounts of data to identify biomarkers of health and disease . 
overcoming these challenges , it can be expected that pioneering biomedical discoveries will be made that in turn can be implemented in the clinical routine in the context of a personalized preventive and therapeutic medicine . compliance with ethical standards conflict of interest author s . 
anatomical , physiological and pathological differences between pediatric and adult airways , rarity of diseases and the necessity of a prompt action even in a scenario of emergency or urgency represent additional difficulties to face [ 2 , 3 ]  . 
diagnostic and therapeutic procedures of airway disease require close interaction between all clinicians involved : pediatric specialist , pneumologist , thoracic surgeon , cardiac surgeon , gastroenterologist , otorhinolaryngologist , neurologist , anaesthesiologist and radiologist [ 4 ]  . 
at giannina gaslini institute ( genova , italy ) , the pediatric multidisciplinary airway team is the ideal setting in which the radiologist chooses the appropriate imaging technique and presents its results . 
in a multidisciplinary conference , the reasoned integration between non - invasive , mini - invasive and invasive diagnostic techniques is the key to provide effectiveness of treatment to patients affected by airway disease avoiding misapplication . 
the knowledge of the features and potentiality of each imaging technique against relative disadvantages are mandatory for the radiologist involved with airway imaging . 1 3 420 imaging techniques chest xray a systematic imaging approach to airway lesions begins with anteroposterior and lateral radiographs of the neck and chest ( x - ray )  . 
in rare , and resounding cases is possible to determinate the location ( nasopharynx , oropharynx , hypopharynx , larynx , trachea ) of the anomalies of aero - digestive tract , through the lateral projection of x - ray . 
in any case , the chest x - ray is useful to evaluate pulmonary parenchyma , even at the bed side for a follow - up evaluation after surgery , with low radiation dose [ 8 ]  . 
x - ray is broadly indicated to evaluate the extremity of the endotracheal tube , the length of tracheal cannula and to exclude post - operative complications as pneumothorax , pneumomediastinum , emphysema of the neck , pleural fluid collection . 
furthermore , x - ray is indicated as a first - line imaging technique to exclude radiopaque foreign body in pediatric airway [ 9 ] , before ct scan , in the selected case . radiol med ( 2017 ) 122 : 419429 tracheobronchography and fluoroscopy ( tbgtbf ) tbf is a mini - invasive exam performed under general anesthesia , widely available in every radiological facility . 
after the introduction of a minimum dose ( 24 ml ) of hydrosoluble contrast medium ( visipaque 270 , off - label application ) in trachea , tbf allows a morphological and dynamic evaluation of the airways , particularly useful to detect the collapse of the tracheal wall during expiration and to determine the longitudinal extent of tracheomalacia [ 10 , 11 ]  . 
c tbf guided tracheoplasty and bioabsorbable stent placement 1 3 radiol med ( 2017 ) 122 : 419429 esophagogastrography and fluoroscopy ( eggegf ) in uncooperative patients , egg and egf are performed without general anesthesia , holding the patient in a immobilization air - insufflate mattress . 
the fluoroscopy starts concurrently with the oral administration ( baby bottle ) of a small amount ( 10 ml ) of uroangiographic contrast medium ( visipaque ) , in anteriorposterior and lateral projection ( 90 )  . 
when tracheo - esophageal fistula and esophageal atresia are suspected , egg and egs are always important to evaluate the gap between the esophageal extremity with the perspective of surgical intervention , and to study the continence of les in the post - operative phase [ 16 , 17 ]  . 
uvf can support the decision of the suitable tracheal tube , and the evaluation of edema of the larynx , in order to support the intubation procedure [ 21 ]  . computed tomography ( ct ) ct has a key role in diagnostic process of disease affecting the airways [ 22 ]  . 
each exam is performed with a spiral monophasic scan covering neck and thorax after venous injection of iodinated non - ionic contrast medium , with low osmolarity ( iomeron 300 , 2 ml / kg ) by an automatic pump ( 23 ml / s ; empower cta , ezem , lake success , usa )  . 
2 at full abduction , asymmetrical opening of vocal folds , and flaccid left fold in a patient with left vocal fold paralysis occurred after surgery ( patent ductus arteriosus ) fig . 
ct scan demonstrated a tracheal stenosis due to brachiocephalic trunk compression ( arrow ) tracheomalacia and life support endotracheal tube , some authors propose to perform the ct scan with controlled ventilation technique , to delimitate the tracheal segment affected with higher accuracy [ 29 , 30 ]  . 
the last generation of ct scanners allows the dynamic evaluation of trachea and main bronchi ( cine ct ) through expiratory phases , demonstrating the presence and extension of tracheobronchomalacia , as well as the study of pulmonary parenchyma and vascular structures in a single exam [ 31 ]  . 
the main workstation automatically elaborates two isotropic datasets , with filters and windowing optimized for pulmonary parenchyma and mediastinu the dataset created is transmitted to digital archive and to satellite workstation for 2d multiplanar reformations and 3d images . 
in patients with magnetic resonance ( mri ) mr exam , which is radiation free and non - invasive , is indicated to study mediastinal vessels with high accuracy in pediatric patient [ 32 ] ( table 1 )  . 
in uncooperative patients , general anesthesia is necessary ( under the age of 7 )  . mr can be preferred to ct to demonstrate the presence of vascular ring or pulmonary sling when functional cardiac information or serial studies are requested [ 33 ]  . 
the high contrast resolution of mri allows the tissue characterization of the most common masses as cervical lymphangioma , venous vascular malformation , neuroblastoma , duplication cyst , lymphoma , teratoma , and can determine with accuracy the relation with the airway [ 35 ]  . 
bolus track technique cine real time free breathing pd t1 black blood cardiac triggering tse t2 black blood cardiac triggering short t1 inversion recoverystir tr 4000 , te 50 tse t1 - weighted tr 500 , te 16 fig . 
6 mri , axial tse t1 ( a ) , tse t2 ( b ) , and sagittal stir ( c ) demonstrate the presence of a cervical complicated duplication cyst radiation exposure , we still prefer tbf , especially when a treatment plan is necessary ( i.e. , measurements of bioabsorbable stent )  . optical coherence tomography ( oct ) oct measures backscattered light intensity using coherence interferometry to construct topographical images of complex tissue . 
some authors are studying improved airway applications based on the diagnostic microstructural potential of oct to detect epithelial , mucosal , cartilaginous , glandular tissues and relative changes in neoplastic , malformative and inflammatory lesion [ 43 ]  . 
in our opinion , the broad clinical adoption of oct is limited because of the poor number of scientific papers focused on pediatric airway and the high cost of the instruments . clinical indications and imaging congenital malformations of the larynx laryngomalacia represents the commonest laryngeal congenital anomaly and the most frequent cause of stridor in the newborn [ 44 ]  . 
it consists in an inward collapse of 1 3 424 radiol med ( 2017 ) 122 : 419429 injury after cardiovascular , mediastinal , and esophageal surgery [ 53 ]  . 
for all cases of vcp , the diagnosis is based on dynamic laryngoscopy ( with flexible or rigid instruments ) , in selected cases integrated with electromyography evaluation of the vocal cords . 
in both unilateral and bilateral vcp , a spontaneous resolution may occur after several months or even years . the only non - invasive diagnostic technique available to study vocal cord function is the ultrasonography , in particular , for unilateral cases . 
the ultrasound findings in case of vcp are : abnormal mobility , hyperechoic air - column band of the glottis rima during phonation , flaccid vocal fold , and asymmetry of the glottal structures [ 54 ]  . 
further limitations of ultrasound in bilateral vcp are : the impossibility of comparison with the contralateral normal movements , and the paradoxical movements of the paretic vocal cords due to the bernoulli effect ( vocal cords adducted during inspiration )  . 
the bernoulli effect can mimic normal vocal cord movements , but the observation of the movement in relation with the respiratory phase and the experience of the operator help to achieve the correct diagnosis . congenital subglottic stenosis ( css ) is the third commonest congenital anomaly of the larynx ( 1015% of cases ) and is the most frequent indication to the tracheotomy during the first year of life . 
css is due to a congenital malformation of the cricoid cartilage ( cartilaginous anomaly ) , while the more frequent acquired subglottic stenosis ( ass ) is usually due to a traumatic injury ( for example , post - intubation stenosis ) , and involves soft tissues . 
ct is indicated after the endoscopy ( and not instead of it ) in two cases : to determine the length of the stenosis when the airway is too narrow for the endoscopic evaluation and to rule out associated anomalies . subglottic hemangioma ( sh ) is an uncommon benign vascular tumor , often associated with other cutaneous hemangiomas , sharing with them the clinical history ( phases of progression , stabilization and regression , and 50% of complete resolution at 5 years of age ) and the therapeutic options ( propranolol )  . 
a axial view of the tracheal wall and longitudinal reformation , b clearly depicts the cartilagineous rings ( arrows ) supraglottic structures during inspiration , with jugular and subcostal visible retractions . 
the natural history is characterized by the onset at around 24 weeks of life , a progression during the first 8 months , then a gradual improvement until spontaneous resolution in most cases at around 18 months of life [ 46 ]  . 
if laryngomalacia is isolated , the diagnosis is easily achieved by a dynamic fiberoptic evaluation , usually associated with a rigid laryngotracheoscopy to rule out other associated conditions , while radiological investigations have a limited value and are not indicated [ 47 ]  . 
mr is limited by the low spatial resolution and lack of dynamic sequences for the study of the upper respiratory tract . the second most frequent congenital airway anomaly is vocal cord palsy ( vcp ) ( 1520% ) [ 48 ]  . 
when vcp is not caused by a traumatic injury to laryngeal recurrent nerve , the vocal cord dysmotility is due to a dysfunctional innervation without signs of complete muscular tone loss or denervation [ 49 ]  . 
unilateral vcp can be due to a peripheral nervous 1 3 radiol med ( 2017 ) 122 : 419429 biphasic stridor or croup episodes typically between 2 and 4 months of age [ 57 ]  . 
 mr can be indicated in case of lesions of large size or not responding to pharmacological treatment , in order to study its potential extension into the mediastinum [ 58 ]  . ductal cysts ( dc ) is the most frequent pharyngo - laryngeal cyst and develops in subglottic region , larynx or pharynx , from the obstruction of the muciparous gland ducts . 
 saccular cyst ( saccular dilatation and herniation filled with mucus ) and laryngocele ( saccular dilatation and herniation filled with air ) can develop at the same site of dc and must be differentiated from thect scan is useful to detect laryngocele [ 59 ] , but cannot differentiate between saccular cysts and dc . 
ltc can be associated with esophageal atresia with tracheo - esophageal fistula , gastroesophageal reflux , tracheobronchomalacia , and present with respiratory symptoms related to the severity of the defect : dyspnea , cough , cyanosis , aspiration [ 60 ]  . 
contrast study of the pharyngeal and laryngeal tract with an iso - osmolar contrast ( not barium ) as previously described may show a passage of contrast from the esophagus into the airway , even if false - positive results can occur in other conditions ( pharyngo - laryngeal incoordination , laryngomalacia )  . 
airway endoscopy allows definitive diagnosis of cleft and the definition of its length [ 61 ]  . congenital malformations of trachea tracheomalacia ( tm ) and tracheobronchomalacia ( tbm ) represent the commonest congenital tracheal anomaly ( 50% of all congenital tracheal anomalies ) and are defined as a softness of the cartilage rings of the trachea and / or bronchi , sometimes associated with an abnormally hyperrepresented pars membranacea , with a consequent collapse of the airway . 
while diffuse tbm is usually primitive , focal tbm can be more frequently due to compression by mediastinal masses ( i.e. , cervical lymphangioma , vascular malformation , neuroblastoma , lymphoma , teratoma , esophageal duplication cystic ) , vascular rings ( aberrant subclavian artery , double aortic arch , right aortic arch , pulmonary sling ) or extrinsic vascular compression ( brachiocephalic artery , dilated pulmonary artery , complex cardiopathy ) [ 2325 ]  . 
however , ct ( or mri ) must be performed to complete the evaluation of tm associated with vascular ring , or tbm with pulmonary sling , when a pulsatility of the tracheal wall is pointed out by endoscopy . 
as this technique requires cooperation , in non - collaborative patient intubation under general anesthesia and dynamic variation of ventilation pressures have been proposed [ 63 ]  . esophageal atresia with tracheo - esophageal fistula ( ea and tef ) are the most common communication between the esophagus and the airway . 
in 60% of cases , tef is associated with tm at the level of the tracheal segment in proximity to the tef , due to the incomplete development or weakness of the transverse trachealis posterior muscles [ 65 ]  . 
in case of ea with tef , the radiography at birth shows gastrointestinal abdominal air and the upper esophageal stump at the mediastinal or neck level . in ea type v ( isolated tef ) , egf can show the tef in most cases . 
in our experience , in cases with negative or not conclusive egf , ct does not add any useful information . congenital tracheal stenosis ( cts ) is a rare anomaly , characterized by the presence of complete cartilaginous rings and consequent narrowing of the tracheal lumen . 
 according to the morphology of the stenosis , cts can be classified into focal stenosis ( 50% of cases ) , generalized stenosis ( 30% ) or funnel shape stenosis ( 20% at the inferior tracheal segment ) [ 66 ]  . 
in our opinion , however , a classification considering not only the extension of the stenosis along the trachea , but also the bronchial morphology and the possible stenotic involvement of the bronchi , gives more useful pre - operative information [ 67 ]  . 
given that the resistance to laminar airflow increases linearly in propor tion to length of stenosis and fourfold relative to calibre decrease , a tight stenosis produces worse symptoms compared with a long and moderate stenosis . 
a different condition classified in cts group is the tracheal web , extremely rare , typically made by thin , entangled membranes detectable by ct , and normal cartilaginous ring [ 69 ]  . 
a complicated , partially air - filled bronchogenic cyst in right hypogenetic lung syndrome only few case reports are published on this topic [ 70 ] ; nevertheless , we expect more comprehensive studies in larger population . tracheal bronchus ( tb ) is often an incidental finding in an asymptomatic patient , without surgical indication , even though the small calibre of the airway and retained secretions may produce expiratory stridor and / or bronchiectasis , atelectasis and recurrent infections . 
indications to ct examination include the direct identification of the tb , potential cardiac malformations associated , and evaluation of pulmonary parenchyma . congenital tracheal atresia ( or agenesis ) ( cta ) is a rare condition , incompatible with life . 
the integration between tbf , tbg , and egf can be indicated to delineate the tracheobronchial anatomy and its relation with the esophagus , in order to plan the treatment . congenital bronchial atresia ( cba ) is determined by atresia or obstruction of a segmental or sub - segmental bronchus with normal distal airway . 
although the majority of patients with bronchial atresia are asymptomatic and the diagnosis is made on chest radiographs performed for other reasons , some authors report a history of recurrent pneumonia . 
this should not be mistaken for a nodule or for lung abnormalities such as lobar emphysema or intralobar sequestration with air trapping [ 2372 ]  . bronchogenic cyst ( bc ) is congenital lesion filled with mucoid content that originate from the embryonic foregut and may be located in the mediastinal space ( 60% ) , in the middle third of the lung ( 30% ) or , less frequently , in the lower neck ( 10% )  . 
a provisional diagnosis of bronchogenic cyst should be considered whenever a wellcircumscribed lesion with fluid density is identified in the middle third of the mediastinum adjacent to the bronchial tree . 
old cyst can have a high protein content and , thus , a slightly increased density with high signal intensity in t1 and lower signal intensity in t2 . 1 3 radiol med ( 2017 ) 122 : 419429 fig . 
b lung window demonstrates right valve - mechanism hyperinflation acquired stenosis of larynx and trachea laryngeal or tracheal post - intubation stenosis ( lis , tis ) is an operative complication , which occurs in 0.93% cases of intubated patients . 
predisposing factors are related to patient ( laryngeal conformation and size , gastroesophageal reflux ) , to tube ( excessive size , poor biocompatibility ) , maneuver , assistance ( insufficient sedation ) and prolonged intubation . 
ct exam is indicated to evaluate the longitudinal extension and the severity of stenosis in patients with tis . neoplastic lesion of larynx , trachea and bronchi ( papillomatosis , hemangioma , rare epithelial or connective tissue tumors ) have benign characteristics in 1 3 428 radiol med ( 2017 ) 122 : 419429 conflict of interest all the authors declare that they have no conflict of interest . compliance with ethical statements no animals were involved . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
informed consent was obtained from all individual participants included in the study . radiol med ( 2017 ) 122 : 464471 doi 10.1007 / s11547 - 017 - 0741 - y radiotherapy synchronous bilateral breast cancer irradiation : clinical and dosimetrical issues using volumetric modulated arc therapy and simultaneous integrated boost alba fiorentino1 rosario mazzola1 stefania naccarato1 niccol giajlevra 1 sergio fersino1 gianluisa sicignano1 umberto tebano2 francesco ricchetti1 ruggero ruggieri1 filippo alongi1 received : 22 august 2016 / accepted : 6 february 2017 / published online : 21 february 2017 italian society of medical radiology 2017 abstract objectives the aim of the present retrospective analysis was to evaluate dosimetric parameters , feasibility and outcome for synchronous bilateral breast cancer ( sbbc ) patients treated with adjuvant radiotherapy ( rt ) by volumetric modulated arc therapy ( vmat )  . methods from september 2011 to april 2016 , 1100 breast cancer ( bc ) patients were referred to our institution to receive adjuvant breast rt , and those with sbbc were selected for the present analysis . 
a total dose of 50 gy in 25 fractions was prescribed to the planning target volume of the whole bilateral breast ( ptvbn ) with or without the supraclavicular and infraclavicular nodes , while a total dose of 60 gy in 25 fractions was prescribed to the surgical bed ( ptvboost )  . 
 several vxgy and dx% parameters were analyzed for the ptvs , together with conformity and homogeneity indexes ( ci , hi ) , and for the critical organs at risk ( oars ) , lungs and heart first . results with a median follow - up of 24 months , no acute or late side effects more than grade 2 were observed . 
in fact , several experiences did not show 1 3 radiol med ( 2017 ) 122 : 464471 clear differences in terms of outcomes between sbbc and unilateral bc [ 2 , 3 ]  . 
consistently , sbbc treatment options are the same of unilateral bc : neoadjuvant or adjuvant chemotherapy , mastectomy or breast conservative surgery ( bcs ) and adjuvant radiotherapy ( rt )  . 
moreover , postoperative rt , after bcs , has shown a decreased risk of local recurrence , providing a 45% survival gain [ 1 , 47 ]  . three - dimensional conformal rt ( 3d - crt ) represents the most common approach after surgery , consisting of whole breast irradiation ( wbi ) after bcs or chest wall irradiation after mastectomy with or without regional nodes . 
 3d - crt is generally delivered by two tangential fields for each breast with a total dose of 4550 gy / 1.82 gy per fraction [ 1 , 810 ]  . 
moreover , to reduce the risk of nodal recurrence , regional nodal irradiation has been suggested in case of ( 1 ) node positive after neoadjuvant chemotherapy , ( 2 ) locally advanced cancer , ( 3 ) inflammatory bc and ( 4 ) presence of more than three positive nodes [ 1 , 4 ]  . in daily clinical practice , 3d - crt technique is typically affected by the risk of over - / underdosage at the field junctions , increased dose heterogeneity over the whole breast , too large portions of the heart and the lungs which cannot be dosimetrically spared . hence , highly conformal rt remains critical to achieve the required target dose coverage while assuring adequate normal tissue sparing [ 11 , 12 ]  . 
the advances in rt , including intensity - modulated rt ( imrt ) or volumetric modulated arc therapy ( vmat ) , represent a suitable option that provides high - precision delivery with adequate sparing of the organs at risk ( oars ) [ 1113 ]  . 
thus , the use of vmat or imrt was strongly suggested for unfavorable situations , such as sbbc [ 1117 ]  . in our institution vmat is commonly adopted for sbbc patients . 
thus , the aim of the present retrospective analysis was to evaluate dosimetric parameters , feasibility and outcome for sbbc patients treated with adjuvant rt by vmat . materials and methods from september 2011 to april 2016 , 1100 bc patients were referred to our institution to receive adjuvant breast rt , and those with sbbc were selected for the present analysis . 
a total of 16 patients , in 98% of which ones an early bc was diagnosed , were identified : 15 patients received bcs and 1 a modified radical mastectomy on both sides . 
 patient characteristics are shown in table 1 . planning the patient was immobilized in a supine position on a posi - board frame ( civco inc . ) and a planning computed tomography without intravenous contrast media ( 3 mm thick slice ) was acquired . 
a total dose of 50 gy in 25 fractions was prescribed ( dp ) to both ptvbn , with or without the supraclavicular and infraclavicular nodes . a ctvboost , including tumor bed , was defined for both sides , if necessary . 
 preoperative imaging , operative report ( including the results of histopathology ) and the position of the surgical incision were reviewed to define the expected position of the surgical bed . 
in cases where uncertainty existed regarding the anatomical region of the surgical cavity , radiopaque catheters and markers were placed to identify palpable breasts , scars and skin markers on the ct images . 
to compensate intra - fraction respiratory motion , a 1 - cm virtual bolus was added interiorly to the body and the final plan re - optimized to extend the apertures of the leaves out of the body . 
to compensate intrafraction respiratory motion , a 1 - cm virtual bolus was added to the body and the final plan re - optimized on a 0.8 - cm ( anteriorly and laterally ) expanded ptvbn with the goal to extend the apertures of the leaves out of the body . 
the homogeneity index ( hi ) , here defined as the range of intra - target dose variability rescaled to a reference target dose [ 20 ] , was evaluopt and ptvboost . 
the conformity index ( ci ) was defined as the ratio of the volume enclosed by the prescribed target dose over the same target volume , consistently with the original definition by rtog [ 22 ] and was computed for ptvboost only . 
an axial slice with dose color wash between 10 and 60 gy on the left ( a ) , and a sagittal reconstruction with doses between 47.5 and 60 gy on right ( b ) are reported 1 3 radiol med ( 2017 ) 122 : 464471 organs at risks oars were contoured according to rtog guidelines [ 19 ]  . 
the constraints on the oars for planning approval were derived from those ones we use for monolateral breast plus supraclavicular nodes : v20 < 10% and dmean < 10 gy to the ipsilateral lung , dmean < 5 gy to the heart , d1cc < 30 gy to the esophagus and d0.1cc < 30 gy to the spinal cord planning - risk - volume ( prv ) , as obtained by a 4 - mm isotropic expansion from the contoured spinal cord . 
in other words , we attempted to assure v20 < 15% and dmean < 15 gy to the total lung , and dmean < 7.5 gy to the heart . statistical analysis in order to summarize the most relevant dosimetric parameters , descriptive statistics were performed . 
for overall survival , death regardless of cause or the last follow up for censoring purpose ( if the patient was alive and still being followed at the time of analysis )  . 
two groups were defined to determine whether there was a difference in terms of heart dose : before darbys study , called as group a and after darbys study , called as group b . 
 5 / 16 patients ( 31.25% ) did not experience any grade of acute side effects , 8 / 16 had g1 skin toxicity , while 3 / 16 ( 18.75% ) experienced g2 skin toxicity . 
with a median follow - up of 24 months , no grade 2 or superior late side effects were registered . moreover , all patients are alive without any sign of disease . 
no local recurrences or metastases were observed . dosimetric results target coverage 355 cm3 and 32 353 cm3 and 22 the range of minimum and maximum values of rt doses was 5060 gy . 
in table 2 , the values of the conceived dn% ( minimum dose to n% of the structure ) and vm ( percentage of the structure receiving m ( gy ) ) dose - volume metrics for both right and left ptvs are reported . 
adequate target dose coverage resulted , being the average v95% dp greater than 95% for both ptvbn and ptvboost on both sides , together with being the average d2% lower than 107% dp for the left ptvboost and lower than 108% dp for the right ptvboost . 
 despite the reduction of acute skin toxicity , the routine use of imrt / vmat in bc irradiation has not been proposed mainly due to the lack of clinical advantages in terms of local recurrence and survival [ 1 , 1113 ]  . due to the limitations of sbbc irradiation , it is well recognized that 3d - crt is usually not adequate for its large target dose heterogeneity and its limited oars sparing . although symptomatic radiation pneumonitis ( rp ) is a rare side effect for unilateral bc , in case of sbbc , rp risk is higher due to the irradiation of larger volumes . 
several factors influenced the incidence and severity of rp : age , pre - existing lung disease , smoke , genetic predisposition , volume of irradiated lung , rt dose and fractionation and concomitant use of tamoxifen [ 2427 ]  . concerning rt - related heart side effects , the radiobiology of cardiac damage has not been established well . 
nevertheless , it is not well recognized whether the cardiovascular effects are related to a high rt dose to a small volume or , on the contrary , to a low average dose to the whole heart [ 28 , 29 ]  . 
estimated a linear correlation between the average heart dose and subsequent significant coronary events : the increased risk to the heart resulted 7.4% per added gy to dmean [ 23 ]  . 
the long - term risk of ischemic heart disease following wbi has been also correlated with several patientfactors , including body mass index , diabetes mellitus , dyslipidaemia , tobacco / alcohol and chemotherapy ( anthracyclines , trastuzumab and tamoxifen ) [ 30 , 31 ]  . the use of modulated rt techniques , such as imrt , vmat and helical tomotherapy ( ht ) also , appeared to be useful in the sbbc setting [ 1 , 1117 ]  . 
this is predominantly due to the lack of clinical advantages of imrt techniques comparing to 3d - crt , in terms of risk of recurrences or advantages in survival [ 32 ]  . 
in sbbc irradiation some criticisms could affect 3d - crt performances such as the lacking of conformal and steep dose gradient between breast and boost volume , with subsequently excessive dose to whole breast ; imrt or vmat can improve the target dose coverage with acceptable cosmetic outcomes and skin toxicities [ 11 , 33 ]  . 
a criticism concerning imrt / vmat delivery could be represented by the higher low - dose exposure of the organs a risks ( oars ) comparing to 3dcrt [ 34 ]  . 
in the setting of early breast cancer irradiation after conserving surgery , several in silico analyses showed a significant advantage of imrt compared to 3dcrt in terms of target dose coverage , integral dose and dose to oars [ 3437 ]  . previous studies reported the feasibility of imrt / vmat / ht in sbbc irradiation [ 1417 , 3840 ]  . 
hence , at our knowledge at least , the present study is the first analysis of sbbc patients treated by vmat , where both dosimetric parameters and tolerability / clinical outcome are reported . for our sbbc patients vmat plans resulted in adequate target dose coverage , with an appreciable dose sparing of the critical oars ( i.e. : lungs , heart )  . 
according to target dose coverage , the average v95% dp was greater than 95% for both ptvbn and ptvboost on both sides , while the average d2% was lower than 107% ( 108% ) dp for the left ( right ) ptvboost , respectively . 
interestingly , the average inter - patient ci values both for the left and for the right ptvboost were compliant with the suggested ranges of values from rtog guidelines for brain srs [ 22 ]  . 
according to the oars sparing , a dmean of 34 gy and v25 gy < 10% to the heart are considered acceptable values for unilateral breast irradiation with respect to the risk of long - term cardiac mortality [ 41 ] by 3d - crt as reported from darby et al . 
for the lungs , a v20 gy less than 30% and a dmean lower than 13 gy were recommended to limit the risk of rp below 20 and 10% , respectively . 
 [ 15 ] evaluated the feasibility of vmat in 2 sbbc cases , who received adjuvant breasts rt with a total dose of 50 gy in 25 fractions without sib . 
the dose prescription was 50 gy in 25 fractions to ptv breasts plus 15 gy in 6 fractions as sequential boost on the tumor bed , but with ht 61 gy in 25 fractions to the ptvboost were concomitantly delivered . 
the best dose sparing of the lungs and the heart was achieved by the ht - sib , when lungs dmean 4.7 gy together with v25 gy 7.4 gy , and dmean 3.5% to the heart resulted [ 16 ]  . kaidar - person et al . 
patients were treated with simultaneous bilateral breasts / chest - wall and bilateral or unilateral regional nodes , including internal mammary nodes . 20 gy and v 25 gy considering that the irradiated volumes were larger than in the present analysis , the authors showed increased oars dose involvement : lungs v20 was 29% . 
furheart dmean thermore , significant side effects were reported : in acute setting , dysphagia ( 5 / 9 ) , fatigue ( 4 / 9 ) , nausea and weight loss ( 1 / 9 ) and skin desquamation ( 9 / 9 ) ; in late setting , pneumonitis ( 1 / 6 ) , elevated liver function tests ( 1 / 6 ) and sternal osteonecrosis ( 1 / 6 ; in patient with prior sternal surgery )  . 
in the present analysis , with a median follow - up of 24 months ( 348 months ) , only 3 / 16 ( 18.7% ) patients , 1 3 470 radiol med ( 2017 ) 122 : 464471 who had received also supra - infraclavicular nodal irradiation , experienced acute g1 dysphagia , while no grades of late side effects were registered . conclusion despite the limitations of the study ( small sample size , retrospective analysis ) , the here reported results , with a follow - up of 2 years , show the feasibility , tolerability and safety of vmat in the treatment of sbbc patients . 
heber1 corinna storz1 fabian bamberg1 received : 9 june 2016 / accepted : 28 august 2016 / published online : 9 september 2016 italian society of medical radiology 2016 abstract advances of computational sciences over the last decades have enabled the introduction of novel methodological approaches in biomedical research . 
this so - called big data approach has recently found entrance into medical imaging and numerous epidemiological studies have been implementing advanced imaging to identify imaging biomarkers that provide information about physiological processes , including normal development and aging but also on the development of pathological disease states . 
the purpose of this article is to present existing epidemiological imaging studies and to discuss opportunities , methodological and organizational aspects , and challenges that population imaging poses to the field of big data research . keywords epidemiology imaging mri big data introduction technical developments over the past decades have enabled us to obtain abundant biological and socioeconomic information about single individuals and whole populations of interest . 
importantly , it has been realized that genetic data alone may not be sufficient to describe biological processes but that it has to be combined with phenotypic information to come to valid scientific conclusions . in this context , medical imaging can play a crucial role by providing detailed phenotypic data about an individuals anatomy and physiology as well as the early manifestation of morphological and functional disease states . 
one longterm goal is to achieve a detailed biological characterization of single individuals that can be used as a basis for preventive or therapeutic measures within the context of individualized medicine . 
however , to understand the biomedical significance of imaging phenotypes , it is necessary to have access to standardized and well - characterized data of a large number of individuals , ideally combined with relevant non - imaging data including genetic and metabolic information . implementation of imaging techniques in prospective , population - based cohort studies has been pursued early on and has resulted in improved understanding of complex disease processes as well as identification of novel imaging biomarkers as a precursor for overt disease states [ 2 ]  . 
prominent examples include the rotterdam study [ 3 ] , the framingham heart study ( fhs ) [ 4 ] , the multi ethnic study of atherosclerosis ( mesa ) [ 5 ] , the heinz nixdorf recall study [ 6 ] , the study of health in pomerania ( ship ) [ 7 ] , and the atherosclerosis risk in communities study ( aric ) [ 8 ]  . 
examples of novel imaging - based markers of risk include coronary calcification by computed tomogra phy ( ct ) [ 9 , 10 ] , assessment of left ventricular function / fibrosis or hepatic steatosis by magnetic resonance imaging ( mri ) [ 11 , 12 ] , and intima - media - thickness by ultrasound [ 13 ]  . 1 3 radiol med ( 2017 ) 122 : 430436 at the same time , magnetic resonance ( mr ) technology has progressed so rapidly that it offers non - ionizing , highresolution visualization of morphologic and functional processes without the need to administer contrast agent . 
its capability to perform examiner - independent , multi - region and whole - body mr scanning in clinical routine is a recent development [ 14 , 15 ] with a potentially high value for comprehensive phenotyping in a population - based imaging setting [ 2 ]  . utilizing these achievements for advanced , high - resolution , whole - body phenotyping , a number of epidemiological imaging studies have recently been initiated with the objective to create large imaging biobanks . 
in a recent position paper by the european society of radiology , imaging biobanks are defined as organised databases of medical images and associated imaging biomarkers ( radiology and beyond ) shared among multiple researchers , and linked to other biorepositories [ 16 ]  . the purpose of this article is to present existing epidemiological imaging studies implementing advanced , whole - body mr imaging and to discuss methodological and organizational aspects as well as challenges of these approaches . methodological requirements for large imaging studies in contrast to clinical imaging studies which focus on single individuals with specific questions , epidemiological imaging studies aim to collect imaging data from a large representative population using a broad protocol to establish the database that is statistically required for the extraction of meaningful information . 
to achieve this goal , imaging modalities used in such studies should meet certain requirements . primarily , safety aspects have to be considered as many epidemiological studies enroll representative samples from the general , primarily healthy population . 
finally , and most importantly for the data quality and thus scientific value , reproducibility , and standardization are main criteria for choosing the appropriate modality . taking into account these aspects , mri has emerged as the modality - of - choice for the majority of large , population - based imaging studies . 
the lack of ionizing radiation , the relatively good accessibility , and especially the combination of high anatomical detail and functional imaging techniques are advantages of mri compared to alternative techniques including computed tomography ( ct ) and sonography . 
the main drawback of mri in the context of population - based imaging studies is the relatively long examination time that limits the throughput of participants and thus results in comparably high cost . 
furthermore , standardization of mr examinations is a challenge and specific measures should be taken to guarantee comparable and constant image content . large epidemiological studies furthermore pose a challenge concerning data storage and distribution . 
data distribution is then performed either by a centralized system where participating researchers only have indirect access on the centrally stored data or a decentralized system where image data can be retrieved and stored at the individual research sites . 
table 1 shows an overview of these studies . table 1 characteristics of large epidemiological imaging studies using whole - body mr imaging epidemiological set up cohort size acquired data imaging studies ship cross - sectional / longitudinal ~10 , 000 biometric , clinical , biochemical , genetic whole - body mri , ultrasound cross - sectional biometric , clinical , biochemical , genetic whole - body mri ( in 30 , 000 participants ) uk biobank cross - sectional biometric , clinical , biochemical , genetic whole - body mri , ultrasound , dxa 200 , 000 100 , 000 1 3 432 the ship study the ship study ( study of health in pomerania ) was one of the first large - scale epidemiological studies that systematically included whole - body mri as part of the study protocol [ 16 ]  . 
in contrast to many other studies , the ship study provides not only cross - sectional but also longitudinal information of follow - up studies in part of the included cohorts . 
 experiences that were gained in the ship study strongly influenced the design of recent studies including the gnc study and uk biobank . several hundreds of studies and publications have been published using data from the ship study . 
among others , associations between imaging phenotypes and cardiometabolic risk could be demonstrated [ 21 , 22 ]  . the gnc study the gnc ( german national cohort ) study is a largescale epidemiological study aiming to identify genotypic and phenotypic features associated with health and disease [ 23 ]  . 
over 20 mio biological samples are expected to be collected in the course of the study that will be stored in a dedicated biobank in southern germany . as part of the gnc study , whole - body mr examinations will be performed in a sub - cohort of 30 , 000 participants beginning in 2015 [ 19 ]  . 
the mr imaging protocol consists of neuroradiological , cardiovascular , musculoskeletal , and whole - body studies that are acquired within one hour of examination time . in a dedicated pre - study that examined the influence of different scanner types on image - derived parameters , it was found that variations were considerably lower when using a single scanner type compared to a multi - scanner multivendor approach [ 24 ]  . 
over a long time period of approximately 25 years about 500 , 000 volunteers will be examined in a cross - sectional setting acquiring demographic , biometric , and functional data as well as biological samples [ 26 ]  . 
the imaging protocol includes ultrasound examinations , dual energy x - ray absorptiometry , and a whole - body mri scan covering neuroradiological , cardiovascular , and musculoskeletal aspects [ 18 , 27 ]  . access to acquired data is granted to researchers meeting the criteria of scientific quality and public interest . 
similar studies will also be possible combining imaging data and genetic data in the future using a radiogenomic approach . data analysis a major challenge of population - based imaging studies is the analysis and interpretation of acquired data . 
this challenge is not only caused by the enormous amount of acquired data but also by the high complexity of acquired multidimensional and multimodal imaging data ( big data ) [ 31 ]  . in general , imaging protocols are not optimized for a specific question but rather aim to provide a general anatomic and physiologic phenotypization of participating individuals . 
as an alternative , non - enhanced sequences have to be used for the purpose of assessing vascular morphology and the validity of such an approach should be examined in comparison to established contrast - enhanced sequences in a small population , potentially outside the main study . in contrast to conventional clinical imaging studies , where patient populations are relatively small , the extent of many epidemiological studies in terms of included participants reaches a magnitude where manual or visual analysis by human readers becomes very time - consuming or even impossible . 
to this end , fully automated or semi - automated algorithms have been developed for the analysis of specific image contents including organ segmentation [ 32 , 33 ] , assessment of adipose tissue distribution [ 34 ] or automated assessment of image quality [ 35 ]  . 
still , further developments in the field of automated image analysis are necessary to be able to fully harvest the large treasure of information that may be hidden in the acquired imaging biobanks . furthermore , it is of utmost importance to include nonimaging biomarkers into the process of analysis to create a frame of reference and to put imaging data in the correct context of interpretation . 
especially in cross - sectional studies , where no follow - up data are available for the assessment of outcomes , non - imaging markers can help to understand the physiological significance of identified patterns in the respective imaging studies . 
this requires a close collaboration between experts in numerous fields including radiologists , biologists , epidemiologist , and statisticians . as a side - effect , the demands on data analysis in epidemiological imaging studies will potentially initiate the development and application of novel research strategies and data extraction tools that can be used not only within these studies but also in routine clinical studies for the benefit of single patients . 
for example , the emerging methods of radiomics and radiogenomics are already conceptually incorporated in epidemiological studies [ 36 ] and may open new perspectives on imaging data . harmonization between studies as already mentioned above , data homogeneity and standardization plays a central role for the assurance of good data quality that guarantees valid , reliable , and reproducible results . 
to overcome this problem and to identify geographical and ethnic factors influencing imaging phenotypes , it would be of great interest to compare the results of different studies that are performed in different populations . 
this is specifically important for imaging studies that are generally not standardized in the same way as genetic or laboratory tests . imaging international population - based as a solution to this problem , it would be important to harmonize imaging protocols between the major national and studies . 
 challenges of populationbased imaging due to their enormous size , epidemiological studies come with many challenges , especially concerning infrastructure , data acquisition , and data handling . as already mentioned above , standardization of data is a specific challenge of population - based imaging studies , especially when mri is used as the main modality . 
 depicted are cine ssfp sequences ( top left three - chamber view , top right four - chamber view , bottom left two - chamber view , bottom right axial orientation )  . 
these sequences are part of the imaging protocol in the ship study , uk biobank and the gnc study evenly important , continuous data quality assurance is a prerequisite for the generation of valid data and thus useful scientific results . 
current approaches for quality control in imaging studies mostly combine statistical analyses of image properties ( such as signal homogeneity , noise , etc . ) with quality analysis by human observers , either technicians at the acquisition sites or radiologists [ 25 ]  . 
first attempts have been made to automate quality assurance by replacing human observers with machine - learning algorithms [ 35 ]  . another specific challenge of epidemiological imaging studies is the process of dealing with incidental findings . 
to provide a prompt report of severe findings , all acquired images have to be analyzed within a short time frame after acquisition , which is timeconsuming and organizationally challenging . 
again , automated analysis tools may help to optimize this process in the future . 1 3 radiol med ( 2017 ) 122 : 430436 conclusion large - scale population - based imaging studies have introduced a novel scientific approach in medical imaging by acquiring and analyzing large amounts of data to identify biomarkers of health and disease . 
overcoming these challenges , it can be expected that pioneering biomedical discoveries will be made that in turn can be implemented in the clinical routine in the context of a personalized preventive and therapeutic medicine . compliance with ethical standards conflict of interest author s . 
it is a potential route for embolic transit from the systemic venous circulation to the brain [ 5 ] , and its prevalence is higher in young patients with cryptogenic stroke than in those with a known stroke etiology [ 6 ]  . 
it is considered small if it has a diameter of 25 mm , and large if its diameter 610 mm [ 7 ] , but it is also possible to quantify its size by measuring right - to - left shunt ( rls ) [ 8 ]  . the most frequent mechanism explaining an increased risk of recurrent stroke is paradoxical embolism due to the systemic passage of venous thrombi through an inter - atrial conduit . 
demonstrated a greater involvement of the vertebro - basilar ( vb ) system in pfo - related stroke ( pfostroke ) , which is usually identified as a cortical ischemic lesion in the vb circle , whereas af - related stroke ( afstroke ) is associated with the presence of cortico - subcortical ischemic lesions involving multiple vascular territories [ 15 ]  . the aim of this study was to map the specific ischemic lesion patterns of distribution of pfo - stroke and af - stroke in our study population . materials and methods inclusion criteria and imaging we retrospectively reviewed the medical records of 750 patients admitted to our hospital with a clinical suspicion of acute ischemic stroke between january 2008 and february 2016 . all patients underwent ct scan of the brain in the emergency department and 534 patients underwent magnetic resonance ( mr ) brain scan during the admission in neurology department . by diagnostic test , including both laboratoristic and instrumental , the patient subtypes were classified using the five categories of the toast classification system [ 2 , 3 ]  . 
when mr studies were not available on pacs , we used all films found in patients records . finally , analysis of the background data of all of the patients identified two groups with different pre - existing diseases : 128 with pfo and 43 with af . 
in few patients of the pfo - group ( 18 ) , imaging was not available and it was considered only radiologic reports . we evaluated the patients symptoms ( headache ) , demographics characteristics ( gender , age ) and risk fig . 
pfo patent foramen ovale , af atrial fibrillation , c - tcd transcranial color doppler ultrasonography with contrast , tee transthoracic echocardiography , ct computed tomography , mri magnetic resonance imaging 1 3 414 radiol med ( 2017 ) 122 : 412418 factors ( hypertension , smoke , dyslipidemic disorders ) , and the presence / absence of an atrial septal aneurysm 10 mm of phasic septal excursion into ( defined as 15 mm durthe atrium or a sum total excursion of ing the cardiorespiratory cycle with base 15 mm as measured using m - mode ) [ 1 ] and rls . 
the entity of the shunt after c - tcd and tee with saline solution was evaluated because these have been considered sensitive methods of detecting a pfo [ 8 ] , which is defined as the passage of > 3 micro - bubbles from the right to the left atrium through the gap during the three cardiac cycle following the complete opacification of the right atrium [ 1 ]  . rls was detected through c - tcd and tte in all patients affected by pfo . 
 respectively , the cardiologist analyzed the count of the maximum number of micro - bubbles seen in left atrium in basal condition and after valsalva maneuver , while the neurologist analyzed the count of the maximum number of micro - bubbles detected in the spectral display of the insonated internal carotid arteries and in the mcas . 
 suggest [ 18 ] , the number of micro - bubbles detected through mca - doppler measurement it could be useful to quantify the rls , so it was possible to classify rls in small ( < 10 bubbles ) , large shunt in shower ( > 25 bubbles ) and curtain ( uncountable signals ) [ 8 ]  . moderate ( 620 bubbles ) , and grade 3 the dwi and flair sequences were used to confirm the ischemic lesions , which were classified in cortical , subcortical and cortical / subcortical . 
only 153 patients were enrolled for this analysis because imaging for 18 was not available . as in other studies , the affected vascular territories were divided into the anterior cerebral artery ( aca ) , mca , vb including pca ( posterior cerebral artery ) , brainstem , and cerebellar [ 19 ]  . 
all 171 patients were considered for this analysis , because also the reports of 18 patients with imaging not available described the sites of ischemia of the brain . two neuroradiologists , with , respectively , 6 and 20 years of experience , made these analyses . this type of work does not require approval by ethics committee , because of the retrospective nature of the study , but before all diagnostic exams patients received and signed informed consent . statistical analysis the differences in the frequency of lesion patterns and the corresponding vascular territory of the lesion between the patients with pfoand af - stroke were compared using pearsons 2 test . 
the size of the pfo was determined in the patients with pfo - stroke , and the correlation between the c - tcd and tee finding were assessed using the index of inter - rater reliability ( cohens k )  . 
age , gender , and risk factors were compared using students t test or pearsons 2 test as appropriate , and the frequency of a history of headache in the pfo - stroke group was analyzed . 
the statistical analyses were made using xlstats ( rodney carr 19972004 ) and graph pad instat software ( 19922009 by graphpad software )  . results 74 were males and n of 171 patients , n females . 
the causes of cryptogenetic stroke comprehend paradoxical af , arterial dissection , vasospasm , migraine - induced stroke , and pfo [ 21 ]  . patients with known causes , evaluated by clinical , laboratoristic , and instrumental findings , were excluded . 
it could be related to a selection bias due to the fact that medical records were from neurologic department . in our study , we did not find lesions in aca territories known and undetermined etiology ( cryptogenic ) [ 2 , 5 ]  . 1 3 416 radiol med ( 2017 ) 122 : 412418 pfo and af are sources of cardio - embolism because they generate arterial occlusions presumably due to an embolus resulting from the heart [ 2 ]  . embolism of cardiac origin is caused by three mechanisms : blood stasis and thrombus formation in an enlarged heart left chamber ( or with intracavitary abnormal structures or aneurysm of the left ventricle ) , supravalvular presence of material , and abnormal passage of venous blood to the arterial circulation ( paradoxical embolism ) [ 22 ]  . one of the most accredited etiopathogenic mechanism of cerebral ischaemia due to pfo is the paradoxical embolism in departure from peripheral venous district . 
this hypothesis assumes the association between venous thromboembolism and rls in the heart , as in the case of pfo [ 18 ]  . stroke in pfo - group involved a younger population than af in our study . 
in hommas metanalysis , several studies described the correlation of pfo with cryptogenic stroke in younger patient populations , however , the association with older patients is still controversial [ 23 , 24 ]  . sathasivam and sathasivam demonstrated the association between pfo and headache , we analyzed the anamnestic background of our study population and we noticed that the majority ( 58% ) of patients with pfo had recurrent episodes of headache [ 25 ]  . 
 [ 1 , 13 ]  . atrial septal aneurysm , an abnormal prolapse of atrial tissue , which protrudes in both or left or right atrium , was present in 16 patients of pfo - group . 
mechanisms of stroke in patients with those abnormalities may include direct embolization from thrombi formed within the aneurysm and also formation of thrombus as a result of atrial arrhythmias , this one was not present in our patients [ 31 ]  . considering that the hemodynamic of the circle of willis is determined by the confluence of flow of the two internal carotid arteries and of the basilar artery , and by the blood flow direction from vessels with high pressure to vessels with low pressure [ 24 , 32 ] , we hypothesized the possible correlation between frequent involvement of the vb territory and an anatomical variance of the pca , such as its embryonic origfrom our preliminary study , we did not achieve a statistically significant correlation ; these results could have been strongly influenced by the low number of patients who had a diagnostic angiographic mr and / or ct in their background . 
4 pattern of cortical involvement of pfo - stroke : left frontal cortical involvement on flair ( a ) and dwi ( b ) images 1 3 radiol med ( 2017 ) 122 : 412418 present embryonic origin of pca ( table 1 ) ; this result probably was obtained because of the limited number of the candidates who underwent angiographic studies ( only 51 patients on a record of 128 )  . 
in spite of the low number of patients with this anatomical variant , a positive association could be found with furthermore studies , because few articles concerning this argument are available in the literature [ 24 , 33 ]  . our study is limited by three factors : at first time , it is a retrospective study . 
four complications of the ipsilateral group were classified as major group c and 1 as major group d , while 1 complication of the contralateral group was classified as minor group b and 1 as major group c according to society of interventional radiology ( sir ) classification . 
no statistical significant difference was seen between complication rates of two groups in regard to sir classification . conclusions spc related complications do not differ in regard to ipsilateral or contralateral side selection on mastectomized patients with breast cancer and lymph node dissection . 
spcs can be implanted on ipsilateral or contralateral sides of the operation in these patients . keywords breast cancer contralateral ipsilateral society of interventional radiology subcutaneous port catheter introduction subcutaneous port catheters ( spcs ) have become an increasingly used technique in the treatment of oncology patients . 
venous access during spc implantation can be challenging in oncology patients , especially in patients with history of breast cancer surgery and / or radiotherapy ( rt ) [ 2 ]  . lymphedema can develop on ipsilateral upper extremity in patients with the history of modified radical mastectomy ( mrm ) or lumpectomy and lymph node dissection . 
although a scientific proof is not present , general opinion is to avoid all venous interventions ( from a simple intravenous cannulation to spc implantation ) in the ipsilateral extremity that lymph node dissection has been done . 
lymphatic drainage can be made partially through alternative ways like internal mammarian nodes in patients with mastectomy and lymph node dissection [ 2 ]  . the aim of this study is to evaluate long - term clinical follow - up results and complication rates of implanting spcs on ipsilateral or contralateral side of the chest with mastectomy side in patients with axillary lymph node dissection . materials and methods protocol inclusion criteria for patients were : female gender , history of breast surgery for breast cancer and eligible for the port implantation procedure ( international normalized ratio [ inr ] below 1.5 , platelet count higher than 75 , 000 / mm3 and good performance status )  . 
spcs were implanted to 73 patients with breast cancer in our department between march 2012 and september 2014 , of which 34 were on the ipsilateral and 39 were on the contralateral side with the operation . 
all of the patients were women and have been treated with breast - sparing surgery ( lumpectomy ) or mrm and lymph node dissection . patients were divided into two groups : ipsilateral group ( 34 patients ) and contralateral group ( 39 patients )  . 
classification of complications according to sir criteria was : minor complications , ( a ) no therapy , no consequence , ( b ) required nominal therapy , no consequence ; included overnight admission for observation ; major complications , ( c ) required therapy , minor hospitalization ( < 48 h ) , ( d ) required major therapy , unplanned increase in level of care , prolonged hospitalization ( > 48 h ) , ( e ) permanent adverse sequelae , ( f ) death . 
local anesthesia alone ( prilocaine 20 mg / ml , citanest , astrazeneca and lidocaine 20 mg / ml epinephrine 0.025 mg / ml , jetokain , adeka ) was adequate for the procedure in most of patients . 
spcs were single lumen catheters and were implanted under the guidance of a monoplane , flat panel angiography unit ( artis zee , siemens , erlangen , germany ) by an experienced interventional radiologist . 
types and characteristic of spcs used are given in table 1 . surgical skin cleansing was made by applying the antiseptic solution ( povidone iodine 10% , batticon , adeka ) to the operation side from mandibular level to lower border of the breast and middle axillary line under sterile conditions in the operation rooa single - wall puncture needle ( 18g ) was introduced into the internal jugular vein under ultrasound ( us ) guidance . 
the port catheter 1 3 474 port table 1 types and characteristics of the implanted ports radiol med ( 2017 ) 122 : 472478 catheter number of patients ( ipsilateral group ) number of patients ( contralateral group ) port - a - cath ii low - profile ( sims deltec , st paul , mn ) pro - fuse ct power injectable low profile ( medcomp , harleysville , pa ) infu - kt titanium standard intravenous access ( fb medical , france ) polysite adult standard ( perouse medical , france ) polysite adult standard ( perouse medical , france ) focus titanium & polysulfone ( promecon gmbh , germany ) 7.8 f , polyurethane 8 f , polyurethane 7.8 f , silicone 7.2 f , polyurethane 9.5 f , polyurethane 10.5 f , polyurethane was introduced into the tunnel by the help of a trocar and it was attached to the reservoir with locking technique . 
functionality of the spc was controlled by injecting 100 u / ml heparinized saline through the port reservoir . patients were followed for 2 h after the procedure in the observation room in regard to hemorrhage and pneumothorax risk . 
the level of significance was determined to be 0.05. results median ages of 34 patients in the ipsilateral group and 39 patients in the contralateral group was 47.3 ( 2866 years ) and 50 ( 3468 years ) , respectively ( table 2 )  . 
group characteristics similar in two groups were : evaluation was retrospective , spc indication was ct , the nature of ct was curative , all patients were outpatient , lymph node dissection history was present in all patients , procedures were technically successful , spcs were implanted under sterile conditions with full dressing in a single session , the procedure was made under fluoroscopy and us guidance , spcs were controlled with heparinized saline injection after the procedure , complete wound closure was ensured , control fluoroscopic images were obtained , there was no malfunction per 100 catheter days and no revision per access site / per 100 catheter days . 
tumor was on the right breast in 31 patients ( 31 / 34 ; 91.2% ) , on the left in 3 patients ( 3 / 34 ; 8.8% ) in the ipsilateral group . 
in ipsilateral group , thrombus was present in jugular vein of three patients ( 3 / 5 ) , in vena cava superior and brachiocephalic vein of one patient ( 1 / 5 ) and in vena cava superior of one patient ( 1 / 5 )  . 
2 findings suggestive of thrombosis on a fluoroscopic image after contrast media injection into the catheter 13 months after implantation of a right sided port catheter in a patient with lumpectomy history in her right breast : contrast media is not passing from superior vena cava into the right atrium and there is pericatheter leakage of the contrast media is to axillary and internal mammary lymph nodes . 
there was no statistical difference between two groups in regard to infections per 1000 days . early ( within 30 days of the procedure ) and late ( after 30 days of the procedure ) complications can happen after spc placement . 
1 axial ( a ) and coronal ( b ) computed tomography angiography images : thrombosis in the catheter and superior vena cava leading to occlusion 11 months after implantation a right sided port catheter in a patient with lumpectomy history in her right breast ( black arrows port catheter , star thrombus ) can be implanted successfully by us and fluoroscopy guidance and procedure related and infective complication rates are low when imaging guidance is used [ 5 , 6 ]  . 
the standard access for spcs is through the subclavian / internal jugular vein or cephalic vein , but a femoral vein access may be preferable in patients with history of breast surgery and / or rt [ 7 ]  . 
we preferred the chest approach and spcs have been implanted with imaging guidance in our interventional radiology unit . lymphatic drainage of the upper extremity is to axillary lymph nodes [ 5 , 10 ] while drainage of the chest wall 1 3 radiol med ( 2017 ) 122 : 472478 fistula , pneumothorax , hemothorax and hematoma are early complications seen within 24 h . 
thrombus most commonly forms at the entrance site of catheter into the vein or with the contact of catheter and wall of the ve it is usually asymptomatic and can lead to infection and pulmonary embolis the effect of type of catheters on thrombus formation is controversial [ 12 ]  . 
 however , this situation did not affect the randomization of the study , because no statistical correlations were observed between complication rates and dimensions / materials of catheters for both groups . one limitation of our study is its retrospective nature . 
we sought to evaluate prevalence and distribution of cn in carotid arteries in correlation with clinical symptoms . methods 178 consecutive patients with unilateral ischemic 2 mm by duplex ultrasound stroke and carotid plaques underwent a carotid - black - blood - 3t - mri with fat - saturated preand post - contrast t1w - , pdw - , t2wand tof images using dedicated surface - coils . 
prevalence of cn was determined in common carotid artery ( cca ) and internal carotid artery ( ica ) in consensus by two reviewers blinded to clinical information . results thirty seven cn in 28 arteries of 26 patients were identified . 
20 , 80336 munich , germany conclusion cn were found in 7.9% of arteries with carotid - plaques 2 mm by duplex - ultrasound ; prevalence was significantly higher in symptomatic arteries with 30% stenosis compared to asymptomatic with < 30% stenosis , suggesting that cn play a role in pathogenesis of ischemic stroke in a small subset of patients . keywords calcified nodules carotid arteries prevalence stroke purpose in western industrial countries atherosclerosis and its thrombotic cardiovascular complications , including myocardial infarction , sudden cardiac death and stroke , are among the most frequent causes of death as well as longterm disability [ 1 , 2 ]  . 
approximately , 2025% of ischemic strokes are due to large artery atherosclerosis and the majority of those are caused by ruptured atherosclerotic plaques at or close to the carotid bifurcation [ 3 ]  . 
therefore , it seems to be of paramount importance to get accurate information about the morphology and the composition , and thus the vulnerability of an atherosclerotic plaque , ideally before an ischemic event can occur . based on studies of culprit plaques [ 4 ] major and minor criteria were defined to assess a plaques vulnerability ( active inflammation , stenosis > 90% , endothelial dysfunc tion , intra - plaque hemorrhage , thin caps with large lipid / necrotic core , fissured plaque , endothelial denudation with or without superficial platelet aggregation and fibrin depo sition , glistening yellow plaques in angioscopy , cn , and outward remodeling )  . 
the pathobiology of atherosclerosis and its clinical consequences varies within the vascular tree , although the disease is a systemic one , that can 1 3 450 radiol med ( 2017 ) 122 : 449457 involve various vascular beds simultaneously [ 4 , 5 ]  . 
hence , markers of plaque vulnerability might not necessarily be identical between distinct vascular beds such as the coronary and carotid arteries . several recent histopathological and in vivo mri studies have confirmed an association of intraplaque hemorrhage [ 6 ] , thin / ruptured fibrous cap and necrotic core size [ 7 ] , thrombus formation and active inflammation with cerebrovascular symptoms in the carotid arteries . 
for other criteria of the vulnerable plaque , such as stenosis > 90% , positive remodeling and calcified nodules the significance of its presence in the carotid arteries has yet to be determined . although calcified nodules are defined as a minor criteria for vulnerable plaques and are known to cause 5% of coronary infarcts [ 8 ] only little data is actual available on the association of these nodules with cerebrovascular events in the carotid arteries . 
consequently calcified nodules are known to be a convex shaped hypointense area in white - blood ( tof ) and black - blood ( t1w , pdw and t2w ) images protruding into the lumen . therefore , the aim of this study is to identify the prevalence , distribution and clinical outcome of patients with calcified nodules in the carotid arteries . materials and methods study population this prospective study was conducted at our department between august 2008 and august 2015 . 
inclusion criteria were the presence of atherosclerotic plaques with 2 mm plaque thickness near or at the carotid bifurcation as determined by duplex ultrasound and ischemic symptoms in the territory of the anterior or middle cerebral artery . 
the subjects were considered to be symptomatic if they had an episode of a transient ischemic attack ( tia ) , stroke or amaurosis fugax in the right or left anterior circulation . 
stroke was defined as an acute dwi lesion and corresponding acute neurological deficit of > 24 h duration , tia was defined as an acute neurological deficit in the anterior circulation of < 24 h duration without dwi lesion on brain mri . 
exclusion criteria were bilateral infarcts on cmri , standard contraindications against mri , allergy to contrast agent , reduced renal function ( gfr glomerular filtration rate < 30 ml / min ) , former radiation therapy to head and / or neck and a surgery within 24 h prior to the carotid mri . the clinical data included age , gender and symptom status . 
in addition presence / absence of cardiovascular disease risk factors ( diabetes , hypercholesterolemia , smoking , arterial hypertension , coronary heart disease , positive family history of cardioor cerebrovascular events ) was documented . mri protocol patients with unilateral ischemic stroke underwent a carotid black - blood 3t - mri ( magnetom verio or magnetom trio , siemens healthcare , erlangen , germany ) with fat - saturated pre - contrast and post - contrast pdw - , t2wt1w - , and tof images using dedicated surface coils according to a previously published protocol [ 9 ]  . 
for improving the signal - to - noise performance and optimizing the spatial resolution , a dedicated 4 - channel surface coil ( machnet b.v. , eelde , netherlands ) for bilateral carotid scans was used . 
for tof slice thickness was 1 mm and for the remaining sequences 2 mm . image review satpoor , 2 sufficient , 3 good and 5 before the review two radiologists rated the image quality by a scale with 5 points ( 1 excellent )  . 
images with a quality isfying , 4 in t1w , t2w or tof 2 were excluded ( indicating a low signal - to - noise ratio or severe blurring that was adjusted to a motion of the subject )  . 
to assess intra - reader reproducibility of the presence / absence of calcified nodules , the initial independent review of the two reviewers was used for analysis , and one of the reviewers re - reviewed 62 arteries of 31 randomly selected patients 3 months after the initial review . 1 3 radiol med ( 2017 ) 122 : 449457 mr criteria for the identification of calcifications , calcified nodules and american heart association ( aha ) lesion type ( please see table 3 ) have been previously reported [ 10 , 11 ]  . 
to compare clinical demographics between patients with and without calcified nodules , we used the fishers exact test for categorical variables , and the unpaired t test with equal or unequal variances ( as appropriate ) for continuous variables . 
2 mr images of the right common carotid artery ( cca ) of an 81 - year - old female with ipsilateral ischemic stroke with 70% stenosis in the internal carotid artery . 
the calcified nodule ( arrowhead ) , which is protruding into the lumen is best seen on tof images although it is clearly visible on all other sequences as well [ asterisk infolding artifact ; tof ( a ) , t1w ( b ) , pd ( c ) and t2w ( d ) ] prevalence and distribution of calcified nodules detailed results of the distribution of calcified nodules in different patient subgroups are shown in table 2 . 
of the 37 calcified nodules , 22 ( 59% ) were found in the common and 15 ( 41% ) were found in the internal carotid artery . the majority of calcified nodules were found near or at the carotid bifurcation . 
figure 4 shows the distribution of calcified nodules in regard to their distance to the carotid bifurcation . calcified nodules , aha lesion types and symptomatic carotid stenosis in 31 out of 37 plaques ( 83.4% ) with calcified nodules the underlying lesion type according to the american heart association ( aha ) was classified as a type vii lesion , 3 underlying lesion types were classified as type iv / v with a large necrotic core covered by an intact fibrous cap and 3 underlying lesions were classified as complicated type vi plaques , with thrombus , hemorrhage and / or rupture of the fibrous cap . 
3 mr images of a calcified nodule in the left internal carotid artery ( ica ) of an 73 - year - old male with contralateral ischemic stroke without luminal stenosis . 
in total we were able to identify 37 calcified nodules in 28 distinct arteries of 26 distinct patients , resulting in a prevalence of 7.9% on an arterial level and of 14.5% on a patient based level . 
we found a higher prevalence of calcified nodules in the common compared to the internal carotid artery and a significantly higher prevalence of calcified nodules in arteries with 30% stenosis ipsilateral to ischemic stroke compared to the contralateral side . 
in addition we found a higher prevalence of calcified nodules in patients with hypercholesterolemia and hypertension . frequency and distribution of calcified nodules to the best of our knowledge there is no published data describing the frequency and distribution of calcified nodule in the carotid arteries and most of our knowledge fig . 
4 distance of calcified nodules ( cn ) to bifurcation in mm ( proximal of bifurcation ; 0 , bifurcation ; , distal of bifurcation ) of calcified nodules , its distribution and its clinical significance are based on histopathological and intravascular ultrasound ( ivus ) studies of the coronary arteries . 
 [ 13 ] found 314 calcified nodules in 250 distinct coronary arteries in table 3 american heart association ( aha ) lesion type and mr criteria for the identification of calcifications , calcified nodules conventional aha lesion type classification modified aha lesion type classification for mri type i : initial lesion with foam cells type iii : near - normal wall thickness , no calcification type ii : fatty streak with multiple foam cell layers type iii : preatheroma with extracellular lipid pools type iii : diffuse intimal thickening or small eccentric plaque with no type iv : atheroma with a confluent extracellular lipid core type v : fibroatheroma type ivv : plaque with a lipid or necrotic core surrounded by fibrous tissue with possible calcification type vi : complex plaque with possible surface defect , hemorrhage , or type vi : complex plaque with possible surface defect , hemorrhage , or thrombus type vii : calcified plaque type viii : fibrotic plaque without lipid core type viii : fibrotic plaque without lipid core and with possible small calcification thrombus type vii : calcified plaque calcifications 1 3 radiol med ( 2017 ) 122 : 449457 697 distinct patients , resulting in a prevalence of calcified nodules of 30% per patient 17% and per artery . 
the lower prevalence of cn in the carotid arteries on a per - patient basis might be due to the fact that we did not image the whole internal and common carotid artery , thus calcified nodules in the proximal common or distal internal carotid artery would have been missed . 
however , in the vast majority of patients carotid atherosclerosis is centered at the carotid bifurcation and therefore it is unlikely that a large number of calcified nodules have been missed due to the limited coverage available in our study . 
another possible reason for the lower prevalence of calcified nodules might have been that we used in vivo mri to visualize calcified nodules ; therefore , very small calcified nodules might have been missed . 
however , we used a similar minimal size for a calcification to be classified as a calcified nodule ( minimum diameter 1 mm ) and previous mr studies have suggested that a spatial reso0.5 mm2 is usually sufficient to identify callution of 0.5 cifications with an area > 1 mm 2 with good correlation to histopathology . there is no precise information about the pathogenesis of calcified nodules . 
based on histological data calcified nodules haveamong the subtypes of vulnerable plaques the greatest relative amount of calcification compared to the total plaque area and are thought to be associated with a healed fibroatheroma and / or recurrent intraplaque hemor rhage [ 8 ]  . 
we found no association of calcified nodules with plaque hemorrhage , since the calcified nodules in our study did not have an area of early or late subacute plaque hemorrhage in its vicinity , suggesting a minor role of recurrent plaque hemorrhage in the pathogenesis of calcified nodules in the carotid arteries . 
however , it has to be pointed out that old hemorrhages are hypointense on all pulse sequences [ 15 ] and , therefore , it is very difficult to distinguish old hemorrhages from calcified tissues by mri , leaving the door open for a role of old hemorrhages in the pathogenesis of these lesions . in our study , we found the highest prevalence of calcified nodules in arteries ipsilateral to ischemic stroke with 30% stenosis , suggesting that calcified nodules could play a role in the pathogenesis of ischemic stroke in a subset of patients . 
overall , 75% of symptomatic arteries with carotid stenosis exhibited features of vulnerable plaques by standard mr criteria and an additional 7.5% of atherosclerotic lesions would have been classified as such if presence of calcified nodules would have been taken into account . 
to date , the impact of this finding remains unclear and larger prospective studies are needed to evaluate whether calcified nodules provide additional value for the characterization of vulnerable plaques . furthermore , we found a higher prevalence of calcified nodules in patients with arterial hypertension and hypercholesterolemia . 
they observed , that there were consistently fewer non - culprit lesions major adverse cardiac events in the patient group with calcified nodules than in the non - calcified nodule group on a follow - up of 1 , 2 or 3 years , suggesting a minor role of calcified nodules on ischemic coronary events . 
to date , no data of the impact of calcified nodules in the carotid arteries on recurrent events is available . several recent cta studies have examined the role of carotid calcification and cardiovascular events . 
another retrospective study with 96 patients who underwent both cta and carotid mra found that adventitial calcification pattern in combination with maximum soft - plaque thickness by cta were highly predictive of plaque hemorrhage by mra [ 17 ]  . 
thus , several studies have examined the role of hard plaque thickness , speckled and adventitial calcification but to the best of our knowledge no study has looked into the role of calcified nodules in the carotid arteries by cta . as a limitation the number of calcified nodules identified in this study is relatively low and consequently no 1 3 456 radiol med ( 2017 ) 122 : 449457 definite association between calcified nodules and ischemic symptoms can be established . 
to date , thanks to improved information technology infrastructures , it is possible to store data from each single cancer patient , including clinical data , medical images , laboratory tests , and pathological and genomic information . 
in the oncologic patient , big data analysis is at the beginning but several useful applications can be envisaged including development of imaging biomarkers to predict disease outcome , assessing the risk of x - ray dose exposure or of renal damage following the administration of contrast agents , and tracking and optimizing patient workflow . 
in medicine , the basic idea behind using big data is to learn new knowledge from every patient we have ever treated and apply this knowledge to the next patient [ 2 ]  . 
in oncology , where information collected from the single patient is extremely variegated , big data analysis could allow definition of specific and efficient diagnostic and therapeutic pathways , improv ing patient workflow and quality of life . 
the aim of this review is to collect current evidence and to envisage how in the future big data may impact on the diagnostic pathway of the oncologic patient . 1 department of surgical sciences , university of torino , a.o.u. 
citt della salute e della scienza , via genova 3 , 10126 turin , italy 2 department of radiology , candiolo cancer institutefpo , irccs , strada provinciale 142 , km 3.95 , candiolo , 10060 turin , italy 3 department of medical physics , candiolo cancer institutefpo , irccs , strada provinciale 142 , km 3.95 , candiolo , 10060 turin , italy big data in oncologic imaging : the rationale the following key concepts related to big data should be considered when approaching oncologic imaging issues : 1 . 
opposite traditional hypothesis - driven cancer research [ 4 ] , big data research may be launched regardless of whether important questions are identified . 1 3 radiol med ( 2017 ) 122 : 458463 fig . 
big data is not about implementing one piece of technology , it also includes data mining and machine learning and offers potential alternative approaches to leveraging large data resources [ 6 , 7 ]  . cancer fits well into these concepts , as it is a complex disease that changes , evolves , and adapts to the surrounding environment . 
its evolution could be better understood by collecting information from different sourcese.g. , demographic , genetic , imaging , treatment , and outcomes that could then be processed as big data . 
in 2012 , at&t estimated that the storage requirements for medical archives were increasing by 2040 % each year , with medical images constituting one - third of total global storage demand [ 9 , 10 ]  . 
extraction of data from radiation and contrast agent dose registries will allow to explore dose effects on subjects with cumulative x - rays , computed tomography ( ct ) scans , radiation therapy treatments , or nuclear medicine examinations and minimize contrast - induced nephrotoxicity by stratifying cancer patients into risk categories . 
finally , processing of big data could support the development of optimized clinical workflows and in the end increase the management efficiency of comprehensive 1 3 460 radiol med ( 2017 ) 122 : 458463 cancer centers and of tertiary health facilities in general [ 13 ]  . big data in oncologic imaging : current developments today , most of what we know about cancer comes from a tiny subset of patients , i.e. , the 3 % who are enrolled in clinical trials ; hence , those data are non - representative of the entire cancer population [ 14 ]  . 
the repository was created with the support of the national cancer institute with the aim of collecting , curating , and managing a rich collection of oncologic imaging data to enable open - science research [ 16 ]  . 
at present , more than 26 million radiologic images contributed by 28 institutions and several thousand pathology images are stored in this repository that is constantly increasing in size and variety [ 15 ]  . 
in this chapter , we will review how the analysis of all this information benefits each individual patient . extracting the dark matter from medical images in medical images , data are usually provided as an orderly set of gray scale pixel values ; however , in this form data are not synonymous of information or knowledge . 
eliot siegel from the university of maryland compared the data hidden in a clinical image , i.e. , data that cannot be directly observed with current technology , as the dark matter in space [ 17 ]  . 
improvements in image analysis will reasonably bridge the gap between the visual content and its numeric representation , which includes encoded color and texture properties of an image , the spatial layout of objects , and geometric shape characteristics of anatomical structures . 
a magnetic resonance ( mr ) examination , for example , includes high - resolution morphological images and information on tissue perfusion and diffusion capturing complex in vivo flow patterns ; similarly , ct dual - energy acquisitions include information on material decomposition and spectral imaging [ 18 ]  . 
furthermore , combining different imaging modalities at the hardware level ( mr / pet , pet / ct ) will open up a range of new opportunities for image analysis [ 5 ]  . pattern recognition software and tools for high - throughput extraction of quantitative features have been implemented in parallel to the increase in dataset size and information . 
radiomic data typically contain first - , second - , and higher - order statistics that can be combined with other patient data to develop models with improved diagnostic , prognostic , and predictive accuracy . diagnostic xray dose exposure during the past 30 years , radiologic procedures involving ionizing radiation have been increasingly used in clinical routine leading to a dramatic increase in individual patient dose exposure . 
individual risk of developing radiation - related cancer from any single imaging procedure is extremely low ; however , repeated examinations may lead to a substantial increase in such risk [ 20 ]  . 
in the future , the opportunity to exploit large databases will help clarify the relationship between cancer - induced pathologies and lowdose radiation levels [ 21 , 22 ]  . 
collected information should include ( 1 ) radiation dose distributions and dosevolume metrics from treatment planning in radiotherapy ( i.e. , dosevolume histograms , the volume receiving a certain dose , minimum dose to a given volume , mean , maximum , and minimum dose ) ; ( 2 ) x - ray doses from radiological imaging ( i.e. , volumetric ct dose index , dose - length product , dose - area product ) ; and ( 3 ) gammaray and other radioisotopes radiation doses from nuclear medicine imaging and treatment . 
a radiation dose registry may allow clinicians to compare dose levels to the averages of other national and international centers , in order to successfully implement low - dose protocols . 
this will also favor standardization , create higher patient confidence in radiation safety , and offer the opportunity for better quality assessment . regulations and guidelines , such as the european directive euratom 97 / 43 , 2013 / 59 / euratom , and the american college of radiology dose whitepaper , express the need for facilities to track radiation dose for patient and population , and support the implementation for dose registries . 
in particular , the european directive 2013 / 59 / euratom 1 3 radiol med ( 2017 ) 122 : 458463 points out that health authorities will be more pervasive on inspecting the dosimetry applied to patients . 
the new ihe radiation exposure monitoring ( rem ) profile facilitates the collection and distribution of the estimated patient radiation exposure information resulting from imaging procedures and provides an implementation guide for vendors . 
in addition , these devices allow optimization of acquisition protocols in order to find the right balance between image quality and dose , minimizing the risk of radiation - induced cancers ( com / article / software - help - manage - medical - imaging - radiation - dose )  . 
 the first is dose capture : non - dicom - sr compatible ct scanners store dose information as images rather than in numerical form , requiring an optical character recognition algorithm to capture the data . 
second , information has to be associated with the patient to be exportable to dose registries such as the american college of radiology ( acr ) dose index registry ( dir )  . 
institutions are provided with periodic feedback reports comparing their results by body part and exam type to aggregate results ( national - radiology - data - registry / dose - index - registry )  . big data and radiation oncology big data repositories include detailed 3 - dimensional dosimetric and imaging data , and their changes over time . 
in a pilot project , prostate cancer was selected as the initial disease site , and information was collected on clinical features , toxicity , and spatial and temporal dose distribution . 
thanks to this pilot study , researchers may now identify best strategy options that allow patients to safely choose to do nothing or opt for mild treatments or surgery [ 26 ]  . 
in the era of genomics , one may envision leveraging large repositories with detailed radiation therapy data , imaging data , and genomic profiles of tumor and normal tissue samples in order to better understand predictors of tumor control and risk of normal tissue injury , providing radiation oncologists the opportunity to potentially offer personalized dose prescriptions improving tumor control and reducing toxicity [ 7 , 27 ]  . predicting renal damage in recent years , the study of acute kidney injury has been facilitated by the increasing availability of stored demographic and clinical patient data [ 28 , 29 ]  . 
this heterogeneity may hinder comparisons and underestimate disease burden , limiting its application in a clinical setting [ 28 ]  . collecting information on kidney functional status could be particularly useful in cancer patients . 
it is well known that iodinated contrast agents are associated with an increased risk of contrast - induced nephrotoxicity ; the risk is particularly high in patients that have impaired renal function and diabetes [ 31 ]  . 
the risk of complications from contrast medium administration is compounded by advanced age , dehydration , the number of times ct is repeated , and co - administration of nephrotoxic chemotherapeutic drugs . 
thus , identification of factors predicting contrast - induced nephrotoxicity is important to avoid potentially serious complications , related to acute deterioration of kidney function [ 31 ]  . 1 3 462 tracking patient workflow oncological patient management is more and more a complex matter requiring constant monitoring throughout chemotherapy lines , radiation therapy sessions , scheduled follow - up assessments , etc . 
conversely , in an integrated healthcare system , where interdisciplinary teams of specialists act together , all information should be linked with the aim of optimizing individual patient care , paving the way to truly personalized medicine . to optimize current oncological workflows , it will be necessary to develop event - tracking systems in which monitoring points based on checklists are implemented . 
 a good system should be able to identify workflow issues and technical errors in every step of patient management , advancing department quality control and improving existing processes or implementing new workflows [ 33 ]  . 
each patient in the processing chain will thus contribute to help clinicians and technicians to detect workflow inefficiencies , as incorrectly transmitted images or information during disease assessment , or delays in scheduled follow - ups . 
a patient tracking system would also simplify pinpointing the sources of error or mismatching within processes , producing as a result an honest picture of the current events , and enhance the ability to respond in real time . 
in the end , again , all of this will improve patients access to treatment , reduce therapy side effects , and contribute to improve his quality of life and , on a population scale , allow healthcare systems to save more lives and contain costs . conclusions the possibility to extract new knowledge from the huge amount of increasingly available unstructured data is crucial for advances in cancer diagnosis and treatment . 
indeed , the radiol med ( 2017 ) 122 : 458463 very point of looking to big data is to identify patterns that create answers to questions you didnt even know to ask [ 34 ]  . 
therefore , the success of big data in creating healthcare value may require some changes in the current polices , to balance the potential societal benefits of big data approaches and the protection of patients confidentiality [ 35 ]  . in conclusion , the benefits of large - scale data mining to the oncologic patient are slowly emerging . 
big data initiatives could be instrumental in improving the management and the quality of life of each individual cancer patient based on the results of imaging biomarker analysis or on the implementation of event - tracking systems . 
because of their intrinsic heterogeneity , it will be very challenging to fully exploit big data . compliance with ethical standards no funding was received for this work . conflict of interest daniele regge declares that he has no conflict of interest . 
we hope to highlight the value of radiological evaluation by integrating studies on the impact of surgical treatments and non - surgical factors on local recurrence of gctb and the current statuses of genetic and molecular prognostic factors of gctb . 
as a non - invasive method , magnetic resonance imaging ( mri ) is especially valuable for the diagnosis and evaluation of bone tumours due to its heightened sensitivity to soft tissue disease and multiplanar image acquisition . 
it is classified as an intermediate [ 3 ] , characterized by locally destructive behaviour that leads to significant local osteolysis and arising mostly in the metaepiphyseal areas of long bones in the appendicular skeleton [ 4 , 5 ]  . local recurrence is an enormous challenge encountered during the clinical treatment of gctb [ 6 ] with incidence rates of 065% [ 7 , 8 ] depending on surgical options , which include curettage with or without adjuvant therapy and wide resection with biological or non - biological reconstruction . 
currently , intralesional excision is the preferred treatment of gctb [ 3 , 9 , 10 ] , rather than wide or radical excision , although the latter are associated with reduced recurrence with the compromise of limb function [ 11 ]  . 
 local recurrences of gctbs are attributed to postoperative residual tumour tissue [ 8 ] , particularly in cases treated via intralesional procedures . the prognostic factors for a local recurrence of gctb merit intensive investigations with the aims of balancing limb function with local control and directing surgical approaches . 
this article reviews currently available studies of factors associated with local recurrence , including 1 3 506 radiol med ( 2017 ) 122 : 505519 surgical treatments , clinical features , imaging findings , and genetic and molecular aspects . 
this review will help to establish a multiple evaluation system [ 18 ] by which prognostic factors of local recurrence can be evaluated systematically . surgical approach and recurrence gctb is an intermediate neoplasm with significant local osteolysis . 
in contrast , intralesional curettage can preserve the adjacent joint and its function , and is preferentially performed alongside adjuvants such as chemicals ( phenol , hydrogen peroxide and sterile water and alcohol ) , toxins , thermal procedures ( liquid nitrogen , argon beam , cryotherapy , electrocautery , and bone cement filling ) and highspeed burrs [ 3 , 10 ]  . 
current studies have reached a consensus [ 3 , 7 ] regarding the lower recurrence rate associated with wide resection ( 012% ) versus intralesional curettage ( 1267% ) [ 8 , 1215 ] ; for the latter , however , the inclusion of the above - listed adjuvants and polymethylmethacrylate ( pmma ) can reduce the rate of local recurrence [ 7 , 8 , 16 , 17 ]  . 
further the tumouricidal activities of pmma , including thermal and toxic effects , can reduce the local recurrence of gctb [ 11 ]  . in clinical practice , most authors advocate intralesional excision with adjuvants as a preferable treatment for gctb [ 8 , 1315 ] , while wide resection is even considered a reasonable surgical option for campanacci grade iii lesions , second recurrences of gctb and cases involving pathological fracture and / or soft tissue extension [ 4 ]  . however , as a conflict over consensus , some authors [ 7 , 8 , 10 , 18 ] suggest that intralesional procedures are preferable even for recurrent patients , including those with second and third recurrences of gctb , as well as for those at risk of metastasis and malignant transformation . 
on the other hand , some authors [ 14 , 19 ] have reported the achievement of desired local control and functional outcomes when adjuvant therapies are administered along with intralesional procedures . 
 [ 20 ] observed satisfactory adjacent joint and extremity function following custom mega - prosthetic arthroplasty , which yields desirable functional outcomes and the lowest risk of complications after wide resection . 
 [ 17 ] demonstrated that the use of cement after curettage could significantly reduce local recurrence ; however , this adjuvant simultaneously increased the risk of subsequent joint replacement . nonsurgical factors of recurrence of gctb aggressive procedures are inevitable when attempting to reduce the risk of local recurrence of gctb . 
the tendency toward recurrence should be predicted preoperatively and the optimal clinical approach should attempt to balance local control and functional preservation . according to contemporary research , the non - surgical factors for local recurrence of gctb remain controversial and ambiguous . 
this study coincided with a report by klenke et al . , which identified age as an independent risk factor for recurrence [ 7 ] irrespective of the disease status and chosen treatment . 
 [ 27 ] reported that the clinical use of bisphosphonates could reduce the local recurrence of gctb , particularly among stage iii cases . location tumour localization in the distal radius [ 28 ] was associated with a higher rate of recurrence of gctb according to odonnell et al . 
the proximal femur [ 29 ] was also identified as a high - risk site for a local recurrence of gctb , a finding that was attributed 1 3 radiol med ( 2017 ) 122 : 505519 to therapeutic challenges associated with this location . 
these findings , which were mostly drawn from statistical analyses , have not yet been explained convincingly through investigations . campanacci classification many authors [ 13 , 30 ] suggested that the jaffe grade was not associated with the biologic behaviour of gctb , and , therefore , could not be used for the histologic prediction of local recurrences . 
 [ 32 ] also observed a higher rate of local recurrence in campanacci grade iii tumours , compared with grade ii tumours . soft tissue extension according to arbeitsgemeinschaft knochentumouren [ 8 ] , tumour extension correlates strongly with recurrence . 
soft tissue extension increased the complexity of surgery , thus increasing the likelihood of tumour tissue remnants . pathologic fracture few reports have described investigations of pathologic fractures in the context of local recurrences of gctb . 
 [ 8 ] explained the conflicting results as follows : because pathologic fracture is considered a risk factor for local recurrence , an awareness of the typically high risk of recurrence resulted in a thorough excision and , consequently , a reduced incidence of recurrence . 
 in brief , although patients with pathologic fractures can be treated via curettage , these cases should be addressed with caution . surgical approaches to gctb should be determined after thoroughly understanding these disease - related variables [ 7 , 8 ]  . 
however , the paradoxical results of the previous studies can be explained by differences in surgical aggressiveness toward gctbs with a higher risk of recurrence [ 8 ] , as more aggressive treatment might reduce the number of potentially recurrent cases . 
therefore , prospective cohort studies of disease - related variables are needed to investigate risk factors for local recurrence of gctb . genetic and molecular prognostic factors for gctb the mechanism underlying the histogenesis of gctb remains unclear [ 34 ]  . 
these tumours are characterized by the presence of large numbers of osteoclastic giant cells uniformly distributed amongst a background comprising mononuclear spindle - like stromal cells and other rounded monocytes [ 5 , 35 , 36 ]  . 
according to a study of phenotypic characterization [ 35 ] , osteoclastogenesis appeared to be generated neither by endomitoses nor exclusively by the fusion of cd14 - expressing mononuclear rounded cells . 
accordingly , the fusion of cd33 - positive pre - osteoclastic cells might comprise the initial trigger of osteoclastogenesis , a suggestion that was verified in a cytological study [ 37 ] in which the stromal cells of gctb ( gctsc ) played a critical role in inducing the differentiation of peripheral blood mononuclear cells to osteoclasts via chemotaxis without cell - to - cell interaction . 
the mononuclear spindle - shaped cells of gctb were generally considered to be truly neoplastic [ 38 ] and some authors [ 39 ] speculated that gctscs were originated from mesenchymal stem cells ( mscs )  . 
according to some recent studies [ 36 , 40 ] of osteoblast lineage characteristics , gctb was found to exhibit osteoblast lineage properties to derive from mature osteoprogenitors or immature osteoblasts , rather than mscs . 
however , the histogenetic aspects of gctb remain enigmatic . despite the controversy surrounding the histogenesis of gctb , many authors have investigated the genetic and molecular prognostic factors associated with this tumour type ( table 1 ) with the intent to contribute to clinical treatment . 
 [ 60 ] year 2005 2010 2008 2009 2011 2006 2013 2013 2013 2009 radiol med ( 2017 ) 122 : 505519 chromosomal abnormalities telomeric associations telomeric fusion tenascin c , ploidy status telomere maintenance glutathione peroxidase 1 ect 20q11.1 amplification p53 mutations p63 expression b - catenin expression vascular endothelial growth factor , matrix metalloproteinase - 9 telomeric dna repair and protection were found to be initially responsible for the telomeric associations and genetic instability that led to tumourigenesis [ 41 , 42 ]  . 
although aneuploidy alone was an insufficient prognostic predictor [ 43 ] , an investigation of magnetically separated cd68 - negative neoplasm cells indicated that the combination of chromosomal abnormalities and telomeric associations might comprise a risk factor for the local recurrence of gctb [ 44 , 45 ]  . the results of a comparative genomic hybridization array ( acgh ) performed to investigate abnormal genomic changes in recurrent gctb identified a 1 - mbp gain at 20q11.1 as the responsible factor . 
 [ 47 ] demonstrated a significant association of epigenetic silencing with tumourigenesis through dna methylation analyses ; however , no studies have addressed the relationship between epigenetic silencing and local recurrence of gctb . 
in the bone , the microrna ( mirna ) mir - 126 - 5p [ 48 ] plays a significant inhibitory role by regulating mmp - 13 expression in gctbs ; accordingly , this mirna might be considered a risk factor of local recurrence . 
these proteins , which included glutathione peroxidase 1 ( gpx1 ) , thioredoxin peroxidase ( prx ) , allograft inflammatory factor 1 ( aif1 ) , and ubiquitin e2 n ( ube2 n ) , were validated as new markers predictive of aggressive gctb behaviour in a prospective cohort study . 
gpx1 , a target of p53 , was found to correlate strongly with local recurrence following p53 mutation [ 45 , 49 ]  . high expression of p63 [ 50 , 51 ] distinguishes gctb from other giant cell - containing lesions of the bone and soft tissues and , therefore , plays a role in the differential diagnosis of these tumours . 
however , de la roza [ 52 ] demonstrated that the specificity on p63 overexpression was insufficient when distinguishing gctbs from primary aneurysmal bone cysts ( abcs ) and chondroblastomas . 
however , de la roza observed a significantly higher proportion of cases with strong staining intensity and / or large numbers of p63 - positive cells among gctb cases , compared to abc and chondroblastoma cases [ 52 ] , as well as significant upregulation of tp73l , which encodes p63 [ 51 ]  . 
overall , further studies are needed to establish optimal criteria for p63 positivity . the roles of cytokines and proteins in tumourigenesis and the biological behaviours of gctb have been evaluated using various methods . 
some authors observed high b - catenin expression in recurrent tumours , relative to primary tumours [ 55 ] , suggesting activation and involvement of the wnt / b - catenin pathway in local recurrence . 
furthermore , tenascin c ( tnc ) was identified and confirmed via real - time polymerase chain reaction ( pcr ) as one of the most significant prognostic biological markers [ 57 ]  . 
additional studies of the link between osteoclast activity and inflammation are needed to identify prognostic factors for gctb [ 45 ]  . the use of denosumab , a rankl - specific monoclonal antibody , for the treatment of gctb follows the clinical implications of molecular and genetic investigations . 
in 2013 , the us food and drug administration approved denosumab for use in patients with recurrent / unresectable / metastatic gctb or those in whom surgery would cause excessive morbidity [ 6 ]  . 
furthermore , mr provides information about the margins and number of soft tissue extensions and involvement of adjacent tissues , and can depict liquefaction and necrosis when intravenous gadolinium contrast is used [ 13 , 14 , 33 ]  . evaluating characteristics of gctb imaging findings have allowed evaluations of disease sever ity . 
the following characteristics of gctb were identified : characteristics of gctb tumour location and size , presence or absence of osteosclerosis , signal intensity and enhancement , cystic changes and intratumoural bleeding , among others . impacts of gctb on surrounding tissues peritumoural oedema , soft tissue mass formation , tumour edge morphology ( smooth or penetrating irregular margins ) , bone cortex losses , adjacent joint involvement , expansile changes , pathological fracture , etc . bone crest a highly dense , spine - like bone crest in the periphery of a gctb can be visualized using ct , especially in the bone window . 
this bone crest , a manifestation of osteosclerosis , can cause difficulty during curettage . paint brush borders sign on mr imaging , the paint brush borders sign indicates the protrusion of an irregular edge from the gctb toward the bone . 
t1 - weighted images provide a stark contrast between the high signal intensity of the bone marrow and low signal intensity of the tumour tissue and , therefore , display the paint brush borders sign more effectively than other sequences . 
morphologic analysis of the tumour edge might provide information about tumour residues , which have been suggested as the culprit of local recurrence . peritumoural oedema peritumoural oedema manifested as an area of significantly high signal intensity on fat - suppressed mr imaging to evaluate joint effusion and oedema . 
theoretically , peritumoural oedema is a reaction to tumour activity and is associated with the aggressiveness of gctb . poor bone cortex integrity bone cortex destruction could be detected by computed tomography ( ct ) or magnetic resonance ( mr )  . 
poor bone cortex integrity is a result of gctb aggressiveness . expansile bone destruction expansile osteolytic bone destruction on radiography is a characteristic of gctbs and may be associated with a longer disease duration . soap bubble sign the soap bubble sign is another characteristic radiographic feature of gctb . 
together with expansile bone destruction , the soap bubble sign is a manifestation of the slow processes of osteogenesis and osteolysis , resulting in the compression and invasion of adjacent bone trabecula with osteosclerosis . in cases of gctb , adjacent adjacent soft tissue invasion soft tissue invasion is indicative of tumour aggressiveness and complicates surgical procedures . 
compared with ct , mr can more sensitively detect soft tissue involvement . cystic cystic changes with or without fluidfluid levels changes and fluidfluid levels indicate liquefactive necrosis and intratumoural haemorrhage . 
necrosis has a close relationship with elevated 1 3 510 radiol med ( 2017 ) 122 : 505519 vegf levels , and elevated vegf levels can , in turn , damage vascular endothelial cells ; together with subsequent narrowing of vessels due to fibrosis , this vascular damage can result in oedema and necrosis [ 61 , 62 ]  . 
found that in cases of advanced gctb , elevated vegf and mmp - 9 levels correlated well with local recurrence [ 63 ]  . as we mentioned previously , the campanacci classification [ 31 ] has been used to predict local recurrences of gctb . 
 t1 - weighted magnetic resonance ( mr ) image shows homogeneous low signal intensity in the tumour , whereas a t2 - weighted mr image shows intermediate - to - high signal intensity . 
the loss of bone cortex on axial ct ( c ) corresponds to a discontinuous area of low signal intensity on an axial t2 - weighted mr image ( white arrow )  . 
patients with gctb should be followed up prospectively after clinical treatment , and imaging features might be correlated with prognosis . gctbs comprise mononuclear cells and multinucleated osteoclast - like giant cells . 
in our previous immunohistochemical study , we demonstrated that multinucleated osteoclast - like giant cell activities , specifically the effects of mmp - 9 , were responsible for osteolytic destruction . 
prospective studies with large sample sizes would allow more definite conclusions . role in surgical guidance radiological evaluation can be used to guide surgical treatment and should play a key role in determining the optimal approach that balances limb function and local control . 
 our investigation [ 33 ] demonstrated that the rate of recurrent gctb with soft tissue extension after intralesional curettage was higher if the soft tissue extension was large , multiple and lacked bone envelope integrity . 
 given the possibility of residual gctb tissue , the tumour margins , involvement of adjacent tissues and tumour edge morphology ( smooth or penetrating irregular margins ) are crucial factors when making decisions about surgical options . 
therefore , mri could be used to identify tumour residues or recurrence postoperatively and predict outcomes of surgical treatments . 1 3 radiol med ( 2017 ) 122 : 505519 1 3 512 radiol med ( 2017 ) 122 : 505519 fig . 
1 continued our review of recent studies of various prognostic factors led us to agree with some authors [ 10 , 34 , 64 ] and advocate a new evaluation system with which to direct gctb treatment ; additionally , more prospective studies with large sample sizes are needed to reliably investigate prognostic factors . 
moreover , a multiple perspective evaluation system that includes clinical features , imaging findings , pathology , and genetic and molecular prognostic factors should be established . regarding molecular and genetic factors , the tumourigenesis of gctb remains unclear ; however , authors [ 5 , 36 , 40 ] have studied the characteristic cellular expression patterns associated with the biologic behaviours of gctb [ 38 , 48 , 49 , 54 , 56 ]  . 
on the t1and t2 - weighted mr images , the tumour appears as a homogeneous area of low - to - intermediate signal intensity and as a heterogeneous area of intermediate - to - high signal intensity , respectively . 
 in addition , marked high signal intensity and low fluidfluid levels suggestive of polycystic components were observed on t2 - weighted images ; these may be consequential to haemorrhage or secondary aneurysmal bone cyst formation . 
we speculate that some factors associated with the soft tissue around the gctb might correlate closely with tumourigenesis and recurrence , even in the absence of cell - to - cell interactions . 
further research is needed to verify our speculation . gctb and giant cell reparative granuloma ( gcrg ) exhibit different predilections regarding localization and p63 expression [ 50 , 51 ] ; however , the lesions exhibit similar imaging findings , histopathological appearances and age of onset . 
 in accordance with this speculation , many authors [ 45 ] have reported that the growth factors and cytokines associated with bone resorption and osteoclast activity might also be crucial pro - inflammatory factors . 
an understanding of the mechanisms underlying inflammation might provide more insights into gctb histogenesis . studies of p63 expression [ 5153 ] revealed a higher rate of p63 positivity among gctbs , as well as stronger 1 3 514 radiol med ( 2017 ) 122 : 505519 fig . 
b , c coronal t1 - weighted and t2 - weighted magnetic resonance ( mr ) images indicate the gctb lesion as a homogeneous area of intermediate signal intensity and a heterogeneous area , respectively . 
a , b sagittal t1 - weighted magnetic resonance ( mr ) and stir images show the lesion as an area of homogeneous low signal intensity and an area of heterogeneous high signal intensity surrounded by oedema , respectively . 
c , d coronal and axial t2 - weighted mr images show the gctb lesion as an area of heterogeneous intermediate - to - high signal intensity ; necrosis appears as an area of high signal intensity . 
rankl is thought to play a role in gctb pathophysiology , and the monoclonal anti - rankl antibody , denosumab , was approved for therapeutic use [ 6 , 66 ]  . 
this research has inspired us to identify additional tumourigenic pathways . methodologically , researchers might initiate new ideas that would clarify our future perspectives and investigations 1 3 515 radiol med ( 2017 ) 122 : 505519 fig . 
a giant cell tumour of the bone ( gctb ) in the distal femur is sectioned and processed for matrix metalloproteinase ( mmp ) staining and subsequent histologic examination fig . 
6 representative immunohistochemistry slides of paraffin - embedded giant cell tumour of the bone ( gctb ) peripheral tissue specimens stained for matrix metalloproteinase - 9 ( mmp - 9 )  . 
7 representative immunohistochemistry slides of paraffin - embedded giant cell tumour of the bone ( gctb ) central tissue specimens stained for matrix metalloproteinase - 9 ( mmp - 9 )  . 
therefore , we can use in conclusion , the identification of prognostic factors is crucial to the balance of local control with functional preservation during the treatment of gctb , as well as to the reduction of local recurrences . 
researchers should advocate the correlation of imaging features with clinical , pathologic , molecular , and genetic aspects of gctbs in an attempt to establish a multiple perspective evaluation syste following our comprehensive review of current studies on prognostic factors of local recurrence of gctb , we propose that additional prospective studies with larger sample sizes are needed to ensure reliable 1 3 radiol med ( 2017 ) 122 : 505519 fig . 
a , b a local recurrence of giant cell tumour of the bone ( gctb ) was detected via mr after curettage with adjuvant cement use , whereas no significant evidence of local recurrence was detected via x - ray examination . 
sagittal - lung ct measurements in terms of bilateral lung height ( lh ) , anterior - posterior lung diameter ( apld ) , diaphragm height ( dh ) , and anterior sternodiaphragmatic angle ( asda ) , as well as inter - pulmonary septum length ( ipsl ) on axial images were measured both before and after bronchodilator ( bd ) administration . 
the acos patients had larger post - bd variations of sagittal - lung ct measurements than patients with pure copd . keywords chronic obstructive pulmonary disease ( copd ) asthma - copd overlap syndrome ( acos ) computed tomography ( ct ) introduction chronic obstructive pulmonary disease ( copd ) is currently defined as a lung disease characterized by persis tent airflow limitation that is not fully reversible [ 1 ]  . 
it is , therefore , important to have more proper patient sub - classification and to select right population for more specific treatment . there is a significant proportion of copd patients exhibiting clinical manifestations of asthma , which is broadly recognized but poorly characterized and makes the diagnosis more complex [ 4 , 5 ]  . 
patients with asthma and copd overlap syndrome ( acos ) always experience more frequent exacerbations , more rapid declines in lung function , and higher mortality rates compared with those 1 3 488 radiol med ( 2017 ) 122 : 487494 suffering from either alone [ 6 , 7 ]  . 
this means acos may be a distinct phenotype from copd and may require distinct management [ 4 ]  . in recent years , the introduction of computed tomography ( ct ) has completely revolutionized the diagnosis of interstitial lung diseases [ 8 ]  . 
through objective quantification of parenchymal destruction , many indexes obtained from chest ct have been proposed to help achieving clinically meaningful phenotype of copd patients , such as the air trapping index ( ati ) , the emphysema index , the percentage of lung volume occupied by low attenuation areas ( laa% ) , the ratio of expiratory / inspiratory lung density ( e / i ratio ) , the longitudinal shape heterogeneity of airway lumen , the wall area percentage ( wa% ) of small airway , and the ct - based functional lung volume ( flv ) [ 915 ]  . 
 [ 16 ] demonstrated that patients with acos had lower ei , greater post - bronchodilator variations in expiratory ati , and larger lung density , compared to pure copd patients . however , all these methods necessitate complicated software or algorithm which are not feasible for clinical practice . 
in this study , we attempt to investigate if this method can distinguish patients with acos from those with pure copd . materials and methods patient selection or destroyed lung ; ( 2 ) thorax malformation or pulmonary resection ; ( 3 ) any sign of infection or copd exacerbation within 4 weeks before / after ct examination ; ( 4 ) post - bronchodilation fev1 / fvc of 0.7. 
all patients were further sub - classified based on the severity of copd according to the new gold guidelines [ 1 , 19 ]  . imaging techniques of ct subjects were scanned with 1 of 2 machines : ge light speed 16 ( ge medical system , milwaukee , wi , usa ; 81 ) and philips brilliance ict ( 256 slices , philips 53 )  . 
each patient healthcare , cleveland , oh , usa , n was examined before and after bronchodilator ( bd ) administration of salbutamol ( ventolin aerosol , 400 g , glaxosmithkline ) within 3 h . 
the scanning parameters were 120 kv , 100 mas , collimation configuration of 16 time of 0.5 s for ge light speed 16 scanner ; and 120 kv , 100 mas , collimation configuration of 20 0.625 mm , pitch of 0.55 , and rotation time of 0.4 s for philips brilliance ict scanner . 
subject was diagnosed as acos when having a fev1 / fvc of < 0.7 , emphysema on hrct of < 15% , and either a history of asthma or hay fever with improvement in fev1 > 200 mls and > 12% following bronchodilator administration or marked improvement in fev1 > 400 mls and > 15% following bronchodilator administration regardless of history of asthma or hay fever [ 4 , 18 , 19 ]  . 
 patients that had any one of the following conditions were excluded : ( 1 ) a history of other respiratory diseases , like lung cancer , pneumothorax , hydrothorax , bronchiectasis , cystic fibrosis , immune deficiencies , tuberculosis sequelae analysis of ct images in a separate sitting , two radiologists ( 7 and 9 years of experience , respectively ) performed the following measurements on sagittal ct at the junction between the medial and middle thirds of each hemidiaphragm as done by hightower et al . 
retrosternal lucency is measured as maximum length of interpulmonary septum ( white arrow ) spirometry of pulmonary function according to the european respiratory society ( ers ) / american thoracic society ( ats ) guidelines [ 20 ] , lung function test was carried out before and 20 min after inhalation of 400 g salbutamol using a spirometer ( jaeger master screen , viasys healthcare , hochberg , germany ) within 1 week before / after ct scanning . 
the forced vital capacity ( fvc ) , forced expiratory volume in one second ( fev1 ) , fev1 / fvc ratio , specific airway resistance ( r aw ) , and residual volume / total lung capacity ( rv / tlc ) were analyzed . statistical analysis inter - observer agreement on ct measurements between the two reviewers was analyzed by calculating intra - class correlation coefficients ( iccs )  . 
the students t test and paired t test were used for analyzing differences of numerical variables and the preto postbd variations of sagittal - lung ct measurements between copd and acos patients . 
the body mass index , the prevalence of smoker , and the gold classifications of patients were also homogeneously distributed between the copd patients and the acos patients ( p > 0.05 , table 1 )  . characteristics of patients spirometry the pulmonary functional parameters of patients were summarized in table 2 . 
the pre - bd fev1% , fev1% predicted , fev1 / fvc ratio , specific r aw , and rv / tlc were not significantly different between the patients with copd and those with acos . 
however , after bd administration , the acos patients presented with smaller left lh , bilateral apld and , bilateral asda , but larger right dh , as compared to the pure copd patients ( p values all < 0.05 ) , although right lh , left dh , and ipsl were not different between patient groups . 
as shown in table 5 , post - bd left lh , right dh , bilateral apld , and asda presented with limited diagnostic accuracies in distinguishing patients with acos from those with copd alone , although their inter - group differences were significantly different ( table 4 )  . 
the acos patients presented with larger variations of sagittal - lung ct measurements than patients with copd when administrated with bronchodilator , which showed excellent diagnostic performance in differentiating these two disease entities . 
these findings were consistent with patients pulmonary functional parameters and corresponding changes after bd administration . current evaluation for features of obstructive airway diseases with hrct relies primarily on axial reconstructions . 
therefore , the sagittal - lung ct reconstructions and measurements are more feasible for clinical practice than the various indexes proposed in recent years which were based on axial images . the traditional indexes for evaluating pulmonary function like emphysema index , air trapping index , and functional lung volume can be very specific for obstructive airway diseases [ 913 , 16 , 22 ]  . 
 [ 17 ] had already confirmed the reliability and reproducibility of the new method used in this study , which showed higher accuracy and less inter - observer variability than the traditional methods in determination of copd . copd is characterized by a large amount of heterogeneities . 
spirometry cannot fully reflect the various phenotypes of this pathophysiologic abnormality that was associated with heterogeneous conditions , although it is essential for making a diagnosis and for assessing severity of copd [ 22 ]  . 
in recent years , many efforts have been made in characterizing acos from pure copd based on different clinical features , radiographic findings , and diagnostic tests [ 26 , 27 ]  . 
 [ 16 ] have revealed in their study that acos is a distinct phenotype to copd in respect of traditional ct densitometry , namely patients with acos always exhibit lower extent of emphysema and greater post - bd variations in air trapping , compared to patients with copd . 
in this study , we had also found different features of acos patients on post - bd sagittal - lung ct reconstructions , and larger variations of sagittal - lung ct measurements from pre - bd to post - bd , than those in patients with copd alone . 
it remains difficult to identify the cause underlying the varieties observed , which may be attributed to the characteristic in acos patient that the expiratory air flow limitation and dynamic hyperinflation are , to some extent , intermittent and reversible , while air flow limitation of copd patient is progressive and irreversible [ 25 , 28 ]  . the most important muscle for inspiration is the diaphragm , and the most important muscle for expiration is located in the abdominal wall . 
a method based on 3d lung motion assessments by using inspiratory / expiratory thin - section ct had confirmed its capability in assessing pulmonary function loss in copd patients [ 14 ]  . 
the mechanisms underlying these alternations were not fully elucidated , but they appear to be related to the degree of airflow limitations : hyperinflation of the rib cage , changes in diaphragmatic function , and increased contribution of accessory inspiratory muscles to the chest wall motions . 
as acos and copd share many characteristics , it is reasonable to assess the alternations of patients with acos from patients with copd based on sagittal - lung ct measurements that are highly linked to lung inflation . the findings of this study exhibited some useful implication to clinical practice . 
when acos is confirmed , the initiation of corticosteroid together with a long - acting 2 agonist is recommended , irrespective of the severity of copd [ 3 , 29 ]  . 
the post - bd variations of sagittal - lung ct measurements indicated the possible diagnosis of acos and prompted the treatment for reversible airflow limitation . 1 3 radiol med ( 2017 ) 122 : 487494 concomitant asthma and copd are common in a significant proportion of adult and elderly patients who present with symptoms of chronic airway disease . 
the precise proportion of patients with features of both diseases is highly variable , with the prevalence rates between 15 and 55% having been reported depending on the diagnostic criteria applied [ 6 , 24 , 25 , 30 ]  . 
current diagnostic criteria have proven insufficient for capturing all patients with the disease as many patients never receive spirometry , let alone postbd spirometry , which is essential to the diagnosis of acos . 
 acos represents a distinct clinical phenotype with more frequent exacerbations and hospitalization , worse quality of life , and higher healthcare costs than either disease alone [ 25 ]  . 
consistent use of sagittal reconstructions to look for characteristics of obstructive airway disease such as those identified here , may increase the accuracy of ct as a diagnostic tool for acos . 
at the very least , these features will help radiologists to better direct clinicians to look for definitive evidence of acos on spirometry and initiate ear lier treatment . our study has several limitations . 
 we were limited by the lack of additional measurements such as sputum cellular profiles , airway hyper - responsiveness , and fractional exhaled nitric oxide to confirm the diagnosis of acos . 
thus , the population studied may not accurately represent the majority of patients who receive chest cts and may be biased toward patients with known underlying lung disease or concerning symptoms . 
as a consequence of working and training together , our radiologists might read more similarly to each other than to radiologists at other institutions . conclusions sagittal - lung ct measurements enable differentiating patients with acos from those with copd alone . 
the acos patients presented larger variations of sagittal - lung ct measurements than patients with copd alone when administrated with bronchodilator . acknowledgements the authors would like to thank the staff of the department of radiology , zhongnan hospital of wuhan university for their assistance to this study . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . compliance with ethical standards this study was approved by the institutional ethics committee of our hospital . 
all procedures performed in this study involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
however , i would like to address a few remarks . permanent pacemakers ( pms ) and implantable cardioverter defibrillator ( icd ) are advanced , implantable devices which can transmit electrical stimuli from a battery to heart via electrodes contacting to heart . 
new features added to cardiac implantable electronic devices over time make these devices more durable , physiological and safer with improved reaction to requirements of body [ 14 ]  . cardiac side effects can be seen during or after radiotherapy delivered to breast or chest wall . 
reported that radiotherapy did not increase need for permanent pms and icd as it did not lead increase in severe ventricular arrhythmias or cardiac conduction abnormalities [ 2 ]  . * yasemin benderli cihan cihany@erciyes.edu.tr 1 department of radiation oncology , kayseri education and research hospital , 38010 kayseri , turkey the patient population with permanent pms or icd requiring radiotherapy is expanding in the community . 
 temporary or permanent damage may occur according to type and dose of radiation , device used in therapy and type of cardiac implantable electronic device ( cied ) [ 26 ]  . 
 although diagnostic radiation have no significant effect on cied , high - energy radiation ( high - energy gamma beam , electrons , protons and neutrons ) used in cancer therapy can lead serious problems . 
many different problems can occur in the mechanisms used for detection and discontinuation of tachyarrhythmia in permanent pms and icds via direct effect or electromagnetic interference ( emi ) caused by high - energy ionizing radiation [ 2 , 6 , 7 ]  . 
reported that malfunction rate was 21% in neutron - producing radiotherapy and 0% in non - neutron producing rt , recommending use of non - neutron producing rt if possible clinically [ 6 ]  . 
in a study on 33 patients underwent rt in the presence of icd , it was suggested that energy applied should be below 10 mv to protect icd [ 3 ]  . problems such as inappropriate shock delivery to overdetection , ventricular tachyarrhythmia , excessive prolongation in charging time and decreased generator capacity have been reported depending on total dose and dose rate used in radiotherapy . 
emphasized that radiation dose delivered to patients with icd should be 300 mu / min ( monitor unit / min ) [ 4 ]  . currently , permanent pms and icds produced using complementary metal oxide semiconductor ( cmos ) technology have become more sensitive to radiotherapy . 
authors reported that lead blocks reduced dose delivered to cieds by 13% in average [ 5 ]  . in conclusion , the effects of radiation on cied is unknown in patients undergoing radiotherapy . 
the knowledge about potential problems related to radiation type , dose , device used in therapy and pacemaker type and taking measures with provision of treatment are important to prevent and reduce morbidity and mortality . 
the lesions included 12 extrapleural hematomas ( 8 post - traumatic and 4 from other causes ) , 3 extrapleural lesions from pleural infection extension , 9 extrapleural lesions from metastases . 
mdct multiplanar minimum intensity projection ( minip ) reconstructions were always obtained ; t - us and mdct findings were correlated . results among 9 patients who underwent t - us 4 / 9 the ultrasonography fat extrapleural sign . 
 showed among 24 patients who underwent chest mdct all show the well - known computed tomography ( ct ) extrapleural fat sign and new auxiliary ( mdct ) findings that serve to strengthen the diagnosis of correct intrathoracic extrapleural space attribution of lesion . conclusions mdct with its multiplanar capabilities and post - processing minip reconstructions and thoracic us play a prominent role in the identification and * tullio valente tullio.valente@gmail.com 1 department of diagnostic imaging , section of general radiology , azienda ospedali dei colli , p.o. 
the amount of extrapleural fat is greater at the posterolateral thoracic region between the fourth and eighth ribs and can result in fat pads several millimeters thick , which extend into the intercostal spaces . 
1 a anatomical axial section , b corresponding scheme and c axial mdct of extrapleural space ( es ) in a patient with pleural metastases and effusion associated with es thickening . 
 es ( white arrow in a ) includes extrapleural fat , endothoracic fascia ( green line in b ) and innermost intercostal muscle ( inner orange line in b ) ; it lies between the parietal pleura ( external red line in b ) and the inner surface of the ribs . 
external to parietal pleura , an adipose tissue layer or extrapleural fat ( 2 in b , c and white arrow in c ) of variable thickness ( average 250 m ) separates the pleura from the endothoracic fascia . 
beyond innermost intercostal muscle and between the ribs lies the intercostal fat ( 3 in b , c and black arrow in c ) , which contains the intercostal vessels and the nerve ( in a consistent pattern , from superior to inferior : intercostal vein , artery , and nerve ) .and is defined by internal and external intercostal muscles ( outer thicker orange line in b and black triangle in c ) unit ( hu ) , usually seen as a 1 mm thick low attenuation line on chest ct and is almost imperceptible in healthy individuals . 
the endothoracic fascia covers the inner surface of the innermost intercostal muscle , ribs , costal cartilages and sternum and fuses with the prevertebral fascia posteriorly , acting as a continuous fibroelastic lining of the thoracic cavity ; it represents the outermost membrane of the thoracic cavity and provides an extrapleural surgical plane [ 7 ]  . 
between the endothoracic fascia and the inner surface of the ribs , the relatively thin innermost intercostal muscle extends between adjacent ribs in most of the lateral side of the chest wall , largely incomplete in the anterior and posterior portion of the thoracic wall , where other muscles , such as the transverse thoracic anteriorly and subcostal muscles posteriorly , can occupy the same relative plane . 
the es is an integral part of the intercostal stripe in ct , an 12 mm thick soft tissue stripe in the anterolateral and posterolateral intercostal spaces at the point of contact between the lung and the chest wall . 
intercostal stripe is formed by the sum of multiple layers ( visceral pleura , fluid filled pleural space , parietal pleura , extrapleural fat , endothoracic fascia and innermost intercostal muscles ) [ 2 ]  . 
without disruption of the parietal pleura , extrapleural masses such as primitive and metastatic tumors , lymph nodes involvement , an abscess , a fluid and / or air collection , an accumulation of blood in the es , displace the overlying extrapleural fat centrally ; the latter condition results in an extrapleural hematoma ( eph ) and is most commonly due to injury to intercostal or internal mammary arteries or veins or from paravertebral muscle trauma [ 812 ]  . 
according to their main constituent , intrathoracic extrapleural lesions are classified into air - containing lesions , fat - containing lesions and soft tissue - containing lesions [ 12 ] ( table 1 )  . 
 the ct extrapleural fat sign in computed tomography ( ct ) the well - known extrapleural fat sign is represented by inward displacement of the extrapleural fat stripe by an extrapleural fluid collection or mass . 
outer collection has increased attenuation , consistent with extrapleural hematoma separated from pleural fluid by parietal pleura and extrapleural fat the purpose of this study was to review the normal anatomy of the extrapleural space , its soft tissue - containing lesions , and to illustrate the extrapleural fat sign with multidetector computed tomography ( mdct ) and ultrasound ( us ) , which was never described so far . materials and methods the study was performed retrospectively on the material and data available in our department and has therefore been performed in accordance with the ethical standards laid down in the declaration of helsinki in 1964 and its subsequent amendments . 
patients were informed and expressed their consent for the use of such material for cumulative and statistical studies . using computerized searches of our pathology and radiology information systems for the time period between december 2010 and september 2015 , we identified 28 consecutive patients who had undergone multidetector computed tomography ( mdct ) and thoracic sonography ( t - us ) for chest examination with citologically / histologically or surgically proven extrapleural soft tissue - containing lesions only in 24 patients . 
 axial ct scans were acquired using a detector configuration of 64 1.25 mm ; pitch factor 0.75 ; gantry rotation time 0.5 s ; 120 kvp ; 100500 mas in automated exposure control ( aec ) with patients in the supine position and during maximal inspiration . all ct data were transferred to a workstation ( adw 4.1 ge ) ; in each mdct examination thin - section multiplanar minip reformatted images centered on medially displaced extrapleural fat were routinely obtained . 
t - us was performed in only 9 patients with iu 22 ultrasound unity ( philips healthcare ) using a linear high - mhz transducer with bandwidth of 8.012.0 mhz , or , when deeper penetration was needed , using a curved microconvex 5.08.0 mhz probe and / or a convex 3.05.0 mhz frequency transducer , evaluating chest lesions in transverse , sagittal and oblique planes . 
 static images and cine loops were stored in a commercially available picture archiving communication system ( pacs )  . with analysis of images mdct multiplanar minip and curved reconstructions , we were able to identify and to emphasize new simple ancillary signs : mdct fat ghost ribs sign generated by the dislocation of the extrapleural fat of the intercostal spaces between the fluid of pleural effusion and extrapleural lesion ( fluid or mass )  . 
it is caused by a greater presence of displaced fat in the intercostal spaces compared to that present inside of the ribs . the displaced fat of the intercostal spaces reproduces the morphology and course of the ribs . 
the extrapleural fat of the intercostal spaces dislocated on the border between the two fluid collections , reproduces the morphology of the ribs generating the sign mdctthe fat ghost ribs . 
the largest diameter ( black line ) of the eph convexity is corresponding to the traumatized ribs ( arrows ) 1 3 radiol med ( 2017 ) 122 : 479486 fig . 
the presence of a thin hypodense band convex towards the chest cavity ( arrows ) due to medial dislocation of the extrapleuric fat suggests the extrapleural pertinence of the lesion . 
the first of them is not subject to movements with the acts of breathing . statistical analysis the small size and the inhomogeneity of our study sample ( table 2 ) undermine the effective values of probability of detection and true negative rate . 
a , b us posterior axial and sagittal views clearly show the anterior medial dislocation of the extrapleural fat represented by a continuous hyperechoic band ( arrows ) and the extrapleural hematoma with biconvex morphology and highly inhomogeneous contents due to large clots ( stars )  . 
note the associated left pleural effusion table 2 small sample size , inhomogeneous group extrapleural pleural lesion es metastases es infection mdct 28 pts t - us 9 / 28 pts table 3 values of probability of detection and true negative rate of mdct and t - us auxiliary signs mdct fat ghost ribs sign t - us extrapleural fat sign the sensitivity and specificity of mdct and t - us signs by a contingency table . for mdct fat ghost sign we have calculated sensitivity of 82% and specificity of 80% , while for t - us extrapleural fat sign we obtained , respectively , 80 and 75% ( table 3 )  . results the lesions included 12 extrapleural hematomas ( eph ) ( 8 as a result of blunt trauma to the chest wall , 1 case due to ruptured thoracic aortic aneurysm , 1 case occurred in patient undergoing anticoagulation therapy , 1 iatrogenic from central venous catheter insertion and 1 from chest tube misplacement ) , 3 extrapleural lesions from pleural empyema extension ( one of tubercolous nature ) , 9 extrapleural lesions from metastases ( 6 lung cancer , 1 mesothelioma , 1 breast carcinoma , 1 renal cell carcinoma )  . 
in almost all patients ( 8 of 9 ) undergoing thoracic ultrasound ( t - us ) , there was pleural effusion while only in 1 of them there was not present . 
in 3 / 9 cases we have not identified t - us extrapleural fat sign . associated rib fracture lines with discontinuity of the anterior rib margin were sonographically identified in 4 of traumatized patients . 
extrapleural fat is a component of the loose connective tissue of the endothoracic fascia , contains the intercostal vessels and nerve . current generation multidetector ct ( mdct ) scanners ( 16 sections and beyond ) generate data sets with high spatial and contrast resolution with isotropic voxels , and allow detailed multiplanar reconstructions ( mpr ) in post - processing evaluation . 
although axial sections remain the mainstay of chest diseases interpretation , specialized three - dimensional ( 3d ) reconstruction techniques permit the visualization of anatomical details , which would be difficult to evaluate using axial reconstructions alone . 
minip images are useful for highlighting hypodense voxels and structures ( e.g. , fat tissue ) within the volume imaged and along with curved multiplanar reconstructions allowed us obtaining new simple mdct auxiliary findings to recognize extrapleural masses and fluid collection . the increasing role of t - us in the evaluation of chest abnormalities , particularly in the emergency and critical care settings is well known [ 1315 ]  . 
it is a fast and effective way of diagnosing pleural effusion that has typical anatomic boundaries of chest wall , diaphragm , and lung , can specifically differentiate effusion from consolidated lung , identify septations within the fluid better than ct imaging [ 16 , 17 ]  . 
less common causes of eph include aortic rupture , anticoagulation therapy , penetrating trauma , hemodialysis patients , and iatrogenic injury ( during insertion of a thoracostomy tube , of a central catheter ) [ 811 , 18 ]  . 
eph are collections variable from small amount up to massive formations with mixed content due to the presence of clots and represent pathological conditions with difficult clinical diagnosis and management . 
particularly , recognition of extrapleural hematoma is important because it can expand rapidly and cause respiratory or circulatory collapse [ 1921 ]  . clinical and surgical management of extrapleural hematomas appears to be conditioned by some ct findings . 
large hematomas are usually biconvex , which is suggestive of arterial rather than venous bleeding , and thus may require surgery or transcatheter arterial embolization [ 21 , 22 ]  . 
a nonconvex eph is usually smaller and may be treated conservatively because it is more often caused by venous ( low - pressure ) bleeding [ 8 , 23 ]  . primary infection or abscess of the chest wall is rare , it can occur spontaneously or in association with diabetes mellitus , immunosuppression and trauma [ 24 ]  . 
tuberculosis ( tb ) of the chest wall constitutes between 1 and 5% of all cases of musculoskeletal tb , commonly occurs with pulmonary tb and may expand into the extrapleural space [ 25 ]  . three mechanisms are described in the pathogenesis of chest wall abscess : direct extension from pleural or pulmonary parenchymal disease , hematogenous dissemination of a dormant tuberculous focus , or direct extension from lymphadenitis of the chest wall . 
direct extension of a pulmonary or pleural neoplastic lesion into the extrapleural space is most frequently encountered in patients with malignant tumor . the majority of chest wall tumors are rib tumors , including metastasic disease , multiple myeloma of the ribs and primary chest wall tumors such as malignant mesothelioma . 
direct invasion into the extrapleural space by malignancies of the lung parenchyma can also occur . the correct recognition and classification of these conditions thus appears essential for optimal patient outcome . 
 1 3 486 radiol med ( 2017 ) 122 : 479486 the knowledge and the specificity of the main and / or ancillary mdct signs associated with not yet described t - us sign have allowed the clinical or surgical correct management of intrathoracic extrapleural space soft tissue - containing lesions . study limitation the small size and heterogeneity of the evaluated sample is one of major limitations , but the pathologies of this particular anatomical region have relatively low incidence and low frequency although this is preliminary study to be verified on a larger sample . another weakness is the pleural effusion . 
the fluid distension of the pleural cavity is a necessary condition for better identification mdct and t - us of some of the auxiliary signs discovered . conclusion current high performance mdct scanners and post - processing techniques such as minip , the main and ancillary mdct findings associated with us findings must immediately indicate to the radiologist the presence of an es mass or collection . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards research involving human participants . 
based on the us and histopathological results , locoregional tumor recurrence was assessed . results the t stages of the 186 patients were t1a ( 8.1% ) , t1b ( 21.5% ) , t2 ( 39.8% ) , t3 ( 30.6% ) , t4a ( 0% ) , and t4b ( 0% )  . 
marys hospital , college of medicine , the catholic university of korea , seoul 06591 , south korea 4 department of radiology , korea university guro hospital , korea university college of medicine , seoul 08308 , south korea 5 department of radiology , research institute and hospital , national cancer center , gyeonggi 10408 , south korea 6 department of radiology , kangbuk samsung hospital , sungkyunkwan university school of medicine , seoul 03181 , south korea 7 department of radiology , thyroid center , daerim st . 
marys hospital , seoul 07442 , south korea 1 3 radiol med ( 2017 ) 122 : 530537 keywords thyroid follicular thyroid carcinoma thyroidectomy ultrasonography recurrence introduction thyroid carcinoma is the most common malignancy involving the endocrine glands [ 1 ]  . 
they do not exhibit the characteristic nuclear features or other diagnostic features ( e.g. , psammoma bodies ) of papillary thyroid carcinomas [ 3 , 4 ]  . selection of the surgical procedure for ftc , like that for papillary thyroid carcinoma , requires preoperative ultrasonography ( us ) for detection of satellite thyroid malignancy and nodal metastasis in the neck . 
unfortunately , these us findings cannot easily differentiate ftc from follicular adenoma , and despite advances in and increased use of us , diagnosis of ftc is still challenging [ 68 ]  . 
therefore , surgical resection has been recommended as the current standard practice for diagnosing and treating ftc [ 8 ]  . although annual follow - up us is generally recommended for 35 years after surgery for differentiated thyroid cancer [ 9 ] , there is little information about the locoregional recurrence rate of ftc or the benefits of such surveillance . 
the need for informed consent was waived owing to the retrospective nature of the study . surgical treatment and histopathology all types of thyroid surgery involving a low - collar incision were performed by experienced head and neck surgeons at each institution . 
tumor stage , nodal stage , and multiplicity were assessed via histopathological review . data analyses and tnm staging demographic data ( patient age , sex , total thyroidectomy , session number , follow - up interval , and us follow - up duration ) were collected from the electronic medical record ( emr ) of each institution . 
histopathological features including primary tumor size , extrathyroidal tumor extension , cervical nodal metastasis , multiplicity ( i.e. , the presence of satellite ftc ) , and bilaterality ( i.e. , the presence of satellite ftc in the contralateral lobe ) were assessed by reviewing the histopathological results and emrs . all patients were staged by retrospective review by one radiologist at each participating hospital in accordance with the american joint committee on cancer tnm staging system , using the histopathological results and emr data [ 10 ]  . 
to determine t stage , the following histopathological parameters were evaluated : tumor size , intraglandular confinement , and extrathyroidal extension to the subcutaneous soft tissue , larynx , trachea , esophagus , recurrent laryngeal nerve , or carotid artery wall . 
the m stage was defined as m1 when distant metastasis was present . materials and methods study population followup us standard deviation ( sd ) 42.6 we retrospectively reviewed the electronic medical records ( emrs ) of 186 patients [ 146 women and 40 men ; mean age 13.7 years ; range 1184 years ] who underwent surgical resection for ftc between 2000 and 2011 at each of seven institutions . 
although each institution began selecting patients at different times , 186 patients from all institutions were twenty - five radiologists from the seven participating hospitals , whose thyroid us experience ranged from 1 to 20 years , performed the follow - up us examinations . 
us instruments ( iu 22 and hdi5000 , philips medical systems , bothell , wa , usa ; logiq9 , ge healthcare , milwaukee , wi , usa ; apolio ssa - 770a , toshiba medical systems , tokyo , japan ; eub - 7500 , hitachi medical corporation , tokyo , japan ) equipped with a 515 - mhz linear probe were used . 
however , the intervals of follow - up us varied according to the discretion of the physician or the situation of the patient , as outlined in the guidelines of each institution . 
in the literature [ 11 , 12 ] , a metastatic lymph node of thyroid malignancy on us includes round shape , hypoechoic or hyperechoic structure , loss of hilar architecture , internal calcifications or cystic appear ance , and infiltrating or irregular margfinal diagnoses of tumor recurrence were made using us - guided fine - needle aspiration or second - look surgery . statistical analysis the data were examined for normal distribution using the kolmogorovsmirnov test . 
of the five patients with satellite ftc , one showed a satellite ftc in the ipsilateral lobe , three showed a satellite ftc in the contralateral lobe , and one showed satellite ftcs in both lobes . 
on preoperative longitudinal gray - scale ( a ) and color doppler ( b ) ultrasonography ( us ) images , a thyroid nodule with homogeneous echogenicity and mixed vascularity ( arrows , 26.9 mm at its largest diameter ) is observed in the left thyroid lobe . 
in the first ( 12 months interval ) , second ( 24 months interval ) , third ( 36 months interval ) , and fourth ( 47 months interval ) followup us , there was no suspicious mass or lymph node in the neck . 
on the transverse gray - scale ( c ) and color doppler ( d ) us images , a solid mass ( arrows , 9.8 mm at its largest diameter ) in the left anterior lower neck was found , and us - guided fine - needle aspiration was immediately performed . 
on preoperative longitudinal grayscale ( a ) and power doppler ( b ) ultrasonography ( us ) images , a mixed echogenic thyroid nodule and peripheral vascularity ( arrows , 20.7 mm at its largest diameter ) is observed in the left thyroid lobe . 
 on preoperative longitudinal gray - scale us image ( c ) , suspicious lymph nodes ( arrows ) in the left mid - neck show intranodal cystic component , echogenic solid component , and loss of echogenic hilu on histopathological examination after total thyroidectomy , this nodule was confirmed as ftc , and perithyroidal tumor invasion and regional nodal metastasis were found . 
in the first ( 12 months inter val ) and second ( 24 months interval ) follow - up us , there was no suspicious mass or lymph node in the neck . 
ftc may be aggressive in the widely invasive histological variant , with a higher incidence of distant metastasis than papillary thyroid carcinoma owing to its propensity for vascular invasion [ 1315 ]  . 
nodal metastasis of ftc , however , is uncommon , with an average incidence of 10% compared with up to 50% ( including microscopic nodal metastases ) for papillary thyroid carcinoma [ 15 , 16 ]  . 
us is a simple , noninvasive , and highly sensitive imaging modality for monitoring locoregional tumor recurrence in patients with differentiated thyroid cancer [ 6 , 17 ] , and its usefulness for such patients is emphasized in the american thyroid association guidelines [ 18 ]  . 
in our study , postoperative us surveillance using high - resolution devices was performed to evaluate tumor recurrence . annual us scans in the first 35 years after surgery for differentiated thyroid cancer have been recommended for the detection of tumor recurrence [ 9 , 18 ]  . 
recently , the study by kim [ 19 ] , which examined papillary thyroid carcinoma rather than ftc , addressed this issue : their results suggest that early and frequent follow - up us sessions after hemithyroidectomy are unnecessary owing to low recurrence rates . 
in addition , our study is the first multicenter study to investigate the usefulness of early postoperative us surveillance after surgical resection in patients with ftc . in this multicenter study , the tumor recurrence rate was only 3.2% ( 6 / 186 )  . 
 the recurrence rate of ftc was much lower in our study than in other studies : previously reported recurrence rates ranged from 5 to 43% ( mean 18.2% ) [ 2024 ]  . 
the low rate of ftc recurrence in our study may reflect the meticulous preoperative imaging work - up that monitors factors indicative of poor prognosis , such as multiplicity , bilaterality , lymph node metastasis , and distant metastasis . 
in the present , we could not determine the appropriate time or interval at which postoperative us should be performed owing to the small number of patients with tumor recurrence . 
 although our data were acquired from day - to - day practice , these factors may affect the quality of the us examinations . 1 3 radiol med ( 2017 ) 122 : 530537 in conclusion , the tumor recurrence rate in patients with ftc after thyroid surgery was low , and tumor recurrence ( as monitored via us ) was rarely detected . 
we evaluated intra and interobserver agreement via blandaltman analysis , intraclass correlation coefficient ( icc ) , standard error of measurement , and smallest detectable difference ( sdd )  . 
 first , we studied the reliability of the hard tissue part of the tweed - merrifield analysis for 73 single cephalograms and for the better ones of patients with two exposures . 
intraobserver reli ability was high ( icc > 0.9 ) , whereas interobserver reliability was good ( icc > 0.83 ) except for fmpa , fmia * adrian neagu neagu@umft.ro 1 center for modeling biological sysems and data analysis , victor babes university of medicine and pharmacy timisoara , piaa eftimie murgu nr . 
2 - 4 , 300041 timisoara , romania 2 department of physics and astronomy , university of missouri , columbia , usa 3 university of medicine and pharmacy trgu - mures , trgu - mures , romania and op . 
retaking cephalograms is ethically questionable in such cases . keywords interobserver agreement intraobserver agreement lateral cephalograms subject posture introduction radiographic cephalometry allows to track the progress of orthodontic treatments , or to demonstrate the results of maxillofacial surgery [ 1 ]  . 
nevertheless , reliability studies are important in cephalometry because they give statistical estimates of typical errors of measurement [ 3 ]  . as argued by donatelli and lee [ 4 ] , the blandaltman ( ba ) method [ 5 , 6 ] is convenient for assessing intra and interobserver agreement in orthodontic research . 
a blandaltman plot conveys an intuitive picture of differences recorded in successive readings by the same observer ( intraobserver differences ) , and differences recorded by different observers ( interobserver differences )  . 
to estimate their relevance for the whole population , it is important to also specify their 95% confidence intervals [ 7 ]  . recent works on the reliability of lateral cephalometry advocate the use of the standard error of measurement ( sem ) and the smallest detectable difference ( sdd ) as measures of intraand interobserver agreement [ 8 , 9 ]  . 
an indicator of repeatability , the sdd is a statistical estimate of the smallest difference that needs to be observed to be fairly sure that a real change occurred in the measured quantity [ 1012 ]  . 
hence , a method of measurement is useful in medical practice if sdd is smaller than the minimum clinically relevant change , defined as the minimum change that clinicians expect or deem as important [ 10 , 13 ]  . the purpose of this paper is twofold : to complement reliability studies of lateral cephalometry with a ba analysis , and to assess the impact of patient positioning on the reliability of 2d cephalometric measurements . ideally , a lateral cephalogram is recorded while the midsagittal plane of the patients head is parallel with the detectors plane . 
our study aims to assess the reliability benefits of recording a second cephalogram when the first is deemed inappropriate . first , we perform a ba study of the intraand interobserver reliability of the tweed - merrifield analysis of lateral cephalograms . 
to confront our results with the literature , we also compute the two - way , random effects model intraclass correlation coefficient ( icc ) , the sem , and sdd . 
 finally , we study pairs of cephalograms , and compare statistical indicators of reliability obtained for bad and good cephalograms ( i.e. , lateral radiographs of the head recorded in inappropriate and improved position , respectively )  . materials and methods in this retrospective study , we analyzed lateral cephalometric radiographs of patients who received orthodontic treatment in our clinic . 
patients included in the study had at most subclinical facial asymmetry , as judged by an experienced orthodontist [ 14 ] , and had at least one lateral cephalogram recorded by a pax - i3d digital cephalostat ( vatech co ltd , korea )  . 
the study was approved by our institutional ethics committee . patients and cephalometric measurements a total of 104 patients were enrolled in the study ; 73 of them had a single cephalogram , whereas the other 31 had two cephalograms , recorded on the same day , because the first was deemed poor due to incorrect patient posture . 
the corresponding anatomical landmarks were averaged , as suggested by brodie [ 16 ] , being localized at the middle of the segment joining the pair of landmarks identified on the images of contralateral structures . statistical analysis four sets of cephalometric measurements , the results of two readings by two observers , were studied using statistical tools to characterize interand intraobserver reliability [ 4 , 9 , 12 ]  . to assess intraobserver reliability using the blandaltman method [ 46 ] , for each cephalometric parameter of interest , we plotted the difference versus the mean of two successive tracings by the same operator . 
to this end , we calculated n , and the t value at the standard error of the bias , sd which students probability density function with n degrees of freedom is equal to 0.05. 
1 ac lateral cephalograms recorded at incorrect ( a ) and correct ( b ) patient posture were analyzed relying on the following anatomic landmarks ( c ) [ 15 ] : s ( sellamidpoint of the pituitary fossa ) , n ( nasionmost anterior point of the frontonasal suture in the median plane ) , po ( porionsuperior point of the external auditory meatus ) , or ( orbitalelowest point in the inferior margin of the orbit ) , ar ( articularepoint at the junction of the posterior border of the ramus and the inferior border of the posterior cranial base ) , ans ( anterior nasal spinetip of bony anterior nasal spine in the median plane ) , pns ( posterior nasal spineposterior spine of the palatine bone constituting the hard palate ) , a ( subspinalepoint at the deepest midline concavity on the maxilla between the anterior nasal spine and prostion ) , b ( supramentalethe point at the deepest midline concavity on the mandibular symphysis between infradentale and pogonion ) , iii ( incision inferius incisalisincisal edge of the most anterior mandibular central incisor ) , lia ( incision inferius apicalis root apex of the most anterior mandibular central incisor ) , me ( mentonmost inferior midline point on the mandibular symphysis ) , gn ( gnathionmost anteroinferior point on the symphysis of the chin ) , go ( gonionthe constructed point of intersection of the plane tangent to the posterior border of the ramus and a plane tangent to the inferior border of the mandible ) , and ocp ( occlusal planeline on the cephalometric radiograph representing an imaginary plane at the level of the occlusion ) table 1 measurements implied in the tweed - merrifield analysis of hard tissues visualized in lateral cephalograms measurement unit description angle determined by points s , n and a angle determined by points s , n and b angle determined by points a , n , and b 4 . 
ao - bo distance between the perpendicular line from point a to the occlusal plane and a perpendicular line from point b to the occlusal plane distance in millimeters from the palatal plane to the menton distance in millimeters from the articulare to the mandibular plane along the posterior border of the ascending ramus ratio of pfh to afh intersection of the frankfort horizontal plane and mandibular plane intersection of the long axis of the lower incisor and frankfort horizontal plane intersection of the mandibular plane and the long axis of the lower incisor the measure of the slope of occlusal plane to the frankfort horizontal plane 1 . 
 ( 1 ) , denoted by icc ( 2 , 1 ) in the classification of shrout and fleiss [ 17 ] , is a measure of reliability in a study that records a single score for each subject in both trials [ 12 ]  . furthermore , we calculated the standard error of measurement , icc , sdall1 where sdall is the grand standard deviation of all 2n values recorded in two trials for each subject . 
1c , we performed the hard tissue part of the tweed - merrifield analysis of both good and bad cephalograms , and computed statistical indicators of intraand interobserver agreement . following the recommendations of donatelli and lee [ 4 ] , we first assessed the reliability of cephalometric measurements via a blandaltman ( ba ) study of the results obtained by two observers in two analyses performed one month apart . 
to assess intraobserver agreement , we performed a ba study of differences between successive measurements ; to characterize interobserver agreement , we studied the differences between the first measurement of observer 1 ( o1 ) and the second measurement of observer 2 ( o2 )  . 
in all cases , we calculated the bias and limits of agreement , as well as their 95% confidence intervals [ 7 ]  . in their study of the reliability of two - dimensional lateral cephalometry [ 9 ] , damstra et al . 
2 af intraand interobserver blandaltman ( ba ) plots for the anterior facial height ( afh ) ( a , c , e ) , and incisor mandibular plane angle ( impa ) ( b , d , f ) , defined in table 1 . 
in a ba plot , each point ( empty circle ) corresponds to one cephalogram , analyzed twice ; the plot represents the difference of two measurements versus their mean . 
 the solid horizontal line represents the bias ( the mean of differences between pairs of measurements ) , whereas the dotted horizontal lines below and above the solid line represent the lower limit of agreement ( lla ) and upper limit of agreement ( ula ) , respectively . 
shown are intraobserver ba plots of observer 1 ( o1 ) ( a , b ) and observer 2 ( o2 ) ( c , d ) , as well as interobserver ba plots that compare the first measurement of o1 with the second measurement of o2 ( e , f ) error of measurement ( sem ) [ 12 ] , and smallest detectable difference ( sdd ) , also called minimum difference or smallest real difference [ 10 , 12 ] , for 14 cephalometric measurements . 
four of their measurements , sna , snb , anb and ao - bo , are common with our analysis , showing good agreement with the first four columns of table 2 . 
3 ad blandaltman plots of interobserver reliability , constructed by comparing the first measurement of observer 1 ( o1 ) with the second measurement of observer 2 ( o2 ) , performed for good ( a , b ) and bad ( c , d ) cephalograms . 
shown are plots for the anterior facial height ( afh ) ( a , c ) and the incisor mandibular plane angle ( impa ) ( b , d )  . 
 compared the mean values of triplicate readings by the two observers [ 9 ] , whereas here we compared individual readings by the two observers , taken one month apart . 
our work is based on duplicate readings by two observers , as needed for a ba analysis . this paper contributes with a ba study to the literature concerned with the reliability of 2d cephalometric measurements . 
2 for one linear measurement ( afh ) and one angular measurement ( impa ) , the ba parameters ( bias and ula ) are reported in table 2 for all the measurements that compose hard tissue part of the tweed - merrifield analysis semi - width ( table 1 )  . 
the bias is 1 3 radiol med ( 2017 ) 122 : 520529 1 3 528 radiol med ( 2017 ) 122 : 520529 negligible for o2 , and the ula is about 5 times smaller for o2 than for o1 ; the corresponding 95% ci are also narrower for o2 than for o1 . 
indeed , when the bias is zero , the ula is equal to the so - called repeatability coefficient [ 5 ] , which is another measure of the smallest detectable difference [ 13 ] ( compare , for example , ula and sdd for afh in table 2 , intra o2 )  . 
3c , d , suggesting that , apart from a slight decrease of the difference between ula and lla , the better radiograph did not improve interobserver agreement . table 3 reveals few reliability benefits of repeated cephalograms . 
neither the bias nor the difference between ula and the bias was significantly smaller for the better radiographs ; icc was slightly lower , whereas sem and sdd were larger for the better radiographs ( reflecting less intraobserver agreement )  . 
in linear measurements ( ao - bo , afh , and pfh ) , o1 proved less reliable in the analysis of the second set of radiographs ; in contrast , o2 performed better for the better radiographs . 
the interobserver bias recorded for ao - bo , fmpa , fmia , and op , remained significant also in the analysis of the improved cephalograms . our results suggest that moderate deviations from the ideal head positioning do not affect the intraand interobserver reliability of cephalometric analysis . 
 [ 21 ] , for axial rotations and lateral flexions of the head of up to 4 , bisecting the images of bilateral structures to construct their midline image ( as proposed by brodie [ 16 ] ) , allows for precise cephalometric analyses . 
remarkably , certain measurements , such as sna , snb , and anb , suffered mild changes even for unusually large deviations from the ideal head posture ( rotations of up to 21 and tilts of up to 10 ) [ 20 ]  . an important source of error in 2d cephalometric analysis is landmark identification . 
landmarks located on anatomical edges are relatively easy to identify , whereas those located on curves , such as points g , a or b , are error - prone [ 24 ]  . 
our results are consistent with the hypothesis that projection errors affect the reliability of lateral cephalometry to a smaller extent than landmark identification errors do . the present study is limited to the evaluation of the reliability of cephalometric analysis in the context of slight variations in head positioning at a given state of the subject . 
as noted by seward [ 26 ] , averaging the positions of bilateral structures can lead to systematic errors in certain measurements , such as in the assessment of the distance between basion and articulare : as the head tilts , the occipital bone reveals more of the neck of one mandibular condyle and less of the other one . 
moreover , effective averaging of bilateral structures hinges on observer experience and requires more time than tracing cephalograms recorded in correct patient posture . conclusion we assessed the impact of subject positioning on the reliability of lateral cephalometric analysis . 
although our study pertains to measurements from the hard tissue part 1 3 radiol med ( 2017 ) 122 : 520529 of a tweed - merryfield analysis , its conclusions are likely to be valid also for other analyses . 
then , for a subset of 31 patients who had two cephalograms recorded on the same day , we performed the reliability analysis for both the initial and the retaken cephalograms . 
 although the second cephalogram was recorded with special care for patient positioning , being considered more satisfactory by the clinicians involved in the study , little improvement was observed in the statistical measures of intraand interobserver reliability . 
hence , moderate deviations from the ideal head positioning do not justify the x - ray exposure that would incur by taking a second cephalogram . acknowledgements part of this work was funded by the european social fund , human resources development operational programme 20072013 , project no . 
all procedures performed in this study were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
we introduced a new ct - score to evaluate hemodynamic changes , only employing ct - pulmonary angiography ( ctpa )  . materials and methods 145 patients affected by cteph underwent hemodynamic and ctpa evaluation . 
hemodynamic assessment considered the values of mean pulmonary artery pressure ( mpap ) and pulmonary vascular resistance ( pvr ) , obtained through right heart catheterization ( rhc )  . 
radiological evaluation included ctpa signs of pulmonary hypertension . results a highly significant statistical correlation was observed between the new ct - score and both mpap and pvr ( p < 0.000 ) in the whole sample and also in the subgroup who underwent pea . 
mpap also correlated with * maria barbara leone leone.barbara@hotmail.it 1 department of specialized , diagnostic and experimental medicine , university of bologna , santorsola - malpighi hospital , via g . 
advanced cteph leads to cardiac remodeling , involving right ventricular ( rv ) dilatation and hypertrophy , tricuspid regurgitation ( tr ) , and interventricular septal bowing ( isb ) , with consequent impact on cardiac function [ 1 ]  . pulmonary endarterectomy ( pea ) represents the therapy of choice for patients with surgically accessible disease . 
pea may be performed with a low mortality risk and results in clinical improvement and improved prognosis [ 24 ]  . radiologic assessment , most commonly with computed tomography ( ct ) , is central in the evaluation of pulmonary hypertension ( ph ) and can assist in elucidating the underlying cause [ 59 ]  . our purpose was to retrospectively evaluate the relationship among radiological , clinical and hemodynamic parameters in patients with cteph and in a subgroup of them who underwent pea . 
right and left ventricular short axes , measured on a reformatted four - chamber view , were defined as the largest distance between the interventricular septum and the free wall of ventricle . 
diameter of superior vena cava ( svc ) was measured at the level of arch of azygos vetricuspid regurgitation was split into four grades of gravity according to the degree of contrast medium reflux into the inferior vena cava and hepatic veins [ 15 ]  . among all parameters , special attention has been focused on pulmonary vascular signs , in particular on the evaluation of presence , location and degree of obstruction due to organized thromboemboli . since there does not exist a ct - scoring system to quantify the severity of cteph , we tried to create a new radiological ct - score that could reflect hemodynamic changes in patients with chronic pulmonary embolism , considering only radiological signs ; in particular we considered : unilateral or bilateral disease ( u / b ) , main pulmonary artery diameter ( mpa ) , mosaic perfusion pattern ( mp ) and tricuspid regurgitation ( tr )  . the new score was calculated as follows : score = u / b + mpa + mp + tr . scores assigned to each item are listed in table 2 . mp was considered as mild if it was < 10% , moderate if < 20 and > 30% and severe if > 30% , using a visual score . the total score can reach a maximum value of 15 . radiological evaluation was made independently and with unblinded clinical information by two radiologists of our department , respectively , with 40 and 5 years of radiological experience . 
mpap and pulmonary vascular resistance ( pvr ) were measured through this invasive technique . indications and surgical technique the selection criteria for patients undergoing pea and operative technique have been thoroughly described by jamieson and kapelanski [ 16 , 17 ]  . 
in particular , surgery is considered technically feasible if at imaging the organized thrombi are not located distal to the lobar arteries or to the origin of the segmental vessels . 
surgical resectability is further influenced by the severity of hemodynamic impair ment , the presence of concomitant diseases , in particular underlying lung disease , and the patients age [ 18 ]  . after median sternotomy and full heparinization , cardiopulmonary bypass ( cpb ) is instituted by cannulation of the ascending aorta and both inferior and superior venae cavae . 
while cooling , before 18 c nasopharyngeal temperature is reached , the aorta is clamped and cold crystalloid cardioplegia ( custodioldr koehler gmbh chemie - alsbach - haehlein ) is administered . 
in particular , mpap presented a significant correlation with the mp and mpa diameter both before and after pea ; pvr correlated with mp before and after pea , while presented a significant statistical correlation with mpa diameter only after pea . finally mpap percent difference correlated significantly with nyha clinical classification ( p 0.002 , each one evaluated in terms of improvement , stability or worsening )  . the new ctscore the statistical analysis of comparison between radiological and hemodynamic parameters is shown in table 5 . 
3 images of 35 - year - old ( a ) and 66 - year - old ( b ) men with bronchial artery hypertrophy in chronic thromboembolic pulmonary hypertension pea in the subgroup of 69 patients , we recognized a ctscore 6 as the median of all the scores and divided the patients into two groups as follows : 1 3 radiol med ( 2017 ) 122 : 495504 fig . 
nowadays , it has been recognized the role of ct scanning in providing more information on different components of the disease , predicting surgical success in the individual patient [ 2224 ]  . in particular , the highly significant correlation emerged for each radiological parameter , evaluated before and after pea ( p < 0.01 ) , allows us to reconfirm the fundamental role of ctpa in assessing the outcome of pea [ 3 , 25 ]  . as shown in table 6 , some radiological parameters did not show substantial modifications on ct executed after surgery ; in particular , it was observed that collateral circles , bah and leftward interventricular septum bowing did not change much after pea , which could be linked to a minor reversibility of these parameters after surgical intervention . 
reesink [ 1 ] analyzed the effect of pulmonary endarterectomy on the restoration of right ventricular remodeling in patients with chronic thromboembolic pulmonary hypertension by magnetic resonance imaging and observed that after pulmonary endarterectomy , pulmonary hemodynamic improved , as we demonstrated as well . 
they also assessed the normalization of leftward ventricular septal bowing ; this last result is different from ours , probably due to the absence of the ecg gating in our study and / or a better evaluation of it through mri [ 1 ]  . 1 3 502 radiol med ( 2017 ) 122 : 495504 also marc heinrich et al . 
they found out the mp as the best parameter for correlation with preoperative hemodynamic measurements , considering mp as a perfusion score demonstrating a strong correlation with mpap and pvr . these outcomes strengthen ours in which patients with a major reduction of mpap after pea also showed a consistent improvement of mosaic perfusion pattern on ct . 
this result can be probably explained as surgical disobstruction of pulmonary vessels causes both a reduction in mpap values and the reperfusion of lung areas which were poorly vascularised before pea , with the consequent disappearance of hypoperfused lung areas on chest ct after surgical intervention . 
 so the mp is the most sensible radiological parameter of the surgical success . in addition the significant relationship between mpap and mpa diameter , evaluated both as absolute value and as percent difference , confirms the relationship between mpa size and ph severity . 
over the last three decades , this relationship has been extensively investigated by several studies which demonstrated a moderate to strong correlation between mpa diameter and mpap , to the extent that a cutoff value of pa size has been proposed to help in the diagnosis or exclusion of ph [ 2632 ]  . 
some authors [ 22 , 33 ] also investigated this relationship in patients with cteph who underwent pea , coming to the same conclusions , in particular , among other parameters , mpa diameter measured on ct showed the strongest correlation with mpap and the most significant reversibility after surgery [ 33 ]  . another aim of our study was evaluating the relationship between mpap percent difference and variation in nyha class after pea ; this variation was also expressed dividing our sample into improved , unchanged and worsened patients . 
axial ctpa images of the main pulmonary artery before ( a ) and after ( b ) pulmonary endarterectomy a further step of our study consisted in evaluating the relationship between variation of radiological and hemodynamic parameters . 
from this analysis , it resulted that the absolute values of mpap and pvr were strongly correlated with the degree of mp evaluated before and after pea ( table 7 )  . 
these data confirm the good correspondence between clinical and hemodynamic improvement after pea and , as many authors already demonstrated [ 34 , 35 ] , further confirm nyha class as a useful parameter in the evaluation of clinical severity in patients with cteph . as concerns the scoring system of cteph , in past years , different scores ( modified miller and walsh scores and , more recently , qanadli and mastora scores ) have been proposed for the quantification of clot burden with ctpa in acute pulmonary embolis however , until now , there is not still a ct index designed to quantify the severity of chronic pe . 
in fact , it was observed both in whole sample and in the subgroup of patients who underwent pea that a greater reduction of ct - score corresponded to a consistent reduction of both hemodynamic parameters considered . 
we correlated each radiological parameter of the ct - score with mpap and pvr and we also tried to use central or peripheral occlusion of pulmonary arteries ; our results led to a stronger correlation of both hemodynamic parameters with the presence of unilateral or bilateral occlusion in preand post - surgical evaluations . from these results , it follows that the ct - score is directly proportional to the hemodynamic severity of cteph ; therefore , it could be used as an index of hemodynamic changes in all cteph patients for a quick assessment of hemodynamic impairment . 
the difference between the median value of the ct - score in the two groups of patients is probably due , in our opinion , to the amount and the different characteristics of the two samples . 
in fact , the median value of all ct - score in the group of 145 patients is evaluated only at the baseline ct , while the one of the other group ( 69 patients ) is evaluated on the preand post - surgical ct . 
these characteristics determine a lower median value of all the ct - score in the subgroup of 69 . in particular , we noticed , in the evaluation before and 6 corresponded to a after pea , that ct - score values mpap values closer to normal ; then a cutoff 6 could help in identifying hemodynamic values almost close to normal . finally , the ct - score proposed seems to be simple , fast to apply and useful in evaluating hemodynamic profile and consequently the severity of ph , using only a ct exam ; in this way the new index could be used to give cardiologists an estimate of hemodynamic changes in patients with cteph , either in those who carry out the intervention and in those who cannot , especially when a rhc is contraindicated or difficult to be performed . rhc is an invasive procedure and the use of an alternative non - invasive imaging modality to reduce the need of rhc at diagnosis or follow - up is an attractive proposition . the limitations of our study are due to the absence of ecg gating and to the fact that our proposed ct - score needs to be largely evaluated in terms of reproducibility . conclusion the results of the present study confirm the fundamental role of ctpa in the evaluation of pulmonary vascular and parenchymal alterations in patients with cteph , highlight the usefulness of ctpa in the radiological evaluation of this patients and in the assessing the outcome of the surgical procedure when executed . finally , our results open a new horizon in the use of ctpa , through the use of the ct - score introduced , even if more studies are needed to assess the reproducibility of the method . 
we can affirm that ct - score here proposed could represent a quick and easy index of hemodynamic changes , not only in surgical but also in not surgical cteph patients , either associated with right heart catheterization or as a substitute for this invasive technique , when it is contraindicated or not possible . compliance with ethical standards no funds were used for the present study . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
this article does not contain any studies with animals performed by any of the authors . informed consent informed consent was obtained from all individual participants included in the study . conflict of interest the authors declare that they have no conflict of interest . 1 3 504 radiol med ( 2017 ) 122 : 556 doi 10.1007 / s11547 - 017 - 0760 - 8 erratum erratum to : a prospective study on predicting local recurrence of giant cell tumour of bone by evaluating preoperative imaging features of the tumour around the knee joint yifeng he1 jun wang2 ji zhang1 fei yuan3 xiaoyi ding1 published online : 1 april 2017 italian society of medical radiology 2017 erratum to : radiol med doi 10.1007 / s1154701707457 in the original publication , the first and last names of the fourth author were interchanged . 
the mr arthrography images were analyzed by two radiologists , respectively with 5 and 15 years of experience in musculoskeletal radiology . results 36 cases of unclassifiable mr arthrography pat tern of the anteriorinferior glenoid labrum were evaluated : in 13 out 36 cases ( 36.1% ) , the glenoid labrum has been described as oedematous and swollen ; in 19 out 36 cases ( 52.8% ) , it has been described as smooth ( not hypoplastic ) ; in 4 out 36 cases ( 11.1% ) , it has been described as degenerated . conclusion the unclassifiable mr arthrography patterns of fibrocartilage glenoid lesions after episodes of recurrent antero - inferior dislocation are commons . 
the unclassifiable mr arthrography patterns require a careful consideration , * luca saba lukas_red@hotmail.it massimo de filippo luca.saba@chb.unicancer.fr in order to improve the diagnostic and therapeutic multidisciplinary approach . keywords unclassified pattern glenoid labrum lesion mr arthrography introduction the episodes of recurrent antero - inferior shoulder dislocation are one of the most common causes of the glenoid labrum tears , which are often associated with a bonybankart lesion [ 1 , 2 ]  . 
the glenoid labrum lesions in recurrent antero - inferior dislocation are a common problem , often occurring in young sportive people [ 1 , 2 ]  . the mr arthrography is the technique that today has the best diagnostic accuracy for the study of glenoid labrum lesions , with a sensitivity of 8691% and a specificity of 8698% [ 3 , 4 ]  . however , the glenoid labrum lesions could present often atypical patterns that are not defined in the current classifications [ 14 ]  . 
the diagnosis of the unclassifiable mr arthrography pattern of labrum injuries is important because it could be change the therapeutic choices . the aim of our study was to evaluate prospectively the incidence of unclassifiable mr arthrography patterns of glenoid anteriorinferior labrum lesions , in patients with at least two episodes of recurrent antero - inferior dislocation . 1 department of radiology and nuclear medicine , centre henri becquerel , rue damiens , 76000 rouen , france 2 department of radiology , parma hospital , via gramsci 14 , 43126 parma , italy the research was performed according to the world medical association declaration of helsinki . 
informed consent was obtained from research subjects . materials and methods 1 3 radiol med ( 2017 ) 122 : 540545 the mr shoulder arthrography images of 36 patients ( out of a server of 118 patients91 males and 27 females , range 1666 ) with at least two episodes of recurrent anteroinferior dislocation over 12 months , with or without bone involvement , were prospectively evaluated , during a period between november 2015 and mai 2016 . the exclusion criteria were : patients with surgical shoulder interventions , age > 70 and < 15 years old , patients with a known diagnosis of glenoid labral lesions . all patients were contacted by our service 6 months after the mr arthrography to evaluate the course of their treatment . we have evaluated : treatement ( conservative ou surgical ) timing of traitement after mr arthrography evaluation quantification of shoulder pain [ from 0 to 5 ] appearance of new dislocations . all images were acquired with mr magnetic field 1.5 tesla faced array coil ( philips , best , the netherlands ) , matrix 224 256 and foveal of 1618 c four standardized sequences were performed for each patient : axial t1 - weighted ( w ) spin echo ( se ) fat - suppressed imaging ; axial , coronal , and sagittal proton density ( pd ) weighted fat - suppressed imaging [ 5 ]  . a few minutes before the examination , the patient was placed on a bed in a supine position . 
3 examples of smooth glenoid fibrocartilage anteriorinferior labrum ( a , b , arrow ) statistical analysis parameters analyzed : results age and sex of the patient ; presence of degenerate , edematous and swollen or smooth glenoid labrum pattern . 
presence of hillsachs and hillsachs reverse lesions . statistical analysis was performed using spss statistics 19.0.0.1 fixpack ( ibm , united states ) using the pearson chi square test [ 7 ]  . about 36 cases of the sub - equatorial glenoid labrum showed a not classifiable pattern with the conventional injuries ; we found : in 13 out 36 cases ( 36.1% ) , the glenoid labrum has been described as oedematous and swollen ; 1 3 radiol med ( 2017 ) 122 : 540545 table 1 evaluation of unclassifiable mr arthrography patterns of glenoid labrum lesions and their outcome after conservative treatment discussion total type total benefit no benefit worse 36 ( 100 ) swollen 13 ( 36.1 ) 10 ( 76.9 ) 3 ( 23 ) smooth 19 ( 52.8 ) 13 ( 68.4 ) 2 ( 10.5 ) 4 ( 21 ) degenerated 4 ( 11 ) 1 ( 25 ) 3 ( 75 ) the unclassifiable mr arthrography patterns of glenoid labrum lesions are frequent . 
for example , the mr arthrography is accurate in enabling classification of acute and chronic anteroinferior injuries , although a correct interpretation of pertheslesions remains difficult [ 12 , 13 , 15 ]  . labroligamentous the unclassifiable mr arthrography pattern of the glenoid labrum is distinguished by a constitutionally hypoplastic glenoid labrum and by glom ( glenoid labrum ovoid mass ) lesion , which is evaluated as a small ovoid mass with a low signal intensity , often localized to the anteriorsuperior glenoid labrum , a result of a previous injury ( usually well recognizable by an expert radiologist ) [ 16 18 ]  . 
in our study , we did not evaluate a glom lesion . it is necessary to distinguish the unclassifiable mr arthrography glenoid from anatomicals variants , in particular : the hypoplastic anterior inferior glenoid labrum , which might simulate a traumatic outcome ; thepresence of a constitutionally dentate ( 15% ) , rounded or flattened ( 8% ) glenoid labrum , or the completeabsence of the glenoid labrum ( 6% ) [ 1921 ]  . 
in these cases , the medical history is diriment . our limitation was the lack of more time for the followup of conservative therapy and the lack of interdisciplinary collaboration with physiatry and orthopedics reference regional centers . in conclusion , the unclassifiable mr arthrography glenoid patterns , after recurrent antero - inferior dislocation , are commons . 
a cluster of association relationships between imaging features was revealed . keywords giant cell tumour of bone medical imaging local recurrence prognostic factor cystic change introduction giant cell tumour of bone ( gctb ) is one of the most intensively examined tumours of the bone in east and southeast asia [ 13 ]  . 
intralesional curettage , with 1 3 radiol med ( 2017 ) 122 : 546555 or without adjuvant methods , is the preferable approach for eliminating the tumour [ 2 , 7 , 8 ]  . 
unfortunately , a tendency to local relapse contributes to a high rate of local recurrence after intralesional curettage ( 1365% ) , which poses a great challenge for clinical treatment [ 912 ]  . therefore , studies of prognostic factors that reduce local recurrence are necessary . 
some investigations have reported that the location [ 1 ] , age [ 10 , 13 ] , soft tissue extension [ 11 ] , campanacci classification [ 14 , 15 ] and pathologic fracture [ 16 ] are risk factors of local recurrence of gctb , but according to other equivalent studies , all these nonsurgical risk factors have been excluded [ 12 , 1720 ]  . 
researchers seldom draw a unanimous conclusion on the risk factors and nonsurgical factors for local recurrence seemed controversial and ambiguous . intralesional curettage [ 10 ] and the residual tumour [ 11 ] were considered responsible for recurrence . 
magnetic resonance ( mr ) imaging is especially valuable for diagnosing bone tumours because of its heightened sensitivity to soft tissue disease and multiplanar image acquisition [ 22 ]  . we , therefore , investigated recurrence - related preoperative imaging features of gctb after intralesional curettage through prospective enrolment of gctbs in the proximal tibia and distal femur . materials and methods patients this prospective study was approved by our institutional review board , and written informed consent was obtained from patients for the use of all clinical and imaging data in this study . 
the patient eligibility requirements were : ( 1 ) histopathologically confirmed gctb ; ( 2 ) gctb located in the distal femur and proximal tibia ; ( 3 ) underwent intralesional curettage with polymethylmethacrylate ( pmma ) packing , which is the preferred standard treatment for gctb by a sub - group of orthopaedics in our hospital ; ( 4 ) radiography , ct and mr scans obtained before intralesional curettage ; and ( 5 ) followed up for at least 2 years . 
 * preoperative imaging features of gctb , including expansibility , the soap bubble sign , osteosclerosis , cortical bone involvement , adjacent soft tissue invasion , cystic changes , and the fluidfluid level increased complexity of surgical treatment , 4 patients with pathological fracture were excluded . imaging procedures patients routinely underwent anteriorposterior and lateral plain radiographs . ct examination was performed with a 64 - slice multidetector spiral ct scanner ( lightspeed vct , general electric medical systems , milwaukee , wi , usa ) according to a routine protocol . 
 phenol was applied in the borders of the cavity with cottontipped applicators and then neutralized with alcohol in 31 cases ; the remaining 25 cases were treated without additional adjuvant . 
finally , the tumour cavity was carefully packed with polymethylmethacrylate ( pmma ) filling . followup all patients were re - examined by x - ray or mr annually , regardless of whether they were symptomatic . 
all p values were two - sided , and the values less than 0.05 were considered statistically significant . results patient characteristics fifty - six patients were eligible for this study ( twentyeight women and twenty - eight men ; average age 34 years ; range 1864 years ; median age 29 years )  . 
 followup and local recurrence forty - eight out of fifty - six ( 85.71% ) patients were successfully followed up , while the remaining eight patients were lost to follow - up . 
for the remaining three recurrent cases , the times of relapse were more than 2 years ( two cases in their fifth year and one patient in her eighth year )  . recurrence prognosis of local recurrence the absorption of the bone graft or / and extension of the radiolucent zone after bone cement filling were reliable indicators for a possible local recurrence [ 23 ]  . 
if any symptoms ( discomfort , abnormal pain and swelling ) occurred after surgery , the patient would be re - examined immediately . these , thirty - two out of 48 patients were found to have a cystic change ; of twenty ( 62.50% ) cases developed recurrence . 
c , d on computed tomography ( ct ) , the focal cortex of bone ( white arrow ) was abnormally the , f , g mr showed the tumour with homogeneous low signal intensity on t1 - weighted image and intermediate - to - high signal on t2 - weighted images 1 3 550 radiol med ( 2017 ) 122 : 546555 fig . 
d , e mr showed the tumour with heterogeneous lowto - high signal intensity on a t1 - weighted image and intermediate - tohigh signal intensity on t2 - weighted images . 
 other imaging features , including expansibility , the soap bubble sign , osteosclerosis , cortical bone involvement , and fluidfluid level , were not associated with recurrence ( p > 0.05 ) , ( table 2 )  . 
there was no 1 3 soap bubble sign , n ( % ) cortical bone invasion yes 1.659 , p > 0.05 osteosclerosis , n ( % ) adjacent soft tissue 5.001 , p < 0.05 * radiol med ( 2017 ) 122 : 546555 table 1 patient characteristics characteristics age , n ( % ) 28 years > 28 years sex , n ( % ) male female location , n ( % ) proximal tibia distal femur expansibility , n ( % ) yes yes yes yes yes yes yes cortical bone invasion , n ( % ) adjacent soft tissue invasion , n ( % ) cystic change , n ( % ) fluidfluid level , n ( % ) significant difference between the recurrent rates of patients with and without additional adjuvant ( p > 0.05 ) ; no significant difference was found in the recurrence rates between the patients enrolled in the earlier years and those enrolled in the later years ( p > 0.05 ) ( table 2 )  . retrospective data analysis : correlations between clinical features and imaging features a cluster of association relationships were revealed by correlation analysis ( table 4 )  . 
this is the first prospective study to be conducted on the prognosis of gctb based on an investigation of the role of imaging features in predicting local recurrence . unlike other invasive tumours , although gctb accompanied occasionally by pulmonary metastasis , it appeared to have a good prognosis after appropriate surgical resection . 
we aimed to standardize the investigation by excluding the impact of varying tumour site by enrolling subjects with gctb involving the knee . gctb with cystic changes showed a higher rate of local recurrence and a cystic change was revealed as an independent risk factor for local recurrence after curettage . 
according to some studies [ 2426 ] , necrosis has a close relationship with elevated levels of vegf , and elevated vegf levels can , in turn , damage vascular endothelial cells and can also , in combination with subsequent narrowing of vessels due to fibrosis , result in oedema and necrosis . 
on the other hand , many authors [ 29 , 30 ] have reported that overexpression of vegf in gctb plays a key role in osteoclast formation and resorptive activity . 
these pieces of evidence could explain how cystic change can be a prognostic factor for local recurrence of gctb . we speculate that gctb with elevated vegf levels might be more prone to cystic changes ; accordingly , those with low vegf expression are more likely to lack cystic changes on mr . 
mr imaging plays a key role in identifying tumour properties , such as cystic changes , that are associated with a poor prognosis . our previous study demonstrated [ 32 ] the role of soft tissue mass in the prognosis of gctb . 
we speculated that surgeons might select a window where there is poor bone cortex integrity or thinner bone cortex to perform the surgery , decreasing the role of adjacent soft tissue invasion in the prognosis . 
on the other hand , in the early stage before the soft tissue mass formed , adjacent soft tissue invasions were more amenable to curettage than soft tissue masses . however , the remaining imaging features failed to predict outcomes , even though they also indicate different tumour properties . 
expansibility and the soap bubble sign were associated with a longer duration ; osteosclerosis was speculated as a protective factor for tumour growth and local aggressiveness ; cortical bone invasion indicated aggressive biological behaviours and was a sign of bone invasion ; the fluidfluid level was a manifestation of intratumoural haemorrhage . 
on the other hand , expansive growth of gctb indicated a slow process of osteogenesis and osteolysis , resulting in compression and invasion of the adjacent bone trabecula with osteosclerosis , which manifested as the soap bubble sign and expansibility . 
these interesting results provided insights into and inspired new ideas about gctb . to learn a lesson from current studies and reduce the controversy , we coupled with some authors [ 8 , 21 , 35 , 36 ] and advocated for a standardized evaluation system that 1 3 radiol med ( 2017 ) 122 : 546555 provided a reliable approach to identify risk factors of local recurrence . 
it resulted from the following two aspects : on the one hand , the surgical procedures were constant in these consecutive patients , and , on the other hand , the impact of tumour sites was excluded by enrolling gctbs around the knee . however , although the application of phenol is controversial in reducing local relapse [ 10 ] , it might be considered as a confounding factor . 
the remaining 3 cases recurred after two years of follow - up ( 2 cases recurred in their fifth year and 1 case recurred in her eighth year )  . 
 although local relapse after two years was considered exceptional [ 9 , 11 ] , we could not exclude the possibility of recurrence in patients who were followed up without a longer period . 
moreover , we enrolled the patients with gctb to investigate the role of the seven imaging features , but no independent prognostic factors were revealed , except for cystic changes . 
finally , even though our single - centre study was standardized by enrolling patients with gctb around the knee , the number of gctb patients was comparatively small . in summary , this prospective study first investigated the role of preoperative imaging features of gctb for predicting local recurrence , and a cystic change was identified as an independent risk factor for local recurrence . 
these findings may be useful for predicting local recurrence of gctb , but a study with a larger population is necessary . compliance with ethical standards funding this study was funded by the science and technology commission of shanghai municipality ( project number : 134119a2402 )  . conflict of interest the authors declare that they have no conflict of interest . 1 3fi 554 radiol med ( 2017 ) 122 : 546555 ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . radiol med ( 2017 ) 122 : 676682 doi 10.1007 / s11547 - 017 - 0768 - 0 neuroradiology stereotactic ablative radiation therapy for brain metastases with volumetric modulated arc therapy and flattening filter free delivery : feasibility and early clinical results alba fiorentino1 niccol giajlevra 1 umberto tebano1 rosario mazzola1 francesco ricchetti1 sergio fersino1 gioacchino di paola2 dario aiello1 ruggero ruggieri1 filippo alongi1 received : 4 november 2016 / accepted : 12 april 2017 / published online : 26 april 2017 italian society of medical radiology 2017 abstract aim for selected patients with brain metastases ( bms ) , the role of stereotactic radiosurgery ( srs ) or fractionated stereotactic radiotherapy ( sfrt ) is well recognized . 
the recent introduction of flattening filter free ( fff ) delivery during linac - based srs or sfrt allows shorter beam - ontime , improving patients comfort and facility workflow . 
aim of the current study was to analyze srs / sfrt linac - based fff delivery for bms in terms of dosimetric and early clinical results . materials and methods patients with life expectancy > 3 months , number of bms < 5 , diameter < 3 cm , and controlled or synchronous primary tumor received srs / sfrt . 
 the prescribed total dose and fractionation , based on bms size and proximity to organs at risk , ranged from 15 gy in 1 fraction to 30 gy in 5 fractions . 
toxicity was assessed according to ctcae v4.0. results from april 2014 to february 2016 , 45 patients ( 89 bms ) were treated with srs / sfrt linac - based fff delivery . 
with a median * niccol giaj - levra niccolo.giajlevra@sacrocuore.it 1 radiation oncology , sacro cuore don calabria cancer care center , via don sempreboni 5 , negrar , 37034 verona , italy 2 statistic science faculty , university of palermo , palermo , italy follow - up time of 12 months ( range 127 months ) , the median overall survival was 14 months and the 6 - month overall survival was 77% . 
acute and late toxicities were acceptable without severe events ( no adverse events g2 were recorded )  . conclusions these preliminary results highlighted the feasibility and safety of linac - based srs / sfrt with fff mode for bms patients . 
a longer follow - up is necessary to confirm the efficacy of this treatment modality in bm patients . keywords brain metastases radiotherapy stereotactic radiotherapy stereotactic fractionated radiotherapy introduction brain metastases ( bms ) are the most common intracranial tumors in adults ; in fact , about 2040% of patients affected by cancer will develop bms during oncological history [ 1 ]  . 
 moreover , in the last decades , the probability to develop bms increased up to five times due to the improving the efficacy of anti - cancer therapies [ 13 ]  . most of bms patients are defined as oligometastatic ( i.e. , patients with a limited number of metastases ) , and in this setting , the role of stereotactic radiosurgery ( srs ) or fractionation stereotactic radiotherapy ( sfrt ) is well recognized [ 4 ]  . 
in particular , srs / sfrt approaches can be recommended in the treatment of 14 bms and in patients with a life expectancy of more than 36 months [ 3 , 5 ]  . 
 recently , srs is preferred over whole - brain radiotherapy ( wbrt ) in order to minimize the probability of developing neurocognitive dysfunctions [ 6 , 7 ] , even though innovative hippocampal avoidance techniques were recently 1 3 radiol med ( 2017 ) 122 : 676682 developed [ 8 ]  . 
moreover , analyzing clinical outcomes , wbrt did not show an improvement in overall survival ( os ) when compared to srs [ 5 , 9 ]  . historically , the definition of intracranial srs was introduced by leksell as a single high dose fraction of radiation , stereotactically directed to an intracranial region of interest [ 10 ]  . 
in fact , beam / time ratio is usually limited to few minutes in single lesion setting , even though several parameters , such as prescription dose and target shape , could affect treatment delivery time [ 15 , 16 ]  . 
in order to further reduce beam - on - time ( bot ) , the removal of linac flattening filter ( ff ) allowed to produce a higher dose rate delivery with a shorter bot . 
nevertheless , the ff - free ( fff ) technique has several dosimetric advantages and hypothetical radiobiological effect , including a steep dose gradients , lower out - of - field dose , leaf transmission , lower dose outside the field edge , and cell killing [ 1720 ]  . 
the aim of the present study was to analyze bms patients treated by srs / sfrt with fff technique in terms of dosimetric and preliminary clinical outcomes . materials and methods patients all cases have been discussed in the multidisciplinary team , which included a radiation oncologist , a neurosurgeon , a medical oncologist , and a neuroradiologist . srs or sfrt was performed according to the following criteria : ( a ) critical anatomic position , ( b ) the absence of acute neurological symptoms , ( c ) life expectancy > 3 months , ( d ) number of brain metastases < 5 , ( e ) diameter < 30 mm , and ( f ) controlled primary tumor or metachronous diagnosis . informed consent was obtained from all individual participants included in the study . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . target definition and treatment computed tomography ( ct ) with contrast enhancement was requested in all patients to define the extracranial disease status , while magnetic resonance imaging ( mri ) with contrast enhancement was performed to evaluate the anatomical presentation and number of brain metastases . 
a co - registration of volumetric ct and mri - t1 sequences , typically a 3 - dimensional spoiled gradient series with 1 - mm slice thickness , was used to define target and organs at risk ( oars )  . 
planning target volume ( ptv ) was obtained adding an isotropic margin of 2 mm in all directions . oars were brain ( normal brain minus ptv ) , eyes , lens , optic chiasm , optic nerves , brainstem , and spinal cord . dose prescription ( ranged between 15 and 30 gy ) and fractionation ( ranged between 1 and 5 fractions ) were based on different clinical and radiological parameters including bm size , the presence of subacute or acute neurological symptoms , proximity to oars , or critical anatomical position . 
all patients were treated with the volumetric modulated arc technique rapidarc ( varian medical system , palo alto , usa ) on true beam equipped with a 6d couch and a micro multi - leaf collimator . 
exactrac ( brainlab , feldkirchen germany ) and cone beam ct imaging were performed daily for patient setup and positioning verification . in all patients , a prophylactic corticosteroid therapy ( dexamethasone 8 mg per day ) was prescribed and progressively reduced after radiotherapy according to clinical conditions and internal institutional protocol . evaluation of tumor response and radiological toxicity evaluation clinical evaluation and mri were requested after 4560 days from the end of the radiation treatment , then every 3 months for the first 2 years , and finally every 1 3 678 radiol med ( 2017 ) 122 : 676682 6 months or as appropriate after 3 years . 
more specifically , the diagnosis of radionecrosis was defined by means of the following radiological features : white matter high signal edema and mass effect early loss of volume later at t2 / flair , white or grey matter single or multiple nodular or curvilinear soap - bubble enhancement at t1 with contrast enhancement , mr spectroscopy : typically low choline , creatine , and n - acetylaspartate at spectroscopy [ 26 ]  . statistical analysis in order to summarize the most relevant features of the clinical variables , descriptive statistics were performed . 
all patients characteristics are shown in table 1 . in srs and sfrt patients , median dose prescriptions were 25 gy ( range 1525 gy ) and 24 gy ( range 2130 gy ) , respectively , while median number of fractions delivered in sfrt patients was 3 ( range 35 )  . 
in the second case , a corticosteroid therapy was prescribed for 50 days with a resolution to radionecrotic process . bms are the most common intracranial tumors in adults and generally , central nervous system metastatic involvement is characterized by a poor prognosis ( 36 months ) [ 1 ]  . 
historically , wbrt with or without surgical resection or srs have been considered the standard treatment for solitary or oligometastatic bms patients , while wbrt alone was performed in multiple bms setting [ 2729 ]  . currently , srs / sfrt alone is proposed to patients with 14 bms ( with diameter inferior to 2.53 cm ) and a life expectancy of more than 3 months [ 5 , 30 ]  . in a prospective study , yamamoto and colleagues reported about the use of srs in 1194 patients with one to ten bms ; authors suggested that srs alone in patients with five to ten bms is non - inferior to that in patients with two to four bms [ 31 ]  . 
nevertheless , these results caused several criticisms concerning the heterogeneity of population of study analyzed . a recent report from the working group on stereotactic radiotherapy of the german society of radiation oncology ( degro ) provides recommendations for the use of srs in bms , suggesting to choose the dose prescription according to the dimension and number of the lesions and the proximity to oars [ 5 ]  . 
analyzing dose prescription , a single dose of 20 gy is considered acceptable , while higher doses ( 2225 gy ) should be limited in small lesions ( < 1 cm )  . 
 in patients with bms diameter greater than 2530 mm , a dose reduction to 18 gy is recommended , despite rtog 90 - 05 considered adequate a dose prescription of 15 gy [ 23 ]  . 
in fact , different dose prescription schedules have been published as 27 gy in 3 fractions [ 32 ] , 25 gy or 30 gy in 5 fractions [ 33 ] , demonstrating good results in terms of clinical outcomes and tolerability . 
thus , from these multiple and various experiences , a standardized dose seems to be not well defined and a heterogeneous prescription still continues to be commonly used in a case of srs and / or sfrt . in the here reported experience , we decided to treat with srs / sfrt up to five bms [ 31 ] and the choice of the dose and / or fractionation was made based on degro guidelines and international clinical experiences [ 5 , 32 , 33 ]  . to our knowledge , this is the second analysis published combining : clinical outcomes , toxicity , and dosimetric results for bms treated with srs / sfrt linac - based and fff mode . 
analyzed the combination of the fff delivery for radiosurgery of brain metastases in comparison to delivery with ff intensity - modulated radiotherapy ( imrt ) and volumetric modulated radiotherapy ( vmat )  . 
authors evaluated the dosimetric superiority of fffvolumetric modulated arc therapy when compared to ffvolumetric modulated arc therapy in the setting of single brain metastasis in 68 patients with a dose prescription of 20 gy in single fraction . 
authors reported an advantage in the use of fff in terms of bot ( 5.45 min ) , treatment delivery time , and mean dose rate ( p < 0.001 ) when compared to ff . 
additionally , normal brain sparing was higher in fff approach with reduction in brain irradiation of about 2% reductions in low - dose regions ( about 510 gy )  . 
in our experience , we obtained a lower bot ( mean srs 140 s ) and a lower brain irradiation ( dmean brain : 0.71 gy ) in patients receiving a srs treatment . in terms of clinical outcomes , the first analysis was reported by rieber et al . 
in regards to the dosimetric parameters , the authors showed a significant reduction of the average bot with fff modality respect to the standard ff , reporting a median value of bot was 128 s ( range 45278 s )  . 
the acute and late toxicities were mild : nausea and headaches in acute setting , and for late side effects , only one case of asymptomatic intracerebral hemorrhage [ 19 ]  . 
in terms of dosimetric and clinical outcomes , the present results were similar to those reported by rieber et al . , despite in the present population , the median number of lesions for patients was two respect to one in the riebers analysis . an important limitation of the present study is related to the absence of basal neurocognitive state evaluation of the patients before and after radiotherapy . 
however , detailed basal neurocognitive state definition will be object of prospective future evaluation . moreover , in the here discussed data , correlation between dosimetric parameters and toxicity / outcomes was not analyzed because the number of events ( radionecrosis / bleeding ) was very limited ( only two cases ) and follow - up was too short for any further consideration . conclusion despite the limitations of the study ( retrospective evaluation , relatively short follow - up time , and limited sample size ) , and considering the few clinical data published , the present results add clinical information about safety and efficacy of the srs / sfrt in bms oligometastatic patients . 
further studies and a longer follow - up are mandatory to confirm our preliminary results in the treatment of bms . compliance with ethical standards this research did not receive any specific grant from funding agencies in the public , commercial , or not - for - profit sectors . 1 3 radiol med ( 2017 ) 122 : 676682 conflict of interest the authors declare that they have no conflict of interest . 
despite its rarity , incidence of pbls has increased over the last four decades and continues to increase for younger women and for some subtypes , and for this reason it is increasingly important to achieve a preoperative pathological diagnosis using core needle biopsy ( cnb ) or fine - needle aspiration cytology ( fna )  . 
diffuse large b cell lymphoma ( dlbcl ) was the most frequent pbls and on cnbs specimens was possible do the fluorescent in situ hybridization analysis to evaluate the presence of chromosomal translocation . 
brambilla 3 , 50134 florence , italy 2 hematology department , azienda ospedaliero - universitaria careggi florence , university of florence , florence , italy 3 emergency radiology , department , azienda ospedalierouniversitaria careggi florence , florence , italy 4 radiation oncology unit , oncology department , azienda ospedaliero - universitaria careggi florence , university of florence , florence , italy 5 division of pathological anatomy , university of florence , florence , italy pbls , especially for dlbcl , in which a correct and fast classification could change the therapeutic approach and the prognosis . keywords breast cancer core needle biopsy primary lymphoma diagnosis introduction primary breast lymphoma ( pbl ) represents a rare clinical entity about 0.040.53% of all breast primaries and about 2.2% of all extranodal lymphomas , and may mimic carcinoma clinically [ 1 ]  . 
lymphomatous involvement of the breast may occur as primary extra lymph node involvement of the breast or as secondary infiltration by systemic disease at the time of either initial diagnosis or disease recurrence . pbl is defined as the presence of both mammary tis sue and lymphoid infiltrate in close association with no evidence of widespread lymphoma or preceding extramammary lymphoma . 
despite its rarity , incidence of pbls has increased over the last four decades and continues to increase for younger women and for some subtypes , and for this reason it is increasingly important to achieve a preoperative pathological diagnosis using core needle biopsy ( cnb ) or fine - needle aspiration cytology ( fna ) [ 2 ]  . about 53% of all pbls are diffused large b cell lymphoma ( dlbcl ) , the usual presentation includes a painless palpable mass similar to that of breast carcinoma , and also mammographic and ecographic distinction is subtle . 
a radiologist of the diagnostic senology unit ( g.b ) consulted the database of the local institution to categorize the histological diagnosis on cnb and collected data of all pbl . patients and methods results we retrospectively collected data from our records on 10 , 500 cnbs performed between january 2000 and december 2016 at the diagnostic senology unit of our centre . 
b mlo mammography of february 2016 , 18 months after chemotherapy with r - chop ( rrituximab , ccyclophosphamide , h doxorubicin , ovincristine , pprednisolone ) , showed the disappearance of the opacity without other alterations , the patient is still in follow up without any recurrence 1 3 radiol med ( 2017 ) 122 : 651655 fig . 
the other five patients underwent directly to staging and therapy , and are still in follow up without any recurrence ( mean time of follow up 38 months , range 984 )  . 
only one patient with marginal zone lymphoma had a contralateral breast relapse two years after the initial diagnoses and was treated with radiotherapy . in three patients with cnbs diagnoses of dlbcl on cnbs specimens was made the fluorescent in situ hybridization ( fish ) analysis to evaluate the presence of chromosomal translocation ( 8 ; 14 ) that can change the therapy and the prognosis of these patients . 
our three patients 1 3 radiol med ( 2017 ) 122 : 651655 654 table 2 clinical and radiological features of seven patients with pbl at the diagnoses patients clinical mammography ( birads ) ultrasound ( birads ) side ultrasound dimension palpable mass irregular opacity ( birads 4 ) multicentric nodules ( birads 4 ) right 40 mm ( greater ) hypervascularized nodule ( birads 5 ) left 15 mm palpable mass multicentric irregular opacity ( birads 4 ) multicentric nodules ( birads 4 ) right 30 mm ( greater ) palpable mass irregular opacity ( birads 4 ) hypervascularized nodule ( birads 5 ) left 26 mm palpable mass irregular opacity ( birads 4 ) hypervascularized nodule ( birads 5 ) right 30 mm multifocal irregular opacity ( birads 4 ) multifocal nodules ( birads 4 ) right 15 mm ( greater ) hypervascularized nodule ( birads 5 ) right 12 mm mm millimeters with dlbcl were negative for translocation and underwent the normal therapy with r - chop ( rrituximab , ccyclophosphamide , hdoxorubicin , ovincristine , pprednisolone )  . the clinical and radiological features of pbls at the diagnoses were summarized in table 2 . 
the four patients that were symptomatic , mean age 66 years ( range 4581 ) underwent mammography ( mr ) according to the american college of radiology ( acr ) appropriateness criteria for the evaluation of palpable breast masses [ 5 ] and then ultrasound ( us ) examinations because the mammography findings were suspicious ( birads 4 ) [ 6 ]  . the three patients who were asymptomatic came from private clinics with suspicious findings at mr and / or us . 
 two of them ( patient 2 and 7 ) did recently mr elsewhere so we did only us , one patient ( patient 6 ) did both mr and all the patients did an ultrasound ( us ) examination before cnb and someone did also mammography ( mrx ) in our center if not elsewhere performed . 
the mean dimensions of the lesion measured on us were 24 mm ( range 1240 )  . discussion the importance of preoperative histological diagnosis in the assessment of breast lesions in women is widely established and also the advantage of cnb than fna as initial needle biopsy method , but in the literature there are few data about the initial histological diagnosis of pbls . 
 [ 7 ] the main reason is probably related to the low incidence of plbs accounts for only 0.040.53% of all breast primaries and about 2.2% of all extranodal lymphomas . despite its rarity , incidence of pbls has increased over the last four decades and continues to increase for younger women and for some subtypes and for this reason it is increasingly important to achieve a preoperative pathological diagnosis using cnb or fna . to our knowledge , the literature is lacking on published experiences on cnb as an initial diagnostic procedure for pbls . 
all seven samples contained sufficient tissue for diagnosis , there were no procedure - related complications , and for all patients it was possible to achieve a correct world health organization ( who ) sub - classification . 
levine and colleagues [ 8 ] analyzed a series of eight fnas of pbls with flow cytometry , achieving only three correct who sub - classifications of pbls ; banik et al . 
 [ 9 ] analyzed two cases of pbls and concluded that the diagnoses based only on histomorphology carries significant risk of misdiagnoses , the ultimate categorization required flow cytometric immuno - phenotyping better did on cell block , and we demonstrated that the use of cnbs with large specimens facilitated this procedure . in accordance with our series , the study of domchek et al . 
 [ 10 ] showed a rate of 53% dlbcl , confirming that dlbcl is the most frequent pbls and in almost all cases patients with pbl showed palpable breast masses . 
the most important advantage we demonstrated in our study was that on cnbs samples the pathologist could directly do the fish analysis to search chromosomal translocation , especially for dlbcl in which the pathologist could change the therapeutic approach and the prognosis . 
in fact , as it is recommended in international literature , for example in the meta - analysis of zhou and colleagues [ 3 ] , it is mandatory to do screening to search chromosomal translocation for dlbcl because it had a prognostic value and guaranteed a tailored therapy for the patients in particular enabled the early identification of dlbcl patients with poor 1 3 radiol med ( 2017 ) 122 : 651655 2 . 
hukkinen k et al ( 2008 ) unsuccessful preoperative biopsies , fine needle aspiration cytology or core needle biopsy , lead to increased costs in the diagnostic workup in breast cancer . 
banik t et al ( 2016 ) two cases of primary non - hodgkins lymphoma of female breast : role of fine - needle aspiration cytology and cell - block immunohistochemistry . 
kiaei a et al ( 2016 ) detection of t ( 8 ; 14 ) c - myc / igh gene rearrangement by long - distance polymerase chain reaction in patients with diffuse large b - cell lymphoma . 
in complete sections , when both retrograde and anterograde stenting singularly failed , we performed a rendez - vous technique with a combined radiological trans - nephrostomic access and urological cystoscopic approach to realign and catheterize the ureteral stumps . 
in patients with bricker urinary diversion , peri - anastomotic leaks were treated by positioning a multihole pig - tail catheter with the inner end in the renal pelvis and the distal portion outgoing from the cutaneous stoma . 
laparoscopy can increase the risk of ureteral injury above all during the surgeons training [ 3 ]  . ureteral injury can be also the obvious consequence of urological procedures , such us ureteroscopy or percutaneous nephrolithotomy , or a complication of vascular intervention , such us aortic - iliac or aortic - femoral bypass [ 3 , 4 ]  . the risk of iatrogenic lesion is principally due to the close anatomic rapport between ureter , visceral organs and vascular structures [ 5 ]  . 
the distal third of the ureter is the most affected tract ( 51% ) , followed by the proximal third ( 30% ) and from the middle third ( 19% )  . the main mechanisms of damage are : accidental ligation , kinking due to attraction by a suture , crushing by clamping , overheat with electrosurgical systems for hemostasis , devascularisation and partial or complete sections [ 6 ]  . 
berkmen affirmed that the most frequent injuries are complete sections [ 7 ]  . severity of ureteral injury is classified into five grades from hematoma to laceration ( section < 50% or > 50% ) to complete transection with devascularization < 2 or > 2 cm [ 8 ]  . 1 3 radiol med ( 2017 ) 122 : 696704 post - operative diagnosis of ureteral lesions is very challenging because clinical manifestations are often non - specific . therefore , imaging plays a key role in the detection of the site and the entity of the injury [ 9 ]  . computed tomography urography is currently the gold standard for diagnosis , allowing the demonstration of the urinary leak and the precise evaluation of the ureteral stumps ( length , position and distance ) that is essential in the treatment planning [ 10 , 11 ]  . in delayed diagnosis ( 6676% of cases ) the ureteral repair strategy is still controversial , including surgical , urological or interventional radiology chances . 
the choice of treatment depends on a number of factors : time between onset and diagnosis , aetiology , site and length of lesions , general condition of the patient , experience and availability of a highly specialized medical staff [ 12 ]  . no specific guidelines discipline the management of these patients . the aim of our work was to evaluate feasibility and effectiveness of interventional radiology procedures in the resolution of iatrogenic urinary leaks in different types of lesions : incomplete / complete sections or peri - anastomotic leakage after surgical urinary diversions . materials and methods our study enrolled 19 patients ( 11 females and 8 males ; mean age 58 years ) with suspected iatrogenic ureteral lesions . 12 / 19 patients came from the surgical oncology department : six patients had undergone a hartmann resection of the sigma . 
in another one the loco - regional extension of the tumor also had necessitated an ileal resection and resection of the distal right ureter confectioning a transureteroureterostomy . three patients had undergone a resection for rectal cancer : in one case surgeons preferred a trans - perineal approach ; one patient received neo - adjuvant radiotherapy ; a pelvic exenteratio with brickers urinary diversion was performed in the last case . one patient had undergone a left hemicolectomy . one patient had undergone a right hemicolectomy . one patient was treated with a pelvic exenteratio with a brickers urinary diversion for a vaginal recurrence of cervical cancer . 4 / 19 patients came from the department of urology : two patients had undergone radical cystectomy with uretero - ileum - cutaneostomia according bricker method . two patients had undergone partial cystectomy . 3 / 18 patients were treated for gynaecological benign disease : one hysterectomy for uterine fibromatosis . one annessiectomia for an ovarian cyst . one caesarean section in a patient who had undergone transvaginal uterine cerclage during pregnancy . intraoperative diagnosis failed in all cases . diagnosis in the recent post - operative time ( from 4 days to 1 month after surgery ) was suggested by the appearance of urine from the abdominal drainage , fever or bowel obstruction . diagnosis was more delayed ( 23 months after surgery ) in patients with bricker - type urinary diversion ; they developed leakage near the ureteral anastomosis with the formation of collections and fistulas in the adjacent subcutaneous - cutaneous tissues . curiously , the patient with history of cesarean section came to our attention after 1 year from surgery for the appearance of a urinary vaginal fistula . in all cases diagnosis was obtained by ct urography that clearly showed extra - ureteral spreading of the contrast medium and urinoma . in six cases the involved ureter was the right , in other six cases was the left one and in the remaining seven cases there was a leak at the surgical anastomosis . 
the patient treated by a trans - perineal surgical approach had a section of the ultra - low ureter with iodine urine spreading through the wound to the buttock line . in six patients ct images showed no opacification of the distal ureteral stump as typical sign of a complete transection . only in three cases there was a modest degree of hydronephrosis . in accordance with our urologists , a ureteral stenting through a retrograde cystoscopic approach was always tried when considered feasible . 
we cross the stenosis using a microguide ( v18 control wire , boston scientific ) and then we per formed a lumen dilatation with a balloon catheter ( diameter 5 mm ; length 40 mm )  . 
finally , we positioned a double - j stent with the caudal extremity in the bladder ( c ) and the cranial extremity in the renal pelvis near the nephrostomic tube ( d ) the guide - catheter descending from leaving the nephrostomic access in the proximal ureteral stump , the patient was placed in the supine position and sedated with anesthesiologic assistance . then , the urologist cannulated the ureteric orifice using a flexible ureteroscope and he passed a hydrophilic guide and a manipulator catheter through the working channel of the instrument , running through the distal ureteral stump and trying to bring the system as close as possible to that previously positioned in the other side . a retrieval goose neck system ( amplatz gooseneck snare kit ) was advanced from the retrograde access within abdomen . then the guide from the nephrostomic approach was inserted in the loop of the goose neck catheter , catched and pulled out exteriorly through the bladder and urethra . after the change of the hydrophilic guide with the amplatz guidewire , maintaining under tension the guide pulling at both its exterior ends , the ureteral stumps were aligned and a double - j stent was finally placed . 1 3 699 radiol med ( 2017 ) 122 : 696704 fig . 
second step was rendez - vous : we catheterized the distal ureteral stump though a cystoscopic approach and tried to bring the system as close as possible to that previously positioned through nephrostomy ( c1 )  . 
then , using an amplatz guide we positioned in retrograde way a multihole pig - tail catheter ( 8 f , length 40 cm ) with the inner end in the renal pelvis . finally , the nephrostomy catheter was repositioned and kept open . 1 3 700 radiol med ( 2017 ) 122 : 696704 treated by hartman procefig . 
after positioning bilateral nephrostomies , in the second step we recovered from the right nephrostomic access the two stent fragments using a goose neck catheter ( b , c )  . 
finally , two new double - j ureteral stents , passing through the anastomotic site ( asterisks ) , were simultaneously positioned from the two nephrostomic accesses ( d , e ) when ureter and ileal conduit were widely misaligned , we used a rendez - vous technique , with both a nephrostomic and a cutaneous stoma access , to restore the continuity of the urinary tract . results after ureteral stenting , we provided a 1 - month - followup by pyelography through the nephrostomy . 
restoration of the continuity of the urinary tract was achieved when the pyelography showed the resolution of the urinary leak . disappearance of the leakage and absence of clinical symptoms ( fever , hematuria , etc . ) allowed us to close the nephrostomy and to remove the outer bag . 
the absence of leakage and the good functioning of the ureteral stent allowed us to remove the nephrostomy . in our experience interventional radiology reached the resolution of the ureteral injury in all patients ( success rate of 100% )  . 
even in cases of complete section of the ureter , the result was obtained thanks to the rendez - vous technique . no patient required surgical re - intervention . there were no procedural complications , except for a case of hematuria due to a small pseudoaneurysm of the renal artery caused by the nephrostomy catheter , treated with a super - selective embolization with some micro - spirals . 1 3 radiol med ( 2017 ) 122 : 696704 fig . 
finally , a pig - tail catheter was placed along the ureter and the pyelographic control showed the resolution of the leak ( d ) the ureteral stents are replaced every 46 months . 
in female patients the replacement is carried out in the angiography suite through urethra by the fluoroscopic guidance . in three patients the stent was completely removed . in one patient , candidate to stent removal , the relief of a ureteral stenosis in correspondence of the damage site recommended to perform an ureteroplastic procedure and to prolong the maintenance of the stent . table 1 summarizes our data . discussion among iatrogenic ureteral injuries partial and complete sections are the most difficult therapeutic challenge . as already theorized by lang [ 13 ] , the rationale of a conservative repair depends on the urothelium ability to reconstitute the injured tract . 
 [ 5 ] proposed an algorithm for conservative treatment of ureteral fistulas in which the first line step was the retrograde ureteral stent placement ; then , if leakage persists , an ipsilateral nephrostomy tube was inserted to obtain an external urinary diversion . 
 [ 16 ] treated conservatively 17 patients with post - gynaecological surgery ureteral injuries , reporting a failure in 6 cases that required a surgical repair ; however , failure might be probably due to an incomplete treatment since only one patient had received the positioning of both the nephrostomy that the stent , while the remaining only a partial urinary diversion with nephrostomy or stents . 1 3 702 table 1 our case series radiol med ( 2017 ) 122 : 696704 case sex age type of surgery damaged nephrostomy stent follow - up ( years ) site ureter stent left ureter left 1x8f removed after 5months removed after 4months right ureter right 1x8f urinary bilateral 2x8f in progress anastomosis urinary bilateral 2x8f in progress urinary bilateral 2x8f died for oncologic anastomosis desease right ureter right 1x8f removed after 8months rendez - vous rendez - vous right ureter right 1x8f in progress left ureter left 1x8f in progress anastomosis urinary urinary left ureter left 1x8f in progress rendez - vous anastomosis bilateral 2x8f in progress anastomosis bilateral 2x8f in progress left ureter left 1x8f in progress rendez - vous rendez - vous right ureter right 1x8f removed after 5months urinary bilateral 2x8f died for oncologic anastomosis desease right ureter right 1x8f in progress urinary anastomosis bilateral 2x8f lost right ureter right 1x8f in progress left ureter left 1x8f in progress left ureter left 1x8f in progress rendez - vous 1 3 radiol med ( 2017 ) 122 : 696704 wein et al . 
reported that the percentage of success of a conservative treatment with nephrostomy and ureteral stent for at least 6 weeks in the restoration of the continuity of the ureter is about 73% . 
when it is not feasible or fails , we take the anterograde route , preliminarily placing a nephrostomy catheter and then positioning the ureteral stent . abdominal fluid collections tend to angular and displace the ureteral stumps , making other procedures more difficult . in the six patients with complete lesions of the ureter , where both the retrograde and the anterograde approach failed individually , we adopted the rendez - vous technique that has been already reported for the treatment of complex ureteral stenosis [ 17 ] and of urinary leaks . in a study that enrolled 40 patients de baere et al . 
 [ 18 ] needed a double nephrostomy and cystoscopic approach in 8 cases : in 3 cases they opacified with the contrast medium the distal stump by the cystoscopy and complete the anterograde stenting ; in the remaining they performed a rendezvous , that was unsuccessful in 2 patients . in 2005 , macri et al . 
 [ 21 ] reported a series of eight patients with post - surgical total section of ureter treated by endoscopic rendez - vous with flexible ureteroscope cranial and rigide ureteroscope caudal ; they obtained in all patients the repair of the urinary tract , estimating that the length of the damaged segment was between 1.5 and 3 c in our view , the main disadvantage of the endoscopic rendez - vous is the need of a wide nephrostomy access ( 18 f ) to allow passage of the instrument ; instead this condition is not required when interventional radiology makes the anterograde part of the rendez - vous . regarding the choice of the size and the number of stents there are no precise rules . 
their management is controversial for the lack of guidelines . radiologists may play a key - role not only in the diagnostic phase demonstrating urinary leaks and urinomas , but also in treatment . 
 since sicilian regional administration today is still disregarding implementation of the provisions contained in the proposal of the ministry of health entitled guidelines on organizational and health care methods of breast centers network in november 2015 the sicilian regional group of the italian society of radiology ( sirm ) decided to carry out a survey to see the position of the sicilian healthcare system and define the gap to bridge over . 
sicilian breast imaging radiologists were asked to fill in a questionnaire concerning the type of job relationship ( public or private sector ) , qualification ( manager , department manager , freelancer ) and years of experience on breast imaging . 
 with regard to technological requirements , were answered the questions about the number , type , age and completeness * placido romeo promeo@sirm.org 1 department of biomedical sciences and morphologic and functional imaging , policlinico universitario g.martino , university of messina , messina , italy 2 breast cancer screening center , asp catania , catania , italy 3 breast cancer screening center , asp messina , messina , italy 4 asl toscana centro , ospedale ss cosma e damiano pescia , pescia , italy 5 uoc radiodiagnostica , aou policlinico vittorio emanuelecatania , catania , italy 6 department of diagnostic imaging , s . 
these data have to be shared with policy makers to enhance quality improvement in sicilian breast center network . keywords breast unit organizational models for breast care guidelines for breast imaging introduction the european society of breast cancer specialists has created quality indicators for breast units to establish the minimum standards of care for patients and to ensure specialist multimodality care with the conscious aim of improving outcomes and decreasing breast cancer mortality [ 1 ]  . 
on december 18th 2014 , the italian state region conference ( csr ) adopted , with protocol 185 , the proposal of the ministry of health entitled guidelines on organizational and health care methods of breast centers network [ 2 ] which provided , within the area of clinical breast imaging , a substantial reshaping of practices for the breast care both for clinic and screening . 
breast centers have been defined as those structures which host the screening activi ties , the instrumental clinical diagnostics and therapy for 1 3 640 radiol med ( 2017 ) 122 : 639650 patients with breast disease , eliminating the dichotomy in the current organization of structures dedicated to screening and clinical breast center [ 3 ]  . 
the models proposed are both vertical ( hub - spoke ) and horizontal ( hubhub ) : the breast care center is the hub to which are functionally referenced screening and clinical / diagnostic centers , representing the spokes . 
the breast center is made up of a cohesive group of dedicated breast cancer specialists , working together as a multidisciplinary team , with access to all the facilities required to deliver high quality care throughout the breast cancer pathway . 
 this group does not necessarily have to be a geographically single entity , as the breast center can be made up by services and specialists from more than one hospital , within the same geographical area , allowing for close multidisciplinary working and guarantee of easy access to all the necessary services [ 2 , 4 ]  . guidelines indicated 6 months from the time of the agreement as deadline for the adaptation to the arrangement . 
moreover , breast radiologists qualification , the working conditions and the technological supplies in the different italian regions is not accurately known . since sicilian regional administration today is still disregarding implementation in november 2015 , the sicilian regional group of the italian society of radiology ( sirm ) decided to carry out a survey to see the position of the healthcare on the sicilian territory and define the gap to bridge over the provisions contained in the cartel by stimulating the regional healthcare department to pay more attention . the aim of this study is to take a snapshot of breast units ( bu ) in our region , sicily , from the radiological point of view and to carry out an analysis on the real situation of breast radiologists working in our area and the technological supplies available at the moment . 
 to better understand the characteristics of the sample , the questions requested information concerning the type of relationship ( public or private sector ) , qualifying ( manager , department manager , freelancer ) and years of experience . 
 six answers described an under 40 - year - old team ; 32 teams were aged between 40 and 58 years mean ; 13 described an over 58 years old mean aged group . 
most of our sample ( 35% ) works in private practice with affiliation to the health care system and around ( 81% ) of sicilian breast imaging radiologists has over 10 years of experience . figure 5a shows the number of radiologists routinely performing a breast clinical examination to the patients undergoing to an imaging workout . 
namely , the 16% of the radiologists read more than 3000 mammograms per year ; 65% does not have the competence requirement set for breast mri , and approximately half of the sample appears proficient 1 3 radiol med ( 2017 ) 122 : 639650 fig . 
almost 60% of the sicilian radiologists work in centers where no multidisciplinary meetings , i.e. , tumor boards , have been activated and only 37% is involved in scientific research . 
us is performed in 65% of cases with a multidisciplinary us system ; less than 40% of the devices have evolved diagnostic software ( contrast media , elastosonography )  . 
90% of technologies have an average age of less than 10 years . resonance concerning magnetic ( mri ) machines , over 40% of radiologists do not perform mri because there is no magnet available and patients who need breast mri are usually sent to nearby hospitals provided with mri and breast coils . 
3 a diagram showing the prevalence of radiologists among the sicilian cities ; b diagram showing the operative unit type ; c the figure represents in percentage the number of breast cancer centers dedicated to the screening setting ; d the catchment area in sicily fig . 
4 a diagram shows in percentage the type of affiliation for radiologists ; b diagram shows in percentage the type of functional position for radiologists ; c diagram shows in percentage the qualification for radiologists , in terms of years of experience 1 3 radiol med ( 2017 ) 122 : 639650 fig . 
5 a diagram shows the percentage of radiologists performing routinely clinical breast examination ; b diagram shows the percentage of mammography performed per year ; c diagram shows the percentage of ultrasound performed per year ; d diagram shows the percentage of mri of the breast performed per year fig . 
6 a diagram shows the percentage of fine needle biopsies of the breast performed per year ; b diagram shows the percentage of core needle biopsies of the breast performed per year ; c diagram shows the percentage of vacuum assisted biopsies of the breast performed per year ; d diagram shows type of needles used from the different units 1 3 646 radiol med ( 2017 ) 122 : 639650 fig . 
7 a diagram shows the percentage of medical dedicated staff ; b diagram shows the percentage of dedicated nurses ; c diagram shows the percentage of dedicated auxiliary staff ; d diagram shows the percentage of dedicated secretaries fig . 
8 a diagram shows preferred types of medical education ; b diagram shows the percentage of centers performing multidisciplinary meetings ; c percentage of centers performing programs of continuous staff training ; d diagram shows the percentage of radiologists involved in the research field 1 3 radiol med ( 2017 ) 122 : 639650 fig . 
9 a diagram shows number of available mammographic systems ; b diagram shows the availability of different types of mammographic systems ; c diagram shows the availability of additional accessories for the mammographic systems ; d diagram shows mammographic systems mean age fig . 
10 a diagram shows the number of available ultrasound systems ; b diagram shows the availability of different types of ultrasound system ; c diagram shows the availability of additional software and accessories for ultrasound devices ; d diagram shows ultrasound systems mean age 1 3 648 radiol med ( 2017 ) 122 : 639650 fig . 
11 a diagram shows the number of available mri machines ; b diagram shows the availability of different tools for breast mri ; c diagram shows mri systems mean age systems do not have advanced diagnostic software ( diffusion , spectroscopy , mri guided biopsy )  . 
about 86% of the surveyed has an average age less than 10 years . about 12% of investigated work in structures without radiology information system ( ris ) orpicture archiving and communication system ( pacs )  . 
therefore , practices with greater numbers of physician members of the sirm or gisma are more likely to be represented in the survey results than practices with fewer sirm or gisma members . 
furthermore , various reasons caused the different number of breast radiologists enrolled for the survey , determining different distribution in the data acquired between eastern and western sicily . our results , anyway , showed a map as real as possible , of sicilian clinical breast cancer centers which greatly varies with excellence and critical areas . 
according to the european society of breast imaging ( eusobi ) [ 6 , 7 ] , mammography is the most important imaging procedure for breast cancer detection and diagnosis , especially in the general female population from 50 to 70 years of age . 
12 a diagram shows centers with the availability of ris - pacs systems ; b diagram shows types of the screens available ; c diagram shows centers in which computer - aided detection ( cad ) systems were available ; d diagram shows workstations mean age mammography devices are not available and these should be considered cases of malpractice . 
radiological equipment has a definite life cycle span , resulting in breakdown and decrease or loss of image quality over the time , which renders equipment useless after 10 years . 
according to the guidelines , technologic devices seem to be up - to - date as highlighted by the survey : 78% of dedicated machines for mammography , ultrasound and mri have an average age of less than 10 years . these results can become an important source of knowledge to be used in a confrontation with the islands health institutions and allowed the working group to formulate proposals for action . of particular interest for the study , it appears the reluctance of young people to approach the sector , likely as a result of more than one of the following reasons : training problems to graduate school , fear of litigation coroner , high upgrade costs as the breast courses are the most expensive , difficult to be dedicated exclusively to breast imaging because of the need to cover the guard duty of general radiology , reduced attractiveness to reach a professional arrangement and an adequate financial remuneration . therefore , there is a need to invest in competence and professionalism , especially with regard to specialist and interventional methods , taking through advantage of the capacity of the centers with the highest diagnostic level for the second - level training . training , also an additional investment is to be made by the departments of management and the private towards even greater specialization of the staff that should , ultimately , be totally dedicated to breast imaging [ 1113 ]  . 
with regard to the technology park , however , it appears that there is not a lack of updated machines , namely some problems are detectable in the acquisition of software and accessories for advanced diagnostic . 
from this analysis , it is clear that the bu in sicily has great room for improvement and to increase the quality of the syste 1 3 650 radiol med ( 2017 ) 122 : 639650 first , a step forward the competence and profession should be moved through a closer network among university hospital , with special interest to screening programs and breast interventional procedures . in conclusion , it is indispensable for an intervention of regional healthcare department for coordination in the definition of the network model to guarantee high level quality and access equity all over the island . 
this seems not to be still regarded as a priority by the sicilian regional institutions . compliance with ethical standards funding no funding was provided for the study . conflict of interest author maria adele marino declares that she has no conflict of interest . 
author placido romeo declares that he is member of the ethic and forensic committee of the italian society of radiology ( sirm )  . ethical approval this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2017 ) 122 : 690695 doi 10.1007 / s11547 - 017 - 0771 - 5 ultrasonography can ultrasonographyguided aspiration and steroid injection treat reflux venous blood flow around our shortterm experience symptomatic bakers cysts ? emin cakmakci1 irfan celebi2 safiye tokgoz ozal3 ayse secil eksioglu1 ozlem kolcak3 mucahit dogru4 received : 11 november 2015 / accepted : 19 april 2017 / published online : 28 april 2017 italian society of medical radiology 2017 abstract objective the aim of the current study was to investigate the efficacy of ultrasonography - guided aspiration treatment with concomitant steroid injection on relieving reflux blood flow in veins located next to symptomatic bakers cyst . methods all patients were examined by ultrasonography at administration and 1 month follow - up after intervention . 
even though the majority of these cysts are asymptomatic , the most common clinical manifestations are stiffness , swelling , mass , pain , bulging and tightness in the back of the knee upon walking or vague posterior knee pain [ 1 , 2 ]  . 
the pathophysiological mechanism underlying bc formation is the onset of a synovial effusion causing an increase in the intra - articular pressure that subsequently causes synovial fluid leakage into the bursae [ 3 ]  . 
imaging modalities may be required for diagnosis and ultrasonography ( us ) is very useful to assess the popliteal fossa . in symptomatic patients , intra - articular corticosteroid injection or direct puncture of bc for aspiration and corticosteroid administration are commonly performed [ 5 , 6 ]  . 
 us - guided cyst aspiration and concomitant corticosteroid injection into the cyst is a good option in the management of patients with bc [ 7 ]  . venous incompetence can be observed by doppler us when provocation maneuvers ( manual proximal compression of the calf or toe movements ) are performed [ 7 ]  . 
if the valves close correctly it is followed at most by a short flow ( 0.51 s ) of blood towards the feet , if at all , until the venous valves prevent any further 1 3 radiol med ( 2017 ) 122 : 690695 fig . 
the transmission of ultrasound waves through fluid gives the appearance of enhancement deep to the lesion ( 8951337 / 1009 / 1171 / 050213 ) board informed consent was taken from the patients . and written a total of 42 patients with symptomatic simple bcs who had been admitted to the radiology department of a tertiary care center between october 2012 and january 2013 for cyst aspiration and concomitant corticosteroid injection , were prospectively included in the study . 
reasons for exclusion were aneurysm of popliteal artery or vein , accompanying vascular adventitial lesions and other popliteal or meniscal cysts , and cases with associated chronic venous disease changes . 
the main symptoms / signs that led to the necessity of treatment were contraction and edema at the popliteal region and pain during knee flexion . us examination and intervention all patients were examined by us and color doppler us by the same radiologist ( e.c. ) at administration and 1 month follow - up after intervention . 
the volume ( v ) of bcs was calculated and recorded with the ( v 0.52 ) ford1 mula , based on the assumption that the structures were antero - posterior , ellipsoids ( d1 longitudinal diameter )  . transverse , d2 after the initial examination , bc was punctured by an 18 g seldinger needle under us guidance under local d2 d3 fig . 
 note that as in the illustration a bakers cyst may deviate to the left which can result in compression on the adjacent venous structures that leads to venous insufficiency or thrombus formation ( copyright of the figure belongs to the senior author ) flow in this direction [ 8 ]  . 
however , they also argue that neurovascular bundle compression syndrome of bakers cysts is rare and there is a selection bias in reporting more severe rare cases . the aim of this prospective study was to investigate the efficacy of us - guided aspiration treatment with concomitant steroid injection on relieving reflux blood flow in popliteal vein ( pv ) and vena saphena parva ( vsp ) during the management of bcs . patients and methods study design the procedures followed were in accordance with the standards of the helsinki declaration of 1975 / 83 . 
puncture and aspiration of the cyst as well as injection of 1 ml dexamethasone were performed by the same radiologist ( ec ) who also performed the sonographic / doppler evaluations . 
reflux was defined as the reverse flow that occurs over 1 s after the proximal compression of the related vessel and was evaluated in four grades : absent ( < 1 s ) , mild ( 12 s ) , moderate ( 24 s ) , severe ( > 4 s )  . all patients were called in for a control us at 1 week and 1 , 3 and 6 months after treatment and were reevaluated by gray - scale and color doppler us in the same manner . 
the changes in cyst size at consecutive appointments and degree of reflux before and 1 month after treatment were compared . statistical analyses data were analyzed using the ibm statistical package for social sciences v21 ( spss inc . , chicago , il , usa )  . 
3 cysts size observed before the treatment and during the follow - up tear of the anterior cruciate ligament ( n and lateral meniscal tears ( n 2 )  . 2 ) , and medial cysts size observed before the treatment and during the follow - up is shown in table 1 and fig . 
 however , cysts size did not differ significantly after treatment ( table 2 )  . compression on popliteal vein and vena saphena parva were encountered in 18 ( 69.2% ) and 16 ( 61.5% ) cases , respectively . 
with respect to age and bmi , patients without any degree of reflux on vena saphena parva ( n 10 ) and patients with reflux ( mild , moderate , or severe ) on popliteal 1 3 radiol med ( 2017 ) 122 : 690695 table 2 the change in cyst size before and after treatment cyst size mean std . 
before the treatment , mild , moderate and mild severe degrees of reflux blood flow were detected in the popliteal vein in five ( 19.2% ) , nine ( 34.6% ) and four ( 15.3% ) patients , respectively . 
before the treatment , mild , moderate and severe degrees of reflux blood flow were detected in vena saphena parva in two ( 7.7% ) , six ( 23.1% ) and eight ( 30.8% ) patients , respectively . significant change was observed in the degree of reflux on popliteal vein and vena saphena parva before and after treatment ( p < 0.05 ) ( table 4 )  . 
similarly , no reflux on vena saphena parva was observed in 16 patients with varying degrees of reflux before treatment . bleeding was noted in six ( 23.1% ) cases before the intervention . 
during the intervention , communication was not observed in any of the patients between the bc and the knee joint on injection of material into the popliteal fossa cyst itself . 
after the treatment , only one patient ( 3.8% ) had a mild degree of reflux blood flow in the popliteal vein ; while no reflux blood flow was observed in the vena saphena parva . 
intracystic hemorrhage was observed in only one patient 6 months after the intervention . table 3 degree of reflux on popliteal vein and vena saphena parva before and after treatment discussion before treatment degree of reflux on popliteal vein degree of reflux on vena saphena parva after treatment degree of reflux on popliteal vein none mild moderate severe none mild moderate severe none mild moderate severe mild moderate severe n ( percent ) 8 ( 30.8% ) 5 ( 19.2% ) 9 ( 34.6% ) 4 ( 15.4% ) 10 ( 38.5% ) 8 ( 30.8% ) 6 ( 23.1% ) 2 ( 7.7% ) 24 ( 92.3% ) 2 ( 7.7% ) in the present study , patients with symptomatic bc were treated with aspirationsteroid injection and were followed . 
in compliance with literature , the success of the aspiration and steroid injection procedure was demonstrated by the decrease in bc volumes . bakers cyst may display a variety of symptoms . 
this may lead to venous insufficiency and consistent symptoms such as numbness , nocturnal cramps , congestion , edema , dermatitis and pigmentation can be observed [ 8 ]  . 
the small saphenous vein arises from the union of the dorsal vein of the little toe with the dorsal venous arch and ascends through the middle of the calf to the lower portion of the popliteal space where it empties into the popliteal ve compression resulting intraluminal distension of the popliteal vein may result in reflux flow in the small saphenous ve us and venous doppler examination are useful for the diagnosis of bc and its relationship with surrounding veins [ 9 , 10 ]  . in spite of different surgical techniques and aggressive surgical intervention , recurrent bc is a well known condition [ 11 ]  . 
 ultrasonographic guidance facilitates the performance of this procedure and avoids the risk of penetration into popliteal artery or vein the present study , an overall reduction of the cysts size was observed in all patients . 
reduction of the cyst size is more evident during the 1st week , which was observed by a slight enlargement during the 1st and the 3rd months controls . rather than blind puncture and injections in the treatment of bc , us - guided interventions seem to be safer and more effective . 
another weakness of us is the difficulty to establish a connection to the joint space , which is essential for distinguishing between a bc and other entities in the differential diagnosis [ 4 , 5 ]  . limitations of our study include the relatively small number of our series . 
one can also state that it is not clear if the reduction of the reflux blood flow in popliteal vein and saphena parva vein is due to bc treatment or cyst volume reduction that relieves decompression of the adjacent venous systefinally , single physician performed all procedures and assessed imaging that also could introduce bias to study results . 
due to these restrictions , associations should be interpreted with caution . in conclusion , us - guided puncture , aspiration and steroid injection seems to yield promising outcomes in terms of relieving the venous reflux flow around simple or complex bcs . 
its delineation is complex and in practice different head position can vary hippocampus morphology on axial images ; so atlas in a single standard position can result ineffective to describe different hippocampal morphologies in different head set - up . 
the purpose of our study was to develop a guide based on magnetic resonance imaging for hippocampus delineation in three different head set - ups . materials and methods three patients were selected to elaborate our guide . 
patients were submitted to a planning computed tomography of the brain district in different head positions : 1 patient in neutral , 2 patient in over - extended and 3 patient in head hypo - extended position ; axial images of 2 - mm thickness were obtained . 
discrepancies were observed in cranial and caudal limit in case of head over / hypo - extension , as well as in hippocampal morphology near the encephalic trunk where * marianna trignani marianna.trignani@unich.it 1 department of radiotherapy , ss annunziata hospital , g . 
dannunzio university , chieti , italy hippocampus takes an oblong shape in over - extended setup , and short and stocky in hypo - extension . conclusion our guide can represent a useful tool for hippocampal delineation in clinical practice and for different anatomic variations due to different head positions . 
certainly , it should be validated in practice . keywords hippocampus radiotherapy delineation atlas introduction in recent years , radiotherapy technologies improvement , both in planning and delivery phase , has increased the need of more accurate delineation of target volume and organs at risk ( oars )  . in brain tumors radiotherapy , the delineation of intracranial oars represents a crucial point because of the potential neurological deficits deriving from the damage of cer ebral tissues . recent experimental and clinical evidences shed light on neurocognitive impairment deriving from irradiation of the hippocampal dentate gyrus [ 1 ]  . thus , delineation of hippocampal region during treatment planning is crucial , especially if high ablative doses using stereotactic radiotherapy are given , as well as in pediatric irradiation , or if treatment of recurrent tumors is required . several factors can affect the accuracy of oars delineation such as inter - observer variability , anatomic complexity of structures , different protocol and atlas of reference available . 
proposed a simplified anatomy atlas on computed tomography ( ct ) and mri of the brain oars including hippocampus [ 24 ]  . the applicability of atlas contouring for the hippocampal region is often limited by ageand disease - specific variability in hippocampal size and location [ 5 ] ; furthermore , headneck position contributes to create further variability . 
in radiotherapy planning and treatment , patient is set up on the treatment table in supine position with the aid of an immobilization device , generally an immobilizing head shoulders thermoplastic mask . 
therefore , it is not possible in all cases to apply the standard reference atlas . we propose a practical guide for hippocampus delineation with three different set / ups based on three different head positions ( neutral , over - extended and hypo - extended )  . 
 this work should aid radiation oncologists to perform accurate segmentations even in case of different anatomic configurations of the hippocampus . materials and methods to elaborate our guide , we selected three patients ( 1 patient with neutral head , 2 patient with over - extended head , 3 patient with hypo - extended head ) from a sample treated with fractionated stereotactic brain radiotherapy , at our radiotherapy institute , from january 2015 to may 2016 . in selected patients , the acquired planning ct of the brain district was representative for neutral , over - extended and hypo - extended position . diagnostic pre - treatment mri was available for all patients . 
the mri was performed on philips achieva 3 - tesla scanner , with an 8 - channel head coil , using 3d fast field echo ( ffe ) t1 - weighted sequences with fat saturation ( 512 gadolinium ( gadovist 0.2 mmol / kg ) administration . 512 - square matrix ) before and after intravenous the planning ct scan ( somatom emotion duo , siemens healthcare , forchheim , germany ) of the brain district was acquired from the vertex to the lower border of c2 , using 2 - mm slice thickness . 
ct and mr images were co - registered and then fused based on gray scale and anatomical landmarks using raystation anatomy ( from ta raysearch )  . for each of these three patients , hippocampus was delineated by a radiation oncologist according to the contouring atlas for radiation therapy oncology group 0933 protocol rtog on t1 - weighted mri co - registered with planning ct [ 2 , 3 ]  . 
all contours were revised jointly by radiation oncologists and two neuro - radiologists with an expertise in neuroimaging > 5 years ; to validate the contouring conformity , a qualitative assessment was performed , disputes were resolved by consensus . contouring was performed on axial images , in clinical condition . 
the hippocampal structure 1 3 radiol med ( 2017 ) 122 : 683689 has a length of 4.5 cm ; the body is on average 1 cm wide , and the head is 1.52 cm wide [ 9 ]  . mesially , the hippocampus is delimitated by the para - hippocampal gyrus . it is arched around the mesencephalon and it can be divided into three segments : the head , or anterior segment , which is transversely oriented and located posteriorly to the amigdala ; the body , or middle segment , which is sagittally oriented and the tail , or posterior segment that follows the course of the lateral ventricle and narrows , disappearing below the splenium [ 10 ]  . mri appearance and contouring of hippocampus t1 - weighted sequences allow a good visualization of hippocampus , since it is formed of gray matter ; its signal is hypo - intense ( gray ) compared to the hyper - intensity of the white matter ( whitish ) ; and it is hyper - intense compared to the low signal intensity of the cerebrospinal fluid into the ventricular system ( black )  . this study , hippocampus was delineated on t1 - weighted without contrast mri sequences fused with planning ct . 
comparative sagittal view of the hippocampus in neutral , overextended and hypo - extended head position in df , respectively 1 3 radiol med ( 2017 ) 122 : 683689 fig . 
orange hippocampus ; a body of the hippocampus is the first visualized portion on the first caudal slice where its signal becomes visible ; b , c head and body of the hippocampus visible in their grater ap extension ; d , e hippocampal head and tail are both visible ; f the last cranial visible portion of the hippocampus head and tail . 
to fully benefit of these new technologies in radiation oncology practice , consistent delineation of targets and oars has become increasingly important [ 11 ]  . in particular , in cranial radiotherapy the contouring accuracy is a key factor in sparing organs at risk especially in hippocampus sparing , because of both anatomical complexity of this structure and clinical implications related to hippocampal injury . avoiding the hippocampus during brain irradiation , while allowing uniform dose delivery to the target volume , poses important challenges for several reasons : central location , unique anatomic shape , inter - observer variability , large variations between protocols of delineation [ 12 , 13 ]  . standard contouring atlases represent a good reference tool for accurate delineation of oars in radiotherapy planning with the aim to reduce inter - observer variability , especially for anatomic structures of some complexity . standardization and uniformity are the modern approach to radiotherapy purpose , but in some situations , in clinical practice , the reality can be different from the standard . 
the imaging sections generated by the scanner in the planning ct can be different from the idealized brain sections and this is made worse by a generally undervalued biologic phenomenon : individual anatomic variation . 
 recent studies investigated the effect of head inclined position in the hippocampal sparing brain radiotherapy showing optimized dose distribution to the planning target volume and a lower dose to the hippocampus [ 1517 ]  . selection of appropriate mri sequences is crucial for correct hippocampus delineation . 
on mri t1 sequences with contrast medium , hippocampus is not well identified because of the reduction in intrinsic contrast between white and gray matter ; therefore , in our study mri contrast t1 sequences were not employed for hippocampal delineation . 
in this work , it is suggested to use mri slices orientation along the axis of the hippocampus to obtain a better visualization [ 4 ]  . these tools are valid and accurate but in some practical situation they are not always exhaustive . 
indeed , real situations deviate from the standard particularly when head setup is over - extended or hypo - extended . the present work resulted from the observation that in over - extended head set - up , on axial sequences , the most caudal extent of the hippocampal head does not correspond to the first caudal slice where temporal horn of the lateral ventricle is visible . 
the splenium of the corpus callosum , in an over - extended set - up , can not represent a useful landmark for the superior extent of hippocampus . our study attempted to answer to critical issues characterizing hippocampus , especially in relation to different anatomic head positions , and to offer a valid tool when a deformable registration algorithm between planning ct and mri is not available . therefore , we produced an institutional mri imagebased guide for daily clinical practice to improve interobserver homogeneity and accurately establish dosevolume relationships . to date , we have not yet quantified the impact of this tool in clinical practice and this is a limitation of the present study . 
however , an evaluation of inter - observer variability with and without the guide is expected . our work aims to highlight hippocampal sparing radiotherapy that is not just contouring but also planning and delivery of low neurocognitive impact treatment . conclusion our guide seems to provide a useful tool for accurate hippocampal delineation in clinical practice and for different anatomic variation due to different head position . 
they selected for the full - text analysis only the abstracts in which the accuracy of intra - articular position of the needle was confirmed on imaging ( humans ) or by a surgical dissection ( cadavers )  . 
however , five articles in which blind injec tion the ghj was used ( 159 shoulders ) reported accuracy as high as 100% . conclusion a comprehensive review of the literature confirms that guided injections of the ghj have overall accu racy higher compared to blind injection . 
a large prospective randomized study is needed to gauge this hypothesis and compare the cost - effectiveness of these two techniques for the most common anatomical approaches . keywords shoulder joint injections intra - articular / methods arthrography fluoroscopy ultrasonography magnetic resonance imaging reproducibility of results interventional humans cadavers introduction gleno - humeral joint ( ghj ) disorders are a frequent cause of morbidity , with a prevalence of 6.934% in the general population and up to 21% in subjects older than 70 years [ 1 ]  . 
shoulder pain can negatively impact the patients global health : the persistence of shoulder pain for three months or longer is significantly correlated with depres sion , anxiety , and sleep disturbance [ 2 ]  . 
corticosteroids ( cs ) , non - steroidal anti - inflammatory drugs ( nsaid ) and hyaluronic acid ( ha ) are used in most clinical settings , even there is a lack of evidence of a real benefit of the intra - articular injection of drugs to treat shoulder pain [ 5 ]  . 
 there is some evidence that imaging guidance for the intraarticular placement of the needle can improve the outcome of patients with a painful ghj treated by cs compared to blind injections [ 6 , 7 ] or injections performed using bony landmarks [ 8 ]  . 
 actually , a recent review article suggested that intra - articular injection of cs may have an effect comparable to systemic administration [ 10 ]  . beyond intra - articular drug injection , an accurate intraarticular injection into the ghj is mandatory to perform computed tomography ( ct ) arthrography or magnetic resonance arthrography ( mra ) for diagnostic purposes . 
mr arthrography is particularly beneficial for the clinical management of elite athletes suffering from a painful shoulder [ 12 ]  . some reviews suggested that imaging - guided injection is more accurate than blind injection for ghj . 
indeed , the use of imaging guidance implies a cost of the imaging examination to guide the injection and an accurate department organization ( e.g. , fluoroscopy or ultrasound unit availability scheduling )  . to date , no large systematic review has been performed to establish whether blind injection can challenge the accuracy of injection performed using imaging guidance or bony landmarks . the aim of the present systematic review was to establish whether a blind injection of the gleno - humeral joint ( ghj ) may be a reliable alternative to the injection performed using imaging guidance in the different anatomic approaches described in literature . materials and methods search strategy for identification of studies the local ethical committee was not solicited for the present study . 
1 the pico strategy ( population / patient , intervention / indicator , comparator / control , outcome ) for systematic review and meta - analysis was used as basic approach to build the strategy to build the search strategies for the different on - line medical database 1 3 658 radiol med ( 2017 ) 122 : 656675 the needle placement was to be controlled by a clinically validated medical imaging method or dissection ; the article had to report only original data or original data could be obtained from the authors ; the article had to be written in one of the languages spoken by one of the authors or mastered by a medical doctor available for the translation in our institution : english , french , german , greek , hungarian , italian , turkish , dutch , arabic or spanish . previous systematic reviews or meta - analyses on the same topic , if any , were collected to be considered in the discussion section in the article , but their data were not considered in analysis . the abstracts of the retrieved articles were selected by two independent reviewers ( mp , fle )  . 
once again the opinion of a third author could be solicited in case of lack of consensus ( ps )  . data extraction a set of relevant data to extract for each article were established by a consensus between all the authors . 
the two tables were fused into a final table by the two authors ( table 1 ) and thoroughly checked independently by two other authors ( mg , ps ) ( table 1 )  . for each selected study , the type of enrollment of patients ( prospective or retrospective ) and the main patient enrollment criteria in terms of shoulder pathology were noted ( e.g. , rotator cuff tear suspicion )  . the number of patients and injections performed was also noted , along with approach and the type of imaging technique used , if any . the level of evidence of each study was noted as reported in the selected article . 
if the level of evidence was not indicated in the study ( mp , fle ) , a third author ( mg ) extracting the data assigned by a consensus a level of evidence to each study on the basis of the published guidelines for radiological articles [ 15 ]  . the reported accuracy of the approach ( es ) investigated by each article was also noted . 
secondary data related to the intra - articular placement of the needle into the ghj including extravasation rate , procedure - related pain , use of anesthetic drugs , the occurrence of vagal reaction and other relevant events were also collected in a word worksheet ( table 1 ) when reported in the articles . data analysis and statistical analysis feasibility due to the heterogeneity of the population in terms of population ( shoulder pathology , volunteers and cadavers ) , population selection criteria ( prospective and retrospective studies , level of evidence , type of pathology ) and imaging devices ( the tremendous evolution over the time of the quality of the imaging devices must be considered ) , we considered that the data were not homogeneous enough to perform a meta - analysis [ 16 ]  . 
in addition , as described by higgins et al , the cohrans q and the i2 would have been not acceptable for a metanalisis due to the heterogeneity of number of cases and because of the large of selected studies [ 16 ]  . hence , in this review we only provide a narrative description of a comprehensive of published articles on this topical matter . 
in all the articles , the accuracy of needle placement by different anatomical approaches with and without imaging guidance was confirmed by a clinically validated medical imaging method ( humans ) or by anatomical dissection ( cadavers )  . critical appraisal of the methodological quality using the assessment of multiple systematic review ( amstar ) tool to objectively assess the methodological quality of the present systematic review , we used the assessment of multiple systematic review ( amstar ) tool [ 17 ]  . 
this published tool was developed by panel of experts to help users to critically and qualitatively assess the value of systematic reviews . the amstar tool includes 11 components [ 17 ]  . 
all studies selected for the final analysis were independently scored by 2 reviewers with a final consensus in case of disagreement ( ps , om ) ( see appendix 4 )  . results search strategy results our search strategy resulted was performed for article published by december 2016 . 
2 flow chart of the study selection process radiol med ( 2017 ) 122 : 656675 one - thousand and twenty - four articles were excluded because inclusion criteria were not matched by the abstract content . 
3. the selected studies included a total of 2309 patients ( 2690 shoulders ) , including 195 cadavers ( 299 shoulders )  . other studies enrolled patients referred by clinicians for various internal pathologies of the ghj . patients with adhesive capsulitis were reported as present in the population in 6 out of 38 ( 16% ) studies [ 26 , 3338 ]  . in two studies of the included studies , all patients included were clinically suspected of suffering from adhesive capsulitis [ 26 , 33 ]  . in two studies , patients were injected under general anesthesia before undergoing arthroscopy [ 39 , 40 ]  . the type of study and level of evidence were established for each article on the basis of evidence - based medicine principles applied to radiology [ 14 ]  . the population features for each study and other relevant type of anatomical of approach information for each particular article are detailed in table 1 . features of included studies patients features and types of articles the number of patients and the number of examined shoulders included in the selected articles was from 3 [ 24 , 25 ] to 256 [ 26 ]  . one study [ 23 ] was performed on normal subjects , while 7 studies were performed on cadavers [ 24 , 2732 ]  . 
 ( 1 ) the site of anterior approach is represented as a blue square ; ( 2 ) the site of the antero - superior approach through the rotator intervals is represented as a yellow star ; ( 3 ) the site of the superior approach is represented as a black point next to the acromio - clavicular joint . 
the palpation is even easier when mobilizing the humerus to better distinguish the almost immobile scapula from the moving humeral head 1 3 666 needle placement guidance in 13 out of 38 studies ( 34% ) , the intra - articular placement of the needle was performed without imaging guidance [ 23 , 27 , 28 , 32 , 34 , 35 , 46 , 50 , 53 , 55 , 57 , 58 , 62 ] ; in these studies , the loss of resistance during the injection was used to assess to intra - articular position of the needle before the injection [ 23 , 26 , 28 , 32 , 33 , 35 , 39 , 41 , 46 , 50 , 53 , 55 , 57 , 58 , 62 ]  . injections performed using multiple bony landmarks to localize the injection point were performed in 4 of 38 studies ( 10% ) [ 26 , 33 , 39 , 41 ]  . in 38 ( 55% ) articles in which injections was performed under imaging guidance [ 22 , 24 , 25 , 27 , 3032 , 37 , 38 , 4245 , 48 , 49 , 51 , 52 , 54 , 56 , 5961 ] , 7 used only us guidance [ 22 , 32 , 37 , 38 , 43 , 49 , 52 , 54 ] , 4 used only mri guidance [ 24 , 45 , 47 , 59 ] , and 2 used only fluoroscopy guidance [ 51 , 56 ]  . 
in one study , injection guided by fluoroscopy was compared to blind injection [ 61 ]  . accuracy overall accuracy the overall accuracy of the intra - articular injection in ghj in the selected articles varied from 42% [ 34 ] to 100% [ 6 , 22 , 24 , 25 , 31 , 37 , 43 , 44 , 48 , 50 , 51 , 54 , 55 , 60 , 63 ]  . accuracy and shoulder features the accuracy of the intraarticular injection into the ghj was 90% in one study on normal subjects [ 23 ]  . the accuracy of intra - articular injections in ghj joint in studies on cadavers [ 24 , 28 , 3032 , 53 , 61 ] ranged from 74% [ 53 ] to 100% [ 24 , 31 ]  . the accuracy of intra - articular injection the ghj in the 2 studies performed in patients with adhesive capsulitis was 90 and 95% , respectively [ 26 , 33 ]  . in the study in which patients were injected under general anesthesia the reported accuracy was 91% [ 39 ]  . radiol med ( 2017 ) 122 : 656675 accuracy and anatomical approach in studies anterior approach , the injection accuracy varied from 42% [ 34 ] to 100% [ 25 , 41 , 43 ]  . in the 8 articles using the antero - superior approach through the rotator interval [ 24 , 39 , 42 , 48 , 49 , 5558 ] , the reported accuracy rate ranged from 89% [ 58 ] to 100% [ 24 ]  . 
 [ 38 ] , comparing the antero - superior approach with the posterior approach under ultrasound guidance . in the 8 studies using the posterior approach [ 22 , 30 , 37 , 5054 ] , the injection accuracy ranged from 72% [ 30 ] and 100% [ 22 , 36 , 37 , 51 ]  . the lowest accuracy rate ( 45.7% ) for the posterior approach was found in the study of tobola et al . 
 [ 35 ] comparing the posterior approach without imaging guidance to supraclavicular and supero - anterior approaches . in the two studies , published by the same group , using the superior approach [ 31 , 32 ] the injection accuracy varied from 94 to 100% . 
the lower accuracy for the anterior approach with ultrasound guidance ( 26.8% ) was reported by sethi [ 27 ] and coworkers who compared the anterior to the posterior approach under ultrasound guidance . in five articles in which the mri guidance was used [ 24 , 25 , 45 , 59 ] , the reported accuracy varied between 96.8% [ 59 ] and 100% [ 24 , 25 , 45 ]  . table 2 features of studies by anatomical approach anatomical approach highest accuracy lowest accuracy number of studies cumulative number of shoulders anterior antero - superior superior posterior 1 3 radiol med ( 2017 ) 122 : 656675 of note , 5 different studies including a total of 159 shoulders [ 25 , 41 , 43 , 47 , 55 ] reported a 100% accuracy of the injection indicating that blind injection may be as accurate as an injection under imaging guidance ( see table 3 )  . discussion secondary data related to the intraarticular needle placement procedure vagal reaction three of the selected articles reported the incidence of vagal collapse [ 37 , 52 , 60 ] with an incidence varying between 3.3% [ 52 ] and 11% [ 37 ]  . pain the procedural pain was evaluated in only 5 [ 35 , 37 , 38 , 42 , 59 ] of articles with a visual analog scale ( vas ) varied from 19 / 100 ( ogul ) [ 38 ] to 5.8 / 10 in the study of tobola and coll [ 35 ]  . use of local anesthesia local anesthesia was used in 22 out of 38 ( 58% ) of selected articles ( see table 1 )  . 
the high volume of lidocaine used was 5 ml of 2% solution [ 50 ]  . extravasation the highest extravasation rate ( 48% ) was reported by ogul [ 38 ] using the antero - superior approach under ultrasound guidance . 
the injection time varied from 100 s [ 30 ] ( injection performed by posterior approach under ultrasounds guidance ) to 17 s [ 6 ]  . critical appraisal of the methodological evaluation of the systematic review using the assessment of multiple systematic review ( amstar ) tool the analysis of the methodological quality using the assessment of multiple systematic review ( amstar ) tool is shown in the appendix 4 . 
these questions had a negative answer because of the heterogeneity of the selected studies in terms of type of patients , selection criteria and type of procedure . ghj pain is highly prevalent in elderly subjects and in overhead athletes with the highest incidence in swimmers and volleyball players of up to 43% of individuals [ 3 ] different drugs have been proposed to reduce pain and it has been suggested that optimal results can be achieved only when the drug is directly injected into the joint space [ 7 , 8 ]  . 
however , it has been claimed that for certain largely employed drugs ( e.g. , cs ) the effect on ghj pain may arise through systemic rather than local effects [ 9 , 10 ]  . beyond the therapeutic effect of drugs , extravasation should be avoided . 
for example , it been reported that in up to 5.8% case of extravasation of cs , the major adverse events can occur including osteomyelitis , protothecosis , cellulitis , ecchymosis , tendon ruptures , fat atrophy and local skin atrophy , hypopigmentation od skin substance loss [ 64 ]  . 
to our knowledge , significant adverse effects in case of extravasation of ha during intra - articular injection are not reported in literature to date . for athletes , an accurate intra - articular needle placement to correctly perform mr and ct arthrography because contrast media extravasation could obscure relevant pathological findings around the joint depending on the anatomical approach and the putative location of the abnormalities [ 11 ]  . many different anatomical approaches were proposed for blind injection using multiple bony landmarks ( such as coracoid , acromion or the soft depression between the scapula and the humeral head )  . 
loss of resistance can be used to check the intra - articular position of the needle into the joint space during the injection ( see table 1 )  . the aim of our systematic review was to assess the blind injection of the ghj that is really less accurate than landmarks and imaging - guided injection as stated on available reviews based on a limited number of articles [ 4 , 65 ]  . imaging guidance enables the operator to guide the position inside the joint visualizing the articular space . 
 table 3 features of studies by guidance technique type of guidance for the injection in the ghj number of studies cumulative number of injected shoulders highest accuracy reported in the group of study ( % ) lowest accuracy reported in the group of study ( % ) blind bony landmarks fluoroscopy us guided mri guided 1091 1 3 668 radiol med ( 2017 ) 122 : 656675 however , this approach is time consuming and implies supplementary costs . 
the present review enabled us to come to some interesting conclusions . first , this review allowed to confirm that there is an overall lower rate of accuracy reported in studies performed under imaging guidance , independently from the anatomical approach ( see table 3 )  . this observation is in keeping with previous reviews . 
 however , the present more comprehensive review revealed that five different studies using blind injection and including a total of 159 shoulders [ 25 , 41 , 43 , 47 , 55 ] reported a 100% accuracy . as mentioned , a metanalysis would be inadequate considering the number and the heterogeneity of the collected articles . 
these data suggest that in some centers the blind approach , rapid and cost effective , may be confidently used in routine practice with an accuracy challenging the accuracy than techniques imaging guidance . a comparative study of costs and benefit of this two technique is needed in a larger population of patients enrolled randomly in a multicentric study . second , the present review shows that there is no significant association between the blind injection and a poorer accuracy in subsets of patients , e.g. , subjects suffering from adhesive capsulitis [ 26 , 33 ]  . third , the extravasation rate , the procedure - related pain , vagal reactions , local anesthetic , time of procedure are very variable in both blind and imaging - guided procedures . the use of nevertheless , a recent article by karkucak et al . 
 [ 67 ] suggested that the use of a us guidance can significantly reduce the anxiety and pain related to the intra - articular injection of the ghj , while the visualization of the procedure on the screen reduces only anxiety levels but not pain score . our study has some limitations . first , as in most systematic reviews the repository of articles eligible for inclusion after the full - text analysis extraction is selected by reading a very large number of abstracts . 
it is not unlikely that , in some cases , the abstract did not match the review inclusion criteria but the full text would have been eligible for data extraction . 
 we performed a double - blind selection of the abstracts with a final consensus to limit this bias and followed the standard procedure recommended for the systematic reviews . second , as mentioned above in this study we do not provide the reader with a meta - analysis to establish the best way to place the needle inside the ghj . 
however , our large systematic review gave us the possibility to be aware that blind approach can be as reliable as guided injections in some centers and to establish that a larger randomized multicentric study is needed to confirm the real superiority of the imaging guidance . last , we did not extend our literature review to the socalled gray literature . 
that research can potentially provide information different from the articles submitted to peer - reviewed . conclusion intra - articular injection in ghj can be required for the treatment of elderly patient and overhead athletes with shoulder pain for both treatment and diagnostic purposes . 
 the overall superiority of the imaging guided approach is confirmed even if accuracy rates are variable in different studies . in five large studies , blind approach showed 100% accuracy for the intra - articular injection , challenging the performance of the imaging - guided techniques . 
 ( joint * shoulder * or glenohumeral joint * or shoulder * joint * or joint * glenohumeral or shoulder * or glenoid * cavit * ) .tw injections , intra - articular / 5 . 
all searches should be supplemented by consulting current contents , reviews , textbooks , specialized registers , or experts in the particular field of study , and by reviewing the references in the studies found . 
 x yes ( cctr , embase , medline , scopus , reference tracking ; keywords for each database are provided in the appendix i , ii , iii ) 4 . 
was the scientific quality of the included studies assessed and documented ? ' a priori ' methods of assessment should be provided ( e.g. , for effectiveness studies if the author ( s ) chose to include only randomized , double - blind , placebo controlled studies , or allocation concealment as inclusion criteria ) ; for other types of studies alternative items will be relevant . 
was the scientific quality of the included studies used appropriately in formulating conclusions ? the results of the methodological rigor and scientific quality should be considered in the analysis and the conclusions of the review , and explicitly stated in formulating recommendations . 
was the likelihood of publication bias assessed ? an assessment of publication bias should include a combination of graphical aids ( e.g. , funnel plot , other available tests ) and / or statistical tests ( e.g. , egger regression test )  . 
sixty - three patients were examined with a new dedicated spot scanning technique ( group i ) , and twenty - two patients underwent conventional segmental planning ct examinations with helical image acquisition serving as controls ( group ii )  . 
median pain reduc tion in both groups was two points on the numeric rating scale . conclusion dedicated spot scanning for planning reduced the total median effective dose of the intervention by more than 64% without increasing the number of images required during the interventional procedure . 
spot scanning is recommended for dose reduction . keywords interventional radiology computed tomography spine lumbar periradicular infiltration therapy injection radiation dosage introduction with a lifetime prevalence of up to 84% , low back pain ( lbp ) has become a major public health problem in western population with high socioeconomic costs [ 13 ]  . 
the most common risk factors are obesity and physical inactivity [ 4 ]  . a wide range of conservative , pharmacological and invasive treatment options are available to patients [ 1 ]  . 
 non - steroidal anti - inflammatory drugs ( nsaids ) have been widely used and well accepted for many years as first - line acute medications [ 5 , 6 ]  . 
most episodes of low back pain can be solved by nsaid intake combined with moderate activity , while confinement to bed turned out 1 3 706 radiol med ( 2017 ) 122 : 705712 to be counterproductive [ 7 ]  . 
among them , periradicular infiltration therapy of the spinal nerve has emerged to be one of the most widely used and best evaluated options with beneficial shortand mid - term effects [ 8 , 9 ]  . 
periradicular infiltration therapy is effective in patients with radioculopathy as the underlying cause of low back pain some patients , the epidural space is targeted instead ( epidural space infiltration , esi ) [ 9 ]  . lbp is classified as chronic when symptoms persist for more than 6 months . 
periradicular infiltration additionally seems to be beneficial as a supportive measure in patients on long - term conservative treatment or resistance to oral pharmacotherapy . various considerations play a role in deciding about the most appropriate way to perform periradicular infiltration therapy including patient safety , cost effectiveness , and clinical outcome [ 11 , 12 ]  . 
another issue is whether image guidance is necessary and which is the best modalityconventional x - ray , computed tomography ( ct ) or even magnetic resonance imaging ( mri ) [ 13 ]  . ct is the most widely used imaging modality for guiding infiltration procedures in general [ 14 ]  . 
in recent years , state - of - the - art ct scanners have become available that allow considerable dose reduction , while radiologists have focused on establishing clinical protocols using these new techniques to minimize patient exposure . 
radiation dose reduction can be accomplished by modifying the tube setup , either with regard to individual parameterstube voltage ( kv ) , electric current ( ma ) , tube rotation time ( s ) or their combinationthe tube currenttime product ( mas ) , the examination protocol , or the reconstruction software [ 2022 ]  . regarding the use of ct to guide periradicular infiltration , all steps involved might be modified to lower radiation exposure ( scout , planning scan and the intervention itself )  . 
therefore , we conducted a study to investigate the effect of dedicated spot scanning for planning purposes in terms of dose , quality , and safety compared with conventional planning ct in patients undergoing periradicular infiltration . materials and methods patients this retrospective study was approved by the institutional review board ( irb ) and included 85 patients who underwent single - site periradicular infiltration therapy of the lumbar spine for relief of lbp . 
informed consent was obtained from patients included . procedure we performed all periradicular infiltrations on an 80 - slice ct scanner ( toshiba aquilion prime , toshiba medical systems , ottawara , japan ) and recorded tube current ( mas ) , tube voltage ( kv ) , and the resulting dose - length product ( dlp ) in mgy cm separately for the planning part and interventional part . 
routinely , patients receive a segmental helical planning ct scan 4 cm in length ( 40 images , 1 mm slice thickness ) acquired with 120 kv and 20 mas . 
the new dose reduction protocol consisted of a single - volume spot scan ( collimation and reconstruction : 4 1 mm slice thickness at 100 kv and 10 mas )  . 
patients were asked to assess their average pain on a numeric rating scale from 0 ( no pain ) to 10 ( worst pain one can imagine ) prior to the intervention and again 6 weeks thereafter . 1 3 radiol med ( 2017 ) 122 : 705712 fig . 
1 ae planning includes a lateral scanogram ( a ) followed by spot scanning with acquisition of four axial images ( de ) of the spinal segment to be treated . 
spot scanning dose is here 0.80 mgy cm table 1 scanning parameters of both groups group i group ii planning mode single volume of 4 mm helical scan of 4 cm pl . 
we calculated deff by multiplying the dose - length product with a previously reported tissuespecific conversion factor of 0.015 , which is generally accepted for abdominal ct imaging [ 26 , 27 ] : d_eff = ( 0.015msv ) / ( mgy cm ) dlp data analysis results statistical analysis and plots were generated using r ( version 3.2.3 , r foundation for statistical computing , vienna , austria ) , which is a gnu project with copyright by the r foundation . the shapirowilk test indicated nonnormal distribution . 
the new protocol was used in 63 patients ( group i : 39 female , 24 male , median age 61 ) and compared to 22 patients with the conventional setup ( group ii : 12 female , 10 male , median age 54 )  . 
since esi and periradicular infiltration use the same technique for treating radiculopathy - associated lbp and target the same anatomic region , we here consider results for the two interventions in terms of overall radiation exposure interchangeably . 
the resulting median dlp doses were 1.24 mgy cm for spot scanning and 3.71 mgy cm for the interventional procedure , resulting in a total dlp of 4.94 mgy cthis low planning dose was accomplished by additionally using available images from table 4 summary of setup and dose parameters during intervention group i group ii p ( wilcoxon ) median range median range dlp planning ( mgy cm ) dlp intervention ( mgy cm ) acquisitions dlp total ( mgy cm ) calculated eff . 
reported a mean dlp of 13.87 for a low - dose protocol investigated in a feasibility study in patients undergoing periradicular infiltration [ 32 ] ; however , obese patients ( bmi > 30 ) were excluded . 
this confirms the robustness of our protocol in patients with higher weight , which is a serious limitation of existing low - dose ct protocols . a major difference of our protocol is that we lowered the tube currenttime product even further compared with the studies discussed above . 
this protocol fully exhausts the potential of dose reduction , because the ct images meeting these criteria need not be of full diagnostic image quality . our successful implementation of spot scanning might not only be advantageous in terms of dose reduction for planning periradicular infiltration therapy but also other ct - guided interventions such as bone puncture , thoracocentesis and lung biopsy . our study has some limitations including its retrospective design . 
there is a misbalance because as the new protocol on trial performed so well we considered it unethical to continue using the higher dose protocol only to have more patients for our control . 
in addition , we enabled aidr 3d ( adaptive iterate dose reduction 3d , toshiba medical systems ) in the scan protocol , a vendor - specific convolution filter that significantly reduces image noise [ 3335 ]  . 
however , this requires individual adjustment and gives up the advantage of using the same planning protocol for all patients . while the planning and interventional ct scan is confined to a few sections in the region to be treated , the dose reduction potential that can be achieved by modification of the scout remains to be explored . the outcome of the interventions was assessed by asking patients for a subjective assessment of the severity of low back pain before and after treatment . 
inclusion of additional parameters ( e.g. , pain peaks , pain quality , functional tests ) would allow a more refined evaluation of therapeutic effects . conclusion the spot scanning ( 100 kv , 10 mas ) protocol presented here allows reduction of the median planning dose by approximately 88% , resulting in over one - third greater dose reduction compared with the results reported by recent studies . 
we can fully recommend our complete ultra - low - dose protocol for planning and conducting periradicular infiltration therapy of the lumbar spine for clinical application , allowing dose reduction while maintaining full patient safety . compliance with ethical standards conflict of interest fabian henry jrgen elsholtz declares that he has no conflict of interest . 
stefan markus niehues declares that he has no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
patient risk factors evaluated include age , inr ( international normalized ratio ) , creatinine , bilirubin , and meld score ( model for end - of - stage liver disease )  . 
the development of he represents an important drawback of this otherwise valuable and life - prolonging intervention [ 2 , 5 , 7 ] , being associated with significant morbidity and increased mortality [ 8 , 9 ]  . 
he post - tips is typically attributed to the portosystemic shunt , but can be precipitated by abrupt changes in portal perfusion , shunt dysfunction , multiple hepatic re - interventions , and recurrent gastrointestinal bleeding or ascites [ 6 ]  . 
patients factors which might have an impact on the onset and features of he are age , international normalized ratio ( inr ) , serum creatinine , serum bilirubin , and the model for end - of - stage liver disease ( meld ) score obtained from the latter three variables [ 7 ] , which is an excellent predictor of survival in patients with end - stage liver disease . the classification of he as minimal , moderate , and severe was standardized in 1998 [ 10 ] and recently reviewed in 2014 in a more comprehensive classification [ 11 ]  . 
some studies considered the overall episodes of he , whereas others considered only the new or worsened he episodes ; some investigators selected the episodes that occurred without an evident precipitating cause [ 9 ] , and others , those leading to hospitalization [ 5 ] ; overt / covert differentiation was rarely used , while in most cases , moderate / severe classification is widely accepted [ 4 ]  . 
 moreover , even if the diagnosis of severe he is relatively straightforward on clinical grounds , it requires exclusion of other neuropsychiatric disorders that can be responsible for similar clinical findings . 
the reporting heterogeneity and the fact that only a few studies have a long - term followup also affects the available meta - analyses [ 7 ]  . an alternative he classification based on the temporal occurrence and recurrence patterns of he after tips was proposed in recent guidelines [ 11 ] , but , as far as we know , it has not yet been used by radiologists . the open questions are as follows : radiol med ( 2017 ) 122 : 713721 is it possible to identify pre - tips indicators ( biomarkers ) of the middle ( 6 months ) and long - term ( 1 year ) post - tips outcome ? for instance , how are the patients risk factors associated with the he onset , features , and resolution ? 2 . 
which extra information can be derived using both severity and time pattern classification ? herein , we report and discuss the outcome of a retrospective evaluation of incidence , features , and evolution of he in a cohort of cirrhotic patients treated with tips in our unit and followed for at least 1 year by the hepatology reference centre of our hospital . 
the goal of our study was to obtain a representation of the scenario at 6 and 12 months after the procedure based on both he classifications ( sever ity and temporal pattern grading )  . materials and methods study population we retrospectively analyzed the radiological and clinical records of all consecutive cirrhotic patients who underwent a technically successful tips procedure in our unit from january 2008 to november 2014 and completed a 12 month follow - up ( fu ) period . 
exclusion criteria were : lack of complete clinical information ( 112 ) , liver transplantation during fu ( 43 ) , death during fu ( 21 ) , and pre - tips encephalopathy , since it might introduce a non - controllable bias ( 25 )  . 
the final sample thus included 75 / 276 ( 27% ) patients . we chose to analyze the patients status as determined by our hepatology reference centre at 6 and 12 months as the best representative of the middle and long - term posttips evolution . the study was conducted in good clinical practice according to the helsinki declaration of 1975 and subsequent modifications . 
in 71 patients , a single dilation was sufficient ; when using the viatorr stent , the dilation was performed with balloon catheters of maximum nominal diameter between 8 and 12 mm , while for patients with luminexx or wallstent stents , dilation ranged between 8 and 14 m balloon dilation was followed by shunt venography . in five cases ( 7% ) , the procedure was completed by embolization of the varicose periesophageal or perigastric circles , highlighted on pre - procedural diagnostic angiography . 
after catheterization , the pressure before and after the balloon dilatation of the hepatic parenchymal tract was evaluated . following tips procedures , patients underwent inpatient monitoring for 4872 h and were then followed as outpatients in the reference centre for liver failure and transplantation . 
medication and diet of 75 patients after tips was the samewe recommended low - protein intake within 3 months after tips , especially the first month , and patients are always asked to keep good bowel movement . 
 no patients were treated with anticoagulant therapy . 1 3 716 he classification we followed the he classification proposed in 2014 by the aasld / easl [ 11 ] , adopting two different classifications : 1 . 
time pattern classification , often used in gastroenter ology [ 11 , 1517 ] , but generally neglected by radiologists , divided into episodic occurrence and recurrent ( bouts of he occurring within 6 months or less ) or persistent ( always present with intermittent episodes of overt he ) occurrence . statistical analysis continuous variables were tested for normality with the shapirowilks test . 
when normality was accepted ( age ) , standard deviation ; the data were presented as mean when normality was rejected ( other risk factors ) , the data were presented as median and interquartile range ( iqr )  . 
 comparisons employed non - parametric tests for k distribu2 and kruskalwallis tions mannwhitney test for k test for k > 2 independent distributions ; wilcoxon test for 2 ; and friedman test for k > 2 correlated distributions . the ability to differentiate between healthy and pathological conditions was tested with the receiver operating characteristic ( roc ) curve procedure ; the quality of discrimination was quantified by the area under the curve ( auc ) , ranging from 0.5 ( chance ) to 1 ( excellent )  . 
the threshold between the two conditions was set at the value which maximized joudens index j and the harmonic mean ( hm ) of sensitivity ( sns ) and specificity ( spc ) while minimizing the distance d of the curve from the ( 0 , 1 ) upper left vertex . 
sns and spc were used to determine the likelihood ratio of a positive test lr , i.e. , the likelihood that a positive test result would be expected in a patient with disease compared to the likelihood that the same result would be expected in a patient without disease . categorical variables , reported as counts and percentc tables studied with the chiages , were arranged in r square test ( with yates correction for 2 2 tables ) or with fishers exact test . 
mcnemars test was used to assess the difference between two correlated proportions . statistical significance was set at two - tails p < 0.05. the analysis was carried out with open source softwares ( and http : / / www.vassarstats.net ) and statplus : mac version v6 ( analystsoft , walnut , usa )  . 
 all statistical procedures were run on at least two different packages . radiol med ( 2017 ) 122 : 713721 the statistical power of the study in some comparisons suffered from the low sample sizes , so some borderline values of p > 0.05 may actually hide significances that the test could not evidence ; however , all results reported as significant originate from 80% power tests . results he incidence and risk factors table 1 shows the liver disease etiology and indication for tips for the 75 patients as assessed through the available clinical records . at 6 months after tips , 27 / 75 ( 36% ) patients were diagnosed with at least one episode of he . 
the results were confirmed by the outcome of the logistic regression . we considered the four patient - related risk factors meld score , inr , creatinine , and bilirubin , and the presence of a large volume of ascites on the day of tips procedure . 
2 age and frequency distributions on the two samples table 3 compares the pre - tips values for the 31 patients who at different times were diagnosed with he and the 44 patients who did not have he in the entire fu year . 
the main features of the 47 hes observed at 6 and 12 months ( 41 moderate and six severe ) are reported in table 5 ( left side )  . at 6 months , there were 13 patients with episodic he and 14 with recurrent / persistent he ; at 12 months , there were three episodic hes and 17 recurrent / persistent hes . 
3 evolution of bilirubin over the three stages pre - tips , he , and recovery he classification the 31 patients who suffered from he had a total of 47 he diagnoses ( 27 at the 6 - month check - up and 20 at the 12 - month check - up )  . 
table 4 shows how they fit the two classificationsin horizontal , the severity grading ; in vertical , the time recurrence pattern ; and in bold , the two conditions that combine a high level of severity with a high frequency of recurrence , i.e. , the worst to manage and those seriously damaging the quality of life of the patients . 
44 / 75 ( 59% ) patients enjoyed complete freedom from he , and 13 / 75 ( 17% ) had only one episode of moderate he overall , the procedure may be considered safe for 57 / 75 ( 76% ) patients . 
casadaban [ 23 ] described an acute ( within 7 days ) twoto three - fold increase in bilirubin , typically resolved within 2 weeks , remaining far from the baseline value only for patients with 90 - day mortality . 
 the transient nature of these alterations is explained by the sudden decrease of hepatic flow ; the subsequent arterial perfusion compensation ( the hepatic arterial buffer response [ 24 , 25 ] ) may allow relative normalization of laboratory test results after tips . 
although the authors do not describe any correlation between hepatobiliary enzymatic elevation and he , we can assert that the more compromised is the liver function ( e.g. , longer is bilirubin elevation ) , the higher is the risk of he . 
it is the precisely timed association : he presencehigh bilirubin versus he absencebasal bilirubin that prevents bilirubin to be used as pre - tips predictor . the overall incidence of patients with he at 6 months ( 36% ) of our series is at the bottom of the range of values present in the literature ( from 30 to 60% )  . 
 [ 7 , 18 , 19 ] considering both severity and temporal pattern grading , we obtain that a large percentage of patients ( 76% ) had no he or had a single moderate episode that was easily managed . 
inr is a marker of liver function which is known to usually increase in the latest stages [ 26 , 27 ] of liver disease , when presumably patients may suffer from more frequent he episodes . 
we could not evaluate 3 - month ( short - term ) hes according to the existence of precipitating factors nor use the overt / covert classification for lack of information in the patients files . conclusions our study determines an overall he incidence of 36% at 6 months , decreasing to 27% at the 1 - year fu . 
the comprehensive ( severity and temporal ) classification of he evidenced that the more devastating form of severe recurrent / persistent he struck only 4% of the patients . age can be considered as pre - tips risk predictor , advising a careful evaluation of patients over 60 years for their significantly higher probability of he . 
furthermore , bilirubin is closely associated with the level of severity characterizing the he , whereas inr is associated with the temporal occurrence of he . although our study involves one of the biggest single institution series [ 7 ] , a reliable test of the validity of the cross - classification matching severity and frequency will require a specifically designed prospective study , possibly a well - coordinated multicenter study to collect large numbers in a short period of time , guaranteeing the necessary homogeneity of treatment . 
 laura bergamasco provided statistical advice for this manuscript . compliance with ethical standards conflict of interest the authors of this manuscript declare no relationships with any companies , whose products or services may be related to the subject matter of the article . ethical standards institutional review board approval was not required because of its retrospective nature . 
the study was conducted in good clinical practice according to the helsinki declaration of 1975 and subsequent modifications . informed consent written informed consent was obtained from all patients in this study . 
two independent readers ( r1 , trained radiology resident ; r2 , lower - trained technician student ) obtained segmented images twice ( > 10day interval ) , using a semi - automated method of segmentation . 
r1 intra - reader reproducibility for the aorta was 99% ( peak velocity ) , 95% ( forward flow ) and 49% ( backward flow ) ; for the pulmonary artery , 99% , 91% and 90% , respectively . 
especially for patients affected with congenital heart disease , cmr plays an important role in 1 3 180 radiol med ( 2017 ) 122 : 179185 the quantification of blood flow and evaluation of valve stenosis / insufficiency using phase - contrast ( pc ) throughplane sequences [ 211 ]  . 
the pc sequences were validated in phantom and in vivo studies and have proven to be a reliable tool for the quantitative and qualitative analysis of blood flow and tissue motion [ 12 ]  . despite its importance for the assessment of disease progression , few data are available about the reproducibility of cmr in the measurement of blood flow in patients with valve stenosis and / or insufficiency [ 2 , 1315 ]  . 
moreover , segmentation methods were validated indirectly , through the ability to provide accurate flow measurement [ 13 , 16 ] or pulse wave velocity [ 16 , 17 ] or directly in terms of operator variability [ 13 , 14 ] or agreement with manual tracing [ 17 ]  . blood flow measurements are based on the segmentation of a vessel contour that may be performed manually or , more typically , semi - automatically , with the use of computer software likely impacting on measurement reproducibility . 
reader experience may play a role as well . thus , the aim of our study was to estimate the intraand inter - reader reproducibility of blood flow cmr measurements through the ascending aorta and main pulmonary artery in patients affected with congenital heart disease or with aortic and / or pulmonary valve disease . 
 time resolution 41 ms ; mean acquisition time 15 for each patient , we initially acquired the pc sequence with a venc of 150 cm / s : in the presence of aliasing , we increased the venc adding 50 cm / s for each new sequence , step - by - step up to the complete disappearance of the aliasing artifact . flow measurements were performed right above the aortic or pulmonary valve in patients with surgical or percutaneous valve replacement . 
the magnitude image depicts the anatomy and allows to identify the vessel boundaries , while the phase velocity map corresponds to blood velocity [ 2 ]  . two independent readers ( r1 and r2 ) performed measurements twice , with at least a 10 - day interval between the two sessions , for a total of four sessions . 
 blandaltman graphs were plotted as well , showing bias ( mean of the differences of the two compared datasets ) , and 95% limits of agreement ( bias cor )  . results of 50 analyzed patients , 46 ( 92% ) had a pulmonary disease , two ( 4% ) ventricular septal defect , one ( 2% ) aortic insufficiency , and one ( 2% ) truncus arteriosus . 
the time needed for measurement was about 5 min per patient , without substantial difference between the two readers . the mean blood peak velocity of the aortic flow measured by r1 was 103 cm / s , accompanied by a cor of 1 cm / s , corresponding to an intra - reader reproducibility of 99% ; the same data for r2 were 103 cm / s , 9 cm / s , and 92% . 
the mean blood peak velocity of the pulmonary flow measured by r1 was 180 cm / s , accompanied by a cor of 1 cm / s , 1 3 182 table 2 intra - reader reproducibility of the first reader radiol med ( 2017 ) 122 : 179185 pulmonary flow forward ( ml / beat ) backward ( ml / beat ) forward ( ml / beat ) backward ( ml / beat ) aortic flow peak velocity ( cm / s ) mean bias reproducibility the first reader was a radiology resident ( see text ) cor coefficient of repeatability mean bias reproducibility the second reader was a technician student ( see text ) cor coefficient of repeatability peak velocity ( cm / s ) peak velocity ( cm / s ) table 3 intra - reader reproducibility of the second reader aortic flow peak velocity ( cm / s ) pulmonary flow forward ( ml / beat ) backward ( ml / beat ) forward ( ml / beat ) backward ( ml / beat ) corresponding to an intra - reader reproducibility of 99% ; the same data for r2 were 181 cm / s , 3 cm / s , and 98% . 
 the inter - reader reproducibility analysis of the aortic flow peak velocity showed a cor of 10 cm / s , over a mean of 103 cm / s , corresponding to an inter - reader reproducibility of 91% ; the same data for the pulmonary flow were 7 cm / s , 180 cm / s , and 96% . 
3. discussion cardiac magnetic resonance has emerged as a reliable imaging technique for assessing heart valve disease , quantify its severity , and to evaluate its effect on the heart morphology and function [ 13 , 7 ]  . 
patient management using cmr includes follow - up for treatment effect monitoring or disease progression [ 19 , 20 ]  . reproducibility means the ability of a reader to provide the same values when repeating the measurement a number of times . 
when a follow - up measurement is performed on a patient , the clinician needs to identify a true change that can be ascribed to treatment effect or worsening of disease , rather than to measurement errors [ 21 ]  . 
in this scenario , the readers experience may play a role and skilled operators may be necessary . in this study , we obtained a good - to - excellent intrareader reproducibility of cmr in flow measurement for all variables under consideration , except for the backward flow of the ascending aorta . 
indeed , intra - reader reproducibility was higher than 90% for the trained reader ( r1 ) and higher than 86% for the lower trained reader ( r2 )  . 
such a good result may be due thanks to the semi - automated method used for segmentation that is not difficult to be used also by less experienced readers [ 9 ]  . 
this means that a readers learning curve should be short and that the segmentation of vessel boundaries through a semi - automated method may also be performed by not highly specialized personnel . 
however , although of a small magnitude , data suggest an additional reproducibility of r1 over r2 , likely due to the different educational background and the different level of training [ 9 ]  . inter - reader reproducibility , even if reaching a maximum of 96% for the blood peak velocity of the pulmonary artery , decreased to 75 and 82% for the forward and backward flow of the pulmonary artery , respectively , being lower than 1 3 radiol med ( 2017 ) 122 : 179185 fig . 
2 blandaltman plots for intra - reader reproducibility analysis of the first reader : a and b peak velocity , c and d forward flow and e and f backward flow of the aorta ( left column ) and pulmonary artery ( right column ) table 4 inter - reader reproducibility analysis aortic flow peak velocity ( cm / s ) forward ( ml / beat ) backward ( ml / beat ) forward ( ml / beat ) backward ( ml / beat ) pulmonary flow peak velocity ( cm / s ) mean bias reproducibility cor coefficient of repeatability 1 3 184 radiol med ( 2017 ) 122 : 179185 fig . 
3 blandaltman plots for inter - reader reproducibility analysis : a and b peak velocity , c and d forward flow and e and f backward flow of the aorta ( left column ) and pulmonary artery ( right column ) that observed in previous studies . 
compared an automated contour detection algorithm for analysis of the ascending aorta flow with a fully manual segmentation , showing intraand inter - reader variability lower than 2% for both manual and automated methods [ 13 ]  . 
in fact , a low to very low reproducibility for this variable was obtained , being lower than 50% for the intra - reader analysis and equal to 20% for the interreader analysis . 
reproducibility being given as percentage of the mean , even subtle measurement variations due to small 1 3 radiol med ( 2017 ) 122 : 179185 differences in segmentation may have a strong negative impact on reproducibility . the major limitation of this study is that results are related to the particular 1.5 - t unit used for imaging patients and to the sequences and technical parameters used , also including the use of breath - hold or respiratory gating for avoiding artifacts from respiratory movements . 
another limitation may be the study population that included patients affected with different cardiovascular diseases ( even if the majority of patients had a tetralogy of fallot ) who had a pathology of the aortic and / or pulmonary valve . 
probably , limiting to a more homogeneous population could demonstrate an even higher reproducibility . in conclusion , this study showed a good - to - excellent intraand inter - reader reproducibility of blood flow measurements in patients with congenital heart disease using cmr and a semi - automated method of segmentation , with a limited impact of the operators training . compliance with ethical standards conflict of interest f . 
in us and europe pediatric radiologists had to face a huge challenge , which brought to the image gently campaign and the eurosafe initiative with the aim to rebut misinformation and to support medical radiation protection . 
the linear no threshold modelwhich is the base of contemporary radioprotectionis increasingly questioned by new recent studies suggesting that low dose radiation would decrease cancer risk thanks to the enhancement of immune system response . 
 when considering benefits and risks , an important risk is * claudio granata cgranata@sirm.org imaging department , bambino ges childrens hospital , irccs , 00146 rome , italy 2 clinical technology innovations research area , bambino ges childrens hospital , irccs , 00146 rome , italy 3 department of radiology , irccs istituto giannina gaslini , 16147 genoa , italy too often ignored : the risk that skipping a diagnostic exam may cause a misdiagnosis , and therefore , a poor outcome . 
the first sentence in sternbergs usa today article was each year , about 1.6 million children in the usa get ct scans to the head and abdomenand about 1500 of these will die later in life of radiation - induced cancer , according to research out today [ 2 ]  . obviously , the article had international echo and paediatric radiologists found themselves facing a huge challenge , which mainly concerned the use of ct [ 4 ]  . 
in the us , their response was brilliant : they created image gently [ 5 ] , not only to implement changes in paediatric radiology practice , but also as a defence mechanism to rebut misinformation . 
eurosafe pursues similar objectives : its mission is : to support and strengthen medical radiation protection across europe following a holistic , inclusive approach [ 8 ]  . finally , the global media campaign had positive results on industry research , and , together with the medical culture , powerfully contributed to reduce substantial variability in imaging techniques used in paediatric imaging also among non - paediatric centers and impelled industry to develop more efficient imaging technologies . 
there were continuing efforts to develop diagnostic reference levels ( drls ) throughout the world and drls for paediatric ct have been established or studied in several european countries [ 9 , 10 ]  . 
the recent pidrl document [ 11 ] is a synthesis of the european reports , and a proposal for a standardized method for the development of future drls in children . 
drls are an advisory measure to improve optimization of patients protection by identifying high patient dose levels that might not be acceptable on the basis of image quality prerequisites . the facts in the present study we considered publications concerning risk of cancer as related to computed tomography scan . 
we subsequently refined the search including further terms , namely adult , child , neoplasms , radiation - induced , radiation dosage , radiol med ( 2017 ) 122 : 215220 radiation exposure , alara . 
in this way we found 1217 articles . the three most cited articles are also the most pessimistic : 3906 citations for the article computed tomography an increasing source of radiation exposure from brenner et al . 
 [ 13 ] , 913 for the article radiation exposure from ct scans in childhood and subsequent risk of leukemia and brain tumours : a retrospective cohort study from pearce et al . 
these simulations were performed by making use of series of computational human paediatric phantoms along with realistic age - dependent ct acquisition parameters [ 3 , 14 , 1720 ]  . the judgement on damage and alarm makes a huge noise and widespread public concern . actually , when we focus on dose management , we paradoxically accentuate the perception that medical imaging doses are dangerous . 
after all , why would we want to manage / reduce the dose if it were not dangerous ? shocking publications continue to be issued and become the titles of newspaper commentaries . 
the methodology used by pearce was harshly criticized by cohen ( only 2 citations ) [ 7 ] , who underscored that , although 178 , 000 children were studied , the study design had major flaws and information reporting was inaccurate . 
in fact , the first proposition of the paper maintained that the authors obtained typical machine settings for ct in young people from u.k. - wide surveys undertaken in 1989 and 2003 . 
 moreover , the study had no control population , and the authors did not evaluate pre - existing conditions that may be related to cancer ( reverse causality )  . 
 ( only 11 citations ) estimated the cancer risk related to childhood ct scans , and examined how cancerpredisposing factors affect radiation - related risk assessment [ 17 ]  . 
 [ 17 ] ( 0 citations ) and states : there are several major differences that complicate direct comparison with our study , particularly the different calendar periods of exposure : 19802002 in the united kingdom vs 20002010 in france . 
in addition , their study population came from a number of specialist hospitals , which resulted in an enriched population for serious conditions and finally they used hospital inpatient data to ascertain the clinical conditions . 
they also used a somewhat different list of cancer - predisposing conditions . surprisingly , there are many uncertainties and there are many inconsistent publications stating that ct scans cause cancer in children . similar biases are in the article of mathews et al . 
this was a retrospective study based on a database concerning people aged 019 years , who had ct scan done during the period 1 january 1985 to 31 december 2005 . 
the authors estimated lifetime attributable risk of cancers from the observed organ doses using ageand sex - specific cancer risk models in the biological effects of ionizing radiations ( beir ) vii [ 16 ] they stated that theoretically nationally , 4 million paediatric ct scans of the head , abdomen / pelvis , chest , or spine performed each year are projected to cause 4870 future cancers . 
however , this study concludes there are 95% uncertainty limits around the projected numbers of cancers on the basis of the coefficient of variation given in the beir - vii report , which provides a gross variability estimate from these three sources of uncertainty . 
unfortunately , only the first message attracted attention . a common issue with studies dealing with radiation exposure from ct studies and cancer risk is the lack of information about the indications for the ct examination . 
terrifying assumptions have easy success . for this reason , it is important to know and understand the opinions of those who question current thinking . the linear no threshold ( lnt ) model is based on the linear relationship assumption summarised as : radiation / mutation and cancerous mutation / cancer . 
the life span study ( lss ) cohort of about 120 , 000 subjects included atomic bomb survivors and residents of hiroshima and nagasaki who were not in either city at the time of the bombing . 
british radiologists who entered service during the period 19551979 , who were likely to be exposed to low - dose radiation , had a cancer death rate lower than the background cancer rate [ 20 , 34 ]  . conclusions paediatric radiologists have many important issues and challenges to deal with . in europe , council directive 2013 / 59 / euratom established that should strengthen the requirements concerning information to be provided to patients , the recording and reporting of doses from medical procedures , the use of diagnostic reference levels and the availability of doseindicating devices . on july 2015 , joint commission stated : the radiation dose ( ctdivol or dlp ) must be exam - specific , summarized by series or anatomic area , and documented in a retrievable format . 
bias by indication : ct is performed for the detection or monitoring of a pathology or symptomatology associated with higher risk of cancer , for example because of a particular genetic syndrome or acquired immunodeficiency . 
the most effective means to decrease radiation dose associated with paediatric imaging is to reduce or preferably eliminate unnecessary or inappropriate procedures , but justification and guidelines depend on different cultures and factors , such as defensive medical decision making . 
malpractice lawsuit is often seen as a mechanism to improve quality of care , but it may actually impede the translation of evidence into practice , damaging patients and decreasing the quality of care . optimization is a process by which a substantial portion of the standard dose is eliminated with a consequent increase in noise , but without loss in diagnostic performance and / or confidence to accomplish the specified medical task . 
in six us paediatric radiology institutions using standard clinical protocols and radiation doses below the 25th percentile , 5% of the studies were judged to be nondiagnostic [ 30 ]  . 
this issue is the essence of clinical ct dose reduction : what do i need to detect ? how much dose do i need to confidently detect its presence or absence ? peer review fails more and more often . 
for instance , all articles on alternative techniques ( us , mri ) for the study of the chest report the absence of ionizing radiation as 1 3 radiol med ( 2017 ) 122 : 215220 ct exams exceeded expected dose ranges identified in imaging protocols [ 35 ]  . going beyond legal problems , a positive message is needed to give confidence . good medical practice includes efficient communication about the benefits and risks of health procedures . 
several stakeholders are involved in the communication of radiation risks and benefits in paediatric imaging : parents , patients , and caregivers . for instance , it is difficult to empathise when speaking about dose units , risk , likelihoods and stochastic effects . 
 in the communication on the risks , the comparison with familiar radiation exposures ( such as chest x - rays or natural background radiation ) has been highly recommended to facilitate understanding of the dose [ 29 ]  . 
but the dose delivered during a chest x - ray is so low that using it as a denominator to estimate the corresponding amount of chest x - rays equivalent with the dose level of any other radiological practice may be misinforming and may unreasonably alarm paediatricians and parents . 
when considering benefits and risks , there is an important risk which is too often ignored : the risk that skipping a diagnostic exam may cause a misdiagnosis , and therefore a poor outcome . 
we are not sure that there is a risk at very low doses , like those doses in the vast majority of x - ray procedures or ct [ 29 ]  . in clinical practice , all these discussions should help determine the situations in which the estimated benefits do not balance the risks and clarify the information to be provided to patients , parents and health - care providers . so far , prudently and wisely , it is correct to follow the risk predictions extrapolated from studies at high doses under the lnt postulation . 
vogl1 stephan zangos4 received : 7 june 2016 / accepted : 14 november 2016 / published online : 28 november 2016 italian society of medical radiology 2016 abstract objective purpose of our study was to demonstrate the feasibility and limitations of acoustic noise reduction in a standard clinical mri protocol for abdominal imaging . methods acoustic noise and image quality were assessed in 17 patients for a standard liver imaging protocol including tse and gre sequences and compared to quiet optimizations as described by heismann et al . 
 during the last years diffusion - weighted imaging ( dwi ) has been increasingly used for the detection and characterization of liver tumors [ 2 ]  . despite the known benefits of mr - imaging , some patients reject an mri examination . 
the most prominent reason for the noise is caused by mechanical vibrations of the gradient coil during rapid switching of the gradients , which intimidate patients who are either physically susceptible to the damaging effects of loud noises like patients of young or old age or patients with cognitive disorders . 
food and drug administration regarding mr - related acoustic noise levels state than an unweigthed peak sound pressure level of 140 db and an a - weighted sound pressure level greater than 99 dba with hearing protection in place should not be exceeded [ 3 ]  . 
the widely used decibel a filter roughly corresponds to the inverse of the 40 db curve with equalloudness for the human hearing at 1 khzalthough it is no physiological parameter . 
reported mr imaging - related sound levels to vary from 84 to 103 db on the linear scale and 8293 db on the a - weighted scale [ 6 ]  . 
studies including pulse sequences with multiple gradients applied simultaneously like three - dimensional , fast gradient echo techniques were reported to have the loudest peak acoustic noise ranging up to 113 dba [ 5 ]  . 
especially sequences with very fast gradient switching and high amplitudes like echo planar imaging suffer from high levels of noise , exemplarily described with 114115 dba for a 1.5 t scanner system by shellock et al . 
for systems with 3 tesla even higher sound levels can be found [ 7 ]  . during the last decades different hardware - based or sequence - based approaches were tested to minimize acoustic mri noise . 
the least expensive way of noise attenuation consists of using earplugs or headphones , which on the one hand decreases acoustic noise by 1030 db , but on the other hand provides a non - uniform noise attenuationusually with poor attenuation results for the typically low mr - imaging related noise frequencies . 
by applying a gradient smoothing algorithm to the standard gradient course the gradient ramps are softened in the modified quiet sequences cancellation has been accomplished in the late eighties using an interference with generated antiphase noise [ 8 ]  . during the last years quiet pulse sequences have been developed , which can even be used with echo planar imaging [ 911 ]  . 
in this approach , an automated gradient smoothing algorithm is applied that subdivides any given pulse sequences into change segments where gradients may be optimized and keep segments in which gradients must remain unchanged , like during excitation and data acquisition . 
in change intervals a spline interpolation is used that keeps the m0 and if needed the m1 moment , which are characterized by the following formulas : m0 = g ( t ) dt m1 = tg ( t ) dt ( cid : 31 ) t1 ( cid : 31 ) t1 with g ( t ) representing the temporal gradient course and t1 and t2 as start and end points of the change interval . 
standard deviations were given for tr and te as parameters featured slight variations among examinations protocol and a protocol with the modified quiet pulse sequences ( table 1 ) , which are commercially available as the siemens quiet suite . 
the quiet sequences feature unchanged intervals comprising radiofrequency pulse and read - out activity , but changed settings in intervals with gradient activity by application of a fourth - order spline interpolation to reduce slew - rates as described by heismann et al . 
except from changed gradient activity imaging parameters were not subject to change . examinations were carried out after informed consent on a 3 t scanner in clinical route with a standard 32 - channel body coil ( magnetom prismafit , siemens healthcare , erlangen , germany ) and a delay of 3 months between the standard protocol and following the quiet protocol . 
 the non - hepatobiliary contrast the administration of agent given per quantity of body weight contained either dotarem ( 0.05 mg / kg ) or gadovist ( 0.01 mg / kg ) and was performed by a standard injector ( accutron mr , medtron ag , saarbrcken , germany ) with a flow of 2 ml / s . the study was performed in accordance with the ethical standards of the institutional review board and with the 1964 helsinki declaration and its later amendments . 
a sound level meter ( sl - 100 , voltcraft , germany ) was placed in front of the bore , facing the isocenter in a distance of 3 the sound level meter was set to two frequency evaluation modes : a mode accounting for the characteristic hearing curve perceived by the human ear ( dba ) and a technical mode receiving a linear frequency curve ( dbc )  . 
during the acquisition of each mri sequence the sound pressure level l was recorded once per second for 125 ms in dbaand dbc - mode over 10 s and an average sound level lm was calculated using the equation : lm = 10 log ( cid : 31 ) ( cid : 30 ) 10li / 10 ( cid : 29 ) with li being the ith recorded value per measurement out of n data values [ 14 ]  . 
in addition to these objective results subjective impressions of the patients have been recorded and evaluated . the loudness ratio z of the quiet and standard sequences was determined from the perceived change in sound pressure level lm by taking the logarithmic character of the unit decibel ( db ) into account : z = 2 ( cid : 31 ) lm lm standard lm quiet in a subjective questionnaire the test persons named the sequence they preferred and had the chance to note differences in their personal acoustic perception . 
the psychoacoustic loudness ratio was calculated for each set of sequences image evaluation cnr = ( siliver simuscle ) /  . the evaluation and comparison of the mr images was performed retrospectively on a standard pacs workstation ( ge healthcare , il , usa ) by two independent blinded radiologists with a different level of experience ( 3 / 12 years ) in abdominal imaging . subjective overall image quality , the delineation of the abdominal organs and the level of confidence in visualization of the anatomy and pathologies was assessed using a 5 - point scale ( 1 : very poor , 2 : poor , 3 : fair , 4 : good , 5 : excellent )  . 
therefore , each of the following anatomic structures were rated : liver parenchyma , liver arteries and veins , portal vein , hepatobiliary duct , gallbladder , pancreas , pancreatic duct , kidneys , adrenal glands , spleen and lymphatic nodes . 
 the evaluation included a general evaluation of artifacts due to cardiac motion , respiratory motion or bowel movement , scored on a 3 - point scale ( 0 : no visible artifact , 1 : minimal artifact that did not interfere with diagnostic quality ; 2 : severe artifact that interfered with diagnostic quality )  . signal intensities ( si ) , signal - to - noise ratio ( snr ) and contrast - to - noise ratio ( cnr ) were measured and calculated for the liver and muscle in each native sequence ( t2 haste , t2 tse , t1 dixon ) and in contrast - enhanced sequences ( t1 flash , t1 dixon )  . 
a circular region of interest ( roi ) with a diameter of 1 cm was placed inside a region free of artifacts and nutritive vessels inside the liver parenchyma and the musculus latissimus dorsi , respectively . 
its location and diameter was visually matched to the corresponding other sequences to achieve optimal intra and inter - individual comparability . snr was calculated out of the mean pixel intensity value of the roi as the si and from the standard deviation ( ) in pixel intensity of the background air as noise according to the method used by the american college of radiology ( acr ) [ 15 ]  . 
for calculation the following equation was used : snr = si /  . the cnr was calculated by the difference of the si in liver parenchyma and muscles , divided by the background noise according to the equation : furthermore both radiologists undertook a randomized , blinded side - by - side comparison of the standard and quiet sequences , rating them as inferior ( 1 ) , comparable ( 0 ) or superior ( 1 ) regarding subjective image quality . statistical analysis statistical analysis was performed using an explorative data analysis . 
the descriptive statistics included the mean , standard deviation , minimum and maximum values . the means of the sound level measurements , the snr and cnr were compared in a paired two - sided t test using holm - sidak method with a significance level set at 0.05. visualization of the sound level measurements was done with a paired box - plot diagram by spss . 
bar plots derived from prism 6 ( graphpad software inc . , san diego , usa ) illustrated snr and cnr values , as well as the ratings of image quality , artifacts , identification of anatomic structures and diagnostic confidence . wilcoxon rank tests detected differences between the various raters evaluations and their level of agreement was derived from spearman correlations with significance lev0.05. 
 the chart compares the acoustic noise in dbc - mode ( technical ) and dba - mode ( acoustic equivalent ) of the investigated quiet and non - quiet sequences . 
 the boxes comprise two quartiles , the whiskers embrace 95% of all values radiol med ( 2017 ) 122 : 194203 the t2 weighted tse and haste sequences show significant lower dba and dbc noise levels than the corresponding non - quiet sequences . 
thus , the decreased sound level lm by 5.2 of the quiet t2 tse sequence results in a noise reduction by 30.7% ; the reduction by 3.7 dba within the quiet t2 haste sequence equals a noise reduction by 22.6%. 
the sideby - side image comparison between the quiet and standard sequences revealed similar results regarding the raters image preference : despite broad standard deviations ( mean 0.76 ) , the standard t1 flash sequences were strongly preferred against the new quiet sequences ( 62.5% ) by both raters . 
comparison of standard and quiet sequences regarding image quality ( a ) , image artifacts ( b ) , the identification of anatomic structures ( c ) and diagnostic confidence ( d )  . 
this suggests that an objective measurement of solely the dba and dbc noise levels gives an idea of the noise , but does not fully cover the patients acoustic perception . 
the only slight reduction of acoustic noise in the t1 dixon sequence is caused by its strict conditions for the echo times , as inand opposed phase echoes need to be maintained . 
to achieve more significant acoustic noise reductions , either a decreased resolution or increased echo times to the next inor opposed phases would be needed . due to the fast timing in the t1 flash sequences fast and strong gradients are needed , resulting in a very high acoustic noise . 
in our quiet protocol , we increased the read - out bandwidth which results in a keep section during the read - out , but therefore longer change sections around the read - out . 
in our study , the sound level meter was positioned in front of the bore , facing the isocenter in a distance of 3 the obtained sound measurement might not be capable to exactly represent the acoustic impressions inside the bore but form a compromise to avoid a potential magneto - electric influence . 
 this implicates an absence of significant magneto - electric influence on the sound level meter , although later it cannot completely be ruled out during the rapid changes of the magnetic field during the image acquisition . 
although the standard and quiet sound measurements were each gathered from the same patient in the same session there was a strikingly greater acoustic variance of the quiet examinations observed . 
as no obvious difference in the variance between dba and dbc measurements could be observed it can be doubted that this effect results from a different frequency filtering by the torso of the almost similar sized and weighting persons or a differing sound conduction by the residual air between patient and scanner gantry . regarding the image quality the more grain is present in the images the more difficult becomes the detection of pathologies . 
in the mri quality control manual of the american college of radiology a snr measurement method in a single image slice is suggested [ 15 ] , which is commonly used by clinical physicists , because of its quick and easy way of measurement . 
but since the noise , which is obtained from the standard deviation of pixel intensities in the background of the image , varies spatially ( e.g. , due to artifacts ) and does not strictly follow distribution functions , snr values obtained from regions of low signal in single images are regarded as inaccurate [ 16 ]  . 
a better representation of image noise is achieved by the nema method 1 , which uses a subtraction image generated from two different acquisitions with the same imaging parameters [ 16 , 17 ]  . 
as the easier snr acquisition method of our study features a good correlation to nema 1 , it is still regarded as appropriate for the use in quality assurance [ 18 ]  . 
the simple method of snr calculation is still severely limited in parallel imaging due a spatially variant noise characterized by the g - factor , the radiofrequency , the coil array and applied filtering processes . 
monte carlo calculations have been proposed to circumvent these limitations involving a noise - only pre - scan and the calculation of the g - factor with the help of noise and snr maps [ 19 ]  . 
these differences are suspected to be dependent on the 3 months delay between the scans , i.e. , because of a different positioning of the flexible abdominal coils or depth of breathhold affecting signal intensities . as implied above high snr and cnr values are only a hint for good image quality but cannot represent all valuable image characteristics ( i.e. , the presence of artifacts or delineation of organs )  . 
hence in our study the t1 flash and t2 tse sequences , which were impaired most by artifacts , received worse subjective ratings in image qualityalthough no significant difference was observed between both groups . 
despite several significant differences in snr and cnr between quiet and standard t2 haste and t1 dixon sequences the subjective ratings offered no significant differences , which leads to the conclusion that the signal measurements might not fully represent the image quality and diagnostic value . 
furthermore , in our sideby - side comparison a more crisp appearance of structural edges was noticed in the quiet t1 flash images by both 1 3 202 radiol med ( 2017 ) 122 : 194203 raters . 
this finding is neither represented by snr or cnr calculations as the roi measurements were not placed on the border region of structural edges but in an homogeneous , hence reproducible region of the liver or muscle . 
but as t1 flash images suffered from severe artifacts this finding should be handled with care and further analysis of the signal distribution around structural edges might be needed for verification . 
noteworthy is a slightly impaired inter - rater correlation for the identification of anatomic and pathologic structures ( k 0.771 ) , which might be attributed to the different level of mr - experience ( 3 versus 12 years )  . 
second , since the images were acquired in clinical routine there was a mean delay of 3 months between the acquisition of first the standard and second the quiet sequences , which can affect the detection rate of pathologies and organ delineation under treatment . 
third , it would have been preferable to solely use one type of contrast agent , although both contrastagents used in our scans were non - hepatobiliary agents . conclusion in conclusion a distinct acoustic noise reduction was achieved with the new quiet mri sequences in a standard abdominal mri protocol for daily routine , which is of special interest for examinations of patients who are susceptible or easily intimidated by loud sounds , i.e. , patients of young or old age or patients with cognitive disorders . although sequence - based noise optimizations faces problems in t1 flash and dixon sequences , there is an important acoustic benefit in t2 tse and t2 haste sequences , which goes along with a maintained image quality and diagnostic confidence . acknowledgements david grodzki is employed by siemens healthcare and provided the prototype mr sequences . 
this work received no funding or financial support . compliances with ethical standards ethical standards the study was performed in accordance with the ethical standards of the institutional review board and with the 1964 helsinki declaration and its later amendments . 
however , the use of sophisticated tools is limited by the high costs and , in some cases , by the utilization of ionizing radiation , which have both great impact on the economy of a nation and on citizens health , respectively . 
guidelines have been published among countries to provide physicians with structured rules to be followed to suggest the correct imaging technique , suiting better the diagnostic question and avoiding inappropriate imaging requests . 
the collaboradi is a research project that addressed the phenomenon of inappropriate imaging prescriptions in sicily ( italy ) and proposed the design * maria adele marino mariaadele.marino@gmail.com 1 department of electrical , electronic and computer engineering , university of catania , catania , italy 2 department of radiological sciences , san vincenzo hospital - taormina , messina , italy 3 department of biomedical sciences and morphologic and functional imaging , policlinico universitario g.martino , university of messina , via consolare valeria , localit gazzi , 98124 messina , me , italy 4 radiology department , regina elena national cancer institute , rome , italy 5 department of radiological sciences , umberto i hospital , 6 department of radiological sciences , belcolle hospital , syracuse , italy viterbo , italy 7 department of diagnostic radiological sciences and interventional radiology , molecular imaging and radiotherapy , university hospital tor vergata , rome , italy and implementation of a clinical decision support system to help physicians to set up the most appropriate diagnostic route for their patients . 
the aim of this paper is to describe the characteristics of the collaboradi software and its potential impact in diminishing inappropriate imaging . keywords clinical guidelines diagnostic imaging rule - based system support decision system introduction there are widespread concerns that the costs of health care all over the world are rising at unsustainable rates . 
one of the major reasons of the rising costs is the increasing use of radiology imaging procedures , particularly advanced imaging techniques such as computed tomography ( ct ) scans and magnetic resonance imaging ( mri )  . most authorities agree that cutting down on inappropriate use of diagnostic procedures could improve quality , save costs and protect patients from undue risks and inconveniences . 
 in 2004 , the italian national agency for regional health services introduced guidelines for diagnostic imaging in congruence to the guidelines applied by other member states of the european union and canada , focusing attention on three key issues : investigation appropriateness , radiation protection and expenditure containment . 
however , guidelines are not always straightforward and easy to follow ; therefore , incorporation of appropriateness criteria into clinical practice is low , mainly reflecting the lack of formal training [ 5 , 6 ]  . 1 3 187 dose radiol med ( 2017 ) 122 : 186193 table 1 dirgs for salivary obstruction ( b ) neck ( for cervical spine see section c [ spine ] ) clinical problem investigation recommendation comment us sialogram indicated ( c ) salivary obstruction xr not indicated routinely except in calculus in floor of mouth , where xr may be all that is required the high percentage of radiological examinations , not meeting appropriateness criteria , suggests a need for decision support to help primary care physicians improve the management of patients , by choosing the correct diagnostic imaging procedure , which is most appropriate [ 7 ]  . collaboradi is an italian eu - funded research project coding the italian diagnostic imaging ( di ) guidelines into evidence - based rules . 
it is a clinical decision support for general practitioners ( gp ) providing a method for incorporation of the italian di guidelines into computerized ordering and electronic health record systems . 
furthermore , the software may be easily implemented according to the further modifications of such guidelines , which may evolve eventually according to technological advances . the paper aims to preliminarily illustrate collaboradi , an electronic software coding data for the diagnostic imaging referral guidelines ( dirgs )  . 
to the best of our knowledge , collaboradi is the first decision support introduced in italy and , in our opinion , it could be a useful example for the management of other health - care systems . national and international guidelines for clinical imaging : an overview in the past 20 years , many efforts have been made to promote the adoption of national and international guidelines for clinical imaging , principally to support the gp in selecting and justifying radiological procedures . 
furthermore , clinical decision support systems ( cdss ) [ 10 ] have been implemented to give real - time feedback to providers ordering imaging tests , including information on test appropriateness for specific indications . 
the italian dirgs are the results of the initiative sponsored by the italian national agency for regional healthcare ( agenas ) , aimed to establish appropriate guidelines for all health professionals entitled to refer patients for imaging [ 11 ]  . 
the authors focused their attention on three main aspects : ( a ) examination appropriateness , ( b ) radiological protection and ( c ) reduction of public spending . the dirgs comprises 13 sections , listed as follows : ( a ) head ; ( b ) neck ; ( c ) spine ; ( d ) musculoskeletal system ; ( e ) cardiovascular system ; ( f ) thoracic system ; ( g ) gastrointestinal system ; ( h ) urological , adrenal and genitourinary systems ; ( i ) obstetrics and gynecology ; ( j ) breast disease ; ( k ) trauma ; ( l ) cancer ; ( m ) pediatrics . 
table 1 shows a guideline sample from the dirgs . the recommendations are designated as follows : ( a ) the investigation most likely contributing to clinical diagnosis and management ; ( b ) specialized investigation ( frequently complex , time - consuming or resource - intensive investigations , usually only requested by medical doctors who have the relevant clinical expertise to evaluate the clinical findings and act on the imaging results ) ; ( c ) not indicated initially ( includes situations where experience shows that the clinical problem usually resolves with time , and where deferring the study is suggested ) ; ( d ) not indicated routinely ( non - routine studies to be carried out if a physician provides cogent reasons or if the radiologist feels the examination represents an appropriate way of furthering the diagnosis and management of the patient ) ; ( e ) not indicated ( examinations that will usually not contribute to the management of the patient )  . 
the estimate of the total risk of stochastic effects ( cancer , leukemia , hereditary effects ) resulting from exposure to radiation is performed using the effective dose , which is measured in sievert ( sv )  . 
table 2 shows the typical effective doses of ionizing radiation from common imaging procedures . collaboradi : design and implementation the approach followed by the collaboradi systems designers was to build a software decision support system that , by leveraging on dirg guidelines coded as rules , could be used by the general practitioners ( gp ) to get advices on the most appropriate di examination to prescribe in response to specific clinical questions . 
 the final decision is of course left to the gp . the collaboradi project focuses on the design and implementation of : a data structure to model the main concepts of the dirgs ; a set of formal rules to capture and fig . 
1 the dirg data model in the er form 1 3 radiol med ( 2017 ) 122 : 186193 model the guidelines contained in the dirgs ; a web application that leverages on the implemented rules to guide physicians in the di prescription . 
clinical problem / phase pairs allow every possible investigation , along with their recommendation , grade of evidence , effective dose and time priority [ 1214 ]  . all of the above information is , respectively , represented by investigation , recommendation , gradeofevidence , effectivedose and priority entities . 
the criteria are therefore represented by ( a ) phase : characterized by the name attribute , which specifies the clinical problems stadium of interest ; ( b ) age , characterized by the minimumage and maximumage attributes ; ( c ) timebetweenexams , characterized by the timeperiod attribute , which describes the minimum time interval to be followed before the patient can undergo the same examination ; ( d ) persistentsymptoms , characterized by the timeperiod attribute , which specifies how long the symptoms have been persisting ; ( e ) unavailableexam , characterized by the name attribute that identifies the non - locally available examination . although there are many different techniques for organizing collections of rules into automated experts , the drools [ 15 ] software was chosen . 
they are just ifthen statements where the antecedent ( if clause ) is a combination of criteria - based conditions and the consequent ( then clause ) is the action related to the investigation selection . 
as reported in the dirg guidelines for thyroid nodules and enlargement , the set of all useful examinations is composed of color doppler us , us - guided fine needle aspiration cytology ( us - fnac ) and scintigraphy . 
the second rule establishes that a deferrable waiting time color doppler us is to be considered when either a thyroid inflammation or a thyroid dysfunction or a goiter is suspected . 
figure 3 illustrates the high - level collaboradi application architecture , which is based on the well - known modelviewcontroller ( mvc ) software design pattern [ 16 ] , to separate internal representations of information from the ways that information is presented to the user . 
3 high level collaboradi architecture diagram radiol med ( 2017 ) 122 : 186193 presentation of the application , ( i.e. , all the elements in the user interface such as buttons , display boxes and so forth ) , whereas the model represents the underlying , logical structure of data and operations ( business logic ) and does not contain any information about the user interface . 
the controller is the component responsible for intercepting and translating user input into actions to be performed by the business logic , which in its turn implements the core operations of the applications . 
3 , the business logic is responsible for interpreting the request coming from the client browser , creating or updating the model , and coordinating the view to be delivered back to the browser . 
4 search clinical problem view with criteria sequence diagram 1 3 radiol med ( 2017 ) 122 : 186193 represents the whole set of criteria - driven rules defined for all the clinical problems , which the dirgs cover . fields on criteria : equivocalexam , persistentsymptoms and suspectedpathology . the collaboradi system in action physicians log on the system through an authentication process based on the username and password . 
4. the interface allows searching the available investigations for a particular clinical problem , whose selection is facilitated by the auto - complete feature that filters all possible matches according to the specified phase . 
by pressing the search investigations button , physicians will be asked to specify one or more criteria , in relation to which an examination will be privileged among the available ones . 
 figure 5 shows the interface presented to physicians in case of a sinus disease , for which they are required to fill in the the persistentsymptoms field is mandatory and must be manually entered as a numerical value ( in days ) , while the other ones can be selected directly from a dropdown list . 
when physicians press the submit criteria button , the system acquires the criteria , interacts with the rule engine and finally returns an investigation list sorted by medical appropriateness in a descending order . 
figure 6 shows the final view for sinus disease resulting from the criteria set out above . 14 , suspectedpathology each investigation includes the information mentioned ( i.e. , explanatory comment , priority , waiting time , recommendation , grade of evidence , effective dose , use of contrast medium )  . 
by doing that , collaboradi analyses the phenomenon of inappropriate di prescriptions and suggests a way to tackle it . collaboradi is now a trial software approved by the ethics committee . 
therefore , pretreatment accurate assessment of extracapsular extension ( ece ) in prostate cancer is essential for selecting an optimal therapy such as radical prostatectomy , radiotherapy , and non - curative systemic therapies [ 2 ]  . 
in other words , accurate assessment of ece improves the accuracy in selecting appropriate patients for active surveillance among those with and without clinically significant cancers and contributes to avoid overand undertreatment [ 3 ]  . transrectal ultrasonography ( trus ) and digital rectal examination ( dre ) which are the conventional techniques for clinical staging are not sufficient in sensitivity and specificity for the detection of ece in prostate cancer [ 46 ]  . 
particularly , dre has been shown to be a poor predictor of tumor location and extent [ 7 ] , and the accuracy for local staging by dre is lower than that by trus [ 8 ]  . 
 furthermore , it has been reported that magnetic resonance imaging ( mri ) using t2 - weighted imaging ( t2wi ) as well as biopsy gleason score ( gs ) are powerful predictors of ece among prostate - specific antigen ( psa ) , psa density , mri using t2wi , trus , and systematic prostate biopsy [ 9 ]  . 1 3 radiol med ( 2017 ) 122 : 228238 thus , prostate mri using t2wi is considered as a useful imaging modality for pretreatment clinical staging of prostate cancer . 
actually , in usual clinical practice , we often experience difficulty in diagnosing ece in patients of pt3 stage without specific mr findings of ece such as obliteration of the rectoprostatic angle and periprostatic fat [ 10 , 2830 ]  . 
 this may be due to the inability to visualize microscopic ece on mri and the increase of small organ - confined prostate cancer in psa era [ 28 , 31 , 32 ]  . on the other hand , although gs is an indicator of tumor aggressiveness , gs obtained by biopsy is underestimated in 2954% as compared with gs obtained by radical prostatectomy , i.e. , the accurate tumor aggressiveness [ 33 ]  . 
previous reports have shown that diffusion - weighted imaging ( dwi ) including apparent diffusion coefficient ( adc ) is useful for not only tumor detection but also assessment of tumor aggressiveness of prostate cancer [ 34 , 35 ]  . 
furthermore , a recent study has reported that the correlation between these variables tended to be stronger when using a 3 - t system than a 1.5 - t system and when using a higher b value such as 0 and 2000 s / mm2 than standard b values such as 0 and 1000 s / mm2 [ 38 ]  . until now , six prospective or retrospective studies have been reported on the added value of dwi with adc for the detection of ece [ 2527 , 3941 ]  . 
however , no studies have been reported with dwi using adc obtained with high b value ( 2000 s / mm2 ) at 3 - t focusing on the detection of the ece in prostate cancer . 
therefore , the goal of this study was to investigate whether high b value dwi at 3 - t contributes to the improvement of diagnostic ability of ece in prostate cancer . materials and methods patient characteristics this retrospective study was approved by our institutional review board , and the requirement for obtaining informed consent from patients was waived . a total of 47 consecutive patients with biopsy - proved prostate cancer underwent mr imaging of the prostate with a 3 - t system between april 2012 and june 2014 at our institution . 
dwi was acquired with motion - probing gradient ( mpg ) pulses applied sequentially along three orthogonal orientations following acquisition at b values of 0 and 2000 s / mm2 . 
adc maps were reconstructed by calculating adc in each pixel of each slice , and the adc values were calculated for a pair of b values : 0 and 2000 s / mm2 . 
data acquisition for dce - mri began simultaneously with initiation of intravenous injection of meglumine gadoterate ( magnescope ; guerbet japan , tokyo , japan ) or gadopentetate dimeglumine ( magnevist ; bayer schering pharma , osaka , japan ) of 0.1 mmol / kg body weight at a rate of 3 ml / s via a power injector , followed by a 40 - ml saline flush at the same rate of contrast media injection . 
multiphase dce - mr images were obtained every 30 s for 3 min ( six phases ) without breath - holding . histopathologic analysis in all 43 patients , the reference standard for tumor localization and ece of prostate cancer was determined using the step - section histologic slices from radical prostatectomy . 
the distal portion of the apex and the proximal portion of base were amputated and were sliced sagittally to assess the resection marg all slices were processed uniformly and submitted entirely . 
after routine hematoxylin - eosin staining , an experienced uropathologist who was blinded to the mri findings evaluated all pathologic specimens and marked tumors and location of ece on the photographs for each slice . 
the pathologist further recorded the tumor location , the presence and location of ece , the tumor gs , the presence of surgical margin , the presence of lymph node metastasis , the presence of distant metastasis , and final pathological stage in the pathological report . 
each tumor was evaluated according to the 2005 international society of urological pathology modified gleason grading system [ 43 ]  . clinical and histopathologic data collection as clinical and histopathologic data , the initial psa level and biopsy gs were collected from the medical and pathological records by a study coordinator . image interpretation and data analysis mr images evaluation was performed using a pacs viewer ( rapideye core ; toshiba medical systems )  . 
two radiologists with 2 and 16 years of experience in prostate mr imaging were reviewed mr images in consensus , and they were aware that patients had prostate cancer but were blinded to other clinical and histopathologic findings . at first , the prostate mr images were reviewed to identify the presence or absence of ece using conventional diagnostic method with t2wi and dcm - mri and recorded the diagnostic certainty degree for mr finding of ece using a four - point scale ( grade 1 , reliable ; 2 , probably reliable ; 3 , questionable ; and 4 , impossible ) ( conventional mri method )  . 
diagnosis of ece on t2wi and dce - mri was based on at least one of the following criteria : interruption of the capsule , broad tumor contact ( > 10 mm ) , obliteration of periprostatic fat , obliteration of the rectoprostatic angle , asymmetric or direct involvement of the neurovascular bundle , angulated prostate gland contour , irregular or spiculated margin on t2wi , and seminal vesicle lesion with both low signal intensity on t2wi and enhancement effect on dce - mri [ 10 , 2830 ]  . after the evaluation of ece , the prostate mr images were further reviewed to identify cancer foci that were subsequently targeted for the image analysis of ece in consensus by the same two radiologists . 
cancer foci were selected if they showed positive finding with 5 mm or more on at least one of the three mr imaging sequences , including t2wi , dwi , and dce - mri . 
a tumor site was considered to match histological findings if the tumor depicted on the image was present in the same region of the prostate indicated in the prostatectomy specimen . 
that is , the final diagnosis of ece in patients with high diagnostic certainty was determined only by conventional mri method , whereas the patients with low diagnostic certainty was considered ece negative when tumor adc value is higher than the adc cutoff value and ece positive when tumor adc value is lower than the adc cutoff value , regardless of the diagnosis of ece by conventional mri method . 
among these 15 patients with pt3a disease , 12 patients ( 80% ) had only microscopic ece less than 1 m the remaining 25 of 43 patients ( 58% ) was organ - confined disease . 
in 43 patients who underwent radical prostatectomy , a total of 43 prostate cancer lesions ( matching the histopathologic findings ) with lowest adc value in each patient were selected . 
other histopathlogical characteristics in 43 patients with prostate cancer are shown in table 2 . evaluation of ece using conventional mri method by conventional mri method , 33 of 43 patients ( 77% ) were diagnosed as ece negative ( t2a in 18 , t2b in one , and t2c in 14 patients ) and the remaining 10 patients ( 23% ) as ece positive ( t3a in 8 and t3b in 2 )  . 
the diagnostic certainty degree for the mri findings of ece were grade 1 in 16 patients ( ece negative in 14 and ece positive in 2 ) , grade 2 in 12 patients ( ece negative in 9 and ece positive in 3 ) , grade 3 in 14 patients ( ece negative in 9 and ece positive in 5 ) , and grade 4 in one patient ( ece negative in 1 )  . 
 accordingly , the tumor adc was shown to be an independent predictor of ece in prostate cancer . comparison of detection ability of ece between conventional mri method and mri method adc 10 in terms of discrimination between ece positive group and ece negative group using adc values , a cutoff value of 3 / mm2 / s resulted in a sensitivity of 83% and a 0.72 specificity of 68% , showing that the sum of sensitivity and specificity is maximized . 
the diagnosis of ece after using adc cutoff value in 11 patients with broad tumor contact was unchanged in 4 patients , changed to correct diagnosis in 6 patients , and changed to incorrect diagnosis in one patient . 
that is , the median psa level of our subjects was 7.57 ng / ml , 60% of patients ( 26 / 43 patients ) were gray - zone psa level ( 410 ng / ml ) , and 80% of patients were microscopic ece less than 1 mrecent studies have reported that in psa screening era non - organ - confined prostate cancer with microscopic ece has increased , and patients with pt3 in psa screening era had a better prognosis compared with pre - psa screening era [ 31 , 32 ]  . 
accordingly , the study for patients with low detection sensitivity of ece on conventional mri is clinically challenging , and new techniques to improve the detection ability of ece is expected for an appropriate management in patients with prostate cancer in psa screening era . in multivariable logistic regression analyses using of psa , histopathologic , and mri findings , tumor adc was an independent predictor for discriminating presence or absence of ece in prostate cancer in all 43 patients in conventional mri method . 
recent studies also reported that tumor adc including not only mean value which was used in this study but also median ; 10th centile and 20th centile values were associated with the presence of ece in patients with prostate cancer [ 25 , 26 , 39 , 40 ]  . 
accordingly , a further large - scale multi - center study will be required for determining the adc value with highest discrimination ability of ece among these indices which were obtained using novel techniques such the adc 1 3 234 radiol med ( 2017 ) 122 : 228238 fig . 
1 a 64 - year - old male with prostate cancer ( psa level of 7.54 ng / ml , prostatectomy gleason score of 4 3 , pathological stage t3a ) in the middle right region in the peripheral zone . 
cancer lesion is shown as a homogeneous hypointense area with mass effect on t2 - weighted imaging ( arrow ) ( a ) , a focal hyperintensity on diffusion - weighted imaging with b values of 0 and 2000 s / mm2 ( arrow ) ( b ) , and a focal hypointensity on apparent diffusion coefficient ( adc ) map ( arrow ) ( c )  . 
readers diagnosed as t3a disease with low diagnostic certainty ( grade 3 ( questionable ) ) for mr findings of broad tumor contact suspecting extracapsular extension ( ece ) on t2 - weighted image ( arrowheads ) ( a )  . 
the lesion with low diagadc value was 0.64 nostic certainty was reevaluated by adc cutoff value ( 0.72 mm2 / s ) , but the diagnosis of ece using conventional mri method was unchanged . 
photograph of a macroscopic specimen shows the cancer lesion ( red circles ) with ece ( red arrow ) ( d ) 10 10 histogram analysis [ 26 , 45 ]  . 
we expected that inclusion of adc cutoff value in the diagnostic process of ece for patients with low diagnostic certainty by conventional mri would result in further improvement of detection ability of ece in prostate cancer . 
accordingly , further multi - center studies on different multiparametric mri systems will be needed to strengthen these initial results for the clinical use of adc cutoff value to detect ece . 10 in conventional mri method alone , 15 of 43 patients ( 35% ) showed low diagnostic certainty for the detection of ece in prostate cancer including grade 3 in 14 patients and grade 4 in one patient , suggesting the difficulty for the diagnosis of ece in our study population . 
ninety - three percentage ( 14 / 15 patients ) among these patients with low diagnostic certainty were led to correct diagnosis of ece by reevaluation using the adc cutoff value ( table 3 )  . 
on the contrary , only one patient turned into incorrect diagnosis using the adc cutoff value . in comparison of detection ability of ece between conventional mri method and mri and adc method , the all indices were substantially higher in mri and adc method than conventional mri method . 
2 a 71 - year - old male with prostate cancer ( psa level of 13.2 ng / ml , prostatectomy gleason score of 4 3 , pathological stage t2a ) in the middle right region in the peripheral zone . 
cancer lesion is shown as a homogeneous hypointense area with mass effect on t2 - weighted imaging ( arrow ) ( a ) , a focal slight hyperintensity on diffusion - weighted imaging ( arrow ) ( b ) , a focal slight hypointensity on apparent diffusion coefficient ( adc ) map ( arrow ) ( c ) , and a slight early enhancement on dynamic contrast - enhanced mr imaging ( dce - mri ) ( arrow ) ( d )  . 
readers diagnosed as t3a disease with low diagnostic certainty ( grade 3 ( questionable ) ) for mr findings of broad tumor contact and irregular margin suspecting extracapsular extension ( ece ) on t2 - weighted image ( arrowheads ) ( a )  . 
and high b value dwi such as a present study will be also necessary . unexpectedly , the detection sensitivity of ece in patients with high diagnostic certainty using conventional mri method was relatively low ( 56% ) against extremely high specificity ( 100% )  . 
further measures for improving the detection sensitivity of ece in patients with high diagnostic certainty for conventional mri findings of ece will be necessary . finally , 72% ( 11 / 15 patients ) of patients with low diagnostic certainty for the detection of ece in prostate cancer were judged based on the criteria of broad tumor contact in t2wi . 
this result is consistent with the statement in esur prostate mr guidelines 2012 , in which broad tumor contact , i.e. , abutment is classified as a low suspicious mr finding ( score 1 ) for the diagnosis of ece [ 46 ]  . 
the addition of adc cutoff method , however , the overall accuracy for the prediction of ece resulted in an extremely high value of 91% ( 10 / 11 patients )  . 
the favorable result may be due to the strong relationship between tumor adc obtained with high b value dwi at 3t and tumor aggressiveness such as gs of 1 3 radiol med ( 2017 ) 122 : 228238 236 4 , pathofig . 
3 a 72 - year - old male with prostate cancer ( psa level of 20.96 ng / ml , prostatectomy gleason score of 3 logical stage t2c ) in the middle right region in the peripheral zone . 
cancer lesion is shown as a homogeneous hypointense area with mass effect on t2 - weighted imaging ( arrow ) ( a ) , a focal hyperintensity on diffusion - weighted imaging ( arrow ) ( b ) , a focal hypointensity on apparent diffusion coefficient ( adc ) map ( arrow ) ( c ) , and an early enhancement on dynamic contrast - enhanced mr imaging ( dce - mri ) ( arrow ) ( d )  . 
readers diagnosed as t2 disease with low diagnostic certainty ( grade 3 ( questionable ) ) for mr findings of broad tumor contact but clear prostatic capsule on t2 - weighted image ( arrowheads ) ( a )  . 
the green circles show high - grade prostatic intraepithelial neoplasia ( pin ) 10 prostate cancer that is used with nomogram to predict ece [ 38 , 47 ]  . our study had several limitations . 
further prospective investigations with larger patient populations are needed to support our results using adc cutoff method obtained at high b value dwi at 3t for the assessment of ece in prostate cancer . 
however , a previous study reported that 3 - t phased - array mri might be equivalent to 1.5 - t endorectal mri in the evaluation of local staging accuracy of prostate cancer without significant loss of image quality [ 23 ]  . 
fourth , when using adc to detect ece in prostate cancer , the adc value may be different under the influence of mr scanner type , magnetic field strength , and b values . 
other functional mr techniques such as qualitative visual assessment using dw image and adc map [ 2527 ] , and mr spectroscopic imaging may correct misdiagnosis of ece using the adc cutoff value and may contribute for further improvement of detection ability of ece in prostate cancer . in conclusion , the addition of adc cutoff value obtained with high b value ( 0 , 2000 s / mm2 ) dwi at 3 - t to patients 1 3 radiol med ( 2017 ) 122 : 228238 with low diagnostic certainty in the assessment of ece using conventional mri method improved the diagnostic ability of ece of prostate cancer . 
vogl1 stephan zangos4 received : 7 june 2016 / accepted : 14 november 2016 / published online : 28 november 2016 italian society of medical radiology 2016 abstract objective purpose of our study was to demonstrate the feasibility and limitations of acoustic noise reduction in a standard clinical mri protocol for abdominal imaging . methods acoustic noise and image quality were assessed in 17 patients for a standard liver imaging protocol including tse and gre sequences and compared to quiet optimizations as described by heismann et al . 
 during the last years diffusion - weighted imaging ( dwi ) has been increasingly used for the detection and characterization of liver tumors [ 2 ]  . despite the known benefits of mr - imaging , some patients reject an mri examination . 
the most prominent reason for the noise is caused by mechanical vibrations of the gradient coil during rapid switching of the gradients , which intimidate patients who are either physically susceptible to the damaging effects of loud noises like patients of young or old age or patients with cognitive disorders . 
food and drug administration regarding mr - related acoustic noise levels state than an unweigthed peak sound pressure level of 140 db and an a - weighted sound pressure level greater than 99 dba with hearing protection in place should not be exceeded [ 3 ]  . 
the widely used decibel a filter roughly corresponds to the inverse of the 40 db curve with equalloudness for the human hearing at 1 khzalthough it is no physiological parameter . 
reported mr imaging - related sound levels to vary from 84 to 103 db on the linear scale and 8293 db on the a - weighted scale [ 6 ]  . 
studies including pulse sequences with multiple gradients applied simultaneously like three - dimensional , fast gradient echo techniques were reported to have the loudest peak acoustic noise ranging up to 113 dba [ 5 ]  . 
especially sequences with very fast gradient switching and high amplitudes like echo planar imaging suffer from high levels of noise , exemplarily described with 114115 dba for a 1.5 t scanner system by shellock et al . 
for systems with 3 tesla even higher sound levels can be found [ 7 ]  . during the last decades different hardware - based or sequence - based approaches were tested to minimize acoustic mri noise . 
the least expensive way of noise attenuation consists of using earplugs or headphones , which on the one hand decreases acoustic noise by 1030 db , but on the other hand provides a non - uniform noise attenuationusually with poor attenuation results for the typically low mr - imaging related noise frequencies . 
by applying a gradient smoothing algorithm to the standard gradient course the gradient ramps are softened in the modified quiet sequences cancellation has been accomplished in the late eighties using an interference with generated antiphase noise [ 8 ]  . during the last years quiet pulse sequences have been developed , which can even be used with echo planar imaging [ 911 ]  . 
in this approach , an automated gradient smoothing algorithm is applied that subdivides any given pulse sequences into change segments where gradients may be optimized and keep segments in which gradients must remain unchanged , like during excitation and data acquisition . 
in change intervals a spline interpolation is used that keeps the m0 and if needed the m1 moment , which are characterized by the following formulas : m0 = g ( t ) dt m1 = tg ( t ) dt ( cid : 31 ) t1 ( cid : 31 ) t1 with g ( t ) representing the temporal gradient course and t1 and t2 as start and end points of the change interval . 
standard deviations were given for tr and te as parameters featured slight variations among examinations protocol and a protocol with the modified quiet pulse sequences ( table 1 ) , which are commercially available as the siemens quiet suite . 
the quiet sequences feature unchanged intervals comprising radiofrequency pulse and read - out activity , but changed settings in intervals with gradient activity by application of a fourth - order spline interpolation to reduce slew - rates as described by heismann et al . 
except from changed gradient activity imaging parameters were not subject to change . examinations were carried out after informed consent on a 3 t scanner in clinical route with a standard 32 - channel body coil ( magnetom prismafit , siemens healthcare , erlangen , germany ) and a delay of 3 months between the standard protocol and following the quiet protocol . 
 the non - hepatobiliary contrast the administration of agent given per quantity of body weight contained either dotarem ( 0.05 mg / kg ) or gadovist ( 0.01 mg / kg ) and was performed by a standard injector ( accutron mr , medtron ag , saarbrcken , germany ) with a flow of 2 ml / s . the study was performed in accordance with the ethical standards of the institutional review board and with the 1964 helsinki declaration and its later amendments . 
a sound level meter ( sl - 100 , voltcraft , germany ) was placed in front of the bore , facing the isocenter in a distance of 3 the sound level meter was set to two frequency evaluation modes : a mode accounting for the characteristic hearing curve perceived by the human ear ( dba ) and a technical mode receiving a linear frequency curve ( dbc )  . 
during the acquisition of each mri sequence the sound pressure level l was recorded once per second for 125 ms in dbaand dbc - mode over 10 s and an average sound level lm was calculated using the equation : lm = 10 log ( cid : 31 ) ( cid : 30 ) 10li / 10 ( cid : 29 ) with li being the ith recorded value per measurement out of n data values [ 14 ]  . 
in addition to these objective results subjective impressions of the patients have been recorded and evaluated . the loudness ratio z of the quiet and standard sequences was determined from the perceived change in sound pressure level lm by taking the logarithmic character of the unit decibel ( db ) into account : z = 2 ( cid : 31 ) lm lm standard lm quiet in a subjective questionnaire the test persons named the sequence they preferred and had the chance to note differences in their personal acoustic perception . 
the psychoacoustic loudness ratio was calculated for each set of sequences image evaluation cnr = ( siliver simuscle ) /  . the evaluation and comparison of the mr images was performed retrospectively on a standard pacs workstation ( ge healthcare , il , usa ) by two independent blinded radiologists with a different level of experience ( 3 / 12 years ) in abdominal imaging . subjective overall image quality , the delineation of the abdominal organs and the level of confidence in visualization of the anatomy and pathologies was assessed using a 5 - point scale ( 1 : very poor , 2 : poor , 3 : fair , 4 : good , 5 : excellent )  . 
therefore , each of the following anatomic structures were rated : liver parenchyma , liver arteries and veins , portal vein , hepatobiliary duct , gallbladder , pancreas , pancreatic duct , kidneys , adrenal glands , spleen and lymphatic nodes . 
 the evaluation included a general evaluation of artifacts due to cardiac motion , respiratory motion or bowel movement , scored on a 3 - point scale ( 0 : no visible artifact , 1 : minimal artifact that did not interfere with diagnostic quality ; 2 : severe artifact that interfered with diagnostic quality )  . signal intensities ( si ) , signal - to - noise ratio ( snr ) and contrast - to - noise ratio ( cnr ) were measured and calculated for the liver and muscle in each native sequence ( t2 haste , t2 tse , t1 dixon ) and in contrast - enhanced sequences ( t1 flash , t1 dixon )  . 
a circular region of interest ( roi ) with a diameter of 1 cm was placed inside a region free of artifacts and nutritive vessels inside the liver parenchyma and the musculus latissimus dorsi , respectively . 
its location and diameter was visually matched to the corresponding other sequences to achieve optimal intra and inter - individual comparability . snr was calculated out of the mean pixel intensity value of the roi as the si and from the standard deviation ( ) in pixel intensity of the background air as noise according to the method used by the american college of radiology ( acr ) [ 15 ]  . 
for calculation the following equation was used : snr = si /  . the cnr was calculated by the difference of the si in liver parenchyma and muscles , divided by the background noise according to the equation : furthermore both radiologists undertook a randomized , blinded side - by - side comparison of the standard and quiet sequences , rating them as inferior ( 1 ) , comparable ( 0 ) or superior ( 1 ) regarding subjective image quality . statistical analysis statistical analysis was performed using an explorative data analysis . 
the descriptive statistics included the mean , standard deviation , minimum and maximum values . the means of the sound level measurements , the snr and cnr were compared in a paired two - sided t test using holm - sidak method with a significance level set at 0.05. visualization of the sound level measurements was done with a paired box - plot diagram by spss . 
bar plots derived from prism 6 ( graphpad software inc . , san diego , usa ) illustrated snr and cnr values , as well as the ratings of image quality , artifacts , identification of anatomic structures and diagnostic confidence . wilcoxon rank tests detected differences between the various raters evaluations and their level of agreement was derived from spearman correlations with significance lev0.05. 
 the chart compares the acoustic noise in dbc - mode ( technical ) and dba - mode ( acoustic equivalent ) of the investigated quiet and non - quiet sequences . 
 the boxes comprise two quartiles , the whiskers embrace 95% of all values radiol med ( 2017 ) 122 : 194203 the t2 weighted tse and haste sequences show significant lower dba and dbc noise levels than the corresponding non - quiet sequences . 
thus , the decreased sound level lm by 5.2 of the quiet t2 tse sequence results in a noise reduction by 30.7% ; the reduction by 3.7 dba within the quiet t2 haste sequence equals a noise reduction by 22.6%. 
the sideby - side image comparison between the quiet and standard sequences revealed similar results regarding the raters image preference : despite broad standard deviations ( mean 0.76 ) , the standard t1 flash sequences were strongly preferred against the new quiet sequences ( 62.5% ) by both raters . 
comparison of standard and quiet sequences regarding image quality ( a ) , image artifacts ( b ) , the identification of anatomic structures ( c ) and diagnostic confidence ( d )  . 
this suggests that an objective measurement of solely the dba and dbc noise levels gives an idea of the noise , but does not fully cover the patients acoustic perception . 
the only slight reduction of acoustic noise in the t1 dixon sequence is caused by its strict conditions for the echo times , as inand opposed phase echoes need to be maintained . 
to achieve more significant acoustic noise reductions , either a decreased resolution or increased echo times to the next inor opposed phases would be needed . due to the fast timing in the t1 flash sequences fast and strong gradients are needed , resulting in a very high acoustic noise . 
in our quiet protocol , we increased the read - out bandwidth which results in a keep section during the read - out , but therefore longer change sections around the read - out . 
in our study , the sound level meter was positioned in front of the bore , facing the isocenter in a distance of 3 the obtained sound measurement might not be capable to exactly represent the acoustic impressions inside the bore but form a compromise to avoid a potential magneto - electric influence . 
 this implicates an absence of significant magneto - electric influence on the sound level meter , although later it cannot completely be ruled out during the rapid changes of the magnetic field during the image acquisition . 
although the standard and quiet sound measurements were each gathered from the same patient in the same session there was a strikingly greater acoustic variance of the quiet examinations observed . 
as no obvious difference in the variance between dba and dbc measurements could be observed it can be doubted that this effect results from a different frequency filtering by the torso of the almost similar sized and weighting persons or a differing sound conduction by the residual air between patient and scanner gantry . regarding the image quality the more grain is present in the images the more difficult becomes the detection of pathologies . 
in the mri quality control manual of the american college of radiology a snr measurement method in a single image slice is suggested [ 15 ] , which is commonly used by clinical physicists , because of its quick and easy way of measurement . 
but since the noise , which is obtained from the standard deviation of pixel intensities in the background of the image , varies spatially ( e.g. , due to artifacts ) and does not strictly follow distribution functions , snr values obtained from regions of low signal in single images are regarded as inaccurate [ 16 ]  . 
a better representation of image noise is achieved by the nema method 1 , which uses a subtraction image generated from two different acquisitions with the same imaging parameters [ 16 , 17 ]  . 
as the easier snr acquisition method of our study features a good correlation to nema 1 , it is still regarded as appropriate for the use in quality assurance [ 18 ]  . 
the simple method of snr calculation is still severely limited in parallel imaging due a spatially variant noise characterized by the g - factor , the radiofrequency , the coil array and applied filtering processes . 
monte carlo calculations have been proposed to circumvent these limitations involving a noise - only pre - scan and the calculation of the g - factor with the help of noise and snr maps [ 19 ]  . 
these differences are suspected to be dependent on the 3 months delay between the scans , i.e. , because of a different positioning of the flexible abdominal coils or depth of breathhold affecting signal intensities . as implied above high snr and cnr values are only a hint for good image quality but cannot represent all valuable image characteristics ( i.e. , the presence of artifacts or delineation of organs )  . 
hence in our study the t1 flash and t2 tse sequences , which were impaired most by artifacts , received worse subjective ratings in image qualityalthough no significant difference was observed between both groups . 
despite several significant differences in snr and cnr between quiet and standard t2 haste and t1 dixon sequences the subjective ratings offered no significant differences , which leads to the conclusion that the signal measurements might not fully represent the image quality and diagnostic value . 
furthermore , in our sideby - side comparison a more crisp appearance of structural edges was noticed in the quiet t1 flash images by both 1 3 202 radiol med ( 2017 ) 122 : 194203 raters . 
this finding is neither represented by snr or cnr calculations as the roi measurements were not placed on the border region of structural edges but in an homogeneous , hence reproducible region of the liver or muscle . 
but as t1 flash images suffered from severe artifacts this finding should be handled with care and further analysis of the signal distribution around structural edges might be needed for verification . 
noteworthy is a slightly impaired inter - rater correlation for the identification of anatomic and pathologic structures ( k 0.771 ) , which might be attributed to the different level of mr - experience ( 3 versus 12 years )  . 
second , since the images were acquired in clinical routine there was a mean delay of 3 months between the acquisition of first the standard and second the quiet sequences , which can affect the detection rate of pathologies and organ delineation under treatment . 
third , it would have been preferable to solely use one type of contrast agent , although both contrastagents used in our scans were non - hepatobiliary agents . conclusion in conclusion a distinct acoustic noise reduction was achieved with the new quiet mri sequences in a standard abdominal mri protocol for daily routine , which is of special interest for examinations of patients who are susceptible or easily intimidated by loud sounds , i.e. , patients of young or old age or patients with cognitive disorders . although sequence - based noise optimizations faces problems in t1 flash and dixon sequences , there is an important acoustic benefit in t2 tse and t2 haste sequences , which goes along with a maintained image quality and diagnostic confidence . acknowledgements david grodzki is employed by siemens healthcare and provided the prototype mr sequences . 
this work received no funding or financial support . compliances with ethical standards ethical standards the study was performed in accordance with the ethical standards of the institutional review board and with the 1964 helsinki declaration and its later amendments . 
two independent readers ( r1 , trained radiology resident ; r2 , lower - trained technician student ) obtained segmented images twice ( > 10day interval ) , using a semi - automated method of segmentation . 
r1 intra - reader reproducibility for the aorta was 99% ( peak velocity ) , 95% ( forward flow ) and 49% ( backward flow ) ; for the pulmonary artery , 99% , 91% and 90% , respectively . 
especially for patients affected with congenital heart disease , cmr plays an important role in 1 3 180 radiol med ( 2017 ) 122 : 179185 the quantification of blood flow and evaluation of valve stenosis / insufficiency using phase - contrast ( pc ) throughplane sequences [ 211 ]  . 
the pc sequences were validated in phantom and in vivo studies and have proven to be a reliable tool for the quantitative and qualitative analysis of blood flow and tissue motion [ 12 ]  . despite its importance for the assessment of disease progression , few data are available about the reproducibility of cmr in the measurement of blood flow in patients with valve stenosis and / or insufficiency [ 2 , 1315 ]  . 
moreover , segmentation methods were validated indirectly , through the ability to provide accurate flow measurement [ 13 , 16 ] or pulse wave velocity [ 16 , 17 ] or directly in terms of operator variability [ 13 , 14 ] or agreement with manual tracing [ 17 ]  . blood flow measurements are based on the segmentation of a vessel contour that may be performed manually or , more typically , semi - automatically , with the use of computer software likely impacting on measurement reproducibility . 
reader experience may play a role as well . thus , the aim of our study was to estimate the intraand inter - reader reproducibility of blood flow cmr measurements through the ascending aorta and main pulmonary artery in patients affected with congenital heart disease or with aortic and / or pulmonary valve disease . 
 time resolution 41 ms ; mean acquisition time 15 for each patient , we initially acquired the pc sequence with a venc of 150 cm / s : in the presence of aliasing , we increased the venc adding 50 cm / s for each new sequence , step - by - step up to the complete disappearance of the aliasing artifact . flow measurements were performed right above the aortic or pulmonary valve in patients with surgical or percutaneous valve replacement . 
the magnitude image depicts the anatomy and allows to identify the vessel boundaries , while the phase velocity map corresponds to blood velocity [ 2 ]  . two independent readers ( r1 and r2 ) performed measurements twice , with at least a 10 - day interval between the two sessions , for a total of four sessions . 
 blandaltman graphs were plotted as well , showing bias ( mean of the differences of the two compared datasets ) , and 95% limits of agreement ( bias cor )  . results of 50 analyzed patients , 46 ( 92% ) had a pulmonary disease , two ( 4% ) ventricular septal defect , one ( 2% ) aortic insufficiency , and one ( 2% ) truncus arteriosus . 
the time needed for measurement was about 5 min per patient , without substantial difference between the two readers . the mean blood peak velocity of the aortic flow measured by r1 was 103 cm / s , accompanied by a cor of 1 cm / s , corresponding to an intra - reader reproducibility of 99% ; the same data for r2 were 103 cm / s , 9 cm / s , and 92% . 
the mean blood peak velocity of the pulmonary flow measured by r1 was 180 cm / s , accompanied by a cor of 1 cm / s , 1 3 182 table 2 intra - reader reproducibility of the first reader radiol med ( 2017 ) 122 : 179185 pulmonary flow forward ( ml / beat ) backward ( ml / beat ) forward ( ml / beat ) backward ( ml / beat ) aortic flow peak velocity ( cm / s ) mean bias reproducibility the first reader was a radiology resident ( see text ) cor coefficient of repeatability mean bias reproducibility the second reader was a technician student ( see text ) cor coefficient of repeatability peak velocity ( cm / s ) peak velocity ( cm / s ) table 3 intra - reader reproducibility of the second reader aortic flow peak velocity ( cm / s ) pulmonary flow forward ( ml / beat ) backward ( ml / beat ) forward ( ml / beat ) backward ( ml / beat ) corresponding to an intra - reader reproducibility of 99% ; the same data for r2 were 181 cm / s , 3 cm / s , and 98% . 
 the inter - reader reproducibility analysis of the aortic flow peak velocity showed a cor of 10 cm / s , over a mean of 103 cm / s , corresponding to an inter - reader reproducibility of 91% ; the same data for the pulmonary flow were 7 cm / s , 180 cm / s , and 96% . 
3. discussion cardiac magnetic resonance has emerged as a reliable imaging technique for assessing heart valve disease , quantify its severity , and to evaluate its effect on the heart morphology and function [ 13 , 7 ]  . 
patient management using cmr includes follow - up for treatment effect monitoring or disease progression [ 19 , 20 ]  . reproducibility means the ability of a reader to provide the same values when repeating the measurement a number of times . 
when a follow - up measurement is performed on a patient , the clinician needs to identify a true change that can be ascribed to treatment effect or worsening of disease , rather than to measurement errors [ 21 ]  . 
in this scenario , the readers experience may play a role and skilled operators may be necessary . in this study , we obtained a good - to - excellent intrareader reproducibility of cmr in flow measurement for all variables under consideration , except for the backward flow of the ascending aorta . 
indeed , intra - reader reproducibility was higher than 90% for the trained reader ( r1 ) and higher than 86% for the lower trained reader ( r2 )  . 
such a good result may be due thanks to the semi - automated method used for segmentation that is not difficult to be used also by less experienced readers [ 9 ]  . 
this means that a readers learning curve should be short and that the segmentation of vessel boundaries through a semi - automated method may also be performed by not highly specialized personnel . 
however , although of a small magnitude , data suggest an additional reproducibility of r1 over r2 , likely due to the different educational background and the different level of training [ 9 ]  . inter - reader reproducibility , even if reaching a maximum of 96% for the blood peak velocity of the pulmonary artery , decreased to 75 and 82% for the forward and backward flow of the pulmonary artery , respectively , being lower than 1 3 radiol med ( 2017 ) 122 : 179185 fig . 
2 blandaltman plots for intra - reader reproducibility analysis of the first reader : a and b peak velocity , c and d forward flow and e and f backward flow of the aorta ( left column ) and pulmonary artery ( right column ) table 4 inter - reader reproducibility analysis aortic flow peak velocity ( cm / s ) forward ( ml / beat ) backward ( ml / beat ) forward ( ml / beat ) backward ( ml / beat ) pulmonary flow peak velocity ( cm / s ) mean bias reproducibility cor coefficient of repeatability 1 3 184 radiol med ( 2017 ) 122 : 179185 fig . 
3 blandaltman plots for inter - reader reproducibility analysis : a and b peak velocity , c and d forward flow and e and f backward flow of the aorta ( left column ) and pulmonary artery ( right column ) that observed in previous studies . 
compared an automated contour detection algorithm for analysis of the ascending aorta flow with a fully manual segmentation , showing intraand inter - reader variability lower than 2% for both manual and automated methods [ 13 ]  . 
in fact , a low to very low reproducibility for this variable was obtained , being lower than 50% for the intra - reader analysis and equal to 20% for the interreader analysis . 
reproducibility being given as percentage of the mean , even subtle measurement variations due to small 1 3 radiol med ( 2017 ) 122 : 179185 differences in segmentation may have a strong negative impact on reproducibility . the major limitation of this study is that results are related to the particular 1.5 - t unit used for imaging patients and to the sequences and technical parameters used , also including the use of breath - hold or respiratory gating for avoiding artifacts from respiratory movements . 
another limitation may be the study population that included patients affected with different cardiovascular diseases ( even if the majority of patients had a tetralogy of fallot ) who had a pathology of the aortic and / or pulmonary valve . 
probably , limiting to a more homogeneous population could demonstrate an even higher reproducibility . in conclusion , this study showed a good - to - excellent intraand inter - reader reproducibility of blood flow measurements in patients with congenital heart disease using cmr and a semi - automated method of segmentation , with a limited impact of the operators training . compliance with ethical standards conflict of interest f . 
therefore , pretreatment accurate assessment of extracapsular extension ( ece ) in prostate cancer is essential for selecting an optimal therapy such as radical prostatectomy , radiotherapy , and non - curative systemic therapies [ 2 ]  . 
in other words , accurate assessment of ece improves the accuracy in selecting appropriate patients for active surveillance among those with and without clinically significant cancers and contributes to avoid overand undertreatment [ 3 ]  . transrectal ultrasonography ( trus ) and digital rectal examination ( dre ) which are the conventional techniques for clinical staging are not sufficient in sensitivity and specificity for the detection of ece in prostate cancer [ 46 ]  . 
particularly , dre has been shown to be a poor predictor of tumor location and extent [ 7 ] , and the accuracy for local staging by dre is lower than that by trus [ 8 ]  . 
 furthermore , it has been reported that magnetic resonance imaging ( mri ) using t2 - weighted imaging ( t2wi ) as well as biopsy gleason score ( gs ) are powerful predictors of ece among prostate - specific antigen ( psa ) , psa density , mri using t2wi , trus , and systematic prostate biopsy [ 9 ]  . 1 3 radiol med ( 2017 ) 122 : 228238 thus , prostate mri using t2wi is considered as a useful imaging modality for pretreatment clinical staging of prostate cancer . 
actually , in usual clinical practice , we often experience difficulty in diagnosing ece in patients of pt3 stage without specific mr findings of ece such as obliteration of the rectoprostatic angle and periprostatic fat [ 10 , 2830 ]  . 
 this may be due to the inability to visualize microscopic ece on mri and the increase of small organ - confined prostate cancer in psa era [ 28 , 31 , 32 ]  . on the other hand , although gs is an indicator of tumor aggressiveness , gs obtained by biopsy is underestimated in 2954% as compared with gs obtained by radical prostatectomy , i.e. , the accurate tumor aggressiveness [ 33 ]  . 
previous reports have shown that diffusion - weighted imaging ( dwi ) including apparent diffusion coefficient ( adc ) is useful for not only tumor detection but also assessment of tumor aggressiveness of prostate cancer [ 34 , 35 ]  . 
furthermore , a recent study has reported that the correlation between these variables tended to be stronger when using a 3 - t system than a 1.5 - t system and when using a higher b value such as 0 and 2000 s / mm2 than standard b values such as 0 and 1000 s / mm2 [ 38 ]  . until now , six prospective or retrospective studies have been reported on the added value of dwi with adc for the detection of ece [ 2527 , 3941 ]  . 
however , no studies have been reported with dwi using adc obtained with high b value ( 2000 s / mm2 ) at 3 - t focusing on the detection of the ece in prostate cancer . 
therefore , the goal of this study was to investigate whether high b value dwi at 3 - t contributes to the improvement of diagnostic ability of ece in prostate cancer . materials and methods patient characteristics this retrospective study was approved by our institutional review board , and the requirement for obtaining informed consent from patients was waived . a total of 47 consecutive patients with biopsy - proved prostate cancer underwent mr imaging of the prostate with a 3 - t system between april 2012 and june 2014 at our institution . 
dwi was acquired with motion - probing gradient ( mpg ) pulses applied sequentially along three orthogonal orientations following acquisition at b values of 0 and 2000 s / mm2 . 
adc maps were reconstructed by calculating adc in each pixel of each slice , and the adc values were calculated for a pair of b values : 0 and 2000 s / mm2 . 
data acquisition for dce - mri began simultaneously with initiation of intravenous injection of meglumine gadoterate ( magnescope ; guerbet japan , tokyo , japan ) or gadopentetate dimeglumine ( magnevist ; bayer schering pharma , osaka , japan ) of 0.1 mmol / kg body weight at a rate of 3 ml / s via a power injector , followed by a 40 - ml saline flush at the same rate of contrast media injection . 
multiphase dce - mr images were obtained every 30 s for 3 min ( six phases ) without breath - holding . histopathologic analysis in all 43 patients , the reference standard for tumor localization and ece of prostate cancer was determined using the step - section histologic slices from radical prostatectomy . 
the distal portion of the apex and the proximal portion of base were amputated and were sliced sagittally to assess the resection marg all slices were processed uniformly and submitted entirely . 
after routine hematoxylin - eosin staining , an experienced uropathologist who was blinded to the mri findings evaluated all pathologic specimens and marked tumors and location of ece on the photographs for each slice . 
the pathologist further recorded the tumor location , the presence and location of ece , the tumor gs , the presence of surgical margin , the presence of lymph node metastasis , the presence of distant metastasis , and final pathological stage in the pathological report . 
each tumor was evaluated according to the 2005 international society of urological pathology modified gleason grading system [ 43 ]  . clinical and histopathologic data collection as clinical and histopathologic data , the initial psa level and biopsy gs were collected from the medical and pathological records by a study coordinator . image interpretation and data analysis mr images evaluation was performed using a pacs viewer ( rapideye core ; toshiba medical systems )  . 
two radiologists with 2 and 16 years of experience in prostate mr imaging were reviewed mr images in consensus , and they were aware that patients had prostate cancer but were blinded to other clinical and histopathologic findings . at first , the prostate mr images were reviewed to identify the presence or absence of ece using conventional diagnostic method with t2wi and dcm - mri and recorded the diagnostic certainty degree for mr finding of ece using a four - point scale ( grade 1 , reliable ; 2 , probably reliable ; 3 , questionable ; and 4 , impossible ) ( conventional mri method )  . 
diagnosis of ece on t2wi and dce - mri was based on at least one of the following criteria : interruption of the capsule , broad tumor contact ( > 10 mm ) , obliteration of periprostatic fat , obliteration of the rectoprostatic angle , asymmetric or direct involvement of the neurovascular bundle , angulated prostate gland contour , irregular or spiculated margin on t2wi , and seminal vesicle lesion with both low signal intensity on t2wi and enhancement effect on dce - mri [ 10 , 2830 ]  . after the evaluation of ece , the prostate mr images were further reviewed to identify cancer foci that were subsequently targeted for the image analysis of ece in consensus by the same two radiologists . 
cancer foci were selected if they showed positive finding with 5 mm or more on at least one of the three mr imaging sequences , including t2wi , dwi , and dce - mri . 
a tumor site was considered to match histological findings if the tumor depicted on the image was present in the same region of the prostate indicated in the prostatectomy specimen . 
that is , the final diagnosis of ece in patients with high diagnostic certainty was determined only by conventional mri method , whereas the patients with low diagnostic certainty was considered ece negative when tumor adc value is higher than the adc cutoff value and ece positive when tumor adc value is lower than the adc cutoff value , regardless of the diagnosis of ece by conventional mri method . 
among these 15 patients with pt3a disease , 12 patients ( 80% ) had only microscopic ece less than 1 m the remaining 25 of 43 patients ( 58% ) was organ - confined disease . 
in 43 patients who underwent radical prostatectomy , a total of 43 prostate cancer lesions ( matching the histopathologic findings ) with lowest adc value in each patient were selected . 
other histopathlogical characteristics in 43 patients with prostate cancer are shown in table 2 . evaluation of ece using conventional mri method by conventional mri method , 33 of 43 patients ( 77% ) were diagnosed as ece negative ( t2a in 18 , t2b in one , and t2c in 14 patients ) and the remaining 10 patients ( 23% ) as ece positive ( t3a in 8 and t3b in 2 )  . 
the diagnostic certainty degree for the mri findings of ece were grade 1 in 16 patients ( ece negative in 14 and ece positive in 2 ) , grade 2 in 12 patients ( ece negative in 9 and ece positive in 3 ) , grade 3 in 14 patients ( ece negative in 9 and ece positive in 5 ) , and grade 4 in one patient ( ece negative in 1 )  . 
 accordingly , the tumor adc was shown to be an independent predictor of ece in prostate cancer . comparison of detection ability of ece between conventional mri method and mri method adc 10 in terms of discrimination between ece positive group and ece negative group using adc values , a cutoff value of 3 / mm2 / s resulted in a sensitivity of 83% and a 0.72 specificity of 68% , showing that the sum of sensitivity and specificity is maximized . 
the diagnosis of ece after using adc cutoff value in 11 patients with broad tumor contact was unchanged in 4 patients , changed to correct diagnosis in 6 patients , and changed to incorrect diagnosis in one patient . 
that is , the median psa level of our subjects was 7.57 ng / ml , 60% of patients ( 26 / 43 patients ) were gray - zone psa level ( 410 ng / ml ) , and 80% of patients were microscopic ece less than 1 mrecent studies have reported that in psa screening era non - organ - confined prostate cancer with microscopic ece has increased , and patients with pt3 in psa screening era had a better prognosis compared with pre - psa screening era [ 31 , 32 ]  . 
accordingly , the study for patients with low detection sensitivity of ece on conventional mri is clinically challenging , and new techniques to improve the detection ability of ece is expected for an appropriate management in patients with prostate cancer in psa screening era . in multivariable logistic regression analyses using of psa , histopathologic , and mri findings , tumor adc was an independent predictor for discriminating presence or absence of ece in prostate cancer in all 43 patients in conventional mri method . 
recent studies also reported that tumor adc including not only mean value which was used in this study but also median ; 10th centile and 20th centile values were associated with the presence of ece in patients with prostate cancer [ 25 , 26 , 39 , 40 ]  . 
accordingly , a further large - scale multi - center study will be required for determining the adc value with highest discrimination ability of ece among these indices which were obtained using novel techniques such the adc 1 3 234 radiol med ( 2017 ) 122 : 228238 fig . 
1 a 64 - year - old male with prostate cancer ( psa level of 7.54 ng / ml , prostatectomy gleason score of 4 3 , pathological stage t3a ) in the middle right region in the peripheral zone . 
cancer lesion is shown as a homogeneous hypointense area with mass effect on t2 - weighted imaging ( arrow ) ( a ) , a focal hyperintensity on diffusion - weighted imaging with b values of 0 and 2000 s / mm2 ( arrow ) ( b ) , and a focal hypointensity on apparent diffusion coefficient ( adc ) map ( arrow ) ( c )  . 
readers diagnosed as t3a disease with low diagnostic certainty ( grade 3 ( questionable ) ) for mr findings of broad tumor contact suspecting extracapsular extension ( ece ) on t2 - weighted image ( arrowheads ) ( a )  . 
the lesion with low diagadc value was 0.64 nostic certainty was reevaluated by adc cutoff value ( 0.72 mm2 / s ) , but the diagnosis of ece using conventional mri method was unchanged . 
photograph of a macroscopic specimen shows the cancer lesion ( red circles ) with ece ( red arrow ) ( d ) 10 10 histogram analysis [ 26 , 45 ]  . 
we expected that inclusion of adc cutoff value in the diagnostic process of ece for patients with low diagnostic certainty by conventional mri would result in further improvement of detection ability of ece in prostate cancer . 
accordingly , further multi - center studies on different multiparametric mri systems will be needed to strengthen these initial results for the clinical use of adc cutoff value to detect ece . 10 in conventional mri method alone , 15 of 43 patients ( 35% ) showed low diagnostic certainty for the detection of ece in prostate cancer including grade 3 in 14 patients and grade 4 in one patient , suggesting the difficulty for the diagnosis of ece in our study population . 
ninety - three percentage ( 14 / 15 patients ) among these patients with low diagnostic certainty were led to correct diagnosis of ece by reevaluation using the adc cutoff value ( table 3 )  . 
on the contrary , only one patient turned into incorrect diagnosis using the adc cutoff value . in comparison of detection ability of ece between conventional mri method and mri and adc method , the all indices were substantially higher in mri and adc method than conventional mri method . 
2 a 71 - year - old male with prostate cancer ( psa level of 13.2 ng / ml , prostatectomy gleason score of 4 3 , pathological stage t2a ) in the middle right region in the peripheral zone . 
cancer lesion is shown as a homogeneous hypointense area with mass effect on t2 - weighted imaging ( arrow ) ( a ) , a focal slight hyperintensity on diffusion - weighted imaging ( arrow ) ( b ) , a focal slight hypointensity on apparent diffusion coefficient ( adc ) map ( arrow ) ( c ) , and a slight early enhancement on dynamic contrast - enhanced mr imaging ( dce - mri ) ( arrow ) ( d )  . 
readers diagnosed as t3a disease with low diagnostic certainty ( grade 3 ( questionable ) ) for mr findings of broad tumor contact and irregular margin suspecting extracapsular extension ( ece ) on t2 - weighted image ( arrowheads ) ( a )  . 
and high b value dwi such as a present study will be also necessary . unexpectedly , the detection sensitivity of ece in patients with high diagnostic certainty using conventional mri method was relatively low ( 56% ) against extremely high specificity ( 100% )  . 
further measures for improving the detection sensitivity of ece in patients with high diagnostic certainty for conventional mri findings of ece will be necessary . finally , 72% ( 11 / 15 patients ) of patients with low diagnostic certainty for the detection of ece in prostate cancer were judged based on the criteria of broad tumor contact in t2wi . 
this result is consistent with the statement in esur prostate mr guidelines 2012 , in which broad tumor contact , i.e. , abutment is classified as a low suspicious mr finding ( score 1 ) for the diagnosis of ece [ 46 ]  . 
the addition of adc cutoff method , however , the overall accuracy for the prediction of ece resulted in an extremely high value of 91% ( 10 / 11 patients )  . 
the favorable result may be due to the strong relationship between tumor adc obtained with high b value dwi at 3t and tumor aggressiveness such as gs of 1 3 radiol med ( 2017 ) 122 : 228238 236 4 , pathofig . 
3 a 72 - year - old male with prostate cancer ( psa level of 20.96 ng / ml , prostatectomy gleason score of 3 logical stage t2c ) in the middle right region in the peripheral zone . 
cancer lesion is shown as a homogeneous hypointense area with mass effect on t2 - weighted imaging ( arrow ) ( a ) , a focal hyperintensity on diffusion - weighted imaging ( arrow ) ( b ) , a focal hypointensity on apparent diffusion coefficient ( adc ) map ( arrow ) ( c ) , and an early enhancement on dynamic contrast - enhanced mr imaging ( dce - mri ) ( arrow ) ( d )  . 
readers diagnosed as t2 disease with low diagnostic certainty ( grade 3 ( questionable ) ) for mr findings of broad tumor contact but clear prostatic capsule on t2 - weighted image ( arrowheads ) ( a )  . 
the green circles show high - grade prostatic intraepithelial neoplasia ( pin ) 10 prostate cancer that is used with nomogram to predict ece [ 38 , 47 ]  . our study had several limitations . 
further prospective investigations with larger patient populations are needed to support our results using adc cutoff method obtained at high b value dwi at 3t for the assessment of ece in prostate cancer . 
however , a previous study reported that 3 - t phased - array mri might be equivalent to 1.5 - t endorectal mri in the evaluation of local staging accuracy of prostate cancer without significant loss of image quality [ 23 ]  . 
fourth , when using adc to detect ece in prostate cancer , the adc value may be different under the influence of mr scanner type , magnetic field strength , and b values . 
other functional mr techniques such as qualitative visual assessment using dw image and adc map [ 2527 ] , and mr spectroscopic imaging may correct misdiagnosis of ece using the adc cutoff value and may contribute for further improvement of detection ability of ece in prostate cancer . in conclusion , the addition of adc cutoff value obtained with high b value ( 0 , 2000 s / mm2 ) dwi at 3 - t to patients 1 3 radiol med ( 2017 ) 122 : 228238 with low diagnostic certainty in the assessment of ece using conventional mri method improved the diagnostic ability of ece of prostate cancer . 
in us and europe pediatric radiologists had to face a huge challenge , which brought to the image gently campaign and the eurosafe initiative with the aim to rebut misinformation and to support medical radiation protection . 
the linear no threshold modelwhich is the base of contemporary radioprotectionis increasingly questioned by new recent studies suggesting that low dose radiation would decrease cancer risk thanks to the enhancement of immune system response . 
 when considering benefits and risks , an important risk is * claudio granata cgranata@sirm.org imaging department , bambino ges childrens hospital , irccs , 00146 rome , italy 2 clinical technology innovations research area , bambino ges childrens hospital , irccs , 00146 rome , italy 3 department of radiology , irccs istituto giannina gaslini , 16147 genoa , italy too often ignored : the risk that skipping a diagnostic exam may cause a misdiagnosis , and therefore , a poor outcome . 
the first sentence in sternbergs usa today article was each year , about 1.6 million children in the usa get ct scans to the head and abdomenand about 1500 of these will die later in life of radiation - induced cancer , according to research out today [ 2 ]  . obviously , the article had international echo and paediatric radiologists found themselves facing a huge challenge , which mainly concerned the use of ct [ 4 ]  . 
in the us , their response was brilliant : they created image gently [ 5 ] , not only to implement changes in paediatric radiology practice , but also as a defence mechanism to rebut misinformation . 
eurosafe pursues similar objectives : its mission is : to support and strengthen medical radiation protection across europe following a holistic , inclusive approach [ 8 ]  . finally , the global media campaign had positive results on industry research , and , together with the medical culture , powerfully contributed to reduce substantial variability in imaging techniques used in paediatric imaging also among non - paediatric centers and impelled industry to develop more efficient imaging technologies . 
there were continuing efforts to develop diagnostic reference levels ( drls ) throughout the world and drls for paediatric ct have been established or studied in several european countries [ 9 , 10 ]  . 
the recent pidrl document [ 11 ] is a synthesis of the european reports , and a proposal for a standardized method for the development of future drls in children . 
drls are an advisory measure to improve optimization of patients protection by identifying high patient dose levels that might not be acceptable on the basis of image quality prerequisites . the facts in the present study we considered publications concerning risk of cancer as related to computed tomography scan . 
we subsequently refined the search including further terms , namely adult , child , neoplasms , radiation - induced , radiation dosage , radiol med ( 2017 ) 122 : 215220 radiation exposure , alara . 
in this way we found 1217 articles . the three most cited articles are also the most pessimistic : 3906 citations for the article computed tomography an increasing source of radiation exposure from brenner et al . 
 [ 13 ] , 913 for the article radiation exposure from ct scans in childhood and subsequent risk of leukemia and brain tumours : a retrospective cohort study from pearce et al . 
these simulations were performed by making use of series of computational human paediatric phantoms along with realistic age - dependent ct acquisition parameters [ 3 , 14 , 1720 ]  . the judgement on damage and alarm makes a huge noise and widespread public concern . actually , when we focus on dose management , we paradoxically accentuate the perception that medical imaging doses are dangerous . 
after all , why would we want to manage / reduce the dose if it were not dangerous ? shocking publications continue to be issued and become the titles of newspaper commentaries . 
the methodology used by pearce was harshly criticized by cohen ( only 2 citations ) [ 7 ] , who underscored that , although 178 , 000 children were studied , the study design had major flaws and information reporting was inaccurate . 
in fact , the first proposition of the paper maintained that the authors obtained typical machine settings for ct in young people from u.k. - wide surveys undertaken in 1989 and 2003 . 
 moreover , the study had no control population , and the authors did not evaluate pre - existing conditions that may be related to cancer ( reverse causality )  . 
 ( only 11 citations ) estimated the cancer risk related to childhood ct scans , and examined how cancerpredisposing factors affect radiation - related risk assessment [ 17 ]  . 
 [ 17 ] ( 0 citations ) and states : there are several major differences that complicate direct comparison with our study , particularly the different calendar periods of exposure : 19802002 in the united kingdom vs 20002010 in france . 
in addition , their study population came from a number of specialist hospitals , which resulted in an enriched population for serious conditions and finally they used hospital inpatient data to ascertain the clinical conditions . 
they also used a somewhat different list of cancer - predisposing conditions . surprisingly , there are many uncertainties and there are many inconsistent publications stating that ct scans cause cancer in children . similar biases are in the article of mathews et al . 
this was a retrospective study based on a database concerning people aged 019 years , who had ct scan done during the period 1 january 1985 to 31 december 2005 . 
the authors estimated lifetime attributable risk of cancers from the observed organ doses using ageand sex - specific cancer risk models in the biological effects of ionizing radiations ( beir ) vii [ 16 ] they stated that theoretically nationally , 4 million paediatric ct scans of the head , abdomen / pelvis , chest , or spine performed each year are projected to cause 4870 future cancers . 
however , this study concludes there are 95% uncertainty limits around the projected numbers of cancers on the basis of the coefficient of variation given in the beir - vii report , which provides a gross variability estimate from these three sources of uncertainty . 
unfortunately , only the first message attracted attention . a common issue with studies dealing with radiation exposure from ct studies and cancer risk is the lack of information about the indications for the ct examination . 
terrifying assumptions have easy success . for this reason , it is important to know and understand the opinions of those who question current thinking . the linear no threshold ( lnt ) model is based on the linear relationship assumption summarised as : radiation / mutation and cancerous mutation / cancer . 
the life span study ( lss ) cohort of about 120 , 000 subjects included atomic bomb survivors and residents of hiroshima and nagasaki who were not in either city at the time of the bombing . 
british radiologists who entered service during the period 19551979 , who were likely to be exposed to low - dose radiation , had a cancer death rate lower than the background cancer rate [ 20 , 34 ]  . conclusions paediatric radiologists have many important issues and challenges to deal with . in europe , council directive 2013 / 59 / euratom established that should strengthen the requirements concerning information to be provided to patients , the recording and reporting of doses from medical procedures , the use of diagnostic reference levels and the availability of doseindicating devices . on july 2015 , joint commission stated : the radiation dose ( ctdivol or dlp ) must be exam - specific , summarized by series or anatomic area , and documented in a retrievable format . 
bias by indication : ct is performed for the detection or monitoring of a pathology or symptomatology associated with higher risk of cancer , for example because of a particular genetic syndrome or acquired immunodeficiency . 
the most effective means to decrease radiation dose associated with paediatric imaging is to reduce or preferably eliminate unnecessary or inappropriate procedures , but justification and guidelines depend on different cultures and factors , such as defensive medical decision making . 
malpractice lawsuit is often seen as a mechanism to improve quality of care , but it may actually impede the translation of evidence into practice , damaging patients and decreasing the quality of care . optimization is a process by which a substantial portion of the standard dose is eliminated with a consequent increase in noise , but without loss in diagnostic performance and / or confidence to accomplish the specified medical task . 
in six us paediatric radiology institutions using standard clinical protocols and radiation doses below the 25th percentile , 5% of the studies were judged to be nondiagnostic [ 30 ]  . 
this issue is the essence of clinical ct dose reduction : what do i need to detect ? how much dose do i need to confidently detect its presence or absence ? peer review fails more and more often . 
for instance , all articles on alternative techniques ( us , mri ) for the study of the chest report the absence of ionizing radiation as 1 3 radiol med ( 2017 ) 122 : 215220 ct exams exceeded expected dose ranges identified in imaging protocols [ 35 ]  . going beyond legal problems , a positive message is needed to give confidence . good medical practice includes efficient communication about the benefits and risks of health procedures . 
several stakeholders are involved in the communication of radiation risks and benefits in paediatric imaging : parents , patients , and caregivers . for instance , it is difficult to empathise when speaking about dose units , risk , likelihoods and stochastic effects . 
 in the communication on the risks , the comparison with familiar radiation exposures ( such as chest x - rays or natural background radiation ) has been highly recommended to facilitate understanding of the dose [ 29 ]  . 
but the dose delivered during a chest x - ray is so low that using it as a denominator to estimate the corresponding amount of chest x - rays equivalent with the dose level of any other radiological practice may be misinforming and may unreasonably alarm paediatricians and parents . 
when considering benefits and risks , there is an important risk which is too often ignored : the risk that skipping a diagnostic exam may cause a misdiagnosis , and therefore a poor outcome . 
we are not sure that there is a risk at very low doses , like those doses in the vast majority of x - ray procedures or ct [ 29 ]  . in clinical practice , all these discussions should help determine the situations in which the estimated benefits do not balance the risks and clarify the information to be provided to patients , parents and health - care providers . so far , prudently and wisely , it is correct to follow the risk predictions extrapolated from studies at high doses under the lnt postulation . 
with respect to wb - ct the highest rate of inappropriate imaging prescriptions came from the haematology clinical operative unit ( ou ) ( 44% ) and emergency medicine ( 33% ) ; with respect to petct , the thoracic surgery ou ( 53% ) and haematology ou ( 48% ) showed the most inappropriate prescriptions . 
for bedside cxrs , the largest inappropriate prescribers were the emergency medicine ou ( 48% ) , the cardiac surgery ou ( 58% ) , the intensive care ou ( 67% ) and anaesthesia resuscitation ou ( 78% )  . 
the most represented classes of inappropriateness were 2 , 3 , 4 and 6 . conclusions the elimination of inappropriate prescriptions would result in an annual savings of approximately 390 , 000 euro . 
however , if the usefulness of a radiological examination is to change patient management , its overuse without clinicaldiagnostic gains may have negative economic and clinical 1 3 222 radiol med ( 2017 ) 122 : 221227 consequences in terms of radioprotection . 
the italian ministry of health has drafted a clinical audit manual which provides a methodology regarding specific medical / healthcare issues and some aspects of the current practices [ 2 ]  . 
 recently , in italy some health - care facilities have included ca as part of clinical practice [ 3 , 4 ]  . the purpose of our study was to audit the level of appropriateness of whole body ct ( wb - ct ) , petct and chest x - rays ( cxrs ) prescribed at the tor vergata university hospital in the inpatient setting and to identify the main categories of inappropriate prescribers and the most frequent inappropriate indications . materials and methods the retrospective observational study has involved a multidisciplinary work group consisting of one medical area facilitator , one surgical area facilitator , two diagnostic imaging facilitators , one hospital directorate manager and the chiefs of the respective clinical operative units ( ou )  . 
the examinations were stratified among the different ous and normalized to the number of discharges of each ous and expressed in percentage ( number of examinations / total discharges 100 )  . 
the wb - ct and petct examinations prescribed by the ous that proved to be equal or to exceed the threshold of 20% of the number of examinations / total number of discharges were included in the analysis of the diagnostic appropriateness . 
with regard to traditional cxrs and bedside cxrs , the analysis included the examinations prescribed by the ous that proved to be equal or to exceed the threshold of 50% of the number of examinations / number of discharges . 
the appropriateness of the examinations was defined following the guidelines of the american college of radiology appropriateness criteria [ 5 ] : a appropridoubtful appropriateness , score 46 , ate , score 79 , d or i inappropriate , score 13 . 
the second step involved categorizing the causes of inappropriateness ( in classes d and i ) , using groupings according to the european union medical imaging guidelines [ 6 ] into one of six possible broad categories : ( 1 ) repeating tests that have already been done ( e.g. , at another hospital )  . 
in our setting , category 1 was assigned to examinations performed too often ( category 2 ) or to investigation whose results were unlikely to affect patient management ( category 3 ) that we found to have already been performed at another hospital ; ( 2 ) investigation when results are unlikely to affect patient management ( e.g. , because the anticipated positive finding is usually irrelevant or because a positive finding is so unlikely ) ; ( 3 ) investigating too often ( e.g. , before the disease could have progressed or resolved , or before the results could influence treatment ) ; ( 4 ) do the wrong test . 
in our study preoperative cxrs were also included in this category ; ( 5 ) failing to provide appropriate clinical information and questions that the imaging investigation should answer ; ( 6 ) excessive investigation . 
some clinicians tend to rely on tests more than others , and some patients have inappropriate expectations of the optimal type of examination . results a total of 2232 wb - ct , 703 petct , 6219 bedside cxrs and 5490 traditional cxrs were performed at tor vergata university hospital during 2014 . 
for the evaluation of the prescriptive appropriateness , the clinical records of 1190 patients were assessed with regard to wb - ct , 353 clinical records for petct , 873 clinical records for bedside 1 3 radiol med ( 2017 ) 122 : 221227 fig . 
with regard to traditional cxrs , the percentage of inappropriateness was consistently distributed among all surgical ous , including ear nose and throat , with an average rate of inappropriateness equal to 63% . 
for bedside cxrs , the most inappropriate prescribers were the ous of emergency medicine ( 48% ) , cardiac surgery ( 58% ) , intensive care ( 67% ) and anaesthesia and resuscitation ( 78% )  . 
the most represented classes of inappropriateness were 2 , 3 , 4 and 6 ( table 1 )  . 1 3 radiol med ( 2017 ) 122 : 221227 table 1 stratification of the causes of inappropriateness in acr classes d and i , using groupings according to the european union medical imaging guidelines into one of six possible broad categories inappropriateness categories wb - ct ( % ) ctpet ( % ) cxr ( % ) bedside cxr ( % ) 1 . 
some clinicians tend to rely on tests more than others , and some patients have inappropriate expectations of the optimal type of examination discussion in recent years , prescriptive inappropriateness has become one of the main issues in health care in terms of waiting times , economic costs and radiation doses . to date , the evaluation of diagnostic imaging prescription appropriateness has been mostly limited to the outpatient settings ; however , the risks of prescriptive inappropriateness may also be present in a more controlled clinical setting such as the inpatients setting [ 4 ]  . in our study , we have revised the prescriptions of imaging examinations with a high economic and numeric impact , such as wb - ct , petct , cxrs and bedside cxrs performed in the inpatient setting during the year 2014 at the tor vergata university hospital . 
in the usa , the institute of medicine has suggested the potential for substantial savings , estimating that $8 billion is spent annually on repeat testing [ 7 ]  . 
although there is wide variation in reporting how much waste exists in our current health - care delivery system and how it should be defined , there is consensus among researchers and policy makers that such waste exists and that action can be taken to reduce it . 
indeed , from both research and policy perspectives , the term repeat testing is ambiguous and is often used to describe many different facets of both appropriate and potentially inappropriate care [ 8 ]  . 
in our setting , category 1 was assigned to examinations performed too often ( category 2 ) or to investigation whose results were unlikely to affect patient management ( category 3 ) that we found to have already been performed at another hospital . 
in these cases , both patient education and improved integration of electronic health records could be solutions for such a waste of resources [ 8 ]  . with regard to emergency medicine , the main category of inappropriate prescription was category 2 , i.e. 
investigation when results are unlikely to affect patient management ( e.g. , because the anticipated positive finding is usually irrelevant or because a positive finding is so unlikely )  . 
 in fact , a number of studies have shown that performing ct in post - traumatic , haemodynamically stable patients with normal clinical parameters does not affect the patients clinical management [ 9 , 10 ]  . 
analysed the medical records of patients presenting with a triage history of motorized blunt force trauma who underwent ct of the chest , abdomen and pelvis at the time of presentation . 
the authors found that the clinical yield of performing ct of the chest , abdomen and pelvis in motorized blunt trauma patients with normal clinical examinations was minimal [ 11 ]  . 
although we recognize the value of a normal ct scan in quickly and accurately triaging patients , extended clinical observation with serial physical examination may be considered as an alternative to ct where appropriate [ 12 ]  . with regard to inappropriate petct requests , the most inappropriate prescriptions came from the haematology ou and fell within category 4 , do the wrong test . 
in particular , 1 3 226 radiol med ( 2017 ) 122 : 221227 most of the inappropriate prescriptions concerned petct routine assessment of patients with chronic lymphocytic leukaemia ( cll )  . 
despite the fact that some studies suggested that pet / ct may helpfully integrate the biologically based prognostic stratification of cll , no usefulness has been documented for petct in the routine surveillance of cll [ 13 , 14 ]  . 
in light of current scientific evidences , performing pet / ct imaging in cll is justified only whenever there is clinical suspicion for disease progression or complications [ 14 ]  . 
however , more prospective clinical trials including large cohorts of patients are certainly warranted to conclusively assess the role and prognostic impact of pet / ct in the routine management of cll patients . the other main inappropriate prescriptions of petct fell within category 6 , excessive investigation . 
 it is now consolidated that for part - solid nodules < 10 mm pet is of limited value and potentially misleading , and ct follow - up is advised [ 15 ]  . 
indeed , false - negative results for spn characterization on petct can occur in three main settings : small lesion size , low tumour metabolic activity and hyperglycaemia [ 16 ]  . 
when the medical community has preached the importance of early detection of cancer for so long , it may prove difficult to convince physicians and the patients that petct of every nodule is unnecessary . with regard to cxrs , since most cxr tests were preoperative , the inappropriateness was consistently distributed among all surgical ous and was categorized as category 4 ( do the wrong test )  . 
the royal college of radiologists has published a multi - centre study that analysed 10 , 619 pre - surgical cxr tests in patients , candidates for elective surgery , reaching the conclusion that the pre - surgical cxr test does not affect the surgical and / or anaesthesiology choice [ 18 ]  . 
evaluated the usefulness of preoperative chest radiographs in 905 patients based on risk factors including history of malignancy , recent history of smoking , exposure to toxic chemicals or signs and symptoms of recent infection . 
 indeed , some preoperative investigations may be appropriate , if they are based on the finding of a specific clinical abnormality and if the results of the test might affect the care of the patient . 
however , this approach requires a most careful examination by the physician but the resultant cost savings are the reward . for bedside cxrs , the ous involved were the emergency medicine , cardiac surgery , intensive care and anaesthesia and resuscitation , and the inappropriateness fell into category 3 ( investigating too often ) and category 2 ( investigation when results are unlikely to affect patient management )  . 
 furthermore , a meta - analysis published by oba and zaza in 2010 , carried out on a sample of 7078 patients hospitalized in intensive care units , half of whom underwent daily cxrs while the other half underwent cxrs only on specific clinical indications , showed that no changes occurred between the two groups with regard to mortality , length of hospitalization or use of pulmotor [ 21 ]  . 
along with these lines of evidences , a white paper by thomson reuters has documented that in the usa , more than 95 million diagnostic imaging examinations are performed each year , of which 2050% are inappropriate with a consequent loss of 250 325 billion of dollars per year [ 23 ]  . 
in italy , the almost uncontrollable growth in the number of diagnostic imaging test prescriptions together with the high number of negative examinations suggests poor appropriateness that does not improve the patients health in the outpatient setting [ 24 ]  . 
 indeed , our data confirm that poor appropriateness can also be present in a more controlled environment such as the inpatient setting and highlight the role of clinical audit as an important tool that can be used to critically review current practice and consequently to reduce the unnecessary use of health - care resources . as a limitation of our study , we accepted published guidelines as the only possible gold standard . 
notably , most of the guidelines are based on the level of evidence c , that is , the consensus in the absence of a firm scientific evidence base [ 25 ]  . 
moreover , the setting of the study was a university hospital with a high burden of diagnostic imaging examinations and patient discharges , of which we selected only a sample by choosing a subjective threshold of 20% of the number of examinations / total number of discharges for the cxrs and 50% for the petct and the wb - ct ; nonetheless , more 5000 clinical records were examined by our committee . 1 3 radiol med ( 2017 ) 122 : 221227 in conclusion based on our data , the elimination of inappropriate prescriptions would allow the diagnostic imaging department of tor vergata to avoid the execution of approximately 4000 examinations / year with savings of 390 , 000 euro / year . 
in light of such evidences , our work group is developing an implementation plan to increase the appropriateness of prescribing through the adaptation of the available evidence to the local context and experience . compliance with ethical standards funding the study received no funding . conflict of interest the authors declare that no conflict of interests exists . ethical approval the study has been approved by the irb and performed in accordance with the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . informed consent all patients gave their informed consent prior to their inclusion in the study . 
all the patients underwent mrl , using a 1.5t mr unit ( signa twin speed hdxt ; ge ) , after the subcutaneous injection of gadobenate dimeglumine ( gd - bopta ) with a little dose of lidocaine into the interdigital webs of the dorsal foot or hand . 
one patient had an early complication 1month after treatment . conclusions mrl is easy and safe to use and combines extensive information on the anatomy and functionality of lymphatic vessels and veins in a single process ; therefore , it could be useful in lva treatment planning and evaluating possible super - microsurgical treatment complications in patients with lymphedema . keywords lymphedema magnetic resonance imaging lymphatic vessels high - resolution mri lymphaticovenous anastomosis introduction lymphedema can occur either because of a congenital malformation of the lymphatic system or as a consequence of damaged lymphatic drainage produced by an injury to the lymphatic vessels and lymph nodes . 
as the cutaneous lymphatics are not functioning , the local immune response is impaired and recurrent skin infections are common , leading to further damage to the tissue and worsening of the edema [ 4 , 5 ]  . 
if lymphedema is left untreated , it will progress to the point of chronic limb enlargement , with disfiguration of the limb associated with severe functional and psychologic impairment [ 6 ]  . 
over the last few years , the lymphaticovenous anastomosis ( lva ) , a super - microsurgical treatment arranged to obtain a spontaneous shunt to surpass the site of the lymphatic obstruction conducting the lymphatic flow to the venous system , has been reported as the favoured treatment of lymphedema [ 7 ]  . 
in this context , magnetic resonance lymphangiography ( mrl ) , owing to its itemised anatomical depiction of the lymphatic system , could represent the preferred technique both in treatment planning and for the early diagnosis of possible super - microsurgical treatment complications [ 8 , 9 ]  . 
in particular mrl , examining the entire lower or upper extremity in several steps using high spatial and temporal resolution , provides both morphological and functional information about contrast agent uptake of the lymphatic vessels and veins in a single examination [ 10 ]  . the purpose of this manuscript is to describe the capability of mrl for imaging lymphatic vessels in patients suffering from lymphedema , its reliability in distinguishing lymphatic vessels from veins , and finally its role in planning lymphaticovenous anastomosis ( lva ) treatment and evaluating possible super - microsurgical treatment complications . materials andmethods patients we conducted a prospective study of 30 patients ( 24 women ) with a mean age of 30years ( range 1870 ) enrolled from february 2014 to october 2016 ; 17 out of 30 were affected by lower limb lymphedema with six cases of primary lymphedema ; the others were secondary to cancer treatment , primarily breast . 
four out of 30 patients ( 13.3% ) had stage i lymphedema , which represented an early accumulation of fluid that subsides with limb elevation and the remaining ( 86.7% ) had stage ii disease , which demonstrated tissue swelling that is rarely reduced by limb elevation alone and some degree of tissue fibrosis in the limb . 
all the patients underwent mrl between 18 and 24h before lva supermicrosurgical treatment ; lva was not performed during the medical operation in one patient because of poor visibility of potentially functional lymphatics . 
all procedures performed in this study involving human participants were undertaken in accordance with the ethical standards of the institutional and / or national research committee and the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
patients were fully informed of the procedure to obtain their complete collaboration and informed consent was obtained from all individual participants included in the study . mr examination patients position the position of the patient changed depending on the site of investigation : ( a ) lower limb : patients were placed in the supine position , feet first , with both legs on a ramp pillow so that the lower extremity was parallel to the main magnetic field and near the most homogeneous area of b0 . 
according to the height of the patient , 3 or 4 stations were examined in order to cover the following anatomical regions : ( 1 ) the lower leg inferior segment and foot region ( feet region ) ; ( 2 ) the lower leg superior segment and upper leg inferior segment , including knee region ( calf region ) ; ( 3 ) the middle upper leg and the proximal upper leg including inguinal region ( thigh region and pelvic region ) ; the toes of both feet emerged from the holes of the coil and were easily accessible for the injection of the contrast agent ; ( b ) upper limb : the same procedure was used to study the upper extremity but the patient was in the prone position , head first with arms extended laterally over the head and palms down . 
two stations were usually examined in order to cover the following anatomical regions : ( 1 ) hand - wrist - forearm ; ( 2 ) elbow - arm - shoulder ( axilla )  . 
direct contact of the coil with the skin was avoided by means of small cushions to reduce the hyperintensity artefacts [ 11 ]  . contrast agent administration the tip of a 2428 gauge ( g ) thin needle was gently inserted subcutaneously into the dorsal aspect of each foot or hand in all four interdigital web spaces . 
a mixture of the standard dose ( 0.1ml / kg body weight ) of gadobenate dimeglumine ( gd - bopta , multihance , 0.5m injectable solution , bracco imaging , milan , italy ) and 1ml of lidocaine 2% for local anaesthesia were subdivided into eight portions and injected 1 3 920 radiol med ( 2017 ) 122 : 918927 by two radiologists consecutively and simultaneously ( one for each extremity ) ; anyway , the contrast medium injection was limited to a maximum total volume of 8ml ( 1ml of multhiance for each interdigital web space )  . image analysis 50min for the upper limb . 
we used a receiving phased - array peripheral vascular coil for the study of the lower extremities ( flow 7000 phased - array peripheral vascular , usa instruments ) and an 8 - channel body array coil for the upper extremities , both with a large anatomical coverage and a good signal - to - noise ratio . the imaging protocol consisted of : ( 1 ) a survey and a calibration performed for all stations , 3 or 4 for the lower extremity ( footanklecalf , calfknee , thighhip ) and 2 or 3 for the upper extremity ( handwristforearm , elbowarmshoulder ) ; ( 2 ) a 3d steady - state free precession ( ssfp ) balanced electrocardiography ( ecg ) - triggered sequence ( fiesta , ge ) with spectral fat saturation ( spectral inversion at lipid , special , ge ) , before the injection of the contrast mediuthe ecg - trigger was acquired with a peripheral gating ( pg , ge ) and a time delay was set for a systolic phase acquisition in order to obtain a good visualisation of both the venous system and the distribution of the lymphedema within the same sequence and at the same time ; ( 3 ) a pre - contrast and post - contrast coronal 3d spoiled gradient - recalled echo t1 - weighted sequence with spectral inversion at lipid ( fspgr with special , ge ) in all stations in order to increase contrast sensitivity and visualised lymphatic vessels . 
the first station was repeated 5 , 20 and 35min after the injection of the contrast mediuthe other stations were examined consecutively and in sequence after the first station at each fixed time ( 5 , 20 and 35min )  . 
each 3dssfp - balanced sequence lasted about 3min and each 3d spoiled gradient - recalled echo t1 - weighted sequence lasted nearly 3min and 50s , with a total average examination time of 1h and 15min for the lower limb [ 3min3 / 4 anatomical regions / stations and 3min and 50s3 / 4 anatomical regions / stations4 times ( time 0 , 5 , 20 and 35min ) ] and one radiologist ( m.f.g. ) and one resident in radiology ( g.f. ) assessed the enhancement of lymphatic vessels and veins at different times after injection of contrast medium and measured vessel diameters . 
enhancement was evaluated calculating signal - to - noise ratio ( snr ) as follows : a region of interest ( roi ) , as large as possible , was placed over the vessels to obtain the signal and then elsewhere on the image to obtain the noise . 
multiplanar reformations ( mpr ) , thin - section maximum intensity projection ( mip ) reconstructions ( section thickness 1015mm ) and the 3d pointer were used to identify and localise the lymphatic and vascular structures for lva treatment . 
the post - processed images , with the essential spatial and depth information , were then recorded in the picture archiving and communication system ( pacs ) , so that they can be easily accessible to the surgeon before performing lva . 
vessels were dissected and 4 or 5 11 / 0 endoluminal sutures ( end - toend anastomosis ) with a 50 micron needle were performed between the lymphatic and venous vessels . 
during surgery , biopsy specimens of the mrl - presumed lymphatic vessels and veins in 18 out of 30 patients were collected and sent to the laboratory for immunoistochemical stainings in order to obtain a histological confirmation . statistical analysis considering the need to analyse repeated measures , a multilevel model for binary responses was used to compare the morphological ( diameter ) and functional ( snr ) methods for distinguishing veins and lymphatic pathways . 
the analysis was divided into 4 steps : ( a ) method efficiency , comparing the snr averages and diameters in affected and healthy limbs ; ( b ) evaluation of snr variability in relation to acquisition time and limb status ( affected or healthy ) ; ( c ) predicted probabilities , determining the probability of finding a vein or lymphatic vessel in relation to snr and acquisition time variability separately , in affected and healthy limbs and ( d ) applying students t test for paired samples to compare the snr of veins and lymphatic vessels , under the following hypothesis : h0 : = 0 h1 : 0 . a p value of less than 0.05 was considered to indicate a significant difference . 
the chi - square test was used to assess the association between mrl findings and immunoistochemical marker of lymphatic endothelium in specimens . all patients completed the examination without any significant complications . 
a total of 79 lymphatic vessels were identified in the affected limbs ; they were distinctly visible and recognised by their tortuous and beaded appearance in 22 patients ( 73.3% ) , whereas they were fundamentally rectilinear in 7 ( 23.3% ) ; the adjacent veins were straight with focal bulging only in the region of the venous valves . 
 the mean maximum diameter of affected lymphatic vessels ( 2.20.5mm ) was similar to that of adjacent veins ( 2.40.2mm ) , p > 0.05 , but greater than lymphatic vessels in the healthy limb ( 1.50.2mm ) , p < 0.05 , the latter rarely visualised ( 5 out of 30 patients , 16.7% ) because their lumen was almost virtual in a physiological condition . 
in one patient with secondary lower limb lymphedema , because of the chronically extreme impaired lymphatic circulation , we did not find any clear lymphatic vessels but only a diffused lightly enhanced honey - combing pattern ; few lymphatic channels were intraoperatively shown to be completely sclerosed 1 3 922 radiol med ( 2017 ) 122 : 918927 fig . 
thus , it is considered the current preferred surgical treatment not only in the early stages of the disease , where it can be curative , but even in patients with a long history of edema showing subcutaneous fibrosis who often exhibit some positive responses [ 12 , 13 ]  . 
in order to accurately plan the best strategy for microsurgical lva reconstruction , patients suffering from lymphedema need to 1 3 radiol med ( 2017 ) 122 : 918927 reformations ( mpr ) and thin - section maximum intensity projection ( mip ) reconstructions ; in particular , after mr examination , the vessels were marked on the skin to exactly localise the surgical sites . 
however , we must point out some mrl limitations : occasional difficulty in distinguishing the affected lymphatic vessels from veins and the lengthy examination time ; in fact , while the colloidbinding tracer of lymphoscintigraphy is very specific for the lymphatic system , gadolinium chelates are water soluble and diffusible , so that a certain amount of contrast agent may permeate into the subcutaneous veins , causing venous enhancement ; this problem was largely demonstrated by previous studies even with the precaution for avoiding to cannulate a small superficial vein [ 11 , 16 , 20 ] ; moreover even in patients over 80kg of body weight , the maximum volume of contrast agent was limited to 8ml , because of its possible accumulation next to the site of injection in case of severe lymph stasis , that could mask small peripheral lymphatic vessels . 
furthermore , because of the weak protein binding of gadobenate dimeglumine that increases its relaxivity , a small amount of contrast agent is generally sufficient for lymphatic vessels visualisation [ 24 ]  . 
regarding the mr technique , even if some authors [ 25 ] still claim that noncontrast mr lymphangiography using very heavily t2 - weighted fast spin eco ( fse ) sequences is a unique , non invasive , imaging modality for the diagnosis of lymphedema , the majority of authors perform mrl using both heavily t2 - weighted and t1 - weighted post - contrast sequences . 
in particular , after the first description , by lohrmann c and colleagues in 2006 , of indirect magnetic resonance ( mr ) lymphangiography with subcutaneous injection of gadodiamide in three patients with lymphedema [ 16 ] , lu etal . 
in 2010 , compared heavily t2 - weigthed with 3d fast spoiled gradient - recalled echo t1 - weighted sequences , reporting a higher possibility of identifying with the former , not only lymphedema but also lymphatic vessels , however , they suggest performing both sequences for an optimal examination [ 14 ]  . 
subsequently performed mrl in patients with gynaecological cancer - related lower limb lymphedema , adopting only 3d spoiled gradient - recalled echo t1 - weighted sequences before and after ( 20min ) subcutaneous injection of the contrast media to identify and distinguish lymphatics from veins [ 26 ]  . 
recently , jeon and colleagues have proposed new mrl protocols consisting of post - contrast 3d isotropic t1 - weighted fse and 3d isotropic intermediate - weighted fse sequences , the former providing better information regarding lymphatic vessels and the latter depicting lymph nodes in lymphedematous extremities ; furthermore , they claimed to distinguish lymphatic fig . 
2 a graph showing the different enhancement course of lymphatic vessels ( blue line ) and veins ( red line ) in affected limbs ; curve trends diverge after 25 min ; b graph showing the similar enhancement course of lymphatic vessels ( blue line ) and veins ( red line ) in healthy limbs undergo appropriate imaging to identify and localise the affected lymphatic vessels and closest veins and obtain the essential spatial and depth information regarding their anatomical position . 
in this scenario , the commonly used radioisotope lymphoscintigraphy , which could have a role in demonstrating the dermal backflow and lymph - node drainage , has insufficient spatial resolution to accurately depict anatomical distribution and localisation of both the lymphatic and vascular structures [ 14 ]  . 
direct lymphangiography , using iodine oil as the contrast agent , which is capable of visualising the lymphatics , is no longer routinely performed because it is highly invasive and difficult to realise and can also lead to life - threatening complications [ 15 ]  . 
since experimental animal models have only shown minor tissue damage after subcutaneous injection or extravasation of a gadolinium agent , demonstrating an acceptable safety profile for this administration route at the recommended dose , mrl using the paramagnetic contrast agent gd - bopta has emerged as the new method for assessing lymphostatic disorders [ 16 19 ]  . 
 thanks to its better spatial and temporal resolution , mrl is a promising technique in depicting the lymphatic network as well as the severity of lymphedema [ 2023 ]  . 
in planning lva , mrl has the role to localise lymphatic vessels and veins to perform the anastomoses through multiplanar 1 3 924 radiol med ( 2017 ) 122 : 918927 fig . 
3d ssfp balanced ecg - triggered sequence provides a map of the venous system ( open arrows , a ) ; post - contrast 3d coronal spoiled gradient - echo t1 - weighted sequences after 5 ( b ) and 35 ( c ) min show a progressive delineation and enhancement of lymphatic vessels ( white solid arrows ) ; it is clear the beaded appearance of lymphatics when compared to veins ( open arrows ) and their different enhancement kinetics ; furthermore precontrast venogram makes easier the subsequent distinction of the different structures vessels from veins merely by their morphology [ 27 ]  . 
after performing 3d heavily t2 - weighted sequence to depict the severity of lymphedema and a highresolution fat suppressed 3d spoiled gradient - eco ( 3d - spgr ) sequence after subcutaneous injection of gdbased mr contrast to image lymphatic vessels , they concluded the examination with an intravenous injection of gdbased - mr contrast to obtain an mr venogram by repeating the high - resolution 3d spgr - sequence . 
in our experience , lymphatic vessels cannot be distinguished from veins only by their appearance , because in 7 out of 30 patients ( 23.3% ) , their morphology is fundamentally similar ; hence , enhancement kinetics analysis is very helpful in distinguishing the different structures , since the curve trend generally diverges after 25min from the contrast agent subcutaneous administration . 
 moreover , we do not use heavily t2 - weighted sequences because this technique makes the distinction between real lymphatic vessels and edematous infiltration of soft tissues very difficult ; on the contrary , we prefer to perform a 3dssfp - balanced sequence before 3d gradient - echo t1 - weighted mrl , to evaluate not only the severity and distribution of lymphedema but also to provide a map of the venous system , thus simplifying distinction between veins and lymphatic vessels on post - contrast sequences and in addition reducing the examination time [ 9 , 11 ]  . 
furthermore , we found the subtraction technique very useful in identifying small lymphatic vessels ; clearly , this method can be invalidated by patient movements , as reported by mitsumori etal . 
 [ 28 ] ; in fact , the average examination time of 1h and 15min for the lower limb and 50min for the upper limb may result in patient discomfort , in particular the study of the latter , and requires patient cooperation and good general conditions , which are essential to the success of the exahowever , the limitation of the long execution time affects lymphoscintigraphy too , where it is even greater than mrl ( till 5h ) [ 29 ]  . 
 in planning lva treatment , the role of mrl is to localise 1 3 radiol med ( 2017 ) 122 : 918927 table 2 main mr findings for all the patients ( affected limb ) number of lymphatic vessels visualised number of patients 3 < 6 lymphatic vessels morphology straight tortuous honey - combing dermal backflow delay of drainage ( score ) lymph - node detection anatomical distribution of lymphedema epifascial epifascial and subfascial delay of drainage ( score ) : 0 no drainage , 1 substantial delay ( pelvic or axilla level > 60min or not reached ) , 2 slight delay ( pelvic or axilla level > 20min ) ; 3 no delay ( reached pelvic or axilla level < 20min ) that post - contrast sequences are fundamental , since lymphatic vessels visualised in this way have certainly , at least , a residual undamaged pump to drain the contrast agent ; on the contrary , t2 - weighted sequences do not provide information about vessels functionality . 
this statement is supported by the significant high number of lymphatic vessels visualised on post - contrast sequences at the distal part of the limb ( footanklecalf , handwristforearm ) than at thigh or upper arm , because of the destruction process of the smooth muscle cells and occlusion of lymphatics , which start at the proximal extremities and progresses towards the distal portion of the limb [ 30 ]  . 
in our population , only in one patient no clearly delineated lymphatic vessels were found on postcontrast images and surgery confirmed the absence of functional vessels , so anastomoses were not performed . although lva is a safe treatment , as the procedure is performed just below the surface of the skin , uncommon complications such as back flow of venous blood with thrombosis and anastomotic leakage are described . 
animal studies reported long - term ( 5months ) anastomosis patency of 80% for end - to - side compared to 47% for end - to - end anastomosis ; however , due to the small sample sizes and heterogeneity of the studies , these data may not be applied in humans [ 31 ]  . 
reported patency rate of about 75% for side - to - end anastomoses at 12months , evaluating them through indocyanine green ( icg ) fluorescence lymphography , even if these results are influenced by the lack of vessels detection when subcutaneous layer is too thick [ 32 ] ; moreover , the above - mentioned complications are usually asymptomatic so reliable prevalence data are unavailable . 
 however , it should be considered that a single anastomosis disfunction does not compromise patient clinical outcome , in case of multiple anastomoses , but it becomes relevant when 3 or less anastomoses for limb are performed . 
we found only one case of anastomosis leak in a symptomatic patient after a short follow - up ( 2months ) ; surgery confirmed mr finding and anastomosis was executed agaall the other patients were asymptomatic therefore mrl was not required after surgery . 
4 a , b a 63 - year - old woman underwent multiple lva because of a secondary lymphedema due to a previous surgery for pelvic cancer ; 3weeks after treatment she felt a severe pain on the dorsal aspect of her foot , where a focal swelling was clear upon clinical examination . 
mrl revealed a lymph leakage ( arrow head , b ) on the site of anastomosis between a pathological lymphatic vessel ( white solid arrows ) and dorsal venous arch of the foot ( open arrows , b ) ; surgery later confirmed the leak conclusion lymphatic vessels but especially to identify those patients with an intact lymph pump , where lva anastomosis can be worth ; in fact , lymph pump dysfunction is not directly related to the duration of edema and may not be clinically evident [ 30 ]  . 
the aim of this article is to provide radiologists who approach pmct imaging cases with some indications for a proper and correct interpretation of pulmonary findings , to avoid misleading forensic conclusions . 
particularly , the following issues will be addressed : pmct imaging of post - mortem changes of the lungs ; pmct imaging of pathological lungs [ ( a ) in thoracic trauma cases , ( b ) in cases without thoracic trauma ]  . 
finally , the possible pitfalls in interpretation of pmct imaging of the lungs will be also discussed . keywords post - mortem ct lungs high resolution computed tomography forensic lung aspiration * laura filograna laura.filograna@gmail.com 1 department ofradiological sciences , catholic university ofrome , largo a . 
gemelli 8 , 00168rome , italy institute offorensic medicine , forensic imaging andvirtopsy , university ofzurich , winterthurerstrasse 190 / 52 , 8057zurich , switzerland 3 present address : department ofdiagnostic imaging , molecular imaging , interventional radiology andradiation therapy , fondazione policlinico tor vergata , viale oxford 81 , 00133rome , italy introduction the lung is one of the most complex organs of the human body . 
it performs , together with the other components of the respiratory system , namely upper airways , central nervous system , chest wall , and the pulmonary circulation , a multitude of vital functions , first the respiratory . the functional complexity of the lungs is reflected in its structural layout , classically divided into three partitions ( interstitium , airways and vascular system )  . 
pathological changes in each one of these partitions cause many abnormal findings on pulmonary imaging that can provide an important clue to clinical diagnosis . post - mortem computed tomography ( pmct ) imaging has been widely introduced in the forensic investigations as a support to classical autopsy , also in paediatric cases [ 1 , 2 ]  . in the thoracic district , for example , pmct imaging has been already proved a valuable method of investigation in cases of sudden death due to acute haemopericardium , providing adjunctive results with respect to autopsy for conducting forensic conclusions about the challenging diagnosis of heart tamponade as the cause of death [ 3 ]  . as well as in clinical imaging , also in post - mortem imaging , the recognition and right interpretation of imaging abnormalities have extreme importance in the assessment of diagnostic conclusions . 
this is even truer for the lungs , which , because of their particular , complex structure , represent one of the organs most submitted to post - mortem changes , also in the early post - mortem period . 
the aim of this paper is to provide both forensic pathologists and radiologists , not jet expert in pmct imaging , but who start approaching forensic cases , with some indications for a better and correct interpretation of postmortem pulmonary imaging and for avoidance of pitfalls in conducing forensic conclusions . in vivo ct imaging ofnonpathological lungs a fundamental assumption to the interpretation of pulmonary pmct findings is the knowledge of the principles that regulate normal ct lung anatomy , as it appears in living patients ct examinations . traditionally , the lung layout has been divided into three partitions : interstitium , airways and vascular systethe lung functional parenchyma is the substance comprised between the core and the periphery of the secondary lobe , as defined by miller [ 5 ] , and consists on alveoli , capillaries , the smallest branches of the airways and pulmonary vessels , and the supporting intralobular interstitium . ct is normally unable to identify these structures themselves , but a greater opacity of the lung parenchyma contrasting with air can be appreciated . on this regard , it is important to underline that the attenuation value of pulmonary parenchyma is not homogeneously distributed within the lungs , and vary also if an expiratory or inspiratory scan is performed . 
in particular , it has been largely proved that an attenuation gradient is recognizable in non - pathological lungs , with an increase of density values in the dependent lung regions , both in inspiratory and in expiratory scans . 
it is due to regional differences in vascular distension and gas volume , which are dependent on gravity , pleural pressures and tension forces acting on the lungs . the lungs can be considered a balloon in a vacuum box that is the thoracic cage , which expands and contracts its volume during the respiratory acts . 
in the inspiration , by flattening of the diaphragm and uplifting of the anteriorly slanted ribs , the thorax cage , and for consequence also the lungs , increases their lengths , width , and depth . 
the result is an increment of the air volume in the lung parenchyma , and a decrement , but no abolition , of the ct attenuation gradient in lung cross section . 
it has been observed that the increase in lung attenuation of the dependent regions during expiration is greater than that occurred in non - dependent lung parts , independently of the position of the patient [ 6 , 8 , 10 , 11 , 13 , 14 ]  . 
 moreover , the expiratory opacity increase in lower lung regions in the supine position is greater than that in middle and upper lung regions , probably due to a greater decrease of air volume in the basal zones related to the more efficacy of the diaphragmatic movements , and to a greater basal blood volume . pmct imaging ofnonpathological lungs the knowledge of some changes affecting the lungs after death has to be considered the starting point for understanding of the pmct imaging of the lungs . most common post - mortem changes of the lungs in pmct , in the absence of known lung pathology , chest trauma , or massive body haemorrhage , are represented by an attenuation gradient with areas of grater opacity mainly of ground glass type , localized in dependent regions ( fig.1 ) [ 15 ]  . these dependent densities are explained as being an effect of regional differences in blood and air volume distribution caused by three events occurring after death : the formation of hypostasis , the cessation of the tension forces by respiratory muscles , and the pushing action of the diaphragm . when the circulation ceases , the blood settles in the capillary bed of the gravitationally dependent regions . 
this is the origin of hypostasis not only in the skin , but also in other tissues and organs , including the lungs . a dark bluish colour and a more accentuated congestion in the dependent portions of the pulmonary parenchyma are an almost constant finding on autopsy analysis of lungs in cases without massive haemorrhage . as well as hypostasis in the skin , distribution and characteristics of post - mortem pulmonary changes are dependent on the time since death and position of the body after death . 
the origin of this phenomenon , studied on an animal model [ 16 ] , has been explained due to a pressure gradient between pulmonary vasculature and the alveolar spaces and to an alteration of capillary permeability that increases with the passage of the time between the death and autopsy . 
in pmct scans , this corresponds to an increase of extent and density ( from ground - glass opacities to consolidations ) of the described attenuation gradient related to post - mortem changes ( fig.2 ) [ 17 ]  . the main theories advanced to explain the fixation of livores [ 1417 ] are discordant in defining the interval from death to the occurrence of true fixation of hypostasis , for some authors ranging from 6 to 8 up to 12 to 24h [ 18 , 19 ] and for others from 2 to 3 or 4 to 5days [ 20 , 21 ]  . 
1 pmct axial images of the thorax performed 10h after death : a an attenuation gradient with areas of grater density localized in dependent regions is recognizable at the level of inferior lung lobe bilaterally ; b the gradient densities , although present in both lung , show less extent in apical regions fig . 
3 pmct axial image at the hilar level of a body found lying in the prone position : this image shows two attenuation gradients localized , respectively , in anteriorly and posteriorly , the most evident localized in the posterior lung regions phenomenon could affect the distribution of the internal livores in the lungs . 
in particular , this is evident when two conditions occur : first the body lied in not supine position up to fixation of the hypostasis , second the body lied in supine position up to formation of additional hypostasis.indeed , in such cases , it can be evidenced a contemporary presence of gradient densities due to post - mortal changes both in dependent regions of the original position and of the supine position ( fig.3 ) [ 22 ]  . also the respiratory level at which a dead body settles in post - mortem period contributes to the formation of the attenuation gradient . 
also after death , it is caused by regional differences in gas distribution , in addition to changes in vascular and capillary bed , as already explained . on the other hand , the position of the diaphragm is another element influencing the air and blood volume distribution within the lungs . 
then , with the formation of putrefactive gas in the abdomen , which pushes the diaphragm up towards the thoracic cavity , this phenomenon could be also accentuated . 1 3 radiol med ( 2017 ) 122 : 902908 pmct imaging ofpathological lungs the correct recognition , identification and isolation of pulmonary pmct findings specific for post - mortem changes are easy often only in the absence of other damage , directly or indirectly influencing the anatomy or function of the pulmonary parenchyma . in these last conditions , in fact , the lung post - mortem changes may request differential diagnosis with other abnormalities resembling , or masking their pmct appearances . on the other hand , the presentation of these confounding alterations of the normal pattern of post - mortem lungs is really the most frequent in forensic cases . 
as stated above , the lungs are in fact an organ with a really complex structure and crucial functions , and for these reasons , they are involved with direct or indirect mechanism in many processes leading to death , thus presenting a great variety of imaging alterations . 
furthermore , the possibility of the absence of abnormalities related to post - mortem hypostatic changes in deaths due to traumatic injuries should be considered , because of the frequently associated occurrence of massive blood loosening ( fig.4 ) [ 16 ]  . pmct lung imaging ofthoracic trauma cases the main findings in post - mortem imaging of thoracic trauma are those characterizing contusions , lacerations , retrograde blood aspiration , hemoand / or pneumo - thorax . 
 their features on pmct scanning resemble completely their appearance in living patients imaging . in many cases , these alterations are associated , so that a clear distinction on pmct images is not always possible . 
 nevertheless , for convenience and clarity of exposition , they are described separately . lung contusions are defined as pulmonary injuries occurring after a blunt or penetrating trauma to the lungs , due to disruption for tear of capillaries or small blood vessels without interruption of alveolar walls . 
consequently , distinguishing isolated contusive areas related to blunt trauma in regions of greater opacity due to hypostatic phenomena and post - mortem changes , if there is a superimposition in location , could be really difficult . lacerations consist on disruption of alveoli , and can occur after blunt trauma for linear tears , or after penetrating trauma , for a rib fracture or bullets , knives , etc . 
5 pmct image of trauma lungs : the image shows rounded areas of ground glass opacity ( thin arrows , exemplar ) , close to lung lacerations ( bold arrow , exemplar ) due to blood aspiration . 
moreover , the presence of a hemothorax results in characteristic semilunar hyperdensities localized in dependent regions of the thorax that do not allow to easily discriminate the pathological status of the underlying pulmonary parenchyma ( figs.5 , 6 ) also by means of compression . 
also in clinical radiology , ground glass opacity is considered a nonspecific imaging pattern being the expression of minimal thickening of alveolar interstitium or of alveolar walls , or of a little amount of cells or fluids filling partially the alveolar spaces , representing , thus , either fibrosis , or inflammation . many are the diseases , in acute , subacute or chronic stage that can be associated in vita with ground glass opacity . 
 among those having an acute presentation are diffuse alveolar damage , acute interstitial pneumonia , acute respiratory distress syndrome or pulmonary oedema of various causes , pulmonary haemorrhage , atypical or viral pneumonias , etc . 
 among the pathologies with subacute or chronic symptoms and ground glass opacities are nonspecific interstitial pneumonia , desquamative interstitial pneumonia , hypersensitivity pneumonitis , lipoid pneumonia , alveolar proteinosis , etc . 
moreover , examples of pulmonary pathologies with a posterior distribution of ground glass opacities in initial or advanced stages are : usual and nonspecific interstitial pneumonia , scleroderma , pulmonary oedema , acute respiratory distress syndrome , hypersensitivity pneumonitis , lipoid pneumonia [ 24 ]  . 
thus , in the presence of the pmct finding of ground glass opacities posteriorly distributed , these in vivo pathologies should be considered in opposition to the diagnosis of normal post - mortem changes . as well as in clinical practice , the analysis of distribution and the knowledge of the clinical history may be useful to reach in many cases diagnostic conclusions [ 23 ]  . here , we describe some pulmonary abnormalities nontraumatic for the lungs in strict sense , but with forensic relevance . in particular , we refer for example to cases with pmct pulmonary alterations related to aspiration of material of variable nature , or to pulmonary oedema of variable origin . the assessment of pulmonary aspiration in cases of death is a main issue in forensic pathology . 
8 pmct images : the axial image a of a case of death by acute myocardial infarct shows ground glass localized in dependent regions of both lungs , associated with interlobular septal thickening . 
in the image b referred to a case of a man died by acute heart failure many areas of ground glass opacity and consolidations are visible another forensic relevant finding in pmct lung imaging is pulmonary oedema of cardiac or non - cardiac origin , which is a frequent source of alteration of post - mortem pulmonary imaging . 
pulmonary hydrostatic oedema may be caused , in fact , by acute heart failure of variable causes ; increased permeability oedema by drug or transfusion reactions , water aspiration , etc . ; mixed permeability and hydrostatic oedema by trauma of central nervous system , postpartum state , etc . ; permeability oedema with diffuse alveolar damage , consisting in ards , by toxic damage from pulmonary diseases , most commonly pneumonia , or from pathologies with extrapulmonary origin , like sepsis , or massive fat embolism . ante - mortem ct features of pulmonary oedema may resemble those of post - mortem changes . 
on the other hand , the presence of imaging alterations in scans obtained after death does not mean necessarily that the lungs were involved in any process with forensic relevance . for what previously discussed , when a radiologists or forensic pathologists approach forensic cases with the modern pmct techniques , above all in case of few experience in post - mortem pulmonary imaging , the following principles should be taken well in mind : ( a ) also non - pathological lungs may present in post - mortem period computed ct relievable abnormalities , exclusively related to normal post - mortem changes ; ( b ) some diseases involving directly or indirectly the lungs during the life in one or more stages of their evolution might resemble the pmct appearances of normal post - mortem changes ; ( c ) some forensic relevant processes involving the lungs can have a pmct presentation superimposable for distribution and appearance to the normal post - mortem changes of the lungs . our suggestions when facing with pmct imaging of the lungs for proper forensic conclusions are : ( 1 ) to search for the eventual presence of other pulmonary and thoracic abnormalities ; ( 2 ) to examine the whole - body images for the identification of all other extrapulmonary abnormalities ; ( 3 ) to consider the information about case circumstances and clinical history of the deceased . only a scrupulous investigation of all these factors together with a meticulous analysis of pmct lung abnormalities is undoubtedly the correct way for reaching the right interpretation of post - mortem pulmonary alterations . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent not - applicable to post - mortem examination . 
with computer assistance based on matlab programming , three features were extracted from rte , i.e. , the median hardness within peripheral gland ( pg ) ( hmed ) , the ratio of the median hardness within pg to that outside pg ( hratio ) , and the ratio of the hard area within pg to the total pg area ( har )  . 
 three rte features were all statistically higher in high - risk pca than in non - high - risk diseases ( p < 0.001 ) , indicating that the pgs in high - risk pca patients were harder than those in non - high - risk patients . 
when predicting high - risk pcas , the multiple regression achieved an area under receiver operating characteristic curve of 0.755 , sensitivity of 73.5% , and specificity of 71.0%. conclusions the elevated hardness of pg identified highrisk pca and served as an independent marker of high - risk pca . 
as a non - invasive imaging modality , the rte could be potentially used in routine clinical practice for the detection of high - risk pca to decrease unnecessary biopsies and reduce overtreatment . keywords prostate cancer ( pca ) real - time elastography ( rte ) transperineal biopsy transrectal ultrasound ( trus ) high - risk cancers tissue elasticity institute ofbiomedical engineering , shanghai university , room 803 , xiangying building , no . 
333 , nanchen rd , shanghai200444 , china 2 department ofultrasound , huashan hospital , fudan university , shanghai200438 , china 3 department ofurology , huashan hospital , fudan university , 4 department ofelectronic engineering , fudan university , shanghai200438 , china shanghai200433 , china introduction prostate cancer ( pca ) is the second highest cause of cancer death in males in developed countries , and the incidence and death of pca have been steadily increased in developing countries [ 1 , 2 ]  . 
however , the biopsies not only vol :  . ( 1234567890 ) 1 3 radiol med ( 2017 ) 122 : 944951 miss many significant pcas but also detect many insignificant pcas that do not require immediate treatment , resulting in overdiagnosis and overtreatment [ 5 , 6 ]  . 
in addition , the biopsies are associated with a rise in severe infectious complications because of the increased resistance to the preventive antibiotics , namely quinolones [ 7 ]  . the overtreatment of pca is partly due to the lack of noninvasive tools for identifying high - risk pca [ 8 , 9 ]  . 
real - time elastography ( rte ) is an imaging technique developed from ultrasound ( us ) for measurement of tissue hardness , which involves compression of tissues using the us transducer to generate tissue strains ( deformations ) and provides diagnostic information regarding the biomechanical properties of prostate [ 4 , 1113 ]  . previous studies employ various rte grading systems for qualitative discrimination between benign and malignant prostate diseases [ 4 , 1417 ]  . 
proposed a five - grade subjective scale based on the degree and distribution of strains on rte in relation to simultaneously displayed hypoechoic areas on b - mode us , where grade 3 or higher was taken as an indicator of a malignant tumour [ 17 ]  . 
proposed another five - point scoring system only including findings of hard areas in the peripheral gland ( pg , i.e. , peripheral zone ) without considering the inner gland findings [ 14 ]  . there are three drawbacks for these grading systems . 
third , the elasticity grades are generally scored by experienced radiologists and are not yet automated , which limits the interand intra - observer reproducibility [ 18 ]  . quantitative assessment of rte images with computer assistance is potentially valuable for more objective measurement of prostate hardness and thus may be useful for detection of high - risk pca . 
the purpose of this study was to examine the role of new quantitative rte features extracted with computer assistance on differentiation between high - risk pca and other prostatic diseases in the initial transperineal biopsy setting . methods patients a total of 103 patients with suspicious pca undergoing both rte and initial transperineal prostate biopsy were included in this retrospective study . 
they were scheduled for prostate biopsies because of an increased prostate - specific antigen ( psa ) level 4ng / ml , abnormal digital rectal examination ( dre ) , and / or abnormal transrectal ultrasound ( trus ) with hypoechoic lesions . 
 longitudinal elastograms were obtained from the center of the prostate to the bilateral sides in an interval of about 0.5cm by slightly compressing and decompressing prostate tissues using the probe . 
the eub - 7500 system provides dual - modality visualization of the prostate in real time with an elastogram on the left of the screen and a b - mode image on the right . 
the 10 - core biopsy consisted of standard sextant biopsy from apex to base , supplemented with two lateral cores from the mid - prostate and two cores from the transition zone . 
in patients treated with radical prostatectomy , the pathological results were based on whole - mount section histopathology . computerassisted quantification ofperipheral gland hardness a computer - assisted program was developed for quantification of peripheral gland hardness using matlab r2010 ( mathworks , natick , ma , usa )  . 
the elastogram shown in the eub - 7500 system is a composite colour image ( left in fig.1 ) displayed as a translucent colour image overlaying the greyscale b - mode image . 
subsequently , the hardness of the pg was quantified by three features , i.e. , the median of hue values within the pg ( hmed ) , the ratio of the median hue within the pg to that outside the pg ( hratio ) , and the ratio of the hard area within the pg to the total pg area ( har )  . 
details of computer - assisted quantification on elastography can be found in our previous studies [ 19 , 21 ]  . statistical analysis all statistical analysis was performed with matlab . 
 the damicos risk stratification method integrating psa , gleason scores and clinical staging was used to classify pca patients into high - , intermediateand low - risk groups of biochemical recurrence after local treatment [ 22 ]  . 
comparisons between highrisk and non - high - risk patients were performed by the chisquare test , t test and kruskalwallis test for categorical , normally distributed continuous and non - normally - distributed continuous data , respectively . a multiple regression model was used to identify markers for high - risk pca . 
sensitivity , specificity , accuracy and area under receiver operating characteristic curve ( auc ) were calculated for evaluating classification performance . results the basic characteristics of the patients are enumerated in table1 . 
the single feature still achieved an auc larger than 0.720 , and the four - feature combination achieved an auc larger than 0.750. discussion to confront the issue of overdiagnosis and overtreatment , the goal of pca detection should be to detect significant pca and to avoid cancer diagnosis in males who are at 1 3 radiol med ( 2017 ) 122 : 944951 low possibility of developing life - altering consequences of the disease [ 10 ]  . 
the most important finding in this study was that the elevated hardness of peripheral gland , quantified by hratio , hmed and har , identified high - risk pca and served as an independent marker of high - risk pca . 
 as a non - invasive imaging modality , the rte could be potentially used in routine clinical practice for detection of high - risk pca to decrease unnecessary biopsies and reduce overdiagnosis and overtreatment . our results on elastography were in agreement with those reported in previous studies [ 810 , 24 , 25 ]  . 
found a positive rte was an independent marker for detection of high - risk pcas in the primary biopsy setting [ 8 ] , and they also reported the combination of rte and prostate cancer gene 3 for identifying intermediateor high - risk pcas [ 25 ]  . 
found prostatic tissue stiffness in patients with low - risk pcas was generally decreased compared with those with intermediateor highrisk pcas [ 24 ] , and they reported the presence of suspicious elastography findings , i.e. , elevated stiffness , was an independent predictor of clinically significant pca [ 10 ]  . 
 our study confirms these findings and indicates that the computer - extracted quantitative rte features are valuable for detecting high - risk pcas and thus better identifying patients in need of prostate biopsies . in our experience , rte seems to be more reproducible and more user - friendly when patients are examined in the lithotomy position than in the left lateral position . 
compared with the lateral compression / decompression , the vertical compression / decompression is more easily controlled with an appropriate frequency and pressure using the probe , and thus it produces more stable images . 
 in addition , the sphincter is tighter when a patient is in the left lateral position than that when he is in the lithotomy position , which increases the difficulty of probe operation . psa has a limited specificity for differentiation between pca and bph , as well as between aggressive and indolent diseases [ 8 ]  . 
 for instance in our cohort , a bph patient reached a psa of 28.0ng / ml with a hypoechoic nodule found on trus , but the nodule was soft on rte . 
therefore , in patients with elevated psa , rte could have added value for characterization and risk stratification of prostatic diseases . in this study , the pca detection rate of systematic biopsy ( 47 / 103 = 45.6% ) and the proportion of high - risk pca patients in all pca patients ( 34 / 47 = 72.3% ) were both higher than in most other studies [ 8 , 26 ]  . 
population - based psa screening [ 27 ] has not been implemented in china , and thus many patients have not measured their psa level before they go to hospital due to symptoms . 
there might be more patients with larger tumours and at a later stage than in heavily screened populations in developed countries . in addition to the us imaging techniques , magnetic resonance imaging ( mri ) is also used in risk assessment of prostatic diseases . 
 demonstrated that patients with low suspicion lesions on multiparametric mri were more likely to have negative biopsies or low - grade tumours , suggesting that patients with low suspicion lesions on multiparametric mri have a risk of clinically significant disease low enough to justify undergoing active surveillance [ 29 ]  . 
however , compared to us , mri requires a sophisticated device and an interdisciplinary approach , takes more time to examine a patient and interpret images , and is less movable , less convenient and more expensive [ 24 ]  . 
thus , rte is a promising option for risk stratification of prostatic diseases in clinical practice . the hardness quantification was mainly confined to peripheral glands due to three reasons : ( 1 ) pca in the inner gland ( transition zone and central zone ) is rare ; ( 2 ) rte may produce stiffness artefacts with increasing depth of us penetration [ 30 ] ; ( 3 ) bph often occurs in the transition zone with calcifications , which could increases tissue hardness in this zone [ 31 ]  . 
our quantification method is consistent with the reported qualitative assessment approaches that exclude inner gland findings from rte [ 14 , 30 ]  . there are some limitations in the present study . 
second , we performed trus - guided systematic biopsies , and combining rte - targeted biopsies and systematic biopsies could increase the cancer detection rate in a future study [ 26 ]  . 
third , our computer - assisted quantification on rte requires manual delineation of the peripheral gland , and a fully automated segmentation technique would further increase the reproducibility of the quantification protocol . 
fourth , the rte measures strains ( deformations ) for indicating tissue elasticity , which is actually relative elasticity ; another sonoelastography modality called the shear - wave elastography can provide absolute elasticity measurement [ 10 , 24 ] , which might be more accurate for evaluation of prostate hardness and deserves future investigation and comparison with rte . in conclusion , the elevated hardness of prostate peripheral gland , quantified on rte , is found to be an independent marker for detecting high - risk pca . 
 prospective electrocardiographic gating with iterative reconstruction can reduce effective radiation dose . objectives to evaluate the diagnostic performance of lowkv ct angiography protocol with prospective ecg - gating technique and iterative reconstruction ( ir ) algorithm in follow - up of cabg patients compared with standard retrospective protocol . methods seventy - four non - obese patients with known coronary disease treated with artery bypass grafting were prospectively enrolled . 
all the patients underwent 256 mdct ( brilliance ict , philips ) ctca using low - dose protocol ( 100kv ; 800 mas ; rotation time : 0.275s ) combined with prospective ecg - triggering acquisition and fourthgeneration ir technique ( idose4 ; philips ) ; all the lengths of the bypass graft were included in the evaluation . 
a control group of 42 similar patients was evaluated with a standard retrospective ecg - gated ctca ( 100kv ; 800 mas ) .on both ct examinations , rois were placed to calculate standard deviation of pixel values and intra - vessel density . 
furthermore , based on the recent guidelines , ccta using 64 - slice ct is considered appropriate for the evaluation of symptomatic patients with prior coronary bypass surgery [ 13 ]  . despite its diagnostic performance , ccta still has some limitations . 
in an average of all age groups , an estimated additional lifetime risk for developing cancer after 10msv exposure is approximately one in 2000 [ 14 ] ccta study for cabg follow - up ; mdct exposes patients to a much higher radiation dose , approximately twice than cardiac ct angiography [ 15 , 16 ]  . recently , prospectively electrocardiogram ( ecg ) - gated axial ( pga ) ccta allowed a marked reduction of the radiation dose exposure as compared to retrospectively ecggated helical ( rgh ) ccta [ 1719 ]  . 
furthermore , new ct scanners are equipped with iterative reconstruction ( ir ) algorithms that allow a further reduction of the radiation dose without theoretically affecting the image quality , especially if used in association with a low - kv scanning protocol [ 2022 ]  . the purpose of our study was to evaluate the diagnostic accuracy and the radiation dose exposure of ccta combined with pga technique on 256 mdct scanner , using a low - kv setting associated with hybrid ir technique ( idose4 )  . materials andmethods study population a total of 116 consecutive patients who underwent ccta for evaluation of graft patency following cabg surgery ( mean 11.6years ) were prospectively evaluated after informed consent was obtained : 74 patients with heart rate < 65 beats / min underwent a pga - ccta , whereas 42 patients underwent a standard rgh - ccta when heart rate was higher than 65 beats / min despite the administration of b - blockers or when there was a clinical request for cardiac functional evaluation . 
 patients were excluded from the study when the following conditions were reported : ( i ) renal insufficiency ( glomerular filtration rate < 30ml / min / 1.73 m2 ) , ( ii ) non - sinus rhythm , ( iii ) high heart rate and contraindications to beta - blocking medication , ( iv ) hemodynamic instability , ( v ) body mass index ( bmi ) > 30kg / m2 , ( vi ) pregnancy , and ( vii ) history of allergy to iodinated contrast agent . patient demographic data , heart rate ( hr ) , body mass index ( bmi ) , and effective radiation dose information were obtained at the time of image acquisition . 
all the patients provided informed consent for the procedures . ccta protocol withprospective ecggating all ccta examinations were performed using a 256 - slice single - source ct scanner ( brilliance ict , philips , eindhoven , the netherlands ) with the following acquisition protocol : 100kvp , 800mas , rotation time of 275ms , temporal resolution of 135ms , collimation of 1280.625mm in a 256 - slice acquisition mode with z - flying focal spot , and scan field of view ( fov ) of 25creal - time arrhythmia management capability was used , enabling the x - ray acquisition to be paused upon the detection of ectopy during a pga scan and then to be resumed at the same axial location once normal sinus rhythm has returned . 
each scan sequence included a scout scanogram , unenhanced ct ( to correct plan the scan volume coverage ) , and a coronary ct angiogra if the patients heart rate exceeded 65 beats / min , i.v. 
betablocking medication ( 515mg metoprolol tartrate , seloken , astrazeneca uk limited , cheshire , uk ) was administered just before the examination , unless contraindicated . a dual - headed injector ( stellant d ; medrad , warrendale , pa ) was used for all exams . 
ccta was performed after administration of a bolus of 90ml of iomeprol ( iomeron 400 , bracco , milan , italy ) at a flow rate of 4.5ml / s , followed by a 50ml saline chaser ( the cm volume injected was the same of the rgh to compare the diagnostic efficacy of employed protocol )  . 
a region of interest ( roi ) was placed in the ascending thoracic aorta and image acquisition was automatically initiated once a selected threshold [ 120 hounsfield units ( hu ) ] had been reached with bolus tracking . 
ccta was performed during an inspiratory breath hold at a slice thickness of 0.625mm from the thoracic inlet to the cardiac apex , in cranial - to - caudal direction . raw images were then reconstructed using hybrid iterative reconstruction technique ( idose4 ) , with a slice thickness of 0.9mm , reconstruction increment of 0.45mm , and cardiac standard filter ( cb )  . ccta protocol withretrospective ecggating in patients with heart rate superior to 65bpm , rgh technique was performed , with 100 kvp , 800 mas , and pitch set at 0.18 ; images were initially reconstructed at mid - diastolic phase ( 78% of rr interval ) of the cardiac cycle . 
curved reformats were generated for each bypass graft in all patients , including whole graft course , especially distal anastomosis together with curved - multiplanar reconstruction ( cpr ) and maximum intensity projection ( mip ) of short - axis , 2 - chamber , and 4 - chamber views . the image quality of each graft was independently evaluated by two radiologists with 4 and 11years of experience in cardiovascular imaging . 
the two readers knew the numbers , types , and sites of the anastomoses of the grafts but were blinded to the radiological ( i.e. , protocol employed ) data , to the rating of the other reader , and also to the ecg - gating technique used . the bypass patency was first evaluated , so if a graft was completely occluded , it was excluded from the qualitative and quantitative evaluation . image quality of the graft at ccta was evaluated for each segment of the graft with a 4 - point grading scale , as previously reported [ 9 ] ( fig.1 ) : 4 was regarded as excellent image quality ( no stair - step artifacts , no motion blur , surrounded by low - attenuation fat ) , 3 as good ( minor motion artifacts or stair - step artifacts affecting < 25% of the vessel diameter ) , 2 as moderate ( noticeably blurred vessel , stairstep artifacts affecting 2550% of the vessel diameter ) , and 1 ( poor ; inadequate delineation between the vessel and the surrounding tissue , severe blurring , or stair - step artifacts affecting > 50% of the vessel diameter )  . furthermore , rois were drawn at the proximal , middle , and distal tract of bypass grafts measuring mean ct - attenuation values ( hu ) , image noise ( considered as the standard deviation of the mean ct - attenuation values ) , and signalto - noise ratio ( snr )  . finally , the two radiologists repeated the evaluation on the native coronary arteries and their main branches ( lmca , lad , lcx , om ; rca , pda , and pl ) , with the same subjective score and measuring the intra - vessels density . 
from the ecg data obtained during the scan , we calculated mean heart rate ( hr ) and heart rate variability ( hrv ) as the sd of the hr during ct angiography . 
the mannwhitney u test was used to evaluate differences between pga group and standard rgh group in terms of image quality , mean attenuation values of bypass lumen ( hu ) , snr , and radiation dose exposure ( dlp )  . 
a total of 172 grafts in the pga group ( 74 arterial grafts and 98 venous ) and 88 in the rgh group ( 40 arterial grafts and 48 venous ) were considered . a total of 564 native coronary arteries were successfully evaluated : 423 coronary arteries in the pga group and 141 in the rgh group , while 248 were excluded because too calcific or occluded . the clinical characteristics of cabg in each pga group and rgh group are summarized in table2 . 
the proportion of each type of bypass graft and supplied coronary artery to graft was not significantly different between the two groups . ct scan andradiation dose the scan time during ccta with pga technique was significantly longer than that with rgh technique ( p = 0.011 ) , with a mean duration time of 7.51.9s in comparison to 4.40.6s. 
in particular , dlp was 27431mgycm in the pga group and 1244173mgycm in the rgh group , respectively , while the effective radiation doses were 3.830.43msv for pga group and 17.412.42msv for rgh group , respectively . 
higher snr was found in pga group in comparison to rgh group for all the evaluated sites ( proximal anastomosis , middle bypass course , and distal anastomosis ) , with no statistically significant p values . we did not found any significant difference ( p value > 0.05 ) in the quantitative evaluation of image quality between arterial and venous grafts in both of the study groups ( i.e. , arterial - pga vs arterial - rgh )  . subjective image quality the image quality scores gave by the two readers for the two techniques are listed in table6 . 
 image example from study group ( left ) and control group ( right ) of 3d volume rendering , curved planar , and centerline reconstructions of left internal mammary artery graft on left anterior descending artery in two different patients with similar body mass index fig . 
furthermore , 1 3 radiol med ( 2017 ) 122 : 893901 several dose reduction tools are actually integrated in these new ct scanners , including hardware components as dynamic helical collimator , adaptive axial collimator and tube - current modulation , and software post - acquisition improvements as iterative reconstruction algorithms [ 27 ]  . our study was designed to obtain the best image quality with the lowest effective dose , using all dose reduction strategies available with our scanner . 
we used idose4 ( level 4 ) , because it is routinely applied in clinical examination at our hospital and it was the best model to reduce the tube - current time product according to technical instructions . idose4 is a fourth - generation hybrid ir algorithm introduced by philips healthcare ( cleveland , oh , usa )  . 
with idose4 , the iterative processing is performed in both the projection and image domains , through an iterative diffusion process ; the noisy data are penalized and edges are preserved . 
the next major component of the idose4 algorithm deals with subtraction of the image noise while preserving the underlying edges associated with true anatomy or pathology . currently , pga technique has been referred to be a very effective method to reduce the radiation dose for the diagnosis of native coronary artery disease [ 17 , 2830 ]  . in a recent study , chazen etal . 
in comparison with these studies performed with 64 - mdct scanners , our results are similar in terms of dose reduction percentage ( 78% ) between pga and rgh protocols . recently , lee et al . 
interestingly , the authors found that the percentages of good and excellent image qualities were 98.3 and 91% in pga and rgh groups , respectively , better than those in the documented results ( 8090% ) using 64 - slice ct . 
the same authors stated that pga might be particularly favorable for 256 - slice ct due to its higher temporal resolution and wider z - axis coverage as compared to 64 - slice ct , reducing incidence of ectopy , respiratory intolerance , and motion artifacts owing to the continuous table movement in rgh acquisition . as for image quality , our results are in line with the aforementioned paper , as we obtained similar snr ratio in pga group in comparison to rgh group but considering the overall radiation dose delivered to the patients , we obtained lower values ( 3.830.43msv for pga group and 17.412.42msv for rgh group )  . these findings are consistent with the integration of pga protocol with 100 kv tube current and iterative reconstruction . 
since absorbed radiation dose varies approximately with the square of tube voltage , a reduction of voltage from 120 to 100kv theoretically would reduce dose by 40% , due to reduced number and lower mean energy of the photons . 
however , lowering the kilovoltage will also increase the image noise as fewer x - ray photons reach the detectors . nevertheless , our results demonstrate that the diagnostic image quality was preserved ; this is in part due to the fact that iodinated contrast is more conspicuous using low - kv imaging due to an increase in peak iodine photon absorption at 100kv , resulting in an increase in the signal - to - noise ratio [ 34 ]  . furthermore , the new iterative reconstruction technique used ( idose4 ) has already been proven to improve image quality on 256 - slice multidetector pga - ccta , providing equivalent or better image quality compared to routine - dose filtered back projection reconstruction using reduced tube output [ 20 ]  . some limitations of our study should be taken into account . 
second , coronary artery angiography ( cca ) , that represents the standard evaluation method , was not performed in all of the patients and we did not directly correlate the imaging findings to the cca results . 
in conclusion , this study shows that , in non - obese patients ( bmi < 30kg / m2 ) with hr < 65bpm , the ccta study protocol with prospective ecg - gating , 100kv tube voltage combined with iterative reconstruction algorithm , leads to a significant reduction of dose ( up to 78% ) in comparison with retrospective ecg - gating ccta , representing a reliable and effective ccta approach , offering high diagnostic quality images , in evaluating cabg , comparable to those of routine standard protocol . compliance with ethical standards conflict of interest the authors of this manuscript declare no relationships with any companies , whose products or services may be related to the subject matter of the article . 
the aim of this cross - sectional study was to investigate the associations between the structural findings on mri ( bone marrow lesions [ bmls ] , synovitis , cartilage defects , meniscal lesions ) , x - ray examination ( kellgren and lawrence [ k / l ] grade ) , and psychological aspects with pain in patients with knee osteoarthritis ( koa )  . methods in this study , patients with symptomatic koa were included . 
mri was performed with a 1.5 t whole - body scanner ; the presence of the following alterations was collected : bmls , infrapatellar fat pad ( ifp ) synovitis , condral defects , and meniscal tears . 
in multiple regression analyses , womac knee pain was significantly associated with the volume of the bmls ( p = 0.0001 ) , ifp synovitis ( p = 0.0036 ) , and sf - 36 mcs ( p = 0.0001 ) , but not with k / l grades , meniscal lesion score , cartilage defect , sex , age , educational level , disease duration and bmi . conclusion in symptomatic koa patients , mri features , such as larger bmls , ifp synovitis , and high levels of psychological distress , are associated with greater knee pa confirmation of these findings in the prospective studies of koa is needed . keywords magnetic resonance imaging knee osteoarthritis pain psychological distress x - ray introduction osteoarthritis ( oa ) is the most prevalent musculoskeletal complaint worldwide , affecting 7.540% of the population by the age of 65years [ 13 ]  . 
in italy , the overall prevalence of symptomatic oa is estimated as 8.95% , and knee is the most frequent site involved , with a prevalence of 5.39% ( 95% ci 3.417.99 ) [ 4 ]  . 
the disease process includes progressive degradation of articular cartilage with concomitant changes in the bone underneath the cartilage , including development of marginal outgrowths ( osteophytes ) , abnormal increase in density and thickness of bone ( bony sclerosis ) , and alterations in trabecular bone structure and bone marrow lesions ( bmls )  . 
these tissues include synovium , which may reveal modest inflammatory infiltrates ; ligaments , which often become lax ; menisci , which may present traumatic and degenerative lesions ; and bridging muscles , which become weak [ 10 ]  . radiological assessment is widely used for the diagnosis of the structural severity of koa , for outcome evaluation in epidemiological studies and in clinical trials of structure - modifying drugs [ 11 ]  . 
however , in cross - sectional studies , radiological changes are not strongly related to the severity of knee joint pain or disability , while a weak correlation between changes in clinical parameters and changes in radiological signs had been demonstrated in longitudinal studies [ 11 ]  . 
furthermore , a major limitation of conventional radiology is the inability to detect early and subtle oa changes . in this context , magnetic resonance imaging ( mri ) is a more appropriate tool , and has the capability to visualize all the structures within the knee joint , including the soft tissues [ 12 ]  . 
reported that in persons with koa , or at risk of koa , a growth in the size of bmls ( seen on knee mri ) is related to the contemporary onset of knee pain [ 14 ]  . 
suggested that knee pain is independently associated with both full and non - fullthickness medial tibial chondral defects , bmls , but not with radiographic koa , expanding our understanding of knee pain in older adults [ 15 ]  . 
other mri studies showed a connection between signal alterations in hoffas fat pad ( or infrapatellar fat pad [ ifp ] ) and knee pain [ 16 ]  . the aims of this cross - sectional study are to describe the associations between the structural findings on mri ( bmls , ifp synovitis , cartilage defects , meniscal lesions ) , x - ray examination ( kellgren and lawrence [ k / l ] grade ) [ 17 ] , and psychological aspects with pain in patients with koa . methods study population this is a cross - sectional study , realized over a 6 - months period , including subjects referring to the department of rheumatology of the polytechnic university of the marche ( jesi , anconaitaly )  . 
the inclusion criteria were the following : an age 50years ; a diagnosis of koa , according to the american college of rheumatology criteria [ 18 ] : the presence of unilateral or bilateral knee pain > 30mm ( knee discomfort on most days for at least one month in past 12months ) measured by the visual analog scale ( vas 0100mm ) ; tibiofemoral oa on posterioranterior weightbearing semi - flexed knee radiographs ( k / l grade 2 ) ; and a clinical examination confirming knee pain or discomfort referable to the knee joint [ 17 ]  . 
exclusion criteria were represented by : a history of a previous knee injury requiring non - weight - bearing treatment for > 24h or surgery ( including arthroscopy ) ; a history of any arthritis ( such as chronic inflammatory arthritis , gout , and calcium pyrophosphate dihydrate deposition disease ) diagnosed by a rheumatologist ; and any contraindication to mri ( including claustrophobia )  . for each patient , weight ( kg ) and height ( m ) were collected to determine the body mass index ( bmi )  . knee selection for each patient , one knee was identified . 
if both knees were eligible , the choice concerned the knee with a greater western ontario and mcmaster universities osteoarthritis index ( womac ) pain subscale score [ 19 ]  . 
all patients were examined by the same rheumatologist . patientreported outcome measures the koa symptoms and the impact on quality of life were assessed using the womac scale and the medical outcomes study sf - 36 health survey ( sf - 36 ) [ 19 ]  . 
in this study , the italian womac was used in its vas format , and all 24 items are rated by the subject on a 100mm vas ranging from 0 ( indicating no pain , stiffness , or difficulty ) to 100 ( indicating extreme pain , stiffness , or difficulty )  . 
the range of the womac scores is pain ( 0500 ) ; stiffness ( 0200 ) , and function ( 01700 ) [ 19 ]  . the sf - 36 questionnaire is a generic instrument exploring general health . 
scores are summarized into eight scales , each of which measures a health domain : physical functioning 1 3 936 radiol med ( 2017 ) 122 : 934943 ( pf ) , role functionphysical aspect ( rp ) , bodily pain ( bp ) , general health perception ( gh ) , vitality ( vt ) , social functioning ( sf ) , role functionemotional aspect ( re ) , and mental health ( mh ) [ 20 ]  . 
the originators of the sf - 36 have developed algorithms to calculate two psychometrically based summary measures : the physical component summary scale score ( pcs ) and the mental component summary scale score ( mcs ) [ 21 ]  . 
the standing weight - bearing anteriorposterior ( ap ) view was used to assess the medial and the lateral tibial femoral joints and a skyline view of the knee to assess the patello - femoral joint . 
the x - rays were then assessed independently using a standardized scoring sheet and also be graded according to the k / l classification [ 17 ] by an experienced musculoskeletal radiologist ( mcwith 15years of experience in musculoskeletal imaging ) , and by an experienced rheumatologic reader ( fs ) , blinded to the clinical and mri results and to each other . 
intraobserver repeatability was assessed in a randomly selected sample of 46 radiographs ( 20 right and 26 left knees ) with a weighted k statistics of 0.821. mri measurements an mri scan of the selected knee was performed in each patient , with a 1.5 t whole - body scanner ( philips achieva 1.5 t ) , using a commercial transmit - receive extremity coil . 
 [ 22 ] : ( 1 ) axial t1 - weighted spin echo ( se : 700 / 11 [ tr msec / te msec ] , 20cm field of view [ fov ] , 5mm / 1mm [ slice thickness / interslice gap ] , 256~192 matrix , frequency encoding [ fe ] anteriorposterior , one excitation ) , ( 2 ) coronal t1 - weighted se ( 600 / 11 , 16cm fov , 4mm / 0.5mm , 256~192 , fe superiorinferior , two excitations averaged ) , ( 3 ) sagittal t1 - weighted se ( 600 / 11 , 16cm fov , 4mm / 0.5mm , 256~192 , fe anteriorposterior , two excitations averaged ) , ( 4 ) sagittal t2 weighted fast spin echo ( fse : 2500 / 90 ; echo train length ( etl ) of eight ; 14cm fov , 4mm / 0mm , 256~192 , fe superiorinferior , two excitation averaged ) with fat suppression ( frequency - selective presaturation ) , ( 5 ) and sagittal fat suppressed t1 - weighted three - dimensional ( 3d ) spoiled gradient echo ( fs - 3dspgr : 58 / 6 , 40 flip angle , 14cm fov , 256~128 matrix , 60 contiguous 2 - mm slices covering all articular cartilage plates in the knee , fe , superiorinferior , one excitation , frequency - selective fat saturation , superiorinferior saturation bands to minimize pulsation artifacts )  . 
subchondral bmls were assessed on the t2 - weighted with fat suppression images and defined as discrete areas of increased signal adjacent to the subcortical bone at the lateral , medial femur and / or tibia [ 24 ]  . 
 given that the results of previous studies have suggested that the size of bmls is associated with pain [ 25 ] , it has been focused on the volume of the lesion as our measure of bmls . 
images were reconstructed and analyzed by osirix md 7 , a dicom software viewer ( osi - rix md version 7 , 64 - bit format ) , on a mac mini ( 2.8ghz intel core 2 duo desktop computer , 16gb random - access memory ; apple computer , cu - pertino , ca , usa ) running mac operating system osx 10.12.2. 
the total segmented volume of bmls was reported in cubic centimeters ( cm3 )  . one radiologist ( mc ) , and one rheumatologist ( fs trained in mri interpretation ) , blinded to both the case / control status and clinical data , evaluated independently of each other the same mris . 
1 example of volumetric analysis of bone marrow lesion through image processing by osirix on the semiautomatic t2 - weighted with fat suppression mri 1 3 radiol med ( 2017 ) 122 : 934943 areas of hyperintensity within hoffas fat pad . 
meniscal lesions were graded in medial and lateral menisci separately based on a combined whole - organ magnetic resonance imaging score ( worms ) scoring system from grade 0 to 2 based on both the sagittal and coronal images [ 22 ]  . 
image shows a effusion at the suprapatellar region and mild signal alterations within hoffas fat pad representing synovitis on non - enhanced mri ( grade 1 ) ; b focal thickness chondral loss at the medial tibial femoral joint without bone marrow lesion . 
 this image also shows effusion with moderate signal alterations within hoffas fat pad ( grade 2 ) ; c marked signal alterations within hoffas fat pad representing synovitis ( grade 3 )  . 
partial thickness chondral loss with subcondral bone marrow lesion of the medial tibial plateau , popliteal cyst , prepatellar bursitis and deep infrapatellar bursitis can also be observed 1 3 938 fig . 
3 coronal t1 ( a ) and t2 - weighted fat sat ( b ) mr images show partial thickness chondral loss with subcondral bone marrow lesion of the medial tibial plate radiol med ( 2017 ) 122 : 934943 independently associated with knee pain ( by womac pain subscale )  . 
age , gender , disease duration , educational level , bmi , and k / l grades were examined as potential confounders based on the significant associations with mri findings . 
table1 summarizes the demographic data as well as the characteristics of all subjects with pain scores , mri and x - ray findings . for the analyses of the present study , we employed only womac pain score and sf - 36 mcs scale score . 
subchondral microfractures , bone stretching with elevation of periosteum due to osteophyte growth , bone remodeling and repair , bmls , and bone angina caused by decreased blood flow and elevated intraosseous pressure are believed as bone - related causes of pacentral factors can deeply modulate the pain perception setting the gain in a chronic disease such as koa . 
interestingly , knee pain was significantly associated with larger bmls , ifp synovitis , and sf - 36 mcs , but not with k / l grades , meniscal lesions , cartilage defects , sex , age , educational level , disease duration , or bmi . 
bmls seem to play an integral if not pivotal role in the symptoms that derive from koa , and mri is the only technique to visualize bone marrow edema [ 25 ]  . 
 first reported that bmls were found in 77.5 and 30% of oa subjects with and without knee pain , respectively , and that large lesions were present almost exclusively in those with knee pain [ 25 ]  . 
other experiences about bmls have been performed mostly in subjects with oa , with reported prevalences ranging from 66 to 91.1% in subjects with symptomatic koa [ 24 , 31 ]  . 
one likely source that remains understudied is that of intraosseous hypertension [ 31 ]  . the volume of bmls was calculated by a semiautomatic image processing ( osirix )  . 
 [ 43 ] recently employed a volumetric measurement of bmls using a modified version of the method originally suggested by schmid [ 41 ]  . synovitis is a frequent detectable feature of koa which may predict other structural changes , even in patients without radiographic evidence of oa [ 44 ]  . 
since the ifp is extensively innervated , the ifp is exquisitely sensitive as are the anterior synovial tissue and capsule 1 3 radiol med ( 2017 ) 122 : 934943 [ 46 ]  . 
studies separately assessing and investigating signal alterations in ifp and joint effusion on non - contrast - enhanced mri images gave controversial results : some indicated that effusion was associated with pain or cartilage loss , while signal alterations in ifp were not [ 49 , 50 ]  . 
 crema and colleagues , in a study using contrast - enhanced mri images , demonstrated that pain is associated with peripatellar synovial thickness and not with signal alterations in ifp itself [ 52 ]  . 
described that perfusion variables observed using dynamic contrast - enhanced ( dce ) mri , reflecting the intensity of inflammation in the ifp , were associated with pain severity in koa [ 53 ]  . as already mentioned , the psycho - affective sphere is strongly impactful in koa . 
central pain sensitivity plays an important role in pain severity among patients with knee oa [ 10 ] , and psychosocial factors account for some of this variance in pain and other symptoms [ 54 , 55 ]  . 
the level of disability experienced in patients with koa showed to correlate more accurately with psychological involvement than with radiographic scores [ 57 ]  . there are some limitations in the present study that have to be mentioned . 
 secondly , the degenerative findings on patients with koa were not compared to an ageand sex - matched control group of asymptomatic subjects and , therefore , the crucial imaging findings responsible for the clinical symptoms could not be isolated . 
however , as of today , in the majority of large epidemiologic studies , contrast has not been used for assessing synovitis , because of the potential toxicity involved with the intravenous administration of contrast agents and the associated costs . 
finally , the difficulty to assess the cross - sectional relationship between mri findings and knee pain has recently been pointed out , demonstrating the fluctuating nature of bmls and knee pain , with the latter dependent on the former . 
longer follow - up is needed to fully evaluate the importance of these oa findings on mri for long - term clinical outcomes , such as the development of persistent pain . conclusions this study presents a comprehensive comparison of radiographicand mri - based structural findings in a cohort of koa patients , who constitute a sound proportion of all koa patients . 
our results suggest that knee pain is independently associated with mri features , such as larger bmls , ifp synovitis , and high levels of psychological distress , but not with radiographic knee oa , expanding our understanding of knee pain in older adults . 
the findings have the potential to be translated towards developing targeted therapies to prevent the development of koa . compliance with ethical standards conflict of interest the authors declare that they have not conflict of interests . ethical approval all applicable international , national , and institutional guidelines for the care and use of animals were followed . 
finally , the image classification of die - punch fracture was formulated . results according to the imaging features of die - punch fracture , it was divided into four types : type i ( dorsal type , 15 cases ) , type ii ( volar type , 8 cases ) , type iii ( splitting type , 10 cases ) , type iv ( collapsed type , 12 cases )  . 
the misclassification rate of x - ray was 15.6% ( 7 / 45 ) and the missed diagnosis rate was 11.1% ( 5 / 45 )  . conclusions ct examination could accurately diagnose die - punch fracture and perform preoperative image classification . keywords die - punch fracture x - ray ct image classification introduction die - punch fracture of intermediate column of the distal radius is a special intra - articular fracture . 
it is caused by the longitudinal violence transmitted to the lunar bone and crushed the lunate articular surface of distal radius ( lunate fossa ) , so it is also known as lunate bones stamping fracture [ 15 ]  . 
according to the three - column theory of distal radius fractures proposed by rikli and regazzoni [ 6 ] , ulnar half of distal radius which consists of lunar bone and sigmoid notch is called intermediate column . 
the intermediate column is the main bearing surface and load transfer hub of the wrist , which plays a key role in the treatment of distal radius fractures [ 7 ]  . 
at present , the relative literature reports are relatively rare ; especially the imaging findings and types of die - punch fracture have not been reported . this study retrospectively analyzed the imaging findings and clinical data of 45 cases with die - punch fracture in our hospital from may 2010 to october 2016 , and combined with the literature and clinical requirements to summarize . 
999 liangxi road , wuxi214062 , jiangsu , china from may 2010 to october 2016 , we screened 45 patients who were admitted in our hospital and met the inclusion criteria for die - punch fractures of the distal radius . 
 all procedures performed in studies involving human participants were approved by the ethics committee of wuxi hand surgery hospital , and in accordance with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
all patients received written informed consent . selection criteria diagnostic criteria : it is a lateral ulnar fracture of the distal radius caused by lunar bone crushing the lunate articular surface of distal radius . exclusion criteria : ( 1 ) fractures caused by simultaneously crushing ulnar half of distal radius and radial half . 
the centerline of the anteroposterior projection is aimed at the midpoint of the ulnar styloid process , and the centerline of lateral projection is aimed at the radial styloid process . 
projection conditions : tube voltage 55kv , tube current 5mas , and focal distance 90cm . ct inspection equipment is the ge 64 row spiral ct ( optima 660 , us )  . 
conventional reconstruction layer thickness and layer spacing is 2.5mm , thin layer reconstruction layer thickness and layer spacing is 1.0mm , fov is 145mm145mthe main image post - processing methods are multi - planar recombination ( mpr ) and volume reproduction ( vr )  . imaging type method the imaging findings of die - punch fractures were examined by two senior diagnostic radiologists with double blind method . 
the classification criteria developed in this study was as follows : type i ( dorsal type ) , referred that the fracture line was only located on margo dorsalis of articular surface of ulnar half of distal radius , and margo volaris had no fracture . 
type ii ( volar type ) , referred that the fracture line was only located on margo volaris of articular surface of ulnar half of distal radius , and margo dorsalis had no fracture . 
type iii ( splitting type ) , referred that margo volaris and margo dorsalis of articular surface of ulnar half of distal radius on sagittal plane all had fracture , and with varying degrees of separation , but no obvious articular surface collapse or crush . 
type iv ( collapsed type ) , referred that articular surface of ulnar half of distal radius had collapsed fracture , collapsed depth 2.0mm , and fracture line was located on the center or in margo volaris and ( or ) margo dorsalis , i.e. , in any one of type iiii , when articular surface step distance 2.0mm , fracture type was classified as this type . 
type ii ( volar type ) in eight cases , and the fracture line was located on margo volaris of articular surface of ulnar half of distal radius and without fracture in margo dorsalis ( fig.1 , shows the x - ray , fig.1 shows the ct scan )  . 
type iii ( splitting type ) in ten cases , and margo volaris and margo dorsalis of articular surface of ulnar half of distal radius all had fracture and 1 3 930 radiol med ( 2017 ) 122 : 928933 fig . 
type ii fracture ( volar type fracture ) without no obvious collapse on articular surface ( fig.2 , shows the x - ray , fig.2 shows the ct scan )  . 
in 45 cases , x - ray examination of 5 cases was negative ( table1 )  . shows the x - ray , image diagnosis results andcomparison 100% , and the classification results of die - punch fracture were completely consistent ( table2 , kappa = 1 )  . 
the reports of x - ray examination for five cases were false negative ( 5 / 45 , missed diagnosis of type i in two cases and type ii in three cases ) , and the missed diagnosis rate was 11.1%. 
the concordance rate of ct diagnosis was discussion because of the nature of the injury , the position of the injury and the patients bone condition , die - punch 1 3 radiol med ( 2017 ) 122 : 928933 fig . 
 type iv fracture ( collapsed type fracture ) table 1 diagnosis results of x - ray plain film and ct of distal diepunch fracture of distal radius imaging examination type i type ii type iii type iv total x - ray plain film 15 cases of type i ( dorsal type )  . 
for example , ao / saif classification method [ 9 ] and rayhack classification method [ 10 ] were mainly used for the classification of distal radius fractures [ 11 ]  . 
thus , the type of fracture reported in this paper is more comprehensive . the lunate articular surface of radius accounted for 46% of the contact surface of wrist joint , greater than the scaphoid articular surface and triangular fibrocartilage surface [ 13 ]  . 
the lunate articular surface reduction is not only related to the coordination of the radiocarpal joint , also affect the stability of distal radioulnar joint [ 7 ] , so the middle column fractures play a key role in the curative effect of distal radial fractures . 
in recent years , many researchers believed that intra - articular fracture of distal radius ( displacement > 12mm ) should be received surgical treatment to meet the maximum the anatomic reduction and fixation , reduce the incidence of traumatic arthritis and benefit the recovery of joint function [ 1421 ]  . 
the reports of x - ray examination for five cases were false negative ( 5 / 45 ) , and the missed diagnosis rate was 11.1% 1 3 932 radiol med ( 2017 ) 122 : 928933 the choice of surgical incision and reduction and internal fixation often requires reference to the fracture site and the mechanical mechanism of fracture [ 22 , 23 ]  . 
the classification in this study reflected the fracture site and the mechanical mechanism of fracture , which could provide a good reference for surgical treatment of die - punch fracture . according to the traditional work experience [ 23 , 24 ] and the die - punch fracture classification in the study , type i fracture should choose dorsal incision in clinical operation , so the fracture reduction was more direct and easy , and had good stability . 
for type iv fractures , it needed percutaneous reduction by leverage firstly , and then plate fixation or kirschner wire with an external stent fixation should be used after reduction . die - punch fractures could generally be diagnosed by x - ray , but for patients who might have overlapping bone structure or subtle fractures , x - ray results might be false negative . 
and due to pain and other reasons , some patients were difficult to cooperate with the examination , which led to non - standard in frontal and lateral x - ray plates , and deviation or misjudgment in display and orientation of fracture line ( figs.1 , 2 , )  . 
 the x - ray examination of different slopes can improve the diagnostic value of x - ray examination , but it is still not worth as high as ct examination . 
it could make up the lack of traditional x - ray , and could accurately display the actual situation of die - punch fracture , which were conducive to the choice of definite diagnosis and accurate fracture classification , and provides reference for treatment [ 20 , 21 ]  . 
therefore , ct scan should be necessary for the diagnosis of die - punch fracture . in summary , die - punch fractures of intermediate column of the distal radius could be divided into dorsal fractures , volar fractures , splitting fractures , and collapsed fractures . 
in the ankle , the etiology is not completely clear , but these lesions are frequently reported after sprains , located particularly on the talar dome [ 1 , 2 ]  . 
ols are clinically relevant , as they may cause remarkable pain on weight bearing , thus limiting sport and daily activities especially in young and active population [ 3 ]  . 
this stabilizes the blood clot obtained after microfracturing and takes advantage of the ability of bone marrow cells to regenerate articular cartilage [ 5 ]  . imaging plays a crucial role in the evaluation of olt prior and after treatment . 
 thus , magnetic resonance imaging ( mri ) represents the standard of reference in this setting , as it is able to evaluate thoroughly the olt and particularly the cartilage layer [ 7 ]  . 
 furthermore , when dealing with operated cartilage , mri is able to evaluate the surface of the cartilage , matrix thickness and volume , subchondral borders , and integration of cartilage matrix with subchondral bone [ 7 ]  . 
however , the association of mocart with the clinical outcome is still not clear [ 10 ] , with authors reporting conflicting results using different surgical techniques [ 1012 ]  . 
furthermore , mocart has been specifically developed for the knee , and its applicability in other joints needs to be further investigated . the aim of our study was to evaluate the applicability and reproducibility of mocart score for morphological evaluation of olt repaired using the amic technique . materials andmethods study population institutional review board approval ( ospedale san raffaele , milano , italy ) was obtained and patients informed consent was waived for this retrospective study . 
this study has been conducted according to the principles expressed in the declaration of helsinki . we retrospectively reviewed the mri scans of the ankle performed after surgery on patients with olt repaired using the amic technique between november 2011 and july 2015 at our institution . 
a total of 13 consecutive patients ( 6 females , 7 males ; age : 38.915.9 , range 1463 ) , who underwent 26 ankle mri scans at 6 and 12months from surgery , were included in this study . 
all patients had one olt treated with amic procedure : out of 13 , 7 were treated with biomimetic osteochondral scaffold implantation , while 6 were treated with bone marrow - derived cell transplantation . surgical cartilage repair technique bone marrow - derived cell transplantation consists of three phases performed during a single surgical session : ( 1 ) preparation of platelet gel ; ( 2 ) preparation of bone marrow aspirate ; and ( 3 ) implantation [ 13 ]  . 
in the first phase , 120 ml of patients venous blood is harvested and processed with a system for on - site preparation of hemoderivates ( vivostat system , vivolution , alleroed , denmark ) 1day before surgery to provide 6ml of platelet - rich fibrin gel . 
the harvested bone marrow is processed in the operating room by removing most of the erythrocytes and plasma using a cell separator ( smartprep ; harvest technologies , plymouth , massachusetts ) to obtain 6ml of concentrate containing nucleated cells ( stem cells , monocytes , lymphocytes , and other cells resident in the bone marrow )  . 
 a layer of platelet - rich fibrin is finally applied over the membrane to provide growth factors . regarding the biomimetic osteochondral scaffold implantation , the lesion site is prepared creating a 9 - mmdeep defect with stable shoulders where the scaffold is placed . 
the lesion is templated with use of aluminum foil , and the scaffold ( maioregen , finceramica faenza , faenza , italy ) is cut to the exact size of the defect and then implanted by press fitting . 
this osteochondral biomimetic scaffold has a porous three - dimensional composite threelayer structure that mimics the osteochondral anatomy [ 14 ]  . from the surgical point of view , medial lesions are usually approached through a medial malleolar osteotomy . 
to ensure that adequate exposure is made , the line of osteotomy should be performed at the junction of the medial plafond . 1 3 radiol med ( 2017 ) 122 : 909917 after the entire set of grafts is implanted , osteotomy is fixed with two malleolar screws that are inserted through predrilled holes . table 1 mocart score category defect fill mri protocol all mri scans were performed at 1.5 t ( magnetom avanto , siemens medical solution , erlangen , germany , gradient strength 45 mt / m , slew rate 200 t / m / ms ; magnetom espree , siemens medical solution , erlangen , germany , gradient strength 33mt / m , slew rate 170t / m / ms ) using a dedicated extremity coil . 
the following sequences were performed : sagittal t1 - weighted turbo spin - echo [ repetition time ( tr ) / echo time ( te ) of 500 / 9.2ms , slice thickness 3mm ] , sagittal short time inversion recovery [ tr / te 3990 / 29ms , inversion time 160ms , slice thickness 3mm ] , axial t1 - weighted turbo spin - echo [ tr / te 500 / 9.2 ms , slice thickness 3 mm ] , axial proton density - weighted fatsaturated [ tr / te 4120 / 32 ms , slice thickness 3 mm ] , coronal proton density - weighted fat - saturated [ tr / te 4120 / 32 ms , slice thickness 3 mm ] , coronal t2 - weighted turbo spin - echo [ tr / te 4500 / 81ms , slice thickness 3mm ]  . image interpretation andstatistical analysis the mocart score is a set of variables created for describing cartilage repair tissues after treatment . 
they include degree of defect filling , cartilage interface , surface , presence of adhesions , structure and signal intensity of the repair tissue , the subchondral lamina and bone , and the presence of effusion [ 8 , 9 , 15 ]  . 
for each variable , a score is given and the total score ranges from 0 to 100 points , where 0 is the worse condition and 100 is the best . 
in our institution , radiologists and orthopaedic surgeons , including residents , are trained in the use of mocart score since all cases of olts surgically repaired are discussed in multidisciplinary sessions . mri scans performed at 6 and 12 months from surgical treatment were independently interpreted at different sessions by : ( 1 ) one musculoskeletal radiologist with 12years experience ( r1 ) ; ( 2 ) one radiology resident with 5 years experience in musculoskeletal radiology ( r2 ) ; ( 3 ) one orthopaedic surgeon with 11 years experience ( o1 ) ; and ( 4 ) an orthopaedic surgery resident with 4years experience ( o2 )  . 
the item points subchondral bone exposed incomplete < 50% incomplete > 50% complete hypertrophy complete demarcating border visible defect visible < 50% defect visible > 50% surface intact surface damaged < 50% of depth surface damaged > 50% of depth absent homogeneous inhomogeneous or cleft formation normal nearly normal abnormal intact not intact intact granulation tissue , cyst , sclerosis absent cartilage interface surface adhesions structure signal intensity subchondral lamina subchondral bone effusion total observers r1 and o1 independently reviewed mri images additionally a second time 1month after the first evaluation in order to assess intra - observer reproducibility . 
there are several surgical options including microfractures , arthroscopic debridement , osteochondral grafting , and autologous chondrocyte implantation , but the best approach is still controversial [ 18 , 19 ]  . 
over the past decades , the advancements in orthopaedic mri have led to the introduction of fast sequences with high spatial and contrast resolution allowing for a non - invasive and more and more accurate evaluation of articular cartilage [ 20 ]  . 
the high diagnostic performance of moderate echo time fast - echo sequences in assessing articular cartilage defects of the knee is well known , especially when using fat saturated images , with high inter - observer agreement [ 21 , 22 ]  . 
coronal proton density - weighted fat - saturated ( a ) , coronal t2 - weighted turbo spin - echo ( b ) , sagittal stir ( c ) and sagittal t1 - weighted turbo spin - echo ( d ) images show complete filling of the osteochondral defect of the medial talar dome by repair tissue with persistent irregularities and edema of the subchondral bone ( arrow )  . 
 the small articular space limits the assessment of repaired cartilage features and the identification of adhesions , especially in the absence of significant articular effusion ( t tibia , f fibula , t talus , c calcaneus ) evaluation of the articular cartilage of the knee [ 23 , 24 ]  . 
 in that anatomic location , the mocart score seems to be strongly reliable for the evaluation of osteochondral lesions treated using different surgical approaches , with high inter - observer agreement [ 9 , 23 ]  . 
however , correlation between clinical scores and mri findings are still controversial [ 9 , 13 , 2325 ]  . although not specifically designed for other joints , several authors have used the mocart in the ankle for the evaluation of olt treated using different surgical 1 3 914 radiol med ( 2017 ) 122 : 909917 fig . 
coronal proton density - weighted fat - saturated ( a ) , coronal t2 - weighted turbo spin - echo ( b ) , axial proton density - weighted fatsaturated ( c ) and axial t1 - weighted turbo spin - echo ( d ) images show complete filling of the osteochondral defect ( arrow ) of the medial talar dome by repair tissue . 
it is difficult to assess cartilage thickness and interface in this case as well , whilst it is easily recognizable the slight subchondral bone edema , the integrity of subchondral lamina and the absence of effusion ( t tibia , f fibula , t talus ) approaches [ 10 , 11 , 2629 ]  . 
 they reported good reliability for degree of defect repair , defect filling , quality of repaired tissue , and synovitis , while reliability of integration and adhesions showed poor to moderate reliability . 
however , the methods of reproducibility analysis are not very clear [ 12 ]  . our data demonstrate the low reliability of the mocart for morphological evaluation of olt repaired using the arthroscopic amic technique with few exceptions . 
the intra - observer reproducibility of both radiologists and 1 3 radiol med ( 2017 ) 122 : 909917 orthopaedic surgeons was substantial when evaluating the cartilage surface , while radiologists had better results in the assessment of subchondral bone and subchondral lamina . 
 however , after surgical treatment of olt , subchondral edema is frequently found and may persist for years without a clear correlation with clinical status of the patient [ 23 , 30 ]  . 
indeed , the main problem in the talar joint is the small articular space limiting the assessment of repaired cartilage features and the identification of adhesions , especially in the absence of significant articular effusion . 
the advantage of proton density - weighted fat - saturated sequences is that high signal intensity of cartilage has good contrast compared to the low signal of the subchondral bone . 
a way to improve the reliability of the mocart score could be the intra - articular administration of contrast agent but this would make invasive a non - invasive technique also increasing the time and costs of the procedure [ 31 ]  . 
however , although gadolinium - based contrast agents have been administered safely for several years due to the minimal patients risk , the awareness of clinicians regarding the potential risks of repeated administrations of these contrast media has recently increased , focusing on the consequences of gadolinium accumulation in human tissues [ 33 , 34 ]  . 
indeed , other available options for the evaluation of repaired olt are t1 mapping , t2 mapping , diffusion - weighted imaging and diffusion tensor imaging that could lead to a quantitative and objective assessment of biological surgical repair of cartilage [ 20 , 24 , 35 ]  . regarding evaluation at 6and 12 - month follow - up , both radiologists and o1 reported a significant improvement of mocart score . 
however , several authors have shown conflicting results in the correlation between the mocart score and the clinical outcome of patients with olt surgically repaired [ 1012 , 29 , 37 , 38 ]  . 
 [ 38 ] showed no relation between the mocart and clinical outcome after treatment of olt with arthroscopic amic , while another study showed good correlation in three out of five variables of the modified mocart after autologous chondrocyte implantation in the ankle [ 13 ]  . 
however , this was beyond the scopes of our work . in conclusion , mri certainly has a crucial role in the follow - up of surgical repaired olt , but the mocart score does not seem to be sufficiently reliable and reproducible to be applied for this purpose . compliance with ethical standards ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the following primary tumor sites were investigated : nasopharynx ( 13% ) , oropharynx ( 42% ) , oral cavity ( 32% ) and larynx non - glottic ( 13% )  . 
specifically , in 5 cases out of 19 oral cavity tumors ( 26% ) , pet / ct detected neck - nodes positive ( not detected at ct - scan )  . 
these findings have allowed to change the patients management , including pet / ct neck - nodes positive in the high - risk rt volumes . conclusion in the rt planning strategy , the present findings support the use of pet / ct to improve upfront regional staging of hnc disease , particularly for oral cavity tumors . 
during the last years , the impact of the metabolic profile in locally advanced hnc by means of 18f - fluorodeoxyglucose positron emission tomography ( pet ) / ct has been investigated in several settings such as pre - treatment staging , radiation therapy ( rt ) planning strategy and to monitor response after treatment [ 13 ]  . 
the usefulness of pet / ct in rt planning is an object of debate : the main criticisms remain specific technical gaps related to visual operator interpretation or variability of gross tumor volume ( gtv ) definition [ 1215 ]  . 
more specifically , in several studies a comparison of gtv delineation by pet / ct versus ct alone or mri was performed : a decrease in gtv extension was found and these results were considered as factor potentially able to influence clinical outcomes [ 12 , 15 ]  . 
pet / ct was performed with the radiotherapy immobilizers ; post - injection , pet / ct images were acquired at 4660 m images were acquired from the vertex to the mid - thighs . 
axial images were acquired using a siemens pet / ctpet mct flow ( global siemens healthcare germany )  . pet / ct scans were visually reviewed by experienced readers blinded to clinical data . 
 due to the absence of reference standard values for maximum standardized uptake value and other semi - quantitative values , we considered pet / ct as positive in this subset of hnc patients only on the basis of qualitative visual assessment performed by two experienced nuclear medicine physicians . 
specifically , pet / ct was defined as positive if the metabolic activity of fdg in the lesion was moderately or markedly increased relative to comparable normal structures or surrounding soft tissues . 
a lesion with no or faint uptake ( less than the surrounding tissues ) of fdg was defined as negative even if a recurrent tumor had been suspected on ct or mri . 
all cases in which a stage migration was recorded , in terms of differences in nodal involvement between ct and pet / ct , were deeply discussed with the nuclear medicine physician and radiologist . 
a treatment planning ct with 3 - mm slice thickness and intravenous contrast was acquired in the treatment position and matched with pet / ct and mri ( when available ) in the treatment position to better define target volumes . 
the contouring system was mim maestro software ( us )  . the gtv was manually expanded to clinical target volume ( ctv1 ) at the discretion of the radiation oncologist . 
a total dose of 70gy to ptv1 , 59.9463gy to ptv2 and 54.4558.1gy to ptv3 were prescribed in 3335 fractions , using simultaneous integrated boost technique . all plans were performed with 9 - fields sliding window intensity modulated rt or 4 - arcs volumetric modulated arc rt ( rapid arc ; varian medical system , palo alto , ca ) and nominal energy of 6mv , as described in other studies [ 1719 ]  . concurrent chemotherapy was prescribed as follows : ( 1 ) cisplatin 100mg / m2 repeated every 21days if eastern cooperative oncology group - performance status ( ecog - ps ) was 01 , age < 70years , disease of any t classification ( t ) / n classification ( n1 ) or t3 to t4 / n0 ; ( 2 ) cisplatin 30mg / m2 weekly if ecog - ps was 2 , age < 70years , disease of any t / n1 or t3 to t4 / n0 ; ( 3 ) no chemotherapy if ecog - ps was > 2 , age > 70years , or t1 to t2 / n0 disease . results patients all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . sixty locally advanced hc patients , treated between october 2013 and february 2017 , were analyzed in the current study . 
primary tumor sites were : nasopharynx in 8 patients ( 13% ) , oropharynx in 25 patients ( 42% ) , oral cavity in 19 patients ( 32% ) and larynx non - glottic in 8 cases ( 13% )  . all patients were staged with ct scan and pet / ct . 
conversely , in one oropharyngeal patient , in which a suspicious lymph node was revealed at ct scan but not confirmed at pet / ct , a radical dose at this level was avoided . 
additionally , in two cases of oropharyngeal cancer , rt was avoided because of distant metastases . findings onstage migration in table1 , the changes in tnm stage by means of pet / ct versus ct based on the population of study are detailed . 
analyzing the subgroups , considering the primary tumor site ( nasopharynx , oropharynx , oral cavity and larynx non - glottic ) , showed that oral cavity tumors were at particular risk of nodal stage migration . 
this event occurred in 26% of oral cavity patients . in 2 / 25 ( 8% ) patients affected by oropharyngeal cancer , pet / ct detected distant metastases ( lung e liver )  . 
additionally , in 1 / 8 cases the detection of ct non - visible t1 - nasopharyngeal primary tumor was found by means of pet / ct . in case of stage migration , fnac was performed in four patients . 
in two patients , with distant metastases detected by pet / ct , fnac confirmed the malignancy from oropharynx hpv positive and , thus , a first line of systemic chemotherapy was administered . conversely , in the remaining four patients with pet / ct neck nodal positivity , fnac was not performed for the following reasons : in a single case due to the procedure - risk ( retropharyngeal node positivity ) , and in the other cases after the multidisciplinary evaluation with nuclear medicine physician and radiologist . impact ofpet / ct onradiotherapy planning strategy in table2 , the results regarding the type of changing in rt volumes by means of pet / ct versus ct - based evaluation are detailed . globally , pet / ct findings caused changes on nodal radiation treatment volumes in 10% of all patients . 
in 5 of the 19 oral cavity patients , neck - nodes pet / ct positive ( not detected at ct - scan ) were included in the high - risk volumes . 
on the other hand , in another nasopharyngeal patient pet / ct identified the primary tumor discussion no consensus regarding the best staging by diagnostic images of locally advanced hnc exists . 
ct scans and mri are the preferred diagnostic modalities : mri is the standard imaging modality in the assessment of nasopharynx , oral cavity tumors , perineural spread and bone marrow invasion [ 20 , 21 ] ; ct is preferred for laryngeal cancer and to assess the bony invasion [ 22 ]  . 
in this context , ct and mri allow to evaluate some criteria of suspect including the nodal size and contrast - enhanced patterns , not always specific of metastatic colonization . 
concerning lymph nodes evaluation , the sensitivities - rates ranged between 14 and 80% for ct - scan and 2985% for mri and specificities from 80 to 100% for both diagnostic modalities [ 16 ]  . 
several studies reported that pet / ct is superior to conventional imaging for neck - nodes metastases detection [ 23 , 24 ]  . although the limits of the current analysis , in particular the wide spectrum of primary disease sites and clinical stages analyzed , in our series , oral cavity tumors revealed to be at risk of nodal stage upgrading by means of pet / ct . 
 on the other hand , this potential gap could be overcame by meta - analysis data showing that pet / ct nodes sensitivity and specificity were estimated in 79 and 86% , respectively . 
 probably , the setting in which pet / ct sensitivity could present some limits remains in ct - cn0 patients , where the estimated rate is 50% ( 95% ci 3763% ) whereas the specificity is 87% ( 95% ci 7693% ) [ 25 ]  . 
concerning other findings of the present analysis , in 8% of patients affected by locally advanced oropharyngeal cancer pet / ct allows to detect distant metastases ( pathologically confirmed )  . 
furthermore , in these patients , rt was avoided , whereas in patients with nodal stage migration hypermetabolic nodes were included in the rt treatment planning high - risk volumes . the issue of the impact of metabolic imaging on the rtplanning optimization has been investigated in various setting [ 11 , 15 , 26 , 27 ]  . 
 [ 15 ] , the role of pet / ct in rt target definition and patient management for hnc was compared with ct alone : no significant changes on the lymph nodes status were found . 
 conversely , cacicedo and colleagues [ 11 ] reported that pet / ct was able to modify dose prescription or the initial planning for rt treatment in 12% cases of cases . 
thus , further investigations are advocated with this last intent . compliance with ethical standards funding this research did not receive any specific grant from funding agencies in the public , commercial , or not - for - profit sectors . conflict of interest the authors declare that they have no conflict of interest . 
furthermore , the correlation between strain ratio values and other variables was investigated . results the mean age of the ht patients was 139.6327.61months , and no significant difference was found between the control group ( 143.0927.32months ) and the patients regarding mean age and gender . 
it was also considered that the elastography si value had higher sensitivity and specificity than the conventional us in ht patients with moderate to advanced tissue hardening . keywords hashimotos thyroiditis children strain index elastography ultrasonography introduction hashimoto thyroiditis ( ht ) , the frequency of which has increased rapidly in recent years , is the most common cause of hypothyroidism in children in developed countries . 
the most important pathophysiological process in the development of the disease is the degeneration of the thyroid gland as secondary autoimmune to the lymphocytic infiltration , frequently before it becomes a multinodular tissue [ 2 ]  . ht is often closely related to the severity of the immune injury , which affects the clinical course of the disease . 
strain elastography ( se ) performed with the freehand method and shear wave elastography ( swe ) , which is a dynamic evaluation method , are frequently used in the elastographic evaluation of the thyroid . 
it has been emphasized that the strain index ( si ) is the most sensitive measurement method for evaluating non - nodular diseases of the thyroid gland [ 4 , 5 ]  . 
however , there are insufficient studies of its use to evaluate hashimoto thyroiditis in pediatric patients . this study aimed to evaluate the efficacy of elastographic si in the diagnosis and grading of pediatric ht patients . material andmethod study design this cross - sectional , controlled trial was performed in the pediatric radiology department of our tertiary care center after the approval of local institutional review board . 
demographic and laboratory data , age , gender , and measurements of thyroid stimulating hormone ( tsh ) and anti - thyroid peroxidase antibody ( anti - tpo ) were recorded for each patient . 
other causes of thyroiditis ( such as graves disease , acute , and subacute thyroiditis ) , patients with a thyroid nodule , those who used thyroid hormone replacement ( levothyroxine - t4 ) and children under the age of 3years were not included in the study as they were not suitable for optimal elastography examination . the demographic information of the patients is given in table1 . 
the present study included a total of 63 patients with ht diagnosis comprising 71.4% girls ( n = 45 ) and 28.6% boys ( n = 18 ) as the patient group and a control group of 47 children comprising 72.3% girls ( n = 34 ) and 27.7% boys ( n = 13 )  . 
the mean age of the ht patients was 139.6327.61months , and no significant difference was found between the control group ( 143.0927.32months ) and the patients regarding mean age and gender . 
 thyroid imaging of all the patients was performed by a pediatric radiologist with 8years experience in thyroid us and 5years experience in elastography , who had no knowledge about the diagnoses and laboratory findings of the patients . conventional ultrasonography examination the us was applied to all patients in the supine position and the heads in dorsal flexion . 
 [ 6 ] ( table2 )  . following the conventional us , regions of interest ( roi ) in both thyroid lobes were fixed through the free hand method , and the si measurement was performed through the elastography software by the same radiologist using the same probe [ 7 ]  . 
in the elastographic measurement , the highest strain ( the softest area ) was observed with a red color in the standard width areas ( average 4mm ) observed in the roi , while the areas with no strain ( the hardest area ) were indicated with a blue color . 
 table 2 ultrasonographic hashimotos thyroiditis staging table developed by sostre and reyes grade sonographic patterns grade 1 ( g1 ) grade 2 ( g2 ) grade 3 ( g3 ) grade 4 ( g4 ) diffusely enlarged gland with a normoechoic ( similar to normal tissue ) pattern multiple hypoechoic foci or patches scattered throughout an otherwise normoechoic gland ; a pattern suggestive of focal rather than diffuse involvement enlarged gland with diffuse but mild hypoechogenicity enlarged gland with diffuse and marked hypoechogenicity fig . 
 the numbers define the strain values , and % defines the strain ratio the conformity of the data to normal distribution was evaluated with the shapirowilk test , while the variance homogeneity was evaluated with the levene test . 
 the independent sample t test was used with bootstrap results , while the mannwhitney u test was used with the monte carlo results when comparing two independent groups on quantitative results . 
 the relationship between the classification determined by the cut - off ( prediction ) values of the groups calculated according to the variables and the real classification , the sensitivity , specificity , positive identification rate ( positive predictivity ) and negative identification rate ( negative predictivity ) were analyzed and expressed through the receiver operating curve ( roc ) analysis . 
the quantitative variables were shown as the meanstandard deviation ( sd ) and median range ( minimummaximum ) , and the categorical variables were shown as number ( n ) and percentage ( % ) in the tables . 
the variables were analyzed at 95% confidence level and a value of p < 0.05 was accepted as statistically significant . results a positive and strong statistically significant correlation was observed between the grade evaluated with us gray scale in the ht patients and the mean si and anti - tpo values ( p < 0.001 ) ( table3 )  . 
the disease has female gender predominance , and although seen in children up to 3years of age , it often occurs after the age of 6 and peaks at 1012years of age [ 8 ]  . 
in the present study , the mean tsh value of the patients was 3.41 and the majority of the patients were found to be euthyroid at the time of diagnosis . approximately 90% of children diagnosed with ht are determined to have high levels of anti - tpo and antithyroglobulin ( anti - tg )  . 
these findings were consistent with the findings of the study conducted by menzilciolu [ 9 ]  . the staging of ht patients using the conventional us gray scale method is an application which has been long used in clinical practice . 
however , in studies where it has been compared with doppler us and biopsy is specifically applied , this application has limited clinical benefit about inflammation and fibrosis , especially in the early period of ht [ 10 ]  . 
although its clinically significant auxiliary effects have been shown in many areas , various studies have been conducted in recent years on its use in thyroid nodules , thyroiditis , and autoimmune thyroid diseases [ 11 ]  . there have been significant results in many studies performed to predict malignant and benign thyroiditis nodules , which are difficult to distinguish particularly with conventional methods compared to the use of us elastography in the thyroid gland . 
as from 2013 , the efsumb guidelines recommend the use of this method in the initial evaluation of the thyroid nodule and patients with negative fine - needle aspiration biopsies . in a study of 54 healthy children by yurttutan et al . , the mean si value was 0.540.38. 
in the current study , the mean si value of the healthy group was found to be 0.260.77 , which is consistent with the result of the previous study [ 12 ]  . 
in the ht group , as expected , the mean si value was significantly higher ( 1.751.46 ) than the control group . the mean si value in patients diagnosed with ht was determined to be significantly higher than that of the control group . 
 in the present study , a significant increase in the sensitivity and specificity of the si value was noticeable in patients with ht , particularly at g3 and g4 stages . 
major limitations of the study were that the number of patients was low and that the criteria [ 6 ] for evaluating the gray scale us could not be applied to normal patients . 
it was also thought that the absence of thyroid biopsies of the patients and us application by the same radiologist might have affected the determination of the desired high susceptibility rates in the study . to the best of our knowledge , this is the first study of elastographic si measurements in pediatric patients diagnosed with ht . 
it was also considered that the elastography si value had higher sensitivity and specificity than the conventional us and doppler us in ( g34 ) ht patients with moderate to advanced tissue hardening . 
this article is an open access publication abstract objectives to assess the diagnostic confidence in detecting and localizing areas of bone marrow edema in the sacroiliac joint of patients with suspected spondyloarthritis using a single - plane method and comparing it with multiplanar unenhanced and enhanced methods . materials and methods patients with clinical suspicion of spondyloarthritis undergoing an mri of the sacroiliac joint were included in this retrospective study . 
to assess sacroiliitis , three methods were applied : single - plane ( i.e. , para - coronal stir alone ) , multiplanar unenhanced ( i.e. , para - coronal stir and para - axial pd - fs ) , and multiplanar enhanced method ( i.e. , para - coronal and para - axial postcontrast t1 - fs )  . 
both multiplanar methods increased the diagnostic 0.405 and p confidence in detection ( p < 0.001 ) and localization ( p < 0.001 ) of sacroiliitis ; no significant difference occurred between the multiplanar unenhanced and enhanced meth1.00 , respectively , for detection ods ( p and localization )  . 
plten , austria radiographic sacroiliitis had a primary role for the diagnosis , classification , and monitoring of patients with spon dyloarthritis ( spa ) since its introduction among the rome classification criteria in 1961 and the modified ny criteria in 1984 [ 13 ]  . in 2009 , the assessment of spondyloarthritis international society ( asas ) [ 4 ] listed magnetic resonance imaging ( mri ) findings of active inflammatory lesions among the diagnostic criteria for spa , and , since then , much effort has been devoted to optimizing a dedicated mri protocol for this category of patients . 
thus , several studies have 1 3 radiol med ( 2017 ) 122 : 752760 focused not only on the role of stir and post - contrast sequences ( i.e. , the main sequences recommended by the asas ) , with the aim of evaluating the necessity for contrast medium ( cm ) application [ 58 ] , but also on the utility of a multiplanar approach to accurately investigate a joint as complex as the sacroiliac joint ( sij ) [ 912 ]  . 
a recently published study showed good diagnostic performance for para - axial proton density fat - sat sequences ( pd - fs ) for both the acute and chronic findings associated with spa [ 13 ]  . 
 however , to date , to the best of our knowledge , no studies have been performed to assess how a multiplanar nonenhanced method , including stir and para - axial pd - fs , might affect the detection and localization of areas of bone marrow edema ( bme )  . thus , the aim of this study was to evaluate the diagnostic confidence in detecting and localizing bme in patients with clinical findings suggestive of spa , using para - coronal stir alone , and comparing it with the diagnostic confidence using a multiplanar method without contrast application , which included para - coronal stir and para - axial proton density fat - saturated sequences , and with a multiplanar contrast - enhanced method . materials and methods patients and study design patients with clinical findings suggestive of spa according to asas guidelines [ 4 ] , referring to our tertiary center for diagnostic assessment with mri of the sij between september 2013 and june 2015 were included in this retrospective , institutional review board approved study . 
each patient has been assessed using the three above - mentioned methods ( i.e. , single plane , multiplanar unenhanced and multiplanar enhanced ) and applying an interval of 4 weeks among the respective analyses , aiming thus to reduce any potential imaging readers bias . diagnostic confidence in detection of bme to assess the presence of bme , the iliac and sacral bones were partitioned on each side into the following regions : antero - superior ; postero - superior ; mid - anterior ; mid - posterior ; antero - inferior ; and postero - inferior . 
the boundary between the superior and mid portion was traced at the level of the first sacral foramina , whereas the mid and the inferior portions were divided at the level of the second sacral foramina . 
a dedicated 4 - point scale was used to rate the unable to localconfidence in localization of bme ( 1 probably able to ize ; 2 localize ; 4 probably unable to localize ; 3 able to localize with confidence )  . for the patient - based assessment , the same criteria applied for the diagnostic confidence in detection were used also for the localization . absolute frequencies and percentages are presented for categorical data . percentages of bme confident detection rating obtained by each method were compared using the cochran q test , followed by post hoc bonferroni - corrected mcnemar test . 
the maximal cranio - caudal extension of each lesion was also assessed on stir and classified according to a 3 - point scale ( < 1 cm intermediate grade ; 3 cm < 2 2 cm 1 ; 1 3 )  . 2 ; results sd , 38.34 seventy - four patients ( 38 males and 36 females ; mean age 10.88 years ) who underwent an mri of the sij at our department for a clinical suspect of spa were enrolled in this study . 
thirty - seven patients ( 50% ) 1 3 radiol med ( 2017 ) 122 : 752760 turned out to be completely negative for sacroiliitis ( i.e. , no bmes were evident with any of the applied methods )  . diagnostic confidence in detection of bme overall , 1776 regions were analyzed with the single plane and multiplanar unenhanced methods , and 1752 with the multiplanar enhanced because for one patient no post - contrast images were available due to an adverse reaction to cm . 
nine areas confidently rated as positive without the application of cm ( i.e. , single plane and multiplanar unenhanced method ) were not confidently assessable by the post - contrast sequences ( i.e. , respectively eight bmes were rated as probably no bme and one as probably bme , all in patients with at least one other bme confidently diagnosed by all methods )  . 
one area considered probably unable to be localized was not confirmed on either multiplanar unenhanced or enhanced images ; therefore , its localization with the last two methods was not feasible . 
as aforementioned , six areas ( i.e. , in five patients ) were detected only on stir alone ( i.e. , detections diag2 ) and not on multiplanar methods nostic confidence ( i.e. , detections diagnostic confidence 1 ) , and therefore , they were also not localized by these last methods . the friedman test , applied to compare the confidence in localization for each lesion , showed a significant difference among the three methods . 
an increasing number of studies have emphasized that the presence of subchondral bme , seen on stir , is considered sufficient to diagnose active sacroiliitis [ 4 , 15 , 16 ] , and suggesting that cm is not mandatory and should only be applied in equivocal cases . 
 [ 7 ] declared that the administration of cm might be beneficial by providing a different view of the lesions with another sequence , and when mri is interpreted by inexperienced readers , or when minimal changes occur . 
 our results showed that the benefits provided not only by a different pulsed sequence , but also by multiple acquisition planes ( e.g. , para - axial ) increase the diagnostic confidence for detecting and localizing each bme area . 
indeed , in our population , the multiplanar unenhanced method allowed a high diagnostic confidence in detection and localization in 46 and 20 1 3 758 radiol med ( 2017 ) 122 : 752760 areas , respectively , which showed a doubtful rating using the single plane method ( i.e. , detections and localizations diagnostic confidence increased overall in 25 and 13 patients , respectively )  . 
even if some ultimate scientific evidence [ 1719 ] affirm that cm might not be necessary for diagnosing bme in young patients with spa ( i.e. , juvenile spondyloarthritis ) , in our case , it allowed a clear distinction of the increased vascularity [ 20 ] and allowed the diagnosis , through pathologic enhancement , of bme otherwise not confidently diagnosable with stir alone or in association with the para - axial pd - fs . 
 conversely , in adults with chronic signs and also possibly under treatment , the assessment of bme might become more difficult due to the presence and overlap of areas of inflammation with zones of fat replacement . 
however , in this setting , stir has already demonstrated the ability to accurately depict bme even better than after cm application [ 6 , 13 , 21 ]  . 
the same observations were made in our study , where the nine areas with low diagnostic confidence for bme detection on multiplanar contrast images and high rating on unenhanced images ( i.e. , both stir alone and multiplanar unenhanced ) were close to fat replacement zones . 
signal intensity and size of the bme areas demonstrated , in our population , to have a role in the confidence of bme detection , as shown by the statistically significant difference in the distribution of certain and uncertain rating according to these two variables ( i.e. , both assessed on stir )  . 
this evidence and the absence of bme with a cranio - caudal diameter greater than 2 cm and with very high si among those with uncertain rating let us assume that small areas with low si benefited from a multiplanar approach for confident detection . 
 as mentioned above , conversely , no statistically significant difference emerged between the distribution of certain and uncertain localizations rating when size and si were taken into account : it is then reasonable to assume that uncertain localization is due to the complex anatomical structure of the sij more than depending on the si and the size of bme area , an assumption that might also justify the use of a multiplanar approach . 
 area of bone marrow edema ( white circle ) easily diagnosed ( i.e. , detections diagnostic confidence 4 ) and localized ( i.e. , localizations diagnostic confidence 4 ) with all three methods : single plane method ( para - coronal stir only in a ) ; multiplanar unenhanced method ( para - coronal stir a and paraaxial pd - fs in b ) ; and multiplanar enhanced method ( paracoronal post - contrast t1 - fs in c and para - axial post - contrast t1 - fs in d ) 1 3 radiol med ( 2017 ) 122 : 752760 confidence for the other spa features ( e.g. , synovitis , enthesitis , capsulitis )  . limitations the main limitation of this study is that there was only one group of raters . 
we believe , however , that the presented results have a sufficient reliability and impact because the raters were two experienced and dedicated musculoskeletal radiologists working in consensus and analyzing each dataset ( i.e. , single plane , multiplanar unenhanced , multiplanar enhanced ) with an interval of 4 weeks in - between . 
thus , we expect that the application of a multiplanar unenhanced method in the daily clinical setting would have an even higher positive impact on radiologists who are not sub - specialized in the musculoskeletal field . as this is a retrospective study , the distribution of the clinical and laboratory information , beside the clinical suspect of spondyloarthritis , was not homogeneous ; therefore , no correlation between the radiological analyses and the clinical parameters confirming the diagnosis was per formed . 
a future prospective longitudinal study may focus on these aspects and further assess the advantages of the hereby - proposed method . the inclusion only of patients with clinical suspect of spa might be considered prone to an overrating of bme and , in association with the absence of controls , to a biasing effect on the readers , but the detection of 37 patients completely negative for sacroiliitis ( i.e. , absence of any bme with each method ) indicates that 50% of the population can be considered as a control group for bme and highlights the accuracy and objectivity of the study . size and si were assessed only on stir and not on the other sequences , because a quantitative evaluation of the measurements obtained from each set of images could have revealed differences that , presumably , would have been mainly dependent on the intrinsic technical differences ( e.g. , snr , fluid sensitivity ) of the applied sequences ( i.e. , stir , pd - fs , postcontrast t1w fs ) [ 2225 ]  . 
a qualitative and quantitative assessment and comparison of the datasets derived from the different sequences based on size and si of each bme area would have exceeded the aim of this study . last , the applied method for the patient - based assessment ( i.e. , in each patient , the confidence of detection and localization was considered improved when a method allowed an increase in rating in at least one area ) might be considered prone to overestimation of the multiplanar methods . 
however , the correct assessment of each bme has an impact on the therapeutic management at diagnosis as much as during the follow - ups especially for patients affected by spa . 
therefore , we believe that our evaluation strategy is justified . in conclusion , the application of a multiplanar method can improve the diagnostic confidence in detecting and accurately localizing areas of bme . 
the absence of statistically significant differences between the proposed unenhanced method , including para - coronal stir and para - axial pd - fs , and the multiplanar post - contrast method suggests that cm does not provide any additional value for a higher diagnostic confidence . 
we thank mary mcallister for her thorough reading and editing of the manuscript and marzia pivetta for editing the drawing . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
becker1 xavier montet1 diomidis botsikas1 received : 13 march 2017 / accepted : 16 june 2017 / published online : 22 june 2017 italian society of medical radiology 2017 abstract objective to compare two fat suppression techniques used for 3d t1 - weighted sequence in breast mri ( magnetic resonance imaging ) , namely dixon versus spectral fat saturation ( fat sat )  . materials and methods all breast mri examinations performed in a philips 3 t unit between march 2013 and october 2015 including either a dixon or a fat sat sequence were retrospectively analyzed . 
the examinations were subjectively evaluated by two independent experienced readers in a scale of 5 for overall quality of fat suppression , homogeneity of fat suppression , definition of anatomic structures and focal lesions , diagnostic confidence for axillary and internal mammary regions and the presence of artifacts , 1 corresponding to excellent and 5 to non - diagnostic quality . 
 it is mainly indicated in breast cancer screening of highrisk patients , in selected cases of pre - operative staging of recently detected breast cancer , in case of discordance between clinical examination and conventional radiographic evaluation , as well as for the follow - up of breast cancer post - neoadjuvant chemotherapy . 
it is also indicated for patients with suspected implant rupture , when conventional imaging is not conclusive as well as for patient with free polyacrylamide gel injection [ 1 ]  . cancer detection on breast mri is mainly based on unenhanced and dynamic contrast enhanced ( dce ) t1 - weighted sequences which aim to detection of contrast uptake by tumoral tissue . 
many researchers , especially at the first years of emergence of breast mri , proposed dynamic t1 - weighted imaging without fat suppression [ 26 ] , their main arguments being that it requires no extra time , and that it is not influenced by magnetic field inhomogeneities but also that fat contributes to overall signal and thus images are of better quality , offering anatomical delineation of lesions included in a fat background . 
 this approach includes post - processing with subtraction of unenhanced t1 - weighted images from the series of dynamic - enhanced acquisitions . the other approach of dynamic contrast enhanced breast mri includes unenhanced and multiple enhanced t1 acquisitions with fat suppression [ 7 ]  . 
the advantage of the dixon is its insensitivity to b0 inhomogeneities [ 12 ] , which radiol med ( 2017 ) 122 : 731742 is very important , in particular when working with 3 t systems where the field heterogeneities can be more prominent . 
given the fact that the t1 - weighted dixon sequence is less sensitive to field inhomogeneities , especially in a 3 t magnetic field and that in our clinical experience it is associated with less artifacts in the axillary region , we would like to test the diagnostic performance of the dixon sequence before adopting it for routine clinical practice . the aim of this study was to quantitatively and qualitatively compare image quality for breast imaging of two fat suppression techniques , dixon versus spectral fat saturation . materials and methods type of study and patients characteristics this retrospective study was accepted by the ethics committee of our institution and informed patient consent was waived . 
all patients who underwent dynamic - enhanced breast mri examination performed on a philips 3 t unit between march 2013 and october 2015 , either a dixon or a spectral fat saturation thrive sequence ( fat sat ) , were included in the study . 
 the first post - contrast image was always performed 90 s after intravenous injection of 0.1 mmol / kg of gadoterate meglumine ( gd - dota , dotarem , guerbet , france ) in the axial plane . 
the choice of performing either the dixon or the fat sat protocol depended on the time available according to the clinical program , given that in our system the dixon sequence required more post - processing time , during which the mri could not be used for the next patient . 
dixon images were reconstructed with a modified algorithm accounting for multi - peak fat modeling and for a more robust separation of fat and water to reduce the water - fat swaps , this algorithm is now part of the latest philips releases but was still in development at the time of the study [ 13 , 14 ]  . image analysis mri examinations were anonymized and transferred to a dedicated workstation ( osirix pixmeo bernex switzerland )  . two experienced radiologists with 5 and 15 years of experience in interpretation of breast mri evaluated all examinations for the following subjective criteria : overall quality of fat suppression , homogeneity of fat suppression , definition of anatomic structures , definition and enhancement pattern of focal lesions , diagnostic confidence for axillary and internal mammary regions and the presence of artifacts . 
the subjective evaluation was performed on the first t1 acquisition performed 90 s after gadolinium injection , as it is the most appropriate for detection of early enhancement of suspicious focal lesions . 
however , for an experienced reader , the difference of images between the two fat suppression techniques was obvious . excellent to 5 the density of the breast was evaluated from 1 to 4 , 1 corresponding to a , 2 to b , 3 to c and 4 to d according to acr birads lexicon [ 15 ] by both readers independently . 
based on these measurements , the maximal total area of the breasts was calculated in the axial plane using the mathematical formula of the ellipsoid area calculation ( area maximal coronal diameter and b maximal anteroposterior diameter of the breast ) , divided by two , considering approximately each breast area as half of that of an ellipsoid . b , where a statistical analysis cohens kappa coefficient was calculated to test interobserver agreement for subjective evaluations . 
interobserver agreement was evaluated with r software ( r version 2.15.3 ( 2013 - 03 - 01 ) security blanket 2013 ; the r foundation for statistical computing )  . 
as shown in the diagrams , there is no significant difference in the linear regression slopes between the two techniques in correlation to breast density . concerning correlation to breast area , significant differences were found : ( 1 ) for anatomic structures definition , the fat sat getting better with bigger breast areas and the dixon getting worse , the two lines crossing at about 320 cm2 total maximal breast area in the axial plane . 
1 linear regression between cumulative subjective and objective variables and the breast area with the corresponding r2 and p values 1 3 738 radiol med ( 2017 ) 122 : 731742 fig . 
2 linear regression between cumulative subjective and objective variables and the breast density with the corresponding r2 and p values 1 3 radiol med ( 2017 ) 122 : 731742 uptake , when the tumor itself is surrounded by suppressed hypointense fat . 
there are basically two different fat suppression techniques , the classical spectral fat saturation and the dixon sequence . the dixon technique [ 16 ] is broadly used in abdominal and pelvic imaging [ 1720 ]  . 
its main advantage is that in the same acquisition it provides 4 different t1 - weighted image datasets ( in - phase , out - of - phase , water , fat )  . 
moreover , compared to classical spectral fat suppression , the dixon sequence is less sensitive to b0 inhomogeneities [ 12 ] , which is very important , in particular when working with 3 t systems where the field heterogeneities can be more prominent . 
 [ 10 ] studied mri images of twenty patients comparing a dixon with a spectral fat saturation sequence , using qualitative criteria and found that the dixon sequence was superior for most studied parameters . 
 [ 11 ] in a series of 19 patients evaluated dixon and spectral fat saturation sequences by studying qualitative parameters and signalto - noise as well as contrast - to - noise ratio for focal breast lesions . 
according to this study , the dixon sequence was proved to be superior to the standard spectral fat saturation . in a larger scale study on a siemens 3 t unit , clauser et al . 
concerning correlation with breast density , for most parameters , the dixon has the tendency to get better with increased breast density , except for evaluation of target lesion enhancement and cnr of target lesion . 
for most parameters studied , the spectral fat saturation technique is independent or gets better with increasing density as well . concerning breast size , for most of the parameters studied , the dixon technique is associated with worse scores with increasing breast size . 
this phantom study showed that metallic artifact with the dixon technique is more hypointense , thus easily recognized , but of smaller size and consequently with less interference with image interpretation . 
this was not the case with dixon images but this can be explained by the fact the dixon technique requires two echoes that act as two averages when the water image is reconstructed . 
axial mr image 3d t1 - weighted gradient echo sequences after injection of gadolinium - based contrast agent ( first acquisition , 90 s after contrast injection ) with spectral fat saturation showing aliasing artifact 1 3 740 radiol med ( 2017 ) 122 : 731742 fig . 
4 mri examinations of two different patients with metallic markers post - percutaneous biopsy : 3d t1 - weighted gradient echo sequences after injection of gadolinium - based contrast agent ( first acquisition , 90 s after contrast injection ) with spectral fat saturation ( a ) showing bilateral magnetic susceptibility artifacts ( white arrows ) in the site of marker clips , implanted after biopsy of papillomas and 3d - t1 dixon technique ( b ) illustrating a large mass of the right breast with clip placement in its centre . 
notice that there is no difference in the appearance of the metallic clips ( white arrows ) as illustrated by fat sat ( a ) and dixon ( b ) technique identified as originating from the injector . 
these artifacts were not very frequent and were eliminated when their origin was identified ; there are , therefore , not to be related to a specific fat suppression technique . concerning axillary regions , the fat sat technique suffers from particularly important pulsation artifacts that in many cases limit the interpretation for the presence of pathological lymph nodes . 
as the role of mri is of increasing importance for the evaluation of the axillary region [ 23 ] , the dixon technique presents a clear advantage as it allows fig . 
 follow - up mr images : 3d t1 - weighted gradient echo sequences after injection of gadolinium - based contrast agent ( first acquisition , 90 s after contrast injection ) with spectral fat saturation ( a ) and dixon technique ( b )  . 
notice that the dixon sequence shows well - defined axillary and internal mammary regions ( b ) , whereas the fat saturation sequence is sub - optimal in these regions due to flow artifacts related to cardiac pulsation ( a ) evaluation of both breast lesions and axillary regions in a one - stop - shopping technique . a great added advantage of the dixon technique is that it provides at the same time the t1w series as well as the fatsuppressed t1w . 
at the same time , if there is a movement between the acquisitions , the fat - suppressed images provide an alternative for correct diagnosis . despite the fact that the dixon outperforms the fat sat sequence in practically all studied parameters , it is considerably longer . 
however , the reconstruction of the 4 separated image series took approximately 15 min with the modified reconstruction algorithm on our systethis situation was not ideal since the system cannot be used 1 3 radiol med ( 2017 ) 122 : 731742 prospective study , it would not have been possible to obtain both sequences in the same time , during the same examination . 
however , for all examinations , all other parameters , as type of contrast medium , time of acquisition and injection rate were unchanged and only the fat suppression technique was different . 
axial mr 3d t1 - weighted gradient echo sequences after injection of gadolinium - based contrast agent ( first acquisition , 90 s after contrast injection ) with spectral fat saturation . 
diagnosis of fai is based on a combination of clinical features and supportive imaging findings ; radiographs and computed tomogra phy may be employed for demonstrating abnormal contact and abutment between the femoral head and the acetabular rim [ 5 ]  . 
magnetic resonance imaging ( mri ) is performed in an increasing number of patients with suspected fai to assess the morphology of the femur and acetabulum and to detect lesions of the labrum and articular cartilage [ 68 ]  . 
 mr arthrography ( mra ) has the advantages of distending the joint , improving contrast - to - noise ratio , and enabling acquisition of higher resolution images [ 9 , 10 ]  . 
in addition , mra has been reported to be more sensitive and specific for the detection of acetabular labral tears and acetabular cartilage defects in the hip than the conventional mri [ 11 16 ]  . 
imaging of the articular cartilage and the labrum in the 1 3 radiol med ( 2017 ) 122 : 774784 hip remains challenging because of the spherical shape of the hip joint , with difficult visualization of anterosuperior and posterosuperior aspects of the joint on coronal and axial images [ 1 ]  . 
since most labral tears are located anterior superiorly or posterior superiorly , the use of the standard imaging planes and conventional sequences may result in partial volume averaging [ 11 ]  . 
recently , three - dimensional ( 3d ) techniques with isotropic resolution have facilitated shorter imaging times and multi - planar reformation in musculoskeletal imaging , minimizing partial volume effects [ 1720 ]  . 
for example , radial mr slices , which are used to visualize anatomic deformities in the setting of fai , can be reconstructed from a single 3d acquisition [ 21 ]  . 
clinical indications for mra were represented by fai , hip pain with no abnormal findings on previous studies , including conventional mri , labral , or chondral lesions suspected on the basis of clinical tests / symptoms . 
the injection was performed with a 22 - gauge spinal needle by a single experienced radiologist ( gf , more than 500 hip mra ) under fluoroscopic guidance with anterior approach . 
extravasation was diagnosed in two cases because of the presence of a large amount of contrast material within the structures located outside to the hip joint or in the iliopsoas bursa ; in these cases , the distention of articular cavity was considered insufficient for diagnostic purposes and these patients were excluded from the study as previously described . 
images were acquired with patients supine with the femur internally rotated , using a flexible fourchannel body matrix phased - array surface coil ( siemens body matrix ) and a six - channel spine matrix coil ( siemens spine matrix ) that were integrated into the examination table . 
hy - 3d images were obtained using a double - echo steady - state sequence increasing the t2 - weighting of fast imaging with steady - state precession ( fisp ) images , allowing improved delineation of fat , joint fluid , and cartilage . 
post - processing was performed on a dedicated 3d processing workstation ( syngo mmwp ve36a , siemens ag , berlin , germany ) ; 3d images were freely reconstructed on axial , coronal , sagittal , and oblique planes with different image thicknesses ( usually 0.72 mm ) according to radiologist choice and depending on the case analyzed ; radial reconstruction images were also obtained . image analysis images were retrospectively and independently reviewed by two experienced radiologists ( gf , ed ; 11 and 4 years of experience in musculoskeletal radiology , respectively ) blinded to clinical and surgical data . 
labral tears were diagnosed when there was interposition of contrast material between the labral base and the adjacent acetabular rim or extension of contrast material within the labrum , or when the labrum was displaced , partially or completely absent [ 24 , 26 ]  . 
diagnosis of acetabular chondral lesions was based on focal or diffuse thinning , discontinuity , or flap of the cartilage , with or without passage of contrast material within the defect [ 27 , 28 ]  . 
 acetabular labral tears and chondral defects were not graded ; each reader described the presence or absence of any positive findings on data sets of images available . surgery surgical data were considered as the reference standard . 
1 four quadrants of the acetabulum : anterosuperior ( as ) , posterosuperior ( ps ) , anteroinferior ( ai ) , and posteroinferior ( pi ) quadrants statistical analysis sensitivity ( se ) and specificity ( sp ) with 95% confidence intervals ( cis ) , positive predictive value ( ppv ) , negative predictive value ( npv ) , and accuracy ( acc ) , of reader 1 and reader 2 in detecting acetabular labral tears and acetabular chondral defects using 2d , hy - 3d and iw - 3d data sets were calculated . 
the false positives ( fp ) and false negatives 1 3 radiol med ( 2017 ) 122 : 774784 ( fn ) as compared with surgical data were assessed , based on the agreement regarding presence / absence of the abnormality and location of the abnormality . 
one patient had two labral tears ( one located as and one ps , respectively ) and one patient had a labral tear extending from as to ps quadrant : both of these cases were correctly diagnosed at mra using all the data sets employed . 
two patients had two chondral defects ( one located as and one ps , respectively ) : both these cases were correctly identified at mra using the three sequences analyzed . 
at imaging , there were no fp findings in the ai and pi quadrants as anterosuperior , ps posterosuperior , tp true positive ( number of patients ) , tn true negative ( number of patients ) , fp false positive ( number of patients ) , fn false negative ( number of patients ) , se sensitivity ( as percentage ) , sp specificity ( as percentage ) , acc accuracy ( as percentage ) , r1 reader 1 , r2 reader 2 fig . 
2 labral lesions : the false - positive ( fp ) and false - negative ( fn ) findings of reader 1 and reader 2 by reading 2d , hy - 3d , and iw - 3d images in the four quadrants of the acetabulutriangles and boxes in each quadrant do not represent a certain localization of the lesion ( s ) we evaluated both an intermediate - weighted fse sequence and a hybrid gre t1 - weighted sequence , in comparison with the standard 2d - fse protocol . 
3 chondral defects : the false - positive ( fp ) and false - negative ( fn ) findings of reader 1 ( r1 ) and reader 2 ( r2 ) by reading 2d , hy - 3d , and iw - 3d images in the four quadrants of the acetabulu there were no chondral lesions located in the ai and pi quadrants at the operating table . 
triangles and boxes in each quadrant do not represent a certain localization of the lesion ( s ) 90.9% obtained by reader 1 using both the 3d data sets to 70.4% for reader 2 using 2d images , were once again in line with those previously reported for similar imaging data sets [ 23 ]  . 
 [ 23 ] , the 3d double - echo steady - state sequence optimized for cartilage imaging did not improve the diagnostic performance in this setting , although conspicuity of cartilage lesions was markedly better than on t1 - weighted spin - echo sequence . 
the average acetabular cartilage thickness of 1.5 mm reported in previous studies [ 20 , 22 ] may explain why both 3d data sets yielded an increase in diagnostic accuracy with respect to 2d data set . 
owing to thin section high - resolution images , these sequences allowed us to diagnose some very small cartilage defects in the 3d images which were missed in the conventional 2d images . 
this increase in diagnostic accuracy may be important in the choice of the best surgical approach , since a delamination of cartilaginous surface could be treated with an arthroscopic fixation , whereas in the case of advanced signs of chondropathy , the patient may undergo a debridement [ 34 ]  . as described by park et al . 
this may be due to the study population enrolled ( mean age 26.7 years ) including many young patients suffering from early stage fai with relatively well preserved hip cartilage , and prevalence of lesions located in as and ps quadrants . in the analysis of labral tears , fn were predominantly located in posterior quadrants in case of 2d images . 
as regard chondral defects , only one fp was pointed out at hy - 3d images by both readers . the injection was performed by a single experienced radiologist under fluoroscopic guidance in our study , without any periprocedural complications . 
an anterior labral tear ( arrow ) is identified on t1 - weighted axial 2d mr image ( a ) and confirmed on pd radial 2d mr image ( b ) ; the tear is well depicted also using hy - 3d 1 , 5 mm reformatted image on axial plane ( c ) and iw - 3d 2 mm reformatted image on sagittal plane ( d )  . 
the anterior labral tear was confirmed at arthroscopy represents an accurate , quick , and radiation - free modality for joint injection [ 35 ] , and could be considered to reduce the exposure to ionizing radiations . as described by pozzi g et al . 
in accordance with the results of this study , gtps was relatively rare in our series because of a prevalence of young adults with a clinical and radiological diagnosis of cam - type fai . 
moreover , as done in previous studies [ 24 , 27 ] , gtps and other imaging findings including cartilage defects of femoral head , teres ligament tears , tendon tears , and bony edema were not considered in our statistical analysis , because they were uncommon in our population . this study had several limitations . 
second , a qualitative assessment of contrast and signal - to - noise ratio was not performed ; however , in our experience , the detection of labral and chondral lesions is usually enhanced by the presence of contrast material distending articular cavity . 
a further issue is that we did not grade labral and chondral lesions , although this was a limitation of similar , recently published studies [ 24 , 27 ]  . 
finally , the leg traction technique was not adopted in this study [ 37 ] , although the sensitivity values obtained are still high thanks to a good distension of the articular cavity in a study population including patients with no significant joint space narrowing . in conclusion , at 1.5 tesla hip mra , the accuracy of iw - 3d and hy - 3d images was not significantly higher 1 3 radiol med ( 2017 ) 122 : 774784 782 fig . 
a subtle anterior labral tear ( arrow ) is identified on pd radial 2d mr image ( a ) and confirmed on iw - 3d 1 mm reformatted image on sagittal plane ( b ) ; this tear was confirmed during arthroscopy . 
 a small flap near labrum base ( thick arrow ) was identified on iw - 3d 0.8 mm reformatted image on para - axial plane only during consensus reading ( d ) fig . 
a chondral defect ( thin arrow ) is identified on pd radial 2d mr image ( a ) ; multiple confluent chondral defects associated to diffuse chondral thinning ( arrowheads ) are nicely demonstrated on hy - 3d 1 and 5 mm reformatted image on axial plane ( b ) ; the chondral defect ( thick arrow ) appears even larger on iw - 3d 2 mm reformatted image on sagittal plane ( c )  . 
however , 3d imaging data sets could be used to reduce the scanning time of hip mra , avoiding the need to obtain multiple similar sequences on different imaging planes , or to increase diagnostic accuracy in case of doubtful findings on 2d imaging . 
in particular , iw - 3d should be preferred for the identification of labral lesions , whereas hy - 3d images could be of help for the identification of small chondral defects . 1 3 radiol med ( 2017 ) 122 : 774784 compliance with ethical standards 14 . 
in addition , none study subjects or cohorts have been previously published . conflict of interest the authors declare that they have no conflict of interest . informed consent since this was a retrospective study , formal consent was not required . 
carbonaro7 francesca caumo8 beatrice cavallomarincola 9 paola clauser10 chiara fedato11 alfonso frigerio12 vania galli13 livia giordano14 paolo giorgi rossi15 paola golinelli16 doralba morrone4 giovanna mariscotti17 laura martincich18 stefania montemezzi19 carlo naldoni20 adriana paduos14 pietro panizza21 federica pediconi9 fiammetta querci22 antonio rizzo23 gianni saguatti24 alberto tagliafico 25 rubina m . 
trimboli26 marco zappa27 chiara zuiani28 francesco sardanelli7 , 29 received : 24 february 2017 / accepted : 12 april 2017 / published online : 25 may 2017 the author ( s ) 2017 . 
this article is an open access publication abstract this position paper , issued by icbr / sirm and gisma , summarizes the evidence on dbt and provides recommendations for its use . 
in the screening setting , dbt in adjunct to digital mammography ( dm ) increased detection rate by 0.52.7 and decreased false positives by 0.83.6% compared to dm alone in observational and double - testing experimental studies . 
however , before introducing dbt as a routine screening tool for average - risk women , we should wait for the results of randomized controlled trials and for a statistically significant and clinically relevant reduction in the interval cancer rate , hopefully associated with a reduction in the advanced cancer rate . 
maria nuova , reggio emilia , italy 16 medical physics service , local health authority , modena , italy italy 1 3 724 radiol med ( 2017 ) 122 : 723730 excluded . 
the possibility to perform needle biopsy or localization under dbt guidance should be offered when dbt - only findings need characterization or surgery . keywords breast cancer digital breast tomosynthesis mammography screening introduction in the last years , many reports have appeared about digital breast tomosynthesis ( dbt ) in both the diagnostic and screening setting . 
in fact , thanks to a pseudo - threedimensional reconstruction , dbt allows for overcoming some limitations of standard two - dimensional ( 2d ) digital mammography ( dm ) caused by structural overlapping and resulting into false - negative and false - positive findings [ 1 ]  . 
the technical solutions proposed by vendors differ for tube movement ( continuous / discontinuous ) , width of oscillation angle , number of projections , type of detector , and other characteristics , although no substantial effects on diagnostic performance related to these differences have been reported so far . this position paper , issued by the italian college of breast radiologists by the italian society of medical radiology ( sirm ) and the italian group for mammography screening ( gisma ) , summarizes the available evidence on dbt and provides practical recommendations for its use . 
 for the levels of evidence ( loe ) reported here , we refer to the definitions given by the centre for evidence - based medicine , oxford , united kingdom [ 4 ]  . dbt for firstlevel screening several studies have evaluated the potential of dbt in first - level screening [ 514 ]  . 
in particular , three european prospective trials conducted in the context of organized population - based screening programs [ 69 ] and five retrospective studies from spontaneous screening settings [ 1014 ] have shown that dbt combined with dm ( or as a stand - alone approach [ 9 ] ) allows for a better diagnostic performance than dm alone . results of dbt differ according to the study design , the screening interval , and the type of screening setting ( organized versus spontaneous )  . 
however , although many experiences have shown the superior diagnostic performance of two - view dbt compared with one - view dbt [ 1618 ] , the availability of synthetic 2d mammograms generated from the dbt dataset ( see below ) has substantially overcome the problem 17 radiologia 1u , dipartimento di diagnostica per immagini , universit di torino , a . 
radiodiagnostica , candiolo cancer institute , fpo , irccs , strada provinciale 142 , km 3.95 , candiolo , 10060 turin , italy 19 dai patologia e diagnostica , azienda ospedaliera universitaria integrata , piazzale a . 
radiologia senologica , irccs ospedale san raffaele , via olgettina 60 , 20132 milan , italy 22 department of prevention , screening centre , local health authority , sassari , italy 23 pathology department , local health authority , asolo , treviso , italy 24 senology unit , local health authority , bologna , italy 25 department of experimental medicine , dimes , institute of anatomy , university of genova , via de toni 14 , 16132 genoa , italy integrative biomedical research phd program , department of biomedical science for health , universit degli studi di milano , via mangiagalli 31 , 20133 milan , italy 27 uoc epidemiologia clinica , istituto per lo studio e la prevenzione oncologica ( ispo ) , florence , italy institute of radiology , university of udine , piazzale s . 
 della misericordia 15 , 33100 udine , italy 29 department of biomedical sciences for health , universit degli studi di milano , via morandi 30 , san donato milanese , 20097 milan , italy 1 3 radiol med ( 2017 ) 122 : 723730 of dose . 
 notably , this variability depends on the baseline recall rate with standard dm because the higher the baseline dm recall rate , the higher the absolute and relative reduction obtained with dbt . 
thus , the advantage of reducing the recall rate could be less prominent in those screening programs which already have low recall rates with standard dm . if both dm and dbt are acquired ( separately or with the so - called combo modality ) , the average glandular dose is approximately doubled . 
however , considering the dose reduction obtained through the introduction of dm as an alternative to film - screen mammography , the dose of these dm / dbt protocols too remains below the upper limit defined by the european guidelines for quality assurance in breast cancer screening and diagnosis published in 2006 [ 23 ]  . of note , radiation exposure would be an issue to take into consideration for a generalized adoption of dm / dbt protocols for population - based mass screening . 
these sdms are virtual 2d mammograms obtained from dbt , paying no tradeoff in terms of radiation exposure [ 2426 ]  . several authors have compared sdm / dbt protocols with dm / dbt protocols demonstrating a similar diagnostic performance [ 2528 ]  . 
therefore , unless additional radiation exposure is specifically justified ( as in the work - up of suspicious findings detected at dm ) , a diagnostic mammography examination can be performed using the sdm / dbt approach . notably , two studies [ 29 , 30 ] have reported that 5457% of additional cancers detected by additional ultrasonography screening after negative dm were detected by dbt . 
 this is a relevant argument in favor of dbt , considering the practical hurdles for a generalized mass screening with ultrasonography in adjunct to dm . however , in the context of organized population - based screening programs , a simple increase in sensitivity and overall diagnostic performance of a new tool , even if statistically significant and clinically relevant , is not enough , per se , for its generalized adoption . 
in particular , considering the pre - existing evidence in favor of screening mammography ( recently confirmed by the international agency for research on cancer [ 32 ] ) , caution is urged due to the possibility that a substantial part of the additional cancers detected by dbt could be overdiagnosed lesions , i.e. 
unnecessary surgery , radiation , and / or medical therapy . it is worth to note that most of the additional cancers detected with dbt have been reported to be invasive [ 6 14 ]  . 
a large study from the united states [ 10 ] has compared dm / dbt in approximately 174 , 000 women with dm alone in approximately 281 , 000 women . 
they include at least sufficient availability of dbt equipments , management of suspicious findings at dbt alone , and increased reading time [ 3436 ] , which implies the need for more breast radiologists involved as screening readers . thus , before introducing dbt as a first - level screening tool , we should wait for the results of randomized controlled trials ( some of which are already ongoing in italy ) comparing a population sample having dm / dbt or sdm / dbt at the first round and dm alone at the subsequent round with a population sample having dm alone at both rounds [ 37 ]  . 
whether the total incidence of breast cancer in the dbt group exceeds that of the control group . the attention paid to interval cancer rate is explained by the possibility to use this measure as a proxy of effectiveness in mortality reduction [ 15 ]  . 
these heavy limitations prevent us to draw any conclusion to be extrapolated to european organized biennial screening programs . dbt for workup of screendetected suspicious findings , as a firstline diagnostic examination in symptomatic women , for preoperative staging , and targeted evaluation after mri several studies [ 4048 ] have shown that dbt is at least equivalent to additional dm views ( magnification , spot compression , 90 views , etc . ) , also reducing radiation exposure in both the diagnostic and screening setting . 
in the presence of palpable lesions , dbt has been reported to be never worse , and often better , than dm for estimating tumor size [ 49 ]  . 
finally , dbt allows for identifying some findings additionally found on preoperative mri also when they are not visible at targeted ultrasonography , permitting a reduction in the number of mr - guided biopsies [ 52 ]  . studies evaluating inter - reader variability for dm / dbt versus dm alone have reported for each reader an increase in the detection rate and a reduction in the recall rate with an overall increase in the diagnostic performance [ 5356 ]  . 
 in the particular context of spontaneous screening , dbt has also been found to reduce the number of short - time repeat examinations [ 55 ]  . all these results allow for recommending dbt for symptomatic women and for work - up of screen - detected suspicious findings . recommendations recommendations are presented here for five categories of women : 1 . 
asymptomatic women at average risk ( first level of organized or spontaneous screening ) these women should undergo dm starting not before the age of 40 , with a screening interval that may vary according to local health authoritys decision . 
as recently stated by the european society of breast imaging [ 57 , 58 ] , direct dm should be preferred to film - screen mammography due to a reduced radiation exposure [ 59 ] and an at least equivalent diagnostic performance [ 60 ] ( loe a )  . 
the preference is also in favor of dm when compared with indirect digital phosphor storage plate ( socalled computer radiography ) [ 61 ]  . dbt can be used as a first - level screening tool in women at average risk : in the context of studies approved by an ethical committee , with enrollment after informed consent signature by the woman ( for randomized controlled trials , refer to the scheme proposed by the osservatorio nazionale screening [ 37 ] ) ; in the well - defined context of centers being part of public population - based screening programs , with previous experience with ethically approved studies concerning at least feasibility of screening dbt , demonstrated through articles published in peerreviewed in both cases , the sdm / dbt approach should be preferred ( loe a )  . 
considering the data management needs , the necessary interactions with information technology services , and the impact of dbt on the whole multidisciplinary team , studies should be performed under umbrella of breast units . 
moreover , usual monitoring data should be collected , in particular absolute and / or proportional incidence of interval cancer and of screen - detected cancers of stage t2 or higher [ 37 , 62 , 63 ]  . 
attention should be paid to avoid that the implementation of dbt studies causes a reduction in screening coverage , compliance , or quality indicators . 1 3 radiol med ( 2017 ) 122 : 723730 2 . 
asymptomatic women at hereditary / familial high risk those with a previous breast cancer up to now , no substantial evidence has been produced in favor or against the use of dbt for screening women at intermediate risk of breast cancer , i.e. 
all these women should undergo screening dm with the same protocols recommended for asymptomatic women at average risk . for asymptomatic women with a previous history of breast cancer ( included in this general category of women at intermediate risk ) , we refer to the recommendations provided by the gisma and the italian college of breast radiologists by sirm [ 64 ]  . 
symptomatic women and women needing work - up of screen - detected suspicious findings we include in this category both women with suspicious clinical symptoms or signs ( asking for a mammogram usually ordered by a general practitioner or a specialist ) and asymptomatic women with screen - detected suspicious findings recalled for work - up in the context of spontaneous or organized screening . 
women with previous history of breast cancer , if having suspicious clinical symptoms / signs or after a suspicious finding on an imaging study , are also included in this category . in these women , if an indication to mammography exists and dbt is available , dbt should be performed ( loe a ) , preferably with a sdm / dbt protocol ( loe b )  . 
 if sdm mammograms are not available , dbt can be performed after dm ( loe b )  . women at hereditary / familial high risk should be screened in the context of dedicated pathways [ 6671 ]  . 
 considering the higher radiosensitivity of their breast tissue and the high sensitivity of mri for breast cancer , mammography can be avoided at least up to 35 years of age , in particular in brca1 mutation carriers . 
asymptomatic women at high risk due to previous chest radiotherapy recommendations regarding breast cancer screening for these women ( mainly lymphoma survivors ) were recently provided by the italian college of breast radiologists by sirm [ 72 ]  . 
needle biopsy under dbt guidance dbt can show doubtful / suspicious findings without any clinical correlate and even undetectable on dm , sdm , or ultrasonography [ 58 ]  . 
in those cases , when the dbt finding is neither detectable at targeted ultrasonography nor at dm review , a needle biopsy ( and , when necessary , also presurgical localization ) should be performed under dbt guidance . 
importantly , dbt guidance offers important advantages in terms of shorter procedure duration and reduced radiation exposure [ 77 , 78 ] ( loe b )  . as a consequence , centers offering dbt should also offer dbt - guided interventions for dbt findings not otherwise identifiable . 
at present , in fact , few centers are equipped with the device for dbtguided interventions . conclusions evidence available for dbt allows to recommend its usage for all cases of symptomatic women and women needing work - up of screen - detected suspicious findings ( consider ing both spontaneous and organized screening )  . 
in these settings , when available , sdm / dbt protocols should be preferred for symptomatic women . 1 3 728 radiol med ( 2017 ) 122 : 723730 breast cancer screening using the current mammography technology has been demonstrated to be effective in reducing mortality from the disease . 
from this perspective , completing the shift from analog film - screen mammography and computed radiography systems , that are still in use , to direct digital mammography systems ranks first in the order of priorities . a generalized adoption of dbt as a first - level screening tool should wait for a specific evidence , in particular for a statistically significant and clinically relevant reduction in interval cancer rate ( hopefully associated with a reduction in advanced cancer rates )  . 
when this evidence will be available , both asymptomatic women at average and intermediate risk ( including those with a previous breast cancer history ) will be allowed to be screened with dbt on a routine basis . 
accurate data collection will be necessary for many years in order to assess the overall impact of dbt technology in terms of mortality reduction and other efficacy / effectiveness indicators . 
for high - risk women , when a mammogram is indicated , a sdm / dbt protocol should be preferred . the already existing evidence , which has been built with a non - negligible contribution of italian breast radiologists , plays in favor of dbt . 
however , even in the united states , where fda approved the use of some dbt devices in some cases for screening , the use of dbt is still quite limited . 
a recent survey [ 79 ] among the members of the society of breast imaging reported that of 670 responders , only 200 ( 30% ) use dbt although 62% of non - users have planned to equip themselves with dbt . studies and researches are still needed for a deeper evaluation of dbt , a relevant innovation in breast imaging . 
there are two theories regarding the origin of os subfibulareone , suggesting that it origi nates from an accessory ossification center [ 1 , 2 ] , and the other , proposing that it is a non - united avulsion fracture of the lateral malleolus resulting from traction of the anterior talofibular ligament ( atfl ) [ 35 ]  . despite the debate regarding its origin , several studies have reported that os subfibulare is associated with chronic lateral ankle pain and instability [ 2 , 68 ]  . 
although conservative treatment including rehabilitation usually alleviates symptoms even in the case of acute trauma overlying an os subfibulare , surgical treatment is sometimes required 1 3 radiol med ( 2017 ) 122 : 766773 in chronic cases with persistent symptoms . 
surgical treatment consists of resection of the ossicle or osteosynthesis [ 912 ]  . however , it is difficult to predict the rehabilitation outcome in patients with chronic symptomatic os subfibulare . 
 specifically , the relationship between radiologic findings and rehabilitation outcome has not been assessed in the literature . therefore , the purpose of our study was to evaluate the radiologic findings for prediction of rehabilitation outcomes in patients with chronic symptomatic os subfibulare . materials and methods subjects this study was approved by the institutional review board of the armed forces medical command . 
the need for informed consent was waived as this was a retrospective investigation . 1025 ankle magnetic resonance imaging ( mri ) examinations performed at our institution from january to october 2016 were retrospectively reviewed by one radiologist ( c.p. ) and the radiologist found 116 patients with os subfibulare . 
1 flow chart for patients selection process ( peroneal muscles ) using elastic bands , ( 3 ) proprioceptive training including weight shifting and single leg standing to improve balance , and ( 4 ) reconditioning or functional exercise for returning to routine daily activities as cycling and jogging [ 14 ]  . 
we recommended that the patient undergo rehabilitation program for at least 6 weeks , and the rehabilitation outcome was assessed after at least 3 months from the start of the rehabilitation program [ 15 ]  . 
the rehabilitation outcomes were judged as good response when the symptoms of the ankle improved and the patient was capable of performing their daily activities without any pain or discomfort requiring no further treatment . 
the rehabilitation outcomes were judged as poor response if the symptoms persisted despite at least 6 weeks of rehabilitation and 3 months of conservative management and activities of daily living were limited . 
the mean time of evaluation after rehabilitation was 5 months ( range 38 months )  . clinical information one rehabilitation medicine physician ( b.s.k. ) obtained clinical information through review of the electronic 1 3 768 radiol med ( 2017 ) 122 : 766773 medical records and telephone survey . 
ankle instability was defined as clinical manifestations of repeated ankle sprain with or without subjective feeling of giving way with clinical evidence of instability on physical examination such as anterior drawer test or talar tilt test . radiologic evaluation all included patients underwent conventional radiographs with anteroposterior ( ap ) , lateral , and mortise views . 
we evaluated radiologic findings using the ap radiography . mri was performed with a 1.5 - t system ( magnetom avanto ; siemens medical solutions , erlangen , germany )  . 
 patients were examined in the supine position with one ankle placed in a neutral position in a dedicated ankle coil ( 8 - channel , foot - and - ankle coil , 1.5 t ; siemens medical solutions , erlangen , germany )  . 
in addition , the size was categorized as small , middle , and large for sizes of < 5 , 510 , and 10 mm , respectively [ 8 ]  . 
the location was categorized on the ap radiograph as level a for those below the tip of the malleolus and level b when on the articular side [ 16 ]  . 
atfl abnormalities were categorized as the following three categories : ( 1 ) normal , for thin , straight , and low si band extending from the talus to the fibular malleolus ; ( 2 ) partial tear , for an irregular / wavy contour or laxity , increased si within the substance of the ligament , or increased thickness ( > 3 mm ) , and ( 3 ) complete tear for discontinuity of the substance of the ligament or non - visualization of the ligament on axial t1wi and fat - suppressed t2wi [ 17 , 18 ]  . 
interposition of fluid si between the os subfibulare and the fibula was defined as present when the normal low si interspace was replaced with high si on axial and sagittal fat - suppressed t2wi . 
bone marrow edema in the os subfibulare was defined as high si on axial fat - suppressed t2wi and as bone marrow replacement on the axial t1wi compared to those of the adjacent fatty marrow . 
if there were multiple os subfibulares , only the one with the greatest diameter was evaluated . after initial independent readings , the final decision for each radiologic finding was reached by consensus between the two readers . statistical analysis a commercially available software program ( spss , version 18.0 ; spss , chicago , il ) was used for statistical analysis . 
based on the icc and kappa values , the inter - observer reliability was considered to be good to excellent . discussion in our study , we found that chronic symptomatic os subfibulare patients with poor rehabilitation outcome had os subfibulare with greater size and more commonly demonstrated the presence of interposition of fluid si between the os subfibulare and the fibula , and bone marrow edema in the os subfibulare compared with those with good rehabilitation outcome . 
if further validated in future studies , these radiologic findings may be used to predict rehabilitation table 1 clinical data in the 38 patients with chronic symptomatic os subfibulare characteristics good response group ( n 20 ) poor response group ( n 18 ) p value age ( years ) , mean ( range ) * male sex combined instability duration of symptoms ( m ) , mean ( range ) 8 ( 2153 ) 19 ( 90 ) 7 ( 35 ) 3 ( 318 ) note : data are no . 
b , c axial t1 - weighted ( b ) and fatsuppressed t2 - weighted images ( c ) show interposition of fluid signal intensity between os subfibulare and fibula ( arrowhead ) and bone marrow edema in the os subfibulare ( black arrow )  . 
a , b axial fat - suppressed t2 - weighted ( a ) and sagittal fat - suppressed t2 - weighted ( b ) images show interposition of fluid signal between os subfibulare and fibula ( arrow ) fig . 
b axial fatsuppressed t2 - weighted image shows bone marrow edema in the os subfibulare ( arrow ) outcome and to plan the optimal treatment in patients with chronic symptomatic os subfibulare . it is generally agreed that the majority of grades i , ii and iii lateral ankle ligament sprains can be managed without surgery balancing the advantages and disadvantages of surgical and non - surgical treatment [ 21 ]  . 
however , in our study , the proportion of poor response group despite at least 6 weeks of rehabilitation and 3 months of conservative management was relatively high [ 20 / 38 ( 53% ) ] and they had more presence of combined instability and longer duration of symptoms . 
several studies reported similar results that os subfibulare is associated with recurrent instability of the ankle and that good clinical outcome was observed after surgical treatment [ 2 , 7 , 912 ]  . until now , only a few studies have assessed the relationship between radiological findings and clinical outcomes . 
specifically , patients who showed a larger gap between the os subfibulare and fibular tip upon injection of contrast media had worse symptoms compared with those in which only little inflow of contrast was seen . 
further more , this degree of displacement of the os subfibulare was correlated with the presence of a fibrous union to lax thin scar tissue or no continuity between the ossicle and fibular tip based on arthroscopy . 
 [ 8 ] demonstrated that contrast enhancement was noted around the ossicle in os subfibulare patients with chronic ankle pain [ 20 / 24 ( 83% ) ] [ 8 ]  . 
our study showed that interposition of fluid si between the os subfibulare and the fibula and bone marrow edema in the os subfibulare were significant factors associated with classifying between the good and poor response groups after rehabilitation . 
considering the results of previous studies and ours , we speculate that os subfibulare without an intact fibrous union between the os subfibulare and fibula may have increased mobility , rendering it unstable and causing inflammation by irritation against the subchondral bone , thereby causing paour study also 1 3 radiol med ( 2017 ) 122 : 766773 table 2 radiologic findings in the 38 patients with chronic symptomatic os subfibulare good response group ( n 20 ) poor response group ( n 18 ) p value size ( mm ) , mean ( range ) * 3 ( 214 ) 3 ( 721 ) < 0.01 findings radiography size group location shape round to oval angular atfl abnormality partial tear complete tear atfl attachment to os subfibulare interposition of fluid signal intensity between os subfibulare and fibula bone marrow edema in os subfibulare note : data are no . 
5 receiver operating characteristic curve using size of os subfibulare for prediction of poor rehabilitation outcome in chronic symptomatic os subfibulare patients showed that size was an important factor associated with classifying between the two groups with 9 mm as the optimal size criterion demonstrating the highest sensitivity and specificity . 
there are several reports that describe the major characteristics of avulsion lesions , which include irregularity of the surface in contact with the malleolus , location of the fragment , a sharp angular shape and conformity with the fracture surface of the malleolus [ 5 , 16 , 22 ]  . 
the findings of our study may indicate that it may not be important whether the os subfibulare has originated from an accessory ossification center or from a nonunited avulsion fracture as radiological findings that are suggestive of avulsion lesions or those related with atfl were not significantly different according to rehabilitation outcomes . our study showed a higher rate of combined instability in the poor response group than the good response group despite the fact that the presence of atfl abnormality or attachment to the os subfibulare were not shown to be significant factors . 
because instability is subjective and apprehensive feeling that his or her ankle is unstable due 1 3 772 radiol med ( 2017 ) 122 : 766773 to various reasons , we suppose that other factors such as pain or increased mobility of the os subfibulare could have contributed to higher rate of instability symptoms in the poor response group . 
for the findings in our study to be accepted and used by clinicians and radiologists , it is noteworthy that not only did we find mri findings that were significantly different between the good and poor response groups , but those findings also demonstrated good to excellent interobserver reliability . our study had some limitations . 
 further studies are needed to elucidate the relationship between preoperative radiologic findings and postoperative clinical outcomes . in conclusion , our study demonstrated that large - sized os subfibulare , interposition of fluid si between the os subfibulare and the fibula , and bone marrow edema in the os subfibulare on mri may implicate poor rehabilitation outcome . acknowledgements the authors wish to thank h.s. 
di diagnostica ecografica avanzata e color - doppler , dipartimento di scienze radiologiche , oncologiche ed anatomopatologiche , policlinico umberto i , sapienza universit di roma , viale regina elena , 324 , 00161 rome , italy keywords patellar height musculoskeletal us musculoskeletal mri insallsalvati index introduction anatomical variations of the patella position can be often correlated with some clinical conditions . 
patella alta ( an abnormal high position of the patella ) is a condition associated with anterior knee pain , patellar instability , and osgoodschlatters disease ; patella baja or infera ( an abnormal low position of the patella ) with anterior knee pain and flexion limitation [ 1 , 2 ]  . in 1938 , blumensaat described for the first time a radio graphic technique to measure patellar height [ 3 ]  . 
in 1971 , insallsalvati ( is ) index was proposed as the ratio of the patella tendon length ( length of the posterior surface of the tendon from the lower pole of the patella to its insertion on the tibia ) to the length of the patella ( greatest pole - to - pole length ) [ 4 ]  . 
however , despite universal reference ranges for patellar height ratios on x - ray , there is yet a uniform consensus on the acceptable reference range for normal patellar height on mri [ 5 , 9 ]  . in the clinical practice , us is often the first - line exami nation for non - traumatic joint disease and it can evaluate 1 3 762 radiol med ( 2017 ) 122 : 761765 the patellar tendon and the patellar cortical profile [ 10 , 11 ]  . 
during a routine us examination , the is index can be evaluated to improve the diagnostic potential of the patellar instability and reduce the need for additional examinations . the aim of the current study was to evaluate whether universally accepted is index obtained with mri can be similarly evaluated with us examination . 
patellar tendon length ( pt ) was obtained with a device for a knee flexion angle of 30 , while patellar length ( pl ) was obtained with knee hyperextension using an ultrasound pad , to better evaluate the anterior patellar surface and compare data with those obtained with mri . all patients underwent mri ( artoscan 0.2 t , c - scan esaote , genoa , italy ) examination in the same us session . 
the scanning parameters were set as follows : the repetition time ( tr ) and echo time ( te ) of sagittal t1 - weighted spin echo , axial t2 - weighted spin echo , coronal gradient echo - short time inversion fig . 
1 a 31 - year - old football player with anterior knee paa patellar tendon measures 38.9 mm on us image and b 38 mm on midsagittal non - fat - saturated t1 - weighted spin echo . 
2 a 60 - year - old man with anterior knee pathe patellar tendon is difficult to evaluate at distal insertion on midsagittal non - fatsaturated t1 - weighted spin echo ( a ) and it measures 54.3 mm ( b )  . 
according to lee et al . , to compare us results with those of mri , an adjustment of 0.16 was addicted to us measurements [ 5 ]  . two operators , with different experiences of musculoskeletal imaging and blinded to the results of other investigators separately performed the mri and us measurements . informed consent was obtained from all individual participants included in the study . statistical analysis standard deviacontinuous data are presented as mean tion ( sd ) and as median with minimum and maximum range . 
 enthesopathy of the patellar tendon insertion was observed in 22 patients . discussion according to the literature , patellar height derangements can lead to progressive cartilage loss , functional impairment , and disability [ 12 ]  . 
 the is index is the most used ratio to evaluate abnormal patellar height , which is the commonest cause of anterior knee pa on x - ray images , cortical bone surface radiol med ( 2017 ) 122 : 761765 is often poorly evaluated ; moreover , the large variability of patella length , the possible presence of osteophytes , and other patellar derangements can limit the evaluation of is index . 
in recent years , patients with anterior knee pain often undergo straight second - level exams and x - ray results are not available at the time of cross - sectional imaging evaluation . 
reported their experience about the assessment of is index with a multimodality approach ( ct , mri , and x - ray ) , noting small quantitative differences between the evaluated diagnostic techniques [ 5 ]  . 
in clinical practice , us is often the first diagnostic approach in patients with not traumatic knee disease , because it is a non - invasive and widely - accessible method used in the differential diagnostic procedure of anterior knee pa martino et al . 
in our study , despite of different experiences of the operators , interobserver agreement using icc was 0.98 for us ( not statistically significant difference ) and pt and pl could be easily evaluated with us to obtain is index . 
 limitation related to mri technique included that it is a second level and expensive technique , more sensitive to susceptibility and motion in comparison with other methods , and available only for selected patients . 
us technique limitations in the evaluation of anterior knee pain included the strong operator - dependence , the difficult evaluation of patella cortical profile , and the incorrect use of the ultrasound pad . 
about structural features of the examined knees , severe patellofemoral osteoarthritis and enthesopathy of the patellar tendon insertion can limit the us evaluation of knee joint , while the presence of metallic structures ( previous surgery , foreign bodies , etc . ) can limit the mri evaluation . 
in conclusion , the evaluation of is index can enlarge the spectrum of us features providing an easy and reliable approach in patients with anterior knee pain , reducing the need of mri examination , particularly in post - traumatic and post - operative patients . compliance with ethical standards conflict of interest the authors declare that they have not conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the patients symptoms and mri features of nasopharyngeal mucosal thickening like location , symmetry , nasopharyngeal bubble , superfi cial mucus , nasopharyngeal retention cysts , serrated protrusions , contrast - enhancement type were documented . 
the most common pattern of nasopharyngeal mucosal thickening in nplh was diffuse wall thickening ( 38.37% ) , while unilateral posterolateral wall thickening ( 39.47% ) was more in t1 stage npc . 
nasopharyngeal bubble , retention cysts , serrated protrusions , symmetry , homogeneous enhancement , slight enhancement and vertical stripes were more common in * wen - bin li liwenbin@sjtu.edu.cn 1 department of radiology , shanghai jiao tong university affiliated sixth peoples hospital , shanghai jiao tong university school of medicine , no . 
contrary to com mon belief , nplh occurs not only in children but also in adult , who were heavy smokers and chronic rhinosinusitis 1 3 744 radiol med ( 2017 ) 122 : 743751 patients [ 2 , 3 ]  . 
while it is easy to discern an obvious npc by identifying signs like invasion of deep tissue , it is still extremely challenging to distinguish between benign nplh and early stage npc especially those found incidentally . endoscopic biopsy is the gold standard to confirm the diagnosis of npc [ 4 ]  . 
however , the endoscopic biopsy is an invasive procedure , carrying the risk of bleeding , and it is also impractical to conduct an endoscopic biopsy in every patient who has nasopharyngeal mucosal thickening [ 5 ]  . 
actually , careful and systematic assessment of nasopharyngeal mucosal thickening on mr imaging might prevent a patient who does not have an npc from undergoing an unnecessary biopsy . in the study of bhatia et al . 
further studies published by this team also demonstrated the value of contrast - enhanced mri in both screening healthy subjects who did not require an endoscopic biopsy , and in finding inconspicuous npcs [ 1 , 5 , 7 ]  . 
there was still a chance that small midline cancers causing no asymmetry could be missed , and benign nplh showing asymmetric nasopharyngeal mucosal thickening could be misdiagnosed as malignancy on mri [ 5 , 7 ]  . 
more advanced mri sequence such as diffusion - weighted imaging was found not to be helpful for the differential diagnosis [ 8 ]  . in our practice , we found that patients symptoms and indirect signs on mr images like accompanying sinus mucosal thickening , middle ear effusion , and cervical lymph nodes enlargement might play an important role in differentiating these two different diseases . 
therefore , the aim of this study is to further investigate the value of contrast - enhanced mri in the discrimination between benign nplh and malignant t1 stage npc . materials and methods study population the study protocol was approved by the institutional review board with a waiver of informed consent for this retrospective study . 
between january 2013 and june 2016 , biopsy - confirmed benign nplh patients and t1 stage npc patients from the ear , nose , and throat outpatient clinic were included in this study . 
the biopsy site was determined with reference to mri findings . according to endoscopic biopsy , the patients were divided into two groups : benign nplh group and t1 stage npc group . 
the nasopharyngeal wall was divided into the roof wall , posterior wall , and lateral walls as being above , level with and below , and overlying the distal ends of the torus tubarius , respectively , on axial mri images [ 6 ]  . nasopharyngeal mucosa exceeding 3 mm in thickness was defined as abnormal thickening . 
t2 - weighted sequences were useful in detecting retention cysts and superficial mucus ( hypo - intense signal on t1 - weighted mr images and t1 - weighted enhanced mr images , while extremely hyper - intense on t2 - weighted mr images )  . 
serrated protrusions were defined as irregular protrusions of the nasopharyngeal mucosa surface . 1 3 radiol med ( 2017 ) 122 : 743751 on t1 - weighted contrast - enhanced images , the pattern of contrast enhancement was classified as homogeneous enhancement or inhomogeneous enhancement . 
to be noted , the presence of retention cysts , bubble , and superficial mucus in unilateral mucosa should not be attributed as asymmetry . besides , possible accompanying signs were also recorded . 
cervical lymph nodes enlargement was defined by the shortest axial diameter equal or greater than 5 mm in the retropharyngeal region , 11 mm in the jugulodigastric region , and 10 mm in all other regions of the neck [ 9 ]  . statistical analyses summary data of the patients demographics and the mri features were described . 
logistic regression analysis was done with a backward - stepping procedure based on a likelihood ratio test with a p value greater than 0.10 used for table 1 basic demographics and symptoms of the nplh and t1 stage npc patients exclusion from the model . 
therefore , a total of 124 patients were included in this study finally , with 86 ( 69.35% ) patients confirmed as nplh and 38 ( 30.65% ) patients confirmed as t1 stage npc . 
the common symptoms of these patients were bloody nasal discharge or epistaxis ; nasal congestion ; ear fullness , conductive hearing loss or tinnitus ; pharynx discomfort or pain ; and neck mass . the detailed patents demographics and symptoms of the two groups are shown in table 1 . 
however , there was no significant difference in the frequency of middle ear effusion and sinus mucosal thickening between the two groups . table 3 shows the results of the logistic regression analysis with all evaluated mri features . 
in this study , we found differences in several mri features between the nplh group and the t1 stage npc group , of which unilateral posterolateral wall thickening , asymmetry , inhomogeneous enhancement and cervical lymph nodes enlargement were the most predictive mri features for malignancy . 
1 axial t1 - weighted image ( a ) and t2 - weighted image ( b ) show the presence of superficial mucus in an nplh patient ( arrows )  . 
2 axial t1 - weighted image ( a ) , t2 - weighted image ( b ) and t1 - weighted enhanced image ( c ) show the presence of serrated protrusions from the nasopharyngeal mucosa in an nplh patient ( arrows ) times more likely to have npc than female [ 10 ]  . 
 hence , the patients symptoms could not be used solely to make a correct differential diagnosis , and more workups like contrast - enhanced mri examination were needed to confirm the final diagnosis . in our study , nplh usually exhibited diffuse nasopharyngeal wall thickening ( 38.37% ) while t1 stage 1 3 748 fig . 
3 axial t1 - weighted image ( a ) , t2 - weighted image ( b ) and t1 - weighted enhanced image ( c ) show the presence of a retention cyst in an nplh patient ( arrows )  . 
although t1 stage npc could also manifest as diffuse nasopharyngeal wall thickening , there were other mri features listed in the below paragraphs that could be helpful in discriminating between the two diseases . asymmetry of nasopharyngeal mucosal thickening was a well - known important mri feature of npc [ 5 ]  . 
therefore , we should be careful in interpreting nasopharyngeal mucosal asymmetry , and other mri features should also be evaluated to make the final differential diagnosis . in our study , the nplh group patients had more signs of nasopharyngeal bubble , nasopharyngeal retention cysts , and serrated protrusions on mri . 
4 axial t1 - weighted image ( a ) , t2 - weighted image ( b ) and t1 - weighted enhanced image ( c ) show round low signal similar to air in the nasopharyngeal mucosa indicating the presence of nasopharyngeal bubble in an nplh patient ( arrows ) fig . 
5 in a t1 stage npc patient , axial t1 - weighted image ( a ) and t2 - weighted image ( b ) show relatively symmetrical nasopharyngeal mucosal thickening . 
6 in an nplh patient , we found asymmetrical nasopharyngeal mucosal thickening in the left lateral pharyngeal recess in axial t1 - weighted image ( a ) , t2 - weighted image ( b ) and t1 - weighted enhanced image ( c )  . 
actually , the middle ear effusion could be caused by the mechanical or functional obstruction of the eustachian tube by both npc [ 13 ] and nplh [ 14 , 15 ]  . 
 as for sinus mucosal thickening , a previous study reported a causative link between adenoids and pediatric rhinosinusitis , as adenoids contained bacteria and could obstruct the nasal airway mechanically [ 16 ]  . 
the sign of enlarged cervical lymph node was another important indicator of npc , as cervical lymph nodes metastasis was frequently seen in npc even in an early stage . although our study found many mri features that showed statistical differences between the nplh group and the t1 stage npc group illustrated in the above paragraphs , only the signs of unilateral posterolateral wall 1 3 radiol med ( 2017 ) 122 : 743751 thickening , asymmetry , inhomogeneous enhancement and cervical lymph nodes enlargement entered the final logistic regression model . 
analyzing the reason , the relatively small sample size in our study might account , and future larger study would cast light on this issue . our study had some limitations . 
however , our results do confirm that contrast - enhanced mri is helpful in the differential diagnosis between nplh and t1 stage npc . conclusions in conclusion , our study showed that patients symptoms could not be used solely to make a correct differential diagnosis between nplh and t1 stage npc . 
firstly , the signs of unilateral posterolateral nasopharyngeal wall thickening , asymmetry , inhomogeneous enhancement and cervical lymph nodes enlargement are the most predictive mri features for malignancy , and further biopsy is highly recommended . 
secondly , the presence of nasopharyngeal bubble , nasopharyngeal retention cysts , serrated protrusions and vertical stripes enhance the diagnostic confidence of benign nplh , and thus further biopsy could be avoided . 
a critical review of the complications was performed . materials and methods between 2010 and 2016 , pregnant women , with a prenatal diagnosis of morbidly adherent placenta ( map ) , were treated with occlusion balloon catheters in both internal iliac arteries . 
parameters such as need for hysterectomy , incidence of pph , grade of map , estimated blood loss during delivery ( ebl ) and transfusion requirements , mean recovery time and duration of the balloon inflation , were collected and reviewed . 
no keywords hysterectomy prevention massive postpartum haemorrhage prophylactic percutaneous occlusion balloon catheter placement uterine artery embolization 1 diagnostic and interventional radiology unit , department of health sciences , san paolo hospital , university of milan , via a . 
georges hospital , blackshaw road , london sw17 0qt , uk interventional radiology unit , careggi academic and regional hospital of florence , largo brambilla 3 , florence 50134 , italy introduction morbidly adherent placenta ( map ) is an abnormal development of the trophoblastic tissue into the uterine wall due to a defect in the decidua basalis and nitabuchs layer [ 1 ]  . 
the term placenta accreta is often used to represent all three placenta subtypes : accreta vera is the superfi cial invasion of the placental villi into the myometrium 1 3 radiol med ( 2017 ) 122 : 798806 without the normal intervening desidua basalis ; increta is the deep invasion of the myometrium ; and percreta is the invasion of serosa and extension into periuterine tissues . the incidence of abnormal placentation has been estimated at 1 in 533 pregnancies and is associated with major complications , including massive haemorrhage , large - volume blood transfusion and peripartum hysterectomy [ 2 ]  . previous caesarean delivery is the most common factor associated with placenta accreta . 
other potential risk factors include procedures that promote formation of an uterine scar , placenta previa , multiparity and advancing maternal age [ 3 , 4 ]  . hysterectomy after delivery is the standard treatment for placenta accreta , but this is associated with significant maternal morbidity including haemorrhage , shock and coagulopathy [ 5 , 6 ]  . 
this approach is suggested for patients with deep invasion of the placenta that carries a high risk of haemorrhage or injury to adjacent tissues and organs [ 7 ]  . 
 some authors propose that the conservative management should only be offered by dedicated centres with adequate equipment and available resources and expertise [ 10 ]  . the use of endovascular interventional procedures has been described in the management of obstetric haemorrhage of various causes , but its role in the management of map is still debatable for both radical and conservative approaches [ 3 , 1113 ]  . 
different endovascular procedures have been described , including the utilisation of balloon occlusion alone in the aorta , common or internal iliac arteries or a combination of balloon occlusion and embolization . 
the current literature has not conclusively shown evidence of superiority of any of these techniques . the efficacy of prophylactic balloon occlusion to reduce surgical bleeding has shown encouraging results in retrospective series , but current literature about its feasibility and safety is still inadequate [ 12 , 14 , 15 ]  . in our unit , management of map is addressed by performing a triple - p procedure which conserves the uterus and has been described elsewhere with encouraging results [ 16 ]  . the triple - p procedure is a 3 - step conservative surgical alternative to peripartum hysterectomy for women with morbidly adherent placentae . 
the procedure involves : perioperative placental localization and delivery of the foetus via transverse uterine incision above the upper border of the placenta ; pelvic devascularization ; and placental nonseparation with myometrial excision and reconstruction of the uterine wall [ 16 ]  . prophylactic occlusion balloons , utilised by our interventional radiology ( ir ) department , assist the triple - p procedure . 
our complication group is defined as any incident that required further management during or post - delivery ( pph , flow limiting or symptomatic arterial thrombosis )  . the primary endpoint of this study is to evaluate outcomes of triple - p procedure with prophylactic occlusion balloon placement ( pobc ) in terms of reducing postpartum haemorrhage ( pph ) , conservation of the uterus and reduced maternal and foetal morbidity . 
thereafter complications and also types of map were reviewed regarding estimated blood loss ( ebl ) , need for blood transfusion , balloon inflation time and the types of balloon utilised . materials and methods between january 2010 and february 2016 , 44 pregnant women , with a high risk of bleeding , were treated with reference to the interventional radiology department for pobc of the internal iliac arteries . 
patients without map or coming from other hospitals for surgical complications after delivery were excluded . our final sample includes 37 patients with a prenatal diagnosis of map ( by us and / or mri ) that underwent a triple - p procedure with pobc . procedure the patient was transferred to the angiography suite following placement of an epidural catheter . 
occlusion balloon catheters ( lemaitre vascular embolectomy catheters 5f - plus or boston scientific , ber enstein occlusion balloon catheters 6f ) were placed with their tips positioned into the anterior division of the contralateral internal iliac artery . 
this was achieved utilising pulsed low dose fluoroscopic guidance ( between 2 and 7.5 pulses per second ) to minimise radiation exposure to the mother and foetus [ 17 ]  . 
the obstetrician then surgically excised as much of the placenta as possible along with any myometrium and reconstructed the 1 3 800 radiol med ( 2017 ) 122 : 798806 the following day , the interventional radiologist would remove both the sheaths and occlusion balloon catheters and the arterial puncture sites sealed with closure devices . the following parameters were recorded for each procedure : hysterectomy , pph , maternal and foetal morbidity , surgical confirmation of the type of map , ebl during the procedure , need for transfusion and blood products required , recovery days post procedure , manufacturer of balloons used , duration of the balloon inflation , arterial thrombosis . patients were divided into two groups . 
patients with no complications ( group 1 ) and those with complications ( group 2 )  . in this paper we considered under group 2 not only the ir related complications , but also anything that required further management ( e.g. , pph which is actually a procedural failure rather than a complication )  . 
the t student test and mannwhitney u test were used to evaluate means , chi - squared test for proportions and kruskalwallis test were used when there were more than two variables test . 
the estimated mean blood loss after the procedure was 2203 , 2933 , and 1649 ml , respectively , with no significant statistical difference between the three groups ( table 2 )  . 
the ratio of patients that required transfusion in the accreta group was 5 / 14 , for the percreta was 3 / 3 and for the percreta was 16 / 20 . 
 in selected cases the balloons were left inflated for longer at the discretion of the obstetrician if it was felt there was an increased likelihood of late bleeding . to prevent potential peripheral ischaemic complications in the legs , rigorous monitoring was performed including : palpation of pedal pulses ; comparison of colour and temperature of feet ; pulse oximetry of both great toes ( to compare with pulse oximetry of finger )  . 
four patients were treated successfully by performing urgent uae and one was addressed laparoscopically by the on call surgeon without alerting the ir tea no secondary pph ( > 24 h ) occurred . 
two of the patients that were treated with uae , developed partial , non - flow limiting , asymptomatic thrombus in common iliac artery , that didnt require any further action . 
in these patients the sheaths had remained in situ longer than usual as a precaution in case of re - bleed . of the four developing arterial thrombosis , three had placenta percreta and one placenta increta . 
all patients were checked angiographically for potential peripheral thromboembolisation , but all were negative . with respect to their clinical presentation , one patient described pins and needles and cold foot 5 - h post - delivery . 
two patients did not have any symptoms , but thrombus formation was detected upon angiography the following day . one patient developed delayed symptoms of claudication and altered sensation of her lower limb 2 weeks following delivery . 
that was attributed to an underlying focal arterial dissection and was treated medically with eventual resolution [ 18 ]  . comparison between the non complicated ( group 1 ) and complicated group ( group 2 ) was performed . 
the rbc transfusion demand between group 1 and group 2 was statistically significant ( p 0.0001 ) ( table 4 )  . further sub - analysis between the two main types of complications ( pph and arterial thrombosis ) showed no statistical significant difference on any of the above parameters ( table 4 )  . 
there was no correlation between arterial thrombosis and the duration of balloon inflation ( table 4 ) neither in respect to the type of balloon catheter utilised . there were no femoral closure device related complications . discussion current evidence concerning the use of prophylactic balloon occlusion of the internal iliac arteries in women with map is still sparse . the literature on the role of ir in map can be divided into series where pobc is used either with planned caesarean hysterectomy or with uterine conservation and the results are different between these two groups . 
 when used with planned caesarean hysterectomy , some authors have reported that the balloon occlusion technique is effective in reducing blood loss , transfusion requirements , and provides favourable surgical conditions in terms of haemostasis and surgical field visibility [ 19 , 20 ]  . 
on the other hand , other authors did not find differences in terms of estimated blood loss , transfusion demand , and postoperative hospital stay duration [ 11 , 2123 ]  . 
2 transfusion requirement in relation to the type of abnormal placentation be relevant to the inhomogeneity of these results as one randomized controlled trial ( rct ) comparing blood loss following caesarean hysterectomy with or without pobc with the catheters in the internal iliac arteries showed no significant difference and it is proposed that common iliac or even aortic occlusion is more effective in preventing blood loss during caesarean hysterectomy [ 23 ]  . pva polyvinyl alcohol particles , ebl estimated blood loss number of patients requiring transfusion thrombosis balloon inflation time 1 3 radiol med ( 2017 ) 122 : 798806 fig . 
others have shown that maternal outcomes after conservative treatment of placenta accreta can preserve the uterus in 78.4% of women with a maternal morbidity rate of 6% , without using the prophylactic balloon catheter technique [ 10 ]  . our study is one of the largest studies in literature where map was treated conservatively using the triplep approach which includes the utilisation of pobc . 
they concluded that women with placenta percreta had a greater need for transfused blood products and had prolonged postoperative recovery times . we also identified a correlation between the required blood transfusion and the degree of placental invasion 0 . 
we also analysed the development of delayed pph ( under the complication group ) that is actually a procedure failure rather than a pobc - related complication . those patients developing either pph or arterial thrombosis ( complication group ) were found to have statistically significant intraprocedural ebl . 
furthermore , not unexpectedly they were found to have statistically significant greater transfusion requirements when compared to the non complicated group . therefore , extrapolating from the data , patients with greater blood loss during the caesarean section are at greater risk of developing complications and requiring further intervention . 
a potential explanation of the higher incidence of thrombosis in this group of patients might be the combination of high volume blood transfusion with the known underlying hypercoagulable state of pregnancy . 
operators should be aware that delayed arterial thrombosis may rarely occur , as one patient developed symptoms of claudication and altered sensation 2 weeks following delivery [ 18 ]  . currently , there are no agreed common guidelines for best practise in dealing with patients with map . 
this fact restricts the statistical results and hinders our capability to draw firm conclusions . more case series and prospective randomized comparative trials are needed to evaluate the efficacy and 1 3 radiol med ( 2017 ) 122 : 798806 complication rates of the different surgical and ir techniques available to date in the management of map . 
furthermore , a subgroup classification of the outcomes based on grade of abnormal placentation could better help us tailor our treatment methods . conclusion prophylactic occlusion balloon catheter placement in internal iliac arteries is an effective adjunctive technique in preventing pph and preserving the uterus . 
 our objective is to investigate fdg uptake levels of high res activity organs ( liver , spleen , bone marrow ) in invasive ductal breast cancer and to evaluate the association with the clinicopathological features . methods in the present study , 193 patients with invasive ductal breast cancer who performed fdg - pet / ct were categorized according to the clinicopathological features including age , tumor size , axillary nodal status , histological grade , the presence of lymphavascular invasion , receptor status , ki - 67 proliferation index and biological subgroup . 
we found that high suvmax in liver , spleen and bone marrow were signifi cantly correlated with worse prognostic clinicopathological features in patient with invasive ductal breast cancer . * ertan s ahin er_ahin@yahoo.com 1 department of nuclear medicine , namk kemal university hospital , tekirda , turkey 2 department of nuclear medicine , gaziantep university hospital , gaziantep , turkey conclusions fdg uptake level in high res activity organs is associated with the presence of tumor , and also directly relating clinicopathological features for patients with invasive ductal breast cancer . keywords reticuloendothelial system fdg clinicopathological features breast cancer introduction immune system is known to play a major role in the protection against diseases or other potentially damaging foreign bodies and in the initiation of antibody production [ 1 , 2 ]  . the mononuclear phagocyte system or mononuclear phagocytic system ( mps ) is a part of the immune syste mps is also known as the reticuloendothelial system ( res ) or macrophage systethe cells of this system are primarily monocytes and macrophages , and they play a role in both of the induction of immune response and of cell - mediated immune reactions . 
the liver , spleen , and bone marrow are known as the organs with the high reticuloendothelial system ( res ) activity [ 3 ]  . as a result of genetic mutations in cancer , various tumorrelated antigens are occured and related to this immune system activates . 
also , tumor cells undergoing necrosis are the other reason of activating immune response . immune system and its relation to diseases could be examined by various laboratory and imaging methods . in the past , when there were no advanced imaging methods , studies related to these subjects [ 46 ] were mostly designed with conventional nuclear imaging methods using radioactive labeled compounds . 
in these past studies [ 46 ] , it showed that the type , size and the activity of tumors are likely variables associated with changes in the res activity . 1 3 786 radiol med ( 2017 ) 122 : 785792 fluorine - 18 fluorodeoxyglucose ( fdg ) - positron emistomography / computed tomography ( pet / ct ) , a sion modality by which glucose metabolism is evaluated , is widely used in the assessment of a variety of malignancies including breast cancer . because of the fact that fdg is a glucose analog , fdg uptake rate in cells is based on the increased glucose consumption in relation to growth rate and energy need . several previous studies [ 710 ] have shown that fdg uptake in breast cancers is relevant to the tumor subtype , the biological , immunohistochemical and clinical prognostic factors , and the high fdg uptake is correlated with the poor prognostic factors . based on all of this information , it can be considered that fdg - pet / ct may show the degree of systemic immune response of induced with malignancy in the organs with the high res activity . in this regard , we hypothesized that the high fdg uptake of high res activity organs would be associated with the poor prognostic factors in breast cancers . although there are some studies which investigate the activation of immune system organs in cancers , to our knowledge , there are no fdg - pet / ct studies which investigate the relationship between the clinicopathological features of breast cancer and the immune system organs . 
 therefore , we aimed to evaluate the association of these clinicopathological features with the high res activity organs fdg uptake level in our study . materials and methods subjects the institutional review board approved this retrospective study . 
this study was conducted as a retrospective crosssectional study at the nuclear medicine department of university hospital . the database of 617 female patients who underwent fdg - pet / ct whole - body scan for clinical staging of breast cancer before initial therapy during the period of june 2007 to july 2016 was retrospectively reviewed . among these , 352 patients with histopathologically diagnosed invasive ductal carcinoma and tumor size greater than 1 cm were included as study candidates . 
these criteria were used to ensure patients homogeneity and to eliminate the partial volume effect depending on small tumor size . the patients with evidence of distant metastasis confirmed by other methods or fdg - pet / ct scan , history of other malignancies , and primary breast tumor showing low fdg uptake ( maximal standardized uptake value ( suvmax ) of the tumor < 2.5 ) were excluded from the study . other exclusion criterias were that lactating , being younger than 18 years , having inadequate clinical and histopathological data , known causes that may affect fdg uptake of liverspleen or bone marrow ( such as drugs , anemia , any inflammatory diseases and invasive procedures ) , prior histories of treatment with granulocyte colony - stimulating factor or granulocytemacrophage colony - stimulating factor . thus , a total of 193 patients with invasive ductal carcinoma were finally included in the study . 
patients were categorized to groups according to clinicopathologic features and reticuloendothelial systems fdg uptake level was compared in these groups . we also identified a control group of 100 subjects for comparison with breast cancer patients for suvmax of liver , spleen , bone marrow , heart and lung . 
the control group was formed with women who underwent whole - body fdg - pet / ct imaging due to various indications ( pulmonary nodules , head and neck pathologies , gastrointestinal genitourinarymusculoskeletal system diseases ) that were suspected to be malignancy clinically or radiologically and did not have any abnormal findings on the pet imaging . 
 they have similar ages and inclusionexclusion criteria with breast cancer patients . subjects preparation and pet / ct imaging protocol all subjects fasted , except for glucose - free oral hydration , for at least 6 h before the iv injection of 370555 mbq ( 1015 mci ) of fdg . 
at the time of the tracer injection , blood glucose levels were checked and confirmed to be less than 150 mg / dl in all patients . all fdg - pet / ct examinations were performed using a pet / ct system ( biograph lso ; siemens medical solutions ) , combining a dedicated , full - ring pet scanner . 
pet scanner integrated with a dual - section helical ct scanner ( somatom emotion ; siemens ) acquired the coregistration of pet and ct images in one session . pet imaging was performed 60 min after injection , extending from the vertex to the upper thigh , with 58 bed positions of 3 min each . 
ct imaging was performed ( 130 kv , 30 ma , 5 mm slice thickness ) within 1 min before pet imaging with the patient in precisely the same position ; no iv . 
the ct data were used for attenuation correction and fusion , and images were reconstructed by 2d iterative reconstruction using a standard ordered - subset expectation maximization ( osem ) algorithm . 1 3 radiol med ( 2017 ) 122 : 785792 image analysis histopathological evaluation the pet / ct images were carefully evaluated by one experienced nuclear medicine physician . 
pet , ct and fused whole - body images displayed in axial , coronal and sagittal planes were available for review . a semiquantitative analysis of fdg activity was measured as suvmax using the software programme . 
it was calculated as decay - corrected activity ( kbq ) per milliliter of tissue volume per injected f - 18 fdg activity ( kbq ) per body mass ( g )  . roi specification for suvmax measurement after image reconstruction , abnormal fdg uptake was defined as a higher intensity than the surrounding tissues , not explained by physiological processes for visual assessment of primary lesions and lymph nodes . 
for the quantitative analysis of fdg uptake as suvmax , a region of interest ( roi ) was placed over the most intense area in the primary lesions and lymph nodes . the rois were drawn manually for obtaining suvmax of bone marrow ( bm ) , spleen and liver on the axial image of the pet / ct . 
the average longitudinalvertical diameters of elliptical roi were 2590 mm for lung . all the roi placements and suvmax measurement were performed solely by one author . the histopathologic analysis was performed using the surgically excised specimens ( mastectomy and wide local excision )  . 
the determination of the tumor type and histopathologic grading ( 1 , well differentiated ; 2 , moderately differentiated ; 3 , poorly differentiated ) was performed using the formalin - fixed paraffin - embedded tumor tissue sections cut at 5 m and stained with hematoxylin and eos immunohistochemical characterization was assessed through using primary antibodies for estrogen and progesterone receptors ( er and pr ) , and c - erbb - 2 . 
the ki - 67 proliferation index was considered high when it was > 14% of nuclear immunostaining . the patients were divided into four subgroups based on the receptor and proliferation index status as follows : 1 . 
in previous several studies [ 3 , 1113 ] , it was revealed that the activation of reticuloendothelial phagocytic function is associated with neoplastic diseases . this system and its relation to diseases have been examined by various imaging methods from past to today . positron emission tomography ( pet ) imaging techniques which are widely used today , as with many others area , have provided good improvements and advantages in the imaging of the immune system organs . in the literature , there are various pet imaging studies [ 1417 ] , which assess fdg uptake level in spleen and liver in some types of cancer . 
similarly to these studies , we found that the suvmax of the liver , spleen , and bone marrow in cancer group is statistically significantly higher than the control group . 
also , it can be explained with the mechanism that increased function or size of reticuloendothelial tissues would lead to require an increase in energy consumption and , hence , an increase in glucose utilization . due to the fact that it is the first fdg - pet / ct study demonstrating the suvmax of high res activity organs in invasive ductal breast cancer , we could not have a chance to compare our results . as shown in previous studies [ 6 , 12 , 13 , 15 , 17 ] , immune system activation is associated with some clinicopathological features in tumors . 
for this purpose , we assessed the relation of high res activity organs ( liver , spleen and bone marrow ) fdg uptake and clinicopathological features in subjects with invasive ductal breast cancer . we found that high suvmax in liver , spleen and bone marrow was significantly correlated with a large tumor size , a high histological grade , the presence of ln metastasis and lymphovascular invasion status . 
also , our study showed that er - positivity , pr - positivity , c - erbb2negativity and lower ki - 67 expression were associated significantly with lower suvmax in these organs . 
 1 3 radiol med ( 2017 ) 122 : 785792 in relation to these , significantly high suvmax was observed in high res activity organs for the worse prognostic biological subgroups such as triple negative . additionally , in multivariate analysis , we showed that the presence of nodal metastasis , ki - 67 scores and triple negative subgroup was independent variables associated with high suvmax level in spleen . as there are no fdg - pet / ct studies that examine the relationship between the clinical features of breast cancer and the high res activity organs activation , we could not compare our results directly . 
on the other hand , our results are compatible with findings obtained in other studies [ 46 , 1517 ] examining immune system activation in various cancer types by scintigraphy and pet imaging . according to our study , these clinicopathological features , which are poor prognostic indicators , were considered to be major variables associated with increased fdg uptake of reticuloendothelial tissues . although none of the cancer patients had evidence of known cause that may affect fdg uptake of liver , spleen or bone marrow , to test if there are any other factors that may affect fdg uptake in these organs , we compared the suvmax levels in heart and lung in subgroups . 
there was no statistically significant difference among the groups in terms of the in that regard , we think that the reason of the higher fdg uptake levels in reticuloendothelial tissues could be related to the increase in function or size of reticuloendothelial tissues associated with more aggressive tumor types . it is known that high fdg uptake in primary tumor was a poor prognostic factor in various cancer types . 
also , we found weak correlation between primary tumor suvmax and each of the liver , spleen and bone marrow suvmax , and it was statistically significant . under all these findings , it can be said that patients with more aggressive types of ductal breast cancers would show higher fdg uptake level in high res activity organs , and this may indicate a worse prognostic factor independent of the primary tumor suvmax . our study has several limitations . 
second , the possible differences by virtue of age in immune system activity could not be eliminated , because it was categorized only according to being under or above 45 years old . 
finally , high res activity organs were not verified by histopathology to exclude other factors affected res organs fdg uptake . conclusion the present study demonstrates that fdg uptake level in high res activity organs is associated with the presence of tumor , and also directly relating clinicopatological features for patients with invasive ductal breast cancer . 
frequency and type of exams performed before admission were analyzed across three 1 , correspond1 - month periods , namely m ing to 9061 , 6031 and 301 days before admission . 
the cost of these services was 106 , 988 ( 19 , 918 for x - rays , 73 , 956 for cts , 9502 for mrs , and 3612 for interventional procedures )  . 
in the end - of - life span , diagnostic excesses should be avoided . keywords radiology hospice end - of - life diagnostic obstinacy oncologic patients introduction in end - stage oncologic patients , care should have palliative intent . 
the world health organization considers palliative care ( pc ) as an approach that improves the quality of life of patients and their families facing the problems associated with life - threatening illness , through the prevention and relief of suffering by means of early identification and impeccable assessment and treatment of pain and other problems , physical , psychosocial and spiritual [ 1 ]  . 
the pc network in the country is entitled to give adequate assistance through two main types of care : home - based and residential care , which is supplied in hospice facilities . end - of - life caregivers should improve the patients quality of life not only by providing pain control and treatment of the other problems related to the precarious conditions of the vulnerable population they are dealing with , but also by avoiding aggressive treatments and by limiting diagnostic workup when the stage of the disease is too advanced to expect any reversion of the condition . 
this is a strategic issue , as nowadays healthcare expenditures are less 1 3 794 radiol med ( 2017 ) 122 : 793797 sustainable than in the past , and the national health service ( nhs ) of many countries is facing spending review ; for these reasons , the available resources should be appropriately allocated . to our knowledge , little is known on the use of diagnostic and interventional radiological services in the eol period of oncologic patients . 
this retrospective study aimed at the evaluation of frequency , type , and cost of diagnostic and interventional radiological exams performed on patients with end - stage oncologic diseases in the 90 days before their admission to the two hospice facilities of a nhs district in italy . materials and methods study population this retrospective observational study was conducted between january 1 , 2012 and june 30 , 2013 . 
all the stage iv oncologic patients ( m according to the tnm system ) who entered the two hospices of a nhs district in italy in the 18 - month study period were considered eligible . 
the data of the hospice patients charts were cross - checked with the radiology information system ( ris ) archive of the radiology department , which collects data from the three radiology units of the district public hospitals . 
age , sex , length of hospice stay and cancer site were recorded for each patient . the study was approved by the local ethics committee and was carried out in accordance with the declaration of helsinki for experiments involving human subjects . 
the need for informed consent was waived due to its retrospective nature . radiological exams radiological exams were categorized as follows : x - ray exams , cts , mrs and interventional procedures . 
the interventional procedures included biliary drainages , ureteral stents positioning , and pulmonary biopsies . ultrasound exams were not included in the evaluation because they were performed mainly outside the radiology department and their records were not available . statistical analysis the study variables were summarized using descriptive statistics ( mean sd , ranges , frequencies )  . 
the total 1 3 radiol med ( 2017 ) 122 : 793797 table 1 general characteristics of the study patients ( n 389 ) table 3 examined patients and radiological exams by monthly prehospice period and type of exam data are expressed as means percentages , as appropriate standard deviations or as counts and table 2 radiological exams performed on the patients ( n the 90 days before hospice admission , and their cost 389 ) in variable male sex , n ( % ) age , years length of hospice stay , days primary cancer site lung , n ( % ) colon , n ( % ) stomach , n ( % ) pancreas , n ( % ) breast , n ( % ) head and neck , n ( % ) liver , n ( % ) bladder , n ( % ) other sites , n ( % ) variable number of patients examined , n ( % ) radiological examinations , n mean per patient 25th , 50th , 75th percentile by type of exam diagnostic : x - rays , n ( % ) diagnostic : ct , n ( % ) diagnostic : mr , n ( % ) interventional , n ( % ) total cost of exams ( ) x - rays ( ) cts ( ) mrs ( ) interventional procedures ( ) cost of these services was 106 , 988 ( mean : 275 per patient ) , so distributed : 19 , 918 for x - rays , 73 , 956 for cts , 9502 for mrs , 3612 for interventional procedures ( table 2 )  . when we analyzed the proportions of examined patients and the frequencies of radiological exams across the three pre - hospice periods , we found that they all increased as hospice admission approached ( see table 3 )  . 
the 90 days before death are usually considered the terminal phase of an oncologic disease , and this was the reason why we arbitrarily decided to collect the data concerning radiological exams of the 90 days before hospice access , considering also the relatively short hospice stay before death in the majority of our patients . palliative care aims at taking care of incurable patients also by avoiding therapeutic obstinacy in the eol . 
this is a critical issue , as literature data showed that in industrialized countries up to 40% of terminal patients who did not enter home - based or residential pc facilities received chemotherapy courses in the last month of life ; when in a pc network , this high proportion decreased to only 5% [ 24 ]  . diagnostic obstinacy , which is the attempt to pose a thorough and complete diagnosis on end - of - life patients without specific therapeutic goals or improvement of the quality of life , should be avoided too . to the best of our knowledge , the current report is the first to evaluate frequency , type , and cost of radiological exams performed before hospice admission in end - stage oncologic patients . 
there are four principal findings from this study : ( 1 ) a high percentage ( 86% ) of patients with stage iv cancer underwent at least one radiological exam in the 90 days before entering hospice , most of them being diagnostic ; ( 2 ) such exams resulted in a high expenditure ; ( 3 ) the closer the date of hospice access , the higher the number of procedures performed , of patients examined , and of exams per patient , potentially configuring a form of diagnostic obstinacy ; and ( 4 ) the number and cost of radiological exams performed during hospice stay were significantly lower if compared to the 90 - day preadmission period . radiological exams at the eol have generally received scarce attention . 
evaluated the use of high - cost diagnostic imaging in patients with stage iv cancer and concluded that more than 33% of patients in the last month of life underwent at least one high - cost imaging procedure ( i.e. , ct , mr , and / or nuclear medicine imaging ) [ 5 ]  . 
notably , cts and mrs accounted for the 38% of all exams in our patients , but were responsible for the 78% of the costs : this underlined the very high expenditures sustained for such imaging . 
our results are in line with the 2012 total public expenditure for outpatients diagnostic imaging in italy studied by ciarrapico et al . , who concluded that high - cost imaging accounted for the 21% of all exams , but generated the 60% of costs [ 6 ]  . 
the population of this study is very different from ours ; however , we could observe that the findings were very similar regarding costs [ 7 ]  . interestingly , we observed that a very limited proportion of the exams were interventional procedures ( 2% )  . 
 although we were unable to retrieve the clinical reasons motivating radiological exams , we hypothesized that the majority of the interventional procedures ( e.g. , biliary drainages and ureteral stents placements ) were performed with a palliative intent . 
in this scenario , such a low number of interventional procedures at the eol was surprising , as they could reduce the discomfort of the patients with the least risk [ 8 ]  . another interesting observation from this study was that the number of radiological exams , as well as the number of patients examined , increased as hospice mission approached . 
investigated the use of drugs , therapeutic and diagnostic procedures in italian cancer patients in the last three days of life , either in hospital or in hospice : they concluded that x - rays , ultrasound and ct were significantly less used in hospice [ 10 ]  . a study by conti et al . 
reported a very low frequency of radiological exams in patients admitted to hospice : 44 x - rays performed on 497 patients ( 9% ) over a 12 - month period [ 11 ]  . 
such figures are in line with the frequency observed in our patients after hospice admission ( 6% ) , and once more highlight that in the pc network attention is given to avoid expensive and sometimes invasive and useless exams . 
palliative care physicians have a specific background on how to interact with eol patients , and this proved to ameliorate the quality of life while reducing medical care expenses [ 12 , 13 ]  . 
these conclusions cannot be drawn from our results , however we could observe that the use of radiology services was massive in terminal 1 3 radiol med ( 2017 ) 122 : 793797 oncologic patients and grew constantly during the 90 - days preadmission period . 
we do not have a straightforward explanation for this ; one could speculate that defensive medicine , with physicians put under pressure by patients and families demands , might have played a role . 
second , we did not have information on the clinical reasons prompting the use of radiological exams , and this is a significant drawback as they could be related to some extent to hospice admission . 
 fourth , this study was not designed to compare the characteristics of exams performed in patients who deceased in hospice to those in patients who deceased in hospital or at home . 
fifth , we were not able to evaluate if the decision on final hospice admission was based on radiological results , because this was only rarely explicitly mentioned in the hospice charts . 
finally , we could not exclude that the total number of radiological exams performed in the 90 - days preadmission period could have been underestimated due to accesses of hospice patients to radiology units of hospitals not involved in the study . in conclusion , the results of the current study indicated that patients with end - stage malignancies underwent frequent radiological exams before hospice admission , most of them being diagnostic . 
the closer the date of admission , the higher the number of exams performed and of patients examined , potentially configuring a form of diagnostic obstinacy , with high expenditures for the nhs . 
the idea that treatments should aim at improving the quality of life in end - stage oncologic patients , rather than prolonging life itself , should be applied also to radiological exams . 
consensus should be reached on the appropriateness criteria in diagnostic and interventional exams on terminally ill patients , in order to avoid inappropriate resources utilization and useless sufferings for the patients . acknowledgements the authors would like to thank sara cortinovis , md , for her help in the ideation of the study . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . funding this article did not receive any specific grant from funding agencies . ethical approval all procedures performed in our study , involving human participants , were in accordance with the ethical standards of the institutional ethical committee and with the 1964 helsinki declaration and its later amendments . 
 bmb has the indisputable advantage of providing defini tive histological evidence of infiltration , but also has some 1 3 624 radiol med ( 2017 ) 122 : 623632 important limitations . 
above all , it is an invasive and painful practice , not completely free from complications which , though infrequent ( 0.08% ) , may be associated with significant morbidity [ 10 ]  . 
in this context , its fundamental advantage with respect to bmb is clearly represented by the whole body technique , or rather , the possibility of evaluating the bm in toto , with simultaneous staging of the other localizations of the disease . 
it is , however , known that focal fdg uptake can also be linked to factors concomitant with or unrelated to the disease , such as reactive hyperplasia of the bm , chemotherapy , infections , inflammation and administration of granulocyte - colony stimulating factor . 
therefore , for ethical and technical reasons , it is not possible to obtain histological diagnosis of all the foci of increased uptake , the major limitation of this method is represented by the possible presence of false positives . 
in addition , all patients underwent wb - mr - dwi , as a procedure included in the protocol of initial staging before the start of treatment . among the patients included ( 26 males ; median age 53 years ) , 21 were suffering from hl and 35 from nhl , including 14 with dlbcl , 14 fl , 5 mantle cell lymphomas ( mcl ) , 1 burkitts lymphoma and 1 anaplastic t - cell lymphoma ( atcl )  . 
the main clinical characteristics of the patients included in the study are reported in table 1 . all patients provided a written informed consent to the diagnostic procedure and for mri examinations . 
the retrospective analysis was approved by the hospital ethics committee . non - targeted , unilateral bmb was performed on all patients , during analgesia , at the level of the posterior iliac spine . 
the images obtained with a value of 1000 mm / s2 were then reformatted into coronal format as multi - planar reconstruction ( mpr ) and maximumintensity projection ( mip ) and evaluated by inversion of the grayscale . 
the total duration of the examination was , on average , 45 m the technical parameters are documented in table 2 . interpretation of the images wb - mr - dwi examinations were interpreted according to per - patient and per - anatomical site analyses . in the per - patient analysis , a qualitative assessment was independently performed by two expert radiologists using as criteria for the diagnosis of bm infiltrationin agreement with the previous literature [ 2527 ] the presence of areas simultaneously characterized by : at the level of the posterior iliac spine , both right and left , paying particular attention to avoiding the site of the bmb to exclude sampling artifacts ( edema and reactive inflammation )  . 
high signal on stir ; restriction of water molecular diffusivity in dwi sequences compared to the background , or rather , a 1000 mm / high signal in the images obtained with b s2 and a low signal in the map of the apparent diffusion coefficient ( adc )  . the per - anatomical site analysis was performed using a quantitative assessment of the dwi images . 
in each patient a circular roi ( regions of interest ) of the same size were manually drawn by a single radiologist statistical analysis in the per - patient analysis , in the absence of a true gold standard , the correlation coefficient ( cohens kappa ) was calculated between the wb - mr - dwi and the method identified as the reference standard . 
wb - mri - dwi revealed in the bm multiple areas of t1 hypointensity ( a ) and stir hyper - intensity ( b ) with restriction of water molecular diffusivity both in dwi ( c ) and adc map ( d )  . 
both techniques were repeated after induction therapy ( wb - mr - dwi with t1 - weighted images ( f ) , stir ( g ) and dwi ( h ) ) demonstrating a conspicuous reduction of adc mean value for cellularity decrease on adc map ( j ) and a complete disappearance of fgd hypercaptation on petct ( i ) , consensually with the right axillary involved nodes . 
4 for quantitative analysis an roi ( region of interest ) was manually drawn on the adc map at the level of right and left posterior iliac spine evaluating the mean adc value ( a ) with a dedicated software . 
the results of the study appear to be affected , however , at least in part , by the use of bmb as a reference standard . in agreement with literature , due to its known limitations , bmb is an imperfect reference standard for evaluating the imaging examinations and , in particular , in calculating false positives and true negatives . 
in this context , the retrospective nature of our study is particularly interesting , since all patients were still subjected to bmb as they were staged before the publication of the aforementioned guidelines . 
however , they reported focal bone lesions in 4 patients with negative bmb ( false positive errors : femoral , iliac and vertebral lesions ) , causing a change in the clinical stage of the disease in two of them ( from ann arbor stage iii to stage iv ) , but without any significant impact on the choice of therapy . in the remaining histological types of nhl , where bmb remains the reference examination , wb - mr - dwi nevertheless showed a greater correlation with respect to fdg petct . 
it is interesting to note that , even in these histologies , wb - mr - dwi did not show any false negatives , correctly identifying the infiltration of bm in all patients . 
 moreover , unlike the avidity for fdg , which varies substantially according to histological type and the aggressiveness of the lymphoma , the morphological and functional parameters obtained with mri , in particular with dwi , do not seem to be influenced by the histology but only by the cellularity [ 38 ]  . conversely , the detection of focal lesions in 4 patients with negative bmb ( false positive errors : tibial , iliac , vertebral and scapular lesions ) results in justification of the non - optimal correlation values . on the whole , wb - mr - dwi has excellent diagnostic performance for bmi assessment with no false negative errors and 8 false positive focal bone lesions that all disappeared after therapy and which could therefore be considered truly positive . unfortunately , to date , in the absence of clinical studies that identify the real prognostic value of focal bm lesions in nhl , the impact that they could play in the management of these patients remains doubtful . while the role of wb - mr - dwi in identifying bm disease by means of qualitative evaluation appears very promising , our data do not support the use of quantitative analysis for identifying infiltration and for evaluating the cellularity of the bm . 
a plausible justification could be linked to the non - significant difference in terms of cellular density of the physiological and infiltrated bm . it is well known that marrow cellularity is influenced by gender , age , growth factors , inflammatory condition and metabolic factors [ 39 , 40 ]  . 
in previous studies no significant differences in adc was found between normal hypercellular marrow and lymphomatous infiltrated marrow [ 41 , 42 ]  . certainly , in this context , a practical limitation is represented by the use of only two b values , which make the evaluation less accurate [ 43 ]  . 
this article is the first description of the prevalence of different variants of pneumatisation in a northern italian population : the occurrence of such forms has to be acknowledged for their possible clinical and surgical consequences . keywords anatomical variants sphenoid sinuses radiology ct scan otorhinolaryngology * daniele gibelli daniele.gibelli@unimi.it 1 dipartimento di scienze biomediche per la salute , universit degli studi di milano , v . 
mangiagalli 31 , milan , italy 2 reparto di radiologia , ospedale fatebenefratelli , asst fatebenefratelli sacco , milan , italy 3 reparto di otorinolaringoiatria , ospedale fatebenefratelli , asst fatebenefratelli sacco , milan , italy introduction sphenoid sinuses are considered the most variable structures in the human body [ 1 ] ; the assessment of anatomical variants of sphenoid bone and sphenoid sinuses has acquired with time a growing importance in different fields of application of clinical anatomy . 
a first example is provided by the improvement of transsphenoidal surgery , first developed in 1907 , which represents a stand ard procedure for the treatment of intrasellar pathologies [ 2 ] and the exploration of cranial base according to the degree of pneumatisation . 
in addition , the pneumatisation of sphenoid sinuses may range from absent to extensive [ 4 ] , sometimes extending into anterior clinoid processes , pterygoid processes , greater wings , clivus , as well as also into other bones such as vomer , palatine and occipital bone [ 5 , 6 ]  . 
therefore , the analysis of pneumatised structured in patients has a relevant importance for a correct planning of surgical procedures [ 7 ] , as shown also by recent publications concerning the use of extended transsphenoidal approach not only to suprasellar and parasellar lesions [ 8 , 9 ] , but also to the floor of the middle cranial fossa [ 10 ] and the petrous apex [ 11 ]  . however , the variable morphology of pneumatised structures of sphenoid bone may also represent a risk for iatrogenic lesions : in fact the degree of pneumatisation is linked with the probability of exposition of important structures , namely internal carotid artery , maxillary nerve and optic nerve into the sinuses [ 4 , 7 ]  . 
in addition , pneumatisation of greater wings increases the risk of penetration into the middle cranial fossa , with consequent leakage of liquor [ 12 ]  . 1 3 576 radiol med ( 2017 ) 122 : 575580 for what concerns otorhinolaryngology , pneumatised structures may represent a risk for chronic sinusitis [ 12 ] , as well as possible involvement of maxillary and optic nerves exposed into the sphenoid sinuses , with respectively trigeminal neuralgia and visual deficit [ 1214 ]  . 
the epidemiological assessment of different variants in general population is crucial : literature has already explored the prevalence in different ethnic groups [ 4 , 1419 ] , but no study has so far analysed the italian population in depth . 
yet the exact knowledge of these variants may have relevant consequences in clinical and surgical practice . this study aims at verifying the prevalence of main anatomical variants of pneumatisation of sphenoid sinuses : the results will add a contribution to the epidemiological data already existing in the literature . materials and methods the study took into consideration 300 patients ( 150 males and 150 females ) aged between 25 and 99 years who underwent a ct scan in a hospital of milan ( northern italy )  . 
the most frequent clinical requests concerned screening for possible cranial fractures in cases of trauma ( 57.3% ) , sinusitis or nasal and paranasal symptoms ( 20.0% ) or neurological symptoms ( 12.7% ) , without differences between males and females . 
all ct scans were performed on a second - generation dual - source scanner , somatom definition flash ( siemens , forchheim , germany ) ; parameters of acquisition : kv : 120 , mas : 320 , collimation : 40 0.6 mm , tube rotation : 1 s ; reconstruction thickness : 3 mm ; reconstruction filters : h21s smooth for soft tissues and h60 sharp for bone . the analysis focused on the assessment of the type of sphenoid sinuses ( conchal , presellar , sellar and postsellar ) [ 7 ] , morphologically appreciable prevalence of the right or left side , possible accessory septa , pneumatisation of pterygoid processes , anterior clinoid processes , and dorsum sellae . 
1 sagittal multiplanar images reconstructed with bone algorithm of different types of sella turcica : a presellar : the sphenoid sinus ends anteriorly to the anterior edge of sella turcica ; b sellar : sphenoid sinus extends under sella turcica ; c retrosellar : sphenoid sinus extends posteriorly to the posterior edge of sella turcica 1 3 radiol med ( 2017 ) 122 : 575580 fig . 
3 axial ct acquisition reconstructed with bone algorithm showing hypertrophic sphenoid sinuses extending up to the greater wings , with a predominance on the left side : the left sinus is segmented by three accessory septa fig . 
5 axial ct acquisition reconstructed with bone algorithm showing an example of pneumatisation of dorsum sellae : in addition , the air space included in the posterior edge of sella turcica is divided by a septum fig . 
as other 1 3 578 radiol med ( 2017 ) 122 : 575580 sphenoid sinuses usually reach the final morphology dur ing the adolescence [ 21 ]  . iperpneumatisation is known in literature , with extension into other structures close to the sphenoid body and other bones , with possible inclusion of internal carotid artery , maxillary , vidian and optic nerves [ 14 ]  . 
variants in pneumatisation of sphenoid bones are symptomless although literature reports a case of swelling in temporal region and slight degree of axial proptosis of the left eye in a subject with high - degree pneumatised sphenoid sinuses [ 22 ]  . the epidemiologic study of variants of pneumatisation of sphenoid bone has a relevant importance to verify the possible ethnically based differences . 
a characteristic of sphenoid sinuses which seems to be strongly related to the ethnic variability is the type of sinus : from this point of view , several classifications have been proposed ; for example , hammer and radberg described three anatomic types of sphenoid sinus , conchal , presellar and sellar , being the sellar the most represented ( 86% ) [ 23 ]  . 
proposed another classification limited to the sellar category , with six types of sinuses based on the direction of pneumatisation ( sphenoid body , lateral type , clival type , lesser wing type , anterior type , combined type ) ; in their population , sellar type was represented by 98% , and among them 59.2% showed a combined type [ 24 ]  . 
sellar type seems to be predominant in different populations [ 7 , 17 , 2629 ] among which asians [ 26 , 27 ] malaysians [ 17 ] and croatians [ 7 ] , as also observed in the northern italian sample analysed in the present article . 
type of sphenoid sinus is crucial as it proved to have a relevant impact on the possible development of aberrant forms of pneumatisation , as they are more frequently observed in highly pneumatised types . 
 the review of the existing literature confirms that the prevalence of each type of sinus is widely influenced by ethnic variability [ 25 ]  . in addition , also the left prevalence of sphenoidal sinuses is confirmed by the existing reviews [ 16 ]  . 
accessory septa could represent a limit for transsphenoidal procedures and , therefore , need to be ascertained for a correct planning of surgical intervention . however , the most relevant variations can be found in the assessment of prevalence of different aberrant forms of pneumatisation ( table 1 ) : for what concerns pterygoid processes , literature highlights a prevalence ranging between 16.0 and 44% with a relevant variability , fig . 
 1 3 radiol med ( 2017 ) 122 : 575580 table 1 prevalence of the main anatomical variants of sphenoid bone in different ethnic groups and comparison with the existing literature source population no . 
this comparison stresses again the importance of population studies for a more precise description of such variants to obtain more information concerning their distribution and origin . in addition , the present study provides other points of discussion which are worth being analysed in depth by further population analyses , first of all the coexistence of different forms of pneumatisation in the same individual : in detail , the statistical analysis highlighted that subjects with a pneumatisation variant are likely to show other forms . 
in addition , surgeons have to expect that probably patients may be affected by different forms of pneumatisation . secondarily , no differences were found according to sex . the importance and limits of the present study need to be discussed : in surgical procedures , the importance of pneumatisation variants of sphenoid sinus is widely recognized , and they are accurately assessed on each patient . 
 however , the epidemiological study of these variants within the general population may provide interesting data , especially for what concerns the existence of ethnic variability and the relative diffusion of different types of morphology within different populations . 
in addition , the increase of data concerning the prevalence of different forms of pneumatisation may help in formulating hypotheses concerning their origin and development . finally , epidemiological data of pneumatisation variants in healthy population are fundamental for next studies concerning their possible role in pathological condition , such as chronic sinusitis : most of the literature in fact highlights that variant forms of pneumatisation are usually asymptomatic and cases of clinically evident symptoms are very rare [ 22 ]  . 
clearly , the most relevant matters of concern linked to pneumatised structures of sphenoid bone are represented by possible damages caused by transsphenoidal surgical approaches : however , this does not exclude that such forms may modify the aeration of pneumatised structures of cranium and , therefore , have a relation with chronic sinusitis . 
further studies on the affected patients may provide additional data . another point for future analyses concerns the possible relation of pneumatisation variants with other air cells and paranasal sinuses : for example , several authors observed a positive correlation between the pneumatisation of sphenoid sinus and mastoid air cells [ 32 , 33 ]  . 
further studies concerning this topic may provide additional information concerning the incompletely known origin of pneumatised cranial bones . in conclusion , this article first provides a description of variants of pneumatised sphenoid structures in a northern italian population . 
further studies are needed to obtain a more precise description of these variants in different populations . compliance with ethical standards conflict of interest none . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
patients with an inoperable neoplastic gdoo were consecutively recruited from 2004 to 2014 ; they were referred from all medical and surgical wards of three general hospitals located in the province of sassari , italy . patients admitted in the radiology department were managed by a multi - specialty and multi - disciplinary team , involving specialists in internal medicine , surgery , anesthesia , endoscopy , interventional radiology , nursing , nutrition . they assessed nutritional status , world health organization ( who ) performance status , potential comorbidities , and blood cell counts and chemistry [ 6 , 7 ]  . an abdominal x - ray performed by philips omnidiagnost elevation x - ray and using contrast agent ( gastrografin , bayer ) to identify site , extension and obstruction size . the ( uncoated wallflexduodenal stent selfexpansible stent , boston scientific ) , advanced over a nitrexguidewires 0.035 inch straight tip , 400 cm ( covidien ) was used to by - pass obstruction . 
its placement was carried out under fluoroscopic guidance ; however , it could be associated with endoscopic guidance in cases of poor who performance status or stenosis distal to treitz ligament . before the procedure , patients were intravenous exposed to the benzodiazepine . 1 department of radiology , universit degli studi di sassari , sassari , italy data were retrieved from the medical files using an ad - hoc electronic form , including demographic , clinical , 1 3 radiol med ( 2017 ) 122 : 564567 and epidemiological variables . 
quantitative covariates were summarized with means and standard deviations ( sd ) or medians and interquartile ranges ( iqr ) in case of a parametric or non - parametric distribution , respectively , whereas qualitative variables were described using absolute frequencies and percentages . 
the overall median ( iqr ) hospitalization stay was 4 ( 44 ) days . a normal diet was administered after a median ( iqr ) time of 2 ( 22 ) days from the procedure . 
it was prescribed a semi - liquid diet in the first 3 days following the surgical intervention . early and late complications were recorded , in particular , the following two ( 3.3% ) early adverse events were diagnosed : one ( 1.6% ) gastroduodenal perforation occurred after 11 days and 1 ( 1.6% ) occlusion due to tumor growth occurred after 10 days . 
the latter complication , categorized as late event , was recorded in 15 ( 24.6% ) patients after a mean ( sd ) period of 42 ( 2.5 ) days ; whose in five ( 33.3% ) cases a jaundice , caused by a biliary obstruction , occurred and required a placement of another stent . 
malnutrition related to the disease and to the obstruction hinders the immediate surgical intervention , requiring palliative therapy which can favors an improvement of the nutritional and a surgical intervention in the near future [ 6 ]  . stenting may represent an important palliative intervention . 
the findings retrieved from our cohort confirm previous results [ 6 , 7 ]  . success of stenting was 100% higher than those reported in other studies [ 8 , 9 ]  . prevalence of early complications ( 3% ) was lower than observed in other studies [ 1012 ]  . 
scientific literature reported studies with no significant differences comparing the two techniques [ 12 ]  . in our center , 82% of patients were treated exclusively under fluoroscopic guidance ( longer procedure ) and 18% with the endoscopic support to better detect the tumor . 
new prospective studies should be carried out to assess the financial impact of stenting , as well as their effectiveness in terms of clinical recovery and mortality . compliance with ethical standards ethical approval all procedures performed in this study were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standard . informed consent informed consent was obtained from all individual participants included in the study . conflict of interest paola crivelli declares that she has no conflict of interest . 
 subsequent anti - cancer treatment after stent insertion may increase the survival . keywords stent malignant superior vena cava syndrome introduction malignant superior vena cava ( svc ) syndrome can be caused by lung cancer , esophageal cancer , or other mediastinal tumor due to the closely anatomic relationship [ 13 ]  . 
these symptoms also decrease the quality of life during their limited survival . at present , stent insertion is usually used as the first - line treatment option in patients with svc syndrome , because stent insertion dose not interfere the subsequent anti - cancer treatment and provide instant relief of symptoms [ 79 ]  . 
tumor stage was evaluated based on the criteria of the american joint committee on cancer / international union against cancer ( ajcc / uicc )  . from june 2010 to april 2016 , 47 patients with malignant svc syndrome were treated with stent insertion in our center . 
 svc stents included sinus - xl ( optimed , ettlingen , germany ) , zilver ( cook , bloomington , indiana , usa ) , luminexx ( bard , murray hill , new jersey , usa ) , and smart ( cordis , miami lakes , florida , usa ) stents . the distal and proximal margins of stent should be at least 10 mm longer than the distal and proximal margins of obstruction , respectively . 
the stent diameter should be 2 mm larger than the svc diameter . treatment procedure diagnosis svc syndrome was diagnosed based on patients history , clinical presentation , and thoracic contrast enhanced computed tomography ( ct ) findings . 
the pressure gradient between the proximal and distal ends of the obstruction and stent was measured before and after stent insertion . if the obstruction involved svc and unilateral brachiocephalic vein ( bcv ) , recanalization of svc and the obstructed bcv was preformed . 
if the obstruction only involved svc with sufficient tumor - free landing zone ( more than 1 cm from the venous confluence ) , the stent was placed in svc . 
if the proximal margin of the involved svc was too close to the venous confluence ( within 1 cm from the venous confluence ) , the stent was placed in svc and right bcv . after treatment , all patients were administered with subcutaneous low - molecular - weight heparin ( 5000 iu / 12 h ) for 3 days , followed by oral warfarin sodiuthe international normalized ratio was maintained at 23 . definitions and endpoints technical success of svc stent insertion is defined as successful placement of the stent across the target lesion with the pressure gradient lower than 10 mmhg between the proximal and distal ends of the stent [ 8 , 9 ]  . 
in the calculation of stent patency time , patients who died without stent dysfunction and living patients without stent dysfunction were regarded as censored data [ 10 , 11 ]  . 
in the previous studies , patient survival was shorter than the cumulative stent patency owing to loss of censored data [ 11 ]  . the standard follow - up protocol included thoracic ct examination and telephone follow - up . 
primary endpoint was survival time , and secondary endpoints included procedure - related complication and stent dysfunction . statistical analysis statistical analysis was performed using spss 16.0 ( spss , inc . , chicago , il , usa )  . 
the symptoms of dyspnea , neck swelling , and upper limb swelling relieved instantly after stent insertion . followup during a mean follow - up period of 6 months ( range 10 days13 months ) , 25 patients underwent subsequent anti - cancer treatment ( chemotherapy : 11 ; radiotherapy : 7 ; chemo - radiotherapy : 7 )  . 
although bypass surgery has been reported for palliative treatment of malignant svc syndrome in selected patients , this type of surgery in terminally ill patients is difficult to justify and is rather invasive for a palliative procedure [ 15 ]  . stent insertion is a minimal invasive , simple , and effective method for patients with malignant svc syndrome [ 79 ]  . 
in addition , stent insertion dose not influence the subsequent anti - cancer treatment . approximately 1060% svc obstruction patients presented with svc and bilateral bcvs obstruction [ 79 ]  . 
in this present study , 19 patients had svc and bilateral bcvs obstruction , and all of them were successfully treated with unilateral stent insertion . although most patients with malignant svc syndrome have a short life expectancy and the stent remained patent until death [ 79 ] , recurrence of svc syndrome after initially successful stent insertion still occurs in up to 41% patients [ 7 , 8 ]  . 
 [ 8 ] reported in a single - center comparative cohort study that unilateral covered stent insertion was associated with higher cumulative stent patency time and lower stent occlusion rate than bare stent for treating svc syndrome . 
in some studies about stent insertion for patients with malignant biliary , 1 3 638 radiol med ( 2017 ) 122 : 633638 colorectal , or airway obstruction , the subsequent anti - cancer treatment after stent insertion can also prolong patients survival [ 1719 ]  . 
therefore , we have no means of comparing this approach to other treatment options . in conclusion , although further clinical trails are needed , this study demonstrated that stent insertion is a simple , safe , and effective palliative treatment for patients with malignant svc syndrome . 
subsequent anti - cancer treatment after stent insertion may prolong patients survival . compliance with ethical standards funding none . conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
 we compared a reference scan and five other dose - reducing methods with regard to effects on dose , practicality , and image quality to determine the most effective method for the reduction of the radiation dose to the eyes during ct examinations of the head . 
relative to the reference scan , the dose to the eye was reduced to 25.88% with nob - tcm , 44.53% with lead goggles , and 36.91% with a bismuth shield . 
relative to the reference scan , the mean signal - to - noise ratio ( snr ) was decreased to 8.02% with nob - tcm , 28.36% with lead goggles , and 32.95% with the bismuth shield . 
the snr of the anterior region * sang - wook yoon jansons@cha.ac.kr 1 department of radiologic technology , chungbuk health & science university , cheongju , chungcheongbuk - do 28150 , republic of korea 2 department of radiologic technology , daegu health college , daegu 41453 , republic of korea 3 department of radiologic science , college of health science , korea university , seoul 02841 , republic of korea 4 department of diagnostic radiology , cha bundang medical center , cha university , 351 , yatap - dong , bundang - gu , sungnam - si , gyunggi - do 13496 , republic of korea of interest was decreased to 11.89% with nob - tcm and 87.89% with the bismuth shield . 
nob - tcm is a superior solution for head ct , including the orbital area , due to the reduction in radiation exposure without significant loss in image quality . keywords new organ - based tube current modulation radiation dose computed tomography dose reduction image quality introduction since its public introduction in the early 1970s , computed tomography ( ct ) has revolutionized not only diagnostic radiology , but also the overall field of medicine . 
in particular , the eye lenses are at risk of radiation exposure when the head and sinuses are scanned , and the radiation effect is thought to represent a deterministic model . 
recently introduced multi - detector ct 1 3 602 radiol med ( 2017 ) 122 : 601608 ( mdct ) systems provide better image quality and better resolution compared to spiral ct ; however , these systems also cause increased radiation exposure during ct procedures [ 4 ]  . 
the international commission on radiological protection recommended that the equivalent dose limit for the lens of the eye be decreased from 150 to 20 msv / y averaged over 5 years [ 5 ]  . 
the eye lens is also considered an organ - at - risk during exposure to lower - dose radiation , especially because of the potential for cataract induction . the use of a heavy metal in - plane shield protects sensitive organs such as the breast , thyroid , and eye lens [ 6 ]  . 
tube - current modulation ( tcm ) techniques automatically adjust the tube current in the xy - plane ( angular modulation ) , along the craniocaudal axis ( z - axis modulation ) , or both , according to the attenuation of the patient and the x - ray beam direction [ 8 ]  . 
in organ - based tube current modulation ( ob - tcm ) techniques , the x - ray tube current is reduced in real - time when the x - ray beam is directed toward the breasts or other dose - sensitive organs such as table 1 routine adult head ct scanning protocol parameters acquisition mode axial detector configu0.625 mm tube voltage 120 kvp distance source to 949.147 mm x - ray tube current 320 ma distance source to 541.0 mm exposure 10 mas convolution kernel standard spacing between 20 mm focal spot 1.2 mm slices slice thickness 0.625 mm noise index ration detector patient the thyroid gland and eye lens . 
however , the first commer cially available ob - tcm was implemented during mdct to reduce the dose to radiosensitive organs through a 30% decrease in the tube current over a prescribed 90 radial arc across the anterior aspect of the patient , while increasing the tube current in the remaining radial arc . 
new organ - based tube current modulation ( nob - tcm ) was designed and developed with the intent to decrease the tube current by 30% over a prescribed 90 radial arc across the anterior aspect of the radiosensitive organ without increasing the tube current in the remaining radial arc [ 9 ]  . in this study , we compared the feasibility of nob - tcm with other dose reduction methods in terms of its effectiveness for dose reduction to the eye and for image quality during head ct . 
other dose reduction techniques involved two types of tcms ( longitudinal tcm and angular tcm )  . methods scanning technique this study was performed using a 64 mdct scanner ( optima660 ; ge healthcare , milwaukee , wi , usa )  . 
an anthropomorphic head phantom ( pbu - 60 ; kyoto kagaku , kyoto , japan ) , ct dose index ( ctdi ) head phantom ( 16 - cm diameter ) and a ge performance phantom were scanned using routine adult head ct protocols ( table 1 )  . 
 scan protocol was used in all in - plane shielding methods and tcm techniques . three types of tcms were implemented using commercial options , which are as follows : 1 , longitudinal tcm ( auto ma ) ; 2 , angular tcm ( smart scan ) ; and 3 , nobtcm ( smart ma )  . 
fom was defined by the following equation that included the snr and exposure dose ( xinc ) : snr 2 fom = xinc a higher fom value results in better image quality capability in terms of snr at a lower exposure . 
snr was defined by the following equation as the ratio of the power of a signal ( meaningful information ) and the power of background noise ( unwanted signal )  . 
ct number of roi was signal and standard deviations of roi was background noise . snr = psignal pniose results compared with the reference scan , the doses to the eye were reduced to 25.88% with nob - tcm , 44.53% with lead goggles , and 36.91% with the bismuth shield ( table 3 )  . 
the ctdivol and dlp at the ctdi head phantom were reduced to 9.39% with nob - tcm . the noise indicates differences in the ct number and the signal in the three - point roi ( anterior hole , mid - central hole , posterior hole ) with respect to radiation exposure to the ge performance phantom ( table 5 )  . 
 trends were also observed with regard to the differences in the ct numbers at each hole , positive values at the anterior hole , and negative values at the mid - central hole . 
as of 2006 , the number of ct examinations was reported to have increased by 10% per year over the past 1015 years , and accounts for 49% of the total collective radiation dose administered to patients undergoing radiological examination ; this corresponds to a 120 - fold increase in the ct collective dose since the 1980s [ 11 ]  . 
in icrp publication 60 , the limit on equivalent dose to eye lens of 150 msv in a year was based on a dose threshold of 0.52 gy for a single exposure [ 12 ]  . 
in 2011 the icrp recommended that the occupational dose limit for an equivalent dose for the lens of the eye to be reduced from 150 to 20 msv per year , averaged over defined periods of 5 years , with no single year exceeding 50 msv . 
eye lens turbidity can be induced at radiation exposure doses below the brain ct radiation value of 0.52 gy , and cataracts and secondary vision disorders can be induced at values of 4 gy or higher [ 12 , 15 ]  . 
however , current studies suggest that eye lenses are much more radiation sensitive than earlier reports indicated [ 16 ]  . the older ob - tcm method used to reduce the radiation dose to the eye resulted in a reduction in ct radiation output at the anterior side of the head , whereas radiation at the posterior side was increased as a compensatory mechanism to ensure image quality . 
nob - tcm can reduce the tube current to the anterior side of the head ( i.e. , radiosensitive eye location ) and maintain the radiation doses to other areas of the body . 
radiation shielding methods reduce the dose from a primary x - ray beam by 3050% when placed on the surface of the target organ [ 16 ]  . in this study , an in - plane shielding ct examination with bismuth shields yielded a 36.91% reduction in radiation exposure , which was similar to the dose reduction rates reported for other studies and much higher than that obtained with nob - tcm . 
however , nob - tcm or shielding materials are alternative solutions in cases of head ct involving the orbital region . 1 3 radiol med ( 2017 ) 122 : 601608 these techniques also increased the ct number and noise value at the anterior hole , compared to the reference scan . 
this technique may have a negative effect on the image quality . the average fom of the ge performance phantom image was increased with longitudinal - tcm and nobtcm , when compared with the reference scan . 
 because a high fom value indicates a relatively better system performance from the roi of radiation exposure and snr , the tcm can improve the image quality rather than the reference ct scan . 
 the nob - tcm was still the most effective technique for combined dose reduction to the eye and image quality . conclusion the nob - tcm was more efficient than in - plane shielding techniques in terms of reducing the radiation dose to the eyes and ensuring image quality . 
this method can be used to reduce the radiation dose to the eyes when the head ct includes the orbital area . acknowledgements the authors thank kyoung - a um and minjeong yun for their help in preparing the ct scanning . compliance with ethical standards conflict of interest author jung - su kim declares that he has no conflict of interest . 
data on technical success rate , procedure time , puncture performance , radiation exposure , complications , and clinical success were collected . results the technical success rate was 95.2% ( 40 / 42 )  . 
 urine leaks or stenosis carry the risk of kidney dysfunction and infections such as infected urinoma , retroperitoneal abscess , pyelonephritis , peritonitis , and urosepsis [ 2 , 3 ]  . 
demonstrated that pn is technically a failure under ultrasound guidance in 15% patients with non - dilated collecting system [ 5 ] , which makes the procedure even more challenging for patients who are obese , have ectopic kidneys and / or a retrorenal colon . 
the location of the injuries were right - sided in 23 cases ( 57.5% ) , left - sided in 15 cases ( 37.5% ) , and bilateral in 2 cases ( 5% )  . 
the etiology of injury was radical hysterectomy in 13 cases ( 32.5% ) , resection of retroperitoneal tumors in nine cases ( 22.5% ) , percutaneous nephrolithotripsy in seven cases ( 17.5% ) , caesarian section in five cases ( 12.5% ) , and ureteroscopy in four cases ( 10% )  . 
 the main reasons for failed ultrasound - guided pn included failed guidewire or nephrostomy tube insertions ( 21 kidneys ) , inability to identify the renal calyx ( 14 kidneys ) , and anatomic obstacles in potential puncture access ( 7 kidneys ) ( table 1 )  . procedures imaging acquisitions data collection total no . 
of patients male / female age ( years ) body mass index ( kg / m2 ) location of injuries clinical symptom flank and / or abdominal pain right left bilateral fever or chill urosepsis peritonitis etiology no . 
the 3d reconstructed volume was first loaded , and the skin entry point and target lesion position were manually selected from orthogonal multi - planar images and marked with a cross and a circle , respectively . 
a contrast agent ( 300 mg i / ml ; jiangsu hengrui medical company , lianyungang , china ) , diluted to 30% with saline , was slowly injected to outline the calyx and pelvis . 
the soft tip of the guidewire was oriented toward the ureteral stenosis or avulsion with the help of an angled catheter and forced gently across the iatrogenic injury segment into the distal ureter and bladder . 
1 preoperative cbct images show the planned needle path ( green line ) to the non - dilated target calyx ( green circle ) , avoiding damage to the spleen , diaphragm , and lung ( a ) real - time fluoroscopic images from bulls eye view ( b )  . 
image ( c ) shows the needle advanced along the planned needle path ( white dotted line ) from the skin entry site ( white cross ) to the target calyx ( white circle )  . 
pelviureterography showed contrast extravasation ( arrow ) ( b ) and percutaneous nephrostomy was performed under real - time fluoroscopy ( arrow ) ( b ) stenosis was first dilated with a standard low - profile highpressure angioplasty of 57 mm ( boston scientific , water own , ma ) , if needed . 
the puncture performance level was assessed by two interventional radiologists ( han x and wu g ) for each puncture on a 5 - point fair , and good , 3 scale ( 5 excellent , 4 average , 2 poor )  . 
scoring scheme for evaluation of the puncture performance was listed as follows : score 1 : unsuccessful puncture due to needle positioning error ; score 2 : successful puncture of renal collecting systems , although more than four needle repositionings or reinsertions were required ; score 3 : successful puncture of renal collecting systems , with three or four needle repositionings ; score 4 : successful puncture of renal collecting systems , with one or two needle repositionings ; and score 5 : successful puncture of renal collecting systems , with no needle repositioning . 
for patients with external drainage , if the guidewire could pass across the injured segment during every pelviureterography , the 8.5 - f external drainage catheter was exchanged with an internalexternal drainage catheter . 
an old female patient was transferred to the intensive care unit for further observation after external drainage ; however , she died after 27 days owing to sepsis from peritonitis related to the colon injury , distinct from her original iatrogenic ureteral injury . clinical outcome in all , 28 kidneys underwent externalinternal drainage , and 12 kidneys underwent external drainage during the first session . 
first analyzed the clinical value of cbct virtual navigation to obtain puncture access for percutaneous nephrolithotomy in 52 patients , and concluded that cbct may provide advantages of improved preoperative imaging , which may be the best guidance technique [ 22 ]  . 
reported their initial experience with establishing puncture access under cbct guidance in children and adolescents , which emphasized that cbct guidance is a very useful tool to establish a safe renal access , especially for patients with non - dilated collecting systems [ 23 ]  . 
analyzed 27 punctures using the same navigation for patients with complex puncture indications owing to unclear ultrasound findings or a suspicion of surrounding bowel , with puncture success rate of 88.9%. 
the clinical success rate was 72.5% and within the range found in the literature with ultrasound or / and fluoroscopy use ( 6993.9% ) [ 25 , 26 ]  . 
the rationale behind waiting several weeks is to allow the edema to subside , tissue planes to be reestablished , and any fistula to become smaller before a repair is attempted . 
external drainage alone without splinting of the damaged ureter is more likely to result in stenosis , which indicated that internalexternal drainage catheter placement should be the preferred drainage method to obtain spontaneous ureteral healing and long - term clinical efficacy . complications of pn , such as pleural injury , colon injury , and severe bleeding , can be decreased by precise imaging guidance [ 27 ]  . 
cbct virtual navigation allowed entry into the pelvicalyceal system through the tip of the calyx within brodels avascular plane , which is considered the route with the least risk of bleeding [ 28 ]  . the effective radiation dose recorded in our study was 5.9 msv , which was lower than the effective dose for conventional abdominal ct ( 7 msv ) [ 29 ] and ct guided 1 3 562 radiol med ( 2017 ) 122 : 557563 drainage procedure ( 13.5 msv ) [ 30 ] , which indicated that radiation exposure via dosing was not a significant proble real - time fluoroscopy during puncture procedure can minimize the number of cbct acquisitions and procedure time , thereby reducing patients exposure to radiation . despite its advantages , the technique does have some limitations . 
the aim of the present study is to summarize the evidence derived from the rapidly growing scientific literature on gadolinium retention in the brain and in the rest of the body . 
the main aspects that emerged were the different effects of linear and macrocyclic gbca on brain mri appearance , the evidence of gadolinium tissue retention in multiple organs , and the debated issue of the possible clinical consequences . 
 although no adverse health effects have been documented so far , updated information about gbca build - up in the body is necessary for health professionals , also in view of the increasing concern in the general population . 
however , while official guidelines are eagerly awaited , some advices may already be given , to help our radiological daily practice . keywords gadolinium - based contrast media mri dentate nucleus gadolinium retention toxicity * enrico tedeschi enrico.tedeschi@unina.it 1 neuroradiology unit , department of advanced biomedical sciences , university of naples federico ii , via s . 
pansini , 5 - 80131 naples , italy 2 department of medicine and health sciences , universit del molise , campobasso , italy introduction gadolinium - based contrast agents ( gbca ) are chemical compounds used in magnetic resonance imaging ( mri ) to exploit their paramagnetic properties , i.e. , their capability to regionally alter the mri signal of the biological compartment in which they accumulate . gadolinium ( gd ) is a paramagnetic lanthanide heavy metal , that , in its free ionic form ( gd3 + ) , can compete with ca2 + and become toxic in biological systems [ 1 ] ; therefore , it must be chelated to an organic ligand . 
commercially available gbca contain gd chelated in different forms , are usually administered intravenously , and have been used in over 100 million patients in the last 29 years [ 2 ] and in roughly 3045% of all clinical mr studies today [ 3 ]  . 
 gbca are credited with an excellent safety profile , as very few , and mostly mild , acute adverse reactions have been reported , despite the large and prolonged use ( 0.080.12% ) [ 4 , 5 ]  . once administered , gbca are eliminated from the body through the urinary , and , to a lesser extent , biliary syste in subjects with normal renal function , they are usually cleared from the blood in about 1.5 h , and completely recovered from the urine in 7 days ( > 90% in the first 12 h ) [ 6 ]  . gbca can be divided into linear and macrocyclic types , the latter being considered more stable . 
indeed , macrocyclic gbca form cage - like structures with gd3 + enclosed in the cavity of the complex and tend to have lower dissociation constants [ 7 ]  . 
the higher the dissociation constant , the more likely free gd can be released into the circulation and tissues [ 8 ]  . between 2006 and 2009 a safety issue emerged for gbca , as nephrogenic systemic fibrosis ( nsf ) , a 1 3 590 radiol med ( 2017 ) 122 : 589600 subacute / chronic disease associated with significant mor bidity , was described and put in relation to previous administration of some linear gbca in patients with renal dysfunction [ 3 ]  . 
however , once a careful evaluation of the renal glomerular filtration rate ( gfr ) has been imposed as a pre - requisite to perform a contrast - enhanced ( ce ) mri scan , the incidence of new nsf cases has almost disappeared [ 9 ]  . since 2014 , a new safety concern regarding the use of gbca has spread over the scientific community : the evidence , and the possible consequences , of long - term retention of gbca in the brain after multiple ce - mri in subjects with normal renal function . 
in fact , there are consistent and ever - growing imaging and histopathologic findings of gd accumulation in individuals with normal gfr who had received , even years earlier , multiple gbca administrations . in this review , we focused on original articles published in peer - reviewed journals in the last 3 years , aiming to : ( i ) summarize the latest evidence deriving from human and animal studies on gd retention in the body , ( ii ) evaluate the methodological aspects of the imaging findings reported so far and ( iii ) critically address the issue of the possible clinical consequences of the existing data . 
finally , some suggestions on the effects of this increased knowledge on our radiological daily practice are presented . gadolinium retention in the brain : imaging findings most ce - mri brain acquisitions exploit the property of gbca to shorten the t1 relaxation time of living tissues after extravasation in the interstitial space . 
however , it is now clear that intravenously injected gd can slowly pass an intact bbb , with mechanisms possibly involving transmetallation , specific metal transporters , or even a pathway through the csf , perivascular spaces and the glymphatic system [ 3 , 10 ]  . 
unenhanced coronal se t1 - weighted images in a patient with relapsingremitting multiple sclerosis at diagnosis ( a ) and in a follow - up study 6 years later ( b ) , after 6 injections of magnevist . 
also note worsening of the supratentorial demyelinating lesions , leading to increased axonal loss the pioneering publication was a retrospective study in 19 brain tumor patients , who underwent at least 6 examinations with linear gbca ( gadopentate dimeglumine , magnevist and / or gadodiamide , omniscan ) , compared with 16 patients who received at least 6 unenhanced mri [ 12 ]  . 
this different behavior of the two gbca classes supports the hypothesis that the observed t1 shortening is related to dissociation of the gd ion from its chelating ligand molecule [ 21 ]  . 
table 1 lists the main features of the gbca approved for cns imaging along with the corresponding findings reported in imaging and pathology studies in humans and animals with a normal renal function . 1 3 radiol med ( 2017 ) 122 : 589600 1 3fi 592 radiol med ( 2017 ) 122 : 589600 since 2014 , some conflicting findings have also been reported . 
for example , multiple injections of multihance were associated with significantly lower dn / middle cer ebellar peduncle and gpt t1w - si ratios compared to patients who received ( also ) omniscan [ 22 , 23 ]  . 
the reason for such susceptibility may be related to the fact that dn are preferential sites of accumulation of metallic ions and calcium [ 37 , 38 ] , as well as to their proximity to the choroid plexus of the fourth ventricle , which is known to sequester toxic heavy metals and metalloid ions [ 39 ]  . 
one may thus speculate that a transport mechanism mediates the preferential accumulation of gd in some brain regions , using the blood / csf barrier as a passageway toward the interstitium [ 40 ]  . the intriguing observation that , by increasing the administered gbca volume , gd accumulation becomes evident in other brain sites involved in the deposition of minerals and metallic ions also supports this hypothesis [ 41 ]  . 
in fact , in 13 patients who received at least 35 doses of linear gbca , a significant t1w hyperintensity was evident not only in dn and gp , but also in the substantia nigra , posterior thalamus , red nucleus , colliculi , superior cerebellar peduncle and caudate nucleus [ 36 ]  . 
in a patient who had undergone > 80 ce - mri with mixed ( linear and macrocyclic ) gbca , t1w hyperintensity was observed not only in dn and basal ganglia , but also in the cortex around the central and calcarine fissures [ 42 ]  . 
conversely , no evidence of significant t1 shortening was observed , both using conventional si [ 16 , 43 ] and relaxometry [ 44 ] methods , even after massive cumulative doses of macrocyclic gbca . 
some authors also used csf as a reference roi [ 17 , 20 ] ; however , gbcas have been shown to pass , at least temporarily , into csf [ 29 , 46 ] and , as previously mentioned , csf may actually represent a pathway to reach deep gm structures . it is currently agreed that se and gradient echo ( gre ) - t1w sequences cannot be used interchangeably for evaluating si , with some authors even preferring the latter for qualitative analysis [ 47 ]  . 
however , serial measurements should obviously be performed using the same sequence and the same field strength , possibly on the same mr scanner . to obviate some of the limitations related to qualitative parameters like si , quantitative approaches for measuring gbca - induced t1 shortening have been proposed . 
 [ 50 ] , using a validated relaxometry method [ 51 , 52 ] , assessed the r1 ( 1 / t1 ) and r2 * ( 1 / t2 * ) relaxation rates , i.e. , quantitative mri metrics intrinsically related to tissue microstructure and not affected by the entangled contrasts of the si images , or by acquisition - related confounding factors [ 53 ]  . 
it was thus demonstrated that dn t1 shortening in patients exposed to magnevist is linked only to the number of previous gbca administrations and not to r2 * changes ( and therefore possible iron build - up ) , nor to ms - related factors such as disease severity or duration . 
using another relaxometry approach , other authors showed that global and regional t1 and t2 values correlate with the number and volume of prior magnevist injections in different gray matter structures [ 54 ]  . recently , quantitative susceptibility mapping ( qsm ) has been used to evaluate dn susceptibility changes 1 3 radiol med ( 2017 ) 122 : 589600 associated with gd retention , showing significantly higher dn susceptibility values in patients exposed to gbca compared to subjects with no history of gbca administration [ 55 ]  . 
quantitative techniques such as qsm were shown useful for differentiating accumulation of paramagnetic metals from calcifications [ 57 ]  . finally , regardless of the imaging technique [ 58 ] , other sources of variability should be taken into account . 
these include the time interval between gbca administration and mri acquisition , patients characteristics such as age , type of disease , concurrent therapies [ 49 ] , and the possible interactions between different classes of gbca . 
 for example , the dn t1w - hyperintensity due to multiple magnevist injection was apparently reduced when patients were subsequently given macrocyclic gbcas , potentially indicating a washout effect or precipitation of gd [ 19 ]  . gadolinium retention in the brain : histopathologic reports in humans and in animal models important information on tissue gd deposition has also been provided by pathology studies . 
the first description of gd retention in the brain of subjects without severe renal failure was a report on 30 biopsies and surgical resections of patients with brain tumors , and was firstly related to the loss of integrity of the bbb . 
this result provided indirect evidence of transmetallation and release of dechelated gd in vivo , defined a different stability of gbca ( as gd deposition was significantly higher in patients that received omniscan than in those exposed to multihance ) and showed that gd accumulation was related to the number of gbca administrations [ 59 ]  . 
later , gd deposition has been assessed using inductively coupled plasma mass spectrometry ( icp - ms ) in post - mortem brain samples of subjects exposed to different linear gbca [ 45 , 60 , 61 ]  . in 13 autopsy subjects exposed in life to > 4 administrations of omniscan , mcdonald et al . 
notably , no signs of neuronal damage in the involved brain tissue were observed [ 45 ]  . in 5 autopsy subjects with an history of > 2 administrations of magnevist and omniscan , a significant gd concentration was observed in dn , gp , cerebellar white matter , frontal lobe cortex , and frontal lobe white matter , highest in dn and gp . 
axial unenhanced se - t1 ( a , c , e , g , i , k ) and ge - t2 * ( b , d , f , h , j , l ) images at the level of dentate nuclei ( upper row ) and basal ganglia ( lower row ) in a patient with fahrs syndrome ( ad ) , in a patient with neurodegeneration with brain iron accumulation ( eh ) , and in a patient with hypoparathyroidism ( il ) , respectively . 
variable gd deposition was found in all subjects in dn , gp , putamen , caudate nucleus , white matter and pons , with higher levels in dn and gp . 
moreover , some confounding factors could not be excluded by the authors , thus limiting the conclusions that can be drawn . several animal studies have also been conducted to evaluate gd deposition after repeated administration of different gbca using mri and / or pathology metrics . in healthy rats , robert et al . 
 [ 62 , 63 ] evaluated the si in the deep cerebellar nuclei ( dcn ) and the concentration of gd , through icp - ms , after repeated administrations of different gbca ( omniscan , multihance , and magnevist ) compared to dotarem and saline . 
both studies indicate that multiple injections of linear gbca were associated with progressive and significant t1w - hyperintensity in dcn ( highest after omniscan ) , and with gd deposition in the cerebellum , while no effects ( either histologic or at mri ) were observed after dotarem or saline administration . in a similar rat model , jost et al . 
in contrast , dcn / pons si ratio was increased after the administration of linear gbcas , most pronounced after omniscan , followed by multihance . further studies with icp - ms have shown that , by increasing the gd load from linear gbca ( by either incrementing the dose or reducing the renal clearance ) , gd deposition is present not only in the dcn , but also in cerebral cortex , subcortical brain , brainstem , olfactory bulbs and pons , [ 40 , 62 , 64 ]  . 
however , it was recently shown that , even after 12 mmol / kg of omniscan , no histopathologic changes were observed in the rat brain , and only 0.00011% of the injected dose was retained at 20 weeks [ 65 ]  . gadolinium retention beyond the brain bone bone has long been known to be a preferential site of gd deposition [ 66 ] , and likely serves as a reservoir of gd in the body [ 67 ]  . 
it has been estimated that approximately 0.251% of the injected gd may be released from the contrast agent and deposited in the bones , even in patients with normal renal function [ 68 ]  . in particular , in the resected femoral heads of patients who underwent total hip arthroplasty 38 days after cemri with omniscan or prohance , the amount of gd deposited in bone was 2.54 times higher in subjects who received the former gbca [ 69 , 70 ]  . 
this difference was not replicated in another study , where resected femoral head bone samples up to 8 years after omniscan or prohance exposure showed high concentrations of gd , especially in the trabecular bone [ 68 ]  . 
therefore , bone measures of gd accumulation have been proposed as an indirect method to indicate approximate levels of gd in brain [ 61 ]  . skin and other sites most of the information about gd deposition in the skin comes from studies in patients with nsf , who showed increased gd content both in affected and unaffected skin [ 7173 ]  . 
the first evidence of nsf was reported in 2006 , showing skin fibrosis resulting from abnormal proliferation of fibroblasts and collagen in patients with severe renal impairment after gbca administration [ 74 ]  . 
it soon became clear that , in patients with renal failure , the highest risk of nsf was associated with previous administration of linear gbca with an incomplete ring [ 75 ]  . 
in an autopsy case of a patient who died of nsf , deposition of insoluble gd - phosphate was observed in skin , liver , lungs , intestinal wall , kidney , skeletal muscles and cerebellum [ 76 ]  . 
however , while several studies suggest that impaired gd clearance leads to tissue accumulation of dissociated gd and promotes nsf development , only a tiny minority of patients with severe renal disease exposed to linear gbca developed nsf [ 3 ]  . more relevant for our purposes is the evidence of detectable gd concentration also in the skin of subjects with normal gfr exposed to gbca [ 73 ]  . 
in a brain tumor patient with normal renal function who received 61 injections of mostly linear gbca , arm and leg biopsies of deep skin layers were performed because of severe generalized joint contractures . 
high levels of gd were deposited in the skin of this subject , associated with signs of inflammation ( as depicted by an increased numbers of fibrocytes or macrophages , as well as increased cd34 immuno - reactivity in subcutaneous adipose tissue ) , in the absence of local skin alterations [ 77 ]  . using icp - ms , murata et al . 
detected a variable amount of gd deposition in the skin ( as well as brain and bone ) in a series of autopsied patients with normal renal 1 3 radiol med ( 2017 ) 122 : 589600 function who had received macrocyclic or linear gbca . 
therefore , in contrast with previous knowledge [ 78 ] , even in patients with normal renal function , in vivo clinical exposure to gbca results in gd accumulation into different body tissues such as skin , bone matrix or bra moreover , gd retention increases with repeated gbca exposure . 
data from rat studies , which have long shown gd accumulation in skin , liver , spleen , bone and brain [ 79 , 80 ] , recently confirmed the marked difference in tissue deposition between linear and macrocyclic gbca [ 81 ]  . 
however , the final form in which gd is deposited in the tissues is still uncertain and little is known about the levels of gd required to induce tissue structural changes and to achieve clinical significance in humans [ 47 ]  . clinical concerns from gadolinium retention after the almost complete disappearance of nsf by limiting or avoiding the use of gbca in subjects with advanced renal failure and employing more stable gbcas , the only unconfounded clinical events associated with gbca administration were sporadic allergic reactions [ 3 ]  . following the reports of gd retention in the brain in 2014 , a variety of symptoms arising shortly after the administration of gbca were described in patients with normal renal function . 
in some of these patients , the persistence of gd was demonstrated by its elevated concentrations in urine , hair , or in the saphena vein [ 82 , 83 ]  . 
this presumed disease process , observed in subjects with normal ( or borderline ) renal function who develop symptoms unexplained by other preexistent or subsequent diseases , has been named gadolinium deposition disease ( gdd ) [ 83 , 84 ]  . alleged gdd symptoms include tightness or excruciating pain of the arms and legs ( like sharp pins and needles , cutting , or burning ) , typically in a distal distribution ( like being fitted with extremely tight glove - and - sock ) , but also in the central torso or generalized in location . 
these symptoms usually appear from hours up to 2 months after the last ce - mri ( mostly within 1 month ) , with persistent pain in the extremities [ 83 ]  . 
however , it should be noted that the clinical picture of the presumed gd toxicity in these subjects was collected by one single research center , using an online anonymous survey where 42 patients selfreported their symptoms , without a control group . 
thus , this approach is heavily exposed to selection bias , as also stated by the authors themselves [ 83 , 85 ]  . in some patients , subcutaneous soft - tissue thickening ( gadolinium - associated plaques ) may be observed . 
in 2 patients without nsf exposed to omniscan , sclerotic bodies ( eosinophilic , collagenous , round or ovoid bodies , thought to be pathognomonic for nsf ) were found at histopathologic examination of the skin [ 86 ]  . the symptoms described might be considered as a toxic effect of gd , resembling the development of nsf . 
according to a team of patient advocates , which timely entered in the field , the reported physical symptoms of gd deposition disease are similar but not identical , and lesser in severity , to those observed in nsf [ 84 , 87 ]  . 
however , the causal relationship between gbca and chronic effects is not fully established , and only hypothesized [ 84 , 88 ]  . the reason why only a small percentage of patients develop symptoms after gbca administration is unclear , as with nsf . 
an hypothesis is that less stable gbca are more likely associated with symptoms , similarly to nsf , with other host factors , such as genetic susceptibility and / or adaptive immune response , likely playing a relevant role in determining the development of gdd [ 84 ]  . 
thus , a well - conducted , prospective evaluation of the real clinical incidence and pathogenesis of the presumed gdd is strongly warranted , especially due to the high impact of this topic not only in the scientific community , but also in non - specialized media . gd neurotoxicity has been rarely described in early cases of presumed gd - induced encephalopathy , in patients with renal dysfunction and other significant comorbidities [ 8992 ]  . 
none of the imaging studies on gd - induced t1w shortening reported neurological symptoms related to gbca administration , and no signs of tissue damage were observed in human or animal pathology studies . 
however , due to the description of nonspecific symptoms , such as pain or cognitive changes , after gd exposure [ 47 ] , further research is warranted to assess the long - term impact on public health and safety of deposition of gd in the brain . the us food and drug administration ( fda ) and the national institutes of health ( nih ) have recommended careful consideration about the indication of gbca , by limiting gbca use to clinical circumstances in which the additional information provided by the contrast is 1 3 596 radiol med ( 2017 ) 122 : 589600 necessary [ 95 ] , and suggested the preferential use of macrocyclic agents [ 96 ]  . 
in january 2017 , the european medicines agency ( ema ) has announced that its pharmacovigilance risk assessment committee ( prac ) will continue to evaluate the risk of gd deposition , and that , once pracs recommendations will be issued , the agencys committee for medicinal products for human use will adopt a definite position . 
 regarding the presumed gdd , the drug safety communication of the us - fda declared that , despite patients selfreports , to date there are no discernable clinical features reasonably linked to gbca administration [ 95 ]  . thus , several clinical questions remain open [ 98 ] : does gd retention affect the function of the tissues where it is deposited and lead to clinical consequences ? does gdd exist and , eventually , is it doseor gbcadependent ? is the gd deposition in the brain one manifestation of a more complex gd deposition syndrome that may also encompass nsf ? what is the role of immune system components and genetics in determining different symptoms ? for all these reasons , a systematic scientific approach is necessary to this delicate matter , which has manifold medical and legal implications [ 93 ]  . 
until additional information is obtained , radiologists and clinicians should work together to monitor the development of nsf - like disease or toxicity symptoms allegedly related to gbca administration in patients with normal renal function , without however scaremongering patients undergoing a ce - mri scan . 
 in such cases , a 24 - h urine testing may be useful for confirming the presence of gd > 30 days after the most recent gbca administration [ 84 ]  . conclusions : what we can do some final considerations and practical suggestions may be summarized from this review of the available literature about gd retention , while waiting for official guidelines and consensus statements developed by major national / international scientific radiological societies or from an international strategy of cooperation , such as the recently established international gadolinium retention evaluation consortium , that involves several worldwide scientists [ 98 ]  . first , in patients referred for a ce - mri , we should try to obtain all information on possible previous gbca administrations and evaluate the need of contrast administration even more critically than ever , especially in pediatric cases . 
 in this respect , the idea of creating and updating an individual gbca administration passport is warranted [ 98 ]  . second , the preferential use of macrocyclic gbcas , due to their higher stability over the linear types , is recommended . 
however , if macrocyclic gbcas are unavailable and a ce - mri is clinically indicated , we believe that linear gbca may be administered , since all gbcas provide essential radiological information with exceedingly positive risk / benefit ratio for the diagnostic challenge of individual patients . third , the presence of t1w hyperintensity in the dn ( or in any other brain region ) should always be described in our reports , and may prompt careful questioning of the patient about the history of prior gd administration . 
therefore , we should not deny the patients a sure benefit in fear of a possible harm . as radiologists we are given a delicate role in providing our patients balanced information on a largely unknown situation . 
a truly informed consent must be obtained from the patient or parent before gbca administration , clearly explaining them the potential risk that gd may be deposited in their body , with still unknown ( but possibly unremarkable ) clinical consequences . 
dannunzio , via dei vestini , 66100 chieti , italy 2 complex structure medical physics , scientific institute hospital citt della salute e della scienza , c.so bramante , 88 , 10126 turin , italy 3 department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 4 department of medical physics , a.s.l. 
lanciano - vastochieti , chieti , italy 5 department of radiology , scientific institute hospital casa sollievo della sofferenza , viale cappuccini 1 , 71013 san giovanni rotondo , fg , italy results the reference protocol with large fov , high resolution quality images , 95 kvp , 5 ma and acquisition time of 24 s resulted in a dap value of 1556 mgy cm2 instead the protocol with reduced kvp from 95 to 80 kvp translated into a value of dap inferior to 35% ( from 1556 to 1013 mgy cm2 )  . 
going from a high resolution to a normal resolution , there was a reduction of the acquisition time to 15 s which allowed further dose reduction of approximately 40% ( 628 mgy cm2 ) ; this protocol resulted in a value of effective dose of 35 microsievert ( sv )  . 
the reason of their frequent use is 1 3 582 radiol med ( 2017 ) 122 : 581588 represented by low costs , ease of execution and low radiation doses to the patient . 
however , not always the anatomical details of these methods are optimal . at the time , other imaging methods , such as computed tomography ( ct ) , are used in odontoiatric radiology changing the way we look at a variety of common diagnostic and treatment issues in daily dental practice . 
ct can be used where more anatomical details are needed and in clinical conditions such as pathologies and traumas in the maxillofacial region , pre surgical implant treatment planning and evaluation of the temporomandibular joint . despite many benefits of ct compared to the other methods , it is not routinely used in dentistry for the high costs , large space needed , long scanning time and high radiation dose provided to patients . cone beam ct ( cbct ) has recently been developed . 
 it allows a shorter scanning time whilst the radiation dose is up to ten times lower compared with helical ct scans [ 1 , 2 ] and the costs significantly reduced . 
the amount of radiation exposure is much lower than helical ct with higher spatial resolution [ 3 , 4 ] , because the voxel size may be as low as 0.2 mm ( it is 0.51 mm for most fan - beam units )  . since its first applications , cbct has been increasingly used for three - dimensional volumetric assessment of the craniofacial region and now is considered the examination of choice in many instances , since it provides high resolution imaging and diagnostic reliability with a positive risk benefit balance [ 5 ]  . 
its use is also recommended in odontoiatric practice for impacted teeth [ 6 ] , temporomandibular joint evaluations [ 7 , 8 ] , 3d views of the upper airways , assessment of maxillofacial growth and dental age estimation . 
cbct has also demonstrated validity for biomechanical simulations , models of bone remodeling , simulations for orthodontic surgical planning [ 9 ] , and measurements taken by digitizing points in 3d coordinates . despite all these advantages , there are still many questions on the use of this method in the routinely evaluation of the patients especially in pediatric age and these concerns focus on the radiation dose that , although considerably less than the helical ct , remains higher than the conventional radiographic studies ones . 
in literature there are many studies of comparison but they are characterized by an enormous variability in cbct related doses , ranging from 68 to 1073 sv [ 10 ] depending on the study protocols . the aim of this prospective study was to evaluate lowdose cbct protocols regarding images quality and radiation doses . methods and materials dose measurements in terms of dose area product ( dap ) were measured for different diagnostic protocols acquired by pax zenith 3d cbct ( vatech , korea ) and for conventional opt ortophos ( sirona dental systems , bernsheim , germany )  . 
fifty - eight locations have been used for the measurements in order to have a good sampling for all the involved organs at risk ( bone marrow , bone surface , brain , salivary glands , thyroid , oral mucosa , extrathoracic airway , esophagus and lymph nodes )  . 
the calculation of the effective doses was based on the international commission on radiological protections ( icrp ) 2007 recommendations [ 14 ]  . to obtain dose reduction we tested five different protocols and in particular we reduced kvp from 95 to 80 and acquisition time from 24 to 15 s . all parameters used for the five different cbct protocols are reported in table 1 . the rando phantom was positioned in such a way as to simulate the actual exam conditions . 
fifteen repeated acquisitions were made , so as to obtain values of absorbed dose compatible with the sensitivity of radiochromic film , even for peripheral sites affected only by scattered radiation . 
1 panoramic ( a ) and cephalometric ( b ) reconstructed images of the anthropomorphic phantom obtained from cbct with protocol 1 : fov of 240 190 mm , 95 kvp , 5 ma and acquisition time of 24 s protocol , with a difference of 18% . 
these results were submitted to the equipment technicians and they were asked to correct the determination methods for this dosimetry indicator . indeed , while the measured values are compatible with the dependencies expected by the exposure parameters ( quadratic dependence on the voltage value which is linear with the exposure time and the beam section ) , the values displayed by the machine do not reflect these trends , as noted , for example in the transition from 95 to 80 kv , which translates into a reduction of the dap displayed only by 7% . 
this experience underlines the importance of dap accuracy verification by a medical physicist , as also evidenced in the european guidelines [ 15 ] ; it is mandatory to carry out regular quality controls to calibrate the most of the equipment as this problem is often found by medical physicists . measurements were then carried out with orthopantomograph equipment with cefalometro siemens ortophos , and the results are showed in table 4 . as it can be observed , the value of the total dap obtained for a panoramic acquisition and the two skull projections with adult parameters leads to a value of dap 123 mgy cm2 , that is equal to about one - fifth of the value of dap for the low - dose cbct protocol . evaluation of effective dose and dose to organs measurements of effective dose and dose to organs were carried out for the third protocol that is the tested protocol proposed for the complete evaluation of the maxillofacial region . applying the weight coefficients defined in the icrp 103 , 2007 [ 14 ] a value of the effective dose of 35.4 sv has been obtained . the calculation made by the program pcxmc , considering the geometrical parameters and the measured value of dap , gives a result of effective dose of 36.8 sv , in perfect agreement with the experimental value obtained . 
the individual assessments of dose to the organs differ less than 30% , which is justified by several factors , and in particular by the different conformation of the phantom which is geometric and not anthropomorphic in the calculation program . so , although the results should be validated with at least one repetition of the measurements , the good correspondence with the data obtained through simulation provides a significant confirmation . the relationship between effective dose and dap results therefore in 0.056 sv for mgy cm2 , less than the value of about 0.1 found in other evaluation works for cbct examinations , with smaller fields of view . 
this difference is attributable to the different distribution of the dose to the organs with the extended volume of 24 19 cwith the same amount of dap the dose to the thyroid significantly increases , but the dose to other organs significantly decreases , including the primary bea indeed with equal dap , that is to switch from one volume of 14 10 to one of 24 19 , means to triple the section of the beam and reduce the dose to a third punctual axis . because of time constraints , it was not possible to evaluate effective dose of the traditional methods , but it was possible to estimate it on the basis of dap measurements 1 3 radiol med ( 2017 ) 122 : 581588 within the craniofacial complex . 
nonstandard orthodontic cases , such as impacted tooth , supernumerary odontomas , or unexpected radiologic observations , such as pathologic lesions or incidental findings , are best visualized with the 3d cbct scan . 
cbct is also be indicated when conventional radiographs suggest a direct inter - relationship between a mandibular third molar and the mandibular canal or for cross - sectional imaging prior to implant placement . 
advanced cbct software applications can also be used to quantify airway space ( relevant for sleep apnea cases ) , to perform superimpositions of objects at different time points to semiquantitatively visualize changes ( e.g. , mandibular growth , temporomandibular joint , airway ) , and generate digital dental models to streamline the workflow in the dental clinic . patient radiation dose is one of the main issues in dental ct examinations and it was investigated in several studies . 
although the related effective dose is lower than most other ct examinations involving thorax and abdomen anatomical districts , there is concern about radiation dose in dental ct as a consequence of the frequency of dental examinations and of the repetition on the same subject , especially for pediatric patients . 
therefore , it is important to know the dental ct patient dose for all machines and protocols , in order to optimize acquisition parameters and to minimize the related radiological risk . 
generally the results show doses for msct equipment ranging from eight to ten times the cbct doses , but it must be underlined that there is a great variability in the cbct protocol definition and often there are possibilities of optimization which have been not completely investigated [ 16 ]  . cbct imaging protocols should take into consideration the relative advantages of this technology over routine radiography , including the quality of the information derived , its potential impact on diagnosis and treatment planning , the ease of use and financial costs . 
as stated in the guidelines on cbct for dental and maxillofacial radiology published by various scientific societies in europe and america , cbct should be used when the question for which imaging is required cannot be obtained adequately by lower dose fig . 
 [ 13 ] , a coefficient from dap to effective dose for panoramic examinations of 0.08 sv mgy cm2 was considered , so that for our panoramic examination there would be an effective dose of about 3 sv . 
in total we obtain about 8 sv , equivalent to about one - fourth of the effective dose associated with cbct . discussion cbct software can manipulate the digital imaging and communications in medicine ( dicom ) data to visualize anatomic structures and accurately display relationships 1 3 586 radiol med ( 2017 ) 122 : 581588 fig . 
3 panoramic ( a ) and cephalometric ( b ) reconstructed images of the anthropomorphic phantom obtained from cbct with low - dose protocol ( protocol 3 ) : fov of 240 190 mm , 80 kvp , 5 ma and acquisition time of 15 s fig . 
it is obvious that all stakeholders have a responsibility to deliver radiographic technology to patients in a responsible way so that the diagnostic accuracy is maximized and radiation doses kept as low as achievable . 
cbct equipment should offer a choice of volume sizes and examinations have to use the smallest that is compatible with the clinical situation if this provides less radiation dose to the patients . our study is not finalized to evaluate guidelines for cbct or to suggest protocols according to the clinical indication , as defined by scientific societies , but to demonstrate that cbct good quality images can be obtained using low - dose protocols with an effective dose to the organs as low as 35 microsievert even when a full fov is needed for clinical purposes . 
in 19902015 , there were nearly 2 million new cases per year worldwide accounting for the 11.5% of all new cancer diagnoses and 19.7% of the deaths [ 1 ]  . 
in particular , low - dose ct screening demonstrated a 6.7% reduction in the death rate compared to chest x - ray with a positive screening test rate for lung cancer detection of 24.2% , compared to 6.9% for conventional x - ray [ 4 ]  . 
analogous results were reached in another study demonstrating that overall survival for patients with lung cancer was six times higher for patients that underwent chest ct [ 5 , 6 ]  . 
the use of ct as a screening test has 1 3 radiol med ( 2017 ) 122 : 568574 nonetheless recently prevailed over the concern for the cost and the radiation burden [ 7 , 8 ]  . 
the effective dose associated with low - dose ct used in screening programs has been evaluated retrospectively on a large cohort of patients to be about 2 msv [ 9 ]  . 
this is much lower than the effective dose used in a conventional ct scan ( 7 msv ) [ 10 ] , but still two orders of magnitude higher than the effective dose of x - ray scan ( 0.02 msv ) [ 11 , 12 ]  . digital tomosynthesis ( dts ) is a limited angle tomography that allows reconstruction of sagittal images from a set of projection acquired over a relatively small angle of x - ray tube movement [ 13 ]  . 
the objective of this investigation was to compare the detection of dts and ct in this cohort of patients . patients and methods each subject of sos , after signing informed consent , underwent dts examinations . 
 briefly , current or former smoker with a smoking history of at least 20 pack - years , aged 4575 years with no previous history of cancer in the past 5 years , and no chest ct study in the 12 months before enrolment underwent a dts . 
subjects , with an uncertain non - calcific nodule larger than 5 mm or with multiple nodules on dts , were addressed to diagnostic ct and managed in keeping with the fleischner society guidelines [ 19 ] for the management of small pulmonary nodules . 
twelve underwent surgery , while six that were in advanced stage ( iiib and iv ) of disease underwent chemotherapy and / or radiotherapy . radiographic technique and dose estimation dts was performed with discovery xr650 ( ge healthcare , milwaukee , wi , usa )  . 
based on organ doses , the loss of life expectancy ( lle ) and the risk of exposure - induced death ( reid ) were calculated for lung cancer and breast cancer using beirvii [ 21 ] model . image analysis two radiologists with 5 and 20 years of experience analyzed the images independently . 
the number of nodules for subjects as well as the positions , right upper , right middle , right lower , left upper , left lower lobes , or extra - pleural , was reported . 
nodule dimensions were measured on the larger diameter and allocated into four classes : < 5 mm , 58 mm , 810 mm , and > 10 m since dts is a quite novel technique and , at the time of study start , no experience existed on its diagnostic accuracy , pleural thickenings and peri - fissural nodes were also described . 
the nodules found in ct and dts , based on their characteristics , position , and dimension , were 1 3 classified in 5 categories of malignancies , similar to those defined by lung - rads [ 22 ] as shown in table 1 . 
the ct was used as gold standard for lung nodule identification . students t test for continuous variable , mcnemars test for categorical , and wilcoxon test for ordinal categories were applied to paired sample . 
the nodules not seen by dts and revealed in ct were only 5 , and were distributed evenly through the different class : 1 smaller than 5 mm , 1 between 5 and 8 mm , and 3 between 8 and 10 mthirtyfour nodules were seen on dts but were not confirmed by ct . 
difference between nodule diameters as measured by dts and ct was not significant measured in dts and ct was 0.08 the number of nodules showing different radiological appearance is shown in table 3 . 
 the development of dts aimed to eliminate over - lapping anatomy , thus providing greater sensitivity in nodule detection at a lower dose and cost compared to ct examinations [ 24 ]  . 
reporting effective dose along with medical imaging is always significant but particularly relevant when dealing with screening programs that involve subjects that , besides being at high risk for lung cancer , at the time of examination , have no clinically symptoms . 
this is a direct consequence of the design of these studies that were conceived to test dts on a population of subjects that already performed , for different reasons , a ct scan . 
the major limitation of our prospective study was that we could not calculate sensitivity because dts was performed as the first exam , while ct was per formed only if non - calcific nodules larger than 5 mm and / or multiple nodules were present . 
within this prospective investigation , we hence primarily concentrated on the characteristics of the nodule in dts using the ct as the reference and tried to apply a lung classification to correlate it with prognosis . firstly we observed that the numbers of nodules detected by the two diagnostic modalities are comparable , with 157 / 213 ( 74% ) of the nodules being correctly classified by dts with respect to ct . 
the relatively higher number of nodules detected in dts ( 213 ) with respect to ct ( 168 ) , in particular for small nodule size , is probably due to the difficulty in identifying clearly the nodules because of the image blurring in the coronal plane as could be seen in figs . 
the position of the nodules in the lobes reflects the non - easy association of nodules to lung lobes more than an actual difference between the two methodologies and the values we found are comparable to those of the literature [ 28 ]  . 
besides , there is a real difficulty in describing nodules that are adjacent to the thoracic wall in dts with respect to ct , because of the spill - in of higher density region into the lung . 
the relatively low number of nodules detected by ct and not by dts is in agreement with other findings in the literature that show sensitivities of 9195% [ 16 ] and of 92% [ 27 ]  . 
with respect to other publications that shows a lower sensitivity , we used a narrower slice thickness ( 3 mm with respect to 5 mm ) and an additional filtration of 0.2 mmcu that possibly enhanced contrast and resolution . 
differently , if we consider lowdensity nodules , ct found three ground glass nodules that were not correctly described by dts confirming the difficulty of dts in detecting sub - solid nodules [ 27 ]  . 
figure 3 shows an example of a ground glass nodule seen by ct and dts in the left upper lung . 14 / 22 ( 64% ) of the nodules were correctly calcified as calcific by dts , raising to 13 / 16 ( 81% ) if we consider nodules larger than 5 mm , in line with the 83% for nodules larger than 4 mm reported by langer et al . 
this is in line with other findings [ 29 ] in the literature inferring that the blurring in the sagittal direction could falsely enlarge the nodule . within this investigation , we use the lung - rads [ 22 ] classification for the malignancies of the nodules . 
even if the differences in classes between ct and dts were not statistically significant , we could see how dts has a slight tendency in up - staging , with some nodules being classified as 1 in ct and as 23 in dts . 
the auc of ct in our study is a little lower than what proposed in nlst trial that was 0.93 [ 31 ] but , as we said , used a slightly different classification . conclusions dts detected and correctly classify 74% of the solid , partially solid , and ground glass opacity nodules seen by ct , but lost 4 nodules identified by ct . 
small and low - density nodules are difficult to be identified by dts , but 86% of the nodules were correctly classified as suspicious / nonsuspicious using lung - rads classification . 
santa croce e carle , the hospital where the study was performed , provided logistic support , telephone lines , software , computer assistance , and an office free of charge . compliance with ethical standards fundings grant support for the sos clinical trial was provided by cassa di risparmio di cuneo foundation . conflict of interests the authors declare that they have not conflict of interests . ethical approval all applicable international , national , and institutional guidelines for the care and use of animals were followed . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institution and national research committee and with the 1964 helsinki declaration and its later amendments of comparable ethical standards . 
descriptive statistics regarding age , gender , type of complication , diagnostic and therapeutic modalities were calculated and presented as number and percentage . results our series consisted of 18 girls and 21 boys . 
the indications for neuroradiological imaging were convulsion and alteration of mental status . conclusion these central nervous system complications may present in a variable spectrum and convulsions and altered mental state were the most frequent clinical pictures . 
clinical history , careful examination and integrated analysis of radiologic data as well as close collaboration and multidisciplinary approach are of utmost importance for establishing the diagnosis rapidly and accurately . keywords liver transplantation neurologic complication children magnetic resonance imaging introduction liver transplantation ( lt ) is the only curative treatment in patients with end - stage liver disease , and neurological complications can affect up to one - third of cases after the transplantation procedure [ 1 , 2 ]  . 
the rates of morbidity and mortality due to cns complications after lt are reported as high as 19 and 47% [ 3 ]  . neurologic complications may develop due to the transplantation itself , or a previously identified organ failure , or both conditions . 
alteration of mental status , seizures , and focal motor deficits may occur , and these morbidities can be associated with several pathogenetic factors like poorly 1 3 618 radiol med ( 2017 ) 122 : 617622 functioning graft , intracranial hemorrhage , cerebral infarctions , infections , or immunosuppressive drug toxicity . 
cerebral atrophy , stroke , meningitis , hemorrhage , cerebrovascular infarct , cerebral abscess , encephalopathy , central pontine myelinolysis , cognitive decline , tremor , peripheral neuropathy and sinus thrombosis are the most frequent neurologic complications reported in lt patients [ 5 ]  . 
both computerized tomography ( ct ) scans and magnetic resonance images ( mri ) may be utilized for imaging in patients that develop cns complications after lt [ 6 ]  . 
increased awareness on the clinical and radiologic findings linked with possible cns complications subsequent transplantation is important to establish the diagnosis and initiate the appropriate treatment without delay [ 5 ]  . the range of indications for lt in pediatric patients is different from adults , and a different spectrum of complications is more likely in children . 
the aim of the current study was to share our experience with cns complications in pediatric lt patients with emphasis on the radiological findings derived from mri . patients and methods study design this retrospective study was carried out following the approval of local institutional review board . 
out of these 300 cases , the case records of 39 pediatric patients ( 18 girls , 21 boys ) who developed acute neurologic signs and symptoms following the procedure were reviewed . 
neuroradiologic imaging was performed using cranial mri . basic descriptive data ( age , sex ) , indications for lt , spectrum of cns complications after lt , initial time of each complication , diagnosis , treatment and follow - up were recorded . 
magnetic resonance images were performed when clinically indicated [ 6 ]  . diagnosis of cns complication was established by pediatric neurologists with respect to history , neurological examination and neuroradiological studies including mri and eeg . 
preoperative neurological examination and postoperative neuropsychological assessment were carried out routinely . statistical analysis descriptive statistics regarding age , gender , type of complication , diagnostic and therapeutic modalities were calculated and presented as number and percentage . results our series consisted of 18 girls and 21 boys with an 56.4 months ( range 15204 )  . 
as average age of 95.7 13 , it can be seen in table 1 , cryptogenic hepatitis ( n 33.3% ) , metabolic diseases ( wilsons disease , tyrosinemia and glycogen storage disease ) ( n 7 , 17.4% ) and fulminant toxic hepatitis ( n 5 , 12.8% ) constitute the most frequent indications for lt . 
we suggest that mri may provide useful data for establishing the diagnosis of cns complication after lt procedure . liver transplantation is a dynamic field in modern medicine and can be a life - saving option for patients with the end - stage liver disease . 
however , the clinical course after lt must be monitored closely since neurologic table 1 indications for liver transplantation in our pediatric population number ( % ) 13 ( 33.3 ) 5 ( 12.8 ) 5 ( 12.2 ) 3 ( 7.7 ) 3 ( 7.7 ) 2 ( 5.1 ) 2 ( 5.1 ) 1 ( 2.6 ) 1 ( 2.6 ) 1 ( 2.6 ) 1 ( 2.6 ) 1 ( 2.6 ) 1 ( 2.6 ) indication cryptogenic hepatitis fulminant toxic hepatitis wilsons disease biliary atresia fulminant hepatitis a hepatoblastoma carole syndrome biliary cirrhosis chronic portal vein thrombosis autoimmune hepatitis tyrosinemia hepatocellular carcinoma glycogen storage disease indication convulsion alteration of mental status tremor visual impairment headache fever cardiopulmonary arrest table 2 indications for neuroradiologic imaging complications that may lead to mortality can occur . 
the incidence of cns complications after lt ranges from 10 to 75% and this wide range may be linked with various inclusion criteria , the definition of cns complications and observation period [ 10 ]  . 
due to the time - based course of cns complication after lt , the majority of complications ( 80% ) occur within one month after transplantation [ 11 ]  . 
this issue gains more importance in pediatric patients for whom the clinical picture may deteriorate abruptly , and morbidity and mortality may develop without very prominent clinical signs and symptoms . after lt , we observed that pres was diagnosed with mri . 
its etiology is not understood completely , but it may be linked to a breakdown in cerebral autoregulation that leads to leakage of the fluid into the interstitium [ 12 , 13 ]  . 
it may occur due to immunosuppressive drug toxicity , and typical radiologic changes involve edema in white matter with symmetrical hyperintense signals in the posterior hemispheres on t2 weighted images [ 5 ]  . 
the etiology was attributed to pres which was linked with table 3 findings derived from magnetic resonance images ( n 45 ) finding normal number ( % ) posterior reversible encephalopathy diffuse cerebral edema 11 ( 28.2 ) diffuse cerebral atrophy 9 ( 23 ) 6 ( 15.4 ) 5 ( 12.8 ) 4 ( 10.3 ) 2 ( 5.1 ) 2 ( 5.1 ) arterial ischemic stroke hyperintensity in basal ganglia changes reflecting chronic infarct intracranial fungal abscesses intraparenchymal hemorrhage hemorrhagic infarct number ( % ) 12 ( 26.7 ) 8 ( 17.8 ) 6 ( 13.3 ) 6 ( 13.3 ) 5 ( 11.1 ) 4 ( 8.9 ) 1 ( 2.2 ) 1 ( 2.2 ) 1 ( 2.2 ) 1 ( 2.2 ) 1 3 620 fig . 
arrows show these findings which are consistent with pres radiol med ( 2017 ) 122 : 617622 tacrolimus toxicity , intracerebral hemorrhage , and electrolyte disturbances . predisposing factors for cns complications after lt include impaired host defense , glucose intolerance , hyperlipidemia , leukopenia and hypertension . 
selection of the appropriate mode of imaging as well as the increased awareness on the significance of radiologic findings is crucial for setting diagnosis timely and starting the appropriate treatment without delay . 
careful assessment of the initial manifestation and symptom may be useful for prediction of the etiologic diagnosis [ 1 , 9 ]  . the main restrictions of the current study include retrospective design , relatively small sample size and data limited to the experience of a single center . 
authors theorize that percutaneous injection of cyanoacrylic glue might represent an effective alternative for post - surgical enteric fistula after failure of conservative and endoscopic treatment , in particular , it might represent an alternative option to avoid surgical treatment in patients with biliary diversions as well as elderly or frail patients . authors report an overall success of the technique in 16 / 18 ( 89% ) of cases , with immediate fistula closure in 11 of 18 ( 69% )  . 
first , they only speculate from a limited series of patients , treated at their institutions with a high surgical volume and by very experienced operators in the management of post - surgical complications [ 3 , 4 ]  . 
also , the wide range of dilution of the material reported ( from 1 : 2 to 1 : 5 ) makes the technique quite variable and difficult to standardize . over the past two decades , interventional radiologists assumed an increasingly important role in the minimally invasive management of post - surgical complications . 
however , the experiences are still quite sparse , and different practices occur among different centers , depending on the availability of a dedicated interventional radiology service and the experience of the operators . until now percutaneous injection of glues to treat postsurgical fistulae has been used only in series with limited number of patients . 
even if it may seem to be a good alternative to surgical reoperation in management of patient with non - healing enteric fistulae , we want to underline how the technique is still not well defined . 
treatment plan , monitoring of thermal damage , and post - procedural assessment of treated volume are performed in real time with mri which guarantees the accuracy and safety of mrgfus [ 1 ]  . unsatisfactory responses to mrgfus have been presented in a subgroup , which is anticipated to have resulted from high fluid contents including vessels [ 2 ]  . 
it has been established that fluid content of tissue can be displayed as mr image parameter , signal intensity ( si ) on t2 - weighted mr images ( t2wi ) [ 24 ]  . 
scaled form of si ( ssi ) is reported to be strongly associated with fibroid response to mrgfus [ 5 ]  . gonadotropin - releasing hormone agonist ( gnrha ) is a superior hormone that regulates hypothalamicpituitary ovarian ( hpo ) axis and ultimately regulates the secretion of sex steroid hormones by ovary . 
 according to a recent histological study , micro - vessel density measured with von willebrand factor , a vessel marker , was significantly decreased following an administration of gnrha [ 6 ]  . gnrha is generally used as pre - treatment to facilitate myomectomy , which can decrease fibroid volume and reduce blood loss [ 7 ]  . 
the authors speculated that gnrha reduces the vascularity of uterine fibroids and enhances responsiveness to heat energy . meanwhile , the usual protocol is composed of three or six cycles of gnrha administered every month and accompanies non - negligible disadvantages [ 7 ]  . 
blood flow to fibroids was reported to decrease within four weeks of gnrha administration [ 9 ]  . we hypothesized that gnrha can reduce fluidity par tially composed of vessels of fibroid within a month and enhance the responsiveness to thermal ablation without adverse effects . 
in this study , we assessed the feasibility of a single - dose gnrha on fibroids and their relevance in mrgfus . materials and methods study design this observational pilot study was performed at mrgfus clinic in university - affiliated teaching hospital . 
after the dosage of gnrha was administered , the duration of one treatment cycle , a month , was permitted to induce the shrinkage of fibroids while reducing the risk of undetected malignancy in study group . 
to analyze the effect of gnrha on treatment outcomes , a control group was retrospectively assembled from the patients who underwent mrgfus without the pre - treatment during the same study period . 
informed consent was obtained from all individual participants included in the prospective test arm . patient selection for mrgfus according to a standard of care in our institute , patient suitability for the mrgfus was determined by screening mr examinations conducted for screening . 
in the screening procedure , patients were positioned prone , feet first , on the mr table inside 1.5t mri ( signa hdxt , ge healthcare , milwaukee , usa ) , using a phased array torso coil . 
to identify anatomical structures within the pelvis , t2 - weighted turbo spin echo images in axial , sagittal and coronal orientations were acquired ( tr of 4830 ms , te 120 ms , matrix size 256 144 , slice thickness 5 mm , spacing 1 mm and fov 30 cm )  . 
to evaluate the presence of hemorrhagic or fatty tissues , t1 - weighted turbo spin echo images were acquired in the axial orientation , [ with tr of 460 ms , te 11 ms , matrix size 256 144 , slice thickness 5 mm , spacing 1 mm and fov 30 cm . ] contrast - enhanced t1wi was obtained after 3 min of bolus injection of 0.1 mmol / kg body weight of gadolinium - based contrast agent ( prohance ; bracco , milan , italy )  . 
fat - saturated contrast - enhanced t1wi was performed to evaluate the hemodynamic characteristics of the fibroids and to assess their potential viability and this sequence was acquired in axial , sagittal and coronal orientations ( tr of 594 ms , te 11 ms , matrix size 256 144 , slice thickness 5 mm , spacing 1 mm and fov 30 cm )  . our criteria for patient selection were modified based on the previous literature [ 4 ]  . 
we included patients with fibroids which directly caused symptoms ( e.g. , abnormal uterine bleeding or pelvic pressure / pain ) , with less than three fibroids , with intestine away from the anterior wall of uterus , and with fibroids having relatively low si on t2wi . 
 women who ever participated in gnrha therapy or other hormonal therapy within 6 months prior to mrgfus for the purpose of managing the symptoms caused by fibroids were excluded from the study . 
in brief , after patients were positioned prone on the exablate treatment table , the radiologist defined the region of treatment ( rot ) so to cover as much of the fibroid volume as possible , while avoiding healthy tissues . 
si signal intensity , uf uterine fibroid , ssi scaled signal intensity 1 3 614 radiol med ( 2017 ) 122 : 611616 npv was divided by energy or sonication number delivered during treatment to assess the thermal dosimetry . adverse events gnrha - related adverse events were collected just before mrgfus in a month of follow - up period . 
patients in study group were given an account of climacteric symptoms such as vasomotor ( e.g. , hot flush ) , somatic ( e.g. , vaginal dryness ) , and psychological symptoms ( e.g. , anxiety and depression )  . 
si can be transformed via formula ( 1 ) to a scale , ssi , which make us to avoid somewhat subjective measurement and si of fibroid to be monitored more objectively [ 5 ]  . in present study , we could quantitatively assess the effects of gnrha on the fibroid tissues using serial mr scans . 
a hemodynamic study examined vessel indexes using color doppler sonography and showed reduction of blood flow in fibroid vessels occurs within 4 weeks of gnrha administration [ 9 ]  . 
this change was followed by a considerable reduction of main uterine artery blood flow and then a significant decrease of uterine and 1 3 radiol med ( 2017 ) 122 : 611616 fibroid volumes . 
this sequential process is well in line with results of our study where the decreased contents of fluid in fibroids were noted within a month since gnrha administration . several publications have reported that gnrha can potentiate the thermal coagulation of mrgfus . 
although they did not analyze the change of vessel density through histologic specimen or imaging parameters , they speculated that the enhanced response may be mediated by the decrease of vascularity . 
 our data also supported that gnrha improved the responsiveness of fibroid tissue in terms of npv per unit energy ( table 1 )  . furthermore , we could validate the mechanism of gnrha in mrgfus by presenting the close relationship between the characteristic of tissue and the responsiveness to thermal ablation . 
therefore , the enhanced efficiency of mrgfus treatment by gnrha was suggested to be induced by the reduction of fluid contents including vascular territory . a single - dose protocol can avoid or reduce the incidence of adverse effects of conventional three - dose protocol . 
at 4 weeks after leuprorelin depot 3.75 mg , most of the patients have no obvious side effects and after 9 weeks of treatment , the incidence of adverse events was significantly increased . 
in this study , we could not report any adverse events within a month from the pre - treatment as we expected . there are some limitations inevitable in our study design . 
we think that large randomized studies are needed to adjust these confounding factors and validate the results of our pilot study . in conclusion , we could prospectively assess that gnrha induces the reduction of fluid contents in fibroids using an objective mri parameter , ssi . 
through these mechanisms , a single dose of gnrha is suggested to be feasible and safe to contribute to the successful ablation of fibroids as a pretreatment of mrgfus . compliance with ethical standards conflict of interest author hyun park declares that he has no conflict of interest . 
the needle path was planned on a cact virtual navigation and real - time fluoroscopy systetechnical success , puncture score , procedure time , local control rate ( lcr ) , radiation exposure , complications and survival were investigated . results the technical success of interstitial 125i brachytherapy under cact guidance was 40 / 40 ( 100% )  . 
the mean survival time was 28.42.3months. conclusion cact can provide virtual navigation and real - time fluoroscopy synchronously for interstitial 125i seed implantation on pulmonary tumors . keywords c - arm computed tomography pulmonary tumors virtual navigation guidance 125i seeds brachytherapy introduction radioactive 125i seeds implantation for lung cancer is often done under conventional computed tomography ( cct ) guidance . 
multiple needle puncture needs repeated ct scans to understand the location of need and puncture access , and there are still many challenges for doubleoblique approach with an angulated trajectory of the needle , which makes the procedure difficult and time - consuming [ 13 ]  . flat detector ( fd ) - equipped angiographic cact can provide virtual navigation tool and real - time fluoroscopy with an increased flexibility in orientation of the detector system around the patient compared with cct [ 4 , 5 ]  . 
cact confirmed the needle position ( b , c ) 1 3 radiol med ( 2017 ) 122 : 829836 then the virtual path was superimposed onto the realtime fluoroscopic image . 
after the procedure , cact or fluoroscopy of the entire chest was done to confirm seed distribution and exclude procedurerelated complications . instrumentation andplanning ofimplantation the 125i radioactive seed ( atom high tech , beijing , china ) was shaped as a cylindrical titanium package , which had a size of 4.50.8mthe radioactivity of 125i was 0.8mci ; the mean energy 2735 kev ; half - life 59.6 days ; arbitrary 1.7cm ; and initial dose rate 7cgy / h . 
prior to 125i implantation , a treatment plan was made for each patient using a computerized treatment planning system ( tps ) ( yuanbo , beijing , china ) to ascertain the treatment dose . 
during the whole procedure , patients were told collection anddefinition ofdata we recorded the total procedure time ( from initial cact to the end of 125i seed implantation ) , number of cact acquisitions , number of seed implantation needles , number of 125i seeds used , the absorbed dose according to postoperative tps , complications and dosearea product ( dap ) including fluoroscopy dose and cact dose . technical success was defined as preoperativeplanned 125i seeds being implanted in the appropriate area within the tumor based on virtual navigation plan . 
the needle was advanced along the planned path of the needle ( dotted line ) from the site of skin entry ( white cross ) to the target lesion site ( white circle ) 1 3 832 radiol med ( 2017 ) 122 : 829836 fig . 
3 during 125i brachytherapy , the implantation needle was inserted accurately into the tumor to implant 125i seeds under fluoroscopy ( c ) and confirmed by cact cross section ( a , b ) table 2 scoring scheme for evaluation of cact - guided puncture performance deviation . 
the follow - up period was prolonged by 36months if there was no evidence of disease progression in the first 6months after the procedure . statistical analyses data analyses were undertaken using excel 2010 ( microsoft , redmond , wa , usa ) and spss v13.0 ( ibm , armonk , ny , usa )  . 
four patients ( three cases with lung adenocarcinoma and one subject with metastasis from a rectal carcinoma ) died of multiple hematogenous metastases , leading to multiple - organ failure . 
two patients with hepatocellular carcinoma died of massive hemorrhage in 1 3 radiol med ( 2017 ) 122 : 829836 table 3 procedure records of cact - guided implantation of radioactive seeds in 30 patients because they were asymptomatic and clinically stable . 
two patients with pneumothorax volume < 20% did not receive specific treatment discussion interstitial 125i brachytherapy has showed promising results for local control of lung malignant solid tumors , prostatic cancer and bone metastases [ 810 ]  . 
we believe that this high prevalence of success of puncture was possible because the cact system enabled selection of a safe and accurate targeting route for navigation of the needle to the target tumor during implantation of 125i seeds . 
first , this strategy can permit better access to tumors in obese patients , space for extension of needles outside the body and superior image support for complex , double - oblique needle trajectories [ 14 , 15 ]  . 
new cact systems can provide a virtual pathway for the needle reaching the target tumor on live monitor , which can decrease scan times compared with conventional ct resulting in a low radiation dose . 
second , 125i seeds were deposited during withdrawal of the needle from the distal to proximal parts of each tumor at intervals of 0.51.0 cm to achieve planned seeds distribution . 
the fluoroscopy function of the c - arm in real time can confirm the location of each seed , while this information was only confirmed 1 3 834 radiol med ( 2017 ) 122 : 829836 fig . 
four months after brachytherapy , the tumor had disappeared , with only well - distributed radioactive seeds remaining ( black arrow ) ( f ) 1 3 radiol med ( 2017 ) 122 : 829836 by another ct scan ( resulting in more radiation ) in cct guidance . 
certainly , precise localization and documentation of each needle and tumor allowed operators to undertake interstitial 125i brachytherapy with confidence , thereby helping to reduce procedure time and subsequent exposure to radiation [ 5 ]  . lcr in small , intermediate and large pulmonary tumors at the 4 - month follow - up was satisfactory . 
 [ 18 ] reported that lcr was 78.1% at the 2 - month follow - up , with 1 - year survival of 65.0% for ct - guided 125i brachytherapy for lung cancer , which was significantly higher compared with that of the control group treated by chemotherapy alone . 
the following may reduce the risk of hemorrhage and pneumothorax : ( 1 ) ensure operators avoid puncture of interlobar fissures , bullae or vessels ; ( 2 ) reduce pleural puncture times ; and ( 3 ) shorten the time required for the procedure without more scans . 
two radiologists reviewed the images in consensus , describing mr imaging features including size , location , growth pattern , signal intensity of tumor , and dynamic enhancement pattern . results nine women and three men were included . 
the average maximum tumor diameter was 7.1 cexophytic growth was present in 9 / 12 cases , mesophytic growth in 2 / 12 , and endophytic growth in 1 / 12 . 
on t1 - weighted images , 2 / 12 displayed homogeneous isointensity , 1 / 12 homogeneous hyperintensity , 5 / 12 heterogeneous hypointensity , and 4 / 12 heterogeneous hyperintensity . 
on dynamic contrast - enhanced mr images , 7 / 12 showed a slow washout enhancement pattern , 2 / 12 a rapid washout pattern , 2 / 12 progressive enhancement , and 1 / 12 persistent enhancement . 
imaging findings were suggestive of hemorrhage ( 50% ) , necrosis ( 25% ) , or cystic change ( 50% ) * huiyi ye 13701100368@163.com * haiyi wang wanghaiyi301@126.com 1 department of radiology , chinese pla general hospital , fuxing road 28 , box 100853 , beijing , china 2 department of pathology , chinese pla general hospital , fuxing road 28 , beijing , china within the tumors . 
no metastases were found on the preoperative mr imaging . conclusion although mri appearances of renal eaml were various , some mri characteristics may contribute to suggest the possibility of renal eaml . keywords angiomyolipoma renal epithelioid angiomyolipoma renal mass magnetic resonance imaging introduction renal angiomyolipoma ( aml ) is the most common benign solid renal tumor , accounting for 2.06.4% of all renal tumors [ 13 ]  . 
most cases of eaml follow a benign course , but about 1 / 3 of eaml cases display aggressive biological behavior or result in distant metastases to the lung , liver , and lymph nodes [ 4 ]  . 
in 2004 , the world health organization classification of renal neoplasms considered eaml as a potentially malignant mesenchymal neoplasm [ 4 ]  . renal eaml can demonstrate different morphological patterns with carcinoma - like growth on histology , and can , therefore , be erroneously diagnosed as sarcoma or renal cell carcinoma ( rcc ) [ 7 , 8 ]  . 
found that eaml is activated through the mtor pathway [ 9 ] , and mtor inhibitors such as sirolimus or temsirolimus have been considered as the best treatment option for patients 1 3 radiol med ( 2017 ) 122 : 814821 with eaml [ 10 , 11 ]  . 
to the best of our knowledge , only two studies have reported on the conventional mr imaging features of eaml , and these included the low sample size of only 6 patients [ 12 ]  . 
therefore , the objective of this study is to present the mr presentation of eaml to improve the understanding of this rare renal tumor . materials and methods patients our institutional review board approved this retrospective study and waived the requirement for informed consent . 
 one patient had another 3 conventional amls in the same kidney confirmed by surgery and pathology . mr imaging sequences mr imaging was performed on 1.5 - t ( n 10 , signa hdxt , ge healthcare , milwaukee , wi ) or 3.0 - t systems ( n 2 , signa excite , ge healthcare ) using a surface phased - array coil . 
the imaging sequence was : ( a ) axial t1 - weighted dual echo out - of - phase and in phase sequences ; ( b ) coronal and axial t2 - weighted fast recovery fast spin echo fat saturation sequences ; ( c ) a diffusion - weighted imaging ( dwi ) sequence using fat - suppressed single - shot echo - planar imaging with b values of 0 and 800 s / mm2 ; ( d ) a transverse three - dimensional fat - suppressed t1 - weighted gradient - echo sequence performed before and at three time points after contrast medium administration . 
gadopentetate dimeglumine ( magnevist ; bayer , leverkusen , germany ; 0.1 mmol / kg of body weight ) was injected intravenously at a rate of 2 ml / s using a power injector ( medrad , warrendale , pa , usa ) , and was followed by a 20 ml saline flush . 
 the acquisition of the cortico - medullary phase was obtained 2530 s after contrast material administration , the nephrographic phase at 60 s , and the excretory phase at 240 s . qualitative mr image analysis all mr images were independently analyzed by two radiologists ( with 5 and 10 years of experience in abdominal imaging ) , with the final decisions being reached by consensus . 
if the signal intensity of the tumor was heterogeneous , the predominant signal was used to represent the signal intensity of the tumor . the enhancement pattern of the tumor on dynamic contrast - enhanced mr images from the cortico - medullary through nephrographic to excretory phases was defined as : i slow washout ; ii rapid washout ; iii progressive enhancement ; iv persistent enhancement . the reviewers also recorded the patients age , sex , clinical symptoms , and nephrectomy method . 1 3 816 radiol med ( 2017 ) 122 : 814821 pathological examination imaging findings twelve surgical resection specimens were fixed in 10% formalin and stained with hematoxylineosin ( he )  . 
eight patients were lost on follow - up , with the follow - up of the other 4 cases lasting 110 months . the imaging characteristics are summarized in table 2 . 
nine out of twelve ( 75% ) lesions displayed exophytic growth , 2 / 12 ( 17% ) mesophytic growth , and 1 / 12 ( 8% ) endophytic growth . on t1 - weighted images , 2 / 12 cases ( 17% ) displayed homogeneous isointensity in comparison with the adjacent normal renal cortex , 5 / 12 ( 42% ) heterogeneous hypointensity , 1 / 12 ( 8% ) homogeneous hyperintensity , and 4 / 12 ( 33% ) heterogeneous hyperintensity . 
microscopic fat was recognized as signal loss on opposed - phase mr images in 6 / 12 ( 50% ) cases in comparison with the in phase t1 - weighted images , while 5 / 12 ( 42% ) cases contained macroscopic and microscopic fat . 
hemorrhage was identified in 6 / 12 ( 50% ) cases and constituted close to 50% of the tumor volume in 4 cases , but less than 25% of the tumor volume in the other 2 cases . 
a cystic change was identified in 6 / 12 ( 50% ) tumors , which constituted less than 20% of the tumor volume in 2 cases , about 50% of the tumor volume in 3 cases , and more than 75% of the tumor volume in 1 case with a fluidfluid level . 
the central part of 3 / 12 ( 25% ) cases presented necrosis . on dwi , 11 tumors demonstrated heterogeneous hyperintensity , while 1 predominantly fat tumor demonstrated hypointensity . images , on dynamic contrast - enhanced mr the enhancement degree varied from mild through moderate to obvious . 
one ( 8% ) tumor showed a mild homogeneous enhancement with persistent enhancement , 2 / 12 ( 17% ) an obvious homogenous pattern with rapid washout , 7 / 12 ( 58% ) a moderate heterogeneous enhancement with a slow washout pattern , and 2 / 12 ( 17% ) a moderate heterogeneous enhancement with progressive enhancement . 
exophytic growth is one of the characteristics of eaml ; the pathological basis for this may be that the infiltrating ability of the benign tumor is lower in the parenchyma , but that it can easily grow in the relatively low resistance of the renal interlobular tissue . 
 e on the fat - suppressed t1 - weighted image the hyperintense area of the lesion on the in phase image shows as a hypointensity , indicating macroscopic fat ( arrow )  . 
patients with a small eaml tumor commonly have no specific clinical symptoms ; the tumors are incidentally detected by imaging examinations performed as a part of routine health checks or unrelated examinations . 
we , therefore , found that the presence of macroscopic fat was not specific to the diagnosis of classic aml , with the presence of macroscopic fat being similar in hepatic eaml [ 23 ]  . in previous studies , the signal intensity or density of the majority of eamls was described as heterogeneous on mr or ct imaging [ 12 , 13 , 16 , 22 ] , with the causes for this being given as hemorrhage , necrosis , or cystic change . 
in our study , hemorrhage was identified in 6 / 12 cases , necrosis in 3 cases , and cystic change in 6 cases , which are rates consistent with previous studies . 
e on the fat - suppressed t1 - weighted image the focal hyperintense area of the lesion on the in phase image shows as a hypointensity , indicating macroscopic fat ( short arrow )  . 
a previous study found that 3 / 4 cases displayed hypointensity on t2 - weighted mr images [ 22 ] , and in our study , 8 / 12 cases displayed hypointensity . 
our data showed that 3 / 12 cases had a mixed solid and cystic - type , 1 case had a multilocular cystic - type , and 8 cases a solid type . 
the degree of diffusivity is determined by the components of the tumor and is reflected by the apparent diffusion coefficient ( adc ) value . 1 3 820 radiol med ( 2017 ) 122 : 814821 fig . 
gh from the nephrographic phase to excretory phase the lesion shows a slow washout pattern on the dynamic contrast - enhanced images , the enhancement patterns were non - specific , with the degree of enhancement also varying [ 12 , 22 ]  . 
in the present study , 7 / 12 cases showed a slow washout and 2 / 12 a rapid washout pattern ; these enhancement patterns are similar to those of aml [ 27 ]  . 
however , not all imaging studies have reported this sign [ 14 , 16 , 22 ]  . approximately a third of eaml cases have been found to present with malignant biological behaviors [ 4 ]  . 
in one study , 2 tumors were locally invasive , and 1 patient had metastatic disease at presentation [ 12 ] , while in another study , 1 of the 10 tumors demonstrated retroperitoneal lymphadenopathy [ 16 ] , and in a third study a thrombus was present in the right renal vein , but none of the cases displayed metastases [ 22 ]  . 
in our study , although 1 case showed renal sinus invasion on mr imaging ; 1 case an invaded renal capsule , and 1 case perirenal fat on pathology , other aggressive signs , such as metastases , enlarged lymph nodes , or thrombus , were not found on the preoperative mr imaging . 
the follow - up on 4 patients also showed no recurrences or metastases . on histology , eaml consists of predominantly epithelioid cells and abundant multi - nucleated giant cells , with minimal or no adipose tissue , while the diagnosis of eaml depends on the detection of epithelioid cells . 
on immunohistochemical analysis , eaml shows similarities with classic aml ; the melanocytic markers ( e.g. , hmb - 45 , melan - a ) and smooth muscle markers ( e.g. , smooth - muscle actin ) are positive , while the epithelial markers are negative [ 6 ]  . 
in our study , 4 out of 12 cases of emal showed more than 10% positivity for ki - 67 index , with 2 cases showing local invasion on pathology . our study had some limitations ; first , the study is retrospective in nature . 
renal eamls demonstrate a range 1 3 radiol med ( 2017 ) 122 : 814821 of mr appearances , and sometimes , it is difficult to distinguish renal eaml from classic aml or renal cell tumor by mri features . 
however , according to the present study , these features include a large size , exophytic growth , minimal macroscopic fat , microscopic fat , massive hemorrhage , enlarged vessels , and hypointensity on t2 - weighted images , may help to identify renal eaml . 
the definitive diagnosis of renal eaml still currently depends on pathology . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants performed by any of the authors . 
this study aimed to assess the preoperative us detection of normal ptgs in patients who underwent hemithyroidectomy . methods between august and october 2016 , 44 patients underwent hemithyroidectomy using a low - collar incision , and 5 were excluded from the study . 
based on the surgical findings of ptgs , the preoperative us detection of ptgs was determined . results of the 39 patients , 3 had no surgical data for ptg ( n = 2 ) and the presence of parathyroid hyperplasia ( n = 1 )  . 
 in the 36 remaining patients , in 3 patients , us identification of a normal ptg was corroborated by surgical findings , whereas in 2 patients , us findings differed from surgical findings , and in 31 patients , us did not detect a normal * dong wook kim dwultra@nate.com tae kwun ha hasus@hanmail.net soo jin jung soojinmd@hanmail.net 1 department ofgeneral surgery , busan paik hospital , inje university college ofmedicine , busan47392 , southkorea 2 department ofradiology , busan paik hospital , inje university college ofmedicine , 75 , bokji - ro , busanjin - gu , busan47392 , southkorea 3 department ofpathology , busan paik hospital , inje university college ofmedicine , busan47392 , southkorea ptg . 
the successful us detection rate of normal ptg was only 8.3% ( 3 / 36 )  . conclusions us cannot be used for identification of normal ptgs . keywords parathyroid gland ultrasound hemithyroidectomy thyroid surgery introduction upon gross pathological examination , normal parathyroid glands ( ptgs ) have a mean size of 1mm3mm5mm and a mean weight of 3540mg [ 1 , 2 ]  . 
depending on the percentage of fat tissue , pro - oxidant cells , and vascularity , the color of ptgs may appear yellowish brown to reddish brown [ 1 , 2 ]  . 
 approximately 80% of superior ptgs are located posterior to the mid - portion of the thyroid lobe at the level of the cricothyroid junction and along the tracheoesophageal groove [ 4 ]  . 
there is greater variation in the location of the inferior ptgs , which can be found anywhere from the angle of the mandible to the pericardium [ 1 , 5 ]  . the imaging modalities that are commonly used for the evaluation of ptgs are high - resolution ultrasound ( us ) , nuclear scintigraphy , thin - section computed tomography , and magnetic resonance imaging ; combination modalities , such as fluorodeoxyglucose positron emission tomography computed ( fdg - pet ) single - photon emission and vol :  . ( 1234567890 ) 1 3 radiol med ( 2017 ) 122 : 866870 study patients underwent us examination without paying a fee . 
us examination for superior ptgs was performed because the location of superior ptgs varies less than that of inferior ptgs . the following features were investigated on real - time us examination : the presence or absence of superior ptgs , as well as the location , thickness , and length of the superior ptgs that were identified . 
the location of superior ptgs was classified as follows : ( 1 ) right and left ; ( 2 ) posterolateral surface , posteromedial surface , anterior surface , and border ; ( 3 ) intraglandular , subcapsular ( attached to the thyroid capsule ) , extracapsular ( attached to the thyroid capsule ) , and perithyroidal ( not attached to the thyroid capsule ) ; and ( 4 ) upper third , upper pole , and mid - third . 
furthermore , normal ptgs have similar us echogenicity with that of the thyroid gland , which limits the role of us in evaluation of ptgs [ 8 , 9 ]  . 
therefore , this study evaluated the preoperative us detection of normal ptgs and sought to identify the characteristics of normal ptgs in patients who were scheduled to undergo hemithyroidectomy , using the surgical findings of ptgs as a reference standard . patients andmethods study population this prospective study was approved by the institutional review board , and informed consent was obtained from all of the patients . 
of the 44 patients , 5 were excluded from the study because of the presence of a known ptg abnormality ( n = 2 ) or patient refusal ( n = 3 )  . 
1 a gross specimen ( a ) of a resected parathyroid gland in the operating roo in intraoperative transverse gray - scale sonogram ( b ) , a resected right superior parathyroid gland ( arrowheads ) and the right thyroid gland ( arrows ) show similar echogenicity . 
in histopathology , the parathyroid gland showed normal parenchyma without hyperplasia 1 3 868 thyroid surgery hemithyroidectomy with a low - collar incision was performed by a single surgeon with 8 years of experience in thyroid surgery . 
during the surgery , the presence or absence of superior ptgs and the location , thickness , and length of superior ptgs were examined as in the us examination : the location of ptgs was similarly classified as follows : ( 1 ) right and left ; ( 2 ) posterolateral surface , posteromedial surface , anterior surface , and border ; ( 3 ) intraglandular , subcapsular ( attached to the thyroid capsule ) , extracapsular ( attached to the thyroid capsule ) , and perithyroidal ( not attached to the thyroid capsule ) ; and ( 4 ) upper third , upper pole , and mid - third . 
histopathological analysis of the ptgs was conducted to assess normality or abnormality ( such as diffuse hyperplasia )  . serum concentrations of parathyroid hormone were also evaluated in all patients during the week preceding thyroid surgery . 
all serological parameters were evaluated using electrochemiluminescence immunoassay on the elecsys automatic system ( roche diagnostics deutschland gmbh , mannheim , germany )  . comparison ofultrasound andsurgical findings when there was complete correspondence between the location , thickness , and length of ptgs in us and surgical findings , the us detection of ptgs was determined to be a success ; however , when one or more parameters differed between both us and surgical findings , the us detection of ptgs was determined to be a failure . results among the 39 patients , there were no surgical data for ptg in 2 ( n = 2 ) patients and the data for 1 patient revealed the presence of parathyroid hyperplasia ( n = 1 )  . 
in these 3 cases with successful us detection , ptg location was extracapsular ( n = 2 ) and subcapsular ( n = 1 ) in both us and surgical findings . 
 in the 2 cases where us and surgical findings did not completely correspond , it is likely that perithyroidal fat , muscle , or nervous structure was considered as a normal ptg on us . 
this did not correspond to the surgical findings of the left superior parathyroid gland in terms of the size and location discussion we found that , in general , normal ptgs are not visible on us , although previous studies had suggested that ptgs appear relatively flat and hypoechoic , and are located along the dorsal aspect of the thyroid gland [ 1 , 9 ]  . 
as a person ages , normal ptgs tend to accumulate more fat cells and granules , which is likely to make them more echogenic and less conspicuous within the other echogenic adipose tissues of the neck on us [ 1 ]  . 
in our study , we attempted to assess the detection of normal ptgs by us in patients who underwent hemithyroidectomy . in the present study , we used high - resolution us , which enables detection of a tiny thyroid nodule with a greatest 1 3 870 radiol med ( 2017 ) 122 : 866870 diameter of only 1mm ; however , the successful us detection rate of normal ptgs was only 8.3% ( 3 / 36 )  . 
in surgical findings , the mean thickness and length of normal ptgs in the successful us detection group ( n = 3 ) were not greater than those in the unsuccessful us detection group ( n = 31 )  . 
 before the study , we presumed that successful us detection of normal ptgs would be possible , because of the high resolution of the us device , because normal ptgs are sufficiently large , and because radiologists have a good knowledge of the us - based anatomy and pathology of neck structures . 
however , the following factors may have affected the ability of us to detect normal ptgs : ( 1 ) factors related to a poor sonic window , such as thickened subcutaneous fat tissue , an enlarged thyroid gland , and underlying thyroid disease including a thyroid nodule or autoimmune thyroiditis ; ( 2 ) the similar echogenicity of ptgs to thyroid gland or perithyroidal fat tissue ; ( 3 ) thin or small ptgs ; and ( 4 ) the diverse location of the normal ptgs . 
this may need to be clarified in a further study . in the measurement of glandular size in those ptgs identified on us , only a small difference between us and surgical findings was found . 
this may be related to the following factors : first , there may be a measurement bias because of the use of different measurement devices : a ruler and caliber were used in the surgery and a specific measurement program was used in the us scan . 
finally , a single radiologist and a single surgeon performed us and assessed surgical findings , respectively ; therefore , this research may not be applicable to wider groups of radiologists and surgeons . in conclusion , us detection of normal ptgs is limited because of factors related to the sonographic window or the similar echogenicity of the ptg and the thyroid , for example ; however , as us devices continue to develop and interest in us detection of normal ptgs increases , it may become possible to visualize these glands on us . author contributions concept and design : dwk . 
 the correlations between the abnormal features detected on hepatic t2wi and dce imaging , and the levels of inflammatory activity and fibrosis were determined . results logistic regression analysis showed increased patchy hyperintensities ( b = 1.869 , p = 0.001 ) on t2wi and patchy enhancement ( b = 1.596 , p = 0.004 ) at the arterial phase along with increased inflammatory activity . 
 however , linear and reticular hyperintensities ( b = 2.356 , p = 0.000 ) on t2wi , and meshwork enhancement ( b = 2.191 , p = 0.000 ) at the equilibrium phase , all correlated with fibrosis . 
multiple effective medications are available to inhibit hbv replication with liver fibrosis regression by reducing liver inflammation and cellular damage in most patients with chronic hepatitis b [ 36 ]  . 
the progress of liver cirrhosis without active inflammation is often slow and asymptomatic even when the patient has reached the irreversible stage ; however , active cirrhosis can cause liver failure or even develop into liver cancer [ 7 , 8 ]  . 
therefore , the assessment of liver inflammatory activity and fibrosis for patients with chronic hepatitis b is helpful for determining prognosis and treatment strategy [ 3 , 9 ]  . in recent years , along with the development of hardware and software technology , magnetic resonance imaging ( mri ) has been widely used for the diagnosis of liver diseases . 
liver imaging ( t2wi ) and dynamic contrast - enhanced ( dce ) imaging fat - suppressed t2 - weighted vol . : ( 0123456789 ) 1 3 808 radiol med ( 2017 ) 122 : 807813 are commonly used sequences for assessing liver diseases [ 1013 ]  . hepatic pathological changes in the chronic hepatitis b are complicated because of chronic pathological processes . 
 in addition to the varying degrees of hepatocyte degeneration and necrosis in hepatic lobule , inflammation of and around the portal area is often obvious , accompanied by varying degrees of fibrosis . 
these lesions do not necessarily lead to general morphological changes in liver , but may cause abnormal water content and distribution in liver , or changes in hepatic microcirculation , all of which may lead to abnormal image features on t2wi and dce imaging of liver [ 1417 ]  . this study explored the correlations between abnormal features seen on fat - suppressed t2wi and dce imaging and the inflammatory activity and fibrosis in chronic hepatitis b . materials andmethods subjects this study was conducted in accordance with the guidelines of the institutional review board of our institution . 
inclusion criteria were : ( 1 ) hospitalized patients with complete clinical data and serological diagnosis of hepatitis b ; ( 2 ) diagnosis of chronic hepatitis through percutaneous liver biopsy ; and ( 3 ) clear images without interference from artifacts . 
exclusion criteria were : ( 1 ) cirrhosis detected by pathology or imaging ; ( 2 ) liver focal lesions > 3cm in diameter , such as liver cancer , hemangioma , etc . 
in the 67 patients , there were 51 patients that undergone the abdominal non - enhanced and triple phase dce - mri and 16 patients only with the abdominal non - enhanced mri . 
eighteen patients were randomly selected ( random number table ) as the control group from 45 patients with splenic or pancreatic focal lesions , such as small cysts , hemangioma , etc . , who underwent abdominal magnetic resonance ( mr ) scanning and were ruled out of any hepatic disease by appropriate clinical , laboratory , and radiologic investigations . 
among the 85 patients , 65 were males and 20 were females , aged 1863years , with a mean age of 41.148.98years. histopathology all 67 patients underwent ultrasound - guided percutaneous liver biopsy using an 18 - gauge spring - loaded biopsy device . 
histological diagnosis , hepatic inflammation ( grades 04 ) , and fibrosis ( stages 04 ) were assessed by a simplified system for scoring in chronic viral hepatitis according to scheuer [ 8 , 18 ]  . 
scanning sequences for all 67 patients included cross - sectional fat - suppressed fast spoiled gradient echo ( fspgr ) t1 - weighted imaging ( t1wi ) , fat - saturated respiratory triggered fast recovery fast spin echo ( frfse ) t2wi , double echo chemical shift t1wi , and coronal and axial fast imaging employing steady - state acquisition ( fiesta ) sequence . 
 frfse fat suppression t2wi scan parameters were repetition time ( tr ) 6000ms , time echo ( te ) 89ms , echo train length 19 , bandwidth 62.5khz , matrix 320224 , number of excitation ( nex ) : 2 , slice thickness 8mm , and interval 1 m dce scanning used liver acquisition with volume acceleration ( lava ) sequence , tr 4.0 ms , te 2.0 ms , matrix 288160 , slice thickness 5.0mm , and overlapping 2.5mm. after precontrast images were obtained , arterial phase images were acquired at 1820 s after the start of 1 3 radiol med ( 2017 ) 122 : 807813 intravenous bolus administration . 
periportal edema is mainly defined as hyperintense tramlines or rings surrounding the portal veins on t2wi or low intensity tramlines or rings around the portal vein at portal phase on dce imaging [ 15 , 19 ]  . 
all review for images were accomplished on the workstation by two abdominal radiologists with 10 years of experience blinded to clinical and pathologic findings together , and the final decisions were reached by consensus . statistical analysis the abnormal images seen on t2wi and dce imaging may be affected by both inflammatory activity and fibrosis levels . 
all statistical analyses were performed using the spss13.0 software , and p0.05 was considered to be statistically significant . results pathological composition forthesample in the 67 patients with chronic hepatitis b retrospectively enrolled , hepatic pathological characteristics included minimal , occasional spotty necrosis ( g1 ) to severe , prominent diffuse hepatocellular damage ( g4 ) , and no fibrosis ( s0 ) , portal fibrosis ( s1 ) , periportal fibrosis ( s2 ) , septal fibrosis ( s3 ) , and early cirrhosis ( s4 )  . 
pathological composition of the control and patient groups is shown in table1 . table 1 distribution of imaging features in different pathological groups grading staging sample size ( n ) patch hyperintensities on t2wi reticular hyperintensities on t2wi periportal edema patchy enhancement at arterial phase on dce meshwork enhancement at equilibrium phase on dce 0 / 18 1 / 10 0 / 18 1 / 10 0 / 18 3 / 10 0 / 18 0 / 18 the number before the / sign denotes the number of patients with the abnormal image features , and the number after the / sign denotes the number of patients in each group 1 3 810 radiol med ( 2017 ) 122 : 807813 fig . 
2 meshwork hyperintense signals ( arrow ) in liver seen in patients with chronic hepatitis b on mr t2wi liver mri findings the liver mr findings in different groups of inflammatory activity and fibrosis are shown in table 1 . 
 the p values of t2wi reticular hyperintense shadow and meshwork enhancement at the equilibrium phase on dce imaging among the normal , mild , and moderate - to - severe groups were all equal to 0.000 ( chi - square test , exact probability calculation method )  . 
moreover , the presence of periportal edema correlated with both g and s ( p < 0.05 ) , and the partial regression coefficient b of g ( 2.635 ) was much larger than that of s ( 1.270 ) , indicating that periportal edema was mainly affected by g . g1 and g2 groups were combined into the mild inflammatory activity group and g3 and g4 into moderate - tosevere groups . 
moreover , the presence of periportal edema correlated with both g and s ( p < 0.05 ) , and was mainly affected by g . pathological changes in the liver are complicated because of different pathological processes caused by chronic hbv infection . 
due to hepatocyte necrotic debris , bridging and multi - lobular necrosis , and fibrous tissue deposition , necrosis and fibrous tissue bands may appear in the liver , accompanied by inflammatory cell infiltration or pseudobile duct formation in the fibrous tissue bands . 
intrahepatic inflammatory exudate , abnormal lymph formation , and reflux can cause edema around the branches of the intrahepatic portal veins , usually seen as high intensity tramlines or rings surrounding the intrahepatic portal veins on t2wi or low intensity tramline or rings at portal phase on dce , which is also known as periportal edema [ 15 , 19 ] , an image feature indicating the presence of active liver inflammation [ 15 , 19 ]  . this study showed that patchy hyperintensities and periportal edema on t2wi correlated with the inflammatory activity . 
these imaging features may be caused by liver tissue necrosis , inflammatory activity , and abnormal lymph formation and reflux , which are all known to result in abnormal water content and distribution in the liver . 
periportal edema is also relevant to liver fibrosis , but its relevance is much lower than that of the inflammatory activity , suggesting that the presence of periportal edema is mainly affected by the inflammatory activity . 
linear and reticular hyperintense signals on t2wi correlated with the degree of liver fibrosis , but were irrelevant to liver inflammatory activity , indicating that linear and reticular hyperintense signals on t2wi are related to fibrous tissue band formation in the liver [ 21 ]  . dce - mri can provide information on liver blood supply and extracellular space . 
in chronic hepatitis , perisinusoidal fibrosis and sinusoidal capillarization caused by collagen deposition , mechanical pressure of fibrous septa , radiol med ( 2017 ) 122 : 807813 and formation of vascular traffic branches , all lead to liver microcirculation disorder . 
 in chronic hepatitis patients with patchy enhancement at the arterial phase on dce - mri , large amounts of macrophage infiltration , hepatocyte necrosis , fatty degeneration , and tissue collapse are found in the liver , indicating that patchy enhancement at the arterial phase might reflect the current or most recent liver cell damage [ 22 , 23 ]  . 
therefore , determining the presence of moderate - to - severe inflammation or moderate - to - severe fibrosis is important for chronic hepatitis prevention and treatment as well as prognosis assessment [ 9 ]  . 
this study found intrahepatic patchy hyperintense signals and periportal edema on t2wi , and patchy enhancement at dce arterial phase was significantly different in normal and mild inflammation groups compared to those in moderate - to - severe inflammation group . 
these features can be used as a standard to diagnose moderate - to - severe hepatitis ( g3 , g4 ) with a relatively high specificity and positive predictive value . 
linear and reticular hyperintense signals on t2wi , and meshwork enhancement at dce equilibrium phase were significantly different in normal and mild fibrosis group ( s1 , s2 ) compared to those in moderate - to - severe fibrosis group ( s3 , s4 )  . 
first , we used liver biopsy results as the gold standard , and sampling error due to heterogeneity in the intrahepatic lesions may affect the results in a single individual . 
in young patients , between 60 and 80% of chest injuries result from blunt trauma , with over half as a consequence of impact with motor vehicles , whereas in adolescents and adults , penetrating trauma has a statistically more prominent role . 
chest x - ray is the first imaging modality of choice to identify patients presenting with life - threatening conditions ( i.e. , tension pneumothorax , huge hemothorax , and mediastinal hematoma ) and those who require a ct examination . 
in fact , the high spatial resolution , along with multiplanar reformation and three - dimensional ( 3d ) reconstructions , makes mdct the ideal imaging method to recognize several chest injuries such as rib fractures , pneumothorax , hemothorax , lung contusions and lacerations , diaphragmatic rupture , and aortic injuries . 
camillo hospital , 3 department of emergency radiology , cisanello hospital , 4 department of radiology , santobono pediatric hospital , rome , italy pisa , italy naples , italy 5 department of radiology , university of foggia , foggia , italy 6 department of radiology , university hospital careggi , l.go giovanni alessandro brambilla , 3 , 50134 florence , italy nevertheless , when imaging a young patient , one should always keep into account the alara concept , to balance an appropriate and low - dose technique with imaging quality and to reduce the amount of ionizing radiation exposure . 
according to this concept , in the recent years , the current trends in pediatric imaging support the rising use of alternative imaging modalities , such as us and mri , to decrease radiation exposure and to answer specific clini cal questions and during the observation period also . 
as an example , ultrasound is the first technique of choice for the diagnosis and treatment of pleural and pericardial effusion ; its emerging indications include the evaluation of pneumothoraces , costocondral and rib fractures , and even pulmonary contusions . keywords emergency radiology trauma imaging major trauma thoracic trauma pediatric trauma introduction chest trauma in pediatric patients can occur from either blunt or penetrating trauma , being the most common source of morbidity and mortality in children and adolescents [ 1 ]  . the most common mechanism involves blunt forces , accounting for 8085% of pediatric thoracic injuries , with motor - vehicle crashes , pedestrian accidents , and falls as the most frequent causes [ 2 ]  . trauma pediatric chest injuries differ from those observed in adults because of the higher compliance of thoracic cage due to a greater cartilage content and ribs incomplete ossification . 
these factors are responsible for a higher involvement of lung parenchyma than of bone structures , resulting thus in fewer rib fractures and prevalence of pulmonary contusions . 1 3 radiol med ( 2017 ) 122 : 850865 in children , the mediastinum is mobile , so that aortic tears and diaphragmatic lesions are very uncommon ; on the other hand , this mobility is a possible cause of respiratory compromise because of angulation and displacement of the trachea and compression of lung by mediastinum [ 2 , 3 ]  . the clinical evaluation and the triage of an injured child may appear very difficult , in relation to the patients age , or in case of unconsciousness . 
on one hand , we have the low - energy and isolated trauma , in which the first diagnostic approach in a child can be performed by chest x - rays . 
when positive , a multidetector computed tomography ( mdct ) is performed ; according to it , if positive findings are highlighted , the young patient is brought to the operating room , while , when negative , a conservative management can be performed . 
compared with adults , children are at least four times more sensitive to ionizing radiations because of a longer life expectancy and a faster cell rate division , thus increasing the risk of developing radiation - induced cancer . when imaging is the only way to achieve the diagnosis , it must always be followed as low as reasonably achievable ( alara ) principle , which aims to reduce the exposure to ionizing radiation using the imaging technique with no or the lowest radiation dose , when possible . 
in fact , it must be kept in mind that a single chest radiograph exposes a patient to a dose of 0.02 millisievert ( msv ) while a chest ct to 5.4 msv of ionizing radiations [ 913 ]  . conservative management high energy trauma low energy trauma unstable patient stable patient chest - x - rays chest - x - rays surgery ct / medical evaluation after surgery fig . 
1 flow chart of diagnostic imaging in high - energy and lowenergy thoracic trauma although the great concerns about this topic , not only in the medical field , but also among parents and media , it must be noticed that there is still a debate about the presence or absence of a threshold and the effects of low - dose radiation causing cancer , as cohen has described [ 14 ]  . 
as the author stresses , there is not a real proof that ct scan causes cancer , since the evidence cited until now are based on regression models derived from exposure to the highest radiation dose from the hiroshima atomic bomb . 
on the other hand , the author mentions the american association of physicists in medicine , which assessed that the risks of medical imaging at effective doses below 50 msv for single procedures or 100 msv for multiple procedures over short time periods are too low to be detectable and may be nonexistent [ 15 ] , concluding that predictions of cancer incidence and deaths in patient populations exposed to low doses are highly speculative and should be discouraged . to help in the optimization process of medical exposure to patients , the concept of diagnostic reference levels ( drls ) has been introduced by the international commission on radiological protection ( icrp ) [ 16 ]  . 
drls do not deal with a dose limit or a dose constrain but with advisory values , taken as the third quartile value of national drl , to establish whether practice is reasonable or not . 
in the absence of dose limits , radiologists have to evaluate drls viability to pediatric patients : thus , they tend to be set , so that if the local drl values involved are exceeded , the radiological procedure needs to be investigated . until now , many european countries still do not have national pediatric drls for many examinations and particularly for pediatric interventional procedures . the european diagnostic reference levels for pediatric imaging pidrl , sponsored by the european community , listed some practical methods to establish pediatric drls ( table 1 )  . 
some of them are : 1 3 852 radiol med ( 2017 ) 122 : 850865 table 1 recommended european drls for computed tomography according to weight and age that have not to be exceeded computed tomography exam weight group ( kg ) age group ( years ) thorax 10 < 15 15 < 30 30 < 60 edrl ctdivol ( mgy ) dlp ( mgy cm ) the european drl ( edrl ) is based on the median ( the 50th percentile ) value of the distribution of the ndrls for a defined clinical imaging task surveyed for standardized patient groupings . 
as many authors experienced on adults populations , us can identify the presence of pneumothorax by observing the absence of two indirect signs , the comet tail artifact , and the lung sliding sign , which are identifiable in the normally aer ated lung . 
authors experience about the feasibility of e - fast on adults is remarkable [ 23 ] ; in this study , ultrasound sensitivity was 77% , specificity 99.8% , positive predictive value 98.5% , negative predictive value 97% , and accuracy 97.2%. 
reported a sensitivity of 1.00 for the us detection of esophageal intubation [ 25 ]  . imaging techniques screening chest radiograph still remains a cost - effective first - line tool in the imaging work - up of pediatric thoracic trauma also because of its indisputable advantages such as widespread availability , relatively low cost , and easy acquisition [ 6 ]  . 
antero - posterior ( ap ) chest radiograph on supine position is usually the most feasible technique owing to the immobilization of the cervical spine in trauma patients ; nevertheless , this is not as sensitive as the erect chest x - ray or computed tomography ( ct ) for detection of thoracic pathology , which could be missed by plain - film x - rays . nowadays , ct plays a key role in the non - invasive evaluation of chest trauma in children when plain radiographs and ultrasound cannot help to get the correct diagnosis . 
in fact , it is more sensitive than plain - film x - rays to detect cage fractures , pleural and lung anomalies , diaphragmatic rupture , and aortic injuries because of its several advantages such as high spatial resolution , multiplanar reformation , three - dimensional ( 3d ) reconstructions , and fast acquisition times [ 7 , 8 ]  . 
the authors advocate the use of ct for patients in whom the mechanism of injury or cardiovascular status is indicative of spinal or vascular injury ; they stated that , if an intrathoracic injury is far to be suspected , an abdomino - pelvic ct scan , including the lower chest , may obviate the need for a dedicated chest ct . different protocols have been prepared to reduce children radiation exposure : they include tube current modulation , a child - size bowtie filter and scanning field of view ( fov ) , or a weight or size - based technique chart able to determine the appropriate kv or mas for each patient . 
some studies demonstrated that this technique , in addition to already low mas , resulted in 1 3 radiol med ( 2017 ) 122 : 850865 significant dose reduction , while image quality remained acceptable , as kim et al . 
routine pediatric thoracic ct should always be performed with adjusted imaging parameters for children : the tube voltage should be reduced to 80100 kvp rather than 120 kvp , protocols and automatic dose modulation software should be applied [ 7 , 25 ]  . 
for ct imaging of the body , typically , a reduction in mas of a factor of 45 from adult techniques is acceptable in infants , whereas for obese patients , an increase of a factor of 2 is appropriate [ 2729 ]  . ultrasound is the first technique of choice for the diagnosis and treatment of pleural and pericardial effusion ; its emerging indications include the evaluation of pneumothoraces , rib fractures , and pulmonary contusions [ 3032 ]  . magnetic resonance imaging ( mri ) is a powerful technique with the capability to answer several questions in dedicated settings although characterized by some drawbacks in the acute emergency field . 
its typical indications include the evaluation of spinal cord lesions when suggested by the neurologic examination and severe spinal pain after thoracic trauma [ 2 ]  . an other potential role of mri is the evaluation of doubtful cases of diaphragmatic hernia in hemodynamically stable patients , as barbiera et al . 
they can be visible on chest radiographs with some delay of up to 6 h [ 3 , 34 , 35 ]  . ct scan is by far more sensitive than plain - film x - rays to depict lung contusions as ground - glass areas located in the periphery or consolidative airspace opacities , associated with a thin zone of surrounding subpleural lucency . 
b ct scan well depicts two peripherally located areas of parenchymal attenuation ( arrows ) in the upper and lower lobes of the left lung as groundglass opacities , as for parenchymal contusions 1 3 854 radiol med ( 2017 ) 122 : 850865 fig . 
3 ad a 5 - year - old boy presenting with blunt chest trauma : ct scans in coronal and axial planes can easily recognize right - sided lung contusion ( arrows ) appearing as ground - glass opacities , associated with lower lobe atelectasis . 
they result from the rupture of the most distal airways after a blunt trauma of the chest wall . laceration radio - lucency , more easily detectable on reformatted images . lacerations become more visible days after the trauma , with the shrinking of the edema and the hemorrhage , both associated with contusion . 
they can be peripherally located or deep within the lung . large lacerations involving the pleural surface may cause the development of a bronchopleural fistula . they heal more slowly than contusions and , sometimes , can leave a persistent cavity called post - traumatic pseudocyst [ 13 , 36 ]  . pulmonary lacerations derive from destruction of lung parenchyma due to penetrating injuries , rib fractures , or compressive shear . 
5 ac a 10 - year - old boy sustaining a blunt thoracic trauma in which chest ct scan well depicts a right - sided peripherally located consolidation , suggestive of lung contusion ( arrows in a , b ) associated with a small amount of apical omolateral pneumothorax ( white arrow in c ) trauma , it occurs because of the increase of intrathoracic pressure and alveolar rupture , tracheobronchial tree injuries , or pleural laceration after a rib fracture . tension pneumothorax is the most severe adverse outcome . 
it requires immediate decompression to avoid cardiovascular collapse . the pathophysiology is characterized by the air flow into the pleural cavity without a means of escape , leading to mediastinal shift , reduced venous blood return to the heart 1 3 856 radiol med ( 2017 ) 122 : 850865 fig . 
6 ac a 5 - year - old girl sustaining a thoraco - abdominal blunt trauma : chest ct on axial plane demonstrates a right lower lobe atelectasis ( arrows in a , b ) , which appears slightly hyperdense after contrast media because of crowding of pulmonary vessels ( arrow in b ) , associated with two hypodense and irregularly shaped hepatic lesions in the right lobe , one of which reaching the capsular surface ( arrowheads in c ) fig . 
7 ae a 6 - year - old boy who sustained a blunt chest trauma : axial ct scans ( ac ) and coronal ( d ) and sagittal ( e ) reformatted multidetector - row ct images demonstrate round and oval collections of air in the right lung parenchyma , suggestive of pneumatoceles ( arrows ) , which are central and surrounded by lung contusions . 
the presence of a tension pneumothorax is suggested by the mediastinal shift to the contralateral side , depression of the ipsilateral diaphragm , and rapid expansion in follow - up x - rays [ 37 ]  . the supine antero - posterior chest radiograph not reliable at detecting pneumothorax , since the radiographic signs are very subtle , with a sensitivity of 3648% in some studies . 
indirect findings are an inferior lung border or cardiac border and a sharply defined diaphrag the deep sulcus sign is a very strong indicator of the presence of pneumothorax , representing lucency of the lateral costophrenic angle extending toward the 1 3 radiol med ( 2017 ) 122 : 850865 fig . 
8 a , b axial ct scan of a 9 - year - old boy sustaining a blunt thoracic trauma shows a right - sided lung contusion ( black arrow ) , appearing as an airspace consolidation with a round collections of the air , suggestive of pneumatocele ( arrowhead in a ) , associated with lung atelectasis ( white arrow in b ) fig . 
9 ac ct scanogram of a 9 - year - old boy who sustained a blunt thoracic trauma demonstrates multiple right - sided round or oval collections of air suggestive of pneumatoceles ( arrowheads in b , arrows in c ) and pleural effusion ( asterisk )  . 
ct is more sensitive for small pneumothoraces than chest radiography [ 42 , 43 ] , which remain clinically silent , and are not detected on plain - film x - rays ( occult pneumothoraces )  . recent surveys highlighted the role of chest us in diagnosing the presence of pneumothorax in adults , as ianniello et al . 
11 a , b axial ct scan of a 15 - year - old boy shows a high - attenuation pleural fluid over the involved hemithorax in the arterial phase ( white arrow in a ) ; active contrast extravasation into the pleural space is revealed in the late phase ( arrow in b )  . 
the high - attenuated pleural effusion was a strong indicator to perform the late phase since active bleeding was suspected collections are rarely seen after a chylothorax ; it requires fluid sampling to confirm the diagnosis [ 1 , 2 , 6 , 7 ]  . penetrating injury , and enter the mediastinum at the ilus and it can follow the path of least resistance . mediastinal abnormalities pneumomediastinum in the absence of demonstrable visceral injury , it has been attributed to the so - called macklin effect . 
this phenomenon consists of a tear in the alveolar sacs near the pulmonary ligament ; the air then dissects along the bronchovascular sheats and gets into the mediastinum [ 4446 ]  . pneumomediastinum indicates the presence of free air within the mediastinum , developing because air dissects along the bronco - vascular sheets , after a blunt or in children , the air frequently collects around the thymus . 
in plain - film x - rays , pneumomediastinum can manifest as mediastinal linear lucencies , as the continuous 1 3 radiol med ( 2017 ) 122 : 850865 this case , the fallen lung sign may be visible on chest radiographs , representing the collapsed lung located away from the mediastinum , in a dependent position , or located inferiorly with respect to the level of the diaphragm . these patients exhibit persistent pneumothorax and / or pneumomediastinum , and subcutaneous emphysema . mdct with thin - section axial and 2d / 3d reconstructions can help in the correct diagnosis of tracheobronchial injuries in children [ 4749 ]  . these injuries require a prompt diagnosis and surgical treatment due to their high rate of mortality ; distal bronchial injuries are managed by anatomic pulmonary resection , while the proximal ones are repaired surgically . 
airway stenosis , atelectasis , and pneumonia can occur as late sequelae [ 2 ]  . aortic injury although very rare in children ( < 0.1% of cases ) , aortic injuries are characterized by a high mortality rate , about 40% , and associated with a high injury severity score and degree of aortic wall disruption . 
 while the most of deaths occur at the time of injury , those patients with who survive hospitalization have a lower injury severity score and are often discharged home rather than to a rehabilitation facility , as malgor et al . 
as a consequence of the tear of the intima and media a pseudoaneurysm may manifest , characterized by a high instability with a high mortality rate ( 8085% )  . 
another sign of traumatic aortic injury is the presence of a periaortic hematoma . plain film performed in the trauma room is the first technique of choice to detect a traumatic aortic injury , although it is not specific enough , with a positive predictive value very low ( 520% )  . 
the signs detected on plain film are an obliterated contour of aortic arch , blurring of the aortopulmonary window , deviation of trachea and nasogastric tube to the right , downward depression of the left main - stem bronchus , widening of the paravertebral and paratracheal stripes , and a left apical pleural cap . mdct is the gold standard for the diagnosis of aortic injury ; in a study by dyer et al . , ct showed a 100% sensitivity and a 100% negative predictive value for the detection of traumatic aortic injury [ 53 ]  . 
 esophageal injuries typically require a surgical treatment [ 46 ]  . tracheobronchial injuries tracheobronchial injuries are very rare in children ( < 1% of pediatric patients with thoracic trauma ) and they usually result from shearing forces after a blunt trauma . the most common locations occur in the distal trachea , just above the carina , and in the main - stem bronchi , especially the right main bronchus . 
in 1 3 860 radiol med ( 2017 ) 122 : 850865 ct was performed more frequently than thoracic aortography because of its non - invasivity , less - expansivity and characterized by short time acquisition . 
both of them can result in cardiac tamponade and require a quick surgical decompression . most children affected by cardiac injuries heal without sequelae ; less than 5% of patients develop long - term complications , such as valvular dysfunction [ 1 , 38 , 39 ]  . commotio cordis is a rare condition in pediatric thoracic trauma , causing sudden death after a blunt impact . 
it is characterized by the absence of cardiac contusion , coronary arterial abnormalities , structural anomalies , or conduction system pathology [ 2 ]  . cardiac and pericardial injury diaphragmatic injury cardiac injury is a very rare event in the setting of pediatric thoracic trauma , with an incidence of 0.34.6%. 
myocardial contusions represent more than 95% of cardiac injuries due to blunt trauma and they are typically occult or cause death quickly after trauma ; they can be suspected on the diaphragmatic injuries usually occur after a motor - vehicle accident , with a incense rate quite low , approximately 12% . 
left - sided injuries are more common than the right ( reported rates of 7080% on the left side , 1524% on the right side , and 5% bilaterally ) , although some authors fig . 
13 a , b 14 - year - old boy sustaining a blunt thoracic trauma : axial ( a ) and sagittal ( b ) ct scans at the level of the aortic isthmus ( a ) show a small amount of periaortic hematoma ( arrowhead ) and an intimal flap ( arrows in a , b ) suggesting an aortic isthmic tear 1 3 radiol med ( 2017 ) 122 : 850865 suggest that this discrepancy may be explained by the fact that the right side sustain more overlooked injuries . normally , the larger the tear the earlier the presentation , although some diaphragmatic ruptures may be diagnosed at a later stage when the patient re - presents with complications such as visceral herniation and / or strangulation [ 38 , 39 ]  . on the left side , the most commonly involved organs are bowel ( stomach , small bowel , and colon ) and spleen while on the right side the liver . the ap chest radiograph can show diaphragmatic tears in 2530% of cases only because of associated injuries ( atelectasis , pulmonary contusions , and pleural effusions ) ; nevertheless , a negative examination does not rule - out a possible injury . 
other criteria include the curled diaphragm sign , a focal thickening of the diaphragm , and the dependent viscera sign referring to herniated viscera apposing the posterior chest wall without interposition of lung parenchyma or diaphragm [ 42 , 43 ]  . chest wall injuries rib fractures in children , rib fractures occur less frequently than in adults owing to their chest wall higher flexibility ; in fact , ribs typically bend instead of breaking when compressed , so that more of the trauma energy is transferred to the intrathoracic organs . 
consequently , significant intrathoracic injuries may occur even in the absence of rib fractures [ 3 ]  . multiple rib fractures are associated with a greater incidence of multi - organ trauma , 70 versus 12% of children with one rib fractures . first rib fractures , usually caused by high - energy trauma , are often associated with severe vascular and intrathoracic injuries ; lower rib fractures are often combined with upper abdominal organs injuries . acute non - displaced rib fractures are very difficult to diagnose on an ap chest radiograph and are missed more fig . 
a severe splenic trauma is also present 1 3 862 radiol med ( 2017 ) 122 : 850865 than 50% of the time ; on the contrary , ct is by far more sensitive , although these lesions do not significantly impact on patient management . they are frequently associated with motor - vehicle accidents ( 50% ) , but also fall from height account for a high percentage ( 24% )  . a flail chest occurs in the presence of parallel double fractures of four or more contiguous ribs with loss of the bony continuity of the thoracic cavity . 
this results in a paradoxical chest wall movement inwards with inspiration , leading to respiratory distress [ 46 ]  . sternal fractures sternal fractures are poorly described in children likely because of the relative plasticity of the pediatric thorax and the difficulty in establishing a correct radiographic diagnosis without dedicated views . 
in the majority of cases , they are the result of severe blunt trauma , such as motor - vehicle crash ; in these cases , the likelihood of intrathoracic injury is very high . its diagnosis is difficult when only minimal displacement of the fracture site is disclosed on plain fil in the recent years , different studies highlighted the role of us to diagnose sternal fractures , compared to the conventional radiograms ; you et al . 
 [ 57 ] demonstrated that simple and unstable compression fractures were more common in the non - junctional spine and that distraction fractures occurred more frequently in the non - junctional tract also , emphasizing the importance of carefully analyzing young patients for this type of injury . all these kinds of fractures are best visualized on lateral radiographs or sagittal reformatted ct images . finally , especially in younger children , spinal cord injury ( hemorrhage , transection , or central cord syndrome ) may occur without disruption of the bony anatomy due to the excessive mobility of the pediatric spine [ 1 , 35 ]  . 
15 a , b axial ct scan of a 13 - year - old boy shows a wide sterno - clavicular disarticulation with anterior lung herniation ( arrows in a , b ) 1 3 radiol med ( 2017 ) 122 : 850865 fig . 
axial ( b ) and sagittal ( b ) images of multidetector - row ct images show unstable fracture ( arrows in b , c ) with rupture of the body of t8 and of the posterior wall of t7 with involvement of the spinal cord by bone fragments . 
axial gre t2 - weighted image ( d ) shows a hypointense area within the medulla ( arrow ) suspect for intra - medullar bleeding conclusions chest x - rays is the most common first imaging technique performed to evaluate pediatric patients undergoing blunt thoracic trauma . md - ct is performed in all stable patients sustaining a high - energy trauma and in those undergoing a lowenergy trauma in which chest x - rays demonstrate positive findings . as mentioned above , when dealing with imaging in children , the alara principle must be taken into consideration to reduce as more as possible childrens exposure to ionizing radiations [ 911 ]  . 
tumor staging of iii ( p = 0.011 ) and iv ( p < 0.001 ) , the nodules number of 24 ( p = 0.016 ) , 59 ( p < 0.001 ) and 1020 ( p < 0.001 ) , the nodules margin of being smooth ( p = 0.001 ) and slight lobulated ( p < 0.001 ) , and nodules with no near short strips ( p = 0.001 ) were significant predictors of changed pns . 
guidelines for following incidental nodules in patients without known malignancy may be not applicable in such settings [ 6 ] , and there exist no universally accepted guidelines regarding their workup . several studies have evaluated the frequency of malignancy in pns in oncology patients . 
these studies were performed with conventional or helical ct using a section thickness of 510mm [ 3 , 7 ] , or included patients with pepm [ 13 ] or varied cancers [ 8 , 9 ] , or included prevalent pns [ 1 , 8 ] or incidental pns [ 2 , 3 , 9 ] , or included lesions with varied sizes [ 13 , 8 , 9 ] or only the largest nodule was analyzed [ 1 , 2 , 8 ]  . 
while , studies predicting metastatic nodules concentrated on imaging features of pns 10mm on thin - section baseline ct in patients with pepm are limited . the purpose of this study was to identify the predictive clinical and imaging factors associated with pulmonary materials andmethods patients the institutional ethics review board approved this retrospective study and waived the need for informed consent . 
 ct reports and clinical records of 1634 patients with histologically proven pepm in our institution between april 2013 and december 2013 were reviewed , a total of 477 patients ( 29.2% ) with pns 10 mm on initial ct were recorded . 
patients were included if the first follow - up interval3months , the number of follow - up 2 , followup duration 6 months , and the treatment records were complete ; and none were excluded on the basis of their primary diagnosis . 
in general , follow - up ct were performed at 2months intervals at the stage of receiving chemotherapy for patients with solid tumors , and then 36 months intervals in 2 years when the tumors were cured or stable . 
for patients with interventional treatment , it started at 1month and continued at 2 or 3months , and then 3months intervals in the first year and 6months intervals thereafter . toshiba aquilion 64 - slice ct ( toshiba medical systems , japan ) and ge discovery ct750 64 - detector ct ( ge medical healthcare , milwaukee , wisconsin ) scanning system were used for follow - up examinations with enhanced chest ct . 
contrast enhanced images were obtained after a bolus intravenous injection of 1.5ml / kg of non - ionic contrast agent ( omnipaque 300 , ge healthcare , shanghai , china ) at a rate of 3ml / s . 
the axial and multiplanar reformation ( mpr ) images were routinely reconstructed at a slice thickness of 1mm and interval of 0.5mm. these images were reviewed by two experienced authors ( one with more than 20 years of experience with subspecialty training in thoracic radiology and one with 4 years of experience ) and decisions were reached by consensus ; when there was a major disagreement , another radiologist with over 20 years of experience was consulted . 
images 1 3 840 radiol med ( 2017 ) 122 : 837849 were reviewed using the institutional picture archiving and communication systems ( pacs ) workstation ( centricity radiology ra1000 , ge health - care )  . determination ofpulmonary metastasis the nature of pns were determined on the interval change in imaging features ( size , density ) on serial ct images between initial ct and the end of study or follow - up . 
serial imaging has become a commonly employed alternative technique to biopsy or radical resection in the evaluation of pns and has been used extensively in several recent studies [ 1 , 2 , 8 ]  . accordingly , pulmonary nodules were classified into two types , namely , stable pns and pns with interval change ( changed pns ) , depending on whether interval change happened on serial ct imaging over time or not . 
nodules were considered to be stable if they showed no interval change in size or a little change of 11.5mm or less ( including measurement error ) as well as no change in density at the end of study / follow - up . 
nodules that disappeared , or that showed persistent increase / shrink in size of 11.5mm or more , or that increaseddecreased or decreasedincreased with an interval change in size of 11.5mm or more at any time , or that ground - glass opacity ( ggo ) grew to mixed - solid / solid nodules or necrosis occurred until the end of study / followup , were defined as changed nodules . 
patients having both stable pns and changed pns were included in the group of patients with changed pns . in the clinical settings , small nodules stable in size and density on serial imaging were more likely to benign lesions [ 8 ]  . 
while , nodules demonstrating constant interval change in size and density after the initial ct and a history of malignancy helped to establish a metastatic diagnosis [ 1 , 1013 ]  . investigated variables the interval and frequency of follow - ups between initial ct and the time of the first change or disappearance of a nodule or newly detected nodules , and duration between initial ct and the last follow - up ct were recorded . to determine clinical records were reviewed the histologic characteristics of the pepm , tumor stage atthetimeofdischarge and smoking history . 
in detail , smooth margin were defined as those with sharply demarcated , round or oval - shaped smooth nodules ; those with distinct margins with some smooth , relatively small convexities were defined as slightly lobulated margin ; and those with well - demarcated polygonal or angular margin which were concave toward the central area of the nodule were defined as polygonal margin ; which were similar to the reported descriptions [ 14 ]  . nodules with regular shape ( round , oval ) and smooth margin were defined as simple pns , nodules with irregular or polygonal shape , or slight lobulated margin , or near short strips were defined as complex pns . 
for patients with non - solitary pns ( the number 2 ) , nodules with similar characteristics of morphology and opacity were defined as pns with identical features ; others were defined as pns with varied features . the incidence rate of change ( irc ) of nodules were separately calculated according to the above studying factors . for patients with non - solitary pns in changed pns group , nodules per patient with synchronous change of persistent enlargement / shrink , or disappear , or increaseddecreased or decreasedincreased , were defined as nodules changed synchronously ; others were defined as nodules changed asynchronously . 
all the pns per patients demonstrating similar prognosis was considered as nodules with consistent prognosis . statistical analysis the comparison of irc of nodules for the above variables were estimated by pearson chi - square test or by kruskalwallis rank sum test . 
the irc of nodules in patients with no histologically proven pns was 36.6%. for patients with stable pns , 42.3% of patients followed up for more than 730days and 76.9% of patients for more than 365days . 
all the nodules with the early interval change in size showed continuous change in subsequent follow - ups . smoking history patients with stable pns had a slightly higher frequency of high - risk smokers than that of patients with changed pns , 32.3 versus ( vs ) 25.4% , p = 0.281. 
tumor staging of iii ( p = 0.011 ) and iv ( p < 0.001 ) , the nodules number of 24 ( p = 0.016 ) , 59 ( p < 0.001 ) and 1020 ( p < 0.001 ) , the nodules margin of being smooth ( p = 0.001 ) and slight lobulated ( p < 0.001 ) , and nodules with no near short strips ( p = 0.001 ) were thus found to be statistically significant predictors of changed pns . tumor characteristics among patients with stage i , ii and iii malignancies , 88.6% of them had stable pns . 
patients with stage iv malignancies had the highest irc of nodules ( 70.0% ) ; the lower was the tumor stage , the smaller was the irc of nodules , in detail , 16.0% for stage iii patients , 8.3% for stage ii fig . 
for changed pns , complex pns were marked by slight lobulated margin ; and for stable pns , complex pns were characterized by polygonal shape or near short strips . results showed a certain correlation between nodules size and simple / complex pns , r = 0.359 ( 95% ci 0.2670.451 ) , p < 0.001. 
the prognosis of pns had a weak correlation with that of the primary malignancies , r = 0.236 ( 95% ci 0.0480.419 ) , p = 0.003. 1 3 radiol med ( 2017 ) 122 : 837849 fig . 
a a mixed - solid nodule in the left upper lobe ( white arrow ) , located peripherally ; b , c a solid nodule in the left lower lobe , with oval shape and near short strips ( white arrowhead ) , located peripherally ; d , e a solid nodule in the right lower lobe ( white arrow ) , with polygonal shape and near short strips , located peripherally ; following up by 887days , the nodules did not demonstrate interval change 1 3 radiol med ( 2017 ) 122 : 837849 846 fig . 
nodules in the left lower lobe , measured 3mm ( a ) and 3mm ( b ) ( white arrows ) , respectively , with round shape and smooth margin , located peripherally ; both nodules decreased after a follow - up interval of 69days by receiving preoperative sutent therapy ( c , d ) ; after right nephrectomy , both nodules disappeared ( e , f ) on 302days . 
several new pns were detected in the bilaterellung over the follow - up , while no recurrent lesions were found in the left renal region 1 3 radiol med ( 2017 ) 122 : 837849 discussion in the present study , we investigated the imaging characteristics of the pns 10mm on initial ct in patients with pepm of a large sample size , as well as the inter - nodular imaging features and prognosis in the non - solitary pns patients . 
we identified a set of primary malignancies - level and nodule - level factors that can predict likelihood of pulmonary metastasis , including tumor stage , the number of nodules , tumor margin , and absence of near short strips . as had been described before , stable pns were likely benign [ 8 ] and changed pns had a higher risk of being pulmonary metastasis [ 1 , 1013 ]  . 
it is undeniable that the interval changes may not only reflect the response to the treatments but also inflammatory process and that there might be certain overlaps between the possible malignant nodules ( changed pns ) and possible benign nodules ( stable pns ) ; although absence of pathologic confirmation , based on a combination of long enough follow - ups for stable pns , the interval change on serial imaging for changed pns , and highly coincident change of nodules in non - solitary pns patients in the present study , we believe that our criteria for deciding the nodule character should be considered reliable . 
 [ 8 ] , in which nodules on initial ct measuring 249 mm in pepm patients and measuring 4 mm in patients with a wide variety of cancers were investigated , respectively . 
the discrepancy was supposed to be mainly relatedto the diversity of study population and nodules size in these studies or the grounds on which pulmonary metastases were suspected and no final histological diagnosis was available . the change in nodules size tended to occur early . 
the interval of the first change varied greatly in this study that was likely because of the variability of the first follow - up interval , or that of the nature growth of the pulmonary metastasis . 
accordingly , the interval for further ct evaluation of uncertain nodules 10mm in a pepm patient that could potentially affect clinical management should be early at 1 , 2 , or 3months or so after detection . 
as for the follow - up interval of these nodules after detection , follow - ups for efficacy evaluation of the primary malignancies should also be considered . notably , the popularity of pulmonary metastasis in these major tumor types presented in this study agreed with that of the general population , though , which was inconsistent with that described in earlier literature [ 13 ] , no significant difference of the irc of nodules was found among the major cancer groups , the possibility was that the number of patients with some individual type of primary malignancy was relatively small . there were statistical differences as well as certain overlaps in terms of size , number , location and morphology between the changed pns and stable pns . 
the larger were the pns , particularly those 5mm , the higher likelihood of pulmonary metastasis was the nodules ; and that , larger nodules had more distinct morphological features . 
scrutinizing the morphological features could provide more information for the diagnosis of the etiology of pns . in some of the previous literature , only the largest nodules were studied in non - solitary pns patients [ 1 , 2 , 10 ]  . 
 accordingtoourexperience , we believed that the individual nodule had its own clinical significance , so we recorded and analyzed all the nodules per patient , and we found that the nature of pns were consistent in the vast majority of non - solitary pns patients and that a large proportion of patients had pns with varied features . 
in view of the fact that 32.7% patients with pns of varied features were identified as changed pns , in non - solitary pns patients with pns of varied features , scrutinizing the morphological features one by one and screening the pns full of diagnostic specificity in indicating high risk of interval change would be of great importance . the current study had several limitations , particularly that of being a retrospective study . 
although defining an inclusive criterion of the first follow - up interval 3months , the first follow - up or early stage follow - ups might be delayed as a result of poor compliance of some patients , so that making our data slightly later than the actual time of the first changes had happened . 
third , we did not analyze the ct value of nodules , because 77.4% of the nodules were less than 5mdensity analysis of such small pns was difficult and of much measurement error . 
 encouragingly , however , nodules morphology characteristics investigation in this study could have differentiated the majority of the pns detected on baseline ct . 1 3 radiol med ( 2017 ) 122 : 837849 848 fig . 
nodules in the right upper lobe ( a ) , right middle lobe ( b ) , right lower lobe ( c ) and left lower lobe ( d ) ( white arrows ) , with round shape and smooth margin ; after receiving a combination of tace and sorafenib , nodules in the right middle lobe and bilaterel lower lobes changed synchronously by an increase on 29days ( eg ) and a dramatic increase on 121days , meanwhile , many new nodules were detected in the bilaterellung ; whereas the nodule in the right upper lobe remained stable over the follow - up 1 3 radiol med ( 2017 ) 122 : 837849 table 5 the ct features , treatment and pathologic diagnosis of histologically proven pns primary malignancies treatment ct features diagnosis staging primary malignancies lobe size , mm margin case 1 esophageal carcinoma radical resection wedge resection of right upper lobe right upper lobe 6.5 with near short strips radical resection wedge resection left upper lobe slight lobulated case 2 esophageal carcinoma of left upper lobe case 3 esophageal carcinoma radical resection wedge resection of right upper lobe right upper lobe 7 smooth pathologic diagnosis chronic granulomatous inflammation hamartoma ( cartilage ) chronic granulomatous inflammation conclusion for pulmonary nodules 10mm in pepm patients on baseline ct , high tumor stage ( stage iii and iv ) , non - solitary nodules , the nodules margin being smooth and slight lobulated , and nodules with no near short strips were significant predictors of changed pns , suggesting more likely to be pulmonary metastasis . 
subjective image quality , depiction of contrast agent and image noise ( 5 - point likert scale ; 5 = excellent ) were assessed in 41 patients , who underwent contrast - enhanced fp with the aforementioned optimized protocol by two radiologists in consensus . 
a conventional digital radiograph ( dr ) acquisition protocol served as the reference standard for radiation dose and image quality analyses . results phantom measurements revealed a general dose reduction of approximately 96% per image for the fp protocol as compared to the dr standard . 
although endoscopy has become the diagnostic gold standard for ugi examinations , fluoroscopy is still frequently used in clinical routine , as it provides additional functional and dynamic information [ 26 ]  . 
this applies in particular to the evaluation of gastrointestinal passage disorders , dynamic evaluation of the swallowing process or leakage of oesophageal and gastric anastomoses , since fluoroscopy is more simple and cost - effective to perform than ct or mri [ 69 ]  . 
furthermore , in paediatric radiology , fluoroscopy , often combined with ultrasound , serves as an alternative to ct to reduce dose exposure in both gastrointestinal and urogenital tract examinations [ 1 , 1013 ]  . according to the alara principles , continuous optimization of examination protocols is demanded to reduce the cumulative dose exposure of the patient to minimize the risk vol :  . ( 1234567890 ) 1 3 radiol med ( 2017 ) 122 : 822828 acquisition pulse rate of 30 / s for high temporal resolution . 
the last image hold was used for table and collimator adjustments . phantom studies to systematically investigate the potential of our optimized fp protocol to reduced radiation burden and to objectify organ dose exposure , we conducted a phantom study using an anthropomorphic male alderson - rando phantom ( type rt200 , humanoid systems , ca , usa ) representing a male patient ( 175cm height and 73.5kg weight ) with similar of radiation effects [ 14 , 15 ]  . 
conventional dr acquisition was the examination of choice for the dynamic evaluation of ugi pathologies after changing from analogue to digital acquisition techniques , providing high - resolution images , however , at a considerable radiation dose [ 16 , 17 ]  . 
 to account for this , several improvements of fluoroscopic hardware and dedicated post - processing software have been developed in recent years allowing for a substantial dose reduction [ 1821 ]  . 
however , focused research evaluating the benefits of these technical advances for fluoroscopic examinations of the upper gastrointestinal tract in adults are outstanding so far [ 16 , 19 ]  . 
moreover , it is still difficult to estimate the actual organ dose applied during such examinations , since dose monitoring in fluoroscopy is commonly performed using the dosearea product ( dap ) [ 22 , 23 ]  . 
dedicated phantom studies investigating absorbed organ doses of radiosensitive organs are rare [ 1 , 11 , 24 ] although it is important to know in favour of patient safety [ 25 ]  . therefore , the aim of this study was to establish an optimized dynamic ultralow - dose digital pulsed fluoroscopy ( fp ) protocol for upper gastrointestinal tract examinations and to investigate the resulting organ doses and its clinical feasibility with conventional digital radiograph ( dr ) acquisitions as reference standard . 
we hypothesized that ultralow - dose digital pulsed fluoroscopy allows for sufficient diagnostic image quality to provide reliable diagnosis while significantly reducing direct and scattered dose exposure . materials andmethods the institutional review board approved this retrospective study and waived the requirement of written informed consent . detector system andprotocols a multifunctional fluoroscopy system ( artis zee mp , siemens healthcare , erlangen , germany ) with a flat - panel detector [ amorphous silicon ( a - si ) with caesium iodide ( csi ) scintillator ; size : 3040cm ; pixel size 154154m ; spatial resolution of 3.25lp / mm ; digitization depth 14 bit ] was used for all phantom and patient measurements . the acquisition parameters of our optimized ultralowdose digital pulsed protocol were as follows : 86.7 kv ; 77ma ; 3.2ms ; a copper filter of 0.9mm was applied for beam hardening ; to compensate for the resulting decrease in image contrast , an automatic post - processing algorithm was implemented to improve contrast ratios ; in addition , automatic noise reduction was used to balance the low mas product ; a resolution of 512 512 was chosen with an fig . 
1 field of view for low - dose fluoroscopy and digital radiograph image acquisition in the phantom study 1 3 824 radiol med ( 2017 ) 122 : 822828 x - ray absorption and scattering as human body tissue . 
for dose measurements , 60 thermoluminescent dosimeters ( tld , lif ( lithium fluoride ) , tld type - 100 ; harshaw , chemical company , ohio , usa ) were placed in radiosensitive organs in the direct ( bone marrow ; lungs ; oesophagus ; stomach ; thymus ) and scattered ( eyes ; liver ; gonads ; thyroid ) beato ensure reliable measures and taking into account the radiation absorption along the examined object in the p.a. 
to consider the extremely lowdose exposure of the fp protocol and to allow for reliable dose detection by the tld , images were acquired until the detector system indicated a cumulative dose of 500mgy . 
 the phantomtube distance was 36cm , while the distance between the phantom and the detector was 28.5cthe measured values for the dap and the organ doses were normalized to the mean examination time in the patient study ( see below ) to provide a useful measure for clinical routine . patient study to assess the image quality of the investigated fp protocol in clinical routine , we included 41 patients , who underwent clinically indicated contrast - enhanced ( imeron 400 , bracco , konstanz , germany ; peritrast 400 , franz khler chemie gmbh , bensheim , germany ) fluoroscopy with our optimized fp protocol and of whom a historical conventional dr acquisition was available in the pacs archive . 
a summary with detailed patient demographics is given in table1 . analysis ofimage quality image quality was subjectively evaluated on a dedicated workstation ( syngommwp ve26a ; siemens healthcare , erlangen , germany ) by two radiologists in consensus with 3 ( a.p. ) and 6years ( m.n. ) of experience in fluoroscopy . 
2 low - dose fluoroscopy ( a ) and digital radiograph ( b ) images of a 72 - year - old patient with zenkers diverticulum partially filled with contrast agent in the left lateral of the oesophagus 1 3 826 radiol med ( 2017 ) 122 : 822828 fig . 
4 low - dose fluoroscopy ( a ) and digital radiograph ( b ) images of a 48 - year - old obese patient ( bmi > 35 ) post - sleeve gastrectomy with comparable diagnostic image quality discussion in this study , we investigated the dose exposure and image quality of an optimized ultralow - dose digital pulsed protocol for fluoroscopic examinations of the ugi . 
we found significantly reduced organ doses in both the direct field of view and in distant radiosensitive organs at a sufficient image quality to ensure a reliable diagnosis . due to frequent clinical use , dose saving strategies are mandatory for fluoroscopic examinations of the ugi . 
the first are at particular risk for developing late radiation damage [ 11 , 26 , 27 ] , whereas the latter inevitably receive a higher radiation exposure as compared to normal weight patients , due to the larger body profile and images are often of minor diagnostic quality , in particular when the radiation dose is limited to a reasonable extent [ 28 , 29 ]  . 
several studies investigating these technical advances are available for diagnostic / interventional 1 3 radiol med ( 2017 ) 122 : 822828 procedures of the vascular system [ 3032 ] and for examinations of the gi and urogenital tract in paediatric radiology [ 1 , 11 , 13 ]  . 
with the investigated ultralowdose protocol comprising the latest hardand software technologies in this study , we fill this gap by providing an analysis of the image quality and reference organ dose measures for an average adult fluoroscopic ugi examination in clinical routine . nevertheless , the results of this study need to be interpreted in the study setting . 
although we consider that the presented organ doses as an overview for a standardized ugi examination in clinical routine using modern hard and software techniques , it is important to remember that these results only apply for the specific protocol settings and detector system used . 
other systems and acquisition parameters will affect the actual dose absorbed by radiosensitive organs ; thus , our results may only serve as a general guideline and must not be seen as absolute values . a well - known fact of x - ray imaging regardless of the chosen modality , is to determine a reasonable trade - off between the required image quality for a reliable diagnosis and the radiation burden of the patient . 
the results of our phantom and patient study indicate that our fp protocol warrants these conditions , as all examinations were considered to be of sufficiently diagnostic image quality at significantly reduced organ doses . 
this dose distribution pattern is in line with emigh etal . , who also conducted a phantom study to investigate dose exposure in paediatric ugi examinations , although a direct comparison is not possible due to their different patient collective and fluoroscopy system [ 1 ]  . our study has the following limitations . 
for indications , in which high temporal resolution is not the primary focus of interest , reducing the pulse / frame rate is advisable to further reduce cumulative radiation dose . 
 we included 46 patients ( 27 male ; mean age : 57 years , range 1285 years ) with histologically proven soft tissue tumours ( 10 benign , 2 intermediate 34 malignant ) grouped into eight tumour type classes . 
approximate receiver operating characteristic curves were created to predict possible uses of adc to differentiate benign from malignant tumours . results there was a significant difference ( p < 0.01 ) in adcs between these three groups excluding myxoid sarcomas . 
a significant difference was also evident between the tumour type classes ( p < 0.001 ) , grade ii and iii myxoid lesions ( p < 0.05 ) , tumour grading classes ( p < 0.001 ) and cellularity scores classes ( p < 0.001 ) , with the lowest adcs in the very high cellularity . 
an optimal cut - off adc value of 1.45 103 mm2 / s with 76.8% accuracy was found to differentiate benign from malignant tumours . conclusions dwi may offer adjunctive information about soft tissue tumours , but its clinical role is still to be defined . keywords diffusion mr imaging soft tissue tumour introduction the last 15 years have witnessed the application of diffusion - weighted imaging ( dwi ) in evaluation of lesions in several anatomical regions , including the brain and breast , so as to assess its ability to provide information regarding histology and grading of tumours [ 1 , 2 ]  . 
several investigators have reported an inverse correlation between the apparent diffusion coefficient ( adc ) values and cellularity , vol . : ( 0123456789 ) 1 3 872 radiol med ( 2017 ) 122 : 871879 evaluated also with the ki - 67 labelling index in the neuroradiological field [ 3 , 4 ]  . 
previous studies have already applied dwi to musculoskeletal oncology attempting to understand the existing correlation between adc values and soft - tissue sarcoma cellularity [ 5 , 6 ] and the presence of some types of matrix , such as those observed in myxoid tumours [ 7 , 8 ]  . 
furthermore , the mechanisms of diffusion in tumours are complex and related to multiple factors , including structure of the vascular network and extracellular matrix , membrane integrity and alteration of water exchanges between the intravascular , extracellular and intracellular spaces , and relative volumes of these spaces [ 10 , 11 ]  . 
in our study , we try to verify whether dwi might be able to investigate the benignancy / malignancy and the tumour type of soft tissue masses , the presence of myxoid matrix and the grading of sarcoma , defining tumour cellularity . 
for this purpose , we reviewed the dwi sequences performed on the patients with soft tissue masses , sent to our orthopaedic oncological referral centre for the study and treatment of soft tissue sarcomas . contrast mediu the routine protocol examination was : axial fse t2 , coronal stir , axial fse t1 fat - sat and sagittal fse t1 before and after contrast - media . 
an axial single - shot epi sequence with diffusion gradient along three directions , two b values ( 0 and 800 s / mm2 ) and an axial t2 - weighted fse sequence with the same geometric parameters were performed . image interpretation the adc was calculated by a linear regression analysis of the function s = s0exp ( badc ) , where b is the diffusion factor , s is the signal intensity after application of the diffusion gradient and s0 is the signal intensity at b = 0s / mm2 . 
quantitative colorimetric adc maps were obtained on a voxel - by - voxel basis , by dedicated software ( functool 3.1 ; ge company ) and were matched against the axial t2 images . 
for each lesion , a large region of interest ( roi ) was outlined by hand on adc maps in at least three consecutive slices , avoiding any suspected necrotic or cystic area at t2 - weighted and contrast - enhanced images . the average of adc values of all rois was calculated for each lesion . materials andmethods histological examination patients we reviewed the dwi sequences performed during the magnetic resonance imaging ( mri ) examinations of soft tissue tumours in the period from august 2012 to december 2015 . 
we included in our study patients with : a new histologically proven soft tissue tumour biopsied at our institution and whose specimen was then evaluated by an experienced pathologist in sarcoma ; a lesion size at least equal or greater than 1cm ; mri performed at our institution with our standard protocol including dwi sequences before any surgery , biopsy , chemotherapy or radiation therapy . 
with these criteria , 46 patients ( 19 female , 27 male ; mean age : 57 years , range 1285 years ) with 46 lesions ( average diameter 9cm ) were enrolled ( table1 )  . institutional review board approval was obtained for this retrospective study with a waiver of the requirement for informed consent . mr protocol the dwi was added to the routine protocol examination and performed before the intravenous administration of in all cases , histological diagnosis was obtained after an ultrasound - guided core - needle biopsy ( 16 - 18g ) by an experienced pathologist in sarcoma . 
 neoadjuvant chemotherapy in six high - grade sarcoma and radiotherapy in one ii grade myxoid liposarcoma were performed . the pathologist grouped the soft tissue masses into six tumour type according to world health organisation ( who ) classification [ 14 ] and evaluated the histopathological grading of sarcoma according to the fdration national des centres de lutte contre le cancer ( fnclcc ) system [ 15 ]  . 
similar statistical analysis was done for the adcs of each grading group ( g1 , g2 , g3 )  . we used the t test , with bonferroni adjustment , between the myxoid and non - myxoid lesions , between ii and iii grade myxoid lesions , between grade ii myxoid lesions and all the others lesions . 
moreover , there was a statistically significant difference between the adcs of grade ii and grade iii myxoid lesions ( p < 0.05 ) and between grade ii myxoid and all the other lesions ( p < 0.002 ) , whilst the statistical difference was less ( p < 0.02 ) between grade iii myxoid lesions and all the non - myxoid lesions ( table4 )  . anova showed a significant difference between the adcs based on tumour grading ( p < 0.001 ) ( table5 ) and on cellularity scores ( p < 0.001 ) ( table 6 )  . 
the diagnostic performances of adc cutoff values to differentiate benign from malignant tumours using roc curve analysis are shown in fig.1. figures2 , 3 , 4 and 5 show some representative cases of our study population . discussion our main findings were the significant differences of adc values between benign , intermediate and malignant soft tissue tumours , especially excluding myxoid sarcomas , and between the tumour type classes , but with a wide overlapping of the average adc values . 
we found also was a significant difference between the adc values of the lesions with very high cellularity and all the others tumours , with a 1 3 876 radiol med ( 2017 ) 122 : 871879 about pathological features of soft tissue masses [ 21 , 22 ]  . 
however , it is not easy to compare our results with those of previous works since different mri protocols were used , especially applying different b values on dwi sequences . 
reported that lymphoma was the only muscle masses that showed statistically significantly lower adc values while muscle sarcoma presented with a broad range of adc values [ 23 ]  . 
it is well known that lymphoma has very high cellularity and elevated nuclear - to - cytoplasm ratio , so there is lower diffusivity of water molecules in localizations of disease , thereby increasing dwi signal intensity of nodal and extranodal lymphomatous lesions [ 24 , 25 ]  . further , the use of dwi is a promising technique for the evaluation of treatment response . 
following chemotherapy , changes in tumour diffusion have been demonstrated to occur prior to morphologic changes [ 26 , 27 ]  . in our study , we also observed the overlap of the adc values but a statistical significant difference was observed fig . 
1 roc curves showing the diagnostic performance of adc to differentiate benign from malignant soft tissue tumours strong correlation between the adc values and the tumour grading and cellularity scores . mri is the method of choice for the diagnostic work - up of soft tissue tumours [ 16 ] , but although the site and the morphology of a lesion may help in the hypothesis of the histological type , mri provides only limited information as to grade of malignancy and histologies . 
as literature has reported statistically proven evidence correlating the adc values of some brain tumours to their cellularity [ 3 , 17 ] , the last 15 years witnessed the introduction of dwi also into the study of other oncologic diseases [ 1820 ] , including soft tissue tumours to obtain further information fig . 
2 axial b800 dwi image ( a ) , axial fse t2 image ( b ) and the colorimetric adc map matched against the corresponding axial t2 image ( c ) show a subcutaneous tumour of the left thigh that was biopsied . 
5 coronal stir image ( a ) axial fse t2 image ( b ) and the colorimetric adc map matched against the corresponding axial t2 image ( c ) , show a subcutaneous lymphoma of the right leg with average adc 0.47103mm2 / s 1 3 878 radiol med ( 2017 ) 122 : 871879 between benign , intermediate and malignant tumours excluding myxoid tumours . 
 while the simple linear regression analysis showed a significant relationship between adc values and tumour cellularity and grading , no significant relationship was found with age , gender , tumour size and histological subtype . significantly higher adc values have been observed in myxoid containing lesions , both of benign and malignant nature , than non - myxoid tumours [ 7 , 8 ]  . 
indeed , myxoid soft tissue tumours have a gelatinous matrix stroma , with high levels of hyaluronic acid and immature collagen fibres [ 28 , 29 ] , where the free water molecules diffuse amply within the large extracellular spaces . 
further , in our work we have demonstrated the presence of a statistically significant difference between the ii grade myxoid lesions , which have high adc values typical of myxoid lesions reported in the literature , and the iii grade myxoid lesions . in 2009 , schnaupauff etal . 
however , it is well known that adc values can increase in malignant soft tissue masses with consistent necrosis and decrease in fat or calcific containing benign soft tissue tumours such as in haemangioma [ 27 ]  . in our study , we have demonstrated a statistically significant difference only between lesions with a very high cellularity , characterized by the lowest adc values , and all the other lesions ( lesions with high , medium and low cellularity )  . 
in this regard , dwi might be helpful to identify , within soft tissue tumours , those areas with the higher cellularity which would be the best target of biopsy to better characterize the lesions . 
the increase in cellularity may also explain the drop in the adc values observed in g3 sarcoma and in iii grade myxoid sarcoma ( grade iii myxoid liposarcoma and grade iii myxofibrosarcoma )  . 
this would also suggest the interaction between the cellularity and the myxoid matrix on the adc values [ 11 ]  . nevertheless , we have to underline the semi - quantitative evaluation of the cellularity performed in our study that represented the strongest limitation of our work and did not allow , in any case , evaluating the linear correlation between the cellularity and the adcs . seven patients were given neoadjuvant therapy after the mr examination and biopsy . 
as anticancer therapy modifies cellularity , these cases show a discrepancy between the pre - therapy cellularity evaluated at dwi and post - therapy cellularity observed by the pathologist on surgical specimens . 
moreover , although most authors advocate the use of a range of values between 0 and 1000s / mm2 , there is still debate as to which b value should be used . 
in the consensus conference held in toronto in 2008 , the use of at least three values , in the range of 150900mm2 / s , was advocated so as to reduce the influence of intra vascular incoherent motion on the adc values [ 30 ]  . 
the perfusion - insensitive diffusion coefficient is calculated using an exponential function fitted only through the high b values ( b 300 , 450 and 600s / mm2 ) that excluded the initial reduction of signal intensity , probably caused by vascular capillary perfusion [ 11 ]  . 
last , another limitation of the study is the relatively small number of patients . in conclusion , although our data are limited , this study demonstrates that dwi may offer adjunctive information regarding soft tissue masses . 
it may discover benign or malignant soft tissue tumours with very high cellularity and the areas with higher cellularity within each mass , but it does not allow a confident diagnosis of benignancy or malignancy before the biopsy . 
therefore , although this and previous studies have investigated the application of dwi on musculoskeletal radiology , it represents an attractive noninvasive diagnostic tool , but its clinical role is still not completely clear . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the definitive diagnosis was established after pregnancy termi nation by means of skeletal standardized x - rays , histopathology and gene analysis . results td and oi - 2 long bones were significantly shorter than controls . 
the spine was steadily characterized by flat tened anterior vertebral bodies . conclusion long bone shortening is not a sufficient and accurate sign for early sonographic differential diagnosis between td and oi - 2 . 
angled diaphysis , axial diaphyseal displacement and a conserved vertebral body height in the prenatal period support the diagnosis of osteogenesis imperfecta type 2 , while moderately regular bowed diaphysis associated with platyspondyly that of thanatophoric dysplasia . keywords short and bent long bones osteogenesis imperfecta 2 thanatophoric dysplasia comparative morphometry introduction shortening and bowing of fetal or newborn long bones are considered a diagnostic sign of skeletal dysplasia . 
1 , 25100 brescia , italy 2 orthopaedic clinic , department of medical and surgical specialties , radiological sciences and public health , university of brescia , brescia , italy 3 prenatal diagnosis unit , department of obstretics and gynecology , asst spedali civili of brescia , brescia , italy 4 genetic laboratory galliera hospital genova , genoa , italy 1 3 radiol med ( 2017 ) 122 : 880891 an analysis of the international skeletal dysplasia registry ( isdr ) not less than 40 dysplasias were observed to be associated with bowed or angulated long bones [ 1 ]  . 
the other dysplasias included : short - rib dysplasia with or without polydactyly ( 10.2% ) , hypophosphatasia ( 3.5% ) , femoral hypoplasia ( fh ) ( 3.5% ) , type 2 collagen defects ( 3.1% ) , stuvewiedemann dysplasia ( 2.2% ) dyssegmental dysplasias ( dd ) ( 1.5% ) , achondroplasia ( ach ) ( 1.3% ) , otopalatodigital syndrome type 2 ( opd2 ) ( 1.3% ) , metaphyseal dysplasias ( 1.1% ) [ 2 ]  . 
on prenatal us , a diagnosis of the specific skeletal dysplasia is often uncertain so that the definitive diagnosis can only be established after birth or pregnancy termination from x - rays , histopathological and genetic investigations [ 35 ]  . size and shape of long bones evaluation is used in prenatal ultrasound to screen for severe or lethal skeletal dysplasias [ 6 ]  . 
in both thanatophoric dysplasia ( td ) and osteogenesis imperfecta type 2 ( oi - 2 ) , short , angulated or bowed long bones are the basic ultrasonographic criteria for the diagnosis . 
td is divided into two subtypes : type i , it is characterized by micromelia with bowed femurs , cloverleaf skull deformity may or may not be present ; type ii , it is characterized by micromelia with straight femurs and usually cloverleaf skull deformity is identified . 
other features common to both types of td include : frontal bossing , short ribs , narrow thorax , protuberant abdomen , and redundant skin folds . fgfr3 is the only mutated gene in td type i and td type ii . 
the clinical features of col1a1 / 2 - related oi represent a continuum ranging from perinatal lethality to individuals with severe skeletal deformities , mobility impairments , and very short stature to nearly asymptomatic individuals with a mild predisposition to fractures , normal dentition , normal stature , and normal life span . 
col1a1 / 2 - related oi has been classified into four types ( i , ii , iii , and iv ) based on clinical presentation and radiographic findings . in the present study , x - ray morphology and morphometry was carried out on long bones and spine after pregnancy termination and the x - ray - based diagnosis was compared with the first us report . 
the purpose of the paper was to assess the morphometric parameters to improve the specificity of the us signs for the early differ ential diagnosis between the two dysplasias . materials and methods fourteen cases of rhizomelic skeletal dysplasia with bent limb were selected from the prenatal ultrasound database of the department of pediatric radiology , spedali civili di brescia ( in the period from january 2007 to december 2013 )  . 
cultured amniocytes showed in all cases a normal karyotype . written informed consent was given by both parents ( or at least by the mother ) for radiological examination of the fetus and histopathological examination , for confirmation / further diagnostic purposes . after delivery , x - rays were taken in lateral and anteroposterior projections of the fetus in a standardized position . 
the thorax and the limbs were secured to the x - rays digital panel surface with adhesive tape ; upper limbs with 30 of shoulders abduction , extended elbows and supinated hands . 
lower limbs were positioned in neutral position unless severe bowing of the femurs , in which the hips were abducted and extra - rotated so that the bowed segment could lie flat on the digital panel as much as possible . 
 a full fetal autopsy was subsequently performed , with extensive tissue sampling for histopathology review . after x - ray and histopathological examination , the definitive diagnosis was td in eight cases and oi - 2 in six cases . 
the radiological and histopathological diagnosis was confirmed on fetal dna after pregnancy termination for td by genetic analysis of fgfr3 gene in seven cases and for oi - 2 by genetic analysis of the col1a1 and col1a2 genes in three cases . 
1 x - ray length measurement of the diaphysis , bar 1 c a in straight femur of the control group ( gestational age 20 weeks ) , the length was measured along the median longitudinal axis . 
in both bowed and angulated bones , the angle formed by the intersection of two straight lines drawn along the median , longitudinal axis of the bone proximal and distal segments . 
the dorsal and lumbar tract mean values were reported separately . statistical analysis upper and lower limb long bones intergroup differences of length and angle and the spine anterior ossification center size , were compared with students t test ( p values < 0.05 were considered statistically significant )  . x - rays were examined and measured independently by two radiologists ( mpb and gdg )  . 
the standard deviation of interobservers and intraobserver variation resulted within the interval 2 sd . histopathology bone specimens processed for histology included : chondro - sternal junctions and anterior arc of the ribs , spine , right femur and / or tibia , calvaria . 
the specimens were fixed for 24 h in neutral , buffered formaldehyde solution ( 10% ) and then stored in a 4% solution of the same fixative at 4 c until further processed . 
after decalcification in edta ( 10% ) for 1 week the specimens were dehydrated in an ascending scale of ethanol , embedded in paraffin and 610 m thick sections were prepared . 
they were stained with haematoxylin eosine and observed with a light microscope olympus bx 51 ( olympus optical ltd , tokio , japan ) equipped with an image view camera ( soft imaging system gmbh , munster , germany ) in bright field and in polarized light . molecular analysis genomic dna was isolated from amniocytes or chorionic villous . fgfr3 exons 7 , 10 , 15 and 19 ( hot spot regions for td mutations ) were amplified separately with one unit of eurobiotaq dna polymerase ( eurobio ) using a set of primers and pcr protocols defined in our laboratory . 
sequencing reactions were purified with multiscreen filter plates ( millipore corporation , bedford , usa ) and run and analysed on an 3130xl genetic analyzer ( applied biosystems )  . all coding exons and flanking exonintron junctions of the col1a1 and col1a2 genes were amplified by pcr and analyzed by direct sequencing , using bigdye terminator version 3.1 cycle sequencing kit and an abi prism 3130xl automated dna sequencer ( applied biosystems , foster city , ca )  . 
in td bowed bone ( a ) and in oi angulated bone images ( b ) ( both with a gestational age of 21 weeks ) , the angle is formed by the intersection of two lines sketched along the median , longitudinal axis of the bone . 
3 x - ray spine height measurement , bar 1 c the height of each vertebral body was measured on the median vertical line ( in ap and ll projections ) ; final measurement was calculated as the mean of these two projections . 
in td ( gestational age 21 weeks ) ( cd ) the ossified vertebral body appears flat and underdeveloped , while in oi ( gestational age 21 weeks ) ( ef ) there is no evidence of vertebral body height reduction results xray morphology thanatophoric dysplasia was characterized by bowed long bones . 
the metaphyseal width was regular , but the bone got narrower toward the midshaft , with a peculiar triangular shape of both the proximal and the distal half shaall the bones were osteopenic and there was no evidence of a true cortical bone . 
no evidence of vertebral body collapse was observed in any of the osteogenesis imperfecta type 2 up to the age of 22 gestational weeks . long bones and spine xray morphometry the anterior ossification center height of dorsal vertebrae ( from d9 to d12 ) was significantly smaller in td cases than in oi - 2 cases and in controls . 
the same analysis for lumbar vertebrae revealed that the anterior ossification center height ( from l1 to l3 ) was significantly smaller in 1 3 886 radiol med ( 2017 ) 122 : 880891 fig . 
spine height was measured in dorsal and lumbar vertebrae from healthy controls ( white bars ) , oi - 2 ( light grey bars ) and td ( grey bars ) fetuses . 
spine height was measured in dorsal and lumbar vertebrae from healthy controls ( white bars ) , oi - 2 ( light grey bars ) and td ( grey bars ) fetuses . 
the mean angulation / bowing angle for single bone type was significantly different between td and oi - 2 , with the exception of right ulna and left femur ( table 3 )  . 
angulation or acute angle bowing were , respectively , related to a recent or previous ( due to the periosteal apposition and remodeling ) fracture of a long bone , therefore , these signs can be considered indicative of osteogenesis imperfecta . 
furthermore , bowing of a long bone may be related to thanatophoric dysplasia too , but in this case it should be characterized by a less acute angle . either deformities were otherwise almost constant in femur , tibia and humerus , with a more frequent observation in lower limb bones in both dysplasias ( table 4 )  . histopathology oi - 2 chondrocytes of the long bones epiphyseal ossification centers , of the metaphyseal growth plate cartilages and of the spine ossification centers showed a regular maturative pattern with columnation , hypertrophy and degeneration . 
therefore , the x - rays documented radiopacity was due exclusively to calcified cartilage . fractures they occurred in different periods of the fetal development as the diaphyses were ubiquitous , discussion the assessment of long bones length and bowing has a relevant role in the prenatal diagnosis of skeletal dysplasias [ 15 ]  . 
however , precision and accuracy of these parameters measurement are certainly conditioned by the technical performance of the employed device and the operator ability , but also by the fetal bones position relatively to the ultrasound probe [ 16 , 17 ]  . these biases are less relevant in the x - ray survey as carried out in the present study . 
 however , since they concern the same targets ( the bones ) examined in different conditions , observation derived from the first method ( x - rays ) can be translated to the second ( us ) and supply useful indications for who is performing both x - ray and us methods of measurement assess only ossified or calcified tissues . 
in the present study , the x - rays projectional bias was limited by standard positioning of the fetal limbs . the prenatal differential diagnosis between the most frequently observed skeletal dysplasias , oi - 2 and td , may often be uncertain [ 17 , 18 ]  . 
it is based on the following ultrasonographic signs : long bones shortening and bowing , fractures , osteopenia , narrow chest , short ribs , cloverleaf skull . the morphometric analysis carried out in the present study documented that a significant shortening was present both in oi - 2 and td compared to controls . 
this was a common feature of all the long 1 3 888 radiol med ( 2017 ) 122 : 880891 1 3 radiol med ( 2017 ) 122 : 880891 fig . 
therefore , we suggest assessing first the bowing angle and then try to discriminate the two conditions based on bowing and angulation of the long bones . from the results of the present study , the us assessment of the vertebral centers morphology and morphometry may be even more relevant than diaphyseal length bowing for differential diagnosis because the oi - 2 spine - calcified car tilage centers do not collapse until the peri - natal or postnatal period . 
this behavior of the spine is explained by size and shape of the calcified cartilage scaffold ( a parallelepiped with small differences in the 3 - d dimensions ) , it can withstand the low axial load in the amniotic environment . 
 differently the long bone diaphysis in the same environment is subjected to tensional or torsional stresses along the longitudinal axis sufficient to overcome the threshold of resistance of the cortex - calcified chondroid tissue . bowing was a constant feature of both dysplasias in humerus , femur and tibia ( the longest bones ) , absent in metacarpals and metatarsals ( the shortest ) , and variable in radius and ulna . 
in the latter population , the curvature of the diaphysis was always shaped as a regular arc , while in oi - 2 angled deformation was documented in approximately onethird of cases . histopathology explains the different pathogenesis of shortening and bowing of oi - 2 and td . 
the displacement , the angulation or the more rounded bending depends on the gestational age at which the fracture occurred , and on time the repair tissue has had to be remodeled . 
on the contrary , the vertebral body calcified cartilage centers do not fracture up to the 22nd week or later [ 19 ] , even if formed only by a scaffold of calcified cartilage they can withstand the low axial load in the amniotic environment and the vertebral soma do not collapse . 
this can occur later in intrauterine life or after birth , when the axial loads on the spine increase . 1 3 890 radiol med ( 2017 ) 122 : 880891 this mechanicistic explanation is supported by the observation of fracture bowing distribution in long bones which follow the length scale of the limb bones : femurs tibia metacarpal / metatarsal . radius / ulna humerus histopathology of td is characterized by a defective chondrocyte differentiation , maturation and organization inside the ossification center [ 19 ]  . 
asymmetrical loads on a structurally weak ossification center of the long bone diaphysis or of the spine can explain the deformities documented by x - ray imaging and histology in this study . 
 the occurrence of fractures cannot be excluded , however , they eventually resemble rather the fatigue fractures of the adult than the displaced diaphyseal fractures of osteogenesis imperfecta type 2 and 3 [ 20 , 21 ]  . the current study has some limitations . 
however , given the short gestational interval at which termination of pregnancy was performed ( 1822 weeks ) and the extreme bone shortening observed in both td and io - 2 fetuses , the lack of adjustement for gestational age of our measurements is unlikely to bias the findings . 
however , the available x - rays and histopathological findings were characteristic enough to assign these cases to one of the two types of dysplasia . in conclusion , x - ray morphometry carried out in oi - 2 and td pregnancy terminations can give a rational basis to the interpretation of early us reports . 
in short limb dysplasias ( like td and oi - 2 ) acute angle bowing or axial displacement of the diaphysis associated to a conserved height of vertebral body calcified scaffold suggests osteogenesis imperfecta type 2 . 
a peripheral part of the metaphyseal growth plate cartilage showing maturation of the chondrocyte but the normal columnation of chondrocyte ( bar ) is not present on the external site of the pericondral bone bark ( arrows )  . 
ethylenevinyl alcohol copolymer was used as embolic agent in 12 patients : alone in 5 cases , in association with glue and with glue and thrombin in 3 and 2 cases , respectively , during tae . 
onyx was injected in two cases of embolization performed with dpsi : in one case alone and in the other in combination with thrombin and glue . results technical success rate was 100% . 
immediate clinical success was 91.7% ; in one patient ceus revealed * gianpaolo carrafiello gcarraf@gmail.com interventional radiology , department of radiology , insubria university , viale borri 57 , 21100 varese , va , italy 2 diagnostic and interventional radiology unit , university of milan , viale di rudin 7 , milan , italy 3 vascular surgery department , university of insubria , viale borri 57 , 21100 varese , va , italy 4 department of radiology , luigi sacco university hospital , via g.b. 
camillo hospital , circonvallazione gianicolense 87 , 00152 rome , italy 6 department of radiology , universit degli studi del molise , campobasso , cb , italy persistent t2 el , decreased if compared with that before the procedure . 
no major or minor complications were registered . conclusions onyx could be an ideal embolic agent for endovascular and percutaneous embolization of t2 el . keywords ethylene - vinyl alcohol copolymer onyx type ii endoleak embolization introduction endovascular aneurysm repair ( evar ) is considered the standard therapy for most patients with abdominal aortic aneurysm ( aaa ) [ 1 ]  . 
el is defined as persistence of blood flow within the excluded aneurysm sac , classified according to the underlying etiology , location , and aortic branch vessel involvement [ 2 ]  . 
type i and type iii endoleaks require early intervention ; however , the treatment strategy for type ii endoleak remains controversial because spontaneous resolution is expected [ 2 ]  . 
several recent studies have demonstrated that nearly 20% of immediate type ii endoleaks persist and that persistent type ii endoleaks are associated with secondary interventions and aneurysm rupture [ 2 , 3 ]  . 
1 axial ct shows aneurysmal sac supplied ( type ii endoleak ) ( arrow ) ( a ) ; multiplanar reconstruction confirms type ii endoleak ( arrow ) ( b ) communicate through a channel . 
direct puncture sac injection ( dpsi ) is usually performed after unsuccessful transarterial embolization ( tae ) or persistent endoleak and enlargement of the aneurismal sac after tae [ 5 ]  . 
due to these properties and because onyx is not absorbable , it is capable of producing permanent vascular occlusion [ 6 ]  . we report our experience with the use of ethylene - vinyl alcohol copolymer ( onyx ) for the treatment of type ii endoleaks after evar either with endovascular that percutaneous approach . materials and methods from march 2007 to march 2015 , 455 patients with aaa underwent to endovascular exclusion . 
patients were routinely monitored at the institution and follow - up included computed tomography angiography ( cta ) at 30 days , cta or contrast enhanced ultrasound ( ceus ) at 6 months and cta at 12 months postoperatively and annually thereafter . 
a total of 22 patients ( 30.5% ) met the criteria for treatment . ceus was performed in all patients before treatment , to confirm t2 el and its origin ( lumbar and / or mesenteric )  . 
 in one of the 22 patients , ceus pre - treatment revealed a high flow el ( t1b el ) , confirmed by angiography and treated with an iliac endogra in 21 patients , t2 el was treated with tae ( n 18 ) , dpsi ( n 10 ) or laparoscopic ligature of the inferior mesenteric artery ( n 1 )  . 
dpsi was considered in case tae was unsuccessful , which occurred in 8 out of 18 patients . in this study , we considered all the embolization performed using ethylenevinyl alcohol copolymer ( onyx , ev3 neurovascular , irvine , california ) as embolic agent , alone or in combination with other embolic agents . 
onyx was injected in two cases of embolization performed with direct puncture of the sac : in one case alone and in the other in combination with thrombin and glue . 
the choice of embolic agent was at the discretion of the operator , although glue and onyx were used primarily when endoleak persisted at the angiography or saccography performed during the procedure . all procedures performed in this study were in accordance with the ethical standards of our institutional research committee and with the 1964 helsinki declaration and its later amendments . 
safety was defined as the frequency of intra - , periand post - procedural complications [ 5 ]  . results eleven men and one woman with a mean age of 62.8 years ( range 5283 years old ) comprised the study population ( table 1 )  . 
the indication for endoleak treatment included persistence of a type ii endoleak after 12 months follow - up and enlarging aneurysm sac size . a direct aneurysm sac access approach was employed in 10 patients and the transarterial access was used in 18 patients . 
3 contrast enhanced ultrasound ( ceus ) confirmed type ii endoleak ( a ) ; direct puncture of the sac was performed using cbct as imaging guidance ( b , c ) ; onyx was injected directly by the needle used for the puncture ( d ) ; final cbct confirmed distribution of the onyx in the sac ( e ) 1 3 158 radiol med ( 2017 ) 122 : 154159 immediate clinical success was 91.7% , in particular in 11 / 12 cases ceus performed at the end of the procedure demonstrated absence of endoleak ; in the remaining case ( 1 / 12 ; 8.3% ) ceus revealed persistent t2 el , decreased if compared with that before the procedure . 
cta was performed as protocol of follow - up and confirmed clinical results reported . secondary clinical success was 91.7% ; until today , in one patient t2 el is persistent , with suspected inflow from a small patent lumbar artery ; nevertheless , at the moment of submission ( follow - up of 24 months ) , the patient remains asymptomatic and the sac diameter is stable ( 55 mm ) , therefore , no indication for re - treatment are present . no major or minor complications were registered during or after the procedure . 
during the procedure , one patient treated with endovascular approach , complained mild abdominal pain , at the beginning of the embolization ( probably related to the arrival of dmso within the el ) , but any analgesic was administered . 
at the end of the procedure , one of the two patients treated with percutaneous approach , experienced mild back pain , solved with common analgesics within 24 h . discussion type ii endoleak is the most common complication after endovascular aneurysm repair ( evar ) which could lead to a possible risk of aneurysmal sac enlargement and rupture [ 2 , 7 , 8 ]  . 
many techniques have been described to treat type ii endoleak . in the past , type ii endoleaks were usually treated surgically , both with graft explantation and with retroperitoneal ligation of collateral feeding vessels . 
if there are no arterial routes for transarterial embolization , dpsi is feasible as alternative method to treat type ii endoleak [ 9 ]  . during these years , embolization of endoleaks has been performed with many different embolic agents like glue , coils , thrombin and onyx . 
the principal advantage of the use of a liquid embolic agent in the treatment of type ii endoleaks relates to the ability of a liquid to fill the endoleak sac completely including all inflow and outflow vessels . 
the solid cast formed by a liquid embolic agent should result in a non compressible structure through which recanalization does not occur , providing more durable repair than that provided by coils . the onyx liquid embolic system consists of an ethylenevinyl alcohol copolymer dissolved in anhydrous dimethyl sulfoxide ( dmso )  . 
using onyx , the embolized vessels are completely filled by the embolic agent and are less fragile because of the lower inflammatory reaction and the absence of polymerization heat compared with nbca - embolized . 
 when the inflammatory reaction caused by onyx was evaluated on histologic specimens on humans , the inflammatory reactions of the vessel wall were less pronounced and were located mainly intravasally , while no reaction of the surrounding interstitium , such as migration of lymphocytes into perivascular areas , was observed [ 12 ]  . 
the inflammatory response and vascular toxicity seemed primarily to be associated with the injection rate , as the slow endovascular delivery of dmso produced no untoward angiographic or pathologic changes but a fast injection of dmso caused endothelial necrosis and severe inflammatory response in the arterial wall [ 13 , 14 ]  . according to this , onyx should be the best way to reach embolization . 
the association with other embolizing agents , like glue , is to prefer when the sac is large ; in this way we can get perfect and safe embolization of the sac . 
 we have started to use it in el that would need too much onyx , in particular the last patient of the list with percutaneous approach and in two recent cases of type ia el embolization by dpsi was used at the end of the procedure to fill proximal cap with extreme precision . the major weak point of the manuscript is represented by the small number of patients ( 12 patients ) enrolled in a long time period ( 9 - years )  . 
in addition , onyx was used alone or combined with other embolic agents , with endovascular or 1 3 radiol med ( 2017 ) 122 : 154159 percutaneous approach on the basis of the operator confidence and / or experience ; even this aspect may be considered a technical bias . no randomized study comparing different embolic agent and its capacity to fill sac is now available ; and it is difficult to achieve because even in large centers the number of cases is never so numerous . on the basis of the characteristics described onyx could be an ideal embolic agent and our experience demonstrated its safety ; to overcome the necessity to use too much onyx for a single procedure , it could be associated with others embolic agents and in particular its role could be to fill the gap remained in the sac filled by other embolic agents and to create a proximal cap communicating with the feeding vessel . 
we further aimed to investigate whether autopsy cases characterized by increased troponin t and i concentrations as well as morphological findings of myocardial ischemia were also characterized by pathological myocardial enhancement at multiphase postmortem computed tomography angiography . materials and methods two different approaches were used . 
in the second approach , 40 forensic autopsy cases that had a cause of death attributed to acute myocardial ischemia were retrospectively selected . results the preliminary results seem to indicate that the identification of a pathological enhancement of the myocardium at postmortem angiography is associated with the presence of increased levels of cardiac troponins in * cristian palmiere cristian.palmiere@chuv.ch 1 service danatomie pathologique et mdecine lgale , cliniques universitaires saint - luc , universit catholique de louvain , brussels , belgium 2 curml , university center of legal medicine , chemin de la vulliette 4 , 1000 lausanne 25 , switzerland 3 dipartimento di sanit pubblica e medicina di comunit , universit degli studi di verona , policlinico g.b. 
 analogously , a pathological enhancement of the myocardium at postmortem angiography can be retrospectively found in the great majority of autopsy cases characterized by increased cardiac troponin levels in postmortem serum and morphological findings of myocardial ischemia . conclusions multiphase postmortem computed tomography angiography is a useful tool in the postmortem setting for investigating ischemically damaged myocardium . keywords postmortem angiography pathological myocardial enhancement forensic autopsy myocardial ischemia postmortem biochemistry troponin introduction myocardial infarction ( mi ) can be defined according to different perspectives related to clinical , electrocardiographic ( ecg ) , biochemical , and pathologic characteristics . 
it is accepted that the term mi reflects a cardiomyocyte death caused by prolonged ischemia , the latter resulting from a perfusion - dependent imbalance between oxygen supply and demand . 
the rupture or erosion of a coronary atherosclerotic plaque is the most frequent underlying condition [ 1 , 2 ]  . traditional assessment of patients presenting to the emergency department ( ed ) with suspected acute coronary syndrome ( acs ) , such as mi , includes clinical risk assessment based on cardiovascular risk factors with serial electrocardiograms and cardiac troponin measurements [ 3 ]  . detection of myocardial cell necrosis resulting from prolonged ischemia can be evaluated by a number of different means , including pathologic examination ( contraction band necrosis , cardiomyocyte necrosis ) , biochemical 1 3 96 radiol med ( 2017 ) 122 : 95105 marker measurement of myocardial cell necrosis in blood ( cardiac troponins , mb fraction of creatine kinase ) , ecg recordings ( st - t segment wave and q wave changes ) , and imaging modalities ( echocardiography and coronary angiography )  . 
indeed , its diagnostic performance in assessing coronary stenosis has been demonstrated in numerous studies [ 1 , 3 ]  . in the realm of forensic pathology , the identification of mi is based on morphological findings ( obtained from autopsy , histology , and immunohistochemistry ) and biochemical investigation results , though the sensitivity and specificity of some techniques may differ markedly due to the onset of decompositional changes [ 4 ]  . indeed , immunohistochemical methods may be influenced by several mechanisms that occur during postmortem alteration , including protein decomposition , antigen diffusion , and unspecific antibody binding in the presence of disrupted protein structures [ 58 ]  . troponin i and t levels have been measured in various studies in postmortem serum obtained from blood sampled at different sampling sites , such as the femoral veins , iliac veins , subclavian veins , aorta , right heart , and left heart . 
 moreover , troponin concentrations measured after death have been demonstrated to correlate with the severity of ischemic myocardial damage , depending on postmortem intervals [ 4 , 9 ]  . on the other hand , additional findings have been described in recent reports . 
these assert that images obtained from multiphase postmortem cta ( mpmcta ) would enable not only coronary artery imaging and evaluation of luminal narrowing to be carried out , but also identification of mi areas as areas characterized by contrast enhancement within the myocardium ( increased radioopacity from contrast medium , mean hounsfield units 95 )  . 
since contrast enhancement is absent in the normal myocardium , this phenomenon is considered pathologic and is thought to be an indirect sign of a myocardial lesion [ 1013 ]  . to the best of our knowledge , no published reports exist to date having combined data obtained from mpmcta , investigation morphological findings and biochemical results in the cases of suspected myocardial ischemia that have undergone forensic autopsies . in the study herein described , troponin t and i concentrations were measured in postmortem serum from femoral blood in a series of forensic autopsy cases that underwent mpmcta . 
our first aim was to assess whether the identification of pathological myocardial enhancement at mpmcta was correlated with increased levels of these biomarkers as well as morphological findings of myocardial ischemia . 
our second aim was to assess whether autopsy cases characterized by increased troponin t and i concentrations as well as macroscopic and microscopic findings of myocardial ischemia were also characterized by pathological myocardial enhancement at mpmcta . materials and methods study design this study was conducted during 20092015 and was designed as a retrospective , single center study . 
mpmcta and troponin t and i measurements were performed as part of medicolegal investigations . mpmcta was performed according to the standardized protocol in three phases described in a previous study [ 14 ]  . two different approaches were used . 
in one , 40 forensic autopsy cases ( 27 male subjects and 13 female subjects between 22 and 90 years of age ) that underwent mpmcta and had pathological enhancement of the myocardium ( mean hounsfield units 95 ) radiologically observed , were retrospectively selected . 
the aim was to assess whether the identification of pathological enhancement of the myocardium at mpmcta was correlated with increased troponin t and i values as well as the morphological findings of myocardial ischemia . 
in 10 out of 40 cases , death and medicolegal investigation intervals ranged between 36 and 48 h . at the same time , in the second approach , 40 forensic autopsy cases ( 28 male subjects and 12 female subjects between 36 and 67 years of age ) that underwent mpmcta and had a cause of death attributed to acute myocardial ischemia based on macroscopic and microscopic findings as well as biochemical investigation results were retrospectively selected . 
the aim was to assess whether autopsy cases characterized by increased troponin t and i concentrations as well as the macroscopic and microscopic findings of myocardial ischemia were also characterized by pathological enhancement of the myocardium at mpmcta . 
in 13 out of 40 cases , death and medicolegal investigation intervals ranged between 34 and 50 h . the cases included in the second case series were characterized by the presence of one of the following combinations of macroscopic and microscopic findings : 1 3 radiol med ( 2017 ) 122 : 95105 coronary artery atherosclerosis and acute coronary thrombosis without acute myocardial infarction . in these cases , postmortem angiography revealed complete interruption of coronary artery opacification at various sites . 
macroscopy and microscopy revealed the presence of acute thromboses in the coronary arteries as well as the presence of morphological signs of myocardial ischemia . coronary artery atherosclerosis and acute coronary thrombosis with acute myocardial infarction . in these cases , postmortem angiography revealed complete interruption of coronary artery opacification at various sites . 
macroscopy and microscopy revealed the presence of acute thromboses in the coronary arteries and the presence of morphological signs of myocardial infarction . rupture or erosion of a coronary atherosclerotic plaque , with or without hemorrhage within the plaque , with or without acute myocardial infarction . in these cases , postmortem angiography revealed various degrees of coronary artery atherosclerosis with no evidence of significant luminal narrowing . 
microscopy revealed the presence of rupture or erosion of a coronary atherosclerotic plaque , with or without hemorrhage within the plaque and with or without morphological signs of acute myocardial infarction . acute myocardial infarction with or without rupture left ventricular free wall rupture . in these cases , postmortem angiography revealed various degrees of coronary artery atherosclerosis , with or without evidence of interruption of coronary artery opacification . 
macroscopy and microscopy revealed the presence of myocardial infarction , with or without left ventricular free wall rupture , with or without acute thromboses in the coronary arteries . coronary artery atherosclerosis , without acute coronary thrombosis , with morphological signs of myocardial ischemia . in these cases , postmortem angiography revealed various degrees of coronary artery atherosclerosis without evidence of interruption of coronary artery opacification . 
 macroscopy and microscopy failed to reveal the presence of acute thromboses in the coronary arteries and revealed the presence of morphological signs of myocardial ischemia . all cases selected for this study originated from forensic practice with deaths occurring outside the hospital . 
medical records and clinical histories of the deceased as well as police reports were consistently reviewed before conclusions were made . case inclusion criteria for the first studied case series consisted of pathological myocardial enhancement at mpmcta and postmortem serum from femoral blood availability at autopsy . case inclusion criteria for the second investigated case series consisted of morphological signs of acute myocardial ischemia or myocardial infarction and postmortem serum from femoral blood availability at autopsy . postmortem investigations and sample collection unenhanced postmortem computed tomography ( ct ) scans were performed before any manipulation of the corpses in all cases included in the study . 
mpmcta was systematically carried out after unenhanced ct scans and prior to autopsies , according to the standardized protocol in three phases described in a previous study [ 14 ]  . 
autopsies were jointly performed by two forensic pathologists ( at least one board - certified ) as in accordance with both local standards and international guidelines for medicolegal cases . the presence or absence of pathological myocardial enhancement and its distribution within the myocardium was investigated by at least one board - certified forensic pathologist ( experienced in forensic imaging ) together with at least one board - certified radiologist unbeknownst to the results of previous investigations . 
the pathological enhancement of the myocardium was first identified in a subjective manner ( the presence or absence of enhancement according to the observers ) and second in an objective manner , by measuring the mean attenuation ( in hounsfield units ) of the myocardium ( using a region of interest of about 15 mm in diameter ) in the images of the three different mpmcta phases . conventional histology included haematoxylineosin ( he ) stains of brain , heart , lung , liver , and kidney samples . 
hearts were sectioned before or after fixation in 10 % neutral buffered formal the major epicardial coronary arteries were either serially sectioned at approximately 2 - mm intervals or longitudinally sectioned intact on the heart . 
in selected cases , histological sections of the coronary arteries were prepared at three different equally 1 3 98 radiol med ( 2017 ) 122 : 95105 spaced levels to best identify plaque rupture sites . 
full thickness areas involving the left anterior , lateral free wall , and left posterior ventricle as well as interventricular septum , and the right anterior , lateral free wall and right posterior ventricle were sampled . 
in selected cases , histology staining analysis for coronary arteries included he , massons trichrome and verhoeff van gieson as well as immunohistochemical investigations . toxicological analysis was performed in selected cases and included blood ethanol determination as well as general screening for volatile and nonvolatile drugs , poisons , and metabolites . peripheral blood from femoral veins was systematically collected for postmortem biochemistry as soon as possible upon arrival of the bodies at the morgue , prior to autopsy and prior to mpmcta . 
the latter were centrifuged immediately post collection at 3000g for 15 mafter centrifugation , the separated supernatant ( postmortem serum ) was collected and stored in preservative - free tubes . 
when analyses were delayed , samples were stored at 20 c . technical data chemically , the contrast medium angiofil is a mixture of esters ( mainly ethyl esters ) of polyiodinated fatty acids . 
 one study stated that combining an oily perfusate with a lipophilic contrast medium allows postmortem circulation and the performance of subsequent high - resolution postmortem angiography to be carried out . 
 paraffinum liquidum has appeared the most appropriated with which to perfuse a human body , while the use of the more viscous paraffinum perliquidum can lead to important extravasations , especially in areas where postmortem autolysis is more significant , such as the pancreas and gastric mucosa . 
by diluting angiofil with a solvent such as decane , viscosity can be decreased to the extent that it can enter the capillaries and , therefore , be used as a contrast medium in micro - angiography [ 8 ]  . 
using angiofil together with paraffinum liquidum as a solvent , as proposed per the standardized protocol of multiphase pmcta , the kinematic viscosity of the mixture measured at 40 c is approximately 6774 mm2 / s [ 10 , 14 ]  . histological alterations induced by oily contrast agents using oily contrast agent has the advantage that no leakage out of the vascular system occurs within the first 72 h . 
optical empty spaces within the vessels or even within the parenchyma are among the most common histological artifact after mpmcta with oily contract agent and are the histological analog to radiologic contrast agent - mediated oedema . 
optical empty spaces frequently appear in all tissues [ 10 ]  . laboratory assays cardiac troponin i was analyzed with the access accutni assay on access ii ( beckman coulter , fullerton , ca , usa )  . 
the clinical reference value ( according to the laboratory where the analysis was performed ) was 0.03 g / l ( corresponding to 0.03 ng / ml )  . levels of postmortem serum cardiac troponin t were measured with hs - tnt reagents by electrochemiluminescence immunoassay ( eclia )  . 
the clinical reference value ( according to the laboratory where the analysis was performed ) was 14 ng / l . toxicology consisted of ethanol determination and general unknown screening for common drugs and illegal substances by gas chromatography - mass spectrometry ( gcms ) using commercial mass spectrum libraries , 1 3 radiol med ( 2017 ) 122 : 95105 high - performance liquid chromatography with diode - array detection ( hplcdad ) , and headspace - gas chromatography flame ionization detection ( hsgcfid )  . all relevant ethical issues were identified and discussed with the local ethical committee . 
all the presented images pertain to the same case in which pathological myocardial enhancement and morphological findings of myocardial ischemia were identified . in the first case series ( 40 cases ) , the identification of pathological myocardial enhancement ( mean hounsfield units 95 ) at mpmcta systematically correlated with increased levels of troponin t and i as well as morphological findings of myocardial ischemia . 
no statistically significant differences between troponin concentrations and postmortem interval ( 1236 and 3648 h ) were observed . no case was noticed that had pathological myocardial enhancement at mpmcta without increased troponin levels or without morphological findings of myocardial ischemia . 
no case had exclusively increased troponin levels without morphological findings of myocardial ischemia , irrespective of the postmortem interval . analogously , no case had exclusively morphological findings of myocardial ischemia without increased troponin levels , irrespective of the postmortem interval . the enhancement of the myocardium at mpmcta ischemia localization of correlated with the the ( macroscopically and microscopically identified ) in all 37 cases . 
in some of these cases , the enhancement of the myocardium at mpmcta was markedly pronounced ( > 200 hounsfield units ) in the subendocardial areas of the left ventricle , where former infarcted areas were also histologically noticed . 
while the arterial phase of the mpmcta showed diffuse myocardial enhancement in most cases , this was more pronounced in the subendocardial regions of the myocardium during the venous and dynamic phases of the mpmcta . in the remaining 3 out of 40 cases , pathological myocardial enhancement at mpmcta correlated with increased levels of troponin t and i as well as various degrees of myocardial ischemia . 
the causes of death were considered to be septic shock , pulmonary embolism and trauma following a fall from heights in a subject with severe coronary artery atherosclerosis , coronary artery calcifications , and myocardial fibrosis . 
these include myocardial ischemia and direct myocardial damage due to substances released into the circulation by pathogens , cytokines , or reactive oxygen radicals released following the infectious process [ 1517 ]  . in pulmonary embolism , the sudden elevation of right ventricular pressure , and consequently increased right ventricular afterload produced by pulmonary artery outflow obstruction , results in right ventricular failure and dilatation . 
no statistically significant differences between troponin concentrations and postmortem interval ( 1434 and 3450 h ) were observed . no case had exclusively increased troponin levels without morphological findings of myocardial ischemia , irrespective of the postmortem interval . 
analogously , no case had exclusively morphological findings of myocardial ischemia without increased troponin levels , irrespective of the postmortem interval . as revealed in the first case series , myocardial enhancement at mpmcta correlated with the localization of the narrowing of the coronary artery and the localization of the myocardial ischemia ( macroscopically and microscopically identified ) in 38 subjects . 
this could be due to the fact that infarcted areas of very limited extension might not be detectable at mpmcta as pathological enhancement . globally considered , these results indicate that the identification of a pathological enhancement of the myocardium at mpmcta ( mean hounsfield units 95 ) is strongly associated with the presence of increased levels of cardiac troponins in postmortem serum and morphological findings of ischemia , irrespective of whether myocardial ischemia is considered the main cause of death , a factor contributing to death or just a potential trigger factor , as hypothesized in the case of the fall from heights in a subject with severe coronary artery atherosclerosis . analogously , a pathological enhancement of the myocardium at mpmcta can be retrospectively found in the great majority of autopsy cases characterized by increased cardiac troponin levels in postmortem serum and morphological findings of myocardial ischemia . 
this suggests the usefulness of combining mpmcta and postmortem biochemical analyses for the investigation of ischemically damaged myocardium . discussion ischemic injury of the myocardium can be differentiated as reversible and irreversible , as well as present in acute and chronic conditions . 
a , b the contrast enhancement within the myocardium ( increased radioopacity from contrast medium ) identified at mpmcta in a situation of narrowing of the coronary artery and myocardial ischemia . 
 g optical empty spaces within the vessels induced by the oily contrast material 1 3 102 radiol med ( 2017 ) 122 : 95105 refers to myocardium that is salvaged by timely reperfusion with transiently impaired contractile function that recovers spontaneously over time . 
hibernating myocardium refers to myocardium with chronically reduced contractile function associated with a local reduction in myocardial perfusion capacity [ 19 , 20 ]  . ischemic cardiomyocyte injury is characterized by progressive membrane damage with a variable degree of cell swelling . 
with prolonged ischemia , myocyte death spreads like a wave across the myocardiu the extent of necrosis depends on the occluded vessels territory , which also determined ischemia duration and the transmural extent of the infarction . 
scar tissue is markedly thinner than healthy myocardiuthe time course of this remodeling process is influenced by several factors and encompasses underlying disease or secondary event severity [ 1925 ]  . while the clinical use of differential contrast enhancement of ischemic myocardium is a relatively recent advance , the concept of differential enhancement / accumulation of contrast material in acute or chronic myocardial infarction in both cardiac magnetic resonance imaging ( mri ) and computed tomography ( ct ) imaging dates back to studies published in the late 1970s [ 26 ]  . in the initial studies that investigated contrast material uptake by ischemically damaged and normal myocardium , iodinated contrast media and ct of extirpated canine hearts with acute and chronic myocardial infarctions were used . 
 delayed scans obtained within minutes of contrast material administration revealed iodine concentrations of infarcted tissue several times greater than that of normal myocardium , irrespective of the injected contrast material ( meglumine / sodium diatrizoate , iodipamide , and an experimental polymer of iothalamic acid )  . 
 the enhancement of acute infarctions was later shown in the in situ beating heart using a prototype electrocardiography ( retrospective ) - gated ct scanner in the early 1980s [ 2636 ]  . great advances have been made in postmortem imaging during the last decade and postmortem cta has become a field of intense research . 
 they have all been demonstrated to significantly increase the quality of postmortem investigations , especially with regard to vascular system injury and disease [ 10 , 37 ]  . specifically , concerning the differential enhancement / accumulation of contrast material in ischemically damaged and normal myocardium , recent reports have indicated that mpmcta ( using the standardized protocol in three phases and a lipophilic contrast agent mixture ) would allow infarcted regions of the myocardium to be identified as areas characterized by pathological enhancement . 
this would likely be due to an abnormal leak in the infarcted myocardiuin comparison , normal myocardium does not reveal any contrast material accumulation [ 1013 ]  . as cardiac myocytes become necrotic , intracellular proteins [ myoglobin , lactate dehydrogenase , mb fraction of creatine kinase ( ck - mb ) , troponins ] leak into the interstitial space and enter the systemic circulation via local microvascular and lymphatic drainage . 
the concentrationtime profile for these markers in peripheral blood depends on their molecular weight , and location within the myocytes as well as their rates of vascular or lymphatic drainage and systemic clearance . 
small cytosolic proteins , such as myoglobin , are detectable within 12 h after tissue injury , whereas large enzymes such as lactate dehydrogenase diffuse much more slowly [ 38 ]  . troponin complex is a component of skeletal and cardiac muscle thin filaments . 
it consists of three subunits : the calcium binding sub - unit , troponin c ( tnc ) ; the inhibitory sub - unit , troponin i ( tni ) ; and an elongated sub - unit , troponin t ( tnt ) , that binds both tnc and tni , anchoring the entire complex to tropomyosin [ 39 ]  . troponins play a crucial role in muscle activity , connecting changes in intracellular ca2 + concentrations with contraction generation . 
 in humans : fast and slow skeletal isoforms and specific cardiac isofor tnt is expressed in humans by three genes coding slow and fast skeletal and cardiac isoforms of the protetnc is expressed in humans by two genes : one located on chromosome 3 that codes the cardiac / slow skeletal isoform of tnc and one located on chromosome 20 that codes the fast skeletal isoform of tnc . 
in an adult human heart muscle , the 35.9 - kda isoform tnt3 is predominantly expressed [ 40 ]  . 1 3 radiol med ( 2017 ) 122 : 95105 cardiac troponin c ( ctnc ) contains two high affinity calcium binding sites that are always occupied by ca2 or mg2 + under physiologic conditions , stabilizing an open conformation that remains anchored to the rest of the troponin complex . 
during muscle activation , calcium binding to ctnc favors an open conformation that binds to the switch region of ctni , removing adjacent inhibitory regions of tni from actin and allowing muscle contraction to proceed . 
it inhibits actomyosin interactions at diastolic levels of intracellular ca2 + [ 39 , 40 ]  . cardiac troponins are coded by specific genes and theoretically have the potential of being unique to the myocardiuindeed , cardiac troponin i ( ctni ) has not been identified outside the myocardiucardiac troponin t ( ctnt ) is expressed to a small extent in skeletal muscle ; however , current ctnt assay does not identify skeletal troponins . 
their concentrations remain raised for four times longer than ck - mb concentrations because of the sustained release of structurally bound protein from disintegrating myofibrils [ 3843 ]  . ctn - t and ctn - i are measured in routine clinical investigations of myocardial damage , mainly for the diagnosis and management of myocardial infarction . 
hence , differences in clinical findings should be carefully considered when evaluating postmortem data and clinical reference values should not be directly used in interpreting results obtained from postmortem serum samples . 
these limits notwithstanding , femoral blood postmortem serum troponin levels have been shown to be reliable in investigating the severity of myocardial damage and correlate with the ischemic myocardial damage severity [ 4 , 9 , 4448 ]  . the results of the study presented herein support the hypothesis that pathological enhancement of the myocardium at mpmcta ( mean hounsfield units 95 ) combined with further postmortem analysis results , such as troponin i and t determination , may be useful in the investigation of myocardial ischemia and myocardial infarction . this is the first study , to the best of our knowledge , to assess the radiological profile of myocardial ischemia combined with further postmortem investigation results ( with specific regard to cardiac troponins ) in a series of cases that had undergone forensic investigations , including postmortem angiography , histology , and biochemistry . 
all patients underwent conventional mri and diffusion - weighted imaging ( dwi ) at baseline and 1 , 3 , 6 , and 18 months after the beginning of therapy . 
tumor volumes and mean adc measurements of the five examination series were compared ; correlation of adc values and tumor regression was estimated . * pietro valerio foti pietrofoti@hotmail.com 1 radiodiagnostic and radiotherapy unit , university hospital policlinico - vittorio emanuele , via santa sofia 78 , 95123 catania , italy 2 department of ophthalmology , university of catania , catania , italy 3 department g.f. 
ingrassia , institute of pathology , university of catania , catania , italy 4 unit di biomedicina molecolare genomica e dei sistemi complessi , genetica , biologia computazionale , department g.f. 
ingrassia , university of catania , catania , italy 5 dipartimento di oftalmologia , universit politecnica delle marche , ancona , italy results mean adc values of ocular melanomas significantly increased already 1 month after therapy whereas tumor volume significantly decreased only 6 months after therapy . 
pretreatment adc value of ocular melanomas and early change in adc value 1 month after therapy significantly correlated with tumor regression . conclusions in ocular melanoma treated with pbt , adc variations precede volume changes . 
both pretreatment adc and early change in adc value may predict treatment response , thus expanding the role of dwi from diagnostic to prognostic . keywords magnetic resonance imaging diffusionweighted imaging uveal melanoma proton therapy treatment response orbit introduction uveal melanoma is the most frequent malignant intraocular tumor with an incidence of 68 per million per year in western europe [ 1 ]  . 
the majority ( 80 % ) of the ocular melanomas originate in the uvea , anatomically consisting of the choroid posteriorly and ciliary body / iris anteriorly , whereas the remainder arise in non - uveal sites , including the conjunctiva [ 2 ]  . the risk factors predicting metastatic disease are large tumor size , tumor thickness , extraocular tumor extension , and secondary glaucoma ( for iris melanomas ) [ 3 ]  . common clinical features of uveal melanoma include blurred vision , visual field defect , decreased visual acuity , floaters , pain , and increased intraocular pressure [ 4 ]  . 
the diagnosis is usually done on fundoscopic examination and ultrasound ( us ) , whereas cross - sectional imaging is necessary in case of opaque lens or significant subretinal effusion [ 5 ]  . 1 3 132 radiol med ( 2017 ) 122 : 131139 the earliest treatment for uveal melanoma was removal of the eye ; in recent years , enucleation has been largely replaced by various forms of radiation therapy ( episcleral brachytherapy , proton - beam radiotherapy , and stereotactic radiotherapy ) having the purpose to achieve local tumor control , conserving the eye and useful vision [ 6 ]  . proton - beam radiotherapy ( pbt ) is available at a few centers ; among the different globe - sparing radiotherapic approaches , it has the widest inclusion criteria . 
owing to their physical properties ( finite range in tissue , sharp lateral penumbra ) [ 7 ] , proton beams make it possible to deliver high doses of radiation to the tumor with relative sparing of adjacent tissues ; the possibility to highly collimate the beam allows to reduce collateral damage to adjacent structures such as the optic nerve and fovea . 
moreover , pbt requires little or no ( in case of iris melanoma ) surgical procedures . although pbt is a safe and effective modality to treat uveal melanoma , with low toxicity and enucleation rates [ 8 ] , however , due to tumors heterogeneous biological behavior and radiotherapy - related complications , additional noninvasive imaging markers that may predict outcome are needed [ 9 ]  . the gold standard for local tumor follow - up is us based on the international collaborative ocular melanoma study ( coms ) criteria , to define tumor relapse and advocate treatment . 
us is useful at baseline and for monitoring the size of a melanoma after irradiation [ 10 , 11 ] ; nevertheless , therapy - induced changes in tumor volume may occur relatively late in the time course of treatment [ 12 ] , therefore assessment of tumor treatment response based on morphological evaluation ( changes in tumor size ) is a late index . cross - sectional imaging modalities such as magnetic resonance imaging ( mri ) can be used to assess the extent of ocular melanoma , to evaluate optic nerve involvement , to visualize possible extraocular spread ( which can change the tumors management ) and to plan proton - beam therapy . in the last years , diffusion - weighted mr imaging ( dwi ) with apparent diffusion coefficient ( adc ) , the quantitative parameter of dwi , has been proposed as the technique of choice for detection of early response to treatment in brain tumors and head and neck cancers [ 1315 ]  . 
this ability of adc measurements to predict response might provide for the opportunity to individualize therapy , thus enabling early termination of treatment in nonresponding patients , preventing additional toxicity , and allowing for early changes in treatment [ 16 ]  . the purpose of this prospective study was to investigate the proton - beam - induced changes in adc values of ocular melanoma treated with pbt in patients undergoing long - term mri follow - up and to assess whether variations in adc constitute a reliable biomarker for predicting and detecting the response of ocular melanoma to pbt . materials and methods patients this study was a single - institution prospective , consecutive case series . 
the work described has been carried out in accordance with the code of ethics of the world medical association ( declaration of helsinki ) for experiments involving humans and in accordance with recommendations of the local ethic committee ; informed consent has been obtained from patients . between may 2012 and february 2015 , 20 patients with diagnosis of ocular melanoma were considered for eligibility . 
all patients were examined by an ophthalmologist specialized on ocular tumors , and the final clinical diagnosis of ocular melanoma was made on the basis of fundoscopic and ultrasonographic findings before the mri examination . 
however , contrary to all other malignant tumors , a biopsy is not required to make a diagnosis of uveal melanoma [ 10 ] ; ophthalmoscopy is the criterion standard for diagnosing ocular melanoma with a diagnostic accuracy as high as 99.7 % [ 17 ]  . inclusion criteria were as follows : posterior tumor margin extending close to optic disk so that plaque radiotherapy could not be administered reliably without causing optic neuropathy ; tumor extending close to fovea so that there was a better chance of conserving central vision with proton - beam radiotherapy than with other methods ; tumor height exceeding 5.5 mm ; inappropriateness of other forms of conservative treatment . exclusion criteria were : tumor previously treated by other methods ; bilateral tumor ; contraindications to mr imaging examination ; insufficient mr imaging quality ( e.g. , owing to movement artifacts ) ; discontinued mr imaging examinations during therapy ; presence of distant metastases . patients underwent serial mr imaging examination ( five examinations per patient : one baseline examination and four follow - up examinations : 1 , 3 , 6 , and 18 months after the beginning of the therapy , respectively )  . 
insertion of tantalum markers was carried out as previously described [ 18 ]  . to exclude distant metastases , all patients underwent also multidetector computed tomography ( mdct ) examinations of chest , abdomen , and pelvis before the beginning of the therapy and during the follow - up period . 1 3 radiol med ( 2017 ) 122 : 131139 fig . 
organs at risk are listed as follow : on ( optic nerve ) , f ( fovea ) , l ( cornea - limbus ) protonbeam therapy protocol treatment was delivered at catana proton therapy facility [ istituto nazionale di fisica nucleare - laboratori nazionali del sud ( infn - lns ) ] , where a 62 - mev proton beam , produced by a superconducting cyclotron ( sc ) , has been used for the treatment of shallow tumors , such as those of the ocular region [ 19 ]  . all patients received a total dose of 60 gy ( relative biological effectiveness , rbe ) , delivered in four consecutive fractions of 15 gy ( rbe ) on four consecutive days , using a constant rbe of 1.1 over the modulated bragg peak . eyeplan software , developed at the massachusetts general hospital for eye tumor therapy using proton beams , was used for treatment planning [ 20 ]  . patients were treated in seated position , with individualized immobilization devices , such as thermoplastic mask and byte - block ; the eyelids were fixed with an adhesive plaster , to reduce eye movements . 
patients were invited to fix a light point , the position of which in space was defined at the time of treatment planning . the optimal fixation point in space was defined with the aim of irradiating the target volume while saving the surrounding healthy organs ( optic disk , fovea and anterior segment structures , lens , and ciliary body , when possible )  . 
all mr examinations included a standard brain study too . image analysis for image analysis , data were transferred to a ge workstation with advanced imaging analysis software . the images of ocular mr examinations were evaluated by two radiologists in consensus ( a neuroradiologist with 10 years of clinical experience and a neuroradiology fellow with 4 years of practice experience )  . 
it was documented whether the ocular tumor touched the lens , the iris , or the ciliary body , and whether there was retinal detachment or extraocular spread . tumor - volume measurements were performed , as previously described [ 18 , 21 ] , on contrast - enhanced axial t1 - weighted images with the use of a computerized imageanalysis tool , available as part of our hospitals picture archiving and communication system ( pacs )  . 
the volumes from the first and fifth scans for each patient were used to calculate percentage variation of tumor volume after 18 months of therapy ( tumor percentage regression )  . in all the five time point examinations , the quantitative adc measurements were performed as previously described [ 18 , 2123 ] , using a dedicated workstation with diffusion analysis software ( advantage windows version 4.6 , software functool , general electric medical systems , milwaukee , wi , usa )  . 
of averages section thickness ( mm ) interslice gap ( mm ) field of view ( mm ) matrix frequency direction b - value ( sec / mm2 ) 160 160 256 256 160 160 256 224 160 160 256 256 right to left anterior to posterior right to left 200 200 192 192 right to left 0100 synoptic table summarizes the imaging parameters of mr sequences . 
t1 - weighted fse spectral presaturation sequences were performed before and after intravenous administration of 0.2 ml gadoteric acid ( gadoterate dimeglumine , dotarem , 0.5 mol / l ; guerbet , roissy , charles - de - gaulle cedex ; france ) per kilogram of body weight . 
therefore , the final study population consisted of 17 eyes of 17 patients ( 11 women and 7 men ; mean age [ sd ] , 45 years [ 5 , 12 ] ; range , 3056 years )  . the right eye was affected in 10 patients ( 59 % ) and the left eye in 7 ( 41 % ) patients . 
no tumors extrascleral spread was found at mr examination . no distant metastases were found at mdct examinations of chest , abdomen , and pelvis neither before the beginning of the therapy , nor during the follow - up period . mean volume changes at baseline examination , mean volume ( sd ) of ocular melanoma was 382 mm3 ( 291 ) , ( range 761120 mm3 )  . 
five year local control rates exceeded 90 % , 5 - year overall survival rates ranged from 70 to 85 % , 5 year metastasis - free survival and disease - specific survival rates from 75 to 90 % , 5 year enucleation rates from 7 to 25 % . 
complication rates vary : glaucoma ( 730 % ) , cataract ( 2062 % ) , vitreous bleeding ( 914 % ) , any type of retinopathy ( 2367 % ) , and optic neuropathy ( 733 % ) [ 8 ]  . it is likely that inherent tumor characteristics may play a role in visual prognosis , since the most common reported predictors of ocular complications following radiotherapy are tumor distance from the optic nerve , tumor thickness , and radiation dose [ 24 ]  . although pbt of uveal melanoma achieves high rates of local tumor control and in the last decade both surgical and medical methods have been developed to treat radiation complications thus improving the toxicity profile of pbt , the biological behavior of the tumor still remains heterogeneous and tumor response to therapy may vary in the same case series . in this setting , it is desirable to rely on early noninvasive markers that correlate with long - term outcome metrics and may predict treatment response . our study revealed the potential of dwi in the detection of early tumor response and its capability to predict treatment outcome in ocular melanoma patients treated with pbt . 
the purpose of this prospective study was to investigate the proton - beam - induced changes in adc values of ocular melanoma treated with pbt in patients undergoing long - term mri follow - up and to assess whether variations in adc constitute a reliable biomarker for predicting and detecting the response of ocular melanoma to pbt . the patients of our series underwent a follow - up of 18 months . 
all except two patients showed the maximum decrease in tumor volume between 3 and 6 months after pbt ; in the remaining two patients the maximum decrease in tumor volume was observed even between 6 and 18 months . 
it is therefore likely that in this time interval ( 318 months ) the effect of therapy on tumor volume is more noticeable , suggesting that changes in tumor volume occur more slowly after pbt than after other types of radiation therapy . 
actually this result confirms previous observation that tumor regression is less rapid after proton - beam treatment than after ruthenium - 106 plaque radiotherapy , probably because of the very high doses of radiation delivered to the tumor base during brachytherapy [ 6 ]  . conversely to the relatively slow changes in tumor volume , adc value modifications after pbt seem to occur more rapidly . in our case series , after pbt , a decrease in tumor volume and a corresponding increase in adc was observed in all the four follow - up time points . 
however , whereas adc values of ocular melanoma significantly increased already 1 month after therapy , tumor volume significantly decreased 6 months after therapy only . significant change of mean adc value occurred in advance of corresponding change in tumor volume , thus indicating that dwi may detect macromolecular and microstructural changes in tissue architecture at the cellular level and is not dependent on relatively slow changes in tumor size . 
therefore , in monitoring tumor response during 1 3 136 radiol med ( 2017 ) 122 : 131139 1 3 radiol med ( 2017 ) 122 : 131139 10 fig . 
2 axial mri images in a 49year - old woman with ocular melanoma of the right eye , who exhibited good response to treatment ( ad before therapy ; eh 1 month after therapy ; il 3 months after therapy ; mp 6 months after therapy ; qt 18 months after therapy ) ( a , e , i , m , q t2 - weighted turbo spin - echo stir images ; b , f , j , n , r postcontrast t1 - weighted spin - echo spectral presaturation images ; c , g , k , o , s diffusion - weighted images ; d , h , l , p , t adc map )  . 
tumor percentage regression was 52 % 10 10 10 10 therapy , dwi may provide earlier indications of therapeutic outcome than changes of tumor volume can do . this result is consistent with previous researchs findings . 
in this previous article , the pretreatment adc value significantly correlated with tumor regression and during the follow - up period the adc values of ocular melanomas significantly increased in advance of the corresponding significant decrease of tumor volume . in ocular melanoma , tumor regression depends on the type of radiotherapy and the cell - doubling time . 
cells can be damaged by ionizing radiation directly or indirectly through the formation of toxic - free radicals ; irradiated cells undergo apoptosis and necrosis , resulting in tumor shrinkage , ischaemia , infarction , and fibrosis [ 6 ]  . 
 [ 29 ] , using an animal tumor model , demonstrated that induction of necrosis with associated apoptotic cell death by cytotoxic treatment causes an increase in tumor adc detectable prior to changes in tumor volume ; on the other hand , apoptosis alone is not sufficient to induce measurable changes in adc . currently , the availability of quantitative measures ( such as adc ) acquired periodically is key in the management of oncologic patients , to monitor the effectiveness of therapies . from this point of view , dwi is preferable to other methods since it is noninvasive , time - sparing , easy to perform , and radiation - free , thus allowing close follow - up during cancer treatment . 
the authors found high - resolution t1and t2 - weighted images at 3 t to be superior to those at 1.5 t in visualization of the anatomic details of the orbit . 
image quality may be improved by adopting some technical expedients such as the application of short echo time , multichannel coil , and parallel imaging that will increase imaging contrast and decrease susceptibility artifacts [ 31 ]  . in our mr protocol , we used an epi sequence for dw imaging . 
epi - dwi suffers from geometrical distortions due to susceptibility artifacts , especially in regions with air - tissue transitions such as in the head and neck area [ 32 ] and particularly in the orbit . 
 [ 32 ] compared haste - dwi with epi - dwi early during crt for their potential to predict locoregional outcome in patients with head and neck squamous cell carcinoma . 
the authors demonstrated that , although haste - dwi has a lower incidence of geometric distortions , it seems to be inadequate in early response prediction , compared to epi - dwi which has greater potential to predict locoregional outcome after chemoradiotherapy . our study has some limitations : the main one is the small number of patients . 
second , in our study the final diagnosis of ocular melanoma was based upon fundoscopic and ultrasonographic findings without histological evidence , hence to perform a correlation between histological features and adc values of the tumor was not possible . conclusions our study demonstrated that in patients with ocular melanoma treated with pbt , undergoing 18 months followup , the major effects of therapy on tumor volume occur between 3 and 18 months . 
in any case , adc variations precede volume changes , thus making dwi useful in determining early treatment response or failure . the significant correlation we observed between pretreatment adc value and tumor regression and between early change in adc value and tumor regression once again confirms the potential of adc to predict treatment response , thus expanding the role of dwi in uveal melanoma from diagnostic to prognostic . the object of future larger clinical studies or systematic review and meta - analysis could be to determine a threshold of pretreatment adc value or early change in adc value for prediction of tumor response , to provide a scientific evidence in this field . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . 
joseph schoepf1 , 4 received : 5 august 2016 / accepted : 31 october 2016 / published online : 14 november 2016 italian society of medical radiology 2016 abstract objective to evaluate the correlation between aortic root calcification ( arc ) markers and coronary artery calcification ( cac ) derived from coronary artery calcium scoring ( cacs ) and their ability to predict obstructive coronary artery disease ( cad )  . methods we retrospectively analyzed 189 patients ( 47% 11.1 years ) with an intermediate probabilmale , age 60.3 ity of cad who underwent clinically indicated cacs and coronary ct angiography ( ccta )  . 
arc markers [ aortic root calcium score ( arcs ) and volume ( arcv ) ] were calculated and compared to cac markers : coronary artery calcium score ( cacs ) , volume ( cacv ) , and mass ( cacm )  . 
 recently , a significant amount of evidence has highlighted the prognostic value of coronary artery calcium and its importance as an independent marker of obstructive coronary artery disease ( cad ) and cardiac risk stratification for assessing mortality and morbidity in patients with atherosclerosis [ 24 ]  . recent studies have shown that calcification of the aortic and mitral valve , aortic arch , and thoracic aorta shares risk factors with cad , and is strongly associated with increased cardiovascular risk and coronary plaque burden [ 58 ]  . 
for patients undergoing transcatheter aortic valve replacement , ct imaging of the aortic root is used for preoperative procedural planning [ 911 ]  . few studies have specifically evaluated the role of aortic root calcification ( arc ) as a predictor of cac and obstructive cad . 
previous studies evaluating the association between aortic calcification , cac , and cad also included mitral annular or mitral valve calcification , aortic valve calcification , or patients with known cad [ 12 , 13 ]  . 
the relationship between arc markers quantified as calcium and volume score , and cac assessed with calcium , volume , and mass scores has not been evaluated in a population with an intermediate pre - test probability for cad . 
furthermore , the ability of arc markers to predict obstructive cad has not been sufficiently investigated to date . thus , we sought to evaluate the association between arc markers and the presence of cac and to investigate their discriminatory power for predicting obstructive cad as defined by coronary ct angiography . radiol med ( 2017 ) 122 : 113120 materials and methods study population the research study protocols were approved by the institutional review board with a waiver of informed consent due to the retrospective nature of this investigation . 
the study was performed in compliance with hipaa practices . we retrospectively analyzed data of patients with intermediate pre - test probability of cad who underwent clinically indicated non - enhanced coronary calcium scans and ccta assessing the possibility of cad between june 2012 and may 2014 . 
 patients were excluded if they had a history of known cad , heart , or valve surgery ( valve replacement / repair , coronary artery bypass grafting , or aortic surgery ) , aortic disease , or cardiac valve disease , including valve calcification . 
covariates and patient baseline characteristics were obtained from medical records . ct acquisition parameters all ccta examinations were performed using either a firstor second - generation dual - source ct ( dsct ) system ( somatom definition or somatom definition flash , siemens healthcare , forchheim , germany )  . 
for the subsequent contrast - enhanced ccta , scan parameters were as follows : a retrospectively ecg - gated protocol for the 1st generation dsct scanner and a prospectively ecg - triggered sequential scan protocol with a padding window for the 2nd generation dsct scanner ; tube voltage of 100120 kv , tube current of 320412 ma , temporal resolution of 83 or 75 ms , and 2 0.6 mm collimation with 64 z - flying focal spot . 
contrast enhancement was achieved by injecting 5080 ml of iopromide ( ultravist 370 mg i / ml , bayer , wayne , nj ) at 46 ml / s followed by a 30 ml saline bolus chaser . 
the extent of cac was quantified semi - automatically on non - contrast scans with the following markers : calcium mass ( cacm ) , volume ( cacv ) , and calcium score ( cacs )  . 
calcium scores according to the agatston method were used to grade cac : moderate ( 100400 ) , or 4 minimal ( 010 ) , 2 severe ( > 400 ) [ 14 ]  . mild ( 10100 ) , 3 analysis of arc markers arc evaluation was performed with the same software and acquisition protocol used for the cac analysis . 
the degree of arc was graded according to the cac measurement . all examinations were evaluated independently by two observers , each with more than 3 years of experience in cardiovascular imaging . 
1 66 - year - old male showing severe calcification of the aortic root ( a b ) , left anterior descending artery ( a ) , and right coronary artery ( b ) on non - contrast coronary calcium scoring images , resulting in an arcv of 1011 mm3 and arcs of 1139 . 
2 74 - year - old female with severe calcification of the aortic root ( a ) and left anterior descending artery ( b ) is shown yielding an arcv of 822 mm3 , arcs of 1014 , and coronary agatston score of 2011 . 
these results are in accordance with previous studies , including ccta and x - ray examinations , which showed a significant association between different aortic calcification markers , cac , and cad [ 8 , 18 , 19 ]  . in reference to the association between arc and cac , our study displayed a significant correlation between the arc markers and the cac - related markers : cacs , cacv , and cacm . 
the validity of arcs and arcv measurements compared to cacs has been previously evaluated , and our results further confirm the conclusions and the prognostic value of these markers [ 18 , 19 ]  . 
this ultimately demonstrates that age is an independent marker for the prevalence of ascending aorta calcification in both men and women aged 5060 years , with a growing probability for patients older than 70 years [ 7 , 13 ]  . 
alternatively , cacv and cacm did not show significant correlation to detect arc . previous studies showed significantly greater coronary calcification for men compared to women in correlation with ascending aorta calcifications [ 21 , 22 ]  . 
in addition , recent results derived from the mesa study ( multi - ethnic study of atherosclerosis ) determined that age , male sex , and aortic calcification were strong predictors for cac [ 5 , 23 , 24 ]  . 
thus , the focus of this study supports these previous findings by demonstrating that age , male sex , as well as both markers of arc are independent markers for cac . 
therefore , the sensitivity and specificity for arcs and arcv to detect obstructive cad were 61 and 78% , and 62 and 80% , respectively . discussion our results demonstrate a significant correlation between the presence of arc and cac . 
more importantly , arcs ( auc 0.67 , p < 0.0001 ) and arcv ( auc 0.68 , p < 0.0001 ) revealed significant discriminatory power and emerged as predictors for obstructive cad , ultimately providing incremental diagnostic value . 
furthermore , we did not compare our results to the golden standard of invasive catheter angiography to confirm the severity of cad . in conclusion , this study demonstrates that arc markers are strongly associated with and independently predict the presence of cac and obstructive cad . 
additionally , further testing is required in patients with severe arc and significant cad in order to reliably obtain these markers from thoracic - ct or x - ray for proper risk classification . compliance with ethical standards conflict of interest schoepf receives research support from astellas , bayer , bracco , ge , medrad , and siemens . 
all other authors have no conflicts of interest to disclose . christian tesche is an exchange visiting scholar supported by a grant from the fulbright visiting scholar program of the u.s. 
km , merkez , malatya 44000 , turkey 2 department of cardiology , inonu university school of medicine , inn niversitesi turgut zal tp merkezi kardiyoloji ana bilimdali , elaz yolu 15 . 
km , merkez , malatya 44000 , turkey 3 department of biostatistics , inonu university school of medicine , inn niversitesi turgut zal tp merkezi biyoistatistik ana bilimdali , elaz yolu 15 . 
no significant correlations were observed between functional analysis measurements and native t1 or ecv values . conclusions our results showed that myocardial fibrosis is unrelated to cardiac functional findings in nidcm patients . 
 therefore , we propose that these patients should be evaluated using mri and tissue characterization techniques , in addition to cardiac functional analysis . keywords cardiac magnetic resonance imaging t1 mapping extracellular volume fraction nonischemic dilated cardiomyopathy myocardial fibrosis left ventricular ejection fraction introduction non - ischemic dilated cardiomyopathy ( nidcm ) can cause heart failure and sudden cardiac death ( scd ) and is clinically defined as left ventricular ( lv ) or biventricular enlargement with decreased systolic function [ 13 ]  . 
this clinical entity is responsible for a significant proportion of newly diagnosed heart failure cases and is the most frequent reason for heart transplantation in adults and children [ 1 3 ]  . 
moreover , although a reduced left ventricular ejection fraction ( lvef ) is a criterion for inserting an implantable cardioverter - defibrillator ( icd ) to prevent scd [ 79 ] , icd candidates should not be 1 3 radiol med ( 2017 ) 122 : 106112 chosen solely on the basis of lvef [ 6 ]  . 
myocardial fibrosis ( mf ) has been sufficiently defined as the main cause of arrhythmogenesis , which is a strong indicator of undesirable cardiac outcomes [ 5 , 6 , 10 , 11 ]  . 
 therefore , assessment of mf has become important for the follow - up and recovery of patients with nidcm . cardiac magnetic resonance ( cmr ) imaging is a powerful visualization method that provides the unique capability to not only detect the presence and position of mf but also quantitatively characterize examined tissue [ 1622 ]  . 
 in contrast , although late gadolinium enhancement ( lge ) imaging can successfully identify localized myocardial scar tissue , diffuse fibrosis may be overlooked , and quantitative assessment is not possible [ 23 , 24 ]  . 
the native t1 mapping technique of cmr imaging , which does not require gadolinium enhancement , permits the detection of overall changes in myocardial tissue , such as fibrosis , edema , and the deposition of iron , lipids or proteins , that predict myocardial pathologies involving myocytes and interstitial spaces [ 2628 ]  . 
furthermore , the extracellular volume fraction ( ecv ) technique of cmr imaging is a novel method that can differentiate the cellular and interstitial parts of the myocardium by measuring the extent of the extracellular space after administration of a contrast agent , thereby delineating mf . 
 the findings of our study could lead to further studies of the follow - up protocols . methods study population based on clinical and echocardiographic findings , 53 patients with dilated cardiomyopathy ( dcm ) who underwent cmr imaging in our radiology department were retrospectively evaluated for nidcm between march 2015 and february 2016 . 
patients were excluded if they exhibited the presence of ischemic dcm , an lvef value > 45% , a focal myocardial scar that was apparent via lge imaging , and / or myocardial edema that could be observed via t2 mapping . scanning protocol cardiac magnetic resonance imaging examinations were performed with a 3.0 t clinical scanner ( magnetom skyra , version e11 , siemens healthcare , erlangen , germany ) with an 18 - channel cardiac coil and electrocardiography gating . 
for functional evaluation of the lv and assessment of the heart chambers , steady - state free - precession cine images in the short axis - view and 3 long - axis views ( 2 , 3 , and 4 - chamber views ) were obtained using the following parameters : tr , 41 ms ; te , 1.2 ms ; flip angle , 47 . 
in all patients , the native and post - contrast t1 mapping data were acquired in a single mid - ventricular short - axis slice using the modified look - locker inversion recovery ( molli ) sequence . 
t2 mapping was obtained in the same mid - ventricular short - axis level used for t1 mapping with the following imaging parameters : tr , 207.4 ms ; te , 1.32 ms ; flip angle , 12 . 
lge images were acquired 15 min after administration of a dose of 0.2 mmol / kg gadolinium using a phase - sensitive inversion recovery sequence ( tr , 775 ms ; te , 2.67 ms ; flip angle , 25 )  . 
the imaging procedure was concluded with post - contrast t1 mapping using the following parameters : tr , 361.6 ms ; te , 1.12 ms ; flip angle , 35 . 
the scanning time for the entire cmr protocol with the t1 mapping technique was approximately 40 min for each patient . image analysis the acquired cmr images were analyzed on a syngo via workstation ( software version va30a , siemens ag , germany ) by the same radiologist ( cag ) who had 3 years of experience in cardiac imaging and was blinded to the patient age , patient gender , and echocardiographic results . 
using the delineated endocardial and epicardial contours , the lvef , left ventricular 1 3 108 radiol med ( 2017 ) 122 : 106112 statistical analysis the data were summarized as means standard deviations ( sds ) and as frequencies with percentages . 
intra - observer intraclass correlation coefficients ( iccs ) were calculated to identify repeatability in the quantitative analyses , and the 95% confidence intervals ( cis ) were also computed . 
1 representative images of a native and b post - contrast t1 maps end - diastolic volume ( lv - edv ) , and left ventricular endsystolic volume ( lv - esv ) were measured and normalized to the body surface area ( bsa )  . focal scar tissue was identified by myocardial lge imaging and qualitatively characterized by myocardial post - contrast signal intensity . 
preand post - contrast pixelwise t1 relaxation times were measured by manual region of interest ( roi ) tracing to detect the lv myocardial circumference at the mid - ventricular level in short - axis images . 
in addition , because no proven treatment option exists for decreasing the mortality or the hospitalization time for nidcm patients who have sufficient lvef [ 29 , 30 ] , the identification of mf has become important . 
further investigations are needed to determine the cut - off values for ecv and t1 mapping to prevent scd , arrhythmogenesis , and heart failure . there are several limitations to our study . 
therefore , we concluded that these data were reliable and reproducible . discussion in this study , to obtain a homogeneous cohort of nidcm patients , we excluded patients who had edema on t2 mapping or positive lge imaging findings . 
first , we showed that the mean native t1 mapping values and ecv measurements in nidcm patients could be obtained using 3.0 t magnetic resonance imaging ( mri ) ; a limited number of previous studies in this area have been reported in the literature . 
 more importantly , our study demonstrated that no significant correlations existed between metrics measuring lv function ( lvef , lv - edv , and lv - esv ) and myocardial 1 3 110 radiol med ( 2017 ) 122 : 106112 largest group of nidcm patients assessed using the ecv technique , our study cohort was relatively small . 
however , a previous study of the detection of mf using cmr imaging showed that ecv images were closely correlated with fibrosis that had been histologically verified [ 43 ]  . in conclusion , the evaluation of cardiac function alone is inadequate for prognostic stratification . 
further research is needed to confirm our findings and evaluate mf in nidcm patients . compliance with ethical standards conflict of interest all authors declare that they have no conflicts of interest . ethical approval this study was performed at a single tertiary center and was approved by the local medical ethics committee . informed consent informed consent was obtained from each participant included in this study . radiol med ( 2017 ) 122 : 146153 doi 10.1007 / s11547 - 016 - 0700 - z radiotherapy threedimensional conformal versus intensity modulated radiotherapy in breast cancer treatment : is necessary a medical reversal ? alba fiorentino1 ruggero ruggieri1 niccol giajlevra1 gianluisa sicignano1 gioacchino di paola2 stefania naccarato1 sergio fersino1 rosario mazzola1 umberto tebano1 , 3 francesco ricchetti1 filippo alongi1 received : 13 september 2016 / accepted : 10 october 2016 / published online : 24 october 2016 italian society of medical radiology 2016 abstract objectives aim of the present study is to compare threedimensional conformal rt ( 3d - crt ) and 4 - fields intensity modulated radiation therapy ( 4f - imrt ) treatment plans , in terms of target dose coverage , integral dose and dose to organs at risk ( oars ) in early breast cancer ( bc )  . methods twenty consecutive bc patients , after lumpectomy , were selected for the present analysis . 
a total dose of 50 gy and a simultaneous dose of 60 gy in 25 fractions was prescribed to planning target volume of the whole breast ( ptvbreast ) and of the surgical bed , respectively . 
 standard whole breast irradiation consists of 4550 gy delivered at 1.82.0 gy / fraction over 4.55 weeks followed by an overdosage irradiation ( boost ) to surgical bed ( 1016 gy / 11.5 weeks ) , when indicated . 
however , to date , several adjuvant rt fractionations ( conventional versus hypo fractionation ) and techniques ( three - dimension conformal rt versus intensity modulated rt modalities , imrt ) and several boost approaches ( concomitant , sequential or simultaneous integrated boost ) are reported in literature , with an ott ranged from 3 to 6 weeks [ 24 ]  . concerning rt techniques , three - dimensional conformal rt ( 3d - crt ) with tangential fields is generally recommended . 
in fact , the american society of radiation oncology does not suggest the routinely use of imrt or volumetric modulated arc therapy ( vmat ) in bc irradiation because no significant clinical advantages , in terms of risk of recurrence or survival , have been demonstrated comparing to 3d - crt [ 2 ]  . 
nevertheless , some criticisms could affect the 3d - crt performances , including the lacking of conformal and steep dose gradient between breast 1 3 radiol med ( 2017 ) 122 : 146153 and boost volume , with subsequently excessive dose to whole breast . 
conversely , the major potential criticism concerning imrt / vmat could be represented by the higher low - dose exposure of the organs a risks ( oars ) , due to the higher number of fields and monitor units adopted [ 6 ]  . 
thus , the issue of the costs / benefit relationship of the introduction of imrt techniques remains to be defined mainly due to the lack of long - term data of imrt [ 3 , 711 ]  . aim of the present study was to compare in silico 3d - crt versus imrt in early stage bc , in terms of target dose coverage , integral dose and dose to oars . patients and methods twenty consecutive patients affected by early bc ( stages t1t2 and n0 ) after lumpectomy and candidate to whole breast rt plus boost were selected for the present planning study . 
eleven patients ( 55 % ) were affected by right bc , while nine patients ( 45 % ) by left bc . patients were immobilized in a supine position on posiboard frame ( civco inc . , orange city , ia )  . 
a 5 mm expansion in the transverse plane , and 8 mm in cranialcaudal direction was used to obtain a whole breast planning target volume ( ptvbreast )  . a ctvboost included the tumor bed , visible surgical clips and anatomical distortion . 
pre - operative imaging , operative report ( including the results of histopathology ) and the position of the surgical incision were reviewed to define the expected position of the surgical bed . 
 respiratory management techniques were not applied . the contraand ipsilateral lung , the contra - lateral breast gland , as well as heart were contoured as oars , according to rtog guidelines . 
a structure for the normal tissue ( nt ) was created : the patients body minus ptvbreast with an additional distance of 0.5 cto evaluate the homogeneity in the target dose , a structure of ptvbreast minus the ptvboost was created . for each patient both a 3d - crt plan with two couples of tangential fields , and a 4 - fields sliding - window imrt plan , at fixed 300 mu / min dose rate , were generated . 
from each one of the two 3d - crt tangential fields two imrt - fields were derived , the first one by increasing the tangentiality of the gantry angle by about 5 , and the second one by decreasing such same tangentiality by about 15 . 
in imrt plans , both ptvbreast and ptvboost were simultaneously optimized . all plans were computed by the eclipse ( v.11.0 , varian medical systems , palo alto , ca ) treatment planning system ( tps ) , with aaa ( v.10.0.28 ) dose calculation algorithm , to be performed on a trilogy ( varian medical systems , palo alto , ca ) linac by 6 mv photon beams . 
 for imrt plans , the dvo ( v.10.0.28 ) optimizer and the smart lmc ( v.10.0.28 ) leaf motion calculator were used . the patients were planned for free - breathing treatments . 
 having the imrt plans to be used for patients treatment , for these plans the fluence maps were expanded in air , with the so called skin - flash technique , by about 1 ca total dose of 60 gy in 25 fractions was prescribed to the ptvboost , while 50 gy in 25 fractions were prescribed to , here defined as ptvbreast minus ptvboost . 
consistently with icru recommendations , an homogeneous ptvboost dose coverage was pursued by assuring to such target volume v95 %dp 95 % ( dp being the prescribed dose ) , and a near - maximum target dose ( d2 % ) < 107 %dp . 
for ptv breast dose coverage v95 %dp 95 % was required also . breast for evaluation of the low - dose exposure to the oars , v5gy , v10gy and various organ specific vxgy values as well as the values of d2 % , d50 % , and dmean were analyzed . 
in particular , for categorical variables the distribution of absolute frequencies , percentages and cumulative has been reported , while for continuous variables mean , standard deviation , median , max , min and range were considered . 
imrt or vmat can improve the target dose coverage , delivering a higher low - dose exposure of oars , with the subsequently potential risk of rt - related malignancies [ 6 ]  . 
several analyses reported a reduction of acute skin toxicity with imrt , mainly represented by moist desquamation [ 3 , 5 , 7 ] , influencing late side effects , including cosmesis . 
thus , to overcome this hypothetical limitation of vmat approach , several authors proposed an hybrid technique , delivering the dose to whole gland by means of imrt - fields while the irradiation of surgical bed ( sib ) by vmat technique [ 16 , 17 ]  . jost and colleagues recently compared 20 treatment plans of 3d - crt with a hybrid technique on the basis of dvh parameters [ 16 ]  . 
the authors showed that the hybrid technique decreased in dose , mainly for the heart and lung dmean , with comparable ci and hi of the target volume in respect to 3d - crt [ 16 ]  . thus , based on this background , to overcome the potential disadvantage of using vmat for ptvboost , the present study was designed to compare a 4 - fields imrt with the standard of care ( 3d - crt ) in early stage bc , in terms of ptv coverage and dose to oars . to our knowledge , no other dosimetric analysis has been reported with 4 - fields imrt technique . 
in fact , 4 - fields imrt showed better hi and ci compared to 3d - crt ( p < 0.0001 ) , reducing the dose to ipsilateral and contralateral oars , including heart and nt . in terms of homogeneity , several previous published analyses showed a better hi with imrt , which reduce the risk of acute toxicities and improve overall cosmesis [ 18 , 19 ]  . 
even though larger ptvs have been associated with improvements using imrt when compared to 3dcrt [ 12 , 20 , 21 ] , in the present patient population , the advantage was reported for 4 - fields imrt in all cases . regarding oars findings , the dose to the heart is a critical issue in rt for bc patients : the radiobiology of rt heart damage has not been established and probably , the most important reason of myocardial rt - related degeneration is attributable to the capillary network damage [ 22 ]  . 
to date , it is not well recognized whether the cardiovascular effects are related to a high rt dose to a small volume or , on the contrary , to the low average dose to the whole heart [ 22 , 23 ]  . 
it is recognized that v25gy < 10 % is associated with a < 1 % probability of long - term cardiac mortality , while the clinical role of heart v5gy and v10gy has not been established [ 22 ]  . concerning the reduction in rt dose for heart during bc , similar results are reported using hybrid technique compared to 3d - crt [ 16 , 17 ]  . surely , the administration of boost increased the risk of heart dose exposure . 
however , the clinical relevance of these dosimetric results remains not clear and should be still under investigation . finally , imrt has been criticized for hypothetical role of low - dose exposure in rt - related carcinogenesis on surrounding healthy tissues [ 5 , 11 ]  . 
the hypothesis of rt - carcinogenesis derived from the atomic bomb survivors life span study and childhood cancer survivors study , reporting a second tumor probability of 7.9 % at 30 years from primary cancer which diminished by 17 % per - decade [ 26 , 27 ]  . 
however , to date , no clear evidences are still available in regards to imrt - related carcinogenesis , especially in the bc adjuvant setting [ 6 , 11 , 25 ]  . in the present analysis , all the conceived dose - volume parameters for the nt structure were in favor of 4 - fields imrt ( p < 0.0001 ) , except the v5gy , according to other experiences [ 12 , 16 ]  . 1 3 152 conclusion in the present analysis , 20 treatment plans of 3d - crt and 4 - fields imrt for early bc were compared . 
 * * * despite the several limitations of this study ( dosimetric analysis , limited sample size ) , 4 - fields imrt technique significantly reduced the dose to oars and nt , with a better target coverage compared to 3d - crt . 
joseph schoepf1 , 4 received : 5 august 2016 / accepted : 31 october 2016 / published online : 14 november 2016 italian society of medical radiology 2016 abstract objective to evaluate the correlation between aortic root calcification ( arc ) markers and coronary artery calcification ( cac ) derived from coronary artery calcium scoring ( cacs ) and their ability to predict obstructive coronary artery disease ( cad )  . methods we retrospectively analyzed 189 patients ( 47% 11.1 years ) with an intermediate probabilmale , age 60.3 ity of cad who underwent clinically indicated cacs and coronary ct angiography ( ccta )  . 
arc markers [ aortic root calcium score ( arcs ) and volume ( arcv ) ] were calculated and compared to cac markers : coronary artery calcium score ( cacs ) , volume ( cacv ) , and mass ( cacm )  . 
 recently , a significant amount of evidence has highlighted the prognostic value of coronary artery calcium and its importance as an independent marker of obstructive coronary artery disease ( cad ) and cardiac risk stratification for assessing mortality and morbidity in patients with atherosclerosis [ 24 ]  . recent studies have shown that calcification of the aortic and mitral valve , aortic arch , and thoracic aorta shares risk factors with cad , and is strongly associated with increased cardiovascular risk and coronary plaque burden [ 58 ]  . 
for patients undergoing transcatheter aortic valve replacement , ct imaging of the aortic root is used for preoperative procedural planning [ 911 ]  . few studies have specifically evaluated the role of aortic root calcification ( arc ) as a predictor of cac and obstructive cad . 
previous studies evaluating the association between aortic calcification , cac , and cad also included mitral annular or mitral valve calcification , aortic valve calcification , or patients with known cad [ 12 , 13 ]  . 
the relationship between arc markers quantified as calcium and volume score , and cac assessed with calcium , volume , and mass scores has not been evaluated in a population with an intermediate pre - test probability for cad . 
furthermore , the ability of arc markers to predict obstructive cad has not been sufficiently investigated to date . thus , we sought to evaluate the association between arc markers and the presence of cac and to investigate their discriminatory power for predicting obstructive cad as defined by coronary ct angiography . radiol med ( 2017 ) 122 : 113120 materials and methods study population the research study protocols were approved by the institutional review board with a waiver of informed consent due to the retrospective nature of this investigation . 
the study was performed in compliance with hipaa practices . we retrospectively analyzed data of patients with intermediate pre - test probability of cad who underwent clinically indicated non - enhanced coronary calcium scans and ccta assessing the possibility of cad between june 2012 and may 2014 . 
 patients were excluded if they had a history of known cad , heart , or valve surgery ( valve replacement / repair , coronary artery bypass grafting , or aortic surgery ) , aortic disease , or cardiac valve disease , including valve calcification . 
covariates and patient baseline characteristics were obtained from medical records . ct acquisition parameters all ccta examinations were performed using either a firstor second - generation dual - source ct ( dsct ) system ( somatom definition or somatom definition flash , siemens healthcare , forchheim , germany )  . 
for the subsequent contrast - enhanced ccta , scan parameters were as follows : a retrospectively ecg - gated protocol for the 1st generation dsct scanner and a prospectively ecg - triggered sequential scan protocol with a padding window for the 2nd generation dsct scanner ; tube voltage of 100120 kv , tube current of 320412 ma , temporal resolution of 83 or 75 ms , and 2 0.6 mm collimation with 64 z - flying focal spot . 
contrast enhancement was achieved by injecting 5080 ml of iopromide ( ultravist 370 mg i / ml , bayer , wayne , nj ) at 46 ml / s followed by a 30 ml saline bolus chaser . 
the extent of cac was quantified semi - automatically on non - contrast scans with the following markers : calcium mass ( cacm ) , volume ( cacv ) , and calcium score ( cacs )  . 
calcium scores according to the agatston method were used to grade cac : moderate ( 100400 ) , or 4 minimal ( 010 ) , 2 severe ( > 400 ) [ 14 ]  . mild ( 10100 ) , 3 analysis of arc markers arc evaluation was performed with the same software and acquisition protocol used for the cac analysis . 
the degree of arc was graded according to the cac measurement . all examinations were evaluated independently by two observers , each with more than 3 years of experience in cardiovascular imaging . 
1 66 - year - old male showing severe calcification of the aortic root ( a b ) , left anterior descending artery ( a ) , and right coronary artery ( b ) on non - contrast coronary calcium scoring images , resulting in an arcv of 1011 mm3 and arcs of 1139 . 
2 74 - year - old female with severe calcification of the aortic root ( a ) and left anterior descending artery ( b ) is shown yielding an arcv of 822 mm3 , arcs of 1014 , and coronary agatston score of 2011 . 
these results are in accordance with previous studies , including ccta and x - ray examinations , which showed a significant association between different aortic calcification markers , cac , and cad [ 8 , 18 , 19 ]  . in reference to the association between arc and cac , our study displayed a significant correlation between the arc markers and the cac - related markers : cacs , cacv , and cacm . 
the validity of arcs and arcv measurements compared to cacs has been previously evaluated , and our results further confirm the conclusions and the prognostic value of these markers [ 18 , 19 ]  . 
this ultimately demonstrates that age is an independent marker for the prevalence of ascending aorta calcification in both men and women aged 5060 years , with a growing probability for patients older than 70 years [ 7 , 13 ]  . 
alternatively , cacv and cacm did not show significant correlation to detect arc . previous studies showed significantly greater coronary calcification for men compared to women in correlation with ascending aorta calcifications [ 21 , 22 ]  . 
in addition , recent results derived from the mesa study ( multi - ethnic study of atherosclerosis ) determined that age , male sex , and aortic calcification were strong predictors for cac [ 5 , 23 , 24 ]  . 
thus , the focus of this study supports these previous findings by demonstrating that age , male sex , as well as both markers of arc are independent markers for cac . 
therefore , the sensitivity and specificity for arcs and arcv to detect obstructive cad were 61 and 78% , and 62 and 80% , respectively . discussion our results demonstrate a significant correlation between the presence of arc and cac . 
more importantly , arcs ( auc 0.67 , p < 0.0001 ) and arcv ( auc 0.68 , p < 0.0001 ) revealed significant discriminatory power and emerged as predictors for obstructive cad , ultimately providing incremental diagnostic value . 
furthermore , we did not compare our results to the golden standard of invasive catheter angiography to confirm the severity of cad . in conclusion , this study demonstrates that arc markers are strongly associated with and independently predict the presence of cac and obstructive cad . 
additionally , further testing is required in patients with severe arc and significant cad in order to reliably obtain these markers from thoracic - ct or x - ray for proper risk classification . compliance with ethical standards conflict of interest schoepf receives research support from astellas , bayer , bracco , ge , medrad , and siemens . 
all other authors have no conflicts of interest to disclose . christian tesche is an exchange visiting scholar supported by a grant from the fulbright visiting scholar program of the u.s. 
we further aimed to investigate whether autopsy cases characterized by increased troponin t and i concentrations as well as morphological findings of myocardial ischemia were also characterized by pathological myocardial enhancement at multiphase postmortem computed tomography angiography . materials and methods two different approaches were used . 
in the second approach , 40 forensic autopsy cases that had a cause of death attributed to acute myocardial ischemia were retrospectively selected . results the preliminary results seem to indicate that the identification of a pathological enhancement of the myocardium at postmortem angiography is associated with the presence of increased levels of cardiac troponins in * cristian palmiere cristian.palmiere@chuv.ch 1 service danatomie pathologique et mdecine lgale , cliniques universitaires saint - luc , universit catholique de louvain , brussels , belgium 2 curml , university center of legal medicine , chemin de la vulliette 4 , 1000 lausanne 25 , switzerland 3 dipartimento di sanit pubblica e medicina di comunit , universit degli studi di verona , policlinico g.b. 
 analogously , a pathological enhancement of the myocardium at postmortem angiography can be retrospectively found in the great majority of autopsy cases characterized by increased cardiac troponin levels in postmortem serum and morphological findings of myocardial ischemia . conclusions multiphase postmortem computed tomography angiography is a useful tool in the postmortem setting for investigating ischemically damaged myocardium . keywords postmortem angiography pathological myocardial enhancement forensic autopsy myocardial ischemia postmortem biochemistry troponin introduction myocardial infarction ( mi ) can be defined according to different perspectives related to clinical , electrocardiographic ( ecg ) , biochemical , and pathologic characteristics . 
it is accepted that the term mi reflects a cardiomyocyte death caused by prolonged ischemia , the latter resulting from a perfusion - dependent imbalance between oxygen supply and demand . 
the rupture or erosion of a coronary atherosclerotic plaque is the most frequent underlying condition [ 1 , 2 ]  . traditional assessment of patients presenting to the emergency department ( ed ) with suspected acute coronary syndrome ( acs ) , such as mi , includes clinical risk assessment based on cardiovascular risk factors with serial electrocardiograms and cardiac troponin measurements [ 3 ]  . detection of myocardial cell necrosis resulting from prolonged ischemia can be evaluated by a number of different means , including pathologic examination ( contraction band necrosis , cardiomyocyte necrosis ) , biochemical 1 3 96 radiol med ( 2017 ) 122 : 95105 marker measurement of myocardial cell necrosis in blood ( cardiac troponins , mb fraction of creatine kinase ) , ecg recordings ( st - t segment wave and q wave changes ) , and imaging modalities ( echocardiography and coronary angiography )  . 
indeed , its diagnostic performance in assessing coronary stenosis has been demonstrated in numerous studies [ 1 , 3 ]  . in the realm of forensic pathology , the identification of mi is based on morphological findings ( obtained from autopsy , histology , and immunohistochemistry ) and biochemical investigation results , though the sensitivity and specificity of some techniques may differ markedly due to the onset of decompositional changes [ 4 ]  . indeed , immunohistochemical methods may be influenced by several mechanisms that occur during postmortem alteration , including protein decomposition , antigen diffusion , and unspecific antibody binding in the presence of disrupted protein structures [ 58 ]  . troponin i and t levels have been measured in various studies in postmortem serum obtained from blood sampled at different sampling sites , such as the femoral veins , iliac veins , subclavian veins , aorta , right heart , and left heart . 
 moreover , troponin concentrations measured after death have been demonstrated to correlate with the severity of ischemic myocardial damage , depending on postmortem intervals [ 4 , 9 ]  . on the other hand , additional findings have been described in recent reports . 
these assert that images obtained from multiphase postmortem cta ( mpmcta ) would enable not only coronary artery imaging and evaluation of luminal narrowing to be carried out , but also identification of mi areas as areas characterized by contrast enhancement within the myocardium ( increased radioopacity from contrast medium , mean hounsfield units 95 )  . 
since contrast enhancement is absent in the normal myocardium , this phenomenon is considered pathologic and is thought to be an indirect sign of a myocardial lesion [ 1013 ]  . to the best of our knowledge , no published reports exist to date having combined data obtained from mpmcta , investigation morphological findings and biochemical results in the cases of suspected myocardial ischemia that have undergone forensic autopsies . in the study herein described , troponin t and i concentrations were measured in postmortem serum from femoral blood in a series of forensic autopsy cases that underwent mpmcta . 
our first aim was to assess whether the identification of pathological myocardial enhancement at mpmcta was correlated with increased levels of these biomarkers as well as morphological findings of myocardial ischemia . 
our second aim was to assess whether autopsy cases characterized by increased troponin t and i concentrations as well as macroscopic and microscopic findings of myocardial ischemia were also characterized by pathological myocardial enhancement at mpmcta . materials and methods study design this study was conducted during 20092015 and was designed as a retrospective , single center study . 
mpmcta and troponin t and i measurements were performed as part of medicolegal investigations . mpmcta was performed according to the standardized protocol in three phases described in a previous study [ 14 ]  . two different approaches were used . 
in one , 40 forensic autopsy cases ( 27 male subjects and 13 female subjects between 22 and 90 years of age ) that underwent mpmcta and had pathological enhancement of the myocardium ( mean hounsfield units 95 ) radiologically observed , were retrospectively selected . 
the aim was to assess whether the identification of pathological enhancement of the myocardium at mpmcta was correlated with increased troponin t and i values as well as the morphological findings of myocardial ischemia . 
in 10 out of 40 cases , death and medicolegal investigation intervals ranged between 36 and 48 h . at the same time , in the second approach , 40 forensic autopsy cases ( 28 male subjects and 12 female subjects between 36 and 67 years of age ) that underwent mpmcta and had a cause of death attributed to acute myocardial ischemia based on macroscopic and microscopic findings as well as biochemical investigation results were retrospectively selected . 
the aim was to assess whether autopsy cases characterized by increased troponin t and i concentrations as well as the macroscopic and microscopic findings of myocardial ischemia were also characterized by pathological enhancement of the myocardium at mpmcta . 
in 13 out of 40 cases , death and medicolegal investigation intervals ranged between 34 and 50 h . the cases included in the second case series were characterized by the presence of one of the following combinations of macroscopic and microscopic findings : 1 3 radiol med ( 2017 ) 122 : 95105 coronary artery atherosclerosis and acute coronary thrombosis without acute myocardial infarction . in these cases , postmortem angiography revealed complete interruption of coronary artery opacification at various sites . 
macroscopy and microscopy revealed the presence of acute thromboses in the coronary arteries as well as the presence of morphological signs of myocardial ischemia . coronary artery atherosclerosis and acute coronary thrombosis with acute myocardial infarction . in these cases , postmortem angiography revealed complete interruption of coronary artery opacification at various sites . 
macroscopy and microscopy revealed the presence of acute thromboses in the coronary arteries and the presence of morphological signs of myocardial infarction . rupture or erosion of a coronary atherosclerotic plaque , with or without hemorrhage within the plaque , with or without acute myocardial infarction . in these cases , postmortem angiography revealed various degrees of coronary artery atherosclerosis with no evidence of significant luminal narrowing . 
microscopy revealed the presence of rupture or erosion of a coronary atherosclerotic plaque , with or without hemorrhage within the plaque and with or without morphological signs of acute myocardial infarction . acute myocardial infarction with or without rupture left ventricular free wall rupture . in these cases , postmortem angiography revealed various degrees of coronary artery atherosclerosis , with or without evidence of interruption of coronary artery opacification . 
macroscopy and microscopy revealed the presence of myocardial infarction , with or without left ventricular free wall rupture , with or without acute thromboses in the coronary arteries . coronary artery atherosclerosis , without acute coronary thrombosis , with morphological signs of myocardial ischemia . in these cases , postmortem angiography revealed various degrees of coronary artery atherosclerosis without evidence of interruption of coronary artery opacification . 
 macroscopy and microscopy failed to reveal the presence of acute thromboses in the coronary arteries and revealed the presence of morphological signs of myocardial ischemia . all cases selected for this study originated from forensic practice with deaths occurring outside the hospital . 
medical records and clinical histories of the deceased as well as police reports were consistently reviewed before conclusions were made . case inclusion criteria for the first studied case series consisted of pathological myocardial enhancement at mpmcta and postmortem serum from femoral blood availability at autopsy . case inclusion criteria for the second investigated case series consisted of morphological signs of acute myocardial ischemia or myocardial infarction and postmortem serum from femoral blood availability at autopsy . postmortem investigations and sample collection unenhanced postmortem computed tomography ( ct ) scans were performed before any manipulation of the corpses in all cases included in the study . 
mpmcta was systematically carried out after unenhanced ct scans and prior to autopsies , according to the standardized protocol in three phases described in a previous study [ 14 ]  . 
autopsies were jointly performed by two forensic pathologists ( at least one board - certified ) as in accordance with both local standards and international guidelines for medicolegal cases . the presence or absence of pathological myocardial enhancement and its distribution within the myocardium was investigated by at least one board - certified forensic pathologist ( experienced in forensic imaging ) together with at least one board - certified radiologist unbeknownst to the results of previous investigations . 
the pathological enhancement of the myocardium was first identified in a subjective manner ( the presence or absence of enhancement according to the observers ) and second in an objective manner , by measuring the mean attenuation ( in hounsfield units ) of the myocardium ( using a region of interest of about 15 mm in diameter ) in the images of the three different mpmcta phases . conventional histology included haematoxylineosin ( he ) stains of brain , heart , lung , liver , and kidney samples . 
hearts were sectioned before or after fixation in 10 % neutral buffered formal the major epicardial coronary arteries were either serially sectioned at approximately 2 - mm intervals or longitudinally sectioned intact on the heart . 
in selected cases , histological sections of the coronary arteries were prepared at three different equally 1 3 98 radiol med ( 2017 ) 122 : 95105 spaced levels to best identify plaque rupture sites . 
full thickness areas involving the left anterior , lateral free wall , and left posterior ventricle as well as interventricular septum , and the right anterior , lateral free wall and right posterior ventricle were sampled . 
in selected cases , histology staining analysis for coronary arteries included he , massons trichrome and verhoeff van gieson as well as immunohistochemical investigations . toxicological analysis was performed in selected cases and included blood ethanol determination as well as general screening for volatile and nonvolatile drugs , poisons , and metabolites . peripheral blood from femoral veins was systematically collected for postmortem biochemistry as soon as possible upon arrival of the bodies at the morgue , prior to autopsy and prior to mpmcta . 
the latter were centrifuged immediately post collection at 3000g for 15 mafter centrifugation , the separated supernatant ( postmortem serum ) was collected and stored in preservative - free tubes . 
when analyses were delayed , samples were stored at 20 c . technical data chemically , the contrast medium angiofil is a mixture of esters ( mainly ethyl esters ) of polyiodinated fatty acids . 
 one study stated that combining an oily perfusate with a lipophilic contrast medium allows postmortem circulation and the performance of subsequent high - resolution postmortem angiography to be carried out . 
 paraffinum liquidum has appeared the most appropriated with which to perfuse a human body , while the use of the more viscous paraffinum perliquidum can lead to important extravasations , especially in areas where postmortem autolysis is more significant , such as the pancreas and gastric mucosa . 
by diluting angiofil with a solvent such as decane , viscosity can be decreased to the extent that it can enter the capillaries and , therefore , be used as a contrast medium in micro - angiography [ 8 ]  . 
using angiofil together with paraffinum liquidum as a solvent , as proposed per the standardized protocol of multiphase pmcta , the kinematic viscosity of the mixture measured at 40 c is approximately 6774 mm2 / s [ 10 , 14 ]  . histological alterations induced by oily contrast agents using oily contrast agent has the advantage that no leakage out of the vascular system occurs within the first 72 h . 
optical empty spaces within the vessels or even within the parenchyma are among the most common histological artifact after mpmcta with oily contract agent and are the histological analog to radiologic contrast agent - mediated oedema . 
optical empty spaces frequently appear in all tissues [ 10 ]  . laboratory assays cardiac troponin i was analyzed with the access accutni assay on access ii ( beckman coulter , fullerton , ca , usa )  . 
the clinical reference value ( according to the laboratory where the analysis was performed ) was 0.03 g / l ( corresponding to 0.03 ng / ml )  . levels of postmortem serum cardiac troponin t were measured with hs - tnt reagents by electrochemiluminescence immunoassay ( eclia )  . 
the clinical reference value ( according to the laboratory where the analysis was performed ) was 14 ng / l . toxicology consisted of ethanol determination and general unknown screening for common drugs and illegal substances by gas chromatography - mass spectrometry ( gcms ) using commercial mass spectrum libraries , 1 3 radiol med ( 2017 ) 122 : 95105 high - performance liquid chromatography with diode - array detection ( hplcdad ) , and headspace - gas chromatography flame ionization detection ( hsgcfid )  . all relevant ethical issues were identified and discussed with the local ethical committee . 
all the presented images pertain to the same case in which pathological myocardial enhancement and morphological findings of myocardial ischemia were identified . in the first case series ( 40 cases ) , the identification of pathological myocardial enhancement ( mean hounsfield units 95 ) at mpmcta systematically correlated with increased levels of troponin t and i as well as morphological findings of myocardial ischemia . 
no statistically significant differences between troponin concentrations and postmortem interval ( 1236 and 3648 h ) were observed . no case was noticed that had pathological myocardial enhancement at mpmcta without increased troponin levels or without morphological findings of myocardial ischemia . 
no case had exclusively increased troponin levels without morphological findings of myocardial ischemia , irrespective of the postmortem interval . analogously , no case had exclusively morphological findings of myocardial ischemia without increased troponin levels , irrespective of the postmortem interval . the enhancement of the myocardium at mpmcta ischemia localization of correlated with the the ( macroscopically and microscopically identified ) in all 37 cases . 
in some of these cases , the enhancement of the myocardium at mpmcta was markedly pronounced ( > 200 hounsfield units ) in the subendocardial areas of the left ventricle , where former infarcted areas were also histologically noticed . 
while the arterial phase of the mpmcta showed diffuse myocardial enhancement in most cases , this was more pronounced in the subendocardial regions of the myocardium during the venous and dynamic phases of the mpmcta . in the remaining 3 out of 40 cases , pathological myocardial enhancement at mpmcta correlated with increased levels of troponin t and i as well as various degrees of myocardial ischemia . 
the causes of death were considered to be septic shock , pulmonary embolism and trauma following a fall from heights in a subject with severe coronary artery atherosclerosis , coronary artery calcifications , and myocardial fibrosis . 
these include myocardial ischemia and direct myocardial damage due to substances released into the circulation by pathogens , cytokines , or reactive oxygen radicals released following the infectious process [ 1517 ]  . in pulmonary embolism , the sudden elevation of right ventricular pressure , and consequently increased right ventricular afterload produced by pulmonary artery outflow obstruction , results in right ventricular failure and dilatation . 
no statistically significant differences between troponin concentrations and postmortem interval ( 1434 and 3450 h ) were observed . no case had exclusively increased troponin levels without morphological findings of myocardial ischemia , irrespective of the postmortem interval . 
analogously , no case had exclusively morphological findings of myocardial ischemia without increased troponin levels , irrespective of the postmortem interval . as revealed in the first case series , myocardial enhancement at mpmcta correlated with the localization of the narrowing of the coronary artery and the localization of the myocardial ischemia ( macroscopically and microscopically identified ) in 38 subjects . 
this could be due to the fact that infarcted areas of very limited extension might not be detectable at mpmcta as pathological enhancement . globally considered , these results indicate that the identification of a pathological enhancement of the myocardium at mpmcta ( mean hounsfield units 95 ) is strongly associated with the presence of increased levels of cardiac troponins in postmortem serum and morphological findings of ischemia , irrespective of whether myocardial ischemia is considered the main cause of death , a factor contributing to death or just a potential trigger factor , as hypothesized in the case of the fall from heights in a subject with severe coronary artery atherosclerosis . analogously , a pathological enhancement of the myocardium at mpmcta can be retrospectively found in the great majority of autopsy cases characterized by increased cardiac troponin levels in postmortem serum and morphological findings of myocardial ischemia . 
this suggests the usefulness of combining mpmcta and postmortem biochemical analyses for the investigation of ischemically damaged myocardium . discussion ischemic injury of the myocardium can be differentiated as reversible and irreversible , as well as present in acute and chronic conditions . 
a , b the contrast enhancement within the myocardium ( increased radioopacity from contrast medium ) identified at mpmcta in a situation of narrowing of the coronary artery and myocardial ischemia . 
 g optical empty spaces within the vessels induced by the oily contrast material 1 3 102 radiol med ( 2017 ) 122 : 95105 refers to myocardium that is salvaged by timely reperfusion with transiently impaired contractile function that recovers spontaneously over time . 
hibernating myocardium refers to myocardium with chronically reduced contractile function associated with a local reduction in myocardial perfusion capacity [ 19 , 20 ]  . ischemic cardiomyocyte injury is characterized by progressive membrane damage with a variable degree of cell swelling . 
with prolonged ischemia , myocyte death spreads like a wave across the myocardiu the extent of necrosis depends on the occluded vessels territory , which also determined ischemia duration and the transmural extent of the infarction . 
scar tissue is markedly thinner than healthy myocardiuthe time course of this remodeling process is influenced by several factors and encompasses underlying disease or secondary event severity [ 1925 ]  . while the clinical use of differential contrast enhancement of ischemic myocardium is a relatively recent advance , the concept of differential enhancement / accumulation of contrast material in acute or chronic myocardial infarction in both cardiac magnetic resonance imaging ( mri ) and computed tomography ( ct ) imaging dates back to studies published in the late 1970s [ 26 ]  . in the initial studies that investigated contrast material uptake by ischemically damaged and normal myocardium , iodinated contrast media and ct of extirpated canine hearts with acute and chronic myocardial infarctions were used . 
 delayed scans obtained within minutes of contrast material administration revealed iodine concentrations of infarcted tissue several times greater than that of normal myocardium , irrespective of the injected contrast material ( meglumine / sodium diatrizoate , iodipamide , and an experimental polymer of iothalamic acid )  . 
 the enhancement of acute infarctions was later shown in the in situ beating heart using a prototype electrocardiography ( retrospective ) - gated ct scanner in the early 1980s [ 2636 ]  . great advances have been made in postmortem imaging during the last decade and postmortem cta has become a field of intense research . 
 they have all been demonstrated to significantly increase the quality of postmortem investigations , especially with regard to vascular system injury and disease [ 10 , 37 ]  . specifically , concerning the differential enhancement / accumulation of contrast material in ischemically damaged and normal myocardium , recent reports have indicated that mpmcta ( using the standardized protocol in three phases and a lipophilic contrast agent mixture ) would allow infarcted regions of the myocardium to be identified as areas characterized by pathological enhancement . 
this would likely be due to an abnormal leak in the infarcted myocardiuin comparison , normal myocardium does not reveal any contrast material accumulation [ 1013 ]  . as cardiac myocytes become necrotic , intracellular proteins [ myoglobin , lactate dehydrogenase , mb fraction of creatine kinase ( ck - mb ) , troponins ] leak into the interstitial space and enter the systemic circulation via local microvascular and lymphatic drainage . 
the concentrationtime profile for these markers in peripheral blood depends on their molecular weight , and location within the myocytes as well as their rates of vascular or lymphatic drainage and systemic clearance . 
small cytosolic proteins , such as myoglobin , are detectable within 12 h after tissue injury , whereas large enzymes such as lactate dehydrogenase diffuse much more slowly [ 38 ]  . troponin complex is a component of skeletal and cardiac muscle thin filaments . 
it consists of three subunits : the calcium binding sub - unit , troponin c ( tnc ) ; the inhibitory sub - unit , troponin i ( tni ) ; and an elongated sub - unit , troponin t ( tnt ) , that binds both tnc and tni , anchoring the entire complex to tropomyosin [ 39 ]  . troponins play a crucial role in muscle activity , connecting changes in intracellular ca2 + concentrations with contraction generation . 
 in humans : fast and slow skeletal isoforms and specific cardiac isofor tnt is expressed in humans by three genes coding slow and fast skeletal and cardiac isoforms of the protetnc is expressed in humans by two genes : one located on chromosome 3 that codes the cardiac / slow skeletal isoform of tnc and one located on chromosome 20 that codes the fast skeletal isoform of tnc . 
in an adult human heart muscle , the 35.9 - kda isoform tnt3 is predominantly expressed [ 40 ]  . 1 3 radiol med ( 2017 ) 122 : 95105 cardiac troponin c ( ctnc ) contains two high affinity calcium binding sites that are always occupied by ca2 or mg2 + under physiologic conditions , stabilizing an open conformation that remains anchored to the rest of the troponin complex . 
during muscle activation , calcium binding to ctnc favors an open conformation that binds to the switch region of ctni , removing adjacent inhibitory regions of tni from actin and allowing muscle contraction to proceed . 
it inhibits actomyosin interactions at diastolic levels of intracellular ca2 + [ 39 , 40 ]  . cardiac troponins are coded by specific genes and theoretically have the potential of being unique to the myocardiuindeed , cardiac troponin i ( ctni ) has not been identified outside the myocardiucardiac troponin t ( ctnt ) is expressed to a small extent in skeletal muscle ; however , current ctnt assay does not identify skeletal troponins . 
their concentrations remain raised for four times longer than ck - mb concentrations because of the sustained release of structurally bound protein from disintegrating myofibrils [ 3843 ]  . ctn - t and ctn - i are measured in routine clinical investigations of myocardial damage , mainly for the diagnosis and management of myocardial infarction . 
hence , differences in clinical findings should be carefully considered when evaluating postmortem data and clinical reference values should not be directly used in interpreting results obtained from postmortem serum samples . 
these limits notwithstanding , femoral blood postmortem serum troponin levels have been shown to be reliable in investigating the severity of myocardial damage and correlate with the ischemic myocardial damage severity [ 4 , 9 , 4448 ]  . the results of the study presented herein support the hypothesis that pathological enhancement of the myocardium at mpmcta ( mean hounsfield units 95 ) combined with further postmortem analysis results , such as troponin i and t determination , may be useful in the investigation of myocardial ischemia and myocardial infarction . this is the first study , to the best of our knowledge , to assess the radiological profile of myocardial ischemia combined with further postmortem investigation results ( with specific regard to cardiac troponins ) in a series of cases that had undergone forensic investigations , including postmortem angiography , histology , and biochemistry . 
ethylenevinyl alcohol copolymer was used as embolic agent in 12 patients : alone in 5 cases , in association with glue and with glue and thrombin in 3 and 2 cases , respectively , during tae . 
onyx was injected in two cases of embolization performed with dpsi : in one case alone and in the other in combination with thrombin and glue . results technical success rate was 100% . 
immediate clinical success was 91.7% ; in one patient ceus revealed * gianpaolo carrafiello gcarraf@gmail.com interventional radiology , department of radiology , insubria university , viale borri 57 , 21100 varese , va , italy 2 diagnostic and interventional radiology unit , university of milan , viale di rudin 7 , milan , italy 3 vascular surgery department , university of insubria , viale borri 57 , 21100 varese , va , italy 4 department of radiology , luigi sacco university hospital , via g.b. 
camillo hospital , circonvallazione gianicolense 87 , 00152 rome , italy 6 department of radiology , universit degli studi del molise , campobasso , cb , italy persistent t2 el , decreased if compared with that before the procedure . 
no major or minor complications were registered . conclusions onyx could be an ideal embolic agent for endovascular and percutaneous embolization of t2 el . keywords ethylene - vinyl alcohol copolymer onyx type ii endoleak embolization introduction endovascular aneurysm repair ( evar ) is considered the standard therapy for most patients with abdominal aortic aneurysm ( aaa ) [ 1 ]  . 
el is defined as persistence of blood flow within the excluded aneurysm sac , classified according to the underlying etiology , location , and aortic branch vessel involvement [ 2 ]  . 
type i and type iii endoleaks require early intervention ; however , the treatment strategy for type ii endoleak remains controversial because spontaneous resolution is expected [ 2 ]  . 
several recent studies have demonstrated that nearly 20% of immediate type ii endoleaks persist and that persistent type ii endoleaks are associated with secondary interventions and aneurysm rupture [ 2 , 3 ]  . 
1 axial ct shows aneurysmal sac supplied ( type ii endoleak ) ( arrow ) ( a ) ; multiplanar reconstruction confirms type ii endoleak ( arrow ) ( b ) communicate through a channel . 
direct puncture sac injection ( dpsi ) is usually performed after unsuccessful transarterial embolization ( tae ) or persistent endoleak and enlargement of the aneurismal sac after tae [ 5 ]  . 
due to these properties and because onyx is not absorbable , it is capable of producing permanent vascular occlusion [ 6 ]  . we report our experience with the use of ethylene - vinyl alcohol copolymer ( onyx ) for the treatment of type ii endoleaks after evar either with endovascular that percutaneous approach . materials and methods from march 2007 to march 2015 , 455 patients with aaa underwent to endovascular exclusion . 
patients were routinely monitored at the institution and follow - up included computed tomography angiography ( cta ) at 30 days , cta or contrast enhanced ultrasound ( ceus ) at 6 months and cta at 12 months postoperatively and annually thereafter . 
a total of 22 patients ( 30.5% ) met the criteria for treatment . ceus was performed in all patients before treatment , to confirm t2 el and its origin ( lumbar and / or mesenteric )  . 
 in one of the 22 patients , ceus pre - treatment revealed a high flow el ( t1b el ) , confirmed by angiography and treated with an iliac endogra in 21 patients , t2 el was treated with tae ( n 18 ) , dpsi ( n 10 ) or laparoscopic ligature of the inferior mesenteric artery ( n 1 )  . 
dpsi was considered in case tae was unsuccessful , which occurred in 8 out of 18 patients . in this study , we considered all the embolization performed using ethylenevinyl alcohol copolymer ( onyx , ev3 neurovascular , irvine , california ) as embolic agent , alone or in combination with other embolic agents . 
onyx was injected in two cases of embolization performed with direct puncture of the sac : in one case alone and in the other in combination with thrombin and glue . 
the choice of embolic agent was at the discretion of the operator , although glue and onyx were used primarily when endoleak persisted at the angiography or saccography performed during the procedure . all procedures performed in this study were in accordance with the ethical standards of our institutional research committee and with the 1964 helsinki declaration and its later amendments . 
safety was defined as the frequency of intra - , periand post - procedural complications [ 5 ]  . results eleven men and one woman with a mean age of 62.8 years ( range 5283 years old ) comprised the study population ( table 1 )  . 
the indication for endoleak treatment included persistence of a type ii endoleak after 12 months follow - up and enlarging aneurysm sac size . a direct aneurysm sac access approach was employed in 10 patients and the transarterial access was used in 18 patients . 
3 contrast enhanced ultrasound ( ceus ) confirmed type ii endoleak ( a ) ; direct puncture of the sac was performed using cbct as imaging guidance ( b , c ) ; onyx was injected directly by the needle used for the puncture ( d ) ; final cbct confirmed distribution of the onyx in the sac ( e ) 1 3 158 radiol med ( 2017 ) 122 : 154159 immediate clinical success was 91.7% , in particular in 11 / 12 cases ceus performed at the end of the procedure demonstrated absence of endoleak ; in the remaining case ( 1 / 12 ; 8.3% ) ceus revealed persistent t2 el , decreased if compared with that before the procedure . 
cta was performed as protocol of follow - up and confirmed clinical results reported . secondary clinical success was 91.7% ; until today , in one patient t2 el is persistent , with suspected inflow from a small patent lumbar artery ; nevertheless , at the moment of submission ( follow - up of 24 months ) , the patient remains asymptomatic and the sac diameter is stable ( 55 mm ) , therefore , no indication for re - treatment are present . no major or minor complications were registered during or after the procedure . 
during the procedure , one patient treated with endovascular approach , complained mild abdominal pain , at the beginning of the embolization ( probably related to the arrival of dmso within the el ) , but any analgesic was administered . 
at the end of the procedure , one of the two patients treated with percutaneous approach , experienced mild back pain , solved with common analgesics within 24 h . discussion type ii endoleak is the most common complication after endovascular aneurysm repair ( evar ) which could lead to a possible risk of aneurysmal sac enlargement and rupture [ 2 , 7 , 8 ]  . 
many techniques have been described to treat type ii endoleak . in the past , type ii endoleaks were usually treated surgically , both with graft explantation and with retroperitoneal ligation of collateral feeding vessels . 
if there are no arterial routes for transarterial embolization , dpsi is feasible as alternative method to treat type ii endoleak [ 9 ]  . during these years , embolization of endoleaks has been performed with many different embolic agents like glue , coils , thrombin and onyx . 
the principal advantage of the use of a liquid embolic agent in the treatment of type ii endoleaks relates to the ability of a liquid to fill the endoleak sac completely including all inflow and outflow vessels . 
the solid cast formed by a liquid embolic agent should result in a non compressible structure through which recanalization does not occur , providing more durable repair than that provided by coils . the onyx liquid embolic system consists of an ethylenevinyl alcohol copolymer dissolved in anhydrous dimethyl sulfoxide ( dmso )  . 
using onyx , the embolized vessels are completely filled by the embolic agent and are less fragile because of the lower inflammatory reaction and the absence of polymerization heat compared with nbca - embolized . 
 when the inflammatory reaction caused by onyx was evaluated on histologic specimens on humans , the inflammatory reactions of the vessel wall were less pronounced and were located mainly intravasally , while no reaction of the surrounding interstitium , such as migration of lymphocytes into perivascular areas , was observed [ 12 ]  . 
the inflammatory response and vascular toxicity seemed primarily to be associated with the injection rate , as the slow endovascular delivery of dmso produced no untoward angiographic or pathologic changes but a fast injection of dmso caused endothelial necrosis and severe inflammatory response in the arterial wall [ 13 , 14 ]  . according to this , onyx should be the best way to reach embolization . 
the association with other embolizing agents , like glue , is to prefer when the sac is large ; in this way we can get perfect and safe embolization of the sac . 
 we have started to use it in el that would need too much onyx , in particular the last patient of the list with percutaneous approach and in two recent cases of type ia el embolization by dpsi was used at the end of the procedure to fill proximal cap with extreme precision . the major weak point of the manuscript is represented by the small number of patients ( 12 patients ) enrolled in a long time period ( 9 - years )  . 
in addition , onyx was used alone or combined with other embolic agents , with endovascular or 1 3 radiol med ( 2017 ) 122 : 154159 percutaneous approach on the basis of the operator confidence and / or experience ; even this aspect may be considered a technical bias . no randomized study comparing different embolic agent and its capacity to fill sac is now available ; and it is difficult to achieve because even in large centers the number of cases is never so numerous . on the basis of the characteristics described onyx could be an ideal embolic agent and our experience demonstrated its safety ; to overcome the necessity to use too much onyx for a single procedure , it could be associated with others embolic agents and in particular its role could be to fill the gap remained in the sac filled by other embolic agents and to create a proximal cap communicating with the feeding vessel . 
all patients underwent conventional mri and diffusion - weighted imaging ( dwi ) at baseline and 1 , 3 , 6 , and 18 months after the beginning of therapy . 
tumor volumes and mean adc measurements of the five examination series were compared ; correlation of adc values and tumor regression was estimated . * pietro valerio foti pietrofoti@hotmail.com 1 radiodiagnostic and radiotherapy unit , university hospital policlinico - vittorio emanuele , via santa sofia 78 , 95123 catania , italy 2 department of ophthalmology , university of catania , catania , italy 3 department g.f. 
ingrassia , institute of pathology , university of catania , catania , italy 4 unit di biomedicina molecolare genomica e dei sistemi complessi , genetica , biologia computazionale , department g.f. 
ingrassia , university of catania , catania , italy 5 dipartimento di oftalmologia , universit politecnica delle marche , ancona , italy results mean adc values of ocular melanomas significantly increased already 1 month after therapy whereas tumor volume significantly decreased only 6 months after therapy . 
pretreatment adc value of ocular melanomas and early change in adc value 1 month after therapy significantly correlated with tumor regression . conclusions in ocular melanoma treated with pbt , adc variations precede volume changes . 
both pretreatment adc and early change in adc value may predict treatment response , thus expanding the role of dwi from diagnostic to prognostic . keywords magnetic resonance imaging diffusionweighted imaging uveal melanoma proton therapy treatment response orbit introduction uveal melanoma is the most frequent malignant intraocular tumor with an incidence of 68 per million per year in western europe [ 1 ]  . 
the majority ( 80 % ) of the ocular melanomas originate in the uvea , anatomically consisting of the choroid posteriorly and ciliary body / iris anteriorly , whereas the remainder arise in non - uveal sites , including the conjunctiva [ 2 ]  . the risk factors predicting metastatic disease are large tumor size , tumor thickness , extraocular tumor extension , and secondary glaucoma ( for iris melanomas ) [ 3 ]  . common clinical features of uveal melanoma include blurred vision , visual field defect , decreased visual acuity , floaters , pain , and increased intraocular pressure [ 4 ]  . 
the diagnosis is usually done on fundoscopic examination and ultrasound ( us ) , whereas cross - sectional imaging is necessary in case of opaque lens or significant subretinal effusion [ 5 ]  . 1 3 132 radiol med ( 2017 ) 122 : 131139 the earliest treatment for uveal melanoma was removal of the eye ; in recent years , enucleation has been largely replaced by various forms of radiation therapy ( episcleral brachytherapy , proton - beam radiotherapy , and stereotactic radiotherapy ) having the purpose to achieve local tumor control , conserving the eye and useful vision [ 6 ]  . proton - beam radiotherapy ( pbt ) is available at a few centers ; among the different globe - sparing radiotherapic approaches , it has the widest inclusion criteria . 
owing to their physical properties ( finite range in tissue , sharp lateral penumbra ) [ 7 ] , proton beams make it possible to deliver high doses of radiation to the tumor with relative sparing of adjacent tissues ; the possibility to highly collimate the beam allows to reduce collateral damage to adjacent structures such as the optic nerve and fovea . 
moreover , pbt requires little or no ( in case of iris melanoma ) surgical procedures . although pbt is a safe and effective modality to treat uveal melanoma , with low toxicity and enucleation rates [ 8 ] , however , due to tumors heterogeneous biological behavior and radiotherapy - related complications , additional noninvasive imaging markers that may predict outcome are needed [ 9 ]  . the gold standard for local tumor follow - up is us based on the international collaborative ocular melanoma study ( coms ) criteria , to define tumor relapse and advocate treatment . 
us is useful at baseline and for monitoring the size of a melanoma after irradiation [ 10 , 11 ] ; nevertheless , therapy - induced changes in tumor volume may occur relatively late in the time course of treatment [ 12 ] , therefore assessment of tumor treatment response based on morphological evaluation ( changes in tumor size ) is a late index . cross - sectional imaging modalities such as magnetic resonance imaging ( mri ) can be used to assess the extent of ocular melanoma , to evaluate optic nerve involvement , to visualize possible extraocular spread ( which can change the tumors management ) and to plan proton - beam therapy . in the last years , diffusion - weighted mr imaging ( dwi ) with apparent diffusion coefficient ( adc ) , the quantitative parameter of dwi , has been proposed as the technique of choice for detection of early response to treatment in brain tumors and head and neck cancers [ 1315 ]  . 
this ability of adc measurements to predict response might provide for the opportunity to individualize therapy , thus enabling early termination of treatment in nonresponding patients , preventing additional toxicity , and allowing for early changes in treatment [ 16 ]  . the purpose of this prospective study was to investigate the proton - beam - induced changes in adc values of ocular melanoma treated with pbt in patients undergoing long - term mri follow - up and to assess whether variations in adc constitute a reliable biomarker for predicting and detecting the response of ocular melanoma to pbt . materials and methods patients this study was a single - institution prospective , consecutive case series . 
the work described has been carried out in accordance with the code of ethics of the world medical association ( declaration of helsinki ) for experiments involving humans and in accordance with recommendations of the local ethic committee ; informed consent has been obtained from patients . between may 2012 and february 2015 , 20 patients with diagnosis of ocular melanoma were considered for eligibility . 
all patients were examined by an ophthalmologist specialized on ocular tumors , and the final clinical diagnosis of ocular melanoma was made on the basis of fundoscopic and ultrasonographic findings before the mri examination . 
however , contrary to all other malignant tumors , a biopsy is not required to make a diagnosis of uveal melanoma [ 10 ] ; ophthalmoscopy is the criterion standard for diagnosing ocular melanoma with a diagnostic accuracy as high as 99.7 % [ 17 ]  . inclusion criteria were as follows : posterior tumor margin extending close to optic disk so that plaque radiotherapy could not be administered reliably without causing optic neuropathy ; tumor extending close to fovea so that there was a better chance of conserving central vision with proton - beam radiotherapy than with other methods ; tumor height exceeding 5.5 mm ; inappropriateness of other forms of conservative treatment . exclusion criteria were : tumor previously treated by other methods ; bilateral tumor ; contraindications to mr imaging examination ; insufficient mr imaging quality ( e.g. , owing to movement artifacts ) ; discontinued mr imaging examinations during therapy ; presence of distant metastases . patients underwent serial mr imaging examination ( five examinations per patient : one baseline examination and four follow - up examinations : 1 , 3 , 6 , and 18 months after the beginning of the therapy , respectively )  . 
insertion of tantalum markers was carried out as previously described [ 18 ]  . to exclude distant metastases , all patients underwent also multidetector computed tomography ( mdct ) examinations of chest , abdomen , and pelvis before the beginning of the therapy and during the follow - up period . 1 3 radiol med ( 2017 ) 122 : 131139 fig . 
organs at risk are listed as follow : on ( optic nerve ) , f ( fovea ) , l ( cornea - limbus ) protonbeam therapy protocol treatment was delivered at catana proton therapy facility [ istituto nazionale di fisica nucleare - laboratori nazionali del sud ( infn - lns ) ] , where a 62 - mev proton beam , produced by a superconducting cyclotron ( sc ) , has been used for the treatment of shallow tumors , such as those of the ocular region [ 19 ]  . all patients received a total dose of 60 gy ( relative biological effectiveness , rbe ) , delivered in four consecutive fractions of 15 gy ( rbe ) on four consecutive days , using a constant rbe of 1.1 over the modulated bragg peak . eyeplan software , developed at the massachusetts general hospital for eye tumor therapy using proton beams , was used for treatment planning [ 20 ]  . patients were treated in seated position , with individualized immobilization devices , such as thermoplastic mask and byte - block ; the eyelids were fixed with an adhesive plaster , to reduce eye movements . 
patients were invited to fix a light point , the position of which in space was defined at the time of treatment planning . the optimal fixation point in space was defined with the aim of irradiating the target volume while saving the surrounding healthy organs ( optic disk , fovea and anterior segment structures , lens , and ciliary body , when possible )  . 
all mr examinations included a standard brain study too . image analysis for image analysis , data were transferred to a ge workstation with advanced imaging analysis software . the images of ocular mr examinations were evaluated by two radiologists in consensus ( a neuroradiologist with 10 years of clinical experience and a neuroradiology fellow with 4 years of practice experience )  . 
it was documented whether the ocular tumor touched the lens , the iris , or the ciliary body , and whether there was retinal detachment or extraocular spread . tumor - volume measurements were performed , as previously described [ 18 , 21 ] , on contrast - enhanced axial t1 - weighted images with the use of a computerized imageanalysis tool , available as part of our hospitals picture archiving and communication system ( pacs )  . 
the volumes from the first and fifth scans for each patient were used to calculate percentage variation of tumor volume after 18 months of therapy ( tumor percentage regression )  . in all the five time point examinations , the quantitative adc measurements were performed as previously described [ 18 , 2123 ] , using a dedicated workstation with diffusion analysis software ( advantage windows version 4.6 , software functool , general electric medical systems , milwaukee , wi , usa )  . 
of averages section thickness ( mm ) interslice gap ( mm ) field of view ( mm ) matrix frequency direction b - value ( sec / mm2 ) 160 160 256 256 160 160 256 224 160 160 256 256 right to left anterior to posterior right to left 200 200 192 192 right to left 0100 synoptic table summarizes the imaging parameters of mr sequences . 
t1 - weighted fse spectral presaturation sequences were performed before and after intravenous administration of 0.2 ml gadoteric acid ( gadoterate dimeglumine , dotarem , 0.5 mol / l ; guerbet , roissy , charles - de - gaulle cedex ; france ) per kilogram of body weight . 
therefore , the final study population consisted of 17 eyes of 17 patients ( 11 women and 7 men ; mean age [ sd ] , 45 years [ 5 , 12 ] ; range , 3056 years )  . the right eye was affected in 10 patients ( 59 % ) and the left eye in 7 ( 41 % ) patients . 
no tumors extrascleral spread was found at mr examination . no distant metastases were found at mdct examinations of chest , abdomen , and pelvis neither before the beginning of the therapy , nor during the follow - up period . mean volume changes at baseline examination , mean volume ( sd ) of ocular melanoma was 382 mm3 ( 291 ) , ( range 761120 mm3 )  . 
five year local control rates exceeded 90 % , 5 - year overall survival rates ranged from 70 to 85 % , 5 year metastasis - free survival and disease - specific survival rates from 75 to 90 % , 5 year enucleation rates from 7 to 25 % . 
complication rates vary : glaucoma ( 730 % ) , cataract ( 2062 % ) , vitreous bleeding ( 914 % ) , any type of retinopathy ( 2367 % ) , and optic neuropathy ( 733 % ) [ 8 ]  . it is likely that inherent tumor characteristics may play a role in visual prognosis , since the most common reported predictors of ocular complications following radiotherapy are tumor distance from the optic nerve , tumor thickness , and radiation dose [ 24 ]  . although pbt of uveal melanoma achieves high rates of local tumor control and in the last decade both surgical and medical methods have been developed to treat radiation complications thus improving the toxicity profile of pbt , the biological behavior of the tumor still remains heterogeneous and tumor response to therapy may vary in the same case series . in this setting , it is desirable to rely on early noninvasive markers that correlate with long - term outcome metrics and may predict treatment response . our study revealed the potential of dwi in the detection of early tumor response and its capability to predict treatment outcome in ocular melanoma patients treated with pbt . 
the purpose of this prospective study was to investigate the proton - beam - induced changes in adc values of ocular melanoma treated with pbt in patients undergoing long - term mri follow - up and to assess whether variations in adc constitute a reliable biomarker for predicting and detecting the response of ocular melanoma to pbt . the patients of our series underwent a follow - up of 18 months . 
all except two patients showed the maximum decrease in tumor volume between 3 and 6 months after pbt ; in the remaining two patients the maximum decrease in tumor volume was observed even between 6 and 18 months . 
it is therefore likely that in this time interval ( 318 months ) the effect of therapy on tumor volume is more noticeable , suggesting that changes in tumor volume occur more slowly after pbt than after other types of radiation therapy . 
actually this result confirms previous observation that tumor regression is less rapid after proton - beam treatment than after ruthenium - 106 plaque radiotherapy , probably because of the very high doses of radiation delivered to the tumor base during brachytherapy [ 6 ]  . conversely to the relatively slow changes in tumor volume , adc value modifications after pbt seem to occur more rapidly . in our case series , after pbt , a decrease in tumor volume and a corresponding increase in adc was observed in all the four follow - up time points . 
however , whereas adc values of ocular melanoma significantly increased already 1 month after therapy , tumor volume significantly decreased 6 months after therapy only . significant change of mean adc value occurred in advance of corresponding change in tumor volume , thus indicating that dwi may detect macromolecular and microstructural changes in tissue architecture at the cellular level and is not dependent on relatively slow changes in tumor size . 
therefore , in monitoring tumor response during 1 3 136 radiol med ( 2017 ) 122 : 131139 1 3 radiol med ( 2017 ) 122 : 131139 10 fig . 
2 axial mri images in a 49year - old woman with ocular melanoma of the right eye , who exhibited good response to treatment ( ad before therapy ; eh 1 month after therapy ; il 3 months after therapy ; mp 6 months after therapy ; qt 18 months after therapy ) ( a , e , i , m , q t2 - weighted turbo spin - echo stir images ; b , f , j , n , r postcontrast t1 - weighted spin - echo spectral presaturation images ; c , g , k , o , s diffusion - weighted images ; d , h , l , p , t adc map )  . 
tumor percentage regression was 52 % 10 10 10 10 therapy , dwi may provide earlier indications of therapeutic outcome than changes of tumor volume can do . this result is consistent with previous researchs findings . 
in this previous article , the pretreatment adc value significantly correlated with tumor regression and during the follow - up period the adc values of ocular melanomas significantly increased in advance of the corresponding significant decrease of tumor volume . in ocular melanoma , tumor regression depends on the type of radiotherapy and the cell - doubling time . 
cells can be damaged by ionizing radiation directly or indirectly through the formation of toxic - free radicals ; irradiated cells undergo apoptosis and necrosis , resulting in tumor shrinkage , ischaemia , infarction , and fibrosis [ 6 ]  . 
 [ 29 ] , using an animal tumor model , demonstrated that induction of necrosis with associated apoptotic cell death by cytotoxic treatment causes an increase in tumor adc detectable prior to changes in tumor volume ; on the other hand , apoptosis alone is not sufficient to induce measurable changes in adc . currently , the availability of quantitative measures ( such as adc ) acquired periodically is key in the management of oncologic patients , to monitor the effectiveness of therapies . from this point of view , dwi is preferable to other methods since it is noninvasive , time - sparing , easy to perform , and radiation - free , thus allowing close follow - up during cancer treatment . 
the authors found high - resolution t1and t2 - weighted images at 3 t to be superior to those at 1.5 t in visualization of the anatomic details of the orbit . 
image quality may be improved by adopting some technical expedients such as the application of short echo time , multichannel coil , and parallel imaging that will increase imaging contrast and decrease susceptibility artifacts [ 31 ]  . in our mr protocol , we used an epi sequence for dw imaging . 
epi - dwi suffers from geometrical distortions due to susceptibility artifacts , especially in regions with air - tissue transitions such as in the head and neck area [ 32 ] and particularly in the orbit . 
 [ 32 ] compared haste - dwi with epi - dwi early during crt for their potential to predict locoregional outcome in patients with head and neck squamous cell carcinoma . 
the authors demonstrated that , although haste - dwi has a lower incidence of geometric distortions , it seems to be inadequate in early response prediction , compared to epi - dwi which has greater potential to predict locoregional outcome after chemoradiotherapy . our study has some limitations : the main one is the small number of patients . 
second , in our study the final diagnosis of ocular melanoma was based upon fundoscopic and ultrasonographic findings without histological evidence , hence to perform a correlation between histological features and adc values of the tumor was not possible . conclusions our study demonstrated that in patients with ocular melanoma treated with pbt , undergoing 18 months followup , the major effects of therapy on tumor volume occur between 3 and 18 months . 
in any case , adc variations precede volume changes , thus making dwi useful in determining early treatment response or failure . the significant correlation we observed between pretreatment adc value and tumor regression and between early change in adc value and tumor regression once again confirms the potential of adc to predict treatment response , thus expanding the role of dwi in uveal melanoma from diagnostic to prognostic . the object of future larger clinical studies or systematic review and meta - analysis could be to determine a threshold of pretreatment adc value or early change in adc value for prediction of tumor response , to provide a scientific evidence in this field . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . 
all authors disclose any financial and personal relationships with other people or organizations that could inappropriately influence their work . ethical statement all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . radiol med ( 2017 ) 122 : 140145 doi 10.1007 / s11547 - 016 - 0699 - 1 radiotherapy hadrontherapy from the italian radiation oncologist point of view : face the reality . 
the italian society of oncological radiotherapy ( airo ) survey giulia marvaso1 barbara vischioni2 barbara alicja jereczekfossa1 , 6 delia ciardo1 piero fossati3 tommaso giandini3 sara morlino5 mauro carrara4 paola romanelli1 elvio russi5 francesca valvo2 riccardo valdagni4 , 6 roberto orecchia6 , 7 received : 12 september 2016 / accepted : 6 october 2016 / published online : 21 october 2016 italian society of medical radiology 2016 abstract hadrontherapy has been in constant progress in the past decades . 
due to the increasing interest in this field and the spreading of the technique in italy and worldwide , the italian society of radiation oncology surveyed ( by an online survey ) its members regarding their perception of hadrontherapy . 
the survey outline addressed different items all related to hadrontherapy , such as : demographics ( 3 items ) , personal knowledge ( 5 items ) , actual use in clinical practice ( 5 items ) , and future perspectives and development ( 5 items )  . 
analysis of our results might picture the clinical attitude of the ro community towards hadrontherapy in italy , and help in promoting targeted initiatives to spread clinical results and knowledge about technical innovations in this field . keywords hadrontherapy survey proton therapy carbon ion radiation oncologist * giulia marvaso giulia.marvaso@ieo.it introduction 1 department of radiotherapy , ieo - european institute of oncology , via ripamonti 435 , 20141 milan , italy 2 clinical division , cnao national center for oncological hadrontherapy , pavia , italy 3 medical physics unit , fondazione irccs istituto nazionale dei tumori , milan , italy 4 division of radiation oncology , fondazione irccs istituto nazionale tumori , milan , italy 5 radiotherapy department , s . 
croce & carle teaching 6 department of oncology and hemato - oncology , university 7 scientific direction , european institute of oncology , milan , hospital , cuneo , italy of milan , milan , italy italy evidence is accumulating for the use of carbon ion radiotherapy [ rt ] in radioresistant tumors , such as soft - tissue sarcomas , mucosal melanomas , and adenoid cystic carcinomas of salivary glands . 
furthermore , an increasing number of patients are being treated worldwide with proton therapy because of advantageous physical properties that allows dose escalation especially in skull base and paraspinal tumors , eye melanomas , and pediatric treatment [ 1 ]  . in a statistic from the official journal of the particle therapy cooperative group ( ptcog ) , it is reported that more than 137 , 000 patients were treated with particle therapy worldwide from 1954 to 2014 , 86 % of which with protons and 14 % with carbon ions and other particles [ 2 ]  . 
in italy , hadrontherapy started in 2011 at cnao national center for oncological hadrotherapy in pavia [ 3 ] , with approximately 1000 cancer patients treated so far . considering the spreading of the technique in italy and worldwide , advantage of hadrontherapy compared to photon rt has become a matter of debate at congresses , and level i evidence with results from controlled randomized trials comparing photon with particle therapy has been advocated from the scientific community . 
waiting for results from ongoing clinical trials , with this survey , we aim at investigating the perception of hadrontherapy among the italian radiation oncologists ( ro )  . survey design and questionnaire the questionnaire was designed within a collaboration of three italian institutes , namely , the european institute of oncology ( ieo ) in milan , the national cancer institute ( int ) in milan , and the national center for oncological hadrontherapy ( cnao ) in pavia , in the framework of a research project supported by the italian association of cancer research ( associazione italiana per la ricerca sul cancro , airc ) , and it was distributed by the italian society of oncological radiotherapy ( airo )  . 
the third and fourth sections ( 5 questions , respectively ) were more specific on the current use of hadronterapy routinely in clinical practice , the perception of potential development and the future perspectives of heavy particles . 
the questionnaire was sent by email to all the active airo members and was available on the airo website from february 2016 to may 2016 . statistical analysis the results of the survey were analyzed using descriptive statistics by sas statistical software . 
1 number of answering participants per question number of participants radiation oncology 224 ( 100 % ) characteristic specialization < 40 years > 40 years unknown / no answer working experiences in training < 5 years > 5 years unknown / no answer geographical distribution north italy center italy south italy unknown / no answer 76 ( 33.9 % ) 138 ( 61.6 % ) 10 ( 4.5 % ) 23 ( 10.3 % ) 31 ( 13.8 % ) 167 ( 74.6 % ) 3 ( 1.3 % ) 130 ( 58.0 % ) 51 ( 22.8 % ) 38 ( 17.0 % ) 5 ( 2.2 % ) per question is shown in fig . 
all the percentages presented below are expressed with respect to the number of nominal number of participating ros ( namely , 224 ) , and not to the effective number of answering ros per question , since the number of non - answering ros is informative itself . section 1 : participants characteristics respondents characteristics are summarized in table 1 . section 2 : personal skills the aim of this section was to investigate the perception about the level of knowledge of hadrontherapy as selfdefined by each responder . 
3 evaluation of the advantages radiobiology background , and ( 3 ) the ongoing clinical trials ( 190 participants answered the question , multiple choices answers ) as shown in fig . 
 the biological superiority in the treatment of hypoxic and radioresistant tissues together with the reduced toxicity to organs at risk received the highest score ( weighted mean 3.9 , in an increasing scale of agreement from 1 to 5 ) , as shown in fig . 
3. the same agreement was observed for the cons most often advocated in disfavor of hadrontherapy : the lack so far of level i clinical evidence and the issue of organ motion and set - up variation are perceived as serious disadvantages ( weighted mean 3.1 ) , besides cost effectiveness and limited number of facilities throughout the country ( weighted mean 3.8 ) , as shown in fig . 
these results were confirmed by a more general question about the use of hadrontherapy ( without distinguishing between the different particles ) : radioresistant tumors ( such as sarcomas ) 1 3 radiol med ( 2017 ) 122 : 140145 fig . 
 despite the questionnaire was submitted twice , we registered a relative low response rate ( about 20 % of the airo active members ) , with a difference in the geographical distribution of participants , for the most part from ro working in clinical institutes from the north of italy . 
in northern italy , two hadrontherapy facilities are in operation at the moment for cancer treatment : the cnao in pavia with a dual beam of both protons and carbon ions since 2011 , and the azienda provinciale per i servizi sanitari ( apss ) 1 3 144 radiol med ( 2017 ) 122 : 140145 proton therapy center located in trento devoted only to proton treatment since 2015 . 
in southern italy , the activity with protons has been underway since 2002 in the laboratories of the south of the istituto nazionale di fisica nucleare ( infn - lns ) , although devoted only to ocular pathology with limited number of patients treated per year [ 4 ]  . 
physicians older than 40 years were more likely to respond to our survey even if hadrontherapy might be considered the relative young branch of rt , probably because of its recent introduction in the clinical reality in italy , and the yet small numbers of devoted chapters in academic books . despite the not high participation obtained in our survey , our results might still reflect the shared vision and expectations among the italian ros regarding hadrontherapy , who declare to acquire more specific knowledge on the field mostly with research articles and at scientific meetings . 
 in line with the great coverage in the literature about the physical and radiobiological peculiarity of particle therapy , there is consensus among the respondent ros about the well - known radiobiological advantages of particles as compared to photons reported in many publications [ 5 ]  . 
as supported by many dosimetric comparison studies , there is also awareness about the reduced toxicity to organs at risk when using particles [ 6 ] in various anatomic sites for treatment of tumors of different origins compared to photons . 
probably because of lack of information about italian treating centers and specific indications among patients and professional medical doctors , respondent ros still report a low number of patients requesting to be referred to hadron treatment during routine clinical activity in rt departments . 
an important technological and scientific ( physics , radiobiology ) effort has been made in parallel in order to reduce the cost of the facilities and to fully take advantages of the beam properties : standardization of beam scanning , image guided treatment , robust and 4 - dimensional ( 4d ) planning [ 8 ]  . 
 furthermore , the increasing number of facilities , the development of hypofractionation , and the selection of indications will contribute to find the true place of particle therapy in the rt scenario , despite the debate on cost effectiveness [ 9 ]  . if the consolidated indications are considered eye melanomas , skull base and pediatric tumors for proton therapy , and soft - tissue sarcomas , salivary glands , and nasal cavity tumors for carbon ions treatment , no tentative conclusion has been drawn about the role of hadrons for other common tumors , such as prostate , breast , and lung cancers , traditionally considered classical targets for conventional radiotherapy . since in silico analysis showed major advantages with particles dose escalation in terms of enhancing effects on all tumor sites without overlapping toxicities [ 6 ] , it is claimed that the conclusive way to demonstrate particle therapy advantages in safely improving outcomes for patients might be by conducting carefully constructed randomized prospective clinical trials [ 10 ]  . since 2013 , more than 200 clinical trials are ongoing , including comparisons between advanced photons modalities , proton therapy and carbon ions therapy . 
the situation for carbon ion therapy is similar , with the longest experience in patient treatment and clinical trials coming from japanese treatment centers [ 11 ]  . randomized controlled trials should remain the ideal tool for research in hadrontherapy : they should be focused ideally on tumor sites where there is a low risk of systemic failure , a high risk of local progression , and / or a high risk of toxicity with conventional therapy [ 10 ]  . in addition to promoting randomized clinical trials , hadrontherapy centers should develop prospective registries with the goal of long - term data collection on an international basis to support the evidence provided by observational studies and comparative effectiveness research trials [ 12 ]  . 
in this way , the use of proton and carbon ion beams could be increased for common cancer rising the number of clinical indications , since the better therapeutic ratio proved by the numerous retrospective studies published so far . the long - term effects assessment on large patient cohorts will allow to evaluate the exciting dosimetric data from in silico analysis produced so far . 
surely , there is space for a better definition of the indications for hadrotherapy , and the optimal patient selection hopefully will be warranted in the near future [ 8 ]  . conclusions in view of the continued increase in the number of hadron therapy centers ( i.e. , neutron , proton and light or heavy ions ) , there is considerable public , scientific , clinical , and technological and health management - related interest in the further development of particle therapy for cancer worldwide . 1 3 radiol med ( 2017 ) 122 : 140145 our survey wanted to picture the interest and attitude in italy for particle therapy among the ro community . 
in the era of precision medicine and in a multidisciplinary strategy , it has been claimed that progress in rt is based on a global approach of the patient and tailored / personalized well - targeted treatment of the tumour , including both technology driven improvement of treatment conformality with hadrons and novel biological targeted drugs [ 13 , 14 ]  . acknowledgments this study was partially supported by the research grants from associazione italiana per la ricerca sul cancro ( airc ) : ig - 14300 carbon ions boost followed by pelvic photon radiotherapy for high - risk prostate cancer , and ig - 13218 shortterm high precision rt for early prostate cancer with concomitant boost to the dominant lesion . compliance with ethical standards ethical approval this article does not contain any studies with human participants or animals performed by any of the authors . funding this study was funded by the research grants from associazione italiana per la ricerca sul cancro ( airc ) : ig - 14300 carbon ions boost followed by pelvic photon radiotherapy for high risk prostate cancer , and ig - 13218 short - term high precision rt for early prostate cancer with concomitant boost to the dominant lesion . conflict of interest gm , tg , and pr have received research grants from associazione italiana per la ricerca sul cancro ( airc ) : ig - 14300 carbon ions boost followed by pelvic photon radiotherapy for high - risk prostate cancer . 
the aim of this review is to analyse the spectrum of radiological signs as reported in the recent literature , in light of our series over a 15 - year period , to pinpoint the most common radiological patterns in a developed country and to determine the role played by the different chest imaging techniques in diagnosis improvement . 
in 21 cases with lymphadenopathies without lymph - bronchial diffusion ( age range 2 months7 years ) , ct identified the ghon focus in 16 / 21 cases ; chest x - ray never identified the ghon focus . 
in our series , pleural tb was present in 8 cases out of 146 under 5 years of age , 5 cases out of 76 under 2 years , and 18 cases out of 71 over 5 years . 
radiologists should be aware of typical patterns of tuberculosis , to provide an early diagnosis . keywords tuberculosis chest ct children chest radiography mri * paolo tom paolo.toma@opbg.net 1 department of imaging , bambino ges children hospital , irccs , rome , italy 2 paediatrics and infectious disease , bambino ges children hospital , irccs , rome , italy introduction the incidence of tuberculosis ( tb ) is increasing in the developed world and children in particular represent a high - risk group for developing the disease [ 13 ]  . 
computed tomography ( ct ) is currently the most accurate tool available for chest imaging . the aim of this review is to analyse the spectrum of radiological signs as reported in the recent literature , in light of our series of 217 / 255 cases of lung tb over a 15 - year period , to pinpoint the most common radiological patterns in a developed country and to determine the role played by the different chest imaging techniques in diagnosis improvement . natural history demonstrates that age is the critical variable influencing the risk that primary m . 
 an infant is at the highest risk , and then , the risk drops but remains significant in the second year of life , to reach its lowest level in infected children aged between 5 and 10 years of age . 
for more than 50 % of children developing the disease , the onset is within 1 year from the primary infection , therefore , children aged less than 2 years , and / or immunocompromised children can reasonably be considered as a high - risk group [ 4 ]  . the immune mechanisms of the adult - type disease are ambiguous , but it is a noticeable observation that it occurs only as children enter into puberty . 
it is crucial to recall that children with adult - type disease are frequently sputum smear positive and that they do represent a factor of disease transmission , mostly in agglomerations , such as schools [ 5 , 6 ]  . the diagnosis of childhood tuberculosis presents a major challenge , as it is complicated : bacteriological confirmation is often inadequate for children because of the paucibacillary 1 3 radiol med ( 2017 ) 122 : 2234 fig . 
on the left , the ghon focuses ( black empty arrow ) not identified by the plain radiographs character of their disease : the poor bacteriologic specimen [ 7 ] and cultures are positive only in 2550 % of cases . 
contrariwise , samples are elevated in children with adult - type disease , and sputum smear microscopy can adequately assess infectious pulmonary tuberculosis in older children ( more than 10 years of age ) [ 9 ]  . the diagnosis of childhood tuberculosis in no endemic areas is usually based on : 1 . 
actually , normal chest x - ray does not rule out tb , as it is negative in 15 % of cases of proven tb [ 1014 ]  . one of the biggest problems in comparing data is related to the poor inter - observer agreement in the diagnosis of primary tb in children using chest x - rays and , more generally , to the selection and description of radiological signs of lung infections in children . 
the readout array , to which the phosphor is coupled , consists of a 43 cm 43 cm amorphous silicon ( a - si ) photodiode and a thin - film transistor ( tft ) array ( 0.143 mm pixel pitch )  . from 2000 to 2010 , ct scans in our hospital have been performed with a somatom plus scanner ( siemens , erlangen , germany )  . 
sedation , however , was required for uncooperative children . from 2010 to date , we have been using a second - generation dual source ct system ( siemens somatom definition flash , siemens erlangen , germany ) with two x - ray tubes and two detectors settled at an angular offset of 95 . 
with the old scanner , contrast was administered by hand injection . at present , we normally use an automatic injector ( stellant , medrad , inianola , usa ) with the following parameters : 1 ml / s for 24 - gauge catheters ( rarely and with the greatest caution ) , 1.52.0 ml / s for 22 - gauge catheters , and 23 ml / s for 20 - gauge catheters , with a pressure limit adjusted to a maximum of 150 psi ( 1034 kpa )  . 
the ct volume data were collected from the thoracic inlet level to the diaphragm level , and were transferred and analysed in pacs ( kodak - carestream healthcare )  . the radiation doses we administered are within the limits of the proposed european diagnostic reference levels for pediatric ct [ 16 ]  . 
lung tb was present in 217 out of 255 patients ( 85 % ) : 146 patients were under 5 years of age ( 76 under 2 years ) and 71 over 5 years ( 41 over 10 years )  . the diagnosis of tuberculosis was established by the detection of three or more of the following elements : ( 1 ) clinical presentation ( symptoms or signs ) ; ( 2 ) contact history ( household and close contacts ) ; ( 3 ) purified protein derivative ( ppd ) tuberculin skin test and igra test ; ( 4 ) chest radiography and ct ; ( 5 ) bacteriological examination ( including examination of sputum , tuberculous pleural effusion , bronchoalveolar lavage , gastric aspirates , cerebrospinal fluid , and peritoneal fluid ) ; ( 6 ) bronchoscopy ; and ( 7 ) biopsy if necessary . 
following the gold standard , the diagnosis of tb was confirmed when mycobacterium tuberculosis ( mtb ) was isolated . in our series of patients , chest x - rays were obtained from 2000 to 2003 with the conventional screen - film radiography ( sfr )  . 
in 2003 , the sfr system was replaced with a computed radiography ( cr ) syste in 2010 , a siemens ysio direct radiography ( dr ) system with a flat panel detector ( siemens , erlangen , germany ) was also introduced . 
in the discussion of diagnostic procedure radiation doses , comparison to more familiar radiation exposures ( such as chest x - rays or natural background radiation ) has been recommended to facilitate the understanding of the dose . 
the dose delivered during a chest x - ray is so low that using it as denominator to estimate the equivalent number of chest x - rays comparable with the level of dose of any other radiological technique may be misinforming and may unreasonably alarm patients and parents [ 22 ]  . in the future , mri could substitute ct mainly in the evaluation of mediastinal lymphadenopathy . 
about the drawbacks for mri of the lung , two of these tissue properties are of the highest 1 3 26 radiol med ( 2017 ) 122 : 2234 importance : the low proton density and the susceptibility differences between tissue and air . 
the respiratory and cardiac movements that cause a decrease of temporal resolution represent another peculiar aspect [ 25 , 26 ]  . rarely , in < 2 years of age or immune compromised children , the ghon focus can evolve directly into consolidation with intra - bronchial spread and bronchopneumonic consolidation [ 27 ]  . imaging findings children are different in size , anatomy , and physiology compared to adults . 
we will describe different patterns differentiating infants and children from adolescents and young adults ( table 1 )  . infants and children we have adopted the radiological classification of tb proposed by marais [ 15 , 27 ]  . 
following this classification , we have distinguished four main entities : lymph node tb ( lymphobronchial tb ) ; air - space parenchymal tb ( consolidation / atelectasis ) ; miliary tb ; pleural tb . the ghon focus is a localized pneumonic process , referred to as the primary parenchymal focus , limited at the site of organism deposition . 
one case ( 7 years ) had a lymph - bronchial disease ( see below )  . younger children , due to their anatomical size , have also narrower airways with less supportive cartilage , making them more compressible . 
in synthesis , complicated lymph node disease includes compression , erosion , ulceration , infiltration , intra - bronchial passage of caseous material , and formation of granulation tissue ( adenobronchial fistula )  . adolescents and young adults absence of lymphadenopathy air - space parenchymal tb cavitation ( 45 % ) bronchogenic spread linear branching opacities tree - in - bud tuberculomas pleural tb consolidation / atelectasis segmental / lobar distribution predilection for the upper lobes lower and middle lobe predominance 1 3 radiol med ( 2017 ) 122 : 2234 in fact , indications for completing the survey with ct after contrast medium are not standardized . ct is useful in clinics , especially for children aged under 2 years , for whom the conventional chest x - ray is often insufficient . 
ct allows to see a mixture of both sharply and poorly defined , 14 mm nodules , in a diffuse , random distribution often associated with intraand interlobular septal thickening . 
the axial view shows unilateral lymphadenopathies ( white arrow ) , peripheral ghon focus ( black empty arrow ) , and lymphangitis ( c ) 1 3 28 radiol med ( 2017 ) 122 : 2234 fig . 
six months later small - calcified foci ( white arrows ) in hilar and mediastinal lymph nodes and in the consolidation ( b , c ) chest x - ray may be normal at disease onset ( 2540 % )  . 
pleural effusion is often unilateral [ 15 ]  . pleural involvement occurs after direct spread of caseous material from a sub - pleural parenchymal or lymph node focus , or from haematogenous spread . 
usually , it represents a hypersensitivity response , but tuberculous empyema rarely develops , depending on the quantity and virulence of bacilli entering the pleural space and on the immune status of the host [ 27 ]  . 
us is crucial in the detection and in the structure evaluation and guiding a pleural tap . pericardial effusion usually develops when a subcarinal lymph node erupts into the pericardial space [ 6 ]  . 
sometimes , the infection causes a thickening of the pericardium without an effusion , and this can also constrain the pumping action ( constrictive pericarditis ) [ 35 ]  . 
traditionally , it refers to both reinfection and reactivation of tb , but the age - related distinction has changed , because primary infection can occur at any age ( especially in countries with low tb incidence )  . 
exogenous reinfection is typical of endemic areas and distinguishing the features of post - primary tuberculosis area predilection for the upper lobes and the absence of lymphadenopathy and cavitation [ 32 ]  . 1 3 radiol med ( 2017 ) 122 : 2234 fig . 
lymphadenopathies with the rim sign : low - density centre and enhancing rim ( white arrows ) tb manifest as parenchymal disease ; airway involvement ; pleural / pericardial extension . parenchymal disease consolidations are typical also of the adult - type disease that first occurs around 810 years of age and becomes the common aspect of the disease during adolescence . 
complications include cavity development and intra - bronchial spread [ 6 ]  . cavity is a gas - filled space within a zone of pulmonary consolidation or within a mass or nodule , produced by the discharge of the necrotic part of the lesion via the bronchial tree [ 32 ]  . 
on the right , the external compression of the bronchus intermedius ( black arrow ) with atelectasis and bronchiectasis of inferior and middle lobe and hyperinflation of the right upper lobe 1 3 30 radiol med ( 2017 ) 122 : 2234 fig . 
compression of the right upper bronchus by tuberculous lymph nodes and consolidation of the upper lobe with the areas of necrotic liquefaction and shift of the mediastinum ( ac ) fig . 
consolidations in the apical and posterior segments of the upper lobe and the apical segment of the left lower lobe with cavities inside ( a , b ) defined margins , and often demonstrate calcifications ( 20 30 % of cases )  . 
satellite nodules around the tuberculoma may be present in as many as 80 % of cases [ 1315 , 32 ]  . airway involvement bronchogenic spread is detected in 95 % of the cases by ct [ 13 , 14 ]  . 
branching nodular and linear opacities ( tree - in - bud ) and centrilobular nodules ( a , b ) disease activity the literature [ 32 , 38 ] reports ct signs of disease activity , which can be summarized as follows : tree - in - bud appearance , clustered nodules , lobular consolidations , thick - walled cavities , rim - enhancing nodes ( short axis > 1 cm ) , and pleural effusion . 
contrast - enhanced ct scan shows the results of a bronchogenic spread ( mainly on the right upper lobe ) with consolidations , several cavities , and centrilobular small nodules ( a )  . 
camillo hospital , circonvallazione gianicolense , 87 , 00152 rome , italy 5 diagnostic and interventional radiology unit , department of health sciences , university of milan , via a . 
no major complications were registered . conclusions a short - term patency benefit may be obtained including pcb in angioplasty treatment of failing hemodialysis arteriovenous shunts . keywords paclitaxel - coated balloon outflow stenoses hemodialysis arteriovenous shunt introduction vascular access complications are one of the main causes associated with an increase in morbidity and mortality in stage 5 chronic kidney disease patients [ 1 ]  . despite the relatively low arteriovenous fistula ( avf ) thrombosis rate , existing guidelines advocate surveillance programs for early detection of stenosis and its correction before thrombosis occurs , to reduce morbidity and prolong access patency [ 2 ]  . the pathophysiology of stenosis of hemodialysis access is complex . 
these mechanisms seem to be similar in autogenous and prosthetic vascular access [ 1 ]  . the main purpose of vascular access monitoring and surveillance programs is the early identification of stenosis , because it is the main cause of avf dysfunction and thrombosis . the nkf - k / doqi guidelines for vascular access recommend the use of vascular adequacy parameters and 1 3 70 radiol med ( 2017 ) 122 : 6976 physical examination for monitoring avf and av grafts ( avg ) [ 2 ]  . in - graft at the venous anastomosis and in the outflow vein in the synthetic av fistula ( table 1 )  . the nfk - k / doqi guidelines recommend that each dialysis center should determine which procedure for the correction of stenosis [ percutaneous transluminal angioplasty ( pta ) or surgery ] is best for the patients , based on the expertise of the center [ 2 ]  . nowadays , endovascular intervention in the form of balloon angioplasty may be considered a safe and effective treatment for failing avfs and avgs . 
re - stenosis is common and angioplasty may be easily repeatable [ 3 ]  . access stenosis should be treated if stenosis is 50 % and is associated with abnormalities such as previous thrombotic episodes , elevated intra - access pressure ( iap ) , abnormal recirculation , abnormal physical signs , unexplained decrease in adequacy dialysis parameters , and decreased blood flow [ 2 ]  . 
the procedure is classified as successful if there is less than a 30 % residual lesion according to nfk - k / doqi [ 2 ]  . a paclitaxel - coated balloon ( pcbs ) provides rapid delivery of the antiproliferative drug to the local vessel wall and inhibition of neointimal hyperplasia compared with plain balloon ( pb ) [ 5 , 6 ]  . 
however , there are few studies in the literature supporting the use of pcb for endovascular management of hemodialysis ( hd ) access vascular stenosis [ 6 ]  . as few other authors [ 68 ] , we hypothesized that combining coronary pcb with conventional plain balloon ( pb ) or cutting balloon ( cb ) would improve the effectiveness of pta for the treatment of outflow lesions . the purpose of this study is to report our experience with drug - eluting balloons for the treatment of outflow stenoses of failing hemodialysis arteriovenous shunt and to evaluate the primary patency ( pp )  . materials and methods the study protocol was approved by our internal review board . 
written informed consent was obtained from each participant before beginning any study - related procedure . this is a prospective , single - center study , designed to evaluate the safety and technical and clinical outcomes of paclitaxel eluting over plain balloon angioplasty for the management of venous stenosis in avgs and avfs . from september 2014 to september 2015 , both autogenous arteriovenous fistulas ( n 20 ) and prosthetic arteriovenous grafts ( n 30 ) were treated . 
the inclusion criteria were asymptomatic stenosis 50 % revealed by routine surveillance , non - complicated symptomatic stenosis causing malfunctions of the vascular access , and symptomatic stenosis complicated by thrombosis . 
balloons 57 mm in diameter were used . a total of 64 stenoses were registered ; central stenoses ( from the axillary vein to the junction between the superior vena cava and the right atrium ) were excluded from our evaluation : 3 in the avf fistula and 3 in avg ; arterygraft anastomosis ( n 1 ) was also excluded . 
 therefore , a total of 57 stenoses were considered in the present study , subdivided into : 24 in avf and 33 in avg ( table 1 )  . the median follow - up was 8 months ( range 615 )  . all the procedures were performed in our angiographic suite ( allura xper fd20 philips , best , the netherlands )  . 
after inducing blood flow from the needle hub , a 150 - cm , 0.035 - inch hydrophilic guide wire was inserted through the plastic hub to advance it into the vessel . 
if one or more stenoses were confirmed , a 7 - f introducer ( cordis , miami lakes , fl ) was inserted via the guide wire , flushed with normal saline , and then fixed in place . 
after removing the introducer , the puncture site was manually compressed until hemostasis was achieved . a successful pta was defined as residual stenosis < 30 % . follow - up was assessed routinely by the same clinical and hemodynamic criteria described earlier . 
the remaining seven ( 12.3 % ) stenoses were associated with another stenosis and incidentally documented during fistulography . the procedure was technically successful in all cases . the clinical success rate was 94.7 % , in particular in three cases ( 6 % ) thrombosis of the vascular access occurred within the first post - procedure 48 h and patients were immediately referred to the surgical theater for thrombectomy ( two pva and one ava )  . in all cases , dialysis was routinely conducted after discharge and cvc placement was never done . 
in four cases , four new significant ( 50 % ) stenoses was registered ; the new stenoses were documented in different sites of those treated . on the basis of sir guidelines [ 9 ] , no major complications were recorded . 
in - hospital mortality was not observed ; major local or systemic morbidity was not observed . # number , sd standard deviation , ihd ischemic heart disease , bmi body mass index , copd chronic obstructive pulmonary disease , ava autogenous vascular access , cvc central vein catheter , p.pt per patient , pva prosthetic vascular access 1 3 74 radiol med ( 2017 ) 122 : 6976 mean hospitalization time was 16 7 h ( range 625 )  . 
 patency of the vascular accesses was 100 % at discharge . discussion in recent years , percutaneous interventional techniques have been tried and established as a viable alternative means in the management of fistula dysfunction . 
angioplasty is efficacious with some advantages compared to conventional surgical treatment , such as a shorter time needed to perform the procedure and shorter hospitalization , less discomfort for the patient and lower infection rates . 
additionally , it enables dialysis immediately after the procedure without the necessity of using a central venous catheter [ 2 , 4 , 9 ]  . percutaneous transluminal angioplasty ( pta ) is the mainstay of treatment in stenosed hemodialysis access [ 2 , 4 ]  . 
this induces vascular damage and may cause subsequent restenosis [ 5 . ] the high incidence of post - pta recoil , caused by the pathogenesis of this type of stenosis [ 11 ] , has stimulated the search for new devices and alterative endovascular procedures [ 12 ]  . 
as regards pta , proposals include the use of high - pressure balloons [ 2 , 4 ] and prolonged inflation with devices that allow simultaneous perfusion of the fistula [ 11 ]  . cutting balloon is a noncompliant balloon equipped with three or four microblades ( atherotomes ) mounted longitudinally on the outer surface of the balloon . 
these factors are apparently responsible for the lower rates of restenosis [ 13 ]  . the use of cutting balloon was introduced to improve hemodialysis access and long - term patency [ 14 ]  . cutting balloon angioplasty proved to be safe and effective in the treatment of graft - to - vein anastomotic stenosis , with significantly higher assisted primary patency than that of conventional balloon angioplasty [ 15 ]  . the concept of developing a balloon - based drug delivery system to prevent arterial restenosis was based on the hypothesis that a durable effect on neointimal proliferation could be achieved following the single - time delivery of paclitaxel into the vessel wall [ 5 ]  . the safety and effectiveness of drug - coated balloons have been confirmed in percutaneous coronary interventions [ 16 , 17 ] and in peripheral interventions [ 18 , 19 ]  . after balloon dilatation , the pathways of the biological tissue response are regarded to be generally similar in arteries and dialysis access vessels . as mentioned above , the pathophysiology underlying the occurrence of stenosis of hemodialysis access is complex . 
potential mediators that have been suggested to play a role in this process include basic fibroblast growth factor ( bfgf ) , platelet - derived growth factor ( pdgf ) , vascular endothelial growth factor ( vegf ) , and extracellular matrix ( ecm ) proteins [ 20 , 21 ]  . 
 [ 6 ] revealed a significantly higher rate of hd access patency at 6 months in 20 patients undergoing hd treated with ptapcb compared with the other 20 patients treated with ptapb ( 7 with arteriovenous fistulas and 13 with arteriovenous grafts in each study arm )  . the results of this study indicate that drug - coated balloons improve the short - term patency and possibly inhibit neointimal hyperplasia in the artery - anastomosed vein , similar to the results described earlier in the coronary artery and peripheral artery . one study indicates that far infrared radiation is a promising therapy for retarding neointimal hyperplasia and improving unassisted patency of functioning arteriovenous fistulas [ 23 ]  . 
many other studies have established that coated paclitaxel is rapidly delivered to the vessel wall and that it delays neointimal growth and prevents vascular restenosis [ 1619 ]  . the present study showed that by including pcb in ptapb treatment , a short - term patency benefit may be obtained , which may result from the short - term antihyperplastic effect induced by the release of paclitaxel into the vessel wall . 
 [ 8 ] concluded that the use of drug - eluting balloons , after standard angioplasty , improves the primary patency and decreases reinterventions of target lesions in juxta - anastomotic stenoses . comparing the results of fistuloplasty between different studies is difficult because of the many variables involved . 
 some authors considered only native fistulas with juxtaanastomotic stenosis , many of which were recurrent [ 24 , 25 ] ; others only de novo stenoses [ 8 ] or only in - stent stenoses in autogenous dialysis fistulas [ 26 ]  . a recent review [ 27 ] demonstrated the limited data available ; currently , in literature six studies ( two randomised control trials ( rcts ) and four cohort studies ) that reported on 254 interventions in 162 participants have been available . 
at 6 months , target lesions primary patency was reported between 70 and 97 % for pcb in the rcts and cohort studies , and 026 % for non - pcb . 
 target lesions treated with pcb were associated with a higher primary patency at 6 months as compared to nonpcb balloons . on the basis of presented data , association of pcb to cutting balloon angioplasty may be considered useful for treatment of failing hemodialysis vascular accesses . 
our results show promising high primary patency ( 87.7 % ) ; longer follow - up and more patients are needed to investigate the incidence of restenosis , and the necessity for repeated procedures as well as a study about cost - effectiveness would be useful . however , the present study has some limitations . 
first , this study includes a heterogeneous population with autogenous and prosthetic vascular access , with distal and proximal lesions , and the nature of differences in the lesions was not fully considered . 
second , this study was performed in a single center and had a limited sample size with a short follow - up ( re - treatment , stenting and surgical revision are not considered in this follow - up period )  . in conclusion , a short - term patency benefit may be obtained including pcb in angioplasty treatment of failing hemodialysis arteriovenous shunts . 
several issues remain to be determined as research advances , and results from large , multicenter randomized controlled trials are awaited to validate the beneficial effect of pcb angioplasty in dialysis access stenoses and establish specific indications according to high - quality evidence . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . radiol med ( 2017 ) 122 : 4352 doi 10.1007 / s11547 - 016 - 0686 - 6 neuroradiology stentassisted coiling in ruptured cerebral aneurysms : multicenter experience in acute phase mario muto1 francesco giurazza2 mario tecame4 emiliano schena5 maurizio de nicola6 alessandro sgreccia6 mirko giannoni6 simone peschillo7 francesco diana7 giulio guidetti7 gianluigi guarnieri1 gennaro ambrosanio1 pasquale vassallo1 francesco briganti3 received : 14 june 2016 / accepted : 29 august 2016 / published online : 8 september 2016 italian society of medical radiology 2016 abstract introduction the purpose of this study is to report on a multicenter experience of ruptured intracranial aneurysms treated in acute phase with stent - assisted coil embolization , including primary success rates and midterm follow - up results . materials and methods retrospective analysis was performed on a sample of 40 patients ( 14 men , 26 women , mean age 59.7 years ) affected by ruptured saccular aneurysms and treated by stent - assisted coiling in acute phase ; double antiplatelet therapy with clopidogrel bisulphate and acetylsalicylic acid was started after the procedure . 
82.5 % had a favorable outcome ( gos : ivv ) , while 17.5 % presented a poor score ( gos : iiii )  . conclusions stent - assisted coil embolization is a feasible endovascular treatment option for ruptured intracranial aneurysms , which is difficult to approach with simple coiling ; however , neurointerventionalists need to consider a mild increase of post - procedural complications rate . inclusion criteria were the presence of acute sah on computed tomography ( ct ) and stent - assisted embolization . 
exclusion criteria included previously treated aneurysms , evidence of dissecting aneurysms or pseudoaneurysms , and contraindication to antiplatelet therapy . data were collected from electronic or physical charts , and angiography . all protocols were reviewed and approved by the institutional review board of each center independently in accordance with the declaration of helsinki principles . keywords stent coiling ruptured aneurysm cerebral acute population data introduction the endovascular embolization of intracranial aneurysms has emerged as a viable and sometimes a preferable method of treatment of intracranial aneurysms [ 1 ]  . 
however , endovascular treatment of wide - necked aneurysms represents still a challenge to neurointerventionalists because of the risk of coils protrusion from the aneurysm into the parent artery [ 2 ]  . assisted techniques with balloons have been developed to obtain a safe coil packing into the sac in these wide - neck lesions . 
there is a reluctance to use intracranial stents during the acute post - hemorrhage period because of the risk of thromboembolic complications in patients who are not pre - treated with antiplatelet therapy , and the fear that using antiplatelet agents in the post - rupture period may increase the risk of re - bleeding or peri - procedural complications related to placement of ventriculostomies [ 3 ]  . balloon remodeling has provided an alternative to intracranial stents especially since it can be used without antiplatelet therapy [ 4 , 5 ] ; however , there is a concern that balloon remodeling is not always the ideal choice of treatment for all wide - necked aneurysms [ 68 ]  . the purpose of this study is to report on a multi - center experience of ruptured intracranial aneurysms treated in acute phase with stent - assisted coil embolization , including primary success rates and midterm follow - up results . materials and methods this is a retrospective study to analyze radiological and clinical outcomes from all patients with ruptured wide - neck intracranial aneurysms treated with stent - assisted coiling . the neurointerventional database was screened for patients presenting with subarachnoid hemorrhage ( sah ) treated in neurointerventional radiology departments during the same hospitalization at three high - volume centers between 2010 and 2014 . a sample of 40 patients was involved in this analysis ( table 1 )  . 
there were 14 men ( 35 % ) and 26 women ( 65 % ) with a mean age of 59.7 years ( range 2984 years )  . the angiographic characteristics of the ruptured aneurysms are provided in table 1 ; on the basis of angiogram or three - dimensional reconstructions , location , dome size , and neck / dome ratio were recorded . 
surgical treatment was usually preferred for anterior circulation aneurysms , when the patients had a large parenchymal hematoma and were very young . in all cases , before the procedure , patients underwent to non - enhanced ct ( nect ) , angio - ct , and digital subtraction angiography ( dsa )  . the duration of angiographic follow - up considered for this analysis was 1 year ( 030 months )  . the protocol included a first follow - up visit with angiographic control study performed at 36 months with mr and angio - mr , depending on the primary result of the endovascular treatment . 
 extended imaging follow - up was tailored to the individual patient . additional coiling was scheduled in cases in which the aneurysm was reopened by coil compaction or resolution of intraluminal thrombus . technique the embolization procedures were performed by experienced interventional radiologists ( 325 years of experience ) , always with patients under general anesthesia . 
coils were deployed using the jailing technique ( releasing the stent after positioning the microcatheter into the aneurysm sac ) or the coil - through technique ( first releasing the stent and then positioning the microcatheter into the aneurysm sac passing through the stent interstice )  . in addition , if the stent was placed after initial - unassisted embolization or balloon - assisted embolization , it was defined as a bailout procedure , and the reason for placement of the stent ( e.g. , instability of coils pack ) was noted . anticoagulation protocol all patients were treated with heparin during the procedure . 
clinical consequences of thromboembolic complications were recorded . the primary occlusion rate was classified as total occlusion ( > 95 % occlusion rate ) , neck remnant ( > 80 % occlusion rate with contrast medium filling only the neck area of the aneurysm ) , partial occlusion ( distal filling of contrast medium in the aneurysm regardless of the occlusion rate ) , or none ( unsuccessful coiling ) [ 9 ]  . 
angiographic occlusion was considered to be adequate if either complete occlusion of the aneurysm or a small neck remnant with over 80 % occlusion was achieved . endovascular treatment was considered to be technically successful if the deployed stent extended at least 5 mm over the aneurysm neck on both sides of the aneurysm and adequate angiographic occlusion was achieved [ 9 ]  . 
all technique - related major complications were considered to constitute technical failures , regardless of angiographic outcome . the sah was pre - operatively radiologically classified on the basis of nect , according to the fisher score . the pre - operative clinical condition of the patients was evaluated using the hunt and hess classification , and the clinical outcome was independently measured by experienced neurosurgeon / neurologists using the glasgow outcome scale ( gos ) [ 10 ]  . statistical analysis nect was performed in all cases immediately after the procedure in order to assess new hemorrhages related to the coiling ; then , according to the ongoing clinical conditions , other ct or magnetic resonance ( mr ) scans were acquired on demand . all data analyses and statistical tests were performed in matlab environment ( mathworks , inc , natick , massachusetts )  . 1 3 46 results two - thirds of the patients were women ; 20 % of the aneurysms were located in the posterior circulation . 
of the 40 aneurysms , 42.5 % were located in the carotid syphon , 20 % in the anterior communicating artery , 12.5 % in the middle cerebral artery , 12.5 % in the basilar artery , 5 % in the posterior communicating artery , 5 % in the anterior cerebral artery , and 2.5 % in the vertebral artery ( table 1 )  . the mean size of the sac was 7 mm ( range 322 mm ) ; 55 % were small ( < 7 mm ) , 35 % medium ( 713 mm ) and 10 % large ( 1424 mm )  . 
in the other 80 % , stent positioning was planned : of this , 50 % was performed with the jailing technique and 50 % with the coil - through technique . 
 the stents adopted for coil assistance are reported in table 2 : the most employed device ( 65 % ) was the enterprise stent ( codman )  . from a technical point of view , the stent deployment was always successful ( 100 % )  . 
in all cases , a nect was performed at the end of the embolization , and no cases of increase of the sah were observed . no intra - procedural re - bleeding occurred ; however , in 12.5 % of the cases , a minor re - bleeding was detected in the first 3 weeks after the procedure , and these were just monitored and not treated because they were reabsorbed earlier , while clopidogrel was suspended for 5 days . 
 hydrocephalus developed in 15 % ( 6 patients ) ; in one case , double antiplatelet therapy was interrupted in order to insert an external drainage . the long - term follow - up showed 25 % of the patients with vessel stenosis documented at the 1 - year dsa of control . 
in six patients ( 15 % ) , the 36 months of follow - up , confirmed by subsequent dsa , revealed aneurysm refilling , 4 involving the sac and 2 only the neck ; in the first group , a new endovascular treatment had been successfully performed . the clinical status was recorded during the hospital recovery after the procedure has been analyzed . 
the stent action is twofold : it serves as a scaffold for the placement of coils enabling dense aneurysm packing [ 15 ] , and it reduces the rate of aneurysm recanalization by redirecting the blood flow reducing the intra - aneurysmal flow [ 16 , 17 ] and promoting the endothelialization at the level of the aneurysm neck [ 18 ]  . 1 3 47 radiol med ( 2017 ) 122 : 4352 fig . 
a nect showing massive sah ; b angio - ct detecting a small aneurysm ( 4 mm ) of left va associated with a fenestration of the origin of ba ; c volume rendering postprocessing ; d dsa anteroposterior projection confirming angio - ct findings ; e release of enterprise stent extending from left va to the ba ; f final dsa run anteroposterior projection confirming aneurysm exclusion after coiling . 
clinical outcome was favorable with a gos 14 at the end of the hospital stay ; no complications occurred during the recovery and long - term follow - up in recent years , stent - assisted coiling has been proposed also for acutely ruptured aneurysms [ 9 , 19 ] : indeed , early treatment of ruptured aneurysms is recommended because of the high risk of subsequent re - rupture [ 20 , 21 ] , and in this scenario , treatment decision is more challenging , especially for wide - neck lesions where stent assistance represents an important addition to the treatment repertoire [ 9 ]  . however , it must be considered that the reported complication rate of stent - assisted coiling with early adverse events in ruptured aneurysms is 10 times higher than that in 1 3 radiol med ( 2017 ) 122 : 4352 fig . 
a angio - ct with maximum intensity projection reconstruction showing a wide - neck small aneurysm of the right carotid syphon ( black arrow ) ; b dsa anteroposterior projection confirming angio - ct findings ( white arrow ) and detecting also the origin of the posterior communicating artery from the neck ( red arrow ) ; c remodeling technique with balloon - assisted embolization : white arrow indicates the tip of the microcatheter into the sac , and the white circles show the markers of the balloon ; d migration of a coil into the vessel lumen despite the balloon ; e bailout stenting ( enterprise ) to contain the coils into the sac ; f final dsa control demonstrating sac exclusion , patency of the carotid syphon and of the posterior communicating artery . 
followup with 3 - month angio - mr and 1 - year dsa confirmed the good procedural success with good clinical table 2 technique and stents adopted technique 80 % planned 20 % bailout 40 % jailing 40 % coil - through enterprise 65 % stent neuroform 25 % solitaire 15 % unruptured aneurysms , with early re - bleeding accounting for most mortality [ 22 ]  . 
a nect showing diffuse sah ; b angio - ct with volume rendering reconstructions showing a small blister aneurysm ( 3 mm ) of right carotid syphon ; c dsa lateral projection confirming angio - ct findings ( arrow ) ; d stentassisted embolization with enterprise stent ( circles ) and coiling ; e post - embolization dsa in lateral projection showing total occlusion of the carotid syphon ( star ) ; f dsa lateral projection showing complete flow restoration after abciximab infusion ; g 2 - week nect follow - up showing resolution of the sah ; h 1 - year follow - up dsa lateral projection showing complete aneurysm exclusion with minor stenosis of the carotid syphon in correspondence of the stent . 
clinical outcome was favorable with a gos 14 at the end of the hospital stay ; no complication occurred during the recovery and long - term follow - up this is mainly related to the double antiplatelet therapy required to avoid stent occlusion ; indeed , sah is itself a hypercoagulable status , and in this setting , a stent is highly thrombogenic for the parent vessel until the stent has been endothelialized [ 24 ] ; hence , post - stenting double antiplatelet therapy ( i.e. , clopidogrel and acetylsalicylic acid ) is essential ; however [ 9 ] , acute sah represents a contraindication to these drugs for the risk of re - bleeding . 
 [ 26 ] concluded that complications of stent - assisted coiling for ruptured intracranial aneurysm can be affected by the method of antiplatelet administration . in literature , the overall stent assistance embolization procedure - related complication rate , including both hemorrhagic and thromboembolic complications , is approximately 13 % [ 23 ] , which is higher than reported complication rates in stent - assisted coiling of unruptured aneurysms , which are in the range of 67 % [ 27 , 28 ] .of particular concern is the risk for hemorrhage in patients who require evd placement or conversion of evd to a permanent shunt , given the need for ongoing antiplatelet therapy . 
the data reported in this study in terms of overall complication rate and clinical outcome are in accordance with literature published data [ 19 , 23 ]  . 1 3 50 radiol med ( 2017 ) 122 : 4352 fig . 
a nect showing mild sah located in the basal cisterns and left silvian scissure ; b rotational dsa with 3d post - processing showing an aneurysm of the anterior communicating artery with a posterior bleb , both a2 origin from the sac ; c stentassisted coiling after positioning an enterprise stent in a1 - a2 left ; d stent thrombosis ( white circle ) , e solved by intra - arterial infusion of abciximab ( reopro 5 ml ) and balloon angioplasty ; f final dsa control showing bilateral patency of a2 and sac exclusion with a minimal perfusion of the neck ; g post - procedural nect showing no re - bleeding in neither ischemic area ; h rotational dsa with 3d postprocessing 7 months after embolization showing patency of both a2 , no signs of stent thrombosis , minimal perfusion of the neck and sac exclusion in this series , the mostly used stent was the enterprise stent . 
 [ 29 ] in their review compared enterprise and neuroform for stent - assisted coiling and observed that deployment failures , intracranial hemorrhage , mortality among all patients , and recanalization were more commonly reported in neuroform - treated aneurysms , while the enterprise was associated with higher reported complete occlusion at follow - up ; they concluded that both devices are safe and effective with comparable permanent morbidity . 
these features of enterprise stent demonstrate that it is easier to deploy than the opened - cell stent and enable the treatment of additional aneurysms [ 30 ] ; the closed - cell design stent has a greater tendency to slightly alter normal vascular anatomy owing to its design . 
delivery of the open - cell design neuroform stent to more distal vessels may be more difficult as it requires the use of a 0.027 diameter microcatheter rather than the 0.021 diameter microcatheter used to deliver the closed - cell design enterprise stent . 
nevertheless , it is important to underline that navigation of either microcatheters occurs in very small vessels , and this circumstance itself already demands a certain level of expertise [ 31 ]  . 
the use of either the enterprise or neuroform stent is at the discretion of the treating neurointerventionalist , and the decision is made on a case - by - case basis . an alternative to stent - assisted coiling is balloon assistance that is a well - documented treatment option for wide - necked intracranial aneurysms and does not entail a prolonged double antiplatelet therapy [ 1 , 2 , 32 ] ; however , literature data are not uniform about the safety of this approach , and in the clinical practice , employing the balloon assistance depends frequently on the confidence of the interventionalist with this device . 
reported high complications rates with balloon - assisted embolization , suggesting to adopt this technique only when simple coil embolization is unfeasible [ 33 ] , while pierot et al . 
 [ 32 ] promoted the use of balloon assistance in ruptured aneurysms analyzing the data from the clarity series , concluding equivalent safety and better anatomic results compared to simple coiling . 1 3 radiol med ( 2017 ) 122 : 4352 this study presents several limitations ; the number of patients enrolled is too small to obtain definitive conclusions and further samples with more subjects involved are required . 
this article is published with open access at springerlink.com abstract background to evaluate the diagnostic performance of radiology residents interpretations for diffusion - weighted mr imaging ( dwi ) in the emergency department at different levels of residency training . method and materials a total of 160 patients who underwent dwi with acute neurologic symptoms were included in this retrospective study with an institutional review board approval . 
 retrospective data collection and analysis were performed according to our local institutional review board ( irb ) guidelines after its approval , and the irb determined that patient approval and informed consent were not required for reviewing images and records . background in the emergency department ( ed ) , patients with acute neurologic deficits are carefully evaluated for a timely diagnosis of intracranial abnormalities by performing neuroimaging studies , such as computed tomography ( ct ) and magnetic resonance ( mr ) imaging . 
we hypothesized that the relative inexperience of junior residents may lead to increased discordances of their interpretations and that the level of residency training may be related to the discordance rate . 
therefore , the purpose of this study was to retrospectively assess the rates of diagnostic discordances for dwi in ed between the interpretations of radiology residents and the final interpretations of an attending neuroradiologist . 
we also sought to evaluate the diagnostic performance of radiology residents at different levels of residency training . materials and methods study population a review of the database of our institution identified 297 consecutive patients who underwent dwi in the emergency department between september 2015 and december 2015 . 
of these 213 patients , 53 were excluded due to inadequate medical records ( n 24 ) ; poor image quality , including motion artifacts or susceptibility artifacts ( n 19 ) ; and inadequate diagnosis by only dwi ( n 10 )  . 
the final 160 patients imaging acquisition mr imaging was performed using a 3 - t system ( achieva ; philips medical systems , best , the netherlands ) with a 32 - channel head coil . 
our dwi protocol included the following sequences : axial dwi , axial fluid - attenuated inversion recovery ( flair ) , and axial t2 * - weighted gradient echo image ( gre )  . 
the parameters for t2 * - weighted gre were as follows : tr / te msec , 529 / 16 ; fov , 21 cm ; section thick193 ; number of slices , 24 ; and ness , 5 mm ; matrix , 324 acquisition time , 1 min 43 s . imaging analyses and reference standard in our institution , we had a total eight radiologic residents in the radiologic department . 
of these eight residents , four residents could not join in this study , because of a secondment for outreach education of interventional radiology , personal reason , and training schedule . 
at the time of this study , the 1st year resident completed one - half of her 1st year of training , had 2 months of neuroradiology experience interpreting both ct and mr imaging , and participated in neuroradiology teaching conferences , including staff lectures and interesting case presentations . 
discordance between the residents and staffs interpretations was classified as either false positive ( fp ; e.g. , misinterpreting normal images as abnormal ) or false negative ( fn ; e.g. , failure to diagnose 1 3 radiol med ( 2017 ) 122 : 3542 an abnormality )  . 
the rate of discordance was the highest for the 1st year resident ( 17.6 % ) , and the level of training had a significant influence on the diagnostic accuracy ( p < 0.05 ) ( table 3 )  . among residents with different years of training , the 4th year resident exhibited the highest diagnostic performance with the largest area under the roc curve table 2 concordances and discordances of diffusionweighted mr studies by level of training level of training correct diagnosis fp results fn results total no . 
therefore , many institutions have used dwi in combination with flair and t2 * - weighted gre as a timesaving substitute for routine brain mr imaging to make a timely diagnosis . 
 at most academic medical centers , physicians in the ed request urgent dwi studies for patients with acute neurologic deficits and radiology residents are often responsible for providing preliminary interpretations of those studies before the final interpretations of the neuroradiologist become available [ 1 ]  . 
however , the physicians need for rapid and accurate diagnoses of neuroimaging studies can conflict with the need for radiologic residents to acquire clinical experience and confidence [ 3 ]  . 
to maintain proper resident training , meticulous analyses of residents misinterpretations and discordances between residents and final interpretations are mandatory , because residents interpretations may impact patient management and treatment planning in the ed . in this study , we retrospectively assessed the rates of diagnostic concordances and discordances for dwi in ed between the interpretations of radiology residents and the final interpretations of attending neuroradiologist . 
although the discordance rate between the initial interpretations of head ct scans by ed physicians and the final interpretations by radiologists has been found to be nearly 39 % [ 7 ] , the discordance fig . 
a good degree of interobserver reliability was noted between all residents and attending neuroradiologist ( p < 0.0001 and table 4 )  . 1 3 radiol med ( 2017 ) 122 : 3542 fig . 
a , b small region of hyperintensity with equivocal adc change is noted in the right median portion of midbrathis finding represents a physiologic hyperintensity by anisotropy of the superior cerebellar peduncle rate of residents is much lower in this study . 
this discordance rate is higher than that reported by investigators who examined radiology residents interpretations of head ct scan or brain mr imaging studies below 5 % [ 1 , 2 , 813 ]  . 
 the discordance rate of our study is better than that previously reported for imaging modalities of other body sections , where disagreement rates as high as 26 % were reported for chest radiography [ 14 ]  . 
of a total of 8 residents , only 4 residents participated in this study due to their training schedule . consistent with the previous results [ 1 , 3 ] , we found that the discordance rate for the 1st year resident was significantly greater than those of 2nd , 3rd , and 4th year residents . 
 although individual differences exist , confident interpretation and decision - making is one of the most important educational and clinical experiences for radiology residents [ 1 , 14 ]  . of 160 cases , 14 fp findings with misinterpretations of acute focal infarction and focal hemorrhage were noted . 
in the case of acute focal infarction , the meticulous evaluation of the apparent diffusion coefficient map can be helpful to make an accurate diagnosis . in addition , our study showed good interobserver reliability between the interpretations of residents and attending neuroradiologist . 
this result suggests the possibility that the residents interpretations of dwi may be reliable in the patient with acute neurologic deficits who visit the ed before the final interpretations of the subspecialized neuroradiologist become available . 
d , e on contrast - enhanced axial ( d ) and sagittal ( e ) t1 - weighted images from the following day , the lesion exhibits homogenous enhancement , suggesting convexity meningioma or more experienced senior attending neuroradiologists are required . acknowledgments the authors would like to thank elsevier language editing service for the english language review and editing ; conclusion in conclusion , high - level residents exhibited a better diagnostic accuracy for interpreting dwi ordered from the ed compared with junior residents , and the level of resident training had a significant effect on their diagnostic performances . 
therefore , radiology residents can safely provide interpretations of dwi requested by the ed , and efforts to focus on detecting small lesions can be helpful to reduce residents errors . authors contributions concept and design : hjb , kb , dsc , dwk . 
final approval : all authors read and approved the final manuscript . availability of data and materials the data set supporting the conclusions of this article is available by email of corresponding author . conflict of interest all authors declare that they have no conflict of interest . conflicts of interest statement and funding the authors declare that they have no competing interests . 1 3 42 radiol med ( 2017 ) 122 : 3542 consent for publication written informed consent was obtained from the patient for publication of this study and accompanying images . 
a copy of the written consent is available for review by the editor - in - chief of this journal on request . ethical approval and consent to participate this was purely an observational retrospective study . 
to detect an ris at an earlier stage , the radiologist should be aware of the common radiological appearances , which can be scrutinized on follow - up scans . the purpose of this study was to document the clinical findings and the radiological features on computed tomography ( ct ) and magnetic resonance imaging ( mri ) of ris in the head and neck following rt for npc . radiotherapy ( rt ) is the curative treatment modality for nasopharyngeal carcinoma ( npc ) , which is a common tumor in the southern chinese population . 
compared with post - radiation squamous cell carcinoma ( scc ) [ 1 ] , radiation - induced sarcomas ( ris ) of the head and neck following rt for npc are even less materials and methods patients q . 
 patients with ris in the head and neck following rt for npc identified from a review of the histological and radiological results from december 1998 to september 2012 met the inclusion criteria . 
 [ 10 ] : a prior history of rt ; the occurrence of a sarcoma within the previously irradiated field ; a latency between irradiation and the second primary sarcoma of at least 3 years ; histologically proven sarcoma arising within the irradiated field . 
one of the co - authors engaged in the pathological 1 3 54 radiol med ( 2017 ) 122 : 5360 table 1 patient characteristics at diagnosis of nasopharyngeal carcinoma ( n 69 ) no . 
the fat - suppression technique was used for the gadoliniumenhanced t1 - weighted coronal images in 15 patients . among the 69 patients , 41 cases underwent ct examination only , 21 cases mri only , and the remaining 7 cases both ct and mri scans . 
in this study , the primary nasopharyngeal tumors were treated with a dose of 4090 gy with the average dose of 68.7 gy , and the neck received 3770 gy with the average dose of 57.7 gy , depending on the lymph nodes involvement . ct and mri examinations a 16 - slice spiral ct ( brilliance tm 16 , philips medical systems , the netherlands ) or a dual - slice ct ( twin flash , philips medical systems , the netherlands ) was used for multiphasic ct scans ( i.e. , nonenhanced phase , arterial and venous phases )  . 
other parameters were as follows : section thickness , 5 or 10 mm ; gap , 5 or 10 mm ; tube current , 250 ma ; and tubular voltage , 125 kv . 
the contrastenhanced ct scanning was performed after an intravenous injection of iopromide at a dosage of 1.5 ml / kg of body weight ( ultravist 300 , schering , germany )  . the mri was performed using a 1.5 t superconductive unit ( signa horizon lx highspeed , general electric medical systems , usa ) with a head coil and a neck coil or a combined head and neck coil . 
the sequences included spin 1 3 radiol med ( 2017 ) 122 : 5360 results patients a total of 69 patients ( from 27714 patients ) with histological evidence of ris were enrolled , including 46 men and 23 women with a ratio of 2 : 1 . 
among them , 42 patients presented with well - marked mass in the maxillofacial region and neck accompanied by pain of certain degrees , 7 patients with serious loss of vision and 20 patients with nasal obstruction and / or bleeding similar to the symptoms of primary npc . the average latency period from the end of radiation therapy to the diagnosis of ris was 10.8 years ( range 337 years )  . 
most of ris ( 44.9 % ) occurred at 510 years after rt , and up to 87.0 % of ris developed within table 2 the latency period from the end of radiation therapy to the diagnosis of radiation - induced sarcomas ( n 69 ) no . 
the median latency of ris originating in the maxillofacial region and in the neck was similar , at 10.8 years with a range of 337 and 519 years , respectively . imaging features the main characteristic of the 69 ris on ct and mri was soft tissue mass formation . 
 all the sarcomas in this study occurred at sites , while in the irradiated field , away from the margins of the original tumor of npc and the metastatic lymph nodes . 
a axial contrast - enhanced ct image showed a large heterogeneous tumor in the right maxillary sinus invading the nasal cavity ( arrows ) ; b axial t2 - weighted image showed heterogeneously high t2 signal intensity of the tumor ; c coronal t1 - weighted contrast - enhanced image showed the mildly enhanced tumor with wide invasion into the right maxillary region ( arrows ) fibrosarcoma ( n 12 ) , respectively . 
all of the other 10 patients who received chemotherapy only ( n 1 ) or chemoradiation ( n 8 ) , rt only ( n 1 ) had uncontrolled lesions . discussion patients with npc treated with radiotherapy are at risk of developing radiation - induced sarcomas in the irradiated fields . 
in this study , we retrospectively reviewed the clinical and ct / mri features of ris , and the results showed that ris was very aggressive and had poor prognosis for most cases . 
here , one thing to say is that among the 69 patients enrolled in this study , 54 had been documented focusing on the locations and histological subtypes of ris in one of our previous studies [ 2 ]  . we acknowledge that not all sarcomas that arise after rt are induced by radiation , so do the cases in our study ; but it is impossible to differentiate ris from primary sarcomas . 
ris in this study arose as a late complication of radiotherapy at an average latency period of 10.8 years , which was in agreement with the previously reported latency periods ranging from 8.8 years to 1 3 radiol med ( 2017 ) 122 : 5360 fig . 
axial contrast - enhanced ct image showed a large heterogeneous tumor , with a large amount of tumor bone formation , arising from the right mandibular ramus destroying the right masseter muscle and medial pterygoid muscle ( arrows ) 12.4 years [ 13 , 13 ]  . 
but it should be noted that intensive follow - up is not necessary ; patients just need to comply with the prescribed periodic follow - ups for npc by radiation oncologist ; and we radiologists should carefully scrutinize the scans , especially the irradiated field , to avoid missing any potential ris lesions . ris had a predilection for arising in the high - radiationdose region , and it is known that a total dose of 55 gy or above increases their risk [ 1 , 14 ] ; our results supported the published findings . 
patients undergoing a full course of rt for npc received an average dose of about 68.7 gy to the nasopharynx in this study , thus putting the surrounding bones and soft tissues at risk of ris . 
in this series , the most common origin site of ris was the maxillary region , which encompasses at least the posterior half of the maxillary sinus and adjacent nasal cavity receiving almost the full radiation dose ; and followed by the neck which received an average dose of about 57.7 gy with lymph node0 fig . 
axial t1 - weighted contrast - enhanced image ( a ) and coronal fat - suppressed t1 - weighted contrast - enhanced image ( b ) showed a large heterogeneously marked enhanced tumor of the right mandibular ramus with bone destruction and wide invasion into the muscles ( arrows ) involvement . 
this highlighted the importance of inspecting the previously irradiated fields , especially the high - radiation - dose regions , on ct and ( or ) mri follow - up scans to improve early detection of ris . despite the small number of cases in this study , a wide variety of sites and subtypes of ris were seen . 
axial contrast - enhanced ct image showed a large heterogeneously marked enhanced tumor with wide invasion into the muscles in the right lower neck ( arrows ) the patients from january 2000 to december 2011 had been reported by cai et al . 
patients in this study were collected from december 1998 to september 2012 ; additionally , we summarized the treatment and outcomes of ris in our institution , some of the patients included in the previous study had been excluded in this study owing to missing clinical data or treated in other institutions . 
most sarcomas in the series were large with extensive local invasion at the time of ct or 5 cthis is partly because mri , 30.4 % of which were they are very aggressive tumors that often grow rapidly . the clinical diagnosis of ris in the head and neck can be difficult because of induration and fibrosis within the irradiated field ; this was also part of the reasons for the late diagnosis of most ris . 
prompt investigation based on the patients symptoms , especially the appearance of or a change in the character of , pain or a mass in the irradiated area several years after rt , could lead to an early diagnosis . 
heterogeneous soft tissue masses with large size , extensive local invasion and ( or ) bony destruction in the irradiated fields on imaging examinations are the main clues to the diagnosis of ris ; if possible , histopathological results are needed . most ris in the series were advanced at diagnosis , leading to a poor prognosis . 
apart from eight patients having missing follow - up , 88.5 % of patients had recurrent or uncontrolled lesions exactly at the original site of ris , which was consistent with data from other studies [ 13 , 1618 ]  . 
axial contrastenhanced ct image ( a ) showed a large heterogeneously marked enhanced tumor in the nasal cavity and left maxillary sinus ( arrows ) ; axial ct on bony window ( b ) of bone destruction not resectable because of their deep - seated location , close to vital structures , and advanced stage at the time of diagnosis . 
 besides , sarcomas did not respond well to rt or chemotherapy [ 3 , 4 , 17 ] ; ris receiving rt or ( and ) chemotherapy only in this study showed worse results of persistent lesions . 1 3 radiol med ( 2017 ) 122 : 5360 table 4 subgroup comparison of radiological findings between osteosarcoma and fibrosarcoma histology no . 
site extent margin definition bone destruction bone formation density / signal intensity un / enhanced tumor yes no ill well yes no yes no heterogeneous homogeneous osteosarcoma 24 maxillary sinus and mandibular ramus fibrosarcoma 22 neck , maxillary sinus and mandibular ramus 14 21 3 16 6 the most common sites table 5 treatment and outcomes of radiation - induced sarcomas ( n 69 ) outcomes treatment surgery chemotherapy radiotherapy ( rt ) surgery therapy chemosurgery chemoradiation no treatment no . 
secondly , it is acknowledged that some of the carcinomas may have been the second primary tumors rather than ris , although our arguments for believing they are related to radiation have been discussed . 
it is possible that imrt with the delivery of a higher integral dose and also the additional effect of chemotherapy ( neoadjuvant and / or concurrent chemotherapy ) in some patients may also impact on the risk of developing ris . 
82.5 % had a favorable outcome ( gos : ivv ) , while 17.5 % presented a poor score ( gos : iiii )  . conclusions stent - assisted coil embolization is a feasible endovascular treatment option for ruptured intracranial aneurysms , which is difficult to approach with simple coiling ; however , neurointerventionalists need to consider a mild increase of post - procedural complications rate . inclusion criteria were the presence of acute sah on computed tomography ( ct ) and stent - assisted embolization . 
exclusion criteria included previously treated aneurysms , evidence of dissecting aneurysms or pseudoaneurysms , and contraindication to antiplatelet therapy . data were collected from electronic or physical charts , and angiography . all protocols were reviewed and approved by the institutional review board of each center independently in accordance with the declaration of helsinki principles . keywords stent coiling ruptured aneurysm cerebral acute population data introduction the endovascular embolization of intracranial aneurysms has emerged as a viable and sometimes a preferable method of treatment of intracranial aneurysms [ 1 ]  . 
however , endovascular treatment of wide - necked aneurysms represents still a challenge to neurointerventionalists because of the risk of coils protrusion from the aneurysm into the parent artery [ 2 ]  . assisted techniques with balloons have been developed to obtain a safe coil packing into the sac in these wide - neck lesions . 
there is a reluctance to use intracranial stents during the acute post - hemorrhage period because of the risk of thromboembolic complications in patients who are not pre - treated with antiplatelet therapy , and the fear that using antiplatelet agents in the post - rupture period may increase the risk of re - bleeding or peri - procedural complications related to placement of ventriculostomies [ 3 ]  . balloon remodeling has provided an alternative to intracranial stents especially since it can be used without antiplatelet therapy [ 4 , 5 ] ; however , there is a concern that balloon remodeling is not always the ideal choice of treatment for all wide - necked aneurysms [ 68 ]  . the purpose of this study is to report on a multi - center experience of ruptured intracranial aneurysms treated in acute phase with stent - assisted coil embolization , including primary success rates and midterm follow - up results . materials and methods this is a retrospective study to analyze radiological and clinical outcomes from all patients with ruptured wide - neck intracranial aneurysms treated with stent - assisted coiling . the neurointerventional database was screened for patients presenting with subarachnoid hemorrhage ( sah ) treated in neurointerventional radiology departments during the same hospitalization at three high - volume centers between 2010 and 2014 . a sample of 40 patients was involved in this analysis ( table 1 )  . 
there were 14 men ( 35 % ) and 26 women ( 65 % ) with a mean age of 59.7 years ( range 2984 years )  . the angiographic characteristics of the ruptured aneurysms are provided in table 1 ; on the basis of angiogram or three - dimensional reconstructions , location , dome size , and neck / dome ratio were recorded . 
surgical treatment was usually preferred for anterior circulation aneurysms , when the patients had a large parenchymal hematoma and were very young . in all cases , before the procedure , patients underwent to non - enhanced ct ( nect ) , angio - ct , and digital subtraction angiography ( dsa )  . the duration of angiographic follow - up considered for this analysis was 1 year ( 030 months )  . the protocol included a first follow - up visit with angiographic control study performed at 36 months with mr and angio - mr , depending on the primary result of the endovascular treatment . 
 extended imaging follow - up was tailored to the individual patient . additional coiling was scheduled in cases in which the aneurysm was reopened by coil compaction or resolution of intraluminal thrombus . technique the embolization procedures were performed by experienced interventional radiologists ( 325 years of experience ) , always with patients under general anesthesia . 
coils were deployed using the jailing technique ( releasing the stent after positioning the microcatheter into the aneurysm sac ) or the coil - through technique ( first releasing the stent and then positioning the microcatheter into the aneurysm sac passing through the stent interstice )  . in addition , if the stent was placed after initial - unassisted embolization or balloon - assisted embolization , it was defined as a bailout procedure , and the reason for placement of the stent ( e.g. , instability of coils pack ) was noted . anticoagulation protocol all patients were treated with heparin during the procedure . 
clinical consequences of thromboembolic complications were recorded . the primary occlusion rate was classified as total occlusion ( > 95 % occlusion rate ) , neck remnant ( > 80 % occlusion rate with contrast medium filling only the neck area of the aneurysm ) , partial occlusion ( distal filling of contrast medium in the aneurysm regardless of the occlusion rate ) , or none ( unsuccessful coiling ) [ 9 ]  . 
angiographic occlusion was considered to be adequate if either complete occlusion of the aneurysm or a small neck remnant with over 80 % occlusion was achieved . endovascular treatment was considered to be technically successful if the deployed stent extended at least 5 mm over the aneurysm neck on both sides of the aneurysm and adequate angiographic occlusion was achieved [ 9 ]  . 
all technique - related major complications were considered to constitute technical failures , regardless of angiographic outcome . the sah was pre - operatively radiologically classified on the basis of nect , according to the fisher score . the pre - operative clinical condition of the patients was evaluated using the hunt and hess classification , and the clinical outcome was independently measured by experienced neurosurgeon / neurologists using the glasgow outcome scale ( gos ) [ 10 ]  . statistical analysis nect was performed in all cases immediately after the procedure in order to assess new hemorrhages related to the coiling ; then , according to the ongoing clinical conditions , other ct or magnetic resonance ( mr ) scans were acquired on demand . all data analyses and statistical tests were performed in matlab environment ( mathworks , inc , natick , massachusetts )  . 1 3 46 results two - thirds of the patients were women ; 20 % of the aneurysms were located in the posterior circulation . 
of the 40 aneurysms , 42.5 % were located in the carotid syphon , 20 % in the anterior communicating artery , 12.5 % in the middle cerebral artery , 12.5 % in the basilar artery , 5 % in the posterior communicating artery , 5 % in the anterior cerebral artery , and 2.5 % in the vertebral artery ( table 1 )  . the mean size of the sac was 7 mm ( range 322 mm ) ; 55 % were small ( < 7 mm ) , 35 % medium ( 713 mm ) and 10 % large ( 1424 mm )  . 
in the other 80 % , stent positioning was planned : of this , 50 % was performed with the jailing technique and 50 % with the coil - through technique . 
 the stents adopted for coil assistance are reported in table 2 : the most employed device ( 65 % ) was the enterprise stent ( codman )  . from a technical point of view , the stent deployment was always successful ( 100 % )  . 
in all cases , a nect was performed at the end of the embolization , and no cases of increase of the sah were observed . no intra - procedural re - bleeding occurred ; however , in 12.5 % of the cases , a minor re - bleeding was detected in the first 3 weeks after the procedure , and these were just monitored and not treated because they were reabsorbed earlier , while clopidogrel was suspended for 5 days . 
 hydrocephalus developed in 15 % ( 6 patients ) ; in one case , double antiplatelet therapy was interrupted in order to insert an external drainage . the long - term follow - up showed 25 % of the patients with vessel stenosis documented at the 1 - year dsa of control . 
in six patients ( 15 % ) , the 36 months of follow - up , confirmed by subsequent dsa , revealed aneurysm refilling , 4 involving the sac and 2 only the neck ; in the first group , a new endovascular treatment had been successfully performed . the clinical status was recorded during the hospital recovery after the procedure has been analyzed . 
the stent action is twofold : it serves as a scaffold for the placement of coils enabling dense aneurysm packing [ 15 ] , and it reduces the rate of aneurysm recanalization by redirecting the blood flow reducing the intra - aneurysmal flow [ 16 , 17 ] and promoting the endothelialization at the level of the aneurysm neck [ 18 ]  . 1 3 47 radiol med ( 2017 ) 122 : 4352 fig . 
a nect showing massive sah ; b angio - ct detecting a small aneurysm ( 4 mm ) of left va associated with a fenestration of the origin of ba ; c volume rendering postprocessing ; d dsa anteroposterior projection confirming angio - ct findings ; e release of enterprise stent extending from left va to the ba ; f final dsa run anteroposterior projection confirming aneurysm exclusion after coiling . 
clinical outcome was favorable with a gos 14 at the end of the hospital stay ; no complications occurred during the recovery and long - term follow - up in recent years , stent - assisted coiling has been proposed also for acutely ruptured aneurysms [ 9 , 19 ] : indeed , early treatment of ruptured aneurysms is recommended because of the high risk of subsequent re - rupture [ 20 , 21 ] , and in this scenario , treatment decision is more challenging , especially for wide - neck lesions where stent assistance represents an important addition to the treatment repertoire [ 9 ]  . however , it must be considered that the reported complication rate of stent - assisted coiling with early adverse events in ruptured aneurysms is 10 times higher than that in 1 3 radiol med ( 2017 ) 122 : 4352 fig . 
a angio - ct with maximum intensity projection reconstruction showing a wide - neck small aneurysm of the right carotid syphon ( black arrow ) ; b dsa anteroposterior projection confirming angio - ct findings ( white arrow ) and detecting also the origin of the posterior communicating artery from the neck ( red arrow ) ; c remodeling technique with balloon - assisted embolization : white arrow indicates the tip of the microcatheter into the sac , and the white circles show the markers of the balloon ; d migration of a coil into the vessel lumen despite the balloon ; e bailout stenting ( enterprise ) to contain the coils into the sac ; f final dsa control demonstrating sac exclusion , patency of the carotid syphon and of the posterior communicating artery . 
followup with 3 - month angio - mr and 1 - year dsa confirmed the good procedural success with good clinical table 2 technique and stents adopted technique 80 % planned 20 % bailout 40 % jailing 40 % coil - through enterprise 65 % stent neuroform 25 % solitaire 15 % unruptured aneurysms , with early re - bleeding accounting for most mortality [ 22 ]  . 
a nect showing diffuse sah ; b angio - ct with volume rendering reconstructions showing a small blister aneurysm ( 3 mm ) of right carotid syphon ; c dsa lateral projection confirming angio - ct findings ( arrow ) ; d stentassisted embolization with enterprise stent ( circles ) and coiling ; e post - embolization dsa in lateral projection showing total occlusion of the carotid syphon ( star ) ; f dsa lateral projection showing complete flow restoration after abciximab infusion ; g 2 - week nect follow - up showing resolution of the sah ; h 1 - year follow - up dsa lateral projection showing complete aneurysm exclusion with minor stenosis of the carotid syphon in correspondence of the stent . 
clinical outcome was favorable with a gos 14 at the end of the hospital stay ; no complication occurred during the recovery and long - term follow - up this is mainly related to the double antiplatelet therapy required to avoid stent occlusion ; indeed , sah is itself a hypercoagulable status , and in this setting , a stent is highly thrombogenic for the parent vessel until the stent has been endothelialized [ 24 ] ; hence , post - stenting double antiplatelet therapy ( i.e. , clopidogrel and acetylsalicylic acid ) is essential ; however [ 9 ] , acute sah represents a contraindication to these drugs for the risk of re - bleeding . 
 [ 26 ] concluded that complications of stent - assisted coiling for ruptured intracranial aneurysm can be affected by the method of antiplatelet administration . in literature , the overall stent assistance embolization procedure - related complication rate , including both hemorrhagic and thromboembolic complications , is approximately 13 % [ 23 ] , which is higher than reported complication rates in stent - assisted coiling of unruptured aneurysms , which are in the range of 67 % [ 27 , 28 ] .of particular concern is the risk for hemorrhage in patients who require evd placement or conversion of evd to a permanent shunt , given the need for ongoing antiplatelet therapy . 
the data reported in this study in terms of overall complication rate and clinical outcome are in accordance with literature published data [ 19 , 23 ]  . 1 3 50 radiol med ( 2017 ) 122 : 4352 fig . 
a nect showing mild sah located in the basal cisterns and left silvian scissure ; b rotational dsa with 3d post - processing showing an aneurysm of the anterior communicating artery with a posterior bleb , both a2 origin from the sac ; c stentassisted coiling after positioning an enterprise stent in a1 - a2 left ; d stent thrombosis ( white circle ) , e solved by intra - arterial infusion of abciximab ( reopro 5 ml ) and balloon angioplasty ; f final dsa control showing bilateral patency of a2 and sac exclusion with a minimal perfusion of the neck ; g post - procedural nect showing no re - bleeding in neither ischemic area ; h rotational dsa with 3d postprocessing 7 months after embolization showing patency of both a2 , no signs of stent thrombosis , minimal perfusion of the neck and sac exclusion in this series , the mostly used stent was the enterprise stent . 
 [ 29 ] in their review compared enterprise and neuroform for stent - assisted coiling and observed that deployment failures , intracranial hemorrhage , mortality among all patients , and recanalization were more commonly reported in neuroform - treated aneurysms , while the enterprise was associated with higher reported complete occlusion at follow - up ; they concluded that both devices are safe and effective with comparable permanent morbidity . 
these features of enterprise stent demonstrate that it is easier to deploy than the opened - cell stent and enable the treatment of additional aneurysms [ 30 ] ; the closed - cell design stent has a greater tendency to slightly alter normal vascular anatomy owing to its design . 
delivery of the open - cell design neuroform stent to more distal vessels may be more difficult as it requires the use of a 0.027 diameter microcatheter rather than the 0.021 diameter microcatheter used to deliver the closed - cell design enterprise stent . 
nevertheless , it is important to underline that navigation of either microcatheters occurs in very small vessels , and this circumstance itself already demands a certain level of expertise [ 31 ]  . 
the use of either the enterprise or neuroform stent is at the discretion of the treating neurointerventionalist , and the decision is made on a case - by - case basis . an alternative to stent - assisted coiling is balloon assistance that is a well - documented treatment option for wide - necked intracranial aneurysms and does not entail a prolonged double antiplatelet therapy [ 1 , 2 , 32 ] ; however , literature data are not uniform about the safety of this approach , and in the clinical practice , employing the balloon assistance depends frequently on the confidence of the interventionalist with this device . 
reported high complications rates with balloon - assisted embolization , suggesting to adopt this technique only when simple coil embolization is unfeasible [ 33 ] , while pierot et al . 
 [ 32 ] promoted the use of balloon assistance in ruptured aneurysms analyzing the data from the clarity series , concluding equivalent safety and better anatomic results compared to simple coiling . 1 3 radiol med ( 2017 ) 122 : 4352 this study presents several limitations ; the number of patients enrolled is too small to obtain definitive conclusions and further samples with more subjects involved are required . 
the aim of this review is to analyse the spectrum of radiological signs as reported in the recent literature , in light of our series over a 15 - year period , to pinpoint the most common radiological patterns in a developed country and to determine the role played by the different chest imaging techniques in diagnosis improvement . 
in 21 cases with lymphadenopathies without lymph - bronchial diffusion ( age range 2 months7 years ) , ct identified the ghon focus in 16 / 21 cases ; chest x - ray never identified the ghon focus . 
in our series , pleural tb was present in 8 cases out of 146 under 5 years of age , 5 cases out of 76 under 2 years , and 18 cases out of 71 over 5 years . 
radiologists should be aware of typical patterns of tuberculosis , to provide an early diagnosis . keywords tuberculosis chest ct children chest radiography mri * paolo tom paolo.toma@opbg.net 1 department of imaging , bambino ges children hospital , irccs , rome , italy 2 paediatrics and infectious disease , bambino ges children hospital , irccs , rome , italy introduction the incidence of tuberculosis ( tb ) is increasing in the developed world and children in particular represent a high - risk group for developing the disease [ 13 ]  . 
computed tomography ( ct ) is currently the most accurate tool available for chest imaging . the aim of this review is to analyse the spectrum of radiological signs as reported in the recent literature , in light of our series of 217 / 255 cases of lung tb over a 15 - year period , to pinpoint the most common radiological patterns in a developed country and to determine the role played by the different chest imaging techniques in diagnosis improvement . natural history demonstrates that age is the critical variable influencing the risk that primary m . 
 an infant is at the highest risk , and then , the risk drops but remains significant in the second year of life , to reach its lowest level in infected children aged between 5 and 10 years of age . 
for more than 50 % of children developing the disease , the onset is within 1 year from the primary infection , therefore , children aged less than 2 years , and / or immunocompromised children can reasonably be considered as a high - risk group [ 4 ]  . the immune mechanisms of the adult - type disease are ambiguous , but it is a noticeable observation that it occurs only as children enter into puberty . 
it is crucial to recall that children with adult - type disease are frequently sputum smear positive and that they do represent a factor of disease transmission , mostly in agglomerations , such as schools [ 5 , 6 ]  . the diagnosis of childhood tuberculosis presents a major challenge , as it is complicated : bacteriological confirmation is often inadequate for children because of the paucibacillary 1 3 radiol med ( 2017 ) 122 : 2234 fig . 
on the left , the ghon focuses ( black empty arrow ) not identified by the plain radiographs character of their disease : the poor bacteriologic specimen [ 7 ] and cultures are positive only in 2550 % of cases . 
contrariwise , samples are elevated in children with adult - type disease , and sputum smear microscopy can adequately assess infectious pulmonary tuberculosis in older children ( more than 10 years of age ) [ 9 ]  . the diagnosis of childhood tuberculosis in no endemic areas is usually based on : 1 . 
actually , normal chest x - ray does not rule out tb , as it is negative in 15 % of cases of proven tb [ 1014 ]  . one of the biggest problems in comparing data is related to the poor inter - observer agreement in the diagnosis of primary tb in children using chest x - rays and , more generally , to the selection and description of radiological signs of lung infections in children . 
the readout array , to which the phosphor is coupled , consists of a 43 cm 43 cm amorphous silicon ( a - si ) photodiode and a thin - film transistor ( tft ) array ( 0.143 mm pixel pitch )  . from 2000 to 2010 , ct scans in our hospital have been performed with a somatom plus scanner ( siemens , erlangen , germany )  . 
sedation , however , was required for uncooperative children . from 2010 to date , we have been using a second - generation dual source ct system ( siemens somatom definition flash , siemens erlangen , germany ) with two x - ray tubes and two detectors settled at an angular offset of 95 . 
with the old scanner , contrast was administered by hand injection . at present , we normally use an automatic injector ( stellant , medrad , inianola , usa ) with the following parameters : 1 ml / s for 24 - gauge catheters ( rarely and with the greatest caution ) , 1.52.0 ml / s for 22 - gauge catheters , and 23 ml / s for 20 - gauge catheters , with a pressure limit adjusted to a maximum of 150 psi ( 1034 kpa )  . 
the ct volume data were collected from the thoracic inlet level to the diaphragm level , and were transferred and analysed in pacs ( kodak - carestream healthcare )  . the radiation doses we administered are within the limits of the proposed european diagnostic reference levels for pediatric ct [ 16 ]  . 
lung tb was present in 217 out of 255 patients ( 85 % ) : 146 patients were under 5 years of age ( 76 under 2 years ) and 71 over 5 years ( 41 over 10 years )  . the diagnosis of tuberculosis was established by the detection of three or more of the following elements : ( 1 ) clinical presentation ( symptoms or signs ) ; ( 2 ) contact history ( household and close contacts ) ; ( 3 ) purified protein derivative ( ppd ) tuberculin skin test and igra test ; ( 4 ) chest radiography and ct ; ( 5 ) bacteriological examination ( including examination of sputum , tuberculous pleural effusion , bronchoalveolar lavage , gastric aspirates , cerebrospinal fluid , and peritoneal fluid ) ; ( 6 ) bronchoscopy ; and ( 7 ) biopsy if necessary . 
following the gold standard , the diagnosis of tb was confirmed when mycobacterium tuberculosis ( mtb ) was isolated . in our series of patients , chest x - rays were obtained from 2000 to 2003 with the conventional screen - film radiography ( sfr )  . 
in 2003 , the sfr system was replaced with a computed radiography ( cr ) syste in 2010 , a siemens ysio direct radiography ( dr ) system with a flat panel detector ( siemens , erlangen , germany ) was also introduced . 
in the discussion of diagnostic procedure radiation doses , comparison to more familiar radiation exposures ( such as chest x - rays or natural background radiation ) has been recommended to facilitate the understanding of the dose . 
the dose delivered during a chest x - ray is so low that using it as denominator to estimate the equivalent number of chest x - rays comparable with the level of dose of any other radiological technique may be misinforming and may unreasonably alarm patients and parents [ 22 ]  . in the future , mri could substitute ct mainly in the evaluation of mediastinal lymphadenopathy . 
about the drawbacks for mri of the lung , two of these tissue properties are of the highest 1 3 26 radiol med ( 2017 ) 122 : 2234 importance : the low proton density and the susceptibility differences between tissue and air . 
the respiratory and cardiac movements that cause a decrease of temporal resolution represent another peculiar aspect [ 25 , 26 ]  . rarely , in < 2 years of age or immune compromised children , the ghon focus can evolve directly into consolidation with intra - bronchial spread and bronchopneumonic consolidation [ 27 ]  . imaging findings children are different in size , anatomy , and physiology compared to adults . 
we will describe different patterns differentiating infants and children from adolescents and young adults ( table 1 )  . infants and children we have adopted the radiological classification of tb proposed by marais [ 15 , 27 ]  . 
following this classification , we have distinguished four main entities : lymph node tb ( lymphobronchial tb ) ; air - space parenchymal tb ( consolidation / atelectasis ) ; miliary tb ; pleural tb . the ghon focus is a localized pneumonic process , referred to as the primary parenchymal focus , limited at the site of organism deposition . 
one case ( 7 years ) had a lymph - bronchial disease ( see below )  . younger children , due to their anatomical size , have also narrower airways with less supportive cartilage , making them more compressible . 
in synthesis , complicated lymph node disease includes compression , erosion , ulceration , infiltration , intra - bronchial passage of caseous material , and formation of granulation tissue ( adenobronchial fistula )  . adolescents and young adults absence of lymphadenopathy air - space parenchymal tb cavitation ( 45 % ) bronchogenic spread linear branching opacities tree - in - bud tuberculomas pleural tb consolidation / atelectasis segmental / lobar distribution predilection for the upper lobes lower and middle lobe predominance 1 3 radiol med ( 2017 ) 122 : 2234 in fact , indications for completing the survey with ct after contrast medium are not standardized . ct is useful in clinics , especially for children aged under 2 years , for whom the conventional chest x - ray is often insufficient . 
ct allows to see a mixture of both sharply and poorly defined , 14 mm nodules , in a diffuse , random distribution often associated with intraand interlobular septal thickening . 
the axial view shows unilateral lymphadenopathies ( white arrow ) , peripheral ghon focus ( black empty arrow ) , and lymphangitis ( c ) 1 3 28 radiol med ( 2017 ) 122 : 2234 fig . 
six months later small - calcified foci ( white arrows ) in hilar and mediastinal lymph nodes and in the consolidation ( b , c ) chest x - ray may be normal at disease onset ( 2540 % )  . 
pleural effusion is often unilateral [ 15 ]  . pleural involvement occurs after direct spread of caseous material from a sub - pleural parenchymal or lymph node focus , or from haematogenous spread . 
usually , it represents a hypersensitivity response , but tuberculous empyema rarely develops , depending on the quantity and virulence of bacilli entering the pleural space and on the immune status of the host [ 27 ]  . 
us is crucial in the detection and in the structure evaluation and guiding a pleural tap . pericardial effusion usually develops when a subcarinal lymph node erupts into the pericardial space [ 6 ]  . 
sometimes , the infection causes a thickening of the pericardium without an effusion , and this can also constrain the pumping action ( constrictive pericarditis ) [ 35 ]  . 
traditionally , it refers to both reinfection and reactivation of tb , but the age - related distinction has changed , because primary infection can occur at any age ( especially in countries with low tb incidence )  . 
exogenous reinfection is typical of endemic areas and distinguishing the features of post - primary tuberculosis area predilection for the upper lobes and the absence of lymphadenopathy and cavitation [ 32 ]  . 1 3 radiol med ( 2017 ) 122 : 2234 fig . 
lymphadenopathies with the rim sign : low - density centre and enhancing rim ( white arrows ) tb manifest as parenchymal disease ; airway involvement ; pleural / pericardial extension . parenchymal disease consolidations are typical also of the adult - type disease that first occurs around 810 years of age and becomes the common aspect of the disease during adolescence . 
complications include cavity development and intra - bronchial spread [ 6 ]  . cavity is a gas - filled space within a zone of pulmonary consolidation or within a mass or nodule , produced by the discharge of the necrotic part of the lesion via the bronchial tree [ 32 ]  . 
on the right , the external compression of the bronchus intermedius ( black arrow ) with atelectasis and bronchiectasis of inferior and middle lobe and hyperinflation of the right upper lobe 1 3 30 radiol med ( 2017 ) 122 : 2234 fig . 
compression of the right upper bronchus by tuberculous lymph nodes and consolidation of the upper lobe with the areas of necrotic liquefaction and shift of the mediastinum ( ac ) fig . 
consolidations in the apical and posterior segments of the upper lobe and the apical segment of the left lower lobe with cavities inside ( a , b ) defined margins , and often demonstrate calcifications ( 20 30 % of cases )  . 
satellite nodules around the tuberculoma may be present in as many as 80 % of cases [ 1315 , 32 ]  . airway involvement bronchogenic spread is detected in 95 % of the cases by ct [ 13 , 14 ]  . 
branching nodular and linear opacities ( tree - in - bud ) and centrilobular nodules ( a , b ) disease activity the literature [ 32 , 38 ] reports ct signs of disease activity , which can be summarized as follows : tree - in - bud appearance , clustered nodules , lobular consolidations , thick - walled cavities , rim - enhancing nodes ( short axis > 1 cm ) , and pleural effusion . 
contrast - enhanced ct scan shows the results of a bronchogenic spread ( mainly on the right upper lobe ) with consolidations , several cavities , and centrilobular small nodules ( a )  . 
camillo hospital , circonvallazione gianicolense , 87 , 00152 rome , italy 5 diagnostic and interventional radiology unit , department of health sciences , university of milan , via a . 
no major complications were registered . conclusions a short - term patency benefit may be obtained including pcb in angioplasty treatment of failing hemodialysis arteriovenous shunts . keywords paclitaxel - coated balloon outflow stenoses hemodialysis arteriovenous shunt introduction vascular access complications are one of the main causes associated with an increase in morbidity and mortality in stage 5 chronic kidney disease patients [ 1 ]  . despite the relatively low arteriovenous fistula ( avf ) thrombosis rate , existing guidelines advocate surveillance programs for early detection of stenosis and its correction before thrombosis occurs , to reduce morbidity and prolong access patency [ 2 ]  . the pathophysiology of stenosis of hemodialysis access is complex . 
these mechanisms seem to be similar in autogenous and prosthetic vascular access [ 1 ]  . the main purpose of vascular access monitoring and surveillance programs is the early identification of stenosis , because it is the main cause of avf dysfunction and thrombosis . the nkf - k / doqi guidelines for vascular access recommend the use of vascular adequacy parameters and 1 3 70 radiol med ( 2017 ) 122 : 6976 physical examination for monitoring avf and av grafts ( avg ) [ 2 ]  . in - graft at the venous anastomosis and in the outflow vein in the synthetic av fistula ( table 1 )  . the nfk - k / doqi guidelines recommend that each dialysis center should determine which procedure for the correction of stenosis [ percutaneous transluminal angioplasty ( pta ) or surgery ] is best for the patients , based on the expertise of the center [ 2 ]  . nowadays , endovascular intervention in the form of balloon angioplasty may be considered a safe and effective treatment for failing avfs and avgs . 
re - stenosis is common and angioplasty may be easily repeatable [ 3 ]  . access stenosis should be treated if stenosis is 50 % and is associated with abnormalities such as previous thrombotic episodes , elevated intra - access pressure ( iap ) , abnormal recirculation , abnormal physical signs , unexplained decrease in adequacy dialysis parameters , and decreased blood flow [ 2 ]  . 
the procedure is classified as successful if there is less than a 30 % residual lesion according to nfk - k / doqi [ 2 ]  . a paclitaxel - coated balloon ( pcbs ) provides rapid delivery of the antiproliferative drug to the local vessel wall and inhibition of neointimal hyperplasia compared with plain balloon ( pb ) [ 5 , 6 ]  . 
however , there are few studies in the literature supporting the use of pcb for endovascular management of hemodialysis ( hd ) access vascular stenosis [ 6 ]  . as few other authors [ 68 ] , we hypothesized that combining coronary pcb with conventional plain balloon ( pb ) or cutting balloon ( cb ) would improve the effectiveness of pta for the treatment of outflow lesions . the purpose of this study is to report our experience with drug - eluting balloons for the treatment of outflow stenoses of failing hemodialysis arteriovenous shunt and to evaluate the primary patency ( pp )  . materials and methods the study protocol was approved by our internal review board . 
written informed consent was obtained from each participant before beginning any study - related procedure . this is a prospective , single - center study , designed to evaluate the safety and technical and clinical outcomes of paclitaxel eluting over plain balloon angioplasty for the management of venous stenosis in avgs and avfs . from september 2014 to september 2015 , both autogenous arteriovenous fistulas ( n 20 ) and prosthetic arteriovenous grafts ( n 30 ) were treated . 
the inclusion criteria were asymptomatic stenosis 50 % revealed by routine surveillance , non - complicated symptomatic stenosis causing malfunctions of the vascular access , and symptomatic stenosis complicated by thrombosis . 
balloons 57 mm in diameter were used . a total of 64 stenoses were registered ; central stenoses ( from the axillary vein to the junction between the superior vena cava and the right atrium ) were excluded from our evaluation : 3 in the avf fistula and 3 in avg ; arterygraft anastomosis ( n 1 ) was also excluded . 
 therefore , a total of 57 stenoses were considered in the present study , subdivided into : 24 in avf and 33 in avg ( table 1 )  . the median follow - up was 8 months ( range 615 )  . all the procedures were performed in our angiographic suite ( allura xper fd20 philips , best , the netherlands )  . 
after inducing blood flow from the needle hub , a 150 - cm , 0.035 - inch hydrophilic guide wire was inserted through the plastic hub to advance it into the vessel . 
if one or more stenoses were confirmed , a 7 - f introducer ( cordis , miami lakes , fl ) was inserted via the guide wire , flushed with normal saline , and then fixed in place . 
after removing the introducer , the puncture site was manually compressed until hemostasis was achieved . a successful pta was defined as residual stenosis < 30 % . follow - up was assessed routinely by the same clinical and hemodynamic criteria described earlier . 
the remaining seven ( 12.3 % ) stenoses were associated with another stenosis and incidentally documented during fistulography . the procedure was technically successful in all cases . the clinical success rate was 94.7 % , in particular in three cases ( 6 % ) thrombosis of the vascular access occurred within the first post - procedure 48 h and patients were immediately referred to the surgical theater for thrombectomy ( two pva and one ava )  . in all cases , dialysis was routinely conducted after discharge and cvc placement was never done . 
in four cases , four new significant ( 50 % ) stenoses was registered ; the new stenoses were documented in different sites of those treated . on the basis of sir guidelines [ 9 ] , no major complications were recorded . 
in - hospital mortality was not observed ; major local or systemic morbidity was not observed . # number , sd standard deviation , ihd ischemic heart disease , bmi body mass index , copd chronic obstructive pulmonary disease , ava autogenous vascular access , cvc central vein catheter , p.pt per patient , pva prosthetic vascular access 1 3 74 radiol med ( 2017 ) 122 : 6976 mean hospitalization time was 16 7 h ( range 625 )  . 
 patency of the vascular accesses was 100 % at discharge . discussion in recent years , percutaneous interventional techniques have been tried and established as a viable alternative means in the management of fistula dysfunction . 
angioplasty is efficacious with some advantages compared to conventional surgical treatment , such as a shorter time needed to perform the procedure and shorter hospitalization , less discomfort for the patient and lower infection rates . 
additionally , it enables dialysis immediately after the procedure without the necessity of using a central venous catheter [ 2 , 4 , 9 ]  . percutaneous transluminal angioplasty ( pta ) is the mainstay of treatment in stenosed hemodialysis access [ 2 , 4 ]  . 
this induces vascular damage and may cause subsequent restenosis [ 5 . ] the high incidence of post - pta recoil , caused by the pathogenesis of this type of stenosis [ 11 ] , has stimulated the search for new devices and alterative endovascular procedures [ 12 ]  . 
as regards pta , proposals include the use of high - pressure balloons [ 2 , 4 ] and prolonged inflation with devices that allow simultaneous perfusion of the fistula [ 11 ]  . cutting balloon is a noncompliant balloon equipped with three or four microblades ( atherotomes ) mounted longitudinally on the outer surface of the balloon . 
these factors are apparently responsible for the lower rates of restenosis [ 13 ]  . the use of cutting balloon was introduced to improve hemodialysis access and long - term patency [ 14 ]  . cutting balloon angioplasty proved to be safe and effective in the treatment of graft - to - vein anastomotic stenosis , with significantly higher assisted primary patency than that of conventional balloon angioplasty [ 15 ]  . the concept of developing a balloon - based drug delivery system to prevent arterial restenosis was based on the hypothesis that a durable effect on neointimal proliferation could be achieved following the single - time delivery of paclitaxel into the vessel wall [ 5 ]  . the safety and effectiveness of drug - coated balloons have been confirmed in percutaneous coronary interventions [ 16 , 17 ] and in peripheral interventions [ 18 , 19 ]  . after balloon dilatation , the pathways of the biological tissue response are regarded to be generally similar in arteries and dialysis access vessels . as mentioned above , the pathophysiology underlying the occurrence of stenosis of hemodialysis access is complex . 
potential mediators that have been suggested to play a role in this process include basic fibroblast growth factor ( bfgf ) , platelet - derived growth factor ( pdgf ) , vascular endothelial growth factor ( vegf ) , and extracellular matrix ( ecm ) proteins [ 20 , 21 ]  . 
 [ 6 ] revealed a significantly higher rate of hd access patency at 6 months in 20 patients undergoing hd treated with ptapcb compared with the other 20 patients treated with ptapb ( 7 with arteriovenous fistulas and 13 with arteriovenous grafts in each study arm )  . the results of this study indicate that drug - coated balloons improve the short - term patency and possibly inhibit neointimal hyperplasia in the artery - anastomosed vein , similar to the results described earlier in the coronary artery and peripheral artery . one study indicates that far infrared radiation is a promising therapy for retarding neointimal hyperplasia and improving unassisted patency of functioning arteriovenous fistulas [ 23 ]  . 
many other studies have established that coated paclitaxel is rapidly delivered to the vessel wall and that it delays neointimal growth and prevents vascular restenosis [ 1619 ]  . the present study showed that by including pcb in ptapb treatment , a short - term patency benefit may be obtained , which may result from the short - term antihyperplastic effect induced by the release of paclitaxel into the vessel wall . 
 [ 8 ] concluded that the use of drug - eluting balloons , after standard angioplasty , improves the primary patency and decreases reinterventions of target lesions in juxta - anastomotic stenoses . comparing the results of fistuloplasty between different studies is difficult because of the many variables involved . 
 some authors considered only native fistulas with juxtaanastomotic stenosis , many of which were recurrent [ 24 , 25 ] ; others only de novo stenoses [ 8 ] or only in - stent stenoses in autogenous dialysis fistulas [ 26 ]  . a recent review [ 27 ] demonstrated the limited data available ; currently , in literature six studies ( two randomised control trials ( rcts ) and four cohort studies ) that reported on 254 interventions in 162 participants have been available . 
at 6 months , target lesions primary patency was reported between 70 and 97 % for pcb in the rcts and cohort studies , and 026 % for non - pcb . 
 target lesions treated with pcb were associated with a higher primary patency at 6 months as compared to nonpcb balloons . on the basis of presented data , association of pcb to cutting balloon angioplasty may be considered useful for treatment of failing hemodialysis vascular accesses . 
our results show promising high primary patency ( 87.7 % ) ; longer follow - up and more patients are needed to investigate the incidence of restenosis , and the necessity for repeated procedures as well as a study about cost - effectiveness would be useful . however , the present study has some limitations . 
first , this study includes a heterogeneous population with autogenous and prosthetic vascular access , with distal and proximal lesions , and the nature of differences in the lesions was not fully considered . 
second , this study was performed in a single center and had a limited sample size with a short follow - up ( re - treatment , stenting and surgical revision are not considered in this follow - up period )  . in conclusion , a short - term patency benefit may be obtained including pcb in angioplasty treatment of failing hemodialysis arteriovenous shunts . 
a cost analysis has been performed to compare the standard embolization endovascular approach , performed postpartum in emergency settlement , with a novel proposed preventive embolization approach , and performed in election in selected high - risk patients before the delivery . 
cardarelli 9 , 80100 naples , italy 2 radiology department , universit campus bio - medico di roma , via alvaro del portillo 200 , 00100 rome , italy 3 department of policy analysis and public management center for research in health and social care management ( cergas ) , bocconi university , via roentgen 1 , 20136 milan , italy 4 measurement and biomedical instrumentation lab , universit campus bio - medico di roma , via alvaro del portillo 200 , 00100 rome , italy derived from the real costs supported by the hospital , based on the regional tariff in the period considered . 
the total expense for the 46 patients of the non - preventive group was 640.551 , 84 ( 13.925 , 04 / patient ) ; all of them received transfusions and 43.4 % underwent to hysterectomy ; the total expense for the 67 patients of the preventive group was 509.720 , 59 ( 7.607 , 77 / patient ) ; 36 % required transfusions and 26 % underwent to hysterectomy . 
in this sample , predelivery uterine artery embolization has proved to be a cost - effective procedure , reducing the length of the hospital stay and the number of transfers to the intensive care unit , in pregnants with placental implant anomalies . keywords uterine arteries embolization cost analysis placental implant anomalies predelivery reducing maternal death is a priority of all the public health systems [ 1 ]  . 
main responsible factors are embolysms , arterial hypertension and especially postpartum hemorrhages , the last accounting for approximately 20 % [ 3 ]  . postpartum hemorrhages occur in 5 % of all deliveries and are the direct cause of about 140 , 000 maternal deaths each year [ 4 ]  . 
massive transfusions , drugs , and obstetrical maneuvers play a relevant role in the management of these clinical issues ; however , when these are not effective , surgical procedures are unavoidable . 
in line with the sir and cirse guidelines for the use of radiations during pregnancy [ 8 ] , several measures were applied to minimize the radiation dose to the fetus : the lowest pulsed rate fluoroscopy allowed by the equipment ( 15 pulses / s ) , no angiography exposure , no enlargement of the field of view , use of the halfdose filter , postero - anterior beam projection , x - ray tube at maximal distance from the patient , low tube current and high tube potential , beam - on time to an absolute minimum . the computation of the detailed costs derived from the real costs observed and supported by the hospital , based on the regional tariff derived in the period considered ; these included six main categories : instrumental exams ( computed tomography , ultrasound , etc . ) , laboratories analysis , specialistic consultants , medical devices , surgical interventions , and daily hospital stay ( table 1 )  . all data analysis and statistical tests ( student t test ) were performed in a matlab environment ( mathworks , inc , natick , massachusetts )  . 
both of these in the preventive group are significantly lower : about the surgical interventions in mean , 636 / patient are saved , while about the hospital stay in mean , 4.707 / patient are saved . overall , in the preventive group , there is a mean saving of 45 % , it else 6.317 / patient ( 13.925 , 04 per patient in the non - preventive group vs 7.607 , 77 per patient in the preventive group )  . the clinical impact of the predelivery embolization in this category of patients has been already discussed [ 7 ] ; briefly , lower rates of blood units transfusions ( and consequent lower risk of developing disseminated intravascular coagulation ) and shorter hospital stays have been reported . patients suffering from postpartum hemorrhages present well - known risk factors , and so with a detailed clinical anamnesis associated with ultrasound and / or magnetic resonance imaging , they can be quickly recognized and addressed to a dedicated management protocol : this allows to apply a preventive approach . this analysis presents some limitations . 
first of all , the study has been performed in italy , and the costs are strictly dependent on the italian public health system ; therefore , the conclusions should be limited to the italian country , even if a shorter hospital stay determines lower costs in every country . 
in particular , a number of diseases show hypertrophy and enlargement of the bronchial circulation with consequential increase in vessel fragility [ 1 ]  . life - threatening or recurrent haemoptysis is an emerging complication in subjects with pulmonary hypertension ( ph ) [ 4 , 5 ]  . 
 the latter included four ( 44.4% ) patients with chronic thromboembolic pulmonary hypertension ( cteph ) , three ( 33.3% ) with idiopathic pulmonary arterial hypertension 4 / 8 , average age 38.96 3 / 6 , average age 9 , m / f 35.55 ( ipah ) , and two ( 22.2% ) with heritable pulmonary arterial hypertension ( hpah )  . 
beyond the 33 selected patients , 2 more patients underwent bae for haemoptysis in the selected period , who were excluded because they were lost to follow - up and no information about haemoptysis recurrence and survival was available in the following 12 months . 
demographics , laboratory , and clinical data were collected and compared between each group ( table 1 ) ; moreover , metrics from right heart catheterisation ( rhc ) were compared between chd - apah and nonchd - apah subgroups ( table 2 )  . 
follow - up at 30 and 90 days from bae was collected for all subjects , and overall survival was calculated for the ph group and compared between its two subgroups . bronchial artery embolization all the bae procedures were performed by an interventional radiologist with 15 years of experience in interventional radiology . after local anaesthesia , vascular access was obtained via transfemoral and / or transbrachial approach , according to the origin and the course of the arteries to be embolized . 
 after the embolization of the target arteries , a final angiographic scan was carried out to ascertain the full occlusion of the selected vessel and to detect possible collateral blood supply from both bronchial and non - bronchial circulation . 
all vardata were presented as mean iables were analysed with descriptive methods ; cross - tabulations were checked with chi - squared test or by fishers exact test , and anova test as appropriate . 
at the time of haemoptysis , 6 / 21 ph patients ( 28.5% ) were under anticoagulant therapy and 17 / 21 ( 80.9% ) were receiving specific medication for ph . 
permanent embolic agents were used as follows : in 21 procedures ( 65.6% ) , we used particles such as polyvinyl alcohol ( pva ) ( contour , boston scientific corporation , maple grove , mn ) , with a diameter ranging between 150 and 1000 m , more often 250350 and 350500 in five procedures ( 15.6% ) , we used n - butyl 2 - cyanoacrylate ( glubran , gem srl , viareggio , italy ) ; pushable metal microcoils ( hilal , cook group inc , bloomington , in ) were used twice ( 6.3% ) , together with pva particles on one of those occasion . 
haemostasis was achieved both manually and by means of a vascular closure device ( exoseal , cordis corporation , bridgewater , nj )  . a total of 67 arteries were embolized as follows : 59 bronchial arteries and eight non - bronchial systemic arteries . 
procedure - related death occurred in one patient with ipah who presented with sudden onset of dyspnoea , diaphoresis , and tachycardia during bae , followed by rapid deterioration of the clinical condition 1 3 radiol med ( 2017 ) 122 : 257264 fig . 
2 a , b an intercostobronchial trunk ( ibt ) , arising from aorta , from which originate an intercostal artery and a right bronchial artery ( a )  . 
chd - apah congenital heart diseaseassociated pah the endovascular treatment of haemoptysis by bae led to improvement of patient management , notably prompt control of bleeding in a range of otherwise untreatable comorbidities [ 27 ]  . 
the treatment of haemoptysis of ph is indeed a relatively low invasive procedure to control the acute onset of pulmonary bleeding in subjects with weak cardiopulmonary dynamic [ 28 ]  . 
as a background note , the chronic onset of bronchial artery hypertrophy causes a particular increase in number of bronchial arteries and morphological distortion that are limiting factor of endovascular treatment of bae in ph [ 29 ]  . 
we also found higher average inr values in the non - chd - apah group , which could be explained by the high proportion of cteph patients ( 44.4% ) , in which life - long anticoagulation therapy is recommended , while in pah patients , the need for an anticoagulation therapy is still debated [ 5 , 31 ]  . despite this is the largest cohort in the literature about the efficacy of bae in the treatment of haemoptysis in ph , fig . 
4 two right bronchial arteries with ectopic origin arising from a thyrocervical trunk 1 3 radiol med ( 2017 ) 122 : 257264 the size still represents a major study limitation . 
however , it allowed us to demonstrate that bae is a useful procedure for immediate haemoptysis control , while further studies are needed to confirm whether urgent lung transplantation is a valid and viable solution in ph patients . 
more studies are required to confirm whether there is no difference in bae complications in these more complex procedures when they are operated by radiologists with different levels of expertise , and whether specific training might be needed . conclusion we showed that bae may be an effective and safe procedure for the treatment of acute haemoptysis in ph patients . 
 bae in ph patients is more complex compared to procedures in subjects without ph because there are a higher number of arteries to be treated and there is more anatomical and morphological variability . 
bae repetition can be useful for haemoptysis control and to improve the quality of life in patients with a chronic pulmonary disease like ph , which seems to have a higher relapsing rate than other conditions associated with haemoptysis . compliance with ethical standards the study was approved by our institutional ethics committee . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
informed consent was obtained from all individual participants included in the study . conflict of interest we have no conflicts of interest to disclose . radiol med ( 2017 ) 122 : 294302 doi 10.1007 / s11547 - 016 - 0720 - 8 neuroradiology reproducibility of dynamic contrastenhanced mri and dynamic susceptibility contrast mri in the study of brain gliomas : a comparison of data obtained using different commercial software gian marco conte1 antonella castellano1 luisa altabella1 , 2 antonella iadanza1 marcello cadioli1 , 3 andrea falini1 nicoletta anzalone1 received : 21 september 2016 / accepted : 19 december 2016 / published online : 9 january 2017 italian society of medical radiology 2017 abstract purpose dynamic susceptibility contrast mri ( dsc ) and dynamic contrast - enhanced mri ( dce ) are useful tools in the diagnosis and follow - up of brain gliomas ; nevertheless , both techniques leave the open issue of data reproducibility . 
we evaluated the reproducibility of data obtained using two different commercial software for perfusion maps calculation and analysis , as one of the potential sources of variability can be the software itself . methods dsc and dce analyses from 20 patients with gliomas were tested for both the intrasoftware ( as intraobserver and interobserver reproducibility ) and the intersoftware reproducibility , as well as the impact of different postprocessing choices [ vascular input function ( vif ) selection and deconvolution algorithms ] on the quantification of perfusion biomarkers plasma volume ( vp ) , volume transfer constant ( ktrans ) and rcbv . 
comparisons of different vif estimation methods for dce biomarkers resulted in icc of 0.636 for ktrans and 0.662 for vp ; comparison of two deconvolution algorithms in dsc resulted in an icc of 0.999. conclusions the use of single software ensures very good intraobserver and interobservers reproducibility . 
most studies published on this topic used perfusion - derived biomarkers 1 3 radiol med ( 2017 ) 122 : 294302 for gliomas grading [ 15 ] , patients outcome prediction [ 6 11 ] and differentiation of tumor recurrence from treatmentrelated effects like radionecrosis and pseudoprogression [ 1216 ]  . however , reproducibility is still an open issue for both techniques : no standardized protocol for acquisition and analysis of perfusion techniques is still available and , consequently , different research groups have used different protocols , generating a wide range of results [ 1722 ]  . 
 recently some steps towards standardization have been made , with the publication of an evidenceand consensusbased standards document for dce [ 23 ] and a white paper for dsc [ 24 ]  . one of the potential sources of variability is the software chosen for perfusion map calculation and analysis [ 2532 ] since each software implements different analysis tools [ i.e. 
 leakage correction for dsc maps or automatic detection of vascular input function ( vif ) ] and sometimes different algorithms . the aim of this study was to test the reproducibility of data obtained from studying the same cohort of patient with two commercial software , which were chosen based on the rationale that they could be used independently from the mr machine available for the acquisition , thus reducing data spread and improving standardization of perfusion analysis . 
this study was approved by the ethical committee of our institution . dce analysis mr imaging was performed on a 3t scanner ( achieva , philips healthcare , best , the netherlands ) equipped with 80 mt / m gradients using a phased - array head 8 channelcoil . 
the total acquisition time for dscmri was 2 min and 4 s . a cumulative fixed dose of 10 ml of gadobutrol ( gadovist , 1 mmol / ml ; bayer schering pharma , 6 berlin , germany ) was administered , splitted in two boluses of 5 ml . 
the first bolus of 5 ml was injected 50 s after the start of the dce sequence using a power injector ( spectris solaris mr injector ; medrad , indianola , pennsylvania ) at a rate of 2 ml / s , immediately followed by a 20 ml continuous saline flush at the same injection rate . 
the second bolus of 5 ml was injected 16 s after the start of the dsc sequence using the same power injector at a rate of 5 ml / s , followed by a 20 ml saline flush at the same injection rate . 
 in both software , preprocessing steps included automatic motion correction by a rigid - body registration , automatic spatial smoothing and background segmentation . for dce analysis , patient - specific baseline t1 maps were derived from vfa axial sequences ( see online resource 1 for acquisition details )  . in both software dce analysis was based on the extended tofts model [ 33 ]  . 
in olea sphere both a manual venous vif and an automatic one were obtained ; the venous one was obtained from the sss , while the automatic one was obtained using a tool implemented in the software [ 34 ] , which selected both arteries and veins as sources of input . 
 parametric maps of volume transfer constant ( ktrans ) and plasma volume ( vp ) were then obtained . 1 3 296 dsc analysis in both software , dsc analysis was performed using the singular value decomposition ( svd ) algorithm for deconvolution [ 35 ]  . 
however , while olea sphere offers different methods for svd , and both the standard truncated svd ( ssvd ) and oscillation - index csvd ( osvd ) were used for analysis , in nordicice only ssvd was available . 
an arterial vif was obtained in olea sphere using an automatic method [ 34 ] while in nordicice it was obtained semi - automatically : the observer selected the axial slice of interest and then the software searched for a valid vascular signal . 
parametric maps of cerebral blood volume ( cbv ) were then obtained . a fixed hematocrit value of 0.45 was set in both software . image analysis all the parametric maps were independently analyzed by two observers ( gmc , with 3 years experience in perfusion analysis , na with 7 years experience in perfusion analysis )  . in both software , perfusion maps were automatically coregistrated with flair and / or post - contrast t1 images by performing a rigid transformation of the datasets . for each parametric map , multiple circular rois , 2530 mm2 in area , were drawn in the tumor area that showed the highest value of perfusion biomarkers , then the one showing the highest mean value for each perfusion biomarker was selected . 
to normalize cbv values , a single elliptic roi , 250300 mm2 in area , was drawn in the contralateral normal appearing white matter ( nawm ) in the centrum semiovale ( ncbv )  . 
the analysis was repeated after one month to assess intraobserver reproducibility . from dce analysis , for each parametric map and each observer three datasets were obtained : one with the automatic vif selection ( olea automatic ) and two with the manual vif selection ( olea manual and nordicice ) ; from dsc two datasets ( olea automatic and nordicice ) were obtained . moreover , to avoid any possible variability due to different rois positioning between observers , intersoftware reproducibility was re - tested drawing the rois in the same tumor area in the two software . 
mean value of selected rois was then used for the comparison . radiol med ( 2017 ) 122 : 294302 to test the impact of different postprocessing options on the quantitative data , additional analyses were performed using olea sphere : for dce , the reproducibility of data obtained using the automatic and the manual vif selection and for dsc the data obtained using the ssvd and osvd methods . 
moreover , especially in neuroimaging , some groups analyze pwi datasets using non ce and fda approved in - house software . the issue of the reproducibility of data derived from different software seems to be independent from imaging technique and anatomical district : previous studies focused on data obtained using different software or different versions of the same software in both ct - pwi [ 27 , 29 , 30 ] and mr - pwi [ 25 , 26 , 28 , 31 , 32 ]  . 
to our best knowledge , this study is the first reporting data on dce reproducibility in brain imaging . intrasoftware reproducibility regarding the intrasoftware analysis , we found good reproducibility for all comparisons ( table 1 )  . 
summary of icc values obtained in all comparisons ; upper and lower limits of the box represent the highest and lowest icc value obtained ; the central line represents the mean icc value obtained 1 3 radiol med ( 2017 ) 122 : 294302 both dsc and dce parameters ; moreover , the 95% confidence interval for icc values showed a wide range of results for all comparisons ( table 2 )  . 
3 comparison of automatic and manual vif selection in the same patient ; in this case automatic vif selection on dce maps shows both arterial ( a ) and venous ( b ) input ; manual vif selection on dce maps consists in venous input only ( d ) ; c , e concentration time curves show different peaks , with the one derived from automatic vif being lower . 
the curve derived from the manual vif is the mean of four different input located around the pixel selected ( e ) 1 3 300 radiol med ( 2017 ) 122 : 294302 fig . 
4 comparison of automatic and manual vif selection in the same patient ; in this case automatic vif selection on dce maps shows only venous input ( a , b ) ; manual vif selection on dce maps consists in venous input only ( d ) ; c , e concentration time curves shows similar peaks . 
the curve derived from the manual vif is the mean of four different input located around the pixel selected ( e ) deconvolution algorithms in dsc value , while some differences are expected in cbf when comparing osvd and ssvd [ 36 ]  . for dsc , one of the proposed factors that may affect reproducibility is the choice of the deconvolution algorithm [ 27 , 30 ]  . 
in our study dsc analyses were performed applying both different and same deconvolution algorithms in the two software , finding low intersoftware reproducibility , that only slightly increased from an icc of 0.4550.582 when selecting the same algorithm ( ssvd ) ( table 3 )  . 
it is possible that the choice of a different algorithm per se does not introduce significant variability ; this was proved comparing the data obtained using the two different svd methods in the same software , resulting in an almost perfect agreement with an icc of 0.999 ( table 4 )  . 
in the intersoftware comparison , a better reproducibility was obtained for both ktrans and vp when the vif was selected manually in both software ( tables 2 , 3 )  . 
our results show that this single change in postprocessing step has a significant impact on data as only moderate agreement was obtained , even if the rois were positioned in the same area and no other differences exist between the datasets compared ( table 4 )  . 
 probably the vif selection itself cannot entirely explain the poor reproducibility but it seems to play a major role in it . our study confirms the recent findings by orsingher [ 26 ] , milchenko [ 31 ] and kelm [ 32 ] , who also found low intersoftware reproducibility of dsc parameter cbv . 
it must be said , however , that a thorough training is necessary to obtain this result and the acquisition and analysis protocol must be followed very strictly . the poor intersoftware reproducibility and the impact of postprocessing options on data reproducibility have consequences on the design of follow - up studies , on the application of data published in literature and on the daily clinical routine use of perfusion analysis . 
it must be said , however , that , as shown in the work by kelm [ 32 ] , different diagnostic accuracy is unlikely to be found among different fda - cleared software . conclusions in conclusion , we found a very good intrasoftware reproducibility and poor intersoftware reproducibility for dce and dsc analyses , suggesting that while the use of a single software ensures reliable results , caution should be taken when comparing data obtained using different software and different postprocessing options , since the reproducibility in this case is not guaranteed anymore . compliance with ethical standards conflict of interest nicoletta anzalone served as a consultant for bayer healthcare . 
all the other authors declare that they have no potential conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the cmr protocol included t2 - weighted ( oedema ) , early ( hyperaemia ) and late ( fibrosis / necrosis ) gadolinium enhancement sequences , according to lake louise criteria . 
quantitative outcomes were checked for normality and compared with the non - parametric wilcoxons test for matched data . results at the clinical follow - up all patients were free of symptoms and reported no cardiac complications . 
by using these indications cmr achieved high diagnostic accuracy ( 78% ) with estimated specificity of 91% [ 2 ]  . the clinical presentation of acute myocarditis is variable [ 3 ] , ranging from a subclinical disease to an infarctlike syndrome , arrhythmias , heart failure and cardiogenic shock ; for infarct - like myocarditis , the cmr sensitivity has been recognized to be very high ( 80% ) [ 4 ] , and in fact suspicion of myocarditis represents one of the most frequent indications to cmr . 
all patients had a low cardiovascular risk factor profile ; invasive coronary angiography excluded the presence of significant coronary artery disease in all of the the cmr exams were performed after a mean time of 8 days ( 412 ) after the onset of symptoms . 
a second cmr examination was performed at the same time of the clinical follow - up at 6 months . at the moment of the cmr examination , all patients were informed about the possible use of their data for study purposes and signed an informed consent for patients information was anonymized prior to the analysis . 
the study is a retrospective trial without any study - related clinical intervention and conforms to the helsinki declaration . cmr protocol cmr imaging was performed with a 1.5 - tesla scanners ( achieva , version 2.6 , philips medical systems , eindhoven , the netherlands ) using a body and phased array coil ( 32 - channel )  . cine steady - state free precession ( cine - ssfp ) cmr images were acquired in the 4 - chamber planes , 2 - chamber , 3 - chamber and short - axis . 
the t2 - weighted short tau inversion recovery ( t2w - stir ) images were acquired firstly on long - axis and then on short - axis planes covering the entire left ventricle during 68 consecutive breath - holds . 
lv end - diastolic volume ( lvedv ) , lv end - systolic volume ( lvesv ) , ejection fraction ( ef ) , and lv mass were determined . t2w - stir images were visually assessed for the presence and extension of hyperintense areas , which identified the presence of myocardial oedema . 
the t2 ratio was calculated as the ratio between the signal intensity of the damaged myocardium to the signal intensity of a skeletal muscle , generally a paraspinal muscle ( drawing two roi in the same image )  . 
 [ 2 , 21 ]  . early gadolinium enhancement ratio ( ege ratio ) was calculated by tracing endocardial and epicardial contours on pre and post - contrast images and placing a reference roi on the skeletal muscle located within the same slice 1 3 radiol med ( 2017 ) 122 : 273279 in order to normalize myocardial enhancement as for the t2 - ratio . 
the spatial extent of these lesions was quantified ( areas with signal intensity at least 3 standard deviations greater than for normal myocardium ) [ 22 ] and was expressed as a percentage of the total myocardial volume . 
the signal intensity ratio between lge area and healthy myocardium ( lge ratio ) was also evaluated . clinical and radiological followup the clinical and cmr follow - ups were performed on the same day . the clinical assessment included a complete cardiologic visit with echocardiogram and both a standard 12 - lead ecg and a holter - ecg . 
the cmr follow - up was performed with the same protocol used in the acute stage . statistical analysis continuous variables were checked for normality with the kolmogorov / lilliefors test , shapirowilk w test and dagostinos tests . 
from the left to right : left ventricular ejection fraction ( lvef ) , left ventricular end - diastolic volume index ( lvedvi ) and left ventricular mass index ( lv mass i )  . 
in summary , we found : good clinical - laboratory evolution of all patients ; reduction in cmr parameters of inflammation and reduction , but with persistence of lge changes . to the best of our knowledge , there are only two studies focused on the follow - up of patients with infarct - like myocarditis . 
 [ 6 ] found that none of their patients reported arrhythmias or further cardiac complications , no cases of persisting oedema on t2 - weighted sequences were reported , late enhancement decreased in 20 of 21 patients and the ejection fraction remained stable or improved in all patients . 
 [ 14 ] found an association between infarct - like myocarditis and major cardiovascular events ( mace ) occurrence and identified nyha functional class > ii and lge as independent predictor of mace . 
encountered some mace already in the first 6 months , but on the other hand also dantis [ 6 ] patients were free of events during the first few months . according to the american heart association ( aha ) and american college of cardiology ( acc ) guidelines [ 23 ] , the interval between initial assessment and retesting before resumption of any sports activity will vary depending on the severity of the initial illness . 
from the top to the bottom : 4 chamber , 3 chamber and short - axis view and from right to left : acute mr and follow - up mr . 
on this basis , we usually scheduled follow - up studies at about 6 months . at clinical follow - up all patients were free of symptoms , no arrhythmias or further cardiac complications were reported and all laboratory data were normalized . 
 [ 24 ] concluded that patients with an increase of lvef by 20% or an lvef > 50% , and a low nyha functional class at 6 months demonstrated an excellent long - term prognosis . 
 these data demonstrate that the diagnosis of complete clinical recovery of infarct - like myocarditis was associated with the reduction in cmr parameters of inflammation , in agreement with the definition of reversible injuries [ 7 ]  . previous studies demonstrated that the presence of lge is the best independent predictor of major cardiovascular events in patients with myocarditis [ 10 , 11 , 14 ]  . 
third , the lack of adverse events in the follow - up , while being an excellent result for the patients , did not allow us to identify any cmr parameters as possible predictors of adverse clinical outcome . 
 our aim was to evaluate myocardial metabolism with 31pmrs and 1h - mrs in hcm patients and cas . materials and methods after ethics committee approval , 15 cas and 7 hcm patients were prospectively enrolled . 
1h - mrs was performed after imaging using standard coil with the patient in the supine position ; thereafter , 31p - mrs was performed using a dedicated coil , in the prone position . 
diastolic dysfunction and outflow tract obstruction of the left ventricle may be present , causing major clinical manifestations such as angina , dyspnea , dizziness and syncope [ 6 , 7 ]  . 
in approximately 30% of hcm patients , ventricular hypertrophy is moderate without obstruction of the outflow tract of the left ventricle , both at rest and under stress and , therefore , the disease is silent [ 8 ]  . 
indeed , hcm was reported to be responsible for 35% of sudden deaths in young athletes [ 9 , 10 ]  . competitive athletes with intense and regular training exercise usually develop cardiovascular changes leading to a reversible paraphysiological myocardial hypertrophy known as athletes heart . 
in 2% of such athletes , the left ventricle wall thickness reaches 1315 mm [ 12 ] , with a distribution partially overlapped with those measured in mild forms of hcm , especially mutations of troponin t [ 13 ]  . 
thus , it is clinically relevant to differentiate between athletes heart and mild forms of non - obstructive hcm . magnetic resonance spectroscopy ( mrs ) is a non - invasive diagnostic technique allowing for the in vivo evaluation of myocardial metabolism [ 14 , 15 ] by measuring the signal intensity of 31p or 1h . 
in particular , with 31p - mrs , the ratio between phosphocreatine ( pcr ) and - adenosine triphosphate ( atp ) may be measured , representing an index of the myocardial energy reserve [ 3 , 1618 ]  . 
on the other side , 1h - mrs allows for estimating the total creatine ( cr ) ( sum of pcr and cr ) [ 19 , 20 ] , which is associated with myocardial contractility [ 21 , 22 ] ; moreover , myocardial lipids may be measured using 1h - mrs [ 23 , 24 ]  . the aim of this study was to evaluate the left ventricle function in patients affected by hcm compared with that of competitive athletes and to assess the myocardial metabolism using 31p - mrs and 1h - mrs in the two populations . radiol med ( 2017 ) 122 : 265272 materials and methods study design and inclusion criteria this prospective cross - sectional study was approved by the local ethics committee and each subject signed a written informed consent . 
inclusion criteria were as follows : patients aged 18 years or more with a known diagnosis of non - obstructive hcm , defined as asymmetric hypertrophy of the left ventricle , with the typical patchy pattern with local distribution of late gadolinium enhancement [ 12 , 13 ] ; competitive athletes aged 18 years or more , in good health , without any reported cardiovascular symptoms and with intense exercise training in the month prior to the enrollment , quantified in at least 10 h per week . 
exclusion criteria were contraindications to magnetic resonance such as pacemakers / defibrillators , intracranial ferromagnetic vascular clips , intraocular metal fragments , or severe claustrophobia . magnetic resonance imaging each enrolled subject underwent a 1.5 - t magnetic resonance ( magnetom sonata maestro class , siemens medical solutions , erlangen , germany ) , including a morphologic and functional imaging study , with the patient in the supine position . the imaging protocol included balanced steady - state free precession sequences ( true fast imaging with steadystate free precession , true - fisp ) using a four - channel surface phased - array coil in the short axis plane covering the entire heart . 
the kinetic study was processed by manual segmentation using syngo argus software ( version ve32b , siemens medical solutions , erlangen , germany ) by a radiologist with a 7 - year experience in cardiac mr imaging . 400 mm2 ; matrix 119 for each subject , the following imaging - derived variables were measured for the left ventricle : end diastolic thickness of the septum ; end diastolic thickness of the posterior wall ; mass index ( i.e. , normalized to the body surface area ) ; end diastolic volume index ( edvi ) ; end systolic volume index ( esvi ) ; ejection fraction ( ef ) ; stroke volume ; and ventricular end diastolic diameter . 
we have also calculated an asymmetry index , defined as the left ventricle septal - to - posterior wall thickness ratio . 1 3 radiol med ( 2017 ) 122 : 265272 1hmrs 20 after morphologic and functional imaging , hydrogencontaining metabolites were measured in a single voxel of 40 mm3 within the interventricular septua point - resolved spectroscopy sequence ( ecg synchronization ; diaphragm navigator ; acquisition in the end systolic phase ; tr / te 2000 / 90 ms ; flip angle 90 ; number of excitations 150 ; suppression of the water signal ; supine position ) was performed using the same four - channel surface phased - array coil used for imaging . a physicist with 8 - year experience in mrs processed all spectra using the jmrui software that implements the amares ( advanced method for accurate , robust , and efficient spectral ) algorithm quantitation [ 25 ]  . 
data were presented as arbitrary units ( au )  . 31pmrs myocardial phosphates were measured through 31p - mrs using a dedicated surface coil tuned for 31p and with the patient in the prone position . 
on the basis of repeated low - resolution scout images , we placed a grid of volumes of interest so as to guarantee at least one voxel within the anterior ventricular junction , trying to minimize contamination by ventricular blood . 
then , we acquired a multivoxel chemical shift imaging sequence for a single slice ( nuclear overhauser enhancement technique ; ecg synchronization for acquisition in the end diastolic phase ; tr / 60 mm3 ; field of view 300 800 / 2.3 ms ; flip angle 90 ; grid size 8 300 mm2 ; free breathing )  . pre - processing included : exponential filter , zero - filling from 1024 to 2048 points , fourier transform , frequency and phase correction and subtraction of the baseline with the polynomial method . 
continuous variables were reported as median and interquartile range ( iqr ) and p values < 0.050 were considered statistically significant . results population characteristics a total of 22 subjects were enrolled , whose characteristics are reported in table 1 . 
1 cardiac magnetic resonance images in diastolic phase of a mid - ventricular short axis section of an athlete ( a ) and a hypertrophic cardiomyopathy patient ( b )  . 
note that the septal thickness of the patient is greater than that of the athlete morphology and function the distribution and comparison of morphologic and functional characteristics of the left ventricle in the two groups are shown in table 2 . 
note that the lipid peak is higher in the patient than in the athlete 31pmrs data from 31p - mrs were not available for two hcm patients due to examination interruption for claustrophobia ( in one case ) or to low signal - to - noise ratio probably related to patient movement ( in the other case )  . 
 bivariate correlation analysis as reported in tables 2 , 3 , and 4 , the variables found to be significantly different in the two groups at bivariate analysis were : age , bmi , stroke volume , edvi , left ventricular mass index , interventricular septal thickness , asymmetry index , 2 , 3 - dpg / atp , lipids at 1.3 ppm and total lipids . 
this study adds a new potential biomarker to the well - known differences in the left ventricle remodeling and function . causes for the accumulation of intramyocardial lipids in early stages of hcm need to be clarified and a thorough explanation is currently not available . 
similar results were obtained in patients affected by type - 2 diabetes [ 36 , 37 ]  . in our study , the phosphate metabolism of athletes heart was preserved and the pcr / atp ratio was in the range of normal values [ 14 ] , as expected [ 38 ]  . 
the 31p - mrs analysis also showed a significant difference between the two groups in terms of 2 , 3 - dpg / atp , with a lower value in hcm patients than in athletes . 
note that pcr / gamma - atp ratio is reduced in the hcm patient 1 3 radiol med ( 2017 ) 122 : 265272 considering that atp alone was not significantly different in the two groups , an increase of 2 , 3 - dpg may explain the difference in 2 , 3 - dpg / atp . 
the reason for this phenomenon could lay in the contamination of the blood pool in the voxel in subjects with a small septuthe variation of pme / pcr and pi / pcr between the two groups was not significant , in line with the literature [ 29 ]  . 
notably , a not significant difference was observed in terms of pcr / atp , as an indicator of energy metabolisthis may be due to the normal value of septal thickness in our athletes population , without any overt athletes heart condition . as a potential clinical application of our study , we highlight that while 1h - mrs required only five additional minutes , the 31p - mrs protocol required the extraction of the patient from the magnet , the change of the coil and a new patient positioning in an uncomfortable prone position . 
it is offered only for 3 - t units , whose results for cardiac imaging were reported to be not clearly better than those obtained with 1.5 - t units in terms of image quality [ 39 ]  . morphologic and functional imaging data , edvi and stroke volume , were significantly lower in hcm patients than in athletes , confirming the typical geometric pattern of the disease on one side and the heart adaptation to the intense sport activity on the other , as already reported [ 6 ]  . 
first , the number of subjects studied was small and bikers and volley players are different in terms of exercise ( low static moderate dynamic for volley ; high static and dynamic for cycling ) , leading to potential differences in cardiac metabolic activity . 
second , the higher bmi and age in hcm patients may represent a source of bias , so that we cannot exclude that they can explain the difference in lipid content ; however , bivariate correlation analysis between lipids and bmi did not show any significant correlation . 
however , the area under the peak as we used in this work can be considered a valid quantitative approach , utilized in cardiac [ 28 , 40 ] and non - cardiac studies [ 41 ]  . 
fifth , ethical issues prevented from performing late gadolinium enhancement in athletes . conclusion in conclusion , we found a significant increase in myocardial lipids in hcm patients compared to competitive athletes at 1h - mrs . 
myocardial 1h - mrs may be an additional final phase of a cardiac mr protocol including standard morphologic and functional imaging in the differential diagnosis between hcm and athletes heart . 
prospective larger studies are needed to confirm this preliminary unexplained , but intriguing observation . acknowledgements this research received no specific grants from any funding agency in the public , commercial or not - for - profit sectors . compliance with ethical standards conflict of interest f secchi and g . 
georgiadis1 received : 6 august 2016 / accepted : 3 january 2017 / published online : 21 january 2017 italian society of medical radiology 2017 abstract endovascular repair of abdominal aortic aneurysms has widely replaced the open surgical repair due to its minimal invasive nature and the accompanying lower perioperative mortality and morbidity . 
during the past two decades , certain improvements and developments have provided a wide variety of endograft structural designs and geometric patterns , enabling the physician to approach a more patient - specific treatment of aaa . 
this review presents the currently available aortic endografts and describes the clinical , technical and mechanical characteristics of them . keywords aortic stent - graft clinical performance abdominal aortic aneurysm hemodynamics endovascular aneurysm repair introduction since its introduction in 1991 , the endovascular repair ( evar ) of abdominal aortic aneurysms ( aaa ) has been widely accepted by physicians and patients due to its minimal invasive nature and its lower perioperative mortality and morbidity [ 1 , 2 ]  . 
the correct choice of stent - graft decreases the complication rate and the need for reinterventions . materials used for the graft covering include polyester and polytetrafluoroethylene ( ptfe ) , whereas stent composition includes stainless steel , nitinol and cobalt chromium alloy . 
some endografts have passive fixation using their radial support and columnar strength and others present active fixation with pins , hooks and barbs . the long - lasting clinical efficacy ( aaa sac exclusion from systematic pressure , avoidance of sac expansion or rupture ) and incidence of complications leading to need for major interventions are the crucial reference issues when comparing the various endografts . 
 moreover , apart from any form of clinical studies , in vitro laboratory studies provide additional information about the biomechanical properties of various endografts patterns and designs or the impact of the latter on the central hemodynamics of the patients . this article provides useful clinical and hemodynamic information for the endografts commercially available and discusses the major drawbacks and limitations between current data . 
this endograft lacks suprarenal fixation and should be used , therefore , with caution in cases of aaa with considerable angulation but limited infarenal neck length . the endurant ii ( medtronic , santa rosa , ca , usa ) is a modular - bifurcated stent - graft composed of nitinol stents and polyester grathe combination of the m - shaped configuration of nitinol stents and improved suprarenal active fixation with anchoring pins provides better resistance to migration in short and angulated proximal aortic necks [ 7 ]  . 
one should bear in mind that after the deployment of the main body and before the removal of the delivery system , it is necessary to recapture the spindle in the tapered tip . 
this is the most important step as failure to withdraw the delivery system until the spindle is retracted into the fabric portion of the stent - graft can result in trapping of a suprarenal crown within the tapered tip sleeve [ 9 ]  . the treovance abdominal stent - graft ( bolton medical , barcelona , spain ) is a tightly woven polyester nitinol trimodular endograft with a main bifurcated stent - graft and two leg extensions . 
the main body comes in three different lengths while the overlapping length between the main body and the limb extension is adjustable ( 40 mm adjustable landing zone for the ipsilateral and 10 mm for the contralateral limb )  . 
notably , the iliac gates have five dull barbs to withstand the displacement forces tending to separate the limbs from the main component , thus eliminating the incidence of endoleaks type iii [ 10 ]  . 
the endograft should be handled with care in rather small access vessels since its relatively large profile and stiffness of its delivery device may cause problems related to such arteries [ 11 ]  . the zenith flex ( cook medical , bloomington , usa ) is a modular - bifurcated system consisting of a stainless steel z - stents sutured to a woven polyester graft material . 
on the other hand , the new zenith low profile is constructed of nitinol stents instead of stainless steel with a thinner polyester material and its new 16 fr delivery system down - sizes the iliac access diameter available for insertion and navigation of the particular endograft to 6 mm and is associated with promising mid - term results in unfavorable iliac anatomies [ 12 ]  . the incraft stent - graft ( cordis , bridgewater , nj , usa ) is designed to overcome the limitation of the small diameter of the access vessels . 
it is a trimodular - bifurcated device constructed of a seamless , low porosity , woven polyester graft supported by a series of self - expanding nitinol stents throughout the entire grasuture knots on the outer surface of the limb prosthesis comprise an interlocking mechanism to eliminate the risk of limb separation . 
the unavailability of aortic extensions in cases of central endoleaks should be taken into consideration when handling challenging infrarenal necks [ 13 ]  . the anaconda one lok stent - graft ( vascutek , uk ) is a three - piece device made of nitinol rings and a polyester graits active infrarenal fixation is accomplished via eight hooks while a magnet system facilitates the cannulation of the contralateral gate [ 14 ]  . 
there are reports depicting high incidence of post - implantation syndrome with this particular endogra [ 15 ]  . the e - vita stent - graft ( jotec , hechingen , germany ) is a modular two - piece endograft with suprarenal fixation composed of polyester fabric and nitinol stents [ 16 ]  . 
most notably , the first nitinol stent of the cranial top has a multiple - tip design to improve the apposition onto an infrarenal neck of marked calcification , or irregular shape . 
the current lack of midor long - term follow - up data precludes its generalized use for the time being . the aorfix stent - graft ( lombard medical technologies , oxfordshire , uk ) possesses cranial rings with a fishmouth 1 3 312 radiol med ( 2017 ) 122 : 309318 shape . 
it has been reported that failure of the cup segment to track and follow adequately the iliac rotating manipulations can result in inadequate orientation of the central fish - mouth with respect to the renal artery ostium , comprising the achilles heel of the aorfix device [ 18 , 19 ]  . in the aneurysm sac , dissociating the sealing efficiency from the shape and contour of the proximal aortic neck . 
the nellix stent - graft is particularly suitable for patients with conical necks as the endobags apply on the entire length of the conical neck elongating the sealing zone [ 22 ]  . 
however , the long - term follow - up is not yet determined nor the type , applicability and efficiency of the treatment modalities in case of immediate or late on set complications . direct accommodation onto the aortic bifurcation the afx stent - graft ( endologix , inc , irvine , ca , usa ) is a unibody endograft based on the concept of anatomic fixation . 
the cobalt chromium stents of the afx device are sutured only at the proximal and distal ends of the inner surface of the graft material , allowing flexibility of the graft material . 
the ovation stent - graft does not depend on the length of neck as long as the first ring seals 13 mm below the inferior renal artery in 30 mm [ 21 ]  . 
it still remains to be determined a diameter the type and efficacy of treatment in cases of complications such as type ia endoleaks with this polymer - based device . mechanical differences between endografts the influence of various stentgrafts on the infrarenal neck influence on the diameter the chronic outward radial pressure exerted on the aaa neck by the nitinol - skeleton endografts has been implicated in the aaa neck distention which facilitates dislodgement of the endograft and migration with resultant loss of sealing and generation of central endoleaks . 
observed no significant neck dilatation in a series of aaa treated with balloon - expandable stent - grafts ( bes ) in a mean follow - up period of 31 months [ 23 ] , while monahan et al . 
measured no significant neck enlargement in any of 88 aaa patients treated with the ovation stent - graft in a multicenter registry of 161 patients with a mean follow - up period of 32 months [ 27 ]  . 
so , it seems that stent - grafts that ensure their sealing without exerting a continuous radial force protect the aaa infrarenal neck from enlargement and consequent need for future interventions . introducing endovascular aneurysm sealing ( evas ) influence on angulation the endovascular aneurysm sealing ( evas ) philosophy was recently introduced with the nellix system ( endologix , inc , irvine , ca , usa ) and offers an alternative approach to endovascular treatment of aaa . 
this endograft consists of dual balloon - expandable endoframes , each surrounded by a polymer - filled endobag , to achieve anatomical fixation it is well known that the aortic neck angulation ( suprarenal and infrarenal ) decreases during and after evar [ 28 ]  . 
reported that the suprarenal angle decreased immediately after evar and continued to decrease during the first month , unlike the infrarenal aortic angle that continued to decrease slowly thereafter [ 29 ]  . 
reported a continuous post - evar decrease of both the suprarenal and infrarenal angles for the talent and the excluder endografts , in a period extending up to 3 years [ 28 ]  . 
the endurant was presumed to have better flexibility due to its nitinol - based skeleton , whereas the zenith with its construction of stainless steel showed a better straightening ability [ 30 ]  . 
have recently demonstrated a significantly greater post - evar decrease in suprarenal neck angulation in the ovation - treated aaa patients when compared with the endurant device [ 31 ]  . 
this change was attributed to the combination of the longer suprarenal stent and the rigid , solidified polymer - filled sealing rings of the ovation endograft . the impact of stent configuration on the iliac limbs of endografts graft limb occlusion represents an important cause of secondary intervention after evar . 
apart from the anatomical ( narrow aortic bifurcation , small diameter , stenosis , calcification , tortuosity and angulation of the iliac arteries ) and technical issues ( extreme oversizing , extension to the external iliac artery ) there are certain devicerelated factors that predispose to iliac limb occlusion [ 32 ]  . 
 the currently available endografts have iliac limbs with a different stent configuration : z - shaped ( talent , endurant , zenith lp ) ; spiral - shaped ( aorfix , excluder ) and circular ( anaconda ) .these variations may result in different adaptations of the graft limb to the iliac anatomy , especially in cases of severe angulation or nonuniform diameter landing zones [ 32 ]  . 
since the iliac limb graft occlusion represent an important cause of reintervention after evar , it becomes apparent that further research should focus on comparing spiral , circular and z - shaped stents of various endografts . the influence of endograft implantation on pulse wave reflection the implantation of an aortic stent - graft for treatment of aaa has been shown to influence the aortic stiffness quite early postoperatively [ 35 , 36 ]  . 
moreover , the increase of aortic systolic blood pressure due to wave reflections ( augmentation index , ai ) represents an additional marker of arterial stiffness [ 41 ]  . the arrival time of the backward pressure waves has a crucial role ; if this reflected pressure wave component arrives before the aortic valve closure , then the left ventricular afterload will be elevated and additional myocardial work will be needed to overcome this . 
the critical issue of myocardial performance remains the most critical task to be investigated postinterventionally , since previous studies have associated pwv and ai with adverse cardiovascular events [ 4042 ]  . in vitro studies a variety of in vitro studies have been conducted to evaluate the performance of the different endografts . 
six different endografts ( treovance , zenith flex , zenith lp , endurant , talent , and anaconda ) were deployed in fresh bovine aortas and pulled out with a pull - axis angulation ranging from 0 to 90 ( in increments of 10 )  . 
this study showed that increasing angulation was inversely correlated to the magnitude of the force needed to destabilize a given endograft , while also showing the extra resistance to dislodgement attributed to the combination of supraand infrarenal fixation of treovance in certain degrees of angulation [ 44 ]  . additionally , melas et al . 
they reported that that endografts equipped with fixation hooks and barbs ( zenith , anaconda , endurant and excluder ) displayed a significantly higher df necessary to dislocate the proximal part of the endograft compared with devices with no such fixation modalities ( talent , powerlink , endofit ) following full graft deployment with balloon dilatation [ 45 ]  . direct comparison of anatomic suitability of different endografts in aaa the anatomic suitability for evar according to the instructions - for - use ( ifu ) of three commercially available bifurcated grafts ( zenith flex , excluder , endurant ) was recently compared by kristmundson et al . 
the anatomic suitability of these aaa for each of the aforementioned alternative endografts ( zenith , excluder , talent ) was 52 , 60 , 73 and 81% , respectively . 
the endurant showed the greatest suitability , but a significant proportion of patients were still treated outside the ifu . comparing the clinical efficacy between various endografts in a retrospective comparison between newer endografts ( endurant , zenith , low - porosity excluder and 2nd generation anaconda ) and older ones ( aneurx , fortron , talent , 1st generation excluder and 1st generation anaconda ) , verzini et al . 
 endurant stent - graft has been well reported in the literature [ 5052 ]  . post - evar regression of the aneurysmal sac is an accepted indicator of aneurysm exclusion and clinical success . 
studied the effect of the stent - graft type on aneurysm shrinkage in 1450 patients undergoing evar at a single center over a 10 - year period [ 53 ]  . 
the authors compared the outcomes between the zenith and the excluder in short aortic necks < 15 mm and infrarenal angulation < 60 , documenting no difference in the incidence of migration and type ia endoleaks [ 55 ]  . postimplantation syndrome ( pis ) post - implantation syndrome is a relatively common complication of evar used to treat aaas and it is associated with features of a systemic inflammatory response and prolongation of hospitalization coagulation disturbances and an increase in inflammatory markers in patients blood [ 15 ]  . 
one study advocates that suprarenal fixation , when compared directly with infrarenal fixation , is associated with a decline in renal function ( as a drop in glomerular filtration rate ) at 12 - month follow - up [ 58 ]  . 
however , the majority of studies as well as a recent meta - analysis failed to identify a difference in the risk of postoperative renal complications between the two fixation methods [ 5961 ]  . discussion comparing the various endografts is not an easy task . 
the time needed for assessment and analysis of evidence from the rct poses a difficulty in keeping up with the rapid evolving technology and evolution of the stent - grafts [ 62 ]  . 
however , the bias in the selection of cases , the lack of a modern , detailed , standardized documentation system of the anatomic characteristics of aaas , the under - reporting of the least favorable results and the variable experience among centers make the direct comparison between stent - grafts difficult , hence restricting the endografts comparison between those of older and newer generations . 
on a practical basis , the disadvantage of the majority of newer endografts is their lack of long - term follow - up data , while the most practical reason of suboptimal performance of endografts is their use outside their instructions - for - use , as clearly depicted by shanzer et al . 
for example , different length ratios between the inlet ( mainbody ) and the outlet ( iliac limbs ) in various endograft designs appropriate for a given aaa are associated with variable predisposition for dissociation of the modular components and resultant endoleak type iii . 
moreover , while the nitinol - based self - expanding newer endografts exert continuous radial force onto the aortic neck leading to aortic neck dilatation , the newer endografts with fixation based on polymer inflation may serve better aaa with marginal aortic neck diameters , acting no outward force and eliminating the aortic neck enlargement [ 64 ]  . 
however , their long - term results are not well documented nor the kind , applicability and efficiency of the rescuing maneuvers needed in case of technical failures or late onset complications . 
more specifically , in the case of a type ia endoleak , placement of a palmaz stent or a fenestrated cuff may not be possible in evar patients treated with the polymerbased endografts . non - invasive modalities of assessing and comparing the effect of different endograft designs on central hemodynamics of recipients may not only help in the improvement of future endograft designs but also contribute to the 1 3 316 radiol med ( 2017 ) 122 : 309318 optimal choice for patients with a given impairment of myocardial function . 
it has been reported that the endoskeleton of the endograft ( nitinol , stainless steel of cobalt alloy ) decreases the compliance and increases the stiffness of the aorta while the resultant mismatch in the mechanical properties between the native and the stented aorta can cause increase in pwv and in the reflection of the pressure waves . 
however , it is not easy to predict the magnitude and the exact impact of the endoskeleton , mainly due to ( a ) the unique interaction between each endografts stent and fabric material , ( b ) the configuration of the stent struts in each device . 
most interestingly , while some endografts ( endurant ii and excluder ) induced a decrease of compliance at the infrarenal region by 1021% , other nitinolbased devices with suprarenal fixation ( zenith ) were not associated with significant decrease of compliance at the infrarenal region [ 66 ]  . 
it should be noted that the literature dealing with stiffness changes after evar is rather limited and focuses exclusively on pwv with no respect to the influence of endografts on the reflexed ( backward ) pressure wave . 
so , studying the pulse wave hemodynamic parameters in evar constitutes a new scientific area of growing interest . to conclude , current technology provides a wide variety of endograft structural designs and geometric patterns enabling the physician to approach a more patient - specific treatment of aaa . 
the cmr protocol included t2 - weighted ( oedema ) , early ( hyperaemia ) and late ( fibrosis / necrosis ) gadolinium enhancement sequences , according to lake louise criteria . 
quantitative outcomes were checked for normality and compared with the non - parametric wilcoxons test for matched data . results at the clinical follow - up all patients were free of symptoms and reported no cardiac complications . 
by using these indications cmr achieved high diagnostic accuracy ( 78% ) with estimated specificity of 91% [ 2 ]  . the clinical presentation of acute myocarditis is variable [ 3 ] , ranging from a subclinical disease to an infarctlike syndrome , arrhythmias , heart failure and cardiogenic shock ; for infarct - like myocarditis , the cmr sensitivity has been recognized to be very high ( 80% ) [ 4 ] , and in fact suspicion of myocarditis represents one of the most frequent indications to cmr . 
all patients had a low cardiovascular risk factor profile ; invasive coronary angiography excluded the presence of significant coronary artery disease in all of the the cmr exams were performed after a mean time of 8 days ( 412 ) after the onset of symptoms . 
a second cmr examination was performed at the same time of the clinical follow - up at 6 months . at the moment of the cmr examination , all patients were informed about the possible use of their data for study purposes and signed an informed consent for patients information was anonymized prior to the analysis . 
the study is a retrospective trial without any study - related clinical intervention and conforms to the helsinki declaration . cmr protocol cmr imaging was performed with a 1.5 - tesla scanners ( achieva , version 2.6 , philips medical systems , eindhoven , the netherlands ) using a body and phased array coil ( 32 - channel )  . cine steady - state free precession ( cine - ssfp ) cmr images were acquired in the 4 - chamber planes , 2 - chamber , 3 - chamber and short - axis . 
the t2 - weighted short tau inversion recovery ( t2w - stir ) images were acquired firstly on long - axis and then on short - axis planes covering the entire left ventricle during 68 consecutive breath - holds . 
lv end - diastolic volume ( lvedv ) , lv end - systolic volume ( lvesv ) , ejection fraction ( ef ) , and lv mass were determined . t2w - stir images were visually assessed for the presence and extension of hyperintense areas , which identified the presence of myocardial oedema . 
the t2 ratio was calculated as the ratio between the signal intensity of the damaged myocardium to the signal intensity of a skeletal muscle , generally a paraspinal muscle ( drawing two roi in the same image )  . 
 [ 2 , 21 ]  . early gadolinium enhancement ratio ( ege ratio ) was calculated by tracing endocardial and epicardial contours on pre and post - contrast images and placing a reference roi on the skeletal muscle located within the same slice 1 3 radiol med ( 2017 ) 122 : 273279 in order to normalize myocardial enhancement as for the t2 - ratio . 
the spatial extent of these lesions was quantified ( areas with signal intensity at least 3 standard deviations greater than for normal myocardium ) [ 22 ] and was expressed as a percentage of the total myocardial volume . 
the signal intensity ratio between lge area and healthy myocardium ( lge ratio ) was also evaluated . clinical and radiological followup the clinical and cmr follow - ups were performed on the same day . the clinical assessment included a complete cardiologic visit with echocardiogram and both a standard 12 - lead ecg and a holter - ecg . 
the cmr follow - up was performed with the same protocol used in the acute stage . statistical analysis continuous variables were checked for normality with the kolmogorov / lilliefors test , shapirowilk w test and dagostinos tests . 
from the left to right : left ventricular ejection fraction ( lvef ) , left ventricular end - diastolic volume index ( lvedvi ) and left ventricular mass index ( lv mass i )  . 
in summary , we found : good clinical - laboratory evolution of all patients ; reduction in cmr parameters of inflammation and reduction , but with persistence of lge changes . to the best of our knowledge , there are only two studies focused on the follow - up of patients with infarct - like myocarditis . 
 [ 6 ] found that none of their patients reported arrhythmias or further cardiac complications , no cases of persisting oedema on t2 - weighted sequences were reported , late enhancement decreased in 20 of 21 patients and the ejection fraction remained stable or improved in all patients . 
 [ 14 ] found an association between infarct - like myocarditis and major cardiovascular events ( mace ) occurrence and identified nyha functional class > ii and lge as independent predictor of mace . 
encountered some mace already in the first 6 months , but on the other hand also dantis [ 6 ] patients were free of events during the first few months . according to the american heart association ( aha ) and american college of cardiology ( acc ) guidelines [ 23 ] , the interval between initial assessment and retesting before resumption of any sports activity will vary depending on the severity of the initial illness . 
from the top to the bottom : 4 chamber , 3 chamber and short - axis view and from right to left : acute mr and follow - up mr . 
on this basis , we usually scheduled follow - up studies at about 6 months . at clinical follow - up all patients were free of symptoms , no arrhythmias or further cardiac complications were reported and all laboratory data were normalized . 
 [ 24 ] concluded that patients with an increase of lvef by 20% or an lvef > 50% , and a low nyha functional class at 6 months demonstrated an excellent long - term prognosis . 
 these data demonstrate that the diagnosis of complete clinical recovery of infarct - like myocarditis was associated with the reduction in cmr parameters of inflammation , in agreement with the definition of reversible injuries [ 7 ]  . previous studies demonstrated that the presence of lge is the best independent predictor of major cardiovascular events in patients with myocarditis [ 10 , 11 , 14 ]  . 
third , the lack of adverse events in the follow - up , while being an excellent result for the patients , did not allow us to identify any cmr parameters as possible predictors of adverse clinical outcome . 
in particular , a number of diseases show hypertrophy and enlargement of the bronchial circulation with consequential increase in vessel fragility [ 1 ]  . life - threatening or recurrent haemoptysis is an emerging complication in subjects with pulmonary hypertension ( ph ) [ 4 , 5 ]  . 
 the latter included four ( 44.4% ) patients with chronic thromboembolic pulmonary hypertension ( cteph ) , three ( 33.3% ) with idiopathic pulmonary arterial hypertension 4 / 8 , average age 38.96 3 / 6 , average age 9 , m / f 35.55 ( ipah ) , and two ( 22.2% ) with heritable pulmonary arterial hypertension ( hpah )  . 
beyond the 33 selected patients , 2 more patients underwent bae for haemoptysis in the selected period , who were excluded because they were lost to follow - up and no information about haemoptysis recurrence and survival was available in the following 12 months . 
demographics , laboratory , and clinical data were collected and compared between each group ( table 1 ) ; moreover , metrics from right heart catheterisation ( rhc ) were compared between chd - apah and nonchd - apah subgroups ( table 2 )  . 
follow - up at 30 and 90 days from bae was collected for all subjects , and overall survival was calculated for the ph group and compared between its two subgroups . bronchial artery embolization all the bae procedures were performed by an interventional radiologist with 15 years of experience in interventional radiology . after local anaesthesia , vascular access was obtained via transfemoral and / or transbrachial approach , according to the origin and the course of the arteries to be embolized . 
 after the embolization of the target arteries , a final angiographic scan was carried out to ascertain the full occlusion of the selected vessel and to detect possible collateral blood supply from both bronchial and non - bronchial circulation . 
all vardata were presented as mean iables were analysed with descriptive methods ; cross - tabulations were checked with chi - squared test or by fishers exact test , and anova test as appropriate . 
at the time of haemoptysis , 6 / 21 ph patients ( 28.5% ) were under anticoagulant therapy and 17 / 21 ( 80.9% ) were receiving specific medication for ph . 
permanent embolic agents were used as follows : in 21 procedures ( 65.6% ) , we used particles such as polyvinyl alcohol ( pva ) ( contour , boston scientific corporation , maple grove , mn ) , with a diameter ranging between 150 and 1000 m , more often 250350 and 350500 in five procedures ( 15.6% ) , we used n - butyl 2 - cyanoacrylate ( glubran , gem srl , viareggio , italy ) ; pushable metal microcoils ( hilal , cook group inc , bloomington , in ) were used twice ( 6.3% ) , together with pva particles on one of those occasion . 
haemostasis was achieved both manually and by means of a vascular closure device ( exoseal , cordis corporation , bridgewater , nj )  . a total of 67 arteries were embolized as follows : 59 bronchial arteries and eight non - bronchial systemic arteries . 
procedure - related death occurred in one patient with ipah who presented with sudden onset of dyspnoea , diaphoresis , and tachycardia during bae , followed by rapid deterioration of the clinical condition 1 3 radiol med ( 2017 ) 122 : 257264 fig . 
2 a , b an intercostobronchial trunk ( ibt ) , arising from aorta , from which originate an intercostal artery and a right bronchial artery ( a )  . 
chd - apah congenital heart diseaseassociated pah the endovascular treatment of haemoptysis by bae led to improvement of patient management , notably prompt control of bleeding in a range of otherwise untreatable comorbidities [ 27 ]  . 
the treatment of haemoptysis of ph is indeed a relatively low invasive procedure to control the acute onset of pulmonary bleeding in subjects with weak cardiopulmonary dynamic [ 28 ]  . 
as a background note , the chronic onset of bronchial artery hypertrophy causes a particular increase in number of bronchial arteries and morphological distortion that are limiting factor of endovascular treatment of bae in ph [ 29 ]  . 
we also found higher average inr values in the non - chd - apah group , which could be explained by the high proportion of cteph patients ( 44.4% ) , in which life - long anticoagulation therapy is recommended , while in pah patients , the need for an anticoagulation therapy is still debated [ 5 , 31 ]  . despite this is the largest cohort in the literature about the efficacy of bae in the treatment of haemoptysis in ph , fig . 
4 two right bronchial arteries with ectopic origin arising from a thyrocervical trunk 1 3 radiol med ( 2017 ) 122 : 257264 the size still represents a major study limitation . 
however , it allowed us to demonstrate that bae is a useful procedure for immediate haemoptysis control , while further studies are needed to confirm whether urgent lung transplantation is a valid and viable solution in ph patients . 
more studies are required to confirm whether there is no difference in bae complications in these more complex procedures when they are operated by radiologists with different levels of expertise , and whether specific training might be needed . conclusion we showed that bae may be an effective and safe procedure for the treatment of acute haemoptysis in ph patients . 
 bae in ph patients is more complex compared to procedures in subjects without ph because there are a higher number of arteries to be treated and there is more anatomical and morphological variability . 
bae repetition can be useful for haemoptysis control and to improve the quality of life in patients with a chronic pulmonary disease like ph , which seems to have a higher relapsing rate than other conditions associated with haemoptysis . compliance with ethical standards the study was approved by our institutional ethics committee . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
georgiadis1 received : 6 august 2016 / accepted : 3 january 2017 / published online : 21 january 2017 italian society of medical radiology 2017 abstract endovascular repair of abdominal aortic aneurysms has widely replaced the open surgical repair due to its minimal invasive nature and the accompanying lower perioperative mortality and morbidity . 
during the past two decades , certain improvements and developments have provided a wide variety of endograft structural designs and geometric patterns , enabling the physician to approach a more patient - specific treatment of aaa . 
this review presents the currently available aortic endografts and describes the clinical , technical and mechanical characteristics of them . keywords aortic stent - graft clinical performance abdominal aortic aneurysm hemodynamics endovascular aneurysm repair introduction since its introduction in 1991 , the endovascular repair ( evar ) of abdominal aortic aneurysms ( aaa ) has been widely accepted by physicians and patients due to its minimal invasive nature and its lower perioperative mortality and morbidity [ 1 , 2 ]  . 
the correct choice of stent - graft decreases the complication rate and the need for reinterventions . materials used for the graft covering include polyester and polytetrafluoroethylene ( ptfe ) , whereas stent composition includes stainless steel , nitinol and cobalt chromium alloy . 
some endografts have passive fixation using their radial support and columnar strength and others present active fixation with pins , hooks and barbs . the long - lasting clinical efficacy ( aaa sac exclusion from systematic pressure , avoidance of sac expansion or rupture ) and incidence of complications leading to need for major interventions are the crucial reference issues when comparing the various endografts . 
 moreover , apart from any form of clinical studies , in vitro laboratory studies provide additional information about the biomechanical properties of various endografts patterns and designs or the impact of the latter on the central hemodynamics of the patients . this article provides useful clinical and hemodynamic information for the endografts commercially available and discusses the major drawbacks and limitations between current data . 
this endograft lacks suprarenal fixation and should be used , therefore , with caution in cases of aaa with considerable angulation but limited infarenal neck length . the endurant ii ( medtronic , santa rosa , ca , usa ) is a modular - bifurcated stent - graft composed of nitinol stents and polyester grathe combination of the m - shaped configuration of nitinol stents and improved suprarenal active fixation with anchoring pins provides better resistance to migration in short and angulated proximal aortic necks [ 7 ]  . 
one should bear in mind that after the deployment of the main body and before the removal of the delivery system , it is necessary to recapture the spindle in the tapered tip . 
this is the most important step as failure to withdraw the delivery system until the spindle is retracted into the fabric portion of the stent - graft can result in trapping of a suprarenal crown within the tapered tip sleeve [ 9 ]  . the treovance abdominal stent - graft ( bolton medical , barcelona , spain ) is a tightly woven polyester nitinol trimodular endograft with a main bifurcated stent - graft and two leg extensions . 
the main body comes in three different lengths while the overlapping length between the main body and the limb extension is adjustable ( 40 mm adjustable landing zone for the ipsilateral and 10 mm for the contralateral limb )  . 
notably , the iliac gates have five dull barbs to withstand the displacement forces tending to separate the limbs from the main component , thus eliminating the incidence of endoleaks type iii [ 10 ]  . 
the endograft should be handled with care in rather small access vessels since its relatively large profile and stiffness of its delivery device may cause problems related to such arteries [ 11 ]  . the zenith flex ( cook medical , bloomington , usa ) is a modular - bifurcated system consisting of a stainless steel z - stents sutured to a woven polyester graft material . 
on the other hand , the new zenith low profile is constructed of nitinol stents instead of stainless steel with a thinner polyester material and its new 16 fr delivery system down - sizes the iliac access diameter available for insertion and navigation of the particular endograft to 6 mm and is associated with promising mid - term results in unfavorable iliac anatomies [ 12 ]  . the incraft stent - graft ( cordis , bridgewater , nj , usa ) is designed to overcome the limitation of the small diameter of the access vessels . 
it is a trimodular - bifurcated device constructed of a seamless , low porosity , woven polyester graft supported by a series of self - expanding nitinol stents throughout the entire grasuture knots on the outer surface of the limb prosthesis comprise an interlocking mechanism to eliminate the risk of limb separation . 
the unavailability of aortic extensions in cases of central endoleaks should be taken into consideration when handling challenging infrarenal necks [ 13 ]  . the anaconda one lok stent - graft ( vascutek , uk ) is a three - piece device made of nitinol rings and a polyester graits active infrarenal fixation is accomplished via eight hooks while a magnet system facilitates the cannulation of the contralateral gate [ 14 ]  . 
there are reports depicting high incidence of post - implantation syndrome with this particular endogra [ 15 ]  . the e - vita stent - graft ( jotec , hechingen , germany ) is a modular two - piece endograft with suprarenal fixation composed of polyester fabric and nitinol stents [ 16 ]  . 
most notably , the first nitinol stent of the cranial top has a multiple - tip design to improve the apposition onto an infrarenal neck of marked calcification , or irregular shape . 
the current lack of midor long - term follow - up data precludes its generalized use for the time being . the aorfix stent - graft ( lombard medical technologies , oxfordshire , uk ) possesses cranial rings with a fishmouth 1 3 312 radiol med ( 2017 ) 122 : 309318 shape . 
it has been reported that failure of the cup segment to track and follow adequately the iliac rotating manipulations can result in inadequate orientation of the central fish - mouth with respect to the renal artery ostium , comprising the achilles heel of the aorfix device [ 18 , 19 ]  . in the aneurysm sac , dissociating the sealing efficiency from the shape and contour of the proximal aortic neck . 
the nellix stent - graft is particularly suitable for patients with conical necks as the endobags apply on the entire length of the conical neck elongating the sealing zone [ 22 ]  . 
however , the long - term follow - up is not yet determined nor the type , applicability and efficiency of the treatment modalities in case of immediate or late on set complications . direct accommodation onto the aortic bifurcation the afx stent - graft ( endologix , inc , irvine , ca , usa ) is a unibody endograft based on the concept of anatomic fixation . 
the cobalt chromium stents of the afx device are sutured only at the proximal and distal ends of the inner surface of the graft material , allowing flexibility of the graft material . 
the ovation stent - graft does not depend on the length of neck as long as the first ring seals 13 mm below the inferior renal artery in 30 mm [ 21 ]  . 
it still remains to be determined a diameter the type and efficacy of treatment in cases of complications such as type ia endoleaks with this polymer - based device . mechanical differences between endografts the influence of various stentgrafts on the infrarenal neck influence on the diameter the chronic outward radial pressure exerted on the aaa neck by the nitinol - skeleton endografts has been implicated in the aaa neck distention which facilitates dislodgement of the endograft and migration with resultant loss of sealing and generation of central endoleaks . 
observed no significant neck dilatation in a series of aaa treated with balloon - expandable stent - grafts ( bes ) in a mean follow - up period of 31 months [ 23 ] , while monahan et al . 
measured no significant neck enlargement in any of 88 aaa patients treated with the ovation stent - graft in a multicenter registry of 161 patients with a mean follow - up period of 32 months [ 27 ]  . 
so , it seems that stent - grafts that ensure their sealing without exerting a continuous radial force protect the aaa infrarenal neck from enlargement and consequent need for future interventions . introducing endovascular aneurysm sealing ( evas ) influence on angulation the endovascular aneurysm sealing ( evas ) philosophy was recently introduced with the nellix system ( endologix , inc , irvine , ca , usa ) and offers an alternative approach to endovascular treatment of aaa . 
this endograft consists of dual balloon - expandable endoframes , each surrounded by a polymer - filled endobag , to achieve anatomical fixation it is well known that the aortic neck angulation ( suprarenal and infrarenal ) decreases during and after evar [ 28 ]  . 
reported that the suprarenal angle decreased immediately after evar and continued to decrease during the first month , unlike the infrarenal aortic angle that continued to decrease slowly thereafter [ 29 ]  . 
reported a continuous post - evar decrease of both the suprarenal and infrarenal angles for the talent and the excluder endografts , in a period extending up to 3 years [ 28 ]  . 
the endurant was presumed to have better flexibility due to its nitinol - based skeleton , whereas the zenith with its construction of stainless steel showed a better straightening ability [ 30 ]  . 
have recently demonstrated a significantly greater post - evar decrease in suprarenal neck angulation in the ovation - treated aaa patients when compared with the endurant device [ 31 ]  . 
this change was attributed to the combination of the longer suprarenal stent and the rigid , solidified polymer - filled sealing rings of the ovation endograft . the impact of stent configuration on the iliac limbs of endografts graft limb occlusion represents an important cause of secondary intervention after evar . 
apart from the anatomical ( narrow aortic bifurcation , small diameter , stenosis , calcification , tortuosity and angulation of the iliac arteries ) and technical issues ( extreme oversizing , extension to the external iliac artery ) there are certain devicerelated factors that predispose to iliac limb occlusion [ 32 ]  . 
 the currently available endografts have iliac limbs with a different stent configuration : z - shaped ( talent , endurant , zenith lp ) ; spiral - shaped ( aorfix , excluder ) and circular ( anaconda ) .these variations may result in different adaptations of the graft limb to the iliac anatomy , especially in cases of severe angulation or nonuniform diameter landing zones [ 32 ]  . 
since the iliac limb graft occlusion represent an important cause of reintervention after evar , it becomes apparent that further research should focus on comparing spiral , circular and z - shaped stents of various endografts . the influence of endograft implantation on pulse wave reflection the implantation of an aortic stent - graft for treatment of aaa has been shown to influence the aortic stiffness quite early postoperatively [ 35 , 36 ]  . 
moreover , the increase of aortic systolic blood pressure due to wave reflections ( augmentation index , ai ) represents an additional marker of arterial stiffness [ 41 ]  . the arrival time of the backward pressure waves has a crucial role ; if this reflected pressure wave component arrives before the aortic valve closure , then the left ventricular afterload will be elevated and additional myocardial work will be needed to overcome this . 
the critical issue of myocardial performance remains the most critical task to be investigated postinterventionally , since previous studies have associated pwv and ai with adverse cardiovascular events [ 4042 ]  . in vitro studies a variety of in vitro studies have been conducted to evaluate the performance of the different endografts . 
six different endografts ( treovance , zenith flex , zenith lp , endurant , talent , and anaconda ) were deployed in fresh bovine aortas and pulled out with a pull - axis angulation ranging from 0 to 90 ( in increments of 10 )  . 
this study showed that increasing angulation was inversely correlated to the magnitude of the force needed to destabilize a given endograft , while also showing the extra resistance to dislodgement attributed to the combination of supraand infrarenal fixation of treovance in certain degrees of angulation [ 44 ]  . additionally , melas et al . 
they reported that that endografts equipped with fixation hooks and barbs ( zenith , anaconda , endurant and excluder ) displayed a significantly higher df necessary to dislocate the proximal part of the endograft compared with devices with no such fixation modalities ( talent , powerlink , endofit ) following full graft deployment with balloon dilatation [ 45 ]  . direct comparison of anatomic suitability of different endografts in aaa the anatomic suitability for evar according to the instructions - for - use ( ifu ) of three commercially available bifurcated grafts ( zenith flex , excluder , endurant ) was recently compared by kristmundson et al . 
the anatomic suitability of these aaa for each of the aforementioned alternative endografts ( zenith , excluder , talent ) was 52 , 60 , 73 and 81% , respectively . 
the endurant showed the greatest suitability , but a significant proportion of patients were still treated outside the ifu . comparing the clinical efficacy between various endografts in a retrospective comparison between newer endografts ( endurant , zenith , low - porosity excluder and 2nd generation anaconda ) and older ones ( aneurx , fortron , talent , 1st generation excluder and 1st generation anaconda ) , verzini et al . 
 endurant stent - graft has been well reported in the literature [ 5052 ]  . post - evar regression of the aneurysmal sac is an accepted indicator of aneurysm exclusion and clinical success . 
studied the effect of the stent - graft type on aneurysm shrinkage in 1450 patients undergoing evar at a single center over a 10 - year period [ 53 ]  . 
the authors compared the outcomes between the zenith and the excluder in short aortic necks < 15 mm and infrarenal angulation < 60 , documenting no difference in the incidence of migration and type ia endoleaks [ 55 ]  . postimplantation syndrome ( pis ) post - implantation syndrome is a relatively common complication of evar used to treat aaas and it is associated with features of a systemic inflammatory response and prolongation of hospitalization coagulation disturbances and an increase in inflammatory markers in patients blood [ 15 ]  . 
one study advocates that suprarenal fixation , when compared directly with infrarenal fixation , is associated with a decline in renal function ( as a drop in glomerular filtration rate ) at 12 - month follow - up [ 58 ]  . 
however , the majority of studies as well as a recent meta - analysis failed to identify a difference in the risk of postoperative renal complications between the two fixation methods [ 5961 ]  . discussion comparing the various endografts is not an easy task . 
the time needed for assessment and analysis of evidence from the rct poses a difficulty in keeping up with the rapid evolving technology and evolution of the stent - grafts [ 62 ]  . 
however , the bias in the selection of cases , the lack of a modern , detailed , standardized documentation system of the anatomic characteristics of aaas , the under - reporting of the least favorable results and the variable experience among centers make the direct comparison between stent - grafts difficult , hence restricting the endografts comparison between those of older and newer generations . 
on a practical basis , the disadvantage of the majority of newer endografts is their lack of long - term follow - up data , while the most practical reason of suboptimal performance of endografts is their use outside their instructions - for - use , as clearly depicted by shanzer et al . 
for example , different length ratios between the inlet ( mainbody ) and the outlet ( iliac limbs ) in various endograft designs appropriate for a given aaa are associated with variable predisposition for dissociation of the modular components and resultant endoleak type iii . 
moreover , while the nitinol - based self - expanding newer endografts exert continuous radial force onto the aortic neck leading to aortic neck dilatation , the newer endografts with fixation based on polymer inflation may serve better aaa with marginal aortic neck diameters , acting no outward force and eliminating the aortic neck enlargement [ 64 ]  . 
however , their long - term results are not well documented nor the kind , applicability and efficiency of the rescuing maneuvers needed in case of technical failures or late onset complications . 
more specifically , in the case of a type ia endoleak , placement of a palmaz stent or a fenestrated cuff may not be possible in evar patients treated with the polymerbased endografts . non - invasive modalities of assessing and comparing the effect of different endograft designs on central hemodynamics of recipients may not only help in the improvement of future endograft designs but also contribute to the 1 3 316 radiol med ( 2017 ) 122 : 309318 optimal choice for patients with a given impairment of myocardial function . 
it has been reported that the endoskeleton of the endograft ( nitinol , stainless steel of cobalt alloy ) decreases the compliance and increases the stiffness of the aorta while the resultant mismatch in the mechanical properties between the native and the stented aorta can cause increase in pwv and in the reflection of the pressure waves . 
however , it is not easy to predict the magnitude and the exact impact of the endoskeleton , mainly due to ( a ) the unique interaction between each endografts stent and fabric material , ( b ) the configuration of the stent struts in each device . 
most interestingly , while some endografts ( endurant ii and excluder ) induced a decrease of compliance at the infrarenal region by 1021% , other nitinolbased devices with suprarenal fixation ( zenith ) were not associated with significant decrease of compliance at the infrarenal region [ 66 ]  . 
it should be noted that the literature dealing with stiffness changes after evar is rather limited and focuses exclusively on pwv with no respect to the influence of endografts on the reflexed ( backward ) pressure wave . 
so , studying the pulse wave hemodynamic parameters in evar constitutes a new scientific area of growing interest . to conclude , current technology provides a wide variety of endograft structural designs and geometric patterns enabling the physician to approach a more patient - specific treatment of aaa . 
detailed information regarding the influence of aaa endografts on central hemodynamics and myocardial performance in the long term is awaited . compliance with ethical standards conflict of interest the authors declare that there is no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2017 ) 122 : 294302 doi 10.1007 / s11547 - 016 - 0720 - 8 neuroradiology reproducibility of dynamic contrastenhanced mri and dynamic susceptibility contrast mri in the study of brain gliomas : a comparison of data obtained using different commercial software gian marco conte1 antonella castellano1 luisa altabella1 , 2 antonella iadanza1 marcello cadioli1 , 3 andrea falini1 nicoletta anzalone1 received : 21 september 2016 / accepted : 19 december 2016 / published online : 9 january 2017 italian society of medical radiology 2017 abstract purpose dynamic susceptibility contrast mri ( dsc ) and dynamic contrast - enhanced mri ( dce ) are useful tools in the diagnosis and follow - up of brain gliomas ; nevertheless , both techniques leave the open issue of data reproducibility . 
we evaluated the reproducibility of data obtained using two different commercial software for perfusion maps calculation and analysis , as one of the potential sources of variability can be the software itself . methods dsc and dce analyses from 20 patients with gliomas were tested for both the intrasoftware ( as intraobserver and interobserver reproducibility ) and the intersoftware reproducibility , as well as the impact of different postprocessing choices [ vascular input function ( vif ) selection and deconvolution algorithms ] on the quantification of perfusion biomarkers plasma volume ( vp ) , volume transfer constant ( ktrans ) and rcbv . 
comparisons of different vif estimation methods for dce biomarkers resulted in icc of 0.636 for ktrans and 0.662 for vp ; comparison of two deconvolution algorithms in dsc resulted in an icc of 0.999. conclusions the use of single software ensures very good intraobserver and interobservers reproducibility . 
most studies published on this topic used perfusion - derived biomarkers 1 3 radiol med ( 2017 ) 122 : 294302 for gliomas grading [ 15 ] , patients outcome prediction [ 6 11 ] and differentiation of tumor recurrence from treatmentrelated effects like radionecrosis and pseudoprogression [ 1216 ]  . however , reproducibility is still an open issue for both techniques : no standardized protocol for acquisition and analysis of perfusion techniques is still available and , consequently , different research groups have used different protocols , generating a wide range of results [ 1722 ]  . 
 recently some steps towards standardization have been made , with the publication of an evidenceand consensusbased standards document for dce [ 23 ] and a white paper for dsc [ 24 ]  . one of the potential sources of variability is the software chosen for perfusion map calculation and analysis [ 2532 ] since each software implements different analysis tools [ i.e. 
 leakage correction for dsc maps or automatic detection of vascular input function ( vif ) ] and sometimes different algorithms . the aim of this study was to test the reproducibility of data obtained from studying the same cohort of patient with two commercial software , which were chosen based on the rationale that they could be used independently from the mr machine available for the acquisition , thus reducing data spread and improving standardization of perfusion analysis . 
this study was approved by the ethical committee of our institution . dce analysis mr imaging was performed on a 3t scanner ( achieva , philips healthcare , best , the netherlands ) equipped with 80 mt / m gradients using a phased - array head 8 channelcoil . 
the total acquisition time for dscmri was 2 min and 4 s . a cumulative fixed dose of 10 ml of gadobutrol ( gadovist , 1 mmol / ml ; bayer schering pharma , 6 berlin , germany ) was administered , splitted in two boluses of 5 ml . 
the first bolus of 5 ml was injected 50 s after the start of the dce sequence using a power injector ( spectris solaris mr injector ; medrad , indianola , pennsylvania ) at a rate of 2 ml / s , immediately followed by a 20 ml continuous saline flush at the same injection rate . 
the second bolus of 5 ml was injected 16 s after the start of the dsc sequence using the same power injector at a rate of 5 ml / s , followed by a 20 ml saline flush at the same injection rate . 
 in both software , preprocessing steps included automatic motion correction by a rigid - body registration , automatic spatial smoothing and background segmentation . for dce analysis , patient - specific baseline t1 maps were derived from vfa axial sequences ( see online resource 1 for acquisition details )  . in both software dce analysis was based on the extended tofts model [ 33 ]  . 
in olea sphere both a manual venous vif and an automatic one were obtained ; the venous one was obtained from the sss , while the automatic one was obtained using a tool implemented in the software [ 34 ] , which selected both arteries and veins as sources of input . 
 parametric maps of volume transfer constant ( ktrans ) and plasma volume ( vp ) were then obtained . 1 3 296 dsc analysis in both software , dsc analysis was performed using the singular value decomposition ( svd ) algorithm for deconvolution [ 35 ]  . 
however , while olea sphere offers different methods for svd , and both the standard truncated svd ( ssvd ) and oscillation - index csvd ( osvd ) were used for analysis , in nordicice only ssvd was available . 
an arterial vif was obtained in olea sphere using an automatic method [ 34 ] while in nordicice it was obtained semi - automatically : the observer selected the axial slice of interest and then the software searched for a valid vascular signal . 
parametric maps of cerebral blood volume ( cbv ) were then obtained . a fixed hematocrit value of 0.45 was set in both software . image analysis all the parametric maps were independently analyzed by two observers ( gmc , with 3 years experience in perfusion analysis , na with 7 years experience in perfusion analysis )  . in both software , perfusion maps were automatically coregistrated with flair and / or post - contrast t1 images by performing a rigid transformation of the datasets . for each parametric map , multiple circular rois , 2530 mm2 in area , were drawn in the tumor area that showed the highest value of perfusion biomarkers , then the one showing the highest mean value for each perfusion biomarker was selected . 
to normalize cbv values , a single elliptic roi , 250300 mm2 in area , was drawn in the contralateral normal appearing white matter ( nawm ) in the centrum semiovale ( ncbv )  . 
the analysis was repeated after one month to assess intraobserver reproducibility . from dce analysis , for each parametric map and each observer three datasets were obtained : one with the automatic vif selection ( olea automatic ) and two with the manual vif selection ( olea manual and nordicice ) ; from dsc two datasets ( olea automatic and nordicice ) were obtained . moreover , to avoid any possible variability due to different rois positioning between observers , intersoftware reproducibility was re - tested drawing the rois in the same tumor area in the two software . 
mean value of selected rois was then used for the comparison . radiol med ( 2017 ) 122 : 294302 to test the impact of different postprocessing options on the quantitative data , additional analyses were performed using olea sphere : for dce , the reproducibility of data obtained using the automatic and the manual vif selection and for dsc the data obtained using the ssvd and osvd methods . 
moreover , especially in neuroimaging , some groups analyze pwi datasets using non ce and fda approved in - house software . the issue of the reproducibility of data derived from different software seems to be independent from imaging technique and anatomical district : previous studies focused on data obtained using different software or different versions of the same software in both ct - pwi [ 27 , 29 , 30 ] and mr - pwi [ 25 , 26 , 28 , 31 , 32 ]  . 
to our best knowledge , this study is the first reporting data on dce reproducibility in brain imaging . intrasoftware reproducibility regarding the intrasoftware analysis , we found good reproducibility for all comparisons ( table 1 )  . 
summary of icc values obtained in all comparisons ; upper and lower limits of the box represent the highest and lowest icc value obtained ; the central line represents the mean icc value obtained 1 3 radiol med ( 2017 ) 122 : 294302 both dsc and dce parameters ; moreover , the 95% confidence interval for icc values showed a wide range of results for all comparisons ( table 2 )  . 
3 comparison of automatic and manual vif selection in the same patient ; in this case automatic vif selection on dce maps shows both arterial ( a ) and venous ( b ) input ; manual vif selection on dce maps consists in venous input only ( d ) ; c , e concentration time curves show different peaks , with the one derived from automatic vif being lower . 
the curve derived from the manual vif is the mean of four different input located around the pixel selected ( e ) 1 3 300 radiol med ( 2017 ) 122 : 294302 fig . 
4 comparison of automatic and manual vif selection in the same patient ; in this case automatic vif selection on dce maps shows only venous input ( a , b ) ; manual vif selection on dce maps consists in venous input only ( d ) ; c , e concentration time curves shows similar peaks . 
the curve derived from the manual vif is the mean of four different input located around the pixel selected ( e ) deconvolution algorithms in dsc value , while some differences are expected in cbf when comparing osvd and ssvd [ 36 ]  . for dsc , one of the proposed factors that may affect reproducibility is the choice of the deconvolution algorithm [ 27 , 30 ]  . 
in our study dsc analyses were performed applying both different and same deconvolution algorithms in the two software , finding low intersoftware reproducibility , that only slightly increased from an icc of 0.4550.582 when selecting the same algorithm ( ssvd ) ( table 3 )  . 
it is possible that the choice of a different algorithm per se does not introduce significant variability ; this was proved comparing the data obtained using the two different svd methods in the same software , resulting in an almost perfect agreement with an icc of 0.999 ( table 4 )  . 
in the intersoftware comparison , a better reproducibility was obtained for both ktrans and vp when the vif was selected manually in both software ( tables 2 , 3 )  . 
our results show that this single change in postprocessing step has a significant impact on data as only moderate agreement was obtained , even if the rois were positioned in the same area and no other differences exist between the datasets compared ( table 4 )  . 
 probably the vif selection itself cannot entirely explain the poor reproducibility but it seems to play a major role in it . our study confirms the recent findings by orsingher [ 26 ] , milchenko [ 31 ] and kelm [ 32 ] , who also found low intersoftware reproducibility of dsc parameter cbv . 
it must be said , however , that a thorough training is necessary to obtain this result and the acquisition and analysis protocol must be followed very strictly . the poor intersoftware reproducibility and the impact of postprocessing options on data reproducibility have consequences on the design of follow - up studies , on the application of data published in literature and on the daily clinical routine use of perfusion analysis . 
it must be said , however , that , as shown in the work by kelm [ 32 ] , different diagnostic accuracy is unlikely to be found among different fda - cleared software . conclusions in conclusion , we found a very good intrasoftware reproducibility and poor intersoftware reproducibility for dce and dsc analyses , suggesting that while the use of a single software ensures reliable results , caution should be taken when comparing data obtained using different software and different postprocessing options , since the reproducibility in this case is not guaranteed anymore . compliance with ethical standards conflict of interest nicoletta anzalone served as a consultant for bayer healthcare . 
all the other authors declare that they have no potential conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
this article does not contain any studies with animals performed by any of the authors . funding no funding was received for this study . informed consent for this type of study formal consent is not required . radiol med ( 2017 ) 122 : 303308 doi 10.1007 / s11547 - 016 - 0722 - 6 radiotherapy late toxicity , evolving radiotherapy techniques , and quality of life in nasopharyngeal carcinoma luciana lastrucci1 roberta de majo1 andrea rampini1 paola pernici1 pietro giovanni gennari1 silvia bertocci1 vittorio bini2 simona borghesi1 received : 1 september 2016 / accepted : 19 december 2016 / published online : 9 january 2017 italian society of medical radiology 2016 abstract purpose to analyze quality of life ( qol ) and functional state ( fs ) by patient - reported outcome ( pro ) questionnaires ( fact - g , fact - np , pss - hn , xeqols , and eq5d - 3l ) in long - term survivors nasopharyngeal carcinoma ( npc ) treated with conventional radiotherapy ( rt ) and intensity modulated radiotherapy ( imrt )  . methods 25 patients answered to five questionnaires about qol and fs . 
the observed xerostomia was lower in the imrt group and in patients who received conventional rt had worse qol according to xeqols ( university of michigan xerostomia - related quality of life scale ) score questionnaire . 
epstein barr virus ( ebv ) is , with smoke , alcohol , and wood dust - related occupations , among the well - known risk factors for this tumor . 
most stage iii tumors are successfully treated by radical radiotherapy ( rt ) , while patients with locoregionally advanced disease ( stage iii - iv ) are cured by combined chemoradiotherapy ( crt ) approach [ 6 ]  . 
over the years , rt techniques evolved : intensity modulated radiotherapy ( imrt ) , compared to the conventional bi - dimensional and tri - dimensional conformal rt ( 2d and 3d - crt ) achieved good tumor coverage , high tumor control rate , and effectively lowered the exposure dose of normal tissues around the tumor , reducing temporal lobe injury , xerostomia , hearing loss , trismus , cataract , retinitis , and damage to brain stem and optic chias traditionally , treatment evaluation has focused on objective measures like survival time , tumor recurrence , overall survival , or standardized toxicity [ 79 ] , but few studies has evaluated a possible impact of treatment on health - related quality of life ( hrqol ) and functional status ( fs ) in patients with head and neck cancer . 
in this study , we used five questionnaires to retrospectively analyze qol , fs , and 1 3 304 radiol med ( 2017 ) 122 : 303308 their correlation to late toxicity , treatment , and patientrelated parameters in long - term npc survivors . 
 the use of more questionnaires ( each one focused on different aspects ) allowed us to have a complete description of patients fs and qol . materials and methods between january 1990 and december 2014 , 56 patients with histologically proven npc have consecutively been treated with rt alone or crt at the radiation oncology unit of the san donato hospital arezzo . 
in december 2014 , at different time after therapy , 25 of 30 long - term npc survivors completed five questionnaires on qol and fs : fact - np ( functional assessment of cancer therapy nasopharyngeal cancer questionnaire ) , fact - g ( functional assessment of cancer therapygeneral ) , xeqols ( university of michigan xerostomia - related quality of life scale ) , pss - hn ( performance status scale for head and neck cancer ) , and eq - 5d - 3l ( generic multi - attribute instrument )  . 
fact - g is a 27 - item measure that is classified into four subscales , and is used to assess physical , social / family , emotional , and functional well - being . 
the npcs consists of additional items specific of patients with npc , such as eating , swallowing , mouth dryness , appetite , taste , voice quality , communication , appearance , pain , neck movement , tinnitus , hearing , vision , smell , and nasal blockage . 
the total fact - np score is the sum of factg and npcs [ 16 ]  . xeqols consists of 15 items and measures impact of salivary gland dysfunction and xerostomia on the four major domains of oral health - related qol : physical , personal / psychological , social functioning , and pain / discomfort issues . 
patients answered to questions by checking the box that describes best how true each statement was during the last 7 days ( not at all , a little , somewhat , quite a bit , very much ) , with 15 scale . 
higher scores represent greater degree of symptoms [ 17 ]  . the pss - hn is a validated clinician - rated instrument designed to evaluate performance in areas of functioning . 
each is rated from 0 to 100 , with higher scores indicating a better performance [ 11 ]  . the eq - 5d - 3l descriptive system comprises the following five areas : mobility , self - care , usual activities , pain / discomfort , and anxiety / depression . 
each dimension has three levels : no problems ( level 1 ) , some problems ( level 2 ) , and extreme problems ( level 3 ) [ 18 ]  . in this study , we analyzed if late toxicity was affected by different predictive factors ( age , gender , stage , time elapsed from the end of treatment , rt techniques , and associated chemotherapy ) and if it was significantly related to questionnaire scores about qol and fs . statistical analysis the kaplanmeier method was used to calculate the disease - specific survival ( dss ) , locoregional recurrence - free survival ( lrrfs ) , distant metastasis - free survival ( dmfs ) , progression free survival ( pfs ) , and overall survival ( os ) rates . 
 lrrfs and dmfs were measured from the date of the 1 3 radiol med ( 2017 ) 122 : 303308 end of rt to the date of the first observation of locoregional recurrence or distant metastasis , respectively . 
in 23 dead patients , 10 ( 43.5% ) had locoregional relapse , 10 ( 43.5% ) had distant metastasis , and 3 ( 13% ) had both locoregional recurrence and distant metastases . 
of the 25 patients who completed questionnaires , 19 were men and 6 women aged 49.6 ( range 1887 ) ; 8 patients were treated 14 years before compiling questionnaires and the remaining 17 received rt at least 4 years before . 
table 4 reports the frequencies of problem levels subdivided according to the eq - 5d - 3l dimensions : 72% of cases had not problems about their cancer , 16% of 1 3 306 radiol med ( 2017 ) 122 : 303308 fig . 
moreover , a trend toward improved qol in patients treated with imrt was showed by pss - hn and 0.07 and p eq - 5d - 3l scores ( p 0.06 , respectively ) ( table 5 )  . 
hearing loss seemed to be related to worse pss - hn score ( p 0.06 ) ( table 6 )  . 1 3 radiol med ( 2017 ) 122 : 303308 table 4 eq - 5d - 3l dimension of health no problems n ( % ) some problems n ( % ) severe problems n ( % ) table 5 correlation between questionnaires and prognostic factors questionnaire p value gender p value technique p value conc . 
 found that besides socio - economic levels , advances in rt technique played a significant role to improve qol of npc patients suggesting that qol may be a prognostic indicator in npc [ 20 ]  . 
in our study , we used a combination of questionnaires , fact - np , fact - g , xeqols , pss - hn , and eq - 5d - 3l , in patients with npc to get more information about qol and fs by disease - specific instruments . 
some studies suggested that imrt is associated with statistically significant improvement in several important qol domain , including swallowing , dry mouth , and social eating [ 19 , 21 , 22 ]  . 
our study showed a trend between imrt and better qol according to pss - hn and eq - 5d - 3l questionnaires , without to reach statistical significance , probably due to the small number of patients analyzed . 
they found that imrt improved qol , but xerostomia - related items still had a significantly negative effect after 2 years from the end of treatment on survivors qol [ 23 ]  . 
in our study , patients with g1 - g2 xerostomia had worse factnp scores , while hearing loss was related to worse pss - hn score . although this study has several limitations , because it includes a small number of patients with heterogeneous treatments , no pre - treatment qol data are available and post - treatment evaluation to assess qol and late toxicity were obtained at only one date for all patients , a very few data are reported on literature about qol of npc long - term survivors . conclusions our preliminary data on pros measures suggest that negative predictors of qol in npc patients are age , techniques , xerostomia , and hearing loss . 
prospectively studies with a larger sample are needed to confirm our findings . 1 3 308 compliance with ethical standards ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . conflict of interest the authors declare that they have no conflict of interest . 
over the past year , we selected 12 patients ( seven men and five women ; mean age 65.8 years , range 4582 ) for the occlusion of five internal iliac arteries ( in three aortoiliac aneurysms , one internal iliac aneurysm and one isolated common iliac artery aneurysm ) , two common iliac arteries ( in two ruptured abdominal aortic aneurysms ) , two subclavian arteries ( in aortic arch aneurysms ) and three splenic artery aneurysms . 
la versatilit del dispositivo ne amplier sicuramente le indicazioni con risultati avvalorati da pubblicazioni ulteriori e studi numericamente pi ampi e con follow - up pi protratto . keywords interventional radiology vascular plug embolization parole chiave radiologia interventistica vascular plug embolizzazione 708 introduction the amplatzer vascular plug ( avp ) consists of a self - expandable nitinol cylinder secured to a stainless - steel delivery cable by a microscrew . 
the device grew out of two precursors designed exclusively for cardiological purposes , the amplatzer septal occluder and the amplatzer duct occluder , used for the occlusion of interatrial defects and patent ductus arteriosus , respectively [ 1 , 2 ]  . 
the systems plug - like shape and availability in several sizes have progressively expanded its applications in interventional radiology , where it offers an alternative to permanent embolising material such as metallic coils or acrylic glue , in the occlusion of smallto mediumsize feeding and draining vessels in the treatment of aneurysms or arteriovenous malformations ( avm ) [ 314 ]  . the aim of this study was to review our experience to confirm the reported indications for the avp , identify possible further indications in interventional radiology and evaluate the immediate and long - term technical success of the avp . materials and methods over the past year , we selected 12 patients ( seven men and five women ; mean age 65.8 years ; age range 4582 ) for the occlusion of five internal iliac arteries close to the origin ( in three aortoiliac aneurysms , one internal iliac aneurysm and one isolated common iliac aneurysm ) , two common iliac arteries ( in ruptured abdominal aortic aneurysms treated on an emergency basis ) , two subclavian arteries ( in aortic arch aneurysms ) and three aneurysms of the mid splenic artery ( two avps were used , one proximal and one distal to the aneurysm )  . 
we used 15 avps ( aga medical corporation , golden valley , mn , usa ) with a diameter 30%50% larger than that of the target vessel : 14 mm or 16 mm in diameter delivered through an 8 - fr guiding catheter ( envoy , cordis , miami , fl , usa ) for the iliac arteries ; 10 mm or 12 mm in diameter delivered through 6to 7fr guiding catheters ( envoy ) for splenic , subclavian and internal iliac arteries , respectively . 
a guiding catheter is preferred to a long introducer sheath because the avp device and its loader cannot cross the haemostasis valve of the sheath . oversizing of the avp by 30%50% with respect to the target vessel is justified by the elasticity of nitinol , which allows the cylinder to expand to fit the diameter of the vessel . after expanding , the device becomes elongated and assumes radiol med ( 2008 ) 113 : 707718 introduzione il sistema vpa un device costituito da un cilindro autoespandibile in nitinol fissato mediante una microvite ad un cavo di introduzione in acciaio inossidabile ; il cavo , con un movimento antiorario , viene svitato dal cilindro consentendone un rilascio controllato . 
il dispositivo nato da due precursori per utilizzo esclusivo in ambito cardiologico , lamplater septal occluder e lamplatzer duct occluder , per locclusione rispettivamente dei difetti interatriali e dei dotti arteriosi pervi [ 1 , 2 ]  . 
le caratteristiche morfologiche a tappo e la disponibilit in pi diametri ne hanno progressivamente ampliato le indicazioni specie in radiologia interventistica , in alternativa allutilizzo di materiale embolizzante di tipo definitivo , quali spirali metalliche o la colla acrilica , nellocclusione di afferenze o efferenze di arterie e vene di piccolo e medio calibro per il trattamento della patologia aneurismatica o delle malformazioni arterovenose ( mav ) [ 314 ]  . 
 scopo del nostro lavoro presentare la nostra esperienza nel confermare le indicazioni allutilizzo del vpa apparse in letteratura e nellindividuare possibili ulteriori indicazioni in radiologia interventistica e valutarne il successo tecnico immediato e a distanza . 
 materiali e metodi nellultimo anno abbiamo selezionato 12 pazienti ( 7 maschi e 5 femmine , et media 65 , 8 anni , range 4582 ) per locclusione mediante 1 vpa di : 5 arterie ipogastriche allorigine ( in 3 aneurismi aorto - iliaci , 1 aneurisma dellarteria ipogastrica e 1 aneurisma isolato dellarteria iliaca comune ) , 2 arterie iliache comuni ( in aneurismi dellaorta addominale rotti trattati in urgenza ) , 2 arterie succlavie ( in aneurismi dellarco aortico ) e di 3 aneurismi dellarteria splenica del tratto intermedio , mediante 2 vpa a monte e a valle dellaneurisma . 
sono stati utilizzati complessivamente 15 vpa ( vascular plug amplatzer , aga medical corporation , golden valley , mn , usa ) del diametro del 30%50% superiore rispetto al calibro del vaso da occludere : da 14 o 16 mm di diametro attraverso cateteri guida da 8 f ( envoy , cordis , miami , fl , usa ) per le arterie iliache ; del diametro da 10 o 12 mm mediante cateteri guida da 67 f ( envoy , cordis , miami , fl , usa ) rispettivamente per larteria splenica , succlavia e ipogastrica . 
il catetere guida da preferirsi allintroduttore lungo in quanto il dispositivo vpa con il suo caricatore non supera la valvola emostatica di questultimo . la sovradimensione del calibro del vap dal 30% al 50% superiore al calibro del vaso da occludere giustificata radiol med ( 2008 ) 113 : 707718 fig . 
1a - g splenic artery aneurysa - c preprocedural computed tomography ( ct ) angiography ( a volume - rendered reconstruction ; b axial image ) and c angiography : a large saccular aneurysm of the middle third of the splenic artery . 
d endovascular ligation with two amplatzer vascular plugs ( avps ) ( asterisk ) in the feeding and draining vessels ; a contrast - agent collection is well evident inside the sac . 
d legatura endovascolare mediante vpa ( asterisco ) a monte e a valle , nei rami afferente ed efferente ; si osserva ristagno di mezzo di contrasto nella sacca aneurismatica esclusa . 
f , g angiotc espletata 1 mese dopo la procedura ( scansioni assiali contigue ) : ben riconoscibile il vpa ( asterisco ) senza artefatti da indurimento del fascio che consente la valutazione della completa esclusione dellaneurisma ( freccia nera ) ; ampio infarto splenico ( testa di freccia )  . 710 radiol med ( 2008 ) 113 : 707718 fig . 
2a - c aortoiliac aneurysa preprocedural computed tomography ( ct ) angiography ( volume - rendered reconstruction ) : aortoiliac aneurysm involving the origin of both internal iliac arteries and small aneurysm of the left internal iliac artery . 
b angiography performed after deployment of a customised bifurcated stent - graft with a branch preserving the patency of the right internal iliac artery ( black arrow ) ; aneurysm of the left internal iliac artery is excluded with endovascular ligation with amplatzer vascular plug ( avp ) in the feeding artery ( black asterisk ) and coils in the draining tract ( white arrow )  . 
b angiografia espletata dopo posizionamento di endoprotesi biforcata custom - made con braccietto protesico che preserva la perviet dellarteria ipogastrica destra ( freccia nera ) ; laneurisma dellarteria ipogastrica sinistra stato escluso mediante legatura endovascolare con vpa a monte ( asterisco nero ) e spirali metalliche a valle ( freccia bianca )  . 
in vessels with a diameter less than 50% that of the cylinder , the device can reach more than 1 cm in length . in 10 / 12 cases , we used percutaneous transfemoral access , whereas in 2 / 12 cases , requiring occlusion of the subclavian artery , percutaneous access was transhumeral . 
in two cases of aortoiliac aneurysm , the internal iliac artery was catheterised with the crossover technique , whereas in the remaining cases , the ostium of the internal iliac artery was catheterised through an ipsilateral access owing to more favourable anatomy . 
once the guiding catheter was close to dalla elasticit del nitinol che permette lespansione sino al raggiungimento del calibro vaso ; successivamente il dispositivo si allunga conferendo la caratteristica morfologia a tappo . 
il vap lungo 7 o 8 mm e lallungamento inversamente proporzionale al calibro del vaso ; con vasi di calibro inferiore al 50% si pu allungare pi di 1 c in 10 / 12 casi lapproccio percutaneo stato effettuato per via trans - femorale ; in 2 / 12 casi , per locclusione dellarteria succlavia , stato utilizzato lapproccio transomerale . 
3a - f isolated common iliac artery aneurysa preprocedural angiography : isolated common iliac artery aneurysm involving the origin of internal iliac artery ; complete exclusion requires occlusion of the orifice of the internal iliac artery . 
where deployment is precluded by the small diameter of the outflow vessel or vascular tortuosity hampering advancement of the guiding catheter , the outflow vessel can be catheterised with a microcatheter and occluded with metallic coils . 
no major complication such as rupture , perforation or dissection was observed . during the follow - up period ( mean 4.6 months , range 36 ) ct angiography and / or contrast - enhanced us demonstrated occlusion of the artery and aneurys no cases of device migration occurred . 
the avp grew out of two cardiac devices used for the closure of interatrial defects or patent ductus arteriosus ( the amplatzer septal occluder and the amplatzer duct occluder , respectively ) [ 1 , 2 ]  . 
the avp in now indicated for the occlusion of mediumto small - size arteries or veins in interventional radiology [ 314 ]  . the main advantage of the avp , compared with other questo punto non pi possibile muovere il dispositivo . 
disponibile in calibri da 4 a 16 mm , con incremento di 2 mm , lungo 7 o 8 m nato da radiol med ( 2008 ) 113 : 707718 embolising devices such as metallic coils lies in the opportunity to occlude the feeding and / or draining vessels of aneurysms or avms with a single device and thus with faster immediate results . 
use of the avp therefore offers an alternative to occlusion with metallic coil embolisation , which requires the placement of several coils of different sizes to occlude a single vessel with 4or 5 - fr catheters or the more expensive microcatheters . moreover , the inability to control coil release with the metallic coils creates a risk of malpositioning or displacement . 
these are mostly case reports regarding extracardiac applications of the amplatzer systems for treating pulmonary avm [ 4 , 7 , 9 , 13 ] , subclavian [ 8 ] , internal iliac [ 6 , 14 ] , pulmonary [ 12 ] and cerebral aneurysms [ 5 ] , for the occlusion of a retroperitoneal shunt in a patient with portal hypertension during transjugular intrahepatic portosystemic shunt ( tips ) creation [ 3 ] and for the occlusion of the internal iliac artery in patients with aortoiliac or iliac aneurysm [ 11 ]  . 
one of the earliest reports described the use of the avp to occlude the origin of the internal iliac artery in the endovascular treatment of aortoiliac and iliac aneurysms to prevent type ii endoleaks [ 11 ]  . 
in particular , pulmonary avm with large feeding arteries , and thus at a greater risk of device migration , were successfully treated with the avp , which showed excellent anchoring to the vessel and immediate occlusion [ 4 , 7 , 9 , 13 ]  . 
the only alternative treatment for pulmonary avm is the use of metallic coils [ 15 , 16 ] , as indications for occlusion with a detachable latex balloon have become obsolete . 
among later studies , a sporadic report of a ruptured isolated aneurysm of the internal iliac artery [ 14 ] described embolisation of the outflow branches and the origin of the internal iliac artery with coils and an avp using the endue precursori per utilizzo esclusivo in ambito cardiologico per la chiusura dei difetti interatriali o dei dotti arteriosi pervii ( amplater septal occluder e lamplatzer duct occluder rispettivamente ) [ 1 , 2 ]  . 
il vpa trova oggi indicazione in radiologia interventistica nellocclusione di arterie o vene di medio e piccolo calibro [ 314 ]  . il vantaggio principale , rispetto ad altri devices embolizzanti come le spirali metalliche , la possibilit di utilizzare un unico dispositivo per locclusione di vasi afferenti e / o efferenti a patologia aneurismatica o malformazioni arterovenose ( mav ) , quindi con un pi veloce risultato immediato ; inoltre le caratteristiche del sistema di rilascio permettono un pi preciso e controllato posizionamento [ 5 , 7 , 9 , 13 ]  . lelasticit del nitinol consente un saldo ancoraggio al vaso per forza radiale evitando le migrazioni con un allungamento prevedibile ; quindi possibile una scelta del calibro del dispositivo sicuramente meno precisa rispetto alla scelta del calibro , della lunghezza e del tipo di spirale . 
si pone quindi , attualmente , quale alternativa allocclusione mediante embolizzazione con spirali metalliche ; questultima prevede il posizionamento di pi spirali di calibro diverso per occlusioni di un unico vaso con cateteri da 4 o 5 f o lutilizzo pi costoso di microcateteri ; inoltre limpossibilit di controllarne il rilascio comporta il rischio di malposizionamento o dislocazione delle stesse . 
durante lultimo anno sono apparsi in letteratura i primi lavori ( tabella 1 ) , la maggior parte case report , riguardanti lutilizzo extracardiologico dei sistemi ampltazer ( tabella 1 ) per il trattamento di mav polmonari [ 4 , 7 , 9 , 13 ] , aneurismi dellarteria succlavia [ 8 ] , ipogastrica [ 6 , 14 ] , polmonare [ 12 ] , cerebrali [ 5 ] , per locclusione di shunt retroperitoneale in paziente con ipertensione portale durante tips [ 3 ] e per locclusione dellarteria ipogastrica in pazienti con aneurisma aorto - iliaco o iliaco [ 11 ]  . 
this technique has been successfully applied to the treatment of visceral aneurysms [ 17 ] and , given that the 10 - mm avp can be used with 6 - fr guiding catheters , we recognised the possibility of excluding aneurysms of the mid splenic artery . 
as an alternative , when vessel tortuosity and the diameter of the outflow vessels preclude advancement of the device , the distal outflow vessels can be embolised with metallic coils and the proximal feeding vessel with the avp , as done by us in the case of the internal iliac aneurysm . in the treatment of peripheral aneurysms , where maintenance of vascular continuity is not a priority , possible options include endovascular ligation or a hybrid approach . the hybrid approach has been reported in the treatment of embolizzante ; in questi casi si osservato lottimo ancoraggio del vpa con immediato effetto occlusivo [ 4 , 7 , 9 , 13 ]  . 
in questi casi lalternativa lutilizzo di spirali metalliche [ 15 , 16 ] ; lindicazione allocclusione mediante palloncino staccabile in lattice ormai per le mav polmonari obsoleta . tra i lavori pubblicati successivamente , un caso sporadico di aneurisma isolato dellarteria ipogastrica in rottura [ 14 ] descrive lembolizzazione mediante spirali metalliche dei rami efferenti di suddivisione e dellorigine dellarteria ipogastrica mediante vpa con la tecnica della legatura endovascolare . 
questultima tecnica stata adottata con successo nel trattamento degli aneurismi viscerali [ 17 ] e poich il vpa del calibro da 10 mm scorre su cateteri guida da 6 f abbiamo individuato la possibilit di escludere gli radiol med ( 2008 ) 113 : 707718 an aneurysm of an aberrant right subclavian artery . 
the origin of the subclavian artery was occluded with an avp , followed by ligation of the subclavian artery above the origin of the vertebral artery and carotid - subclavian bypass , resulting in less invasiveness and intraoperative mortality [ 8 ]  . in agreement with ha et al . 
 [ 11 ] , we successfully explored the possibility of treating isolated iliac aneurysms by positioning an avp to exclude the internal iliac ostium , when involved , and prevent a type ii endoleak before endograft placement , as an alternative to occlusion with metallic coils . 
rapid placement and availability of several sizes , all of which can be used with 6or 7 - fr guiding catheters and transhumeral approach , makes the avp a valuable alternative to coil embolisation . 
the alternative is a stentgraft occluder available only for some uni - iliac stent - grafts ( zenit , cook and talent , medtronic ) or coil embolisation [ 19 ]  . 
the advantage of the avp over these other occluding devices is its more precise positioning close to the iliac bifurcation , in that a single avp device can accommodate a range of diameters , permitting better preservation of patency of the external and internal iliac arteries . 
additionally , the avp is advanced through smaller arterial introducers . the only case of avp failure was reported in a ruptured aneurysm of the internal iliac artery in which avp recanalisation occurred at 4 weeks after treatment [ 6 ]  . aneurismi dellarteria splenica del tratto intermedio . 
in alternativa , qualora la tortuosit del vaso e il calibro dei rami efferenti allaneurisma non consentano lavanzamento del device possibile embolizzare le efferenze distali mediante spirali metalliche e lafferenza prossimale mediante il vpa come effettuato nella nostra esperienza nel trattamento di un aneurisma dellarteria ipogastrica . 
 nel trattamento degli aneurismi periferici qualora non sia necessario garantire una continuit vascolare possibile una legatura endovascolare o un approccio ibrido come apparso in letteratura di trattamento di un aneurisma dellarteria lusoria con occlusione dellorigine della succlavia mediante vpa e successiva legatura dellarteria succlavia a monte dellorigine dellarteria vertebrale e successivo bypass carotido - succlavio di minore invasivit e mortalit perioperatoria [ 8 ]  . 
 [ 11 ] abbiamo valutato con successo la possibilit di trattare gli aneurismi isolati dellasse iliaco con esclusione dellorigine dellarteria ipogastrica mediante vpa qualora coinvolta , prima del posizionamento dello stent - graft , al fine di escludere il rifornimento retrogrado , in alternativa allocclusione mediante spirali metalliche . 
b , c angiografia espletata per via anterograda ( b ) e retrograda ( c ) dopo posizionamento di endoprotesi aorto - uniliaca e avp in corrispondenza dellarteria iliaca comune destra : completa esclusione dellaneurisma e regolare perviet delle arterie ipogastrica e iliaca esterna destra . ca esterna e ipogastrica ed evitando la legatura chirurgica con una pi rapida esclusione degli aneurismi rotti . 
questo tipo di approccio comunque fattibile anche nel trattamento in elezione ; lalternativa lo stent - graft occlusore disponibile solo per alcune endoprotesi uniliache ( zenit , cook e talent , medtronic ) o lembolizzazione con spirali [ 19 ] ; il vantaggio rispetto a questi dispositivi occlusori un pi preciso posizionamento a ridosso della biforcazione iliaca , in quanto un unico vpa abbraccia pi calibri , con una conseguente pi sicura preservazione della perviet delle arterie iliaca esterna e ipogastrica ; inoltre il vpa avanzato attraverso introduttori arteriosi di minor calibro . 
 lunico caso di insuccesso del vpa stato riportato nel trattamento di un aneurisma rotto dellarteria ipogastrica nel quale si verificata una ricanalizzazione del vpa a 4 settimane dal trattamento [ 6 ]  . conclusioni in conclusione , la semplicit della scelta e dellutilizzo del fig . 
5 amplatzer vascular plug ( avp ) : a self - expandable , cylindrical device made from a nitinol wire mesh , secured on both ends with platinum marker bands . 
dispositivo cilindrico autoespandibile realizzato in maglia metallica di nitinol fissato alle due estremit con fasce di marker in platino ; a quella prossimale saldata una microvite in acciaio che consente il fissaggio al cavo di introduzione . 
il dispositivo , una volta rilasciato nel vaso assume una caratteristica morfologia a tappo . radiol med ( 2008 ) 113 : 707718 conclusions in conclusion , easy selection and use of the device combined with precise and controlled release and immediate technical success justifies the widespread use of the avp in interventional radiology . 
the avp can and in some cases has already replaced metallic coils for endovascular repair of aortic aneurysms , for the prevention of type ii endoleaks from the internal iliac and subclavian arteries , and in endovascular ligation of visceral aneurysms where the device can be placed distal and proximal to the aneurysms . 
the avp may also replace the occluder device of the aortic stent - graft in the aorto - uni - iliac kit , especially in emergencies due to ruptured aneurysthe versatility of the device and further use by operators addressing a variety of therapeutic problems will extend the indications , no doubt also in extravascular contexts [ 20 ]  . dispositivo , nonch il preciso e controllato rilascio , con immediato successo tecnico , ne giustificano , secondo la nostra esperienza , la divulgazione in radiologia interventistica . 
il vpa pu e in alcuni casi ha di gi sostituito lutilizzo delle spirali metalliche nel trattamento endovascolare degli aneurismi dellaorta , per la prevenzione degli endoleak di tipo ii da arteria ipogastrica e da arteria succlavia , e nel trattamento mediante legatura endovascolare degli aneurismi viscerali qualora sia possibile il posizionamento a monte e a valle . 
la versatilit del dispositivo e lutilizzo ulteriore da parte pi operatori che affrontano problematiche terapeutiche diverse ne amplieranno le indicazioni , sicuramente anche in ambito extravascolare [ 20 ]  . 
karantanas1 1department of radiology , university hospital of heraklion , stavrakia , heraklion 711 10 , crete , greece 2messinia diagnostic center , kalamata , greece 3ika hospital , athens , greece correspondence to : a.h. 
karantanas , associate professor of radiology , department of radiology , university hospital , stavrakia , heraklion 711 10 , greece , tel : + 30 - 281 - 0392541 , fax : + 30 - 281 - 0542095 , e - mail : apolsen@yahoo.com received : 12 june 2007 / accepted : 18 september 2007 / published online : 17 july 2008 springer - verlag 2008 abstract purpose . 
transient osteoporosis of the hip ( toh ) , associated with pregnancy , is a self - limiting skeletal disorder affecting women , usually in the third trimester , which resolves spontaneously within few months postpartubilateral involvement is rare . 
toh associated with pregnancy does not necessarily occur in the third trimester of pregnancy and may be bilateral . keywords bone marrow edema hip transient osteoporosis pregnancy / postpartum mr diagnosis riassunto obiettivo . 
losteoporosi transitoria dellanca associata con la gravidanza rappresenta un disordine autolimitante scheletrico che colpisce le donne tipicamente al terzo trimestre di gravidanza e si risolve spontaneamente nellarco di alcuni mesi dal parto . 
losteoporosi transitoria dellanca associata con la gravidanza non necessariamente si sviluppa nel terzo trimestre di gravidanza e pu essere bilaterale . parole chiave edema midollare anca osteoporosi transitoria gravidanza post - partum diagnosi rm 690 introduction transient osteoporosis of the hip ( toh ) in pregnancy is an idiopathic , self - limiting disorder clinically characterised by sudden onset of hip pain without any history of systemic disorders or traumatic injuries [ 1 , 2 ]  . 
no case with postpartum presentation has been reported to our knowledge . we report on three cases of toh , demonstrated with synchronous bilateral involvement , soon after delivery . materials and methods all magnetic resonance ( mr ) imaging examinations were performed on 1.5 - tesla magnets ( siemens , sonata , maestro class , erlangen , germany ; and philips intera , best , the netherlands )  . 
the mr imaging protocol included coronal t1 - weighted turbo spin echo ( tse ) , coronal short tau inversion recovery ( stir ) - tse , transverse fat - suppressed t2 - weighted tse and oblique axial fat - suppressed contrast - enhanced t1 - weighted se separately for each hip with a 16 - cm field of view . case 1 case 2 a 31 - year - old woman presented with abrupt onset of bilateral hip pain just after delivery . 
non stato riportato , secondo la nostra conoscenza , alcun caso con presentazione post - parturiportiamo tre casi di osteoporosi transitoria dellanca dimostrata con coinvolgimento sincrono bilaterale direttamente dopo il parto . materiali e metodi tutti gli esami rm sono stati eseguiti tramite apparecchiatura 1 , 5 t ( siemens , sonata , maestro class , erlangen , germania e philips intera , best , olanda )  . 
il protocollo rm ha incluso acquisizioni t1 dipendenti tse , sequenze coronali stir - tse , assiali t2 dipendenti tse con soppressione del grasso , e assiali oblique con soppressione del grasso t1 pesate dopo somministrazione di chelati del gadolinio ev , solamente dal lato anormale , con campo di vista di 16 c caso 1 caso 2 una donna di 31 anni si presentata con improvviso dolore bilaterale allanca direttamente dopo il parto . 
la paziente stata trattata in maniera conservativa con scarico dellarticolazione dopo la gravidanza e 11 mesi dopo il parto il dolore si risolto . una donna di 36 anni si presentata con dolore allanca destra insorto direttamente dopo il parto di primogenito seguito due settimane dopo da dolore anche allanca controlaterale . 
data lassenza di pregressi traumi o malattie locali stata sospettata osteoporosi transitoria dellanca e quindi confermata quando la paziente stata esaminata con rm radiol med ( 2008 ) 113 : 689694 fig . 
a the coronal t1 - weighted magnetic resonance ( mr ) image at onset of symptoms shows low signal intensity in the bone marrow of both femoral heads ( arrows )  . 
this disorder , however , more commonly affects men between the fourth and the sixth decade of life and , as a rule , has a predilection for unilateral involvement [ 1 , 4 , 5 ]  . 
in most cases , there is hip pain of sudden onset without a history of trauma , with both physical and laboratory findings being normal , minimal or nonspecific . the pain characteristically resolves over weeks to months under conservative treatment , such as restricted weightbearing , antiresorptive medications and analgesics [ 1 , 46 ]  . the diagnosis of toh is established by correlating clinical and imaging findings . 
a diffuse pattern of bone marrow oedema , appearing on mr images as ill - defined , hypointense areas on t1 - weighted images and hyperintense on stir or fat - suppressed t2 - weighted images , limited to the donna di 26 anni si presentata un mese dopo il parto con dolore allanca bilaterale ad insorgenza improvvisa . 
sulla base dellassenza di storia pregressa di patologie locali e assenza di fattori di rischio , stata stabilita diagnosi di osteoporosi transitoria della testa femorale ed stato praticato trattamento conservativo . 
questo disordine colpisce pi frequentemente gli uomini tra la quarta e la sesta decade di vita e di regola ha un coinvolgimento unilaterale [ 1 , 4 , 5 ]  . 
a the coronal t1weighted turbo spin echo ( tse ) magnetic resonance ( mr ) image shows low signal intensity in the marrow of both femoral heads extending to the neck ( arrows )  . 
a limmagine coronale t1 dipendente e tse dimostra una bassa intensit di segnale al midollo di entrambe le teste femorali che si estende fino al collo ( frecce )  . 
d sette mesi dopo la scansione stir sul piano coronale dimostra la pressoch completa risoluzione delledema midollare che corrisponde ad un miglioramento clinico ; vie solamente unarea confinata di elevata intensit di segnale alla testa femorale di sinistra ( freccia )  . 
il dolore caratteristicamente si risolve in un periodo compreso tra settimane e mesi , il trattamento conservativo e comprende scarico dellarticolazione , analgesici e farmaci antiriassorbimento [ 1 , 46 ]  . 
un quadro di diffuso edema midollare presente allindagine rm che appare come area a margini mal definiti ipointensa nelle sequenze t1 dipendenti , e iperintense sulle sequenze stir o t2 dipendenti con soppressione del grasso , limitata alla testa femorale o estesa al collo e alla regione intertrocanterica , accompagnata da un grado variabile di soffusione dellarticolazione sono i segni distintivi di osteoporosi transitoria dellanca [ 1 , 58 ]  . 
il quadro di edema midollare non specifico dato che si correla a un ampio ventaglio di cause come losteoporosi transitoria , la sindrome delledema midollare transitorio , la frattura da stress dellepifisi , losteomiefig . 
la scansione stir sul piano coronale dimostra ledema midollare in entrambe le teste femorali ( frecce )  . radiol med ( 2008 ) 113 : 689694 femoral head or extending to the neck and intertrochanteric region , accompanied by a variable degree of joint effusion , are the findings suggestive of toh [ 1 , 58 ]  . 
the pattern of bone marrow oedema is nonspecific , as it implies a wide range of entities such as transient osteoporosis or transient bone marrow edema syndrome , epiphyseal stress fracture , osteomyelitis , neoplasm , osteonecrosis and degenerative arthritis [ 2 , 5 , 7 , 9 , 11 ]  . in the case of toh in pregnancy , a predilection for the left hip has been observed , whereas in toh affecting men , no side predilection has been reported so far in the literature [ 9 ]  . 
migratory osteoporosis with bone marrow oedema shifting from one hip to the other or from the hip to another joint occurs months or years after the original involvement [ 1 ]  . 
 the pathogenetic mechanism of toh has long been debated , with some authors suggesting an impairment of venous return and local hyperaemia [ 1214 ] , and others believing that toh is a nontraumatic form of algodystrophy caused by vasomotor disturbances of the sympathetic nervous system [ 15 , 16 ]  . 
however , the most possible pathogenetic pathway of toh has been suggested by frost and other authors [ 1820 ] , who proposed that under noxious stimuli in the regional biological processes ( blood flow , cell metabolism and turnover , and also bone tissue modelling and remodelling ) are probably accelerated . 
such prolonged or excessive phenomena activate an inflammatory response and a large number of bone turnover foci , which are responsible for the bone marrow oedema and the focal osteoporosis seen in toh . 
on plain radiographs ( up to 87% sensitivity , taken at least 5 weeks after the onset of symptoms ) , the osteoporotic area is depicted as a focal , more radiolucent , region with an intact cortex and joint preservation . 
currently , mr imaging constitutes the modality of choice for the early dilite , le neoplasie , losteonecrosi , lartrite degenerativa [ 2 , 5 , 7 , 9 , 11 ]  . 
 in corso di osteoporosi transitoria dellanca in gravidanza stata osservata una predilezione per lanca di sinistra mentre nella osteoporosi dellanca che colpisce i soggetti di sesso maschile secondo i dati forniti dalla letteratura non vi predilezione di sede [ 9 ]  . 
losteoporosi migrante con edema midollare che si sposta dallanca affetta a quella controlaterale oppure da unanca ad una articolazione differente pu insorgere mesi o anni dopo il coinvolgimento originario [ 1 ]  . 
alcuni autori hanno suggerito un indebolimento del ritorno venoso associato ad uniperemia focale [ 1214 ] , altri hanno riferito losteonecrosi come una forma non traumatica di algodistrofia causata da disturbi vasomotori del sistema nervoso simpatico [ 15 , 16 ]  . 
comunque il percorso patogenetico pi verosimile dellosteoporosi transitoria stato suggerito frost e altri autori [ 1820 ] che hanno proposto che dopo lintervento di noxa patogene il processo biologico focale ( flusso ematico , metabolismo cellulare , turnover cellulare e rimodellamento tissutale osseo ) viene probabilmente accelerato . 
i radiogrammi standard ( sensibilit fino all87% ) ottenuti almeno 5 settimane dopo lesordio della sintomatologia permettono di dimostrare un area di osteoporosi come una regione radiotrasparente con corticale ossea intatta e preservazione della superficie articolare . 
 ad oggi , la rm costituisce modalit di scelta per la diagnosi precoce della osteoporosi transitoria per il fatto che 694 radiol med ( 2008 ) 113 : 689694 agnosis of toh , as it depicts findings within 48 h from the onset of symptoms [ 11 ]  . dimostra i reperti significativi entro 48 ore dallesordio della sintomatologia [ 11 ]  . the three cases presented here underline the possibility that bilateral synchronous toh may occur in women in the immediate postpartum period . 
rampoldi interventional radiology , niguarda hospital , piazza ospedale maggiore 3 , 20162 milan , italy correspondence to : r corso , tel . : + 39 - 02 - 64442793 , fax + 39 - 02 - 64443090 , e - mail : roccocorso@jumpy.it received : 16 may 2007 / accepted : 4 july 2007 / published online : 17 july 2008 springer - verlag 2008 abstract purpose . 
this study was performed to evaluate the safety and efficacy of transjugular intrahepatic portosystemic shunt ( tips ) in the treatment of patients affected by buddchiari syndrome ( bcs )  . 
from january 1999 to december 2006 , 15 patients ( seven male and eight female subjects , age range 752 years ) with bcs uncontrolled by medical therapy were treated with tips placement . 
acute leukaemia was the cause of the single early death and was unrelated to the procedure . the patient with portal vein thrombosis underwent thrombolysis before tips , but the vein occluded again after 3 weeks , and the patient died 6 months later . 
dal gennaio 1999 al dicembre 2006 , 15 pazienti ( 7 maschi e 8 femmine , di et compresa tra 752 anni ) affetti da sbc non controllata dalla terapia medica sono stati sottoposti a tips . 
in otto pazienti ( 53 , 4% ) stato posizionato uno stent non ricoperto mentre in sette pazienti ( 46 , 6% ) stato utilizzato uno stent - grail follow - up stato di 3 , 268 mesi ( mediana 29 , 4 mesi ) risultati . 
il paziente con trombosi portale stato sottoposto prima della tips a fibrinolisi , ma si osservata riocclusione della tips a distanza di tre settimane con decesso del paziente dopo 6 mesi . 
nessuno dei pazienti ha richiesto o stato inserito in lista per un trapianto di fegato . 728 radiol med ( 2008 ) 113 : 727738 traditional surgical portosystemic shunting or liver transplantation . keywords budd - chiari syndrome transjugular intrahepatic portosystemic shunt ( tips ) liver transplantation surgical portosystemic shunt conclusioni . 
la tips nella sbc un trattamento efficace e sicuro e dovrebbe essere considerata una valida alternativa al tradizionale shunt porto - sistemico chirurgico o al trapianto di fegato . parole chiave sindrome di budd - chiari tips trapianto di fegato shunt portosistemico chirurgico introduction introduzione budd - chiari syndrome ( bcs ) is a rare condition resulting from obstruction of the hepatic venous outflow due to thrombotic or nonthrombotic occlusion , either complete or incomplete , of the hepatic veins and / or suprahepatic inferior vena cava [ 1 ]  . 
the rapid rise in intrahepatic pressure and the resulting liver congestion lead to hepatocellular necrosis ( especially of hepatocytes located in the more peripheral parts of the circulatory region ) due both to anoxia and to mechanical compression . 
as a consequence , the clinical picture may vary from acute or hyperacute fulminant liver failure to subacute or chronic forms with progressive congestive fibrosis and cirrhosis and the development of portal hypertension with its possible complications such as variceal bleeding , intractable ascites , hepatorenal syndrome and spontaneous bacterial peritonitis [ 2 ]  . 
blood and myeloproliferative disorders causing hypercoagulability ( polycythemia vera , paroxysmal nocturnal hemoglobinuria , essential thrombocythemia , factor - v leiden mutation , myelofibrosis , presence of anticardiolipin antibodies , etc . ) and congenital membranous webs within the vena cava or hepatic veins are among the most significant known causes . other less frequent causes include oral contraceptive use , trauma , infections ( amoebic abscesses , aspergillosis , hydatid cysts ) , certain kinds of tumour ( hepatocellular carcinoma , renal or adrenal carcinoma , vessel leiomyosarcoma ) , pregnancy and postpartum [ 4 ]  . 
the prognosis , especially in untreated acute forms or those with complete thrombosis of the hepatic veins , is often poor , with reported 2 - year survival rates between 10% and 40% [ 5 , 6 ]  . 
medical managela sindrome di budd - chiari ( sbc ) una rara condizione di ostacolato deflusso venoso epatico per occlusione trombotica o non trombotica , completa o incompleta , delle vene sovraepatiche e / o del tratto sovraepatico della vena cava inferiore [ 1 ]  . 
il rapido aumento della pressione intraepatica e di conseguenza la congestione del fegato causa di necrosi degli epatociti ( soprattutto di quelli localizzati nelle regioni pi periferiche del distretto circolatorio ) legata sia a fenomeni di tipo anossico che a compressione meccanica . 
 il quadro anatomo - patologico caratterizzato da necrosi centrolobulare che , se non efficacemente contrastata mediante terapie decompressive , evolve in modo pi o meno rapido verso una progressiva distruzione di aree sempre pi estese di parenchima epatico . 
possono pertanto determinarsi quadri clinici di insufficienza epatica variabili da forme acute o iperacute ( insufficienza epatica fulminante ) a quadri subacuti o cronici con progressiva fibrosi e cirrosi di tipo congestizio , sviluppo di ipertensione portale con le sue possibili complicanze quali sanguinamento da varici esofagee , ascite refrattaria , sindrome epatorenale e peritonite batterica spontanea [ 2 ]  . 
 lesordio clinico caratterizzato dai sintomi e segni legati allipertensione portale ed allinsufficienza epatica . dal punto di visto sintomatologico il paziente lamenta dolore ai quadranti addominali superiori , anoressia , nausea , vomito e distensione addominale . 
most cases require surgical portal decompression , and in the past , the surgical creation of shunts between the mesenteric - portal and systemic circulation ( portacaval , mesocaval , mesoatrial ) was the only treatment available for patients with bcs . 
more recently , orthotopic liver transplantation has been used to treat endstage hepatic failure in bcs , but the long waiting lists heavily limit the use of this option [ 8 ]  . 
 percutaneous interventional radiology procedures , and in particular transjugular intrahepatic portosystemic shunt ( tips ) , have been recently proposed as an alternative to surgical shunting and liver transplantation [ 9 , 10 ]  . 
the purpose of our study was to evaluate the feasibility and efficacy of tips in the treatment of patients with bcs . materials and methods between january 1999 and december 2006 , tips was performed on 15 patients ( seven male and eight female subjects ; age range 752 years ; median age 31 ) with a diagnosis of bcs . 
 procedures were performed in interventional radiology suites with two angiography units ( integris allura and integris c2000 , philips , the netherlands ) ; most procedures were done with the patient under general anaesthesia . 
la prognosi dei pazienti , in particolare nelle forme acute non trattate o con completa trombosi delle vene sovraepatiche , spesso grave : in letteratura vengono riportati dati di sopravvivenza a due anni variabili dal 10% al 40% [ 5 , 6 ]  . 
nella maggior parte dei casi risulta necessaria una decompressione invasiva del sistema portale ed in passato venivano eseguiti unicamente shunt chirurgici tra il sistema mesenterico - portale e quello sistemico ( porto - cavale , meso - cavale , meso - atriale )  . 
pi recentemente il trapianto ortotopico di fegato stato proposto ed eseguito come trattamento dellinsufficienza epatica terminale anche nei pazienti affetti da sbc : tuttavia le lunghe liste di attesa limitano fortemente questa opzione terapeutica [ 8 ]  . 
 negli ultimi anni in alternativa agli shunt chirurgici e al trapianto di fegato sono state proposte ed utilizzate procedure percutanee di radiologia interventistica : tra queste la principale rappresentata dallo shunt portosistemico intraepatico realizzato per via transgiugulare ( tips ) [ 9 , 10 ]  . scopo del nostro studio stato quello di valutare fattibilit ed efficacia della tips nel trattamento dei pazienti affetti da sbc . materiali e metodi dal gennaio 1999 a dicembre 2006 abbiamo sottoposto a tips 15 pazienti ( 7 maschi e 8 femmine ) di et compresa tra i 7 ed i 52 anni ( mediana 31 anni ) con diagnosi di sbc ed il cui esordio clinico era caratterizzato da ascite refrattaria ( 100% ) associata o meno ad ematemesi ( 40% ) ; in percentuali inferiori erano presenti idrotorace ( 20% ) o quadri di encefalopatia ( 6 , 6% )  . 
in sette pazienti ( 46 , 6% ) la causa della sbc era idiopatica , in 4 casi ( 26 , 6% ) da mielofibrosi ed in singoli casi da mutazione del fattore v di leiden , da policitemia vera , da emoglobinuria parossistica notturna e da anticorpi anticardiolipina ( tabella 1 )  . 
 tutte le procedure sono state eseguite in sale dedicate di radiologia interventistica utilizzando due apparecchi angiografici ( integris allura e integris c2000 , philips , olanda ) e nella maggior parte dei casi con pazienti in anestesia genetable 1 demographic , aetiological and clinical data of the 15 patients with budd - chiari syndrome patient no . aetiology symptoms and signs radiol med ( 2008 ) 113 : 727738 tabella 1 dati anagrafici , eziologici e clinici dei 15 pazienti con sbc pz , n sesso anni eziologia segni e sintomi myelofibrosis idiopathic myelofibrosis factor v leiden mutation idiopathic idiopathic idiopathic anticardiolipin antibodies polycythemia vera idiopathic idiopathic myelofibrosis myelofibrosis idiopathic paroxysmal nocturnal haemoglobinuria refractory ascites , encephalopathy refractory ascites refractory ascites , haematemesis refractory ascites , haematemesis refractory ascites refractory ascites , hydrothorax refractory ascites , haematemesis refractory ascites , hydrothorax refractory ascites , haematemesis refractory ascites refractory ascites , hydrothorax , encephalopathy refractory ascites , haematemesis refractory ascites , encephalopathy refractory ascites refractory ascites , haematemesis mielofibrosi idiopatica mielofibrosi mutazione fattore v leiden idiopatica idiopatica idiopatica anticorpi anticardiolipina policitemia vera idiopatica idiopatica mielofibrosi mielofibrosi idiopatica emoglobinuria parossistica notturna ascite refrattaria , encefalopatia ascite refrattaria ascite refrattaria , ematemesi ascite refrattaria , ematemesi ascite refrattaria ascite refrattaria , idrotorace ascite refrattaria , ematemesi ascite refrattaria , idrotorace ascite refrattaria , ematemesi ascite refrattaria ascite refrattaria , idrotorace , encefalopatia ascite refrattaria , ematemesi ascite refrattaria , encefalopatia ascite refrattaria ascite refrattaria , ematemesi were unable to use the hepatic veins to create the shunt , we adopted the transcaval technique with direct proximal access through the wall of the intrahepatic inferior vena cava [ 11 ]  . 
nei casi in cui per la realizzazione dello shunt non era possibile utilizzare le vene sovraepatiche stata utilizzata la tecnica transcavale mediante accesradiol med ( 2008 ) 113 : 727738 fig . 
angiography and tips revision were only performed in selected cases showing clinical recurrence or doppler us findings of significant stenosis or shunt thrombosis ( absence / reduction of signal in the tips , more than 50% decrease in portal flow velocity , inversion of portal venous flow )  . 
tips efficacy was also assessed by comparing clinical and laboratory data obtained before and 60 days after the procedure . results indications for tips placement were progressive acute or subacute liver failure associated with symptoms refractory to medical therapy in 11 patients ( 73.3% ) and chronic disease in four patients ( 26.6% ) with poor hepatic compensation . 
a hepatic vein remnant was visualised and used as an access site in 10 / 15 cases ( 66.6% ) , whereas in the remaining cases we had to directly puncture the intrahepatic inferior vena cava to create a proximal access . 
in 8 pazienti ( 53 , 3% ) abbiamo utilizzato stent metallici autoespansibili ( wallstent , boston scientific , watertown , usa e smart control , cordis , miami , usa ) ed in 7 casi ( 46 , 7% ) stent - graft ( viatorr endoprothesis , w.l. gore medical , flagstaff , usa ) , dilatati da 8 a 10 m in ogni paziente stata eseguita la misurazione della pressione portale ed atriale destra prima e dopo la creazione dello shunt definendo come ideale un gradiente pressorio portosistemico dopo tips < 12 mmhg . 
dopo la creazione della tips , in assenza di controindicazioni , stata intrapresa terapia farmacologica con anticoagulanti inizialmente con eparina per via parenterale sostituita nel giro di pochi giorni con warfarin mantenendo un inr ( international normalised ratio ) tra 2 , 53 , 5 . 
lo studio angiografico e leventuale revisione della tips stata effettuata solo in casi selezionati per ricomparsa della sintomatologia o dei segni clinici o riscontro allecodoppler di significativa stenosi o trombosi dello shunt ( assenza / riduzione di segnale nella tips , riduzione al di sotto del 50% della velocit del flusso portale , inversione del flusso nel sistema portale )  . 
significant decompression of the portal venous system was obtained in 13 cases ( 86.6% ) : the arterioportal pressure gradient decreased from a mean value of 26.45.8 mmhg before tips ( range 1931 mmhg ) to 9.76.2 mmhg ( range 714 mmhg ) after tips , with a median reduction of 63.3% ( range 54%70% ; table 2 )  . 
the patient with complete portal thrombosis underwent portal vein recanalisation before tips radiol med ( 2008 ) 113 : 727738 valutata anche sulla base delle condizioni cliniche e dei dati laboratoristici rilevati prima ed a 60 giorni dalla procedura . risultati lindicazione allesecuzione della tips stata linsufficienza epatica progressiva in forma acuta o subacuta associata a sintomatologia non controllabile con trattamento farmacologico in 11 pazienti ( 73 , 3% ) ed unevoluzione cronica della malattia in 4 pazienti ( 26 , 6% ) in precario compenso epatico . 
la creazione della tips stata possibile in tutti i casi in assenza di mortalit precoce o grave morbilit associata alla procedura . in 10 / 15 casi ( 66 , 6% ) stato possibile visualizzare ed utilizzare come sito daccesso un moncone di vena sovraepatica mentre nei restanti casi stato necessario eseguire direttamente la puntura della parete della vena cava inferiore intraepatica per creare un accesso prossimale . 
una significativa decompressione del sistema venoso portale stata ottenuta in 13 casi ( 86 , 6% ) : il gradiente pressorio atrio - portale si ridotto da una media di 26 , 45 , 8 mmhg pre - tips ( range 1931 mmhg ) a 9 , 76 , 2 mmhg post - tips ( range 714 mmhg ) con una mediana di riduzione percentuale del 63 , 3% ( range 54%70% ; tabella 2 )  . 
nel paziente con trombosi portale completa , prima della creazione della tips , la vena porta stata ricanalizzata inizialmente mediante fibrinolisi ad ultrasuoni ( alcolysis , angiosonic , morrisville , usa ) e quindi con fibrinolisi farmacologica ( infusione loco - regionale di urochinasi )  . 
a distanza di 23 giorni dalla tips si osservata riocclusione della vena porta e della tips con progressiva ricomparsa della sintomatologia clinica e dellinsufficienza epatica che ha condotto al decesso del paziente dopo 6 mesi . 
la maggior parte dei pazienti a 60 giorni dalla tips ha mostrato un progressivo miglioramento sia clinico che biochimico ( tabella 3 ) e sono vivi ad una mediana di follow - up di 29 , 4 mesi ( range 3 , 268 mesi )  . 
in sei pazienti , di cui 5 del sottogruppo con stent non radiol med ( 2008 ) 113 : 727738 table 2 portosystemic pressure gradient and percentage difference after transjugular intrahepatic portosystemic shunt ( tips ) tabella 2 gradiente pressorio porto - sistemico e variazione percentuale dopo tips patient no . 
analizzando separatamente i pazienti in cui stato posizionato uno stent non ricoperto ( 8 casi ) rispetto a quelli con stent ricoperto ( 7 casi ) abbiamo osservato una significativa differenza sia nella perviet primaria ( rispettivamente del 22 , 4% e 87 , 7% , p < 0 , 01 ) che nelle percentuali di reintervento per malfunzionamento ( rispettivamente del 62 , 5% e 14 , 2% , p < 0 , 01 )  . 
twenty - three days after tips , the portal vein and the tips reoccluded , with reappearance of the clinical symptoms and liver failure that led to the patients death 6 months later . 
at follow - up after 60 days , most patients showed clinical and biochemical improvements ( table 3 ) , and most of them were alive at discussione la terapia medica nella sbc viene riservata alle forme croniche che abbiano evidenziato alla biopsia epatica un quadro di congestione epatica con scarsa o assente necrosi epatocitaria . 
medical management is , however , poorly effective in controlling liver failure and the symptoms of portal hypertension in the medium to long term [ 12 , 13 ]  . 
as a result , patients refractory to medical therapy or those showing significant liver necrosis on liver biopsy have been offered surgical portal decompression as the only alternative treatment option , even though the results have been variable and often related to the experience of single centres , with reported 5 - year patency rates for both surgical mesenteric - systemic and portosystemic shunts ranging from 57% to 94% [ 14 , 15 ]  . 
however , it should be noted that in patients with bcs , who are often in critical general condition , surgical shunting has several disadvantages : first , it involves a highly invasive major operation , which increases surgical risk . 
second , the rate of shunt occlusions detected at follow - up and due to hypercoagulable states is not negligible ( > 30% ) , leading to increased overall morbidity and mortality [ 6 ]  . 
finally , there are technical problems related to the infrequent obstruction or compression of the inferior vena cava by a hypertrophic caudate lobe ( because venous outflow occurs through a series of short veins directly into the systemic circulation ) , which requires a mesoatrial shunt and is associated with a higher rate of thrombotic occlusions and technical failures [ 7 , 16 ]  . 
 in recent years , liver transplantation was suggested as a valuable alternative for treating bcs , particularly in small subsets of patients with acute liver failure or advanced cirrhosis or fibrosis on histology [ 17 ]  . 
a recent review by the european registry examined data of 248 bcs patients who underwent liver transplant between 1988 and 1999 in 51 eutecnica operatoria rappresentate dalla non frequente ostruzione o compressione della vena cava inferiore da parte del lobo caudato ipertrofico ( in quanto il suo deflusso venoso avviene attraverso una serie di corte vene direttamente nel circolo sistemico ) che impone il confezionamento di uno shunt meso - atriale che si accompagna ad una pi elevata percentuale di occlusioni trombotiche e di insuccessi tecnici [ 7 , 16 ]  . 
 negli anni pi recenti nella sbc il trapianto di fegato si posto come valida alternativa terapeutica in particolare nei sottogruppi minoritari di pazienti con associata insufficienza epatica acuta o che allistologia mostrano quadri di cirrosi o fibrosi avanzata [ 17 ]  . 
una recente analisi del registro europeo ha analizzato i dati di 248 pazienti affetti da sbc sottoposti a trapianto di fegato dal 1988 al 1999 , con follow - up completo , in 51 centri trapiantologi europei riportando elevati tassi di sopravvivenza attuariale del 75 , 6% , 71 , 4% e 68% rispettivamente a 1 , 5 e 10 anni [ 18 ]  . 
 negli ultimi decenni le tecniche di radiologia interventistica quali langioplastica e / o lo stenting hanno ampliato le alternative terapeutiche inizialmente in quei pochi pazienti affetti da sbc in cui si evidenziavano stenosi o membrane a livello delle vene sovraepatiche o della vena cava inferiore , riscontri peraltro molto pi comuni nei paesi asiatici rispetto a quelli occidentali [ 19 , 20 ]  . 
nella maggior parte dei casi esiste gi una trombosi pi o meno completa delle vene sovraepatiche e la realizzazione della tips si dimostrata lunica tecnica di tipo radiologico utilizzabile in particolare nelle forme acute o subacute che presentano progressivo deterioramento clinico e / o biochimico non rispondenti alla terapia medica [ 21 , 22 ]  . 
in most cases , there is already more or less complete thrombosis of the hepatic veins , and tips creation is the only possible interventional technique , particularly in acute or subacute forms presenting with progressive clinical and / or biochemical deterioration unresponsive to medical therapy [ 21 , 22 ]  . tips creation is a much less invasive decompression technique than is surgery , as it requires no laparotomy or vessel clamping and is therefore associated with lower morbidity and mortality , even in patients in critical condition [ 23 , 24 ]  . 
the limits of tips are essentially shunt malfunction caused by stenosis and / or occlusion of the intrahepatic tract due to intimal hyperplasia or thrombosis generally caused by biliary contamination . 
in addition , bcs is characterised by thrombophilia and hypercoagulability , which , if not effectively corrected by anticoagulation therapy , increase the incidence of shunt thrombosis up to 80% after 1 year , with resulting reappearance or worsening of the complications of portal hypertension [ 26 , 27 ]  . 
in recent years , new stents covered with polytetrafluoroethylene ( ptfe ) membranes have become available that dramatically reduce the rate of tips malfunction / thrombosis and consequently the need for periodic revisions , which were very frequent when only bare stents were used [ 28 ]  . 
a recent study compared tips with uncovered and covered stents in 13 patients with bcs , reporting primary patency rates of 16.7% vs 100% , respectively , at 6 months and 0% vs 85.7% at 12 months [ 29 ]  . 
in most cases , tips was very effective in controlling the clinical symptoms and significantly reducing the portosystemic pressure gradient and consequently the complications of portal hypertension ( 63.3% reduction in the portosystemic pressure gradient )  . 
 as suggested by some authors , in subjects with bcs and end - stage liver disease tips may act as a bridge to liver transplantation as it improves patients clinical condition condizioni critiche [ 23 , 24 ] ; inoltre essa pu realizzarsi anche nei casi di ostruzione cavale . 
i limiti della tips consistono essenzialmente nel malfunzionamento dello shunt per stenosi e / o occlusione del tramite intraepatico da iperplasia intimale o trombosi dovute nella maggior parte dei casi alla contaminazione dello shunt da parte di bile . 
inoltre nella sbc si aggiunge uno stato trombofilico e di ipercoagulabilit ematica che , se non corretto efficacemente da terapia con anticoagulanti , innalza ulteriormente lincidenza di trombosi dello shunt fino anche all80% ad 1 anno con conseguente ricomparsa o aggravamento delle complicanze legate allipertensione portale [ 26 , 27 ]  . 
negli ultimi anni tuttavia si sono resi disponibili sul mercato nuovi tipi di stent ricoperti con tessuto in ptfe ( poli - tetrafluoroetilene ) che hanno drammaticamente ridotto i tassi di malfunzionamento / trombosi della tips e di conseguenza la necessit delle periodiche revisioni che in passato erano alquanto frequenti quando venivano impiegati in modo quasi esclusivo stent non ricoperti [ 28 ]  . 
recentemente alcuni autori hanno trattato con tips 13 pazienti affetti da sbc riportando tassi di perviet primaria nel gruppo con stent non ricoperto o ricoperto in ptfe rispettivamente del 16 , 7% e 100% a 6 mesi e dello 0% e 85 , 7% a 12 mesi [ 29 ]  . 
anche nel nostro studio il sottogruppo di pazienti in cui sono stati posizionati stent ricoperti ha mostrato tassi di perviet primaria significativamente superiori rispetto al sottogruppo con stent non ricoperto ( rispettivamente 87 , 7% e 22 , 4% ) e bassissime percentuali di revisione dello shunt ( 14 , 2% )  . 
nella maggior parte dei casi la tips risultata molto efficace nel controllare la sintomatologia clinica e nel ridurre in modo significativo il gradiente pressorio porto - sistemico con conseguente abbattimento delle complicanze associate allipertensione portale ( riduzione del gradiente pressorio porto - sistemico del 63 , 3% )  . 
 come suggerito da alcuni autori nei soggetti con sbc in stadio di malattia terminale per grave deterioramento della funzionalit epatica , la tips pu rappresentare un ponte in modo da poter attendere , in condizioni cliniche migliori , un eventuale trapianto di fegato che , viste le attuali carenze di organi , determina lunghe liste di attesa durante le quali una certa percentuale di pazienti non sopravvive [ 30 ]  . 
nel nostro studio abbiamo osservato un elevato tasso di sopravvivenza pari all86 , 6% pari a quello riscontrabile in altri lavori presenti in letteratura [ 9 , 31 ]  . alla luce dei buoni risultati ottenuti dopo tips in termini di sopravvivenza e di miglioramento dei parametri clinici e radiol med ( 2008 ) 113 : 727738 and enables them to survive the long waiting lists generated by the current shortage of organs [ 30 ] .the survival rate in our study was 86.6% , in keeping with that reported by other authors [ 9 , 31 ]  . 
the good results of tips in terms of survival and improved clinical and biochemical parameters meant that none of our patients was subsequently included in a waiting list for liver transplantation , as also reported by other studies [ 32 ]  . 
 conclusions our study confirms previous reports on the feasibility and efficacy of tips in controlling the complications of portal hypertension , improving liver function and consequently the clinical status of patients with bcs . 
 tips should therefore be considered the first - line procedure in subjects with acute or chronic bcs who fail to respond to medical therapy and require portal decompression . biochimici per nessuno dei nostri pazienti stato necessario il successivo inserimento in lista per un trapianto di fegato , atteggiamento peraltro riscontrato anche in altri studi [ 32 ]  . 
 conclusioni la nostra esperienza conferma i dati presenti in letteratura su fattibilit ed efficacia della tips nel controllare le complicanze dellipertensione portale , migliorare la funzionalit epatica e di conseguenza le condizioni cliniche dei pazienti affetti da sbc . 
se eseguita in centri altamente specializzati , per la sua sicurezza ed efficacia , rappresenta una valida alternativa agli shunt di tipo chirurgico proponendosi come trattamento risolutivo a lungo termine senza necessit di ulteriori interventi , in particolare se si impiegano stent ricoperti piuttosto che non ricoperti in quanto nella nostra casistica i primi hanno mostrato tassi di perviet nettamente superiori dei secondi . 
nine cerebral abscesses ( five pyogenic , four from toxoplasma gondii ) , ten glioblastomas and five cerebral metastases in 19 patients were studied with gadolinium - enhanced magnetic resonance imaging , diffusion - weighted imaging ( dwi ) including calculation of mean apparent diffusion coefficient ( adc ) of the lesion core , and pwi . 
nove ascessi cerebrali ( 5 da piogeni , 4 da toxoplasma gondii ) , 10 glioblastomi e 5 metastasi cerebrali in 19 pazienti sono stati studiati con risonanza magnetica con gadolinio endovena , diffusione - rm con calcolo del valore medio del coefficiente di diffusione apparente ( dwi - adc ) del centro della lesione e perfusione - rm . 
alti valori del rcbv nelle aree periferiche dovrebbero indurre al sospetto di tumore necrotico , mentre bassi valori del rcbv possono orientare verso lascesso . 748 radiol med ( 2008 ) 113 : 747757 keywords cerebral abscess cerebral tumours diffusion - weighted imaging perfusion - weighted imaging ring - enhancement parole chiave ascesso cerebrale ring - enhancement diffusione - rm perfusione - rm tumori cerebrali introduction introduzione the differential diagnosis of ring - enhancing cerebral lesions , such as abscesses and necrotic tumours ( high - grade gliomas and metastases ) , is not always possible with conventional magnetic resonance imaging ( mri ) sequences before and after intravenous administration of paramagnetic contrast material [ 1 , 2 ]  . 
the introduction of diffusionweighted imaging ( dwi ) with calculation of the apparent diffusion coefficient ( adc ) has contributed useful information to the differential diagnosis [ 35 ] , with a significant increase in the possibilities of mri , although dwi is encumbered with specificity problems [ 613 ]  . 
proton mr spectroscopy ( 1h - mrs ) has also added to the differential diagnosis , although problems inherent in the technique , lengthy acquisition times and the relatively restricted diffusion of the technique limit its use [ 1416 ]  . 
the rapid passage of paramagnetic contrast material leads to a loss in t2 or t2 * signal in the tissue as a result of magnetic susceptibility in proportion to tissue capillary density . 
the inclusion of the pwi study in clinical practice is becoming increasingly more frequent , in part due to the fast examination and postprocessing times provided by the latest technological innovations . 
the use of pwi in studying brain tumours has received significant attention in the literature [ 1721 ] , although few studies have compared the findings of conventional mri , dwi and pwi in the differential diagnosis between brain abscesses and necrotic brain tumours [ 2225 ]  . the aim of this study was to assess the usefulness of pwi in the differential diagnosis between brain abscesses , highgrade gliomas and brain metastases . la diagnosi differenziale delle lesioni cerebrali che si presentano con ring - enhancement , quali ascessi e tumori necrotici ( gliomi di alto grado e metastasi ) , non sempre possibile mediante uno studio di risonanza magnetica ( rm ) con sequenze convenzionali prima e dopo somministrazione ev di mezzo di contrasto paramagnetico ( mdc ) [ 1 , 2 ]  . 
lintroduzione della tecnica in diffusione con il calcolo del coefficiente di diffusione apparente ( dwi - adc ) ha aggiunto utili elementi di diagnostica differenziale [ 35 ] , con consensuale significativo incremento delle possibilit della rm , ma anche lo studio dwi - adc resta gravato da problemi di specificit [ 613 ]  . 
lutilizzo della spettroscopia dellidrogeno con rm ( 1h - mrs ) ha fornito un valido contributo nella diagnosi differenziale , ma alcuni problemi inerenti alla tecnica , i lunghi tempi di acquisizione e la relativamente scarsa diffusione sul territorio limitano lutilizzo di questa possibilit [ 1416 ]  . 
il rapido passaggio di mdc paramagnetico somministrato a bolo determina la riduzione del segnale t2 o t2 * nei tessuti , per effetto di suscettibilit magnetica , in rapporto alla densit capillare del tessuto . 
linclusione dello studio in perfusione - rm nella pratica clinica sempre pi frequente , in rapporto alla rapidit dellesecuzione e della elaborazione nel post - processing grazie alle pi recenti evoluzioni tecnologiche . 
the patient with multiple toxoplasma brain abscesses was suffering from aids and was immunocompromised . conventional mri study was performed with conventional t2 [ fast spin echo ( fse ) , fluid - attenuated inversion recovery ( flair ) ] and t1 ( flair ) sequences , with the latter also being used after the intravenous administration of paramagnetic contrast material ( gadobutrol , 0.1 mmol / kg , gadovist , schering , germany )  . 
the dwi study was performed with a t2 - weighted , echoplanar spin - echo sequence ( tr 10 , 000 , te 78 , matrix 128128 , slice thickness 5 mm , gap 1.5 ) with a duration of 40 s and b = 0 and b = 1 , 000 . isotropic maps of the adc were calculated , and the mean adc was measured in the lesion core . 
the pwi study was performed with a t2 - weighted echoplanar spin - echo sequence ( tr 1 , 900 , te 80 , matrix 192128 , slice thickness 7 mm , gap 0 , number of scans 13 ) with a duration of 67 s . forty images per second were acquired during the passage of a bolus of 0.1 mmol / kg of gadobutrol , injected with an automatic injector at a flow velocity of 5 ml / s through an 18to 20 - gauge needle cannula , followed by 20 ml of saline solution . 
colour maps of the cerebral blood volume were generated , and the mean of the maximum regional cerebral blood volume ( rcbv ) was calculated by placing a region of interest ( roi ) in the peripheral solid areas showing a colour at the upper end of the colour scale . 
data were then compared with those of the normal - appearing contralateral white matter and expressed as a ratio of rcbv [ ratio = rcbv ( lesion ) / rcbv ( contralateral white matter ) ]  . diagnoses of pyogenic abscess , high - grade glioma and metastasis were in all cases performed by stereotactic biopsy . 
lo studio dwi - adc stato condotto mediante una sequenza eco - planare spin - echo t2 pesata ( tr 10000 , te 78 , matrice 128128 , spessore 5 , gap 1 , 5 ) , della durata di 40 secondi con un valore del b = 0 e b = 1000 . 
sono state calcolate le mappe isotropiche delladc e misurato il valore medio delladc nellarea centrale delle lesioni . lo studio perfusione - rm stato condotto mediante una sequenza eco - planare spin - echo t2 pesata ( tr 1900 , te 80 , matrice 192128 , spessore 7 , gap 0 , numero di scansioni 13 ) , della durata di 67 secondi , con acquisizioni di 40 immagini per sezione , durante il passaggio di un bolo di 0 , 1 mmol / kg di gadobutrolo , iniettato alla velocit di flusso di 5 ml / s , tramite iniettore automatico , attraverso agocannula di 1820 gauge , seguito da un flush di 20 ml di soluzione salina . 
il calcolo del valore medio del massimo volume ematico cerebrale regionale ( rcbv ) stato valutato tramite posizionamento di roi nelle aree solide periferiche che mostravano un colore posto nella parte pi alta della scala cromatica . 
i dati ottenuti sono stati successivamente confrontati con quelli della sostanza bianca controlaterale di aspetto normale e considerati come ratio del rcbv [ ratio = rcbv ( lesione ) / rcbv ( sostanza bianca controlaterale ) ]  . 
la diagnosi di ascessi cerebrali da toxoplasma gondii stata eseguita sulla base dellefficacia della terapia antibiotica specifica al controllo clinico - neuroradiologico . risultati nello studio rm convenzionale ( figg 1a , 2a , 3a , 4a ) , tutte le lesioni presentavano il tipico aspetto a ring - enhancement , circondate da un variabile grado di edema perilesionale vasogenico . 
several signs indicative of brain abscess have been described , such as hyperintensity on t1 - weighted images and / or hypointensity on t2 - weighted images of the capsule , the presence of satellite lesions and a hypointense rithese signs , however , are not specific and can also be encountered in highgrade gliomas and brain metastases [ 1 , 2 ]  . dwi study provided useful support for determining the nature of ring - enhancing lesions [ 3 , 5 ]  . 
the appropriate antibiotic therapy leads to improved diffusion and increased adc values [ 26 ]  . restricted diffusion in ring - enhancing lesions , however , is not pathognomic of brain abscess . 
the literature describes cases of brain metastases with hyperintense signal on dwi and reduced adc values [ 4 , 810 ] and cases of glioblastoma multiforme with low adc values in the necrotic core , similar to findings in pyogenic abscesses [ 6 , 7 ]  . 
in addition , as most of the few cases reported in the literature demonstrate , some brain abscesses , such as those due to toxoplasmosis , can produce hypointensity on dwi images and high adc values in the necrotic core . 
these values are the same as or higher than those of normal - appearing white matter and not reduced as in pyogenic abscesses [ 12 , 13 ]  . nello studio perfusione - rm , gli ascessi cerebrali hanno presentato una media della ratio del rcbv della porzione capsulare di 0 , 770 , 9 ( range : 0 , 60 , 91 )  . 
sono stati descritti alcuni segni indicativi di ascesso cerebrale , quali liperintensit nelle immagini t1 - dipendenti e / o la ipointensit in quelle t2 - dipendenti della capsula , la presenza di lesioni satelliti ed un cercine periferico di impregnazione sottile e regolare . 
lappropriata terapia antibiotica ne induce la riduzione della diffusione con aumento dei valori delladc [ 26 ]  . la ridotta diffusione nelle lesioni con ring - enhancement , tuttavia , non patognomonica di ascesso cerebrale . 
in letteratura , sono stati descritti casi di metastasi cerebrali iperintense in dwi e con ridotti valori delladc [ 4 , 810 ] e casi di glioblastoma multiforme con bassi valori delladc nel centro necrotico , come riscontrabile di solito negli ascessi da piogeni [ 6 , 7 ]  . 
inoltre , alcuni ascessi cerebrali , quali quelli da toxoplasma gondii , possono presentare ipointensit nelle immagini dwi ed elevati valori di adc nellarea centrale necrotica , uguale o aumentato rispetto alla sostanza bianca , e non ridotti come negli ascessi da piogeni , come dimostrato nella gran parte dei pochi casi riportati in letteratura [ 12 , 13 ]  . le caratteristiche istopatologiche dellascesso da toxoplasma gondii ed il tipo della risposta immunitaria del paradiol med ( 2008 ) 113 : 747757 the histopathological characteristics of toxoplasma abscesses and the type of immune response by the patient appear to explain the different dwi appearance with respect to pyogenic abscesses [ 12 ]  . 
the encephalitis caused by toxoplasmosis can progress with the formation of abscesses peripherally composed of inflammatory cells , free tachyzoites and encysted bradyzoites , and with a core of primarily necrotic tissue that does not have the viscous , proteinaceous material of pus that tends to restrict the diffusion of water molecules . 
therefore , the dwi appearance of toxoplasma abscesses is more similar to that of necrotic tumours than of pyogenic abscesses , which suggests that dwi does not always contribute to the correct differential diagnosis between abscesses and necrotic tumours . combined 1h - mrs and dwi has made an important contribution to the differential diagnosis . 
pyogenic abscesses and necrotic tumours both display lactate and lipid peaks produced by anaerobic glycolysis and cellular necrosis . however , in pyogenic brain abscesses 1h - mrs shows acetate , lactate and amino acid peaks the products of bacterial metabolism and the absence of normal cerebral components such as n - acetyl - aspartate ( naa ) , choline ( cho ) and creatine ( cr ) [ 16 ]  . 
these characteristic spectra are not found in pyogenic abscesses treated with antibiotics , which rather show nonspecific lactate and lipid peaks , which are also found in cystic tumours [ 5 ]  . glioblastomas display elevated cho and cr peaks and a reduction in naa . 
approximately two thirds of metastases display an elevated lipid peak in the absence of naa , but this pattern can also be found in 10% of glioblastomas [ 15 ]  . in toxoplasma abscesses , one study demonstrated variability in the spectroscopic peaks , with a consequent absence of specificity [ 27 ]  . 
in addition , 1h - mrs has the disadvantages of relatively long acquisition times and possible spectra contamination by normal brain parenchyma or adjacent oedema [ 13 ]  . pwi is a technique that provides information about cerebral haemodynamics . 
administration of a bolus of paramagnetic contrast material causes a loss in the t2 or t2 * signal of brain tissue due to magnetic susceptibility in proportion to tissue capillary density . 
in intracranial lesions , mr signal intensification after gadolinium administration is associated with the rupture of the blood - brain barrier , whereas in pwi , the signal is independent of the condition of the blood - brain barrier yet dependent on the microvascularity of the lesions themselves . 
the measurement of rcbv can therefore be used to identify and quantify the areas of neovascularisation ; rcbv maps are generally used to characterise intraand extra - axial tumours , to grade ziente spiegherebbero il diverso aspetto dwi - adc rispetto allascesso da piogeni [ 12 ]  . 
lencefalite da toxoplasma gondii pu evolvere con la formazione di ascessi costituiti alla periferia da cellule infiammatorie , tachizoidi liberi , bradizoidi incistati , e da unarea centrale necrotica con cellule infiammatorie e proteine la cui viscosit sarebbe inferiore rispetto a quella degli ascessi da piogeni con un aumento della diffusione delle molecole dacqua libere . 
queste osservazioni dimostrano che la dwi - adc non contribuisce sempre alla corretta diagnosi differenziale tra ascessi e tumori necrotici . la combinazione della 1h - mrs ha apportato un valido contributo nella diagnosi differenziale . 
tuttavia , negli ascessi cerebrali da piogeni la 1hmrs dimostra picchi di acetato , lattato e amino - acidi , quali prodotti del metabolismo batterico , ed assenza dei normali componenti cerebrali di n - acetil - aspartato ( naa ) , colina ( cho ) , creatina ( cr ) [ 16 ]  . 
questo caratteristico spettro non si riscontra negli ascessi da piogeni trattati con antibiotici che mostrano un picco di lattato e lipidi non specifico , riscontrabile anche nelle neoplasie cistiche [ 5 ]  . 
circa i 2 / 3 delle metastasi mostrano un picco elevato di lipidi in assenza del picco di naa , ma questo pattern pu essere riscontrato anche nel 10% dei glioblastomi [ 15 ]  . 
come noto , inoltre , lo studio con 1h - mrs presenta degli svantaggi , quali i tempi di acquisizione relativamente lunghi e la possibile contaminazione dello spettro da parte del parenchima cerebrale normale o delledema adiacente [ 13 ]  . la perfusione - rm una tecnica che fornisce informazioni sullemodinamica cerebrale . 
la somministrazione a bolo del mdc paramagnetico determina una riduzione del segnale t2 o t2 * del tessuto cerebrale , per effetto di suscettibilit magnetica , in rapporto alla densit capillare del tessuto . 
nelle lesioni cerebrali , lintensificazione del segnale rm dopo la somministrazione di gadolinio associato alla rottura della barriera emato - encefalica , mentre nella perfusione - rm il segnale indipendente dalle condizioni della barriera emato - encefalica ma dipende dalla microvascolarizzazione delle lesioni stesse . 
unlike 1h - mrs , pwi can be implemented rapidly in daily clinical practice , and the postprocessing does not influence the number of examinations to be performed during an mri session , thanks to recent technological advancements . the usefulness of pwi in the study of brain tumours has e dellintervento neurochirurgico , ed infine possono consentire la diagnosi differenziale tra recidiva tumorale e radionecrosi . 
a nostra conoscenza , non esistono in letteratura studi che confrontano i reperti allo studio rm convenzionale , dwi - adc e perfusione rm nella diagnosi differenziale tra ascessi cerebrali da piogeni , ascessi da toxoplasma gondii , gliomi di alto grado e metastasi necrotiche . 
alcuni studi hanno dimostrato bassi valori del rcbv misurato alla periferia degli ascessi da piogeni rispetto agli alti valori misurati alla periferia dei gliomi di alto grado e del754 radiol med ( 2008 ) 113 : 747757 fig . 
gadolinium - enhanced t1 - weighted magnetic resonance image ( gd - mri ) , diffusionweighted ( dwi , b = 1 , 000 ) , apparent diffusion coefficient ( adc ) map and regional cerebral blood volume ( rcbv ) perfusion - weighted ( pwi ) axial images of a pyogenic abscess in the left frontal lobe . 
the central component of the lesion shows clear - cut high signal intensity at dwi ( b ) , and hypointense signal ( 1 ) in adc map ( c ) when compared with contralateral normal - appearing white matter at dwi , these findings being consistent with restricted diffusion . 
immagini rm assiali ottenute con sequenza t1 - dipendente dopo gadolinio ev ( gd - rm ) , diffusione - rm ( dwi , b = 1000 ) , coefficiente di diffusione apparente ( adc ) , e perfusione - rm con misura del volume ematico cerebrale regionale ( rcbv ) di un ascesso da piogeno frontale sinistro . 
la componente centrale della lesione appare iperintensa alla dwi ( b ) ed ipointensa ( 1 ) nella mappa adc ( c ) rispetto alla sostanza bianca controlaterale normale alla dwi - adc , reperti congrui con riduzione della diffusione . 
gadolinium - enhanced t1 - weighted magnetic resonance image ( gd - mri ) ( a ) , diffusionweighted ( dwi , b = 1 , 000 ) ( b ) and apparent diffusion coefficient ( adc ) ( c ) and regional cerebral blood volume ( rcbv ) perfusion - weighted imaging ( pwi ) axial images of a toxoplasma gondii abscess in the right frontal lobe . 
immagini rm assiali ottenute con sequenza t1 - dipendente dopo gadolinio ev ( gd - rm ) , diffusione - rm ( dwi , b = 1000 ) , coefficiente di diffusione apparente ( adc ) , e perfusione - rm con misura del volume ematico cerebrale regionale ( rcbv ) di un ascesso da toxoplasma gondii in sede frontale destra . limmagine gd - rm ( a ) mostra una lesione con caratteristiche a tipo ring - enhancement e marcato edema vasogenico perilesionale . 
la componente centrale della lesione appare isointenso alla sostanza bianca controlaterale normale alla dwi ( b ) ed iperintensa nella mappa adc ( c ) rispetto alla sostanza bianca controlaterale normale alla dwi - adc , reperti congrui con incremento della diffusione . 
gadolinium - enhanced t1 - weighted magnetic resonance image ( gd - mri ) ( a ) , diffusionweighted ( dwi , b = 1 , 000 ) ( b ) and apparent diffusion coefficient ( adc ) ( c ) and regional cerebral blood volume ( rcbv ) perfusion - weighted imaging ( pwi ) axial images of a glioblastoma in the left frontal lobe . 
the central component of the lesion shows isointensity at dwi ( b ) and high signal intensity ( 1 ) in the adc map ( c ) when compared with the contralateral normal - appearing white matter at dwi - adc , findings that are consistent with increased diffusion . 
immagini rm assiali ottenute con sequenza t1 - dipendente dopo gadolinio ev ( gd - rm ) , diffusione - rm ( dwi , b = 1000 ) , coefficiente di diffusione apparente ( adc ) , e perfusione - rm con misura del volume ematico cerebrale regionale ( rcbv ) di un glioblastoma frontale sinistra . 
la componente centrale della lesione appare isointenso alla dwi ( b ) ed iperintensa nella mappa adc ( c ) rispetto alla sostanza bianca controlaterale normale alla dwi - adc , reperti congrui con incremento della diffusione . 
gadolinium - enhanced t1 - weighted magnetic resonance image ( gd - mri ) ( a ) , diffusionweighted ( dwi , b = 1 , 000 ) ( b ) and apparent diffusion coefficient ( adc ) ( c ) and regional cerebral blood volume ( rcbv ) perfusion - weighted imaging ( pwi ) axial images of a right frontal lobe metastasis from breast carcinoma . 
the central component of the lesion shows low signal intensity at dwi ( b ) and high signal intensity in the adc map ( c ) when compared with contralateral normal - appearing white matter at dwi - adc ; these findings are consistent with increased diffusion . 
immagini rm assiali ottenute con sequenza t1 - dipendente dopo gadolinio ev ( gd - rm ) , diffusione - rm ( dwi , b = 1000 ) , coefficiente di diffusione apparente ( adc ) , e perfusione - rm con misura del volume ematico cerebrale regionale ( rcbv ) di una metastasi da carcinoma della mammella in sede frontale destra . 
la cavit della lesione appare ipointensa alla dwi ( b ) ed iperintensa nella mappa adc ( c ) rispetto alla sostanza bianca controlaterale normale alla dwi - adc , segni congrui con incremento della diffusione . 
these findings agree with our results , which showed an rcbv ratio in the capsular portion of the five pyogenic abscesses of 0.720.08 , in the periphery of high - grade gliomas of 4.451.50 and in metastases of 3.580.68. the explanation for the pwi findings lies in the fact that the capsule of pyogenic abscesses is prevalently composed of collagen fibres with a low capillary density and reduced rcbv , whereas high - grade tumours and metastases are associated with increased neovascularisation , with high capillary density and therefore high rcbv values . the periphery of the four toxoplasma abscesses described in this study also presented low rcbv values ( 0.840.07 ) , in agreement with the limited data reported in the literature [ 13 , 22 ]  . 
only the pwi findings , therefore , suggested the lesion was not a necrotic tumour , as the abscess showed a hypovascularity in the capsule with respect to normal - appearing white matter . le metastasi [ 2325 ]  . 
 [ 23 ] hanno osservato un valore medio della ratio del rcbv nella capsula di quattro ascessi cerebrali ( 0 , 450 , 11 ) inferiore a quella valutata nella rima periferica di impregnazione di lesioni neoplastiche infette ( 2 , 900 , 62 )  . 
 [ 25 ] hanno descritto quattro ascessi da piogeni con una ratio del rcbv di 0 , 760 , 12 , nettamente inferiore rispetto ai valori riscontrati in otto gliomi di alto grado ( 5 , 512 , 08 ) e sette metastasi ( 4 , 582 , 19 )  . questi dati concordano con i nostri risultati che hanno evidenziato una ratio del rcbv nella porzione capsulare dei 5 ascessi da piogeni di 0 , 720 , 08 e nella periferia dei gliomi di alto grado di 4 , 451 , 5 e delle metastasi di 3 , 580 , 68 . la spiegazione dei reperti alla perfusione - rm che la capsula degli ascessi da piogeni costituita prevalentemente da fibre collagene con una bassa densit capillare e ridotti valori di rcbv , mentre le neoplasie di alto grado e le metastasi sono associate ad un incremento della neovascolarizzazione , con alta densit capillare e conseguenti elevati valori di rcbv . anche alla periferia dei quattro ascessi da toxoplasma gondii descritti in questo lavoro , abbiamo riscontrato bassi valori dellrcbv , con una media della ratio di 0 , 840 , 07 , in accordo con i pochi dati della letteratura [ 13 , 22 ]  . 
in particolare , i quattro ascessi nel paziente affetto da toxoplasma gondii si presentavano come lesioni con ringenhancement , isointensi nelle immagini dwi , con elevato valore delladc rispetto agli ascessi da piogeni , ma con media della ratio del rcbv nellarea periferica di 0 , 840 , 07 ( range : 0 , 750 , 91 )  . 
soltanto i reperti della perfusione - rm , quindi , ponevano il dubbio che non si trattasse di tumori necrotici , dimostrando una ipovascolarizzazione della capsula rispetto alla sostanza bianca indenne . conclusions conclusioni even with the use of dwi and 1h - mrs , mri does not present absolute specificity in the differential diagnosis of ring - enhancing brain lesions . 
further validation can be provided by spectroscopy , although pwi has faster examination and postprocessing time . pur con lutilizzo di dwi - adc e 1h - mrs , lo studio rm non presenta una specificit assoluta nella diagnosi differenziale delle lesioni cerebrali con ring - enhancement . 
alti valori del rcbv nelle aree periferiche di lesioni con ring - enhancement dovrebbero indurre al sospetto di neoplasia necrotica ; viceversa bassi valori del rcbv possono orientare verso la diagnosi di ascesso cerebrale . 
brambilla6 1dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 2dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria di parma , parma , italy 3dipartimento di radiologia , universit degli studi di napoli , napoli , italy 4dipartimento di radiologia , universit degli studi di milano , milano , italy 5dipartimento di radiologia , universit degli studi di verona , verona , italy 6unit di riabilitazione cardiovascolare , fondazione don gnocchi onlus , parma , italy correspondence to : f . 
cademartiri , viale rustici 2 , 43100 parma , italy , tel . : + 39 - 052 - 1961833 , e - mail : filippocademartiri@hotmail.com received : 5 july 2007 / accepted : 6 september 2007 / published online : 13 may 2008 springer - verlag 2008 abstract purpose . 
forty - nine patients with type 2 diabetes mellitus ( dm ) [ group 1 ; mean age 67.78.8 years ; 32 men ; mean body mass index ( bmi ) 283.9 ] and 49 patients without dm ( group 2 , with similar demographic and clinical characteristics ) were studied with msct coronary angiography to exclude the presence of ischaemic coronary artery disease ( cad )  . 
each group comprised 26 patients ( 53% ) with no history of ischaemic coronary disease and 23 patients ( 47% ) with a history of myocardial infarction and / or myocardial revascularisation . 
quarantanove pazienti con diabete mellito tipo - 2 ( dm ) , gruppo i , ( et media : 67 , 78 , 8 anni ; maschi 32 ; bmi medio : 283 , 9 ) e 49 pazienti senza dm , gruppo ii , con sovrapponibili caratteristiche demografiche e cliniche , sono stati sottoposti a studio coronarografico con tcms per escludere la presenza di coronaropatia ischemica . 
relativamente ad ogni gruppo , 26 pazienti ( 53% ) erano senza storia di cardiopatia ischemica , mentre 23 ( 47% ) avevano storia di pregresso infarto miocardico e / o rivascolarizzazione miocardica . 
event - free survival is significantly lower in the diabetic population compared with the normal control population ( p = 0.046 ) and is closely correlated with the presence of significant cad . 
inoltre , il tasso di eventi cardiaci cumulativi risultato significativamente correlato alla presenza di malattia significativa ( stenosi > 50% ) in entrambi i gruppi ( gruppo i : p = 0 , 003 ; gruppo ii : p = 0 , 0004 )  . 
la sopravvivenza libera da eventi cardiaci significativamente pi bassa nella popolazione diabetica rispetto alla popolazione normale di controllo ( p = 0 , 046 ) ed strettamente correlata alla presenza di malattia significativa . 
la tcms una metodica efficace nella stratificazione del rischio e , insieme allaccuratezza diagnostica , offre un valore prognostico aggiunto . parole chiave valore prognostico tc multistrato diabete mellito coronarografia non invasiva introduction introduzione the increasing prevalence of type 2 ( non - insulin - dependent ) diabetes mellitus ( dm ) throughout the world will have major cardiovascular consequences in the future given that dm is the main risk factor for atherosclerotic disease [ 1 ]  . 
previous epidemiological studies have established that the risk of death due to ischaemic heart disease is two to four times higher among diabetic than nondiabetic patients [ 2 ]  . 
furthermore , the long - term rate of cardiac events in diabetic patients without a history of cad is similar to that in nondiabetic patients with known cad [ 3 ]  . 
the added value of msct ( apart from noninvasiveness ) with respect to the gold standard , coronary angiography , is that it provides high diagnostic accuracy in the assessment of the coronary artery wall , plaque morphology and distribution and arterial lumen . 
the aim of this study was to assess the prognostic value of msct in diabetic patients with known or suspected cad and to compare it with a nondiabetic control population having similar clinical and demographic characteristics . 
in particular , we evaluated how dm and cad severity affect event - free survival in a population studied by msct for suspected cad . materials and methods patients laumento della prevalenza del diabete mellito ( dm ) tipo - 2 ( non insulino - dipendente ) che si sta registrando in tutto il mondo avr nel futuro importanti conseguenze cardiovascolari dato che il principale fattore di rischio per lo sviluppo della malattia aterosclerotica [ 1 ]  . 
da precedenti studi epidemiologici , ormai noto che il rischio di mortalit per cardiopatia ischemica da 2 a 4 volte maggiore nei pazienti diabetici rispetto alla popolazione non diabetica [ 2 ]  . 
inoltre , gli eventi cardiaci a lungo termine nei pazienti diabetici senza storia di cad sono sovrapponibili a quelli della popolazione non diabetica con nota cad [ 3 ]  . 
il valore aggiunto della tcms ( oltre alla non invasivit ) rispetto al gold - standard rappresentato dalla coronarografia , di consentire unanalisi della parete coronarica e della morfologia e distribuzione di placca , oltre che del lume arterioso , con elevata accuratezza diagnostica . 
lo scopo di questo lavoro di valutare il valore prognostico della tcms nei pazienti diabetici con nota o sospetta cad e confrontarla con una popolazione non diabetica di confronto con analoghe caratteristiche cliniche e demografiche . 
in particolare , analizzeremo come il dm e la severit della malattia coronarica rilevata influiscano sulla sopravvivenza libera da eventi cardiaci in una popolazione sottoposta a tcms per sospetta cad . materiali e metodi pazienti between january and june 2005 , 49 consecutive patients with a diagnosis of dm ( group 1 ) and 49 consecutive padurante il periodo gennaio - giugno 2005 , 49 pazienti conseradiol med ( 2008 ) 113 : 627643 tients without dm ( group 2 ) with similar demographic and clinical characteristics were studied with msct coronary angiography to exclude the presence of ischaemic cad . the characteristics of the two populations are summarised in table 1 . 
we included patients with a diagnosis of type 2 dm for at least 5 years on the basis of impaired glucose tolerance ( fasting plasma glu 126 mg / dl or post oral glucose tolerance test ( ogtt ) 200 mg / dl ) and receiving treatment with diet , oral hypoglycaemic medications or insulthe indication for msct was based on symptoms ( typical chest pain , atypical chest pain , other symptoms ) and / or cardiovascular risk profile and / or abnormal or equivocal functional tests . 
each group comprised 26 patients ( 53% ) with no history of ischaemic heart disease and 23 ( 47% ) with a history of myocardial infarction and / or myocardial revascularisation . 
moreover , in each group , ten patients were asymptomatic ( 20.4% ) , 14 had typical chest pain ( 28.6% ) , 16 had atypical chest pain ( 32.6% ) and nine ( 18.4% ) had dyspnoea or arrhythmia ( other symptoms )  . 
inclusion criteria for the msct study were regular heart rhythm < 65 bpm , no contraindications for the use of contrast medium , and ability to hold breath for 15 s . 
all patients were interviewed at the time of the examination to assess symptoms and risk factors . all patients provided informed consent to the study protocol , which received the approval of the local ethics committee . follow - up patients were followed up by either clinical visits or telephone interviews . 
nonfatal myocardial infarction was defined on the basis of typical chest pain , elevation of cardiac enzyme levels and typical changes on the electrocardiogram . cutivi con diagnosi di dm , gruppo i , e 49 pazienti consecutivi senza dm , gruppo ii , con sovrapponibili caratteristiche demografiche e cliniche sono stati sottoposti a studio coronarografico con tcms per escludere la presenza di coronaropatia ischemica . 
abbiamo incluso pazienti con diagnosi di dm tipo - 2 da almeno 5 anni sulla base della conferma di ridotta tolleranza al glucosio ( glu plasmatico a digiuno 126 mg / dl o post - ogtt 200 mg / dl ) e del trattamento con dieta , ipoglicemizzanti orali o insulina . 
lindicazione alla tcms stata posta sulla base dei sintomi ( dolore toracico tipico , dolore toracico atipico , altri sintomi ) e / o del profilo di rischio cardiovascolare e / o dei test diagnostici funzionali anormali o dubbi . 
relativamente ad ogni gruppo , 26 pazienti ( 53% ) erano senza storia di cardiopatia ischemica , mentre 23 ( 47% ) avevano storia di pregresso infarto miocardico e / o rivascolarizzazione miocardica . 
inoltre , rispetto ad ogni gruppo , 10 pazienti erano asintomatici ( 20 , 4% ) , 14 con dolore toracico tipico ( 28 , 6% ) , 16 con dolore toracico atipico ( 32 , 6% ) e 9 ( 18 , 4% ) con dispnea o aritmia ( altri sintomi )  . 
i criteri di inclusione per lesecuzione dellesame sono stati : ritmo cardiaco regolare < 65 bpm ; assenza di controindicazioni allutilizzo di mezzo di contrasto ; capacit di mantenere unapnea per 15 secondi . 
tutti i pazienti sono stati intervistati al momento dellesame per la valutazione dei sintomi e dei fattori di rischio e hanno fornito per iscritto il loro consenso informato per lo studio approvato dal comitato etico locale . follow - up tutti i pazienti sono stati sottoposti a follow - up clinico e / o tramite intervista telefonica , con successiva consultazione dellarchivio cardiologico interno dellospedale per la conferma delle informazioni raccolte . 
gli end - point clinici che abbiamo valutato sono stati le rivascolarizzazioni miocardiche ( percutanee e chirurgiche ) e gli eventi cardiaci maggiori ( ecm ) : morte cardiaca , infarto miocardico non fatale e ospedalizzazione per angina instabile . 
linfarto miocardico non fatale stato definito sulla base dei criteri di dolore toracico tipico , innalzamento degli enzimi miocardiospecifici e modificazioni tipiche dellelettrocardiogramma . scan protocol protocollo di scansione all examinations were conducted with a 64 - slice ct scanner ( somatom sensation 64 , siemens medical solution , germany ) with cardiac synchronisation . 
all patients received instructions with respect to the examination and the breath - hold procedure . patients were administered 100 ml of contrast medium ( iomeron 400 , bracco , milan , italy ) in an antecubital vein at a high flow rate ( 45 ml / s ) , followed by a 40 - ml bolus of saline at the same rate . lesame stato condotto con apparecchiatura tcms a 64strati ( somatom sensation 64 , siemens medical solution , germania ) con sincronizzazione cardiaca . 
attraverso una vena antecubitale del braccio , sono stati somministrati 100 ml di mezzo di contrasto ( iomeron 400 , bracco , milano , italia ) ad alto flusso ( 45 ml / s ) seguiti da un bolo di soluzione fisiologica di 40 ml alla stessa velocit di flusso . patient characteristics group 1 : diabetic patients group 2 : nondiabetic patients radiol med ( 2008 ) 113 : 627643 table 1 patient characteristics no . 
of patients age ( years ; meansd ) males ( % ) bmi ( kg / m2 ; meansd ) mean heart rate ( bpm ) follow - up ( months ; meansd ) cad history negative ( % ) positive ( % ) prior ami ( % ) prior revascularisation ( % ) prior ami + revascularisation ( % ) risk factors no . 
 bmi , body mass index ; bpm , battiti per minuti ; cad , malattia aterosclerotica coronarica ; ima , infarto miocardico acuto radiol med ( 2008 ) 113 : 627643 synchronisation of the scan with the arrival of the contrast bolus was achieved by using the bolus tracking technique with a threshold of 100 hounsfield units [ 12 ]  . 
scan parameters were number of detectors 322 , individual detector width 0.6 mm , gantry rotation time 330 ms , effective temporal resolution 165 ms , table feed 3.84 mm / rotation , tube voltage 120 kvp , tube current 900 mas , scanning direction craniocaudal . 
to obtain optimal image quality , the data sets were reconstructed in the mid to end diastolic and end systolic phase using retrospective electrocardiogram ( ecg ) gating ( 350 ms and + 275 ms )  . 
cad was defined as the presence of any atherosclerotic plaque , intended as a structure > 1 mm within or adjacent to the coronary artery lumen , which could be clearly distinguished from the vessel lumen and the surrounding pericardial tissue [ 9 ]  . 
the results obtained were divided into three groups : intact coronary arteries ( no evidence of atherosclerotic plaque ) , nonsignificant disease ( plaque causing 50% luminal narrowing ) and significant disease ( plaque causing > 50% luminal narrowing )  . statistical analysis to analyse the frequency of disease distribution ( intact coronaries , nonsignificant and significant disease ) , we used the chi square test or the fisher exact test . 
i parametri di acquisizione sono stati : numero di detettori : 322 ; ampiezza individuale del rilevatore : 0 , 6 mm ; tempo di rotazione del gantry : 330 ms ; risoluzione temporale effettiva : 165 ms ; avanzamento del lettino porta - pazienti : 3 , 84 mm / rotazione ; tensione del tubo : 120 kvp ; corrente 900 mas ; direzione della scansione craniocaudale . 
per ottenere una qualit delle immagini ottimale , i set di dati sono stati ricostruiti nella fase meso / tele - diastolica e tele - sistolica utilizzando lecg - gating retrospettivo ( 350 ms e + 275 ms )  . 
le ricostruzioni assiali venivano poi trasferite ad una stazione di lavoro dedicata ( leonardo , siemens , forchheim , germania ) per il post - processing e la conseguente analisi . 
in caso di disaccordo , dopo unanalisi comune veniva trovato un accordo . le coronarie sono state suddivise in 15 segmenti in accordo alla classificazione modificata dellamerican heart association [ 13 ]  . 
la malattia coronaria stata definita dalla presenza di qualsiasi placca aterosclerotica , intesa come struttura > 1 mm allinterno o adiacente al lume coronarico , che pu essere chiaramente distinta dal lume del vaso e dal tessuto pericardio circostante [ 9 ]  . 
i risultati ottenuti sono stati suddivisi in 3 gruppi : coronarie indenni ( nessuna evidenza di placche aterosclerotiche ) , malattia non significativa ( placca aterosclerotica determinante restringimento del lume 50% ) e malattia significativa ( placca aterosclerotica determinante restringimento del lume > 50% )  . analisi statistica per lanalisi delle frequenze relative alla distribuzione di malattia ( coronarie indenni , malattia non significativa e malattia significativa ) stato utilizzato il test del chi - quadrato o il test esatto di fisher . 
the log - rank test was used to assess the relationship between the rate of cardiac events and cad severity as detected on msct ( intact coronaries , nonsignificant and significant disease ) for each group . 
contestualmente per ogni gruppo stata valutata , mediante log - rank test , la relazione fra il tasso di eventi cardiaci e la presenza e la severit della coronaropatia riscontrata alla tcms , considerando tre sottogruppi : coronarie indenni ( nessuna evidenza di malattia coronarica ) , malattia non significativa ( malattia coronarica determinante stenosi 50% ) e malattia significativa ( malattia coronarica determinante stenosi > 50% )  . 
among the diabetic population ( group 1 ) the prevalence of intact coronary arteries was 6.1% , that of nonsignificant disease was 34.7% and that of significant disease was 59.2%. 
a correlation was evident between typical chest pain and significant disease for both groups , and among the diabetic population there was a higher prevalence of significant disease , whereas in the nondiabetic population there was a prevalence of intact coronary arteries ( p value not significant )  . 
there was a higher prevalence of obstructive disease ( causing > 50% luminal narrowing ) in the diabetic population ( p = 0.02 ) , which also affected 33% of asymptomatic patients . tutti i segmenti coronarici ( 1470 ) sono stati considerati valutabili . 
relativamente alla popolazione diabetica generale , gruppo i , la prevalenza delle coronarie indenni stata del 6 , 1% , della malattia non significativa del 34 , 7% e della malattia significativa del 59 , 2% . 
la stessa prevalenza nei pazienti non diabetici , gruppo ii , stata del 20 , 4% per le coronarie indenni , del 40 , 8% per la malattia non significativa e del 38 , 8% per la malattia significativa . 
la differenza statistica permane suddividendo entrambi i gruppi in base alla storia clinica e considerando i pazienti senza storia pregressa di cardiopatia ischemica ( cad ) ( p = 0 , 02 )  . 
11 , 5% ( p = 0 , 02 )  . analizzando i pazienti con storia pregressa di cad , nessuna differenza statistica stata osservata relativamente alla presenza e distribuzione della malattia coronarica , essendo la prevalenza di malattia nei pazienti diabetici vs . 
1 viene riportata la distribuzione di malattia in funzione dei sintomi e della presenza del dm , nella quale si osserva una correlazione fra dolore tipico e malattia significativa per entrambi i gruppi e come nella popolazione diabetica vi sia una maggior prevalenza di malattia significativa , al contrario della popolazione non diabetica nella quale prevalgono le coronarie indenni ( valore di p non significativo )  . 
graphs show a higher prevalence of significant disease in the diabetic population ( top graph ) and of intact coronary arteries in the nondiabetic population ( bottom graph )  . 
i grafici illustrano come vi sia una maggior prevalenza di malattia significativa nella popolazione diabetica ( in alto ) e di coronarie indenni nella popolazione non diabetica ( in basso )  . 
la prevalenza di malattia significativa e quella di malattia coronarica significativa e non significativa insieme pi elevata nei pazienti diabetici rispetto ai non diabetici . in particolare si osserva anche come nei diabetici esista una consistente prevalenza di malattia significativa nella categoria altri sintomi . 
in group 1 , there were six mce in five patients ( 10.2% ) , of which three were hospital admissions for unstable angina and three were non - stsegment - elevation myocardial infarctions ( nstemi )  . 
relativamente al gruppo i , abbiamo registrato 6 ecm in 5 pazienti ( 10 , 2% ) , di cui 3 ricoveri per angina instabile e 3 sindromi coronariche acute senza sopra - slivellamento del tratto st ( nstemi )  . 
the graphs show a significantly higher prevalence of significant disease ( p = 0.02 ) among diabetic ( top graph ) than nondiabetic ( bottom graph ) patients , whereas the prevalence of intact coronary arteries is higher in the nondiabetic population . 
le figure illustrano come la prevalenza di malattia significativa sia significativamente maggiore ( valore di p = 0 , 02 ) nei pazienti diabetici ( in alto ) rispetto ai non diabetici ( in basso ) mentre la prevalenza di coronarie indenni maggiore nella popolazione non diabetica . 
relativamente al gruppo ii , abbiamo registrato un infarto miocardico non - q in un paziente ( 2% ) sintomatico con storia pregressa di rivascolarizzazione e malattia coronarica significativa alla tcms . il numero totale delle rivascolarizzazione miocardiche nel gruppo i stato 26 in 16 pazienti ( 32 , 6% ) , di cui 6 pazienti erano senza storia pregressa di cad e 10 pazienti con storia nota di cad . 
the total number of revascularisation procedures in group 2 was ten in eight patients ( 16.3% ) , three of whom were without a history of cad and five with a known history of cad . 
il numero totale delle rivascolarizzazioni miocardiche nel gruppo ii stato invece 10 in 8 pazienti ( 16 , 3% ) , di cui 3 pazienti erano senza storia pregressa di cad e 5 pazienti con storia nota di cad . 
la sopravvivenza libera da eventi a 25 mesi di follow - up stata del 64 , 1% per il gruppo i e del 83 , 7% per il gruppo ii . 
la sopravvivenza libera da eventi a 25 mesi di followup in presenza di malattia significativa ( stenosi > 50% ) stata del 38 , 8% nei pazienti diabetici ( sopravvivenza media 547 giorni ) e del 57 , 9% nei soggetti non diabetici . 
3a - d kaplan - meier survival curves for diabetic patients ( group 1 , n = 49 ) and nondiabetic patients ( group 2 , n = 49 )  . 
3a - d curve di sopravvivenza ( kaplan - meier ) dei pazienti diabetici ( gruppo i , n = 49 ) e dei pazienti non diabetici ( gruppo ii , n = 49 )  . 
in a il tasso di eventi cardiaci cumulativi significativamente pi alto nella popolazione generale diabetica a confronto con la popolazione non diabetica ( p = 0 , 046 )  . 
in c e d riportato il tasso di eventi cardiaci cumulativi a confronto fra i due sottogruppi rispettivamente senza storia di cad e con pregressa storia di cad . group 1 cad and 78.3% for group 2 cad +  . 
4a - d kaplan - meier survival curves for diabetic patients ( group 1 , n = 49 ) and nondiabetic patients ( group 2 , n = 49 ) according to severity of coronary artery disease on multislice computed tomography . 
4a - d curve di sopravvivenza ( kaplan - meier ) dei pazienti diabetici ( gruppo i , n = 49 ) e dei pazienti non diabetici ( gruppo ii , n = 49 ) in relazione alla malattia coronarica rilevata dalla tcms . 
in entrambi i gruppi la malattia significativa significativamente correlata ad un outcome avverso , considerando il tasso sia di eventi cumulativi ( a e c ) , sia di eventi cardiaci maggiori ( b , d ) , mentre la probabilit di eventi associata alla presenza di coronarie indenni pari a 0% . cardiovascular events compared with the nondiabetic population . 
the negative impact of dm on outcomes is related to the more rapid progression of atherosclerotic disease , the onset of autonomic neuropathy , microangiopathy and , often , diabetic heart disease . 
there is substantial evidence that the risk of cardiovascular events associated with dm is two to four times higher compared la principale causa di morte rappresentando il 52% di tutte le cause [ 14 ]  . 
limpatto prognostico negativo del dm legato allo sviluppo pi precoce e severo della malattia aterosclerotica , allinsorgenza della neuropatia autonomica , della microangiopatia e spesso della cardiomiopatia diabete - correlata . 
esistono ormai evidenze che il rischio di eventi cardiovascolari associato al dm da 2 a 4 volte superiore rispetto alla popolazione non diabetica [ 2 ] e pu essere considerato equivalente a quello dei pazienti non diabetici con storia di infarto miocardico [ 3 ]  . 
5 kaplan - meier survival curves for both diabetic ( group 1 , n = 49 ) and nondiabetic ( group 2 , n = 49 ) patients according to clinical history . 
survival curves show that event - free survival is better for nondiabetic patients without a history of coronary artery disease ( cad ) ( group 2 , cad ) , whereas a worse outcome is correlated with type 2 diabetes melitis and a history of cad ( group 1 , cad + )  . 
5 curve di sopravvivenza cumulativa ( kaplan - meier ) dei pazienti diabetici ( gruppo i , n = 49 ) e dei pazienti non diabetici ( gruppo ii , n = 49 ) in relazione alla storia clinica . 
le curve di sopravvivenza dimostrano come la sopravvivenza libera da eventi sia migliore per i pazienti non diabetici senza storia di cad ( gruppo ii , cad - ) mentre la prognosi peggiore correlata alla presenza del dm nei soggetti con storia di cad ( gruppo i , cad + )  . 
inoltre , i pazienti diabetici senza storia di cad ( gruppo i , cad ) hanno un outcome clinico sovrapponibile ai pazienti non diabetici con cad nota ( gruppo ii , cad + )  . with nondiabetic subjects [ 2 ] and comparable to the risk in nondiabetic patients with a history of myocardial infarction [ 3 ]  . 
hence , the recommendation of the european association for the study of diabetes and the american diabetes association to consider dm as a risk factor equivalent to known cad [ 15 , 16 ]  . the early detection of ischaemic cad and risk stratification in patients with known cad are crucial for optimising the management of diabetic patients . 
the prognostic usefulness of these examinations has been validated by numerous studies and , in general , patients with normal cardiac stress imaging have a yearly rate of cardiac events < 1% . 
in diabetic patients , several confounding factors exist for the interpretation and value of the examination : the high pain threshold due to autonomic neuropathy , the multivessel nature of cad , ecg abnormalities at baseline , a frequently poor exercise capacity , coexistence of peripheral artery disease and the use of combination therdazione da parte delle societ scientifiche americane ed europee per lo studio del diabete di considerare il dm come un fattore di rischio equivalente alla malattia coronarica nota [ 15 , 16 ]  . 
i test diagnostici fino ad oggi usati sono stati lelettrocardiogramma sotto forzo e le metodiche di imaging cardiaco sotto stress farmacologico ( ecografia , scintigrafia miocardica e risonanza magnetica nucleare )  . 
lutilit prognostica di questi esami stata validata in numerosi studi e , in generale , i pazienti con imaging cardiaco sotto stress normale hanno un tasso annuale di eventi cardiaci < 1% . 
la microangiopatia e la multi - distrettualit della malattia aterosclerotica nei pazienti diabetici non sono facilmente valutabili da metodiche di imaging che intrinsecamente identificano anormalit regionali della perfusione o della funzione miocardica contrattile . 
nei pazienti diabetici esistono diversi fattori confondenti per linterpretazione e la validit dellesame : lelevata soglia del dolore per la neuropatia autonomica , la natura multivasale della coronaropatia , le anormalit elettrocardiografiche di base , una frequente ridotta performance allesercizio , la coesistenza di arteriopatia periferica e lutilizzo di una terapia multi - farmaco . 
all these factors contribute to elevate the number of false negative findings on stress cardiac imaging tests in diabetic patients . several studies have confirmed that despite a negative stress test , diabetic patients have a twofold greater likelihood of myocardial infarction or cardiac death compared with nondiabetic patients ( 3%6% depending on the series ) [ 1820 ]  . 
in particular , many series have demonstrated a high negative predictive value ( close to 100% ) compared with coronary angiography , which enables msct to be used as a useful noninvasive diagnostic tool to exclude the presence of cad [ 411 ]  . 
 [ 21 ] recently demonstrated that msct is able to provide independent prognostic information over clinical risk factors . the authors studied 100 symptomatic patients with known ( 35% ) or suspected ( 65% ) cad and found , as we did , that the presence of intact coronary arteries was associated with a 0% incidence of cardiac events at 12 months , whereas patients with cad had a higher risk of cumulative cardiac events ( 63% for significant disease , 8% for nonsignificant disease )  . in our study as well , the presence of intact coronary arteries was associated with excellent prognosis in both diabetic and nondiabetic patients ( event rate 0% )  . 
as a result , the absence of cad on msct has a strong negative predictive value for short - term cardiac events , even in patients at high cardiovascular risk such as those with dm . 
an interesting finding of our study was that the prevalence of significant disease was higher in group 1 subjects , especially in the subgroup without a history of cad ( p = 0.02 ) , where it affected also 33% of asymptomatic patients . 
it is has been reported that two asymptomatic diabetic patients out of five have an abnormal stress test suggesting silent myocardial ischaemia [ 22 ] and that 65% of them have significant cad ( 50% stenosis ) documented by coronary angiography [ 23 ]  . 
furthermore , in a large autoptic study of diabetic patients without ante mortem evidence of cad , the prevalence of high - grade cad was approximately 50% among subjects < 65 years and 75% for those < 65 years [ 24 ]  . 
 in numerosi studi , stato infatti confermato come , in presenza di un esame di imaging sotto stress negativo , i pazienti diabetici abbiano una probabilit superiore a 2 volte di infarto miocardico o morte cardiaca rispetto ai non diabetici ( dal 3% al 6% a seconda delle casistiche ) [ 1820 ]  . 
in particolare , in numerose serie stato dimostrato lelevato valore predittivo negativo ( prossimo al 100% ) a confronto con la coronarografia che consente di utilizzare la tcms come utile strumento diagnostico non invasivo per escludere la presenza di coronaropatia [ 411 ]  . 
gli autori hanno studiato 100 pazienti sintomatici con nota ( 35% ) o sospetta ( 65% ) cad , e come nel nostro studio , hanno riscontrato che la presenza di coronarie indenni associata ad unincidenza di eventi cardiaci a 12 mesi dello 0% , mentre i pazienti con lesioni coronariche hanno associato il rischio pi elevato di eventi cardiaci cumulativi ( 63% per la malattia significativa , 8% per la malattia non significativa )  . anche nel nostro studio la presenza di coronarie indenni associata ad una prognosi eccellente , in entrambi i gruppi di pazienti diabetici e non diabetici ( tasso di eventi 0% )  . di conseguenza lassenza di malattia coronarica documentabile alla tcms ha un forte valore predittivo negativo di eventi cardiaci nel breve termine , anche nei pazienti con elevato rischio cardiovascolare come nel dm . 
un dato del nostro lavoro che la prevalenza di malattia significativa maggiore nel gruppo i , soprattutto nel sottogruppo senza storia di cad pregressa ( p = 0 , 02 ) dove presente anche nel 33% dei pazienti asintomatici . 
 noto dalla letteratura che 2 pazienti diabetici asintomatici su 5 hanno uno stress test anormale indicativo di ischemia miocardica silente [ 22 ] e di questi il 65% ha una coronaropatia significativa ( stenosi 50% ) documentata allangiografia coronarica [ 23 ]  . 
inoltre , in un ampio studio autoptico in pazienti diabetici senza evidenza ante - mortem di cad , la prevalenza di coronaropatia di alto grado stata approssimativamente del 50% al di sotto dei 65 anni e del 75% per quelli < 65 anni [ 24 ]  . 
volume - rendered ( vr ) and curved multiplanar reconstructions ( mprs ) of the left main coronary artery ( a - d ) show the presence of three diagonal branches and one marginal branch . 
le immagini della coronaria sinistra ( a - d ) in volume rendering e mediante ricostruzioni multiplanari curvate mostrano la presenza di 3 rami diagonali e di un ramo marginale . 
ao , aorta ascendente ; cdx , coronaria destra ; cx , coronaria circonflessa ; iva , coronaria interventricolare o discendente anteriore ; d2 e d3 , rami diagonali ; ivp , coronaria interventricolare posteriore ; pl , ramo postero - laterale ; vd , ventricolo destro ; vs , ventricolo sinistro . radiol med ( 2008 ) 113 : 627643 fig . 
7a - c a 45 - year - old nondiabetic man with negative stress test ( exercise electrocardiogram ) and significant coronary artery disease ( > 50% stenosis ) on multislice computed tomography . 
the same curved mpr image ( c ) shows the presence of an atheromatous segment ( arrow ) without significant narrowing , which can also be seen on volume - rendered image between the middle and distal segment of the right coronary artery . 
analogamente limmagine multiplanare curvata ( b ) premette di valutare la presenza della stenosi ( testa di freccia ) con le caratteristiche della placca che appare eccentrica e prevalentemente non calcifica . 
nella stessa immagine multiplanare curvata ( c ) si osserva la presenza di un tratto ateromasico ( freccia ) senza significativa riduzione di calibro che appare evidente anche sullimmagine volume rendering al passaggio tra segmento medio e distale della cdx . 
ao , aorta ascendente ; cdx , coronaria destra ; ivp , coronaria interventricolare posteriore ; pl , ramo postero - laterale ; vd , ventricolo destro . pared with nondiabetic patients ( p = 0.0017 ) ; this could indicate greater instability and progression of atherosclerotic disease . 
in particular , giri et al . , in their large multicentric study , demonstrated that the outcome of diabetic patients with normal myocardial perfusion imaging was initially identical to that of nondiabetic patients but worsened dramatically after 2 years [ 25 ]  . 
similar results have been reported by cortigiani et al . , who studied a large number of patients with known or suspected cad using pharmacological stress echocardiography [ 26 ]  . 
during a mean follow - up of 31 months , the incidence of cardiac stati sottoposti ad un numero totale di rivascolarizzazioni significativamente pi alto rispetto ai non diabetici ( p = 0 , 0017 ) ; questo potrebbe indicare una maggior instabilit e progressione della malattia aterosclerotica . 
in particolare , giri et al . , nel loro ampio studio multi - centrico , hanno dimostrato come la prognosi nei pazienti diabetici con normale scintigrafia sotto stress sia inizialmente paragonabile a quella dei pazienti non diabetici , con drammatico peggioramento dopo i 2 anni [ 25 ]  . 
inoltre , in presenza di un esame scintigrafico positivo , i pazienti diabetici rispetto ai non diabetici hanno un maggior rischio di eventi cardiaci per ogni grado di anormalit di perfusione dimostrata . risultati simili sono stati riportati dal gruppo di cortigiani che ha studiato un ampio numero di pazienti con nota o sospetta cad tramite ecografia sotto stress farmacologico 642 radiol med ( 2008 ) 113 : 627643 events was significantly higher among diabetic subjects without a history of cad than among nondiabetic patients with known cad . 
al follow - up medio di 31 mesi , lincidenza di eventi cardiaci risultata significativamente pi alta nei soggetti diabetici senza storia di cad rispetto ai pazienti non diabetici con nota cad . 
 [ 27 ] hanno dimostrato un tasso estremamente basso di mortalit da tutte le cause nei soggetti diabetici asintomatici senza calcio coronarico ( circa l1% a 5 anni )  . 
tuttavia , il ruolo dellebct rimane controverso in quanto uno studio successivo non riuscito a dimostrarne il beneficio prognostico nei pazienti diabetici [ 28 ]  . conclusions conclusioni in conclusion , together with good diagnostic accuracy , msct can provide additional prognostic value . 
our results in the midterm follow - up agree with those of previous epidemiological and prognostic studies , according to which dm is associated with significantly worse outcomes relative to the general population . 
our midterm results demonstrate that msct has 100% negative predictive value in subjects with intact coronary arteries and enables risk stratification in patients with cad , given that the rate of cardiac events is significantly correlated with the presence of significant disease . concludendo , la tcms , insieme allaccuratezza diagnostica , pu offrire un valore prognostico aggiunto . 
i nostri risultati , nel follow - up a medio termine , sono concordi a quelli di precedenti studi epidemiologici e prognostici secondo cui il dm associato ad un outcome significativamente peggiore rispetto alla popolazione normale di controllo . 
diagnostica per immagini 2dipartimento di patologia testa e collo , seconda universit degli studi di napoli , piazza miraglia 2 , 80127 napoli , italy 3universit del molise , dip . 
cappabianca , via amendola 8 , 81055 santa maria capua vetere , caserta , italy , tel . : + 39 - 081 - 5665201 , fax : + 39 - 081 - 5665201 , e - mail : salvatore.cappabianca@unina2.it received : 20 june 2007 / accepted : 16 july 2007 / published online : 14 april 2008 springer - verlag 2008 abstract purpose . 
on ct images , lipomas and fibrolipomas appeared as smooth ( 38 / 50 cases ) or lobulated ( 12 / 50 cases ) well - defined masses associated with moderate displacement of surrounding tissues ; tumours had high signal intensity on mr t1 - weighted images , with relative decreasing signal on t2 - weighted images . 
nelle immagini di tomografia computerizzata i lipomi ed i fibrolipomi appaiono come masse ben definite con margini lisci ( 38 / 50 casi ) o lobulati ( 12 / 50 casi ) associate , con modesta dislocazione dei tessuti circostanti ; le lesioni appaiono iperintense nelle immagini di risonanza magnetica ottenute con sequenze t1 - pesate con riduzione proporzionale del segnale nelle immagini t2 - pesate . 
most lipomas , in fact , tend to grow insidiously without any symptoms and cause few problems other than those of a localised mass and cosmetic concerns . superficial lipomas may be diagnosed by clinical history and examination because of their typically soft texture and superficial location , whereas deep lipomas are frequently not explorable on examination , making it difficult to evaluate the relationship between the mass and the surrounding tissues . 
in such cases , the diagnosis should be based on imaging obtained to characterise suspicious soft tissue masses and to evaluate the lesions deep extension and relationship with surrounding tissues . the authors performed a retrospective review of computed tomography ( ct ) an magnetic resonance imaging ( mri ) records of surgically proven soft tissue masses suspected to be lipomatous lesions of the head and neck region . 
the findings in some atypical presentations of lipomatous lesions are also presented . materials and methods the ct and mri examinations of 78 patients ( 43 male , 35 female , aged 1280 years ; mean 47.5 ) surgically treated for lipomatous lesions of the head and neck region between january 1995 and june 2005 were retrospectively reviewed . the anatomical distribution was neck ( 19 ) , buccal and vestibular mucosa ( 10 ) , parotid - masseter region ( 14 ) , submandibular region ( 8 ) , jaws ( 7 ) , floor of the mouth ( 5 ) , lips ( 4 ) , tongue ( 4 ) , frontal bone ( 2 ) and zygomatic bone ( 1 )  . the study also included four cases of multiple fat - containing lesions of the neck and upper trunk ( madelungs disease )  . 
analysis of the surgical specimens revealed the following histological types : lipoma ( 33 ) , fibrolipoma ( 22 ) , infiltrating muscular lipoma ( 6 , two in the tongue ) , angiolipoma ( 2 ) , sialolipoma ( 2 ) , intraosseous fat - containing lesions il lipoma il tumore mesenchimale pi comune ma solo nel 25% circa dei casi tale neoplasia e le sue varianti originano nella regione testa - collo , dove costituiscono lo 0 , 1%5% del totale dei tumori benigni [ 15 ]  . 
la maggior parte dei lipomi , infatti , si accrescono insidiosamente in assenza di sintomi e causano la comparsa di pochi disturbi , principalmente alterazioni estetiche legate alla presenza di una tumefazione localizzata che compromette laspetto del paziente affetto . 
i lipomi a sede superficiale , per la loro caratteristica consistenza soffice e per la localizzazione sottocutanea , possono essere diagnosticati sulla scorta dellanamnesi e dellesame obiettivo ; i lipomi a sede profonda , invece , risultano spesso di difficile accesso allesplorazione clinica per cui difficile dimostrare le relazioni tra la lesione ed i tessuti circostanti . 
in tali casi la diagnosi dovrebbe essere fondata sulla valutazione strumentale , valida ai fini della caratterizzazione delle masse sospette di consistenza soffice e della definizione dellestensione profonda e dei rapporti con i tessuti circostanti . gli autori effettueranno una analisi retrospettiva dei reperti di tomografia computerizzata e di risonanza magnetica di masse che , ritenute lesioni lipomatose del distretto testa - collo , sono state asportate chirurgicamente . 
gli autori descriveranno , inoltre , reperti particolari riscontrati in alcune presentazioni atipiche dei lipomi . materiali e metodi gli esami di tomografia computerizzata e di risonanza magnetica di 78 pazienti ( 43 maschi , 35 femmine , di et compresa tra i 12 e gli 80 anni , con unet media di 47 , 5 anni ) sottoposti ad intervento chirurgico per lasportazione di lesioni lipomatose del distretto testa - collo tra gennaio del 1995 e giugno del 2005 , sono stati analizzati retrospettivamente . 
la distribuzione delle sedi anatomiche di lesione era : collo , 19 ; cavit orale e mucosa vestibolare , 10 ; regione parotido - masseterina , 14 ; regione sottomandibolare , 8 ; ossa mascellari , 7 ; pavimento della bocca , 5 ; labbra , 4 ; lingua , 4 ; 760 radiol med ( 2008 ) 113 : 758770 ( 11 ) , giant infiltrating lipoma ( 1 ) and lipomatous hyperplasia ( 1 )  . all patients underwent both ct and mri scans with a standardised protocol followed by surgical removal of the mass within 30 days . 
ct scans were performed using conventional equipment ( somatom hiq , siemens , erlangen , germany ) both in the axial and coronal planes in 38 cases and using four - slice multidetector equipment ( aquilion , toshiba , tokyo , japan ) , with multiplanar reformatted ( mpr ) images in the sagittal and coronal planes in 40 cases . intravenous iodinated contrast medium was administered in 13 cases . 
in 35 of 50 cases ( 70% ) , the lesion had well - defined margins , and in all cases , there was moderate displacement of the surrounding soft tissues . 
lipomas and fibrolipomas had high signal intensity on t1 - weighted images with proportional reduction in signal intensity in t2 ; as expected , they showed low or absent signal in the fat - suppressed sequences . 
in 19 of 50 cases ( 38% ) , the lesion margins were not clearly defined , and in nine of them , contrast - enhanced t1 - weighted images were acquired ; in two cases ( 6.9 % ) diffuse areas of contrast enhancement at the lesion centre osso frontale , 2 ; osso zigomatico , 1 ; sono stati inclusi nello studio anche 4 pazienti con lesioni contenenti tessuto adiposo localizzate nella regione cervicale e nella porzione superiore del tronco ( malattia di madelung )  . 
i campioni istologici hanno rivelato i seguenti tipi istologici : lipoma , 33 ; fibrolipoma , 22 ; lipoma muscolare infiltrante , 6 ( 2 di tali lesioni interessavano la lingua ) ; angiolipoma , 2 ; sialolipoma , 2 ; lesioni intraossee contenenti tessuto adiposo , 11 ; lipoma gigante infiltrante , 1 ; iperplasia lipomatosa , 1 . in tutti i pazienti sono stati effettuati esami di tomografia computerizzata e di risonanza magnetica seguendo un protocollo standardizzato ; lasportazione delle lesioni identificate stata effettuata entro massimo 30 giorni dallesecuzione degli esami strumentali . 
gli esami di tomografia computerizzata sono stati effettuati in 38 casi utilizzando un apparecchio convenzionale ( somatom hiq , siemens , erlangen , germania ) con lacquisizione di scansioni assiali e coronali ed in 40 casi utilizzando un apparecchio multistrato dotato di quattro detettori ( aquilion , toshiba , tokyo , giappone ) con lacquisizione di immagini multiplanari ricostruite nei piani sagittale e coronale . 
lesame di risonanza magnetica stato effettuato utilizzando uno scanner superconduttivo da 1 tesla ( magnetom sp 42 e , siemens , erlangen , germania ) ; sono state acquisite immagini nei piani assiali , coronali e sagittali con lutilizzo di sequenze spin echo t1 - pesate ( tr : 450512 , te : 1017 ms ) ; sono state pure acquisite immagini assiali ottenute con lutilizzo di sequenze spin echo t1 - pesate con tecnica di soppressione per il grasso con un valore di selective chemical shift di 45 hz ( tr : 900 , te : 22 ms ) e immagini assiali ottenute con sequenze spin echo t2 - pesate ( tr : 2000 , te : 13 / 80 ms )  . 
in 11 casi stato somministrato gadolinio ad una dose standard di 0 , 1 mmol / kg ( magnevist , schering , berlino , germania )  . unanalisi delle immagini di tomografia computerizzata e di risonanza magnetica stata effettuata in maniera indipendente da due gruppi di radiologi esperti in patologie del massiccio facciale , cui era stato chiesto di definire i seguenti parametri : definizione dei margini ; valore hounsfield / intensit di segnale ; omogeneit ; presenza di setti intralesionali ; dislocazione od infiltrazione dei tessuti molli circostanti . i reperti iconografici sono stati successivamente confrontati con quelli istologici . risultati confrontando i reperti di tomografia computerizzata e di risonanza magnetica con i reperti istologici , gli autori sono giunti ai seguenti risultati . 
1a scansione assiale dopo somministrazione di mezzo di contrasto : lesione ipodensa nella regione parotido - masseterina di destra ; la lesione , di verosimile natura lipomatosa , appare come una massa ben definita con margini netti e regolari ; evidente una modesta dislocazione dei tessuti circostanti in assenza di infiltrazione . 
b scansione tc assiale dopo somministrazione di mezzo di contrasto : lesione simile alla precedente localizzata nella regione parotidea di destra ; il lipoma appare come una massa lobulata con margini regolari e sottili setti interni composti da tessuto molle ( frecce )  . stravano valori densitometrici compresi tra 64 e 123 unit hounfield , eccetto che a livello dei sottili setti che , composti da tessuto molle , sono stati chiaramente evidenziati in 26 su 29 casi di fibrolipoma ( 89 , 6% )  . 
i lipomi ed i fibrolipomi presentavano un elevato segnale nelle immagini ottenute con sequenze t1 - pesate con riduzione proporzionale del segnale nelle immagini ottenute con sequenze t2 - pesate e presentavano , come nelle aspettative , basso o nullo segnale nelle immagini ottenute con limpiego di sequenze per la soppressione del grasso . 
limmagine di risonanza magnetica dimostra il comportamento espansivo della lesione , mancando del tutto i segni di infiltrazione delle strutture circostanti . 762 radiol med ( 2008 ) 113 : 758770 fig . 
le immagini ottenute con limpiego di sequenze t2 - pesate mostrano un orletto sottile iperintenso che riveste il versante posteriore della lesione ; tale reperto stato interpretato come sottile reazione edematosa perilesionale . 
in one case of a small lipoma of the lip , neither ct nor mri was able to depict the lesion owing the lesions small size and location . six histological records of infiltrating lipoma were reviewed . 
there were no calcifications within the masses or signs of infiltration of contiguous bones and / or surrounding structures , but the margins were poorly defined , and no clear cleavage plane could be identified . nanza magnetica sono state in grado di identificare la lesione , sia per la localizzazione sia per le piccole dimensioni . sono stati esaminati 6 reperti istologici di lipomi infiltranti . 
4 coronal t1 - weighted image acquired after intravenous administration of gadoliniuin the left neck region , magnetic resonance ( mr ) images show an inhomogeneous mass characterised by markedly hyperintense signal and containing scattered and confluent areas of contrast enhancement . 
the lesion was located on the superficial lateral aspect of the parotid gland and appeared as a typical fatty lesion , the upper profile of which was partially indistinguishable from the contiguous glandular parenchyma . 
the lesion is located at the superficial inferolateral aspect of the left parotid gland and appears as a typical fatty lesion whose deep profile is in part indistinguishable from the contiguous glandular parenchyma . 
both the radiologist and maxillofacial surgeon interpreted the lesion as a simple lipoma , but at surgery , it showed a superficial thin capsule and appeared slightly infiltrating with respect to the salivary gland parenchyma . 
la lesione localizzata superficialmente sul versante infero - laterale della parotide di sinistra , appare come una tipica massa costituita da tessuto adiposo il cui margine profondo risulta parzialmente indistinguibile dal parenchima ghiandolare contiguo . 
la valutazione combinata radiologica e maxillo - facciale faceva propendere per un lipoma semplice ma al momento dellintervento chirurgico la lesione ha mostrato una capsula sottile superficiale , con scarsa tendenza infiltrante a carico del parenchima salivare . 
6 immagine assiale di tomografia computerizzata ( a ) di sialolipoma localizzato nel lobo profondo della ghiandola parotide di sinistra ; la lesione appare di ipodensit omogenea e del tutto contenuta allinterno della ghiandola parotide . 
i lipomi insorgono raramente nella regione anteriore del collo , nella fossa infratemporale , allinterno ed intorno alla cavit orale , nella laringe , nellarea tonsillare , in quella parotidea , nellipofaringe , nel nasofaringe , nello spazio retrofaringeo [ 8 , 9 ]  . i tumori benigni di natura lipomatosa sono stati sottoclassificati in relazione alle loro caratteristiche istologiche e al loro pattern di crescita in lipomi classici ( solitari o multipli ) , fibrolipomi , angiolipomi , lipomi infiltranti , lipomi intramuscolari , hibernomi , lipomi pleiomorfici , lipoblastomatosi e lipoblastomatosi diffusa [ 9 ]  . 
queste lesioni , composte da tessuto adiposo maturo che , a differenza di quello normalmente presente nellorganismo , non pu essere utilizzato nei processi metabolici , sono circondate da una sottile capsula fibrosa . 
7a , b lipoma infiltrante gigante : limmagine tc assiale ( a ) e quella rm coronale t1 pesata ( b ) mostrano una massa espansiva che occupa la regione parotido - masseterina ( la parotide compressa e dislocata posteriormente ) , lo spazio infraorbitario e larea sottomandibolare . 
la lesione lipomatosa si estende in profondit verso lo spazio parafaringeo di destra senza un definito piano di clivaggio che la separi dalle strutture muscolari adiacenti . 766 radiol med ( 2008 ) 113 : 758770 fig . 
8 cervicothoracic coronal magnetic resonance ( mr ) ( a ) and computed tomography ( ct ) images ( b ) showing large multiple symmetrical masses involving the neck region and in part the upper trunk and presenting typical density and signal intensity of fat tissue . 
only about diagnosticati sulla scorta dellanamnesi e della palpazione a causa della loro tipica consistenza soffice e della loro localizzazione superficiale , mentre i lipomi profondi risultano spesso non palpabili ; per questo motivo risulta difficile varadiol med ( 2008 ) 113 : 758770 25% occur in head and neck region [ 6 ] , whereas they most commonly arise subcutaneously in the posterior neck region [ 7 ]  . 
lipomas rarely develop in the anterior neck region , infratemporal fossa , in or around the oral cavity , larynx , tonsillar area , parotid area , hypopharynx , nasopharynx or retropharyngeal space [ 8 , 9 ]  . benign lipomatous tumours have been subclassified according to their histological features and growth patterns into classic lipomas ( solitary or multiple ) , fibrolipoma , angiolipoma , infiltrating lipomas , intramuscular lipomas , hibernoma , pleomorphic lipoma , lipoblastomatosis and diffuse lipoblastomatosis [ 9 ]  . 
these lesions are composed of mature fat tissue that , unlike normal body fat , is not available for metabolic transformation , and they are usually surrounded by a thin , fibrous capsule . 
superficial lipomas may be diagnosed by clinical history and palpation because of their typically soft texture and superficial location , whereas deep lipomas are sometimes not palpable , making it difficult to evaluate the relationship between the mass and surrounding tissues . 
in such cases , diagnosis is based on imaging that should be obtained for all suspected lipomatous lesions in order to evaluate extension of the mass [ 10 ]  . intraosseous lipomas are included among the most uncommon ( 0.1% ) of all bone tumours , and their occurrence within skull bones is very rare [ 11 , 12 ]  . 
the occurrence of intraosseous mandibular and frontal lipomas is also extremely rare ( 8 and 13 cases , respectively , reported in the literature ) [ 12 , 14 ]  . 
although adipocytes are distributed throughout the bone marrow of the human skeleton , lipomas have rarely been considered as primary intraosseous tumours [ 15 ] in that they arise from the fatty marrow ( intramedullary lipoma ) , periosteum ( periosteal lipoma ) and soft tissue adjacent to the bone . 
to date , there have been no reported cases of recurrence or malignant transformation of these fatty lesions in mandibular sites , although there are four reports of malignant transformation of intraosseous lipoma in other sites [ 16 ]  . radiological features are determined by lesion stage . stage 1 lesions contain only a small amount of adipocytes and appear well defined , sometimes with cortical expansion , and radiolucent appearance on plain films and ct . 
stage 3 lesions show nearly or totally complete involution with the presence of radiodensity on ct images both centrally and along the lesion border , caused by reactive ossification around the calcified necrotic fat [ 15 ]  . 
we found two cases of intraosseous lipoma of the skull bones , and in one case , the lesion was characterised by lutare la relazione tra la massa neoplastica ed i tessuti circostanti . 
in tali casi la diagnosi fondata sulla valutazione strumentale utile nella definizione dellestensione delle masse di probabile natura lipomatosa [ 10 ]  . le lesioni intraossee rientrano nel numero dei tumori ossei rari ( 0 , 1% di tutti i tumori ossei ) e la loro insorgenza a livello delle ossa craniche assai infrequente [ 11 , 12 ] ; infatti stato documentato solo un numero limitato di lipomi a carico delle ossa mascellari [ 13 ]  . 
allo stesso modo estremamente raro il riscontro di lipomi intraossei a sede frontale e mandibolare ( in letteratura ne sono stati riportati rispettivamente 8 e 13 casi ) [ 12 , 14 ]  . 
sebbene gli adipociti siano presenti allinterno del midollo osseo dello scheletro umano , i lipomi sono stati considerati raramente tumori primitivi dellosso [ 15 ] , originando dal midollo giallo ( lipoma intramidollare ) , dal periostio ( lipoma periostale ) e dai tessuti molli che circondano losso . 
ad oggi non sono stati riportati casi di recidiva o di trasformazione maligna di tali lesioni lipomatose in sede mandibolare ; tuttavia esistono 4 casi di trasformazione sarcomatosa di lesioni intraossee localizzate in altra sede [ 16 ]  . le caratteristiche radiologiche sono determinate dallo stadio della lesione : le lesioni in stadio 1 contengono una scarso numero di adipociti ed appaiono ben definite , talvolta con aspetti di espansione della corticale e quadri di radiotrasparenza in radiografia tradizionale e tomografia computerizzata . 
le lesioni in stadio 2 mostrano aspetti simili ma contengono aree definite di iperdensit in corrispondenza di aree calcifiche di tessuto adiposo ; queste ultime si formano in conseguenza di eventi necrotici . 
nello stadio 3 c una involuzione parziale o totale delle lesioni , con aspetti di iperdensit obiettivabili sia centralmente che ai margini della lesione ; tale reperto attribuibile ai processi di ossificazione reattivi che si sviluppano attorno al grasso necrotico e calcifico [ 15 ]  . 
abbiamo riscontrato due lipomi intraossei delle ossa craniche : in un caso la lesione era caratterizzata dalla presenza di uninterruzione focale della corticale ossea sul versante vestibolare della mandibola . il primo caso di lipoma infiltrante fu descritto da hoffman nel 1941 ma solo regan defin con precisione tale entit nel 1946 . 
tale lesione lipomatosa un tumore benigno raro che in genere insorge a livello degli arti superiori e del tronco in sede sottocutanea [ 17 ] ; non rivestita da una capsula ed coinvolge in maniera estesa i tessuti molli profondi , i muscoli , i nervi e la sinovia [ 18 ]  . 
lalto tasso di recidiva ( registrata in una percentuale superiore al 60% nei casi associati a coinvolgimento del distretto testa - collo ) [ 19 ] pu essere attribuita alla difficolt nellesecuzione di una escissione radicale ; in letteratura non stato riportato nessun caso di trasformazione sarcomatosa a partire da un lipoma infiltrante [ 17 ]  . 
sono state descritte due varianti di li768 radiol med ( 2008 ) 113 : 758770 focal interruption of the cortical bone on the vestibular aspect of the mandible . the first case of infiltrating benign lipoma was reported by hoffman in 1941 , but the entity was defined by regan in 1946 . 
angiolipoma is characterised by prominent vascular components , whereas infiltrating lipoma is composed of mature adipose cells , inconspicuous blood vessels and delicate strands of connective tissue [ 18 , 20 ]  . 
these lesions seem to be larger than ordinary oral lipomas , and they occur in the cheek and tongue in approximately half of reported cases [ 18 , 2129 ]  . in our study , an atypical lipoma of the inferior lip could not be identified on either ct or contrast - enhanced mri because of its small size and location and poor patient cooperation . 
this malignant lesion is included in a group of tumours further subclassified by the world health organization into adipocytic ( lipoma - like ) , sclerosing , and inflammatory subtypes . 
consequently , the recommended management is a wide local excision , with postoperative radiotherapy reserved for selected cases in which resection margins are doubtful or technically difficult to achieve [ 30 , 32 ]  . madelungs disease is a rare condition clinically characterised by the abnormal proliferation of brown adipose tissue in the head , neck and shoulder areas , mainly affecting white men aged 2560 years . 
these patients often have a history of alcohol abuse , but a wide variety of other disorders may be associated with madelungs disease , including dyslipidaemia , diabetes mellitus and glucose intolerance , hyperthyroidism , liver disease , arterial hypertension , tubular acidosis , macrocytic hyperuricaemia , anaemia , polyneuropathy , hiv infection treated with antiretroviral therapy and treatment with protease inhibitors [ 33 , 34 ]  . renal conclusions radiological evaluation of soft - tissue tumours has undergone a dramatic evolution with the advent of ct and mri . both techniques are very useful for detecting lipomatous lepomi infiltranti a sede profonda : il lipoma e langiolipoma . langiolipoma caratterizzato dalla presenza prevalente di strutture vascolari , mentre il lipoma infiltrante composto da cellule adipose mature , da scarsi vasi sanguigni e da esili strie di tessuto connettivo [ 18 , 20 ]  . 
tali lesioni assumono dimensioni maggiori rispetto ai comuni lipomi della cavit orale , insorgono nella guancia e nella lingua in circa la met dei casi riportati in letteratura [ 18 , 2129 ]  . nel nostro studio n con la tomografia computerizzata n con la risonanza magnetica stato possibile identificare un lipoma atipico del labbro inferiore a causa delle sue dimensioni , della sua localizzazione e della scarsa collaborazione del paziente . 
queste lesioni sono caratterizzate da un serio rischio di recidiva locale ( avviene nel 30% dei casi circa ) ma non risultano mai associate allinsorgenza di metastasi ; di conseguenza la gestione pi corretta di tali masse consiste in unampia escissione locale , con radioterapia post - operatoria riservata ai casi selezionati in cui i margini di resezione risultano dubbi o di difficile acquisizione tecnica [ 30 , 32 ]  . la malattia di madelung una patologia rara , caratterizzata dal punto di vista clinico dalla presenza di unabnorme proliferazione di tessuto adiposo bruno a livello cranico , cervicale e nella porzione superiore del tronco ; interessa principalmente maschi di razza caucasica di et compresa tra i 25 ed i 60 anni . 
tali pazienti spesso riferiscono una storia di abuso alcolico ma unampia gamma di disturbi pu riscontrarsi in associazione con la malattia di madelung , ad esempio dislipidemia , diabete mellito ed intolleranza al glucosio , ipertiroidismo , epatopatia , ipertensione arteriosa , iperuricemia , acidosi tubulare renale , anemia macrocitica , polineuropatia , infezione da hiv trattata con terapia antiretrovirale , trattamento con inibitori delle proteasi [ 33 , 34 ]  . conclusioni la valutazione strumentale dei tumori dei tessuti molli ha subito una notevole evoluzione con lavvento delle tecniche di tomografia computerizzata e risonanza magnetica . 
sebbene entrambe le tecniche siano utili nella identificazione delle lesioni lipomatose , la risonanza magnetica fornisce una migliore definizione del tumore per la sua maggiore risoluzione di contrasto nello studio dei tessuti molli e per la capacit di definire chiaramente la sede e lestensione profonda della massa . 
la capacit multiplanare , inoltre , consente di dimostrare chiaramente il piano di clivaggio esistente tra il lipoma e le strutture muscolari e nervose ; ci di estrema importanza nel caso delle lesioni localizzate nella regione oro - facciale : a tale livello , infatti , essendo taradiol med ( 2008 ) 113 : 758770 sions , although mri with its superior soft - tissue contrast resolution provides a better tumour delineation as well as a clear definition of the location and longitudinal extension of the mass . 
multiplanar capability , moreover , clearly demonstrates cleavage planes between the lipoma , muscle and vessels , which is particularly important in the orofacial region where the margins of lipomas are commonly ill - defined , being often surrounded by normal fat tissue and having a very thin capsule . if most lipomatous lesions do not present any particular diagnostic problems , a group of fatty tumours , such as infiltrating lipoma , pleomorphic lipoma , spindle - cell lipoma and lipoblastoma , may cause considerable diagnostic difficulties and may be mistaken for liposarcoma . 
however , appearance of lesion margins , homogeneity of mr signal intensity and ct density , size , peritumoral signal intensity and relationships with adjacent structures , though not always detectable , are reliable features for differentiating benign from malignant masses and especially from well - differentiated liposarcomas . 
these tumours contain a large amount of fat , usually more than 75% of their volume , and resemble lipomas on both ct and mr images but present internal septa that may be larger and more nodular than those seen in lipomas . 
intravenous administration of gadolinium better depicts the tumour margins and can visualise irregular vascularisation when sarcomatous degeneration is considered , but pathological examination may be required to establish the final diagnosis . the authors underline the fundamental role of mri in studying lipomatous lesion extension and particularly in characterising uncommon lipomatous lesions of the head and neck . 
we suggest a more extensive use of mri in deciding upon the most appropriate surgical approach especially in the case of larger lesions and infiltrating lipomas . li lesioni spesso delimitate da una capsula assai esile e circondate da tessuto grasso normale , i margini dei lipomi sono scarsamente definiti . se la maggior parte delle lesioni lipomatose non presentano particolari difficolt diagnostiche , un gruppo di tumori costituiti da tessuto adiposo come il lipoma infiltrante , il lipoma pleiomorfico , il lipoma a cellule fusiformi ed il lipoblastoma possono causare notevoli difficolt diagnostiche e possono essere confuse con il liposarcoma ; comunque laspetto dei margini lesionali , lomegeneit dellintensit di segnale nelle immagini di risonanza magnetica e di densit nelle immagini di tomografia computerizzata , lintensit di segnale registrata in sede peritumorale e la relazione con le strutture adiacenti sono aspetti che , seppure non sempre riscontrabili , risultano utili nella distinzione tra le lesioni benigne da quelle maligne , specialmente dai liposarcomi scarsamente differenziati . 
questi tumori , contenenti una grossa quantit di grasso , in genere pi del 75% del loro volume , ricordano i lipomi sia nelle immagini di tomografia computerizzata che in quelle di risonanza magnetica , ma presentano setti interni che possono essere pi ampi e nodulari di quelli riscontrati nei lipomi . 
sacral bone remodelling with abnormal dilatation of intervertebral foramina is usually associated with tarlov cysts but can be caused by slow - growth lesions , which also may present cerebrospinal - fluid ( csf ) - like signal or density . 
we describe three patients with a similar history of lower back pain presenting csf - like density / signal lesions with extensive sacral bone remodelling who were affected by a tarlov cyst , an epidermoid cyst and a giant neurofibroma , respectively . 
la dilatazione , talora abnorme , dei forami di coniugazione con rimodellamento del sacro solitamente attribuita alla presenza di cisti di tarlov , ma pu essere riscontrata in formazioni espansive a crescita lenta , che sia in tc che in rm possono presentare caratteristiche di segnale simil - liquorali . 
mediante scanner a 1 , 0 t sono state effettuate sequenze sagittali ed assiali t2 e t1 pree postcontrasto ; sono state inoltre utilizzate sequenze sagittali ed assiali eco - planari pesate in diffusione con relative mappe adc . 
dwi e valori adc sembrano in grado di differenziare chiaramente le cisti di tarlov dalle lesioni espansive a crescita lenta . keywords csf - like lesions dwi giant sacral neurofibrom spinal epidermoid cyst tarlov cyst parole chiave lesioni csf - like dwi neurofibroma gigante del sacro cisti epidermide spinale cisti di tarlov 740 introduction sacral bone remodelling with abnormal dilatation of the intervertebral foramina is often seen on magnetic resonance imaging ( mri ) and computed tomography ( ct ) scans of the lumbosacral region [ 1 ] and is usually associated with the presence of enlarged radicular pockets ( tarlov cysts ) [ 2 , 3 ]  . this diagnosis is confirmed by densitometric values or signal intensity compatible with cerebrospinal fluid ( csf ) within the perineural cysts and usually does not require further investigation . 
a preoperative distinction is important when dealing with these forms insofar as neoplastic lesions are generally treated by surgical resection whereas tarlov cysts are treated conservatively . in recent years , diffusion - weighted imaging ( dwi ) has been developed , allowing facilitated differentiation of epidermoid cysts from arachnoid cysts [ 7 , 8 ]  . 
we present three cases that demonstrate the capability of dwi to contribute to the differential diagnosis of different cystic lesions underlying extensive bone remodelling of the sacral bone . materials and methods mri studies were performed with 1.0 - t magnet ( marconi picker polaris )  . 
all axial and sagittal images had identical thickness , gap ( 4 and 0.5 mm , respectively ) and position . case 1 radiol med ( 2008 ) 113 : 739746 introduzione la dilatazione , talora abnorme , dei forami di coniugazione con rimodellamento del sacro un riscontro frequente in esami rm e tc del tratto lombosacrale [ 1 ] , solitamente associato alla presenza di tasche radicolari ingrandite ( cisti di tarlov ) [ 2 , 3 ]  . 
 da alcuni anni sono state sviluppate le sequenze pesate in diffusione ( dwi ) in grado di differenziare con facilit , per esempio , la cisti epidermoide dalle cisti aracnoidali [ 7 , 8 ]  . 
tali sequenze hanno avuto ampio impiego in ambito cerebrale mentre hanno avuto scarso utilizzo in ambito spinale , soprattutto per la presenza di marcati artefatti da suscettivit magnetica , indotti dalle strutture ossee , che degradano la qualit delle immagini . 
presentiamo alcuni casi che evidenziano come le sequenze pesate in diffusione possano in realt contribuire significativamente a differenziare la natura delle diverse lesioni che si presentano con esteso rimodellamento del sacro e con densit / segnale simil - liquorale , permettendo una corretta pianificazione terapeutica . materiali e metodi gli esami sono stati effettuati mediante uno scanner marconi picker medical system 1 , 0 t polaris con sequenze se t1 prima e dopo la somministrazione di mezzo di contrasto ( 450 / 12 / 3 [ tr / te / nex ] ) e fse t2 ( 4500 / 120 / 3 / 16 , etl 4 ) secondo sezioni assiali e sagittali . 
inoltre sono state utilizzate sequenze assiali e sagittali echo - planari single - shot pesate in diffusione ( 6597 / 113 , 4 ; b - value di 800 s / mm2 , matrice 128128 ) con spessore ( 4 mm ) , gap ( 0 , 5 mm ) e posizionamento delle sezioni identico a quello utilizzato nelle sequenze convenzionali . 
 a 55 - year - old woman with a clinical history of left sciatica and an l5s1 discectomy 19 years earlier was admitted to our unit because of persistent hypoesthesia / hyposthenia in the radicular region of s1 . 
sagittal t2 ( c ) and t1 - weighted ( d ) images 19 years later : the lesion maintains the same signal characteristics ( arrowheads ) but has clearly increased in size ; bone remodelling is more evident . 
sagittal diffusion - weighted image ( e ) at the same level using a single - shot spin - echo echo - planar sequence : the lesion is barely visible ( open arrows )  . 
immagini sagittali t2 ( a ) e t1 ( b ) , eseguite prima dellintervento di discectomia l5 - s1 , mostrano una piccola cisti di tarlov ( frecce ) ; la lesione appare caratteristicamente ipointensa in t1 ed iperintensa in t2 . 
the lesions were therefore judged as wide radicular pockets ( tarlov cysts ) , and the patient was treated with physical therapy . case 2 a 25 - year - old woman with a history of meningitis at the age of 6 years had been suffering from increasingly severe low back pain for a few months . 
a hip mri showed a wide cystic lesion of the sacrum , with bone remodelling of the vertebral canal and marked dilatation of the intervertebral foramina , which was interpreted as a tarlov cyst . 
 caso 2 una donna di 25 anni con una storia di meningite allet di 6 anni presentava , da alcuni mesi , lombalgia ingravescente . la rm del bacino mostrava unampia lesione cistica sacrale con rimodellamento dello speco vertebrale al passaggio lombosacrale e marcata dilatazione dei relativi forami di coniugazione , interpretata come cisti di tarlov . 
sagittal t2 ( a ) and t1 - weighted ( b ) images revealing a cerebrospinal - fluid - like lesion ( white arrows ) with extensive bone remodelling at the lumbosacral passage . 
densitometric values were consistent with csf , and the lesion was interpreted as large tarlov cysts . sphincter incontinence and numbness over a 4 - day period led the patient to undergo a lumbosacral mri . 
a 2 anni dallintervento chirurgico , ad un controllo rm lombosacrale si rilevata una nuova formazione di aspetto cistico simil - liquorale nelle sequenze standard ed iperintensa in diffusione , interpretata come recidiva di cisti epidermoide . caso 3 una donna di 61 anni lamentava da circa 1 mese lombosciatalgia destra resistente ai farmaci . 
dato il peggiorare della sintomatologia dolorosa la paziente era stata sottoposta a tc lombosacrale che rilevava un netto allargamento dei forami di coniugazione al passaggio lombosacrale con rimodellamento del sacro ; i valori densitometrici erano compatibili con quelli del liquor e pertanto il reperto era stato interpretato come ampie cisti di tarlov . 
tale esame confermava il rimodellamento della porzione superiore del sacro e la presenza di una formazione simil - cistica con segnale ipointenso in t1 ed iperintenso radiol med ( 2008 ) 113 : 739746 fig . 
on sagittal t2 ( a ) and t1 - weighted ( b ) images , the cerebrospinal - fluid ( csf ) - like lesion ( white arrows ) remodels the upper sacrum and displaces the peridural fat and the exiting spinal roots . 
axial magnetic resonance images at the s1 level : t2 ( c ) , t1 - weighted postcontrast medium administration ( d ) , diffusion - weighted image ( dwi ) ( e ) and apparent diffusion coefficient ( adc ) maps ( f )  . 
on dwi the multilobulated mass is isohypointense , whereas the adc map shows reduced adc values in comparison with csf ( 1 , 3001 , 500 s / mm2 instead of typical csf values 2 , 5003 , 500 s / mm2 )  . 
nelle immagini t2 sagittali ( a ) e t1 ( b ) la lesione simil - liquorale ( frecce bianche ) rimodella la porzione superiore del sacro e disloca il tessuto adiposo peridurale e le contigue radici spinali . 
la lesione appare iperintesa in t2 ed ipointensa in t1 ( non mostrato ) ; nelle immagini pesate in diffusione la massa multilobulata iso - ipointensa , mentre le mappe adc mostrano valori adc ridotti rispetto al liquor ( 13001500 s / mm2 vs 25003500 s / mm2 )  . 
the patient was operated on and histology was consistent with a giant neurofibroma of the sacru discussion the ct and mri finding of lumbosacral csf - like cysts , in which remodelling of the intervertebral foramina and the sacrum was present , generally recalls an initial diagnosis of perineural cysts . 
however , at the lumbosacral level , other expansile slow - growth lesions can lead to a similar bone remodelling [ 46 ] and seem analogous in ct scans and conventional mri sequences ( t1and t2 - weighted images ) to be examples of giant sacral neurofibroma and epidermoid cysts [ 2 , 6 , 914 ]  . 
spinal neurofibromas often show , on the other hand , a hazy but delayed enhancement [ 6 , 9 ] , which cannot be easily identified on early contrast - enhanced images . 
sulla base dei reperti in dwi e dei valori adc stata sospettata la presenza di una lesione solida tumorale e lesame stato completato con la somministrazione del mezzo di contrasto . 
la paziente stata sottoposta ad intervento chirurgico confermando la presenza di una formazione neoplastica solida risultata poi essere un neurofibroma gigante del sacro . discussione il riscontro in tc e rm a livello lombosacrale di cisti a contenuto simil - liquorale , rimodellanti i forami di coniugazione e il sacro , evoca in prima ipotesi la diagnosi di cisti perineurali . 
a tale livello per altre lesioni espansive a lenta crescita possono causare un simile rimodellamento osseo [ 46 ] e possono presentare caratteristiche analoghe in tc e nelle sequenze convenzionali di rm ( t1 e t2 ) , tra le quali il neurofibroma gigante del sacro e le cisti epidermoidi [ 2 , 6 , 914 ]  . 
sono riportati in letteratura casi di tenue impregnazione limitatamente al tessu744 radiol med ( 2008 ) 113 : 739746 spinal fluid signal by making it hypointense , has been widely used at an intracranial level [ 15 ]  . 
this imaging sequence cannot completely suppress the internal signal of either epidermoid cysts or neurofibromas , and for this reason , they appear patchy and clearly distinguishable from the surrounding csf . 
it is thought that this type of growth is due to the ball - valve mechanism , which allows spinal fluid to enter but only to partially leave [ 3 ]  . 
epidermoid cysts , on the other hand , due to reasons not yet clarified , remain isointense in adc maps but markedly hyperintense in dwi ( table 1 )  . 
due to their distinguishing behaviour in dwi , these sequences have an important role in the diagnosis of intracranial epidermoid cysts [ 7 , 8 ] and in their differentiation with arachnoid cysts . 
also , in the spinal region , dwi and adc imaging , despite susceptibility artefacts due to magnetic field inhomogeneity , show a marked hyperintensity of the epidermoid cysts with respect to surrounding structures . 
i neurofibromi spinali presentano invece spesso uno sfumato ma tardivo enhancement [ 6 , 9 ] , che pu non essere evidenziato se le sequenze dopo somministrazione di mezzo di contrasto vengono effettuate precocemente . 
infine , anche il criterio diagnostico basato sulla crescita delle lesioni espansive rispetto alle cisti di tarlov non risolutivo : le cisti perineurali possono infatti aumentare lentamente di volume nel tempo . 
nel caso 1 , la rm lombosacrale eseguita dalla nostra paziente 19 anni prima testimonia lavvenuta crescita delle cisti sacrali perineurali con conseguente rimodellamento osseo del sacro ed allargamento dei forami di coniugazione . 
lutilizzo recente delle sequenze dwi e delle mappe adc in cui lintensit del segnale dipende dal grado di mobilit dellacqua nei tessuti , permette di differenziare lacqua libera ( per esempio liquor ) dallacqua tissutale o intracellulare . 
in particolare , le cisti di tarlov , per il loro contenuto liquorale , appaiono iperintense nelle mappe adc ed ipointense in dwi ; le lesioni neoplastiche , per la loro natura solida che determina restrizione della diffusione delle molecole dacqua , appaiono isointense sia nelle mappe adc che nelle immagini dwi ; le cisti epidermoidi invece , per motivi non ancora del tutto chiariti , si mantengono isointense nelle mappe adc ma appaiono marcatamente iperintense in dwi ( tabella 2 )  . 
per questo loro particolare comportamento le sequenze pesate in diffusione hanno trovato largo impiego nella diagnosi delle cisti epidermoidi in ambito intracranico [ 7 , 8 ] e nella loro differenziazione con le cisti aracnoidali . 
anche a livello spinale le immagini dwi e adc , seppur inficiate da artefatti da suscettivit magnetica , evidenziano una marcata iperintensit delle cisti epidermoidi rispetto alle strutture circostanti tale che , con laiuto delle immagini anatomiche delle sequenze convenzionali , la diagnosi risulta comunque agevole [ 14 , 1720 ed esperienza personale ]  . 
 il rilievo dei valori adc non sembra presentare particolari difficolt dato che le misurazioni sono effettuate su leradiol med ( 2008 ) 113 : 739746 table 1 signal magnetic resonance imaging pattern of lesions causing sacrum remodelling on conventional imaging ( t1and t2 - weighted ) , diffusionweighted imaging and apparent diffusion coefficient maps lesion type t1 + gd adc maps adc values tarlov cyst hypointense hyperintense absent hypointense hyperintense epidermoid cyst hypointense hyperintense hyperintense isointense neurofibroma hypointense hyperintense isointense isointense absent / soft and peripheral scant or tardy 2 , 5003 , 500 spinal fluid 6001 , 000 parenchyma 1 , 0001 , 500 parenchyma t1 + gd , postcontrast t1 - weighted images ; dwi , diffusion weighted imaging ; adc , apparent diffusion coefficient tabella 1 caratteristiche di segnale rm delle lesioni che causano rimodellamento del sacro nelle sequenze convenzionali ( pesate in t1 e t2 ) , pesate in diffusione e nelle mappe dei coefficienti di diffusione apparente tipo di lesione t1 + gd mappe adc valori adc cisti di tarlov ipointensa iperintensa assente ipointensa iperintensa cisti epidermoide ipointensa iperintensa iperintensa isointensa neurofibroma ipointenso iperintenso isointenso isointenso assente / scarso e periferico scarso e tardivo 25003500 liquido cerebrospinale 6001000 parenchima 10001500 parenchima t1 + gd , sequenze pesate in t1 dopo somministrazione del mezzo di contrasto ; dwi , diffusion weighted imaging ; adc , apparent diffusion coefficient they are carried out on relatively large lesions that are easily recognisable , even in the presence of image distortion . furthermore , lesion dimensions help to reduce problems deriving from partial - volume - related artefacts , thus guaranteeing reliability of the measurement . 
dwi can also be quite useful for postoperative follow - up of epidermoid cysts , which , if not completely removed or dispersed during surgery ( as in our case ) , can be easily identified and differentiated from later postoperative spinal fluid cysts . 
 sioni relativamente grandi , facilmente riconoscibili anche in presenza di distorsione dellimmagine ; inoltre le dimensioni delle lesioni riducono i problemi dovuti ad artefatti da volume parziale garantendo laffidabilit delle misurazioni effettuate . 
kardamakis types of bone metastases in women with breast cancer undergoing systemic treatments university of patras medical school , department of radiation oncology , patras , greece correspondence to : d . 
kardamakis , university of patras medical school , department of radiotherapy , 26500 patras , greece , tel . : + 30 - 261 - 0999540 , fax : + 30 - 261 - 0994475 , e - mail : kardim@med.upatras.gr springer - verlag 2008 published online : 17 july 2008 dear editor , we read with great interest the article published in your journal by quattrocchi et al . 
the higher prevalence of osteoblastic lesions in the years 20012005 was attributed to the use of zoledronic acid treatment [ 1 ]  . we recently published two studies in which ct was used to group patients according to type of bone metastases ( recruitment period 20032006 ) [ 2 , 3 ]  . 
this is also suggested by other literature data , as bonadonna et al . found received that breast cancer patients who chemotherapy had mostly mixed or sclerotic bone metastases , which were asymptomatic in 66% of cases [ 4 ]  . 
in contrast , 66% of breast cancer patients with metastatic bone disease who had not received chemotherapy had lytic lesions , and 70% were symptomatic [ 5 ]  . another important aspect that should be noted is that the above results show that the level of bone resorption at metastatic bone sites correlates with patient morbidity levels , something that was also revealed in the study investigating the correlation between types of bone metastases and patients clinical status [ 2 ]  . 
we agree with the authors that further studies are required to assess the impact of systemic treatment on the radiologic appearance of bone metastases . yours sincerely , vassilios vassiliou and dimitrios kardamakis . radiol med ( 2008 ) 113 : 771773 3 . 
bonadonna g , rossi a , valagussa p et giannopoulou e et al ( 2007 ) a novel study investigating the therapeutic outcome of patients with lytic , mixed and sclerotic bone metastases treated with combined radiotherapy and ibandronate . 
sforza 35 , 20122 milano , italy 2professore ordinario di egittologia , universit degli studi di milano , via festa del perdono 7 , 20122 milano , italy correspondence to : p . 
the first radiological study of an egyptian mummy was performed by flinders petrie shortly after the discovery of x - rays in 1895 , and since then , radiology has never stopped investigating these special patients . 
by the end of the 1970s , computed tomography ( ct ) scanning permitted more in - depth studies to be carried out without requiring the mummies to be removed from their cartonnage . 
ct images can be used to obtain a three - dimensional reconstruction of the mummy that provides important new information , in part thanks to the virtual endoscopy technique known as fly through . 
moreover , starting from ct data and using sophisticated graphics software , one can reconstruct an image of the face of the mummified individual at the time of his or her death . 
the history of imaging , from its origins until now , from the simplest to the most sophisticated technique , allows us to appreciate why these studies have been , and still are , fundamental in the study of egyptian mummies . riassunto pochi secoli dopo la definitiva abolizione della pratica della mummificazione , avvenuta nel vii secolo dc , le mummie cominciarono a colpire limmaginario collettivo esercitando un fascino misterioso che continua fino ai nostri giorni . 
lo studio radiografico delle mummie anticoegiziane ha , fin dal suo inizio , permesso di raccogliere informazioni importanti non solo dal punto di vista medico ma anche dal punto di vista antropologico e archeologico . poco dopo la scoperta dei raggi x del 1895 , flinders petrie ottenne la prima immagine radiografica di una mummia egizia . 
alla fine degli anni 70 , lesame tac ha permesso di approfondire lo studio , consentendo di lasciare la mummia nel suo sarcofago . dalle immagini tac si pu ottenere la ricostruzione tridimensionale della mummia che permette di fornire altre e importanti informazioni , grazie anche allutilizzo della tecnica di endoscopia virtuale . 
inoltre , sempre partendo dai dati tac e utilizzando sofisticati programmi di grafica elettronica , si pu ottenere la ricostruzione dellimmagine del volto dellindividuo mummificato al momento della sua morte . 
la storia degli studi di imaging , dallinizio a oggi , dai pi semplici ai pi sofisticati , ci permette di capire che essi sono stati e restano fondamentali nello studio delle mummie antico - egiziane . keywords diagnostic imaging mummies egypt parole chiave diagnostica per immagini mummie egitto 616 introduction the first egyptian mummies date back to the early third century b.c. 
between 391 and 392 a.d. , in fact , four theodosian decrees ( that followed the edict of thessaloniki de fide catholica of february 27 , 380 , through which emperor theodosius i declared christianity as the official religion of the roman empire ) indirectly banned the practice of mummification , which went into gradual decline , eventually to be completely abandoned with the arab conquest of egypt in 641 . 
within a few centuries , egyptian mummies started to capture the collective imagination and exert a mysterious fascination that continues to this day , with mummies becoming a fashionable subject in both literature and film - making . in the twelfth century , medicine began to develop an interest in egyptian mummies , as witnessed by the mention of them in treatises by the physician matthaeus platearius of salerno ( 11301160 ) and the arab physician abd el - latif ( 11621231 ) , who highlight the virtues of the bituminous substance found in the abdomen and skull of embalmed corpses . 
this substance was named almma al - quburi ( the mumia of tombs ) by the physician and botanist from malaga , ibn al - baytar ( 11791248 ) to differentiate it from the similar substance of mineral origin [ 3 ]  . on the other hand , the possible healing properties of bitumen , pissasphalt or similar materials momya in persian and mma in arabic were already known in antiquity , as documented by the greek physician dioscorides pedanius ( 4090 a.d. ) and the persian physician ibn sina ( 9801037 ) , better known as avicenna . 
mma , of both the mineral kind found in nature and the kind employed during embalming and thus contained in corpses was especially recommended for use as an unguent to promote the healing of wounds and fractures and coagulation of blood . 
it was also recommended per os as a painkiller , antiemetic and a remedy for poisoning , liver disease , and seizures , as well as in the form of inhalations to treat cough and sore throat . in 1584 the famous french surgeon ambroise par ( 15091590 ) vehemently condemned the use of the substance , describing its many more disadvantages that benefits and commenting ironically on its use ( egyptians were not embalmed to be eaten by christians ) [ 4 ]  . 
mummy powder was still being used against haemorrhage by the arabs of the village of gurna in egypt in the early twentieth century , and in the mid 1970s , it could still be found in some new york drugstores where it was apparently sold for use in magic potions [ 5 ]  . 
 radiol med ( 2008 ) 113 : 615626 introduzione le pi antiche mummie egizie risalgono agli inizi del iii millennio ac , le ultime al v secolo dc [ 1 , 2 ]  . 
tra il 391 e il 392 infatti , con i quattro decreti teodosiani ( che fanno seguito alleditto di tessalonica de fide catholica del 27 febbraio 380 , con il quale limperatore teodosio i proclamava il cristianesimo religione ufficiale dellimpero romano ) , veniva proibita , sia pure indirettamente , la pratica della mummificazione che in tal modo gradualmente declin , per essere poi del tutto abbandonata con la conquista araba dellegitto nel 641 . 
ma gi pochi secoli dopo le mummie cominciarono ad attirare e colpire limmaginario collettivo , esercitando un fascino misterioso che continuato e si accresciuto sino ad oggi , facendo della mummia loggetto di una vera e propria moda tanto nella letteratura quanto nella cinematografia . la medicina inizi a interessarsi delle mummie egizie nel xii secolo , come attestato dalle menzioni che in allora ne fecero nei loro trattati il medico salernitano matthaeus platearius ( 11301160 ) e il medico arabo abd el - latif ( 1162 1231 ) sottolineando le virt della sostanza bituminosa ritrovata nelladdome e nel cranio dei cadaveri imbalsamati ; tale sostanza fu chiamata almma al - quburi ( la mumia delle tombe ) dal medico e botanico malaghegno ibn al - baytar ( 11791248 ) per differenziarla dalla sostanza analoga di origine minerale [ 3 ]  . daltra parte , che il bitume , il pissasfalto o materie simili in persiano momya , quindi in arabo mma avessero poteri curativi era gi noto dallantichit , come ricorda il medico greco dioscoride pedanio ( 4090 dc ) e il medico persiano ibn sina ( 9801037 ) , meglio noto come avicenna . 
lutilizzazione della mma , sia di quella minerale che si trovava direttamente in natura sia di quella usata durante limbalsamazione e conservata quindi allinterno dei cadaveri , era soprattutto raccomandata , sotto forma di unguento , per favorire la guarigione di ferite , il consolidamento di fratture e la coagulazione del sangue , ma era anche consigliata , assunta per os , come antidolorifico , antiemetico , in casi di avvelenamento , per le malattie del fegato , per le crisi epilettiche , e sotto forma di suffumigi per curare tosse e faringodinia . nel 1584 il celebre chirurgo francese ambroise par ( 15091590 ) condann aspramente lutilizzo di questa sostanza descrivendone gli svantaggi di molto maggiori rispetto ai vantaggi e ironizzando sul suo utilizzo ( gli egizi non si sono fatti imbalsamare per essere mangiati dai cristiani ) [ 4 ]  . 
ci nonostante la mma continu a essere utilizzata per almeno altri trecento anni per lo pi sotto forma di unguenti , creme e tinture ; ancora agli inizi del xx secolo la polvere di mummia era utilizzata dagli arabi del radiol med ( 2008 ) 113 : 615626 history of radiological study of egyptian mummies with the discovery of x - rays in the late nineteenth century , the medical community began to regard mummies no longer as a source of health remedies but as objects of investigation in themselves , capable of providing direct testimony of a long - gone world : hence , the importance of mummies for the purposes of scientific , archaeological and historical research . since its beginnings , the radiological study of egyptian mummies produced excellent - quality material , allowing collection of important paleopathological and anthropological information . 
the mummies of egypt , traversed by beams of ionising radiation , travel through time to tell the story not only of their own lives , but also of their epoch . 
they provide both direct evidence of pathophysiological data , and are thus of paleopathological relevance , and a indirect testimony to the culture of their period , and are thus of anthropological and archaeological relevance [ 6 ]  . 
 furthermore , important additional information is provided by the mummification process itself and the radical changes it underwent over time from the natural desiccation of the older mummies by the dry desert sands placed in direct contact with the body , to the sophisticated methods of perfect artificial mummification through the use of desiccating agents such as the mixture of natural sodium carbonate and bicarbonate known as natron and certain resins [ 7 ]  . 
early in the history of ancient egypt , in the pre - dynastic period ( before 3100 b.c. ) , the mummification process was unintentional and produced by natural factors . 
it was not until the beginning of the archaic period ( 3100 b.c. ) that the process became artificial , though very simple : the body was left intact and wrapped in thin strips of linen . 
moreover , starting from the early old kingdom , the increasingly sophisticated process appears to have been an obligation for royal descendants , which then extended to high - ranking officials , and later connected only to the census and finally not even to the census . 
during the persian rule ( circa sixth and fifth centuries b.c. ) , anyone could request to be mummified , and they had a choice of three embalming methods : one more expensive , one simple and inexpensive and one intermediate [ 811 ]  . 
as a result , a careful study of the type of mummification and its variants and of funerary customs indirectly reveal the individuals social status and the culture of the historical period . 
analysis of radiographic images provides information on the individuals gender and villaggio di gurna , in egitto , per combattere le emorragie e , alla met degli anni 70 del secolo scorso , la si poteva trovare in alcuni drugstore di new york , apparentemente destinata a essere utilizzata in pozioni magiche [ 5 ]  . 
 storia dello studio radiografico delle mummie anticoegiziane alla fine del xix secolo , con la scoperta dei raggi x , la medicina cominci a considerare le mummie non pi come matrici di sostanza a scopo terapeutico , ma come oggetti di investigazione per desumerne diretta testimonianza di un mondo scomparso : di qui la loro importanza ai fini della ricerca scientifica , archeologica e storica . 
lo studio radiografico dei corpi mummificati degli antichi egizi ha prodotto , fin dal suo esordio , materiale di eccellente qualit che ha permesso di raccogliere dati paleopatologici e informazioni antropologiche di rilievo . 
le mummie dellantico egitto , attraversate da fasci di radiazioni ionizzanti , hanno a loro volta attraversato il tempo per raccontarci non solo la loro vita ma anche quella della loro epoca : esse sono sia segni diretti di dati fisio - patologici , tali da interessare la paleopatologia , sia testimonianza indiretta della cultura del periodo vissuto , tali da interessare lantropologia e larcheologia [ 6 ]  . 
 inoltre , proprio il procedimento di mummificazione , radicalmente modificatosi nel tempo , passando da un processo naturale di essiccazione delle mummie pi antiche operato , grazie alle eccezionali condizioni climatiche presenti in egitto , dalle aride sabbie del deserto poste a diretto contatto con il corpo ai sofisticati e complessi metodi di perfetta mummificazione artificiale operati dalluomo per mezzo di agenti disidratanti , come ad esempio la miscela di sali naturali a base di carbonato e bicarbonato di sodio detta natron e alcune resine fornisce ulteriori dati molto importanti [ 7 ]  . 
allinizio della storia dellantico egitto , nel periodo predinastico ( prima del 3100 ac ) , il processo di mummificazione infatti , come detto , sostanzialmente casuale poich operato da fattori naturali e a noi giunto fortunosamente . 
 allinizio del periodo arcaico ( 3100 ac ) che il processo diventa artificiale , anche se molto semplice : il corpo infatti , lasciato intatto , viene unicamente avvolto da sottili strisce di lino . 
in epoca tarda prima e tolemaica poi ( 67230 ac ) larte gradualmente decliner per ritornare a essere caratterizzata unicamente dal bendaggio esterno durante il periodo delloccupazione romana ( 30 aciv secolo dc )  . 
inoltre , a partire dallinizio dellantico regno , il processo , come detto , sempre pi raffinato sembra essere stato un obbligo per i discendenti reali , poi allargato a personaggi altolocati , in 618 radiol med ( 2008 ) 113 : 615626 fig . 
the data are clearly closely interrelated [ 12 ]  . the discovery of x - rays by wilhelm conrad roentgen on 8 november 1895 was immediately perceived as a major breakthrough , not only for use on living beings . 
the first application of radiography to the study of egyptian mummies was not , however , the work of a radiologist but of an archaeologist : the earliest publication on the subject , dated 1898 , was by sir william flinders petrie , the father of british egyptology . 
ne consegue che lo studio attento del tipo di mummificazione , delle sue varianti , del costume funerario permette di rilevare indirettamente lo stato sociale dellindividuo e il processo di identificazione culturale del periodo storico , mentre lanalisi radiografica diretta consente di ottenere informazioni circa il sesso e let dellindividuo , il suo stato di salute e di malattia . 
i dati , naturalmente , si compenetrano [ 12 ]  . la scoperta dei raggi x da parte di wilhelm conrad roentgen l8 novembre 1895 , fu percepita immediatamente come una grande svolta non solo per il mondo vivente . 
la prima utilizzazione della tecnica radiografica applicata allo studio delle mummie dellantico egitto non fu per opera di un radiologo ma di un archeologo : la prima pubblicazione in materia , del 1898 , infatti di sir william flinders petrie , il padre della egittologia britannica . 
i raggi sconosciuti furono da lui utilizzati per esaradiol med ( 2008 ) 113 : 615626 minare il contenuto di un sarcofago egizio del museo di storia naturale di vienna e dimostrarne con sorpresa il contenuto non umano . 
poco dopo a parigi , nel 1913 , usando i raggi x per verificare leventuale presenza di gioielli nascosti tra il bendaggio , fu notato un vizio di differenziazione regionale della colonna vertebrale in una mummia della xi dinastia [ 17 ]  . 
lo studio radiografico delle mummie dellantico egitto si diversific subito a seconda del materiale radiografato : mummie comuni e mummie reali ; il primo esteso studio radiografico del 1931 e di tre anni dopo il secondo studio radiologico di una mummia reale [ 18 , 19 ]  . 
conseguenza di ci fu che , inizialmente , la tecnica di esame con metodo tradizionale , pur venendo sempre eseguita sfruttando tutte le proiezioni possibili ( che per non potevano essere molte ) , poteva richiedere , per garantire una maggiore definizione , lutilizzazione di materiale preparato , cio sbendato , anche se solo in parte , e manipolato ; questa preparazione , atta sia a cercare di eliminare eventuali artefatti provocati dalle immagini radiografiche delle bende sia a non tralasciare nulla di nascosto , rischiava tuttavia di danneggiare i resti mortali e causare inopportuni cambi di posizione di alcune strutture ossee [ 20 ]  . 
ci si avvide subito , inoltre , che le differenti tecniche di imbalsamazione utilizzate nei vari periodi davano variazioni considerevoli alla penetrazione dei raggi x fino a condizionare in certi casi la completa mancata visualizzazione di alcuni dettagli ossei ; per contro , gli esami radiografici dimostrarono e fecero conoscere proprio una grande variabilit di trattamento nel processo di mummificazione , sia della testa che del corpo , arricchendo cos le nozioni su questa tecnica [ 21 ]  . trentanni dopo , a seguito di metodici e continui esami radiografici , potevano gi essere documentate ed elencate fig . 
3 x - ray of the mummy of sethi i ( new kingdom ; xix dynasty ) , where a protective amulet ( called horuseye ) is placed on the left humerus . 
3 radiografia della mummia di sethi i ( nuovo regno , xix dinastia ) in cui si nota la presenza di un amuleto ( detto occhio di horus ) posizionato in corrispondenza dellomero di sinistra . 
per gentile concessione : milano , universit degli studi , archivi di egittologia ( fondo edel )  . in 1912 , in a fine description of the royal mummies of the cairo museum , australian physician grafton elliot smith ( chair of anatomy at the cairo school of medicine from 1900 to 1909 ) , who in 1904 x - rayed the mummy of tuthmosis iv after having transported it to a nearby sanatorium on a horse - drawn hackney carriage , stated that examination with the aid of x - rays would , no doubt , have provided much additional information [ 16 ]  . 
a few years later , in paris in 1913 , the use of x - rays to detect the presence of jewels concealed in the wrappings revealed a regional differentiation defect of the spine of a mummy of the xi dynasty [ 17 ]  . 
the first extensive 620 radiol med ( 2008 ) 113 : 615626 radiographic study dates back to 1931 , and the second study of a royal mummy was carried out 3 yeas later [ 18 , 19 ]  . 
 the x - ray source and detector systems used at the time inevitably provided relatively poorly defined images [ 18 ]  . one result was that , initially , although always performed in all possible projections ( which were nonetheless limited ) , the examination could require the use of prepared material , that is , at least partially unwrapped and manipulated , to ensure better definition . 
such preparation to eliminate possible artefacts due to the bandages and make sure nothing remained undisclosed entailed a risk , however , of damaging the mortal remains and causing undesired changes in the position of some of the bony structures [ 20 ]  . 
it was also soon realised that the different embalming techniques used in the various periods produced considerable differences in x - ray penetration , in some cases leading to complete failure to visualise some bony details . 
also , it was established that certain radiographic patterns of the humerus ( for example , the presence of bone - surface rugosity , thinning of the diaphyseal cortical bone , hyperlucent areas in the humeral head ) could be reasonably considered as indicators to establish an approximate age of the embalmed individual at the time of his or her death [ 23 ]  . the radiographic technique was still , however , in its infancy . 
in the late 1960s , for example , with the use of the radioactive isotope ytterbium 169 ( 169yb ) as an x - ray source and film cassettes equipped with an image intensifier , exposure time ranged from 2 s to 5 min , depending on whether the mummy was still in its sarcophagus or protected only by a thin wooden board . 
to obviate the difficulties in transporting the mummy to an x - ray facility , as early as the 1970s , radiographic studies were carried out with portable equipment , which could be used in galleries and museums to obtain , where possible , radiographs of remains appropriately left on site [ 21 ]  . 
4 x - ray of the mummy of amenhotep i ( new kingdom ; xviii dynasty ) showing the anomalous position of the arms ( with fracture and displacement ) , most likely occurred following re - wrapping by priests of the xx dynasty : on the left side , the radius and ulna are well separated from humerus and the hand is placed near the pelvis ; on the right side , the radius and ulna are slightly bent and the hand is fractured . 
4 radiografia della mummia di amenhotep i ( nuovo regno , xviii dinastia ) in cui si nota la posizione anomala delle braccia ( condizionata da frattura e dislocazione ) , verosimilmente occorsa dopo essere stata ribendata dai sacerdoti della xx dinastia : a sinistra radio e ulna appaiono visibilmente separati dallomero e la mano risulta sovrapposta in parte alla pelvi mentre a destra radio e ulna appaiono appena ripiegati e la mano presenta una frattura . 
e allo stesso modo si stabiliva che radiol med ( 2008 ) 113 : 615626 starting from the 1960s , the egyptian mummies of some major museums started to be x - rayed and studied systematically . 
for example , in 1968 , the egyptian government approved the project of a team of researchers from the university of michigan to x - ray all of the mummies preserved in the cairo museum [ 25 ]  . 
this led to the collection and publication , in the 1980s , of the complete studies and important radiographic atlases that mark the fascinating history of the radiological study of the mummies of ancient egypt [ 21 , 2629 ]  . 
 that same period , and precisely 1972 , saw the birth of the multidisciplinary research project of manchester university ( manchester mummy project ) , a project that aimed to systematically study the mummies and within which radiology played a central role [ 32 , 33 ]  . 
this was followed by several other similar , albeit smaller , studies , such as the minnesota mummy project and the national museums of scotland mummy project [ 34 , 35 ]  . however , it was at the end of the 1970s , with the advent of computed axial tomography ( ct ) , that the study of egyptian mummies experienced a true breakthrough . 
the use of this sophisticated tool for radiographic investigation , which images bodies in slices , not only broadened and better defined the field of investigation but also changed the approach to the archaeological find . 
in the 10 years that followed , numerous accurate ct studies were performed on individual mummies or on groups of mummies , as in the case of the study of one of the largest collections of egyptian mummies , which is held by the boston museum of fine arts [ 3741 ]  . 
the process was virtual , and the mummy was left unaltered : powerful x - ray sources combined with complex detector techniques and sophisticated postprocessing software made it possible not to touch the fragile specimen being examined , which could even be left inside its sarcophagus . 
 alcuni aspetti radiografici dellomero ( come , per esempio , la presenza o meno di rugosit della superficie ossea , di assottigliamento della corticale diafisaria , di lacune iperdiafane nel contesto della testa omerale ) potevano essere considerati a ragion veduta indicatori per stabilire approssimativamente let del soggetto mummificato al momento della sua morte [ 23 ]  . la tecnica radiografica era comunque ancora ai suoi esordi . 
alla fine degli anni 60 del secolo scorso , per esempio , con sorgente radiogena fornita dallisotopo radioattivo ytterbium 169 ( 169yb ) e pellicola radiografica contenuta nella cassetta dotata di amplificatore di brillanza , lesposizione variava da due secondi a cinque minuti , a seconda che la mummia fosse ancora nel suo sarcofago o fosse protetta unicamente da una sottile asse di legno . 
i kv impiegati variavano da 70 a 90 , i mas da 4 , 0 a 15 , 0 e la distanza oggetto - pellicola era pari a 60 pollici ( poco pi di un metro e mezzo ) ; poteva essere radiografato tutto il corpo o soltanto la testa ( cos detto cefalogramma )  . 
per ovviare allinconveniente della difficile mobilizzazione della mummia da radiografare si pens e si attu , gi negli anni 70 , lutilizzo di un equipaggiamento radiografico di base portatile , utile per lo studio nelle gallerie e nei musei e tale da permettere , ove possibile , di radiografare reperti lasciati opportunamente in situ [ 21 ]  . 
tale tecnica viene approfondita ancora oggi nei suoi vari componenti [ 24 ]  . dagli anni 60 in poi le mummie antico - egiziane di alcuni importanti musei iniziarono a essere radiografate e studiate sistematicamente . 
per esempio , nel 1968 , il governo egiziano approv il progetto di un gruppo di ricercatori delluniversit del michigan di radiografare tutte le mummie conservate nel museo del cairo [ 25 ]  . 
ci permise alla tecnica radiografica semplice di trovare la sua massima espressione nella compilazione e nella pubblicazione , negli anni 80 , di studi completi e di atlanti radiografici importanti che segnano laffascinante storia dello studio radiografico delle mummie dellantico egitto [ 21 , 2629 ]  . 
 non a caso fu proprio in quel periodo , pi precisamente nel 1972 , che nacque il progetto di studio sistematico interdisciplinare delluniversit di manchester ( manchester mummy project ) , un progetto volto a creare uno studio unitario e allinterno del quale la parte radiologica aveva un ruolo cardine [ 32 , 33 ]  . 
ad esso hanno fatto seguito numerosi studi analoghi , anche se di entit minore , come , ad esempio , quello in minnesota ( minnesota mummy project ) e quello elaborato in scozia ( national museums of scotland mummy project ) [ 34 , 35 ]  . ma con la fine degli anni 70 , e cio con lavvento della tomografia assiale computerizzata , che lo studio delle 622 radiol med ( 2008 ) 113 : 615626 fig . 
in addition , by identifying the chemical components of the substances used for embalming , ct provided curators with valuable information to plan the restoration of the mummy [ 43 , 44 ]  . for a few years now , ct has been able to avail itself of multiple detector rows to capture the image , which is better defined as a result ( mdct ) [ 45 ]  . 
ct is today the only non - destructive method for obtaining fundamental data for the three - dimensional reconstruction of the entire mummy ( both of the face and of the body ) ; the reconstruction is achieved by combining the axial images with the sagittal and coronal ones , the last obtained through reformatting , thanks to an algorithm process known as post - processing . 
the possibility of reconstructing the mummy three - dimensionally , using voxels ( unit of volume with x , y , z , coordinates and corresponding to a pixel in 2d imaging ) allows one to obtain images that can be processed electronically on a dedicated workstation running specific software , and thus images that can be better mummie dellantico egitto ha assunto maggior valore e ha subito una svolta : lutilizzo della sofisticata metodica di indagine radiografica che rappresenta i corpi a fette non solo ha allargato il campo di osservazione , peraltro definendolo maggiormente , ma ha altres modificato lapproccio al reperto archeologico . 
nei dieci anni successivi furono pubblicati numerosi e accurati studi tac effettuati sia su singole mummie sia su gruppi di esse , come ne esempio lo studio di una delle pi grandi collezioni di mummie egizie e cio quella del museum of fine arts di boston [ 3741 ]  . 
questi studi continuano tuttoggi con modalit sempre pi sofisticate [ 42 ]  . i vantaggi della nuova metodica furono subito evidenti . lutilizzo della tac permetteva di non sbendare la mummia , o meglio di sbendarla virtualmente , senza alterarla in nessun modo : le potenti sorgenti radiogene unite alle complesse tecniche di rilevazione e alle sofisticate elaborazioni elettroniche consentivano infatti di non toccare il fragile materiale in esame che poteva essere addirittura lasciato nel suo sarcofago . 
in aggiunta a ci la tc poteva dare alcune informazioni utili ai conservatori per pianificare il restauro delle mummie , potendo identificare al contempo i componenti chimici delle sostanze utilizzate per limbalsamazione [ 44 ]  . da qualche anno la tac pu avvalersi di un sistema di rilevazione multiplo , o meglio pu utilizzare una fila di detettori per la cattura dellimmagine che risulta cos pi definita ( mdct ) [ 45 ]  . 
la tac infatti oggi il solo metodo non invasivo per ottenere dati fondamentali per la ricostruzione tridimensionale dellintera mummia ( cio tanto del volto quanto del corpo ) , ricostruzione realizzata mediante la combinazione delle immagini assiali con quelle sagittali e coronali , queste ultime ottenute per riformattazione , grazie a un processo di algoritmi chiamato post - processing . la possibilit di ricostruire virtualmente la mummia nel suo volume , cio in 3d , usando voxel ( unit di volume con coordinate x , y , z , conosciuto come pixel nel mondo 2d ) permette di ottenere immagini che possono essere elaborate elettronicamente , utilizzando una workstation dedicata dotata di software specifico , e quindi meglio studiate [ 47 ]  . 
con la ricostruzione in 3d possibile valutare con accuratezza i materiali e i metodi di mummificazione , avere modelli anatomici e minimi particolari in pi piani , illustrare la preservazione dei tessuti molli e , in dettaglio , laspetto fisico delle mummie . 
tali complessi studi proseguono analiticamente dalla fine degli anni 80 a oggi , spesso mettendo in stretta collaborazione musei con universit , come nel caso del recente gruppo di studio delluniversit di tolosa con il locale museo georges labit [ 4856 ]  . 
 il 1 luglio 2004 , presso il british museum , stato aperto al pubblico il silicon graphic reality center dove i visitatori possono esplorare in un viaggio virtuale di ventidue minuti una mummia della xxii dinastia virtualmente ricostruita . 
7 x - ray of mummy of queen nedjemet ( third intermediate period ; xxi dynasty ) showing a large heart scarab of intense radiopacity ( probably not metallic ) and the four sons of horus of lesser radiopacity ( moulded in wax ) in the thorax . 
7 radiografia della mummia della regina nedjemet ( terzo periodo intermedio , xxi dinastia ) in cui si nota la presenza nel torace , in sede paracardiaca , di un grande scarabeo del cuore di radiopacit intensa ( ma verosimilmente non metallica ) e dei quattro figli di horus di radiopacit relativamente minore ( modellati in cera )  . 
3d reconstruction allows accurate evaluation of embalming materials and methods , it provides anatomical models and visualises minor details in several planes , it illustrates the preservation of soft tissue and gives a detailed view of the physical appearance of the mummies . 
such complex studies have continued since the late 1980s , often involving the close cooperation between museums and universities , as is the recent case of the research team from the university of toulouse and the local georges labit museum [ 4856 ]  . 
 on july 1 , 2004 , the british museum opened the silicon 624 radiol med ( 2008 ) 113 : 615626 graphics reality center where visitors can explore , in a virtual tour lasting 22 minutes , a mummy of the xxii dynasty that has been totally reconstructed virtually . 
 additionally , over the past ten years , the use of ct or mdct images of the face in combination with sophisticated processing and graphics software has made it possible to carry out a complex and suggestive three - dimensional reconstruction of the contours of mummys original face at an age close to that of his or her death . 
the digital model obtained from the virtual three - dimensional ct data of the skull surface is used as a basis either for stereolitography ( which , with the assistance of a sculptor , starts from a resin prototype to reconstruct the different thicknesses of the facial tissues and create a face ) or for computer - aided reconstruction ( which creates a face for the individual , which , if not a true likeness , appears scientifically consistent with the available data ) or for completely computerised and virtual reconstruction ( the head and the face are completely reconstructed by the computer ) [ 5763 ]  . the dehydrated body of the mummy , which does not produce sufficient signal to generate a resonance image , clearly represents a limitation for the use of magnetic resonance imaging , although this modality has already been used to visualise some residual nervous structures [ 34 , 64 ]  . conventional endoscopy , by means of a flexible or stiff fibre - optic endoscope , has instead been successfully used for many years in the study of egyptian mummies , both for the non - destructive study of the head and neck region especially to study the nasal cavities and auditory passages and as a basic aid for tissue biopsies [ 33 , 65 , 66 ]  . today , the high quality of standard radiographic images , conventional axial ct imaging , multiplanar reformation , three - dimensional reconstruction , facial reconstruction and finally the suggestive virtual flight through the inside of the mummy obtained with the use of virtual endoscopy are all methods that are employed in the radiological study of the mummies of ancient egypt . 
imaging techniques , from the most basic to the most sophisticated have therefore taken on a fundamental role in this field of study , and the history of imaging has shown that advances in radiographic technique , from the discovery of x - rays over a century ago to the three - dimensional reconstructions of today , have led from clinical hypotheses to accurate and reliable analyses and fascinating multiplanar image reconstructions . the close collaboration of physicians , archaeologists and engineers thus expands our medical and historical knowledge of ancient egypt , while ensuring that the integrity of this shared archaeological heritage is preserved . di grafica elettronica , da circa dieci anni pu essere eseguita la complessa e suggestiva ricostruzione facciale tridimensionale di base che porta a delineare il volto originario della mummia presa in esame , simulato in unet vicina a quella dellindividuo al momento della morte . 
il modello digitale che si ottiene partendo dai dati tac tridimensionali virtuali della superficie del cranio usato come base o per lo sviluppo della tecnica stereolitografica ( che con laiuto di uno scultore , partendo da un prototipo di resina , ricostruisce i differenti spessori dei tessuti facciali creando cos un volto ) o per la ricostruzione assistita dal calcolatore ( che crea un volto dellindividuo che , se non somigliante , appare scientificamente coerente con le informazioni a disposizione ) o ancora per la ricostruzione completamente computerizzata e virtuale ( una ricostruzione del capo e del volto operata dal computer ) [ 5763 ]  . lessiccato e disidratato corpo della mummia , che non fornisce segnale sufficiente per generare una immagine di risonanza , rimane ovviamente un limite per luso dellesame di risonanza magnetica , sebbene tale esame sia stato gi utilizzato per visualizzare unicamente alcune strutture nervose residuali [ 34 , 64 ]  . la tecnica endoscopica tradizionale , mediante endoscopio flessibile o rigido a fibre ottiche , invece da tempo validamente utilizzata per lo studio delle mummie egizie , sia per un esame non distruttivo del capo e del collo in particolare per lo studio delle cavit nasali e dei condotti uditivi sia come base di supporto per eventuali biopsie [ 33 , 65 , 66 ]  . oggi , lalta qualit della immagine radiografica standard , limmagine tc assiale convenzionale , la riformattazione multiplanare , la ricostruzione tridimensionale , la ricostruzione del volto e , da ultimo , anche il suggestivo volo virtuale attraverso linterno della mummia , ottenuto sfruttando le tecniche di endoscopia virtuale , sono tutte metodiche che vengono utilizzate nellanalisi radiografica delle mummie dellantico egitto . 
although low - dose protocols will soon be available , a substantial dose reduction can already be achieved by tailoring mdctu to the clinical problem rather than using a standardised approach . 
in our department , the last urographic procedure was performed in may 2006 . keywords multislice computed tomography urography urinary tract kidney riassunto lanalisi della letteratura sulla accuratezza diagnostica di uro - tc ed urografia mette in rilievo la scarsit di dati comparativi disponibili . 
ci si sta avviando verso protocolli a bassa dose , ma gi ora una riduzione consistente della dose si pu ottenere modificando leffettuazione dellindagine in base al problema clinico . tutte queste considerazioni fanno s che lurografia possa veder cancellato anche il limitato spazio che ha mantenuto negli ultimi anni . 
nel nostro istituto lultimo esame urografico stato effettuato nel maggio 2006 . parole chiave tomografia computerizzata multistrato urografia via escretrice urinaria rene introduction introduzione computed tomography urography ( ctu ) is a dedicated multiphasic ct scanning technique optimised for the imaging of the urinary tract in which intravascular contrast mediluro - tc una tecnica tc dedicata , multifasica , utilizzata per limaging dellapparato urinario nella quale viene somministrato mezzo di contrasto per via endovascolare e nella radiol med ( 2008 ) 113 : 658669 um is used and in which high - resolution images of the renal parenchyma and urinary tract ( including bladder ) are obtained . 
this is the definition of ctu suggested by the ct urography working group of the european society of urogenital radiology ( esur ) in their society meeting in 2006 [ 1 ]  . 
the use of this definition means that ct examination of many of the current indications for ct of the urinary tract , such as characterisation of complex renal masses , staging of renal cell carcinoma , acute flank pain , renal infection and evaluation of renal arteries for possible renovascular hypertension , should not be labelled ct urography . 
in fact , this procedure is optimised for evaluating both the renal parenchyma and the entire excretory pathway . acquisition of high - resolution images of the urinary tract may challenge the residual role of intravenous urography ( ivu ) , which progressively declined over recent decades following the introduction of ultrasonography and ct . 
based on the recent technological developments and literature data , it appears worthwhile to now compare ctu and ivu in terms of diagnostic accuracy , patient and referring physician acceptance , radiation dose and costs in order to evaluate the role of these procedures . indications for multidetector computed tomography urography in 2001 , dalla palma [ 3 ] summarised the residual roles of intravenous urography ( ivu ) , which at the time was indicated for asymptomatic haematuria [ in which it complemented ultrasound , plain film of the abdomen and cystoscopy ] , congenital anomalies of the urinary tract , prior to endourological procedures , possible fistulas , renal transplantation , urinary tuberculosis and suspected ureteral pathology . 
five years later , nolte - ernsting and cowan [ 4 ] reported the most frequent indications for multidetector computed tomography urography ( mdctu ) , namely , suspected urothelial tumour ( haematuria or unexplained hydronephrosis ) , urinary tract trauma , preand postoperative urinary tract assessment , three - dimensional planning for difficult cases of percutaneous nephrolithotomy and complex cases of urinary tract infection , including tuberculosis . there is considerable overlap between these indications and those listed in 2001 as residual roles of ivu . 
an analysis of the results of comparative studies of mdctu and ivu is required in order to compare the diagnostic accuracy of the two techniques . quale vengono ottenute immagini ad alta risoluzione del parenchima renale e delle vie escretrici ( vescica compresa )  . questa la definizione di uro - tc proposta dal ct urography working group dellesur nel meeting della societ tenutosi nel 2006 [ 1 ]  . 
tale definizione implica che molte delle principali indicazioni allo studio tc dellapparato urinario , quali la caratterizzazione di masse renali complesse , la stadiazione di neoplasie renali , la valutazione di pazienti con dolore acuto al fianco , lo studio delle infezioni renali e dellipertensione di possibile origine nefrovascolare , ovvero numerose consolidate indicazioni alla tc , non rientrano tra gli esami uro - tc , con i quali viene ottimizzata sia la valutazione del parenchima renale , sia la valutazione della via escretrice dellintero apparato urinario . lacquisizione in particolare di immagini ad alta risoluzione della via escretrice pu mettere in discussione il ruolo residuo dellurografia che si andato via via riducendo nel corso degli ultimi decenni , con lavvento dellecografia prima e della tomografia computerizzata successivamente . su questa rivista stata pubblicata pochi anni or sono una messa a punto sulluro - tc [ 2 ]  . 
alla luce degli sviluppi tecnologici e degli ulteriori dati della letteratura appare oggi opportuno mettere a confronto uro - tc ed urografia in termini di accuratezza diagnostica , accettabilit da parte del paziente e del medico inviante , dose di radiazioni e costi , valutando alla luce di tali aspetti quale pu essere allo stato dellarte il campo di applicazione di queste indagini . indicazioni della uro - tc nel 2001 dalla palma [ 3 ] ha sintetizzato il ruolo residuo dellurografia , che trovava allora indicazioni nellematuria asintomatica ( situazione in cui risultava complementare allecografia , allesame diretto delladdome ed alla cistoscopia ) , nelle anomalie congenite dellapparato urinario , prima di procedure endourologiche , in caso di possibili fistole , nel rene trapiantato , nella tubercolosi urinaria e nel sospetto di patologia ureterale . 
a distanza di 5 anni nolteernsting e cowan [ 4 ] elencavano le indicazioni pi frequenti allutilizzo della uro - tc , ed in particolare sospetta neoplasia urologica ( ematuria o idronefrosi di natura da determinare ) , traumi dellapparato urinario , valutazione dellapparato urinario pree post - chirurgia , planning tridimensionale nei casi difficili di nefrolitotomia percutanea e infezioni urinarie complesse , tra cui la tubercolosi . 
queste indicazioni appaiono in larga misura sovrapponibili a quelle che costituivano il ruolo residuo dellurografia nel 2001 . morcos [ 5 ] era ancora pi determinato , e sosteneva che le applicazioni delluro - tc sono le stesse dellurografia . 
appare quindi opportuno valutare i risultati di studi compara660 mdctu : technique the radiological literature describes several technical variants for executing mdctu [ 616 ] , the differences mainly concerning contrast - agent administration , number of phases , examination technique ( supine or prone patient position , use of ureteral compression , saline infusion , oral hydration or use diuretics such as furosemide ) and acquisition timing . at our institution , mdctu is performed with a 64 - slice scanner using the split - bolus technique , which allows us to limit the number of scans obtained . 
as shown in table 1 , once the patient is positioned on the table , furosemide is administered intravenously ( 0.1 mg / kg ) , and an unenhanced scan is acquired from the upper pole of the kidneys to the bladder base . 
a first bolus of 400 mgi / kg is injected , followed by a second bolus of 200 mgi / kg after a 6 - min delay and a saline flush . 
two minutes after the second bolus , a second scan is acquired of the entire abdomen and pelvis , which affords both an effective nephrographic - phase image ( thanks to the second bolus of contrast material ) and good opacification and distension of the urinary tract ( thanks to the time delay after the first bolus )  . the results obtained with the preliminary administration of a diuretic ( furosemide ) were compared with those of a similar technique involving intravenous administration of 250 ml of saline solution before the examination . 
the system assesses image quality at the level of the calyces on a scale from 0 to 5 ( higher scores reflect better opacification and distension )  . the modified scoring system was used to compare the two techniques in 70 patients ( table 3 ) and showed significantly better results at the level of the calyces , ureters and bladder in patients who received furosemide . table 1 multidetector computed tomography urography : split - bolus technique contrast medium ( 400 mgi / kg ) 2 ml / s 6 min contrast medium ( 200 mgi / kg ) 2 ml / s 2 min unenhanced scan nephrograhic - excretory scan tabella 1 uro - tc : tecnica split bolus mezzo di contrasto ( 400 mgi / kg ) 2 ml / s 6 min mezzo di contrasto ( 200 mgi / kg ) 2 ml / s 2 min scansione diretta scansione nefro - escretoria radiol med ( 2008 ) 113 : 658669 tivi tra uro - tc ed urografia per mettere a confronto la rispettiva accuratezza diagnostica di queste due metodiche . uro - tc : cenni di tecnica va sottolineato come in letteratura [ 616 ] siano riportate numerose varianti tecniche per lesecuzione delluro - tc , che differiscono in termini di modalit di somministrazione del mezzo di contrasto , numero di fasi , tecnica desame ( posizionamento del paziente supino o prono , utilizzo di compressione ureterale , ricorso a infusione di soluzione fisiologica , a idratazione orale o a somministrazione di diuretici quali la furosemide ) e tempistica di acquisizione delle immagini . nel nostro istituto si effettuano gli esami uro - tc con apparecchiatura a 64 strati utilizzando la cosiddetta tecnica split bolus , che consente di limitare il numero di scansioni ( tabella 1 )  . 
come illustra la tabella , al paziente , non appena posizionato sul lettino , viene effettuata uniniezione endovenosa di furosemide ( 0 , 1 mg / kg ) e si effettua successivamente una scansione senza mezzo di contrasto dal polo superiore dei reni alla base vescicale . 
in particolare viene iniettato un primo bolo di 400 mgi / kg e dopo un intervallo di 6 minuti un ulteriore bolo di 200 mgi / kg seguiti da infusione di soluzione fisiologica . 
due minuti dopo questo secondo bolo viene effettuata una seconda acquisizione , che comprende lintero addome e la pelvi e consente di ottenere sia una valida nefrografia ( grazie al secondo bolo di mezzo di contrasto ) sia una buona opacizzazione e distensione della via escretrice ( dato il tempo intercorso dal primo bolo )  . i risultati ottenuti con questa tecnica che prevede la somministrazione preliminare del diuretico ( furosemide ) sono stati confrontati con tecnica analoga che prevedeva invece preliminare somministrazione di 250 ml di soluzione fisiologica per via endovenosa . 
per un confronto del genere vi la necessit di utilizzare un modello di valutazione dettagliato e accurato che permetta di analizzare la qualit dellimmagine ( in termini di opacizzazione e di distensione della via escretrice ) confrontando cos le diverse tecniche . nella tabella 2 proposto un modello di valutazione che si riconduce a quello suggerito da kelsey fry et al . 
questo modello valorizza in particolare la qualit dimmagine a livello caliceale e utilizza una scala da 0 a 5 ( attribuendo il punteggio pi elevato quando opacizzazione e distensione sono ottimali )  . 
lang [ 18 ] ha pubblicato un lavoro retrospettivo in cui considerava gruppi di pazienti con microematuria e urografia negativa che venivano successivamente sottoposti ad uro - tc la quale risultava in grado di riconoscere un numero elevato di lesioni che erano sfuggite allurografia . 
confronto di due tecniche di idratazione ( 70 pazienti ) calici pelvi ureteri vescica media media media media furosemide ( 35 pts ) 250 ml soluzione fisiologica ( 35 pts ) furosemide vs 250 ml soluzione fisiologica 25 , 8 24 , 0 0 , 73 0 , 95 0 , 55 0 , 63 0 , 86 0 , 63 p < 0 , 05 n.s. p < 0 , 05 p < 0 , 05 ds , deviazione standard ; ns , non significativo 662 radiol med ( 2008 ) 113 : 658669 fig . 
3 uro - tc che evidenzia neoplasia uroteliale che interessa i calici del gruppo inferiore e il bacinetto del rene sinistro con stenosi a margini irregolari dei calici stessi . erano significativamente migliori con luro - tc sia in termini di sensibilit ( 100% vs 60 , 5% ) che di specificit ( 97% vs 90 , 9% ) e di accuratezza diagnostica ( 98 , 3% vs 80 , 9% )  . 
the authors , however , only reported using a spiral ct scanner without providing further details on the device ( it is unknown whether it was a singleor multislice scanner )  . 
a retrospective review identified 24 out of 27 . unfortunately , a comparative evaluation with ivu was only possible on six lesions , all of which were identified on mdctu and only three on ivu . 
these data are , however , too limited to allow any definitive conclusions . mccarthy and cowan [ 21 ] compared mdct with retrograde pyelography in patients with haematuria and unexplained hydronephrosis . 
the better performance of mdctu was related to its ability to detect ureteral lesions causing wall thickening without producing changes in calibre ( which explained the failed detection at retrograde pyelography )  . when comparing mdctu and ivu , it is important to consider the performance of the two techniques in detecting bladder tumours , even though cystoscopy remains the method of choice for this diagnosis . 
turney et al [ 22 ] studied 200 consecutive patients with haematuria who underwent mdctu and flexible cystoscopy on the same day . mdctu , performed with an 8 - slice scanner , yielded 93% sensitivity , 99% specificity , a positive predictive value of 98% and a negative predictive value of 97% using cystoscopy as the gold standard . 
additionally , it should be remembered that it is impossible to compare clinical results obtained with mdctu using scanners with different numbers of slices . mdctu vs ivu : acceptance by patients and by referring clinicians patients no doubt accept mdctu more readily than ivu , as it requires no preparatory bowel cleansing . 
questi numeri sono peraltro troppo ridotti per poter giungere a conclusioni in merito . mc carthy e cowan [ 21 ] hanno invece messo a confronto la tc con apparecchiatura multidetettore con la pielografia retrograda in pazienti con ematuria e idronefrosi inesplicata . 
va in particolare sottolineato come i risultati migliori delluro - tc fossero legati alla possibilit di riconoscere lesioni ureterali che determinavano un ispessimento della parete del viscere senza peraltro causare una variazione del suo calibro ( il che giustificava il mancato riconoscimento alla pielografia retrograda )  . nel confronto tra uro - tc ed urografia rilevante analizzare i risultati di queste due indagini nel riconoscimento di neoplasie vescicali , anche se va ricordato come la cistoscopia risulti lindagine di riferimento per la diagnosi di questa patologia . 
luro - tc , effettuata con apparecchiatura a 8 strati , ha raggiunto una sensibilit del 93% , una specificit del 99% , un valore predittivo positivo del 98% e un valore predittivo negativo del 97% , utilizzando la cistoscopia come gold standard . 
lanalisi della letteratura fa infatti rilevare come la sensibilit dellurografia nella diagnosi di tumore vescicale vari tra il 62% e l86% [ 23 , 24 ] , quindi nettamente inferiore ai risultati riportati per luro - tc . 664 radiol med ( 2008 ) 113 : 658669 fig . 
4a intravenous urography ( ivu ) demonstrates a gap in the opacification on the lumbar portion of the right ureter ( arrow ) , which was constantly seen on all radiograms . 
 c mdctu : in addition to the cystic lesion within the lower sinus of the right kidney , a small pelvic filling defect is demonstrated on the same side , which was missed on urography ( arrow )  . 
oltre la lesione cistica nel contesto del recesso sinusale inferiore del rene di destra si evidenzia , sempre da tale lato , piccolo difetto di riempimento a livello della pelvi che non stato riconosciuto urograficamente ( freccia )  . 
it might , in fact , be helpful to select and transmit only key images that document abnormal findings and provide ( urography - like ) maximum intensity projection ( mip ) reconstructions and curved multiplanar reconstructions ( mpr ) along the course of the ureters . 
transmission of diagnostic information that is of superior quality to that obtained with urography , in a clear and concise manner and with urography - like images , will help to rapidly overcome any understandable initial difficulties . mdctu vs ivu : cost analysis using a method adopted in a previous study [ 25 ] , we performed a cost analysis based on the activity carried out at our institution . 
va inoltre rilevato come non vi sia allo stato attuale alcuna possibilit di confrontare i risultati clinici che si ottengono con uro - tc con apparecchiature a diverso numero di strati . 
 uro - tc versus urografia : accettazione da parte dei pazienti e dei medici invianti non vi alcun dubbio che i pazienti accettino molto pi volentieri luro - tc rispetto allurografia , non essendo necessario con la prima il ricorso ad alcuna preparazione per ottenere una toilette intestinale . 
non vi dubbio che luro - tc fornisca al medico inviante un volume notevolissimo di informazioni che riguardano il parenchima renale , lintera via escretrice , ed ancora gli altri organi e strutture addominali . 
riteniamo che possa essere opportuno evidenziare e trasmettere immagini chiave che documentano le alterazioni rilevate e accanto a queste fornire ricostruzioni mip ( simil - urografiche ) e ricostruzioni multiplanari curve lungo il decorso degli ureteri . 
la trasmissione di informazioni diagnostiche superiori a quelle urografiche fornite in maniera chiara , sintetica e con un imaging simil - urografico porter a superare rapidamente le comprensibili difficolt iniziali . uro - tc versus urografia : analisi dei costi abbiamo effettuato nel nostro istituto unanalisi dei costi che considera lattivit effettuata allinterno dellistituto di radiologia , utilizzando una metodologia gi messa a punto in precedente studio [ 25 ]  . 
stato preso in esame il costo differenziale di ciascuna indagine ( uro - tc , urografia ) i costi comuni e il costo pieno di ogni modalit ( rappresentato dalla somma di costo differenziale e costo comune )  . 
va rilevato come stato stimato limpegno temporale delle singole figure professionali , considerando per quanto riguarda il personale medico anche i tempi relativi alla elaborazione delle immagini e alla refertazione . 
sono stati quindi presi in considerazione i costi comuni , ossia quei costi relativi a personale di supporto ( archivisti , dattilografe , ) e a materiale di supporto ( computer , stampanti , ) comuni a tutti gli esami . lassunto che questi costi si distribuiscono in maniera identica tra tutti gli esami effettuati nellistituto di radiologia . 
da ci deriva che il costo pieno delluro - tc nella nostra realt operativa di 141 , 30 euro , mentre quello dellurografia di 98 , 20 euro . va sottolineato come questi sono i costi di tali indagine nel nostro istituto nella nostra attuale realt operativa . 
tali dati non vanno quindi esportati in maniera acritica in altri ambienti ove potrebbero risultare sensibilmente diversi , ad esempio per il diverso costo dellapparecchiatura , per limpiego di diverse quantit di mezzo di contrasto , per un diverso impiego del personale e ancora per parametri stipendiali diversi . emerge comunque nella nostra realt operativa come il costo delluro - tc sia superiore di circa il 50% rispetto allurografia . 
 [ 22 ] in their study of mdctu in patients with bladder tumours . the authors believe that mdctu is a useful first - line exam in patients with haematuria , as it avoids the need for cystoscopy in patients with negative mdctu and leads to resection in those with evident tumours . 
because fewer examinations are required , this approach could accelerate the diagnostic process , with clear economic advantages . mdctu vs ivu : radiation dose wide variations in radiation dose have been reported for mdctu , first of all depending on the number of phases used . 
table 6 shows indicative dose levels derived from the literature [ 1 , 4 , 13 , 26 , 27 ] : 2535 msv for four - phase mdctu ( unenhanced , arterial , parenchymal and excretory ) ; radiol med ( 2008 ) 113 : 658669 tro sottolineato come questa analisi prenda in considerazione solo i costi allinterno della struttura di radiologia , mentre una visione pi ampia deve considerare la possibilit che luro - tc possa modificare gli approcci diagnostici ad alcune categorie di pazienti e da ci potrebbe derivare un indubbio vantaggio economico . 
in particolare lo ct urography working group dellesur [ 1 ] ha rilevato come luro - tc possa essere utilizzata come primo esame in pazienti con una elevata probabilit pre - test di neoplasie dellapparato urinario . 
in questi pazienti la sostituzione delliter consueto ( ecografia , urografia , cistoscopia ) con un iter pi rapido ( uro - tc e cistoscopia ) potrebbe assicurare benefici economici . 
questi autori ritengono che luro - tc sia un utile esame di primo approccio nei pazienti con ematuria , evitando la necessit della cistoscopia in quelli in cui luro - tc negativa e conducendo alla resezione quelli con evidenti tumori . 
i vantaggi in termini economici sarebbero quindi evidenti . uro - tc vs urografia : dose di radiazioni in letteratura sono riportati valori di dose molto diversi per quanto riguarda luro - tc , dato che dipende innanzitutto dal numero di fasi che vengono acquisite . 
nella tabella 6 vengono riportati dei valori di dose indicativi desunti dalla letteratura [ 1 , 4 , 13 , 26 , 27 ] che risultano tra i 25 e i 35 msv per luro - tc con 4 fasi ( diretta , arteriosa , parenchimale ed escretrice ) , di 1525 msv per luro - tc con 3 fasi ( diretta , nefrografica ed escretoria ) e di circa 10 msv per luro - tc con 2 fasi ( diretta e nefro - escretoria combinata ) da noi preferita . 
tali valori sono comunque superiori a quelli dellurografia la cui dose si aggira intorno a 5 msv , dato anchesso estremamente variabile , legato soprattutto al numero di esposizioni e allutilizzo delleventuale tomografia . 
pur sottolineando la variabilit di tali dati , non vi dubbio che allo stato attuale luro - tc , comunque eseguita , eroga una dose superiore a quella erogata dallurografia . 
va peraltro sottolineato come la via escretrice opacizzata sia una struttura ad alto contrasto e come tali strutture vengono riconosciute con tomografia computerizzata senza sostanziali variazioni della qualit entro un range di dose ampio [ 28 ]  . 
soradiol med ( 2008 ) 113 : 658669 table 6 multidetector computed tomography urography ( ctu ) versus intravenous urography ( ivu ) : radiation dose tabella 6 uro - ct vs urografia . 
these dose values are consistently higher than those of ivu , which delivers a dose of approximately 5 msv , even though this value is also very variable and dependent on the number of exposures and possible use of tomography . 
furthermore , use of automatic tube - current modulation may reduce the dose by 10%30% . although no definite solutions for dose reduction exist , there is an awareness that radiation exposure may be decreased significantly without influencing diagnostic accuracy . 
it is very likely that low - dose protocols will soon become available for mdctu , as happened for the ct study of acute flank pa however , it is also becoming clearer that the best way to reduce radiation dose is to tailor the mdctu examination to the individual patients clinical problefor example , the unenhanced phase is not always necessary and may be eliminated when evaluating congenital malformations of the urinary tract [ 1 ]  . 
another possibility is to use the split - bolus technique to combine the nephrographic and excretory phases , as this produces an effective nephrographic - phase image and good opacification and distension of the urinary tract with a single scan . 
 [ 29 ] che ha rilevato sperimentalmente come la riduzione da 120 a 90 kv porti ad una riduzione di dose del 60% senza effetti sul rapporto contrasto / rumore . 
una riduzione automatica della corrente del tubo pu condurre inoltre ad una riduzione di dose che varia dal 10% al 30% . allo stato attuale non vi sono quindi soluzioni gi definite , ma vi la netta percezione che la dose pu essere notevolmente ridotta senza che ci condizioni il risultato diagnostico . 
 assai verosimile che in un prossimo futuro si utilizzeranno in uro - tc protocolli a bassa dose analogamente a quanto avvenuto negli anni passati per la valutazione tc di pazienti con dolore acuto al fianco , situazione clinica che attualmente viene affrontata con limpiego di protocolli a bassa dose . 
vi comunque la percezione sempre pi chiara che il modo migliore per ridurre la dose sia leffettuazione di esami uro - tc non standardizzati ma modificati in base al problema clinico del singolo paziente . ad esempio va rilevato come la fase diretta non sia sempre necessaria , evitabile ad esempio nella valutazione delle malformazioni congenite dellapparato urinario [ 1 ]  . unaltra possibilit rappresentata dalla combinazione della fase nefrografica con quella escretoria , con la tecnica split bolus , che consente di ottenere in ununica scansione una valida nefrografia e una buona opacizzazione e distensione della via escretrice . 
studi di screening o la valutazione di varianti congenite 668 radiol med ( 2008 ) 113 : 658669 urographic acquisitions are based on the clinical problem and the findings identified during the procedure . 
in the evaluation of patients with a high pretest probability of malignant disease , a higher radiation dose is justified ( three phases are suggested ) a differentiated approach was also suggested by nolteernsting and cowan [ 4 ] for patients with haematuria : the authors recommended different diagnostic algorithms according to the type of haematuria ( microor macroscopic ) and the patients age ( younger or older than 40 years )  . 
mdctu is never indicated for patients younger than 40 years of age ( whether with microor macrohaematuria )  . the literature thus indicates that it is technically possible to significantly reduce mdctu dose but that it is the radiologists duty to use the technique rationally and adapt it to the patients clinical problem , as this will lead to a substantial reduction in radiation exposure . conclusions our review of the literature on the diagnostic accuracy of mdctu and ivu revealed a relative lack of comparative data . 
from an economic point of view , although mdctu has a higher cost than ivu , it allows for considerable economic savings by simplifying the diagnostic workup in some cases . 
nella valutazione di pazienti con elevata probabilit pretest di patologia maligna giustificata una maggiore dose di radiazioni ( si suggeriscono tre fasi )  . un approccio differenziato anche quello proposto da nolte - ernsting e cowan [ 4 ] nei pazienti con ematuria : essi suggeriscono un algoritmo diagnostico diverso a seconda della tipologia di ematuria ( microo macroscopica ) e dellet del paziente ( inferiore o superiore ai 40 anni )  . luro - tc stata presa in considerazione nei pazienti con microematuria di et superiore ai 40 anni qualora ecografia e cistoscopia fossero negative e i sintomi persistessero . in tal caso gli autori suggeriscono il ricorso alluro - tc o allurografia . 
lurotc non viene invece proposta per i pazienti di et inferiore ai 40 anni ( sia con microche con macroematuria )  . appare quindi chiaro dallanalisi della letteratura che ci sono i presupporti tecnici per ridurre considerevolmente la dose in uro - tc ma che fin dora deve essere compito del radiologo utilizzare in maniera ragionata questa tecnica , modulandola in base al problema clinico del singolo paziente , e ci potr portare a una riduzione particolarmente consistente della esposizione radiante . conclusioni lanalisi della letteratura sulla accuratezza diagnostica di uro - tc ed urografia mette in rilievo la scarsit di dati comparativi disponibili . 
ci si sta avviando verso protocolli a bassa dose , ma gi ora una riduzione consistente della dose si pu ottenere modificando leffettuazione dellindagine in base al problema clinico . tutte queste considerazioni fanno s che lurografia posradiol med ( 2008 ) 113 : 658669 already be achieved by tailoring the examination to individual patients clinical problem . in the light of these considerations , it is likely that ivu may lose its residual role . 
in our institution , the last urographic examination was performed in may 2006 , a date that marked the end of ivu in our experience . sa veder cancellato anche il limitato spazio che ha mantenuto negli ultimi anni . 
patti1 1department of diagnostic and interventional radiology , ospedale ferrarotto , via trieste 14 , 95127 catania , italy 2department of radiology , university of crete , faculty of medicine , crete , greece 3division of biostatistics , medical school of crete , crete , greece 4department of angiology , ospedale ferrarotto , catania , italy 5department of nephrology , ospedale vittorio emanuele , catania , italy 6department of interventional radiology and vascular surgery , multimedica irccs , sesto san giovanni , milan , italy correspondence to : a . 
seventeen patients ( 12 men and five women ; age range 5479 years , mean age 66.5 ) with stenosis or occlusion at the proximal or distal anastomoses of peripheral bypass grafts were treated with cba . 
the diameter of the selected cutting balloon was 1 - mm smaller than the vessel distal to the anastomosis and , in the event of suboptimal outcome , the procedure was completed with repeat dilatation with a larger standard balloon ( + 1 mm )  . 
during a mean follow - up period of 10.4 months ( range 521 months ) , two restenoses developed at 9 and 7 months , which were treated with the same technique ; in one patient with recurrent bypass occlusion at 5 months , a new bypass was created surgically owing to contraindications for locoregional thrombolysis . 
diciassette pazienti ( 12 uomini , 5 donne ; et 5479 anni , media 66 , 5 anni ) con stenosi od occlusione in corrispondenza delle anastomosi prossimale o distale di bypass periferico sono stati sottoposti ad angioplastica con cb . 
durante un follow - up variabile tra 5 e 21 mesi ( media 10 , 4 mesi ) , sono state evidenziate 2 restenosi a 9 e 7 mesi trattate con medesima tecnica ; in un paziente con occlusione ricorrente del 720 radiol med ( 2008 ) 113 : 719726 12 and 18 months was 82.35% , whereas the two cases of restenoses treated with repeat cba underwent further follow - up at 10 and 7 months , respectively . 
our data confirm the efficacy of cba in the treatment of anastomotic stenoses of peripheral arterial bypass grafts . keywords angioplasty bypass graft stenosis bypass a 5 mesi stato confezionato chirurgicamente un nuovo bypass vista la presenza di controindicazioni alla terapia trombolitica locoregionale . 
i nostri dati confermano lefficacia del cb nel trattamento delle stenosi anastomotiche dei bypass arteriosi periferici . parole chiave angioplastica bypass stenosi introduction introduzione several factors limit the long - term patency of peripheral arterial bypass grafts . 
these factors are mainly technical and related to the technique used for creating the bypass graft , such as graft material , graft length and surgical anastomosis site [ 1 , 2 ] , and individual patient factors , such as hypertension , diabetes , hyperlipidaemia and smoking . 
there are two kinds of anastomotic stenoses : early stenoses , mostly related to incorrect surgical procedure [ 3 , 4 ] , and late stenoses , arising more than 1 month after surgery , which are mainly related to intimal hyperplasia [ 5 ] and are often resistant to dilatation . 
interventional radiology options for treating anastomotic stenoses include angioplasty , metallic - stent placement , fibrinolysis and mechanical thrombectomy [ 2 ]  . recent reports have proposed the use of cutting balloons , that is , noncompliant balloon catheters featuring three to four atherotomes ( microsurgical blades ) mounted longitudinally on the outer surface and covered by the folds of the balloon when deflated [ 6 ]  . 
during inflation , the blades are exposed and come into contact with the vessel - wall lesion , thereby dilating and cutting into extremely resistant stenotic lesions , such as those on the anastomoses of bypass grafts [ 79 ]  . 
the purpose of this paper is to present our experience with a series of patients with anastomotic strictures of peripheral bypass grafts treated with cutting - balloon angioplasty ( cba )  . materials and methods between october 2005 and december 2006 , 17 patients ( 12 men , five women ; age range 5479 years , mean age 66.5 ) underwent percutaneous cba for focal stenoses ( < 2 cm ) at the distal ( 10 ) and proximal ( 7 ) anastomoses of peripheral arterial bypass grafts . 
the stenoses were diagnosed on the basis of clinical and colour - doppler ultrasound findings and confirmed by morphological angiography and intravascular measurement of pressure gradients above and below the numerosi fattori limitano la perviet a lungo termine dei bypass arteriosi periferici . 
riconosciamo principalmente fattori legati alla tecnica di confezionamento del bypass come il materiale , la lunghezza del bypass , la sede chirurgica anastomotica [ 1 , 2 ] , ed altri legati alle caratteristiche proprie del paziente , riconosciute altres come fattori di rischio cardiovascolare , ovvero lipertensione , il diabete , liperlipoproteinemia ed il fumo . 
esistono due tipi di stenosi anastomotiche , quelle precoci , fondamentalmente correlate ad una scorretta procedura chirurgica [ 3 , 4 ] e stenosi tardive ( a pi di un mese dallintervento ) , principalmente da riferire al fenomeno delliperplasia intimale [ 5 ] ; queste ultime risultano spesso resistenti alla dilatazione . 
le opzioni proprie della radiologia interventistica nel trattamento di tali stenosi comprendono lutilizzo dellangioplastica , il posizionamento di stent metallici , la fibrinolisi e la trombectomia meccanica [ 2 ]  . 
recentemente stato anche proposto lutilizzo del cutting balloon ( cb ) , un catetere a palloncino non compliante che presenta sulla superficie esterna 3 o 4 microtomi longitudinali , ovvero delle vere e proprie lame piccolissime nascoste dalle pieghe del palloncino quando sgonfio [ 6 ] , che durante la dilatazione vengono esposte sulla superficie del palloncino entrando in contatto con la parete vascolare lesionata , potendo cos dilatare ed incidere stenosi particolarmente resistenti come quelle presenti sulle anastomosi dei bypass [ 79 ]  . 
scopo di questo lavoro quello di presentare la nostra esperienza in una serie di pazienti portatori di stenosi anastomotiche di bypass periferici trattate mediante cb . materiali e metodi tra ottobre 2005 e dicembre 2006 , 17 pazienti ( 12 uomini , 5 donne ; et 5479 anni , media 66 , 5 anni ) sono stati sottoposti ad angioplastica percutanea con cb per stenosi focali ( < 2 cm ) localizzate a livello delle anastomosi distali ( n = 10 ) radiol med ( 2008 ) 113 : 719726 fig . 
controllo postprocedura ( c )  . e prossimali ( n = 7 ) di bypass arteriosi periferici ; le stenosi sono state diagnosticate clinicamente , mediante esame ecocolor doppler e confermate dai dati morfologici angiografici e dalla misurazione endovascolare dei gradienti pressori prima e dopo la stenosi . 
quattro pazienti al momento del trattamento si trovavano in uno stadio clinico iia secondo la classificazione di fontaine , 9 pazienti in stadio iib , mentre in 3 casi i pazienti si trovavano in ischemia acuta da occlusione recente del bypass ( pazienti 3 , 11 , 17 )  . in questi ultimi casi stata istituita terapia trombolitica locoregionale mediante urochinasi ( bolo 300000 ui in 20 minuti , seguito da una dose di 100000 ui / ora / 24 ore )  . 
in relazione alle linee guida della society of interventional radiology [ 10 ] , il successo tecnico della procedura stato definito come il miglioramento del lume vasale di pi del 50% con una stenosi residua inferiore al 20% , con un gradiente pressorio trans - stenosi inferiore a 5 mmhg . 
the types of grafts were polytetrafluoroethylene ( ptfe ) grafts ( 9 ) , grafts with in situ vein ( 2 ) , grafts with reversed vein ( 4 ) , and dacron grafts ( 2 )  . 
at the time of the procedure , four patients had stage iia disease and nine had stage iib disease according to fontaines classification , whereas three patients had acute ischaemia due to recent bypass occlusion ( patients 3 , 11 and 17 )  . 
the three patients with acute ischaemia received locoregional thrombolysis with urokinase ( bolus of 300 , 000 iu in 20 min , followed by a dose of 100 , 000 iu / h for 24 h )  . prior to cba , all patients were routinely administered a 5 , 000 - iu bolus of intra - arterial heparin accordance with the guidelines of the society of interventional radiology 722 table 1 summary of procedures performed pt . 
il follow - up stato eseguito mediante eco doppler sulla base di un criterio morfologico ( stenosi maggiore del 50% ) ed in base al picco sistolico ( psv < 160 cm / s )  . 
negli altri 8 casi stato utilizzato un cb da 5 mm , mentre in 3 soli casi si radiol med ( 2008 ) 113 : 719726 tabella 1 sommario dei trattamenti eseguiti pz . 
in eight cases , we used a 5 - mm cutting balloon , whereas only three cases were treated with a 3 - mm cutting balloon ( table 1 )  . 
during a follow - up period of 521 months ( mean 10.4 months ) , two restenoses occurred at 9 and 7 months that were treated with the same technique . 
at the time of writing , neither of the two patients who underwent repeat cba were found to have developed recurrences at further follow - up at 10 and 7 months , respectively . 
the cumulative primary patency rate at 12 and 18 months was 82.35% ( 14 of 17 cases ) , whereas the two patients treated with a second cba for restenosis had a further follow up of respectively 10 and 7 months . utilizzato un diametro di 3 mm ( tabella 1 )  . 
durante un follow - up variabile tra 5 e 21 mesi ( media 10 , 4 mesi ) , sono state evidenziate 2 stenosi ricorrenti a 9 e 7 mesi trattate con medesima tecnica ; in un paziente con occlusione ricorrente del bypass a 5 mesi stato confezionato chirurgicamente un nuovo bypass vista la presenza di controindicazioni alla terapia trombolitica loco - regionale . 
la perviet primaria cumulativa a 12 e 18 mesi stata di 14 / 17 casi ( 82 , 35% ) , mentre i due pazienti trattati con cb per restenosi hanno presentato un ulteriore follow - up rispettivamente di 10 e 7 mesi . discussion discussione the rationale for cba is to reduce the inflammatory response responsible for neointimal proliferation by minimising the trauma to the vessel wall associated with balloon dilatation [ 9 , 11 , 12 ]  . 
originally developed for cardiac appliil principio su cui si basa lutilizzo del cb quello di ridurre i fenomeni infiammatori responsabili della proliferazione neointimale mediante la riduzione del trauma vascolare ottenuto con lincisione della placca [ 9 , 11 , 12 ]  . 
inizialmente utilizzato solo in ambito cardiaco , lutilizzo del cb si ne724 cations , use of the cutting balloon has recently extended to the treatment of in - stent stenoses [ 13 ] and stenoses of dialysis fistulas [ 14 , 15 ]  . according to the literature , the results of interventional approaches to anastomotic stenosis of bypass grafts with angioplasty , atherectomy or stent placement are inferior to those of surgery . 
for this reason , a classification of distal bypass graft stenoses into simple ( single nonrestenotic lesions shorter than 1.5 cm , bypass diameter greater than 3 mm ) and complex ( restenoses , longer than 1.5 cm , bypass diameter less than 3 mm ) was proposed in 1991 [ 20 ]  . 
in light of this classification , the results obtained by the same authors and confirmed by later reports vary considerably in relation to the type of stenosis , with a 66% patency rate at 2 radiol med ( 2008 ) 113 : 719726 fig . 
2a - c stenosi anastomotica prossimale di un bypass femoro - popliteo ( a ) ; limmagine mostra il cb sgonfio posizionato a livello della stenosi che occlude completamente il flusso nel bypass ( b ) ; il controllo post - procedura mostra lottimo risultato della procedura ( c )  . gli ultimi anni allargato al trattamento di stenosi intrastent [ 13 ] o quelle riscontrabili nelle fistole da dialisi [ 14 , 15 ]  . in letteratura , lapproccio interventistico delle stenosi anastomotiche dei bypass con angioplastica , aterectomia o posizionamento di stent non raggiunge i risultati della chirurgia ; in particolare riportata una perviet ad 1 e 2 anni variabile rispettivamente dal 44% al 62 , 7% e dal 39 , 4% al 58 , 2% per quanto riguarda la sola angioplastica , che comunque non supera il 65% a 5 anni come perviet primaria assistita [ 2 , 1619 ]  . 
il successo a distanza di tempo comunque correlato sensibilmente alla presenza di una o pi lesioni ed alla loro stessa lunghezza , per tale motivo stata proposta nel 1991 [ 20 ] una classificazione delle stenosi dei bypass distali in stenosi semplici ( lesioni singole non restenotiche , lunghezza inferiore ad 1 , 5 cm , diametro del bypass maggiore di 3 mm ) e complesse ( restenosi , lunghezza maggiore di 1 , 5 cm con diametro del bypass inferiore a 3 mm )  . 
in base a ci i risultati degli stessi autori per altro confermati da altre pubblicazioni successive , variavano notevolmente in relazione al tipo di stenosi trattate , presentando un 66% di perviet a 2 anni nel caso di lesioni semplici ed un 17% nel caso di lesioni complesse [ 20 ]  . 
both of these options are technically limited . atherectomy , which has fallen into disuse , yields excellent results ( 78%88% patency at 1 and 2 years ) [ 21 , 22 ] but is limited by a high rate of complications ( 611% ) that are mostly related to the calibre of the devices used ( 810 french ) [ 21 , 22 ]  . 
recently obtained better results with primary and primary - assisted patency rates of 95% and 95% , 71% and 81% , and 71% and 76% at 6 , 12 , and 24 months , respectively [ 24 ]  . with regard to cba results , only five reports have been published in the literature . 
 [ 8 ] reported on a series of 19 patients treated for simple anastomotic and nonanastomotic stenoses , with a mean follow - up of 11.47 months and one single restenosis . 
the first complication ( pseudoaneurysm ) of cba was reported in early 2007 in a patient treated for an anastomotic stenosis of a peripheral bypass graft ; the study did not , however , compare standard balloon angioplasty and cba [ 25 ]  . 
 [ 26 ] evaluated 27 patients treated with standard balloon angioplasty ( 16 ) and cba ( 11 ) and reported a technical success rate of 74% and 82% , respectively , and primary patency rates of 62% and 36% for standard angioplasty and of 80% and 50% for cba at 6 months and 12 months , respectively . 
finally , garvin and reifsnyder [ 27 ] reported a 6 - month primary patency rate of 48% and a secondary patency rate of 99% , with 12 complications ( 11% )  . 
the results of these studies appear to be worse compared with previous reports and with our series , in part because the stenoses were not exclusively anastomotic , as in our series . 
hanno pubblicato dati pi soddisfacenti , con una percentuale di perviet primaria e primaria assistita rispettivamente del 95% e del 95% , 71% ed 81% , e 71% e 76% a 6 , 12 e 24 mesi [ 24 ]  . per quanto riguarda invece i risultati del cb , argomento di questa pubblicazione , troviamo in letteratura solo 5 pubblicazioni in merito . 
 [ 8 ] hanno invece riportato una serie di 19 pazienti trattati per stenosi semplici anastomotiche e non anastomotiche , con un follow - up medio di 11 , 47 mesi e con una sola restenosi . 
agli inizi del 2007 stata riportata la prima complicanza ( pseudoaneurisma ) in un paziente trattato con cb per una stenosi allanastomosi di un bypass periferico in una serie di pazienti in cui per non stata realizzata nessuna comparazione tra angioplastica standard e con cb [ 25 ] ; sempre nello stesso anno sono state pubblicate altre due serie interessanti ; nella prima vikram et al . 
 [ 26 ] hanno valutato 27 pazienti trattati con angioplastica standard ( n = 16 ) e con cb ( n = 11 ) riportano un successo tecnico della procedura rispettivamente del 74% e dell82% , con una perviet primaria a 6 mesi e 12 mesi del 62% e del 36% per la angioplastica standard e dell80% e del 50% per il cb . 
 [ 27 ] hanno riportato una perviet primaria a 6 mesi del 48% e secondaria del 99% , con 12 complicanze ( 11% ) ; gli ultimi lavori presentano dei dati meno positivi rispetto ai precedenti articoli ed anche alla serie da noi presentata probabilmente in relazione al fatto che le stenosi trattate non erano soltanto anastomotiche come nella nostra serie . 
 conclusions conclusioni although there is a need for even more accurate studies on larger populations and with long - term follow - up to determine the most effective treatment for peripheral bypass graft stenoses , our experience confirms and improves on the results reported in the literature concerning the treatment of simple anastomotic stenoses with cba . 
muto , via petrarca 57 , 80122 napoli , italy , tel : + 39 - 081 - 7473838 , fax : + 39 - 081 - 7173125 , e - mail : mario.muto@ospedalecardarelli.it received : 20 april 2007 / accepted : 21 november 2007 / published online : 1 july 2008 springer - verlag 2008 abstract purpose . 
from june 2000 to december 2006 , we performed o2 - o3 chemonucleolysis procedures in 2 , 900 patients affected by lumbar disk herniation . patients were selected on the basis of clinical , psychological , neurological and neuroradiological criteria . exclusion criteria were extruded hernia and / or free disc fragments , hyperalgesic - paralysing sciatica and progressive neurological impairment of the affected limb . all percutaneous treatments were performed under computed tomography ( ct ) guidance . 
according to our data , minimally invasive percutaneous treatment by intradiscal , periradicular or periganglionic o2 - o3 infiltration is a valuable and competitive technique that provides excellent results at low cost and without complications . 
i criteri di esclusione sono stati : ernia discale espulsa e / o frammento erniario libero , grave deficit motorio dellarto e / o disturbi sfinterici , sciatalgia iperalgica , deficit neurologico progressivo dellarto interessato . 
secondo la nostra casistica , il trattamento percutaneo mini - invasivo con infiltrazione di o2 - o3 intradiscale e periradicolare risulta essere unalternativa 696 radiol med ( 2008 ) 113 : 695706 keywords minimally invasive percutaneous technique o2 - o3 infiltration valida e competitiva rispetto alle altre tecniche percutanee garantendo un ottimo risultato terapeutico in termini percentuali , a basso costo , facilmente ripetibile e in assenza di complicanze . parole chiave tecniche percutanee mini - invasive ossigeno - ozono terapia introduction introduzione low back pain is among the most common spinal disorders and the leading cause of absence from work in industrialised countries [ 1 ]  . 
approximately 80% of adults experience at least one episode of low back pain during a lifetime , whereas 55% suffer from low back pain associated with radicular syndrome [ 1 ]  . 
pain may resolve spontaneously in more than 60% of patients , with computed tomography ( ct ) or magnetic resonance imaging ( mri ) evidence of hernia reduction within 89 months of presentation [ 2 , 3 ]  . surgical treatment of a herniated disc is reported to have a short - term success rate of 85%90% , with an incidence of true recurrence of disc herniation of 2%6% . 
the success rate tends to decrease to 70%80% during long - term follow - up ( more than 6 months ) as a result of the appearance of symptoms related to failed back surgery syndrome ( fbss ) [ 4 ]  . 
this syndrome is often characterised by recurrence and / or hypertrophic scar giving rise to severe symptoms in 20% of cases and a true fbss in 15% of patients [ 5 ]  . 
neurosurgeons have consequently tended to adopt a less aggressive approach , and it is estimated that only 3%4% of all patients affected by low back pain and / or sciatica receive surgical treatment in the united states [ 6 ]  . the pathogenesis of low back pain is multifactorial , with causes including mechanical compression of the nerve root associated with both immune - cell - mediated and nonimmune biohumoral inflammatory response [ 7 ]  . 
new knowledge about the pathogenesis of low back pain and fbss and the widespread conviction that conservative treatment is as beneficial as surgery in the long term have prompted research techniques , such as chemodiscolysis with chymopapain , automated percutaneous lumbar discectomy according to onik ( apld ) [ 8 ] , percutaneous laser disc decompression ( pldd ) , intradiscal electrothermal therapy ( idet ) , percutaneous coblation nucleoplasty , percutaneous dekompressor lumbar discectomy , and intradiscal oxygenozone ( o2 - o3 )  . 
differentiation between radicular pain and facet syndrome or la lombalgia una delle affezioni pi comuni della colonna vertebrale , ed la causa pi frequente di assenza dal lavoro nei paesi industrializzati [ 1 ]  . 
circa l80% degli adulti soffre di almeno un episodio di lombalgia nella propria vita , mentre il 55% affetto da mal di schiena associato a sindrome radicolare [ 1 ]  . 
la sintomatologia dolorosa pu risolversi spontaneamente in oltre il 60% dei pazienti , con riduzione dellernia rilevata alla tc o alla rm entro 89 mesi dalla comparsa dei sintomi [ 2 , 3 ]  . nelle casistiche chirurgiche il tasso di successo a breve termine dopo trattamento chirurgico di ernia del disco intorno all85%90% con una incidenza di recidiva erniaria vera del 2%6% . 
tale percentuale di successo chirurgico ( 85%90% ) a breve termine tende a scendere intorno al 70%80% nel follow - up a lungo termine ( pi di 6 mesi ) in relazione alla comparsa spesso dei sintomi legati alla sindrome da fallimento chirurgico ( fbss ) [ 4 ]  . 
questa spesso caratterizzata da recidiva e / o da cicatrice ipertrofica che comporta una sintomatologia severa nel 20% dei casi e una vera e propria fbss nel 15% dei pazienti [ 5 ]  . per questo motivo latteggiamento dei neurochirurghi divenuto sempre meno aggressivo e negli stati uniti si stima che tra tutti i pazienti affetti da lombalgia / lombosciatalgia solo il 3%4% viene sottoposto ad intervento chirurgico [ 6 ]  . la patogenesi del dolore lombare multi - fattoriale . 
infatti , alle cause meccaniche - compressive sulla radice nervosa , si associano sia una reazione infiammatoria cellulomediata che una non immuno - mediata , secondaria a fattori bioumorali [ 7 ]  . 
a team approach to be able to guarantee the best possible long - term outcome this paper describes our experience with minimally invasive intradiscal , intraforaminal and periradicular o2 - o3 injection ( o2 - o3 chemodiscolysis ) , illustrates the procedure and patient selection and exclusion criteria , and discusses the benefits and complications of the technique compared with surgical treatment . materials and methods between january 2000 and december 2006 , 2 , 900 patients ( 1 , 753 men and 1 , 147 women aged 1986 years ) were treated with o2 - o3 injection : 2 , 650 of them had soft - disc herniation , 250 had calcified herniation , 350 had multiple herniations and 200 had fbss . 
exclusion criteria were extruded disc herniation and / or free disc fragment , severe motor impairment of the limb and / or sphincter disorders , hyperalgesic sciatica and progressive neurological impairment of the affected limb . 
clinical : low back pain and / or sciatica refractory to medical management , physiotherapy and other treatments ( manipulations , acupuncture , etc . ) lasting at least 23 months 2 . 
neuroradiological : ct and / or mri evidence of small or medium - size disc herniations consistent with the symptoms , with or without degenerative disease of the discvertebral unit all procedures were carried out with ct guidance and the patient in the prone position to better evaluate the distribution of the injected gas mixture and the possible presence of a retropsoas bowel loop to be avoided during the procedure . 
when technically and anatomically feasible , all patients received intradiscal and periganglionic treatment , whereas those with noncompressive inflammatory radiculopathy received intraforaminal treatment . after locating the diseased disc with a scanogram , an 18to 20gauge needle 710 cm long was inserted in the nucleus pulposus through a paravertebral oblique access . 
lavorare in equipe per poter garantire al paziente il miglior trattamento possibile a lungo termine . scopo di questo lavoro di illustrare la tecnica mininvasiva di infiltrazione di ossigeno - ozono ( chemiodiscolisi con miscela di o2 - o3 ) intradiscale , intraforaminale e periradicolare , riportando la nostra esperienza , discutendone la modalit di esecuzione , i criteri di selezione ed esclusione dei pazienti affetti da ernia discale lombare , dimostrando vantaggi ed complicanze che il trattamento comporta confrontato al trattamento chirurgico . materiali e metodi da gennaio 2000 a dicembre 2006 , sono stati trattati con infiltrazione o2 - o3 terapia 2900 pazienti ( 1753 maschi , 1147 femmine ) di et compresa tra 19 e 86 anni : 2650 erano affetti da ernie molli , 250 da ernie calcifiche , 350 presentavano ernie multiple e 200 erano affetti da fbss . 
i criteri di esclusione sono stati : ernia discale espulsa e / o frammento erniario libero , grave deficit motorio dellarto e / o disturbi sfinterici , sciatalgia iperalgica , deficit neurologico progressivo dellarto interessato . 
neuroradiologici ( tc e / o rm ) : visualizzazione di ernie discali di piccole e medie dimensioni adeguate alla sintomatologia complicate o meno da patologia degenerativa dellunit disco - vertebrale . la tecnica stata eseguita sempre sotto guida tc , posizionando il paziente . 
the o2 - o3 gas mixture was injected into the disc ( 34 ml ) and the foramen ( 10 ml )  . leventuale presenza di unansa retro - psoica , da evitare durante il trattamento . 
la concentrazione somministrata per trattare il disco di 3040 micron / ml ed risultata essere da studi sperimentali ottimale per disidratare il nucleo e ridurre linfiammazione [ 8 ]  . 
nel caso del disco l5 - s1 , la procedura a volte stata pi difficoltosa in quanto per raggiungere il disco specifico talvolta occorreva unulteriore inclinazione dellago di 30 in direzione cranio - caudale . 
il paziente stato rivalutato clinicamente a distanza di un mese dal trattamento per decidere linvio ad un centro di fisioterapia ( nel caso di un significativo miglioramento clinico ) oppure lesecuzione di un secondo trattamento ( in caso di successo parziale con miglioramento delle condizioni cliniche del 50% )  . 
secondo la visual analogyc scale , i risultati ottenuti sono stati buoni , con una riduzione superiore a 3 punti rispetto alla valutazione iniziale ai controlli a distanza nell85% dei casi . secondo la oswestry disability scale , abbiamo notato una riduzione percentuale significativa ( intorno al 30% ) nei controlli tardivi . 
3a rm assiale t2w ernia discale postero - laterale destro a livello di l5 - s1 , b , c rm assiale t2w follow - up dopo 6 mesi dalla terapia di infiltrazione di o2 - o3 intradiscale . the concentration administered was 3040 m / ml , a concentration that has been experimentally demonstrated to be optimal for dehydrating the disc and reducing inflammation [ 8 ]  . 
no neurological or infectious le tecniche mini - invasive percutanee per il trattamento dellernia discale lombare introdotte nella pratica clinica nel corso degli anni sono state numerose : chemiodiscolisi con chimopapaina ; nucleoaspirazione secondo onik ( apld ) [ 8 ] ; discectomia percutanea laser ( pldd ) ; terapia elettrotermica intradiscale ( idet ) ; nucleoplastica percutanea in coblazione ; discectomia lombare percutanea dekompressor ; o2 - o3 intradiscale . 
richiedono un breve periodo di ospedalizzazione e , non intervenendo direttamente sul canale spinale , evitano o riducono radiol med ( 2008 ) 113 : 695706 table 1 modified mac nab classification successful treatment excellent disappearance of symptoms complete recovery of working and sports activities good occasional episodes of low back pain or sciatica sufficient improvement in symptoms limitation of normal physical activity tabella 1 metodo mac nab modificato successo eccellente scomparsa della sintomatologia dolorosa completa ripresa dellattivit fisica e lavorativa buono occasionali episodi di mal di schiena o sciatica failure of treatment poor insufficient improvement of symptoms periodic use of analgesic medications limitation of physical activity no result no improvement of symptoms need for surgical operation negative worsening of symptoms need for surgical operation insuccesso mediocre scarso miglioramento della sintomatologia dolorosa assunzione periodica di antidolorifici limitazione dellattivit fisica nessun risultato nessun miglioramento della sintomatologia dolorosa necessit di intervento chirurgico sufficiente miglioramento della sintomatologia dolorosa limitazione dellattivit fisica normale negativo peggioramento della sintomatologia dolorosa necessit di intervento chirurgico complications were reported during the short - term or longterm follow - up . vas scores indicated good results , with a reduction of more than three points at long - term follow - up compared with baseline in 85% of cases . 
in fbss excellent : 25% good or sufficient : 35% moderate or poor : 40% discussion numerous minimally invasive percutaneous techniques have been introduced into clinical practice for the treatment le complicanze post - chirurgiche quali ad esempio le infezioni e le cicatrici ipertrofiche . 
 il razionale su cui si basano tutte le tecniche mini - invasive percutanee di ridurre mediante azioni differenti la pressione intradiscale , creando conseguentemente lo spazio necessario per la retropulsione o digestione del disco . 
these include chymopapain chemodiscolysis , apld according to onik [ 8 ] , pldd , idet , percutaneous coblation nucleoplasty , percutaneous dekompressor lumbar discectomy , and intradiscal o2 - o3 . all of them offer satisfactory clinical outcomes combined with good patient compliance and a low cost . 
they all require a short hospital stay and , by avoiding the spinal canal , eliminate or reduce the risk of postoperative infections and hypertrophic scarring , which is often responsible for the recurrence of symptoms [ 4 , 5 ]  . 
chymopapain chemodiscolysis was the first percutaneous technique to be used in the treatment of disc herniation , with the earliest clinical series by smith dating back to more than 40 years ago [ 9 ]  . 
the technique consists of the intradiscal injection of chymopapain , a proteolytic enzyme derived from the papaya fruit , which catalyses the hydrolysis of the nucleus pulposus proteoglycans [ 10 ]  . 
the circular fibres of the annulus have a reduced ability to contain the nucleus in the presence of increased intradiscal pressure . once injected into the disc , chymopapain induces dehydration of the nucleus pulposus with consequent reduction of pressure on the annulus and creation of the space necessary for retropulsion . 
despite strong initial interest , the technique lost favour due to the patient selection criteria that limited eligibility to contained disc herniations to avoid contact between the proteolytic enzymes , the dural sac and the nerve roots [ 10 ]  . apld was introduced by onik in 1985 [ 8 ]  . 
it uses a device called a nucleotome , consisting of a pneumatic pump powered by compressed air or nitrogen , which is connected to an aspiratingcutting probe with an outer diameter of only 2 mthe probe is introduced into the disc under fluoroscopic guidance , and nucleus pulposus material is suctioned through a side opening in the probe , cut off with a cutting device and aspirated through the probe [ 11 ]  . pldd , introduced by choy in the mid 1980s [ 13 ] , uses a very thin optical fibre connected to a laser . 
the optical fibre is introduced with a thin needle into the nucleus pulposus , where energy from a solid - state source is released to vaporise a portion of the nucleus and hence decompress the disc [ 12 ]  . idet , introduced by saal in 1997 [ 15 ] , is only indicated in discogenic low back pain such as bulging disc or contained herniation . 
heating of the posterior annulus reduces symptoms and stabilises the disc lesion by restructuring the collagen fibres , stiffening the disc , sealing annular tears and ablating nerve endings [ 13 ]  . tipo di paziente da sottoporre al trattamento : affetto cio da ernie discali contenute al fine di evitare il contatto tra enzimi proteolitici , sacco durale e radici nervose [ 10 ]  . la discectomia lombare percutanea automatizzata ( alpd ) , introdotta da onik nel 1985 [ 8 ] , utilizza , sotto controllo fluoroscopico , uno strumento detto nucleotomo , composto da una pompa pneumatica che funziona ad aria o ad azoto compresso a cui viene collegata una sonda aspirante - taglienteche ha un diametro esterno di soli 2 mm . una volta introdotta nel disco , la sonda permette di aspirare porzioni di nucleo polposo frammentato dalla lama posta coassialmente allinterno della sonda , drenandole allesterno [ 11 ]  . la discectomia percutanea laser ( pdll ) , introdotta da daniel s.j. 
questa , introdotta nel nucleo polposo tramite un ago sottile , determina mediante fonte di energia allo stato solido una vaporizzazione di una quota di nucleo polposo con conseguente decompressione della pressione intradiscale [ 12 ]  . 
essa agisce sulla parte posteriore del anulus fibroso utilizzando una resistenza scaldata a 90c posta alla estremit di un catetere elettro - termico flessibile circonferenzialmente introdotto lungo il confine tra nucleo polposo e anulus . 
il processo di riscaldamento dellanulus posteriore riduce la sintomatologia e stabilizza la lesione discale attraverso la riorganizzazione delle fibre di collagene , il rafforzamento del disco , lalterazione delle fessure anelliformi , e lablazione dei nocicettori [ 13 ]  . la nucleoplastica percutanea in coablazione prevede temperature in radiofrequenza a basse lablazione ( 5070c ) del nucleo polposo attraverso un elettrodo termocoagulatore ( perc - d coblation probe ) introdotto sotto fluoroscopia . 
the physical principle underlying the technique , which also limits its utilisation , is that of a closed hydraulic systean intervertebral disc with an intact annulus behaves like a closed hydraulic space where removal of even a small amount of material generates a large decrease in internal hydraulic pressure . the results obtained in controlled trials report relief of pain for least 6 months in 70% of cases [ 14 , 15 ]  . percutaneous dekompressor lumbar discectomy uses a 1.5 - mm helical decompression probe ( stryker , kalamazoo , mi , usa ) , which is advanced like a screw into the nucleus pulposus through an outer cannula . 
 removal of a few cubic centimetres of disc material results in a significant decrease in pressure on the peripheral disc , with resolution of the disc - nerve root conflict , and greater than 70% reduction in symptoms in 70%72% of patients [ 16 , 17 ]  . our attention has chiefly focused on minimally invasive , percutaneous , intradiscal , periganglionic and periradicular injection of oxygen - ozone ( o2 - o3 therapy ) , because we found it faster and easier to perform than other techniques . also , it has a low complication rate , it can be repeated and it is applicable to a variety of patients with lumbar disc herniation provided they are symptomatic and the symptoms are consistent with the radiological findings . only recently adopted in europe , chiefly in italy , germany and spain [ 7 ] , the technique uses ozone , an unstable , colourless , irritant gas that has a pungent odour and strong antioxidant - stimulating capabilities as well as antiseptic , disinfectant and antiviral properties . 
it is prepared and used as required by transforming a small amount of medical o2 into o3 by means of appropriate generators . the rationale for o2 - o3 therapy is that the patients pain is caused by mechanical compression of the nerve root associated with periganglionic and periradicular inflammatory responses [ 18 , 19 ]  . 
attraverso il motore rotante applicato alla sonda , unitamente ai movimenti della sonda stessa prodotti dalloperatore , il sistema permette di rimuovere frammenti del nucleo erniato che risalgono la sonda e vengono espulsi allesterno . la rimozione di pochi cm3 di materiale discale esita in significativo decremento della pressione sulla porzione periferica del disco , risolvendo il conflitto disco radicolare con una riduzione della sintomatologia dolorosa di oltre il 70% nel 70%72% dei pazienti trattati [ 16 , 17 ]  . la nostra attenzione si rivolta prevalentemente al trattamento percutaneo mininvasivo di infiltrazione intradiscale , perigangliare e periradicolare di ossigeno - ozono ( o2 - o3 terapia ) in quanto crediamo che , a confronto delle altre tecniche , sia la pi rapida e facile da eseguire con basso tasso di complicanze , facile riproducibilit ma soprattutto estendibile a pi pazienti affetti da ernia discale lombare , purch siano sintomatici ed a tale sintomatologia corrisponda un quadro radiologico congruo . diffusasi solo di recente in europa ( principalmente in italia , germania e spagna [ 7 ] ) questa tecnica utilizza lozono , un gas instabile , incolore , irritante , con un odore pungente che ha un forte potere anti - ossidante , antisettico , disinfettante ed antivirale . 
 il razionale della tecnica o2 - o3 terapia si basa sul principio che il dolore causato dalla compressione meccanica sulla radice nervosa cui si associano fenomeni infiammatori perigangliari e periradicolari [ 18 , 19 ]  . 
questo effetto stato confermato dai rilievi istologici sui frammenti discali precedentemente trattati con o2 - o3 terapia e rimossi durante interventi di microdiscectomia che confermano la disidrazione della matrice fibrillare del nucleo polposo . 
 studi sperimentali hanno dimostrato che una miscela di o2 - o3 alla concentrazione usata per liniezione intradiscale produce gli stessi effetti degli steroidi sulla produzione di citochine e di conseguenza riduce il dolore [ 21 ]  . 
si di dimostrato , altres , che iniettato in alte dosi e concentrazioni negli spazi sub - aracnoidei non determina nessun tipo di alterazione del midollo spinale o del liquido cerebro - spinale 704 radiol med ( 2008 ) 113 : 695706 venous stasis leading to increased local oxygen supply and reduced ischaemia and nerve root oedema 3 . 
this effect has been confirmed by histological studies of fragments of discs treated with o2 - o3 therapy and removed during microdiscectomy that showed dehydration of the fibrillary matrix of the nucleus pulposus . experimental studies have shown that an o2 - o3 gas mixture at the concentration used for intradiscal injection has the same effect as steroids on inhibiting cytokine production and hence on relieving pain [ 21 ]  . 
it has also been demonstrated that a o2 - o3 gas mixture injected at high doses and concentrations into the subarachnoid spaces does not cause damage to the spinal cord or cerebrospinal fluid [ 22 ]  . 
the therapeutic efficacy of o2 - o3 therapy in the treatment of nerveroot impingement due to disc herniation has long been known , with reported success rates varying between 70% and 80% and no complications [ 2330 ]  . a recent randomised controlled study [ 31 ] comparing surgical vs . 
long - term conservative treatment in patients with sciatica due to herniated disc demonstrated that 39% ( 55 / 142 ) of patients assigned to conservative treatment underwent surgery during the first year because of intractable pain , and 1.8% of them had recurrent sciatica leading to a second surgical intervention . 
in a series of approximately 3 , 000 patients treated with o2 - o3 therapy , andreula et al . [ 32 ] reported success rates of 77% in l4l5 and l5s1 herniations , 80% in degenerative spinal disease complicated by disc herniation , 69% in multiple disc herniations and 65% in fbss , with no early or late neurological or infectious complications . 
 [ 33 ] achieved a higher success rate with o2 - o3 therapy combined with intraforaminal and intradiscal steroid and anaesthetic injection compared with steroid injection alone , probably because of the longer - lasting effect of o2 - o3 compared with steroids . 
 [ 20 ] reported a 78.3% success rate ( 235 / 300 ) in patients treated with o2 - o3 therapy and periganglionic steroid injection compared with a 70.3% rate ( 211 / 300 ) in those treated with o2 - o3 therapy alone ; complications occurred in 2 / 235 patients and consisted of episodes of impaired sensitivity in the lower limb on the treated side , which resolved spontaneously within 2 h . 
 [ 35 ] reported an 80% success rate at short - term followup ( 6 months ) and a 75% success rate at long - term followup ( 18 months ) , with no major or minor side effects . in our series , we achieved success rates of 75%80% in [ 22 ]  . 
lefficacia terapeutica dello2 - o3 terapia nel trattamento dei conflitti disco - radicolari da ernia discale nota da tempo e in letteratura viene riportata una percentuale di successo terapeutico variabile tra il 70% e 80% , e non vengono riportate complicanze [ 2330 ]  . un recente studio randomizzato [ 31 ] con follow - up di un anno di confronto trattamento chirurgico versus trattamento conservativo ha dimostrato come il 39% ( 55 su 142 pazienti ) dei pazienti affetti da sciatalgia da ernia discale sia stato poi sottoposto a un primo intervento chirurgico con una complicanza di reintervento a 1 anno del 1 , 8% . 
andreula [ 32 ] su unesperienza di circa 3000 pazienti trattati con o2 - o3 terapia riporta un successo della metodica di circa il 77% nei pazienti affetti da ernia discale l4l5 e l5s1 , di circa l80% nei pazienti affetti da patologia degenerativa del rachide complicata con ernia discale , di circa il 69% nei pazienti affetti da ernie discali multiple e di circa il 65% nei pazienti affetti da fbss ; senza complicanze neurologiche o infettive precoci o tardive . 
 [ 33 ] riportano un successo maggiore della terapia con infiltrazione di o2 - o3 associata a iniezione di steroidi e anestetici locali , a sede intraforaminale e intradiscale rispetto alla sola infiltrazione di steroidi , a causa presumibilmente dellazione pi duratura nel tempo dello2 - o3 rispetto a quella temporanea degli steroidi . 
 [ 34 ] , in uno studio randomizzato e controllato su un totale di 306 pazienti affetti da low back pain e sciatica , sottoposti a o2 - o3 terapia o infiltrazione di steroidi periradicolare , hanno dimostrato una maggiore e pi rapida efficacia del trattamento o2 - o3 terapia versus la sola infiltrazione di steroidi periradicolare . 
 [ 20 ] hanno riportato un successo nel 78 , 3% dei pazienti su 235 pazienti sottoposti a o2o3 terapia e steroidi perigangliare per leffetto cumulativo delle due sostanze rispetto alloutcome rilevato con il solo trattamento o2 - o3 terapia , riportando come complicanza in 2 / 235 pazienti trattati la perdita transitoria della sensibilit allarto inferiore ipselaterale al trattamento risolta spontaneamente 2 ore dopo . 
 [ 35 ] su 820 pazienti sottoposti a con o2 - o3 terapia hanno riportato un successo 80% dei casi nei di follow - up a breve termine ( 6 mesi ) e del 75% dei casi trattati nel follow - up a lungo termine ( 18 mesi ) , senza comparsa di effetti collaterali maggiori o minori . nella nostra casistica , abbiamo ottenuto un successo variabile tra il 75%80% per le ernie discali molli , del 70% per le ernie discali multiple e del 55% per la sindrome da fallimento chirurgico ( fbss ) , senza riscontrare alcuna complicanza neurologica o infettiva nel follow - up breve o lungo termine . 
dai dati della letteratura , e secondo la nostra casistica , riteniamo che , sulla base del meccanismo dazione della o2 - o3 terapia , questa metodica risulti essere una tecnica versatile e pi facilmente eseguibile e riproducibile sul paziente sintomatico affetto da ernia discale lombare eccetto per che nei casi di : radiol med ( 2008 ) 113 : 695706 soft disc herniations , 70% in multiple herniations and 55% in fbss without any early or late neurological or infections complications . 
on the basis of our results and the literature data , we believe o2 - o3 therapy to be a versatile technique that is easy to perform and reproduce on patients with symptomatic lumbar disc herniation , except in cases of : 1 . 
hyperalgesic sciatica the last three conditions listed are in fact absolute indications for urgent surgical treatment . a further advantage of percutaneous o2 - o3 injection is that it can be extended to patients with fbss , who can benefit from the action of ozone on chronic inflammation and venous stasis , and to those with large or free fragments but without significant clinical symptoms . conclusions cost - effectiveness and the absence of complications make o2 - o3 chemodiscolysis with periradicular and periganglionic injection a reliable and competitive treatment compared with other percutaneous techniques . 
low back pain and sciatica are common complaints , and surgical treatment is only indicated in urgent cases or in patients who have undergone medical and physical therapy for at least 8 weeks . 
il paziente affetto da lombalgia e da lombosciatalgia una evenienza molto frequente e la terapia chirurgica trova indicazione nei casi urgenti o in casi selezionati dopo terapia medica e fisica per almeno 8 settimane . 
giaccone , via del vespro 127 , 90127 palermo , italy 2department of radiology , irccs fondazione santa lucia , rome , italy 3department of radiology and cardiology , university hospital , parma , italy 4department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands correspondence to : g . 
multiphase reconstruction data sets were obtained with a retrospective electrocardiogram ( ecg ) - gated 40 - mdct coronary angiography scan from 0% to 95% every 5% of the r - r interval . 
in group a , the optimal reconstruction windows were at 70% ( 55 / 110 , 71 / 110 and 69 / 110 for the right coronary artery , left anterior descending and the left circumflex , respectively ) and 75% ( 26 / 110 , 28 / 110 and 28 / 110 , respectively ) of the r - r interval . 
in group b , a wide range of reconstruction windows were employed , both in the end - systolic phase at 40% ( 32 / 60 , 18 / 60 and 17 / 60 , for the right coronary artery , left anterior descending and circumflex , respectively ) and diastolic phases at 70% ( 12 / 60 , 22 / 60 and 19 / 60 , respectively )  . 
nel gruppo a le fasi di ricostruzione ritenute ottimali sono state il 70% ( 55 / 110 , 71 / 110 e 69 / 110 , rispettivamente , per la coronaria destra cdx per linterventricolare anteriore iva e per la circonflessa cx ) ed il 75% ( 26 / 110 , 28 / 110 e 28 / 110 , rispettivamente )  . nel gruppo b stata utilizzata un ampia gamma di ricostruzioni , in particolare al 40% ( 32 / 60 , 18 / 60 e 17 / 60 , rispettivamente per la cdx , per liva e per la cx ) ed al 70% ( 12 / 60 , 22 / 60 e 19 / 60 , rispettivamente )  . 
reconstruction phases from 30% to 45% are advisable for higher heart rates . keywords multislice computed tomography coronary angiography retrospective ecg gating heart rate diastolica consentono spesso una valutazione ottimale con fc65 bpla scelta delle fasi sistoliche ( 30%45% ) consigliabile , invece , per fc pi elevate . parole chiave tomografia computerizzata multistrato angiografia coronarica sincronizzazione retrospettiva allecg frequenza cardiaca introduction introduzione coronary angiography with multidetector - row computed tomography ( mdct ) is finding increasing use in routine clinical practice as a noninvasive diagnostic tool for evaluating coronary arteries . 
scanners with increasing spatial and temporal resolution have been developed over the years [ 16 ]  . however , regardless of their diagnostic performance , artefacts caused by heart motion are still the greatest obstacle in clinical practice , given their negative influence on the diagnostic accuracy of the technique . image quality is highly dependent on heart rate ( hr ) and the reconstruction window selected using retrospective electrocardiogram ( ecg ) gating . 
various studies have evaluated the optimal reconstruction window with 4 - slice [ 79 ] , 16 - slice [ 1012 ] and recently 64 - slice ct [ 13 ]  . 
increasing temporal resolution could lead to use of a single reconstruction window , thus limiting the amount of data to be reconstructed and therefore the amount of data to be archived , as well as minimising the dose of ionising radiation delivered to the patient [ 14 ]  . the aim of our study was to evaluate the influence of hr on the choice of the optimal reconstruction window for reporting an examination performed with 40 - slice mdct coronary angiography . langiografia coronarica mediante tomografia computerizzata multistrato ( ac - tcms ) viene sempre pi spesso utilizzata nella routine clinica come strumento diagnostico non invasivo per la valutazione delle arterie coronarie . 
tuttavia , a prescindere dal miglioramento della performance diagnostica , gli artefatti da movimento cardiaco continuano a costituire la pi grossa difficolt della routine clinica determinando un peggioramento dellaccuratezza diagnostica della metodica . la qualit dellimmagine fortemente dipendente dalla frequenza cardiaca ( fc ) e dalla finestra temporale di ricostruzione selezionata utilizzando il gating retrospettivo allecg . 
numerosi studi hanno valutato lintervallo ottimale di ricostruzione con la tc a 4 strati [ 79 ] , con la tc a 16 strati [ 1012 ] e recentemente con la tc a 64 strati [ 13 ]  . 
laumento della risoluzione temporale potrebbe condurre in futuro allimpiego di un singolo intervallo di ricostruzione , ridimensionando lammontare dei dati ricostruiti e , quindi , gli spazi di archiviazione , e minimizzando la dose di radiazioni ionizzanti assorbita dal paziente [ 14 ]  . scopo del presente lavoro valutare linfluenza della fc nella scelta della fase di ricostruzione ottimale per la refertazione di un esame di ac - tcms a 40 strati . materials and methods study population materiali e metodi popolazione studiata between february and may 2006 , 170 consecutive patients ( 114 men , 56 women ; mean age 6011.3 years , range 1980 years ) underwent 40 - mdct coronary angiography ( brilliance 40 , philips medical systems , cleveland , oh , usa )  . indications for examination were stable angina ( 61 ) , atypical chest pain ( 37 ) , unstable angina ( 5 ) , follow - up of proximal stents ( 20 ) , follow - up of bypass grafts ( 30 ) , elevated cardiovascular risk ( patients with metabolic syndrome 11 ) , suspected coronary anomalies ( 2 ) , suspected cardiac masses ( 2 ) and preoperative planning for valve replacement ( 2 )  . nel periodo compreso tra febbraio e maggio 2006 , 170 pazienti ( 114 uomini , 56 donne ; et media 6011 , 3 anni , range 1980 anni ) consecutivi sono stati sottoposti ad angiografia coronarica tc a 40 strati ( brilliance 40 , philips medical systems , cleveland , ohio , usa )  . 
i pazienti hanno eseguito lindagine per angina stabile ( n = 61 ) , dolore toracico atipico ( n = 37 ) , angina instabile ( n = 5 ) , follow - up di stent prossimali ( n = 20 ) , follow - up di by - pass ( n = 30 ) , rischio 646 radiol med ( 2008 ) 113 : 644657 the normally recognised inclusion criteria for mdct coronary angiography are sinus cardiac rhythm with < 70 beats per minute ( bpm ) and ability to maintain breath - hold for at least 15 s . 
for clinical reasons , our study also included patients with a mean hr 70 bpunless contraindicated , patients with an initial hr 70 bpm ( 98 ; 57.6% ) received a 20 - mg oral dose of propranolol ( inderal , astrazeneca reim , reims , cedex , france ) 30 min prior to the examination , and the entire population received a 2.5 - mg dose of diazepam ( tranquirit , aventis pharma , waterford , ireland )  . patients with demonstrated refractoriness to a single dose of beta - blockers received an additional dose of the same agent ( 73 ; 43% )  . 
tube current modulation was not selected by the operator . a bolus of 120 ml of nonionic iodinated contrast material ( iomeprol , iomeron 400 , bracco , milan , italy ) was injected at a flow rate of 5 ml / s with an automatic power injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an 18gauge needle cannula with right antecubital access . 
to optimise intraluminal enhancement of the coronary arteries , the beginning of the scan was synchronised by using the bolustracking technique ( philips medical systems , cleveland , ohio , usa ) with a region of interest ( roi ) at the level of the ascending aorta . 
the scan began automatically with a delay of cardiovascolare elevato ( pazienti affetti da sindrome metabolica , n = 11 ) , sospette anomalie coronariche ( n = 2 ) , sospette masse cardiache ( n = 2 ) , in previsione di un intervento di sostituzione valvolare ( n = 2 )  . 
 i criteri di inclusione normalmente riconosciuti per la ac - tcms sono : ritmo cardiaco sinusale e < 70 battiti per minuto ( bpm ) , e capacit di mantenere unapnea inspiratoria per almeno 15 secondi . 
per ragioni cliniche nel nostro studio sono stati inclusi anche pazienti con frequenza cardiaca ( fc ) media 70 bpnei pazienti che presentavano una fc media inizialmente 70 bpm ( n = 98 pazienti , 57 , 6% ) , a meno di controindicazioni , sono state somministrate 30 minuti prima della scansione , una dose orale di 20 mg propanololo cloridrato ( inderal , astrazeneca reims , reims , cedex , francia ) , ed allintera popolazione studiata una dose di 2 , 5 mg di diazepam ( tranquirit , aventis pharma , waterford , irlanda )  . 
i criteri di esclusione sono stati : rifiuto di fornire il consenso informato , grave compromissione renale ( creatininemia > 120 mol / l ) , allergia nota ai mezzi di contrasto iodati , possibile gravidanza , presenza di aritmie ipercinetiche ( ad esempio fibrillazione atriale , extrasistolia , ecc . ) , compromissione della funzione respiratoria , disordini tiroidei , stato clinico instabile o marcata insufficienza cardiaca . a tutti i pazienti sono state spiegate le diverse fasi della procedura desame e la corretta modalit di esecuzione dellapnea inspiratoria . 
 nonostante la somministrazione di 2040 mg di - bloccante , in 20 pazienti la fc media registrata durante la scansione si mantenuta > 70 bp i pazienti ( frequenza cardiaca media 62 , 99 , 3 bpm , range 4294 bpm ) sono stati suddivisi in due gruppi , impiegando un valore soglia di 65 bpm ( gruppo a : fc65 bpm ; gruppo b : fc > 65 bpm )  . parametri di scansione e di ricostruzione tutte le scansioni sono state effettuate con una tc a 40 strati ( brilliance 40 , philips medical systems , cleveland , ohio , usa )  . 
stata eseguita una quantificazione del calcio coronarico mediante gating prospettico al 70% dellintervallo r - r , con i seguenti parametri di scansione : fov 150200 mm , kv 120 , mas 70 , spessore 2 , 5 mm e sovrapposizione del 50% . le scansioni angiografiche sono state effettuate con i seguenti parametri : modalit di sincronizzazione retrospettiva tracciato ecg , numero di detettori / collimazione 400 , 625 mm , voxel 0 , 34 mm3 ( risoluzione isotropica ) , tempo di rotazione 420 ms ( risoluzione temporale effettiva , con algoritmo di ricostruzione lineare a 180 , 210 ms ) , avanzamento / rotazione 11 , 9 mm / s ( pitch 0 , 2 ) , voltaggio del tubo radiogeno 120 kv , tensione del tubo radiogeno 1035 mas , radiol med ( 2008 ) 113 : 644657 8 s after the threshold of 120 hu was reached within the roi . a retrospective reconstruction was performed for each coronary artery ( right coronary artery rca ; left anterior descending coronary artery lad : left circumflex coronary artery lcx ) in the various phases of the cardiac cycle , each 5% of the r - r interval from 0% to 95% , for a total of 20 data sets . 
the reconstructions were performed with the following parameters : slice thickness 0.8 mm , reconstruction increment 0.4 mm , medium ( cb ) and sharp ( cc ) convolution kernels . 
the data sets were transferred to a dedicated workstation ( extended brilliancetm workspace , version 3.0.1.3200 , philips medical systems , cleveland , ohio , usa )  . data analysis data analysis was performed on all segments of the coronary arteries with a diameter 1.5 m all reconstructed images were evaluated by two radiologists with level - 3 experience in mdct coronary angiography by using multiplanar reconstructions ( mip ) and maximum intensity projections ( mip ) [ 15 ]  . the data sets retrospectively reconstructed every 5% of the r - r interval were compared , and the data set with the best image quality per individual vessel was identified . 
for each mdct coronary angiography examination , a global assessment was made of image quality in relation to a single reconstructed data set or the integration of several data sets . 
a four - point scale was used to evaluate the coronary arteries with a diameter 1.5 mm : absence of motion artefacts and clear outline of the vessel ( grade 1 ) ; minor artefacts with minimal blurring ( grade 2 ) ; blurring artefacts without interruption in the course of the vessel ( grade 3 ) ; artefacts with severe doubling / interruption of the course of the vessel ( grade 4 ) [ 16 ]  . 
the operators performed all evaluations by consensus . statistical analysis statistical analysis was performed with a dedicated software package ( statistica , version 5.0 , statsoft italia , vigonza , pd , italy )  . 
an estimation was made of the statistical difference between the two groups in terms of age ( t test ) , agatston calcium score ( t test ) , gender and administration of beta - blockers ( fishers exact test )  . 
dalloperatore non stata scelta la modalit di modulazione dellamperaggio del tubo radiogeno . un bolo di 120 ml di mezzo di contrasto iodato non - ionico ( iomeprol , iomeron 400 , bracco , milano , italia ) stato iniettato con un flusso di 5 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , pa , usa ) collegato ad unagocannula da 18 gauge , posizionata in una vena antecubitale destra . 
allo scopo di ottimizzare lenhancement intraluminale dei vasi arteriosi coronarici la sincronizzazione dellinizio della scansione con il passaggio del bolo di mezzo di contrasto stata eseguita mediante tecnica del bolus tracking ( philips medical systems , cleveland , ohio , usa ) , con una roi ( region of interest ) posizionata al livello dellaorta ascendente . 
la scansione partita automaticamente con un ritardo di 8 secondi dopo il raggiungimento allinterno della roi di una soglia di 120 uh . per ogni coronaria ( arteria coronaria destra , cdx ; arteria interventricolare anteriore , iva ; arteria circonflessa , cx ) stata effettuata una ricostruzione retrospettiva nelle varie fasi del ciclo cardiaco ogni 5% dellintervallo r - r dallo 0% al 95% per un totale di 19 dataset . 
le ricostruzioni sono state effettuate con i seguenti parametri : spessore 0 , 8 mm , incremento 0 , 4 mm , filtri di convoluzione medio ( cb ) e sharp ( cc )  . 
i dataset sono stati trasferiti su una workstation dedicata ( extended brilliancetm workspace , versione 3.0.1.3200 , philips medical systems , cleveland , ohio , usa )  . analisi dei dati lanalisi stata effettuata in tutti i segmenti di arterie coronarie con diametro 1 , 5 mtutte le immagini ricostruite sono state indipendentemente valutate da due radiologi con esperienza di livello 3 in ac - tcms mediante riformattazioni multiplanari ( mpr ) e proiezioni di massima intensit ( mip ) [ 15 ]  . tra i dataset ricostruiti retrospettivamente ogni 5% dellintervallo r - r , stato identificato quello con la migliore qualit di immagine per singolo vaso coronarico ed in grado di consentire lottimale espressione di un giudizio diagnostico . 
stata utilizzata una scala in gradi per la valutazione delle arterie coronarie con diametro 1 , 5 mm : assenza di artefatti di movimento con chiara delineazione del vaso ( grado 1 ) ; artefatti minori con minimo blurring ( grado 2 ) ; artefatti da blurring senza discontinuit di decorso dei vasi ( grado 3 ) ; artefatti severi con sdoppiamento / discontinuit dei vasi ( grado 4 ) [ 16 ]  . 
only six patients ( 3.5% ) with a mean hr > 65 bpm during the scan were considered grade 4 , as none of the available data sets allowed an acceptable diagclinica . 
tutte le valutazioni sono state svolte in accordo dagli operatori . analisi statistica lanalisi statistica stata eseguita con un software dedicato ( statistica , versione 5.0 , statsoft italia , vigonza , pd , italia )  . 
stata stimata la differenza statistica tra i due gruppi per et ( test t di student ) , calcium score calcolato secondo il sistema di agatston ( test t di student ) , sesso e somministrazione di - bloccanti ( test esatto di fisher )  . 
in group a , the optimal reconstruction windows for diagnostic quality images were at 70% ( 55 / 110 , 71 / 110 and 69 / 110 for the rca , lad and lcx , respectively ) and 75% ( 26 / 110 , 28 / 110 and 28 / 110 , respectively ) of the r - r interval . 
a prevalence of the end - systolic phase was noted for the evaluation of the rca ( 65% )  . at the same time , a significant number of reconstructions in the end - systolic phase were optimal for the evaluation of the lad ( 43.3% ) and the lcx ( 43.3% ) ( table 3 )  . 
only six examinations ( mean hr during the scan of 82 , 83 , 84 , 92 , 94 and 94 bpm ) were compromised by severe artefacts ( grade 4 ) and were therefore assessed as nondiagnostic . risultati nessuna differenza significativa stata riscontrata tra i due gruppi per et ( gruppo a : 60 , 710 , 7 anni ; gruppo b : 5912 , 3 anni ; p = 0 , 29 ) , calcium score calcolato secondo il sistema di agatston ( gruppo a : 185278 ; gruppo b 205352 ; p = 0 , 68 ) e somministrazione di - bloccanti ( 61 pazienti nel gruppo a ; 37 pazienti nel gruppo b ; p = 0 , 51 )  . 
 stato riscontrato un numero significativamente pi alto di pazienti di sesso femminile nel gruppo b ( 30 pazienti ; p < 0 , 05 )  . centosessantaquattro esami sono stati ritenuti idonei per il raggiungimento di un giudizio diagnostico nella routine clinica ( mancanza di artefatti da movimento con chiara delineazione del vaso ; minima presenza di artefatti con modesto blurring ; artefatti moderati , blurring moderato senza discontinuit delle strutture dei vasi )  . 
 solamente 6 pazienti ( 3 , 5% ) con fc media > 65 bpm durante la scansione sono stati considerati come grado 4 poich nessun dataset disponibile consentiva una valutazione diagnostica accettabile a causa della presenza di eccessivi artefatti da movimento ( sdoppiamento / discontinuit dei vasi )  . nel gruppo a una qualit dimmagine accettabile ( gradi 13 ) stata raggiunta nel 100% dei pazienti , in larga misura senza artefatti da movimento ( 71 , 8% )  . 
for this reason , data corresponding to the phase in which heart motion is at a minimum needs to be radiol med ( 2008 ) 113 : 644657 ni ac - tcms prive di artefatti ( 36 , 7% )  . 
nel gruppo a le fasi ottimali di ricostruzione per esprimere un giudizio diagnostico risultano al 70% ( 55 / 110 , 71 / 110 e 69 / 110 per la cdx , la iva e la cx ) ed al 75% ( 26 / 110 , 28 / 110 e 28 / 110 , rispettivamente )  . 
nel gruppo b stata utilizzata unampia gamma di fasi di ricostruzioni : in particolare al 40% ( 32 / 60 , 18 / 60 e 17 / 60 , rispettivamente ) ed al 70% ( 12 / 60 , 22 / 60 e 19 / 60 , rispettivamente )  . 
allo stesso tempo , un consistente numero di ricostruzioni in fase telesistolica stato riscontrato per la valutazione di iva ( 43 , 3% ) e cx ( 43 , 3% ) ( tabella 3 )  . 
solamente 6 indagini di actcms ( fc media durante la scansione di 82 , 83 , 84 , 92 e 94 , questultima in due casi ) sono state considerate inficiate da artefatti severi ( grado 4 ) e quindi reputate non diagnostiche . discussione lacquisizione dei dati dellimmagine in ac - tcms continua allinterno del ciclo cardiaco se si utilizza un gating cardiaco di tipo retrospettivo , per tale motivo i dati corrispondenti alla fase in cui il movimento cardiaco minimo devono essere estratti , spostando il punto dinizio della ricostruzione delle immagini relativamente allonda r con il fine di ridurre al minimo gli artefatti da blurring e da movimento [ 17 ]  . numerosi approcci possono essere utilizzati quando si eseguono le ricostruzioni . 
una reale ottimizzazione della tecnica di gating retrospettivo deve ancora essere raggiunta . le quattro tecniche possono essere utilizzate indiscriminatamente , ma questo dipende dal grado di esperienza delloperatore , dalle capacit del software / hardware e dal tempo disponibile per le ricostruzioni . 
la fase del ciclo cardiaco che fornisce la maggior parte delle informazioni quella compresa tra mesoe telediastole ; in questa fase il cuore in riempimento isovolumetrico e il movimento riradiol med ( 2008 ) 113 : 644657 extracted by shifting the beginning of image reconstruction with regard to the r wave , with the aim of reducing motion and blurring artefacts to a minimum [ 17 ]  . a number of approaches can be used when performing the reconstructions . 
these include : ( 1 ) relative delay strategy , whereby the delay time is a percentage of the r - r interval ; ( 2 ) absolute delay strategy , whereby the delay time is constant after the previous r wave ; ( 3 ) absolute reverse delay strategy , whereby the delay time is constant prior to the next r wave ; ( 4 ) end of the time window positioned at the peak of the p wave [ 18 ]  . 
the four techniques described can be used indiscriminately , but this depends on the degree of experience of the operator , the software / hardware capabilities and the time available for reconstruction . 
in this phase , the heart is in isovolumetric filling , and motion is at a minimu in many cases , the end - systolic phase can provide relevant information , as the motion of the coronary arteries is also at a minimum at the end of myocardial contraction [ 8 ]  . multiple reconstructions are usually performed in different reconstruction windows , and later the operator selects the data set where motion artefacts are at a minimum , possibly using different reconstruction windows in the same patient for visualisation of the rca , lad and lcx [ 15 ]  . 
of course , routine clinical practice in this case is conditioned by two factors : ( 1 ) the time required by the operator to perform the reconstructions and any consequent increase in archiving space , and ( 2 ) the radiation dose used for retrospective gating , which poses important questions for justification of the examination . various studies have investigated the relationship between image quality and the optimal reconstruction window with 4 - , 16and 64 - slice scanners [ 713 , 19 ]  . 
with 4 - mdct , the lad is best visualised at 50%70% , the lcx at 50%60% and the rca at 40%50% of the r - r interval [ 79 ] , thus indicating the need for separate reconstructions for the different vessels . 
with 16 - mdct , optimal image quality is usually obtained in mid diastole ( 350 ms , 400 ms or 450 ms , corresponding approximately to 60%70% ) [ 10 ] , with additional reconstructions in the end - systolic phase for higher hr where required [ 1012 ]  . 
with 64 - mdct showed that additional reconstructions during systole were no longer necessary , even at higher hr , as even at hr > 65 bpm , the 4% of segments with better image quality during systole were also of diagnostic quality during diastole [ 13 ]  . 
as mdct coronary angiography is characterised by the use of high doses of ionising radiation , particularly with 64 - mdct , the results of this study could pave the way for the widespread use of ecg pulsing , that is , an acquisition targeted exclusively at the midto end - diastolic reconstruction windows , thus reducing dotto al minimo . 
in numerosi casi la fase telesistolica pu fornire informazioni rilevanti ; infatti , anche al termine della contrazione miocardica il movimento delle arterie coronarie risulta minimo [ 8 ]  . di solito , vengono eseguite multiple ricostruzioni in differenti finestre temporali e loperatore , successivamente , sceglie il dataset dove gli artefatti da movimento sono ridotti al minimo , eventualmente utilizzando nello stesso paziente differenti finestre temporali per la rappresentazione della cdx , delliva e della cx [ 15 ]  . 
indubbiamente , la routine clinica condizionata , in questo caso , da due fattori : il tempo necessario per le operazioni di ricostruzione da parte delloperatore cui consegue certamente un aumento degli spazi di archiviazione ; la dose di radiazioni impiegata nellutilizzo del gating retrospettivo che pone in partenza seri interrogativi sulla giustificazione dellesame . 
 vari studi hanno indagato sul rapporto tra qualit dimmagine ed intervallo temporale ottimale di ricostruzione con differenti tc a 4 , 16 e 64 detettori [ 713 , 19 ]  . 
con la tc a 4 strati , liva era meglio visualizzata al 50%70% , la cx al 50%60% , la cdx al 40%50% dellintervallo r - r [ 79 ] , indicando il bisogno di ricostruzioni separate per i vari vasi . 
con la tc a 16 strati la migliore qualit di immagine veniva solitamente raggiunta nella diastole media ( 350 ms , 400 ms o 450 ms , corrispondenti approssimativamente al 60%70% ) [ 10 ] , con eventuali ricostruzioni addizionali telesistoliche per frequenze elevate [ 1012 ]  . 
 [ 13 ] con la tc a 64 strati ha messo in evidenza che ricostruzioni addizionali durante la sistole non sono pi necessarie , anche a frequenze elevate , dal momento che anche con frequenze > 65 bpm , il 4% dei segmenti con miglior qualit dimmagine in sistole raggiungeva una qualit dimmagine diagnostica anche in diastole [ 13 ]  . dal momento che la ac - tcms con gating retrospettivo caratterizzata dallutilizzo di unelevata dose di radiazioni ionizzanti specialmente con la tc a 64 strati , i risultati di questo studio potrebbero autorizzare in futuro allutilizzo indiscriminato dellecg - pulsing , cio ad unacquisizione mirata esclusivamente nelle finestre temporali meso - telediastoliche , con riduzione di dose del 48% negli uomini e del 45% nelle donne [ 4 , 14 ]  . 
nonostante ci tutti gli studi con tc a 64 strati per la valutazione dellaccuratezza diagnostica nellindividuazione delle stenosi emodinamicamente significative su popolazioni selezionate non applicano questa tecnica ed utilizzano pi finestre temporali di ricostruzione del ciclo cardiaco [ 15 ]  . 
 la recente introduzione di tc a 64 strati con doppio tubo radiogeno - sistema rilevatore ( dual source - ct ) , grazie ad una migliore risoluzione temporale ( 82 , 5 ms ) , offre la possibilit di ottenere una qualit dimmagine indipendente dalla fc e rende , pertanto , superfluo lutilizzo dei bloccanti per ridurla [ 20 , 21 ]  . 
lutilizzo di questa nuova tecnologia di tcms con la possibilit di modulare la cor652 radiol med ( 2008 ) 113 : 644657 the radiation dose by 48% in men and 45% in women [ 4 , 14 ]  . 
despite this , most studies with 64 - mdct for the evaluation of diagnostic accuracy in the identification of haemodynamically significant stenoses in selected populations do not apply this technique and , instead , use reconstruction windows from different phases of the cardiac cycle [ 15 ]  . with its significant improvement in temporal resolution ( 82.5 ms ) , the recently introduced 64 - slice dual - source ct offers the possibility of obtaining image quality independent of hr and therefore eliminates the need for beta - blockers to reduce hr [ 20 , 21 ]  . 
a further development could be 256 - mdct with its real - time scanning and ecg gating , which would eliminate the need for reconstructions in different time windows of the cardiac cycle , although at present , the only study reported in the literature is a work in progress limited to two patients [ 22 ]  . in routine clinical practice , however , despite the administration of beta - blockers to reduce hr or where their administration is contraindicated , the hr may unexpectedly rise above 65 bpm ( due to anxiety and reaction to high flow rates of contrast material , particularly in women )  . 
nonetheless , the current ecg - pulsing model does not rente del tubo radiogeno potrebbe consentire lottimizzazione dei meccanismi di ecg - pulsing con una riduzione della dose di radiazioni al paziente [ 20 , 21 ]  . 
nel gruppo b ( fc > 65 bpm ) ( figg . 35 ) stata utilizzata , invece , unampia gamma di ricostruzioni , con rilievo particolare di quelle telesistoliche al 40% ( 32 / 60 , 18 / 60 e 17 / 60 , rispettivamente )  . 
tuttavia il modello attuale di ecgpulsing non appare ancora consigliabile per le valutazioni cliniche dal momento che tutti gli studi di accuratezza diagnostica della ac - tcms riportati in letteratura si servono , radiol med ( 2008 ) 113 : 644657 fig . 
3 volume - rendered reconstructions performed every 5% of the rr interval from 0% to 95% of the cardiac cycle for a total of 20 data sets in the same group a patient as fig . 
3 riformattazioni volume rendering effettuate ogni 5% dellintervallo r - r dallo 0% al 95% del ciclo cardiaco per un totale di 20 dataset , nello stesso paziente del gruppo a riportato in fig . 
2 , con frequenza cardiaca media di 49 bp anche per lalbero coronarico sinistro ( tronco comune , arteria coronaria interventricolare anteriore , arteria circonflessa e ramo intermedio ) possibile utilizzare a scopo valutativo diagnostico le finestre temporali di ricostruzione sia in fase telesistolica ( 40% ) che in meso - telediastolica ( dal 60% all80% ) , in maniera del tutto sovrapponibile a quelle per larteria coronaria destra . 654 radiol med ( 2008 ) 113 : 644657 fig . 
5 riformattazioni volume rendering effettuate ogni 5% dellintervallo r - r dallo 0% al 95% del ciclo cardiaco per un totale di 20 dataset , in un paziente del gruppo b , con frequenza cardiaca media di 81 bple finestre temporali di ricostruzione utilizzabili a scopo diagnostico per larteria coronaria destra sono quelle che comprendono la sistole ( dal 30% al 45% )  . radiol med ( 2008 ) 113 : 644657 n pt fig . 
6 volume - rendered reconstructions performed every 5% of the r - r interval from 0% to 95% of the cardiac cycle for a total of 20 data sets in a group b patient with a mean heart rate of 73 bpm . the reconstruction windows useful for diagnostic purposes of the left anterior descending and left circumflex coronary arteries are those in midto end - diastole ( from 60% to 80% )  . 
6 riformattazioni volume rendering effettuate ogni 5% dellintervallo r - r dallo 0% al 95% del ciclo cardiaco per un totale di 20 dataset , in un paziente del gruppo b , con frequenza cardiaca media di 73 bp le finestre temporali di ricostruzione utilizzabili a scopo diagnostico per larteria coronaria interventricolare anteriore e larteria coronaria circonflessa sono quelle in fase mesotelediastolica ( dal 60% all80% )  . 
7 distribuzione delle finestre temporali di ricostruzione utilizzate per la valutazione diagnostica nel gruppo a suddivise per singolo vaso coronarico ( cdx , arteria coronaria destra ; iva , arteria coronaria interventricolare anteriore ; cx , arteria coronaria circonflessa )  . reconstruction windows appear advisable for clinical evaluation , as all of the published studies of diagnostic accuracy of mdct coronary angiography perform the evaluation with a number of different reconstruction windows of the cardiac cycle . conclusions on the basis of our clinical experience with mdct coronary angiography , the choice of the reconstruction window of the comunque , per la valutazione di pi ricostruzioni in differenti finestre temporali del ciclo cardiaco . conclusioni sulla base della nostra esperienza clinica con ac - tcms la scelta della finestra temporale di ricostruzione del ciclo cardiaco appare influenzata dalla frequenza cardiaca media registrata durante la scansione . 
8 distribuzione delle finestre temporali di ricostruzione utilizzate per la valutazione diagnostica nel gruppo b suddivise per singolo vaso coronarico ( cdx , arteria coronaria destra ; iva , arteria coronaria interventricolare anteriore ; cx , arteria coronaria circonflessa )  . reconstruction windows cardiac cycle appears to be influenced by the mean hr recorded during the scan . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , 2dipartimento di biopatologia e diagnostica per immagini , cattedra di anatomia ed istologia patologica , 3cattedra di urologia , universit di roma , policlinico tor vergata , viale oxford 81 , 00133 roma , italy correspondence to : m carlani , tel . : + 39 - 06 - 20902401 , fax : + 39 - 06 - 20902404 , e - mail : marco_carlani@libero.it received : 28 september 2006 / accepted : 27 november 2006 / published online : 20 may 2008 springer - verlag 2008 abstract purpose . 
mri , mrsi and dce - mri with a 3 - tesla whole - body scanner were performed in 30 patients with biopsy - proven prostate cancer before radical prostatectomy . 
high - resolution t2 - weighted turbo spin echo ( tse ) images were evaluated for visualisation of the peripheral zone , central gland , visibility of the cancer lesion , prostatic capsule delineation and overall image quality according to a five - point scale . 
relative levels of the prostate metabolites citrate , choline and creatine were determined in cancer and in the normal peripheral zone ( pz ) and central gland ( cg )  . 
the high signal - to - noise ratio ( snr ) at 3 tesla provided t2 - weighted tse images with excellent anatomical detail ( in - plane voxel size of 0.220.22 mm ) and good t2 contrast . 
le immagini t2 pesate ad alta risoluzione sono state valutate in base ad una scala di 5 punti per la visualizzazione della zona periferica , della ghiandola centrale , della lesione tumorale , per la delineazione della capsula prostatica e per la qualit complessiva dellimmagine . 
sono stati determinati i valori relativi dei metaboliti prostatici citrato , colina e creatina nel cancro , nella zona periferica normale ( pz ) e nella ghiandola centrale ( cg )  . 
lelevato rapporto segnale - rumore ( snr ) a 3 tesla ha permesso di ottenere immagini tse t2 pesate con radiol med ( 2008 ) 113 : 670688 was sufficient to separate the choline and creatine resonances and allow delineation of the four peaks of citrate resonance . 
the combination of vascular information from dce - mri and metabolic data from mrsi has excellent potential for improved accuracy in delineating and staging prostate carcinoma . these results suggest that high magnetic field strengths offer the possibility of studying prostate cancer without use of an endorectal coil . keywords prostate cancer dynamic contrast - enhanced magnetic resonance imaging ( dce - mri ) magnetic resonance spectroscopic imaging ( mrsi ) high - field strength ( 3 - t ) mr imaging un eccellente dettaglio anatomico ( dimensioni in piano del voxel di 0 , 220 , 22 mm ) e buon contrasto t2 . lincrementata risoluzione spettrale risultata sufficiente a separare la risonanza della colina e della creatina e ha permesso di delineare i 4 picchi della risonanza del citrato . 
il rapporto ( colina + creatina ) / citrato risultato pi elevato nel cancro rispetto a quello individuato nella pz e nella cg ( p < 0 , 001 )  . 
questi risultati suggeriscono come campi i magnetici ad elevata intensit offrano la possibilit di studiare il cancro prostatico senza luso di una bobina endorettale . parole chiave cancro prostatico imaging dinamico postcontrastografico ( dce - mri ) imaging spettroscopico ( mrsi ) imaging ad alta intensit di campo ( 3 t ) introduction introduzione the current availability of magnetic resonance imaging ( mri ) scanners operating at 3 tesla ( 3 t ) and equipped with whole - body radiofrequency coils has enabled the study of prostatic disease at high field strength . 
from a theoretical point of view , the signal - to - noise ratio ( snr ) of a 3 - t system is twice that of a 1.5 - t scanner [ 1 ] , with a gain comparable with that offered by a dedicated surface coil compared with a whole - body coil . 
the increased snr can potentially be exploited to improve either the spatial or the temporal resolution of mri acquisitions [ 2 ]  . the wide variability in the diagnostic accuracy of morphological mri ( mainly based on t2 - weighted sequences ) in prostate cancer staging ( 54%88% ) [ 3 , 4 ] indicates that although the use of endorectal coils with 1.5 - t magnets has allowed for a high spatial resolution in the study of the la disponibilit attuale di apparecchiature di risonanza magnetica ( rm ) a 3 tesla ( 3 t ) equipaggiate con bobine di radiofrequenza whole - body ha fornito lopportunit di studiare la patologia prostatica con alta intensit di campo . da un punto di vista puramente teorico , il rapporto segnale / rumore ( snr ) fornito da un sistema a 3 t due volte superiore rispetto a quello di uno scanner a 1 , 5 t [ 1 ] , con un guadagno che pu essere comparato al vantaggio offerto da una bobina di superficie dedicata rispetto ad una per lintero corpo . 
lincrementato snr pu essere potenzialmente utilizzato per migliorare o la risoluzione spaziale o quella temporale nelle acquisizioni rm [ 2 ]  . lampia variabilit , riportata in letteratura , nei valori di accuratezza diagnostica degli studi morfologici ( basati essenzialmente sulle sequenze t2 pesate ) della rm nella sta672 radiol med ( 2008 ) 113 : 670688 prostate , there is still room for improvement , and additional progress may come from higher field strengths , which could also make endorectal coils unnecessary . 
furthermore , the accuracy of dynamic contrast - enhanced mri ( dce - mri ) , which has provided a further tool for the evaluation of prostate cancer [ 5 , 6 ] , could improve the distinction between pathological and normal vascularity thanks to its higher spatial and temporal resolution . 
finally , the mri technique that might best benefit from the use of a field strength of 3 t is be functional imaging such as hydrogen spectroscopy ( [ 1h ] - mrs )  . it is well recognised that spectroscopy increases the specificity of mri in the evaluation of prostate cancer [ 7 ] by identifying , through the reduction or disappearance of citrate and the simultaneous elevation of choline and creatine , the characteristic marker of prostate cancer . 
however , because at 1.5 t the amplitude of resonance lines in the prostate is similar to or even greater than dispersion due to the chemical shift of choline and creatine , it is difficult to quantify the two metabolites separately . 
although the switch from a 1.5 - t system to one operating at 3 t allows doubling the snr , it has potential drawbacks that require special evaluation in clinical settings , such as shorter t2 relaxation time , longer t1 time [ 8 ] , increased radiofrequency energy deposition [ specific absorption rate ( sar ) ] on the patient [ 9 ] , greater field heterogeneity within the organ or tissue being studied [ 10 ] and greater susceptibility artefacts that might offset the theoretical benefits of increased snr . the aim of our work was to verify the feasibility of an in vivo study of the prostate gland and prostate cancer using 3t mri with a phased - array pelvic coil and present our preliminary experience in 30 patients . 
we analysed the possible benefits and drawbacks of the use of a high field strength in terms of spatial and temporal resolution for t2 - weighted anatomical imaging and for dce - mri , and the potential of [ 1h ] - mrs and its combination with dce - mri in the differentiation between normal prostate and cancer . materials and methods patients between july and december 2005 , mri studies were conducted on 30 patients with prostate cancer diagnosed by means of ultrasound - guided random sector biopsy [ performed for abnormal serum prostate - specific antigen ( psa ) at least 6 weeks before mri evaluation ]  . 
the padiazione del cancro prostatico ( 54%88% ) [ 3 , 4 ] dimostra che , sebbene lutilizzo della bobina endorettale con magneti da 1 , 5 t abbia sin ora consentito uno studio della loggia prostatica caratterizzato da un elevato dettaglio spaziale , ci sono sicuramente dei margini di miglioramento che potrebbero essere offerti proprio dallutilizzo di pi intensi campi magnetici che tra laltro possano non rendere pi necessario lutilizzo della bobina endorettale . 
inoltre laccuratezza degli studi post - contrastografici di tipo dinamico ( dce - mri ) , che si sono dimostrati essere uno strumento addizionale nella valutazione del cancro prostatico [ 5 , 6 ] potrebbe , grazie alla gi citata incrementata risoluzione spaziale e temporale , permettere di distinguere pi precisamente le caratteristiche di vascolarizzazione patologiche da quelle normali . 
infine ad usufruire maggiormente dellutilizzo di un campo magnetico a 3 t dovrebbe essere limaging di tipo funzionale come la spettroscopia dellidrogeno ( 1h - mrsi )  . ormai assodato come lanalisi spettroscopica apporti unelevata specificit nella valutazione rm del cancro prostatico [ 7 ] individuando nella riduzione o scomparsa del citrato e nella contemporanea elevazione della colina e della creatina il marker metabolico caratteristico del tessuto neoplastico prostatico . 
poich , per , lampiezza delle linee di risonanza nella prostata ad 1 , 5 t paragonabile o addirittura maggiore della dispersione dovuta al chemical shift della colina e della creatina , risulta difficile quantificare i due metaboliti separatamente . 
lutilizzazione di un campo magnetico a pi alta intensit , incrementando la dispersione dovuta al chemical shift dovrebbe facilitare una pi precisa separazione e quantificazione dei singoli metaboliti . sebbene , come abbiamo gi detto , il passaggio da un sistema a 1 , 5 t ad uno a 3 t comporti un raddoppio del snr , esso porta con s anche una serie di potenziali aspetti negativi che vanno valutati soprattutto in ambito clinico , come laccorciamento del tempo di rilassamento t2 , lallungamento del tempo t1 [ 8 ] un aumentato trasferimento al soggetto esaminato dellenergia legata agli impulsi di radiofrequenza ( sar , specific absortion rate ) [ 9 ] , una maggiore eterogeneit del campo magnetico allinterno dellorgano e del tessuto di interesse [ 10 ] e pi cospicui artefatti legati alla suscettivit magnetica che potrebbero controbilanciare i teorici benefici correlati allincrementato snr . scopo del presente lavoro quello di verificare la fattibilit di uno studio in vivo della ghiandola prostatica e del cancro prostatico con scanner rm a 3 t , utilizzando una bobina pelvica phased - array , presentando la nostra preliminare esperienza relativa a 30 pazienti . 
analizzeremo i possibili vantaggi e svantaggi dellutilizzo di un campo magnetico ad elevata intensit in termini di risoluzione spaziale e temporale per limaging anatomico basato sulle acquisizioni t2 pesate e per il dce - mri , le potenzialit del 1hmrsi e della sua combinazione con il dce - mri nella differenziazione tra ghiandola normale e tumore . radiol med ( 2008 ) 113 : 670688 tients had a mean age of 61 ( range 5468 ) years , median serum psa of 8 ng / ml ( range 3.042.0 ng / ml ) , localised cancer on rectal digital examination and a median gleason score of 7 ( range 610 )  . 
to reduce bowel peristalsis artefacts , all patients received an intravenous injection of 30 mg of butyl scopolamine ( buscopan ; boehringer , ingelheim , germany ) before being positioned on the mri table . 
all patients underwent radical prostatectomy within 20 days ( 15.5 days on average ) after the mri examination . mri technique all mris were acquired with a 3 - t scanner ( philips intera achieva , best , the netherlands ) equipped with a gradient system allowing a maximum amplitude and slew rate of 80 mt / m and 200 mt / m / ms , respectively . 
a body coil was used for pulse transmission and a two - element phased - array coil for signal reception ; the latter consisted of two circular elements with a maximum diameter of 19 cm ( flexm ) placed one opposite the other in the anterior and posterior pelvic region . 
after acquisition of a rapid localising multiplanar sequence [ half - fourier single - shot turbo spin echo ( haste ) ] , we proceeded with the morphological study . this consisted of high - spatial - resolution t2 - weighted turbo spin echo ( tse ) sequences acquired in the three orthogonal planes , providing coverage of the entire prostate and seminal vesicles in the acquisition volume . 
acquisition parameters were as follows : tr 3 , 295 ms , te 150 m , slice thickness 3 mm with interslice gap of 0.3 mm , 6 excitations , fov 160 mm and a matrix of 720720 with an in - plane voxel size of 0.220.22 mt1 - weighted tse images ( tr 469 ms , te 11 ms , slice thickness 3 mm with interslice gap of 0.3 mm , 3 excitations , fov 160 mm , matrix of 256512 ) were also acquired in the axial plane to allow detection of haemoglobin degradation products resulting from previous biopsies . 
based on the t2 - weighted images , a radiologist experienced in prostate imaging selected the areas suspicious for malignancy , which were subsequently used to position the spectroscopic acquisition volume . the volume of interest ( voi ) to be studied with spectroscopy was selected taking care to include the prostatic parenchyma and exclude as much periglandular fat as possible . 
to this end , we used a double spin - echo point - resolved spatially localised spectroscopic ( press ) sequence with a two - dimensional technique ( 2dsi ) along with a te ( 135 ms ) optimised for the quantitative evaluation of citrate and choline with multivoxel analysis . 
the following acquisition parameters were used : tr 1 , 200 ms , te 135 ms , spectral bandwidth 2.000 hz , matrix 2020 , fov 120 , nominal voxel resolution of materiali e metodi pazienti nel periodo compreso tra luglio e dicembre 2005 sono stati sottoposti ad esame rm 30 pazienti con neoplasia prostatica diagnosticata mediante biopsia settoriale random ecoguidata ( eseguita in relazione a livelli alterati di psa sierico almeno 6 settimane prima della valutazione rm ) , candidati ad intervento chirurgico di prostatectomia radicale retropubica . 
i pazienti esaminati avevano un et media di 61 anni ( intervallo 5468 anni ) con un valore mediano di psa sierico di 8 ng / ml ( intervallo 3 , 042 , 0 ng / ml ) , neoplasia localizzata allesplorazione digito - rettale e valore mediano di gleason score pari a 7 ( intervallo 610 )  . 
al fine di ridurre gli artefatti da movimento legati alla peristalsi intestinale , prima di essere posizionati sul lettino della rm , ai pazienti sono stati somministrati per via endovenosa , 30 mg di butylscopolamina ( buscopan , boehringer , ingelheim , germania )  . 
tutti i pazienti sono stati sottoposti a prostatectomia radicale non oltre 20 giorni ( media 15 , 5 gg ) dallesame rm . tecnica rm tutte le immagini rm sono state acquisite con uno scanner ad intensit di campo di 3 t ( philips intera achieva , best , olanda ) equipaggiato con gradienti di ampiezza e slew rate massimi rispettivamente di 80 mt / m e 200 mt / m / ms , utilizzando la bobina del corpo per la trasmissione degli impulsi di eccitazione e una bobina phased - array , costituita da due elementi circolari del diametro massimo di 19 cm ( flexm ) posizionati in maniera contrapposta e speculare in sede pelvica anteriore e posteriore , per la ricezione del segnale . 
dopo aver acquisito una sequenza multiplanare rapida di centraggio ( half - fourier single shot turbo spin echo , haste ) , si proceduto alla studio morfologico della loggia prostatica . 
a tal fine sono state acquisite immagini con tecnica turbo spin echo ( tse ) t2 pesate ad alta risoluzione spaziale sui tre piani ortogonali dello spazio includendo nel volume dacquisizione lintera prostata e le vescicole seminali . 
i parametri di acquisizione sono stati i seguenti : tr 3295 ms , te 150 ms , spessore di sezione 3 mm con intervallo tra le sezioni di 0 , 3 mm , 6 eccitazioni , fov di 160 mm e una matrice di 720720 con una dimensione in piano del voxel di 0 , 220 , 22 mimmagini t1 pesate , con tecnica tse ( tr 469 ms , te 11 ms , spessore di sezione 3 mm con intervallo tra le sezioni di 0 , 3 mm , 3 eccitazioni , fov di 160 mm , matrice di 256512 ) sono state inoltre acquisite sul piano assiale con lo scopo di evidenziare leventuale presenza di pigmenti di degradazione ematica in relazione alle pregresse biopsie . 
sulla base delle immagini t2 pesate un radiologo esperto nellimaging prostatico ha individuato le aree sospette per la presenza di neoplasia , che sono state cos selezionate per il 674 radiol med ( 2008 ) 113 : 670688 6610 m acquisition time for the spectroscopic sequence was approximately 13 min . dce - mri was performed after the spectroscopy to avoid possible distortion of the spectral bands and local field inhomogeneity due to susceptibility induced by the paramagnetic contrast material . 
the total time required to perform the entire morphological and functional imaging protocol , including patient preparation and positioning , was approximately 45 min . histological analysis the radical prostatectomy specimens were fixed overnight in 10% formalthe seminal vesicles were removed from the prostate and examined separately . 
the sections were then embedded in paraffin and 4 - m microsections were prepared and stained with haematoxylin - eosthe extent of the neoplastic lesion was outlined on the glass slide cover by a pathologist experienced in prostate disease who was blinded to the mri results . 
the mr images and the histological sections were subsequently compared and correlated . data processing and image analysis analysis of the morphological images was done by a radiologist experienced in abdominopelvic mri . 
a tal fine stata utilizzata una sequenza press ( double spin - echo point - resolved spatially localized spectroscopic sequence ) con tecnica bidimensionale ( 2dsi ) con un te ( 135 ms ) ottimizzato per la valutazione quantitativa del citrato e della colina con analisi multivoxel . 
la soppressione del grasso e dellacqua stata effettuata utilizzando la tecnica di inversione selettiva di banda con gradiente di defasamento ( tecnica basing ) [ 11 ]  . lomogeneizzazione del campo magnetico a livello del voi stata effettuata con una procedura automatica di shimming tridimensionale localizzato . 
sono stati utilizzati i seguenti parametri di acquisizione : tr 1200 ms , te 135 ms , ampiezza spettrale 2000 hz , con matrice di 2020 , fov di 120 , con risoluzione nominale del voxel di 6610 mil tempo di acquisizione della sequenza spettroscopica stato in media di 13 minuti . il dce - mri stato effettuato dopo lacquisizione della sequenza di spettroscopia al fine di evitare i possibili effetti distorsivi sulle bande spettrali e di disomogeneizzazione locale del campo magnetico legati alla suscettivit magnetica indotta dal mezzo di contrasto paramagnetico . 
sono state acquisite 30 dinamiche di cui la prima senza somministrazione di mezzo di contrasto e le restanti 29 durante infusione endovenosa di un bolo ( 15 ml , 0 , 5 m , 2 , 5 ml / s ) di gadobenate dimeglumine ( gd - bopta , multihance , bracco imaging spa , milano , italia ) seguita da un bolo di spinta di 20 ml di soluzione fisiologica , per mezzo di un iniettore automatico a due vie ( stellant mr injection system , medrad , pittsburg , pa )  . 
il tempo totale di acquisizione stato di 2 , 23 minuti , con una risoluzione temporale per dinamica di 4 , 7 secondi e un numero totale di 1200 immagini . le acquisizioni per lo studio morfologico e per il dce - mri sono state effettuate con tecnica di imaging parallelo sense ( sensitivity encoding ) utilizzando un fattore di riduzione pari a 2 . 
il tempo totale richiesto per eseguire lintero protocollo di acquisizione dellimaging morfologico e funzionale compresa la preparazione ed il posizionamento del paziente , stato approssimativamente di 45 minuti . analisi istologica i campioni derivanti dalla prostatectomia , sono stati fissati per una notte in formalina al 10% . 
lintera prostata stata sezionata in strati di radiol med ( 2008 ) 113 : 670688 the visualisation of low - intensity stripes on the t2 - weighted images representing the prostate capsule and pseudocapsule [ 12 ]  . 
images were assessed qualitatively for : visibility of the peripheral zone visibility of the central zone lesion conspicuity delineation of the prostatic capsule overall image quality according to a five - point scale ( 1 very poor , 2 poor , 3 moderate , 4 good , 5 excellent )  . the likelihood of cancer being present in the peripheral zone was defined by assessing the following criteria on the t2 - weighted images : nonvisualisation of hypointense areas was considered as a sign of normality presence of a heterogeneously hypointense area with irregular margins was considered equivocal for cancer presence of a homogeneously hypointense area with rounded contour and blurred margins was considered suspicious for cancer . the single voxels of the volume selected in the spectroscopic sequence were automatically displayed by the software in the form of a 2d grid overlaid on the corresponding axial t2 - weighted images . 
in addition , the ratio between the integral of the citrate peak and that of the choline peak and the ratio of the integral of the choline plus citrate peak were also calculated for each voxel . 
the spectra were also analysed qualitatively by evaluating the separation of the citrate , choline and creatine signal and the degree of fat and water suppression . images acquired in the dynamic sequences were reviewed on a dedicated workstation ( viewforum , philips , best , the netherlands )  . 
after reviewing all images in cine mode , a radiologist in consensus with a pathologist drew a region of interest ( roi ) over the area of the neoplastic lesion , correlating it directly with the histological sections . two additional rois where possible , of the same size as the first were also drawn over the healthy peripheral and central zone on the same image . 
successivamente le immagini di rm e le sezioni istologiche sono state confrontate e correlate . elaborazione dei dati ed analisi delle immagini lanalisi delle immagini morfologiche stata effettuata da un radiologo esperto nellimaging rm delle strutture addomino - pelviche . 
i confini della zona periferica sono stati definiti grazie alla visualizzazione delle bande di bassa intensit di segnale nelle immagini t2 pesate riferibili alla capsula e alla pseudocapsula prostatica [ 12 ]  . 
le immagini sono state analizzate qualitativamente , per la visualizzazione di : zona periferica ; zona centrale ; visibilit della lesione ; delineazione della capsula prostatica ; qualit globale dellimmagine secondo una scala di 5 punti ( 1 : molto scadente , 2 : scadente , 3 : moderata , 4 : buona , 5 : eccellente )  . la probabilit della presenza della neoplasia a livello della zona periferica stata definita analizzando le immagini t2 pesate in base ai seguenti criteri : la mancata visualizzazione di aree ipointense stata considerata come segno di normalit ; la presenza di unarea disomogeneamente ipointensa a margini irregolari stata considerata come equivoca per neoplasia ; la presenza di unarea omogeneamente ipointensa a margini rotondeggianti e limiti sfumati stata valutata come sospetta per neoplasia . i singoli voxel del volume selezionato nella sequenza spettroscopica sono stati rappresentati automaticamente dal software dedicato allanalisi spettroscopica presente nella consolle di acquisizione in forma grafica di griglia bidimensionale sovrapposta alle corrispondenti immagini assiali t2 pesate . 
per ciascun voxel stato calcolato inoltre il rapporto tra il valore degli integrali relativi al picco del citrato e a quello della colina e il rapporto tra il valore dellintegrale del picco della colina sommato a quello della creatina rispetto a 676 fig . 
b tipo ii : continuo incremento dellintensit di segnale . increase in signal intensity between enhancement onset and maximum enhancement divided by time to peak ( wash - in rate ) difference between peak and baseline intensity ( maximum enhancement ) the above parameters were also displayed graphically as colour maps superimposed on the corresponding contrastenhanced images . to correlate these parameters with the ( choline + creatine ) / citrate ratio , the spectroscopic grid was automatically overlaid on the colour maps , and the mean value for each parameter was calculated within each voxel . radiol med ( 2008 ) 113 : 670688 quello del picco del citrato . 
gli spettri sono stati analizzati anche qualitativamente valutando la separazione del segnale del citrato , della colina , della creatina e il grado di soppressione del segnale adiposo e dellacqua . le immagini acquisite nelle sequenze dinamiche sono state trasferite ed analizzate su di una stazione di lavoro dedicata ( viewforum , philips , best , olanda )  . 
dopo aver revisionato tutte le immagini , facendole scorrere in modalit cine , un radiologo in accordo con il patologo ha tracciato una roi comprendente larea della lesione neoplastica correlandola direttamente con le sezioni istologiche . 
per la valutazione delle differenze tra i valori dei parametri quantitativi di uptake del contrasto e quelli relativi ai rapporti dei metaboliti a livello delle lesioni neoplastiche , della zona periferica e di quella centrale stata utilizzata lanalisi della varianza ( anova )  . 
il test del 2 stato utilizzato nella comparazione tra le diverse tipologie delle curve intenradiol med ( 2008 ) 113 : 670688 table 1 qualitative assessment of t2 weighted images parameters visibility of the peripheral zone visibility of central gland capsule delineation lesion delineation overall image quality tse , turbo spin echo amean values of visual assessment on a scale of 15 tabella 1 valutazione qualitativa delle immagini t2 pesate parametri visualizzazione zona periferica visualizzazione zona centrale delineamento della capsula visibilit della lesione qualit globale delle immagini sequence tse - t2w tse - t2w tse - t2w tse - t2w tse - t2w sequenza tse - t2w tse - t2w tse - t2w tse - t2w tse - t2w tse , turbo spin echo avalore medio di valutazione visiva secondo una scala da 1 a 5 statistical analysis all quantitative data were expressed as mean and standard deviation ( sd )  . 
analysis of variance ( anova ) was used to evaluate differences among the quantitative parameters of contrast uptake and those relating to the metabolite ratios at the level of the cancer , peripheral zone and central zone . the correlation between metabolite ratios and enhancement parameters was evaluated using pearsons correlation analysis . 
il picco del citrato risultato essere composto da una componente centrale pi cospicua centrata a 2 , 60 ppm ( caratterizzata a sua volta da due picchi distinti ) e da due componenti pi esterne di minore entit . 
componenti lipidiche residue non soppresse , localizzate intorno a 1 , 3 ppm e 2 , 1 ppm , sono state evidenziate nelle vicinanze dellarea di risonanza del citrato senza tuttavia produrre un oscuramento dei picchi di interesse e senza comportare la decisione di eliminare lo spettro dallanalisi quantitativa . sovrapponendo la griglia corrispondente al voi di acquisizione spettroscopica alle immagini t2 tse assiali e comparandole visivamente con le sezioni istologiche , i voxel sono stati classificati come appartenenti allarea neoplasti678 radiol med ( 2008 ) 113 : 670688 fig . 
turbo spin - echo t2 - weighted high - resolution images ( tr / te 3295 / 150 , in - plane voxel size 0.220.22 mm ) showing a tumour as an area of decreased signal intensity ( arrows ) in the right peripheral zone . 
immagini tse t2 pesate ad alta risoluzione ( tr / te : 3295 / 150 , dimensione del voxel : 0 , 220 , 22 mm ) che dimostrano la presenza di un focus tumorale visualizzato come area di ridotta intensit di segnale ( frecce ) in corrispondenza della porzione destra della zona periferica . 
piano assiale ( a , b ) , piano coronale ( c ) e piano sagittale ( d )  . resonance area of citrate ; they did not , however , cause obscuration of the peaks of interest , nor did they require the spectrum to be eliminated from the quantitative analysis . by overlaying the grid of spectroscopic vois on the axial t2 tse images and visually comparing them with the histological sections , the voxels were assigned to the neoplastic area , the normal peripheral zone and the central zone . on the basis of this subdivision , a quantitative analysis was subsequently performed on 118 spectra from the healthy peripheral zone , 96 from neoplastic areas and 190 from the ca , alla zona periferica normale e a quella centrale . 
in base a tale suddivisione la successiva analisi quantitativa stata effettuata su 118 spettri derivanti dalla zona periferica indenne , 96 dalle aree neoplastiche e 190 dalla zona centrale . i rimanenti 53 spettri sono stati assegnati alla porzione ghiandolare periuretrale ( 21 ) o ad aree di tessuto misto ( 32 )  . 
nella tabella 2 sono riassunti i valori medi dei rapporti dei metaboliti derivati dallesame spettroscopico . la valutazione quantitativa dei metaboliti effettuata a livello di ciascun spettro ha evidenziato che nelle regioni doradiol med ( 2008 ) 113 : 670688 fig . 
tr 1200 ms , te 135 ms , spectral bandwidth 2000 hz , matrix 2020 , fov 120 mm , nominal voxel size 6610 mb magnetic resonance spectrum obtained from normal left peripheral zone ( a ) demonstrates a normal spectral pattern with high citrate level and no abnormal elevation in choline . 
sequenza press ( tr 1200 ms , te 135 ms , ampiezza spettrale 2000 hz , con matrice di 2020 , fov di 120 , con risoluzione nominale del voxel di 6610 mm )  . 
b spettro ottenuto a livello della zona periferica normale ( a ) di sinistra che dimostra lesistenza di un pattern metabolico normale con elevati livelli di citrato e non elevazione patologica della colina . 
d spettro ottenuto in corrispondenza dei voxels a livello dellarea di alterata intensit di segnale ( e ) nella zona periferica di destra che mostra un elevazione del livello della colina compatibile con la presenza di tessuto neoplastico . 
for all parameters , there is a significant difference between carcinoma and normal tissue ( p < 0.05 ) tabella 3 parametri del dce - mri per la distinzione tra carcinoma e tessuto prostatico normale parametri tempo di arrivo t0 ( s ) tempo di picco ( s ) enhancement massimo ( au ) percentuale di wash in ( 1 / s ) cancro 26 , 55 , 3 73 , 26 , 8 2223932 67 , 215 31 , 73 , 3 982 , 4 1389487 32 , 513 tessuto normale zona periferica tessuto normale zona centrale tutti i dati sono espressi come mediadeviazione standard ( ds )  . 
a significant difference between these two ratios was also found between cancer and the central zone . dynamic contrast - enhanced t1 - weighted acquisitions were successfully completed in all patients ( table 3 )  . 
a significant difference ( p < 0.05 ) was observed in the type of ve era presente il cancro il valore medio del rapporto citrato / colina era significativamente pi basso ( p < 0 , 001 ) che non nella zona periferica non patologica ; al contrario era significativamente ( p < 0 , 001 ) pi elevato il valore medio del rapporto ( colina + creatina / citrato )  . 
una differenza significativa tra questi due rapporti stata evidenziata anche tra il tumore e la zona ghiandolare centrale . in tutti i pazienti le acquisizioni dinamiche t1 pesate dopo somministrazione di mezzo di contrasto sono state eseguite con successo ( tabella 3 )  . 
il carcinoma pu essere individuato in entrambe le mappe parametriche . time - intensity curve between cancers and healthy prostatic tissue , with type 1 curves being more frequent in cancers ( 13 / 30 , 43% ) than in the normal peripheral zone ( 2 / 30 , 7% ) and central zone ( 1 / 30 , 3% )  . 
a axial t2 - weighted turbo spin - echo image ( tr / te 3 , 295 / 150 , in - plane voxel size 0.220.22 mm ) showing hypointense region suspicious for malignancy ( t ) in the right peripheral zone . 
a immagine assiale tse t2 pesata ( tr / te : 3295 / 150 , dimensione del voxel : 0 , 220 , 22 mm ) che dimostra la presenza di una regione ipointensa ( t ) in corrispondenza della zona periferica a destra sospetta per cancro . 
d microfotografia della sezione istologica che mostra il tumore ( t ) a livello della porzione medio - ghiandolare di destra con un grado di gleason di 3 + 4 . 
histological analysis of the surgical specimen in this case revealed coexisting severe inflammation extending throughout the prostate . despite the statistically significant difference in the mean values of enhancement parameters , the high sd values reflect a certain variability among the patient sample . 
a similar finding was also observed for the different ratios between metabolites , the lowest sd being recorded in the ( choline + creatine ) / citrate ratio . we expected the combination of information from the scontrato un valore di maximum enhancement pi basso in corrispondenza della lesione neoplastica che a livello del tessuto normale . 
lanalisi istologica del reperto operatorio in questo caso ha evidenziato una severa condizione flogistica coesistente , diffusa a tutto il tessuto prostatico . sebbene vi fosse una differenza statisticamente significativa nei valori medi relativi ai parametri della dinamica contrastografica , gli elevati valori di deviazione standard registrati indicavano come essi fossero caratterizzati da una certa dispersione nel campione di pazienti . 
un dato analogo stato osservato anche per i diversi rapporti tra i metaboliti con il pi basso valore di deviazione standard osservato radiol med ( 2008 ) 113 : 670688 two evaluations ( mrs and dce - mri ) to allow better distinction between neoplastic lesion , normal peripheral zone and central zone . 
in effect , when we evaluated the correlation between metabolic data and enhancement indices , we obtained relatively weak correlation coefficients that reached significance ( r = 0.713 , p = 0.001 ) for the correlation between the ( choline + creatine ) / citrate ratio and the washin rate in peripheral - zone cancer . 
based on this principle elevation of the ( choline + creatine ) / citrate ratio proved to be a more effective absolute criterion for cancer identification compared with the washin rate . 
the results demonstrate that the intrinsic high snr associated with the use of a high field strength ( 3 t ) can be exploited to increase the spatial resolution of morphological imaging . 
the t2 - weighted sequences were acquired with a slice thickness of 3 mm / 0.3 mm , a matrix of 720720 , and a fov of 160 mm , which provided an in - plane voxel size of 0.22 mm2 , a value much lower than the 0.66 mm2 reported in the international literature as the limit ( associated with a reasonable snr ) for 1.5t imaging with an endorectal coil [ 13 ]  . 
the high spatial resolution provided precise anatomical detail , as demonstrated by the high scores reached on image assessment ( table 1 ) , as well as precise delineation of the cancer . 
furthermore , the high level of anatomical detail and the precise depiction of the capsular profile potentially allow for better distinction between intraglandular disease and disease spreading beyond the capsule , a crucial factor for patient management . although no direct comparison was made with results obtained with a 1.5 - t scanner , our findings suggest that the use of higher field strengths can improve the diagnostic accuracy of morphological imaging in local disease staging . as stated , even spectroscopic studies can in theory benefit greatly from the use of a high field strength , which results per il rapporto ( colina + creatina ) / citrato . ci si aspettava che la combinazione delle informazioni proveniente dalle due valutazioni ( spettroscopica e dinamica postcontrastografica ) permettesse una migliore distinzione tra lesione cancerosa , zona periferica e centrale normale . 
in base a questo principio lelevazione del rapporto ( colina + creatina ) / citrato si dimostrato un criterio assoluto pi efficace nella definizione del cancro rispetto al wash in rate . 
le sequenze t2 pesate sono state infatti acquisite con spessore di sezione 3 mm / 0 , 3 mm , con una matrice di 720720 , ed un fov di 160 mm il che ha consentito di ottenere una dimensione in piano del voxel di 0 , 22 mm2 valore nettamente inferiore a quello di 0 , 66 mm2 che nella letteratura internazionale oggi viene riportato come valore limite ( associato ad un ragionevole snr ) per unapparecchiatura a 1 , 5 t con bobina endorettale [ 13 ]  . 
lelevata risoluzione spaziale ha permesso una precisa visualizzazione dei dettagli anatomici ghiandolari , dimostrata dagli alti punteggi raggiunti nella valutazione qualitativa delle immagini ( tabella 1 ) , cos come una precisa definizione della lesione neoplastica . 
cancer voxels may be distinguished from normal peripheral - zone voxels by the combination of elevated wash - in rate and elevated ( choline + creatine ) / citrate ratio . 
i voxel che rappresentano il cancro possono essere distinti da quelli presenti nella zona periferica normale dalla combinazione di un elevato wash in rate e rapporto ( colina + creatina ) / citrato . 
i pallini neri nel quadrante ii rappresentano i tumori che sono identificati dalla combinazione dellimaging contrastografico dinamico con quello spettroscopico , mentre quelli presenti nel i e iv rappresentano i tumori identificati grazie ad una sola delle due metodiche , rispettivamente imaging contrastografico o spettroscopia . in increased spectral resolution [ 14 ]  . 
the increased spectral resolution allowed us to clearly separate the resonances of the main metabolites from one another and from the residual signal coming from water and lipids , thus improving specificity in the evaluation of prostate cancer . 
better optimisation of pulse timing could have been achieved by analysing the relaxation times of the metabolite signals [ 15 ] , but this was beyond the scope of our study . at dce - mri , the higher snr was used to increase temporal resolution of acquisitions . 
the possibility of analysing the entire prostate volume with a temporal resolution of 4.7 s for each of the 30 dynamic scans allowed us to accurately study enhancement kinetics in normal and neoplastic tissue . analysis of the results showed that the addition of spectroscopic imaging and dce imaging to anatomical - morradiol med ( 2008 ) 113 : 670688 ne tra malattia confinata e malattia che ha sconfinato oltre il profilo capsulare fattore questultimo di cruciale importanza nella gestione del paziente . 
 sebbene non fosse stato fatto un confronto diretto con i risultati ottenuti con apparecchiatura a 1 , 5 t , le nostre osservazioni hanno suggerito come lutilizzo di campi magnetici pi elevati offra la possibilit di migliorare i valori di accuratezza diagnostica dellimaging morfologico nella determinazione della stadiazione locale di malattia . come abbiamo gi detto anche gli studi spettroscopici in teoria beneficiano grandemente dellimpiego di unalta intensit di campo che determina un incremento della risoluzione spettrale [ 14 ]  . 
lincrementata risoluzione spettrale ha permesso di separare chiaramente le risonanze dei principali metaboliti le une dalle altre e dal segnale residuo proveniente dallacqua e dai lipidi consentendo una migliore specificit nella valutazione del cancro prostatico . 
sarebbe stato possibile raggiungere una pi precisa ottimizzazione del timing degli impulsi della sequenza analizzando i tempi di rilassamento del segnale dei metaboliti [ 15 ] , ma uno studio del genere andava al di l degli scopi del nostro lavoro . 
la possibilit di poter analizzare lintero volume prostatico con una risoluzione temporale di 4 , 7 secondi per ciascuna delle 30 dinamiche ha consentito di analizzare con precisione i parametri cinetici del bolo di contrasto nel tessuto ghiandolare normale ed in quello neoplastico . 
 analizzando i risultati relativi alla popolazione di pazienti studiata emerso come laggiunta dellimaging spettroscopico e di quello dinamico contrastografico alla sola valutazione anatomica - morfologica sia in grado di migliorare laccuratezza diagnostica e la localizzazione del cancro prostatico . 
in effetti , sia i parametri quantitativi della cinesi del contrasto , sia il rapporto ( colina + creatina ) / citrato sono risultati significativamente differenti nella lesione neoplastica rispetto alla zona periferica normale . la possibilit di valutare in maniera precisa il comportamento dinamico del mezzo di contrasto a livello del tessuto prostatico rappresenta uno strumento promettente nella gestione del cancro prostatico in relazione alla capacit di mappare laumentata densit e permeabilit microvasale che si associa con la crescita tumorale maligna . 
dati di letteratura hanno dimostrato come , quando la valutazione dinamica contrastografica associata con limaging morfologico basato sulle sequenze t2 pesate , essa sia in grado di migliorare laccuratezza nella stadiazione del cancro prostatico in particolare nei casi ambigui di sconfinamento capsulare ed invasione delle vescicole seminali [ 16 ]  . 
pi recentemente inoltre stato riportato come in casi individuali il potenziamento massimo valutato in corrispondenza dei voxels nella lesione neoplastica sia sensibilmente pi elevato che nella zona periferica e centrale normale [ 5 ]  . radiol med ( 2008 ) 113 : 670688 phological mri improve the diagnostic accuracy and localisation of prostate cancer . 
in fact , both the quantitative parameters of enhancement kinetics and the ( choline + creatine ) / citrate ratio proved to be significantly different in the neoplastic lesion and normal peripheral zone . the possibility of evaluating precisely enhancement kinetics in prostate tissue is a promising tool in the management of prostate cancer , as it allows mapping of the increased microvascular density and permeability associated with tumour growth . 
literature data have demonstrated that the addition of dce imaging to morphological imaging based on t2 - weighted sequences improves accuracy in prostate cancer staging , in particular in equivocal cases of capsular spread and seminal vesicle invasion [ 16 ]  . 
more recently , it has been reported that in individual cases , the peak enhancement measured in voxels in neoplastic tissue was substantially higher than in the normal peripheral and central zone [ 5 ]  . in assessing the dce - mri study , we first analysed the morphology of the time - intensity curve . 
previous studies have reported that the presence of a curve characterised by a rapid signal increase and early wash - out ( type 1 curve described above ) , like the one typically seen in highly vascular breast cancers , may be used as a diagnostic criterion in prostate cancer also [ 17 ]  . 
however , type 2 curves were predominantly found in both neoplastic and healthy areas , limiting the value of this type of evaluation as a diagnostic criterion . quantitative analysis of dce - mri , on the other hand , demonstrated that prostate cancer has significantly different enhancement patterns from normal tissue . 
studi precedenti hanno evidenziato come la presenza di una curva intensit - tempo caratterizzata da un rapido incremento del segnale ed un rapido wash out ( curva di tipo i descritta precedentemente ) , la quale caratterizza tipicamente i carcinomi mammari fortemente vascolarizzati , possa essere utilizzata come criterio diagnostico anche nel cancro prostatico [ 17 ]  . 
tuttavia una curva di tipo ii stata complessivamente individuata con maggiore frequenza sia nelle zone neoplastiche sia in quelle normali limitando , nella nostra esperienza , il valore di questo tipo di valutazione . 
 ipotizzabile che queste differenze dipendano dallaumentata densit microvasale legata alla neoangiogenesi tumorale [ 18 ]  . risultati discordanti sono presenti in letteratura sul valore che pu essere attribuito al time of arrival nella diagnosi del cancro prostatico [ 619 ]  . 
nei nostri risultati , mediamente la differenza nellinizio del potenziamento tra cancro e zona periferica e centrale stata rispettivamente di 5 , 2 e 4 , 8 secondi , valori che non sarebbero stati evidenziati utilizzando la risoluzione temporale impiegata nello studio di padhani , pari a 910 secondi . 
inoltre egli non aveva utilizzato come standard di riferimento il dato istologico della prostatectomia radicale . nel nostro studio le lesioni tumorali presentavano valori di massima intensit di segnale ( maximum enhancement ) pi elevati rispetto alla ghiandola normale e tali valori venivano raggiunti in un tempo significativamente pi precoce ( time to peak ) ; inoltre il wash in rate ( che ha rilevato la maggiore capacit di discriminare tra tessuto malato e tessuto sano ) era sensibilmente maggiore nel tumore che non nelle aree non tumorali . 
partendo dallassunto che la componente maggiore dellincremento dellintensit di segnale non derivi dal mezzo di contrasto allinterno dei vasi ma dal suo accumulo nello spazio interstiziale , tale parametro riflette per lo pi da una parte la permeabilit vasale e dallaltra lampiezza dello spazio interstiziale . 
 [ 20 ] e confermano come le differenze nelle caratteristiche di potenziamento tra tessuto benigno e maligno siano apprezzate nel modo migliore durante la fase di primo passaggio del contrasto e che una accurata valutazione di questa fase richieda acquisizioni caratterizzate da unelevata risoluzione temporale . 
assuming that the major component of increased signal intensity does not derive from the contrast medium in the blood vessels but rather from its accumulation in the interstitial space , this parameter reflects mostly vascular permeability on the one hand and the size of the interstitial space on the other . 
 [ 20 ] and confirm that differences in enhancement patterns between benign and malignant tissue are best appreciated during the first pass of the contrast bolus and that accurate evaluation of this phase requires acquisitions with a high temporal resolution . 
it is therefore clear that the high temporal resolution achieved in our study as a result of the high snr allows for a more accurate assessment of parameters characterising the initial portion of the time - intensity curve , which as we have seen is most important . analysis of the quantitative parameters of enhancement kinetics obtained in our study showed that although they were significantly different between tumour and normal prostate tissue , they varied widely from patient to patient ( high sd values )  . 
this observation indicates that there is intrinsic individual variability as regards vascular permeability and blood flow in both normal and neoplastic tissue . our study confirms that spectroscopic imaging is able to identify significant differences in the relative levels of citrate , choline and creatine between cancer and normal prostate tissue . 
 [ 22 ] used as an absolute criterion for the determination of cancer a mean ( choline + creatine ) / citrate ratio greater than two or three sd above that in the normal peripheral zone . 
 previous studies have shown that the addition of metabolic data provided by spectroscopy can significantly improve specificity in the intraglandular localisation of cancer compared with conventional morphological imaging with t2 - weighted sequences [ 7 ]  . 
on this subject , it should be recalled that it is difficult to obtain a perfect correspondence between spectroscopy images and histological sections , in part owing to the risk of prostate deformation during fixation and sectioning of the surgical specimen . 
incorrect classification of a healthy portion of gland as a neoplastic area may thus have contributed to that partial overlap of metabolite ratios and quantitative parameters in the spectroscopic and dce - mri acquisitions . the lower spatial resolution of the spectroscopic sedunque come lelevata risoluzione temporale ottenuta nel nostro studio grazie agli alti valori di snr consenta una pi accurata valutazione dei parametri che caratterizzano proprio la porzione iniziale della curva intensit - tempo che abbiamo visto essere la pi importante . dallanalisi dei parametri quantitativi della dinamica contrastografica ottenuti nel nostro studio emerso come , sebbene essi fossero significativamente differenti tra tumore e tessuto ghiandolare normale , essi dimostravano una variabilit piuttosto ampia ( indicata dagli elevati valori di deviazione standard ) da paziente a paziente . 
questa osservazione indica come vi sia unintrinseca variabilit individuale riguardo alla permeabilit vasale e il flusso sanguigno sia nel tessuto normale che in quello neoplastico . il nostro studio conferma come limaging spettroscopico sia in grado di evidenziare significative differenze nei livelli relativi del citrato , colina e creatina , tra il cancro e il tessuto ghiandolare normale . 
 [ 22 ] hanno utilizzato come criterio assoluto per la determinazione del cancro un valore medio del rapporto ( colina + creatina ) / citrato di due o tre deviazioni standard pi elevato rispetto a quello evidenziato nella zona periferica normale . 
in base ai nostri risultati queste soglie corrisponderebbero ad un valore del rapporto ( colina + creatina ) / citrato rispettivamente di 0 , 68 e 0 , 86 il che in sostanziale accordo con quanto individuato da kurhanewicz et al . 
nel nostro studio , tuttavia , stato notato un certo grado di sovrapposizione nei valori dei rapporti tra i metaboliti evidenziati nella zona periferica , in quella centrale e nelle aree neoplastiche . 
a tal riguardo deve essere ricordato come la perfetta corrispondenza tra le immagini di spettroscopia e le sezioni istologiche sia difficile da ottenere anche in relazione alle possibili deformazioni della ghiandola prostatica che possono intervenire durante i processi di fissazione e sezionamento del pezzo operatorio . 
una classificazione non corretta di una porzione ghiandolare sana come area neoplastica pu aver contribuito quindi a quella parziale sovrapposizione dei valori dei rapporti dei metaboliti e dei parametri quantitativi nelle acquisizioni spettroscopica e dce - mri . la pi bassa risoluzione spaziale della sequenza spettroscopica rispetto a quella delle acquisizioni dinamiche ( dimensioni del voxel rispettivamente di 6610 mm e 1 , 131 , 13 mm ) rende la prima poco adatta da sola alla individuazione di tumori molto piccoli sebbene dobbiamo ricordare che tumori con volume inferiore a 0 , 5 ml assumono uno scarso significato clinico . 
 [ 23 ] hanno dimostrato come una valutazione spettroscopica a singolo voxel pu essere combinata con uno studio contrastografico dinamico migliorando potenzialmente laccuratezza diagnostica radiol med ( 2008 ) 113 : 670688 quence compared with the dynamic acquisitions ( voxel size 6610 mm and 1.131.13 mm , respectively ) makes spectroscopy alone unsuitable for identifying very small tumours , even though tumours < 0.5 ml are known to have little clinical significance . 
our study showed that it is feasible to combine , in a single mri session , a high spectral - resolution spectroscopic study with a quantitative evaluation of enhancement kinetics characterised by high spatial and temporal resolution . 
several studies have reported that spectroscopy [ 24 ] and dynamic studies [ 25 ] can be used to monitor response to different treatments capable of acting on cancer metabolism and microvasculature . 
by combining the potential of spectroscopy with that of dce - mri , we can clearly acquire additional and more in - depth knowledge about the metabolic and microvascular changes characterising tumour growth and its response to therapy . as we have seen , a high ( choline + creatine ) / citrate ratio proved to be a more effective criterion than wash - in rate for cancer detection . 
the t2 - weighted sequences provide full anatomical coverage of the prostate with a high level of detail , without appreciable artefacts , with reasonable examination times and sar within the recommended values . 
finally , increased spectral resolution permits accurate evaluation of prostate metabolites and their changes due to malignant transformation . these results lead us to believe that the use of high field strengths expands the potential clinical applications of mri in the evaluation of the prostate gland , marking its transition from a morphological and macroscopic imaging technique to a functional imaging technique , thus making it an increasingly reliable tool in the study of prostate pathology , including cancer . 
further studies on larger patient populations are nonetheless required to confirm our preliminary results and identify the true potential of the technique in the clinical management of patients with prostate cancer . nella localizzazione del cancro prostatico . 
nel presente studio abbiamo dimostrato la fattibilit di eseguire in ununica sessione di risonanza magnetica uno studio spettroscopico ad elevata risoluzione spettrale insieme ad uno di valutazione quantitativa della dinamica del contrasto caratterizzato da unelevata risoluzione spaziale e temporale . 
diversi lavori hanno dimostrato come la spettroscopia [ 24 ] e gli studi dinamici [ 25 ] possono essere impiegati per monitorare la risposta a diversi tipi di trattamenti terapeutici che sono in grado di agire sul metabolismo della neoplasia e sulla sua organizzazione microvasale ; chiaro che combinando le potenzialit offerte dallimaging spettroscopico con quelle della valutazione contrastografica dinamica possibile ottenere nuove e pi profonde conoscenze sui cambiamenti metabolici e microvascolari che caratterizzano la crescita del tumore e la sua risposta alla terapia . 
con le sequenze t2 pesate possibile ottenere una copertura anatomica dellintera prostata con elevato dettaglio anatomico senza apprezzabili artefatti dimmagine ed in un tempo di acquisizione ragionevole e con valori di sar ( specific absorption rate ) contenuti nei limiti stabiliti nelle linee guida . 
laumentata risoluzione spettrale consente infine una accurata valutazione dei metaboliti ghiandolari e delle loro alterazioni legate alla trasformazione neoplastica . questi risultati ci fanno ritenere che lutilizzo di alte intensit di campo magnetico estenda le potenziali applicazioni cliniche della risonanza magnetica nella valutazione della prostata , segnandone il passaggio da un ambito di tipo morfologico e macroscopico ad uno sempre pi legato alla funzione dorgano , facendone , in tal modo , uno strumento sempre pi affidabile nello studio della sua patologia e quindi anche di quella neoplastica . 
zompatori1 1dipartimento di scienze cliniche , sezione di scienze radiologiche , universit degli studi di parma , via gramsci 14 , 43100 parma , italy 2dipartimento di anatomia umana , farmacologia e medicina forense , sezione di anatomia umana , universit degli studi di parma , parma , italy 3dipartimento di scienze chirurgiche , sezione di chirurgia generale e terapia chirurgica , universit degli studi di parma , parma , italy 4dipartimento di medicina sperimentale , sezione di diagnostica radiologica , universit di genova , genova , italy correspondence to : m . 
three - hundred and fifty patients of both sexes ( 150 females , 200 males , age range 076 years , average age 38 years ) underwent mrcp for clinically suspected lithiasic , neoplastic or inflammatory disease of the bile and pancreatic ducts . 
patients were imaged with a 1.5 - t superconductive magnet ( magnetom vision , siemens , erlangen , germany ) , a four - channel phased - array body coil , breath - hold technique , with multislice t2 - weighted half - fourier acquisition single - shot turbo spin echo ( haste ) , mip reconstructions , and a single - shot t2 - weighted turbo - spin - echo sequence rapid acquisition with relaxation enhancement ( rare ) with different slice thicknesses . 
trecentocinquanta pazienti di entrambi i sessi ( 150 f e 200 m ; range di et 076 anni , et media 38 anni ) sono stati sottoposti a cprm per i sospetti clinici di patologia litiasica , neoplastica e flogistica delle vie biliari e pancreatiche . 
stato impiegato un magnete superconduttivo da 1 , 5 t con bobina body phased - array a quattro canali , tecnica breath - hold , acquisizioni half - fourier con t2 - w ( haste ) multislice , ricostruzioni mip , e single shot t2 - w turbo - spin - echo ( rare ) con differente spessore di strato . 
la cprm ha documentato vie biliari e pancreatiche ricorrenti e pertanto considerate normali nel 57 , 7% dei pazienti ; nel restante 42 , 3% ha rilevato varianti anatomiche ( 41% ) ed anomalie congenite ( 1 , 3% )  . 
mrcp identified a double gall bladder in 3% of patients and anatomical variants of the biliopancreatic system in 8.2% : pancreas divisum ( 5.2% ) and a long sphincter of oddi ( 3% )  . 
the congenital anomalies and anatomical variants of the bile and pancreatic ducts present a complex spectrum of frequent alterations , which are worthy of attention in both the clinical and surgical settings and are readily identified by mrcp . keywords bile and pancreatic ducts anatomical variations congenital anomalies mrcp bisegmentario anteriore destro confluente nel dotto biliare di sinistra ( 3 , 1% ) , dotto bisegmentario posteriore destro confluente nel dotto epatico sinistro ( 7 , 9% ) e nel dotto epatico comune ( 3 , 3% )  . 
la presenza di varianti anatomiche delle vie biliari extraepatiche stata riscontrata nell8 , 8% dei pazienti : bassa inserzione del dotto cistico nel dotto epatico comune ( 4 , 5% ) , sbocco del dotto cistico nel dotto epatico destro ( 2 , 7% ) , grosso ramo di secondo ordine drenante nel dotto cistico ( 1 , 6% )  . 
la cprm ha identificato un 3% di pazienti con colecisti doppia ed un 8 , 2% di pazienti con varianti anatomiche del sistema bilio - pancreatico : pancreas divisum ( 5 , 2% ) e sfintere di oddi lungo ( 3% )  . 
le anomalie congenite e le varianti anatomiche delle vie biliari e pancreatiche costituiscono uno spettro complesso di frequenti alterazioni , documentabili agevolmente in cprm e meritevoli di attenzione in ambito sia clinico sia chirurgico . parole chiave vie biliari e pancreatiche varianti anatomiche anomalie congenite cprm introduction introduzione congenital anomalies and variations of the bile and pancreatic ducts are frequent anatomical entities in children and adults . le anomalie congenite e le varianti delle vie biliari e pancreatiche rappresentano entit anatomiche di non infrequente riscontro nei bambini e negli adulti . anatomical variations are defined as anomalies of the course of the bile and pancreatic ducts that are generally asymptomatic , even though they may predispose to pathological conditions [ 1 ]  . 
the most frequent entity of this group ( 13%19% of the population ) is the confluence of right bisegmented posterior bile duct ( rbpbd ) into the left hepatic duct . 
this is followed ( with a frequency of 12% and 11% , respectively ) by the confluence of the anterior branch of the right hepatic duct ( abrhd ) into the left hepatic duct and the triple confluence . 
the most common variation of the pancreatic ducts is the bifid configuration of wirsung and santorini per varianti anatomiche si intendono le deviazioni della normale distribuzione dellalbero biliare e pancreatico che , generalmente , non hanno significato clinico ma che potrebbero predisporre a quadri patologici [ 1 ]  . 
secondo i diversi studi presenti in letteratura , tra le entit presenti in questo gruppo , la pi comune ( dal 13% al 19% circa della popolazione ) la confluenza del dotto epatico bisegmentario posteriore di destra nel dotto epatico di sinistra . 
these anatomical variants tend to be asymptomatic in the majority of cases and only become clinically manifest as a result of the development of complications such as dyskinesia , inflammation , calculosis and jaundice . 
for about 15 years now , it has been possible to carry out noninvasive studies of the bile and pancreatic duct systems by means of magnetic resonance cholangiopancreatography ( mrcp ) through the use of specific sequences available in high - magnetic - field scanners having specific gradients . 
in comparison with mrcp , this method is certainly highly accurate diagnostically but may be complicated by extreme invasiveness [ 8 ] , high risk of complications ( endoluminal bleeding , duodenal perforation , biliary sepsis , bile leak and biliary peritonitis ) [ 9 ] , use of ionising radiation and ionic iodinated contrast medium , failure in 3%10% of cases ( when bile duct canalisation is prevented by technical difficulties or anatomical factors ) , high and level of dependence on the operators skill [ 10 , 11 ]  . 
moreover , mrcp has the great advantage over ercp of documenting the biliary tree proximal to a total obstruction and at the same time allowing tissue evaluation of the liver and pancreas , thus enabling alternative diagnoses . 
dal punto di vista clinico , tutte queste varianti anatomiche delle vie biliari e pancreatiche , nella maggior parte dei casi , sono asintomatiche e si rendono manifeste solo inseguito allo sviluppo di complicanze , quali , discinesie , flogosi , calcolosi ed ittero . per anomalie congenite delle vie biliari e pancreatiche si considerano invece le deviazioni dalla normalit che originano da alterazioni dello sviluppo fetale e che hanno un significato patologico [ 1 ]  . 
secondo i vari studi presenti in letteratura , in questo gruppo le entit anatomiche di pi frequente riscontro nella popolazione sono : la cisti coledocica ed il pancreas divisum [ 2 ]  . 
negli adulti la cisti coledocica presenta una sintomatologia aspecifica che causa ritardo nella diagnosi , mentre nei bambini si manifesta con : dolore addominale , massa palpabile in ipocondrio destro ed ittero [ 3 ]  . 
il pancreas divisum invece pi frequentemente riscontrato in pazienti con dolore addominale cronico e nei pazienti con pancreatite idiopatica o con pancreatiti ricorrenti [ 46 ]  . la conoscenza da parte di chirurghi e radiologi , della presenza , nei singoli pazienti , di queste varianti anatomiche ed anomalie congenite , pu evitare gravi danni iatrogeni ; ad esempio : dotti biliari accessori o aberranti possono predisporre ad una inavvertita legatura duttale durante un intervento di colecistectomia laparoscopica con conseguenti complicanze anatomo - cliniche ( coliche biliari , calcolosi , atrofia dei segmenti epatici tributari dei dotti epatici legati , colangiti , ecc )  . 
 la conoscenza di tali varianti anatomiche delle vie biliari , in pazienti che si sottopongono ad interventi di colecistectomia laparoscopica , di resezione epatica sinistra o di trapianto di fegato , importante nel planning chirurgico perch pu prevenire inavvertite lesioni duttali responsabili di gravi complicanze o che inficiano il buon esito dellintervento , ed inoltre pu evitare errori diagnostici [ 7 ]  . 
recentemente , ad un maggior riconoscimento di queste entit ha contribuito lo sviluppo tecnologico nel campo dellimaging radiologico . da circa 15 anni lo studio non invasivo dei sistemi duttali biliari e pancreatici pu essere effettuato con colangiopancreato - rm ( cprm ) mediante limpiego di specifiche sequenze presenti nelle apparecchiature ad alto campo magnetico , dotate di gradienti performanti . 
tale metodica sicuramente dotata di una elevata accuratezza diagnostica , ma , rispetto alla cprm , gravata da : unelevata invasivit [ 8 ] ; un elevato rischio di complicanze ( sanguinamento endoluminale , perforazione duodenale , sepsi biliare , bile leak e peritonite biliare ) [ 9 ] ; impiego di radiazione 844 radiol med ( 2008 ) 113 : 841859 our study describes mrcp findings , assessing the epidemiology and discussing the clinical and surgical implications of possible anatomical variations and abnormalities of the intraand extrahepatic bile ducts and main pancreatic duct in a sample of 350 patients undergoing mrcp for a clinical suspicion of lithiasic , neoplastic and inflammatory disease of the intraand extrahepatic bile ducts . materials and methods from february 2004 to february 2007 , two radiologists ( mdf and ns ) , with 10 and 8 years of experience in mrcp , respectively , prospectively evaluated 350 mrcp examinations carried out on patients of both sexes ( 150 females and 200 males , age range 076 years , average age 38 years ) with clinical symptoms of lithiasic , inflammatory or neoplastic disease of the biliary and pancreatic systethe results obtained were used to calculate the degree of interobserver agreement . 
anatomical variations were defined as variants in outlet location , length and course of the intraand extrahepatic bile ducts , variants in the number of gall bladders , pancreas divisum and a long sphincter of oddi . congenital anomalies of the bile pathways were defined as choledochal cysts , biliary hamartomatosis and bile duct atresia ( both intrahepatic and of the carrefour ) ; annular pancreas was considered as a congenital anomaly of the pancreatic pathways . mrcp was carried out with a 1.5 - t superconductive magnet ( magnetom vision ; siemens , erlangen , germany ) with a 40 mt / m gradient and a four - channel body phasedarray coil . 
with the exception of a 20 - day - old patient , who was breastfed 2 h before the mrcp examination , all patients fasted for at least 6 h to enable filling and optimal visualisation of the bile ducts and gall bladder . 
to suppress the signal produced by the gastric contents and the first loops of the small intestine , patients were administered approximately 150 ml of a superparamagnetic contrast medium ( lumirem , guerbet laboratories , france ) 30 min before the examination . 
la cprm presenta , rispetto alla ercp , il grande vantaggio di documentare lalbero biliare a monte di una eventuale ostruzione serrata e consente contestualmente anche una valutazione tissutale del fegato e del pancreas , permettendo cos la possibilit di diagnosi alternative . 
sulla scorta di quanto affermato , nel nostro studio , non stata impiegata la ercp per la conferma della presenza di varianti e di anomalie anatomiche delle vie biliari e pancreatiche riscontrate in cprm . 
 lo scopo del nostro studio stato triplice : descrivere gli aspetti cprm , valutare lepidemiologia e discutere le ricadute clinico - chirurgiche delle possibili varianti ed anomalie anatomiche delle vie biliari intraed extra - epatiche e del dotto pancreatico principale , in un campione di 350 pazienti ( studiati con per i sospetti clinici di patologia litiasica , neoplastica e flogistica delle vie biliari intraed extra - epatiche )  . materiali e metodi due radiologi ( mdf ed ns ) , rispettivamente con 10 ed 8 anni di esperienza in cprm imaging , hanno valutato in cieco 350 esami cprm , eseguiti in pazienti consecutivi di entrambi i sessi ( 150 f e 200 m ; range di et 076 anni , et media 38 anni ) , con sospetti clinici di patologia litiasica , flogistica o neoplastica del sistema biliare e pancreatico , nel periodo compreso tra febbraio 2004 e febbraio 2007 . 
i risultati ottenuti sono stati poi utilizzati per il calcolo della concordanza tra i due radiologi ( interobserver - agreement )  . sono state considerate varianti anatomiche le variazioni di sbocco , lunghezza e decorso delle vie biliari intraed extraepatiche , le variazioni di numero della colecisti , il drenaggio del dotto cistico , il pancreas divisum e lo sfintere lungo di oddi . 
abbiamo considerato anomalie congenite delle vie biliari le cisti coledociche , gli amartomi e le atresie delle vie biliari ( nelle due forme : intra - epatica e del carrefour biliare ) ; per anomalie congenite delle vie pancreatiche si considerato il pancreas anulare . 
 gli esami cprm sono stati ottenuti con apparecchiatura dotata di magnete superconduttivo da 1 , 5 tesla ( magnetom vision , siemens , erlangen , germania ) gradienti 40 mt / m , con bobina body phased - array a 4 canali . 
i pazienti sono stati tenuti a digiuno da almeno 6 ore , per favorire il riempimento e lottimale visualizzazione delle vie biliari e della colecisti , fatta eccezione per un paziente di 20 giorni di vita che era stato allattato due ore prima dellesame cprm . con lo scopo di annullare il segnale prodotto dal contenuto gastrico e dalle prime anse dellintestino tenue , 30 minuti prima dellesecuzione dellesame , ai pazienti a digiuno , sono stati somministrati per os 150 ml circa di un mezzo di radiol med ( 2008 ) 113 : 113 : 841859 the region of interest ( roi ) and the patients build . 
with the multislice technique , half - fourier acquisition single - shot turbo spin echo ( haste ) sequences were obtained with a half - fourier single - shot technique ( tr ms / te ms ratio = 95 ; flip angle 150 ; echo train length 128 ; fov 270270 mm , number of signals acquired = 1 ; matrix of 220256 with 4 - mm slice thickness without gap )  . 
examinations in oncological patients were completed with fat - sat 3d t1 gradient - echo sequences during the intravenous injection of gadolinium diethylene triamine pentaacetate acid ( dtpa ) ( 0.2 ml / kg )  . 
the images obtained were reconstructed using an mip 3d algorithm in the coronal plane . statistical analysis the interobserver agreement in identifying the anatomical variations and congenital anomalies of the bile and pancreatic pathways was calculated using the weighted kappa statistic ( ) [ 12 ] ; values < 0 indicate insufficient agreement , 00.2 low agreement , 0.210.40 fair agreement , 0.410.60 moderate agreement , 0.610.80 substantial agreement and 0.811.0 almost perfect agreement [ 13 ]  . 
dopo le acquisizioni scout , stata eseguita una sequenza gradient - echo ( fast imaging steady state procession fisp , tr 4 , 8 ms , te 2 , 3 ms , ritardo 200 ms , flip angle 70 gradi , ampiezza di banda 650 hz per pixel ) sul piano coronale al fine di localizzare lilo epatico . successivamente sono state usate due differenti tecniche a respiro sospeso per lacquisizione dei dati : una di tipo single - shot con acquisizione di singole slice ( projection technique ) e laltra di tipo multislice 2d con post - processing in maximum intensity projection ( mip )  . 
con la prima tecnica , stata effettuata una colangiopancreatografia mediante impiego di sequenze turbo spin echo ( se ) fortemente t2 pesate ( tr 2800 ms , te 1100 ms , matrice di 240256 , lunghezza dellecotreno 240 ) con soppressione del segnale del grasso , avente spessore di strato di 70 mm e campo di vista ( fov ) variabile da 25 a 30 cm in relazione allarea dinteresse ed alla costituzione del paziente . 
con tecnica multislice , invece , sono state eseguite sequenze turbo spin - echo ( haste ) , con tecnica single - shot half - fourier ( rapporto tr ms / te ms = 95 ; flip angle 150 gradi ; lunghezza dei treni deco 128 ; fov 270270 mm ; numero dei segnali acquisiti = 1 ; matrice di 220256 con spessore di strato di 4 mm senza gap ) ; sono stati acquisiti 15 strati contigui , durante una singola apnea della durata di 20 secondi , secondo un piano parallelo allasse longitudinale della via biliare principale . 
alcuni esami , in pazienti oncologici , sono stati completati con sequenze gradient echo 3d t1w fat - sat durante somministrazione in vena periferica di mezzo di contrasto gadolinium - dtpa administration ( 0 , 2 ml / kg )  . 
le immagini ottenute sono state ricostruite con algoritmo mip 3d sul piano coronale . analisi statistica linterobserver agreement tra i due radiologi per la individuazione delle varianti anatomiche e delle anomalie congenite delle vie biliari e pancreatiche stato valutato mediante il kappa statistico calcolato come un - weighted kappa ( ) [ 12 ]  . 
 risultati i risultati del nostro studio sono riassunti nella tabella 1 . dei 350 pazienti esaminati , il 57 , 7% ( n = 202 ) presentava 846 radiol med ( 2008 ) 113 : 841859 table 1 number and percentage of patients with normal magnetic resonance cholangiopancreatography ( mrcp ) findings and patients with anatomical variants and congenital anomalies of the biliopancreatic system number of patients percent values ( % ) normal mrcp findings anatomical variations a . 
a fat saturation ( fat - sat ) t2 turbo spin echo ( tse ) ( thickness 7 cm ) , coronal view : large arrow shows the outlet of the rbabd into the left hepatic duct ; concomitant interruption of the intermediate segment of the main bile duct due to the presence of a tumour of the head of the pancreas ( asterisk )  . 
in a tse t2 fat - sat ( spessore di strato 7 cm ) , in sezione coronale , la freccia grande indica lo sbocco del dbad nel dotto epatico sinistro ; concomita interruzione del tratto intermedio della via biliare principale per la presenza di tumore della testa del pancreas ( asterisco )  . 
in b e c tse t2 ( spessore di strato 5 mm ) , rispettivamente in sezione assiale e coronale , e d tse t2 fat - sat ( spessore di strato 7 cm ) , in sezione coronale : sbocco del dbad nel dotto epatico sinistro , clampato erroneamente durante la laparoscopia . 
4a - c fat saturation ( fat - sat ) t2 turbo spin echo ( tse ) ( thickness 7 cm ) , coronal view . outlet of the right posterior bisegmentary bile duct ( rbpbd ) into the common hepatic duct . a regular outcome of cholecystectomy ( the presence of the anatomic variant was known to the surgeon )  . 
b iatrogenic substenosis of the rbpbd ( arrow ) : during laparoscopic cholecystectomy , the rbpbd was partially clamped ( the presence of the anatomic variant was unknown to the surgeon )  . 
in b si osserva substenosi iatrogena del dbpd ( freccia ) : durante lintervento di colecistectomia per via laparoscopica il dbpd era stato parzialmente clampato ( la presenza della variante anatomica non era nota al chirurgo )  . 
nel nostro studio emersa la presenza di varianti anatomiche delle vie biliari intraed extra - epatiche nel 29 , 8% dei pazienti , alterazioni congenite della colecisti nel 3% e varianti del sistema duttale pancreatico nel 5 , 2% dei casi ; la frequenza delle anomalie congenite emersa stata complessivamente di circa 1 , 3% . 
tali dati non si discostano dalle percentuali riportate nella letteratura internazionale ( tabella 2 ) sia per le varianti anatomiche sia per le anomalie congenite delle vie biliari e pancreatiche [ 1 , 2 , 14 ]  . le varianti anatomiche di prevalente interesse chirurgico sono relative a variazioni di numero e posizione per quanto riguarda la colecisti e a variazioni di sbocco , lunghezza e decorso per ci che concerne le vie biliari intraed extrafig . 
generalmente ( nel 60% dei casi circa ) il dotto epatico destro e quello sinistro convergono allilo epatico per formare il dotto epatico comune ; il dotto epatico destro ha due rami principali : anteriore ( per i segmenti v e viii ) e posteriore ( per i segmenti vi e vii )  . 
il dotto epatico sinistro ha il ramo mediale e laterale per i segmenti ii e iii ricevendo anche dotti dai segmenti i e iv [ 1 ]  . quando il dbpd converge nel dotto epatico sinistro piuttosto che immettersi nel dotto epatico destro , crea una variante anatomica ( crossover anomaly ) [ 7 ] ; analogamente il dbad , anzich confluire con il dbpd nel dotto epatico destro , pu confluire nel dotto biliare di sinistra [ 15 , 16 ] ; altra variante lassenza del dotto biliare destro ; ci comporta che il ramo anteriore e posteriore di destra confluiscono direttamente nel il dotto epatico sinistro ( triforcazione ) [ 11 ] ; queste ultime tre varianti anatomiche hanno significato chirurgico quando si preveda unepatectomia sinistra ( neoplasie , trapianti , ecc . ) ; in tal caso la sutura epatica sarebbe responsabile della legatura delle varianti anatomiche determinando una inevitabile cirrosi biliare del vi - vii o del v - viii segmento [ 11 ] ; non raro lo sbocco del dbpd nel dotto epatico comune , in corrispondenza dello sbocco distale del dotto cistico [ 11 , 17 ]  . 
se tale variante misconosciuta al chirurgo per una mancata segnalazione nella valutazione pre - operatoria con cprm , durante intervento di colecistectomia per via laparoscopica , al clampaggio del fig . 
in a presenza di due colecisti con drenaggi indipendenti nella via biliare principale ; in b colecisti con setto endoluminale che mima una doppia colecisti avente unico dotto cistico . radiol med ( 2008 ) 113 : 113 : 841859 fig . 
9a - e pancreas divisua incomplete pancreas divisum and b complete pancreas divisum are shown by half - fourier acquisition single - shot turbo spin echo ( haste ) sequences and maximum intensity projection ( mip ) reconstruction . 
schematic representation of c incomplete and d complete variants of the pancreas divisue incomplete pancreas divisum , axial view ( t2 turbo spin echo ; thickness 5 mm ) : outlet of the main pancreatic duct ( large arrow ) into the papilla minor . 
rappresentazione schematica delle varianti incompleta ( c ) e completa ( d ) del pancreas divisu in e pancreas divisum incompleto osservato in sezione assiale ( tse t2w ; spessore di strato 5 mm ) : il dotto pancreatico principale ( freccia lunga ) drena nella papilla minor . 
la freccia corta indica la comunicazione tra il dotto pancreatico maggiore e quello minore ( pancreas divisum incompleto )  . the presence of congenital anomalies was observed in 1.3% ( 4 ) of patients . 
il risultato di tale danno iatrogeno la persistenza di coliche biliari con inevitabile litiasi biliare intraepatica e tardivamente atrofia del vi e del vii segmento epatico ( circa il 60% del volume del lobo epatico destro )  . 852 radiol med ( 2008 ) 113 : 841859 fig . 
12a , b t2 turbo spin echo ( tse ) , a oblique coronal view and b axial view : atresia of the biliary pathways in 20 days old male . 
il dotto cistico solitamente si innesta con una certa angolatura nel dotto epatico comune ( talora pu essere parallelo o avere decorso a spirale ) decorrendo a destra dellarteria epatica ; il punto di confluenza pi comunemente riradiol med ( 2008 ) 113 : 113 : 841859 fig . 
si noti in c la scarsa impregnazione di mdc dei noduli ( sequenze ge fat - sat t1 w )  . scontrato a livello della porzione del dotto epatico comune compresa tra la convergenza dei dotti epatici di destra e di sinistra e lorigine del coledoco retroduodenale . 
in tale ambito , leventuale presenza di bassa inserzione del dotto cistico nel dotto epatico comune , sbocco del cistico nel dotto epatico destro ( molto raro , tuttavia presente nella nostra casistica ) , il drenaggio di un grosso ramo di secondo ordine nel dotto cistico o del dotto epatico destro nel cistico ( assai raro ) [ 17 ] , devono essere opportunamente segnalati nel referto di una cprm [ 18 ]  . tali varianti nel corso di un intervento di colecistectomia laparoscopica sono di difficile riconoscimento : il dotto epatico comune o il dotto epatico di destra possono essere confusi con il dotto cistico . 
il clampaggio erroneamente alto del dotto cistico drenante in corrispondenza nel coledoco terminale , in corso di colecistectomia laparoscopica , come abbiamo osservato in un caso , pu essere responsabile di persistenza di coliche biliari per il ristagno di bile , favorendo inoltre la formazione di calcoli . 
in our series , anatomical variants of the intraand extrahepatic bile ducts were demonstrated in 29.8% of patients , congenital anomalies of the gall bladder in 3% and variations of the principal pancreatic duct in about 5.2% ; the overall frequency of congenital anomalies was approximately 1.3%. 
these data are consistent with the reported rates of anatomical variants and congenital anomalies of the bile and pancreatic pathways ( table 2 ) [ 1 , 2 , 7 , 14 ]  . anatomical variants of major surgical interest involve variations in the number and position of the gall bladder and variations in outflow , length and course of the intra854 radiol med ( 2008 ) 113 : 841859 table 2 correlations between percentages of principal anatomical variations of bile pathways demonstrated in our study and percentages reported in the literature de filippo et al . 
in our experience , the anatomical variants of the intrahepatic bile ducts most frequently involve drainage of the anterior and posterior segments of the right liver lobe , as reported in the literature . generally ( in about 60% of cases ) , the right and left hepatic ducts converge into the hepatic hilum to form the common hepatic duct . 
the right hepatic duct has two main branches , the anterior branch ( for the v and viii segments ) and the posterior branch ( for the vi and vii segments )  . 
the left hepatic duct has the medial and lateral branch for segments ii and iii , and also receives the ducts from segments i and iv [ 1 ]  . when the rbpbd converges into the left hepatic duct instead of entering the right hepatic duct , it forms an anatomical variant ( crossover anomaly ) [ 7 ] at the same time , the abrhd can flow into the left bile duct instead of converging with the rbpbd into the right hepatic duct [ 15 , 16 ] another variant is the absence of the right bile duct , which causes the right anterior and posterior branches to converge directly with the left hepatic duct ( trifurcation ) [ 11 ] the latter three anatomical variants have surgical significance when a left hepatectomy is programmed ( neoplasm , transplant , etc . ) ; in this case , the hepatic suture will be responsible for ligation of the anatomic variants , leading to inevitable liver cirrhosis of the vivii or the vviii segments [ 11 ] the flow of the rbpbd into the common hepatic duct at the level of the distal outlet of the cystic duct is not rare [ 11 , 17 ]  . 
 possible variants of the confluence of the two main hepatic ducts and cystic duct are also particularly important . the cystic duct usually joins the common hepatic duct at a certain angle ( it may also run parallel or have a spiral course ) , coursing to the right of the hepatic artery ; the most common point of confluence is at the level of the segment of the common hepatic duct between the convergence of the left and right hepatic ducts and the origin of the retroduodenal bile duct . 
in this situation , the possible low insertion of the cystic duct into the common hepatic duct , the outlet of the cystic duct into the right hepatic duct ( very rare ) , draining of a large second - order - branch hepatic duct into the cystic duct or of the right hepatic duct into the cystic duct ( extremely rare ) [ 17 ] must be appropriately noted in the mrcp report [ 18 ]  . 
le complicanze associate a colecisti doppia includono la calcolosi , la torsione e lo sviluppo di papilloma , carcinoma , ostruzione del dotto comune e cirrosi biliare secondaria [ 20 ]  . 
le varianti anatomiche della doppia colecisti sono ancora differenziate secondo la classificazione di boyden [ 21 ] : colecisti esternamente normale ma divisa internamente da un setto longitudinale ; colecisti bifida dalla quale emerge un unico dotto cistico ; doppia colecisti con due dotti cistici che si uniscono a formare un dotto comune prima della confluenza nel dotto epatico ; doppia colecisti con due dotti cistici drenanti separatasuch variants are difficult to recognise during laparomente nel dotto epatico comune . 856 radiol med ( 2008 ) 113 : 841859 scopic cholecystectomy : the common hepatic duct or the right hepatic duct can be confused with the cystic duct . 
this can result in the erroneous ligation or rupture of the common hepatic duct or the right hepatic duct , the latter responsible for bile leakage [ 11 ]  . 
the erroneous high ligation of the cystic duct in correspondence with the terminal common bile duct during laparoscopic cholecystectomy , observed in one case in our series , can be responsible for persistent pain due to bile stagnation and promote the production of bile stones . one anatomical variant observed in our study , which causes important clinical , diagnostic and surgical problems , is a double gall bladder ; this variant has an incidence of one subject in 4 , 000 [ 19 ]  . 
the complications associated with a double gall bladder include calculosis , torsion and development of papilloma , carcinoma , obstruction of the common bile duct and secondary bile cirrhosis [ 20 ]  . 
the anatomical variants of a double gall bladder are still differentiated according to the boyden classification [ 21 ] : externally normal gall bladder divided internally by a bifid gall bladder from which a single cystic duct longitudinal septum emerges double gall bladder with two cystic ducts that unite to form a common duct before the confluence into the hepatic duct double gall bladder with two cystic ducts draining separately into the common hepatic duct the preoperative diagnosis of double gall bladder is fundamental , especially if laparoscopic cholecystectomy is programmed . 
if the surgeon is not informed of the presence of this variant , the second gall bladder may be disregarded , particularly if it is infrahepatic , with the risk of another surgical operation [ 22 ]  . moreover , our study revealed some anatomical variants of the biliopancreatic system , such as pancreas divisum and variations in the confluence of the pancreatic ducts . 
the head and the uncinate process are drained by the duct of wirsung , which terminates in the papilla major ; the body and tail are drained by the duct of santorini , which opens into the duodenum via the papilla minor [ 23 ]  . 
according to one hypothesis , in pancreas divisum , there is a mismatch between the calibre of the main pancreatic duct draining the secretions of the pancreatic body and tail and the small diameter of the minor papilla , a situation that results in slow flow or blockage of pancreatic secretions and chronic stasis . 
la freccia lunga indica il clampaggio accidentale del dbpd associata al clampaggio del dotto cistico , durante lintervento di colecistectomia laparoscopica . la diagnosi preoperatoria di colecisti doppia fondamentale soprattutto se in previsione di un intervento di colecistectomia laparoscopica : qualora il chirurgo non sia informato sulla presenza di tale variante pu trascurare la seconda colecisti , soprattutto se infraepatica , rischiando il paziente un secondo intervento [ 22 ]  . dallo studio sono emerse inoltre varianti anatomiche del sistema biliopancreatico quali pancreas divisum e varianti nella confluenza dei dotti pancreatici . 
la testa ed il processo uncinato vengono drenati dal dotto di wirsung , che termina nella papilla major ; il corpo e la coda sono invece drenati dal dotto di santorini , che si apre nel duodeno attraverso la papilla minor [ 23 ]  . 
stata avanzata lipotesi che nel pancreas divisum vi sia unincongruenza tra il calibro del dotto pancreatico principale , drenante il volume di secreti del corpo e della coda del pancreas , ed il piccolo calibro della papilla minor ; ci determinerebbe rallentamenti o ingorghi cronici del flusso del secreto pancreatico . 
high pressure inside the pancreatic duct associated with the lack of an efficient ductal sphincter allows free reflux of enzymes within the biliary tree , which , by weakening the bile - duct wall , can lead to the formation of a choledochocele [ 2 , 14 ]  . 
this anatomical variant should be diagnosed and treated surgically by means of endoscopic sphincterotomy before the onset of complications , such as parietal bile duct alterations , pancreatitis or the development of cholangiocarcinoma [ 24 ]  . in particular , the endoscopist will require data on the length of the sphincterial canal in order to perform a correct sphincterotomy , thus preventing possible recurrences of complications and a repeat operation . 
our study included cases of choledochal cysts , hamartomas and atresia of the bile pathways . choledochal cysts refer to a congenital cystic dilatation of any portion of the principal extrahepatic bile pathway , most commonly located in the principal portion of the bile duct . 
pure rare intrahepatic variations of carolis disease such anatomical conditions must be surgically corrected , as they present a very high risk of malignant degeneration into cholangiocarcinoma , onset of pancreatitis , development of recurrent cholangitis and rupture with subsequent biliary peritonitis [ 25 ]  . atresia of the biliary pathways is the most frequent indication for liver transplantation in children . 
lalta pressione allinterno del dotto pancreatico associata alla mancanza di uno sfintere duttale efficiente consente il libero reflusso di enzimi nellalbero biliare che , indebolendo la parete del coledoco , pu portare alla formazione di coledococele [ 2 , 14 ]  . 
tale variante anatomica dovrebbe essere diagnosticata e trattata mediante sfinterotomia per via endoscopica prima dellinsorgenza di complicanze quali alterazioni parietali coledociche , pancreatiti e sviluppo di colangiocarcinomi [ 24 ]  . 
in particolare , il dato sulla lunghezza del canale sfinteriale importante per lendoscopista al fine di effettuare una corretta sfinterotomia , prevenendo possibili recidive di complicanze e quindi il ricorso ad un reintervento . 
nel nostro studio sono stati riscontrati cisti coledociche , amartomi e atresia delle vie biliari . la cisti coledocica una dilatazione cistica congenita di una qualsiasi porzione della via biliare principale extraepatica , pi comunemente localizzata nella porzione principale del coledoco . 
rara variante intraepatica pura della malattia di caroli . tali condizioni anatomiche devono essere corrette chirurgicamente dal momento che il rischio di degenerazione maligna in colangiocarcinoma , di insorgenza di pancreatiti , di sviluppo di colangiti ricorrenti , di rottura con successiva peritonite biliare molto alto [ 25 ]  . 
for a definitive diagnosis , however , microhistological examination is necessary . we did not observe cases of annular pancreas , a rare congenital anomaly characterised by the incomplete rotation of the apical part of the ventral bud of the pancreas with the development of a ring of pancreatic tissue around the second portion of the duodenuthis induces variable compression on the duodenum up to its complete obstruction . 
the condition may be symptomatic at birth , with symptoms mostly relating to duodenal obstruction ; in these cases , the condition is quite often associated with other congenital anomalies . 
in adults , symptoms may be different ( abdominal pain , nausea and vomiting are the most frequent ) and are often associated with peptic ulcer , obstructive jaundice , duodenal obstruction and pancreatitis . 
the definitive diagnosis is often established during laparoscopy or laparotomy [ 27 ]  . in conclusion , congenital anomalies and anatomic variants of the bile and pancreatic pathways present a complex range of frequent alterations that are easily documented with mrcp and that deserve attention in both surgical and clinical settings . nigna del fegato riscontrata solitamente allautopsia o occasionalmente in corso di interventi chirurgici . 
il pancreas anulare , di fatto unanomalia congenita rarissima , caratterizzata da unincompleta rotazione della parte apicale della gemma ventrale del pancreas , con sviluppo di un anello di tessuto pancreatico attorno alla seconda porzione del duodeno ; ci induce un grado variabile di compressione sul duodeno fino allostruzione . 
una condizione che pu essere sintomatica alla nascita : la sintomatologia legata nella maggioranza dei casi allostruzione del duodeno ; in questi casi spesso presente associazione con altre anomalie congenite . 
in et adulta i sintomi sono variabili ( dolore addominale , nausea e vomito sono i pi frequenti ) e spesso legati a patologie associate : ulcera peptica , ittero ostruttivo , ostruzione duodenale , pancreatite . 
cova1 1unit clinica operativa di radiologia , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , 34149 trieste , italy 2unit clinica operativa di psichiatria , universit degli studi di trieste , via p . 
ralli 5 , 34100 trieste , italy 3brain center for neuroscience , universit degli studi di trieste , via fleming 22 , 34100 trieste , italy correspondence to : m . 
gli esami di rm sono stati eseguiti con un magnete da 1 , 5 t mediante sequenze convenzionali e una sequenza pesata in diffusione con tensori applicati secondo 32 direzioni . 
stata valutata lanisotropia frazionaria ( fa ) a livello della sostanza bianca frontale , parietale , occipitale e temporale nonch a livello dello splenio e del ginocchio del corpo calloso . 
emersa una differenza statisticamente significativa a livello dello splenio per quanto riguarda la fa tra i soggetti con mci ed i controlli ( p < 0 , 007 ) e tra soggetti con ad ed i controlli ( p < 0 , 05 ) , a livello del ginocchio tra i controlli e i soggetti con ad ( p < 0 , 016 ) e a livello della sostanza bianca frontale destra fra controlli e soggetti con ad ( p < 0 , 024 )  . 
lutilizzo dei tensori di diffusione nei pazienti con ad e mci consente una precoce valutazione 916 radiol med ( 2008 ) 113 : 915922 of white - matter damage in patients with mci and ad . 
i valori di dti correlano con i test neuropsicologici . keywords alzheimers disease diffusion tensor imaging magnetic resonance parole chiave malattia di alzheimer tensori di diffusione risonanza magnetica introduction introduzione dementias are chronic degenerative diseases , the incidence of which are destined to increase exponentially over the next decades , leading to a rise in health care and social expenditure required to address clinical , management and therapeutic aspects . 
alzheimers disease ( ad ) is the most common form of dementia [ 1 ] , and it is characterised by a progressive destruction of neuronal function , leading to deterioration of cognitive and functional abilities and to behavioural changes . 
mild cognitive impairment ( mci ) refers to a dynamic situation characterised by both objective and subjective memory impairment that may or may not progress to full - blown ad [ 1 ]  . 
 there is a need to establish an accurate and early clinical and imaging diagnosis to be able to initiate , whenever possible , pharmacological treatment and / or rehabilitation programmes . 
pathological studies have shown that not only the grey matter but also the white matter is extensively involved in patients with ad and mci and that the alterations are present well before the onset on clinical symptoms [ 24 ]  . 
new imaging techniques are therefore needed that are capable of detecting brain alterations at an early stage . the purpose of our study was to evaluate possible white matter alterations in patients with ad and mci by using magnetic resonance ( mr ) diffusion tensor imaging ( dti )  . le demenze sono delle patologie cronico - degenerative destinate ad avere nel corso dei prossimi anni un incremento esponenziale con un conseguente aumento della spesa sanitaria e sociale derivanti dalla gestione di aspetti clinici , gestionali e terapeutici . 
la malattia di alzheimer ( ad ) rappresenta attualmente la forma pi comune di demenza [ 1 ] ed caratterizzata da una progressiva distruzione della funzionalit neuronale con conseguente deterioramento delle funzioni cognitive , delle capacit funzionali e da modificazioni comportamentali . 
il mild cognitive impairment ( mci ) rappresenta invece una situazione dinamica durante la quale i soggetti presentano disturbi mnesici sia oggettivi che soggettivi e che pu o meno evolvere verso un ad conclamato [ 1 ]  . 
 da tutto ci si evince che si sentita la necessit , negli ultimi anni , di una diagnosi sia clinica che strumentale sempre pi precisa e precoce per poter , dove possibile , intraprendere una terapia farmacologica e / o riabilitativa . 
numerosi studi anatomopatologici hanno evidenziato come non solo la sostanza grigia ma anche la sostanza bianca sia estesamente coinvolta dal processo patologico nei soggetti con ad e mci e che tali alterazioni sono presenti ben prima dellinsorgenza dei sintomi clinici [ 24 ]  . 
 lo scopo del nostro lavoro stato quello di valutare mediante risonanza magnetica ( rm ) con tensori di diffusione ( dti ) le alterazioni della sostanza bianca in soggetti con ad e in soggetti con mci . materials and methods we studied 47 subjects , including 14 patients with mild ad according to the diagnostic and statistical manual of mental disorders , fourth revision ( dsm - iv ) of the american psychiatric association , 15 patients with amnestic mci according to petersens criteria [ 5 , 6 ] , and 18 healthy controls . 
 all subjects underwent an accurate neurological and neuropsychological evaluation consisting of the mini - mental status examination ( mmse ) , adjusted for age and schooling , and other tests assessing memory function , executive materiali e metodi nel presente studio sono stati valutati complessivamente 47 soggetti e precisamente 14 pazienti con diagnosi di malattia di alzheimer di grado lieve secondo i criteri del dsm - iv ( diagnostic and statistical manual of mental disorders , american psychiatric association ) , 15 pazienti con diagnosi di mild cognitive impairment di tipo amnesico secondo i criteri di petersen [ 5 , 6 ] e 18 soggetti sani di controllo . 
in particolare tutti i soggetti sono stati sottoposti al mini mental status examination ( mmse ) test corretto per et e scolarit e a ulteriori test atti a valutare le funzioni mnesiche , le funzioni esecutive ed il ragionamento . 
an initial morphological study was obtained in the axial and coronal planes , with t1 - weighted ( tr / te = 786 / 15 ms ) , proton - density - weighted and t2weighted ( tr / te = 2 , 780 / 2080 ms ) spin echo ( se ) sequences . 
diffusion - weighted ( dw ) mri was subsequently performed with b values of 0 and 1 , 000 mm2 / s and gradients applied in 32 directions ( 40 slices , slice thickness 2 mm , interslice gap 0 ; tr = 7895 ms , te = 92 ms , flip angle = 90 , number of echoes = 1 , scan time = 5 min )  . 
data sets were processed on a dedicated workstation with the dtistudio programme ( version 2.4 ) [ 7 ] developed by susumu mori ( john hopkins , baltimore , md , usa )  . 
the manual placement of 0.8 - cm2 regions of interest ( rois ) allowed us to measure fractional anisotropy in the white matter of the genu and splenium of the corpus callosum , and of the frontal , temporal , occipital and parietal regions bilaterally . statistical analysis of comparisons between groups ( mci vs controls , mci vs ad , and ad vs controls ) was done with the nonparametric mann - whitney u test . 
le principali caratteristiche cliniche dei tre gruppi sono riportate nella tabella 1 . tutti i soggetti sono stati sottoposti ad un esame di risonanza magnetica mediante apparecchiatura operante a 1 , 5 t con gradienti pari a 30 mt / m e slew - rate pari a 150 mt / m / s ( intera master , philips , best , olanda )  . 
in tutti i soggetti stato eseguito uno studio morfologico mediante piani di scansione assiali e coronali con sequenze se pesate in t1 ( tr / te = 786 / 15 ms ) , densit protonica e t2 ( tr / te = 2780 / 2080 ms )  . 
in tutti i soggetti stata successivamente eseguita una sequenza pesata in diffusione con valori di b pari a 0 e 1000 mm2 / s con gradienti sensibilizzati alla diffusione applicati in 32 direzioni dello spazio ( 40 strati , spessore di strato pari a 2 mm , gap tra gli strati pari a 0 ; tr = 7895 ms , te = 92 ms , flip angle = 90 , numero di echi = 1 , tempo di scansione = 5 min )  . 
i dati cos ottenuti sono stati elaborati su una consolle separata mediante lutilizzo del programma dti studio ( versione 2.4 ) [ 7 ] sviluppato da susumu mori ( john hopkins , baltimore , usa )  . 
mediante il posizionamento manuale di regioni di interesse delle dimensioni pari a 0 , 8 cm2 stata ottenuta lanisotropia frazionaria della sostanza bianca del ginocchio e splenio del corpo calloso , delle regioni frontali , delle regioni temporali , occipitali e parietali bilateralmente . 
 la valutazione statistica per quanto riguarda il confronto tra gruppi ( mci vs controlli , mci vs ad e ad vs controlli ) stata eseguita con il test non parametrico mann whitney - u . 
dal confronto tra i soggetti di controllo ed il gruppo di soggetti con mci emersa una differenza statisticamente significativa a livello dello splenio ( p < 0 , 007 )  . 
all of these factors produce ultrastructural changes in the white matter , which in turn affect the water diffusivity of protons , measurable through a series of dti indices , such as fa [ 8 , 9 ]  . over the past few years , several studies have evaluated white matter in subjects with ad and mci by using diffusion - tensor mri [ 1016 ]  . 
one common result is the finding of decreased fa in the corpus callosum , in particular in the splenium , which indicates that the most posterior portions of the corpus callosum site of the temporal , parietal and occipital connections are particularly sensitive to degenerative processes [ 11 , 15 , 17 ]  . 
early involvement of the splenium in subjects with memory impairment , ad and mci has also been demonstrated with volumetric techniques [ 1820 ] , which revealed loss of volume of the corpus callosum also in normal elderly subjects , though less marked than in subjects with ad , mci and memory disorders . in contrast to previous studies [ 1012 , 14 ] , we found fa to be decreased at the level of the genu of the corpus callosum in subjects with ad but not in those with mci . 
the failure to identify reduced fa in the genu of subjects with mci could depend on the very early stage of disease characterised by memory disorders only , with intact cognitive function . 
this might in part have influenced our results , given that the higher number of directions could increase the techniques sensitivity . i meccanismi eziopatogenetici tipici della malattia di alzheimer quali la deposizione di beta - amiloide e i depositi neurofibrillari sembrano interferire precocemente con la funzionalit del neurone , provocando una serie di modificazioni ultrastrutturali che coinvolgono gli assoni , principali componenti della sostanza bianca . 
i danni derivanti coinvolgono il trasporto assonale , la struttura dei microtubuli e dei neurofilamenti e lintegrit della guaina mielinica [ 4 ]  . tutti questi fattori portano ad una modificazione ultrastrutturale della sostanza bianca con conseguente modificazione della diffusivit dei protoni dellacqua , misurabile con la dti , attraverso una serie di indici fra cui lanisotropia frazionaria ( fa ) [ 8 , 9 ]  . nel corso degli ultimi anni sono stati pubblicati diversi lavori focalizzati sulla valutazione della sostanza bianca in soggetti con ad e in soggetti con mci mediante limpiego della rm con tensori di diffusione [ 1016 ]  . 
i diversi lavori differiscono alquanto per quanto riguarda la selezione dei soggetti da includere nello studio , la tecnica desame e almeno parzialmente per quanto riguarda i risultati ottenuti . un risultato comune rappresentato dal riscontro di una riduzione della fa a livello del corpo calloso , e pi precisamente a livello dello splenio , riflettendo cos la particolare sensibilit delle porzioni pi posteriori del corpo calloso , in cui transitano le interconnessioni temporali , parietali e occipitali , ai fenomeni degenerativi [ 11 , 15 , 17 ]  . 
anche nel nostro studio , che comprendeva soggetti in uno stadio molto precoce di malattia , abbiamo osservato una riduzione della fa a livello dello splenio del corpo calloso sia nei soggetti con ad che in quelli con mci . 
il precoce coinvolgimento dello splenio del corpo calloso nei soggetti con disturbi mnesici , ad e mci stato dimostrato anche con tecniche volumetriche [ 1820 ] che hanno evidenziato come una riduzione di volume del corpo calloso avviene anche nei soggetti normali con il progredire dellet , ma appare pi accentuata nei soggetti con ad , mci e disturbi mnesici . nel nostro studio , a differenza di altri autori [ 1012 , 14 ] , stata riscontrata una riduzione della fa anche a livello del ginocchio del corpo calloso nel soggetti con ad ma non nei soggetti con mci . 
la mancata riduzione della fa a livello del ginocchio del corpo calloso nei soggetti con mci potrebbe dipendere dallo stadio estremamente precoce della malattia in questo gruppo di soggetti affetti da disturbi esclusivamente mnesici e funzioni cognitive integre . 
per quanto riguarda la discrepanza con gli altri studi presenti in letteratura il motivo potrebbe essere ricercato nellesiguo numero di soggetti in ogni gruppo anche se non si pu non tener conto della diversa tecnica desame da noi utilizzata . infatti in letteratura , a nostra conoscenza , non ci sono lavori simili nei quali la valutazione dei tensori della fa si stata fatta con gradienti applicati lungo le 32 direzioni . 
 in accordo con i pi recenti dati riportati in letteratura 920 radiol med ( 2008 ) 113 : 915922 in agreement with recent reports , we observed a statistically significant difference in fa values in the right frontal white matter in patients with ad compared with normal subjects [ 11 , 12 , 21 ] , whereas fa on the left side was higher in patients than in controls . 
this group of ad patients showed a nonsignificant tendency to increased fa values in the white matter in the following anatomical sites : left frontal , bilateral parietal , bilateral temporal and bilateral occipital . 
these findings are difficult to interpret , and the most likely explanation might lie in the heterogeneity of the sample population . several theories have been proposed to explain the early involvement of frontal white matter in ad ; in particular , it has been suggested that it could be due to early frontaltemporal disconnection [ 22 ]  . 
again , this discrepancy could be in part due to the characteristics of the study sample ( small sample size , early disease stage ) , and in part due to the different imaging technique used . 
 in agreement with other studies , we noted a correlation between fa values and mmse scores , which demonstrates that white - matter degeneration is reflected in cognitive performance [ 12 ]  . 
this is mostly likely explained by the relatively small clinical difference between the two patient groups and the limited memory impairment in those with ad . there are some limitations to our study . 
several methods have been proposed to overcome this problem , including the use of histograms [ 24 ] and the voxel - based method [ 10 ]  . secondly , we decided to measure fa values and not individual eigenvalues . 
the reasons for this are essentially two : the first is the inevitable lengthening of examination times , a problem when imaging uncooperative subjects ; the second abbiamo trovato una differenza statisticamente significativa per quanto riguarda la sostanza bianca frontale destra nei pazienti con ad se confrontati con i soggetti normali [ 11 , 12 , 21 ] , mentre nel lato sinistro i valori fa dei pazienti sono pi elevati dei controlli . 
in questo gruppo di pazienti ad c una tendenza non significativa ad un aumento dei valori di fa nella sostanza bianca nelle seguenti sedi anatomiche : frontale sinistra , parietale bilaterale , temporale bilaterale , occipitale bilaterale . 
 sono state proposte diverse teorie per spiegare il precoce coinvolgimento della sostanza bianca a livello frontale in questi soggetti ed in particolare questo potrebbe essere dovuto alla precoce disconnessione fronto - temporale [ 22 ]  . 
per quanto riguarda le rimanenti sedi da noi valutate non abbiamo riscontrato differenze statisticamente significative a differenza di alcuni autori [ 12 , 15 , 23 ]  . in particolare non abbiamo trovato differenze tra i gruppi per quanto riguarda la fa a livello del lobo temporale . 
 in accordo con alcuni studi in letteratura stata riscontrata una correlazione tra fa e i risultati del mmse , fatto che dimostra come la degenerazione della sostanza bianca si rifletta sulle performance cognitive [ 12 ]  . 
il principale motivo verosimilmente legato alla relativamente poca differenza anche dal punto di vista clinico tra i due gruppi di pazienti ed in particolare al relativamente limitato coinvolgimento delle funzioni mnesiche nei soggetti con ad . il presente studio presenta sicuramente dei limiti . 
per ovviare a questo problema sono stati proposti diversi metodi tra cui il metodo che prevede lutilizzo di istogrammi [ 24 ] o il metodo voxel based [ 10 ]  . 
i motivi del mancato impiego del gating cardiaco sono stati essenzialmente due : il primo riguarda linevitabile allungamento dellesame in soggetti con collaborazione coradiol med ( 2008 ) 113 : 915922 is that we thought the size and number of voxels in each roi were sufficiently large for us to consider that the results would not be significantly influenced by cerebrospinal fluid pulsation artefacts . munque limitata mentre per quanto riguarda il secondo abbiamo ritenuto che le dimensioni dei voxel il numero dei voxel per singola roi fossero sufficientemente grandi da poter considerare gli artefatti da pulsazione liquorale poco influenti ai fini della significativit del risultato . conclusions conclusioni despite its limitations , our study confirmed early involvement of the splenium of the corpus callosum both in subjects with ad and in those with mci , a finding in agreement with previous studies that differ from ours in terms of patient characteristics and imaging technique used . 
further , larger studies with homogeneous samples and imaging techniques are required to confirm this role and maximise the effectiveness of the technique . pur con i limiti sopradescritti , il presente lavoro ha confermato , in accordo con i dati della letteratura che peraltro differiscono in parte per la caratteristiche del campione e in parte per la tecnica utilizzata , il precoce coinvolgimento dello splenio del corpo calloso sia nei soggetti con ad che nei soggetti con mci . 
grassi2 1associated professor of radiology , section of radiology , department magrassi - lanzara , second university of naples , via amendola 8 , 81055 santa maria capua vetere , caserta , italy 2section of radiology , 3section of gastrointestinal sougery , department magrassi - lanzara , second university of naples , caserta , italy correspondence to : s . 
for the combined study , we used a dyno compact computerised system ( menfis biomedical s.r.l. , bologna , italy ) equipped with : ( 1 ) graphics card for the management of ultrasonographic or radiological images ; ( 2 ) a.vi.u.s. 
dedicated software package , which enables digital - quality recording ( pal / ntsc , composite video or s - video ) of the videofluoroscopy study in avi format with 320240 resolution and 25 hz acquisition frequency . 
the delay introduced by the process of image digitalisation is in the order of 200 ms , so for analysis purposes , the images can be considered synchronised with the manometric recordings . 
data were collected on a specifically designed grid for the evaluation of 46 videofluoroscopic items , of which 34 are derived from the laterolateral view ( seven in the oral preparatory phase , 15 in the oral transport phase and 12 in the pharyngeal phase ) and 12 in the anteroposterior view ( six in the oral preparatory phase and six in the oropharyngeal phase )  . 
software dedicato , attraverso il quale possibile registrare in qualit digitale ( pal / ntsc , video composito o s - video ) la videofluoroscopia , in filmati avi con risoluzione 320240 e con frequenza di acquisizione di 25 hz ; il ritardo introdotto dal processo di digitalizzazione dellimmagine dellordine dei 200 ms , quindi , ai fini dellanalisi , limmagine si pu considerare sincronizzata con i tracciati pressori . 
i dati vengono raccolti su una griglia precostituita per la valutazione di 46 items videofluoroscopici , di cui 34 derivano dallo studio in proiezione latero - laterale ( 7 in fase buccale , 15 in fase orale e 12 in fase faringea ) e 12 dallo studio in proiezione antero - posteriore ( 6 in fase buccale e 6 in fase orofaringea ) ; la positivit ai singoli parametri espressa in maniera binaria . 
an early and effective diagnosis of oropharyngeal dysphagia means being able to effectively implement appropriate rehabilitation techniques , improve the patients quality of life , and minimise the complications associated with swallowing disorders ( choking , aspiration pneumonia , malnourishment )  . distinction of the anatomical level of dysphagia is not a matter of simple classification ; rather , it is essential in that different clinical presentations require different diagnostic strategies , and a precise definition of the anatomicalfunctional substrate is required to implement the correct therapeutic approach . 
this study presents the authors experience with the use of combined videofluoroscopy and manometry with particular emphasis on the examination technique . keywords phazynx videofluoromanometry dysphagia items manometrici , a loro volta divisi in 4 criteri maggiori e 7 minori risultati . 
la valutazione fluoroscopica dinamica della deglutizione con registrazione video abbinata alla manometria simultanea , ha permesso di registrare contemporaneamente le alterazioni anatomiche correlandole al dato funzionale della pressione orofaringea , consentendo durante la medesima registrazione di valutare la situazione anatomica , biomeccanica e fisiologica della deglutizione e le modalit di propulsione e transito del bolo . 
fare precocemente una buona diagnosi di disfagia orofaringea significa poter intervenire efficacemente con tecniche riabilitative logopediche , migliorare la qualit di vita del paziente , nonch ridurre al minimo le complicanze che questa comporta ( soffocamento , polmonite ab ingestis , malnutrizione )  . 
la differenziazione del livello anatomico della disfagia non riveste una semplice categorizzazione , ma indispensabile in quanto alla diversit di presentazione clinica corrisponde un differente approccio metodologico diagnostico , ed a una precisa definizione del substrato anatomo - funzionale responsabile del sintomo , corrisponde un diverso approccio terapeutico . 
gli autori con il presente contributo presentano la loro esperienza nellimpiego della videofluoromanometria ed in particolare la metodologia di conduzione dellesame . parole chiave faringe videofluoromanometria disfagia introduction introduzione swallowing is a complex physiological mechanism during which the food bolus passes from the mouth to the digestive tract via the pharynx [ 15 ]  . 
swallowing is generally divided into three phases : the oral phase is voluntary , whereas the pharyngeal and oesophageal phases are involuntary [ 2 ]  . dysphagia is a symptom of different pathological conditions characterised by alteration of the swallowing mechanism , which can occur at different levels . 
differentiation of the level at which dysphagia occurs is not simply a matter of classification ; rather , it is essential in that the different clinical presentations require different diagnostic approaches . 
clinically , patients affected by oropharyngeal dysphagia present symptoms characterised by difficulty in the initial phase of swallowing , such as cough , sense of choking associated with aspiration of food into the airways , nasal regurgitation and sialorla deglutizione un meccanismo fisiologico complesso durante il quale il bolo alimentare transita dalla bocca al canale digestivo attraverso la via aero - digestiva superiore ed in particolare attraverso il faringe [ 15 ]  . 
la deglutizione viene generalmente distinta in tre fasi , delle quali la fase orale sottoposta al controllo volontario , mentre le fasi faringea ed esofagea sono involontarie [ 2 ]  . la disfagia un sintomo sotteso da differenti quadri patologici , in cui si verifica unalterazione del meccanismo deglutitorio , che pu estrinsecarsi a vari livelli . 
i quadri disfagici vengono catalogati in relazione al livello in cui si verifica lalterazione funzionale , cos da distinguere disfagie orofaringee e disfagie faringo - esofagee ( tabella 1 ) [ 6 ]  . 
la differenziazione del livello anatomico della disfagia non riveste una semplice categorizzazione , ma indispensabile in quanto alla diversit di presentazione clinica corrisponde un differente approccio metodologico diagnostico , ed a una precisa definizione del substrato anatomo - funzionale responsabile del sintomo , corrisponde un diverso approccio terapeutico . 
in contrast , when the anatomical - functional problem is located more distally pharyngeal - oesophageal dysphagia the patient experiences difficulty in the late swallowing phase with the sensation of food sticking in the lower part of the pharynx or chest , retrosternal pain , odynophagia and pyrosis . the correct diagnosis of dysphagia and its aetiopathogenetic features requires a multidisciplinary approach involving the radiologist , gastroenterologist , speech therapist and , in particularly complex cases , the neurologist , ear , nose and throat specialist , geriatrician or paediatrician . 
in addition to a thorough patient history , the diagnostic workup requires an accurate physical examination involving evaluation of the motor and sensory functions of the mouth and oral cavity and deep reflexes of the cranial nerves ; inspection and two - handed palpation of the mouth floor , tongue and neck region ; and assessment of the movements of the thyroid cartilage during swallowing [ 7 , 8 ]  . various instruments providing both a morphological and functional study are used for diagnosing dysphagia . 
combined studies enabling simultaneous morphological and functional assessment , such as videofluoroscopy combined with manometry , have taken on an increasingly front - line role in the diagnosis of dysphagia , particularly in patients with underlying neurological disorders . 
the mean examination time , including catheter placement , image acquisition and compensatory manoeuvres , was 25 mall patients , even those with neurological disease , were able to breathe , speak and swallow autonomously , and none suffered from neurological deficit to the point of undermining compliance . the diagnostic team included a radiologist with experience in videofluoroscopy , a gastrointestinal surgeon with a good understanding of manometry and its application to the sentano allosservazione clinica con sintomi caratterizzati da difficolt nella fase iniziale della deglutizione , tosse , senso di soffocamento legato alla aspirazione di materiale alimentare nelle vie aeree , rigurgito nasale e scialorrea . quando invece il problema anatomo - funzionale si localizza in sedi pi distali , disfagia faringo - esofagea , il paziente avverte difficolt nella fase terminale della deglutizione con sensazione di cibo arrestato nella parte bassa del faringe o nel torace , dolore retrosternale , odinofagia , pirosi . il corretto inquadramento diagnostico della disfagia e dei rispettivi aspetti eziopatogenetici necessita di un approccio multidisciplinare in cui indispensabile una stretta sinergia tra radiologo , gastroenterologo , logopedista , e , in casi particolarmente complessi , neurologo , otorinolaringoiatra , geriatra o pediatra . 
liter clinico - diagnostico richiede unattenta anamnesi del paziente , un corretto esame obiettivo che comprenda anche la valutazione delle funzioni motorie e sensitive della bocca e del cavo orale , dei riflessi profondi dei nervi cranici , osservazione e palpazione bimanuale del pavimento della bocca , della lingua , della regione del collo e dei movimenti dello scudo cartilagineo tiroideo durante gli atti deglutitori [ 7 , 8 ]  . la diagnostica strumentale della disfagia si avvale di differenti tecniche di studio sia di tipo morfologico che funzionale tra cui si annoverano la videofluoroscopia , la videoendoscopia , lultrasonografia , la manometria e lelettromiografia . 
di recente le indagini combinate , che consentano nel medesimo tempo valutazioni di tipo morfologico e funzionale , quali la videofluoromanometria ( vfm ) assumono sempre pi un ruolo di primo piano nellinquadramento del paziente disfagico e in particolar modo di quelli per cause neurologiche . 
i pazienti , 57 maschi e 52 femmine , presentavano et compresa tra i 18 e i 76 anni . in realt il numero di pazienti era superiore di due unit nelle quali non stato possibile eseguire lesame videofluoromanometrico per impossibilit al posizionamento del sondino dovuta alla scarsa collaborazione dei pazienti . 
il tempo meradiol med ( 2008 ) 113 : 923940 table 1 causes of dysphagia oropharyngeal dysphagia neuromuscular diseases diseases of the central nervous system : cerebrovascular accident parkinsons disease brain - stem tumours degenerative diseases amyotrophic lateral sclerosis multiple sclerosis huntingtons disease postinfectious poliomyelitis syphilis peripheral nervous system peripheral neuropathy motor end - plate dysfunction myasthenia gravis skeletal muscle disease ( myopathies ) polymyositis dermatomyositis muscular dystrophy ( myotonic dystrophy , oculopharyngeal dystrophy ) cricopharyngeal ( upper oesophageal sphincter ) , achalasia obstructive lesions tumours inflammatory masses trauma / surgical resection zenker 's diverticulum oesophageal webs extrinsic structural lesions anterior mediastinal masses cervical spondylosis esophageal dysphagia neuromuscular disorders achalasia spastic motor disorders : diffuse oesophageal spasm hypertensive lower oesophageal sphincter nutcracker oesophagus scleroderma obstructive lesions intrinsic structural lesions tumours strictures peptic radiation - induced chemical - induced medication - induced lower oesophageal rings ( schatzkis ring ) oesophageal webs foreign bodies extrinsic structural lesions vascular compression enlarged aorta or left atrium aberrant vessels mediastinal masses lymphadenopathy substernal thyroid study of the pharynx and a speech therapist . 
training required to gain sufficient familiarity with the instrumentation was estimated at about eight to ten procedures under the guidance of sufficiently expert personnel . the role of the speech therapist in the diagnostic workup of dysphagia is divided into three phases : 1 . 
before the combined videofluoroscopy and manometry study , the speech therapist informs the radiologist of the factors triggering the disorder in the patient , with particular regard to the type of bolus ( solid , liquid or both ) and its dio di presenza del paziente in diagnostica , comprensivo del posizionamento del sondino - esecuzione esame - manovre di compenso , stato calcolato pari a circa 25 mtutti i pazienti reclutati , ancorch portatori di patologie neurologiche erano autonomi dal punto di vista respiratorio , fonatorio e deglutitorio e nessuno di essi aveva turbe della coscienza tali da pregiudicare la compliance del paziente . 
 il gruppo di studio prevede un radiologo con esperienza nella valutazione videofluoroscopica della deglutizione , uno specialista in chirurgia dellapparato digerente con buona conoscenza della tecnica manometrica e della sua applicazione allo studio del faringe e un logopedista . 
il training per acquisire la corretta manualit , anche ai fini di garantire una non precoce usura dello strumentario , pu essere stimabile in circa 810 procedure sotto la guida di personale gi sufficientemente esperto . il reale ruolo che il logopedista svolge nel iter diagnostico della disfagia si articola in tre fasi : 1 . 
accoglie il paziente che giunge alla nostra osservazione radiol med ( 2008 ) 113 : 923940 tabella 1 cause di disfagia disfagia orofaringea incidente cerebrovascolare malattia neuromuscolare malattie del sistema nervosa centrale morbo di parkinson tumori cerebrali malattie degenerative sclerosi laterale amiotrofica sclerosi multipla malattia di huntington post - infezioni poliomielite sifilide sistema nervosa periferico neuropatia periferica disfunzione delle placche motorie miastenia grave malattia del muscolo scheletrico ( miopatie ) polimiosite dermatomiosite distrofia muscolare ( distrofia miotonica , distrofia oculofaringea ) acalasia cricofaringea ( sfintere dellesofago superiore ) lesioni ostruttive tumori masse infiammatorie traumi / resezioni chirurgiche diverticolo di zenker reti esofagee lesioni estrinseche strutturali masse mediastiniche anteriori spondilosi cervicale disfagia esofagea disordini neuromuscolari acalasia disordini spastici motori spasmo esofageo diffuso sfintere esofageo inferiore iperteso esofago a schiaccianoci scleroderma lesioni ostruttive lesioni intrinseche strutturali tumori restringimenti peptica anelli dellesofago inferiore ( anelli di schatzki ) reti esofagee corpi estranei indotta da radiazioni indotta da sostanze chimiche indotta da interventi medici lesioni estrinseche strutturali compressione vascolare espansione dellaorta o dellatrio sinistro vasi aberranti masse madiastiniche linfoadenopatie tiroide sottosternale size , as well as the presence or absence of the cough reflex and voluntary coughing . 
the radiological study is therefore tailored to the different types of dysphagia , with the main aim being to immediately qualify and quantify the swallowing disorder and minimise examination times and radiation exposure 2 . 
in the next diagnostic phase of the videofluoroscopy and manometry swallow study , the operators , after having induced and studied the swallowing disorder , search for elements capable of guiding dietary interventions and speech therapy rehabilitation . 
at the end of the radiological study , the speech therapist gives the patient instructions regarding type and consistency of foods the patient may safely eat and , where necessary , indications regarding posture and compensatory mechanisms . 
prima di effettuare lesame vfm il logopedista informa il radiologo riguardo le circostanze che scatenano il disturbo nel soggetto , in particolare per quale tipologia di bolo ( solido , liquido o entrambi ) e per quali dimensioni , e sulla presenza / assenza del riflesso tussigeno e del colpo di tosse volontario . 
speech therapy follow - up is recommended to monitor the effect of the rehabilitation . data acquisition the combined swallow study involves videofluoroscopy and the simultaneous recording of the manometric trace . 
for the combined study , we used a dyno compact computerised system ( menfis biomedical s.r.l. , bologna , italy ) equipped with : ( 1 ) graphics card for the management of ultrasonographic or radiological images ; ( 2 ) a.vi.u.s. 
dedicated software , which enables the digital - quality recording ( pal / ntsc , composite video or s - video ) of videofluoroscopic images in avi format with 320240 resolution and 25 hz acquisition frequency . 
the delay introduced by the process of image digitalisation is in the order of 200 ms , so for analysis purposes , the images can be considered synchronised with the manometric recordings . 
once the data have been acquired , data analysis is performed either in real time poi un secondo momento , di indirizzo diagnostico , in cui gli operatori , dopo aver indotto e studiato il disturbo disfagico , procedono alla ricerca degli elementi necessari ad indirizzare il successivo intervento dietetico e riabilitativo logopedico . 
infine viene consigliato un follow - up logopedico per il monitoraggio degli effetti della terapia riabilitativa . acquisizione dei dati la videofluoromanometria prevede lesecuzione contemporanea della videofluoroscopia con la simultanea registrazione di un tracciato manometrico . 
our study was conducted with the use of prevalently liquid barium contrast material ( a single package of prontobario hd , bracco s.p.a. , milan , diluted in 65 cc of water )  . 
the technique involved the administration of a bolus of contrast material in a quantity optimised for the patients performance status , between 5 and 10 cc , with the aim of simulating normal swallowing as closely as possible . 
all phases of the process were videorecorded first in the anteroposterior and then in the laterolateral view . concurrent pressure measurements were performed with a manometry catheter with endoluminal four - channel solidstate microtransducers 5 cm apart and with an angle of 12090 . 
in the cervical oesophagus , 4 cm below the inferior margin of the upper oesophageal sphincter ( uos ) , or at the level of the passavants ridge to evaluate the correct closure of the rhinopharynx during swallowing and phonation 2 . 
in the uos , with an evaluation of the correct placement with the appearance of the characteristic m - wave ( fig . 2 ) , confirmed also at videofluoroscopy 3 . 
software dedicato , attraverso il quale possibile registrare in qualit digitale ( pal / ntsc , video composito o svideo ) la videofluoroscopia , in filmati avi con risoluzione 320240 e con frequenza di acquisizione di 25 hz ; il ritardo introdotto dal processo di digitalizzazione dellimmagine dellordine dei 200 ms , quindi , ai fini dellanalisi , limmagine si pu considerare sincronizzata con i tracciati pressori . 
in corso di analisi il video viene visualizzato sullo schermo pc in tempo reale durante lacquisizione dellesame ; i tracciati manometrici possono essere visualizzati sovrapposti ad esso , in modo da sfruttare la massima risoluzione , oppure affiancati al video , con minima perdita di risoluzione . 
nella fase di acquisizione dei dati i filmati sono riprodotti a fianco dei tracciati ed un cursore che scorre su di essi mostra lesatta corrispondenza tra il filmato ed i tracciati . 
per lindagine videofluoroscopica stato utilizzato mezzo di contrasto baritato prevalentemente allo stato liquido ( una confezione di prontobario hd , bracco s.p.a. , milano , diluita in 65 cc di acqua ) , con paziente in ortostatismo , salvo i casi in cui la compromissione della funzione statica dei pazienti ha reso necessaria lacquisizione dellesame in posizione seduta . 
la tecnica prevede la somministrazione di boli di mdc in quantit ottimizzate in relazione al performance status del paziente , comprese tra 5 e 10 cc , con lo scopo di rendere lindagine il pi simile possibile alla deglutizione normale . 
tutte le fasi del processo vengono documentate con la videoregistrazione dapprima in proiezione antero - posteriore e poi in latero - laterale . la contemporanea valutazione pressoria viene effettuata mediante il posizionamento di un sondino manometrico con microtrasduttori endoluminali allo stato solido con 4 canali , distanziati 5 c luno dallaltro e con un angolo di 12090 . 
nellesofago cervicale , 4 cm al di sotto del margine inferiore dello sfintere esofageo superiore , o a livello del cuscinetto del passavant per la valutazione della corretta chiusura del rinofaringe durante la deglutizione e la fonazione . 930 radiol med ( 2008 ) 113 : 923940 fig . 
limmagine videofluroscopica ( a ) ha una buona qualit ; il tracciato monometrico ( b ) presenta un marker ( barra verticale ) che correla la rilevazione per immagini con il tracciato manometrico . positive findings for the individual parameters are expressed in a binary fashion . 
a positive finding in one of the major criteria defines the patient as dysphagic , whereas in the absence of major criteria , at least six minor criteria are required for the diagnosis of dysphagia ( tables 24 )  . evaluation of the manometric recordings was based on 11 items , which were divided into four major and seven minor criteria ( tables 5 , 6 )  . 
this type of check list arises from the need for an interdisciplinary approach between the referring specialist and the various operators so as to find a shared and consistent language for diagnosis and follow - up . the distinction between major and minor criteria was extrapolated from a retrospective review of our teams experience , which took into account the different capabilities of the speech - therapy evaluation , the clinical - neurological evaluation and the videofluoroscopy - manometry findings in determining dysphagia severity . 
videofluoroscopy confirmed the presence of aspiration in only 57 / 109 ( 52.3% ) patients , and in the remaining cases , it accurately identified swallowing alterations ( without aspiration ) that were compatible with the clinical indications . 
in 6 / 109 cases , the alteration was in the oral preparatory phase , in 8 / 109 cases in the oral transport phase , in 5 / 109 cases in the pharyngeal phase and in 6 / 109 cases in all swallowing phases . 
questo tipo di refertazione a check list nasce da un esigenza di interdisciplinariet fra lo specialista richiedente e i diversi operatori al fine di riuscire a trovare un linguaggio comune e coerente per lindirizzo diagnostico e il successivo follow - up del paziente . 
la differenziazione in criteri maggiori e minori stata estrapolata da una valutazione retrospettiva interna al nostro gruppo che ha tenuto in considerazione le diverse capacit di identificazione della gravit del soggetto disfagico che esistono fra valutazione logopedica , valutazione clinica - neurologica e rilievi videofluoroscopici - manometrici . 
dallosservazione videofluoroscopica inoltre stato valutato se latto deglutitorio avveniva in posizione indifferente , ovvero se il paziente per completare latto della deglutizione senza complicanze soggettivamente rilevabili , era costretto ad assumere particolari posture del capo o del collo . risultati i risultati delle tre valutazioni ( logopedica , radiologica e monometrica ) singolarmente esaminati hanno fatto porre la diagnosi di disfagia in una percentuale pressoch uguale ( 75% ) ma con alcune differenze per sottocategorie di disturbi deglutitori e di pazienti . 
la valutazione logopedica radiol med ( 2008 ) 113 : 923940 table 6 minor manometric indicators pressure of passavants ridge in mmhg motor coordination intrabolus pressure peristalsis pharyngo - oesophageal reflux tracheo - oesophageal fistula zenkers diverticulum hypertonic ues in mmhg hypotonic ues in mmhg mean value of ues in mmhg maximum peak of ues in mmhg length of ues in cm duration of relaxation ues , upper esophageal sphincter tabella 6 indicatori manometrici minori pressione del cuscino del passavant in mmhg coordinamento motorio pressione intrabolo peristalsi reflusso esofago faringeo fistola tracheo esofagea diverticolo di zenker ipertono del s.e.s. 
pressure changes associated with each swallowing act were simultaneously recorded as negative or positive waves , and the relationship between the forces created by the opposition of the tongue , pharynx , larynx , oesophagus and bolus was studied . 
accurate synchronisation of manometry and videofluoroscopy recordings proved particularly useful for identifying subgroups of swallowing disorders and enabled distinction between a weak opening of the uos in 20 / 109 casha evidenziato pazienti con disfagia con aspirazione in 64 / 109 ( 58 , 7% ) mentre nei restanti casi erano presenti alterazioni delle fasi della deglutizione senza sospetto di aspirazione . 
la valutazione radiologica ha confermato la presenza di aspirazione solo in 57 / 109 ( 52 , 3% ) e nella restante percentuale ha identificato in maniera precisa le alterazioni nelle differenti fasi della deglutizione ( senza aspirazione ) compatibili con le indicazioni cliniche e in particolare in 6 / 109 vi era alterazione della fase buccale , in 8 / 109 della fase orale e in 5 / 109 della fase faringea e in 6 / 109 la contemporanea alterazioni di tutte le fasi della deglutizione . nei restanti 27 / 109 ( 24 , 8% ) lesame non presentava alterazioni della dinamica deglutitoria e in particolare nella nostra esperienza non stato identificato nessuna ipertrofia del muscolo cricofaringeo . 
infine la valutazione manometrica ha identificato come patologici una percentuale superiori di soggetti esaminati ( 84 / 109 , 77% ) con un collocazione meno precisa delle alterazioni nelle diverse fasi della deglutizione . 
con tale tecnica i cambiamenti dei regimi pressori associati ad ogni atto deglutitorio sono stati documentati simultaneamente come onde negative o positive ed inoltre stato possibile studiare la relazione tra le forze create dallopposizione della lingua , del faringe , della laringe , dellesofago e del bolo . 
allo stato vengono impiegate per lo studio delle disfagie , differenti tecniche e metodiche , pi o meno invasive , quali la videofluoroscopia , la videofaringolaradiol med ( 2008 ) 113 : 923940 fig . 
5 integrazione tra valutazione qualitativa e quantitativa : caduta pre deglutitoria ( freccia tratteggiata ) e penetrazione ( freccia bianca ) allimmagine videofluoroscopica che corrisponde con un picco di pressione ectopico allesame monometrico . sult ; ( 2 ) reveal the aetiopathological mechanism that could not be identified with the individual techniques ; and ( 3 ) classify as compensatory a number of mechanisms that the individual techniques identified as pathological . discussion the aims of instrumental diagnostics in general and diagnostic imaging in particular are to accurately define the possible anatomical alterations underlying dysphagia and identify the functional substrates involved in the condition [ 912 ]  . 
one particularly promising technique is combined videofluoroscopy and manometry , which brings together the advantages of the dynamic visualisation of swallowing and the functional data provided by the simultaneous recording of pressure variations at different points in the pharynx and oesophagus [ 13 ]  . videofluoroscopy swallow study , also known as modified barium swallow study ( mbss ) , is a radiographic test that differs from the conventional barium swallow study . videofluoroscopy is the gold standard for defining the site of dysphagia in that it is noninvasive and allows real - time assessment of all phases of the swallowing process and identification of the site of the anatomical and / or functional alteration impairing the normal progression of the food bolus . 
the examination is traditionally performed by giving the patient radiopaque boluses of different consistencies and amounts , which are chosen on a case - by - case basis according to the clinical findings and the subjective symptoms . videofluoroscopy is performed with the patient in different positions and the acquisition of different views so as to obtain optimal visualisation of the oral , pharyngeal and larynringoscopia e la manometria faringoesofagea , ciascuna delle quali in grado di rappresentare differenti parametri o di tipo morfologico o funzionale . 
tecnica estremamente interessante nellambito di tali tipi di patologie , la videofluoromanometria ( vfm ) , che unisce al vantaggio della visualizzazione dinamica per immagini del processo della deglutizione , la possibilit di correlare il dato morfologico al dato funzionale , mediante il rilievo simultaneo delle variazioni pressorie a livello di pi punti del complesso faringo - esofageo [ 13 ]  . lesame videofluoroscopico dinamico della deglutizione definito anche deglutizione al bario modificata una videofluoroscopia ( vfs ) , test radiografico che differisce dalla procedura tradizionale di valutazione della deglutizione al bario . 
una tecnica radiologica che rappresenta il gold standard per la definizione della sede della disfagia , in quanto non invasiva e consente in tempo reale lo studio delle differenti fasi della deglutizione a partire gi dalla fase buccale identificando la sede dellalterazione organica e / o funzionale della normale progressione del bolo ingestuale . 
tradizionalmente lesame si effettua mediante la somministrazione di un bolo radiopaco la cui differente consistenza e le dimensioni , vengono di volta in volta scelte in relazione al quesito clinico ed alla sintomatologia soggettiva . 
la valutazione videofluoroscopica viene effettuata mediante studio in posizioni e con proiezioni differenti al fine di ottenere unottimale visualizzazione delle strutture orali , faringee e laringee e del loro assetto funzionale durante la deglutizione , nonch dei meccanismi di compenso messi in atto dal paziente al fine di migliorare la qualit della deglutizione e di ovviare ad inconvenienti soggettivi che si manifestano durante le differenti fasi di essa [ 14 ]  . un corretto studio videofluoroscopico per la valutazione di alterazioni della deglutizione deve essere finalizzato a : 1 . 
 936 radiol med ( 2008 ) 113 : 923940 geal structures during swallowing as well as the compensatory mechanisms carried out by the patient to improve the quality of swallowing and avoid possible discomfort during the different swallowing phases [ 14 ]  . 
examining the short - term effects of therapeutic strategies aimed at eliminating or compensating for the dysfunction . although other instrumental procedures , such as videoendoscopy , ultrasonography , manometry , electromyography or some combination of these , are able to focus on specific components of the swallowing mechanism , none of them can be considered on a par with videofluoroscopy . 
recent studies have emphasised the role of videofluoroscopy , underlining its ability to identify the causes of the swallowing disorder and define the best therapeutic strategies [ 15 ]  . pharyngo - oesophageal manometry is the gold standard for identifying functional oesophageal alterations , but its role in the study of the pharynx is still somewhat limited by technical problems ( opening mechanism of the uos , rapidity of events , breathing , movement of the catheter ) [ 1618 ]  . combined videofluoroscopy and manometry can , to a large extent , overcome these difficulties , in part because visualisation of the anatomical structures allows the manometry catheter to be correctly positioned throughout the various study phases . 
this system , however , is now considered inadequate for the quantitative measurement of pharyngeal contraction due to the low - frequency response of the perfusion syste in 1988 , mcconnel et al . 
 [ 22 ] , who concluded that with the use of solid - state transducers , the manometric study is complementary to videofluoroscopy , as the latter visualises the transit of the bolus and the former records the pressure exerted by the pharyngeal wall . 
when used in combination , videofluoroscopy and manometry are able to evaluate the causes and effects of pharyngeal dysfunction that cannot be examined by each of the techniques individually [ 23 ]  . an example is provided by the differentiation in uos opening , which at videofluoroscopy is defined as the correct passage of contrast material , and uos relaxation , which can only be evaluated manometrically . 
 sebbene altre metodiche investigative , come la videoendoscopia , lultrasonografia , la manometria , lelettromiografia , o loro combinazioni possano successivamente permettere di focalizzare lo studio su elementi particolari del meccanismo deglutitorio , nessuna di queste pu considerarsi sostitutiva della vfs . 
recenti lavori hanno enfatizzato il ruolo di tale metodica diagnostica , in quanto la valutazione vfs consente di individuare le cause e permette di definire le pi idonee strategie terapeutiche [ 15 ]  . 
 la manometria faringoesofagea il gold standard per le alterazioni funzionali esofagee , mentre il suo ruolo nello studio del faringe ha ancora alcune limitazioni legate a problemi tecnici ( meccanismo di apertura del ses , rapidit degli eventi , respirazione , movimento del catetere ) [ 1618 ]  . la tecnica combinata della videofluoromanometria permette in buona misura di eludere alcune di queste problematiche , legando inscindibilmente tra di loro le due valutazioni diagnostiche e consentendo di valutare anche il corretto posizionamento della sonda monometriche durante le differenti fasi di studio . 
questa tecnica stata descritta per la prima volta nel 1966 da sokol et al . , che impiegavano un manometro con cateteri a per fusione [ 19 ] : tale sistema considerato attualmente inadeguato per la misurazione quantitativa della contrazione faringea a causa della risposta a bassa frequenza del sistema a perfusione e nel 1988 , mcconnel et al . 
hanno dimostrato che questi problemi possono essere superati con luso di trasduttori a stato solido con risposta ad alta frequenza [ 20 ] , dati confermati anche successivamente da castell et al . 
 [ 21 ] e da olsson et al . [ 22 ] i quali concludono che con lutilizzo di trasduttori a stato solido , lo studio manometrico risulta complementare a quello videofluoroscopico poich questo ultimo riflette il transito del bolo , mentre la manometria rivela le pressioni esercitate dalla parete faringea . 
quando sono effettuate contemporaneamente , le due metodiche ( videofluoroscopia e manometria ) permettono la valutazione delle cause e degli effetti della disfunzione faringea che non sono esaminabili con le singole indagini [ 23 ]  . 
un esempio su tutti dato dalla differenziazione tra apertura dello ses , definita dallesame radiologico anche come corretto passaggio del mdc , e rilassamento dello stesso che possibile valutare solo manometricamente . 
nel nostro studio e in letteratura riportata , infatti , la presenza di un rilassamento dello sfintere , da normale ad assente , in caso di apertura dello stesso , come a dire quindi che apertura e rilassamento non sono sinonimi e che lapertura dello sfintere , che permette il passaggio del mdc , in alcuni casi legato allaumento della pressione intrabolo e non al rilassamento della muscolatura sfinteriale radiol med ( 2008 ) 113 : 923940 from normal to absent , in the event of opening of the sphincter itself . 
this suggests that opening and relaxation are not synonymous and that opening of the sphincter , which allows passage of contrast material , is in some cases linked to increased intrabolus pressure and not to relaxation of the uos musculature [ 24 ]  . 
in addition , it has been reported that hypertrophy of the cricopharyngeal muscle , which is clearly seen at videofluoroscopy , is not directly correlated with uos achalasia [ 25 ]  . 
indeed , of all cases with videofluoroscopic and manometric evidence of failed uos opening , only one showed cricopharyngeal hypertrophy at videofluoroscopy alone [ 26 ]  . in addition , the aetiology of oropharyngeal dysphagia is not always correctly detected , even after clinical , laboratory or radiological assessment , magnetic resonance imaging included [ 27 ]  . 
our brief experience and published studies demonstrate that the use of this type of technique enabled a diagnosis of neurological damage in patients with dysphagia with an unknown cause and at the same time suggest conservative or surgical treatment ( dilatation of the cricopharyngeal muscle , myotomy , botulin injection ) for patients with definite neurological dysphagia . 
all of this , however , is of little worth if this type of approach fails to affect the outcomes of dysphagic patients , as reported by cook and kahrilas [ 28 ] and as suggested by our preliminary experience , to be validated by the follow - up of our patients . integration of the two instrumental studies functional and morphological enabled , in agreement with the previously acquired clinical data , accurate definition of anatomical and / or functional changes produced by different underlying conditions , thus suggesting the most appropriate therapy for each patient . 
these include the initial purchase of the instrumentation ( up to 20 , 000 euro ) ; the learning curve required with this new technique , which is , however , inversely proportional to the experience of the individual operator ; and patient discomfort associated with the procedure , which may be considered minimal given the small diameter of the manometry catheter . conclusions an early and accurate diagnosis of oropharyngeal dysphagia means being able to effectively intervene with speech therapy techniques , improve the patients quality of life and minimise complications ( choking , aspiration pneumonia , malnourishment )  . the impact of dysphagia in clinical practice can be gleaned from epidemiological data . 
inoltre stato riportato che lipertrofia del muscolo cricofaringeo , evidente allesame radiologico non direttamente correlato con lacalasia dello sfintere [ 25 ] ; infatti di tutti i casi in cui lesame videofluoromanometrico aveva evidenziato una mancata apertura dello ses soltanto in uno di questi era evidente lipertrofia del muscolo cricofaringeo alla sola valutazione radiologica [ 26 ]  . a tutto questo va aggiunto che spesso leziologia della disfagia oro - faringea non sempre svelata correttamente anche dopo le valutazioni cliniche , laboratoristiche e radiologiche inclusa la risonanza magnetica [ 27 ]  . 
riteniamo che alla luce della nostra seppur breve esperienza e di quella della letteratura possibile asserire che lutilizzo di questo tipo di metodica ci ha permesso di indirizzare verso un danno di tipo neurologico soggetti affetti da una disfagia senza causa e allo stesso tempo di indirizzare verso un trattamento conservativo o chirurgico ( dilatazione del muscolo cricofaringeo , miotonia , iniezione di botulino ) i pazienti affetti da disfagia di sicura natura neurologica . 
ma tutto questo non ha ragione di essere se questo tipo di approccio non riesce ad incidere sulloutcomes del paziente disfagico come riportato dagli autori cook e kahrilas [ 28 ] e come sembra emergere in maniera confortante dalla nostra esperienza preliminare che sar sicuramente validata in maniera pi evidente con i dati del follow - up dei pazienti . 
 lintegrazione dunque delle due differenti tipologie di rilievo , funzionale e morfologico , ci ha permesso di definire accuratamente , in accordo con il dato clinico , preventivamente acquisito , alterazioni anatomiche e / o funzionali implicate nelle differenti patologie a manifestazione disfagica , consentendo di definire in maniera adeguata la idonea strategia terapeutica per ogni paziente . 
ma sicuramente ci sono da affrontare una serie di svantaggi insiti alla metodica , soprattutto se confrontati con la valutazione vfs , legati ad un costo iniziale per lacquisto dellapparecchiatura ( < 20000 euro ) alla curva di apprendimento della nuova metodica che per inversamente proporzionale allesperienza dei singoli operatori e non ultimo al discomfort del paziente che minimo se si considera il ridotto diametro del sondino monometrico . conclusioni fare precocemente una buona diagnosi di disfagia orofaringea significa poter intervenire efficacemente con tecniche riabilitative logopediche , migliorare la qualit di vita del paziente , nonch ridurre al minimo le complicanze che questa comporta ( soffocamento , polmonite ab ingestis , malnutrizione )  . per dare unidea dellimpatto che la disfagia ha nella pratica clinica , bisogna fare ricorso a dati epidemiologici . stato messo in evidenza che nella popolazione adulta e involutiva prevalgono disturbi della deglutizione per compromissione delle fasi faringea , esofagea e gastrica , mentre in 938 radiol med ( 2008 ) 113 : 923940 tend to involve the pharyngeal , oesophageal and gastric phases , whereas in paediatric patients , the oral preparatory and oral transport phases are more commonly affected . 
the prevalence in the general population is estimated at about 20% , with a significant increase in specific subgroups such as the elderly and patients with neurodegenerative diseases , head injuries or stroke . cerebrovascular accidents ( ischaemic or haemorrhagic ) are the leading cause of disability and the third cause of death throughout the world . 
about half of these patients suffer from swallowing problems , and some 90% of these have radiological evidence of food lodging in the glossoepiglottic valleculae and reduced pharyngeal peristalsis . amyotrophic lateral sclerosis and huntingtons disease also need to be considered , as swallowing disorders in both of these diseases have a prevalence of next to 100% . 
the clinical - diagnostic workup requires a thorough patient history ( time of symptom onset , associated symptoms , use of medications , tobacco , comorbidities ) , a correct physical examination ( evaluation of mental state , motor and sensory functions of the mouth and oral cavity , deep reflexes of the cranial nerves ) and inspection and two - handed palpation of the floor of the mouth , the tongue , the neck region and assessment of the motion of the thyroid cartilage during swallowing . the instrumental diagnostic assessment of dysphagia uses a variety of both morphological and functional techniques capable of identifying specific changes due to different underlying causes . 
despite the drawbacks associated with patient discomfort during the use of the manometric catheter , the technique is able to identify slight changes in the swallowing mechanism before they give rise to evident clinical signs , thus providing the time required to implement the necessary rehabilitative strategies aimed at improving the patients quality of life . 
the combined videofluoroscopy and manometry study aims to overcome the limitations of each of these techniques . videofluoroscopy provides images of the events occurring during bolus transport but fails to give information regarding what causes its motion , i.e. 
la prevalenza nella popolazione generale viene stimata intorno al 20% con aumenti significativi in popolazioni specifiche come quella anziana , nei soggetti affetti da malattie neurodegenerative , nei traumatizzati cranici , negli ictus cerebri . gli accidenti cerebrovascolari ( ischemici o emorragici ) costituiscono tuttora la prima causa di disabilit nel mondo e la terza causa di morte . 
circa il 50% di questi soggetti lamentano sintomi disfagici e il 90% circa di coloro che lamentavano una sintomatologia disfagica avevano evidenze radiologiche quali stasi nelle vallecole glossoepiglottiche e ridotta peristalsi faringea . devono essere prese , inoltre , in gran considerazione anche la sclerosi laterale amiotrofica e la malattia di huntington , poich in entrambe queste malattie il sintomo disfagia raggiunge una prevalenza sostanzialmente del 100% , ma , nel caso della sla , la precocit di insorgenza e la rapidit del decorso , fino a rendere necessaria lalimentazione per via enterale , sono decisamente maggiori . 
liter clinico - diagnostico richiede unadeguata anamnesi del paziente ( tempo di comparsa del sintomo , sintomi associati , uso di farmaci , tabacco , fumo , preesistenti patologie ) , un corretto esame obiettivo ( valutazione dello stato mentale del paziente , delle funzioni motorie e sensitive della bocca e del cavo orale , dei riflessi profondi dei nervi cranici ) , osservazione e palpazione bimanuale del pavimento della bocca , della lingua , della regione del collo e dei movimenti dello scudo cartilagineo tiroideo durante gli atti deglutitori . 
 la diagnostica strumentale delle disfagie si avvale di differenti tecniche di studio sia di tipo morfologico che funzionale che mettono in evidenza alterazioni specifiche delle diverse cause di disfagia . possiamo dunque affermare , che lesame combinato videofluoromanometrico risulta essere una metodica valida nello studio delle alterazioni della deglutizione , in quanto , nonostante sia gravata da qualche discomfort legato in particolare alluso del catetere manometrico , permette di evidenziare anche fini alterazioni del complesso meccanismo deglutitorio prima ancora che esse diano evidenza clinica conclamata dando il tempo di potere applicare tutte quelle manovre riabilitative atte a donare al paziente disfagico un migliore qualit di vita . 
on the other hand , manometry alone is unable to correlate pressure recordings with the various phases of bolus transit or measure the pressure applied to the bolus and the pressure generated by the bolus itself , or determine the relationship between pressure and the velocity of bolus motion . 
lastly , conventional manometry is unable to define which anatomical structures tongue , palate , larynx or pharynx generate the pressure recorded at a given moment . only combined videofluoroscopy and manometry is able to measure the pressure generated by each anatomical structure , the pressure gradients required to move the bolus , and the pressure of the bolus motion . 
this assessment enables the choice of optimal therapy and , on the basis of the correction of motor and / or pressure anomalies , avoids expensive and cumbersome treatment options , such as percutaneous endoscopic gastrostomy . la videofluoroscopia documenta per immagini ci che avviene durante il transito del bolo ma non d informazioni su ci che provoca il passaggio , cio le pressioni generate dalla contrazione e dal movimento di numerose strutture muscolari . 
daltra parte con la manometria impossibile correlare le pressioni registrate con le varie fasi del passaggio del bolo , misurare le pressioni applicate al bolo e quelle generate dal bolo stesso , determinare la relazione fra pressione e velocit di flusso del bolo . 
infine la manometria tradizionale non in grado di definire quale delle strutture anatomiche , lingua , palato , laringe , faringe , generi la pressione misurata in un dato momento . solo la videofluoromanometria consente la misura delle pressioni generate da ogni formazione anatomica , dei gradienti di pressione necessari al movimento del bolo , delle pressioni di flusso del bolo . 
pozzi mucelli gg idelson - gnocchi srl naples , new york ( 2008 ) isbn - 13 : 978 - 8 - 8794 - 7473 - 3 published online : 22 september 2008 springer - verlag 2008 this book is a practical overview of pancreatic computer tomography ( ct ) based on the broad experience of the contributors . 
it is dedicated to carlo procacci , a well - known radiologist of verona , italy , who died in 2004 . the book is divided into ten chapters that cover the different aspects of diagnostic ct of the pancreas . 
the various radiological aspects of acute and chronic pancreatitis , exocrine and endocrine pancreatic cancer ( adenocarcinoma , neuroendocrine tumours , cystic cancer , rare neoplasms ) , traumatic abnormalities , imaging aspects of the gland after surgery and imaging findings after pancreas transplantation are reported in detail . we emphasise that not only are the characteristics of imaging the common pancreatic diseases described , but unusual or rare aspects of pancreatic pathology are also covered . 
another important aspect is that the initial approach to the various pancreatic diseases is based on clinical , surgical and pathological aspects and their relationship with imaging findings . questo libro una panoramica sullutilizzo della tomografia computerizzata ( tc ) nelle malattie del pancreas , basata sulla grande esperienza degli autori . 
sono riportati in dettaglio i vari aspetti della radiologia della pancreatite acuta e cronica , delle neoplasie esocrine ed endocrine ( adenocarcinoma , tumori neuroendocrini , neoplasie cistiche , neoplasie rare ) , gli aspetti post - traumatici , gli aspetti della ghiandola dopo intervento chirurgico e , infine , limaging tc dopo trapianto di pancreas . sono riportate in modo semplice e chiaro le caratteristiche morfologiche tc delle comuni malattie pancreatiche come pure gli aspetti di patologie pancreatiche insolite o rare . 
un altro aspetto importante del libro lapproccio iniziale delle varie malattie del pancreas basato su aspetti clinici , chirurgici e anatomo - patologici e sulle loro relazioni con i risultati dellimaging . it is a great pity that a book of this importance is written in italian only and therefore will not gain the international appreciation it deserves . un vero peccato che il libro per la sua importanza sia scritto in italiano e per questo motivo non possa avere un apprezzamento internazionale . a final note : radiologists will find all the information in this book valuable in their daily practice . 
internists , gastroenterologists and surgeons will also find it useful to better understand the information provided by modern ct radiology . nota finale : il radiologo trover nel libro tutte le informazioni utili per la sua pratica quotidiana . 
contrast - enhanced hepatic ultrasonography with the us contrast agent sonovue was performed on 38 patients with diagnoses of hepatic cirrhosis based on unequivocal clinical signs or liver biopsy findings ( childpugh classes a in 19 , b in 16 and c in three ) , 31 patients with noncirrhotic diffuse liver disease ( biopsy confirmed ) and 14 controls without diffuse liver disease . 
stato effettuato lesame ecografico del fegato con mezzo di contrasto sonovue in 38 pazienti con diagnosi di cirrosi basata su segni clinici inequivocabili o su biopsia epatica ( child - pugh a in 19 pazienti , b in 16 e c in 3 )  . 
sono stati analizzati i diagrammi tempo / intensit di segnale della vena sovraepatica utilizzando criteri oggettivi per determinare il tempo di inizio dellenhancement ( tempo di arrivo della vena sovraepatica ) e il picco di enhancement ( tempo di picco della vena sovraepatica )  . 
il tempo di arrivo della vena sovraepatica nei pazienti cirrotici risultato significativamente pi breve ( p < 0 , 01 ) rispetto ai pazienti non cirrotici ( patologia epatica cronica e controlli )  . 
lanalisi del tempo di inizio dellenhancement contrastografico della vena sovraepatica appare un potenziale e non invasivo supplemento allecografia convenzionale e allesame doppler nel follow - up di pazienti con patologia epatica cronica diffusa . 
in contrast , there is an increase in intrahepatic vascular resistance , which results in reduced portal blood flow and liver perfusion and compensatory increases in arterial inflow [ 2 , 3 ]  . 
intrahepatic shunts can also develop between branches of the portal vein ( pv ) , the hepatic veins ( hv ) , and the hepatic artery [ 4 ]  . 
early changes in portal flow may be caused by distortion of the portal branches , capillarisation of sinusoids , and contractile activity of activated stellate cells located in the space of disse [ 5 , 6 ]  . 
intrahepatic portal - systemic collaterals can increase resistance to portal flow , and their formation precedes the clinical manifestations of portal hypertension [ 6 , 7 ]  . the first - line imaging study for the workup of patients with diffuse liver disease is often b - mode ultrasonography ( us ) [ 8 ]  . 
some authors also include doppler studies in the sonographic evaluation of patients with chronic liver disease , although it does not appear to have any major impact on the accuracy of diagnosing cirrhosis [ 14 ]  . the recently developed technique of contrast - enhanced ultrasonography ( ceus ) has expanded the possibilities for sonographic haemodynamic studies . 
intravascular flow signals are enhanced by the presence of small gas - filled microbubbles that are administered intravenously [ 1517 ]  . la cirrosi associata ad alterazioni emodinamiche intraepatiche e sistemiche . 
la circolazione sistemica nei pazienti cirrotici diventa iperdinamica con un incremento di gittata cardiaca e una riduzione delle resistenze vascolari che incrementano il flusso attraverso il circuito splancnico e gli altri distretti [ 1 ]  . 
per contro , c un incremento delle resistenze vascolari cui consegue una riduzione del flusso portale e della perfusione del fegato ed un incremento del flusso arterioso di tipo compensatorio [ 2 , 3 ]  . 
le modificazioni precoci del flusso portale possono essere causate dalla distorsione dei rami portali , dalla capillarizzazione dei sinusoidi e dalla attivit contrattile delle cellule stellate attivate localizzate nello spazio di disse [ 5 , 6 ]  . 
gli shunt intraepatici porto - sistemici possono incrementare la resistenza al flusso portale e la loro formazione precede le manifestazioni cliniche dellipertensione portale [ 6 , 7 ]  . spesso lecografia ( us ) , tra gli esami di diagnostica per immagini , il primo con il quale vengono studiati i pazienti affetti da patologia epatica diffusa [ 8 ]  . 
alcuni autori includono anche lesame doppler nella valutazione ecografica dei pazienti con patologia diffusa del fegato sebbene questo esame non sembra avere un impatto maggiore in termini di accuratezza nella diagnosi di cirrosi [ 14 ]  . il recente sviluppo tecnico dellecografia con mezzo di contrasto ( ceus ) ha migliorato le possibilit diagnostiche 862 radiol med ( 2008 ) 113 : 860874 these contrast agents can be used for kinetic studies to evaluate haemodynamic changes accompanying cirrhosis [ 18 ]  . previous research has shown , for example , that contrast enhancement of the hv begins earlier in cirrhotic patients than it does in noncirrhotic subjects [ 19 ]  . 
most of these studies were performed with first - generation us contrast enhancement achieved with microbubbles that are easily destroyed by the energy from the sound waves used for scanning . 
these blood - pool contrast agents allow simpler and more accurate assessment of the haemodynamic changes associated with chronic liver disease [ 20 ]  . few data are available on contrast - agent transit times in patients with chronic liver disease other than that related to hepatitis c virus ( hcv ) [ 21 ]  . the primary objective of this prospective study was to determine whether analysis of us contrast - agent transit times could be used to reliably differentiate liver cirrhosis from noncirrhotic stages of liver disease . 
our secondary aim was to compare its performance in this setting with that of a score based on commonly evaluated b - mode us and doppler parameters . materials and methods the study protocol , which conformed to the guidelines outlined in the 1975 declaration of helsinki , was preapproved by the institutional ethics committee . 
ricerche precedenti hanno mostrato , per esempio , che lincremento di contrasto a livello della vena sovraepatica precoce nei pazienti cirrotici rispetto ai pazienti non cirrotici [ 19 ]  . 
la maggior parte di questi studi stata effettuata con mezzo di contrasto ecografico di prima generazione costituito da microbolle che sono facilmente distrutte dallenergia degli ultrasuoni utilizzati per effettuare lesame . 
invece , le microbolle stabilizzate che compongono il mezzo di contrasto ecografico di seconda generazione , rimangono in circolo pi a lungo permettendo una corretta scansione in real - time . 
sono disponibili pochi dati riguardanti il tempo di transito nei pazienti con epatite cronica a prescindere da quelli relativi allepatite c [ 21 ]  . lo scopo primario di questo studio prospettico stato di determinare se lanalisi del tempo di transito del mezzo di contrasto ecografico di seconda generazione potesse essere utilizzata per differenziare la patologia cirrotica da quella pre - cirrotica . 
il secondo obiettivo stato di comparare il tempo di arrivo del mezzo di contrasto con un punteggio ( score ) costituito dalle principali valutazioni ecografiche b - mode e dai parametri doppler . 
they included 14 patients ( eight men ) aged 2883 years ( mean 53 years ) with no liver disease based on history and blood chemistry data ( control group ) and 69 who had diffuse chronic liver disease . 
none of the patients in the control group was taking any type of medication that could influence intraor extrahepatic circulation . the 69 patients with chronic liver disease were divided into two subgroups . 
the first subgroup consisted of 31 patients ( age range 3075 years ) in whom the presence of chronic liver disease and the absence of cirrhosis had been confirmed by liver biopsy ( noncirrhotic group )  . 
the second subgroup consisted of 38 patients ( age range 3784 years ) ( cirrhotic group ) with cirrhosis who had been diagnosed based on either liver biopsy ( 2 ) or commonly accepted clinical criteria . 
this criteria consisted of a history of chronic liver disease coupled with two or more of the following il protocollo di studio , conforme alle linee guida della dichiarazione di helsinki del 1975 , stato preventivamente approvato dal comitato etico ed stato richiesto il consenso informato scritto a tutti i pazienti reclutati . pazienti esaminati nel periodo compreso tra il 2004 e marzo 2007 , stata studiata una serie consecutiva di 83 pazienti ( tabella 1 )  . 
il gruppo includeva 14 pazienti ( 8 uomini ) di et compresa fra 28 e 83 anni ( et media 53 anni ) senza patologia epatica come desunto dai dati clinico - laboratoristici ( gruppo di controllo ) e 69 pazienti con epatopatia diffusa . 
pt , tempo di protrombina ; alt , alanina aminotransferasi ( 40 iu / l ) ; score meld per stadiazione della patologia epatica ; anumero di pazienti ; bp < 0 , 01 versus altri gruppi ; cp < 0 , 01 versus gruppo dei non cirrotici signs of portal hypertension : endoscopic evidence of oesophageal or gastric varices and / or portal hypertensive gastropathy , presence of hypersplenism ( white blood cells < 3 , 500 / mm3 and / or platelet count < 100 , 000 / mm3 ) or clinical / us evidence of ascites [ 22 , 23 ]  . 
 a single independent liver pathologist blinded to the patients clinical data and the results of their hepatic us examinations examined all liver biopsies performed in patients with chronic liver disease . 
 the demographic and clinical characteristics of the three study groups are shown in table 1 . cui la presenza di epatite cronica e lassenza di cirrosi era stata confermata da biopsia epatica ( gruppo dei non cirrotici ) e 38 pazienti ( range det : 3784 anni ) ( gruppo dei cirrotici ) con cirrosi diagnosticata o con biopsia ( n = 2 ) o con criterio clinico comunemente accettato . 
dal punto di vista clinico viene comunemente considerata cirrosi una storia di patologia epatica cronica associata a due o pi dei seguenti segni di ipertensione portale : evidenza endoscopica di varici esofagee o gastriche e / o gastropatia ipertensiva , presenza di ipersplenismo ( globuli bianchi ematici < 3500 / mm3 e / o conteggio piastrinico < 100000 / mm3 ) o evidenza clinica / ecografica di ascite [ 22 , 23 ]  . 
la severit della cirrosi stata valutata con il sistema child - pugh [ 24 ] e meld ( model for end - stage liver disease ) [ 25 ]  . 
 un anatomo - patologo indipendente specializzato in pa864 ultrasound analysis examinations were carried out by two blinded examiners using a ge logiq 9 scanner and a 3.5 - mhz convex transducer . 
 the examination began with a standard b - mode scan followed by colour and power doppler examinations [ pulse repetition frequency ( prf ) 1 , 000 hz , low wall filters for colour doppler ]  . 
in nine of the 69 subjects , an acceptable signal could not be obtained from this vein due to abdominal gas , and the left ( three subjects ) or right ( six subjects ) hv was used in these cases . 
the hv segment included in the gate was always at least 3 cm long , and every effort was made to exclude adjacent arterial and / or portal vessels from the region of interest . 
the amount of time required for the contrast agent to reach the hv [ hepatic - vein arrival time ( hvat ) ] and the time required for peak enhancement of this vein [ heradiol med ( 2008 ) 113 : 860874 tologia epatica ha esaminato le biopsie epatiche dei pazienti con epatite cronica senza essere a conoscenza dei dati clinici e dei risultati dellesame ecografico . 
la valutazione di attivit istologica stata determinata con lo score haiknodell ( histology activity index ) [ 26 ]  . le caratteristiche cliniche e demografiche dei tre gruppi di studio sono mostrate nella tabella 1 . analisi ecografia gli esami ecografici sono stati condotti da due esaminatori in cieco utilizzando un ecografo ge logiq 9 con trasduttore convex da 3 , 5 mhz . 
 nella prima parte dellesame sono state effettuate scansioni b - mode standard seguite da esame color e power doppler ( prf = frequenza di ripetizione pulsata : 1000 hz , bassi filtri di parete per lesame color doppler )  . 
 stato assegnato un punto per ciascuna delle seguenti caratteristiche : margini epatici polilobati , ipertrofia del lobo caudato , diametro longitudinale della milza > 12 cm ; velocit di flusso nella vena porta < 16 cm / s ; congestion index > 0 , 08 e indice di resistenza dellarteria epatica > 0 , 65 [ 28 ]  . 
 analisi della performance del mezzo di contrasto ecografico la seconda fase dellesame rappresentata dalla valutazione del tempo di transito del mezzo di contrasto ecografico . sono stati registrati inizialmente i segnali di base della hv ( vena sovraepatica ) per 20 secondi . 
successivamente stato iniettato manualmente un bolo di 2 , 5 ml di mezzo di contrasto ecografico , sonovue ( bracco spa , milano , italia ) , nella vena antecubitale alla velocit di 1 ml / secondo seguito da un bolo di 2 , 5 ml di soluzione fisiologica alla stessa velocit . 
 stata effettuata una registrazione dellenhancement contrastografico della hv per 130 secondi dopo liniezione di mezzo di contrasto . per la valutazione del tempo di transito del mezzo di contrasto , stata posizionata una roi sopra la vena sovraepatica media ad almeno 3 cm dalla confluenza dove gli radiol med ( 2008 ) 113 : 860874 fig . 
2a - c signal - enhancement time curves showing hepatic - vein arrival time ( white arrows ) for contrast enhancement in a in a control patient ( 27 s after the initiation of the contrast - agent injection ) ; b a patient with precirrhotic liver disease ( 23 s from contrast injection ) and c a cirrhotic patient ( 13 s from contrast infusion )  . 
2a - c diagrammi intensit di segnale / tempo che mostrano il tempo di arrivo del mezzo di contrasto nella vena sovraepatica ( frecce bianche ) in a paziente di controllo ( 27 secondi dopo linizio delliniezione di mezzo di contrasto ) ; b paziente con patologia pre - cirrotica ( 23 s dalliniezione del mezzo di contrasto ) ; c paziente cirrotico ( 13 s dalliniezione del mezzo di contrasto )  . 
le frecce sono posizionate sotto il secondo punto della curva in cui lintensit di segnale eccede la linea basale di intensit del 10% . 866 radiol med ( 2008 ) 113 : 860874 patic - vein peak enhancement time ( hvpet ) ] were then measured from the initiation of the contrast - agent injection ( second 21 of the recording )  . 
hvpet was expressed as the interval from the beginning of the sonovue injection time to the point on the curve representing maximal signal intensity . patients vital signs were monitored for 1 h after the examination , and patients were interviewed by phone 48 h after discharge to identify any adverse effects . statistical analysis hvat and hvpet data were expressed as group meansstandard deviations ( sd )  . 
mcgraw - hill primer statistical software ( second edition , 1986 ) was used for all analyses . for assessment of interobserver variation in measurements of contrast - agent transit times and us / doppler scores , the videotapes of each examination were independently and blindly reviewed by the two observers . 
interand intraobserver agreement in classification of patients as cirrhotic versus noncirrhotic was calculated using statistics . results ultrasound and doppler findings the results of the conventional b - mode and doppler examinations in the three groups are summarised in table 2 . 
in 9 dei 69 pazienti , non stato ottenuto un segnale accettabile della vena sovraepatica media per meteorismo intestinale e in questi casi , sono state utilizzate la vena sovraepatica sinistra ( 3 pazienti ) o destra ( 6 pazienti )  . 
il segmento della hv che era incluso nella roi era lungo almeno 3 cm ed stato fatto il possibile per escludere i rami arteriosi adiacenti e / o i vasi portali dalla regione dinteresse . 
sono stati misurati dal momento delliniezione del mezzo di contrasto ( 21 secondi dallinizio della registrazione ) il tempo necessario al mezzo di contrasto per raggiungere la hv [ tempo di arrivo a livello della vena sovraepatica ( hvat ) ] e il tempo necessario al raggiungimento del picco di enhancement sempre a livello della hv [ tempo di picco a livello della vena sovraepatica ( hvpet ) ]  . 
i parametri vitali del paziente sono stati monitorati per 1 h dopo lesame e i pazienti sono stati richiamati al telefono 48 h dopo lesame per verificare leventuale presenza di reazioni avverse . analisi statistica i dati dellhvat e dellhvpet sono stati espressi come gruppo mediodeviazione standard . 
le differenze fra i tre gruppi ( pazienti cirrotici , non - cirrotici e pazienti di controllo ) sono stati valutati con lanalisi della varianza , e il valore p < 0 , 05 stato considerato significativo . 
per la valutazione della variabilit delle misurazioni del tempo di transito del mezzo di contrasto e dello score us / doppler , il videotape di ciascun paziente stato rivalutato indipendentemente e in cieco da due osservatori . 
no cirrhotic patients were negative for all three doppler criteria . total us / doppler scores of four or more were recorded for 0 / 14 controls , 1 / 31 of the noncirrhotic patients and 18 / 38 of the cirrhotic patients . 
the majority of these patients had normal - sized spleens ( 3 / 20 ) , smooth hepatic margins ( 18 / 20 ) and no evidence of caudate - lobe hypertrophy ( 18 / 20 ) ; in some cases ( 12 / 20 ) , the mean pv flow velocity was also within normal limits ( probably as a result of intraand extrahepatic shunting )  . contrast - enhanced ultrasound us and doppler studies were completed and hvat and hvpet were successfully calculated for all study participants . 
laccordo intered intraosservatore nella classificazione dei pazienti come cirrotici piuttosto che come non cirrotici stato calcolato utilizzando la statistica  . risultati conclusioni b - mode e doppler i risultati degli esami b - mode standard e doppler dei tre gruppi sono riassunti nella tabella 2 . 
il diametro longitudinale della milza nei pazienti cirrotici stato significativamente maggiore rispetto a quello dei pazienti di controllo e dei pazienti con patologia epatica diffusa non cirrogena ( p < 0 , 01 )  . 
per quanto riguarda le caratteristiche doppler , lindice di resistenza medio dellarteria epatica ha , nel gruppo cirrotico ( 0 , 740 , 06 ) stato significativamente ( p < 0 , 01 ) pi alto rispetto a quello degli altri due gruppi . 
il flusso medio portale ( pv ) risultato significativamente ( p < 0 , 01 ) pi basso nei pazienti cirrotici ( 17 , 26 , 3 ) rispetto ai controlli ( 32 , 914 , 4 ) e ai pazienti con patologia diffusa non cirrogena ( 25 , 610 , 4 )  . 
i pazienti cirrotici avevano anche un congestion index medio signifi868 radiol med ( 2008 ) 113 : 860874 the cirrhotic group was significantly shorter than both that of the control group and of patients with noncirrhotic liver disease ( p < 0.01 ) ( table 3 )  . 
reexamination of these three patients indicated that the values recorded probably reflected enhancement of a vessel other than the hv . comparison of the vessel examined by the gate with low mechanical index and the one captured in the prerecording image from the original examination revealed that the vessels were not the same . 
 hvpet also decreased progressively as liver status worsened , and the mean value for the cirrhotic group ( in contrast to that of the noncirrhotic patients ) was significantly reduced compared with that of the control group ( table 3 )  . 
when stratified according to the child - pugh score , cirrhotic patients showed a progrescativamente ( p < 0 , 01 ) pi alto ( 0 , 110 , 05 ) rispetto ai controlli ( 0 , 030 , 01 ) e ai pazienti non cirrotici ( 0 , 060 , 02 )  . nessun paziente cirrotico era negativo per tutti e tre i criteri doppler . in 0 / 14 controlli , 1 / 31 pazienti con epatopatia cronica e in 18 / 38 pazienti cirrotici si sono evidenziati score totali us / doppler di 4 punti o pi . 
la maggior parte di questi pazienti aveva la milza di dimensioni normali ( 3 / 20 ) , margini epatici lisci ( 18 / 20 ) e non presentavano ipertrofia del lobo caudato ( 18 / 20 ) ; in alcuni casi ( 12 / 20 ) , la velocit media del flusso portale era normale ( probabilmente a causa della presenza degli shunt intraed extra - epatici )  . ecografia con mezzo di contrasto tutti gli studi ecografici e doppler sono stati completati e sono stati successivamente calcolati hvat e hvpet in tutti i partecipanti allo studio . 
lintervallo medio nel gruppo cirrotico stato significativamente pi breve rispetto al gruppo dei controlli e a quello dei pazienti con cirrosi ( p < 0 , 01 ) ( tabella 3 )  . 
se non altrimenti indicato le differenze fra i gruppi non sono risultate statisticamente significative . ap < 0 , 01 versus altri gruppi combinati , bp < 0 , 01 versus pazienti di controllo radiol med ( 2008 ) 113 : 860874 17 seconds control patients non - cirrhotic patients cirrhotic patients control patients non - cirrhotic patients cirrhotic patients fig . 
 sive reduction of mean hvats as liver status worsened ( table 4 ) ; however , we found no statistically significant differences among subsets based on child - pugh classes . 
il confronto del vaso esaminato con la roi a basso indice meccanico con quello visualizzato nelle immagini pre - registrazione originali ha rivelato che il vaso non era lo stesso . 
la ripetizione dellesame in questi pazienti ha evidenziato un hvat di 20 , 21 e 22 secondi rispettivamente , valori che sono risultati perfettamente coerenti con quelli degli altri pazienti con patologia epatica diffusa non cirrogena confermata dalla biopsia ( cio , 18 secondi o pi )  . 
lanalisi dei risultati originali ( i risultati corretti dei tre pazienti sopra descritti non sono stati considerati nellanalisi statistica ) ha mostrato che il cut - off di 17 secondi dellhvat distingueva i pazienti cirrotici dai 45 pazienti senza cirrosi con un 100% di sensibilit e 93 , 3% di specificit . 
 lhvpet inoltre decresce progressivamente al peggiorare dello stato del fegato , e il valore medio per il gruppo cirrotico ( a differenza di quello dei pazienti non cirrotici ) era significativamente ridotto in confronto con quello del gruppo di controllo ( tabella 3 )  . 
i pazienti cirrotici dopo essere stati suddivisi secondo il sistema child - pugh , hanno mostrato una progressiva riduzione dellhvat medio al peggiorare dello stato del fegato ( tabella 4 ) ; non sono state trovate differenze statisticamente significative fra i sottogruppi della classificazione childpugh . 
tutti i 20 pazienti cirrotici che sono stati classificati in base allo score us / doppler sono stati correttamente diagnosticati mediante hvat . laccordo interosservatore stato notevolmente pi basso per lo score us / doppler ( coefficiente = 0 , 75 )  . 
all 20 cirrhotic patients who were misclassified based on us / doppler scores were correctly diagnosed based on hvat . i pazienti con epatite cronica , una volta sviluppata la cirrosi , necessitano di un follow - up pi stretto [ 29 ] , inclusa lecografia delladdome ( idealmente ogni 612 mesi ) per evidenziare la presenza di epatocarcinoma [ 30 ]  . 
 discussion once cirrhosis has developed , patients with chronic liver disease require more frequent follow - up [ 29 ] , including sonographic examination of the abdomen ( ideally every 612 months ) to rule out the presence of hepatocellular carcinoma [ 30 ]  . 
changes in the surface and dimensions of the liver , splenic enlargement , slowed portal flow and increased ha resistance are all highly specific signs associated with cirrhosis , but they are present only in a limited number of patients . 
 in our study , we demonstrated that analysis of transit times for the second - generation us contrast agent sonovue can be useful in the diagnosis of cirrhosis in patients with chronic liver disease . 
in the group of 38 cirrhotic patients we examined , the onset of contrast enhancement in the hv occurred significantly earlier than it did in noncirrhotic patients ( with or without chronic liver disease )  . 
in fact , hvat alone was superior for excluding the presence of cirrhosis compared with a us / doppler score based on six different markers of liver cirrhosis or its complications ( such as portal hypertension )  . 
for ethical reasons , we do not propose liver biopsy for cirrhotic patients whose diagnosis has already been established on the basis of clinical and / or endoscopic findings [ 23 ]  . 
le modificazioni della superficie e delle dimensioni del fegato , laumento volumetrico della milza , il rallentamento del flusso portale e lincremento degli indici di resistenza della ha sono tutti segni altamente indicativi di cirrosi , ma sono presenti solo in un numero limitato di pazienti . 
 in questo studio , stato dimostrato che lanalisi del tempo di transito del mezzo di contrasto ecografico di seconda generazione sonovue pu essere utile nella diagnosi di cirrosi nei pazienti con epatite cronica . 
nel gruppo dei 38 cirrotici che sono stati esaminati , linizio dellenhancement contrastografico nella hv stato significativamente pi precoce rispetto a quello dei pazienti non cirrotici ( con o senza patologia cronica del fegato )  . 
infatti , solo hvat risultato superiore nella esclusione della presenza di cirrosi confrontato con lo score us / doppler basato su sei differenti caratteristiche di cirrosi o sulle sue complicanze ( ad esempio lipertensione portale )  . una delle limitazioni potenziali del nostro studio che la maggior parte dei pazienti cirrotici stata diagnosticata basandosi su criteri largamente accettati ( ad esempio segni di scompenso della funzionalit epatica in un paziente con una storia conosciuta di patologia epatica diffusa ) , senza conferma bioptica . 
per ragioni etiche , non abbiamo proposto la biopsia epatica ai pazienti cirrotici la cui diagnosi era gi stata definita sulla base di criteri clinici e / o endoscopici [ 23 ]  . 
questa una delle ragioni per le quali un approccio non invasivo ad una diagnosi di cirrosi ( ad esempio ceus , transient elastografia [ 22 ] ) cos necessaria ( specialmente per i casi nei quali i segni clinici sono inconcludenti )  . 
i due pazienti cirrotici la cui diagnosi era basata sulla biopsia epatica ( un paziente con infezione cronica hcv correlata e laltro con cirrosi biliare primitiva ) presentavano segni clinici , biochimici ed endoscopici negativi per cirrosi al tempo dellarruolamento . 
nondimeno , il loro hvat ( 12 e 14 secondi ) era entro il range dei pazienti con cirrosi . questi due casi suggeriscono che lanalisi dellhvat potrebbe anche essere utile per la diagnosi di cirrosi non clinicamente apparente . 
the two cirrhotic patients whose diagnoses were based on liver biopsy ( one with chronic hcv infection , and the other with primary biliary cirrhosis ) presented clinical , biochemical and endoscopic profiles that were negative for cirrhosis at the time of enrolment . 
these two cases suggest that hvat analysis might also be useful for diagnosing cirrhosis that is not clinically apparent . the cases described above tend to confirm the hypothesis of sugimoto et al . 
although this finding contrasts with those of other investigators [ 33 ] , our experience suggests that ceus is probably of limited value for assessing the severity of precirrhotic liver disease , which is generally not associated with intrahepatic shunting . 
the latter finding is not surprising , as the liver failure reflected by these scores is related mainly to loss of functioning hepatocytes . transit - time analysis during ceus thus focuses on a different aspect of cirrhosis ( intrahepatic shunting ) from those normally considered in clinical settings , e.g. 
 hvat analysis during ceus also displayed better reproducibility than the us / doppler score : only two patients with noncirrhotic chronic liver disease were discordantly classified by the two examiners based on hvat analysis . 
sebbene questi risultati ottenuti contrastino con quelli di altri ricercatori [ 33 ] , la nostra esperienza suggerisce che la ceus probabilmente di valore limitato per la valutazione della severit della patologia epatica diffusa pre - cirrotica , che non generalmente associata con gli shunt intraepatici . 
nel gruppo di pazienti con cirrosi , lhvat non apparsa correlata alleziologia ( alcolica vs . virale ) , ai segni clinici di ipertensione portale ( ascite e varici esofagee ) , o allutilizzo di farmaci anti - ipertensivi , e non ha mostrato correlazione con la classificazione childpugh ( tabella 4 )  . 
 lanalisi del tempo di transito ceus focalizza cos lattenzione su un diverso aspetto della cirrosi ( shunt intraepatici ) da quello normalmente considerato tra i segni clinici , ad esempio lipertensione portale , lipersplenismo e i segni biochimici di insufficienza epatica . 
nella nostra casistica , luso dellanalisi dellhvat nei 20 pazienti cirrotici ha permesso una diagnosi corretta in tutti i casi in cui la diagnosi non era stata corretta sulla base dello score us / doppler . lanalisi dellhvat durante lesame ceus mostra anche una migliore riproducibilit rispetto allo score us / doppler : solo due pazienti con epatite cronica sono stati classificati in modo discordante dai due esaminatori sulla base dellanalisi hvat . 
le tre diagnosi di falsi positivi ceus che ci sono stati in questo studio ( due con epatite cronica c , laltro con epatite autoimmune con hvat di 17 , 15 e 17 secondi ) sono stati causati dallerrato posizionamento della roi su un vaso diverso dallhv . 
the three falsepositive ceus diagnoses that emerged from this study ( two with chronic hepatitis c , the other with autoimmune hepatitis , with hvats of 17 , 15 , and 17 s , respectively ) were caused by faulty placement of the gate over a vessel other than the hv . 
although it is fairly simple to position the gate over the hv , when the screen subsequently goes black ( due to the low mechanical index ) , the gate may inadvertently be shifted ( particularly if the patient moves )  . 
to our knowledge , the only condition other than cirrhosis that would be expected to reduce the hvat is the presence of a primary intrahepatic arterialportal venous fistula , which is extremely rare [ 34 ]  . conclusions in conclusion , the follow - up of patients with chronic liver disease inevitably becomes more intensive after the onset of cirrhosis , which is a major risk factor for hepatocellular carcinoma . 
reliable identification of patients who are still in the precirrhotic stages of disease can thus save time and reduce the costs of follow - up , as these patients can usually be managed with a lower - frequency schedule of examinations ( us , endoscopy , clinical workup )  . 
b - mode us , with or without doppler studies , has proved to be a safe , economical approach that can diagnose cirrhosis with a high level of specificity , but its negative predictive value is low . 
per conoscenza , lunica condizione diversa dalla cirrosi che ci potremmo aspettare come causa di riduzione dellhvat la presenza di una fistola artero - portale che tuttavia estremamente rara [ 34 ]  . conclusioni in conclusione il follow - up di pazienti con epatopatia cronica inevitabilmente diventa pi intenso dopo linizio della cirrosi che rappresenta il maggior fattore di rischio di epatocarcinoma . 
una affidabile identificazione di pazienti che sono ancora in fase pre - cirrotica di malattia consente quindi di risparmiare tempo e ridurre i costi del followup perch questi pazienti possono essere abitualmente gestiti con un programma di esami poco frequenti ( ecografia , endoscopia ed esame clinico )  . 
lesame ecografico b - mode , con o senza lesame doppler , ha dimostrato di essere un sicuro approccio economico che pu diagnosticare la cirrosi con un alto livello di specificit , ma il suo valore predittivo negativo basso . 
la nostra esperienza suggerisce che lanalisi dell hvat durante lesame ceus un mezzo complementare potenzialmente utile per il follow - up dei pazienti con patologia epatica cronica diffusa del fegato . 
personal experience and pictorial assay il ruolo della tcmd nella definizione anatomica del complesso atrio sinistro - vene polmonari nei pazienti affetti da fibrillazione atriale . esperienza personale e rassegna iconografica k . 
in 63 patients , the mdct examination was performed using retrospective cardiac electrocardiographic ( ecg ) gating and dose modulation , with reconstructions performed at 75% of r - r interval . 
we identified 286 pv : 157 right and 129 leon the right side , eight pv were supernumerary and one was a common trunk , whereas on the left side , we found 22 common trunks and one supernumerary vein 61.3% of patients , the anatomical pattern was typical ( two right and two left pv )  . 
illustrare quadro tipico e varianti anatomiche del complesso atrio sinistro - vene polmonari ( as - vp ) studiato con tc spirale multidetettore a 16 strati ( tcmd ) in una popolazione di pazienti affetti da fibrillazione atriale ( fa ) in attesa di essere sottoposti ad intervento di ablazione trans - catetere in atrio sinistro . 
mdct identified branching of the right inferior pv in 94.5% , of the right superior pv in 75.6% , of the left superior pv in 7.5% and of the left inferior pv in 7.5% ; 3 / 8 of the right supernumerary veins presented branching . 
 keywords multidetector computed tomography atrial fibrillation pulmonary veins ablation anatomico era tipico ( 2 vp destre e sinistre ) e atipico nel restante 38 , 7% dei pazienti ( 26 , 6% 2 vp destre - tronco comune sinistro ; 6 , 7% 3 vp destre - 2 vp sinistre ; 2 , 6% 3 vp destre - tronco comune sinistro ; 1 , 3% 3 vp destre - 3 vp sinistre ; 1 , 3% tronco comune destro - 2 vp sinistre )  . 
nella definizione dei rami di confluenza pre - ostiali delle vp ( branching ) , la tcmd ha identificato il branching della vp inferiore destra nel 94 , 5% dei casi , della vp superiore destra nel 75 , 6% , della vp superiore sinistra nel 7 , 5% e della vp inferiore sinistra nel 7 , 5% ; 3 / 8 delle vene soprannumerarie destre presentavano branching . 
rispetto allostio delle vp sinistre , lorifizio delle 74 auricole identificate era in posizione alta nel 85 , 1% dei casi , in posizione intermedia nel 12 , 1% e bassa nel 2 , 8% . 
il radiologo deve conoscere le varianti anatomiche e farne capire limportanza allelettrofisiologo interventista . parole chiave tomografia computerizzata multidetettore fibrillazione atriale vene polmonari ablazione introduction introduzione atrial fibrillation ( af ) is the most commonly encountered cardiac arrhythmia . 
more than 5 million individuals are estimated to be affected worldwide , with a prevalence varying between 0.5% among the population aged 5059 years and 10% in subjects aged older than 80 years [ 13 ]  . 
in italy , af affects more than 500 , 000 people , and the atrial fibrillation / flutter italian registry ( fire ) study established that 1.5% of presentations to emergency departments and 3.3% of hospital admissions are related to this form of arrhythmia [ 4 ] , with a substantial use of health care resources . af is responsible for a significant increase in the risk of stroke ( five times higher than average ) , a major decrease in cardiac output and the development of tachycardia - related cardiomyopathy [ 57 ] , with a twofold higher mortality than average . 
in electrophysiological terms , af consists of a rapid and disorganised propagation of electrical impulses within the atria , with resulting deterioration of normal atrial mechanical function [ 1 ] on account of the highly irregular cardiac rhythm and often very rapid ventricular response . 
this can lead to cardiac decompensation and thrombus formation , with a high risk of thromboembolisclinically , af poses problems related to an inadela fibrillazione atriale ( fa ) laritmia cardiaca pi comune : si stima che , a livello mondiale , ne siano affetti oltre 5 milioni di individui , con una prevalenza che varia dal 0 , 5% della popolazione tra 50 e 59 anni fino al 10% dei soggetti con pi di 80 anni [ 13 ]  . 
in italia la fa colpisce pi di 500000 persone e lo studio fire ha stabilito che 1 , 5% degli accessi in pronto soccorso e 3 , 3% dei ricoveri ospedalieri correlato a questa aritmia [ 4 ] , ci che determina un notevole impegno delle strutture sanitarie . la fa responsabile di un importante aumento del rischio di stroke ( 5 volte superiore alla media ) , di una significativa diminuzione della gittata cardiaca e dello sviluppo di cardiomiopatia tachicardia - mediata [ 57 ] con un indice di mortalit 2 volte superiore alla media . 
sotto il profilo elettrofisiologico , la fa consiste in una propagazione rapida e disorganizzata dellimpulso elettrico nelle camere atriali , con conseguente compromissione della normale funzionalit meccanica [ 1 ] , stante la notevole irregolarit del ritmo cardiaco e la risposta ventricolare spesso molto elevata . 
dal punto di vista clinico , la fa pone notevoli problemi causati da unincompleta comprensione dei meccanismi fisiopatologiradiol med ( 2008 ) 113 : 779798 quate understanding of the pathophysiological mechanisms underlying the disorder . 
in addition to focal changes and various forms of reentrant activity [ 8 ] , a broad spectrum of modulating factors have been identified , including ionic and structural remodelling [ 9 ] and anatomical and haemodynamic determinants of atrial dilatation and stretching [ 10 , 11 ]  . 
the most innovative treatment strategy is transcatheter ablation of the pulmonary veins ( pv ) , which is based on the results achieved with the atrial compartmentalisation surgery ( maze procedure ) described by cox [ 12 , 13 ]  . 
the earliest transcatheter pv ablations for the treatment of af were performed in the late 1990s by haissaguerre et al . , who demonstrated that in > 90% of cases , the pv can generate the triggers responsible for cardiac rhythm disturbances [ 14 , 15 ]  . 
the triggers originate from sleeves of myocardial tissue that , during embryological development of the left atriumpulmonary vein ( la - pv ) complex , may extend or remain trapped in the ostial and preostial portions of the pv [ 16 , 17 ]  . 
a variety of ablation techniques have been developed and refined in recent years : the most commonly used aim to electrically isolate the pv from the la by using energy sources ( radiofrequency waves , thermal waves , ultrasound , laser beam ) to create linear transmural lesions around the circumference of the venous ostia [ 18 , 19 ]  . 
despite the development of nonfluoroscopic endoscopic navigation systems capable of generating three - dimensional electroanatomical maps to help identify the sites to be treated , it is nonetheless useful to precede this mapping with an imaging study providing high - resolution images . among the cardiac applications of multidetector computed tomography ( mdct ) , the study of the la - pv complex is clinically one of the most interesting [ 2332 ]  . 
although other modern multiplanar imaging techniques ( transoesophageal and intracardiac ultrasound , electron - beam tomography , magnetic resonance imaging ) are capable of depicting the complex anatomy of the region , mdct is superior in terms of higher spatial and temporal resolution and a relatively widespread availability that allows us to meet the increasing demand for such studies . 
 the aim of this paper is to illustrate the typical patterns and anatomical variants of the la - pv complex seen at 16slice mdct in a population of 75 patients affected by af and scheduled for transcatheter ablation . 
the detailed knowledge of the regional anatomy offered by mdct guarantees a more effective interventional procedure with fewer complications , as reported in the international guidelines on ablation treatment for af [ 33 , 34 ]  . 
oltre alle alterazioni di tipo focale e alle varie forme di attivit rientrante [ 8 ] , stato individuato un vasto spettro di fattori modulanti , che includono il rimodellamento ionico e strutturale ( remodeling ) [ 9 ] nonch determinanti anatomiche e emodinamiche , che sono responsabili della dilatazione e dello stretch atriale [ 10 , 11 ]  . 
 la complessit dei meccanismi fisiopatologici della fa ha influenzato il trattamento : attualmente la strategia terapeutica pi innovativa rappresentata dallablazione transcatetere delle vene polmonari ( vp ) , basata sui risultati ottenuti con gli interventi cardiochirurgici di compartimentalizzazione atriale ( maze procedure ) descritti da cox [ 12 , 13 ]  . 
le prime ablazioni trans - catetere delle vp per il trattamento della fa furono eseguite da haissaguerre alla fine del secolo scorso ; egli dimostr come , in oltre il 90% dei casi , dalle vp possono nascere impulsi ( trigger ) che stanno alla base dellinnesco dellaritmia [ 14 , 15 ]  . 
i trigger originano da bande di tessuto miocardico ( sleeves ) che , durante lo sviluppo embriologico del complesso atrio sinistro - vene polmonari ( as - vp ) , possono prolungarsi o rimanere intrappolate nelle porzioni ostiali e pre - ostiali delle vp [ 16 , 17 ]  . 
negli ultimi anni , le tecniche ablative si sono sviluppate e raffinate : attualmente , le pi utilizzate mirano alla deconnessione elettrica di tutte le vp dallatrio sinistro ( as ) attraverso la creazione di lesioni transmurali lineari che circoscrivano gli osti venosi utilizzando varie forme di energia ( onde di radiofrequenza , onde termiche , ultrasuoni , raggi laser ) [ 18 , 19 ]  . 
la esatta collocazione dei punti di ablazione sulla parete dellas vincolante sia per il successo della procedura che per la riduzione delle complicanze , prima fra tutte la stenosi delle vp [ 2022 ]  . 
nonostante siano stati sviluppati dei sistemi di navigazione endocardica non fluoroscopici , in grado di generare mappe elettro - anatomiche tridimensionali per facilitare lindividuazione dei siti da trattare , si ritiene di grande utilit far precedere a tale mappaggio unindagine che fornisca immagini a maggiore risoluzione spaziale . tra le applicazioni cardiache della tc multidetettore ( tcmd ) , lo studio del complesso as - vp tra quelli di maggiore interesse clinico [ 2332 ]  . 
bench la comprensione della complessa anatomia regionale possa essere garantita anche dalle altre moderne tecniche di imaging multiplanare ( ecografia trans - esofagea e endocardiaca , tomografia a fascio di elettroni , risonanza magnetica ) , la tcmd si dimostra superiore a queste metodiche in rapporto alle elevatissime risoluzioni spaziale e temporale e alla relativamente ampia diffusione delle apparecchiature sul territorio , ci che consente di soddisfare la crescente richiesta di indagini in tale campo . 
la conoscenza anatomica regionale , garantita dalla tcmd , indispensabile per realizzare la procedura interventistica in modo pi efficace e efficiente , riducendo nel contempo le complicanze , come riportato nelle linee guida internazionali per il trattamento mediante ablazione della fa [ 33 , 34 ]  . 
 materiali e metodi nel periodo compreso tra gennaio 2004 e marzo 2007 sono stati studiati 75 pz ( 57 maschi , 18 femmine ; et media 58 , 3 anni , et mediana 59 anni ) affetti da fa parossistica ( 43 / 75 pz , 57 , 4% ; aritmia che si interrompe spontaneamente ) e cronica ( 32 / 75 pz , 42 , 6% ) : in questultimo gruppo abbiamo accorpato le forme di fa cronica propriamente detta ( il ritmo sinusale non ripristinabile o si rinuncia a tentarne il ripristino ) e quelle persistenti ( laritmia non si interrompe spontaneamente ma solo con interventi terapeutici ) poich table 1 technical parameters of the multidetector computed tomography study of the left atrium pulmonary vein complex parameters value mas / slice field of view slice thickness ( mm ) reconstruction index ( mm ) effective slice thickness ( mm ) rotation time ( s ) pitch reconstruction filter contrast medium trigger gating 120140 180250 0.42 automatic based on patient heart rate 70100 ml + 40 saline solution @ 4 ml / s . 
 ( preferable iodine concentration 370400 mgi / ml ) automatic bolus tracking with region of interest on left atrium when possible , retrospective with reconstruction of 70%80% r - r electrocardiograph interval . dose modulation tabella 1 parametri tecnici dellesame tcmd del complesso atrio sinistro - vene polmonari valore 120140 180250 parametro mas / slice spessore di slice ( mm ) indice di ricostruzione ( mm ) spessore effettivo di ricostruzione ( mm ) tempo di rotazione ( s ) pitch filtro di ricostruzione trigger gating 0 , 42 ad adattamento automatico a seconda della frequenza cardiaca del paziente 70100 ml + 40 ml soluzione fisiologica @ 4 ml / s ( concentrazione di iodio preferibile 370400 mgi / ml ) bolus tracking automatico con roi sullas quando possibile , retrospettivo con ricostruzione del 70%80% dellintervallo rr dellecg . modulazione della dose radiol med ( 2008 ) 113 : 779798 protocol , with a scan range from the tracheal carina to the cardiac base , scanning time ranges from 10 s to 16 s , depending on heart size and rate . 
during acquisition , 70100 ml of nonionic iodinated contrast material at high concentration ( 370400 mgi / ml ) is administered via a dual - head injector at a flow rate of 4 ml / s . 
the contrast bolus is followed by a 40 - ml saline bolus chaser to ensure constant and optimal opacification of the la - pv complex and exploit the whole volume of contrast material injected , thus reducing the total amount required ( from 20% to 40% )  . 
a region of interest ( roi ) is placed over the centre of the la , and when the predefined attenuation threshold is exceeded [ 100 hounsfield units ( hu ) ] , the scan is triggered automatically ( bolus tracking )  . 
 in 63 / 75 patients , the mdct study was performed with retrospective cardiac gating : the electrocardiographic ( ecg ) trace is recorded throughout the scan , and data are reconstructed in relation to the r - wave peak of the ecg for each instant of the cardiac cycle . 
the temporal reconstruction window is placed in the end - diastolic phase of the r - r interval ( from 70% to 80% ) , which is less heavily affected by heart pulsation artefacts . 
in order to reduce patient exposure during the gated acquisition , we used dose modulation that lowers the dose to values comparable to a nongated study . in the remaining 12 patients with high - frequency af and irregular ecg , cardiac gating was not applied . 
we first evaluated the native images , then the paracoronal multiplanar reformations ( mpr ) and maximum intensity projection ( mip ) images , the volume - rendered ( vr ) images and the virtual endoscopy reconstructions ( voyager )  . 
images were initially assessed for the number of pv and the presence of preostial branching , intended as the confluence of venous branches into the terminal branch within 510 mm of the atriovenous junction . 
the transseptal angle was calculated on the native axial images just below the aortic valve plane by intersecting the line passing through the la horizontal axis with the line perpendicular to the interatrial septumeasurement of the atrial axes , which provides an estimate of the size of the atrial chamber , was performed according to the technique proposed by ho et al . 
the laterolateral axis is the length between the midpoint of the right and left pv traced on the axial oblique mpr / mip images ; the anteroposterior and craniocaudal axes are meaentrambe riconoscono identici meccanismi elettrofisiologici , risultando caratterizzate , contrariamente a quanto avviene nelle forme parossistiche , da una netta prevalenza del substrato rispetto al trigger . 
utilizzando tale protocollo di studio il tempo di scansione per coprire il volume anatomico in esame , esteso dalla carena tracheale alla base cardiaca , varia da 10 a 16 s , dipendendo sia dalle dimensioni del cuore che dalla frequenza cardiaca del paziente . 
le immagini native vengono ricostruite dai dati grezzi acquisiti da una rotazione del tubo radiogeno di 180 : conseguentemente , la risoluzione temporale per 420 ms di rotazione corrisponde a 210 ms . durante lacquisizione , mediante un iniettore a doppia testata , vengono somministrati 70100 ml di mezzo di contrasto ( mdc ) organo - iodato non - ionico con elevata concentrazione di iodio ( 370400 mgi / ml ) , ad un flusso di 4 ml / s . 
al mdc segue un bolo di 40 ml di soluzione fisiologica ( bolus chaser ) , che permette di mantenere costante e ottimale lopacizzazione del complesso as - vp e di sfruttare tutto il volume di mdc iniettato , riducendone la quantit assoluta ( dal 20% al 40% )  . 
inoltre il bolus chaser determina una riduzione dei valori di attenuazione nella vena cava superiore e nellatrio destro causati dal transito del bolo di mdc , che talora genera artefatti tali da limitare la valutazione delle vp sul lato destro . 
una regione di interesse ( roi ) viene posizionata al centro dellas e una volta superato un valore soglia predefinito ( 100 hounsfield unit , hu ) la scansione parte automaticamente ( bolus tracking )  . 
 in 63 / 75 pz lindagine tcmd stata effettuata con gating cardiaco retrospettivo : il tracciato elettrocardiografico ( ecg ) viene registrato durante tutta lacquisizione e , successivamente , i dati vengono ricostruiti con riferimento al picco r dellecg per ogni istante del ciclo cardiaco ; la finestra temporale di ricostruzione posizionata nella fase telediastolica dellintervallo rr ( dal 70% al 80% ) , laddove gli artefatti da pulsatilit cardiaca sono minori . 
allo scopo di ridurre la dose erogata al paziente durante lacquisizione gated stata attivata la modulazione della dose in grado di ridurre lesposizione a valori sovrapponibili ad un analogo esame non - gated . 
 al termine dellindagine , lanalisi e il post - processing delle immagini sono stati realizzati mediante una workstation sulla quale installato un software dedicato agli esami 784 radiol med ( 2008 ) 113 : 779798 sured at the midpoint of the transverse axis in the axial and sagittal oblique reconstructions , respectively . 
taking as a reference the venous ostia , the orifice was considered to be high when lying at the same height or above the superior vein , low when at the same height or below the inferior vein and intermediate when at midpoint between the two veins . statistical analysis differences in the incidence of the various anatomical pv variants in the groups of patients with paroxysmal and chronic af were verified by applying the chi - square test to a 22 contingency table . 
differences in the means of nominal variables , such as measurements of the atrial axes and transseptal angles , were verified by applying the students t test for unpaired data after assessing for normal distribution . results total patients with af in all patients studied , we identified 286 pv , of which 157 were on the left and 129 on the right . 
data are summarised in table 3 . in 75 / 75 patients , the transseptal angle was between 43 and 80 , with a mean value of 645.7 and a median value of 65 . 
with regard to atrial axes , the mean anteroposterior axis was 41.9 mm ( median 42 mm ) ; the mean lateral axis was 73.4 mm ( median 72.5 mm ) ; the mean craniocaudal axis was 62.3 mm ( median 62.5 mm ) ( table 4 )  . 
 cardio - tc , rispettando un percorso a tappe standardizzato , che inizia dalla valutazione delle immagini native , per passare a quella delle ricostruzioni multiplanari ( mprmip ) sui piani paracoronali , quindi delle ricostruzioni in volume rendering ( vr ) e concludersi con lanalisi delle ricostruzioni in endoscopia virtuale ( voyager )  . 
innanzitutto , sono stati valutati numero delle vp e presenza di branching pre - ostiale , inteso come confluenza di rami venosi nel vaso terminale a meno di 510 mm dallo sbocco di questultimo nellas . 
successivamente , sono state effettuate le misurazioni dellangolo trans - settale e degli assi atriali : il primo stato calcolato sulle immagini assiali native poste immediatamente al di sotto del piano valvolare aortico intersecando la retta passante per lasse orizzontale dellas con la perpendicolare al setto inter - atriale ; la misurazione degli assi atriali , che fornisce una stima delle dimensioni della camera atriale , stata condotta facendo riferimento alla tecnica proposta da ho et al . 
 [ 35 ] : lasse latero - laterale la distanza passante per il punto intermedio delle vp di entrambi i lati , tracciata sulle mpr / mip assiali oblique ; gli assi antero - posteriore e cranio - caudale vengono misurati nel punto centrale dellasse trasversale , rispettivamente nelle ricostruzioni assiali oblique e sagittali oblique . 
infine , la valutazione della posizione dellorifizio dellauricola , che giace immediatamente al davanti degli osti delle vp di sinistra , stata effettuata utilizzando il voyager : prendendo come riferimento lostio delle vene , lorifizio viene considerato in posizione alta se situato alla stessa altezza o sopra alla vena superiore , bassa se alla stessa altezza o sotto la vena inferiore e , conseguentemente , intermedia quando situato tra i due vasi . analisi statistica la presenza di differenze di incidenza delle diverse varianti anatomiche delle vp nei gruppi di pazienti con fa parossistica e cronica sono state verificate applicando il test chi quadrato ad una tabella di contingenza 22 . 
la differenza delle medie di valori nominali quali le misure degli assi atriali e dellangolo transettale misurati nei pazienti con fa parossistica e cronica sono state verificate applicando il test t di student per dati non appaiati dopo verifica della normalit delle distribuzioni . risultati totalit dei pazienti con fa nei pz studiati si sono identificate 286 vp , di cui 157 a destra e 129 a sinistra . 
delle 157 vp destre , 8 sono soprannumerarie ( 5 , 0% ) e 1 tronco comune ( 0 , 6% ) ; delle 129 vp sinistre , 22 sono tronchi comuni ( 17% ) e 1 soprannumeradiol med ( 2008 ) 113 : 779798 fig . 
vp superiore destra ( 1 ) con branching precoce ( freccia ) ; vp inferiore destra ( 2 ) ; vp superiore sinistra ( 3 ) ; vp inferiore sinistra ( 4 )  . mdct depicted the appendage in 74 / 75 patients . 
 patients with paroxysmal af in the 43 / 75 patients with paroxysmal af , mdct recognised 160 pv : 88 on the right and 72 on the le of the right - sided pv , 3 / 88 were supernumerary and 1 / 88 was a raria ( 0 , 7% )  . 
 nella definizione dei rami di confluenza pre - ostiali delle vp ( branching ) , 70 / 74 vp inferiori destre ( 94 , 5% ) , 56 / 74 786 radiol med ( 2008 ) 113 : 779798 fig . 
4 two distinct pv on the right ( 1 ; 2 ) and a ct on the left : in this patient , the ct is shorter than that of the previous figure . 
4 due distinte vp a destra ( 1 , 2 ) e un tronco comune ( ct ) a sinistra : in questo paziente il ct pi corto di quello della figura precedente . 
the small ostia of the right ( white arrow ) and left ( black arrow ) suprannumerary veins are located between those of the two main pv ( 1 and 2 on the right ; 3 and 4 on the left )  . 
i piccoli osti delle vene soprannumerarie di destra ( freccia bianca ) e di sinistra ( freccia nera ) sono situati tra quelli delle vp principali ( 1 e 2 a destra ; 3 e 4 a sinistra )  . 
branching was not present in the 14 left common trunks but was present in the only case of right common trunk ( table 3 )  . in 43 / 43 patients , the transseptal angle was between 43 and 80 ( mean value 646.8 and median 65 )  . 
questi dati sono riassunti nella tabella 3 . nei 75 pazienti langolo trans - settale compreso tra 43 e 80 , con un valore medio di 645 , 7 e mediano di 65 . relativamente agli assi atriali , lantero - posteriore medio di 41 , 9 mm , mediano di 42 mm ; il latero - laterale rispettivamente di 73 , 4 e 72 , 5 mm ; infine , lasse cranio - caudale rispettivamente di 62 , 3 e 62 , 5 mm ( tabella 4 )  . 
tre / 8 vene soprannumerarie a destra presentano branching . in nessun caso allinterno dellauricola sono stati riconosciuti trombi . pazienti con fa parossistica nei 43 / 75 pz con fa parossistica le vp riconosciute allesame tcmd sono 160 , di cui 88 destre e 72 sinistre . 
a sinistra , 14 / 72 vp sono tronchi comuni di cui 2 lunghi . in 27 / 43 pz il quadro anatomico tipico ( 2 vp destre e sinistre : 62 , 7% ) ed atipico nei restanti 16 pazienti ( 37 , 3% )  . tra le varianti anatomiche la pi frequente rappresentata da 2 vp destre - tronco comune sinistro ( 12 / 43 : 27 , 9% ) ; in 2 / 43 pz ( 4 , 6% ) si rilevano 3 vp destre - tronco comune sinistro mentre ciascuna delle varianti 3 vp destre - 2 vp sinistre e tronco comune destro - 2 vp sinistre sono presenti in 1 / 43 pz ( 2 , 4% )  . 
in nessun caso si osservata la variante 3 vp destre - 3 sinistre ( tabella 2 )  . presentano branching 40 / 42 vp inferiori destre ( 95 , 2% ) , 30 / 42 vp superiori destre ( 71 , 4% ) , 4 / 29 vp superiori sinistre ( 13 , 7% ) e solo una delle 29 vp inferiori sinistre ( 3 , 4% )  . delle 3 vp soprannumerarie riconosciute a destra 2 presentano branching . 
i 14 tronchi comuni a sinistra non presentano branching mentre si osserva nellunico tronco comune destro ( tabella 3 )  . nei 43 pz langolo trans - settale compreso tra 43 e 80 ( valore medio di 646 , 8 e mediano di 65 )  . 
lasse atriale antero - posteriore medio di 38 , 8 mm , mediano di 40 mm ; lasse latero - laterale rispettivamente di 70 , 3 e 70 mm ; infine , lasse cranio - caudale rispettivamente di 61 , 4 e 61 , 5 mm ( tabella 4 )  . 
ostio della vp superiore ( spv ) , ostio della vp inferiore ( ipv ) , ridge ( linea tratteggiata )  . radiol med ( 2008 ) 113 : 779798 pazienti con fa cronica nei 32 / 75 pz con fa cronica le vp riconosciute allesame tcmd sono 126 , di cui 69 destre e 57 sinistre . 
tra le varianti anatomiche la pi frequente rappresentata da 2 vp destre - tronco comune sinistro ( 8 / 32 : 25% ) ; in 4 / 32 pz ( 12 , 5% ) si rilevano 3 vp destre - 2 vp sinistre , mentre un solo pazienti ( 3 , 1% ) presenta il quadro 3 vp destre - 3 sinistre . 
lasse antero - posteriore medio di 45 , 9 mm , mediano di 45 , 5 mm ; lasse latero - laterale rispettivamente di 77 , 5 e 77 , 5 mm ; infine , lasse craniocaudale rispettivamente di 63 , 5 e 63 , 2 mm ( tabella 4 )  . 
rispetto agli osti delle vp sinistre , lorifizio dellauricola risulta in posizione alta in 29 / 32 pz ( 90 , 6% ) , intermedia in 2 / 32 pz ( 6 , 2% ) e bassa in 1 / 32 pz ( 3 , 1% )  . aspetti dosimetrici come sopra menzionato , in 63 / 75 pz lindagine tcmd stata effettuata con gating cardiaco e modulazione della dose ( cardiac - dose ecg modulation ) in telediastole ( 70%80% dellintervallo rr dellecg ) , fase del ciclo utilizzata per la ricostruzione retrospettiva delle immagini . tale algoritmo si basa sulla riduzione del milliamperaggio ( fino al 80% ) durante le fasi del ciclo cardiaco che non vengono utilizzate per la successiva ricostruzione retrospettiva . 
in un sottogruppo di 12 pz , si stimata la percentuale di riduzione della dose , espressa in termini di dlp ( dose - lenght product ) e ctdi ( computed tomography dose index ) , in rapporto ai 12 pazienti in cui non stato possibile utilizzare il gating e , pertanto , la modulazione della dose : la riduzione media ottenuta per il dlp e il ctdi stata rispettivamente del 30 , 3% e del 30 , 7% ( range dlp : 9 , 3%45 , 9% ; range ctdi 10 , 1%46 , 7% )  . 
anche se in termini assoluti la dose erogata maggiore nei pz con bassa frequenza cardiaca , in relazione a una riduzione del pitch che permette la cardiosincronizzazione , si osservato che la diminuzione di dose percentualmente maggiore proprio in questi pz rispetto a quelli con elevata frequenza : tafig . 
in the upper row , the ridge ( dotted line ) separates the two left pv ( superior spv ; inferior ipv ) from the orifice of the appendage ( a )  . 
11 rappresentazione schematica della visione endoscopica e corrispondente vista endoscopica ( voyager ) del lato sinistro dellatrio : nella riga superiore , il ridge ( linea tratteggiata ) separa le 2 vp di sinistra ( superiore : spv ; inferiore : ipv ) dallorifizio dellauricola ( a )  . 
si noti la posizione pi profonda della sella interposta tra le branche che confluiscono nel ct , che in questo caso non origina dal bordo del ridge . anteroposterior atrial axis was 38.8 mm ( median 40 mm ) ; the mean lateral axis was 70.3 mm ( median 70 mm ) ; the mean craniocaudal axis was 61.4 mm ( median 61.5 mm ) ( table 4 )  . 
the most frequent anatomical variation was two right pv - left common trunk ( 8 / 32 ; 25% ) ; in 4 / 32 pa792 radiol med ( 2008 ) 113 : 779798 tients ( 12.5% ) , we identified three right pv - two left pv , whereas only one patient ( 3.1% ) showed the pattern three right pv - three left pv . 
of the five supernumerary right pv , one had branching , which was absent in the only left supernumerary pv and in the eight left common trunks ( table 3 )  . 
even though in absolute terms patients with low heart receive a greater dose because of the low pitch that allows cardiac synchronisation , dose reduction rates were found to be higher in these patients compared with those with high heart rate . 
this is explained by the longer exposure and hence the longer time available for dose modulation . discussion the literature contains numerous studies describing the extreme anatomical variability of the la - pv complex [ 2332 , 3541 ]  . 
in our series , atypical patterns were seen in as many as 38.7% of patients , a result similar to that reported by previous authors [ 38 ] and slightly lower than found in two recent papers [ 39 , 40 ]  . 
nella casistica personale ben il 38 , 7% dei pazienti presenta un pattern anatomico atipico , in accordo con quanto descritto da altri autori [ 38 ] e in percentuale lievemente inferiore rispetto a quanto segnalato in due recenti lavori [ 39 , 40 ]  . 
nelle forme di fa parossistica e cronica le varianti anatomiche incidono rispettivamente per il 37 , 3% e il 40 , 7% dei pz , senza differenze statisticamente significative sia riguardo al loro numero complessivo che ai singoli quadri . 
a questo proposito , va comunque rilevato come la variante 3 vp destre - 2 vp sinistre sia nella nostra casistica ampiamente prevalente ( 4 versus 1 ) nei pz affetti da fa cronica rispetto a quelli con fa parossistica , anche in questo caso senza raggiungere la significativit statistica ( p = 0 , 2 )  . 
intorno alla vii settimana di gestazione , la vp primitiva si sviluppa come unescrescenza della parete atriale dorsale [ 4143 ]  . quando la camera cardiaca si ingrandisce la vp primitiva e i suoi rami principali vengono gradualmente incorporati nella parete dellas con la conseguente formazione di 4 vp , 2 per ciascun lato . 
le vp soprannumerarie sono molto frequenti a destra e rarissime a sinistra [ 44 , 45 ] mentre si osserva una situazione opposta per quanto riguarda i tronchi comuni [ 37 ] , che rappresentano la variante anatomica pi frequente in assoluto ( 12%25% ) e il cui riscontro pressoch esclusivo sul lato sinistro . 
la sovrastima del numero dei tronchi comuni a destra in questo lavoro rispetto a tutti gli altri contributi della letteratura da imputare alla modalit di classificazione delle vp che si basa sullanalisi della giunzione venoatriale mediante mpr - mip sul piano assiale , con slab di spessore considerevole . 
ci fa s che le due vp superiore e inferiore a destra giacciano apparentemente nello stesso piano e che confluiscano in un tronco comune a una distanza minima ( 5 mm ) dal bordo atriale . 
 [ 27 ] identifica solo nel 2% dei 201 pazienti studiati un tronco coradiol med ( 2008 ) 113 : 779798 ther overall number or prevalence of a single pattern . 
as the heart chamber enlarges , the primitive pv and its main branches are gradually incorporated into the left atrial wall with the subsequent formation of four pv , two on each side . 
supernumerary pv are very frequent on the right side and very rare on the left [ 44 , 45 ] , whereas the reverse is true for common trunks [ 37 ] , which constitute the most common anatomical variant in absolute terms ( 12%25% ) and one that is exclusively encountered on the left side . these data were confirmed in our personal series and conflict partly with jongbloed et al.s finding [ 31 ] of right - sided common trunks in 39% . 
overestimation of the number of right common trunks in jongbloed et al.s report compared with all other published studies can be ascribed to the fact that the authors classified pv by analysing the venoatrial junction on axial mpr - mip images with considerable slab thickness . 
this causes the right superior and inferior pv to appear to be lying in the same plane and converging into a common trunk at a minimum distance ( 5 mm ) from the atrial border . 
in our experience , as in numerous previous reports [ 27 , 29 , 31 , 3840 ] , supernumerary pv were almost exclusively identified on the right side . in particular , only one patient in our series showed a left supernumerary pv , in agreement with jongbloed et al . 
the number of pv would instead appear to be more dependent on asymmetrical incorporation between the two sides greater on the right side and lesser on the left with the resulting presence of supernumerary veins on the right and common trunks on the le as reported by previous authors [ 23 , 3840 ] , our experience confirmed that the voyager technique is the most appropriate technique for establishing the number of pv . 
this is particularly true for the left side : on the volume - rendered epicardial views , it may be impossible to distinguish a common trunk from two separate pv , above all when the veins drain into the atrium alongside each other , as occurs in the majority of cases . 
nello stesso tempo nella nostra esperienza e in numerosi altri lavori della letteratura [ 27 , 29 , 31 , 3840 ] le vp soprannumerarie sono un rilievo pressoch esclusivo del lato destro : in particolare , nella casistica personale solo 1 pazienti presenta una vp soprannumeraria sinistra , analogamente a quanto segnalato da jongbloed et al . 
come gi dimostrato da alcuni autori [ 23 , 3840 ] anche nellesperienza personale il voyager risulta la modalit in assoluto pi idonea per stabilire il reale numero di vp . 
ci particolarmente valido sul lato sinistro : nella vista epicardica garantita dal vr non sempre possibile differenziare un tronco comune da due distinte vp soprattutto quando , come si osserva nella maggior parte dei casi , tali vene sboccano in adiacenza . anche le mpr / mip e le immagini native non sono particolarmente utili per quantificare il reale numero di vp . 
le vp sinistre sono separate dallorifizio dellauricola da una sottile cresta di tessuto miocardico , denominata ridge , che riveste il legamento di marshall , residuo della vena cardinale comune di sinistra [ 25 , 49 ]  . 
nel caso in cui il tronco comune sia particolarmente lungo anche le mpr / mip sui piani para - coronali e il vr possono far riconoscere agevolmente la variante anatomica , che condiziona la strategia ablativa : in presenza di un tronco i punti di ablazione devono interessare solo il margine dellampio ostio comune , evitando accuratamente di coinvolgere gli osti delle branche di confluenza , ci che esporrebbe il paziente al rischio di stenosi venosa . 
infatti , lapplicazione delle onde di radiofrequenza o di altri tipi di energia direttamente nel lume del vaso pu determinarne la contrazione e la proliferazione della lamina elastica che , in associazione ad un processo di flogosi cronica perivasale , causano una stenosi progressiva , che pu arrivare fino allocclusione completa con conseguente comparsa di sintomi di ipertensione polmonare segmentale , talora molto gravi e potenzialmente fatali [ 22 , 24 ]  . 794 radiol med ( 2008 ) 113 : 779798 tual number of pv . 
the left pv are separated from the appendage orifice by a thin ridge of myocardial tissue that covers the marshall ligament , a remnant of the left common cardinal vein [ 25 , 49 ]  . 
if the common trunk is particularly long , the anatomical variation can also be identified on the paracoronal mpr / mip and vr images , with an impact on the ablation strategy . 
in the presence of a trunk , the ablation points must be applied only around the border of the wide common ostium , taking care to avoid the ostia of the confluent branches , as this would expose the patient to a risk of venous stasis . 
in fact , application of radiofrequency waves or other energy sources directly inside the lumen may lead to contraction and proliferation of the elastic lamina , which associated with chronic perivascular inflammation can progress to complete occlusion with severe and potentially life - threatening symptoms of segmental pulmonary hypertension [ 22 , 24 ]  . voyager images are also the best for determining the presence of supernumerary veins [ 23 ] , potential af triggers , even though both vr and paracoronal mpr / mip are also informative in this respect . 
furthermore , to correctly plan the ablation procedure and reduce complications ( stenosis ) , the supernumerary veins must be accurately differentiated from preostial branching , venous branches joining the terminal vein within 510 mm of its ostium into the la [ 23 , 2527 , 30 , 50 ]  . 
in the first case , even the small ostia of the supernumerary veins have to be included in the ablation field , whereas in the second , the converging pv branches need to carefully avoided to prevent stenosis . 
several authors [ 17 , 26 ] have hypothesised that the presence of early branching may protect against af , as it may prevent the extension of myocardial sleeves into the pv lumen . the transseptal angle is strictly related to la orientation . advance knowledge of this angle facilitates transseptal puncture , reducing the risk of perforating adjacent cardioil voyager rappresenta la modalit di visualizzazione migliore anche per determinare la presenza di eventuali vene soprannumerarie [ 23 ] , potenziali trigger della fa , bench in tal senso sia il vr che le mpr / mip sui piani para - coronali forniscano buone informazioni . 
inoltre , ai fini di una corretta pianificazione della procedura di ablazione e di una riduzione delle complicanze ( stenosi ) , le vene soprannumerarie devono essere accuratamente differenziate dalla presenza del branching pre - ostiale , rami venosi che confluiscono nella vena terminale a meno di 510 mm dallo sbocco di questultima nellas [ 23 , 2527 , 30 , 50 ]  . 
come pocanzi accennato , la distinzione fra vene soprannumerarie e branching precoce ha una grande rilevanza per lelettrofisiologo : nel primo caso egli dovr comprendere nel campo di ablazione anche i piccoli osti dei vasi soprannumerari mentre nel secondo dovr evitare accuratamente di intervenire su rami di confluenza delle vp , per i quali il rischio di stenosi maggiore . 
alcuni autori [ 17 , 26 ] hanno ipotizzato che la presenza di un branching precoce possa rappresentare un fattore protettivo nei confronti dellinsorgenza di fa poich impedirebbe lestensione delle lingue di tessuto miocardico anomalo nel lume delle vp . langolo trans - settale strettamente vincolato allorientamento del as : conoscere in anticipo tale angolo , facilita la manovra di puntura del setto e , nel contempo , riduce il rischio di perforazione delle strutture cardio - vascolari adiacenti , complicanza peraltro segnalata raramente [ 24 , 29 , 51 ]  . 
si segnala tuttavia il riscontro di rari casi di angolo trans - settale molto lontani dai valori medi nei pazienti con scoliosi del rachide dorsale nei quali il rischio di complicanze maggiore . la misura degli assi atriali ha il precipuo scopo di fornire allelettrofisiologo una stima delle dimensioni e della morfologia della camera atriale . 
dallanalisi statistica di confronto dellincidenza delle diverse varianti anatomiche del complesso as - vp nei gruppi di pazienti con fa paradiol med ( 2008 ) 113 : 779798 vascular structures , a rare complication of the procedure [ 24 , 29 , 51 ]  . 
there were , however , sporadic cases of transseptal angles strongly deviating from the mean in patients with thoracic scoliosis , whose risk of complications is greater . measurement of the atrial axes is chiefly aimed at providing the electrophysiologist with an estimate of the dimensions and morphology of the atrial chamber . 
la enlargement appears to be ascribable to an axial dilatation of the atrial walls ( laterolateral and anteroposterior axes ) , whereas longitudinal extension remains unchanged ( craniocaudal axis ) as a result of the greater physical constraints of regional anatomical structures : the pulmonary arteries cranially and the diaphragmatic dome caudally . knowledge of the appendage orifice position relative to the left pv ostia is required by the electrophysiologist to limit complications ( perforation ) and to better understand the local anatomical situation , which may sometimes be particularly complex . 
moreover , several reports in the literature have noted that pv stenosis , the most frequent complication of ablation , has a higher incidence in left pv , which are more difficult to reach owing to their spatial orientation and relationship with the appendage [ 29 , 5355 ]  . 
lunica eccezione riguarda solo la misura degli assi latero - laterale e antero - posteriore dellas che risultano superiori ( p < 0 , 001 ) rispettivamente del 10% e del 18% nei pazienti con fa cronica . 
tale incremento dimensionale sembra ascrivibile ad una dilatazione sul piano assiale delle pareti atriali ( assi latero - laterale e antero - posteriore ) mentre rimane invariata lestensione longitudinale ( asse cranio - caudale ) della camera cardiaca , ci che impedito dai maggiori vincoli opposti dallanatomia regionale : cranialmente la presenza delle arterie polmonari e caudalmente della cupola diaframmatica . la valutazione della posizione dellorifizio dellauricola rispetto agli osti delle vp di sinistra informazione che lelettrofisiologo richiede allimaging tcmd con il duplice scopo di ridurre le complicanze ( perforazione ) e per meglio comprendere la situazione anatomica locale , che talora pu risultare particolarmente complessa . 
inoltre , numerosi contributi della letteratura segnalano come la stenosi delle vp , la complicanza pi frequente della ablazione , abbia maggiore incidenza per quanto riguarda le vp sinistre , che sono pi difficili da raggiungere durante la procedura interventistica , in relazione al loro orientamento spaziale e , soprattutto , ai rapporti con lauricola [ 29 , 5355 ]  . 
nella popolazione studiata la maggior parte delle auricole ha un orifizio che giace in posizione alta , a livello del piano passante per lostio della vp superiore ( 85 , 1% ) mentre pi raramente intermedio ( tra gli osti delle due vp : 12 , 1% ) o basso ( allaltezza dellostio della vp inferiore : 2 , 8% )  . sia il voyager che le mpr / mip sui piani para - sagittali sono in grado di definire con precisione la morfologia e i diametri degli osti delle vp : a destra le vene hanno un aspetto pi rotondeggiante mentre a sinistra pi ovalare [ 24 , 27 , 31 , 32 , 3840 ]  . 
linformazione sulle dimensioni degli osti potrebbe essere utile nei casi in cui vengano utilizzati cateteri di forma circolare finalizzati allablazione 796 radiol med ( 2008 ) 113 : 779798 volving ablation lines external to the pv ostium [ 18 ]  . 
information about ostial diameters could be useful in a segmental approach , in which circular catheters are used to ablate the pv ostium [ 15 ]  . conclusioni dellostio della vp seguendo un approccio di tipo segmentale [ 15 ]  . conclusions our study confirms the common anatomical variability of the la - pv complex and the fundamental role of a preablation mdct study of the region . 
the commercial availability and widespread use of software allowing the fusion of mdct images with electroanatomical maps obtained in electrophysiology laboratories enables the cardiologist to perform the ablation procedure while navigating within 3d on - line images rather than having to rely on a series of offline anatomical reconstructions . 
only by integrating these two different professional competences diagnostic and clinical will it be possible to improve the success of the interventional ablation procedure while reducing fluoroscopy time and the possible complications of ablation . lesperienza personale conferma la frequente variabilit anatomica del complesso as - vp e il ruolo fondamentale dello studio pre - ablazione di questa regione con tcmd . la recente commercializzazione e diffusione di software di fusione di immagini tcmd con le mappe elettroanatomiche acquisite nei laboratori di elettrofisiologia consente al cardiologo di effettuare la procedura di ablazione non pi basandosi solo su una serie di ricostruzioni anatomiche off - line ma navigando allinterno delle immagini 3d on - line , durante la procedura stessa . 
ciononostante , il ruolo del radiologo rimane fondamentale sia per ottimizzare gli aspetti tecnici dellindagine tcmd che , soprattutto , per far comprendere allelettrofisiologo la realt di questa complessa regione anatomica . 
seven out of 45 patients , five of whom were women treated with the longo technique and two men with the starr technique , developed rectal diverticula . one diverticulum was located on the left lateral rectal wall , four on the posterior wall and two on the anterior wall . 
di questi ( 5 in pazienti di sesso femminile e 2 in pazienti di sesso maschile ) 1 era localizzato a livello della parete laterale sinistra , 4 della parete posteriore e 2 di quella anteriore . 
con luso di suturatrici meccaniche endorettali possibile linstaurarsi di aree di debolezza focale della parete rettale , in corrispondenza della sutura chirurgica , che possono rappresentare punti di minor resistenza e quindi fattore predisponente allinsorgenza di un diverticolo rettale . keywords circular stapler defecography rectal diverticulum parole chiave suturatrice meccanica ( stapler ) defecografia diverticolo rettale 888 introduction colonic diverticula are acquired herniations of the mucosa and part of the submucosa through the muscularis propria . diverticular disease is very common in the western world . the two main factors contributing the development of diverticula are : ( 1 ) a pressure gradient between the bowel lumen and the mucosa ; ( 2 ) areas of relative weakness of the bowel wall . 
the colonic wall is weaker where the intramural vasa recta penetrate the submucosal layers , that is , on the side of both the mesocolic taenia and mesenteric taenia of the taenia libera and taenia omentalis . 
diverticula may , however , arise at points of focal weakness of the rectal wall due to congenital or acquired causes [ 13 ]  . we report seven cases of isolated diverticulum of the rectal wall seen on defaecography in patients undergoing follow - up functional imaging after surgery according to the longo and stapled transanal rectal resection ( starr ) techniques . 
the aim of this paper is to demonstrate that the use of mechanical circular staplers for the treatment of haemorrhoids ( longo ) or obstructed defaecation syndrome due to rectal prolapse ( starr ) may cause areas of relative focal weakness in the rectal wall and lead to development of rectal diverticula . 
of these , 45 were postoperative follow - up studies of patients who had been treated with the longo ( n = 13 ) and starr ( n = 32 ) techniques . 
on the basis of our protocol [ 13 ] , the examinations were performed after opacification of both the jejunoileal loops and the rectum , and in female patients , of the vagina and bladder also . 
rectal opacification was achieved with 200 ml of barium paste ( prontobario esofago , bracco ) , bladder opacification with 250 ml of 50% iodinated contrast in saline and vaginal opacification with 20 ml of a 1 : 1 solution of sonographic gel and iodinated contrast material . 
i due fattori fondamentali che contribuiscono allo sviluppo di diverticoli sono : ( 1 ) un gradiente pressorio tra il lume intestinale e la mucosa ; ( 2 ) aree di relativa debolezza della parete intestinale . 
la parete del colon pi debole laddove i vasi retti intramurali penetrano negli strati sottomucosi ovvero sia sul lato della tenia mesocolica sia su quello mesenteriale della tenia libera e della tenia omentale . 
il diverticolo appendicolare si riscontra nello 0 , 2%2% dei pazienti mentre il diverticolo rettale estremamente raro con una frequenza stimata inferiore allo 0 , 1% dei casi di diverticolosi colica . 
esso si pu formare in aree di debolezza focale della parete rettale dovute a cause congenite o acquisite [ 13 ]  . riportiamo il riscontro defecografico di 7 casi di diverticolo isolato della parete rettale in pazienti giunti alla nostra osservazione per il controllo funzionale degli esiti di interventi chirurgici di longo e di starr . 
scopo del nostro lavoro dimostrare che luso di suturatici meccaniche circolari ( stapler ) per il trattamento di patologia emorroidaria ( longo ) o di sindrome da ostruita defecazione sostenute da prolasso rettale e rettocele ( starr ) pu determinare la formazione di punti di relativa debolezza della parete rettale tali da consentire lemergenza di diverticoli . 
in base alla nostra procedura [ 13 ] gli esami sono stati effettuati previa opacizzazione sia delle anse digiunoileali che del retto e , nelle pazienti di sesso femminile , anche della vagina e della vescica . 
the patient , a woman who had undergone mucosal - haemorrhoidal prolapse surgery according to longo 4 months earlier , was referred for a double - contrast e per la vagina 20 ml di una soluzione di gel ecografico e contrasto iodato nella proporzione di 1 / 1 . 
lo studio defecografico e stato eseguito in 4 proiezioni ( riposo , contrazione , ponzamento e fase evacuativa ) con paziente il ll , ed integrato con videofluororegistrazione [ 4 , 5 ]  . la valutazione di pazienti gi sottoposti ad intervento chirurgico rientra nella procedura di controllo delle variazioni morfo - funzionali dellampolla rettale e di possibili complicanze dopo trattamento con tecnica longo / starr . 
altre due pazienti , entrambe di sesso femminile , erano state trattate con intervento di starr per sindrome da ostruita defecazione sostenuta da intussuscezione rettale ed associata a rettocele anteriore . 
la paziente , operata 4 mesi prima di prolassectomia muco - emorroidaria secondo longo , stata sottoposta ad esame radiografico del colon a doppio contrasto in seguito ad episodi ripetuti di diarrea alternata a stipsi con emissione di feci sottili . 
2 diverticolo posteriore a livello della giunzione ano - rettale ( freccia ) in paziente operato di longo . discussione barium enema because of alternating diarrhoea and constipation with the production of thin stools . 
supplementation of defaecography with an ap view is fundamental for detecting disorders affecting the lateral rectal walls , which might otherwise go undetected . il diverticolo rettale unevenienza molto rara .generalmente una malattia asintomatica il cui riscontro casuale . 
ristagno di feci nel diverticolo e decubito dello stesso sulla parete posteriore dellampolla . mento mucoso particolarmente lasso in modo da permettere alla mucosa di scorrere facilmente sulla muscolare . lesistenza di uno strato connettivo cellulare tra la muscolare e la mucosa rende possibile lasportazione isolata di questultima . i fattori che possono contribuire alla formazione di un diverticolo rettale non sono ancora completamente chiariti . 
in proiezione ap il diverticolo si rileva come piccola estroflessione gassosa ( freccia ) della parete laterale sinistra dellampolla rettale . dinal fibres are arranged in a uniform layer and not in three bands , as in the colon . 
the existence of a layer of cellular connective tissue between the muscularis and the mucosa makes it possible to remove the mucosa separately . although the factors contributing to the development of a rectal diverticulum have not been completely elucidated , the presence of areas of focal weakness in the rectal wall due to congenital or acquired causes is known to predispose to the condition . 
typically , they are located along the lateral walls of the rectum , as the longitudinal layer tends to be thicker at anterior and posterior locations compared with lateral locations [ 911 ]  . 
complications associated with rectal diverticula include diverticulitis with perforation and abscess formation , rectal prolapse due to inverted rectal diverticulum , postinflammatory rectal stenosis , rectovesical fistula and faecal impaction in the diverticulum . for several years now , the use of semicircular or circular mechanical suturing devices ( staplers ) has become common te o acquisite . 
le cause acquisite includono il rilassamento del setto retto - vaginale , limpatto fecale ricorrente , con aumento di pressione e distensione del retto , il trauma pelvico ed infezioni che determinino debolezza della parete rettale . 
le complicanze associate al diverticolo rettale possono includere la diverticolite con perforazione e formazione di ascessi , il prolasso rettale da diverticolo rettale invertito , la stenosi post - infiammatoria del retto , la fistola retto - vescicale e la formazione di fecalomi nel diverticolo . da molti anni si andato affermando luso di suturatici meccaniche semicircolari o circolari sia per il trattamento della malattia emorroidaria ( prolassectomia muco - emorroidaria secondo longo ) , sia nelle sindromi da ostruita defecazione sorrette da prolasso mucoso o intussuscezione associati o meno a rettocele ( stapled transanal rectal resection - starr )  . 
la tecnica di prolassectomia mucoemorroidaria secondo longo , anche detta anopessia circolare o mucosectomia circonferenziale , consiste nella resezione della mucosa prolassata e nella legatura dei peduncoli emorroidari interni [ 12 , 13 ]  . 
lintera procedura radiol med ( 2008 ) 113 : 887894 for treating both haemorrhoidal disease ( mucosal - haemorrhoidal prolapse surgery according to longo ) and obstructed defaecation syndrome caused by mucosal prolapse or intussusception with or without rectocele ( starr )  . 
mucosalhaemorrhoidal prolapse surgery according to longo , also known as circular anopexy or circumferential mucosectomy , consists of resecting the prolapsed mucosa and ligating the internal haemorrhoidal pedicles [ 12 , 13 ]  . 
the finding of muscular fibres at histological examination of the excised tissue is not uncommon [ 1922 ]  . in addition , in consideration of rate of failure of circular anopexy due to incomplete resection of prolapsed tissue , the starr technique has recently gained ground for treating haemorrhoids , especially when associated with rectal or rectoanal prolapse . 
the starr technique is thought to allow for a more complete resection of prolapsed tissue [ 2325 ]  . the technique , which is indicated for treating obstructed defaecation syndrome due to rectal mucosal prolapse or rectocele , involves a two - step resection first anterior then posterior of the distal rectum with the use of two staplers . 
in starr , the purse - string sutures , usually two or three on each side , must extend to the entire thickness of the wall . resection of the distal rectum is therefore total and extends to the circular musculature , with the formation of a fibrous ring of sutures , which tends to loosen with time [ 26 , 27 ]  . for either technique , it is thus possible to hypothesise the development of areas of focal weakness of the rectal wall as a result of tears or the absence of the muscular lining , which may constitute points of least resistance and therefore become a predisposing factor for the development of rectal diverticula . 
 viene eseguita allinterno della zona non sensoriale del retto , sopra la linea dentata , utilizzando una suturatrice meccanica circolare ( stapler ) che consente di realizzare una mucosectomia con sutura sterile muco - mucosa . 
non infrequente il riscontro di fibre muscolari allanalisi istologica dei segmenti mucosi asportati [ 1922 ]  . recentemente inoltre , in considerazione della percentuale di insuccessi dellintervento di anopessia con stapled legati allincompleta resezione del tessuto prolassato , si sta affermando lutilizzo della tecnica starr anche per il trattamento della malattia emorroidaria specie se associata a prolasso rettale o retto - anale . 
questa tecnica infatti , indicata nel trattamento delle sindromi da ostruita defecazione sostenute da prolasso mucoso rettale e / o rettocele , consiste nella resezione in due tempi , prima anteriormente , poi posteriormente , del retto distale con lutilizzo di due stapled . 
si determina quindi una resezione totale del retto distale che comprende la muscolatura circolare , con formazione di un anello fibroso di sutura che col tempo tende a rilasciarsi [ 26 , 27 ]  . con entrambe queste tecniche quindi , possibile ipotizzare linstaurarsi di aree di debolezza focale della parete rettale , per lacerazione o assenza del rivestimento muscolare , che possono rappresentare punti di minor resistenza della parete e quindi fattore predisponente allinsorgenza di un diverticolo rettale . 
moreover , it should be kept in mind that iatrogenic diverticula of the lateral rectal walls may be missed on defaecographic examinations performed in ll projections and that an ap view should always be obtained to complete the examination . esiste un solo caso riportato in letteratura di diverticolo su emorroidectomia secondo longo [ 28 ]  . 
giovanni calibita , fatebenefratelli isola tiberina , via di ponte quattro capi 39 , 00186 roma , italy 2mikai s.p.a. , genova , italy 3dipartimento di fisiologia umana e farmacologica v . 
the aim of this study was to test the potential application of a new nonmagnetic device capable of diagnostically evaluating stress of the knee joint during magnetic resonance imaging ( mri ) investigation . 
the preliminary data regarding this new mr method , performed using the knee loader prototype , demonstrate that it is possible to obtain functional images of the knee comparable with those obtained by traditional radiological techniques . 
sono stati eseguiti 20 esami rm in volontari sani , in condizioni di base e con limpiego di una forza di entit nota ( in kg ) sui diversi compartimenti articolari . 
saranno necessari ulteriori studi per essere in grado di correlare dati anatomici , patologici e funzionali delle strutture capsulo - legamentose di ginocchio , utilizzando il prototipo knee loader in studio . 
 keywords knee mri knee instability parole chiave rm di ginocchio instabilit di ginocchio 906 introduction all central and peripheral traumatic lesions to the structures responsible for knee stability cause biomechanical alterations of the joint structures and how they interact . 
it is of paramount importance to understand how , and to what extent , these events affect the joint to be able to choose a correct therapeutic strategy , whether surgical or conservative . numerous biomechanical studies of the knee have been performed in vitro [ 13 ] or in vivo in an attempt to better define one of the most complex systems of joint kinematics , with the aid of orthopaedic and radiographic devices [ 46 ]  . in fact , conventional radiography has always been considered the gold standard for demonstrating subluxation or pathological deviation of the tibiofemoral and patellofemoral relationships , by means of either mechanical stress or muscular contraction [ 711 ]  . 
however , this method does have some limitations . on the other hand , magnetic resonance imaging ( mri ) is extremely accurate in diagnosing capsular or ligament lesions of the knee in baseline conditions but is extremely limited by its inability to perform functional investigations , apart from assessing the patellofemoral joint . 
these limitations derive from its constructional features that impose the supine position . only recently has it become possible to evaluate joint function by means of mri - compatible devices that can be put into use while the patient is on the mri bed . 
mri studies with 3d reconstructed images , capable of supplying data required for evaluating both patellofemoral and tibiofemoral joint congruence during various degrees of flexion , have been described in the literature [ 1214 ]  . 
 for biomechanical evaluation of the tibiofemoral joint , we were given the opportunity to test the prototype of a nonmagnetic device suitable for assessing knee stress while the patient is lying on the bed of the mri scanner ( knee loader , mikai , genova , italy )  . 
the working principle of this device is based on a procedure similar to the telos radiological test [ 15 ] in which a known force is applied to a specific sector of the joint with the patient in a supine or lateral position . 
we decided to use this device to study the knee in conditions of stress : the technique used is described here , as are our preliminary results . materials and methods radiol med ( 2008 ) 113 : 905914 introduzione tutte le lesioni traumatiche periferiche o centrali che coinvolgono le componenti di stabilizzazione del ginocchio determinano alterazioni biomeccaniche dei rapporti articolari . 
la dimostrazione degli effetti di tali eventi e la loro entit importante al fine di pianificare correttamente lintervento chirurgico , oppure un trattamento conservativo . in letteratura sono numerosi gli studi di biomeccanica di ginocchio in vitro [ 13 ] ed in vivo , mediante apparecchiature ortopediche e radiografiche [ 46 ] , per riuscire a definire meglio uno dei pi complessi sistemi di cinematica articolare . 
la radiologia tradizionale sempre stata la metodica di riferimento per dimostrare , sia mediante radiogrammi in carico , che con stress meccanici o da contrazione muscolare , sub - lussazioni o deviazioni patologiche dei rapporti femoro - tibiali e femoro - rotulei [ 711 ]  . 
tuttavia lesame radiografico presenta alcune limitazioni . la rm al contrario ha unelevatissima accuratezza diagnostica nelle lesioni capsulo - legamentose del ginocchio in condizioni di base , mentre ha sempre avuto come grande limite limpossibilit di eseguire studi funzionali , ad esclusione degli studio sullarticolazione femoro - rotulea . 
tali limiti sono secondari alle caratteristiche costruttive e lobbligata posizione supina . solo recentemente stato possibile studiare la funzionalit articolare con apparecchiature mri compatibili , utilizzabili direttamente sul lettino della risonanza . 
sono presenti in letteratura studi mri che , mediante ricostruzioni 3d , hanno potuto fornire dati per la valutazione della congruenza articolare nel movimento a vari gradi di flessione sia per lo studio della femoro - rotulea , che per i rapporti femoro - tibiali [ 1214 ]  . 
 per la valutazione biomeccanica dei rapporti femoro - tibiali abbiamo avuto a disposizione il prototipo di un apparecchio amagnetico idoneo allo studio in stress del ginocchio direttamente sul tavolo dellapparecchio di rm ( knee loader , mikai , genova , italia )  . 
il principio di funzionamento si basa su una procedura simile al test radiologico del telos [ 15 ] con lapplicazione di una forza di intensit nota , a livello di un preciso settore dellarticolazione , a paziente supino ovvero in appoggio sul fianco destro o sinistro . 
presentiamo in questo lavoro i nostri dati preliminari . the prototype knee loader was built along the lines of the axial loader already in use for the vertebral column , with the aim of reproducing the modifications to which the joint materiali e metodi il prototipo knee loader stato realizzato sfruttando i radiol med ( 2008 ) 113 : 905914 is subjected during the physiological load - bearing that occurs with daily activities . 
the device generates an amount of force measured in kilograms that can be applied to the tibia either anteroposteriorly or posteroanteriorly : force is applied to the rim of the femorotibial joint so that a varus or valgus moment is produced . 
the device does not interfere whatsoever with the magnetic field of the mri . in light of the published data [ 15 ] , we decided to apply a force of 25 kg , equal to 245 , 25n , in all patients to evaluate varus - valgus stress and to induce anterior and posterior tibial translation . 
for anterior tibial principi dellaxial loader gi in uso sul rachide , al fine di riprodurre modificazioni articolari durante le fisiologiche condizioni di carico a cui sottoposto il paziente nelle normali attivit . 
lapparecchio genera una forza misurabile in kg , che pu essere applicata sulla tibia in senso antero - posteriore / postero - anteriore , ovvero sulla rima articolare femoro - tibiale per produrre uno stress con direzione in varo o in valgo . 
lapparecchio non costituisce nessuna interferenza per il campo magnetico di base . in considerazione dei dati presenti in letteratura [ 15 ] , stata scelto di applicare a tutti i pazienti una forza di entit nota di 25 kg , equivalente a 245 , 25 n , per lo stress in varovalgo e per linduzione della traslazione tibiale anteriore e posteriore . 
knee loader with application of resistance points posteriorly to the distal femur and above the tibial - tarsal joint : the piston generates a tibial translation force with an anteroposterior vector . 
the force vector applied to the anterior tibial rim was directed so that it did not reach the anterior tibial tuberosity , the site of insertion of the patellar tendon . 
in fact , when the latter event occurs , the force vector breaks down into the vectors deriving from it and therefore becomes lost along the tendineal structures of the anterior compartment . 
the patients position varied according to the anatomical area being assessed : supine when stress evaluation involved the medial and lateral compartments ( along the coronal plane ) , lying on one side for assessment of tibial translation ( along the sagittal plane )  . 
the mri scanner was a philips intera 1.5 - t with a q - body coil . the study was performed in two phases : at rest and during dynamic stress . 
during the rest phase , images were acquired in axial , sagittal and coronal planes , with t1and t2 - weighted spin echo ( se ) , fast field echo ( ffe ) t2 and t2 - weighted fat - suppression sequences . 
after the rest phase had been completed , dynamic images were obtained about 2 min after a force had been applied to allow neuromuscular and capsularligament adaptation of the knee to the modified joint conditions . 
infatti , in questultimo caso il vettore di forza si scomporrebbe nei vettori da essa derivabili e quindi si dissiperebbe in parte lungo le strutture tendinee del compartimento anteriore . sono stati studiati 20 volontari sani : 16 maschi e 4 femmine , di et compresa tra 22 e 35 anni ( media di 27 , 5 anni ) per la messa a punto della metodica e delle tecniche di misurazione . 
la posizione del paziente variava in relazione al distretto anatomico da valutare : supino per lo stress sui compartimenti mediale e laterale , lungo il piano coronale , mentre era sul fianco del lato in esame per la valutazione dellentit della traslazione tibiale , lungo il piano sagittale . larto stato posizionato in estensione a paziente supino , mentre se il paziente era in decubito sul fianco larto veniva posizionato a pochi gradi di flessione , tra 20 e 30 . 
nella fase di riposo sono state acquisite immagini su piani assiali , sagittali e coronali , con scansioni se t1 e t2 pesate , ffe t2 e fat suppression t2 , a paziente supino per la valutazione varo - valgo , ed in decubito laterale per la valutazione della traslazione tibiale anteriore o posteriore , su entrambe le ginocchia del paziente . 
successivamente alla fase di riposo stata eseguita lacquisizione dinamica circa 2 minuti dopo lapplicazione della forza , per permettere ladattamento neuro - muscolare e capsulo - legamentoso del ginocchio alla nuova condizione articolare . 
for the anterior drawer test , the normal range is 03 mm ; for the posterior drawer test , it is 05 mm . evaluation of varus - valgus loading tibiofemoral modifications involving the medial segment were obtained by applying valgus loading . 
il range fisiologico 910 radiol med ( 2008 ) 113 : 905914 compreso tra 0 e 3 mm per il cassetto anteriore , mentre per il cassetto posteriore compreso tra 0 e 5 mm . valutazione della prova di varo - valgo le modificazioni femoro - tibiali del compartimento mediale sono state ottenute con lapplicazione di uno stress in valgo , mentre la forza applicata medialmente per ottenere unapertura del compartimento laterale al fine di studiare lo stress in varo . 
apertura dellemirima articolare mediale dopo uno stress in valgo . lapiezza dello spazio articolare dopo stress si misura considerando la distanza tra le tangenti condiloidea e tibiale sul compartimento mediale . risultati applied medially to achieve opening of the lateral compartment . 
the amount of widening of the articular rim resulting from varus - valgus stress is calculated with reference to the coronal plane passing through the midline of the tibial plate . the lines of reference considered were the bicondyloid tangent and the tangent of the tibial joint plate , whose extensions define the varus and valgus angulations . 
 varus stress in the two cases evaluated , the width of the lateral articular le principali strutture capsulo - legamentose si oppongono , come avviene in vivo nella deambulazione , nella corsa e nelle altre sollecitazioni meccaniche alla variazione eccessiva dei rapporti articolari femoro - tibiali per la corretta congruenza articolare . non vi sono in letteratura lavori di stress in rm mediante un compressore articolare amagnetico . 
6a , b sequenze se t1 pesate sul piano sagittale , in condizioni di base ( a ) ed dopo lesame funzionale ( b ) , dimostrano lentit del cassetto posteriore , che in questo caso e di 4 mm . 912 radiol med ( 2008 ) 113 : 905914 fig . 
notwithstanding their negative medical history , our healthy volunteers were firstly assessed by baseline mri to exclude the presence of occult or misdiagnosed traumatic lesions involving the central or peripheral knee structures . this is why the numerical values representing tibial translation or varus - valgus loading modifications presented a very limited range , owing to the fact that the structures of the central pivot and the angle points were anatomically normal . 
 in our study , forces applied at the level of the tibiofemoral joint modified articular relationships in all cases on both anteroposterior and posteroanterior planes , as well as in both mediolateral and lateromedial directions . 
the sagittal plane was found to be useful for biomechanical assessment of the pivot structures , whereas the coronal plane was superior for studying the medial collateral ligament posterointernal angle and the lateral capsular structures external angle . 
orientation of the various scans was strictly reproduced to ensure a valid comparative evaluation between rest and stress lontari sani sono stati esaminati preliminarmente con una rm di base per escludere ( oltre alla negativit anamnestica ) la presenza di lesioni occulte o misconosciute delle strutture centrali e periferiche del ginnocchio , di origine traumatica . 
per questo motivo i valori numerici delle traslazioni tibiali e delle modificazioni in varo - o valgo - stress hanno un range numerico molto ristretto per la completa integrit anatomica delle strutture del pivot centrale e dei punti dangolo . nel nostro studio lappicazione della forza a livello dellarticolazione femoro - tibiale produce in tutti i casi una modificazione dei rapporti articolari , sia su piano anteroposteriore o postero - anteriore che in senso medio - laterale e latero - mediale . 
il piano sagittale si dimostrato utile per la valutazione biomeccanica delle strutture del pivot , mentre il piano coronale risultato essere il migliore per lo studio del legamento collaterale mediale - punto dangolo postero - interno e delle strutture capsulari laterali - punto dangolo postero - esterno . 
sono stati scelti dei parametri anatomici oggettivi , per la misura precisa delle variazioni dei rapporti scheletrici : sul piano sagittale stato scelto lapice della linea di blumensaat e la proiezione ortogonale dello stesso sul piano tibiale . 
nel caso dello stress in varo e valgo stata considerata la tangente bicondiloidea rispetto al piano articolare corticale tibiale , presi su una scansione coronale mediana della tibia . le sequenze se t1 pesate sono risultate essere le migliori per ottenere una buona risoluzione anatomica e un radiol med ( 2008 ) 113 : 905914 fig . 
objective anatomical parameters were chosen to allow precise measurement of any variations in skeletal relationships : in the sagittal plane , the tip of blumensaats line and its orthogonal projection in the tibial plane were chosen . for varus and valgus stress , the bicondyloid tangent with respect to the tibial articular surface was chosen : evaluation was done with a medial coronal scan of the tibia . 
 on mri , t1 - weighted se sequences proved to be better for obtaining good anatomical resolution and a correct signalto - noise ratio in the shortest time possible , both before and after stress application . 
the force applied to the tibia to study the pivot structures produced tibial translation that was anterior for the anterior cruciate ligament ( acl ) and posterior for the posterior cruciate ligament ( pcl )  . 
besides a millimetric assessment of the varus and valgus moment , it was possible to evaluate differences in the angle delineated by the abovementioned markers , with an increase of this angle when force is applied . 
in all cases , measurements demonstrated that the prototype is capable of reproducing modifications of the tibiofemoral joint structures under conditions of stress in the same way as traditional stress radiography [ 1617 ]  . the advantages of using mri in young patients are the absence of ionising radiation and the greater anatomical accuracy in identifying injury before performing objective measurements . 
in all patients , tibiofemoral joint alterations demonstrated by the knee loader prototype in clinically stable patients corresponded with those described in the literature and were therefore considered within normal range [ 15 , 18 , 19 ]  . our preliminary results demonstrate that the information provided by integrating baseline mri findings with the functional data obtained using the knee loader could be useful corretto rapporto segnale - rumore , nel minor tempo possibile , sia prima che dopo lapplicazione dello stress . 
la forza applicata alla tibia per lo studio delle strutture del pivot ha generato una traslazione tibiale rispettivamente anteriore per il legamento crociato anteriore ( lca ) e posteriore per il legamento crociato posteriore ( lcp )  . 
oltre alle valutazioni in millimetri per quanto riguarda lo stress in varo e valgo si pu utilizzare anche una valutazione delle differenze angolari tra le linee di repere suddette con * incremento dellangolo allapplicazione della forza . 
questa esperienza pelimininare ha dimostrato che il sistema prototipo sperimentato in grado di riprodurre le stesse modificazioni dei rapporti articolari femoro - tibiali in condizioni di stress articolare analogamente a quanto avviene nella radiologia tradizionale [ 1617 ]  . 
 il vantaggio nellutilizzo dellapparecchiatura rm su pazienti giovani sicuramente lassenza di radiazioni ionzzanti e la maggiore accuratezza nellidentificazione anatomica della sede del danno , sui cui poi verrebbero eseguite misurazioni oggettive . 
grigenti springer - verlag italia ( 2008 ) isbn 978 - 88 - 470 - 0681 - 2 published online : 22 september 2008 springer - verlag 2008 the radiological report is a very important topic for all radiologists , and in this book , francesco schiavon , long respected in the radiological field , along with an expert in the communication sciences , presents a uniform methodology by which the radiological report can be most effectively written and communicated to the prescribing doctor . 
the book provides a complete overview of the reporting procedure and compares that procedure with the italian and european experience . the book is very well organised and is divided into several chapters discussing all the different aspects of the radiological reporting . 
a chapter dedicated to the principal report typologies proposes a classification of exam types : report are divided into initial exam , follow - up exam , additional exam and preventive exachapters 7 and 8 deal with the sensitivity and the psychology of the radiologist in reporting , while the following chapters are dedicated to the semiotics , the importance of the clinical descriptions and the rationale of reporting methodology . 
 noto da tempo limpegno di francesco schiavon per un argomento quello del referto molto caro a noi radiologi . in questo libro , egli , insieme allesperto di scienza della comunicazione , si propone di costruire e trasmettere una metodologia condivisa allo scopo di uniformare , nel modo migliore e il pi possibile , la refertazione ; lobiettivo posto risulta essere quello di comunicare efficacemente i risultati dellesame radiologico al medico prescrittore , consentendo di avere una visione panoramica completa e un confronto con lesperienza europea e nostra specifica . il libro ottimamente organizzato e suddiviso in capitoli che prendono in considerazione i diversi aspetti della refertazione radiologica . 
fa seguito un capitolo dedicato alle principali tipologie di referto , che vengono classificati in referti di esami iniziali , esami di followup , esami aggiuntivi e esami a scopo preventivo . 
i capitoli 7 e 8 trattano gli aspetti psicologici che coinvolgono il radiologo nella refertazione mentre il capitolo successivo dedicato alla semeiotica , alla importanza dei dati clinici e alla metodologia di refertazione . 
giovanni battista hospital , university of turin , turin , italy 3nuclear medicine unit , department of clinical physiopathology , university of florence , florence , italy correspondence to : e . 
fifty - six consecutive patients with increased serum prostate - specific antigen ( psa ) levels after radical prostatectomy were included in the study . none of them was receiving hormone treatment at the time of the examination or had been treated during the previous 6 months . 
all patients underwent whole - body 18f - choline pet imaging , and the pathological findings were compared with those of further imaging exams , biopsy and follow - up . 
in patients with biochemical relapse after radical treatment for prostate cancer , 18f - choline pet - ct represents a single step , whole - body , noninvasive study that allows disease detection and localisation . 
nei pazienti trattati radicalmente per carcinoma della prostata , in presenza di recidiva biochimica , lesame pet / tc total - body con 18f - colina rappresenta unindagine singola e non invasiva , che consente di identificare e localizzare la recidiva di 896 radiol med ( 2008 ) 113 : 895904 keywords 18f - choline pet - ct prostate cancer radical prostatectomy biochemical relapse psa malattia ; la sua percentuale di identificazione correlata con i livelli serici del psa . parole chiave 18f - colina pet / tc neoplasia prostatica prostatectomia radicale recidiva biochimica psa introduction introduzione prostate cancer is one of the most common neoplasms in men . 
in the european union , the incidence is 78.9 / 100 , 000 men per year , and the mortality rate is 30.6 / 100 , 000 men per year [ 1 ]  . 
at diagnosis , most patients present with locally confined disease ( t1 - 4 nxm0 ) , making radical prostatectomy or radiation therapy ( external beam or brachytherapy ) the primary therapeutic approach . 
however , tumour recurrence is frequent ( about 30% of cases [ 2 ] ) and presents with an increase in serum prostate - specific antigen ( psa ) levels . in particular , serum psa testing is considered the gold standard in the follow - up of patients after surgical treatment , and detectable psa levels are regarded as an indication of disease recurrence . 
once increased psa levels are detected , the key clinical consideration is to differentiate between local and systemic relapse to direct patients to appropriate treatment ( radiotherapy or salvage prostatectomy for local recurrence ; hormone therapy for systemic disease [ 3 ] )  . 
although the velocity of psa increase has been used to distinguish local recurrence from systemic disease [ 4 ] , psa is not a specific indicator , and multiple diagnostic tests are necessary to stage disease recurrence . positron emission tomography computed tomography ( pet - ct ) with 18f - fluorodeoxyglucose ( fdg ) is a noninvasive , whole - body imaging modality commonly used in the evaluation of many neoplasms . 
it allows disease staging at diagnosis , restaging in the case of suspected recurrence , evaluation of early and final response to the treatment and distinction between residual scar and recurrence [ 5 ]  . 
18f - choline ( fch ) is a new pet tracer that has recently been introduced to study prostate cancer [ 69 ] and its accuracy in detecting the primary neoplasm , metastases and recurrences has been evaluated by a number of preliminary studies [ 1013 ]  . 
biochemical analyses show that choline - kinase activity is substantially up - regulated in tumour cells [ 14 ]  . our study was conducted to evaluate the role of fchpet - ct in detecting and localising disease recurrence in a il carcinoma della prostata una delle neoplasie pi frequenti nelluomo . 
nellunione europea lincidenza di questo tumore di 78 , 9 / 100000 casi / anno , e la mortalit di 30 , 6 / 100000 casi / anno [ 1 ]  . 
al momento della diagnosi , la maggior parte dei pazienti presenta una neoplasia localmente confinata ( t1 - 4nxm0 ) e di conseguenza la prostatectomia radicale o la radioterapia ( per campi esterni o brachiterapia ) rappresentano lapproccio terapeutico delezione . 
ci nonostante , la recidiva della neoplasia frequente ( circa il 30% dei casi [ 2 ] ) e si presenta con un aumento dei livelli serici di antigene prostatico specifico ( psa )  . 
nei pazienti trattati con chirurgia radicale , il dosaggio serico del psa considerato il test di riferimento per il follow - up e livelli serici dosabili sono indicativi di recidiva di malattia . nel momento in cui si identifica un incremento del psa serico , il pi importante quesito diagnostico la stadiazione di malattia ed in particolare la distinzione tra recidiva locale e sistemica della stessa . 
il trattamento di queste due entit infatti completamente diverso : radioterapia o prostatectomia di salvataggio in caso di recidiva locale ; terapia ormonale in caso di ripresa sistemica di malattia [ 3 ]  . 
sebbene la velocit di incremento dei livelli serici del psa sia stata utilizzata da alcuni autori per distinguere la recidiva locale da quella sistemica [ 4 ] , in realt il psa non un indice specifico di malattia e sono pertanto necessarie pi indagini diagnostiche per una ristadiazione completa della stessa . la tomografia ad emissione di positroni / tomografia computerizzata ( pet / tc ) con 18f - desossi - glucosio ( fdg ) una metodica di imaging non invasiva e total - body utilizzata per lo studio di numerose neoplasie maligne che consente la stadiazione della malattia alla diagnosi , la ristadiazione in caso di recidiva , la valutazione della risposta precoce e finale al trattamento , la distinzione tra tessuto cicatriziale residuo e recidiva e cos via [ 5 ]  . 
la 18f - colina ( fch ) un tracciante pet recentemente introdotto , disponibile per lo studio di questa neoplasia [ 69 ] ; laccuratezza diagnostica dellesame pet con fch nellidentificazione del tumore primitivo , delle metastasi e nella ristadiazione in caso di recidiva biochimica stata valutata in alcuni studi preliminari [ 1013 ]  . 
le cellule neoplastiche sono caratterizzate dalla capacit di assumere atradiol med ( 2008 ) 113 : 895904 group of patients with detectable serum psa levels after radical treatment for prostate cancer . materials and methods patient population this study included 56 consecutive patients [ mean agestandard deviation ( sd ) : 67.97 years ] radically treated for prostate cancer ( radical prostatectomy ) who underwent whole - body fch - pet - ct study to detect disease recurrence . 
none was receiving hormone treatment at the time of the examination or had been treated in the previous 6 months . pet acquisition protocol all patients underwent whole - body fch - pet - ct at our pet centre . 
injection of 185259 mbq fch ( iasocholine , graz - seiersberg , austria ) and oral administration of 10 ml of contrast medium in half a litre of water ( gastrografin , schering spa , segrate , italy )  . 
no adverse events were observed in any of the patients after administration of fch or the oral contrast mediuthe acquisition protocol started with a scout view ( a ct bidimensional projection of the patient ) , which was used to define the axial extension ( start and end position ) over which to acquire the ct and pet data . 
once the scan range had been defined , usually from the proximal femur to the base of the skull , a low - dose ct scan was acquired ( 140 kv and 60 mas )  . 
pet emission data of the whole - body distribution of the tracer were acquired ( 3.5 min per fov ) in 3d mode ( from the pelvis to the neck )  . 
analisi biochimiche hanno dimostrato che lattivit di questo enzima fortemente incrementata nella cellula neoplastica [ 14 ]  . lo scopo del nostro studio stato quello di valutare il ruolo dellesame pet / tc con 18f - colina nella identificazione e localizzazione di recidiva di malattia in un gruppo di pazienti sottoposti a trattamento chirurgico radicale per neoplasia prostatica , in presenza di attuale recidiva biochimica . materiali e metodi pazienti sono stati inclusi 56 pazienti consecutivi ( et mediadeviazione standard ( ds ) : 67 , 97 anni ) precedentemente trattati con chirurgia radicale per carcinoma della prostata ( prostatectomia radicale )  . 
al momento dellindagine pet tutti presentavano recidiva biochimica ( definita come livelli serici di psa dosabili ) : psa mediods : 4 , 597 , 87 ng / ml ; range 0 , 139 ng / ml . 
nessuno di loro era in trattamento ormonale al momento dellesame , n era stato trattato nei 6 mesi precedenti . protocollo di acquisizione della tomografia ad emissione di positroni tutti i pazienti inclusi nello studio sono stati sottoposti ad esame pet / tc total - body nello stesso centro pet . 
secondo il protocollo di acquisizione , lesame comincia 60 minuti dopo liniezione endovenosa di 18f - colina ( iasocholine , graz - seiersberg , austria ; range dose 185259 mbq ) e dopo lassunzione di un mezzo di contrasto per via orale ( gastrografin , schering spa , segrate , italia ; 10 ml in mezzo litro di acqua )  . 
il protocollo di acquisizione dellesame pet / tc prevede inizialmente lesecuzione di uno scout view ( una proiezione bidimensionale del paziente ) che permette di definire lestensione assiale del corpo ( posizione iniziale e finale ) a livello della quale acquisire lesame tc e quello pet . 
una volta stabilita lestensione di scansione ( normalmente tra la porzione prossimale del femore e la base cranica ) , viene acquisito lesame tc a basso dosaggio ( 140 kv , 60 ma / s )  . 
neoplastic disease on pet was diagnosed when one or more areas of focal abnormal increase in tracer uptake were visually evident . data and statistical analysis because all patients had been surgically treated for prostate cancer by radical prostatectomy , detectable serum psa levels were considered the indicator of disease relapse . 
all pet findings were compared with the wholebody , low - dose ct acquired simultaneously to the pet study , and when available , with diagnostic tests performed within 1 month of the pet scan ( abdominopelvic contrastenhanced ct , pelvic mri , bone mri , bone scintigraphy , transrectal ultrasound ) , with biopsy and follow - up . 
however , in each of these patients , at least one area of pathological uptake of fch was further investigated through biopsy ( in the case of the prostate bed ) or mri ( in the case of lymph nodes and bone metastases )  . on the basis of the serum psa levels , we divided our patient population into three subgroups : ( a ) psa ( cid : 2 ) 1 ng / ml , ( b ) 1 < psa ( cid : 2 ) 5 ng / ml and ( c ) psa > 5 ng / ml . 
among the four patients with local recurrence , further studies did not identify distant metastases , and prostate - bed biopsy confirmed the pet finding . therefore , these patients underwent further local curative treatment . 
in the remaining 20 patients with positive pet findings , at least one area of pathological fch uptake underwent further testing and was confirmed to be a relapse by biopsy or by mri ( true positive )  . 
in caso di indagine pet negativa , i pazienti sono stati sottoposti ad ulteriori esami ( come biopsia della loggia prostatica , tc con mezzo di contrasto , risonanza magnetica , rm ) o sono stati seguiti nel follow - up , oppure hanno iniziato terapia ormonale . 
infatti , tutti i reperti pet sono stati confrontati con la tc total - body a bassa dose acquisita contestualmente allo studio pet e , quando disponibile , con altre indagini diagnostiche eseguite entro un mese dallesame pet ( tc addome / pelvi con mezzo di contrasto , rm della pelvi , rm scheletrica , scintigrafia ossea total - body , ecografia transrettale ) , con la biopsia e con il follow - up . 
b - e sezioni transassiali pet e pet / tc ( b , c ) evidenziano ipercaptazioni patologiche a livello della loggia prostatica e ulteriori ipercaptazioni patologiche ( d , e ) nei linfonodi pelvici ( frecce )  . of the 32 remaining cases ( 32 / 56 ) , there was one patient with a single pathological bone uptake ( left rib ) at pet ( psa 1.07 ng / ml ) ; however , further studies demonstrated the presence of a posttraumatic fracture . 
nei restanti 20 pazienti con pet positiva almeno uno degli accumuli patologici di 18f - colina stato ulteriormente studiato e confermato come recidiva tramite biopsia o rm ( veri positivi , vp )  . 
tutti questi pazienti sono stati sottoposti a trattamento ormonale . tra i restanti 32 casi ( 32 / 56 ) , un paziente ( psa 1 , 07 ng / ml ) presentava allesame pet una singola focalit patologica a livello scheletrico ( un arco costale sinistro ) ; ulteriori indagini hanno tuttavia evidenziato a tale livello una frattura di origine traumatica . 
 radiol med ( 2008 ) 113 : 895904 discussione lidentificazione della recidiva di malattia nel carcinoma prostatico , in pazienti trattati radicalmente e con psa serico dosabile un argomento di estrema importanza in considerazione delle successive strategie terapeutiche disponibili . 
 sfortunatamente , seppure il dosaggio del psa serico un indice di recidiva di malattia , lidentificazione e la localizzazione della stessa continuano a rappresentare una vera e propria sfida diagnostica . 
tra questi , per lo studio della loggia prostatica : la risonanza magnetica , la risonanza magnetica con bobina endorettale , la risonanza magnetica con spettroscopia e lecografia trans - rettale . 
seppure queste metodiche diagnostiche presentano livelli soddisfacenti di sensibilit e specificit , la biopsia della loggia prostatica rimane esame necessario per confermare / escludere la presenza di recidiva locale [ 1518 ]  . 
dallaltra parte la biopsia prostatica una procedura dolorosa e presenta bassi livelli di sensibilit ( 48%50% ) in assenza di unarea sospetta ben localizzata [ 16 , 17 ]  . 
infine , per la ricerca delle metastasi scheletriche , i pazienti si sottopongono alla scintigrafia ossea , la quale presenta livelli di sensibilit alti ma bassa specificit , e spesso necessita di ulteriori esami dimaging allo scopo di caratterizzare reperti patologici . 
 in campo oncologico lo studio pet / tc divenuto rapidamente una importante metodica diagnostica , essendo un esame che , in singola seduta e non invasivamente , consente di stadiare la malattia localmente e a distanza . 
lo studio pet consente la caratterizzazione metabolica di qualunque lesione , indipendentemente dalle sue dimensioni e la distinzione di tessuti neoplastici da quelli fibrotici o necrotici . inoltre , lintroduzione dei tomografi ibridi pet / tc ha consentito di aggiungere e coregistrare linformazione morfologica ( tc ) a quella funzionale ( pet ) incrementando i livelli di sensibilit e specificit . 
cos , nel caso delladenocarcinoma prostatico , lesame pet / tc consente di studiare la loggia prostatica , i linfonodi addomino - pelvici , le ossa e tutti gli altri distretti corporei . 
nonostante alcuni buoni risultati iniziali [ 2 ] , il 18f - desossi - glucosio presenta bassi valori di sensibilit ( dovuti alla scarsa fissazione di questo composto da parte delle cellule delladenocarcinoma prostatico ) e non adatto per la valutazione della neoplasia primitiva , a causa dellescrezione urinaria [ 19 , fig . 
4 percentuale di identificazione della recidiva di malattia con esame pet / tc con 18f - colina rispetto ai livelli serici del psa ( ng / ml )  . discussion detection of prostate cancer recurrence in patients who have undergone radical treatment and have detectable serum psa levels is a major issue due to its impact on subsequent treatment strategies . 
unfortunately , although serum psa is a marker of disease relapse , identification and localisation of recurrence remains a challenge . currently , several diagnostic tests are needed for accurate staging of these patients . 
on the other hand , prostate - bed biopsy is an invasive and painful procedure that has low sensitivity levels ( 48%50% ) in the absence of a well - localised suspected area [ 16 , 17 ]  . 
finally , for studying bone metastases , patients usually undergo whole - body bone scintigraphy , which has high sensitivity but low specificity and often requires the use of additional imaging studies , such as mri , to verify pathological findings . 
thus , a single noninvasive diagnostic test is desirable to reduce the time required to locate and stage the disease . pet - ct plays an important , emerging role in oncology and is a noninvasive whole - body examination that allows evaluation of local and distant disease in one step . 
pet 902 radiol med ( 2008 ) 113 : 895904 study provides a metabolic characterisation of morphological lesions , independently of their size , and enables neoplastic tissue to be distinguished from fibrosis and necrosis . moreover , the hybrid pet - ct scanner offers the additional advantage of combining morphological information ( ct ) with the functional information provided by pet , allowing a gain in both sensitivity and specificity . 
despite some initial good results [ 2 ] , fdg has low sensitivity ( due to low uptake by prostate adenocarcinoma cells ) and is unsuitable for evaluating the primary neoplasm because of its urinary excretion [ 19 , 20 ]  . 
recently , the usefulness of acetate in patients with suspected prostate cancer recurrence has been evaluated , but despite the promising results , further studies are required to validate its use [ 2123 ]  . 11c - labelled and 18f - labelled choline analogues are new oncological pet tracers : choline metabolism in tumour cells is a marker of duplication rate due to the fact that cells need choline for synthesising cell membrane phospholipids [ 6 , 7 , 14 , 24 ]  . 
other authors demonstrate the utility of 11c - choline both in detecting recurrences [ 26 , 27 ] and in preoperative staging [ 28 ] , with higher sensitivity levels compared with mri spectroscopy [ 29 ]  . 
however , due to the short half - life of 11c ( 20 min ) , the use of 11c - choline is limited to pet centres with an on - site cyclotron . 
among these 24 patients , pet enabled differentiation between local and systemic relapse and therefore helped in the planning of appropriate treatment . in contrast , 31 cases were negative at the pet study . one reason for this high rate of negative pet scans could be lesion size , given that the pet resolution limit is between 5 mm and 10 mthis hypothesis seems to be confirmed by several data . 
first , the higher number of negative results found in patients with lower serum psa levels , and therefore probably with a limited amount of disease ( our series included three patients with psa lower than 0.2 ng / ml , all of whom were negative at pet )  . 
pi recentemente stato valutato luso dellacetato in pazienti con sospetto di recidiva di neoplasia della prostata , ma seppure alcuni studi riportano per questo tracciante un ruolo promettente [ 2123 ] , sono necessarie ricerche ulteriori . gli analoghi della colina marcati con 11c e 18f sono nuovi traccianti oncologici usati in pet : il metabolismo della colina nelle cellule tumorali un indice della velocit di duplicazione visto che le cellule necessitano di colina per la sintesi dei fosfolipidi , costituenti delle loro membrane [ 6 , 7 , 14 , 24 ]  . 
 [ 25 ] riportano migliore sensibilit e specificit della pet con 11c - colina nella ristadiazione del tumore della prostata quando confrontata con la pet con fdg [ 25 ]  . 
altri autori hanno dimostrato lutilit della 11c - colina sia nel riconoscimento delle recidive [ 26 , 27 ] , che nella stadiazione prima dellintervento [ 28 ] , con sensibilit migliore della rm con spettroscopia [ 29 ]  . 
tuttavia , a causa della breve emivita del 11c ( 20 minuti ) , luso della 11c - colina limitato solo a quei centri pet che dispongono di un ciclotrone in sito . 
infatti lemivita del 18f , che di 110 minuti , consente il suo trasporto a distanza , permettendone luso anche in quei centri in cui il ciclotrone non disponibile . nella nostra esperienza , comprendente pazienti trattati radicalmente per adenocarcinoma prostatico ed in presenza di recidiva biochimica , lesame pet / tc con fch ha consentito di identificare la recidiva di malattia nel 42 , 9% dei casi . 
in questi 24 pazienti , lesame pet ha permesso di distinguere tra recidiva locale e sistemica e dunque di pianificare il trattamento pi appropriato . daltra parte abbiamo avuto 31 casi risultati negativi allesame pet . 
una ragione per spiegare questo alto valore di esami pet negativi potrebbe essere la dimensione della lesione : infatti i limiti della risoluzione dellesame pet sono tra 5 e 10 mquesta ipotesi sembra essere confermata da alcuni dati : primo , lalto numero di risultati negativi in pazienti con psa basso , e quindi , probabilmente con una quantit limitata di malattia ( per esempio nella nostra popolazione , abbiamo incluso 3 pazienti con valori serici di psa minori di 0 , 2 ng / ml e tutti sono risultati negativi allesame pet ) ; secondo , laumento dei livelli di psa strettamente correlato con laumento della percentuale di identificazione di recidiva , come mostrato in figura 4 ; infine , 26 pazienti tra i 31 negativi alla pet , sono risultati negativi in tutti gli altri esami eseguiti per identificare la recidiva di malattia . nello studio della loggia prostatica abbiamo trovato 5 radiol med ( 2008 ) 113 : 895904 in pet sensitivity , as shown in fig . 
finally , in 26 of the 31 patients with a negative pet study , all other tests carried out to identify disease relapse proved negative as well . study of the prostate bed yielded five false negative cases . 
probably , as suggested by heinisch et al . , sensitivity in detecting local disease relapse can be improved by using different image acquisition protocols , in particular , early dynamic acquisition [ 12 ]  . another finding of our study was the relation between serum psa levels and pet detection rate . 
however , even though the detection rate was indeed very low ( 20% ) in the subgroup with psa < 1 ng / ml , pet was positive and provided correct localisation of disease in 44% of patients in the subgroup with psa between 1 and 5 ng / ml . finally , in the study of the prostate bed , we had five patients with biopsy - proven disease recurrence and negative pet scans . 
probably , as suggested by heinisch et al . , the sensitivity in detecting local disease relapse can be improved by using different image acquisition protocols , in particular , early dynamic acquisition [ 12 ]  . study limitations we were unable to confirm the histopathology of all areas of abnormal fch uptake . 
however , the ct correlate was available in all cases , and the lack of histopathological confirmation is a common problem shared with all clinical studies on this topic . conclusions despite the limits of this study and the need for further and larger - scale investigations , whole - body fch - pet - ct confirms its usefulness for detecting disease in patients presenting biochemical relapse after radical treatment for prostate cancer ( 42 , 9% detection rate in our series )  . 
 [ 12 ] , la sensibilit nellidentificazione della recidiva locale pu migliorare usando protocolli diversi dacquisizione dellimmagine ed in particolare lacquisizione dinamica precoce . un altro risultato della nostra esperienza la relazione diretta tra il livello serico del psa e la percentuale di identificazione di recidiva di malattia dellesame pet , come chiaramente mostrato dalla fig . 
invece nei sottogruppi di pazienti con psa minore di 5 ng / ml la bassa percentuale di identificazione della malattia con fch - pet / tc suggerirebbe di eseguire questo esame almeno dopo lo studio della loggia prostatica . 
in ogni caso , anche importante sottolineare che , se nel sottogruppo con psa minore di 1 ng / ml la percentuale di identificazione dellesame risultata molto bassa ( cio 20% ) , viceversa in quasi uno su due casi , lesame pet ha permesso di localizzare correttamente la malattia nel sottogruppo di pazienti con livelli di psa compresi tra 1 e 5 ng / ml . infine , nello studio della loggia prostatica abbiamo avuto 5 pazienti con recidiva di malattia locale accertata dalla biopsia ma con esame pet negativo . 
 limiti dello studio in questo studio non abbiamo avuto la possibilit di verificare istologicamente tutte le fissazioni anomale di fch . tuttavia bisogna sottolineare che un correlato tc risultato disponibile in tutti i casi e che lassenza di conferma istopatologica un problema comune condiviso con tutti gli altri studi clinici su questo tema . 
 conclusioni nonostante alcuni limiti e la necessit di ulteriori e pi ampie indagini , questo studio conferma lutilit dellesame fch - pet / tc total body nellidentificazione della recidiva in pazienti radicalmente trattati per adenocarcinoma prostatico , in presenza di recidiva biochimica . 
rotondo1 1institute of radiology , second university of naples , piazza miraglia , 80138 naples , italy 2department of radiology , university of palermo , palermo , italy correspondence to : r . 
micro - pet ( positron emission tomography ) , micro - spect ( single photon emission computed tomography ) , micro - ct ( computed tomography ) , micro - mr ( magnetic resonance ) , micro - us ( ultrasound ) and optical imaging are all molecular imaging techniques , several of which are applied only in preclinical settings on animal models . 
research on small animals allows investigation of the genesis and development of diseases , as well as drug efficacy and the development of personalized therapies , through the study of biological processes that precede the expression of common symptoms of a pathology . 
advances in molecular imaging were made possible only by collaboration among scientists in the fields of radiology , chemistry , molecular and cell biology , physics , mathematics , pharmacology , gene therapy and oncology . 
although until now researchers have traditionally limited their interactions , it is only by increasing these connections that the current gaps in terminology , methods and approaches that inhibit scientific progress can be eliminated . riassunto in tre parole , genomica , proteomica e nanotecnologie , racchiusa la rivoluzione della medicina del terzo millennio , che sar caratterizzata da una pi accurata prevenzione , diagnosi e terapia delle malattie . 
questa trova piena espressione nellimaging molecolare : una nuova scienza che coniuga insieme la biologia molecolare e limaging in vivo e rappresenta la chiave delle applicazioni per una medicina personalizzata . 
la micropet e la micro - spect ma anche la micro - tc , la microrm , micro - ecografia e loptical imaging sono procedure di imaging molecolare , di cui alcune vengono applicate solamente in campo pre - clinico su modelli animali da laboratorio , altre gi trovano analoga e routinaria applicazione sia in campo clinico ed ora preclinico . mediante la sperimentazione su piccoli animali si possono studiare linsorgenza e levolversi delle malattie ovvero lefficacia dei farmaci e lo sviluppo di trattamenti personalizzati , attraverso , ad esempio , lo studio dei processi biologici che precedono il palesarsi dei tipici sintomi di una patologia . 
tutto ci richiede la stretta collaborazione di scienziati nel campo della radiologia , chimica , biologia cellulare e molecolare , fisica , matematica , farmacologia , terapia genica , oncologia . sebbene , fino ad ora , i ricercatori abbiano generalmente limitato le loro interrelazioni , solo incrementando questi rapporti che il gap attuale , nella terminologia , nei metodi e nellapproccio , che rallenta il progresso , pu essere finalmente eliminato . keywords genomics proteomics nanotechnology molecular imaging radiology parole chiave genomica proteomica nanotecnologie imaging molecolare radiologia 776 radiol med ( 2008 ) 113 : 775778 in these three words genomics [ 1 ] , proteomics [ 2 ] and nanotechnologies [ 3 ] is the future of the medicine of the third millennium , which will be characterised by more careful attention to disease prevention , diagnosis and therapy . 
in recent years , there has been an explosion of knowledge surrounding the nature and function of genes and proteins that establish communication systems within and between cells . decoding and understanding the genome , which contains every gene , and the proteome , which contains every protein , will allow identification of genetic and / or protein alterations that sustain many pathologies . 
therefore , the possibility of understanding the underlying mechanisms at the root of diseases and of initiating therapies directed at causes and not symptoms , is an exciting concept . however , to study these phenomena , complex technologies , such as the new so - called nanotechnologies , are necessary to identify at the molecular level the alterations in the human body composition . 
the use of microelectronic mechanical system ( mems ) [ 5 ] allows to directly image cells in their biological activity , also in living organisms . to meet the growing need of investigating the pathogenetic basis of diseases and the therapeutic response to drugs on animals in vivo , in the last years there has been a growing diffusion of saifs ( small animal imaging facilities ) with highly specialized staff , able to support the diverse necessities of the scientific community . 
molecular imaging is a new science that bridges molecular biology and in vivo imaging and represents the key to the application of a personalized medicine . micro - pet ( positron emission tomography ) , microspect ( single photon emission tomography ) , micro - ct ( computed tomography ) , micro - mr ( magnetic resonance ) , micro - us ( ultrasonography ) and optical imaging are molecular imaging techniques , several of which are applied only in the preclinical setting on animal models ( e.g. , optical imaging ) , whereas others are routinely applied in clinical and preclinical settings . 
 research on small animals allows investigation into the genesis and development of diseases , as well as studying drug efficacy and developing personalized treatments by investigating biological processes that precede the expression of common symptoms of a pathology . 
 the significant progress attained in recent years in noninvasive imaging techniques , probes , imaging analysis and biological and mathematical models has allowed detection in tre parole , genomica [ 1 ] , proteomica [ 2 ] e nanotecnologie [ 3 ] , racchiusa la rivoluzione della medicina del terzo millennio , che sar caratterizzata da una pi accurata prevenzione , diagnosi e terapia delle malattie . 
negli ultimi anni si verificata unesplosione di conoscenze circa la natura e le funzioni dei geni e delle proteine che creano sistemi di comunicazione tra le cellule del nostro corpo e allinterno di esse . 
 la possibilit di disporre del genoma , linsieme dei geni , e del proteoma , linsieme delle proteine , consentir di identificare le singole alterazioni geniche e / o proteiche alla base di molte patologie ; sar quindi possibile comprendere gli intimi meccanismi alla base delle malattie ed intervenire con cure che mirino alle cause e non alla sintomatologia di un qualsiasi processo morboso . 
tra le nanotecnologie , i sistemi meccanici di microelettronica , o mems [ 5 ] , una tecnica dimaging molecolare che permette di osservare le cellule in azione in organismi viventi , e di valutare i processi biologici in vivo . 
al fine di soddisfare la crescente necessit di studiare i meccanismi patogenetici delle malattie e la risposta terapeutica ai farmaci sugli animali in vivo , negli ultimi anni hanno si assistito alla nascita e alla diffusione di servizi per limaging su piccoli animali ( saif ) capaci di supportare , con personale altamente specialistico , le differenti necessit della comunit scientifica . 
limaging molecolare dunque una nuova scienza che coniuga insieme la biologia molecolare e limaging in vivo e rappresenta la chiave delle applicazioni per una medicina personalizzata . essa linsieme di tecnologie avanzate di diagnostica per immagini che consentono di visualizzare i processi molecolari che avvengono a livello cellulare in un organismo vivente . 
la micro - pet ( tomografia ad emissione di positroni ) e micro - spect ( tomografia ad emissione di un singolo fotone ) ma anche la micro - tc , la micro - rm , microecografia ed loptical imaging sono procedure di imaging molecolare , di cui alcune vengono applicate solamente in campo pre - clinico su modelli animali da laboratorio ( come loptical imaging ) , altre gi trovano analoga e routinaria applicazione sia in campo clinico ed ora preclinico . mediante la sperimentazione su piccoli animali si possono studiare linsorgenza e levolversi delle malattie ovvero lefficacia dei farmaci e lo sviluppo di trattamenti personalizzati , attraverso , ad esempio lo studio dei processi biologici che precedono il palesarsi dei tipici sintomi di una patologia . 
 lenorme progresso raggiunto nei recenti anni nel radiol med ( 2008 ) 113 : 775778 and identification of molecules in living organisms and the study of genic expression in vivo . 
these advances thus create the prospect of developing pre - emptive medicine by making use of precise molecular knowledge to detect disease before symptoms are manifest and by intervening before disease can develop [ 6 ]  . nevertheless , only by creating strong cooperation between various disciplines can that goal be achieved , because interdisciplinary and multimodality cooperation are essential to progress in this area . 
in fact , to develop pre - emptive , predictive medicine in the twenty - first century , to fully capitalise on the sequencing of the human genome and to take full advantage of recent advances in molecular and cell biology , the research community will require wide access to technologies , databases , and other scientific resources that are sensitive , robust , and more easily adaptable to researchers individual needs . 
for example , advances in molecular imaging were made possible only by collaboration among scientists in the fields of radiology , chemistry , molecular and cell biology , physics , mathematics , pharmacology , gene therapy and oncology . 
although until now researchers traditionally have limited their interactions to their own scientific studies , it is only by forging these critical connections that the current gaps in terminology , methods and approaches that so seriously impede progress can be eliminated [ 6 ]  . methods based on molecular imaging have attained a primary role in the biomedical arena , with enormous development , especially in oncological , neurological and cardiology fields . 
available animal models are often inadequate ; they do not reproduce in a satisfying manner several diseases . moreover , we have no basis to determine how accurate a particular study on animals is , because a positive result on animals is not always replicable on humans [ 7 ] 2 . 
in the future , it will be important to collaborate with local doctors , particularly in patient management , considering the increased prevalence of chronic conditions with respect to acute ones 3 . 
the increased time spent for clinical activity and the reduced financial margins diminish the attention of clinical and translational researchers devoted to the research mission of academic institutions campo degli strumenti dimaging non invasivi , di sonde , dellanalisi di immagine , nei modelli biologici e matematici ha reso possibile localizzare e rilevare molecole negli organismi viventi e visualizzare lespressione genica in vivo . 
ne scaturisce la possibilit di poter finalmente praticare una medicina preventiva , facendo uso di una precisa conoscenza molecolare per individuare la malattia prima che i sintomi si manifestino , ed intervenendo prima che la malattia stessa si scateni [ 6 ]  . 
infatti , per poter sviluppare la medicina predittiva e preventiva del 21 secolo , fruire del sequenziamento del genoma umano , e prendere pieno vantaggio dalle recenti scoperte nel campo della biologia molecolare e cellulare , la comunit scientifica necessiter di un pi ampio accesso alle tecnologie , ai database e ad altre risorse scientifiche pi sensibili , pi robuste e pi facilmente adattabili alle necessit singole dei ricercatori . 
lentit e la complessit delle recenti difficolt della ricerca biomedica richiedono che gli scienziati si muovano oltre i confini delle loro proprie discipline ed esplorino nuovi modelli organizzativi per gruppi scientifici . i progressi nellimaging molecolare , per esempio , richiedono la collaborazione di scienziati nel campo della radiologia , chimica , biologia cellulare e molecolare , fisica , matematica , farmacologia , terapia genica , oncologia . 
sebbene fino ad ora nella loro vita scientifica , i ricercatori hanno generalmente limitato le loro relazioni , solo cementando questi critici rapporti che il gap attuale nella terminologia , nei metodi , e nellapproccio , che cos seriamente impedisce il progresso , pu essere finalmente eliminato [ 6 ]  . le metodiche basate sullimaging molecolare hanno cos assunto un ruolo determinante nel settore biomedico , con uno sviluppo vertiginoso specie in campo oncologico , neurologico e cardiologico . 
laumento del tempo dedicato alle attivit cliniche e la riduzione dei fondi distrae i ricercatori clinici e traslazionali dalla missione scientifica dellistituzione . 778 radiol med ( 2008 ) 113 : 775778 4 . 
clinical and translational research encompasses the acquisition of new knowledge about health and disease prevention , pre - emption and treatment and the methodologic research necessary to develop or improve research tools . 
radiologists , especially those who work in university and research sites , need to make an effort to participate in the development of this fascinating new area of diagnostic imaging . 
in this area , young radiologists , who are able to shift their clinical expertise into the preclinical and research sector , will definitely broaden their job opportunities and find new possibilities for utilising their training and expertise . 
la ricerca clinica e traslazionale abbraccia sia lacquisizione di nuove conoscenze in termini di salute e malattia , sia la prevenzione , il trattamento e la ricerca metodologica necessarie a sviluppare e migliorare i mezzi scientifici . 
i radiologi , specie quelli che operano in sedi universitarie e di ricerca , devono applicarsi e partecipare alla nascita di questo nuovo e affascinante settore di attivit della diagnostica per immagini . 
all patients underwent a whole - body pet / computed tomography ( ct ) scan ( pet - 1 ) acquired 1 h post [ 18f ] fluorodeoxyglucose ( fdg ) injection , and a liver pet / ct scan [ that is , one or two fields of view ( fov ) of the upper abdomen ; pet - 2 ] acquired 2 h postinjection . in all cases , image reconstruction was performed as 3d reconstruction algorithm fourier rebinning ( fore ) iterative , fov 50 cm , image matrix size 128128 . 
thirty - seven of 95 patients ( 38.9% ) presented liver lesions at both pet - 1 and pet - 2 exams , whereas there were two ( 2.2% ) only at pet - 2 . 
scopo di questo studio stato quello di valutare se in pazienti con sospette secondariet epatiche , la riacquisizione di immagini , 2 ore dopo la somministrazione del radiofarmaco ( tardiva ) , comporta un miglioramento della sensibilit dellesame pet . 
trentasette dei 95 pazienti ( 38 , 9% ) hanno presentato anomale iperfissazioni di radiofarmaco a livello epatico in entrambi gli esami pet ; 2 pazienti ( 2 , 2% ) sono risultati positivi solo in pet - 2 . 
its role in tumour staging / restaging , in the early and / or final evaluation of response to treatment and in the differentiation between radiotherapy - induced scar tissue and disease relapse is widely recognised . 
the introduction of the pet / computed tomography ( ct ) hybrid scanners , which superimposes pet functional images and low - dose ct morphological images , allows a more precise localisation and thus a better characterisation of fdg uptake , with a consequent increment of pet accuracy but in particular of pet specificity [ 1 ]  . 
this solution , by gating respiratory activity , removes artefacts due to respiratory movement , allows a more precise definition of tumour volume and position and improves pet sensitivity in lesion detection [ 13 ]  . 
this approach seems to imnellinquadramento e nella gestione del paziente oncologico , la tomografia ad emissione di positroni ( pet ) con 18f - fluorodeossiglucosio ( fdg ) considerata uno strumento diagnostico di grande importanza . 
il suo ruolo nella stadiazione / ristadiazione , nella valutazione precoce della risposta e / o alla fine del trattamento e nella caratterizzazione metabolica di lesioni morfologiche di dubbia natura ( come per esempio la differenziazione tra esiti cicatriziali post - attinici e ripresa di malattia neoplastica ) ampiamente provato e riconosciuto . 
lintroduzione dei tomografi ibridi pet / tc , permettendo la coregistrazione di immagini pet , di tipo funzionale , con immagini tc , di tipo morfologico , consente una maggiore precisione e perci , una migliore caratterizzazione degli up - take di fdg , con conseguente aumento dellaccuratezza della pet e , in particolare , della sua specificit [ 1 ]  . 
primo , il comportamento biologico del tumore stesso : esistono infatti alcune neoplasie , come i carcinoidi , il carcinoma bronchioloalveolare , il carcinoma della prostata , lepatocarcinoma , ecc . 
con un basso metabolismo glucidico e / o con una scarsa ritenzione di glucosio ( e dunque di fdg ) [ 25 ] ; secondo , i livelli plasmatici basali di glucosio e di insulina [ 6 ] ; terzo , le dimensioni della massa tumorale ( la risoluzione del tomografo pet di circa 510 mm ) [ 79 ] ; quarto , il basso rapporto lesione / fondo , soprattutto negli organi che in condizioni fisiologiche presentano alta fissazione di glucosio [ 10 ] ; infine , il movimento della lesione durante lacquisizione delle immagini emissive pet ( dovuto ai movimenti conseguenti allatto respiratorio , al battito cardiaco , alla peristalsi intestinale ) , movimento che riduce la qualit delle immagini pet e dunque la capacit di visualizzazione della lesione stessa [ 11 ]  . 
in particolare , il fegato , sembra essere uno degli organi che viene influenzato pi negativamente ; esso presenta infatti una fissazione fisiologica di fdg piuttosto elevata ed fortemente soggetto ad artefatti legati al movimento respiratorio . 
lidentificazione delle metastasi epatiche con lesame fdg - pet risultava correlata con le dimensioni delle stesse e la sensibilit dello studio pet era del 14% per lesioni inferiori a 1 , 5 cm [ 12 ]  . 
 per superare questo limite sono state proposte diverse radiol med ( 2008 ) 113 : 875886 prove pet sensitivity in detecting small liver metastases by overcoming artefacts from respiratory movement and minimising the offset in image fusion [ 14 ]  . 
in this way , it seems possible to achieve greater contrast between the tumour ( which , unlike normal tissue , continues to accumulate fdg over time ) and background ( that shows a progressive washout of the tracer ) and thus to improve pet sensitivity [ 15 ]  . the aim of this study was to evaluate whether detection of liver pathological uptakes could be improved by acquiring delayed pet images at the upper abdominal level . materials and methods patients the study population included 95 patients ( 46 women and 49 men ; mean age 63.8 years ) who underwent whole - body pet / ct between march and december 2006 . 
all selected patients had been previously treated for neoplastic disease ( colon / rectum n = 42 ; pancreas / liver n = 14 ; breast n = 10 ; lung n = 8 ; upper bowel n = 8 ; uterus / ovary n = 6 ; carcinoma with unknown primary tumour syndrome n = 2 ; sarcoma n = 2 ; lymphoma n = 2 ; testes n = 1 )  . 
all patients were referred for whole - body fdg - pet for clinical restaging after an increase of specific serum tumour marker or to metabolically characterise a morphological finding suspicious for recurrence . pet protocol pet studies were acquired using a pet / ct scanner ( discovery st , general electric medical systems , waukesha , wi , usa )  . 
all patients were requested to refrain from food intake for at least 6 h before the exaat the time of tracer injection , glucose blood levels , meanstandard deviation ( sd ) , were 9812 mg / dl ( range 79184 mg / dl )  . 
pet emission data were acquired after the intravenous injection of fdg ( mean injected activity 19225 mbq , range 152307 mbq ) and after oral administration of a contrast medium ( gastrografin , schering spa , segrate , milan , italy : 10 ml in a half litre of water )  . 
da una parte lutilizzo di accorgimenti in grado di ridurre gli artefatti da movimento respiratorio durante lacquisizione delle immagini emissive pet ( tecnica 4d , con gating respiratorio [ 13 ] ; riacquisizione di unimmagine emissiva pet di 45 secondi , con paziente in inspirazione profonda [ 14 ] )  . 
con questa soluzione sembrerebbe possibile di ottenere una significativa riduzione della captazione di fdg da parte del tessuto epatico sano , con conseguente maggiore contrasto tra la massa tumorale ( che continua ad accumulare fdg ) e il fondo ( che presenta un progressivo wash - out ) [ 15 ]  . scopo del presente lavoro stato quello di valutare se lidentificazione di anomale iperfissazioni a livello epatico possa essere migliorata con la riacquisizione di immagini pet tardive . materiali e metodi pazienti in questo studio sono stati inclusi 95 pazienti ( 46 donne e 49 uomini ; et media 63 , 8 anni ) , sottoposti ad un esame pet / tc , tra marzo e dicembre 2006 . 
i pazienti selezionati erano stati precedentemente trattati per malattie neoplastiche ( colon - retto n = 42 ; pancreas / fegato n = 14 ; mammella n = 10 ; polmone n = 8 ; esofago / stomaco / duodeno n = 8 ; utero / ovaio n = 6 ; sindrome da carcinoma occulto n = 2 ; sarcoma n = 2 ; linfoma n = 2 ; seminoma n = 1 )  . 
tutti hanno eseguito esame pet / tc con 18f - fluorodesossiglucosio per ristadiazione clinica in seguito allaumento dei valori serici di un marcatore tumorale oppure per caratterizzare metabolicamente una o pi lesioni sospette per recidiva . protocollo pet lo studio pet stato effettuato con un tomografo ibrido pet / tc ( discovery st , general electric medical systems , waukesha , wi , usa )  . 
i dati emissivi della pet sono stati acquisiti dopo liniezione di fdg ( attivit media iniettata , 19225 mbq , range 152307 mbq ) e dopo la somministrazione di un mezzo di contrasto per via orale ( gastrografin , schering spa , segrate , italia ; 10 ml in 500 ml dacqua )  . 
i pazienti si sono sottoposti ad un esame pet / tc total body ( pet - 1 ) , acquisito unora dopo liniezione ed ad un secondo esame pet / tc fegato ( pet - 2 ; cio uno o due campi di vista fov delladdome superiore ) acquisito 2 ore dopo liniezione . 878 radiol med ( 2008 ) 113 : 875886 pet - 1 : whole - body fdg - pet / ct study pet - 1 : studio fdg - pet / tc total body the acquisition protocol started with a scout view ( a ct bidimensional projection of the patient ) that was used to define the body axial extension ( start and end position ) over which to acquire the ct and pet data . 
once the scan range had been defined , the ct scan was performed from neck to pelvis , with a voltage of 140 kv and tube current of 60 mas . this scan lasted approximately 1 min and was used for both anatomical localisation and attenuation correction of pet emission data . 
pet emission data of the whole - body distribution of the tracer were acquired in 3d mode ( 8 to 9 fovs of 3.5 min each ) from the pelvis to the neck . 
image reconstruction was performed as a 3d reconstruction algorithm fourier rebinning ( fore ) iterative , fov 50 cm , image matrix size 128128 . pet - 2 : liver fdg - pet / ct study to define the axial extension over which to acquire the ct and pet data , the acquisition protocol started with the scout view . 
once the scan range had been defined , the ct scan was performed from the lower part of the lung to the lower abdomen , with a voltage of 140 kv and tube current of 60 mas . 
image reconstruction was performed as a 3d reconstruction algorithm fore iterative , fov 50 cm , image matrix size 128128 . il protocollo di acquisizione comprende uno scout view ( proiezione tc bidimensionale del paziente ) , utilizzato per definire la scansione assiale del corpo ( posizione di inizio e fine ) sulla quale acquisire i dati tc e pet . 
una volta definito lintervallo di scansione , dalla base cranica fino alla porzione prossimale del femore , viene eseguita una scansione tc ( voltaggio di 140 kv e intensit di corrente di 60 mas )  . 
la ricostruzione delle immagini realizzata con algoritmo di ricostruzione 3d fore iterativo , campo di vista 50 cm , dimensione della matrice di immagini 128128 . pet - 2 : fdg - pet / tc del fegato il protocollo di acquisizione inizia con uno scout view per definire lestensione assiale a livello della quale acquisire le immagini pet e tc . 
una volta definito lintervallo di scansione , la scansione tc viene eseguita dalla parte inferiore del polmone fino alladdome inferiore con voltaggio di 140 kv e intensit di corrente di 60 mas ; i dati emissivi pet vengono acquisiti in modalit 3d ( 12 fov di 3 , 5 oppure 5 oppure 10 minuti )  . 
la ricostruzione delle immagini ottenuta con algoritmo di ricostruzione 3d fore iterativo , campo di vista 50 cm , dimensione della matrice di immagini 128128 . pet image analysis analisi delle immagini pet first , a preliminary qualitative analysis of all pet - 1 and pet - 2 studies was performed to identify all pathological fdg uptake in the liver parenchyma by the same two nuclear medicine physicians ( ep and va )  . 
to evaluate lesions and background behaviour over time , a semiquantitative analysis [ based on the standard uptake value ( suv ) body weight value , i.e. : suvbw = [ measured activity concentration ( bq / g ) body weight ( g ) ] / injected activity ( bq ) was also performed . 
in particular : lesion suvmax and suvmean ( l1or l2 - suvmax , l1or l2 - suvmean ) , background suvmean ( bg1or bg2 - suvmean ) , and ratio lesion / background suvmean ( l / bg1 and l / bg2 )  . 
successivamente , per valutare landamento temporale della fissazione del radiotracciante a livello di lesioni e parenchima epatico sano ( fondo ) stata eseguita unanalisi semiquantitativa basata sui valori di suvbw ( peso corporeo ) , cio : suvbw = [ concentrazione misurata dellattivit ( bq / g ) massa corporea ( g ) ] / attivit iniettata ( bq )  . 
in particolare : suv massimo e suv medio della lesione ( l1oppure l2 - suvmax , l1oppure l2 - suvmedio ) , suvmedio del fondo epatico ( bg1oppure bg2 - suvmedio ) , e il rapporto suvmedio lesione / fondo ( l / bg1 e l / bg2 )  . l1and l2 - suvmax and suvmean l1e l2 - suvmax e suvmedio on the basis of the experience of the same nuclear medicine sulla base dellesperienza degli stessi medici nucleari , il voradiol med ( 2008 ) 113 : 875886 physician , the volume of the region with enhanced glucose metabolic activity was manually drawn on the pet - 2 study and then transferred to the same region of the pet - 1 study . the suvmax represents the standard uptake value of the maximum activity voxel cluster , whilst the suvmean represents the average values over the fdg lesion volume . 
il suvmax rappresenta il valore di suv del voxel con maggiore attivit allinterno della regione di interesse individuata ; il suvmedio rappresenta il valore medio di suv nella stessa regione di interesse . 
 bg1or bg2 - suvmean bg1e bg2 - suvmedio a standard volume region of interest ( roi ) was manually drawn on the pet - 2 study in a part of the liver parenchyma that did not present any pathological uptake or artefact and then transferred to the same region of the pet - 1 study . 
patients were divided into three groups : group a ( n = 31 patients ) , pet - 2 data acquisition per bed position 10 min ; group b ( n = 37 patients ) , pet - 2 data acquisition per bed position 5 min ; group c ( n = 27 patients ) , pet - 2 data acquisition per bed position 3.5 m moreover , data were analysed according to the primary cancer of each patient ( colon / rectum adenocarcinoma versus all other neoplasms )  . the increase / decrease between the semiquantitative parameters calculated at pet - 1 and pet - 2 studies ( delta ) was calculated as follows : delta = [ 100 ( pet - 2 pet - 1 ) ] / pet2 ]  . 
the differences between the semiquantitative parameters calculated in pet - 1 and pet - 2 studies were statistically evaluated using the wilcoxon test for all the lesions and separately for all the different groups . 
 the correlation between body mass index ( bmi ) and delta bg - suvmean , bmi and delta lesion / background ratios , glycaemia and delta bg - suvmean , glycaemia and delta lesion / background ratios , was evaluated using pearsons correlation coefficient ( r )  . 
a further una regione di interesse di dimensione standard stata disegnata manualmente nello studio pet - 2 , a livello del parenchima epatico che non presentava alcuna fissazione patologica di fdg , n artefatti ; la stessa regione dinteresse stata quindi trasferita nella stessa regione dello studio pet1 . 
i dati sono stati analizzati anche a seconda della durata dellacquisizione per fov in pet - 2 ( per questa analisi i pazienti sono stati suddivisi in tre gruppi : gruppo a , n = 31 pazienti , studio pet - 2 acquisito con fov di 10 minuti ; gruppo b , n = 37 pazienti , studio pet - 2 acquisito con fov di 5 minuti ; gruppo c , n = 27 pazienti , studio pet - 2 acquisito con fov di 3 , 5 minuti )  . 
 lincremento / decremento tra i parametri semi - quantitativi calcolati negli studi pet - 1 e pet - 2 ( delta ) stato calcolato come segue : delta = [ 100 ( pet - 2pet - 1 ) ] / pet - 2 . le differenze tra i parametri semi - quantitativi calcolati negli studi pet - 1 e pet - 2 sono state valutate statisticamente con il test di wilcoxon , sia per tutte le lesioni individuate che separatamente per i 3 diversi sottogruppi . la correlazione tra : body mass index ( bmi ) e delta bgsuvmedio , bmi e delta del rapporto lesione / fondo , glicemia e delta bg - suvmedio , glicemia e delta del rapporto lesione / fondo , sono stati valutati utilizzando il coefficiente di correlazione di pearson ( r )  . 
nove accumuli patologici di fdg ( 11 , 1% ) sono stati osservati a livello epatico solo allesame pet - 2 ( tabella 1 )  . nel gruppo a ( n = 31 ) abbiamo riscontrato 28 lesioni in radiol med ( 2008 ) 113 : 875886 fig . 
pet - 2 ( fov 5 minuti ) , mip ( a2 ) ed immagini transassiali ( b2 ) evidenziano una ipercaptazione patologica di fdg nel fegato ( frecce )  . 
pet - 2 ( fov 10 minuti ) , immagini transassiali ( b ) : si evidenzia una ipercaptazione patologica di fdg in ambito epatico . nine liver pathological uptakes ( 11.1% ) were observed only at pet - 2 exam ( table 1 )  . in group a ( n = 31 ) , we observed 28 lesions in 15 patients at pet - 1 and 33 lesions in 16 patients at pet - 2 . 
in group c ( n = 27 ) , we observed 23 lesions in ten patients at pet - 1 and 25 lesions in ten patients at pet - 2 . semiquantitative analysis lesions ( n = 90 )  . 
nel gruppo c ( n = 27 ) abbiamo riscontrato 23 lesioni in 10 pazienti , in pet - 1 e 25 lesioni in 10 pazienti , in pet - 2 . analisi semi - quantitativa lesioni ( n = 90 )  . 
 radiol med ( 2008 ) 113 : 875886 table 1 number of liver pathological uptakes per patient at positron emission tomography ( pet ) - 1 and pet - 2 study number of liver pathological uptakes number of patients ( pet - 1 scan ) number of patients ( pet - 2 scan ) tabella 1 distribuzione delle lesioni epatiche evidenziate allesame pet - 1 e pet - 2 nella popolazione di pazienti studiata numero di up - takes patologici del fegato numero di pazienti ( scansione pet - 1 ) numero di pazienti ( scansione pet - 2 ) l / bg1 ratio , meansd was 2.101.24 ; l / bg2 ratio 2.641.53 ( p < 0.001 , wilcoxon test )  . 
in the group of patients with primary colorectal adenocarcinoma ( n = 42 ) , we observed 58 liver lesions at both pet - 1 and pet - 2 studies and further six liver pathological uptakes ( 10.3% ) at pet - 2 . in the remaining patients ( n = 53 ) , we observed 23 liver lesions at both pet studies and a further three liver pathological uptakes ( 13% ) at pet - 2 scan . 
nel gruppo dei pazienti con adenocarcinoma primitivo del colon - retto ( n = 42 ) abbiamo riscontrato 58 lesioni epatiche in entrambi gli esami pet - 1 e pet - 2 , e ulteriori 6 accumuli patologici epatici ( 10 , 3% ) allesame pet - 2 ; nei rimanenti pazienti ( n = 53 ) , abbiamo riscontrato 23 lesioni epatiche in entrambi gli esami pet e 3 ulteriori accumuli epatici nella pet - 2 ( 13% )  . 
infine , non abbiamo trovato una correlazione tra bmi e delta bg - suvmedio ( r = 0 , 0026 ) , bmi e delta rapporto lesione / fondo ( r = 0 , 0004 ) , glicemia e delta bg - suvmedio ( r = 0 , 0002 ) , glicemia e delta rapporto lesione / fondo ( r = 0 , 0026 )  . discussione lesame pet total body viene normalmente acquisito 1 ora dopo la somministrazione di fdg . 
questo sembra infatti il miglior compromesso tra la fissazione di radiofarmaco nelle cellule tumorali ( visualizzazione del tumore ) e lemivita effettiva dello stesso radiofarmaco ( che rappresenta la quantit di tracciante radioattivo ancora presente al momento dellacquisizione dellesame emissivo pet ; quantit che peraltro influenza significativamente il tempo di durata di ogni fov necessario per ottenere immagini di buona qualit )  . 
 [ 15 ] on 22 patients , the delayed acquisition of pet emission data ( 2 h after the radiotracer injection ) led to an increase of the tumour / background ratio and a better qualitative evaluation of pet images . 
in particular , progressive reduction of kidney and liver background uptakes , due to the tracer wash - out , allowed better visualisation of lesions in the abdomen [ 15 ]  . 
 [ 15 ] con lacquisizione di immagini tardive ( 2 ore dopo la somministrazione del tracciante ) hanno evidenziato , in un gruppo di 22 pazienti , un incremento del rapporto lesione / fondo ed una conseguente migliore valutazione qualitativa delle immagini pet ottenute . 
nel loro lavoro gli autori evidenziavano come nel tempo si avesse una progressiva riduzione del fondo a livello renale ed epatico ( dovuta al wash - out del radiotracciante ) con migliore visualizzazione dei quadranti addominali superiori [ 15 ]  . 
 [ 18 ] hanno utilizzato un protocollo di acquisizione in due fasi ( precoce a 70 minuti , tardiva a 98 minuti ) , nel tentativo di differenziare le fissazioni dovute a neoplasia da quelle di tipo infiammatorio nella regione della testa - collo . 
in a study on 36 patients with suspected lung nodules ; in that study , lesions suv increased from 3.661.95 in the early to 4.432.43 in the delayed acquisition [ 19 ]  . 
 [ 20 ] studied 15 patients with liver tumours ( 11 with hepatocarcinoma and four with hepatic metastases from colorectal carcinoma ) with a dual - phase pet protocol ( 1 and 2 h post - fdg injection )  . 
the authors concluded that even though in patients with hepatocarcinoma the delayed pet acquisition did not bring any benefits ( probably due to the similar fdg metabolism in well - differentiated hepatocarcinoma and in normal liver tissue [ 20 , 21 ] ) , delayed images proved useful in patients with liver metastases from colorectal cancer [ 22 ]  . 
 [ 23 ] studied the utility of pet in 86 patients with suspected pancreatic cancer acquiring early ( 1 h postinjection ) and delayed ( 2 h postinjection ) pet scans . 
moreover , the delayed pet scan enabled identification of further liver metastases [ 23 ]  . our results are in agreement with these previous experiences and based on well - known metabolic processes . 
the level of glucose - 6 - phosphatase ( the enzyme that transforms the fdg - 6 - phosphate in fdg ) is high in the liver [ 22 , 24 ]  . this enzyme , during the time , determines a progressive wash - out of fdg from the hepatocyte . 
this leads to a continuous increase of fdg in tumour tissue [ 17 ]  . based on these facts , lesion maximum and mean suv were higher in the pet - 2 exam in respect to pet - 1 . 
 to the best of our knowledge , this is the first time that the problem of pet sensitivity in detecting liver pathological uptakes has been investigated and that a possible solution to improve its sensitivity has been suggested . 
however , as expected , when the pet - 2 duration of data acquisition per bed position was 5 or 10 min ( instead of 3.5 ) , we obtained the best qualitative and semiquantitative results ( that is , delta ratio group a = 21.7% , group b = 24.2% , group c = 16.1% ; due to the minor differences between results of group a and b , we can consider the duration of 5 min for data acquisition per bed position as the most appropriate in clinical practice )  . gliore valutazione delle immagini pet [ 18 ]  . 
 [ 19 ] hanno ottenuto risultati simili ; in questo studio il valore di suv delle lesioni mostrava un aumento da 3 , 661 , 95 nelle acquisizioni precoci , a 4 , 432 , 43 in quelle tardive . 
 [ 20 ] hanno studiato 15 pazienti con neoplasie a livello epatico ( 11 con epatocarcinoma e 4 con metastasi epatiche da carcinoma del retto ) con acquisizione dellesame pet in due fasi ( 1 e 2 ore dopo la somministrazione di fdg ) , concludendo che le immagini tardive , nei pazienti con epatocarcinoma , non portano nessun beneficio ( questo risultato va probabilmente imputato al fatto che il metabolismo tumorale simile nellepatocarcinoma ben differenziato a quello del tessuto epatico sano [ 20 , 21 ] ) , mentre le acquisizioni tardive miglioravano la visualizzazione delle metastasi epatiche nei pazienti con carcinoma del retto [ 22 ]  . 
 [ 23 ] hanno utilizzato un protocollo che prevedeva lacquisizione precoce e tardiva ( 1 e 2 ore dopo la somministrazione ) in un gruppo di 86 pazienti con lesioni pancreatiche di sospetta natura neoplastica . 
in questo studio , il valore di suvmedio delle lesioni neoplastiche nelle acquisizioni tardive mostrava un aumento molto significativo e le immagini tardive evidenziavano localizzazioni epatiche non visibili nelle precoci [ 23 ]  . i risultati del nostro studio concordano con quelli dei lavori citati . 
la spiegazione si basa su processi metabolici noti : il livello della glucoso - 6 - fosfatasi ( lenzima che catalizza la trasformazione di fdg - 6 - fosfato in fdg ) nel fegato elevato [ 22 , 24 ] e determina , nel tempo , un progressivo wash - out di fdg da parte degli epatociti , con conseguente riduzione dei valori di suvmedio epatico ( fondo ) tra lacquisizione precoce e quella tardiva . 
viceversa , lo stesso enzima quasi totalmente assente nelle cellule tumorali metastatiche [ 22 , 25 ] ; questo spiega il continuo incremento di fdg nei tessuti neoplastici [ 17 ] e dunque laumento dei valori di suvmax e suvmedio tra pet - 1 e pet - 2 . nel presente lavoro stato affrontato il problema della bassa sensibilit dellesame pet nellidentificazione di accumuli patologici a livello epatico ed stato verificato se la riacquisizione di immagini tardive poteva rappresentare una realistica soluzione . 
i nostri risultati hanno dimostrato che lacquisizione tardiva a livello epatico , migliora la valutazione delle immagini sia qualitativamente ( sono stati identificati 90 e 81 accumuli patologici di fdg , rispettivamente negli esami pet - 2 e pet - 1 ) che semi - quantitativamente ( delta rapporto lesione / fondo 20 , 7% )  . 
tuttavia , in considerazione delle non significative differenze tra i risultati del gruppo a e b , la riacquisizione con fov di 5 minuti risulta la pi vantaggiosa nella pratica clinica quotidiana . basandoci su questi risultati , possiamo ipotizzare due diverse conseguenze nella routine clinica . 
firstly , the case of patients with suspected liver metastases : if the wholebody fdg - pet study acquired one h after the radiotracer injection is negative , a delayed acquisition at the upper abdominal level should be repeated to exclude the presence of disease ( in our patient population , at pet - 2 , two out of the 58 cases negative at pet - 1 showed a liver pathological uptake )  . 
secondly , timing of fdg - pet acquisition : if we consider our and previous findings , it is unequivocal that delayed acquisition is better than the earlier one , with distinct advantages in detection and visualisation of fdg pathological uptakes , and not only in the liver parenchyma . 
se lesame fdg - pet total body risulta negativo dopo acquisizione standard , opportuno ripetere una seconda acquisizione delle immagini in fase tardiva a livello delladdome superiore onde escludere la presenza di malattia ( nella nostra casistica 2 dei 58 pazienti negativi in pet - 1 diventavano positivi nellesame pet - 2 )  . 
dai nostri risultati ma anche da quelli degli studi precedentemente effettuati , risulta infatti chiaro che lacquisizione tardiva migliore di quella precoce , con vantaggi nellidentificazione e nella valutazione degli accumuli patologici di fdg , non soltanto nel parenchima epatico . 
per questo motivo , lintervallo migliore tra la somministrazione del tracciante e lacquisizione delle immagini pet potrebbe essere quello di 2 ore . study limitations limiti dello studio this study shows some limitations . 
therefore , we can conclude that delayed acquisition improves visualisation of fdg pathological uptake with respect to early acquisition , but we cannot state that delayed acquisition improves visualisation of metastases . 
however , considering that the common behaviour of tumour and inflammatory lesions is different and that none of the patients referred to our pet centre had received liver treatment in the previous 3 months or presented suspicious inflammatory lesions in the liver parenchyma , it is reasonable to conclude that all pathological uptakes were liver metastases . 
secondly , the study was performed with a discovery st scanner , acquiring pet emission data in the 3d mode ; these results need further confirmation when using the 2d acquisition mode . 
primo , come dichiarato nel nostro obiettivo , stato eseguito col solo scopo di migliorare lidentificazione di accumuli patologici di fdg a livello epatico ; dunque , la maggior parte delle lesioni identificate non sono state ulteriormente indagate . 
conseguentemente possiamo concludere che lacquisizione di immagini emissive tardive migliora la visualizzazione di accumuli epatici patologici rispetto a quella precoce , ma non possiamo dimostrare che lacquisizione tardiva migliora lidentificazione delle metastasi . 
tuttavia , considerando il diverso comportamento metabolico delle lesioni neoplastiche e di quelle infiammatorie ( normalmente in accumulo le prime , in wash - out le altre ) e considerando che nessuno dei pazienti inclusi in questa casistica aveva subito alcuna terapia nei tre mesi precedenti n presentava alcuna patologia infiammatoria nota a livello epatico , altamente probabile che le lesioni visualizzate fossero metastasi . 
tuttavia opportuno sottolineare che allo stato attuale lacquisizione in modalit 3d lunica possibile per i tomografi pet di philips e siemens ; ge viceversa lunico produttore che commercializza uno scanner ancora in grado di acquisire sia in modalit 2d che 3d , ma nella maggior parte dei centri , compreso il nostro , gli esami vengono acquisiti in modalit 3d . 
 conclusions conclusioni our data demonstrate that by acquiring a delayed pet scan of the upper abdomen , both a better visualisation of liver pathological uptake and an increase in pet sensitivity are achieved . 
these results are strongly related to the reduction of suvmean values in the background and with the concomitant increase of suvmean values of the lesion itself , with a final significant gain of the lesion - to - background ratio . 
therefore , our suggestion is that in patients with clinii nostri dati dimostrano che lacquisizione di immagini pet tardive delladdome superiore favorisce la visualizzazione di accumuli patologici di fdg a livello epatico aumentando la sensibilit dellesame pet . 
questi risultati sono significativamente correlati con la riduzione dei valori del fondo a livello epatico e con il concomitante incremento dei valori di suvmedio della lesione stessa , con significativo incremento del rapporto lesione / fondo . 
perci , la nostra conclusione 886 radiol med ( 2008 ) 113 : 875886 cally suspected liver metastases , when the standard pet scan is negative , a delayed pet study of the upper abdomen should be acquired to improve the sensitivity of the technique . 
 che nei pazienti con sospetto clinico di metastasi epatiche , quando lesame pet standard risulta negativo , dovrebbe essere effettuata una riacquisizione tardiva delladdome superiore per migliorare la sensibilit dello studio . 
inoltre , lintervallo tra iniezione e acquisizione delle immagini emissive pet dovrebbe essere rivalutato , e lacquisizione di immagini pet a due ore dalla somministrazione di fdg dovrebbe essere presa in considerazione nella routine clinica . the experiment complies with the current laws of italy , where it was performed and was approved by the ethics committee . il presente lavoro stato eseguito in attemperanza con le norme italiane in materia ed stato approvato dal comitato etico . growth of the pediatric skeleton . 
oestreich springer verlag , berlin , heidelberg , new york , 2008 isbn 978 - 3 - 540 - 37688 - 0 published online : 22 september 2008 springer - verlag 2008 this is a very unusual at least from a radiologist point of view small book . 
instead , drawings represent bones : their normal shape , how they develop , and how they change over time due to physiologic growth or to disease congenital or acquired . oestreichs goal was to share with the reader the expertise he has gained over many years of studying the growing skeleton . 
this primer is intended to acquaint the reader with all the conundrums that must be learnt and acquired before gaining expert diagnostic skill in this field . terms such as periphysis , bone bark , acrophysis and paraphysis are to be well digested , as they are clues for clear understanding of the text . 
oestreich , nella stesura del testo , era di mettere a disposizione del lettore lesperienza da lui maturata nel corso di lunghi anni di studio dello scheletro in via di crescita e questo manualetto / bigino ha proprio lo scopo di rendere edotto il lettore di tutte le problematiche e gli enigmi che debbono essere affrontati e giustamente appresi prima di poter raggiungere una capacit diagnostica corretta in tale campo . termini come periphysis , bone bark , acrophysis , paraphysis devono essere ben digeriti dal momento che sono la chiave per il corretto apprendimento di quanto scritto nel testo . 
da tener presente inoltre i riferimenti alla genetica di fronte a termine come ox genes e simili . le pagine del testo sono 92 , divise in 16 capitoli , tutti piuttosto concisi e che trattano dei differenti aspetti dellosso , dal tipo di formazione dello stesso ( encondrale e membranoso ) allo sviluppo prenatale , alla colonna vertebrale , le esostosi e gli encondromi , le malattie metaboliche , le displasie e le disostosi , le artriti e le malattie associate , i ritardi o laccelerazione della crescita encondrale , la concatenazione dei rapporti spaziali , la regola dei 10 giorni , le ossa pari e curve , le anomalie dellallineamento e le caratteristiche ossee specifiche di ossa specifiche . nel leggere il testo netta la sensazione di sentire la voce dellautore ( per lo meno per chi lo conosce ) mettere in evidenza particolari punti secondo il suo modo di vedere ed affrontare determinati problemi : come messo in chiaro e ben spiegato dai disegni preparati dallabilit artistica della moglie . dal momento che si tratta di un manualetto , il lettore non trover nello stesso tutti i possibili dettagli e sottigliez942 radiol med ( 2008 ) 113 : 941942 extended x - ray books dealing with the topic ; surely , however , this book will stimulate thoughts and meditation concerning the subject matter . 
 given its price and the valuable information to be found in it , this book is warmly recommended for the libraries of radiology departments and the property of trainees in radiology and orthopaedics . ze ritrovabili nei testi radiologici classici riguardanti largomento . 
simonetti dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e terapia radiante , policlinico universitario tor vergata ( ptv ) , viale oxford 81 , 00133 , roma , italy correspondence to : t . 
in 47 patients , a total of 47 suspicious breast lesions ( mean maximum diameter 9 mm ) seen with mri ( no suspicious changes on breast ultrasound or mammography ) were sampled using a 10 - gauge vacuum - assisted breast biopsy ( vab ) device under mri guidance . 
technical success was achieved in all biopsies . histological results from vab revealed malignancy in 15 lesions ( 32% ) , atypical ductal hyperplasia in four lesions ( 8% ) and benign findings in 28 lesions ( 60% )  . 
47 lesioni ( diametro massimo 9 mm ) visibili unicamente allesame rm , sono state caratterizzate usando un sistema portatile ad aspirazione retroazionata ( vab ) con ago da 10 gauge , sotto guida rm . 
i risultati istologici della biopsia vab hanno mostrato 15 lesioni maligne ( 32% ) , 4 lesioni classificabili come iperplasia duttale atipica ( adh ) ( 8% ) , e 28 lesioni come benigne ( 60% )  . 
alla istologia definitiva una delle quattro lesioni classificate come adh stata riclassificata come carcinoma duttale in situ ( dcis ) , mentre una delle lesioni classificate come dcis stata riclassificata come carcinoma invasivo . 
due lesioni benigne che allimaging rm hanno mostrato una modificazione della morfologia , sono andate incontro ad intervento chirurgico che ha confermato la benignit della lesione . ad eccezione di un massivo sanguinamento in 1 caso , non si sono osservate complicanze . 
 metodica sicura ed efficace per la caratterizzazione delle lesioni mammarie visibili unicamente allrm . keywords magnetic resonance breast carcinoma vacuum - assisted breast biopsy ( vab ) parole chiave risonanza magnetica carcinoma mammario sistema di biopsia vab introduction introduzione over the past 15 years , magnetic resonance imaging ( mri ) of the breast has taken on an important role as an adjunct to conventional imaging modalities in the early detection of breast cancer . 
although mri has high sensitivity , its specificity is relatively low ( 37%97% ) [ 3 ]  . the number of lesions identified at mri alone has led to a need to develop mri - guided interventional procedures enabling correct characterisation of lesions . 
 recent technological innovations have made it possible to perform minimally invasive diagnostic procedures such as core needle biopsy ( cnb ) and vacuum - assisted biopsy ( vab ) , even under mri guidance [ 46 ]  . 
the aim of our study was to evaluate the accuracy and complications of mri - guided 10 - gauge vab in the characterisation of nonpalpable breast lesions visible with mri only . materials and methods patients between january 2003 and january 2006 , 47 mri - detected breast lesions ( mean maximum diameter 9 mm ; range 412 mm ) in 47 women ( mean age 54 ; age range 3073 ) were histologically characterised with mri - guided vab . 
all patients were studied by mammography ( mx ) , ultrasound ( us ) , and mri with paramagnetic contrast material [ gadolinium diethylene triaminopentoacetic acid ( dtpa ) ]  . they also underwent blood testing to assess coagulation profiles and electrocardiography . 
the clinical indications for mri were detection of additional malignant foci in 24 patients undergoing surgery for suspicious mx and us findings , assessment of the surgical scar in ten patients who had undergone surgery for malignant disease , detection of mamnegli ultimi quindici anni la risonanza magnetica ( rm ) della mammella ha assunto un ruolo fondamentale quale indagine diagnostica complementare allimaging convenzionale nella diagnosi precoce del carcinoma mammario . 
il suo utilizzo consente di evidenziare lesioni non altrimenti apprezzabili alle indagini convenzionali mammografiche ed ecografiche in una percentuale di casi di circa il 20% [ 1 , 2 ]  . sebbene la rm abbia una elevata sensibilit tuttavia a tuttoggi la sua specificit non pu essere considerata altrettanto soddisfacente ( 37%97% ) [ 3 ]  . 
 le recenti innovazioni tecnologiche hanno permesso con successo lesecuzione delle strategie diagnostiche mininvasive quali la core needle biopsy ( cnb ) e le biopsie con sistema ad aspirazione retroazionata ( vab ) anche sotto guida rm [ 46 ]  . 
obiettivo del nostro studio stato quello di valutare laccuratezza e le complicanze della procedura vab 10 gauge sotto guida rm nella caratterizzazione delle lesioni non palpabili della mammella visibili unicamente alla rm . materiali e metodi pazienti dal gennaio 2003 al gennaio 2006 , sono state sottoposte a caratterizzazione istologica mediante prelievo vab sottoguida rm 47 lesioni ( diametro massimo medio 9 mm ; range 412 mm ) visibili unicamente alla rm presenti in 47 pazienti di et compresa da 30 a 73 anni ( et media 54 anni )  . 
tutte le pazienti hanno effettuato un esame mammografico ( mx ) , 832 radiol med ( 2008 ) 113 : 830840 mographically and sonographically occult breast cancer in five patients with metastatic lymph nodes [ carcinoma with unknown primary tumour ( cup ) syndrome ] , and in the remaining eight cases , mri was used as a follow - up in patients with a strong family history of breast cancer . 
if the lesions were visible on second - look us , the patients were excluded from the study , and the lesions were sampled under us guidance , as the procedure is less expensive and generally simpler and faster . 
further exclusion criteria were the presence of major changes in coagulation parameters , breast implants or ineligibility for the mri study ( pacemakers , claustrophobia ) or superficial lesions in the inner quadrants . magnetic resonance imaging all mri studies were carried out on a 1.5 - t intera mri system ( philips medical systems , best , the netherlands )  . 
lesion coordinates were calculated by acquiring only axial t2 sequences if the lesion was easily identifiable even without contrast administration ; otherwise , dynamic axial t1 sequences were acquired ( tr 300 ms ; te 4.3 ms ; flip angle 90 ; fov 240 ; rfov , 80% ; matrix 256512 ; scan percentage 70% ; nsa 1 ; slice thickness 3 mm ) before and after the intravenous administration of 0.2 mmol gd - dtpa / kg at a rate of 2 ml / s , followed by 20 ml of saline solution ; four dynamic sequences lasting 70 s each . 
correct positioning of the external fiducial marker and coaxial introducer was checked with the acquisition of either dynamic t1 sequences or , for lesions identifiable even without contrast administration , axial t2 sequences . mri - compatible stereotactic system the procedure was carried out using a dedicated mri - compatible stereotactic system ( philips medical systems , the netherlands )  . 
this system consists of a breast support that keeps the patient in a semiprone position tilted 20 with respect to the horizontal plane and two 20 - mm - thick compression plates , one internal and one external , used to immobilise the breast . 
the external plate has an add - on mri - visible fiducial system consisting of two crossed horizontal and vertical markers , which is used to calculate lesion coordinates and select the appropriate entry hole and penetration depth of the needle . ecografico ( eco ) e la risonanza magnetica ( rm ) con mezzo di contrasto paramagnetico ( gadolinio - dtpa )  . 
la rm stata richiesta in 24 casi per la ricerca di foci maligni addizionali in pazienti candidate allintervento chirurgico per patologia maligna sospetta allimaging mammo - ecografico ; in 10 casi per una corretta valutazione della cicatrice chirurgica in pazienti gi sottoposte ad intervento chirurgico per patologia maligna ; in 5 casi per ricerca di focolai di carcinoma mammario occulto in pazienti con linfonodi positivi per metastasi da carcinoma mammario senza evidenza di lesioni primitive allesame mammografico ed ecografico ( cup syndrome ) ; nei rimanenti 8 casi la rm stata eseguita come esame di follow - up in pazienti con familiarit per carcinoma mammario . 
nei casi in cui venivano identificate una o pi lesioni alla risonanza magnetica , sono stati valutati retrospettivamente gli esami mammografici ed ecografici ed stato ripetuto un esame ecografico mirato ( second look ) alla ricerca del reperti evidenziati . sono state escluse dallo studio le pazienti nelle quali il second - look ecografico , ha permesso lindividuazione della lesione . 
ulteriori criteri di esclusione dallo studio sono stati la presenza di importanti alterazioni del profilo di coagulazione del sangue , la presenza di protesi mammarie o la impossibilit da parte delle pazienti di eseguire lesame rm ( presenza di pace - maker , claustrofobia ) o lesioni localizzate nei quadranti interni in sede superficiale . risonanza magnetica tutti gli esami rm sono stati effettuati con sistema rm intera 1 , 5 ( philips medical systems , best , olanda )  . 
per il calcolo delle coordinate spaziali della lesione sono state acquisite solo sequenze t2 assiali nel caso in cui la lesione fosse ben visibile anche in assenza di somministrazione di mezzo di contrasto , nel caso contrario , sono state eseguite sequenze t1 assiali dinamiche ( tr 300 ms ; te 4 , 3 ms ; flip angle 90 ; fov 240 ; rfov , 80% ; matrice 256512 ; scan percentage 70% ; nsa 1 ; spessore di strato di 3 mm ) prima e dopo somministrazione di 0 , 2 mmol gd - dtpa / kg endovena con flusso pari a 2 ml / s , seguite da 20 ml di soluzione salina ; quattro dinamiche della durata di 70 secondi per singola dinamica . 
per la valutazione del corretto posizionamento del fiducial esterno e dellintroduttore coassiale sono state eseguite o sequenze t1 dinamiche , oppure sequenze t2 assiali in tutti i casi in cui la lesione era ben identificabile anche in assenza di enhancement . radiol med ( 2008 ) 113 : 830840 sistema stereotassico dedicato rm compatibile per effettuare la procedura rm stato utilizzato un sistema stereotassico dedicato rm compatibile ( philips medical systems , olanda )  . 
tale sistema costituito da un supporto per lalloggiamento del seno , che sostiene la paziente in posizione semiprona , con una inclinazione di 20 rispetto al piano orizzontale , e da due piatti di compressione di 20 mm di spessore , utilizzati per immobilizzare la mammella , uno interno e laltro esterno . 
il piatto esterno dotato di due markers rimovibili , rm visibili , uno orizzontale e laltro verticale , disposti a croce , utilizzati come riferimento per il calcolo delle coordinate spaziali della lesione , necessarie per stabilire il foro di ingresso dellago e la profondit alla quale deve essere inserito . 
this is a handheld electromechanical device for vab capable of generating vacuum through an electric motor controlled by a microprocessor and powered by a lithium - ion battery ( 7.2 volts ) and controlled through an integrated touch pad . 
tale sistema un dispositivo elettromeccanico per biopsia sotto vuoto che pu essere utilizzato come dispositivo palmare , capace di generare vuoto a pressione attraverso un motore elettrico dotato di un microprocessore e alimentato da una batteria al litio ( 7 , 2 volts ) , controllato da una tastiera integrata a sfioramento . 
2 sistema portatile vab vacora con sonda coassiale 10 g . 834 radiol med ( 2008 ) 113 : 830840 cannula esterna ruota e avanza sopra la camera di campionamento per tagliare il campione di tessuto . 
nel caso di mammelle piccole o nel caso di lesioni superficiali stato utilizzato uno spaziatore di 10 mm , posizionato tra lazionatore e la sonda per ridurre la lunghezza della camera di campionamento da 20 mm a 10 mper le lesioni localizzate ad una profondit maggiore di 5 cm sono state utilizzate sonde lunghe ( 140 mm )  . procedura prima di effettuare il prelievo da tutte le pazienti stato ottenuto consenso informato alla procedura . 
a tal fine sono state acquisite o sequenze t1 assiali prima e dopo somministrazione di mezzo di contrasto , o sequenze t2 assiali , qualora la lesione fosse ben identificabile anche in assenza di enhancement , come descritto nel paragrafo risonanza magnetica nella sezione materiali e metodi . 
il calcolo delle coordinate spaziali in direzione anteroposteriore , cranio - caudale e latero - mediale ( profondit ) , utilizzando come riferimenti i markers a croce posti sulla piastra esterna stato effettuato come gi descritto in letteratura [ 7 ]  . 
una volta stabilito il foro di ingresso della sonda , stato preliminarmente posizionato un fiducial esterno il cui corretto posizionamento rispetto alla lesione stato valutato eseguendo o una sequenza t1 assiale dinamica o una sequenza t2 assiale qualora la lesione fosse chiaramente identificabile anche in assenza di mezzo di contrasto . 
si proceduto al successivo inserimento dellintroduttore coassiale , composto da una cannula in plastica e da un madrino in titanio , previa anestesia cutanea ( 10 cc di lidocaina cloridrato diluita al 2% ) e incisione con bisturi oftalmico ( v - lance knife , alcon surgical ) al fine di agevolarne lentrata . 
when sampling small breasts or superficial lesions , a 10 - mm spacer was placed between the drive and the probe to shorten the sample window from 20 mm to 10 m for lesions located deeper than 5 cm , we used long probes ( 140 mm )  . 
this was accomplished either with axial t1 sequences before and after contrast administration or with axial t2 sequences if the lesion was identified even without contrast administration . calculation of the spatial coordinates in the anteroposterior , craniocaudal and lateromedial ( depth ) direction was carried out using the crossed markers as references , as previously described [ 7 ]  . 
4 calcolo della profondit dellintroduttore coassiale , misurata in funzione della profondit della lesione e della lunghezza della camera di campionamento della sonda utilizzata ( 20 mm o 10 mm ) in modo da far s che la lesione si trovi sempre al centro della camera di prelievo . 
per gentile concessione della bard , biopsy systems , tempe , fl , usa . the probe , an external fiducial marker was positioned , and its correct location relative to the lesion was verified with a dynamic axial t1 sequence or an axial t2 sequence if the lesion could be identified even without contrast administration . 
the coaxial introducer , consisting of the plastic cannula and titanium stylet , was then inserted after the skin had been anaesthetised ( 10 cc of lidocaine hydrochloride 2% ) and a small incision had been made with an ophthalmic scalpel ( v - lance knife , alcon surgical ) to facilitate entry of the introducer . 
twelve core specimens were then retrieved in all patients with the exception of two in whom eight samples were retrieved because of bleeding . in 35 out of 47 patients , a titanium clip was deployed at the biopsy site ( mammo - mark biopsy site marker ; artemis medical , hayward , ca , usa )  . 
no clip was deployed when the location of a positive lesion would have changed surgical planning from quadrantectomy to mastectomy ( six cases ) , in cases of massive bleeding ( two cases ) , patient refusal ( three cases ) and technical difficulties ( four cases )  . 
successivamente , stato rimosso il mandrino della cannula coassiale ruotandolo in senso antiorario ed stata inserita la sonda . sono stati quindi prelevati 12 frustoli in tutti i casi ad eccezione di 2 pazienti in cui ne sono stati prelevati 8 a causa del sanguinamento . in 35 pazienti su 47 stata rilasciata una clip in titanio ( mammo - mark biopsy site marker , artemis medical , hayward , california ) nella sede di biopsia . 
la clip non stata posizionata quando la positivit della lesione , in virt della sua localizzazione avrebbe comunque cambiato il planning chirurgico da quadrantectomia a mastectomia ( 6 casi ) , in caso di abbondante sanguinamento ( 2 casi ) , rifiuto della paziente ( 3 casi ) e difficolt tecnica da parte delloperatore ( 4 casi )  . 
nel nostro studio , al termine della procedura , abbiamo scelto di non effettuare il controllo rm postprocedura nellimmediato , ma di procedere alla subitanea compressione della mammella per 10 minuti ed alla successiva fasciatura compressiva . 
la biopsia escissionale di tutte le lesioni diagnosticate come maligne o come iperplasia duttale atipica ( adh ) stata eseguita a circa 1 settimana dalla procedura bioptica e la diagnosi istologica definitiva stata confrontata con quella ottenuta con il vab . 
5a - d a 57 - year - old woman with biopsy - proven cancer in the right breast shows a suspicious mass on magnetic resonance imaging ( mri ) of the left breast . 
axial t1 - weighted image of left breast shows a suspicious mass measuring 0.8 cm in the upper - inner quadrant ( arrow ) : a before gadolinium injection , b after gadolinium injection . 
c axial t2 - weighted image obtained with the patient in the semiprone position and compression of the left breast : the suspicious mass is well visible in the upper - inner quadrant ( arrow )  . 
immagine t1 assiale diagnostica prima ( a ) e dopo somministrazione ev di gadolinio ( b ) mostra la lesione sospetta di 0 , 8 cm localizzata al quadrante supero interno ( freccia )  . 
d dopo il posizionamento dellintroduttore coassiale : lestremit distale della cannula coassiale si trova a 10 mm prossimalmente dal centro della lesione ( testa di freccia )  . study , we decided not to perform postprocedural mri immediately after the procedure but rather to compress the breast for 10 min and apply a compressive bandage . 
excisional biopsy of all lesions diagnosed as malignant or as atypical ductal hyperplasia ( adh ) was carried out approximately 1 week after biopsy , and the final histological diagnosis was compared with that obtained with vab . 
the benignity of lesions classified as benign with vab was confirmed by evidence of stable findings at follow - up mri after 12 or 24 months ( mean follow - up , 18 months ) or by final histological diagnosis in the case of lesions showing morphological or dimensional changes in the area of residual enhancement at follow - up . classificate come benigne con il prelievo vab si basata sulla valutazione della stabilit del reperto rm ai successivi controlli rm eseguiti a distanza di 12 o 24 mesi ( followup medio , 18 mesi ) o sul riscontro istologico definitivo nel caso in cui fossero evidenziati dei cambiamenti morfologici o dimensionali dellarea di enhancement residua ai controlli di follow - up . risultati in tutti i casi le procedure bioptiche sono state portate a termine con successo . 
sono stati prelevati 12 frustoli di tessuto in 45 / 47 pazienti , nei rimanenti casi ( 2 / 47 ) sono stati prelevati 8 frustoli in quanto la procedura stata sospesa per radiol med ( 2008 ) 113 : 830840 results all biopsy procedures were successfully completed . 
the histological diagnosis provided by vab ( table 1 ) was malignancy in 15 / 47 lesions ( 32% ) [ eight invasive ductal carcinomas and seven ductal carcinomas in situ ( dcis ) ] , benignity in 28 / 47 lesions ( 60% ) ( six cases of adenosis , five of fibroadenoma , one papilloma and 16 of fibrocystic disease ) and atypical ductal hyperplasia in 4 / 47 cases ( 8% )  . 
for two lesions diagnosed at vab as invasive carcinoma smaller than 5 mm , definitive histological validation could not be obtained because of complete lesion removal during the vab procedure ( table 2 )  . 
one of the seven lesions diagnosed as dcis at vab was upgraded to invasive carcinoma by definitive histology ; one of the four lesions diagnosed as adh at vab was upgraded to dcis by definitive histology ( table 2 )  . 
of patients tabella 1 diagnosi istologica dei prelievi vab effettuati sotto guida rm diagnosi istologica n pazienti benign lesions fibrocystic disease adenosis fibroadenoma papilloma malignant lesions invasive ductal carcinoma ductal carcinoma in situ atypical ductal hyperplasia total lesions vab , vacuum - assisted biopsies lesioni benigne malattia fibrocistica adenosi fibroadenoma papilloma lesioni maligne carcinoma duttale infiltrante carcinoma duttale in situ iperplasia duttale atipica totale lesioni vab , vacuum assisted biopsy 28 ( 60% ) 15 ( 32% ) 4 ( 8% ) 28 ( 60% ) 15 ( 32% ) 4 ( 8% ) sanguinamento . 
la diagnosi istologica al prelievo vab ( tabella 1 ) stata in 15 / 47 lesioni ( 32% ) di malignit ( 8 carcinomi duttali infiltranti e 7 carcinomi duttali in situ ) ; in 28 / 47 lesioni ( 60% ) di benignit ( 6 casi di adenosi , 5 di fibroadenomi ; 1 papilloma e 16 casi di malattia fibrocistica ) ; in 4 / 47 casi ( 8% ) stata diagnosticata iperplasia duttale atipica . 
in tutti i casi di lesioni caratterizzate come maligne o come iperplasia duttale atipica al vab si proceduto a biopsia escissionale chirurgica . tutte le lesioni diagnosticate con il vab come carcinomi infiltranti sono state confermate allistologico definitivo ( tabella 2 )  . 
per due casi diagnosticati al vab come carcinoma infiltrante delle dimensioni inferiori ai 5 mm non stato possibile avere un riscontro allistologico definitivo , in quanto le lesioni sono state totalmente asportate durante la procedura vab ( tabella 2 )  . 
una delle 7 lesioni diagnosticate con il vab come carcinoma in situ stata caratterizzata come carcinoma infiltrante alla valutazione istologica definitiva ; uno dei 4 casi diagnosticato come iperplasia atipica con il vab stato classificato come carcinoma duttale in situ allistologico definitivo ( tabella 2 )  . 
il successivo follow - up rm a 12 e 24 mesi ( follow - up medio , 18 mesi ) delle lesioni diagnosticate come benigne al vab ha confermato lassenza di enhancement negli 8 casi in cui non era pi visibile lenhancement post - procedura e la stabilit degli enhancement residui in 18 / 20 casi . 
dalla nostra esperienza i valori di sensibilit riscontrati della procedura vab sono del 93 , 3% e di specificit del 100% , con un valore predittivo positivo del 100% , valore predittivo negativo del 96 , 7% . 
non abbiamo osservato significative complicanze ad eccezione della presenza di importante sanguinamento in due casi , che si sono risolti con la semplice compressione della mammella . discussion le recenti innovazioni tecnologiche hanno portato alla possibilit di effettuare sotto guida di risonanza magnetica 838 radiol med ( 2008 ) 113 : 830840 table 2 comparison of histopathological diagnoses at vacuum - assisted breast biopsy ( vab ) and at surgery tabella 2 confronto tra diagnosi istologica del vab ( vacuum assisted biopsy ) e dellintervento chirurgico histopathological diagnosis surgery diagnosi istologica chirurgia invasive ductal carcinoma ductal carcinoma in situ atypical ductal hyperplasia carcinoma duttale infiltrante carcinoma duttale in situ iperplasia duttale atipica athe group comprises one case of ducal carcinoma in situ ( dcis ) at vab , which after surgical biopsy was classified as invasive carcinoma ; two cases of invasive carcinoma could not be verified , as they were completely removed with vab ; bthe group comprises one case of atypical hyperplasia at vab , which after surgical biopsy was classified as dcis ail gruppo comprende un caso di ca . 
infiltrante ; 2ca infiltranti non sono stati evidenziati in quanto totalmente asportati con il vab ; bil gruppo comprende un caso di iperplasia atipica allistologico del vab che dopo lescissione chirurgica stato classificato come ca . 
residual enhancement was seen in 20 cases and no enhancement in the remaining eight . mri follow - up at 12 and 24 months ( mean follow - up 18 months ) of benign lesions at vab confirmed the absence of enhancement in the eight cases without residual enhancement and stability of the residual enhancement in 18 / 20 cases . 
there were no significant complications , with the exception of two cases of massive bleeding , both resolved with breast compression . discussion recent technological developments have made it possible to perform effective minimally invasive diagnostic procedures such as cnb and vab under mri guidance . 
however , recent studies reported that 50% of lesions diagnosed as adh at cnb were found to contain areas of dcis , whereas 30% of dcis contained areas of invasive carcinoma [ 8 ]  . 
recent reports have shown that the introduction of new sampling technologies such as vab allows retrieval of larger amounts of tissue compared with cnb , with a consequent reduction in adh and dcis un ( rm ) le nuove efficaci strategie diagnostiche mininvasive quali la core needle biopsy ( cnb ) e le biopsie con sistema ad aspirazione retroazionata ( vab )  . 
tuttavia , recenti studi hanno messo in evidenza che il 50% delle lesioni diagnosticate come iperplasia duttale atipica ( adh ) alla cnb contenevano aree di carcinoma in situ , mentre il 30% dei carcinomi in situ contengono aree di carcinoma infiltrante [ 8 ]  . 
inoltre vi sono dei limiti per lapplicabilit di tale tipologia di prelievo derivante dalle caratteristiche morfologiche ed in particolare dalle dimensioni della lesione che deve essere necessariamente superiore a 78 mm [ 9 , 10 ]  . 
il suo utilizzo su lesioni di dimensioni inferiori a 7 mm aumenta infatti la possibilit di errore correlato al non corretto posizionamento dellago , che pu portare a diagnosi falsamente negative [ 3 , 1214 ]  . 
lesperienza degli ultimi anni ha dimostrato che lintroduzione di una nuova tecnologie di prelievo quale laspirazione retroazionata ( vacuum assisted biopsy , vab ) consente di campionare un volume di tessuto maggiore rispetto alla cnb , con la conseguente riduzione della sottostima delladh e del carcinoma in situ ( 20% per ladh e 30% per il carcinoma in situ ) [ 8 ]  . 
grazie al vab possibile inoltre correggere di qualche millimetro gli errori derivanti dal non idoneo posizionamento dellago , particolarmente importante per la caratterizzazione di lesioni di piccole dimensioni sotto guida rm . 
infatti , labilit del vab di poter acquisire un volume di tessuto maggiore , rispetto alla cnb , e la presenza di aspirazione continua durante il prelievo , possono compensare per eventuali inaccuratezze nel posizionamento dellago [ 15 ]  . 
nella nostra esperienza utilizzando il sistema vab vacora 10 gauge sotto guida rm abbiamo caratterizzato 47 lesioni , di cui il 60% benigne , il 32% maligne e l8% di iperplasia duttale atipica , con una specificit del 100% ed una sensibilit radiol med ( 2008 ) 113 : 830840 derestimation ( 20% for adh and 30% for dcis ) [ 8 ]  . 
the ability of vab to acquire larger volumes of tissue compared with cnb and the presence of continuous suction during the sampling procedure can compensate for possible inaccuracies in needle placement [ 15 ]  . 
in our experience , the use of the 10 - gauge vab vacora system under mri guidance allowed the characterisation of 47 lesions 60% of which were benign , 32% malignant and 8% atypical ductal hyperplasia with a specificity of 100% and sensitivity of 93.7%. in our series , the underestimation rate was 25% for adh and 14% for dcis . 
all lesions characterised as benign ( 28 lesions ) at vab vacora were confirmed to be benign at mri follow - up or definitive histology ( 2 / 28 )  . 
the use of a diagnostic technique such as vab may therefore help to reduce the number of surgical biopsies on patients with benign breast lesions ( approximately 50%60% of all surgical biopsies in italy )  . 
tutte le lesioni caratterizzate al vab vacora come benigne ( 28 lesioni ) sono state confermate come tali al follow - up rm o al riscontro istologico definitivo ( 2 / 28 )  . 
la procedura stata complessivamente ben tollerata da tutte le pazienti che hanno lamentato disagio pi per la posizione obbligata che per il dolore derivante dallintroduzione dellago o dal prelievo stesso . 
infatti una compressione energica pu interferire con lenhancement della lesione nelle sequenze dinamiche , provocandone la mancata visualizzazione ( vanishing target ) e quindi il fallimento della procedura [ 9 , 16 ]  . 
limpiego di una strategia diagnostica come il vab pu quindi ridurre lesecuzione dellintervento chirurgico per le pazienti portatrici di lesioni mammarie benigne ( in italia circa il 50%60% di tutti gli interventi chirurgici ) offrendo la possibilit di affrontare grossi bacini di utenza impiegando minor quantit di risorse interne con notevole abbattimento dei costi di sala operatoria , riduzione del personale impiegato e smaltimento delle liste dattesa . 
 conclusioni conclusions in conclusion , advances in technology and equipment allow us to regard mri - guided vab of lesions visible on mri only as an important innovation in breast diagnostics , capable of significantly enhancing the diagnostic potential of mri by combining a substantial increase in specificity with its well - known high sensitivity . 
such procedures should therefore become increasingly adopted in the clinical practice of high - level breast centres . in conclusione , lottimizzazione della tecnologia e dei materiali impiegati permettono di poter considerare i prelievi vab sotto guida rm per lesioni non identificabili con le metodiche di imaging convenzionali una importante innovazione nel campo della diagnostica senologica , in grado di incrementare significativamente le potenzialit diagnostiche della rm , affiancando alla elevata sensibilit della metodica un notevole incremento della sua specificit . 
the scanning protocol comprised two acquisitions : an electrocardiograph ( ecg ) - gated scan at the level of the heart , followed by a total - body , low - dose scan of the systemic arterial circulation . 
in ten patients , the delay between the two acquisitions was set at 40 s , whereas in the remaining patients , it varied between 45 s and 65 s . 
three hundred coronary segments were analysed . arterial - wall changes were depicted in 155 ( 51% ) segments , and in 35 ( 23% ) , the degree of stenosis was > 50% . 
of the 640 extracoronary arterial segments , 250 ( 39% ) presented atherosclerotic wall alterations , in 50 ( 20% ) , the degree of stenosis was > 50% and five were affected by aneurysmal dilatation . 
ottimizzare un protocollo di scansione con somministrazione bifasica del mezzo di contrasto ( mdc ) per la valutazione angio - tc con scanner a 64 detettori delle arterie coronarie e del circolo arterioso sistemico in un unico esame . 
il protocollo di scansione ha previsto una prima acquisizione con gating cardiaco per lo studio delle coronarie seguita da una scansione total - body a bassa dose per la vascolarizzazione sistemica , utilizzando due iniezioni di mdc . 
sono stati esaminati 20 pazienti utilizzando due differenti strategie di ritardo ( fisso : 40 s , o variabile : 4565 s ) tra prima e seconda somministrazione del mdc . 
per entrambi i protocolli lo studio extracoronarico stato valutato quantitativamente misurando il grado di opacizzazione arteriosa ed il gradiente di attenuazione delle strutture arteriose e venose a 6 differenti livelli . 
le numerose informazioni ottenibili sullo stato globale della patologia aterosclerotica offrono potenzialmente opzioni terapeutiche importanti soprattutto in distretti ad alto rischio , non ancora sintomatici . parole chiave aterosclerosi imaging whole body arterie coronarie arterie extracoronarie circolo sistemico introduction introduzione atherothrombotic disease ( atd ) , a degenerative polyvascular disease affecting largeto medium - size arteries , is the leading cause of mortality and morbidity worldwide [ 15 ]  . the chief clinical presentations of atd are coronary and cerebral ischaemic disease , renovascular hypertension , peripheral arterial occlusive disease of the lower extremities and bowel ischaemia . 
many diagnostic tests are available for evaluating patients with suspected atd , including digital subtraction angiography ( dsa ) , colour - doppler ultrasonography ( us ) , magnetic resonance angiography ( mra ) and computed tomography angiography ( ct angiography )  . 
because of limitations inherent in each of these modalities , for many years , the diagnostic approach to atd has been segmental and targeted to the symptomatic arterial beds despite the systemic nature of the disease . 
amongst noninvasive modalities , ct angiography has the highest diagnostic accuracy in the detection of extracoronary atherosclerotic disease [ 914 ] and has become the standard of reference for studying the coronary vessels before or after endovascular or surgical repair [ 1522 ]  . 
ct scanners with four or 16 detector rows are technically inadequate to provide a comprehensive study ( coronary and extracoronary ) of the entire arterial circulation ( whole body )  . 
however , the recent introduction of 64 - slice ct scanners has enabled extensive anatomical regions to be studied with high spatial resolution and excellent depiction of even the smaller vascular branches , with shorter scanning time and smaller contrast volume [ 2330 ]  . 
 this study was undertaken to optimise the scanning and contrast administration protocol for studying the arteries of la malattia aterotrombotica ( ma ) , intesa come patologia degenerativa con impatto multidistrettuale , interessando i vasi arteriosi di grosso e medio calibro , costituisce la prima causa di mortalit e morbilit nel mondo [ 15 ]  . 
i principali quadri clinici che ne conseguono sono la malattia ischemica coronarica e cerebrale , lipertensione nefrovascolare , larteriopatia ostruttiva degli arti inferiori e lischemia intestinale : in ognuno di questi casi unaccurata classificazione della patologia in termini di localizzazione , estensione e severit appare basilare per un corretto planning terapeutico [ 68 ]  . 
le tecniche diagnostiche disponibili per la valutazione dei pazienti con sospetta ma sono molteplici ed includono langiografia con sottrazione digitale ( dsa ) , leco - colordoppler ( us ) , langiografia con risonanza magnetica ( angio - rm ) e langiografia con tc ( angio - tc )  . 
a causa delle limitazioni intrinseche a ciascuna di queste metodiche , lapproccio diagnostico alla ma rimasto per lungo tempo segmentario mirato , quindi , ai soli distretti arteriosi sintomatici , pur trattandosi di una patologia sistemica . 
tra le metodiche non invasive , langio - tc offre la migliore accuratezza diagnostica per lindividuazione e la caratterizzazione della patologia aterosclerotica extra - coronarica [ 914 ] ed la tecnica di riferimento per lo studio dei vasi coronarici pre e post - trattamento endovascolare o chirurgico [ 1522 ]  . 
gli scanner tc configurati con 4 o 16 strati di detettori , sono tuttavia tecnicamente inadeguati per uno studio integrale ( sia coronarico che extra - coronarico ) dellintero circolo arterioso ( whole - body )  . 
da questo punto di vista , la recente introduzione dei tomografi a 64 strati , offre la possibilit di effetuare uno studio completo di larghi distretti corporei con elevata risoluzione spaziale ed eccellente visualizzazione dei pi piccoli rami vascolari , riducendo al contempo la durata della scansione e la quantit di mezzo di contrasto ( mdc ) impiegato [ 2330 ]  . 
 radiol med ( 2008 ) 113 : 799816 the entire body with whole - body ct ( wb - ct angiography ) using a 64 - detector row scanner . materials and methods population between march and june 2006 , we enrolled 20 patients ( age range 4569 years ) referred to our division for typical or atypical chest pain ( 8 ) , clinical indications for coronary angiography ( 8 ) , investigation of coronary stent patency ( 2 ) and of aortocoronary bypass graft patency ( 2 )  . 
exclusion criteria were heart rate > 80 bpm , age < 35 years , history of adverse reactions to contrast material , renal failure ( serum creatinine > 120 mmol / l ) , impaired cardiorespiratory function and pregnancy . 
all patients with a heart rate > 60 bpm but < 80 bpm received 50 mg of metoprolol per os approximately 60 min before the scan to lower their heart rate to at least 65 bppatients were divided into two equal groups of ten subjects each ( group a and group b ) that were comparable for age , gender , weight and clinical features . 
the study was approved by the local ethics committee , and all patients gave their informed consent after receiving a clear explanation of the risks and benefits of the examination . 
i criteri desclusione sono stati : frequenza cardiaca > 80 bpm , et < 35 anni , precedenti reazioni avverse al mezzo di contrasto , insufficienza renale ( creatinina sierica > 120 mmol / l ) , compromissione della funzione cardio - respiratoria , gravidanza . 
tutti i pazienti con frequenza cardiaca > 60 bpm ma < 80 bpm sono stati sottoposti a bradicardizzazione tramite somministrazione orale di 50 mg di metoprololo 60 minuti circa prima dellesame sino a raggiungere una frequenza di almeno 65 bp i pazienti sono stati divisi in due gruppi ( gruppo a e gruppo b ) di 10 soggetti , omogenei per et , sesso , peso , e caratteristiche cliniche . 
lo studio ha ricevuto lapprovazione del comitato etico locale e tutti i pazienti hanno fornito il proprio consenso informato alla procedura dopo una chiara spiegazione dei potenziali rischi e dei benefici intrinseci allesame . 
patients were placed supine on the ct table with their arms raised above their head . three electrodes were placed on the patients chest ( right subclavicular area and right and left flank ) to monitor the patients ecg and obtain a tracing with a lead similar to l1 , in which the p wave , qrs complex and t wave could be distinguished . scanning protocol a preliminary 1.558 - mm scout view of the patients body was acquired in all cases . 
the wb - ct angiography protocol includes an initial scan limited to the cardiac region ( coronary ct angiography ) , followed by a whole - body scan ( extracoronary ct angiography )  . 
 coronary ct angiography an 18 - gauge needle cannula was inserted into a superficial vein of the antecubital fossa of the right arm or dorsum of the right hand , and the patients received a high iodine concentration contrast medium ( 400 mgi / ml ; iomeron 400 , bracco , milan , italy ) followed by a saline bolus . 
a series of dynamic low - dose scans ( 120 kvp , 30 mas ) at 1 - s intervals was acquired at the level of the aortic arch until aortic enhancement reached the preset threshold of 100 hounsfield units ( hu )  . 
the best temporal window ( percentage of r - r interval with no motion artefacts affecting the coronary arteries ) for retrospective image reconstruction was selected using postprocessing software , providing a preview of multiphase reconstructions at the level of the single axial images . 
 extracoronary ct angiography a second scan was obtained ( table 2 ) that covered a volume from the skull base to the ankles ; a second 70 - ml bolus of the same contrast material was injected at a rate of 4 ml / s , followed by a 30 - ml saline flush . 
in group a , we used an interval of 4560 s between the two angiografia con tc whole body tutti gli esami sono stati effettuati utilizzando uno scanner tc a 64 ( 322 ) strati di detettori ( somatom sensation 64 , siemens ag , forchheim , germania ; con tecnologia a macchia focale flottante o z - flying focal spot , gantry rotation time = 0 , 33 s )  . 
posizionando tre elettrodi sul torace ( rispettivamente in sede sotto - claveare destra ed in corrispondenza del fianco destro e sinistro ) stato possibile monitorare lecg del paziente , fino ad ottenere un tracciato con derivazione simile a d1 in cui fosse possibile riconoscere e differenziare londa p , il complesso qrs e londa t . protocollo di scansione in tutti i casi stato acquisito un topogramma preliminare del corpo del paziente per una lunghezza totale di 1 , 558 mla strategia di acquisizione del protocollo angio - tcwb prevede una prima scansione limitata allo studio del distretto cardiaco ( angio - tc coronarica ) , seguita da unacquisizione del corpo intero ( angio - tc extra - coronarica )  . 
 angio - tc coronarica attraverso unagocannula ( 18 gauge ) , posizionata in una vena superficiale a livello della fossa antecubitale del braccio destro o del dorso della mano destra , stato somministrato un mdc ad alta concentrazione di iodio ( 400 mgi / ml ; iomeron 400 , bracco , milano , italia ) seguito da un bolo di soluzione fisiologica . 
liniezione stata effettuata utilizzando un iniettore automatico a doppia testata ( medrad stellant dual ; medrad , palo alto pa , usa ) con i seguenti parametri : 80 ml di mdc + 30 ml di soluzione fisiologica ad un flusso di 4 ml / s , con durata totale della somministrazione di 27 , 5 secondi . per la scelta del ritardo ideale tra la somministrazione del mdc e linizio della scansione stata utilizzata una tecnica di bolus tracking : multiple acquisizioni dinamiche a bassa dose ( 120 kvp , 30 mas ) a livello dellarco aortico con intervalli di 1 secondo e soglia predefinita per linizio della scansione fissata 100 unit hounsfield ( hu ) , con intervallo di tempo di 7 secondi tra raggiungimento del valore soglia ed inizio della scansione stessa ( protocollo riassunto in tabella 2 )  . 
la scelta della miglior finestra temporale ( vale a dire , percentuale intervallo r - r con assenza di artefatti da movimento a carico delle arterie coronariche ) in cui ricostruire retrospettivamente le immagini stata efradiol med ( 2008 ) 113 : 799816 table 2 scanning protocols for computed tomography ( ct ) angiography of the coronary and extracoronary arterial circulation . 
fov , field of view ; hu , hounsfield units fettuata utilizzando un software di post - processing per lanteprima di ricostruzioni multifasiche a livello di una singola immagine assiale . 
 ct angiography coronary extra - coronary angio - tc extra - coronarica parameters scan protocol tube current ( kv ) reference values mas effetive mas collimation slice trickness ( mm ) scan time ( s ) pitch fov ( mm ) reconstruction algorithm contrast agent delay monitor threshold ( hu ) delay from threeshold ( s ) volume ( ml ) flow ( ml / s ) saline volume saline flow 367512 640 , 6 0 , 75 b20b36 3266 640 , 6 automatico aortic arch derived 5 ( minimum ) tabella 2 protocolli di scansione per lo studio angio - tc del circolo arterioso coronarico ed extra - coronarico . 
fov , campo di vista ; hu , unit di hounsfield studio angio - tc coronarica extra - coronarica parametri protocollo di scansione corrente di tubo ( kv ) valori di riferimento mas mas effettivi collimazione spessore ( mm ) tempo si scansione ( s ) pitch fov ( mm ) algoritmo di deconvoluzione mezzo di contrasto ritardo posizione di monitoraggio soglia ( hu ) ritardo dal raggiungimento della soglia ( s ) volume ( ml ) flusso ( ml / s ) volume di soluzione fisiologica 30 flusso di soluzione fisiologica 367512 640 , 6 0 , 75 b20b36 3266 640 , 6 automatico derivato arco aortico na 5 ( minimo ) boluses , whereas in group b , we used a fixed interval of 40 s . 
 successivamente , stata effettuata una seconda scansione ( protocollo riassunto in tabella 2 ) includendo un volume compreso dal basi - cranio fino alle caviglie ; un secondo bolo di 70 ml dello stesso mdc stato iniettato ad un flusso di 4 ml / s , seguito dallinfusione di 30 ml di soluzione fisiologica . 
nei due differenti gruppi di pazienti sono state valutate due tecniche alternative per la somministrazione del secondo bolo di mdc : nel gruppo a stato utilizzato un ritardo tra prima e seconda somministrazione variabile tra 45 e 60 secondi , mentre nel gruppo b stato utilizzato un ritardo fisso di 40 secondi . 
 tecnica di limitazione della dose in tutti i pazienti stato utilizzato un sistema di limitazione automatica della dose ( combined applications to reduce exposure , care dose 4d , siemens medical solutions , forchheim , germania ) in grado di modulare lintensit di corrente emessa dal tubo radiogeno , in relazione ai valori di attenuazione angolare della regione in esame . 
il software impact ctdosimetry ( versione 0.99w ) stato utilizzato per calcolare la dose effettiva mentre i valori di ctdivol sono stati estrapolati direttamente dalla console tc . analisi delle immagini le immagini sono state elaborate utilizzando una workstation dedicata dotata di software specifico per applicazioni cardiovascolari ( aquarius , terarecon , san matteo , california , usa ) : per una valutazione panoramica del letto vascolare stata utilizzata una tecnica di ricostruzione maximum intensity projection ( mip ) , mentre il grado di stenosi dei vasi e stato stimato con tecniche di ricostruzione multi planare ( mpr ) sia diretta che curva ( c - mpr ) , elaborata cio lungo lasse longitudinale del vaso . 
tutti i pazienti sono stati valutati da due osservatori in consenso ; la circolazione corporea , sia coronarica che extra - coronarica , e stata ripartita in segmenti arteriosi ( tabella 3 ) , cos come di seguito riportato : 1 . 
lalbero coronarico stato suddiviso in 15 segmenti , se804 exposure - control technique in all patients , we used an automatic exposure - control system [ combined applications to reduce exposure ( care ) dose 4d , siemens medical solutions , forchheim , germany ] capable of modulating tube current in relation to the angular attenuation of the anatomical region being studied . the reference values for image quality were 800 mas for coronary scans and 120 mas for extracoronary scans . 
the software package impact ctdosimetry ( version 0.99w ) was used to determine the effective dose , whereas the ctdivol values were extrapolated directly from the ct console . image analysis images were postprocessed on a dedicated workstation equipped with software for cardiovascular applications ( aquarius , terarecon , san matteo , ca , usa )  . 
for a comprehensive assessment of the vascular bed , we used the maximum intensity projection ( mip ) reconstruction algorithm , whereas the degree of vessel stenosis was determined using multiplanar reconstructions ( mpr ) , both direct and curved ( c - mpr ) , that is , along the longitudinal axis of the vessel . 
the coronary tree was divided into 15 segments according to the american heart association classification [ 31 ]  . for each segment , image quality was scored on a scale from 1 to 3 : poor diagnostic quality due to high heart rate or motion artefacts ( 1 ) , poor image quality due to inadequate opacification or calcium deposits ( 2 ) and adequate diagnostic quality ( 3 )  . 
each segment was scored according to degree of stenosis : 0 , normal ; 1 , moderate radiol med ( 2008 ) 113 : 799816 condo la classificazione dellamerican heart association [ 31 ] ; ad ogni segmento stato assegnato uno dei possibili livelli di qualit dellimmagine utilizzando una scala a 3 valori : scarsa qualit diagnostica per elevata frequenza cardiaca o artefatti da movimento in genere ( 1 ) , scarsa qualit diagnostica per insufficiente opacizzazione o eccesso di calcio ( 2 ) , adeguata qualit diagnostica ( 3 )  . 
la presenza di patologia aterosclerotica stata valutata qualitativamente sia per segmento ( valutando ogni segmento della singola arteria ) sia per paziente ( valutando la presenza / assenza di lesioni nel singolo soggetto ) in base al grado di stenosi : 0 , normale ; 1 , stenosi moderata ( < 50% ) ; 2 , stenosi significativa ( > 50% ) ; 2 . 
ad ogni segmento arterioso stato assegnato uno dei possibili livelli di stenosi : 0 , normale ; 1 , stenosi moderata ( < 50% ) ; 2 , stenosi moderato - severa ( 50%75% ) ; 3 , stenosi severa - preocclusiva ( 75%95% ) ; 4 , occlusione ; 5 , aneurisma . 
il grado di stenosi pi severo stato utilizzato per caratterizzare ogni segmento vascolare ( ad esempio : lesioni sincrone con stenosi del 40% e del 75% = stenosi di grado 3 )  . 
nei pazienti portatori di stent e di by - pass ( sia coronarici che a livello del circolo periferico ) stata analizzata la presenza o meno di stenosi significative ( riduzione del calibro50% )  . 
lenhancement dellalbero vascolare periferico stato valutato quantitativamente sia a livello dei vasi arteriosi che di quelli venosi in corrispondenza di 5 distretti anatomici ( collo - torace : carotide comune , vena giugulare ed arco aortico , vena cava superiore ; addome : aorta addominale , vena cava inferiore ; pelvi : arterie iliache comuni , vene iliache comuni ; coscia : arterie femorali comuni , vene femorali comuni ; gamba : arterie poplitee , vene poplitee ) ; la differenza in hu tra opacizzazione arteriosa e venosa ha fornito la stima del coefficiente di demarcazione tra strutture arteriose e venose . analisi statistica la prevalenza , la severit e la qualit della ma nella popolazione studiata sono state calcolate per segmento e per paziente per entrambi i distretti coronarico ed extra - coronarico . 
in patients with tra arterie e vene nel distretto extra - coronarico , il valore medio di opacizzazione arteriosa e la relativa deviazione standard per entrambi i gruppi e tra un gruppo e laltro di pazienti . 
infine stato calcolato indipendentemente il tempo necessario alla valutazione dei datasets dei distretti coronarici ed extra - coronarici per entrambi i gruppi di pazienti . 806 radiol med ( 2008 ) 113 : 799816 fig . 
1a - f quantitative assessment of the degree of opacification with measurements in hounsfield units , on regions of interest placed at six locations : common carotid artery ( a ) , thoracic aorta ( b ) and infrarenal aorta ( c ) , common iliac artery ( d ) and superficial femoral artery ( e ) , and popliteal artery ( f )  . 
1a - f valutazione quantitativa del grado di opacizzazione con misurazioni del valore di unit hounsfield , in corrispondenza di roi posizionate a 6 differenti livelli : arteria carotide comune ( a ) , aorta toracica ( b ) e addominale sottorenale ( c ) , arteria iliaca comune ( d ) ed arteria femorale superficiale ( e ) , arteria poplitea ( f )  . 
stenoses were classified according to location along the graft and anastomotic site . peripheral vascular tree enhancement was assessed quantitatively in arteries and veins in five anatomical regions ( neck - chest : common carotid , jugular vein and aortic arch , superior vena cava ; abdomen : abdominal aorta , inferior vena cava ; pelvis : common iliac arteries , common iliac veins ; thigh : common femoral arteries , common femoral veins ; leg : popliteal arteries , popliteal veins )  . 
hu gradient between arterial and venous attenuation provided an estimate of the differentiation coefficient between arterial and venous structures . statistical analysis the prevalence , severity and quality of atd were calculated for coronary and extracoronary circulation on a segment - bysegment and patient - by - patient basis . 
we also calculated the difference in attenuation between arteries and veins in the extracoronary circulation , the mean values and standard dedifferenze statisticamente significative sono state considerate per un valore di p < 0 , 05 . risultati lesame angio - tc whole - body stato portato a termine senza alcuna complicanza in tutti i pazienti . 
in due pazienti ( 10% ) , non sono state osservate alterazioni della parete arteriosa a carico delle arterie coronarie ed anche in sede extra - coronarica . radiol med ( 2008 ) 113 : 799816 viation of arterial attenuation within each group and between the two groups of patients . 
two patients ( 10% ) showed no mural alterations in either the coronary or extracoronary arteries . coronary circulation the optimal interval for reconstructing images of the coronary circulation varied in relation to the patients heart rate during the scan . 
the most frequently used percentiles ranged from 65% to 30% for heart rates < 60 bpm and from 25% to 45% for heart rates > 70 bp the number of nonassessable segments due to artefacts was 38 ( 37 cases of extrasystole , one pacemaker )  . 
of these , 97 ( 65% ) showed predominantly calcified plaque , 51 ( 31% ) showed predominantly fibrofatty plaque and six showed focal ectasia ( 4% ) due to previous angioplasty in two cases and to poststenotic dilatation in four cases . 
in 86 segments ( 54% ) , plaque caused < 50% stenosis , in 35 ( 23% ) > 50% stenosis , in 14 ( 9% ) a subocclusion and in 18 ( 13% ) a complete vessel occlusion . 
the time required to evaluate the data sets of the coronary circulation was 11.53 min in group a and 122 min in group b ; the difference was not statistically significant . 
2a - i dopo aver acquisito uno scout dalla base cranica al terzo mediodistale di gamba ( a ) , viene effettuata , a seguito della somministrazione di mdc , una prima scansione a livello cardiaco ( b ricostruzione vr ; g ricostruzione mip ) ; la successiva scansione viene effettuata sullintero corpo per la visualizzazione dellalbero arterioso sistemico , dalle arterie carotidi al circolo arterioso periferico ( c - e ricostruzione vr ; f , h , i ricostruzione mip )  . circolo coronarico lintervallo ottimale per la ricostruzione delle immagini del circolo coronarico variato in relazione alla frequenza cardiaca del paziente durante la scansione : i percentili pi utilizzati per le ricostruzioni sono risultati il 65% ed il 30% per frequenze < 60 bpm ed il 25% e 45% per frequenze > 70 bpi segmenti non valutabili a causa di artefatti sono stati 38 ( fenomeni di tipo extrasistolico n 37 , pace - maker n = 1 )  . sono stati valutati in totale 300 segmenti ( tabella 4 ) evidenziando la presenza di patologia in 155 ( 51% ) : di questi , 97 ( 65% ) presentavano apposizioni parietali prevalentemente calcifiche , 51 ( 31% ) apposizioni parietali prevalente808 radiol med ( 2008 ) 113 : 799816 fig . 
langiotc whole body dimostra la presenza di una placca morbida ulcerata a carico dellarteria carotide interna sinistra , con stenosi di grado moderatosevero ( a ricostruzione vr ; e ricostruzione mip ) ; larteria discendente anteriore presenta diffuse alterazioni parietali fibrocalcifiche lungo tutto il suo decorso ( b ricostruzione vr ; f ricostruzione mip ) ; le arterie iliache e femorali presentano sparse apposizioni prevalentemente calcifiche con concomitanti stenosi segmentarie di grado moderato ( c , d ricostruzione vr ; g , h ricostruzione mip )  . mente fibro - lipidiche e 6 presentavano una focale ectasia ( 4% ) , rispettivamente riconducibili ad esiti di pregressa angioplastica ( 2 ) e dilatazione post - stenotica ( 4 )  . 
in 86 segmenti ( 54% ) la placca determinava una stenosi < 50% , in 35 ( 23% ) una stenosi > 50% , in 14 ( 9% ) una stenosi pre - occlusiva ed in 18 ( 13% ) unocclusione completa del vaso . 
sono stati analizzati inoltre 3 stent ed un totale di 6 bypass : il lume intra - stent risultato ben visualizzabile e non si sono osservati artefatti da indurimento del fascio tali da impedirne una corretta valutazione . 
il tempo di valutazione dei datasets del distretto coronarico stato di 11 , 53 minuti nel gruppo a e di 122 minuti , nel gruppo b , senza evidenza di differenze statisticamente significative . 
 circolo sistemico sono stati valutati in totale 640 segmenti a carico del circolo arterioso sistemico extra - coronarico ( tabella 4 ) : lo studio angio - tc ha messo in evidenza 250 ( 38% ) segmenti con alterazioni riconducibili a patologia aterosclerotica ; di questi , 159 ( 63% ) presentavano placche ateromasiche a densit prevalentemente calcifica , 91 ( 37% ) placche prevalentemente di tipo fibro - lipidico . 
in 195 segmenti ( 77% ) la placca determinava una stenosi < 50% , in 26 una riduzione del calibro > 50% ( 9 , 5% ) , in 11 la placca determinava stenosi pre - occlusiva ( 4% ) , in 18 occlusione del vaso ( 7 , 5% ) , e in 5 ( 2% ) casi si evidenziava la presenza di una formazione aneurismatica . 
le sedi arteriose extra - coronariche maggiormente interessate da patologia sono state i vasi epiaortici ( 32 segmenti , 13% ) ed in particolare le arterie carotidi interne in corrispondenza della biforcazione , laorta addominale nel suo tratto sotto - renale ( 14 segmenti , 5% ) e lasse iliaco - femorale ( 64 segmenti , 26% )  . 
nei due gruppi di pazienti la valutazione quantitativa a carico dei segmenti del circolo sistemico ha fornito una mappa del grado di enhancement ottenuto nei vari distretti anatomici durante la scansione ( tabella 5 ) e contemporaneamente ha permesso di differenziare i valori densitometrici tra strutture arteriose e venose ( tabella 6 )  . 
in 195 segments ( 77% ) , plaque caused < 50% stenosis , in 26 > 50% stenosis ( 9.5% ) , in 11 subocclusion ( 4% ) , in 18 lanalisi quantitativa delle roi posizionate a livello dei vasi campione ha fornito valori omogenei , senza significative differenze di attenuazione nei diversi distretti ( p > 0.05 ) ; tuttavia lopacizzazione arteriosa , seppur costante a livello dei diversi distretti , risultata globalmente non ottimale dal punto di vista diagnostico . 
i valori di enhancement arterioso sono staradiol med ( 2008 ) 113 : 799816 table 4 results of evaluation of coronary and extracoronary arterial circulation pathology type , number and degree of occlusion coronary vessels ( 300 segments evaluated ) , pathological segments 155 ( 51% ) calcified plaques 97 ( 65% ) fibrofatty plaques 51 ( 31% ) focal dilatation 6 ( 4% ) calcified plaques 159 ( 63% ) fibrofatty plaques 91 ( 37% ) extracoronary vessels ( 640 segments evaluated ) , pathological segments 250 ( 39% ) tabella 4 risultati della valutazione del circolo arterioso coronarico ed extra - coronarico patologia type , number and degree of occlusion segmenti coronarici ( 300 segmenti valutati ) , segmenti affetti da patologia 155 ( 51% ) apposizioni calcifiche 97 ( 65% ) apposizioni fibro - lipidiche 51 ( 31% ) estasia focale 6 ( 4% ) apposizioni calcifiche 159 ( 63% ) apposizioni fibro - lipidiche 91 ( 37% ) segmenti extra - coronarici ( 640 segmenti valutati ) , segmenti affetti da patologia 250 ( 39% ) stenosis < 50% 86 ( 54% ) stenosis > 50% 35 ( 23% ) subocclusion 14 ( 9% ) occlusion 18 ( 13% ) stenosis < 50% 195 ( 77% ) stenosis > 50% 26 ( 9.5% ) subocclusion 11 ( 4% ) occlusion 18 ( 7.5% ) aneurysm 5 ( 2% ) stenosi < 50% 86 ( 54% ) stenosi > 50% 35 ( 23% ) stenosi pre - occlusiva 14 ( 9% ) occlusione 18 ( 13% ) stenosi < 50% 195 ( 77% ) stenosi > 50% 26 ( 9 , 5% ) stenosi pre - occlusiva 11 ( 4% ) occlusione 18 ( 7 , 5% ) aneurisma 5 ( 2% ) occlusion ( 7.5% ) , and in five cases ( 2% ) an aneurysm was present ( table 7 )  . 
the most frequently involved extracoronary arteries were the epiaortic vessels ( 32 segments , 13% ) , and in particular , the internal carotid arteries at the bifurcation , the infrarenal portion of the abdominal aorta ( 14 segments , 5% ) and the femoral - iliac axis ( 64 segments , 26% )  . 
in the two groups of patients , the quantitative evaluation of the systemic circulation segments provided a map of the degree of enhancement obtained in the different anatomical regions ( table 5 ) and allowed differentiation between the density values of arterial and venous structures ( table 6 )  . 
in nessun caso , infatti , i 810 radiol med ( 2008 ) 113 : 799816 common carotid artery thoracic aorta abdominal aorta common iliac arteries superficial femoral artery popliteal artery common carotid artery thoracic aorta abdominal aorta common iliac arteries superficial femoral artery popliteal artery group a group b ateria carotide comune aorta toracica aorta addominale art . 
mean attenuation was 2805 hu at the common carotid arteries , 250.38 hu at the aortic archthoracic aorta , 210.45 hu at the infrarenal aorta , 202.05 hu at the common iliac arteries , 189.65 hu at the superficial femoral valori di enhancement arterioso sono scesi al di sotto di 220 hu . 
a livello delle carotidi comuni il valore medio di atteradiol med ( 2008 ) 113 : 799816 arteriovenous attenuation difference neckthorax abdomen pelvis upper leg lowwer leg abdomen pelvis upper leg lowwer leg neckthorax group a group a differenza di attenuazione artero - venosa collotorace addome pelvi coscia gamba addome pelvi coscia gamba collotorace gruppo a gruppo b table 6 arteriovenous attenuation differences between group a and group b patients at the level of the five anatomical regions considered tabella 6 differenze tra attenuazione arteriosa e venosa tra pazienti del gruppo a e pazienti del gruppo b a livello dei cinque distretti corporei analizzati arteries and 193.79 hu at the popliteal arteries . 
substantial venous enhancement ( up to 220 hu at the jugular vein , that is , 150 hu above baseline ) was observed in all patients , with reduced discrimination between arteries and veins . 
mean attenuation values were 360.35 hu at the common carotid arteries , 333.89 hu at the aortic arch - thoracic aorta , 320.26 hu at the infrarenal aorta , 319.05 hu at the common iliac arteries , 308.28 hu at the superficial femoral arteries and 305.37 hu at the popliteal arteries . 
mean effective dose during extracoronary angiography was 4.10.7 msv , with a cdtivol of 3.61.1 mgy , that is , significantly lower ( p < 0.001 ) than that delivered during the coronary phase . 
in tutti i pazienti si e osservata una trascurabile opacizzazione venosa ( valore massimo di 100 uh ; 30 uh al disopra del livello basale ) , con eccellente discriminazione tra vasi arteriosi e venosi : la differenza media tra valori di attenuazione arteriosi e venosi a livello delle 6 differenti roi campionate stata di 209 uh ( p < 0 , 001 )  . 
nel gruppo b stata dimostrata un differenza superiore ( p > 0 , 001 ) tra opacizzazione arteriosa / venosa ottenuta nei vari distretti anatomici , rispetto a quanto valutato nel gruppo a . 
il tempo di valutazione dei datasets del distretto extra - coronarico stato di 23 , 53 minuti nel gruppo a e di 172 minuti , nel gruppo b , con evidenza di una differenza statisticamente significativa tra i due gruppi ( p > 0 , 001 )  . dose somministrata la dose effettiva media somministrata durante la angio - tc coronarica stata di 10 , 92 , 2 msv , con un ctdivol corrispondente a 40 , 27 , 1 mgy . 
la dose effettiva media somministrata durante lacquisizione angiografica extracoronarica stata di 4 , 10 , 7 msv , con un cdtivol di 3 , 61 , 1 mgy ; questultima significativamente minore ( p < 0 , 001 ) di quella somministrata durante la fase coronarica . 
la dose effettiva totale somministrata rientrata nel range 12 , 916 , 7 msv per paziente . risultata discussione background in alcuni contesti clinici ad alto rischio per lo sviluppo di ma con estensione sistemica , come ad esempio in pazienti con patologia diabetica scompensata , dislipidemie gravi e sindrome metabolica , lindividuazione precoce di alterazioni polidistrettuali potrebbe influenzare positivamente il management , indirizzando verso la prevenzione secondaria ( e isolatamente primaria ) di eventi vascolari avversi attraverso una strategia terapeutica ottimizzata . 
 angio - tc whole body : considerazioni tecniche lottimizzazione del protocollo di studio da noi valutato dimostra come sia tecnicamente possibile una valutazione completa del carico totale di aterosclerosi in pazienti affetti da ma . 
i nostri risultati hanno tuttavia messo chiaramente in evidenza che il ritardo intercorrente tra la prima e la seconda parte delliniezione bifasica del mdc deve essere rigidaradiol med ( 2008 ) 113 : 799816 ( and primary prevention in isolated cases ) of adverse vascular events through optimised treatment planning . 
our results have clearly shown that the time interval between the first and second phase of the biphasic contrast injection needs to be carefully calculated so as not to risk acquiring images of the extracoronary arteries , with suboptimal arterial enhancement and substantial venous contamination , and inadequate arteriovenous attenuation gradients in the same anatomical region . 
on the basis of our experience , we recommend a time interval of approximately 40 s between the first and second bolus , as this will ensure enhancement of the extracoronary arteries . 
this time window is related to the circulatory kinetics of contrast material that , once injected , reaches and travels through the arterial and venous system before returning to the pulmonary circulation and the heart and recirculating , to a large extent , in the arterial system [ 32 , 33 ]  . in group b subjects , despite the use of small contrast volumes , optimisation of timing provided excellent arterial opacification almost free of venous contamination , creating the best conditions for a whole - body ct angiography study . 
particularly interesting in this respect was the opportunity to obtain accurate imaging of the entire arterial system of the lower limbs , even in the presence of severe stenotic or occlusive disease . 
 whole - body ct angiography : clinical issues in 90% of patients who were referred due to a strong clinical - diagnostic suspicion of atd and should thus be considered at high risk , we identified the presence of synchronous coronary and extracoronary lesions . 
ten of them proceeded to preventive treatment ( 5 carotid stents for > 70% stenosis , one iliac and one femoral stent for subocclusions , one iliacfemoral bypass graft , 2 endografts for an aneurysm > 5 cm of the infrarenal aorta )  . 
recent studies have shown that patients with polyvascular atd are more likely to suffer adverse cardiovascular events compared with those with disease of a single arterial bed or the presence of risk factors only [ 34 ]  . 
it is therefore particularly important to identify mente calcolato , pena lacquisizione di immagini extra - coronariche con enhancement arterioso globalmente non ottimale e presenza di rilevante contaminazione venosa , con scarsi gradienti di attenuazione arteria / vena nello stesso distretto anatomico . 
sulla base della nostra esperienza , il ritardo consigliato tra la somministrazione del primo e del secondo bolo , necessario allopacizzazione dei distretti arteriosi extracoronarici , deve essere di circa 40 secondi . 
questa finestra temporale determinata dalla peculiare cinetica circolatoria del mdc che , una volta iniettato , raggiunge ed attraversa progressivamente il sistema arterioso e quello venoso per poi tornare al piccolo circolo ed al cuore , tornando in gran parte a perfondere nuovamente il circolo arterioso [ 32 , 33 ]  . 
nei soggetti appartenenti al gruppo b , nonostante limpiego di basse quantit di mdc , lottimizzazione della tempistica ha permesso di ottenere unopacizzazione arteriosa eccellente e sostanzialmente esente da contaminazione venosa , realizzando le migliori condizioni per uno studio angio - tc whole body . 
interessante , a tale proposito , appare soprattutto la possibilit di fornire un imaging accurato dellintero distretto arterioso degli arti inferiori , anche in presenza di severe alterazioni a carattere steno - ostruttivo : la nostra esperienza conferma quanto dimostrato in letteratura [ 1233 ] utilizzando protocolli di scansione a ritardo fisso , non modificato in relazione alla patologia di base del paziente . 
 un uleriore dato rilevante proviene dal calcolo del tempo di valutazione dei datasets extra - coronarici : i tempi ottenuti con protocollo non ottimizzato ( gruppo a ) sono risultati significativamente superiori a quelli ottenuti con protocollo ottimizzato ( gruppob )  . 
 angio - tc whole body : considerazioni cliniche nel 90% dei pazienti inclusi al nostro studio , valutati sulla base di rilevanti sospetti clinico - diagnostici e quindi da ritenersi una popolazione ad alto rischio per ma , sono state evidenziate lesioni sincrone coronariche ed extra - coronariche . 
tra i pazienti studiati , 10 sono stati indirizzati a trattamento preventivo ( 5 stent carotidei per stenosi > 70% , uno stent iliaco ed uno femorale per alterazioni pre - occlusive , un by - pass iliaco - femorale , 2 intervento di endoprotesi per aneurisma dellaorta addominale sottorenale di dimensioni > 5 cm )  . 
recenti studi hanno evidenziato come pazienti con interessamento polidistrettuale da ma abbiano una pi alta predisposizione ad eventi cardiovascolari avversi rispetto a pazienti con interessamento monodistrettuale o con semplice presenza di fattori di rischio [ 34 ]  . 
appare dunque particolarmente rilevante la possibilit di individuare alterazioni asintomatiche , ad uno stadio pre - clinico , altrimenti misconosciute : le lesioni da ma sintomatiche rappresentano infatti stadi avanzati di patologia , difficilmente trattabili con successo , mentre lesioni silenti possono beneficiare enormemente della terapia farmacologica o eventualmente 814 radiol med ( 2008 ) 113 : 799816 asymptomatic , preclinical alterations that would otherwise go undetected . 
symptomatic atd lesions in fact reflect advanced stages of disease that are difficult to treat successfully , whereas silent lesions can benefit greatly from pharmacological treatment or , where necessary , noninvasive endovascular treatment . innovations and limitations our study introduces an innovative opportunity to perform a complete cardiovascular evaluation allowing identification , characterisation and staging of atd with a single examination . 
however , in selected clinical settings presenting with a definite risk of polyvascular atd , the potential clinical value of a noninvasive , fast and reliable modality such as whole - body ct angiography could bring substantial benefits in the management of subjects at high cardiovascular risk , with a potential reduction of mortality and morbidity . 
the highest patient dose was found to be delivered during the coronary scan , with a limited ( albeit considerable ) amount of radiation being absorbed by the patient during the extracoronary study . 
 the total amount of contrast administered for the two studies was no greater than would have been necessary for parenchymal opacification , based on the patients body weight ( mean 76 kg ; 152 ml of contrast medium ) , and was at any rate within the minimum ranges suggested in theoretical models [ 32 , 33 ]  . 
the small number of patients studied is not sufficient to ensure the accuracy of the statistical estimate of the prevalence of extracoronary disease among subjects undergoing ct coronary angiography . larger studies with a diagnostic reference standard are therefore needed to validate our data . 
the first is whether , and to what extent , patient dose can be reduced to ensure an reasonable trade - off between diagnostic quality and patient safety ; the second is what might be the costbenefit ratio of identifying extra findings , that is , any accessory findings detected in extravascular sites during the examination . essere trattate in maniera non invasiva con approccio endovascolare . innovazioni e limiti il nostro studio introduce linnovativa possibilit di effettuare una valutazione cardiovascolare completa che permetta di identificare , caratterizzare e stadiare la ma con unico esame . 
per ovvie considerazioni radioprotezionistiche , il protocollo presentato lungi dal rappresentare uno strumento di screening utilizzabile su larga scala ; tuttavia , in contesti clinici selezionati che presentino un concreto rischio di ma polidistrettuale , il potenziale valore clinico di una metodica diagnostica non invasiva , rapida ed affidabile come la angio - tc whole body potrebbe apportare sostanziali benefici nella gestione dei soggetti ad alto rischio cardiovascolare , potenzialmente riducendone mortalit e morbilit . 
il maggior carico di dose e risultato durante la scansione coronarica con contenuto ( seppur importante ) quantitativo di raggi x assorbiti dal paziente nello studio extracoronarico ; il volume totale di mdc somministrato al paziente durante le due somministrazioni non e stato superiore a quello necessario per lopacizzazione parenchimale richiesta dal peso corporeo dei pazienti che hanno costituito la nostra popolazione ( media : 76 kg ; 152 ml di mdc ) , ed risultato peraltro nei range minimi suggeriti sulle base teoriche disponibili in letteratura [ 32 , 33 ]  . 
the problems raised need to be addressed in a larger study in order to formulate a definitive judgement on the usefulness of this method , which though not being proposed as a screening technique appears to be a feasible and promising innovation in the diagnostic workup of vascular atd . body , la cui fattibilit stata dimostrata nel presente lavoro , offre opportunit diagnostiche senza precedenti e potenzialmente con importanti ricadute cliniche , in selezionati pazienti . 
pescarolo , radiologia - padiglione barbieri - ospedale maggiore di parma , via gramsci 14 , 43100 parma , italy tel . : + 39 - 052 - 1703660 , fax : + 39 - 052 - 1986352 , e - mail : manupeschy@libero.it received : 17 september 2007 / accepted : 30 october 2007 / published online : 10 july 2008 springer - verlag 2008 abstract purpose . 
la gravit della broncopneumopatia cronica ostruttiva ( bpco ) pu essere classificata impiegando una stadiazione stilata dal progetto mondiale per la diagnosi , il trattamento e la prevenzione della broncopneumopatia cronica ostruttiva ( global iniziative for the diagnosis , management and prevention of chronic obstructive lung disease gold )  . 
lo scopo del nostro studio valutare se le classi gold correlano con lestensione dellenfisema polmonare ed altre caratteristiche rilevabili alla tc in una popolazione di fumatori con bpco in fase stabilizzata . 
nelle classi i ed ii , lestensione dellenfisema variava da minima a severa , mentre nella maggior parte dei pazienti in stadio iii e iv abbiamo osservato enfisema di grado severo . 
secondo il modello di regressione , soltanto il valore di estensione dell enfisema , valutato alla tc , ha predetto in modo indipendente la classe gold ( r2 = 0 , 58 ; p < 0 , 001 )  . 
anche se abbiamo trovato una correlazione significativa fra lestensione dell enfisema alla tc e le classi gold , una percentuale differente di enfisema pu essere osservata in ciascuna di esse . 
 parole chiave broncopneumopatia cronica ostruttiva linee guida del progetto mondiale per la broncopneumopatia cronica ostruttiva tc ad alta risoluzione introduction introduzione the global initiative for chronic obstructive lung disease ( gold ) guidelines were published in 2001 [ 1 ] and revised in 2004 [ 2 ] with the aim of increasing awareness of chronic obstructive pulmonary disease ( copd ) and decreasing morbidity and mortality from the disease . 
the gold has released a five - stage classification of copd severity based on spirometry and especially on forced expiratory volume in 1 s ( fev1 ) [ 2 ]  . 
at least as important , by setting a standard , gold has stimulated researchers to challenge its assumptions and use this classification as an aid in the interpretation of other patient - related observations . 
however , gold stresses that these cutoff points have not been clinically validated and that patient contact is mostly driven by symptoms as well as by the development of complications . 
it is well known that fev1 correlates poorly with symptoms , quality of life and exacerbation frequency ; the need to assess exercise tolerance and systemic features such as the measurement of the body mass index ( bmi ) is recognised by recent evidence [ 7 , 8 ]  . 
highresolution ct ( hrct ) scanning is the method of choice for noninvasive and sensitive assessment of pathologic changes in emphysema and has been shown to correlate well with pathologic grading [ 9 , 10 ]  . 
serial hrct has been reported to be a sensitive method of monitoring the progress of emphysema in patients with 1 - antitrypsin deficiency [ 11 ]  . moreover , ct quantification of emphysema has been used to demonstrate a decrease in emphysema after lung - volume le linee guida gold ( progetto mondiale per la diagnosi , il trattamento e la prevenzione della broncopneumopatia cronica ostruttiva ) sono state pubblicate nel 2001 [ 1 ] e riviste nel 2004 [ 2 ] allo scopo di migliorare il management della malattia e di ridurne la morbilit e la mortalit . 
il progetto gold ha stilato una classificazione di gravit della bpco costituita da cinque stadi basati sui dati spirometrici , in particolare sul volume espiratorio forzato in un secondo ( fev1 ) [ 2 ]  . 
inoltre le linee guida gold , stabilendo un valore standard , hanno stimolato i ricercatori a metterne in dubbio i presupposti ed usare questa classificazione come punto di riferimento nellinterpretazione di altre osservazioni riguardanti il paziente con bpco . 
tuttavia , il progetto gold sottolinea che questi valori non sono stati validati clinicamente e che lapproccio al paziente guidato principalmente dai sintomi e dallo sviluppo di complicanze . ben noto inoltre che il fev1 correla male con i sintomi , la qualit di vita e la frequenza delle esacerbazioni ; infatti , la tolleranza allesercizio fisico e i caratteri sistemici della malattia , quale la misura dellindice di massa corporea ( bmi ) , sono una recente dimostrazione della necessit di trovare parametri pi rappresentativi dello stato di malattia [ 7 , 8 ]  . inoltre , la classificazione gold non prende in considerazione il ruolo di altri parametri , quale la presenza di enfisema alla tomografia computerizzata ( tc )  . 
 attualmente , il ruolo della tc nella valutazione dei pazienti affetti da bpco non definito con chiarezza , anche se costituisce uno strumento sensibile e specifico per valutare le anomalie connesse con la malattia . 
la tc ad alta risoluzione ( hrct ) attualmente il metodo di scelta per una valutazione non invasiva e sensibile dellenfisema poich si osservato che essa correla bene con la classificazione radiol med ( 2008 ) 113 : 817829 reduction surgery [ 12 , 13 ] and to predict postoperative function in patients with lung cancer [ 14 , 15 ]  . the prevalence and the natural history of clinical emphysema in copd are not yet clear , but it might be important to investigate whether functional impairment is a true reflection of morphologic disease extent in copd patients . 
although there is still evidence that ct - demonstrated severity of emphysema is variably related to fev1 and other functional parameters , the correlation with gold stages has not been clearly elucidated . 
the aim of our study was to prospectively verify whether the extent of emphysema and other ancillary ct features correlate with gold stages and to determine the distribution of the severity of emphysema among gold stages in a population of smokers with stable copd . materials and methods patients were consecutively recruited from the centre for smoking cessation at the university of parma from november 2003 to december 2005 . 
a history of asthma ( variability of spirometric parameters , improvement in fev1 of > 20% after inhalation of 2 agonists , nocturnal symptoms , seasonal allergies , allergic rhinitis or eczema ) was carefully excluded . 
all individuals gave informed consent at presentation for the hrct scan and pulmonary function tests . based on clinical assessment and lung function testing , all subjects were classified into five groups according to gold criteria [ 2 ] : stage 0 , i , ii , iii or iv . 
informed consent was obtained for the use of physiologic data and ct scans . pulmonary function testing pulmonary function was evaluated by a flow - sensing spirometer and a pletismograph connected to a computer for data analysis ( vmax 22 and 6200 , sensor medics , yorba linda , ca , usa )  . 
total lung capacity ( tlc ) , inspiratory capacity ( ic ) , fev1 , fev1 / forced vital capacity ( fvc ) expressed as absolute value ( litres ) and as percentage of predicted value were recorded . 
the inspiratory - to - total lung capacity ( ic / tlc ) ratio was calculated , as it has been demonanatomo - patologica [ 9 , 10 ]  . 
inoltre , la quantificazione tc dellenfisema stata utilizzata per dimostrarne una diminuzione dopo interventi di riduzione chirurgica del volume polmonare [ 12 , 13 ] e per predire la funzionalit residua post operatoria in pazienti con il cancro polmonare [ 14 , 15 ]  . la prevalenza e la storia naturale dellenfisema nei pazienti con bpco non sono ancora chiare , ma potrebbe essere importante valutare se il danno funzionale riflette con accuratezza lestensione morfologica della malattia in questi pazienti . 
sebbene sia gi evidente che la gravit dellenfisema valutata con tc correla in modo variabile con il fev1 ed altri parametri funzionali , la correlazione con gli stadi gold non stata ancora chiaramente esplorata . 
lo scopo del nostro studio stato quello di verificare se lestensione dellenfisema ed altre anomalie tc correlano con le classi gold , determinandone la distribuzione fra le varie classi in una popolazione di fumatori con bpco in fase stabilizzata ( senza riacutizzazioni )  . materiali e metodi i pazienti sono stati reclutati in modo consecutivo dal centro antifumo delluniversit di parma tra novembre 2003 e dicembre 2005 . 
una storia di asma ( variabilit dei parametri spirometrici , miglioramento del fev1 > 20% dopo inalazione di 2 - agonisti , sintomi notturni , allergie stagionali , riniti allergiche , o eczema ) stata attentamente esclusa . 
sulla base della valutazione clinica e della funzionalit polmonare tutti i soggetti sono stati suddivisi in cinque classi secondo le linee guida gold [ 2 ] : classe 0 , i , ii , iii e iv . 
lindagine hrct stata effettuata una settimana dopo i test di funzionalit polmonare allo scopo di valutare sia lenfisema che le anomalie a carico delle vie aeree periferiche . lo studio stato approvato dal nostro comitato etico . 
il consenso informato stato ottenuto per luso dei dati fisiologici e per le scansioni tc . valutazione funzionale del polmone la valutazione funzionale a riposo stata eseguita median820 radiol med ( 2008 ) 113 : 817829 strated to be an independent risk factor for mortality in subjects with copd [ 16 ]  . 
forced expiratory flow ( fef ) measured at 25% , 50% and 75% of fvc ( fef25 , fef50 , fef75 , respectively ) were taken on the flow - volume loops . 
at least three measures were recorded for every variable , with the purpose of ensuring reproducibility of the data . ct technique ct scans were obtained with a 16 - detector - row ct scanner ( sensation 16 - siemens medical solutions , forhheim , germany ) and a 64 - detector - row ct scanner ( somatom cardiac 64 - siemens medical solutions , forhheim , germany )  . thin sections ( 1 mm ) were acquired in the supine position , with images obtained at full inspiration and without intravenous injection of contrast mediu images were reconstructed with a high - spatial - resolution algorithm and photographed at appropriate window settings ( level , 500 to 600 hu ; width , 1 , 500 to 1 , 600 hu )  . two observers scored the ct scans on hard - copy images independently , in random order , and on separate occasions without knowledge of the clinical data . 
emphysema was defined as areas of hypovascular low attenuation , usually lacking a well - defined wall , and where marked , associated with a disruption of the normal vascular markings . 
each lung on each image was scored according to the following grading : 0 , normal ; 1 , < 25% emphysema ; 2 , 25%50% emphysema ; 3 , 50%75% emphysema ; 4 , > 75% emphysema . 
the scores were then combined from each lung and , by multiplying the number of images obtained of the lungs , a final score was calculated [ 24 ]  . 
emphysema was classified into three main subtypes ( centrilobular , paraseptal and panlobular emphysema ) , and its craniocaudal distribution was also assessed . the analysis of airway abnormalities were performed on six lobes ( the lingula was regarded as a separate lobe )  . 
the extent of bronchiectasis was graded as follows : grade 1 , localised bronchiectasis affecting one or part of one bronchopulmonary segment ; grade 2 , bronchiectasis in more than one bronchopulmonary segment ; grade 3 , generalised bronchiectasis . te uno spirometro rilevante il flusso ed un pletismografo corporeo collegati ad un calcolatore per lanalisi dei dati ( vmax 22 e 6200 , sensor medics , yorba linda , ca , us )  . sono stati valutati la capacit polmonare totale ( tlc ) , la capacit inspiratoria ( ic ) , il fev1 ed il fev1 / fvc ( espresso come valore assoluto in litri e come percentuale del valore predetto )  . 
stato calcolato anche il rapporto ic / cpt , poich stato dimostrato essere questo un fattore di rischio indipendente per la mortalit nei soggetti con bpco [ 16 ]  . il flusso espiratorio forzato misurato al 25% , al 50% ed al 75% del fvc ( fef25 , fef50 , fef75 rispettivamente ) stato estrapolato dai cicli flusso - volume . 
almeno tre misure sono state registrate per ogni variabile , con lo scopo di garantire la riproducibilit dei dati . studio hrct le scansioni hrct sono state ottenute con uno scanner a 16 ( sensation 16 - siemens medical solutions , forhheim , germania ) ed uno a 64 banchi di detettori ( somatom cardiac 64 - siemens , medical solutions , forhheim , germania )  . sono state acquisite sezioni sottili ( 1 mm ) a paziente supino , nella massima inspirazione ( cpt ) e senza iniezione endovenosa di mezzo di contrasto . 
le immagini sono state ricostruite con un algoritmo ad alta risoluzione spaziale e stampate con appropriati livelli di finestra ( livello da 500 a 600 hu ; 15001600 hu )  . 
lenfisema stato valutato a tre livelli ( larco aortico , la carena tracheale e la vena polmonare inferiore di destra ) ; per ciascuna scansione di ciascun emitorace stato assegnato un punteggio secondo la seguente scala : 0 , normale ; 1 , meno del 25% di enfisema ; 2 , tra 25% e 50% di enfisema ; 3 , tra 50% e 75% di enfisema ; 4 , pi del 75% di enfisema . 
sono stati sommati i punteggi di ciascun emitorace ed il punteggio finale stato ottenuto moltiplicando questo valore per 100 e diviso per il punteggio massimo teorico [ 24 ]  . 
the presence of small airway disease was also detected by consensus ; small airways disease corresponded to a mosaic attenuation pattern that was eventually confirmed with the addition of expiratory scans . statistical analysis data are reported as meanstandard deviation ( sd ) unless otherwise specified . 
relationships between measures were estimated by spearmans rank correlation coefficient ( rs ) and linear regression analysis . multiple regression analysis was performed to determine which ct indexes ( emphysema extent , extent and severity of bronchiectasis ) would best predict gold stages . 
receiver operative characteristic ( roc ) curve method was used to evaluate screening cutoff for emphysema score with respect to sensitivity and specificity of gold stage [ 18 ]  . 
changes ranged from small local areas of destruction with normal surrounding lung to frank confluent destruction ( panlobular or advanced centrilobular emphysema ) ; emphysema extent ranged from 2% to 69% of total lung area . 
as shown in table 1 , five patients could not be classified according to gold stages , as they had an fev1 / fvc ratio of > 70% despite having a reduced fev1 ( < 80% predicted )  . 
lestensione delle bronchiectasie stata classificata come segue : grado 1 , bronchiectasie localizzate a uno o una parte di un segmento broncopolmonare ; grado 2 , bronchiectasie in pi di un segmento broncopolmonare e grado 3 , bronchiectasie diffuse . la severit della dilatazione bronchiale stata misurata confrontando il diametro interno del bronco con larteria polmonare adiacente : grado 0 , normale ; grado 1 , dilatazione inferiore a due volte rispetto il diametro dellarteria polmonare omologa ; 2 , dilatazione pi di tre volte il diametro dellarteria polmonare omologa . 
il pattern di attenuazione a mosaico attribuibile alla patologia delle piccole vie aeree stato valutato per consenso ; le scansioni espiratorie , che erano state ottenute prospetticamente , sono state integrate per la valutazione visiva dellair trapping . analisi statistica i dati sono stati espressi come mediadeviazione standard ( ds ) , se non altrimenti specificato . 
lanalisi di regressione multipla stata effettuata per determinare quale degli indici tc ( estensione dellenfisema , estensione delle bronchiectasie , ecc . ) correlasse meglio con le classi gold . il metodo della curva roc stato usato per individuare un valore cut - off di screening per lo score di enfisema , rispettando la sensibilit e la specificit delle classi gold [ 18 ]  . 
 risultati sono stati esaminati un totale di 43 pazienti con bpco in fase stabilizzata ( 25 m e 19 f , et media 62 anni , range di et tra 44 e 81 )  . 
le anomalie variavano da piccole aree focali fino a zone confluenti di distruzione parenchimale ( enfisema panlobulare o centrolobulare evoluto ) ; lestensione dellenfisema era compresa in un intervallo tra il 2% ed il 69% dellarea polmonare totale . 
solamente 4 pazienti presentavano enfisema parasettale isolato , mentre 11 avevano enfisema centrolobulare isolato e 21 822 radiol med ( 2008 ) 113 : 817829 table 1 extent of emphysema among gold stages . 
neither bronchiectasis scoring nor mosaic attenuation pattern entrambi i tipi di enfisema ; lenfisema era predominante nei lobi superiori , ma in 7 sette pazienti era esteso ai lobi inferiori . 
sia le bronchiectasie che il pattern di attenuazione a mosaico non hanno mostrato alcuna correlazione con lestensione dellenfisema , con le classi gold e con gli indici di funzionalit polmonare . 
secondo il modello di regressione , solamente lestensione dellenfisema alla tc ha predetto in modo indipendente la classe gold . lanalisi di regressione multipla ha fornito la seguente equazione : classe gold = 0 , 233 + 0 , 051 estensione dellenfisema alla tc ( r2 = 0 , 58 ; p < 0 , 001 )  . discussione in questo studio stato evidenziato principalmente che la severit dellenfisema allhrct mostra una buona correlazione con le classi gold , sebbene la relativa estensione di enfisema sia abbastanza variabile per ciascuna classe . 
3 scansione hrct espiratoria a livello della carena tracheale che mostra vasto pattern a mosaico dovuto a bronchiolite obliterante in paziente appartenente a classe gold iii . showed any correlation with the extent of emphysema , gold classes and pulmonary function indexes . 
il punto di cut - off accettabile estrapolato dalla curva ( area sotto la curva = 0 , 862 , p < 0 , 001 ) 31 , 5% ( sensibilit 85% ; specificit 84% ) ed indica i pazienti appartenenti ad uno stadio gold iii . the regression model , only ct emphysema extent independently predicted gold stage . 
these results are not surprising , as gold stages are essentially based on fev1 , which demonstrated good correlation coefficients with the severity of emphysema on ct in many studies . 
questo dato significativo , poich fev1 / fvc una misura pi sensibile della limitazione del flusso aereo e un fev1 / fvc inferiore al 70% dei valori previsti considerato un segno precoce di ostruzione in pazienti in cui il fev1 ancora nella norma [ 1 ]  . 
 nel nostro studio , anche se correlazioni significative sono state osservate fra estensione dellenfisema e , sia fev1 che fev1 / fvc , lanalisi di regressione ha mostrato che lestensione dellenfisema teneva conto solamente della met circa della variabilit delle classi gold ( r2 = 0 , 58 )  . infatti la bpco una patologia sia multifattoriale che multicompartimentale [ 8 , 22 ] , ed altri lavori non sono riusciti a dimostrare un rapporto diretto fra lestensione dellenfisema alla tc e la severit del danno funzionale [ 23 , 24 ] , suggerendo che lestensione dellenfisema non lunica anomalia morfologica che causa lostruzione del flusso aereo . quindi il rapporto fra enfisema ed ostruzione pi complesso e meno chiaramente definito di quello che spesso viene insegnato . 
 stato dimostrato che persino lenfisema centrolobulare severo , che di gran lunga la tipologia pi comune di enfisema nei fumatori , non necessariamente associato alla presenza di unostruzione funzionale [ 25 ]  . 
di conseguenza la presenza di enfisema nei pazienti di classe gold 0 non era ingiustificata , perch nelle loro fasi iniziali , lenfisema e lostruzione del flusso aereo sembrano essere indipendenti , anche se entrambi collegati allabitudine del fumo di sigaretta [ 26 ]  . 
 [ 27 ] hanno mostrato che nei soggetti appartenenti allo stadio 0 il fumo ha avuto effetti sulle alterazioni rilevate alla tc del torace , poich la proporzione di enfisema nei fumatori in questo stadio era significativamente superiore a quella dei non fumatori della medesima classe . 
sebbene sia stato dimostrato che nei pazienti appartenenti allo stadio 0 i sintomi della bronchite cronica non aumentino il rischio di progressione alle fasi pi severe di bpco [ 28 ] , nessuno studio longitudinale ha indicato quale sia il ruolo dellenfisema in questa fase . 
i soggetti in classe 0 che presentano enfisema alla tc potrebbero essere a rischio di sviluppare successivamente bpco severa nel corso della loro vita . in accordo con kohler et al . 
however , the research field has lost sight of the fact that copd is a multicomponent as well as multicompartment disease [ 8 , 22 ] , and other studies have failed to show a direct relationship between the extent of neato come la classificazione gold abbia tralasciato un sottogruppo importante di pazienti con bpco lieve , noi non abbiamo potuto far rientrare 5 pazienti in nessuna classe gold , poich presentavano un rapporto fev1 / fvc del 70% , malgrado un fev1 ridotto ( < 80% del previsto )  . 
inoltre , solamente un paziente apparteneva allo stadio gold i . sebbene lostruzione del flusso aereo nei fumatori sia causata dalla patologia intrinseca delle vie aeree e / o dalla perdita di retrazione elastica polmonare ( indipendente dallenfisema rilevabile ) [ 30 ] , nella bpco stabilizzata vi una correlazione pi forte fra lestensione dellenfisema e 826 radiol med ( 2008 ) 113 : 817829 emphysema on ct and the severity of airflow obstruction [ 23 , 24 ] , suggesting that the extent of emphysema is not the only morphological abnormality causing airflow obstruction . 
 it has been shown that even severe centrilobular emphysema , which is by far the most common type of emphysema in smokers , may be not associated with airflow obstruction [ 25 ]  . 
the presence of emphysema among patients with stage 0 disease was not unwarranted , because in their early stages , emphysema and airflow obstruction appear to occur independently , although both are linked to the smoking habit [ 26 ]  . 
showed that in stage 0 subjects , smoking had effects on the abnormality of chest ct findings , as the proportion of emphysema in smoking stage 0 subjects was significantly higher than that in nonsmoking stage 0 subjects . 
the subjects of stage 0 with emphysema on ct might be at risk for developing severe copd later in life . although it has been demonstrated in patients of stage 0 that symptoms of chronic bronchitis do not increase the risk for progression to the more severe stages of copd [ 28 ] , no longitudinal study has yet shown what the role of emphysema is at that stage . 
 [ 29 ] , who showed that gold classification missed an important subgroup of patients with mild copd , we could not classify five patients , as they had an fev1 / fvc ratio of > 70% despite having a reduced fev1 ( < 80% predicted )  . 
 although early in its genesis airflow obstruction in smokers is due either to intrinsic airway disease or to loss of lung elastic recoil pressure ( independent of detectable emphysema ) [ 30 ] , in established copd , there is a more robust correlation between emphysema extent and airflow obstruction [ 31 ]  . 
the cutoff value of emphysema extent of 31.5% allowed us to distinguish patients with fev1 < 50% , which is indicated as a crucial boundary that heralds to a higher frequency of exacerbations of the disease [ 32 ] as well as to a dramatic worsening of health status [ 5 ]  . although the presence of small airways disease did not hrct emphysema extent ( % ) fig . 
questo valore corrisponde al 31 , 5% e consente di distinguere i pazienti con un fev1 < 50% , che indicato come una linea di confine cruciale oltre la quale i pazienti vanno incontro ad una pi alta frequenza di riacutizzazioni della malattia [ 32 ] e ad un drammatico peggioramento dello stato di salute [ 5 ]  . la presenza di patologia delle piccole vie aeree non sembrata avere uninfluenza statisticamente significativa , probabilmente perch la prevalenza di reperti consistenti era troppo bassa per permetterne unanalisi . 
tuttavia , il riscontro di un valore elevato di vr nei pazienti in stadi gold avanzati suggerisce la presenza di intrappolamento aereo a bassi volumi polmonari , presumibilmente dovuto a malattia delle piccole vie aeree . 
infatti la maggior parte dei pattern di attenuazione a mosaico radiol med ( 2008 ) 113 : 817829 seem to have a statistically significant influence , the prevalence of findings consistent with small airways disease was probably too low to warrant analysis . 
it remains uncertain whether the low scores of mosaic attenuation pattern reflect a true prevalence of this pattern , which is very difficult to identify on an inhomogeneous background of widespread emphysema . 
 we used the visual score to evaluate emphysema extent because it is easy , quick and can be performed on only three slices so the patient can be exposed to the lowest possible radiation dose [ 34 ]  . 
several studies showed that the extent of emphysema scored visually on ct scans correlates significantly with the extent of emphysema scored on macroscopic lung sections obtained from resected specimens [ 9 , 35 , 36 ]  . 
some studies have shown that the radial distribution of emphysema may have a functional impact also ; emphysema located in the lung periphery has less effect on dlco than does more central emphysema [ 19 , 38 ]  . 
therefore , the relatively high percentage of paraseptal emphysema ( 25 / 43 patients ) as well as the predominance of mild extent of emphysema may explain the lack of correlation with the gas transfer indexes in our study . interestingly , we observed a significant correlation between the extent of emphysema and the pack - years index and the ic / tlc ratio ( r = 0.53 , p < 0.01 ) , which has been shown to be an independent predictor of all - cause and respiratory mortality in patients with copd [ 16 ]  . 
 abbiamo utilizzato lo score visivo per valutare lestensione dellenfisema perch facile e rapido e pu essere effettuato su tre sezioni , per esporre il paziente alla dose radiante pi bassa possibile [ 34 ]  . 
diversi studi hanno indicato che lestensione dellenfisema valutata visivamente sulle scansioni tc si correla significativamente con quella valutata su sezioni macroscopiche di polmone ottenute da campioni resecati [ 9 , 35 , 36 ]  . 
tuttavia , abbiamo valutato solamente lestensione globale dellenfisema senza considerare altri aspetti eterogenei della malattia che possono contribuire a predire meglio le anomalie funzionali . alcuni studi hanno infatti indicato che la distribuzione radiale dellenfisema pu influenzare il danno funzionale : lenfisema localizzato alla periferia del polmone influisce meno sulla riduzione della dlco rispetto allenfisema pi centrale [ 19 , 38 ]  . 
di conseguenza , la relativamente alta percentuale di enfisema parasettale ( 25 su 43 pazienti ) come pure la predominanza di enfisema a bassa estensione pu spiegare la mancanza di correlazione con gli indici di diffusione del gas nel nostro studio . 
 altri dati interessanti , meritevoli di approfondimenti futuri sono state le correlazioni significative fra lestensione dellenfisema e lindice pacchi / anno , ed il rapporto ic / cpt ( r = 0 , 53 , p < 0 , 01 ) , il quale stato indicato come un fattore di predizione indipendente da tutte le altre cause della mortalit nei pazienti con bpco [ 16 ]  . 
sono stati valutati i fattori di rischio cardiovascolari , le caratteristiche delle lesioni secondo la classificazione tasc , lo stato del run - off , i dati clinici pree postprocedurali ed i risultati procedurali . 
la perviet primaria e secondaria a 6 e 12 mesi risultata essere di 82 , 7% e 88 , 8% , e 74 , 3% e 81 , 5% , rispettivamente . 
la perviet primaria a 12 mesi risultata essere del 61 , 6% per lesioni associate a scarso run - off distale e del 78 , 8% per lesioni associate ad adeguato run - off distale ( p < 0 , 05 )  . 
because atherosclerosis is almost always systemic , patients with critical limb ischaemia have a 46% mortality rate due to cardiovascular events at 5 years and a 27% amputation rate at 1 year [ 14 ]  . the femoropopliteal region is the most frequent site of atheromas , which occur in this area in 50% of cases . 
femoropopliteal lesions are often associated with infrapopliteal lesions , especially in diabetic patients , making the treatment of more cranial lesions a compulsory step in the treatment of distal lesions . 
leg muscle motion is such that the superficial femoral and the popliteal arteries undergo constant and combined torsion , flexion , compression , stretching and shortening , leading to elastic recoil . 
the superficial femoral artery is subject to a low diastolic flow responsible for flow turbulence , and the intima at this level is characterised by marked intrinsic inflammatory features . all of the above may account for a greater tendency to endovascular intimal hyperplasia pta / stenting procedures compared with other regions . 
in particular , metallic stent placement in these areas is limited by a poor mean patency and a high rate of fractures , occlusions and kinking [ 57 ]  . response the aim of our study was to evaluate the shortand midterm patency rates of pta in the treatment of femoropopliteal steno - obstructive lesions . 
the secondary purpose was to analyse the possible influence of the most common cardiovascular risk factors on primary and secondary postprocedural patency . materials and methods study population radiol med ( 2008 ) 113 : 10431055 introduzione le arteriopatie ostruttive croniche degli arti inferiori ( aocp ) ad eziologia aterosclerotica sono patologie diffuse , con una percentuale variabile dell1 , 4% e l1 , 9% tra 40 e 49 anni , del 6 , 9% tra i 50 e 59 anni e superiore al 10% tra 60 e 69 anni , ed una netta prevalenza per il sesso maschile . leziologia quasi sempre a localizzazione multidistrettuale , il che comporta , nei pazienti con ischemia critica , un tasso di mortalit per accidenti cardiovascolari del 46% a 5 anni ed una percentuale del 27% di amputazione ad 1 anno [ 14 ]  . 
spesso , soprattutto nei pazienti diabetici , alle lesioni femoro - poplitee si associano lesioni infra - poplitee , per cui il trattamento delle lesioni pi craniali pu rappresentare un passaggio obbligatorio per il trattamento delle lesioni pi distali . 
infatti la dinamica muscolare della gamba fa s che larteria femorale superficiale e larteria poplitea siano sottoposte di continuo e in maniera combinata a movimenti di torsione , flessione , compressione , allungamento e accorciamento con conseguente elastic recoil di parete . 
larteria femorale superficiale inoltre soggetta ad un basso flusso diastolico responsabile di turbolenze di flusso ed infine lintima , a tale livello , caratterizzata da una spiccata propriet infiammatoria intrinseca . 
in particolare limpianto di stent metallici in tali sedi gravato da una perviet mediamente bassa e da un alto tasso di fratture , occlusioni e kinking [ 57 ]  . termine del scopo del nostro lavoro stato di valutare la perviet a breve - medio trattamento endovascolare mediante pta delle lesioni steno - ostruttive del distretto femoro - popliteo . 
scopo secondario stato analizzare leventuale influenza dei pi frequenti fattori di rischio per le malattie cardiovascolari sulla perviet primaria e secondaria post - procedura . from may 2004 to september 2005 , 100 patients ( 74 men and 26 women ; age range 5288 years ) affected by chronic peripheral arterial disease with femoropopliteal stenoobstructive lesions region underwent endovascular pta for a total of 104 procedures ( four patients had bilateral lesions )  . all patients were selected after clinical and laboratory assessment , followed by colour doppler ultrasonography materiali e metodi popolazione dello studio da maggio 2004 a settembre 2005 , 100 pazienti ( 74 uomini e 26 donne ; range di et 5288 anni ) affetti da aocp con radiol med ( 2008 ) 113 : 10431055 1045 ( cdus )  . 
patients with an indication for treatment also underwent computed tomography ( ct ) or magnetic resonance ( mr ) angiography to define the most appropriate approach ( surgical / endovascular )  . clinical evaluation included stress testing ( speed 3.5 km / h , slope 12% ) and measurement of the anklebrachial index ( abi )  . 
risk factors included smoking habit ( smokers and ex - smokers ) in 57% ( 57 / 100 ) , diabetes in 59% ( 59 / 100 ) , and dyslipidaemia in 42% ( 42 / 100 ) , which often coexisted . 
nei pazienti con indicazione al trattamento , la valutazione morfologica stata completata mediante esame angio - tc o angio - rmn in base al quale stato pianificato lintervento ( chirurgico / endovascolare ) pi idoneo . 
 la valutazione clinica ha incluso un test da sforzo ( velocit 3 , 5 km / h , pendenza 12% ) e la misurazione dellindice caviglia - braccio ( abi )  . 
sono stati selezionati : 36 pazienti ( 36 / 100 , 36% ) con claudicatio severa ( rutherford 3 ) , 48 pazienti ( 48 / 100 , 48% ) con dolore a riposo ( rutherford 4 ) e 16 pazienti ( 16 / 100 , 16% ) con lesioni trofiche ( rutherford 56 )  . 
tutti i pazienti presentavano una claudicatio significativa ( distanza relativa : 2918 metri ; distanza assoluta 8748 metri ) ed un indice abi ridotto ( abi a riposo : 0 , 42 ; abi dopo esercizio : 0 , 31 )  . 
in tutti i pazienti sono stati valutati i seguenti fattori di rischio : abitudine al fumo ( fumatori ed ex - fumatori ) nel 57% ( 57 / 100 ) , diabete nel 59% ( 59 / 100 ) e dislipidemia nel 42% ( 42 / 100 ) che spesso coesistevano . 
 lo stato del run - off distale , valutato in base alla presenza e al numero di vasi di gamba indenni da lesioni emodinamicamente significative , stato giudicato : discreto ( 2 - 3 vasi ) nel 58 , 7% ( 61 / 104 procedure ) e scarso ( 01 vasi ) nel 41 , 3% ( 43 / 104 procedure )  . procedure endovascolari tutte le procedure sono state eseguite in anestesia locale e con monitoraggio dellelettrocardiogramma e della pressione arteriosa . 
antiaggregant treatment with acetylsalicylic acid ( 100 mg / day ) and ticlopidine ( 250 mg / day ) was initiated the day before the procedure and maintained for 30 days . 
on completion of the procedure , postprocedural angiography was used to verify the outcome and evaluate the adequacy of distal runoff . definitions technical success was defined as the angiographic persistence of < 20% residual stenosis relative to the diameter of the artery immediately above or below the stenosis . 
haemodynamic success was defined as peak systolic velocity ( psv ) 150 cm / s in the treated segment , assessed at postprocedural b - mode and colour doppler us . 
at follow - up , restenosis was defined as a psv 230 cm / s and / or a psv ratio 2.5 in the treated area , indicators of stenoses > 50% . long - term follow - up evaluated the treated areas only , without considering other lesions . 
minor complications not requiring treatment were not considered [ 5 ]  . follow - up all patients underwent clinical and colour doppler us evaluation at 1 , 6 and 12 months after the procedure in the absence of significant complications . 
ct or mr angiography was only performed on patients with positive clinical and imaging findings to verify the need for additional surgical or endovascular treatment and to plan the interventional procedure if required . mediante la tecnica del cross - over . 
quattro / 104 ( 3 , 9% ) procedure , invece , sono state eseguite in sala operatoria , in anestesia epidurale , previa esposizione chirurgica dellarteria femorale comune omolaterale , sede di concomitante patologia steno - ostruttiva , come fase successiva alla tea chirurgica ( trattamento ibrido chirurgico - endovascolare )  . le procedure sono state eseguite previo posizionamento di introduttore vascolare 5 f ( 68 / 104 procedure ) e 6 f ( 36 / 104 procedure ) con superamento della lesione stenoostruttiva mediante guida idrofilica 0 , 035 o guida in acciaio 0 , 014 . 
langioplastica stata effettuata mediante cateteri a palloncino di diametro variabile da 4 a 6 mm , con lunghezza da 2 ad 8 c in 7 / 104 procedure ( 6 , 7% ) il trattamento stato completato mediante posizionamento di stent autoespandibile di diametro compreso tra 6 e 8 mm e lunghezza compresa tra 80 e 100 m stata posta indicazione al posizionamento di uno stent in 1 / 7 procedure ( 14 , 2% ) per una dissezione ostacolante il flusso post - pta e nelle rimanenti 6 / 7 procedure ( 85 , 8% ) per un risultato morfologico insoddisfacente della sola pta . 
in tutti i pazienti stata iniettata ev una dose variabile da 2500 a 5000 ui di eparina in relazione al peso corporeo mentre una terapia antiaggregante a base di acido - acetilsalicilico ( 100 mg / die ) e ticlopidina ( 250 mg / die ) stata somministrata il giorno prima del trattamento e protratta per i 30 giorni successivi . 
 definizioni il successo tecnico della procedura stato definito dal persistere allangiografia di una stenosi residua non superiore al 20% rispetto al calibro dellarteria immediatamente a monte o a valle del tratto stenotico . 
nel follow - up , stata definita restenosi un valore di pvs230 cm / s e / o da un psv ratio2 , 5 nella sede trattata , indici di stenosi > 50% . 
la perviet primaria stata definita come perviet persistente in assenza di re - intervento nella sede del trattamento , mentre la perviet secondaria stata definita come perviet ottenuta dopo efficace nuova procedura endovascolare . 
come successo clinico stata considerata una riduzione / scomparsa della sintomatologia con spostaradiol med ( 2008 ) 113 : 10431055 statistical analysis on the basis of the intra / periprocedural and follow - up results , we assessed technical success ( residual stenosis 20% ) and clinical success ( pain relief or significant improvement of symptoms and change in abi ) and cumulative primary ( without reintervention ) and secondary ( with reintervention ) patency rates at 6 and 12 months using the kaplanmeier test . 
in none of these cases did the attempt to recanalise modify the following surgical treatment in terms of bypass graft length and distal anastomosis site ( suprageniculate femoropopliteal bypass )  . 
in the postprocedural phase , we obtained clinical success in 91% of patients ( 91 / 100 )  . intraand periprocedural complications there were no deaths at 30 days after the procedure and no complications requiring minor / major amputation . 
in 1 / 4 patients with technical failure and in one patient with a technically successful treatment , the procedure was complicated by distal thromboembolism of the leg vessels , which was treated successfully with fibrinolysis ( actilyse )  . 
another of the four patients in whom treatment failed had focal rupture of the distal superficial femoral artery , with leakage of contrast agent into the soft tissues above the occlusion . 
only one of these dissections caused significant flow obstruction and was treated by 1047 mento2 categorie di rutherford associata ad un miglioramento dellabi ( > 0 , 10 )  . 
non sono state valutate le complicanze minori che non hanno richiesto alcun trattamento [ 5 ]  . follow - up tutti i pazienti trattati sono stati sottoposti a valutazione clinica ed eco - color doppler a 1 , 6 e 12 mesi dalla procedura , in assenza di complicanze significative . 
uno studio angiografico mediante tc o rm stato effettuato solo nei pazienti con esame clinico - strumentale positivo al fine di verificare la necessit di ulteriore trattamento , chirurgico od endovascolare , ed in questultimo caso di pianificare la modalit di esecuzione della procedura interventistica . 
 valutazione statistica sulla base dei risultati intra / periprocedurali e a distanza stato valutato il successo tecnico ( procedura tecnicamente riuscita con stenosi residua20% ) e clinico ( scomparsa del dolore o significativo miglioramento della sintomatologia e variazione dellabi ) delle procedure e la perviet cumulativa primaria ( in assenza di ritrattamento ) e secondaria ( mediante nuovo trattamento endovascolare ) a 6 e 12 mesi utilizzando il test di kaplan - meier . 
stata inoltre valutata la perviet primaria e secondaria distinta sulla base della classificazione tasc delle lesioni , dello stato del run - off distale e in relazione ai vari fattori di rischio ( sottogruppi fumatori vs non fumatori , diabetici vs non diabetici , dislipidemici vs non dislipidemici ) al fine di verificare la loro eventuale influenza sui risultati a distanza . 
in the remaining 11 patients , the dissection was treated by low - pressure angioplasty with prolonged balloon inflation ( at least three 180 - s inflations alternating with 30 s of free flow )  . 
the overall percentage of stents placed after pta was 7% ( 7 / 100 procedures )  . follow - up results at the 6 - month follow - up , we only assessed the 100 technically successful procedures ( 96 patients )  . 
three out of 96 patients ( 3.1% ) in whom three lesions had been treated died from causes unrelated to the procedure ( myocardial infarction ) at 2 , 3 and 5 months , respectively . 
with regard to primary / secondary patency , of a total of 97 successfully treated lesions , excluding the three lesions in the three deceased patients , 80 showed no recurrence , ten developed significant restenosis and the remaining seven developed an occlusion . 
the remaining two lesions were not treated , in one case because of clinical improvement and in the other because of the patients refusal ( severe cardiorespiratory compromise )  . 
of the seven cases of occlusion , two ( detected at 3 and 5 months , respectively ) were treated by surgical intervention ( subgeniculate femoropopliteal bypass ) and one by repeat pta , with poor periprocedural clinical success and subsequent major amputation due to inadequate distal runoff . 
of the six lesions ( four patients ) subjected to a second endovascular treatment for restenosis , three were patent , and two showed restenosis ( 10 and 11 months after initial treatment ) and were successfully treated by repeat pta and pta + stenting . 
two of the five restenoses were mento chirurgico in termini di lunghezza del by - pass e sede dellanastomosi distale ( by - pass femoro - popliteo sovragenicolato )  . 
in fase post - procedurale si registrato un successo clinico nel 91% dei pazienti ( 91 / 100 ) stato ottenuto . complicanze intra - peri - procedurali non si sono registrati decessi a 30 giorni dalla procedura n complicanze tali da richiedere il ricorso ad amputazione minor / major . 
in 1 dei 4 pazienti con insuccesso tecnico e in 1 paziente in cui il trattamento risultato tecnicamente riuscito , la procedura stata complicata da tromboembolia distale dei vasi di gamba , trattata con successo mediante fibrinolisi ( actylise )  . 
in un altro dei 4 pazienti in cui il trattamento non riuscito , si verificata la rottura focale del tratto distale dellarteria femorale superficiale con stravaso di mezzo di contrasto nei tessuti molli a monte dellostruzione . 
tale complicanza si risolta spontaneamente senza alcuna sintomatologia clinica . in 12 / 100 procedure tecnicamente riuscite ( 12% ) si osservata una dissezione intimale post - pta , delle quali una sola ostacolante il flusso in maniera significativa e quindi trattata mediante posizionamento di stent autoespandibile . negli altri 11 pazienti la dissezione stata trattata con angioplastica a bassa pressione con gonfiaggio prolungato del palloncino ( almeno tre gonfiaggi della durata di 180 secondi alternata a 30 secondi di flusso libero )  . 
in questi ultimi 6 pazienti , le placche erano caratterizzate da grossolane calcificazioni con disposizione a manicotto . la percentuale totale di stent posizionati post - pta risultata essere pari a 7% ( 7 / 100 trattamenti )  . risultati follow - up nel follow - up a 6 mesi sono state inserite solo le 100 lesioni ( 96 pazienti ) trattate con successo tecnico . 
3 / 96 pazienti ( 3 , 1% ) nei quali erano state trattate 3 lesioni , sono deceduti per cause non correlate al trattamento ( infarto miocardico ) , rispettivamente a 2 , 3 e 5 mesi dal trattamento . 
ai fini della perviet primaria / secondaria , su un totale di 97 lesioni valutabili trattate con successo , escludendo le 3 lesioni trattate nei 3 pazienti deceduti , 80 sono risultate indenni da recidiva , 10 hanno presentato restenosi significativa , mentre nelle restanti 7 lesioni si diagnosticata unocclusione . 
digital subtraction angiography ( dsa ) shows a proximal superficial femoral artery obstruction ( > 10 cm ) ( a , arrow ) [ transatlantic inter - society consensus ( tasc ) c ] , which was treated with stent placement after failed percutaneous transluminal angioplasty ( pta ) ( b , c )  . 
il controllo ecd a 12 mesi conferma la perviet dello stent e del vaso trattato ( d )  . treated by a second endovascular treatment ( pta ) , whereas the other three were not retreated ( in two cases due to patient refusal and in the third due to severe cardiorespiratory compromise )  . 
delle 7 ostruzioni , in 2 casi ( documentate rispettivamente a 3 e 5 mesi dal trattamento ) si deciso di effettuare un intervento chirurgico ( confezionamento di by - pass femoro - popliteo sottogenicolato ) , in 1 caso si proceduto a nuovo trattamento con pta con scarso successo clinico peri - procedurale e necessit di amputazione major per associato scarso run - off distale . 
delle 6 lesioni ( 4 pazienti ) sottoposte a nuovo trattamento endovascolare per resteno - ostruzione , 3 sono risultate pervie , 2 hanno ripresentato una restenosi ( 10 e 11 mesi dal primo trattamento ) con necessit rispettivamente di nuova procedura di pta e pta + stenting eseguita con successo . 
due delle 5 restenosi sono state ritrattate per via endovascolare ( pta ) mentre per le altre 3 non si eseguita nessuna correzione ( in 2 casi per rifiuto del paziente e nellultimo per concomitante grave patologia cardio - respiratoria )  . 
la perviet primaria e secondaria a 12 mesi risultata pertanto pari a 74 , 3% e 81 , 5% , rispettivamente , con un tasso di salvataggio darto pari al 95% . 
i risultati della perviet primaria e secondaria ottenuti mediante il test di kaplan - maier sono riassunti in tabella 1 e 2 . i risultati ottenuti riguardo la perviet a 6 e 12 mesi , considerando i sottogruppi suddivisi in base alla classificazione tasc delle lesioni , sono illustrati in tabella 3 , in base allo stato del run - off distale in tabella 4 ed in base alla presenza / assenza dei fattori di rischio in tabella 5 . 
la perviet primaria a medio - termine ( 12 mesi ) risultata 1052 radiol med ( 2008 ) 113 : 10431055 table 4 primary patency rates at 6 and 12 months according to distal runoff status runoff no . 
specific features of the femoropopliteal region appear to be responsible for a lower long - term success of endovascular procedures , namely , complexity of the anatomical area , which facilitates elastic recoil ; low diastolic flow producing such turbulence as to justify a greater tendency to intimal hyperplasia ; intrinsic inflammatory properties causing a stronger reactive response to angioplasty and stent placement . 
non si sono invece ottenute differenze statisticamente significative in termini di perviet a distanza confrontando i sottogruppi con presenza / assenza dei fattori di rischio specifici ( fumo , diabete e dislipidemia ) ( p = ns )  . discussione la localizzazione della patologia steno - ostruttiva nel distretto femoro - popliteo rappresenta pi del 50% di tutte le lesioni dellaocp ed clinicamente rilevante in quanto frequente causa di claudicatio di grado severo o dischemia critica [ 4 ]  . 
tale distretto mostra delle caratteristiche peculiari che sembrerebbero essere responsabili di una minore efficacia nel tempo delle procedure endovascolari : la sede anatomica complessa che favorisce lelastic recoil di parete ; il basso flusso diastolico con conseguente turbolenza tale da giustificare una maggiore tendenza alliperplasia intimale ; le propriet infiammatorie intrinseche con conseguente maggiore risposta reattiva allangioplastica e al posizionamento di stent . 
in particolare , lutilizzo di stent metallici non ha modificato significativamente i risultati a distanza della ricanalizzazione endovascolare sia per le suddette propriet infiammatorie e la tendenza alliperplasia intimale intrastent , sia per la frequenza di danni strutturali dei devices in relazione agli insulti meccanici ai quali gli stent vengono sottoposti dai vari movimenti di torsione , flessione , compressione , allungamento e accorciamento della gamba con conseguente restenosi e / o occlusione [ 6 , 7 , 1012 ]  . 
nello studio comparativo condotto da grimm , con una lunghezza media delle lesioni trattate pari a 2 , 9 cm2 , 5 cm , riportata infatti una perviet dell84 , 2% ad 1 anno e del 77 , 2% a 2 anni per la pta e del 75% ad 1 anno e del 72% a 2 anni per lo stent [ 13 ]  . tuttavia in un recente studio eseguito da rand [ 14 ] , la perviet primaria a 6 mesi per lesioni di lunghezza pari a 2 , 4 cm risultata significativamente maggiore nel gruppo stent rispetto al gruppo pta , sia in presenza di restenosi critica ( 83 , 7% vs 61 , 1% ) che subcritica ( 79 , 7% vs 45 , 6% ) [ 14 ]  . 
nel lavoro di gordon , con lunghezza media del segmento trattato superiore ai 14 cm , riportata una perviet primaria e radiol med ( 2008 ) 113 : 10431055 1053 inflammatory properties and tendency to in - stent intimal hyperplasia and the high rate of structural damage to the stents related to torsion , flexion , compression , stretching and shortening leg movements , which lead to restenosis and / or occlusion [ 6 , 7 , 1012 ]  . 
clearly , the outcome of stent placement appears to be closely influenced by the length of the segment treated , with worse long - term patency rates for long lesions . 
on lesions with a mean length > 14 cm , the 1 - year primary and secondary patency rates of stainless steel stents ( wallstent ) were 22% and 30% , respectively [ 7 ]  . 
for these reasons , surgical bypass grafting whenever possible with autologous saphenous vein ( on site or reversed ) has become the treatment of choice for long lesions , with 5 - year patency rates of 50%75% , that is , higher than those provided by pta alone , as confirmed by the study of nguyen [ 15 ] and by the recent basic trial ( bypass or angioplasty in severe intermittent claudication ) ( 2004 ) [ 16 ]  . 
these data lend support to the tasc recommendations to use endovascular pta for type a lesions , and surgical treatment for long , type d lesions ; precise indications for the intermediate class b and c lesions are lacking [ 8 ]  . 
in our experience , instead , indications for stent placement were dissection obstructing secondaria ad 1 anno per gli stent in acciaio ( wallstent ) pari al 22% e 30% , rispettivamente [ 7 ]  . 
per tali motivi , in caso di occlusione lunga la rivascolarizzazione chirurgica , basata sul confezionamento di by - pass , eseguiti ove possibile con vena safena autologa ( in situ o invertita ) , rappresenta a tuttoggi la terapia di scelta con perviet a 5 anni variabile tra il 50% e il 75% , superiore al solo trattamento di pta come anche dimostrato dallo studio di nguyen [ 15 ] e dal recente trial basic ( bypass or angioplasty in severe intermittent claudication ) ( 2004 ) [ 16 ]  . 
tali dati giustificano e supportano le raccomandazioni suggerite dal tasc per cui il trattamento endovascolare con pta consigliato per lesioni di tipo a mentre il trattamento di tipo chirurgico consigliato per lesioni lunghe , di tipo d , in assenza tuttavia di precise indicazioni per le classi intermedie ( b e c ) [ 8 ]  . 
 nella nostra esperienza , il trattamento endovascolare con pta di lesioni con lunghezza media di 6 , 3 cm ha consentito di ottenere un successo tecnico pari al 96 , 1% ed una perviet primaria e secondaria a 6 e 12 mesi pari a 82 , 7% ed 88 , 7% , ed a 74 , 3% e 81 , 5% rispettivamente , con un tasso di salvataggio darto a 12 mesi pari a 95% . 
tali risultati appaiono sostanzialmente simili a quelli riportati nel lavoro di surowiec [ 17 ] in cui per , tutte le lesioni di tipo c e d sono state trattate mediante posizionamento di stent . 
nella nostra esperienza , invece , lindicazione al posizionamento di stent stata posta solo in caso di dissezione ostacolante il flusso o di persistenza di una stenosi significativa ( 6 , 7% )  . 
tale dato appare supportato dal concetto che nel distretto femoro - popliteo pu risultare utile anche una sorta di by - pass temporaneo in grado di riattivare i circoli collaterali tra larteria femorale profonda e larteria poplitea responsabili di un miglioramento del quadro clinico del paziente e di una ridotta probabilit di ischemia critica / necessit di amputazione , anche nel caso di restenosi o occlusione del sito di trattamento . 
this finding is supported by the idea that a sort of temporary bypass may serve to reactivate the collateral circulation between the deep femoral artery and the popliteal artery , leading to improvement in the patients clinical condition and reduced likelihood of critical ischaemia / need of amputation , even in the event of restenosis or occlusion of the treatment site . analysis of long - term patency rates obtained in the various tasc subgroups confirms the close correlation existing between patency and the morphological and structural features of the lesions . 
 [ 20 ] , who reported that tobacco smoking , which has an important role in development of atherosclerotic plaque , does not appear to negatively affect long - term patency rates . 
angelelli , unit operativa radiodiagnostica universitaria , azienda ospedaliera universitaria - ospedale policlinico consorziale , piazza giulio cesare 11 , 70124 bari , italy , tel . : + 39 - 080 - 5478840 , fax : + 39 - 080 - 5592911 , e - mail : g.angelelli@radiologia.uniba.it received : 26 october 2007 / accepted : 27 february 2008 / published online : 8 september 2008 springer - verlag 2008 abstract purpose . 
ct studies of 32 patients with pulmonary metastases were retrospectively reviewed . images were assessed for the following parameters : number , size , location , distribution of the nodules and the presence of the mass - vessel sign . 
two - dimensional ( 2d ) axial images and mip and vr reconstructions exhibited 100% sensitivity for lesions > 10 mfor nodules 610 mm , sensitivity was 49%55% for the 2d images , 90% for mip and 80%85% for vr reconstructions . 
per lesioni > 10 mm le immagini assiali 2d , mip e vr hanno presentato sensibilit del 100% ; per noduli di 610 mm le 2d del 49%55% , le mip del 90% e le vr dell80%85% ; per metastasi 5 mm le 2d del 22% , le mip del 87%89% , le vr del 55%58% . 
le mip sono le ricostruzioni pi sensibili nel riconoscimento dei piccoli noduli polmonari . parole chiave metastasi polmonari noduli polmonari tcms radiol med ( 2008 ) 113 : 954967 introduction introduzione in the staging and follow - up of oncological disease , one of the main purposes of diagnostic imaging techniques is to search for pulmonary metastases . 
the primary target organ of haematogenous metastases may be the lungs in renal tumours , sarcomas and melanomas ; otherwise , pulmonary involvement can be secondary to other localizations , as often occurs in gastrointestinal or ovarian tumours . 
endobronchial metastasis is rare , having an incidence of 2% , and mainly occurs in cases of bronchioloalveolar carcinoma [ 1 ]  . diagnostic imaging techniques for detecting pulmonary metastases include chest x - ray , computed tomography ( ct ) and positron emission tomography ( pet ) , the latter being used as a second - level tool for the functional evaluation of pulmonary nodules [ 2 ]  . 
various studies have shown that conventional radiology has a sensitivity of 44%56% in detecting lung metastases , but despite this poor performance , it is still used in the follow - up protocols of some malignant tumours [ 36 ]  . 
however , the first ct devices had some limitations due to the fact that they acquired single contiguous slices and had only a modest temporal resolution , causing artefacts due to heart beat and respiratory movements [ 8 ]  . 
 the introduction of spiral technology has brought about a significant increase in nodules detection , because spiral scanners provide volumetric images and reduce the rate of false negatives attributable to respiratory movements [ 7 , 9 , 10 ]  . this method is estimated to have an overall sensitivity of about 79% [ 11 ] and a 47%69% sensitivity in detecting nodules with a diameter < 67 mm [ 12 ]  . 
in addition , the isotropic volumetric data provided enable excellent quality multi - planar reformatting ( mpr ) , maximum intensity projection ( mip ) and volume rendering ( vr ) reconstructions , which are particularly useful in the study of focal and diffuse pulmonary disease [ 13 ]  . 
 the aim of this work was to assess the performance of multi - slice ct ( msct ) using mpr , mip and vr to detect and analyse pulmonary nodules attributable to metastasis in cancer patients . materials and methods all cancer patients who presented ct findings of pulmonary nella stadiazione e nel follow - up del paziente oncologico la ricerca delle metastasi polmonari rappresenta uno dei principali obiettivi della diagnostica per immagini . 
le metastasi per via ematica possono interessare come primo organo il polmone nei tumori renali , sarcomi e melanomi ; oppure linteressamento polmonare pu essere secondario ad altre localizzazioni , soprattutto quella epatica , come spesso avviene nei tumori del tratto gastro - enterico od ovarici . 
pi rara la metastatizzazione per via endobronchiale che ha una incidenza del 2% e si verifica prevalentemente nei carcinomi bronchioloalveolari [ 1 ]  . la diagnostica per immagini delle metastasi polmonari si basa sullindividuazione di noduli polmonari multipli e si avvale della radiografia del torace , della tomografia computerizzata ( tc ) e della tomografia ad emissione di positroni ( pet ) , questultima utilizzata come indagine di secondo livello per ottenere valutazioni funzionali [ 2 ]  . 
diversi studi hanno dimostrato che la radiologia tradizionale nella individuazione delle metastasi polmonari presenta una sensibilit del 44%56% , tuttavia prevista nei protocolli di follow - up di alcuni tumori maligni [ 36 ]  . 
le prime apparecchiature tc presentavano alcuni limiti legati allacquisizione di singole sezioni contigue e ad una modesta risoluzione temporale causa di artefatti da pulsazioni cardiache e da respiro [ 8 ]  . un significativo incremento nella identificazione dei noduli derivato dalla introduzione della tecnologia spirale che fornisce immagini volumetriche e riduce la percentuale di falsi negativi in rapporto allescursione respiratoria [ 7 , 9 , 10 ]  . 
la sensibilit di tale metodica stimata , complessivamente , intorno al 79% [ 11 ] ed in particolare al 47%69% nella individuazione di noduli con diametro inferiore a 67 mm [ 12 ]  . 
inoltre i dati volumetrici isotropici forniti da tali apparecchiature consentono di ottenere ricostruzioni multi - planar reformatting ( mpr ) , maximum intensity projection ( mip ) e volume rendering ( vr ) di eccellente qualit , particolarmente utili nello studio della patologia polmonare focale e diffusa [ 13 ]  . scopo del seguente lavoro valutare le potenzialit della tc a 16 strati ( tcms ) utilizzando le ricostruzioni mpr , mip e vr nella ricerca dei noduli polmonari , riferibili a metastasi in pazienti oncologici . 956 radiol med ( 2008 ) 113 : 954967 nodules attributable to metastatic dissemination were retrospectively analysed . 
patients were selected for whom comparison could be made with a previous ct scan either not showing any nodule or demonstrating an increase in nodule number and / or dimensions . 
in all 32 patients ct scans of the chest had been performed without or with contrast medium as part of the periodical oncological follow - up , which also included scans of the abdomen and pelvis . ct scans of the chest were performed with the same 16 - slice device ( aquilion 16 , toshiba , tokyo , japan ) using the following parameters : slice thickness 1 mm , reconstruction thickness 0.8 mm , pitch 1 , rotation time 0.5 s , 120 kv , 100 mas , craniocaudal scans during an inspiratory breathhold with a ct dose index ( ctdi ) of 20 mgy . 
in all cases , the ct scans were reviewed by two radiologists , vg ( observer 1 ) and fs ( observer 2 ) , with , respectively , 2 and 4 years of experience in thoracic imaging and who had not been involved in performing the scans and were blinded to the patients clinical and general data . 
after a further 15 days , vr reconstructions , with a thickness of 10 mm , were analysed . all images were presented randomly to the two observers to avoid memory of the previous reading . 
ct scans were assessed for : number of nodules size distribution ( upper , middle , lower lobe ) relationships with the anatomical structures of the secondary pulmonary lobule ( centrilobular arterial and interlobular septa ) to classify nodules into centrilobular , interlobular and subpleural connection between the nodule and the centrilobular arterial vessel ( mass - vessel sign )  . sensitivity was then calculated for each reconstruction technique with respect to a gold standard , which was based on all pulmonary nodules detected by consensus by two independent radiologists , ga and as , with 35 and 10 years experience , respectively . 
a tal fine stata effettuata una ricerca nel database dei referti degli esami tc eseguiti nel periodo compreso tra maggio 2005 e luglio 2007 e sono stati selezionati i pazienti per i quali era possibile effettuare un confronto con un esame tc precedente che non evidenziava lesioni nodulari o che ne dimostrava un incremento numerico e / o dimensionale . 
tale ricerca ha prodotto una lista di 74 pazienti , dai quali ne sono stati esclusi 17 che presentavano noduli di diametro maggiore di 15 mm e 25 portatori di un numero di noduli superiore a 20 . alla fine sono stati arruolati 32 pazienti ( 18 di sesso maschile e 14 di sesso femminile ) , di et compresa tra i 27 e gli 85 anni ed et media di 6512 anni . 
in tutti i 32 pazienti selezionati le scansioni tc erano state eseguite senza o con mezzo di contrasto , utilizzato poich lesame rientrava nel controllo periodico di pazienti neoplastici e prevedeva anche lo studio delladdome e della pelvi . gli esami tc erano stati tutti eseguiti con la stessa apparecchiatura a 16 detettori ( aquilion 16 , toshiba , tokyo , giappone ) utilizzando , per lo studio del torace , i seguenti parametri di acquisizione : spessore di strato 1 mm , spessore di ricostruzione 0 , 8 mm , pitch 1 , tempo di rotazione del tubo 0 , 5 s , 120 kv , 100 mas , acquisizione cranio - caudale in apnea inspiratoria con un valore di indice tc di dose ( ctdi ) 20 mgy . le immagini ottenute sono state trasferite su una workstation dotata di software per il post processing dei dati volumetrici ( vitrea 3.5 , vital imaging , seattle , usa )  . 
le immagini tc sono state esaminate da due radiologi vg ( osservatore 1 ) e fs ( osservatore 2 ) rispettivamente con 2 anni e 4 anni di esperienza in radiologia toracica , i quali non avevano partecipato attivamente allesecuzione dellesame ed in cieco rispetto ai dati clinici ed anagrafici del paziente . 
le immagini nei piani assiali e le ricostruzioni coronali e sagittali sono state valutate per prime , quelle in mip , utilizzando uno spessore di ricostruzione di 10 mm , sono state esaminate a distanza di 15 giorni . 
in seguito , a distanza di altri 15 giorni , sono state analizzate le immagini ricostruite in vr con spessore di 10 m tutte le immagini sono state fornite ai due osservatori in maniera randomizzata per evitare che potesse rimanere memoria delle precedenti osservazioni . 
nel valutare le immagini tc sono stati considerati : numero dei noduli ; dimensioni ; distribuzione ( lobo superiore , medio , inferiore ) ; radiol med ( 2008 ) 113 : 954967 case simultaneously using both the axial - source images and mpr , mip and vr reconstructions . 
 subsequently the compatibility of each reconstruction technique with the gold standard was verified by using students t test , with statistical significance set at p > 0.05. finally , interobserver agreement in the evaluation of the same nodules was measured with the cohen k statistic . statistical analysis was carried out with the dedicated software epi - info 6.6 ( public domain software - cdc , atlanta , ca , usa ; who , geneva , switzerland )  . results the results obtained by the two radiologists acting as the gold standard in assessing the number , size and distribution of pulmonary nodules , their relationship with the anatomical structures of the secondary pulmonary lobule and presence of the mass - vessel sign are shown in table 1 . 
results obtained by the two observers are shown in tables 2 and 3 . as can be seen in tables 2 and 3 , the axial images depicted a total of 267277 metastases , with a mean sensitivity of 35% . 
coronal table 1 gold standard number size distribution rapporti con le strutture anatomiche del lobulo polmonare secondario ( arteriola centrolobulare e setti interlobulari ) per differenziare i noduli in centrolobulari ed intralobulari ; dimostrazione di una diretta connessione tra nodulo metastatico e vaso arterioso centrolobulare ( segno del vaso )  . sono stati , quindi , calcolati i valori di sensibilit di ciascuna tecnica di ricostruzione rispetto ad un gold standard , rappresentato dai noduli polmonari rilevati in consenso da due radiologi indipendenti , ga e as , rispettivamente con 35 anni e 10 anni di esperienza , che hanno esaminato contemporaneamente ogni paziente potendo utilizzare sia le immagini assiali , che le ricostruzioni mpr , mip e vr . 
 successivamente stata verificata la compatibilit di ciascuna tecnica di ricostruzione con il gold standard mediante il test statistico t di student con livello di significativit fissato per valori di p > 0 , 05 . 
infine , stata calcolata la concordanza tra i due osservatori nella valutazione dei medesimi noduli utilizzando il test statistico k ( di cohen )  . lelaborazione statistica dei dati stata effettuata con software dedicato epi - info 6.6 ( public domain softwarecdc atlanta , georgia ; who geneve , svizzera )  . risultati i risultati ottenuti dai due radiologi esperti e considerati come gold standard riguardanti il numero , le dimensioni , la distribuzione dei noduli polmonari , il loro rapporto con le strutture del lobulo polmonare secondario e lincidenza del segno del vaso sono riportati nella tabella 1 , quelli ottenuti dai due osservatori nelle tabelle 2 e 3 . 
come risulta dalle tabelle 2 e 3 nellanalisi dei due osservatori , le immagini assiali hanno evidenziato globalmente 267277 metastasi con una sensibilit media del 35% ; in particolare per noduli di diametro 5 mm la sensibilit stata del 22% , per relationship with structures of the secondary lobule mass - vessel sign 5 mm 610 mm > 10 mm upper middle lower centrilobular interlobular number % tabella 1 gold standard numero dimensioni distribuzione rapporti con le strutture del lobulo secondario segno del vaso 5 mm 610 mm > 10 mm superiore media inferiore centro - lobulari inter - lobulari numero 958 table 2 pulmonary nodules detected ( observer 1 ) number size distribution radiol med ( 2008 ) 113 : 954967 relationship with the structures of the secondary lobule mass vessel sign 5 mm 610 mm > 10 mm upper middle lower centri - lobular inter - lobula mpr , multiplanar reconstruction ; mip , maximum intensity projection ; vr , volume rendering tabella 2 noduli polmonari evidenziati ( osservatore 1 ) numero dimensioni distribuzione 5 mm 610 mm > 10 mm superiore media inferiore centro - lobulari inter - lobulari rapporto con le strutture del lobulo secondario segno del vaso axial coronal 252 sagittal axial coronal 652 sagittal axial coronal 482 sagittal assiali mpr coronali mpr sagittali mip assiali mip coronali mip sagittali assiali coronali sagittali 77 ( 29% ) 73 ( 29% ) 72 ( 29% ) 289 ( 42% ) 274 ( 42% ) 265 ( 41% ) 211 ( 42% ) 197 ( 41% ) 200 ( 41% ) 77 ( 29% ) 73 ( 29% ) 72 ( 29% ) 289 ( 42% ) 274 ( 42% ) 265 ( 41% ) 211 ( 42% ) 197 ( 41% ) 200 ( 41% ) mpr , multiplanar reconstruction ; mip , maximum intensity projection ; vr , volume rendering mip reconstructions demonstrated 652656 metastases , with a mean sensitivity of 84.5%. 
in particular , sensitivity for nodules 5 mm was 80%81% , for nodules 610 mm , 87% ; and for noduli di diametro compreso tra 6 e 10 mm stata del 49%53% e del 100% per noduli di diametro > 10 mle ricostruzioni mpr coronali hanno evidenziato globalmente 252264 metastasi con una sensibilit media del 33 , 5% ; in particolare la sensibilit stata del 21% per noduli di diametro 5 mm , del 46%51% per noduli di diametro compreso tra 6 e 10 mm e del 94% per noduli di diametro radiol med ( 2008 ) 113 : 954967 table 3 pulmonary nodules detected ( observer 2 ) number size distribution 5 mm 610 mm > 10 mm upper middle lower centri - lobular inter - lobular relationship with the structures of the secondary lobule mass vessel sign mpr , multiplanar reconstruction ; mip , maximum intensity projection ; vr , volume rendering tabella 3 noduli polmonari evidenziati ( osservatore 2 ) numero dimensioni distribuzione 5 mm 610 mm > 10 mm superioremedia inferiore centro - lobulari inter - lobulari rapporto con le strutture del lobulo secondario segno del vaso axial coronal 264 sagittal axial coronal 656 sagittal axial coronal 507 sagittal assiali coronali sagittali assiali mip coronali mip sagittali assiali coronali sagittali 80 ( 29% ) 76 ( 29% ) 75 ( 29% ) 286 ( 41% ) 267 ( 41% ) 259 ( 40% ) 266 ( 41% ) 211 ( 40% ) 199 ( 40% ) 80 ( 29% ) 76 ( 29% ) 75 ( 29% ) 286 ( 41% ) 267 ( 41% ) 259 ( 40% ) 266 ( 41% ) 211 ( 40% ) 199 ( 40% ) mpr , multiplanar reconstruction ; mip , maximum intensity projection ; vr , volume rendering nodules > 10 mm , 100% . 
in particular , sensitivity for nodules 5 mm was 51%54% and for nodules 610 mm , > 10 mle ricostruzioni mpr sagittali hanno evidenziato globalmente 253258 metastasi ed hanno dimostrato sensibilit media del 33% ; in particolare la sensibilit stata del 21% per noduli di diametro 5 mm , del 45%47% per noduli di diametro compreso tra 6 e 10 mm e del 98% per noduli di diametro > 10 m le ricostruzioni mip assiali hanno evidenziato complessivamente 687699 metastasi ed hanno 960 radiol med ( 2008 ) 113 : 954967 80%85% . 
axial , coronal and sagittal vr reconstructions showed a sensitivity of 100% in detecting nodules > 10 mm . statistical analysis performed with students t test for both observers demonstrated that : 1 . 
in detecting pulmonary nodules > 10 mm in diameter , axial source images and mpr , mip and vr reconstructions were equivalent to the gold standard ( p > 0.05 ) , with sensitivity values from 94% to 100% 2 . 
in recognition nodules between 6 mm and 10 mm in diameter , only vr and mip reconstructions showed high consistency with the gold standard ( p > 0.05 ) and sensitivity values of 80%89% ; on the contrary , 2d reconstructions ( p < 0.05 ) had a sensitivity of 45%53% 3 . 
moreover , coronal and sagittal mpr , mip and vr reconstructions did not significantly improve the assessment of the number and size of the nodules compared with the corresponding axial images . 
there is still no consensus as to whether it is useful to perform chest ct in all patients with ascertained cancer [ 3 ] , although it is generally agreed that this examination should dimostrato una sensibilit media dell89 , 5% ; in particolare la sensibilit stata dell87%89% per noduli di diametro 5 mm , 90% per noduli di diametro compreso tra 6 e 10 mm e 100% per noduli di diametro > 10 m le ricostruzioni mip coronali hanno evidenziato globalmente 652656 metastasi ed hanno mostrato una sensibilit media dell84 , 5% ; in particolare la sensibilit stata dell81%82% per noduli di diametro 5 mm , dell87% per noduli di diametro tra 6 e 10 mm e 100% per noduli di diametro > 10 mle mip sagittali hanno evidenziato complessivamente 646650 metastasi ed hanno dimostrato una sensibilit media dell83% ; in particolare la sensibilit stata dell80%81% per noduli di diametro 5 mm , dell87% per noduli di diametro compreso tra 6 e 10 mm e del 100% per noduli di diametro > 10 mle ricostruzioni vr assiali hanno evidenziato globalmente 500529 metastasi ed hanno dimostrato una sensibilit media del 66 , 5% ; in particolare la sensibilit stata del 55%58% per noduli di diametro 5 mm , dell80%85% per noduli di diametro compreso tra 6 e 10 mle ricostruzioni vr coronali hanno evidenziato globalmente 482507 metastasi ed hanno dimostrato una sensibilit media del 63 , 5% , in particolare del 51%54% per noduli di diametro 5 mm e dell80%85% per noduli di diametro compreso tra 6 e 10 mm ; le vr sagittali hanno evidenziato globalmente 480502 metastasi ed hanno mostrato una sensibilit media del 63 , 5% , in particolare del 51%54% per noduli di diametro 5 mm , dell80%84% per noduli di diametro compreso tra 6 e 10 mle ricostruzioni vr assiali , coronali e sagittali hanno dimostrato una sensibilit del 100% per noduli di diametro > 10 mm . dall analisi statistica di questi risultati , effettuata con il test t di student , si evince che per entrambi gli osservatori : 1 . 
c immagine assiale mip : riconoscibile il piccolo nodulo nel lobo inferiore sinistro ( freccia ) e sono , inoltre , evidenti due noduli nel lobo inferiore omolaterale e nel lobo medio ( teste di freccia )  . tati ottenuti considerando i rapporti dei noduli con le strutture del lobulo polmonare secondario sono riportati nelle tabelle 2 e 3 relative rispettivamente allosservatore 1 e allosservatore 2 . 
tutti i tumori , ad eccezione dei tumori cerebrali , possono metastatizzare nel parenchima polmonare che rappresenta un filtro per le cellule neoplastiche presenti nel circolo ematico e nel sistema linfatico [ 17 ]  . 
lutilit di eseguire una tc del torace in tutti i pazienti con patologia neoplastica accertata ancora oggetto di discussione [ 3 ] , al contrario ormai condivisa , come sottolineato in letteratura , lopportunit di eseguire lindagine nei casi in cui il tumore primitivo presenti propensione a metastatizzare al polmone o qualora la presenza di localizzazioni secondarie polmonari determini un cambiamento nel programma terapeutico [ 18 ]  . 
in passato a tal fine veniva utilizzata la radiografia del torace , ma gi da anni stata dimostrata la superiorit della tc [ 4 , 19 ] , anche se di tipo convenzionale , con risultati di sensibilit segnalati in letteratura del 44%56% per la radiografia del torace e del 68%78% per la tc [ 3 , 5 , 6 ]  . 
la superiorit della tc in rapporto ad una maggiore risoluzione di contrasto tra nodulo e parenchima polmonare ed ad un pi agevole riconoscimento delle lesioni in assenza di sovrapposizione di strutture quali parete toracica , mediastino , diaframma e vasi [ 20 ]  . nellambito della tecnologia tc , un incremento nella identificazione dei noduli polmonari derivato dalla diffusione delle apparecchiature spirali [ 8 , 21 ] che forniscono immagini volumetriche e riducono il numero delle lesioni non identificate in rapporto allescursione respiratoria ed alle pulsazioni cardiache , con valori di sensibilit riportati in letteratura del 79% e di specificit del 91% [ 11 ] conside962 radiol med ( 2008 ) 113 : 954967 fig . 
 ( c ) immagine coronale mpr : il segno del vaso non evidente . radiol med ( 2008 ) 113 : 954967 be performed in all cases in which the primary tumour is likely to metastasise to the lung or cases in which the presence of secondary pulmonary localisations has dictated a change in the therapeutic schedule [ 18 ]  . 
although chest x - rays were once used , it has long been demonstrated that ct , including conventional ct , is far superior [ 4 , 19 ] , yielding a sensitivity of 68%78% as opposed to 44%56% for chest x - rays [ 3 , 5 , 6 ]  . 
this superiority is attributable to the greater contrast resolution between the nodule and the lung parenchyma and easier detection of lesions , thanks to elimination of the superimposition of structures such as the chest wall , mediastinum , diaphragm and vessels [ 20 ]  . the advent of spiral ct devices has dramatically increased the detection rate of pulmonary nodules [ 8 , 21 ] , thanks to volumetric imaging and reduction of the rate of false negatives due to respiratory movements and the heart beat . 
the new devices are reported to have an overall sensitivity of 79% and specificity of 91% [ 11 ] in diagnosing metastatic lesions , whatever their diameter , and a sensitivity of 47%69% for nodules with a diameter < 67 mm [ 12 ]  . 
it has been shown that the increased sensitivity of spiral ct compared with conventional ct is inversely proportional to lesion diameter , being most evident in nodules with a diameter < 1 cm [ 8 ]  . 
the advantages of spiral ct are compounded by reconstruction techniques using partially overlapping slices , which reduce the risk of failing to detect a nodule located in an area of lung parenchyma missing in the slices [ 2224 ]  . 
in this sense , the main drawback of single - detector spiral ct is the minimal collimation value , which cannot be < 57 mm , to assess the whole lung parenchyma in a single inspiratory breath - hold [ 10 ]  . in the study of pulmonary metastases , the introduction of msct devices enabled scanning times to be reduced and hence the whole chest to be assessed during a single breathhold , even using collimation values of 3.0 mm or less [ 7 ]  . moreover , msct can provide high - resolution isotropic voxel data , which are essential for achieving high - quality mpr and 3d reconstructions [ 13 ]  . 
used mip reconstructions of axial images obtained with a dual - slice scanner and a collimation thickness of 3 mm , reporting a 2.8 - fold increase in detecting pulmonary nodules compared with conventional imaging [ 29 ]  . 
in a study by gruden et al . , mip reconstructions improved the accuracy pulmonary lesion diagnosis , esperando complessivamente lesioni metastatiche , indipendentemente dal loro diametro , ed una sensibilit del 47%69% per noduli con diametro inferiore a 67 mm [ 12 ]  . 
inoltre stato dimostrato che lincremento della sensibilit della tc spirale rispetto alla tc convenzionale inversamente proporzionale al diametro delle lesioni ed soprattutto evidente nei noduli di diametro inferiore ad 1 cm [ 8 ]  . 
i vantaggi della tc spirale sono ampliati , in fase di ricostruzione , dallimpiego di sezioni parzialmente sovrapposte che riducono il rischio di mancato riconoscimento dei noduli localizzati nel parenchima polmonare non compreso nelle sezioni [ 2224 ]  . 
a tale proposito il principale limite della tc spirale a singolo detettore rappresentato dal valore minimo di collimazione che per valutare interamente il parenchima polmonare in ununica apnea non pu essere inferiore a 57 mm [ 10 ]  . nello studio delle metastasi polmonari una maggiore accuratezza diagnostica derivata dallintroduzione delle apparecchiature tc dotate di sistemi di acquisizione multistrato ( tcms ) che consentono la riduzione del tempo di acquisizione e quindi permettono di valutare in una singola apnea lintero torace anche impiegando valori di collimazione pari o inferiori a 3 , 0 mm [ 7 ]  . 
nellambito delle ricostruzioni particolarmente utile appare il ricorso alle mip che , come riportato in letteratura , evidenziano in maniera ottimale le strutture vascolari , riducono il numero di immagini da valutare e facilitano il riconoscimento delle lesioni nodulari [ 8 , 2628 ]  . 
 [ 29 ] hanno utilizzato le ricostruzioni mip su immagini assiali ottenute con uno scanner dual slice con spessore di collimazione di 3 mm ed hanno dimostrato nellindividuazione dei noduli polmonari un incremento di 2 , 18 volte rispetto alle immagini convenzionali . 
 [ 10 ] , limpiego delle ricostruzioni mip migliora laccuratezza nella diagnosi delle lesioni nodulari polmonari in particolare di quelle peri - ilari ed inoltre , riduce la variabilit tra i diversi osservatori nella individuazione della patologia . 
 [ 30 ] hanno confrontato le ricostruzioni mip e vr nella ricerca di noduli polmonari ed hanno riportato valori di sensibilit , in rapporto alle dimensioni delle lesioni , 964 radiol med ( 2008 ) 113 : 954967 cially perihilar lesions , and also reduced observer bias . 
the rate of misdiagnosed lesions was estimated to be 20%39% using axial scans and only 12% when using mip reconstructions [ 10 ]  . in an investigation of mip success rate in detecting pulmonary metastatic nodules , diederich et al . 
according to these authors , detecting a greater number of nodules with vr reconstructions is attributable to better spatial depiction of the pulmonary anatomical structures and a virtual magnification of their size , which makes them easier to identify [ 30 ]  . 
 [ 31 ] , in a recent paper comparing axial - source images , mip reconstructions and use of a computer - assisted detection system ( cad ) in the search for pulmonary nodules , revealed that mip was more sensitive for nodules 3 mm and less time consuming than the use of cad . 
the cad system presents interesting perspectives in the study of pulmonary nodules [ 3137 ] , but studies comparing the capabilities of different reconstructions with cad are still too limited to define the most accurate methodology . the results obtained in our study showed that coronal and sagittal mpr reconstructions yielded no diagnostic improvement with respect to axial - source images in detecting pulmonary nodules , presenting essentially equivalent sensitivity values ( 33%36% )  . 
however , only mip reconstructions can be considered a valid diagnostic tool in detecting nodules 5 mm , with a sensitivity of 80%89% in contrast to vr , which presents values of 51%57% . 
in determining the number of nodules detected , our study has the limitation of not having calculated specificity values , which clearly cannot be done without histological examination of surgical specimens . 
as reported in the literature , for this purpose , it is essential to precisely define the distribution and anatomical location of the disease with respect to the secondary facile compresi per le immagini mip tra 45 , 1%91 , 9% e per le immagini vr tra 76 , 5%97 , 3% . 
secondo questi autori il riconoscimento di un maggior numero di noduli con le ricostruzioni vr sarebbe da attribuire ad una migliore rappresentazione spaziale delle strutture anatomiche polmonari e ad un aumento virtuale delle dimensioni degli stessi che ne individuazione [ 30 ]  . permetterebbero una pi jankowski et al . 
 [ 31 ] in un recente lavoro hanno confrontato i risultati ottenuti con le immagini assiali , le mip e limpiego di un software di computed assisted detection ( cad ) nella ricerca di noduli polmonari ed hanno riscontrato una maggiore sensibilit delle ricostruzioni mip per noduli di diametro 3 mm e la necessit di un tempo minore per la lettura delle immagini mip rispetto a quello necessario utilizzando il sistema cad . 
certamente tale software presenta interessanti prospettive nello studio dei noduli polmonari [ 3137 ] , ma allo stato attuale le esperienze in cui siano state confrontate le potenzialit delle varie ricostruzioni rispetto al cad sono troppo limitate per poter definire la metodologia pi accurata . i risultati del nostro studio hanno evidenziato che le ricostruzioni mpr coronali e sagittali non apportano alcun vantaggio diagnostico rispetto alle immagini assiali di base nella ricerca dei noduli polmonari , presentando valori di sensibilit tra loro equivalenti ( 33%36% ) ed hanno confermato quanto riportato in letteratura riguardo ai vantaggi offerti dalle ricostruzioni mip e vr . 
in particolare , i risultati forniti dalle immagini mip e vr sono sovrapponibili per lesioni di diametro compreso tra 6 e 10 mm con valori di sensibilit dell85%89% , mentre nella dimostrazione dei noduli di diametro 5 mm solo le ricostruzioni mip costituiscono un valido strumento diagnostico con sensibilit dell80%89% , a differenza delle vr che presentano valori del 51%57% . 
nel valutare il numero di lesioni riconoscibili , nel nostro lavoro esiste il limite rappresentato dal fatto che non sono stati calcolati valori di specificit , che ovviamente non possono essere ottenuti in maniera precisa in assenza di controlli su pezzi anatomici . il secondo problema diagnostico da affrontare nei pazienti con lesioni polmonari nodulari rappresentato dalla necessit di definire con precisione la distribuzione e la localizzazione anatomica della patologia rispetto al lobulo polmonare secondario , infatti tutti gli algoritmi per la caratterizzazione della patologia multinodulare considerano la loro localizzazione centrolobulare , perilinfatica e random [ 38 , 39 ]  . 
this distribution occurs because the neoplastic cells reach the lungs through the bloodstream but can also cross the endothelium of the arterioles and capillaries and distribute within the perivascular tissues [ 41 ]  . 
 [ 42 ] studied the relationship between pulmonary metastases < 3 mm in diameter and centrilobular structures , reporting that only about 12% of pulmonary metastases were centrilobular , with about 68% being located between the centrilobular structures and the interlobular septa and 20% at the level of the interlobular septa . our mip and vr reconstructions yielded comparable results , as 65% of nodules were centrilobular and 35% interlobular . for nodules with a random distribution , differential diagnosis must be made among haematogenous metastases , miliary tuberculosis , mycotic infections , viral diseases , langerhans cells histiocytosis , silicosis and other forms of pneumoconiosis [ 38 , 39 , 43 ]  . 
this differential diagnosis of pulmonary metastases can generally be made on the patients clinical data , but it is always advisable to consider ct signs of the nodules , as these can make a valuable contribution to the diagnosis . 
an important element in this context is the mass - vessel sign , indicative of haematogenous spread , demonstrated by a close relationship between the nodule and the centrilobular arterial branch [ 44 , 45 ]  . this sign has been described as significant but not exclusive to secondary pulmonary lesions , as it can also be observed in cases of pulmonary infarction or septic emboli [ 44 , 45 ]  . 
 [ 42 ] showed that the mass - vessel sign was not detectable , presumably because the vessels supplying the lesions are too small to be visualised by hrct , whereas it appears in only 27% of cases of larger metastatic lesions ( with a diameter > 3 mm )  . 
 [ 46 ] , in a study of ten patients with pulmonary metastases , detected the mass vessel sign in 38% of nodules on axial source images , whereas it was recognizable in 15% of nodules only on the mip images . the authors emphasised that with mip images , it was possible to demonstrate that the mass - vessel sign was caused by a strict connection between the nodule and a venous vessel . 
in our study based on 32 patients , we tano una distribuzione random e rispetto al lobulo secondario , si possono localizzare in rapporto alle strutture centrolobulari , a livello dei setti interlobulari e nellinterstizio subpleurico [ 3840 ]  . 
tale distribuzione si determina poich le cellule neoplastiche raggiungono il polmone per via ematogena , ma possono attraversare lendotelio delle arteriole e dei capillari e distribuirsi nei tessuti perivascolari [ 41 ]  . 
 [ 42 ] hanno studiato su sezioni anatomiche la relazione tra metastasi polmonari con diametro inferiore a 3 mm e strutture centrolobulari ed hanno riportato che solo il 12% circa delle metastasi polmonari erano centrolobulari , il 68% circa era situato tra strutture centrolobulari e setti interlobulari ed il 20% circa dei noduli erano localizzati a livello dei setti interlobulari . 
considerando le ricostruzioni mip e vr i risultati da noi ottenuti sono sostanzialmente sovrapponibili , infatti abbiamo riscontrato il 65% di noduli centrolobulari ed il 35% di noduli interlobulari . la diagnosi differenziale dei noduli a distribuzione random comprende le metastasi ematogene , la tubercolosi miliare , le infezioni micotiche , le malattie virali , listiocitosi a cellule di langherans , la silicosi ed altre pneumoconiosi [ 38 , 39 , 43 ]  . 
generalmente , considerando i dati clinici del paziente , pu essere ottenuta una differenziazione delle metastasi polmonari dalle altre patologie , tuttavia sempre opportuno considerare la semeiotica tc dei noduli poich in grado di contribuire ad un preciso orientamento diagnostico . a tale proposito un elemento importante da ricercare , poich significativo della diffusione ematogena della patologia , rappresentato dal segno del vaso che si caratterizza per uno stretto rapporto del nodulo con il ramo arterioso centrolobulare [ 44 , 45 ]  . 
tale segno stato descritto come significativo , ma non esclusivo di lesioni secondarie polmonari ed , infatti , si pu osservare anche in caso di infarto polmonare o di emboli settici [ 44 , 45 ]  . 
lincidenza di tale segno nelle metastasi polmonari controversa ed in uno studio di milne e zerhouni [ 44 ] , eseguito con tc ad alta risoluzione ( hrtc ) , compare nel 75% dei noduli metastatici polmonari . al contrario murata et al . 
 [ 42 ] , nella loro esperienza eseguita con hrct , hanno riportato che nei piccoli noduli il segno del vasonon riconoscibile poich presumibilmente i vasi afferenti alle lesioni sono troppo piccoli per essere visualizzati e nelle lesioni metastatiche pi voluminose ( con diametro superiore a 3 mm ) compare solo nel 27% dei casi . 
 [ 46 ] , in uno studio condotto su 10 pazienti con metastasi polmonari , hanno riscontrato nelle immagini assiali di base il segno del vaso nel 38% dei noduli , mentre nelle immagini mip compariva soltanto nel 15% dei noduli . inoltre , in base a quanto sottolineato dagli autori , nelle immagini mip era possibile dimostrare che il segno del vaso era determinato da uno stretto rapporto tra nodulo ed una struttura vascolare venosa . 
nel nostro studio , condotto su 32 pazienti , il segno del vaso stato riconosciuto nel 29% dei casi nelle immagini assiali , mentre nel 41%42% 966 radiol med ( 2008 ) 113 : 954967 detected the mass - vessel sign in 29% of cases on axial source images and in 41%42% of cases on mip and vr images . 
 [ 46 ] , and in our experience , mip and vr reconstructions increased the incidence of the mass - vessel sign . however , lacking any histological examination , it was not possible to define whether the centrilobular arterial branch actually entered the nodule or was only contiguous to it . conclusions our study has some limitations related to its retrospective design and lack of pathological correlation of the ct findings . 
 our results with msct in studying patients with suspected pulmonary metastases show that mip reconstructions should be considered an essential methodological tool , as they can increase the detection rate and improve characterisation of small nodular lesions . 
 dei casi nelle immagini mip e vr e grazie allimpiego di queste ricostruzioni , inoltre , stato pi agevole dimostrare la natura arteriosa del vaso in rapporto con i noduli . i nostri risultati , pertanto , sono discordanti da quelli riportati nel lavoro di dodd et al . 
 [ 46 ] e , nella nostra esperienza , le mip e le vr implementano lincidenza del segno del vaso ; in assenza di un controllo istologico , tuttavia , non possibile stabilire se larteriola centrolobulare penetri allinterno del nodulo o abbia soltanto un rapporto di contiguit . conclusioni il nostro lavoro presenta alcuni limiti , poich condotto in maniera retrospettiva ed privo di un controllo anatomico delle immagini tc . 
from august 2001 to august 2006 , 95 patients ( 49 men and 46 women ; mean age 61 years , range 2592 ) with 107 abscesses underwent imageguided percutaneous drainage . 
thirty - one abscesses were retroperitoneal ( 9 peripancreatic , 17 perirenal , 5 pararenal ) , 37 intraperitoneal ( 2 in communication with the small bowel ) , 8 intrahepatic ( 2 in communication with the extrahepatic biliary system and 2 with the intrahepatic biliary system ) , 4 perisplenic and 27 pelvic ( 4 in communication with the large bowel )  . 
dallagosto 2001 allagosto 2006 , 95 pazienti ( 49 uomini e 46 donne , et media 61 anni , range 2592 ) portatori di 107 raccolte sono stati sottoposti a drenaggio percutaneo imaging guidato . 
trentuno raccolte erano retroperitoneali ( 9 peripancreatiche , 17 perirenali , 5 pararenali ) , 37 intraperitoneali ( 2 comunicanti con lintestino tenue ) , 8 intra - epatiche ( 2 in comunicazione con il sistema biliare extraepatico e 2 con il sistema biliare intraepatico ) , 4 peri - spleniche e 27 pelviche ( 6 comunicanti con lintestino crasso )  . 
la procedura percutanea si dimostrata tecnicamente fattibile ed efficace nel trattamento delle raccolte addominali e pelviche proponendosi in parte come tecnica propedeutica , in prevalenza come valida 1000 radiol med ( 2008 ) 113 : 9991007 procedure does not , however , preclude a subsequent surgical operation . alternativa alla chirurgia tradizionale che peraltro non viene preclusa in caso di insuccesso . keywords abdominal percutaneous abscesses percutaneous drainage interventional radiology parole chiave ascessi addomino pelvici drenaggio percutaneo radiologia interventistica introduction introduzione thanks to technological advances in diagnostic imaging and the development of interventional radiology materials and techniques , image - guided percutaneous drainage of fluid collection has come to play an important role in patients at high surgical risk because of cardiorespiratory comorbidities . 
however , in many cases imageguided percutaneous drainage of fluid collection has become the first - line treatment , as it is less invasive and has a lower rate of periprocedural complications [ 4 ]  . 
the aim of this study was to evaluate the feasibility and effectiveness of image - guided percutaneous drainage in selected patients by determining both the technical and clinical success of the procedure . grazie al progresso tecnologico della diagnostica per immagini e allinnovazione dei materiali e delle procedure di radiologia interventistica attualmente il drenaggio delle raccolte mediante approccio percutaneo imaging - guidato gioca un ruolo importate nei pazienti ad alto rischio chirurgico per comorbilit cardio - respiratorie ; pu essere risolutivo ed evitare il reintervento . 
chiaramente la corretta diagnosi una condizione fondamentale per la gestione di questi pazienti in quanto un ritardo nel trattamento comporta un aumento dei tassi di mortalit e morbilit [ 1 ]  . infatti le raccolte ascessuali non drenate presentano una percentuale di mortalit tra l80% e il 100% che si riduce significativamente nei pazienti trattati chirurgicamente [ 14 ]  . 
attualmente imagingguidato nel trattamento delle raccolte , per le sue caratteristiche di minor invasivit e minor tasso di complicanze periprocedurali , rappresenta in molti casi lopzione terapeutica di prima scelta [ 4 ]  . 
lobiettivo di questo studio quello di dimostrare la fattibilit e lefficacia del drenaggio percutaneo imaging - guidato in pazienti selezionati , valutando sia il successo tecnico che il successo clinico . lapproccio percutaneo materials and methods materiali e metodi between august 2001 and august 2006 , image - guided percutaneous drainage was carried out on 95 patients ( 49 men and 46 women ; mean age 61 years , age range 2592 ) with 107 fluid collections ( 6 patients had two abscesses and 3 had 3 )  . 
thirty - one collections were retroperitoneal ( 9 peripancreatic , 17 perirenal , 5 pararenal ) , 37 were intraperitoneal ( 2 communicating with the small bowel ) , 8 were intrahepatic ( 2 communicating with the extrahepatic biliary system and 2 with the intrahepatic biliary system ) , 4 were perisplenic and 27 were pelvic ( 4 communicating with the large bowel )  . 
in all cases , 8to 14 - fr drainage catheters were used . in 68 / 95 patients , the abscesses were postoperative and followed surgery for malignancy ( 42 ) , inflammatory disease ( 13 ) , kidney transplant ( 6 ) , orthopaedic disorders ( 3 ) , polytrauma ( 2 ) and abdominal aorta aneurysms ( 2 )  . 
 in the remaining 27 / 95 patients , the abscesses developed as a complication of diverticular disease ( 16 ) , acute pancrenel periodo compreso tra agosto 2001 e agosto 2006 , 95 pazienti ( 49 uomini e 46 donne , et media 61 anni , range 2592 ) portatori di 107 raccolte ( 6 pazienti con 2 ascessi e 3 pazienti con 3 ) sono stati sottoposti a drenaggio per cutaneo imaging - guidato . 
trentuno raccolte erano retroperitoneali ( 9 peripancreatiche , 17 perirenali , 5 pararenali ) , 37 intraperitoneali ( 2 comunicanti con lintestino tenue ) , 8 intra - epatiche ( 2 in comunicazione con il sistema biliare extraepatico e 2 con il sistema biliare intraepatico ) , 4 peri - spleniche e 27 pelviche ( 4 comunicanti con lintestino crasso )  . 
settantuno procedure su 107 sono state realizzate sotto guida ecografica , 36 / 107 sotto guida tc utilizzando drenaggi percutanei di calibro variabile tra 814 fr . in 68 / 95 pazienti , lascesso si verificato in seguito ad intervento chirurgico : oncologico ( n = 42 ) , per patologia infiammatoria ( n = 13 ) , per trapianto di rene ( n = 6 ) , per intervento ortopedico ( n = 3 ) , per politrauma ( n = 2 ) e per aneurismi dellaorta addominale ( n = 2 )  . 
nei rimanenti 27 / 95 pazienti , le raccolte ascessuali sono state una complicanza della malattia diverticolare ( n = 16 ) , della pancreatite radiol med ( 2008 ) 113 : 9991007 1001 fig . 
b , c computed tomography ( ct ) ( contiguous axial images in the venous phase ) : multiloculated lesion with central septations and homogeneous content with density slightly greater than that of the fluid in the posterior pararenal region and partially invading the quadratus lumborum and iliopsoas muscle . 
raccolta pluriloculata con sepimentazioni centrali e contenuto omogeneo a densit poco superiore a quella del liquido indovata in prevalenza nello spazio pararenale posteriore che in parte penetra il muscolo quadrato dei lombi e il muscolo ileo - psoas . 
 atitis ( 8 ) and sepsis in immunosuppressed patients ( 3 )  . the suspicion of a fluid collection was based on clinical and laboratory findings and confirmed by us and ct . 
on imaging , abscesses are characterised by a thick rim of peripheral granulation tissue ( hyperechoic or hyperdense at us and ct , respectively ) and heterogeneous content with a ct density slightly higher than fluid . 
 acuta ( n = 8 ) e di uno stato settico in pazienti immunodepressi ( n = 3 )  . il sospetto di raccolta ascessuale , posto sulla base dei rilievi clinico - laboratoristici , stato poi confermato mediante ecografia e tc . 
lascesso si caratterizzata per uno spesso cercine di granulazione periferico ( iperecogeno o iperdenso rispettivamente allecografia e alla tc ) e contenuto disomogeneo a densit ( con la tc ) poco superiore al liquido con possibili sepimentazioni ed inclusi aerei nel contesto ( figg . 1ac e 2a , b )  . 
i pazienti con presunta diagnosi di ascesso sono stati sottoposti a trattamento antibiotico empirico a largo spettro prima della procedura ; in seguito la terapia veniva modificata sulla base dellantibiogramma effettuato sul prelievo colturale realizzato durante la procedura . 
2a - e hepatic abscess in communication with the intrahepatic biliary systea , b computed tomography ( ct ) [ a sagittal multiplanar reconstruction ( mpr ) ; b coronal mpr ] : abscess in the sixth hepatic segment communicating with the dilated intrahepatic biliary system ( arrow )  . 
c cholangiography : opacification of the intrahepatic biliary system ; dilatation of the biliary system with leakage of contrast medium in the hepatic abscess , where the pigtail drainage catheter is recognisable ( arrow )  . 
c colangiografia : opacizzazione delle vie biliari intra - epatiche : dilatazione delle vie biliari con spandimento di mdc che opacizza lascesso epatico nel cui contesto riconoscibile drenaggio a pig - tail ( freccia )  . 
e controllo tc dopo 3 mesi ( ricostruzione mpr sagittale ) : risoluzione dellascesso epatico e della dilatazione delle vie biliari . radiol med ( 2008 ) 113 : 9991007 1003 ance ( technos mpx , esaote , genoa , italy ) , whereas ct guidance ( lightspeedplus , ge , milwaukee , wi , usa and aquilion 64 , toshiba , tokyo , japan ) was preferred in 36 cases showing lack of an adequate acoustic window or inaccessible location of the collection . 
the cannula was then removed , the access site was crossed with fascial dilators of increasing diameter from 6 fr up to 12 fr ( cook , bloomington , in , usa ) and the pigtail drainage catheter was finally positioned . 
 in tutti i casi stata effettuata una puntura imagingguidata mediante ago - cannula ( tla needle sheath 19g , boston scientific , ratingen , germania ) e successivamente estratto lago attraverso la cannula stata avanzata nel contesto della raccolta una guida rigida 0 , 035 ( amplatz , boston scientific ratingen , germania )  . 
rimossa la cannula il sito daccesso stato poi attraversato con dilatatori fasciali di calibro progressivamente crescente 681012 f ( cook , bloomington , in , usa ) ed stato infine posizionato il catetere di drenaggio con estremo distale a pig - tail . 
il follow - up stato effettuato mediante esame ecografico e tc , valutazione clinica e laboratoristica durante il primo mese . results risultati immediate technical success , defined as correct placement of the distal tip of the drainage catheter inside the abscess cavity , was achieved in 100% of cases . 
despite fixation of the drainage catheter to the skin with sutures , there were 12 / 107 cases of catheter displacement and 6 / 107 cases of obstruction that could not be crossed with a metal guidewire or recanalised by saline irrigation . 
these cases ( 18 / 107 ) necessitated a second procedure to replace the drainage catheter . the volume of fluid drained from the 107 collections ranged from 5 ml to 8 , 500 ml ( mean 440 ml )  . 
fluid culture il successo tecnico immediato , per il corretto posizionamento dellestremo distale del catetere di drenaggio nel contesto della raccolta , stato ottenuto nel 100% dei casi . non si sono registrate complicanze peri - procedurali maggiori quali perforazione di anse e sanguinamenti che hanno richiesto il trattamento chirurgico . 
in 1 paziente , in seconda giornata , si assistito ad una progressiva emorragia venosa con anemizzazione sviluppata dopo il drenaggio di un ascesso epatico e controllata con trasfusione di 2 unit di sangue ; in 1 paziente si osservata una transitoria batteriemia . 
il tasso di mortalit a 30 giorni dalla procedura stato del 3 , 2% ( 3 / 95 ) per cause tuttavia non correlate alla procedura ma alla malattia di fondo ( patologia neoplastica ) in fase avanzata . 
malgrado lancoraggio del drenaggio con punti di sutura alla cute , si sono verificati 12 / 107 sposizionamenti e in 6 / 107 casi lostruzione del catetere , non valicata n con guida metallica , n ricanalizzata mediante liniezione di soluzione fisiologica . in questi casi ( 18 / 107 ) stata necessaria la sostituzione del drenaggio mediante nuova procedura . 1004 radiol med ( 2008 ) 113 : 9991007 yielded 260 bacterial species , with a prevalence of bacteroides spp ( 17% ) , escherichia coli ( 17% ) and enterococcus spp ( 10% )  . 
nine out of 107 cases necessitated surgery ( repair of dehiscence of intestinal anastomosis in five cases and debridement of a multiloculated collection with predominant corpuscular component in four abscesses secondary to acute pancreatitis )  . il volume del materiale drenato delle 107 raccolte variava da 5 a 8500 ml ( media : 440 ml )  . 
hanno prevalso bacteroidi ( 17% ) , escherichia coli ( 17% ) , enterococchi ( 10% )  . nel 67% delle raccolte lascesso era polimicrobico . complessivamente il drenaggio rimasto in sede da 2 a 120 giorni ( media : 14 , 2 giorni ) ; nelle raccolte fistolizzate con lintestino rimasto in sede in media 22 , 3 giorni ; tra le raccolte intrae peri - epatiche quelle non in comunicazione con il sistema biliare hanno richiesto un tempo medio di drenaggio di 16 , 1 giorni , mentre quelle in comunicazione un tempo medio di 49 , 7 giorni . complessivamente si dunque assistito al successo clinico in 98 / 107 ( 91 , 5% ) raccolte documentato dalla risoluzione del quadro clinico e dalla scomparsa o riduzione dimensionale della raccolta . 
in 9 / 107 casi stato necessario lintervento chirurgico ( correzione di deiscenza anastomotica intestinale in 5 casi ; toilette chirurgica di raccolta pluriconcamerata a prevalentemente componente corpuscolata in 4 casi in esiti di pancreatite acuta )  . discussion discussione one of the major advances in the management of abscesses over the past two decades has been the introduction of image - guided percutaneous drainage procedures [ 5 , 6 ]  . 
the development of improved imaging modalities , together with broad - spectrum antibiotics and new drainage catheters , has changed the management of patients with infected intraabdominal fluid collections that previously required an urgent operation [ 5 , 6 ]  . 
the earliest experiences with imageguided percutaneous drainage of intra - abdominal fluid collection date back to the late 1970s , when gerzof et al . reported a success rate of 86% in 67 patients treated with the procedure [ 7 ]  . 
additional reports published during the next several years demonstrated and confirmed the efficacy of the procedure , with success rates ranging from 70% to 100% [ 3 , 5 , 819 ]  . percutaneous drainage has therefore become a consolidated procedure , with lower mortality rates ( 1.4%15% ) compared with surgical drainage [ 911 , 20 ] , even though the differences in mortality , morbidity and success rates in one report did not reach statistical significance [ 12 ]  . 
lower success rates , between 71% and 88% , were reported for abscesses in communication with the gastrointestinal tract compared with those not showing communication [ 2123 ]  . in our series , 5 / 6 abscesses communicating with the large and small bowel were treated successfully . 
il miglioramento e lintroduzione di nuove metodiche di imaging , lavvento di antibiotici a largo spettro e nuovi cateteri di drenaggio ha modificato lapproccio e la gestione di pazienti portatori di raccolte infette intra - addominali , che precedentemente richiedevano un intervento chirurgico urgente [ 5 , 6 ]  . 
negli anni successivi altre esperienze hanno dimostrato e confermato lefficacia di questa procedura con tassi di successo compresi tra 70%100% [ 3 , 5 , 819 ]  . il drenaggio percutaneo si dunque trasformato oggi in una procedura consolidata con tassi di mortalit pi bassi rispetto al drenaggio chirurgico , variabile tra 1 , 4% e 15% [ 911 , 20 ] , anche se alcuni autori non hanno segnalato differenze statisticamente significative fra la mortalit , la morbilit ed i tassi di successo di drenaggio percutaneo e chirurgico [ 12 ]  . 
i tassi pi bassi di successo che variano da 71% a 88% sono stati segnalati per gli ascessi in comunicazione col tratto gastrointestinale rispetto a quelli non comunicanti [ 2123 ]  . 
tuttavia , il tempo medio di drenaggio pi lungo in questo gruppo ( 22 , 3 vs 14 , 2 giorni )  . radiol med ( 2008 ) 113 : 9991007 1005 biliary systeequivalent success rates have been reported for the drainage of hepatic abscesses with or without intrahepatic biliary communication [ 9 , 19 , 24 ] , the only difference being the longer time required to drain those with biliary communication . 
abscesses in communication with the extrahepatic biliary system necessitate the simultaneous placement of an external - internal biliary drain , as the lack of hepatic parenchymal tamponade and the presence of high pressures of bile within the extrahepatic ducts result in continuous filling of the abscess [ 9 ]  . 
biliary diversion excludes the communication and promotes its closure . percutaneous drainage of splenic abscesses offers an alternative to splenectomy , in particular in patients ineligible for surgery and in young patients for whom preservation of splenic function is desired . 
splenic abscesses are relatively rare occurrences , and the five splenic abscesses treated in our series were successfully resolved , above all thanks to the unilocular structure and low viscosity of the collection [ 2531 ]  . 
in diverticular pelvic abscesses , percutaneous drainage has a 90% rate of clinical success in resolving the infection [ 30 , 31 ] and may obviate the need for surgery or defer surgery to an elective setting . 
drainage may even obviate the need for surgery altogether or facilitate surgery by providing a cleaner surgical field . reported recurrence rates following successful percutaneous drainage range from 1% to 10% [ 9 , 14 , 33 , 34 ]  . 
accidental catheter displacement , inappropriate antibiotic selection and communication between the collection and the gastrointestinal , urogenital and biliary systems are the main causes of recurrence [ 9 , 14 , 20 ]  . 
in their series , surgery was avoided in 56% of cases , thanks to complete evacuation of the cavity [ 34 ]  . mortality is related to the patients underlying disease or immune status and the virulence and resistance of the microorganisms . 
 antibiotic prophylaxis plays a crucial role in treatment . in addition to bacteriostasis , it avoids perforation of the cavity wall and the consequent spread of infection by contiguity , thus minimising the risk of bacteraemia [ 14 , 33 ]  . 
dalla letteratura si evince che il drenaggio degli ascessi epatici con e senza comunicazione biliare intraepatica ha tassi simili di successo [ 9 , 19 , 24 ] e che lunica differenza fra lascesso con comunicazione biliare e lascesso senza comunicazione anche in questi casi il tempo di drenaggio maggiore . 
anche la nostra esperienza concorda con quanto gi segnalato in letteratura : tempo di drenaggio maggiore per le raccolte comunicanti ( media : 49 , 7 giorni ) rispetto a quelle non comunicanti ( media : 16 , 1 giorni )  . 
gli ascessi in comunicazione con il sistema biliare extra - epatico richiedono il posizionamento di un drenaggio biliare percutaneo esterno - interno in quanto la mancanza delleffetto tampone del parenchima epatico e di alte pressioni allinterno dei dotti biliari extraepatici comporta un rifornimento dellascesso [ 9 ] ; il drenaggio biliare consente di drenare la bile e di mettere a riposo il tramite fistoloso , favorendone la chiusura . 
il drenaggio degli ascessi splenici unalternativa alla splenectomia in particolare in pazienti per i quali la chirurgia controindicata ed in pazienti giovani nei quali si desidera preservare la funzionalit splenica . 
 un evenienza abbastanza rara in letteratura ; nella nostra esperienza i 5 ascessi splenici sono stati trattati con successo grazie soprattutto allarchitettura uniloculare e alla fluidit della raccolta [ 2531 ]  . 
il drenaggio percutaneo degli ascessi pelvici diverticolari ha un tasso di successo clinico del 90% nella risoluzione della sepsi [ 30 , 31 ] , pu evitare o posticipare in elezione lintervento chirurgico . 
il drenaggio pu addirittura eliminare lesigenza della chirurgia , o dopo il drenaggio , la chirurgia pu essere effettuata in un campo operatorio meno infetto . i tassi di recidiva segnalati variano dall 1% al 10% dopo drenaggio percutaneo riuscito [ 9 , 14 , 33 , 34 ]  . 
lo sposizionamento accidentale del catetere , le errate scelte antibiotiche , le comunicazioni delle raccolte con il sistema gastrointestinale , urogenitale e biliare , sono state le cause principali di recidiva [ 9 , 14 , 20 ]  . 
nella nostra esperienza , la setticemia ( 1 pazienti ) e la mof ( 1 pazienti ) hanno provocato la morte in due pazienti ( 2 , 8% ) a 30 giorni dopo la procedura . 
 la profilassi antibiotica svolge un ruolo cruciale ; oltre al ruolo batteriostatico evita infatti la perforazione della parete della raccolta e la conseguente diffusione per conti1006 radiol med ( 2008 ) 113 : 9991007 mately 10% [ 9 , 14 ] , may be related to the catheter ( displacement and obstruction ) , the operator ( attempting a us - guided approach in collections in unreachable locations ) , the clinician and nursing personnel ( inappropriate catheter care ) and the patient ( responsible for displacement )  . 
clinical success is clearly dependent on size , location and multiloculated structure of the collection and its communication with adjacent organs . guit minimizzando il rischio di batteremia [ 14 , 33 ]  . 
 le complicanze di questa procedura , segnalate intorno al 10% [ 9 , 14 ] , possono essere relative al catetere ( sposizionameno e ostruzione ) , alloperatore ( azzardare approccio ecografico in raccolte non raggiungibili per sede ) , al clinico e al personale infermieristico ( cura impropria del catetere ) ed al paziente ( responsabile dello sposizionamento )  . 
il supporto delle tecniche di imaging garantisce una precisa localizzazione delle raccolte ed una buona determinazione dei rapporti con le strutture circostanti consentendo cos di evitare complicanze come lesioni vascolari o agli organi adiacenti [ 9 , 12 , 14 ]  . 
vansonnenberg e gerzof [ 14 , 33 ] hanno segnalato i pi alti tassi di complicanza in presenza di ascessi multi - loculati , generalmente di grosse dimensioni in cui un solo drenaggio non bastevole . 
chiaramente il successo clinico in relazione alle dimensioni , alla localizzazione , allarchitettura pluriconcamerata , alla fistolizzazione con organi adiacenti della raccolta . conclusions conclusioni percutaneous drainage plays an important role in treating abdominal and pelvic fluid collections , above all in patients at high surgical risk and those who have recently undergone surgery . 
the radiologist can therefore provide a valuable contribution to both the diagnosis and performance of image - guided percutaneous drainage . il drenaggio percutaneo gioca un ruolo importante , specie in pazienti ad alto rischio chirurgico e nei pazienti gi operati per problematiche riguardanti il reintervento . attualmente rappresenta la tecnica di prima scelta per i tassi pi bassi di morbilit e mortalit rispetto alla chirurgia . 
somatostatin receptor scintigraphy with [ 111in ] diethylene triamine pentaacetate acid ( dtpa ) - octreotide is an accurate method for detecting neuroendocrine tumours ( nets ) but often does not provide clear anatomical localisation of lesions . 
planar and single - photon - emission computed tomography ( spect ) imaging was performed using a dual - head gamma camera equipped with an integrated x - ray transmission system , and the images were first interpreted alone by two nuclear medicine physicians and then compared with spect / ct fusion images together with a radiologist . 
fusion images improved spect interpretation in 23 cases , providing precise anatomical localisation of increased tracer uptake in 20 cases and disease exclusion in sites of physiological uptake in 5 . 
in 10 patients , spect / ct allowed definition of the functional significance of lesions detected by diagnostic ct . spect / ct data modified clinical management in 14 cases by changing the diagnostic approach in 8 and the therapeutic modality in 6 . 
le immagini di fusione hanno migliorato linterpretazione spect in 23 casi , permettendo una precisa localizzazione anatomica dei siti patologici in 20 casi e lesclusione di malattia in siti di accumulo fisiologico in 5 . 
il nostro studio dimostra che la fusione di immagini chiaramente superiore alla sola spect , permettendo una precisa localizzazione delle lesioni individuate e riducendo i risultati falsi positivi . radiol med ( 2008 ) 113 : 10561067 1057 keywords neuroendocrine tumours fusion images spect / ct parole chiave tumori neuroendocrini immagini di fusione spect / tc introduction introduzione neuroendocrine tumours ( nets ) represent a heterogeneous group of neoplasms originating from endocrine cells . 
these tumours may be functioning or nonfunctioning and , according to the new world health organisation ( who ) classification , can be divided into three groups on the basis of degree of differentiation [ 3 ]  . approximately 70% of these neoplasms originate from the gastrointestinal tract , and the majority is able to produce chromogranin a , which represents the most important biological marker of nets . somatostatin receptor overexpression at the cell membrane of several nets constitutes the basis of the clinical use of somatostatin analogues labelled with and emitters for diagnostic and therapeutic purposes , respectively . 
somatostatin receptor scintigraphy ( srs ) with [ 111in ] - diethylene triamine pentaacetate acid ( dtpa ) octreotide is generally considered the first - choice procedure for diagnosing primary and metastatic nets , with the only exception being insulinomas , and its sensitivity is higher if associated with single - photon - emission computed tomography ( spect ) [ 47 ]  . 
on the contrary , computed tomography ( ct ) and magnetic resonance imaging ( mri ) provide anatomical details but are unable to supply precise functional information . although a separate visual analysis of scintigraphic and radiologic images with a subsequent mental integration by the observer sometimes can be sufficient , a more accurate correlation is obtained through image fusion [ 8 ]  . different approaches have been attempted to combine anatomical and functional imaging modalities , each with several advantages and disadvantages [ 9 ]  . 
one disadvantage of this method is the different positioning of the patient during spect and ct acquisition , which leads to a reduction in the quality of the fused images [ 10 ]  . i tumori neuroendocrini rappresentano un eterogeneo gruppo di neoplasie derivanti dalle cellule neuroendocrine , caratterizzati da una bassa incidenza , una bassa attivit proliferativa e talvolta dalla capacit di secernere sostanze biologicamente attive [ 1 ]  . 
tali tumori possono infatti essere funzionanti e non funzionanti e secondo la nuova classificazione approvata dalla who possono essere distinti in tre gruppi in base al grado di differenziazione [ 3 ]  . il 70% di tali tumori origina dal distretto gastroenteropancreatico e nella maggior parte dei casi esprimono la cromogranina a , che a tuttoggi rappresenta il pi importante marker biochimico dei tumori neuroendocrini . 
 questi si caratterizzano inoltre per una maggiore densit dei recettori per la somatostatina rispetto ai tessuti normali , permettendo limpiego di analoghi della somatostatina coniugati ad isotopi gammao beta - emittenti a scopo , rispettivamente , diagnostico e terapeutico . 
la scintigrafia con 111in - dtpa - octreotide ( srs ) comunemente considerata la metodica di imaging di prima scelta nella diagnosi di tumori neuroendocrini primitivi e metastatici , con la sola eccezione dellinsulinoma e la sua sensibilit aumenta se associata a rilevazioni single - photon emission computed tomography ( spect ) [ 47 ]  . 
al contrario la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm ) sono in grado di fornire dettagliate informazioni di tipo anatomico senza tuttavia consentirne la caratterizzazione funzionale . 
 sebbene in molti casi sia sufficiente lanalisi visiva di immagini scintigrafiche e radiologiche ottenute separatamente e la loro successiva integrazione visiva da parte dellosservatore , in alcune situazioni cliniche pu risultare utile una pi accurata correlazione anatomico - funzionale attraverso la fusione di immagini [ 8 ]  . 
un inconveniente di tale metodica rappresentato dal non corretto riposizionamento del paziente durante le due acquisizioni , con conseguente peggioramento della qualit delle immagini di fusione [ 10 ]  . la recente introduzione di una gamma - camera a doppia 1058 radiol med ( 2008 ) 113 : 10561067 recently , a gamma camera with an integrated low - dose x - ray tube for combined transmission and emission tomography has become available ; this procedure is useful for attenuation correction and to acquire anatomical and functional data simultaneously with the same imaging device and without moving the patient [ 11 , 12 ]  . 
consequently , low - dose ct can be insufficient for a full radiological interpretation , and important diagnostic information can be lost [ 10 ]  . the aim of this study was ( 1 ) to assess in a group of patients with neuroendocrine tumours the clinical usefulness of spect / ct image fusion obtained by a gamma camera with an integrated low - dose ct compared to spect images alone , and ( 2 ) to allow definition of the functional significance of lesions detected by diagnostic ct . materials and methods between january 2005 and december 2006 , 61 patients ( 32 women and 29 men ) with known or suspected net ( according to clinical , biochemical or radiological data ) were retrospectively evaluated . 
seven patients ( five men and two women ) were excluded due to lack of data for validation of imaging results . among 54 patients included in the study ( 30 women and 24 men , age range 3080 years , mean 56 years ) , 25 were evaluated for carcinoid tumour ( 15 respiratory and ten gastrointestinal tract ) , 19 for gastroenteropancreatic tumour , five for metastatic lesions with net features , three for medullary thyroid carcinoma and two for paraganglioma . srs was aimed at diagnosis of the primary tumour in two patients , tumour staging in 27 and follow - up in 25 . all patients underwent somatostatin receptor scintigraphy with [ 111in ] - dtpa - octreotide within 1 month from multislice , contrast - enhanced ct ( arterial , portal venous and delayed - phase imaging ) of the chest and / or abdomen and / or pelvis , according to the specific clinical indication . srs was performed after i.v. 
planar views were obtained using a dual - head gamma camera ( infinia vc & hawkeye , ge medical systems ) equipped with an integrated x - ray transmission system ( low - dose ct : v = 140 kev ; a = 2.5 ma ) to provide anatomical maps for attenuation correction and fusion images . 
whole - body scans were obtained 4 h after radionuclide administration and completed by planar views of selected body areas 4 , 24 and , if necessary , 48 h after testa integrata con una tc a basso amperaggio ha permesso di effettuare la correzione per lattenuazione e la fusione di immagini co - registrate nella stessa seduta , senza richiedere il riposizionamento del paziente [ 11 , 12 ]  . 
dallanalisi sono poi stati esclusi 7 pazienti ( 5 uomini e 2 donne ) in cui non erano disponibili dati sufficienti per confermare o escludere la natura maligna delle lesioni rilevate allindagine scintigrafica . dei 54 pazienti inclusi nello studio ( 30 donne e 24 uomini , di et compresa tra 30 e 80 anni , et media 56 anni ) , 25 sono stati valutati per carcinoide ( di cui 15 localizzati a livello toracico e 10 a livello del tratto gastrointestinale ) , 19 per tumore endocrino pancreatico , 5 per metastasi da tumore neuroendocrino di origine sconosciuta , 3 per carcinoma midollare della tiroide e 2 per paraganglioma . 
 tutti i pazienti sono stati sottoposti a scintigrafia con 111in - dtpa - octreotide entro un mese dallesecuzione di un esame tc multistrato torace - addome - pelvi nelle fasi di enhancement vascolare di tipo arterioso , portale e tardivo e con mezzo di contrasto a livello del torace e / o delladdome e / o altra regione anatomica in base allindicazione clinica . srs stata eseguita dopo iniezione ev di 200 mbq di 111indtpa - octreotide . 
le immagini planari e spect sono state ottenute utilizzando una gamma - camera a doppia testa ( infinia vc & hawkeye , ge medical systems ) equipaggiata con un sistema trasmissivo integrato tc ( tc a basso amperaggio : v = 140 kev ; a = 2 , 5 ma ) in modo da ottenere una mappa anatomica per la correzione dellattenuazione e la fusione di immagini . 
il protocollo includeva riprese scintigrafiche whole body a 4 ore , acquisizioni planari statiche della regione cervico - toracica e addominale a 4 e 24 ore , e , solo se ritenuto necessario , a 48 ore dalliniezione del radiol med ( 2008 ) 113 : 10561067 1059 injection . 
after 24 h , spect was performed , and immediately thereafter , a transmission scan of the corresponding region was obtained in 11 m abdominal spect was performed in all patients . 
in addition , spect of the chest was obtained in 17 patients , of the head and neck in six patients and of the pelvis in two patients according to the different clinical situations . 
in the first phase of image analysis , scintigraphy ( planar and spect ) and diagnostic ct studies were evaluated independently by two nuclear medicine physicians and an experienced radiologist , respectively . 
in a second phase ( within 2 weeks ) , fused spect / ct images were analysed and then compared with spect alone and diagnostic ct images . the improvement provided by spect / ct in the interpretation of spect data ( in terms of a precise anatomical localisation of increased tracer uptake and disease exclusion in sites of physiological uptake ) and any modification in therapeutic management were patient diagnostic or recorded . 
the gold standard for confirming the presence or absence of malignancy was either histopathology , available after surgery in 41 patients , or clinical or radiological follow - up over at least 6 months , available for 13 patients . results srs planar and spect images were negative in nine , positive in 43 and of uncertain significance in two of the 54 patients studied . 
in 29 / 54 patients ( 54% ) , including eight negative and 21 positive , spect / ct fusion images did not add any significant information to spect alone . 
the two cases of uncertain significance were classified again as positive and negative , respectively . spect / ct images provided additional information in 25 / 54 patients ( 46% )  . 
fusion images improved spect interpretation in 23 cases ( 42% ) , providing precise anatomical localisation of increased tracer uptake in 20 cases ( 37% ) and disease exclusion in sites of physiological uptake in five ( 9% )  . 
rilevazioni spect addizionali a livello del torace sono state effettuate in 17 casi , di testa e collo in 6 pazienti e della pelvi in 2 casi in base allindicazione clinica . 
in una prima fase le immagini scintigrafiche ( planari e spect ) e quelle ottenute mediante tc diagnostica sono state rispettivamente valutate in maniera indipendente da due medici nucleari e un radiologo esperto . 
in una seconda fase ( entro 2 settimane dalla prima ) sono state analizzate le immagini di fusione spect / tc e quindi confrontate con le immagini spect e quelle della tc diagnostica . ai tre osservatori stato dunque richiesto di registrare eventuali miglioramenti nellinterpretazione dei dati ( in termini di precisa localizzazione della sede di lesione o esclusione di foci di fisiologico uptake ) o modificazioni del management diagnostico o terapeutico dei pazienti studiati , apportati dalla spect / tc rispetto alla sola spect . 
il gold standard per la conferma o lesclusione della natura maligna delle lesioni rilevate allindagine scintigrafica era rappresentato dai dati istopatologici , disponibili dopo asportazione chirurgica in 41 pazienti , o da un follow - up clinico o radiologico superiore a 6 mesi , disponibile in 13 pazienti . risultati le immagini scintigrafiche planari e spect con 111indtpa - octreotide sono risultate negative in 9 , positive in 43 e di non univoca interpretazione in 2 dei 54 pazienti valutati . 
la fusione di immagini spect / tc non ha permesso di ottenere informazioni aggiuntive rispetto alle sole immagini spect in 29 / 54 casi ( 54% ) , includendo 8 studi negativi e 21 positivi . 
le immagini di fusione hanno migliorato linterpretazione delle immagini spect in 23 casi ( 42% ) , permettendo una precisa localizzazione anatomica dei siti di aumentata captazione del radiofarmaco in 20 casi ( 37% ) e lesclusione di malattia in siti di uptake fisiologico in 5 casi ( 9% )  . 
in 10 pazienti ( 18% ) la spect / tc ha permesso la corretta caratterizzazione funzionale di lesioni ( 3 linfonodali , 1 muscolare , 1 cardiaca , 1 vertebrale , 1 1060 radiol med ( 2008 ) 113 : 10561067 vertebra , one bronchus , two pancreas , one sigmoid )  . spect / ct data modified clinical management in 14 cases ( 26% ) by changing the diagnostic approach in eight ( 15% ) and the therapeutic modality in six ( 11% )  . 
la fusione di immagini ha inoltre modificato il management clinico in 14 pazienti ( 26% ) , attraverso un cambiamento dellapproccio diagnostico in 8 ( 15% ) e del piano terapeutico in 6 ( 11% )  . 
in entrambi i casi un successivo follow - up clinico superiore a 6 mesi ha confermato la natura maligna delle lesioni individuate . discussion discussione nets represent a heterogeneous group of neoplasms originating from endocrine glands such as the pituitary , parathyroids and adrenal medulla , as well as endocrine islets within the thyroid or pancreas and neuroendocrine cells dispersed in the digestive and respiratory tracts . 
uptake 1 is an active , sodium and energy - dependent and specific uptake mechanism in the cell membrane of sympathomedullary tissues ; uptake 2 is a nonspecific passive diffusion in the cell membrane of different tissues . 
for these reasons , srs represents the procedure of first choice for the diagnosis of nets , and its sensitivity which varies between 82% and 95% is higher than that of ct and mri [ 47 , 17 ]  . 
 [ 18 ] , in a study carried out on 27 patients , demonstrated that helical ct appeared to be more sensitive than srs in detecting i tumori neuroendocrini costituiscono un eterogeneo gruppo di neoplasie derivanti da ghiandole endocrine come ipofisi , paratiroidi e midollare del surrene o da cellule endocrine localizzate allinterno della tiroide o del pancreas o disperse nel tratto gastro - entero - pancreatico o respiratorio , accomunate da un particolare pattern istologico dovuto alla presenza di specifici prodotti secretori e proteine citoplasmatiche [ 1 , 13 ]  . 
lincidenza dei tumori neuroendocrini generalmente considerata bassa ma tale dato potrebbe essere sottostimato a causa della difficolt nel diagnosticare forme asintomatiche e in stadio iniziale [ 14 ]  . la diagnosi deve dunque basarsi sullintegrazione di dati clinici , di laboratorio , e metodiche di imaging , sia di tipo morfologico ( risonanza magnetica , tc diagnostica , angiografia , ecografia ) che funzionale . 
in medicina nucleare sono infatti numerosi i radiofarmaci proposti per lidentificazione dei tumori neuroendocrini , la maggior parte dei quali basati su specifici meccanismi di uptake [ 15 ]  . 
tra questi i pi importanti sono rappresentati dalla metaiodobenzilguanidina ( 123i o 131i - mibg ) , caratterizzata da una specificit di tipo tessutale , e dal 111in - dtpa - octreotide , la cui specificit di tipo recettoriale . 
luptake di tipo 1 un processo sodio ed energia dipendente , che determina un accumulo del radiofarmaco di tipo specifico nel tessuto simpatico ; luptake di tipo 2 un processo di diffusione passiva che determina un accumulo aspecifico del radiofarmaco in vari tessuti . 
la captazione del 111in - dtpa - octreotide dipende dalla presenza dei recettori della somatostatina sulla membrana cellulare ; tali recettori , suddivisi in 5 sottotipi , sono infatti espressi dalla maggior parte dei tumori neuroendocrini , anche se con diversa incidenza e densit [ 16 ]  . 
per questi motivi srs rappresenta la metodica di prima scelta per lidentificazione dei tumori neuroendocrini e la sua sensibilit , riportata in letteratura tra 82% e 95% , risulta pertanto superiore a quella di tc e rm [ 47 , 17 ]  . 
however , even in the presence of a high density of somatostatin receptors , srs may not be sufficient to provide precise anatomical localisation of increased tracer uptake and , because of the physiological uptake of the tracer , detect abdominal lesions , thus often requiring a correlation with anatomical imaging modalities . 
in most cases it is very difficult to achieve complete alignment of anatomical and functional data obtained by different procedures at different times , for example , as a result of uncontrollable movement of internal organs . 
moreover , these methods require complicated and expensive software and longer imaging times . da tumore neuroendocrino mentre le due metodiche sono risultate simili , in termini di accuratezza , sensibilit e specificit , nellidentificazione del tumore primitivo e delle metastasi epatiche . la sensibilit della scintigrafia con 111in - dtpa - octreotide dipende dalle dimensioni del tumore e dalla densit dei recettori per la somatostatina di tipo 2 e 5 sulla superficie delle cellule tumorali . 
tuttavia anche in presenza di unelevata densit di recettori per la somatostatina la srs pu non essere in grado di localizzare con precisione la sede della lesione individuata e , a causa della fisiologica captazione intestinale del tracciante , di caratterizzare lesioni addominali , necessitando quindi del confronto con altre metodiche di imaging . 
in molti casi non possibile per ottenere un perfetto riallineamento dei dati anatomici e funzionali ottenuti con dispositivi diversi e in giorni diversi , a causa per esempio del movimento degli organi interni . 
in our study , fusion images improved spect interpretation in 23 cases ( 42% ) , providing precise anatomical localisation of increased tracer uptake in 20 cases ( 37% ) and disease exclusion in sites of physiological uptake in five ( 9% )  . 
in 39% of cases , the more precise localisation of sites of increased uptake regarded lymph nodes , and all cases of disease exclusion in sites of physiological uptake involved the gut . 
these lesions corresponded in three cases to lymph nodes , in one to muscle , in one to cardiac muscle , in one to a vertebra , in one to the bronchi , in two to the pancreas and in one to the sigma . 
 testa integrata con una low - dose tc ha permesso di eseguire la correzione per lattenuazione e la corretta fusione di immagini co - registrate nella stessa seduta , senza richiedere il riposizionamento del paziente o limpiego di punti di riferimento esterni o di complessi algoritmi [ 21 ]  . 
nel nostro studio le immagini fuse spect / tc ottenute attraverso la suddetta metodica hanno migliorato linterpretazione delle sole immagini spect in 23 casi ( 42% ) , permettendo la precisa localizzazione anatomica delle lesioni in 20 casi ( 37% ) e lesclusione di malattia in sedi di fisiologico accumulo del radiofarmaco in 5 casi ( 9% )  . 
nel 39% dei casi il miglioramento della localizzazione anatomica delle sedi di malattia riguardava stazioni linfonodali , mentre in tutti i casi di esclusione di malattia la captazione fisiologica era circoscritta a livello di anse intestinali . 
tali lesioni erano localizzate in 3 casi a livello linfonodale , in uno a livello muscolare , in uno nel muscolo cardiaco , in un paziente a livello vertebrale , in un altro a livello bronchiale , in due pazienti in corrispondenza del pancreas e in uno nel sigma . 
1a - c donna di 53 anni con metastasi multiple da carcinoide polmonare . a la spect mostra unarea di abnorme captazione a livello mediastinico ( frecce ) ; altra area focale ipercaptante evidente in regione mammaria sinistra ( testa di freccia )  . 
a somatostatin receptor scintigraphy ( srs ) planar imaging of the abdomen shows a large mass with a suspected secondary lesion in the left pelvis ( arrow ) ; b singlephoton - emission computed tomography / computed tomography ( spect / ct ) correctly locates the lesion in the left internal oblique muscle ( arrows )  . 
a immagine planare addome - pelvi evidenzia una massa addominale con sospetta lesione secondaria delemibacino sinistro ( freccia ) ; b la spect - tc localizza correttamente la lesione a livello del muscolo obliquo interno di sinistra ( frecce ) ; c la rilettura dellesame tc conferma la presenza di lesione muscolare ( freccia )  . radiol med ( 2008 ) 113 : 10561067 1065 anatomical localisation of spect - detected lesions in 32% of net patients evaluated with srs . 
moreover , fusion images provided a retrospective detection of lesions previously missed by diagnostic ct in four of these patients . similar results were obtained in studies performed in patients with pheochromocytoma [ 23 ] and differentiated thyroid cancer [ 24 ]  . in our experience , spect / ct data modified the clinical management in 26% of cases by changing the diagnostic approach in eight ( 15% ) and the therapeutic modality in six ( 11% )  . 
for this reason , a greater diffusion of hybrid imaging systems that combine a gamma camera with diagnostic ct predictable in managing nets . localizzazione anatomica di lesioni individuate alla spect dopo fusione di immagini spect / tc nel 32% dei pazienti con tumore neuroendocrino studiati con srs . 
risultati simili sono stati ottenuti utilizzando immagini fuse spect / tc per la valutazione di pazienti con feocromocitoma [ 23 ] e carcinoma differenziato della tiroide [ 24 ]  . nella nostra esperienza , limpiego di immagini fuse spect / tc ha inoltre avuto ripercussioni sul management clinico di un considerevole numero di pazienti ( 26% )  . 
 [ 26 ] riportano una modificazione del management terapeutico in un considerevole numero di pazienti con tumore neuroendocrino ( 28% )  . alcuni autori hanno valutato limpatto della correzione per lattenuazione fornita dallimpiego della tc sui dati srsspect in pazienti con tumore neuroendocrino ; per esempio ruf et al . 
la tomografia ad emissione di positroni ( pet ) possiede infatti una pi elevata risoluzione spaziale ( 36 mm vs 1015 mm ) rispetto alla srs - spect e permette di quantificare la captazione del tracciante . 
 [ 28 ] hanno dimostrato la superiorit della pet con 68ga - dota - toc rispetto alla scintigrafia con 111indtpa - octreotide nellidentificazione di localizzazioni polmonari e scheletriche di tumore neuroendocrino e che le due metodiche sono simili nel caso di localizzazioni epatiche e cerebrali . 
 [ 29 ] hanno riportato una pi elevata sensibilit della pet con 68ga - dota - toc rispetto alla scintigrafia con 111in - dtpa - octreotide e alla tc diagnostica con conseguenti ripercussioni cliniche in un considerevole numero di pazienti anche se lutilizzo combinato della pet a della tc mostra la pi alta accuratezza globale . 
 alla luce dei risultati ottenuti risulta evidente che lintegrazione dei dati ottenuti mediante spect - tc a basso amperaggio e tc diagnostica consente di ottenere la pi alta accuratezza nella diagnosi dei tumori neuroendocrini . per tale motivo auspicabile , per il management dei tumori neuroendocrini , una maggiore diffusione di apparecchiature ibride che associano alla gamma - camera una tc diagnostica . 1066 conclusions radiol med ( 2008 ) 113 : 10561067 conclusioni in conclusion , results of this study indicate that combined anatomical - functional imaging with spect / ct has a high diagnostic accuracy . 
ultrasound ( us ) - assisted liver biopsy is the most widespread practice for the staging of chronic hepatitis , but there are no data about a comparison with the us - guided procedure in terms of safety and diagnostic yield . 
specimens obtained by us - guided liver biopsy were 27 mm long ( range 2528.9 mm ) versus 13 mm mean value ( range 12.213.9 mm , p < 0.0001 ) of samples from us - assisted liver biopsies and contained 15.7 portal tracts ( range 14.716.7 ) versus 11 mean value ( range 1011.9 , p < 0.0001 ) of specimens obtained by echo - assisted needle biopsy . 
le biopsie eseguite con tecnica eco - guidata hanno dato esito a frustoli lunghi in media 27 mm , ( range 2528 , 9 mm ) e con una media di 15 , 7 spazi portali ( range 14 , 716 , 7 )  . 
 parole chiave biopsia epatica ecografia epatite cronica radiol med ( 2008 ) 113 : 992998 introduction introduzione liver biopsy is commonly used for obtaining liver tissue in patients affected by viral chronic hepatitis . 
percutaneous needle biopsy is the tool of first choice for assessing liver injury , as transjugular biopsy or laparoscopic biopsy are applied in a very limited subset of patients and hardly ever in chronic viral hepatitis . 
liver biopsy by routine ultrasound ( us ) assessment of the puncture site is now the most common practice in several departments all over the world , as the literature of the last 20 years has shown that this procedure is safer than blind liver biopsy [ 2 , 3 ]  . 
we must also remark that mortality is still described and that cutting needles , such as tru - cut needle , may increase the risk of bleeding [ 4 ]  . 
us is commonly used only to mark the site for percutaneous biopsy and to detect complications after the procedure , whereas us - guided liver biopsy is performed only in fine - needle - aspiration biopsy of focal lesions . 
some authors remarked that using this procedure in routine liver biopsy can increase the risk of complications because the needle requires a longer time in the liver during the biopsy [ 5 ]  . 
 for several years , physicians with expertise in interventional us have been performing routine us - guided needle biopsy instead of us - assisted practice in patients affected by diffuse liver diseases , but the differences between tissue yield and safety of these two needle biopsy procedures have never been systematically investigated . 
 materials and methods we retrospectively analysed 357 consecutive patients affected by chronic hepatitis c virus ( hcv ) and hepatitis b virus ( hbv ) or hcv - hbv infections . 
one hundred seventy - six patients admitted from february 2005 to june 2006 were submitted to us - guided liver biopsy because of evidence of macroscopically larger samples obtained by using the us - guided procedure . 
lago - biopsia percutanea lesame di prima scelta per la valutazione del danno epatico dal momento che la biopsia trans - giugulare e laparoscopica sono tecniche ormai applicate in un numero molto ristretto di pazienti e molto raramente vengono impiegate su pazienti affetti da epatiti virali croniche . 
la biopsia epatica , eseguita dopo valutazione ecografica del sito dingresso dellago , attualmente la pratica bioptica pi comunemente adottata in molti reparti clinici un po in tutto il mondo da quando la letteratura scientifica degli ultimi venti anni ha mostrato come tale procedura sia pi sicura della tecnica di biopsia epatica definita alla cieca [ 2 , 3 ]  . va anche ricordato che la mortalit in seguito a biopsia epatica viene ancora descritta in letteratura e che luso di aghi taglienti quali il tru - cut pu aumentare il rischio emorragico [ 4 ]  . 
lesame ecografico viene attualmente utilizzato per individuare il sito pi adatto alla penetrazione percutanea dellago e ad evidenziare precocemente eventuali complicanze post - bioptiche mentre la procedura eco - guidata viene generalmente utilizzata soltanto per effettuare agoaspirazioni di lesioni focali . 
alcuni autori hanno sottolineato come lutilizzo della procedura eco - guidata per il prelievo bioptico di routine nelle epatopatie diffuse possa aumentare il rischio di sanguinamento a causa di una persistenza pi prolungata dellago allinterno del parenchima epatico [ 5 ]  . daltro canto , da alcuni anni , sono sempre pi numerosi i radiologi o gli ecografisti interventisti che utilizzano comunemente , in casi di epatopatie diffuse , la tecnica bioptica eco - guidata piuttosto che eco - assistita nonostante le differenze in termini di sicurezza e resa diagnostica di queste due procedure non siano mai state valutate in modo sistematico . materiali e metodi abbiamo analizzato retrospettivamente 357 pazienti consecutivi affetti da infezione cronica da virus dellepatite c ( hcv ) e b ( hbv ) o coinfetti da entrambi i virus . 
centosettantasei pazienti ricoverati dal febbraio 2005 al giugno 2006 sono stati sottoposti a biopsia epatica percutanea ecoguidata a causa dellevidenza di frustoli epatici macroscopicamente pi grandi di quelli ottenuti con procedura ecoassistita . 
tutti i pazienti hanno reso un consenso informato 994 radiol med ( 2008 ) 113 : 992998 abdominal us examination was performed in all patients before and 3 h after the needle biopsy . 
the us - assisted procedure was performed by scanning the last intercostal spaces to assess the most suitable and safe access to the liver and to avoid the pleura and adjacent organs . 
the same physician , with comparable experience in us - assisted and us - guided biopsy procedures , carried out all percutaneous needle biopsies over the course of 28 months . 
 diagnostic yield was evaluated considering the 2003 guidelines [ 6 ] of the italian association for the study of the liver ( associazione italiana per lo studio del fegato , aisf ) and the italian society of anatomical pathology and cytopathology ( societ italiana di anatomia patologica e citopatologia diagnostica , siapec )  . 
in 3 / 176 us - guided versus 2 / 181 us - assisted liver biopsies , two passes were scritto alla biopsia epatica per cutanea eco - guidata o ecoassistita . 
lo studio stato approvato dal locale comitato etico ed stato effettuato in accordo con gli standards etici della dichiarazione di helsinki del 1964 . esame ecografico e biopsia epatica i pazienti sono stati esaminati con un apparecchio ecografico ge ( general electrics , usa ) logiq 5 expert usando una sonda tipo convex da 3 , 6 mhz . 
le biopsie epatiche sono state effettuate durante ricovero in regime di day hospital . sono stati considerati validi , ai fini della determinazione dei parametri della coagulazione , valori di attivit protrombinica pari a non meno del 40% ed una conta delle piastrine nel siero pari a non meno di 40000 / mm3 . 
la procedura eco - assistita stata effettuata eseguendo alcune scansioni sugli ultimi spazi intercostali destri prima del prelievo in modo da individuare laccesso bioptico pi agevole e sicuro ed evitare la puntura accidentale della pleura o di organi adiacenti . 
 la resa diagnostica stata valutata inoltre considerando anche le linee guida redatte nel 2003 [ 6 ] dalla associazione italiana studio del fegato ( aisf ) e dalla societ italiana di anatomia patologica e fitopatologia ( siapec )  . 
il grado di infiammazione e lo stadio di fibrosi tissutale del campione bioptico sono stati analizzati usando il sistema di classificazione delle epatiti croniche di tipo quantitativo secondo ishak [ 7 ]  . 
degree of fibrosis was advanced in 61 / 181 liver samples ( 33.7% ) obtained by us - assisted needle biopsy and in 41 / 176 liver samples ( 22.3% ) obtained by the us - guided procedure . 
considering the biopsy size cutoff value for histological evaluation of chronic viral hepatitis recommended by aisf and siapec guidelines , 83% of specimens obtained from us - guided liver biopsy were more than 20 mm long versus 12.5% of specimens obtained from us - assisted liver biopsy . 
it is known that sampling error and sampling variability depend on the kind and size of the needle and on operator expertise [ 11 , 12 ]  . analisi statistica le differenze statistiche tra i campioni ottenuti dai due gruppi di pazienti sono state analizzate con welch - test ( considerando differenze non eguali )  . 
le differenze tra campioni bioptici e gruppi di biopsie sono state considerate statisticamente significative se p risultava minore di 0 , 05 . risultati non abbiamo osservato nessun decesso nella nostra casistica . 
una frammentazione del frustolo stata osservata in 22 su 176 ( 12 , 5% ) biopsie ecoguidate ed in 32 su 181 ( 33 , 7% ) biopsie eco - assistite ( p = 0 , 22 )  . 
lo stadio della fibrosi risultato essere avanzato in 61 su 181 ( 33 , 7% ) campioni di tessuto epatico ottenuto con ago - biopsia eco - assistita ed in 41 su 176 ( 22 , 3% ) campioni di tessuto ottenuti con la procedura eco - guidata . 
prendendo in considerazione i limiti di validit istologica del campione bioptico indicati dalle linee guida dellaisf e siapec per la valutazione delle epatiti virali croniche , nell83% dei casi i frustoli ottenuti con biopsia eco - guidata misuravano pi di 20 mm di lunghezza contro il 12% dei campioni prelevati con biopsia eco - assistita . 
la differenza tra i due gruppi di biopsie risultata essere del 18% ( 95% ci ; 8 , 427 , 6 ; p < 0 , 001 )  . discussione echo - guided needle biopsies echo - assisted needle biopsies fig . 
1 dimensioni del frustolo bioptico nei due campioni di biopsie epatiche . ampiamente noto che leffettuare biopsie epatiche con lausilio dellesame ecografico produca una riduzione del rischio di complicanze [ 3 , 810 ]  . 
2 numero di spazi portali nei due campioni di biopsie epatiche . on the other hand , we know that the extent of liver injury may vary among portal triads and that performing liver biopsy with coarse instead of fine needles as well as trucut instead of suction needles can increase diagnostic yield [ 13 , 14 ]  . 
however , the literature in support of such a position is far from conclusive because of the different meanings often attributed to diagnostic yield , including number of samples suitable for histological diagnosis , size of the specimens or adequate number of portal spaces . 
in fact , some authors recently showed that correct histological assessment in patients with chronic viral hepatitis is possible only by sampling a specimen not less than 2 cm long with a 16 - gauge needle ( diameter 1.4 mm ) or not less than 2.5 cm long with an 18 - gauge needle ( diameter 1.2 mm ) [ 6 , 16 ]  . this liver biopsy size , statistically containing more than ten portal spaces , allows pathologists to establish the real extent of fibrosis and hepatic injury . 
we reduced the sampling error variability as well as radiol med ( 2008 ) 113 : 992998 inoltre noto che lerrore e la variabilit di campionamento bioptico dipendono dal tipo e dal calibro dellago utilizzato cos come dallesperienza delloperatore [ 11 , 12 ]  . sappiamo inoltre che lestensione del danno fibrotico del fegato pu variare nelle diverse triadi portali e che la resa diagnostica pu essere aumentata utilizzando aghi di grosso calibro piuttosto che aghi sottili o utilizzando aghi trancianti di tipo tru - cut piuttosto che aghi con meccanismo di aspirazione [ 13 , 14 ]  . 
la letteratura in supporto di tali affermazioni tuttavia lontana dal dare considerazioni conclusive a causa del diverso significato spesso attribuito alla resa diagnostica identificata come sia come numero di campioni adeguati , che come dimensioni del campione o numero di spazi portali necessari alla diagnosi istologica . un frustolo epatico di 1 , 5 cm di lunghezza comunemente ritenuto adeguato per una valutazione istologica delle epatopatie diffuse . 
in effetti recentemente alcuni autori hanno mostrato come una corretta valutazione istologica dei campioni bioptici di pazienti affetti da epatite virale cronica possa essere possibile solo su frustoli di tessuto epatico non inferiori ai 2 cm di lunghezza se prelevati con ago di calibro pari a 16 g ( diametro di 1 , 4 mm ) o non inferiori a 2 , 5 cm di lunghezza se prelevati con ago di calibro pari a 18 g ( diametro di 1 , 2 mm ) [ 6 , 16 ]  . 
sulla base di tali risultati clinici in italia , nel 2004 , laisf e la siapec hanno pubblicato delle linee guida ufficiali circa le dimensioni adeguate del frustolo epatico da campionamento bioptico . 
esiste attualmente una tendenza da parte di molti reparti clinici di adottare esclusivamente la procedura di biopsia epatica ecoassistita nonostante non esistano linee guida che suggeriscano tale metodica di prelievo . 
in effetti non esistono in letteratura dei trias clinici che comparino la biopsia epatica eco - guidata con quella eco - assistita circa la sicurezza e la resa diagnostica delle due procedure di prelievo . 
abbiamo potuto ridurre la variabilit dellerrore di campionamento cos come la variabilit interosservatore poich ogni ago - biopsia stata eseguita da un singolo operatore in un periodo di tempo molto breve ( circa 28 mesi ) usando lo stesso accesso bioptico oltre che lo stesso tipo e calibro dellago . 
tutti i frustoli epatici sono stati inoltre analizzati dallo stesso gruppo di anatomopatologi , usando il medesimo sistema di score numerico . abbiamo osservato che entrambe le procedure sono egualmente sicure e che producono una buona qualit di radiol med ( 2008 ) 113 : 992998 the interobserver variation because each liver biopsy was performed by a single physician over a very short period ( about 28 months ) using needles of similar type and size . also , each biopsy was performed using the same approach . these specimens were analysed by a single pathologist team using the same numerical scoring systewe noted that both methods are equally safe and both procedures produce a good quality of biopsy cylinders considering the sample size cutoff values used to evaluate diffuse liver diseases . 
however , considering the size of liver biopsy samples recommended by the aisf and siapec guidelines , we showed that us - guided needle biopsy is superior to the us - assisted procedure , as specimens were significantly longer and contained significantly more portal tracts with the former technique . 
in fact , we know that histological numerical scores for assessing chronic viral hepatitis tend to underestimate liver fibrosis if the specimens are too small , so that the smaller the sample , the milder the disease seems to be [ 6 ]  . 
the two study groups were not comparable in relation to fibrosis degree , but this did not seem to entail significant differences in sample fragmentation . in conclusion , we can say that , in our experience , usguided liver biopsy improves tissue yield by producing larger liver samples . 
 we must also note that the us - guided procedure requires expertise in interventional us and can be performed by a single physician only by using an automatic needle , which is , of course more expensive than a conventional menghini needle . 
 campioni considerando i parametri dimensionali comunemente utilizzati per la valutazione delle epatopatie diffuse . sulla base delle linee guida aisf - siapec abbiamo tuttavia notato come la biopsia eco - guidata risulti superiore alla procedura eco - assistita in quanto i campioni prelevati sotto guida ecografica sono significativamente pi lunghi e contengono un maggior numero di spazi portali . 
tale dato sicuramente rilevante considerando che i sistemi di valutazione istologica di tipo numerico tendono a sottostimare la fibrosi epatica qualora il materiale tissutale sia scarso , cos che pi piccolo il campione e pi lieve sembra la essere la stessa patologia [ 6 ]  . 
dobbiamo anche sottolineare come leffettuare un ago - biopsia eco - guidata richieda sempre unesperienza in ecografia interventistica e possa essere effettuata da un singolo operatore soltanto usando un ago automatico , necessariamente pi costoso di un ago tradizionale di tipo menghini . 
in italia il costo medio di un ago tranciante con aspirazione automatica di circa 56 , 25 euro ( range 4072 , 5 euro ) mentre il costo medio di un ago menghini modificato di 50 euro ( range 3664 euro ) cos che la differenza media tra i costi di questi due tipi di ago risulta essere di soli 6 , 25 euro ( range 48 , 5 euro )  . sebbene luso dellecografia nellausilio alla biopsia epatica sia stato dimostrato essere superiore per costi e benefici alla tecnica di biopsia alla cieca [ 17 ] , i reali costi e la reale efficacia della tecnica di biopsia eco - guidata o eco - assistita dovrebbero essere valutati in studi futuri al fine di poter produrre delle linee guida specifiche circa lutilizzo delle diverse procedure di biopsia nella pratica clinica . 
 + 91 - 416 - 2282027 , fax : - 91 - 416 - 2232035 , e - mail : gibikote@cmcvellore.ac.in published online : 20 october 2008 springer - verlag 2008 the article by copetti and cattarossi [ 1 ] is a welcome addition to the literature on the use of ultrasonographic diagnosis of pulmonary disease in children [ 2 ]  . 
however , there are certain limitations of their study that bear mentioning . although the authors described the different possible ultrasound ( us ) findings in consolidation , they did not specify which diagnostic criteria were used in the 60 children diagnosed on us to have pneumonia . 
was it only the presence of b lines , or was the diagnosis made on seeing a solid , hepatised lung ; or a combination of hypoechoic pleural line , air inlets and dynamic air ; or fluid bronchograms ? a table showing the relative frequency of each finding would have been helpful in assessing the specificity and sensitivity of each finding in diagnosing pneumonia in this group of children . the authors also missed the opportunity to compare us findings with the chest x - ray ( cxr ) appearance . 
were there differences in the frequency of positive us findings in the 30 children with lung infiltrates on chest x - ray when compared with the 23 children with parenchymal consolidation ? the methodology of the study in having chest x - rays read by the junior radiologist on duty followed by one senior radiologist has led to a high interobserver variability in cxr interpretation , with 12 ( 22.5% ) of 53 x - rays called normal by the junior radiologist yet being read as pneumonia by the senior radiologist . 
at the same time , having the us done by a single expert operator gives this study unwanted bias towards better results for us when compared with cxr in the diagnosis of pneumonia . 
4a that was interpreted as normal actually shows a retrocardiac density obscuring the medial left hemidiaphragm , which in our opinion and using standard world health organisation ( who ) definitions [ 3 ] should be interpreted as a retrocardiac basal consolidation on the left side . 
training cxr readers to use standardised definitions would minimize interand intraobserver variability in larticolo di copetti e cattarossi [ 1 ] un ulteriore contributo alla letteratura sullimpiego degli ultrasuoni nella diagnosi delle malattie polmonari nel bambino [ 2 ]  . 
peraltro vi sono alcuni limiti nello studio che vanno sottolineati . sebbene gli autori descrivano i diversi aspetti ecografici nella consolidazione polmonare , essi non hanno specificato quali criteri sono stati impiegati per porre la diagnosi nei 60 bambini con diagnosi di polmonite allecografia . 
si trattava solo della presenza delle b lines o la diagnosi stata fatta in base alla presenza di un polmone con aree di epatizzazione oppure sulla base di una associazione di aspetti ( linee pleuriche ipoecogene , broncogramma fluido ecc . ) ? riteniamo che sarebbe stato utile presentare una tabella con le rispettive incidenze di ogni singolo segno nella diagnosi di polmonite . 
gli autori non hanno inoltre colto lopportunit di confrontare gli aspetti ecografici con quelli radiografici . sono state a questo proposito osservate delle differenze tra le frequenze degli aspetti ecografici positivi nei 30 bambini con infiltrati polmonari alla radiografia del torace rispetto ai 23 bambini con consolidamento parenchimale ? il fatto di aver utilizzato una doppia lettura da parte di un radiologo junior seguita da un radiologo senior ha portato ad una elevata variabilit inter - osservatore nella interpretazione dei radiogrammi , con 12 ( 22 , 5% ) dei 53 radiogrammi del torace definiti normali dal radiologo junior refertati invece come positivi per polmonite dal radiologo senior . 
allo stesso tempo , il fatto che lecografia sia stata eseguita da un unico operatore esperto ha portato a un bias determinando un risultato superiore dellecografia rispetto alla radiografia del torace nella diagnosi di polmonite . 
4a , interpretata come normale , dimostra una opacit retrocardiaca che oscura la parte mediale dellemidiaframma di sinistra , che nella nostra interpretazione ( utilizzando gli standard who [ 3 ] ) , dovrebbe essere interpretata come una consolidazione basale retrocardiaca a sinistra . 
il training nella lettura dei radiogrammi del torace utilizzando delle definizioni standardizzate dovrebbe ridurre al minimo le variabilit intero intra - osservatore nei lavori di confronto 1080 radiol med ( 2008 ) 113 : 10791081 any study comparing cxr and us for diagnosing pneumonia in children [ 4 ]  . in assessing the ease of performing us examinations of the chest in children , readers would also be keen to know the approximate time taken for an average us examination , how well younger children cooperated and whether sedation was needed for any of theus is an important diagnostic tool in differentiating pulmonary , pleural and mediastinal lesions when the cxr shows an opaque hemithorax and is helpful in therapeutic decision making on thoracentesis for pleural effusions that show fibrinous strands , septations or loculations [ 5 ]  . 
whereas we agree that us avoids the use of ionising radiation , we believe that the limitations of this study prevent the authors from providing sufficient evidence in support of their statement that a clear clinical picture of pneumonia associated with positive lung us findings excludes the need to perform cxr . 
we feel that the operator - dependent nature of us interpretation and the ease of training even nonradiologists [ 4 ] in cxr interpretation with standardized definitions continue to make cxr the mainstay in diagnosing childhood pneumonia . tra radiologia del torace e ecografia nella diagnosi di polmonite nel bambino [ 4 ]  . nella definizione della facilit di esecuzione dellecografia del polmone nei bambini , il lettore desidererebbe conoscere il tempo approssimativo per un esame ecografico medio , i problemi di cooperazione dei bambini pi piccoli e la necessit di sedazione in alcuni casi . lecografia una metodica diagnostica importante nella diagnosi differenziale tra lesioni polmonari , pleuriche e mediastiniche nei casi in cui il radiogramma del torace evidenzia una opacit di un emitorace , ed utile nel prendere una decisione su una toracentesi per un versamento pleurico che dimostra tralci di fibrina , setti o aspetti multiloculari [ 5 ]  . 
mentre concordiamo sul fatto che lecografia evita il ricorso alle radiazioni ionizzanti , riteniamo che i limiti di questo studio precludono dallaffermare che un quadro clinico chiaro di polmonite associato a una ecografia polmonare positiva escluda il ricorso alla radiografia del torace . 
cerizza4 1servizio di fisica sanitaria , ospedale di circolo , viale borri 57 , 21100 varese , italy 2scuola di specializzazione in fisica sanitaria , universit degli studi di milano , milano , italy 3dipartimento di scienze cliniche e biologiche , universit dellinsubria , varese , italy 4divisione di radioterapia , ospedale di circolo , varese , italy correspondence to : c . 
the study considered 110 patients treated between 2001 and 2006 with external beam radiation therapy and / or brachytherapy with either ldr ( afterloader selectron , 137cs ) or hdr ( afterloader microselectron classic , 192ir )  . 
nello studio rientrano 110 pazienti trattate nel nostro centro dal 2001 al 2006 con radioterapia a fasci esterni e / o brachiterapia ldr ( afterloader selectron , 137cs ) o hdr ( afterloader microselectron classic , 192ir )  . 
la differenza tra i diversi tipi di trattamento risultata significativa solo in un caso ; allinterno di ogni singola metodica si per riscontrata notevole variabilit di efficacia , causata dalla diversit degli schemi di frazionamento e dalla disparit della durata totale del trattamento . 
numerose variabili nel trattamento possono causare notevoli disparit di efficacia ; la valutazione radiobiologica personalizzata un utile supporto a quella radiol med ( 2008 ) 113 : 10681078 1069 planning equivalent treatments that satisfy all dosimetric constraints . clinica per impostare trattamenti equivalenti nel rispetto dei vincoli dosimetrici . keywords brachytherapy bed optimisation gynaecological parole chiave brachiterapia bed ottimizzazione ginecologico introduction introduzione the treatment of gynaecological malignancies involves initial external beam radiation therapy ( ebrt ) , in some cases followed by an additional intracavitary brachytherapy ( bt ) boost . 
in the past few years , our centre has offered multiplefraction high - dose - rate ( hdr ) bt alongside conventional single - fraction low - dose - rate ( ldr ) bt , with important radiobiological implications . 
bed is , in fact , defined as the product of the absorbed dose and a relative effectiveness factor that accounts for both the radiation delivery pattern and the radiobiological features of the irradiated tissue . 
bed thus permits prediction of the best effectivenesstoxicity ratio . the aims of the study were to verify whether there any were differences in therapeutic effectiveness ( bed to tumour ) or involvement of normal tissue ( bed to rectum ) among patients receiving different treatments for the same disease ( ebrt + ldr , ebrt + hdr , hdr alone ) and to study the effect of the variable factors within each group of patients . 
in this respect , dose fractionation and adjustment of the total dose are crucial for limiting complications without compromising treatment outcome . materials and methods patients the study included 110 patients ( median age 65.8 years , range 32.093.6 years ) treated with ebrt followed by il trattamento dei tumori del distretto ginecologico prevede una prima fase di radioterapia a fasci esterni ( ebrt ) , seguita in alcuni casi da un boost di brachiterapia ( bt ) endocavitaria . 
negli ultimi anni il nostro centro ha visto affiancarsi al trattamento brachiterapico tradizionale con singola frazione a basso rateo di dose ( ldr ) quello con pi frazioni ad alto rateo di dose ( hdr ) , con notevoli implicazioni di carattere radiobiologico . 
recenti studi presenti in letteratura [ 1 ] sembrano indicare la superiorit dei trattamenti frazionati ad alto rateo di dose ( hdr ) con dose / frazione tra 5 e 7 gy rispetto a trattamenti continui con basso rateo di dose ( ldr ) in trattamenti radianti della cervice uterina . 
il nostro studio vorrebbe confrontare fra loro i trattamenti utilizzati nel nostro centro nel periodo compreso fra il 2001 e il 2006 per le pazienti con lesioni maligne al distretto ginecologico ; le modalit di trattamento differiscono fra loro per lo schema di frazionamento , il dose - rate , il tempo totale di trattamento . 
la dose biologicamente efficace ( bed ) , desunta dal formalismo del modello lineare quadratico , soddisfa tali requisiti ; essa infatti definita come il prodotto della dose assorbita per un fattore di efficacia relativa che tiene conto della modalit di somministrazione di tale dose e delle caratteristiche biologiche del tessuto irraggiato . 
essa dunque permette anche di prevedere il miglior rapporto efficacia / tossicit . lo scopo iniziale quello di verificare se esistano differenze di efficacia terapeutica ( bed al tumore ) o di interessamento dei tessuti sani ( bed al retto ) fra pazienti con la medesima patologia ma trattate con modalit differenti ( ebrt + ldr , ebrt + hdr , solo hdr ) , ed eventualmente di studiare leffetto dei fattori di variabilit allinterno di ciascun gruppo . 
the occurrence of possible late complications is currently being evaluated . ldr treatments were performed with a selectron remote afterloader using 137cs sources , whereas hdr treatments were performed with a microselectron classic remote afterloader with a 192ir source . radiobiological evaluation comparison of the different techniques was based on bed values to the tumour and to the rectum [ 1 ]  . 
the reason for our choice to calculate bed to the rectum is that the literature has provided a threshold for rectal toxicity conveniently expressed in bed , which is indispensable for treatment optimisation . 
for fractionated hdr treatment , we table 1 subdivision of patients according to clinical status minuzione delle complicanze senza compromettere i risultati della terapia . materiali e metodi pazienti nello studio rientrano 110 pazienti di et mediana 65 , 8 anni , range 32 , 093 , 6 , trattate dal 2001 al 2006 per tumori del distretto ginecologico ( carcinomi della cervice uterina , dellendometrio e recidive vaginali ) con radioterapia a fasci esterni seguita da brachiterapia ldr o hdr . 
lintento curativo si riferisce a pazienti trattate a titolo radicale con ebrt fino a 60 , 4 gy ( 1 , 82 gy / frazione , 5 frazioni / settimana ) seguita da boost brachiterapico ; lintento adiuvante invece relativo a pazienti sottoposte a chirurgia pelvica e irradiate a titolo postoperatorio con ebrt fino a 50 , 4 gy ( 1 , 82 gy / frazione , 5 frazioni / settimana ) seguita da boost brachiterapico , oppure con brachiterapia esclusiva hdr ( tabelle 1 e 2 )  . per quanto riguarda la tollerabilit dei trattamenti sia ldr che hdr non stata riscontrata , in corso di terapia , nessuna complicanza acuta rettale , vaginale o vescicale . anche ai primi controlli clinici , a tre mesi dalla fine del trattamento radiante , non sono state osservate complicanze acute . 
gli organi a rischio durante lirraggiamento della pelvi sono il retto e la vescica ; la scelta di valutare la bed al retto motivata dal fatto che per tale organo la letteratura fornisce un valore di soglia di tossicit espresso in termini di bed , indispensabile per lottimizzazione del trattamento . 
per il trattamento frazionato hdr si assunto un riparo completo fra le frazioni ( intervallo sufficientemente lungo da permettere che tutti i danni sub - letali fossero riparati ) , e per frazioni di durata inferiore a 900 s si trascurato il recupero del danno sub - letale durante la somministrazione della dose . 
per la singola frazione ldr , al contrario , la durata della frazione tale da rendere necessaria la valutazione del recupero del danno sub - letale radiol med ( 2008 ) 113 : 10681078 table 2 subdivision of patients according to treatment 1071 adjuvant no . 
nel caso dei tessuti sani si tratta di un fenomeno trascurabile se si considerano i tempi tipici di un trattamento , pertanto esso viene considerato solo nel caso del tumore . 
bed values calculated with different / values are not comparable . the parameters used in the bed calculation were as follows : / ratio : late - responding normal tissue ( rectum ) : / = 3gy ( in the literature / 14 gy ) [ 5 ]  . tumour and early responding normal tissue : / = 10 gy ( in the literature / 520 gy ) [ 5 ] parameter : tumour : = 0.3 gy1 [ 6 ] constant for sublethal damage repair , : late - responding normal tissue : = 0.46 h1 , t1 / 2 rep = 1.5 h tumour and early responding normal tissue : = 1.4 h1 , t1 / 2 rep = 0.5 h [ 5 ] there is moderate variability in the literature , with t1 / 2 rep for late - responding normal tissue in the range of 0.22.5 h [ 7 ]  . onset time for proliferation , to : twenty - one days although this has been reported to be 2135 days [ 6 ] , we decided to consider the more conservative value . mean tumour doubling time , teff : dove teff , detto tempo medio di raddoppio del tumore , esprime la velocit di replicazione del tumore , e ( gy1 ) uno dei due parametri caratteristici della curva di sopravvivenza cellulare come descritta dal formalismo linearequadratico . 
nellindicare i valori numerici del bed si utilizza lunit di misura gy indicando a pedice il valore di / impiegato per il calcolo ; valori di bed calcolati con diversi valori di / non sono fra loro confrontabili . i parametri da noi utilizzati nel calcolo del bed sono : rapporto / : tessuto sano a risposta tardiva ( retto ) : / = 3gy ( in letteratura / 14 gy ) [ 5 ] tumore e tessuto sano a risposta veloce : / = 10 gy ( in letteratura / 520 gy ) [ 5 ] parametro : tumore : = 0 , 3 gy1 [ 6 ] costante di riparazione del danno sub - letale : tessuto sano a risposta tardiva : = 0 , 46 h1 , t1 / 2rep = 1 , 5 h tumore e tessuto sano a risposta veloce : = 1 , 4 h1 , t1 / 2rep = 0 , 5 h [ 5 ] in letteratura si riscontra una discreta variabilit , con t1 / 2rep per il tessuto sano a risposta tardiva nel range 0 , 22 , 5 h [ 7 ] tempo di proliferazione del tumore to : 21 giorni in letteratura : 2135 giorni [ 6 ]  . 
si scelto di considerare il valore pi conservativo tempo medio di raddoppio del tumore teff : five days in actual fact , there is wide variation among tumours and among patients . 
a more realistic and accurate estimate 5 giorni radiol med ( 2008 ) 113 : 10681078 1073 could be derived from the evaluation of biopsy material . where this has been done , the range is 1.475 days ( mean 6.8 days ) [ 6 ]  . dose reduction factor , f : 0.7 [ 8 ] results influence of radiobiological parameters the values of the radiobiological parameters for bed calculation are not known , and each parameter has a range of variability that influences the calculated bed values . 
this is no doubt one of the main limitations of the dosimetric approach based on bed . in our study , bed was used in relative rather than absolute terms , as our aim was to render treatments for the same disease biologically equivalent . 
where bed is used in absolute terms , it is important to be aware of the extent to which the bed calculations are influenced by the range of variation of the parameters . for all patients enrolled in our study , bed was calculated for different values of / to , and teff . 
in each case , the parameter being examined was made to vary within the reported range of variation , whereas the other parameters were kept constant at the reference values [ / = 3 ( 10 ) gy for the rectum ( tumour ) to = 21 g , teff = 5 g ]  . 
the / ratio was found to be particularly critical for bed evaluation , both for bedrectum ( + 80% , 20% ) and for bedtumour ( + 30% , 15% )  . 
on the other hand , bed variation as a function of teff was greater close to the 5 days considered as a reference value . analysis of clinical series the initial aim of this study was to understand whether patients with the same disease treated with different radiotherapy techniques received equivalent treatment in terms of the biologically effective dose and , if not , to identify and eliminate the factors causing the differences so as to ensure the delivery of uniform treatments . 
in tal caso dalla letteratura : 1 , 475 giorni ( media 6 , 8 giorni ) [ 6 ] fattore di riduzione della dose f : 0 , 7 [ 8 ]  . risultati influenza dei parametri radiobiologici i valori dei parametri radiobiologici per il calcolo del bed non sono noti con precisione , esiste al contrario per ciascuno di essi un range di variabilit che si ripercuote sul valore di bed calcolato ; questo indubbiamente uno dei maggiori punti deboli dellapproccio dosimetrico basato sul bed . nel nostro studio il bed non stato impiegato tanto in termini assoluti quanto in termini di confronto , allo scopo di rendere biologicamente equivalenti i trattamenti di una medesima patologia . 
qualora invece si impieghi il bed in termini assoluti importante essere consapevoli di quanto gli intervalli di variazione dei parametri influiscano sul valore di bed calcolato . per tutte le pazienti dello studio si valutato il bed per diversi valori dei parametri / to e teff . 
in ciascun caso stato fatto variare il parametro in esame entro il range di variabilit riscontrato in letteratura mantenendo costanti tutti gli altri parametri ai valori di riferimento ( / = 3 ( 10 ) gy per il retto ( tumore ) , to = 21 g , teff = 5 g )  . 
i valori del rapporto / risultano essere particolarmente critici per la valutazione del bed , sia nel caso di bedretto ( + 80% , 20% ) sia nel caso di bedtumore ( + 30% , 15% )  . 
la variazione di bed in funzione di teff invece di maggiore entit proprio nellintorno dei 5 giorni da noi assunti come valore di riferimento . analisi della casistica clinica lo scopo iniziale di questo studio stato quello di capire se le pazienti con la medesima patologia , ma curate in modi diversi hanno ricevuto trattamenti equivalenti dal punto di 1074 radiol med ( 2008 ) 113 : 10681078 fig . 
1a - d variazione percentuale di bedretto ( a ) e bedtumore ( b - d ) rispetto a bedref al variare di / retto ( a ) , / tumore ( b ) , to ( c ) e teff ( d )  . adjuvant treatment three treatment techniques were used in this group ( table 2 )  . 
the main variability factors were ebrt dose , bt dose , dose rate ( ldr ) , fractionation scheme ( hdr ) , and overall treatment time ( start ebrt to end bt )  . the mean bedtumour and bedrectum values are summarised in table 3 . 
multiple pairwise comparisons with bonferroni correction ( significance level at 0.05 / 3 = 0.0167 ) revealed a significant difference only between hdr and ebrt + ldr ( p < 0.0167 ) with regard to bedtumour , whereas treatment with hdr alone differed significantly from the two combined treatments ( p < 0.0167 ) with regard to bedrectum ; there was no significant difference between the two combined treatments . vista dellefficacia biologica e , nel caso di elevata variabilit , individuare ed eliminare i fattori maggiormente responsabili allo scopo di uniformare i trattamenti . 
 il test statistico di analisi della varianza ad un criterio di classificazione , che indica una differenza significativa fra le tre medie a livello di confidenza del 5% , sia per bedtumore ( p < 0 , 025 ) sia per bedretto ( p < 0 , 001 )  . 
dal confronto multiplo a coppie con correzione di bonferroni ( livello di significativit pari a 0 , 05 / 3 = 0 , 0167 ) si riscontra che nel caso di bedtumore c differenza significativa solo fra hdr e ebrt + ldr ( p < 0 , 0167 ) , mentre per bedretto il trattamento con solo hdr significativamente differente da entrambi i 1076 discussion influence of radiobiological parameters the / ratio values are particularly critical in evaluating the bed , but we chose the values with major consensus in the literature . 
the use of reference values ( / rectum = 3 gy , / tumour = 10 gy ) is thus justified and enables comparison with other studies , in particular the clinical ones looking for a implications of the relationship between bed and toxicity . the results , summarised in fig . 
this result might have been expected in our group of patients and is explained by the fact that in early attempts to achieve equivalence in hdr treatments , we adopted the french schools recommendation to reduce the bt doses by 30%50% when using hdr compared with ldr . 
4 is in fact that the longer the treatment duration , the more the repopulation factor will reduce the effectiveness of treatment ( bedtumour )  . optimisation having noted considerable variation in the biological effectiveness of bt among patients , we calculated for both hdr and ldr the optimal treatment for each patient , that is , treatment delivering the required bed to the tumour while minimising damage to normal tissue . 
selection of a hdr radiol med ( 2008 ) 113 : 10681078 trattamenti combinati ( p < 0 , 0167 ) , tra i quali non vi invece differenza statisticamente significativa . trattamento curativo allinterno di questo gruppo sono state attuate due modalit di trattamento ( tabella 2 )  . 
dal confronto statistico fra due medie per campioni indipendenti non si riscontra differenza significativa , a livello di confidenza del 5% , fra le sia per bedtumore trattamento , due modalit di ( p = 0 , 99 > 0 , 05 ) sia per bedretto ( p = 0 , 13 > 0 , 05 )  . 
 discussione influenza dei parametri radiobiologici i valori del rapporto / risultano essere particolarmente critici per la valutazione del bed , ma sono anche quelli per i quali si ritrova maggiore accordo in letteratura : lutilizzo dei valori di riferimento ( / retto = 3 gy , / tumore = 10 gy ) pertanto giustificato e consente il confronto con altri studi , in particolar modo quelli che affrontano anche con un riscontro clinico lo studio della correlazione bed - tossicit . i risultati riassunti in fig . 
1 sono comunque indicativi del fatto che lapproccio radiobiologico pu essere considerato un utile supporto alla pianificazione dosimetria , ma senza la pretesa di esaurire nel solo parametro bed la complessit della valutazione clinica . analisi della casistica clinica nel caso adiuvante , lanalisi statistica ha mostrato una differenza significativa tra le modalit di trattamento combinato ebrt + bt e il trattamento con solo hdr . 
tale risultato nel nostro gruppo di pazienti era forse prevedibile ed comunque interpretabile , in quanto nei primi tentativi di equivalenza nei trattamenti con hdr era stata fatta propria unindicazione della scuola francese secondo cui le dosi prescritte in brachiterapia dovrebbero essere ridotte dal 30% al 50% con hdr rispetto a ldr . 
2a , b distribuzione della durata totale del trattamento adiuvante ( a ) e curativo ( b )  . fractionation scheme or ldr dose should aim to customise treatment by taking into account ebrt time ( especially in the presence of long waiting intervals ) , ebrt dose and treatment intent . 
for adjuvant treatment , the protocol dose is 281.8 gy ebrt + 12 gy bt ; for curative treatment , the dose is 281.8 gy ebrt + 52 gy ebrt on a reduced volume + 15 gy bt . 
in bt , the target dose is delivered 0.5 cm from the applicator surface , and when evaluating bed to the rectum , it is assumed that the rectum receives at least 70% of the prescribed dose in the absence of ct scans [ 8 ]  . we created a microsoft excel spreadsheet to plan a bt boost after the completion of ebrt . 
4 segue infatti che il fattore di ripopolamento riduce lefficacia ( bedtumore ) tanto maggiormente quanto pi lunga la durata del trattamento . ottimizzazione avendo notato leffetto non trascurabile dei molti fattori di variabilit da paziente a paziente , ci si posti lobiettivo di calcolare , sia nel caso hdr sia nel caso ldr , il trattamento ottimale per ciascuna paziente , che dia il valore di bed desiderato al tumore con il minimo danno ai tessuti sani . 
la scelta del frazionamento hdr o della dose ldr quindi deve prevedere sicuramente la personalizzazione del trattamento , tenendo conto dei tempi della ebrt ( soprattutto in presenza di lunghi intervalli di attesa ) , della dose ebrt e dellintento terapeutico . 
per la finalit adiuvante esso prevede 281 , 8 gy ebrt + 12 gy bt , per quella radicale 281 , 8 gy ebrt + 52 gy ebrt su volume ridotto + 15 gy bt ; in entrambi i casi il dose - rate ritenuto ottimale di 0 , 7 gy / h . 
per il trattamento bt , la dose al bersaglio viene prescritta a 0 , 5 cm dalla superficie dellapplicatore , e per quanto riguarda la valutazione della bed al retto , in assenza di immagini tc si assume che questo riceva uniformemente almeno il 70% della dose prescritta [ 8 ]  . stata elaborata una cartella interattiva ( microsoft excel ) da utilizzare per pianificare il boost brachiterapico a trattamento ebrt gi concluso ; essa permette di individuare , per il singolo caso , il trattamento ottimale nel rispetto dei constraints dosimetrici . 
bedretto < 125 gy3 : tale limite stato desunto da studi con riscontro clinico [ 9 , 10 ] che utilizzano gli stessi valori dei parametri radiobiologici di questo lavoro . 
a < bedtumore < b : a e b dipendono dalla finalit del trattamento , in particolare nel nostro centro si utilizza a = 60 gy10 , b = 65 gy10 nel caso adiuvante e a = 70 gy10 , b = 75 gy10 in quello curativo . 
questi valori sono stati fissati calcolando bedtumore per i trattamenti di riferi1078 radiol med ( 2008 ) 113 : 10681078 adjuvant treatment and a = 70 gy10 , b = 75 gy10 for curative treatment . 
 input data are the radiobiological parameters and the ebrt parameters ( number of fractions , dose per fraction , time between end of ebrt and beginning of bt )  . 
in entrambi i casi si pu tenere memoria di diverse soluzioni allo scopo di valutare , a seguito di un confronto con il medico , quella migliore . conclusioni conclusions we found considerable variation in the biological effectiveness of bt , whether used in combination or as exclusive treatment . 
we therefore created an interactive microsoft excel spreadsheet that takes into account all of the variability factors and helps to plan optimal treatment for each patient , allowing us to achieve the required effectiveness whilst keeping within the toxicity threshold for normal tissue . si riscontrata una notevole variabilit di efficacia biologica nei trattamenti di brachiterapia , esclusivi e non . 
sartor springer - verlag , berlin heidelberg new york , 2008 isbn 978 - 3 - 540 - 33748 - 5 published online : 20 october 2008 springer - verlag 2008 on my desk sit the first and second editions of this successful book . 
what a change in their presentation : a huge increase in the number of pages ( from 195 to 360 ) ; an important increase in the number of chapters ( from 11 to 17 ) ; an incredible amount of perfectly reproduced images reflecting the use of the most advanced technical modalities in the study of the neonatal chest . 
the first edition was published in 2002 : what transpired in this short time span were the introduction of multidetector computed tomography ( ct ) , the increased use of magnetic resonance imaging ( mri ) and the ever - increasing importance of ultrasound ( us ) in the study of the neonatal chest . 
emphasis is duly placed on radiation protection and dose reduction , especially when using mdct . all the above factors are well described and demonstrated in this new edition . comparing the chapters of the old edition with those of the new one , the reader will find an increased amount of information , especially that which is dedicated to the antenatal and postnatal imaging of chest malformations . 
new chapters deal with computed and digital radiography in neonatal chest examination , computed tomography of the central and peripheral airways , ultrasound of the neonatal thorax , ultrasound in congenital heart disease , magnetic resonance imaging in congenital heart disease and computed tomography in congenital heart disease . 
che cambiamenti ! notevole la differenza nel numero delle pagine ( da 195 a 360 ) , laumento dei capitoli ( da 11 a 17 ) e lincredibile numero di immagini perfettamente riprodotte che riflettono luso delle pi avanzate tecniche di indagine nello studio del torace neonatale . 
in questo breve lasso di tempo quello che ha rivoluzionato la materia sono state lintroduzione della tc multi - detettore , il sempre pi largo uso della rm e la sempre pi evidente importanza dellecografia nello studio del torace neonatale . 
il risultato di tutto ci stato una riduzione significativa delluso dei cateterismi diagnostici , della sedazione o dellanestesia generale ( in particolare dopo lintroduzione della tcms ) , mentre segnalato lincremento nel numero delle procedure interventistiche cardio - vascolari , che offrono sempre pi spesso al paziente delle possibilit terapeutiche al di fuori di quelle chirurgiche . 
 se il lettore si prender la briga di confrontare i capitoli della vecchia con quelli della nuova edizione , trover un aumento nel numero di pagine del loro testo , in particolare in quelli dedicati allo studio delle malformazioni pree post - natali del torace . 
i nuovi capitoli sono dedicati a : computed and digital radiography in neonatal chest examination , computed tomography of the central and peripheral airways , ultrasound of the neonatal thorax , ultrasound in congenital heart disease , magnetic resonance imaging in congenital heart disease e computed tomography in congenital heart disease . 
in ciascuno di essi viene data una ottima visione e trattazione della materia . se un appunto pu essere rivolto agli autori degli stessi , questo riguarda luso degli acronimi che rende talvolta problematica la lettura e fa sorgere la domanda : che cosa significa questa abbreviazione ? vengono spesso ribaditi i concetti sulla protezione e la radiol med ( 2008 ) 113 : 10821083 1083 if a criticism must be made , it would be regarding the large use of acronyms , which often causes the reader ask : what does that mean ? i have found this book rich in information and most useful , and i recommend it not only to paediatric and adult radiologists but also to intensive care neonatologists , pediatric cardiologists , anaesthetists and obstetricians , as well as other professionals dealing with fetal ultrasound . riduzione della dose , cosa da tenere ben in conto , in particolare nelluso della tcmd . 
 ho trovato questo libro molto utile e ricco di informazioni e mi sento di raccomandarlo non solo ai radiologi delladulto e pediatrici , ma anche ai colleghi dei reparti di terapia intensiva neonatale , ai cardiologi , agli anestesisti ed agli ostetrici od a coloro che si occupano di ecografia fetale . 
scuro 10 , 37134 verona , italy correspondence to : mirko donofrio , tel . : + 39 - 045 - 8124301 , fax : + 39 - 045 - 8277808 , e - mail : mirko.donofrio@univr.it received : 22 august 2007 / accepted : 7 november 2007 / published online : 8 september 2008 springer - verlag 2008 abstract purpose . 
this study aimed to evaluate the diagnostic value of contrast - enhanced ultrasound ( ceus ) in characterising focal liver lesions in cirrhosis and to validate its use in lesions discovered during surveillance for hepatocellular carcinoma ( hcc )  . 
between 2003 and 2006 , 128 cirrhotic patients with focal liver lesions at baseline ultrasonography ( us ) were studied by power colour doppler us ( doppler us ) and ceus . 
 fine - needle biopsy or other reference modalities such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) or digital subtraction angiography ( dsa ) were used as the gold standard . 
the accuracy of baseline us , doppler us , afp levels , combined us and afp levels and combined us , doppler us and ceus in characterising focal liver lesions was assessed . 
valutare il valore diagnostico dellecografia con mdc ( ceus ) nella caratterizzazione delle lesioni focali epatiche in cirrosi , cercando di validarne lutilizzo qualora le lesioni focali epatiche siano scoperte in corso di sorveglianza per hcc . 
dal 2003 al 2006 , 128 pazienti affetti da cirrosi con lesioni focali epatiche sono stati sottoposti ad ecografia color - power doppler ( eco doppler ) e ad ecografia con mezzo di contrasto ( ceus )  . 
in tutti i pazienti sono stati valutati i livelli di alfa - fetoproteina sierica ( afp )  . la biopsia ad ago sottile o altre metodiche di riferimento quali la tomografia computerizzata , la risonanza magnetica o langiografia ( tc , rm , dsa ) sono state utilizzate come gold standard . 
stata valutata laccuratezza dellecografia , delleco doppler , del livello di afp , dellassociazione di ecografia con il livello di afp , dellassociazione di ecografia con eco doppler e ceus nella caratterizzazione delle lesioni focali epatiche . 
la sensibilit e la specificit del ceus nella caratterizzazione delle lesioni sono state rispettivamente del 96 , 2% e 97 , 0% ; i valori predittivi positivo e negativo sono stati del 97 , 1% e 96 , 1% . 
ceus can characterise focal liver lesions with 96.6% accuracy , a value higher than us , doppler us , afp levels , combined us and afp levels and combined us and doppler us . 
ceus should therefore be used to characterise focal liver lesions detected during hcc surveillance of cirrhotic patients . keywords contrast - enhanced ultrasonography ( ceus ) ultrasonography ( us ) hepatic cirrhosis focal liver lesions hepatocellular carcinoma ( hcc ) alphafetoprotein doppler us delleco doppler ( 70 , 0% ) , della afp ( 65 , 7% ) , dellassociazione tra ecografia e eco doppler ( 70 , 0% ) e dellecografia con afp ( 90 , 3% )  . 
il ceus permette di caratterizzare le lesioni focali epatiche con una accuratezza del 96 , 6% , pi alta dellecografia , delleco doppler , del livello di afp , dellassociazione di ecografia con lafp e dellecografia con eco doppler . 
lesame ceus dovrebbe quindi essere usato per caratterizzare lesioni focali epatiche riscontrate durante i programmi di sorveglianza della cirrosi . parole chiave ecografia con mezzo di contrasto ( ceus ) ecografia ( us ) cirrosi epatica lesioni focali epatiche carcinoma epatocellulare ( hcc ) alfa - fetoproteina ; doppler - us introduction introduzione cirrhosis is the main risk factor for hepatocellular carcinoma ( hcc ) [ 1 ] , the most common primary malignancy of the liver and one whose incidence has nearly doubled over the last 20 years [ 25 ]  . 
ultrasonography ( us ) and serum alpha - fetoprotein ( afp ) testing are the main screening methods for the early detection of hcc in patients with chronic liver disease and cirrhosis , even in the early stages [ 4 , 711 ]  . 
although the good spatial resolution of us ensures high sensitivity in detecting focal liver lesions , the technique has less capability for characterising small lesions , particularly in the cirrhotic liver [ 10 , 12 ]  . in the past 10 years , hepatic us imaging has experienced a technological revolution [ 13 ] brought about by the introduction of microbubble contrast agents that have made it possible to overcome the limitations of baseline ultrasound in identifying and characterising lesions [ 1420 ]  . the purpose of this study was to assess the value of contrast - enhanced us ( ceus ) in characterising focal lesions in liver cirrhosis and to attempt to validate its use in focal lesions detected in the course of hcc surveillance programmes . materials and methods la cirrosi il pi importante fattore di rischio per il carcinoma epatocellulare ( hcc ) [ 1 ] , che il pi comune tumore maligno primitivo del fegato ; la sua incidenza sta aumentando ed quasi duplicata negli ultimi 20 anni [ 25 ]  . 
lipervascolarizzazione in fase arteriosa dovuta alla assunzione di mezzo di contrasto , rispetto al parenchima epatico circostante , la caratteristica peculiare dellhcc [ 6 ]  . lecografia ( us ) ed il dosaggio dellalfa - fetoproteina sierica ( afp ) sono le principali metodiche di screening per la diagnosi di hcc precoce nei pazienti con malattie croniche e cirrosi , anche in stadio iniziale [ 4 , 711 ]  . 
lelevata risoluzione spaziale dellus garantisce una buona sensibilit nella identificazione delle lesioni focali epatiche , ma presenta un minor potenziale nella caratterizzazione delle lesioni pi piccole , in particolare nel fegato cirrotico [ 10 , 12 ]  . limaging del fegato mediante ultrasuoni stato rivoluzionato tecnologicamente negli ultimi dieci anni [ 13 ] , merito dei mezzi di contrasto ( mdc ) a microbolle che offrono lopportunit di valicare i limiti dellecografia basale nella identificazione e caratterizzazione delle lesioni [ 1420 ]  . lo scopo di questo studio stato di valutare il valore dellecografia con mdc ( ceus ) nella caratterizzazione delle lesioni focali epatiche in cirrosi , cercando di validarne lutilizzo qualora le lesioni focali epatiche siano scoperte in corso di sorveglianza per hcc . between 2003 and 2006 , 128 cirrhotic patients ( 80 men and 48 women ; age range 2183 years ; mean age , 46 ) with focal liver lesions identified at baseline us were studied with colour power doppler us ( doppler us ) and ceus . 
all materiali e metodi dal 2003 al 2006 , 128 pazienti , 80 maschi e 48 femmine ( range da 21 a 83 anni ; et media 46 ) , affetti da cirrosi con 980 radiol med ( 2008 ) 113 : 978991 lesions were also imaged with a second modality such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) or digital subtraction angiography ( dsa )  . 
nodules with indeterminate appearance on imaging ( or when the two imaging modalities were discordant ) were followed up at 3 months or examined by biopsy if > 1 cm , as reported in the literature [ 9 ]  . 
informed consent was obtained from all patients , and the study was approved by our institutional ethics committee . us imaging was performed on a sequoia 512 , 6.0 unit ( acuson , siemens , usa - germany )  . 
macrocirculation features were table 1 modalities used in the study of 207 focal liver lesions modality riscontro ecografico basale di lesioni focali epatiche , sono stati sottoposti ad ecografia mediante color - power doppler ( eco doppler ) e ceus . 
tutte le lesioni sono state studiate anche con una seconda modalit di imaging quale tomografia computerizzata ( tc ) , risonanza magnetica ( rm ) o angiografia digitale ( dsa )  . 
la diagnosi stata ottenuta mediante esame anatomo - patologico della lesione in 56 casi , di cui analisi istologica post - operatoria in 31 lesioni ed analisi citologica percutanea in 25 lesioni . 
i noduli non determinati allimaging ( o quando le due modalit sono state discordanti ) sono stati rivalutati dopo tre mesi o sottoposti a biopsia qualora maggiori di 1 cm , come riportato in letteratura [ 9 ]  . 
 gli esami ecografici sono stati eseguiti mediante apdiagnosis biopsy / surgery benign lesions regenerative nodule haemangioma focal nodular hyperplasia malignant lesions dysplastic nodule hepatocellular carcinoma diagnosi lesioni benigne nodulo di rigenerazione angioma iperplasia focale nodulare lesioni maligne nodulo displastico carcinoma epatocellulare tc , tomografia computerizzata ; rm , risonanza magnetica ; dsa , angiografia digitale ct , computed tomography ; mri , magnetic resonance imaging ; dsa , digital subtraction angiography tabella 1 metodiche utilizzate per lo studio delle 207 lesioni focali epatiche metodica biopsia / chirurgia 16 / / 30 16 / / 30 radiol med ( 2008 ) 113 : 978991 evaluated in all lesions with colour and powerdoppler us with spectral analysis of intraand peritumoural vessels . doppler imaging findings were considered diagnostic for hcc if they met the previously published criteria [ 10 , 11 ]  . all ceus exams were performed after the intravenous injection of a 2.4 - ml bolus of second - generation contrast material ( sonovue , bracco , milan , italy )  . 
lesion enhancement after contrast administration was compared with that of the liver parenchyma and classified as intralesional , peripheral , peripheral nodular , centrifugal and diffuse homogeneous or heterogeneous enhancement . 
during the dynamic study , lesion echogenicity appeared greater , equal to or less than the adjacent liver , so the lesion itself was classified as hypervascular or nonhypervascular in the arterial phase and as hyper - , isoor hypoechoic in the late phase , respectively . lesions showing even minimal partial intralesional hypoechogenicity in the late phase were classified as hypoechoic . lesion characterisation was based on previously reported enhancement patterns [ 17 , 18 ]  . 
the scanning protocol involved the acquisition of in - phase and out - of - phase t1 - weighted spoiled gradient echo , t2weighted turbo spin echo , and t2 - weighted turbo inversion recovery sequences , with 5 - mm thickness . 
dynamic images were obtained after the intravenous injection of gadobenate dimeglumine ( gd - bopta , multihance , bracco , italy ) with t1 - weighted gradient echo fs - 3d and vibe sequences in the arterial ( 30 s ) , portal ( 70 s ) , late ( 5 min ) and delayed ( 5 min and 1 h ) phases . angiography ( multistar plus t.o.p. , siemens , germany ) was always performed for therapeutic purposes ( transarterial chemoembolisation )  . the examinations on each patient were performed within a short time interval ( up to 3 weeks )  . 
lassunzione del mezzo di contrasto stata valutata dinamicamente , nelle fasi arteriosa ( 1020 secondi dopo liniezione del bolo ) , venosa portale ( 3040 secondi dopo liniezione del bolo ) e tardiva ( 120 secondi dopo liniezione del bolo )  . 
lenhancement della lesione dopo iniezione di mdc stata valutata rispetto al parenchima epatico , e classificata come intra - lesionale , periferica , nodulare periferica , centrifuga , diffusa omogenea o eterogenea . 
nel corso dello studio dinamico lecogenicit della lesione stata pi elevata , simile o minore del parenchima epatico adiacente , cos la lesione stessa stata definita rispettivamente come ipero non ipervascolare in fase arteriosa e come iper - , isoo ipo - ecogena nella fase tardiva . 
 gli esami tc sono stati eseguiti mediante apparecchio tc spirale a strato singolo ( somatom plus 4 , siemens , germania ) e multiplo ( philips brilliance , eindhoven , olanda ) dopo somministrazione intra - venosa di 130 ml di contrasto non ionico ( ultravist 370 , schering , germania ) ad una velocit di 3 , 5 ml / s . 
il protocollo ha previsto lacquisizione di sequenze spoiled gradient echo t1 - pesate in fase e fuori fase , turbo spin echo t2 - pesate , turbo inversion recovery t2 - pesate , a 5 mm di spessore . 
sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy for characterising lesions as benign or malignant were calculated for us , doppler us , afp levels , combined us and afp levels , combined us and doppler us and ceus . the sensitivity and specificity of ceus and us were compared using the mcnemar test with 95% confidence intervals ( ci )  . 
none of the patients had both benign and malignant lesions . benign lesions us identified 36 haemangiomas ( mean diameter 2.060.64 cm ; range 0.63.5 cm ) : 32 were hyperechoic , one was hyperechoic with a peripheral hypoechoic halo , two were hypoechoic and one was hypoechoic with a peripheral hyperechoic halo . 
on doppler us , six showed peripheral and intranodular arterial vessels , one had arterial vascularity with high velocity flow and resistive index and one showed absence of arterial flow and presence of venous flow . 
the two arteriosa ( circa 30 s ) , portale ( circa 70 s ) , tardiva ( 5 min ) ed in fase tardiva ( 5 minuti e 1 ora )  . la angiografia ( multistar plus t.o.p. , siemens , germania ) stata sempre eseguita con intento terapeutico ( chemioembolizzazione trans arteriosa )  . gli esami nel singolo paziente sono stati eseguiti in un breve periodo di tempo ( massimo 3 settimane )  . 
in presenza di diagnosi di benignit in almeno due metodiche di imaging , la lesione stata controllata a 3 e 6 mesi ( durata media 13 , 3 mesi )  . 
sono state calcolate la sensibilit , specificit , valore predittivo positivo ( ppv ) , valore predittivo negativo ( npv ) e accuratezza per la caratterizzazione della lesioni , in termini di benignit versus malignit , per lecografia , leco doppler , per il livello di afp , per lassociazione ecografia e livello di afp , per ecografia e eco doppler , e per il ceus . 
un valore di p < 0 , 05 stato ritenuto come significativo . risultati sono state riscontrate 207 lesioni focali epatiche ( range 0 , 518 cm , media 2 , 37 cm , deviazione standard 1 , 59 ) in 128 pazienti , 80 maschi e 48 femmine ( range da 21 a 83 anni ; et media 46 )  . 
centosei lesioni sono risultate maligne : 10 lesioni erano pre - maligne ( noduli displastici ) e 96 hcc , in 66 / 128 pazienti ( 51 , 6% )  . 
in nessun caso sono state riscontrate sia lesioni benigne che maligne . lesioni benigne allecografia sono stati identificati trentasei angiomi ( diametro medio 2 , 060 , 64 cm ; range 0 , 63 , 5 cm ) : 32 erano iper - ecogeni , 1 iper - ecogeno con alone periferico ipoecogeno , 2 ipoecogeni , e 1 ipoecogeno con alone periferico iper - ecogeno . 
twenty - six nodules appeared slightly or markedly hypoechoic with sharp allecografia sono state riscontrate anche 8 iperplasie focali nodulari ( fnh ) ( diametro medio 3 , 451 , 11 cm ; range 2 , 56 cm )  . 
allesame ecografico le iperplasie apparivano ipo - ecogene in 6 casi , disomogeneamente e tenuemente iper - ecogene in un caso , eterogenee nel caso 984 radiol med ( 2008 ) 113 : 978991 dellfnh . 
alleco doppler 6 mostravano vasi arteriosi periferici e intra - nodulari , in 1 caso vasi arteriosi ad alta velocit di flusso e resistenza ( fnh ) e in 1 caso assenza di flusso arterioso e presenza di flusso venoso . 
questi ultimi due lesioni sono stati correttamente caratterizzate mediante esame rm con mdc epatospecifico . allecografia la dimensione media dei 57 noduli rigenerativi era 1 , 570 , 72 cm ( range 0 , 54 cm )  . 
ventisei noduli apparivano tenuemente o fortemente ipo - ecogeni con margini delineati , 6 ipo - ecogeni a margini indefiniti , 24 iper - ecogeni a margini netti , e 1 disomogeneamente iperecogeno a margini indefiniti . 
un nodulo mostrava enhancement precoce nella fase arteriosa : questa lesione stata biopsiata con diagnosi patologica di nodulo rigenerativo . durante la fase tardiva , 55 noduli mostravano isoecogenicit rispetto al fegato circostante durante la fase arteriosa e tardiva ( tabella 2 )  . 
durante la fase tardiva una lesione era leggermente iper - ecogena , ed una ipo - ecogena ; la lesione ipo - ecogena stata sottoposta a biopsia , con diagnosi patologica finale di nodulo rigenerativo ( tabella 2 )  . 
la diagnosi di noduli rigenerativi stata effettuata con biopsia in 16 / 57 casi mentre nei rimanenti casi ci si basati sullassenza di modificazioni volumetriche e / o perfusionali dai 3 e 6 mesi fino a 16 mesi di follow - up . 
lafp era elevata ( > 20 ng / ml ) solo in 4 / 62 pazienti con lesioni benigne . allecografia sono stati riscontrati 10 noduli displastici ( diametro medio 1 , 910 , 55 cm ; range 12 , 5 cm )  . 
sette di queste lesioni erano ipo - ecogene con margini netti allecografia , 1 era ipo - ecogeno a margini sfumati , 1 ipoecogeno con unarea periferica iper - ecogena , e 1 tenuemente iper - ecogeno . 
la diagnosi di noduli displastici stata confermata allesame anatomo - patologico in tutti i casi . novantasei carcinomi epatocellulari sono stati riscontrati con lecografia in 57 pazienti ( 48 maschi e 9 femmine ; et media 67 , 2 anni )  . 
il ceus ( b ) mostra un nodulo ( freccia ) con enhancement sovrapponibile a quella del parenchima epatico adiacente durante la fase dinamica . margins , six were hypoechoic with ill - defined margins , 24 were hyperechoic with sharp margins and one was inhomogeneously hyperechoic with ill - defined margins . 
on doppler us , 54 nodules had peripheral venous vessels , two showed no intralesional flow and one showed an arterial flow with a low - flow velocity and resistive index . 
the diagnosis of regenerative nodules was confirmed by biopsy in 16 / 57 cases and the lack of any change in volume and / or perfusion at follow - up at 36 months up to 16 months . 
the diagnosis of dysplastic nodule was confirmed by pathological examination in all cases . us also identified 96 hepatocellular carcinomas in 57 allecografia era 2 , 932 , 01 cm ( range 118 cm )  . 
in 34 / 96 ( 35 , 4% ) casi lhcc aveva diametro minore di 2 cm mentre in 29 / 96 ( 30 , 2% ) tra 2 e 3 cin 26 / 57 pazienti lhcc era multifocale ; nei rimanenti singolo nodulo maligno . 31 / 57 era presente un allecografia 70 / 96 ( 72 , 9% ) hcc apparivano ipo - ecogeni : 19 / 70 mostravano disomogeneit ecostrutturale e 2 / 70 mostravano una piccola porzione iper - ecogena . 
allesame con eco doppler , 55 di 96 hcc ( 57 , 3% ) presentavano iper - vascolarizzazione ; in particolare il basket pattern era presente in 7 / 55 . 
in 34 / 96 cases ( 35.4% ) , the hcc was less than 2 cm in diameter , whereas in 29 / 96 cases ( 30.2% ) , it was 23 chcc was multifocal in 26 / 57 patients and unifocal in the remaining 31 / 57 . 
the us appearance of hcc was hypoechoic in 70 / 96 cases ( 72.9% ) : 19 / 70 showed inhomogeneous echostructure , and 2 / 70 exhibited a small hyperechoic area . 
in 6 / 96 ( 6.2% ) cases , the hccs were not hypervascular in the arterial phase but markedly hypoechoic in the late phase in four cases and isoechoic in two cases ( table 2 )  . 
 afp levels ranged from 20 to 400 ng / ml in 14 / 57 patients with malignant lesions ; 8 / 14 lesions were smaller than 3 cm . afp levels were > 400 ng / ml in 8 / 57 patients ; 5 / 8 lesions were smaller than 2 cm , one lesion had a diameter between 2 and 3 cm and two lesions were larger than 3 cm . table 3 summarises sensitivity , specificity and diagnostic accuracy of the modalities considered . 
sensitivity and specificity of us in lesion characterisation were 85.8% ( 91 / 106 ) and 57.4% ( 58 / 101 ) , respectively , with a ppv of 67.9% ( 91 / 134 ) , an npv of 79.4% ( 58 / 73 ) and a diagnostic accuracy of 72.0% ( 149 / 207 )  . 
thus , ceus had greater accuracy than us , doppler us , afp levels , combined us and doppler us and combined us and afp levels ( table 3 )  . 
 i valori di afp in 14 / 57 pazienti con lesioni maligne erano tra 20 e 400 ng / ml ; 8 / 14 lesioni erano minori di 3 cm . i valori di afp in 8 / 57 pazienti erano > 400 ng / ml ; 5 / 8 lesioni erano minori di 2 cm , una lesione era tra 2 e 3 cm e 2 / 8 erano maggiori di 3 cm . la sensibilit , specificit ed accuratezza delle indagini prese in considerazione sono riportate in tabella 3 . 
la sensibilit e la specificit dellecografia nella caratterizzazione delle lesioni sono state rispettivamente di 85 , 8% ( 91 / 106 ) e 57 , 4% ( 58 / 101 ) , con un valore predittivo positivo di 67 , 9% ( 91 / 134 ) , un valore predittivo negativo di 79 , 4% ( 58 / 73 ) e unaccuratezza del 72 , 0% ( 149 / 207 ) ( tabella 3 )  . 
in particolare laccurarisultata pi elevata tezza dellesame ceus dellecografia , delleco doppler , dei livelli di afp , dellassociazione tra ecografia e eco doppler , e tra ecografia e il livello di afp ( tabella 3 )  . 
le differenze nella sensibilit e specificit tra ceus ed ecografia basale sono state statisticamente significative ( p = 0 , 0074 e p < 0 , 0001 , rispettivamente )  . discussione lidentificazione e la caratterizzazione delle lesioni focali epatiche sono estremamente importanti per il trattamento dei pazienti cirrotici . 
il problema critico nella sorveglianza delle malattie epatiche croniche rappresentato dalla diagnosi di piccoli hcc e di lesioni premaligne , lesioni di cui certi autori raccomandano la resezione [ 6 ]  . 
la limite del sensibilit dellecografia rappresenta programma di sorveglianza dellhcc [ 4 , 10 ] , infatti negli studi con correlazione istologica del 30%60% e cala al 20% per lesioni minori di un centimetro o multifocali [ 3 , 4 , 811 ]  . alcuni autori hanno riportato che la combinazione con i livelli di afp aumentano la sensibilit e la specificit dellecografia al 79%87% [ 9 , 21 ]  . 
il ceus rileva che il nodulo ( freccia ) ha una maggiore assunzione di mdc nella fase arteriosa risultando isoecogeno rispetto al resto del parenchima epatico in fase tardiva ( c , d )  . very important in managing cirrhotic patients . 
us sensitivity is the main limitation of surveillance programmes for hcc [ 4 , 10 ] , given that histological correlation studies have reported a sensitivity of 30%60% , which decreases to 20% for lesions < 1 cm or multifocal lesions [ 3 , 4 , 811 ]  . zione ecografia e afp ha mostrato una sensibilit del 100% , confermando lefficacia del programma di sorveglianza [ 22 ]  . 
 ad ogni modo stato dimostrato che pi di un terzo delle diagnosi falsi positivi di hcc rappresentato da angiomi , piccoli shunts artero - venosi e pseudoaneurismi [ 12 ]  . 
infatti la caratterizzazione delle lesioni focali epatiche pu essere estremamente difficoltosa in pazienti con malattia epatica cronica [ 20 ] , e allecografia basale le lesioni focali epatiche frequentemente rappresentano un problema diagnostico , specialmente in corso di cirrosi [ 20 , 23 , 24 ]  . va sottolineato tuttavia come nella nostra casistica quasi tutti gli angiomi hanno dimostrato caratteristiche tipiche al ceus agevolandone la diagnosi . 
il ceus rileva che il nodulo ( freccia ) ha una maggiore assunzione di mdc nella fase arteriosa ( b ) risultando lievemente ipo - ecogeno rispetto al resto del parenchima epatico in fase tardiva ( c )  . some authors have reported that the combination of us and afp levels increases sensitivity and specificity to 79%87% [ 9 , 21 ]  . 
characterising focal liver lesions can prove very difficult in patients with chronic liver disease [ 20 ] , and focal liver lesions , especially when encountered in cirrhosis , frequently represent a diagnostic challenge on us [ 20 , 23 , 24 ]  . 
 alto flusso e piccoli shunts artero - venosi ha sicuramente contribuito alla accuratezza della metodica risultata nella caratterizzazione lesionale . nella nostra serie la combinazione ecografia e livelli di afp stata in grado di caratterizzare le lesioni focali epatiche riscontrate allecografia con una sensibilit e specificit rispettivamente del 90 , 6% e 90 , 1% . 
 tra le lesioni benigne epatiche , 32 / 36 angiomi hanno mostrato il classico aspetto iper - ecogeno allecografia ; altres , la maggioranza delle lesioni benigne avevano un aspetto indeterminato . 
i livelli di afp erano elevati in 4 / 62 pazienti con lesioni benigne e in solo 22 / 56 pazienti con lesioni maligne . tra le lesioni maligne , solo 10 / 96 ( 10 , 4% ) hcc hanno mostrato il classico aspetto a mosaico allecografia , mentre 13 / 96 ( 13 , 5% ) sono apparse maggiormente iperecogene . 
questo secondo aspetto , che mima gli angiomi , spiegato dalla degenerazione neoplastica degli epatociti , frequentemente accompagnata da aree iper - ecogene di metaplasia grassosa [ 25 ]  . 
afp levels were elevated in 4 / 62 patients with benign lesions and in only 22 / 56 patients with malignant lesions . among malignant lesions , only 10 / 96 ( 10.4% ) hccs exhibited the classic mosaic pattern at us , whereas 13 / 96 ( 13.5% ) appeared mostly hyperechoic . 
this hyperechoic appearance mimics that of haemangiomas and is explained by the neoplastic degeneration of hepatocytes that is frequently accompanied by hyperechoic areas of fatty change [ 25 ]  . 
study of the vascularity of liver lesions is therefore crucial , and doppler us can help identify the macrocirculation of the lesion by evaluating its qualitative and quantitative characteristics [ 10 ]  . 
this result , only in part consistent with previous reports [ 18 , 19 ] , might be related to the classification of lesions during the late phase adopted in our study . 
this no doubt influenced the accuracy of ceus reported in our study . ceus is a relatively new imaging technique that has been shown to improve characterisation of focal liver lesions , with zione delle lesioni epatiche perci cruciale . 
tale risultato , solo parzialmente aderente ai risultati riportati in letteratura [ 18 , 19 ] , deriverebbe dalla classificazione delle lesioni in fase post - contrastografica tardiva adottata nel presente studio . 
questo criterio adottato per la rilettura trova giustificazione nella tipologia della popolazione oggetto di studio , costituita esclusivamente da pazienti affetti da cirrosi , al fine di garantire la pi elevata sensibilit nei confronti della malignit . 
questo ha sicuramente influenzato i risultati di accuratezza del ceus riportati nel presente studio . la ceus una tecnica di imaging relativamente nuova che sta dimostrando di migliorare la caratterizzazione delle lesioni focali epatiche , con risultati simili a tc e rm [ 18 , 24 , 2629 ]  . 
nella nostra serie , la ceus ha permesso di caratterizzare come iper - vascolari in fase arteriosa 90 / 96 ( 93 , 7% ) noduli di hcc , 41 dei quali ( 42 , 7% ) non erano iper - vascolari alleco doppler . 
in our series , ceus allowed 90 / 96 hcc nodules ( 93.7% ) to be characterised as hypervascular during the arterial phase ; of these 41 ( 42.7% ) were not hypervascular on doppler us . 
this result confirms that the late phase is helpful in characterising liver lesions , despite reports of its limited value for detecting hccs in hepatic cirrhosis [ 32 ]  . the main limitation of our study is the lack of histological confirmation for all lesions detected at baseline us and studied with ceus . 
ceus should therefore be used to characterise focal liver lesions detected during surveillance for hcc in patients with chronic liver disease . ceus sta dimostrando di essere utile nel confermare la natura maligna dei noduli sospetti [ 30 , 31 ]  . 
questo risultato conferma come la fase tardiva sia di aiuto nella caratterizzazione delle lesioni epatiche , anche se in letteratura il valore della fase tardiva nella determinazione dellhcc nella cirrosi epatica appare limitato [ 32 ]  . lesioni istologica per il maggior limite del nostro studio la mancanza della identificate conferma tutte allecografia basale e approfondite mediante ceus : anche se la diagnosi definitiva di alcune lesioni , specialmente le benigne , pu essere ragionevolmente ottenuta tramite la correlazione tra metodiche imaging differenti o mediante follow - up . 
i risultati del nostro studio supportano lintroduzione del ceus nei programmi di sorveglianza per hcc in pazienti affetti da cirrosi per migliorare la caratterizzazione delle lesioni focali epatiche immediatamente dopo la loro scoperta . conclusioni lo studio ceus permette di caratterizzare le lesioni focali epatiche in pazienti con cirrosi con unaccuratezza del 96 , 6% , pi elevata dellecografia , delleco doppler , dei livelli di afp , dellassociazione tra ecografia e eco doppler , e tra ecografia e il livello di afp . 
zompatori3 1scuola di specializzazione in radiodiagnostica , universit degli studi di parma , azienda ospedaliero - universitaria di parma , via gramsci 11 , 43100 parma , italy 2radiologia canini , policlinico s . 
due radiologi con differenti livelli di esperienza hanno separatamente ricercato le anomalie vertebrali presenti in tali pazienti e le hanno classificate in lievi , moderate e severe secondo lindice semiquantitativo di genant . 
diciotto pazienti ( 18 / 145 = 12 , 4% ) presentavano fratture vertebrali clinicamente rilevanti : moderate 13 pazienti , severe 5 ; fratture singole in 12 pazienti , multiple in 6 . la concordanza tra i due esaminatori stata molto elevata ( = 0 , 9 )  . 
il radiogramma toracico laterale pu rappresentare un vantaggioso sistema per identificare le fratture vertebrali osteoporotiche non note in una popolazione asintomatica e senza fattori di rischio per osteoporosi . radiol med ( 2008 ) 113 : 968977 keywords osteoporosis vertebral fractures chest radiograph parole chiave osteoporosi fratture vertebrali radiogramma toracico introduction introduzione osteoporosis is the most common metabolic degenerative bone disease . 
low bone mass and deterioration of normal bone microarchitecture in this disease increase skeletal fragility and the risk of disabling fractures , mainly of the pelvis , femur , wrist , and vertebrae [ 1 ]  . 
because these processes are age - related , the incidence of osteoporotic fractures has considerably increased in recent decades as a result of the ageing population and longer life expectancy . 
osteoporosis has thus become a major public health problem from a health care , social and economic perspective [ 2 ]  . vertebral fractures are the most frequent and early manifestations of osteoporosis , and they often represent the first clinical manifestation of the disease . 
severe cases with multiple vertebral fractures may develop the vertebral fracture syndrome , in which hyperkyphosis leads to altered respiratory mechanics , decreased lung volume , and eventually respiratory failure . 
 to assess the prevalence of unknown and clinically unsuspected osteoporotic vertebral deformities or fractures , we prospectively reviewed 314 digital chest radiographs in the lateral projection performed on outpatients for various indications unrelated to osteoporosis . 
the aim of our study was to verify the usefulness and appropriateness of lateral chest radiographs performed for other reasons to screen for undiagnosed osteoporotic fractures requiring specific diagnostic investigation in a population with no clinical risk factors for osteoporosis . materials and methods between november and december 2006 , 314 consecutive outpatients underwent posteroanterior and lateral digital chest radiography for various indications at the radiology division of our university hospital . 
in particular , we looked for the presence of current or past neoplasms , chronic losteoporosi la pi comune osteopatia metabolico - degenerativa in cui la perdita di massa ossea e il deterioramento della normale micro - architettura dellosso si traducono in una aumentata fragilit dello scheletro e , conseguentemente , in un maggior rischio di fratture patologiche , specie a carico di bacino , femore , polso e vertebre [ 1 ]  . 
trattandosi di processi correlati allet , lincidenza delle fratture su base osteoporotica notevolmente incrementata negli ultimi decenni in relazione allaumento dellet media della popolazione e dellaspettativa di vita ; per tali motivi losteoporosi costituisce oggi un rilevante problema di salute pubblica dal punto di vista sanitario , sociale ed economico [ 2 ]  . le fratture vertebrali sono le pi frequenti e precoci manifestazioni dellosteoporosi e spesso rappresentano la prima evidenza clinica della malattia , causando dolore cronico , accentuazione della fisiologica cifosi dorsale , con riduzione della statura e progressiva limitazione funzionale [ 1 , 3 , 4 ]  . 
nei casi pi severi , in presenza di fratture vertebrali multiple , si pu configurare la cosiddetta sindrome da fratture vertebrali in cui lipercifosi dorsale porta ad una alterazione della meccanica ventilatoria con riduzione dei volumi polmonari ed insufficienza respiratoria . 
pertanto , molte di esse rappresentano un riscontro accidentale nel corso di esami radiografici eseguiti per altri motivi , compresi i radiogrammi del torace . abbiamo pertanto condotto uno studio prospettico basato sul riesame di 314 radiogrammi digitali del torace in proiezione laterale eseguiti in regime ambulatoriale per varie indicazioni non correlate allosteoporosi in pazienti di entrambi i sessi , di et superiore ai 50 anni , senza manifestazioni cliniche o specifici fattori di rischio per osteoporosi al fine di valutare la prevalenza di deformit o fratture vertebrali osteoporotiche non note , n sospettate clinicamente . 
obiettivo del nostro studio quello di verificare lutilit e lappropriatezza del radiogramma laterale del torace eseguito per altri motivi come esame di screening delle fratture osteoporotiche misconosciute e meritevoli di approfondimenti diagnostici mirati in questo tipo di popolazione non clinicamente a rischio per osteoporosi . materiali e metodi nel periodo novembre - dicembre 2006 presso la sezione e u.o.c. 
di scienze radiologiche della nostra azienda ospe970 radiol med ( 2008 ) 113 : 968977 table 1 study exclusion criteria tabella 1 criteri di esclusione della popolazione di studio exclusion parameters patients ( 169 ) criteri di esclusione pazienti ( 169 ) age < 50 years known neoplastic disease ( current or past ) chronic use of steroid drugs ( current or past ) chronic renal failure vertebral trauma bone marrow or organ transplantations known history of osteoporosis et < 50 anni storia di malattia neoplastica ( attuale o pregressa ) 68 terapia steroidea cronica ( attuale o pregressa ) insufficienza renale cronica ( irc ) traumi vertebrali trapianti dorgano o di midollo osseo pregressa diagnosi di osteoporosi steroid treatment , vertebral trauma , chronic renal failure ( crf , with / without haemodialysis ) and organ or bone marrow transplantation ; in women , we also recorded age at menopause and use of hormone replacement therapy . 
on the basis of these data , 169 patients were excluded ( table 1 ) and the remaining 145 patients , representing a population not clinically at risk for osteoporosis , were considered eligible for the study . chest radiographs of the 314 patients were acquired with digital equipment ( dr axiom aristos fx , siemens ; 125 kv , 0.89 mas for the posteroanterior projection ; 122 kv , 2.03 mas for the lateral projection ) and stored on the hospital digital archives ( pacs ; picture archiving and communication system )  . 
the radiographs of the patients included in the study were then independently reviewed by a trainee radiologist ( vc ) , who was instructed in the radiographic assessment of osteoporotic vertebral fractures , and by a radiologist with extensive experience in chest disease ( mz )  . all vertebrae clearly visualised on the lateral radiograms were separately reviewed by applying a semiquantitative method based on the visual estimation of the anterior , central and posterior heights of each vertebral body . 
vertebral anomalies were classified according to the genant index ( also known as the sfi ; spinal fracture index ) into mild ( grade 1 ) , moderate ( grade 2 ) and severe ( grade 3 ) , regardless of fracture morphology ( wedge , biconcave , or crush ) ( table 2 )  . 
discrepant interpretations were resolved by consensus . eight patients with grades 2 and 3 vertebral fractures ( 8 / 18 ) subsequently underwent , with their consent and in agreement with the referring physician , targeted spine daliero - universitaria sono stati eseguiti consecutivamente radiogrammi digitali del torace in 2 proiezioni ( postero - anteriore e laterale ) a 314 pazienti in regime ambulatoriale , per varie indicazioni . 
in particolare abbiamo indagato la presenza di neoplasie attuali o pregresse , terapie steroidee croniche , traumi vertebrali , insufficienza renale cronica ( irc , con / senza terapia emodialitica ) e trapianti dorgano o di midollo ; nelle donne abbiamo registrato let menopausale e leventuale terapia ormonale sostitutiva ; inoltre abbiamo verificato che non fosse gi stata posta diagnosi di osteoporosi e iniziato leventuale trattamento . 
abbiamo infine registrato i dati anagrafici con particolare riferimento allet . sulla base di questi dati abbiamo escluso 169 pazienti ( tabella 1 ) ; i rimanenti 145 pazienti , rappresentando una popolazione non clinicamente a rischio per osteoporosi , sono risultati eleggibili per il nostro studio . i radiogrammi toracici dei 314 pazienti sono stati acquisiti con tecnica digitale ( dr axiom aristos fx , siemens ; parametri tecnici di acquisizione : 125 kv , 0 , 89 mas per la proiezione postero - anteriore ; 122 kv , 2 , 03 mas per la proiezione laterale ) , archiviati nellarchivio digitale ospedaliero ( pacs ) e inizialmente esaminati e refertati dal radiologo di turno . 
finally , official reports of chest radiographs performed on the 145 patients were reviewed to verify the prevalence of documented vertebral fractures . results our study population included 145 patients , 73 men and 72 women ( age range 5086 years ; mean age 67.5 ) , who met the inclusion criteria . 
the most frequent indications for chest radiography were respiratory symptoms ( 37% ) or follow - up of lung diseases ( 11% ) , heart disease ( 16% ) , screening in heavy smokers ( 9% ) and chest or cervical pain ( 8% )  . evaluation of the lateral chest radiographs revealed that 18 patients were affected by clinically relevant osteoporotic vertebral fractures : five were women aged from 76 to 84 years ( mean 82 years ) , and the other 13 were men aged from 50 to 86 years ( mean age 68 years )  . 
abbiamo definito frattura vertebrale solo le deformit moderate - severe ( gradi 23 ) , equivalenti ad una riduzione di una delle tre altezze del corpo vertebrale maggiore o uguale al 25% . 
stata successivamente eseguita una terza lettura comune per trovare un accordo di valutazione nei casi in cui erano emerse differenze interpretative . otto dei pazienti risultati portatori di fratture vertebrali di grado 2 e 3 ( 8 / 18 ) sono stati successivamente sottoposti , con il loro consenso ed in accordo con i rispettivi medici curanti , ad un studio radiografico mirato del rachide per confermare i rilievi emersi dal radiogramma toracico laterale e verificare la eventuale presenza di simili alterazioni vertebrali anche nel tratto lombare della colonna vertebrale ; negli altri pazienti non sono state eseguite ulteriori indagini di approfondimento per rifiuto ( 2 pazienti ) o perch non erano rintracciabili ( 8 pazienti )  . 
allo scopo di verificare laffidabilit e la riproducibilit del metodo visivo semiquantitativo da noi applicato per la identificazione e la classificazione delle frattu972 radiol med ( 2008 ) 113 : 968977 re vertebrali abbiamo valutato statisticamente la variabilit interosservatore attraverso il calcolo del parametro statistico k . 
infine abbiamo riesaminato i referti ufficiali degli esami dei 145 pazienti inclusi nello studio per verificare la prevalenza delle fratture vertebrali segnalate nei referti . risultati la nostra popolazione di studio composta da 145 pazienti , 73 maschi e 72 femmine con et compresa tra 50 e 86 anni ( et media 67 , 5 anni ) che soddisfacevano i criteri di inclusione prestabiliti . 
le pi comuni indicazioni allesame radiografico attuale erano : presenza di sintomi respiratori ( 37% ) o follow - up di patologie polmonari ( 11% ) , patologie cardiache ( 16% ) , controllo in pazienti forti fumatori ( 9% ) , dolore toracico o cervicalgia ( 8% )  . dallanalisi dei radiogrammi toracici in proiezione laterale , 18 di questi pazienti sono risultati affetti da fratture vertebrali osteoporotiche clinicamente rilevanti : 5 pazienti erano donne di et compresa tra 76 e 84 anni ( media 82 anni ) , i restanti 13 erano maschi tra 50 e 86 anni ( et media 68 anni )  . 
le deformit vertebrali riscontrate interessavano con maggior frequenza il tratto dorsale medio - inferiore del rachide ( 9 / 18 ) ; in altri 8 casi erano localizzate al tratto dorsale medio mentre in un solo paziente il tratto dorsale superiore . 
 nella successiva fase dello studio , i radiogrammi mirati del rachide dorsale e lombare ( disponibili in 8 / 18 pazienti ) hanno confermato i rilievi patologici del radiogramma toracico in 6 casi ; in uno di questi emergeva anche una ulteriore frattura vertebrale localizzata in una delle prime vertebre dorsali e per questo non visualizzabile nel radiogramma toracico laterale per motivi di sovrapposizione con altre strutture . 
2 il radiogramma toracico in proiezione laterale di una donna di 77 anni ha evidenziato la presenza di due fratture vertebrali severe non sospettate clinicamente a carico del tratto superiore ( d4 ) e medio ( d8 ) del rachide dorsale ( frecce )  . the overall prevalence of vertebral fractures was 12.4% ( 18 / 145 ) ( table 3 )  . 
the vertebral deformities tended to involve the mid - lower thoracic spine ( 9 / 18 ) ; eight cases involved the mid thoracic spine and one case only involved the upper thoracic spine . 
in two patients only had these findings been documented in the official reports ( 2 / 18 ; 11% )  . characterisation of moderate and severe vertebral deformities with genants method did not raise any diagnostic doubts in the two readers . 
diversamente dalle fratture dellanca o del polso , meno comuni ma usualmente pi gravi ed invalidanti , le fratture vertebrali risultano spesso asintomatiche e rimangono clinicamente non riconosciute fino a 2 / 3 dei casi [ 1 , 2 , 4 , 5 ]  . 
il valore della densit minerale ossea ( dmo ) rappresenta il singolo pi importante fattore predittivo delle fratture osteoporotiche . tuttavia , sebbene esista un rapporto lineare e continuo tra riduzione della densit ossea ed aumento del rischio di fratture , valori normali di dmo non escludono completamente la possibilit di insorgenza di fratture da fragilit ma indicano semplicemente che tale evento meno probabile [ 6 , 7 ]  . 
infatti bisogna anche considerare che le nuove tecniche densitometriche di misurazione della densit minerale ossea quali la dxa ( dual energy x - ray absoptiometry ) , per quanto accurate e precoci nel porre diagnosi di osteoporosi ( dmo 2 , 5 ds rispetto ai normali valori di picco di massa ossea di riferimento , secondo la definizione della world health organization ) [ 8 , 9 ] eseguono una stima puramente quantitativa che non tiene conto della struttura dellosso e la qualit del tessuto osseo residuo , che pure possono incidere significativamente sul rischio di frattura [ 7 ]  . 
inoltre , poich la dmo ha una distribuzione gaussiana e la maggior parte della popolazione presenta valori di dmo che rientrano nellarea centrale della curva di distribuzione , molte fratture vertebrali da fragilit si verificano in soggetti con valori di densit ossea ancora nei limiti della norma [ 1 , 6 , 7 ]  . 
3 nel radiogramma laterale del torace riscontro accidentale di due deformit vertebrali moderate - severe adiacenti a carico dei corpi di d6 e d7 ( frecce ) in un uomo di 50 anni , asintomatico per osteoporosi . confirmed the findings of the chest radiographs in six cases . in one of these cases , an additional fracture was evidenced in one of the uppermost thoracic vertebrae , which was obscured by overlapping structures on the lateral chest radiograph . 
in two patients , vertebral deformities classified as moderate on chest radiography proved to be mild and hence not clinically relevant . table 3 vertebral fractures incidentally detected on lateral chest radiographs tabella 3 fratture vertebrali riscontrate incidentalmente al radiogramma laterale del torace vertebral fractures characteristics caratteristiche delle fratture vertebrali moderate severe single multiple contiguous noncontiguous upper thoracic region mid - thoracic region lower thoracic region fractures already mentioned in the official radiology reports patients ( n = 145 ) 13 ( 9% ) 5 ( 3 , 4% ) moderate severe singole multiple adiacenti non adiacenti toraciche superiori medio - toraciche toraciche inferiori fratture riportate nei referti ufficiali pazienti ( n = 145 ) 13 ( 9% ) 5 ( 3 , 4% ) 974 discussion osteoporosis is an important public health problem worldwide , and vertebral fractures , the earliest and most frequent clinical sign of disease , are responsible for substantial morbidity in the middleto advanced - age population [ 2 ]  . 
unlike hip or wrist fractures that are less common but more severe and disabling , vertebral fractures are often asymptomatic and remain clinically unrecognised in almost 2 / 3 of cases [ 1 , 2 , 4 , 5 ]  . 
bone mineral density ( bmd ) is the single most important predictive factor for osteoporotic fractures . however , despite the linear , continuous relationship between bone density reduction and increased risk of fractures , normal bmd alone cannot rule out the possibility of fragility fractures but only indicates that these are less likely [ 6 , 7 ]  . 
moreover , the newer techniques for bmd measurement such as dual - energy x - ray absorptiometry ( dxa ) , despite allowing an accurate and early diagnosis of osteoporosis [ bmd 2.5 standard deviations ( sd ) below the mean peak values for normal bone according to the world health organization ] [ 8 , 9 ] , provide only a quantitative estimation that does not account for bone structure and quality of residual bone , which may significantly affect the risk of fractures [ 7 ]  . 
additionally , because bmd has a gaussian distribution and most subjects have bmd values in the central area of the curve , many fragility fractures occur in patients with bmd within normal limits [ 1 , 6 , 7 ]  . for example , in the large longitudinal national osteoporosis risk assessment ( nora ) study , 82% of women who developed osteoporotic fractures during the observation period had t scores > 2.5 sd , and 67% had scores > 2 [ 6 ]  . 
 in contrast , additional risk factors and especially preexisting vertebral fractures , even mild and asymptomatic , have been shown to increase the predictive value of bmd [ 6 , 7 , 10 , 11 ]  . on the basis of these considerations , the world health organization [ 8 ] and national osteoporosis foundation [ 12 ] guidelines state that bone mass measurement alone is insufficient for evaluating fracture risk in osteoporotic patients and that radiographic evidence of a vertebral deformity or fracture , even if mild and asymptomatic , can effectively prevent severe disabling vertebral fractures by allowing the institution of pharmacological treatment for osteoporosis [ 4 , 12 ]  . 
early diagnosis of vertebral fractures , even those not associated with clinical symptoms and / or reduced bone mass , could thus reduce the morbidity , health care and economic impact of osteoporosis . 
in routine clinical practice , the diagnosis of suspected osteoporosis and / or vertebral compression fractures relies on targeted spine radiographs in two projections ( anteroposterior and lateral ) [ 9 ] , followed by vertebral morphometry ( voxel - based morphometry , vbm )  . according to a recent paper by chassang et al . 
 [ 13 ] , radiol med ( 2008 ) 113 : 968977 dio longitudinale statunitense nora ( national osteoporosis risk assessment ) , l82% delle donne che avevano sviluppato fratture osteoporotiche nel periodo di osservazione presentava valori di t - score > 2 , 5 ds e il 67% valori > 2 [ 6 ]  . 
per contro , provato che fattori di rischio aggiuntivi ed in particolare la presenza di una pre - esistente frattura vertebrale , anche se lieve ed asintomatica , aumentano il valore predittivo della dmo [ 6 , 7 , 10 , 11 ]  . sulla base di queste considerazioni le linee guida internazionali della world health organization [ 8 ] e della national osteoporosis foundation [ 12 ] affermano che nella valutazione del rischio fratturativo del paziente osteoporotico la sola misurazione della massa ossea non sufficiente ; al contrario , levidenza radiografica di una deformit o frattura vertebrale , anche lieve ed asintomatica , rappresenta il pi efficace sistema per prevenire le fratture vertebrali pi gravi e clinicamente invalidanti attraverso la terapia farmacologica dellosteoporosi [ 4 , 12 ]  . 
pertanto la diagnosi precoce delle fratture vertebrali , anche se non associate a sintomatologia clinica e / o ridotta massa ossea potrebbe essere un valido sistema per ridurre la morbilit e limpatto sanitario ed economico legato a questa patologia . 
nella pratica clinica comune , liter diagnostico del paziente con sospetta osteoporosi e / o fratture vertebrali da compressione prevede in prima istanza lesecuzione del radiogramma mirato del rachide in 2 proiezioni ( antero - posteriore e laterale ) [ 9 ] su cui eseguire la morfometria vertebrale ( morfometria radiografica , mrx )  . secondo un recentissimo lavoro di chassang [ 13 ] , inoltre , la tc multislice a bassa dose , pur non essendo un esame di primo livello , potrebbe essere una realistica alternativa al radiogramma standard in pazienti sintomatici affetti da diverse patologie scheletriche del rachide . 
paragonando le immagini del rachide di 111 pazienti affetti da mieloma multiplo , metastasi vertebrali e fratture vertebrali osteoporotiche ottenute con tc a bassa dose e radiogrammi standard in due proiezioni lautore ha osservato che con la tc si pu raggiungere una maggiore sensibilit diagnostica ( sia in termini di numero di lesioni vertebrali individuate sia di lesioni extra - scheletriche associate e non sospettate clinicamente ) e con pi brevi tempi tecnici di esecuzione dellesame , a scapito di una maggior dose erogata ai pazienti considerata tuttavia trascurabile in considerazione del rapporto rischio - beneficio . poich le fratture vertebrali su base osteoporotica si localizzano elettivamente nel tratto medio del rachide dorsale ( specie d7d8 ) ed al passaggio dorso - lombare ( d12l1 ) , molte di esse possono risultare adeguatamente visualizzabili anche nei radiogrammi toracici in proiezione laterale [ 5 , 14 ]  . 
in letteratura alcuni recenti studi hanno descritto la possibilit di individuare la presenza di fratture vertebrali misconosciute nei radiogrammi del torace in proiezione laterale eseguiti routinariamente per altre indicazioni radiol med ( 2008 ) 113 : 968977 low - dose multislice computed tomography ( ct ) , though not a first - level examination , could be a realistic alternative to conventional radiography in symptomatic patients with different spine diseases . 
by comparing the images of 111 patients with multiple myeloma , vertebral metastases and osteoporotic fractures obtained with low - dose ct and conventional two - view radiography , the authors found that ct had better diagnostic sensitivity ( in terms of both the number of vertebral lesions and unsuspected associated extraskeletal lesions ) and shorter examination times compared with conventional radiography . 
the higher radiation dose of ct was considered negligible in relation to the risk - benefit ratio . as osteoporotic vertebral fractures tend to be located in the mid - thoracic spine ( mainly t7t8 ) and dorsolumbar spine ( t12l1 ) , many of them may be easily visualised also on lateral chest radiographs [ 5 , 14 ]  . 
recent studies have reported on the possibility of identifying vertebral fractures on lateral chest radiographs performed for other indications [ 5 , 1416 ] and have investigated the real contribution of lateral chest radiography in detecting unknown vertebral fractures . 
 [ 15 ] found a 14% prevalence of previously unknown moderatesevere osteoporotic fractures . in another series of 106 postmenopausal women studied with chest radiography for different indications , mui et al . [ 5 ] identified undiagnosed osteoporotic fractures in 25% of cases ( 26 / 106 )  . 
 [ 14 ] reported a 22% prevalence of osteoporotic vertebral fractures on the chest radiographs of 100 patients ( women and men older than 60 years ) presenting to the emergency department for various reasons . 
according to this method , the lateral chest radiographs are evaluated visually , and each vertebral fracture is classified as normal , borderline , mild , moderate or severe , depending on the extent of reduction of the three vertebral heights ( anterior , central and posterior ) ( table 2 ) [ 17 ]  . 
although this aspect simplifies the interpretation of the deformities , it also constitutes a disadvantage , as biconcave deformity ( reduced central vertebral height ) is known to increase the risk of future fractures [ 18 ]  . 
despite these limitations , the genant index has been [ 5 , 1416 ] ed hanno indagato il reale contributo del radiogramma toracico laterale nella diagnosi di fratture vertebrali ancora misconosciute . 
 [ 15 ] , in un lavoro eseguito su una popolazione di 934 donne in et postmenopausale , hanno osservato dallanalisi dei loro radiogrammi toracici laterali una prevalenza di fratture osteoporotiche di grado moderato - severo non precedentemente note del 14% . 
 [ 14 ] hanno indagato la prevalenza di fratture vertebrali osteoporotiche nei radiogrammi toracici di 100 pazienti ( uomini e donne di et superiore ai 60 anni ) afferiti al dipartimento di emergenza per altri motivi : la prevalenza osservata stata del 22% . 
 [ 16 ] i quali riportano una prevalenza di fratture vertebrali misconosciute identificate con i radiogrammi toracici del 16% . nel nostro studio abbiamo riscontrato una prevalenza di fratture osteoporotiche moderate - severe non note del 12 , 4% . 
secondo tale metodo , effettuando una valutazione puramente visiva dei radiogrammi in proiezione laterale , le singole vertebre vengono classificate in normali , borderline , fratture lievi , moderate e gravi sulla base dellentit della riduzione delle tre altezze vertebrali ( anteriore , centrale e posteriore ) ( tabella 2 ) [ 17 ]  . 
se da un lato questo aspetto costituisce un vantaggio del metodo , perch semplifica linterpretazione delle deformit osservate , dallaltro rappresenta un limite poich si visto che la deformit a lente biconcava ( riduzione dellaltezza centrale ) quella associata al maggior rischio di insorgenza di successive ulteriori fratture [ 18 ]  . 
nonostante questi limiti lindice di genant stato adottato sia dalla international osteoporosis foundation che dalla european society of skeletal radiology perch si dimostrato un metodo rapido , affidabile ed altamente riproducibile per la diagnosi sia di prevalenza che di incidenza della fratture vertebrali su base osteoporotica [ 18 ]  . 
 [ 19 ] , ha studiato la concordanza tra la valutazione semiquantitativa di genant e diversi metodi quantitativi dimostrando che con il primo metodo sono risultate superiori sia la concordanza intra - osservatore che quella inter - osservatore . nella nostra casistica solo l11% ( 2 / 18 ) delle fratture in976 radiol med ( 2008 ) 113 : 968977 adopted by both the international osteoporosis foundation and the european society of skeletal radiology owing to its rapidity , reliability and reproducibility in the diagnosis of prevalent and incident osteoporotic vertebral fractures [ 18 ]  . 
 [ 19 ] compared the reproducibility of the semiquantitative genant evaluation and a number of quantitative methods and demonstrated that the semiquantitative method had higher intraand interobserver concordance . in our study , only 11% ( 2 / 18 ) of fractures was documented in the radiology reports ( table 3 )  . 
this finding is clearly noteworthy and confirms the known tendency of radiologists not to document in their official reports chronic incidental findings unrelated to the diagnostic query [ 4 , 5 , 1416 , 20 ]  . 
although our patient series was numerically too small to allow for any conclusive interpretation of this finding ( a limitation shared by other similar studies ) , we believe the series to be nonetheless adequately representative of the general population . 
in addition , the finding is especially important if we consider that it relates to subjects with no risk factors for osteoporosis ( steroid therapy , chronic renal failure ) other than age > 50 years , or clinical manifestations ( patients with a known history of osteoporosis and / or vertebral fractures were excluded )  . another limitation to our study could be that we considered moderate to severe fractures only ( clinically relevant fractures ) , as these allow for higher diagnostic accuracy and reproducibility with the semiquantitative method used . 
this may have led us to underestimate the actual prevalence of osteoporotic vertebral fractures in our study population . moreover , it is important to remember that even mild asymptomatic fractures , though more difficult to identify , increase the risk of fractures in these patients . in agreement with previous reports , our experience suggests that lateral chest radiographs , while not the reference standard for studying spinal osteoporosis , may be adequate for identifying vertebral fragility fractures . 
lateral chest radiographs performed for other indications provide a valuable and effective opportunity [ 5 ] to search for signs of unknown osteoporosis and establish an early diagnosis of asymptomatic vertebral compression fractures in at - risk populations . 
to increase the number of early diagnoses based on chest radiography , however , we need to address the problem of underreporting , by sensitising radiologists to the importance of documenting vertebral fractures independently of the main clinical indication for the examination [ 5 , 20 ]  . dividuate era stata riportata nei referti ufficiali ( tabella 3 )  . per ovvie ragioni , questo ci sembra un dato di estremo interesse che conferma , nella nostra esperienza , un fenomeno gi sottolineato da altri autori , riguardo la tendenza dei radiologi a non menzionare nei referti ufficiali rilievi legati a patologie , specie croniche , non strettamente correlati con il quesito diagnostico dellesame [ 4 , 5 , 1416 , 20 ]  . 
anche nel nostro caso , come daltra parte negli studi precedenti , il dato stato ottenuto su un campione di studio non sufficientemente ampio per trarre risultati conclusivi , ma , nonostante questo , riteniamo adeguatamente rappresentativo della popolazione generale . 
a nostro parere , inoltre , il risultato osservato assume particolare rilevanza se si tiene conto che esso si riferisce ad una popolazione di soggetti senza fattori di rischio aggiuntivi per osteoporosi ( terapie steroidee , irc ) , eccezione fatta per let superiore a 50 anni , e senza manifestazioni cliniche ( esclusione dei pazienti con storia gi nota di osteoporosi e / o fratture vertebrali )  . un altro limite del nostro studio potrebbe essere legato al fatto che abbiamo preso in considerazione solo le fratture moderate e severe ( fratture clinicamente rilevanti ) perch sono quelle valutabili con maggior accuratezza diagnostica e riproducibilit con il metodo visivo semiquantitativo da noi applicato . 
inoltre non bisogna dimenticare che anche fratture lievi ed asintomatiche , sebbene pi difficili da identificare , comportano un aumento del rischio di frattura in questi pazienti . in accordo con gli autori degli studi presenti in letteratura la nostra esperienza ci suggerisce che il radiogramma laterale del torace , sebbene non sia lesame di riferimento per lo studio dellosteoporosi nel rachide , pu ugualmente essere adeguato per la identificazione di deformit vertebrali da fragilit . 
possiamo pertanto affermare che , in unottica di diagnosi precoce delle deformit vertebrali da compressione ancora asintomatiche nella popolazione a rischio , la ricerca dei segni di patologia osteoporotica non nota nei radiogrammi laterali del torace eseguiti per qualsiasi indicazione clinica diversa rappresenta una opportunit estremamente efficace , utile e vantaggiosa [ 5 ]  . 
zompatori1 1dipartimento di scienze cliniche , sezione di scienze radiologiche , 2dipartimento di scienze chirurgiche , sezione di chirurgia toracica , 3dipartimento pneumologico , sezione di pneumologia ed endoscopia toracica , 4dipartimento di medicina 2 , sezione di oncologia medica , universit degli studi di parma , parma , italy correspondence to : m . 
de filippo , scienze radiologiche , azienda ospedaliero - universitaria di parma , via gramsci 14 , padiglione barbieri , 43100 parma , italy , tel . : + 39 - 052 - 1703660 , e - mail : massimo.defilippo@unipr.it received : 4 february 2008 / accepted : 25 february 2008 / published online : 25 september 2008 springer - verlag 2008 abstract purpose . 
mdct - guided transthoracic needle biopsy ( tnb ) was performed on 84 patients ( 55 men and 29 women ; mean age 65 years ) with suspected lung neoplasm by using a spiral mdct scanner with the simultaneous acquisition of six slices per rotation . 
eseguita agobiopsia transtoracica ( tnb , transthoracic needle biopsy ) tcmd - guidata in 84 pazienti ( 55 maschi e 29 femmine , et media 65 anni ) con lesione polmonare sospetta per neoplasia . 
sulla base di immagini assiali native ed mpr sagittali o coronali stato introdotto un ago chiba point centimetrato da 22 gauge ( g ) scegliendo : il tragitto pi breve in cui non si sovrappongano grossi vasi , bronchi principali e lobari , scissure pleuriche e strutture scheletriche ; ingresso nel parenchima polmonare il pi perpendicolare possibile al piano pleurico ; le zone di tessuto non calcifico pi dense della lesione da sottoporre a biopsia . 
in addition , because the various histological types of neoplasms respond differently to chemotherapy , the correct chemotherapeutic agent needs to be selected for the individual patient . cytohistological characterisation is also required in patients with a history of apparently remitting neoplasm , those with concurrent neoplasms or those with residual lesions after chemoor radiotherapy [ 3 ]  . 
the techniques used to guide pulmonary fnab are fluoroscopy , bronchoscopy and multidetector - row spiral computed tomography ( mdct )  . fluoroscopy - guided transthoracic needle biopsy ( tnb ) is a rapid and inexpensive technique that allows real - time monitoring of the procedure . 
 where mdct is not present , fluoroscopy - guided tnb remains a valuable option , especially for peripheral lesions located in areas of the lung affected by respiratory motion . transbronchial biopsy , with or without fluoroscopic guidance , is a commonly used technique that is often an integral step in the workup of lesions amenable to diagnosis by flexible bronchoscopy . mdct allows direct visualisation of small , low - density lesions and of lesions located in areas that cannot be seen with fluoroscopy . 
this makes mdct - guided tnb an excellagoaspirato polmonare con prelievo citologico ( fnab , fine needle aspiration biopsy ) , eseguito con approccio percutaneo transtoracico una procedura minimamente invasiva , di provata sicurezza , efficacia e tollerabilit , impiegata nella diagnostica delle lesioni polmonari , del mediastino e della parete toracica [ 1 , 2 ]  . 
 inoltre necessaria la caratterizzazione citoistologica per i pazienti con storia di neoplasia in apparente remissione clinica , con presenza di neoplasie concomitanti o con lesione residua post chemio - radioterapia [ 3 ]  . le tecniche che permettono la guida di una agobiopsia polmonare sono la fluoroscopia , la broncoscopia e la tc spirale multidetettore ( tcmd )  . la biopsia transtoracica ( tnb , transthoracic needle biopsy ) in fluoroscopia una tecnica di rapida esecuzione , con bassi costi e che consente la visualizzazione della manovra in tempo reale . 
nonostante questi vantaggi una metodica gradualmente in disuso per : la bassa risoluzione spaziale della metodica ; lesposizione delloperatore alle radiazioni ionizzanti ; la grande diffusione sul territorio della tcmd . 
 resta comunque valida ( qualora non fosse disponibile una tcmd ) , soprattutto per le lesioni periferiche e situate in aree del polmone particolarmente sensibili agli atti respiratori . la biopsia transbronchiale , con e senza guida fluoroscopica , una metodica largamente diffusa ; rappresenta molto spesso un passaggio obbligato nelliter diagnostico delle lesioni polmonari che possono essere avvicinate con il broncoscopio flessibile . 
all patients gave written informed consent after receiving verbal and written information about the benefits and risks of the procedure . patients were placed on the mdct table in the supine , prone or lateral position depending on lesion site and distance from the chest wall . 
la sensibilit di tale metodica del 90%95% per lesioni neoplastiche maligne con diametro superiore a 11 , 5 cm e scende al 70%75% per lesioni di diametro inferiore ; la tnb tcmdguidata pertanto uneccellente tecnica diagnostica [ 4 , 5 ]  . lintroduzione della tcmd inoltre ha permesso di ottenere ricostruzioni di immagini multiplanari ( mpr , multiplanar reformations ) di apprezzabile qualit , a nostro avviso , particolarmente vantaggiose nella guida dellagobiopsia percutanea polmonare . 
i pazienti sono stati studiati con scanner tcmd ( somatom emotion 6 , siemens , erlangen , germania ) a scansione elicoidale , con acquisizione simultanea di sei strati per ogni rotazione completa . 
i parametri tecnici utilizzati sono stati i seguenti : 90 mas , 130 kv , 10 , 26 mgv , collimazione 62 mm , slice 2 , 5 mm e record increment di 1 mil post - processing delle immagini stato ottenuto con workstation leonardo ( workstation leonardo , siemens )  . 
la tnb stata eseguita in regime di ricovero ordinario o di day hospital , dopo avere ottenuto il consenso firmato dal paziente , previa informazione verbale e scritta sui vantaggi e le possibili complicanze correlate alla procedura . i pazienti vengono posizionati sul lettino della tcmd in decubito supino , prono o laterale a seconda della sede del nodulo da sottoporre ad agobiopsia e della sua distanza dalla parete toracica . 
sulla base di immagini assiali native ed mpr sagittali o coronali , previa disinfezione della cute , si introduce un ago chiba point centimetrato da 22 g , scegliendo : 948 radiol med ( 2008 ) 113 : 945953 fig . 
1 double ( craniocaudal and mediolateral ) inclination of the needle ( n ) necessary to sample the lesion ( l ) while avoiding the superimposition of ribs , fissures and large vessels . 
1 dimostrazione schematica di una doppia inclinazione ( cranio - caudale e latero - mediale ) dellago , indicato con n , utile per centrare la lesione ( l ) da sottoporre a biopsia , evitando coste , scissure e grossi vasi sovrapposti . 
of 73 nodules , 18 were covered by ribs and two by pleural fissures ; in these cases , mpr images proved essential for needle guidance . two nodules were located in the hilar - mediastinal region : one on the right side and the other on the left . definitive cytological diagnosis revealed malignancy in 70 cases : non - small - cell carcinoma ( 19 ) ; adenocarcinoma ( 24 ) ; bronchioloalveolar carcinoma ( 2 ) ; epidermoid carcinoma ( 10 ) ; small cell carcinoma ( 1 ) ; metastasis ( 10 ) ; lymphoma ( 1 ) ; sarcomatoid mesothelioma ( 1 ) ; carcinoid ( 1 ) ; lymphomatoid granulomatosis ( 1 )  . 
four cytological samples were inadequate . minor complications included 11 cases of small pneumothorax ( < 2 - cm thick ) that resolved spontaneously , one case of extensive pneumothorax requiring chest tube drainage and three cases of perilesional bleeding . 
there were no major complications . il tragitto pi breve in cui non si sovrappongono grossi vasi , bronchi principali e lobari , scissure pleuriche e strutture scheletriche ; ingresso nel parenchima polmonare il pi perpendicolare possibile al piano pleurico ; le zone di tessuto non calcifico pi dense . 
le lesioni sottoposte ad agobiopsia avevano caratteristiche del nodulo solido non calcifico di dimensioni inferiori ai 2 cm , in 73 pazienti ; 11 lesioni erano in forma di massa ( dimensioni comprese tra i 2 e 16 cm )  . 
due noduli erano localizzati radiol med ( 2008 ) 113 : 945953 discussion since haaga and aifridi described the first ct - guided lung biopsy in 1976 [ 6 ] , the technique has become increasingly popular . 
needle - track seeding following fnab is very infrequent [ 8 ] , as are the following major complications of percutaneous transthoracic needle biopsies : gas embolism ( cerebral 0.07% ) from bronchovascular fistula or pulmonary artery puncture neoplastic seeding ( very rare ) vagal reaction infectious complications cardiac tamponade lung torsion mortality is very low ( 0.08%0.1% ) and may be caused by air embolism , untreated hypertensive pneumothorax , massive haemorrhage or myocardial infarction . 
the most common minor complications of transthoracic biopsy are pneumothorax ( 10%15% , only 5%10% requiring chest drainage ) , perilesional bleeding ( up to 10% ) , mild haemoptysis ( 10% ) and , rarely , haemothorax . 
 risk factors in pneumothorax : lesion size lesion depth emphysema approach angle < 90 multiple transpleural passes needle size procedure time perilesional bleeding is frequent but it is rarely a cause of haemoptysis and only when the bleeding is profuse . although pneumothorax is a minor complication , it should be noted that even a small pneumothorax can constitute a major complication in patients with impaired respiratory function . 
the risk of developing pneumothorax is related to the number of needle passes through the pleural surfaces ( the greater the number of passes , the higher the risk ) , length of the needle path and patients respiratory function [ the incidence of pneumothorax in patients with a forced expiratory volume in 1 s ( fev1 ) > 70% is significantly lower than in those with fev1 < 70% ] [ 9 ]  . 
although fine - needle aspiration of lesions with extensive pleural contact is unlikely to cause pneumothorax , the risk increases in the case of small subpleural lesions [ 11 ]  . 
for such lesions , some investigators have advocated adopting an oblique approach tangential to the pleura rather than a direct approach , even if the in sede ilo - mediastinica , rispettivamente uno a destra , laltro a sinistra . 
 lanalisi citologica definitiva del campione ha portato a diagnosi di malignit in 70 casi , ponendo la diagnosi di : carcinoma non a piccole cellule ( 19 casi ) ; adenocarcinoma ( 24 casi ) ; carcinoma bronchiolo - alveolare ( 2 casi ) ; carcinoma epidermoide ( 10 casi ) ; carcinoma a piccole cellule ( 1 caso ) ; metastasi ( 10 casi ) ; linfoma ( 1 caso ) ; mesotelioma sarcomatoide ( 1 caso ) ; carcinoide ( 1 caso ) ; granulomatosi linfomatoide ( 1 caso )  . 
in 10 casi emersa la natura benigna della lesione , tra cui un nodulo granulomatoso da sarcoidosi , un nodulo di natura tubercolare , ed altre lesioni di natura flogistica acuta alcune con caratteri purulenti . quattro prelievi sono risultati inadeguati . le complicanze minori sono state : 11 pazienti con piccole falde di pneumotorace ( pnx ) ( < 2 cm di spessore ) risoltesi spontaneamente ; 1 paziente con pnx di maggiore entit che ha richiesto il posizionamento di tubo di drenaggio ; 3 pazienti con soffusione emorragica perilesionale . 
non si verificata nessuna complicanza maggiore . discussione dal 1976 , data in cui haaga e aifridi [ 6 ] descrissero la prima biopsia polmonare tc guidata , vi stato un crescente e diffuso utilizzo di tale metodica . 
molto rare sono le complicanze maggiori delle biopsie percutanee transtoraciche con ago sottile : embolia gassosa ( cerebrale 0 , 07% ) per fistola broncovenosa o puntura di arteria polmonare ; seeding neoplastico ( estremamente raro ) ; reazione vagale ; complicanze infettive ; tamponamento cardiaco ; torsione polmonare . la mortalit legata alla metodica molto bassa ( 0 , 08%0 , 1% ) e pu essere causata da : embolia gassosa , pneumotorace iperteso non trattato , emorragia massiva , infarto del miocardio . 
 ( 10%15% , solo nel 5%10% necessita di drenaggio toracico ) , emorragia parenchimale perilesionale ( fino al 10% ) , emoftoe ( 10% ) , emotorace ( raro )  . fattori di rischio : dimensione della lesione ; profondit della lesione ; presenza di enfisema ; 950 radiol med ( 2008 ) 113 : 945953 needle path becomes exceptionally long [ 5 , 11 ]  . 
mpr needle guidance allowed us to avoid crossing pleural fissures and to select a plane parallel to the needle path , which may account for the low rate of pneumothorax in our study . 
 by using mpr , we were able to appreciate the several advantages of mdct over fluoroscopic guidance and transangolo di ingresso < 90 ; passaggi transpleurici multipli ; dimensione dellago ; durata della procedura ; lemorragia perilesionale molto frequente ma solo raramente e solo quando di dimensioni considerevoli , responsabile di emoftoe . 
il rischio di sviluppare pnx in relazione al numero di passaggi dellago attraverso i foglietti pleurici ( maggiore il numero di passaggi , maggiore il rischio di pnx ) , alla lunghezza di penetrazione dellago e alla funzionalit respiratoria : la percentuale di pnx in pazienti con volume espiratorio forzato al 1 ( fev1 ) secondo maggiore del 70% significativamente minore rispetto ai pazienti con fev1 minore del 70% [ 9 ]  . 
il rischio di sviluppare pnx inoltre aumentato dal calibro dellago ( luso di aghi di piccolo calibro diminuisce il rischio di pnx ) , dallangolo di penetrazione , dal tempo di permanenza dellago allinterno del parenchima . 
a the four axial multidetector computed tomography ( mdct ) sections show a 20 - mm solid noncalcified pulmonary lesion totally covered by a rib ( arrows ) in the dorsal segment of the right lower lobe . 
b the axial ( left quadrant ) and right parasagittal ( right quadrant ) multiplanar reconstruction ( mpr ) images show the caudocranial and lateromedial spatial orientation of the needle ( double inclination )  . 
a le 4 sezioni assiali tcmd documentano una lesione polmonare solida non calcifica di 20 mm ( frecce ) , completamente coperta da una costa , situata nel segmento dorsale del lobo polmonare inferiore destro . 
b le immagine mpr in sezione para - sagittale destra ( quadrante di destra ) ed assiale ( quadrante di sinistra ) dimostrano lorientamento spaziale dellago in senso caudo - craniale e latero - mediale ( doppia inclinazione )  . 
si noti come nellimmagine mpr si individui un adeguato approccio intercostale e si documenti la punta dellago allinterno del nodulo ( frecce )  . radiol med ( 2008 ) 113 : 945953 fig . 
a a 25 - mm solid noncalcified pulmonary lesion can be seen in the dorsal segment of the right lower lobe ; the arrow shows the needle tip inside the lesion . 
a lesione polmonare solida non calcifica di 25 mm , nel segmento dorsale del lobo polmonare inferiore destro ; la freccia indica la punta dellago allinterno della lesione ( freccia )  . 
fluoroscopy is limited by high radiation exposure for the operator , the inability to reach small hilar - mediastinal lesions that cannot be distinguished from vascular structures and all those lesions with insufficient density for fluoroscopic visualisation . 
transbronchial biopsy is almost exclusively indicated for nonperipheral lesions having some relationship with the feeding bronchus and thus enabling correct access with the bronchoscope . even slight bronchial angulations , displacements or subocclusions are enough to hinder passage of the bronchoscope and make it impossible to access the lesion with the forceps or needle [ 12 ]  . 
a sagittal multiplanar reconstruction ( mpr ) image ( left quadrant ) shows a 20 - mm solid noncalcified pulmonary lesion in the dorsal segment of right lower lobe adhering to the infracostal visceral pleura ( arrow )  . 
b left parasagittal mpr image shows the appropriate intercostal approach and the caudocranial inclination of the needle , the needle tip ( arrow ) and the rib covering the lesion ( arrowhead )  . 
a limmagine sagittale mpr nel quadrante a sinistra documenta una lesione polmonare solida non calcifica di 20 mm , nel segmento dorsale del lobo polmonare inferiore sinistro , adesa alla pleura viscerale sottocostale ( freccia )  . 
b limmagine mpr in sezione para - sagittale sinistra documenta ladeguato approccio intercostale , linclinazione dellago in senso caudo - craniale , la punta dellago ( freccia ) e la costa che copre la lesione ( testa di freccia )  . 
si noti come il nodulo , una volta ancorato dallago , non riesca a risalire ed a ricollocarsi completamente dietro la costa . causa di pnx sono anche i passaggi attraverso scissure pleuriche o bolle di enfisema subpleuriche [ 10 ]  . 
lagoaspirato di una lesione con ampia base dappoggio pleurico ha una bassa probabilit di causare pnx ; maggiore il rischio di pnx se la lesione , pur in sede subpleurica , di piccolo calibro [ 11 ]  . 
in questultimo caso alcuni autori consigliano un approccio obliquo , tangenziale alla pleura , anche se il percorso dellago diviene particolarmente lungo , rispetto allapproccio diretto con tragitto pi breve [ 5 , 11 ]  . using mpr images during mdct - guided lung biopsies improves overall diagnostic accuracy in pulmonary lesions nel nostro studio non abbiamo osservato , rispetto ai dati correnti nella letteratura , un incremento delle complicanze 952 fig . 
5a - c a 82 - year - old female nonsmoker who had undergone left upper lobectomy for non - small - cell lung cancer 4 years earlier , with recurrence at the ipsilateral hilua left parasagittal multiplanar reconstruction ( mpr ) image shows the needle path in left pulmonary parahilar location where there are no overlying ribs or large vessels . 
5a - c paziente femmina non fumatrice di 82 anni , operata 4 anni prima di lobectomia superiore sinistra per neoplasia polmonare non a piccole cellule , con recidiva di malattia allilo polmonare omolaterale . 
la guida dellago con immagini mpr ha permesso di evitare la penetrazione nelle scissure pleuriche e di scegliere un piano ortogonale alla penetrazione dellago ; ci potrebbe spiegare la bassa percentuale di pnx registrata nel nostro studio . 
il miglioramento dellaccuratezza diagnostica dellmpr si osservato non solo in questultime lesioni ma anche nei noduli polmonari solitari di diametro inferiore ai 20 mm , la cui guida era agevole gi con le immagini assiali tcmd ; una loro visualizzazione multiplanare stata infatti ugualmente utile per individuare la sede pi opportuna del prelievo . il ricorso a ricostruzioni mpr ha permesso di rimarcare i vantaggi della tcmd rispetto alla guida fluoroscopica ed alla biopsia transbronchiale . 
lutilizzo del fluoroscopio gravato da un alta esposizione a radiazioni ionizzanti per loperatore , allincapacit di raggiungere le piccole lesioni ilo - mediastiniche , in quanto indistinguibili dalle strutture vascolari , nonch tutte quelle lesioni di densit insufficiente per una visualizzazione fluoroscopica . 
la biopsia transbronchiale ha indicazione quasi esclusiva per lesioni non periferiche e che presentino un rapporto con il bronco tributario tale da consentire al broncoscopio il giusto approccio per il prelievo . 
sono sufficienti infatti anche piccole angolazioni nelle vie aeree , dislocazioni o subocclusioni , che il passaggio del broncoscopio ne viene largamente limitato al punto da rendere impossibile lestensione della pinza tranciante o dellago e quindi il campionamento della lesione [ 12 ]  . 
non va dimenticato inoltre quanto questa manovra sia mal tollerata dai pazienti [ 13 ]  . limpiego di ricostruzioni mpr ottenute con tcmd , riteniamo permetta di evitare linstallazione di hardware di guida fluoroscopica negli scanner tcmd , ancora particolarmente costosi e che esporrebbero a radiazioni ionizzanti loperatore ed oltremisura il paziente . conclusioni limpiego di ricostruzioni mpr durante biopsie polmonari tcmd guidate , migliora laccuratezza diagnostica delle lesioni polmonari , in quanto permette : una corretta pianificazione della traiettoria dellago ; una precisa documentazione della posizione della punta dellago nel contesto della lesione ; una migliore identificazione di aree necrotiche da radiol med ( 2008 ) 113 : 945953 in that it allows optimal planning of the needle path , precise depiction of the needle tip inside the lesion and better visualisation of necrotic areas to be avoided due to the risk of false negative results . 
furthermore , our experience suggests that in percutaneous mdct - guided fine - needle biopsy , mpr images are especially useful for sampling biological tissue in lesions that are difficult to access with axial images alone owing to overlying bony structures ( ribs , sternum , scapulae ) or critical location ( pulmonary hilum , proximity to the heart or large mediastinal vessels )  . 
la nostra esperienza suggerisce che il ricorso alla tecnica mpr nellagobiopsia percutanea tcmd guidata particolarmente utile nel prelievo di materiale biologico di lesioni difficilmente raggiungibili con la sola osservazione delle immagini tcmd assiali , in quanto coperte da strutture scheletriche ( coste , sterno e scapole ) o situate in zone critiche ( ilo polmonare , in corrispondenza del cuore o dei grossi vasi mediastinici )  . 
barbiero , via fogarine 59 , 30030 foss ( ve ) , tel . : + 39 - 0424 - 888645 , fax : + 39 - 0424 - 888791 , e - mail : giuliobarbiero@katamail.com received : 27 october 2007 / accepted : 14 january 2008 / published online : 13 september 2008 springer - verlag 2008 abstract purpose . 
ninety - five patients ( m / f = 92 / 3 ; mean age at time of operation 70.77.8 years ) who underwent endovascular repair of infrarenal aaa between april 1997 and october 2004 were considered . 
a total of 37 el occurred in 33 / 95 patients ( 34.7% ) , four of whom had two el of different types . eighteen el were treated , 16 by endoluminal treatment . six el were type i : 2 were treated by percutaneous transluminal angioplasty ( pta ) and 4 by cuff deployment ( 2 proximal cuffs and 2 distal cuffs )  . 
eight el were type ii : 2 were treated by pta , 2 by cuff deployment , 1 by transcatheter coil embolisation of the inferior mesenteric artery , two by thrombin injection in the aneurysm sac and one underwent surgical conversion during an attempt to treat a concomitant type i el . 
sono stati considerati retrospettivamente 95 pazienti consecutivi ( m / f = 92 / 3 ; et media al momento dellimpianto 70 , 77 , 8 anni ) sottoposti nel periodo aprile 1997ottobre 2004 ad impianto di ep per esclusione di aaa infrarenale . 
otto el erano di tipo ii : 2 sono stati trattati con pta , 2 con il posizionamento di una cuffia iliaca , 1 con embolizzazione transcatetere dellarteria mesenterica inferiore , 2 con iniezione di trombina allinterno della sacca aneurismatica e in un caso , associato anche ad el di tipo i , nel tentativo di trattamento di questultimo , si ricorsi a conversione chirurgica . 
il tasso di successo tecnico stato del 75% ( 12 / 16 el ) , essendovi stata necessit di conversione chirurgica in 3 / 16 casi ( 18 , 8% ) ed essendo un paziente deceduto il giorno successivo al trattamento 1030 radiol med ( 2008 ) 113 : 10291042 enlargement . 
sono sempre candidati al trattamento gli el graft - correlati ( tipi i e iii ) , mentre gli el di tipo ii ( e tipo v ) devono essere trattati solo se associati a crescita dimensionale dellaaa . gli el di tipo iv solitamente si risolvono con regressione spontanea . 
il trattamento endovascolare possibile secondo diverse modalit in base alleziologia dellel , ma non sempre risolutivo e talvolta necessario ricorrere alla conversione chirurgica . parole chiave aneurima aortico addominale trattamento endovascolare endoleak endoprotesi introduction introduzione endoleak ( el ) is one of the most common complications [ 15 ] after exclusion of an abdominal aorta aneurysm ( aaa ) by endografting . 
it has been defined [ 6 ] as the persistence of blood flow around the endograft within the aneurysmal sac , which may lead to sac expansion and eventually rupture [ 710 ]  . 
 lendoleak ( el ) rappresenta una delle complicanze pi frequenti [ 15 ] dopo intervento di esclusione di un aneurisma dellaorta addominale ( aaa ) dal torrente circolatorio mediante endoprotesi ( ep ) , ed stato definito [ 6 ] come la persistenza di flusso sanguigno periprotesico allinterno della sacca aneurismatica , che pu determinare ingrandimento della sacca stessa , fino alla sua rottura [ 710 ]  . 
secondo la classificazione eziologica di white et al . ( tabella 1 ) [ 2 , 6 , 1113 ] gli el possono essere causati da incompleta adesione alle pareti vasali di uno degli estremi dellep ( tipo i : a = prossimale , b = distale ) ; da rifornimento retrogrado della sacca aneurismatica ( tipo ii ) ad opera di rami collaterali ( arteria mesenterica inferiore , arterie lombari , arterie ipogastriche , arterie renali accessorie , arterie gonadiche ) ; da disconnessione o rottura degli elementi protesici ( tipo iii ) ; da porosit del tessuto protesico ( tipo iv ) ; infine da pressurizzazione persistente della sacca aneurismatica senza tuttavia dimostrazione di flusso sanguigno periprotesico con le comuni metodiche di imaging ( tipo v o endotension ) [ 12 , 1416 ]  . scopo di questo lavoro rivalutare , in base alla nostra esperienza , le indicazioni e le opzioni terapeutiche per il trattamento degli el successivi al trattamento endovascolare degli aaa . materiali e metodi sono stati considerati retrospettivamente 95 pazienti ( m / f = 92 / 3 ; et media al momento dellimpianto di 70 , 77 , 8 anni , range 49 , 989 , 6 anni ) sottoposti a posizionamento di ep per via transfemorale per aaa infrarenale nel periodo aprile 1997ottobre 2004 . 
ct angiography was performed with a conventional scanner ( tomoscan lx , philips , eindhoven , nl ) from 1997 to 2000 and , from 2000 onwards , with a spiral scanner ( somatom emotion , siemens , erlangen , germany )  . 
the spiral ct protocol consisted of an initial unenhanced scan with acquisition volume encompassing the endograft ( collimation thickness 8 mm , table feed 16 mm , reconstruction thickness 7 mm )  . 
 sono state impiegate 94 ep aorto - bisiliache ( 39 talent , medtronic , santa rosa , ca , usa ; 24 excluder , gore , flagstaff , az , usa ; 22 aneurx , medtronic , santa rosa , ca , usa ; 4 vanguard , boston scientific , natick , ma , usa ; 3 anaconda , sulzer vascutek ltd , scozia ; 2 endologix , bard , murray hill , nj , usa ) e 1 ep retta aorto - aortica ( passager , boston scientific , natick , ma , usa )  . il follow - up dei pazienti trattati prevedeva un esame ecocolor - doppler ( sonda da 3 , 5 mhz ) alla dimissione o lesecuzione di un angio - tc in 7a giornata , seguito da controlli periodici mediante angio - tc a 1 , 3 , 6 , 12 mesi e quindi annualmente . 
lo studio angio - tc stato eseguito dal 1997 al 2000 mediante tc tradizionale ( tomoscan lx , philips , eindhoven , nl ) e , a partire dal 2000 , con tc spirale ( somatom emotion , siemens , erlangen , germania )  . 
injection of 120150 ml nonionic contrast medium ( omnipaque 350 , nycomed , oslo , norway ) at a flow rate of 34 ml / s via an automated power injector . 
to this end , a 5 - f pigtail or straight catheter was placed with its distal end above the origin of the renal arteries , and 30 ml of nonionic contrast material ( omnipaque 350 , nycomed ) was administered at a flow rate of 15 ml / s via an automatic power injector . 
infine veniva eseguita una terza acquisizione in fase tardiva ( a 90 secondi dallinizio delliniezione di mdc ) con gli stessi parametri della fase arteriosa ma con volume di acquisizione comprendente la protesi . 
le immagini assiali acquisite in fase arteriosa venivano poi elaborate su postazione di elaborazione ( work station , magic view 1000 , siemens , erlangen , germania ) per lottenimento di ricostruzioni multiplanari ( mpr ) e tridimensionali ( mip , ssd e vrt )  . 
there were 24 primary el ( occurring within 30 days ) and 13 secondary el ( occurring after 30 days )  . diametro medio dellaaa 48 , 86 , 4 mm ( range ( range 570 mm ) ; 3280 mm ) ; lunghezza media dellaaa 72 , 610 , 6 mm ( range 30130 mm )  . la durata media del follow - up stata di 34 , 558 , 7 mesi ( range 189 mesi )  . 
three were proximal : two were treated by placement of an aortic cuff , of which one was deployed successfully in the postoperative period , and the other , deployed at 23 months , became displaced requiring surgical conversion ; the third case , which arose at 60 months , underwent immediate surgical conversion owing to doubts about the efficacy of endovascular treatment . 
among the primary el , ten resolved spontaneously 3 days to 7 months after the procedure , two remained unchanged during follow - up ( at 1 and 24 months , respectively ) , and 1 , slightly increased , el was not treated , as it was associated with aaa shrinkage . finally , three el supplied by the hypogastric artery were treated by placing an iliac extension ( one case , with success ) and by pta of the iliac limb of the graft ( two cases , one successfully and 1 with surgical conversion due to rupture of the common iliac artery the following day )  . among the ten secondary el , one case ( occurring at 7 months ) resolved spontaneously , and four cases remained si sono verificati 7 el di tipo i in 7 pazienti ( 5 primari e 2 secondari )  . 
gli el prossimali erano 3 : due el trattati mediante posizionamento di una cuffia aortica , rispettivamente uno nel post - impianto con successo e laltro a 23 mesi con dislocazione della cuffia e conseguente conversione chirurgica ; il 3 caso , comparso a 60 mesi dallimpianto , stato subito sottoposto a conversione laparotomica per i dubbi sullefficacia di un eventuale trattamento endoluminale . 
gli el distali erano 4 ( tutti primari ) : 2 el trattati immediatamente con pta con successo e 2 con posizionamento di una cuffia iliaca , di cui 1 caso con successo , mentre laltro con aumento dellel e decesso del paziente per rottura dellaaa a 18 mesi . 
fra gli el primari , 10 el sono andati incontro a risoluzione spontanea in un intervallo di tempo compreso fra 3 giorni e 7 mesi , 2 el sono rimasti sostanzialmente invariati nei controlli successivi ( rispettivamente a 1 e 24 mesi di follow - up ) , 1 el in lieve aumento non stato trattato perch associato a riduzione dellaaa e infine 3 el da arteria ipogastrica sono stati trattati rispettivamente con pta della branca iliaca protesica ( 2 casi , di cui 1 con successo e 1 con conversione chirurgica per rottura dellarteria iliaca comune il giorno seguente ) , e con posizionamento di unestensione iliaca ( 1 caso con successo )  . 
two were primary and arose in the area of overlap between the body and iliac limb of the gra these were successfully treated by pta and placement of an iliac extension , respectively . 
in base allorigine degli el di tipo ii , 10 casi erano riconducibili a rifornimento retrogrado dellaaa attraverso larteria mesenterica inferiore , 7 casi attraverso arterie lombari , 6 casi attraverso arterie ipogastriche e 3 casi di tipo misto ( da lombari e mesenterica inferiore in un caso ; da lombari , mesenterica inferiore e ipogastriche in un altro ; da lombari e unarteria renale accessoria lultimo caso )  . 
da notare che in 3 casi di el di tipo ii da arteria mesenterica inferiore risoltisi spontaneamente , vi era persistente perviet dellarteria rispettivamente a 1 , 11 e 12 mesi dalla chiusura spontanea dellel . 
attualmente sono in osservazione 9 casi di el di tipo ii , dei quali 3 associati a lieve aumento delle dimensioni della sacca aneurismatica : 2 el sono stati gi trattati rispettivamente mediante embolizzazione dellarteria mesenterica inferiore e iniezione di trombina intra - aneurismatica , mentre 1 caso di el ( di tipo misto ) non stato ancora trattato in quanto giudicato non fattibile il trattamento percutaneo con trombina n quello endovascolare , e tuttora sotto stretto follow - up . tipo iii tipo iv si sono osservati 3 el di tipo iii in altrettanti pazienti ( 3 , 2% ) , di cui 2 el primari nella zona di embricazione fra corpo principale e branca iliaca della protesi , trattati con successo rispettivamente con pta e con posizionamento di unestensione iliaca , mentre 1 caso di el secondario dovuto a rottura dello stent prossimale ( vanguard ) a 51 mesi dallimpianto stato sottoposto a conversione laparotomica . c stato un unico caso di verosimile el di tipo iv che scomparso spontaneamente al controllo tc in 12a giornata post - procedurale . complessivamente sono stati trattati 18 el : 2 con conversione laparotomica immediata e 16 per via endovascolare ; di questi ultimi , 3 casi sono esitati in conversione chirurgica e 1 caso esitato nel decesso del paziente per rottura dellaaa , per cui il tasso di successo tecnico nel trattamento endovascolare degli el stato del 75% ( 12 / 16 casi )  . radiol med ( 2008 ) 113 : 10291042 1037 a total of 18 el were treated : two with immediate surgical conversions and 16 with an endovascular procedure . 
if the el is caused by inadequate endograft seal ( type i ) , one may try to achieve a complete seal by balloon dilatation of the endograft ends or by adding proximal or distal cuffs . 
in the latter case , however , it should be borne in mind that cuffs carry a risk of displacement and failure due to incorrect sizing [ 23 ]  . 
un ulteriore possibile rischio delle cuffie , poi , quello di andare a ricoprire lorigine di rami arteriosi collaterali importanti ( arterie renali , arterie ipogastriche ) , con conseguente ischemia distale . 
nella nostra piccola esperienza risultato efficace , quando era fattibile , il trattamento degli el di tipo ib mediante pta delle estremit dellep ( 2 casi , 100% successo tecnico ) , mentre il posizionamento di cuffie aortiche o iliache non stato scevro di complicanze ( 4 cuffie , di cui 1 con conversione chirurgica e 1 con decesso del paziente per rottura dellaaa a 18 mesi )  . le opzioni terapeutiche per gli el di tipo ii sono molteplici [ 2432 ] : dilatazione dellep con cateteri a palloncino in corrispondenza del punto di rifornimento retrogrado della sacca aneurismatica ( rischio di rottura del vaso ) ; posizionamento di cuffie a cavaliere del vaso arterioso rifornente per assicurare un migliore contatto dellep alle pareti vasali ( rischio di dislocazione delle cuffie ) ; embolizzazione transcatetere con microspirali o altri agenti embolizzanti ( tipo spongostan ) del ramo arterioso che rifornisce la sacca aneurismatica ( attraverso larteria mesenterica superiore e larcata di riolano per el da arteria mesenterica inferiore , oppure attraverso larteria ipogastrica e lileo - lombare per el da arterie lombari ) , con i rischi connessi a tutte le procedure di embolizzazione ( impossibilit tecnica di cateterismo superselettivo anche con luso di microcateteri in caso di anatomie complesse , embolizzazione incompleta del ramo arterioso rifornente , migrazione distale dellagente embolizzante , ecc . ) ; iniezione diretta nella sacca aneurismatica , in genere per via translombare o , pi recentemente , anche per via transcavale inferiore , sotto guida tc , di trombina , o spirali , o colle ( rischi 1038 radiol med ( 2008 ) 113 : 10291042 etc . ) ; direct ct - guided injection of thrombin into the aneurysm sac , or coils , or glues , generally with a translumbar approach or , more recently , with an inferior transcaval approach ( risks related to the translumbar or transcaval puncture , and risks linked to the embolising agent )  . 
this blocks the persistent , usually massive , refilling of the aneurysmal sac , preventing its enlargement and thus sparing the patient a further procedure ( endovascular or surgical )  . 
nella nostra esperienza su 8 el di tipo ii associati ad aumento significativo ( > 5 mm ) del diametro dellaaa trattati per via endovascolare , ci sono stati 6 / 8 casi ( 75% ) di risultati favorevoli ( scomparsa o riduzione dellel ai controlli successivi ) , mentre in 2 / 8 casi ( 25% ) stata necessaria la conversione chirurgica , segno che il trattamento endovascolare degli el di tipo ii rimane tuttora non sempre risolutivo . per gli el di tipo iii , se sono causati da disgiunzione degli elementi protesici si pu tentare di ricostituire la continuit della protesi mediante pta con eventuale posizionamento di una cuffia intermedia di calibro adeguato ( rischio di dislocazione della cuffia o di persistenza dellel per errato dimensionamento ) , mentre per gli el causati da rottura degli elementi protesici non resta che ricorrere alla conversione chirurgica [ 23 ]  . 
nella nostra piccola esperienza , su 3 casi di el di tipo iii trattati per via endovascolare , 2 casi hanno avuto successo rispettivamente con pta e con posizionamento di una cuffia iliaca , mentre stato necessario ricorrere alla conversione chirurgica nel 3 caso , causato da rottura dello stent pi craniale , eventualit che non lasciava spazio ad alcuna procedura endovascolare . quanto agli el di tipo iv solitamente essi vanno incontro a risoluzione spontanea per chiusura ( trombizzazione ) dei piccoli pori presenti nel tessuto protesico , anche se negli ultimi anni tali el sono diventati assai meno frequenti per il miglioramento tecnico delle caratteristiche delle ep , come confermato dal fatto che nella nostra esperienza c stato un unico caso di verosimile el di tipo iv ( scomparso spontaneamente alla tc di controllo in 12a giornata po ) verificatosi allinizio della nostra casistica con un modello di ep ( talent ) che ha poi subito dei consistenti miglioramenti . quando trattare un endoleak la scelta di quando trattare un el deve essere ponderata . generalmente una volta posta indicazione al trattamento ( endovascolare o chirurgico ) di un el , questo deve essere eseguito nel pi breve tempo possibile e , nel caso in cui un el di tipo i o iii venga riconosciuto durante il posizionamento dellep ( insuccesso tecnico primario ) deve essere trattato nella stessa seduta dellimpianto [ 4 ]  . 
in questo modo si corregge la persistente perfusione , di solito imponente , della sacca aneurismatica , evitando che questa possa aumentare di volume nel tempo ed evitando di sottoporre il paziente ad unaltra seduta operatoria ( endovascolare o chirurgica )  . lunica eccezione data dagli el di tipo ii che , come gi detto sopra , vengono ritenuti da trattare solo qualora si associno a incremento significativo ( > 5 mm ) del diametro dellaaa , oppure secondo taluni autori se persiste per pi di 612 mesi [ 34 , 35 ] , valutabile soltanto nel follow - up . 
nella radiol med ( 2008 ) 113 : 10291042 1039 or , according to some authors , if it persists longer than 612 months [ 34 , 35 ] , as demonstrated during the follow - up . 
the ten cases ( 38.5% ) of spontaneous resolution observed in our study occurred 3 days to 7 months after el appearance and were all primary , developing within 30 days after endograft deployments . 
early appearance of an el in the postoperative period might thus nostra esperienza , su 26 casi di el di tipo ii sono stati trattati soltanto gli 8 el associati ad aumento significativo del diametro dellaaa , mentre i restanti 18 casi non sono stati trattati perch associati a risoluzione o riduzione spontanea dellel o a riduzione dimensionale spontanea dellaaa . invece i 7 casi di el di tipo i e i 3 casi di el di tipo iii sono stati tutti trattati , di cui 3 con conversione chirurgica . perch trattare un endoleak essendo definito come la persistenza di flusso sanguigno allinterno della sacca aneurismatica ma allesterno dellep [ 6 ] , lel pu portare a incremento volumetrico dellaaa fino alla sua possibile rottura [ 710 ]  . 
fra gli el che si associano a crescita dellaaa vi sono tutti gli el di tipo i e iii ( el graft - correlati ) , in quanto i difetti di adesione dellep alle pareti vasali o la disgiunzione / rottura degli elementi protesici sono tali che lentit di tali tipi di el sempre cospicua , determinando una trasmissione pressoch completa della pressione arteriosa sistolica alle pareti della sacca , per cui tali el devono essere trattati subito , nella stessa seduta dellimpianto se primari ( insuccesso tecnico primario ) [ 4 , 19 , 21 , 39 ]  . tipo i tipo ii gli el primari di tipo i si sono verificati nel 5 , 3% dei casi ( 5 / 95 ) ( 7 , 5% in letteratura ) , il 60% dei quali ( 3 / 5 ) scomparso dopo trattamento endovascolare . 
in altri 2 casi ( 40% ) , invece , si avuta persistenza dellel anche dopo trattamento endovascolare , di cui uno esitato in rottura dellaaa a 18 mesi dallimpianto dellep . 
si sono avuti soltanto 2 / 7 casi ( 28 , 6% ) di el secondari di tipo i , confermando la necessit di uno stretto follow - up dei pazienti trattati , specie nel 1 mese dopo il posizionamento dellep , poich i difetti di adesione delle estremit dello stent - graft alle pareti vasali sono precoci a comparire [ 2 , 10 ]  . gli el di tipo ii sono i pi frequenti ( 26 / 37 el , 70 , 3% ) e il loro significato clinico rimane tuttora controverso [ 7 , 34 , 35 , 40 , 41 ]  . 
infatti , a differenza degli el di tipo i e iii generalmente sempre associati ad un significativo aumento dimensionale dellaaa e , quindi , ad aumentato rischio di rottura , quelli di tipo ii possono associarsi a stabilit o , addirittura , a riduzione volumetrica dellaaa e possono evolvere anche nella risoluzione spontanea [ 34 , 41 ]  . 
i 10 casi ( 38 , 5% ) di risoluzione spontanea si sono verificati in un intervallo di tempo compreso fra 3 giorni e 7 mesi dalla comparsa dellel ed erano tutti el primari , ossia comparsi precocemente . 
pertanto un fattore predittivo per la trombosi spontanea dellel potrebbe essere la sua comparsa precoce nel post - impianto , e la chiusura spontanea di un 1040 radiol med ( 2008 ) 113 : 10291042 be a predictor of its spontaneous thrombosis , and spontaneous closure of an el is rare after 12 months , as reported in the literature [ 34 , 35 , 42 ]  . 
il trattamento degli el di tipo ii , invece , viene riservato solamente ai casi associati a significativa crescita dimensionale dellaaa , mantenendo un atteggiamento di vigile attesa negli altri casi [ 4 , 2325 , 35 ]  . 
si sono verificati , infatti , 20 casi ( 76 , 9% ) di stabilit e 2 casi ( 7 , 7% ) di riduzione significativa del diametro massimo dellaaa , pur in presenza di el di tipo ii , a conferma che lassociazione fra crescita dellaaa e presenza di el non sempre valida per gli el di tipo ii [ 8 , 34 , 40 , 41 , 43 ]  . type iii tipo iii there were three cases ( 11.5% ) of type iii el . 
of these , two were primary , at the junction between graft body and iliac limb , and one was secondary due to failure of the uppermost stent after 51 months . 
the latter required surgical conversion and occurred with an endograft model ( vanguard ) that has now been withdrawn from the market , a sign of the ongoing evolution of materials and designs . 
this may have been due either to persistence of the previous el but markedly reduced flow ( less than the sensitivity threshold of ct ) or to persistent pressurisation of the aneurysm sac ( endotension ) [ 12 , 1416 ]  . with regard to the relationship between el and type of endograft , the el observed occurred with all types of endografts used , so that the model of endograft does not appear to affect the possible appearance of an el [ 44 ]  . non c stato nessun caso dimostrabile di el di tipo v , ma un paziente portatore di un piccolo el di tipo ii da arteria ipogastrica , trattato con successo mediante posizionamento di unestensione iliaca omolaterale a 12 mesi dallimpianto , ha avuto comunque un lieve incremento del diametro dellaaa nei controlli tc successivi , spiegabile o con una persistenza dellel precedente ma con flusso assai ridotto ( inferiore alla soglia di sensibilit della tc ) , oppure con una pressurizzazione persistente della sacca aneurismatica ( endotension ) [ 12 , 1416 ]  . per quanto riguarda il rapporto degli el con il tipo di ep , gli el si sono verificati con tutti i tipi di ep utilizzate , per cui il tipo di ep impiantata non sembra condizionare leventuale comparsa di el [ 44 ]  . conclusions conclusioni el remains a relatively common complication following exclusion of an aaa by endografting . 
sono candidati al trattamento endovascolare gli el di tipo i e iii , e gli el di tipo ii ( e v ) associati a radiol med ( 2008 ) 113 : 10291042 1041 ciated with significant growth of the aaa . 
we reviewed the medical records of 72 patients with severely impaired liver function who underwent transjugular biopsy at our department . contraindications to percutaneous liver biopsy included thrombocytopenia , severe coagulopathy , marked ascites or a combination of the above . 
group 1 included 44 patients ( 58% ) with acute abnormalities of liver function , whereas groups 2 , 3 and 4 included patients with chronic abnormalities suspected to be due to infectious cirrhosis ( 12 patients , 16% ) , alcoholic cirrhosis ( seven patients , 9% ) and cirrhosis of unknown origin ( 13 patients , 17% ) , respectively . 
transjugular liver biopsy proved to be a safe procedure that provided important information for the clinical and therapeutic management of patients in whom treatment would have been either empirical or unfeasible . 
abbiamo revisionato le cartelle cliniche di 72 pazienti con severa alterazione della funzionalit epatica che sono stati sottoposti a biopsia transgiugulare presso il nostro dipartimento . i pazienti sono stati suddivisi in 4 gruppi , in base al sospetto clinico dellorigine della malattia epatica . 
la biopsia epatica per via transgiugulare permette di ottenere importanti dati relativi al trattamento clinico e terapeutico di pazienti nei quali la terapia sarebbe altrimenti empirica o non proponibile , con una bassa incidenza di complicanze . 
 radiol med ( 2008 ) 113 : 10081017 1009 keywords liver liver biopsy liver diseases cirrhosis parole chiave fegato biopsia epatica malattie del fegato cirrosi introduction introduction liver biopsy is considered to be very useful in diagnosing and treating patients with abnormal liver function tests [ 14 ]  . 
after 6 years of experience as interventional radiologists of the ospedale maggiore policlinico in milan , we decided to evaluate the impact of transjugular liver biopsy on the diagnostic and therapeutic management of patients with severe liver disease . 
to this end , we reviewed the medical records of all patients who underwent transjugular liver biopsy because of acute and chronic liver function abnormalities . la biopsia epatica considerata molto utile nella diagnosi e nella cura di pazienti con alterazioni della funzionalit epatica [ 14 ]  . 
il prelievo bioptico per via transgiugulare permette di ottenere campioni istologici in pazienti per i quali la puntura per via percutanea controindicata [ 5 , 6 ]  . dopo unesperienza di 6 anni dei radiologi interventisti dellospedale maggiore policlinico di milano , abbiamo voluto valutare limpatto di questa procedura nella valutazione diagnostica e nella gestione terapeutica di pazienti epatopatici gravi , con disfunzioni sia acute , sia croniche della funzionalit epatica . 
a questo scopo , abbiamo revisionato le cartelle cliniche di tutti i pazienti che si sono sottoposti alla procedura in questo periodo di tempo . materials and methods we reviewed the medical records of 72 patients who underwent transjugular liver biopsy at ospedale maggiore policlinico di milano , for a total of 76 procedures performed by a single team of radiologists . 
percutaneous biopsy was contraindicated because of severe thrombocytopenia ( defined as a platelet count < 50109 / l ) ( 44 ; 58% ) , severe coagulopathy [ international normalised ratio ( inr ) > 1.5 ] ( 3 ; 4% ) , marked ascites ( 3 ; 4% ) or a combination of the above ( 26 ; 34% ) [ 57 ]  . 
table 1 shows the clinical indications for transjugular liver biopsy in our series . coagulopathy and thrombocytopenia were the principal indications for the transjugular approach [ 35 ] and were encountered in combination or separately in 52 procedures ( 68% )  . 
in addition , because thrombocytopenia and / or coagulopathy were also considered the main indications in the 21 cases in which they were associated with ascites ( 28% ) , the two conditions accounted for 96% of all indications for transjugular biopsy . 
twenty - three of them , with a history of bone marrow transplant , had a clinical suspicion of graft - versus - host disease ( gvhd ) or of veno - occlusive disease ( vod ) ( subgroup a ) ; three , with previous liver transplantation , had a clinical suspicion of organ rejection ( subgroup b ) ; and for the remaining 18 patients , miscellaneous diagnostic hypotheses was formulated ( except for two subjects with a clinical suspicion of mycotic infection ) ( subgroup c )  . 
group 2 was made up of 12 patients with materiali e metodi sono state riesaminate le cartelle cliniche di 72 pazienti , che si sono sottoposti a biopsia del fegato per via transgiugulare presso lospedale maggiore policlinico di milano , per un totale di 76 procedure interventistiche , eseguite dallo stesso gruppo di medici radiologi . 
in tutti questi pazienti la biopsia per via percutanea era controindicata o per piastrinopenia grave ( nello studio stata considerata una conta piastrinica inferiore a 50109 / l ) ( 44 pazienti , 58% ) , o per difetti rilevanti dei fattori della coagulazione ( nella nostra casistica stato considerato controindicato per la biopsia percutanea un inr > 1 , 5 ) ( 3 pazienti , 4% ) o per la presenza di ascite massiva ( 3 pazienti , 4% ) o per unassociazione di tali condizioni ( 26 pazienti , 34% ) [ 57 ]  . 
la tabella 1 presenta le situazioni cliniche che hanno motivato lesecuzione di una biopsia epatica per via transgiugulare . le alterazioni dellemocoagulazione e la piastrinopenia hanno rappresentato le indicazioni maggiori allesecuzione della biopsia per via transgiugulare [ 35 ] ; le due situazioni cliniche erano presenti in associazione o singolarmente in 52 procedure ( 68% )  . 
bisogna aggiungere che nelle 21 procedure con epatopatia ascitogena associata a piastrinopenia e / o a coagulopatia ( 28% ) , queste ultime sono state considerate le maggiori controindicazioni per lesecuzione di una biopsia percutanea rappresentando quindi in totale il 96% delle indicazioni ; nella nostra casistica lascite , come indicazione principale , ha contribuito solamente in tre casi ( 4% ) allesecuzione di una biopsia per via transgiugulare . 
 abbiamo assegnato ogni paziente a una di 4 categorie cliniche ( gruppo 1 , 2 , 3 e 4 ) , individuate sulla base dei dati anamnestici e dei risultati degli esami di laboratorio . 
il 1010 radiol med ( 2008 ) 113 : 10081017 table 1 indications for transjugular liver biopsy in our series indications for transjugular liver biopsy isolated thrombocytopenia isolated coagulopathy isolated ascites combination of thrombocytopenia and coagulopathy combination of thrombocytopenia and ascites combination of coagulopathy and ascites combination thrombocytopenia , coagulopathy , and ascites 8 total procedures tabella 1 indicazioni per lesecuzione della biopsia epatica per via transgiugulare indicazioni per la biopsia epatica per via transgiugulare n procedure con piastrinopenia come unica condizione procedure con coagulopatia come unica condizione procedure con ascite come unica condizione procedure con piastrinopenia e coagulopatia come condizioni associate procedure con piastrinopenia e ascite come condizioni associate procedure con coagulopatia e ascite come condizioni associate procedure con piastrinopenia , coagulopatia e ascite come condizioni associate totale procedure suspected infectious cirrhosis . 
the histological diagnoses were assessed for each category of patients , and correlation between histological and clinical findings produced three possible results : ( 1 ) histology confirmed the clinical suspicion , ( 2 ) histology refuted the clinical suspicion or ( 3 ) histology was indeterminate . 
the last category included inadequate specimens or sampling errors and inconclusive biopsy results . all procedures were carried out under local anaesthesia of the puncture site ( the right internal jugular vein ) to allow easier catheterisation of the suprahepatic veins . 
questultima comprende i pazienti in cui il prelievo bioptico stato insufficiente o non corretto e i pazienti in cui anche lesito della biopsia non ha permesso di chiarire i dubbi diagnostici . 
 la procedura prevede la somministrazione di un anestetico locale nella sede della puntura , che quella della vena giugulare interna destra , che ovviamente permette un pi agevole cateterismo delle vene sovraepatiche . 
quando si osserva reflusso di sangue nella siringa , si fa procedere la cannula oltre lago e dopo aver ritirato lago , viene introdotta una guida standard da 0 , 035 pollici ( cordis , miami , florida , usa ) , che viene introdotta nella vena cava inferiore . 
viene utilizzato inizialmente un introduttore da 5 f che , una volta cateterizzata con un catetere multipurpose da 5 f una vena sovraepatica ( generalmente la destra ) , viene sostituito da un introduttore da 7 f ( set per accesso e biopsia epatica della cook vascular incorporated , leechburg , pa , usa ) ; questo giunge fino alla sovraepatica precedentemente cateterizzata e permette lintroduzione dellago [ 8 , 9 ]  . 
nel nostro studio stato utilizzato un ago quick core da 18 - gauge , lungo 60 cm ( cook , prodotto dalla proact ltd . , state college , pa , usa ) che permette il prelievo in modo automatico , a scatto [ 7 , 8 ]  . 
la punta dellago viene avanzata oltre lestremo del catetere , nel parenchima epatico , durante lapnea respiratoria del paziente e con un meccanismo automatico , azionato dalla mano delloperatore , viene ottenuto un campione di tessuto di circa 2 c la procedura viene controllata in fluroroscopia e vengono monitorati i parametri vitali del paziente durante tutta lindagine . 
a tissue core of up to 2 cm was obtained by manually triggering the spring - loaded mechanis the procedure was performed under fluoroscopic guidance , and the patients vital signs were continuously monitored . 
specimens judged to be adequate were placed either into a test tube containing 10% formalin or into a dry ( suspected haemochromatosis or wilsons disease ) and sent for histological examination . 
 for metal quantification tube test there were three cases of failure to locate the right internal jugular ve in two patients , we used the right external transjugular approach and in one , the left internal jugular approach . 
in the third patient , with a transplanted liver , a transfemoral access was chosen after preliminary angiography had documented the new anatomical configuration of the suprahepatic veins relative to the inferior vena cava . 
in all other cases , we used the seldinger technique , with puncture of the right internal jugular vein several cases , puncture of the internal jugular vein was facilitated by ultrasonography , which reduced the risk of puncturing the ipsilateral common carotid artery . 
it should , in fact , be recalled that in patients with serious coagulopathy and / or thrombocytopenia , even the slightest injury to this vessel can result in severe haemorrhage . results of 76 procedures performed on 72 patients , biopsies proved diagnostic in 69 cases ( 91% )  . 
there were two cases ( 3% ) of sampling error ( acquisition of renal tissue ) and five cases ( 6% ) of nonconclusive histology ( one patient with suspected gvhd , two with acute liver dysfunction of unknown origin and two with chronic liver dysfunction of unknown origin )  . 
the fistula was successfully embolised by the same team of intervencampione giudicato idoneo viene posto in una provetta con formalina al 10% o in una provetta a secco , nel caso di un dosaggio quantitativo dei metalli ( sospetta emocromatosi o morbo di wilson ) e avviato allesame istologico . 
 in 3 casi di irreperibilit della giugulare interna destra la tecnica di esecuzione della procedura si avvalsa in 2 pazienti dellapproccio per via transgiugulare esterna destra e in 1 soggetto della puntura della giugulare interna sinistra , mentre in un paziente trapiantato di fegato , documentata con unangiografia preliminare la nuova conformazione anatomica delle vene sovraepatiche rispetto alla vena cava inferiore , stato preferito un accesso per via transfemorale ; in tutti gli altri casi stata usata la tecnica percutanea di seldinger pungendo la vena giugulare interna destra . 
tra laltro , lutilizzo di un ecografo ha facilitato in diversi casi la puntura della giugulare interna , riducendo i rischi di puntura dellarteria carotide comune omolaterale : non va dimenticato che in pazienti con gravi problemi dellemocoagulazione e / o piastrinopenici la lesione se pur minima di tale vaso , pu provocare seri fenomeni emorragici . risultati nelle 76 procedure interventistiche eseguite su un totale di 72 pazienti , le biopsie risultate informative ai fini diagnostici sono state 69 ( 91% )  . 
in 2 casi ( 3% ) il prelievo non si era rivelato corretto ( tessuto renale ) e in altri 5 casi ( 6% ) la biopsia non ha fornito una diagnosi di certezza ( in 1 paziente con sospetta gvhd , in 2 con epatopatia acuta di origine sconosciuta e in due pazienti con epatopatia cronica di origine ignota )  . 
le 4 procedure aggiuntive sono state eseguite , con esito questa volta positivo , nei 2 pazienti in cui era stato prelevato erroneamente tessuto renale , e in due pazienti per escludere con sicurezza il sospetto di gvhd . solo in 1 caso , su 76 procedure eseguite ( 1% ) si avuta una complicanza maggiore , rappresentata dalla formazione di una fistola artero - venosa e artero - biliare con conseguente emorragia ed anemizzazione del paziente . 
 altre complicanze minori ( 5% ) sono state 1 ematoma laterocervicale destro e 3 casi di dolenzia nella sede della puntura , che in 1 paziente ha richiesto la somministrazione di un antidolorifico . 
nel gruppo 1 ( sottogruppo a ) , su 23 procedure eseguite ( 3 sono state ripetute 2 volte negli stessi pazienti ) , si sono ottenute 21 diagnosi conclusive di cui 14 diverse rispetto a quelle sospettate clinicamente di gvhd o vod ( 69% )  . 
nel gruppo 1 ( sottogruppo b ) , 3 pazienti su 3 ( 100% ) hanno avuto la diagnosi 1012 radiol med ( 2008 ) 113 : 10081017 tional radiologists , and the patients haemodynamic status stabilised . 
in patients with suspected gvhd or vod ( group 1 , subgroup a ) , histology provided 21 conclusive diagnoses out of 23 procedures on 21 patients ( three patients underwent repeat sampling ) ; 14 of these differed from the clinically suspected diagnoses of gvhd or vod ( 69% )  . 
among patients with a clinical suspicion of organ rejection ( group 1 , subgroup b ) , 3 / 3 patients ( 100% ) were found not to have organ rejection . 
nel gruppo 4 , 2 pazienti su 11 ( 18% ) con diagnosi conclusiva , hanno avuto una diagnosi diversa da quella di cirrosi . complessivamente le diagnosi ottenute con la biopsia hanno confermato il sospetto clinico in 35 casi su 69 ( 51% ) , mentre ha portato ad una nuova diagnosi in 34 casi su 69 ( 49% )  . 
histology proved inconclusive in 7 / 76 procedures ( 9% )  . in 11 / 34 cases ( 32% ) in which biopsy changed the clinical diagnosis , the definitive diagnosis allowed us to institute a treatment that otherwise would have been empirical : in eight patients with acute liver disease , in two with alcoholic liver disease and in one with chronic liver disease of unknown origclinically relevant information was thus gained in 34 / 69 successful procedures ( 49% )  . discussion the significance of liver biopsy in the evaluation of patients with abnormal liver function tests is universally accepted [ 14 ]  . 
in fact , we had one major complication only ( 1% ) and an in un paziente con epatopatia cronica di origine sconosciuta . su 69 procedure che hanno avuto successo si sono ottenute informazioni clinicamente importanti in 34 casi ( 49% )  . discussione limportanza della biopsia epatica per la valutazione delle alterazioni della funzionalit epatica ormai riconosciuta universalmente [ 14 ]  . 
la piastrinopenia grave , le coagulopatie e lascite massiva , situazioni cliniche frequenti nei pazienti epatopatici , controindicano lesecuzione della biopsia del fegato per via percutanea [ 57 ]  . 
le nostre osservazioni su 76 procedure eseguite hanno confermato la bassa percentuale di complicanze maggiori , solo un caso ( 1% ) , e lelevata adeguatezza [ 10 ] dei campioni bioptici ottenuti che , non considerando i due errori tecnici di prelievo di tessuto renale , stata del 100% , anche se 5 esiti di normalit istologica del prelievo bioptico non hanno contribuito a raggiungere una diagnosi conclusiva sulla base del quesito clinico . 
in questi casi prima di procedere alla puntura si consiglia lesecuzione di uno studio angiografico o di prendere visione di precedenti esami strumentali del paziente ( tc o rmn ) che documentino lesatta anatomia vascolare . 
the number and diversity of the possible causes of liver function abnormalities support the need for correct histological sampling to establish the correct diagnosis and thus be able to plan a safer therapeutic and prognostic management . elevato delle possibili patologie allorigine delle alterazioni della funzionalit epatica dimostrano lopportunit di ottenere un corretto prelievo istologico in questi pazienti per unappropriata diagnosi e di conseguenza una gestione terapeutica e prognostica pi sicura . 
 tabella 5 risultati della biopsia epatica , gruppi 2 , 3 e 4 : rispettivamente pazienti con sospetta cirrosi di eziologia infettiva , alcolica e ad eziologia ignota our results also emphasise the importance of biopsy even in patients for whom it has not been ordered because of poor general health or contraindications to percutaneous biopsy . 
with regard to group 1 , a firm diagnosis of gvhd or vod ( subgroup a ) is essential for deciding to undertake immunosuppressive therapy , which might otherwise be avoided . 
likewise , a diagnosis of organ rejection in liver transplant patients ( subgroup b ) is crucial for deciding whether to increase the dose of immunosuppressive medications or to address other causes of liver failure . 
a histological diagnosis also allows correct treatment planning in patients with acute liver dysfunction of unknown una gvhd o una vod ( sottogruppo a ) infatti fondamentale per poter decidere se intraprendere una terapia immunodepressiva , altrimenti evitabile . 
analogamente , diagnosi di rigetto dorgano in pazienti trapiantati di fegato ( sottogruppo b ) indispensabile per valutare la necessit di aumentare la posologia di farmaci immunodepressivi o , invece , di indirizzarsi verso altre cause di insufficienza epatica . 
vi , poi , la possibilit di intraprendere le misure terapeutiche pi corrette nei pazienti in cui la disfunzione epatica acuta di origine sconosciuta ( sottogruppo c ) : la documentazione di unepatopatia di tipo tossico da farmaci ( come avvenuto in 4 pazienti della nostra casistica ) permette di risolvere lalterazione sospendendo o diminuendo la posologia dei farmaci somministrati ; in altri casi stato possibile escludere la riacutizzazione di malattia 1016 radiol med ( 2008 ) 113 : 10081017 origin ( subgroup c ) : demonstration of a toxic , druginduced liver disorder ( as occurred in four of our patients ) allows the abnormality to be corrected by discontinuing the drug or reducing the doses . 
in other cases , histology enabled us to exclude acute exacerbation of the underlying condition ( as in one patient with systemic lupus erythematosus ) and avoid increasing the dose of corticosteroids , to suggest other diagnostic hypotheses or different diagnostic tests ( as occurred in one patient with portal thrombosis ) , or to discover three cases of previously unknown cirrhosis . 
the subdivision of group 1 into subgroups was justified by the different treatment strategies applicable to each subgroup [ 3 , 11 ]  . in patients with suspected cirrhosis ( groups 2 , 3 , 4 ) , who additionally had a worse clinical prognosis compared with group 1 , biopsy played a far less significant role . 
this was particularly true for groups 2 and 4 , in which the number of incorrect clinical diagnoses was 5 / 23 ( 22% ) and clinical accuracy was 88% . 
instead , biopsy proved useful in group 3 where histology rejected as many as three clinical diagnoses of alcoholic cirrhosis in seven patients ( 43% ) , most likely the result of a failure to quantify the duration and magnitude of alcohol abuse [ 12 ]  . 
this emphasises the importance of an accurate patient history and the usefulness of histology where the history is inadequate . our experience highlights the role of transjugular liver biopsy in patients with acute liver function abnormalities whose clinical condition may be substantially improved by a correct diagnosis and appropriate therapy . 
furthermore , in 8 / 15 cases ( 53% ) with a definitive diagnosis ( subgroup c ) , the biopsy result guided treatment that otherwise would have been empirical [ 1316 ]  . 
in group 3 , histology provided 7 / 7 ( 100% ) conclusive diagnoses , three of which would not have been established on the basis of the clinical data ( 43% )  . 
this points to the importance of biopsy in patients with suspected alcoholic cirrhosis , especially in cases of clinically undemonstrated alcohol abuse , given that abstinence can dramatically improve clinical status ( 17 )  . 
by contrast , in patients with suspected cirrhosis , either infectious or of other aetiology ( groups 2 and 4 ) , biopsy results largely confirmed the clinical suspicion , as only 5 / 23 patients ( 22% ) turned out to have clinically unsuspected conditions . 
only 2 / 25 ( 8% ) diagnoses were inconclusive in these two groups . ( 1 paziente con lupus eritematoso sistemico ) , evitando di aumentare la posologia dei corticosteroidi , o indirizzare i clinici verso altre ipotesi diagnostiche o differenti indagini strumentali ( come in un paziente affetto da trombosi portale ) , e si sono potuti scoprire 3 casi di cirrosi , mai documentati in precedenza . 
la suddivisione del gruppo 1 in sottogruppi stata giustificata dal diverso atteggiamento terapeutico che si pu intraprendere nei soggetti di ciascuno dei sottogruppi [ 3 , 11 ]  . nei pazienti con sospetta cirrosi ( gruppi 2 , 3 e 4 ) , in cui tra laltro la prognosi clinica era peggiore rispetto a quelli del gruppo 1 , il ruolo della biopsia risultato sicuramente inferiore , in particolare nei gruppi 2 e 4 , dove complessivamente le diagnosi cliniche mancate sono state 5 su un totale di 23 pazienti ( 22% ) con unaccuratezza clinica quindi dell88% , mentre si rilevata utile nel gruppo 3 dove ben 3 sospette diagnosi cliniche di cirrosi alcolica su 7 pazienti ( 43% ) non sono state confermate dal risultato del prelievo istologico , probabilmente per la mancata quantificazione del reale consumo alcolico di tali pazienti e del tempo per cui questo abuso stato protratto [ 12 ]  . 
se ne deduce , per questi pazienti , limportanza dellanamnesi e , dove questa sia carente , lutilit di una biopsia . dalla nostra esperienza appare fondamentale lutilizzo della biopsia del fegato per via transgiugulare nei pazienti con unalterazione acuta della funzionalit epatica in cui una corretta diagnosi e la successiva terapia possono portare a un cospicuo miglioramento delle sue funzioni : in questo gruppo infatti complessivamente si sono avute 25 nuove diagnosi su 39 casi in cui si raggiunta una diagnosi sicura ( 64% ) , di cui il risultato pi significativo considerando la casistica si avuto nel sottogruppo a con una percentuale di nuove diagnosi del 67% . 
inoltre in 8 casi su 15 ( 53% ) con diagnosi definitiva ( sottogruppo c ) , si potuta instaurare una terapia altrimenti non proponibile se non empiricamente [ 1316 ]  . 
le diagnosi conclusive nel gruppo 3 sono state 7 su 7 ( 100% ) con 3 diagnosi non documentabili in base ai soli dati clinici ( 43% ) , che dimostrano limportanza della biopsia anche in quei pazienti con sospetta cirrosi da abuso alcolico dove questo non sia ben definito , soprattutto perch lastinenza pu migliorare in modo importante le loro condizioni cliniche ( 17 )  . 
nelle sospette cirrosi su base infettiva o di altra eziologia , invece , i risultati dellindagine bioptica hanno sostanzialmente confermato gli orientamenti diagnostici ottenuti con le indagini di laboratorio e lesame clinico , considerando che solo 5 pazienti su 23 ( 22% ) hanno rivelato quadri clinici inaspettati . 
patti1 1department of diagnostic and interventional radiology , 2intensive care unit , 3department of surgery v , ospedale ferrarotto , via citelli 16 , 95124 catania , italy 4department of radiology , policlinico paolo giaccone , palermo , italy 5department of radiology , ospedale garibaldi centro , catania , italy 6unit of oncology , ospedale vittorio emanuele , via plebiscito 125 , 95124 , catania , italy 7department of haematology , ospedale ferrarotto , via citelli 16 , 95124 , catania , italy correspondence to : a . 
basile , via trieste 14 , 95124 catania , italy , tel . : + 39 - 095 - 7435947 , e - mail : antodoc@yahoo.com received : 8 october 2007 / accepted : 10 december 2007 / published online : 8 september 2008 springer - verlag 2008 abstract purpose . 
cementoplasty alone or in combination with radiofrequency ( rf ) ablation was performed in 14 skeletal extravertebral segments in 13 patients with ages ranging from 50 to 74 ( average 67 ) years . 
the primary tumours were myeloma ( n = 5 ) , renal carcinoma ( n = 5 ) , hepatocellular carcinoma ( n = 2 ) and bladder carcinoma ( n = 2 )  . 
sono state trattate con cementoplastica 14 lesioni in 13 pazienti con et compresa tra 50 e 74 anni , media 67 anni , quattro di queste precedute dalla ablazione con rf ; le neoplasie primitive erano mieloma ( n = 5 ) , carcinoma renale ( n = 5 ) , carcinoma epatocellulare ( n = 2 ) , carcinoma vescicale ( n = 2 )  . 
lindicazione clinica al trattamento stata data dalla presenza di un valore della visual analogue scale ( vas ) superiore a 5 , refrattario o parzialmente refrattario al trattamento con analgesici . 
in 10 pazienti stata eseguita la sola cementoplastica mentre in 3 pazienti rispettivamente con grossa metastasi scapolare successivamente recidivata e con masse osteolitiche allosso iliaco , la cementoplastica stata preceduta dalla ablazione con rf . 
in our experience , cementoplasty alone for small lesions or combined with rf ablation in larger lesions is an effective and safe therapy in the palliative management of painful extraspinal bone metastases . keywords cementoplasty radiofrequency ablation bone metastasis riduzione del valore vas rimasto pressoch costante durante i follow - up successivi . 
nella nostra esperienza la cementoplastica , da sola in lesioni di piccole dimensioni o preceduta dalla ablazione con rf per lesioni di maggiori dimensioni rappresenta una efficace terapia nel trattamento del dolore derivante da metastasi ossee extra - spinali . 
 parole chiave cementoplastica ablazione con radiofrequenze metastasi ossee introduction introduzione the approach to inoperable and painful bone metastases is essentially conservative and based on the use of radiotherapy and chemotherapy combined with supportive pain relief involving , in some cases , administration of massive doses of analgesics . 
cementoplasty was originally used under the name of vertebroplasty in spinal metastases [ 1 , 2 ] and was later extended to extraspinal lesions [ 3 , 4 ]  . 
rf ablation was employed for years in parenchymal lesions , with excellent results , and its applications have only recently been extended to bone lesions [ 5 , 6 ]  . 
the combination of rf ablation and cementoplasty has been very effective in managing pain due to extraspinal bone metastasis , with success rates ranging from 95% to 100% [ 7 , 8 ]  . 
each method can also be used alone , particularly in small lesions without signs of extracompartmental involvement where the effectiveness of combined therapy has not been univocally demonstrated . although a large body of literature exists on the use of these techniques in spinal lesions , few reports have addressed extraspinal applications . 
this paper illustrates our experience with interventional treatment of extraspinal bone metastases using cementoplasty alone in small lesions and cementoplasty combined with rf ablation in larger lesions . materials and methods we retrospectively reviewed the records of 13 patients ( ten men and three women ; age range 5074 years ; mean age 67 years ) who underwent cementoplasty for painful osteolytic metastases between june 2006 and august 2007 ( table 1 )  . we treated 14 extraspinal secondary localisations of lattuale trattamento delle metastasi ossee dolorose inoperabili sostanzialmente conservativo , e si basa principalmente sullutilizzo della radioterapia e della chemioterapia , integrate da terapie antalgiche di supporto , che talvolta , prevedono la somministrazione di ampie dosi di analgesici . negli ultimi anni , alcune metodiche interventistiche quali la cementoplastica e la ablazione con radiofrequenze ( rf ) sono entrate a pieno titolo nel management palliativo delle lesioni ossee dolorose , primitivamente applicate nelle localizzazioni rachidee col termine di vertebroplastica [ 1 , 2 ] , e poi estese in ambito extra - spinale [ 3 , 4 ]  . 
in particolare lablazione con rf stata per anni utilizzata in ambito parenchimale con ottimi risultati e solo da poco ha esteso lapplicazione anche a livello osseo [ 5 , 6 ]  . 
lassociazione dellablazione con rf combinata con la cementoplastica risultata molto efficace nel controllo del dolore da metastasi ossea extrarachidea , con una percentuale di successo che varia dal 95% al 100% [ 7 , 8 ]  . 
ciascuna delle metodiche potrebbe anche essere utilizzata da sola , soprattutto nelle lesioni di piccole dimensioni senza segni di extra - compartimentalit , in quanto in questi casi non stata ancora univocamente dimostrata lefficacia della terapia combinata sulla singola tecnica . 
presentiamo la nostra esperienza nel trattamento interventistico delle neoplasie ossee extraspinali mediante lutilizzo della sola cementoplastica nelle lesioni di piccole dimensioni , in combinazione con lablazione con rf per metastasi di dimensioni maggiori . materiali e metodi abbiamo analizzato retrospettivamente i dati di 13 pazienti 1020 radiol med ( 2008 ) 113 : 10181028 radiol med ( 2008 ) 113 : 10181028 1021 myeloma ( 5 ) , renal carcinoma ( 5 ) , hepatocellular carcinoma ( 2 ) and bladder carcinoma ( 2 )  . 
the clinical indication for treatment was a pain intensity score of 5 or higher on the visual analogue scale ( vas ) and pain totally or partially refractory to analgesic treatment in patients with a life expectancy > 1 month . 
the indication for treatment was established by a team of oncologists , radiotherapists , surgeons and radiologists on the basis of a detailed correlation between clinical history , particularly current symptoms , and ct or mri findings after evaluating the various treatment options and possible contraindications . cementoplasty was performed with 11 or 13 - gauge beveltip needles 10to 15 - cm long and cement ( polymethylmethacrylate ) ( spine - fix , teknimed , france ; cardinal health , france )  . 
a subjective assessment of perceived pain intensity was obtained through analysis of vas scores , where 0 indicates total absence of pain and 10 the worst pain ever experienced , recorded before and immediately after treatment and during the follow - up period . 
in patients with bone metastasis to the pelvis or lower limbs , we also assessed motor function , rated from 0 to 3 on the basis of ambulation ability ( 0 total immobility ; 1 ambulation only with walking aid ; 2 ambulation without walking aid ; 3 total ambulation autonomy )  . 
imaging followup was carried out according to the standard follow - up schedule for the primary tumour , anticipated in the event of worsening of pa technical failure was defined as the inability to access the lesion using the approach established at previous ct and mr imaging . 
clinical success was con et compresa tra 50 e 74 anni ( 10 maschi , 3 donne ) , media 67 anni , sottoposti a cementoplastica per lesioni metastatiche osteolitiche dolorose extra - spinali da giugno 2006 ad agosto 2007 ( tabella 1 )  . 
abbiamo trattato un totale di 14 localizzazioni extra - spinali da mieloma ( n = 5 ) , carcinoma renale ( n = 5 ) , carcinoma epatocellulare ( n = 2 ) e carcinoma vescicale ( n = 2 )  . 
le dimensioni delle lesioni trattate hanno presentato un range compreso tra 9 , 28 , 8cm ( paziente n 9 ) a 23 , 3cm ( paziente n 8 )  . 
lindicazione al trattamento stata posta da un team di oncologi , radioterapisti , chirurghi e radiologi sulla base di una dettagliata correlazione tra storia clinica , con particolare enfasi per la attuale sintomatologia , e con i reperti di imaging tc o rm , valutando le varie opzioni terapeutiche e le eventuali controindicazioni . 
 le cementoplastiche sono state realizzate utilizzando aghi con punta a becco di flauto da 11 o 13 gauges lunghi 1015 cm e con cemento ( polimetilmetacrilato ) ( spine - fix , teknimed , francia ; cardinal health , francia )  . 
tutte le procedure sono state eseguite sotto guida fluoroscopica , in 8 casi integrata alla guida tc ( brilliance 16 , philips , olanda ) , mentre stato eseguito sempre un immediato controllo post - procedura mediante tc . 
la valutazione soggettiva della percezione del dolore per singolo paziente stata eseguita mediante lanalisi del valore della visual analogue scale ( vas ) dove 0 rappresenta lassenza assoluta di sintomatologia algica e 10 il grado massimo di dolore percepito 1022 radiol med ( 2008 ) 113 : 10181028 defined as a quantitative reduction in analgesic medication and improved vas score compared with baseline , as well as improvement in motor function , where applicable . 
complications were classified based on the standards of the society of interventional radiology [ 9 ] into major and minor according to the length of hospitalisation after the procedure , where the lowest grade of major complication involved therapy and hospitalisation for < 48 h . results technical success was achieved in all cases . 
vas scores in all patients were significantly lower , between 3 and 7 points ( mean 4.6 ) within 24 h of the procedure , and they remained substantially unchanged throughout the follow - up period ( table 1 )  . 
among the patients who underwent motor function assessment immediately after the procedure , 2 / 10 showed no functional improvement , so the procedure was considered to have had an antalgic effect only ; the remaining eight patients showed increased motor capabilities . 
we had one major complication : 72 h after the procedure , patient 3 developed fever and leucocytosis , with ct evidence of an abscess in the treated area , which was resolved by percutaneous placement of a drainage catheter . discussion the first interventional procedure proposed for treating pathological bone fractures was vertebroplasty , described by galibert et al . 
the use of cementoplasty in extraspinal sites is based on the principle that the pain caused by vertebral and extravertebral bone tumours has nella propria vita , valutato prima , immediatamente dopo e durante i follow - up . 
per quanto riguarda i pazienti con lesioni alla pelvi o agli arti inferiori stata altres valutata la funzionalit motoria classificata con valori da 0 a 3 in base alla capacit di deambulazione ( 0 = assoluta immobilit ; 1 = deambulazione solo con ausilio ; 2 = deambulazione senza ausilio ; 3 = totale autosufficienza motoria )  . 
i controlli post - procedure sono stati realizzati mediante la valutazione del valore della vas immediatamente dopo il trattamento e per un periodo variabile da 2 a 14 mesi , durante sedute ambulatoriali o mediante interviste telefoniche . 
i controlli con imaging hanno seguito i regolari protocolli oncologici delle singole patologie primitive , anticipati in caso di riscontro di un peggioramento della sintomatologia algica . limpossibilit ad accedere alla lesione secondo lapproccio prestabilito sulla base delle immagini tc ed rm stato considerato come insuccesso tecnico della procedura . per successo clinico si considerato la riduzione quantitativa della terapia antalgica somministrata in precedenza e del parametro vas , nonch delleventuale miglioramento della funzionalit motoria . 
le complicanze della procedure sono state valutate secondo gli standard della society of interventional radiology [ 9 ] , in maggiori e minori a seconda del correlato tempo di ricovero post - procedura dove il grado minore di complicanze maggiori prevede la necessaria terapia supplementare ed il ricovero per meno di 48 ore . risultati il successo tecnico della procedura stato ottenuto in tutti i casi . 
tutti i pazienti hanno immediatamente avvertito dopo la procedura un miglioramento della sintomatologia , riscontrato in una riduzione del valore della vas ( tabella 1 ) e della dose di analgesici . 
a axial computed tomography ( ct ) image and b coronal reconstruction depict the osteolytic lesion and its extension to soft tissues ; c planning of the radiofrequency ( rf ) ablation procedure ( asterisks ) along the lesions longitudinal axis and of d cementoplasty with dual access along the anatomical borders of the scapula ( arrows )  . 
a immagine tc sul piano assiale e b ricostruzione coronale che mostrano la lesione osteolitica , estesa ai tessuti molli , con la pianificazione degli interventi di ablazione con radiofrequenze ( c ; asterischi ) lungo lasse maggiore della lesione , e di cementoplastica ( d ) con doppio accesso lungo i reperi anatomici della scapola ( frecce ) ; e controllo tc finale con ricostruzione mip mostra il risultato della procedura . similar aetiology , namely , mechanical stress on the periosteal nociceptors and a cascade of biohumoural factors and cytokines produced by the tumour cells themselves [ 11 ]  . 
the analgesic effect of tumour necrosis is , instead , the rationale that led to the application of rf ablation to bony tissues , initially in vertebral and then in extravertebral settings , employing both standard and bipolar techniques [ 4 , 8 , 13 , 14 ]  . 
both treatments are therefore aimed at relieving pathe most modern approach to managing painful bone tumours is to use the two treatments in combination , even though there is follow - up stato ottenuto in tutti i pazienti ed variato da 2 a 14 mesi . 
nelle immediate 24 ore dopo la procedura si ottenuta una riduzione significativa del vas score in tutti i pazienti , variabile da 3 a 7 ( media = 4 , 6 ) sostanzialmente invariato durante tutto il periodo di follow - up ( tabella 1 )  . 
nei pazienti valutati anche per la funzionalit motoria immediatamente post - trattamento , 2 / 10 di questi non hanno avuto un miglioramento funzionale , pertanto la procedura ha avuto solo valore antalgico , mentre in tutti gli altri si avuto una aumento della potenzialit motoria in tal senso . 
3 che ha accusato a 72 ore dalla procedura febbre e leucocitosi con evidenza alla tc di un ascesso nella zona trattata risolto con il posizionamento di un drenaggio per cutaneo . discussione la prima applicazione interventistica nel trattamento delle fratture ossee patologiche rappresentata dalla vertebroplastica , descritta per primo da galibert nel 1987 [ 10 ]  . lutilizzo della ementoplastica in sedi extra - spinali si basa sul principio secondo il quale il dolore da neoplasia ossea in sede vertebrale ed extravertebrale sia sotteso da identiche cause eziogenetiche , ed in particolare dallo stress meccanico operato sulle terminazioni nocicettive del periostio e su tutto una cascata di fattori bioumorali e di citochine secreti dalle stesse cellule tumorali [ 11 ]  . 
lazione analgesica data dalla necrosi del tessuto tumorale rappresenta invece la base dellapplicazione della ablazione con rf anche in ambito osseo , anche in questo caso prima in ambito vertebrale e successivamente in ambito extraspinale sia con tecnica standard che bipolare [ 4 , 8 , 13 , 14 ]  . per entrambe le terapie perci , il fine quello di ridurre il dolore . 
lindirizzo pi moderno oggi rappresentato dallutilizzo combinato delle due procedure nel management del dolore da neoplasia ossea , tuttavia a tuttoggi deve ancora essere dimostrata una chiara maggior efficacia dellassociazione della ablazione con rf con la cementoplastica nel trattamento delle lesioni di piccole dimensioni , anzi , in un recente articolo , kojima et al . 
 [ 15 ] trattando 28 metastasi ossee dolorose mediante ablazione con rf con e senza combinazione con cementoplastica o con radioterapia , non ha riscontrato nessuna correlazione tra lefficacia del trattamento , la dimensione delle neoplasie , la combinazione delle terapie e la percentuale della necrosi tumorale . 
a immagine tc assiale che mostra la frattura patologica della scapola ( freccia ) a distanza di 7 mesi dal primo trattamento ; le immagini in tc mostrano il trattamento mediante posizionamento di ago elettrodo ( b ) e cementoplastica con controllo finale tc ( c ) che mostra il cemento inserito tra la precedente soluzione di continuo dei monconi ossei . radiol med ( 2008 ) 113 : 10181028 1025 fig . 
3a - n a 71 - year - old man ( patient 9 ) with osteolytic metastasis to the iliac bone completely disrupting bone anatomy and showing signs of extracompartmental involvement . 
a frontal computed tomography ( ct ) reconstruction shows massive osteolysis of the iliac bone ( arrow ) , b also evident on reconstructions in the axial plane and c along the long axis of the iliac bone . 
in particular , the first approach was e parallel to the sacrum and sacro - iliac joint , f , g as can be seen on the fluoroscopic images and h final postprocedural ct scan . 
i , l reconstructed ct images show the second approach with the radiofrequency ( rf ) electrode ( white arrow ) inserted coaxially within the cementoplasty needle ( black arrow )  . 
a ricostruzione tc su piano frontale mostra la massiva osteolisi dellosso iliaco ( freccia ) , ulteriormente mostrata anche con ricostruzioni assiali ( b ) e sullasse maggiore dellosso iliaco ( c ) ; d pianificazione dellintervento su ricostruzione tc sagittale che mostra il doppio approccio ( frecce ) sulla base delle linee di forza e dei riferimenti anatomici dellosso . 
in particolare stato eseguito un primo approccio parallelo al sacro ed allarticolazione sacro - iliaca ( e ) ben visibile nelle immagini fluoroscopiche ( f , g ) e dal controllo finale tc ( h ) ; i , l immagini tc ricostruite che mostrano il secondo approccio con lago da rf ( freccia bianca ) inserito coassialmente allinterno dellago da cementoplastica ( freccia nera ) ; m , n ricostruzione tc sul piano frontale e sagittale mostrano risultato finale della procedura dopo lesecuzione della cementoplastica . 1026 radiol med ( 2008 ) 113 : 10181028 no conclusive evidence on the greater efficacy of rf ablation combined with cementoplasty in treating small lesions . indeed , in a recent study , kojima et al . 
sono descritte infatti in letteratura complicanze post - rf di lieve o moderata entit come nei casi di transitoria incontinenza vescicale ed intestinale in un paziente sottoposto a radiofrequenza del sacro o a ustioni cutanee [ 7 ] o di maggiore entit come i casi di incompleta emiplegia in pazienti trattati con rf per tumori vertebrali [ 4 ]  . 
the reported complications of rf ablation are mild or moderate , such as transient bowel and bladder incontinence after treatment of a metastasis involving the sacrum , or skin burns [ 7 ] ; or more severe , such as incomplete hemiplegia in patients treated for vertebral malignancies [ 8 ]  . 
 [ 16 ] treated 23 metastases , 15 of which were extraspinal , with rf ablation and cementoplasty , achieving pain relief in 100% of cases and reduction of analgesic use in 41% ( 7 / 17 patients )  . 
improvement in vas score was 4.62.2 for large tumours ( > 5 cm ; 12 ) and 3.51.3 for the four tumours treated with rf ablation and cementoplasty , without significant differences among the treatment groups . our findings are in broad agreement with those reported in the literature and confirm the high level of efficacy and low rate of complications of both cementoplasty and rf ablation in treating painful skeletal metastases . 
additionally , vas scores remained constant during the follow - up in a patient population with mortality rates ( due to clinical status and tumour progression ) of 50% at 6 months and 66% at 1 year . 
this testifies to the high efficacy of these treatments in improving quality of life , even in patients with a short life expectancy . tistico di metastasi ossee e fra gli studi presenti ancor meno la percentuale riguardante localizzazioni extraspinali . 
 [ 8 ] nel 2004 hanno pubblicato 23 tumori ossei di cui solo 4 extra - assiali , trattati con ablazione a rf e cementoplastica , con il 100% di efficacia analgesica nel giro di una settimana . 
nel 2005 [ 16 ] hanno trattato 23 metastasi con ablazione a rf pi cementoplastica , 15 in sede extra - spinale con una risoluzione del dolore ottenuta nel 100% dei casi e con riduzione della terapia analgesica ottenuta nel 41% dei casi ( 7 su 17 pazienti )  . 
in tale serie 4 metastasi con rf e con cementoplastica e 5 con rf e radioterapia ; il miglioramenti maggiore nel valore vas stato di 4 , 62 , 2 per tumori di grandi dimensioni ( > 5 cm , n = 12 ) , e di 3 , 51 , 3 per i 4 tumori trattati con rf e cementoplastica , come gi accennato , senza significative differenze tra i pazienti trattati con le diverse metodiche . i nostri dati concordano sostanzialmente con quelli della letteratura brevemente riportati , la quale descrive lalta efficacia sia della cementoplastica che della ablazione con rf nel trattamento delle metastasi dolorose scheletriche con basse percentuali di complicanze . 
del maschio4 1 university of milan school of medicine , department of medical and surgical sciences , radiology unit , irccs policlinico san donato , via morandi 30 , 20097 san donato milanese , milan , italy 2 service dimagerie medicale , saint - eloi hospital , chu montpellier , france 3 institute of radiology , university of ancona , italy 4 department of radiology , vita - salute university , san raffaele hospital , milan , italy 5 department of senology , policlinico universitario , bari , italy correspondence to : f . 
ninety patients ( aged 58.616.1 years ) who were candidates for unilateral ( n = 81 ) or bilateral ( n = 9 ) mastectomy underwent mammography and dynamic contrast - enhanced breast mri using a coronal three - dimensional gradient - echo sequence with slice thickness 3 mm before and after intravenous injection of gadoteridol ( 0.1 mmol / kg )  . 
novanta pazienti ( et 58.616.1 anni ) candidate alla mastectomia monolaterale ( n = 81 ) o bilaterale ( n = 9 ) sono state sottoposte a mammografia e rm a contrasto dinamico mediante sequenza tridimensionale coronale gradient - echo con spessore di strato 3 mm , prima e dopo iniezione endovenosa di gadoteridolo ( 0.1 mmol / kg )  . 
la sensibilit risultata del 35% ( 9 / 26 ) per la mammografia e del 38% ( 10 / 26 ) per la rm ( differenza non significativa , test di mcnemar )  . 
mammografia e rm sono risultate entrambe vere positive in 7 casi ( 4 dei quali con diametro misurato istologicamente , pari a 20.012.9 mm , mediana 440 radiol med ( 2008 ) 113 : 439451 median 20 mm ) and a false negative result in 14 cases ( 10 of them measured at pathology , with a diameter of 4.21.9 mm ; median 4.6 mm ) ( p = 0.024 , mann - whitney u test )  . only 46% ( 12 / 26 ) of dcis were detected at mammography and / or mri ; the remaining 54% ( 14 / 26 ) were diagnosed only at pathological examination . 
allorquando lintera mammella assunta come standard di riferimento istologico , sia la mammografia che la rm mostrano ridotta sensibilit per il dcis . parole chiave mammella carcinoma duttale in situ risonanza magnetica ( rm ) a contrasto dinamico mammografia introduction introduzione ductal carcinoma in situ ( dcis ) is a challenging diagnosis in breast imaging . 
its importance is related to the currently favoured hypothesis that invasive ductal carcinoma ( idc ) evolves progressively through sequential stages , usually from ductal hyperplasia without cellular atypia to atypical ductal hyperplasia , to dcis , and , eventually , to idc [ 1 , 2 ]  . this conceptual evolutionary tree may give birth to many branches and dead ends , and many lesions may arrest or even regress [ 1 ]  . 
however , lobular carcinoma in situ ( lcis ) has been recently defined as only a high - risk lesion and grouped with atypical lobular hyperplasia into the socalled lobular intraepithelial neoplasia . 
the risk for invasive breast cancer is estimated to be six to ten times higher for patients with lcis [ 3 , 4 ] and eight to ten times higher for patients with dcis [ 5 , 6 ]  . dcis is a complex histopathological condition in which malignant breast epithelial cells arise and proliferate in the ducts but do not invade the surrounding stroma [ 7 ]  . 
pathologically , lobular neoplasia is characterised by a solid proliferation of loosely cohesive , uniform , small cells that fill and distend the acini of one or more terminal duct lobular units . according to the world health organisation , lobular neoplasia includes as already mentioned both atypical lobular hyperplasia and lcis ; moreover , and lcis was excluded from the list of true malignancies , even though the correct il carcinoma duttale in situ ( dcis , ductal carcinoma in situ ) rappresenta una sfida diagnostica nellimaging mammario . limportanza di tali lesioni collegata allipotesi attualmente favorita secondo la quale il carcinoma duttale invasivo ( idc , invasive ductal carcinoma ) sia il risultato di una progressione sequenziale attraverso stadi successivi , dalliperplasia duttale senza atipie cellulari , alliperplasia atipica , al dcis e , infine , allidc [ 1 , 2 ]  . 
sebbene il carcinoma lobulare in situ ( lcis , lobular carcinoma in situ ) sia stato recentemente definito solo come lesione ad alto rischio e raggruppato con la displasia lobulare atipica nella cosiddetta neoplasia lobulare intraepitealiale , questo quadro concettuale vale anche per i tumori lobulari . 
il rischio di tumori invasivi si incrementa di 6 - 10 volte nelle pazienti con lcis [ 3 , 4 ] e di 810 volte nelle pazienti con dcis [ 5 , 6 ]  . il dcis una lesione istologicamente complessa nella quale cellule epiteliali mammarie maligne nascono e proliferano nel dotto ma non invadono lo stroma circostante [ 7 ]  . si tratta di unentit eterogenea che pu presentare varianti morfologiche che differiscono marcatamente per quadro macroscopico , modello di crescita e caratteristiche cellulari . 
istologicamente si tratta di una proliferazione solida non strettamente coesiva di cellule uniformemente piccole che riempiono e distendono gli acini di una o pi unit globulari di un dotto terminale . secondo lorganizzazione mondiale della sanit , il termine radiol med ( 2008 ) 113 : 439451 definition and treatment of this type of lesions is still debated [ 79 ]  . 
the prevalence of lcis appears to be lower , about 0.1% , although few data are available [ 12 ]  . dcis accounts for 1520% of all cases of breast cancer [ 14 ]  . 
 mammography is commonly considered highly sensitive for dcis due to the frequent association with microcalcifications and the increasing use of screening mammography , which explains its increase in incidence [ 1520 ]  . 
the diagnosis of lcis is relatively rare , as it usually has no specific clinical or mammographic findings [ 21 , 22 ] ; in some cases , it may present as a mass or cause unilateral nipple discharge [ 23 , 24 ] or associated with microcalcifications [ 22 , 25 , 26 ]  . it is commonly identified incidentally in breast tissue biopsies obtained for other reasons . gd - enhanced dynamic magnetic resonance ( mr ) imaging is considered highly sensitive for invasive breast cancer , with a sensitivity of 95%100% [ 2735 ] , but less sensitive for dcis , with a reported sensitivity ranging from 20% to 95% [ 2731 , 3346 ]  . 
according to some authors , mr imaging may be more sensitive for dcis detection compared with mammography but lacks of specificity and may miss small lesions [ 27 , 37 ]  . 
however , most studies on diagnostic accuracy of dcis have a heavy selection bias due to inclusion on the basis of detection with mammography or , less frequently , with mr imaging , without considering dcis missed with both techniques . the purpose of this study was to compare mammography and contrast - enhanced dynamic mr imaging in detecting dcis , using the whole - breast examination as a histopathological reference standard , by reviewing the results of a multicenter prospective study . materials and methods study design and enrolment a multicenter nonrandomised prospective study was performed between 1998 and 2000 involving 18 italian centres with proven breast imaging experience [ 47 ]  . 
we enrolled patients aged 18 years or older of any race with proven bc and a planned unilateral or bilateral mastectomy ( proposed by the surgeon and / or the oncologist or based on the patients preference )  . 
we excluded patients with : absolute contraindications to mr imaging , pregnancy or breast feeding ; severe renal failure ; known hypersensitivity to gd - chelates ; clinical status that would have limited data reliability ; or patients who had been included in other clinical trials during the month prior the enrolment . 
each patient gave written informed consent to the protocol and to the use of data for publication . neoplasia lobulare comprende come abbiamo detto sia liperplasia lobulare atipica che il lcis ; inoltre il lcis stato rimosso dallelenco delle lesioni considerate propriamente maligne , anche se la corretta definizione e il trattamento di questa lesione ancora oggetto di dibattito [ 79 ]  . 
la prevalenza del dcis negli studi autoptici oscilla tra 0.2% e 16% [ 1014 ] ; quella del lcis minore , circa lo 0.1% , anche se i dati disponibili sono limitati [ 12 ]  . 
 la mammografia comunemente considerata molto sensibile per il dcis , data la frequente associazione con la presenza di microcalcificazioni e la diffusione dei programmi di screening mammografico che possono spiegare lincremento osservato dellincidenza di dcis [ 1520 ]  . 
la diagnosi di lcis un evento relativamente raro , poich frequentemente privo di caratteristiche cliniche o mammografiche specifiche [ 21 , 22 ] ; occasionalmente pu presentarsi come massa o dare segno di s attraverso una secrezione unilaterale dal capezzolo [ 23 , 24 ] o essere associato a microcalcificazioni [ 22 , 25 , 26 ]  . 
per lo pi un reperto incidentale nel contesto di tessuto mammario biopsiato per altri motivi . la risonanza magnetica ( rm ) a contrasto dinamico ritenuta altamente sensibile per i tumori mammari invasivi , con livelli di sensibilit tra il 95% e il 100% [ 2735 ] , non altrettanto per i dcis , con livelli di sensibilit tra il 20% e il 95% [ 2731 , 3346 ]  . 
secondo alcuni autori , la sensibilit della rm per i dcis potrebbe essere superiore a quella della mammografia , comunque limitata in caso di lesioni di piccole dimensioni e associata a bassa specificit [ 27 , 37 ]  . 
tuttavia , la maggior parte degli studi sullaccuratezza diagnostica della rm per i dcis soffre di una pesante distorsione sistematica nella selezione dei casi dovuta allinclusione sulla base della diagnosi mammografica o , meno frequentemente , rm delle lesioni , senza considerare i dcis non riconosciuti da entrambe le modalit diagnostiche . lo scopo di questo studio stato quindi confrontare mammografia e rm a contrasto dinamico nel riconoscimento dei dcis , utilizzando lesame istologico dellintera mammella come reference standard , mediante la revisione del data base di uno studio multicentrico prospettico . materiali e metodi disegno dello studio e arruolamento tra il 1998 e il 2000 stato realizzato uno studio prospettico multicentrico non randomizzato che ha coinvolto 18 centri italiani con elevata esperienza nellimaging senologico [ 47 ]  . 
 imaging film - screen mammography was performed with standard high - quality methods ( two or three views per breast examination ) , using additional projections and / or targeted compression and magnification when required . 
an intravenous bolus injection of gadoteridol ( prohance , bracco , milan , italy ) was given at a standard single dose of 0.1 mmol / kg of body weight at a rate of 2 ml / s , followed by a flush of 20 ml of saline solution at the same rate , using an automatic injector . 
the postcontrast sequence , identical to the precontrast sequence , was acquired beginning 12 s after the start of the contrast injection and was repeated up to 8 min after injection . 
 postprocessing was performed using temporal subtraction ( postcontrast minus precontrast ) , maximum intensity projections ( mips ) and multiplanar reconstructions ( mprs ) , and generating dynamic signal intensity - to - time and / or percentage enhancement - to - time curves for regions of interest ( roi ) of 33 pixels positioned within the lesion on subjectively recognised areas of maximal contrast enhancement . 
lesion location was defined using a nine - region map ( eight segments plus the nipple region ) and were classified according to the 1981 who classification of breast cancers [ 49 ]  . 
sono state arruolate pazienti maggiorenni di qualsiasi gruppo razziale o etnico , alle quale fosse stato diagnosticato un tumore mammario e per le quali fosse programmata una mastectomia monoo bilaterale ( su proposta del chirurgo e / o delloncologo o perch tale trattamento era preferito dalla paziente )  . 
ha rappresentato motivo di esclusione la presenza di : controindicazioni assolute alla rm ; gravidanza o allattamento ; insufficienza renale severa ; nota ipersensibilit ai chelati del gadolinio ; stato clinico che avrebbe potuto limitare laffidabilit dei dati ; arruolamento in altri trial clinici nel mese precedente larruolamento nello studio . 
mammografia , rm ed esame istopatologico sono stati effettuati in un intervallo temporale massimo di 60 giorni . imaging le indagini mammografiche sono state effettuate con tecnica analogica standard di elevata qualit ( due o tre proiezioni per ciascuna mammella ) , eseguendo ulteriori proiezioni e / o ingrandimento con compressione mirata quando ritenute necessarie . 
la rm stata effettuata a 1 o 1.5 t , nelle donne fertili tra il 7 e il 14 giorno del ciclo mestruale , senza limitazioni di programmazione nelle donne in postmenopausa . 
 stata iniettata per via endovenosa mediante iniettore automatico una singola dose di 0.1 mmol / kg di gadoteridolo ( prohance , bracco , milano ) a 2 ml / s , seguita da 20 ml di soluzione fisiologica alla stessa velocit . 
la sequenza postcontrasto , identica alla precontrasto , stata acquisita a partire da 12 secondi dopo linizio della somministrazione del contrasto e ripetuta fino a 8 minuti dopo liniezione del contrasto . 
 il postprocessing stato realizzato mediante sottrazione temporale ( immagini postcontrasto meno precontrasto ) , proiezioni con algoritmo di massima intensit ( mip ) , ricoradiol med ( 2008 ) 113 : 439451 lected and processed by a central unit . 
the offsite reviewing of mammograms and mr images was performed by two breast radiologists with more than 10 years experience in both techniques ( fifth and sixth authors ) , in consensus . 
the breast imaging reporting and data systems ( bi - rads ) diagnostic score from 1 to 5 ( 1 negative , 2 benign , 3 probably benign , 4 suspicious and 5 highly suggestive of malignancy ) was assigned to each mammographic or mr finding . 
for mr imaging , morphological and dynamic data ( initial signal intensity increase , post - initial - signal dynamic behaviour , shape , border and contrast agent distribution within enhancing lesions ) were combined according to the multifactorial scoring system proposed by fischer et al [ 44 ] and subsequently tested by baum et al [ 50 ]  . 
the absence of contrast enhancement was translated into bi - rads 1 ; a fisher - baum score from 0 to 2 was translated into bi - rads 2 ; the fisher - baum score 3 was translated into bi - rads 3 ; a fisherbaum score 4 or 5 was translated into bi - rads 4 ; and a fisher - baum score from 6 to 8 was translated into birads 5 . 
the density pattern on mammography was distinguished as fatty or almost entirely fatty ( pooled as fatty pattern ) or scattered fibroglandular , heterogeneously dense or extremely dense ( pooled as nonfatty pattern )  . 
 comparison of the location of the breast lesions at mammography , mr imaging and pathological examination was performed offsite using the same nine - region map by a third radiologist ( first author ) who matched mammographic and mr imaging findings with pathological reports . 
attention was paid during the lesion - matching procedure to account for vertical displacement in the oblique projection on mammograms and to consider all available mr imaging data ( native and subtracted scans , mips and mprs )  . 
as already described in the previous report concerning the general results of the multicenter study [ 48 ] , 90 patients [ 58.616.1 years old , meanstandard deviation ( sd ) ] with complete mammographic , mr imaging and pathological correlation were available for evaluation . 
this population included nine bilateral synchronous breast cancers , providing a total of 99 breasts for subsequent analysis . statistical analysis nonparametric mcnemar and mann - whitney u tests were used . 
 esame istopatologico la valutazione istopatologica dellintera mammella stata realizzata da ciascun centro mediante sezioni ogni 5 mle lesioni sono state localizzate su una mappa a nove regioni ( 8 segmenti pi la regione areolare ) e classificate secondo le norme stabilite nel 1981 dallorganizzazione mondiale della sanit [ 49 ]  . 
 analisi delle immagini e correlazione radiologicopatologica tutte le immagini mammografiche e rm e i risultati istopatologici sono stati raccolti e processati da ununit centrale . la revisione centrale delle immagini mammografiche e rm stata condotta da due radiologi con oltre 10 anni esperienza in entrambe le tecniche ( quinto e sesto autore ) , in consenso . 
stato attribuito un punteggio diagnostico bi - rads da 1 a 5 ( 1 , negativo ; 2 , benigno ; 3 , probabilmente benigno ; 4 , sospetto ; e 5 , altamente suggestivo di malignit ) a ciascun reperto mammografico e rm . 
per la rm i parametri morfologici e dinamici ( incremento precoce dellintensit del segnale , comportamento dinamico , forma , margini , e distribuzione del contrasto nel contesto della lesione ) sono stati combinati secondo il punteggio multifattoriale proposto da fischer et al [ 44 ] e successivamente testato da baum et al [ 50 ]  . 
i reperti rm con punteggio da 1 a 3 secondo lo schema di fischer e baum sono stati considerati negativi mentre quelli con punteggi da 4 a 8 sono stati considerati positivi . 
la densit mammografica stata categorizzata come pattern adiposo o quasi completamente adiposo ( raggruppati come pattern adiposo ) o fibroghiandolare sparso , disomogeneamente denso o estremamente denso ( raggruppati come pattern non adiposo )  . 
 la comparazione della sede di ciascuna lesione alla mammografia , alla rm e allesame istopatologico stata realizzata centralmente da un terzo radiologo ( primo autore ) che ha correlato i reperti mammografici e rm con il risultato istopatologico utilizzando la medesima mappa a 9 444 radiol med ( 2008 ) 113 : 439451 table 1 size at pathology of the 26 dcis maximal diameter number less than 5 mm from 5 to less than 10 mm from 10 to less than 20 mm equal to or greater than 20 mm not assessed total tabella 1 dimensioni dei 26 dcis allesame istopatologico diametro massimo numero meno di 5 mm da 5 a 10 mm da 10 a 20 mm uguale o maggiore di 20 mm non valutati totale results of 99 breasts examined , pathology revealed 27 dcis , but one of them was subsequently excluded because pathological re - evaluation gave a conclusive report for microinvasive tumour . 
thus , 26 dcis in 14 breasts of 14 patients [ age 52.09.6 ( meansd ) , median 50 years ] were considered . details on the dcis size are reported in table 1 . 
 mammography detected ( bi - rads > 3 ) 9 dcis : four masses , two masses with microcalcifications , two clusters of microcalcifications not associated with a mass and one architectural distortion . 
details are reported in table 2 . the sensitivity for dcis of mammography and mr was 35% ( 9 / 26 ) and 38% ( 10 / 26 ) , respectively , without significant differences ( mcnemar test )  . 
a significant difference in size was found between the group of four lesions detected by both modalities and measured at pathology versus that of the ten lesions missed by both modalities and measured at pathology ( p = 0.024 , mann - whitney u test )  . the number of true positive and false negative findings for each of the two imaging techniques is reported in table 4 . 
 the combined sensitivity of mammography and mr imaging for the 26 dcis of our series was 46% ( 12 / 26 )  . thus , 54% ( 14 / 26 ) of dcis remained undetected at both regioni . 
il confronto stato realizzato tenendo conto della dislocazione verticale dei reperti alle proiezioni mammografiche medio - laterali oblique e considerando tutti i dati rm disponibili ( immagini native e sottratte , mips e mprs )  . 
come descritto nel precedente report relativo ai risultati generali dello studio multicentrico [ 48 ] , sono state valutate 90 pazienti ( et 58.616.1 anni , mediadeviazione standard ) con completa comparazione tra mammografia , rm e istopatologia . 
sono stati considerati significativi valori di p inferiori a 0.05. risultati sul totale di 99 mammelle esaminate , lesame istopatologico ha dimostrato 27 dcis , uno dei quali stato successivamente escluso dallanalisi poich alla rivalutazione patologica si trattava di un carcinoma microinvasivo . 
sono stati quindi considerati per la presente analisi 26 dcis puri in 14 mammelle di 14 pazienti ( et 52.09.6 , mediana 50 ) ; tipo istologico e dimensioni di queste lesioni sono riportati in tabella 1 . 
 alla mammografia sono state riconosciuti 9 dcis con punteggio bi - rads > 3 : 4 opacit , 2 opacit con microcalcificazioni , 2 cluster di microcalcificazioni isolate , 1 distorsione architetturale . 
i dati sono riportati in dettaglio in tabella 2 . la sensibilit della mammografia nel riconoscimento di dcis risultata 35% ( 9 / 26 ) , quella della rm 38% ( 10 / 26 ) , con differenza non significativa ( test di mcnemar )  . 
stata osservata , per le dimensioni , una differenza significativa tra i 4 dcis riconosciuti ad entrambe le tecniche e istopatologicamente misurati e i 10 dcis non riconosciuti ad entrambe le tecniche e istopatologicamente misurate ( p = 0.024 , test u di mann - whitney )  . radiol med ( 2008 ) 113 : 439451 table 2 morphologic and dynamic characteristics of ten dcis detected by mr imaging characteristic descriptor number shape border round , oval , or lobulated linear , dendritic or stellate well defined ill defined contrast material pattern homogeneous inhomogeneus 0%50% 50%100% > 100% initial enhancement post - initial enhancement continuous plateau washout tabella 2 caratteristiche morfologiche e dinamiche dei 10 dcis riconosciuti alla rm caratteristica descrittore numero forma margini rotondeggiante , ovalare o lobulata lineare , dendritica o stellata 4 ben definiti indefiniti disomogeneo periferico 0%50% 50%100% > 100% plateau washout pattern dellenhancement omogeneo enhancement inizale cinetica dellenhancement continuo mammography and mr imaging . 
the ten dcis not measured at pathology were as follows : three true positive at both techniques ; four false negative at both techniques ; two false negative at mammography and true positive at mr imaging ; and one true positive at mammography and false negative at mr imaging . the sensitivity of the techniques for the two breast density pattern subgroups is reported in table 5 . 
the sensitivity of mammography and mr imaging did not significantly differ in the two groups of fatty or nonfatty breasts ( mcnemar test )  . discussion this study showed that if the pathological examination of il numero totale di veri positivi e falsi negativi per tipo istologico e riconoscibilit alle modalit di imaging riportato in tabella 4 . 
 la sensibilit combinata della mammografia e della rm per i 26 dcis della nostra serie risultata del 46% ( 12 / 26 )  . il 54% ( 14 / 26 ) dei dcis risultato quindi falsamente negativo ad entrambe le modalit di imaging . 
i 10 dcis per le quali non era disponibile il diametro allistopatologia erano : 3 veri positivi ad entrambe le modalit di imaging ; 4 falsi negativi ad entrambe le modalit di imaging ; 2 falsi negativi alla mammografia e veri positivi alla rm e un vero positivo alla mammografia e falso negativo alla rm . la sensibilit di entrambe le modalit di imaging per i due sottogruppi di densit mammografica riportata in tabella 5 . 
non sono state osservate differenze significative tra la sensibilit della mammografia e quella della rm sia nelle mammelle con pattern adiposo che in quelle con pattern non adiposo ( test di mcnemar )  . discussione il presente studio ha evidenziato che , allorquando il reference standard istopatologico sia costituito dallintera mammella , si osserva una bassa sensibilit per i dcis sia per la mammografia ( 35% ) che per la rm ( 38% ) , come pure per le due modalit integrate ( 46% )  . in questa esperienza le dimensioni delle lesioni rappresentano probabilmente il fattore principale nella determinazione della riconoscibilit dei dcis sia alla mammografia che alla rm . 
infatti , mentre nel nostro studio le dimensioni allistopatologia ( disponibili per solo 16 delle 26 lesioni della serie ) erano 8.79.8 mm ( mediana 5.0 mm ) , altri autori hanno descritto lesioni non invasive con dimensioni sensibilmente pi elevate che possono quindi spiegare le maggiori sensibilit ottenute [ 14 , 20 , 27 , 28 , 36 , 46 ]  . 
hanno descritto una serie di dcis con diametro medio di 55.1 mm , ottenendo una sensibilit dell87% per la rm e del 77% per la mammografia [ 14 ] mentre gilles et al . 
in fact , whereas in our study lesion size at pathology ( available for only 16 of the 26 lesions ) was 8.79.8 mm with a median of 5.0 mm , other authors reported series of larger lesions , which can explain the higher sensitivity obtained [ 14 , 20 , 27 , 28 , 36 , 46 ]  . 
described a series of dcis with a mean diameter of 55.1 mm , reporting a sensitivity of 87% for mr imaging and 77% for mammography [ 14 ] , whereas gilles et al . 
nella nostra serie nel 50% ( 7 / 14 ) delle mammelle e delle pazienti si osservata malattia multifocale ( 2 / 14 , 14% ) o multicentrica ( 5 / 14 , 36% )  . 
 ( 37% di lesioni non invasive multicentriche ) in un analogo contesto clinico ( mastectomie di pazienti con tumori invasivi ) [ 54 ]  . la sensibilit della mammografia per dcis ritenuta tra il 27% e 78% , quella della rm tra il 20% e il 95% , sebbene tali dati derivino per lo pi da studi nei quali il reference standard istopatologico non costituito dallintera mammella [ 1520 , 2731 , 3345 , 53 , 5557 ]  . 
tuttavia , nella nostra esperienza con referadiol med ( 2008 ) 113 : 439451 36 dcis studied with mr imaging , with a mean lesion size of 45 mm [ 36 ]  . 
whereas holland et al , found that most cases of dcis were not multicentric ( only one multicentric lesion in their radiologic - pathologic correlation study of 119 mastectomy specimens from patients with dcis ) [ 51 ] , other studies reported percentages of multicentric or multifocal dcis in breast specimens between 8% and 36% [ 52 , 53 ]  . 
 ( 37% of multicentric dcis ) in a similar clinical setting ( mastectomy specimens of patients with invasive cancers ) [ 54 ]  . for dcis , the sensitivity of mammography is considered to be between 27% and 78% and that of mr imaging between 20% and 95% , although in most studies , detection by imaging modalities is not defined on the basis of a wholebreast histopathology as a reference standard [ 1520 , 2731 , 3345 , 53 , 5557 ]  . 
however , in our series , using the whole breast as a pathological reference standard , microcalcifications did not make the difference : they were present only in four of the 9 lesions diagnosed with mammography . 
 three main factors should be taken in account for the depiction of dcis on mr imaging : spatial resolution , enhancement morphology and distribution ( pattern ) , and enhancement kinetics . 
reported a relatively high detection rate of dcis with breast mr imaging , with 70% of dcis seen on mammography identified at mr imaging with a high - resolution , inversion - recovery , prepared - pulse sequence [ 27 ]  . according to other authors , dcis may be accurately depicted by mr imaging in 95% of cases , compared with 70% on mammography , using a high - resolution dedicated sequence , i.e. 
high spatial resolution also appears to be preferable to define the different enhancement patterns reported for dcis ( focal , diffuse , ductal - linear or branching ) , and this point represents a limit of our study , even though we used current imaging protocols [ 27 , 29 , 39 , 42 , 43 , 58 - 62 ]  . enhancement kinetics is the third factor for depicting dcis at mr imaging . 
reported only a 20% mr imaging sensitivity for dcis using the presence of washout ( type 3 curve ) ; however , sensitivity increased to table 5 sensitivity of mammography and mr imaging breast density fatty non - fatty total sensitivity mammography mr imaging 50% ( 5 / 11 ) 24% ( 4 / 15 ) 35% ( 9 / 26 ) 54% ( 6 / 11 ) 24% ( 4 / 15 ) 38% ( 10 / 26 ) tabella 5 sensibilit della mammografia e della rm secondo la densit mammaria densit mammaria sensibilit mammografia adiposa non adiposa totale 50% ( 5 / 11 ) 24% ( 4 / 15 ) 35% ( 9 / 26 ) 54% ( 6 / 11 ) 24% ( 4 / 15 ) 38% ( 10 / 26 ) rence standard istopatologico sullintera mammella , le microcalcificazioni non fanno la differenza , essendo presenti in solo 4 delle 9 lesioni rilevate alla mammografia . 
hanno osservato una sensibilit per dcis relativamente elevata con tecnica rm ad alta risoluzione spaziale e impulso preparatorio inversion - recovery : il 70% dei dcis rilevati alla mammografia erano riconosciuti alla rm [ 27 ]  . 
altri autori riportano una sensibilit per dcis della rm con sequenza dedicata ( rotating delivery of excitation off - resonance ) ad alta risoluzione spaziale pari al 95% in confronto al 70% della mammografia [ 37 ]  . 
una risoluzione spaziale elevata sembra essere pi adeguata alla definizione dei differenti quadri morfologici dellenhancement riportati per il dcis ( focale , diffuso , duttale - lineare o con biforcazioni )  . 
questo aspetto rappresenta un limite del nostro studio , sebbene sia stato condotto secondo protocolli di imaging attualmente in uso [ 27 , 29 , 39 , 42 , 43 , 5862 ]  . 
hanno riportato una sensibilit della rm per i dcis limitata al 20% utilizzando la presenza di washout ( curva di tipo 3 ) ; tuttavia , la sensibilit giungeva al 60% se anche le curve con plateau ( tipo 2 ) erano considerate sospette [ 63 ]  . 
the level of enhancement was associated with lesion size and density packing of dcis - involved ducts , and the two mr - undetected cases were pathologically demonstrated to have weak tumour angiogenesis around the ducts involved by the dcis [ 36 ]  . 
an earlier study demonstrated that the mean microvessel size was higher in dcis tissue than in normal gland tissue , suggesting that contrast enhancement is to be related to tumour angiogenesis in stroma surrounding dcis - involved ducts [ 64 ]  . 
 in our study , the morphological appearance was equally distributed between round , oval , or lobular ( 6 / 10 ) and linear , dendritic , or stellate ( 4 / 10 ) ; moreover , 90% ( 9 / 10 ) of the mr - detected lesions demonstrated early enhancement > 100% , whereas 80% ( 8 / 10 ) of them presented a washout kinetic pattern . 
 in the presence of nonfatty breasts , the sensitivity of mammography versus mr imaging for invasive cancers and dcis is significantly reduced , as already shown in the previously published general results of our multicenter trial [ 48 ]  . 
however , in the subgroup of the dcis considered in the current study , mr imaging did not provide better results compared with mammography , even in nonfatty breasts . this result is probably related to the combination of small size and low neoangiogenesis of the undetected dcis . 
in fact , in the subgroup of patients here considered , frequency and characteristics of dcis could substantially differ from those of the general population or those of patients with mammographically detected dcis . 
however , the data here reported offer an evaluation of dcis from a different point of view , the whole - breast pathology , from that usually presented in the literature , i.e. 
in fact , pooling together the 31 dcis detected in six prospective studies in high - risk women [ 6570 ] , we have a sensitivity of 17 / 31 ( 55% ) for mammography versus 20 / 31 ( 65% ) for mr imaging [ 71 ]  . 
in three studies in which clinical breast examination , mammography , us , and mr imaging were used [ 67 , 69 , 70 ] , only three of 83 cancers were detected solely by mammography ( 4% ) , all of them being dcis . 
in the study by kuhl et al . , eight of nine dcis were diagnosed with mr imaging ( the false negative was detected but misdiagnosed as probably benign ) , three with mammography and none with us [ 69 ]  . 
 in other words , when entry criteria other than mammographic detection are used , the sensitivity of mammography decreases , as occurred in our study in which the wholebreast pathological examination served as a reference stanla lesione e alla densit dellinteressamento duttale ; i due casi non visibili alla rm erano caratterizzati istologicamente da debole angiogenesi tumorale intorno ai dotti interessati dal dcis [ 36 ]  . 
uno studio precedente aveva dimostrato che le dimensioni medie dei microvasi sono pi alte nel tessuto con dcis rispetto a quello ghiandolare normale , suggerendo che lenhancement da correlare allangiogenesi tumorale nello stroma che circonda i dotti interessati dal dcis [ 64 ]  . 
 nel nostro studio laspetto morfologico risultato equamente distribuito tra rotondeggiante - ovalare ( 6 / 10 ) e lineare o stellato ( 4 / 10 ) e il 90% ( 9 / 10 ) delle lesioni riconosciute alla rm presentava enhancement iniziale superiore al 100% mentre l80% ( 8 / 10 ) presentava washout ( curva di tipo 3 )  . 
nelle mammelle non adipose , la sensibilit della mammografia per lesioni neoplastiche invasive o dcis significativamente ridotta rispetto a quella della rm , come gi dimostrato nei risultati generali dello studio multicentrico gi pubblicati [ 48 ]  . 
infatti , nel sottogruppo di pazienti qui considerate , frequenza e caratteristiche dei dcis potrebbero differire sostanzialmente da quelle della popolazione generale o da quelle con dcis riconosciuti alla mammografia ( o alla rm )  . 
tuttavia , i dati qui riportati possono essere unutile finestra sui dcis da un differente punto di vista rispetto a quello usualmente presentato in letteratura , ovvero la diagnosi mammografica . 
infatti , combinando insieme i 31 dcis diagnosticati in sei studi prospettici in donne ad alto rischio [ 6570 ] , otteniamo una sensibilit pari a 17 / 31 ( 55% ) per la mammografia versus 20 / 31 ( 65% ) per la rm [ 71 ]  . 
nei tre studi nei quali sono state eseguite visita clinica , mammografia , ecografia e rm [ 67 , 69 , 70 ] , su un totale di 83 tumori , solo 3 sono stati riconosciuti alla sola mammografia ( 4% ) , risultati dcis allesame istopatologico . 
nello studio di kuhl et al , su 9 dcis , 8 sono stati diagnosticati con rm ( il falso negativo era stato evidenziato ma caratterizzato come probabilmente benigno ) , tre con mammografia e nessuno con ecografia [ 69 ]  . 
 in altri termini , allorquando si utilizzino criteri di selezione differenti dalla diagnosi mammografica , la sensibilit della mammografia si riduce , come accaduto in questo studio nel quale il reference standard istopatologico era costituito dallintera mammella . 
this opinion has been recently confirmed by a large observational study considering 167 women who had undergone mammography and mr imaging and received a final diagnosis of pure dcis [ 72 ]  . 
moreover , of the 89 high - grade dcis , 43 ( 48% ) were missed at mammography but diagnosed with mr imaging ; on the other hand , mr imaging diagnosed 87 ( 98% ) high - grade dcis , the two missed cases having been diagnosed by mammography . the second limitation of our study is due to the interpretation setting : offsite consensus reading by two observers aware of the entry criterion ( planned mastectomy )  . 
a fourth limitation is the small number of dcis , although the wholebreast pathology as a reference standard partly compensates for this problem . in conclusion , in a series of 99 mastectomies , the sensitivity for dcis of mr imaging for was low ( 38% ) and not significantly different from that of mammography ( 35% ) , both techniques being compared with the whole - breast pathology as a reference standard . 
as a consequence , the sensitivity of mammography and mr imaging for dcis appears to be generally overestimated in studies not using whole - breast pathology as a reference standard . 
inoltre , degli 89 dcis ad alto grado istologico , 43 ( 48% ) sono risultati falsi negativi alla mammografia e veri positivi alla rm ; la rm ha diagnosticato 87 dcis ad alto grado ( 98% ) con i rimanenti due diagnosticati dalla mammografia . 
 un secondo limite del nostro studio dato dalla particolare modalit di lettura delle indagini : lettura centralizzata da parte di due osservatori in consenso , informati del criterio di selezione ( pazienti candidate alla mastectomia )  . 
occorre infine considerare il ridotto numero di lesioni che limita il valore dei risultati , parzialmente compensato dallutilizzo del reference standard riferito allintera mammella . in conclusione , su una serie di 99 mastectomie che hanno costituito il reference standard istopatologico , la sensibilit della rm per dcis risultata bassa ( 38% ) e non significativamente differente rispetto a quella della mammografia ( 35% )  . 
le ridotte dimensioni delle lesioni , determinanti sia la visibilit , sia probabilmente la neoangiogenesi , verosimile costituiscano il fattore principale alla base della riconoscibilit per entrambe le modalit di imaging . 
torricelli1 1cattedra e servizio di radiologia 1 , dipartimento di servizi diagnostici e per immagine , 2cattedra e servizio di cardiologia , dipartimento di emergenza - urgenza , azienda ospedaliero - universitaria policlinico di modena , universit degli studi di modena e reggio emilia , via del pozzo 71 , 41100 modena , italy correspondence to : g . 
we compared 3 - tesla ( 3 - t ) and 1.5 - tesla ( 1.5 - t ) cardiac magnetic resonance imaging ( mri ) for the assessment of myocardial viability in nearly identical experimental conditions . 
thirty - five patients ( mean age 6311 ; 94.2% men ) submitted to primary coronary angioplasty underwent both 3 - t and 1.5 - t cardiac mri , which was considered the gold standard . 
comparison was performed on the basis of the same viability imaging protocol , which included resting cine - mr [ balanced fastfield echo ( b - ffe ) sequence ] followed by contrastenhanced mr to evaluate perfusion and delayed enhancement ( de )  . 
confrontare la risonanza magnetica ( rm ) cardiaca a 3 tesla ( 3 t ) con quella a 1 , 5 tesla ( 1 , 5 t ) per la valutazione della vitalit miocardica in condizioni sperimentali essenzialmente identiche . 
trentacinque pazienti ( et media di 6311 ; 94 , 2% maschi ) dopo essere stati sottoposti ad angioplastica primaria sono stati esaminati sia con rm cardiaca a 3 t che rm cardiaca a 1 , 5 t , che stata considerata il gold standard . 
il confronto stato effettuato basandosi sullo stesso protocollo di imaging di vitalit che includeva : cine - mr a riposo ( sequenza b - ffe ) seguito da somministrazione di contrasto per la valutazione della perfusione e dellenhancement tardivo ( de )  . 
la rm a 3 tesla ha dimostrato una alta concordanza con quella a 1 , 5 tesla riguardo alla valutazione dei parametri funzionali e di vitalit con una pi cospicua evidenza del miocardio danneggiato . parole chiave risonanza magnetica cuore qualit immagine introduction introduzione magnetic resonance imaging ( mri ) is of increasing importance in cardiovascular medicine . 
heart function is commonly evaluated by bright - blood steady - state sequences obtained during a few seconds of breath - hold , which are used to acquire short - axis cine views of the entire left ventricle ( lv ) [ 1 ]  . 
the study of viability with de imaging relies on several inversion recovery sequences that permit one to suppress the signal of healthy myocardium to maximise the contrast between normal and necrotic tissue . 
besides myocardial viability , contrast - enhanced perfusion imaging also allows detection of the resting perfusion defect known as the no reflow phenomenon , which is currently considered a negative prognostic factor in the settings of ventricular remodelling . 
3 tesla ( 3 t ) to research settings expecting an improvement in signal to noise ratio ( snr ) due to higher signal intensity ( si ) and reported improved delineation of anatomical brain structures and vessels [ 5 , 6 ]  . 
preliminary phantom and volunteer data support those expectations , but the extent to which doubling of the static magnetic field improves or benefits routine clinical practice is still an open question [ 7 ]  . the aim of this study was to compare 3 - t with 1.5 - t cardiac mri , the latter being considered the gold standard , in nearly identical experimental conditions . 
in the comparison , both clinical ( myocardial function measurement and viability assessment ) and image - quality parameters [ snr and contrast to noise ratio ( cnr ) ] were taken into account . 
 la risonanza magnetica ( rm ) cardiaca di crescente importanza nella medicina cardiovascolare ed largamente riconosciuta come una metodica accurata e affidabile per la valutazione della funzione e dellanatomia del cuore e dei grossi vasi . 
la funzione cardiaca correntemente valutata mediante sequenze steady state a sangue bianco , ottenute mediante apnee di pochi secondi , che sono utilizzate per acquisire immagini in movimento in asse corto dellintero ventricolo di sinistra ( vs ) [ 1 ]  . 
lo studio della vitalit con limaging di de dipende da sequenze di inversione che permettono di annullare il segnale del miocardio sano per enfatizzare il contrasto tra tessuto normale e tessuto necrotico . 
oltre alla vitalit miocardica , limaging di perfusione permette di individuare dei difetti di perfusione a riposo ( fenomeno del no - reflow ) , considerati attualmente fattore prognostico negativo nellinsorgenza di rimodellamento ventricolare . recentemente , luso di alti campi magnetici ( 3 t ) stato impiegato in ambito di ricerca neuroradiologico per latteso miglioramento del snr dovuto allaumento della intensit di segnale ( si ) risultante in una miglior definizione delle strutture e dei vasi [ 5 , 6 ]  . 
dati preliminari su fantocci e volontari sani hanno supportato tali ipotesi , ma la questione ancora aperta quanto migliori , o pi specificamente , quanto sia il beneficio nella pratica clinica dato dal raddoppio del campo magnetico statico [ 7 ]  . lo scopo di questo studio di paragonare la rm a 3 t con la rm a 1 , 5 t , considerata come gold standard , in condizioni sperimentali essenzialmente identiche . 
nel confronto sia i parametri clinici ( funzione ventricolare e valutazione di vitalit ) che di qualit di immagine ( rapporto segnalerumore , snr , e rapporto contrasto - rumore , cnr ) sono stati presi in considerazione . radiol med ( 2008 ) 113 : 347362 materials and methods materiali e metodi patient population and study protocol popolazione e protocollo di studio cardiac mri was performed to evaluate the extent and transmurality of infarction and the presence of microvascular obstruction in 35 consecutive patients treated successfully with percutaneous transluminal coronary angioplasty ( ptca ) for acute myocardial infarction . 
inclusion criteria were age > 18 years , angiographically proven coronary artery disease that had been successfully treated , clinically documented myocardial infarction [ creatinine kinase isoenzyme muscle - brain ( ckmb ) peak > 50 ] and sinus rhythpatients with severe valve disease , unstable coronary artery disease , pacemakers or intracranial clips were excluded . 
each patient gave informed consent to the study protocol , which was approved by the local ethics committee . la rm cardiaca stata effettuata per valutare lestensione e la transmuralit dellinfarto e la presenza di ostruzione microvascolare in 35 pazienti consecutivi dopo efficace procedura di angioplastica coronarica ( pca ) , effettuata dopo infarto miocardico acuto . 
 data acquisition acquisizione dei dati a 1.5 - t intera mri scanner and a 3 - t intera mri scanner ( philips medical systems , best , the netherlands ) , both equipped with quasar gradients , were used . 
the study protocol did not differ between the two scanners and consisted of cine mri at rest to evaluate regional and global lv function and volumes followed by sono state utilizzate una rm 1 , 5 t intera ed una rm 3 t intera ( philips medical systems , best , olanda ) con gradienti quasar . 
depending on heart size , 1012 cine short - axis views were imaged from apex to base with a sensitivity - encoded balanced fastfield echo ( b - ffe ) sequence . 
the same sequence was repeated in the two - chamber long - axis and four - chamber long - axis views . perfusion imaging was evaluated in four different shortaxis planes by means of a ffe sequence after bolus injection of 0.1 mmol / kg gadoterate meglumine ( gadoliniumdota , dotarem , guerbet sa , cedex , france ) administered at a rate of 4 ml / s and flushed by 20 ml of saline . 
the inversion time ( ti ) permitting complete suppression of normal myocardium signal was individually adapted and selected using a look - locker sequence that acquires images with 2328 different inversion times depending on the patients heart rate . 
lv volumes were quantified using the simpson rule by direct summation of areas after endocardial and epicardial contour tracing in end - diastolic and end - systolic phases on each tomographic slice ; this has been shown to be the most reliable and reproducible approach [ 8 ]  . 
 cine mris were also visually evaluated using a 17 - segment model , as previously described [ 9 ] , and each segment was assigned a wall - motion score on a 5 - point scale : 0 ( normal wall motion ) , 1 ( mild hypokinesia ) , 2 ( severe hypokinesia ) , 3 ( akinesia ) and 4 ( dyskinesia )  . 
perfusion and de images were also scored visually using the same 17 - segment model as used for kinetic analysis and a 5 - point studio con contrasto per determinare la presenza e lestensione di difetti di perfusione e di aree infartuate . 
la stessa sequenza stata poi ripetuta sul piano asse lungo due camere e asse lungo quattro camere . limaging di perfusione stato valutato a quattro differenti livelli in asse corto cardiaco mediante una sequenza ffe dopo somministrazione di gadolinio 0 , 1 mmol / kg ( gadolinium - dota , dotarem , guerbet s.a. , cedex , francia ) ad un flusso di 4 ml / s seguito da 20 ml di soluzione fisiologica . 
il tempo di inversione ( ti ) che determinava la completa soppressione del segnale del miocardio stato adattato e selezionato individualmente utilizzando una sequenza ( look locker ) che permette di acquisire le immagini con 2328 tempi di inversioni differenti a seconda della frequenza cardiaca del paziente . 
la durata media dellesame stata 4311 minuti a 1 , 5 t e 4015 minuti a 3 t . analisi dei dati entrambi gli esami effettuati a 1 , 5 t e 3 t sono stati analizzati su una console di rielaborazione off - line ( viewforum 3.2 , philips medical systems , best , olanda )  . 
i volumi del vs sono stati quantificati utilizzando la regola di simpson derivata dalla somma diretta delle aree dopo disegno dei contorni endocardici ed epicardici in fase telesistolica e telesiastolica in ogni fetta acquisita . 
la detection dei bordi endoed epicardici stata effettuata con un approccio di riconoscimento automatico seguito da correzione manuale degli errori ; i muscoli papillari sono stati considerati parte della cavit ventricolare sinistra . le immagini cine rm sono state valutate anche visivamente utilizzando un modello a 17 segmenti del cuore come descritto in precedenza [ 9 ] e ad ogni segmento stato assegnato un punteggio di motilit utilizzando una scala a 5 punti : 0 ( normocinesi ) , 1 ( lieve ipocinesi ) , 2 ( ipocinesi severa ) , 3 ( acinesi ) a 4 ( discinesi )  . 
fa , ( flip angle ) value is expressed in degrees and slice thickness ( st ) in millimetres tr , ( tempo di ripetizione ) ; te , ( tempo di eco ) ; ti , ( tempo di inversione ) e pre - impulso ; tfe , di ritardo sono espressi in millisecondi . 
in particular , perfusion defect was defined as a hypoperfused myocardial region related to a coronary artery territory , with subendocardial or transmural distribution , evident on more than six consecutive images . 
a visual perfusion score was assigned to each segment as follows : 0 no hypoperfusion , 1 hypoperfusion of 1%25% of lv wall thickness , 2 hypoperfusion extending to 26%50% of lv wall thickness , 3 hypoperfusion extending to 51%75% of lv wall thickness , 4 hypoperfusion extending to 76%100% of lv wall thickness . 
each segment was also assigned a segmental scar score considering the transmural distribution of the hyperenhancement : 0 no hyperenhancement , 1 hyperenhancement of 1%25% of lv wall thickness , 2 hyperenhancement extending to 26%50% of lv wall thickness , 3 hyperenhancement extending to 51%75% of lv wall thickness , 4 hyperenhancement extending to 76%100% of lv wall thickness [ 10 ]  . 
the sum of the patients segmental scores yielded the patients overall perfusion score and scar score . segmentali del paziente ha portato al punteggio di cinesi complessivo ( che riflette la funzione o la disfunzione sistolico del paziente )  . 
in particolare il difetto di perfusione stato diagnosticato come presente se la regione miocardica ipo - perfusa era in relazione al territorio di distribuzione di una coronaria , con una distribuzione subendocardica o transmurale , evidente per almeno 6 immagini consecutive . 
il punteggio di perfusione stato assegnato ad ogni segmento come segue : 0 = assenza di ipoperfusione , 1 = ipoperfusione interessante il 1%25% dello spessore del vs , 2 = ipoperfusione interessante il 26%50% dello spessore del vs , 3 = ipoperfusione interessante il 51%75% dello spessore del vs , 4 = ipoperfusione interessante il 76%100% dello spessore del vs . 
the 3 - tesla magnetic resonance image on the left represents the estimation of signal intensity ( si ) within the ventricle cavity adjacent to the free wall in the end - diastolic phase . 
limmagine acquisita con rm a 3 t sulla sinistra rappresenta la misura dellintensit di segnale ( si ) allinterno della cavit ventricolare adiacente alla parete libera in fase tele - diastolica . 
la finestra dei risultati sulla destra dellimmagine mostra larea , le intensit di segnale medie , la deviazione standard , il valore minimo e massimo e lindice di circolarit di ogni roi . 
i risultati 14 esprimono rispettivamente lintensit di segnale dei segmenti miocardici anteriore , laterale , inferiore e settale ; i risultati 58 sono le intensit di segnale del sangue adiacente ; i risultati 912 esprimono le intensit di segnale delle roi 14 misurate in fase tele - sistolica . snr on ffe images was calculated through a freeware software ( rasband , w.s. , image - j , national institutes of health , bethesda , md , usa , 19972005 ) in a midventricular short - axis slice . 
mean si in four regions of interests ( rois ) of approximately 60 mm2 were measured within the lv myocardium , without including blood or epicardial fat , in the anterior , septal , inferior and lateral segments . 
noise was defined as the mean of the standard deviation ( sd ) of si measured inside each roi . to reduce sampling errors due to partial volume artefacts , measurements were repeated both in end - diastolic and endsystolic phases . 
cnr between myocardium and blood was also measured by subtracting from blood si ( siblood ) the mean of the myocardium si as measured in the four lv segments ( simyo ) divided by the square root of the sum of the square of noise measured inside blood and myocardiunoise was again considered as the mean of the enhancement , 1 = enhancement 1%25% dello spessore del vs , 2 = enhancement 26%50% dello spessore del vs , 3 = enhancement 51%75% dello spessore del vs , 4 = enhancement 76%100% dello spessore del vs [ 10 ]  . 
la somma degli score segmentali ha portato al punteggio di perfusione e di infarto complessivi . il snr nelle immagini ffe stato calcolato utilizzando un software gratuito ( rasband , w.s. , image - j , national institutes of health , bethesda , maryland , usa , 1997–2005 ) su una sezione in asse corto a livello medio - ventricolare : le medie dellintensit di segnale ( si ) sono state misurate in quattro regioni di interesse ( region od interest , roi ) di circa 60 mm2 nello spessore del muscolo cardiaco , senza includere sangue o grasso epicardico nei segmenti anteriore , settale , inferiore e laterale . 
cnr between infarction and normal suppressed myocardium was calculated by subtracting from the si of infarction ( siinfarct ) the mean of the myocardium si as measured in at least two adjacent ventricular segments ( sinormal ) in the same slice , divided by the square root of the sum of the square of noise measured inside damaged and healthy myocardiutherefore , the following formula was applied : cnr = siinfarct sinormal ( cid : 2 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) infarct n2 normal statistical analysis two radiologists ( rr , gl ) assessed cine , perfusion and viability images blinded to the clinical and coronary angiographic data . 
all patients had significant coronary artery disease on angiography ( > 70% reduction in luminal diameter of at least one major epicardial coronary artery ) treated with coronary angioplasty followed by stent implantation ( total number of stents = 48 )  . 
inoltre stato misurato il si del sangue in quattro roi di 60 mm2 posizionate nella cavit ventricolare in adiacenza alla prime quattro descritte . stato calcolato il cnr tra miocardio e sangue sottraendo dal si del sangue ( sisangue ) la media delle si del miocardio misurato nel quattro segmenti ( simio ) diviso la radice quadrata della somma del quadrato del rumore misurato nel sangue e nel miocardio ; il rumore stato nuovamente considerato come la media della deviazione standard del si misurata dentro le differenti roi . 
il cnr stato quindi calcolato sulla base della seguente formula : cnr = sisangue simio ( cid : 2 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) ( cid : 3 ) sangue n2 stato inoltre ripetuto il calcolo per la stima del snr e cnr nelle sequenze di perfusione e di enhancement tardivo . allo stesso modo nelle sequenze di perfusione , sono stati misurati lintensit di segnale del miocardio e del sangue intracavitario con roi della medesima ampiezza posizionate su fette medio ventricolari . 
solo nelle immagini di perfusione lintensit di segnale stata normalizzata al segnale di base . nelle immagini di de le si sono state misurate sulle regioni con enhancement ; il cnr tra la zona infartuata e di miocardio normale soppresso stata calcolata sottraendo dalla si dellinfarto ( siinfarto ) la media delle si del miocardio misurato in almeno due segmenti ventricolari adiacenti ( sinormale ) nella stessa fetta , diviso per la radice quadrata della somma del quadrato del rumore misurato nel miocardio infartuato e nel miocardio sano . 
de was detected in 255 segments with the following distribution : < 25% of lv wall thickness in 54 ( 21.2% ) ( 24 at 1.5 t , 30 at 3 t ) , hyperenhancement extending from 26% to 50% in 33 ( 12.9% ) ( 15 at 1.5 t , 18 at 3 t ) , hyperenhancement extending to 5175% in 66 ( 25.9% ) ( 34 at 1.5 t , 32 at 3 t ) and transmural hyperenhancement was identified in 102 ( 40% ) segments ( 49 at 1.5 t , 53 at 3 t )  . we found nonstatistically significant differences between the two scanners ( p = ns ) in measuring the following functional and viability parameters : ejection fraction , stroke volume , cardiac output , kinesis score , perfusion score , de score . 
tutti i pazienti erano portatori di malattia coronarica significativa alla coronarografia ( riduzione di pi del 70% del diametro luminale a carico di almeno una coronaria epicardica ) e sono stati trattati mediante angioplastica con impianto di stent ( numero totale di stent impiantati 48 )  . 
i pazienti sono stati randomizzati rispetto alla prima apparecchiatura di rm : 20 ( 57% ) sono stati sottoposti a rm 1 , 5 t prima e in seguito a rm a 3 t e i rimanenti ( 15 ; 43% ) sono stati sottoposti a rm a 3 t prima . 
non si sono verificati eventi cardiaci avversi maggiori ( morte , infarto miocardico ) come descritto in precedenza [ 11 ] e nessuno dei pazienti ha riportato dolore toracico o altro durante gli esami sia su 1 , 5 t che su 3 t . stato valutato un totale di 1190 segmenti , di cui 77 , 9% con cinesi nella norma . 
non abbiamo trovato differenze statisticamente significative tra le due apparecchiature ( p = ns ) nel calcolo di parametri funzionali e di vitalit , quali : frazione di eiezione , gittata sistolico , gittata cardiaca , punteggio di cinesi , punteggio di perfusione e punteggio di de . 
i risultati sono riassunti nella tabella 3 . riguardo alla qualit dimmagine , stato trovato che il snr del miocardico aumenta a 3 t del 61 , 5% ; in particolare esso era significativamente maggiore a 3 t sia in fase teledisatolica che in fase telesistolica : 0 , 6210 , 236 e 0 , 6560 , 120 vs 0 , 3950 , 128 e 0 , 3900 , 063 rispettivamente a 3 t e 1 , 5 t ( p < 0 , 05 )  . 
i valori di p sono non significativi per tutti i parametri la risonanza magnetica attualmente la metodica di scelta per il follow - up di pazienti sottoposti ad interventi terapeutici sulle coronarie [ 12 , 13 ] ; in particolare lo studio rm con contrasto sta rapidamente evolvendo come efficace strumento per predire la vitalit miocardica , dato che permette di distinguere il cambiamento regionale della funzione miocardica nellinsorgenza di rimodellamento ventricolare [ 14 ] e che gli studi di primo passaggio permettono una stima accurata dei difetti di perfusione [ 15 ]  . 
images in the upper row were acquired with a 1.5 - tesla ( t ) scanner , whereas those in the lower row were acquired with a 3 - t scanner . 
4 comparison between signal to noise ( snr ) and contrast to noise ratio ( cnr ) between blood and myocardium evaluated at 1.5 tesla ( t ) and 3 t in perfusion imaging . 
4 paragone tra il rapporto segnale - rumore ( snr ) e contrasto - rumore ( cnr ) del sangue e del miocardio misurati a 1 , 5 t e 3 t nelle immagini di perfusione . 
i dati sono espressi come valori medi delle misurazione nelle 4 regioni di interesse ( roi ) deviazione standard . snrmyo , rapporto segnale - rumore del miocardio ; snrblood , rapporto segnale - rumore del sangue ; cnrperf , rapporto contrasto - rumore a 1 , 5 t e 3 t . radiol med ( 2008 ) 113 : 347362 fig . 
during the first - pass study after injection of contrast agent , a subendocardial hypoenhanced area is evident in the inferior and inferolateral segments ( small arrows ) , consistent with a perfusion defect . 
during delayed - enhancement ( de ) imaging , performed 15 min after contrast injection , there is evidence of myocardial damage involving the same segments ( large arrows ) , which were assigned a de score of 2 . 
durante le immagini di perfusione ottenute dopo liniezione di mezzo di contrasto si evidenza unarea di ipo - enhancement in sede sub - endocardica a carico dei segmenti infero - laterali ( frecce piccole ) compatibili con difetto di perfusione . 
le immagini di enhancement tardivo , acquisite 15 minuti dopo liniezione di contrasto , evidenziano il danno miocardico coinvolgente gli stessi segmenti ( frecce grandi ) a cui stato assegnato un punteggio 2 . 
6 comparison between signal to noise ratio ( snr ) and contrast to noise ratio ( cnr ) between blood and myocardium evaluated at 1.5 tesla and 3 t in delayed - enhancement ( de ) imaging . 
at 3 t , there is a considerable increase in snr of the infarcted region ; cnr therefore increases more than threefold . data are expressed as mean values among measurements in the four different regions of interestone standard deviation . 
6 paragone tra il rapporto segnale - rumore ( snr ) e contrasto - rumore ( cnr ) del sangue e del miocardio misurati a 1 , 5 t e 3 t nelle immagini di enhancement tardivo . 
snrnormal , rapporto segnale - rumore del miocardio non infartuato ; snrinfarct , rapporto segnale - rumore del miocardio infartuato ; cnrde , rapporto contrasto - rumore a 1 , 5 t e 3 t . 358 discussion mri is the method of choice for longitudinal follow - up of patients undergoing therapeutic interventions on coronary arteries [ 12 , 13 ]  . 
in particular , contrast - enhanced mri is rapidly evolving as a means to accurately predict myocardial viability , as it enables one to discern regional heterogeneity of myocardial function in the setting of postinfarct remodelling [ 14 ] , and first - pass studies have provided an accurate estimation of perfusion defects [ 15 ]  . 
we also found de in a similar number of segments but with a different distribution , with a prevalence of segments scoring 34 ( enhancement extension greater than half of wall thickness ) and only few segments with a score of 1 ( less than 25% of wall thickness )  . the differences in de scores are unlikely due to an estimation error , as visual assessment of hyperenhancement transmurality was tested with schuijfs quantitative method , and the results showed an excellent agreement between the two methods [ 17 ]  . 
the greater number segments in the two lower quintiles can be explained by the success achieved by the pca procedure in that a smaller de reflects greater viability , as can be confirmed by dobutamine stress imaging [ 18 ]  . 
recently observed that current clinical practice and recommendations to postpone mri studies until 8 weeks after stent placement do not seem necessary with field strengths up to 1.5 t [ 11 ] ; our study suggests that this may also apply to a field strength of 3 t . 
these results suggest that ssfp sequences are efficient at higher field strength ( 3 t ) and allow us to postulate that a sufficient homogeneity of the static magnetic field has been achieved . this statement is supported by the fact that perfusion defects and areas of de can be detected with equivalent accuradiol med ( 2008 ) 113 : 347362 che tutti i pazienti inclusi in questo studio erano stati sottoposti ad una efficace procedura di rivascolarizzazione percutanea , mentre nel lavoro di kaandorp et al . 
nel nostro studio sono stati trovati un numero di segmenti infartuati , ma con una prevalenza di segmenti con punteggio di 3 o 4 ( estensione dellinfarto maggiore della met dello spessore ventricolare ) e solo pochi segmenti con punteggio di 1 ( meno del 25% dello spessore di parete )  . 
le differenze riportate nei punteggi di de , difficilmente sono dovute ad un errore di stima , in quanto la valutazione visiva della transmuralit dellinfarto stata dimostrata in ottima concordanza con i metodo quantitativo [ 17 ]  . 
il maggior numero di segmenti nel quintile inferiore spiegabile con il successo ottenuto mediante la procedura di angioplastica ; infatti un de minore in concordanza con una maggiore vitalit , come pu essere confermato dallimaging con stress dobutaminico [ 18 ]  . 
 [ 11 ] recentemente hanno riportato che non sembra essere necessario proporre nella pratica clinica quotidiana lo studio cardiaco con rm a 1 , 5 t dopo otto settimane dal posizionamento di stent ; questo studio suggerisce che lo studio cardiaco pu essere eseguibile anche a 3 t . inoltre limaging a 3 t mostra una alta correlazione con limaging a 1 , 5 t , nella valutazione della funzione e vitalit ventricolare . 
la rm a 1 , 5 t infatti considerata attualmente il gold standard per la misurazione dei volumi ventricolari , della frazione di eiezione grazie alla sua alta accuratezza e riproducibilit e alla superiore risoluzione di contrasto nei confronti dellecocardiografia [ 19 ]  . 
in particolare le sequenze ssfs permettono una definizione ottimale dei bordi endocardici del vs con la possibilit di utilizzare nel post - processing un metodo semiautomatico [ 20 , 21 ]  . questo articolo dimostra una sostanziale identit tra la stima dei parametri funzionali tra 1 , 5 e 3 t . 
i risultati riportati su una popolazione di 35 pazienti sono consistenti con quanto riportato in letteratura su volontari sani [ 22 ] e suggeriscono che le sequenze ssfp sono utilizzabili anche a campi magnetici alti ( 3 t ) permettendoci di affermare che stata ottenuta una omogeneit di campo magnetico sufficiente . 
questa affermazione supportata anche dal fatto che la diagnosi di difetti di perfusione ed il riconoscimento di aree di enhancement tardivo pu essere effettuata in modo equivalente a 3 t utilizzando le medesime sequenze . 
queste distorsioni sono dovute a minime disomogeneit del campo magnetico esterno che non sono correttamente annullate dal posizionamento dello shim , normalmente posto sul volume del cuore . allo stesso tempo , il 3 t permette di ottenere un pi alto snr del miocardio ( 61% in pi )  . 
il valore misurato per pi basso del valore teorico raggiungibile , dato che ci si radiol med ( 2008 ) 113 : 347362 racy at higher field strengths using identical sequences . curved black bands are almost constantly visible at the borders of 3 - t images , even though they do not affect image interpretation and quantitative measurements . 
the measured value is lower than the theoretical increase achievable at 3 t , as si is expected to increase fourfold with a corresponding doubling of noise with respect to 1.5 t [ 23 ]  . 
there are only few reports regarding myocardium snr changes at high magnetic field strengths : dougherty reported that the anterior myocardium snr at 4 t was 2.9 times higher than that of the same region at 1.5 t [ 24 ]  . 
first , t1 and t2 relaxation times are not affected by the increase in field strength in the same way , as t1 is prolonged but there is a nonproportional shortening of t2 [ 25 ]  . 
also , repetition time ( tr ) and consequently echo time ( te ) values need to be modified to increase the signal of blood and consequently obtain a better snr as measured inside ventricular cavities . unfortunately , these cannot be shortened excessively , for as is well known the main limiting factor at higher field strengths is the specific energy absorption rate ( sar ) [ 26 ]  . parallel imaging affects the possibility of correctly estimating snr and cnr variations at 3 t , as it is also well known that noise is not homogeneously distributed in the mr image if sensitivity encoding ( sense ) is applied . 
ci sono solo pochi lavori sulla variazione del snr del miocardio ad alto campo : dougherty ha riportato che il snr della parete anteriore del miocardio a 4 t era 2 , 9 volte pi alto di quello nella stessa regione a 1 , 5 t [ 23 ]  . 
la differenza tra il guadagno teorico ed attuale del snr pu essere spiegato da numerosi fattori : il primo tra i quali il fatto che i tempi di rilassamento t1 e t2 non sono ugualmente influenzati dallaumento del campo magnetico , dato che il t1 allungato senza un accorciamento proporzionale del t2 [ 24 ]  . 
tuttavia questi non possono essere accorciati troppo , siccome il limite maggiore ad alto campo la deposizione di energia sul paziente ( sar - specific energy absorption rate ) [ 25 ]  . 
limaging parallelo non permette per di stimare correttamente le variazioni di snr e cnr , dato che il rumore non distribuito in modo omogeneo sulla immagine di rm se il fattore sense applicato ; per superare questo problema sono state acquisite nel presente studio delle immagini con un fattore sense identico per le due apparecchiature e sono stati fatti pi campionamenti in regioni differenti del ventricolo . 
 luso dellimaging parallelo ( sense ) influenza la stima delle variazioni di cnr e snr : recentemente mc gee ha misurato i cambiamenti di snr e cnr del miocardio a 1 , 5 t e 3 t in fantocci e volontari [ 26 ] trovando che il raddoppio del campo magnetico incrementa il valore di snr e cnr di un fattore di 1 , 86 e 1 , 35 rispettivamente . 
inoltre nel suo studio , ha evidenziato come lutilizzo dellimaging parallelo con un fattore 2 decresce il snr e cnr di 2 , 65 e 2 , 05 a 1 , 5 t e 1 , 99 e 1 , 75 a 3 t rispettivamente . 
nel presente studio il fattore sense stato scelto a 1 , 6 in entrambe le apparecchiature : ci ha il vantaggio di accelerare lacquisizione del 60% ( significa che 2 fette in asse corto possono essere acquisite in 1015 secondi di apnea , in dipendenza dalla frequenza cardiaca ) senza la perdita di snr riportata da mc gee con un fattore sense di 2 . 
 la perdita di contrasto riscontrata nelle sequenze di perfusione difficile da chiarire ed in contrasto con la recente letteratura [ 2729 ] ; questi autori hanno trovato un in360 radiol med ( 2008 ) 113 : 347362 by mcgee using a sense factor of two . 
these reports found a substantial increase in myocardial enhancement in first - pass perfusion imaging over a range of different gadolinium doses . nonetheless , we were able to detect perfusion defects and correctly estimate their transmural extension . 
 if the same gadolinium dose is injected , the main advantage of 3 t is evident in de imaging , even though the same mri acquisition parameters as 1.5 t are used , with the exception of inversion time , which needs to be adapted . 
the more than threefold increase in infarcted tissue si and the comparable gain of cnr with respect to healthy myocardium is even higher than the theoretical gain ( 200% )  . 
to acquire the whole lv during a single breath - hold , de images were obtained by an inversion - recovery 3d gradient - echo sequence with a sense factor of two in both scanners . 
this may explain the increase in snr and cnr we reported . this statement has the limit that the values of snr and cnr presented were estimated on images acquired with 50% longer inversion time at 3 t and that the choice of the correct inversion time was arbitrary and based only on the visual determination of the time enabling the best suppression of normal myocardiuhowever , the increase in image quality is so evident that it cannot be attributed only to an erroneous estimation . 
the latter approach would probably result in advantages in first - pass imaging also , in which the highly concentrated gadolinium inside the ventricular cavity and subendocardial regions causes si loss at the interface due to susceptibility artefacts [ 30 ]  . cremento significativo dellenhancement del miocardio durante limaging di primo passaggio con un differente dosaggio di gadolinio . 
 se viene somministrata la stessa dose , il vantaggio maggiore del 3 t evidente nelle immagini di enhancement tardivo pur utilizzando gli stessi parametri di acquisizione dell1 , 5 t , con leccezione del tempo di inversione , che deve essere ottimizzato . 
lincremento di oltre tre volte della si del tessuto infartuato e il conseguente guadagno di cnr rispetto al miocardico sano molto maggiore anche rispetto al guadagno teorico ( 200% )  . 
per ottenere tutto il vs in una singola apnea , le immagini di de sono state acquisite con una sequenza inversion - recovery 3d gradient echo con fattore sense pari a 2 . 
luso dellimaging parallelo accorcia la durata della scansione a discapito del snr e cnr : queste perdite sono per compensate a 3 t , infatti pi alto il fattore sense per ridurre il sar ad alto campo pi i vantaggi di questo sono evidenti : questo pu essere il motivo dellincremento di snr e cnr che stato riportato . 
 questa ultima affermazione ha il limite che i valori di snr e cnr presentati sono stati valutati con un tempo di inversione pi lungo del 50% e la scelta del corretto tempo di inversione stata arbitraria , su base visiva della miglior soppressione del miocardio sano . 
questo vantaggio pu essere direzionato verso lacquisizione di immagini di de ad alta risoluzione ( usando una matrice pi alta ) o , in combinazione ad un fattore sense maggiore , riducendo la dose di gadolinio alla met ( es , 0 , 1 mmol / kg ) oppure entrambe . lultimo approccio probabilmente porta vantaggi anche nellimaging di perfusione al primo passaggio dove il gadolinio altamente concentrato dentro la cavit ventricolare e soprattutto nelle regioni subendocardiche responsabile della perdita dellintensit di segnale a livello dellinterfaccia per artefatti da suscettibilit magnetica [ 30 ]  . conclusioni conclusions this study shows that 3 - t cardiac mri provides nearly identical results to 1.5 t in evaluating cardiac function and viability . 
even though the ssfp sequence provided a substantial gain in myocardial snr at the higher field strength , the theoretical snr gain at 3 t is questo studio dimostra come la rm cardiaca a 3 t permetta di ottenere risultati similari a quelli ottenibili a 1 , 5 t nella valutazione dei parametri cardiaci di funzionalit e vitalit . 
 + 39 - 06 - 30154977 , fax : + 39 - 06 - 35501928 , e - mail : pmarano@sirm.org introduction introduzione in the italian health system , which , unlike those operating overseas , is based on equity and solidarity , clinicalradiological appropriateness in clinical radiology are not only real problems that confront us daily but are also innovative and demanding issues that are unfortunately constantly disregarded . 
in radiological practice , the exponential growth of knowledge and technologies clashes with a very different reality conditioned by a high number of inappropriate requests ( 50% or more useless examinations ) , waiting lists , and the cup ( the centro unico prenotazioni , or examination booking centre )  . 
as a result , amidst the total indifference of medical personnel and the general public , only the quantity , not the quality , of radiological examinations is really appreciated , and all appropriateness and pertinence requirements provided for by law no . 
this is the current paradox of italian radiology . is it preferable to ignore the problem , as occurs today , because its possible solution is complex , difficult , and demanding and may be detrimental to the personal interests of a few individuals ? do we really think that the solution to this highly specific problem lies in adopting recommendations that come to us from very different health care settings and therefore bear little relevance to our workplaces , are uncritically imposed on us from higher up , and are often outdated ? lappropriatezza clinica - radiologica e la radiologia clinica sono , in una sanit sociale e solidaristica come la nostra , diversa da quelloperante oltre oceano , problemi reali , attuali e quotidiani , ma anche innovativi ed impegnativi , purtroppo costantemente disattesi . 
infatti , nonostante le ben note disposizioni legislative della legge 187 sulla giustificazione e pertinenza delle indagini radiologiche [ 1 ] , la realt del medico radiologo italiano nella sua quotidiana attivit professionale completamente diversa . 
la crescita costante ed esponenziale delle conoscenze e delle tecnologie si scontra , nel concreto dellattivit radiologica quotidiana , con una realt profondamente diversa , condizionata da un numero elevato di richieste non appropriate ( 50% e pi desami inutili ) dalle liste dattesa e dal cup dove in sostanza valutato e valorizzato , nellindifferenza generale pi completa di tutti , medica e non , solo la quantit e non la qualit delle indagini , trascurando completamente tutte le problematiche dellappropriatezza e della pertinenza delle indagini radiologiche riportate nel dispositivo legislativo . questo contesto professionale non qualificante tende in concreto a ridurre e vanificare il ruolo scientifico , il prestigio professionale , il domani stesso della radiologia clinica . questo il paradosso attuale della radiologia italiana . preferibile trascurare questo problema , come di fatto avviene oggi , nascondendolo , tenendo il tutto sotto cenere , perch complesso , difficile , impegnativo e forse anche , per alcuni , lesivo dinteressi personali ? pensiamo sia pi che sufficiente avvalersi ed utilizzare solo indicazioni avulse dai propri ambiti di lavoro , che ci pervengono da contesti sanitari profondamente diversi dai nostri , imposte acriticamente dallalto e spesso anche datate nel tempo , per risolvere questo specifico problema ? 308 radiol med ( 2008 ) 113 : 307318 or should we , instead , perhaps undertake a critical and constructive analysis on the current significance of clinical radiology ? is radiology only a matter of machinery and technique , where the technical role markedly predominates over the clinical role ? what is the clinical role of radiology , and how is this role expressed in our daily practice ? to answer these questions , we need to reflect critically upon the education and professionalism of physicians and of radiologists in particular in the context of our constantly evolving society . 
help in this regard is provided by the meeting on doctorpatient communication in italy , which was organised by the censis biomedical research forum in july 2007 in rome [ 2 ]  . 
this was a highly relevant and welltimed meeting , given the need to consider whether or not communication difficulties in medicine and particularly in radiology are the result of a medical education that is lagging behind and unable to meet the changing needs of society . 
knowledge is necessary for an immediate impact on society and is no longer considered an end in and of itself but as a resource for economic growth : this is a utilitarian vision that is spreading and dominating in a host of fields , including scientific research and academic education . 
this kind of knowledge is not so much the object of reflection in the search for truth as the accumulation of notions capable if well arranged of generating innovations that can be exploited in practice . 
it follows that the knowledge society is increasingly also becoming an information society , as witnessed by the explosive development of the internet , with its use by the educationally lower - middle classes rising from 2.8% in 2003 to 13% in 2006 . 
such rapid evolution seems to contrast with the immobility of a university system that has always preached the unity of teaching and research and with regard to medical faculties patient care , a view grounded in the belief that separation of these three functions damages education and that a university can be considered as such only if it produces culture , operates within a cultural environment and is not merely a place where culture is transmitted [ 3 ]  . 
but is this belief still valid ? o forse necessario una riflessione critica costruttiva sul significato attuale della radiologia clinica ? la radiologia oggi solo macchina e tecnica con netta prevalenza del ruolo tecnico su quello clinico ? quale il suo ruolo clinico ? e come si esplica concretamente e praticamente questo ruolo clinico nella quotidiana attivit professionale ? rispondere a questi ultimi interrogativi significa riflettere criticamente sulla formazione e sulla professione del medico , del medico - radiologo in particolare , inserito oggi in una societ in costante evoluzione . 
in questo non semplice ed impegnativo approfondimento c valido supporto convegno che il censis forum per le ricerche biomediche ha organizzato nel luglio 2007 a roma sulla comunicazione medico - paziente nella societ italiana [ 2 ]  . 
convegno oltremodo opportuno data la necessit di riflettere se la difficolt a comunicare in medicina , in radiologia in particolare , sia , o no , la conseguenza di una formazione medica in ritardo rispetto alle trasformazioni di una societ che va mutando le proprie esigenze . 
stiamo vivendo la trasformazione da una societ della produzione ad una societ del servizio che privilegia il lavoro intellettuale rispetto al manuale e che , di conseguenza , esprime una forte richiesta di conoscenze . 
ma non soltanto : si vuole anche che la conoscenza abbia un immediato impatto sociale ; essa non appare pi come un traguardo , ma come una risorsa diretta alla crescita delleconomia . 
a tale tipo di conoscenza non interessa tanto la riflessione intellettuale per la ricerca del vero , quanto lacquisizione di una massa dinformazioni capaci , se bene organizzate , di produrre novit praticamente utilizzabili . 
ne segue che la societ della conoscenza sta sempre pi divenendo anche una societ dellinformazione , e ne testimone il tumultuoso sviluppo dinternet , il cui utilizzo passato nei ceti secolarmente medio - bassi dal 2 , 8% del 2003 al 13% nel 2006 . 
nella convinzione che la separazione di queste funzioni nuoccia alla formazione culturale , mentre luniversit pu dirsi tale solo se crea e produce cultura , se opera in un ambiente di cultura e non se costituisce un semplice luogo in cui simmette cultura [ 3 ]  . 
ma questa convinzione ancora valida ? humboldts idea lidea di humboldt the first to formulate the concept of unity of research , teaching and patient care in academic medical education was wilhelm von humboldt ( not his brother alexander , who was a naturalist and an explorer ) , a prussian minister , the founder of berlin university , and an expert on education and teaching [ 4 ]  . 
his view dominated in the second half of the nineteenth century , when most european universities adopted the german model prompted by the excellent fu wilhelm von humboldt ( e non il fratello alexander , naturalista ed esploratore ) , ministro prussiano , fondatore delluniversit di berlino , esperto deducazione ed istruzione [ 4 ] , a formulare per primo lidea di uninscindibilit fra ricerca , didattica ed assistenza nella formazione medica universitaria . 
lidea si imposta nella seconda met dell800 , che ha visto ladeguarsi della maggior parte delle universit europee al modello tedesco , nella scia del gran prestigio , in tutti i campi , della germania guglielmina . radiol med ( 2008 ) 113 : 307318 reputation enjoyed by germany at the time of emperor wilhelm ii . 
patient care was influenced by the need to recruit patients best suited to the research being carried out , so that the care delivered in academic centres had a different connotation from that delivered in hospital facilities , a difference that has gradually disappeared . 
all of we senior professors can still remember the fascination exerted by the lectures of scholars , profound thinkers and skilled communicators who , precisely because they lectured on subjects they were passionate about and pursued as scientists , succeeded in transmitting their enthusiasm and stimulating their students spirit of emulation . 
although my experience as a university professor and faculty dean [ 5 , 6 ] has turned me into a strong supporter of student - centred teaching , i have also realised that despite the greater commitment required of teachers , student - centred teaching sometimes involves a colder , more impersonal and bureaucratic , approach to teaching . 
 however , what we should be considering is whether the unity of teaching , research and patient care is still viable and appropriate at a time when research tends to move away from universities and escape the control of the academic teaching staff . 
unlike traditional academic research , so - called research and innovation a reflection of new social needs tends to become all absorbing on account of its complexity , rapid changes , high running costs and the consequent active involvement of industry . 
 there is a need to clarify the relationships between new approaches in research , teaching and patient care , on the one hand , and their impact on education and professionalism , on the other . 
if we allow the basic misunderstanding to persist , we risk compromising or even thwarting valuable national initiatives taking place in the fields of education and patient care , which is , in fact , already happening . 
examples of such initiatives are the creation of the steering committee for research evaluation ( formerly civr , now anvur , that is , the national agency for the evaluation of the university system and research ) and the national committee for the evaluation of the university system ( cnvsu ) ; the redesigned curriculum for the schools of specialisation ; and the ministers recent proposals to address the university paradox [ 7 ] between a managerial autonomy without decision - making powers and decision - making powers with heavily limited managerial functions . 
 in questo inscindibile trinomio la ricerca ha fatto per lungo tempo la parte del leone e luniversit ha finito per essere percepita , anche dallopinione pubblica , come il luogo per eccellenza della ricerca scientifica . 
ci ha fortemente influenzato , in medicina , anche la didattica e lassistenza : la didattica divenendo teacher centred con docenti sempre pi orientati a coltivare ed esporre gli argomenti corrispondenti ai propri interessi scientifici ed unassistenza condizionata dallopportunit di reclutare i pazienti meglio adatti alle ricerche e studi in corso ; il che contribuiva a conferire allassistenza nei centri universitari una connotazione diversa da quella praticata nei centri ospedalieri , differenza che si persa , anzi completamente scomparsa , nel tempo . non si deve pensare che questi orientamenti siano stati inefficaci . 
tutti noi anziani ricordiamo la profonda suggestione esercitata dalle lezioni tenuteci da maestri , profondi nel pensare ed abili nellesporre che , proprio perch parlavano degli argomenti che li appassionavano e coltivavano scientificamente , sapevano trascinare gli studenti allentusiasmo e , comunicando qualcosa del proprio fuoco , stimolarne il desiderio demulazione . 
chi scrive si convinto , nella sua esperienza di docente e di preside [ 5 , 6 ] della preminente importanza della didattica student centred ; ma ha potuto avvertire anche come in essa , pur in presenza di un necessario maggior impegno del docente vi sia talvolta qualcosa di pi freddo , impersonale e burocratico rispetto al passato . quello che per dobbiamo chiederci : questi orientamenti sono ancora possibili ed opportuni oggi , in tempi nei quali la ricerca tende a svincolarsi dalle universit e a sottrarsi al controllo stesso degli universitari ? la cosiddetta ricerca e innovazione , espressione di nuove istanze sociali , tende oggi per la sua complessit , per il suo rapido divenire , per gli elevati costi di gestione e conseguente coinvolgimento attivo dellindustria , a divenire omniassorbente , a differenza di quanto avveniva in passato con la tradizionale ricerca universitaria . bisogna far chiarezza sui rapporti fra nuovi orientamenti in campo di ricerca , didattica ed assistenza e successive ricadute formative e professionali ; se persiste lequivoco di base si rischia che iniziative valide in atto nello scenario nazionale , sia in ambito della formazione sia dellassistenza , possano essere fortemente penalizzate o vanificate , come di fatto avviene . 
cito , a titolo desempio , listituzione dei comitati dindirizzo per la valutazione della ricerca ( civr ora anvur , agenzia nazionale per la valutazione della ricerca universitaria ) e del sistema universitario ( cnvsu ) , il nuovo ordinamento delle scuole di specializzazioni e le stesse recenti proposte ministeriali finalizzate a modificare quel paradosso universitario [ 7 ] tra unautonomia gestionale che non ha potere decisionale ed un potere di decisione che ha limitatissime funzioni di gestione . 
 tutto ci pone unimpegnativa problematica che opportuno affrontare con unanalisi critica delle tre diverse funzioni , partendo dallequivoco culturale sulla ricerca , proprio dellattuale societ della conoscenza e dellinformazione , per spostarci poi sul ritardo culturale della for310 radiol med ( 2008 ) 113 : 307318 all of the above issues raise complex problems that need to be discussed through a critical analysis of the three functions of universities . 
in particular , we should start from the misunderstanding regarding research , which is specific to the knowledge and information society , and then move on to the cultural delay with respect to education and patient care the former mainly teacher - centred , the latter strictly based on economic - organisational requirements , and both probably still very far from the education and patient care demanded by modern society . 
 research and innovation : a threat to academic culture ? the expression research and innovation usually refers to studies funded by sponsors ( agencies or industry ; in medicine , often pharmaceutical and / or medical device companies ) , the objectives and programmes of which are mostly determined by the sponsors themselves , though in collaboration with the study investigators . 
research and innovation is a significant component of todays society and one that amidst the general indifference is paradoxically undermining the traditional scientific methods of education , the scientific nature of professional activity and the doctorpatient relationship . 
as further reading , i suggest a book presented at the milan meeting la ricerca tradita ( betrayed research ) [ 13 ] , as well as linnovazione nella tutela della salute , internet e territorio ( innovation in health protection , internet and the territory ) [ 14 ]  . 
 regarding the international literature , evidence that these problems are not exclusive to italy is provided by the wellknown charter on medical professionalism [ 16 ] published in the leading international medical journals ( but so far ignored ) , and by the icram ( international campaign to revitalise academic medicine ) challenge to the invisible mazione e della assistenza , tuttora prevalentemente teacher centred la prima e rigidamente impostata su esigenze economiche - organizzative la seconda , probabilmente entrambe lontane da quella formazione dello studente e da quella assistenza del paziente che i tempi moderni richiedono e rivendicano . 
 ricerca e innovazione : una minaccia alla cultura universitaria ? viene abitualmente definita ricerca e innovazione la ricerca commissionata da sponsors ( enti o industria : assai spesso , in campo medico , industrie farmaceutiche e / o produttrici di apparecchiature elettro - medicali ) , con obiettivi e programmi esecutivi prevalentemente determinati dallo sponsor ( anche se in collaborazione con chi esegue la ricerca ) , non necessariamente svolta nei soli centri universitari ( ma anche in centri di ricerca specializzati , in istituti di ricovero e cura a carattere scientifico , in importanti ospedali , ecc )  . ; spesso questa ricerca pluricentrica e coinvolge istituzioni di varia tipologia . 
essa rappresenta unimportante e significativa realt nellattuale societ , che paradossalmente sta penalizzando , nellindifferenza generale , la tradizionale metodologia scientifica della formazione , la scientificit dellattivit professionale e lo stesso rapporto medico - paziente . 
nel convegno di milano stato sottolineato che la ricerca da sempre tensione , vive da un lato di duro lavoro e dallaltro di lampi di genio che stravolgono continuamente il contesto delle conoscenze . 
a camerino stato precisato che la ricerca universitaria tradizionale da sempre una ricerca ad accesso completamente aperto , focalizzata sulla radiol med ( 2008 ) 113 : 307318 leaders of academic medicine [ 17 ]  . 
the camerino meeting instead stressed the point that traditional academic research has always been characterised by fully open access , focus on research methodology more than on results and mediumto long - term returns [ 11 ]  . 
in contrast , the kind of research promoted by research and innovation has restricted access , encouraged a prevalent focus on results and exploitability , provided significant economic returns , and is aimed at obtaining and exploiting patents ( spinoff ) more or less in the short term . research and innovation differs from traditional academic research in several other important respects . 
however , because it lacks the features typical of pure and disinterested enquiry , it differs from academic research in both substance and objectives . it is not that academia rejects the market . 
rather , it regards it as an instrument to test the feasibility of ideas , a place where innovative solutions are created that can be used by others as well . 
this is the only respect in which collaboration among universities does not exclude competition in the sense of competition of ideas rather than competition for funds and in this sense competition may even become the highest form of cooperation . 
failure to maintain this distinction and a lack of clarity and transparency about ideas or line of action will only lead to confusion ( and often conflict of interest ) regarding the core roles and functions of the university , with consequent cultural delay and penalisation of the component with lowest economic return ( that is , pure or basic research ) , which is obviously the traditional component of academic research . 
in fact , where researchers for the sake of gain become mere executors of projects set out by others , their dignity is damaged . it must be admitted that italy is currently witnessing a metodologia della ricerca stessa pi che sul suo risultato , con ricadute in tempi medio - lunghi [ 11 ]  . 
la ricerca e innovazione , al contrario una ricerca ad accesso rigidamente chiuso , focalizzata prevalentemente sul risultato e sulla sua fruibilit , a significativa ricaduta economica , che mira al brevetto e alla sua utilizzazione ( spin - off ) in tempi piuttosto brevi . vi sono anche altre caratteristiche che differenziano la ricerca e innovazione dalla ricerca universitaria tradizionale che meritano di essere qui sottolineate . 
queste ricerche che oggi fanno mercato sono ricerche di certo importanti nellattuale societ della conoscenza ; ma , mancando di quella caratteristica specifica propria della ricerca pura e disinteressata , sono ricerche sostanzialmente e finalisticamente diverse da quelle che da sempre qualificano e caratterizzano la ricerca universitaria . non che luniversit rifiuti il mercato , ma lo ritiene un mezzo per esplorare la fattibilit delle idee , un terreno in cui si creano soluzioni innovative che possono essere usate anche da altri . 
solo in questo senso la collaborazione tra universit non esclude la competizione , che gara didee e non lotta economica , e pu anzi divenire la pi alta forma di collaborazione . la ricerca e innovazione pu essere inserita anche nel contesto delle attivit delle strutture universitarie ; ma sempre e solo unattivit aggiuntiva che va distinta e non confusa dalla tradizionale attivit delle strutture universitarie ; se manca questa distinzione , se non c chiarezza e trasparenza di idee e di operato si crea solo confusione nei ruoli e nelle funzioni istituzionali delluniversit ( e spesso conflitti dinteresse ) , conseguente ritardo culturale e penalizzazione della componente a minor ricaduta economica ( la ricerca pura o di base ) che ovviamente la componente universitaria tradizionale . 
la sua dignit viene meno se per lucro egli diviene un mero esecutore di programmi messi a punto da altri . dobbiamo purtroppo constatare che oggi in italia si sta assistendo ad uno stravolgimento del significato dello scopo e delle finalit della ricerca universitaria , nellindifferenza generale del mondo accademico ( corporativismo ? incomprensione del cambiamento ? ) ed anche , cosa ancor pi preoccupante , degli stessi organi ministeriali e di qualificati osservatori esterni , editorialisti della carta stampata inclusi . 
sempre pi spesso oggigiorno si parla , nelle sedi pi diverse , solo ed esclusivamente di ricerca e innovazione . in questo nuovo contesto qual il significato attuale dellinscindibilit della ricerca dalla formazione e dalla assistenza e quale il ruolo e limportanza di tutta una tradizione orientata alla ricerca pura e disinteressata ? 312 radiol med ( 2008 ) 113 : 307318 subversion of the meaning , aim and purposes of academic research . 
and this is happening among the general indifference both of the academic world ( out of corporatism or inability to understand the change ? ) and even more disturbingly of ministry organs , qualified external observers , and editorialists . 
 but what , then , is the current significance of the unity of research , education and patient care in this new context ? and what is the role and value of a whole tradition focused on pure and disinterested research ? the delay of the culture of education perhaps on account of its involvement in the lucrative issues of research and innovation , the academic world has found itself largely unprepared , in epistemological and pedagogical terms , to redress the problems underlying the current cultural delay in medical education and professionalis from the epistemological point of view , there is a need to revise the current organisation of knowledge , which suffers excessive fragmentation into specialties and subspecialties , scientific - disciplinary areas , and scientific associations [ 12 ]  . 
for example , although the existence of 350 or more academic scientific - disciplinary areas is just about justified by the number of research specialties , it appears absolutely excessive ( as well as possibly clannish and partisan ) in relation to the requirements of providing basic knowledge and designing adequate curricula . 
this will also prevent excessive fragmentation that , though no doubt useful to expand and organise scientific knowledge , is inadequate for managing and understanding the complexity of single professional activities ( clinical practice )  . 
the review should aim to promote course planning , which involves not only setting objectives that are both relevant to needs and consistent with results , but also an epistemological reflection on the content of the disciplines being taught and on their educational and professionalizing purposes . 
nowadays , knowledge must be sought , created , discovered , shared and experienced , and the aim of higher education should be not just to transmit received knowledge but to teach students how to learn and how to be [ 12 , 18 ]  . knowledge in the past was relatively stable , so that what il ritardo della cultura della formazione forse perch coinvolto nelle lucrative problematiche della ricerca e innovazione , il mondo universitario si trovato in larga misura impreparato , sia da un punto di vista epistemologico che pedagogico , ad affrontare e risolvere i problemi che sono alla base dellattuale ritardo culturale delle formazione e della professione medica . 
dal punto di vista epistemologico necessario oggi rivedere lattuale organizzazione del sapere , troppo frazionata in discipline specialistiche e sub - specialistiche , in settori scientifici - disciplinari , in societ scientifiche [ 12 ]  . 
i 350 e pi settori scientifico disciplinari , in ambito accademico , riescono gi con difficolt a giustificarsi con gli specialismi della ricerca , ma sono certamente eccessivi ( oltre che settoriali ed anche di parte ) per creare conoscenze di base ed adeguatamente strutturare i corsi di studio . 
 necessaria uninnovazione culturale che sappia raccogliere ad unit e dare significato alla complessit dei fenomeni naturali , tecnologici , sociali , evitando leccessiva frammentazione delle discipline che , utile di certo per accrescere ed organizzare la conoscenza scientifica oggi insufficiente a cogliere e gestire la complessit delle singole attivit professionali ( pratica clinica )  . compito impegnativo per il quale necessario che il maggior numero possibile di docenti si impegni nella revisione degli ordinamenti didattici , non solo singolarmente , ma anche con lavoro di gruppo ed integrazione delle competenze . 
una revisione intesa a diffondere una cultura della progettazione , che non solo costruzione dobiettivi formativi pertinenti alla rilevanza dei bisogni e coerenti con i risultati , ma anche riflessione epistemologica sul contenuto delle discipline oggetto del proprio insegnamento e sulle loro finalit formative e professionalizzanti . 
dal punto di vista pedagogico oggi solo illusione pensare che , nellattuale societ della conoscenza , il sapere possa essere cristallizzato ed insegnato come avveniva in passato , e non invece ricercato , costruito , scoperto , condiviso e vissuto , finalizzando listruzione superiore non tanto e non solo alla trasmissione di conoscenze date , quanto allimparare ad imparare e allimparare ad essere [ 12 , 18 ]  . in passato il sapere era relativamente stabile per cui ci che si insegnava a scuola si modificava solo per effetto dellesperienza . 
oggi invece la crescita continua delle conoscenze e delle tecnologie ha reso provvisorio ogni sapere per cui ci che si impara a scuola solo la base sulla quale il sapere continua a crescere . 
ogni professionista , di conseguenza , deve continuare ad imparare per tutta la vita professionale per adeguare le proprie conoscenze alle diverse necessit , non sempre prevedibili in fase formativa . il sistema produttivo non chiede pi , in questo nuovo contesto , laureati che servono solo alloggi , a fare cio quello che si sta gi facendo . 
per acquisire le competenze del mestiere oggi non necessaria la laurea , ma possono essere sufficienti i corsi di formazione , i briefing , che sono tanto di moda , come testimoniato dai criticati 23000 e pi corsi di formazione sanitaria che si svolgono annualmente in italia . 
compito istituzionale prioritario di ununiversit inserita nellattuale societ , invece preparare laureati radiol med ( 2008 ) 113 : 307318 was taught at school would only change by virtue of experience . 
in contrast , the incessant growth of knowledge and technology today has made all knowledge provisional , and what is learned at school is no more than the basis on which knowledge continues to grow . 
consequently , all professionals have to continue to learn throughout their lives to be able to adapt what they know to a variety of needs that cannot always be predicted in the educational stage . 
moreover , one no longer needs a university degree to learn the skills of the trade : training courses or briefings may be sufficient , as demonstrated by the much criticised 23 , 000 and more courses for health professionals held in italy every year . 
in other words , they must be able to not only impart knowledge and carry out research to expand that knowledge ( objectivist approach ) , but also be prepared to acquire new potential knowledge [ 19 ] ( constructivist approach )  . academic education is not something episodic that starts at enrolment and ends at graduation . 
to educate means to transmit a scientific methodology [ 20 ] ; it means equipping students with the means to critically and creatively appraise the scientific literature throughout their professional lives . the professionalizing mission of the university is best fulfilled when it relates to work settings requiring scientific reasoning and an ability to mediate between theory and practice ; between principles and general and specific cases . 
this means integrating existing , ready - toapply knowledge with more fluid and problematic knowledge that is open to innovative solutions and methods fit for challenging experience and experimenting on phenomena with a view to better understanding and controlling reality . 
on the contrary , it means being able to integrate the informationist paradigm of traditional , teacher - centred reception learning with the student - centred interactionist paradigm , in which instructional communication is viewed as a network of meaningful interpersonal relations that value individual learning styles [ 12 ]  . 
in other words , students explore and observe reality in the laboratory and in the field ; they act on phenomena by posing problems and finding solutions ; they use analogical and simulation strategies for the production , organisation and representation of knowledge . education takes place through learning experiences , the adatti ad apportare innovazioni culturali nel contesto sociale gestendo situazioni complesse con capacit creative . capaci cio non solo di trasmettere il sapere in atto e fare ricerca per aumentarlo ( approccio oggettivistico ) , ma anche di prepararsi ad affrontare il sapere [ 19 ] in potenza ( approccio costruttivistico )  . il tempo delluniversit non qualcosa depisodico , che comincia con liscrizione e finisce con la laurea . 
insegnare significa trasmettere una metodologia scientifica [ 20 ] ; significa educare lo studente a cimentarsi , per tutta la vita professionale , con la produzione scientifica , stimolandolo a mettere in gioco principalmente le capacit critiche e creative e non solo quelle recettive . 
il mandato professionalizzante delluniversit si realizza al meglio quando riferito a contesti di lavoro in cui sia richiesto pensiero scientifico e competenze di mediazione tra la teoria e la prassi , tra il principio e i casi generali e particolari . un sapere nutrito di metodologia scientifica sollecita anche la riflessione sulle implicazioni etiche e deontologiche delle sua traduzione nellambito professionale e sulla necessit di costruire competenze trasversali . 
ci significa integrare saperi stabilizzati , pronti allapplicazione diretta , con saperi fluidi , problematici , aperti a soluzioni innovative e alla ricerca di metodi e tecniche per interrogare lesperienza e sperimentare sui fenomeni della realt onde meglio comprenderla e meglio dominarla . 
significa invece saper inserire ed integrare il paradigma informazionista del tradizionale apprendimento per ricezione teacher centred con il paradigma interazionista student centred che considera la comunicazione didattica come sistema tecnologico di relazioni interpersonali significative , che valorizzano le formae mentis individuali [ 12 ]  . 
loggetto di conoscenza , per conseguenza , non pi il sapere cosa ma il sapere come ; si tratta di esplorare ed osservare la realt in laboratorio e sul campo , di intervenire nei fenomeni ponendo i problemi e ricercando le procedure di soluzioni , di utilizzare strategie analogiche e simulative di produzione , organizzazione e rappresentazione delle conoscenze . 
si realizzano cos esperienze formative , le cui parole - chiavie sono progetto , trasformazione , cambiamento , in cui il ruolo del docente non pi quello di trasferire / spiegare conoscenze , ma piuttosto quello di aiutare a scegliere il metodo corretto per risolvere problemi . 
in questo paradigma di apprendimento non necessario un insegnante per trasferire conoscenze , ma c bisogno di un istruttore , di un mentore che incoraggi e sostenga , che provi schemi di relazioni impegnative per la collaborazione di gruppo , che valorizzi le assegnazioni ai singoli , che trasferisca la responsabilit delle azioni e delle decisioni agli allievi , secondo le dinamiche proprie del gruppo di lavoro . opportuno precisare che il passaggio dallistruzione in presenza alla didattica a distanza , oggi in fase ascendente , innova di per s solo la natura dello stimolo / messaggio che da orale / scritto si trasforma in audiovisivo / informatico , ma non la metodologia ; anche nella formazione a distanza la didattica si innova profondamente solo quando alle for314 radiol med ( 2008 ) 113 : 307318 keywords of which are project , transformation and change , and in which the educators role is no longer to impart knowledge but to help the student choose the best method for solving a proble such a learning paradigm does not envisage a teacher who imparts knowledge but an instructor , a mentor , who provides encouragement and support , sets up challenging patterns of group interaction , values individual assignments , and transfers the responsibility for actions and decisions to the students according to the dynamics of teamwork . it should be noted that in itself , the growing shift from classroom teaching to distance teaching affects only the form of the stimulus / message , which becomes audio visual / computerised instead of oral / written . 
even in distance education , teaching is deeply innovated only when self - study with the aid of multimedia materials is accompanied by discovery learning and problem solving [ 12 , 21 ]  . 
additionally , in todays knowledge - based society , given that university education is no longer episodic , the scientific educational method represents the foundation for the continuing education of the single professional [ 22 ]  . the delay of the culture of patient care the italian health system is equityand solidarity - based and therefore substantially different from the those operating overseas . 
in fact , there was no need for film producer michael moores documentary sicko to tell us that despite the frequent , but often unfounded , talk of medical malpractice the italian health system is among the best in the world . 
however , the rising health care expenditure and the corporatisation of health care facilities have forced us to consider a concept that has become very important today : that of appropriateness . 
the sirm glossary defines appropriateness as a component of the quality of care that refers to the technical - scientific value , acceptability and pertinence ( with regard to persons , circumstances and place , current state of knowledge ) of health services . this concept of appropriateness established itself with the relatively recent health care reforms inspired by the doctrine known as new public management . 
appropriateness also involves an assessment of the economic impact of a certain clinical intervention proposed to address the patients medical conditions , that is , whether it is too costly and whether it can be replaced with another , equally effective but less expensive , treatment . without going into the complexities of health care policy , i feel it necessary to point out that in health care ( but not only ) , the correct balancing of needs , demand and supply represents an ideal goal that is , however , quite difficult me di auto - apprendimento con supporto di materiali multimediali si accompagna anche il gi ricordato apprendimento per scoperta , con soluzione dei problemi [ 12 , 21 ]  . 
sono queste le nuove caratteristiche specifiche che legano oggi inscindibilmente la ricerca alla formazione universitaria ; non essendo poi , come gi ricordato , il tempo delluniversit qualcosa di episodico , il metodo scientifico di formazione costituisce , nellattuale societ della conoscenza , a differenza di quanto avveniva in passato , cardine e base dellaggiornamento professionale continuativo del singolo professionista [ 22 ]  . il ritardo della cultura della assistenza la nostra sanit sociale e solidaristica , sostanzialmente diversa da quella doltre oceano . 
non occorre che venga il regista michael moore con il suo documentario sicko ad insegnarci che il nostro sistema , nonostante tanto si chiacchieri , spesso a vanvera , di malasanit , in buona sostanza uno dei migliori esistenti . 
lappropriatezza ( neologismo stilisticamente non bello , che non si ritrova nei dizionari italiani pi vecchi ) definita nel glossario sirm : componente della qualit dellassistenza che fa riferimento a validit tecnico - scientifica , accettabilit e pertinenza ( rispetto a persone , circostanze e luogo , stato corrente delle conoscenze ) delle prestazioni sanitarie . 
esso implica anche la valutazione di come un certo provvedimento clinico proposto per far fronte alla situazione patologica di un paziente incida economicamente , se lo faccia aumentando eccessivamente i costi e se non possa venire sostituito da un altro procedimento di pari validit , ma di minor costo . senza voler entrare in complesse implicazioni di politica sanitaria , ritengo opportuno evidenziare che in sanit ( ma non solo in sanit ) la corretta composizione dei bisogni , della domanda e dellofferta rappresenta il fine ideale , purtroppo difficile da raggiungere nella realt del quotidiano . laddove tuttavia domanda ed offerta si estendono al di l del dominio dei bisogni , lofferta non appropriata e la domanda pu essere artificiosamente sollecitata proprio dagli stessi produttori della gi ricordata ricerca e innovazione , con pesanti ricadute negative sul sistema sanitario e , cosa pi grave , sul singolo paziente . 
 proprio la ricerca quotidiana dellappropriatezza economica - organizzativa nel processo di re - ingegnerizzazione in atto nelle strutture sanitarie ha portato a rilevare , in ambito nazionale ed internazionale , che nellazienda sanitaria , a differenza di quanto avviene nelle altre realt azienradiol med ( 2008 ) 113 : 307318 to achieve in practice . 
when demand and supply extend beyond the domain of needs , supply is inappropriate and demand may be artificially stimulated by the research and innovation industry , with severe negative repercussions on the health care system and more importantly on the individual patient . 
 the constant search for economic - organisational appropriateness in reengineering health care delivery has shown , at national and international levels , that the health care enterprise differs from other types of business in that the final quality of the service is not dependent on organisation alone but on the scientific knowledge of the health care professional performing the clinical service . 
this explains why the concept of appropriateness has recently expanded to encompass new educational and professional goals as well ; in medicine , for example , appropriateness also refers to the choice of acts and procedures that define , qualify and enhance the professionalism ( cultural , scientific and empathetic ) of the physician delivering the service . 
the meaning of appropriateness is therefore broadening , and the economic - organisational notions of efficiency and effectiveness of a medical act , largely related to technology , are integrated with the predictive value of the act , which is strongly affected by the physicians professionalisan intervention that is ineffective clearly cannot be considered appropriate . 
 it follows that a complete evaluation of appropriateness in our health care system cannot be restricted to a single aspect of the medical service , for example the organisational - managerial aspect . 
on the contrary , it should consider multiple aspects and assess effectiveness in relation to the single patient , his or her needs and the complexity of care in each single case . 
if medical care is considered in terms of knowledge , we will need to evaluate methodological appropriateness and scientific appropriateness ; on the other hand , if care is evaluated as an interpersonal activity , we will have to assess deontological appropriateness , ethical appropriateness and economic - organisational - managerial appropriateness [ 23 ]  . in this new cultural context , clinical practice has become a complex activity involving teamwork and multiple competences . 
consequently , determining appropriateness should be carried out for each of the single phases in this teamwork that , in radiological practice , includes prescription , methodology , technique , diagnosis and reporting . if we consider data presented during the myriad of scientific congresses held in italy every year , in the biomedical literature and generally by the press and television , we can dali , la sola organizzazione non in grado di determinare la qualit dellatto finale , non potendo prescindere dalle conoscenze scientifiche del professionista che effettua la pratica clinica . 
per questo in questi ultimi anni il termine appropriatezza , tende ad incorporare , andando anche oltre la definizione sopra riportata , il concetto di nuovi obiettivi specifici educativi e professionali , e incomincia ad essere usato in medicina anche per caratterizzare la scelta datti e procedure specifiche che definiscono , qualificano e valorizzano la qualit professionale ( culturale , scientifica ed empatica ) del medico che effettua le singole prestazioni . 
il termine appropriatezza sta quindi ampliando il suo significato , cos da integrare le valenze economico - organizzative dellefficienza e dellefficacia dellatto medico , legate in gran parte alla tecnologia , con il valore predittivo dello stesso atto , fortemente condizionato dalla qualit professionale del medico . 
di certo un intervento inefficace non pu essere appropriato ; tuttavia anche un intervento per il quale vi sia prova scientifica certa defficacia potrebbe non essere appropriato , qualora effettuato su un paziente per il quale non indicato . 
 ne deriva che una valutazione completa dellappropriatezza nella nostra sanit sociale non possa limitarsi a considerare un solo aspetto dellattivit medica , quale pu essere il pur importante dato organizzativo - gestionale , ma deve invece prendere in considerazione i suoi multiformi aspetti , costituendo una sorta di valutazione defficacia sul singolo paziente , in relazione con i suoi bisogni e con la complessit assistenziale del particolare caso . 
cos se la pratica medica viene considerata dal punto di vista della conoscenza si dovr valutare unappropriatezza metodologica ed unappropriatezza scientifica ; se invece si valuter la medicina come attivit che comporta relazione tra persone , si dovranno considerare unappropriatezza deontologica , unappropriatezza etica ed unappropriatezza economico - organizzativo - gestionale [ 23 ]  . in questo nuovo contesto culturale la pratica clinica oggi , a differenza del passato , unopera complessa , un lavoro di gruppo che coinvolge competenze diverse , in continuo divenire ; di conseguenza lappropriatezza nel suo complesso va applicata nelle singole e diverse fasi di questo lavoro di gruppo , che per lattivit radiologica sono le fasi prescrittiva , metodologica , tecnica , diagnostica e refertativa . se ci rapportiamo a quanto si discute nella miriade dei congressi scientifici che annualmente si svolgono in italia , ai dati della letteratura , o a quanto si legge sulla carta stampata o si vede in televisione emerge , con chiarezza , come ruolo e importanza della sensibilit e specificit delle singole tecniche e metodiche prevalgono di gran lunga sullappropriatezza in generale , su quella prescrittiva , in particolare , sistematicamente e costantemente trascurata , nonostante precise normative legislative vigenti , con ovvie ripercussioni negative sul ruolo clinico della stessa radiologia . la mancata applicazione della legge 187 sulla giustifi316 radiol med ( 2008 ) 113 : 307318 clearly see how the role and importance of sensitivity and specificity of single techniques and methods by far predominate over overall appropriateness and in particular prescribing appropriateness . 
187 concerning the justification and pertinence of radiological examinations , resulting from both epistemological shortcomings and serious administrative - bureaucratic inconsistencies , leads to that absurd waste of public money due to the uselessness ( or extremely limited usefulness ) of at least 50% of all radiological examinations performed in italy . 
and all this occurs amidst a general indifference , because the issue of prescribing appropriateness does not pay politically despite the indisputable waste of public money and , more importantly , the harm suffered by patients truly in need of specialised medical treatment . 
so much so for patient - centred care ! the cultural reclaiming of humboldts unity and its present significance in the past , clinical practice did not pose the problem of appropriateness in such as pressing manner as it does today . the activity of the physician at the bedside appeared selfcontained , the instruments available to help in achieving ones goal were few and assessment of ones performance was straightforward . 
subsequently , the increasing complexity of the medical act and the demands of research and innovation led us to believe that humboldts idea of the unity of research , teaching and care in medical education was out of date and that the new patterns of academic education necessarily involved the decline of traditional academic roles and functions . in a continuously evolving society , learning a scientific methodology which is quite different from spasmodically searching for usable research results should instead enhance the scientific nature of education and professional activity and promote sharing , coresponsibility , cooperation and interactive teamwork . 
 students who have been taught during education and training to use scientific methods for problem solving will , once graduated , be able to adapt their professional knowledge to the changes not always predictable in medicine and society . 
students who have been taught to use scientific methods to acquire potential knowledge will be able to transfer those methods to their work setting and implement that patient - centredness called for by so many but constantly disregarded . 
perhaps humboldt was aware of this when he portano cazione e pertinenza delle indagini radiologiche , legata sia alle gi ricordate carenze epistemologiche che a gravi inamministrative - burocratiche congruenze quellassurdo spreco del denaro pubblico per linutilit ( o la scarsissima utilit ) del 50% e pi degli esami radiologici che si eseguono in italia . 
il tutto nellindifferenza di tutti , nessun escluso , perch paradossalmente il problema dellappropriatezza prescrittiva politicamente non paga nonostante lincontrovertibile spreco di denaro pubblico e , cosa ancora pi grave , il danno significativo per qui pazienti che hanno realmente bisogno di prestazioni mediche specialistiche . 
questa purtroppo la centralit del paziente di cui oggi tanto si parla ! il recupero culturale dellinscindibilit humboldtiana e suo significato attuale in passato la pratica medica non poneva il problema dellappropriatezza in modo pressante come oggi . 
successivamente proprio le complessit crescenti dellatto medico e le esigenze , sempre pi omniassorbenti della ricerca e innovazione , hanno fatto credere inattuale lidea originaria di humboldt sullinscindibilit universitaria tra ricerca , formazione ed assistenza , e indotto a pensare che i nuovi dinamici modelli di formazione universitaria rendessero inevitabile il tramonto di ruoli e funzioni tradizionali delluniversit . lapprendimento di una metodologia scientifica , che ben altra cosa della ricerca spasmodica del risultato praticamente utile di una ricerca , dovrebbe invece servire a valorizzare , in una societ in evoluzione , la scientificit nella formazione e nellattivit professionale , e a favorire condivisione , corresponsabilit , collaborazione , lavoro di gruppo interattivo ; dando cos nuovo e concreto significato culturale allinscindibilit dei ruoli , incentivando , contemporaneamente , nel contesto del lavoro quotidiano , una riflessione critica sulle finalit formative e professionalizzanti delle singole discipline . lo studente formato e educato alla metodologia scientifica della soluzione dei problemi , nella formazione e nellattivit assistenziale , sar capace da professionista di organizzarsi in ogni evenienza , adeguando la propria formazione professionale ai cambiamenti , non sempre prevedibili , della medicina e della stessa societ . 
lo studente preparato e educato ad acquisire conoscenza in potenza , con metodologia scientifica , sapr portare nellambiente di lavoro il metodo culturale che lo ha formato e realizzare , in ambito assistenziale , quella centralit del paziente da tanti invocata , ma costantemente disattesa . 
questo forse aveva intuito humboldt , quando introdusse la ricerca scientifica , accanto e a monte di quella funzione didattica che era da sempre patrimonio delluniversit . la realizzazione concreta di questo modello culturale radiol med ( 2008 ) 113 : 307318 added scientific research to the traditional teaching role of universities . 
 the practical implementation of such a cultural model of integration in todays knowledge - based society is heavily conditioned by assessing the quality of the final product ( professionalism ) and production process ( educational function ) , an aspect that cannot be ignored . 
subsequently , through maturation of the concept of continuous quality improvement , it further evolved into the current vision of total quality management . recent experience shows that the initial efforts required to assimilate and apply the notions of total quality management and the greater cost of implementing it are widely rewarded in the midto short term by achieving a better product . 
 unfortunately , i have the impression that , with regard to teaching and medical professionalism , in italy we have yet to reach the 1930s stage that is , quality control of the finished product . 
the approach to university and licensing examinations , the approach to graduation and specialisation theses , the emphasis on quantity over quality in patient care and the confusion with regard to the concept of research are all far from ensuring the quality of the final product , let alone that of the production process ( teaching function ) , which is totally overlooked . 
the new meaning of the unity which values interactivity and problem - solving learning to ensure students ability to acquire potential new knowledge becomes the foundation of continuing medical education . 
if we really want continuing medical education to serve its role of effectively maintaining knowledge , expertise and professional skills , then we need to introduce not only structural and functional changes but also cultural innovations into a system that overall is showing clear signs of inadequacy [ 22 ]  . experiential learning , realised through integrated learning environments [ 12 ] , could and indeed should represent the dynamic new form of education produced by this cultural innovation . 
an integrated learning environment relates information processes ( scientific - disciplinary organisation of knowledge : linear , modular , hypertextual ) both to knowledge processes ( reception , exploration , contextualisation ) and learning processes ( behaviourist , cognitivist , constructivist )  . dintegrazione nellattuale societ della conoscenza fortemente condizionato dalla verifica della qualit del prodotto finale ( professione medica ) e dalla qualit del processo produttivo ( funzione docente )  . 
la metodologia dellassicurazione di qualit , sviluppatasi in una vera e propria scienza , impronta di s ormai tutti i rami della produzione , ivi compresi quelli della formazione e dellassistenza sanitaria . 
nata negli anni 30 dal concetto di controllo di qualit del prodotto finito , evoluta poi nellassicurazione di qualit ( come insieme delle attivit che sorvegliano il processo produttivo ) fino a giungere , attraverso la maturazione del concetto di miglioramento continuo di qualit allattuale visione di total quality management . 
lesperienza pi recente evidenzia che lo sforzo iniziale necessario ad assorbire ed applicare i concetti del total quality management , nonch il maggior costo necessario a produrlo , sono ripagati , nel medio e lungo termine , dallottenimento di un prodotto migliore . 
il che non avviene dove tutto ci ignorato completamente o affrontato con il pressappochismo di chi crede di saper tutto per scienza infusa ho purtroppo limpressione che per quanto riguarda la formazione e la professione medica in italia non siamo neppure alla fase degli anni 30 , cio a quella del controllo di qualit del prodotto finito : limpostazione vigente degli esami di profitto e dabilitazione professionale , le tesi di laurea e di specializzazione , come sono oggi impostate , il privilegiare in ambito assistenziale il dato quantitativo su quello qualitativo , la confusione sullattuale concetto di ricerca non garantiscono la qualit del prodotto finale . 
la nuova concezione culturale di integrazione tra ricerca , didattica ed assistenza nella formazione medica universitaria , precedentemente enucleata e delineata , incide significativamente , a differenza del passato , anche in ambito professionale . 
il nuovo significato culturale di inscindibilit , che valorizza interattivit e apprendimento fondato sulla soluzione dei problemi per garantire capacit di acquisire conoscenze in potenza , diventa , di conseguenza e di necessit cardine e base del moderno aggiornamento professionale del singolo medico . 
se si vuole realmente che leducazione continua in medicina ( ecm ) svolga la sua funzione di mantenimento efficace delle conoscenze , competenze e abilit professionali sono necessarie innovazioni culturali , oltre che strutturali e funzionali , di un sistema che nel suo complesso sta dando segni palesi di inadeguatezza [ 22 ]  . le gi ricordate esperienze formative , concretizzandosi negli ambienti formativi integrati [ 12 ] potrebbero ( dovrebbero ) rappresentare le nuove realt dinamiche da raggiungere con questinnovazione culturale , relazionando i processi dinformazione ( organizzazione scientifico disciplinare dei saperi : lineare , modulare , ipertestuale ) sia con i processi di conoscenza ( ricezione , esplorazione , contestualizzazione ) che con i processi dellapprendimento ( comportamentista , cognitivista , costruttivista )  . 318 radiol med ( 2008 ) 113 : 307318 these are no doubt challenging innovations that involve cultural , educational and professional reengineering . 
this difficult task must be carried out by all physicians , including radiologists , in all professional settings whether universities , hospitals or clinics ; whether in family , specialty or subspecialty medicine . 
not only that , it is a task that physicians and radiologists cannot and must not delegate to others but must undertake themselves , with commitment and shared responsibility , for the sake of the future of clinical radiology . 
 innovazioni tutte di certo impegnative , vera re - ingegnerizzazione culturale , formativa e professionale , difficile da raggiungere ma necessaria per tutti i medici , radiologi inclusi , ovunque essi operino ; in ambito accademico , ospedaliero o ambulatoriale , in medicina generale , specialistica e sub specialistica . 
mascalchi1 1radiodiagnostic section , department of clinical physiopathology , university of florence , viale morgagni 85 , 50134 florence , italy 2radiodiagnostic unit , careggi hospital , florence italy correspondence to : m . 
ten patients ( mean age 45 years , range 23 - 83 ) with haemoptysis due to bronchoscopic biopsy of indeterminate lung nodules , lung cancer , tubercular bronchiectasis , cystic bronchiectasis or sarcoidosis underwent embolization of the bronchial arteries responsible for the bleeding using detachable coils . patients were followed - up for a median of 14 months . 
use of detachable coils for embolization of bronchial arteries in patients with haemoptysis is advantageous since it eliminates the risk of migration typical of other embolic materials and enables rapid and permanent vessel occlusion . keywords bronchial embolization hemoptysis detachable coils riassunto obiettivo . 
limpiego di spirali a distacco controllato per lembolizzazione delle arterie bronchiali in pazienti con emottisi vantaggioso in quanto elimina il rischio di migrazione proprio di altri materiali embolizzanti e permette una occlusione vascolare rapida e permanente . parole chiave embolizzazione bronchiale emottisi spirali a distacco controllato radiol med ( 2008 ) 113 : 452460 introduction bronchial artery embolization ( bae ) is an effective treatment for massive haemoptysis in patients who cannot undergo surgery due to reduced ventilatory capacity or concurrent diseases or in patients with recurrent haemoptysis not responding to medical or endobronchial treatments [ 16 ]  . 
 in eight patients the underlying diseases were tubercolosis ( five patients ) , bronchogenic carcinoma ( one patient ) , cystic bronchiectasis ( one patient ) and sarcoidosis ( one patient ) ; they caused recurrent episodes of haemoptysis with decreased haemoglobin levels and were unresponsive to medical and endobronchial treatment ( cold saline solution lavage , endobronchial balloon tamponade with or without instillation of epinephrine )  . 
finally , in one additional patient ( n 3 ) haemoptysis had recurred one month after microsphere embolization of the right bronchial artery for a bleeding lung cancer , and diagnostic arteriography showed recanalization of the same vessel . 
the ct and diagnostic angiography findings obtained before bae in all patients are detailed in table 1 . angiography and embolization were performed using high - resolution digital subtraction angiography units and a standard femoral route with 4 or 5 f vascular sheath . 
the selective study of the bronchial , intercostal and subclavian arteries was done using 4 or 5 f pre - shaped hydrophilic cobra 12 , simmons 1 catheters ( terumo corporation , tokyo , japan )  . 
the source of bronchial bleeding was identified by taking into account one or a combination of the following arteriography features : hypertrophy of the bronchial artery , presence of vascular blush or of a shunt with pulmonary arteries and veins , presence of pseudoaneurysm - like vascular ectasia and extravasation of contrast agent . 
superselecintroduzione lembolizzazione delle arterie bronchiali ( eab ) rappresenta unopzione terapeutica efficace nel trattamento di pazienti con emottisi massiva che non possono essere sottoposti ad intervento chirurgico per una ridotta riserva respiratoria o per altre patologie associate . 
lindicazione al trattamento di eab sempre stata posta dopo discussione del caso tra il clinico di riferimento , il chirurgo toracico , il broncoscopista ed il radiologo interventista . otto pazienti erano affetti rispettivamente da tubercolosi ( 5 pazienti ) , neoplasia polmonare ( 1 pazienti ) , bronchiectasie cistiche ( 1 paziente ) , sarcoidosi ( 1 paziente ) e presentavano ripetuti episodi di emottisi non responsivi a trattamenti medici o broncoscopici ( lavaggio con soluzione fisiologica fredda , tamponamento endobronchiale ) associati a riduzione dei livelli di emoglobina . 
una paziente stata inviata dalla terapia intensiva per emottisi massiva complicata da arresto cardio - respiratorio a distanza di 5 giorni dallesecuzione di biopsia transbronchiale per la definizione di noduli polmonari a distribuzione peribronchiale . 
le caratteristiche demografiche , leziologia dellemottisi , i reperti della tomografia computerizzata ( tc ) e dellangiografia diagnostica insieme alla tecnica di embolizzazione sono elencati nella tabella 1 . tutte le procedure sono state effettuate in sala angiografica con apparecchiature digitali ad alta risoluzione . 
dopo cateterismo arterioso femorale con introduttore 4 o 5 f stato eseguito lo studio selettivo delle arterie bronchiali , intercostali e succlavie impiegando cateteri idrofilici cobra 1 - 2 e simmons 1 ( terumo corporation , tokio , giappone )  . sono stati considerati reperti angiografici significativi lipervascolarizzazione , la presenza di shunt con larteria o le vene polmonari , ectasie focali a tipo pseudoaneurisma e lo stravaso di mezzo di contrasto . 
una volta identificato il vaso o i vasi patologici si proceduto al cateterismo superselettivo con microcatetere coassiale prowler plus 454 radiol med ( 2008 ) 113 : 452460 tive catheterization of the vessel responsible for bronchial bleeding was carried out with a prowler plus coaxial microcatheters ( cordis , miami , florida ) and a terumo gt 0.16 ( terumo corporation , tokyo , japan ) hydrophilic microguide to preserve the proximal segment of the bronchial artery from which spinal or visceral arteries can arise . 
all patients received wide - spectrum antibiot ( cordis , miami , florida ) e microguida idrofila terumo gt 0.16 ( terumo corporation , tokio , giappone ) con lobbiettivo di preservare il tratto prossimale dellarteria bronchiale da cui possono originare rami spinali o viscerali per gli organi mediastinici . in 4 pazienti che presentavano intensa ed estesa ipervascolarizzazione stata eseguita embolizzazione preliminare con microsfere costituite da un polimero acrilico impregnato di gelatina idrofila ( embosphere , biosphere medical , cedex , francia ) di dimensioni comprese tra 500700 micron . 
origine dellab sinistra dallarteria succlavia . due sessioni di embolizzazione con microsfere e spirali . lesioni cavitarie in entrambi i lobi superiori bronchiectasie cistiche nel lobo medio lesioni cavitarie nel lobo superiore destro aree di consolidazione nei lobi superiori aree di consolidazione e lesioni cavitarie nel lobo superiore di sinistra lesioni cavitarie nei lobi superiori bronchiectasie , fibrosi polmonare massiva ed esteso ispessimento pleurico di entrambi i lobi superiori ab , arteria bronchiale , ai , arteria intercostale , tbc , tubercolosi ic therapy for 6 - 7 days after the procedure . 
along with development of new catheters and embolic materials , the efficacy and the indications of bae have increased . the pathophysiological background for bae as a treatment of haemoptysis is that the bronchial arteries are the source of bronchial bleeding in 90% of cases . 
in particular in many acute and chronic lung diseases the small vessels originating from the pulmonary arteries show narrowed lumen or even occlusion due to hypoxic vasoconstriction , thrombosis or inflammatory changes . 
this induces compensatory hypertrophy of the small vessels originating from the bronchial arteries which , however , can rupture following erosion of the vessel wall caused by inflammation , tumour growth or regional increase in blood pressure [ 15 ]  . the bronchial arteries typically exhibit several anatomic variants of origin and course . 
usually they arise directly from the descending thoracic aorta between the fifth and sixth thoracic vertebrae as a single vessel or jointly with the intercostal artery ( intercostal - bronchial trunk )  . 
 the bronchial arteries provide blood supply not only to the trachea and bronchi but also to other mediastinal organs caratterizzata da una grossa arteria bronchiale sinistra che originava dallarteria succlavia non riconosciuta nel primo trattamento che stata occlusa con spirali nella seconda sessione di embolizzazione . discussione leab nel trattamento dellemottisi massiva stata introdotta negli anni settanta [ 6 ] e perfezionata nel corso degli anni grazie allintroduzione di nuove tipologie di cateteri e di nuovi materiali embolizzanti , migliorandone lefficacia ed ampliandone le indicazioni . le basi fisiopatologiche per leab risiedono nel fatto che nel 90% dei casi la fonte dellemottisi deriva dalla circolazione bronchiale piuttosto che da quella polmonare . 
in molte patologie polmonari acute e croniche infatti le arteriole polmonari si riducono di calibro o si occludono per vasocostrizione ipossica , trombosi o vasculite con conseguente ipertrofia delle arterie bronchiali che si possono rompere per erosioni causate dal processo infiammatorio stesso o per incrementi regionali della pressione [ 15 ]  . le arterie bronchiali mostrano numerose varianti anatomiche di origine e decorso ; nella maggioranza dei casi originano direttamente dallaorta toracica discendente ad un livello variabile tra la quinta e la sesta vertebra toracica sia come vaso singolo sia con origine comune allarteria intercostale ( tronco intercosto - bronchiale )  . 
le origini anomale pi frequenti sono a livello dellarco aortico , dellarteria mammaria interna e dellarteria succlavia [ 4 ]  . le arterie bronchiali oltre ad irrorare la trachea ed i bronchi si distribuiscono anche ad altri organi mediastinici radiol med ( 2008 ) 113 : 452460 fig . 
left subclavian artery angiogram before bae ( b ) shows multiple parietal branches originating from the subclavian artery and accessory bronchial artery ( arrow ) which feed a wide hypervascular area and multiple vascular fistulas with the pulmonary artery . 
lo studio angiografico pre - embolizzazione dellarteria succlavia sinistra ( b ) dimostra rami parietali multipli e unarteria bronchiale accessoria ( freccia ) che alimentano un esteso letto vascolare e multiple fistole con larteria polmonare . 
rarely bronchial arteries can give origin to radiculomedullary branches [ 4 ]  . before bae all our patients were evaluated with ct , bronchoscopy and diagnostic arteriography aimed at locating the site of bronchial bleeding . 
in particular ct , especially if performed with multi - detector scanners , can demonstrate hypertrophic bronchial arteries , the site and the cause of haemoptysis as well as pleural involvement [ 7 ]  . 
the latter is important since it is associated with recruitment of extra - bronchial arteries supplying the chest wall which need to be accurately investigated during the bae procedure [ 1 , 46 ]  . coaxial microcatheters enable superselective catheterization of distal small - size and tortuous vessels and stable positioning for coil detachment without harm for the proximal portion of the bronchial artery [ 14 ]  . the embolic material usually used for bae consists of corquali pleura viscerale , esofago , linfonodi , parete aortica . raramente le arterie bronchiali possono dare origine a rami radicolo - midollari [ 4 ]  . tutti i nostri pazienti sono stati sottoposti prima della procedura di eab ad esame tc del torace , broncoscopia e angiografia diagnostica per identificare la sede dellemottisi . 
in particolare lesame tc , soprattutto se eseguito su apparecchiature multislice , pu consentire di rilevare i vasi bronchiale ipertrofici , la causa e la sede del sanguinamento ed evidenziare un coinvolgimento della pleura [ 7 ]  . 
questultimo infatti determina il reclutamento di arterie extrabronchiali dirette alla parete toracica che devono essere attentamente ricercate durante lembolizzazione [ 1 , 46 ]  . il cateterismo coassiale tramite microcatetere consente uno studio superselettivo anche di vasi di piccolo calibro e con decorso tortuoso permettendo di raggiungere una posizione stabile del catetere e di risparmiare il tratto prossimale dellarteria da cui possono originare rami per gli orradiol med ( 2008 ) 113 : 452460 pusculate particles such as gelfoam and pva which are readily available and easy to manage . 
however , bae with particles exposes to the risk of retrograde embolization of non - target areas with the possibility of lung infarction and necrosis of the oesophageal , bronchial and aortic walls and spinal cord ischaemia to avoid these complications , particles of diameter equal to or above 300 micron are recommended that cannot pass the bronchopulmonary anastomoses and occlude the vasa vasorum of the mediastinal organs [ 4 ]  . 
the risk is particularly high when large amounts of embolizing particles are needed to occlude large abnormal vascular beds or hypertrophic vessels . metal coils overcome some of the drawbacks of the corpusculate materials for bae and at the same time afford permanent occlusion of the vessel [ 1 , 8 ]  . 
moreover the variable length and diameter of these coils makes it possible to match the coil size to arteries of variable shape , allowing the rapid and permanent occlusion of even hypertrophic vessels . 
however , control arteriography revealed that in both patients recurrence was due to disease progression with recruitment of new feeding vessels and not to recanalization of the bronchial arteries previously embolized with coils . 
in line with previous reports no recurrence was observed in patients with haemoptysis due to tuberculosis [ 3 ]  . gani mediastinici ed arterie radicolo - midollari [ 14 ]  . generalmente nelleab vengono utilizzati materiali embolizzanti corpuscolati di vario tipo , in particolare particelle di gelfoam e di pva , grazie alla loro ampia disponibilit e facilit di impiego . 
fra gli svantaggi dei materiali corpuscolati va ricordata la possibilit di reflusso con embolizzazione di organi non bersaglio e linsorgenza di infarto polmonare o di necrosi parietale a livello dellesofago , dei bronchi o della parete aortica . 
per evitare questultima complicanza si consiglia infatti lutilizzo di particelle di diametro non inferiore ai 300 micron per evitare il superamento delle anastomosi bronco - polmonari e locclusione dei vasa - vasorum degli organi mediastinici [ 4 ]  . 
i rischi descritti aumentano se necessario utilizzare grandi quantit di materiali embolizzanti per locclusione di estesi circoli patologici o di vasi ipertrofici . le spirali metalliche consentono di superare alcuni dei limiti descritti per i materiali corpuscolati , in particolare permettono locclusione permanente del vaso [ 1 , 8 ]  . 
 nella nostra esperienza il vantaggio maggiore rispetto ad altri tipi di spirali risiede nel meccanismo di distacco efficace ed intuitivo che consente di verificare la posizione e la stabilit della spirale prima del rilascio evitando il rischio di migrazione . 
inoltre la notevole variabilit di lunghezza e diametro con cui sono disponibili permette un ottimale adattamento ad arterie di varie dimensioni rendendo possibile locclusione permanente anche di vasi ipertrofici . questa caratteristica ha consentito una rapida stabilizzazione delle condizioni emodinamiche nella paziente con emottisi massiva dopo biopsia transbronchiale . in 3 pazienti in cui langiografia mostrava estesa ipervascolarizzazione abbiamo eseguito unembolizzazione preliminare con microsfere per ottenere una devascolarizzazione distale e cercare di evitare una ricanalizzazione da parte di altri vasi . 
in accordo con i dati della letteratura non si sono avuti nuovi episodi di sanguinamento nei pazienti affetti da bronchiectasie tubercolari [ 3 ]  . conclusions conclusioni bae using detachable coils was effective in halting the bronchial bleeding within 24 hours with no complication and no recanalization of the occluded vessels . 
however , the limited number of patients does not allow conclusions about possible advantages of detachable coils as opposed to other embolic materials in the treatment of haemoptysis , especially with regard the long - term outcome . leab in tutti i pazienti stata efficace nellarrestare il sanguinamento entro le 24 ore in assenza di complicanze legate alla procedura . 
quando invece hanno attenuazione pari a quella dei tessuti molli , devono essere prese in considerazione nella diagnosi differenziale altre lesioni solide ; in questi casi la rm pu essere utile per determinarne la natura cistica . parole chiave tc torace lesioni cistiche 386 introduction bronchogenic cysts are congenital lesions secondary to abnormal budding of the bronchial tree during embryonic development [ 1 ]  . 
the majority of cysts are located in the mediastinum , although they may also be found in the lung , pericardium , retroperitoneum , thymus , diaphragm or neck [ 15 ]  . bronchogenic cysts have a round or oval shape , unilocular appearance and air or fluid contents . 
rarely discovered in the period from childhood to late adulthood , they are often an incidental finding on radiographs performed for other reasons or to investigate the presence of related symptoms ( cough , chest pain , hyperthermia , dyspnoea on exertion , dysphagia , haemoptysis ) [ 24 , 610 ]  . 
a more precise diagnostic characterisation is provided by computed tomography ( ct ) scans : cysts involving the lung usually exhibit either airfluid density or only air or only fluid density , whereas mediastinal cysts show attenuation values typical of fluid content [ 35 , 11 , 12 ]  . 
an atypical pattern of high density suggestive of solid contents is also possible , which makes the differential diagnosis more difficult [ 13 ]  . we retrospectively reviewed the imaging studies ( biplanar radiographs and ct ) of all surgically confirmed bronchogenic cysts observed in our department over the past 15 years to identify the findings that are most useful for detection and , when possible , characterisation of this disease . materials and methods we considered 26 adult patients discharged with a histological diagnosis of bronchogenic cyst as of 1992 . 
the ct scans performed at our department were acquired with a dual - detector array ( twin flash ) , 5.5 - mm slice thickness and pitch 1.5 , before and after i.v. 
all examinations were reviewed by three chest radiologists who analysed the images independently and discussed the findings to reach a consensus . on the basis of location , lesions were classified as pulradiol med ( 2008 ) 113 : 385394 introduzione le cisti broncogene sono lesioni congenite secondarie ad unanomala gemmazione dellalbero bronchiale durante la fase embriologica [ 1 ]  . 
nella maggior parte dei casi , secondo quanto riportato in letteratura , sono situate nel mediastino , ma possono essere riscontrate anche nel polmone , nel pericardio , nel retroperitoneo , nel timo , nel diaframma o nel collo [ 15 ]  . 
di osservazione infrequente in soggetti di et compresa dallinfanzia alla tarda et adulta , costituiscono molto spesso reperto occasionale in radiogrammi effettuati per svariate motivazioni o , talvolta , in presenza di sintomatologia correlabile ( tosse , algie toraciche , ipertermia , dispnea da sforzo , disfagia , emottisi ) [ 24 , 610 ]  . 
successivamente allesame radiologico si ricorre , per una pi precisa definizione diagnostica , ad indagine tc : le lesioni a sede polmonare presentano abitualmente contenuto di densit idro - aerea , aerea o totalmente liquida , mentre quelle mediastiniche hanno valori di attenuazione propri di un contenuto liquido [ 35 , 11 , 12 ]  . 
talvolta possibile osservare aspetti atipici con riscontro di elevate densit , suggestive di contenuto solido e conseguente difficolt di diagnosi differenziale con altre patologie [ 13 ]  . stata analizzata retrospettivamente la documentazione radiologica ( radiogrammi biplani e tc ) di tutte le cisti broncogene toraciche , con successivo riscontro chirurgico , occorse alla nostra attenzione negli ultimi 15 anni : scopo del nostro lavoro stato rivalutare i reperti della diagnostica per immagini pi idonei per lindividuazione e , ove possibile , per la caratterizzazione di tale patologia . 
stato possibile ottenere la documentazione iconografica di 21 di essi : 16 pazienti hanno fornito sia i radiogrammi biplani del torace sia gli esami tc ( di cui 5 sia in condizioni basali sia dopo somministrazione di mezzo di contrasto ev ) mentre 5 disponevano dei soli esami radiografici . 
il campione da noi analizzato pertanto composto da 21 pazienti adulti di cui 11 femmine e 10 maschi , con et compresa tra 18 e 74 anni ( et media 43 , 1 anni )  . 
alcuni pazienti sono stati ricoverati gi in possesso della tc , effettuata quindi presso diversi centri con differenti modalit : le indagini tc eseguite presso il nostro servizio sono state effettuate con apparecchiatura a doppia corona di detettori ( twin flash ) con scansioni aventi spessore di 5 , 5 mm e pitch di 1 , 5 , dapprima in condizioni basali e successivamente radiol med ( 2008 ) 113 : 385394 monary or mediastinal . 
mediastinal lesions were then further characterised as anterior mediastinal if anterior to the heart and the great vessels , posterior mediastinal if located in the paraspinal region and middle mediastinal if located in the paratracheal or subcarinal regions or along the course of the oesophagus . at ct , mediastinal bronchogenic cysts were classified on the basis of their attenuation values as fluid - density cysts or soft - tissue - density cysts . 
this classification was established by two techniques : if region - of - interest ( roi ) measurements within the cyst were available , lesions were classified as fluid density if their attenuation was < 20 hu and as soft - tissue density if attenuation was > 20 hu . 
if cyst attenuation was similar to fluid in the gallbladder , the cyst was defined as fluid density , and if attenuation was greater , it was classified as soft - tissue density . lesions with a density similar to soft tissue were further subdivided into lesions with cystic , solid or indeterminate appearance , according to the criteria proposed by mcadams et al . 
lesions were defined as cystic if their attable 1 computed tomography classification of bronchogenic cysts fluid - attenuation values 020 hu solid - attenuation values 2090 hu cystic appearing attenuation less than soft tissues homogeneous contents no enhancement thin wall solid - appearing attenuation similar to soft tissues inhomogeneous contents no wall indeterminate not meeting criteria for cysticor solid - appearing cyst tabella 1 classificazione densitometrica delle cisti broncogene densit liquida 020 uh densit solida 2090 uh aspetto cistico attenuazione inferiore a quella dei tessuti molli circostanti contenuto omogeneo non enhancement parete sottile aspetto solido attenuazione simile a quella tessuti molli circostanti contenuto eterogeneo non evidenza di parete aspetto indeterminato assenza dei criteri indicati nelle precedenti categorie dopo somministrazione di mezzo di contrasto ( mdc ) endovenoso . 
sono stati rivalutati gli atti operatori per ottenere informazioni sulla localizzazione delle cisti e sulla presenza di eventuali peduncoli o zone di stretta adesione a strutture mediastiniche adiacenti quali lesofago o lalbero tracheobronchiale : tutti gli esami sono stati riletti da tre radiologi toracici che separatamente hanno valutato le immagini raggiungendo un accordo per consensus . sulla base della localizzazione le lesioni sono state classificate in polmonari e mediastiniche . 
quelle mediastiniche sono state ulteriormente differenziate in mediastiniche anteriori se localizzate anteriormente al cuore e ai grossi vasi ; mediastiniche posteriori se localizzate in sede paraspinale ; mediastiniche medie se localizzate nelle regioni paratracheale o subcarinale o lungo il decorso dellesofago . allesame tc le cisti broncogene mediastiniche sono state classificate , sulla base dei valori di attenuazione , in cisti a densit liquida e in cisti a densit dei tessuti molli . 
tale classificazione stata effettuata con due modalit : se era stata valutata la densit della cisti con area di interesse ( roi ) , le lesioni venivano classificate a densit liquida se il relativo coefficiente di attenuazione era inferiore a 20 hu e a densit simile ai tessuti molli se maggiore di 20 hu . quando tale valutazione non era disponibile , la classificazione era qualitativa , mediante confronto visivo con la densit del contenuto della colecisti : se le cisti presentavano attenuazione approssimativamente simile a questo erano definite a densit liquida , se invece presentavano attenuazione maggiore erano definite a densit dei tessuti molli . le lesioni con densit simile ai tessuti molli sono state ulteriormente classificate in lesioni di aspetto cistico , solido e indeterminato secondo i criteri esposti da mc adams et al . [ 4 ] ( tabella 1 ) : la lesione era definita di aspetto cistico se con valori di attenuazione inferiori ai tessuti molli circostanti , di aspetto omogeneo con assenza di enhancement e delimitazione con parete sottile ; di aspetto solido se lattenuazione era simile a quella dei tessuti molli circostanti e di aspetto eterogeneo quando non delimitata da parete sottile . infine venivano definite indeterminate le lesioni che non corrispondevano ai precedenti criteri . abbiamo infine effettuato una suddivisione in 3 gruppi delle lesioni mediastiniche valutate con tc basandoci su due parametri , sede e densit , allo scopo di rappresentare 3 livelli di probabilit diagnostica : il primo livello , in cui la diagnosi appare probabile , include le lesioni con sede tipica sottocarenale e densit liquida . 
nel secondo livello la diagnosi di cisti broncogena possibile e rientra tra le ipotesi diagnostiche insieme ad altre patologie ; abbiamo inserito in questo gruppo le lesioni con sede tipica e densit solida e le lesioni con sede non tipica e densit liquida . 
nel terzo livello sono state considerate invece le lesioni con se388 radiol med ( 2008 ) 113 : 385394 tenuation was less than that of surrounding soft tissue , if they were homogeneous , without enhancement and with a thin wall . 
they were defined as solid if attenuation was similar to that of the surrounding soft tissues , if they were heterogeneous and if they did not have a thin wall . 
lesions not meeting any of the above criteria were classified as indeterminate . finally , we subdivided mediastinal lesions into three groups on the basis of their site and density , with the aim of establishing three levels of diagnostic probability . 
the second level , possible diagnosis , encompassed lesions for which bronchogenic cyst entered the differential diagnosis with other conditions and included lesions with typical location and solid density and lesions with atypical location and fluid density . 
the third level , unlikely diagnosis , included lesions with atypical location and solid density . results the location of bronchogenic cysts was pulmonary in 5 / 21 cases ( 24% ) , two of which were in the left upper lobe , two in the right upper lobe and one in the left lower lobe . 
in 16 / 21 cases , the cysts were mediastinal ( 76% ) , six of which ( 37% ) were in the posterior mediastinum , eight ( 50% ) in the middle , two in the superior mediastinum ( 13% ) and none in the anterior mediastinum . chest radiography allowed the detection of lesions in all cases . 
by contrast , mediastinal lesions ( 16 cases ) had variable density that , based on the criteria established beforehand , could be classified as fluid ( 4 / 16 ) or solid ( 10 / 16 ) ; two lesions exhibited air attenuation . 
le cisti broncogene polmonari ( 5 casi ) si sono presentate in 2 / 5 quali opacit con livello idro - aereo nei campi polmonari superiori bilateralmente , in 1 / 5 nel campo polmonare inferiore destro , in 1 / 5 quale cisti aerea a pareti sottili localizzata nel campo polmonare superiore sinistro radiol med ( 2008 ) 113 : 385394 fig . 
le lesioni a sede mediastinica ( 16 casi ) presentavano al contrario densit variabile che , in base ai criteri tomodensitometrici precedentemente stabiliti , poteva essere classificata quale liquida ( 4 / 16 ) o solida ( 10 / 16 ) , avendo anche riscontrato 2 lesioni ad attenuazione aerea . 
nel gruppo delle lesioni solide abbiamo riconosciuto in 7 / 10 le caratteristiche delle cisti di aspetto indeterminato , in 2 / 10 quelle di tipo solido ed in 1 / 10 di tipo simil - cistico ( tabella 2 )  . discussione le cisti broncogene sono lesioni congenite che derivano da unanomala gemmazione verificatasi a livello dellalbero tracheo - bronchiale [ 4 , 7 ] , il cui sviluppo ha luogo nelle prime 16 settimane di et gestazionale e il cui contenuto pu essere aereo , sieroso , mucoso o misto [ 9 ] ; la localizzazione topografica dipende dallepoca della comparsa : se la gemmazione irregolare precoce la cisti si colloca nel mediastino , se pi tardiva si sviluppa perifericamente a livello del parenchima polmonare [ 1 ]  . 
4 tc : cisti broncogena che occupa totalmente il lobo superiore sinistro , che non possibile differenziare da una bolla di enfisema . sions , 7 / 10 displayed the features of indeterminate lesions , 2 / 10 of solid - appearing lesions and 1 / 10 of cystic - appearing lesions ( table 2 )  . discussion bronchogenic cysts are congenital lesions derived from abnormal budding of the tracheobronchial tree [ 4 , 7 ] that occurs during the first 16 weeks of gestation . 
location depends on the time of development : if the irregular budding takes place early on , the cysts develop in the mediastinum ; if it occurs table 2 computed tomography lesion attenuation density water soft tissue cystic appearing solid appearing undetermined tabella 2 densit delle lesioni alla tc aerea idrica tessuti molli similcistica solida aspetto indeterminato 2 ( 13% ) 4 ( 25% ) 10 ( 62% ) 1 ( 6% ) 2 ( 12% ) 7 ( 43% ) 2 ( 13% ) 4 ( 25% ) 10 ( 62% ) 1 ( 6% ) 2 ( 12% ) 7 ( 43% ) densit nostra casistica ( n = 16 ) mcadams et al . 
distribution varies , although subcarinal location in the middle mediastinum is the most typical site [ 16 ]  . mediastinal cysts are usually located in the middle and posterior mediastinum and less frequently in the anterior mediastinum [ 6 , 7 , 17 , 18 ]  . 
these data were confirmed in our series , in which location was predominantly mediastinal ( 76% ) , with 50% in the middle , 37% in the posterior and 13% in the superior mediastinum ; intrapulmonary location was less common ( five cases , 24% )  . pulmonary bronchogenic cysts are more frequently located in the lower lobes , without distinction between the right or left side , and are sometimes in communication with the airways [ 5 , 9 , 10 ]  . 
on conventional radiology , mediastinal bronchogenic cysts appear as sharply marginated round or oval masses with homogeneous opacity , which either protrude from or are contained within the mediastinum without modifying its contours [ 1 , 2 , 12 ]  . 
wall or intracystic calcification is rare ; the presence of airfluid levels may be seen when fistulation of the tracheobronchial tree occurs [ 9 , 12 ]  . in our study , the most frequent radiographic finding in mediastinal cysts consisted of well - defined opacities either protruding beyond the right mediastinal contour or , more fig . 
la distribuzione variabile anche se la localizzazione subcarinale nel mediastino medio rappresenta la sede pi tipica [ 16 ]  . nel complesso le cisti mediastiniche sono solitamente localizzate nel mediastino medio e in quello posteriore , pi di rado nel mediastino anteriore [ 6 , 7 , 17 , 18 ]  . 
tale dato confermato dalla nostra casistica , ove presentano localizzazione preferenziale mediastinica ( 76% ) di cui il 50% nel mediastino medio , 37% in quello posteriore e 13% in quello superiore : meno frequente si rivelata la localizzazione polmonare ( 5 casi , 24% )  . le cisti broncogene polmonari sono , invece , localizzate pi frequentemente nei lobi inferiori senza distinzione tra lato destro e sinistro e sono talvolta comunicanti con le vie aeree [ 5 , 9 , 10 ]  . 
alla radiologia tradizionale le cisti broncogene mediastiniche si presentano quali masse rotondeggianti od ovali con margini netti che possono debordare dal mediastino o esserne contenute allinterno senza alterarne il profilo , presentando spesso opacit omogenea [ 1 , 2 , 12 ]  . 
raramente si apprezzano calcificazioni della parete od intracistiche ; si pu rilevare la presenza di livello idro - aereo quando si crei fistolizzazione con lalbero tracheobronchiale [ 9 , 12 ]  . 
 nel nostro studio il rilievo radiografico pi frequente delle cisti mediastiniche costituito da opacit a margini netti le quali , nella maggior parte , determinano alterazione del profilo mediastinico , pi frequentemente lungo il margine destro , mentre in taluni casi lopacit risultata totalmente intramediastinica . 
le cisti con sede polmonare hanno rivelato ai radiogrammi pareti sottili ( 12 mm ) e contenuto totalmente aereo o con livello idro - aereo per comunicazione con lalbero tracheobronchiale : tale aspetto rilevabile anche in altre patologie polmonari cistiche , congenite o acquisite quali il sequestro polmonare , lascesso e la cisti idatidea ed in alterazioni a contenuto gassoso ( bolla di enfisema ) , da considerare nella diagnosi differenziale [ 5 , 7 , 19 ]  . le caratteristiche tc delle cisti broncogene sono variabili : talune lesioni , di meno frequente riscontro , presentano densit simile a quella dellacqua ( 020 hu ) che ne suggerisce la natura liquida [ 2 , 4 , 20 ]  . 
tuttavia pi spesso si riscontrano lesioni con elevata densit ( da 20 fino a 90 hu ) , simile a quella di altre strutture mediastiniche e di difficile differenziazione da masse solide quali linfomi ed adenopatie [ 3 , 4 , 12 , 21 , 22 ] : il liquido contenuto nelle cisti broncogene spesso una miscela a variabile contenuto proteico o radiol med ( 2008 ) 113 : 385394 fig . 
aspetto al radiogramma del torace ( a ) e alle ricostruzioni mpr in tc con mezzo di contrasto ( b , c )  . rarely , completely contained within the mediastinuat radiography , pulmonary cysts were thin - walled ( 12 mm ) and completely air - filled or with air - fluid levels , communicating with the tracheobronchial tree . 
this pattern is also seen in other congenital or acquired pulmonary cystic diseases , such as pulmonary sequestration , abscess , and hydatid cysts , and in gaseous alterations ( bullous emphysema ) , which have to be considered in the differential diagnosis [ 5 , 7 , 19 ]  . the ct features of bronchogenic cysts vary . 
higher - density lesions with attenuation similar to that of other mediastinal structures ( 2090 hu ) are more common and difficult to differentiate from solid masses such as lymphomas and adenopathy [ 3 , 4 , 12 , 21 , 22 ]  . 
measuring wall thickness may help in the differential diagnosis between bronchogenic cyst and malignant cystic tumours , as the presence of thick and irregular walls are suggestive of a necrotic lesion or lymphatic mass [ 23 ]  . mucinoso , spiegandone cos leterogeneit di attenuazione [ 4 ]  . 
la parete delle cisti solitamente sottile e liscia e , in alcuni casi , presenta enhancement dopo somministrazione endovenosa di mezzo di contrasto mentre il contenuto non modifica i valori di attenuazione [ 1 , 4 , 20 ] ; la valutazione dello spessore della parete pu aiutare ad orientarsi nella diagnosi differenziale fra tra cisti broncogena e tumori cistici maligni , deponendo la presenza di parete spessa ed irregolare per una neoplasia necrotica o una massa linfonodale [ 23 ]  . nel campione da noi esaminato la tc ha consentito di porre la diagnosi di cisti broncogena in 1 caso , grazie al riscontro di alcune caratteristiche quali il contenuto liquido e la sede sottocarenale , tipiche di questa lesione . 
in unaltra osservazione , la sede sottocarenale della lesione ha orientato verso la diagnosi di cisti broncogena : tuttavia lelevato valore di densit , non caratteristico , ha suggerito approfondimento diagnostico con rm . 
due lesioni a densit liquida sono state attribuite rispettivamente ad una generica formazione cistica e ad una cisti pleuro - pericardica : in questultimo caso la sede paracardiaca della lesione , estendentesi allangolo cardiofrenico , ha suggerito lipotesi di cisti mesoteliale . 
ancora , la sede paravertebrale di due lesioni , entrambe con densit dei tessuti molli , ha fatto prendere in radiol med ( 2008 ) 113 : 385394 in our series , ct enabled a diagnosis of bronchogenic cysts in one case , thanks to the characteristic findings of fluid content and subcarinal location . 
two fluid - density lesions were attributed to a nonspecific cystic mass and to a pleuropericardial cyst : in the latter case , the paracardiac location extending to the cardiophrenic angle was suggestive of a mesothelial cyst . 
the only two pulmonary cysts examined by ct were large and air - filled , features that supported a hypothesis of bullous emphysema or pneumothorax in one case . comparison of our data with those of mcadams [ 4 ] revealed some differences in the distribution of soft - tissuedensity lesions , which we believe to be related to the different populations considered in the two studies . 
in particular , whereas we confined our study to lesions diagnosed during adulthood , mcadams also considered cysts detected during childhood , a difference that also explains the smaller number of patients in our study . 
moreover , it should be noted that both studies were retrospective and thus suffer the limitations of the use of different techniques and devices . conclusions at conventional radiology , mediastinal bronchogenic cysts appeared as round or oval lesions with homogeneous density , whereas pulmonary bronchogenic cysts exhibited air - fluid levels or were completely air - filled . 
at ct , performed almost exclusively on mediastinal cysts , the lesions appeared as masses in the posterior and middle mediastinum , with well - defined margins and fluid or soft - tissue density . 
le uniche due cisti a sede polmonare esaminate mediante tc presentavano dimensioni voluminose e contenuto totalmente aereo ; tali caratteristiche hanno fatto propendere in un caso verso lipotesi diagnostica di bolla di enfisema oppure di falda di pneumotorace . confrontando i nostri dati con quelli di mc adams et al . [ 4 ] si possono apprezzare alcune differenze nella distribuzione delle lesioni delle sottoclassi con densit dei tessuti molli , correlabili a nostro avviso alle differenti popolazioni prese in esame nei due lavori : noi , in particolare abbiamo selezionato solamente le lesioni diagnosticate in et adulta mentre mc adams ha preso in considerazione anche le cisti diagnosticate in et infantile ; ci spiega anche il numero pi ridotto di pazienti reclutati nel nostro studio . 
inoltre , occorre considerare la natura retrospettiva e lutilizzo di diverse tecniche ed apparecchiature come un limite di entrambi gli studi . conclusioni alla radiologia tradizionale le cisti broncogene mediastiniche si sono manifestate quali lesioni tondeggianti od ovalari con densit omogenea ; le cisti broncogene polmonari hanno presentato invece livello idro - aereo oppure contenuto totalmente aereo . 
allo studio tc , che ha interessato quasi esclusivamente le cisti a sede mediastinica , tali lesioni si sono rivelate quali masse localizzate nel mediastino posteriore e medio , a margini ben definiti e di densit liquida o dei tessuti molli . 
le cisti a densit liquida possono essere diagnosticate in modo abbastanza affidabile con tc basale , mentre quelle con densit solida , che nella nostra casistica hanno rappresentato la maggioranza , devono essere studiate mediante tc da eseguire sia in condizioni basali sia con mezzo di contrasto per valutare leventuale enhancement , assente nelle cisti broncogene . 
 table 3 classification of diagnostic likelihood based on computed tomography features location ct density sede densit tc level 1 : likely diagnosis typical fluid 4 cases 1 livello : diagnosi probabile tipica liquida 4 casi level 2 : possible diagnosis atypical typical fluid 10 cases 2 cases solid 2 livello : diagnosi possibile atipica liquida 10 casi tipica solida 2 casi level 3 : unlikely diagnosis atypical solid 3 livello : diagnosi improbabile atipica solida tabella 3 classificazione di probabilit diagnostica delle cisti mediastiniche sulla base della localizzazione e della densit ad esame tc 394 radiol med ( 2008 ) 113 : 385394 whereas solid cysts , the majority of lesions in our series , require preand postcontrast ct to identify internal enhancement , which is absent in bronchogenic cysts . ct suggests the bronchogenic origin of mediastinal cysts when it demonstrates fluid content and subcarinal location , which are almost exclusive to these lesions . 
fluid - density lesions in other than subcarinal locations may be due not only to bronchogenic cysts but also to cystic masses with similar ct appearance ( enterogenous cysts , pleuropericardial cysts ) , which need to be included in the differential diagnosis ( table 3 )  . despite the limited number of cases examined , we can confirm the improved diagnostic yield of ct performed before and after administration of iodinated contrast material ( five cases )  . 
where diagnostic uncertainty persists , mri is believed to be helpful , even though it was never used on our study . possiamo affermare che la tc consente di ipotizzare lorigine broncogena delle cisti mediastiniche quando ne dimostri il contenuto liquido e la sede sottocarenale , caratteristiche riscontrabili quasi esclusivamente in tale lesione . le lesioni a densit liquida , ma con sede differente da quella sottocarenale possono invece essere attribuite non solamente a cisti broncogene ma anche a lesioni cistiche di simile aspetto tc ( cisti enterogena , cisti pleuro - pericardica ) , con le quali si impone la diagnosi differenziale ( tabella 3 )  . nonostante lesiguit della casistica presentata possiamo affermare la maggiore resa diagnostica delle indagini tc effettuate sia in condizioni basali sia con mezzo di contrasto iodato ( 5 casi ) : le scansioni basali sono infatti essenziali per escludere la presenza di enhancement lesionale , elemento diagnostico importante quando tali lesioni , presentandosi a contenuto denso , possano simulare una lesione solida . 
lucaya and strife plus their international team are back on the lime with a most impressive second edition of their book . there have been many changes in it : apart from the number of pages ( from 304 to 448 ) , the number of figures ( from 303 in 578 images in the first edition to 445 in 925 images 54 of them in colour in the present one ) it is the number and the topic of the single chapters ( 18 now from the previous 16 ) which makes the difference . some chapters ( 10 ) have the same title of the previous edition : chest ultrasound ( us ) ; the contribution of nuclear medicine to pulmonary imaging ; high - resolution ct of the lung in children ; pulmonary malformations beyond the neonatal period ; pediatric tuberculosis ; imaging evaluation of the thymus and thymic disorders in children ; lymphoma controversies in imaging the chest ; chest tumours other than lymphoma ; thoracic manifestations of systemic diseases ; radiology of the chest wall ; 4 have slight , not significant changes : helical multidetector chest ct ; ct of acute pulmonary disease : infection , infarction , and trauma ; foreign body aspiration : imaging aspects ; pediatric cardiac mri ; 1 a different target : how to perform ad interpret mr sleep studies for obstructive sleep apnea in children and 3 are completely new : pediatric cardiac ct ; fetal mri of the chest ; neonatal chest imaging , being quite impressive and information rich . 
apart from the new chapters all the old ones have been enlarged , up - dated and enriched by new images as in the previous edition , the present one aims to make fa sempre piacere il vedere la seconda edizione di un testo di medicina : significa che la prima ha avuto successo . cinque anni dopo la prima edizione i colleghi lucaya e strife con la collaborazione della loro squadra internazionale sono tornati sulla scena editoriale con una importante seconda edizione del volume da loro curato . sono parecchie e sostanziali le modifiche ritrovabili : non solo considerando il diverso numero delle pagine ( da 304 a 448 ) , delle figure ( dalle 303 in 578 immagini della prima edizione alle 445 con 925 di cui 54 a coloridellattuale ) ma anche il numero e gli argomenti dei singoli capitoli ( 18 ora dai 16 precedenti ) che fanno la differenza con la prima edizione . 
 alcuni capitoli ( 10 ) hanno lo stesso titolo della prima edizione : chest ultrasound ( us ) ; the contribution of nuclear medicine to pulmonary imaging ; high - resolution ct of the lung in children , pulmonary malformations beyond the neonatal period ; pediatric tuberculosis ; imaging evaluation of the thymus and thymic disorders in children ; lymphoma controversies in imaging the chest ; chest tumours other than lymphoma ; thoracic manifestations of systemic diseases ; radiology of the chest wall ; 4 presentano lievi modificazioni : helical multidetector chest ct ; ct of acute pulmonary disease : infection , infarction , and trauma ; foreign body aspiration : imaging aspects ; pediatric cardiac mri ; 1 un argomento diverso : how to perform ad interpret mr sleep studies for obstructive sleep apnea in children and 3 sono completamente nuovi : pediatric cardiac ct ; fetal mri of the chest ; neonatal chest imaging , molto importanti e ricchi di informazioni . al contrario e purtroppo con dispiacere il capitolo su pulmonary manifestations of aids stato cancellato a causa della morte del suo estensore . 
escludendo i nuovi capitoli , tutti i precedenti sono stati allargati , ammodernati ed arricchiti da nuove immagini . come nella precedente edizione anche lattuale intende porgere al lettore informazioni circa le pi avanzate 462 radiol med ( 2008 ) 113 : 461463 the reader to be informed about the most up - dated techniques and modalities ( us , nuclear medicine pet and pet / ct , high - resolution chest ct , helical ct , pediatric cardiac ct and cardiac mri ) allowing the best and possibly precise diagnosis of chest diseases in children , at all ages , from tiny new - borns and prematures to grown - up adolescents . some chapters have been thoroughly enlarged , encompassing images and data derived from the above modalities i.e. 
 among the good things of this edition the use of colour in identifying summary boxes of technical data and doses , diagnostic procedures and protocols is relevant and will be much appreciated . 
 noteworthy are also changes in the values of technical parameters to be used for high resolution ct ( 90120 kvp instead of 120140 ; 2040 ma instead of 2550 ) , which , in authors hands deliver depending on agea dose between 10% and 20% of that used for a helical procedure ; and once more the stress given to expiratory ct scans in the detection of air trapping in lung diseases . as already stated in the review of the previous edition the authors have largely ousted general anaesthesia , sparingly used , as well as sedation , further reduced as well ( 1 , 5% in children under the age of 6 years ) by the use of helical ct and hrct . 
 at the end of each chapter reference lists have been significantly increased and accordingly to the draw - back always to be found in a book updated as much as possible to recent data , making them a further implement to the utility of the book . images using all possible modalities are of superior quality and perfect reproduction . all along the book , especially in chapters regarding cardiac ct and mr , the reader will find a large use of acronyms : this is in some way distressing if one is not familiar with their meaning . 
distressing is also the in extenso quotation of long lists of authors reference names ( a feature of the series )  . wherever possible stress is drawn on nuclear medicine imaging , most of all the use of 18 f - fdg - pet and pet - ct in detection and characterisation of lymphomatous lesions ( lung nodules etc . ) having it replaced gallium as the preferred functional imaging modality for staging of lymphomas . 
 modalit e tecniche di indagine ( ecografia , medicina nucleare pet e pet / ct , tc ad alta risoluzione del torace , tc spirale , cardio tc e cardio rm ) che possono permettere la diagnosi migliore e pi precisa delle malattie polmoni nei bambini di tutte le et , dal pi piccolo neonato e prematuro alladolescente . 
 alcuni capitoli sono stati diffusamente ingranditi , utilizzando le immagini ed i dati derivanti dalle tecniche di cui sopra , in particolare mediante i contributi della medicina nucleare allo studio per immagini del polmone , allimpiego della tc spirale multidetettore od alla tc ad alta risoluzione . 
 tra le novit , significativo luso del colore nellidentificazione delle tabelle e degli schemi dei dati tecnici , delle dosi , delle procedure e dei protocolli diagnostici , novit che sar assai apprezzata . notevoli sono poi anche i cambiamenti dei parametri tecnici di esecuzione della ct ad alta risoluzione ( 90120 kvp invece di 120140 ; 2040 ma invece of 2550 ) , dati che , nelle mani degli autori , ed a seconda dellet del paziente , forniscono una dose dal 10% al 20% di quella impartita da una tc spirale . 
ancora una volta poi viene ribadita limportanza della ripresa in fase tc espiratoria nei casi in cui necessario dimostrare la presenza di intrappolamento di aria nelle malattie polmonari . come gi segnalato nella recensione della precedente edizione , gli autori hanno nettamente ridotto se non del tutto eliminato limpiego dellanestesia generale , nonch ulteriormente ridotto la sedazione ( ora impiegata nell1 , 5% dei bambini al di sotto dei 6 anni ) mediante limpiego della tc spirale e della tc ad alta risoluzione . 
 credo che le sezioni del libro che si occupano di tali argomenti dovrebbero essere studiate con attenzione sia dai radiologi che dagli anestesisti coinvolti in questo tipo di indagini . al termine di ogni capitolo la bibliografia stata ampiamente aumentata ed aggiornata per quanto possibile , nota dolente di ogni libro , rendendola un utile ed importante ausilio per il lettore . le immagini utilizzate , di qualsiasi modalit impiegata , sono di alta qualit e riproduzione perfetta . il lettore , nello scorrere il volume , trover un ampio uso di acronimi : ci in particolare nei capitoli riguardanti tc e rm : uso spesso defatigante , in particolare per chi non famigliare con il loro significato . 
defatigante anche luso di lunghi elenchi di nomi in extenso degli autori di riferimento ( caratteristica per della serie ) ovunque ci possibile viene data importanza alle indagini di medicina nucleare , in particolare alluso del 18 f - fdg - pet e della pet - ct nella valutazione e caratterizzazione delle alterazioni linfomatose ( noduli polmonari ecc . ) avendo queste metodiche sostituito il gallio come immagine funzionale di riferimento per la stadiazione dei linfomi . 
 da rilevare alcuni errori nella segnalazione di figure a few mistakes in referring the reader to figures are to be come anche pochi errori tipografici . radiol med ( 2008 ) 113 : 461463 met , as well as a few printing misprints . as written in my previous review , since the book is a joint effort , the same condition can be mentioned in more than one chapter : this is not a flaw , on the contrary , since repetita iuvant particularly when described and treated in different ways according to the writers abilities . once more i believe this book to be of great theoretical and practical importance and stress this opinion . 
i hope it will be used at large non only by paediatric radiologists but also by all radiologists who have to deal with chest disease in children as well as by paediatricians , pneumologists and paediatric surgeons . 
in any case it should become a must in all radiology schools . come scritto nelle recensione della precedente edizione , dal momento che questo il risultato di uno sforzo comune , possibile che la stessa alterazione venga segnalata in pi di un capitolo . 
questo non un errore , al contrario , dato che repetita iuvant tenuto anche conto delle differenze nella capacit di scrittura degli autori . ancora una volta ritengo che questo volume sia si grande importanza , sia teorica che pratica e ribadisco qui questa opinione . 
spero che esso venga usato ampiamente non soli dai radiologi pediatrici ma anche da tutti i radiologi che hanno a che fare con malattie polmonari del bambino , come anche da pediatri , pneumologi , anestesisti e chirurghi pediatrici . 
bergamaschi1 1istituto di medicina del lavoro delluniversit cattolica del sacro cuore , largo gemelli 8 , 00168 roma , italy 2istituto nazionale di riposo e cura dellanziano ( inrca ) , u.o. 
radiologia , roma , italy 3istituto di bioetica delluniversit cattolica del sacro cuore , roma , italy 4dipartimento di bioimmagini e scienze radiologiche , universit cattolica del sacro cuore , roma , italy 5medico del lavoro , roma , italy 6ministero dellambiente , roma , italy correspondence to : n . 
female radiologists and radiotherapists showed higher levels of organisational discomfort than their male colleagues . younger and less experienced radiologists and radiotherapists had higher strain scores than their older and more experienced colleagues . 
i partecipanti a due congressi sono stati invitati a compilare un questionario composto da quattro diverse sezioni per misurare il rischio ( disagio , contenuto del lavoro secondo il modello di karasek , discrepanza tra impegno e risultati secondo il modello di siegrist , e soddisfazione lavorativa secondo warr ) e quattro sezioni per misurare gli effetti dello stress da lavoro ( ansia e depressione secondo il questionario di goldberg , malessere secondo il general health questionnaire , stili di vita )  . 
nelle risposte rilevate , i medici del campione analizzato esprimono mediamente elevati livelli di discrezionalit , di ricompensa e di soddisfazione dal lavoro , che tuttavia si associano ad un elevato livello di disagio per le condizioni di lavoro nel 38 , 5% degli specialisti . 
il 24% degli intervistati si trova in condizioni di job strain , il 28% soffre per la discrepanza tra impegno prestato sul lavoro e risultati ottenuti , il 25% insoddisfatto del lavoro . 
 necessario un impegno specifico per la prevenzione di tale condizione . parole chiave radiologi radioterapisti stress da lavoro introduction introduzione physicians are exposed to major occupational stress factors . studies conducted in northern europe reported that physicians have a higher - than - average risk of suffering from one of the so - called three ds ( drugs , drink and depression ) , which can lead to higher suicide rates [ 1 , 2 ]  . 
as a consequence , each category of physicians can be said to be exposed to a specific type of occupational risk , which is intrinsically related to the type of activity performed . 
in particular , radiologists and radiotherapists are confronted with a variety of occupational stress factors that bring about feelings of discomfort and may lead to a higher frequency of clinical errors [ 4 ]  . 
among the causes of discomfort is the introduction of hospital diagnostic - related groupings and the heavier workload expected of health professionals to ensure that increasingly higher goals are reached . 
this effort has probably not been fully understood and appreciated by the other components of the medical community , and this may have heightened the sensation of isolation and stress felt by radiologists . 
 this study , the first of its kind , aimed at analysing the relevance and extent of occupational stress factors in a large sample of radiologists and radiotherapists and examining the effects of work stress on the subjects health . materials and methods specialist physicians participating in two radiology and oni medici sono una categoria esposta a rilevanti fattori di stress professionale . 
in studi condotti nel nord europa stato osservato che i medici hanno pi probabilit della media di soffrire di una delle cosiddette tre d : drug , drink and depression , che determinano un elevato tasso di suicidi [ 1 , 2 ]  . 
in particolare i radiologi e i radioterapisti devono fronteggiare una serie di fattori di stress professionali specifici , che sono allorigine di condizioni di disagio e che potrebbero determinare un aumento della frequenza degli errori clinici [ 4 ]  . 
tra le cause di disagio , vengono segnalati lintroduzione dei drg ospedalieri e il conseguente aumento dei carichi di lavoro richiesti agli operatori sanitari per il raggiungimento di obiettivi sempre pi elevati . 
in ambito diagnostico inoltre levoluzione tecnologica ha imposto il ricorso a tecniche innovative e pi complesse per semeiotica e quantit di dati da analizzare ( tomografia computerizzata , tomografia computerizzata multistrato , risonanza magnetica , ecografia , radiologia interventistica , ecc . ) , che hanno sostituito in gran parte la radiologia tradizionale , aumentando allo stesso tempo la difficolt della refertazione e il relativo tempo necessario . 
nessuna categoria professionale , come i radiologi , ha dovuto aggiornare le proprie conoscenze in modo altrettanto rapido e profondo nellultimo decennio : questo sforzo non stato probabilmente compreso e apprezzato fino in fondo dalle altre componenti del panorama sanitario , e ci potrebbe aver contribuito ad aumentare la sensazione di isolamento e stress nei radiologi . 
 con questo studio - pilota , che il primo del genere , abbiamo inteso analizzare il rilievo e la portata dei fattori di stress professionale in un consistente numero di radiologi e radioterapisti , esaminando gli effetti sul loro stato di salute . radiol med ( 2008 ) 113 : 329346 cology radiotherapy conferences were invited to complete an anonymous questionnaire investigating workplace stress , health and lifestyles as part of a study on medical malpractice and diagnostic errors . 
to investigate occupational stress we , used eight psychodiagnostic instruments : four questionnaires measuring risk ( discomfort , job content , effort - reward imbalance and job satisfaction ) and four measuring the health effects of occupational stress ( anxiety , depression , distress , lifestyle )  . occupational discomfort the first part of the questionnaire , devised by a focus group of radiologists and radiotherapists , asked respondents to provide demographic data ( gender , age group , years of experience , professional role or qualification , public or private practice ) and included a series of items relating to malpractice and the causes of medical error . 
the focus group identified eight factors for occupational discomfort ; for each one , participants were asked to rate their response according to a numerical - verbal likert scale between ( 1 ) totally irrelevant and ( 5 ) highly relevant . 
seven questions were selected that related to seven factors intrinsic to work : excessive workload , insufficient time , obsolete equipment , lack of opportunity to consult with colleagues , inadequate continuing education , poor work organisation and uncooperative and tense work climate [ 4 ]  . 
the indicator of discomfort and negative experiences was calculated by adding up the relevant answers and had a score ranging from 7 to 35 . the second part of the questionnaire included the italian version of a series of standard questionnaires modified to adapt them to the sample being studied . 
the questionnaires were chosen , from among the many present in the literature , on the basis of availability , simplicity , brevity and applicability , as demonstrated by international studies , to populations composed of working ( and therefore healthy ) subjects rather than psychiatric patients . 
 occupational stress occupational stress was evaluated on the basis of the two most widely used questionnaires in the international literature : karaseks job content questionnaire ( jcq ) and siegrists effort - reward imbalance ( eri )  . the jcq is based on the principle that the relationship between high job demands and low control leads to a state of perceived job strain [ 5 ]  . 
the shorter version , used in our materiali e metodi i medici specialisti partecipanti a due congressi di radiologia e di radioterapia oncologica sono stati invitati a compilare un questionario anonimo , che indagava il livello di tensione lavorativa , la salute e gli stili di vita , nellambito di una ricerca sul tema della malpractice medica e degli errori diagnostici . 
complessivamente , nellindagine sullo stress sono stati utilizzati otto strumenti psicodiagnostici : quattro questionari per misurare il rischio ( disagio , contenuto del lavoro , discrepanza tra impegno e risultati e soddisfazione lavorativa ) e quattro per misurare gli effetti dello stress da lavoro ( ansia , depressione , malessere , stili di vita )  . disagio la prima parte del questionario richiedeva lindicazione di alcuni dati anagrafici ( sesso , classe di et , anni di esperienza professionale , ruolo o qualifica professionale , tipo di attivit professionale pubblica o privata ) e conteneva una serie di domande relative alla malpractice ed alle cause di errore medico , elaborate mediante un focus group di radiologi e radioterapisti . 
il focus group aveva identificato otto fattori di disagio lavorativo ; per ciascuno di essi i partecipanti allindagine sono stati invitati a graduare la propria risposta secondo una scala analogica verbale - numerica di likert tra ( 1 ) assolutamente non rilevante e ( 5 ) molto importante . 
sono state estratte sette domande relative ad altrettanti fattori intrinseci del lavoro : ritmi di lavoro eccessivi , tempi insufficienti , macchine obsolete , mancanza di possibilit di consultazione con colleghi , insufficiente aggiornamento professionale , cattiva organizzazione del lavoro , clima lavorativo non collaborativo e carico di tensioni [ 4 ]  . 
lindicatore di disagio ed esperienze negative , composto addizionando le relative risposte , assume un punteggio che pu essere compreso tra 7 e 35 . la seconda parte del questionario conteneva la versione italiana di alcuni questionari standardizzati , con opportune modificazioni necessarie per adeguarli alla casistica in oggetto . 
i questionari sono stati scelti , tra i numerosi presenti in letteratura , per criteri di diffusione , semplicit e brevit , oltre che per la applicabilit , documentata nel corso di studi internazionali , su popolazioni composte da soggetti in attivit lavorativa ( e quindi sani ) piuttosto che su pazienti psichiatrici . 
 stress da lavoro lo stress da lavoro stato valutato mediante i due modelli pi diffusi nella letteratura internazionale : lo job content questionnaire ( jcq ) di karasek e leffort - reward imbalance ( eri ) di siegrist . 332 radiol med ( 2008 ) 113 : 329346 study , comprises 17 questions , of which five relate to job demands , six to control and six to social support . 
both the complete and short versions have been applied in comparisons between different occupations , where they provided identification of four working conditions : ( 1 ) high strain , i.e. 
high demands with low control ; ( 2 ) passive , low demands with low control ( typical of jobs that fail to challenge the individuals capabilities , with high levels of dissatisfaction ) ; ( 3 ) active , high demands with high control ( jobs characterised by a high degree of training and that require quick action and a high degree of responsibility ) ; ( 4 ) low strain , low demand with high control ( ideal working situation in which the individual can manage his or her own time )  . 
karaseks original model was further expanded in the 1980s with the addition of social support as a third dimension , which has a mitigating effect on job strain [ 20 ]  . 
the term isostrain refers to high strain in conjunction with low social support [ 6 ]  . siegrists eri [ 21 ] is based on a model that conceives workplace stress as an imbalance between the effort put into a job and the rewards received in return . 
the ratio between effort and reward is a continuous variable that expresses the imbalance between the two variables ; the upper quartile of the distribution is believed to contain subjects at risk of workplace stress . 
an attempt to combine the two models into a single questionnaire ( by means of factorial analysis and logistic regression ) did not yield encouraging results [ 32 ]  . 
hence , we decided to use the two instruments separately . job satisfaction a quantity that is closely , though inversely , related to workplace stress is the degree of satisfaction derived from ones job . 
the questionnaire includes ten il modello del jcq si fonda sul principio che la relazione tra elevata domanda lavorativa e bassa discrezionalit intesa come possibilit decisionali permesse al soggetto definisca una condizione di tensione lavorativa percepita o job strain [ 5 ]  . 
la versione pi concisa del questionario , da noi usata , si articola in 17 domande , cinque riferite alle richieste del lavoro , sei al controllo sul lavoro , sei al sostegno sociale . 
al pari della versione maggiore , essa stata applicata ai confronti tra diverse attivit professionali , nelle quali consente di identificare quattro condizioni di lavoro , caratterizzate da : ( 1 ) alta tensione ( high strain ) , ossia elevata domanda con bassa facolt di decisione ; ( 2 ) passivo ( passive ) , bassa domanda con bassa facolt di decisione ( tipica di mansioni che non incentivano le capacit individuali , con marcati livelli di insoddisfazione ) ; ( 3 ) attivo ( active ) , elevata domanda con elevata facolt di decisione ( occupazioni caratterizzate da un elevato grado di apprendimento e che impongono allindividuo un intervento in tempi rapidi e con elevata responsabilit ) ; ( 4 ) bassa tensione ( low strain ) , bassa domanda con elevata facolt di decisione ( situazione lavorativa ottimale , in cui lindividuo pu gestire in autonomia il suo tempo lavorativo )  . 
in alternativa , il questionario consente di ricavare una misura dello stress da lavoro o job strain , inteso come variabile continua derivante dal rapporto tra richieste di lavoro ( demand ) e controllo ( control )  . 
il modello originale di karasek stato arricchito negli anni 80 , con laggiunta di una terza dimensione , il sostegno sociale , che esplica una funzione moderatrice sullo stress da lavoro [ 20 ]  . 
il termine isostrain si riferisce a condizioni di alta tensione lavorativa , associate con basso supporto sociale [ 6 ]  . leri di siegrist [ 21 ] si basa su un modello che concepisce lo stress da lavoro come una discrepanza tra limpegno prestato ed i risultati raggiunti , e indaga inoltre un terzo fattore ossia leccessivo impegno ( overcommitment ) , che esplica un effetto aggravante della condizione di stress . anche questo strumento stato tradotto in numerose lingue [ 2228 ] , ed applicato nei pi diversi settori produttivi e , spesso , in campo sanitario [ 2931 ]  . 
in questa indagine abbiamo impiegato la versione pi concisa , con cinque domande riferite allo sforzo ( effort ) , nove alla ricompensa ( reward ) , sei alleccessivo impegno ( overcommitment )  . 
il rapporto tra sforzo e ricompensa una variabile continua ed esprime la discrepanza ( imbalance ) tra le due variabili ; si ritiene che il quartile superiore della distribuzione contenga i soggetti a rischio di stress da lavoro . radiol med ( 2008 ) 113 : 329346 items , which respondents are invited to rate on a seven - point likert scale . 
a score of 35 represents the midpoint between satisfaction and dissatisfaction , so scores lower than 35 express prevalent dissatisfaction . leccessivo impegno rappresenta un fattore aggravante . i due modelli ( jcq e eri ) forniscono contributi differenziati e complementari alla valutazione dello stress da lavoro . 
un tentativo di combinare i due modelli , ricavando un unico questionario ( mediante analisi fattoriale e regressione logistica ) , non ha fornito risultati incoraggianti [ 32 ]  . 
da ci la nostra decisione di utilizzarli entrambi . psychological well - being soddisfazione dal lavoro psychological well - being at the time of the study was evaluated using goldbergs general health questionnaire ( ghq ) [ 32 , 3541 ] in its shortest available version consisting of 12 items . 
each item of the ghq - 12 offers the choice of four responses , which can either be interpreted in a bimodal fashion or with an increasing score in the manner of a normal likert scale . adoption of the former or latter method only influences the frequency of subjects classified as possible cases but not the validity of results at the group level [ 42 ]  . if a four - point likert scale is used , the results will better approach the normal distribution . 
the final score ranges from 12 to 48 points ; low values correspond to complete well - being , whereas higher values are indicative of distress . in contrast , if the bimodal scoring system is used , in which zero points are assigned to responses indicating well - being and one point to those indicating distress , a score higher than five suggests a possible case of distress . the second measure of mental health was derived from goldbergs anxiety and depression scales ( ads ) [ 43 ]  . this very simple indicator was developed as a screening tool for use by general practitioners and designed to identify subjects at risk of anxiety and depression deserving of referral to specialised services . 
high scores ( at least 16 points on the anxiety scale , i.e. , at least seven positive responses , and 15 points on the depression scale , i.e. , six positive responses ) indicate that the subject may be at risk of anxiety or depression . health and lifestyles physical health and lifestyle were investigated with a scale comprising 13 items relating to the use of tobacco and alcohol , the frequency of medical check - ups , awareness of blood pressure and lipid levels , physical exercise , body weight , dietary habits , sleep habits , frequency of back ache and feelings of being stressed . 
per valutare questa variabile abbiamo usato il questionario messo a punto da warr [ 33 , 34 ] , nella versione specificamente impiegata per indagini su popolazioni composte da medici [ 35 ]  . 
il punteggio di 35 punti rappresenta lequivalenza tra soddisfazione e insoddisfazione , quindi i punteggi inferiori a 35 esprimono prevalente insoddisfazione dal lavoro . benessere psicofisico lo stato di benessere psicofisico al momento dellindagine stato valutato tramite il general health questionnaire di goldberg [ 32 , 3541 ] , nella versione pi breve tra quelle disponibili , in 12 domande . 
ciascuna delle domande del ghq - 12 prevede quattro risposte , che possono essere interpretate con un punteggio dicotomo , o con un punteggio crescente come una comune scala likert . 
ladozione di uno o dellaltro metodo influenza solo la frequenza di soggetti classificabili come possibili casi , ma non la validit dei risultati a livello di gruppo [ 42 ]  . 
impiegando invece il punteggio dicotomo , nel quale si assegnano rispettivamente zero punti alle risposte che indicano benessere e un punto a quelle che esprimono malessere , il punteggio superiore a 5 indica un possibile caso di malessere . una seconda misura di salute mentale stata ottenuta dalle scale di ansia e depressione elaborate dallo stesso goldberg [ 43 ]  . 
si tratta di un indicatore molto semplice , studiato per essere applicato dal medico di medicina generale durante lattesa in ambulatorio e finalizzato ad indicare il rischio di una patologia la cui diagnosi richiede ulteriori accertamenti . 
anche questo questionario stato larga334 radiol med ( 2008 ) 113 : 329346 healthy lifestyle , whereas higher scores indicate unhealthy lifestyles . statistical analysis we distributed 350 questionnaires at the two congresses : 321 were returned , of which seven were discarded as being incomplete . 
a total of 314 physicians therefore responded to the questionnaires , equivalent to a response rate of 89.7%. analysis of the responses , exhaustively described in our previous paper [ 4 ] , did not reveal any significant differences between the radiologists and radiotherapists with regard to demographics or responses to individual items . 
as a result , the sample was analysed as a single group . data were analysed with the spss software package ( statistical package for social sciences ) , version 14.0. analysis of the frequency of individual variables was conducted using descriptive statistics . 
comparisons between groups were performed with the mann - whitney u test for nonparametric data in the case of two independent groups and with the kruskal - wallis test in the case of three or more . 
the correlation among variables was studied using spearmans rho for nonparametric data . the observation that the majority of variables showed high levels of asymmetry and kurtosis , often more than double the standard error , suggested a need for a logarithmic transformation of the variables before statistical tests based on the assumption of normal distributions could be applied . we applied simple linear regression to investigate the relationship between the normalised variables indicating workplace stress and those indicating negative health effects . results the demographic and occupational variables of our sample are shown in table 1 . 
the distribution shows a superguassian or leptokurtic distribution with a very sharp peak ( kurtosis 5.1 ) and skewed to the right ( skewness 1.7 ) due to the high prevalence of responses close to the value reflecting the highest level of occupational discomfort . we considered scores higher than 32 , corresponding to maximum discomfort for four out of the seven factors investigated , to be indicative of severe occupational discomfort . 
punteggi elevati ( almeno 16 punti per la scala dellansia , corrispondenti ad almeno sette risposte affermative su nove ; 15 punti , cio sei risposte affermative , per la scala della depressione ) indicano che il soggetto potrebbe essere a rischio di ansia e , rispettivamente , di depressione . salute e stili di vita lo stato di salute fisica e gli stili di vita sono stati indagati con una scala composta da 13 domande che indagano labitudine al fumo ed allalcol , la frequenza dei controlli medici , la conoscenza dei propri valori pressori e lipemici , lesercizio fisico , il peso corporeo , la dieta , il sonno , la frequenza del mal di schiena e della sensazione di essere stressato . 
il punteggio di 13 corrisponde al migliore stile di vita , punteggi pi elevati sono indicativi di abitudini dannose per la salute . analisi statistica nelle sedi congressuali sono stati distribuiti 350 questionari ; i medici ne hanno restituiti 321 e di questi 7 sono stati scartati perch incompleti . 
lanalisi delle risposte , estesamente riportata nella precedente pubblicazione [ 4 ] , non ha evidenziato alcuna differenza significativa tra radiologi e radioterapisti , n per quanto riguarda i dati anagrafici , n per le risposte alle singole domande . 
i confronti tra gruppi sono stati effettuati con il test u di mann whitney per dati non parametrici se i gruppi indipendenti erano due , e con il test di kruskal wallis se erano tre o pi . 
la correlazione tra le variabili indagate stata studiata con il rho di spearman per dati non parametrici . losservazione che la maggior parte delle variabili presentava valori elevati di asimmetria e di curtosi , spesso pi che doppi rispetto allerrore standard , ha reso necessario operare la trasformazione logaritmica delle variabili prima dellapplicazione di test statistici basati sullassunzione di normalit delle distribuzioni . 
abbiamo applicato la regressione lineare semplice per indagare la relazione tra le variabili normalizzate che esprimono stress da lavoro e quelle che indicano danni per la salute . radiol med ( 2008 ) 113 : 329346 table 1 sample demographics entire group age range ( years ) 3640 4145 4650 5155 5560 3640 4145 4650 5155 5560 no . 
heads of division or heads of department ( p < 0.0001 ) and among specialists with less than 5 years of risultati le caratteristiche anagrafiche e lavorative del gruppo esaminato sono riportate nella tabella 1 . 
la distribuzione assume un andamento che si definisce supergaussiano o leptocurtico , cio con un picco molto aguzzo ( curtosi 5 , 1 ) e asimmetrico a destra ( skewness = 1 , 7 ) , per la spiccata prevalenza di risposte prossime al valore che esprime il massimo disagio ambientale . 
tale punteggio riportato da 121 colleghi , pari al 38 , 5% degli intervistati . il disagio significativamente maggiore nei radiologi / radioterapisti donne ( test u di mann whitney , p < 0 , 0001 ) rispetto ai colleghi maschi ; in coloro che operano nelle strutture pubbliche rispetto ai privati ( p < 0 , 007 ) ; nei dirigenti medici di i livello rispetto ai dirigenti di ii livello e ai direttori di struttura semplice e complessa ( p < 0 , 0001 ) ; negli specialisti con meno di cinque anni di attivit ( test di kruskal wallis p < 0 , 011 )  . 
non si rilevano differenze tra radiologi e radioterapisti . stress da lavoro lo stress da lavoro secondo il modello di karasek ricavato dal rapporto tra la variabile che esprime il carico di lavoro e di responsabilit ( demand ) e quella che indica la discrezionalit gestionale ( control )  . 
il carico di lavoro ha una curva piuttosto stretta , raggruppata attorno a valori di 16 punti , che esprimono un impegno di lavoro elevato per tutti i radiologi / radioterapisti intervistati ( curva deviata a destra , con asimmetria pari a 0 , 7 )  . 
la variabile che deriva dal rapporto tra domanda e controllo , denominata tensione percepita o job strain , presenta valore medio pari a 1 , 18 , indicando quindi che la tensione nel gruppo maggiore rispetto allideale equivalenza tra carico di lavoro e capacit di controllo . 
there were no differences between radiologists and radiotherapists . occupational stress occupational stress according to karaseks model is derived from the relationship between the variable relating to workload and demands and the variable indicating control . 
in the presenta valori mediamente elevati , con prevalenza dei soggetti con un livello di supporto maggiore della media ( asimmetria negativa della curva )  . dividendo i valori rilevati di demand e control al di sopra e al di sotto della mediana , si ricavano nel campione le quattro categorie sopra descritte come alta o bassa tensione , attivo e passivo ( tabella 3 )  . 
suddividendo in tre terzili la variabile job strain ottenuta dal rapporto tra domanda e controllo , e in altrettanti terzili la variabile soradiol med ( 2008 ) 113 : 329346 table 3 subdivision of the sample into categories of job content identified according to karaseks job content questionnaire [ 5 ] control total high number ( % ) number ( % ) number ( % ) passive 80 ( 25.5% ) low strain 89 ( 28.3% ) 169 ( 53.8% ) high strain 75 ( 23.9% ) active 70 ( 22.3% ) 145 ( 46.2% ) 155 ( 49.4% ) 159 ( 50.6% ) 314 ( 100.0% ) tabella 3 suddivisione della popolazione nelle categorie che caratterizzano il contenuto del lavoro ( job content ) secondo il modello di karasek [ 5 ] demands low bassa domanda high alta total totale control totale basso alto numero ( % ) numero ( % ) numero ( % ) passivo 80 ( 25 , 5% ) bassa tensione 89 ( 28 , 3% ) 169 ( 53 , 8% ) alta tensione 75 ( 23 , 9% ) 155 ( 49 , 4% ) 159 ( 50 , 6% ) attivo 70 ( 22 , 3% ) 314 ( 100 , 0% ) 145 ( 46 , 2% ) sample considered , both of these variables had an approximately normal distribution ( table 2 )  . 
the variable derived from the relationship between job demands and control or perceived job strain had a mean value of 1.18 , indicating that the group perceives a higher level of strain compared with an ideal situation in which workload and control are equal . 
the curve appears fairly flat because of the high dispersion of values , suggesting a wide variety of experiences in terms of job strain within the same sample . social support generally had high values , with a prevalence of subjects with higher levels of social support than average ( negative skewness of the curve )  . by dividing the demand and control values above and below the median , we obtained the four categories of high or low strain , active and passive ( table 3 )  . 
after splitting the variable job strain derived from the demand and control ratio and the variable social support into tertiles , 54 subjects ( 17.2% of the group ) were in a situation of isostrain , that is , a high level of strain ( upper tertile ) and a low level of social support ( lower tertile ) ( table 4 )  . 
situations of low social support can be seen to affect mostly subjects with high levels of job strain ( pearsons chi - square test equal to 13.5 , p = 0.09 ) , thus increasing the potential harm of workplace stress . 
possibile osservare che le condizioni di basso sostegno sociale riguardano soprattutto i soggetti con elevata tensione lavorativa ( test del 2 di pearson pari a 13 , 5 , p = 0 , 09 ) , cos aumentando la potenziale nocivit dello stress da lavoro . la tensione da lavoro e il sostegno sociale non variano significativamente nei due sessi n a seconda del tipo di struttura in cui si lavora , pubblica o privata . 
si osserva che lo strain maggiore nei dirigenti di i livello e nei responsabili di struttura semplice rispetto ai direttori ( p < 0 , 004 ) , mentre il sostegno sociale risulta maggiore tra i direttori ( p < 0 , 001 )  . 
alle domande relative allimpegno nellattivit lavorativa ( effort ) i medici intervistati rispondono in modo piuttosto differenziato , cos che la distribuzione della variabile si allontana dalla normalit per una elevata curtosi negativa . 
le ricompense ottenute dal lavoro ( reward ) sono mediamente elevate ( punteggio medio superiore a 42 in una scala da 11 a 55 , asimmetria di segno negativo )  . 
lo stress da lavoro , calcolato secondo siegrist come discrepanza tra impegno e ricompensa , ha mediamente valore inferiore a uno , il che rappresenta un bilancio favorevole nella maggior parte dei casi . 
workplace stress , calculated according to siegrists model as an imbalance between effort and rewards , yielded a value lower than one , which reflects a positive balance in the majority of cases . 
eri scores lower than one were , in fact , achieved by 72% of participants , whereas the remaining 28% ( 88 cases ) reported a negative balance between the effort put into their jobs and the rewards received in return ( eri greater then one )  . 
there was a greater effort - reward imbalproprio in questa ultima quota si colloca la maggior parte di coloro che cercano di compensare la mancanza di risultati con un impegno eccessivo nel lavoro ( overcommitment ) , come si osserva nella tabella 5 . 
settanta radiologi / radioterapisti , pari al 22 , 3% del totale , presentano una discrepanza tra impegno sul lavoro e risultati ottenuti , e sono al tempo stesso impegnati a fornire un ulteriore sforzo , che potrebbe risultare nocivo . 
risulta maggiore la discrepanza tra impegno e ricompense nei lavoratori del pubblico rispetto al privato ( p < 0 , 01 ) , nei dirigenti di i livello rispetto alle categorie gerarchicamente superiori ( p < 0 , 0001 ) , nei radiologi / radioterapisti pi giovani ( p < 0 , 004 ) e in quelli con meno anni di attivit ( p < 0 , 0001 ) rispetto agli altri . 
i radiologi tendono ad avere una discrepanza maggiore rispetto ai radioterapisti ( p = 0 , 0238 )  . soddisfazione dal lavoro la soddisfazione tratta dal lavoro , valutabile mediante il questionario di warr , mediamente elevata ( punteggio medio prossimo a 44 in una scala compresa tra 10 e 70 )  . 
la soddisfazione significativamente maggiore nei maschi ( p < 0 , 02 ) , nei direttori ( p < 0 , 0001 ) e negli specialisti con oltre 20 anni di attivit ( p < 0 , 003 ) , mentre non varia a secondo del tipo di struttura o dellet . 
i radioterapisti risultano significativamente pi soddisfatti dei radiologi ( p = 0 , 0018 )  . job satisfaction the satisfaction derived from work , assessed through warrs questionnaire , showed generally high levels ( mean score close to 44 on a scale from 10 to 70 )  . 
satisfaction was significantly higher among men ( p < 0.02 ) , among department heads ( p < 0.0001 ) and among specialists with more than 20 years of experience ( p < 0.003 ) , whereas it was not affected by productive sector or by age . 
the mean score of 23 in our series , with strong skewness to the left ( positive ) , stato di salute e stili di vita il questionario ghq fornisce un punteggio complessivo compreso tra 12 ( corrispondente al massimo benessere ) e 48 ( massimo malessere )  . 
nella nostra casistica il punteggio medio di 23 punti , con spiccata asimmetria a sinistra ( di segno positivo ) indicativo di un discreto livello di benessere psicofisico nellintera popolazione . 
il livello di benessere psicofisico significativamente peggiore nei soggetti di genere femminile ( p < 0 , 038 ) , nei pi giovani ( p < 0 , 002 ) ed in quelli con minore durata di attivit ( p < 0 , 008 )  . 
non si osservano differenze di punteggio tra radiologi e radioterapisti . conteggiando le risposte al ghq con metodo binario possibile individuare un certo numero di soggetti che presentano un punteggio indicativo di un possibile stato di malessere psicologico : i possibili casi sono 36 , pari all11 , 5% . le scale di ansia e depressione di goldberg presentano valori medi rispettivamente pari a 13 e 12 punti , di conseguenza non eccessivamente elevati . 
tuttavia il 30 , 7% degli 340 radiol med ( 2008 ) 113 : 329346 is indicative of a fair level of physical and mental well - being in the population studied . 
there were no differences in the distribution of anxiety and depression scores between the age and experience subgroups . questions relating to lifestyle showed a gaussian distribution , with values uniformly clustered around the mean . none of the respondents adopted the best lifestyle for any of the questions . 
table 6 summarises the samples conditions relative to the occupational risk factors investigated and the indicators of psychosocial distress . correlation among the variables investigated table 7 shows the correlation coefficients among the indicators used . 
all indicators of risk were found to correlate with one another ( satisfaction was inversely correlated to the others , being the only variable with positive significance ) and with the indicators of risk . 
only the correlation between occupational discomfort and lifestyles failed to reach statistical significance . we studied the relationship between the variables indicating workplace stress ( discomfort , job strain according to the jcq , effort - reward imbalance , job satisfaction ) and those indicating possible health effects ( anxiety , depression , psychological distress according to the ghq , lifestyles )  . 
in all models , effortreward imbalance was sigintervistati ( 96 soggetti ) presenta punteggi elevati di ansia ed da ritenersi a rischio per un disturbo psicologico di tale tipo , mentre il 16 , 9% dei radiologi ( 53 soggetti ) potrebbe essere a rischio di depressione . 
il punteggio di ansia significativamente pi alto nei radiologi di genere femminile ( p = 0 , 026 ) e nei radiologi rispetto ai radioterapisti ( p = 0 , 019 )  . 
non si osservano differenze nella distribuzione dei punteggi di ansia e depressione nelle diverse classi di et o di esperienza lavorativa . le domande relative allo stile di vita delineano una distribuzione di carattere gaussiano , con valori omogeneamente raccolti attorno alla media . 
non si osservano evidenti variazioni degli stili di vita in funzione del genere , del tipo di specializzazione , dellet o della durata di attivit . nella tabella 6 sono sintetizzate le condizioni del campione esaminato in relazione ai fattori di rischio professionale indagati e agli indicatori di danno psicosociale . correlazione tra le variabili indagate nella tabella 7 sono indicati i coefficienti di correlazione tra gli indicatori utilizzati . 
tutti gli indicatori di rischio risultano correlati tra loro ( la soddisfazione correlata inversamente con le altre , essendo lunica variabile di significato positivo ) e con gli indicatori di danno . 
solo la correlazione tra fattori di disagio lavorativo e stili di vita non raggiunge la significativit statistica . abbiamo studiato la relazione tra le variabili indicative di strain ( disagio , tensione da lavoro secondo jcq , discrepanza tra sforzi e risultati secondo eri , soddisfazione ) e quelle che indicano i possibili effetti ( ansia , depressione , malessere psicologico secondo ghq , stili di vita )  . 
sono stati cos costruiti quattro modelli di regressione lineare multipla con selezione stepwise tra le trasformate normali delle variabili indipendenti e ciascuna delle variabili dipendenti ( tabella 8 )  . 
le altre variabili sono entrate incostantemente nel modello di predizione , e precisamente : la soddisfazione dal lavoro risultata significativamente correlata in senso inverso con il malessere generale ( ghq ) e con la depressione , il disagio lavorativo con lansia e la depressione , mentre il punteggio del job strain ( jcq ) secondo kararasek non entrato in nessuno dei modelli . 
la percentuale di varianza stimata dai vari modelli radiol med ( 2008 ) 113 : 329346 table 6 prevalence of psychosocial risk factors and their effects in the observed sample tabella 6 prevalenza dei fattori di rischio professionale e dei danni psicosociali nel campione esaminato indicator no . 
the other variables entered the prediction model in an inconsistent manner , and in particular , job satisfaction showed a significant inverse correlation with psychological distress ( ghq ) and depression and occupational discomfort with anxiety and depression , whereas the score for job strain ( jcq ) did not enter any of the models . 
the variance rate estimated from the various models was generally moderate and almost significant for lifestyles . discussion and conclusions workplace stress is a complex issue and its study requires specific models to identify risk factors and effects on health . the complexity of the issue is ill - suited to the requirements of time , simplicity and economy that generally characterise epidemiological studies of working populations . 
there is a strong need to utilise instruments that are both reliable and quick to complete and score . an additional obstacle for italian - language studies is the limited number of original instruments and validated translations available . 
to overcome these problems , we used multiple instruments to measure the occupational risk factors and the effects of workplace stress , combining original italian instruments with the validated translations of the most commonly used tests at the international level . our work , which aimed to refine and test the psychodiagnostic instruments with a view to future broader studies , is to our knowledge the first to investigate occupational 38 , 5 indicatore di rischio disagio lavorativo alta tensione da lavoro ( job strain , jcq ) tensione e mancanza di sostegno ( isostrain , jcq ) discrepanza tra impegno e risultati ( imbalance , eri ) impegno eccessivo ( overcommitment , eri ) insoddisfazione indicatore di effetto ansia depressione malessere psicologico ( ghq ) 23 , 9 17 , 2 28 , 0 22 , 3 24 , 8 30 , 7 16 , 9 11 , 5 jcq , job content questionnaire ( karasek [ 5 ] ) ; ghq , general hospital questionnaire ( goldberg [ 32 ] ) ; eri , effort - reward imbalance ( siegrist [ 2 ] ) era generalmente modesta e ai limiti della significativit per gli stili di vita . discussione e conclusioni lo stress da lavoro un fenomeno complesso , il cui studio richiede specifici modelli per lidentificazione dei fattori di rischio e degli effetti dello stress sulla salute . 
 viva lesigenza di fruire di strumenti che siano al tempo stesso affidabili e rapidi da compilare ed elaborare . un ostacolo aggiuntivo per le ricerche in lingua italiana la scarsa disponibilit di strumenti originali o di traduzioni valide . 
per risolvere questi problemi nel nostro studio - pilota abbiamo impiegato strumenti molteplici per misurare i fattori di rischio professionale e le conseguenze dello stress da lavoro , affiancando strumenti originali in lingua italiana con le versioni validate dei test pi diffusi in campo internazionale . 
questa indagine , che ha avuto lo scopo di mettere a punto gli strumenti psicodiagnostici in vista di impegni di maggiori dimensioni , rappresenta , per quanto dato di sapere , la prima finalizzata allo studio dello stress nei radiologi e radioterapisti . 
radiology appears to be at the centre of a phenomenon of increased occupational stress that results on the one hand from increasing production demands , often with a shortage of resources , and on the other hand from the introduction of sophisticated imaging techniques and invasive modalities , which require a entrambe le discipline radiologia diagnostica e radioterapia sono soggette a simili esigenze di efficienza produttiva che penalizzano sempre di pi il tempo a disposizione del medico per valutare lesame o il piano terapeutico , e in definitiva per la cura del malato . 
ne consegue il deterioramento del quadro relativo al contenzioso medico - legale , con radiol med ( 2008 ) 113 : 329346 table 8 linear association between predictive variables and health effects . 
sono indicati i coefficienti di regressione standardizzati calcolati al termine dellanalisi di regressione lineare multipla con metodo stepwise effetto jcq ( karasek ) eri ( siegrist ) soddisf ( warr ) coeff . 
both diagnostic radiology and radiotherapy are subject to the same requirements of productive efficiency , which increasingly limit the time available for evaluating examinations or planning treatment and ultimately the time for patient care . 
as a consequence , the medical litigation situation is deteriorating , with the risk of claims for alleged malpractice reaching levels at which every italian radiologist and radiotherapist has the statistical certainty that they will be sued at least once in the course of their working lives [ 50 ]  . 
women show greater job strain as well as signs of major psychological distress compared with men . in clinical terms , the cross - sectional nature of the study did not allow us to establish a causal relationship between stress factors and poor health ; however , the existence of such a relationship is likely on the grounds of the literature and clinical experience . comparison of results obtained with the two models of workplace stress is particularly interesting . 
karaseks jcq yielded a mean level of job strain greater than one . this indicates that workload and responsibility at the group level exceeds the individuals capabilities and decisional power despite the control dimension being high among medical specialists . 
about one quarter of respondents could un crescente rischio di denunce per presunta malpractice che ormai ha raggiunto , per i radiologi e radioterapisti italiani , la certezza statistica di ricevere almeno una denuncia per responsabilit civile nel corso della vita lavorativa [ 50 ]  . 
le donne presentano maggiore tensione e alcuni segni di maggiore sofferenza psicologica rispetto agli uomini . sotto il profilo clinico , il carattere trasversale dello studio non consente di affermare il nesso di causalit tra fattori di stress e condizioni negative di salute ; tale nesso , tuttavia , appare verosimile sulla scorta della letteratura e dellesperienza clinica . di particolare interesse appare il confronto dei risultati ottenibili con i due modelli di stress professionale applicati . il questionario jcq di karasek fornisce un livello medio di tensione da lavoro superiore ad uno . 
circa un quarto degli intervistati classificabile come sotto tensione secondo il modello di karasek , e la maggior parte di questo gruppo versa in condizioni di contemporaneo isolamento sociale , che aggrava leffetto dello stress . viceversa , leri di siegrist fornisce un rapporto tra impegno e ricompensa inferiore allunit , dimostrando che in 344 radiol med ( 2008 ) 113 : 329346 be classified as stressed according to karaseks model , and the majority of these simultaneously experience a condition of social isolation , which magnifies the effects of stress . in contrast , siegrists eri yielded an effortreward imbalance ratio lower than one , which demonstrates that radiologists are generally satisfied with their professional achievements in relation to the efforts made . 
nonetheless , more than one quarter of radiologists suffers from a mismatch between effort and rewards and often reacts by excessive striving or overcommitment , which further reduces the chances of compensation and recovery . 
the high correlations among the variables are proof that the indicators used are similar , though not identical , and that there is a relationship between the factors of workplace stress and poor health . 
 linear regression analysis showed that stress measured as an effort - reward imbalance correlates with all the negative effects on health , whereas the other measures , and in particular the karasek measure of stress , had a weaker correlation . 
this effect was already observed by calnan [ 32 ] and might indicate that the factors investigated by the siegrist model are more relevant , at least to the specialist physicians interviewed . 
this result is even more disconcerting when considering that radiation risk makes radiologists and radiotherapists the most closely monitored professional group in the workplace , with compulsory medical checkups at least once a year . 
deteriorating health , which is even worse if the subject is unaware of it , also has a bearing on correct medical practice , as numerous conditions affecting the physician may impair his or her judgement skills and thus , through malpractice situations , harm patients [ 51 , 52 ]  . 
the attention devoted to treating patients health conditions should not lead one to neglect ones own health . in conclusion , the results of our pilot study indicate a need for effective measures to prevent workplace stress , a phenomenon that affects not only the health of physicians but also the health of patients entrusted to their care . media i radiologi sono soddisfatti dei risultati professionali raggiunti in relazione allimpegno profuso . 
ci nonostante , oltre un quarto dei radiologi soffre di una discrepanza tra limpegno profuso sul lavoro ed i risultati ottenuti , e reagisce spesso con un incremento dellattivit che riduce ulteriormente le possibilit di compenso e recupero . le elevate correlazioni tra le variabili testimoniano del fatto che gli indicatori usati sono simili , anche se non sovrapponibili , e che esiste una relazione tra fattori di stress da lavoro e danni per la salute . mediante analisi della regressione lineare abbiamo osservato che lo stress misurato secondo siegrist come discrepanza tra impegno e ricompense si correla con tutti gli effetti negativi per la salute , mentre le altre misure , ed in particolare lo stress misurato secondo karasek , hanno minore correlazione . 
tale effetto stato gi osservato da calnan [ 32 ] , e potrebbe indicare che gli aspetti indagati dal modello di siegrist siano pi rilevanti , almeno per quanto riguarda gli specialisti intervistati . 
una proporzione rilevante del campione in esame presenta elevati livelli di job strain , spesso associato ad isolamento sociale , e di discrepanza tra impegno e ricompense da lavoro , aggravato dalla tendenza alleccessivo coinvolgimento nellattivit lavorativa . 
tale risultato ancora pi sconcertante , se si pensa che i radiologi e i radioterapisti sono indubbiamente la categoria professionale medica maggiormente sorvegliata sui luoghi di lavoro per quanto attiene al rischio radiologico , per il quale sono obbligatori controlli medici almeno annuali . 
il deterioramento dello stato di salute , che ancora pi grave se il soggetto ne inconsapevole , non senza rilievo anche ai fini del corretto esercizio della professione medica , giacch innumerevoli malattie del medico potrebbero alterare la sua capacit di giudizio e quindi determinare , attraverso situazioni di malpractice , un danno per i pazienti [ 51 , 52 ]  . 
di rudin 8 , 20142 milan , italy 2department of radiology , umass memorial medical center , university of massachusetts , 55 lake avenue north , worcester , ma 01655 , usa 3is bioinformatics unit , university of massachusetts medical school , 55 lake avenue north , worcester , ma 01655 , usa correspondence to : s . 
 + 39 - 333 - 3111021 , fax : + 39 - 02 - 50323393 , e - mail : silvia.3soldi@tin.it received : 19 july 2007 / received : 24 august 2007 / published online : 25 april 2008 springer - verlag 2008 abstract purpose . 
we retrospectively reviewed 220 reports of 40 - row mdct exams in consecutive patients ( 101 men , 119 women ; mean age 55 years ( cid : 2 ) 18 ) suspected for acute pe . 
chest mdct , with an excellent overall image quality , provided an explanation for the clinical presentation in about 50% of emergency department patients studied and was useful in detecting pe and other thoracic diseases with symptoms mimicking pe . 
abbiamo analizzato retrospettivamente i referti tc 40 - strati di 220 pazienti consecutivi ( 101 maschi , 119 femmine ; et media 55 ( cid : 2 ) 18 anni ) con sospetto di ep acuta . 
all8 , 6% dei pazienti ( n = 19 ) stata fatta diagnosi di embolia polmonare , al 45 , 9% ( n = 101 ) sono stati identificati altri reperti toracici clinicamente rilevanti . 
la 40 - tcmd del torace , grazie anche ad uneccellente qualit dellimmagine , ha fornito una spiegazione alla presentazione clinica in circa met dei pazienti studiati , risultando utile nellidentificazione 374 radiol med ( 2008 ) 113 : 373384 keywords thoracic diseases pulmonary artery pulmonary embolism computed tomography dellembolia polmonare e di altre patologie toraciche con sintomi simili . 
tuttavia la met degli esami risultata negativa . parole chiave patologia toracica arteria polmonare embolia polmonare tomografia computerizzata introduction introduzione pulmonary embolism ( pe ) is a common , potentially fatal condition . 
mdct is a fast , accurate , noninvasive diagnostic tool capable of evaluating both pe and deep venous thrombosis ( dvt ) , with an excellent cost - benefit ratio . 
we evaluated the benefits of 40 - detector - row mdct on image quality and diagnostic value . the goal of this study was to evaluate the incidence of pulmonary embolism and of other clinically relevant thoracic findings discovered on thoracic contrast - enhanced 40detector - row mdct examination in patients with a clinical suspicion of acute pe presenting to the emergency department of a tertiary care centre . lembolia polmonare ( ep ) una patologia comune , potenzialmente fatale . 
la diagnosi di embolia polmonare spesso difficile a causa della presentazione clinica aspecifica [ 3 , 68 ] ed il dosaggio del d - dimero si dimostrato efficace solo nellescludere la presenza di embolia [ 3 , 6 ]  . attualmente la diagnosi di embolia polmonare spesso si basa sullimaging . 
la tcmd una metodica diagnostica veloce , accurata e non invasiva , capace di valutare nello stesso esame la presenza di embolia polmonare e di trombosi venosa profonda ( tvp ) con un eccellente rapporto costo - beneficio . 
all data were saved in both lung window ( window width 2 , 000 hu ; window level 700 hu ) and mediastinal window ( window width 700 hu , window level , 70 hu ) following reconstruction with edge enhancement and soft - tissue algorithms , respectively . 
coronal reformatted images of the thoracic images were obtained in all cases . ct venography was performed at a fixed 3 - min delay following contrast medium injection at 5 - mm collimation at 20 - mm intervals extending from the popliteal area to the level of l3 vertebral body . 
the remaining 32% were read by board - certified staff general radiologists . the radiology reports were reviewed retrospectively . ct chest image quality was assessed using a 4 - point scale to evaluate contrast enhancement ( 1 no enhancement ; 2 poor enhancement ; 3 satisfactory - adequate to evaluate the main lobar arteries ; 4 good enhancement ) and a 3 - point scale to evaluate motion artefacts ( 1 severe ; 2 moderate ; 3 no motion )  . 
if the description of motion and degree of contrast enhancement in the radiological report was unclear , the interpreting radiologist reviewed the case retrospectively . frequency of pe and other clinically relevant thoracic findings was evaluated on the basis of the radiological report as well as the frequency of dvt . 
thoracic findings not known before the mdct exam were classified as acute ( if they required prompt medical or surgical intervention ) or nonacute ( if they required medical or surgical intervention at a later time )  . 
acute findings included the following : moderate or severe consolidation / pneumonia ( if not specified by 119 femmine ; et compresa tra 18 e 98 anni ; et media 5518 anni ) con sospetta embolia polmonare acuta , sottoposti , tra gennaio e maggio 2006 , ad esame 40 - tcmd del torace e degli arti inferiori . acquisizione delle immagini gli esami sono stati acquisiti in senso cranio - caudale dalle clavicole al diaframma , durante ununica apnea , con unapparecchiatura tcmd ( philips brilliance 40 - canali , philips medical systems ) , con i seguenti parametri : configurazione dei detettori 400 , 625 mm , spessore di strato 1 mm , incremento di ricostruzione 0 , 5 mm , pitch 0 , 876 , tempo di rotazione 0 , 75 s , 210 mas , 120 kvp . 
il ritardo di scansione stato determinato automaticamente mediante software di bolus tracking con regione di interesse ( roi ) posizionata a livello dellarteria polmonare principale ed inizio della scansione al raggiungimento della soglia prestabilita ( + 100 hu )  . 
tutti i dati sono stati salvati con finestra per il parenchima polmonare ( ampiezza 2000 hu ; livello 700 hu ) e per il mediastino ( ampiezza 700 hu ; livello 70 hu ) con ricostruzioni con filtro dedicato e con algoritmo per i tessuti molli , rispettivamente . 
in tutti i casi sono state ottenute ricostruzioni sul piano coronale . lo studio degli arti inferiori stato condotto con un ritardo di 3 minuti dalliniezione del mezzo di contrasto con collimazione di 5 mm ad intervalli di 20 mm dal poplite ad un livello corrispondente al corpo vertebrale di l3 . 
in un caso , in cui la paziente era in presunto stato di gravidanza , le vene degli arti inferiori non sono state studiate . interpretazione delle immagini ed analisi dei dati le immagini sono state visualizzate su una workstation pacs ( idx imagecast )  . 
i referti sono stati interpretati retrospettivamente . abbiamo valutato la qualit delle immagini degli esami tc del torace con una scala di valori da 1 a 4 per valutare lenhancement ( 1 , nessun enhancement ; 2 , enhancement scarso ; 3 , soddisfacente , adatto alla valutazione delle arterie polmonari principali ; 4 , buon enhancement ) e una scala da 1 a 3 per valutare gli artefatti da movimento ( 1 , numerosi ; 2 , alcuni ; 3 , nessun artefatto )  . 
in caso nel referto la descrizione del grado di enhancement e di movimento non fosse chiara , sono state riguardate le immagini retrospettivamente dallesecutore dello studio . 376 radiol med ( 2008 ) 113 : 373384 lincidenza di embolia polmonare , di altri reperti toracici clinicamente rilevanti e di trombosi venosa profonda stata valutata sulla base del referto radiologico . 
i reperti toracici non noti prima dellesame tc sono stati classificati in acuti ( quando richiedevano un intervento medico o chirurgico immediato ) o non acuti ( quando richiedevano un intervento medico o chirurgico posticipabile in un secondo momento )  . 
sono stati considerati non acuti i seguenti reperti : linfonodi mediastinici od ilari > 1 cm , enfisema polmonare moderato , ipertensione polmonare ( diametro arteria polmonare principale > 3 cm ) , masse mediastiniche > 1 cm , alveolite , atelettasia polmonare di grado moderato o severo , noduli polmonari > 3 mm , lesioni vertebrali sospette per lesioni neoplastiche , ectasia dellaorta toracica ( diametro > 3 cm ) , ectasia delle arterie bronchiali e linfangite carcinomatosa . 
di ciascun paziente sono stati classificati i sintomi di presentazione ed i fattori di rischio . analisi statistica abbiamo calcolato lincidenza di embolia polmonare , di trombosi venosa profonda e degli altri reperti toracici . 
tutte le analisi sono state fatte con lutilizzo di spss statistical software package , versione 14.0 ( spss , chicago , ill )  . risultati in tabella 1 riassunta la valutazione della qualit delle immagini . 
sulla base dei referti radiologici il 96 , 8% ( n = 213 ) degli esami tc del torace sono stati considerati diagnostici ; il 3 , 2% ( n = 7 ) non diagnostici . 
dei 16 pazienti con diagnosi di embolia polmonare allesame tc ed esame tc degli arti inferiori considerato diagnostico 9 ( 56 , 2% ) sono risultati affetti da tvp mentre dei 148 pazienti senza embolia fig . 
1 acute thoracic finding in a pulmonary embolism ( pe ) - negative patient : contrast - enhanced multidetector computed tomography ( mdct ) axial image showing a severe pericardial effusion ( asterisks ) that can surely justify the patients shortness of breath and dyspnoea . 
1 esempio di reperto toracico acuto in un paziente in cui la tc ha escluso la presenza di embolia polmonare : immagine assiale tcmd con mezzo di contrasto che documenta un importante versamento pericardico ( asterischi ) , probabile causa della dispnea e tachipnea lamentate dal paziente . 
nonacute findings included enlarged ( > 1 cm ) mediastinal or hilar lymph nodes , moderate pulmonary emphysema , pulmonary hypertension ( main pulmonary artery diameter > 3 cm ) , mediastinal masses ( > 1 cm ) , alveolitis , severe or moderate lung atelectasis , pulmonary nodules ( > 3 mm ) , vertebral lesions suspicious for malignancy , ectatic thoracic aorta ( diameter > 3 cm ) , bronchial artery dilatation and lymphangitic spread of malignancy . 
all analyses were performed using the spss statistical software package , version 14.0 ( spss , chicago , il , usa )  . polmonare 7 ( 4 , 7% ) sono risultati affetti da tvp , con una differenza statisticamente significativa ( p < 0 , 001 , 2 )  . il 38 , 2% ( n = 84 ) della popolazione aveva fattori di rischio maggiori o minori per embolia polmonare ( tabella 3 )  . 
il 14 , 5% ( n = 32 ) dei pazienti aveva pi di un fattore di rischio e 136 ( 61 , 8% ) pazienti non avevano fattori di rischio . l82 , 7% ( n = 182 ) dei pazienti presentava sintomi suggestivi per embolia polmonare ( tabella 4 ) ; il 10 , 9% ( n = 24 ) dei pazienti aveva due sintomi ed il 17 , 3% ( n = 38 ) non aveva nessuno dei sintomi considerati . 
tra i 19 pazienti con embolia polmonare , 6 ( 31 , 6% ) avevano sia sintomi sia fattori di rischio , 9 ( 47 , 4 % ) sintomi ma non fattori di rischio e 4 ( 21% ) fattori di rischio ma non sintomi . 
le ragioni per cui sono stati sottoposti a tcmd erano : d - dimero positivo ( n = 3 ) , dolore addominale ( n = 3 ) , storia di patologia polmoresults image quality evaluation is shown in table 1 . 
based on the radiological reports , 96.8% ( 213 ) of the thoracic ct examinations were considered diagnostic for the evaluation of pe ; 3.2% ( 7 ) were regarded as nondiagnostic . 
symptoms suggesting the clinical diagnosis of pe were found in 82.7% ( 182 ) of patients and are listed in table 4 ; 10.9% ( 24 ) of patients presented with two symptoms and 17.3% ( 38 ) had no symptoms . 
among the 19 patients with pe , six ( 31.6% ) presented with symptoms and risk factors , nine ( 47.4 % ) with symptoms but lack of risk factors and four ( 21% ) had risk factors but no symptoms . 
2a , b segmental pulmonary embolism ( pe ) in the artery for the medial segment of the middle lobe ( white arrow in a ) associated with type b chronic aortic dissection ( black arrows )  . 
2a , b esempio di embolia polmonare segmentaria nellarteria per il segmento mediale del lobo medio ( freccia bianca in a ) associata a dissezione cronica di tipo b dellaorta toracica ( frecce nere ) ; la dissezione non stata considerata un reperto rilevante in quanto gi nota al momento dellesame . 
a nessuno di questi pazienti stata fatta diagnosi di embolia polmonare alla tcmd . sono stati identificati 154 reperti toracici clinicamente significativi nel 45 , 9% ( n = 101 ) dei pazienti . 
patients percent patients pe positive pe negative nondiagnostic total pe , pulmonary embolism positivo per ep negativo per ep non diagnostico totale ep , embolia polmonare 88.2 88 , 2 tabella 2 risultati degli esami angio - tcmd delle arterie polmonari risultati n pazienti % pazienti sons these patients underwent mdct were positive ddimer test ( 3 ) , abdominal pain ( 3 ) , history of chronic obstructive pulmonary disease ( 3 ) , hypoxaemia ( 2 ) , weakness ( 1 ) , pneumonia ( 1 ) , haemoptysis ( 1 ) , pain in the back ( 1 ) , table 3 incidence of risk factors in the patient population major risk factor minor risk factor recent major surgery malignancy orthopaedic surgery prior pe / dvt leg / pelvic fracture obstetrics obesity cerebrovascular accident history of heart failure trauma overdose pe , pulmonary embolism ; dvt , deep venous thrombosis tabella 3 incidenza di fattori di rischio nella popolazione in esame fattori di rischio maggiori fattori di rischio minori recente intervento di chirurgia maggiore neoplasia maligna intervento di chirurgia ortopedica storia di ep / tvp frattura arti inferiori / bacino cause ostetrico / ginecologiche obesit accidenti cerebrovascolari storia di scompenso cardiaco trauma overdose ep , embolia polmonare ; tvp , trombosi venosa profonda 11.8 11 , 8 caratteristiche n pazienti % pazienti radiol med ( 2008 ) 113 : 373384 table 4 patient symptoms suggesting pulmonary embolism tabella 4 sintomi di presentazione suggestivi per embolia polmonare symptom no . 
patients with dvt were 7.3% ( 16 ) of the population . half of the patients ( 110 ) had neither pe nor other clinically relevant thoracic findings . discussion the incidence of pe in the united states is estimated at 650 , 000 new cases per year [ 5 ]  . 
 [ 9 ] , the number of patients referred for pe testing increased markedly and the use of ventilation perfusion scanning and pulmonary angiography fell after the helical ct scan became available . in our study , the incidence of nondiagnostic ct pulmonary angiograms was 3.2% , comparable with the 4% reported by brunot et al . 
 [ 10 ] and somewhat better than the rates ( 6.1%10.4% ) reported previously in other studies ; none of those studies was performed with mdct with more than 16 - slice equipment [ 1114 ]  . 
furthermore , the double injection is likely to have decreased contrast - induced artefacts from the superior vena cava . the availability of mdct in the emergency department discussione lincidenza di embolia polmonare negli usa stimata attorno a 650000 nuovi casi allanno [ 5 ]  . 
 [ 9 ] , il numero di pazienti sottoposti a test diagnostici per escludere lembolia polmonare in aumento e luso della scintigrafia e dellangiografia polmonare drasticamente diminuito da quando stato introdotto lutilizzo della tc . nel nostro studio lincidenza di esami tc , mirati allo studio delle arterie polmonari , considerati non diagnostici del 3 , 2% , paragonabile con il 4% di brunot et al . 
 [ 10 ] ed un po meglio dei dati ( 6 , 1%10.4% ) riportati in studi precedenti ; nessuno di questi studi stato condotto su tc a pi di 16 file di detettori [ 1114 ]  . 
laumento del livello di confidenza nella diagnosi di embolia polmonare con la tc a 40 file di detettori dovuto alla minore incidenza di artefatti da movimento ( 90 , 9% degli esami non avevano artefatti da movimento )  . 
inoltre , grazie al doppio iniettore , vi una diminuzione degli artefatti dovuti alla presenza di mdc in vena cava superiore . la disponibilit di unapparecchiatura tcmd in pronto soccorso la rende la modalit diagnostica di scelta nella valutazione dellembolia polmonare [ 2 , 7 ]  . 
questo stato confermato da un recente studio sulla pratica clinica che riporta un trend crescente di valutazione dellembolia polmonare tramite tc senza che ci sia alcuna variazione nel numero di pazienti sottoposti a test diagnostico per escludere la presenza di embolia polmonare [ 9 ]  . 
 [ 11 ] hanno descritto una prevalenza di tromboembolia del 9 , 6% che raggiunge il 16 , 8% dopo lesclusione di pazienti con una bassa probabilit pre - test e valori di d - dimero nella norma . 
 [ 15 ] , che riporta il 26% di esami positivi per embolia polmonare , sono stati esclusi i pazienti con valori normali di d - dimero e bassa probabilit clinica di tromboembolia . 380 radiol med ( 2008 ) 113 : 373384 table 5 classes of thoracic findings ( acute and non - acute ) ; number of cases and correlation with pulmonary embolism pe positive pe negative acute thoracic findings severe consolidation / pneumonia severe pleural effusion moderate consolidation / pneumonia moderate pleural effusion patchy pneumonia severe pulmonary emphysema pulmonary oedema heart failure pneumomediastinum pneumothorax severe pericardial effusion wrong position endotracheal tube total nonacute thoracic finding lymph nodes ( > 1 cm ) moderate pulmonary emphysema pulmonary hypertension mass ( > 1 cm ) alveolitis moderate atelectasis nodule ( > 5 mm ) nodule ( 35 mm ) vertebral lesion ( suspicious for metastasis ) severe atelectasis ectatic thoracic aorta bronchial artery dilatation lymphangitic spread total total acute and nonacute pe , pulmonary embolism makes it the diagnostic imaging modality of choice to evaluate for pe [ 2 , 7 ]  . 
this is confirmed by a recent study on clinical practice that reports a trend towards increased evaluation for pe via ct pulmonary angiography without any change in the likelihood of pe among patients referred for testing [ 9 ]  . prior research reports a range of prevalence of pe that correlates with patient demographics . 
 [ 15 ] , who reported 26% of pe - positive exams , patients with normal d - dimer test and low clinical probability of thromboembolism were excluded from the study . 
due studi retrospettivi [ 2 , 7 ] che analizzano reperti accessori in pazienti con sospetta embolia polmonare riportano una prevalenza di embolia polmonare dell8 , 5% e del 10% . 
la prevalenza di embolia polmonare nel nostro studio dell8 , 6% . il rischio di embolia polmonare aumenta da 5 a 20 volte in seguito a chirurgia maggiore e chirurgia addominale , chirurgia ortopedica degli arti inferiori , fratture degli arti inferiori , neoplasie maligne e varie condizioni ostetrico - giradiol med ( 2008 ) 113 : 373384 tabella 5 classificazione reperti toracici : acuti o non acuti ; numero di casi e correlazione con la presenza di embolia polmonare no ep reperti toracici acuti polmonite di grado severo versamento pleurico massivo polmonite di grado moderato versamento pleurico di grado moderato polmonite a mosaico enfisema polmonare grave edema polmonare scompenso cardiaco pneumomediastino pneumotorace versamento pericardico massivo errato posizionamento cannula endotracheale totale reperti toracici non acuti linfonodi > 1 cm enfisema polmonare di grado moderato ipertensione polmonare masse mediastiniche > 1 cm alveolite atelettasia polmonare di grado moderato noduli polmonari ( > 5 mm ) noduli polmonari ( 35 mm ) lesioni vertebrali ( sospette per metastasi ) atelettasia polmonare di grado severo ectasia dellaorta toracica ectasia delle arterie bronchiali linfangite carcinomatosa totale acuti e non acuti ep , embolia polmonare 23% in inpatients . 
the prevalence of pe in patients with risk factors was 11.9% ( 10 of 84 ) , and 30% ( 3 of 10 ) of them presented with no symptoms . 
in our study , chest pain was the most common symptom ( 41.4% ) , but it was present only in four ( 21% ) patients with pe , whereas shortness of breath was present in 47.4% necologiche ( per esempio gravidanza a termine , parto cesareo ) , precedenti episodi tromboembolici e in caso di prolungata immobilizzazione [ 3 , 6 , 16 ]  . 
la prevalenza di embolia polmonare nei pazienti con fattori di rischio era dell11 , 9% ( 10 su 84 ) il 30% dei quali ( 3 su 10 ) asintomatico . 
nel nostro studio il sintomo pi comune il dolore toracico ( 41 , 4% ) , presente per solo in 4 ( 21% ) pazienti con embolia polmonare mentre la tachipnea era presente nel 47 , 4% dei pazienti con embolia polmonare ( n = 9 )  . 
sicuramente la valutazione clinica e la gestione dei pazienti di pronto soccorso con dolore toracico o dispnea pi facile con la tc che con la scintigrafia ventilatoria / perfusionale per il risultato univoco della tc e la sua abilit nellidentificare patologie alternative . 
in futuro si dovr sviluppare un algoritmo per la valutazione del dolore toracico ; dovr valutare lembolia polmonare , linfarto miocardico e la disse382 radiol med ( 2008 ) 113 : 373384 of the patients with pe ( 9 )  . 
surely , the clinical evaluation and management of emergency department patients with chest pain or dyspnoea is easier with ct than with ventilation perfusion scan because of its binary result and its ability to identify alternative disease processes . 
systematic d - dimer assays and clinical assessment along with new electrocardiogram - gated 40and 64 - mdct will help achieve this goal [ 16 , 17 ]  . concurrent evaluation of thoracic structures in addition to the pulmonary vessels represents a diagnostic advantage for mdct over ventilation perfusion scintigraphy [ 14 , 18 ]  . ninety - one ( 45.3% ) of the 201 patients without pe had an alternative diagnosis on mdct consistent with the prevalence in prior studies [ 1 , 7 , 14 , 18 , 19 ]  . 
an explanation for the clinical presentation could be offered to 51.8% ( 114 ) of our population undergoing mdct evaluation for suspected pe [ 2 , 6 , 7 , 14 , 18 ]  . 
 [ 18 ] , was seen in a similar percentage of patients with pe ( 2 ; 7.7% of pe patients ) and without pe ( 21 ; 10.8% of non pe patients )  . 
while the combination of ct angiography and ct venography increases the average effective dose , the risk - to - benefit ratio remains low considering the potential morbidity and mortality related to thromboembolism , especially in elderly patients . 
we found that approximately half of the patients with dvt did not have concurrent pe , confirming the value of the combined ct pulmonary angiography and ct venography to rule out thromboembolic disease [ 11 , 13 ]  . 
in our study , two patients had dvt in the inferior vena cava and two in the iliac veins . this region is not evaluated well by lower - extremity ultrasonography [ 1 , 20 ]  . 
 [ 12 ] cite seven clinical outcome studies of patients with negative findings at ct who were untreated . even though with 40 - detector - row ct in the emergency department , we found a prevalence of pe that lies within the range of previous reports [ 2 , 7 , 8 , 10 , 11 , 15 ]  . 
risulteranno utili , a tale scopo , oltre al dosaggio del d - dimero e alla valutazione clinica , le nuove apparecchiature tcmd a 40 e 64 strati [ 16 , 17 ]  . la possibilit di valutare non solo i vasi polmonari ma tutte le strutture toraciche rappresenta un vantaggio della tcmd rispetto alla scintigrafia [ 14 , 18 ]  . 
novantuno ( 45 , 3% ) dei 201 pazienti senza embolia polmonare hanno ricevuto una diagnosi alternativa alla tcmd , dato concorde con la prevalenza riportata in studi precedenti [ 1 , 7 , 14 , 18 , 19 ]  . 
una spiegazione alla presentazione clinica stata trovata nel 51 , 8% ( n = 114 ) della nostra popolazione sottoposta a tcmd nel sospetto clinico di embolia polmonare [ 2 , 6 , 7 , 14 , 18 ]  . 
un altro reperto acuto frequente stato il versamento pleurico massivo ( n = 11 ) o moderato ( n = 10 ) che , in accordo con shah et al . 
se da un lato lo studio , nella stessa seduta tc , del torace e degli arti inferiori aumenta la dose media , il rapporto rischio - beneficio rimane basso in considerazione della potenziale morbilit e mortalit associate alla tromboembolia , soprattutto nei pazienti pi anziani . 
abbiamo scoperto che circa la met dei pazienti con tvp non aveva unembolia polmonare , dato che conferma il valore aggiunto dellesame tc combinato del torace e degli arti inferiori nellescludere una patologia tromboembolica [ 11 , 13 ]  . 
 [ 12 ] citano sette studi di follow - up in cui pazienti con tc negative per embolia polmonare non sono stati trattati . anche se con la 40 - tcmd in pronto soccorso abbiamo trovato una prevalenza di embolia polmonare nel range di studi precedenti [ 2 , 7 , 8 , 10 , 11 , 15 ] , la possibilit di ottenere facilmente un esame tc , utile nello studio di ogni tipo di patologia toracica , pu influenzare il comportamento dei clinici che possono ordinare tc per escludere embolia polmonare anche se la loro reale motivazione escludere altre patologie [ 7 ]  . 
nel nostro studio all8 , 6% ( n = 19 ) dei pazienti stata fatta diagnosi di embolia polmonare ma i paradiol med ( 2008 ) 113 : 373384 who can order ct scans to rule out pe even if their real motivation is to rule out other , more common , problems [ 7 ]  . 
in our study , 8.6% ( 19 ) of patients were found to have pe , but patients with no pe and with other thoracic findings were about five times ( 91 ) more frequent . 
moreover , we found that half of the patients who underwent chest mdct examination had neither pe nor clinically relevant thoracic findings ; all these patients had neither risk factors nor symptoms suggesting a diagnosis of pe . 
first , the protocol used in our hospital does not include a noncontrast ct scan of the entire thorax that could be useful in identifying calcified thrombi [ 10 ]  . 
the incidence of such findings can also be affected by study population demographics . conclusions we found that , accompanied by an excellent overall image quality , thoracic contrast - enhanced 40 - detector - row mdct examination provided an explanation for the clinical presentation in about 50% of emergency department patients with suspected pe . 
this diagnostic technique can detect both pe and other significant thoracic or mediastinal diseases with symptoms mimicking pe , with a gain in terms of justifying patients symptoms and starting adequate therapy . 
however , clinicians should be careful not to order ct if there is no specific indication : in our experience , half of the exams turned out to be negative . zienti senza embolia e con diagnosi alternative erano circa cinque volte pi numerosi ( n = 91 )  . 
in pi , met dei pazienti sottoposti a tcmd del torace non aveva n embolia polmonare n reperti toracici clinicamente rilevanti ; tutti questi pazienti non avevano n fattori di rischio n sintomi sospetti per embolia polmonare . 
questo deve essere valutato attentamente in quanto se , da un lato , si pu affermare che lesame tc stato utile per escludere varie patologie , dallaltro non vanno sottovalutati i costi , anche in termini di tempo . il nostro studio ha dei limiti . 
quarto : il nostro elenco di reperti toracici era strettamente dipendente dai reperti descritti nei referti radiologici . conclusioni il nostro studio dimostra che , grazie anche ad unelevata qualit dellimmagine , lesame 40 - tcmd del torace pu fornire una spiegazione alla presentazione clinica del paziente in circa il 50% dei pazienti giunti in pronto soccorso per sospetta embolia polmonare acuta . 
questa metodica pu rilevare la presenza sia di embolia polmonare sia di altre patologie toraciche o mediastiniche con sintomi di presentazione simili a quelli dellembolia polmonare , con un guadagno in termini di tempestivit diagnostica e terapeutica . 
tuttavia i clinici devono essere attenti a non richiedere esami tc se non ci sono indicazioni specifiche : nella nostra esperienza met degli esami sono risultati negativi . acknowledgements the authors thank f . 
mollet1 1dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 2dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria di parma , viale rustici , 23100 parma , italy 3dipartimento di radiologia , universit degli studi di napoli , napoli , italy 4dipartimento di radiologia , universit degli studi di milano , milano , italy 5dipartimento di radiologia , universit degli studi di verona , verona , italy 6dibimel , sezione di scienze radiologiche , universit di palermo , palermo , italy 7unit di riabilitazione cardiovascolare , fondazione don gnocchi onlus , parma , italy 8dipartimento di cardiologia , ospedale san gennaro , napoli , italy 9dipartimento di cardiologia , ospedale versilia , lido di camaiore , viareggio , italy correspondence to : f . 
we studied 163 patients ( mean age 65.5 years ; 101 men and 62 women ) referred for multidetector computed tomography coronary angiography ( mdct - ca ) to rule out cad . 
the percentage of coronary arteries with no plaque , nonsignificant disease and significant disease was 55% , 41% and 4% , respectively , in patients with zero or one rf ; riassunto obiettivo . 
abbiamo studiato 163 pazienti ( et media 65 , 510 , 6 anni ; 101 maschi e 62 femmine ) che hanno eseguito una angiografia coronarica mediante tomografia computerizzata multistrato ( tcms ) con lo scopo di escludere la presenza di patologia coronarica ; tutti i pazienti erano sintomatici e nessuno aveva storia di rivascolarizzazione o infarto miocardio . 
sono stati suddivisi i pazienti in tre gruppi in base al numero dei fdr : con 0 o 1 , con 2 o 3 e con 4 o pi 364 radiol med ( 2008 ) 113 : 363372 27% , 51% and 22% , respectively , in patients with two or three rf ; and 19% , 38% and 44% , respectively , in patients with four or more rf . 
severity and type of disease is highly correlated with rf number and assumes different characteristics according to clinical presentation . keywords ct coronary angiography risk factors epidemiology suspected coronary artery disease fdr . 
la percentuale di coronarie indenni , malattia non significativa e malattia significativa era , rispettivamente , del 55% , 41% , 4% nei pazienti con 0 o 1 fdr , del 27% , 51% , 22% nei pazienti con 2 o 3 fdr e del 19% , 38% , 44% nei pazienti con 4 o pi fdr . 
la severit e il tipo di malattia fortemente correlato al numero dei fdr e assume caratteristiche differenti in base alla presentazione clinica . parole chiave coronarografia tc fattori di rischio epidemiologia sospetta malattia coronaria introduction introduzione multidetector computed tomography coronary angiography ( mdct - ca ) is an emerging technique capable of providing accurate and noninvasive assessment of the coronary tree . the techniques diagnostic accuracy in comparison with angiography in visualising the presence and severity of coronary atherosclerosis has already been demonstrated [ 18 ]  . mdct - ca has also been reported to provide additional information on the coronary artery walls compared with conventional angiography , as it can identify the presence of plaque with prevalent outward expansion as well as define its morphological characteristics [ 9 , 10 ]  . 
studies have been performed that describe the probability of coronary artery disease ( cad ) in relation to risk factors ( rf ) [ 11 ] and the degree of coronary calcification [ 12 ]  . 
no similar studies , however , have been published that take into consideration parameters in the assessment of the coronary arteries with mdct - ca . the aim of this study was to describe the relationship between the numerous coronary rf and the presence , severity and characteristics of coronary atherosclerosis in a population of patients with symptoms of ischaemic heart disease with different risk profiles and to assess how the disease characteristics vary in relation to the different types of clinical presentation . la tomografia computerizzata multistrato ( tcms ) una tecnica emergente che permette di ottenere una accurata valutazione dellalbero coronarico in modo non invasivo . laccuratezza diagnostica nel rilevare la presenza e la severit della aterosclerosi coronarica rispetto alla angiografia gi stata dimostrata [ 18 ]  . 
stato descritto , inoltre , come questa tecnica permette di ottenere informazioni aggiuntive rispetto allesame angiografico tradizionale per quanto riguarda lo studio della parete delle coronarie , potendo individuare la presenza di placche che si estendono prevalentemente allesterno del lume e definendone le loro caratteristiche morfologiche [ 9 , 10 ]  . 
esistono studi che hanno descritto la probabilit di malattia coronarica correlata ai fattori di rischio ( fdr ) [ 11 ] e al grado di calcificazione coronarica [ 12 ]  . 
non esistono tuttavia analoghi lavori che prendono in considerazioni tali parametri nella valutazione delle coronarie con tcms . lo scopo di questo studio quello di descrivere la relazione esistente tra i numerosi fdr coronarici , la presenza , la severit e le caratteristiche della aterosclerosi coronarica in una popolazione sintomatica per cardiopatia ischemica con diversi profili di rischio e valutare come variano le caratteristiche della malattia in base alle differenti modalit di presentazione clinica . radiol med ( 2008 ) 113 : 363372 materials and methods patients materiali e metodi pazienti we used mdct - ca to study 163 patients ( mean age 66.510.6 years , 101 men and 62 women )  . 
likewise , patients with a known allergy to contrast material , with kidney failure ( serum creatinine > 120 mmol / l ) or with impaired respiratory function were also excluded . the study was approved by the local ethics committee , and all patients provided written informed consent . 
the following rf were evaluated : ( 1 ) arterial hypertension ( defined as arterial ( cid : 2 ) 140 / 90 mmhg or the need for antihypertensive therapy ) ; ( 2 ) hypercholesterolaemia ( defined as cholesterol levels ( cid : 2 ) 5 mmol / l or the need for statin therapy ) ; ( 3 ) diabetes mellitus ( defined as resting glycaemia ( cid : 2 ) 7 mmol / l or the need for insulin or oral hypoglycaemic agents ) ; ( 4 ) smoking habits ( current or ex - smoker ) ; ( 5 ) obesity ( body mass index > 30 ) ; ( 6 ) family history of heart disease . 
symptoms were classified as typical pain , atypical pain or other symptoms . scan protocol all examinations were performed with a 64 - slice spiral ct scanner ( sensation 64 , siemens , forchheim , germany )  . 
la popolazione dello studio ha compreso pazienti che sono stati inviati alla angiografia coronarica mediante tcms per sospetta cardiopatia ischemica in base ai sintomi , il profilo ad alto rischio o test diagnostici anormali ; tutti i pazienti erano sintomatici ( tabella 1 )  . 
anche pazienti con nota allergia ai mezzi di contrasto , con insufficienza renale ( creatinina sierica > 120 mmol / l ) o con compromissione della funzionalit respiratoria sono stati esclusi . lo studio stato approvato dal comitato etico locale e tutti i pazienti hanno fornito per iscritto il loro consenso informato . 
i sintomi sono stati classificati come dolore tipico , dolore atipico o altri sintomi . table 1 patient population characteristics tabella 1 caratteristiche della popolazione value ( n ; % ) parametro valore ( n ; % ) parameter total patients women age ( meansd ) diabetes smokers cholestero hypertension family history obesity typical pain atypical pain other symptoms 101 ( 62% ) 62 ( 38% ) 65.510.6 21 ( 13% ) 66 ( 40% ) l88 ( 54% ) 99 ( 61% ) 77 ( 47% ) 35 ( 21% ) 24 ( 15% ) 86 ( 53% ) 53 ( 32% ) totale pazienti maschi femmine et ( mediads ) diabete fumo colesterolo ipertensione familiarit obesit dolore tipico dolore atipico altri sintomi 101 ( 62% ) 62 ( 38% ) 65 , 510 , 6 21 ( 13% ) 66 ( 40% ) 88 ( 54% ) 99 ( 61% ) 77 ( 47% ) 35 ( 21% ) 24 ( 15% ) 86 ( 53% ) 53 ( 32% ) 366 radiol med ( 2008 ) 113 : 363372 the heart rate was > 65 bpm , patients received i.v. 
they received 100 ml of iodinated contrast material at an injection speed of 45 ml / s ( iomeron , bracco , milan , italy ) followed by a 40 - ml bolus of saline solution at the same injection rate through an antecubital vescan synchronisation with the passage of the bolus of contrast material was achieved with the bolus - tracking technique [ 13 ]  . the scan was performed with the following parameters : number of detectors 64 , detector width 0.6 mm , gantry rotation speed 330 ms , effective temporal resolution 165 ms , table feed 3.8 mm / rotation , tube voltage 120 kvp , tube current 900 mas , craniocaudal scanning direction . 
to obtain optimal - quality images , the data sets were reconstructed in the mid - to - end diastolic phase using retrospective electrocardiograph ( ecg ) gating ( 350 ms and + 275 ms )  . 
the axial data were then transferred to a dedicated workstation ( leonardo , siemens , forchheim , germany ) for postprocessing and subsequent assessment . data analysis all examinations were assessed by two expert observers who were unaware of patients clinical history using a standard analysis . 
coronary plaque were defined as structures > 1 mm within or adjacent to the coronary artery lumen , which could be clearly distinguished from the vessel lumen and the surrounding pericardial tissue , as previously described [ 9 ]  . 
analysis of the abnormal coronary arteries with one or more plaque also identified those with obstructive plaque ( ( cid : 2 ) 50% lumen narrowing ) in one or more segments . protocollo di scansione tutti gli esami sono stati eseguiti con una tomografia computerizzata spirale a 64 strati ( sensation 64 , siemens , forchheim , germania )  . 
sono stati somministrati 100 ml di mezzo di contrasto iodato alla velocit di 45 ml / s ( iomeron 400 , bracco , milano , italia ) seguiti da un bolo di soluzione fisiologica di 40 ml alla stessa velocit di iniezione attraverso una vena antecubitale del braccio . 
la sincronizzazione della scansione con il passaggio del bolo di mezzo di contrasto stata eseguita mediante tecnica del bolus tracking [ 13 ]  . i parametri di scansione sono stati : numero di rilevatori 64 , larghezza del rilevatore 0 , 6 mm , periodo di rotazione del tubo 330 ms , risoluzione temporale effettiva 165 ms , avanzamento 3 , 8 mm / rotazione , tensione del tubo kvp 120 , corrente 900 mas , direzione della scansione cranio - caudale . 
per ottenere una qualit delle immagini ottimale , i set di dati sono stati ricostruiti nella fase medio - tele diastolica e tele - sistolica utilizzando lecg - gating retrospettico ( 350 ms e + 275 ms )  . 
se erano presenti artefatti , venivano effettuate ulteriori ricostruzioni in differenti punti dellintervallo r - r . i dati assiali venivano poi trasferiti a una stazione di lavoro dedicata ( leonardo , siemens , forchheim , germania ) per il post - processing e per la conseguente valutazione . analisi dei dati tutti gli esami sono stati valutati da due osservatori esperti che non conoscevano la storia clinica dei pazienti , usando unanalisi standard . 
per prima cosa ogni segmento stato classificato come interpretabile o meno . successivamente i segmenti interpretabili sono stati valutati per la presenza di qualsiasi placca aterosclerotica usando immagini assiali e ricostruzioni curve multiplanari . 
le placche coronariche sono state definite come strutture > 1 mm dentro o adiacenti al lume coronarico , che possono essere chiaramente distinte dal lume del vaso e dal tessuto pericardio circostante , come precedentemente descritto [ 9 ]  . ogni placca stata assegnata in un segmento . 
a - c a patient with normal coronary arteries : a volume rendering ( vr ) of the left coronary artery ; b , c curved multiplanar reconstructions ( mpr ) of the circumflex and left anterior descending arteries , respectively . 
d - f a patient with prevalently calcified nonobstructive atheromatous coronary arteries ( d vr of the left coronary artery ; e , f curved mpr of the left anterior descending and circumflex arteries , respectively )  . 
g , h a patient with prevalently noncalcified and nonsignificant atheromatous coronary arteries : g vr of the right coronary artery ; h curved mpr of the right coronary artery showing a long and eccentric lesion ; 1 , transverse section of the lesion showing the noncalcified eccentric plaque . 
a - c paziente con coronarie indenni ( a volume rendering della coronaria sinistra ; b , c ricostruzioni multiplanari curvate della coronaria circonflessa e della coronaria discendente anteriore , rispettivamente )  . 
d - f paziente con coronarie caratterizzate da ateromasia prevalentemente calcifica non ostruttiva ( d volume rendering della coronaria sinistra ; e , f ricostruzioni multiplanari curvate della coronaria discendente anteriore e della coronaria circonflessa , rispettivamente )  . 
g , h paziente con coronarie caratterizzate da ateromasia prevalentemente non calcifica e non significativa ( g volume rendering della coronaria destra ; h ricostruzione multiplanare curvata della coronaria destra che mostra una lesione lunga ed eccentrica ; 1 , sezione trasversa della lesione che mostra la placca non calcifica eccentrica )  . 
i , j paziente con coronarie caratterizzate da ateromasia prevalentemente non calcifica significativa ( i volume rendering della coronaria destra ; j ricostruzione multiplanare curvata della coronaria destra che mostra una lesione lunga e concentrica del tratto medio ; j 13 , sezioni trasversali della lesione che mostrano la placca non calcifica concentrica )  . 
the group with zero or one rf was composed of 49 patients , of whom 27 ( 55% ) had normal coronary arteries , 20 ( 41% ) had nonsignificant cad and two ( 4% ) had significant cad . 
the group with two or three rf was composed of 82 patients , of whom 22 ( 27% ) had normal coronary arteries , 42 ( 51% ) had nonsignificant cad and 18 ( 22% ) had significant cad . 
la malattia viene stratificata come coronarie indenni ( coro indenni , ossia assenza di alterazioni della parete coronarica riferibili ad aterosclerosi ) , malattia non significativa ( mal non significativa , ossia malattia della parete coronarica che determina stenosi del lume < 50% ) , malattia significativa ( mal significativa , ossia malattia della parete coronarica che determina stenosi del lume ( cid : 2 ) 50% )  . 
al gruppo con 2 o 3 fdr appartenevano 82 pazienti di cui 22 ( 27% ) con coronarie indenni , 42 ( 51% ) con malattia non significativa e 18 ( 22% ) con malattia significativa . 
al gruppo con 4 o pi fdr appartenevano 32 pazienti di cui 6 ( 19% ) con coronarie indenni , 12 ( 38% ) con malattia non significativa e 14 ( 44% ) con malattia significativa . 
la percentuale di coronarie indenni nei tre gruppi di fdr era 50% , 20% , 0% nei pazienti con dolore tipico e 46% , 24% , 12% in quelli con dolore atipico , mentre la percentuale di malattia significativa nei pazienti con dolore atipico era 0% , 47% , 86% e in quelli con dolore atipico era 4% , 20% , 29% . discussione con lavvento degli scanner di ultima generazione si assistito negli ultimi anni ad un incremento dellaccuratezza diagnostica della tcms grazie ad un progressivo miglioramento delle caratteristiche tecniche ( numero di detettori , risoluzione spaziale e temporale ) che ha reso possibile lo studio del lume e della parete delle coronarie in modo non invasivo [ 13 ]  . 
within a population of patients with nonsignificant cad patients who therefore will not undergo coronary angiography and possible revascularisation at least three broad patterns of atherosclerosis can be easily identified . 
normal coronary arteries absence of changes to the coronary artery wall due to atherosclerosis , nonsignificant disease coronary artery wall disease leading to < 50% stenosis of the lumen , significant disease coronary artery wall disease leading to ( cid : 2 ) 50% stenosis of the lumen . 
una ulteriore stratificazione mostra la prevalenza del tipo di ateromasica , nella popolazione di pazienti con malattia non significativa , suddivisa in placca calcifica ( ossia placche ateromasiche a prevalente contenuto calcifico ) , placca soft ( ossia placche ateromasiche a prevalente contenuto non calcifico ) e placche miste ( ossia placche ateromasiche a contenuto sia calcifico che non calcifico )  . 
il grafico mostra come allinterno della popolazione di pazienti con malattia coronarica non significativa ( e che quindi non andranno incontro a coronarografia ed eventuale rivascolacolarizzazione ) si possano identificare in modo molto semplice almeno tre grossolani pattern di aterosclerosi . 
4a , b distribution of coronary artery disease ( cad ) on the basis of the number of risk factors ( rf ) and clinical presentation ( typical and atypical pain ) at computed tomography ( ct )  . 
the near linear increase in the prevalence of significant cad to the detriment of normal coronary arteries is much more marked in the typical chest pain group than in the atypical group . 
la figura mostra la prevalenza della malattia coronarica , come identificata alla tcms , nella popolazione con dolore toracico tipico ( a ) e atipico ( b ) , studiata allaumentare dei fattori di rischio cardiovascolari ( fdr )  . 
coro indenni , assenza di alterazioni della parete coronarica riferibili ad aterosclerosi ; mal non significativa , malattia della parete coronarica che determina stenosi del lume < 50% ; mal significativa , malattia della parete coronarica che determina stenosi del lume ( cid : 2 ) 50% . 370 radiol med ( 2008 ) 113 : 363372 technical improvements ( number of detectors , spatial and temporal resolution ) , enabling the noninvasive study of the lumen and walls of the coronary arteries [ 13 ]  . 
the aim of our study was not to further the analysis of the diagnostic accuracy of mdct but , rather , to highlight the additional information regarding the presence of mural plaque that mdct is able to produce in contrast to conventional angiography . previous studies have described the prevalence of cad in relation to number of rf [ 15 , 16 ] and clinical presentation [ 16 ]  . 
more recent studies have attempted to demonstrate the relationship between rf , calcium score and cad [ 12 , 18 ] , focussing on the incidence of cad , particularly significant cad , and demonstrating how its prevalence correlates with the increased number of rf and clinical presentation . 
in addition , variations with age and gender have been described . the same assessments can be performed with mdct to detect both critical and , more importantly , noncritical plaque . 
this is highly important , because often the plaque cause positive wall remodelling , with outward expansion rather than shrinkage of the vessel wall , and this is one reason they are underestimated in coronary angiography . plaque characterisation very challenging and much investigated . 
one of the main clinical applications of plaque characterisation is the possibility of assigning different prognostic significance to the different types of plaque , as shown by pundziute et al . 
although other diagnostic techniques provide useful information about plaque , such as calcium scoring [ 20 , 21 ] or intravascular ultrasound ( ivus ) [ 22 , 23 ] , ct - ca offers different information with respect to these tests . 
compared with calcium scoring , which quantifies the presence of calcium in the coronary arteries , ct is able to accurately study the plaque , quantify the degree of stenosis and even identify the noncalcified components . compared with ivus , which is the gold standard for its high level of accuracy , ct - ca has the nonnegligible advantage of being a noninvasive technique . another aim of our study was to emphasise the importance of a thorough patient history and an adequate knowledge of cad to accurately determine the patients risk profile and type of clinical presentation . 
indeed , it appears clear that there is an inverse relationship between the incidence of significant cad and normal coronary arteries and a close correlation between the incidence of significant cad and the increase in rf . 
the incidence of significant cad increases from 4% quelle informazioni aggiuntive riguardanti la presenza di placche parietali che la tcms pu fornire rispetto alla coronarografia . in passato sono stati pubblicati lavori che hanno descritto la prevalenza della malattia coronarica in relazione al numero dei fattori di rischio [ 15 , 16 ] e del quadro clinico [ 16 ]  . 
studi pi recenti hanno voluto dimostrare la relazione esistente tra i fdr , il calcium score e la malattia coronarica [ 12 , 18 ] , focalizzandosi sullincidenza della malattia coronarica , in particolar modo quella significativa e dimostrando come la sua prevalenza sia correlata allaumento del numero dei fdr e alla presentazione clinica . 
sono state descritte , inoltre , le variazioni esistenti tra sessi differenti e diversi gruppi di et . con la tcms le stesse valutazioni possono essere effettuate , sia per quanto riguarda il rilevamento delle placche critiche , ma soprattutto per lindividuazione delle placche non critiche . 
ci molto importante perch spesso le placche determinano un rimodellamento positivo della parete , nel momento in cui si sviluppano maggiormente verso lesterno piuttosto che verso il lume del vaso e questo il motivo per cui vengono sottostimate alla coronarografia . limportanza della definizione del tipo di placca ad oggi un argomento molto stimolante e molto studiato . 
una delle sue principali applicazioni cliniche la possibilit attribuire un significato prognostico in base al differente tipo di placca , come stato dimostrato dal gruppo di pundziute [ 19 ]  . 
esistono altre tecniche diagnostiche che permettono di ottenere informazioni utili sulle placche come il calcium score [ 20 , 21 ] o livus [ 22 , 23 ] , anche se la tcms permette di ottenere informazioni differenti rispetto a questi test . 
rispetto al calcium score , che analizza con un valore quantitativo la presenza di calcio nelle coronarie , la tc offre la possibilit di studiare la placca in modo accurato , di quantificare il grado di stenosi e di valutare anche le componenti non calcifiche . 
rispetto allivus , che rappresenta il gold standard per lelevato grado di accuratezza , la tcms ha il vantaggio non trascurabile di essere una metodica non invasiva . un altro obiettivo del nostro studio stato quello di sottolineare limportanza di unaccurata anamnesi e di una conoscenza adeguata della patologia coronarica per studiare accuratamente il profilo di rischio e le differenti presentazioni cliniche dei pazienti . 
lincidenza della malattia significativa aumenta dal radiol med ( 2008 ) 113 : 363372 to 22% and to 44% in groups with zero to one , two or three and more than four rf , respectively , whereas the incidence of normal coronary arteries decreases from 55% to 27% and to 19% in the same rf groups . 
in addition , in the middle of these two extremes is a large group with nonsignificant cad whose incidence does not appear to be so closely affected by the increase in rf . another fundamental fact can be drawn from a comparison between the distribution of cad in patients with typical chest pain and those with atypical pa figure 4 clearly shows how the slope of the significant cad curve in patients presenting with typical chest pain is very steep , indicating a dramatic increase in incidence with increasing rf , whereas the slope is flatter in patients with atypical pain , suggesting a more gradual increase . 
in the group with typical chest pain , nonsignificant cad tends to decrease significantly with the increase in significant cad , whereas in the group with atypical chest pain , the incidence remains constant . 4% al 22% e al 44% nei gruppi rispettivamente con 0 - 1 , 23 e con pi di 4 fdr mentre lincidenza di coronarie indenni diminuisce dal 55% al 27% e al 19% negli stessi gruppi di fdr . 
inoltre , in mezzo a questi estremi , esiste una larga fascia di popolazione con malattia non significativa la cui incidenza non risulta essere cos strettamente modificata dallaumento dei fdr . un altro dato fondamentale deriva dal confronto tra la distribuzione della malattia nei pazienti con dolore tipico e quelli con dolore atipico ; si pu osservare come differente sia la pendenza della curva della malattia significativa che molto ripida , a indicare un drastico aumento dellincidenza allaumentare dei fdr , mentre ha un andamento pi orizzontale nei pazienti con dolore atipico , espressione di un incremento pi graduale . 
 inoltre interessante notare come varia la malattia non significativa tra i due gruppi ; nel gruppo del dolore tipico questa tende a ridursi in modo significativo per laumentare della patologia significativa , mentre nel gruppo del dolore atipico lincidenza si mantiene costante . conclusions conclusioni mdct - ca plays an important role in the identification of cad in patients with suspected ischaemic heart disease . disease severity and type are closely correlated with the number of rf , and in particular , the incidence of significant cad is directly proportional to the increase in rf , whereas the incidence of normal coronary arteries is inversely proportional to rf and the incidence of nonsignificant cad remains relatively stable . 
cad is also correlated with clinical presentation and takes on different characteristics of severity between patients with typical and those with atypical pain . la tcms ha un ruolo importante nella identificazione della patologia coronarica nei pazienti con sospetta cardiopatia ischemica . 
la severit e il tipo di malattia fortemente correlato al numero dei fdr , in particolare lincidenza di malattia significativa direttamente proporzionale allaumento dei fdr , mentre lincidenza delle coronarie indenni ha un andamento inverso ; andamento pi stabile ha , invece , lincidenza della malattia non significativa . 
the current challenge lies in professional education and development which must be able to ensure a high quality of services , with image interpretation closely correlated to clinical information , given that modern medicine is image guided . 
only a clinical radiologist will be able to interact with the clinician on a par , and assume that central role already assigned to him / her by the current law . 
 although a new concept of health care act is emerging , as a complex and multifaceted set of services , competences , knowledge and actions of several medically and non - medically qualified health care professionals , it needs to be emphasised that the performance of a health care act falls within the scope of team health care , intended not as simultaneous interventions but as consequential actions , in other words a series of actions directed to the same end and carried out by different health professionals . 
 the italian society of medical radiology has approved a statement on the radiological medical act intended as a specialised professional service provided for diagnostic viviamo un periodo di cambiamento epocale nella medicina : in questo contesto la professionalit del medico radiologo ha avuto mutamenti rapidi determinati e condizionati tanto dal tumultuoso incessante evolversi della tecnologia e del mercato , quanto dalle sostanziali modifiche del percorso formativo e del medico radiologo e dei tsrm . 
il momento di sfida rappresentato dalla formazione e dallaggiornamento professionale che devono essere in grado di assicurare elevata qualit di prestazioni , con interpretazione strettamente correlata alla clinica , e tanto perch the modern medicine is image guided . 
 per quanto sia emergente una nuova concezione dellatto sanitario , come un insieme complesso ed articolato di prestazioni , competenze , conoscenze ed agire di pi professioni , non solo mediche , si precisa che lo svolgimento dellatto sanitario si inserisce nellambito delle prestazioni sanitarie di equipe , non nel senso della contestualit degli interventi , ma nel senso di una serie di atti consequenziali , cio di un insieme di azioni concorrenti ad un fine unitario e svolte da diverse figure professionali . 
 la societ italiana di radiologia medica ha approvato un documento su latto medico radiologico inteso come prestazione professionale specialistica che ha finalit diagnostiradiol med ( 2008 ) 113 : 319328 motivated request inclusive of clinical query from referring physician evaluation of clinical information and review of possible previous imaging investigations justification of the proposed examination ( or motivated non - justification with possible suggestion of alternative techniques and methods ) table 1 radiological medical act provision of information and informed consent execution adequacy of equipment / optimisation effective professional competence technical aspects of the procedure images interpretation / reporting communication / discussion with the clinician archiving tabella 1 atto medico radiologico adeguatezza delle attrezzature / ottimizzazione competenza professionale effettiva aspetti tecnici della procedura documentazione iconografica interpretazione / refertazione comunicazione / discussione con il clinico archiviazione inquadramento clinico - anamnestico , con valutazione di eventuali esami precedenti motivata richiesta di prestazione del medico prescrivente con quesito clinico giustificazione dellesame proposto ( o non giustificazione motivata con possibile proposta di tecniche e metodologia sostitutive ) esecuzione informativa per il consenso e consenso and / or interventional purposes and consisting of a series of closely interrelated and inseparable steps ( table 1 )  . 
 motivated request inclusive of clinical query from referring physician motivata richiesta di prestazione del medico prescrivente con quesito clinico a request for a diagnostic imaging examination should be intended as a request for a service to be provided by a specialist in diagnostic imaging . 
notwithstanding that all requests should be accurately completed , certain cases may require clinico - radiological meetings to justify the imaging study and / or propose alternative techniques and methods . 
the ultimate aim is for requests to contain the clinical query and accurate clinical information to enable the radiologist to select the most appropriate imaging technique for the individual case . 
 linvio di una richiesta desame di dpi va intesa come una richiesta di prestazione da parte di uno specialista in dpi . per quanto sia auspicabile che le richieste siano sempre compilate accuratamente , talvolta , al fine della giustificazione dellindagine e / o per la proposta di tecniche e metodologie diverse , sono auspicabili riunioni clinico - radiologiche . 
lobiettivo quello di giungere a richieste nelle quali sia indicato il quesito clinico con accurata anamnesi e il medico radiologo dovr scegliere tra le metodologie la pi appropriata al caso . 
 radiol med ( 2008 ) 113 : 319328 evaluation of clinical information and review of possible previous imaging investigations inquadramento clinico - anamnestico , con valutazione di eventuali esami precedenti radiologists must be supplied with all the relevant clinical information in order for them to reach , on the basis of their specific competence , the most correct evaluation of each clinical case . 
only if the radiologist has access to this information , as well as possible previous imaging studies , will he / she be able to fulfil the next requirement ( justification ) , and establish the most appropriate temporal sequence for the imaging studies . 
 il medico radiologo deve essere a conoscenza degli elementi che gli possano consentire , sulla base della competenza della propria specialit , il pi corretto inquadramento del singolo caso clinico . 
solo in tal modo , infatti , egli potr e dovr , anche in considerazione della valutazione di eventuali esami precedenti , procedere al punto successivo , definendo inoltre la pi idonea sequenza temporale delle indagini strumentali . 
 justification of the proposed examination ( or motivated non - justification with possible proposal of alternative techniques and methods ) a procedure is justified for a given patient if it produces more benefit than harm , and in any case if it influences patient care . 
the process of justification involves an initial general justification for each diagnostic examination or interventional procedure , and a specific justification relating to the individual patient after assessment of the clinical data , specific situation , technology available , operators experience / competence , organisational context and economic impact . 
 in consideration of the wide variations in the usage of healthcare procedures and interventions and the actual impossibility of continuing professional development for each professional , the assr ( italian agency for regional health services ) in collaboration with the scientific associations and the ministry of health published the national guidelines in diagnostic imaging ( official gazette of may 2 , 2005 )  . 
the guidelines are to be intended as recommendations for clinical practice , formulated through a process of systematic review of the literature and expert opinion , with the aim of assisting physicians and patients in making decisions regarding the most appropriate healthcare pathways in specific clinical situations . 
 the guidelines aim at reducing the number of inappropriately requested and performed imaging investigations and helping improve contact between the referring physician and the diagnostic imaging specialist so as to optimise the diagnostic pathways and thus resource utilisation . 
 it is , however , understood that in routine cases ( e.g. , chest x - ray , radiological examinations for minor injuries , ) giustificazione dellesame proposto ( o non giustificazione motivata con possibile proposta di tecniche e metodologie sostitutive ) giustificata una procedura per un determinato paziente se essa comporta in concreto pi beneficio che danno , influenzando comunque il management del paziente . 
questo deve avvenire attraverso una prima giustificazione di base per ogni singolo esame diagnostico o procedura interventistica ed una giustificazione specifica relativa al singolo paziente attraverso la valutazione del caso , della situazione specifica , della disponibilit tecnologica , dellesperienza / competenza delloperatore , del contesto organizzativo e dei risvolti economici . 
le linee guida vanno intese come raccomandazioni di comportamento clinico , elaborate mediante un processo di revisione sistematica della letteratura e delle opinioni di esperti , con lo scopo di aiutare i medici e i pazienti a decidere le modalit assistenziali pi appropriate in specifiche situazioni cliniche . 
i percorsi diagnostico - terapeutici rappresentano i risultati degli adattamenti delle linee guida alle situazioni locali , con le loro specifiche caratteristiche organizzative e gestionali . quindi , legittimo considerare che le stesse linee - guida possano trovare modalit di applicazioni diverse a seconda dei diversi contesti regionali e locali . 
 gli obiettivi delle linee guida sono una riduzione del numero degli esami radiologici inappropriatamente richiesti ed eseguiti e quello di contribuire a migliorare i contatti tra il medico curante / prescrivente e lo specialista in dpi nellottica della ottimizzazione dei percorsi diagnostici e quindi di una migliore utilizzazione delle risorse . 
 resta comunque logicamente inteso che per i casi della pratica corrente ( es . , esame radiologico del torace , esami radiologici per piccola traumatologia , ) il tsrm , in col322 radiol med ( 2008 ) 113 : 319328 the radiographer , in constant liaison with the radiologist , autonomously performs the technical phase of the examination for which he / she is competent , using methodologies previously agreed and shared with the radiologist . 
this development should , however , be addressed in a rational and balanced manner avoiding any headlong rush : if misapplied , technological developments can result in the creation of inappropriate organisational and management models , considering that radiology is a clinical service not a reporting service ! ! legamento costante con il medico radiologo , svolge in autonomia professionale la fase tecnica di competenza , sulla base di modalit preventivamente concordate e condivise con il medico radiologo . 
ma questa evoluzione va vissuta in modo razionale e con equilibrio senza incorrere in fughe in avanti : levoluzione tecnologica , se mal gestita , porta a definire modelli organizzativi e gestionali non corretti in radiologia considerando che radiology is a clinical service not a reporting service ! ! provision of information and informed consent informativa per il consenso e consenso tion , in routine clinical practice rente , sempre previa informazione ; the current regulations contain precise instructions with regard to how consent should be obtained : it is incorrect to state that in routine clinical practice consent should always and without exception be expressed in writing . 
the only exception to the principle of mandatory consent to a medical act is represented by a state of necessity , that is , in the case of urgent / emergent care . 
the duty to inform the patient , although the responsibility of the radiologist , also rests with the radiographer , within the limits of his / her area of competence , i . 
screening has created a new scenario , in which the radiologist and the patient have a direct relationship without the intermediation of the referring physician , and the radiologist assumes significant responsibility for overall clinical management . 
 le normative vigenti contengono precise disposizioni in merito allacquisizione del consenso : non lecito affermare che il consenso nella comune pratica medica debba essere sempre e categoricamente espresso in forma scritta . 
 le esposizioni per ricerca sono possibili solo a seguito di consenso scritto espresso liberamente e consapevolmente . lunica deroga al principio della tassativit del consenso allatto medico rappresentata dallo stato di necessit . , cio nellassistenza in urgenza indifferibile / emergenza . 
il dovere di informazione dellammalato , pur se compito del medico specialista , grava anche sul tsrm , in relazione alle sue competenze professionali , cio limitatamente allaspetto tecnico dellesame un aspetto particolare riguarda linformativa per il consenso nellambito della prevenzione secondaria delle malattie laddove la diagnostica per immagini ha svolge e svolger un ruolo fondamentale . 
si viene a creare un nuovo scenario con una relazione diretta medico radiologo / paziente , senza lintermediazione del medico prescrivente , con significativa responsabilit nella gestione clinica complessiva dellutenza . 
 radiol med ( 2008 ) 113 : 319328 execution this phase comprises several parameters : adequacy of equipment - optimisation effective professional competence technical aspects of the procedure images connected to justification is the requirement of optimisation , whereby each exposure must be kept as low as readily achievable , a duty that clearly involves the radiologist and the radiographer . 
 the radiologist must have a valid competence in modalities suitable for both elective and urgent - emergent care settings : this competence cannot logically be maximal for all technological - methodological aspects , but it must be represented by the lowest common denominator of at least those core competences required for dealing with any situation , perhaps even pending consultation with a colleague more knowledgeable in the specific technological - methodological , diagnostic and interventional aspect . 
as much as it seems logical in interventional radiology , the final judgement on the patients eligibility to undergo a radiological procedure requiring contrast material falls within the exclusive remit of the radiologist , who bases his / her decision on the assessment of the patients clinical data , history , and laboratory findings . 
this aspect falls within the principle of reasonable , mitigated , relative , concerted and planned allocation of tasks and responsibilities . delegation should therefore be intended as a natural acknowledgement of the qualification and greater responsibility of the radiographer , to whom the physician allocates the practical aspects of the examination , in part to promote the efficiency of the whole organisation . 
additionally , it emerges that the radiographer cannot practise in the absence of a medical referral and without the radiologist assuming clinical responsibility for the justification of procedures ( which , as stated previously , does not need to be expressed for each case but , in the most common cases , can be expressed as a procedure protocol validated by the head of the radiological facility ) , and in any case always in full respect of the radiation esecuzione questa fase si compone di molteplici parametri : adeguatezza delle attrezzature - ottimizzazione ; competenza professionale effettiva ; aspetti tecnici della procedura ; documentazione iconografica . collegato alla giustificazione il principio dellottimizzazione secondo il quale ogni esposizione deve essere mantenuta bassa quanto ragionevolmente possibile ( as low as readily achievable ) , e coinvolge logicamente sia il medico specialista radiologo che il tsrm . 
 il medico radiologo deve possedere valida competenza delle metodologie utilizzabili tanto in elezione che in urgenza - emergenza : tale competenza , logicamente , non potr essere massima per ogni aspetto tecnico - metodologico ma dovr essere rappresentata come minimo comun denominatore da quelle capacit almeno di base per poter gestire ogni situazione , magari anche in attesa di un eventuale riscontro successivo da parte di altro collega pi specificatamente competente nel particolare aspetto tecnico - metodologico , diagnostico ed interventistico . 
pare logico poter affermare e ribadire , sin da ora , che nel minimo comun denominatore non debbano essere comprese complesse manovre di radiologia interventistica che va effettuata da medici radiologi con specifica e verificata esperienza nel campo . 
per quanto appaia logico in radiologia interventistica , il giudizio finale sullidoneit del paziente ad essere sottoposto a prestazione radiologica che necessiti di somministrazione di mdc di competenza esclusiva del medico radiologo , sulla base dellinquadramento clinico - anamnestico e laboratoristico ritenuto necessario . 
 il medico radiologo indirizza , nel rispetto delle competenze professionali , lattivit svolta dal tsrm concordandola e programmandola con questa figura professionale . rientra questo aspetto nel principio dellaffidamento ragionevolmente inteso , temperato , relativo , concordato e programmato . 
la delega quindi va intesa come logico riconoscimento di qualificazione e di maggiore responsabilit per il tsrm , cui il medico specialista affida gli aspetti pratici di competenza , anche con lobiettivo di promuovere lefficienza dellintera organizzazione . 
emerge peraltro che lattivit del tsrm non sia effettuabile in assenza di prescrizione medica e senza la responsabilit clinica del medico specialista nel processo di giustificazione delle procedure ( che , come gi sottolineato , non necessariamente espressa in ogni singolo caso , ma , nelle pratiche pi comuni , espressa come protocollo validato dal responsabile dellimpianto radiologico di svolgimento del processo ) , e 324 radiol med ( 2008 ) 113 : 319328 protection regulations laid out by the european union . 
this does not mean depriving radiographers of any initiative , provided that this falls within the scope of the areas of competence regulated by their professional qualification and that the initiative is taken in constant liaison with the radiologist , also to be able transfer to the radiologist any useful information and / or seek possible operating clarifications . 
the executive / technological phase notwithstanding the radiologists active participation in the execution of examinations where this is required due to clinical - diagnostic reasons ! does not coincide with the radiological medical act but is a part of it ! ! it is therefore not possible to hypothesise a separation between clinical aspects , on the one hand , and purely executive , technological aspects , on the other . 
 even in telemanagement it is understood that in current practice ( e.g. , chest x - rays , radiological investigations for minor injuries , ) the radiographer , liaising constantly with the radiologist , autonomously carries out the technical phase for which he / she is competent , on the basis of methodologies previously agreed and shared with the radiologist . 
if necessary , the radiologist can request that the images be processed for documentation purposes , a task that is carried out by the radiographer on the basis of previously defined protocols , except in the case of direct intervention of the radiologist for clinical purposes . 
tanto logicamente non vuol significare privare luso di ogni iniziativa al tsrm , sempre logicamente nellambito delle sua competenza professionale normata peraltro anche dal percorso formativo e sempre in un collegamento costante anche al fine di trasferire al medico radiologo ogni informazione utile e / o per richiedere eventuali precisazioni operative . 
la fase esecutiva / tecnologica ferma restando la partecipazione attiva esecutiva del medico radiologo , laddove per motivazioni clinico - diagnostiche se ne ravveda la necessit ! non si identifica con latto medico radiologico ma fa parte dello stesso ! ! non risulta possibile , quindi , ipotizzare una divisione tra laspetto clinico da un lato e quello puramente esecutivo , tecnologico dallaltro . 
 anche in telegestione inteso che nella pratica corrente ( es . , esame radiologico del torace , esami radiologici per piccola traumatologia , ) il tsrm , in collegamento costante con il medico radiologo , svolge in autonomia professionale la fase tecnica di sua competenza , sulla base di modalit preventivamente concordate e condivise con il medico radiologo . 
la valutazione dellutilit diagnostica delliconografia , compete al medico radiologo , il quale ne dispone leventuale elaborazione ai fini documentali che viene effettuata dal tsrm , sulla base di protocolli preventivamente definiti , salvo lintervento diretto del medico specialista ai fini clinici . 
 interpretation / reporting / communication / discussion with the clinician interpretazione / refertazione / comunicazione / discussione con il clinico interpretation and reporting represent the most significant phase of the radiological medical act . 
interpretation , especially in urgentemergent situations , must be immediate and timely and , whenever particularly severe findings are detected , these must be transmitted to the clinician , initially even only verbally , to enable the most appropriate treatment strategies and possible complementary diagnostic investigations to be undertaken . 
sono i momenti in cui il radiologo esprime la sua valutazione di medico , con la semeiologia della propria specialit , al quesito posto dal clinico ed quindi la sintesi della prestazione intellettuale medico - specialistica . 
linterpretazione , specie in casi di urgenza - emergenza , deve essere immediata e tempestiva e laddove si rilevino elementi di particolare gravit deve essere fornita al clinico , anche se solo verbalmente in una prima fase , per i pi opportuni provvedimenti terapeutici ed eventualmente diagnostici integrativi . 
 radiol med ( 2008 ) 113 : 319328 it is worth emphasising that reporting represents the validation of the entire radiological work - up and that interpreting and reporting are a radiologists core duties . 
 reporting , which encompasses a series of closely related steps ( perception , description , interpretation , decision , conclusion / opinion ) represents the opinion of the radiologist : it is , in other words , a subjective interpretation of an objective finding . 
 a specific aspect of reporting is that of image reconstruction : this is an important component of the radiological act , owing to the active process of interaction with the images . 
in many cases image reconstruction using non - standard planes or parameters is dictated by the needs of the radiologist during the reporting phase : in fact , digital imaging and the use of reconstructions renders all radiological investigations increasingly operator - dependent . 
even in this field , it should , however , be recalled that many reconstructions have become routine and standardised : in this case , the execution of reconstructions , preliminarily agreed , in common practice is entrusted to the radiographer . 
 the report should include , in addition to the patients identification data , the clinical query and reference to the technique or methodology used , a description of the pathological findings , interpretation and / or diagnostic hypothesis , and a proposal for additional and / or follow - up studies . on the issue of report writing , we feel it necessary for the report to contain also the clinical query : in practical terms the report is a reply to a question , and therefore no reply can exist ( = report ) without a question ( = query )  . 
soft - copy reporting is a necessary step towards the complete digitalisation of the diagnostic process and the introduction of image processing and computer - assisted diagnosis techniques into clinical practice . 
as a result , there is increased use of new reporting methods for electronic data management , which supersedes the combination of text / image ( paper / film ) merging them into objects of a similar nature , where the text is replaced by a hypertext . 
a targeted selection to illustrate the findings , with the aim of better meeting clinical needs : this also forms an integral part of the radiological medical act given the radiologists exclusive professional expertise for selecting the images . 
for the report to have legal status and value and be accepted as legal evidence , it must bear the reporting physicians legible signature , if pavale la pena sottolineare che la refertazione assume valore di validazione di tutto liter radiologico che linterpretazione e la refertazione sono obblighi istituzionali per il medico radiologo . 
lottimizzazione del referto obiettivo da perseguire e tanto perch , ancora oggi , esiste molta variabilit dovuta a diversi fattori ( impropriet di linguaggio , scarsa chiarezza , eccessivo tecnicismo , differenti destinatari , differente tipologia di utente esterno , interno , )  . 
 la refertazione che prevede vari momenti strettamente correlati ( percezione , descrizione , interpretazione , decisione , conclusione / opinione ) rappresenta lopinione di un medico radiologo : cio linterpretazione soggettiva di un elemento obiettivo . 
in molti casi la ricostruzione delle immagini , secondo piani o parametri diversi da quelli standardizzati , dettata da esigenze del medico radiologo in fase di refertazione : in effetti limaging digitale ed il ricorso alle ricostruzioni rende tutte le indagini sempre pi operatore - dipendenti . 
anche in questo settore va per ricordato che molte delle ricostruzioni sono ormai diventate routinarie e standardizzate : in questo caso la loro esecuzione , preliminarmente gi concordata , viene affidata nella pratica corrente al tsrm . 
 il referto dovrebbe comprendere , oltre che logicamente i dati identificativi , il quesito clinico a monte ed il riferimento alla tecnica ed alla metodologia impiegate , la descrizione dei reperti patologici riscontrati , linterpretazione e / o lipotesi diagnostica nonch la proposta di ulteriori accertamenti e / o controlli . 
in tema di elaborazione , si ritiene che il referto debba contenere anche il quesito clinico : in concreto il referto la risposta ad un quesito , pertanto non vi pu essere una riposta ( = referto ) se non vi una domanda ( = quesito )  . 
la refertazione soft - copy un passaggio obbligato per la completa digitalizzazione del processo diagnostico e per lintroduzione nella pratica clinica di tecniche di elaborazione delle immagini e di ausilio alla diagnosi ( cad = computer assisted diagnosis )  . 
pertanto si diffondono sempre pi nuove metodologie di refertazione per la gestione elettronica dei dati , il che fa perdere senso allaccoppiata testo / immagini ( carta / pellicole ) fondendole in oggetti della stessa natura , in cui il testo viene sostituito da un ipertesto . 
al referto quindi si pu allegare solo una parte delliconogafia , quale scelta mirata di quanto descritto nel referto , nella logica di soddisfare al meglio le esigenze cliniche : questo fa parte integrante dellatto medico radiologico per lesclusiva capacit professionale di selezione delle immagini . 
il referto , per avere dignit giuridica e per ot326 radiol med ( 2008 ) 113 : 319328 per - based , or a qualified electronic signature in accordance with the current law . 
 the objective of revitalising contacts between the treating / referring physician and the radiologist is paramount not only in the justification phase but also in subsequent phases , that is , where an interdisciplinary meeting is deemed necessary to discuss a radiological finding . 
clinico - radiological meetings , whether one - to - one or group meetings , should become more frequent so that each specialist can , and should , bring his / her significant and often crucial contribution to patient management . 
the radiologists report should specify that the report is based on images transmitted electronically , and indicate the individual / s responsible for executing the examination , the referrer and the method of transmission . 
an important aspect is the number of images received electronically : in specifying that the report constitutes legal evidence exclusively with regard to the images received , teleradiology reports should explicitly indicate the number of images received and evaluated . 
the use of telediagnosis limited to the sole ( tele ) reporting phase does not appear in any way acceptable , on account of the interrelated phases of the radiological medical act . 
the medical situations that may lead to the use of teleconsultation include the need for specific competences in given fields , an uneven distribution of resources and competences , and access to excellence . 
 lobiettivo di rivitalizzare i contatti tra medico curante / prescrivente e medico radiologo irrinunciabile non solo nel processo di giustificazione ma anche a valle , cio nel momento laddove si ritiene opportuna un confronto interdisciplinare sul reperto riscontrato . 
riunioni clinico - radiologiche , di gruppo o singole , vanno incrementate e tanto perch ogni specialista , possa e debba apportare un significativo e spesso determinante contributo nel management del paziente . 
opportuno che il medico radiologo precisi che il referto stesso stato eseguito su immagini ricevute per via telematica , segnalando inoltre lo / gli esecutore / i dellindagine , il medico prescrivente e le modalit di trasmissione . 
tra le esigenze mediche che possono portare allutilizzo del teleconsulto si segnala la necessit di specifiche competenze in alcuni settori , per una distribuzione non omogenea delle risorse e delle competenze , per un accesso alleccellenza . 
 in conventional or analogic radiology , films constitute the unique and unmodifiable record , and are stored in the radiology division archives or given to the patient together with the report , in accordance with the regulations . 
 in digital radiology , the record is represented by digital images acquired and reconstructed through the application of the most appropriate software , and selected by the radiologist for each individual patient on the basis of the medical data and the clinical query that justified the investigation . images obtained in this manner constitute the imaging sia il reperto che il referto sono soggetti ad archiviazione per legge . 
 noto come in radiologia tradizionale o analogica le pellicole costituiscono il reperto , unico e non modificabile , e siano conservate negli archivi di reparto o consegnate al paziente assieme al referto , secondo normativa . 
 in radiologia digitale , infatti , il reperto costituito dallinsieme delle immagini in formato digitale , acquisite e ricostruite mediante lapplicazione dei programmi specifici ritenuti pi idonei , scelti per ciascun paziente dal radiologo in relazione al quadro ed al quesito clinico , e che hanno giustificato lindagine . 
sono le immagini cos ottenute che costituiscono il reperto iconografico : sono parte integrante radiol med ( 2008 ) 113 : 319328 record : they are an integral part of the professional service that allows the radiologist to formulate the clinical - radiological considerations and deductions contained in the report which , whether paper - based or digital , must always be retained and stored indefinitely . 
 the radiologist may attach all of the images to the report or only a selection of images to illustrate the findings described in the report and to be used by the patient or referrer , in a perspective of best meeting the clinical needs ( structured report )  . 
 partly for radiation protection purposes , there is a legal requirement to store all ( analogic or digital ) images obtained with the use of ionising radiation for a minimum of ten years , unless they are given to the patient . 
this means storing diagnostic images produced with conventional methods on film or , in the case of digital imaging , not the proprietary raw data but the native images obtained by using proprietary software that manipulates and processes the raw data allowing reconstruction and elaboration ( dicom format )  . 
 it is implied that the same raw data , if processed with different processing algorithms or in response to different clinical queries , will produce different images from those used by the radiologist when performing and reporting the examination to answer the clinical query . 
 the radiologist should also indicate the imaging environment used for his / her radiological medical act and apply his / her electronic digital signature and temporal marking on the report and images used for the professional service in an unmodifiable manner . 
 conclusions the epochal changes underway in the field of health care and education of medical and non - medical health professionals have resulted in a transformation of the professional model . 
in radiology , the main goal in this challenge is the della prestazione professionale e che hanno consentito di formulare le considerazioni e le deduzioni clinico - radiologiche contenute nel referto , che deve essere comunque conservato a tempo indeterminato , sia esso cartaceo che digitale . 
 il radiologo pu allegare al referto tutte , o una parte , quale scelta mirata delle immagini utilizzate , ad evidenza di quanto descritto nel referto e ad uso del paziente e del curante nella logica di soddisfare al meglio le esigenze cliniche ( referto strutturato )  . 
 in base alla normativa in vigore , anche ai fini radioprotezionistici , vi lobbligo , se non consegnate al paziente , di conservare ed archiviare le immagini , analogiche o digitali , ottenute con radiazioni ionizzanti per il tempo previsto dalla normativa , non inferiore ai 10 anni ; pertanto devono essere conservate le immagini prodotte ai fini diagnostici con supporti tradizionali su pellicola o , per le indagini ottenute in maniera digitale , non dei raw data ( dati grezzi e proprietari ) ma delle immagini native , ottenute con i sistemi software proprietari che modificano e processano i dati grezzi , che ne consentono la loro ricostruzione ed elaborazione ( formato dicom )  . 
 implicito che gli stessi dati grezzi possono produrre , con diverse elaborazioni o per quesiti clinici diversi , immagini differenti da quelle utilizzate dal medico radiologo nellatto proprio desecuzione e refertazione per rispondere al quesito diagnostico dellesame . 
in radiologia , la grande sfida ha come obiettivo primario la clinicizzazione del medico radiologo , padrone delle tecniche , delle metodologie e 328 radiol med ( 2008 ) 113 : 319328 clinicalisation of the radiologist , who has a deep knowledge of imaging techniques , methodologies and informatics , and is an expert in current laws and regulations and relationships with users and other medical and non - medical health professionals . 
 once more and today for the future ! academic institutions , with the support of hospitals , the scientific society and the national radiologists union ( snr ) are called upon to seriously and constructively act together in the primary interest of users and the entire society towards an increasing qualification of the radiologist in performing the radiological clinical act . 
 ancora una volta , ed oggi per il domani ! , le istituzioni universitarie per la formazione , con il concreto determinante supporto delle strutture ospedaliere , la societ scientifica ed il snr , in piena comunit di intenti , sono chiamate ad un interesse impegno serio e costruttivo , nel primario dellutenza e quindi della societ tutta , per un sempre maggiore qualificazione del medico radiologo nello svolgimento del suo atto clinico . 
gandini1 1radiologia diagnostica universitaria , ospedale san giovanni battista , via genova 3 , 10126 torino , italy 2struttura complessa fisica sanitaria i , ospedale san giovanni battista , corso bramante 88 / 90 , 10126 torino , italy correspondence to : o . 
effective dose rates and entrance skin - dose ( esd ) rates per minute of fluoroscopy were measured by using a plexiglas phantom ( thickness 10 cm ) simulating the patient and by varying the exposure parameters ( type of pulsed fluoroscopy , image intensifier diameter , presence of diaphragms ) to identify the technique delivering the lowest patient dose . 
sono stati misurati i ratei di dose efficace e di dose superficiale in ingresso ( esd ) per minuto di scopia , simulando la presenza del paziente con fantoccio in plexiglass di 10 cm di spessore e variando i parametri di esposizione ( tipo di scopia pulsata , diametro ib , presenza di diaframmi ) al fine di individuare le modalit che consentono di minimizzare la dose . 
sono stati stabiliti i parametri di esposizione che consentono di ottenere la qualit di immagine desiderata con la minima dose , per lapparecchiatura utilizzata e per questa tipologia di procedure . 
i valori di dose efficace e le considerazioni conseguenti relative alla probabilit di induzione di tumori letali consentono di affermare che i benefici associati a questo tipo di procedure giustificano ampiamente lesposizione del paziente al rischio radiologico associato . 430 radiol med ( 2008 ) 113 : 429438 keywords paediatric liver transplantation dosimetry percutaneous biliary drainage bilioplasty parole chiave trapianto di fegato pediatrico dosimetria drenaggio biliare percutaneo bilioplastica introduction introduzione biliary complications in liver transplantation are the most frequent cause of postoperative morbidity , with incidence rates of 30%60% . 
mostly strictures or fistulae , these complications appear more frequently within the first 3 months after surgery ( early complications ) and rarely after the first year ( late complications )  . 
anastomotic strictures are also a frequent complication of paediatric liver transplantation . they may appear within the first few weeks as a result of technical errors or ischemic , immunological or infectious causes , or after several months , usually as a result of relapse or chronic evolution of early complications . 
among minor biliary complications , the most common ( 6%29% ) is the formation of debris , stones and biliary sludge of varying severity [ 1 , 2 ]  . treatment for biliary complications , such as strictures of the biliodigestive anastomosis or lithiasis , by percutaneous biliary drainage and bilioplasty or by lithotripsy is successful in most cases , allowing resolution without surgical revision or repeat transplantation [ 3 , 4 ]  . 
the use of interventional procedures in children who have undergone orthotopic liver transplantation ( olt ) allows a safe and minimally invasive approach to many postoperative complications and spares the patients further surgical procedures [ 5 , 6 ]  . 
percutaneous biliary drainage , as well as permitting the performance of direct cholangiography , allows drainage and saline lavage of the bile duct and is the first step in subsequent treatment with bilioplasty and lithotripsy . percutaneous treatment of biliary complications is also the initial approach in children who have undergone olt [ 7 , 8 ]  . 
however , reduced patient cooperation , long fluoroscopy times and the need for repeat procedures demand that special attention be paid to radiation protection issues , in consideration of the higher sensitivity to ionising radiation and the longer life expectancy of paediatric patients . the radiological risk associated with these procedures may be deterministic , in particular with regard to possible skin injury , or it may be stochastic , referring to the increased likelihood of cancer . 
the dosimetric quantity used to evaluate deterministic effects to the skin is the entrance skin dose ( esd ) , whereas stochastic risk can be measured by estimating the effective dose . 
in addition to these , the dose - area product ( dap ) is an indicator of the total patient dose and can serve as a valuable tool for comparison . le complicanze biliari nel trapianto di fegato rappresentano la pi frequente causa di morbilit post chirurgica , con percentuali del 30%60% ; si tratta principalmente di stenosi o fistole , ed insorgono pi frequentemente nei primi tre mesi ( complicanze precoci ) , pi di rado dopo il primo anno ( complicanze tardive )  . 
le stenosi anastomotiche rappresentano anche nel trapianto pediatrico le complicanze pi frequenti ; si manifestano entro le prime settimane per causa ischemica , immunologica , infettiva o errore tecnico oppure dopo molti mesi dal trapianto solitamente per recidiva o cronizzazione di complicanze precoci . 
tra le complicanze biliari minori la pi frequente ( dal 6% al 29% ) rappresentata dalla formazione di detriti , calcoli e sludge biliare di varia entit sino ai quadri pi gravi [ 1 , 2 ]  . il trattamento delle complicanze biliari post trapianto epatico , quali la stenosi dellanastomosi bilio - digestiva o la litiasi , mediante procedure di drenaggio biliare percutaneo transepatico associato a bilioplastica o litotripsia percutanea consente di risolvere il maggior numero di complicanze di questo tipo senza ricorrere alla revisione chirurgica o al ritrapianto [ 3 , 4 ]  . 
il ricorso a procedure interventistiche in pazienti pediatrici sottoposti a trapianto di fegato ( olt , orthotopic liver transplant ) consente di affrontare in modo sicuro e poco invasivo le molte complicanze post - chirurgiche , evitando ai pazienti ulteriori interventi chirurgici [ 5 , 6 ]  . 
il drenaggio biliare percutaneo , oltre a consentire lesecuzione di un colangiogramma diretto , consente il drenaggio della bile , lesecuzione di lavaggi con soluzione fisiologica ed il primo tempo per il successivo trattamento con bilioplastica e litotripsia . il trattamento percutaneo delle complicanze biliari rappresenta attualmente il primo approccio anche nel paziente pediatrico sottoposto ad olt [ 7 , 8 ] ; tuttavia la scarsa collaborazione dei pazienti , i lunghi tempi di fluoroscopia e la necessit di trattamenti spesso ripetuti nel tempo , impongono di porre estrema attenzione agli aspetti radioprotezionistici tenendo conto della maggiore suscettibilit alle radiazioni ionizzanti e la maggiore spettanza di vita del paziente pediatrico . 
i rischi di natura radiologica associati a tali procedure possono essere di carattere deterministico , in particolare per la possibilit di danni alla cute , e stocastico , con laumento della probabilit di insorgenza di neoplasie . risulta quindi utile una valutazione della dose ricevuta dal paziente per stimare la severit del rischio associato allesposizione . 
la grandezza dosimetrica che consente di valutare il raggiungimento di effetti deterministici alla cute radiol med ( 2008 ) 113 : 429438 the purpose of this study was to evaluate the dose to the patient , through measurements and calculations , of the various exposure conditions during a procedure to obtain information for dose optimisation . 
in three cases , we performed in vivo measurements to evaluate the effective dose to the patient and present some considerations about the related risks . materials and methods between october 1999 and november 2006 , eight children with post - olt biliary complications underwent interventional biliary drainage with bilioplasty at our institution . 
in vivo measurements of patient dose were obtained during procedures on three patients ( two girls and one boy ; ages 14 months , 3 years and 5 months , and 3 years , respectively ; mean age 30.3 months ) who presented with tight stenosis of the biliodigestive anastomosis after olt . 
in addition , measurements were obtained by simulating the operating conditions with a 10 - cm - thick plexiglas phantom . interventional procedure when placing the transhepatic biliary drain and performing bilioplasty with balloon catheters in children , special care must be taken to minimise exposure by limiting the use of ionising radiation as far as possible and employing ultrasonography . 
after cholangiography with a brief fluoroscopy run with reduced parameters to confirm the outla dose dingresso superficiale ( esd , entrance skin dose ) mentre il rischio stocastico pu essere quantificato per mezzo di una stima della dose efficace . 
accanto a queste grandezze inoltre utile la valutazione del prodotto dose per area ( dap ) come indicatore di dose totale al paziente e strumento di confronto . scopo del lavoro stato quello di valutare la dose al paziente , mediante misure e calcolo , per le diverse condizioni di esposizione che si verificano durante una procedura , in modo da ottenere informazioni utili per lottimizzazione della dose . 
in tre casi sono state inoltre effettuate delle misure in vivo che hanno permesso di valutare la dose efficace al paziente e di effettuare delle considerazioni sul rischio correlato . materiali e metodi nel periodo tra ottobre 1999 e novembre 2006 presso listituto universitario di radiodiagnostica dellospedale molinette ( torino ) sono state eseguite procedure interventistiche di drenaggio biliare con bilioplastica su 8 pazienti pediatrici con complicanze biliari post olt . 
b previa embolizzazione del tramite sotto guida ecografica con spirale metallica si rimuove laccesso percutaneo . dosimetric measurements in addition to the measurements normally recorded for our quality - assurance programme , specific dosimetric measurements were performed to characterise the device used and produce a reliable dose estimate . 
to assess the impact of operator - dependent exposure parameters ( fluoroscopy mode , image intensifier diameter and field - limiting diaphragm ) , measurements were performed by simulating the operating conditions , with a 10 - cm - thick plexiglas phantom , focus - patient distance 75 cm , focus - image intensifier distance 120 cm , posteroanterior projection with the beam perpendicular to the bed . 
negli altri due casi per il posizionamento di catetere di drenaggio biliare interno od interno - esterno si utilizzata la guida ecotomografica ed un rapido flash di scopia al termine della manovra . il successo tecnico stato totale nei casi in esame e non si sono verificate complicanze peri - procedurali , ci ha permesso di ridurre al minimo il tempo medio di scopia che stato di 3 , 7 minuti . misurazioni dosimetriche oltre a quelle normalmente eseguite nellambito del programma di controllo della qualit , per eseguire una affidabile stima preventiva della dose sono state eseguite misure dosimetriche specifiche per la caratterizzazione dellapparecchio utilizzato . 
per valutare linfluenza dei parametri di esposizione selezionabili dalloperatore ( tipo di scopia , diametro dellib e diaframmatura del campo ) sono state effettuate misure simulando le condizioni operative delle procedure , con un fantoccio in plexiglass di 10 cm di spessore , distanza fuoco ingresso paziente di 75 cm , distanza fuoco ib di 120 cm , proiezione pa con fascio perpendicolare al lettino . 
per le misure stata utilizzata una camera a ionizzazione trasmissiva a doppio canale con misura contemporanea di dap e kerma in aria puntuale ( diamentor m4kdk , ptw , freiburg )  . 
nel caso di misure in vivo , oltre alle misure con camera trasmissiva per valutare le dimensioni del fascio allingresso sul paziente sono state utilizzate pellicole kodak x - omat v [ 9 ]  . 
tra le tipologie di scopia , risulta che la pulsata indicata sul tavolo di comando con i due impulsi quella 434 radiol med ( 2008 ) 113 : 429438 fig . 
5 valori di dose in ingresso per minuto di scopia al variare del diametro dellib ( diversi ingrandimenti dellimmagine ) e del tipo di scopia . tion chamber providing simultaneous measurement of the dap and air kerma ( diamentor m4kdk , ptw , freiburg ) was used for the measurements . 
in addition to the transmission chamber measurements , for in vivo measurements , we determined the size of the beam area at the patient entrance using kodak x - omat v films [ 9 ]  . 
to evaluate the effective dose , we used the pcxmc programme ( stuk radiation and nuclear safety authority , helsinki , finland ) , which is based on the monte carlo method [ 10 ] and takes into account the age and actual size of the patient . results results of the assessments performed on the phantom are shown in figs . 
among fluoroscopy modes , it appears that pulsed fluoroscopy , indicated by two pulses on the operating console , is the technique that imparts the lowche minimizza la dose al paziente . 
la scopia pulsata 3 impulsi e quella continua presentano valori simili di dose , mentre la scopia 4 impulsi quella con i valori maggiori , da utilizzare quindi solo se giustificata dallesigenza di una qualit di immagine solo con essa ottenibile . 
le misure sono state effettuate in 3 condizioni con diaframmatura crescente : con diaframmi appena presenti sui bordi del campo , con diaframmi tali da formare un campo quadrato inscritto nellarea dellib e con diaframmi tali da creare un campo quadrato interno allarea ib . 
three - pulse and continuous fluoroscopy have similar dose values , whereas four - pulse fluoroscopy shows the highest values and should be used only when justified by a need for excellent image quality . 
measurements were performed in three conditions with increasing limitation of the field : with diaphragms present at the edges of the field only , with diaphragms forming a square field inscribed in the image intensifier area and with diaphragms forming a square field within the image intensifier area . 
entrance dose was found to be virtually independent of diaphragm size , whereas effective dose decreased significantly as diaphragm gresso risulta praticamente indipendente dalla diaframmatura , mentre la dose efficace si riduce considerevolmente allaumentare della diaframmatura . 
i risultati delle misure dosimetriche in vivo ottenuti nelle tre procedure seguite sono quelli mostrati nella tabella 1 . discussione dai risultati ottenuti emerge che per il tipo di procedura qui analizzato non sussistono particolari problemi di ordine radioprotezionistico anche per pazienti pediatrici . 
infatti i ratei di dose misurati in condizioni di esposizione standard ( < 1 msv / min per la dose efficace , ordine di grandezza di 10 mgy / min per la dose dingresso superficiale ) , tenendo conto che i tempi di esposizione tipici sono di pochi minuti , portano a valori di dose al paziente pienamente accettabili . 
the results of the in vivo dosimetric measurements obtained during three procedures are shown in table 1 . discussion our results indicate that the kind of procedure considered does not pose particular radiation protection problems , even if performed on children . 
the dose rates measured under standard exposure conditions ( < 1 msv / min for the effective dose , in the order of 10 mgy / min for the esd ) , if we consider typical exposure times of only a few minutes , imply perfectly acceptable patient dose values . 
typical exposure times refer to technically optimal procedures , with no complications arising during any phase of the procedure ( percutaneous puncture of bile ducts , crossing of biliary stenoses , bilioplasty and embolisation of the percutaneous tract ) and consequently no need to prolong fluoroscopy time . as for esd , comparison with the threshold values for skin injury indicated by the international commission of radiation protection ( icrp ) [ 11 ] shows that to reach skin doses likely to cause skin injury , exposure time should be at least one order of magnitude higher than is typical for the procedure . 
even under the worst possible exposure conditions , the first threshold value of 2 , 000 mgy is attained only with a fluoroscopy time of 135 mthe choice of optimal exposure parameters must therefore be chiefly aimed at minimising the effective dose . 
operatively , it is advisable to complicanza nelle varie fasi intra - , perie post - procedurali ( puntura percutanea dei dotti biliari , superamento delle stenosi biliari , bilioplastica ed embolizzazione del tramite percutaneo ) e che quindi non abbia richiesto un allungamento dei tempi di scopia . per quanto riguarda la dose dingresso superficiale , una comparazione con i valori soglia indicati dallinternational commission of radiation protection ( icrp ) [ 11 ] in corrispondenza dei quali possibile linsorgenza di danni alla cute , mostra che per raggiungere valori di dose alla cute tali da rendere possibili la manifestazione di tali effetti , il tempo di esposizione dovrebbe essere di almeno un ordine di grandezza superiore a quello tipico della procedura . 
appare quindi evidente che anche riguardo ai rischi di tipo stocastico la metodica acradiol med ( 2008 ) 113 : 429438 use a small image intensifier ( maximum magnification ) , which allows both minimisation of the effective dose ( figs . 4 , 6 ) and the best image quality for the patients anatomical characteristics . the typical effective dose rate , again assuming typical exposure times , provides an estimate of the effective dose in the order of 1 msv , similar to the values found in radiodiagnostics . 
in vivo measurements confirmed estimates derived from measurements on the phantothe procedures in question show a maximum entrance dose of approximately 50 mgy , meaning that an exposure time 40 times greater than needed to reach the first threshold value of 2 , 000 mgy would be necessary . 
the likelihood of radiation - induced cancer can be quantified [ 12 ] as a factor of 0.013% / msv for boy and of 0.016% / msv for girls under 10 years of age . 
the effective dose for the two procedures is in the range of 0.91.5 msv ; hence , the likelihood of malignancy is in the order of a few hundred parts per million . conclusions in paediatric patients , transhepatic cholangiography followed by percutaneous drainage is the procedure of choice for diagnosing and treating biliary complications of olt , such as strictures , fistulae or intrahepatic lithiasis . 
exposure parameters have been established , for the equipment used and for this kind of procedure , that allow one to obtain the desired image quality with the lowest dose . 
per le procedure esaminate si ha infatti un valore massimo di dose in ingresso di circa 50 mgy , per cui occorrerebbe un tempo di esposizione maggiore di 40 volte rispetto a quello impiegato per arrivare al primo valore soglia di 2000 mgy . 
la probabilit di insorgenza di un tumore letale indotto quantificabile [ 12 ] in un fattore di 0 , 013% per msv per i maschi e di 0 , 016% per msv per le femmine , per soggetti con et inferiore a 10 anni . 
la dose efficace per le due procedure seguite compresa nellintervallo 0 , 91 , 5 msv , quindi la probabilit di insorgenza dellordine di alcune centinaia di parti per milione . conclusioni la colangiografia transepatica seguita dal drenaggio percutaneo rappresenta lintervento delezione nelle complicanze biliari dei pazienti pediatrici sottoposti ad olt sia dal punto di vista diagnostico sia dal punto di vista terapeutico nel trattamento di stenosi , fistole o litiasi intraepatica . 
sono stati stabiliti i parametri di esposizione che consentono di ottenere la qualit di immagine desiderata con la minima dose , per lapparecchiatura utilizzata e per questa tipologia di procedure . 
radiodiagnostica , azienda ospedaliera s.croce e carle , via coppino 26 , 12100 cuneo , italy 2istituto di genetica , universit degli studi di pavia 3unit operativa di gastroenterologia ed endoscopia digestiva , ospedale maggiore , l.go dossena 2 , 26013 crema , italy correspondence to : m . 
from december 2001 to february 2007 , we embolised 60 pavms in 35 procedures performed on 30 patients , all referred by the hht centre in crema and enrolled in a screening programme of hht families . 
tra il dicembre 2001 e il febbraio 2007 sono state embolizzate 60 mav , in 35 interventi su 30 pazienti , tutti giunti alla nostra osservazione dal centro italiano delle teleangiectasie emorragiche ereditarie ( hht ) di crema , reclutati in corso di uno screening programmato multidisciplinare sulle famiglie hht , previo inquadramento clinico , studio ecotomografico , ecocardiografico con mdc e tc - spirale . 
la nostra 396 radiol med ( 2008 ) 113 : 395413 keywords rendu - osler - weber disease hht pulmonary arterio - venous malformations embolisation esperienza in accordo con i dati in letteratura : basso tasso di complicanze , ottimi risultati dal punto di vista tecnico e clinico , risparmio del parenchima polmonare sano dalla resezione chirurgica . parole chiave malattia di rendu - osler - weber hht malformazione artero - venosa polmonare embolizzazione introduction introduzione hereditary haemorrhagic telangiectasia ( hht ) is also known as rendu - osler - weber disease for the names of the first authors who identified the clinical entity between the end of the nineteenth and the beginning of the twentieth centuries [ 13 ]  . 
the estimated prevalence of hht in the overall population is 1020 / 100 , 000 , with different distributions among the various races and ethnic groups [ 4 ]  . 
the incidence of pulmonary arteriovenous malformations ( pavms ) varies according to the specific genetic mutation : alterations of chromosomes 9 and 12 have been identified , but they are not pathognomonic for the disorder , showing different rates of penetrance . the classic the diagnosis of hht is straightforward if patients pretriad : epistaxis ( onset during sent with infancy / adolescence in 50% of cases ) , skin telangiectasia ( with older age of onset ) and a positive family history [ 5 ]  . additional significant findings are visceral vascular malformations , especially involving the lung , stomach , duodenum and liver [ 6 ]  . 
histologically , these consist of arteriovenous malformations ( avm ) , terminal vessel ectasia or dilated capillaries and venules , with substantially reduced wall thickness leading to wall fragility and tendency to rupture [ 7 ]  . 
has established consensus criteria to permit a clinical diagnosis ( curaao criteria , table 1 )  . the incidence of pavms ranges from 15% to 33% , with predominant localisation in the lower lobes . 
pulmonary lesions , however , deserve investigation , even when no symptoms are present . failure to exclude pulmonary fistulae in patients with hht involves a potentially unacceptable risk of hypoxia or paradoxical embolism . macroscopically , two types of pavm have been distinguished . 
the first type involves small peripheral arterioles and venules and leads to small telangiectasias , which tend to la teleangiectasia emorragica ereditaria ( hereditary hemorragic telangiectasia , hht ) anche nota come malattia di rendu - osler - weber ( dal nome dei primi autori che a cavallo tra xix e xx secolo ne identificarono il quadro clinico [ 13 ] )  . 
lincidenza delle malformazioni artero - venose ( mav ) varia a seconda della specifica mutazione genetica : sono state identificate alterazioni sui cromosomi 9 e 12 , che per non sono patognomoniche di malattia , con differenti percentuali di penetranza . la diagnosi di hht agevole in presenza della triade classica di presentazione della malattia : epistassi ( nel 50% dei casi insorta gi nellinfanzia / adolescenza ) , teleangiectasie cutanee ( ad insorgenza pi tardiva ) e anamnesi familiare positiva per ereditariet [ 5 ]  . 
reperti accessori , ma non per questo meno significativi , sono le malformazioni vascolari viscerali , specie a livello polmonare , gastrico , duodenale ed epatico [ 6 ]  . 
dal punto di vista istologico si tratta di malformazioni artero - venose ( mav ) , ectasie dei vasi terminali , ovvero dilatazioni di capillari e venule con assottigliamento notevole delle pareti , le quali diventano fragili e tendono facilmente alla rottura [ 7 ]  . 
criteri di consenso per porre diagnosi clinica ( criteri di curaao , tabella 1 )  . lincidenza di mav polmonari ( pulmonary artero - venous malformations , pavm ) variabile dal 15% al 33% , con principale localizzazione ai lobi inferiori . 
family history diagnosis of hht is : definite possible or suspected improbable spontaneous , recurrent nosebleeds multiple , at characteristic sites : lips mouth fingers nose such as gastrointestinal telangiectasia ( with or without bleeding ) pulmonary avm hepatic avm cerebral avm spinal avm first - degree relative with hht if three criteria are present if two criteria are present if fewer than two criteria are present all offspring of a patient with hereditary haemorrhagic telangiectasia ( hht ) are at risk of the disease , as it can manifest at an advanced age . 
storia familiare la diagnosi di hht : definita possibile o sospetta improbabile spontanea , sanguinamento nasale ricorrente multiple , in sedi caratteristiche : labbra cavit orale dita naso quali : teleangiectasie gastrointestinali ( con o senza sanguinamento ) mav polmonari mav epatiche mav cerebrali mav midollari primo grado di parentela con un paziente con hht secondo i suddetti criteri se sono presenti 3 criteri se sono presenti 2 criteri se sono presenti meno di due criteri macroscopicamente si distinguono due tipologie di pavm . 
nel primo tipo , esse interessano le piccole arteriole periferiche e le venule ; ne risultano piccole teleangiectasie , che per lo pi rimangono tali e che non causano alterazioni emodinamiche e funzionali del piccolo circolo . 
le aree teleangiectasiche , di regola multiple e numerosissime , appaiono come focolai di colorito rossastro , simili a petecchie , di regola pi larghi e pi numerosi nelle regioni sottopleuriche [ 10 ]  . 
ne conseguono iposaturazione arteriosa di ossigeno , cianosi , dispnea , iperglobulia , ippocratismo digitale , manifestazioni emorragiche ed emottisi . istologicamente , le fistole polmonari sono composte da spazi cavernosi ripieni di sangue , strettamente addossati tra loro ; la parete costituita da uno strato intimale ispessito su una sottile lamina elastica . 
la conferma definitiva della loro presenza pu essere ottenuta mediante tc multislice ( con mezzo di contrasto ) , che dimostra con chiarezza larchitettura dei vasi allinterno della malformazione ; inoltre possibile effettuare ricostruzioni volume rendering in caso di lesione complessa [ 11 , 12 ]  . 
lindagine tc significativamente pi sensibile nel rilievo di lesioni arterovenose polmonari rispetto alle procedure angiografiche ( 98% vs 60% ) [ 13 ]  . langiografia , metodica altamente invasiva , viene impiegata quando si prospetta un contemporaneo trattamento correttivo mediante embolizzazione [ 14 ]  . il trattamento delle pavm deve essere preso in considerazione per tutte quelle lesioni con arteria afferente di calibro superiore a 3 mlapproccio chirurgico [ 15 ] stato lunico trattamento possibile fino al 1978 , anno in cui taylor et al . 
oggi il trattamento di scelta lapproccio radiologico percutaneo mininvasivo . scopo del lavoro presentare i risultati dellesperienza del nostro centro nella chiusura percutanea delle fistole ad alto flusso mediante accesso mininvasivo . tutta la progenie di un individuo con hht a rischio di malattia , poich essa pu manifestarsi in tarda et . 
anomalie viscerali nei bambini dovrebbero spingere ad accurate indagini sugli altri componenti della famiglia . questi criteri saranno probabilmente ridefiniti quando , nei prossimi anni , diverrano disponibili studi di biologia molecolare . 
mav , malformazioni artero - venose materiali e metodi nel nostro servizio di radiologia interventistica dal dicembre 2001 al febbraio 2007 sono state eseguite 60 embolizzazioni percutanee di malformazioni artero - venose polmonari in 30 pazienti ( 14 maschi e 16 femmine ) di et compresa tra 398 radiol med ( 2008 ) 113 : 395413 remain small without producing haemodynamic or functional alterations to the pulmonary circulation . 
this leads to decreased arterial oxygen saturation , cyanosis , dyspnoea , polyglobulia , digital clubbing , haemorrhage and haemoptysis . histologically , pulmonary fistulae consist of tightly packed , cavernous , blood - filled spaces ; the walls of which consist of a thickened intimal layer over a thin elastic lamina . 
angiography is a highly invasive technique and is therefore only used in the case of simultaneous embolisation [ 14 ]  . pavm treatment should be considered in all lesions with a feeding artery > 3 mm in diameter . 
today , the treatment of choice is a minimally invasive percutaneous interventional radiology procedure . the aim of this paper is to present the results of our experience with minimally invasive percutaneous embolisation of high - flow fistulae . materials and methods from december 2001 to february 2007 , our interventional radiology department performed 60 percutaneous embolisation procedures on pavm in 30 patients ( 14 men and 16 women ) , with age ranging from 19 to 75 [ meanstandard deviation ( sd ) 47.813.3 , median 50 ] years , for a total of 35 sessions ( table 2 )  . 
patients with pavm were identified by the centre for the diagnosis and surveillance of hereditary haemorrhagic telangiectasia in crema , italy on the basis of the protocol for family hht screening ; genetic diagnoses were performed by the institute of genetics in pavia , italy . twenty - one sessions involved the treatment of a single 19 e 75 anni ( et mediadeviazione standard , 47 , 813 , 3 anni , et mediana 50 anni ) in un totale di 35 sedute ( tabella 2 )  . 
i pazienti con pavm sono stati identificati dal centro per la diagnosi e la sorveglianza di teleangiectasia emorragica ereditaria di crema , sulla base del protocollo di screening famigliare per la hht ; la diagnosi genetica stata effettuata dallistituto di genetica di pavia . ventuno sedute hanno riguardato il trattamento di una sola lesione . 
vi infine stato il caso eccezionale di sette lesioni trattate nella stessa seduta ( 3 a destra , 4 a sinistra ) in una paziente di 41 anni gi nota e trattata in precedenza . 
a proposito della distribuzione familiare della hht ( almeno 16 pazienti su 30 hanno segnalato almeno un familiare affetto da malattia ) , due pazienti trattate sono tra loro sorelle e due sono tra loro fratelli . dallanamnesi possiamo rilevare che lepistassi il sintomo che si presenta nella maggior parte dei nostri pazienti ( 21 / 30 , 70 , 0% ) , mentre le teleangiectasie , la dispnea da sforzo e lemoftoe sono presenti in varie combinazioni in tutti i casi . 
gli esami ematochimici sono risultati nella norma in 21 pazienti su 30 ( 70 , 0% ) , mentre in 7 casi ( 23 , 3% ) emerso un quadro di anemia . 
tutti i pazienti , preventivamente informati sulla procedura , devono accordare il proprio consenso al trattamento . lintervento di embolizzazione viene eseguito in sala angiografica , dove disponibile un angiografo digitale di ultima generazione che rende possibile il road mapping , che facilita il cateterismo superselettivo delle arterie . 
lembolizzazione della fistola viene effettuata occludendo larteriola afferente alla pavm stessa ; non viene pertanto eseguito il cateterismo selettivo della sacca aneurismatica , ma solo dellarteria afferente , in quanto unocclusione della sacca avrebbe un maggiore rischio di migrazione delle spirali nella vena polmonare quindi nel circolo sistemico . 
one case involved the treatment of seven lesions during the same session ( three on the right , four on the left ) in a 41 - year - old patient who had been treated previously . 
overall , four cases were treated over different sessions to complete previous embolisation procedures and / or treat additional lesions . with regard to familiarity for hht ( 16 / 30 patients reported at least one family member with the disease ) , two patients treated were sisters and two were brothers . our patients medical history showed that epistaxis was the most common symptom ( 21 / 30 , 70.0% ) , and telangiectasia , dyspnoea on exertion and blood - tinged sputum were present in different combinations in all cases . 
embolisation is performed by occluding the feeding arteriole , so that selective catheterisation is only performed on the feeding artery and not on the aneurysmal sac , since sac occlusion would involve a greater risk of coil migration towards the pulmonary vein and into the systemic circulation . 
the study is completed by right and left pulmonary artery imaging with anteroposterior , oblique and lateral projections , if needed . during the procedure , immediately before performing the embolisation , 2 , 500 iu of heparin is administered to prevent clot formation and the risk of cerebral embolisation . preanaesthesia is normally achieved with promethazine and atropine . 
antibiotic prophylaxis is then administered to prevent the risk of cerebral abscess in the case of paradoxical embolism . once the supplying artery is identified , a 6 - f , 65 - cm - long introducer , used as a vector catheter , is positioned in the gnostico mediante catetere posizionato nel tronco dellarteria polmonare ; lo studio viene successivamente completato dallimaging delle arterie polmonari destra e sinistra , con eventuali proiezioni antero - posteriore , obliqua e laterale . durante la procedura , immediatamente prima di eseguire lembolizzazione si somministrano 2500 ui di eparina , per evitare la formazione di coaguli ed il possibile rischio di embolizzazione al distretto cerebrale . 
si procede poi ad una profilassi antibiotica , per prevenire il rischio di ascessi cerebrali in caso di embolia paradossa . una volta evidenziate le arterie alimentanti la mav da embolizzare , si procede al posizionamento di un introduttore 6 f lungo 65 cm nel tronco dellarteria polmonare ( o , pi selettivamente , nellarteria polmonare del lato da trattare ) , utilizzato come catetere vettore . 
i palloncini staccabili sono stati usati precedentemente , ma risultano di pi complessa introduzione , sono gravati da un maggior costo e presentano possibili svantaggi legati a una precoce desufflazione del pallone stesso . 
d il controllo finale dimostra la completa esclusione dal circolo della lesione . pulmonary artery ( or , more selectively , in the pulmonary artery on the side to be treated )  . 
in especially large fistulae , longer coils are used , such risultati in tutti i casi stato ottenuto un successo tecnico immediato con esclusione delle malformazioni e conseguente incremento dei valori della pressione parziale arteriosa di ossigeno . 
a seguito delle procedure di embolizzazione si rileva un notevole miglioramento dellossigenazione , in quei pazienti con diminuzione della pao2 ( che passa da una media del 93% al 97% ) ; nei pazienti con sintomatologia ipossica in particolar modo dopo sforzo si rileva la pressoch totale risoluzione dei sintomi . 
in some cases , more than one artery is involved in pavm vascularisation , making it necspirali per parziale ricanalizzazione di mav precedentemente embolizzate , con risultato definitivo . al termine di una procedura , si verificata unischemia cerebrale transitoria con modesta afasia , risoltasi in 72 ore , in un paziente con voluminosa mav , con vasi arteriosi afferenti ectasici . 
inoltre , soprattutto nei casi di mav complesse , alimentate da pi di un vaso arterioso , si pu verificare a distanza di tempo un ulteriore apporto ematico noradiol med ( 2008 ) 113 : 395413 results immediate technical success , with complete exclusion of malformations and resulting increase in partial pressure of arterial oxygen , was achieved in all cases . 
after embolisation , a marked improvement in oxygenation was seen in patients with decreased pao2 ( from 93% to 97% on average )  . in patients with hypoxia mostly on exertion the symptoms resolved completely . 
two patients required further coil embolisation owing to partial recanalisation of previously treated avms , with definitive resolution . after one procedure , transient cerebral ischaemia with moderate aphasia , which resolved in 72 h , was observed in a patient with a large avm with dilated feeding arteries . 
at present , surgical resection of avm is indicated in patients after failed percutaneous embolisation and in those with severe bleeding despite embolisation , with intrapleural avm rupture , with major allergies to contrast media or with lesions that cannot be treated percutaneously [ 17 ]  . 
the risks of avm surgery are comparable with those of any other chest operation , although mortality and morbidity rates are minimal in well - selected patients [ 18 ]  . 
surgery becomes the treatment of choice when percutaneous treatment is not possible [ 19 , 20 ]  . percutaneous treatment is performed using metal coils , detachable balloons or endovascular plugs [ 2124 ]  . 
both techniques involve selective catheterisation of the feeding artery , superselective angiography , positioning of the catheter tip near the avm neck and release of the occlusive device at this site [ 25 , 26 ]  . nostante le spirali gi posizionate , con necessit di un nuovo accesso percutaneo per ulteriore procedura di embolizzazione . 
attualmente la resezione chirurgica delle mav indicata nei pazienti in cui il trattamento percutaneo mediante embolizzazione fallito , in pazienti con severe complicanze emorragiche nonostante lembolizzazione , con rottura intrapleurica della mav , con allergia importante al contrasto o con lesioni non trattabili per via percutanea [ 17 ]  . 
le possibilit chirurgiche sono lescissione locale , la resezione di un segmento , la lobectomia , la legatura del vaso arterioso afferente ed eventualmente la pneumonectomia . la resezione locale e la segmentectomia sono le procedure di scelta quando possibile . 
il rischio chirurgico di un intervento per mav paragonabile a quello di un altro intervento chirurgico toracico , ma praticamente minimo per quanto riguarda la mortalit e la morbilit se i pazienti sono ben selezionati [ 18 ]  . 
entrambe le tecniche prevedono la cateterizzazione selettiva dellarteria afferente , lo studio angiografico superselettivo , il posizionamento dellestremit distale del catetere prossimalmente al colletto della mav ed infine il rilascio del device occlusivo in tale sede [ 25 , 26 ]  . 
 per ridurre il rischio di possibili migrazioni distali delle spirali , stato proposto lutilizzo di spirali a rilascio controllato , di derivazione neuroradiologica , ma lelevato costo non ne giustifica un suo routinario impiego . 
in alternativa , per ridurre tale rischio , si impiega la tecnica secondo white , che prevede lutilizzo di spirali lunghe ( oltre 14 cm ) con iniziale posizionamento in un ramo collaterale per ottenere un buon ancoraggio e successivo rilascio nel ramo afferente . 
fibre sintetiche ( dacron ) si dipartono dal core metallico e facilitano lembolizzazione . un device pi recente per lembolizzazione lamplatzer vascular plug : si tratta di un device metallico cilindrico autoespandibile in nitinolo che pu essere ritirato in caso di incorretto posizionamento e che offre buone garanzie di stabilit e durata nel tempo . 
lutilizzo di tale dispositivo utile in presenza di grosse arterie afferenti in quanto esclude il 408 radiol med ( 2008 ) 113 : 395413 to minimise the risk of distal coil migration , it has been suggested to use the controlled - release coils normally used in neuroradiology , but the high cost does not justify their routine use . 
alternatively , the risk can be reduced by using the technique first proposed by white , involving the use of long coils ( > 14 cm ) to be initially positioned in a collateral branch for optimal anchoring and later released into the feeding vessel . 
the coil model used in our series was first suggested by white and consist of metal strands > 14 cm long , which , once released from the guide , assume a helical shape with variable pitch and diameter . 
this device is useful in the presence of large feeding arteries in that it rischio di migrazione delle spirali dalla sacca con possibile embolia sistemica e consente di occludere con un solo dispositivo voluminose mav che richiederebbero limpiego di molte spirali . 
nella nostra casistica , in accordo con la letteratura , abbiamo dimostrato che lembolizzazione con spirali associata a una bassa morbilit e che garantisce un buon risultato a medio - lungo termine ( tabella 3 ) [ 2729 ]  . 
 lindicazione al trattamento delle mav era stata proposta in origine in quei casi in cui larteria afferente ha un diametro di almeno 3 mm ; recentemente si ritiene peraltro indicato il trattamento di tutte le mav tecnicamente embolizzabili in presenza di positivit allecocardiogramma con mezzo di contrasto , in cui evidente uno shunt destro - sinistro . 
e , f controllo tc dopo il trattamento che dimostra un buon risultato . 410 radiol med ( 2008 ) 113 : 395413 eliminates the risk of coil migration from the sac with possible systemic embolism and allows occlusion with a single device of large avms that would otherwise require several coils . 
in agreement with the literature , our experience demonstrated that coil embolisation is associated with low morbidity and has good midto long - term results ( table 3 ) [ 2729 ]  . treatment of avms was originally indicated in the case of feeding arteries > 3 mm in diameter ; however , recently , treatment is indicated in all technically embolisable avms in the presence of positive contrast - enhanced echocardiogram showing right - to - left shunting . 
it is important to preserve those vessels originating from the feeding arteriole that are not visualised on preembolisation angiography because of the shunt ; this makes it possible to preserve the oxygen capacity of the lung portion involved . 
however , this entails a marked increase in the cost of materials and in treatment complexity . in addition , the incidence of paradoxical embolism due to implanted material is low , especially in centres with a high level of experience with the embolisation procedures . 
the only known contraindications include the rare cases ( approximately 1% ) in which the feeding artery is too short ( 2 cm or less ) and has a high flow or an irregular diameter [ 31 ]  . minor complications occurred in 14% of patients , which included chest pain and self - limiting pleurisy , with a 10%15% frequency . 
importante preservare quei vasi originanti dallarteriola afferente che non vengono visualizzati allesame angiografico precedente lembolizzazione a causa dello shunt ; in tal modo possibile conservare la capacit di ossigenazione della porzione di polmone interessata . 
sebbene non sia clinicamente importante preservare la perviet di tali vasi in pazienti portatori di una o due lesioni , invece rilevante in quei soggetti con un numero maggiore di shunts oppure in presenza di patologie polmonari concomitanti . 
locclusione distale riduce con ogni probabilit la perfusione del sacco venoso che proviene da anastomosi bronco - polmonari fisiologiche . attualmente in dibattito la necessit o meno di procedere , oltre allembolizzazione arteriosa , al completo riempimento della sacca aneurismatica . 
le sole controindicazioni in letteratura si limitano a rari casi ( circa l1% ) in cui larteria afferente sia troppo breve ( 2 cm o meno ) ed abbia un alto flusso o un diametro irregolare [ 31 ]  . nella nostra casistica , sono state riportate complicanze minori nel 14% dei pazienti , in cui sono inclusi dolore toracico e pleuriti autolimitanti con una frequenza del 10%15% . 
the event occurred due to microembolisation caused by clots in a patient with a large avm who was not preventively treated with hepar since then , all patients receive anticoagulation therapy during the embolisation procedure . the use of detachable balloons has been abandoned due to unsatisfactory midterm outcomes . 
in particular , a study conducted by peuster reported that during a 3 - year follow - up , coil radiopacity decreased in 9 / 13 patients , and in five studied by angiography , recanalisation of treated arteriovenous fistulae occurred [ 34 ]  . 
this occurrence was also seen in our series in a patient who had previously undergone tungstencoil embolisation at another hospital and was later treated in our department following partial avm recanalisation . it is important that follow - up be performed by ct scans to evaluate both the correct positioning of the device and possible avm recanalisation [ 35 ]  . 
in two cases only did we observe partial recanalisation of some of the lesions , which were subsequently embolised with a second angiographic procedure . in cases of multiple and complex avms , if the procedure takes longer than 3 h , it is preferable to intervene on the largest lesions and reschedule embolisation of other lesions to further sessions . 
available data allow us to state that the dose delivered during the treatment was always 1 gy and therefore below the levels indicated by the international commission of radiological protection [ 36 ]  . croembolizzazione da coaguli in presenza di voluminosa mav e in cui non era stata effettuata la terapia eparinica preventiva . 
da allora a tutti i pazienti viene somministrata terapia anticoagulante durante la procedura di embolizzazione . sono ormai stati abbandonati i palloncini staccabili , con risultati a medio termine poco soddisfacenti . 
dalla letteratura degli ultimi anni si evince che i limiti principali di tali dispositivi sono i costi elevati e la tendenza alla desufflazione nellarco di 24 anni [ 32 ]  . 
inoltre una delle pazienti della nostra casistica aveva effettuato precedenti embolizzazioni con spirali in tungsteno , con risultati insoddisfacenti . lo studio sulla biocompatibilit delle spirali in tungsteno ha evidenziato la presenza di elevati livelli di tale metallo nel sangue , nei capelli e nelle urine dei pazienti rilasciati nel corso dei mesi successivi al trattamento [ 33 ]  . 
in particolare , in uno studio condotto da puester stato rilevato che , in un follow - up di tre anni , la radiopacit delle spirali era diminuita in 9 pazienti su 13 e in 5 di essi , sottoposti ad angiografia , si era verificata ricanalizzazione delle fistole artero - venose sottoposte a trattamento [ 34 ]  . 
tale fenomeno si verificato anche in un paziente , precedentemente sottoposto ad embolizzazione con spirali in tungsteno presso altra sede , con parziale rifornimento della mav successivamente ritrattata da noi . fondamentale che il follow - up venga effettuato mediante controlli tc per valutare sia il corretto posizionamento del dispositivo , sia leventuale ricanalizzazione della mav [ 35 ]  . 
un nuovo accesso in sala angiografica ha consentito la loro embolizzazione definitiva . in caso di mav multiple e complesse , se la procedura si protrae oltre le 3 ore di intervento , preferibile intervenire su quelle di maggiori dimensioni e differire lembolizzazione delle altre lesioni a sedute successive . 
dai dati a nostra disposizione possiamo dire che la dose erogata durante il trattamento sempre inferiore o uguale a 1 gy quindi ampiamente nei limiti stabiliti dallicrp [ 36 ]  . conclusions conclusioni metal - coil percutaneous embolisation is the treatment of choice in pavms occurring in the presence of renduosler - weber disease , as it allows selective occlusion with pulmonary parenchyma preservation [ 3739 ]  . 
treatment is indicated in all fistulae with a feeding artery > 3 mm in diameter or in the presence of evident right - to - left shunts . nonmagnetic metal coils , in particular vortex coils ( vortx , boston scientific ) , represent , in our opinion , the most suitable devices owing to ease of use and certainty of achieving lembolizzazione percutanea con spirali metalliche il trattamento di scelta delle pavm nella malattia di renduosler - weber , poich consente unocclusione selettiva e risparmio del parenchima polmonare [ 3739 ]  . 
the angiographic procedure permits a minimally invasive approach with a low complication rate and effective reduction in right - to - left shunting with improved arterial oxygenation . acknowledgements the authors thank their colleagues at the hht - net ( network of centres for the treatment of hereditary haemorrhagic telangiectasia ) for their cooperation : g . 
boccardi10 1uo gastroenterologia ed endoscopia digestiva ospedale maggiore , crema , italy 2uo cardiologia , ospedale maggiore , crema , italy 3 uo otorinolaringoiatria , ospedale maggiore , crema , italy 4uo radiologia , ospedale maggiore , crema , italy 5istituto di genetica medica , universit di pavia , pavia , italy 6uo otorinolaringoiatria , fondazione policlinico s matteo , pavia , italy 7istituto di radiologia , fondazione policlinico s matteo , pavia , italy 8istituto di cardiologia , fondazione policlinico s matteo , pavia , italy 9dipartimento di cardiologia , istituto g . 
la procedura angiografica consente un approccio mini - invasivo , con una bassa incidenza di complicanze e uneffettiva riduzione dello shunt destro - sinistro e conseguente miglioramento dellossigenazione arteriosa . ringraziamenti gli autori sono grati , per la fattiva collaborazione , ai colleghi dellhht - net ( rete di centri per la teleangiectasia emorragica ereditaria ) g . 
boccardi10 1uo gastroenterologia ed endoscopia digestiva ospedale maggiore , crema 2uo cardiologia , ospedale maggiore , crema 3uo otorinolaringoiatria , ospedale maggiore , crema 4uo radiologia , ospedale maggiore , crema 5istituto di genetica medica , universit di pavia 6uo otorinolaringoiatria , fondazione policlinico s matteo , pavia 7istituto di radiologia , fondazione policlinico s matteo , pavia 8istituto di cardiologia , fondazione policlinico s matteo pavia 9dipartimento di cardiologia , istituto g . 
this paper describes the magnetic resonance imaging ( mri ) and magnetic resonance cholangiopancreatography ( mrcp ) pattern of multifocal intraductal papillary mucinous tumours ( ipmt ) of the pancreatic side branches and its evolution during followmaterials and methods . 
inclusion criteria were ( cid : 2 ) 2 ectasic side branches , presence of communication with the main pancreatic duct , and ( cid : 2 ) 2 mri / mrcp examinations after ( cid : 2 ) 612 months . 
exclusion criteria were ipmt involving both the main pancreatic duct and its branch ducts , previous surgery and lack of follow - up mri examinations . median follow - up was 27 ( range 659 ) months . 
qualitative assessment considered : the number of cystic lesions of the branch ducts , morphology of the communication between the cystic lesion and the main duct ( direct or neck ) , presence of intraluminal filling defects within the cystic lesions , presence of mural nodules and mural enhancement of the cystic lesion . 
criteri di inclusione : ( cid : 2 ) 2 dotti ii ectasici , presenza di comunicazione con il dotto pancreatico principale ( dpp ) , ( cid : 2 ) 2 rm / cprm a distanza ( cid : 2 ) 612 mesi . criteri di esclusione : tipm coinvolgenti sia il dpp che i dotti ii , pregressa chirurgia , assenza di controllo rm . mediana del monitoraggio : 27 mesi ( range 659 mesi )  . analisi qualitativa : numero delle dilatazioni cistiche dei dotti ii , morfologia della comunicazione tra ectasie dei dotti ii e dpp ( diretta / colletto ) , presenza di difetti di riempimento endoluminali delle dilatazioni dei dotti ii , presenza di noduli parietali , impregnazione di contrasto parietale delle dilatazioni cistiche dei dotti ii . 
the mean diameter of the cystic lesions was 18.8 mthe mean length of the communication neck was 6.9 mat follow - up , the mean number of cystic lesions of the side branches was 8.4. 
intraluminal filling defects in the side branches were detected in 7 / 26 patients ( 27% ) ; mural nodules were seen in 2 / 26 patients ( 8% )  . 
in our series , only 2 / 26 patients showed mural nodules . keywords pancreas pancreatic neoplasm intraductal papillary mucinous tumours mr imaging il diametro medio delle dilatazioni cistiche dei dotti ii era di 18 , 8 mla lunghezza media dei colletti di comunicazione era 6 , 9 mcontrollo . 
difetti endoluminali erano presenti in 7 / 26 pz ( 27% ) ; noduli parietali in 2 / 26 pz ( 8% ) ; ed in 2 / 26 ( 8% ) era presente impregnazione di contrasto parietale . 
solo 2 / 26 pz ( 8% ) hanno dimostrato noduli parietali . parole chiave pancreas neoplasie pancreatiche tumori intraduttali papillari mucino - secernenti risonanza magnetica introduction introduzione intraductal papillary mucinous tumours ( ipmt ) are cystic neoplasms arising from the epithelial lining of the pancreatic ductal system [ 1 ]  . 
the malignancy rate of central ipmt is 60%92% [ 3 , 6 ] , whereas that of peripheral ipmt is 6%40% [ 7 , 8 ] , as demonstrated by histopathological studies . 
their different biological behaviour translates into different treatment approaches , with central ipmt being candidates for surgical treatment and peripheral ipmt for close monitoring over time . peripheral ipmt may manifest either as a single lesion or as multiple lesions scattered throughout the entire pancreas . in the latter case , they are defined as multifocal peripheral ipmt [ 912 ]  . 
sono classificati in centrali e periferici [ 2 ] in base alla loro localizzazione lungo il sistema duttale [ 35 ] : i primi si sviluppano nel dotto pancreatico principale ( dpp ) , i secondi , invece , in un dotto secondario . limportanza di tale suddivisione dovuta al fatto che il comportamento biologico di tali tumori differente : i tipm centrali sono maligni nel 60%92% [ 3 , 6 ] dei casi , mentre i tipm periferici nel 6%40% [ 7 , 8 ] dei casi , come risulta da studi anatomo - patologici . 
the aim of this paper is to describe the mri and mrcp patterns of multifocal peripheral ipmt and their evolution over time . cogliere leventuale comparsa di segni indicativi di degenerazione ( aumento del diametro delle lesioni , comparsa di vegetazioni parietali , ed impregnazione di contrasto ) [ 10 , 1416 ]  . 
la risonanza magnetica ( rm ) rappresenta la metodica di elezione nello studio di queste neoplasie , per la sua capacit di studiare simultaneamente il parenchima ed il sistema duttale pancreatico , mediante la colangiopancreatografia con rm ( cprm ) [ 10 , 1517 ]  . 
scopo di questo lavoro quello di descrivere le caratteristiche rm e di cprm dei tipm periferici multifocali e la loro evoluzione nel tempo . materials and methods patient population from january 2001 to december 2006 , 89 patients with a diagnosis of multifocal ipmt of the pancreatic branch ducts examined by mri and mrcp were enrolled in this retrospective study . 
inclusion criteria were presence of two or more branch duct dilatations in any pancreatic segment ( head ; body - tail ) , presence of a communication between at least two lesions and the main pancreatic duct and two or more follow - up mri / mrcp examinations at least 6 months after the diagnosis . 
exclusion criteria included lesions involving both the branch ducts and the main pancreatic duct ( combined - type ipmt ) ( n = 19 ) , previous pancreatic surgery ( n = 1 ) , follow - up mri / mrcp performed at another centre or follow - up with computed tomography ( ct ) ( n = 43 )  . the final population was composed of 26 patients ( ten men , 16 women ) with a mean age of 67 ( range 2979 ) years . 
at the time of observation , all patients were asymptomatic with regard to pancreatic lesions . after the initial diagnosis , all patients underwent followup with mri / mrcp at 6 - monthly or yearly intervals for a total of 29 months ( median 27 , range 659 months ) and a mean number of examinations of 3.19 ( range 27 )  . 
confirmation of the diagnosis of multifocal peripheral ipmt was obtained at follow - up mri / mrcp performed at least 6 months after the diagnosis ( table 1 )  . mri / mrcp technique and protocol mri examinations were carried out with 1.5 - tesla equipment ( magnetom symphony , siemens , erlangen , germany ) with a four - channel coil positioned on the patients upper abdomen . 
in addition , they received 50150 ml of oral superparamagnetic contrast material ( lumirem , guerbet , paris , france ) or pineapple juice 1020 min before the examinamateriali e metodi popolazione di pazienti dal gennaio 2001 al dicembre 2006 , 89 pazienti con diagnosi di tipm multifocale dei soli dotti collaterali e sottoposti ad esame di risonanza magnetica e di colangiopancreatografia con rm ( rm / cprm ) , sono stati considerati per linclusione in questo studio retrospettivo . 
i criteri di inclusione dello studio comprendevano : presenza di due o pi ectasie dei dotti di secondo ordine , indipendentemente dalla loro sede ( testa ; corpo - coda ) ; presenza di comunicazione tra almeno due lesioni ed il dotto pancreatico principale ; due o pi esami rm / cprm a distanza di almeno sei mesi . sono stati esclusi dallo studio i pazienti con lesioni coinvolgenti sia i dotti secondari che il dotto pancreatico principale ( dpp ) ( tipm misti ) ( n = 19 ) ; pazienti gi sottoposti ad interventi di resezione chirurgica pancreatica ( n = 1 ) ; e pazienti senza esami rm / cprm di controllo eseguiti presso il nostro istituto , o pazienti sottoposti a monitoraggio mediante tomografia computerizzata ( tc ) ( n = 43 )  . la popolazione considerata quindi di 26 pazienti ( 10 maschi ; 16 femmine ) con unet media di 67 anni ( range 2979 anni )  . 
al momento dellosservazione tutti i pazienti erano asintomatici per lesioni pancreatiche . dal momento della diagnosi , tutti i pazienti sono stati sottoposti a controlli periodici con rm / cprm , a cadenza semestrale o annuale , per una media di 29 mesi ( mediana 27 ; range 659 mesi ) , con un numero di indagini medio di 3 , 19 ( range 27 )  . 
la conferma del quadro rm / cprm negli esami di controllo , eseguito ( cid : 2 ) 6 mesi , ha confermato la diagnosi di tipm periferico multifocale ( tabella 1 )  . tecnica e protocollo rm / cprm le indagini di rm sono state eseguite su unapparecchiaturadiol med ( 2008 ) 113 : 414428 table 1 multifocal intraductal papillary mucinous tumours ( ipmt ) of the sided branches : number and frequency of magnetic resonance imaging / magnetic resonance cholangiopancreatography ( mri / mrcp ) examinations tabella 1 tumori intraduttali papillari mucino - secernenti ( tipm ) multifocali dei dotti secondari : numero e frequenza delle indagini di rm / cprm length of follow - up ( months ) no . 
of mri / mrcp examinations interval of follow - up ( months ) durata del controllo ( mesi ) n indagini rm / cprm cadenza del controllo ( mesi ) patient number mean median numero pazienti media mediana tion to eliminate the signal from gastroduodenal fluid in t2 - weighted sequences . 
no medication was given to reduce bowel peristalsis . the mri protocol involved the use of t1 - weighted gradient echo ( gre ) sequences with in - phase and out - of - phase echo time ( te ) , with the following parameters : repetition time ( tr ) / te 107160 / 2.44.8 ms , flip angle 7080 , slice thickness 7 mm with a 10% gap . 
axial t2 - weighted rapid acquisition relaxation enhancement ( rare ) sequences were obtained with a tr / te 4 , 950 / 102 ms and a slice thickness of 7 mm with a 5%10% gap . 
subsequently , t1weighted fat - suppressed gre sequences centred on the pancreatic parenchyma were acquired with the following parameters : tr / te 107 / 4.8 ms , flip angle 7585 , slice thickness 56 mm with a 10% gap . 
t2 - weighted half - fourier single - shot turbo spin - echo ( haste ) sequences were obtained with the following parameters : tr / te ( cid : 3 ) / 60102 ms , echo train length 128 , slice thickness 4 mm without gap . 
this sequence was performed in the axial , sagittal , coronal and paracoronal planes at different angles ( from 3 to 10 ; mean : 6 ) relative to the long axis of the pancreas to optimise visura con magnete da 1 , 5 tesla ( magnetom symphony , siemens , erlangen , germania ) , con bobina multicanale ( 4 canali ) posta sulladdome superiore . 
a tutti i pazienti stato richiesto il digiuno ( 46 ore ) prima dellesecuzione dellesame ; inoltre sono stati somministrati 50150 ml di mdc superparamagnetico ( lumirem , guerbet , parigi , francia ) o in alternativa succo di ananas , per os , 1020 minuti prima dellesame , al fine di annullare lintensit di segnale del fluido gastroduodenale nelle sequenze t2dipendenti . 
non stato somministrato alcun farmaco per ridurre la peristalsi intestinale . il protocollo rm utilizzato prevede limpiego di sequenze gradient eco ( gre ) t1 - dipendenti con te in fase e fuori fase , con i seguenti parametri tempo di ripetizione ( tr ) / tempo di eco ( te ) 107160 / 2 , 44 , 8 , angolo di deflessione : 7080 ; spessore della scansione 7 mm , con intervallo del 10% . 
sono state anche acquisite immagini assiali t2 - dipendenti rapid acquisition with relaxation enhancement ( rare ) con un tr / te 4950 / 102 , con spessore di scansione di 7 mm , con intervallo 5%10% . 
successivamente sono state ottenute sequenze in eco di gradiente t1 - dipen418 radiol med ( 2008 ) 113 : 414428 alisation of the pancreatic ductal system . the mrcp protocol used the haste sequence with tr / te ( cid : 3 ) / 1 , 100 ms , slice thickness 4080 mm to cover the entire biliary tree and pancreatic ductal system , including both papillae . 
the dynamic study was performed during administration of 0.1 mmol / kg body weight of gadolinium chelates ( multihance , bracco , milan , italy ) with a fourphase technique : precontrast , pancreatic phase ( 3545 s ) , portal venous phase ( 8590 s ) and delayed phase ( > 180 s )  . the dynamic study used a t1 - weighted 3d gre volumetric interpolated breath - hold examination ( vibe ) sequence with chemically selective fat saturation in the axial plane . 
presence of mural nodules ( defined as any papillary growth or protrusion within the single cystic lesion , provided it was not in a gravity - dependent position ) 5 . 
presence of malformations or anatomical variants of the pancreatic ductal system ; presence of signs suggestive of malignancy , including secondary liver lesions , ascites , enlarged lymph nodes , peritoneal deposits , and vessel invasion quantitative analysis was carried out by a third observer not involved in the qualitative analysis ( sm , with 4 years of experience ) and took into account the following : 1 . 
length of the communicating neck , if present , connectdenti con saturazione del grasso , centrate sul parenchima pancreatico , con i seguenti parametri : tr / te 107 / 4 , 8 ms , angolo di deflessione 7585 , spessore della scansione 56 mm , intervallo 10% . 
immagini half fourier single - shot turbo spin - echo ( haste ) t2 - dipendenti sono state acquisite con i seguenti parametri : tr / te : ( cid : 3 ) / 60102 ; treni di echi 128 ; spessore della scansione 4 mm senza intervallo . tale sequenza stata condotta nei piani assiale , sagittale , coronale e para - coronale secondo diverse angolazioni ( da 3 a 10 acquisizioni ; media : 6 ) , rispetto allasse maggiore del pancreas al fine di ottimizzare la visualizzazione del sistema duttale pancreatico . lo studio cprm utilizzato si avvale dellimpiego della sequenza , half - fourier single - shot turbo spin - echo ( haste ) con tr / te ( cid : 3 ) / 1100 ms , con spessore di strato di 4080 mm , comprendendo nello spessore della scansione tutto lalbero biliare ed il sistema duttale pancreatico , comprese ambedue le papille . 
lo studio dinamico stato ottenuto durante la somministrazione di 0 , 1 mmol / kg di peso corporeo di chelati del gadolinio ( multihance , bracco , milano , italia ) , con tecnica quadrifasica : pre - contrasto , fase pancreatica ( 3545 s ) , venosa portale ( 8590 s ) , e tardiva ( > 180 s )  . 
lo studio dinamico stato eseguito mediante sequenze in eco di gradiente , t1 - dipendenti , volumetriche , con saturazione del grasso chimicamente selettiva volume interpolated breathold examination ( vibe ) lungo il piano assiale . 
i parametri impiegati sono stati : tr / te 4 , 5 / 1 , 7 ms , spessore della scansione 2 , 63 mm , matrice 235256512 . lanalisi delle immagini stata eseguita da due osservatori ( rm , rg ) ( > 15 anni di esperienza ) che hanno valutato tutte le indagini rm / cprm della diagnosi , in maniera indipendente , sia su film ( 8 esami ) che alla consolle ( 18 esami )  . 
le immagini di rm / cprm ottenute durante i controlli sono state valutate a confronto con quelle della diagnosi , per evidenziare le eventuali variazioni , in maniera indipendente dai due osservatori , con consensus finale . 
 branches analisi delle immagini radiol med ( 2008 ) 113 : 414428 table 2 multifocal intraductal papillary mucinous tumours ( ipmt ) of the side branches : magnetic resonance imaging / magnetic resonance cholangiopancreatography ( mri / mrcp ) pattern at diagnosis and follow - up . 
analisi qualitativa aspetti diagnosi statistica k controllo statistica k n medio dei dotti ii ectasici presenza di colletto di comunicazione 16 / 26 ( 61% ) pz . 0 , 64 20 / 26 ( 77% ) pz . difetti declivi noduli murali 6 / 26 ( 23% ) pz . 1 / 26 ( 4% ) pz . imprengazione di contrasto 1 / 26 ( 4% ) pz . 7 / 26 ( 27% ) pz . 2 / 26 ( 8% ) pz . 2 / 26 ( 8% ) pz . 0 , 34 0 , 45 dotti ii , dotti pancreatici secondari 0 , 55 0 , 24 ing the branch - duct cystic lesion and the main pancreatic duct 5 . 
 statistical analysis in the qualitative analysis , the k statistic was used to calculate interobserver variability in the detection of communication between the main pancreatic duct and the cystic lesions of the side branches , the presence of intraluminal gravitydependent filling defects within the cystic lesions , the presence of mural nodules and mural enhancement of the cystic dilatation , both at diagnosis and at follow - up . 
interobserver agreement was considered slight at k < 0.20 , fair at 0.21 < k < 0.40 , moderate at 0.41 < k < 0.60 , substantial at 0.61 < k < 0.80 and almost perfect at 0.81 < k < 1.00. students t test for paired data was applied to analyse variations in the maximum diameter of the cystic lesion of the major side branches and in the mean diameter of the main pancreatic duct ( head and body - tail ) and its side branches at diagnosis and on follow - up . 
presenza di malformazioni / varianti anatomiche del sistema duttale pancreatico ; presenza di segni indicativi di malignit come presenza di lesioni epatiche secondarie , ascite , linfoadenomegalie , placche peritoneali , infiltrazione dei vasi da parte delle lesioni . lanalisi quantitativa delle immagini stata fatta da un osservatore non coinvolto nellanalisi qualitativa ( sm ) ( 4 anni di esperienza ) , ed ha preso in considerazione i seguenti parametri : 1 . 
diametro massimo del dotto pancreatico principale nella testa e nel corpo - coda . analisi statistica nellanalisi qualitativa stata calcolata la variabilit intable 3 multifocal intraductal papillary mucinous tumours ( ipmt ) of the side branches : magnetic resonance imaging / magnetic resonance cholangiopancreatography ( mri / mrcp ) pattern at diagnosis and follow - up . 
statistically significant results from the analysis of each patients data at diagnosis and last follow - up examination are reported in tables 2 and 3 . results findings at diagnosis qualitative analysis of the images obtained at diagnosis revealed that : 1 . 
nodular mural enhancement of at least one lesion was demonstrated in 1 / 26 patients ( 4% ) , the same patient terosservatore nella rilevazione della comunicazione tra dpp ed ectasie cistiche dei dotti secondari ; presenza di difetti endoluminali declivi allinterno delle ectasie cistiche ; presenza di noduli parietali ; impregnazione di contrasto della parete dellectasia cistica dei dotti secondari , mediante statistica k , sia alla diagnosi che durante il controllo . la correlazione interosservatore stata considerata scarsa per un valore k < 0 , 20 ; sufficiente per 0 , 21 < k < 0 , 40 ; moderata per 0 , 41 < k < 0 , 60 ; buona per valori 0 , 61 < k < 0 , 80 e molto buona per valori 0 , 81 < k < 1 , 00 . inoltre stato applicato il test t di student per dati appaiati per analizzare la variazione del diametro massimo della lesione cistica dei dotti secondari di maggiori dimensioni e del calibro medio del dotto pancreatico principale , nella testa e nel corpo - coda , e dei dotti pancreatici secondari , alla diagnosi ed al controllo . 
risultata significativa ( p = 0 , 01 ) la variazione del diametro medio della lesione cistica dei dotti secondari di maggiori dimensioni . lanalisi statistica stata eseguita impiegando il software spss ( spss per windows , versione 11.0 , 2001 ; spss chicago , il , usa ) ; sono stati considerati significativi valori di p0 , 05 .i risultati significativi dellanalisi statistica dei dati ottenuti dallosservazione degli esami eseguiti alla diagnosi e di quelli dellultimo controllo di ogni paziente sono riportati nelle tabelle 2 e 3 . radiol med ( 2008 ) 113 : 414428 fig . 
a coronal t2 - weighted mrcp image , obtained using half - fourier single - shot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 1 , 100 ms ) sequences shows multiple cystic dilations of the side branches extending along the entire pancreas , with a communication neck between the cystic dilations and main pancreatic duct , which maintains its regular diameter . 
1a , b aspetto di risonanza magnetica ( rm ) colangiopancreatografia con rm ( cprm ) dei tumori intraduttali papillari mucino - sernenti ( tipm ) multifocali dei dotti secondari . 
a limmagine t2 - dipendente di cprm con sequenze half fourier single - shot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 1100 ms ) lungo il piano coronale , dimostra unectasia cistica di multipli dotti pancreatici secondari , lungo tutta lestensione della ghiandola , in comunicazione con il dpp con morfologia a colletto del dotto di comunicazione . 
three of 26 patients ( 11% ) had pancreas divisum . none of the patients exhibited signs suggestive of malignancy , such as secondary hepatic lesions , ascites , lymph node enlargement , peritoneal deposits or vessel invasion by the lesions . 
the main pancreatic duct was not visualised in 1 / 26 patients ( 4% ) , whereas in the remaining 25 patients ( 96% ) , it had a mean diameter of 3.1 mm ( range 25 mm ) in the head and 2.3 mm ( range 25 mm ) in the body - tail of the pancreas ( table 3 )  . risultati osservazioni alla diagnosi lanalisi qualitativa delle immagini degli esami eseguiti alla diagnosi ha evidenziato : 1 . 
a coronal t2 - weighted magnetic resonance cholangiopancreatography ( mrcp ) image using half - fourier single - shot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 1100 ms ) sequences shows an intraluminal filling defect in a branch - duct cystic dilation in the body of the pancreas ( arrow )  . 
a immagine t2 - dipendente di cprm , ottenuta con sequenze half fourier single - shot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 1100 ms ) , dimostra un difetto di riempimento allinterno del lume di unectasia cistica di uno dei dotti secondari a livello del corpo ( freccia )  . 
b nelle immagini assiali t2 - dipendenti half fourier singleshot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 102 ms ) , si conferma la sede declive del difetto di riempimento ( freccia )  . findings at last follow - up examination qualitative analysis of the images of each patients last follow - up examination revealed that : 1 . 
in 3 / 26 ( 11% ) pz stato osservato un pancreas divisum . nessuno dei pazienti ha dimostrato segni indicativi di malignit come lesioni epatiche secondarie , ascite , linfoadenomegalie , placche peritoneali , infiltrazione dei vasi da parte delle lesioni . 
la variabilit interosservatore risulta avere , alla diagnosi , un buon grado di correlazione per la rilevazione del colletto di comunicazione ( k = 0 , 64 ) , un grado di correlazione sufficiente per losservazione di noduli murali ( k = 0 , 34 ) e un grado di correlazione moderato ( k = 0 , 45 ) per limpregnazione di contrasto . lanalisi quantitativa ha evidenziato : 1 . 
il dotto pancreatico principale non stato visualizzato in 1 / 26 ( 4% ) pz , negli altri 25 ( 96% ) pz presentava un diametro medio di 3 , 1 mm ( range 25 mm ) nella testa della ghiandola , e di 2 , 3 mm ( range 25 mm ) nel corpo - coda ( tabella 3 )  . osservazioni allultimo controllo lanalisi qualitativa delle immagini di ogni paziente ha fatto rilevare : 1 . 
in nessuno dei pazienti si osservata la comparsa di segni indicativi di malignit come lesioni epatiche secondarie , ascite , linfoadenomegalie , placche peritoneali , infiltrazione dei vasi da parte delle lesioni . radiol med ( 2008 ) 113 : 414428 fig . 
3a - d multifocal intraductal papillary mucinous tumours ( ipmt ) of the side branches : non - gravity - dependent mural nodules and their evolution on follow - up . 
a immagine assiale t2 - dipendente half fourier single - shot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 102 ms ) , eseguita alla diagnosi ( 9 / 2001 ) documenta due ectasie cistiche dei dotti secondari a livello del corpo , senza vegetazioni parietali n abnorme impregnazione di contrasto ( freccia ) nelle immagini vibe t1 - dipendenti ( tr / te 4 , 5 / 1 , 7 ms ) ( b ) , ottenute in fase venosa portale dopo somministrazione di chelati del gadolinio ( freccia )  . 
a coronal half - fourier single - shot turbo spin - echo ( haste ) t2 - weighted magnetic resonance cholangiopancreatography ( mrcp ) ( tr / te ( cid : 3 ) / 1100 ms ) , performed at diagnosis ( 10 / 2001 ) , shows multiple branch - duct cystic dilations throughout the pancreas . 
a limmagine t2 - dipendente di cprm , ottenuta alla diagnosi ( 10 / 2001 ) con sequenze half fourier single - shot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 1100 ms ) , lungo il piano coronale mostra multiple ectasie cistiche dei dotti pancreatici secondari , lungo tutta lestensione della ghiandola , il cui numero appare aumentato rispetto nel successivo controllo eseguito nel 10 / 2003 ( b )  . 
in tutti i pazienti stato possibile individuare il dotto pancreatico principale , che risultato avere un diametro medio di 3 , 3 mm ( range : 25 mm ) alla testa e di 2 , 6 mm ( range : 25 mm ) al corpo - coda ( tabella 3 )  . non si osservato un aumento significativo del calibro radiol med ( 2008 ) 113 : 414428 fig . 
a coronal half - fourier single - shot turbo spin - echo ( haste ) t2 - weighted magnetic resonance cholangiopancreatography ( mrcp ) ( tr / te ( cid : 3 ) / 1 , 100 ms ) , performed at diagnosis ( 06 / 2000 ) , shows multiple branch - duct cystic dilations throughout the pancreas , with normal size of the main pancreatic duct . 
a limmagine t2 - dipendente di cprm con sequenze half fourier single - shot turbo spin - echo ( haste ) ( tr / te ( cid : 3 ) / 1100 ms ) lungo il piano coronale , ottenuta alla diagnosi ( 6 / 2000 ) , documenta multiple ectasie cistiche dei dotti secondari lungo tutta lestensione della ghiandola , con normale calibro del dotto pancreatico principale . 
b il quadro appare immodificato alla cprm di controllo del 5 / 2005 . tients diagnostic and last follow - up examination is shown in table 2 . quantitative analysis revealed that : 1 . 
the main pancreatic duct was visualised in all patients and had a mean diameter of 3.3 mm ( range 25 mm ) in the head and 2.6 mm ( range 25 mm ) in the body - tail segments , corresponding to a nonsignificant increase in diameter on follow - up images ( table 3 )  . comparison of data from the quantitative analysis of each patients diagnostic and last follow - up examination is shown in table 3 . discussion ipmt are cystic neoplasms arising in the epithelial lining of the pancreatic ductal system at the level of the main pancreatic duct or its side branches . 
the characteristic features of these tumours are a papillary growth pattern and production of excessive amounts of highly viscous extracellular mucin that obstructs the lumen of the pancreatic ducts causing pawith time , the walls of the affected duct or ducts become distended , producing the typical appearance of a cystic pancreatic mass [ 6 , 13 ]  . del dotto pancreatico principale nelle misurazioni effettuate negli esami di controllo rispetto a quelle ottenute alla diagnosi ( tabella 3 )  . il confronto dei dati ottenuti dallosservazione quantitativa degli esami eseguiti alla diagnosi e di quelli dellultimo controllo di ogni paziente sono riportati in tabella 3 . discussione i tumori intraduttali papillari mucino - secernenti ( tipm ) , sono neoplasie cistiche che si originano dallepitelio del sistema duttale pancreatico , sia a livello del dotto pancreatico principale che dei dotti secondari . 
la peculiarit di questi tumori quella di avere una crescita papillare e produrre uneccessiva quantit di mucina extracellulare , che per la sua viscosit responsabile di unocclusione del lume dei dotti pancreatici , con possibile comparsa di dolore . 
con il tempo si assiste ad uno sfiancamento delle pareti del dotto , o dei dotti in cui il tipm si sviluppa , che conferisce il tipico aspetto di neoformazione cistica del pancreas [ 6 , 13 ]  . le caratteristiche istologiche dei tipm variano dalladenoma , al tumore borderline , al carcinoma in situ ed al carcinoma . 
il rischio di degenerazione di tali neoplasie varia in base alla loro sede : i tipm che si originano dal dotto pancreatico principale possiedono un rischio di degenerazione maligna del 60%92% [ 3 , 6 ] dei casi , mentre i tipm che si originano nei dotti pancreatici secondari del 6%40% [ 7 , 8 ]  . 
pertanto i tipm ad origine dal dpp sono candidati 426 radiol med ( 2008 ) 113 : 414428 histological abnormalities of ipmt range from adenoma to borderline tumours , carcinoma in situ and invasive carcinoma . 
the risk of malignant degeneration of these tumours varies according to their location : the malignancy rate of main - duct - type ipmt is 60%92% [ 3 , 6 ] , whereas that of branch - duct - type is 6%40% [ 7 , 8 ]  . 
patients with multifocal ipmt therefore require close surveillance to ensure early detection of signs of progression or degeneration , including new - onset diabetes , enlargement of lesions , involvement of the main pancreatic duct and appearance of mural nodules or mural contrast enhancement [ 10 , 14 , 16 ]  . in our series , we observed a nonsignificant increase in the mean number of cystic lesions over time . 
instead , a significant increase was noted in the mean diameter of branchduct cystic lesions , a sign of disease progression , as suggested by previous reports [ 18 ]  . 
this finding does not , however , indicate malignant transformation nor does it warrant increased suspicion of malignancy or changes to the followup schedule , considering the slow growth of this tumour [ 19 , 20 ]  . in our study , we did not record a significant increase in the diameter of the main pancreatic duct , which would have indicated possible disease extension from the side branches to the main duct . 
such a finding would have been suspicious , as involvement of the main duct is associated with an increased risk of malignant change . in 1 / 26 patients ( 4% ) , we observed the appearance of enhancing mural nodules , a sign associated with malignant transformation . 
however , the patient exhibited none of the other imaging signs of malignancy identified in the literature [ 10 , 1416 ] nor did he report any clinical symptoms . this induced us not to perform a pancreatic resection but to intensify the follow - up ( every 6 months ) [ 13 ]  . the appearance of suspicious elements during the follow - up period , even in the absence of clinical manifestations , should , however , be carefully evaluated , as it may be a possible expression of degeneration . 
in such cases , patients should undergo reassessment by the surgeon , including laboratory testing , as potential candidates for resection , and the imaging follow - up intervals should be shortened as a conservative measure [ 21 ]  . 
on the other hand , the absence of suspicious elements should not lead us to underestimate ad un intervento chirurgico mentre per i tipm che si originano dai dotti secondari lindicazione ad un intervento chirurgico mutilante pi incerta . 
questi segni comprendono : comparsa di diabete , ingrandimento delle lesioni , coinvolgimento del dotto pancreatico principale , comparsa di vegetazioni parietali e di impregnazione di contrasto delle pareti [ 10 , 14 , 16 ]  . nella nostra serie , abbiamo osservato un aumento non significativo del numero medio delle ectasie cistiche nel tempo . 
significativo , invece , stato laumento del diametro medio delle ectasie cistiche dei dotti pancreatici secondari , indice di unevoluzione della malattia , come gi suggerito da altri studi [ 18 ]  . 
questo dato , peraltro , non deve far aumentare il sospetto in questi pazienti , in quanto non rappresenta segno suggestivo di trasformazione maligna e , in considerazione dei lunghi tempi di crescita , non richiede un cambiamento del programma di controllo nel tempo [ 19 , 20 ]  . nella nostra serie non abbiamo invece rilevato un aumento significativo del calibro del dotto pancreatico principale , che potrebbe essere indicativo di estensione della neoplasia , dai dotti secondari al dpp . 
questo dato sarebbe stato sospetto in quanto il coinvolgimento del dpp si associa ad un aumentato rischio di trasformazione maligna . in 1 / 26 ( 4% ) pazienti della nostra serie abbiamo osservato la comparsa di nodulazioni parietali , con impregnazione di contrasto , che rappresenta pertanto un sospetto di evoluzione nel processo di trasformazione . 
questo paziente , tuttavia , non ha manifestato contemporaneamente altri criteri di diagnostica per immagini di malignit , identificati dalla letteratura [ 10 , 1416 ] , n ha accusato alcuna sintomatologia clinica . 
pertanto stato deciso di non sottoporlo ad intervento di resezione pancreatica , ma a controlli periodici pi frequenti ( ogni 6 mesi ) [ 13 ]  . la comparsa di alcuni elementi di sospetto nel corso dei controlli periodici , pur in assenza di manifestazioni cliniche , va comunque guardata con particolare attenzione in quanto possibile espressione di degenerazione . 
pertanto , in tali evenienze , i pazienti andrebbero rivalutati dal chirurgo , anche dal punto di vista laboratoristico , in quanto potenziali candidati alla resezione chirurgica , e lintervallo di controllo radiologico andrebbe ridotto a scopo prudenziale [ 21 ]  . 
va comunque sottolineato che lassenza di tali elementi di sospetto non deve fare sottostimare la potenradiol med ( 2008 ) 113 : 414428 the malignant potential of multifocal peripheral ipmt and to a recommendation of long follow - up intervals , which may prove hazardous . ziale malignit del tipm periferico multifocale , suggerendo al paziente rischiosi ampi intervalli di controllo . conclusions because multifocal branch - duct - type ipmt involves the entire pancreas , it should be considered an organ disease , with a tendency to progress , albeit very slowly . 
mean age of patients in our series was 67 years . on the basis of our observations , we consider a follow - up with mri / mrcp at intervals of at least 612 months to be a valid approach . 
it allows early detection of even slight morphological changes that may indicate malignant transformation and provides precise surgical indication that is neither too early , leading to radical resection in asymptomatic patients , nor too late , when effective curative treatment is no longer feasible . conclusioni il tipm dei dotti collaterali con caratteristiche multifocali , per il fatto che interessa tutta lestensione del pancreas , va considerato una malattia dorgano , con tendenza allevoluzione , seppur molto lenta . 
questa neoplasia risulta essere quasi sempre un reperto occasionale , diagnosticata in pazienti spesso asintomatici e in et adulta : et media 67 anni , nella nostra serie . le nostre osservazioni ci portano a ritenere valido un controllo con rm / cprm del paziente con un intervallo di almeno 6 o 12 mesi . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica , radioterapia , policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy 2istituto di oculistica , policlinico universitario tor vergata , roma , policlinico casilino / presidio sanitario usl - b , via casilina 1049 , 00100 roma , italy 3uoc di anestesia e rianimazione , policlinico casilino / presidio sanitario usl - b , via casilina 1049 , 00100 roma , italy correspondence to : m . 
complications included pain in three cases , eyelid inflammation in four cases and severe bleeding in one case . postprocedural mucocele was observed in five patients . mean time without symptoms was 31 weeks . 
there were 24 cases of stent obstruction : 15 were treated with highpressure 5% n - acetyl - cysteine and saline flush , achieving resolution in two cases ; in three cases , attempts to recanalise the obstruction with a guidewire failed . 
the occluded stents were removed in 22 patients : seven remained asymptomatic , 15 had recurrence of epiphora , nine received a new stent after dacryocystography and six underwent dacryocystorhinostomy . 
advantages of the procedure include the lack of anatomical alterations to the lacrimal ducts and a low short - term complication rate , whereas limitations include restricted duration of stent patency . 
abbiamo rilevato 24 ostruzioni : 15 trattate con lavaggi ad alta pressione di n - acetil - cisteina 5% con soluzione fisiologica ottenendo completa guarigione in 2 pazienti , stato effettuato un tentativo infruttuoso ( 3 casi ) di ricanalizzare lostruzione con una guida . 
limiti : perviet dello stent limitata . prospettive : individuare gli eventi fisiopatologici che portano ad ostruzione e correlarli con la morfologia dello stent . 1212 radiol med ( 2008 ) 113 : 12111218 keywords epiphora lacrimal gland nasolacrimal stenting parole chiave epifora ghiandola lacrimale stent nasolacrimale introduction introduzione epiphora refers to inadequate lacrimal - duct drainage and is seen in 3% of ophthalmology consultations [ 1 , 2 ] , with an incidence of 30%40% among the population older than 50 years of age [ 3 ]  . 
the main risk factors include white race ( especially mediterranean ) , advanced age , female gender ( 4 to 5 women for every one man ) and poor hygiene in low socioeconomic settings [ 3 ]  . 
 diagnosis is based on clinical assessment and diagnostic imaging with dacryocystography , computed tomography ( ct ) - dacryocystography and magnetic resonance ( mr ) dacryocystography , which provide information on the nature and site of the obstruction [ 3 ]  . 
treatment options include dacryocystorhinostomy ( dcr ) and stent placement . the first is a surgical procedure performed under general anaesthesia , with an 89%95% rate of technical success [ 48 ]  . 
the purpose of this study was to evaluate the patency of the song polyurethane nasolacrimal stent ( song nasolacrimal duct stent set , cook , qld , australia ) implanted in patients with lacrimal - duct stenoses obstructions and to assess its long - term effectiveness over a 5 - year follow - up . lepifora corrisponde allinsufficiente drenaggio da parte delle vie lacrimali e viene riscontrata nel 3% delle visite oculistiche [ 1 , 2 ]  . 
i pi importanti fattori di rischio correlati con questa patologia : frequente in persone di razza caucasica ( soprattutto mediterranei ) , aumenta con let , viene colpito soprattutto il sesso femminile ( 45 donne per uomo ) , lincidenza aumentata per minore igiene negli ambienti socioeconomici meno sviluppati [ 3 ]  . la diagnosi si effettua soprattutto con la clinica e la diagnostica per immagini con la dacriocistografia , la dacriotc e la dacrio - rm fornisce informazioni sulla natura e la localizzazione dellostruzione [ 3 ]  . 
la prima una tecnica chirurgica condotta in anestesia generale con successo tecnico 89%95% [ 48 ] ; le complicanze maggiormente riscontrate sono il sanguinamento , che richiede un buon controllo pressorio per moderarne la entit . 
la chiusura del tramite fistoloso creato [ 9 ]  . laltra tecnica stata sviluppata da diversi anni e consiste nellapplicazione di uno stent nella via naturale per via interventistica non chirurgica . 
il nostro obiettivo di valutare la perviet dello stent nasolacrimale in poliuretano disegnato da song impiantato in pazienti con steno - ostruzioni delle vie lacrimali e constatarne la perviet a lungo termine con follow up fino a 5 anni . materials and methods materiali e metodi from 2003 to march 2007 , we implanted 76 polyurethane song nasolacrimal stents in 73 consecutive patients ( 16 men and 57 women ; mean age 56 years ; age range 1981 ) with recurrent epiphora and / or dacryocystitis due to nasolacrimal duct obstruction . 
in our department , the procedure is tra il 2003 e marzo 2007 abbiamo impiantato 76 protesi naso - lacrimali in poliuretano ideate da song ( song nasolacrimal duct stent set , cook , queensland , australia ) in 73 pazienti consecutivi con epifora e / o dacriocistiti ricorrenti , dovute ad ostruzione del dotto naso - lacrimale . 
local anaesthesia was induced with novesin drops to reduce ocular reflex , followed by lidocaine hydrochloride ( 200 mg / 10 ml ) in medial orbital ( infratrochlear ) location and close to the infraand supraor1213 casi ( 4 , 1% )  . 
nel nostro dipartimento diamo indicazione per la procedura nei pazienti con grado > 3 o nei casi di dacriocistiti . la diagnostica pre - procedurale viene effettuata mediante esame dacriocistografico integrato con esame dacrio - tc per ottenere informazioni sul livello dellostruzione e lanatomia del paziente . 
limpianto dello stent stato realizzato dal servizio di diagnostica per immagini imaging molecolare radiologia interventistica e radioterapia del policlinico universitario tor vergata roma e dalla uoc di radiologia del policlinico casilino asl roma b in regime day hospital . 
si procede con anestesia locale con novesina gocce per ridurre i riflessi oculari , quindi con anestesia con lidocaina cloridrato ( 200 mg / 10 ml ) in localizzazione orbitaria mediale ( infratrocleare ) ed adiacente ai forami infra e sovraorbitari . 
stata sempre associata anche lapplicazione nella fossa nasale inferiore di garza imbevuta in soluzione contenente quota di vasocostrittore unitamente allanestetico locale ( 30 cc di soluzione fisiologica con 10 cc di lidocaina cloridrato 2% , 0 , 5 mg adrenalina ) ; la finalit di questa procedura di avere anestesia a livello della fossa nasale inferiore e vasocostrizione della mucosa nasale per ridurre il sanguinamento a carico della mucosa dei turbinati durante la fase nasale della procedura . 
si introduce una guida metallica ( calibro 0 , 018 ) con oliva allestremit distale attraverso il puntino lacrimale , generalmente il superiore , precedentemente dilatato , avanzandola fino al sacco lacrimale . 
1a , b dacriocistografia in paziente donna di 75 anni che evidenzia ostruzione infundibolare del canale naso lacrimale di sinistra . 1214 radiol med ( 2008 ) 113 : 12111218 fig . 
the nasal cavity was packed with gauze soaked in a solution of 30 cc of saline with 10 cc of 2% lidocaine hydrochloride and 0.5 mg adrenaline to achieve anaesthesia and vasoconstriction of the nasal mucosa and reduce bleeding of the turbinate during the nasal phase of the procedure . dacryocystography was then performed to locate the anatomical landmarks and confirm the diagnosis of lacrimal - duct obstruction . 
a 6 - f introducer sheath with a dilator was passed over the guidewire and advanced to the lacrimal sac , where the dilator was removed while the sheath was left in place . 
after reaching the lacrimal sac , the stent was inserted into the sheath and advanced up to the desired position ; the introducer was then pulled back and the stent left in situ . 
con dilatatore ed una volta raggiunto il sacco lacrimale si rimuove la camicia dellintroduttore ( dilatatore ) mantenendo in situ lintroduttore , dopo aver raggiunto il sacco lacrimale , si inserisce nellintroduttore sempre per via trans nasale la protesi che viene spinta fino alla posizione desiderata per poi rimuovere lintroduttore con tecnica pull back e lasciate lo stent in situ . 
i successivi controlli sono affidati alla divisione di oftalmologia del nostro policlinico universitario . risultati il tempo medio procedurale di 16 minuti ( massimo 44 minuti , minimo 8 minuti )  . 
in 2 dei tre casi in cui non risultata possibile le ricanalizzazione la guida ha superato lostruzione ma il recupero con lapposito gancio non stato possibile ; nel caso rimanente non risultato possibile superare radiol med ( 2008 ) 113 : 12111218 1215 fig . 
in two cases , recanalisation failed because we were unable to remove the guidewire with the hook despite having crossed the obstruction ; in one case , the obstruction could not be crossed . two patients had posttraumatic epiphora , and one had a lostruzione . 
le principali complicanze riscontrate sono : dolore in 3 ( 3 , 96% ) procedure , infiammazione palpebrale in 4 ( 5 , 2% ) procedure , emorragia in cui stato necessaria la consulenza otorinolaringoiatria 1 ( 1 , 3% ) caso , mucocele post - procedura riscontrato in 5 ( 6 , 5% ) pazienti . 
in un paziente si registrata stazionariet del quadro clinico pur con il rilevo di un inappropriato posizionamento dello stent ; dopo 3 mesi si deciso di sostituirlo con risultati soddisfacenti . 
one patient , with evidence of stent malposition , showed no clinical benefit , and the stent was replaced after 3 months with satisfactory results . the mean follow - up period was 1 year . 
in 15 cases of obstruction , we attempted to recanalise the duct with highpressure flushing with saline solution and 5% nacetyl - cysteine through the superior punctum ; this succeeded in restoring stent patency for the entire duration of the follow - up period in two patients . 
these cases are eligible for a possible reimplantation of a polyurethane stent : of the 15 patients with epiphora after stent removal , nine opted for stent reimplantation and six for dcr . 
follow - up of these nine patients demonstrated early recurrence in five ; this could be due to an inflammatory reaction caused by the close proximity of the head of the stent to the lacrimal sac in patients with a small sac , with the production of large amounts of granulation tissue . discussion the use of song stents has several advantages compared with traditional surgical techniques : local anaesthesia , easy placement , safety , no facial scar , less bleeding and better tolerance by patients [ 11 ]  . 
technical success rates ( 96% ) are similar to those reported for dcr ( 89%93% ) [ 12 ] and are greater than those of metallic - stent implantation ( 25% ) [ 13 ] or balloon dilation ( 45% ) [ 10 ]  . 
in 15 casi con ostruzione abbiamo tentato di ricanalizzare lo stent mediante lavaggi forzati con soluzione fisiologica e n - acetilcisteina 5% tramite il puntino lacrimale superiore ottenendo perviet nellintero follow - up in 2 pazienti ; abbiamo tentato la ricanalizzazione mediante guida posizionata dal radiologo interventista in 3 casi con mancata disostruzione . negli altri 22 pazienti abbiamo optato per la rimozione della protesi ostruita . 
abbiamo trovato materiale mucoso in 8 protesi e tessuto di granulazione nelle altre 14 . in 18 dei 22 pazienti in cui abbiamo rimosso lo stent ostruito , la via lacrimale tornata pervia . 
questi pazienti sono candidati per un eventuale riposizionamento dello stent in poliuretano : dei 15 pazienti con epifora dopo la rimozione dello stent lacrimale , 9 di loro hanno optato per il riposizionamento dello stent e gli altri 6 per la dcr . 
il follow - up di questi 9 pazienti documentava recidiva a breve termine della sintomatologia in 5 ; tale fenomeno potrebbe essere attribuibile ad una reazione infiammatoria dovuta ad uno stretto rapporto tra la parte prossimale dello stent con il sacco lacrimale in pazienti con sacco lacrimale di esigue dimensioni pertanto si sviluppa unimportante quota di tessuto di granulazione . 
 discussione il posizionamento dello stent di song presenta notevoli vantaggi rispetto alle tecniche chirurgiche tradizionali : anestesia locale , facilit di esecuzione , elevata sicurezza della procedura , assenza di ferite chirurgiche facciali , ridotti sanguinamenti , maggiore tollerabilit da parte dei pazienti [ 11 ]  . 
il successo tecnico ottenuto ( 96% ) comparabile con quello riportato per la dacriocistorinostomia ( 89%93% ) [ 12 ] e supera i risultati ottenuti con il posizionamento dello stent metallico ( 25% ) [ 13 ] o la dilatazione con palloncino ( 45% ) [ 10 ]  . 
 nel nostro studio la ricorrenza dei sintomi si verificata in 24 casi ( 31 , 6% ) , di questi dopo lavaggi con soluzione fisiologica e n - acetil - cisteina 5% tramite il puntino lacrimale superiore ottenendo ricanalizzazione in 2 ; negli altri abbiamo optato per la rimozione dello stent , tale procedura non preclude la possibilit di riposizionare un secondo stent in caso di ricorrenza dellepifora che si verificata in 15 pazienti ( 4 dal momento in cui stato rimosso lo stent e 11 nel follow up a 39 settimane )  . 
prima di riposizionare un nuovo stent dobbiamo ripetere tutte le indagini di diagnoradiol med ( 2008 ) 113 : 12111218 1217 tum , whereas the other patients had the stents removed . stent removal does not preclude placement of a new stent should epiphora recur , as it did in 15 of our patients ( four at the time of stent removal and 11 at the 39 - week follow - up )  . before stent reimplantation , however , all imaging exams must be repeated to evaluate the exact grade and level of stenosis obstruction . unlike surgery , which produces irreversible anatomical alterations , this minimally invasive technique is less traumatic , requires a shorter hospital stay with similar results and above all allows nonfunctional stents to be removed without altering the patients normal anatomy . there is evidence to indicate that the position of the head of the stent may play an important role in stent patency and function : in particular , stent patency seems to be longer when the head of the stent is not in close contact with the upper portion of the lacrimal sac ( confluence of the canaliculi , upper fornix )  . 
this view is supported by reports [ 14 ] that stents modified in their extreme end ( mushroom tip ) had 79% patency rates at 24 months [ 15 ]  . therefore minimising interaction between the head of the stent and the lacrimal sac is thought to better preserve normal lacrimal dynamics and consequently ensure longer stent survival . 
this may be explained by tear - flow dynamics and the possible blockage of the pump system produced by the musculus orbicularis by the head of a stent that is placed too cranially . 
 in this case , the stent was found to be positioned very cranially and in close contact with the upper fornix of the lacrimal sac . conclusions advantages of this procedure are that it does not alter the anatomy of the lacrimal outflow pathway , it can be repeated and has a low rate of intra - , peri - , and postprocedural complications . 
it is necessary that the causes of stent obstruction ( fibrous tissue around the stent ) be accurately investigated , including the role of tear - fluid composition and superimposed inflammatory processes . the lacrimal stents in use today may not be ideal . 
the position of the stent head within the lacrimal sac and , in particular , its contact with the common duct and the upper fornix , need to be evaluated in relation to symptoms and the duration of stent patency . stica per immagini necessarie per valutare la precisa entit della steno - ostruzione ed il livello . al contrario della tecnica chirurgica che genera modificazioni anatomiche non ripristinabili in caso di fallimento , la tecnica mini - invasiva si pu avvalere del vantaggio della minor traumaticit , minore degenza con risultati comparabili e soprattutto la possibilit di potere rimuovere lo stent posizionato non funzionante rispettando la normale anatomia del paziente . alcuni elementi indicano che la posizione dellestremo oculare dello stent pu giocare un ruolo importante nella durata della perviet e nella funzionalit dello stent : in particolare meno stretto il rapporto con lestremit craniale del sacco lacrimale ( confluente dei canalini , recesso superiore ) e maggiore sembra essere il periodo di perviet dello stent . 
questa teoria viene supportata da studi [ 15 ] che hanno segnalato che stent modificati nella estremit oculare garantiscono una durata della perviet di 79% a 24 mesi [ 14 ]  . 
pertanto possiamo ritenere che quanto meno lo stent interagisce con il sacco tanto maggiore la conservazione della normale dinamica lacrimale e di conseguenza la durata dello stent nella sua funzione . la motivazione pu essere ricercata nella dinamica stessa del flusso lacrimale , in particolare nelle possibili interferenze sul sistema di pompa generato dai muscoli orbicolari che lo stent posizionato troppo cranialmente pu determinare . 
in questa caso lo stent risultava posizionato in situazione alquanto craniale a stretto ridosso del recesso superiore . conclusioni vantaggi : procedura che lascia inalterata la anatomia di deflusso delle vie lacrimali , ripetibile , con complicanze intra - peri - postprocedurali basse . 
limiti : durata della perviet dello stent limitata , con ampie variazioni tra caso e caso ( casi che durano da oltre cinque anni ; casi che si ostruiscono dopo pochi mesi )  . 
prospettive : vanno individuati con maggiore precisione i motivi per i quali si verifica la ostruzione ( tessuto fibroso intorno allo stent ) che possono in varie maniere essere determinate dalla qualit del fluido lacrimale e dalla sovrapposizione di processi flogistici . lo stent lacrimale attualmente in uso potrebbe non essere quello ideale ; esistono valide indicazioni per sperimentare limpiego di stent di nuova concezione che rispondano ai requisiti indicati . 
the aim of this study was to describe magnetic resonance imaging ( mri ) patterns in 21 patients with histologically proven invasive lobular cancer ( ilc ) of the breast . 
we retrospectively reviewed mr images of 21 out of 24 women with ilc of the breast . three women were excluded from the study because they underwent neoadjuvant chemotherapy after mri . 
all 24 patients underwent mammography , sonography and mri . mri was performed to evaluate disease extent and multifocality / multicentricity before modified radical mastectomy ( n = 5 ) or quadrantectomy ( n = 16 )  . 
rm stata effettuata per valutare lestensione locale di malattia e leventuale presenza di multifocalit o multicentricit , prima che le pazienti fossero sotttoposte a mastectomia radicale modificata ( n = 5 ) o quadrantectomia ( n = 16 )  . 
le caratteristiche morfologiche e dinamiche sono importanti nellinterpretazione della rm mammaria . ilc pu essere identificato dalla rm sulla base della presenza di lesioni solitarie o multiple , che corrispondono ai reperti anatomo - patologici . 
indagini rm negative sono rare , ma possibili in una bassa percentuale di ilc . parole chiave mammella risonanza magnetica carcinoma lobulare invasivo radiol med ( 2008 ) 113 : 11101125 introduction introduzione 1111 invasive lobular carcinoma ( ilc ) is a neoplasm originating in the lobular epithelium of the breast . 
first described in 1941 , its unique growth patterns were noted , including a linear arrangement of cells ( so - called indian - file pattern ) and a scattered growth pattern [ 3 ]  . 
a single - file infiltration of malignant cells has also been described [ 46 ] through the breast stroma with a relative paucity of desmoplastic response , haemorrhage , necrosis or calcifications [ 6 ]  . 
these histological patterns may account for the higher false - negative rate on mammography than observed for other types of invasive breast carcinoma [ 5 , 7 ] , so the reported sensitivity for detection is 57%92% [ 8 , 9 ]  . clinically , these tumours can appear as a fixed palpable mass that may exhibit skin retraction . 
on sonography , detection of ilc may be difficult : the range of sensitivity has been reported to be 68%87.7% , with the sensitivity for lesions smaller than 1 cm in the range of 25%85.7% [ 10 , 13 ]  . 
patients with ilc are reported to have a relatively high frequency of multifocal , multicentric or bilateral breast cancer ( 14%31% ) [ 4 , 8 , 14 , 15 ]  . 
for the correct choice between breast - conserving treatment and mastectomy , accurate definition of disease extent and possible multifocality / multicentricity of bilateral breast cancer are essential [ 16 ]  . previous studies have shown breast magnetic resonance imaging ( mri ) to be a useful adjunct to mammography and ultrasound ( us ) , with sensitivity reaching 100% in the detection of invasive breast cancer [ 4 , 16 , 17 ] and specificity varying from 37% to 86% [ 1823 ]  . 
 [ 1 ] reported that mri revealed more extensive tumour burden than did conventional imaging in seven of 18 patients with ilc . we retrospectively compared the findings of preoperative dynamic mri with those of mammography and us in 24 patients with pure ilc of the breast , using results from histopathological examination as the gold standard . 
la seconda , in ordine di frequenza , tra le neoplasie maligne della mammella e pu presentarsi in pressoch qualsiasi fascia di et della donna adulta [ 1 ]  . 
descritta per la prima volta nel 1941 , vennero da subito notati le singolari modalit di crescita , rappresentate da ununica filiera di cellule ( il cosiddetto pattern a fila indiana ) o , in alternativa , da una proliferazione in ordine sparso [ 3 ] ; inoltre , descritto anche un comportamento caratterizzato da una infiltrazione di cellule maligne in fila singola [ 46 ] attraverso il parenchima mammario con una relativa scarsit di risposta desmoplastica , di emorragia , necrosi o calcificazioni [ 6 ]  . 
questi aspetti istologici sono ritenuti responsabili della percentuale di indagini mammografiche falsamente negative pi elevata rispetto a quanto accade per altre neoplasie mammarie [ 5 , 7 ] , con una sensibilit di rilevazione riportata intorno al 57%92% [ 8 , 9 ]  . clinicamente , queste neoplasie possono apparire come masse palpabili fisse rispetto ai piani circostanti , a volte associate a retrazione dei piani cutanei . 
in ogni caso , ilc spesso si presenta come un processo infiltrativo diffuso in assenza di alcuna massa clinicamente palpabile [ 912 ]  . lidentificazione di ilc mediante ecografia pu essere difficoltosa : lintervallo di sensibilit riportato 68%87 , 7% , con una sensibilit per lesioni dimensionalmente inferiori al centimetro nellintervallo di 25%85 , 7% [ 10 , 13 ]  . 
i pazienti con ilc sono ritenuti soggetti a una maggior frequenza di multifocalit , multicentricit o bilateralit della localizzazione ( 14%31% ) [ 4 , 8 , 14 , 15 ]  . 
per una corretta scelta tra trattamento chirurgico conservativo e mastectomia sono essenziali unaccurata definizione dellestensione di malattia e la identificazione della possibile multifocalit / multicentricit o bilateralit del cancro mammario [ 16 ]  . studi precedenti hanno gi dimostrato lutilit della rm mammaria in ausilio di mammografia ed ecografia , con una sensibilit che raggiunge il 100% nellidentificazione del cancro mammario invasivo [ 4 , 16 , 17 ] ed una specificit che varia tra il 37% e l86% [ 1823 ] , ma solo pochi studi si sono focalizzati sulla utilit della rm mammaria in pazienti con ilc [ 17 , 24 ]  . 
 [ 4 ] hanno posto in correlazione lestensione del ilc definita allindagine istologica in 20 pazienti che precedentemente erano stati sottoposti a mr mammaria con apparecchiature ad altra risoluzione e utilizzo del mezzo di contrasto paramagnetico e mammografia . 
 [ 1 ] hanno riportato in una casistica 1112 radiol med ( 2008 ) 113 : 11101125 had been diagnosed with ilc between march 2005 and december 2006 and who had undergone preoperative breast mri at our hospital ( a medium - sized , nonacademic institution )  . 
all mammography and us image and reports were reviewed by two experienced breast radiologists . a senographe diamond ( instrumentarium imaging inc . , milwaukee , wi , usa ) was used to obtain all conventional mammographic images . 
breast composition was reported and defined as d1 ( almost entirely fat ) , d2 ( scattered fibroglandular densities ) , d3 ( heterogeneously dense ) or d4 ( extremely dense ) breast tissue . on us , lesions were evaluated and classified as a result of combined morphological characteristics : lesion margins , hyporeflectivity or hyperreflectivity , posterior acoustic shadowing and shape of the mass . 
 another set of unenhanced images was obtained with the following parameters : coronal t2 - weighted turbo spin echo ( tse ) ( tr / te , 3 , 800 / 140 ) , flip angle of 90 , and 512512 matrix . 
a late postcontrast set of images was obtained with the following parameters : coronal t1 - weighted , threedi 18 pazienti affetti da ilc una differente valutazione dimensionale di mr rispetto a mammografia , con una sottostima da parte di questultima metodica 7 casi su 18 . nel presente studio abbiamo retrospettivamente confrontato i reperti di mr mammarie , effettuate prima dellintervento chirurgico di asportazione di neoplasia , con mammografia ed ecografia in 24 pazienti con ilc puro della mammella , utilizzando i dati dellindagine anatomo - patologica come standard di riferimento . materiali e metodi abbiamo retrospettivamente esaminato le immagini di 24 donne con diagnosi di ilc effettuata tra marzo 2005 e dicembre 2006 e che sono state sottoposte a mr mammaria pre - operatoria nel nostro ospedale ( unazienda ospedaliera non universitaria di medie dimensioni )  . 
tutte le mammografie e le indagini ecografiche sono state riviste od eseguite da due radiologi esperti in patologia mammaria . un mammografo diamond ( instrumentarium imaging inc . , milwaukee , wisconsin , usa ) stato utilizzato per effettuare tutte le mammografie . 
le ecografie sono state effettuate con lutilizzo di una sonda a 5 , 57 , 5 mhz ( envisor , philips medical system , pc best , olanda )  . tutte le mammografie sono state interpretate utilizzando il lessico breast imaging reporting and data system ( birads ) alla luce dei reperti clinici [ 25 ]  . 
la densit radiologica del seno stata segnalata e definita come d1 ( pressoch completamente adiposo ) , d2 ( densit fibroghiandolare sparsa ) , d3 ( eterogeneamente denso ) o d4 ( estremamente denso )  . 
 allindagine ecografica , le lesioni sono state valutate e classificate in relazione alla combinazione delle caratteristiche morfologiche : margini della lesione , ipoo iperecogenicit , attenuazione acustica posteriore e forma della massa . 
 before the mri ( minimum 4 days , maximum 44 days ; mean 22.4 days ) , nine patients had undergone fine - needleaspiration cytology ( fnac ) followed by vacuum - assisted biopsy ( vab ) , six had undergone fnac followed by usguided tru - cut microbiopsy , one had undergone fnac on an axillary adenopathy ( negative mammography and us examination of the entire breast ) , three had undergone fnac only and two had undergone vab only without prior fnac . both radiologists reviewed the mri studies of all 21 women . 
morphological mri parameters described by the radiologists included lesion type ( mass , focal / regional enhancement , ductal or linear enhancement , distortion ) , mass margins ( well - circumscribed , ill - defined , obscured or spiculated ) and mass shape ( round , oval , lobular , irregular )  . 
for most sites , it is suggested that the immediate contrast - enhanced series be centred over roughly 2 min ( images obtained within 4 min ) and the delayed contrast - enhanced series be centred over 47 min ( images obtained within 8 min )  . pazienti sono state studiate con mr prima dellintervento chirurgico . 
stata utilizzata unapparecchiature rm 1 , 0 t intera achieva ( philips medical systems , pc best , olanda ) ; le pazienti sono state posizionate in decubito prono con una bobina bilaterale di superficie dedicata sense ( sensitivity encoding )  . 
le mammelle sono state studiate prima e sei volte dopo liniezione endovenosa ( velocit di iniezione 2 cc / s , seguita da 15 ml di soluzione salina ) di gadopentate dimeglumine 0 , 2 mmol / kg ( magnevist , schering , berlino , germania ) con una sequenza coronale t1 pesata , 3d fast field echo gradient - echo ( tr / te , 6 , 7 / 3 , 2 ) , con un flip angle di 25 , campo di vista di 320340 mm , spessore della fetta di 3 mm , senza intervallo tra le fette , matrice di 512512 . 
un altro gruppo di immagini stato ottenuto prima dellinfusione di mezzo di contrasto coi seguenti parametri : coronale t2 pesata turbo spin echo ( tr / te , 3800 / 140 ) , flip angle di 90 , matrice di 512512 . un ultimo gruppo di immagini tardive dopo infusione di mezzo di contrasto stato ottenuto coi seguenti parametri : coronale t1 pesata , 3d ffe gradient echo ( tr / tr , 19 , 0 / 9 , 6 ) , proset ( pro - selective ) water - selective , con un flip angle di 25 , campo di vista di 320340 mm , spessore di fetta di 3 mm , nessun intervallo tra gli strati , matrice di 512512 . 
le immagini pre - contrastografiche sono state poi sottratte dalla prima immagine pre - contrastografica . prima di effettuare lindagine mr ( minimo 4 giorni , massimo 44 giorni ; intervallo medio 22 , 4 giorni ) , 9 pazienti sono state sottoposte ad agoaspirato ( fnac ) ecoguidato seguito da microbiopsia ( vacuum assisted biopsy ) , 6 sono state sottoposte ad agoaspirato ( fnac ) ecoguidato seguito da microbiopsia ecoguidata con ago tru - cut , 1 stata sottoposta a fnac su adenopatia ascellare ( questa paziente era stata gi sottoposta ad indagine mammografia ed ecografia mammaria con esito negativo ) , 3 sono state sottoposte alla sola fnac , 2 sono state sottoposte alla sola vab senza precedente fnac . entrambi i radiologi hanno riesaminato le immagini mr delle 21 donne . 
i parametri morfologici mr descritti hanno incluso il tipo di lesione ( massa , impregnazione contrastografica focale o regionale , impregnazione contrastografica a distribuzione duttale o lineare , distorsione parenchimale ) , i margini della lesione ( netti , mal definiti , non valutabili o spiculati ) e la forma della lesione ( tondeggiante , ovalare , lobulare , irregolare )  . 
il tipo di impregnazione stato suddiviso tra omogenea , disomogenea o ad anello . 1114 radiol med ( 2008 ) 113 : 11101125 to classify areas on the mr examination as having or not having significant enhancement , pixel values at the unenhanced and first contrast - enhanced series are compared . 
if the pixel value on the delayed series decreases by more than 10% of its immediate contrast - enhanced value , that pixel is colour - coded red on the monitor , indicating washout of contrast material . 
finally , the radiologist may select a specific area of significant enhancement , and the programme will automatically generate a synopsis of the full volume of that lesion , including the percentage of the lesion that shows washout , plateau and persistent enhancement . 
lesions suspicious for malignancy were classified as unifocal , multifocal , single - quadrant or multiquadrant disease using the same definitions as mentioned above . morphological findings on mammography , us and mri and the detection of unifocal , multifocal , single - quadrant , multiquadrant or bilateral breast cancer by the three imaging modalities were compared , with results of the final histopathological examination as the gold standard . results thirteen cases were positive on clinical examination . 
questo software stato progettato per la rielaborazione automatica e analisi delle immagini che sono tradizionalmente effettuate manualmente dal tecnico sanitario di radiologia medica e dal medico radiologo . tutti i dati rielaborati sono stati salvati e presentati al medico radiologo per linterpretazione . 
in aggiunta , esso consente di visualizzare automaticamente le curve di impregnazione contrastografica e i dettagli di tutte le regioni con impregnazione contrastografica . per le indagini mr mammaria , il programma utilizza ai fini del calcolo 7 acquisizioni seriate : una serie t1 pesata senza mezzo di contrasto , una serie t1 pesata acquisita immediatamente dopo la somministrazione di mezzo di contrasto , e 5 serie post - contrastografiche successive pesate in t1 ( tempo di acquisizione per ogni sequenza ffe gradient echo 3d t1 57 , 4 secondi )  . 
per la maggior parte degli ospedali , consigliata lacquisizione della serie post - contrastografica centrata attorno ai 2 minuti ( per immagini ottenute nellarco di 4 minuti ) e lacquisizione della serie post - contrastografica tardiva centrata oltre i 47 minuti ( per immagini ottenute nellarco di 8 minuti )  . per classificare le aree nellindagine mr come aventi o meno unimpregnazione contrastografica significativa , vengono confrontati i valori di intensit di segnale dello stesso pixel nella sequenza prima e in quella immediatamente successiva linfusione di mezzo di contrasto . 
se il valore del pixel della serie tardiva decresce di oltre il 10% rispetto al valore della serie immediatamente successiva linfusione di mezzo di contrasto , quel pixel codificato in colore rosso sul monitor , indicando wash - out del mezzo di contrasto . 
in one case only , axillary adenopathy was found . eight women had no suspicious findings on physical examination . breast - tissue densities on mammography of the 21 cases were almost entirely fat ( d1 ) ( n = 10 ) , scattered fibroglandular densities ( d2 ) ( n = 6 ) , heterogeneously dense ( d3 ) ( n = 4 ) and extremely dense ( d4 ) ( n = 1 )  . 
in the subgroup of ten patients with almost entirely fatty breasts , three had no clinically relevant finding , two presented with a palpable mass , three presented with increased density without a palpable mass , one presented with increased density associated with nipple retraction and one presented with increased density associated with nipple retraction and increased skin thickness . 
 mammography obtained before biopsy failed to detect ilc in four ( 19% ) out of 21 cases : clinical and us findings of this subgroup are reported in table 2 . 
in 17 ( 81% ) of 21 cases , a mammographic finding was present ( table 3 )  . all 21 patients had sonographic examination , the results of which are given in table 4 . 
in seventeen of 21 cases , a mammographic abnormality corresponded to the sonoto mr indicante regioni di impregnazione contrastografica significativa , con informazioni sulla cinetica di impregnazione e sullestensione dellarea in cui questa si verifica . infine , il medico radiologo pu selezionare unarea di impregnazione significativa consentendo al programma di generare automaticamente una sinossi del volume totale della lesione , incluse le percentuali della lesione che mostrano impregnazione con cinetica wash - out , plateau e persistente . quando una lesione stata selezionata dal medico radiologo , questa informazione generata dal programma completamente automatica [ 26 ]  . tutte le pazienti sono state sottoposte ad intervento chirurgico dopo leffettuazione dellindagine mr . 
in one of these four cases , the first sonographic evaluation was negative , and only a second us examination , performed with knowledge of the mri results , was positive . 
these findings were confirmed at pathological examination . classificate come unifocali , multifocali , localizzate ad un singolo quadrante o a pi quadranti , utilizzando la terminologia gi descritta sopra . i reperti morfologici descritti su mammografia , ecografia e mr e la evidenza di malattia unifocale o multifocale , localizzata ad uno o pi quadranti , monoo bilaterale sono stati confrontati con i risultati dellindagine istologica utilizzata come gold standard . risultati tredici pazienti presentavano reperti palpatori sospetti allindagine clinica . 
otto donne non presentavano allesame clinico alcun reperto sospetto . le densit mammografiche riportate dei 21 casi sono state : pressoch interamente adiposa ( d1 ) ( n = 10 ) , densit fibroghiandolare sparsa ( d2 ) ( n = 6 ) , eterogeneamente densa ( d3 ) ( n = 4 ) , estremamente densa ( d4 ) ( n = 1 )  . 
nel sottogruppo di 10 pazienti con mammelle pressoch totalmente adipose , 3 non presentavano reperti clinici significativi , 2 erano portatrici di una massa palpabile , 3 presentavano radiol med ( 2008 ) 113 : 11101125 1117 table 5 correlation between positive ( 17 / 21 ) mammographic findings and breast densities mammographic finding breast density increased density increased density increased density 1 opacity 3 opacity 6 distortion 7 microcalcifications 8 opacity 9 opacity 10 distortion 11 distortion 12 increased density 13 opacity with microcalcifications 14 opacity 15 opacity 16 increased density 17 opacity 1 opacit 2 aumento della densit 3 opacit 4 aumento della densit 5 aumento della densit 6 distorsione 7 microcalcificazioni 8 opacit 9 opacit 10 distorsione 11 distorsione 12 aumento della densit 13 opacit associata a microcalcificazioni 14 opacit 15 opacit 16 aumento della densit 17 opacit tabella 5 correlazione tra reperti mammografici sospetti ( 17 / 21 ) e densit mammografiche reperto mammografico densit mammografica accuracy of computer - defined significant enhancement twenty lesions showed significant enhancement at the 100% threshold . 
all 20 enhancing lesions exhibited a significant degree of washout of contrast material . incremento di consistenza alla palpazione senza massa palpabile , una presentava un incremento di consistenza alla palpazione con retrazione del capezzolo , una presentava incremento di consistenza alla palpazione con retrazione del capezzolo e ispessimento cutaneo ; lecografia sempre risultata positiva in questo sottogruppo di donne ( tabella 1 )  . la mammografia effettuata prima di qualsiasi accertamento invasivo non stata in grado di identificare ilc in 4 ( 19% ) dei 21 casi : i reperti clinici ed ecografica di questo sottogruppo sono riportati in tabella 2 . 
in 17 ( 81% ) dei 21 casi , era invece presente un reperto mammografico sospetto ( tabella 3 )  . tutte le 21 pazienti sono state sottoposte ad ecografia del seno , i cui risultati sono riassunti nella tabella 4 . 
in 4 casi su 21 il reperto mammografico risultato negativo , a fronte di un reperto ecografico sospetto ; le densit mammografiche di queste 4 donne con mammografia negativa sono risultate essere , rispettivamente , d3 ( 2 casi ) e d1 ( due casi ) ; in uno di questi 4 ultimi casi la prima ecografia risultata negativa e solo una seconda ecografia effettuata alla luce del reperto mr risultata positiva . 
le dimensioni istopatologiche delle lesioni sono risultate essere da 0 , 4 a 3 , 3 cla dimensione media delle neoplasie risultata essere 1 , 56 cm . diciotto carcinomi della mammella sono stati descritti dalla rm come unifocali , 2 come multifocali , uno come multicentrico , rispetto a quanto emerso dalle indagini di diagnostica per immagini tradizionali : questi reperti sono stati confermati allindagine anatomo - patologica . accuratezza della definizione di impregnazione contrastografica significativa fornita dal software venti lesioni maligne hanno mostrato significativa impregnazione contrastografica utilizzando la soglia del 100% di incremento della intensit di segnale ( si ) nel primo minuto . una sola lesione non ha raggiunto la soglia del 100% nel primo minuto , con questo non rendendosi possibile la analisi automatica di tale lesione da parte del software . 
tutte queste 20 lesioni dotate di significativa impregnazione contrastografica nel primo minuto sono risultate dotate di significativa dismissione del mezzo di contrasto stesso . due radiologi hanno descritto , raggiungendo il consenso dopo discussione dei casi dubbi , la morfologia delle lesioni in mr . 
immagine rm coronale sottratta fast field echo ( tr / te , 19 / 10 ) che dimostra unarea di impregnazione contrastografica a margini irregolari ( pattern 1 )  . the two radiologists reached overall consensus in lesion description on breast mri . 
in eight women ( 40% ) , mri revealed additional findings , none of which were confirmed by us examination . five women underwent modified radical mastectomy and 16 underwent quadrantectomy . 
la rm ha rivelato in 8 donne ( 40% ) reperti aggiuntivi rispetto alle indagini tradizionali , nessuno dei quali stato confermato dalla verifica ecografica . cinque donne sono state sottoposte a mastectomia radicale modificata secondo madden , 16 donne sono state sottoposte a quadrantectomia . 
immagine rm coronale sottratta ffe ( tr / te , 19 / 10 ) che dimostra la presenza di multipli foci di impregnazione contrastografica connessi tra loro ( pattern 3 )  . clinica e per le metodiche diagnostiche convenzionali , risultando perci inferiore la sensibilit diagnostica rispetto a quanto accade per il carcinoma duttale invasivo ( idc )  . 
la maggior parte di questi tumori sono identificati come incrementi di densit senza margini ben definiti , incluse le distorsioni architetturali del parenchima , o come masse di elevata densit con margini irregolari . 
il tasso di mammografie interpretate come falsamente negative in donne portatrici di ilc , spesso caratterizzate dalla presenza di elevata densit radiografica delle mammelle , riportato oscillare tra il 16% ed il 43% [ 8 , 9 , 28 , 3134 ]  . 
noi abbiamo riscontrato , nelle 4 mammografie falsamente negative , 2 casi con d3 e 2 casi con d1 . i benefici dellindagine ecografica associata alla mammografia , nella diagnosi di ilc , sono variabili . 
alcuni autori hanno affermato che lecografia migliora significativa1120 radiol med ( 2008 ) 113 : 11101125 mente il tasso di identificazione del ilc in pazienti che si presentano con noduli palpabili e mammografia negativa [ 5 , 10 , 35 , 36 ]  . 
altri autori hanno osservato che lecografia riveste un ruolo limitato nelle pazienti affette da ilc per la variet di presentazione ecografica di questultimo e per le basse sensibilit e specificit proprie della metodica nella diagnosi dei piccoli tumori [ 16 , 37 ]  . 
nel presente studio lecografia ha fornito informazioni aggiuntive in tutti i 4 casi di ilc con mammografia negativa : ha messo in evidenza una massa mal definita in 2 casi , uno sbarramento acustico in 1 caso , una massa a contorni ben definiti in 1 caso . i limiti riscontrati sia nellecografia che nella mammografia hanno contribuito ad aumentare linteresse nei confronti della mr della mammella , la quale attualmente sta assumendo un ruolo sempre pi importante nella gestione della patologia mammaria [ 19 , 38 , 39 ]  . 
 [ 24 ] hanno descritto questo pattern in dodici di 26 , dieci di 18 , 19 di 20 , 4 di 13 e 8 di 20 casi , rispettivamente . 
il secondo pattern pi comune da noi riscontrato consistito in una massa a margini netti : non stato possibile trovare altre conferme al nostro riscontro , come recentemente descritto dal nostro gruppo [ 41 ]  . 
 [ 40 ] , i setti dotati di impregnazione contrastografica in assenza di una massa dominante menzionati da quayyum [ 17 ] , n limpregnazione regionale e distorsione architetturale descritte da weinstein et al . 
i tassi di identificazione di carcinoma multifocale o multicentrico rilevato alla mr ma occulto a ecografia e mammografia oscillano tra 16% e 37% [ 19 , 43 , 46 ]  . 
lindagine anatomo - patologica su pezzo operatorio eseguita dopo quadrantectomia ha dimostrato la presenza di un carcinoma lobulare invasivo del diametro massimo di 1 , 1 c table 7 patterns of t2 - weighted signal intensity on magnetic resonance imaging ( mri ) in 20 mr - detectable invasive lobular carcinomas t2 signal homogeneously hypointense homogeneously mildly hyperintense nonhomogeneously hyperintense nonhomogeneously hypointense tabella 7 patterns t2 in 20 ilc visibili in rm segnale nelle sequenze t2 - pesate omogeneamente ipointenso omogeneamente teneuemente iperintenso disomogeneamente iperintenso disomogeneamente ipointenso discussion ilc often presents with diagnostic difficulties on clinical examination and conventional imaging , resulting in lower sensitivities for ilc than for invasive ductal carcinomas ( idc )  . 
most tumours are identified either as an asymmetric density without definable margins , including architectural distortion , or as a high - density mass with spiculated radiol med ( 2008 ) 113 : 11101125 1121 margins . 
the rate of false - negative mammographic interpretation of ilc , often associated with increased breast parenchyma , has been reported to be in the range of 16%43% [ 8 , 9 , 28 , 3134 ]  . 
we found breast densities d3 ( two cases ) and d1 ( two cases ) in the four negative mammograms . results of breast us as an adjunct to mammography in diagnosing ilc are variable . 
some investigators found that us significantly improved the detection of ilc in patients presenting with palpable nodules and no mammographically detected masses [ 5 , 10 , 35 , 36 ]  . 
others found that us had a limited role in ilc because of the variety of us appearances and a very low sensitivity and specificity for the diagnosis of small cancers [ 16 , 37 ]  . 
in our study , us revealed additional information in all four cases with negative mammograms : us demonstrated an ill - defined mass in two cases , an area of shadowing in one case and a discrete mass in one case . the limitations of mammography and us have prompted considerable interest in mri of the breast , which is now playing an increasingly important role in the management of breast disease [ 19 , 38 , 39 ]  . 
immagine rm coronale t2 pesata turbo spin echo ( tr / te , 3800 / 140 ) che mostra unarea disomogeneamente ipointensa ( freccia )  . centricit e bilateralit del ilc la mr della mammella raccomandata per valutare la reale estensione di malattia prima dellopzione chirurgica [ 4 , 12 , 14 , 16 , 4347 ]  . 
 [ 1 ] , mr ha definito lestensione del tumore pi accuratamente di quanto non stato possibile fare con le metodiche convenzionali in 16 su 32 pazienti . harms [ 19 ] ha descritto come in una serie di 47 tumori mammari maligni tutti i cinque ilc sono stati ben 1122 radiol med ( 2008 ) 113 : 11101125 termine the extent of cancer within the breast more accurately than can be accomplished with conventional methods [ 4 , 16 , 19 , 4246 ]  . 
the reported rates of multifocal or multicentric cancer , detected on mri but occult on us and mammography , range from 16% to 37% [ 19 , 43 , 46 ]  . 
 due to the high rate of multicentricity and bilaterality of ilc , breast mri can be performed to assess the extent of disease before treatment planning [ 4 , 12 , 14 , 16 , 4347 ]  . 
for dynamic breast mri , t2 - weighted sequences have not been attributed a major role , and a t2 - weighted pulse sequence is , for the most part , considered optional . three reports [ 5153 ] have addressed the issue of t2weighted images and concluded that t2 - weighted sequences are not useful for differential diagnosis in breast mri . 
the results of another study [ 54 ] showed that in nonfat - suppressed t2 - weighted tse pulse sequences , fibroadenomas tend to demonstrate different signal intensities ( a significant difference between the prevalence of high si and low si lesions in breast cancers and fibroadenomas )  . 
therefore , in practice , if a well - circumscribed enhancing lesion is detected in breast mri , a high si in the corresponding t2weighted tse image could be used to support the diagnosis of a benign lesion . in contrast with this report , we found , among 20 enhancing ilc , the contemporary presence of hypoand hyperintense lesions on t2 - weighted tse images . 
because of the histological features in ilc , perifocal fibrosis , dense cellularity and / or a high nucleus - to - plasma ratio may dimostrati dalla mr e le loro dimensioni sono state valutate con accettabile accuratezza . 
in ogni caso , questi reperti falsi negativi sono stati riscontrati in pazienti che avevano subito una biopsia escissionale prima delleffettuazione della mr . noi abbiamo descritto una paziente con un ilc unifocale identificato come massa allecografia , ma occulto allesame clinico , alla mammografia ed alla mr ; questa paziente stata sottoposta a fnac ecoguidato con referto citologico c1 i.e. 
inadeguato [ 50 ] e successivamente a microbiopsia escissionale ecoguidata , con esito di carcinoma invasivo : il reperto anatomopatologico sul pezzo operatorio ha dimostrato la presenza di un ilc di 1 , 1 cm . la possibilit di differenziare mediante la mr dinamica mammaria le lesioni benigne dalla maligne basata quasi completamente sulla modalit di impregnazione contrastografica e sulla morfologia delle lesioni ; nel campo della mr dinamica mammaria le sequenze t2 pesate non hanno acquisito grande importanza ; una sequenza t2 pesata ritenuta dalla maggior parte degli autori opzionale , non funzionale alla diagnosi differenziale . 
tre pubblicazioni [ 5153 ] si sono occupate del tema delle immagini t2 pesate , concludendo che le sequenze pesate in t2 non forniscono informazioni utili alla diagnosi differenziale delle lesioni . 
i risultati di un altro studio [ 54 ] hanno mostrato come , nelle sequenze turbo spin echo t2 pesate senza soppressione del grasso , i fibroadenomi hanno la tendenza a manifestare differenti intensit di segnale ( esiste una significativa differenza tra la prevalenza di intensit di segnale elevate e basse fra carcinomi e fibroadenomi ) cosicch , in pratica , se viene rilevata dalla mr una lesione dotata di impregnazione contrastografica con bordi netti , il dato di un elevato segnale nella corrispondente sequenza t2 pesata potrebbe esser utilizzato a supporto della diagnosi di benignit della lesione stessa . in contrasto con questo dato , nel nostro studio abbiamo riscontrato , nel gruppo dei 20 ilc dotati di significativa impregnazione contrastografica , la presenza contemporanea di lesioni ipoed iperintense nelle sequenze t2 pesate . 
potrebbero essere le peculiarit istologiche del ilc , cio fibrosi perifocale , densa cellularit e / o elevato rapporto nucleo / citoplasma , ad essere responsabili del basso segnale nelle sequenze t2 pesate rispetto al parenchima mammario normale . 
dallaltra parte , le procedure di diagnostica invasiva ( fnac , microbiopsia con metodo tru - cut , microbiopsia vacuum - assisted ) possono essere responsabili di edema , emorragia locale e necrosi determinanti lincremento dellintensit di segnale nelle sequenze t2 pesate . radiol med ( 2008 ) 113 : 11101125 1123 contribute to the particularly low signal on t2 - weighted tse images with respect to the normal parenchyma . 
on the other hand , the diagnostic invasive procedures performed on many of these lesions before mri ( fnac , tru - cut microbiopsy , vab ) may be responsible for oedema , local haemorrhage and necrosis and subsequent increment of t2weighted si . 
a large prospective study is needed to confirm our findings and those published earlier . conclusions in conclusion , the most frequent feature of ilc seen on mri is a spiculated inhomogeneous mass , and the second feature in frequency is a mass with smooth margins . 
even if the diagnosis of ilc is difficult , use of all available techniques and the clinical examination itself may be helpful for detecting and characterising this neoplasmri may play an important role in evaluating multifocal or multiquadrant locations , but palpation , mammography and us remain of great value . 
the combination of approaches could lead to a correct diagnosis and the appropriate choice of therapeutic options . una limitazione del nostro studio consiste nel fatto che i radiologi che hanno rivisto le immagini mr erano al corrente della diagnosi istologica delle pazienti : essi erano al corrente della presenza di ilc in tutte le 21 donne , fatto che pu aver influenzato la loro interpretazione delle immagini mr . 
 conclusioni in conclusione , laspetto morfologico di ilc da noi pi frequentemente riscontrato in mr costituito da una massa disomogenea a bordi irregolari ; la seconda modalit di presentazione , in ordine di frequenza , costituita da una massa con bordi netti . 
la mr pu rivestire un ruolo importante nella valutazione della presenza di malattia a distribuzione multifocale o multicentrica , ma la palpazione , la mammografia e lecografia mantengono un valore fondamentale . 
biopsies were obtained in patients with no known primary cancer ( 75 )  . kyphoplasty was performed in 39 patients with magerl type a1 and a3 fractures within 3 months from the trauma . a bipedicular approach was used in all cases . 
in patients treated with vertebroplasty , success rates at 2472 h were 90% for osteoporotic fractures , 100% for vertebral haemangiomas and 77% for metastatic fractures . extravertebral vascular or discal leakage of cement occurred in 39 patients , but only two of them reported radicular pain due to epidural involvement . 
la biopsia stata eseguita nei casi di lesioni dubbie ( 75 pazienti ) , senza lesione primitiva nota . trentanove pazienti , affetti da frattura vertebrale traumatica tipo a1 e a3 secondo magerl , sono stati sottoposti a kp entro 3 mesi dal trauma . 
nei pazienti sottoposti a vp , nel giro di 2472 h , abbiamo riscontrato un successo della procedura nel 90% dei crolli porotici , nel 100% di quelli angiomatosici e nel 77% di quelli neoplastici . 
entrambe le metodiche sono valide nel management delle sindromi antalgiche vertebrali . 1172 radiol med ( 2008 ) 113 : 11711184 kyphoplasty is suggested in acute traumatic fractures of type a1 and a3 according to magerl , as it allows recovery of vertebral stability and a better distribution of the cement . keywords vertebral fractures vertebroplasty kyphoplasty secondo la nostra esperienza e i nostri risultati , riteniamo che , a fronte delle differenze tecniche ed economiche delle due metodiche , il ricorso alla vp nei crolli porotici , angiomatosici aggressivi e neoplastici , pi indicato per la rapida esecuzione e minore invasivit . 
la kp , invece , preferibile nelle fratture vertebrali recenti tipo magerl a1 e a3 , per la caratteristica di ripristino della statica vertebrale e per una migliore distribuzione del cemento nel metamero fratturato . parole chiave fratture vertebrali vertebroplastica cifoplastica introduction introduzione vertebroplasty and kyphoplasty , new techniques for treating vertebral - body fractures , have generated much interest in recent years . 
both techniques are based on the assumption that the percutaneous injection of acrylic material into the vertebral body is capable of stabilising the fractured vertebra and relieving vertebral pain . vertebroplasty was first described by galibert and deramond and coworkers [ 1 ] , a french neurosurgeon and a french radiologist who published a technical note on the treatment of vertebral haemangiomas in the journal neurochirurgie in 1987 . 
although the french investigators deserve all credit for introducing the technique , it was the rigourous methodological approach later adopted by the north american authors that led to its success and popularity [ 36 ]  . 
 in the usa , the estimated prevalence of osteoporotic vertebral compression fractures is approximately 700 , 000 cases annually , although the figure is probably underestimated due to underreporting of the condition in the elderly [ 7 , 8 ]  . the prevalence in europe is 438 , 750 per annum , equal to 117 cases in 100 , 000 [ 9 ]  . 
among women older than 50 years , the prevalence is 26% , and it increases to approximately 40% in women older than 80 years [ 9 , 10 ]  . kyphoplasty was developed as a modification of vertebroplasty . 
first performed in california in 1998 [ 11 ] , it consists in delivering polymethylmethacrylate ( pmma ) or other types of cement into the fractured vertebral body under fluoroscopic guidance after the cancellous bone has been compacted with dedicated balloon tamps . 
the goal is to combine the analgesic and vertebral consolidation effect of nel corso degli ultimi anni hanno suscitato notevole interesse due nuove modalit di trattamento per le fratture da crolli vertebrali : la vertebroplastica ( vp ) e la cifoplastica ( kp )  . 
il presupposto fondamentale di entrambe le metodiche che con tecnica percutanea miniinvasiva , attraverso il peduncolo , si introduce nel soma vertebrale materiale acrilico rendendo cos stabile la vertebra fratturata con conseguente effetto positivo sul sintomo dolore . la vertebroplastica fu descritta per la prima volta nel 1987 da galibert e deramond [ 1 ] , rispettivamente neurochirurgo e radiologo francese che pubblicarono sulla rivista di neurochirurgie delle note tecniche per il trattamento degli emangiomi vertebrali . 
agli autori francesi va certamente il merito di aver iniziato questo tipo di trattamento mentre agli autori statunitensi , che lapplicarono in seguito , bisogna riconoscere un approccio metodologico rigoroso nellidentificazione dei meccanismi alla base del successo del trattamento nonch della diffusione della tecnica [ 36 ]  . 
 negli usa , lincidenza annuale di fratture vertebrali da osteoporosi stimata essere intorno ai 700000 casi , sebbene questo numero sia probabilmente sottostimato rispetto alla reale incidenza per unattenzione limitata a questo tipo di patologia nella popolazione pi anziana [ 7 , 8 ]  . 
nelle donne di et superiore ai 50 anni lincidenza di crolli porotici stata stimata essere del 26% , radiol med ( 2008 ) 113 : 11711184 1173 vertebroplasty with restoration of the physiological height of the collapsed vertebral body , with resulting normal vertebral statics and biomechanics . 
the aim of this study was to compare vertebroplasty and kyphoplasty by illustrating the two techniques , analysing their results , and discussing their indications in relation to the type of fracture . materials and methods patients between april 2001 and december 2006 , we performed vertebroplasty on 805 vertebrae in 485 patients ( 282 women , 205 men ; mean age 59 years ) affected by osteoporosis ( 310 ) , vertebral metastasis ( 160 ) and vertebral haemangioma ( 15 )  . 
thirty - nine patients ( 32 men and seven women ; mean age 42 years ) were treated with kyphoplasty for type a1 ( 30 ) and a3 ( 9 ) traumatic vertebral fractures according to magerls classification [ 20 ]  . all vertebroplasty procedures were performed with the patient in the prone position . 
biopsy was performed in 75 patients with no known primary cancer and equivocal computed tomography ( ct ) or magnetic resonance imaging ( mri ) findings . procedures were performed under local anaesthesia combined with neuroleptanalgesia ; no patient received general anaesthesia . all kyphoplasty procedures were performed with the patient in the prone position . 
thirty - one patients received general anaesthesia , whereas only eight received local neuroleptanalgesia based on the type of traumatic fracture . patient selection : inclusion criteria patients were considered eligible for vertebroplasty or kyphoplasty if they had intense , nonradicular , midline vertebral pain , strongly exacerbated by palpation of the spinous process of the affected vertebra and refractory to conventional medical treatment ( bracing and bed rest )  . 
patients were eligible for kyphoplasty if they had sustained a traumatic vertebral fracture ( accidental / domestic ) of type a1 and a3 according to magerl no more than 3 months before the procedure to allow correct expansion of the kyphotic vertebra and better and safer cement distribution . con tendenza ad aumento con let , raggiungendo circa il 40% in donne con et superiore agli 80 anni [ 9 , 10 ]  . sulla base del successo ottenuto dalla vp , si sviluppata poi la kp . 
la cifoplastica , effettuata per la prima volta nel 1998 in california da reiley [ 11 ] , consiste nella introduzione di polimetilmetacrilato ( pmma ) , o altri tipi di cemento , allinterno dei corpi vertebrali fratturati sotto guida fluoroscopica , previa distensione della spongiosa mediante cateteri a palloncino dedicati . 
in tale modo si cerca di unire alleffetto antalgico e di consolidamento del soma fratturato proprio della vp , il ripristino della fisiologica altezza del soma collassato , ristabilendo la normale statica e biomeccanica vertebrale . 
 negli ultimi 15 anni il successo ottenuto con tali tecniche ha permesso lampliamento delle indicazioni alle sindromi vertebrali dolorose , non rispondenti alla terapia conservativa [ 6 , 1219 ]  . 
scopo di questo lavoro quello di mettere a confronto le due metodiche , illustrando la tecnica , analizzandone i risultati e confrontando le indicazioni della loro esecuzione sulla base del tipo di frattura . materiali e metodi pazienti dallaprile 2001 al dicembre 2006 , 485 pazienti ( 282 donne , 205 uomini ; et media 59 anni ) sono stati sottoposti a vp per un totale di 805 metameri , cos distribuiti : 310 trattati per osteoporosi ; 160 trattati per metastasi vertebrali ; 15 trattati per angioma . 
trentanove pazienti ( 32 uomini e 7 donne ; et media 42 anni ) sono stati sottoposti a kp , in quanto affetti da frattura vertebrale traumatica di tipo a1 e a3 secondo la classificazione di magerl [ 20 ] , cosi distribuite : 30 fratture tipo a1 secondo magerl ; 9 fratture tipo a3 secondo magerl . nei pazienti sottoposti a vp , stato seguito un approccio monopeduncolare in 365 pazienti e bipeduncolare in 120 pazienti , a paziente prono . 
abbiamo preferito un approccio trans - peduncolare nel trattamento di vertebre lombari e dorsali basse , mentre nel trattamento di crolli dorsali alti abbiamo preferito un approccio pi laterale , di tipo intercosto - trasversario . 
tutte le procedure di vp sono state eseguite in anestesia locale utilizzando la neuroleptoanalgesia ; in nessun caso stato necessario praticare anestesia generale . tutte le procedure di kp sono state eseguite con approccio trans - peduncolare bilaterale a paziente prono . 
in 31 casi abbiamo preferito lanestesia generale , mentre in soli 8 casi abbiamo optato per la neuroleptoanalgesia locale sulla base del tipo di frattura traumatica . 1174 radiol med ( 2008 ) 113 : 11711184 patient selection : absolute exclusion criteria selezione dei pazienti : criteri di inclusione absolute exclusion criteria were : ( 1 ) asymptomatic vertebral fractures ; ( 2 ) diffuse , nonfocal pain without mri evidence of altered trabecular - bone signal ; ( 3 ) systemic or local infections ; ( 4 ) uncorrectable coagulation disorders ; ( 5 ) osteoblastic tumours . patient selection : relative exclusion criteria relative exclusion criteria were : ( 1 ) radicular or medullary involvement ; ( 2 ) complete loss of vertebral height ( vertebra plana ) ; ( 3 ) interruption of the posterior vertebral margin or pedicles . diagnostic imaging diagnostic workup was aimed at selecting the most appropriate treatment . 
this was followed by mri to define the nature of the vertebral fracture and establish the vertebral level on the basis of increased t2 - weighted and short tau inversion recovery ( stir ) signals corresponding to bone marrow oedema . 
once the type and nature of the vertebral fracture had been established , we opted for vertebroplasty , the less invasive and expensive technique , in all patients affected by vertebral fractures due to osteoporosis , metastasis and haemangiomas , and wee reserved kyphoplasty for those affected by type a1 and a3 traumatic vertebral fractures according to magerl . 
fluoroscopic guidance was used in patients with osteoporosis ( 310 ) and vertebral haemangioma ( 15 ) , whereas in those with metastatic lesions ( 160 ) , we preferred ct associated with a portable c - arm , as it allowed for an easier approach and more precise placement of the needle in the osteolytic area . 
all kyphoplasty procedures were performed with fluoroscopic guidance . patients were evaluated on the basis of a visual analogue scale ( vas ) and the oswestry disability index ( odi ) before the procedure and at 1 , 3 and 6 months . vertebroplasty : technique after obtaining a radiographic image in which the upper and sono stati considerati eleggibili di un trattamento di vp o kp i pazienti che presentavano un dolore vertebrale intenso , non radicolare , localizzato lungo la linea mediana , fortemente evocato alla manovra di digito - pressione sullapofisi spinosa del soma crollato e resistente alle comuni terapie mediche convenzionali ( ortesi a riposo )  . 
abbiamo considerato eleggibili di kp i pazienti con frattura somatica traumatica ( accidentale / domestica ) tipo a1 e a3 secondo magerl , entro 3 mesi dal trauma , al fine di determinare una corretta espansione del soma cifotizzato e per una migliore e pi sicura distribuzione del cemento . selezione dei pazienti : criteri di esclusione assoluta sono stati esclusi pazienti : ( 1 ) portatori di fratture vertebrali asintomatiche ; ( 2 ) con dolore diffuso , non focale , con esame rm negativo per alterazione di segnale della spongiosa ; ( 3 ) affetti da uninfezione sistemica o locale ; ( 4 ) affetti da disturbi della coagulazione non correggibili ; ( 5 ) affetti da lesioni neoplastiche di tipo osteoblastico . selezione dei pazienti : criteri di esclusione relativa ( 1 ) pazienti con una sofferenza radicolare o midollare ; ( 2 ) pazienti con il collasso completo del metamero ( vertebra plana ) ; ( 3 ) pazienti con interruzione dellintegrit del muro posteriore o dei peduncoli vertebrali . diagnostica per immagini liter diagnostico finalizzato alla scelta del tipo di trattamento da eseguire ha previsto come esame di primo livello quello di radiologia tradizionale per lidentificazione dellalterazione strutturale del soma vertebrale . 
seguito poi un esame di rm per una corretta diagnosi di natura del crollo e per stabilire il soma sofferente , denunciato dalliperintensit di segnale nelle sequenze pesate in t2 e stir corrispondente alledema intra - spongioso . 
stabilito quindi il tipo e la natura della frattura somatica , abbiamo optato per il trattamento di vp , meno aggressivo e costoso , per tutti i pazienti affetti da crolli porotici , metastatici e angiomatosici ; riservando il trattamento di kp unicamente ai pazienti affetti da fratture traumatiche di tipo a1 e a3 secondo magerl . la metodica di vp stata eseguita a diversi livelli sino ad un massimo di sei metameri in 8 pazienti ed stata condotta sotto guida fluoroscopia nei pazienti affetti da osteoporosi ( 310 pazienti ) e da angioma vertebrale ( 15 pazienti ) ; radiol med ( 2008 ) 113 : 11711184 1175 lower endplates were perfectly aligned and the spinous processes were projected in midline , the pedicle was approached with an 11or 13 - gauge bevelled needle between 10 and 15 cm long , with side wings to facilitate rotation . once inside the pedicle , the needle was advanced to the anterior third of the vertebra and the cement injected into the body . 
the amount of cement used ranged from 2 to 4 ml for thoracic vertebrae treated with unipedicular approach , to 5 to 6 ml for dorsolumbar vertebrae and 12 ml for lumbar vertebrae . kyphoplasty : technique unlike vertebroplasty , kyphoplasty is always performed with a bilateral transpedicular approach and the patient in prone position . 
after a 1 - cm skin incision extending to the muscle fascia was made to facilitate insertion of the trocar needle , the 11 - gauge needle was advanced at an oblique angle into the pedicle under fluoroscopic guidance . 
a kirschner wire was then introduced coaxially to the needle to serve as a guide for the working cannula , which was driven up to 3 mm beyond the posterior wall of the vertebral body . 
a small hand - mounted drill was used to create a bone channel , with the distal end a few millimetres from the anterior cortical margin to allow insertion of the balloon into the vertebral body . 
the same procedure was carried out through the contralateral pedicle . once inside the vertebra , the balloon catheters were simultaneously inflated with a mixture of contrast material , under continuous fluoroscopic and manometric monitoring . they were then deflated and removed , and the same working cannula was used as a route for pmma delivery into the newly created cavity . 
often , the cement volume was approximately 12 cc greater than the final inflation volume to allow the central bolus to interdigitate with the surrounding cancellous bone . results vertebroplasty the results of vertebroplasty in the 485 patients , divided by condition causing the symptoms , are shown in table 1 . 
the best results were seen in patients with mentre nei casi di lesioni litiche di origine metastatica ( 160 pazienti ) lutilizzo della tc associata ad un arco c portatile ha permesso un pi facile approccio e preciso posizionamento dellago nellarea di osteolisi . 
tutte le procedure di kp sono state eseguite sotto guida fluoroscopica . i pazienti sono stati valutati prima e dopo il trattamento a 1 , 3 e 6 mesi con il metodo visual analogyc scale ( vas ) e oswestry disability scale ( ods )  . tecniche di esecuzione della vp una volta ottenuta unimmagine radiografica in cui le limitanti somatiche superiori e inferiori del soma risultavano perfettamente sovrapponibili e le apofisi spinose proiettate sulla linea mediana , si proceduto allapproccio del peduncolo vertebrale mediante un ago da 11 g o 13 g , di una lunghezza variabile da 10 cm a 15 cm , con estremit a becco di flauto e munito di alette laterali per facilitarne la rotazione . 
la quantit di cemento iniettata nei pazienti sottoposti a vp stata variabile da un minimo di 24 ml per metameri dorsali con approccio mono - peduncolare sino a 56 ml a livello dorso - lombare e 12 ml a livello lombare . tecnica di esecuzione della kp differentemente dalla vertebroplastica , la cifoplastica prevede sempre accessi trans - peduncolari bilateralmente a paziente prono . 
sotto guida fluoroscopica lago da biopsia ossea da 11 g stato fatto avanzare nel peduncolo vertebrale con uninclinazione idonea dopo incisione cutanea di circa 1 cm estesa alla fascia muscolare per favorire lingresso del trokar . 
successivamente , coassialmente allago , si inserito lago di kirshner che stato utilizzato come guida per far scorrere fino a 3 mm oltre il muro posteriore del corpo vertebrale una cannula di servizio . 
 stato creato quindi mediante un piccolo trapano a mano un canale osseo intraspongioso con estremo distale a pochi millimetri dal margine corticale anteriore per consentire linserimento del catetere a palloncino allinterno del corpo vertebrale fratturato . 
la medesima procedura stata eseguita attraverso il peduncolo controlaterale . una volta posizionati allinterno del soma fratturato entrambi i cateteri a palloncino dedicati , si proceduto al loro simultaneo e progressivo gonfiaggio mediante una miscela di mdc sotto continuo controllo fluoroscopico e manometrico . 
il cemento stato rilasciato lentamen1176 table 1 vertebroplasty results osteoporosis haemangiomas secondary lesions success 90% failure 10% success 100% failure 0% success 77% failure 23% radiol med ( 2008 ) 113 : 11711184 te a bassa pressione e sotto continua guida fluoroscopica in ll in quantit variabile da 4 ml a 6 ml a metamero in funzione del volume finale raggiunto dal catetere a palloncino gonfiato nel soma fratturato e visualizzato sul display del sistema di gonfiaggio . 
1a , b rm sagittale stir e t2w : iperintensit visibile solo nella sequenza sagittale pesata in stir come da edema della spongiosa dei somi l1 e l3 ; c , d controllo dopo vp di l1 , l2 e l3 : buono il riempimento somatico . radiol med ( 2008 ) 113 : 11711184 1177 fig . 
e esame in ll dopo vp , piccola fuga di cemento asintomatica a livello del forame sinistro di l4 . extravertebral cement leakage into the vascular system or intervertebral disc occurred in 39 patients . 
nel follow - up , nei soli pazienti affetti da osteoporosi abbiamo riscontrato fratture di vertebre adiacenti in 25 pazienti e nuove fratture di vertebre a distanza da quella gi trattata in 19 pazienti . radiol med ( 2008 ) 113 : 11711184 1178 fig . 
nella tabella 2 sono riportati i risultati dei 39 pazienti trattati suddivisi in base alla tipo di frattura valutando il dolore prima e dopo il trattamento secondo la valutazione con i metodi vas e ods . 
a controllo in ll sotto scopia del corretto posizionamento dei trokar con approccio bi - peduncolare e dilatazione dei palloncini ; b , c controllo post trattamento kp in ll e ap con buona la distribuzione del cemento e visibilit di peduncoloplastica ; d ricostruzione mpr sagittale del soma trattato con kp e peduncoloplastica . table 2 kyphoplasty results discussione magerl a1 fractures magerl a3 fractures success 95% failure 5% success 90 % failure 10 % tabella 2 risultati della cifoplasica fratture a1 secondo magerl frattura a3 secondo magerl successo 95% insuccesso 5% successo 90% insuccesso 10% le differenze tecniche dei due trattamenti possono essere cosi riassunte : entrambe richiedono lutilizzo costante della guida rxscopica ( apparecchio angiografico o arco a c portatile ) per il corretto posizionamento degli aghi di accesso al corpo vertebrale da trattare ; la procedura di vp viene eseguita in anestesia locale associata a neuroleptoanalgesia ; differentemente la tecnica di kp viene eseguita preferibilmente in anestesia generale , poich maggiormente invasiva e dolorosa ; lapproccio per la vp pu essere bi - peduncolare o mono - peduncolare se lago utilizzato viene posizionato nel 1180 radiol med ( 2008 ) 113 : 11711184 techniques vertebroplasty and kyphoplasty may be summarised as follows : both require constant fluoroscopic monitoring ( angiographic equipment or portable c - arm ) to ensure correct needle position vertebroplasty is performed under local anaesthesia associated with neuroleptanalgesia , whereas kyphoplasty , which is more invasive and painful , is preferably performed under general anaesthesia the approach in vertebroplasty may be bipedicular or unipedicular , with the needle in the midline of the fractured vertebra ; in kyphoplasty , instead , to achieve reexpansion of the vertebra , the approach is necessarily bipedicular , with trocars mounting inflatable balloon tamps in both techniques , the medial wall of the pedicle should never be crossed before reaching the posterior wall of the vertebra , as confirmed on posteroanterior and lateral views both techniques employ pmma . 
for kyphoplasty , however , new cements such as calcibon or tricalcium phosphate / hydroxyapatite can be used to extend the indications to young subjects with recent traumatic fractures the only absolute contraindication is the presence of local or systemic infections reported complications are similar . 
however , the risk of cement leakage during kyphoplasty is lower because the newly created cavity has the effect of containing the cement , the cavity is filled a low pressure , the cement is highly viscous and the volume of cement is predetermined on the basis of the volume of the fully inflated balloon tamp . 
the rationale for the two techniques is that pmma injection into the vertebral body immobilises the vertebral microfractures responsible for pain , thus making the vertebral body more compact and resistant . vertebroplasty is most commonly used to treat osteoporotic vertebral fractures , achieving pain relief in 90%95% of cases [ 21 ]  . 
eligible secondary lesions are osteolytic or mixed lesions , usually secondary to breast cancer ( 30% ) and lung cancer ( 25% ) [ 4 ] , in which symptoms are alleviated in 70%90% of cases . 
recent studies have suggested that the use of pmma in cancer patients has an additional antitumoral effect resulting from the exothermic soma fratturato sulla linea mediana , tale da permettere una distribuzione simmetrica del pmma ; differentemente nella kp , ai fini di ottenere la riespansione del soma , lapproccio necessariamente bi - peduncolare mediante trokar montanti palloncini dedicati ; per entrambe le metodiche non bisogna mai superare la parete mediale del peduncolo sin quando non si raggiunto il muro posteriore del corpo vertebrale , controllato in pa ed ll ; il pmma utilizzato il medesimo in entrambe . 
per la kp si possono utilizzare cementi di pi nuova generazione come il calcibon o il fosfato tricalcico di idrossiapatite estendendo ulteriormente la sua indicazione nei soggetti giovani portatori di fratture traumatiche recenti ; lunica controindicazione assoluta la presenza di infezione sistemica o locale ; le complicanze riportate in letteratura sono pressoch simili . 
tuttavia , il rischio di stravasi di cemento durante la kp ridotto grazie alleffetto contenutivo della cavit preformata nel corpo vertebrale in cui il riempimento del cemento altamente viscoso avviene a bassa pressione e in maniera predeterminata in base al volume della cavit preformata in rapporto al volume raggiunto del palloncino . 
il razionale delle due metodiche si basa sul principio che liniezione del pmma nel soma fratturato permette di stabilizzare i movimenti delle microfratture trabecolari della spongiosa ossea , responsabili della sintomatologia dolorosa , rendono quindi il corpo vertebrale pi compatto e resistente . certamente , data la loro rilevanza epidemiologica , i crolli vertebrali di origine osteoporotica costituiscono le lesioni vertebrali maggiormente trattate con la vp , con una riduzione del dolore variabile dal 90% al 95% dei casi [ 21 ]  . infatti nella nostra casistica , 280 / 310 pazienti ( 90% ) hanno giovato di un miglioramento della sintomatologia dolorosa nelle prime 2472 h secondo la scala vas e ods . 
le lesioni secondarie da trattare sono quelle osteolitiche o miste , pi frequentemente da cancro mammella ( 30% ) o polmone ( 25% ) [ 4 ] , dove la remissione della sintomatologia dolorosa avviene nel 70%90% dei casi . 
nella popolazione neoplastica , studi recenti hanno osservato che , oltre allazione stabilizzatrice del pmma , il cemento provoca una attivit carcinolitica sulle cellule neoplastiche grazie alla reazione esotermica che libera quando polimerizza allinterno del soma vertebrale [ 6 , 22 ]  . il principale rischio della vp consiste nella fuoriuscita del cemento durante la sua introduzione in sede extraverteradiol med ( 2008 ) 113 : 11711184 1181 reaction during polymerisation within the vertebral body [ 6 , 22 ]  . 
 the main risk of vertebroplasty is the extravertebral leakage of cement into the spinal canal and preand paravertebral venous plexus , with consequent compression of nervous structures or pulmonary embolism [ 2329 ]  . 
the rate of thromboembolic complications has been reduced considerably by increased operator skill and the use of denser cements and is now 0.5%1% in osteoporotic fractures [ 22 ]  . 
no cases of pulmonary thromboembolism occurred in our series , whereas symptomatic extravertebral cement leaks into the vascular system or intervertebral disc occurred in 39 out of 485 patients and were treated conservatively . 
the rate of local or systemic complications in patients affected by spinal metastasis ranges from 2% to 5.1% [ 33 , 34 ]  . the risk of new fractures following vertebroplasty is reported to range from 10% to 30% [ 3540 ]  . 
in effect , it is still unclear whether this is related to the natural history of the underlying disease or to the treatment , especially if we consider that the presence of a single vertebral fracture in an osteoporotic patient is highly predictive of future fractures and that women with a single osteoporotic fracture have a 19.2% increased risk of developing new fractures in the following year [ 4143 ]  . vertebroplasty is the treatment of choice for symptomatic aggressive vertebral haemangiomas exhibiting t2 hyperintensity and t1 contrast - enhancement at mri [ 40 ]  . 
the treatment provides definitive sclerosis of the vertebral angioma by completely filling the lesion with cement , with pain relief in 90%100% of cases and no substantial early or late complications [ 44 , 45 ]  . 
a similar result was achieved in our series ( 100% )  . cement distribution and vertebral filling is generally more uniform and regular in patients affected by osteoporosis or haemangiomas compared with those with secondary lesions . 
in addition , no correlation has been found between cement volume and pain relief , as the volume injected depends on the degree of vertebral collapse and on the vertebral level treated , with smaller amounts being injected into thoracic vertebrae with wedge deformity ( as little as 4 ml ) compared with lumbar vertebrae without wedging ( up to 12 ml )  . 
il leakage extrasomatico pi frequente nelle fratture vertebrali metastatiche , con una percentuale variabile tra il 30% e 60% dei casi , e meno frequentemente nei crolli porotici di circa il 10% dei casi [ 3032 ]  . 
il tasso di complicanze tromboemboliche si ridotto considerevolmente , sia per la maggiore confidenza da parte degli operatori , sia per la commercializzazione di nuovi cementi pi densi ed attualmente dellordine del 0 , 5%1% dei casi nelle fratture porotiche [ 22 ]  . 
nella nostra casistica non abbiamo osservato casi di tromboembolie polmonari ; mentre abbiamo riscontrato fughe extravertebrali vascolari o discali , responsabili di sintomatologia radicolare , trattata con terapia medica , in 39 su 485 sottoposti a vp . 
il tasso di complicanze locali o sistemiche nei pazienti trattati con vp affetti da metastasi vertebrali invece variabile dal 2% al 5 , 1% [ 33 , 34 ]  . il rischio di nuove fratture a distanza di tempo dopo lesecuzione del trattamento con vp variabile dal 10% al 30% dei casi [ 3540 ]  . 
in realt non ancora chiaro se questo fenomeno sia legato alla normale evoluzione della malattia di base o al trattamento eseguito , considerando che una sola frattura vertebrale nel paziente porotico altamente predittiva per la comparsa di pi fratture in futuro e che in donne portatrici di un primo crollo porotico , il rischio di sviluppare nuove fratture nellanno successivo dimostrato essere di circa il 19 , 2% [ 4143 ]  . la vp la tecnica di scelta per il trattamento degli angiomi vertebrali sintomatici con segni di aggressivit alla rm denunciati dalliperintensit in t2 e dallimpregnazione di mdc ev in t1 [ 40 ]  . 
lo scopo di ottenere una sclerosi definitiva dellangioma vertebrale attraverso il riempimento completo della lesione mediante il cemento con remissione della sintomatologia dolorosa variabile dal 90% al 100% dei casi , senza sostanziali complicanze precoci o tardive [ 44 , 45 ] ; infatti noi abbiamo osservato un analogo risultato ( 100% )  . la diffusione ed il riempimento dei metameri trattati con vp stato generalmente molto pi omogeneo e regolare nei casi affetti da osteoporosi o angiomi rispetto a quelli affetti da lesioni secondarie ; tuttavia il successo del trattamento non correlabile alla diffusione omogenea o disomogenea del cemento nel contesto del metamero trattato . 
inoltre , non dimostrata alcuna correlazione tra quantit di cemento iniettata e remissione della sintomatologia in quanto ci dipeso dal grado di schiacciamento del metamero e dal livello del metamero trattato con minore quantit di cemento iniettata a livello dorsale con cuneizzazione ( anche solo 4 ml ) rispetto ai metameri lombari non cuneizzati ( sino a 12 ml )  . 
 kyphoplasty is used for the treatment of type a1 and a3 traumatic vertebral fractures according to the magerl le fratture vertebrali traumatiche trattate con la kp sono quelle di tipo a1 e a3 secondo la classificazione di 1182 radiol med ( 2008 ) 113 : 11711184 classification [ 20 ]  . 
by reexpanding the vertebra with balloon tamps , kyphoplasty reduces the pathological kyphosis , allowing restoration of normal vertebral biomechanics , early mobilisation of the patient and pain relief in 90%100% of cases , provided that the procedure is performed no later than 3 months after the trauma and the pedicles are intact and of adequate size [ 31 , 32 , 46 , 47 ]  . 
in effect , kyphoplasty has been shown to restore vertebral height in 10%20% of cases , with a reduction in wedge angle varying between 6 and 9 [ 47 , 49 , 50 ]  . 
in our series , we achieved pain relief in 90%95% of cases , depending on type of fracture , and an increase in vertebral body height sufficient to allow early mobilisation of the patient and restoration of the physiological distribution of postural forces 5153 ]  . 
however , even vertebroplasty has been shown to restore vertebral body height and correct pathological kyphosis , with outcomes that are only slightly inferior to kyphoplasty [ 5456 ]  . magerl [ 20 ] per le quali la sola terapia fin dora stata quella conservativa mediante lapplicazione di unortesi per un periodo che va da 4 a 6 mesi , spesso seguita da una guarigione costantemente in cifosi della vertebra fratturata . 
la kp , riespandendo il soma in altezza mediante i cateteri a palloncino , permette di ridurre la cifosi patologica ristabilendo la normale bio - meccanica vertebrale , di mobilizzare il paziente in tempi brevi e di ridurre la sintomatologia dolorosa nel 90%100% dei casi , purch eseguita entro 3 mesi dal trauma e i peduncoli siano integri e di adeguate dimensioni [ 31 , 32 , 46 , 47 ]  . 
 [ 48 ] , da uno studio su cadaveri , hanno dimostrato che ogni kp produce un ripristino dellaltezza somatica nel 47% dei casi e una correzione della cifosi nel 10% . 
in realt si visto che la kp permette di ripristinare laltezza del soma fratturato in una percentuale variabile dal 10% al 20% dei casi con un escursione in termini di gradi variabili da 6 a 9 gradi [ 47 , 49 , 50 ]  . 
nella nostra casistica , abbiamo ottenuto una riduzione della sintomatologia dolorosa variabile dal 90% al 95% a seconda del tipo di frattura registrando un incremento minimo dellaltezza somatica tale da garantire una rapida mobilizzazione del paziente e ripristinando fisiologica distribuzione delle forze posturali [ 5153 ]  . 
tuttavia , anche nella vp dimostrato una capacit di ripristinare laltezza del soma e di correggerne la cifosi patologica con un outcome di poco inferiore rispetto a quello ottenuto con la kp [ 5456 ]  . conclusions conclusioni on the basis of our results and the literature , we believe that both techniques vertebroplasty and kyphoplasty are effective for managing spinal pain and symptomatic vertebral fractures due to osteoporosis , aggressive haemangiomas and osteolytic neoplasms without involvement of the posterior vertebral wall or epidural space . 
alignment of the fractured vertebral body with reduction of posttraumatic kyphosis , physiological distribution of postural forces , early mobilisation of the patient and no need for postoperative bracing widely justify the exclusive use of kyphoplasty in this setting , especially in view of the current availability of biological cements that undergo rapid and complete osteointegration . sulla base di questi dati e su quanto esposto , riteniamo che entrambe le metodiche permettono un buon management delle sindromi antalgiche vertebrali e nei crolli sintomatici su base osteoporotica , angiomatosici con caratteri di aggressivit , di tipo neoplastico - osteolitico senza compromissione del muro posteriore e senza interessamento epidurale . in tali patologie la scelta delluna o dellaltra metodica a favore decisamente per la vp , in considerazione anche dell elevato costo della kp , purch eseguita con idonea tecnologia . 
crisi1 1dipartimento di diagnostica per immagine , azienda ospedaliero - universitaria , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , olanda 3dipartimento di radiologia , universit degli studi , verona , italy 4dipartimento di radiologia , universit degli studi , trieste , italy 5dipartimento di radiologia , universit degli studi , palermo , italy 6dipartimento di radiologia , irccs santa lucia , roma , italy correspondence to : f . 
cademartiri , viale rustici 2 , 43100 parma , italy , tel . : + 39 - 052 - 1961833 , e - mail : filippocademartiri@hotmail.com received : 8 august 2007 / accepted : 11 february 2008 / published online : 29 october 2008 springer - verlag 2008 abstract purpose . 
forty - five patients ( 29 men ; mean age 68 ) underwent msct angiography of the abdomen for suspected cmi ( main clinical finding : postprandial abdominal pain )  . 
the scan protocol was detectors / collimation 16 / 0.75 mm ; feed 36 mm / s ; rotation time 500 ms ; increment 0.4 mm ; 120150 mas and 120 kvp . 
a volume of 80 ml of contrast material was administered through an antecubital vein ( rate 4 ml / s ) , followed by 40 ml of saline ( rate 4 ml / s )  . 
images were analysed on the workstation with different algorithms ( axial image scrolling , multiplanar reconstructions , maximum intensity projection , volume rendering )  . targeted central lumen - line reconstructions ( curved reconstructions ) were obtained along the celiac trunk ( cet ) and superior mesenteric artery ( sma )  . 
image generation and interpretation required 25 mstenosis and / or occlusions were detected in 29 ( 65% ) cases on the cet and in 32 ( 71% ) on the sma . 
of those lesions ( n = 61 ) , 44 ( 49% ) were classified as not significant . in 16 ( 35% ) cases , there was a simultaneous stenosis riassunto obiettivo . 
quarantacinque pazienti ( 29 uomini ; et media 68 ) sono stati sottoposti ad angiografia dei vasi addominali mediante msct per sospetta icm ( principale sintomo clinico : dolore addominale post - prandiale )  . protocollo di scansione : detettori / collimazione 16 / 0 , 75 mm ; avanzamento 36 mm / s ; tempo di rotazione 500 ms ; incremento 0 , 4 mm ; mas 120150 e kvp 120 . 
ottanta millilitri di mezzo di contrasto sono stati somministrati per via antecubitale ( velocit : 4 ml / s ) , seguiti da 40 ml di soluzione salina ( velocit : 4 ml / s )  . 
le immagini sono state analizzate mediante workstation con diversi algoritmi ( cinescrolling delle immagini assiali , mpr - ricostruzioni multiplanari reconstructions , mip , maximum intensity projections , vr , volume rendering )  . 
ricostruzioni multiplanari curvate sono state effettuate lungo il tronco celiaco ( tce ) e larteria mesenterica superiore ( ams )  . locclusione e la stenosi significativa ( > 50% ) sono state rilevate . 
la generazione ed interpretazione delle immagini hanno richiesto in media 25 mstenosi e / o occlusione sono state rilevate in 29 ( 65% ) casi sul tce , ed in 32 ( 71% ) casi sullams . 
di queste lesioni ( n = 61 ) , 44 ( 49% ) sono 1136 radiol med ( 2008 ) 113 : 11351142 and / or occlusion of the cet and sma ( confirmed by conventional angiography )  . 
msct angiography can play a major role in the detection of stenosis of the abdominal arteries in patients with suspected cmi . keywords msct angiography chronic mesenteric ischaemia abdominal angina state classificate come non significative . 
in 16 ( 35% ) casi stata osservata una stenosi e / o occlusione simultanea di tce e ams ( confermate con angiografia convenzionale )  . in 6 ( 13% ) casi non vi era alcuna lesione a carico del tce , dellams o dei loro rami principali ( confermato al followup clinico )  . 
langiografia msct pu avere un ruolo importante nella rilevazione delle stenosi dei vasi addominali in pazienti con sospetta icm . parole chiave angiografia tc ischemia cronica mesenterica angina addominale introduction introduzione chronic mesenteric ischaemia ( cmi ) is an uncommon syndrome with a fairly typical clinical presentation . 
the slowly progressive development of postprandial epigastric pain associated with weight loss in an approximately 60year - old patient ( especially one affected by other atherosclerotic conditions ) is strongly suspicious for a vascular insufficiency of the splanchnic circulation . 
the diagnostic approach aims to identify the atherosclerotic obstruction , which is generally located at the origins of the celiac trunk ( cet ) , superior mesenteric artery ( sma ) and inferior mesenteric artery ( ima )  . doppler ultrasound is currently used as a noninvasive method to study the proximal splanchnic vessels , but intraabdominal gas , respiratory movements , obesity and any previous abdominal surgery may hinder or impede the gathering of diagnostic information . 
magnetic resonance angiography ( mra ) has the potential to provide both morphological ( stenosis ) and functional ( flow ) information [ 1 , 2 ]  . noninvasive imaging of the abdominal arteries with fourdetector - row multislice computed tomography ( msct ) has been shown to be effective [ 35 ] in providing a clear depiction of the branches of the sma and cet [ 3 , 5 ]  . 
moreover , msct angiography provides additional information about the surrounding tissues , which may prove crucial for developing the differential diagnosis and planning patient management . new generations of msct scanners with 16 or more detector rows have been commercially available for several years . 
these technical improvements allow accurate depiction of the abdominal vessels down to the most distal branches , with depiction of stenosis , collateral vessels and possibly even characteristics of atherosclerotic plaque . 
il lento sviluppo di un dolore epigastrico post - prandiale , associato con calo ponderale , in un paziente di circa 60 anni di et ( specialmente se caratterizzato da altre patologie aterosclerotiche associate ) , permette di sospettare con elevata probabilit una insufficienza vascolare del circolo splancnico . 
lapproccio diagnostico focalizzato allidentificazione della ostruzione aterosclerotica in genere localizzata allorigine del tronco celiaco ( tce ) , della arteria mesenterica superiore ( ams ) , e della arteria mesenterica inferiore ( ami )  . correntemente , lecotomografia doppler utilizzata come metodo non invasivo per studiare i vasi splancnici prossimali , ma il gas intra - addominale , i movimenti respiratori , lobesit , e qualunque precedente chirurgia addominale pu limitare o impedire la rilevazione delle informazioni diagnostiche . 
langiografia a risonanza magnetica ( angio - rm ) mostra invece un elevato potenziale data la sua capacit di visualizzare informazioni morfologiche ( stenosi ) e funzionali ( flusso ) [ 1 , 2 ]  . 
questi miglioramenti tecnici permettono di effettuare studi accurati dei vasi addominali fino a diramazioni molto distali , potendo definire la presenza di stenosi , circoli collaterali ed eventualmente le caratteristiche delle placche aterosclerotiche . 
basandoci sui recenti sviluppi tecnici e sui precedenti radiol med ( 2008 ) 113 : 11351142 1137 previously reported excellent results , we developed an msct angiography protocol to evaluate patients with suspected cmi . ottimi risultati , abbiamo sviluppato un protocollo per angiografia msct per la valutazione dei pazienti con sospetta ischemia cronica mesenterica ( icm )  . materials and methods materiali e metodi forty - five patients ( 29 men ; mean age 68 years ; age range 2881 ) gave their informed consent to undergo abdominal msct angiography for suspected cmi ( the main clinical finding was postprandial abdominal pain )  . 
the scanning parameters were ( table 1 ) : number of detectors / collimation 16 / 0.75 mm ; effective slice thickness 0.75 mm ; feed 36 mm / s ; rotation time 500 ms ; increment 0.4 mm ; 120150 mas ; 120 kvp . 
a volume of 80 ml of iodinated contrast medium ( visipaque 320 , amersham health , uk ) was administered via a dual - head injector ( stellant , medrad , usa ) through an antecubital vein ( flow rate 4 ml / s ) , immediately followed by a 40 - ml saline flush ( flow rate 4 ml / s )  . 
the estimated radiation dose was approximately 10 msv . quarantacinque pazienti ( 29 uomini ; et media 68 ; range 2881 ) hanno fornito consenso informato e sono stati sottoposti ad angiografica msct delladdome per sospetta icm ( principale reperto clinico : dolore addominale post - prandiale )  . 
i parametri di scansione erano ( tabella 1 ) : numero di dettettori / collimazione 16 / 0 , 75 mm ; spessore effettivo dello strato 0 , 75 mm ; avanzamento 36 mm / s ; tempo di rotazione 500 ms ; incremento 0 , 4 mm ; mas 120150 e kvp 120 . 
un volume di 80 millilitri di mezzo di contrasto iodato ( visipaque 320 , amersham health , regno unito ) stato somministrato con un iniettore automatico a doppia testa ( stellant , medrad , usa ) attraverso una vena antecubitale ( flusso = 4 ml / s ) , seguiti immediatamente da 40 ml di soluzione salina ( flusso = 4 ml / s )  . 
no motion artefacts due to vascular pulsation were observed . the anatomy of the cet and sma and their branches was successfully analysed down to the first generation ( even though possible , analysis beyond the first generation would have had no clinical role in this study )  . 
lanatomia del tce e dellams e dei loro rami stata analizzata agevolmente fino alla prima generazione ( oltre , anche se possibile non avrebbe avuto un ruolo clinico in questo studio )  . 
b after segmentation of the relevant vascular structures , the celiac trunk ( tce on the image ) is visualised with its main branches for the liver and spleen ; the superior mesenteric artery ( ams ) is displayed with all its main branches , including a stenosed ileocolic artery ( arrowhead ) , and also the inferior mesenteric artery ( ami ) and its branches . 
dopo segmentazione delle strutture vascolari di interesse ( b ) , il tronco celiaco ( tce ) visualizzato con i suoi rami principali per il fegato e per la milza , larteria mesenterica superiore ( ams ) visualizzata con tutti i suoi rami principali incluso un ramo ilieo - colico stenotico ( testa di freccia ) , ed anche larteria mesenterica inferiore ( ami ) ed i suoi rami . 
unarcata di riolano ipertrofica ( freccia sottile ) dimostra la presenza di una circolazione collaterale compensatoria tra lams e lami . was simultaneous stenosis and / or occlusion of the cet and sma ( confirmed by conventional angiography )  . 
in six ( 13% ) cases , no lesion was identified on the cet , sma or their branches ( negative finding confirmed by clinical follow - up at 3 and 6 months )  . 
in 12 ( 27% ) cases , we performed a percutaneous interventional procedure ( dilatation and / or stenting ) on the basis of the indication established with msct angiography . 
in five ( 11% ) cases , we performed a double percutaneous procedure involving stenting of the cet and sma and in one case an sma angioplasty . discussion cmi , also known as abdominal angina , is a syndrome due to chronic arterial insufficiency of the intestines . 
ancillary reports state that 18% of patients older than 65 years have mesenteric arterial stenosis 50% , even though only a small minority of them are symptomatic [ 7 , 8 ]  . tce e ams ( confermata dalla ac )  . 
in 6 ( 13% ) casi nessuna lesione era presente sul tce , ams o sui loro rami visualizzati ( reperto negativo confermato al follow - up clinico a 3 e 6 mesi )  . 
in 5 ( 11% ) casi stata effettuata una doppia procedura percutanea di stenting del tce e dellams , ed in un caso un angioplastica dellams . discussione lischemia cronica mesenterica ( icm ) , anche nota come angina addominale , una sindrome da insufficienza arteriosa cronica dellintestino . 
casistiche ancillari affermano che il 18% dei pazienti al di sopra dei 65 anni di et porta una stenosi 50% delle arterie mesenteriche , anche se una quota molto bassa di questi mostra sintomi [ 7 , 8 ]  . licm causata tipicamente da una stenosi / occlusione del tce , della ams , e della ami . 
the degree of stenosis or obstruction capable of determining clinical symptoms of each single artery varies and probably depends on anatomical configuration , rate of progression of the stenotic or obstructive process and the presence of collateral vessels . generally , all three vascular axes are variably occluded or stenotic . 
in fact , because of extensive collateral vessels between the vascular territories of the three main splanchnic arteries , abdominal angina tends to occur whenever at least two of the three vessels are obstructed . the atherosclerotic obstruction is usually located at the level of the cet and sma . 
complications such as bowel infarction or malnutrition are responsible for the high morbidity and mortality rates and determine the need for treatment . the hallmark of cmi is a characteristic intermittent dull or cramping epigastric and / or paraumbilical pain arising 1560 min after meals and lasting for several hours . the pain may be relieved by defecation . 
other associated signs and symptoms include constipation , flatulence and diarrhoea with or without some blood admixture . significant weight loss is observed over time and is primarily due to reduced food intake ( fear of eating )  . chronic ischaemia may also produce mucosal damage with loss of absorptive surface , which in turn aggravates the weight loss . 
if doubts persist about the nature of the diagnosis , quantitative mapping of portal flow with mri before and after a standard test meal may demonstrate the lack of normal postprandial increase in portal flow volume [ 1 , 2 ]  . the consecutive series selected on the basis of clinical findings of postprandial abdominal pain demonstrates the robustness of the msct technique and technology for evaluating the abdominal splanchnic vessels . 
the relatively pure patient population characterised by exclusively atherosclerotic stenoses ( in one unusually young patient , the clinical suspicion was supported by familial hypercholesterolaemia ) showed a prevalence of lesions > 60% on each of the major arterial axes ( cet and sma ) , for a total of about half of the visualised arteries being affected by stenosis or occlusions . 
il grado stenosi / occlusione capace di produrre sintomi clinici per ogni singolo asse vascolare variabile e probabilmente dipende dalla configurazione anatomica individuale , dalla velocit di progressione del processo stenotico / occlusivo e dalla presenza di circoli collaterali . 
generalmente , tutti e tre gli assi vascolari sono variabilmente occlusi / stenotici . infatti , a causa dellestensiva presenza e formazione di circoli collaterali tra i territori vascolari dei tre principali assi splancnici , langina addominale insorge pi comunemente quando almeno due dei tre vasi sono ostruiti . 
linsorgenza di complicazioni come linfarto intestinale e la malnutrizione sono le cause dellelevata morbidit e mortalit e della necessit di trattamento . il quadro patognomonico della icm caratterizzato da un dolore addominale intermittente epigastrico e / o paraombelicale di tipo gravativo o crampiforme che insorge da 15 a 60 minuti dopo un pasto , e si prolunga per diverse ore . il dolore pu essere alleviato dalla defecazione . 
meno di frequente possono essere presenti nausea e vomito . la diagnosi si basa sullidentificazione di stenosi significative prossimali a carico dei vasi splancnici in assenza di altre patologie che possano causare i sintomi . 
se i dubbi persistono sulla natura della diagnosi , un mapping del flusso mediante rm quantitativa prima e dopo un pasto standard pu mostrare la mancanza di un normale aumento del flusso portale post - prandiale [ 1 , 2 ]  . la casistica consecutiva da noi selezionata sulla base del quadro clinico dominato da dolore addominale post - prandiale di tipo anginoso mostra primariamente la robustezza della tecnica e della tecnologia di tc multistrato nella valutazione dei vasi splancnici addominali . 
la popolazione relativamente pura e caratterizzata da stenosi di natura unicamente aterosclerotica ( in un paziente di giovane et il sospetto clinico era sostenuto anche unipercolesterolemia familiare ) ha mostrato una prevalenza di lesioni superiore al 60% su ciascuno dei due maggiori assi ( tronco celiaco ed arteria mesenterica superiore ) per un totale di circa la met dei vasi visualizzati affetti da stenosi o occlusioni . 
solo 21 lesioni stenosanti sono state giudicate significative ( > 50% di riduzione del lume vascolare ) , e solo in 16 casi si osservata la simultanea presenza di lesioni del tronco celiaco dellarteria mesenterica superiore . 
sei pazienti sono risultati completamente negativi ( incluso il paziente di giovane et con ipercolesterolemia familiare )  . radiol med ( 2008 ) 113 : 11351142 1141 ( including the young patient with familial hypercholesterolaemia )  . in our experience , the vessel lumen and stenoses were well depicted by msct , even though the comparison with conventional angiography was possible in a limited number of cases only . 
in this setting , the value of mra is limited by artefacts due to stent composition . we encountered a few limitations of msct angiography . the first limitation is the lack of dynamic visualisation , which can be compensated for only in part by the high spatial resolution . 
thus , the indication for msct angiography must be considered carefully , and the examination should be reserved for patients older than 40 years . one limitation that may have biased results is related to patient selection and the fact that the principal inclusion criterion was postprandial abdominal pa addition of a more stringent inclusion criterion such as weight loss might have increased the prevalence of patients with a diagnosis of abdominal angina and thus of patients who would have benefited from percutaneous treatment . nellesperienza qui descritta , il lume vascolare e le stenosi sono ben visualizzate mediante msct , anche se il confronto con lac stato possibile in un numero limitato di casi . 
come potenziale informazione aggiunta la presenza di placche aterosclerotiche pu essere valutata non solo come restringimento del lume vascolare ( come nel caso dellac ) , ma anche in termini di caratterizzazione tissutale misurata mediante valore di attenuazione . questo tipo di informazione non ha ancora un ruolo clinicamente definito . se confrontata con lac , la msct facilmente in grado di escludere cause estrinseche di ostruzione vascolare ( i.e. : incarceramento del vaso e / o compressione da effetto massa ) che per non sono state rilevate nella nostra casistica [ 915 ]  . 
dopo trattamento dellangina addominale mediante il posizionamento di stent , lmsct pu essere inoltre utilizzata per il follow - up non - invasivo e valutare la presenza di re - stenosi allinterno dello stent . 
in questa applicazione langio - rm soffre degli artefatti dovuti alla composizione metallica dello stent . abbiamo incontrato alcune limitazioni per langiografia msct : la prima legato alla mancanza di visualizzazione dinamica , che solo in parte compensata dallelevata risoluzione spaziale . 
queste considerazioni dovrebbero far pesare adeguatamente lindicazione ad angiografia msct , riservandola a pazienti di et superiore ai 40 anni . una limitazione che pu aver modificato in senso difensivo i risultati legata al fatto che il maggior criterio di inclusione per lo studio tc stato il dolore addominale postprandiale . 
laggiunta di un criterio di inclusione pi rigido come il calo ponderale potrebbe aver aumentato la prevalenza di pazienti con diagnosi di angina addominale e che avrebbero quindi beneficiato del trattamento percutaneo . conclusions conclusioni our preliminary experience indicates a new field of application of msct angiography in noninvasive evaluation of vascular diseases . 
in patients with suspected cmi , msct angiography may become the one - stop - shop modality to exclude vascular disease or identify , quantify and plan the la nostra esperienza preliminare mostra un nuovo campo di applicazione per langiografia msct nella valutazione noninvasiva delle malattie vascolari . 
in pazienti con sospetta icm langiografia msct pu diventare la modalit onestop - shop per escludere il coinvolgimento vascolare o per rilevare , quantificare e pianificare la migliore opzione 1142 radiol med ( 2008 ) 113 : 11351142 best treatment strategy . 
thirty - three patients ( 21 women , 12 men , median age 58 years , range 2778 ) were enrolled . histological proof of malignancy was obtained in all cases . the primary tumour was unknown in 1 patient . 
bs and wb - mri were performed as staging procedures in 15 patients , during the follow - up in 6 and to investigate pain in 9 and neurological symptoms in 3 . 
two patients with negative wb - mri had focal and intense uptake in the ribs on bs . out of 264 examined areas , bone metastases were detected in 34 ( 13% )  . 
la scintigrafia ossea ( bs ) e la risonanza magnetica whole - body ( wb - mri ) sono state eseguite come procedure di stadiazione in 15 pazienti , durante il follow - up in 6 , per presenza di dolore in 9 e per la comparsa di sintomi neurologici in 3 . 
 parole chiave risonanza magnetica whole - body scintigrafia ossea midollo osseo metastasi introduction introduzione whole - body bone scintigraphy ( bs ) has long been considered the reference method to detect or exclude skeletal metastases and is widely used to assess metastatic spread in high - risk patients with breast , prostate and lung cancer [ 1 , 2 ]  . 
bs is sensitive for detecting bone metastases , but supplemental imaging studies are needed to define unclear findings , as bs has limited specificity [ 3 , 4 ]  . magnetic resonance imaging ( mri ) provides excellent soft tissue contrast and is thus quite useful for assessing patients with metastatic disease [ 5 ]  . 
skeletal metastases may frequently , but not always , manifest as deposits of tumour cells in the active haematopoietic bone marrow , which is typically found in the axial skeleton [ 6 ]  . 
however , the high rate of metastatic lesions in the femur , skull , pelvis and small bones requires a whole - body survey [ 7 ] , and conventional mri has not been routinely used in this diagnostic setting owing to the long imaging times and high cost . 
the purpose of this study was to evaluate the accuracy and feasibility of wbmri in comparison with bs with technetium 99mmethylene diphosphonate ( 99mtc - mdp ) in the detection of bone metastases . la scintigrafia ossea whole - body ( bs ) stata per lungo tempo considerata la metodica di riferimento nellidentificazione o nellesclusione delle metastasi scheletriche ed tuttavia ampiamente usata per valutare la diffusione metastatica in pazienti ad alto rischio affetti da neoplasia della mammella , della prostata e del polmone [ 1 , 2 ]  . 
la bs una metodica sensibile per la diagnosi di metastasi ossee ma non altamente specifica e pertanto necessita di integrazioni diagnostiche per chiarire risultati equivoci [ 3 , 4 ]  . la rm presenta elevata risoluzione di contrasto ed efficace nella valutazione dei pazienti con malattia metastatica [ 5 ]  . 
le metastasi scheletriche frequentemente , ma non sempre , possono presentarsi come deposti di cellule neoplastiche nel midollo osseo emopoieticamente attivo , tipicamente presente a livello dello scheletro assiale [ 6 ]  . 
per tali ragioni la rm attualmente considerata uno strumento diagnostico sensibile nella valutazione del midollo osseo . tuttavia lelevata frequenza di lesioni metastatiche a livello del femore , del cranio , della pelvi e delle piccole ossa richiede una valutazione panoramica dellintero corpo [ 7 ]  . inoltre , per i lunghi tempi di acquisizione e per i costi elevati , la rm convenzionale non stata impiegata routinariamente in questo contesto diagnostico . 
obiettivo di questo studio stata quella di valutare laccuratezza della wb - mri in confronto alla scintigrafia ossea con 99mtcmdp per lindividuazione delle metastasi scheletriche . materials and methods study group materiali e metodi gruppo dello studio thirty - three patients ( 21 women and 12 men ; median age 58 years ; age range 2778 ) were enrolled in the study . histological proof of malignancy was obtained in all cases . sono stati arruolati in questo studio trentatre pazienti ( 21 donne e 12 uomini , et media 58 anni , range 2778 anni )  . in tutti i casi stata ottenuta una conferma istologica radiol med ( 2008 ) 113 : 11571170 1159 primary tumour locations were : breast ( 1 ) , lung ( 7 ) , prostate ( 4 ) , colon ( 2 ) , bladder ( 2 ) , kidney ( 2 ) , soft tissues ( 1 ) , oesophagus ( 1 ) , pancreas ( 1 ) and head and neck region ( 1 )  . 
bs and wb - mri were performed as staging procedures in 15 patients , during the follow - up in six and to investigate pain in nine and neurological symptoms in three . 
patients characteristics are summarised in table 1 . a classification system was created based on the location of skeletal metastases rather than on their number , as some bone metastases revealed conglomeration . 
metastases were sought in eight skeletal segments : ribs ( r ) , skull ( s ) , cervicothoracic spine ( cts ) , lumbosacral spine ( ls ) , clavicle - scapula - sternum ( css ) , pelvis ( p ) , upper extremities ( ue ) and lower extremities ( le )  . 
il tumore primitivo era localizzato alla mammella in 11 casi , al polmone in 7 , alla prostata in 4 , al colon , alla vescica ed al rene in 2 , ai tessuti molli , allesofago , al pancreas ed al distretto testa - collo in 1 caso . il sito di primitivit tumorale rimasto ignoto in un solo paziente ( n 31 )  . 
bs e wb - mri sono state effettuate come procedure di stadiazione in 15 pazienti , durante il follow - up in 6 , per presenza di dolore in 9 e per sintomi neurologici in 3 . 
le caratteristiche dei pazienti sono riassunte in tabella 1 . stato inoltre creato un sistema di classificazione basato sulla sede della localizzazione scheletrica piuttosto che sul numero delle lesioni , poich queste spesso tendono a conglomerare . 
le metastasi sono state pertanto ricercate in 8 differenti segmenti scheletrici : coste ( r ) , cranio ( s ) , rachide cervico - dorsale ( cts ) , rachide lombosacrale ( ls ) , clavicola - scapola - sterno ( css ) , pelvi ( p ) , arti superiori ( ue ) , arti inferiori ( le )  . 
 t1 - weighted and short - tau inversion - recovery ( stir ) images were acquired for seven different body stations from head to toe using a combination of moving tabletop , tabletop extender and image - melding software ( mobiview software ; philips medical systems , best , the netherlands )  . 
 wb - mri tutte le immagini whole - body sono state acquisite usando uno scanner whole - body da 1 , 5 t ( achieva 1 , 5t , philips medical system , best , olanda ) con paziente posizionato sul tavolo porta - paziente in posizione piede - testa , supino e con le braccia posizionate ai lati del corpo . 
il fov di maggiori dimensioni consente di scannerizzare dalla testa ai piedi pazienti adulti senza necessit di riposizionamento [ 12 ]  . sono state eseguite sequenze turbo spin echo usando solo la bobina integrata body . 
 sono state acquisite immagini t1 - pesate e stir per sette differenti stazioni corporee dalla testa ai piedi usando la combinazione del tavolo porta - paziente in movimento , table extender e fusione delle immagini ( mobyview software , philips medical system , best , olanda )  . 
per ogni stazione corporea sono state acquisite 36 slices usando scansioni con la sincronizzazione del respiro per i distretti toracici ed addominali ( 18 slices / sincronizzazione del respiro )  . 
linterpretazione generalmente avviene in uno spazio di tempo breve di circa 1015 minuti [ 11 ]  . 1160 table 1 patient characteristics radiol med ( 2008 ) 113 : 11571170 patient gender primary tumour indication breast breast prostate lung breast colon breast oesophagus lung prostate breast breast lung prostate breast colon lung renal gastrinoma head & neck breast kidney prostate bladder sarcoma breast lung breast breast lung lung bladder follow - up staging staging pain staging neurological symptoms staging staging pain follow - up staging staging pain follow - up neurological symptoms pain staging pain staging staging paraplegia pain follow - up pain staging follow - up pain staging staging staging staging follow - up pain cup , cancer of unknown primary radionuclide bs scintigrafia ossea each bone scan was carried out 3 h after intravenous injection of 740 mbq ( 20 mci ) tc99m - hmdp ( schering pharma , bruxelles , belgium )  . 
a standard wb scan was performed with a dual - head gamma camera ( infinia ii , general electric , milwaukee , wi , usa ) equipped with lowenergy high - resolution collimators . 
 image interpretation la scintigrafia stata effettuata 3 ore dopo la somministrazione endovenosa di 740 mbq ( 20 mci ) di tc99m - hmdp ( 99 m tc idrossi methilene difosfonato , schering pharma , bruxelles , belgio )  . 
la scansione standard dellintero corpo stata effettuata con una gamma camera doppia testa ( infinia ii , general electric , milwaukee , wisconsin , usa ) equipaggiata con collimatori ad alta risoluzione e bassa energia . 
la velocit di scansione stata predefinita a 12 cm / min con una matrice di acquisizione di 2561024 pixels . ulteriori acquisizioni planari ad alta risoluzione o tomografiche sono state effettuate quando necessarie per chiarire risultati dubbi . mri was considered positive for metastatic bone disease when focal , often multiple , lesions were detected that exhibited low signal intensity on t1 - weighted images and high signal intensity relative to the surrounding marrow on stir - weighted sequences . 
hypointense lesions on all pulse interpretazione delle immagini la rm stata considerata positiva per metastasi scheletriche in presenza di lesioni focali , spesso multiple , con bassa intensit di segnale nelle immagini t1 - pesate e con radiol med ( 2008 ) 113 : 11571170 tabella 1 caratteristiche dei pazienti 1161 paziente sesso tumore primitivo indicazione mammella mammella prostata polmone mammella colon mammella esofago polmone prostata mammella mammella polmone prostata mammella colon polmone rene gastrinoma testa - collo mammella rene prostata vescica sarcoma mammella polmone mammella mammella polmone polmone vescica controllo stadiazione stadiazione dolore stadiazione sintomi neurologici stadiazione stadiazione dolore controllo stadiazione stadiazione dolore controllo sintomi neurologici dolore stadiazione dolore stadiazione stadiazione paraplegia dolore controllo dolore stadiazione controllo dolore stadiazione stadiazione stadiazione stadiazione controllo dolore cup , tumore primitivo di origine sconosciuta sequences were classified as sclerotic bone metastases [ 13 ]  . additional criteria for malignant involvement of the spine included bulging posterior margin of a vertebral body , signal - intensity change in the pedicles and the presence of paraosseous tumour extension . 
areas of radiopharmaceutical uptake were judged as benign when they were not focal or located adjacent to the joint surface . lesions appearing as areas of intense linear uptake in correspondence with the thoracic or lumbar vertebral body were considered benign , as were symmetrical hot spots in consecutive ribs . 
areas of increased uptake with intense and focal distribution were considered malignant when findings could not be explained by degenerative or traumatic conditions . iperintensit rispetto al midollo circostante nelle sequenze stir . 
per il rachide sono stati inclusi criteri addizionali per infiltrazione maligna quali bulging del margine posteriore del corpo vertebrale , variazione dellintensit di segnale nei peduncoli vertebrali e la presenza di estensione tumorale paraossea . 
 le anomalie presenti alla scintigrafia ossea sono state interpretate sulla base della distribuzione della captazione del radiofarmaco cos come della localizzazione , della forma ed intensit della aree di ipercaptazione focale . 
le aree di intensa ipercaptazione con aspetto lineare in corrispondenza del rachide dorsale o lombare sono state considerate benigne , cos come in presenza di 1162 radiol med ( 2008 ) 113 : 11571170 radiol med ( 2008 ) 113 : 11571170 1163 fig . 
wb / mri positiva per lesione metastatica in sede acetabolare destra ( a ) , mentre la scintigrafia ossea risulta negativa ( b )  . cold spots not due to artefacts were also considered malignant [ 2 ]  . bone metastasis was assumed in the event of concordantly positive wb - mri and bs or clear evidence of a skeletal lesion on one procedure only . 
cases were categorised as equivocal if wb - mri and bs were discordant and the finding could not be definitely defined as malignant or benign on one or both of the diagnostic procedures . equivocal cases were also studied by plain radiography , computed tomography ( ct ) , positron emission tomography / ct ( pet / ct ) and / or were followed for at least 12 months . 
egualmente sono state considerate le aree di ipocaptazione non dovute ad artefatti [ 2 ]  . la presenza di metastasi ossee stata pertanto assunta in caso di concordanza positiva tra wb - mri e bs o in caso di chiara di localizzazione metastatica anche se presente in una sola procedura . 
sono stati classificati come equivoci i casi discordanti tra wb - mri e bs per la presenza di unanomalia non chiaramente definibile come benigna o maligna , in una o in entrambe le procedure diagnostiche . 
i risultati equivoci sono stati valutati sulla base dei risultati radiografici , ct , ct - pet e / o seguiti per altri 12 mesi . results risultati we detected bone metastases in 18 of 33 patients , with an overall incidence of 55% . 
sono state riscontrate inoltre lesioni metastatiche in 8 dei 12 pazienti ( 67% ) con 1164 radiol med ( 2008 ) 113 : 11571170 detected in eight cases ( 67% )  . 
the overall results are reported in table 3 . patient - by - patient analysis revealed multiple lesions in 8 / 16 ( 50% ) patients with positive mri findings , and multiple focal hot spots in 8 / 13 ( 61.5% ) patients with positive bs findings . 
although each of these techniques has some limitations , an invasive approach based on core needle biopsy and fine - needle aspiration is reserved for a minority of cases in which doubts persist after intensive diagnostic evaluation [ 14 ]  . 
it is recommended for evaluating bone pain and is frequently used to clarify areas of increased uptake on bs to differentiate traumatic conditions from skeletal metastases [ 15 , 16 ]  . 
 radionuclide bs is largely accepted as a highly sensitive method but is limited by a lack of specificity because phosphonates accumulate in the malignant process as well as in infections , fractures , traumatic lesions and other benign conditions . 
in questo sotto - gruppo di pazienti , la wb - mri ha evidenziato lesioni del rachide toracico in 2 casi , di cui uno con multiple localizzazioni ( n 17 )  . 
 lanalisi per paziente ha rilevato la presenza di multiple lesioni metastatiche in 8 dei 16 pazienti ( 50% ) positivi alla wb - mri ; ugualmente in 8 dei 13 pazienti ( 61 , 5% ) positivi alla bs erano presenti focolai multipli . 
nessuno dei pazienti arruolati stato classificato come caso equivoco . discussione varie tecniche e metodiche sono impiegate per diagnosticare e monitorare la malattia metastatica scheletrica . sebbene ognuna di queste metodiche presenti dei limiti , un approccio invasivo con limpiego della biopsia , limitato ad una minima parte dei casi , in cui persista un dubbio diagnostico dopo una intensa valutazione [ 14 ]  . la radiologia tradizionale ampiamente disponibile , rapida ed economica , e dovrebbe essere utilizzata nella valutazione del paziente con dolore osseo ed routinariamente impiegata per chiarire le aree di ipercaptazione alla scintigrafia ossea differenziando condizioni traumatiche da malattia metastatica [ 15 , 16 ]  . 
 la scintigrafia ossea diffusamente accettata quale metodica altamente sensibile , ma limitata da una bassa sensibilit , poich i fosfonati possono concentrarsi sia in processi neoplastici che nelle infezioni , fratture , traumi ed in altre patologie benigne . 
moreover , three - dimensional evaluation of the skeletal system using the single - photon - emission tomography ( spet ) technique represents an improvement in terms of specificity because it provides better una sensibilit dell82% , con un valore predittivo positivo e negativo del 99 , 8% e del 72 , 8% rispettivamente [ 18 ]  . 
inoltre lo studio tomografico con tecnica spet rappresenta un ulteriore miglioramento in termini di specificit in virt del maggiore dettaglio anatomico e di una superiore risoluzione spaziale [ 19 ]  . 
al contrario , la sensibilit della 1166 radiol med ( 2008 ) 113 : 11571170 table 3 results of whole - body magnetic resonance imaging ( mri ) and bone scintigraphy ( bs ) patient mri findings mri lesion mri no . 
many authors have demonstrated lower diagnostic value in the spine , especially in the cervicothoracic tract , as well as in detecting lesions of the extremities [ 22 ]  . in particular , in obese patients or when using a gamma camera with a small field of view ( fov ) , the upper extremities may not be accurately represented . 
these data are in agreement with those reported in our series , where wb - mri had a higher diagnostic accuracy than bs , especially for metastases affecting the spine , clavicles or scapulae . 
la crescente mole di dati sui limiti di sensibilit della scintigrafia ossea ha posto qualche dubbio riguardo il suo impiego estensivo . lanalisi dei dati concernente laccuratezza della scintigrafia ossea rivela infatti limiti correlati sia alla sede anatomica della localizzazione che di fattori biologici . 
molti autori hanno dimostrato un limitato valore diagnostico nello studio del rachide , specialmente del distretto cervico - toracico , cos come nellindividuazione di lesioni localizzate agli arti [ 22 ]  . 
questi dati sono in accordo con quanto riportato nel nostro studio , dove la wb - mri presenta una accuratezza diagnostica pi elevata rispetto alla scintigrafia ossea , soprattutto per localizzazioni al rachide , alle clavicole o alle scapole . 
3 sensibilit della scintigrafia ossea e delle risonanza magnetica total body in funzione del distretto scheletrico interessato . cts , rachide cervico - toracico ; ls , rachide lombosacrale ; ssc , clavicola - scapolasterno ; p , pelvi ; ve , estremit superiori ; le , estremit inferiori . 
 mri is the only imaging technique that allows direct visualisation of bone marrow and its components , in nel diagnosticare lesioni costali o della teca cranica [ 23 ]  . le dimensioni delle lesioni ed il sito di interessamento ( raramente localizzazioni intratrabecolari sono positive alla bs ) sono altri fattori che sono chiamati in causa per spiegare la bassa sensibilit della scintigrafia ossea [ 24 ]  . 1168 radiol med ( 2008 ) 113 : 11571170 contrast to scintigraphy that permits the recognition of secondary osteoblastic response only . 
technical improvements concerning new sequences and faster methods for localising the signal have made it possible to use mri as a rapid imaging tool for whole - body surveys and thus to screen patients for bone metastases . 
 many recent studies report an excellent correlation between bs and wb - mri , although lesions in ribs , scapulae or skull may be better detected by bs , whereas additional metastases have been identified in the spine , pelvis and femur by wb - mri [ 27 , 28 ]  . 
these data , in agreement with our own findings , support the higher detection rate of wb - mri because of the wider range of detectable lesions in terms of both anatomical location and biological behaviour . 
 in detecting skeletal metastases , wb - mri has some advantages over bs : mri does not involve ionising radiation , and overall imaging time is shorter given that bs must be performed 24 h after isotope injection . 
 wb - mri , as well as positron emission tomography / computed tomography ( pet / ct ) , represent a step forward in the development of a single staging procedure capable of providing information about metastatic spread to the skeletal compartment and soft tissue organs and thus facilitating an overview of total tumour burden in affected patients . 
optimal wb - mri evaluation , however , requires specific training in order to gain experience and competence in compartments such as bone marrow , where knowledge of normal and pathological findings is crucial for distinguishing the effects of treatment and providing a comprehensive diagnosis [ 30 ]  . 
although many factors still affect the image quality and specificity of this technique , the inclusion of wb - mri in the diagnostic scenario represents a clear advantage for the appropriate management of cancer patients . 
wb - mri provides a valuable alternative to la rm la sola metodica di diagnostica per immagini che consente una immediata visualizzazione del midollo osseo e delle sue componenti , al contrario della scintigrafia che permette il solo riconoscimento delle risposta osteoblastica secondaria . 
il progresso tecnologico con lintroduzione di nuove sequenze e di tecniche pi veloci di localizzazione del segnale , fornisce la possibilit di impiegare la rm come strumento rapido per uno studio whole - body . 
la wb - mri permette infatti lo studio simultaneo sia dei tessuti molli che di organi fornendo una valutazione complessiva dellestensione neoplastica nel paziente oncologico [ 10 ]  . molti studi recenti riportano uneccellente correlazione tra la bs e la wb - mri , sebbene le localizzazioni alle coste , alla scapola ed al cranio possano essere meglio evidenziate dalla bs , mentre nella valutazione del rachide , della pelvi e dei femori la wb - mri risulta pi accurata [ 27 , 28 ]  . 
tali dati in accordo con i nostri risultati , mostrano la maggiore efficacia diagnostica della wb - mri in funzione del pi ampio spettro di lesioni evidenziabili , in termini sia di localizzazione anatomica che di comportamento biologico . la wb - mri presenta inoltre ulteriori vantaggi rispetto alla scintigrafia ossea : non impiega radiazioni ionizzanti e richiede un tempo minore di esecuzione poich la scintigrafia eseguita dopo 24 ore dalla somministrazione del radiofarmaco . 
la wb - mri , cos come la pet - ct , rappresenta uno step verso lo sviluppo di una singola procedura di staging , che sia capace di fornire informazioni sulla diffusione metastatica al compartimento scheletrico ed ai tessuti molli , ma che sia idonea a garantire una visione totale della diffusione neoplastica . 
 la wb - mri per la sua panoramicit dalla testa ai piedi , in grado di rivelare localizzazioni aggiuntive di rilevante significato terapeutico e prognostico [ 29 ]  . comunque lopportuno utilizzo della wb - mri richiede una formazione professionale dedicata per poter raggiungere esperienza e competenza in distretti come il midollo osseo , dove la conoscenza degli aspetti normali e patologici cruciale per il radiologo affinch possa distinguere gli effetti della terapia e fornisca una diagnosi esauriente [ 30 ]  . molti fattori ancora influenzano negativamente tale metodica , specialmente in termini di qualit di immagini e specificit , sebbene limpiego della wb - mri nello scenario diagnostico rappresenti un chiaro vantaggio nella appropriata gestione del paziente oncologico . 
la wb - mri radiol med ( 2008 ) 113 : 11571170 1169 the stepwise , multimodality approach to evaluating metastatic disease , in view of its high diagnostic accuracy , which exceeds even that of pet / ct [ 31 ]  . 
in addition , mri with diffusion - weighted sequences allows further improvement in the ability to detect skeletal lesions ( i.e. differentiating between neoplastic and osteoporotic vertebral collapse ) [ 3234 ]  . rappresenta unalternativa allapproccio multimodale per la valutazione della malattia metastatica , in virt della sua elevata accuratezza diagnostica , superiore anche a quella della pet / ct , almeno secondo alcuni autori [ 31 ]  . 
2005062137 of the italian ministry of education , university and research ( miur ) colonscopia virtuale : progetto prin ( progetto di rilevante interesse nazionale ) del miur ( ministero delluniversit e della ricerca ) , numero 2005062137 e . 
bartolozzi1 1radiologia diagnostica e interventistica , dipartimento di oncologia , trapianti e nuove tecnologie in medicina , universit di pisa , via roma 67 , 56100 pisa , italy 2dipartimento di scienze radiologiche , polo pontino , uos tecniche diagnostiche avanzate , universit la sapienza , roma , italy 3ircc ( istituto per la ricerca e cura del cancro ) , candiolo , torino , italy 4dipartimento dellimmagine , universit di siena , siena , italy 5image processing and informatics laboratory , university of southern california , marina del rey , ca , usa 6divisione di gastroenterologia , dipartimento di medicina interna , universit di pisa , pisa , italy correspondence to : e . 
the web site was created with microsoft office publisher 2003 software , which allows the realisation of multiple web pages linked through a main menu located on the home page . 
the web site contains a database of computed tomography ( ct ) colonography studies in the digital imaging and communications in medicine ( dicom ) standard , all acquired with multidetector - row ct according to the parameters defined by the european society of abdominal and gastrointestinal radiology ( esgar )  . 
the cases present different bowel - cleansing and tagging methods , and each case has been anonymised and classified according to the colonography reporting and data system ( c - rads )  . 
the web site is available at address www.ctcolonography.org and is composed of eight pages . download times for a 294 - mbyte file were 33 min from a residential adsl ( 6 mbit / s ) network , 200 s from a local university network ( 100 mbit / s ) and 2 h and 50 min from a riassunto obiettivo . 
il sito web stato realizzato con il software microsoft office publisher 2003 che consente la realizzazione di pagine web multiple , tra loro collegate attraverso un menu principale localizzato nella home page . 
nel suo interno sono archiviati studi dicom di cv , acquisiti con apparecchiature multistrato seguendo i parametri di qualit definiti dallesgar ; i casi presentano differenti metodi di pulizia intestinale . 
nelle prove di scaricamento dei dati tc da tecnologia adsl ( 6 mbit / s ) , un file di 294 mbytes stato scaricato in 33 minuti , da rete universitaria ( 100 mbit / s ) in 200 secondi , da sito remoto accademico negli usa in 2 ore e 50 minuti . il monitoraggio del numero di accessi in 22 giorni , dal giorno di pubblicazione , ha evidenziato 220 accessi . 
 keywords ct colonography computed tomography internet image archive image processing 3d imaging parole chiave colonscopia virtuale tomografia computerizzata internet archivio immagini elaborazione immagini elaborazione 3d introduction introduzione ct colonography , also known as virtual colonoscopy , is a recently introduced imaging technique that allows the targeted study of the colon by means of computed tomography ( ct )  . 
once the ct volume has been acquired ( preferably with low - dose , thinsection multislice imaging ) [ 1 , 2 ] , the native images can be directly viewed on the monitor of the reporting workstation ( 2d technique ) or processed on dedicated workstations for intraluminal viewing ( virtual endoscopic or 3d technique )  . many authors agree that the diagnostic efficiency of ct colonography is improved by using the two visualisation techniques in combination [ 2 , 3 ]  . 
a recent survey carried out by the italian society for medical radiology ( sirm ) among its members showed that ct colonography is now offered by 35 centres across the country [ 4 , 5 ]  . 
 although the examination has entered clinical practice , several outstanding issues rema the first relates to economic aspects in that the real cost of the study with respect to conventional colonoscopy or double contrast enema is still unknown . 
second , the quality and diagnostic accuracy of ct colonography is influenced by several technical problems , in particular by adequate bowel preparation associated with fluid and faecal tagging and by correct image interpretation ( 2d vs 3d technique )  . 
 the participating research centres are the divisions of diagnostic and interventional radiology and of gastroenla colonscopia virtuale ( cv ) , in lingua inglese ct colonography , una metodica di recente introduzione nella pratica clinica che consente uno studio dedicato del colon mediante tomografia computerizzata ( tc )  . 
 una volta condotta lacquisizione del volume tc ( preferibilmente con metodica multistrato con bassa dose e spessori di strato sottili ) [ 1 , 2 ] , le immagini native possono essere visualizzate direttamente al monitor della consolle di refertazione ( tecnica 2d ) o elaborate su stazioni di lavoro dedicate per una visualizzazione endoluminale del colon ( endoscopia virtuale o tecnica 3d )  . 
un recente questionario proposto dalla sirm a tutti i suoi soci ha dimostrato che la cv offerta da 35 centri di diverse regioni italiane [ 4 , 5 ]  . 
in particolare , si dimostrano di estrema rilevanza una idonea preparazione intestinale , associata a marcatura dei residui fluidi e fecali , e una corretta analisi delle immagini ( tecnica 2d vs 3d )  . 
 1128 radiol med ( 2008 ) 113 : 11261134 terology , both of the university of pisa , the polo pontino of the department of radiological science of la sapienza university of rome , the department of radiological science of the university of siena , and the institute for cancer research and treatment ( ircc ) of candiolo , tur the first step in the research project involved the creation of a web site , which is available at the internet address the aim of this paper is to describe the web site and present the prototype of the online database . 
 materials and methods the web site was developed with microsoft office publisher 2003 software ( microsoft srl , segrate , milan , italy ) , which allows the creation of multiple web pages linked to a main menu located on the home page [ 6 ]  . 
the menu located on the left of the home page contains hyperlinks to the web pages , and each page is displayed within a frame on the home page so as not to modify the web sites navigation bar and thus renders navigation of the site easy and fast , even for less experienced users . 
the web site physically resides on the server of the italian internet provider aruba ( aruba s.p.a. , soci , ar ) , which provides internet access with unlimited storage capacity . 
this feature was influential in our decision to choose this provider , as the storage of numerous ct colonography data sets ( acquired with multislice ct ) requires a large memory capacity . 
 the ct colonography data sets were acquired with multislice ct scanners according to the quality parameters established by the european society of abdominal and gastrointestinal radiology ( esgar ) consensus statement [ 2 ] , namely , a slice thickness not exceeding 2.5 mm , scans in the supine or prone position without administration of intravenous contrast material , low radiation dose ( 120 kvp and 50100 mas ) , manual insufflation of approximately 2 l of room air or automated insufflation of 3 l of carbon dioxide with a dedicated insufflator ( protoco2l colon insufflator system ; e - z - em , ny , usa )  . 
nel menu posto al margine sinistro della pagina sono presenti i collegamenti ipertestuali alle pagine web e ciascuna pagina viene visualizzata allinterno della home page stessa come una sua parte integrante ( frame ) , senza modificare linterfaccia di navigazione allinterno del sito ; ci rende la navigazione stessa facile e veloce anche per gli utenti meno esperti . 
tale elemento ha condizionato la scelta di questo fornitore ( o internet provider ) , in quanto per larchiviazione di molti esami di cv ( acquisiti con tc multistrato ) nel database necessaria una ampia capacit di memoria . 
 i dati di cv sono stati acquisiti con apparecchiature multistrato seguendo i parametri di qualit definiti dallesgar consensus statement [ 2 ] , in particolare : spessore di strato non superiore a 2 , 5 mm , acquisizione in decubito supino e prono senza mdc ev , bassa dose radiante ( 120 kvp e 50100 mas ) , insufflazione manuale di circa 2 l di aria ambiente o insufflazione automatica di 3 l di co2 con insufflatore dedicato ( protoco2l colon insufflator system ; e - z - em , ny , usa )  . 
 radiol med ( 2008 ) 113 : 11261134 1129 header indicating the institution where the study was performed , with the software voxar 3d workstation 6.2 ( barco nv , kortrijk , belgium ) and advantage windows 4.2 ( ge healthcare , wi , usa )  . 
after anonymisation , each study , made up of the scout views and the two supine and prone acquisitions , was compressed in zip format ( compression ratio 2 : 1 without information loss ) to create a single file . 
 the cases , all validated by endoscopic investigation after ct colonography , were classified using the ct colonography reporting and data system ( c - rads ) recently suggested by zalis et al . 
the classification is as follows : c0 , inadequate study , in which significant lesions cannot be excluded ; c1 , negative study ; c2 , presence of one or two polyps 69 mm in diameter ; c3 , presence of three or more polyps each 69 mm in diameter or one or more polyps 1 cm or larger ; c4 , presence of intraluminal mass ( mass being defined as a lesion measuring 3 cm or more in diameter )  . extracolonic findings were also considered and classified as follows : e0 , limited examination for the evaluation of extracolonic soft tissues ; e1 , no extracolonic abnormalities visible ; e2 , presence of clinically unimportant findings ; e3 , likely benign extracolonic finding ; e4 , important extracolonic finding requiring immediate further investigation . each case was uploaded onto the server and inserted as a hypertext link . 
 especially interesting ct colonography links are those connecting to ongoing multicentre trials : the italian multicenter polyps accuracy ctc study ( impact project ) promoted by the sirm , with estimated completion date in 2007 and available at and the national ct colonography trial 4 . 
bario e dulcolax ( boehringer ingelheim italia s.p.a. , milano ) in aggiunta a dieta priva di scorie . tutti i dati sono stati anonimizzati , conservando esclusivamente lheader dicom relativo alla istituzione di provenienza , con il software voxar 3d workstation 6.2 ( barco nv , kortrijk , belgio ) e con advantage windows 4.2 ( ge healthcare , wi , usa )  . 
dopo il processo di anonimizzazione , ciascuno studio , comprendente le acquisizioni di centraggio ( scout view ) e le due acquisizioni nei decubiti supino e prono , stato compresso in formato zip ( rapporto di compressione 2 : 1 senza perdita di informazioni ) , realizzando un unico file . 
 i casi , tutti comprovati da verifica endoscopica successiva allesame di colonscopia virtuale , sono stati classificati secondo il sistema c - rads ( ct colonography reporting and data system ) , proposto recentemente da zalis et al . 
 [ 7 ] , come di seguito : c0 , esame di scarsa qualit diagnostica dove non possibile escludere lesioni significative ; c1 , esame negativo ; c2 , presenza di 12 polipi con diametro massimo compreso tra 6 e 9 mm ; c3 , presenza di oltre 3 polipi con diametro massimo compreso tra 6 e 9 mm o polipi con diametro massimo maggiore o uguale a 1 cm ; c4 , presenza di masse endoluminali ( considerando la definizione di massa per lesioni con diametro massimo maggiore o uguale a 3 cm )  . 
sono stati considerati anche i reperti extracolici , che vengono classificati come segue : e0 , esame di scarsa qualit diagnostica per linterpretazione di reperti extracolici ; e1 , assenza di reperti extracolici ; e2 , presenza di reperti extra - colici di scarso significato clinico ; e3 , reperti extracolici di probabile natura benigna ; e4 , reperti extracolici rilevanti che necessitano immediato e ulteriore approfondimento diagnostico . 
 le prove di scaricamento sono state condotte da rete adsl residenziale con larghezza di banda a 6 mbit / s , da rete lan universitaria a 100 mbit / s e infine da sito remoto accademico negli usa su rete a 100 mbit / s ( image processing and informatics laboratory , university of southern california , marina del rey , ca , stati uniti )  . 
 the download tests were conducted in the morning ( 811 a.m. ) , when internet traffic is presumed to be at its heaviest . with residential adsl technology , a 294 - mbyte file was downloaded in 33 min at an average speed of 164 kbit / s ( min 150 ; max 190 )  . 
5a , b esempio di un caso classificato come c3 , scaricato e visualizzato su dicom viewer , dove apprezzabile un polipo peduncolato di dimensioni significative , nel decubito supino ( a ) e prono ( b )  . discussion publication of web sites addressing specific medical issues is becoming increasingly widespread on the internet . 
nel caso della tecnologia adsl residenziale , un file di 294 mbytes stato scaricato in 33 minuti con velocit media di 164 kbit / s ( min 150 max 190 )  . 
lo scaricamento del file da rete universitaria ha consentito di ricevere lintero esame in 200 secondi , con una velocit media di 1200 kbit / s ( min 1000max 1600 )  . 
lo scaricamento dal sito remoto accademico di marina del rey stato effettuato in 2 ore e 50 minuti con una velocit media di 28 kbit / s ( min 27 max 32 )  . 
esistono peraltro siti in cui laccesso viene differenziato tra pagine per i pazienti e pagine per il medico , con contenuti ovviamente dedicati allutente specifico e con differente approfondimento della materia [ 813 ]  . 
i collegamenti agli altri siti web sono stati scelti in base a criteri di stabilit degli stessi ; di frequente infatti alcuni siti web o radiol med ( 2008 ) 113 : 11261134 1133 fact sheets for patients and medical professionals . 
in fact , some web sites or web pages are often short - lived because either they are suppressed owing to lack of interest or they are moved to new addresses . 
this implies that when surfing the internet , one can never be sure to find again a resource that one has consulted in the past [ 12 , 13 ]  . 
 the peculiarity of this web site , compared with others on the same topic , is the creation of a database of complete dicom data sets from ct colonography based on the crads classification . 
this aspect of the database is very innovative in that the radiology learning resources available on the internet tend to present only the most significant images of a clinical case , which in most cases is adequate for the e - learning purpose of the resource in question [ 1416 ]  . 
in the case of ct colonography , the training of radiologists on an adequate number of cases is a prerequisite for defining the radiologist an expert : according to several authors , radiologists need to have interpreted at least 50 examinations controlled with conventional colonoscopy before undertaking diagnostic activity [ 1720 ]  . 
the database developed within the project should therefore prove useful ( even minimally ) for training radiologists to read ct colonography examinations , as it provides users with colonography data sets obtained with latest - generation ct scanners and all controlled by endoscopy . 
further , considering that the data refer to an entire native examination , they can be downloaded at a reasonable speed for a learning resource ( as shown by our download tests )  . 
 the web site developed within the framework of the miur project on ct colonography is an immediate and upto - date tool for publicising the activity of the research group among radiologists and clinicians . 
 la peculiarit di questo sito , rispetto ad altri siti web con stessa tematica , la realizzazione di un database di dati dicom di colonscopia virtuale tc , completi , basato sulla classificazione c - rads . 
tale classificazione ha lo scopo di guidare il medico radiologo verso una diagnosi sistematica e di pi facile comprensione anche per il clinico che dovr interpretare il referto radiologico ; si tratta comunque dellunica attualmente disponibile . pertanto la scelta di classificare i dati secondo c - rads consente allutente di scaricare un caso clinico di una specifica categoria diagnostica . 
questo aspetto del database da considerarsi molto innovativo , in quanto le risorse didattiche radiologiche disponibili su internet si limitano a presentare le immagini pi significative del caso clinico e nella maggior parte dei casi sono sufficienti allo scopo delle - learning della risorsa in oggetto [ 1416 ]  . 
nel caso specifico della colonscopia virtuale , laddestramento del radiologo su un congruo numero di casi rappresenta una fase necessaria affinch egli possa essere definito esperto ; secondo alcuni autori il medico radiologo dovrebbe aver interpretato almeno 50 esami controllati con colonscopia tradizionale prima di iniziare lattivit diagnostica [ 1720 ]  . 
il database sviluppato nellambito del progetto descritto in questo lavoro , dovrebbe quindi risultare utile ( anche se in minima parte ) allo scopo di addestramento alla lettura di esami di colonscopia virtuale , poich fornisce allutente dati di colonscopia virtuale ottenuti con tc di ultima generazione e tutti controllati endoscopicamente . 
i dati inoltre possono essere scaricati a velocit di trasmissione accettabili per una risorsa didattica , considerando che si tratta dellintero esame nativo ( come dimostrato dalle prove di scaricamento eseguite nel presente lavoro )  . 
lobiettivo primario del nostro lavoro quello di illustrare le caratteristiche rm delle recidive di neoplasia uterina dopo chirurgia , e delle relative modificazioni dopo la terapia radio - chemioterapica concomitante . 
sono state incluse in questo studio prospettico 22 pazienti con recidiva di neoplasia uterina , dopo terapia chirurgica ( cervice : 13 pazienti ; endometrio : 9 pazienti ) , confermate istologicamente . 
criteri di inclusione sono stati : esecuzione di una risonanza magnetica ( rm ) , alla diagnosi e durante il follow - up , e candidate al trattamento radio - chemioterapico concomitante . 
la sede della recidiva pelvica stata : cupola vaginale in 9 / 22 ( 41% ) pazienti , vagina in 5 / 22 ( 23% ) , cupola vaginale con estensione alla parete pelvica in 5 / 22 ( 23% ) ; parete pelvica in 3 / 22 ( 13% )  . 1144 radiol med ( 2008 ) 113 : 11431156 complete response was seen in 11 / 22 ( 50% ) patients , partial response in 8 / 22 ( 36% ) and no change in 3 / 22 ( 14% )  . 
il volume 3d medio della recidiva , nelle immagini rm pre - trattamento , stato di 38 , 83 cm3 . nelle immagini rm dopo trattamento la lesione apparsa ipointensa in 19 / 22 ( 86% ) pazienti ed iperintensa in 3 / 22 ( 14% )  . 
undici / 22 ( 50% ) pazienti hanno mostrato una risposta completa , 8 / 22 ( 36% ) una risposta parziale , 3 / 22 ( 14% ) nessun cambiamento . 
 parole chiave neoplasie recidive rm neoplasie utero radio - chemioterapia concomitante introduction introduzione uterine cancer relapses in 10%20% of patients after surgical treatment , regardless of whether the origin is the uterine cervix or corpus [ 14 ]  . 
the choice of treatment for recurrent uterine cancer is based on multiple factors : patients clinical condition , recurrence site , presence of metastasis and previous treatment [ 5 ]  . 
when the pelvis is the recurrence site , radiotherapy is usually the treatment of choice [ 4 ] , as surgery must be highly aggressive to ensure radical resection of the tumour and often involves pelvic exenteration [ 2 ] , with consequent limitation of the patients quality of life [ 610 ]  . 
 an increasingly common alternative is the use of concurrent chemoradiation with fluorouracil and / or cisplatthe rationale is to exploit the radiosensitising effect of chemotherapy to reduce radiotherapy dose and thus limit actinic complications while ensuring a cytotoxic effect [ 4 ] , as has been demonstrated in the local control of advanced squamous cell carcinoma of the anal canal [ 11 ] and uterine cervix [ 4 , 1216 ]  . 
the medical needs in planning chemoradiation of relapsing squamous cell carcinomas of the cervix or endometrial adenocarcinoma are to define recurrence site , extent and volume to calculate the target volume . 
 magnetic resonance ( mr ) imaging , with its high - contrast resolution and multiplanar capabilities , is helpful for distinguishing relapsing tumour from pelvic organs or structures and for determining tumour extent and volume . 
thanks to the ability of mr imaging to differentiate relapse from le neoplasie dellutero recidivano nel 10%20% dei casi dopo trattamento chirurgico , indipendentemente dalla loro sede di origine : cervice o corpo dellutero [ 14 ]  . 
la scelta del trattamento delle recidive di neoplasia uterina si basa su multipli fattori : condizioni cliniche della paziente , sede della recidiva , eventuale presenza di metastasi , e precedente trattamento [ 5 ]  . quando la sede della recidiva pelvica , la radioterapia solitamente il trattamento di scelta [ 4 ] , poich la chirurgia , per ottenere la radicalit oncologica , altamente aggressiva dovendo spesso ricorrere alla exenteratio pelvica [ 2 ] , con conseguente limitazione della qualit della vita delle pazienti [ 610 ]  . 
tuttavia , la radioterapia esclusiva quando viene somministrata in presenza di diverticoli intestinali o di aderenze post - opeartorie pu causare complicanze postattiniche , alle dosi necessarie per controllare la recidiva neoplastica . 
 pertanto attualmente trova sempre pi applicazione la radio - chemioterapia concomitante , con fluorouracile e / o cisplatino , che sfrutta leffetto radiosensibilizzante della chemioterapia che permette di ridurre le dosi di radioterapia limitando le complicazione post - attiniche e garantendo , al contempo , leffetto citoriduttivo [ 4 ] , come gi stato dimostrato nel controllo locale del carcinoma squamoso avanzato del canale anale [ 11 ] e della cervice uterina [ 4 , 1216 ]  . 
pertanto la necessit medica nella pianificazione del trattamento radio - chemioterapico delle neoplasie recidive dellutero , sia da carcinoma squamoso della cervice che da adenocarcinoma dellendometrio , quella di definire la sede del recidiva , i suoi limiti ed il volume del radiol med ( 2008 ) 113 : 11431156 1145 fibrosis [ 17 ] , it can also be used to assess response to chemoradiation [ 18 ]  . the primary objective of our study was to describe mr imaging patterns of pelvic recurrence of uterine cancer ( cervical and endometrial ) after surgery and to assess their changes after concurrent chemoradiation as an indicator of response to treatment . 
the secondary objective was to identify mr imaging parameters that might be useful in predicting outcome . materials and methods patient population twenty - two women ( mean age 52.7 years ; range 3169 ) with local recurrence of uterine cancer after surgery ( cervix 13 patients ; endometrium 9 patients ) were enrolled in this study after providing written informed consent . 
at preoperative diagnosis , 2 / 13 ( 15% ) patients had international federation of gynecology and obstetrics ( figo ) stage ia2 cervical carcinoma , 6 / 13 ( 46% ) had stage ib , 1 / 13 ( 8% ) had stage iia and 4 / 13 ( 31% ) had stage iib . 
 in all patients , disease recurrence was suspected clinically on the basis of bleeding from the external genitalia or elevated tumour markers ( ta4 - scc for the cervix and ca125 for the endometrium ) and subsequently confirmed by biopsy : 13 / 22 ( 59% ) patients had squamous cell carcinoma of the cervix and 9 / 22 ( 41% ) had endometrial adenocarcinoma . 
the mean disease - free interval between surgery and relapse was 13 months ( 154 months )  . the treatment schedule was established by a multidisciplinary group made up of an oncological gynaecologist , a radiotherapist , a radiologist and a pathologist after evaluation of the mr and gynaecological examination findings . 
 la risonanza magnetica ( rm ) , grazie allalta risoluzione di contrasto ed alla multiplanariet , utile nel distinguere la recidiva tumorale da altri organi o strutture pelviche , nel valutare lestensione del tumore e nella determinazione del volume dello stesso . 
grazie alla capacit della rm di distinguere la recidiva dalla fibrosi [ 17 ] , possibile valutare la risposta della recidiva tumorale alla radio - chemioterapia [ 18 ]  . lobiettivo primario del nostro studio stato quello di descrivere le caratteristiche di rm delle recidive pelviche di neoplasia uterina ( cervice ed endometrio ) dopo trattamento chirurgico ; e di valutare le loro modificazioni dopo radiochemioterapia concomitante , indice di risposta al trattamento . 
lobiettivo secondario stato quello di identificare parametri rm che avessero un ruolo nella prognosi della malattia . materiali e metodi popolazione delle pazienti ventidue donne ( et media 52 , 7 ; range 3169 ) con cancro uterino recidivato localmente dopo la chirurgia ( cervice : 13 pazienti ; endometrio : 9 pazienti ) sono state arruolate in questo studio , previo consenso informato scritto . 
tutte le pazienti hanno subito listerectomia radicale ( classe iv , secondo piver ) [ 19 ] con linfoadenectomia pelvica ; 11 / 22 pazienti , inoltre , hanno subito una linfoadenectomia lomboaortica . 
alla diagnosi pre - chirurgia , delle pazienti con carcinoma cervicale ( n = 13 ) , 2 / 13 ( 15% ) presentavano uno stadio ia2 secondo la figo , 6 / 13 ( 46% ) pazienti stadio ib , 1 / 13 ( 8% ) pazienti stadio iia e 4 / 13 ( 31% ) stadio iib . 
delle pazienti con adenocarcinoma dellendometrio ( n = 9 ) , 1 / 9 ( 11% ) presentavano uno stadio figo ia , 4 / 9 ( 45% ) pazienti stadio ib , 3 / 9 ( 33% ) pazienti stadio ic e 1 / 9 ( 11% ) pazienti stadio iii . 
 in tutte le pazienti , la diagnosi di recidiva di neoplasia stata sospettata clinicamente quando sono comparse perdite ematiche da genitali esterni , o quando si avuto un aumento dei marker tumorali ( ta4 - scc per la cervice e ca125 per lendometrio ) e successivamente confermata mediante biopsia : 13 / 22 ( 59% ) pazienti avevano un carcinoma squamoso della cervice e 9 / 22 ( 41% ) pazienti un adenocarcinoma endometriale . 
intracavitary therapy was indicated in vaginal recurrences or those centred on the vaginal vault within 5 mm of the uppermost edge of the intravaginal applicator ; ebrt was indicated for pelvic recurrences located > 8 mm from the vaginal vault . 
la terapia radiante , costituita da un fascio esterno ( ebrt ) , stata applicata sulla pelvi , con fascio di fotoni di energia mv > 10 con tecnica box ; le pazienti sono state posizionate in decubito prono su di un tavolo con un dispositivo up - down ( udt ) , per spostare cranialmente le anse intestinali . 
poich lintenzione del trattamento era curativa , le pazienti hanno ricevuto una dose complessiva di 46 , 8 gy , con una frazione giornaliera di 1 , 8 gy , secondo licru 50 [ 20 ] ; inoltre la dose totale stata somministrata in due sessioni separate da 23 , 4 + 23 , 4 gy ( split regimen ) , con un intervallo di 4 settimane , per ridurre la tossicit sullintestino , in relazione al pregresso intervento chirurgico che stato radicale ( classe iv sec . piver ) [ 19 ]  . 
il protocollo terapeutico prevedeva uninfusione endovenosa continua per 4 giorni di 5 - fluorouracile ( 5 - fu ) , in una dose di 1 g / m2 / die ( senza superare 1 , 5 g / m2 / die ) e in uninfusione a bolo di mitomicina c ( mit - c ) , 10 mg / m2 , dal momento dellinizio dellinfusione del 5 - fu ( primo giorno )  . 
la chemioterapia stata somministrata attraverso catetere venoso centrale , 7f con doppio lume ( hohn , bard , salt lake city , ut ) con una pompa di infusione radiol med ( 2008 ) 113 : 11431156 1147 patients underwent follow - up mr imaging at 45 days , at 6month intervals during the first 2 years and annually thereafter to evaluate response to treatment . 
 mr imaging all patients were studied with the same technique using a 1.5 - tesla superconductive magnet ( echospeed , ge medical system , milwaukee , wi , usa ) with a multichannel phased - array coil positioned on the pelvis . 
to reduce intestinal peristalsis , patients received an intramuscular injection of 1 mg butyl scopolamine ( buscopan , schering , germany ) 10 min before the beginning of the examination . axial t1 - weighted spin echo ( se ) images were acquired with the following parameters : tr / te 500 / 14 ms , slice thickness 4 mm with 1 - mm interval , matrix 256256 , and field of view ( fov ) 24 caxial t2 - weighted rapid acquisition with relaxation enhancement ( rare ) fast spin echo ( fse ) images were acquired with the following parameters : tr / te 4 , 000 / 85 ms , echo train length ( etl ) 12 , slice thickness 4 mm with 1 - mm interval , matrix 256256 , and fov 24 c the parameters used to obtain the sagittal and coronal t2 - weighted rare sequences were tr / te 3 , 5004 , 000 / 90 ms , etl 12 , slice thickness 3 mm with 1mm interval , matrix 256256 , and fov 24 cin addition , axial t2 - weighted rare images , acquired with a body coil , were obtained up to the renal hilum to search for lumboaortic nodal enlargement , with the following parameters : tr / te 4 , 000 / 90 ms , slice thickness 8 mm , interval 1 mm , matrix 256192 , and fov 40 cm . image analysis mr images were prospectively assessed by two radiologists ( rm , sb ) with experience in pelvic mr imaging ( > 10 and > 6 years , respectively )  . 
dopo 2 settimane dalla radio - chemioterapia concomitante , 14 / 22 ( 64% ) pazienti hanno ricevuto una dose supplementare di radiazione ( boost ) con brachiterapia endocavitaria a basse dosi ( ldr ) ( 2025 gy a 0 , 5 cm dalla superficie dellapplicatore ) mentre 8 / 22 ( 36% ) pazienti con fasci esterni ( 1420 gy )  . 
lobiettivo e la tecnica di somministrazione della dose supplementare di radioterapia ( boost ) sono stati scelti in base alla morfologia ed alla sede del tumore residuo : la terapia endocavitaria stata indicata nelle recidive vaginali o quelle centrate sulla cupola vaginale entro 5 mm dal bordo superiore del dispositivo endovaginale ; mentre la radioterapia con fasci esterni stata indicata per le recidive pelviche , a pi di 8 mm dalla cupola vaginale . 
tutte le pazienti hanno eseguito un esame di rm di follow - up 45 giorni dopo la fine del trattamento , ogni 6 mesi durante i primi 2 anni e successivamente annuale , per valutare la risposta al trattamento . 
 immagini rm tutte le pazienti sono state studiate con la medesima tecnica di studio utilizzando un magnete da 1 , 5 tesla superconduttivo ( echospeed , ge , milwaukee , wi , usa ) con bobina di superficie multicanale ( phased array ) posizionata sulla pelvi . 
per ridurre la peristalsi intestinale stato somministrato a le pazienti 1 mg di butilscopolamina ( buscopan , schering , germania ) intramuscolo , 10 minuti prima dellinizio dellesame . le immagini assiali t1 - dipendenti spin echo ( se ) sono state ottenute con i seguenti parametri : tr / te 500 / 14 di ms , 4 mm di spessore , con 1 mm di intervallo , matrice 256256 , fov 24 c le immagini t2 - dipendenti assiali rare ( rapid acquisition with relaxation enhancement ) ( fast spin echo , fse ) sono state ottenute con i seguenti parametri : tr / te 4000 / 85 ms , etl 12 , 4 mm di spessore con 1 mm di intervallo , matrice 256256 , fov 24 cle immagini sagittali e coronali t2 - dipendenti rare sono state ottenute con i seguenti parametri : tr / te 35004000 / 90 ms , etl 12 , 3 mm di spessore con 1 mm di intervallo , matrice 256256 , fov 24 c immagini assiali t2 - dipendenti rare , ottenute con la bobina del body , sono state acquisite fino allilo renale per ricercare la presenza di linfoadenomegalie lombo - aortiche . 
i parametri utilizzati sono stati : tr / te 4000 / 90 ms , spessore di scansione 8 mm , intervallo 1 mm , matrice 256192 , fov 40 cm . analisi delle immagini snr was determined by measuring t2 signal intensity in le immagini rm sono state analizzate in maniera prospettica 1148 radiol med ( 2008 ) 113 : 11431156 a region of interest ( roi ) placed over the recurrence , taking care to avoid other tissues , whereas background signal intensity was measured in an area unaffected by movement or respiratory artefacts . 
 for the evaluation of enlarged pelvic lymph nodes , all detected nodes were considered to be positive in view of the fact that all patients had previously undergone pelvic lymph node dissection . 
in contrast , when evaluating enlargement of lumboaortic lymph nodes , we used a size of 1 cm in short axis diameter as a cutoff to differentiate between reactive and metastatic lymph nodes . 
 the 3d volume of the tumour recurrence was calculated on mr images using an ellipsoid formula [ 22 ] : volume , v = 4 / 3a / 2b / 2c / 2 = 0.52 abc where a , b and c are the orthogonal dimensions . posttreatment mr images were compared with those obtained before treatment by analysing the following parameters : t2 signal intensity of the lesion relative to adjacent muscle ( hypointense , isointense , hyperintense ) ; changes in signal intensity of the recurrence with respect to pretreatment images ; presence / absence of mass effect ; dimensions of recurrence ; invasion of adjacent organs ( ureters / bladder , rectum , vessels ) ; presence of thrombosis of the iliac vessels ; enlarged pelvic or lumboaortic lymph nodes . response to concurrent chemoradiation was classified into four groups [ 23 ] based on the comparison of tumour size on the preand posttreatment images : complete response ( > 90% tumour shrinkage ) ; partial response ( > 50% ) ; no change ( < 25% ) and progression . 
all parameters of the recurrence were analysed on mr images obtained 45 days after treatment and again on those obtained at each follow - up mr examination . statistical analysis curves for local control , survival and disease - free interval were calculated according to the kaplan - meier actuarial method using the histopathological confirmation of carcinoma obtained at the beginning of the treatment [ 24 ]  . differences in survival in relation to volume and relapse site were assessed by the log - rank test [ 25 ] and cox proportional hazards method [ 26 ]  . results pretreatment mr images recurrences appeared hyperintense relative to surrounding muscle on t2 - weighted images in 22 / 22 ( 100% ) patients ; da due radiologi ( rm , sb ) , con esperienza di rm pelvica ( > 10 e > 6 anni , rispettivamente )  . 
le immagini rm pre - trattamento sono state analizzate considerando i seguenti parametri : intensit del segnale della lesione , nelle immagini t2 - dipendenti , a confronto con lintensit di segnale del tessuto muscolare adiacente ( ipointensa , isointensa , iperintensa ) ; rapporto segnale - rumore medio della recidiva e del tessuto muscolare ; presenza / assenza di effetto massa della lesione ; sede della recidiva pelvica ; infiltrazione degli organi adiacenti ( ureteri / vescica , retto , vasi ) ( valutati come obliterazione dellipointensit di segnale della parete , nelle immagini t2 - dipendenti ) ; presenza di trombosi dei vasi iliaci e presenza di linfoadenomegalie pelviche o lombo - aortiche . la sede della recidiva stata classificata come segue : recidiva vaginale limitata alla parete vaginale o alla mucosa vaginale , cupola vaginale senza estensione alla parete pelvica , cupola vaginale con estensione alla parete pelvica , parete pelvica . per la valutazione del rapporto segnale - rumore stata misurata lintensit di segnale nella immagini t2 - dipendenti , ponendo il cursore ( region - of - interest , roi ) sulla recidiva , evitando altri tessuti , mentre lintensit di segnale del rumore di fondo stata misurata in unarea scevra da artefatti da movimento / respiro . 
 per la valutazione delle linfoadenomegalie pelviche sono stati considerati positivi tutti i linfonodi osservati , in considerazione del fatto che tutte le pazienti erano state precedentemente sottoposte a linfadenectomia ; mentre per le linfoadenomegalie lombo - aortiche stato impiegato il criterio di 1 cm secondo lasse minore per la diagnosi differenziale tra linfonodi reattivi e metastatici . 
 il volume tridimensionale ( 3d ) della recidiva , inoltre , stato calcolato sulle immagini rm usando una formula dellellissoide [ 22 ] : volume , v = 4 / 3a / 2b / 2c / 2 = 0 , 52 abc dove a , b e c sono le misure ortogonali . 
 isointensa , le immagini rm dopo trattamento sono state confrontate con quelle pre - trattamento analizzando i seguenti parametri : intensit del segnale sulle immagini t2 - dipendenti della lesione a confronto con il muscolo adiacente ( ipointensa , cambiamenti dellintensit di segnale della recidiva a confronto con le immagini pre - trattamento ; presenza / assenza di effetto massa ; dimensioni della recidiva ; infiltrazione degli organi adiacenti ( ureteri / vescica , retto , vasi ) ; presenza di trombosi dei vasi iliaci e di linfoadenomegalie pelviche o lombo - aortiche . iperintensa ) ; la risposta al trattamento radio - chemioterapico concomitante stata classificata in 4 gruppi : risposta completa ( riduzione del tumore > 90% ) ; risposta parziale ( > 50% ) ; radiol med ( 2008 ) 113 : 11431156 1149 fig . 
2a , b small ( < 50 mm3 ) recurrence of squamous cell carcinoma of the uterine cervix located on the vaginal vault without extension to the pelvic sidewall : axial and coronal t2 - weighted rapid acquisition with relaxation enhancement ( rare ) images . 
2a , b neoplasia recidiva di carcinoma squamoso della cervice uterina , alla cupola vaginale di piccolo volume ( < 50 mm3 ) , senza estensione alla parete pelvica : immagini assiali e coronali t2 - dipendenti rapid acquisition with relaxation enhancement ( rare )  . 
la rm della pelvi dimostra una lesione iperintensa , con margini irregolari della cupola vaginale ( freccia ) nelle immagini assiali ( a tr / te 4000 / 85 ms ) e coronali ( b tr / te 4000 / 90 ms ) t2 - dipendenti rare . mean snr of recurrences was 7.041.99 , whereas that of muscle was 3.090.76. 
 analisi statistica le curve di controllo locale , di sopravvivenza e di intervallo libero da malattia sono state calcolate secondo il metodo attuariale di kaplan - meier utilizzando la conferma istopatologica di carcinoma effettuata allinizio del trattamento [ 24 ]  . 
le differenze nelle curve di sopravvivenza , per quanto riguarda il volume e la sede della recidiva , sono state valutate attraverso il test di log - rank [ 25 ] ed il modello di cox proportional hazard [ 26 ]  . risultati immagini rm pre - trattamento la recidiva di tumore risultata iperintensa nelle immagini t2 dipendenti , rispetto al muscolo adiacente , in 22 / 22 ( 100% ) pazienti ; la media del rapporto segnale - rumore ( rsr ) della recidiva stata di 7 , 041 , 99 , mentre del tessuto muscolare stata di 3 , 090 , 76 . 
uninfiltrazione degli organi adiacenti stata rilevata in 9 / 22 ( 41% ) pazienti : in 8 / 22 ( 36% ) paziente la recidiva infiltrava il tratto distale delluretere , mentre in 1 / 22 pazienti coinvolgeva i vasi iliaci . nessuna paziente ha presentato infiltrazione della vescica , o del retto , n trombosi delle vene iliache . 
il volume medio della recidiva , calcolato sulle immagini rm pre - trattamento , stato di 38 , 83 cm3 ( range 0 , 29302 , 49 cm3 )  . 
 immagini post - trattamento nelle immagini rm dopo - trattamento , la lesione risultata ipointensa , rispetto al muscolo adiacente , in 19 / 22 ( 86% ) 1150 radiol med ( 2008 ) 113 : 11431156 fig . 
3a - c large ( > 50 mm3 ) vaginal recurrence from endometrial adenocarcinoma , with partial response to chemoradiation : axial and sagittal t2weighted rapid acquisition with relaxation enhancement ( rare ) images . axial ( a tr / te 4 , 000 / 85 ms ) and sagittal ( b tr / te 3800 / 90 ms ) magnetic resonance images show recurrent uterine cancer to the vaginal vault ( arrow in a ) with mass effect , as indicated by the distension of the vaginal lumen ( arrow in b )  . 
3a - c recidiva vaginale di adenocarcinoma dellendometrio di grande volume ( > 50 mm3 ) , con risposta parziale al trattamento radio - chemioterapico concomitante : immagini assiali e coronali t2 - dipendenti rapid acquisition with relaxation enhancement ( rare )  . 
le immagini di rm , lungo il piano assiale ( a tr / te 4000 / 85 ms ) e sagittale ( b tr / te 3800 / 90 ms ) dimostrano una recidiva di neoplasia dellutero alla cupola vaginale ( freccia in a ) con effetto massa , come indicato dalla distensione del lume vaginale ( freccia in b )  . 
infiltration of adjacent organs was seen in 9 / 22 ( 41% ) patients : the distal ureter was involved in 8 / 22 ( 36% ) and the iliac vessels in 1 / 22 . 
4a - d vaginal vault recurrence from squamous cell carcinoma of the uterine cervix , extending to the pelvic sidewall , before ( a , b ) and after ( c , d ) concurrent chemoradiation . 
on pretreatment ( april 2002 ) , coronal ( a tr / te 4 , 000 / 90 ms ) and axial ( b tr / te 4 , 000 / 85 ms ) t2 - weighted rapid acquisition with relaxation enhancement ( rare ) images , a pelvic recurrence is detected centred on the vaginal vault ( arrowhead ) and extending to the right pelvic vessels ( arrows )  . 
on posttreatment ( january 2003 ) axial ( c tr / te 4 , 000 / 85 ms ) and coronal ( d tr / te 4 , 000 / 90 ms ) t2 - weighted images , the tumour recurrence is reduced in size and is hypointense compared with muscle ( arrows ) , suggesting complete response to chemoradiation . 
4a - d recidiva di carcinoma squamo - cellulare della cervice dellutero alla cupola vaginale , con estensione alla parete pelvica , prima ( a , b ) e dopo radio - chemioterapia concomitante ( c , d )  . 
nelle immagini t2 - dipendneti rare coronale ( a tr / te 4000 / 90 ms ) ed assiale ( b tr / te 4000 / 85 ms ) pre - trattamento ( aprile 2002 ) , si osserva una recidiva pelvica con epicentro nella cupola vaginale ( testa di freccia ) ed estensione ai vasi pelvici di destra ( frecce )  . nelle immagini t2 - dipendenti rare assiale ( c ; tr / te 4000 / 85 ms ) e coronale ( d ; tr / te 4000 / 90 ms ) post - trattamento ( gennaio 2003 ) , si osserva una riduzione delle dimensioni della recidiva neoplastica , che risulta ipointensa rispetto al tessuto muscolare adiacente ( frecce ) , indicativo di risposta completa al trattamento radio - chemioterapico concomitante . 
fivenon hanno mostrato ripresa malattia ( ned ) e 7 / 22 ( 32% ) pazienti sono vive con malattia ( awd ) ; 3 / 22 ( 14% ) pazienti sono decedute a causa della recidiva tumorale . 
le pazienti con recidiva 1152 radiol med ( 2008 ) 113 : 11431156 tumorale 50 mm3 hanno mostrato una tendenza migliore alla sopravvivenza libera da malattia rispetto alle pazienti con volumi tumorali > 50 mm3 ( p < 0 , 1 )  . 
inoltre la sede della recidiva ha mostrato un ruolo sulla prognosi : le pazienti con recidiva tumorale limitata alla vagina ed alla cupola vaginale hanno mostrato risultati di controllo loco - regionale della malattia migliori rispetto alle pazienti con recidiva localizzata alla parete pelvica ; questa differenza , tuttavia , non risultata significativa . 
recentemente , le procedure alternative per mantenere lintegrit degli sfinteri , sono state proposte , ma i risultati a lungo termine di questo tipo di chirurgia resettiva non sono conosciuti [ 27 ]  . 
la radiochemioterapia concomitante stata recentemente suggerita per il trattamento delle recidive dellutero , in considerazione della sua efficacia nel trattamento del carcinoma localmente avanzato della cervice uterina [ 29 , 30 ]  . 
questi risultati migliori possono essere legati alleffetto di sensibilizzazione della chemioterapia ; per di pi leffetto sinergico dei due regimi terapeutici pu anche spiegare la bassa tossicit segnalata nella nostra serie ( tabella 1 )  . 
secondo le immagini rm , 14 / 22 ( 63% ) pazienti mostravano recidive pelviche centrali ( vagina e cupola vaginali ) , che sono associate con una prognosi migliore secondo alcuni autori [ 2 , 3 , 6 , 8 , 9 ]  . nella nostra esperienza , inoltre , abbiamo trovato la tendenza verso una prognosi migliore delle pazienti con recidive vaginali o della cupola vaginale , rispetto alle pazienti con recidiva pelvica , tuttavia questa differenza non risultata significativa . 
questa discrepanza fra la nostra serie e le altre , probabilmente legata al limitato follow - up di alcune pazienti della nostra casistica ( follow - up 3 mesi4 , 8 anni ) e probabilmente tale differenza raggiunger importanza statistica con ulteriori follow - up , in accordo con la serie sopraccennata , diversamente da altri autori , che dichiarano che la sede vaginale della recidiva non presenta valore prognostico [ 29 ]  . la multiplanariet della rm permette di fare un calcolo fig . 
5 large ( > 50 mm3 ) tumour recurrence of the pelvic sidewall from squamous cell carcinoma of the uterine cervix : coronal t2 - weighted rapid acquisition with relaxation enhancement ( rare ) image . 
on coronal ( tr / te 4 , 000 / 90 ms ) t2 - weighted rare images , a pelvic recurrence is detected centred on the right pelvic sidewall infiltrating the right ureter and the iliac vessels ( arrows )  . 
5 recidiva di neoplasia da carcinoma squamoso della cervice uterina alla parete pelvica , di grande volume ( > 50 mm3 ) : immagine coronali t2dipendente rapid acquisition with relaxation enhancement ( rare )  . nellimmagine coronale t2 - dipendnete rare ( tr / te 4000 / 90 ms ) , si osserva una recidiva di neoplasia con epicentro sulla parete pelvica di destra , che infiltra luretere ed i vasi iliaci omolaterali ( frecce )  . 
6 controllo loco - regionale a 5 anni , sopravvivenza libera da malattia e sopravvivenza delle pazienti con recidiva di neoplasia uterina , sottoposte a trattamento radio - chemioterapico concomitante . 
7a , b controllo locale ( a ) e loco - regionale ( b ) delle recidive di neoplasia uterina , in base al volume tumorale . 1154 radiol med ( 2008 ) 113 : 11431156 [ 27 ]  . 
 is not known sphincter preservation have recently been proposed , but the long - term outcome intensive chemotherapy can provide good results but is nonetheless highly toxic [ 28 ]  . 
concurrent chemoradiation has recently been proposed for treating endometrial cancer recurrences on the grounds of its effectiveness in treating locally advanced cervical cancer [ 29 , 30 ] and has been shown to provide good results in these patients [ 30 ]  . 
these results may be radiosensitising effect of chemotherapy , a synergistic effect of the two regimens that may also account for the low toxicity reported in our series ( table 1 )  . 
 related the in view of their intrinsic high - contrast resolution , mr images are very accurate in evaluating the site and extension of pelvic recurrence [ 31 ]  . 
based on mr imaging , 14 / 22 ( 63% ) patients had central pelvic recurrences ( vagina and vaginal vault ) , which are associated with a more favourable prognosis [ 2 , 3 , 6 , 8 , 9 ]  . 
in our study , patients with recurrences involving the vagina or vaginal vault were more likely to have better outcomes than those with pelvic recurrences , although the difference was not statistically significant . 
the discrepancy between our finding and previous studies is probably related to the short follow - up of some of our patients ( 3 months to 4.8 years ) , and the difference may well reach statistical significance with further follow - up . should this be the case , our findings would agree with those of the previously cited study but disagree with other authors who claim that the vagina as a site of relapse has no prognostic value [ 29 ]  . the multiplanar capabilities of mr imaging allow 3d determination of the volume of the relapse . 
relapse site and dimensions can also guide decisions as to whether to deliver the boost dose with ldr for vaginal recurrences or recurrences within 5 mm of the vaginal vault , or with ebrt for pelvic recurrences or those located > 5 mm from the vaginal vault . table 1 acute toxicity after concurrent chemoradiation toxicity grade gastrointestinal skin vaginal rectal vesical haematological gastrointestinale cute vaginale rettale vescicale ematologica tabella 1 tossicit acuta dopo radio - chemioterapia concomitante tossicit grado tridimensionale ( 3d ) del volume della recidiva . 
il volume 3d stato misurato sulle immagini rm , ed ha mostrato una buona correlazione con le misure dellanatomia patologica nel caso di carcinoma squamoso della cervice uterina . lapplicazione di tale metodo permette una valutazione pi precisa del volume del tumore per progettare la radioterapia e per valutare la risposta al trattamento . 
per di pi la valutazione 3d del volume , pu permettere di adattare un trattamento radiante , per risparmiare il pi possibile il tessuto normale ed aumentare la dose sulla recidiva migliorando cos la percentuale di risposta . 
la sede e le dimensioni della neoplasia recidiva , permettendo di decidere se eseguire un ulteriore dose di radioterapia mediante brachiterapia ( ldr ) , per le recidive vaginali o entro 5 mm dalla cupola vaginale , oppure mediante fasci esterni ( ebrt ) per le recidive pelviche o > 5 mm dalla cupola vaginale . abbiamo raggruppato insieme tumori recidivanti con differenti istotipi : carcinoma squamoso originante dalla radiol med ( 2008 ) 113 : 11431156 1155 we grouped together tumour recurrences of different histological types : cervical squamous cell carcinoma and endometrial adenocarcinoma . 
however , in planning radiotherapy , there is a medical need to define disease extent and calculate the target volume , and after treatment , to assess changes in tumour volume . 
these parameters are all independent of histological type . in our series , mr imaging helped us to stage tumour recurrence in order to plan treatment and assess response to chemoradiation . 
mr imaging may also assist in identifying factors likely to affect outcome and thus help stratify patients according to prognostic factors and modulate treatment accordingly . cervice uterina , e adenocarcinoma dellendometrio . 
ci rappresenta un limite per il nostro studio dal momento che il comportamento biologico differente per questi tumori . tuttavia nella programmazione della terapia radiante la necessit medica quella di definire lestensione della malattia e di calcolare il volume bersaglio e , dopo il trattamento valutare le modificazioni del volume tumorale , tutti parametri questi che sono indipendenti dallistotipo . nella nostra casistica la rm in grado di stadiare la recidiva del tumore per pianificare il trattamento e per valutare la risposta tumorale dopo radio - chemioterapia concomitante . 
starting with a review of basic anatomy unchanged and indispensable the book goes on to address the principles of ct and mr imaging , illustrate finer ct and mr anatomy with hundreds of images and diagrams , and provide an orderly description of each disease complete with definitions , aetiopathogenesis and basic elements of semeiotics . the ct images are impressive and the mr images cover a large number of cases , some of which are provided by other radiologists and otoneurosurgeons , and all are perfectly incorporated into the main focus of the book ; and all the figures are accompanied by extensive and complete legends . it is difficult to find any shortcomings of this presentation of diagnostic imaging of the ear . 
diagnostic imaging of the ear by mario di egidio will no doubt become a very useful con molto piacere presento ai radiologi italiani , attraverso la nostra radiologia medica , il libro realizzato da mario di egidio . 
dopo la conclusione della sua lunga e prestigiosa attivit professionale di radiologo , entra di diritto nella biblioteca di qualsiasi medico interessato alle malattie dellorecchio , sia esso specialista in radiologia , otorinolaringoiatria , neurochirurgia , neurologia . il testo certamente il pi completo disponibile in lingua italiana e nelle sue oltre 300 pagine lautore dimostra la sua padronanza dellargomento e il suo aggiornamento ai progressi tecnologici pi recenti della diagnostica per immagini . nei 13 capitoli , corredati da migliaia di immagini , vengono presentate : lanatomia dellosso temporale , la tecnica tc / p , lanatomia in tc ed rm , le strutture vascolari e nervose , la diagnostica per immagini della patologia dellorecchio esterno , medio ed interno , le fratture dellosso temporale , la diagnosi delle lesioni dellangolo ponto - cerebellare , dellapice petroso e del nervo facciale ed infine i paragangliomi . il maggior pregio dellopera di di egidio la completezza . 
si parte dalle conoscenze anatomiche di base immutabili ed indispensabili si passa attraverso i principi della tc e della rm , si illustra con centinaia di immagini e schemi la fine anatomia tc ed rm e per ogni patologia vengono fornite ordinatamente al lettore definizione , eziopatogenesi , elementi essenziali di semeiotica . liconografia tc impressionante e quella rm arricchita dai numerosi casi , forniti anche da altri radiologi e oto - neurochirurghi , casi che sono perfettamente integrati nel filo conduttore del libro . 
difficile trovare lacune nella trattazione della diagnostica per immagini dellorecchio e tutte le figure sono corredate da didascalie ampie e complete , il testo di mario di egidio sar un utilissimo e piacevole compagno per tutti gli oto - radiologi ma rappresen1242 radiol med ( 2008 ) 113 : 12411242 and readable companion for all otoradiologists , but it also provides an example of how the combination of experience , passion and unfailing dedication produces the best results , regardless of an authors age and available resources . ta anche lesempio di come la combinazione di esperienza , passione e tanto , tanto impegno conduce ai migliori risultati , ben al di l dellet anagrafica e dei mezzi a disposizione . cesare colosimo dipartimento di bio - immagini e scienze radiologiche , sezione di radiodiagnostica , universit cattolica del sacro cuore , policlinico a . 
gandini2 1struttura complessa fisica sanitaria i , aso san giovanni battista e della citt di torino ( molinette ) , corso bramante 88 / 90 , 10126 torino , italy 2scdu radiodiagnostica 4 , radiologia diagnostica e interventistica universit di torino , aso san giovanni battista e della citt di torino ( sede molinette ) , via genova 3 , 10126 torino , italy correspondence to : o . 
on the basis of these data , the effective dose ( ed ) was calculated using simulation software based on the monte carlo method for determining the absorbed dose to organs . 
le valutazioni sono state effettuate per 39 esami , su di un campione di pazienti costituito da 32 donne e 7 uomini , con peso medio di 117 kg ( intervallo 68175 kg ) e con indice di massa corporeo medio di 43 , 7 ( intervallo 22 , 254 , 9 )  . 
i pazienti operati nellarco di tempo della durata dello studio sono stati sottoposti a controllo radiologico post - operatorio tra la ii e la vii giornata mediante somministrazione per os di circa 70 ml di mdc iodato idrosolubile ( gastrografin ) e acquisizione di radiogrammi eseguiti dapprima in ortostatismo in proiezione ap , obliqua destra e sinistra e successivamente a paziente supino . 
per lintera durata di ciascuna procedura sono state registrate le condizioni di esposizione e i valori di prodotto dose per area ( dap ) e di dose di ingresso al paziente ( esd )  . 
sulla base dei dati rilevati stato effettuato un calcolo della dose efficace ( ed ) al paziente utilizzando un programma di calcolo basato sul metodo monte carlo per la stima della dose assorbita agli organi . 
when performing radiological contrast studies in patients with morbid obesity , every possible precaution should be taken to minimise patient dose . special care should be taken to evaluate justification of the radiological procedure . keywords radiological contrast studies obese patients patient dose che il passaggio da spessori analoghi a quelli dei pazienti normotipo a quelli dei pazienti oggetto dello studio pu comportare un aumento di dose di un fattore quattro . 
nellesecuzione di esami contrastografici in pazienti obesi occorre adottare tutte le precauzioni possibili per ridurre al minimo la dose al paziente . particolare attenzione deve essere posta alla giustificazione dellesame . parole chiave esami radiologici contrastografici pazienti obesi dose al paziente introduction introduzione obesity is a morbid condition that has recently become so widespread as to be recognised as a social disease . 
the ineffectiveness of medical therapy alone , mainly in the form of pharmacotherapy and psychiatric support , in a relatively high proportion of obese individuals has led to the widespread use of bariatric surgery . 
bariatric surgery is based on the following techniques : vertical banded gastroplasty ( vbg ) , roux - en - y gastric bypass ( rygbp ) , adjustable silicone gastric banding ( asgb ) and biliopancreatic diversion ( bpd )  . 
this pouch is continuous with the oesophagus and communicates with the remaining portion of the stomach through a tight orifice ( neopylorus ) , with an inner diameter of approximately 1 c the neopylorus is reinforced by a polypropylene band to prevent dilatation . 
vbg reduces calorie intake thanks to the early feeling of satiety resulting from the small size of the gastric pouch . rygbp surgery involves dividing the stomach with a linear stapler to create an isolated proximal gastric pouch of 3050 cm3 , with an antecolic gastrojejunal anastomosis and a roux - en - y enteroenteral anastomosis . asgb is a gastric restriction procedure in which a small biocompatible band is positioned around the proximal portion of the stomach to create a gastric pouch of approximately 50 cm3 in volume . 
injection of a radiopaque isotonic solution or saline through the reservoir allows the diameter of the pseudopylorus to be calibrated . bpd ( scopinaro procedure ) is a complex malabsorption lobesit diventata ormai uno stato morboso che , negli ultimi anni , ha assunto le caratteristiche di malattia sociale . in un numero piuttosto elevato di obesi la sola terapia medica , costituita prevalentemente dalla terapia farmacologica e dal supporto psichiatrico , risulta inefficace e da tale insuccesso deriva la grande diffusione della chirurgia bariatrica . 
la chirurgia dellobesit si basa sugli interventi di gastroplastica verticale ( vbg ) , di bypass gastrico su ansa alla roux ( rygbp ) , di banding gastrico ( asgb ) e di diversione bilio - pancreatica ( bpd )  . 
 la gastroplastica verticale , introdotta da mason nel 1980 [ 1 ] , un intervento di riduzione della capacit gastrica che prevede la creazione , mediante lutilizzo di suturatici meccaniche , di una tasca gastrica del volume di 30 ml in continuit con lesofago e comunicante con la restante porzione dello stomaco tramite uno stretto orifizio , neopiloro , del calibro interno di circa 1 cm ; il neopiloro rinforzato con una benderella di polipropilene al fine di evitarne la successiva dilatazione . 
 il bypass gastrico consiste invece nella creazione di una tasca gastrica prossimale isolata della capacit di 3050 cc , con il confezionamento di una gastro - digiuno anastomosi antecolica e di una entero - entero anastomosi su ansa alla roux , mediante lutilizzo di una suturatrice lineare in grado di sezionare lo stomaco . il bendaggio gastrico un intervento di tipo restrittivo che consiste nel posizionamento di una banderilla di materiale biocompatibile attorno alla porzione craniale dello stomaco al fine di creare una tasca gastrica del volume di radiol med ( 2008 ) 113 : 12291240 1231 procedure that is not always reversible and seldom implemented . 
it involves reducing the volume of the gastric cavity by partial resection and creating a gastroenteral anastomosis to exclude the duodenum and jejunum from the alimentary canal to induce malabsorption of dietary fat . indications for surgery are a body mass index ( bmi ) in excess of 40 kg / m2 or of 35 kg / m2 associated with obesityrelated disorders or with complications or failures of previous bariatric surgery [ 2 ]  . contrast - enhanced radiological studies are obtained in the immediate postoperative period or in the later follow - up to document the morphological and functional outcome of the procedure and identify possible complications ( fistulas , stenoses , anastomotic dehiscence ) [ 3 ]  . 
in particular , it is well known that the exposure parameters needed to ensure adequate image quality in obese patients are characterised by higher kv and ma values than those used in normal - size patients , with faster absorption of skin dose and higher values of effective dose [ 5 ]  . 
 the purpose of this study was to evaluate the dose delivered to patients during contrast - enhanced imaging studies performed after vbg or rygbp surgery for pathological obesity . materials and methods between october and december 2006 , 39 contrastenhanced studies were carried out in 39 patients who had undergone bariatric surgery , and specifically vbg ( n = 24 ) and rygbp ( n = 15 )  . 
liniezione di una soluzione radio - opaca isotonica o di una soluzione salina attraverso il reservoir consente di calibrare il diametro dello pseudopiloro . la diversione biliopancreatica ( intervento di scopinaro ) fa parte degli interventi chirurgici di tipo malassorbitivo , una procedura complessa , non sempre reversibile , raramente applicata . 
essa consiste nella riduzione di volume della cavit gastrica mediante una resezione parziale e nel successivo confezionamento di una gastro - entero anastomosi che esclude il duodeno ed il digiuno dal transito alimentare causando il malassorbimento soprattutto dei grassi alimentari . le indicazioni al trattamento chirurgico sono rappresentate da un indice di massa corporea ( body mass index , bmi ) superiore a 40 kg / m2 o a 35 kg / m2 in presenza di patologie associate allobesit oppure da complicanze o insuccessi di una precedente chirurgia bariatrica [ 2 ]  . gli esami radiologici con mezzo di contrasto , eseguiti nellimmediato post - operatorio o a distanza , consentono di documentare gli esiti morfologici e funzionali dellintervento e le eventuali complicanze ( fistole , stenosi , deiescenze anastomotiche ) [ 3 ]  . 
in particolare noto che per i pazienti obesi i parametri di esposizione necessari a garantire un adeguata qualit dellimmagine sono caratterizzati da valori di kv e di ma maggiori di quelli impiegati per i pazienti normotipo , con un accumulo pi rapido di dose alla cute e con valori maggiori di dose efficace [ 5 ]  . 
 lo scopo di questo lavoro stato quello di valutare la dose al paziente nel corso di esami contrastografici eseguiti in pazienti sottoposti ad interventi chirurgici di gastroplastica o di bypass gastrico per obesit patologica . materiali e metodi nel trimestre compreso tra ottobre e dicembre 2006 sono stati eseguiti 39 esami contrastografici in altrettanti pazienti sottoposti ad interventi chirurgici per il trattamento dellobesit di cui 24 vbg e 15 rygbp . 
il campione di pazienti era composto da 32 femmine e 7 maschi , di et compresa fra 1860 anni ( media 43 anni , mediana 41 anni ) , con peso di 68175 kg ( medio 117 kg , mediano 113 kg ) , e indice di massa corporeo compreso nellintervallo 22 , 254 , 9 ( medio 43 , 7 , mediano 44 , 1 )  . 
le procedure sono state eseguite con un apparecchio telecomandato philips omnidiagnost eleva ( philips medical systems , best , olanda )  . 1232 radiol med ( 2008 ) 113 : 12291240 fig . 
preliminarmente allassunzione del mdc sono sempre stati eseguiti radiogrammi diretti del torace e delladdome ; gli esami contrastografici sono stati eseguiti sia in orto sia in clinostatismo nelle proiezioni antero - posteriore , obliqua destra e sinistra con proiezioni aggiuntive ogniqualvolta queste si siano rese necessarie per dimostrare complicanze o dirimere dubbi diagnostici . 
a conclusione dellesame sempre stato eseguito un radiogramma panoramico delladdome per valutare la regolare canalizzazione enterica distale . al fine di determinare le condizioni ottimali di esposizione sono state effettuate misure di dose utilizzando fantocci di plexiglas di diverso spessore per simulare le diverse tipologie di pazienti ; mediante una camera a ionizzazione trasmissiva diamentor m4kdk a doppio canale fig . 
all studies were completed by a panoramic radiograph of the abdomen to radiol med ( 2008 ) 113 : 12291240 1233 ( ptw , freiburg ) sono stati misurati i ratei di prodotto dose per area ( espressi in gy cm2 / s ) e i ratei di dose in ingresso ( espressi in mgy / s ) al variare dei parametri di esposizione selezionati dalloperatore . 
in particolare i ratei sono stati misurati per le diverse tipologie di scopia ( modalit normal e modalit low dose ) , per i diversi diametri e per i relativi ingrandimenti dellintensificatore di brillanza , per la presenza o meno di diaframmi e infine per i diversi spessori del fantoccio . 
le misure sono state eseguite anche in modalit grafia , con acquisizione di immagini ripetute registrando i valori di dap per immagine . le valutazioni di dose in vivo sono state effettuate in termini di dap e di dose superficiale di ingresso ( esd )  . entrambi i dati sono stati forniti direttamente dallapparecchiatura che dotata di camera a ionizzazione trasmissiva integrata . 
sulla base dei valori di esd ottenuti stato possibile valutare se questo tipo di esami comportino linsorgenza di danni alla cute , per i quali esistono valori soglia di dose indicati dalla commissione internazionale di radioprotezione [ 6 ]  . per quantificare il rischio stocastico di induzione di tumori letali conseguenti allesposizione stato necessario invece valutare la dose efficace ( e )  . 
per effettuare correttamente il calcolo durante le procedure sono stati registrati i valori di dap per ciascuna proiezione impiegata insieme con i valori di kv , ma , tempo di scopia , numero di immagini in grafia , distanza fuoco paziente , diametro dellintensificatore di brillanza , presenza dei diaframmi e indicazione del punto di ingresso del centro del fascio sul paziente ( e conseguentemente sul fantoccio software impiegato per il calcolo )  . 
per il calcolo della dose agli organi il programma di calcolo ha tenuto conto delle dimensioni reali del paziente desunte sulla base del peso e dellaltezza di ciascuno . risultati nelle figure 4 e 5 sono riportati i valori di dose efficace ottenuti per i diversi diametri dellib ( intensificatore di brillanza ) selezionabili sia per lesposizione in scopia ( msv per minuto ) sia per lesposizione in grafia ( msv per immagine )  . in entrambi i casi si nota un lieve incremento di rateo di dose efficace allaumentare dellingrandimento ( utilizzo dei diametri minori )  . 
passando da un diametro di 38 cm ad uno di 25 cm si ha un aumento di dose efficace per minuto del 12% e un aumento della dose efficace per immagine del fig . 
3 controllo post - operatorio precoce di gastroplastica verticale a paziente supino con regolare opacizzazione del fondo gastrico . evaluate the correct distal intestinal canalisation . to determine the optimal exposure conditions , dose measurements were taken using plexiglas phantoms of different thickness to simulate the various kinds of patients . a double - channel ionisation chamber transmission diamentor m4kdk ( ptw , freiburg ) was used to measure the dose - area product ( dap ) rates ( in gy cm2 / s ) and the entrance skin dose ( esd ) rates ( in mgy / s ) at different exposure setting selected by the operator . 
in particular , the rates were measured for different fluoroscopy modes ( normal and low dose ) , for different image intensifier diameters and magnifications , for the presence or absence of field - limiting diaphragms and for different phantom thicknesses . measurements were also obtained during radiography through the acquisition of repeated images and recording of the dap values for each image . the in - vivo dose assessments involved measuring the dap and esd values . 
on the basis of the esd values , we were able to determine whether these imaging studies exceed the dose threshold for injury to the skin established by the international radiation protection committee [ 6 ]  . to quantify the stochastic risk of radiation - induced fatal tumours , we assessed the effective dose . 
the effective dose was estimated by the pcxmc computer programme ( stuk radiation and nuclear safety authority , helsinki , finland ) , which is based on monte carlo simulations [ 7 ]  . 
to verify the correctness of the calculations made during the 1234 radiol med ( 2008 ) 113 : 12291240 procedures , dap values of each projection were recorded , along with the kv and ma values , fluoroscopy time , number of radiographic images , focuspatient distance , image intensifier diameter , presence of diaphragms and specification of the beam entrance point on the patient ( and , consequently , on the software phantom used for the calculation )  . 
4 and 5 show the effective dose values obtained for the different image intensifier diameters that can be selected for fluoroscopy ( msv per minute ) and radiography ( msv per image )  . 
instead , if we consider the esd , the dose rate increases by 19% for fluoroscopy and by 56% for radiography , for the same change in diameter from 38 cm to 25 cthe smaller variations in effective dose result from the fact that the increase in point dose , related to greater magnification , are in part compensated for by the smaller irradiated field . 
 with regard to the use of diaphragms , we verified that diaphragm closure does not involve significant esd changes but leads to a reduction of the exposed area , hence of the dap and the effective dose , with the changes in 29% . 
se si considera invece la esd gli incrementi di rateo di dose variando il diametro da 38 cm a 25 cm risultano essere del 19% per la scopia e del 56% per la grafia . 
 riguardo lutilizzo dei diaframmi , abbiamo verificato che la chiusura dei diaframmi non comporta grosse variazioni di esd , ma determina una diminuzione dellarea esposta e quindi del dap e della dose efficace , con landamento qualitativo mostrato in figura 6 . 
i valori sono stati ottenuti con un diametro dellib di 38 cm , una distanza fuoco ib di 110 cm e uno spessore del fantoccio di 25 c i ratei di dose efficace al variare dello spessore del fantoccio sono riportati nelle figure 7 e 8 . 
per quanto riguarda la scopia si osservato un brusco aumento nel passaggio da 20 a 30 cm di spessore , mentre si constatato un leggero decremento da 30 a 35 cci dovuto al fatto che gi con 30 cm di plexiglass lapparecchio raggiunge i valori massimi consentiti di 110 kv e di 6 ma . 
i ratei di esd e di dap sono quindi costanti per spessori maggiori di 30 cm e il leggero decremento di dose efficace dovuto alla diversa distribuzione di dose agli organi al variare dello spessore del paziente . 
con 30 cm di spessore il rateo di dose efficace circa 4 volte maggiore di quello che si ottiene con 20 cil comportamento osservato in grafia stato diverso , in quanto i valori dei parametri di esposizione ( in particolare dei mas per singola immagine ) hanno mostrato un incremento anche per spessori maggiori di 30 cpassando da uno spessore di 25 cm ad uno spessore di 35 cm si avuto anche in questo caso un incremento di un fattore 4 sulla dose efficace . 
5 valori di rateo di dose efficace per immagine di grafia per i diversi diametri di ib selezionabili . radiol med ( 2008 ) 113 : 12291240 1235 quality shown in fig . 
the values were obtained with an image - intensifier diameter of 38 cm , a focus - intensifier distance of 110 cm and a phantom thickness of 25 c the effective dose rates for the various phantom thicknesses are shown in figs . 
during fluoroscopy , an abrupt increase in effective dose was observed when passing from a thickness of 20 cm to 30 cm and a slight decrease from 30 cm to 35 c this happens because the system reaches the maximum allowed values of 110 kv and 6 ma , even with 30 cm of plexiglas . 
the esd and dap rates are therefore constant for thicknesses exceeding 30 cm , and the slight decrease in effective dose is due to the different organ dose distribution with changes in patient thickness . 
al variare dello spessore si verificato come un minuto di scopia sia equivalente a circa 10 immagini di grafia per gli spessori pi elevati e a circa 23 immagini per spessori minori . 
si inoltre constatato che i parametri di esposizione scelti in automatico dallapparecchio fanno riferimento ad un paziente identificato sulla base dei dati anagrafici e morfologici inseriti ( data di nascita , altezza e peso ) prima dellinizio dellesame , e presentano unelevata dipendenza dallet del paziente ( paziente neonato , pediatrico o adulto ) , e la possibilit , per i pazienti adulti , i scegliere fra 4 categorie : small , normal , large e extra large . 
la diversa tipologia dei pazienti non condiziona i parametri di esposizione in scopia e i valori scelti dipendono solo dallo spessore , mentre riguardo la grafia , i valori selezionati , anche a parit di spessore , dipendono dal tipo di paziente . 
ne deriva che con uno spessore di 30 cm i valori di kv selezionati sono di 105 per un paziente normal e di 115 per un paziente extra large , tali da ridurre la dose in ingresso e migliorare la qualit di immagine , con una sensibile diminuzione anche in termini di rateo di dose efficace da 0 , 31 msv / immagine a 0 , 28 msv / immagine . 
si verificato che tale modalit dimezza i ma utilizzati e di conseguenza tutte le grandezze dosimetriche , con un effetto peggiorativo sulla qualit dellimmagine e un notevole incremento del rumore . 
8 valori di rateo di dose efficace per immagine di grafia con diversi spessori di fantoccio . 1236 radiol med ( 2008 ) 113 : 12291240 thickness of 30 cm , the effective dose rate is approximately four times greater than that obtained with 20 cthe behaviour observed during radiography was different because the values of the exposure parameters ( especially mas per image ) increased , even with thicknesses exceeding 30 cif the thickness changed from 25 cm to 35 cm , there was again a fourfold increase in effective dose . 
with varying thicknesses , it was confirmed that 1 min of fluoroscopy is equivalent to approximately ten radiographic images for large thicknesses and to approximately 23 radiographic images for small thicknesses . 
it was also found that the exposure parameters automatically selected by the system refer to a patient identified from the personal details and the morphological data entered ( date of birth , height , and weight ) before the examination and are highly dependent on the patients age ( infant , child or adult ) , with the option , for adult patients , to choose among four categories : small , normal , large and extralarge . 
the mean values and standard deviations , the lowest and highest values and the indicators of the statistical distribution in the first and third quartile are specified for each quantity . 
the calculation of these values did not include data from two patients who had undergone surgery a few years earlier and had a bmi less than 30 , the threshold value for obesity . 
 with regard to exposure parameters , we observed a moderate dispersion of the kv and ma values , close to the maximum values allowed by the device , as had been found in the phantom measurements . 
by contrast , there was greater variability in total fluoroscopy time and in the number of images , which depends on several factors that make these studies impossible to standardise in terms of number of projections and duration . 
per ciascuna grandezza sono indicati i valori medi con le relative deviazioni standard , i valori minimi e massimi e gli indicatori della distribuzione statistica di i e iii quartile . 
dal calcolo di questi valori sono stati esclusi i dati relativi agli esami di due pazienti che avendo effettuato lintervento alcuni anni prima presentavano un indice di massa corporeo inferiore a 30 , valore solitamente assunto come soglia per definire lo stato di obesit . 
 riguardo ai parametri di esposizione si nota una dispersione non elevata dei valori di kv e di ma , vicini ai massimi consentiti dallapparecchio , gi evidenziati nelle misure con fantoccio . 
al contrario si apprezza una maggiore variabilit per quanto riguarda il tempo totale di scopia e il numero di immagini , conseguente a diversi fattori che rendono questi esami non standardizzabili come numero di proiezioni e durata di ciascuna procedura . 
 per quanto riguarda lesd si osserva come anche i valori massimi siano stati notevolmente al di sotto della prima soglia di dose alla cute per insorgenza di danni deterministici , che di 2000 mgy corrispondente ad un probabile eritema temporaneo ( riferimento icrp )  . 
tali valori sono stati calcolati a partire dai valori degli incrementi di dap per ciascuna delle proiezioni effettuate per ogni esame , utilizzando il software di simulazione pcxmc considerando i valori reali di altezza e peso . 
i coefficienti che permettono di passare dal dap al valore di e sono quindi differenti per le diverse proiezioni , i diversi valori di kv e le diverse dimensioni dei radiol med ( 2008 ) 113 : 12291240 1237 effects , which amounts to 2 , 000 mgy , corresponding to probable transient erythema ( international commission on radiological protection )  . 
 the effective dose values were relatively high , with a maximum value of 45 msv and 29 msv in the third quartile . these values were derived from the values of the dap increases for each of the projections in each study , using the pcxmc simulation software and considering the real height and weight values . 
however , to verify whether it is possible as a first approximation to consider one conversion coefficient from dap to effective dose only for this type of study and patients , fig . 
the largest difference between the estimated effective dose values and those of the interpolation line is around 65% , whereas 90% of the data show differences below 30% . discussion the measurements in phantoms allowed us to identify the optimal working conditions with regard to patient dose . these conditions were taken into account during the performance of radiological contrast studies : steps were taken to minimise fluoroscopy time and the number of images obtained using the maximum diameter of the image intensifier with field - limiting diaphragms . 
given that contrast studies of the digestive system are among those delivering the highest patient doses , there is a justified concern and effort to optimise study protocols to achieve both diagnostic pazienti . 
tuttavia , al fine di verificare se sia possibile in prima approssimazione considerare un unico coefficiente di trasformazione da dap a e per questa tipologia di esami e di pazienti , in fig . 
la differenza massima tra i valori di e stimati e quelli della retta di interpolazione di circa il 65% , mentre il 90% dei dati presenta differenze inferiori al 30% . discussione linsieme delle misure effettuate su fantoccio ha permesso di identificare le condizioni di lavoro ottimali dal punto di vista della dose al paziente , delle quali si tenuto conto nel corso dellesecuzione degli esami contrastografici : si posta infatti attenzione a ridurre al minimo il tempo di scopia e il numero di immagini effettuate , utilizzando il massimo diametro dellib con campi diaframmati . 
 [ 11 ] hanno dimostrato lutilit , dal punto di vista della riduzione della dose , di una filtrazione aggiuntiva di alcuni decimi di mm di rame [ 7 ]  . nel nostro studio per non stato possibile utilizzare tale espediente in quanto avrebbe comportato un aumento del carico anodico non sopportabile dallapparecchiatura . 
 se si confrontano i valori di dap e di e risultanti dal nostro studio con quelli riferiti in letteratura per esami table 1 summary of results from some dosimetric studies on contrast - enhanced examinations reported in the literature authors patient type fluoroscopy time ( min ) dose - area product ( gy cm2 ) effective dose ( msv ) geleijns [ 8 ] carroll [ 9 ] delichas [ 10 ] martin [ 4 ] standard ( 70 kg male ) 7020 kg 7415 kg 7020 kg 1.77.0 ( minmax ) 756 ( minmax ) 2.519 ( minmax ) 1.54.5 ( minmax ) 31.8 ( meansd ) 1.12.8 ( minmax ) 0.543.7 ( minmax ) 2511 ( meansd ) 213.7 ( minmax ) 8.64 ( meansd ) 0.72.7 ( minmax ) tabella 1 sintesi dei risultati di alcuni studi di dosimetria per esami contrastografici riferiti in letteratura autori indicazioni tipo paziente t scopia ( min ) dap ( gy cm2 ) e ( msv ) geleijns j [ 8 ] standard ( uomo 70 kg ) carroll em [ 9 ] 7020 kg delichas mg [ 10 ] 7415 kg 7020 kg martin cj [ 4 ] 1 , 77 , 0 ( minmax ) 756 ( minmax ) 2 , 519 ( minmax ) 1 , 54 , 5 ( minmax ) 31 , 8 ( mediads ) 1 , 12 , 8 ( minmax ) 0 , 543 , 7 ( minmax ) 2511 ( mediads ) 213 , 7 ( minmax ) 8 , 64 ( mediads ) 0 , 72 , 7 ( minmax ) 1238 radiol med ( 2008 ) 113 : 12291240 quality and dose containment . 
in our study , however , we were unable to implement this measure , as it would have implied increasing the tube load to a level not tolerated by our equipment . 
 if the dap and effective dose values of our study are compared with those in the literature for radiological contrast studies in normal - sized patients , significant differences can be observed . 
the dap and effective dose values show a very high level of dispersion but are approximately lower than those of our study by a factor similar to the one found in phantom measurements between the largest and smallest thicknesses , except in the study by martin et al . 
 to our knowledge , the literature contains only one study of the dosimetric aspects of radiological contrast studies in obese patients [ 12 ] , in whom the reported dap and effective dose values were considerably lower as a result of short examination times and the low tube current used . 
i valori di dap e di e presentano una dispersione molto elevata , ma risultano approssimativamente inferiori a quelli del nostro studio per un fattore simile a quello riscontrato nelle misure in fantoccio tra gli spessori pi grandi e quelli minori , ad eccezione di martin et al . 
 per quanto ci dato conoscere , esiste in letteratura un solo lavoro che riporta dati dosimetrici relativi ad esami contrastografici in pazienti obesi [ 12 ] , in cui i valori di dap e di e riferiti sono notevolmente inferiori , legati ai tempi brevi e ai bassi valori di corrente anodica utilizzati . infatti tali parametri tecnici sono stati impiegati per lo studio prevalentemente di calibrazione di bendaggi gastrici sotto guida radioscopica ( 85% dei casi ) , procedura che solitamente richiede brevi tempi di scopia ed un ridotto numero di acquisizioni radiografiche . come stato sottolineato da bryk [ 5 ] , lesecuzione di esami fluoroscopici in pazienti obesi presenta notevoli difficolt . 
 operators performing this kind of examination must consequently be aware that dose rates are remarkably higher than in normal - sized patients , and they should take all optimisation measures compatible with the performance of the examination . 
 gli operatori che eseguono questo tipo di esame devono pertanto essere consapevoli che i ratei di dose sono notevolmente maggiori di quelli riscontrabili nei pazienti normotipo al fine di poter adottare tutte le misure di ottimizzazione compatibili con lesecuzione dellesame . 
anche il numero e la frequenza degli esami di controllo da eseguire nel follow - up devono essere programmati tenendo conto della dose complessiva che pu derivare dallintero percorso diagnostico . conclusions in our study , we obtained phantom - based and in vivo dose measurements for radiological contrast studies of the gastrointestinal tract in obese patients who had undergone vbg and rygbp . 
for radiation protection purposes , it is essential to enter the height and weight correctly when recording patient data and to conduct the diagnostic investigation as quickly , and acquiring as few radiographs , as possible , collimating the beam on the region of interest and limiting the use of magnification to what is strictly necessary . 
the studies should be carried out during follow - up only when needed to evaluate the postoperative course , and the number of examinations per year should be kept to a minimu acknowledgements this work was supported in part by the research project riduzione del rischio associato allesposizione a radiazioni ionizzanti per fini medici ( reduction of risk associated with exposure to ionising radiation for medical purposes ) compagnia san paolo di torino . conclusioni nel nostro studio abbiamo effettuato misure di dose su fantoccio e in vivo per esami contrastografici del tratto gastro - enterico in pazienti obesi sottoposti a interventi di gastroplastica verticale e bypass gastrico e i risultati ottenuti dimostrano che i valori di dap e di e sono decisamente superiori a quelli valutati per i pazienti normotipo . ai fini protezionistici pertanto necessario inserire correttamente i dati relativi ad altezza e peso al momento della registrazione del paziente e svolgere lindagine diagnostica nel minor tempo possibile , acquisendo il minor numero di grafie possibile , collimando il fascio sulla regione di interesse e limitando luso degli ingrandimenti allo stretto necessario . 
crisi1 1dipartimento di diagnostica per immagine , azienda ospedaliero - universitaria , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , olanda 3dipartimento di radiologia , universit degli studi , verona , italy 4dipartimento di radiologia , universit degli studi , trieste , italy 5dipartimento di radiologia , universit degli studi , palermo , italy 6dipartimento di radiologia , irccs santa lucia , roma , italy correspondence to : f . 
cademartiri , viale rustici 2 , 43100 parma , italy , tel . : + 39 - 052 - 1961833 , e - mail : filippocademartiri@hotmail.com received : 8 august 2007 / accepted : 11 february 2008 / published online : 29 october 2008 springer - verlag 2008 abstract purpose . 
forty - five patients ( 29 men ; mean age 68 ) underwent msct angiography of the abdomen for suspected cmi ( main clinical finding : postprandial abdominal pain )  . 
the scan protocol was detectors / collimation 16 / 0.75 mm ; feed 36 mm / s ; rotation time 500 ms ; increment 0.4 mm ; 120150 mas and 120 kvp . 
a volume of 80 ml of contrast material was administered through an antecubital vein ( rate 4 ml / s ) , followed by 40 ml of saline ( rate 4 ml / s )  . 
images were analysed on the workstation with different algorithms ( axial image scrolling , multiplanar reconstructions , maximum intensity projection , volume rendering )  . targeted central lumen - line reconstructions ( curved reconstructions ) were obtained along the celiac trunk ( cet ) and superior mesenteric artery ( sma )  . 
image generation and interpretation required 25 mstenosis and / or occlusions were detected in 29 ( 65% ) cases on the cet and in 32 ( 71% ) on the sma . 
of those lesions ( n = 61 ) , 44 ( 49% ) were classified as not significant . in 16 ( 35% ) cases , there was a simultaneous stenosis riassunto obiettivo . 
quarantacinque pazienti ( 29 uomini ; et media 68 ) sono stati sottoposti ad angiografia dei vasi addominali mediante msct per sospetta icm ( principale sintomo clinico : dolore addominale post - prandiale )  . protocollo di scansione : detettori / collimazione 16 / 0 , 75 mm ; avanzamento 36 mm / s ; tempo di rotazione 500 ms ; incremento 0 , 4 mm ; mas 120150 e kvp 120 . 
ottanta millilitri di mezzo di contrasto sono stati somministrati per via antecubitale ( velocit : 4 ml / s ) , seguiti da 40 ml di soluzione salina ( velocit : 4 ml / s )  . 
le immagini sono state analizzate mediante workstation con diversi algoritmi ( cinescrolling delle immagini assiali , mpr - ricostruzioni multiplanari reconstructions , mip , maximum intensity projections , vr , volume rendering )  . 
ricostruzioni multiplanari curvate sono state effettuate lungo il tronco celiaco ( tce ) e larteria mesenterica superiore ( ams )  . locclusione e la stenosi significativa ( > 50% ) sono state rilevate . 
la generazione ed interpretazione delle immagini hanno richiesto in media 25 mstenosi e / o occlusione sono state rilevate in 29 ( 65% ) casi sul tce , ed in 32 ( 71% ) casi sullams . 
di queste lesioni ( n = 61 ) , 44 ( 49% ) sono 1136 radiol med ( 2008 ) 113 : 11351142 and / or occlusion of the cet and sma ( confirmed by conventional angiography )  . 
msct angiography can play a major role in the detection of stenosis of the abdominal arteries in patients with suspected cmi . keywords msct angiography chronic mesenteric ischaemia abdominal angina state classificate come non significative . 
in 16 ( 35% ) casi stata osservata una stenosi e / o occlusione simultanea di tce e ams ( confermate con angiografia convenzionale )  . in 6 ( 13% ) casi non vi era alcuna lesione a carico del tce , dellams o dei loro rami principali ( confermato al followup clinico )  . 
langiografia msct pu avere un ruolo importante nella rilevazione delle stenosi dei vasi addominali in pazienti con sospetta icm . parole chiave angiografia tc ischemia cronica mesenterica angina addominale introduction introduzione chronic mesenteric ischaemia ( cmi ) is an uncommon syndrome with a fairly typical clinical presentation . 
the slowly progressive development of postprandial epigastric pain associated with weight loss in an approximately 60year - old patient ( especially one affected by other atherosclerotic conditions ) is strongly suspicious for a vascular insufficiency of the splanchnic circulation . 
the diagnostic approach aims to identify the atherosclerotic obstruction , which is generally located at the origins of the celiac trunk ( cet ) , superior mesenteric artery ( sma ) and inferior mesenteric artery ( ima )  . doppler ultrasound is currently used as a noninvasive method to study the proximal splanchnic vessels , but intraabdominal gas , respiratory movements , obesity and any previous abdominal surgery may hinder or impede the gathering of diagnostic information . 
magnetic resonance angiography ( mra ) has the potential to provide both morphological ( stenosis ) and functional ( flow ) information [ 1 , 2 ]  . noninvasive imaging of the abdominal arteries with fourdetector - row multislice computed tomography ( msct ) has been shown to be effective [ 35 ] in providing a clear depiction of the branches of the sma and cet [ 3 , 5 ]  . 
moreover , msct angiography provides additional information about the surrounding tissues , which may prove crucial for developing the differential diagnosis and planning patient management . new generations of msct scanners with 16 or more detector rows have been commercially available for several years . 
these technical improvements allow accurate depiction of the abdominal vessels down to the most distal branches , with depiction of stenosis , collateral vessels and possibly even characteristics of atherosclerotic plaque . 
il lento sviluppo di un dolore epigastrico post - prandiale , associato con calo ponderale , in un paziente di circa 60 anni di et ( specialmente se caratterizzato da altre patologie aterosclerotiche associate ) , permette di sospettare con elevata probabilit una insufficienza vascolare del circolo splancnico . 
lapproccio diagnostico focalizzato allidentificazione della ostruzione aterosclerotica in genere localizzata allorigine del tronco celiaco ( tce ) , della arteria mesenterica superiore ( ams ) , e della arteria mesenterica inferiore ( ami )  . correntemente , lecotomografia doppler utilizzata come metodo non invasivo per studiare i vasi splancnici prossimali , ma il gas intra - addominale , i movimenti respiratori , lobesit , e qualunque precedente chirurgia addominale pu limitare o impedire la rilevazione delle informazioni diagnostiche . 
langiografia a risonanza magnetica ( angio - rm ) mostra invece un elevato potenziale data la sua capacit di visualizzare informazioni morfologiche ( stenosi ) e funzionali ( flusso ) [ 1 , 2 ]  . 
questi miglioramenti tecnici permettono di effettuare studi accurati dei vasi addominali fino a diramazioni molto distali , potendo definire la presenza di stenosi , circoli collaterali ed eventualmente le caratteristiche delle placche aterosclerotiche . 
basandoci sui recenti sviluppi tecnici e sui precedenti radiol med ( 2008 ) 113 : 11351142 1137 previously reported excellent results , we developed an msct angiography protocol to evaluate patients with suspected cmi . ottimi risultati , abbiamo sviluppato un protocollo per angiografia msct per la valutazione dei pazienti con sospetta ischemia cronica mesenterica ( icm )  . materials and methods materiali e metodi forty - five patients ( 29 men ; mean age 68 years ; age range 2881 ) gave their informed consent to undergo abdominal msct angiography for suspected cmi ( the main clinical finding was postprandial abdominal pain )  . 
the scanning parameters were ( table 1 ) : number of detectors / collimation 16 / 0.75 mm ; effective slice thickness 0.75 mm ; feed 36 mm / s ; rotation time 500 ms ; increment 0.4 mm ; 120150 mas ; 120 kvp . 
a volume of 80 ml of iodinated contrast medium ( visipaque 320 , amersham health , uk ) was administered via a dual - head injector ( stellant , medrad , usa ) through an antecubital vein ( flow rate 4 ml / s ) , immediately followed by a 40 - ml saline flush ( flow rate 4 ml / s )  . 
the estimated radiation dose was approximately 10 msv . quarantacinque pazienti ( 29 uomini ; et media 68 ; range 2881 ) hanno fornito consenso informato e sono stati sottoposti ad angiografica msct delladdome per sospetta icm ( principale reperto clinico : dolore addominale post - prandiale )  . 
i parametri di scansione erano ( tabella 1 ) : numero di dettettori / collimazione 16 / 0 , 75 mm ; spessore effettivo dello strato 0 , 75 mm ; avanzamento 36 mm / s ; tempo di rotazione 500 ms ; incremento 0 , 4 mm ; mas 120150 e kvp 120 . 
un volume di 80 millilitri di mezzo di contrasto iodato ( visipaque 320 , amersham health , regno unito ) stato somministrato con un iniettore automatico a doppia testa ( stellant , medrad , usa ) attraverso una vena antecubitale ( flusso = 4 ml / s ) , seguiti immediatamente da 40 ml di soluzione salina ( flusso = 4 ml / s )  . 
no motion artefacts due to vascular pulsation were observed . the anatomy of the cet and sma and their branches was successfully analysed down to the first generation ( even though possible , analysis beyond the first generation would have had no clinical role in this study )  . 
lanatomia del tce e dellams e dei loro rami stata analizzata agevolmente fino alla prima generazione ( oltre , anche se possibile non avrebbe avuto un ruolo clinico in questo studio )  . 
b after segmentation of the relevant vascular structures , the celiac trunk ( tce on the image ) is visualised with its main branches for the liver and spleen ; the superior mesenteric artery ( ams ) is displayed with all its main branches , including a stenosed ileocolic artery ( arrowhead ) , and also the inferior mesenteric artery ( ami ) and its branches . 
dopo segmentazione delle strutture vascolari di interesse ( b ) , il tronco celiaco ( tce ) visualizzato con i suoi rami principali per il fegato e per la milza , larteria mesenterica superiore ( ams ) visualizzata con tutti i suoi rami principali incluso un ramo ilieo - colico stenotico ( testa di freccia ) , ed anche larteria mesenterica inferiore ( ami ) ed i suoi rami . 
unarcata di riolano ipertrofica ( freccia sottile ) dimostra la presenza di una circolazione collaterale compensatoria tra lams e lami . was simultaneous stenosis and / or occlusion of the cet and sma ( confirmed by conventional angiography )  . 
in six ( 13% ) cases , no lesion was identified on the cet , sma or their branches ( negative finding confirmed by clinical follow - up at 3 and 6 months )  . 
in 12 ( 27% ) cases , we performed a percutaneous interventional procedure ( dilatation and / or stenting ) on the basis of the indication established with msct angiography . 
in five ( 11% ) cases , we performed a double percutaneous procedure involving stenting of the cet and sma and in one case an sma angioplasty . discussion cmi , also known as abdominal angina , is a syndrome due to chronic arterial insufficiency of the intestines . 
ancillary reports state that 18% of patients older than 65 years have mesenteric arterial stenosis 50% , even though only a small minority of them are symptomatic [ 7 , 8 ]  . tce e ams ( confermata dalla ac )  . 
in 6 ( 13% ) casi nessuna lesione era presente sul tce , ams o sui loro rami visualizzati ( reperto negativo confermato al follow - up clinico a 3 e 6 mesi )  . 
in 5 ( 11% ) casi stata effettuata una doppia procedura percutanea di stenting del tce e dellams , ed in un caso un angioplastica dellams . discussione lischemia cronica mesenterica ( icm ) , anche nota come angina addominale , una sindrome da insufficienza arteriosa cronica dellintestino . 
casistiche ancillari affermano che il 18% dei pazienti al di sopra dei 65 anni di et porta una stenosi 50% delle arterie mesenteriche , anche se una quota molto bassa di questi mostra sintomi [ 7 , 8 ]  . licm causata tipicamente da una stenosi / occlusione del tce , della ams , e della ami . 
the degree of stenosis or obstruction capable of determining clinical symptoms of each single artery varies and probably depends on anatomical configuration , rate of progression of the stenotic or obstructive process and the presence of collateral vessels . generally , all three vascular axes are variably occluded or stenotic . 
in fact , because of extensive collateral vessels between the vascular territories of the three main splanchnic arteries , abdominal angina tends to occur whenever at least two of the three vessels are obstructed . the atherosclerotic obstruction is usually located at the level of the cet and sma . 
complications such as bowel infarction or malnutrition are responsible for the high morbidity and mortality rates and determine the need for treatment . the hallmark of cmi is a characteristic intermittent dull or cramping epigastric and / or paraumbilical pain arising 1560 min after meals and lasting for several hours . the pain may be relieved by defecation . 
other associated signs and symptoms include constipation , flatulence and diarrhoea with or without some blood admixture . significant weight loss is observed over time and is primarily due to reduced food intake ( fear of eating )  . chronic ischaemia may also produce mucosal damage with loss of absorptive surface , which in turn aggravates the weight loss . 
if doubts persist about the nature of the diagnosis , quantitative mapping of portal flow with mri before and after a standard test meal may demonstrate the lack of normal postprandial increase in portal flow volume [ 1 , 2 ]  . the consecutive series selected on the basis of clinical findings of postprandial abdominal pain demonstrates the robustness of the msct technique and technology for evaluating the abdominal splanchnic vessels . 
the relatively pure patient population characterised by exclusively atherosclerotic stenoses ( in one unusually young patient , the clinical suspicion was supported by familial hypercholesterolaemia ) showed a prevalence of lesions > 60% on each of the major arterial axes ( cet and sma ) , for a total of about half of the visualised arteries being affected by stenosis or occlusions . 
il grado stenosi / occlusione capace di produrre sintomi clinici per ogni singolo asse vascolare variabile e probabilmente dipende dalla configurazione anatomica individuale , dalla velocit di progressione del processo stenotico / occlusivo e dalla presenza di circoli collaterali . 
generalmente , tutti e tre gli assi vascolari sono variabilmente occlusi / stenotici . infatti , a causa dellestensiva presenza e formazione di circoli collaterali tra i territori vascolari dei tre principali assi splancnici , langina addominale insorge pi comunemente quando almeno due dei tre vasi sono ostruiti . 
linsorgenza di complicazioni come linfarto intestinale e la malnutrizione sono le cause dellelevata morbidit e mortalit e della necessit di trattamento . il quadro patognomonico della icm caratterizzato da un dolore addominale intermittente epigastrico e / o paraombelicale di tipo gravativo o crampiforme che insorge da 15 a 60 minuti dopo un pasto , e si prolunga per diverse ore . il dolore pu essere alleviato dalla defecazione . 
meno di frequente possono essere presenti nausea e vomito . la diagnosi si basa sullidentificazione di stenosi significative prossimali a carico dei vasi splancnici in assenza di altre patologie che possano causare i sintomi . 
se i dubbi persistono sulla natura della diagnosi , un mapping del flusso mediante rm quantitativa prima e dopo un pasto standard pu mostrare la mancanza di un normale aumento del flusso portale post - prandiale [ 1 , 2 ]  . la casistica consecutiva da noi selezionata sulla base del quadro clinico dominato da dolore addominale post - prandiale di tipo anginoso mostra primariamente la robustezza della tecnica e della tecnologia di tc multistrato nella valutazione dei vasi splancnici addominali . 
la popolazione relativamente pura e caratterizzata da stenosi di natura unicamente aterosclerotica ( in un paziente di giovane et il sospetto clinico era sostenuto anche unipercolesterolemia familiare ) ha mostrato una prevalenza di lesioni superiore al 60% su ciascuno dei due maggiori assi ( tronco celiaco ed arteria mesenterica superiore ) per un totale di circa la met dei vasi visualizzati affetti da stenosi o occlusioni . 
solo 21 lesioni stenosanti sono state giudicate significative ( > 50% di riduzione del lume vascolare ) , e solo in 16 casi si osservata la simultanea presenza di lesioni del tronco celiaco dellarteria mesenterica superiore . 
sei pazienti sono risultati completamente negativi ( incluso il paziente di giovane et con ipercolesterolemia familiare )  . radiol med ( 2008 ) 113 : 11351142 1141 ( including the young patient with familial hypercholesterolaemia )  . in our experience , the vessel lumen and stenoses were well depicted by msct , even though the comparison with conventional angiography was possible in a limited number of cases only . 
in this setting , the value of mra is limited by artefacts due to stent composition . we encountered a few limitations of msct angiography . the first limitation is the lack of dynamic visualisation , which can be compensated for only in part by the high spatial resolution . 
thus , the indication for msct angiography must be considered carefully , and the examination should be reserved for patients older than 40 years . one limitation that may have biased results is related to patient selection and the fact that the principal inclusion criterion was postprandial abdominal pa addition of a more stringent inclusion criterion such as weight loss might have increased the prevalence of patients with a diagnosis of abdominal angina and thus of patients who would have benefited from percutaneous treatment . nellesperienza qui descritta , il lume vascolare e le stenosi sono ben visualizzate mediante msct , anche se il confronto con lac stato possibile in un numero limitato di casi . 
come potenziale informazione aggiunta la presenza di placche aterosclerotiche pu essere valutata non solo come restringimento del lume vascolare ( come nel caso dellac ) , ma anche in termini di caratterizzazione tissutale misurata mediante valore di attenuazione . questo tipo di informazione non ha ancora un ruolo clinicamente definito . se confrontata con lac , la msct facilmente in grado di escludere cause estrinseche di ostruzione vascolare ( i.e. : incarceramento del vaso e / o compressione da effetto massa ) che per non sono state rilevate nella nostra casistica [ 915 ]  . 
dopo trattamento dellangina addominale mediante il posizionamento di stent , lmsct pu essere inoltre utilizzata per il follow - up non - invasivo e valutare la presenza di re - stenosi allinterno dello stent . 
in questa applicazione langio - rm soffre degli artefatti dovuti alla composizione metallica dello stent . abbiamo incontrato alcune limitazioni per langiografia msct : la prima legato alla mancanza di visualizzazione dinamica , che solo in parte compensata dallelevata risoluzione spaziale . 
queste considerazioni dovrebbero far pesare adeguatamente lindicazione ad angiografia msct , riservandola a pazienti di et superiore ai 40 anni . una limitazione che pu aver modificato in senso difensivo i risultati legata al fatto che il maggior criterio di inclusione per lo studio tc stato il dolore addominale postprandiale . 
laggiunta di un criterio di inclusione pi rigido come il calo ponderale potrebbe aver aumentato la prevalenza di pazienti con diagnosi di angina addominale e che avrebbero quindi beneficiato del trattamento percutaneo . conclusions conclusioni our preliminary experience indicates a new field of application of msct angiography in noninvasive evaluation of vascular diseases . 
in patients with suspected cmi , msct angiography may become the one - stop - shop modality to exclude vascular disease or identify , quantify and plan the la nostra esperienza preliminare mostra un nuovo campo di applicazione per langiografia msct nella valutazione noninvasiva delle malattie vascolari . 
in pazienti con sospetta icm langiografia msct pu diventare la modalit onestop - shop per escludere il coinvolgimento vascolare o per rilevare , quantificare e pianificare la migliore opzione 1142 radiol med ( 2008 ) 113 : 11351142 best treatment strategy . 
the aim of this study was to describe magnetic resonance imaging ( mri ) patterns in 21 patients with histologically proven invasive lobular cancer ( ilc ) of the breast . 
we retrospectively reviewed mr images of 21 out of 24 women with ilc of the breast . three women were excluded from the study because they underwent neoadjuvant chemotherapy after mri . 
all 24 patients underwent mammography , sonography and mri . mri was performed to evaluate disease extent and multifocality / multicentricity before modified radical mastectomy ( n = 5 ) or quadrantectomy ( n = 16 )  . 
rm stata effettuata per valutare lestensione locale di malattia e leventuale presenza di multifocalit o multicentricit , prima che le pazienti fossero sotttoposte a mastectomia radicale modificata ( n = 5 ) o quadrantectomia ( n = 16 )  . 
le caratteristiche morfologiche e dinamiche sono importanti nellinterpretazione della rm mammaria . ilc pu essere identificato dalla rm sulla base della presenza di lesioni solitarie o multiple , che corrispondono ai reperti anatomo - patologici . 
indagini rm negative sono rare , ma possibili in una bassa percentuale di ilc . parole chiave mammella risonanza magnetica carcinoma lobulare invasivo radiol med ( 2008 ) 113 : 11101125 introduction introduzione 1111 invasive lobular carcinoma ( ilc ) is a neoplasm originating in the lobular epithelium of the breast . 
first described in 1941 , its unique growth patterns were noted , including a linear arrangement of cells ( so - called indian - file pattern ) and a scattered growth pattern [ 3 ]  . 
a single - file infiltration of malignant cells has also been described [ 46 ] through the breast stroma with a relative paucity of desmoplastic response , haemorrhage , necrosis or calcifications [ 6 ]  . 
these histological patterns may account for the higher false - negative rate on mammography than observed for other types of invasive breast carcinoma [ 5 , 7 ] , so the reported sensitivity for detection is 57%92% [ 8 , 9 ]  . clinically , these tumours can appear as a fixed palpable mass that may exhibit skin retraction . 
on sonography , detection of ilc may be difficult : the range of sensitivity has been reported to be 68%87.7% , with the sensitivity for lesions smaller than 1 cm in the range of 25%85.7% [ 10 , 13 ]  . 
patients with ilc are reported to have a relatively high frequency of multifocal , multicentric or bilateral breast cancer ( 14%31% ) [ 4 , 8 , 14 , 15 ]  . 
for the correct choice between breast - conserving treatment and mastectomy , accurate definition of disease extent and possible multifocality / multicentricity of bilateral breast cancer are essential [ 16 ]  . previous studies have shown breast magnetic resonance imaging ( mri ) to be a useful adjunct to mammography and ultrasound ( us ) , with sensitivity reaching 100% in the detection of invasive breast cancer [ 4 , 16 , 17 ] and specificity varying from 37% to 86% [ 1823 ]  . 
 [ 1 ] reported that mri revealed more extensive tumour burden than did conventional imaging in seven of 18 patients with ilc . we retrospectively compared the findings of preoperative dynamic mri with those of mammography and us in 24 patients with pure ilc of the breast , using results from histopathological examination as the gold standard . 
la seconda , in ordine di frequenza , tra le neoplasie maligne della mammella e pu presentarsi in pressoch qualsiasi fascia di et della donna adulta [ 1 ]  . 
descritta per la prima volta nel 1941 , vennero da subito notati le singolari modalit di crescita , rappresentate da ununica filiera di cellule ( il cosiddetto pattern a fila indiana ) o , in alternativa , da una proliferazione in ordine sparso [ 3 ] ; inoltre , descritto anche un comportamento caratterizzato da una infiltrazione di cellule maligne in fila singola [ 46 ] attraverso il parenchima mammario con una relativa scarsit di risposta desmoplastica , di emorragia , necrosi o calcificazioni [ 6 ]  . 
questi aspetti istologici sono ritenuti responsabili della percentuale di indagini mammografiche falsamente negative pi elevata rispetto a quanto accade per altre neoplasie mammarie [ 5 , 7 ] , con una sensibilit di rilevazione riportata intorno al 57%92% [ 8 , 9 ]  . clinicamente , queste neoplasie possono apparire come masse palpabili fisse rispetto ai piani circostanti , a volte associate a retrazione dei piani cutanei . 
in ogni caso , ilc spesso si presenta come un processo infiltrativo diffuso in assenza di alcuna massa clinicamente palpabile [ 912 ]  . lidentificazione di ilc mediante ecografia pu essere difficoltosa : lintervallo di sensibilit riportato 68%87 , 7% , con una sensibilit per lesioni dimensionalmente inferiori al centimetro nellintervallo di 25%85 , 7% [ 10 , 13 ]  . 
i pazienti con ilc sono ritenuti soggetti a una maggior frequenza di multifocalit , multicentricit o bilateralit della localizzazione ( 14%31% ) [ 4 , 8 , 14 , 15 ]  . 
per una corretta scelta tra trattamento chirurgico conservativo e mastectomia sono essenziali unaccurata definizione dellestensione di malattia e la identificazione della possibile multifocalit / multicentricit o bilateralit del cancro mammario [ 16 ]  . studi precedenti hanno gi dimostrato lutilit della rm mammaria in ausilio di mammografia ed ecografia , con una sensibilit che raggiunge il 100% nellidentificazione del cancro mammario invasivo [ 4 , 16 , 17 ] ed una specificit che varia tra il 37% e l86% [ 1823 ] , ma solo pochi studi si sono focalizzati sulla utilit della rm mammaria in pazienti con ilc [ 17 , 24 ]  . 
 [ 4 ] hanno posto in correlazione lestensione del ilc definita allindagine istologica in 20 pazienti che precedentemente erano stati sottoposti a mr mammaria con apparecchiature ad altra risoluzione e utilizzo del mezzo di contrasto paramagnetico e mammografia . 
 [ 1 ] hanno riportato in una casistica 1112 radiol med ( 2008 ) 113 : 11101125 had been diagnosed with ilc between march 2005 and december 2006 and who had undergone preoperative breast mri at our hospital ( a medium - sized , nonacademic institution )  . 
all mammography and us image and reports were reviewed by two experienced breast radiologists . a senographe diamond ( instrumentarium imaging inc . , milwaukee , wi , usa ) was used to obtain all conventional mammographic images . 
breast composition was reported and defined as d1 ( almost entirely fat ) , d2 ( scattered fibroglandular densities ) , d3 ( heterogeneously dense ) or d4 ( extremely dense ) breast tissue . on us , lesions were evaluated and classified as a result of combined morphological characteristics : lesion margins , hyporeflectivity or hyperreflectivity , posterior acoustic shadowing and shape of the mass . 
 another set of unenhanced images was obtained with the following parameters : coronal t2 - weighted turbo spin echo ( tse ) ( tr / te , 3 , 800 / 140 ) , flip angle of 90 , and 512512 matrix . 
a late postcontrast set of images was obtained with the following parameters : coronal t1 - weighted , threedi 18 pazienti affetti da ilc una differente valutazione dimensionale di mr rispetto a mammografia , con una sottostima da parte di questultima metodica 7 casi su 18 . nel presente studio abbiamo retrospettivamente confrontato i reperti di mr mammarie , effettuate prima dellintervento chirurgico di asportazione di neoplasia , con mammografia ed ecografia in 24 pazienti con ilc puro della mammella , utilizzando i dati dellindagine anatomo - patologica come standard di riferimento . materiali e metodi abbiamo retrospettivamente esaminato le immagini di 24 donne con diagnosi di ilc effettuata tra marzo 2005 e dicembre 2006 e che sono state sottoposte a mr mammaria pre - operatoria nel nostro ospedale ( unazienda ospedaliera non universitaria di medie dimensioni )  . 
tutte le mammografie e le indagini ecografiche sono state riviste od eseguite da due radiologi esperti in patologia mammaria . un mammografo diamond ( instrumentarium imaging inc . , milwaukee , wisconsin , usa ) stato utilizzato per effettuare tutte le mammografie . 
le ecografie sono state effettuate con lutilizzo di una sonda a 5 , 57 , 5 mhz ( envisor , philips medical system , pc best , olanda )  . tutte le mammografie sono state interpretate utilizzando il lessico breast imaging reporting and data system ( birads ) alla luce dei reperti clinici [ 25 ]  . 
la densit radiologica del seno stata segnalata e definita come d1 ( pressoch completamente adiposo ) , d2 ( densit fibroghiandolare sparsa ) , d3 ( eterogeneamente denso ) o d4 ( estremamente denso )  . 
 allindagine ecografica , le lesioni sono state valutate e classificate in relazione alla combinazione delle caratteristiche morfologiche : margini della lesione , ipoo iperecogenicit , attenuazione acustica posteriore e forma della massa . 
 before the mri ( minimum 4 days , maximum 44 days ; mean 22.4 days ) , nine patients had undergone fine - needleaspiration cytology ( fnac ) followed by vacuum - assisted biopsy ( vab ) , six had undergone fnac followed by usguided tru - cut microbiopsy , one had undergone fnac on an axillary adenopathy ( negative mammography and us examination of the entire breast ) , three had undergone fnac only and two had undergone vab only without prior fnac . both radiologists reviewed the mri studies of all 21 women . 
morphological mri parameters described by the radiologists included lesion type ( mass , focal / regional enhancement , ductal or linear enhancement , distortion ) , mass margins ( well - circumscribed , ill - defined , obscured or spiculated ) and mass shape ( round , oval , lobular , irregular )  . 
for most sites , it is suggested that the immediate contrast - enhanced series be centred over roughly 2 min ( images obtained within 4 min ) and the delayed contrast - enhanced series be centred over 47 min ( images obtained within 8 min )  . pazienti sono state studiate con mr prima dellintervento chirurgico . 
stata utilizzata unapparecchiature rm 1 , 0 t intera achieva ( philips medical systems , pc best , olanda ) ; le pazienti sono state posizionate in decubito prono con una bobina bilaterale di superficie dedicata sense ( sensitivity encoding )  . 
le mammelle sono state studiate prima e sei volte dopo liniezione endovenosa ( velocit di iniezione 2 cc / s , seguita da 15 ml di soluzione salina ) di gadopentate dimeglumine 0 , 2 mmol / kg ( magnevist , schering , berlino , germania ) con una sequenza coronale t1 pesata , 3d fast field echo gradient - echo ( tr / te , 6 , 7 / 3 , 2 ) , con un flip angle di 25 , campo di vista di 320340 mm , spessore della fetta di 3 mm , senza intervallo tra le fette , matrice di 512512 . 
un altro gruppo di immagini stato ottenuto prima dellinfusione di mezzo di contrasto coi seguenti parametri : coronale t2 pesata turbo spin echo ( tr / te , 3800 / 140 ) , flip angle di 90 , matrice di 512512 . un ultimo gruppo di immagini tardive dopo infusione di mezzo di contrasto stato ottenuto coi seguenti parametri : coronale t1 pesata , 3d ffe gradient echo ( tr / tr , 19 , 0 / 9 , 6 ) , proset ( pro - selective ) water - selective , con un flip angle di 25 , campo di vista di 320340 mm , spessore di fetta di 3 mm , nessun intervallo tra gli strati , matrice di 512512 . 
le immagini pre - contrastografiche sono state poi sottratte dalla prima immagine pre - contrastografica . prima di effettuare lindagine mr ( minimo 4 giorni , massimo 44 giorni ; intervallo medio 22 , 4 giorni ) , 9 pazienti sono state sottoposte ad agoaspirato ( fnac ) ecoguidato seguito da microbiopsia ( vacuum assisted biopsy ) , 6 sono state sottoposte ad agoaspirato ( fnac ) ecoguidato seguito da microbiopsia ecoguidata con ago tru - cut , 1 stata sottoposta a fnac su adenopatia ascellare ( questa paziente era stata gi sottoposta ad indagine mammografia ed ecografia mammaria con esito negativo ) , 3 sono state sottoposte alla sola fnac , 2 sono state sottoposte alla sola vab senza precedente fnac . entrambi i radiologi hanno riesaminato le immagini mr delle 21 donne . 
i parametri morfologici mr descritti hanno incluso il tipo di lesione ( massa , impregnazione contrastografica focale o regionale , impregnazione contrastografica a distribuzione duttale o lineare , distorsione parenchimale ) , i margini della lesione ( netti , mal definiti , non valutabili o spiculati ) e la forma della lesione ( tondeggiante , ovalare , lobulare , irregolare )  . 
il tipo di impregnazione stato suddiviso tra omogenea , disomogenea o ad anello . 1114 radiol med ( 2008 ) 113 : 11101125 to classify areas on the mr examination as having or not having significant enhancement , pixel values at the unenhanced and first contrast - enhanced series are compared . 
if the pixel value on the delayed series decreases by more than 10% of its immediate contrast - enhanced value , that pixel is colour - coded red on the monitor , indicating washout of contrast material . 
finally , the radiologist may select a specific area of significant enhancement , and the programme will automatically generate a synopsis of the full volume of that lesion , including the percentage of the lesion that shows washout , plateau and persistent enhancement . 
lesions suspicious for malignancy were classified as unifocal , multifocal , single - quadrant or multiquadrant disease using the same definitions as mentioned above . morphological findings on mammography , us and mri and the detection of unifocal , multifocal , single - quadrant , multiquadrant or bilateral breast cancer by the three imaging modalities were compared , with results of the final histopathological examination as the gold standard . results thirteen cases were positive on clinical examination . 
questo software stato progettato per la rielaborazione automatica e analisi delle immagini che sono tradizionalmente effettuate manualmente dal tecnico sanitario di radiologia medica e dal medico radiologo . tutti i dati rielaborati sono stati salvati e presentati al medico radiologo per linterpretazione . 
in aggiunta , esso consente di visualizzare automaticamente le curve di impregnazione contrastografica e i dettagli di tutte le regioni con impregnazione contrastografica . per le indagini mr mammaria , il programma utilizza ai fini del calcolo 7 acquisizioni seriate : una serie t1 pesata senza mezzo di contrasto , una serie t1 pesata acquisita immediatamente dopo la somministrazione di mezzo di contrasto , e 5 serie post - contrastografiche successive pesate in t1 ( tempo di acquisizione per ogni sequenza ffe gradient echo 3d t1 57 , 4 secondi )  . 
per la maggior parte degli ospedali , consigliata lacquisizione della serie post - contrastografica centrata attorno ai 2 minuti ( per immagini ottenute nellarco di 4 minuti ) e lacquisizione della serie post - contrastografica tardiva centrata oltre i 47 minuti ( per immagini ottenute nellarco di 8 minuti )  . per classificare le aree nellindagine mr come aventi o meno unimpregnazione contrastografica significativa , vengono confrontati i valori di intensit di segnale dello stesso pixel nella sequenza prima e in quella immediatamente successiva linfusione di mezzo di contrasto . 
se il valore del pixel della serie tardiva decresce di oltre il 10% rispetto al valore della serie immediatamente successiva linfusione di mezzo di contrasto , quel pixel codificato in colore rosso sul monitor , indicando wash - out del mezzo di contrasto . 
in one case only , axillary adenopathy was found . eight women had no suspicious findings on physical examination . breast - tissue densities on mammography of the 21 cases were almost entirely fat ( d1 ) ( n = 10 ) , scattered fibroglandular densities ( d2 ) ( n = 6 ) , heterogeneously dense ( d3 ) ( n = 4 ) and extremely dense ( d4 ) ( n = 1 )  . 
in the subgroup of ten patients with almost entirely fatty breasts , three had no clinically relevant finding , two presented with a palpable mass , three presented with increased density without a palpable mass , one presented with increased density associated with nipple retraction and one presented with increased density associated with nipple retraction and increased skin thickness . 
 mammography obtained before biopsy failed to detect ilc in four ( 19% ) out of 21 cases : clinical and us findings of this subgroup are reported in table 2 . 
in 17 ( 81% ) of 21 cases , a mammographic finding was present ( table 3 )  . all 21 patients had sonographic examination , the results of which are given in table 4 . 
in seventeen of 21 cases , a mammographic abnormality corresponded to the sonoto mr indicante regioni di impregnazione contrastografica significativa , con informazioni sulla cinetica di impregnazione e sullestensione dellarea in cui questa si verifica . infine , il medico radiologo pu selezionare unarea di impregnazione significativa consentendo al programma di generare automaticamente una sinossi del volume totale della lesione , incluse le percentuali della lesione che mostrano impregnazione con cinetica wash - out , plateau e persistente . quando una lesione stata selezionata dal medico radiologo , questa informazione generata dal programma completamente automatica [ 26 ]  . tutte le pazienti sono state sottoposte ad intervento chirurgico dopo leffettuazione dellindagine mr . 
in one of these four cases , the first sonographic evaluation was negative , and only a second us examination , performed with knowledge of the mri results , was positive . 
these findings were confirmed at pathological examination . classificate come unifocali , multifocali , localizzate ad un singolo quadrante o a pi quadranti , utilizzando la terminologia gi descritta sopra . i reperti morfologici descritti su mammografia , ecografia e mr e la evidenza di malattia unifocale o multifocale , localizzata ad uno o pi quadranti , monoo bilaterale sono stati confrontati con i risultati dellindagine istologica utilizzata come gold standard . risultati tredici pazienti presentavano reperti palpatori sospetti allindagine clinica . 
otto donne non presentavano allesame clinico alcun reperto sospetto . le densit mammografiche riportate dei 21 casi sono state : pressoch interamente adiposa ( d1 ) ( n = 10 ) , densit fibroghiandolare sparsa ( d2 ) ( n = 6 ) , eterogeneamente densa ( d3 ) ( n = 4 ) , estremamente densa ( d4 ) ( n = 1 )  . 
nel sottogruppo di 10 pazienti con mammelle pressoch totalmente adipose , 3 non presentavano reperti clinici significativi , 2 erano portatrici di una massa palpabile , 3 presentavano radiol med ( 2008 ) 113 : 11101125 1117 table 5 correlation between positive ( 17 / 21 ) mammographic findings and breast densities mammographic finding breast density increased density increased density increased density 1 opacity 3 opacity 6 distortion 7 microcalcifications 8 opacity 9 opacity 10 distortion 11 distortion 12 increased density 13 opacity with microcalcifications 14 opacity 15 opacity 16 increased density 17 opacity 1 opacit 2 aumento della densit 3 opacit 4 aumento della densit 5 aumento della densit 6 distorsione 7 microcalcificazioni 8 opacit 9 opacit 10 distorsione 11 distorsione 12 aumento della densit 13 opacit associata a microcalcificazioni 14 opacit 15 opacit 16 aumento della densit 17 opacit tabella 5 correlazione tra reperti mammografici sospetti ( 17 / 21 ) e densit mammografiche reperto mammografico densit mammografica accuracy of computer - defined significant enhancement twenty lesions showed significant enhancement at the 100% threshold . 
all 20 enhancing lesions exhibited a significant degree of washout of contrast material . incremento di consistenza alla palpazione senza massa palpabile , una presentava un incremento di consistenza alla palpazione con retrazione del capezzolo , una presentava incremento di consistenza alla palpazione con retrazione del capezzolo e ispessimento cutaneo ; lecografia sempre risultata positiva in questo sottogruppo di donne ( tabella 1 )  . la mammografia effettuata prima di qualsiasi accertamento invasivo non stata in grado di identificare ilc in 4 ( 19% ) dei 21 casi : i reperti clinici ed ecografica di questo sottogruppo sono riportati in tabella 2 . 
in 17 ( 81% ) dei 21 casi , era invece presente un reperto mammografico sospetto ( tabella 3 )  . tutte le 21 pazienti sono state sottoposte ad ecografia del seno , i cui risultati sono riassunti nella tabella 4 . 
in 4 casi su 21 il reperto mammografico risultato negativo , a fronte di un reperto ecografico sospetto ; le densit mammografiche di queste 4 donne con mammografia negativa sono risultate essere , rispettivamente , d3 ( 2 casi ) e d1 ( due casi ) ; in uno di questi 4 ultimi casi la prima ecografia risultata negativa e solo una seconda ecografia effettuata alla luce del reperto mr risultata positiva . 
le dimensioni istopatologiche delle lesioni sono risultate essere da 0 , 4 a 3 , 3 cla dimensione media delle neoplasie risultata essere 1 , 56 cm . diciotto carcinomi della mammella sono stati descritti dalla rm come unifocali , 2 come multifocali , uno come multicentrico , rispetto a quanto emerso dalle indagini di diagnostica per immagini tradizionali : questi reperti sono stati confermati allindagine anatomo - patologica . accuratezza della definizione di impregnazione contrastografica significativa fornita dal software venti lesioni maligne hanno mostrato significativa impregnazione contrastografica utilizzando la soglia del 100% di incremento della intensit di segnale ( si ) nel primo minuto . una sola lesione non ha raggiunto la soglia del 100% nel primo minuto , con questo non rendendosi possibile la analisi automatica di tale lesione da parte del software . 
tutte queste 20 lesioni dotate di significativa impregnazione contrastografica nel primo minuto sono risultate dotate di significativa dismissione del mezzo di contrasto stesso . due radiologi hanno descritto , raggiungendo il consenso dopo discussione dei casi dubbi , la morfologia delle lesioni in mr . 
immagine rm coronale sottratta fast field echo ( tr / te , 19 / 10 ) che dimostra unarea di impregnazione contrastografica a margini irregolari ( pattern 1 )  . the two radiologists reached overall consensus in lesion description on breast mri . 
in eight women ( 40% ) , mri revealed additional findings , none of which were confirmed by us examination . five women underwent modified radical mastectomy and 16 underwent quadrantectomy . 
la rm ha rivelato in 8 donne ( 40% ) reperti aggiuntivi rispetto alle indagini tradizionali , nessuno dei quali stato confermato dalla verifica ecografica . cinque donne sono state sottoposte a mastectomia radicale modificata secondo madden , 16 donne sono state sottoposte a quadrantectomia . 
immagine rm coronale sottratta ffe ( tr / te , 19 / 10 ) che dimostra la presenza di multipli foci di impregnazione contrastografica connessi tra loro ( pattern 3 )  . clinica e per le metodiche diagnostiche convenzionali , risultando perci inferiore la sensibilit diagnostica rispetto a quanto accade per il carcinoma duttale invasivo ( idc )  . 
la maggior parte di questi tumori sono identificati come incrementi di densit senza margini ben definiti , incluse le distorsioni architetturali del parenchima , o come masse di elevata densit con margini irregolari . 
il tasso di mammografie interpretate come falsamente negative in donne portatrici di ilc , spesso caratterizzate dalla presenza di elevata densit radiografica delle mammelle , riportato oscillare tra il 16% ed il 43% [ 8 , 9 , 28 , 3134 ]  . 
noi abbiamo riscontrato , nelle 4 mammografie falsamente negative , 2 casi con d3 e 2 casi con d1 . i benefici dellindagine ecografica associata alla mammografia , nella diagnosi di ilc , sono variabili . 
alcuni autori hanno affermato che lecografia migliora significativa1120 radiol med ( 2008 ) 113 : 11101125 mente il tasso di identificazione del ilc in pazienti che si presentano con noduli palpabili e mammografia negativa [ 5 , 10 , 35 , 36 ]  . 
altri autori hanno osservato che lecografia riveste un ruolo limitato nelle pazienti affette da ilc per la variet di presentazione ecografica di questultimo e per le basse sensibilit e specificit proprie della metodica nella diagnosi dei piccoli tumori [ 16 , 37 ]  . 
nel presente studio lecografia ha fornito informazioni aggiuntive in tutti i 4 casi di ilc con mammografia negativa : ha messo in evidenza una massa mal definita in 2 casi , uno sbarramento acustico in 1 caso , una massa a contorni ben definiti in 1 caso . i limiti riscontrati sia nellecografia che nella mammografia hanno contribuito ad aumentare linteresse nei confronti della mr della mammella , la quale attualmente sta assumendo un ruolo sempre pi importante nella gestione della patologia mammaria [ 19 , 38 , 39 ]  . 
 [ 24 ] hanno descritto questo pattern in dodici di 26 , dieci di 18 , 19 di 20 , 4 di 13 e 8 di 20 casi , rispettivamente . 
il secondo pattern pi comune da noi riscontrato consistito in una massa a margini netti : non stato possibile trovare altre conferme al nostro riscontro , come recentemente descritto dal nostro gruppo [ 41 ]  . 
 [ 40 ] , i setti dotati di impregnazione contrastografica in assenza di una massa dominante menzionati da quayyum [ 17 ] , n limpregnazione regionale e distorsione architetturale descritte da weinstein et al . 
i tassi di identificazione di carcinoma multifocale o multicentrico rilevato alla mr ma occulto a ecografia e mammografia oscillano tra 16% e 37% [ 19 , 43 , 46 ]  . 
lindagine anatomo - patologica su pezzo operatorio eseguita dopo quadrantectomia ha dimostrato la presenza di un carcinoma lobulare invasivo del diametro massimo di 1 , 1 c table 7 patterns of t2 - weighted signal intensity on magnetic resonance imaging ( mri ) in 20 mr - detectable invasive lobular carcinomas t2 signal homogeneously hypointense homogeneously mildly hyperintense nonhomogeneously hyperintense nonhomogeneously hypointense tabella 7 patterns t2 in 20 ilc visibili in rm segnale nelle sequenze t2 - pesate omogeneamente ipointenso omogeneamente teneuemente iperintenso disomogeneamente iperintenso disomogeneamente ipointenso discussion ilc often presents with diagnostic difficulties on clinical examination and conventional imaging , resulting in lower sensitivities for ilc than for invasive ductal carcinomas ( idc )  . 
most tumours are identified either as an asymmetric density without definable margins , including architectural distortion , or as a high - density mass with spiculated radiol med ( 2008 ) 113 : 11101125 1121 margins . 
the rate of false - negative mammographic interpretation of ilc , often associated with increased breast parenchyma , has been reported to be in the range of 16%43% [ 8 , 9 , 28 , 3134 ]  . 
we found breast densities d3 ( two cases ) and d1 ( two cases ) in the four negative mammograms . results of breast us as an adjunct to mammography in diagnosing ilc are variable . 
some investigators found that us significantly improved the detection of ilc in patients presenting with palpable nodules and no mammographically detected masses [ 5 , 10 , 35 , 36 ]  . 
others found that us had a limited role in ilc because of the variety of us appearances and a very low sensitivity and specificity for the diagnosis of small cancers [ 16 , 37 ]  . 
in our study , us revealed additional information in all four cases with negative mammograms : us demonstrated an ill - defined mass in two cases , an area of shadowing in one case and a discrete mass in one case . the limitations of mammography and us have prompted considerable interest in mri of the breast , which is now playing an increasingly important role in the management of breast disease [ 19 , 38 , 39 ]  . 
immagine rm coronale t2 pesata turbo spin echo ( tr / te , 3800 / 140 ) che mostra unarea disomogeneamente ipointensa ( freccia )  . centricit e bilateralit del ilc la mr della mammella raccomandata per valutare la reale estensione di malattia prima dellopzione chirurgica [ 4 , 12 , 14 , 16 , 4347 ]  . 
 [ 1 ] , mr ha definito lestensione del tumore pi accuratamente di quanto non stato possibile fare con le metodiche convenzionali in 16 su 32 pazienti . harms [ 19 ] ha descritto come in una serie di 47 tumori mammari maligni tutti i cinque ilc sono stati ben 1122 radiol med ( 2008 ) 113 : 11101125 termine the extent of cancer within the breast more accurately than can be accomplished with conventional methods [ 4 , 16 , 19 , 4246 ]  . 
the reported rates of multifocal or multicentric cancer , detected on mri but occult on us and mammography , range from 16% to 37% [ 19 , 43 , 46 ]  . 
 due to the high rate of multicentricity and bilaterality of ilc , breast mri can be performed to assess the extent of disease before treatment planning [ 4 , 12 , 14 , 16 , 4347 ]  . 
for dynamic breast mri , t2 - weighted sequences have not been attributed a major role , and a t2 - weighted pulse sequence is , for the most part , considered optional . three reports [ 5153 ] have addressed the issue of t2weighted images and concluded that t2 - weighted sequences are not useful for differential diagnosis in breast mri . 
the results of another study [ 54 ] showed that in nonfat - suppressed t2 - weighted tse pulse sequences , fibroadenomas tend to demonstrate different signal intensities ( a significant difference between the prevalence of high si and low si lesions in breast cancers and fibroadenomas )  . 
therefore , in practice , if a well - circumscribed enhancing lesion is detected in breast mri , a high si in the corresponding t2weighted tse image could be used to support the diagnosis of a benign lesion . in contrast with this report , we found , among 20 enhancing ilc , the contemporary presence of hypoand hyperintense lesions on t2 - weighted tse images . 
because of the histological features in ilc , perifocal fibrosis , dense cellularity and / or a high nucleus - to - plasma ratio may dimostrati dalla mr e le loro dimensioni sono state valutate con accettabile accuratezza . 
in ogni caso , questi reperti falsi negativi sono stati riscontrati in pazienti che avevano subito una biopsia escissionale prima delleffettuazione della mr . noi abbiamo descritto una paziente con un ilc unifocale identificato come massa allecografia , ma occulto allesame clinico , alla mammografia ed alla mr ; questa paziente stata sottoposta a fnac ecoguidato con referto citologico c1 i.e. 
inadeguato [ 50 ] e successivamente a microbiopsia escissionale ecoguidata , con esito di carcinoma invasivo : il reperto anatomopatologico sul pezzo operatorio ha dimostrato la presenza di un ilc di 1 , 1 cm . la possibilit di differenziare mediante la mr dinamica mammaria le lesioni benigne dalla maligne basata quasi completamente sulla modalit di impregnazione contrastografica e sulla morfologia delle lesioni ; nel campo della mr dinamica mammaria le sequenze t2 pesate non hanno acquisito grande importanza ; una sequenza t2 pesata ritenuta dalla maggior parte degli autori opzionale , non funzionale alla diagnosi differenziale . 
tre pubblicazioni [ 5153 ] si sono occupate del tema delle immagini t2 pesate , concludendo che le sequenze pesate in t2 non forniscono informazioni utili alla diagnosi differenziale delle lesioni . 
i risultati di un altro studio [ 54 ] hanno mostrato come , nelle sequenze turbo spin echo t2 pesate senza soppressione del grasso , i fibroadenomi hanno la tendenza a manifestare differenti intensit di segnale ( esiste una significativa differenza tra la prevalenza di intensit di segnale elevate e basse fra carcinomi e fibroadenomi ) cosicch , in pratica , se viene rilevata dalla mr una lesione dotata di impregnazione contrastografica con bordi netti , il dato di un elevato segnale nella corrispondente sequenza t2 pesata potrebbe esser utilizzato a supporto della diagnosi di benignit della lesione stessa . in contrasto con questo dato , nel nostro studio abbiamo riscontrato , nel gruppo dei 20 ilc dotati di significativa impregnazione contrastografica , la presenza contemporanea di lesioni ipoed iperintense nelle sequenze t2 pesate . 
potrebbero essere le peculiarit istologiche del ilc , cio fibrosi perifocale , densa cellularit e / o elevato rapporto nucleo / citoplasma , ad essere responsabili del basso segnale nelle sequenze t2 pesate rispetto al parenchima mammario normale . 
dallaltra parte , le procedure di diagnostica invasiva ( fnac , microbiopsia con metodo tru - cut , microbiopsia vacuum - assisted ) possono essere responsabili di edema , emorragia locale e necrosi determinanti lincremento dellintensit di segnale nelle sequenze t2 pesate . radiol med ( 2008 ) 113 : 11101125 1123 contribute to the particularly low signal on t2 - weighted tse images with respect to the normal parenchyma . 
on the other hand , the diagnostic invasive procedures performed on many of these lesions before mri ( fnac , tru - cut microbiopsy , vab ) may be responsible for oedema , local haemorrhage and necrosis and subsequent increment of t2weighted si . 
a large prospective study is needed to confirm our findings and those published earlier . conclusions in conclusion , the most frequent feature of ilc seen on mri is a spiculated inhomogeneous mass , and the second feature in frequency is a mass with smooth margins . 
even if the diagnosis of ilc is difficult , use of all available techniques and the clinical examination itself may be helpful for detecting and characterising this neoplasmri may play an important role in evaluating multifocal or multiquadrant locations , but palpation , mammography and us remain of great value . 
the combination of approaches could lead to a correct diagnosis and the appropriate choice of therapeutic options . una limitazione del nostro studio consiste nel fatto che i radiologi che hanno rivisto le immagini mr erano al corrente della diagnosi istologica delle pazienti : essi erano al corrente della presenza di ilc in tutte le 21 donne , fatto che pu aver influenzato la loro interpretazione delle immagini mr . 
 conclusioni in conclusione , laspetto morfologico di ilc da noi pi frequentemente riscontrato in mr costituito da una massa disomogenea a bordi irregolari ; la seconda modalit di presentazione , in ordine di frequenza , costituita da una massa con bordi netti . 
la mr pu rivestire un ruolo importante nella valutazione della presenza di malattia a distribuzione multifocale o multicentrica , ma la palpazione , la mammografia e lecografia mantengono un valore fondamentale . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica , radioterapia , policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy 2istituto di oculistica , policlinico universitario tor vergata , roma , policlinico casilino / presidio sanitario usl - b , via casilina 1049 , 00100 roma , italy 3uoc di anestesia e rianimazione , policlinico casilino / presidio sanitario usl - b , via casilina 1049 , 00100 roma , italy correspondence to : m . 
complications included pain in three cases , eyelid inflammation in four cases and severe bleeding in one case . postprocedural mucocele was observed in five patients . mean time without symptoms was 31 weeks . 
there were 24 cases of stent obstruction : 15 were treated with highpressure 5% n - acetyl - cysteine and saline flush , achieving resolution in two cases ; in three cases , attempts to recanalise the obstruction with a guidewire failed . 
the occluded stents were removed in 22 patients : seven remained asymptomatic , 15 had recurrence of epiphora , nine received a new stent after dacryocystography and six underwent dacryocystorhinostomy . 
advantages of the procedure include the lack of anatomical alterations to the lacrimal ducts and a low short - term complication rate , whereas limitations include restricted duration of stent patency . 
abbiamo rilevato 24 ostruzioni : 15 trattate con lavaggi ad alta pressione di n - acetil - cisteina 5% con soluzione fisiologica ottenendo completa guarigione in 2 pazienti , stato effettuato un tentativo infruttuoso ( 3 casi ) di ricanalizzare lostruzione con una guida . 
limiti : perviet dello stent limitata . prospettive : individuare gli eventi fisiopatologici che portano ad ostruzione e correlarli con la morfologia dello stent . 1212 radiol med ( 2008 ) 113 : 12111218 keywords epiphora lacrimal gland nasolacrimal stenting parole chiave epifora ghiandola lacrimale stent nasolacrimale introduction introduzione epiphora refers to inadequate lacrimal - duct drainage and is seen in 3% of ophthalmology consultations [ 1 , 2 ] , with an incidence of 30%40% among the population older than 50 years of age [ 3 ]  . 
the main risk factors include white race ( especially mediterranean ) , advanced age , female gender ( 4 to 5 women for every one man ) and poor hygiene in low socioeconomic settings [ 3 ]  . 
 diagnosis is based on clinical assessment and diagnostic imaging with dacryocystography , computed tomography ( ct ) - dacryocystography and magnetic resonance ( mr ) dacryocystography , which provide information on the nature and site of the obstruction [ 3 ]  . 
treatment options include dacryocystorhinostomy ( dcr ) and stent placement . the first is a surgical procedure performed under general anaesthesia , with an 89%95% rate of technical success [ 48 ]  . 
the purpose of this study was to evaluate the patency of the song polyurethane nasolacrimal stent ( song nasolacrimal duct stent set , cook , qld , australia ) implanted in patients with lacrimal - duct stenoses obstructions and to assess its long - term effectiveness over a 5 - year follow - up . lepifora corrisponde allinsufficiente drenaggio da parte delle vie lacrimali e viene riscontrata nel 3% delle visite oculistiche [ 1 , 2 ]  . 
i pi importanti fattori di rischio correlati con questa patologia : frequente in persone di razza caucasica ( soprattutto mediterranei ) , aumenta con let , viene colpito soprattutto il sesso femminile ( 45 donne per uomo ) , lincidenza aumentata per minore igiene negli ambienti socioeconomici meno sviluppati [ 3 ]  . la diagnosi si effettua soprattutto con la clinica e la diagnostica per immagini con la dacriocistografia , la dacriotc e la dacrio - rm fornisce informazioni sulla natura e la localizzazione dellostruzione [ 3 ]  . 
la prima una tecnica chirurgica condotta in anestesia generale con successo tecnico 89%95% [ 48 ] ; le complicanze maggiormente riscontrate sono il sanguinamento , che richiede un buon controllo pressorio per moderarne la entit . 
la chiusura del tramite fistoloso creato [ 9 ]  . laltra tecnica stata sviluppata da diversi anni e consiste nellapplicazione di uno stent nella via naturale per via interventistica non chirurgica . 
il nostro obiettivo di valutare la perviet dello stent nasolacrimale in poliuretano disegnato da song impiantato in pazienti con steno - ostruzioni delle vie lacrimali e constatarne la perviet a lungo termine con follow up fino a 5 anni . materials and methods materiali e metodi from 2003 to march 2007 , we implanted 76 polyurethane song nasolacrimal stents in 73 consecutive patients ( 16 men and 57 women ; mean age 56 years ; age range 1981 ) with recurrent epiphora and / or dacryocystitis due to nasolacrimal duct obstruction . 
in our department , the procedure is tra il 2003 e marzo 2007 abbiamo impiantato 76 protesi naso - lacrimali in poliuretano ideate da song ( song nasolacrimal duct stent set , cook , queensland , australia ) in 73 pazienti consecutivi con epifora e / o dacriocistiti ricorrenti , dovute ad ostruzione del dotto naso - lacrimale . 
local anaesthesia was induced with novesin drops to reduce ocular reflex , followed by lidocaine hydrochloride ( 200 mg / 10 ml ) in medial orbital ( infratrochlear ) location and close to the infraand supraor1213 casi ( 4 , 1% )  . 
nel nostro dipartimento diamo indicazione per la procedura nei pazienti con grado > 3 o nei casi di dacriocistiti . la diagnostica pre - procedurale viene effettuata mediante esame dacriocistografico integrato con esame dacrio - tc per ottenere informazioni sul livello dellostruzione e lanatomia del paziente . 
limpianto dello stent stato realizzato dal servizio di diagnostica per immagini imaging molecolare radiologia interventistica e radioterapia del policlinico universitario tor vergata roma e dalla uoc di radiologia del policlinico casilino asl roma b in regime day hospital . 
si procede con anestesia locale con novesina gocce per ridurre i riflessi oculari , quindi con anestesia con lidocaina cloridrato ( 200 mg / 10 ml ) in localizzazione orbitaria mediale ( infratrocleare ) ed adiacente ai forami infra e sovraorbitari . 
stata sempre associata anche lapplicazione nella fossa nasale inferiore di garza imbevuta in soluzione contenente quota di vasocostrittore unitamente allanestetico locale ( 30 cc di soluzione fisiologica con 10 cc di lidocaina cloridrato 2% , 0 , 5 mg adrenalina ) ; la finalit di questa procedura di avere anestesia a livello della fossa nasale inferiore e vasocostrizione della mucosa nasale per ridurre il sanguinamento a carico della mucosa dei turbinati durante la fase nasale della procedura . 
si introduce una guida metallica ( calibro 0 , 018 ) con oliva allestremit distale attraverso il puntino lacrimale , generalmente il superiore , precedentemente dilatato , avanzandola fino al sacco lacrimale . 
1a , b dacriocistografia in paziente donna di 75 anni che evidenzia ostruzione infundibolare del canale naso lacrimale di sinistra . 1214 radiol med ( 2008 ) 113 : 12111218 fig . 
the nasal cavity was packed with gauze soaked in a solution of 30 cc of saline with 10 cc of 2% lidocaine hydrochloride and 0.5 mg adrenaline to achieve anaesthesia and vasoconstriction of the nasal mucosa and reduce bleeding of the turbinate during the nasal phase of the procedure . dacryocystography was then performed to locate the anatomical landmarks and confirm the diagnosis of lacrimal - duct obstruction . 
a 6 - f introducer sheath with a dilator was passed over the guidewire and advanced to the lacrimal sac , where the dilator was removed while the sheath was left in place . 
after reaching the lacrimal sac , the stent was inserted into the sheath and advanced up to the desired position ; the introducer was then pulled back and the stent left in situ . 
con dilatatore ed una volta raggiunto il sacco lacrimale si rimuove la camicia dellintroduttore ( dilatatore ) mantenendo in situ lintroduttore , dopo aver raggiunto il sacco lacrimale , si inserisce nellintroduttore sempre per via trans nasale la protesi che viene spinta fino alla posizione desiderata per poi rimuovere lintroduttore con tecnica pull back e lasciate lo stent in situ . 
i successivi controlli sono affidati alla divisione di oftalmologia del nostro policlinico universitario . risultati il tempo medio procedurale di 16 minuti ( massimo 44 minuti , minimo 8 minuti )  . 
in 2 dei tre casi in cui non risultata possibile le ricanalizzazione la guida ha superato lostruzione ma il recupero con lapposito gancio non stato possibile ; nel caso rimanente non risultato possibile superare radiol med ( 2008 ) 113 : 12111218 1215 fig . 
in two cases , recanalisation failed because we were unable to remove the guidewire with the hook despite having crossed the obstruction ; in one case , the obstruction could not be crossed . two patients had posttraumatic epiphora , and one had a lostruzione . 
le principali complicanze riscontrate sono : dolore in 3 ( 3 , 96% ) procedure , infiammazione palpebrale in 4 ( 5 , 2% ) procedure , emorragia in cui stato necessaria la consulenza otorinolaringoiatria 1 ( 1 , 3% ) caso , mucocele post - procedura riscontrato in 5 ( 6 , 5% ) pazienti . 
in un paziente si registrata stazionariet del quadro clinico pur con il rilevo di un inappropriato posizionamento dello stent ; dopo 3 mesi si deciso di sostituirlo con risultati soddisfacenti . 
one patient , with evidence of stent malposition , showed no clinical benefit , and the stent was replaced after 3 months with satisfactory results . the mean follow - up period was 1 year . 
in 15 cases of obstruction , we attempted to recanalise the duct with highpressure flushing with saline solution and 5% nacetyl - cysteine through the superior punctum ; this succeeded in restoring stent patency for the entire duration of the follow - up period in two patients . 
these cases are eligible for a possible reimplantation of a polyurethane stent : of the 15 patients with epiphora after stent removal , nine opted for stent reimplantation and six for dcr . 
follow - up of these nine patients demonstrated early recurrence in five ; this could be due to an inflammatory reaction caused by the close proximity of the head of the stent to the lacrimal sac in patients with a small sac , with the production of large amounts of granulation tissue . discussion the use of song stents has several advantages compared with traditional surgical techniques : local anaesthesia , easy placement , safety , no facial scar , less bleeding and better tolerance by patients [ 11 ]  . 
technical success rates ( 96% ) are similar to those reported for dcr ( 89%93% ) [ 12 ] and are greater than those of metallic - stent implantation ( 25% ) [ 13 ] or balloon dilation ( 45% ) [ 10 ]  . 
in 15 casi con ostruzione abbiamo tentato di ricanalizzare lo stent mediante lavaggi forzati con soluzione fisiologica e n - acetilcisteina 5% tramite il puntino lacrimale superiore ottenendo perviet nellintero follow - up in 2 pazienti ; abbiamo tentato la ricanalizzazione mediante guida posizionata dal radiologo interventista in 3 casi con mancata disostruzione . negli altri 22 pazienti abbiamo optato per la rimozione della protesi ostruita . 
abbiamo trovato materiale mucoso in 8 protesi e tessuto di granulazione nelle altre 14 . in 18 dei 22 pazienti in cui abbiamo rimosso lo stent ostruito , la via lacrimale tornata pervia . 
questi pazienti sono candidati per un eventuale riposizionamento dello stent in poliuretano : dei 15 pazienti con epifora dopo la rimozione dello stent lacrimale , 9 di loro hanno optato per il riposizionamento dello stent e gli altri 6 per la dcr . 
il follow - up di questi 9 pazienti documentava recidiva a breve termine della sintomatologia in 5 ; tale fenomeno potrebbe essere attribuibile ad una reazione infiammatoria dovuta ad uno stretto rapporto tra la parte prossimale dello stent con il sacco lacrimale in pazienti con sacco lacrimale di esigue dimensioni pertanto si sviluppa unimportante quota di tessuto di granulazione . 
 discussione il posizionamento dello stent di song presenta notevoli vantaggi rispetto alle tecniche chirurgiche tradizionali : anestesia locale , facilit di esecuzione , elevata sicurezza della procedura , assenza di ferite chirurgiche facciali , ridotti sanguinamenti , maggiore tollerabilit da parte dei pazienti [ 11 ]  . 
il successo tecnico ottenuto ( 96% ) comparabile con quello riportato per la dacriocistorinostomia ( 89%93% ) [ 12 ] e supera i risultati ottenuti con il posizionamento dello stent metallico ( 25% ) [ 13 ] o la dilatazione con palloncino ( 45% ) [ 10 ]  . 
 nel nostro studio la ricorrenza dei sintomi si verificata in 24 casi ( 31 , 6% ) , di questi dopo lavaggi con soluzione fisiologica e n - acetil - cisteina 5% tramite il puntino lacrimale superiore ottenendo ricanalizzazione in 2 ; negli altri abbiamo optato per la rimozione dello stent , tale procedura non preclude la possibilit di riposizionare un secondo stent in caso di ricorrenza dellepifora che si verificata in 15 pazienti ( 4 dal momento in cui stato rimosso lo stent e 11 nel follow up a 39 settimane )  . 
prima di riposizionare un nuovo stent dobbiamo ripetere tutte le indagini di diagnoradiol med ( 2008 ) 113 : 12111218 1217 tum , whereas the other patients had the stents removed . stent removal does not preclude placement of a new stent should epiphora recur , as it did in 15 of our patients ( four at the time of stent removal and 11 at the 39 - week follow - up )  . before stent reimplantation , however , all imaging exams must be repeated to evaluate the exact grade and level of stenosis obstruction . unlike surgery , which produces irreversible anatomical alterations , this minimally invasive technique is less traumatic , requires a shorter hospital stay with similar results and above all allows nonfunctional stents to be removed without altering the patients normal anatomy . there is evidence to indicate that the position of the head of the stent may play an important role in stent patency and function : in particular , stent patency seems to be longer when the head of the stent is not in close contact with the upper portion of the lacrimal sac ( confluence of the canaliculi , upper fornix )  . 
this view is supported by reports [ 14 ] that stents modified in their extreme end ( mushroom tip ) had 79% patency rates at 24 months [ 15 ]  . therefore minimising interaction between the head of the stent and the lacrimal sac is thought to better preserve normal lacrimal dynamics and consequently ensure longer stent survival . 
this may be explained by tear - flow dynamics and the possible blockage of the pump system produced by the musculus orbicularis by the head of a stent that is placed too cranially . 
 in this case , the stent was found to be positioned very cranially and in close contact with the upper fornix of the lacrimal sac . conclusions advantages of this procedure are that it does not alter the anatomy of the lacrimal outflow pathway , it can be repeated and has a low rate of intra - , peri - , and postprocedural complications . 
it is necessary that the causes of stent obstruction ( fibrous tissue around the stent ) be accurately investigated , including the role of tear - fluid composition and superimposed inflammatory processes . the lacrimal stents in use today may not be ideal . 
the position of the stent head within the lacrimal sac and , in particular , its contact with the common duct and the upper fornix , need to be evaluated in relation to symptoms and the duration of stent patency . stica per immagini necessarie per valutare la precisa entit della steno - ostruzione ed il livello . al contrario della tecnica chirurgica che genera modificazioni anatomiche non ripristinabili in caso di fallimento , la tecnica mini - invasiva si pu avvalere del vantaggio della minor traumaticit , minore degenza con risultati comparabili e soprattutto la possibilit di potere rimuovere lo stent posizionato non funzionante rispettando la normale anatomia del paziente . alcuni elementi indicano che la posizione dellestremo oculare dello stent pu giocare un ruolo importante nella durata della perviet e nella funzionalit dello stent : in particolare meno stretto il rapporto con lestremit craniale del sacco lacrimale ( confluente dei canalini , recesso superiore ) e maggiore sembra essere il periodo di perviet dello stent . 
questa teoria viene supportata da studi [ 15 ] che hanno segnalato che stent modificati nella estremit oculare garantiscono una durata della perviet di 79% a 24 mesi [ 14 ]  . 
pertanto possiamo ritenere che quanto meno lo stent interagisce con il sacco tanto maggiore la conservazione della normale dinamica lacrimale e di conseguenza la durata dello stent nella sua funzione . la motivazione pu essere ricercata nella dinamica stessa del flusso lacrimale , in particolare nelle possibili interferenze sul sistema di pompa generato dai muscoli orbicolari che lo stent posizionato troppo cranialmente pu determinare . 
in questa caso lo stent risultava posizionato in situazione alquanto craniale a stretto ridosso del recesso superiore . conclusioni vantaggi : procedura che lascia inalterata la anatomia di deflusso delle vie lacrimali , ripetibile , con complicanze intra - peri - postprocedurali basse . 
limiti : durata della perviet dello stent limitata , con ampie variazioni tra caso e caso ( casi che durano da oltre cinque anni ; casi che si ostruiscono dopo pochi mesi )  . 
prospettive : vanno individuati con maggiore precisione i motivi per i quali si verifica la ostruzione ( tessuto fibroso intorno allo stent ) che possono in varie maniere essere determinate dalla qualit del fluido lacrimale e dalla sovrapposizione di processi flogistici . lo stent lacrimale attualmente in uso potrebbe non essere quello ideale ; esistono valide indicazioni per sperimentare limpiego di stent di nuova concezione che rispondano ai requisiti indicati . 
biopsies were obtained in patients with no known primary cancer ( 75 )  . kyphoplasty was performed in 39 patients with magerl type a1 and a3 fractures within 3 months from the trauma . a bipedicular approach was used in all cases . 
in patients treated with vertebroplasty , success rates at 2472 h were 90% for osteoporotic fractures , 100% for vertebral haemangiomas and 77% for metastatic fractures . extravertebral vascular or discal leakage of cement occurred in 39 patients , but only two of them reported radicular pain due to epidural involvement . 
la biopsia stata eseguita nei casi di lesioni dubbie ( 75 pazienti ) , senza lesione primitiva nota . trentanove pazienti , affetti da frattura vertebrale traumatica tipo a1 e a3 secondo magerl , sono stati sottoposti a kp entro 3 mesi dal trauma . 
nei pazienti sottoposti a vp , nel giro di 2472 h , abbiamo riscontrato un successo della procedura nel 90% dei crolli porotici , nel 100% di quelli angiomatosici e nel 77% di quelli neoplastici . 
entrambe le metodiche sono valide nel management delle sindromi antalgiche vertebrali . 1172 radiol med ( 2008 ) 113 : 11711184 kyphoplasty is suggested in acute traumatic fractures of type a1 and a3 according to magerl , as it allows recovery of vertebral stability and a better distribution of the cement . keywords vertebral fractures vertebroplasty kyphoplasty secondo la nostra esperienza e i nostri risultati , riteniamo che , a fronte delle differenze tecniche ed economiche delle due metodiche , il ricorso alla vp nei crolli porotici , angiomatosici aggressivi e neoplastici , pi indicato per la rapida esecuzione e minore invasivit . 
la kp , invece , preferibile nelle fratture vertebrali recenti tipo magerl a1 e a3 , per la caratteristica di ripristino della statica vertebrale e per una migliore distribuzione del cemento nel metamero fratturato . parole chiave fratture vertebrali vertebroplastica cifoplastica introduction introduzione vertebroplasty and kyphoplasty , new techniques for treating vertebral - body fractures , have generated much interest in recent years . 
both techniques are based on the assumption that the percutaneous injection of acrylic material into the vertebral body is capable of stabilising the fractured vertebra and relieving vertebral pain . vertebroplasty was first described by galibert and deramond and coworkers [ 1 ] , a french neurosurgeon and a french radiologist who published a technical note on the treatment of vertebral haemangiomas in the journal neurochirurgie in 1987 . 
although the french investigators deserve all credit for introducing the technique , it was the rigourous methodological approach later adopted by the north american authors that led to its success and popularity [ 36 ]  . 
 in the usa , the estimated prevalence of osteoporotic vertebral compression fractures is approximately 700 , 000 cases annually , although the figure is probably underestimated due to underreporting of the condition in the elderly [ 7 , 8 ]  . the prevalence in europe is 438 , 750 per annum , equal to 117 cases in 100 , 000 [ 9 ]  . 
among women older than 50 years , the prevalence is 26% , and it increases to approximately 40% in women older than 80 years [ 9 , 10 ]  . kyphoplasty was developed as a modification of vertebroplasty . 
first performed in california in 1998 [ 11 ] , it consists in delivering polymethylmethacrylate ( pmma ) or other types of cement into the fractured vertebral body under fluoroscopic guidance after the cancellous bone has been compacted with dedicated balloon tamps . 
the goal is to combine the analgesic and vertebral consolidation effect of nel corso degli ultimi anni hanno suscitato notevole interesse due nuove modalit di trattamento per le fratture da crolli vertebrali : la vertebroplastica ( vp ) e la cifoplastica ( kp )  . 
il presupposto fondamentale di entrambe le metodiche che con tecnica percutanea miniinvasiva , attraverso il peduncolo , si introduce nel soma vertebrale materiale acrilico rendendo cos stabile la vertebra fratturata con conseguente effetto positivo sul sintomo dolore . la vertebroplastica fu descritta per la prima volta nel 1987 da galibert e deramond [ 1 ] , rispettivamente neurochirurgo e radiologo francese che pubblicarono sulla rivista di neurochirurgie delle note tecniche per il trattamento degli emangiomi vertebrali . 
agli autori francesi va certamente il merito di aver iniziato questo tipo di trattamento mentre agli autori statunitensi , che lapplicarono in seguito , bisogna riconoscere un approccio metodologico rigoroso nellidentificazione dei meccanismi alla base del successo del trattamento nonch della diffusione della tecnica [ 36 ]  . 
 negli usa , lincidenza annuale di fratture vertebrali da osteoporosi stimata essere intorno ai 700000 casi , sebbene questo numero sia probabilmente sottostimato rispetto alla reale incidenza per unattenzione limitata a questo tipo di patologia nella popolazione pi anziana [ 7 , 8 ]  . 
nelle donne di et superiore ai 50 anni lincidenza di crolli porotici stata stimata essere del 26% , radiol med ( 2008 ) 113 : 11711184 1173 vertebroplasty with restoration of the physiological height of the collapsed vertebral body , with resulting normal vertebral statics and biomechanics . 
the aim of this study was to compare vertebroplasty and kyphoplasty by illustrating the two techniques , analysing their results , and discussing their indications in relation to the type of fracture . materials and methods patients between april 2001 and december 2006 , we performed vertebroplasty on 805 vertebrae in 485 patients ( 282 women , 205 men ; mean age 59 years ) affected by osteoporosis ( 310 ) , vertebral metastasis ( 160 ) and vertebral haemangioma ( 15 )  . 
thirty - nine patients ( 32 men and seven women ; mean age 42 years ) were treated with kyphoplasty for type a1 ( 30 ) and a3 ( 9 ) traumatic vertebral fractures according to magerls classification [ 20 ]  . all vertebroplasty procedures were performed with the patient in the prone position . 
biopsy was performed in 75 patients with no known primary cancer and equivocal computed tomography ( ct ) or magnetic resonance imaging ( mri ) findings . procedures were performed under local anaesthesia combined with neuroleptanalgesia ; no patient received general anaesthesia . all kyphoplasty procedures were performed with the patient in the prone position . 
thirty - one patients received general anaesthesia , whereas only eight received local neuroleptanalgesia based on the type of traumatic fracture . patient selection : inclusion criteria patients were considered eligible for vertebroplasty or kyphoplasty if they had intense , nonradicular , midline vertebral pain , strongly exacerbated by palpation of the spinous process of the affected vertebra and refractory to conventional medical treatment ( bracing and bed rest )  . 
patients were eligible for kyphoplasty if they had sustained a traumatic vertebral fracture ( accidental / domestic ) of type a1 and a3 according to magerl no more than 3 months before the procedure to allow correct expansion of the kyphotic vertebra and better and safer cement distribution . con tendenza ad aumento con let , raggiungendo circa il 40% in donne con et superiore agli 80 anni [ 9 , 10 ]  . sulla base del successo ottenuto dalla vp , si sviluppata poi la kp . 
la cifoplastica , effettuata per la prima volta nel 1998 in california da reiley [ 11 ] , consiste nella introduzione di polimetilmetacrilato ( pmma ) , o altri tipi di cemento , allinterno dei corpi vertebrali fratturati sotto guida fluoroscopica , previa distensione della spongiosa mediante cateteri a palloncino dedicati . 
in tale modo si cerca di unire alleffetto antalgico e di consolidamento del soma fratturato proprio della vp , il ripristino della fisiologica altezza del soma collassato , ristabilendo la normale statica e biomeccanica vertebrale . 
 negli ultimi 15 anni il successo ottenuto con tali tecniche ha permesso lampliamento delle indicazioni alle sindromi vertebrali dolorose , non rispondenti alla terapia conservativa [ 6 , 1219 ]  . 
scopo di questo lavoro quello di mettere a confronto le due metodiche , illustrando la tecnica , analizzandone i risultati e confrontando le indicazioni della loro esecuzione sulla base del tipo di frattura . materiali e metodi pazienti dallaprile 2001 al dicembre 2006 , 485 pazienti ( 282 donne , 205 uomini ; et media 59 anni ) sono stati sottoposti a vp per un totale di 805 metameri , cos distribuiti : 310 trattati per osteoporosi ; 160 trattati per metastasi vertebrali ; 15 trattati per angioma . 
trentanove pazienti ( 32 uomini e 7 donne ; et media 42 anni ) sono stati sottoposti a kp , in quanto affetti da frattura vertebrale traumatica di tipo a1 e a3 secondo la classificazione di magerl [ 20 ] , cosi distribuite : 30 fratture tipo a1 secondo magerl ; 9 fratture tipo a3 secondo magerl . nei pazienti sottoposti a vp , stato seguito un approccio monopeduncolare in 365 pazienti e bipeduncolare in 120 pazienti , a paziente prono . 
abbiamo preferito un approccio trans - peduncolare nel trattamento di vertebre lombari e dorsali basse , mentre nel trattamento di crolli dorsali alti abbiamo preferito un approccio pi laterale , di tipo intercosto - trasversario . 
tutte le procedure di vp sono state eseguite in anestesia locale utilizzando la neuroleptoanalgesia ; in nessun caso stato necessario praticare anestesia generale . tutte le procedure di kp sono state eseguite con approccio trans - peduncolare bilaterale a paziente prono . 
in 31 casi abbiamo preferito lanestesia generale , mentre in soli 8 casi abbiamo optato per la neuroleptoanalgesia locale sulla base del tipo di frattura traumatica . 1174 radiol med ( 2008 ) 113 : 11711184 patient selection : absolute exclusion criteria selezione dei pazienti : criteri di inclusione absolute exclusion criteria were : ( 1 ) asymptomatic vertebral fractures ; ( 2 ) diffuse , nonfocal pain without mri evidence of altered trabecular - bone signal ; ( 3 ) systemic or local infections ; ( 4 ) uncorrectable coagulation disorders ; ( 5 ) osteoblastic tumours . patient selection : relative exclusion criteria relative exclusion criteria were : ( 1 ) radicular or medullary involvement ; ( 2 ) complete loss of vertebral height ( vertebra plana ) ; ( 3 ) interruption of the posterior vertebral margin or pedicles . diagnostic imaging diagnostic workup was aimed at selecting the most appropriate treatment . 
this was followed by mri to define the nature of the vertebral fracture and establish the vertebral level on the basis of increased t2 - weighted and short tau inversion recovery ( stir ) signals corresponding to bone marrow oedema . 
once the type and nature of the vertebral fracture had been established , we opted for vertebroplasty , the less invasive and expensive technique , in all patients affected by vertebral fractures due to osteoporosis , metastasis and haemangiomas , and wee reserved kyphoplasty for those affected by type a1 and a3 traumatic vertebral fractures according to magerl . 
fluoroscopic guidance was used in patients with osteoporosis ( 310 ) and vertebral haemangioma ( 15 ) , whereas in those with metastatic lesions ( 160 ) , we preferred ct associated with a portable c - arm , as it allowed for an easier approach and more precise placement of the needle in the osteolytic area . 
all kyphoplasty procedures were performed with fluoroscopic guidance . patients were evaluated on the basis of a visual analogue scale ( vas ) and the oswestry disability index ( odi ) before the procedure and at 1 , 3 and 6 months . vertebroplasty : technique after obtaining a radiographic image in which the upper and sono stati considerati eleggibili di un trattamento di vp o kp i pazienti che presentavano un dolore vertebrale intenso , non radicolare , localizzato lungo la linea mediana , fortemente evocato alla manovra di digito - pressione sullapofisi spinosa del soma crollato e resistente alle comuni terapie mediche convenzionali ( ortesi a riposo )  . 
abbiamo considerato eleggibili di kp i pazienti con frattura somatica traumatica ( accidentale / domestica ) tipo a1 e a3 secondo magerl , entro 3 mesi dal trauma , al fine di determinare una corretta espansione del soma cifotizzato e per una migliore e pi sicura distribuzione del cemento . selezione dei pazienti : criteri di esclusione assoluta sono stati esclusi pazienti : ( 1 ) portatori di fratture vertebrali asintomatiche ; ( 2 ) con dolore diffuso , non focale , con esame rm negativo per alterazione di segnale della spongiosa ; ( 3 ) affetti da uninfezione sistemica o locale ; ( 4 ) affetti da disturbi della coagulazione non correggibili ; ( 5 ) affetti da lesioni neoplastiche di tipo osteoblastico . selezione dei pazienti : criteri di esclusione relativa ( 1 ) pazienti con una sofferenza radicolare o midollare ; ( 2 ) pazienti con il collasso completo del metamero ( vertebra plana ) ; ( 3 ) pazienti con interruzione dellintegrit del muro posteriore o dei peduncoli vertebrali . diagnostica per immagini liter diagnostico finalizzato alla scelta del tipo di trattamento da eseguire ha previsto come esame di primo livello quello di radiologia tradizionale per lidentificazione dellalterazione strutturale del soma vertebrale . 
seguito poi un esame di rm per una corretta diagnosi di natura del crollo e per stabilire il soma sofferente , denunciato dalliperintensit di segnale nelle sequenze pesate in t2 e stir corrispondente alledema intra - spongioso . 
stabilito quindi il tipo e la natura della frattura somatica , abbiamo optato per il trattamento di vp , meno aggressivo e costoso , per tutti i pazienti affetti da crolli porotici , metastatici e angiomatosici ; riservando il trattamento di kp unicamente ai pazienti affetti da fratture traumatiche di tipo a1 e a3 secondo magerl . la metodica di vp stata eseguita a diversi livelli sino ad un massimo di sei metameri in 8 pazienti ed stata condotta sotto guida fluoroscopia nei pazienti affetti da osteoporosi ( 310 pazienti ) e da angioma vertebrale ( 15 pazienti ) ; radiol med ( 2008 ) 113 : 11711184 1175 lower endplates were perfectly aligned and the spinous processes were projected in midline , the pedicle was approached with an 11or 13 - gauge bevelled needle between 10 and 15 cm long , with side wings to facilitate rotation . once inside the pedicle , the needle was advanced to the anterior third of the vertebra and the cement injected into the body . 
the amount of cement used ranged from 2 to 4 ml for thoracic vertebrae treated with unipedicular approach , to 5 to 6 ml for dorsolumbar vertebrae and 12 ml for lumbar vertebrae . kyphoplasty : technique unlike vertebroplasty , kyphoplasty is always performed with a bilateral transpedicular approach and the patient in prone position . 
after a 1 - cm skin incision extending to the muscle fascia was made to facilitate insertion of the trocar needle , the 11 - gauge needle was advanced at an oblique angle into the pedicle under fluoroscopic guidance . 
a kirschner wire was then introduced coaxially to the needle to serve as a guide for the working cannula , which was driven up to 3 mm beyond the posterior wall of the vertebral body . 
a small hand - mounted drill was used to create a bone channel , with the distal end a few millimetres from the anterior cortical margin to allow insertion of the balloon into the vertebral body . 
the same procedure was carried out through the contralateral pedicle . once inside the vertebra , the balloon catheters were simultaneously inflated with a mixture of contrast material , under continuous fluoroscopic and manometric monitoring . they were then deflated and removed , and the same working cannula was used as a route for pmma delivery into the newly created cavity . 
often , the cement volume was approximately 12 cc greater than the final inflation volume to allow the central bolus to interdigitate with the surrounding cancellous bone . results vertebroplasty the results of vertebroplasty in the 485 patients , divided by condition causing the symptoms , are shown in table 1 . 
the best results were seen in patients with mentre nei casi di lesioni litiche di origine metastatica ( 160 pazienti ) lutilizzo della tc associata ad un arco c portatile ha permesso un pi facile approccio e preciso posizionamento dellago nellarea di osteolisi . 
tutte le procedure di kp sono state eseguite sotto guida fluoroscopica . i pazienti sono stati valutati prima e dopo il trattamento a 1 , 3 e 6 mesi con il metodo visual analogyc scale ( vas ) e oswestry disability scale ( ods )  . tecniche di esecuzione della vp una volta ottenuta unimmagine radiografica in cui le limitanti somatiche superiori e inferiori del soma risultavano perfettamente sovrapponibili e le apofisi spinose proiettate sulla linea mediana , si proceduto allapproccio del peduncolo vertebrale mediante un ago da 11 g o 13 g , di una lunghezza variabile da 10 cm a 15 cm , con estremit a becco di flauto e munito di alette laterali per facilitarne la rotazione . 
la quantit di cemento iniettata nei pazienti sottoposti a vp stata variabile da un minimo di 24 ml per metameri dorsali con approccio mono - peduncolare sino a 56 ml a livello dorso - lombare e 12 ml a livello lombare . tecnica di esecuzione della kp differentemente dalla vertebroplastica , la cifoplastica prevede sempre accessi trans - peduncolari bilateralmente a paziente prono . 
sotto guida fluoroscopica lago da biopsia ossea da 11 g stato fatto avanzare nel peduncolo vertebrale con uninclinazione idonea dopo incisione cutanea di circa 1 cm estesa alla fascia muscolare per favorire lingresso del trokar . 
successivamente , coassialmente allago , si inserito lago di kirshner che stato utilizzato come guida per far scorrere fino a 3 mm oltre il muro posteriore del corpo vertebrale una cannula di servizio . 
 stato creato quindi mediante un piccolo trapano a mano un canale osseo intraspongioso con estremo distale a pochi millimetri dal margine corticale anteriore per consentire linserimento del catetere a palloncino allinterno del corpo vertebrale fratturato . 
la medesima procedura stata eseguita attraverso il peduncolo controlaterale . una volta posizionati allinterno del soma fratturato entrambi i cateteri a palloncino dedicati , si proceduto al loro simultaneo e progressivo gonfiaggio mediante una miscela di mdc sotto continuo controllo fluoroscopico e manometrico . 
il cemento stato rilasciato lentamen1176 table 1 vertebroplasty results osteoporosis haemangiomas secondary lesions success 90% failure 10% success 100% failure 0% success 77% failure 23% radiol med ( 2008 ) 113 : 11711184 te a bassa pressione e sotto continua guida fluoroscopica in ll in quantit variabile da 4 ml a 6 ml a metamero in funzione del volume finale raggiunto dal catetere a palloncino gonfiato nel soma fratturato e visualizzato sul display del sistema di gonfiaggio . 
1a , b rm sagittale stir e t2w : iperintensit visibile solo nella sequenza sagittale pesata in stir come da edema della spongiosa dei somi l1 e l3 ; c , d controllo dopo vp di l1 , l2 e l3 : buono il riempimento somatico . radiol med ( 2008 ) 113 : 11711184 1177 fig . 
e esame in ll dopo vp , piccola fuga di cemento asintomatica a livello del forame sinistro di l4 . extravertebral cement leakage into the vascular system or intervertebral disc occurred in 39 patients . 
nel follow - up , nei soli pazienti affetti da osteoporosi abbiamo riscontrato fratture di vertebre adiacenti in 25 pazienti e nuove fratture di vertebre a distanza da quella gi trattata in 19 pazienti . radiol med ( 2008 ) 113 : 11711184 1178 fig . 
nella tabella 2 sono riportati i risultati dei 39 pazienti trattati suddivisi in base alla tipo di frattura valutando il dolore prima e dopo il trattamento secondo la valutazione con i metodi vas e ods . 
a controllo in ll sotto scopia del corretto posizionamento dei trokar con approccio bi - peduncolare e dilatazione dei palloncini ; b , c controllo post trattamento kp in ll e ap con buona la distribuzione del cemento e visibilit di peduncoloplastica ; d ricostruzione mpr sagittale del soma trattato con kp e peduncoloplastica . table 2 kyphoplasty results discussione magerl a1 fractures magerl a3 fractures success 95% failure 5% success 90 % failure 10 % tabella 2 risultati della cifoplasica fratture a1 secondo magerl frattura a3 secondo magerl successo 95% insuccesso 5% successo 90% insuccesso 10% le differenze tecniche dei due trattamenti possono essere cosi riassunte : entrambe richiedono lutilizzo costante della guida rxscopica ( apparecchio angiografico o arco a c portatile ) per il corretto posizionamento degli aghi di accesso al corpo vertebrale da trattare ; la procedura di vp viene eseguita in anestesia locale associata a neuroleptoanalgesia ; differentemente la tecnica di kp viene eseguita preferibilmente in anestesia generale , poich maggiormente invasiva e dolorosa ; lapproccio per la vp pu essere bi - peduncolare o mono - peduncolare se lago utilizzato viene posizionato nel 1180 radiol med ( 2008 ) 113 : 11711184 techniques vertebroplasty and kyphoplasty may be summarised as follows : both require constant fluoroscopic monitoring ( angiographic equipment or portable c - arm ) to ensure correct needle position vertebroplasty is performed under local anaesthesia associated with neuroleptanalgesia , whereas kyphoplasty , which is more invasive and painful , is preferably performed under general anaesthesia the approach in vertebroplasty may be bipedicular or unipedicular , with the needle in the midline of the fractured vertebra ; in kyphoplasty , instead , to achieve reexpansion of the vertebra , the approach is necessarily bipedicular , with trocars mounting inflatable balloon tamps in both techniques , the medial wall of the pedicle should never be crossed before reaching the posterior wall of the vertebra , as confirmed on posteroanterior and lateral views both techniques employ pmma . 
for kyphoplasty , however , new cements such as calcibon or tricalcium phosphate / hydroxyapatite can be used to extend the indications to young subjects with recent traumatic fractures the only absolute contraindication is the presence of local or systemic infections reported complications are similar . 
however , the risk of cement leakage during kyphoplasty is lower because the newly created cavity has the effect of containing the cement , the cavity is filled a low pressure , the cement is highly viscous and the volume of cement is predetermined on the basis of the volume of the fully inflated balloon tamp . 
the rationale for the two techniques is that pmma injection into the vertebral body immobilises the vertebral microfractures responsible for pain , thus making the vertebral body more compact and resistant . vertebroplasty is most commonly used to treat osteoporotic vertebral fractures , achieving pain relief in 90%95% of cases [ 21 ]  . 
eligible secondary lesions are osteolytic or mixed lesions , usually secondary to breast cancer ( 30% ) and lung cancer ( 25% ) [ 4 ] , in which symptoms are alleviated in 70%90% of cases . 
recent studies have suggested that the use of pmma in cancer patients has an additional antitumoral effect resulting from the exothermic soma fratturato sulla linea mediana , tale da permettere una distribuzione simmetrica del pmma ; differentemente nella kp , ai fini di ottenere la riespansione del soma , lapproccio necessariamente bi - peduncolare mediante trokar montanti palloncini dedicati ; per entrambe le metodiche non bisogna mai superare la parete mediale del peduncolo sin quando non si raggiunto il muro posteriore del corpo vertebrale , controllato in pa ed ll ; il pmma utilizzato il medesimo in entrambe . 
per la kp si possono utilizzare cementi di pi nuova generazione come il calcibon o il fosfato tricalcico di idrossiapatite estendendo ulteriormente la sua indicazione nei soggetti giovani portatori di fratture traumatiche recenti ; lunica controindicazione assoluta la presenza di infezione sistemica o locale ; le complicanze riportate in letteratura sono pressoch simili . 
tuttavia , il rischio di stravasi di cemento durante la kp ridotto grazie alleffetto contenutivo della cavit preformata nel corpo vertebrale in cui il riempimento del cemento altamente viscoso avviene a bassa pressione e in maniera predeterminata in base al volume della cavit preformata in rapporto al volume raggiunto del palloncino . 
il razionale delle due metodiche si basa sul principio che liniezione del pmma nel soma fratturato permette di stabilizzare i movimenti delle microfratture trabecolari della spongiosa ossea , responsabili della sintomatologia dolorosa , rendono quindi il corpo vertebrale pi compatto e resistente . certamente , data la loro rilevanza epidemiologica , i crolli vertebrali di origine osteoporotica costituiscono le lesioni vertebrali maggiormente trattate con la vp , con una riduzione del dolore variabile dal 90% al 95% dei casi [ 21 ]  . infatti nella nostra casistica , 280 / 310 pazienti ( 90% ) hanno giovato di un miglioramento della sintomatologia dolorosa nelle prime 2472 h secondo la scala vas e ods . 
le lesioni secondarie da trattare sono quelle osteolitiche o miste , pi frequentemente da cancro mammella ( 30% ) o polmone ( 25% ) [ 4 ] , dove la remissione della sintomatologia dolorosa avviene nel 70%90% dei casi . 
nella popolazione neoplastica , studi recenti hanno osservato che , oltre allazione stabilizzatrice del pmma , il cemento provoca una attivit carcinolitica sulle cellule neoplastiche grazie alla reazione esotermica che libera quando polimerizza allinterno del soma vertebrale [ 6 , 22 ]  . il principale rischio della vp consiste nella fuoriuscita del cemento durante la sua introduzione in sede extraverteradiol med ( 2008 ) 113 : 11711184 1181 reaction during polymerisation within the vertebral body [ 6 , 22 ]  . 
 the main risk of vertebroplasty is the extravertebral leakage of cement into the spinal canal and preand paravertebral venous plexus , with consequent compression of nervous structures or pulmonary embolism [ 2329 ]  . 
the rate of thromboembolic complications has been reduced considerably by increased operator skill and the use of denser cements and is now 0.5%1% in osteoporotic fractures [ 22 ]  . 
no cases of pulmonary thromboembolism occurred in our series , whereas symptomatic extravertebral cement leaks into the vascular system or intervertebral disc occurred in 39 out of 485 patients and were treated conservatively . 
the rate of local or systemic complications in patients affected by spinal metastasis ranges from 2% to 5.1% [ 33 , 34 ]  . the risk of new fractures following vertebroplasty is reported to range from 10% to 30% [ 3540 ]  . 
in effect , it is still unclear whether this is related to the natural history of the underlying disease or to the treatment , especially if we consider that the presence of a single vertebral fracture in an osteoporotic patient is highly predictive of future fractures and that women with a single osteoporotic fracture have a 19.2% increased risk of developing new fractures in the following year [ 4143 ]  . vertebroplasty is the treatment of choice for symptomatic aggressive vertebral haemangiomas exhibiting t2 hyperintensity and t1 contrast - enhancement at mri [ 40 ]  . 
the treatment provides definitive sclerosis of the vertebral angioma by completely filling the lesion with cement , with pain relief in 90%100% of cases and no substantial early or late complications [ 44 , 45 ]  . 
a similar result was achieved in our series ( 100% )  . cement distribution and vertebral filling is generally more uniform and regular in patients affected by osteoporosis or haemangiomas compared with those with secondary lesions . 
in addition , no correlation has been found between cement volume and pain relief , as the volume injected depends on the degree of vertebral collapse and on the vertebral level treated , with smaller amounts being injected into thoracic vertebrae with wedge deformity ( as little as 4 ml ) compared with lumbar vertebrae without wedging ( up to 12 ml )  . 
il leakage extrasomatico pi frequente nelle fratture vertebrali metastatiche , con una percentuale variabile tra il 30% e 60% dei casi , e meno frequentemente nei crolli porotici di circa il 10% dei casi [ 3032 ]  . 
il tasso di complicanze tromboemboliche si ridotto considerevolmente , sia per la maggiore confidenza da parte degli operatori , sia per la commercializzazione di nuovi cementi pi densi ed attualmente dellordine del 0 , 5%1% dei casi nelle fratture porotiche [ 22 ]  . 
nella nostra casistica non abbiamo osservato casi di tromboembolie polmonari ; mentre abbiamo riscontrato fughe extravertebrali vascolari o discali , responsabili di sintomatologia radicolare , trattata con terapia medica , in 39 su 485 sottoposti a vp . 
il tasso di complicanze locali o sistemiche nei pazienti trattati con vp affetti da metastasi vertebrali invece variabile dal 2% al 5 , 1% [ 33 , 34 ]  . il rischio di nuove fratture a distanza di tempo dopo lesecuzione del trattamento con vp variabile dal 10% al 30% dei casi [ 3540 ]  . 
in realt non ancora chiaro se questo fenomeno sia legato alla normale evoluzione della malattia di base o al trattamento eseguito , considerando che una sola frattura vertebrale nel paziente porotico altamente predittiva per la comparsa di pi fratture in futuro e che in donne portatrici di un primo crollo porotico , il rischio di sviluppare nuove fratture nellanno successivo dimostrato essere di circa il 19 , 2% [ 4143 ]  . la vp la tecnica di scelta per il trattamento degli angiomi vertebrali sintomatici con segni di aggressivit alla rm denunciati dalliperintensit in t2 e dallimpregnazione di mdc ev in t1 [ 40 ]  . 
lo scopo di ottenere una sclerosi definitiva dellangioma vertebrale attraverso il riempimento completo della lesione mediante il cemento con remissione della sintomatologia dolorosa variabile dal 90% al 100% dei casi , senza sostanziali complicanze precoci o tardive [ 44 , 45 ] ; infatti noi abbiamo osservato un analogo risultato ( 100% )  . la diffusione ed il riempimento dei metameri trattati con vp stato generalmente molto pi omogeneo e regolare nei casi affetti da osteoporosi o angiomi rispetto a quelli affetti da lesioni secondarie ; tuttavia il successo del trattamento non correlabile alla diffusione omogenea o disomogenea del cemento nel contesto del metamero trattato . 
inoltre , non dimostrata alcuna correlazione tra quantit di cemento iniettata e remissione della sintomatologia in quanto ci dipeso dal grado di schiacciamento del metamero e dal livello del metamero trattato con minore quantit di cemento iniettata a livello dorsale con cuneizzazione ( anche solo 4 ml ) rispetto ai metameri lombari non cuneizzati ( sino a 12 ml )  . 
 kyphoplasty is used for the treatment of type a1 and a3 traumatic vertebral fractures according to the magerl le fratture vertebrali traumatiche trattate con la kp sono quelle di tipo a1 e a3 secondo la classificazione di 1182 radiol med ( 2008 ) 113 : 11711184 classification [ 20 ]  . 
by reexpanding the vertebra with balloon tamps , kyphoplasty reduces the pathological kyphosis , allowing restoration of normal vertebral biomechanics , early mobilisation of the patient and pain relief in 90%100% of cases , provided that the procedure is performed no later than 3 months after the trauma and the pedicles are intact and of adequate size [ 31 , 32 , 46 , 47 ]  . 
in effect , kyphoplasty has been shown to restore vertebral height in 10%20% of cases , with a reduction in wedge angle varying between 6 and 9 [ 47 , 49 , 50 ]  . 
in our series , we achieved pain relief in 90%95% of cases , depending on type of fracture , and an increase in vertebral body height sufficient to allow early mobilisation of the patient and restoration of the physiological distribution of postural forces 5153 ]  . 
however , even vertebroplasty has been shown to restore vertebral body height and correct pathological kyphosis , with outcomes that are only slightly inferior to kyphoplasty [ 5456 ]  . magerl [ 20 ] per le quali la sola terapia fin dora stata quella conservativa mediante lapplicazione di unortesi per un periodo che va da 4 a 6 mesi , spesso seguita da una guarigione costantemente in cifosi della vertebra fratturata . 
la kp , riespandendo il soma in altezza mediante i cateteri a palloncino , permette di ridurre la cifosi patologica ristabilendo la normale bio - meccanica vertebrale , di mobilizzare il paziente in tempi brevi e di ridurre la sintomatologia dolorosa nel 90%100% dei casi , purch eseguita entro 3 mesi dal trauma e i peduncoli siano integri e di adeguate dimensioni [ 31 , 32 , 46 , 47 ]  . 
 [ 48 ] , da uno studio su cadaveri , hanno dimostrato che ogni kp produce un ripristino dellaltezza somatica nel 47% dei casi e una correzione della cifosi nel 10% . 
in realt si visto che la kp permette di ripristinare laltezza del soma fratturato in una percentuale variabile dal 10% al 20% dei casi con un escursione in termini di gradi variabili da 6 a 9 gradi [ 47 , 49 , 50 ]  . 
nella nostra casistica , abbiamo ottenuto una riduzione della sintomatologia dolorosa variabile dal 90% al 95% a seconda del tipo di frattura registrando un incremento minimo dellaltezza somatica tale da garantire una rapida mobilizzazione del paziente e ripristinando fisiologica distribuzione delle forze posturali [ 5153 ]  . 
tuttavia , anche nella vp dimostrato una capacit di ripristinare laltezza del soma e di correggerne la cifosi patologica con un outcome di poco inferiore rispetto a quello ottenuto con la kp [ 5456 ]  . conclusions conclusioni on the basis of our results and the literature , we believe that both techniques vertebroplasty and kyphoplasty are effective for managing spinal pain and symptomatic vertebral fractures due to osteoporosis , aggressive haemangiomas and osteolytic neoplasms without involvement of the posterior vertebral wall or epidural space . 
alignment of the fractured vertebral body with reduction of posttraumatic kyphosis , physiological distribution of postural forces , early mobilisation of the patient and no need for postoperative bracing widely justify the exclusive use of kyphoplasty in this setting , especially in view of the current availability of biological cements that undergo rapid and complete osteointegration . sulla base di questi dati e su quanto esposto , riteniamo che entrambe le metodiche permettono un buon management delle sindromi antalgiche vertebrali e nei crolli sintomatici su base osteoporotica , angiomatosici con caratteri di aggressivit , di tipo neoplastico - osteolitico senza compromissione del muro posteriore e senza interessamento epidurale . in tali patologie la scelta delluna o dellaltra metodica a favore decisamente per la vp , in considerazione anche dell elevato costo della kp , purch eseguita con idonea tecnologia . 
chieffi 40 , 70051 barletta , italy , tel . : + 39 - 339 - 2452701 , fax : + 39 - 088 - 1733866 , e - mail : paomi03@libero.it received : 6 august 2007 / accepted : 25 february 2008 / published online : 25 october 2008 springer - verlag 2008 abstract purpose . 
thirty - one patients underwent arthroscopic surgery for acl reconstruction using doubled gracilis and semitendinosus tendons fixed to the tibial tunnel with plla - ha ( biorci - ha ) screws . 
valutare con imaging rm gli aspetti dei processi di degradazione ed osteointegrazione di una nuova classe di viti ad interferenza bioriassorbibili in acidi l - polilattici ed idrossiapatite ( plla - ha ) , utilizzate per la fissazione di innesti tendinei nelle plastiche pro - lca . 
trentuno pazienti sono stati sottoposti ad intervento chirurgico di ricostruzione di lca con tendini di muscoli gracile e semitendinoso duplicati , fissati a livello del tunnel tibiale con viti plla - ha . 
due gruppi di pazienti sono stati valutati dopo lintervento chirurgico rispettivamente a distanza , uno di 1013 mesi , laltro di 3040 mesi , utilizzando la scheda dellinternational knee documentation committee ( ikdc ) per la valutazione clinica ; la valutazione radiologica stata effettuata mediante rm . 
dallanalisi dei risultati rm emerso che nei controlli pi ravvicinati erano presenti reperti legati ai processi di guarigione ed integrazione osso - innesto - vite , non pi evidenti nel follow - up effettuato tardivamente . 
lassenza di artefatti 1186 radiol med ( 2008 ) 113 : 11851197 adequate evaluation of ligament synovialisation , screw degradation and graft osteointegration . keywords bioabsorbable interference screws hydroxyapatite osteointegration magnetic resonance ferromagnetici delle viti ha consentito unefficace valutazione con rm dei processi di sinovializzazione del neo - legamento , di quelli di degradazione delle viti bioriassorbibili e di osteointegrazione dellinnesto . parole chiave vib idrossiapatite osteointegrazione risonanza magnetica introduction introduzione first described by kurosaka et al . 
primary fixation of the graft is fundamental during the initial period of knee stabilisation , and it is necessary that the screws preserve their structural integrity until osteointegration of the bonescrewgraft system has been achieved . 
in recent years , special attention has been paid to screws composed of polyl - lactic acid polymers ( plla ) , which ensure strong fixation of the new ligament comparable with that of metallic implants the possibility of surgical revision , poor inflammatory response , low incidence of adverse reactions and easy biological incorporation of the graft into the bone tunnel [ 3 ]  . 
these are related to surgical technique , excessive hydrolysation of the screw , decreased ph , biocompatibility problems and incomplete osteointegration with resulting loss of torsional strength and graft instability [ 46 ]  . 
this has led to the introduction of screws composed of materials having biomechanical properties that are both more reliable and closer to those of metallic implants , that is , materials that are not only bioabsorbable and biocompatible but also osteoinductive : polymer - ceramic composite materials made up of plla and hydroxyapatite ( ha ) granules . knowledge of the structural and biological properties of ha ( biorci - ha ) and evaluation of their osteointegration processes are essential for understanding clinical outcome and radiological patterns . 
a peculiar feature of ha is that it forms crystal deposits arranged in a network of cells that are subsequently colonised by osteoblasts , and thus it provides the scaffold on which the new bone will grow [ 7 ]  . the literature contains no magnetic resonance imaging ( mri ) studies carried out in humans to investigate the precise significance of signal - intensity changes of plla - ha screws used for tibial fixation of acl grafts or the degradation and osteointegration processes of such screws . 
the aim of this study was to evaluate the mri features of the degradation of plla - ha bioabsorbable screws and of their biological behaviour and osteointegration processes . le viti ad interferenza bioriassorbibili , descritte per la prima volta da lambert e kurosaka , rappresentato il gold standard nella moderna chirurgia artroscopica del ginocchio [ 1 , 2 ]  . 
la fissazione primaria dellinnesto di fondamentale importanza nel periodo di stabilizzazione iniziale ed necessario che le viti conservino la propria integrit strutturale fino alla integrazione del sistema osso - viteinnesto . 
negli ultimi anni le applicazioni cliniche hanno rivolto particolare interesse a viti composte da polimeri di acidi polilattici ( plla ) , che sono dotate di resistente fissazione del neo - legamento , paragonabile a quella dei mezzi di sintesi metallici , possibilit di revisione chirurgica , scarsa risposta infiammatoria , bassa incidenza a reazioni avverse , facilit di incorporazione biologica dellinnesto nel tunnel osseo [ 3 ]  . 
tali viti tuttavia non sono scevre da limiti che sono in parte legati alla tecnica operatoria , in parte dovuti alla eccessiva idrolisi che subisce la vite , alla diminuizione del ph e a problemi di biocompatibilit , e in parte dovuti alla non completa integrazione ossea con conseguente perdita della forza torsionale dellinnesto e conseguente instabilit [ 46 ]  . 
pertanto si pensato allintroduzione di viti costituite da materiali dotati di caratteristiche biomeccaniche pi affidabili e pi vicine a quelle dei mezzi di sintesi metallici , ovvero a composti che oltre che dotati di caratteristiche di bioriassorbibilit e biocompatibilit posseggono altres la peculiarit di essere osteoinducenti ; si tratta di composti polimerici - ceramici costituiti da acidi polilattici ( plla ) e granuli di idrossiapatite ( ha )  . la conoscenza delle propriet strutturali e biologiche delle vib - ha e la valutazione dei processi di osteointegrazione delle stesse sono fondamentali per la comprensione dei risultati clinici e di semeiotica radiologica . 
lidrossiapatite possiede la peculiare caratteristica di creare depositi di cristalli che si dispongono creando un reticolo di cellette che saranno successivamente colonizzate da osteoblasti e costituiranno lo scheletro nel quale crescer il futuro osso neofomato [ 7 ]  . in letteratura non sono riportati studi con rm su uomo che stabiliscano con esattezza il significato delle alterazioni di segnale delle viti plla - ha utilizzate per la fissazione tibiale di innesti pro - lca , nonch dei processi di degradaradiol med ( 2008 ) 113 : 11851197 materials and methods between december 2003 and june 2007 , we evaluated 31 patients who had undergone arthroscopic surgery for acl reconstruction in 2003 ( 18 on the right knee and 13 on the left knee ) due to anterior laxity . 
the tibial tunnel was drilled under arthroscopic guidance with the aid of an adequately sized drill guide placed at an angle of 55 in the sagittal plane and approximately 20 in the frontal plane . 
 of the 31 patients ( 20 men and 11 women ; age range 1749 years , mean age 26.7 ) , 15 had sustained a sports trauma , nine a road accident and seven other types of accident . 
associated lesions were diagnosed with mri and confirmed at surgery in 22 knees : 16 lesions of the medial meniscus , three of the lateral meniscus , four grade 1 or grade 2 chondropathies of the medial femoral condyle and one grade 2 chondropathy of the medial tibial plateau ; there were no associated ligament lesions . all patients underwent follow - up clinical assessment with the international knee documentation committee ( ikdc ) form consisting of a subjective evaluation of symptoms and functional tests , as well as radiological assessment with mri to evaluate osteointegration of the graft at the tibial level . 
patients were divided into two groups according to the time elapsed between arthroscopic surgery and the follow - up assessments : one group , consisting of 15 patients , was evaluated after 1013 months ; the other group , consisting of 16 patients , was evaluated after 3040 months . mri assessment was carried out with a 1.5 - tesla unit ( magnetom 63p , siemens )  . 
the study protocol featured the use of a dedicated surface coil for the knee ; scans in the axial , coronal and sagittal plane with a slice thickness of 34 mm ; field of view ( fov ) 160 mm ; rectangular field of view ( rfov ) 80% ; matrix 192256 . 
scopo del nostro lavoro stato valutare gli aspetti rm dei processi di degradazione delle viti bioriassorbibili plla - ha , del comportamento biologico e dei processi di osteointegrazione cui vanno incontro . materiali e metodi nel periodo tra dicembre 2003 e giugno 2007 , sono stati valutati 31 pazienti sottoposti ad intervento chirurgico , nel 2003 , per via artroscopica , di ricostruzione del legamento crociato anteriore del ginocchio ( 18 del ginocchio destro e 13 del ginocchio sinistro ) per lassit anteriore . 
per la fissazione degli innesti sono stati utilizzati il sistema cross - pin per il tunnel femorale e le viti ad interferenza bioriassorbibili composte da una miscela di plla - ha ( vite biorci - ha ) per il tunnel tibiale . la preparazione del tunnel tibiale , sotto guida artroscopica , avvenuta con lausilio di una fresa di dimensioni adeguate allinnesto con angolo di 55 sul piano sagittale e 20 circa sul piano frontale . 
 dei 31 pazienti ( 20 maschi e 11 femmine ) , con et variabile tra 17 e 49 anni e con una media di 26 , 7 anni , 15 avevano subito un trauma sportivo , 9 un trauma stradale e 7 un trauma accidentale . 
in 22 ginocchia erano associate altre lesioni diagnosticate con studio rm e poi confermate chirurgicamente : 16 del menisco mediale , 3 del menisco laterale , 4 condropatie del condilo femorale mediale ( cfm ) di 1 / 2 , ed 1 condropatia del piatto tibiale mediale ( ptm ) di 2 ; nessuno riportava lesioni legamentose associate . tutti i pazienti sono stati sottoposti a controlli clinici , utilizzando la scheda international knee documentation commitee ( ikdc ) che prevede oltre che una valutazione soggettiva dei sintomi anche tests funzionali , e a controlli radiologici con valutazione rm dello stato ed avvenuta osteointegrazione dellinnesto a livello tibiale . 
i pazienti sono stati suddivisi in due gruppi a seconda della distanza di tempo dallintervento chirurgico cui venivano effettuati i controlli : un gruppo , di 15 pazienti , valutato a breve distanza di tempo ( dopo 1013 mesi ) ; un gruppo , di 16 pazienti , valutato a lunga distanza di tempo ( dopo 3040 mesi )  . per la valutazione radiologica i pazienti sono stati sottoposti ad esami rm con unapparecchiatura da 1 , 5 tesla ( magnetom 63p , siemens )  . 
lo studio ha previsto lutilizzo di una bobina di superficie dedicata allo studio del ginocchio , scansioni sui piani assiale , coronale e sagittale con spessore di strato di 34 mm , campo di vista ( fov ) 160 mm , campo di ricostruzione ( rfov ) 80% , matrice di 192256 . 
sono 1188 radiol med ( 2008 ) 113 : 11851197 stabilisation period , which varies according to the tendons used and is reported to be 812 weeks for the gracilis and semitendinosus tendons [ 8 , 9 ]  . mr images were assessed independently by three radiologists who considered the following : 1 . 
eight patients were classified as group b ( mean subjective score of 80% , joint disturbances during moderate physical activity , complete range of movement , negative lachman test with 2to 3.5 - mm translation , moderate femoropatellar crepitation and functional test scores of 76%90% )  . 
this patient had a negative subjective evaluation , pain during mild physical activity , complete range of motion , positive lachman test and a functional test score of table 1 results of the international knee documentation committee ( ikdc ) evaluation form group group a group b group c group d gruppi gruppo a gruppo b gruppo c gruppo d tabella 1 scheda valutazione ikcd n . 
i processi di maturazione del neo - legamento : valutati secondo i parametri presenti in letteratura [ 814 ]  . risultati nella valutazione clinica eseguita utilizzando la scheda ikdc ( tabella 1 ) , 22 pazienti sono rientrati nel gruppo a con valutazione soggettiva media del 90% , con lieve dolore dopo strenua attivit fisica , arco di movimento completo , lachman negativo con il 40% con traslazione di 12 mm ed il 60% di 2 , 53 , 5 mm e test funzionale valutato al 90%100% . 8 pazienti sono stati riportati nel gruppo b , con evidenza di una valutazione soggettiva media dell80% , comparsa di disturbi articolari durante moderata attivit fisica , arco di movimento completo e test di lachman negativo con traslazione di 23 , 5 mm , moderati crepitii femoro - rotulei e test funzionale al 76%90% . 
in questo paziente sono stati riscontrati una valutazione soggettiva negativa , comparsa di dolore durante attivit fisica leggera , arco di movimento completo e test di lachman positivo con un test funzionale al 50% . 
axial t2 * weighted gradient echo ( ge ) ( a ) and coronal t2 - weighted inversion recovery ( ir ) ( b ) magnetic resonance ( mr ) images . 
the screw was surrounded by a rim of hyperintense tissue , ascribable to hydration of the screw itself , and representing a slight effusion and / or fluid produced by early degradation processes ; this tissue tended to become hypointense at later follow - up examinations as a result of tissue transformation . 
all cases showed a reduction in signal intensity at later follow - up examinations ascribable to the presence of fibrous tissue around the screw and likely calcification . arthrosynovitis was seen in 20 cases ( 19 mild and one marked )  . 
la vite era circondata da un vallo di tessuto inizialmente con segnale iperintenso , attribuibile alla idratazione della vite stessa , rappresentato da sottile falda di versamento e / o da liquido prodotto dagli iniziali processi di degradazione della vite , che diveniva ipointenso nei controlli a distanza come per trasformazione tissutale . 
in tutti i casi , infatti , stata anche rilevata una riduzione di segnale nei follow - up pi tardivi da imputare alla presenza di tessuto simil - fibrotico intorno alla vite e alla probabile involuzione calcifica dello stesso . lartrosinovite stata riscontrata in 20 casi , in 19 di grado lieve ed in 1 di grado marcato in 2 casi , nei controlli a breve distanza di tempo dallintervento chirurgico , era 1190 radiol med ( 2008 ) 113 : 11851197 fig . 
il sistema cross - pin di fissazione del neo - legamento a livello del tunnel femorale ( a ) appare come una struttura lineare ipointesa ( punta di freccia )  . 
axial t2 * weighted gradient echo ( ge ) ( a ) and coronal t2 - weighted inversion recovery ( ir ) ( b ) magnetic resonance ( mr ) images . 
axial t2 - weighted spin echo ( se ) ( a ) and coronal t2 - weighted inversion recovery ( ir ) ( b ) magnetic resonance ( mr ) images . 
1 confermano la presenza della formazione simil - cistica ( frecce ) e dimostrano il neo - legamento lca slargato , disomogeneo e inglobato da reazione sinoviale in una fase precoce del processo di sinovializzazione ( punte di freccia )  . 1192 radiol med ( 2008 ) 113 : 11851197 fig . 
sagittal t1 - weighted spin echo ( se ) ( a ) and t2 * weighted gradient echo ( ge ) ( b ) magnetic resonance ( mr ) images . 
this process is related to progressive intrinsic revascularisation that starts at the periphery , with vascular branches originating from the synovial membrane and extending to the central portion of the new ligament [ 1114 ]  . 
the biorci - ha screw was always identified in all patients , even after 3040 months . discussion acl injuries are very frequent in sports enthusiasts , with an estimated incidence of more than 100 , 000 / year among skiers in the usa and france [ 1518 ]  . 
in tutti i pazienti stata sempre identificata la vite biorci - ha , anche nelle valutazioni pi tardive . le lesioni del legamento crociato anteriore ( lca ) sono radiol med ( 2008 ) 113 : 11851197 table 2 magnetic resonance imaging results findings mild arthrosynovitis severe arthrosynovitis slight bone oedema around the tunnel tunnel effusion tunnel cyst screw visualisation fibrous - like tissue around the screw tabella 2 risultati rm aspetti artrosinovite lieve artrosinovite severa tenue edema osseo peri - tunnel versamento nel tunnel cisti nel tunnel visualizzazione vite tessuto simil - fibrotico peri - vite mri is , in fact , the only method able to document , albeit through indirect criteria , the healing of new ligaments [ 10 , 18 , 2225 ]  . 
the advantages include gradual resorption and replacement with new bone leading to graft osteointegration , a replacement that does not seem to occur with plain biorci screws [ 28 ]  . in vivo investigations in animal models demonstrated that the screws persisted for years after their surgical role had ended , a finding confirmed by long - term histopathological studies . 
the first reaction of tissue to the presence of the screw is the sequestration of the implant within new bone during the initial 3 months ( stage i )  . 
after a period of nonreactivity ( stage ii ) , a second tissue reaction is associated with early signs of plla degradation at 1 year ( stage iii )  . 
subsequently , the polymer mass is replaced by avascular fibrous tissue containing macrophages and varying numbers of multinucleated giant cells on the implant surface ( stage iv )  . after 3 years , much of the polymer is still present , although in isolated fragments [ 29 ]  . 
one study performed with ct and standard radiography on patients who had undergone acl reconstruction with patellar tendon and plla bioabsorbable screws reported no evidence of screw remnants 7 years after surgery [ 28 ]  . the mechanism for absorption of the plla screw is essentially that of a 360 degradation of the implant edges , 1193 molto frequenti negli sportivi con stime che attestano oltre 100000 lesioni / anno solo nella pratica dello sci in usa e in francia [ 1518 ]  . 
infatti al radiologo viene sempre pi richiesta una valutazione del risultato chirurgico e una attenta valutazione dellattecchimento e integrazione del trapianto [ 1921 ]  . al momento infatti non esistono altre metodiche se non la rm in grado di fornire dei criteri sia pure indiretti sulla guarigione del neo - legamento [ 10 , 18 , 2225 ]  . 
la loro utilit va ricercata nel riassorbimento graduale e nella loro sostituzione con osso neoformato determinando la cosiddetta osteointegrazione dellinnesto , sostituzione ossea che non sembra verificarsi con le semplici viti ad interferenza bioriassorbibili [ 28 ]  . in vivo gli studi sulle viti sono stati possibili su modelli animali in cui stato possibile verificare la persitenza per anni delle stesse , dopo che la propria funzione chirurgica sia conclusa ; questo confermato da studi istopatologici a lungo termine effettuati su animale . 
segue un periodo di non reattivit ( stadio ii ) e successivamente una seconda reazione tissutale associata agli iniziali segni di degradazione del plla ad un anno ( stadio iii )  . 
uno studio effettuato , con valutazioni con tc e radiografie standard , su pazienti sottoposti a ricostruzione di lca con tendine rotuleo e viti bioriassorbibili di plla , ha riportato che dopo 7 anni dallintervento chirurgico non sono pi evidenti segni di materiale residuo della vite bioriassorbibile [ 28 ]  . il meccanismo dassorbimento della vite bioriassorbibile di plla essenzialmente quello di una degradazione periferica a 360 ; in sostanza la vite si riduce perifericamente nel tempo sostituita da tessuto cicatriziale fibrotico ; questo aspetto potrebbe per non favorire nel tempo losteointegrazione nella spongiosa . 
nelle viti con rinforzo di ha , mentre lelemento in polilattico metabolizzato , la parte in ha costituisce uno scheletro che continua nel tempo a mantenere la sua integrit strutturale e quindi a sostenere la compressione dellinnesto . 
la porosit utilizzata dagli osteoblasti per la colonizzazione delle vite completando dunque il processo di osteointegrazione [ 7 ]  . lintroduzione di tali materiali composti da miscele di acidi polimerici cristallini , plla ed idrossiapatite , hanno 1194 radiol med ( 2008 ) 113 : 11851197 which shrink over time and are replaced by fibrous scar tissue ; this aspect may , however , hinder osteointegration in the cancellous bone . 
in screws reinforced with ha , the polylactic component is metabolised , whereas the ha portion constitutes a scaffold that retains its structural integrity and continues to support compression of the graft . porosity favours screw colonisation by osteoblasts and thus the osteointegration process [ 7 ]  . 
 principal mri findings in evaluation of the integration and degradation of the biorci - ha screws were : signal intensity and morphological features of the screw ( relating to degradation and complete or partial visualisation ) articular inflammatory reaction processes ( arthrosynovitis ) , bone and tunnel aspects : presence of oedema , effusion , cysts and granulation and fibrous tissue maturation processes of the new ligament . arthrosynovitis and joint effusion were more frequent at follow - up after 1013 months . 
they may be related to the first three stages of screw degradation [ 29 ] and as such are normal findings , reflecting the physiological response to surgery and the introduction of a foreign body . 
cancellous bone oedema around the tunnel is a reaction to a surgical insult , such as thermal necrosis , rather than a specific reaction to the bioabsorbable screw [ 30 ]  . 
the absence of cancellous bone oedema at 3040 months may be explained by the rapid healing of the bonetendon / new ligament interface . mri is highly sensitive for demonstrating bone marrow oedema , and the healing is confirmed by the absence of high signal intensity in the cancellous bone around the tunnel on high - contrast images [ 10 ]  . with regard to the presence of cyst - like formations in the tunnel , seen in only three cases in our series , we can state that they were the result of pressure and gravity forces causing the effusion to be arranged into more - or - less circumscribed fluid collections . 
previous studies have reported the appearance of tibial cysts 8 months after surgery with biorci screws , but such cysts were also observed with the use of metallic osteosynthesis devices [ 31 , 32 ]  . 
in our study , these cyst - like masses had sharp margins at 1013 months and hazy margins at later followup studies , and they initially contained hyperintense , hydrated tissue on t2 - weighted images , accounted for by the product of screw hydrolysis ; at 3040 months , the tissue had fibrous - like signal intensity probably due to dehydration . 
we hypothesise that screw degradation is responsible for effusion due to leakage of biodegradable material that subsequently becomes organised into cyst - like formations in which there is calcium precipitation and subsequent bone remodelling . 
 gli elementi semeiologici rm di maggiore rilievo nella valutazione dei processi di integrazione e degradazione delle viti biorci - ha da noi considerati sono stati : le caratteristiche di segnale e morfologiche della vite ( relative alla sua degradazione e alla visualizzazione completa e parziale ) ; i processi flogistico - reattivi articolari ( artrosinovite ) gli aspetti dellosso e del tunnel : presenza di edema , versamento , cisti e tessuto di granulazione e fibrotico ; i processi di maturazione del neolegamento . lartrosinovite e il versamento articolare sono stati maggiori nei casi con follow - up pi ravvicinato e potrebbero essere legati ai primi tre stadi di degradazione delle viti [ 29 ] risultando quindi normali reperti dovuti alla fisiologica risposta dellorganismo allintervento chirurgico e allintroduzione della vite quale corpo estraneo . 
ledema osseo intra - spongioso peri - tunnel riconducibile ad una reazione allinsulto chirurgico come necrosi termica oltre che ad una eventuale associata reazione specifica alla vite bioriassorbibile [ 30 ]  . 
lassenza dello stesso , nei controlli effettuati a maggiore distanza di tempo , ha come possibile spiegazione una rapida guarigione dellinterfaccia ossotendine / neo - legamento e la rm altamente sensibile nella dimostrazione delledema midollare , confermata dalla assenza di iperintensit del segnale nelle immagini ad alto contrasto che consentono di dimostrare lassenza di iperintensit del segnale della spongiosa adiacente al tunnel [ 10 ]  . in merito alla presenza di formazioni simil - cistiche allinterno del tunnel , da noi riscontrate in soli 3 casi , possiamo dire che le prime non sono altro che il risultato di forze di pressione e di gravit che rendono conto della disposizione del versamento in raccolte pi o meno circoscritte . 
in letteratura stata descritta la comparsa di una cisti tibiale dopo 8 mesi dallintervento chirurgico con vib ma tali fenomeni sono stati osservati anche quando erano utilizzati mezzi di sintesi metallica [ 31 , 32 ]  . 
nel nostro studio tali formazioni avevano margini netti nei controlli effettuati a breve distanza di tempo , mentre erano pi sfumati nei controlli a maggiore distanza di tempo , e contenevano allinizio un tessuto iperintenso nelle immagini t2w , idratato , riferibile al prodotto didrolisi della vite ; nei controlli a lunga distanza tale tessuto mostrava segnale simil - fibrotico probabilmente per un processo di disidratazione . 
noi avanziamo lipotesi di una degradazione della vite che responsabile della presenza del versamento per stravaso del materiale biodegradabile che successivamente si organizza in formazioni cistiche nelle quali si ha precipitazione di calcio e successivo rimodellamento osseo . 
in letteratura sono state riportate anche formazioni cistiche peri - tunnel , la cui natura stata ricondotta a gangli intraossei , da considerare reperti occasionali , probabilmente preesistenti , e di nessun significato clinico [ 30 , 33 ]  . in tutti i pazienti stata sempre identificata la vite biorci - ha , anche nel follow - up pi tardivo , con segnale radiol med ( 2008 ) 113 : 11851197 1195 formations around the tunnel , which are thought to represent intraosseous ganglia , and probably preexisting incidental findings of no clinical significance [ 30 , 33 ]  . the biorci - ha screw was always identified in all patients , even at later follow - up examinations , with a signal that became more hypointense the longer the time between surgery and mri follow - up . 
this hypointensity could be ascribed to bone apposition promoted by ha and progressive calcification of the fibrous tissue formed around the screw during the initial degradation stage . with regard to implant appearance , we found , in agreement with amiel et al . 
synovial maturation , which results from activation of synovial fibroblasts , transforms the tendon tissue by altering the structure of collagen fibres and producing neoangiogenesis , until the implant matrix shows similar histological and biochemical characteristics to the fibrous tissue of the healthy cruciate ligament . 
on mri , this is reflected in a progressive change of signal intensity over time , with three main phases : ( 1 ) periligamentous proliferation phase , where t1 - weighted se images reveal a central portion of hypointensity and a concentric peripheral portion of fibroblastic proliferation with marked signal hyperintensity ; ( 2 ) intraligament proliferation phase , where t1 - weighted se images show the synovial maturation phenomena to extend the central portion of the graft , which has stronger signal intensity and a more inhomogeneous appearance ; ( 3 ) final maturation , in which the mature implant displays low signal intensity similar to the healthy ligament [ 10 ]  . the new acl in our study appeared irregular and inhomogeneous at 10 months and showed regular course and homogeneous signal at 3040 months , probably as a result of complete synovialisation of the gracilis and semitendinosus tendons . 
tale ipointensit potrebbe essere riferita alla neoapposizione ossea favorita dallidrossiapatite e dalla progressiva calcificazione del tessuto fibrotico costituitosi intorno alla vite nelliniziale periodo di degradazione della stessa . per quanto concerne laspetto del trapianto , nella nostra esperienza , come anche riportato da amiel e howell [ 23 , 24 ] , il neolegamento ha mutato nel tempo le caratteristiche del segnale rm in accordo con il procedere dei processi di maturazione sinoviale . 
tale fenomeno dovuto allattivazione dei fibroblasti sinoviali trasforma il tessuto tendineo modificando la struttura delle fibrille collagene , producendo una neo - angiogenesi , sino a che la matrice del trapianto assume caratteristiche strutturali istologiche e biochimiche molto simili al tessuto fibroso del legamento crociato sano . 
 il neo - lca nel nostro studio appariva infatti , irregolare e disomogeneo nei controlli pi ravvicinati ( a 10 mesi ) ; nei controlli effettuati a 3040 mesi dallintervento chirurgico mostrava regolare decorso e segnale omogeneo verosimilmente per il completamento del processo di sinovializzazione dei tendini gracile e semitendinoso . 
 conclusions biorci screws composed of plla blended with ha represent a valuable alternative to metallic interference screws . effusion within the tunnel and cyst - like and fibrous - like tissue should not be considered adverse reactions to the bioabsorbable screw but normal findings during the initial period of integration of the screwbonegraft system and screw degradation , which explains why none of these findings are detected at later mri follow - up examinations ( 3040 months )  . in addition to greater primary stability and superior osteoconduction due to the presence of ha , which promotes new bone apposition [ 34 , 35 ] , another advantage of the use biorci - ha screws is related to the basic ph of ha and its conclusioni le viti ad interferenza bioriassorbibili composte da acidi polilattici in configurazione levogira ( plla ) in miscela con idrossiapatite ( ha ) costituiscono una valida alternativa ai mezzi di sintesi metallici . 
il versamento nel tunnel , il tessuto simil - cistico e quello simil - fibrotico non devono essere considerati una reazione avversa alla vite bioriassorbibile ma normali reperti durante il periodo iniziale di integrazione del sistema vite - osso - innesto e di degradazione delle viti motivo per cui nessuno di tali reperti pi visualizzabile nei controlli rm a maggiore distanza di tempo ( 3040 mesi )  . oltre ad una maggiore stabilit primaria ed una superiore osteoconducibilit dovuta alla presenza di ha che ne garantirebbe una reale neoapposizione ossea [ 34 , 35 ]  . 
un ulteriore vantaggio nellutilizzo delle viti biorci - ha sarebbe legato al ph basico della ha stessa e quindi alla 1196 radiol med ( 2008 ) 113 : 11851197 ability to neutralise the acidic ph of the synovial fluid , thereby decreasing its aggressiveness and the risk of complications . 
biorci - ha screws do not give rise to ferromagnetic artefacts and are thus suitable for follow - up with mri . mri findings of the absence of oedema or possible hypertrophic synovial reactions around the tendons , and the morphology , thickness and signal intensity of the new ligament , will reassure both the surgeon and the patient , as they reflect normal progression that is free of complications [ 10 ]  . sua capacit di svolgere unazione di neutralizzazione del ph acido del liquido sinoviale riducendone la sua aggressivit e la possibilit del verificarsi di complicanze . 
the implants examined were : 22 vibrant soundbridge implants , 5 at the long limb of the incus and 17 at the round window , 350 cochlear implants , 95 brainstem implants and 1 implant at the inferior colliculus . 
sono state analizzate retrospettivamente le immagini di tomografia computerizzata ( tc ) di 468 pazienti affetti da ipoacusia congenita o acquisita trasmissiva o neurosensoriale , sottoposti a intervento chirurgico protesico . 
i modelli di impianto esaminati sono stati : 22 vibrant , di cui 5 allapofisi lunga dellincudine e 17 alla finestra rotonda , 350 impianti cocleari , 95 impianti al tronco e 1 al collicolo inferiore . 
la tc e la tcd si sono rivelate metodiche affidabili e relativamente veloci per determinare con 266 radiol med ( 2008 ) 113 : 265277 keywords bionic ear implant computed tomography cone - beam computed tomography precisione la posizione dellimpianto allorecchio medio . la tcd preferibile alla tc per la minor dose radiante somministrata ; la sola radiografia del cranio , sufficiente per visualizzare gli impianti cocleari , al tronco ed al collicolo inferiore , e per effettuarne il follow - up . parole chiave orecchio bionico impianti tomografia computerizzata tomografia computerizzata a raggio conico introduction introduzione deafness is a condition that has significantly increased in recent years : about one quarter of the people affected suffer from severe hearing loss , regardless of age . 
nonetheless , the incidence among the elderly population is the highest , given that over 60% of people aged 70 and older have a hearing loss of at least 25 decibels , whereas 30% of them have such a marked hearing loss that it considerably compromises their ability to communicate . in younger patients , hearing loss ( hypoacusis ) needs to be identified early to effectively intervene and improve the quality of social relations . 
in order to identify the appropriate therapy , knowledge is required regarding aetiology ( genetic or acquired hypoacusis ) , time of onset ( preor postnatal , preor postverbal ) , site ( unior bilateral , symmetrical or not ) and type of hypoacusis ( transmissive , neurosensory , mixed ) [ 13 ]  . moderate to severe hypoacusis is treated with the application of electromagnetic prosthetic implants , known as bionic ear , which are capable of directly stimulating the healthy anatomical structures of the auditory canal , thus compensating for the nonfunctioning structures that impede transmission of audio messages . 
radiological techniques for assessing correct implant positioning require the use of ionising radiation , as the devices are currently a contraindication for the use of magnetic resonance imaging . the aim of the study was to identify the best radiological technique to use in the postoperative follow - up of patients with a bionic ear , taking into consideration diagnostic capabilities and radiation dose administered , particularly as these patients may be young adults or children . materials and methods between january 1993 and june 2006 , we assessed 468 patients ( mean age 34 years , range 3 months to 77 years ) suffering from transmissive or neurosensory hypoacusis who la sordit una patologia che negli ultimi anni significativamente aumentata : circa un quarto delle persone affette ha un grave deficit uditivo , indipendentemente dalla fascia di et . 
la popolazione anziana ne rappresenta comunque la percentuale maggiore , dato che oltre il 60% degli ultrasettantenni presenta una perdita di almeno 25 decibel , ed il 30% di essi affetto da un deficit uditivo cos marcato che determina una notevole compromissione delle capacit di comunicazione . in particolare , nei pazienti pi giovani necessario individuare precocemente il deficit acustico ( ipoacusia ) per intervenire pi efficacemente e migliorare linserimento nella vita di relazione . 
per poter indicare il pi idoneo approccio terapeutico necessario procedere al corretto inquadramento clinico - strumentale del deficit sensoriale del paziente tenendo conto delleziologia , sia essa ipoacusia genetica o acquisita , dellepoca di insorgenza preo post - natale ( preo post - verbale ) , della sede , mono o bilaterale , simmetrica o meno , e del tipo di ipoacusia : trasmissiva , neurosensoriale o mista [ 13 ]  . lipoacusia da moderata a severa viene trattata mediante lapplicazione di impianti protesici elettromagnetici , definiti orecchio bionico , in grado di stimolare direttamente strutture anatomiche integre della via uditiva , supplendo a quelle non pi funzionanti che impediscono la trasmissione del messaggio sonoro . 
 lo scopo del presente lavoro quello di individuare quale sia la migliore tecnica radiologica da utilizzare nel controllo postoperatorio e nel follow - up dei pazienti con orecchio bionico , che tenga conto della capacit diagnostica nel rispetto della dose radiante somministrata , proprio perch talora i pazienti sono giovani o in et pediatrica . radiol med ( 2008 ) 113 : 265277 were unable to benefit from mechanical implants at the auditory ossicles and who underwent surgery for bionic ear implant during this period . 
as well as functional and instrumental tests , the patients treated for hypoacusis underwent plain - film radiography and / or high - resolution computed tomography ( hrct ) and / or cone - beam ct ( table 1 )  . 
some of these patients ( the first in chronological order ) underwent all of the radiological techniques , given the lack of similar studies with cbct to refer to in the international literature . after acquiring the necessary preliminary experience , we used the technique with the lowest radiation dose for equivalent diagnostic information . 
twenty - two received vibrant soundbridge ( vsb ) devices at the middle ear , of which 5 were fixed to the long limb of the incus ( mean age 45 , range 3756 years ) and 17 to the round window ( mean age 42 , range 176 years )  . three hundred and fifty received cochlear implants ( mean age 45 years , range 3 months to 56 years )  . 
ninety - five implants were inserted on the brainstem at the level of the cochlear nucleus [ auditory brainstem implantation ( abi ) ] ( mean age 39 years , range 14 months to 70 years )  . 
 i pazienti trattati per ipoacusia , oltre alle indagini oto - funzionali e strumentali , sono stati studiati mediante radiologia convenzionale ( rx ) e con tomografia computerizzata ( tc e / o cone beam computed tomography , cbct ) ( tabella 1 )  . 
alcuni di questi pazienti ( i primi in ordine cronologico ) sono stati sottoposti a tutte le metodiche radiologiche , dal momento che non esiste analoga esperienza con cbct a livello internazionale a cui fare riferimento . 
cbct images were acquired with a maxiscan device ( qr - dvt 9000 , verona , italy ) in the axial plane with a cone base diameter of 15 cm and electronic reconstruction in the coronal plane . type of implants knowledge of the structural components of the different types of bionic implants is desirable for correct interpretation of the radiological images . 
the device used for middle ear implants , which can be fixed to the incus or the round window , is the vsb ( med - el , innsbruck , austria ) , which is made up of an external portion ( the processor ) and an internal portion ( composed of a receiver and a transducer ) ( vorp : internal vibrating ossicular prosthesis )  . 
the processor , which is placed on the scalp in the retroauricular region , contains a magnet to transmit information by electromagnetic induction to the internal parts , a microphone to pick up sounds , a battery and electronic components to convert the acoustic signal into an electronic signal to be transmitted through the skthe processor processes sounds using a programme specifically designed for the type of hypoacusis , and the receiver , implanted beneath the skin , receives the signal from the processor . 
the latter then connects with the transducer , also known as floating mass transducer ( fmt ) [ 4 , 5 ] , which is surgically fixed to the long limb of the incus with a titanium clip and which through a magnet converts the electrical signal into mechanical vibrations , which are then transmitted to the stapes and therefore to the scala vestibuli . 
movement of the perilymphatic fluids reverberates on the cochlear duct and hair cells of the organ of corti , thus stimulating the physiological hearing response [ 6 , 7 ]  . 
the implant is effective in patients with severe mixed hypoacusis resulting from chronic otitis media , malformations of the auditory ossicles or oval window otosclerosis [ 8 ]  . in our ear , nose and throat division , a variation of this type of implant has been developed . 
in this way , the energy is transmitted from the scala tympani , and given the communication with the scala vestibuli at the level of the helicotrema , stimulation of the organ of corti takes place in a similar fashion to the previous technique with the inversion of movement of the fluids [ 9 , 10 ]  . 
this type of implant is suitable for patients suffering from severe forms of appartengono alla casistica 5 pazienti trattati presso altra struttura ospedaliera per ipoacusia neurosensoriale con lapplicazione di un apparecchio vsb sul processo lungo dellincudine . in base alla tipologia di impianto utilizzato , come spiegato pi avanti , i pazienti hanno eseguito un esame rx tradizionale del cranio ( nelle proiezioni convenzionali anteroposteriore , latero - laterale o secondo stenvers ) e / o tc ad alta risoluzione o , in alternativa a questultima , la cbct . le immagini tc mirate alla rocca petrosa sono state effettuate con apparecchi somatom plus ( siemens , erlangen , germania ) secondo i piani trasversale e coronale ( spessore 1 mm ; tecnica sequenziale , incremento del tavolo 1 mm ) e brilliance ct 6 ( philips , eindowen , olanda ) solo sul piano trasversale con ricostruzione elettronica di quello coronale ( spessore 0 , 75 mm ; tecnica spirale , pitch 6 : 0 , 75 )  . 
le immagini cbct sono state effettuate con apparecchio maxiscan ( qr - dvt 9000 , verona , italia ) e acquisite sul piano assiale mediante fascio radiante conico ( diametro base 15 cm ) con ricostruzione elettronica secondo il piano coronale . tipologie di impianti per interpretare le immagini radiologiche ottenute opportuno conoscere le componenti strutturali dei diversi tipi di sussidi bionici . 
la protesi utilizzata per gli impianti dellorecchio medio , che pu essere fissata allincudine o alla finestra rotonda , il modello vsb ( med - el , innsbruck , austria ) che si compone di una parte esterna , il processore , e di una parte interna , costituita dal ricevitore e dal trasduttore ( vorp : internal vibrating ossicular prosthesis )  . il processore , posto sulla cute del cuoio capelluto , in regione retro - auricolare , contiene un magnete per trasmettere informazioni per induzione elettromagnetica alle parti interne , un microfono per captare i suoni , la batteria e le componenti elettroniche per convertire il segnale acustico in segnale elettrico da trasmettere attraverso la cute . 
il processore ha la funzione di elaborare i suoni mediante programmi adattati al tipo di ipoacusia ; il ricevitore , impiantato sotto la cute , raccoglie il segnale proveniente dal processore e si collega al trasduttore , denominato anche massa vibrante o fmt ( floating mass transducer ) [ 4 , 5 ] , che fissato chirurgicamente allapofisi lunga dellincudine mediante un gancio in titanio e converte tramite un magnete il segnale elettrico in vibrazioni meccaniche che vengono trasmesse alla staffa e quindi alla scala vestibolare . 
tale protesi si rivela efficace nei pazienti affetti da ipoacusia di tipo misto di gravit severa in esiti di otite media cronica , in caso di processi malformativi a carico della catena ossiculare e di otosclerosi fenestrale [ 8 ]  . radiol med ( 2008 ) 113 : 265277 otosclerosis , congenital alterations to the auditory ossicles and severe acquired alterations to the auditory ossicles due to prior reconstructive surgery ( ossiculoplasty )  . in cases in which hypoacusis cannot be treated with a middle ear implant and the cochlear nerve is intact and functioning , the preferred treatment involves a cochlear implant [ 11 , 12 ]  . 
when the anatomical alterations contraindicate the placement of implants in the middle ear or within the cochlea , patients can benefit from a device placed at the brainstem level ( abi ) : the nucleus 24 ( cochlear corp ) device . 
similar to the other implants , with this device , sounds are picked up by a microphone and converted by a transmitter into electrical impulses that directly stimulate the cochlear nucleus through a series of electrodes at the level of the lateral recess of the fourth ventricle . 
the implant consists of 21 platinum microelectrodes , each with a diameter of about 0.7 mm , mounted on a 38.5 - mm silicon support in three rows [ 1315 ]  . 
the implant is suitable for use in patients suffering from severe congenital malformations of the internal ear and the balance and hearing nerves , patients suffering from postinfectious cochlear degeneration ( particularly postmeningitic ) , patients with severe forms of otospongiosis or who have suffered severe trauma causing bilateral fracture of the cochlea , and patients suffering from neurofibromatosis type ii with bilateral involvement of the eighth cranial nerve [ 3 , 16 , 17 ]  . guaranteeing prosthetic device placement at the cochlear nucleus level was not possible in all patients for anatomopathological reasons , particularly in the case of neurofibromatosis type ii . 
in these patients , the use of a similarly constructed abi was proposed , with the difference being that the electrodes were positioned on the dorsal surface of the inferior colliculus . results cochlear implants were studied with conventional radiography ( stenvers projection ) in all 350 patients . 
conventional radiography provided adequate information regarding electrode positioning at the cochlea level , although the examination required accurate assessment and correct identification of anatomical structures adjacent to the prosthetic device , particularly the superior semicircular canal . 
to assess correct prosthetic device placement with plain - film radiography , the vertical line passing through the radiolucency of the superior semicircular canal needs to be presso la divisione otorinolaringoiatrica stata approntata una variante a questa tipologia di impianto : linnovazione consiste in una semplice rimozione del gancio per permettere il posizionamento della massa vibrante a livello della fr . 
lenergia si trasmette in questo modo alla scala timpanica e , vista la comunicazione con la vestibolare a livello dellelicotrema , la stimolazione dellorgano del corti avviene in modo analogo alla tecnica precedente con linversione del movimento dei fluidi ( sonoinversione ) [ 9 , 10 ]  . da questa particolare protesi traggono beneficio i pazienti affetti da gravi forme di otosclerosi , alterazioni congenite a carico della catena ossiculare , e gravi alterazioni acquisite a carico della catena ossiculare da pregressi interventi ricostruttivi di ossiculoplastica . 
 qualora non sia possibile trattare le ipoacusie tramite protesi allorecchio medio ed il nervo cocleare sia integro e funzionante , la soluzione il trattamento con impianto cocleare [ 11 , 12 ]  . 
quando le alterazioni anatomiche sono tali da controindicare il posizionamento di impianti allorecchio medio o allinterno della coclea , i pazienti possono beneficiare di una protesi a livello del tronco encefalico o abi del tipo nucleus 24 ( cochlear corp )  . 
analogamente ai precedenti presidi terapeutici , le onde sonore vengono captate da un microfono e convertite da un trasmettitore in impulsi elettrici che stimolano , attraverso una serie di elettrodi , direttamente i nuclei cocleari a livello del recesso laterale del iv ventricolo . 
la protesi costituita da 21 micro - elettrodi di platino , ciascuno del diametro di circa 0 , 7 mm , montati su un supporto di silicone di 3 per 8 , 5 mm , disposti su tre file [ 1315 ]  . 
trovano indicazione al trattamento con abi i pazienti affetti da gravi malformazioni congenite dellorecchio interno e del pacchetto vestibolo - cocleare , quelli affetti da degenerazione cocleare post - infettiva , in particolare post - meningitica , i pazienti con gravi fenomeni di otospongiosi o che hanno subito gravi traumi che hanno determinato frattura bilaterale della coclea , ed i pazienti affetti da neurofibromatosi di tipo ii con interessamento bilaterale del viii nervo cranico [ 3 , 16 , 17 ]  . per i pazienti in cui per motivi anatomo - patologici non possibile ottenere il sicuro posizionamento a livello dei nuclei cocleari , in particolare nel caso di neurofibromatosi di tipo ii , stato proposto lutilizzo di un impianto abi , di costituzione analoga al precedente ma con gli elettrodi posti in corrispondenza della superficie dorsale del collicolo inferiore . 270 radiol med ( 2008 ) 113 : 265277 traced . 
conventional radiography of the head in ap and ll orthogonal projections , performed after activation of the prosthetic device at about 15 days after surgery , was considered a reference point for radiographic follow - up . 
the procedure was standardised by identifying a connecting line in the ll projection between the posterior clinoid processes and the basion ( tuberculum sella - basion line ) and the basion - opisthion line . 
1a , b impianto cocleare ; gli elettrodi sono posizionati medialmente alla linea verticale passante per il canale semicircolare superiore e quindi tutti inseriti nella coclea ( a ) ; gli elettrodi risultano collocati solo a livello del giro basale ( b )  . risultati la protesi da impianto protesico cocleare stata studiata con rx ( proiezione secondo stenvers ) , in tutti i 350 pazienti , con tc in 10 / 350 , nessuno ha eseguito cbct . 
le indagini radiografiche hanno fornito adeguate informazioni per quanto concerne il posizionamento degli elettrodi a livello della coclea ; tale indagine tuttavia richiede una accurata valutazione e la corretta individuazione delle strutture anatomiche adiacenti alla protesi , in particolare il canale semicircolare superiore . 
si preferito avere come riferimento per i controlli successivi gli angoli piuttosto che la distanza da tali reperi per evitare eventuali errori di valutazione legati allingrandimento o alla riduzione delle dimensioni del radiogramma dovuti alla digitalizzazione dellimmagine . i pazienti trattati con protesi vsb alla fr , che hanno eseguito controllo con rx ( proiezione secondo stenvers ) , sono stati 2 / 17 ; quelli sottoposti a tc sono stati 4 / 17 e 17 / 17 soggetti hanno espletato una indagine cbct . 
angles rather than distances from those landmarks were preferably used as references for follow - up examinations to avoid possible assessment errors linked to radiograph enlargement or reduction due to image digitalisation . only 2 / 17 patients treated with a vsb at the round window were examined with conventional radiography ( stenvers projection ) , whereas 4 / 17 were examined with hrct and 17 / 17 with cbct . 
5 rx del cranio in antero - posteriore in paziente con impianto al tronco : sono stati evidenziati le linee di riferimento e langolo di posizionamento degli elettrodi . radiol med ( 2008 ) 113 : 265277 fig . 
a plain - film radiograph could not be obtained due to the patients refusal to undergo further examinations . there were no cases of postoperative complications . discussione dallanalisi dei risultati ottenuti si evince come ogni paziente , trattato per risolvere la propria ipoacusia mediante apposizione di orecchio bionico , pu trovare adeguata documentazione radiologica ( rx o tccbct ) in base al tipo di protesi installata . 
sono stati sottoposti a doppia indagine solo i pazienti che per primi sono stati trattati presso questa struttura per poter stabilire quale fosse la migliore metodica da impiegare , necessit insorta in quanto si trattava di interventi chirurgici di cui non si poteva disporre di univoci dati in letteratura [ 1826 ]  . 274 radiol med ( 2008 ) 113 : 265277 fig . 
8a - d impianto acustico al collicolo inferiore ( freccia ) : tc in sezione trasversale ( a ) , sagittale ( b ) e coronale ( c )  . 
la ricostruzione ssd identifica meglio la protesi rispetto alladiacente meningioma calcifico ( d )  . radiol med ( 2008 ) 113 : 265277 discussion results analysis revealed how adequate radiological information ( conventional radiography or hrctcbct ) can be obtained for each patient treated for hypoacusis following bionic ear placement on the basis of the prosthetic device implanted . 
this was necessary given the lack of agreement in the literature regarding the relevant surgical procedures [ 1826 ]  . patients treated with vsb with traditional placement on the long limb of the incus provided radiographic and ct images obtained in another centre . 
to date , no similar findings have been reported in the literature . conventional radiography was performed in the ap , ll and stenvers projections only in the first 2 / 17 patients who underwent round window vsb implantation , because the surgical procedure had not been previously performed in any other centre . 
the conventional radiographic examination was immediately abandoned , as it did not guarantee precise information regarding correct device positioning . we therefore felt that the best technique for assessing correct fmt placement was cbct . 
hrct , which was performed on a limited number of patients ( 4 / 17 ) , did not prove to be better than cbct . the first patients ( 10 / 350 ) who received cochlear implants underwent both radiographic and hrct examination to confirm the correct electrode position within the cochlear turns . 
the following 340 / 350 patients treated with the cochlear implant were examined with a radiograph in the stenvers projection alone , in agreement with the literature [ 11 ]  . 
given the results obtained with cbct for implants on the round window , it is hoped that cbct will provide adequate information ( similar to hrct ) in the follow - up of cochlear implants , as dalchow et al . 
indeed , cbct guarantees adequate information for correct diagnosis , with the advantage of administering a radiation dose 60% lower than conventional ct [ 2528 ]  . the need to perform hrct in patients who have undergone brainstem implantation arises solely from the presence of a postoperative protocol . 
the examination does , however , guarantee exact localisation of the prosthetic device at the brainstem level , such that subsequent follow - up can comprise conventional radiography alone . in the only patient treated with implantation at the inferii pazienti trattati con impianto elettromagnetico di tipo vsb con tradizionale innesto sullapofisi lunga dellincudine hanno prodotto documentazione radiografica e tc espletata in altra sede , presentandosi alla nostra attenzione in virt di un nuovo deficit uditivo allorecchio trattato : tutti questi pazienti sono stati quindi sottoposti ad indagine cbct . 
dallanalisi degli esami radiologici tradizionali effettuati stato confermato come tale metodica non sia in grado di fornire le informazioni richieste ; queste ultime , per contro , sono state correttamente ottenute mediante cbct : ad oggi non esiste analoga esperienza in letteratura . le indagini radiografiche ap , ll e stenvers sono state eseguite solo sui primi 2 / 17 pazienti operati per protesi vsb posizionate a livello della finestra rotonda , poich tale tipo di intervento non era mai stato eseguito in nessuna altra struttura . 
lindagine radiografica stata immediatamente abbandonata in quanto non garantiva informazioni sicure sul corretto posizionamento ; pertanto riteniamo che la metodica migliore per verificare il corretto posizionamento della massa vibrante sia la cbct . 
la tc , eseguita su un numero esiguo di pazienti ( 4 / 17 ) , non si dimostrata superiore alla cbct . i primi pazienti ( 10 / 350 ) sottoposti ad impianto di protesi cocleare hanno eseguito , oltre allindagine radiografica , anche la indagine tc per confermare la corretta posizione degli elettrodi allinterno dei giri cocleari ; tale indagine stata effettuata essenzialmente per verificare la concordanza delle informazioni offerte dalle due metodiche . 
i pazienti ( 340 / 350 ) successivamente trattati mediante tale protesi , sono stati esaminati unicamente con radiogramma con proiezione secondo stenvers in accordo con la letteratura [ 11 ]  . 
auspicabile , visti i risultati con la cbct per gli impianti protesici alla finestra rotonda che la cbct possa fornire adeguate informazioni ( analogamente alla tc ) anche nel controllo di tali impianti protesici , come peraltro suggerito da dalchow et al . 
 [ 25 , 26 ] ; la cbct , infatti , garantisce informazioni adeguate per la corretta diagnosi con il vantaggio di somministrare una dose radiante inferiore di circa il 60% rispetto alla tc convenzionale [ 2528 ]  . la necessit di espletare una indagine tc in pazienti operati di impianto al tronco nasce solo dalla presenza di un protocollo post - chirurgico ; tale indagine tuttavia garantisce lesatta collocazione della protesi a livello del tronco encefalico , per la quale pu essere programmato un followup con la sola radiologia convenzionale . nellunico paziente trattato con impianto al collicolo inferiore , la tc postoperatoria , completata con ricostruzioni multiplanari e 3d si rivelata necessaria anche per meglio valutare il corretto posizionamento degli elettrodi a livello della lamina quadrigemina . 
nonostante non sia disponibile per questo caso documentazione radiografica , si ritiene , sulla scorta dellesperienza acquisita con gli impianti al 276 radiol med ( 2008 ) 113 : 265277 or colliculus , the postoperative hrct , complete with mpr and 3d , proved necessary to better assess electrode positioning at the quadrigeminal plate level . 
even though there was no radiographic documentation for this case , it was thought that on the basis of the experience gained in relation to brainstem implants , calculation of the angles formed by the intersection of codified lines in the ap and ll radiographs is the correct methodology for follow - up of this procedure . conclusions hrct is the gold standard in bionic ear imaging . 
in the case of cochlear implants , conventional radiography alone ( stenvers projection ) leads to lower doses of ionising radiation in these often young patients while providing adequate diagnostic information . 
however , the possible structural alterations of the cochlea following implantation ( cochlear ossification , which can englobe the electrodes without dislodging them ) may not be visualised radiographically , thus calling for hrct examination . conventional radiography ( ap and ll projections ) , after the required postoperative hrct examination , can be considered the technique that guarantees correct follow - up of brainstem and inferior colliculus implantations . 
cbct , for vsb inserted at the incus or the round window , guarantees adequate information for correct prosthetic device location , with the advantage of administering a lower radiation dose than hrct , such that where the technique is available , it should be used as the main technique for this application . tronco , che il calcolo degli angoli formati dallintersezione di linee codificate nei radiogrammi in antero - posteriore e latero - laterale , sia la giusta metodologia per il follow - up della protesi . conclusioni lindagine tc rappresenta al momento attuale il gold standard nellimaging dellorecchio bionico . 
nel caso di impianti cocleari la sola radiologia convenzionale ( proiezione secondo stenvers ) ha consentito di somministrare minor dose di radiazioni ionizzanti a questi pazienti , sovente di giovane et , con riscontro di adeguate informazioni diagnostiche ; le eventuali alterazioni strutturali della coclea successive allimpianto ( fenomeni di ossificazione cocleare che possono inglobare senza dislocare gli elettrodi ) possono non essere visualizzate radiograficamente e necessitano pertanto di valutazione tc . la radiologia convenzionale ( proiezioni antero - posteriore e latero - laterale ) rappresenta , dopo il previsto necessario controllo tc post - chirurgico , la metodica che garantisce il corretto follow - up degli impianti protesici al tronco ed al collicolo inferiore . 
ardissino2 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , holland 3dibimel , sezione di scienze radiologiche , universit di palermo , parma , italy 4dipartimento di radiologia , universit degli studi di verona , verona , italy 5dipartimento di emergenza , azienda ospedaliero - universitaria di parma , parma , italy correspondence to : f . 
cademartiri , viale rustici 2 , 43100 parma , italy , tel . : + 39 - 052 - 1961833 , e - mail : filippocademartiri@hotmail.com received : 9 january 2007 / accepted : 19 april 2007 / published online : 28 march 2008 springer - verlag 2008 abstract purpose . 
for the ctca scan ( sensation 64 , siemens , germany ) , we administered an iv bolus of 100 ml of iodinated contrast material ( iomeprol 400 mgi / ml , bracco , italy )  . 
valutare laccuratezza diagnostica dellangiografia coronarica non invasiva con tomografia computerizzata ( ct - ca ) a 64 strati nellindividuazione delle stenosi coronariche significative ( riduzione del lume coronarico ( cid : 2 ) 50% ) basando la valutazione sulla refertazione clinica . 
dal database della ct - ca sono stati arruolati nello studio 145 pazienti ( 92 maschi , 52 femmine , et media 63 , 410 , 2 anni ) con sospetta malattia coronarica . 
per la scansione ct - ca ( sensation 64 , siemens , germania ) sono stati iniettati endovena 100 ml di mezzo di contrasto . ( iomeprol 400 mgi / ml , bracco , italia )  . 
sensibilit , specificit , valore predittivo positivo e negativo della ct - ca nella determinazione delle stenosi significative utilizzando unanalisi per segmento , per vaso e per paziente sono risultate del 75 , 6% , 85 , 1% , 97 , 6% ; 86 , 9% , 164 radiol med ( 2008 ) 113 : 163180 minimal presence of coronary calcification improved diagnostic accuracy . 
the excellent negative predictive value and negative likelihood ratio make ctca a noninvasive gold standard for exclusion of significant coronary artery disease . keywords multislice computed tomography conventional coronary angiography coronary artery disease 81 , 8% , 58 , 0% ; 48 , 2% , 68 , 1% , 79 , 6% ; e 95 , 7% , 92 , 3% , 93 , 5% , rispettivamente . 
i valori ottimali di valore predittivo negativo e likelihood ratio negativo collocano la ct - ca tra le metodiche non invasive gold standard per lesclusione di malattia coronarica critica . parole chiave tomografia computerizzata multistrato angiografia coronarica convenzionale malattia aterosclerotica coronarica introduction introduzione computed tomography coronary angiography ( ctca ) is progressively entering clinical practice for the diagnosis of obstructive coronary disease [ 17 ]  . 
in particular , the patient population enrolled in most cases was composed of patients with suspected or known coronary artery disease who were already candidates for conventional coronary angiography ( ca )  . 
in fact , patients enrolled in these studies were often characterised by stable angina and therefore by a high prevalence of disease [ 317 ]  . nonetheless , the current guidelines and international panels recommend the use of ctca in lowto medium - risk patients with nondiagnostic stress tests or unable to exercise [ 1820 ]  . before extending the clinical use of ctca to these patient populations , the technique needs to be validated in different clinical contexts from those characterising classical studies . 
evaluation times are reduced , and the operators capable of evaluating ctca studies are few and pressured by the other activities and needs of diagnostic radiology . this study aimed to compare the diagnostic performance of ctca with ca in the detection of coronary artery stenola coronarografia mediante tomografia computerizzata ( ct - ca ) sta progressivamente entrando nella pratica clinica per la diagnosi di malattia coronarica ostruttiva [ 17 ]  . gli studi che fino ad ora hanno dimostrato laccuratezza diagnostica della ct - ca a 64 strati hanno utilizzato metodologie atte alla validazione [ 317 ]  . 
questo approccio permette una adeguata validazione della metodica ma non consente di estrapolare completamente al contesto clinico i risultati . le popolazioni arruolate in questi studi , infatti , erano spesso caratterizzate da angina stabile e quindi da elevata prevalenza di malattia [ 317 ]  . 
tuttavia , le correnti linee guida ed i panel internazionali raccomandano lutilizzo della ctca in popolazioni di pazienti a rischio basso - intermedio con test provocativi dubbi o non eseguibili [ 1820 ]  . prima di poter estendere a queste popolazioni lutilizzo clinico della ct - ca serve poter validare la metodica in contesti clinici differenti da quelli che caratterizzano gli studi classici . 
i tempi di valutazione dellesame sono ridotti e gli operatori in grado di valutare le indagini ct - ca sono pochi e pressati dalle altre attivit di una diagnostica radiologica con molteplici esigenze . questo studio volto a confrontare la performance diaradiol med ( 2008 ) 113 : 163180 sis by comparing the clinical findings of the two techniques in a hospital where ctca has already been implemented . gnostica della ct - ca rispetto alla cag nella rilevazione di stenosi coronariche confrontando i referti clinici delle due metodiche in un ospedale dove questa metodica gi stata implementata . materials and methods patient population between january 2005 and june 2005 , 145 patients ( 92 men , 52 women , mean age 63.410.2 years ) with suspected coronary artery disease ( atypical chest pain and stable angina pectoris ) who had undergone both ctca and ca were enrolled for the study . 
patients with acute coronary syndrome and those with absolute contraindications for the intravenous administration of iodinated contrast material ( known allergy , kidney failure or thyroid disorder ) were excluded . the ethics committee of our centre approved the study protocol , and all patients gave informed consent . patient preparation patients with a heart rate ( hr ) greater than 65 beats per minute ( bpm ) and without specific contraindications received a 5 - mg intravenous dose of beta - blockers ( atenolol , tenormin , astrazeneca )  . 
in addition , in the absence of contraindications , patients received a 5 - mg sublingual dose of nitrate ( isosorbide dinitrate , carvasin , wyeth lederle )  . ctca scan protocol and image reconstruction the ct study was performed with a 64 - slice scanner ( sensation 64 , siemens , forchheim , germany ) [ 4 , 5 ]  . 
number of slices per rotation 322 , gantry rotation time 330 ms , feed / rotation 6 mm ( pitch 0.2 ) , voltage 120 kv , current 150 mas . 
the images were reconstructed with the following parameters : effective slice thickness 3 mm , reconstruction increment 1.5 mm , field of view ( fov ) 150180 mm , convolution kernel for the calcium score . the time windows were positioned at 350 ms of the subsequent r wave b . 
number of slices per rotation 322 , slice thickness 0.6 mm , gantry rotation time 330 ms , feed / rotation 3.84 mm ( pitch 0.2 ) , voltage 120 kv , current 850950 mas , effective slice thickness 0.60.75 mm , reconstruction increment 0.4 mm , fov 150180 mm , medium - smooth convolution kernel . 
prospective modulation of the x - ray tube was not used . materiali e metodi popolazione esaminata da gennaio 2005 a giugno 2005 , 145 pazienti ( 92 maschi , 52 femmine , et media 63 , 410 , 2 anni ) con sospetta malattia coronarica ( dolore toracico atipico e angina pectoris stabile ) che hanno eseguito sia la ct - ca , sia la cag sono stati arruolati per lo studio . 
solo i pazienti con ritmo sinusale , mai sottoposti ad angioplastica percutanea o ad intervento chirurgico per il posizionamento di by - pass e capaci di trattenere il respiro per almeno 12 s , sono stati inclusi nello studio . 
il comitato etico della nostra istituzione ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . preparazione del paziente ai pazienti con una frequenza cardiaca ( fc ) superiore a 65 battiti per minuto ( bpm ) e senza specifiche controindicazioni stata somministrata per via endovenosa una fiala di beta - bloccante ( atenololo , tenormin , astrazeneca ) da 5 mg . inoltre , in assenza di contro indicazioni , pochi minuti prima della scansione stato somministrato del nitrato sublinguale ( isosorbide dinitrato , carvasin 5mg , wyeth lederle )  . 
 protocollo di scansione ct - ca e ricostruzione delle immagini per lo studio mediante tc stato utilizzato uno scanner a 64 strati ( sensation 64 , siemens , forchheim , germania ) [ 4 , 5 ]  . 
numero di strati per rotazione 32 2 , tempo di rotazione del gantry 330 ms , avanzamento / rotazione 6 mm ( pitch 0 , 2 ) , voltaggio del tubo radiogeno kv 120 , potenza del tubo radiogeno mas 150 . 
le immagini sono state ricostruite con i seguenti parametri : spessore di strato ef166 radiol med ( 2008 ) 113 : 163180 a dedicated software package ( windose , medical physics institute , erlangen , germany ) was used to calculate radiation dose to patients during the angiographic scan ( mean value 15.2 msv for women and 21.4 msv for men ) [ 7 ]  . 
a dose of 80100 ml of iodinated contrast material ( iomeprol , iomeron 400 , bracco , milan ) was administered at a speed of 45 ml / s with a power injector ( stellant , medrad , pittsburgh , pa , usa ) attached to an 18to 20gauge needle cannula positioned in an antecubital vein [ 5 ]  . with the aim of optimising coronary artery enhancement , the bolus tracking technique ( care bolus , siemens , forchheim , germany ) was used to synchronise the arrival of contrast material in the coronary arteries with the beginning of the scan [ 5 , 21 ]  . 
the angiography scan data were obtained during a single breath - hold of 1012 s . retrospective reconstructions were performed based on the electrocardiogram ( ecg ) signal to obtain an image quality unaffected by motion artefacts . 
the time windows used were the midand end - diastolic phases ( from 300 to 450 ms before the subsequent r wave and / or from 60% to 70% of the r - r interval )  . 
the segments were classified as not significantly stenotic ( normal or with wall irregularities or noncritical stenosis < 70% ) or significantly stenotic ( stenosis ( cid : 2 ) 70% ) using the conventional classifications and guidelines . 
the operator assessed coronary stenoses during the angiographic session in the projection of maximal stenosis by visual evaluation . ctca image assessment all ctca scans were analysed by an observer with 5 years of experience in the field and who was unaware of the ca findings . 
all conventional visualisation modalities were used by the operator [ axial , multiplanar images ( mpi ) , curved multiplanar images ( cmpi ) , volume rendering ( vr ) ]  . 
the segments were classified as not significantly fettivo 3 mm , incremento di ricostruzione 1 , 5 mm , campo di vista ( fov ) 150 - 180 mm , filtro di convoluzione dedicato per il calcium score . 
numero di strati per rotazione 32 2 , spessore di strato 0 , 6 mm , tempo di rotazione 330 ms , avanzamento per rotazione 3 , 84 mm ( pitch 0 , 2 ) , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 850950 mas , spessore di strato effettivo ricostruito 0 , 60 , 75 mm , incremento di ricostruzione 0 , 4 mm , campo di vista ( fov ) 150180 mm , filtro di convoluzione medium - smooth . 
non stata utilizzata la modulazione prospettica del tubo radiogeno . utilizzando un software dedicato ( windose , istituto di fisica medica , erlangen , germania ) stata calcolata la dose di radiazioni ionizzanti alla quale i pazienti sono stati esposti durante la scansione angiografica ( valore medio 15 , 2 msv per le donne e 21 , 4 msv per gli uomini ) [ 7 ]  . 
sono stati somministrati 80100 ml di mezzo di contrasto iodato ( iomeprol , iomeron 400 , bracco , milano ) alla velocit di 45 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 1820 gauge preventivamente posizionata in una vena antecubitale [ 5 ]  . 
allo scopo di ottimizzare lopacizzazione dei vasi arteriosi coronarici stata utilizzata la tecnica del bolustracking ( care bolus , siemens , forchheim , germania ) per sincronizzare larrivo del mezzo di contrasto nelle arterie coronarie con linizio della scansione [ 5 , 21 ]  . 
le finestre temporali utilizzate sono state la fase mesoe telediastolica ( da 300 a 450 ms prima della successiva onda r e / o dal 60% al 70% dellintervallo r - r )  . 
quando ritenuto necessario ( ad esempio in caso di persistente movimento cardiaco residuo che riduce la qualit diagnostica dellimmagine ) sono state analizzate altre ricostruzioni in differenti finestre temporali di ricostruzioni del ciclo cardiaco , generalmente dal 25% al 35% dellintervallo r - r ( oppure + 225 ms , + 275 ms , e + 325 ms dopo la precedente onda r )  . 
lalgoritmo di ricostruzione utilizzato preleva i dati derivanti da un singolo battito cardiaco ottenuto durante met rotazione del tubo radiogeno . coronarografia convenzionale ( cag ) la cag stata eseguita entro 2 settimane dalla ct - ca con tecnica convenzionale . 
loperatore ha identificato i segmenti coronarici utilizzando una classificazione in 17 segmenti modificata da radiol med ( 2008 ) 113 : 163180 stenotic ( normal or with wall irregularities or noncritical stenosis < 50% ) or significantly stenotic ( stenosis ( cid : 2 ) 50% ) using the commonly applied classifications [ 3 , 6 , 7 ]  . statistical analysis the diagnostic performance of ctca was assessed by comparing reports stored in the information retrieval system of our centre for ctca and ca , respectively . 
mean reporting time for ctca was 15 min and for ca 10 min . lesions were considered significant if lumen occlusion was ( cid : 2 ) 50% for ctca and ( cid : 2 ) 70% for ca . 
diagnostic accuracy was therefore calculated as sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) , with 95% confidence intervals ( ci ) calculated with binomial expansion . 
lr + corresponds to sensitivity divided by 1 specificity , whereas lr corresponds to 1 sensitivity divided by specificity . comparison between ctca and ca was performed per segment , per vessel and per patient . 
values were calculated on the entire population ( group a : 134 patients ) and for the subpopulations with hr < 70 bpm ( group b : 107 patients ) , hr < 65 bpm ( group c : 89 patients ) and hr < 70 bpm and agatston coronary artery calcium score ( cascore ) ( cid : 3 ) 10 ( group d : 41 patients )  . 
statistical analyses were performed with a dedicated software package ( statistical package for the social sciences , version 11.5 , spss , chicago , il , usa )  . results eleven of 145 ( 11.6% ) patients were excluded from the analysis due to poor scan quality . 
about one fifth of patients had single - vessel disease ( 22.1% , 32 / 145 ) , a little more than one sixth had three - vessel disease ( 17.9% , 26 / 145 ) and about one third had multivessel disease ( 35.9% , 52 / 145 )  . cascore proved to be intermediate , with a wide degree of variability [ meanstandard deviation ( sd ) 235.3392.8 , range 02 , 265 ] , thus reflecting a heterogeneous population with an intermediate to high prevalence of coronary artery disease ( 63% in the per - patient analysis )  . the diagnostic accuracy of ctca in identifying significant lesions on a per - segment , per - vessel and per - patient baquella fornita dallamerican heart association [ 22 ]  . 
i segmenti sono stati classificati come non significativamente stenotici ( normali o con irregolarit della parete o con stenosi non critica < 70% ) o significativamente stenotici ( stenosi critica ( cid : 2 ) 70% ) , utilizzando le classificazioni convenzionali e linee guida . 
le stenosi coronariche sono state valutate dalloperatore durante la seduta angiografica nella proiezione di massima stenosi mediante valutazione visiva . valutazione dellimmagine di ct - ca tutte le ct - ca scansioni sono state analizzate da un osservatore con 5 anni di esperienza nel settore non a conoscenza dei risultati della cag . 
i segmenti sono stati classificati come non significativamente stenotici ( normali o con irregolarit della parete o con stenosi non critica < 50% ) o significativamente stenotici ( stenosi critica ( cid : 2 ) 50% ) , utilizzando le classificazioni comunemente applicate [ 3 , 6 , 7 ]  . analisi statistica la performance diagnostica della ct - ca stata valutata confrontando i referti archiviati nel sistema informatico dellospedale per la ct - ca e per la cag , rispettivamente . detti referti sono stati stilati immediatamente dopo le procedure . 
per la ct - ca il tempo medio di refertazione stato di 15 min mentre per la cag stato di 10 min . le lesioni sono state considerate significative se ( cid : 2 ) 50% per la ct - ca e se ( cid : 2 ) 70% per la cag . 
sono stati inoltre calcolati la prevalenza di malattia , ed i likelihood ratio positivo e negativo ( lr + e lr , rispettivamente ) con intervalli di confidenza del 95% per ogni sotto - analisi . 
il lr + corrisponde alla sensibilit diviso 1 - specificit , mentre il lr corrisponde a 1 - sensibilit diviso la specificit . il confronto tra ct - ca e cag stata eseguita per - segmento , per - vaso e per - paziente . 
i valori sono stati calcolati su tutta la popolazione ( gruppo a , 134 pazienti ) e per le sotto - popolazioni con : frequenza cardiaca < 70 bpm ( gruppo b , 107 pazienti ) , frequenza cardiaca < 65 bpm ( gruppo c , 89 pazienti ) ; frequenza cardiaca < 70 bpm e cascore ( cid : 3 ) 10 ( gruppo d , 41 pazienti )  . 
circa un quinto dei pazienti aveva malattia monovasale ( 22 , 1% ; 32 / 145 ) , poco pi di un sesto aveva malattia trivasale ( 17 , 9% ; 26 / 145 ) e circa un terzo dei pazienti ( 35 , 9% ; 52 / 145 ) aveva malattia multivasale . il calcium score coronarico secondo agatston risultato intermedio con ampia variabilit ( mediads , 235 , 3392 , 8 ; range = 02265 ) , rispecchiando una popolazione eterogenea ed prevalenza di malattia coronarica medio - alta nella popolazione ( 63% nellanalisi per paziente )  . 
 laccuratezza diagnostica della ct - ca nellindividuazione delle lesioni significative con valutazione per - segmento , per - vaso e per - paziente mostrata in tabella 3 e nella fig . 
la ct - ca ha generato 183 falsi positivi e 55 falsi negativi . questo ha determinato dei valori di accuratezza diagnostica inferiori rispetto a quelli documentati in letteratura ( sensibilit 76% e specificit 87% )  . 
 235 , 3392 , 8 ( 02265 ) valutazione per vaso ds , deviazione standard ; m / f , rapporto maschi / femmine ; bmi , body mass index sis is summarised in table 3 and fig . 
the diagnostic accuracy values are lower than those reported in recent validation studies [ 7 , 1315 , 17 ]  . sono stati inclusi nella valutazione 536 vasi coronarici . di questi , 168 ( 31 , 3% ) avevano stenosi critiche alla cag . la ct - ca ha generato 67 falsi positivi e 25 falsi negativi . questo ha determinato dei valori di accuratezza diagnostica migliori rispetto alla valutazione per segmento ( sensibilit 85 , 1% e specificit 81 , 8% )  . 
dei 4 vasi valutati il tronco radiol med ( 2008 ) 113 : 163180 table 2 distribution of coronary atherosclerotic disease in the patients enrolled for the coronary angiography study comune sinistro ha mostrato i migliori valori di accuratezza diagnostica ( sensibilit 100% e specificit 97 , 7% )  . disease extension absence of disease or nonsignificant disease ( % ) single - vessel disease ( % ) two - vessel disease ( % ) three - vessel disease ( % ) multivessel disease ( % ) total tabella 2 distribuzione della malattia aterosclerotica coronarica nei pazienti arruolati per lo studio alla cag entit della malattia assenza di malattia o malattia non significativa ( % ) malattia ad interessamento monovasale ( % ) malattia ad interessamento bivasale ( % ) malattia ad interessamento trivasale ( % ) malattia ad interessamento multivasale ( % ) totale total 61 ( 42.1 ) 32 ( 22.1 ) 23 ( 15.9 ) 26 ( 17.9 ) 52 ( 35.9 ) totale 61 ( 42 , 1 ) 32 ( 22 , 1 ) 23 ( 15 , 9 ) 26 ( 17 , 9 ) 52 ( 35 , 9 ) assessment per segment comparison with ca was performed on 1 , 621 segments ( 12 segments per patient )  . 
this led to diagnostic accuracy values being lower than those reported in the literature ( sensitivity 76% and specificity 87% )  . assessment per vessel the assessment included 536 coronary arteries . 
in una popolazione come quella analizzata caratterizzata da alta prevalenza complessiva per paziente ( 62% ) , lanalisi per segmento riduce notevolmente la prevalenza di segmenti con stenosi significative fino ad invertire completamente il rapporto tra positivo e negativo . 
questo determina una perdita in termini di lr + ( 2 , 32 ) , mentre diventa estremamente valido il risultato in termini di lr ( 0 , 041 )  . nelle sotto - popolazioni a bassa frequenza cardiaca 170 radiol med ( 2008 ) 113 : 163180 table 3 diagnostic accuracy of 64 - slice computed tomography in the assessment of coronary stenosis no . 
a patient with anomalous origin of the circumflex artery ( cx ) ( from the right coronary sinus with a retroaortic course ) and significant stenosis on ct at the proximal lad ( a , b arrowhead )  . 
un paziente con anomalia di origine della coronaria circonflessa ( dal seno coronarico di destra ed a decorso retro - aortico ) e stenosi significativa alla tc al tratto prossimale della discendente anteriore ( a , b , testa di freccia )  . 
la lesione mostra caratteristiche peculiari alla tc , ossia : assenza di evidenti calcificazioni e presenza di rimodellamento vascolare positivo ( b , riquadro ; c )  . la coronarografia convenzionale eseguita in seguito ( d ) , ha confermato la presenza ed entit della lesione che stata trattata mediante angioplastica e stenting ( e )  . radiol med ( 2008 ) 113 : 163180 fig . 
nellesempio si osserva tc di una coronaria destra che losservatore ha interpretato come lesione breve con calcificazione nodulare < 50% per la presenza di artefatti da movimento residuo ( a - c )  . 
la coronarografia convenzionale eseguita in seguito ha mostrato una lesione critica nello stesso segmento ( d ) , che stata trattata mediante angioplastica percutanea e stenting ( e )  . hr < 70 bpm or < 65 bpan analysis of diagnostic accuracy only in patients with hr < 70 bpm and with cascore ( cid : 3 ) 10 revealed an increase in all parameters . prevalence of disease and likelihood ratio the prevalence of disease in each subgroup was calculated to demonstrate how this parameter is substantially modified in a per - segment , per - vessel and per - patient analysis . 
in a population such as the one analysed , characterised by a high overall prevalence per patient ( 62% ) , the per - segment analysis noticeably reduces the prevalence of segments with significant stenosis to the point of completely inverting the relationship between positive and negative . 
i tempi di valutazione della ct - ca vengono raramente riportati ed in genere sono liberi e svincolati dal contesto clinico nel quale le prestazioni ( anche differenti dalla ct - ca ) sono numerose e necessitano di risposte rapide . 
i pazienti arruolati per gli studi erano in genere pazienti gi candidati alla cag che per motivi di studio venivano condotti alla ct - ca . in alcune indicazioni e raccomandazioni preliminari allutilizzo clinico della ct - ca , tuttavia , stanno emergendo concetti lievemente discrepanti rispetto alle evidenze della letteratura . 
infatti , sia nelle recenti linee guida della societ europea di cardiologia [ 18 ] , sia in un recente documento di consenso sullappropriatezza delle indicazioni della cardio - tc e cardio - rm [ 19 ] , viene suggerito che un utilizzo congruo della metodica sarebbe nei casi in cui il paziente sia a rischio basso - intermedio ed i test provocativi siano dubbi , non fattibili o inconclusivi . allo stato attuale nessuno studio riporta la reale accuratezza diagnostica estrapolata da un contesto clinico . questa consiste della effettiva performance della metodica sul campo . 
in these studies , the validation context is characterised by the evaluation of ctca with at least two observers and the assessment of ca using a quantitative software package [ i.e. 
ctca evaluation times are rarely reported and are generally free from constraints of the clinical context in which numerous examinations ( and not only ctca ) are performed , all of which require rapid responses . 
stenosis in these studies is usually defined as a ( cid : 2 ) 50% reduction in the lumen for both ctca and ca , and the subjects enrolled are in general already candidates for ca who for research reasons are also studied by ctca . in several preliminary indications and recommendations for the clinical use of ctca , however , a number of slight discrepancies are emerging with respect to the evidence presented in the literature . 
in fact , both the recent european society of cardiology guidelines [ 18 ] and a recent consensus document on the appropriateness of the indications for cardiac ct and cardiac magnetic resonance imaging ( mri ) [ 19 ] suggest that an appropriate use of the technique is in cases where the patient is at lowto medium risk and the stress tests are doubtful , unfeasible or inconclusive . to date , no study has reported the real diagnostic accuracy extrapolated from a clinical setting , which would indicate the effective performance of the technique in the field . 
in this study , we have tried to express this performance by comparing the clinical reports of ctca and ca in a cardiovascular imaging department that performs ctca for clinical purposes . 
this study reports the results of the first 6 months of implementation . the results of our study show diagnostic accuracy values in the assessment per segment and per vessel lower than those of the best validation studies [ 6 , 7 , 1215 , 17 ]  . 
this change in values can be explained as follows . in the clinical setting , ctca is used as a gatekeeper for ca . the operator should therefore be inclined to reason in terms of patients rather than segments or vessels . 
in addition , in no case can the decision to treat a lesion , or which of the lesions to treat , be based solely on the information obtained from ctca . 
questo studio riporta i risultati dei primi sei mesi di implementazione . i risultati del nostro studio mostrano dei valori di accuratezza diagnostica nella valutazione per segmento e per vaso inferiori a quelli dei migliori studi di validazione [ 6 , 7 , 1215 , 17 ]  . 
inoltre , in nessun caso la decisione di trattare una lesione o quale delle lesioni presenti debba essere trattata pu essere basata unicamente sulle informazioni derivanti dalla ct - ca . 
questo approccio determina una progressiva perdita di specificit . basandosi sui dati per paziente dello studio , si osserva come 21 ( 15 , 5% ) pazienti siano stati inviati a cag che poi ha dimostrato lassenza di stenosi critiche . 
di questi uno aveva una stenosi singola su arteria circonflessa prossimale di piccolo calibro ( 2 mm ) e severamente calcifica e laltro aveva una frequenza cardiaca di 83 bpm . dallosservazione della popolazione con frequenza cardiaca < 70 bpm o < 65 bpm non si evidenziano significative modificazioni dei valori di accuratezza diagnostica . 
5a - d nelle sezioni a e b sono mostrati i valori raggruppati per livello di analisi ( segmento , 1 ; vaso , 2 ; paziente , 3 ) , mentre nelle sezioni c e d sono raggruppati per sotto - gruppo analizzato ( gruppi ad vedi legenda ; criteri : frequenza cardiaca e calcio coronarico )  . 
an analysis of the per - patient data in the study reveals that 21 ( 15.5% ) patients were studied by ca , which then revealed the absence of critical stenosis . 
one of these had a single , small - calibre and severely calcified stenosis of the proximal circumflex artery ( 2 mm ) and the other an hr of 83 bpm . analysis of the patient group with an hr < 70 bpm or < 65 bpm did not reveal significant changes in the diagnostic accuracy values . 
the lr + tells us how much the odds of disease increase when the test is positive , whereas the lr tells us how much the odds of disease decrease when the test is negative . 
in pratica , la tc delle coronarie nel mondo reale conferma la sua elevatissima performance quando viene utilizzata per escludere la malattia coronarica mentre non ancora da considerare al pari del gold standard ( i.e. cag ) quando si tratta di confermare una diagnosi di malattia coronarica critica . table 4 diagnostic accuracy in the subpopulation who underwent ecg stress test , computed tomography coronary angiography ( ctca ) and conventional coronary angiography ( ca ) diagnostic accuracy ( 75 patients ) cardiac stress test radiol med ( 2008 ) 113 : 163180 for the diagnostic accuracy of ctca , the same criteria were used as for table 3 . 
vp , veri positivi ; vn , veri negativi ; fp , falsi positivi ; fn , falsi negativi ; vpp , valore predittivo positivo ; vpn , valore predittivo negativo nary calcium parameters . 
in practice , ctca in the real world confirms its high performance when it is used to exclude coronary disease , whereas it still cannot be considered on the same level as the gold standard ( ca ) with regard to confirming a diagnosis of critical coronary disease . the study presented is innovative in that it describes the real performance of 64 - slice ctca in a clinical setting where patients are not necessarily enrolled for ca . 
in this context , ctca findings determine the next diagnostic step lo studio presentato innovativo nella misura in cui descrive la performance reale della ct - ca a 64 strati in un ambiente clinico dove i pazienti non sono necessariamente arruolati per la cag . 
in questo senso il presente studio il primo che possa definirsi di accuratezza diagnostica clinica . qualche breve considerazione pu essere fatta anche sulla prova da sforzo che nella popolazione studiata avrebbe consentito di identificare come pazienti candidati alla cag solo il 16% , nel restante 84% dei casi il risultato negativo o dubbio avrebbe fermato liter diagnostico o necessitato di ulteriori approfondimenti mediante altre tecniche atte dimostrare lischemia . 
in this sense , the study is the first that can be defined as providing clinical diagnostic accuracy . a few remarks should also be made regarding the cardiac stress test , which in the studied population would have identified ca candidates in only 16% of patients . 
the negative or doubtful result in the remaining 84% of patients would have halted the diagnostic course or required further studies with other techniques capable of demonstrating ischaemia . the findings of the preliminary subanalysis of the 75 patients who underwent the cardiac stress test are even more interesting . 
with a prevalence of disease at 51% , sensitivity , specificity , ppv and npv for the cardiac stress test and ctca were 16% and 95% , 60% and 68% , 29% and 75% , 41% and 93% , respectively . limitations a limitation of the study is that patients were enrolled on the basis of availability in the clinical database of ctca and ca reports for the same patient . 
this is due to the still widespread perception that ctca can be used to assess patients with suspected ischaemic coronary artery disease immediately prior to ca . however , even the validation studies published to date enrolled patients who were already candidates for ca and therefore characterised by a high pre - test likelihood of disease . 
indeed , it will become less and less ethical to send patients to ca if their ctca is completely negative . the estimated radiation dose during ctca ( 15.221.4 msv ) is higher than the dose for ca . 
devices equipped with higher temporal resolution [ dual - source ct ( dsct ) 83 ms ] can improve clinical results in patients with medium to low hr and allow the examination to be extended to patients with a higher and irregular hr [ 2629 ]  . tata la sotto - analisi preliminare nei 75 pazienti che hanno effettuato la prova da sforzo . 
con una prevalenza di malattia del 51% , sensibilit , specificit , valore predittivo positivo e negativo sono risultate : 16% e 95% , 60% e 68% , 29% e 75% , 41% e 93% , per la prova da sforzo e per la ct - ca , rispettivamente . limitazioni una limitazione dello studio che il criterio di arruolamento si basava sulla disponibilit nel database clinico dellistituzione della ct - ca e della cag per lo stesso paziente . 
tuttavia , anche gli studi di validazione fino ad ora pubblicati hanno arruolato popolazioni di pazienti gi candidati a cag e quindi caratterizzati da una probabilit pre - test elevata . 
diventer infatti sempre meno etico inviare a cag un paziente con ct - ca completamente negativa . la dose di radiazioni stimata durante lac - tc ( 15 , 221 , 4 msv ) superiore a quella di una cag . 
apparecchiature dotate di maggiore risoluzione temporale ( dual - source ct , dsct ; 83 ms ) potranno migliorare i risultati clinici nei pazienti a frequenza medio - bassa e consentire di estendere lindagine a pazienti con frequenza cardiaca superiore ed irregolare [ 2629 ]  . conclusioni conclusions ctca with a 64 - slice device has good diagnostic accuracy even in a purely clinical context . 
in addition , the diagnostic accuracy of ctca shows significantly higher values than the diagnostic accuracy of the cardiac stress test in the real world . la ct - ca mediante apparecchiature a 64 strati mantiene una buona accuratezza diagnostica anche in contesto puramente clinico . 
salvatore dipartimento di scienze biomorfologiche e funzionali ( dsbmf ) , universit degli studi di napoli federico ii ( unina ) , istituto di biostrutture e bioimmagini ( ibb ) , consiglio nazionale delle ricerche ( cnr ) , napoli , italy correspondence to : o . 
caleo , via adige 40 , 84091 battipaglia ( sa ) , italy , tel . : + 39 - 081 - 7463560 , + 39 - 339 - 2046663 , fax : + 39 - 081 - 5457081 / 2296117 , e - mail : olivierocaleo@libero.it received : 27 december 2006 / accepted : 2 july 2007 / published online : 28 march 2008 springer - verlag 2008 abstract purpose . 
the aim of this study was to compare the results of ultrasound ( us ) , whole - body scintigraphy with iodine131 ( i - 131 wbs ) and positron emission tomography with fluorine - 18 deoxyglucose ( fdg - pet ) in the follow - up of patients after thyroidectomy for differentiated thyroid carcinoma ( dtc )  . 
in each patient six anatomical regions ( right and left thyroid bed , right and left cervical region , right and left supraclavicular region ) were investigated , for a total of 78 regions . 
imaging findings were compared with the reference standards , such as fine - needle aspiration cytology ( 2 ) , biopsy ( 4 ) or clinical - radiological studies ( 7 )  . 
in the remaining 7 regions ( 9% ) , the imaging results were discordant ; in particular , tumour lesions , nodal metastases ( 4 ) and thyroid bed recurrences ( 3 ) were detected by us only ( 3 ) , by us and i - 131 wbs ( 1 ) and by fdg - pet only ( 3 )  . 
nelle restanti 7 ( 9% ) regioni , il risultato delle tre metodiche stato discordante ; in particolare , le lesioni tumorali , metastasi linfonodali ( n = 4 ) e ripresa di malattia in loggia radiol med ( 2008 ) 113 : 278288 patients ( 9 ) ; in one patient only were the two imaging techniques concordant in their positive result . 
because the thyroid is the only site of tg secretion , increased serum tg levels are caused by tumour recurrence ; after total thyroidectomy and radioiodine ablation , disease - free patients should have undetectable serum tg levels ( < 1 ng / ml ) [ 3 , 4 ]  . 
recent technical developments in ultrasound ( us ) imaging and in particular the advent of high - frequency small - parts probes have improved the techniques resolution and diagnostic accuracy , and the role of us in the follow - up of patients after thyroidectomy has been demonstrated by several studies [ 5 , 6 ]  . 
in such patients , whole - body scintigraphy ( wbs ) with a therapeutic dose of iodine - 131 ( i - 131 ) is commonly performed in conjunction with ablation of the thyroid remnant with the aim i pazienti con carcinoma differenziato della tiroide ( cdt ) richiedono unaccurata valutazione diagnostica durante il follow - up dopo terapia in quanto possono sviluppare segni di ripresa di malattia anche dopo un efficace trattamento iniziale [ 1 , 2 ]  . 
il dosaggio plasmatico della tireoglobulina ( tg ) svolge un ruolo fondamentale in quanto il tessuto tiroideo la sola sede di secrezione di tg per cui il tessuto neoplastico in caso di recidiva tumorale determina un incremento sierico della tg ; dopo tiroidectomia totale e successiva ablazione con radioiodio , la tg sierica dovrebbe essere indosabile in un paziente libero da malattia ( < 1 ng / ml ) [ 3 , 4 ]  . 
limpiego dellecografia e la sua evoluzione tecnica , grazie soprattutto allutilizzo di sonde small - parts ad elevata frequenza , ha consentito un incremento del potere di risoluzione di tale metodica con il conseguimento di informazioni diagnostiche sempre pi accurate ; il ruolo dellesame ecografico nella valutazione in follow - up di pazienti tiroidectomizzati dimostrato in diversi studi [ 5 , 6 ] ; in tali 280 radiol med ( 2008 ) 113 : 278288 of identifying possible metastatic lesions [ 7 ]  . 
us is more sensitive ( 96% ) than serum tg levels ( 57% ) and scintigraphy with a therapeutic dose of i - 131 ( 45% ) in detecting involvement of the cervical lymph nodes [ 9 ] 4 scintigraphy with a therapeutic dose of i - 131 plays a crucial role in the detection of recurrences and distant metastases in patients with high serum tg levels or a strong clinical suspicion of metastasis 5 . 
undifferentiated tumours that do not accumulate i - 131 represent a limitation of scintigraphy [ 7 ] , leading to the use of alternative radiotracers and in particular fluorine - 18 ( f18 ) fluorodeoxyglucose ( fdg ) with the acquisition of positron emission tomography ( pet ) images [ 10 , 11 ]  . 
 this paper reports our experience with a group of patients with dtc treated with thyroidectomy and followed up with us , i - 131 scintigraphy and fdg - pet with a view to comparing the results of the three techniques in identifying sites of residual disease , locoregional recurrences and distant metastases . materials and methods population we studied 13 patients ( three men , ten women ; mean age 37.817.4 years ) affected by dtc who underwent total or near - total thyroidectomy and lymphadenectomy of metastatic nodes . 
patients needing further diagnostic investigations were studied by computed tomography ( ct ) ( 7 ) or magnetic resonance imaging ( mri ) ( 2 )  . ultrasound us was performed using an atl 5500 hdi unit and a multifrequency probe ( 7.513 mhz ) with the patient lying supine with hyperextended neck to permit visualisation of the central compartment of the neck . 
the neck was imaged pazienti la scintigrafia total - body con dose terapeutica di iodio - 131 comunemente utilizzata in una fase contestuale allablazione del residuo ghiandolare allo scopo di identificare leventuale presenza di lesioni metastatiche [ 7 ]  . 
al contrario , il ruolo della scintigrafia con dose diagnostica di i - 131 nel follow - up post - chirurgico di pazienti con cdt controverso in quanto studi recenti hanno dimostrato che : 1 . 
i tumori indifferenziati non captanti lo iodio 131 rappresentano un limite dellesame scintigrafico [ 7 ] tanto che sono stati proposti traccianti alternativi tra cui quello di maggiore interesse rappresentato dal fluoro - 18 ( f18 ) fluorodesossiglucosio ( fdg ) con acquisizione di immagini in tomografia ad emissione di positroni ( pet ) [ 10 , 11 ]  . 
 riportiamo la nostra esperienza relativa ad un gruppo di pazienti affetti da cdt trattati con tiroidectomia totale studiati durante il follow - up post - chirurgico allo scopo di confrontare i risultati ecografici , della scintigrafia con i - 131 e della pet con fdg nellidentificazione dei siti di malattia residua , di recidive loco - regionali e di metastasi a distanza . materiali e metodi popolazione sono stati studiati 13 pazienti ( 3 m , 10 f , et media 37 , 817 , 4 ) affetti da cdt sottoposti a tiroidectomia totale o subtotale e linfoadenectomia dei linfonodi metastatici ; dei 13 pazienti , 8 ( 61 , 5% ) avevano una diagnosi di carcinoma papillifero e 5 ( 38 , 5% ) di carcinoma follicolare ( tabella 1 )  . in tutti i pazienti sono stati misurati i valori della tg e dellormone tireotropo ( tsh ) nella fase diagnostica postchirurgica ( tabella 1 ) ; tutti i pazienti sono stati sottoposti ad esame ecografico del collo , scintigrafia con i - 131 dopo una dose terapeutica e pet con fdg ; in tutti i casi ad eccezione di tre pazienti stato sospeso il trattamento sostitutivo con l - tiroxina in preparazione alla somministrazione dello iodio - 131 ( tsh > 50 ui / ml )  . 
gender age surgery histology type variant tnm stage therapeutic tsh dose i - 131 mbq ui / ml ng / ml iggantitg ui / ml tnm , tumour node metastasis ; tsh , thyroid - stimulating hormone ; tg , thyroglobulin ; igg , immunoglobulin g ; ca , carcinoma ; tt , total thyroidectomy ; rcl , right cervical lymphadenectomy . 
 valori di riferimento : tg : 525 ui / ml ; tsh : 0 , 15 ng / ml ; igg anti - tg < 40 ui / ml with axial and sagittal scans , and colour doppler imaging was used to evaluate the vascularity of lesions detected at baseline us . stati studiati con tomografia computerizzata ( tc ) ( n = 7 ) o risonanza magnetica ( rm ) ( n = 2 )  . ecografia whole - body i - 131 scintigraphy i - 131 scintigraphy was performed following administration of a therapeutic dose of i - 131 between 3 , 700 and 5 , 500 mbq using a whole - body scanner ( e.cam 180 dual detector - camera , siemens medical system )  . 
the whole body was scanned in the anterior and posterior projections 57 days after administration of the radionuclide . lesame ecografico stato eseguito utilizzando una sonda a multi - frequenza ( 7 , 513 mhz con ecografo atl 5500 hdi ) con il paziente in posizione supina e con il capo iperesteso permettendo la visualizzazione del compartimento centrale del collo ; sono state acquisite scansioni secondo i piani assiale e sagittale ; lintegrazione con limpiego del color - doppler ha consensito di valutare la vasco282 radiol med ( 2008 ) 113 : 278288 fluorine - 18 deoxyglucose positron emission tomography larizzazione delle lesioni evidenziate allesame convenzionale . pet was performed using a discovery ls4 ( ge medical systems ) scanner and pet / ct technique 60 min after i.v. 
administration of 300350 mbq of f - 18 fdg ; images of tracer distribution were obtained with the reconstruction of 4 - to 5mm - thick sections in the axial , coronal and sagittal planes . data analysis for each patient , we identified six anatomical regions ( right and left thyroid bed , right and left cervical regions , right and left supraclavicular regions ) to be evaluated with neck us , i - 131 scintigraphy and fdg - pet , for a total of 78 anatomical regions . 
us findings were considered indicative of lymph node involvement whenever the long to short axis ratio was > 0.7 associated with nodal hypoechogenicity and structural heterogeneity , intralesional microcalcification and diffuse hypervascularity on colour doppler imaging . 
qualitative assessment of the areas of pathological radiotracer uptake on wbs ( i - 131 and fdg - pet ) was carried out by a nuclear physician with experience in differentiating tumour lesions from areas of nonspecific uptake and by comparing the results with those of ct or mri . 
results of the qualitative analysis of images obtained with us , i - 131 scintigraphy and fdg - pet were correlated with the reference standards such as cytology ( 2 ) , histology ( 4 ) or clinical radiological studies ( 7 ) to ensure correct interpretation of imaging findings . results table 2 summarises results of the analysis carried out in the different neck regions . 
us , pet and i - 131 wbs yielded concordant results in most neck regions ( 91% ) , of which 70 were negative , and one was positive with left cervical nodal metastases . 
in three regions , the tumour was detected by us only : one case of right cervical nodes , one case of left cervical nodes and one case of left thyroid bed tumour recurrence . 
in three regions , the tumour lesion was detected by fdg - pet only : two cases of recurrence in the right thyroid bed and one case of metastatic left cervical nodes . with regard to distant metastases , fdg - pet and i - 131 wbs showed concordance of results in the majority of pascintigrafia total - body con i - 131 la scintigrafia con i - 131 stata effettuata dopo una dose terapeutica di iodio - 131 compresa tra i 3700 ed i 5500 mbq utilizzando uno scanner total - body ( e.cam 180 dual detector - camera siemens medical system )  . 
sono state eseguite scansioni del corpo intero in proiezione anteriore e posteriore dopo 57 giorni dalla somministrazione del radionuclide . pet con fluoro - 18 fdg la pet stata eseguita con uno scanner discovery ls4 ge medical system e tecnica pet / tc 60 minuti dopo la somministrazione endovenosa di una dose di f - 18 fdg compresa tra i 300 ed i 350 mbq ; sono state ottenute immagini della distribuzione del tracciante con ricostruzione di sezioni tomografiche di 4 - 5mm di spessore orientate secondo i piani assiale , coronale e sagittale . analisi dei dati per ciascun paziente sono state identificate 6 regioni anatomiche ( loggia tiroidea destra e sinistra , regione latero - cervicale destra e sinistra , regione sovra - claveare destra e sinistra ) valutate con ecografia del collo , scintigrafia con i - 131 e pet con fdg , per un totale di 78 regioni anatomiche analizzate . 
le lesioni a distanza sono state considerate come un ulteriore gruppo dellanalisi in cui sono stati confrontati i risultati della scintigrafia con i - 131 e della pet con fdg . 
il risultato ecografico stato considerato significativo per impegno linfoghiandolare da malattia nel caso in cui il rapporto tra asse maggiore ed asse minore del linfonodo risultava > 0 , 7 associato a ipoecogenicit e disomogeneit strutturale del linfonodo stesso , coesistenza di microcalcificazioni allinterno della lesione e diffusa ipervascolarizzazione alle immagini con color - doppler . 
la valutazione qualitativa delle aree patologiche captanti negli studi scintigrafici del corpo intero ( i - 131 e pet con fdg ) stata affidata allesperienza del medico nucleare nel differenziare le lesioni tumorali dalle aree di captazione aspecifica ed al confronto di tali risultati con quelli della tc o della rm . 
in two of the three discordant cases , the distant lesions ( right hemithorax and left iliac fossa , and middle mediastinum ) were identified by i - 131 wbs only , and in the third case ( left pleura ) by fdg - pet only . 
 results of the integrated surgical and radioablation therapy showed three cases of disease - free status and ten of persistence of disease at the level of the locoregional lymph nodes ( 6 ) or distant metastasis ( 4 )  . 
of the four patients with distant metastases , three were treated with a further dose of radioiodine , whereas the last patient was ineligible for further i - 131 treatment due to lack of uptake by the distant lesion . discussion results of our experience with patients with dtc treated with surgery and followed up with us , wbs after a therapeutic dose of i - 131 and fdg - pet clearly indicate a complementary role for the three techniques . 
 i risultati della terapia integrata , chirurgica e radioablativa , hanno mostrato tre casi in cui i pazienti risultavano liberi da malattia ; al contrario , in 10 casi stata osservata persistenza di malattia a livello dei linfonodi loco - regionali ( n = 6 ) o a distanza ( n = 4 ) ; in particolare , i pazienti con malattia loco - regionale sono stati trattati con lifoadenectomia in 4 casi o con una dose ulteriore del radio - iodio in 2 casi ; i pazienti con malattia metastatica a distanza sono stati trattati con una dose ulteriore di radio - iodio in 3 casi , mentre lultimo paziente non mostrava i presupposti per ulteriore terapia con i - 131 data lassenza di captazione da parte della lesione a distanza . discussione i risultati emersi dalla nostra esperienza relativa ad un gruppo di pazienti affetti da cdt , trattati con terapia chirurgica e studiati in follow - up con ecografia , scintigrafia tb dopo dose terapeutica di i - 131 ed esame pet con fdg , suggeriscono certamente un ruolo integrato delle tre tecniche diagnostiche in quanto ogni metodica mostra indicazioni specifiche a seconda che si consideri una particolare regione anatomica , la differenziazione o meno del tessuto neoplastico e la valutazione globale del corpo intero . 
per quanto riguarda le singole metodiche , i risultati del nostro studio confermano limportanza dellecografia nella valutazione della regione del collo ( loggia tiroidea , regioni latero - cervicali e sovra - claveari ) [ 5 , 6 , 9 ] durante il follow - up post - chirurgico di pazienti affetti da cdt ; a tale proposito , lecografia ha mostrato una maggiore sensibilit diagnostica rispetto alla scintigrafia con i - 131 ed alla pet con fdg nel riconoscimento in tali distretti anatomici di lesioni neoplastiche residue , recidivanti o espressione di linfoadenopatie loco - regionali . 
tale risultato , insieme agli indiscutibili vantaggi metodologici di tale tecnica quali la non invasivit , la rapidit di esecuzione ed il costo limitato radiol med ( 2008 ) 113 : 278288 fig . 
in most cases , us , whole - body i - 131 scintigraphy and fdg - pet yielded concordant results in the evaluation of the different neck regions ( 91% ) and in the identification of distant metastases rendono tale esame diagnostico pressoch insostituibile nel follow - up dei pazienti tiroidectomizzati per cdt [ 12 ]  . 
tuttavia lincidenza di un certo numero di falsi negativi , la dipendenza dalloperatore dellesame ecografico con la inevitabile ripercussione sui valori di sensibilit della metodi286 radiol med ( 2008 ) 113 : 278288 ( 77% )  . 
it should , however , be noted that the concordance was prevalently a concordance of negative findings , that is , absence of residual or recurrent disease and absence of distant metastases . 
with regard to the single modalities , our results confirm the importance of us in the evaluation of the neck region [ 5 , 6 , 9 ] ( thyroid bed ; cervical and supraclavicular regions ) during postsurgical follow - up of patients with dtc . 
this finding , together with the well - known advantages of us , such as lack of invasiveness , rapidity and inexpensiveness , make the technique virtually irreplaceable in the postsurgical follow - up of patients with dtc [ 12 ]  . however , the incidence of a certain number of false negative results , operator dependency with the inevitable impact on sensitivity , and the inability to evaluate distant metastases all call for the use of additional imaging techniques and in particular for integration with whole - body i - 131 scintigraphy and fdg - pet . 
 although the importance of i - 131 scintigraphy in detecting distant metastases during the postsurgical follow - up of patients with dtc has been widely demonstrated , its role in the search for locoregional recurrences and / or cervical or supraclavicular nodal metastases has been reconsidered , with recent studies showing greater levels of diagnostic accuracy for serum tg measurement [ 2 ] and us [ 4 ]  . 
this observation was confirmed in our study where i - 131 scintigraphy documented pathological uptake in only two out of five sites of disease , demonstrated both by pathological levels of tg and by us . 
our results with regard to the ability of i - 131 scintigraphy to detect locoregional lesions in the neck thus confirm previous doubts about the methods efficacy in detecting local recurrences in the cervical lymph nodes . 
however , although the sensitivity of i - 131 scintigraphy was indeed low ( positive in 2 / 8 cases , 25% ) , the need to administer radioiodine for radiometabolic ablation therapy of the thyroid remnants after thyroidectomy allowed us to obtain whole - body images that are fundamental in the identification of possible distant metastases . a growing number of studies have demonstrated the effectiveness of fdg - pet in the detection of distant metastases in patients with dtc [ 11 , 13 ] , although it is still unclear what additional information this technique can offer in the search for lesions in the neck during follow - up after surgery . 
in our study , the use of fdg - pet to detect locoregional lesions demonstrated definitely lower accuracy levels compared with us , confirming , as in the case of us and i131 scintigraphy , the superiority of us for the study of the neck . 
on this subject , it should be noted that the use of combined pet - ct increases the accuracy of pet alone in the evaluation of cervical lymph node stations to levels comparable with us [ 13 ]  . 
however , one of the three cases in which ca e limpossibilit di valutare la presenza di metastasi a distanza , impongono lapprofondimento diagnostico con altre tecniche di diagnostica per immagini ed in particolare lintegrazione dellecografia con la scintigrafia del corpo intero con i - 131 e recentemente con la pet - fdg . 
 pur essendo largamente dimostrata limportanza della scintigrafia con i - 131 nel follow - up post - chirurgico dei pazienti affetti da cdt sottoposti a tiroidectomia allo scopo di identificare metastasi a distanza , il ruolo di tale metodica nella ricerca di recidive loco - regionali e / o metastasi linfonodali latero - cervicali e sovraclaveari stato rivalutato in quanto recenti studi hanno dimostrano una maggiore accuratezza diagnostica del dosaggio della tg [ 2 ] e dellecografia [ 4 ] a tale scopo ; tale osservazione stata confermata nel nostro studio in quanto su 5 siti di malattia a livello del collo dimostrati sia dai livelli patologici della tg che dal risultato ecografico , solo in 2 casi la scintigrafia con i - 131 mostrava lesioni con patologica captazione . 
i risultati della nostra esperienza relativamente alla capacit della scintigrafia con i - 131 di identificare lesioni loco - regionali a livello del collo confermano dunque i dubbi sullefficacia di tale metodica nellindividuare recidive locali a livello dei linfonodi metastatici latero - cervicali ; infatti , la scintigrafia con i - 131 ha mostrato a tale proposito una bassa sensibilit diagnostica ( positivit in 2 casi su 8 , 25% ) ; tuttavia , la necessit di effettuare la somministrazione del radioiodio per il trattamento radiometabolico a scopo ablativo del residuo tiroideo dopo tiroidectomia ha consentito di ottenere lacquisizione di immagini del corpo intero ( tb ) , fondamentali per la ricerca di eventuali metastasi a distanza . sempre un numero maggiore di studi dimostrano lefficacia della pet con fdg nella ricerca di metastasi a distanza in pazienti con cdt [ 11 , 13 ] ma non ancora chiaro quali informazioni possa aggiungere tale tecnica alla ricerca di lesioni neoplastiche nella regione del collo durante il follow - up post - chirurgico . 
tuttavia , importante notare che in uno dei tre casi in cui la pet con fdg stata lunica tecnica ad individuare la lesione neoplastica a livello della loggia tiroidea destra il livello plasmatico della tg risultava indosabile ; in tale caso , lassenza di captazione di i - 131 e di secrezione di tg esprimevano probabilmente la sdifferenziazione del tessuto neoplastico nel corso del follow - up della malattia e , dunque , radiol med ( 2008 ) 113 : 278288 fig . 
le immagini mostrano la discordanza tra i risultati della scintigrafia total body con i - 131 ( a ) che non mostra alcuna captazione patologica del tracciante e la pet ( b ) che identifica lesioni linfonodali metastatiche in sede latero - cervicale sinistra , come confermato dal follow - up ecografico esame ecografico . fdg - pet was the only technique to identify the tumour in the right thyroid bed had undetectable serum tg levels . 
in this case , the lack of i - 131 uptake and tg secretion probably reflected dedifferentiation of the neoplastic tissue during the follow - up and therefore the inability of tests such as tg measurement and i - 131 scintigraphy to reveal the presence of active disease [ 14 ]  . in the identification of distant metastases , the results of i131 scintigraphy and fdg - pet were similar . 
a number of studies [ 15 , 16 ] have demonstrated variable patterns of iodine and fdg uptake by dtc metastases , referred to as flipflop uptake behaviour ; therefore , it is not uncommon to observe metastases that accumulate iodine but not fdg and others that accumulate only fdg [ 13 ]  . 
the results of our study demonstrated a similar , but heterogeneous , sensitivity and specificity of i - 131 scintigraphy and fdg - pet in the detection of distant metastases , with three cases of positive i131 scintigraphy and negative fdg - pet and two cases of metastases accumulating fdg but not i - 131 . 
these data demonstrate that the two scintigraphic techniques are complementary and equally effective in detecting distant metastases and confirm the inconsistent patterns of uptake of the two tracers previously reported in the literature . 
una serie di studi [ 15 , 16 ] hanno mostrato una variabile captazione dello iodio e del fdg da parte di metastasi da cdt , definendo con il termine di flip - flop questa differenza di captazione ; pertanto non raro osservare metastasi che captano lo iodio ma non il fdg ed altre che captano solo il fdg [ 13 ]  . 
questi dati dimostrano quindi la complementariet e lefficacia delle due tecniche scintigrafiche nella ricerca di metastasi a distanza e confermano leterogeneit di captazione dei due traccianti gi riportata in letteratura . 
pertanto , certamente da ipotizzare la possibilit di un impiego integrato della pet - fdg e della scintigrafia tb con i - 131 nel follow - up post - chirurgico di pazienti affetti da cdt in base alle problematiche clinico diagnostiche di ogni singolo caso . 288 radiol med ( 2008 ) 113 : 278288 tients affected by dtc , according to the individual patients clinical and diagnostic situation . conclusione conclusion in conclusion , our results suggest a fundamental role for us in the evaluation of the various neck regions during postsurgical follow - up of patients with dtc , especially those with a low risk of disease recurrence . 
however , whole - body i - 131 scintigraphy with a therapeutic dose is equally important for characterising tumour tissue in terms of differentiation , for correct assessment and quantification of the thyroid remnant , and for detection of locoregional and / or distant metastases in high - risk patients with differentiated tumours . 
reports from the literature as well as our preliminary results suggest that it plays a role , especially in cases of dtc that has become undifferentiated and consequently no longer secretes tg or accumulates iodine - 131 at the level of locoregional or distant lesions and is therefore undetectable by serum tg measurements or i - 131 scintigraphy . 
sardanelli5 1 department of neuroradiology , ospedale imperia , asl 1 imperiese , imperia , italy 2 department of medical physics , san martino hospital , genova , italy 3 department of health sciences , university of genoa , genoa , italy 4 department of neurological sciences ophthalmology and genetics , university of genoa , genoa , italy 5 department of medical and surgical sciences , university of milan school of medicine , irccs policlinico san donato , unit of radiology , san donato milanese , milan , italy correspondence to : r.c. 
neuroradiologia , ospedale di imperia , via santagata 57 , 18100 imperia , italy , e - mail : rcparodi@mac.com received : 1 august 2006 / accepted : 18 october 2006 / published online : 28 march 2008 springer - verlag 2008 abstract purpose . 
the procedure was validated for enhancing lesions on t1 - weighted spin - echo images after intravenous administration of 0.1 mmol / kg of paramagnetic contrast agent , randomly selected from a dataset of a longitudinal mr study on ten relapsingremitting ms patients followed for 25 years . 
during the validation session , two readers decided by consensus whether two lesions , present on the same slice of two examinations performed on subsequent dates , were the same or not . 
tale procedura stata validata su un dataset di lesioni con contrast - enhancement visibili su immagini spin - echo t1 - pesate ottenute dopo somministrazione endovenosa di 0.1 mmol / kg di mezzo di contrasto paramagnetico , selezionate mediante randomizzazione da uno studio longitudinale di 10 pazienti affetti da sm intermittenteremittente , seguiti nel tempo per 25 anni . 
in tal modo la costante k stata calibrata fino a definirne un valore per il quale lalgoritmo era in grado di fornire automaticamente la stessa valutazione dei due osservatori . radiol med ( 2008 ) 113 : 300306 was able to identify new enhancing lesions , avoiding visual inspection , which is usually a lengthy procedure . 
definito il valore opportuno di k , la pac in grado di identificare le nuove lesioni in modo automatico , evitando il controllo visuale delloperatore che normalmente comporta tempi prolungati . parole chiave : rm , risonanza magnetica sclerosi multipla nuove lesioni con contrast - enhancement introduction introduzione longitudinal trials on patients affected with multiple sclerosis ( ms ) are commonly performed including brain magnetic resonance ( mr ) imaging findings as an endpoint of the study [ 15 ]  . 
mr dataset mostly consists of number and area ( or volume ) of hyperintense lesions on unenhanced spin - echo ( se ) or fast - se dual - echo or fluid - attenuated inversion recovery images ( flair ) or of number and area ( or volume ) of enhancing lesions on t1 - weighted se images after intravenous administration of a gadolinium ( gd ) - based paramagnetic contrast agent on repeated mr exams [ 6 ]  . 
considerable expert readers time is needed to obtain these measures , especially for a slice - by - slice lesion area calculation ( from which the volume is easily derived ) , even if software has been developed to do this job in a semiautomated or totally automated manner , with large time saving [ 3 , 79 ]  . 
in fact , enhancing lesions are considered a disease activity marker and their longitudinal fluctuation in number and area or volume are useful data regarding the natural history and evolution of ms [ 11 , 12 ]  . 
 the aim of this paper is to present a supervised automatic procedure ( sap ) to decide whether an ms lesion is new or not on the basis of a comparison between two brain contrast - enhanced mr exams performed on different scan dates ( typically , subsequent examinations )  . 
si tratta per lo pi del numero e dellarea ( o volume ) delle lesioni iperintense alle sequenze precontrasto spin - echo ( se ) , fast - se dual echo o fluid attenuated inversion - recovery ( flair ) , o del numero e dellarea ( o volume ) delle lesioni con contrast - enhancement alle sequenze se t1 - pesate dopo somministrazione endovenosa di mezzo di contrasto paramagnetico a base di gadolinio , in esami rm ripetuti nel tempo [ 6 ]  . 
la realizzazione di queste misure richiede un notevole dispendio di tempo da parte di operatori esperti , soprattutto per il calcolo dellarea lesionale strato per strato ( dalla quale facilmente derivato il volume ) , sebbene siano stati sviluppati e proposti software automatici o semiautomatici in grado di ridurre i tempi di misura [ 3 , 79 ]  . 
 un altro importante end - point rm il numero delle nuove lesioni , in particolare di quelle caratterizzate da contrast - enhancement [ 10 ] ; tali lesioni sono infatti considerate un indicatore di malattia attiva e la loro variazione longitudinale in numero e area o volume fornisce informazioni preziose sulla storia naturale e levoluzione della malattia [ 11 , 12 ]  . 
le lesioni con contrast - enhancement indicano le sedi di rottura della barriera emato - encefalica e di infiammazione attiva associate al processo patologico della sm [ 13 , 14 ]  . 
gd - enhanced t1 - weighted se images were obtained five minutes after intravenous manual injection of a single ( 0.1 mmol / kg of body weight ) dose of gadopentetate dimeglumine ( gd - dtpa , magnevist , schering ag , berlin , germany )  . 
acquisition parameters were : tr 660 ms , tr 20 ms , number of excitations 2 ; field of view 250 mm ( rectangular , 6 / 8 or 7 / 8 ) ; image matrix 192 * 256 or 224 * 256 ; and slice thickness 5 mother sequences were performed but were not considered in the current study . 
 after patient positioning , the scans were located using internal brain reference points following a well - defined protocol with a high interstudy reproducibility and scan - byscan control of the scan planes [ 13 ]  . 
segmentation of enhancing lesions on postcontrast images was performed using a semiautomated software giving an output consisting of patient identification , scan date , slice position , cartesian coordinates of the centre of each lesion , and area of each lesion , as already described [ 3 ]  . 
cartesian coordinates are referred to three operator - defined orthogonal axes : one fitting the middle sagittal structures on the coronal plane ( craniocaudal , vertical or oblique axis ) and two others fitting the anterior / posterior and laterolateral aspects of the brain ( anteroposterior and laterolateral perpendicular axes )  . 
for each image , the image of the corresponding slice on the previous examination , performed one month before , was used as a reference for defining if each lesion was old ( present also on the previous exam ) or new ( absent on the previous exam )  . 
sono state ottenute scansioni se t1 - pesate 5 minuti dopo la somministrazione endovenosa manuale di una dose singola ( 0.1 mmol / kg ) di gadopentato dimeglumina ( gd - dtpa , magnevist , schering ag , berlino , germania ) con i seguenti parametri tecnici : tr 660 ms , tr 20 ms , 2 eccitazioni ; campo di vista 250 mm ( rettangolare , 6 / 8 o 7 / 8 ) ; matrice 192 * 256 o 224 * 256 ; spessore di strato 5 msono state altres eseguite altre sequenze rm , non considerate nel presente studio . per ogni indagine , dopo il posizionamento del paziente , la localizzazione dei piani di scansione stata realizzata sulla base di riferimenti endocranici secondo un protocollo ad alta riproducibilit con controllo delleffettiva posizione dei piani di scansione per ogni sequenza eseguita [ 13 ]  . 
la segmentazione delle lesioni con contrast - enhancement stata realizzata con un software semiautomatico in grado di fornire : dati di identificazione del paziente , data dellindagine , posizione dello strato , coordinate cartesiane del centro e area di ciascuna lesione , come descritto in un precedente lavoro [ 3 ]  . 
tale software utilizza una tecnica di segmentazione a regione crescente con soglia dellintensit di segnale definibile dalloperatore , fino ad ottenere lottimale corrispondenza della regione segmentata con lestensione della lesione visualizzata dalloperatore . 
le coordinate cartesiane sono riferite a tre piani ortogonali definiti dalloperatore , il primo posizionato in sede sagittale mediana sul piano di riferimento coronale ( asse cranio - caudale verticale o obliquo ) , gli altri due sulla base della simmetria antero - posteriore e latero - laterale dellencefalo ( assi perpendicolari antero - posteriore e latero - laterale )  . 
grazie allaccurato riposizionamento e allutilizzo dei punti di riferimento endocranici , la localizzazione di ciascuna lesione ( ovvero , del suo centro ) riferita al sistema di coordinate e pu essere affidabilmente comparata con la localizzazione di qualsiasi lesione osservata in indagini precedenti o successive . da questo studio abbiamo selezionato , mediante randomizzazione , 40 immagini postcontrasto contenenti almeno una lesione con contrast enhancement . 
per ciascuna immagine stata ricercata limmagine dello strato corrispondente dellindagine eseguita il mese precedente al fine di definire se ciascuna lesione era vecchia ( ovvero presente anche nellindagine precedente ) o nuova ( ovvero assente nellindagine precedente )  . la pac ha utilizzato il seguente algoritmo . 
 xa , ya e aa sono , rispettivamente , lascissa del centro , xa , ya , and aa are the abscissa of the centre , the ordinate of the centre , and the area of the lesion a , respectively xb , yb , and ab are the abscissa of the centre , the ordinate of the centre and the area of the lesion b , respectively dove : radiol med ( 2008 ) 113 : 300306 k is a constant ( 0 < k1 ) to be calculated . 
when the inequality is true , the sap stops to ask the human reader ( in this case , two neuroradiologists by consensus ) a visual control presenting the two images on the monitor with indication of the two lesions to be compared . if the two lesions are visually defined to be the same , the k value remains unmodified ; if the two lesions are visually defined to be different , the k value is reduced , step - by - step until the inequality becomes false . 
 results lordinata del centro e larea della lesione ; xb , yb e ab sono , rispettivamente , lascissa del centro , lordinata del centro e larea della lesione b ; k la costante ( 0 < k1 ) che deve essere calcolata . il software analizza il data base delle lesioni partendo con k = 1 . 
quando lineguaglianza vera , la pac si interrompe e chiede alloperatore ( in questo caso due neuroradiologi , per consenso ) il controllo visuale mediante presentazione delle due immagini su monitor con indicazione delle due lesioni da confrontare . 
se loperatore afferma che le due lesioni sono diverse , il valore di k viene progressivamente ridotto fino a quando lineguaglianza diviene falsa . we performed ten session using sap to evaluate the lesions database ; each new session started with k = 1 . 
in a , the distance between the centres of the two lesions ( segment cick ) is larger than the sum of the two radii ( ri + rk )  . 
in b , the distance between the centres of the two lesions ( segment cick ) is smaller than the sum of the two radii ( ri + rk )  . 
in this case , the visual confirmation judges that the two lesions are not the same : the constant value ( k ) will be lowered to make the inequality false . 
1a - c disegno schematico di coppie di lesioni , completamente separate ( a ) , incompletamente separate ma considerate differenti ( b ) e incompletamente separate ( ovvero ampiamente sovrapposte ) ma considerate come la stessa lesione ( c )  . 
in a la distanza tra i centri delle due lesioni ( segmento cick ) maggiore della somma dei due raggi ( ri + rk ) ; le due lesioni non hanno quindi alcuna area sovrapposta e sono completamente separate ; lineguaglianza quindi falsa e le due lesioni non possono essere considerate la stessa . 
in b la distanza tra i centri delle due lesioni ( segmento cick ) minore della somma dei due raggi ( ri + rk ) ; le due lesioni hanno quindi unarea sovrapposta e non sono completamente separate ; lineguaglianza quindi vera e le due lesioni potrebbero essere la stessa . 
subsequenly , no other modification of the k value was needed , giving an automatic differentiation between new and old lesions , without any visual control . discussion in clinical trials , automatic or semiautomatic procedures are commonly used to segment brain ms lesions : hyperintense lesions on proton - density or t2 - weighted or flair images ; gd - enhancing lesions on t1 - weighted images ; hypointense lesions on unenhanced t1 - weighted images ( black holes )  . commonly , after that a neuroradiologist has marked all lesions on a film hardcopy , dedicated operators segment the images using software giving an output consisting of lesionby - lesion area ( and volume ) and total lesion load . 
this procedure is mainly performed to reduce the neuroradiologists work time and to obtain a high reproducibility of lesion load evaluation . evaluating the number of enhancing lesion and the number of new enhancing lesions ( predictor of the occurrence of relapses [ 15 ] ) , trials on new therapies for ms can be shorter , including less patient , and less expensive . 
 however , recognition of new lesions is necessarily performed by a neuroradiologist who should control what images are present on both the current and the previous mr scan to distinguish old and new lesions . 
it is based on a geometrical algorithm able to distinguish new from old lesions with a total agreement with human visual control . the geometrical assumption works as follows : 1 . 
in this manner , on the left of the inequality , we have an estimate of the distance between the two centres ; on the right of the inequality , we have an estimate of the sum of the length of the radii 3 . 
when the estimate of the distance between centres is larger than the estimated sum of the radii , the two lesions should be considered different ; otherwise , there is the possibility that the two lesions are the same 4 . 
per lo pi , dopo che un neuroradiologo ha indicato le lesioni su pellicola , operatori dedicati segmentano le immagini mediante software che forniscono larea ( e il volume ) per ogni lesione e il carico lesionale totale . 
calcolando il numero delle lesioni con contrast - enhancement e , tra queste , il numero delle nuove ( predittivo di ricaduta clinica , [ 15 ] ) , i trial finalizzati alla valutazione di nuove terapie per la sm possono essere di durata pi breve , includere meno pazienti ed essere gravati da costi economici ridotti . 
essa basata su un algoritmo geometrico capace di distinguere le nuove dalle vecchie lesioni in totale accordo col controllo visuale degli operatori esperti . lassunzione geometrica pu essere definita come segue : 1 . 
cos , a sinistra dellineguaglianza abbiamo una stima della distanza tra i due centri mentre a destra abbiamo una stima della somma della lunghezza dei raggi . 1 / 2 + ab 3 . 
k is a modifier of the inequality and , reducing the latter part of the inequality , it determines how large the overlapping area must be to make the inequality true . 
the operator can decrease the value of k to increase the specificity of the algorithm ; in this manner , only lesions with a large overlapping surface are considered the same . different software and algorithms were introduced for automatic or semiautomatic detection or segmentation of ms lesions on unenhanced or contrast - enhanced mr images [ 3 , 1620 ]  . 
thus , to the best of our knowledge , this is the first time that a computed procedure has been proposed with the particular aim of automatic recognition of new enhancing lesions in ms . 
the first limitation is intrinsic to the segmentation method presented here and is due to the fact that each lesion is studied in a two - dimensional space , not in a three - dimensional space , making a virtually perfect slice matching between serial longitudinal mr examinations mandatory . 
 finally , it should be noted that our method could be tested for unenhanced mr images of ms lesions ( t1 - weighted se , proton - density or t2 - weighted fast se , or flair sequences )  . 
finally , due to its simple logical structure , the same method might be applied to mr ( or also computed tomography ) longitudinal studies for defining the number of new round lesions in other organs or body parts , as is the case of liver lung metastases . 
regardless , even using a conservative approach ( only a very high level of overlapping lesions being automatically defined as old , and only lesions completely separated by other lesions in the previous exam being automatically defined as new , with partial or minimal overlapping defined by human visual control ) , our method can give 4 . 
loperatore esperto pu ulteriormente ridurre il valore di k per aumentare la specificit : in tal modo solo lesioni con grande overlapping saranno considerate come la stessa lesione . in letteratura sono stati presentati numerosi software e algoritmi per il riconoscimento o la segmentazione automatica o semiautomatica di lesioni sm alle scansioni rm pree postcontrasto [ 3 , 1620 ]  . 
una di queste esperienze esplora il dominio del tempo ( ovvero le variazioni di intensit del pixel nel tempo ) dopo procedure di post - processing , per mantenere stabile la posizione tridimensionale di ciascuna lesione ( brightness normalization , field bias correction , brain masking ) [ 20 ]  . 
quindi , per quanto sia a nostra conoscenza , questa la prima volta che viene proposta una procedura computerizzata col compito specifico del riconoscimento automatico delle nuove lesioni con contrast - enhancement in pazienti affetti da sm . 
il primo intrinseco al metodo di segmentazione da noi utilizzato : ciascuna lesione studiata in uno spazio bidimensionale , non in uno spazio tridimensionale , rendendo obbligatoria una corrispondenza virtualmente perfetta tra gli strati della serie longitudinale di esami rm . 
il secondo limite il numero relativamente piccolo di nuove lesioni con contrastenhancement valutate . infine , bene osservare che il metodo qui proposto potrebbe essere testato per le lesioni sm rilevabili alle scansioni rm precontrasto ( sequenze se t1 - pesate , fast - se pesate in densit protonicao t2 - , o flair )  . 
data la semplicit della sua struttura logica , lo stesso metodo potrebbe essere applicato a studi londitudinali rm ( o anche tc ) per definire il numero di nuove lesioni rotondeggianti in altri organi o parti corporee , ad esempio metastasi epatiche o polmonari . in conclusione , abbiamo qui presentato un metodo per il riconoscimento automatico di nuove lesioni con contrastenhancement alla rm encefalica nello studio longitudinale pazienti affetti da sm . 
simonetti1 1 dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , 2 dipartimento di anatomia patologica , 3 dipartimento di urologia , policlinico universitario tor vergata di roma , viale oxford 81 , 00133 roma , italy correspondence to : g . 
thirty - seven patients ( ten healthy volunteers and 27 patients with suspected renal malignancy ) underwent t1 - , t2 - weighted and t1weighted contrast - enhanced magnetic resonance imaging ( mri )  . 
diffusion - weighted images were obtained with a single - shot spin - echo echo - planar imaging ( se - epi ) sequence with a b value of 500 s / mm2 . 
the mean adc value in normal renal parenchyma was 2.350.3110 - 3 mm2 / s , whereas mean adc value in renal malignancies was 1.720.2110 - 3 mm2 / s . 
trentasette pazienti ( 10 volontari sani e 27 con lesioni renali sospette ) sono stati studiati con imaging rm e sequenze t1 , t2 pesate e t1 pesate dopo somministrazione di bolo di contrasto paramagnetico . 
the increase in the number of imaging studies of the urogenital region in recent years is probably the main cause for the rising incidence of tumours diagnosed in the subclinical phase . high - field magnetic resonance imaging ( mri ) systems ( 3 t ) are able to perform morphological examinations with high spatial , temporal and contrast resolution , as well as physiological , metabolic and functional studies . 
by studying molecular diffusion , the ultrastructural characteristics of tissue can be studied in vivo through sampling water molecules and by exploiting the natural sensitivity of mri to the motion [ 2 ]  . 
to date , the only way of measuring molecular diffusion in vivo is the spin - echo ( se ) sequence integrated with motion - sensitive gradient pulses ( stejskal - tanner gradients ) [ 3 ]  . water transport plays a vital role in the kidney for the functions of reabsorption , concentration and / or dilution of urine . 
diffusion is anisotropic in the kidney and therefore not random in the different directions in space , with a predominance of the vector directed from the pelvis to the renal cortex , probably due to the radial orientation of the main renal structures such as tubules and vessels [ 4 , 5 ]  . 
the specific transport of ions and metabolites and the mechanism of urine concentration produce the different apparent diffusion coefficient ( adc ) values in the various renal compartments . a number of studies have assessed the diffusion characteristics of renal parenchyma to detect diseases , such as kidney ladenocarcinoma renale costituisce il 90%95% dei tumori di origine renale e circa il 3 , 5% di tutti i tumori maligni delladulto , rappresentando la sesta causa di morte per neoplasia nel mondo . 
secondo lamerican cancer society nel 2007 ci saranno 51190 nuovi casi e 12890 decessi per neoplasia del rene e della pelvi renale con un rapporto sia di incidenza che di mortalit m : f pari a circa 60 : 40 [ 1 ]  . laumento del numero di esami di imaging del distretto uro - genitale negli ultimi anni probabilmente la principale causa di incremento dellincidenza di tumori che vengono diagnosticati in fase subclinica . i sistemi di risonanza magnetica ad alto campo ( 3 t ) consentono di effettuare esami morfologici con alta risoluzione spaziale , temporale e contrastografica oltre a studi fisiologici , metabolici e funzionali . 
gli studi basati sulla tecnica di diffusione hanno ottenuto particolari vantaggi da questa evoluzione tecnologica , risultando ora pi attendibili ed accurati grazie al pi elevato rapporto segnale / rumore ed alla maggiore risoluzione spaziale . 
 nel presente studio sono riportati i risultati dellapplicazione di una sequenza single - shot echo - planare pesata in diffusione ( dwi ) con due valori del fattore b ( 0 e 500 ) , su volontari sani e pazienti con neoplasie renali precedentemente diagnosticate con altre metodiche e successivamente asportate chirurgicamente . 
lo studio di diffusione molecolare permette di esplorare in vivo le caratteristiche ultrastrutturali di un tessuto , campionate dalle molecole di acqua , sfruttando la naturale sensibilit della risonanza magnetica al movimento [ 2 ]  . 
ad oggi lunica modalit di misurazione in vivo della diffusione molecolare la sequenza spin - echo integrata da impulsi di gradiente di sensibilizzazione al movimento ( gradienti di stejskal - tanner ) [ 3 ]  . il trasporto dellacqua ha un ruolo precipuo nel rene per le sue funzioni di riassorbimento , concentrazione e / o diluizione delle urine . 
in questo organo la diffusione anisotropa poich non casuale nelle differenti direzioni dello spazio , con una predominanza del vettore diretto dalla pelvi alla corticale renale , probabilmente per lorientamento radiale delle principali strutture costituenti il parenchima renale radiol med ( 2008 ) 113 : 199213 failure , renal artery stenosis and ureteral obstruction , in which the intrinsic motion of water is altered [ 58 ]  . 
this information is fundamental for recognising and characterising renal masses [ 9 ]  . the aim of this study was to determine the mean adc value in normal renal parenchyma and renal malignancies using a high - field ( 3 - t ) device and assess the possible contribution of dwi to the differential diagnosis between the different histological types of renal carcinoma by analysing the statistical correlation between adc values and cellular density of the individual tumours . materials and methods patient population the patient population was made up of ten healthy volunteers ( six men and four women , age range 3072 years , mean age 50 years ) with morphologically and dimensionally normal kidneys on the basis of ultrasound and normal kidney function on the basis of creatininaemia , azotaemia and proteinuria , and 27 patients ( 16 men and 11 women , age range 4585 years , mean age 62 years ) suffering from expansile kidney lesions previously diagnosed with ultrasound or multislice computed tomography ( ct )  . 
all subjects underwent mri of the upper abdomen with the use of a high - field ( 3 - t ) device . focal expansile renal lesions included 17 clear - cell renal cell carcinoma ( rcc ) , four papillary rcc , three chromophobe rcc ( granular variant ) , one sarcomatoid rcc and two transitional - cell rcc , which were all histologically diagnosed following surgical resection performed 312 days after the mri study . 
all patients were informed of the study aims and provided informed consent to the diagnostic protocol , which was approved by our centres ethics committee . mri study technique the mri was performed with a 3 - t superconductive magnet ( achieva , philips medical system , best , the netherlands ) with a maximum gradient intensity of 80 mt / m and a minimum slew rate of 200 mt / m / ms , using a six - element surface coil . 
before acquisition of functional dwi sequence , a morphological study of the upper abdomen with standard sequences in baseline conditions was performed . for each patient , therefore , four breath - hold sequences were acquired : axial t1 - weighted turbo field echo ( tfe ) , axial t2 - weighted single - shot turbo spin echo ( tse ) , axial t2weighted single - shot tse with fat suppression [ spectral selection attenuated inversion recovery ( spair ) ] and coronal quali tubuli e vasi [ 4 , 5 ]  . 
la valutazione delle caratteristiche di diffusione del parenchima renale stata utilizzata in vari studi per evidenziare malattie renali quali linsufficienza renale , la stenosi dellarteria renale e lostruzione ureterale in cui si manifestano alterazioni della mobilit intrinseca dellacqua [ 58 ]  . 
tali informazioni sono di fondamentale importanza per il riconoscimento e la caratterizzazione delle neoformazioni renali [ 9 ]  . gli obiettivi dello studio attuale sono stati di determinare un valore di coefficiente apparente di diffusione ( adc ) medio del parenchima renale normale e delle lesioni neoplastiche del rene in alto campo ( 3 t ) e valutare il possibile contributo della dwi nella diagnosi differenziale tra le diverse varianti istologiche del carcinoma renale determinando la correlazione statistica tra i valori di adc e la densit cellulare delle singole lesioni neoplastiche . 
 materiali e metodi popolazione di pazienti dieci volontari sani ( 6 maschi e 4 femmine , et compresa tra 30 e 72 anni ; et media 50 anni ) con reni ecotomograficamente normali per morfologia e dimensioni e normale funzionalit renale sulla base del dosaggio di creatininemia , azotemia e proteinuria e 27 pazienti ( 16 maschi e 11 femmine , et compresa tra i 45 e 85 anni , et media 62 anni ) affetti da lesioni renali espansive precedentemente diagnosticate con ecotomografia e / o tc multistrato , sono stati sottoposti ad esame di risonanza magnetica delladdome superiore con utilizzo di magnete ad alto campo ( 3 t )  . le lesioni espansive focali del rene erano 17 carcinomi renali a cellule chiare , 4 carcinomi renali cromofili ( variante papillare ) , 3 carcinomi renali cromofobi ( variante granulare ) , 1 carcinoma renale della variante sarcomatoide e 2 carcinomi a cellule di transizione , tutti diagnosticati istologicamente dopo asportazione chirurgica effettuata entro 312 giorni dallo studio di risonanza magnetica . 
tutti i pazienti sono stati informati sulle finalit dello studio ed stato da loro ottenuto il consenso al protocollo diagnostico approvato dal comitato etico del nostro centro . tecnica di studio rm lesame rm stato eseguito con un magnete superconduttivo da 3t ( achieva , philips medical system , best , olanda ) 202 radiol med ( 2008 ) 113 : 199213 table 1 morphological sequences optimised for the 3t mri study of the kidneys t2 tse ( ssh ) coronal t2 tse ( ssh ) axial t2 tse ( ssh ) spair axial t1 ffe axial tr / te flip angle thickness / interval fov / rfov matrix ( acq / rec ) no . 
additional diffusion gradients were executed immediately before and after the 180 pulse in the se pulse train and applied along the directions of slice selection , frequency encoding and phase encoding , thus all presenting the same characteristics given by the width , duration and time interval between them . at the end of the functional study , a dynamic study was performed using volumetric ( 3d ) isotropic fast - field echo ( ffe ) t1 - weighted sequences with spair fat - signal suppression [ t1 - weighted high resolution isotropic volume examination ( thrive ) ] in the axial plane . 
this was done after intravenous administration of 0.2 mmol / kg of 0.5 mol gadolinium - diethylenetriaminepentaacetic acid ( gd - dtpa ) contrast material ( magnevist , schering , berlin , germany ) with an injection rate of 2.0 ml / s , followed by 20 cc of saline solution with an injection rate of 2.0 ml / s ( table 1 )  . con intensit massima dei gradienti pari a 80 mt / m e tempo di risalita minimo di 200 mt / m / ms , utilizzando una bobina di superficie a 6 elementi . 
i gradienti di diffusione aggiuntivi utilizzati immediatamente prima e dopo limpulso a 180 del modulo spin - echo sono stati applicati lungo le direzioni di codifica dello strato , frequenza e fase presentando tutti le stesse caradiol med ( 2008 ) 113 : 199213 table 2 diffusion - weighted imaging ( dwi ) sequence parameters for the magnetic resonance imaging study of kidneys and renal focal lesions ssh , single - shot ; nsa , number of signal acquired tabella 2 parametri della sequenza pesata in diffusione utilizzata per lo studio rm a 3t dei reni e delle lesioni focali renali tr / te 1 , 365 / 58 ms epi factor thickness / interval fov / rfov matrix ( acq / rec ) b value no . 
of sections scan length ( s ) tr / te 1365 / 58 ms epi factor thickness / interval fov / rfov matrix ( acq / rec ) b value no . 
the corticomedullary junction also seems to be less subject to contaratteristiche date dallampiezza , durata e intervallo di tempo tra gli stessi . al termine dello studio funzionale , stato effettuato uno studio dinamico trifasico utilizzando sequenze volumetriche ( 3d ) isotropiche t1 pesate ffe con soppressione del grasso spair ( thrive ) sul piano assiale , dopo somministrazione endovenosa a bolo di mezzo di contrasto gadoliniodtpa 0 , 5 molare ( magnevist , schering , berlino , germania ) 0 , 2 mmol / kg con flusso 2 , 0 ml / s , seguito da 20 cc di soluzione fisiologica di spinta a 2 , 0 ml / s . 
il posizionamento delle regioni di interesse al terzo medio parenchimale stato dettato dalla necessit di evitare il campionamento in aree soggette ad artefatti da suscettibilit di interfaccia , a livello delle regioni polari . 
la giunzione cortico - midollare sembra inoltre meno soggetta ad inquinamenti della diffusione molecolare dalla microperfusione dellorgano . per la misurazione del valore medio e della relativa deviazione standard di adc delle lesioni focali stata tracciata una singola roi di 9 pixels per lesioni con diametro massimo inferiore a 3 cm , mentre 3 roi delle stesse dimensioni sono state tracciate nelle lesioni con diametro massimo maggiore di 3 cm , evitando selettivamente il campionamento di aree necrotiche , emorragiche , calcifiche e cistiche , preliminarmente identificate allimaging morfologico e contrastografico . 
roi size in relation to the matrix used and stato eseguito il calcolo della cellularit tumorale mediante valutazione quantitativa eseguita su preparato istologico colorato con ematossilina - eosina utilizzando un microscopio ottico ( nikon eclipse e 600 , nikon corporation , osaka , giappone ) previa digitalizzazione dellimmagine con scanner piano e software di calcolo automatico . 
il valore della cellularit stato calcolato come il numero di nuclei di cellule neoplastiche in 10 campi ad alto ingrandimento ( 600 ) in aree cellulari prive di fenomeni di tipo regressivo - degenerativo ( necrosi , emorragia , fibrosi , aree cistiche )  . 
tumour cellularity was then calculated with a quantitative assessment performed on a histological sample stained with haematoxylin and eosin using a light microscope ( nikon eclipse e 600 , nikon , osaka , japan ) ; images were digitalised with a flatbed scanner , and automatic cell calculation software was used . 
cellularity was calculated as the number of neoplastic cell nuclei in ten high - power fields ( 600 ) in cellular areas , with no evidence of regressive - degenerative changes ( necrosis , haemorrhage , fibrosis , cystic areas )  . 
to reduce the risk of overor underestimating the statistical correlation , three rois were used to sample the larger tumours . analisi statistica sono stati comparati mediante test t di student non accoppiato i valori medi di adc del tessuto sano dei soggetti volontari e del tessuto sano dei soggetti portatori di lesioni focali . 
stata infine eseguita unanalisi di regressione lineare semplice per il calcolo del coefficiente di correlazione di pearson tra i dati di cellularit tumorale e di adc delle singole lesioni focali . 
data were processed using the spss software package version 12.0 ( statistical package for social sciences , chicago , il , usa )  . results we obtained 60 adc values in normal renal tissue of healthy subjects and 81 adc values in normal tissue of patients with focal lesions . 
the adc value of individual histological types , calculated as the mean of adc values of individual lesions belonging to the same histological type , was 1.740.610 - 3 mm2 / s for clear - cell rcc , 1.810.410 - 3 mm2 / s for papillary rcc , 1.740.710 - 3 mm2 / s for chromophobe rcc , 1.710.310 - 3 mm2 / s for sarcomatoid rcc and 1.440.5310 - 3 mm2 / s for transitional - cell rcc ( table 4 )  . 
per tutti i test eseguiti stato considerato statisticamente significativo un valore di p < 0 , 05 . i dati sono stati elaborati con il software spss versione 12.0 ( statistical package for social sciences , chicago , illinois )  . risultati sono stati ottenuti 60 valori di adc nel tessuto renale normale dei soggetti volontari e 81 valori di adc nel tessuto normale dei soggetti portatori di lesioni focali . 
nei 27 pazienti esaminati sono state riscontrate 27 lesioni espansive focali ( dimensioni medie 4014 , 9 mm ) , di cui 19 con dimensioni maggiori di 3 cm ( media 489 , 8 mm ) e 8 con dimensioni inferiori a 3 cm ( media 224 , 6 mm )  . 
il valore medio di adc nel parenchima normale dei volontari sani risultato pari a 2 , 350.31x10 - 3 mm2 / s ( range 2 , 102 , 6110 - 3 mm2 / s )  . 
il valore di adc dei singoli istotipi , calcolato come media dei valori di adc delle singole lesioni focali appartenenti allo stesso istotipo , risultato rispettivamente di 1 , 740 , 610 - 3 mm2 / s per il carcinoma renale a cellule chiare ; 1 , 810 , 410 - 3 mm2 / s per il carcinoma renale papillare ; 1 , 740 , 710 - 3 mm2 / s per il carcinoma renale granulare , 1 , 710 , 310 - 3 mm2 / s per il carcinoma renale variante sarcomatoide e 1 , 440 , 5310 - 3 mm2 / s per il carcinoma a cellule transizionali ( tabella 4 )  . 
 il test t di student per la comparazione tra i valori medi di adc delle lesioni renali focali e quelli del parenchima renale sano ha dimostrato valori di adc delle lesioni renaradiol med ( 2008 ) 113 : 199213 li focali significativamente inferiori rispetto al parenchima renale sano ( p < 0 , 01 )  . 
lo sviluppo tecnologico ha permesso lacquisizione di sequenze per lo studio delladdome superiore in singola apnea respiratoria , eliminando cos gli artefatti dovuti ai movimenti volontari e riducendo significativamente quelli involontari . 
la velocit di acquisizione dei dati stata inoltre ulteriormente incrementable 4 mean apparent diffusion coefficient ( adc ) values and standard deviation for each histological type of focal lesion in the patient group histotype no . 
of cases adc mean value ( 10 - 3 mm2 / s ) tabella 4 valori di adc medi con relativa deviazione standard dei singoli istotipi neoplastici relativi alle lesioni renali focali dei pazienti esaminati istotipo n . 
the acquisition speed has also been further increased with the application of sense : arrays of multiple receiver coils simultaneously sample the signal returning from more than one part of the body surface and then separate the encoded data provided by each element of the coil . although the degree of diffusion weighting of a sequence is indicated by the b value , which encompasses the main characteristics of diffusion gradients ( amplitude , duration and time interval between gradients ) , the use of a characteristic b value for tissue under study is still broadly debated in the literature owing to the presence of often conflicting results [ 12 , 13 ]  . 
the main limitation in the application of dwi sequences to the abdomen when using 1.5 - t devices is the impossibility of applying gradients capable of obtaining a very high b value because of the low snr . 
a further advantage of high - field devices in dwi is the greater spatial resolution obtained ( 5 mm slice thickness ) compared with 1.5 - t scanners , in which the lowest slice thickness capable of providing a diagnostic image is 7 mm , with the advantage of reducing partial volume artefacts and therefore increasing the precision of calculating the adc value of neoplastic tissue . 
there are no dwi studies of renal parenchyma performed with high - field scanners ( 3 t ) published in the literature . with lower b values ( 30100 s / mm2 ) the perfusion component and the t2 component of tissues lead to an overestimation of the adc value , whereas a b value > 1 , 000 s / mm2 leads to formation of highly noisy images , because the t2 of abdominal tissue is lower than that of cerebral tissue . 
in our study , we used a diffusion sequence with an echo time ( te ) of 61 ms and a b value of 500 , which is a valid compromise between high diffusion weighting for the same amplitude tata applicando la tecnica di codifica del segnale sense mediante lutilizzo di bobine multicanale che campionano contemporaneamente il segnale proveniente da pi parti della superficie corporea e poi separano i dati di codifica forniti da ciascun elemento della bobina . 
 lentit della pesatura in diffusione di una sequenza indicata dal valore del fattore b che racchiude in s le principali caratteristiche dei gradienti di diffusione ( ampiezza , durata e intervallo di tempo tra i gradienti ) , ma lutilizzo di valori di un fattore b caratteristico per il tessuto in esame resta un problema ampiamente dibattuto in letteratura per la presenza di risultati spesso discordanti [ 12 , 13 ]  . 
la principale limitazione nellapplicazione delle sequenze di diffusione alladdome con sistemi ad 1 , 5 t dovuta allimpossibilit di attivare gradienti tali da ottenere valori di fattore b molto elevati a causa del basso rapporto segnale / rumore . 
un vantaggio ulteriore dellutilizzo di macchinari ad alto campo nella formazione dellimmagine in diffusione rappresentato dalla pi elevata risoluzione spaziale ( spessore di strato 5 mm ) rispetto a quelli a 1 , 5 t , in cui lo spessore di strato pi basso per ottenere unimmagine diagnostica di 7 mm , con il vantaggio di ridurre gli artefatti da volume parziale e quindi di rendere pi preciso il calcolo del valore di adc del tessuto neoplastico . 
in letteratura non sono riportati studi di diffusione del parenchima renale eseguiti con sistemi ad alto campo magnetico ( 3 t )  . per bassi valori di fattore b ( 30100 s / mm2 ) la componente perfusionale e la componente t2 dei tessuti determinano la sovrastima del valore di adc mentre , valori di fattore b maggiori di 1000 s / mm2 determinano la formazione fig . 
the rois were positioned at the level of the corticomedullary junction , with preference for the middle kidney region , since this area is less subject to the effects of capillary perfusion [ 8 ]  . studies published in the literature over the last 10 years have reported different results regarding the adc value of healthy renal parenchyma in vivo obtained with different 1.5 - t scanners and different diffusion sequences . 
in a later study , the same authors [ 15 ] assessed the same group of dehydrated and subsequently rehydrated patients and obtained adc values of normal renal parenchyma between 2.880.6510 - 3 mm2 / s and 3.560.3210 - 3 mm2 / s . 
nel presente studio stata utilizzata una sequenza di diffusione con un tempo di eco ( te ) di 61 ms ed un valore di fattore b di 500 , valido compromesso tra elevata pesatura in diffusione a parit di ampiezza di banda e qualit finale dellimmagine . le roi sono state posizionate a livello della giunzione cortico - midollare , preferendo la sede medio - renale , in quanto meno influenzata dagli effetti della perfusione capillare [ 8 ]  . nella letteratura dellultimo decennio sono stati riportati diversi risultati del valore di adc del parenchima renale sano in vivo ottenuti con differenti tomografi a 1 , 5 t e differenti sequenze di diffusione . 
in our study , we recorded a mean adc value in healthy subjects in conditions of normal hydration of 2.350.3110 - 3 mm2 / s , a value that is confirmed when compared with previous studies using 1.5 - t scanners [ 8 , 11 , 12 ]  . pathological processes alter the structural organisation of parenchyma because of the presence of necrotic and / or regenerative processes , as well as modifications at the cellular level ( inflammation , tissue scarring , neoplastic infiltration )  . 
these changes indirectly influence the ultrastructure of the intercellular compartment and therefore the number of water molecules present in the tissues as a result of variations in permeability , osmolarity or active transmembrane transport . 
 [ 5 ] , in contrast , studied how diffusion can differentiate hydronephrosis from pyonephrosis , with much higher adc values in the first case ( 2.980.6510 - 3 mm2 / s ) than in the second ( 0.640.3510 - 3 mm2 / s )  . 
 [ 6 ] recorded lower adc values of healthy renal parenchyma in three patients with acute pyelonephritis , in one case of pyogenic abscess and in one 2 , 880 , 6510 - 3 mm2 / s e 3 , 560 , 3210 - 3 mm2 / s . 
 [ 4 ] hanno campionato nel parenchima renale sano valori di 1 , 680 , 1510 - 3 mm2 / s mentre fukuda [ 17 ] rappresentava valori di 1 , 50 e 1 , 5310 - 3 mm2 / s in sede mediorenale utilizzando fattori b compresi tra 317 e 932 s / mm2 . nella nostra esperienza , a livello del parenchima renale sano dei pazienti volontari , in condizioni di normale idratazione , abbiamo registrato un valore medio di adc di 2 , 350 , 3110 - 3 mm2 / s . ; valori che si confermano se confrontati con le precedenti esperienze effettuate con magneti da 1 , 5 t [ 8 , 11 , 12 ]  . i processi patologici alterano lorganizzazione strutturale di un parenchima sia per la presenza di processi necrotici e / o rigenerativi , sia per lintervento di modificazioni a livello cellulare ( infiammazione , tessuto cicatriziale , infiltrazione neoplastica )  . 
tali fenomeni si ripercuotono indirettamente sullultrastruttura del compartimento intercellulare e quindi sul numero di molecole di acqua presenti nei tessuti a causa di variazioni di permeabilit , osmolarit o capacit di trasporto attivo trans - membrana . 
 [ 7 ] hanno registrato valori di adc significativamente inferiori nellinsufficienza renale cronica , tanto a livello corticale quanto a livello della midollare , rispetto ad analoghi valori del parenchima sano . 
 [ 18 ] assessed pathological conditions such as pyelonephritis , acute kidney failure , chronic kidney failure and ureteral obstruction and recorded lower mean adc values in patients with kidney disease than in healthy volunteers . 
 [ 5 ] hanno invece valutato come la diffusione possa differenziare tra loro condizioni renali patologiche , quali lidronefrosi e la pionefrosi , riscontrando valori di adc molto pi elevati per la prima ( 2 , 980 , 6510 - 3 mm2 / s ) rispetto alla seconda condizione ( 0 , 640 , 3510 - 3 mm2 / s )  . 
 [ 6 ] hanno riportato valori di adc pi bassi di quelli del parenchima renale sano in tre pazienti con pielonefrite acuta , in un caso di ascesso da piogeni e in un paziente con pielonefrite xantogranulomatosa . 
 [ 18 ] hanno valutato condizioni patologiche quali pielonefriti , insufficienza renale acuta , cronica e ostruzione ureterale , riscontrando valori di adc medio minori nei pazienti affetti da patologie renali rispetto ai pazienti volontari sani . 
 un valore di restrizione alla diffusione molecolare dellacqua nei tessuti neoplastici pu essere correlato tanto alla maggiore densit cellulare tissutale , generata dallelevato indice di replicazione neoplastica con conseguente riduzione dellampiezza degli spazi intercellulari , quanto alla reale alterazione ultrastrutturale del tessuto renale . 
la riduzione della coerenza di movimento delle molecole di acqua nei tre assi dello spazio , con conseguente riduzione del segnale rm sarebbe quindi dovuta allanarchia di organizzazione ed accrescimento delle cellule neoplastiche , non organizzate nella tipica morfologia a setti vasculo - tubulari orientati radialmente in senso cortico - midollare . 
 come gi dimostrato nei risultati , lanalisi non ha documentato differenze statisticamente significative del valore medio di adc tra le singole varianti istologiche neoplastiche di adenocarcinoma considerate , per cui non possibile distinguere i differenti istotipi neoplastici del carcinoma renale sulla base del valore di adc . 
even though mean adc values from several rois for lesions with a diameter > 3 cm and a statistically significant correlation was found between mean adc and cellularity , the overall analysis may have been invalidated by an overor underestimation of the values reported . 
in addition , although macroscopic colliquative and necrotic areas were excluded when selecting the rois to apply to lesions > 3 cm , the mean adc value may have been influenced by microscopic degenerations , which were not visible in mri morphological sequences . 
it therefore cannot be ruled out that enrolling a greater number of renal tumours of limited size in the case series would not have led to a variation in the findings . nonetheless , the use of dwi sequences in a single breath - hold and with the technical parameters described above could prove to be a noninvasive , effective and repeatable technique for identifying neoplastic renal lesions in the case of doubt at morphological imaging , which would not significantly change the standard acquisition times of the mri diagnostic examination . 
routine application of the technique in diagnostic practice could provide the necessary data for its validation in characterising parenchymal neoplastic lesions . corrisponde precisamente al campione di tessuto analizzato dallanatomo - patologo per il calcolo della cellularit . 
nonostante siano stati ottenuti valori medi di adc da pi regioni di interesse per le neoplasie di diametro > 3 cm e sia stata riscontrata una concordanza statisticamente significativa tra adc e cellularit media , lanalisi complessiva potrebbe una essere inficiata da una sovra o sottostima dei valori riportati . 
inoltre , bench siano state escluse le aree necrotiche e colliquative macroscopiche nella selezione delle roi da applicare nelle lesioni > 3 cm , il valore medio di adc potrebbe essere stato condizionato da degenerazioni microscopiche non visibili nelle sequenze morfologiche di risonanza magnetica . 
non possibile quindi escludere che larruolamento nella casistica di un maggior numero di neoplasie renali di dimensioni contenute non avrebbe portato ad una qualche variazione dei risultati . lutilizzo della sequenza di diffusione rm in singola apnea respiratoria e con i parametri tecnici da noi descritti potrebbe comunque rappresentare nel futuro uno strumento non invasivo , efficace e ripetibile per lidentificazione della patologia neoplastica renale nei casi dubbi alla valutazione morfologica e senza modificare sensibilmente i tempi standard di acquisizione dellesame diagnostico di risonanza magnetica . 
lauspicabile applicazione routinaria della tecnica nella pratica diagnostica potrebbe infine fornire i dati necessari alla validazione di questo nuovo espediente tecnologico nella caratterizzazione delle neoplasie parenchimali . conclusions conclusioni on the basis of this preliminary experience , diffusionweighted sequences have proved to be a reliable and repeatable technique for differentiating healthy renal parenchyma from neoplastic tissue . 
dw - mri with high - field scanners , while still within the examination times of a normal morphological diagnostic examination , appears to be useful in distinguishing neoplastic lesions from the healthy kidney . mri diffusion is , in fact , an indirect index of the changes in intercellular spaces , intercellular junctions and quantity of water contained in tissues and can become a useful noninvasive instrument for characterising neoplastic kidney lesions . 
larger patient populations , with a greater number of small - sized lesions , are required for consistent validation of the technique . sulla base di questa esperienza preliminare , le sequenze pesate in diffusione si sono dimostrate uno strumento affidabile e riproducibile per differenziare il parenchima renale sano dal tessuto neoplastico . 
la diffusione rm con sistemi ad alto campo , pur rimanendo nei tempi di esecuzione di un normale esame diagnostico morfologico , appare utile nella distinzione delle neoplasie dal rene sano . 
la diffusione rm rappresenta infatti un indice indiretto della modificazione degli spazi intercellulari , delle giunzioni intercellulari e della quantit di acqua contenuta nei tessuti e pu divenire uno strumento utile e non invasivo per la caratterizzazione delle lesioni neoplastiche del rene . 
simonetti1 dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , 2cattedra di gastroenterologia , unit di epatologia , policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy 3philips medical systems italia correspondence to : a . 
the aim of this study was to correlate the in vivo high - field ( 3 - tesla ) 1h mrs features of noncirrhotic chronic hepatitis c patients stratified according to the histopathological stages of fibrosis . 
the subdivision of patients into the histopathological stages of fibrosis was based on the ishak fibrosis ( f ) scoring system : mild hepatitis ( 0f1 ) , moderate ( 2f3 ) and severe hepatitis ( 4f5 )  . 
the particular metabolite content was evaluated in relative units ( ru ) , according to the pattern metabolite / h2o = area of the metabolite 1 , 000 / area of nonsuppressed water . 
i pazienti sono stati suddivisi in tre gruppi in base al grado di fibrosi epatica utilizzando il sistema di classificazione della fibrosi di ishak : fibrosi lieve ( 0f1 ) , fibrosi moderata ( 2f3 ) e severa ( 4f5 )  . 
in conslusione la 1h mrs con alto campo 3t in grado di differenziare la fibrosi lieve / moderata da quella severa nelle epatiti croniche e pu essere considerata un utile complemento degli esami di imaging tradizionali nello studio del fegato . parole chiave fegato fibrosi risonanza magnetica , spettroscopia epatiti croniche introduction introduzione chronic diffuse liver disease is a worldwide problem [ 1 , 2 ]  . whereas histology remains the gold standard by which to diagnose hepatic fibrosis , sampling error is inherent in the technique [ 3 ] , and it has been postulated that hepatic magnetic resonance spectroscopy ( mrs ) could potentially provide a more accurate representation of the disease process . recently , in vivo hepatic mrs has been suggested for the evaluation of chronic diffuse liver disease [ 48 ]  . whereas in vivo hepatic 31p mrs has been shown to correlate with disease severity in chronic liver disease as assessed by histopathological analysis , its availability as a technique is not widespread [ 9 ]  . 
based on these results , we undertook a study to correlate the in vivo 3 - t 1h mrs features of stratified chronic hepatitis c with different disease severity with the corresponding histopathologic stages of fibrosis . materials and methods patients from november 2005 to september 2006 , 23 consecutive la patologia epatica cronica una malattia di larga diffusione a livello mondiale ( 1 , 2 )  . 
in particolare , la 31p mrs in vivo ha dimostrato di correlare con la severit dellepatopatia cronica [ 9 ] ; tuttavia tale tecnica non ampiamente diffusa , dato che richiede la necessit di dover implementare gli scanner tradizionali con harware aggiuntivi . 
cho e colleghi , utilizzando questa tecnica con uno scanner rm 1 , 5t , sono stati in grado di individuare differenze tra i vari stadi dellepatite cronica [ 10 ]  . 
laumento della risoluzione spettrale ed un pi alto rapporto segnale - rumore pu essere ottenuto passando da uno scanner a 1 , 5 t ad uno con campo magnetico 3 t . 
a tal riguardo , alcuni autori hanno riportato un incremento della risoluzione spettrale utilizzando uno scanner rm 3 t rispetto allo scanner rm 1 , 5 t [ 11 ]  . 
sulla base di questi risultati abbiamo condotto uno studio in vivo finalizzato a correlare la classificazione istopatologica del grado di fibrosi ottenuta con la biopsia con le caratteristiche spettroscopiche dei fegati di pazienti con epatopatia cronica evolutiva valutate in vivo con un sistema di 1h mrs a 3 t . radiol med ( 2008 ) 113 : 289299 patients ( 16 men and seven women ; mean age 65 years ; range 5672 ) with chronic hepatitis c who had undergone liver biopsy were included in this study ( table 1 )  . 
quantification of hcv - rna in serum samples was performed using a commercially available kit ( amplicor hcv monitor tm test , roche diagnostic systems , branchburg , nj , usa )  . 
a fasting blood sample was obtained on the day of liver biopsy for analysis of the following parameters : serum alanine aminotransferase ( alt ) , - glutamyl transferase , bilirubin , alkaline phosphatase , serum glucose , cholesterol and triglycerides . all patients had persistently abnormal liver function tests ( lfts ) with elevated serum levels of alt : geometric mean 51.0 [ interquartile range ( iqr ) 2792 iu / l ] and / or serum glutamyl transferase ( gt ) : geometric mean 53.2 ( iqr 2773 iu / l )  . 
physical activity was comparable in both groups , as all were included in the moderate physical activity level ( categorical score 2 ) according to the international physical activity questionnaire [ 12 ]  . 
informed conmateriali e metodi pazienti dal novembre 2005 al settembre 2006 , sono stati inclusi in questo studio 23 pazienti ( 16 maschi e 7 femmine ; et media 65 anni ; range 5672 ) con epatite cronica c , precedentemente sottoposti a biopsia epatica , ( tabella i )  . 
sono stati esclusi dallo studio pazienti che presentavano markers di infezione da virus dellimmunodeficienza umana , pazienti con positivit per la presenza di antigene di superficie dellepatite b , e con evidenza di processi autoimmuni . 
un campione ematico a digiuno stato ottenuto lo stesso giorno della biopsia epatica per lanalisi dei seguenti parametri : alanina aminotransferasi sierica ( alt ) , - glutammil transferasi , bilirubina , fosfatasi alcalina , glucosio sierico , colesterolo e trigliceridi . 
the subdivision of patients into disease stages was based on the ishak fibrosis ( f ) scoring system : mild hepatitis ( 0f1 ) , moderate ( 2f3 ) and severe hepatitis ( 4f5 )  . mr spectroscopy image guided , 1h localised , mrs and t2 - weighted imaging were performed on a 3 - t intera achieva mr scanner ( philips medical systems , the netherlands ) using the q body for the radiofrequency transmitting signal and a body surface coil for signal receiving . 
t2 - weighted images acquired in orthogonal planes were used for graphical prescription of the spectroscopy volume of interest ( voi )  . vois were centred within the right hepatic lobe , taking care to avoid large blood vessels and the gall bladder . 
imageguided water - suppressed spectra were acquired using the point - resolved spectroscopy sequence ( press ) technique ( tr = 1 , 500 ms , te = 38 ms , bandwidth 2 , 000 hz , 256 measurements , 1 , 024 sample points yielding an acquisition time of 6 : 38 min )  . 
fully automated shimming was carried out on the voxel ( 303040 mm ) to ensure maximum field homogeneity , and excitation water suppression was used to suppress signal from water during data acquisition . 
unsuppressed water spectra using the press technique ( tr = 1 , 500 ms , te = 38 ms , 64 measurements , bandwidth 2 , 000 hz , 1 , 024 sample points , acquisition time 3 min ) were also acquired for use as an internal standard . 
to assess intraexamination reproducibility of the 1h mrs results , the analysis that consisted of the acquisition of both water - suppressed spectra and water - unsuppressed spectra was performed in triplicate and the coefficient of variation measured . 
the total examination time was about 30 m interexamination reproducibility was assessed by performing the analysis on a voxel from the same position in the liver , in each given subject , on three different occasions . 
to determine potential regional metabolite variation within the liver , 1h mr spectra were obtained in all patients by performing the analysis on a same - sized voxel in two different positions within the right lobe of the liver . 
spectroscopy was conducted in the fasting state . spectral data processing spectra obtained during the examinations were processed automatically using the table of chemical shift based on 10 pazienti sono risultati con unepatite di grado moderato , mentre 6 pazienti con epatite di grado severo . 
i 6 soggetti sani di controllo comprendevano 4 maschi e 2 femmine ; con et media comparabile rispetto a quella del gruppo in esame ( p < 0 , 05 )  . 
lattivit fisica dei soggetti di controllo , valutata secondo i criteri del physical activity questionnaire [ 12 ] era uguale a quella del gruppo in esame , ovvero tutti i soggetti avevano dimostrato avere un livello di attivit fisica moderata ( score due )  . 
lo studio stato approvato dal nostro comitato etico interno . valutazione istologica i campioni di tessuto sono stati fissati in paraffina , tagliati e colorati con colorazioni ematossilina - eosina e van gieson ( collagene )  . 
i pazienti sono stati classificati nei diversi stadi di malattia utilizzando il sistema di classificazione del grado di fibrosi secondo ishak ( f ) : fibrosi lieve ( 0f1 ) , moderata ( 2f3 ) e severa ( 4 f 5 )  . spettroscopia rm sono state acquisite immagini t2 - pesate e , sulla base delle immagini morfologiche , stato posizionato il voxel per lacquisizione spettroscopica 1h mrs , utilizzando uno scanner rm 3 tesla intera achieva ( philips medical systems ; olanda ) .una bobina q body stata impiegata per la trasmissione del segnale di radiofrequenza ed una bobina body di superficie per la ricezione del segnale . 
sono stati ottenuti spettri con soppressione dellacqua utilizzando la tecnica point - resolved spectroscopy sequence ( press ) ( tr = 1500 ms , te = 38 ms , bandwidth 2000 hz , 256 misurazioni , 1024 campionamenti , per un tempo di acquisizione totale di 6 : 38 min )  . 
on the basis of obtained spectra , we evaluated the particular metabolite contents , in relative units ( ru ) , according to the pattern : metabolite / h2o = area of the metabolite 1 , 000 / area of nonsuppressed water . 
analysis of covariance ( ancova ) and partial correlation analysis were used to assess the effect of anthropometric variables on the correlations between the mrs - derived ratios and fibrosis . 
per stabilire la riproducibilit intra - esame dei risultati della 1h mrs , le acquisizioni degli spettri , rispettivamente con soppressione e senza soppressione dellacqua , sono state eseguite tre volte ed il coefficiente di variazione stato misurato . 
il tempo desame totale risultato essere di circa 30 mla riproducibilit interesame stata valutata eseguendo lanalisi su un voxel localizzato nella medesima posizione allinterno del fegato in ciascun soggetto , in tre differenti occasioni . 
per determinare la potenziale variazione regionale nella concentrazione dei metaboliti allinterno del fegato , in tutti i pazienti sono stati ottenuti spettri acquisendo i dati posizionando il voxel in due siti differenti allinterno del lobo destro del fegato . lesame spettroscopico stato condotto in condizione di digiuno . results repeated interand intraindividual measurements generated reproducible results with approximately 8% and 5% variation . 
1h mrs liver spectra were successfully obtained in all examinations , and no regional metabolite variations were observed when changing the position of the voxel within the right lobe of the same patient . 
la concentrazione dei metaboliti ottenuti mediante esame spettroscopico stata calcolata in unit relative ( ru ) , in base alla formula : metabolita / h2o = area del metabolita 1000 / area di acqua non soppressa . analisi statistica sono state calcolate le differenze tra i due gruppi utilizzando il test non parametrico mann - whitney u test . 
non sono state osservate significative variazioni regionali nella concentrazione dei metaboliti nelle misurazioni ottenute spostando la posizione del voxel allinterno del lobo destro in ciascun radiol med ( 2008 ) 113 : 289299 fig . 
1a - c ratios of choline - containing compounds ( ccc ) / h2o ( a ) , glutamine / glutamate ( glx ) / h2o ( b ) , and lipid / h2o ( c ) on 1h magnetic resonance spectra at various stages of fibrosis severity . 
the elevation of ccc , glx and lipids with severity of disease is shown , with clear separation between the mild / moderate fibrosis and the severe fibrosis groups . fig 1a - c i grafici illustrano le concentrazioni relative di ccc ( a ) , glx ( b ) e lip ( c ) misurate con 1h mrs durante i diversi stadi della fibrosi . 
the results , shown in table 2 , show that all mrs - derived ratios were significantly associated with fibrosis , even after adjusting for bmi , whr and waist . 
in tutti gli spettri esaminati i picchi dei lipidi erano localizzati a 0 , 9 - 1 , 4 ppm , il complesso glutammato / glutammina ( glx ) a 2 , 12 , 6 ppm ed i prodotti contenenti colina ( ccc ) a 3.3 pp stata osservata una correlazione diretta tra la concentrazione della glx e della ccc e il grado di malattia ( ccc , r = 0 , 7880 , 95% intervallo di confidenza da 0 , 5685 a 0 , 9028 , p < 0 , 0001 ; glx , r = 0 , 8323 , 95% intervallo di confidenza da 0 , 6381 a 0 , 9269 , p < 0 , 0001 )  . 
analogamente , una correlazione diretta significativa stata trovata tra la concentrazione dei lipidi e la severit della malattia ( r = 0 , 7626 , 95% intervallo di confidenza 0 , 5014 a 0 , 8964 , p < 0 , 0001 )  . 
i risultati , riportati nella tabella 2 , mostrano che le concentrazioni spettroscopiche dei metaboliti sono significativamente associate con la fibrosi anche dopo correzione per il bmi , la vita e il whr . 
difatti , anche lanalisi di correlazione parziale , eseguita dopo correzione per il bmi , la vita ed il whr , come evidenziato nella tabella 3 , ha mostrato che la correlazione tra lipidi e fibrosi risultata ridotta ( r = 0 , 76 , p < 0 , 0001 vs r = 0 , 56 , p = 0 , 01 ) ma non in modo significativo ( p = 0 , 05 ) , mentre non stata osservata nessuna riduzione nella correlazione tra fibrosi e ccc e glx dopo correzione ( ccc , r = 0 , 79 , p < 0 , 0001 vs r = 0 , 78 , p < 0 , 0001 ; glx r = 0 , 83 , p < 0 , 0001 vs r = 0 , 77 , p < 0 , 0001 )  . discussione in questo studio abbiamo mostrato che la 1h mrs con magnete 3t in pazienti con epatite cronica c - correlata , pu contribuire a caratterizzare in maniera non invasiva la severit della malattia . 
i nostri dati hanno mostrato che sia il rapporto del ccc che del glx rispetto allacqua , misurati con 1h mrs , sono un sensibile marker della severit della malattia epatica . 
nel nostro studio abbiamo trovato un incremento progressivo con la severit della malattia dei rapporti ccc / h20 , glx / h20 e lip / h20 i nostri risultati sono in parte in accordo con i dati ottenuti da cho et al . 
essi hanno riportato in un gruppo di 75 pazienti con epatite cronica b e c una progressivo aumento dei ccc e del glx con lincremento dello stadio istologico [ 10 ]  . 
tuttavia , al contrario dei nostri risultati , cho e colleghi hanno dimostrato una riduzione del picco di lipidi progressivo con la severit della malattia , ben evidente , nella fase avanzata della malattia ( cirrosi )  . questa discrepanza pu essere spiegata dal fatto che nel loro studio sono stati inclusi pazienti con sia epatite cronica hcv che hbv - correlata . 
however , they reported a decrease in the lipid peak progressive with disease severity , which was well evident , according to their data , in end - stage cirrhosis . 
moreover , in this study we chose not to include patients with complete cirrhosis ( stage 6 fibrosis ) , who can be easily differentiated from noncirrhotic subjects on clinical and biochemical grounds . as phospholipid cell membrane precursors [ phosphomonoesters ( pme ) such as phosphocholine ( pc ) ] and cellmembrane degradation products [ phosphodiesters ( pde ) such as glycerophosphorylcholine ( gpc ) ] all contribute to the ccc compounds , a limitation of our 1h mrs study , as with all 1h liver mrs , is the impossibility of discriminating between pme and pde . 
however , based on the literature data obtained with 31p mrs , we assumed that the progressive increase in ccc observed was probably due to the increase in the pme component . 
tuttavia , sulla base dei dati presenti in letteratura ottenuti con 31p mrs , possiamo ipotizzare che il progressivo incremento della concentrazione di ccc da noi osservato sia dovuto ad un incremento dei pme . 
infatti , numerosi studi sul metabolismo epatico eseguiti mediante 31p mrs nei pazienti con alterazioni epatiche infiammatorie e cirrosi epatica , hanno mostrato un incremento nella concentrazione dei pme , probabile espressione dellaumento della sintesi dei fosfolipidi di membrana indotta dal processo di rigenerazione epatocitaria . 
hanno trovato una correlazione significativa tra rapporto pme / pde e stadio istologico in una serie di 48 soggetti con epatite cronica c [ 9 ] .un indiscutibile vantaggio della 1h mrs per lo studio del fegato la possibilit di una valutazione quantitativa del contenuto totale di lipidi in vivo . 
found a significant correlation between pme / pde ratio and biopsy scores in a series of 48 subjects with chronic hepatitis c [ 9 ]  . an unquestionable advantage of 1h mrs use for liver examination is the possibility of a quantitative evaluation of total lipid compound contents in vivo . 
observed a correlation between lipid amounts in the liver as determined with 1h mrs and chemical methods on liver biopsy specimens in patients with alcohol - induced liver steatosis [ 17 ]  . 
indeed , hepatic steatosis is a frequent histological finding in patients with chronic hepatitis c and has been shown to be one of the characteristic feature of chronic hcv infection [ 18 , 19 ]  . 
to assess the possible contribution of body fat conhanno mostrato una significativa relazione tra grado istologico di steatosi e il contenuto lipidico stimato mediante esame 1h mrs [ 16 ]  . 
utilizzando la 1h mrs hanno osservato una correlazione tra la concentrazione spettroscopica dei lipidi nel fegato e i lipidi valutati istologicamente su campioni bioptici epatici di pazienti con steatosi epatica alcolica [ 17 ]  . 
ci non sorprendente , infatti , la steatosi epatica un riscontro istologico frequente in pazienti con epatite cronica c ed stata dimostrata essere una delle caratteristiche dellinfezione da virus dellepatite c [ 18 , 19 ]  . 
 noto che esiste una stretta correlazione tra il contenuto di grasso corporeo e il contenuto lipidico epatico . per valutare il possibile contributo del contenuto lipidico corporeo nella associazione tra i lipidi determinati con la spettroscopia e la fibrosi , abbiamo eseguito unanalisi della covarianza utilizzando come covariate il rapporto vitafianco ( whr ) , la vita e lindice di massa corporea ( bmi )  . bench la correlazione tra lipidi epatici e fibrosi si sia ridotta dopo la correzione , indicando un possibile contributo della massa lipidica corporea sulla quota di lipidi epatici , rimasta statisticamente significativa . 
un altro limite del nostro studio che la concentrazione dei metaboliti stata 298 radiol med ( 2008 ) 113 : 289299 tent on the association between liver - mrs - derived lipids and fibrosis , we performed a correlation analysis adjusting for bmi , waist and whr . 
although the correlation between liver lipids and fibrosis was lessened after the adjustment , indicating a possible contribution of body fat content on liver lipids , it was still statistically significant . 
however , absolute quantisation of metabolites is difficult to achieve in vivo , as a number of parameters are additionally required to interpret the mr signal from a specific spectrum in terms of metabolite concentration . 
a reference mr signal from an external reference standard of known concentration is required , in addition to knowledge of the relaxation parameters of the metabolites of interest [ 20 ]  . 
often , this requires extra scanning time , which may not be feasible in a clinical context , particularly when the mrs examination has been added on to the end of a standard clinical protocol , as in our case . 
however , whereas mrs can obtain information from a large volume within the liver , these discrepancies possibly could be explained by biopsy sampling errors in which only a small tissue sample is obtained for histological characterisation , which may not necessarily be representative of the liver as a whole . 
biopsy at present is taken as the gold standard , but we suggest that the sampling voxel volume used in this study ( 303040 mm ) , which is many times the size of a liver biopsy sample , possibly could reflect a more accurate picture of diffuse hepatic disease . 
moreover , histopathological analysis is a qualitative analysis that evaluates liver architectural distortion due to liver fibrosis that occurs during disease progression and does not quantify liver fibrosis itself [ 21 ]  . 
la quantificazione assoluta dei metaboliti difficile da ottenere in vivo , sopratutto in ambito clinico , poich , oltre a dover determinare il tempo di rilassamento per ciascun metabolita di interesse necessario effettuare acquisizioni spettroscopiche aggiuntive utilizzando uno standard esterno a concetrazione nota [ 20 ]  . 
spesso questo comporta un prolungamento dei tempi di scansione , non sempre possibile in un contesto clinico , in particolare quando lesame spettroscopico eseguito al termine di un protocollo desame standard , come nel nostro caso . 
tuttavia , poich la spettroscopia pu ottenere informazioni relative ad un volume epatico maggiore rispetto a quello valutato dalla biopsia , questa discrepanza pu essere in parte spiegata da errori di campionamento bioptico , dove solo un piccolo campione di tessuto non necessariamente rappresentativo del fegato nel suo insieme , esaminato . 
la biopsia attualmente considerata il gold standard , tuttavia noi suggeriamo che il volume campionato nel nostro studio ( 30 mm30 mm40 mm ) , superiore per dimensioni a quello ottenuto con la biopsia , possa riflettere pi accuratamente il quadro della patologia epatica diffusa . inoltre , lanalisi istopatologica unanalisi qualitativa che non quantifica la fibrosi epatica di per s , ma valuta la distorsione architetturale epatica dovuta alla progressione della fibrosi nel corso della malattia [ 21 ]  . conclusione conclusion in conclusion , based on our data , we suggest that high - field 1h mrs would complement workup of patients with hcv infection in that spectroscopic information can be obtained as a complement to most standard imaging protocols of the liver . 
copetti , via libert 58 , 33010 cassacco , italy , tel . : + 39 - 340 - 2454399 , fax : + 39 - 043 - 3488318 , e - mail : robcopet@tin.it received : 20 february 2007 / accepted : 25 june 2007 / published online : 28 march 2008 springer - verlag 2008 abstract purpose . 
in four patients with negative cxr and positive ultrasound findings , pneumonia was confirmed by chest computed tomography ( ct ) ( performed for recurrent pneumonia in the same location )  . 
in 4 pazienti con radiografia negativa ed ecografia polmonare positiva la polmonite stata confermata dalla tomografia assiale computerizzata ( eseguita per la ricorrenza della polmonite nella medesima sede )  . 
affidabile quanto la radiografia del torace , pu essere ripetuta facilmente al letto del paziente e non espone a radiazioni ionizzanti . parole chiave ecografia polmonare polmonite radiografia del torace consolidamento polmonare ultrasuoni introduction introduzione children and infants with pneumonia may present with a number of clinical symptoms and signs such as fever , cough and tachypnoea . 
a minority of children present with fever la polmonite in bambini e lattanti si manifesta con febbre , tosse e tachipnea , una piccola percentuale di pazienti pu presentare febbre di origine sconosciuta in assenza di sinradiol med ( 2008 ) 113 : 190198 of unknown origin and may have no respiratory symptoms or signs . 
in some cases , radiological examination is necessary , and the chest x - ray ( cxr ) is still considered to be the first imaging step for diagnosing pneumonia in children . 
computed tomography ( ct ) has a high level of accuracy but cannot used as a first - line radiological examination due to high exposure to ionising radiation , availability and cost . 
in adults , lung ultrasonography ( us ) has been shown to be a very promising technique for its high sensitivity in detecting pleural effusion , lung embolism , pneumonia , pneumothorax , alveolar - interstitial syndrome and atelectasis [ 115 ] , whereas there is limited research on this topic in children [ 1621 ]  . 
 certain anatomical characteristics in children , such as a thinner chest wall and smaller thoracic width and lung mass , facilitate us imaging and ensure good - quality images of the lung . 
 [ 22 ] demonstrated that beginners are able to detect the presence of pulmonary interstitial syndrome after fewer than ten examinations and a total training time of 30 min . the aim of this study was to evaluate the ability of us to depict pneumonia in children with clinical signs suggesting lung infection . materials and methods we used a 3.55 mhz convex probe and a high - resolution 7.510 mhz linear probe ( megas cvx , esaote medical systems , florence , italy )  . 
 we examined 79 children admitted to the emergency department with clinical signs suggesting pneumonia ( cough , tachypnea , crackles and / or decreased breath sounds , fever with or without chills , chest and / or abdominal pain ) [ 23 ]  . 
 [ 22 ] hanno dimostrato che la capacit di rilevare la presenza di sindrome alveolo - interstiziale da parte di principianti viene raggiunta dopo meno di 10 esami con un addestramento di 30 minuti . 
 in questo studio abbiamo valutato la capacit dellep di visualizzare la polmonite rispetto alla rx in un campione di pazienti pediatrici con sospetto clinico di polmonite . materiali e metodi stata utilizzata una sonda convex da 3 , 55 mhz ed una lineare ad alta risoluzione da 7 , 510 mhz ( megas cvx , esaote medical systems , firenze , italia )  . 
i campi posteriori sono stati esplorati in decubito laterale ed in posizione seduta [ 2 , 10 ] per lo studio delle aree sottoscapolari e sopraclaveari abbiamo utilizzato una sonda microconvex da 57 , 5 mhz . sono stati studiati 79 bambini giunti al dipartimento di emergenza con segni clinici suggestivi di polmonite ( tosse , tachipnea , rantoli o diminuzione del murmure vescicolare , febbre con o senza brivido , dolore toracico e / o addominale ) [ 23 ] con et compresa fra 6 mesi a 16 anni ( media 5 , 1 anni , sd5 )  . 
a tutti i pazienti con sospetta polmonite stata eseguita una radiografia in proiezione postero - anteriore e , in accordo con le linee guida della british thoracic socurrent pneumonia in the same area to rule out malformations or inhalation of foreign bodies . 
la tc stata eseguita con un apparecchio ge lightspeed multidetector ( general electric , milwaukee , wisconsin , usa )  . risultati anatomia ecografica normale gli strati superficiali del torace sono costituiti dal tessuto sottocutaneo e dai muscoli . 
in nessun paziente con polmonite , il controllo ecografico dopo tre mesi ha dimostrato reperti patologici . reperti ecografici nel bambino la polmonite appare come una area ipoecogena con margini mal definiti e artefatti a coda di cometa compatti posteriori alladdensamento che possono essere presenti anche nelle aree contigue . 
levidenza di aria che si muove in modo sincrono con gli atti respiratori allinterno dei broncogrammi ( broncogrammi aerei dinamici ) testimonia la perviet dei bronchi ed esclude la natura atelettasica del consolidamento . 
artefatti patologici verticali a coda di cometa ( linee b )  . patients among the 79 children with suspected pneumonia on admission , 60 had lung us findings consistent with pneumonia . 
all patients underwent white blood cell count and c - reactive proteneutrophil cell count was increased in 53 patients , whereas c - reactive protein was significantly elevated in all patients with positive us . 
these findings did not , however , influence the diagnosis of pneumonia , which was made according to the clinical findings and imaging pattern . in no patient with confirmed pneumonia were pathological findings observed at 3 months follow - up . us findings in children , pneumonia appears as a hypoechogenic area with poorly defined borders and compact underlying comettail artifacts . 
the sinusoid sign confirms the presence of low viscosity pleural effusion . discussion at present , lung us is not included in the guidelines for diagnosing pneumonia , and cxr is considered to be the gold standard . 
the finding of consolidation on cxr appears to be the most reliable sign for diagnosing pneumonia [ 25 ]  . however , there is significant variation in intraand interobserver agreement among radiologists on the interpretation of the same cxr images and on the radiographic features used for diagnosis [ 25 ]  . 
this was particularly evident in the interprediscussione al momento attuale lep non fa parte delle linee guida per la diagnosi di polmonite e la rx considerata essere lindagine di riferimento . 
nel caso di atelettasia il polmone assume una ecogenicit simile a quella epatica ( epatizzazione ) e nelle fasi in cui non vi sia stato ancora il completo riassorbimento dellaria i broncogrammi aerei presentano un decorso parallelo . 
nel caso di polmonite i radiol med ( 2008 ) 113 : 190198 tation of lung infiltrates and retrocardiac consolidation . in adults , lung consolidations extend to the pleura in 98.5% of cases and can be seen on us [ 15 ]  . 
in atelectasis , the airless lung is similar in echogenicity and echotexture to liver and , before the air has been completely reabsorbed , the air bronchograms appear crowded and parallel . 
lung atelectasis can be definitely excluded if dynamic air bronchograms are present [ 26 ]  . identifying the normal pulmonary vasculature is an indicator of lung consolidation , as vascular architecture is disrupted in the case of a tumour mass [ 27 , 28 ]  . 
finally , a cxr suggesting pneumonia in the absence of respiratory signs or fever may be attributed to the stage of pulmonary infection ( initial or resolving stage ) [ 24 ]  . although neutrophilic leucocytosis and elevated c - reactive protein were not considered significant in distinguishing bacterial from viral infection [ 24 , 29 ] , they may be useful for monitoring patients with a complicated disease course . our data indicate that lung us can be adopted as a simple and noninvasive method for evaluating children with pneumonia . 
we believe that lung us may be used extensively in cases of suspected pneumonia and that a clear clinical picture of pneumonia associated with positive lung us findings excludes the need to perform cxr . 
on the other hand , because the value of lung us for detecting pulmonary consolidation has been demonstrated in adults [ 2 , 6 , 9 , 1315 , 27 , 28 ] , it seems obvious that similar results may be confirmed in the paediatric age . the study did not allow us to determine lung us sensitivity and specificity , as the gold standard is undoubtedly ct , which cannot be routinely used for obvious ethical reasons . us scans were performed by a single expert operator , and it is reasonable to hypothesise that similar results cannot be immediately achieved by less experienced operators . 
however , it should be considered that learning the technique and image interpretation is a relatively simple and fast process . broncogrammi aerei mantengono invece un decorso di tipo arboriforme [ 16 ]  . 
infine una rx compatibile con la diagnosi di polmonite in un soggetto senza segni clinici pu dipendere da una infezione polmonare iniziale o in fase di risoluzione [ 24 ]  . 
 sebbene la leucocitosi neutrofila e lincremento della proteina c reattiva non siano considerati significativi nel distinguere una infezione virale da una batterica [ 24 , 29 ] , possono essere un utile strumento di monitoraggio nei casi con decorso complicato . i nostri dati indicano che lep debba essere considerata uno strumento diagnostico utile per la valutazione dei pazienti pediatrici con sospetta polmonite . 
riteniamo che in futuro lep possa essere estesamente impiegata nei casi di sospetta polmonite e che un quadro clinico suggestivo associato ad una ep positiva escluda la necessit di eseguire la rx . 
daltra parte , poich lutilizzazione dellep per la diagnosi di consolidamenti polmonare stato gi provato nelladulto [ 2 , 6 , 9 , 1315 , 27 , 28 ] , sembra ovvio che simili risultati possano essere confermati anche in et pediatrica . questo studio non permette di definire la sensibilit e la specificit dellep in quanto il vero gold standard indubbiamente la tc , non eseguibile routinariamente per ovvi motivi etici . 
we retrospectively reviewed the ct features of air collections contiguous to the tracheal or main bronchial wall and communicating with the airway in 16 patients undergoing ct for other reasons . 
only one patient had a bronchial diverticulum . the most frequent site was the right posterolateral wall of the trachea at the level of the second or third thoracic vertebral body . 
although chronic inflammatory tracheobronchial changes and increased endoluminal pressure may be important causes , we hypothesise that other , as yet unknown , aetiopathological factors could exist . keywords diverticula trachea bronchi ct airways riassunto obiettivo . 
vengono esaminate retrospettivamente le caratteristiche tc di raccolte aeree contigue alle pareti della trachea e dei bronchi e comunicanti con i rispettivi lumi aerei rilevate in 16 pazienti sottoposti ad esame tc per altra patologia . 
la tc risultata la metodica pi efficace nel valutare sia la presenza che le caratteristiche dei diverticoli . parole chiave diverticoli trachea bronchi tc delle vie aeree 182 introduction air collections contiguous to and communicating with the trachea and main bronchi ( tracheocele and diverticula ) represent an uncommon finding that occurs in approximately 1%2% of cases [ 1 ]  . 
diverticula are typically thin - walled , may be multilobular and range in size from a few millimetres to 34 cthe communicating channel between the air collection and the tracheal wall is always very narrow , with a longitudinal extension ranging from 5 mm in sessile forms to 15 mm in pedunculated masses . 
diverticula must be differentiated from other conditions giving rise to abnormal , well - circumscribed air collections such as bronchogenic cysts , laryngocele , oesophageal diverticula and apical lung hernia [ 1 ]  . 
computed tomography ( ct ) , especially with multidetector technology ( mdct ) , has increased the frequency with which such abnormalities are identified . the aim of this paper is to describe ct signs and clinical presentation of this relatively unknown condition that has rarely been studied from a radiological point of view . materials and methods the ability of volumetric ct scanners to identify previously undetectable alterations has led the authors ( pr , ca ) , both experts in chest ct , to the occasional , though not so infrequent , discovery of diverticular airway malformations . for this reason , 5 , 400 chest ct scans performed for different clinical reasons between june 2001 and june 2003 were retrospectively reviewed . 
among these , we identified 16 patients ( 0.3% of our series ) , ten men and six women , age range 3083 ( mean 55 ) years , with incidental findings of air collections contiguous to the trachea and the main bronchi . the ct studies had been performed to investigate productive cough in six cases , to stage extrathoracic tumours in nine cases without respiratory symptoms and to evaluate possible lung disease in one patient , also without respiratory symptoms , with ulcerative rectocolitis . the scans were acquired with a single - detector spiral ct secura scanner , av e1 ( philips , eindhoven , the netherlands ) and with a multislice ct aquilion 16 scanner ( toshiba medical system , tochigi , japan ) , with a slice thickness 35 mm , a pitch of 1.5 , reconstruction intervals of 2 mm and 3 mm , respectively , followed by sequential high - resolution ( hrct ) scans with 1 - mm slice thickness in seven cases . 
in eight examinations , a remote workstation ( easy vision 4 ) was used to obtain multiplanar ( mpr ) , minimum intensity projection ( minip ) , and volume rendering radiol med ( 2008 ) 113 : 181189 introduzione le raccolte a contenuto aereo contigue ed in comunicazione con la trachea ed i bronchi principali ( tracheoceli e diverticoli ) rappresentano un raro riscontro nelle indagini tc con frequenza non ben determinata , ma valutata in circa l1%2% dei casi [ 1 ]  . 
tipicamente i diverticoli mostrano parete sottile , possono essere plurilobulati e di dimensioni variabili da pochi millimetri e 34 cil tramite tra la raccolta aerea e la soluzione di contiguit della parete tracheale sempre molto sottile con estensione longitudinale variabile tra 5 mm nelle forme con morfologia sessile e 15 mm in quelle con aspetto peduncolato . 
lorigine dal lume aereo tracheale per le esigue dimensioni di difficoltoso rilievo broncoscopico e i diverticoli devono essere differenziati da altre evenienze in cui si riscontrano abnormi immagini di circoscritte raccolte aeree quali le cisti broncogene , i laringoceli , i diverticoli esofagei e le ernie polmonari degli apici [ 1 ]  . 
tra questi sono stati individuati 16 pazienti ( 0 , 3% della nostra casistica ) , 10 maschi e 6 femmine , con et compresa tra 30 ed 83 anni ( media 55 ) e con riscontro occasionale di formazioni a contenuto aereo contigue alla trachea ed ai bronchi principali . 
i pazienti erano stati sottoposti allindagine tc rispettivamente 6 per sintomatologia respiratoria caratterizzata prevalentemente da tosse con espettorazione , 9 per stadiazione di neoplasie extratoraciche , non sintomatici , uno per valutazione di eventuale patologia respiratoria in rettocolite ulcerosa , non sintomatico . le indagini sono state effettuate con tc spirale a singolo detettore ct secura , av e1 ( philips , heindoven , olanda ) e multistrato ct aquilion 16 ( toshiba medical system , tochigi , giappone ) , con spessore di strato compreso tra 3 e 5 mm , pitch 1 , 5 , intervallo di ricostruzione radiol med ( 2008 ) 113 : 181189 ( vr ) reconstructions . 
three patients also underwent fibreoptic bronchoscopy ( fob ) and four cases virtual bronchoscopy ( vb ) , in one case after fob and in another case preceding it . fob alone was performed in one case only . 
the main criterion for the diagnosis of tracheal or bronchial diverticulum was ct or fob evidence of communication between the air collection and the airway . results the clinical and imaging findings are shown in table 1 . 
of patients chronic obstructive pulmonary disease lack of respiratory symptoms computed tomography locations single diverticula multiple diverticula trachea ( right posterolateral wall ) trachea ( left posterolateral wall ) right main bronchus bilateral main bronchi associated signs tracheobronchomegaly ( mounier - kuhn syndrome ) tracheal sabre - sheath deformity bronchiectasis emphysema tabella 1 correlazioni clinico - radiologiche ( 16 pazienti , 30 formazioni diverticolari ) clinica n . 
pazienti bpco assenza di sintomatologia respiratoria localizzazioni tc diverticoli singoli diverticoli multipli trachea ( parete postero - laterale destra ) trachea ( parete postero - laterale sinistra ) bronco principale destro bronchi principali bilaterali segni tc associati tracheobroncomegalia ( sindrome di mounier - kuhn ) deformazione a fodero di sciabola della trachea bronchiettasie enfisema rispettivamente di 2 mm e 3 mm , completate in 7 casi da scansioni sequenziali in alta risoluzione ( hrct ) con spessore di strato di 1 min 4 casi sono state acquisite scansioni mirate con tecnica volumetrica in alta risoluzione ( vhrct ) con spessore di strato di 1 mm , pitch 1 ed intervallo di ricostruzione di 0 , 5 min 8 indagini sono state ottenute con work station remota ( easy vision 4 ) ricostruzioni multiplanari ( mpr ) , minimum intensity projection ( minip ) , volume rendering ( vr )  . 
in 3 pazienti stata eseguita la fibrobroncoscopia ( fb ) e in 4 casi stata eseguita anche endoscopia virtuale ( ve ) , che in un caso ha seguito la fb , in un altro lha preceduta . 
criterio determinante la diagnosi di diverticolo tracheale o bronchiale stato il riscontro tc o fibrobroncoscopico di una comunicazione della raccolta aerea con la via aerea principale . risultati i risultati clinico - radiologici ottenuti sono riportati nella tabella 1 . 
in 13 casi i diverticoli sono risultati unici , in 3 multipli , per un totale di 30 formazioni diverticolari in 16 pazienti , con dimensioni comprese tra 2 mm e 31 mm ( media 16 ) con rapporto maschi : femmine di 2 : 1 e maggior distribuzione nella fascia di et compresa tra 50 ed 83 anni rispetto a quella tra 30 e 50 . in 11 pazienti non erano presenti segni o sintomi riconducibili a patologia respiratoria ed il rilievo di diverticoli stato incidentale . 
in 5 casi era presente broncopneumopatia cronica , con tracheobroncomegalia e bronchiettasie in 2 casi e con deformazione a fodero di sciabola della trachea , bronchiettasie ed enfisema in 3 casi . 
nellunico caso sottoposto a trattamento chirurgico , lesclusione dalla ventilazione del polmone destro ha determinato il collasso totale delle pareti della raccolta aerea comunicante con il bronco principale corrispondente , dimostrandone la non rigidit . 
the diverticula ranged in size from 2 mm to 31 mm ( mean 16 mm ) , were prevalent among men ( 2 : 1 ) and were more common among patients aged 5083 years than among those aged 3050 years . eleven patients had no signs or symptoms of respiratory disease , and the finding was incidental . 
in one case , of a single diverticulum originating from the lower wall of the right main bronchus , we were unable to visualise the 2 - mm orifice on the bronchial wall detected at fob , probably because it lay parallel to the scanning plane ( partial volume effect )  . 
in un caso di diverticolo unico originante dalla parete inferiore del bronco principale destro non stato possibile neppure retrospettivamente visualizzare la soluzione di continuit della parete bronchiale risultata di 2 mm alla fb , verosimilmente perch parallela al piano di scansione ( effetto di volume parziale )  . 
in soli 2 casi la presenza di raccolte aeree paratracheali indeterminate era stata sospettata nellesame radiologico convenzionale del torace . discussione i diverticoli tracheo - bronchiali rappresentano una patologia rara ed infrequentemente diagnosticata , poco indagata nei suoi aspetti semeiologici e nella eziopatogenesi rappresentata da invaginazioni singole o multiple della parete tracheale . 
questa alterazione stata descritta per la prima volta da rokitansky nel 1838 [ 2 ] e la casistica pi ampia stata riportata da goo nel 1999 con 64 casi , con una frequenza autoptica del 1% nei pazienti adulti [ 3 ]  . esistono due tipi di diverticoli , congeniti e acquisiti , con differenze istologiche e di sede . 
quelli congeniti sono pi frequenti nei maschi rispetto alle femmine e sono pi frequentemente localizzati 45 cm al di sotto delle corde vocali e al di sopra della carena , di solito in corrisponfig . 
molteplici orifizi parietali espressione del colletto diverticolare a livello delle pareti tracheali . ticulum in three cases out of four studied with the technique . in only two cases had the presence of indeterminate paratracheal air collections been suggested by conventional chest x - ray . denza della parete laterale destra della trachea , sono piccoli e con tratto di comunicazione molto stretto con la via aerea . 
i diverticoli acquisiti sono presenti a qualsiasi livello , anche se sono pi frequenti lungo la parete postero - laterale e nel tratto di passaggio cervico - toracico della trachea , verosimilmente in rapporto ad un difetto anatomico in questa sede . 
la loro formazione legata ad un aumento della pressione intraluminale che determina lerniazione della mucosa attraverso una porzione pi debole della parete bronchiale , come succede nelle malattie polmonari caratterizzate da tosse cronica , per esempio nella broncopneumopatia cronica ostruttiva . 
la presenza di multipli diverticoli di tipo acquisito pu essere indicativa di tracheobroncomegalia o sindrome di mounier - khun [ 4 , 5 ]  . la diversit tra diverticoli e tracheoceli consiste per alcuni autori [ 6 ] solo nella differenza di numero e dimensioni , con diverticoli come lesioni multiple e con diametro inferiore a 2 cm e tracheocele come lesione singola e con diametro maggiore di 2 cm . normalmente i pazienti non presentano sintomo legati a questa alterazione . 
a volte , invece , possono essere sede di secrezioni con conseguente flogosi cronica della vie aeree [ 7 ] e , se molto grandi , possono determinare disfonia da fig . 
these single or multiple outpouchings of the tracheal wall were first described by rokitansky in 1838 [ 2 ] , and the largest series , 64 cases , was described by goo et al . 
in 1999 , who cited a prevalence at autopsy of 1% in adult patients [ 3 ]  . radiol med ( 2008 ) 113 : 181189 two types of diverticula exist , congenital and acquired , with different histology and location . 
congenital diverticula are more common in men and tend to arise on the right tracheal wall 45 cm below the vocal cords above the carina . they are usually very small , with a very narrow communication with the airway . 
acquired diverticula may arise at any level , although they are more frequent along the posterolateral wall and at the tracheal cervicothoracic junction , possibly as a result of an anatomical defect at this site . 
their development is related to increased intraluminal pressure and mucosal herniation through a weakened portion of the bronchial wall , as occurs in diseases characterised by chronic cough , such as chronic obstructive pulmonary disease . 
the difference between tracheal diverticula and tracheocele , according to some authors [ 6 ] , is only a matter of number and size , with diverticula being multiple lesions with a diameter smaller than 2 cm and tracheocele being a single lesion larger than 2 cm . tracheal diverticula are normally asymptomatic . 
however , they can act as a reservoir for secretions leading to chronic tracheobronchial infections [ 7 ] and , if very large , may cause dysphonia as a result of compression and paralysis of the recurrent laryngeal nerve or produce a vagal nerve stimulation with cough , dyspnoea and dysphagia . 
in symptomatic patients in our review , however , symptoms were nonspecific , such as cough ( 70% ) and blood - tinged sputum ( 5% ) , and may have been part of the overall picture of chronic obstructive pulmonary disease [ 8 ]  . 
only in one case of a large right paratracheal diverticulum did the patient report a sensation of foreign object in the right infraclavicular region ; clinical findings in this case included a soft swelling that hardened during a valsalva manoeuvre and exacerbation of cough on lying down . in our series , no close cause - and - effect relationship was identified between chronic obstructive pulmonary disease , present in five out of 16 ( 33% ) patients only , and tracheobronchial diverticula . 
the finding in 2 / 3 of cases of diverticula in completely asymptomatic patients as well as the high prevalence of lesions at the junction between cartilaginous and membranous portions of the upper intrathoracic trachea compressione e paralisi del nervo ricorrente o essere causa di stimolazione vagale con presenza di tosse , dispnea e disfagia . 
comunque nei casi di pazienti con sintomatologia respiratoria non si riscontrata specificit sintomi quali la tosse ( 70% ) e lescreato striato di sangue ( 5% ) potendo essi far parte del quadro complessivo di broncopneumopatia cronica ostruttiva [ 8 ]  . 
in un unico caso di voluminoso diverticolo paratracheale destro stata riferita sensazione di ingombro infraclaveare destro con rilievo clinico di tumefazione soffice che incrementava di consistenza nella manovra di valsalva ed esacerbazione della tosse in clinostatismo . nei casi da noi descritti non stata documentato uno stretto rapporto causale tra broncopneumopatia cronica ostruttiva , presente in soli 5 pazienti su 16 ( 33% ) , e diverticoli tracheo - bronchiali . 
comunque il riscontro che la quasi totalit dei diverticoli in pazienti non affetti da altra patologia bronco - polmonare origini comunque dalla parete postero - laterale destra della trachea in corrispondenza della ii e iii vertebra toracica , induce a ritenere che a tale livello esistano anche delle altre condizioni di ordine anatomico non acquisite favorenti la estroflessione della mucosa [ 5 , 9 ]  . 
la molto minor frequenza di diverticoli originanti dalla parete postero - laterale sinistra potrebbe trovare spiegazione dalla stretta vicinanza a livello dellinlet dellesofago e da un suo possibile effetto tampone [ 3 ]  . 
sono quindi auspicabili studi anatomici e fisiopatologici al fine di determinare lesistenza di un eventuale locus minoris resistentiae a livello soprattutto del tratto di giunzione tra pars membranacea e pars cartilaginea della trachea nel suo tratto intratoracico iniziale e il ruolo non ben definito e comunque non prevalente della broncopneumopatia cronica ostruttiva nella formazione delle estroflessioni diverticolari [ 8 ]  . la tc risultata metodica efficace nel valutarne la presenza , il numero e le dimensioni . 
nella quasi totalit dei casi la tc , evidenziando il tramite come sottile soluzione di continuit della parete tracheale , ne ha consentito una attribuzione anatomica differenziando il diverticolo tracheale da laringoceli o diverticoli esofagei [ 10 , 11 , 12 ]  . 
la tc pu contribuire efficacemente anche alla individuazione di eventuali complicanze quali flogosi o perforazioni delle pareti , teoricamente possibili , ma non riscontrate in nessun caso descritto [ 13 ]  . 
however , the fact that almost all diverticula seen in patients not affected by other bronchopulmonary disease originated from the right posterolateral tracheal wall at the second and third thoracic vertebra implies the presence of other , nonacquired , anatomical conditions that might facilitate the outpouching of mucosa at that site [ 5 , 9 ]  . 
further anatomical and pathophysiological studies are therefore needed to ascertain the existence of a possible locus minoris resistentiae , mainly at the junction of membranous and cartilaginous portions of the upper intrathoracic trachea , and the role of chronic obstructive pulmonary disease in diverticula formation [ 8 ]  . ct proved to be an effective technique in evaluating the presence , number and size of tracheal diverticula . 
in almost all cases , by demonstrating the narrow communication through the tracheal wall , ct enabled anatomical characterisation and differentiation of tracheal diverticula from laryngocele or oesophageal diverticula [ 10 , 11 , 12 ]  . 
furthermore , the high - resolution technique allows detection of the typical signs of chronic obstructive pulmonary disease , such as emphysema , bronchiectasis and changes in tracheal morphology [ 14 ]  . the small number of correlations between ct and fob do not allow us to establish the diagnostic roles of the techniques , although ct appears to be superior , above all in cases where the diverticula origin is small and oriented in an opposite direction to the endoscopic view [ 15 ]  . 
the use of contrast material was not influential due to the lack of enhancement of the structures examined and the considerable difference in natural contrast between lesions and anatomical structures in the region . 
mpr and vr techniques have been shown to improve the spatial evaluation of lesions [ 16 ]  . air collections in the paratracheal region need to be differentiated from laryngocele and pharyngocele , zenker diverticulum , apical lung hernia and bullae due to paraseptal emphysema . 
although barium studies of the digestive tract may aid differentiation from pharyngocele and zenker diverticulum , the possibility of assessing longitudinal intrathoracic structures by mdct has facilitated the differential diagnosis of lesions at this level [ 4 , 11 ]  . although no complications were identified in our series , there is a known risk of mucous plugging leading to infections [ 17 , 18 ]  . 
there are no reports of rupture of the diverticular walls , with secondary pneumomediastinum , whereas a single case of airway exclusion by the diverticulum has been reported in a newborn [ 19 ]  . treatment is only surgical and aimed at preventing complications [ 1 ]  . 
5 le dimensioni dei diverticoli possono essere anche molto piccole . evidente lorigine dal punto di giunzione ideale tra pars membranacea e pars cartilaginea della trachea . il limitato numero di correlazioni tra tc e fb non consentono una definizione del loro ruolo diagnostico anche se la tc sembrerebbe superiore soprattutto in quei casi in cui lorigine dei tramiti diverticolari sia di piccole dimensioni ed orientata nel senso opposto alla visione endoscopica [ 15 ]  . 
la somministrazione del mezzo di contrasto risultata non influente sia per lassenza di contrast enhacement delle strutture anatomiche esaminate , sia per lelevata differenza di contrasto naturale tra le lesioni e le strutture anatomiche della regione . 
 la presenza di una raccolta aerea in regione paratracheale necessita di diagnosi differenziale per eludere laringoceli e faringoceli , diverticolo di zencher , ernia di un apice polmonare e bolle in enfisema parasettale . 
sicuramente lo studio delle vie delle vie digestive con bario pu aiutare in caso di faringocele e diverticolo di zencher , ma la possibilit di studiare le strutture intratoraciche a decorso longitudinale con la mdct ha facilitato la diagnosi differenziale delle lesioni a questo livello [ 4 , 11 ]  . 
 sebbene nella nostra casistica non siano stati documentati allatto dellindagine fattori complicanti i diverticoli conosciuta la possibilit di ristagni mucosi nel loro lume con possibilit di infezioni [ 17 , 18 ]  . 
descritto un unico caso in et neonatale di esclusione della via aerea per intubazione del tramite diverticolare [ 19 ]  . il trattamento pu essere solo chirurgico al fine di prevenire complicanze [ 1 ]  . 
nella nostra casistica ci si verificato in un unico caso di diverticolo bronchiale contestualmente ad apicectomia sinistra per bolle di enfisema deterradiol med ( 2008 ) 113 : 181189 verticulum was treated surgically during left apicectomy for bullae causing recurrent spontaneous pneumothorax . 
nei due casi di voluminosi diverticoli multipli tracheali e bronchiali in tracheobroncomalacia ( sindrome di mounier - kohun ) le condizioni di insufficienza respiratoria non hanno consentito opzioni chirurgiche [ 8 ]  . 
maria delle croci , v.le randi 5 , 48100 ravenna , italy 2istituto di radiodiagnostica , universit degli studi di ferrara , corso della giovecca 203 , 44100 ferrara , italy correspondence to : g.c. 
between january 2000 and december 2006 , 42 patients ( nine women and 33 men , age range 4587 years ) treated by endovascular renal artery stenting were studied with cdus . 
in the remaining ten patients ( 23.8% ) , who had no signs of severe nephropathy , angiography confirmed the cdus findings of in - stent restenosis in all cases . 
nei restanti 10 pazienti ( 23 , 8% ) , che non presentavano segni di severa nefropatia , il reperto ecd di ristenosi a livello dello stent stato confermato in tutti i casi . 
lecd svolge un ruolo fondamentale nel monitoraggio dei pazienti sottoposti a rivascolarizzazione dellarteria renale mediante posizionamento di stent , consentendo una diagnosi precoce di ristenosi ed una valutazione della nefropatia spesso associata alla stenosi dellarteria renale ( sar )  . 
lecd fornisce elementi essenziali alla successiva gestione terapeutica di questi pazienti . radiol med ( 2008 ) 113 : 242248 keywords color doppler sonography nephrographyc hypertension stent renal artery parole chiave eco - color doppler ipertensione nefrovascolare stent arterie renali introduction introduzione renal artery stenosis ( ras ) is most common in elderly subjects with associated systemic disease such as arterial hypertension , diabetes and dyslipidaemia . 
it is predominantly caused by atheromatous plaque ( 90% ) progressing into the renal artery from the aortic wall , resulting in stenosis that prevalently involves the ostial renal artery ( within 510 mm from the aorta lumen ) [ 1 ]  . 
in ostial ras not associated with severe nephropathy , the treatment of choice is revascularisation by endovascular stent placement , which prevents plaque recoil and allows for improved primary patency at 12 months compared with percutaneous transluminal angioplasty ( pta ) [ 2 ]  . 
stent restenosis , often due to fibrointimal hyperplasia , usually arises 312 months after the revascularisation procedure , with an incidence between 8% and 25% [ 3 ] , and may be silent until the development of massive thrombosis , which occurs in about 15% of patients [ 4 ]  . 
in the light of these data , there is a need for a noninvasive , reliable and repeatable modality capable of monitoring these patients over time . color - doppler ultrasonography ( cdus ) of the renal arteries is the principal screening tool used to detect ras , with many international studies reporting sensitivity and specificity values of 83%96% and 76%98% , respectively [ 513 ]  . 
the advantages of the technique are its noninvasiveness , repeatability , low cost and good negative predictive value when used in selected populations , whereas its known limitations are operator dependence , obesity , bowel gas and vascular abnormalities , especially anatomical variants of the renal artery [ 6 , 1317 ]  . the purpose of this study was to assess the role and reliability of cdus in the follow - up of patients after renal artery stenting and , more specifically , in enabling early detection of flow changes indicative of restenosis in order to intervene with a further endoluminal revascularisation procedure . materials and methods between 2000 and 2006 , we studied 42 patients ( nine women and 33 men ) , aged 4587 years , who underwent renal artery stenting for haemodynamically significant stenoses without signs of severe nephropathy ( longitudinal renal diameter > 9 cm , intrarenal arterial resistive index < 0.8 , parenchymal thickness > 1 cm , adequate renal vascularity on colorand power - doppler imaging ) detected on cdus . 
during the follow - up , patients were examined by a single operator with philips ssd 800 and ge logic 7 pro la stenosi dellarteria renale ( sar ) , pi frequente in soggetti anziani con patologie sistemiche correlate quali ipertensione arteriosa , diabete e dislipidemie , dovuta nella maggior parte dei casi alla presenza di placche ateromasiche ( 90% ) , che protrudendo dalla parete aortica allinterno dellarteria renale determinano restringimento del lume , prevalentemente in sede ostiale ( entro 510 mm dal lume aortico ) [ 1 ]  . 
il trattamento delezione nelle forme ostiali , in assenza di severa nefropatia , prevede attualmente la rivascolarizzazione mediante il posizionamento per via endoluminale di uno stent , in grado di prevenire il recoil della placca , migliorando , nei confronti della pta , la perviet primaria a 12 mesi [ 2 ]  . la ristenosi su stent , dovuta spesso a iperplasia fibrointimale , avviene di solito a 312 mesi dallintervento di rivascolarizzazione con un tasso di incidenza tra l8% e il 25% [ 3 ] e pu essere silente in circa 15% dei pazienti , fino allo sviluppo di trombosi massiva [ 4 ]  . 
alla luce di queste osservazioni , diviene necessario individuare una metodica poco invasiva , affidabile e ripetibile , in grado di monitorare nel tempo questi pazienti . attualmente lecd delle arterie renali risulta la principale metodica di screening nella diagnosi di stenosi della arteria renale con numerosi studi in ambito internazionale che attribuiscono a tale metodica valori di sensibilit pari all83%96% e di specificit del 76%98% [ 513 ]  . 
i vantaggi della metodica sono rappresentati dalla non invasivit , ripetibilit , basso costo e buon valore predittivo negativo se eseguito in popolazione selezionata , mentre i limiti riconosciuti sono loperatore - dipendenza , lobesit , il meteorismo e le anomalie vascolari , con particolare riguardo alla presenza di varianti anatomiche dellarteria renale [ 6 , 1317 ]  . scopo del nostro studio valutare il ruolo e laffidabilit dellecd nel follow - up del paziente sottoposto ad intervento di rivascolarizzazione mediante posizionamento di stent in arteria renale , con lintento di svelare precoci alterazioni flussimetriche , indicative di ristenosi e poter attuare cos un eventuale ulteriore intervento di rivascolarizzazione endoluminale . materiali e metodi nel periodo 20002006 sono giunti alla nostra osservazione 42 pazienti ( 9 donne e 33 uomini ) , di et compresa tra 244 radiol med ( 2008 ) 113 : 242248 ultrasound units equipped with colorand power - doppler modules and a 3.5 - mhz convex - array transducer . 
examinations aimed at evaluating stent patency , in - stent flow profile and overall renal haemodynamics ( intrarenal arterial resistive index , hilar and parenchymal flow )  . in accordance with the literature , haemodynamically significant lesions suspicious for in - stent restenosis were defined by peak systolic velocity ( psv ) ( cid : 2 ) 200 cm / s ( with angle < 60 ) at the stent level , parvustardus pulse pattern in the hilar region and / or in the segment below the stent , turbulence and aliasing . 
of these , three patients did not undergo angiography due to ischaemic nephropathy deterioration ( cdus evidence of shrunken kidney , longitudinal renal diameter < 9 cm , renal insufficiency ( ri ) > 0.8 and poor parenchymal vascularity on color - doppler and powerdoppler imaging )  . two patients had been treated with talent endovascular stent - grafts for exclusion of an abdominal aorta aneurysm at the bifurcation level ; one patient had been treated with a stent - graft to exclude an aortic aneurysm 3 years after the revascularisation procedure . 
restenosis in these patients was caused by in - stent intimal hyperplasia ( six patients ) , formation of a preor poststent atheroma ( three patients ) and a combination of the above factors ( one patient )  . 
in 19% ( eight patients ) of cases studied by cdus , the restenoses arose within 1 year of stent placement ( two at 4 months ; one at 5 months ; two at 9 months ; one at 11 months ; two at 12 months )  . 
among all 42 patients who underwent angiography , only one showed clinical , laboratory and biopsy evidence of cholesterol atheroembolism after the interventional procedure . cdus yielded one false positive case : in this patient , who had already undergone repeat revascularisation 5 months earlier due to cdus evidence of in - stent restenosis , the stent protruded into the aortic lumen generating high 4587 anni , sottoposti ad intervento di rivascolarizzazione dellarteria renale mediante posizionamento di stent in quanto portatori di stenosi emodinamicamente significativa allecd , in assenza di segni di grave nefropatia ( diametro longitudinale renale > 9 cm , indice di resistenza arterioso intrarenale < 0 , 8 , spessore parenchimale > 1 cm , sufficiente vascolarizzazione renale al cd e power doppler )  . 
i pazienti , successivamente sottoposti a follow - up , sono stati esaminati da un unico operatore con apparecchiatura ecografica philips ssd 800 e ge logic 7 pro , con utilizzo di sonda convex 3 , 5 mhz con modulo color e power doppler , ed stata valutata la perviet , il profilo flussimetrico a livello dello stent nonch lemodinamica renale globale ( indice di resistenza arterioso intrarenale , flusso ilare e parenchimale )  . in accordo coi dati di letteratura , abbiamo definito alterazioni emodinamicamente significative , sospette per la presenza di ristenosi a livello dello stent , la presenza di : velocit del flusso in fase sistolica ( psv ) ( cid : 2 ) 200 cm / s ( con angolo < 60 ) a livello dello stent , polso parvus et tardus in sede ilare e / o nel tratto a valle lo stent , turbolenze , fenomeno di aliasing . 
di questi , 3 pazienti non sono stati sottoposti ad angiografia per peggioramento della nefropatia ischemica ( presenza al ecd di rene grinzo , diametro longitudinale renale < 9 cm , ir > 0 , 8 e scarsa vascolarizzazione parenchimale al cd e power doppler )  . due pazienti erano stati trattati con protesi endovascolare tipo talent per esclusione di aneurisma dellaorta addominale a livello della biforcazione ed un paziente , dopo 3 anni dallintervento di rivascolarizzazione dellarteria renale , stato trattato con endoprotesi per esclusione dellaneurisma aortico . 
i restanti 10 pazienti ( 23 , 8% ) , che non presentavano segni ecd di severa nefropatia , sono stati sottoposti ad angiografia che ha confermato in 10 pazienradiol med ( 2008 ) 113 : 242248 fig . 
b alterazioni emodinamicamente significative in presenza di ristenosi dello stent in arteria renale destra : aspetto ecd . psv flows and turbulence that were incorrectly interpreted as evidence of restenosis . discussion ras is an increasingly common finding , particularly in the course of angiographic studies performed to identify peripheral or coronary vascular disease in elderly subjects affected by arterial hypertension , dyslipidaemia and diabetes . 
currently , the treatment of choice for ostial ras is endovascular stent placement that provides better 12 - month patency rates [ 2 ] compared with transluminal angioplasty and reduces the incidence of restenosis . 
given that approximately 15% of restenoses are silent [ 4 ] , our study aimed at assessing the role of cdus as a noninvasive and repeatable examination in the follow - up of patients with renal artery stents . 
more specifically , we evaluated its ability to detect flow alterations indicative of restenosis and prevent ischaemic nephropathy and renovascular hypertension by permitting a timely repeat revascularisation procedure . the diagnostic value of the other available imaging modalities such as computed tomography ( ct ) angiography and magnetic resonance ( mr ) angiography is in part limited by the presence of artefacts related to the stent - graft material [ 18 ]  . 
in particular , mr angiography , a noninvasive examination that is also indicated in patients with ri , is unable to image the stents - grafts currently used because the ferromagnetic material substantially reduces the signal at the stent level . 
in questi pazienti la ristenosi era causata da iperplasia intimale intra - stent ( 6 pazienti ) , dallo sviluppo di placca aterosclerotica preo post - stent ( 3 pazienti ) e per la concomitante presenza delle due cause sovraesposte ( 1 paziente )  . 
di tutti i 42 pazienti sottoposti ad angiografia solo in 1 caso erano presenti dopo la procedura interventistica segni clinico - laboratoristici e bioptici di ateroembolismo colesterinico . vi stato un falso positivo allecd : in questo paziente , gi sottoposto a re - intervento di rivascolarizzazione 5 mesi prima per riscontro ecd di ristesosi a livello dello stent , questo protrudeva nel lume aortico creando flussi con elevati vps e turbolenze che sono stati erroneamente interpretate come ristenosi . 
 discussione il riscontro di stenosi dellarteria renale sempre pi frequente , in particolare in corso di indagini angiografiche per ricerca di patologie vascolari periferiche o coronariche , prevalentemente in soggetti anziani , affetti da ipertensione arteriosa , dislipidemie e diabete . 
b ripristino della perviet in arteria renale destra : aspetto agiografico . stent itself and calcified plaque having similar attenuation to the contrast agent , leading to misinterpretation of the extent of possible restenosis . 
new multislice ct technology , despite producing images with high spatial resolution thanks to isotropic voxels and volumetric postprocessing software ( maximum intensity projection , volume rendering ) with dedicated filters for the study of stents [ 19 ] , exposes the patient to a higher radiation dose . 
this , combined with the nephrotoxicity of iodinated contrast media , contraindicates its use as a first - line modality in the follow - up of patients with impaired renal function . several studies have demonstrated the reliability of sonographic parameters such as the psv acceleration index , parvus - tardus pulse pattern and the renal aortic ratio ( rar : renal psv / aortic psv ) for detecting haemodynamically significant ras subsequently confirmed by angiography [ 18 , 20 , 21 ]  . 
because the rar may be affected by aortic pressure changes in the presence of aneurysms , atherosclerosis or cardiac insufficiency , a psv > 200 cm / s and the parvus - tardus pulse pattern below the stent should be used as the principal indicators of restenosis . 
poich circa il 15% delle ristenosi pu essere silente [ 4 ] , lo scopo del nostro studio stato di valutare il ruolo dellecd , quale esame non invasivo e ripetibile , nel follow - up di pazienti portatori di stent dellarteria renale , per individuare precocemente alterazioni flussimentriche indicative di ristenosi e prevenire cos linsorgere di nefropatia ischemica ed ipertensione nefrovascolare , attraverso un tempestivo intervento di rivascolarizzazione . il valore diagnostico di altre indagini di imaging disponibili , quali angio - tc e angio - rm , in parte gravato dalla presenza di artefatti dovuti al materiale protesico dello stent [ 18 ] ; in particolare langio - rm , indagine poco invasiva ed indicata anche in pazienti con insufficienza renale , non in grado di studiare gli stent attualmente in uso , costituiti da materiale ferromagnetico che riduce nettamente il segnale a livello dello stent . 
langio - tc in parte condizionata nel valutare il lume dello stent da artefatti di indurimento del fascio dovuti allo stent stesso e ad eventuali placche calcifiche che non presentano significative differenze di densit rispetto al mdc , portando quindi a misconoscere o mal valutare lentit della eventuale restenosi . 
le nuove tc multislice , nonostante producano immagini ad elevata risoluzione spaziale grazie a voxel isotropici e software di rielaborazione volumetrica ( mip , vr ) con lutilizzo di filtri dedicati per lo studio degli stent [ 19 ] , comportano un aumento della dose radiante che , insieme alla nefrotossicit del mezzo di contrasto iodato , non la rendono consigliabile come indagine di prima istanza nel follow - up in pazienti con funzionalit renale in labile compenso . 
 diversi studi hanno dimostrato una buona affidabilit di parametri ecografici , quali lindice di accelerazione del picco sistolico ( psv ) , il polso parvus et tardus ed il rapporto reno - aortico ( rar : psv renale / psv aortica ) nel riscontro di stenosi emodinamicamente significative a livello dellarteria renale , confermate poi da esame angiografico [ 18 , 20 , 21 ]  . 
poich il rar pu essere influenzato da alterazioni pressorie a livello dellaorta in presenza di aneurismi , patologia aterosclerotica o insufficienza cardiaca , il psv > 200 cm / s e l effetto parvus et tardus nel tratto a valle dello stent dovrebbero essere usati come principali indici di ristenosi . 
in particolare i dati di letteratura indicano che il psv ha sensibilit elevata ( 97%100% ) e specificit che cresce sensibilmente con laumento del cut - off dal 15% ( psv > 125 cm / s ) fino a raggiungere il 79% di specificit ( psv > 200 cm / s ) cui corrisponde valore predittivo negativo del 95% [ 18 , 20 , 21 ]  . nella nostra casistica , lesame ecd ha rilevato in 13 pazienti su 42 stenosi emodinamicamente significative in corrispondenza dello stent con presenza di polso parvus et tardus nel tratto a valle dovuto , nella maggior parte , radiol med ( 2008 ) 113 : 242248 ous reports indicated that psv has a high sensitivity ( 97%100% ) and a specificity that increases substantially as the psv cutoff point is increased from 15% ( psv > 125 cm / s ) to 79% ( psv > 200 cm / s ) corresponding to a negative predictive value of 95% [ 18 , 20 , 21 ]  . in our series , cdus detected haemodynamically significant stenoses of the stent with a parvustardus pulse pattern below the stent in 13 of 42 patients ; in most cases , restenosis was due to fibrointimal hyperplasia ( seven cases ) or atheromas ( four cases ) located proximally or distally to the stent . three cases had rapid progression of ischaemic nephropathy ( longitudinal renal diameter < 9 cm , re > 0.8 , parenchymal thickness < 1 cm ) , which contraindicated a further revascularisation procedure . 
this finding emphasises the importance of an overall assessment of renal haemodynamics when considering revascularisation in untreated patients or in patients who have already undergone renal artery stenting for ras . angiography confirmed the haemodynamically significant stenosis of the renal artery in all cases detected on cdus , allowing pta revascularisation during the same session and coaxial stent placement where necessary . 
cdus produced one false positive case due to a stent protruding into the aortic lumen and creating flows with high turbulence and acceleration , which were incorrectly interpreted as restenosis in a patient who had undergone a revascularisation procedure 5 months earlier ; this was correctly detected by cdus . 
in these cases , monitoring of alternative parameters ( parvus - tardus pulse pattern , intraparenchymal ri ) may become crucial for revealing flow variations suspicious for restenosis in difficult cases . conclusions our study confirms the existing literature that recognises cdus as a reliable modality when performed by expert operators in studying primary renal artery stenosis and in the subsequent follow - up of patients after stent placement [ 22 ]  . in contrast to other imaging modalities such as ct angiography and mr angiography , in the monitoring of patients after endoluminal revascularisation by stent placement , cdus is a safe and repeatable technique that can detect haemodynamically significant lesions early on and thus help the decision making process regarding subsequent diagnostic and therapeutic management . the importance of ri in influencing the survival of patients with ras is well known [ 23 ]  . 
this fact and our experience indicate a need to identify a noninvasive method for monitoring patients with renal artery stents to provide clinicians with relevant information for deciding on the correct clinical and therapeutic approach . alla presenza di iperplasia fibrointimale ( 7 ) o a placche aterosclerotiche ( 4 ) site prossimalmente o distalmente rispetto allo stent . 
in 3 casi si avuta rapida evoluzione della nefropatia ischemica ( diametro longitudinale renale < 9 cm , ir > 0 , 8 , spessore parenchimale < 1 cm ) che ha sconsigliato il ricorso allintervento di ulteriore rivascolarizzazione . 
questo aspetto sottolinea inoltre limportanza della valutazione globale dellemodinamica renale qualora si prospetti un intervento di rivascolarizzazione in pazienti non trattati o gi sottoposti a stent dellarteria renale per sar . lesame angiografico ha confermato una ristenosi emodinamicamente significativa dellarteria renale in tutti i pazienti individuati allecd , consentendo lintervento di rivascolarizzazione nella stessa seduta mediante pta ed eventuale posizionamento di uno stent coassiale . 
vi stato 1 falso positivo allecd dovuto allo stent che protrudendo nel lume aortico ha creato flussi ad elevate turbolenze ed accelerazioni , erroneamente interpretati come ristenosi in paziente che 5 mesi prima era stato sottoposto ad intervento di rivascolarizzazione correttamente rilevato allecd . 
in questi casi il monitoraggio di parametri alternativi ( polso parvus et tardus , ir intra - parenchimale ) possono assumere importanza rilevante in pazienti difficili nello svelare variazioni flussimetriche che risultino sospette per ristenosi . conclusioni il nostro studio conferma i dati di letteratura che riconoscono lecd come metodica affidabile , quando eseguita da operatori esperti , nello studio delle stenosi primitiva dellarteria renale e nel successivo follow - up dopo posizionamento di stent [ 22 ]  . 
a differenza di altre metodiche di imaging , quali angio - tc ed angio - rm , lecd indagine sicura e ripetibile nel monitoraggio dei pazienti sottoposti a trattamento endovascolare di rivascolarizzazione mediante stent , in grado di diagnosticare precocemente alterazioni emodinamicamente significative cos da poter decidere il successivo iter diagnostico e terapeutico . limportanza dellinsufficienza renale nel determinare la prognosi quoad vitam dei pazienti con sar nota in letteratura [ 23 ]  . 
ultrasonography , negative in 18 patients , identified 26 cases of ductal ectasia ( 12 simple , nine with solid intraductal echoes and wall thickening , five with inhomogeneous parenchyma )  . 
five papillomatoses appeared as patchy , homogeneous enhancing areas , 15 intraductal papillomas as areas with well - defined margins and type ii time - intensity curves , and two atypical ductal hyperplasias as diffuse nodular enhancement . 
lecografia negativa in 18 casi , identificava ectasia duttale in 26 : semplici in 12 , con proliferazione solida intraduttale ed ispessimento parietale in 9 e con disomogeneit ghiandolare in 5 ; la galattografia negativa in 3 e positiva in 9 . 
cinque papillomatosi duttali si identificavano come potenziamento lineare ed omogeneo ; 15 papillomi : enhancement a margini netti e curva intensit - tempo di tipo ii , 2 iperplasie duttali atipiche : potenziamento nodulare diffuso . 
un carcinoma papillare , 1 cdis con aspetto micropapillare e 1 cdi si evidenziavano come 2 aree di potenziamento segmentale e unarea di potenziamento nodulare a margini irregolari ( bi - rads4 )  . 
breast mri can be considered a valuable examination in the diagnosis of suspected ductal disease and an alternative to galactography when the latter cannot be used . keywords nipple discharge breast mri diagnosis ductal disease duttale con secrezione , in alternativa alla galattografia quando questa metodica non sia utilizzabile . parole chiave secrezione dal capezzolo mammella risonanza magnetica diagnosi patologia duttale introduction introduzione pathological nipple discharge is defined as a spontaneous secretion from the breast unrelated to physiological conditions such as pregnancy and lactation [ 1 ]  . 
another less common but important cause is breast cancer , in which the secretion is frequently bloody or serosanguineous , a symptom encountered in 5%21% of cases [ 57 ]  . diagnostic imaging plays a fundamental role in the study of patients with nipple discharge . 
these findings , which are not consistently detectable on galactography , may be identified in both benign and malignant breast lesions , a fact that makes the differential diagnosis relatively difficult . moreover , galactography is an invasive examination that requires placement of a cannula and introduction of contrast material in the duct [ 5 ]  . 
this may be due to the small size of the masses being examined , the absence of calcification and the predominantly intraductal growth of the lesions [ 13 ]  . 
the method has a high sensitivity for detecting intraductal lesions when used by radiologists experienced in breast imaging [ 14 , 15 ]  . in recent years breast magnetic resonance imaging ( mri ) has taken on a crucial role in diagnosing invasive breast cancer as a result of its high sensitivity ( 94%100% ) and specificity ( 37%97% ) [ 16 , 17 ]  . 
it is also considered a useful diagnostic tool in selected cases , in particular for clarifyla secrezione dal capezzolo di tipo patologico viene descritta come una secrezione mammaria spontanea , non associata a condizioni fisiologiche come gravidanza o allattamento [ 1 ]  . il secreto pu essere di natura sierosa , siero - ematica , ematica o purulenta [ 2 ]  . 
in questultima condizione , la secrezione risulta frequentemente essere di tipo ematico o siero - ematico , sintomo che si manifesta con una frequenza che si aggira tra il 5% ed il 21% dei casi [ 57 ]  . fondamentali risultano quindi , le differenti metodiche di diagnostica per immagini nello studio di pazienti con secrezione dal capezzolo . 
i reperti di pi frequente riscontro sono caratterizzati dalla presenza di : dilatazione duttale , difetto di riempimento o completa ostruzione di un dotto e lirregolarit parietale del dotto stesso [ 1012 ]  . 
la galattografia inoltre risulta un esame invasivo perch richiede , previo incannulamento di un dotto lattifero , lintroduzione di mezzo di contrasto ( mdc ) nello stesso [ 5 ]  . 
lintegrazione diagnostica con esame mammografico pu rivelarsi di ridotta utilit , in quanto frequentemente i reperti risultano del tutto negativi , soprattutto nelle pazienti con patologia di natura benigna , come ad esempio per il papilloma intraduttale . 
questa metodica infatti presenta una elevata sensibilit nella diagnosi di lesione intraduttaradiol med ( 2008 ) 113 : 249264 ing doubtful results from other breast imaging studies , identifying breast cancer recurrences and studying women with breast implants . 
whereas the role of mri in detecting clinically and mammographically occult breast cancers is established , few studies have investigated its diagnostic value in relation to intraductal disorders that are occult on commonly used imaging modalities : for example , ductal carcinoma in situ ( dcis ) and benign lesions such as solitary intraductal papilloma and papillomatosis [ 1820 ]  . 
a few studies have emphasised the importance of mri in the differential diagnosis between breast papillomas and malignancies with an intraductal component , especially in cases where other modalities have failed to provide a definitive diagnosis of the nature of the lesion [ 21 , 22 ]  . the aim of our work was to evaluate the diagnostic potential of breast mri in studying patients with bloody or serosanguineous nipple discharge by comparing mri with galactography , mammography and ultrasonography . materials and methods between february 2005 and august 2006 , 43 women and one man , aged between 28 and 65 ( mean 42 ) years with bloody or serosanguineous single - duct nipple discharge were studied by breast mri . 
all patients underwent a preliminary us study at our department , using siemens antares or aloka prosound ssd - 5500 units with high - frequency ( 7.510 , 1013 mhz ) linear - array transducers for superficial tissues . 
twelve patients underwent galactography ; in the remaining 32 , the examination could not be carried out owing to inability to cannulate the duct ( n = 9 ) , contrast leakage ( n = 8 ) and patient refusal to undergo the examination ( n = 15 )  . the mri study was performed with a 1.5 - tesla magnet ( magnetom vision , siemens , erlangen , germany ; gradients 25 mt / m2 , slew rate 800 t / m / s , rise time 400 s ) equipped with a double breast coil . 
the examination was carried out with standard sequences for breast study : t2 - weighted short - tau inversion recovery ( stir ) sequences in the axial plane ( tr / te 6 , 690 / 74 ; slice thickness 3.5 mm ; fov 2828 cm ) and t1 - weighted 3d fast low - angle shot ( flash ) sequences ( tr / te 14 / 7 ; flip angle : 25 ; slice thickness 1.96 mm without gap ; matrix 192256 ; fov 3055 cm ) in the sagittal and axial planes . 
the first involves acquisition of axial t2 - weighted sequences to oble , soprattutto se utilizzata da radiologi con particolare esperienza nellambito senologico [ 14 , 15 ]  . negli ultimi anni la risonanza magnetica ( rm ) mammaria ha assunto un ruolo di fondamentale importanza nella diagnosi del carcinoma invasivo del seno , in virt della sua elevata sensibilit ( 94%100% ) e specificit ( 37%97% ) [ 16 , 17 ]  . 
risulta inoltre un utile strumento diagnostico in alcuni casi selezionati , in particolare : per la risoluzione di casi dubbi alle altre indagini strumentali senologiche , nella ricerca di recidive da tumore mammario e nello studio delle protesi . 
mentre stato ormai definito il ruolo della risonanza magnetica per lo studio e la diagnosi di carcinoma della mammella occulto allesame clinico e mammografico , scarse sono le ricerche effettuate per valutare le potenzialit diagnostiche di tale metodica nella diagnosi di patologie intraduttali occulte con le pi comuni tecniche di diagnostica per immagini , sia per la diagnosi di carcinoma duttale in situ ( dcis ) sia delle lesioni benigne in particolare il papilloma intraduttale solitario e la papillomatosi [ 1820 ]  . 
alcuni studi hanno sottolineato limportanza della risonanza magnetica nella diagnosi differenziale tra papilloma del seno e lesione di natura maligna con componente intraduttale , soprattutto in casi in cui altre metodiche dimaging non siano state in grado di effettuare una diagnosi definitiva di natura della lesione [ 21 , 22 ]  . scopo del nostro lavoro stato quello di valutare le potenzialit diagnostiche della rm mammaria nello studio di pazienti con secrezione ematica o siero - ematica dal capezzolo , confrontando la rm con le metodiche quali la galattografia , la mammografia e lecografia . materiali e metodi da febbraio 2005 ad agosto 2006 , 43 pazienti di sesso femminile ed 1 di sesso maschile , di et compresa tra 28 e 65 anni ( et media : 42 anni ) con secrezione monorifiziale dal capezzolo di natura ematica e / o sieroematica , sono stati sottopostia studio con risonanza magnetica mammaria . 
tutti i pazienti avevano effettuato preliminarmente esame ecografico presso il nostro dipartimento , utilizzando apparecchi siemens antares o aloka prosound ssd - 5500 con trasduttori lineari ad alta frequenza ( 7 , 510 , 1013 mhz ) per i tessuti superficiali . 
dodici pazienti hanno effettuato esame galattografico ; nei restanti 32 pazienti non era stato possibile effettuare lesame a causa della difficolt nellincannulamento del dotto ( 9 pazienti ) , lo stravaso del mezzo di contrasto ( 8 ) ed il mancato consenso allesame da parte della paziente ( 15 casi )  . lo studio mediante risonanza magnetica stato eseguito utilizzando un magnete da 1 , 5 tesla ( magnetom vision , siemens , erlangen , germania ; gradienti 25 mt / m2 , slew rate 800 t / m / s , rise time 400 / s ) dotato di bobina doppia dedi252 radiol med ( 2008 ) 113 : 249264 tain a preliminary anatomical assessment of the breast . 
after contrast administration , another five consecutive sequences with similar parameters are acquired in the axial plane followed by a final single axial sequence with the same parameters as the first one . 
intravenous gadolinium - gadobenate dimeglumine ( dtpa ) ( multihance , bracco , milan , italy ) was administered at a rate of 2 ml / s via an automatic injector at a dose of 0.10.2 mmol / l per kilogram of body weight , together with a 10 - ml bolus of saline solution . image processing with digital subtraction of the precontrast t1 - weighted 3d flash sequences from the postcontrast sequences and generation of axial and coronal maximum intensity projection ( mip ) reconstructions were automatically performed by the systems software . 
 evaluation started with a preliminary assessment of the ductal system on the t2 - weighted stir images to identify signs of dilated ducts in subareolar location and / or in the remaining breast quadrants . 
precontrast t1 - weighted fat - saturation ( fs ) 3d flash sequences were used to characterise intraluminal fluid , which was considered haemorrhagic when it showed high signal intensity relative to the surrounding parenchyma . 
when ductal ectasia with or without a filling defect was identified , analysis focused on the corresponding anatomical area in the preand postcontrast t1 - weighted 3d flash sequences . postcontrast t1 sequences were assessed for areas of enhancement that , when present , were evaluated on the basis of morphological criteria and with reference to the breast imaging and reporting data systems ( bi - rads ) dynamic criteria [ 23 ]  . 
evaluation of postcontrast t1 - weighted sequences considered the presence and morphology of the enhancement , that is , whether it was focal ( mass - like ) , linear , segmental or periductal ( non - mass - like ) , features that could be isolated or combined . the mr images were then correlated with the findings cata alla studio del seno . 
lesame di risonanza magnetica stato eseguito con le sequenze standard per lo studio della mammella : sequenze stir t2 - pesate sul piano assiale ( tr / te : 6690 / 74 , slice thickness : 3 , 5 mm , fov : 2828 cm ) e flash 3d t1 - pesate ( tr / te : 14 / 7 , flip angle : 25 , slice thickness : 1 , 96 mm senza gap , matrice : 192256 , fov : 3055 cm ) sui piani assiale . lesame in pazienti con secrezione dal capezzolo diviso in due momenti : il primo prevede lacquisizione delle sequenze stir t2 - pesate assiali , necessarie per avere un inquadramento anatomico preliminare delle mammelle ed il secondo in cui sono effettuate le immagini flash 3d t1 - pesate prima della somministrazione di mezzo di contrasto per via endovenosa ( mdc ev ) la prima sul piano sagittale della mammella affetta da secrezione seguita dalla sequenza assiale e successivamente , dopo lintroduzione del mdc , lesecuzione di altre 5 sequenze consecutive con parametri analoghi sul piano assiale ed unultima ed unica sequenza sul piano sagittale , con parametri identici alla prima  . 
lintroduzione del mdc ev stata effettuata mediante iniettore automatico con somministrazione di gadolinio - dtpa ( gadobenato dimeglumina : multihance , bracco , milano italia ) alla dose di 0 , 10 , 2 mmol / l per chilogrammo di peso corporeo con una velocit di 2 ml / s unitamente a 10 ml di soluzione fisiologica in bolo . le elaborazioni delle immagini con la sottrazione digitale della sequenza flash 3d t1 - pesata pre - contrasto dalle sequenze post - contrasto e le ricostruzioni mip ( maximum intensity projection ) sul piano assiale e coronale , vengono effettuate in maniera automatica dal software . 
qualora sia presente unarea con enhancement sospetto , la stessa stata valutata con posizionamento di una regione di interesse ( roi ) e la misurazione dellincremento dellintensit di segnale nel tempo . 
per ectasia duttale ci riferiamo ad immagini con aspetto tubulare uniche o multiple ( in questultimo caso con aspetto confluente tra loro ) , che presentano elevata intensit di segnale nelle sequenze t2 - pesate . 
le sequenze flash 3d fat saturation ( fs ) t1 - pesate precontrasto sono state utilizzate per la caratterizzazione del contenuto fluido endoluminale , considerato di natura ematica se mostrava unelevata intensit di segnale rispetto al parenchima ghiandolare circostante . 
in tutti i casi in cui era riconoscibile unimmagine di ectasia duttale , con o senza difetto di riempimento , lo studio stato mirato allarea anatomica corrispondente nelle sequenze flash 3d t1 - pesate pre e post - contrasto . radiol med ( 2008 ) 113 : 249264 on mammography , us and galactography . 
when mri identified a well - circumscribed area of homogeneous enhancement appearing within the first minute and showing a type ii time - intensity curve ( bi - rads 3 probably benign finding ) , the lesion was sampled by core biopsy if it was 1 cm and detectable on us ( all occult lesions on initial us underwent second - look us after mri ) and by excisional biopsy if it was < 1 cin these cases , the clinical suspicion of ductal disease based on nipple discharge made excision mandatory because of the reported minimal risk of an association between breast cancer and conditions such as papilloma and papillomatosis . 
patients in whom mri revealed both the presence of enhancing areas with irregular or ill - defined margins or segmental and asymmetrical distribution , with enhancement rate > 100% within the first minute and type ii time - intensity curve , underwent excisional biopsy due to the strong suspicion of malignancy . 
all patients in whom mri did not show enhancement or showed benign enhancement according to the two radiologists were followed up by clinical examination , us and cytology of the nipple discharge at 6 and 12 months . 
only one patient required appropriate pharmacological treatment before being scheduled for follow - up at 6 , 12 and 18 months . results mammographic features in 35 / 43 patients , mammography failed to visualise pathological findings due to high breast density . 
in 6 / 43 patients , it demonstrated a prominent ductal pattern , associated in two patients with the presence of two opacities smaller than 1 cm in subareolar location . 
in 2 / 43 cases , it identified asymmetrical density ( table 1 )  . galactographic features nelle sequenze t1 dopo contrasto abbiamo verificato se fossero presenti aree dotate di potenziamento ; e qualora questo fosse presente veniva valutato in base a criteri morfologici e in riferimento ai criteri bi - rads , dinamici [ 23 ]  . 
nella valutazione delle sequenze t1 - pesate post - contrasto venivano considerati la presenza e la morfologia del potenziamento se di tipo focale ( mass - like ) , lineare , segmentale o periduttale ( non - masslike ) aspetti presenti sia singolarmente che associati . le immagini ottenute nel corso degli esami di rm sono state poi confrontate con i dati emersi nelle indagini mammografiche ma soprattutto ecografiche e galattografiche . nei casi in cui la rm identificava aree dotate di potenziamento omogeneo con margini regolari , intenso al i minuto e curva intensit / tempo del ii tipo , classificate come bi - rads 3 ( potenziamento dubbio ma con prevalenza di benignit ) stata effettuata core - biopsy nelle lesioni 1 cm e riconoscibili mediante ecografia ( in tutte le lesioni non riconosciute al primo esame ecografico stato effettuato second - look dopo l ? esame rm ) e biopsia chirurgica nelle lesioni < 1 cm in quanto il sospetto di patologia duttale indicato dal sintomo secrezione rendeva necessaria lescissione della lesione , relativamente al rischio , se pur minimo , indicato in alcune casistiche , dellassociazione tra patologie tra i quali papillomi e papillomatosi con il carcinoma della mammella . 
nei pazienti in cui la risonanza magnetica metteva in evidenza sia la presenza di aree di potenziamento con margini irregolari , sfumati o tipo segmentale ed asimmetrico , un tasso di potenziamento della lesione > 100% al i minuto e curva intensit / tempo del ii tipo sono state sottoposte a biopsia chirurgica della lesione perch forte era il sospetto di malignit . hanno invece effettuato follow - up clinico , ecografico e citologico della secrezione , con una cadenza di 6 e 12 mesi , sia tutti i pazienti che non presentavano potenziamento sia quelli che allesame di rm mostravano potenziamenti considerati dai radiologi , di natura benigna . 
ununica paziente veniva precedentemente sottoposta ad un adeguato trattamento farmacologico seguito da follow - up clinico ed ecografico con cadenza di 6 , 12 , 18 mesi . galactography was performed in 12 / 44 patients and was negative in three of the the nine patients with positive findings showed simple ductal ectasia ( n = 3 ) , subareolar ectasia ( n = 1 ) , ectasia associated with gross filling defect ( n = 2 ) and ectasia associated with multiple filling defects ( n = 3 )  . risultati aspetti mammografici sonographic features us was negative in 18 / 44 cases ( 40.9% ) ; in the remaining 26 / 44 ( 59% ) , it identified diffuse simple ductal ectasia of in 35 / 43 pazienti lesame mammografico a causa dellelevata densit strutturale della ghiandola non permetteva di visualizzare immagini di significato patologico . 
in 6 / 43 pazienti dimostrava prominenza del disegno duttale , che in due pazienti si associava alla presenza di due opacit del diametro inferiore ad 1 cm in sede retroareolare . 
of patients mammographic features duct ectasia negative : high density asymmetrical density tabella 1 reperti mammografici numero pazienti reperto mammografico aspetti ecografici prominenza del disegno duttale assenza di reperti : elevata densit ghiandolare asimmetria del disegno ghiandolare table 2 sonographic features no . 
of patients sonographic features tabella 2 reperti ultrasonografici numero pazienti reperto ecografico negative simple ductal ectasia ductal ectasia with solid internal echoes and duct wall thickening ductal ectasia with inhomogeneous breast parenchyma negativo ectasia duttale semplice ectasia duttale con pareti ispessite e proliferazione solida intraduttale ectasia duttale associata a disomogeneit del parenchima mammario the larger ducts ( n = 12 ) , regional ductal ectasia associated with duct wall thickening and intraductal proliferation ( n = 9 ) and regional ductal ectasia ( n = 5 ) associated with inhomogeneous surrounding parenchyma ( n = 3 ) ( table 2 )  . mri features no pathological findings were identified in the t2 stir sequences in 17 / 44 cases . 
le 9 pazienti con esame positivo presentavano : ectasia duttale semplice ( 3 donne ) , ectasia in sede retroareolare ( 1 caso ) , ectasia associata ad un grossolano difetto di riempimento ( 2 ) ed ectasia associata a multipli difetti di riempimento in 3 pazienti . allesame ecografico in 18 / 44 casi ( 40 , 9% ) non erano evidenti immagini di rilievo ; nelle restanti 26 / 44 ( 59% ) pazienti lecografia aveva identificato : ectasia della componente duttale generalizzata dei dotti di maggior calibro in 12 , dilatazione distrettuale dei dotti associata ad ispessimento della parete duttale ed alla presenza di proliferazione intraduttale in 9 mentre in 5 ectasia duttale distrettuale che in 3 pazienti si associava a disomogeneit del parenchima mammario limitrofo ( tabella 2 )  . aspetti di risonanza magnetica allesame di risonanza magnetica nelle sequenze t2 stir in 17 / 44 casi non erano evidenti immagini patologiche . 
nei rimananti 26 / 44 casi era presente dilatazione duttale , che in 12 casi risultava di tipo generalizzato ( definendo con questo termine una dilatazione che interessi i dotti di maggior calibro e risulti estesa ai dotti periferici in pi di due quadranti ) ed in 14 di tipo distrettuale ( cio una dilatazione di uno o pi dotti allinterno di un quadrante o nella regione retroareolare ) ; in 4 / 26 pazienti stato possibile riconoscere difetto di riempimento del lume duttale ectasico . per quanto riguarda la valutazione del contenuto dei dotti ectasici , in 5 casi , allesame con risonanza magnetica , si identificava un elevato segnale nelle sequenze flash 3d t1pesate , precontrasto , suggestivo per natura ematica o proteinacea del fluido . 
nei restanti casi seppure ci fosse una storia clinica positiva per secrezione ematica o sieroematica dal capezzolo il contenuto del dotto mostrava un basso segnale nelle sequenze flash 3d t1 - pesate precontrasto ma un alto nelle sequenze stir t2 - pesate ( tabella 3 )  . nelle sequenze t1 - pesate effettuate dopo somminstrazione di mdc ev in 12 casi la risonanza magnetica non identificava potenziamenti patologici ( bi - rads 1 ) mentre in 7 pazienti era presente unarea di modesto potenziamento con morfologia nodulare o puntiforme : reperto considerato dai radiologi bi - rads 2 . in 22 / 44 pazienti si evidenziavano aree di potenziamento con morfologia lineare o nodulare e contorni regolari classificate come categoria diagnostica definitiva bi - rads 3 . 
in 3 / 44 pazienti la risonanza magnetica mostrava aree di potenziamento con caratteristiche fortemente sospette per la radiol med ( 2008 ) 113 : 249264 table 3 magnetic resonance imaging findings on precontrast sequences architectural features of the ducts on t2 - weighted sequences duct contents on t2 - weighted sequences duct contents on t1 - weighted sequences suspicious filling defects ( 4 patients ) , absence of intraductal defects ( 10 patients ) absence of intraductal defects ( 12 patients ) high signal intensity ( 5 patients )  . 
 low signal intensity ( 9 patients ) low signal intensity ( 12 patients ) absence of ductal ectasia ( 17 patients ) hyperintense subareolar oval mass ( 1 patient ) peripheral ductal ectasia ( 14 patients ) diffuse ductal ectasia ( 12 patients ) tabella 3 reperti rm nelle sequenze precontrasto immagini dei dotti nelle sequenze t2 - pesate contenuto dei dotti nelle sequenze t2 pesate contenuto dei dotti nelle sequenze t1 pesate precontrasto assenza di dilatazione duttale ( 17 pz ) immagine ovalare iperintensa retroareolare ( 1 pz ) ectasia distrettuale ( 14 pz ) ectasia generalizzata ( 12 pz ) sospetti difetti di riempimento ( 4 pz ) assenza di irregolarit intraduttali ( 10 pz ) assenza di irregolarit intraduttali ( 12 pz ) elevato segnale ( 5 pz ) basso segnale ( 9 pz ) basso segnale ( 12 pz ) ing 26 / 44 , cases it showed ductal dilatation , which was diffuse in 12 cases ( affecting the larger ducts and extending to the peripheral ducts in one or more quadrants ) and regional in 14 cases ( affecting one or more ducts within one quadrant or in the subareolar region ) ; in 4 / 26 patients , an intraluminal filling defect was observed in the dilated duct . with regard to evaluation of duct contents , precontrast t1 - weighted 3d flash sequences demonstrated high signal intensity suggestive of haemorrhagic or proteinaceous fluid in five cases . 
in the remaining cases , despite a clinical history of bloody or serosanguineous nipple discharge , duct contents showed low signal intensity on precontrast t1weighted 3d flash sequences but high signal intensity on t2 - weighted stir images ( table 3 )  . in the t1 - weighted sequences obtained after contrast administration , mri visualised no pathological enhancement in 12 cases ( bi - rads 1 ) and an area of moderate enhancement with nodular or punctuate morphology in seven cases , a finding classified as bi - rads 2 . 
in 3 / 44 patients , mri showed enhancing lesions with suspicious features ( definitive diagnostic category bi - rads 4 ) : mass - like enhancement with irregular and ill - defined margins ( one case ) and with segmental distribution ( two cases )  . 
these patients also had ductal ectasia with prevalent location in the same region as the suspicious mass - like enhancement ( table 4 )  . ten out of 22 patients classified as bi - rads 3 underwent preliminary core biopsy , whereas 12 / 22 underwent cytology . 
the presence of disease of ductal origin associated with clinical evidence of nipple discharge indicated a need presenza di lesione di tipo evolutivo ( categoria diagnostica definitiva bi - rads 4 ) : potenziamento con morfologia nodulare a margini irregolari e sfumati ( 1 caso ) e di tipo segmentale ( 2 caso )  . 
in tali pazienti si associava la presenza di ectasia duttale con localizzazione prevalentemente distrettuale localizzata nella medesima sede del potenziamento sospetto ( tabella 4 )  . dieci / 22 pazienti classificate come bi - rads 3 venivano sottoposte preliminarmente a core - biosy mentre 12 / 22 ad esame citologico : la presenza di patologia ad origine duttale associata allesame clinico positivo per secrezione dal capezzolo , indicava lopportunit di effettuare comunque la biopsia chirurgica a cui sono state tutte sottoposte . 
in particolare nei 22 pazienti con reperti benigni , in 12 casi si riscontrava la presenza di papillomi singoli intraduttali ( 8 singoli e 4 multipli ) , in 3 di papillomi retroareolari , in 5 una condizione di papillomatosi e 2 casi di iperplasia duttale atipica . 
in particular , of the 22 patients with benign findings , 12 had intraductal papillomas ( eight single and four multiple ) , three had subareolar papillomas , five had papillomatosis and two had atypical ductal hyperplasia . 
the three subareolar papillomas appeared as nodular subareolar areas of homogenous delle 12 pazienti con papilloma intraduttale solo 5 avevano effettuato la galattografia che in 1 caso mostrava ectasia semplice dei dotti retroareolari , in 2 dilatazione duttale semplice e in 2 pazienti un grossolano difetto di riempimento con dilatazione duttale associata . i 3 papillomi retroareolari si identificavano come formazioni nodulari con potenziamento omogeneo ( curva intensit / tempo ii tipo , > 100% al ii minuto ) in sede retroareolare non associati a dilatazione duttale . 
in 3 casi di papillomatosi duttale , alla risonanza magnetica , venivano identificate aree di potenziamento duttale di tipo lineare , mentre nelle altre 2 pazienti si osservavano aree di potenziamento omogeneo con morfologia nodulare e margini policiclici , la curva intensit / tempo effettuata su tali aree risultava del ii tipo . 
lesame galattografico effettuato su tutte le 5 pazienti con papillomatosi mostrava in 1 caso dilatazione duttale con associati multipli difetti di riempimento , in 2 ectasia semplice dei dotti ed in 2 casi non risultava diagnostica . 
i 2 casi di iperplasia duttale atipica venivano identificate alla risonanza magnetica come noduli multipli di intenso potenziamento , localizzati prevalentemente in un unico quadrante , e con curva intensit / tempo del ii tipo . nelle 3 pazienti classificate bi - rads 4 , lesame istologico dimostrava la presenza di un carcinoma papillare , 1 caso di carcinoma intraduttale con aspetto micropapillare ed 1 caso di idc . 
1a precontrast axial t2 - weighted short - tau inversion recovery images show ductal ectasia in the right subareolar region with an oval , hypointense associated mass ( 1 cm )  . 
1a immagini t2 pesate stir acquisite sul piano assiale : a destra in sede retroareolare si osserva una immagine allungata e tortuosa iperintensa da riferire ad un dotto ectasico nel suo contesto presente una immagine rotondeggiante ipointensa di circa 1 cb immagini di sottrazione digitale t1 pesate flash 3d , acquisite sul piano assiale : a destra si documentano alcune aree di potenziamento omogeneo , rotondeggianti a margini netti . enhancement ( type ii time - intensity curve , > 100% during the second minute ) not associated with ductal dilatation . in three cases of ductal papillomatosis , mri showed linear areas of ductal enhancement , whereas in the other two patients , it revealed nodular areas of homogeneous enhancement with lobular margins and type ii time - intensity curves . 
galactography , performed on all five patients with papillomatosis , showed ductal dilatation , with multiple associated filling defects in one case and simple ductal ectasia in two cases ; in two cases , it was not diagnostic . 
the two cases of atypical ductal hyperplasia were identified on mri as multiple intensely enhancing nodules , prevalently confined to a single quadrant and with type ii time - intensity curve . 
in the three patients classed as bi - rads 4 , histology po somministrazione di mdc ev , lesistenza di unarea di potenziamento segmentale in 2 casi ( il potenziamento risultava asimmetrico rispetto alla mammella controlaterale ) e di tipo nodulare nella restante paziente . 
i reperti dellesame galattografico di due di queste pazienti erano caratterizzati da multipli difetti di riempimento duttale con irregolarit di calibro sia nella paziente con carcinoma intraduttale di aspetto micropapillare 258 radiol med ( 2008 ) 113 : 249264 fig . 
b le immagini flash 3d t1 - pesate effettuate dopo somministrazione di mdc ev identificano nella medesima sede unarea dintenso potenziamento . demonstrated one case of papillary carcinoma , one of intraductal carcinoma with micropapillary appearance and one of idc . 
in these three patients , postcontrast t1 - weighted 3d flash sequences had shown an area of segmental enhancement in two cases ( asymmetrical relative to the contralateral breast ) and an area of nodular enhancement in the remaining case . 
galactography in two of these patients had revealed multiple ductal filling defects with duct wall irregularities both in the patient with intraductal carcinoma with micropapillary appearance and in the one with papillary carcinoma . the 19 patients with negative mri findings did not undergo excisional biopsy but were followed up with clinical examination , us and cytology of the nipple discharge at 6 sia nella paziente con carcinoma papillare . i 19 pazienti che non presentavano alla rm immagini patologiche , non venivano sottoposti a biopsia chirurgica ma effettuavano follow - up clinico , ecografico e citologico della secrezione , con una cadenza di 6 e 12 mesi , non presentando modifiche significative del quadro strumentale nel tempo e con regressione del sintomo clinico ( secrezione ) in 13 casi . lunica paziente in cui la rm metteva in evidenza la presenza di un tragitto fistoloso con potenziamento con tipologia benigna ( birads 2 ) veniva sottoposta ad unadeguata terapia farmacologia cui seguiva follow - up clinico e strumentale mediante ecografia . second - look in 11 casi stato effettuato il second - look ecografico in quanto larea di potenziamento contrastografico messo in evidenza allesame di rm non era visualizzato al precedente esame ecografico a cui le pazienti venivano sottoposte . 
no significant changes were identified in the imaging and laboratory findings , and clinical symptom ( nipple discharge ) resolved in 13 cases . the only patient in whom mri demonstrated a fistula with benign - appearing enhancement ( birads 2 ) underwent pharmacological treatment and subsequent clinical and sonographic follow - up . un solo caso il second - look non ha dato esito positivo ; si trattava di una paziente giovane con secrezione prevalentemente ematica in cui la mammografia non era diagnostica , lecografia non evidenziava immagini patologiche e durante lesame galattografico non era stato possibile incannulare il dotto secernente . 
 260 radiol med ( 2008 ) 113 : 249264 second - look ultrasound discussione eleven cases underwent second - look us , as the area of enhancement revealed by mri had not been detected at the previous us examination . 
in only one case was second - look us negative ; this was a young patient with prevalently bloody nipple discharge in whom mammography had been nondiagnostic , us was negative and galactography unsuccessful due to failure to cannulate the secreting duct . 
clinical findings suggesting a lesion that requires excisional biopsy are spontaneous and unilateral bloody or serosanguineous nipple discharge , drainage from a single duct and palpable breast mass [ 18 ]  . nipple discharge may be caused not only by benign ductal disease but also , less commonly , by malignant lesions such as breast cancer . 
in rare cases , nipple discharge may be related to hormonal changes affecting the breast [ 4 , 24 ]  . the reported diagnostic workup of a patient with spontaneous unilateral nipple discharge that is bloody or serosanguineous consists of cytological assessment of the secretion combined with diagnostic imaging studies such as galactography and mammography . 
the diagnostic value of galactography is still controversial due to the techniques many limitations : difficulty cannulating the duct , possible contrast leakage , patients refusal to undergo the test and patients young age . 
in our series , galactography was performed in 12 women only owing to some of these limitations . the most frequent galactographic findings in women with nipple discharge associated with ductal pathology are ductal ectasia , filling defects and irregularities with possible distortion of the ductal pattern . 
in our study , galactography identified , as positive signs of ductal disease , ductal ectasia in nine cases , multiple filling defects in three and a gross filling defect in two . la secrezione dal capezzolo rappresenta un sintomo comune in presenza di patologia duttale . 
la secrezione dal capezzolo pu distinguersi in spontanea o indotta e unilaterale o bilaterale [ 35 ]  . i reperti clinici che suggeriscono la presenza di una lesione che richiede la necessit di escissione bioptica sono la secrezione spontanea ematica o siero - ematica dal capezzolo a sede monolaterale , il drenaggio ad origine da un singolo dotto e la presenza di una massa palpabile intramammaria [ 18 ]  . la secrezione dal capezzolo infatti pu essere causata non solo da patologie benigne ad origine dallalbero duttale , come occorre pi frequentemente , ma anche da lesioni di natura maligna , come ad esempio il carcinoma mammario . in casi rari , tale condizione pu essere indotta da modificazioni ormonali che si riflettono sulla ghiandola mammaria [ 4 , 24 ]  . in letteratura , liter diagnostico , in una paziente con secrezione spontanea , monolaterale dal capezzolo di natura ematica o siero - ematica rappresentato dallesame citologico del secreto in associazione con alcuni esami strumentali di diagnostica per immagini quali la galattografia e la mammografia . 
in passato lesame galattografico ha rappresentato la metodica dimaging di prima scelta nelle pazienti con secrezione dal capezzolo , utilizzata prevalentemente per la localizzazione della lesione [ 35 ]  . 
le capacit diagnostiche della galattografia rimangono tuttora controverse . molti sono , infatti i limiti allutilizzo di tale metodica : difficolt nellincannulare il dotto , possibile stravaso del mezzo di contrasto , mancato consenso allesecuzione da parte della paziente e la giovane et della stessa . 
nella nostra casistica lesame galattografico era stato effettuato infatti , unicamente in 12 donne proprio a causa di alcune delle limitazioni sopra menzionate . i reperti galattografici di maggior riscontro in pazienti con secrezione dal capezzolo a cui si associa patologia duttale sono caratterizzati dalla presenza di : ectasia duttale , difetti di riempimento ed irregolarit con eventuale distorsione del disegno duttale . 
nel nostro studio tale metodica identificava come reperti positivi per patologia duttale la presenza di dilatazione duttale in 9 casi , multipli difetti di riempimento in 3 e un grossolano difetto di riempimento in 2 donne . ponendo a confronto i reperti galattografici con quelli ottenuti mediante rm , la galattografia non risultata diagnostica nei 2 casi di papillomatosi diffusa mentre nei rimanemti 10 casi mostrava immagini aspecifiche come la dilatazione duttale o i difetti di riempimento unici o multipli . 
frequentemente esistono aspetti galattografici che possono definirsi del tutto aspecifici , come i difetti di riempimento e le irregolarit del calibro duttale : tali reperti infatti non permettono una diagnosi differenziale certa tra patologia duttale di natura benigna e lesione neoplastica . 
dobbiamo inoltre ricordare che lesame galattografico risulta sempre una metodica radiol med ( 2008 ) 113 : 249264 comparing galactography and mri findings , galactography proved nondiagnostic in the two cases of diffuse papillomatosis , whereas in the remaining ten cases , it showed nonspecific findings such as ductal ectasia or single or multiple filling defects . 
moreover , galactography is always an invasive technique that entails introduction of contrast material into the duct and a risk of complications such as allergic reactions , mastitis or abscesses . mammography in patients with nipple discharge is negative in 60% of cases , probably as a result of the small size of intraductal lesions , generally less than 1 cm [ 3 , 10 ]  . 
some benign ductal lesions , such as papilloma or papillomatosis , may present on mammography as one or several well - circumscribed nodules of varying size or as ductal ectasia . less commonly , they may appear as calcifications of varying morphology round , egg - shell or microcalcification clusters a finding that is difficult to differentiate from the typical pattern of malignant masses [ 8 ]  . the most common sonographic features in our study were duct dilatation , particularly associated with solid internal echoes and duct wall thickening . 
the site of these abnormalities was generally central and / or subareolar . in patients with unilateral nipple discharge , it is essential to differentiate benign lesions , such as papilloma , papillomatosis and ductal inflammation that causes accumulation of bloody secretion within a dilated duct , from malignancies , such as papillary carcinoma , dcis and idc , which in rare cases may be responsible for spontaneous discharge [ 25 , 26 ]  . 
in all these conditions , in addition to the patients clinical history and cytological evaluation of the nipple discharge , the findings of us - guided fine - needle aspiration biopsy are fundamental [ 27 ]  . the limitations of mammography , us and galactography in the diagnosis of suspected ductal disease in women with nipple discharge has prompted some investigators to turn to other diagnostic imaging modalities , such as mri . 
although many studies have confirmed that mri can be used to detect clinically and mammographically occult breast cancers , relatively little data exists on its possible role in the study of patients with unilateral nipple discharge emanating from a single duct . some studies have focused on the typical mri features of solitary intraductal papilloma . 
this was found to appear as an oval mass with regular or lobulated margins , associatinvasiva per lintroduzione del mezzo di contrasto nel dotto e la possibilit dinsorgenza di complicanze limitanti il suo svolgimento : reazioni allergiche , mastiti o ascessi . lesame mammografico in pazienti affette da secrezione dal capezzolo nel 60% dei casi negativo , tale reperto probabilmente dovuto alle ridotte dimensioni delle lesioni intraduttali , generalmente al di sotto del centimetro [ 3 , 10 ]  . nel nostro studio la mammografia ha identificato solo in 8 / 43 casi reperti indicativi per patologia mammaria come la presenza di asimmetria ghiandolare e prominenza del disegno duttale . 
talvolta una lesione duttale benigna come il papilloma o la papillomatosi multipla , pu manifestarsi allesame mammografico sottoforma di uno o pi noduli di varia grandezza , con margini ben definiti o come prominenza del disegno duttale e pi raramente come calcificazioni . questultime possono avere differente morfologia : rotondeggiante , a guscio duovo o cluster di microcalcificazioni , reperto di difficile differenziazione da quello caratteristico delle formazioni di natura maligna [ 8 ]  . i reperti ecografici pi frequenti nel nostro studio erano rappresentati dalla dilatazione duttale in particolare associata a proliferazione solida intraduttale ed ispessimento della parete del dotto . 
la sede di tali rilievi era generalmente centrale e / o retroareolare . nelle pazienti affette da secrezione monolaterale dal capezzolo di fondamentale importanza risulta la diagnosi differenziale tra lesioni di natura benigna come il papilloma , la papillomatosi e le varie patologie flogistiche endoduttali che determinano accumulo di secreto emorragico allinterno di un dotto ectasico e la presenza di lesioni maligne quali il carcinoma papillare , il cdis ed lidc , che pure se in percentuale bassa possono essere la causa di secrezione spontanea [ 25 , 26 ]  . 
in tutte queste condizioni oltre alla storia clinica della paziente ed alla citologia del secreto , fondamentale nella diagnosi sar il reperto dellagoaspirato ecoguidato [ 27 ]  . i limiti di metodiche quali la mammografia , lecografia e la galattografia nella diagnosi di una sospetta patologia duttale in donne con secrezione dal capezzolo ha indotto alcuni studiosi a dedicarsi allutilizzo di ulteriori metodiche di diagnostica radiologica quali ad esempio la risonanza magnetica . 
sebbene molti siano gli studi che confermano come la risonanza magnetica possa essere usata nella diagnosi di tumori mammari clinicamente e mammograficamente occulti , relativamente scarse sono le ricerche sul possibile ruolo nello studio di pazienti affette da secrezione ematica monolaterale mono - orifiziale . alcuni studi hanno focalizzato lattenzione sullaspetto caratteristico del papilloma solitario intraduttale allesame rm che appare come una formazione ovalare a margini regolari o lobulati , associata o meno alla presenza di dilatazione duttale e di brusco restringimento del lume duttale e che nelle sequenze dopo somministrazione di mezzo di contrasto ev , mostra potenziamento che pu essere di discreta entit e patchy oppure intenso ed omogeneo , concludendo 262 radiol med ( 2008 ) 113 : 249264 ed or unassociated with ductal dilatation and abrupt narrowing of the duct lumen . 
enhancement after contrast administration ranged from minimal and patchy to marked and homogeneous , leading the authors to conclude that no findings exist that are highly suggestive for this type of lesion [ 5 , 2022 ]  . in our study , mri appearance of intraductal papillomas varied : well - circumscribed areas of homogeneous enhancement with well - defined margins and oval shape ( ten cases ) and areas of homogeneous enhancement with linear shape and enhancement rate > 70% within the first minute ( two cases )  . 
the most frequent site was periareolar . in contrast , the three subareolar papillomas were identified by the presence of an enhancing subareolar nodule ( type ii curve , with enhancement rate > 100% during the first minute )  . 
intraductal papillomatosis did not show typical patterns , appearing as either areas of linear enhancement or multiple areas of nodular enhancement with lobulated margins and type ii time - intensity curve . among the three patients with carcinoma , one had dense breasts and two had asymmetrical density . 
us identified the presence of solid internal echoes in one case ( in correspondence with the dilated duct ) and regional ductal ectasia associated with nonhomogenous periductal parenchyma in two cases . 
in these patients , mri demonstrated a mass - like enhancement with irregular margins in one patient and a marked segmental enhancement anatomically coinciding with the areas of ductal dilatation on the t2 - weighted stir sequences in two cases . 
in these cases , mri undoubtedly provided the best lesion characterisation , as , in contrast to the general information provided by mammography , us and galactography , it allowed us both to localise the lesion and to define its extension a crucial factor for surgical planning . another interesting aspect to be considered is the histological result in the two patients who showed marked segmental enhancement without associated mass - like findings on mri . 
these patients were found to be affected by infiltrating ductal carcinoma with papillary features and papillary carcinoma , respectively , both with extensive involvement of the ductal system . in our series , the 19 patients with nonsuspicious or frankly benign mri findings did not undergo excisional biopsy . 
all were scheduled for follow - up by clinical examination , us and cytology of nipple discharge . although some studies claim that breast mri is unable to differentiate between ductal disease , such as intraductal pache non esiste un reperto altamente indicativo per questo tipo di lesione [ 5 , 2022 ]  . nel nostro studio allesame con risonanza magnetica , i reperti di papilloma intraduttale si sono caratterizzati per la variabilit nellaspetto : aree di potenziamento omogeneo e circoscritto a margini netti e con morfologia ovalare ( 10 casi ) e aree di potenziamento omogeneo con morfologia lineare e tasso di enhancement > 70% al i minuto , in 2 pazienti . 
i 3 papillomi retroareolari invece si identificavano con la presenza di un nodulo retroareolare dotato di potenziamento ( curva del ii tipo , con tasso di potenziamento > 100% al i minuto )  . 
la papillomatosi intraduttale , invece non mostrava un aspetto tipico : identificavamo sia aree di potenziamento lineare sia aree multiple di enhancement nodulare a margini policiclici e curva intensit / tempo del ii tipo . le 3 pazienti che sono risultate affette da carcinoma presentavano mammelle dense in 1 caso ed in 2 casi una condizione di asimmetria ghiandolare . 
lesame ecografico identificava in 1 caso la presenza di una proliferazione solida periduttale ( in corrispondenza di un dotto ectasico ) ed in 2 pazienti dotti ectasici distrettuali associati a disomogeneit del parenchima periduttale . 
la risonanza magnetica in queste pazienti dimostrava in una paziente unarea di potenziamento nodulare a contorni irregolari e nelle altre due un potenziamento segmentale di elevata intensit corrispondente alle aree parenchimali in cui erano riconoscibili dotti ectasici nelle sequenze stir t2 - pesate . 
in questi 3 casi lindagine che ha permesso una migliore caratterizzazione della patologia stata senza dubbio la rm , in quanto mentre la mammografia , lecografia e la galattografia fornivano informazioni generiche sulla tipologia della lesione causa della secrezione la rm ha permesso di localizzare la lesione e soprattutto di definirne lestensione , aspetto di notevole importanza a fini chirurgici . altro aspetto interessante , meritevole di riflessione il risultato istologico delle due pazienti che presentavano alla rm un intenso potenziamento di tipo segmentale , senza aspetti nodulari associati : tali pazienti sono risultate affette rispettivamente da carcinoma duttale infiltrante con aspetti papilliferi e da carcinoma papillare , entrambi con interessamento di unestesa porzione dellalbero duttale . nella nostra casistica i 19 pazienti che presentavano allesame di risonanza magnetica reperti considerati non sospetti per malignit o francamente benigni non sono stati sottoposti a biospia chirurgica . 
tutte sono successivamente state seguite nel tempo con follow - up clinici , ecografici e del citologico a breve distanza di tempo . sebbene in alcuni studi sia riportato che la rm mammaria non sia ad oggi in grado di effettuare , nellambito della radiol med ( 2008 ) 113 : 249264 pilloma and frankly malignant lesions , it is important to emphasise that careful evaluation of the morphology and dynamics of lesion enhancement may guide towards a more accurate diagnosis [ 5 , 22 ]  . 
in studying patients with nipple discharge , mri can therefore be regarded as a modality with considerable diagnostic potential in combination with mammography and us and a useful tool whenever galactography cannot be performed . patologia duttale , diagnosi differenziale tra lesione benigna , come ad esempio il papilloma intraduttale , ed una formazione di natura francamente maligna importante sottolineare come unattenta valutazione sia della morfologia che della dinamica del potenziamento della lesione possano orientare ad una diagnosi pi accurata [ 5 , 22 ]  . 
la risonanza magnetica , nello studio di pazienti con secrezione dal capezzolo , dunque pu essere considerata una metodica dotata di potenzialit diagnostiche non trascurabili in associazione alla mammografia ed ecografia e utile strumento qualora la galattografia non sia effettuabile . conclusions conclusioni although our series was not sufficiently large to allow statistical analysis of results , and the patient group was not homogeneous in that not all of them were studied by galactography , we believe mri to be a valuable technique for studying patients with bloody or serosanguineous nipple discharge . in contrast to galactography , which is limited by its invasiveness , potential complications and poor acceptability to some patients , breast mri provides excellent visualisation of dilated ducts and their contents without requiring duct cannulation ( t2 - weighted stir sequences )  . 
benzi 8 , 16132 genoa , italy 2 cattedra di nefrologia - dimi , university of genoa , viale benedetto xv 6 , 16132 , genoa , italy correspondence to : m.b. 
ten volunteers underwent dwmri imaging of the kidneys with a breath - hold single - shot spin - echo planar imaging ( se - epi ) sequence in the axial and coronal planes with b values of 300 , 500 , 800 s / mm2 , in different states of hydration . 
stato condotto studio rm - dw renale con sequenza single - shot echo planare in breath - hold ( se - epi ) assiale e coronale ( valori di b di 300 , 500 , 800 s / mm2 ) in 10 volontari sani , in differente stato di idratazione , con controllo di osmolarit urinaria ( osmu ) e sodiuria ( nau )  . 
the technique , which was developed from the model presented by stejskal and tanner , is based on the application of two gradients of equal intensity and duration but opposite sign , which causes dephasing of spins , thereby accelerating intravoxel incoherent motion signal loss proportionally to the time interval between the application of the first and second gradient [ 1 ]  . 
whereas dw - mri has become a well - established diagnostic tool in neuroradiology [ 2 ] , only recently has the technique made headway in abdominal imaging , largely thanks to the introduction of ultrafast echoplanar breath - hold sequences [ 3 , 4 ]  . 
this is due to the low spatial resolution of the images and difficulties concerning the intrinsic sensitivity to motion and the magnetic susceptibility of diffusion - weighted sequences , with the consequent artefacts related to cardiac activity and intestinal peristalsis [ 5 ]  . in the field of abdominal imaging , diffusion study of the kidney is without doubt one of the most promising areas . this is due to both the relative immobility of the organ that , given its extraperitoneal location , is less susceptible to motion artefacts , and the prospects offered by functional imaging in nephrology a sector in which anatomy and physiology go hand in hand . 
diffusion - weighted imaging could be integrated into an all - in - one morphologicalfunctional mr study , a study which several authors suggest could provide highly useful information regarding parenchymal microstructure without the use of ionising radiation or potentially nephrotoxic contrast agents [ 69 ]  . data reported in the literature on renal dw - mri are noticeably variable , which often renders direct comparison difficult . 
the b value expresses the degree of sensitivity of the diffusion sequences , which depends on the distance , the intensity and the duration of the additional pulsed gradients according to the model proposed by stejskal and tanner [ 1 ]  . in abdominal imaging , the choice of the b value , and therefore the degree of diffusion weighting , is a significant problem that remains unsolved . 
there is no real agreement regarding the optimal b value for studying the kidney , the optimal scan plane ( even though the anisotropy of the kidney requires the application of gradients along the three orthogonal axes : x , y , and z ) nor where the region of interest ( roi ) introduzione le potenzialit di valutazione quali - quantitativa del movimento molecolare in funzione dellorganizzazione microstrutturale del distretto studiato offerte dalle tecniche di imaging rm pesate in diffusione ( rm - dw ) presentano un grande interesse clinico . 
questa tecnica si basa fondamentalmente sullapplicazione , secondo il modello di steiskal e tanner , di due gradienti aggiuntivi di segno opposto , ma di uguale intensit e durata , tali da determinare una perdita di coerenza di fase degli spin proporzionale al loro moto casuale nellintervallo di tempo tra lapplicazione del primo e del secondo gradiente [ 1 ]  . 
mentre in campo neuroradiologico la rm - dw costituisce una realt diagnostica consolidata [ 2 ] , in campo addominale la stessa una tecnica di recente acquisizione , attuabile solo grazie allintroduzione delle tecniche di acquisizione ecoplanari ultraveloci in respiro sospeso [ 3 , 4 ]  . 
le applicazioni in campo addominale sono , tuttavia , ancora oggetto di studio data la bassa risoluzione spaziale delle immagini e le problematiche legate allintrinseca sensibilit al movimento e alla suscettivit magnetica delle sequenze diffusione pesate con conseguenti artefatti legati allattivit cardiaca e alla peristalsi intestinale [ 5 ]  . nellambito delle applicazioni addominali , lo studio in diffusione del rene costituisce senza dubbio una realt promettente sia per la relativa immobilit dellorgano che , situato in regione extraperitoneale , risulta meno suscettibile ad artefatti da movimento , sia per linteresse legato allimaging funzionale in nefrologia , un settore dove anatomia e fisiologia sono strettamente legate . 
limaging in diffusione potrebbe essere integrato nellambito di uno studio rm morfologico - funzionale all in one in cui , come suggerito da alcuni autori , potrebbe fornire importanti informazioni sulla microstruttura parenchimale , in assenza di radiazioni ionizzanti e senza utilizzo di mdc potenzialmente nefrotossico [ 69 ]  . 
le differenze riscontrate possono , in parte , essere correlate allutilizzo di apparecchiature e tecniche di esame differenti , ma soprattutto alla differente pesatura in diffusione della sequenza , ossia al suo valore di b . 
il valore di b esprime il grado di sensibilizzazione alla diffusione della sequenza che dipende dalla distanza , dallintensit e dalla durata dei gradienti pulsati aggiuntivi secondo il modello proposto da steiskal e tanner [ 1 ]  . 
la scelta del valore di b , e quindi del grado di pesatura in diffusione , in campo addominale , un problema non trascurabile e ancora oggi non risolto ; se osserviamo la letteratura riguardante largomento , infatti , vari autori , utilizzando valori diversi di b , sono giunti a risultati non sovrapponibili [ 9 ]  . 
non ancora univoco quale sia il valore di b ottimale da utilizzare nello studio del rene , quale sia il piano ottimale di scansione ( anche se comunque lanisotropia del rene richiede lapplicazione dei gradienti lungo i tre assi ortogonali x , y , z ) e 216 radiol med ( 2008 ) 113 : 214224 should be located for calculating the apparent diffusion coefficient ( adc ) value . 
in addition , an inverse relationship has been described between the b value and adc , as well as an influence of the kidneys hydration state on adc [ 8 ]  . the aim of our study was to determine , in healthy volunteers , mean renal adc in both the axial and coronal planes at the corticomedullary junction in the middle portion of the kidney using different b values ( 300 , 500 and 800 s / mm2 ) to analyse measurement repeatability and assess the influence of hydration status on adc . dove debba essere localizzata la roi per il calcolo del valore di adc . 
inoltre descritta una relazione inversa tra valore di b e valori di adc e uninfluenza dello stato di idratazione sui valori di adc misurati [ 8 ]  . scopo del nostro lavoro stato calcolare in soggetti volontari sani il valore medio di adc renale a livello della giunzione corticomidollare in sede mesorenale , sia su piano assiale che coronale , utilizzando valori di b differenti ( 300 , 500 , 800 s / mm2 ) ; analizzare la ripetibilit di tali misurazioni e valutare linfluenza dello stato di idratazione sui valori di adc . materials and methods materiali e metodi between march and july 2006 , we performed dw - mri examinations in ten healthy volunteers ( four women , six men , mean age 284 , range 2439 years ) with no previous history of kidney disease , hypertension , diabetes or other vascular disease . 
all subjects gave informed consent . the examinations were performed with a 1.5 - t device ( signa excite , ge medical systems , milwaukee , wi , usa ) with an abdominal phased - array coil . 
we performed a preliminary breath - hold assessment of the kidney with t1weighted gradient echo ( gre ) sequences in phase and in phase opposition relative to the fat signal [ repetition time / echo time ( tr / te ) 150 / 2.24.4 ] and t2 - weighted single - shot sequences ( tr / te 1 , 126 / 89.9 ) in the axial and coronal planes . 
these were followed by dw - mri using a single - shot echoplanar imaging ( se - epi ) breath - hold sequence acquired in the axial and coronal planes with the field of view ( fov ) centred on the middle portion of the kidney . the following se - epi sequence parameters were used : 16 slices , slice thickness 7 mm , gap 1 mm , tr 2 , 883 ms , te 61 ms , flip angle 90 , mean fov 320 ( range 300340 mm ) and matrix 128256 . 
sequences were performed along the three orthogonal directions to minimise the effects of anisotropy and were repeated using different b values ( 0 , 300 , 500 and 800 s / mm2 )  . 
adc maps were then calculated for the different weightings : b 0300 , b 0500 and b 0800 . three rois approximately 1 cm in diameter were positioned in both kidneys of each subject . 
in the axial maps , the rois were positioned at the level of the middle portion of the kidney ( anterior labrum , posterior labrum and intermediate site )  . 
in the coronal maps , the rois were positioned at the corticomedullary junction at the level of the upper pole , the middle of the kidney and the lower pole [ 10 ]  . 
each adc value expressed in mm2 / s was calculated on the basis of the following equation : nel periodo marzo - luglio 2006 dieci soggetti volontari sani ( 4 donne , 6 uomini ; et media 284 anni , range 2439 anni ) senza storia di malattie renali , ipertensione , diabete o altra patologia vascolare sono stati selezionati per eseguire studio rm - dw . 
tutti i soggetti esaminati hanno dato il loro consenso informato allo studio . gli esami sono stati condotti con magnete superconduttivo a 1 , 5 t ( signa excite , ge medical systems , milwaukee , wi , usa ) con bobina phasedarray per uso addominale . dopo una preliminare valutazione morfologica renale con sequenze in respiro sospeso : gre t1 pesate in fase e in opposizione di fase relativamente al segnale dei lipidi ( tr / te : 150 / 2 , 24 , 4 ) e single shot t2 pesate ( tr / te 1126 / 89 , 9 ) su piano assiale e coronale , stato condotto lo studio rm - dw utilizzando una sequenza single - shot spinecho echoplanare ( se - epi ) in respiro sospeso , acquisita per piano assiale e per piano coronale , con centratura del fov sul mesorene . i parametri della sequenza se - epi erano ( 16 strati , spessore di strato 7 mm , gap 1 mm ; tempo di ripetizione , tr = 2883 ; tempo di eco , te = 61 ms , flip angle = 90 , campo di vista medio 320 mm ( range 300340 mm ) , matrix 128256 ) ; la sequenza stata eseguita con gradienti di diffusione applicati nelle tre direzioni ortogonali x , y , z al fine di minimizzare gli effetti legati allanisotropia , e ripetuta utilizzando diversi valori di b ( 0 , 300 , 500 , 800 s / mm2 )  . 
 stata quindi calcolata mappa delladc per le diverse pesature : b 0300 ; 0500 e 0800 . per ogni soggetto sono state quindi posizionate tre roi per rene del diametro approssimativo di 1 cm ; nelle mappe assiali le roi sono state posizionate a livello del piano passante per il mesorene : una roi a livello del labbro anteriore , una nel labbro posteriore e una intermedia . 
the mean of the six adc values derived from the six rois ( three in the left kidney and three in the right ) was then calculated in both the axial and coronal plane . 
in addition , mean adc was calculated for each b value and in the different states of hydration . normal hydration ( nh ) was defined as the volemic state resulting from the free intake of food and water , hyperhydration ( hy ) as that resulting from the intake of 20 ml / kg body weight of water in the hour prior to the examination , and dehydration ( dhy ) from the complete abstinence from food and water for 12 h prior to the examination . urine samples were collected immediately before the examination and assessed for urine osmolarity ( osmu ) and sodium excretion ( nau )  . 
i valori medi di adc sono stati calcolati per ogni valore di b e nei diversi stati di idratazione . stata definita normoidratazione ( nh ) lo stato volemico conseguente ad una libera assunzione di cibo e acqua , stato di carico idrico ( hy ) quello conseguente allassunzione di 20 ml / kg peso corporeo di acqua nellora precedente lesame ; e stato di restrizione idrica ( dhy ) quello conseguente alla mancata assunzione di cibo ed acqua nelle 12 ore precedenti lesame . prima di ogni esame sono state controllate losmolarit urinaria ( osmu ) e la sodiuria ( nau ) su un campione di urine ottenuto subito prima dellesame . 
i valori di osmolarit urinaria sono stati calcolati valutando il punto di congelamento con micro - osmometer ( advanced instruments inc . , massachussets , usa ) ; la sodiuria stata dosata con metodo colorimetrico utilizzando un synchron clinical system cx3 delta ( beckman , coulter , usa )  . 
al fine di valutare la ripetibilit dellindagine e dei risultati , 5 soggetti hanno ripetuto lo studio dopo circa 3 mesi dalla prima valutazione , nelle stesse condizioni cliniche ed emodinamiche . 
lanalisi statistica stata condotta con software dedicato spss versione 13.0 , utilizzando test t di student per dati appaiati e considerando significative p < 0 , 05 . results risultati morphological assessment of the kidneys of the healthy volunteers revealed no significant abnormalities , with the exception of two cortical cysts smaller than 1 cm in two subjects . 
in addition , the adc values for the same b values revealed no statistically significant differences in the various states of hyla valutazione morfologica dei reni dei soggetti volontari sani esaminati non ha mostrato anormalit di rilievo , ad eccezione di 2 millimetriche cisti corticali ( diametro < 1 cm ) in 2 soggetti . 
inoltre i valori di adc , a parit di valore di b , non risultano statisticamente differenti nei diversi stati di radiol med ( 2008 ) 113 : 214224 fig . 
2a - c mappa del coefficiente di diffusione apparente ( adc ) su piano assiale in un volontario sano di 30 anni con reni normali ottenuta con valore di b = 0 , 300 ( a ) ; 0 , 500 ( b ) ; 0 , 800 ( c ) : i valori medi di adc sono misurati posizionando 3 regioni di interesse ( roi ) su ciascun rene a livello di un piano passante per il mesorene ( labbro anteriore , labbro posteriore e in regione intermedia )  . radiol med ( 2008 ) 113 : 214224 fig . 
i valori di osmu e nau sono invece risultati statisticamente differenti nei differenti stati di idratazione sia nello studio basale sia nello studio di controllo ( tabella 3 )  . discussion magnetic resonance offers numerous interesting diagnostic possibilities in nephrology . 
mri is , in fact , the only technique capable of measuring molecular diffusion in tissues , thanks to the use of additional dephasing gradients , which produce a reduction in signal intensity proportional to the motion of water molecules in tissues [ 5 ]  . discussione la risonanza magnetica in campo nefrologico offre interessanti possibilit diagnostiche , ad oggi ancora parzialmente inesplorate , soprattutto per quello che riguarda lassociazione tra dato anatomico e dato funzionale , avendo la potenzialit di fornire , in un unico esame , una valutazione completa del processo patologico in studio [ 11 ]  . lutilizzo infatti di apparecchiature ad alto campo e lintroduzione di nuove sequenze ultrarapide ha aperto la strada a nuove tecniche di indagine , una tra queste la quantificazione dei moti browniani delle molecole dacqua tissutali ( o immagine pesata in diffusione )  . 
however , before assessing the clinical implications of these measurements , optimal sequence parameters need to be defined , as well as how the patient should be prepared for the examination ( with regard to hydration status ) and how data te che potr entrare a far parte dei protocolli clinici di risonanza magnetica nello studio del rene , vista anche la rapidit di esecuzione di tali sequenze . 
prima di valutare i possibili risvolti clinici di queste misurazioni , resta tuttavia ancora da definire quali siano i parametri ottimali della sequenza , come debba essere preparato il paziente allesame ( relativamente allo stato di idratazione ) , e come debbano 222 radiol med ( 2008 ) 113 : 214224 should be interpreted [ 812 ]  . 
indeed , as described above , diffusion - weighted data correspond to the total microscopic translations that take place within the voxel the intravoxel incoherent motions ( ivim ) which , as well as the diffusion of water molecules , includes the microcirculation of blood ( perfusion ) [ 5 ]  . 
this probably explains why the kidney , being highly perfused , has adc values measured at the level of the parenchyma that are much higher than those of other organs [ 813 ]  . 
to this end , we used a singleshot breath - hold se - epi sequence and adapted the parameters to obtain data comparable with the literature , using diffusion gradients in the x , y and z planes to minimise the effects of anisotropy [ 14 ]  . we also decided to place the rois at the level of the corticomedullary junction in the middle portion of the kidney and not selectively in the cortex or medulla . 
placing rois separately in the two sites is difficult , as other studies have demonstrated [ 10 , 14 ] , because of the low spatial resolution of epi and motion artefacts , particularly in breath - hold dwmri sequences with high b values , at least with regard to studying the native kidney . 
 [ 8 ] reported that adc measurements varied widely with different states of hydration of the patient . with regard to adc parameters , our data are in agreement with those reported in the recent literature . 
the values calculated on maps obtained by dw - mr images with b = 500 were 2.470.2910 - 3 mm2 / s , range 2.043.1210 - 3 mm2 / s . 
 [ 15 ] , who used a different dw - mri sequence with free breathing with a duration of about 9 min : this sequence was less susceptible to motion artefacts and produced images of acceptable quality , even at high b values , but essere interpretati i dati [ 812 ]  . 
infatti , i dati relativi alla pesatura in diffusionecorrispondono , come precedentemente descritto , allinsieme delle microscopiche traslazioni che si verificano allinterno del voxel , i cosiddetti ivim o intravoxel incoherent motions che includono oltre alla diffusione delle molecole dacqua anche la microcircolazione del sangue ( perfusione ) [ 5 ]  . 
pertanto il valore di adc renale in vivo include tanto gli effetti della diffusione propriamente detta o vera , quanto quelli della perfusione ( pseudodiffusione ) ; quanto pi si aumenta la pesatura in diffusione ( ossia il valore di b della sequenza ) tanto pi si misura il coefficiente di diffusione vero e proprio [ 14 , 15 ]  . tuttavia , in campo addominale , lutilizzo di alti valori di b determina una bassa risoluzione spaziale e un basso rapporto segnale rumore delle immagini con conseguente scarsa qualit e limitata ripetibilit delle valutazioni . 
infatti , stata descritta da muller et al . [ 8 ] una variabilit delle misurazioni in relazione al diverso stato di idratazione del paziente . i nostri dati risultano , per quanto riguarda i parametri di adc , sovrapponibili a quelli riportati nella recente letteratura . 
 [ 8 ] , we failed to encounter a significant influence of hydration status on adc data measured with b values of 300 , 500 and 800 s / mm2 . 
it is surprising that a major increase in urinary output due to drug - induced diuresis failed to cause substantial changes in the adc value . hydration status and urinary output are , in fact , highly correlated due to the action of adh at the level of the renal tubules . 
the differences observed could simply be secondary to different methods of roi placement and different b values used with different weightings in true diffusion . the limitations of our study are both the low number of cases and the fact that the subjects were all young and healthy . 
dw - mr images with intermediate weighting ( b = 500 ) can be seen as an acceptable compromise between image quality , signal - to - noise ratio and true diffusion weighting , with acceptable acquisition times . 
on the basis of data obtained in normal conditions , the diffusion - weighed technique can be applied to studying the pathological kidney , with the aim of identifying clinical situations in which diffusion measurement can be beneficial . lizzata una sequenza rm - dw differente in respiro libero , della durata di circa 9 minuti , meno suscettibile ad artefatti da movimento e con qualit di immagine accettabile anche ad alti valori di b , a spese tuttavia del tempo di acquisizione totale . 
questi autori hanno segnalato una differenza significativa dei valori di adc in soggetti volontari sani in stato di disidratazione vs idratazione ( 2 , 9 vs 3 , 610 - 3 mm2 / s ) senza tuttavia evidenziare , nellanimale da esperimento , una significativa correlazione tra adc e flusso urinario ( con variazioni del flusso urinario da 2 , 4 a 16 ml / min )  . 
sorprendente che un importante incremento del flusso urinario da diuresi farmacoindotta non determini sostanziali modificazioni delladc ; infatti stato di idratazione e flusso urinario sono strettamente correlati tra loro tramite lazione delladh a livello tubulare . 
le differenze osservate potrebbero semplicemente essere secondarie alle differenti modalit di posizionamento delle roi e ai diversi valori di b usati con differente pesatura in diffusione vera . i limiti del nostro studio sono legati sia al numero esiguo di casi studiati sia al fatto che lo stesso sia stato eseguito su soggetti giovani e sani . 
inoltre i soggetti da noi esaminati hanno unet relativamente giovane e omogenea ( range 2439 ) mentre , come precedentemente segnalato da thoeny , esiste una verosimile graduale lenta riduzione dei valori fisiologici di adc con let [ 15 ]  . 
sulla base della nostra esperienza si pu ipotizzare di poter studiare i pazienti con rm - dw in normoidratazione e quindi durante il normale svolgimento di un esame di routine ; le immagini rm - dw con pesatura intermedia ( b value = 500 ) possono costituire , per una valutazione quali - quantitativa della diffusione renale , un compromesso accettabile tra qualit delle immagini , rapporto segnale / rumore e pesatura in diffusione vera , con tempi di acquisizione accettabili . 
manganaro1 1dipartimento di scienze radiologiche , 2dipartimento di ostetricia e ginecologia , universit degli studi di roma la sapienza , via regina elena 324 , 00161 roma , italy correspondence to : a . 
we used the following imaging protocol : t2 - weighted single - shot fast spin - echo sequences for all foetuses and , in selected cases , gradient echo with steadystate free precession ( ssfp ) , t1 - weighted spoiled gradient echo [ fast low - angle shot ( flash ) ] with and without fat saturation , and t2 thick - slab sequences with multiplanar technique . 
mri confirmed the positive us diagnosis in 67 of 109 cases ( 61.5% ) ; in 11 cases it changed the us diagnosis , and in 31 / 109 the examination was negative . 
abbiamo utilizzato il seguente protocollo : per tutti i feti sequenze t2 pesate single shot fast spin echo e in casi selezionati sequenze gradient echo con tecnica steady state free precession ( ssfp ) , sequenze spoiled gradient echo t1 pesate ( fast low angle shot , flash ) con e senza saturazione del segnale del grasso e sequenze t2 thick slab acquisite con tecnica multiplanare . 
nei 16 casi gi negativi allecografia , lrm ha confermato il risultato ecografico . lrm ha confermato come positive 67 diagnosi ecografiche su 109 casi ( 61 , 5% ) ; in 11 casi , invece , lrm ha modificato la diagnosi ecografica ed in 31 pazienti lesame risultato negativo . 
lrm fetale , grazie alle sequenze ultra - fast , consente di visualizzare buoni dettagli dellanatomia fetale e di caratterizzare sospette anomalie . parole chiave patologia fetale risonanza magnetica ecografia 226 introduction ultrasonography ( us ) is the technique of choice for the screening foetal anomalies because it provides images in real time with excellent spatial resolution and presents no risks to mother or foetus . 
in addition , in complex fetal anomalies , us is not always able to provide sufficiently diagnostic information in terms of management of the pregnant patient . the growing number of cases of litigation brought against the gynaecologist therefore has led to the use of additional imaging techniques to complement us . 
magnetic resonance imaging ( mri ) can be used as a second - line technique and an adjunct to us in the study of obstetric disorders , and in particular to assess a number of pathologies affecting the foetus , the gravid uterus and the placenta . 
the main international guidelines ( safety committee of the society of magnetic resonance imaging ) , however , advise that the examination be performed in the second or third trimester of gestation when a preliminary us examination proves inadequate or inconclusive . in this study we report our experience with mri in the assessment of the foetus for definition of he anatomical structures and the main fetal pathologies . materials and methods our retrospective study involved 128 pregnant women between the 22nd and 38th week of gestation ( wg ) ( mean 27th wg ) who visited our centre between february 2002 and july 2006 for an obstetric mri examination . 
informed consent was obtained from all patients before performing the examinations . in most cases ( 112 / 128 ) , the indication for mri was the need to further assess fetal anomalies previously visualised at obstetric us but not fully characterised . 
in these cases , the mri study was confined to the anatomical area of interest : 46 examinations were performed to assess the head , 17 the amniotic fluid , 12 the urinary system , nine to provide an overall assessment of the foetus ( six due to growth restriction , two due suspected platyspondylia and dwarfism and one due to complex malformation ) , eight thorax , eight the radiol med ( 2008 ) 113 : 225241 introduzione lecografia ( eg ) rappresenta la metodica elettiva per lo screening delle anomalie fetali poich fornisce immagini in real time con ottima risoluzione spaziale e non presenta aspetti nocivi per la madre e per il feto . 
nel caso di anomalie fetali complesse , inoltre , leg non sempre consente di ottenere informazioni sufficientemente diagnostiche ai fini della gestione terapeutica della paziente in gravidanza . le crescenti problematiche medico - legali che investono il ginecologo impongono pertanto il ricorso ad altre metodiche di imaging complementari allecografia . 
la risonanza magnetica ( rm ) si pone come metodica di seconda scelta , di supporto alleg , nello studio della patologia ostetrica in particolare per lo studio di alcune patologie fetali , dellutero gravidico , e della placenta . 
la rm ostetrica consente di ottenere informazioni dettagliate grazie allelevata risoluzione spaziale e di contrasto delle sequenze ultrarapide di ultima generazione e alla possibilit di valutazioni multiplanari ; non una metodica strettamente operatore - dipendente ma la sua comprensione comunque subordinata allottima conoscenza dellanatomia fetale normale . 
allo stato attuale non stato dimostrato che essa pu indurre danni al feto per campi di esposizione inferiori a 1 , 5 tesla ; le maggiori linee guida internazionali ( safety committee of the society for magnetic resonance imaging ) consigliano comunque di eseguire lesame nel ii o iii trimestre di gravidanza quando un preliminare esame ecografico risulti inadeguato e comunque inconclusivo nella diagnosi . 
 in questo studio riportiamo la nostra esperienza con la rm nella valutazione del feto per la definizione delle strutture anatomiche e delle principali patologie fetali . materiali e metodi stato condotto uno studio retrospettivo su 128 donne in stato di gravidanza tra la 22a e la 38a settimana di gestazione ( media 27a settimana ) che , dal febbraio 2002 al luglio 2006 , si sono recate presso il nostro dipartimento di scienze radiologiche per sottoporsi ad un esame di risonanza magnetica ostetrica . 
 nella maggior parte dei casi ( 112 / 128 ) lindicazione alleffettuazione della rm stata la necessit di unulteriore valutazione di anomalie fetali precedentemente visualizzate con lecografia ostetrica ma non del tutto caratterizzate . 
al momento dellesame rm , quindi , lo studio stato radiol med ( 2008 ) 113 : 225241 placenta and annexes , seven the abdominal wall and abdomen and two the facial region . three of the 112 cases were twin pregnancies , and although the indication for mri was to evaluate specific abnormalities identified at us ( gastroschisis , omphalocele and suspected twin - to - twin transfusion syndrome ) , the examination was aimed at the overall assessment of the growth of both foetuses . 
in the remaining 16 cases , the patients presented with a negative us examination , and the indication for mri was a previous abnormal pregnancy ( three cases ) , a foetus with a chromosome disease ( three cases ) , a mother with a recent cytomegalovirus infection ( three cases ) or toxoplasmosis ( one case ) , twin pregnancy ( two additional cases ) , eclampsia ( three cases ) and maternal foggy vision and dysarthria ( one case )  . 
we used the following protocol ( table 2 ) for all foetuses : t2 - weighted single - shot fast spin - echo sequences [ ssfse in the modified version with half - fourier acquisition ( haste ) ] oriented in the coronal plane of the mother to identify the position of the foetus and followed by the same sequences in the axial , coronal and sagittal planes of the foetus and particularly of the organ ( s ) of interest to characterise the fetal anomaly . 
images of each series were used as scout views for the following sequences to minimise orientation problems related to changes in foetus position . in specific cases , we also used breath - hold gradient - echo sequences with the ssfp [ true fast imaging with steadystate precession ( fisp ) for our device ] , t2 thick - slab sequences acquired with the multiplanar technique on the foetus and t1 - weighted spoiled gradient - echo sequences [ fast low - angle shot ( flash ) ] with and without fat signal saturation . 
we also performed diffusion - weighted imaging ( dwi ) sequences on 32 foetuses aimed at the brain , kidneys and lungs ( b value 400700 s / mm2 for the brain , 200700 s / mm2 for the lungs and 200500 s / mm2 for the kidneys ) with gradients in the three spatial axes . 
overall examination time was between 15 and 20 min , even in cases where fetal motion required the same sequence to be repeated twice consecutively . the mr images were consensually evaluated by two radiologists with experience in both mri ( 10 years of experience ) particularly imaging of the pelvis and normal feorientato verso larea anatomica dinteresse ; in particolare 46 esami sono stati mirati alla valutazione del cranio , 17 alla valutazione del liquido amniotico , 12 a quella dellapparato urinario , 9 mirati allo studio complessivo del feto ( 6 per ritardo di crescita , 2 per sospetta platispondilia e nanismo , 1 malformazione complessa ) , 8 allo studio del torace , 8 allo studio della placenta e degli annessi , 7 allo studio della parete addominale e delladdome , 2 allo studio del massiccio facciale . in 3 dei 112 casi sopra citati la gravidanza era bigemellare , e nonostante lindicazione alla rm fosse per precise anomalie segnalate alleg ( schisi addominale , onfalocele e sospetta stuck syndrome ) , lesame stato mirato comunque alla valutazione complessiva dellaccrescimento di entrambi i feti . 
nei restanti 16 casi le pazienti si sono presentate con un esame ecografico negativo e il ricorso alla rm stato cos motivato : precedenti gravidanze anomale ( 3 casi ) , feti portatori di una cromosomopatia ( 3 casi ) , madri portatrici di uninfezione recente da citomegalovirus ( 3 ) o toxoplasma ( 1 ) , gravidanza bigemellare ( altri 2 casi ) , eclampsie ( 3 casi ) , annebbiamento del visus e disartria materna ( 1 caso )  . 
pure in questi casi stato eseguito uno studio complessivo del feto ( tabella 1 )  . lo studio stato eseguito con un magnete da 1 , 5 tesla ( siemens magneton plus fino al gennaio 2006 , successivamente siemens avanto , enlargen , germania ) , con la paziente in posizione supina o in decubito laterale sinistro nei casi in cui la madre non tollerava la posizione supina ( es : compressione cavale ) ; alle donne era permesso di rilassarsi allinterno del magnete per qualche istante prima dellesame per ridurre il movimento spontaneo fetale . 
stato utilizzato il seguente protocollo ( tabella 2 ) : per tutti i feti , sequenze t2 pesate single shot fast spin echo ( ssfse , nella versione modificata con acquisizione half - fourierhaste ) , orientate sul piano coronale della madre per lindividuazione della posizione fetale ed in seguito le stesse sequenze sono state orientate sui piani assiale , coronale e sagittale del feto ed in particolare dellorgano / i di interesse per una caratterizzazione di dettaglio dellanatomia fetale . le immagini dogni serie sono state utilizzate come scout per le sequenze successive in modo da minimizzare i problemi di orientamento legati al cambiamento della posizione fetale . in casi specifici abbiamo utilizzato anche sequenze gradient echo con tecnica steady state free precession ( ssfp , true - fisp per la nostra apparecchiatura ) breath hold ; sequenze t2 thick slab acquisite con tecnica multiplanare sul feto ; sequenze spoiled gradient echo t1 pesate ( fast low angle shotflash ) con e senza saturazione del segnale del grasso . 
gastrointestinale ( 7 ) torace ( 8 ) massiccio facciale ( 2 ) liquido amniotico ( 17 ) placenta e annessi ( 8 ) studio complessivo del feto ( 12 ) negativo ( 16 ) studio complessivo del feto growth restriction ( 6 ) platyspondylia and dwarfism ( 2 ) complex malformation ( 1 ) twin pregnancy ( 3 ) twin pregnancy ( 2 ) chromosome disease ( 3 ) maternal infection previous abnormal pregnancies ( 3 ) eclampsia ( 3 ) maternal foggy vision and dysarthria ( 1 ) cmv ( 3 ) toxoplasmosis ( 1 ) ritardo crescita ( 6 ) platispondilia e nanismo ( 2 ) malformazione complessa ( 1 ) grav . 
bigemellare ( 2 ) cromosomopatia ( 3 ) infezione materna cmv ( 3 ) toxoplasma ( 1 ) precedenti gravidanze anomale ( 3 ) eclampsia ( 3 ) annebbiamento visus e disartria materna ( 1 ) cmv , citomegalovirus tal anatomy . 
secondly , in all cases where mri identified a fetal pathology , the importance of the mr assessment was studied in terms of the correct identification of the pathology , also in comparison with us findings . 
these values were not calculated for the us examination in that the technique in many cases identified the anomalous region without providing a diagnosis . results we excluded from the analysis the 16 cases with negative us findings that also proved negative at mri and for which no fetal anomaly was observed at clinical - imaging postnatal follow - up . 
in one case , the mri examination was not completed due to claustrophobia . comparison between mri and postnatal clinical - imaging findings produced the following : sensitivity 92.4% ( 73 / 79 ) , specificity 78.1% ( 25 / 32 ) , ppv 91.2% ( 73 / 70 ) and npv 80.6% ( 25 / 31 )  . 
false negative cases included a heart malformation identified at us in which mri was unable to identify the heart with the required anatomical detail , and a suspected renal agenesis in which sharp and conclusive images capable of confirming or rejecting us suspicion could not be obtained due to fetal motion . 
in secondo luogo , in tutti quei casi in cui lesame rm ha individuato una patologia del feto , stata studiata limportanza della valutazione con risonanza magnetica ai fini del corretto inquadramento della patologia , anche in confronto con il dato ecografico . 
i risultati ottenuti con risonanza magnetica sono stati confermati o confutati dagli esami clinico - strumentali effettuati prima e dopo la nascita ed in alcuni casi dallautopsia post - natale ( dopo il termine legale della gravidanza o aborto spontaneo ) , che hanno rappresentato quindi il nostro gold standard . 
in seguito , abbiamo calcolato i valori di sensibilit , specificit , valore predittivo negativo e positivo dellesame di risonanza magnetica ; i suddetti valori non sono stati calcolati , invece , per lesame ecografico poich in molti casi questultimo ha indicato il distretto anomalo senza porre una diagnosi . risultati abbiamo escluso dallanalisi dei risultati i 16 casi negativi allesame eg , giunti alla nostra osservazione per i motivi sopra riportati , e risultati negativi anche allesame rm , che non ha riscontrato alcunanomalia fetale , ed ai successivi controlli clinico - strumentali post - natali . 
of particular interest were the cases of a twin pregnancy with gastroschisis of a foetus where a sacrococcygeal teratoma was identified , and the two cases of growth restriction in which lung immaturity was diagnosed in one and dilatation of the occipital horns in the other . 
in particolare , i casi falsi negativi fanno riferimento ad una malformazione cardiaca , identificata con lesame eg , in cui la rm non riuscita ad evidenziare con il giusto dettaglio anatomico il cuore e ad una sospetta agenesia renale in cui , a causa del notevole movimento fetale , non stata possibile lacquisizione di immagini nitide e conclusive tali da poter escludere o confermare il sospetto ecografico . 
la rm inoltre non stata in grado di identificare la presenza di calcificazioni epatiche , a causa delle piccole dimensioni e del segnale ipointenso in tutte le sequenze utilizzate ; ha diagnosticato come previa una placenta che al momento del parto risultata increta ; ed infine non ha riconosciuto il ritardo di crescita in due feti . 
nei casi sopra descritti , fatta eccezione per la valutazione della placenta , lesame ecografico risultato invece dirimente . per quanto riguarda , invece , i casi falsi positivi in 6 casi su 7 si tratta di dilatazione non marcata degli spazi liquorali non pi evidente alla nascita ed in un caso diagnosticato come ipoplasia polmonare sulla base dellintensit di segnale nelle sequenze t2 - pesate . 
 dal confronto tra dato ecografico e risonanza magnetica emerso un sostanziale accordo tra le due metodiche in 67 casi sui 109 gi positivi allesame eg ( 61 , 5% , abbiamo escluso dal confronto i 2 casi non diagnostici ) , ed in 10 di questi 67 ha consentito lindividuazione e lapprofondimento delle anomalie segnalate ( la dilatazione degli spazi liquorali stata per confutata alla nascita come detto prima )  . nel 10 , 1% dei casi ( 11 / 109 ) lapporto della rm stato determinante nel riconoscimento della patologia ponendo una esatta diagnosi , differente rispetto allesame eg . 
infine nel 28 , 4% dei casi ( 31 / 109 ) non ha mostrato alcuna alterazione , considerando i feti e gli annessi completamente negativi ; 3 casi di questi , ovvero le calcificazioni epatiche e i ritardi crescita non sono stati confermati alla nascita . in 8 casi inoltre stato possibile documentare nuove anomalie fetali misconosciute al precedente esame ecografico ; di particolare interesse sono stati i casi di una gravidanza gemellare con schisi addominale di un feto in cui stato evidenziato anche un teratoma sacrococcigeo , di due ritardi di crescita in cui sono state documentate rispettivamente una scarsa maturazione polmonare ed una dilatazione dei corni occipitali . 
in due casi di anidramnios la rm ha consentito di stabilirne la causa cio lagenesia renale bilaterale , ed in un caso di feto con idronefrosi stata riscontrata unipoplasia polmonare associata . analizzando i diversi apparati abbiamo osservato che nei casi di sospette alterazioni a carico del distretto testa - collo la rm ha confermato ed approfondito il dato ecografico in radiol med ( 2008 ) 113 : 225241 fig . 
2a , b sequenza ssfp assiale ( a ) e coronale ( b ) : idrocefalo con dilatazione massiva dei ventricoli laterali ; si associa appiattimento dei solchi e riduzione del parenchima cerebrale . 232 radiol med ( 2008 ) 113 : 225241 fig . 
6a - c left multicystic kidney ; coronal steady - state free precession t2weighted ( a ) and diffusion - weighted with b values = 0 ( b ) and 500 s / mm2 ( c ) images . 
nelle immagini in diffusione con b = 500 s / mm2 si osserva una perdita dellintensit di segnale . of amniotic fluid ( 13 out of 17 ) and in the assessment of placental implantation ( eight out of eight )  . the greatest amount of disagreement between mri and us was in assessment of growth restriction ( two cases confirmed out of six foetuses studied ) and in complex skeletal malformations ( different diagnosis in two out of two cases )  . discussion whereas it is still the technique of choice for the study of fetal anomalies , in some circumstances , obstetric us provides indicative information that is nonetheless not sufficiently conclusive for a therapeutic decision . 
7a , b coronal steady - state free precession t2 - weighted images at the 24th ( a ) and 31st ( b ) weeks of gestation ( wg )  . 
alla 31a settimana di gestazione si osserva una regressione quasi totale della malformazione e mediastino in sede . for reasons of maternal origin , such as obesity or the presence of large uterine fibroids , and for reasons of fetal origin , such as oligohydramnios or unfavourable fetal position . 
 il maggiore dissenso tra rm ed ecografia si avuto nella valutazione dei sospetti ritardi di crescita ( 2 conferme su 6 feti studiati ) e delle malformazioni scheletriche complesse ( diagnosi differente in 2 casi su 2 )  . discussione pur rimanendo la metodica di scelta per lo studio delle anomalie fetali , lecografia ostetrica in alcune circostanze fornisce informazioni indicative , ma non conclusive per una decisione terapeutica ; in altre risulta tecnicamente difficile da eseguire sia per cause di origine materna come lobesit o la presenza di grandi fibromi uterini sia per cause di origine fetale come loligo - anidramnios o la posizione non favorevole del feto . 
in questi casi la rm si pone come modalit di imaging complementare . in passato la rm pelvica era stata utilizzata durante la gravidanza per valutare la normale anatomia materna e sue eventuali anomalie ( es : masse annessiali che richiedevano una caratterizzazione pi precisa ) , mentre lanatomia fetale non era adeguatamente visualizzata con le sequenze convenzionali a causa dei tempi dacquisizione relativamente lunghi [ 1 , 2 ]  . 
questo problema stato superato in seguito allintroduzione di sequenze veloci ed ultraveloci ( < 1 s ) t1 e t2 - pesate che hanno sensibilmente ridotto i tempi di acquisizione e quindi gli artefatti da movimento fetale , senza necessit di ricorrere alla sedazione [ 35 ]  . un nostro protocollo tipico per lo studio fetale include sequenze ssfse t2 pesate , ssfp , spoiled gradient echo t1 pesate e sequenze in diffusione ; talora anche sequenze inversion recovery con per la soppressione del liquor ( flair ) e sequenze t2 pesate thick - slab . 
 le sequenze che hanno rivoluzionato limaging con rm sono state le sequenze ssfse pesate in t2 che offrono un ottimo compromesso tra la risoluzione dellimmagine e il rapporto segnale - rumore ( snr ) [ 6 ]  . 
il loro vantaggio principale rappresentato dalla rapidit , infatti , lacquisizione totale dei dati inferiore ad 1 secondo per cui si pu ottenere unimmagine priva di artefatti senza necessit di apnea respiratoria ( breath hold ) per la madre . 
queste sequenze mostrano lanatomia fetale in maniera eccellente durante tutte le fasi della gravidanza ed in particolare possono essere applicate allo studio dellencefalo fetale , delle cavit contenenti fluidi ( cavit nasali ed orale , faringe , trachea , stomaco e piccolo intestino , sistema urinario , colecisti ) , dei polmoni , della placenta e della superficie fetale [ 3 , 6 ]  . 
in a i polmoni normali appaiono iperintensi ( adc = 1 , 420 , 1110 - 3 mm2 / s ) in accordo con let gestazionale ; nellimmagine b , invece , si osserva un ritardo dello sviluppo polmonare ( adc = 1 , 420 , 1110 - 3 mm2 / s ) mentre nella parte c una maturazione polmonare normale ( adc = 2 , 410 , 1110 - 3 mm2 / s ) alla stessa settimana di gestazione . in the past , pelvic mri was used during pregnancy to assess normal uterine anatomy and possible anomalies ( e.g. adnexal masses that require more precise characterisation ) , whereas fetal anatomy was not adequately visualised with conventional sequences due to the relatively long acquisition times [ 1 , 2 ]  . 
this problem was overcome with the introduction of fast and ultrafast t1and t2 - weighted sequences ( < 1 s ) , which significantly reduced acquisition times and therefore fetal motion artefacts without the need for sedation [ 35 ]  . a typical protocol used at our centre for the study of the foetus includes t2 - weighted ssfse sequences , ssfp sequences , t1 - weighted spoiled gradient - echo and diffusionweighted sequences . 
inversion recovery sequences for csf suppression ( flair ) and t2 - weighted thick - slab sequences are also sometimes used . sequences that have revolutionised mri are t2 - weighted ssfse sequences , which provide an excellent compromise between image resolution and signal - to - noise ratio ( snr ) [ 6 ]  . 
their main advantage is their speed ; in fact , total acquisition time is less than 1 s , such that images free from artefacts are obtained without the need for breath - holding . these sequences display fetal anatomy with excellent detail cambiare alcuni parametri per poter ottenere un buon contrasto . 
per questa ragione sono generalmente utilizzate le sequenze gradient echo t1 / t2 pesate ssfp , essenziali soprattutto per lo studio della maturazione cerebrale nel terzo trimestre grazie alla loro rapidit , scarsa sensibilit al movimento , ed alto rapporto segnale - rumore ; il limite di queste sequenze rappresentato dal largo fov che esse richiedono e che pu impedire lidentificazione di piccoli dettagli [ 7 , 8 ]  . per quanto riguarda le sequenze t1 pesate possono essere utilizzate vari tipi di sequenze con e senza la soppressione del grasso , ma le migliori sono le spoiled gradient echo che forniscono immagini di alta qualit soprattutto nello studio delladdome [ 9 ]  . 
alcuni organi e tessuti possono essere selettivamente visualizzati nelle sequenze t1 pesate in virt della loro alta intensit di segnale ; in particolare pu essere studiata la ghiandola tiroide e pu essere preventivamente individuato un eventuale gozzo o unectopia tiroidea . 
anche il fegato e le anse intestinali contenenti meconio mostrano un segnale elevato , cos come i focolai emorragici contenenti metaemoglobina ed alcune strutture encefaliche a partire dalla 24a settimana quali il piatto corticale , il cervelletto e i gangli della base [ 1013 ] , mentre le calcificazioni possono essere dedotte dal loro basso segnale [ 14 ]  . 236 radiol med ( 2008 ) 113 : 225241 throughout the entire gestation , and they can be applied to the study of the fetal brain , fluid - containing cavities ( nasal and oral cavities , pharynx , trachea , stomach and small intestine , urinary system , gall bladder ) , the lungs , the placenta and the fetal surfaces [ 3 , 6 ]  . in larger foetuses , beyond the 35th wg , some parameters need to be changed to obtain good contrast . 
for this reason , t1 / t2 - weighted ssfp gradient - echo sequences are used , particularly for the study of brain maturation in the third trimester , thanks to their speed , limited sensitivity to motion and high snr . 
the main limitation of these sequences is that they require a large field of view , which can impede the identification of small details [ 7 , 8 ]  . various types of t1 - weighted sequences can be used with and without fat saturation , but the best are spoiled gradient - echo sequences , which provide high quality images particularly in the study of the abdomen [ 9 ]  . 
the liver and the bowel loops containing meconium also show an elevated signal , as do haemorrhagic foci containing methaemoglobin and some cerebral structures from the 24th wg on , such as the cortical plate , the cerebellum and the basal ganglia [ 1013 ] , whereas calcifications can be deduced by their low signal [ 14 ]  . 
the healthy placenta appears homogeneously hypointense in t1 - weighted sequences , but venous stasis and / or thromboses may cause hyperintense foci . in addition , over the last few years dwi sequences have been introduced into routine practice . 
although dwi sequences were initially used in the study of brain maturation , recent studies suggest their use in the study of pulmonary and renal maturation [ 1518 ]  . 
to eliminate the effects of these parameters , adc maps can be generated in which the areas of reduced motility of the water molecules appear hypointense . the most important contribution of mri in the study of the foetus has been the assessment of the normal and pathological anatomy of the central nervous system ( cns ) [ 19 ]  . as our study also shows , mri produces images of high diagnostic value in the study of the brain , particularly with regard to the assessment of the csf spaces and the periventricular cerebral spaces ( with the contribution of t2 - flair sequences ) , anomalies of cerebral myelinization , migration and sulcation . 
in smaller foetuses t2 - weighted sequences better discriminate between grey and white matter , the latter having a higher water content than the post - fetal brain , la placenta sana appare omogeneamente ipointensa nelle sequenze t1 - pesate , ma stasi venosa e o fenomeni trombotici possono portare a foci iperintensi nel suo contesto . negli ultimi anni inoltre sono state introdotte nella pratica quotidiana le sequenze pesate in diffusione ( dwi ) , con tempi di acquisizione inferiori a 20 secondi , che forniscono informazioni sul movimento microscopico delle molecole dacqua , libera e legata , nei tessuti biologici . 
le sequenze in dwi sono state utilizzate inizialmente per lo studio della maturazione cerebrale , ma studi recenti suggeriscono il loro utilizzo per lo studio della maturazione polmonare e renale [ 1518 ]  . 
le immagini pesate in diffusione risentono anche di altri parametri tissutali quali il t2 e la densit protonica cos come della direzionalit dei gradienti applicati . per eliminare leffetto di questi parametri si possono generare delle immagini sintetiche del coefficiente di diffusione apparente , dette mappe di adc , in cui le aree con ridotta mobilit delle molecole dacqua appaiono ipointense . la rm ha dato il suo maggior contributo nella valutazione dellanatomia normale e patologica del sistema nervoso centrale ( snc ) [ 19 ]  . 
come dimostrato anche dalla nostra esperienza la risonanza magnetica fornisce immagini di elevato valore diagnostico per lo studio del distretto encefalico in particolare per quel che riguarda la valutazione degli spazi liquorali e del parenchima cerebrale periventricolare ( con il contributo delle sequenze t2 - flair ) , delle anomalie della mielinizzazione cerebrale , della migrazione e della solcazione . 
nei feti pi piccoli le sequenze t2 pesate permettono una migliore discriminazione tra sostanza grigia e bianca , questultima a maggior contenuto dacqua rispetto allencefalo post - fetale ; mentre nello studio della mielinizzazione le sequenze ge t1 - pesate aggiungono importanti informazioni sulle modificazioni biochimiche che interessano la sostanza bianca quali laumento della quantit di colesterolo e glicolipidi cos come della densit cellulare che producono un segnale iperintenso nelle sequenze t1 [ 20 , 21 ]  . 
il ricorso alle sequenze in diffusione ci ha consentito di valutare la maturazione della sostanza bianca e corticale con maggiore sensibilit e precocit rispetto alle sequenze t1 e t2 pesate : in dwi il cervello fetale caratterizzato da bassa intensit di segnale a livello della sostanza bianca sottocorticale e da una pi alta intensit di segnale allinterno della corteccia e della sostanza grigia profonda [ 22 , 23 ]  . 
anche le anomalie della migrazione neuronale sono ben documentate dalla rm che in grado di correlare gli stadi di maturazione dei solchi e dei giri con let gestazionale [ 24 ]  . nello studio delle emorragie e delle lesioni ipossicoischemiche intracraniche la risonanza magnetica , con lulteriore apporto delle suddette sequenze in diffusione , contribuisce a definire lestensione delle lesioni e le condizioni dei tessuti circostanti nonch lepoca del sanguinamento [ 25 ]  . radiol med ( 2008 ) 113 : 225241 whereas in the study of myelinization t1 - weighted gradientecho sequences add important information regarding biochemical modifications occurring in the white matter , such as increase in the quantity of cholesterol and glycolipids or cellular density , which produce a hyperintense signal in t1weighted sequences [ 20 , 21 ]  . 
the use of dwi sequences has enabled development of the white matter and cerebral cortex to be assessed earlier and with greater sensitivity than with t1and t2 - weighted sequences ; in dwi , the fetal brain is characterised by low signal intensity at the level of the subcortical white matter and by higher signal intensity within the cortex and the deep grey matter [ 22 , 23 ]  . 
anomalies of neuronal migration are also well documented by mri , which is able to correlate the developmental stages of the sulci and the gyrations with gestational age [ 24 ]  . in the study of intracranial haemorrhage and hypoxicischaemic lesions , mri with dwi sequences contribute to defining lesion extension and surrounding tissue conditions , as well as the time of onset of bleeding [ 25 ]  . as reported by a number of studies , obstetric mri not only confirms anomalous conditions , such as ventriculomegaly , but is also able to visualise possible associated anomalies with recognition of the corpus callosum and differentiation between complete and partial ageneses , particularly in sagittal scans [ 26 ]  . in the study of the posterior cranial fossa , the role of mri is fundamental in that , unlike us , it is not impeded by ossification of the skull and is therefore able to visualise the skull base , the pons , the third and fourth ventricles , the tentorium and the foramen magnumri is therefore able to differentiate between dilatation of the cerebellomedullary cistern , dandy - walker variants , arnold - chiari malformation , cerebellar hypoplasia and arachnoid cysts , in the study of which it has contributed to defining their extension and relations with the surrounding structures . 
defects of the neural tube can be studied in detail with mri , which enables differential diagnosis with teratomas , in particular , sacrococcygeal teratomas [ 27 ]  . in our study , most diagnoses of cns anomalies were confirmed at birth or postmortem , with the exception of dilatation of the csf spaces , which was rejected after birth . there is , however , doubt that the mri finding was effectively incorrect , given the frequency with which the finding regresses during gestation . mri has played a fundamental role in the study of the neck , as it is able to distinguish between cystic hygroma and cervical lymphangioma , conditions that are the main causes of airway obstruction at birth . 
mri can also visualise relations between a tumour and the airways as well as the degree of compression and dislocation of the latter . with regard to the fetal lung , our study was in agreement with the literature in showing a relation between signal intensity and organ maturity due to the progressive increase of come riportato da vari autori la rm ostetrica non solo conferma problematiche come la ventricolomegalia , ma permette anche di visualizzare eventuali anomalie associate come il riconoscimento del corpo calloso e leventuale differenziazione tra agenesie complete e parziali , soprattutto nelle scansioni sagittali [ 26 ]  . nello studio della fossa cranica posteriore il ruolo della rm determinante dal momento che a differenza dellecografia non risulta ostacolata dallossificazione della teca cranica permettendo in tal modo di visualizzare il basicranio , il ponte , terzo e quarto ventricolo , il tentorio e il forame magno : in tal modo sono risultate differenziabili la dilatazione della cisterna magna , le varianti di dandy walker , la malformazione di arnold - chiari , lipoplasia cerebellare e le cisti aracnoidee , nello studio delle quali ha contribuito a definirne lestensione e i rapporti con le strutture circostanti . 
i difetti del tubo neurale sono indagati in maniera dettagliata con la risonanza che permette la diagnosi differenziale con i teratomi in particolare sacrococcigei [ 27 ]  . nel nostro studio la maggior parte delle diagnosi di anomalie a carico del snc sono state confermate alla nascita o allesame autoptico , fatta eccezione per la dilatazione degli spazi liquorali confutata dopo la nascita . 
rimane il dubbio se il reperto riscontrato con lesame di risonanza magnetica sia effettivamente errato , data la frequenza con cui questo reperto va incontro a regressione con il progredire della gravidanza . nello studio del collo stato fondamentale il ruolo svolto dalla rm nel distinguere ligroma cistico dal linfangioma cervicale ; entrambe queste condizioni sono le principali cause di ostruzione delle vie aeree alla nascita e la rm consente di mostrare i rapporti tra tumore e vie aeree e il grado di compressione e dislocazione di questultime . per quanto riguarda il polmone fetale nel nostro studio , in accordo con i dati della letteratura , stata osservata una relazione tra intensit di segnale e sviluppo dovuta al progressivo aumento del fluido alveolare ( iperintenso nelle sequenze t2 pesate ) con il progredire della maturazione polmonare . 
in particolare fino alla 24 settimana lintensit di segnale del parenchima polmonare appare ipointensa rispetto al liquor , mentre dopo la 30 settimana il segnale appare isointenso rispetto a questultimo [ 15 ]  . 
al contrario la diminuita intensit di segnale del polmone riscontrata in feti con ritardata maturazione polmonare potrebbe essere collegata ad una riduzione del surfactante alveolare e ci faciliterebbe la diagnosi dellipoplasia polmonare . 
studi recenti pongono laccento sullutilit delle sequenze in diffusione e delle mappe di adc nellindicare il grado di sviluppo polmonare poich permettono di costruire delle tabelle di riferimento oggettive , in base alle quali i valori di adc aumentano con la crescita fetale secondo valori stabiliti [ 16 ]  . lutilizzo delle sequenze in diffusione stato fondamentale in due feti che presentavano luno un ritardo di crescita e 238 radiol med ( 2008 ) 113 : 225241 alveolar fluid ( hyperintense in t2 - weighted sequences ) with lung maturation . 
up until the 24th wg , the signal intensity of pulmonary parenchyma appeared hypointense with respect to csf , whereas after the 30th wg , the signal appeared isointense [ 15 ]  . 
in contrast , reduced signal intensity of the lung encountered in foetuses with growth restriction could be linked to a reduction in alveolar surfactant , a finding that would favour a diagnosis of pulmonary hypoplasia . recent studies highlighted the usefulness of dwi sequences and adc maps in indicating the degree of pulmonary maturity , as they aid in constructing objective reference tables , on the basis of which adc values increase with fetal growth according to established values [ 16 ]  . 
in these cases , the lungs produced a reduced but not very evident signal intensity in t2 - weighted sequences ; the use of adc maps allowed us to compare the values obtained with those reported in the literature and verify the restricted growth with respect to gestational age , thus prompting the gynaecological team to administer corticosteroids . 
in this regard , it is worth noting that one of the false positives was in fact a condition of pulmonary hypoplasia diagnosed with mri , which prompted the aforementioned therapy , such that at birth , the infant presented normal lung development . mri provides important details in the study of the main fetal thoracic masses , such as congenital diaphragmatic hernia , congenital cystic adenomatoid malformation , hydrothorax and bronchopulmonary sequestration [ 28 ]  . 
in our study , we were not only able to visualise congenital diaphragmatic hernia but also identify herniated organs , such as the left hepatic lobe , which appeared hyperintense in t1 - weighted sequences and hypointense in t2 - weighted sequences . 
the compressed pulmonary parenchyma appeared hypointense in the t2 - weighted sequences in a more - or - less marked fashion in relation to the degree of homolateral pulmonary hypoplasia , which the condition caused . recognising congenital cystic adenomatoid malformation was not difficult : in our cases , it presented hyperintense in t2 - weighted sequences and hypointense in flair and t1weighted sequences with respect to the normal parenchyma . with regard to study of the abdomen and pelvis , assessment of all systems was possible ( stomach , liver , urinary system , bladder and bowel loops ) , including the anatomical location of any anomalies and their characterisation . 
mri provided supplementary information to us in the assessment , for example , of omphalocele and gastroschisis , cloacal malformations , enterogenic cysts , fetal ascites , lymphangiomas , hepatic cysts , gastric duplication , intestinal stenosis and possible abdominopelvic masses . 
as stated above , the stomach , the gallbladder and the proximal portion of the small intestine appear hyperintense in t2 - weighted selaltro una condizione di idronefrosi ; in entrambe le condizioni concomitava la presenza di polmoni ipoplasici . 
in questi casi i polmoni presentavano unintensit di segnale ridotta ma non molto evidente nelle sequenze t2 pesate ; il ricorso alla mappa di adc ci ha permesso di confrontare i valori ottenuti con quelli riportati dalla letteratura e verificarne il ritardo di maturazione rispetto allet gestazionale permettendo ai medici ginecologi la precoce somministrazione di corticosteroidi . 
a tal proposito va rilevato che uno dei casi falsi positivi era appunto una condizione di ipoplasia polmonare diagnosticata dalla rm in conseguenza della quale i medici hanno eseguito la terapia , cos che alla nascita il bambino ha presentato una normale maturazione polmonare . la rm fornisce importanti dettagli nello studio delle principali masse toraciche fetali come lernia diaframmatica congenita , la malformazione adenomatosa cistica congenita , lidrotorace e il sequestro bronco - polmonare [ 28 ]  . nella nostra esperienza stato possibile non solo visualizzare lernia diaframmatica congenita ma abbiamo anche individuato gli organi erniati come il lobo sinistro epatico che appare iperintenso nelle sequenze t1 pesate e ipointenso nelle sequenze t2 pesate . 
 non stato difficile riconoscere la malformazione adenomatosa cistica congenita che nei nostri casi si presentava iperintensa in t2 e ipointensa nelle sequenze flair e t1 pesate rispetto al parenchima polmonare normale . riguardo allo studio delladdome e della pelvi stata possibile una valutazione di tutti gli apparati ( stomaco , fegato , sistema urinario , vescica e anse intestinali ) , compresa la localizzazione anatomica delle eventuali anomalie presenti e la loro caratterizzazione . 
la risonanza magnetica fornisce dati aggiuntivi a quelli ecografici nella valutazione , ad esempio , dellonfalocele e della gastroschisi , delle malformazioni cloacali , delle cisti enterogene , dellascite fetale , del linfangioma , delle cisti epatiche , della duplicazione gastrica , delle stenosi intestinali e di possibili masse addomino - pelviche . 
come detto sopra , lo stomaco , la colecisti e la parte prossimale del piccolo intestino appaiono iperintensi nelle sequenze t2 - pesate mentre la porzione distale del piccolo intestino e il colon appaiono iperintensi in t1 . 
nei casi di oligoidramnios comunque il piccolo intestino pu presentare bassa intensit di segnale nelle sequenze t2 e pu essere confuso con una massa [ 12 , 29 ]  . 
 nel nostro studio lunico limite stato rappresentato dalla presenza di calcificazioni intraepatiche che essendo ipointense nelle sequenze t1 - pesate e t2 - pesate non sono state identificate nellambito del parenchima epatico fetale , comunque di piccole dimensioni . i dati forniti dalla rm sono cruciali per lo studio delle radiol med ( 2008 ) 113 : 225241 quences , whereas the distal portion of the small intestine and the colon appear hyperintense in t1 . 
in the case of oligohydramnios , however , the small intestine can present low signal intensity in t2 - weighted sequences and can be confused with a mass [ 12 , 29 ]  . in our study , the only limitation was the presence of intrahepatic calcifications that , being hypointense in both t1and t2 - weighted sequences , were not identified in the fetal hepatic parenchyma ; they were , nonetheless , small . data provided by mri are crucial in the study of malformations of the urinary tract associated with oligohydramnios , conditions that render us study difficult , whereas autosomal recessive polycystic kidney disease , multicystic kidney dysplasia , renal ageneses , pelvicalyceal dilatations and renal masses are well depicted with mri [ 3032 ]  . 
similar to our approach with the lungs , in our study , the use of dwi sequences was fundamental for the differential diagnosis between hydronephrosis and multicystic kidney dysplasia , the latter of which produces loss of signal intensity in dwi and hyperintensity in adc maps . with regard to renal maturation , mri showed that in healthy foetuses , the kidneys increase in size with gestational age , with an intermediate signal in t2 - weighted sequences and the cortex presenting a lower signal than the medulla . 
as in the study of lung maturation , the study of renal maturation also can benefit from dwi sequences and adc maps , the values of which decrease from the 17th to the 28th wg , whereas no change is seen between the 28th and the 38th wg [ 18 , 33 ]  . 
with regard to assessment of fetal growth , mri produced good but not excellent results due to the lack of specific reference tables for mri [ 16 , 32 , 34 ]  . the main limitations to the mri examination are represented by the fetal heart and skeleton . 
with regard to the skeleton , the main impediment concerns the limbs , particularly the small extremities , due to fetal motion artefacts and the impossibility of visualising an entire bone segment in a single image . 
even in this case , echoplanar ( epi ) sequences have proved to be the only ones capable of effectively visualising the fetal skeleton after the 27th wg in that they excellently display bone as hypointense and epiphyseal cartilage as hyperintense [ 35 ]  . 
study of the limbs , particularly in complex malformations , can benefit from the use of t2 - weighted thick - slab sequences , which in less than 1 s generate three - dimension - like images [ 35 ]  . 
with regard to the heart , until now , mri has only been able to identify the margins of the heart and the large vessels and verify malformazioni del tratto urinario associate ad oligoo anidramnios , condizioni queste che rendono tecnicamente difficile lo studio ecografico : reni policistici autosomici recessivi , reni multicistici del bambino , agenesie renali , dilatazioni pelvicaliceali e masse renali sono ben visualizzabili mediante risonanza magnetica [ 3032 ]  . 
nella nostra esperienza , cos come per la valutazione polmonare , stato importante il ricorso alle sequenze di diffusione grazie alla quale stato possibile fare una diagnosi differenziale tra idronefrosi e rene multicistico , rappresentata dalla perdita dellintensit di segnale in dwi e liperintensit nelle mappe di adc in questultima condizione . a proposito della maturazione renale , la rm dimostra che nei feti sani i reni aumentano di dimensione con let gestazionale , mostrando segnale intermedio nelle sequenze t2 - pesate ; in particolare la corteccia presenta un segnale pi basso rispetto alla midollare . 
come per lo studio della maturazione polmonare anche per lo sviluppo renale pu essere utile il ricorso alle sequenze in diffusione ed alle mappe di adc i cui valori diminuiscono tra la 17a e la 28a settimana mentre nessun cambiamento si osserva tra la 28a e la 36a settimana [ 18 , 33 ]  . 
per quanto riguarda lo scheletro , il principale ostacolo riguarda gli arti e soprattutto le piccole estremit per artefatti legati ai movimenti del feto e allimpossibilit di visualizzare un segmento osseo intero in ununica immagine : in rm non quindi possibile la valutazione della biometria scheletrica . 
anche in questo caso le sequenze epi si sono dimostrate le uniche in grado di ben visualizzare lo scheletro fetale dopo la 27a settimana in quanto mostrano in modo eccellente losso come ipointenso e le cartilagini epifisarie iperintense [ 35 ]  . lo studio degli arti soprattutto nelle malformazioni complesse pu avvalersi anche delle sequenze t2 pesate thickslab che generano in meno di un secondo unimmagine simil tridimensionale [ 35 ]  . 
fino ad oggi la risonanza era solamente in grado di individuare i contorni del cuore e dei grossi vasi e di determinare se la posizione cardiaca fosse in asse con la linea mediana , a causa dei numerosi artefatti da movimento legati allelevata frequenza cardiaca fetale ( 140 battiti al minuto ) e a causa delle piccole dimensioni 240 radiol med ( 2008 ) 113 : 225241 whether the position of the heart is in line with the median axis . 
alcuni miglioramenti si sono ottenuti con lutilizzo di sequenze echo - planari ( epi ) che acquisiscono immagini in alcuni millisecondi superando il problema degli artefatti da movimento [ 33 ]  . 
tuttavia , il futuro dellimaging cardiaco la cine - rm esguita mediante acquisizione di sequenze steady - state free precession dinamiche ; queste sequenze permettono inoltre la valutazione dei movimenti intrafetali come le onde peristaltiche e le escursioni diaframmatiche . conclusioni conclusions mri with fast imaging has a crucial role in the recognition of the finest details of normal fetal anatomy . 
the technique , which is still complementary to obstetric us in the characterisation of suspected organ anomalies , contributes to pregnancy management and therapy planning preor postnatally , when required . la rm con fast imaging svolge un ruolo cruciale nel riconoscimento dei dettagli pi fini della normale anatomia del feto . 
this study was performed to clarify the role of perfusion - weighted imaging ( pwi ) at 3 tesla in the characterisation of haemodynamic heterogeneity within gliomas and surrounding tissues and in the differentiation of high - grade from low - grade gliomas . 
pwi was performed by first - pass gadopentetate dimeglumine t2 * - weighted echo - planar images , and cerebral blood volume ( cbv ) maps were computed with a nondiffusible tracer model . 
oedematous - appearing areas were divided in two groups according to signal intensity on t2 - weighted images : tumour with lower ( nearly isointense to grey matter ) and oedema with higher ( scarcely isointense to cerebrospinal fluid ) signal intensity . 
il pwi stato ottenuto mediante immagini eco - planari t2 * - pesate con primo passaggio di gadopentetato di dimeglumina , e le mappe di volume ematico cerebrale ( cbv ) sono state elaborate con il modello del tracciante non diffusibile . 
nei gliomi di alto grado , lrcbv appariva marcatamente incrementato nella massa ( mediasd , 4 , 31 , 2 ) ed ai margini ( 4 , 01 , 1 ) , e ridotto nelle aree necrotiche ( 0 , 30 , 3 )  . 
le regioni apparentemente edematose sono state divise in due gruppi sulla base dellintensit di segnale nelle immagini pesate in t2 : tumore con pi basso segnale ( quasi isointenso alla sostanza grigia ) ed edema con segnale pi elevato ( quasi isointenso al liquido cefalorachidiano )  . 
esso facilita la caratterizzazione in rm dei gliomi cerebrali e fornisce utili informazioni per la pianificazione del trattamento chirurgico e radiante . parole chiave tumori cerebrali risonanza magnetica volume ematico cerebrale imaging pesato in perfusione introduction introduzione gliomas account for approximately 51% of all central nervous system tumours , and their incidence is increasing , especially among the oldest patients [ 1 ]  . 
therapeutic management and prognosis depend on the reliable distinction between high - grade and low - grade gliomas , and a variety of imaging modalities have been proposed for accurate identification of tumour grade [ 2 ]  . 
the combination of t1and t2weighted and contrast - enhanced magnetic resonance ( mr ) imaging is considered the gold standard for diagnosis of cerebral gliomas , but discrepancies between mr imaging findings and pathologic reports have been encountered [ 3 ]  . 
 perfusion - weighted imaging ( pwi ) is a fast and powerful mr technique that is increasingly used in the study of intracranial mass lesions [ 2 , 4 , 5 ]  . 
numerous techniques have been proposed to measure perfusion - related parameters , such as blood volume , transit time , clearance , extraction fraction , blood flow and permeabilitysurface area product , in the brain [ 6 ]  . 
however , dynamic susceptibilityweighted bolus - tracking method , using an exogenous endovascular tracer such as gadopentetate dimeglumine , and cerebral blood volume ( cbv ) , within haemodynamic parameters , have been widely used in clinical settings [ 717 ]  . this pwi method can depict areas of varying haemodynamic activities within tumours and surrounding tissue and can help grade cerebral gliomas [ 717 ]  . 
several studies have demonstrated that the quantitative estimate of cbv reflects tumour microvasculature and angiogenesis [ 79 ]  . the degree of vascularity is directly correlated with malignancy , and the density of microvessels is a prognostic indicator in patients with gliomas [ 18 ]  . 
however , low - grade gliomas , most notably oligodendrogliomas , can present high relative cbv ( rcbv ) foci not reflective of malignancy and may confound the accuracy of rcbv mapping in glial tumour grading [ 19 ]  . i gliomi rappresentano circa il 51% di tutti i tumori del sistema nervoso centrale ( snc ) e la loro incidenza sta aumentando particolarmente fra i pazienti pi anziani [ 1 ]  . limpostazione terapeutica e la prognosi dipendono dalla accurata distinzione tra tumori di alto e di basso grado , e sono state proposte diverse modalit di imaging per permettere laccurata identificazione del grado di malignit [ 2 ]  . 
lutilizzo di immagini rm pesate in t1 , prima e dopo mezzo di contrasto , e in t2 considerato il gold standard per la diagnosi dei tumori cerebrali , ma sono state segnalate alcune discrepanze tra reperti rm e referti anatomo - patologici [ 3 ]  . limaging pesato in perfusione ( pwi ) una tecnica rm veloce ed efficace che viene sempre pi spesso utilizzata nello studio delle neoformazioni cerebrali [ 2 , 4 , 5 ]  . 
numerose sono le tecniche proposte per misurare parametri di perfusione cerebrale quali il volume ematico , il tempo di transito , la clearance , la frazione di estrazione , il flusso ematico e il prodotto permeabilit - area di superfice [ 6 ]  . 
nella pratica clinica , comunque , la metodica che stata pi largamente utilizzata quella dinamica basata sulla suscettibilit magnetica da iniezione in bolo di un mezzo di contrasto endovascolare esogeno , quale il gadopentetato di dimeglumina , ed il parametro emodinamico pi misurato stato il volume ematico cerebrale ( cbv ) [ 717 ]  . 
tale metodica consente di individuare , nel contesto della massa tumorale e dei tessuti circostanti , aree con diverse caratteristiche emodinamiche e pu aiutare nellidentificazione del grado di malignit dei gliomi [ 717 ]  . 
il grado di vascolarizzazione di un tumore correlato direttamente col suo grado di malignit , e la densit dei microvasi tumorali un importante indice prognostico in pazienti con glioma [ 18 ]  . 
tuttavia , i gliomi di basso grado quali gli oligodendrogliomi possono pre136 radiol med ( 2008 ) 113 : 134143 with the integration of 3 - tesla ( 3t ) imagers into clinical practice , there is growing interest in the diagnostic performance of mr imaging techniques at 3t with respect to the established magnetic field strength of 1.5 t [ 2022 ]  . 
mr performed at a higher magnetic field strength has the advantages of higher signal - to - noise ratio ( snr ) and therefore of improved spatial and temporal resolution . 
these gains , however , can be partially lost because of several limitations , such as changes in relaxation times , increase in chemicalshift artefacts and magnetic susceptibility effects and security issues [ 21 , 23 , 24 ]  . 
histopathologic assessment according to the criteria of the revised world health organization ( who ) classification revealed two grade i gangliogliomas , three grade ii astrocytomas , four grade ii oligodendrogliomas , two grade ii oligoastrocytomas , two grade iii oligodendrogliomas , two grade iii anaplastic astrocytomas and 21 grade iv glioblastomas . 
for statistical purposes , grades i and ii gliomas ( 11 patients ) were designed as low grade , and grades iii and iv ( 25 patients ) as high grade . 
the local institutional review board approved the retrospective study . imaging mr examinations were performed using a 3 - t system ( ge medical systems , milwaukee , wi , usa ) with standard quadrature head coil prior to stereotactic biopsy or open surgery . 
tali vantaggi possono essere in parte perduti per effetto di alcune limitazioni , quali le modificazioni dei tempi di rilassamento , laumento degli artefatti da chemical shift e da suscettibilit magnetica e le problematiche inerenti la sicurezza [ 21 , 23 , 24 ]  . lo scopo di questo studio stato quello di caratterizzare leterogeneit spaziale dellemodinamica nei gliomi e nei tessuti peritumorali mediante pwi a 3t , e di valutare il ruolo di questo approccio nella differenziazione dei glomi di alto grado da quelli di basso grado . materiali e metodi pazienti sono stati studiati retrospettivamente 36 pazienti con glioma non trattato ( 22 uomini e 14 donne ; et mediasd , 56 anni12 ; range di et , 2976 anni )  . 
le diagnosi istopatologiche , effettuate secondo la classificazione proposta dallorganizzazione mondiale della sanit ( who ) , includevano : 2 gangliogliomi di i grado , 3 astrocitomi di ii grado , 4 oligodendrogliomi di ii grado , 2 oligoastrocitomi di ii grado , 2 oligodendrogliomi di iii grado , 2 astrocitomi anaplastici di iii grado e 21 glioblastomi di iv grado . 
per lanalisi statistica , i gliomi di grado i e ii ( 11 pazienti ) sono stati considerati tumori di basso grado e i gliomi di grado iii e iv ( 25 pazienti ) tumori di alto grado . 
lo studio retrospettivo stato approvato dalla commissione etica locale . imaging gli esami rm sono stati effettuati con unapparecchiatura a 3 tesla ( ge medical systems , milwaukee , wi ) con bobine in quadratura standard per encefalo , prima della biopsia stereotassica o dellintervento chirurgico . 
after the first ten acquisitions , a bolus of gadopentetate dimeglumine ( 0.07 mmol / kg ) was injected with a mechanical injection pump ( 3 ml / s ) through an 18or 20 - gauge intravenous catheter , followed by a 20 - ml saline flush . 
images were inspected for overall image quality and motion artefacts and transferred to a workstation for postprocessing with a dedicated software package ( functool performance , ge medical systems )  . 
the software calculated , on a voxel - by - voxel basis , curves of signal intensity changes over time , t2 * relaxation rate ( r2 * ) , the baseline to be subtracted to the r2 * curve , and area under the fitted r2 * curve . 
the r2 * was calculated by the equation r2 * = ln ( st / s0 ) / te , where st is the signal intensity at time t , s0 is the precontrast signal intensity ( excluding the first one to two images acquired while reaching of the steady - state mr signal ) and te is the echo time . baseline was estimated by calculating the average background intensity prior to onset and after completion of the transient signal intensity change . 
cbv maps were generated by the numerical integration of r2 * for the first - pass bolus through each pixel on the basis of kinetic principles for nondiffusible tracers [ 6 ] , and the relative cbv ( rcbv ) was calculated by rcbv = cbv [ tumour ] / cbv [ contralateral normal white matter ]  . 
 regions of interest ( rois ) were selectively drawn in the necrotic or cystic regions of the tumour , the apparently nonnecrotic mass , the margins , the oedematous - appearing areas and the surrounding normal - appearing tissue . 
areas of altered signal outside the enhanced margins were taken as apparently oedematous , and areas surrounding the tumours without enhancement or signal alteration in all sequences were considered as apparently normal . 
 il pwi stato ottenuto con sequenze echo - planari ad impulso singolo di tipo gradient - echo ( spessore 5 mm , gap 1 mm , tr 1700 ms , te 48 ms , fa 90 , fov 22 , matrice 164164 , nex 1 , n di fette 12 , tempo di acquisizione 1 min )  . 
dopo le prime 10 acquisizioni , stato somministrato un bolo di gadopentetato di dimeglumina ( 0 , 07 mmol / kg ) con un iniettore automatico ( 3 ml / s ) attraverso un catetere endovenoso di 1820 gauge , seguito immediatamente dalla somministrazione di 20 ml di soluzione fisiologica . 
le immagini ottenute sono state prima visionate per valutare la loro qualit e la eventuale presenza di artefatti da movimento , e poi sono state trasferite su una workstation per lelaborazione mediante un software dedicato ( functool systems , performance , general electric medical milwaukee , wi )  . 
il software calcolava , per ogni voxel : le curve di variazione nel tempo dellintensit di segnale , il tasso di rilassamento t2 * ( r2 * ) , la linea di base da sottrarre alla curva di r2 * , e infine larea sottesa alla curva r2 *  . 
il valore di r2 * stato calcolato con la seguente equazione : r2 * = ln ( st / s0 ) / te , dove st lintensit di segnale al tempo t , s0 lintensit di segnale prima del contrasto ( escludendo le prime 12 immagini acquisite durante il raggiungimento dello stato stazionario del segnale rm ) e te il tempo di eco . 
le mappe di cbv sono state generate attraverso lintegrale numerico del r2 * al primo passaggio del bolo , in ogni pixel , sulla base dei principi cinetici dei traccianti non diffusibili [ 6 ] , e il valore di rcbv stato calcolato con la formula : rcbv = cbv [ tumore ] / cbv [ sostanza bianca normale controlaterale ]  . 
 le roi sono state tracciate nelle regioni tumorali necrotiche o cistiche , nella massa tumorale apparentemente non necrotica , nei margini tumorali , nelle regioni apparentemente edematose e in quelle apparentemente sane . 
le aree di alterato segnale che circondavano i margini neoplastici impregnati sono state considerate come apparentemente edematose , mentre quelle che non presentavano alterazioni di segnale o impregnazioni patologiche sono state considerate come apparentemente normali . 
1a - c conventional t1 - weighted contrast - enhanced ( a ) and t2 - weighted ( b ) images and cerebral blood volume ( cbv ) map ( c ) in a patient with a temporal glioblastoma . 
margins ( d ) : area nearly isointense to grey matter ( tumour ) ( e ) and area scarcely isointense to cerebrospinal fluid ( oedema ) ( f ) surrounding the tumour , and contralateral normal white matter ( g )  . 
1a - c immagini rm pesate in t1 dopo mezzo di contrasto ( a ) e in t2 ( b ) , e mappa di volume ematico cerebrale ( cbv ) ( c ) in un paziente con glioblastoma temporale . 
margini ( d ) ; area quasi isointensa alla sostanza grigia ( tumore ) ( e ) e area quasi isointensa al liquor ( edema ) ( f ) circostanti il tumore , e sostanza bianca normale controlaterale ( g )  . 
le differenze tra i gruppi sono state valutate utilizzando lanalisi della varianza e il test t di student post hoc a due code con un livello di significativit di p < 0 , 05 , dopo correzione secondo bonferroni . 
le valutazioni statistiche di massa e margini tumorali sono state effettuate separatamente perch in 8 casi il glioma era ridotto a un sottile anello di impregnazione intorno ad unarea centrale necrotica . two - tailed students t test with a bonferroni corrected significance level of p < 0.05. 
oedematous - appearing rois were divided in two groups according to signal intensity on t2weighted images : tumour , with relatively lower signal intensity ( nearly isointense to grey matter ) ; and oedema , with relatively higher signal intensity ( scarcely isointense to cerebrospinal fluid )  . 
 discussion in this study , pwi performed at 3 t provided results similar to those previously reported at 1.5 t , as it allows differentiation of high - grade from low - grade gliomas and the distinction of different tumour structures . 
2a - c conventional t1 - weighted contrast - enhanced ( a ) and fluid - attenuated inversion recovery ( b ) images , and cerebral blood volume ( cbv ) map ( c ) in a patient with a grade ii temporoparietooccipital oligoastrocytoma . 
2a - c immagini rm pesate in t1 dopo mezzo di contrasto ( a ) e flair ( b ) , e mappa di volume ematico cerebrale ( cbv ) ( c ) in un paziente con oligoastrocitoma temporo - parieto - occipitale di ii grado . 
tale reperto pu essere spiegato dallosservazione che 140 radiol med ( 2008 ) 113 : 134143 table 1 rcbv [ meanstandard deviation ( sd ) ] in the selected regions of interest ( rois ) of high - grade and low - grade gliomas rcbv , relative cerebral blood volume ; rois , regions of interest . 
observations that the average vessel size of a tumour is greater than that of capillaries and that the ge - epi technique is highly sensitive to those larger vessels in contrast to se - epi that have higher sensitivity to capillaries may explain this finding [ 8 ]  . 
consequently , temporal changes of signal amplitude during the first passage of the contrast bolus are dominated by t2 * effects , and difference in t1 - weighting due to variations in tr can be neglected . 
in contrast , glioblastomas typically demonstrate a breakdown of the il calibro medio dei vasi tumorali maggiore di quello dei capillari e che le sequenze ge - epi sono pi sensibili ai vasi di calibro maggiore , al contrario delle sequenze se - epi pi sensibili ai capillari [ 8 ]  . 
di conseguenza , le variazioni temporali dellintensit di segnale al primo passaggio del bolo di contrasto sono determinate principalmente dagli effetti t2 * ed eventuali differenze di pesatura in t1 , legate ai diversi tr , possono essere trascurate . 
di conseguenza , il decremento del segnale t2 * pu essere parzialmente compensato da un aumento del segnale t1 e ci pu condurre ad una sottostima dell rcbv [ 4 , 11 ]  . 
altri autori hanno usato tr lunghi e / o flip angle ridotti per diminuire la pesatura in t1 [ 4 , 9 , 13 ] , o la tecnica del double - echo [ 25 ]  . 
therefore , the t2 * - related signal decrease can be partly compensated for by a t1 - related signal increase , which may lead to an underestimation of rcbv [ 11 , 4 ]  . 
others used long tr and / or a small flip angle to reduce t1 weighting [ 4 , 9 , 13 ] , and others used the doubleecho technique [ 25 ]  . 
correction of rcbv maps for contrast - agent extravasation by means of a linearfitting algorithm is a new , promising method that allows rcbv values significantly correlated with glioma tumour grade [ 16 ]  . the different doses and infusion rates of contrast agent , which were used by the different authors , can also explain the discrepancies . 
in any case , high - grade gliomas present a marked heterogeneity of histologic composition , including varying degrees of vascularity and frequent areas of necrosis , which can account for the large range of rcbv values [ 4 ]  . in this study performed at a higher magnetic field , we used ge - epi with a relatively long te , lower contrast dose and infusion rate and did not research maximum rcbv values . 
the lower contrast agent dose and infusion rate and the lack of predose injection are the more likely explanations for the lower rcbv values we found in high - grade gliomas . pwi takes advantage of increased susceptibility effect at 3 t , resulting in higher sensitivity to transitory t2 * changes due to the bolus of contrast medium [ 23 ]  . 
in our study , in fact , no patient complained of unpleasant feelings of warmth and / or nausea , symptoms often reported by patients when we previously tried to use higher infusion rates . 
however , increased susceptibility effect also has some disadvantages , such as t2 * shortening and stronger distortion artefacts , particularly close to bone and air spaces at the skull base [ 23 ]  . 
geepi , in particular , can potentially show increased ghosting and shearing effects , which may compromise image quality presenta specifici vantaggi e svantaggi [ 2 , 26 ]  . 
la correzione delle mappe di rcbv per lo stravaso di mezzo di contrasto con lutilizzo di un algoritmo di fitting lineare rappresenta un nuovo promettente metodo che permette di avere rcbv che correlano significativamente con il grado di malignit del glioma [ 16 ]  . 
inoltre , in molti studi le roi sono state posizionate nel contesto delle aree tumorali con pi alti valori di rcbv , misurandone in tal modo soltanto i valori massimi [ 4 , 8 , 9 , 11 , 14 , 15 ]  . 
in ogni modo , i gliomi di alto grado presentano una notevole eterogeneit istopatologica , con differenti gradi di vascolarizzazione e frequenti aree di necrosi , caratteristiche che possono in parte spiegare la vasta gamma di valori di rcbv riportati [ 4 ]  . in questo studio realizzato a pi alto campo magnetico , abbiamo utilizzato sequenze ge - epi con un te relativamente lungo , dosi di contrasto e velocit di infusione pi basse e non abbiamo ricercato valori massimi di rcbv . luso di basse dosi di contrasto e di ridotte velocit di infusione e la mancanza di uniniezione pre - dose di contrasto rappresentano la spiegazione pi probabile per i bassi valori di rcbv che abbiamo rilevato nei gliomi di alto grado . 
il pwi trae vantaggio dallaumento della suscettibilit magnetica a 3t , risultando in una pi alta sensibilit alle variazioni transitorie di t2 * legate allarrivo del bolo di contrasto [ 23 ]  . 
 [ 28 ] hanno dimostrato che il pwi a 3t pu essere praticabile anche a basse dosi di contrasto come 0 , 05 mmol / kg . un altro vantaggio , derivante dallutilizzo di dosi e velocit di infusione pi basse , il miglior comfort dei pazienti . 
nel presente studio , infatti , nessun paziente ha lamentato sgradevole sensazione di calore e / o nausea , sintomi spesso manifestati quando precedentemente avevamo utilizzato pi alte velocit di infusione . 
tuttavia , laumentata suscettibilit magnetica presenta anche alcuni svantaggi , quali la riduzione del t2 * e i pi evidenti artefatti da distorsione , specialmente in vicinanza delle strutture ossee ed degli spazi aerei della base del cranio [ 23 ]  . 
lutilizzo delle sequenze ge - epi , in particolare , pu potenzialmente causare un aumento degli effetti di shearing e ghosting , che possono compromettere la qualit delle immagini e linterpretazione diagnostica [ 23 ]  . 
from the histopathological point of view , regions of altered signal outside the enhancing margins of high - grade gliomas represent a variable combination of vasogenic oedema and infiltrating tumour cells [ 29 ]  . 
in our study , areas nearly isointense to grey matter ( tumour ) on t2 - weighted images showed high rcbv , suggesting incremented size and / or number of vessels and hence tumour angiogenesis . 
on the contrary , areas scarcely isointense to cerebrospinal fluid ( oedema ) presented low rcbv , suggesting a reduction of microvessel density due to the increase of interstitial water . the finding that perienhancing regions of metastasis , containing pure vasogenic oedema , showed rcbv lower than those of high - grade gliomas , containing infiltrating tumour cells , supports our hypothesis [ 30 , 31 ]  . 
a larger study population including a balanced number of patients with different who grades and a trial to correlate mr and histopathological findings will be useful to further support the results of this study . istopatologico , le regioni di alterato segnale esterne ai margini impregnati dei gliomi di alto grado rappresentano una combinazione variabile di edema vasogenico e di cellule tumorali infiltranti [ 29 ]  . 
in tale studio le aree approssimativamente isointense alla sostanza grigia nelle immagini t2 - pesate ( tumore ) mostrano alti valori di rcbv , suggerendo un incremento del calibro e / o del numero dei vasi e , quindi , una angiogenesi tumorale . 
al contrario , le aree quasi isointense al liquido cerebrospinale ( edema ) presentano bassi valori di rcbv , suggerendo una riduzione di densit microvascolare legata allaumento di acqua interstiziale . 
il rilievo che le aree circostanti le aree di impregnazione delle metastasi , contenenti edema vasogenico puro , presentano valori di rcbv pi bassi di quelli delle aree peritumorali dei gliomi di alto grado , caratterizzate oltre che da edema anche da cellule tumorali infiltranti , di supporto alla nostra ipotesi [ 30 , 31 ]  . 
 il presente studio ha due rimarchevoli limiti : il ristretto numero di pazienti con astrocitoma anaplastico , che pu aver influenzato i risultati statistici , e la mancanza di conferme istopatologiche . 
uno studio su una popolazione pi ampia di pazienti , con una distribuzione pi bilanciata di gliomi con diverso grado who , e un trial per correlare i reperti rm con quelli istopatologici potrebbero essere utili per supportare ulteriormente i risultati di questo studio . conclusioni conclusions pwi at 3 t helps distinguish necrosis from tumour mass , infiltrating tumour from oedema and high - grade from lowgrade gliomas . 
riconoscendo i suoi vantaggi ed i potenziali svantaggi e adattando le procedure di imaging alle modificazioni indotte dallalto campo , il pwi a 3t pu essere utilizzato come parte integrante dellesame rm di routine delle lesioni espansive intracraniche per migliorare laccuratezza diagnostica , la valutazione pre - trattamento ed il follow - up dei pazienti con glioma cerebrale . acknowledgement the authors are grateful to piero ghedin and fred frigo ( ge healthcare ) for expert technical assistance . 
in 4 / 20 patients , all with wegeners granulomatosis , cxr was negative or demonstrated only nodular opacities ; in two of these cases , ct revealed ground - glass opacities . 
a complete follow - up was available for ten patients : initially , they showed consolidation opacities in 36 / 60 zones , which persisted in 16 / 60 after 7 days and in 11 / 60 after 15 days . 
studio retrospettivo di 23 episodi di ead in 20 pazienti , 17 con eziologia identificata , 3 senza causa specifica , studiati tutti con rx torace e 15 con tc . 
la tc , pi sensibile dellrx nel riconoscere opacit ground - glass , indispensabile in pazienti con possibile ead e quadro rx negativo . parole chiave polmone , emorragia radiografia , toracica polmone , tc radiol med ( 2008 ) 113 : 1628 introduction diffuse alveolar haemorrhage ( dah ) is a rare clinicopathological syndrome characterised by diffuse intra - alveolar bleeding , which may have an insidious chronic course or may present as an acute event in subjects of any age , including children [ 1 , 2 ]  . 
the fundamental pathogenetic mechanisms are deposition of immune complexes formed in the bloodstream or in situ on the vessel endothelium or walls , production of antineutrophil cytoplasmic antibodies ( anca ) and production of antiglomerular basement membrane ( anti - gbm ) antibodies [ 5 ]  . the most frequent histopathological finding ( an almost constant finding in systemic vasculitis ) is pulmonary capillaritis characterised by fibrin thrombi in the interalveolar capillaries and septa , fibrinoid necrosis of capillaries , granulocyte infiltrates , erythrocytes and haemosiderin in the interstitiuin the absence of damage to the alveolar interstitium , there may be mild alveolar haemorrhage ; in the case of recurring haemorrhage , interstitial fibrosis and tissue haemosiderosis may develop [ 6 ]  . 
a less frequent histological pattern is diffuse alveolar damage ( dad ) characterised by interstitial and alveolar oedema , capillary congestion with microthrombi and , above all , intra - alveolar hyaline membranes [ 6 ]  . dah may develop in a number of systemic diseases , as a result of coagulation disorders , inhaled toxins or infections ( table 1 ) , but it may even have no specific cause [ 5 , 6 ]  . 
in the acute phases , it is characterised by the presence of dyspnoea with hypoxaemia , haemoptysis ( in 70% of cases ) and sideropenic anaemia [ 1 ]  . 
anaemia is the most constant finding in patients with pulmonary haemorrhage and is present in virtually all patients with goodpastures syndrome [ 1 ]  . haemoptysis is the most striking symptom and may be present intermittently for weeks before the acute event or , more commonly , it may manifest or worsen dramatically and suddenly over a few days or even hours . 
other symptoms include cough , fever and chest pain . the radiographic pattern of dah is characterised by consolidation or ground - glass alveolar - filling opacities of extremely varying size that are usually bilateral and prevalently distributed in parahilar regions . 
in chronic or recurrent dah , persistent fibrotic interstitial involvement may develop in the later phases [ 4 ]  . introduzione lemorragia alveolare diffusa ( ead ) una rara sindrome clinico - patologica caratterizzata da sanguinamento intraalveolare diffuso , che pu avere un decorso insidioso e cronico o presentarsi come un evento acuto in soggetti di qualsiasi et , compresi pazienti in et pediatrica [ 1 , 2 ]  . 
lead deve essere distinta dallaspirazione alveolare diffusa di sangue proveniente da lesioni focali del polmone ( es . : bronchiettasie , tumori , infezioni ) , che sono di solito radiograficamente individuabili [ 3 , 4 ]  . 
i meccanismi patogenetici fondamentali sono : la precipitazione di immunocomplessi , formati o in circolo o in situ , a livello dellendotelio o delle pareti vasali ; la produzione di anticorpi diretti contro componenti citoplasmatici dei neutrofili ( anca ) ; la produzione di anticorpi anti - membrana basale ( ambg ) [ 5 ]  . 
 il quadro istopatologico pi comune ( pressoch costante in corso di vasculite sistemica ) la capillarite polmonare , caratterizzata da trombi di fibrina nei capillari e nei setti interalveolari , necrosi fibrinoide dei capillari , infiltrati granulocitari , eritrociti ed emosiderina nellinterstizio . 
pi raro il riscontro del pattern istologico del danno alveolare diffuso ( dad ) , caratterizzato da edema interstiziale ed alveolare , congestione capillare con microtrombi e , soprattutto , presenza di membrane ialine intra - alveolari [ 6 ]  . lead pu comparire nel corso di numerose malattie sistemiche , in seguito a disordini coagulativi o inalazione di tossine o infezioni ( tabella 1 ) , ma pu anche rimanere senza una causa specifica [ 5 , 6 ]  . 
lemottisi il sintomo pi eclatante , e pu presentarsi in modo intermittente per settimane prima della presentazione dellevento acuto o , pi spesso , manifestarsi o aggravarsi in maniera drammatica e improvvisa nel corso di pochi giorni o addirittura di alcune ore . 
altri sintomi sono la tosse , la febbre e il dolore toracico . il quadro radiografico tradizionale dellemorragia alveolare diffusa caratterizzato da opacit da occupazione alveolare , abitualmente bilaterali , di tipo consolidativo o ground glass , di estensione assai variabile ; spesso la distribuzione predominante in sede parailare . 
nelle forme croniche , o recidivanti di emorragia table 1 main causes of diffuse alveolar haemorrhage vasculitis connectivitis drugs other vasculiti connettiviti farmaci varie tabella 1 principali cause di ead wegeners disease micropolyangiitis churg strauss syndrome idiopathic pulmonaryrenal syndromes systemic lupus erythematosus rheumatoid arthritis polydermatomyositis scleroderma penicillamine cytarabine bleomycin goodpastures syndrome idiopathic haemosiderosis antiphospholipid antibody syndrome coagulation disorders bone marrow transplantation morbo di wegener micropoliangioite sindrome di churg strauss sindromi nefro - polmonari idiopatiche lupus eritematoso sistemico artrite reumatoide polidermatomiosite sclerodermia penicillina citarabina bleomicina sindrome di goodpasture emosiderosi idiopatica sindrome da anticorpi antifosfolipidi coagulopatie trapianto di midollo radiol med ( 2008 ) 113 : 1628 alveolare diffusa , pu comparire tardivamente un quadro di persistente impegno interstiziale di natura fibrotica [ 4 ]  . in tc , lead in fase acuta si presenta con opacit ground glass o consolidative che spesso risparmiano il mantello polmonare e gli apici [ 9 ]  . 
nelle forme pi blande o in fase subacuta possono associarsi ai quadri di ground glass tenui opacit pseudo - nodulari , senza distribuzione preferenziale [ 10 ] ; infine pu essere osservato il pattern del crazy paving caratterizzato da opacit ground glass sovrapposte a una fine trama reticolare . 
le opacit lineari che producono il pattern reticolare non sono dovute a inspessimento dei setti lobulari secondari , ma a deposito di materiale emorragico in alveoli alla periferia del lobulo [ 9 ]  . 
la tc , soprattutto se eseguita con tecnica ad alta risoluzione , ritenuta pi sensibile dellrx standard per individuare focolai circoscritti di ead , specie con pattern ground glass , ma non risulta comunque pi specifica . il sospetto clinico - radiografico di ead impone lesecuzione di una broncoscopia con bal , con evidenza della presenza nelle vie aeree di sangue rosso vivo o a lavatura di carne proveniente da sedi multiple , e riscontro microscopico di macrofagi alveolari che contengono emosiderina ( siderofagi ) in quantit crescente in relazione alla cronicit della patologia [ 2 , 11 ] ; in alcuni casi pu per essere indispensabile il ricorso alla biopsia . 
 scopo del lavoro descrivere i reperti della ead in unampia casistica di pazienti sottoposti a esami rx e tc . quando disponibili sono state valutate anche le indagini eseguite nel follow - up ravvicinato , per meglio caratterizzare il decorso radiologico della malattia . 
si sono poi confrontate la sensibilit e la specificit dei radiogrammi standard del torace e della tc convenzionale o a alta risoluzione per meglio definirne il rispettivo ruolo nella diagnosi della malattia . on computed tomography ( ct ) , dah presents with ground - glass or consolidation opacities in the acute phases , often with sparing of the subpleura and apices [ 9 ]  . 
in milder forms or in the subacute phase , slight pseudonodular opacities without preferential distribution [ 10 ] may be associated with ground - glass findings ; finally , a crazy - paving pattern characterised by ground - glass opacities over a thin reticular pattern may be observed . 
the linear opacities producing the reticular pattern are not related to thickened secondary lobular septa but to the deposition of haemorrhagic material inside the alveoli at the lobule periphery [ 9 ]  . 
ct , in particular high - resolution ct ( hrct ) , is considered more sensitive than standard x - ray in identifying limited foci of dah , especially with ground - glass patterns , but it is no more specific . clinical and radiographic suspicion of dah requires confirmation by bronchoscopy with bronchoalveolar lavage ( bal ) , with demonstration of bright red blood from multimateriali e metodi stato eseguito uno studio retrospettivo multicentrico , reclutando un totale di 20 pazienti affetti da emorragia alveolare diffusa , giunti allosservazione tra il 1991 e il 2004 . 
una diagnosi eziologica precisa stata ottenuta in 17 / 20 integrando i dati clinico - anamnestici , bioptici e laboratoristici specifici ( canca , panca , ambg , sierologia per il lupus eritematoso sistemico , anticorpi antifosfolipidi ) : 8 pazienti risultavano affetti da granulomatosi di wegener ( gw ) , 3 da micropoliangioite ( mpa ) , 2 da sindrome di goodpasture ( gp ) , 3 da emosiderosi polmonare idiopatica ( eip ) , 1 da sindrome da anticorpi antifosfolipidi ( aps )  . 
b quasi completa risoluzione delle lesioni a un mese di distanza con persistenza di pattern reticolo - nodulare medio - basale . ple sites in the airways and microscopic evidence of alveolar haemosiderin - containing macrophages ( siderophages ) whose number increases in proportion to the chronicity of the disease [ 2 , 11 ]  . 
in a few cases , the use of biopsy may be indispensable . the purpose of this paper is to describe dah findings in a large series of patients studied by cxr and ct . 
sensitivity and specificity of standard cxr and conventional or high - resolution ct were then compared to establish the respective roles of the two modalities in the diagnosis of the disease . materials and methods a retrospective multicentric study was conducted on 20 patients with dah who presented between 1991 and 2004 . the diagnosis of dah was established on the basis of clinical findings of anaemia ( haemoglobin less than 10 mg / dl ) in 20 / 20 patients , dyspnoea ( 20 / 20 ) , haemoptysis ( 13 / 20 ) and the results of bronchoscopy ( 20 / 20 ) , bal ( 20 / 20 ) and biopsy ( 12 / 20 )  . 
an accurate aetiological diagnosis was achieved in 17 / 20 cases after integrating specific clinical , biopsy and laboratory data [ cytoplasmic - staining antineutrophil cytoplasmic antibodies ( c - anca ) , perinuclearstaining anca ( p - anca ) , antiglomerular basement membrane ( anti - gbm ) antibodies , serology for systemic lupus erythematosus , antiphospholipid antibodies ]  . 
 erano disponibili controlli radiografici in tutti i 20 pazienti , ed esami tc in 15 / 20 , di cui 14 in fase acuta ed uno in corso di follow - up ; gli esami tc sono stati eseguiti con tecniche ed apparecchiature diverse . 
per la valutazione degli esami rx e tc ognuno dei due polmoni stato diviso in tre regioni : una zona superiore , compresa fra gli apici e la carena , una zona intermedia , fra la carena e le vene polmonari , e una regione inferiore , dalle vene polmonari ai diaframmi , per un totale di sei zone . 
in ciascun settore dei due polmoni si ricercata la presenza di consolidamenti o di opacit ground glass ( a vetro smerigliato ) , registrando quale regione fosse pi interessata e se venissero risparmiati gli apici e le regioni mantellari . 
veniva inoltre registrata la presenza di reperti patologici non strettamente correlati alla ead : opacit nodulari , pattern interstiziali reticolonodulari , strie fibrotiche o segni di honeycomb , versamento pleurico . 
episodi ripetuti di ead in un singolo paziente sono stati considerati separatamente e sono stati quindi valutatati complessivamente 23 episodi . risultati la distribuzione delle opacit dimostrate radiograficamente nei 23 episodi di ead riassunta nella tabella 3 . radiol med ( 2008 ) 113 : 1628 were affected by wegeners granulomatosis , three by micropolyangiitis , two by goodpastures syndrome , three by idiopathic pulmonary haemosiderosis and one by antiphospholipid antibody syndrome . 
patient demographic data are shown in table 2 . cxr studies were available for all 20 patients and ct scans for 15 / 20 , 14 of which were in the acute phase and one from the follow - up . 
to evaluate the cxr and ct studies , each lung was divided into three regions upper zone , from the apices to the carina ; middle zone , between the carina and the pulmonary veins ; and lower zone , from the pulmonary veins to the diaphragm for a total of six zones ( three on each side )  . 
repeated dah episodes in a single patient were considered separately , resulting in a total of 23 episodes . results the distribution of opacities shown radiographically in the 23 dah episodes is summarised in table 3 . dah in wegeners granulomatosis eight patients presented with one dah episode each , at the onset of wegeners granulomatosis . 
un esame tc era disponibile in 7 / 8 pazienti , di cui 6 / 8 al momento dellepisodio di ead e 1 / 8 eseguito in follow - up . valutazione rx quattro / 8 presentavano allesordio un quadro rx compatibile con ead , caratterizzato da opacit ground glass o consolidative , con un numero medio di zone coinvolte di 4 , 6 / 6 . in 2 pazienti si apprezzavano esclusivamente opacit di tipo consolidativo diffuse a tutte e sei le zone polmonari , negli altri 2 , meno gravi , erano presenti entrambe le lesioni . 
in 3 casi stato possibile valutare levoluzione radiografica in follow - up : in 2 / 3 si assisteva ad una rapida regressione delle lesioni sin dai primi controlli successivi , con scomparsa delle opacit consolidative ( eventualmente dopo una modificazione in pattern ground glass ) entro 15 giorni . 
in 1 / 3 si osservava inizialmente un aggravamento del quadro con sostituzione delle opacit ground glass con opacit consolidative , e a partire dallottava giornata miglioramento con risoluzione a radiol med ( 2008 ) 113 : 1628 table 3 results diagnosis wegeners granulomatosis micropolyangiitis goodpastures syndrome idiopathic haemosiderosis antiphospholipid syndrome other total tabella 3 risultati diagnosi granulomatosi di wegener micropoliangioite sindrome di goodpasture emosiderosi polidiopatica s . 
one of the eight patients had completely negative cxr . ct evaluation three of four patients with cxr findings typical of dah also underwent ct , which proved to be more accurate in defining the zones involved and the extent of the groundglass pattern , although it provided no significant additional elements . 
in 2 / 3 patients with cxr evidence of nodular lesions but no consolidation or ground - glass opacities , ct documented the presence of ground - glass opacity in one zone in one case but failed to reveal typical findings of dah in the other and only confirmed the existence of nodular lesions . 
tre / 8 dimostravano esclusivamente lesioni nodulari a volte cavitate , caratteristiche della granulomatosi di wegener , senza opacit consolidative o ground glass . uno / 8 presentava un reperto rx totalmente negativo . valutazione tc in 3 / 4 pazienti con reperti radiografici caratteristici di ead veniva eseguita anche la tc , che risultava pi accurata nel definire le zone interessate e lestensione del pattern ground glass , ma nel complesso non forniva elementi aggiuntivi significativi . 
in 2 / 3 pazienti con rx positivo per lesioni nodulari , ma negativo per opacit consolidative o ground glass la tc documentava in un caso la presenza di ground glass in ununica zona , mentre nellaltro non permetteva di evidenziare gli aspetti tipici delle ead , confermando la presenza di lesioni nodulari . 
nel caso con quadro rx completamente negativo la tc documentava un pattern di tipo ground glass nelle 2 zone intermedie ( parailari )  . ead in corso di micropoliangioite di tutti e 3 i pazienti erano disponibili controlli rx e tc . 
un paziente presentava un unico episodio di ead con opacit consolidative inizialmente monolaterali ( 2 / 6 ) , che si erano radiol med ( 2008 ) 113 : 1628 poi diffuse a 6 / 6 dopo tre giorni . 
i restanti pazienti hanno presentato rispettivamente due e tre successivi episodi di ead , prima che fosse possibile stabilire la diagnosi corretta e impostare una terapia adeguata . il primo paziente esordiva con un reperto rx di opacit di tipo consolidativo in 5 / 6 zone e , dopo un netto miglioramento senza reliquati , presentava dopo un anno un ulteriore episodio di ead con opacit consolidative in 5 / 6 zone . la completa normalizzazione si aveva dopo appena una settimana . 
nel secondo paziente il radiogramma mostrava un addensamento consolidativo nella zona inferiore di destra , mentre allindagine tc si osservava un quadro di opacit prevalentemente ground glass in 4 / 6 zone . 
nel terzo si apprezzava un impegno tipo ground glass in tutte le zone con risparmio mantellare e dellapice sinistro . ead in corso di sindrome da anticorpi antifosfolipidi lunico paziente della nostra casistica mostrava al radiogramma del torace delle opacit consolidative perilari e medio - basali ( 4 / 6 zone ) , con estensione a 6 / 6 dopo solo poche ore . 
lhrct documenta opacit prevalentemente di tipo ground glass ( freccia ) , con zone di pattern crazy paving ( frecce doppie )  . dah in micropolyangiitis cxr and ct studies were available for all three patients . one patient presented with a single episode of dah with initially unilateral consolidation opacities ( 2 / 6 ) , which had spread to 6 / 6 zones 3 days later . 
ct performed after the first episode confirmed the ground - glass pattern in 6 / 6 zones , with additional areas of crazy - paving patterns . dah in idiopathic pulmonary haemosiderosis in one patient , a ground - glass pattern was observed in 2 / 6 zones in the middle field on both sides . 
in the second patient , cxr showed a dense consolidation in the lower right zone , entrambi i pazienti presentavano opacit diffuse a 6 / 6 zone , con aspetto prevalentemente ground glass in un paziente e consolidative nel secondo . 
in the third patient , a ground - glass pattern was observed in all zones , with sparing of the subpleura and left apex . dah in antiphospholipid antibody syndrome the only patient with this syndrome showed perihilar and middle - basal consolidation opacities on cxr ( 4 / 6 zones ) , which extended to 6 / 6 zones after only a few hours . 
solo di questo paziente stata valutato un esame tc , che presentava anchesso un pattern di tipo ground glass in 4 / 6 zone , ma in sedi diverse rispetto al reperto dellrx standard . risultati complessivi complessivamente opacit consolidative o ground glass caratteristiche di ead erano dimostrate allrx standard in 16 / 20 pazienti . 
 nei 23 episodi di ead risultavano interessate allesordio 84 / 138 zone ( 60 , 8% ) , con opacit consolidative in 53 / 138 ( 38% ) , e ground glass in 31 / 138 ( 22% )  . 
le zone superiori erano interessate nel 43% , le zone intermedie nel 73% e le zone inferiori nel 65% . in 10 pazienti stato valutato il follow - up rx ( tabella 4 )  . 
le opacit ground glass inizialmente aumentavano ( 14 / 60 ) per lattenuazione delle opacit consolidative , riducendosi dopo 15 giorni a 5 / 60 ( 8% ) ; in soli due casi da causa ignota , per i quali non fu instaurata terapia eziologica , le lesioni persistevano oltre un mese . 
come reperti associati sono stati apprezzati noduli in 5 casi , strie fibrotiche in 2 , versamento pleurico in 6 ( in un caso anche pericardico ) , incremento delle dimensioni cardiache in 4 pazienti . radiol med ( 2008 ) 113 : 1628 picture improved after 24 h and normalised completely after 15 days . 
 dah in goodpastures syndrome both patients presented with opacities extending to 6 / 6 zones , with a prevalently ground - glass appearance in one patient and a consolidation appearance in the other . 
the ct available for one patient demonstrated limited sparing of the apical regions . dah of unknown cause in three patients with a single dah episode , the aetiological diagnosis could not be established with certainty . 
ct was performed on this patient only : it demonstrated a ground - glass pattern involving 4 / 6 zones as well , but in different sites compared with cxr findings . 
 in the 23 dah episodes , 84 / 138 zones ( 60.8 % ) were affected at onset , with consolidation opacities in 53 / 138 ( 38% ) and ground - glass opacities in 31 / 138 ( 22% )  . 
 follow - up cxr was evaluated in ten patients ( table 4 )  . at onset , 35 / 60 ( 58% ) zones were involved by consolidation opacities and 11 / 60 ( 18% ) were affected by ground - glass opacities . 
after 1 week , consolidation opacities persisted in 16 / 60 ( 26% ) , whereas 15 days later , they persisted in 11 / 60 ( 18% )  . 
ground - glass opacities initially increased ( 14 / 60 ) as a result of the regression of consolidation opacities but decreased after 15 days to 5 / 60 zones ( 8% )  . 
b alla hrct evidenza di aree di opacit ground glass da ead confermata dal lavaggio bronco - alveolare . discussione lead una sindrome clinico - patologica piuttosto rara , caratterizzata da sanguinamento alveolare diffuso , che si manifesta con emottisi , tosse , dispnea ed ipossiemia fino allinsufficienza respiratoria , anemia sideropenica ed opacit radiografiche da occupazione alveolare [ 1 ]  . 
lemottisi , sintomo cardine , di enradiol med ( 2008 ) 113 : 1628 table 4 progression of lesions in 10 patients consolidations ground - glass opacities 36 / 60 11 / 60 onset 7 days later 16 / 60 14 / 60 15 days later 11 / 60 5 / 60 table 5 comparison between chest x - ray ( cxr ) and computed tomography ( ct ) in 14 patients consolidations ground - glass opacities 30 / 84 ( 37% ) 14 / 84 ( 16% ) 32 / 84 ( 38% ) 36 / 84 ( 43% ) tabella 4 evoluzione delle lesioni in 10 pazienti tabella 5 confronto rx / tc in 14 pazienti esordio 7 giorni dopo 15 giorni dopo opacit consolidative opacit ground glass 30 / 84 ( 37% ) 14 / 84 ( 16% ) 32 / 84 ( 38% ) 36 / 84 ( 43% ) opacit consolidative opacit ground glass 36 / 60 11 / 60 16 / 60 14 / 60 11 / 60 5 / 60 in one case a patient with dah in micropolyangiitis ct demonstrated a crazy - paving pattern . 
associated findings included nodules in five cases , fibrotic streaks in two , pleural effusion in six ( in one case also pericardial effusion ) and enlarged heart in four . discussion dah is a rare clinicopathological syndrome characterised by diffuse alveolar bleeding accompanied by haemoptysis , cough , dyspnoea and hypoxaemia , respiratory failure , sideropenic anaemia , and cxr opacities due to alveolar filling [ 1 ]  . 
other signs and symptoms frequently associated with dah are fever , chest pain , elevated erythrocyte sedimentation rate ( esr ) and joint pain [ 11 ]  . in the diagnosis of dah , the following factors are essential : complete blood count , bal ( not always feasible in more acute or severe forms ) , coagulation tests and autoantibody tests ( anca , anti - gbm antibodies )  . 
respiratory function tests , which may indicate increased lung diffusion capacity for carbon monoxide ( dlco ) are not usually possible in the acute phases , whereas they may be helpful in milder forms and during the follow - up . 
in doubtful cases , renal or pulmonary biopsy with surgical or transbronchial sampling may prove useful . the histological pattern , which is almost constant in systemic vasculitis or autoimmune processes , is marked by capillarity [ 12 ]  . 
the essential pathogenetic mechanisms are the precipitation of immunocomplexes on the vessel walls and the production of anca or anti - gbm antibodies tit molto variabile e manca in 1 / 3 dei casi , mentre lanemia pi costante [ 1 ]  . 
altri segni e sintomi che si associano allemorragia alveolare diffusa sono la febbre , le toracoalgie , il rialzo dei valori della eritrosedimentazione ( ves ) , le artralgie [ 11 ]  . per la diagnosi di ead sono fondamentali : lemocromo , il bal , non sempre eseguibile nelle forme pi acute e severe , i test della coagulazione e la ricerca di diversi tipi di autoanticorpi ( anca , ambg )  . 
le prove di funzionalit respiratoria , che possono evidenziare un incremento dei valori della diffusione polmonare del co ( dlco ) , non sono di solito utilizzabili in fase acuta , mentre possono risultare utili nei casi pi lievi e nel follow - up . 
nei casi dubbi pu essere utile lesecuzione di una biopsia renale o polmonare , con prelievo chirurgico o transbronchiale . il quadro istologico , pressoch costante in presenza di vasculite sistemica o di processi autoimmuni , quello della capillarite [ 12 ]  . 
i meccanismi patogenetici fondamentali sono la precipitazione di immunocomplessi a livello delle pareti vasali , la produzione di anca o di anticorpi anti - mb [ 5 , 13 ]  . 
il quadro radiologico dellead caratterizzato da opacit parenchimali da occupazione alveolare , bilaterali , diffuse , di tipo consolidativo o ground glass , con distribuzione predominante in sede perilare ( ad ali di farfalla ) , e risparmio di apici e seni costofrenici . 
 la diagnosi differenziale va posta con le altre cause di opacit da occupazione alveolare come ledema cardiogeno , abitualmente associato a versamento pleurico bilaterale e cardiomegalia o non cardiogeno , e con lessudato inradiol med ( 2008 ) 113 : 1628 fig . 
5a - d diffuse alveolar haemorrhage in micropolyangiitis : chest xray obtained a at onset , b at 24 h and c at 36 h show bilateral consolidations spreading rapidly . 
the radiological pattern of dah is characterised by diffuse , bilateral consolidation or ground - glass opacities due to alveolar filling , predominantly distributed in the perihilar regions ( butterfly wings ) and sparing of the apices and costophrenic angles . 
the parenchymal opacities often appear suddenly , with major changes of site , extension and density observed at short - term follow - up studies [ 7 , 8 ]  . 
in the event of recurrences , incomplete resolution of the opacities evolving into fibrosis may be identified [ 4 ]  . dah needs to be differentiated from other causes of opacity due to alveolar filling , such as cardiogenic oedema usually associated with bilateral pleural effusion and cardiomegaly or noncardiogenic oedema , and from the inflammatory exudate from infectious or eosinophilic pneumonia [ 1 ]  . 
in addition to ground - glass or consolidation opacities , ct may also reveal crazy - paving patterns . our retrospective study reviewed the cxr and ct images of 20 patients with dah . 
specific causes wegeners granulomatosis in eight cases , goodpastures syndrome in two , miidiopathic pulmonary croscopic polyangiitis three , fiammatorio caratteristico delle polmoniti infettive o eosinofile [ 1 ]  . 
in tc si osservano , oltre alle opacit ground glass o consolidative , anche quadri di pattern crazy paving . nel nostro studio retrospettivo sono stati revisionate le indagini radiografiche e tc di venti pazienti affetti da emorragia alveolare diffusa . 
le specifiche cause della emorragia alveolare diffusa erano : in otto casi la granulomatosi di wegener , in due la sindrome di goodpasture , in tre la poliangioite microscopica , in tre lemosiderosi polmonare idiopatica e in uno la sindrome da anticorpi antifosfolipidi . 
in dieci pazienti era possibile valutare levoluzione del quadro radiologico nel follow - up ravvicinato . tipico della ead allesame rx standard , in accordo con i dati della letteratura , la presenza di opacit parenchimali da occupazione alveolare , che si presentano con aspetto di tipo consolidativo o ground glass , diffuse e bilaterali , pi frequenti nei campi polmonari medi con maggioradiol med ( 2008 ) 113 : 1628 haemosiderosis in three and antiphospholipid antibody syndrome in one case . 
 a finding typical of dah on standard cxr , in agreement with the literature , is the presence of diffuse and bilateral parenchymal opacities due to alveolar filling , with a consolidation or ground - glass appearance , more frequent in the middle fields and more evident in perihilar sites ( 75% )  . in our study , the finding was moderately less frequent in the lower zones ( 65% ) and markedly less so in the upper zones ( 43% )  . 
in seven cases with complete or almost complete extension of parenchymal opacities over both lung fields , there was at least partial sparing of the apices or subpleura in five , in agreement with the literature . in patients ( 10 / 20 ) for whom short - term follow - up studies were available , we almost constantly observed a rapid improvement , with findings normalising in 20% after 1 week and in 60% after 2 weeks . 
this result differs slightly from previous studies that report complete normalisation occurring after only 7 days . ct and hrct can confirm the possible presence of consolidation opacities and can detect ground - glass zones more easily . 
ct also identified a single case of crazy - paving pattern , which is characteristic though not pathognomonic of dah [ it may also appear in acute respiratory distress syndrome ( ards ) or acute interstitial pneumonia ]  . 
cxrct correlation was not always possible , as ct studies are difficult to perform in the acute stage when respiratory impairment is most severe . during the follow - up , ct showed no particular advantages over cxr in documenting the evolution of dah . conclusions dah is a relatively rare syndrome characterised by nonspecific radiological patterns of alveolar filling , which usually do not allow for a firm radiological diagnosis . 
a diagnosis or suspicion of dah requires correlation with clinical data that support the diagnostic hypothesis : episodes of haemoptysis or , more importantly , rapid - onset anaemia . the diagnosis of suspected alveolar haemorrhage , if supported by clinical data , may also be established by the radiologist based on the finding of diffuse alveolar - filling opacities , especially if a rapid change of parenchymal opacities is observed . 
the radiological suspicion may often prompt the clinician to rapidly order further imaging and laboratory re evidenza in sede perilare ( 75% ) ; una frequenza modicamente inferiore stata rilevata dal nostro studio nelle zone inferiori ( 65% ) , mentre nettamente inferiore nelle zone superiori ( 43% )  . 
in sette casi , in cui era presente un completa o quasi completa diffusione delle opacit parenchimali su entrambi i campi polmonari , ben 5 presentavano un risparmio almeno parziale degli apici o della regione mantellare , in accordo con quanto riportato in letteratura . dei pazienti ( 10 / 20 ) di cui era disponibile un follow - up ravvicinato si osservato pressoch costantemente rapido miglioramento , con normalizzazione del quadro nel 20% dopo una settimana e nel 60% dopo due settimane . 
ci differisce lievemente dai dati della letteratura che riportano in media una completa normalizzazione gi dopo 7 giorni . lindagine tc e hrtc in grado di confermare la eventuale presenza di opacit consolidative e di evidenziare pi facilmente le zone di ground glass . 
non sempre stato possibile comunque correlare strettamente i quadri rx con quelli tc e hrtc per la difficolt ad effettuare uno studio tc nelle fasi acute di pi severa compromissione respiratoria dei pazienti . 
nel follow - up la tc non ha dimostrato particolari vantaggi rispetto allesame rx per documentare levoluzione della ead . conclusioni lead una sindrome piuttosto rara , con aspetti radiologici aspecifici , di occupazione alveolare che non consentono , di solito , ununivoca diagnosi radiologica . 
per la diagnosi o il semplice sospetto di ead indispensabile la correlazione con i dati clinico - anamnestici che supportino lipotesi diagnostica : episodi di emottisi o , ancora pi importante , una condizione di anemia insorta rapidamente . la diagnosi di sospetto di emorragia alveolare , se supportata dalla clinica , pu essere posta anche dal radiologo sulla base del reperto di opacit diffuse da occupazione alveolare , a maggior ragione se si riscontra una rapida modificazione delle opacit parenchimali ; il sospetto radiologico pu spesso indirizzare il clinico alla rapida esecuzione delle ulteriori indagini strumentali e laboratoristiche indispensabili al definitivo inquadramento della patologia . radiol med ( 2008 ) 113 : 1628 studies , which are vital for the definitive diagnosis . ct , especially hrct , can better evaluate the extent of disease and are definitely more sensitive than cxr , in particular in identifying ground - glass opacities . 
the higher sensitivity of hrct supports its use in patients with possible dah and a negative cxr , such as patients with connectivitis , vasculitis or bone marrow transplant presenting with haemoptysis and mild anaemia . 
the hrct finding of ground - glass areas , although not entirely specific , can guide investigations towards subsequent bronchoscopy and biopsy . la tc e meglio la hrtc consentono di meglio valutare lestensione della patologia e sono sicuramente pi sensibili dellrx , in particolare nel riconoscimento di opacit ground - glass , ma non pi specifiche . 
la maggior sensibilit della hrtc impone il ricorso a questa metodica in pazienti con possibile ead e quadro radiografico negativo , quali pazienti affetti da connettiviti , vasculiti o sottoposti a trapianto di midollo che presentino emottisi e lieve anemia . 
fugazzola1 1vascular and interventional radiology , department of radiology , 2department of oncology , 3department of anaesthesiology , university of insubria , viale borri 57 , 21100 varese , italy correspondence to : d . 
this study was done to assess the effectiveness and advantages of computed tomography ( ct ) fluoroscopy as a guide for locating and treating lesions that are not amenable to ultrasound ( us ) guidance , and to evaluate the ct signs of immediate technical success and the shortterm results . 
over the past year , we selected 14 patients ( four women and ten men ; mean age 73 , range 6183 years ) out of 103 candidates for hepatic radiofrequency ablation ( rfa )  . 
the 14 lesions comprised seven residual tumours after combined embolisation and us - guided rfa of a large hepatocellular carcinoma ( hcc ) , which were indistinguishable from necrosis or surrounding healthy parenchyma ; two hcc nodules in locations that were inaccessible by us ; five metastases ( two from renal carcinoma , two from colorectal adenocarcinoma and one from lung carcinoma ) , of which one could not be distinguished from the surrounding healthy parenchyma on us and four were inaccessible by us . 
nellultimo anno abbiamo selezionato 14 / 103 pazienti ( 4 femmine e 10 maschi ) candidati a un trattamento di radiofrequenza ( rf ) epatica , et media 73 anni ( range 6183 ) portatori di 14 lesioni epatiche : 7 residui di grosso hcc , esito di terapia combinata mediante embolizzazione e rf eco - guidata non distinguibili dalla necrosi o dal parenchima epatico sano circostante ; 2 noduli di hcc non raggiungibili con guida ecografica per sede ; 5 metastasi ( 2 da carcinoma del rene , 2 da adenocarcinoma del colon - retto e 1 da carcinoma del polmone ) , di cui 1 non distinguibile dal parenchima sano circostante allecografia e 4 non raggiungibili per sede . 
le lesioni presentavano diametro compreso tra 1 , 4 e 3 , 5 cm . le procedure sono state espletate in sala tc in assistenza anestesiologica con ago elettrodo di leveen coassiale ( 14 gauge , diametro apertura uncini da 2 a 4 cm )  . 
nelle 3 lesioni metastatiche a prevalente vascolarizzazione veno - portale si documentato successo tecnico immediato e assenza di radiol med ( 2008 ) 113 : 87100 observed disease progression , with the appearance of additional nodules at 6 months . 
the two metastases with arterial supply showed no signs of recurrence at 3 months ; one case developed a recurrence along the ablation margin , with the appearance of satellite nodules at 6 months . 
ct fluoroscopy is overcoming the limitations of ct in locating and treating lesions with different hepatic vascularisation and those unamenable to us ; furthermore , it reduces the length of the procedure , thanks to the faster and more accurate placement of the needle electrode . 
le 2 metastasi a prevalente vascolarizzazione arteriosa , non hanno evidenziato a 3 mesi segni tc di recidiva ; a 6 mesi in 1 caso si documentata una recidiva lungo il margine di ablazione e comparsa di microlesioni satelliti . 
la guida fluoro - tc ha attualmente superato i limiti della tc nel localizzare e trattare lesioni a differente vascolarizzazione epatica e quelle non fattibili sotto guida ecografica ; inoltre ha ridotto i tempi di procedura per il pi veloce ed accurato posizionamento dellago - elettrodo . 
la tcms si dimostrata metodica affidabile nella valutazione dei risultati della rf immediati e a breve distanza . parole chiave radiofrequenza mdct fluoro - tc introduction introduzione the indications and limitations of treating primary and secondary liver tumours with radiofrequency ablation ( rfa ) have been extensively debated and are now well established [ 13 ]  . 
although ultrasound ( us ) guidance is the fastest , it is unfeasible in several cases ; for example , when the lesion has an echogenicity that does not permit differentiation from the surrounding parenchyma or when its location renders the lesion inaccessible . 
in particular , ct - fluoroscopy guidance combines the high spatial resolution and good contrast resolution inherent to contrast - enhanced ct [ 4 ] with the immediacy of fluoroscopic monitoring [ 5 ]  . 
nonetheless , ct guidance is limited in centring hypervascular lesions because of the short duration of arterial enhancement . the purpose of this study was to assess the effectiveness of ct - fluoroscopy guidance in the location and treatment of lesions with arterial or portal vein supply and unamenable to us because of their location , and to assess ct signs of immediate and short - term technical success . le indicazioni ed i limiti del trattamento dei tumori primitivi e secondari del fegato mediante ablazione con radiofrequenza ( rf ) sono stati ampiamente discussi e ben codificati [ 13 ]  . 
la guida ecografica sicuramente la pi veloce ma in alcuni casi non fattibile , qualora la lesione abbia unecogenicit non distinguibile dal parenchima circostante o non sia raggiungibile per la sua sede . 
in tali casi la guida mediante tomografia computerizzata ( tc ) offre una valida alternativa ; in particolare la guida fluorotc somma lalta risoluzione spaziale della tc e la buona risoluzione di contrasto ottenibile mediante linfusione di mezzo di contrasto ( mdc ) [ 4 ] con limmediatezza del controllo fluoroscopico [ 5 ] ; la guida tc presenta comunque dei limiti nella centratura di lesioni ipervascolari in relazione alla breve durata dellenhancement arterioso . scopo del lavoro valutare lefficacia dellulteriore vantaggio della guida fluoro - tc nel localizzare e trattare lesioni a differente vascolarizzazione epatica non fattibili o non raggiungibili per sede con guida ecografica e valutarne i segni tc di successo tecnico immediato e a breve distanza di tempo . radiol med ( 2008 ) 113 : 87100 materials and methods between october 2005 and october 2006 , 103 hepatic rfa procedures were carried out at our institute : 89 / 103 were performed under us guidance , whereas 14 lesions in 14 patients ( 4 women and 10 men ) , mean age 73 ( range 6183 years ) were treated under ct - fluoroscopy guidance ( aquilian 64 - slice ct , toshiba europe medical systems )  . 
of the four patients with metastasis , 2 / 4 , with metastasis from colorectal cancer , presented high carcinoembryonic antigen ( cea ) levels ( 75 ng / ml and 104 ng / ml ) , whereas 1 / 4 , with metastasis from squamous cell lung carcinoma , had elevated cytokeratin 19 fragment ( cyfra 21 - 1 ) levels ( 3.2 ng / ml )  . 
seven patients ( with residual tumour from hcc ) had previously undergone liver rfa ; the remaining 7 / 14 had undergone no previous surgical or percutaneous treatment on the liver . 
 the procedure was carried out in the ct room with anaesthesiological assistance ( patient sedated with 12 mg of midazolam , 13 mg of alfentanil , 50150 mg of propofol intravenously , and oxygen by face mask )  . 
 in all cases , we used a coaxial 14 - gauge leveen needle electrode ( boston scientific , san jos , ca , usa ) , with a 2to 4 - cm array diameter , connected to a 200 - w generator ( rf 300 , boston scientific )  . 
le lesioni presentavano diametro compreso tra 1 , 4 e 3 , 5 c undici lesioni avevano una prevalente vascolarizzazione arteriosa quindi caratterizzate da una fugace iperdensit nella sola fase arteriosa e 3 lesioni invece vascolarizzazione portale , quindi a marcata ipodensit nella sola fase veno - portale . 
dei 4 pazienti con metastasi , 2 / 4 con metastasi da colonretto presentavano un incremento dei valori del cea ( 75 ng / ml e 104 ng / ml ) in 1 / 4 con metastasi da carcinoma spinocellulare del polmone un aumento del cyfra 21 - 1 ( 3 , 2 ng / ml ) ; il paziente con metastasi da carcinoma del rene non presentava alterazione dei marcatori tumorali . 
sette pazienti ( con residuo di hcc ) erano stati sottoposti in precedenza a rf epatica ; i rimanenti 7 / 14 non avevano subito pregressi trattamenti chirurgici o percutanei a livello epatico . 
 le procedure sono state espletate in sala tc in assistenza anestesiologica ( paziente in sedazione ottenuta con somministrazione endovenosa di midazolam 12 mg , alfentanyl 13 mg , propofol 50150 mg , associata ad ossigeno in maschera ) ; stata inoltre praticata anestesia locale lungo il sito daccesso mediante 5 ml carbocaina 2% ( carbocaina , astrazeneca , basiglio , italia )  . in tutti i pazienti stata inoltre effettuata una profilassi antibiotica . 
mean hospital stay was 2.3 ( range 15 ) days . tanea di mdc solo per le lesioni ipervascolarizzate con rapido wash - out ( 12 boli da 50 ml a 4 ml / s , concentrazione 400 mgi / ml seguita da 30 ml di fisiologica a 4 ml / s ; la dose massima complessiva di mdc somministrata stata , come raccomandato , di 2 ml per kg di peso del paziente )  . 
b , c due to its size , the lesion was treated with embolisation ( b ) ( black arrow ) combined with radiofrequency ablation ( c ) ( white arrow )  . 
d mdct at 1 month , arterial phase : a marginal residual nodule is seen ( black arrow ) ; small lipiodol residues from the previous embolisation can be seen close to the residual tumour . 
f , g mdct at 3 months : no signs of recurrence along the ablation margins ; small lipiodol residues persist inside the ablation area ( black arrow ) ; the size of the ablation area is unchanged . 
h , i mdct at 12 months : no signs of recurrence , and ablation area unchanged in size ; disease progression with the appearance of satellite micronodules ( black arrow )  . 
b , c le dimensioni fanno optare per il sinergismo della terapia combinata della lesione mediante embolizzazione ( b ) ( freccia nera ) e rf ( c ) ( freccia bianca )  . 
marcatamente aumentato in dimensioni il nodulo da insemenzamento sottocutaneo ( freccia bianca )  . risultati stato ottenuto successo tecnico immediato in 13 / 14 pazienti , valutato mediante tcms come assenza di residuo per mancata impregnazione della lesione a prevalente vascolarizzazione arteriosa e in tutti i casi per margini di ablazione che comprendevano e superavano la lesione . 
nelle 3 lesioni metastatiche a prevalente vascolarizzazione veno - portale ( 2 da adenocarcinoma colon - rettale e 1 da carcinoma spinocellulare polmonare ) , si documentato successo tecnico immediato e assenza di recidiva a 3 e 6 mesi in tutti i 3 casi . 
larea di ablazione presentava ridotta densit a margini ben definiti con cercine di granulazione assente e dimensioni superiori alla lesione trattata a 3 mesi e pressoch immodificata per dimensioni e caratteristiche al controllo a 6 mesi ; laltra ha avuto una ripresa di malattia a 6 mesi per comparsa di ulteriori noduli epatici . 
b ricostruzioni mpr con finestra da polmone : riconoscibile lungo tutto il decorso lago elettrodo avanzato mediante approccio trans - polmonare con dispiegamento degli uncini nel contesto della lesione sottodiaframmatica . 
 d tcms a 6 mesi : area di ablazione di ridotta densit a grossolana morfologia semilunare con dimensioni nettamente superiori rispetto alla lesione trattata ; assente il cercine denso marginale di granulazione . results immediate technical success was achieved in 13 / 14 patients , defined as mdct absence of residual tumour based on lack of enhancement of lesions with arterial supply and ablation margins comprising and extending beyond the lesion in all cases . 
in the three metastatic lesions with portal vein supply ( two from colorectal adenocarcinoma and one from squamous cell carcinoma of the lung ) , mdct demonstrated immediate technical success and no recurrence at 3 and 6 months . 
the ablation area showed low density , well - defined margins and absence of granulation riit appeared larger than the treated lesion at 3 months and remained unchanged in size and shape at 6 months . 
3 a multidetector computed tomography ( mdct ) at 1 month , arterial phase : near the low - density area ( black arrow ) , the outcome of an ultrasoundguided radiofrequency ablation , a crescent - shaped , hyperdense area due to residual hepatocellular carcinoma can be seen ( white arrow )  . 
b postprocedural mdct , arterial phase : the hypervascular lesion has disappeared and has been replaced by a rounded hypodense ablation area with a dense marginal rim produced by inflammation ( black arrow )  . 
within the ablated area , the hooks of the needle electrode can be clearly seen , with their typical umbrella - like shape ( white arrow ) c , d mdct at 3 months ( c arterial phase ; d portal phase ) : the dense marginal rim has disappeared ; it is partially recognisable as a thin rim in the portal phase only ( black arrow ) ; the ablation area is well delimited and appears smaller . 
e , f mdct at 6 months : further shrinkage of the ablation area without signs of recurrence along the ablation margins ( black arrow )  . fig 3 a tcms a 1 mese , fase arteriosa : a ridosso di area di ridotta densit ( freccia nera ) esito di rf con guida ecografia ; riconoscibile area iperdensa semilunare con significato di residuo di hcc ( freccia bianca )  . 
b tcms post - procedura , fase arteriosa : non pi riconoscibile la lesione ipervascolarizzata sostituita da area tondeggiante di ablazione di ridotta densit con spesso cercine denso marginale di tipo infiammatorio ( freccia nera )  . 
c , d tcms a 3 mesi ( c fase arteriosa ; d fase veno - portale ) : assente il cercine denso marginale riconoscibile a tratti nella sola fase veno - portale ( freccia nera ) come sottile orletto . 
the granulation rim can be distinguished from residual tumour in that it is concentric , has regular margins , appears hypervascular in the arterial and / or portal phase and never shows portal - phase washout , which is typical of viable tumour . 
it was later applied to primary and secondary lesions of the liver and lung and less commonly to renal , adrenal , and bone neoplasms , to thyroid and parathyroid nodules and to breast and prostate cancers [ 812 ]  . rfa is based on the generation of heat inside the lesion , with temperatures exceeding 50c . 
if that temperature is maintained for more than 3 min , intracellular proteins are denatured and membrane lipids dissolved , resulting in cell death by coagulation necrosis [ 1015 ]  . 
the availability of a coaxial system is especially useful for needle placement under ct guidance : this system allows preliminary positioning of a needle discussione la termoablazione percutanea con rf una tecnica mini - invasiva che stata inizialmente proposta per il trattamento delle anomalie della conduzione cardiaca , della nevralgia del trigemino [ 6 ] e dellosteoma osteoide [ 7 , 8 ] ; successivamente stata applicata alle lesioni primitive e secondarie del fegato e del polmone e , pi raramente , alle neoplasie renali , surrenali , ossee , ai noduli tiroidei e paratiroidei , nonch ai tumori della mammella e della prostata [ 812 ]  . la tecnica di rf si basa sullo sviluppo di calore allinterno della lesione con temperature superiori ai 50c . 
il mantenimento di tale temperatura per pi di 3 minuti determina la denaturazione delle proteine intracellulari e la dissoluzione dei lipidi di membrana con conseguente morte cellulare per necrosi coagulativa [ 1015 ]  . 
lago - elettrodo di leveen ( 14 g ) utilizzato nel nostro studio dotato di 10 uncini retrattili che una volta aperti vanno ad assumere la tipica configurazione ad ombrello . 
particolarmente utile per il posizionamento mediante guida tc la disponibilit di un sistema coassiale che consente il preliminare posizionamento di un ago - trocar , con inserimento successivo dellago elettrodo e apertura degli uncini ; il materiale del trocar non trasmette il calore lungo il suo decorso garantendo quindi un sicuro approccio anche trans - polmonare [ 17 ] e inoltre , in questi , casi retraendo la cannula , al termine della procedura , possibile aspirare eventuali falde di pneumotorace . per quanto riguarda le indicazioni , la rf epatica attualmente proposta come terapia curativa , con il vantaggio , rispetto alla chirurgia , di preservare pi parenchima epatico sano , nella lesione singola primitiva epatica con dimensioni non superiori ai 4 cm in relazione alle attuali dimensioni dellago . 
in pazienti con cirrosi epatica compensata ( child a / b ) possibile effettuare lablazione di un massimo di 3 lesioni di hcc , se confinati ad un singolo lobo epatico , con diametro non superiore ai 4 cm [ 18 ]  . 
possibile effettuare un trattamento con pi infissioni o pi sedute e ripetere ulteriormente il trattamento quando compare una nuova lesione , come accade nella maggior parte dei pazienti cirrotici entro 5 anni . 
parimenti indicata in pazienti con metastasi epatiche anche se interessano entrambi i lobi epatici , fino ad un massimo di 5 lesioni con diametro non superiore ai 4 cm , secondarie a qualunque neoplasia primitiva precedentemente trattata radicalmente , nei confronti delle quali la chirurgia non attuabile , controindicata o non tollerata dal paziente [ 3 ]  . radiol med ( 2008 ) 113 : 87100 trocar , with subsequent insertion of the needle electrode and deployment of the hooks . 
in addition , in these cases , on removing the cannula at the end of the procedure , possible areas of pneumothorax can be aspirated . hepatic rfa is currently indicated as a curative procedure for single primary liver lesions up to 4 cm in diameter in relation to the size of current needles . 
in patients with compensated liver cirrhosis ( child a / b ) , as many as three hcc lesions up to 4 cm can be ablated if they are confined to a single hepatic lobe [ 18 ]  . treatment with multiple electrode placements or over multiple sessions is also possible , and the same treatment can be repeated when a new lesion appears , as occurs within 5 years in most cirrhotic patients . 
rfa is also indicated for liver metastases affecting both hepatic lobes : in particular , up to five lesions 4 cm or less in diameter secondary to cancers that have been resected , in which surgery is impossible , contraindicated or not tolerated by the patient [ 3 ]  . today , size is no longer an absolute limitation of rfa of neoplastic lesions , thanks to the development of larger needle electrodes of varying shape producing a 4to 5 - cm area of necrosis per placement , the possibility of multiple needle placements and the local infusion of hypertonic saline solution , which would increase the volume of necrosis by increasing tissue impedance [ 10 , 16 ]  . 
currently , most primary and secondary hepatic lesions are treated under us guidance , as the method is widely available , inexpensive , allows virtually unlimited viewing angles even with the transcostal approach and is carried out in real time . 
the procedure is markedly operator dependent , as success is influenced by the operators promptness in locating and penetrating the lesion at the passage of the us contrast agent , and the treatment can only be performed on lesions that are isoechoic to the surrounding parenchyma [ 19 ]  . ct - fluoroscopy guidance , in our experience , is indispensable , as it is the only technique capable of reaching the lesion and it is useful when the lesion , although visualised on us , cannot be accessed with us because of its location . furthermore , as sporadically reported in the literature [ 17 , 18 , 20 ] , ct guidance allows transpulmonary access to subdiaphragmatic hepatic lesions , which are usually inaccessible under us guidance . 
attualmente la maggior parte delle lesioni primitive e secondarie del fegato vengono trattate sotto guida ecografica , poich questa metodica ampiamente disponibile , a basso costo , le angolazioni possibili sono virtualmente illimitate , anche mediante approccio trans - costale , e la procedura viene eseguita in tempo reale . 
inoltre possibile lutilizzo del mdc ecografico che ha il solo limite della singola dose e della fugacit che comporta un limitato tempo di azione ; pertanto il successo del trattamento dipende dalla velocit e dalla rapidit delloperatore nel localizzare e penetrare la lesione al passaggio del mdc ecografico , quindi molto operatore dipendente e attuabile chiaramente solo nelle lesioni che presentano una diversa ecogenicit rispetto al parenchima circostante [ 19 ]  . la guida fluoro - tc , nella nostra esperienza , ha dimostrato di essere una alternativa indispensabile quando la sola tecnica capace di raggiungere la lesione e diviene utile quando la lesione , pur essendo identificabile con lecografia , non aggredibile con tale metodica a causa della sua localizzazione . 
inoltre la guida tc permette laccesso trans - polmonare per le lesioni epatiche localizzate in sede sottodiaframmatica generalmente inaccessibili con guida ecografia come riportato in letteratura in casi sporadici [ 17 , 18 , 20 ]  . 
da una revisione della letteratura [ 4 , 17 , 18 , 2023 ] di alcuni autori che hanno utilizzato la guida tc quale alternativa allecografia risultano trattate con guida tc 49 lesioni ( 2 delle quali mediante fluoro - tc ) ; di queste lesioni , 34 / 49 sono hcc mentre le rimanenti sono metastasi con una netta prevalenza di lesioni secondarie ad adenocarcinoma colon - rettale . 
 la rapida identificazione di lesioni a differente vascolarizzazione e della punta / direzione dellago il sicuro vantaggio della guida fluoro - tc dovuto al tempo di scansione tanto breve quanto sufficiente per la ricostruzione dellimmagine . 
questo combina lelevata risoluzione spaziale sul piano assiale tipica della tc , con lelevata risoluzione temporale della fluoroscopia , permettendo la visualizzazione in tempo reale della lesione , della punta e della direzione dellago durante tutta la procedura . 
 prompt visualisation of lesions with arterial or portal supply and of the tip / direction of the needle is a major advantage of ct fluoroscopy , resulting from a scan time that is as short as needed for reconstruction . 
this combines the high spatial resolution in the axial plane of ct with the high temporal resolution of fluoroscopy , allowing real - time visualisation of the lesion , and the tip and direction of the needle throughout the procedure . 
from the control console , the operator can independently move the table , tilt the tube and acquire fluoroscopic images that can be viewed on the control monitor next to the ct table . therefore , the procedure is performed during the simultaneous assessment of three contiguous scan planes displayed on the monitor : the plane of the lesion and the planes immediately above and below . 
this increases significantly the longitudinal resolution along the z axis and consequently the systems reliability , as the actual direction of the needle is more accurately defined in the craniocaudal direction . 
if , as the needle advances , the tip is no longer visualised in the lesion plane but in the plane above the lesion , it means that the needle is being tilted too cranially ; if , conversely , the tip appears in the plane below , its direction will be too caudal . ct fluoroscopy can be used with three operational modes : continuous fluoroscopy , used from the moment the needle is inserted to when the lesion is reached ; spot - check fluoroscopy , to confirm the position of the tip and ensure direction is maintained after a short advancement of the needle ; mixed continuous and spot check , where the continuous mode is used only to overcome particularly difficult anatomical and procedural situations [ 24 ]  . 
 when rfa is performed under continuous ct - fluoroscopy guidance , one needs to take into account the possible consequences of exposure of the operators hands to the direct beam and therefore to higher radiation doses [ 25 ]  . dose measurements for the operators hand carried out by irie et al . 
given these dose rates , the operator may be forced to limit the number of procedures done each year to keep within the dose limits of 20 msv / year for the entire body and of 500 msv / year for the hands . 
pertanto la procedura viene effettuata mediante la simultanea valutazione di una triplice immagine fluoroscopica , vale a dire che sul monitor vengono visualizzati contemporaneamente 3 piani contigui di scansione : il piano della lesione e i piani adiacenti sopra e sottostanti . 
questa opportunit incrementa notevolmente la risoluzione longitudinale lungo lasse z e quindi laffidabilit del sistema , in quanto viene pi dettagliatamente definita leffettiva direzione in senso cranio - caudale dellago . 
se , infatti , durante lavanzamento dellago si nota che la punta non viene pi visualizzata nel piano centrale ma in quello soprastante si intuisce che si sta imprimendo allago uninclinazione troppo craniale , se viceversa si visualizza la punta nel piano sottostante la direzione sar troppo caudale . sono possibili 3 modalit operative : la fluoroscopia continua durante linserimento dellago fino al raggiungimento della lesione ; la fluoroscopia di rapido controllo o spot caratterizzata da avanzamento per breve tratto dellago e successivo spot di scopia , il pi breve possibile , per la verifica della posizione della punta e del mantenimento della direzione programmata ; da ultimo possibile una modalit mista , sia continua che spot , riservando la modalit continua al superamento di situazioni anatomiche ed operative particolarmente problematiche [ 24 ]  . 
 quando il trattamento di rf viene condotto sotto guida fluoro - tc continua , bisogna considerare anche le possibili conseguenze derivate dallesposizione delle mani delloperatore al fascio diretto quindi a dosi di radiazione pi elevate [ 25 ]  . 
con queste misurazioni pu accadere che loperatore deve limitarsi a realizzare solo un certo numero di interventi per anno considerando la limitazione della dose a 20 msv / anno per lintero corpo e 500 msv / anno per le mani . 
una significativa riduzione della dose per loperatore pu essere ottenuta utilizzando solo dei sottili guanti di protezione in piombo , i quali riducono del 77% la dose sulla mano delloperatore . 
pi lungo il supporto dellago minori sono le radiol med ( 2008 ) 113 : 87100 operators from scattered radiation consists in placing lead drapes under and over the patient , close to the access site , as indicated by previous studies [ 29 ]  . 
finally , the use of needle supports ( either long or short ) allows the hands to be kept away from the direct beathe longer the needle support , the lower the radiation doses to the hand . 
nonetheless , needle supports cannot be used in all cases because of the difficulty in manoeuvring the needle , especially when the force applied is not sufficient to reach deep lesions . 
the combination of lead drapes , bismuth gloves and needle supports proved to be the most effective solution , with almost 100% dose reduction [ 30 ]  . in the assessment of immediate and long - term results , contrast - enhanced us has been proposed to determine the extent of the ablation area and the absence of residual tumour [ 19 ]  . 
ct is , however , the most widely used technique for the assessment of long - term results in lesions treated with rfa , even though mri according to some authors is more accurate in monitoring the acute effects of the treatment [ 10 , 15 , 31 ]  . 
an advantage of mri is its ability to assess the volume of coagulation necrosis in real time during the application of energy [ 16 , 32 ]  . postprocedural ct shows a hypodense area often containing numerous , irregularly distributed , small air inclusions of varying size , which indicate that coagulation necrosis has taken place . 
two minutes after rfa , attenuation of the treated tissue decreases by 14 hu compared with the healthy liver , a difference that increases to 22 hu after 8 min [ 33 ]  . 
the ablated area appears rounded , with well - defined borders and surrounded by a thick , relatively hyperdense , rim representing an inflammatory reaction , and larger than the initial lesion . 
in contrast , in the case of incomplete ablation , the borders are ill defined , and the peripheral viable tumour shows similar enhancement to that of the initial lesion [ 16 , 37 ]  . 
minor complications include haemobilia , asymptomatic pleural effusion , cholecystitis ( with lesions adjacent to the gallbladder ) , abdominal pain caused by peritoneal irritation , shoulder pain from diaphragmatic irritation , fever due to treatment - induced necrosis , abscesses and biliary fistula [ 39 , 40 ]  . 
tuttavia , non in tutti i casi pu essere utilizzato il supporto , a causa delle difficolt nel manovrare lago , specialmente quando viene esercitata una forza di penetrazione insufficiente per raggiungere lesioni profonde . 
la combinazione di teli di piombo , guanti di bismuto , ed il supporto per lago si dimostrata la soluzione pi efficace con una riduzione di circa il 100% [ 30 ]  . nella valutazione dei risultati immediati e a distanza lecografia con mdc stata proposta per determinare lestensione dellarea di ablazione e lassenza di residui [ 19 ] ; comunque la tc la tecnica maggiormente utilizzata per la valutazione dei risultati a distanza delle lesioni sottoposte a rf , bench la rm secondo alcuni autori sia pi accurata per il monitoraggio degli effetti acuti del trattamento [ 10 , 15 , 31 ]  . 
a 2 minuti dalla rf il tessuto trattato mostra unattenuazione inferiore di 14 uh rispetto al tessuto epatico sano , e questa differenza aumenta a 22 uh dopo 8 minuti [ 33 ]  . 
dopo somministrazione di mdc , la differenza di attenuazione tra il tessuto sottoposto ad ablazione con rf e il tessuto epatico sano aumenta a 55 uh [ 3436 ]  . 
larea di ablazione appare a morfologia tondeggiante con profili ben definiti per spesso cercine marginale di relativa iperdensit espressione di avvenuta reazione infiammatoria , di dimensioni maggiori rispetto al nodulo di partenza . 
nel caso di ablazione parziale , invece , i profili risultano mal definiti e il tessuto tumorale marginale vitale mantiene un enhancement analogo a quello della lesione iniziale [ 16 , 37 ]  . 
tra le complicanze minori sono stati descritti : emobilia , versamento pleurico asintomatico , colecistite ( in caso di lesione localizzata a ridosso della colecisti ) , dolore addominale da irritazione peritoneale , dolore alla spalla da irritazione diaframmatica , iperpiressia dovuta ai fenomeni necrotici indotti dal trattamento , ascessi , fistola biliare [ 39 , 40 ]  . 
this might be caused , as postulated by various authors [ 41 ] , by a previous biopsy of the lesion or by multiple placements of the needle cannula or needle electrode inside the lesion before the ablation . in addition to the postprocedural assessment of the immediate technical success to differentiate residual tumour from the dense inflammatory rim , further evaluations need to be performed after some time . 
this time interval allows identification of possible nodular recurrences along the ablation margins , which can be distinguished from the thin , dense peripheral granulation rim that is absent or discontinuous after 3 months . 
the ablation area , or scar , is larger than the treated lesion , as it includes the lesion and a safety margin of at least 0.51 cif treatment is successful , after 6 months or sometimes longer the scar shrinks , with complete disappearance of the peripheral granulation rim and unchanged hypodensity ( 22 hu )  . the world health organisation or response evaluation criteria in solid tumours ( recist ) dimensional criteria [ 42 ] , therefore , cannot be used to document response to ablation therapies , at least not in the immediate posttreatment period . 
based on these criteria , the effectiveness of cancer treatment is assessed by measuring the extent of tumour shrinkage , a parameter that cannot be applied to thermal ablation procedures . 
however , the most common criterion to assess the procedures effectiveness on ct , mri or contrast - enhanced us is the absence of enhancement in the treated tissue , although this may change with the introduction of routine positron emission tomography ( pet )  . 
questo possibile che si realizzi , come da pi autori ipotizzato [ 41 ] , per pregressa biopsia della lesione o per pi posizionamenti dellago cannula o dellagoelettrodo allinterno della lesione prima dellablazione . oltre alla valutazione del successo tecnico immediato post - procedura che differenzia il residuo dal cercine denso marginale di tipo infiammatorio necessario eseguire una valutazione a distanza ; questo intervallo di tempo consente di identificare leventuale recidiva nodulare generalmente lungo i margini di ablazione gi distinguibile dallesile cercine denso marginale di granulazione assente o riconoscibile solo a tratti ai 3 mesi . 
larea di ablazione o scar ( cicatrice ) risulta pi grande della lesione trattata , includendo la lesione e un margine di sicurezza di almeno 0 , 51 ca 6 mesi se il trattamento ha avuto successo , questa cicatrice diminuisce di dimensioni , anche se questo pu avvenire pi lentamente , con completa scomparsa del cercine di granulazione marginale e mantenendo immodificata lipodensit ( 22 uh )  . i criteri dimensionali della who o del recist [ 42 ] , pertanto , non possono essere applicati per documentare la risposta alle terapie ablative almeno non nellimmediato periodo post - trattamento . 
quindi sono necessari altri metodi per accertare lefficacia della rf ; attualmente non c un chiaro consenso su quali metodiche di imaging siano pi appropriate per il follow - up post - ablazione . 
in ogni caso il criterio pi comunemente utilizzato per valutare lefficacia delle procedura attraverso la tc , la rm o lecografia con mdc lassenza dellenhancement del tessuto trattato in attesa di poter utilizzare la pet di routine . oggi nella valutazione dei risultati il ricorso alla pet o alla pet - tc da riservare , secondo alcuni , ai casi dubbi ; la proposta di impiegare tale metodica conseguente ai buoni risultati ottenuti nella valutazione dei risultati di lesioni trattate con rf anche in altri distretti [ 43 ]  . 
limaging per la valutazione dei risultati viene poi necessariamente integrato con un controllo clinico e bioumorale specifico [ 10 ]  . conclusions conclusioni ct guidance has always proved to be a valid percutaneous approach to rfa of primary and secondary liver tumours that cannot be accessed under us guidance owing to their location . 
real - time ct - fluoroscopy guidance has overcome the limitations of ct in the localisation and treatment of lesions that are inaccessible to us guidance , even when the lesions are small and have a transient and rapid enhancela guida tc ha da sempre dimostrato di essere un valido approccio percutaneo al trattamento mediante rf dei tumori primitivi e secondari del fegato non raggiungibili sotto guida ecografia per sede con le medesime indicazioni e risultati . 
la guida fluoro - tc in tempo reale ha attualmente superato i limiti della tc nel localizzare quindi trattare lesioni non fattibili sotto guida ecografica anche di piccole radiol med ( 2008 ) 113 : 87100 ment in the arterial phase alone . 
rasori 10 , 43100 parma , italy 2dipartimento di scienze radiologiche , sezione di diagnostica per immagini , ospedale maggiore - universit degli studi di parma , via gramsci 14 , 43100 parma correspondence to : a . 
in all subjects , hrct scanning , at suspended end - expiratory volume , was performed at rest and during ventilation with 6 and 12 cmh2o by nasal insufflation with continuous positive airway pressure ( ncpap ) , both at baseline and after inhalation of 200 g oxitropium bromide metered dose inhaler ( mdi )  . 
abbiamo studiato 7 pazienti ( 2 maschi , range di et : 3669 anni ) con asma cronica in condizioni cliniche stabili ( fev1 range : 30%87% del valore predetto ; fev1 / fvc range : 48%75% del valore predetto ) e 6 controlli sani ( 3 maschi , range di et : 2950 anni )  . 
in tutti i soggetti sono state effettuate scansioni hrct a fine espirazione a riposo e durante ventilazione mediante cpap con 6 e 12 cmh2o , sia in condizioni basali , sia dopo inalazione di 200 g di oxitropio bromuro mdi . 
nei pazienti asmatici , linsufflazione con la pressione di 12 cmh2o ha cambiato in modo significativo il diametro di base del lume ( 3 , 30 , 7 mm vs 3 , 80 , 6 mm ; p < 0 . , 01 ) e il diametro esterno ( 6 , 20 , 9 mm vs 6 , 70 , 8 mm ; p < 0 , 05 ) mentre nei controlli sani , linsufflazione con la pressione di 6 cmh2o e di 12 cmh2o ha prodotto cambiamenti significativi a carico del diametro basale del lume ( 4 , 01 , 6 mm vs 4 , 81 , 6 mm e 4 , 71 , 7 mm ; p < 0 , 01 )  . nei pazienti asmatici , linalazione di oxitropio bromuro ha cambiato significativamente il diametro di base del lume ( 3 , 30 , 7 mm vs 4 , 40 , 6 mm ; p < 0 , 05 ) mentre radiol med ( 2008 ) 113 : 4355 the application of 6 or 12 cmh2o insufflation did not modify any bronchial diameters . 
nei controlli sani linalazione di oxitropio bromuro ha modificato in modo significativo il diametro di base del lume ( 4 , 01 , 6 mm vs 5 , 01 , 5 mm ; p < 0 , 05 )  . 
i nostri risultati dimostrano che nei pazienti asmatici il grado di distensibilit delle vie aeree , misurato mediante hrct , pu essere diverso se comparato a quello dei controlli sani . 
la hrtc pu fornire informazioni utili sulla distensibilit delle vie aeree . parole chiave asma imaging del torace tc ad alta risoluzione introduction introduzione asthma is an inflammatory lung disease characterised by increased airway reactivity to various stimuli and airflow obstruction that is at least partially reversible [ 1 ]  . 
whereas acute inflammation is a beneficial nonspecific response of tissues to injury that generally leads to repair and restoration of normal structure and function , asthma represents a chronic inflammatory process followed by healing , the end result of which is characteristically an altered structure referred to as airway remodelling [ 2 ]  . 
the subgroup of asthmatic subjects with irreversible airflow obstruction is of importance because these subjects experience considerable morbidity and account for a high percentage of asthma - related health costs [ 4 ]  . 
early markers of airway remodelling might be important for managing asthmatic patients . we used high - resolution computed tomography ( hrct ) to examine the ability of mechanical pressures via nasal insufflation to distend the airways of subjects with chronic asthma , who were compared with healthy subjects at baseline and after reducing airway tone with an anticholinergic drug . 
 materials and methods six healthy controls and seven individuals with asthma were lasma una malattia infiammatoria dei polmoni che caratterizzata da uniper - reattivit delle vie aeree verso vari stimoli e da unostruzione al flusso parzialmente reversibile [ 1 ]  . 
mentre linfiammazione acuta una risposta non specifica dei tessuti che generalmente conduce alla riparazione strutturale e al ripristino funzionale nei confronti di un meccanismo lesivo , lasma rappresenta un processo infiammatorio cronico delle vie aeree il cui risultato finale caratteristicamente unalterazione strutturale definita come rimodellamento [ 2 ]  . 
importante tenere in considerazione il sottogruppo di pazienti asmatici con ostruzione irreversibile a carico delle vie aeree , perch questi pazienti sono affetti da una considerevole morbilit e sono rappresentano unalta percentuale dei costi in termini di salute dovuti allasma [ 4 ]  . 
marcatori precoci di rimodellamento delle vie aeree potrebbero essere importanti per il management dei pazienti asmatici . in questo studio abbiamo utilizzato la tc ad alta risoluzione ( hrct ) per esaminare la capacit delle pressioni meccaniche , attraverso linsufflazione nasale , di distendere le vie aeree dei soggetti affetti da asma cronica rispetto a controlli sani in condizioni basali e dopo riduzione del tono delle vie aeree mediante un farmaco anti - colinergico . radiol med ( 2008 ) 113 : 4355 enrolled in the study . 
the seven patients affected by chronic asthma ( two men , age range 3669 years ) had a diagnosis of asthma according to the american thoracic society criteria [ 5 ] for at least 5 years , and they had no acute exacerbation within the preceding 3 months . 
 spirometry spirometry was measured by a flow - sensing spirometer connected to a computer for data analysis ( koko spirometer , ferraris respiratory , louisville , co , us )  . 
each time , fev1 values were recorded as the highest of three readings made at 1min intervals . ct and airway analysis all patients underwent thin - section ct examination of the entire thorax using a 16 - slice scanner ( sensation 16 - siemens medical solutions , foreheim , germany ) without i.v. 
injection of contrast mediuthe scanning parameters were : 120 kvp , 100 mas , rotation time 0.5 s , feed / rotation 18 mm , the smallest possible field of view ( fov ) covering both lungs , bone filter , collimation 0.75 mm with 1 - mm reconstruction . 
ai sette pazienti affetti da asma cronico ( 2 maschi , range det : 3669 anni ) era stata fatta diagnosi di asma , in accordo con i criteri della american thoracic society [ 5 ] , da almeno 5 anni ed essi non avevano presentato riesacerbazioni nei tre mesi antecedenti . 
anche i pazienti hanno rilasciato il loro consenso informato allo studio . spirometria la spirometria stata effettuata mediante un respiratore connesso ad un computer per lanalisi dei dati ( koko spirometer , ferraris respiratory , louisville , usa )  . 
sono stati misurati i valori di base del fev1 e dopo 15 minuti di inalazione di 200 g di oxitropio bromuro . ogni volta , i valori di fev1 sono stati registrati come il pi alto valore delle tre letture fatte ad intervalli di un minuto . 
 tc del torace e protocollo di studio tutti i pazienti sono stati sottoposti a scansioni del torace con tc a strato sottile mediante tc multidetettore a 16 strati ( sensation 16 - siemens medical solution , foreheim , germania ) senza somministrazione ev di mezzo di contrasto . 
i parametri di scansione sono stati : 120 kvp , 100 mas , tempo di rotazione di 0 , 5 s , feed / rotation pari a 18 mm , il pi piccolo campo di vista possibile ( fov ) in grado di coprire entrambi i polmoni , un filtro per losso , una collimazione pari a 0 , 75 mm con ricostruzioni di 1 mm . dopo alcuni respiri in condizioni di stabilit , i soggetti sono stati chiamati ad effettuare una inspirazione massimale seguita immediatamente dallespirazione . 
2a - c le scansioni tc dimostrano la tecnica di misurazione del diametro bronchiale del bronco segmentale apicale del lobo superiore destro nei soggetti sani a riposo ( a ) , dopo cpap con 6 cmh2o ( b ) e dopo cpap con 12 cmh2o ( c ) , prima della somministrazione di oxitropio bromuro . ated all ct scans , measuring both internal and external diameters of the apical bronchus of the right upper lobe . 
questi dati sono stati utilizzati per calcolare laccordo interosservatore . la media dei valori misurati dai due osservatori stata considerata come valore di riferimento finale delle misurazioni . analisi statistica i valori sono stati rappresentati come mediadeviazione standard ( sd )  . 
le differenze fra i dati di base e i dati post - inradiol med ( 2008 ) 113 : 4355 table 1 characteristics of asthmatic subjects and healthy nonsmoking volunteers asthmatic subjects ( n = 7 ) healthy subjects ( n = 6 ) tervento sono state esaminate attraverso lanalisi della varianza e il test di comparazione multipla di dunnett . 
stato considerato significativo un valore di p < 0 , 05 . age ( years ) gender ( f / m ) disease duration ( years ) fev1 ( % predicted ) fev1 / fvc ( % ) 4711 6718 * 6710 * 378 11115 1045 risultati fev1 , forced expiratory volume in the first second ; fvc , forced vital capacity . 
values are expressed as meanstandard deviation ; * p < 0.05 tabella 1 caratteristiche dei soggetti asmatici e dei volontari sani non fumatori pazienti asmatici ( n = 7 ) soggetti sani ( n = 6 ) et ( anni ) sesso ( f / m ) durata malattia ( anni ) fev1 ( %vp ) fev1 / fvc ( % ) 4711 6718 * 6710 * 378 11115 1045 fev1 , volume di aria espirata nel primo secondo ; fvc , capacit vitale forzata . 
i valori sono stati espressi come mediasd ; * p < 0 , 05 the baseline fev1 and fev1 / forced vital capacity ( fvc ) among the two groups , as expected from our stratification ( table 1 )  . 
after administration of the bronchodilator , we found a significant difference in the change of both baseline fev1 and fev1 / fvc in asthmatic patients only ( p < 0.05 , table 2 )  . le caratteristiche dei soggetti sono mostrate in tabella 1 . 
dopo la somministrazione del broncodilatatore , abbiamo riscontrato un cambiamento significativo dei valori basali di fev1 e fev1 / fvc solo nei soggetti asmatici ( p < 0 , 05 , tabella 2 )  . laccordo interosservatore nelle misurazioni ct stato buono sia per il diametro interno ( ri = 0 , 67 ) che per quello esterno ( ri = 0 , 75 )  . 
la somministrazione di una pressione di 12 cmh2o ha modificato significativamente entrambi i diametri bronchiali nei pazienti asmatici , mentre nei controlli sani cambiato in modo significativo solo il diametro interno ( tabella 3 )  . 
we show that only administration of 12 cmh2o pressure modified airway diameters in asthmatic patients , but positive pressures did not further modify airway diameters after the addition of the bronchodilator . 
by contrast , in healthy subjects , administration of both 6 cmh2o and 12 cmh2o positive pressure , with and without oxitropium bromide inhalation , significantly changed airway diameters ( tables 4 and 5 )  . 
usando questo metodo innovativo , essenzialmente basato sullinsufflazione nasale a pressione positiva continua , abbiamo rilevato che la distensibilit delle vie aeree nei pazienti con asma cronico risultata diversa se paragonata con quella dei soggetti sani . 
abbiamo mostrato che nei pazienti asmatici solo la somministrazione di una pressione di 12 cmh2o ha modificato il calibro delle vie aeree , ma le pressioni positive non hanno modificato i diametri delle vie aeree dopo laggiunta del broncodilatatore . 
al contrario , nei soggetti sani sia la somministrazione di una pressione di 6 cmh2o sia di 12 cmh2o , con e senza linalazione di oxitropio bromuro , ha modificato significativamente i diametri delle vie aeree ( tabella 4 e 5 )  . 
questi reperti indicavano che le vie aeree dei pazienti con asma cronica erano risultate pi rigide di quelle dei soggetti sani . esistono diversi cambiamenti strutturali , tutti inclusi nel termine di rimodellamento delle vie aeree . 
lispessimento della membrana basale reticolare , lipertrofia del muscolo liscio e la fibrosi sub - epiteliale sono i markers probabilmente pi utili e rilevanti [ 6 , 7 ]  . 
6 valori individuali e valore medio del lume bronchiale del bronco segmentale apicale del lobo superiore destro a riposo e dopo insufflazione di una pressione di 6 cmh2o e di 12 cmh2o nei pazienti asmatici . post 6 cmh2o post 12 cmh2o after oxitropium post 6 cmh2o post 12 cmh2o p < 0.01 condizioni basali post 6 cmh2o post 12 cmh2o dopo oxitropio post 6 cmh2o post 12 cmh2o radiol med ( 2008 ) 113 : 4355 table 4 values of external and lumen diameters at baseline and after oxitropium bromide in asthmatic subjects pre and post 6 and 12 cmh2o pressure insufflation study population baseline after oxitropium external diameter lumen diameter external diameter lumen diameter gender pre post 6 post 12 post 6 post 12 post 6 post 12 post 6 post 12 asthmatic subjects mean standard deviation soggetti asmatici pz 1 pz 2 pz 3 pz 4 pz 5 pz 6 pz 7 media tabella 4 valori del diametro esterno e del diametro interno in condizioni basali e dopo oxitropio bromuro nei soggetti asmatici pree post - insufflazione a pressione positiva con 6 e 12 cmh2o studio sulla popolazione condizioni basali dopo oxitropio diametro esterno diametro interno diametro esterno diametro interno sesso post 6 post 12 post 6 post 12 post 6 post 12 post 6 post 12 a number of structural changes are grouped together under the umbrella term airway remodelling . 
it has been demonstrated in dogs that even relatively high levels of positive end - expiratory pressures cannot always prevent airway closure when there is sufficient stimulation of the airway smooth muscle [ 9 ]  . 
stato dimostrato che , anche nei cani , livelli relativamente alti di pressioni positive di fine espirazione non possono sempre prevenire la chiusura delle vie aeree in presenza di una sufficiente stimolazione della muscolatura liscia delle vie aeree [ 9 ]  . 
inducendo il rilassamento della muscolatura liscia ( mediante un broncodilatatore anti - colinergico , come loxitropio bromuro ) , abbiamo riscontrato che la somministrazione di pressioni positive non incrementa ulteriormente la dilatazione bronchiale nei soggetti asmatici in paragone con i controlli . 
kasahara and colleagues reported a significant negative correlation between postbronchodilator fev1 and both bronchial - wall thickening on hrct and reticular basement membrane thickness in endobronchial biopsy [ 10 ]  . 
however , other cross - sectional studies failed to demonstrate an association between fev1 and either bronchial - wall thickening or reticular basement membrane thickness [ 4 , 11 , 12 ]  . airway diameters measured on axial images depend on the lung volume and angle between the airway central axis and the plane of section [ 13 ]  . 
 [ 10 ] hanno riportato una significativa correlazione negativa fra i valori di fev1 dopo broncodilatatore , lispessimento della parete bronchiale alla hrct e lispessimento della membrana basale reticolare alla biopsia endobronchiale . 
comunque altri studi trasversali non sono stati in grado di dimostrare unassociazione fra fev1 , lispessimento della parete bronchiale e lo spessore della membrana basale reticolare [ 4 , 11 , 12 ]  . 
 i diametri delle vie aeree misurati sul piano assiale dipendono dal volume polmonare e dallangolo compreso fra lasse centrale della via aerea ed il piano di sezione [ 13 ]  . abbiamo estratto le misure dei diametri da quelle del tronco del bronco apicale del lobo superiore destro , il quale viene di solito sezionato nelle scansioni assiali ed facilmente identificato alla tc . 
il mantenimento di un volume polmonare relativamente costante fra le scansioni hrct un aspetradiol med ( 2008 ) 113 : 4355 surements from the trunk of the apical bronchus of the right upper lobe , which is usually sliced in cross - section and easily identified on ct scans . 
most recent software may overcome some limitations related to the use of two - dimensional planar data for airway analysis , as it can depict a three - dimensional airway skeleton and measure airway luminal and wall areas very precisely at any site in the lungs [ 14 , 15 ]  . 
therefore , we hope that future studies with more advanced techniques can verify our results . however , this study is the first to provide a dynamic measure of the airways obtained by ncpap . 
this is a new method that may have important clinical implications , as hrct might be used to measure dynamic changes in airway diameter in vivo that may be not detectable by conventional global lung measurements . 
anche se non abbiamo fatto uso di una regolare sincronizzazione respiratoria , il monitoraggio delle curve flusso - volume ci ha permesso di ottenere questo risultato con una buona affidabilit . 
la potenziale variabilit interosservatore nella misurazione dei diametri bronchiali mediante calibri elettronici ha portato allo sviluppo di metodi computerizzati per determinare le dimensioni della parete delle vie aeree . anche se abbiamo garantito un adeguato livello di concordanza fra gli osservatori nellanalisi semiquantitativa , lutilizzo di dati planari bidimensionali per lanalisi delle vie aeree presenta tuttavia alcuni limiti . 
molti softwares pi recenti possono superare qualche limite legato alluso di dati planari bidimensionali , dal momento che sono in grado di rappresentare uno scheletro tridimensionale delle vie aeree e misurarne larea endoluminale e larea di parete in maniera molto precisa e a qualsiasi livello dei polmoni [ 14 , 15 ]  . 
dunque , ci auguriamo che ulteriori indagini con tecniche pi avanzate possano verificare i nostri risultati . questo studio comunque il primo a fornire dati sulla misurazione dinamica delle vie aeree , ottenuta attraverso linsufflazione nasale a pressione continua . 
il metodo innovativo e pu avere importanti implicazioni cliniche , visto che la hrct pu essere utilizzata per misurare cambiamenti dinamici del calibro in vivo , che non possono essere individuati attraverso misurazioni convenzionali globali del polmone . 
scuro 10 , 37134 verona , italy 2istituto di radiologia , universit la sapienza , roma 3istituto di radiologia , casa di cura pederzoli di peschiera , verona , italy 4istituto di radiologia , ospedale maggiore , lodi , italy correspondence to : m . 
donofrio , tel : + 39 - 045 - 582445 , fax : + 39 - 045 - 8277808 , e - mail : mirko.donofrio@univr.it received : 31 january 2007 / accepted : 9 march 2007 / published online : 25 february 2008 springer - verlag 2008 abstract purpose . 
lesions were single in 18 / 23 cases ( 78% ) , single with nearby satellite lesions in 1 / 23 ( 4% ) cases and multifocal with distant secondary lesions in 4 / 23 ( 17% ) cases . 
ct showed that the lesions were hypovascular in the arterial phase in 15 / 23 cases ( 66% ) and hypervascular in 7 / 23 ( 30% ) cases ; one lesion ( 1 / 23 ; 4% ) was isovascular . 
analisi retrospettiva di 23 casi di colangiocarcinoma periferico istologicamente accertati . tutte le lesioni sono state studiate con ceus utilizzando microbolle a base di esaflururo di zolfo ricoperte da una capsula di fosfolipidi quale mezzo di contrasto e con tc dinamica . 
in 18 / 23 ( 78% ) la lesione era singola , in 1 / 23 ( 4% ) singola con lesioni satelliti a ridosso della lesione principale e in 4 / 23 ( 17% ) multifocale con lesioni a distanza rispetto alla lesione prinicipale . 
la ceus ha evidenziato ipervascolarizzazione delle lesioni in 16 / 23 ( 70% )  . ventidue su 23 lesioni ( 96% ) in fase tardiva ceus , sono risultate marcatamente ipoecogene . 
la tc ha evidenziato ipovascolarizzazione delle lesioni in fase arteriosa in 15 / 23 ( 66% ) ed ipervascolarizzazione in 7 / 23 ( 30% ) ; una lesione ( 1 / 23 ; 4% ) era isovascolarizzata . 
in fase tardiva tc la lesione era iperdensa in 17 / 23 ( 74% ) casi , ipodensa in 5 / 23 ( 22% ) e isodensa in 1 / 23 ( 43% ) casi . radiol med ( 2008 ) 113 : 7686 ( hyperdensity ) is common semiological findings in the study of ipcc . keywords biliary ducts cholangiocarcinoma ultrasound microbubbles multislice ct conclusioni . 
il riscontro di una discordanza di enhancement in fase tardiva tra ceus ( ipoecogenicit ) e tc ( iperdensit ) rappresenta frequente rilievo semeiologico nello studio del colangiocarcinoma intraepatico periferico . parole chiave vie biliari colangiocarcinoma ecografia microbolle tc multistrato introduction introduzione intrahepatic peripheral cholangiocarcinoma ( ipcc ) is a rare malignancy , accounting for 20%25% of all cholangiocarcinomas [ 13 ]  . 
it has been reported that the enhancement pattern of ipcc on delayed - phase computed tomography ( ct ) is of significant diagnostic value [ 912 ] ; lesion characterisation on ct may nonetheless remain indefinite . sonographic contrast microbubbles based on sulfur hexafluoride covered by a phospholipid shell ( sonovue , bracco , milan , italy ) have a mean diameter of 2.5 m and exhibit a strong harmonic response when insonated at low harmonic power ( mechanical index < 0.2 ; kpa < 50 )  . 
however , few studies have specifically focused on ipcc with ceus [ 20 ]  . the purpose of this paper is to compare ceus and dynamic ct in the evaluation of the perfusion patterns of ipcc with the aim of determining the diagnostic accuracy of the two techniques in combination for characterising these lesions . il colangiocarcinoma intra - epatico periferico ( ipcc ) un tumore raro rappresentando il 20%25% di tutti i colangiocarcinomi [ 13 ]  . 
 le microbolle di mezzo di contrasto ecografico a base di esaflururo di zolfo ricoperte da una capsula di fosfolipidi ( sonovue , bracco , milano , italia ) hanno diametro medio 2 , 5 m e si caratterizzano per lintensa risposta armonica allinsonazione armonica a bassa potenza ( mechanical index < 0 , 2 ; kpa < 50 )  . 
lecografia con mezzo di contrasto ( contrast - enanhced ultrasonography , ceus ) metodica accurata nella caratterizzazione delle lesioni focali epatiche come documentato da numerosi contributi [ 1319 ]  . 
tuttavia le segnalazioni di studi specificatamente dedicati al colangiocarcinoma intra - epatico periferico con ceus sono ancora piuttosto limitate [ 20 ]  . lo scopo di questo lavoro confrontare ceus e tc dinamica nella valutazione delle caratteristiche perfusionali del colangiocarcinoma periferico con lintento di calcolare laccuratezza diagnostica dellassociazione delle due indagini ai fini di una caratterizzazione lesionale . materials and methods patients materiali e metodi pazienti we retrospectively reviewed 23 cases of histologically proven ipcc obtained from the radiology - pathology archives of three institutions . 
all patients ( 13 men and 10 women ; age range 4982 years ; mean age 65 years ) had been studied with ceus and ct between 2004 and 2005 . dallarchivio radio - patologico di tre istituti abbiamo valutato retrospettivamente 23 pazienti affetti da ipcc ( 13 uomini e 10 donne ; range et 4982 anni ; et media , 65 anni ) , diagnosticati istologicamente e studiati con ceus e tc tra il 2004 e 2005 . 
 imaging methods metodiche di imaging radiol med ( 2008 ) 113 : 7686 contrast - enhanced ultrasonography ecografia con mezzo di contrasto conventional ultrasonography ( us ) and ceus were performed by the same operator . 
ceus studies were conducted using a second - generation sonographic contrast agent 2.4 ml of sulfur hexafluoride microbubbles ( sonovue , bracco , milan , italy ) injected as a rapid bolus via an antecubital vein , followed by 5 ml of saline solution . 
microbubble - specific harmonic imaging with insonation power was performed using a sequoia 512 unit ( coherent contrast imaging ; acuson , siemens , erlangen , germany ) and a vx aplio device ( vascular recognition imaging ; toshiba , osaka , japan )  . 
the use of two different sonographic machines for the study of lesion perfusion was related to the multicentric nature of the study , with cases being collected from different centres and hence studied with different sonographic equipment . 
no preset delay time after contrast injection was used to determine postcontrast phases because insonation of the liver lesion was constant , with dynamic observation of the transition between the preand postcontrast phases . 
after injecting 120140 ml of a nonionic contrast agent ultravist 370 ( schering , berlin , germany ) through an antecubital vein at a 3to 4 - ml / s flow rate , the ct images were acquired with a delay time after contrast injection set at 2530 s for the arterial phase , at 6070 s for the venous phase and at > 23 min for the delayed interstitial phase . 
scan parameters for all phases were the following : collimation 5 mm ; table feed / rotation 7.5 / 12 mm ; reconstruction interval 5 / 3 mall ct examinations were carried out within 1 week of ceus . image analysis recorded ceus and ct images were independently reviewed by two radiologists with experience in liver imaging ; cases of disagreement were solved by consensus . 
limaging armonico specifico per microbolle con potenza di insonazione stato effettuato su un apparecchio sequoia 512 ( coherent contrast imaging ; acuson , siemens , enlargen , germania ) e su un apparecchio vx aplio ( vascular recognition imaging ; toshiba , osaka , giappone )  . 
la presenza di due differenti equipaggiamenti ecografici per lo studio perfusionale della lesione legato alla multicentricit dello studio con raccolta della casistica in differenti centri con quindi differenti apparecchiature ecografiche . 
non si utilizzato alcun ritardo dalliniezione del mezzo di contrasto per definire le fasi contrastografiche in quanto linsonazione della lesione epatica stata continua attraverso losservazione dinamica del passaggio dalla fase precontrastografica alle fasi contrastografiche . 
la fase tardiva , caratterizzata dal progressivo accumulo delle microbolle nei sinusoidi , stata invece definita a partire da 120 s dopo liniezione e durante questa fase tutte le lesioni sono state monitorate per almeno cinque minuti . tc con mezzo di contrasto lesame tc stato realizzato con macchina somatom plus 4 e somatom sensation 16 ( siemens ag ; erlangen , germania )  . 
dopo iniezione ( 120140 ml ) di mezzo di contrasto non ionico , ultravist 370 ( schering , berlino , germania ) , attraverso una vena antecubitale a velocit di flusso di 34 ml / s , sono state acquisite immagini tc con un ritardo dalliniezione del mezzo di contrasto fissato a 2530 s per la fase arteriosa , 6070 s per la fase venosa e > 23 minuti per la fase tardiva interstiziale . 
lesion enhancement in the arterial and delayed phases was assessed as absent ( poor enhancement ) or present ( homogeneous / inhomogeneous enhancement )  . data analysis results the frequency of the perfusion patterns in the postcontrast phases of ceus and dynamic ct was calculated . analisi dei dati on both ceus and ct , in 18 / 23 cases ( 78% ) the lesion was single , in 1 / 23 cases ( 4% ) it was single with satellite lesions surrounding the main lesion within the same liver segment and in 4 / 23 cases ( 17% ) lesions were multifocal with additional lesions at a distance from the main lesion within both hepatic lobes . 
of these , 15 / 22 ( 68% ) appeared hypervascular , 3 / 22 ( 14% ) hypovascular , and 4 / 22 ( 18% ) isovascular in the arterial phase . 
of the 17 hyperdense lesions , 11 / 17 ( 65% ) appeared hypodense , 5 / 17 ( 29% ) hyperdense and 1 / 17 ( 6% ) isodense in the arterial phase . 
stata valutato laspetto della lesione in fase arteriosa , venosa e tardiva , definendo la lesione come ipervascolare ( iperecogena / iperdensa ) , isovascolare ( isoecogena / isodensa ) o ipovascolare ( ipoecogena / ipodensa ) rispetto al parenchima epatico adiacente . 
durante la fase arteriosa e tardiva lenhancement della lesione stata giudicata se assente ( enhancement scarso ) o presente ( enhancement omogeneo / disomogeneo )  . stata calcolata la frequenza degli aspetti perfusionali nelle fasi contrastografiche in ecografia con mezzo di contrasto e tc dinamica . risultati sono state riscontrate 18 / 23 lesioni singole ( 78% ) , 1 / 23 ( 4% ) lesione singola con lesioni satelliti , a ridosso della lesione principale nel contesto del medesimo segmento epatico , sia allesame ecografico che tc e 4 / 23 ( 17% ) lesioni multifocali , con lesioni aggiuntive a distanza rispetto alla lesione principale nel contesto di entrambi i lobi epatici , ad entrambe le metodiche . 
di queste 15 / 22 ( 68% ) in fase arteriosa erano apparse ipervascolarizzate , 3 / 22 ( 14% ) ipovascolarizzate e 4 / 22 ( 18% ) isovascolarizzate . 
una sola lesione ( 1 / 23 ; 4% ) , ipervascolarizzata in fase arteriosa , risultata isoecogena in fase tardiva . alle scansioni tc pre - contrastografiche tutte le lesioni a parte una erano omogeneamente ipodense . 
in one case only ( 1 / 23 ; 43% ) did a hypervascular lesion in the arterial phase become isodense in the delayed phase . ceus and ct comparison between the two modalities showed that in the arterial phase , in 9 / 23 cases ( 39% ) , the lesion was hyperechoic on ceus and hypodense on ct ; in 7 / 23 cases ( 31% ) , the lesion appeared hyperechoic and hyperdense in the arterial phase on ceus and ct , respectively ; in 4 / 23 cases ( 17% ) , the lesions appeared isoechoic on ceus , whereas on ct 3 / 4 were hypodense and 1 / 4 was isodense ; finally , 3 / 23 lesions ( 13% ) appeared hypoechoic on ceus and hypodense on ct . 
 thus in the arterial phase , ceus and ct demonstrated a similar perfusion pattern in 11 / 23 cases ( 48% ) , showing insione ( 1 / 23 ; 4% ) era isodensa in fase arteriosa . 
per quanto riguarda le 17 lesioni apparse iperdense , 11 / 17 ( 65% ) si erano presentate ipodense , 5 / 17 ( 29% ) iperdense , 1 / 17 ( 6% ) isodensa in fase arteriosa . 
in un solo caso ( 1 / 23 ; 43% ) la lesione ipervascolarizzata in fase arteriosa poi divenuta isodensa in fase tardiva . ceus e tc dal confronto tra le due metodiche emerso quanto segue . in fase arteriosa in 9 / 23 ( 39% ) casi la lesione era iperecogena allesame ceus mentre era ipodensa allindagine tc ; in 7 / 23 ( 31% ) casi la lesione si presentava iperecogena ed iperdensa in fase arteriosa rispettivamente allindagine ceus e tc ; in 4 / 23 ( 17% ) casi la lesione appariva isoecogena allesame ceus mentre , allesame tc , 3 / 4 erano ipodense e 1 / 4 era isodensa ; infine 3 / 23 ( 13% ) lesioni erano ipoecogene allesame ceus ed ipodense allesame tc . 
 quindi in fase arteriosa gli esami ceus e tc hanno mostrato comportamento perfusionale analogo in 11 / 23 ( 48% ) casi , dimostrando unaumentata captazione di contrasto in relazione alla ipervascolarizzazione della lesione in 7 / 11 ( 64% ) casi , unipovascolarizzazione in 3 / 11 ( 27% ) ed isovascolarizzazione in 1 / 11 ( 9% )  . 
in 12 / 23 ( 52% ) casi si assistitito ad una discordanza tra le caratteristiche perfusionali tc e ceus con 9 / 12 ( 75% ) lesioni ipervascolarizzate allindagine ecografica ed ipovascolarizzate allesame tc mentre 3 / 12 ( 25% ) lesioni erano isovascolarizzate ed ipodense rispettivamente allindagine ceus e tc . in fase venosa tutte le lesioni a parte una ( 22 / 23 ; 96% ) sono risultate ipoecogene allesame ceus ed apparivano ipodense in 14 / 22 ( 64% ) ed isodensa in 8 / 22 ( 36% ) casi . 
in particolare il 73% ( 16 / 22 ) delle lesioni che in fase tardiva erano ipoecogene allindagine ecografica si presentavano invece iperdense allindagine tc . radiol med ( 2008 ) 113 : 7686 creased contrast uptake due to lesion hypervascularity in 7 / 11 cases ( 64% ) , hypovascularity in 3 / 11 ( 27% ) and isovascularity in 1 / 11 ( 9% )  . 
in 12 / 23 cases ( 52% ) , there was discordance between ct and ceus perfusion patterns , with 9 / 12 ( 75% ) lesions appearing hypervascular on ceus and hypovascular on ct and 3 / 12 ( 25% ) appearing isovascular on ceus and hypodense on ct . in the venous phase , all lesions but one ( 22 / 23 ; 96% ) were hypoechoic on ceus and appeared hypodense in 14 / 22 cases ( 64% ) and isodense in 8 / 22 cases ( 36% )  . 
one isoechoic lesion ( 1 / 23 ; 4% ) was hyperdense on venous - phase ct . in the delayed phase , all lesions but one ( 22 / 23 ; 96% ) were hypoechoic on ceus ; they appeared hyperdense on discussione il colangiocarcinoma intra - epatico un adenocarcinoma ben differenziato in circa il 95% dei casi [ 5 , 19 ]  . 
nello studio mediante imaging di questo tumore stato raccomandato limpiego della classificazione morfologica dei colangiocarcinomi proposta dal liver cancer study group of japan [ 21 ] basata sulle caratteristiche di crescita identificando tre tipi di tumore , formante - massa , periduttale - infiltrante ed intraduttale , facilitando in questo modo la correlazione tra reperti radiologici e patologici e consentendo di ottenere un planning terapeutico chirurgico ottimale [ 2 , 20 , 21 ]  . 
b , c on contrast - enhanced ultrasound , the lesion shows inhomogeneous enhancement in the arterial phase ( arrows in b ) , becoming markedly hypoechoic in the sinusoidal phase ( caliper in c )  . 
b , c allecografia con mezzo di contrasto ( ceus ) la lesione dimostra impregnazione disomogenea in fase arteriosa ( frecce in b ) divenendo quindi marcatamente ipoecogena in fase post - contrastografica sinusoidale ( caliper in c )  . 
d , e allesame tc la lesione risulta prevalentemente ipodensa in fase arteriosa ( frecce in d ) quindi nettamente iperdensa in fase post - contrastografica tardiva ( frecce in e )  . radiol med ( 2008 ) 113 : 7686 fig . 
b on computed tomography ( ct ) , a large ipcc ( asterisk ) is seen , marked by inhomogeneous enhancement in the arterial phase , occupying the lateral portions of the right hepatic lobe ( vi segment )  . 
b allesame tc si riconosce voluminoso ipcc ( asterisco ) , con disomogenea impregnazione in fase arteriosa , che occupa i settori laterali del lobo epatico di destra ( vi segmento )  . 
 lecografia rappresenta la prima indagine nelliter radiol med ( 2008 ) 113 : 7686 were hypoechoic on delayed - phase ceus appeared hyperdense on ct . discussion ipcc is a well - differentiated adenocarcinoma in approximately 95% of cases [ 5 , 19 ]  . 
based on growth patterns , this classification identifies three types of tumour mass forming , periductal infiltrating , and intraductal growing facilitating the correlation between radiological and pathological findings and optimising surgical planning [ 2 , 20 , 21 ]  . 
 us is the first - line diagnostic modality for suspected obstruction of the intrahepatic bile ducts , as association with a biliary malignancy can only be hypothesised after ruling out the presence of gallstones [ 2 , 5 ]  . 
however , final diagnosis remains difficult to establish in many cases , especially when an ipcc ( growing within the bile duct ) needs to be differentiated from some forms of hypovascular metastases of the gastrointestinal tract [ 2325 ]  . 
to achieve a final diagnosis , fine - needle aspiration with or without image - guided core biopsy is required , which allows the exclusion of liver metastases , hepatocellular carcinoma or rare cases of advanced intraductal intrahepatic cholangiocarcinoma [ 26 ]  . 
guidelines on the diagnosis and treatment of cholangiocarcinomas do not recommend the use of percutaneous or open biopsy in resectable cases due to the risk of tumour seeding , even though a large proportion are diagnosed when surgery is no longer a viable option [ 23 ]  . as a consequence , ipcc characterisation , though difficult on imaging , is fundamental for ensuring correct treatment . on unenhanced ct , ipcc has been described as a homogeneously hypodense mass with irregular margins [ 27 ]  . 
on dynamic ct , both in the arterial and venous phases , it appears prevalently hypodense with a thin and incomplete rim of peripheral enhancement and progressive centripetal filling in the subsequent phases , in contrast to the pattern seen in angiomas [ 11 , 27 ]  . 
less frequently reported features include peripheral enhancement in the form of a thick , continuous rim in both phases or a homogeneous hyperenhancing area in the diagnostico in caso di una sospetta ostruzione alle vie biliari intraepatiche che si pu ipotizzare associata ad un tumore delle vie biliari solo dopo aver escluso la presenza di calcoli [ 2 , 5 ]  . 
la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm ) sono metodiche comunemente utilizzate per identificare e stadiare i colangiocarcinomi [ 3 , 11 , 23 , 24 ]  . 
una diagnosi definitiva , in ogni caso , ancora difficile da raggiungere in molti casi , soprattutto nella distinzione tra un icpp ( che cresce allinterno del dotto biliare ) ed alcuni tipi di metastasi ipovascolarizzate del tratto gastroenterico [ 2325 ]  . 
per giungere alla diagnosi definitiva necessario lagoaspirato con ago sottile con o senza core - biopsy guidati da metodiche di imaging , permettendo di escludere metastasi epatiche o hcc o rari casi di colangiocarcinoma intraepatico intraduttale avanzato [ 26 ]  . 
nelle linee - guida sulla diagnosi e trattamento del colangiocarcinoma si sconsiglia di praticare una biopsia percutanea o aperta nei pazienti operabili per il rischio di disseminazione tumorale , anche se in unelevata percentuale di pazienti , al momento della diagnosi , non pi possibile un approccio chirurgico terapeutico [ 23 ]  . 
ne segue che la caratterizzazione dellipcc per quanto difficile allimaging di fondamentale importanza per assicurare il corretto iter terapeutico . in tc in fase precontrastografica , i colangiocarcinomi periferici sono stati descritti come una massa a margini irregolari , omogeneamente ipodensa [ 27 ]  . 
in tc dinamica , sia in fase arteriosa che venosa , stato riscontrato un aspetto della lesione prevalentemente ipodenso con impregnazione periferica ad anello sottile ed incompleto e progressivo riempimento centripeto nelle fasi successive , diverso da quello degli angiomi [ 11 , 27 ]  . 
in fase tardiva la lesione pu , quindi , presentare captazione di mezzo di contrasto diffusa o , pi spesso , prevalentemente centrale . questo aspetto piuttosto caratteristico dellipcc e consente di ipotizzare correttamente la natura della lesione [ 11 , 27 ]  . 
in letteratura sono state riscontrate con minor frequenza altre caratteristiche come unimpregnazione periferica ad anello spesso e continuo in entrambe le fasi od unarea omogenea ipercaptante in fase arteriosa che diventata ipodensa in fase portale con una parte periferica iperdensa [ 3 , 9 , 11 ]  . 
sono inoltre state osservate aree intratumorali ad elevata o bassa attenuazione in tutte le fasi , nel 14 , 2% fino al 97% delle lesioni a seconda dei lavori [ 11 , 27 ]  . 
stata comprovata da molti studi lutilit della fase tardiva in tc nellidentificazione del colangiocarcinoma dovuta alla sua componente di stroma fibroso che trattiene contrasto pi a lungo rispetto al parenchima epatico circostante , con aumento della captazione di contrasto [ 7 , 911 ]  . 
tuttavia la percentuale di ipcc iperdensi in fase tardiva abbastanza diversa variando dal 36% [ 28 ] al 70% [ 27 ] , 74% [ 9 ] , fino all81 , 8% [ 11 ]  . 
il motivo di questa differenza potrebbe essere correlato alle diverse dimenradiol med ( 2008 ) 113 : 7686 arterial phase that becomes hypodense in the portal phase with a hyperdense peripheral portion [ 3 , 9 , 11 ]  . 
intratumoural areas of high or low attenuation in all phases have also been observed , in 14.2%97% of lesions , depending on the series [ 11 , 27 ]  . 
many studies have demonstrated the usefulness of delayed - phase ct for the identification of cholangiocarcinoma due to the fibrous stroma retaining contrast material longer than the surrounding liver parenchyma , thus increasing enhancement [ 7 , 911 ]  . 
in our study , 17 / 23 ( 74% ) of ipcc appeared hyperdense on delayed - phase ct . the presence of fibrosis though not pathognomonic given the existence of nonscirrhous cholangiocarcinoma that accounts for lesion hyperdensity on delayed - phase ct and dilation of the intrahepatic biliary ducts are the main characteristics of peripheral cholangiocarcinoma [ 29 , 30 ]  . ceus has been shown to improve diagnostic confidence compared with baseline us for distinguishing between malignant and benign focal hepatic lesions and , in particular , for differentiating malignant and benign hypoechoic lesions with 95% diagnostic accuracy [ 13 , 15 , 31 , 32 ]  . 
only few reports in the literature have described the main ceus characteristics of peripheral cholangiocarcinomas , and only in studies investigating focal hepatic lesions in general [ 15 , 16 , 31 , 32 , 34 , 35 ]  . 
nicolau and bru reported that most peripheral cholangiocarcinomas are hypoechoic on ceus in the arterial phase , whereas lesion hyperechogenicity due to hypervascularity is seen in 30% of cases [ 31 ]  . 
in particular , whereas 22 / 23 lesions ( 96% ) were hypoechoic on ceus in the sinusoidal phase , 17 / 23 ( 74% ) were hyperdense on ct in the delayed phase . 
the former is intravascular , that is , it does not flow outside the vascular bed , whereas the latter is intra / extravascular , that is , it flows into the interstitium until it reaches a state of equilibrium [ 32 , 35 ]  . 
it follows that in the later phases of postcontrast studies , the fibrous component due to desmoplastic reaction will appear nonenhancing ( hypoechoic ) on ultrasound and enhancing ( hyperdense ) on ct . ceus alone provides limited information for the characterisation of ipcc because , as previously observed , it is unable to distinguish it from other malignant focal hepatic lesions ( metastases )  . 
la presenza di fibrosi , sebbene non patognomonica ( visto lesistenza del colangiocarcinoma non scirroso ) , che rende ragione delliperdensit in fase tc tardiva , e la dilatazione delle vie biliari intraepatiche rimangono le caratteristiche principali del colangiocarcinoma periferico [ 29 , 30 ]  . lo studio ceus stato dimostrato migliorare la confidenza diagnostica rispetto allecografia basale , ai fini della distinzione tra lesioni focali epatiche maligne e benigne ed in particolare nel differenziare le lesioni ipoecogene maligne dalle benigne con unaccuratezza diagnostica del 95% [ 13 , 15 , 31 , 32 ]  . 
in letteratura poche segnalazioni riportano le principali caratteristiche dei colangiocarcinomi periferici con ceus peraltro allinterno di lavori dedicati allo studio delle lesioni focali epatiche in generale [ 15 , 16 , 31 , 32 , 34 , 35 ]  . 
nicolau e bru hanno riportato che la maggior parte dei colangiocarcinomi periferici sono ipoecogeni in fase arteriosa con ceus mentre una iperecogenicit della lesione da ipervascolarizzazione presente nel 30% dei casi [ 31 ]  . 
questa discordanza pu essere spiegata dalla conoscenza della diversa distribuzione tra il mezzo di contrasto impiegato in ecografia ed in tc , essendo il primo intra - vascolare , cio che non fuoriesce dal letto vascolare , ed il secondo intra - / extra - vascolare , cio in grado di diffondere nello spazio interstiziale fino al raggiungimento della fase di equilibrio [ 32 , 35 ]  . 
ne segue che nelle fasi avanzate delle indagini contrastografiche , la componente fibrosa da reazione desmoplastica del ipcc risulter priva di mezzo di contrasto ( ipoecogena ) in ecografia ed impregnata di mezzo di contrasto ( iperdensa ) in tc . 
lecografia con mezzo di contrasto presa singolarmente ha scarso potere informativo ai fini della caratterizzazione del colangiocarcinoma periferico del fegato in quanto come osservato non consente di distinguerlo dalle altre lesioni focali epatiche maligne ( metastasi )  . 
tuttavia lecografia con mezzo di contrasto in associazione alla tc dinamica pu contribuire alla caratterizzazione tissutale rafforzando lipotesi circa la diagnosi di natura . le limitazioni del presente studio risiedono nel numero contenuto di lesioni valutate e nellutilizzo di diverse apradiol med ( 2008 ) 113 : 7686 can help characterise the lesion by reinforcing the provisional diagnosis of the nature of the lesion . the limitations of this study lie in the small number of lesions studied and the fact that different imaging equipment was used because of its multicentric nature . 
to evaluate the influence of slice thickness , reconstruction algorithm and tube current ( ma ) on the performance of a software package in determining the volume of solid pulmonary nodules on multidetector - row computed tomography ( mdct )  . 
a chest phantom containing artificial solid nodules with known volume was imaged with two mdct scans at 100 and 40 mas ( 200 ma and 80 ma , 0.5 - s rotation time ) , respectively . 
mean values of the differences , which better approximated the real volume of the nodules , were obtained with high - spatial - resolution algorithms on both 100 and 40 mas images at 1.25 - mm slice thickness . 
the best performance of the software , on both 100 and 40 mas images , was observed with a slice thickness of 1.25 mm and high - spatial - resolution algorithms . 
valutare linfluenza di spessore di strato , algoritmo di ricostruzione e corrente del tubo ( ma ) sulla performance di un software nella volumetria dei noduli polmonari solidi in tc multidetettore ( tcmd )  . 
il torace di un fantoccio , contenente noduli solidi artificiali di volume noto , stato sottoposto a due scansioni tcmd , rispettivamente a 100 e 40 mas ( 200 ma e 80 ma , tempo di rotazione di 0 , 5 s )  . 
lo spessore di 1 , 25 mm e gli algoritmi ad alta risoluzione hanno consentito la migliore performance del software , sia a 100 che a 40 mas . keywords pulmonary nodule mdct 3d volumetry parole chiave nodulo polmonare tcmd volumetria 3d introduction multidetector computed tomography ( mdct ) is considered the most sensitive modality for detecting pulmonary nodules . multidetector technology has improved spatial resolution and image quality by enabling acquisition of the whole lung with thin collimation and extremely fast scanning times [ 1 ]  . 
however , it has resulted in the routine detection of an increasing number of pulmonary nodules smaller than 1 cm in diameter , which determinate a significant management challenge [ 2 ]  . 
 as is known [ 3 ] , solitary pulmonary nodules larger than 1 cm have a high likelihood of malignancy and therefore warrant further investigation [ dynamic ct and / or positron emission tomography ( pet ) - ct or percutaneous needle biopsy ] [ 2 ]  . 
nodules smaller than 1 cm are more frequently benign , but they are difficult to characterise because of their small size [ 4 , 5 ] and often cannot be studied by pet owing to the limited spatial resolution of pet scanners [ 1 ]  . in recent years , there has been growing interest in the possibility of characterising indeterminate solitary pulmonary nodules , above all those smaller than 1 cm in diameter , by follow - up imaging studies and assessment of nodule growth [ 6 ]  . 
growth of a pulmonary nodule is normally assessed on ct by measuring the axial diameters manually or with the aid of electronic calipers and determining doubling time , that is , the time it takes the lesion to double in volume . this corresponds to a 26% increase in nodule diameter [ 1 ]  . generally , doubling times between 30 and 500 days are considered suggestive of malignancy [ 7 ]  . 
 in clinical practice , however , the reliable detection of minimal but significant nodule growth with two - dimensional ( 2d ) methods is problematic , especially in the presence of small nodules with asymmetrical growth patterns [ 8 , 9 ]  . 
the limitations of 2d techniques have indicated a need to assess nodule growth on follow - up imaging by using three - dimensional ( 3d ) techniques for volume determination [ 6 ]  . 
 automated volume measurement may , however , be influenced by a number of factors , such as the patients position , level of inspiration and , above all , the technique used [ 7 ]  . 
the use of standardised technical protocols is fundamental for allowing adequate comparison between scans and improving the reliability and repeatability of automated volume measurements [ 7 , 11 ]  . 
automated volumetric systems generally rely on complex shape - analysis algorithms radiol med ( 2008 ) 113 : 2942 introduzione la tc multidetettore ( tcmd ) considerata la metodica pi sensibile nella identificazione dei noduli polmonari . 
la tecnologia multidetettore ha migliorato la risoluzione spaziale e la qualit delle immagini grazie alla possibilit di acquisire lintero polmone con collimazioni sottili e in tempi estremamente brevi [ 1 ]  . 
tuttavia , ha comportato il riscontro routinario di un numero crescente di noduli polmonari di dimensioni inferiori al centimetro , che pongono problematiche di gestione clinica [ 2 ]  . 
 come noto [ 3 ] , i noduli polmonari solitari con diametro maggiore di 1 cm hanno unelevata probabilit di essere maligni e sono destinati , pertanto , ad ulteriori approfondimenti diagnostici ( tc dinamica e / o pet - tc o ago - biopsia percutanea ) [ 2 ] ; i noduli con diametro inferiore a 1 cm risultano pi comunemente di natura benigna , ma difficili da caratterizzare per le piccole dimensioni [ 4 , 5 ] , e spesso non sono valutabili in pet per i limiti di risoluzione spaziale intrinseci alla metodica [ 1 ]  . negli ultimi anni cresciuto linteresse sulla possibilit di caratterizzare i noduli polmonari solitari indeterminati , soprattutto quelli di diametro inferiore a 1 cm , mediante il follow - up radiologico e lidentificazione delleventuale crescita dimensionale [ 6 ]  . 
laccrescimento dei noduli polmonari viene valutato comunemente in tomografia computerizzata ( tc ) misurando i diametri assiali , con metodo manuale o con caliper elettronico , e considerando il tempo di raddoppiamento , ovvero il tempo che la lesione impiega a raddoppiare il suo volume ; ci corrisponde ad un aumento del diametro del 26% [ 1 ]  . 
 nella pratica clinica , tuttavia , risulta difficoltoso rilevare in modo affidabile accrescimenti minimi ma significativi dei noduli con le misurazioni bidimensionali , soprattutto in presenza di noduli di piccole dimensioni e con crescita di tipo asimmetrico [ 8 , 9 ]  . 
i limiti delle tecniche bidimensionali hanno suggerito la necessit di ricorrere alla valutazione della crescita dei noduli sottoposti a follow - up mediante il calcolo del volume con metodo tridimensionale ( 3d ) [ 6 ]  . 
 [ 11 ] hanno dimostrato che il sistema automatico di calcolo 3d del volume con software dedicato ha una bassa variabilit intered intra - osservatore e una elevata ripetibilit nelle misurazioni . 
 [ 7 ] hanno anche dimostrato lutilit della volumetria tridimensionale nel distinguere le lesioni di natura benigna da quelle di natura maligna , sulla base del calcolo automatico del loro tempo di raddoppiamento . 
 le misurazioni volumetriche con metodo automatico , tutradiol med ( 2008 ) 113 : 2942 to separate the nodules from adjacent structures and determine their volume [ 11 ]  . 
even the environment surrounding the nodule air in the lung parenchyma or structures having similar density to the nodule ( pulmonary vessels , mediastinal structures , chest wall , diaphragm ) can affect the segmentation process [ 11 ]  . 
 several in vivo studies have assessed the effect of technical parameters , such as slice thickness and reconstruction interval , on the automatic detection of pulmonary nodules on ct [ 12 , 13 ]  . 
instead , one recent paper compared the performance of several automated volumetric systems at different doses , slice thicknesses and reconstruction kernels both in vivo and on a phantom , identifying the system with the best performance [ 14 ]  . 
use of an anthropomorphic phantom represents a useful method for testing technical parameters in artificial conditions and transferring the results into clinical practice [ 2 , 15 ]  . to our knowledge , no published report has analysed on a phantom the reciprocal effect of several technical parameters on the performance of an automated 3d system in the volumetry pulmonary nodules . 
the aims of our study were to evaluate the effect of slice thickness , reconstruction algorithm and tube current ( ma ) on the ability of a volumetric software , in use at our institution , to segment and calculate the volume of solid pulmonary nodules in an anthropomorphic phantom and to validate a study protocol for the follow - up of pulmonary nodules by mdct . 
di fondamentale importanza , infatti , limpiego di protocolli tecnici standardizzati al fine di consentire un adeguato confronto tra esami diversi e migliorare laffidabilit e la ripetibilit delle misurazioni volumetriche automatiche [ 7 , 11 ]  . 
anche lambiente circostante il nodulo , rappresentato dallaria contenuta nel parenchima polmonare o dalle strutture a densit simile a quella del nodulo ( vasi polmonari , strutture mediastiniche , parete toracica , diaframma ) , pu influenzare il processo di segmentazione [ 11 ]  . 
 in letteratura sono stati condotti alcuni studi in vivo che hanno valutato leffetto di parametri tecnici , quali spessore di strato ed intervallo di ricostruzione , sulla identificazione automatica dei noduli polmonari in tc [ 12 , 13 ]  . 
un recente studio ha , invece , confrontato la performance di sistemi automatici diversi nella volumetria 3d dei noduli , a differente dose , spessore di strato e kernel di ricostruzione , sia in vivo che su fantoccio , indicando il sistema con la migliore prestazione [ 14 ]  . 
limpiego di fantocci antropomorfi rappresenta un metodo per testare parametri tecnici in condizioni artificiali e trasferire poi i risultati ottenuti alla pratica clinica [ 2 , 15 ]  . a nostra conoscenza , non esistono segnalazioni in letteratura che abbiano analizzato su fantoccio linfluenza reciproca di pi parametri tecnici sulla performance di un sistema automatico 3d nella volumetria dei noduli polmonari . 
gli obiettivi del nostro studio sono stati : valutare leffetto dello spessore di strato , dellalgoritmo di ricostruzione e della corrente del tubo ( ma ) sulla capacit del software 3d , in dotazione nel nostro istituto , di segmentare e calcolare il volume di noduli polmonari solidi , utilizzando un fantoccio antropomorfo ; validare un protocollo di studio da applicare nel follow - up dei noduli polmonari in tcmd . 
i tre noduli avevano diametro e volumi noti : 17 mm e 2 , 804 cm3 il nodulo iuxtapleurico , 9 , 7 mm e 0 , 496 cm3 il nodulo iuxtavascolare , 10 mm e 0 , 520 cm3 il nodulo centroparenchimale ben circoscritto . tecnica di esame il torace del fantoccio stato sottoposto a due scansioni tcmd consecutive con apparecchio 16 strati ( lightspeed pro 16 ; ge healthcare )  . 
sono state condotte due acquisizioni dagli apici alle basi polmonari a diversa corrente del tubo radiogeno ( ma ) per un tempo di rotazione di 0 , 5 secondi ( mas ) , senza limpiego del sistema di modulazione dellamperaggio : la prima acquisizione a 100 mas ( 200 ma0 , 5 s ) e 120 kv ( protocollo standard ) e la seconda a 40 mas ( 80 ma0 , 5 s ) e 120 kv ( protocollo a bassa dose )  . 
il protocollo standard , rapportato ad un paziente normotipo di sesso maschile con peso corporeo inferiore a 80 kg , corrisponderebbe a una dose efficace ( e ) di circa 7 , 9 msv e quello a bassa dose di circa 3 , 2 msv . 
sono stati utilizzati i seguenti parametri tecnici : configurazione dei detettori o collimazione di 161 , 25 mm , velocit di spostamento 27 , 5 mm / s , pitch 1 , 375 : 1 , campo di vista ( field of view o fov ) 39 cm e matrice di acquisizione 512512 pixel . i dati ottenuti dalle due acquisizioni sono stati ricostruiti utilizzando due differenti spessori di strato ( 1 , 25 mm e 2 , 5 mm , con rispettivi intervalli di 1 , 25 e 2 , 5 mm ) e cinque diversi algoritmi di ricostruzione o kernel ( standard , lung , detail , bone e bone + ; ge healthcare ) , per un totale di 20 set di immagini assiali ( 2 valori di mas , 2 spessori di strato , 5 kernel di ricostruzione )  . analisi delle immagini le immagini state analizzate su una workstation ( adw 4.2 ; ge healthcare ) , impiegando un software 3d dedicato per la valutazione del nodulo polmonare ( advanced lung analysis 2 ; ge healthcare )  . 
two scans were obtained from the lung apex to the lung base at different tube currents per 0.5 - s rotation time ( mas ) , without tube - current modulation . 
the first scan was acquired at 100 mas ( 200 ma0.5 s ) and 120 kv ( standard protocol ) and the second at 40 mas ( 80 ma0.5 s ) and 120 kv ( low - dose protocol )  . 
2a - c i tre noduli ( frecce ) nel polmone del fantoccio ; a nodulo iuxtapleurico ; b nodulo iuxtavascolare ; c nodulo centroparenchimale ben circoscritto . image analysis images were analysed at a workstation ( adw 4.2 ; ge healthcare ) by using a dedicated volumetric software for the assessment of pulmonary nodules ( advanced lung analysis 2 ; ge healthcare )  . 
the volume of the three solid nodules was calculated on each of the reconstructions , with different slice thicknesses , reconstruction kernels and mas , for a total of 60 volumetric measurements . statistical analysis we calculated the differences between the volume measured by the 3d method in cubic centimetres ( cm3 ) and the real volume of the nodules ( cm3 )  . 
we reported the mean values and confidence intervals ( ci ) of the differences obtained for each nodule and for each reconstruction with different slice thickness , algorithm and mas , comparing them to one other . 
sono stati riportati i valori delle medie e degli intervalli di confidenza ( ic ) delle differenze ottenute per ciascun nodulo e ciascuna ricostruzione a differente spessore di strato , algoritmo e mas , confrontandoli tra loro . 
in tal modo stato possibile identificare lalgoritmo di ricostruzione che ha consentito il calcolo automatico del volume pi prossimo a quello reale al variare dello spessore di strato e della corrente del tubo . sono state poi confrontate tra loro ( test t di student ) le differenze tra il volume calcolato e quello reale ottenute per ciascun nodulo e ciascun algoritmo , rispettivamente a 100 e a 40 mas , sia nelle ricostruzioni a spessore di 1 , 25 mm che di 2 , 5 mm , al fine di valutare linfluenza dello spessore di strato sulla volumetria dei noduli al variare dellalgoritmo e della corrente del tubo . 
allo stesso modo sono state confrontate tra loro ( test t di student ) le differenze tra il volume calcolato e quello reale ottenute per ciascun nodulo e ciascun algoritmo , rispettivamente a spessore di 1 , 25 mm e di 2 , 5 mm , sia a 100 che a 40 mas , al fine di valutare linfluenza della corrente del tubo sulla volumetria radiol med ( 2008 ) 113 : 2942 ing algorithms and tube currents . 
 tables 2 and 3 show comparisons of the differences between calculated and real volumes ( ) for each nodule and algorithm at 100 and 40 mas ( table 2 ) and 1.25 - mm and 2.5 - mm slice thickness ( table 3 )  . 
similarly , no significant differences were found between 100 mas and 40 mas with 2.5 - mm slice thickness for the juxtavascular and intraparenchymal well - circumscribed nodule . regarding the juxtapleural nodule , we were unable to compare the differences calculated for all algorithms at 100 mas and 40 mas , because nodule segmentation was only achieved with the standard kernel at 2.5 mm and low tubecurrent settings ( 40 mas )  . 
instead , significant differences were identified nella tabella 1 sono riportati per ciascuno dei tre noduli i volumi reali e quelli calcolati automaticamente su ciascuna delle 20 ricostruzioni effettuate a differente spessore di strato , algoritmo e mas . 
con 40 mas e spessore di strato di 1 , 25 mm , lalgoritmo bone + ha consentito la misurazione pi precisa del volume dei tre noduli ( 0 , 230 , 44 )  . 
 nelle tabelle 2 e 3 sono riportati i confronti tra le differenze dei volumi calcolati da quelli reali ( ) per ciascun nodulo e ciascun algoritmo , effettuati tra le ricostruzioni a 100 e a 40 mas ( tabella 2 ) e tra quelle a spessore di 1 , 25 mm e 2 , 5 mm ( tabella 3 )  . 
le differenze riportate nella tabella 2 , a 100 mas e a 40 mas , non sono risultate statisticamente significative , nelle ricostruzioni con spessore di 1 , 25 mm . analogamente , non significative sono state le differenze tra 100 e 40 mas sulle ricostruzioni a spessore di 2 , 5 mm , per i noduli iuxtavascolare e centroparenchimale ben circoscritto . 
per il nodulo iuxtapleurico , non stato possibile confrontare le differenze calcolate con tutti gli algoritmi a 100 mas e a 40 mas , poich il nodulo stato segmentato a 2 , 5 mm e a basso amperaggio ( 40 mas ) soltanto utilizzando il kernel standard . 
con questo algoritmo , la misurazione a 40 mas stata meno precisa di quella a 100 mas , con differenze tra volume calcolato e reale ( ) rispettivamente di 0 , 375 e di 0 , 151 . 
 le differenze riportate nella tabella 3 , comparate tra spessore di strato di 1 , 25 e 2 , 5 mm , non sono risultate statisticamente significative a 100 mas . 
at low tube - current settings , volume measurements proved less accurate at 2.5 mm , with greater differences between calculated and real volumes in all algoscolare e centroparenchimale ben circoscritto . 
a basso amperaggio la misurazione dei volumi stata meno precisa a 2 , 5 mm , con differenze tra volume calcolato e volume reale maggiori per tutti gli algoritmi , ad eccezione del lung per il radiol med ( 2008 ) 113 : 2942 fig . 
3 confronto tra la performance del software utilizzando i kernel standard e bone nelle ricostruzioni a 100 mas con spessore di 1 , 25 mm ; il kernel bone meglio stima il volume reale del nodulo ( vr = 0 , 496 cm3 )  . 
4 confronto tra la performance del software utilizzando i kernel standard e bone nelle ricostruzioni a 100 mas con spessore di 2 , 5 mm ; il kernel standard meglio stima il volume reale del nodulo iuxtapleurico ( vr = 2 , 804 cm3 )  . 
anche in questo caso , non stato possibile confrontare le differenze calcolate per il nodulo iuxtapleurico a 40 mas con tutti gli algoritmi , ma soltanto con quello standard ; con questo algoritmo la misurazione del volume a basso amperaggio stata meno precisa a 1 , 25 mm ( = 0 , 783 a 1 , 25 mm vs = 0 , 375 a 2 , 5 mm )  . 
anche il confronto tra queste differenze risultato statisticamente significativo . discussion discussione the volumetric software used in this study showed a good overall performance , allowing nodule segmentation and volume measurement in most reconstructions at different slice thicknesses , mas and algorithms . 
however , the system failed to segment the juxtapleural nodule in reconstructions at 40 mas , with 2.5 - mm slice thickness and algorithms with medium to high spatial resolution . 
however , the partial volume effect resulting from greater slice thickness and the increase in noise due to the low tube - current settings and il software 3d impiegato in questo studio ha dimostrato una buona performance complessiva , consentendo di segmentare e calcolare il volume dei noduli considerati nella maggior parte delle ricostruzioni a diversi spessore di strato , algoritmo e mas . 
tuttavia , il nodulo iuxtapleurico non stato segmentato nelle ricostruzioni a 40 mas , con spessore di strato di 2 , 5 mm ed algoritmi a medio - alta risoluzione spaziale . 
tuttavia , anche leffetto di volume parziale dovuto allutilizzo dello spessore di strato magradiol med ( 2008 ) 113 : 2942 table 2 comparison between the differences of the calculated and real volumes ( , cm3 ) for each nodule at 100 mas and 40 mas . 
the differences are expressed for each reconstruction at different slice thickness and kernel slice thickness kernel juxtapleural nodule 100 mas 40 mas juxtavascular nodule 100 mas 40 mas circumscribed nodule 100 mas 40 mas a statistically significant differences ( students t test ) tabella 2 confronto tra le differenze dei volumi calcolati da quelli reali ( , cm3 ) per ciascun nodulo , a 100 mas e a 40 mas . 
this finding indicates that nodule segmentation , regardless of location , is best achieved at 2.5 - mm slice thickness when standard tube - current settings are used ( 100 mas )  . these results give rise to several considerations . 
in particular , selection of the most appropriate algorithm in relation to giore e laumento del rumore dovuto allimpiego del basso amperaggio e di algoritmi a medio - alta risoluzione potrebbero aver contribuito alla mancata segmentazione di tale nodulo . 
 tutti gli algoritmi hanno , invece , consentito la segmentazione dei tre noduli considerati , quando stato impiegato lo spessore di strato di 2 , 5 mm e 100 mas ; tuttavia , lalgoritmo a minore risoluzione spaziale ( standard ) ha fornito la stima pi precisa del volume reale dei noduli . 
questo dato indica la possibilit di ottenere una migliore segmentazione dei noduli , qualunque sia la loro sede , a spessore di 2 , 5 mm , se vengono utilizzati milliamperaggi standard ( 100 mas )  . da questi risultati scaturiscono alcune osservazioni . 
with a slice thickness of 2.5 mm , high - spatial - resolution algorithms should not be used , either with standard or low tube - current settings . the most reliable estimation of the real volume of the three nodules , at 1.25 - mm slice thickness , was obtained with high - spatial - resolution algorithms ( bone and bone + ) at 100 mas and at 40 mas , respectively . 
 results of the comparison of the differences between calculated and real volumes at 100 mas and 40 mas showed no significant differences at 1.25 mthis suggests that protocols with standard or low tube - current settings may be applied indifferently when thin reconstruction slices are used sede dei noduli pu influenzare il processo di segmentazione in rapporto ai diversi parametri tecnici impiegati , quali spessore di strato , algoritmo di ricostruzione e corrente del tubo ; in particolare , la scelta dellalgoritmo pi adeguato rispetto ai restanti parametri pu migliorare la performance del software 3d . 
 la stima pi attendibile del volume reale dei tre noduli , utilizzando uno spessore di 1 , 25 mm , stata ottenuta impiegando gli algoritmi ad alta risoluzione spaziale ( bone e bone + ) , rispettivamente a 100 mas e a 40 mas : ci indica la necessit di migliorare la risoluzione spaziale quando si utilizzano spessori sottili o protocolli a basso amperaggio , in rapporto allaumento del rumore . 
this is particularly interesting in consideration of the possible application of automated volumetry in the follow - up of nodules detected in lung cancer screening programmes , which involve low - dose protocols ( 20 , 40 or 50 mas )  . although similar results were also obtained at 2.5 mm for the juxtavascular and well - circumscribed nodules , segmentation of the juxtapleural nodule at 40 mas could only be achieved with the standard algorith with this kernel , however , volume determination of the juxtapleural nodule proved to be significantly more precise at a standard tubecurrent setting . 
moreover , the advent of mdct has increased the incidental discovery of small pulmonary nodules ( diameter < 1 cm ) that are difficult to characterise and that require radiologic follow - up [ 4 ] , considered more reliable when based on automatic volume determination . 
risultato interessante , se si considera la possibile applicazione dei sistemi automatici di volumetria 3d dei noduli nel follow - up dei pazienti inseriti nei programmi di screening del tumore polmonare , che prevedono limpiego di protocolli a bassa dose ( 20 , 40 o 50 mas )  . sebbene medesimi risultati siano stati ottenuti anche a 2 , 5 mm per i noduli iuxtavascolare e ben circoscritto , la segmentazione del nodulo iuxtapleurico a 40 mas stata possibile soltanto con lalgoritmo standard ; tuttavia , con questo kernel la misurazione del volume del nodulo iuxtapleurico risultata significativamente pi precisa ad amperaggio standard . 
quando si utilizzano milliamperaggi bassi devono essere evitati spessori di strato superiori a 1 , 25 mm , che possono associarsi ad errori del sistema nel calcolo del volume dei noduli , soprattutto se con ampie connessioni con la superficie pleurica . i risultati del confronto tra le differenze dei volumi calcolati da quelli reali , effettuato tra le ricostruzioni a spessore di strato di 1 , 25 mm e 2 , 5 mm , non hanno dimostrato differenze significative a 100 mas . 
la possibilit di utilizzare indifferentemente uno spessore sottile ( 1 , 25 mm ) o uno spessore relativamente maggiore ( 2 , 5 mm ) , ad amperaggio standard , avvalora il possibile impiego dei sistemi automatici di volumetria negli esami di routine del torace , generalmente non eseguiti con spessore di strato sottile . 
inoltre , con lavvento della tcmd divenuto frequente riscontrare , negli esami del torace eseguiti per altri motivi , noduli polmonari di piccole dimensioni ( diametro < 1 cm ) , difficili da caratterizzare e per i quali richiesto un follow - up radiologico [ 4 ] , considerato pi affidabile se effettuato con il calcolo automatico del volume . 
 i risultati del confronto a 40 mas indicano , al contrario , una differenza significativa tra i valori delle differenze dei volumi calcolati sulle ricostruzioni a 1 , 25 mm rispetto a quelli calcolati a 2 , 5 mm , sia per il nodulo iuxtavascolare che per quello ben circoscritto . 
la stima pi precisa del volume di questi noduli a basso amperaggio stata osservata a 1 , 25 mm , indipendentemente dallalgoritmo impiegato ( con leccezione del lung per il nodulo ben circoscritto , che comunque non ha inciso sul risultato finale )  . 
tali dati indicano che la performance del software a basso amperaggio pu essere significativamente inferiore quando si utilizza radiol med ( 2008 ) 113 : 2942 by contrast , results of the comparison at 40 mas indicate a significant difference between volume differences calculated on the 1.25 - mm and 2.5 - mm reconstructions with regard to both the juxtavascular and the well - circumscribed nodules . the most accurate estimation of the volume of these nodules , at low tube - current settings , was observed at 1.25 mm , regardless of the algorithm used ( with the exception of the lung algorithm for the well - circumscribed nodule , which in any case did not affect the final result )  . 
first , the small number of nodules considered may have influenced the results ; the poor performance of the system with regard to the juxtapleural nodule needs to be confirmed on a larger number of nodules of varying size and in a similar location . 
in addition , we tested the performance of the software in use at our institution only , so the results obtained may not apply to other automated systems . comparative studies using the same materials and technical parameters are required to compare the performance of different software packages . 
the influence of collimation less than 1.25 mm was not analysed ; if , on the one hand , use of very thin collimation ( 0.625 mm ) improves spatial resolution and the systems segmentation capabilities , on the other hand , it entails higher patient doses . 
these nodules , in particular nonsolid nodules , have density values that are closuno spessore di strato maggiore di 1 , 25 minoltre , il nodulo iuxtapleurico stato segmentato a 40 mas soltanto con lalgoritmo standard , per il quale stato possibile confrontare le differenze dei volumi calcolate a 1 , 25 e a 2 , 5 mm ; la stima del volume di questo nodulo risultata paradossalmente pi accurata a 2 , 5 mquesti risultati , apparentemente in contraddizione , potrebbero essere dipendenti da un errore sistematico del software nelle misurazioni volumetriche sul nodulo iuxtapleurico , a basso amperaggio e a spessore di strato maggiore di 1 , 25 m il nostro studio presenta alcuni limiti . 
innanzitutto , la bassa numerosit del campione di noduli che pu aver influenzato i risultati ; la scarsa performance del sistema sul nodulo iuxtapleurico andrebbe confermata su un numero maggiore di noduli localizzati in tale sede e di dimensioni diverse . 
per quanto riguarda le dimensioni dei noduli impiegati , non sono stati analizzati noduli con diametro inferiore o uguale a 0 , 5 cm . i sistemi automatici sono stati introdotti inizialmente solo allo scopo di identificare e poi anche di calcolare il volume dei noduli , soprattutto di piccole dimensioni , il cui accrescimento difficile da valutare con i metodi bidimensionali . 
linfluenza di collimazioni inferiori a 1 , 25 mm non stata analizzata ; se da un alto collimazioni ultrasottili ( 0 , 625 mm ) migliorano la risoluzione spaziale e la capacit di segmentazione del sistema , dallaltro comportano un incremento dosimetrico al paziente . 
questi noduli , e in particolare quelli non solidi , hanno valori densitometrici pi vicini a quelli del parenchima aerato e il processo di segmentazione automatica potrebbe essere sensibilmente influenzato dalla loro densit oltre che dai parametri tecnici selezionati . 
 radiol med ( 2008 ) 113 : 2942 er to those of the aerated lung , and the automated segmentation process might be substantially affected by nodule density as well as by the technical parameters selected . 
moreover , nodule location may affect segmentation and volume measurement in relation to the technical parameters selected for the study . further investigations on larger samples of artificial nodules , with varying density , diameter and location , and comparative studies of the performance of different automated systems are required to validate the results of our study . 
lalgoritmo di ricostruzione che meglio stima il volume dei noduli solidi , varia in rapporto allo spessore di strato utilizzato ; indicato luso di un kernel ad alta risoluzione spaziale se lo spessore impiegato 1 , 25 mm e di un kernel a minore risoluzione se lo spessore 2 , 5 mm . la corrente del tubo o amperaggio per tempo di rotazione ( mas ) un fattore limitante la volumetria in relazione allo spessore di strato scelto ; quando viene utilizzato uno spessore di strato sottile ( 1 , 25 mm ) si possono impiegare indifferentemente milliamperaggi standard ( 100 mas ) o bassi ( 40 mas ) , mentre a spessore di 2 , 5 mm e a basso amperaggio , il software presenta performance inferiori e possibili errori sistematici nella segmentazione dei noduli , in particolare di quelli con connessioni pleuriche . lo spessore di strato non influenza la segmentazione dei noduli in modo significativo ad amperaggio standard , potendo utilizzare indifferentemente spessori di 1 , 25 mm e di 2 , 5 mm ; questo risultato incoraggia limpiego della volumetria 3d nella pratica clinica . 
la migliore performance del nostro software stata osservata utilizzando uno spessore di strato di 1 , 25 mm ed algoritmi ad elevata risoluzione spaziale , sia a 100 che a 40 mas . 
barai5 1unit operative di diagnostica per immagini , 2ortopedia e traumatologia , 3medicina generale ( sezione di malattie osteometaboliche ) , 4oncologia , 5servizio di fisica sanitaria , azienda ospedaliera carlo poma , viale albertoni 1 , 46100 mantova , italy correspondence to : r . 
the first 78 patients were treated using computed tomography ( ct ) combined with conventional fluoroscopy as an imaging guide ( 135 pvp )  . in 28 patients , the procedure was performed with multislice ct fluoroscopy ( 47 pvp )  . 
partial or complete pain relief was obtained in 98% of patients within 24 h from the treatment ; significant results were also obtained with regard to improvement in functional mobility and reduction of analgesic use . 
the use of ct guidance reduces the risk of complications in comparison with conventional fluoroscopy alone , as well as facilitates the detection of small cement leakages . keywords spine vertebroplasty spine fractures spine ct spine secondary neoplasms osteoporosis riassunto obiettivo . 
nei primi 78 pazienti la guida tc stata associata alla radio - fluoroscopia tradizionale ( 135 vpp )  . in 28 pazienti si utilizzata solo tc - scopia con apparecchiatura multistrato ( 47 vpp )  . 
nel 98% dei pazienti si rilevata riduzione / scomparsa del dolore entro 24 ore dal trattamento ; i risultati sono stati significativi anche per la riduzione della terapia farmacologica ed il miglioramento della autonomia motoria . 
limpiego della guida tc riduce i rischi di complicanze rispetto alla sola guida fluoroscopica convenzionale e rende pi agevole il riconoscimento di piccole fughe extravertebrali di cemento . parole chiave vertebroplastica fratture vertebrali tc vertebrale metastasi vertebrali osteoporosi radiol med ( 2008 ) 113 : 114133 introduction percutaneous vertebroplasty ( pvp ) is a minimally invasive , image - guided procedure that entails injecting acrylic cement into a vertebral body to reinforce the compressed segment and achieve pain relief . 
initially used to treat aggressive vertebral haemangioma , pvp was later extended to other painful vertebral lesions caused by metastases , osteoporotic vertebral compression fractures , myeloma and other less common conditions ( histocytosis , osteogenesis imperfecta ) [ 3 ]  . 
since the earliest experiences , pvp has undergone numerous modifications in patient selection and procedure technique as a result of the constant refinement of materials and imaging guides ; this has led to better results , shorter procedure times and fewer complications [ 4 ]  . we review our personal series to describe the criteria used for patient selection , the technique and the results achieved with pvp performed under computed tomography ( ct ) guidance . 
 materials and methods series collection our series was collected from october 2003 to april 2006 . we performed 182 pvp in 106 patients , 67 of whom had osteoporosis and 39 of whom had metastases ( table 1 ) from cancers of the breast ( 17 ) , lung ( 7 ) , kidney ( 4 ) , colon ( 3 ) , prostate ( 1 ) , oesophagus ( 1 ) , liver ( 1 ) , neuroendocrine tumours ( 1 ) and myeloma ( 4 )  . 
patients with osteoporosis underwent 120 pvp procedures , 93 of which were at the lumbar level ( 77.5% ) ; patients with metastasis underwent 62 pvp , 35 of which were at the dorsal level ( 56.4% ) ( table 1 )  . 
 patient selection patient selection was performed by a multidisciplinary team consisting of an internist specialized in metabolic bone disease ( lv ) , an oncologist ( ea ) , an orthopaedic surgeon ( lrb ) and a radiologist ( rc )  . 
indications for pvp were dorsolumbar vertebral fractures due to recent osteoporotic vertebral collapse accompanied by pain not responding to medical therapy ( rest , analgesics , orthopaedic corset ) and dorsolumbar vertebral metastases with fractures and / or areas of vertebral body osteolysis with inadequate response to medical therapy . 
contraindications to pvp were involvement of the spinal canal by retropulsed fracture fragments or by tumour introduzione la vertebroplastica percutanea ( vpp ) una procedura minimamente invasiva effettuata con guida imaging , che consiste nella introduzione di cemento acrilico nel soma di una vertebra per ottenere la riduzione del dolore mediante il rinforzo strutturale del metamero compromesso . 
inizialmente la vpp stata utilizzata per il trattamento degli emangiomi vertebrali aggressivi e successivamente estesa ad altre lesioni dolorose vertebrali causate da metastasi , cedimenti osteoporotici , mieloma , e anche da altre condizioni meno frequenti ( istiocitosi , osteogenesis imperfecta ) [ 3 ]  . 
dalle prime esperienze a tuttoggi , la vpp stata oggetto di continue modifiche per quanto concerne la selezione dei pazienti e le modalit di effettuazione , grazie al continuo affinamento dei materiali e delle apparecchiature di guida imaging ; ne sono conseguiti miglioramento dei risultati , riduzione dei tempi di effettuazione e delle complicanze [ 4 ]  . il nostro lavoro si basa sulla revisione della casistica personale presentando le modalit di selezione dei pazienti , la metodologia ed i risultati conseguiti utilizzando un approccio tc - guidato . materiali e metodi raccolta della casistica la casistica personale stata raccolta dallottobre 2003 allaprile 2006 . 
sono state effettuate 182 vpp in 106 pazienti , dei quali 67 affetti da osteoporosi e 39 da metastasi ( tabella 1 ) da tumori della mammella ( 17 ) , del polmone ( 7 ) , del rene ( 4 ) , del colon ( 3 ) , della prostata ( 1 ) , dellesofago ( 1 ) , del fegato ( 1 ) , neuroendocrini ( 1 ) e da mieloma ( 4 )  . 
nei pazienti affetti da osteoporosi sono state effettuate 120 vpp di cui 93 a livello lombare ( 77 , 5% ) ; nei pazienti affetti da metastasi sono state effettuate 62 vpp di cui 35 a livello dorsale ( 56 , 4% ) ( tabella 1 )  . 
 selezione dei pazienti la selezione dei pazienti stata compiuta da un gruppo multidisciplinare cos composto : un internista specializzato in osteopatie metaboliche ( lv ) , un oncologo ( ea ) , un ortopedico ( lrb ) e un radiologo ( rc )  . 
the first level of selection , carried out by the internist , oncologist and orthopaedic surgeon , identified patients with osteoporotic vertebral collapse or metastases to the dorsolumbar vertebrae accompanied by pain not sufficiently responsive to medical therapy . 
all patients were administered the following assessment scales to ascertain clinical eligibility for pvp : 10 - point visual analogue scale ( vas ) ( 10 worst ever pain ; 1 no pain ) for pain assessment [ 6 ] , 4 - point functional mobility scale ( 4 bedridden ; 3 use of wheelchair ; 2 limited painful ambulation ; 1 normal ambulation ) and 3 - point analgesic use scale ( 3 complete daily coverage ; 2 partial daily coverage ; 1 occasional coverage )  . 
all patients underwent radiographic assessment ( anteroposterior and lateral radiograms ) and magnetic resonance imaging ( mri ) with 0.5 - t ( philips - gyroscan t5 - nt , eindoven , netherlands ) or 1.5 - t ( siemens - avanto , erlangen , germany ) superconductive units . 
sono state accettate come controindicazioni alla vpp : il coinvolgimento del canale spinale da parte di frammenti di frattura retropulsi o da estensione tumorale epidurale ; il collasso vertebrale severo con riduzione dellaltezza somatica a meno di 1 / 3 di quella originaria ; le spondilodisciti ; le diatesi emorragiche ; le allergie note a qualsiasi prodotto utilizzato nella procedura ( anestetico locale ; cemento acrilico )  . le indicazioni e le controindicazioni adottate sono state verificate in due livelli di selezione . 
un primo livello clinico , di competenza dellinternista , delloncologo e dellortopedico , nel quale sono stati identificati i pazienti con cedimento osteoporotico o con metastasi alle vertebre dorso - lombari , accompagnato a dolore con insufficiente risposta alla terapia medica . 
tutti i pazienti sono stati sottoposti alle seguenti scale di valutazione per la verifica dellesistenza della compatibilit clinica alla effettuazione della vpp : scala del dolore utilizzando la scala vas ( visual analogic scale ) di 10 punti ( 10 peggiore ; 1 nessuno ) , riportata in letteratura [ 6 ] ; scala dellautonomia motoria di 4 punti ( 4 : allettato ; 3 : utilizzo di sedia a rotelle ; 2 : deambulazione limitata con dolore ; 1 : deambulazione normale ) ; scala delleventuale terapia farmacologia antalgica di 3 punti ( 3 : copertura giornaliera completa ; 2 : copertura giornaliera parziale ; 1 : copertura occasionale )  . 
a in the lateral x - ray view , compression fracture of the l3 vertebral body with height not less than one third of the original one ( see text )  . 
b , c sagittal magnetic resonance images obtained with turbo spin - echo t1 - weighted ( b ) and fat - suppressed short tau inversion recovery ( stir ) t2 - weighted ( c ) sequences show a change in signal intensity at the l5 vertebral body , characterized by t1 hypointensity and stir t2 hyperintensity owing to bone marrow oedema resulting from a recent vertebral collapse that was causing pain ( clinical correspondence )  . 
normale laltezza degli altri corpi vertebrali lombari . b , c nelle sezioni rm sagittali ottenute con sequenze turbo spin echo t1 dipendente ( b ) e con soppressione del segnale adiposo ( stir ) t2 dipendente ( c ) , si apprezza modificazione del segnale a livello di l5 caratterizzata da ipointensit t1 e da iperintensit t2 dovuta ad edema endospongioso somatico da cedimento recente , responsabile della sintomatologia dolorosa ( concordanza clinica )  . 
anatomical compatibility was based on the following findings : evidence on the lateral radiogram and / or midsagittal mr images of vertebral collapse , with at least one third of original height preserved , as shown by comparison with previous normal radiographs and / or mr images or , if unavailable , by measuring normal - appearing vertebral bodies adjacent to the collapsed one [ 7 , 8 ] evidence on the lateral radiogram and / or mr images of areas of osteolysis and / or vertebral body fracture with intact posterior wall , vertebral pedicles and spinal canal no mr evidence of spinal cord or nerve root compression signs of recent vertebral collapse with mr signal change due to bone marrow oedema and characterized by t1 hypointensity and t2 hyperintensity enhanced by fat suppression ture superconduttive da 0 , 5 t ( philips - gyroscan t5 - nt , eindoven , olanda ) o da 1 , 5 t ( siemens - avanto , erlangen , germania )  . 
le indagini rm sono state condotte sui piani sagittali ed assiali con sequenze turbo - spin - echo t1 e t2 dipendenti , senza e con soppressione del segnale adiposo ; nelle metastasi vertebrali stato somministrato mdc paramagnetico per via ev ( 0 , 2 cc / kg di peso corporeo ) gadopentato di dimeglumina ( magnevist - schering , berlino , germania )  . 
la compatibilit anatomica stata caratterizzata dalle seguenti evenienze : cedimento strutturale nel radiogramma laterale e / o nelle immagini rm medio - sagittali , con altezza somatica non < 1 / 3 di quella originaria , questultima valutata nei radiogrammi e / o nelle immagini rm precedenti normali se disponibili , oppure , se non disponibili , mediante la misurazione dei corpi vertebrali apparentemente normali 118 radiol med ( 2008 ) 113 : 114133 fig . 
a in the anteroposterior x - ray view , osteolysis of the right vertebral pedicle ( arrow ) due to a metastasis ; the contralateral pedicle is normal ( empty arrow )  . 
a nel radiogramma in proiezione antero - posteriore , osteolisi del peduncolo vertebrale di destra ( freccia ) da localizzazione secondaria ; normale il peduncolo controlaterale ( freccia vuota )  . 
 materials materials were prevalently a simko kit ( optimed , ettlingen , germany ) composed of needles with stylet and bevel or diamond tip , 15 - , 13and 10 - gauge calibre and 10to 15cm - long , syringe with a metal manual injector and attachments for the aspiration / injection of acrylic cement . 
in all cases , we used the radiopaque acrylic cement mendec spine ( tecres s.p.a. , sommacampagna , verona , italy ) adiacenti a quello collassato , cos come suggerito in letteratura [ 7 , 8 ] ; area di osteolisi e / o frattura del soma vertebrale con integrit del muro vertebrale posteriore , dei peduncoli vertebrali e del canale spinale nel radiogramma laterale e / o nelle immagini rm ; assenza di compressione mielo - radicolare nelle immagini rm ; segni di cedimento somatico recente con modificazione del segnale rm dovuta ad edema midollare endospongioso , caratterizzata da ipointensit t1 , iperintensit t2 questultima enfatizzata con soppressione del segnale adiposo ; concordanza fra il livello / i somatico / i della modificazione del segnale endospongioso e la sede / i del dolore ; assenza di enhancement dopo mdc paramagnetico del tessuto epidurale , indicativo di diffusione tumorale nelle immagini rm delle metastasi ; assenza di osteocondensazione della tela spongiosa somatica nei radiogrammi ( secondaria a fenomeni osteoriparativi spontanei o indotti dal trattamento chemio e / o radioterapico ) che possa ostacolare la introduzione del cemento nel corpo vertebrale . 
 il tempo medio dedicato alla selezione dei pazienti fino radiol med ( 2008 ) 113 : 114133 predominantly composed of polymethylmethacrylate ( pmma ) and with a polymerization ( hardening ) time less than 10 mpreparation of the acrylic cement involved mixing the solvent ( 9.4g of mma , n , n - dimethyl - p - toluidine , hydroquinone ) with the powder ( 20g of pmma , 30% barium sulphate , benzoyl peroxide ) for 30 s in a closed bottle to avoid the formation of potentially toxic vapours [ 9 ]  . 
we also used a 10 - cc syringe to inject the local anaesthetic , needles included in the kit or chiba needles ( 1819 gauge ; length 20 cm ) both for deep anaesthesia and as a guide to advance the pvp needle coaxially from the skin to the bone cortex , after cutting the external tip of the needle when necessary ( plastic connector in the chiba needles )  . 
finally , we used a scalpel for the skin incision at the entry point and a 3 - hg surgical hammer to help the needle penetrate the bone . methods as regards methodology , patients were informed about the benefits and risks of the procedure before providing their informed consent . 
to minimise the risk of infection , in agreement with the literature [ 4 , 10 ] , patients who were immunocompromised because of cancer therapy received antibiotic prophylaxis 3 days before the procedure . pvp was carried out under ct guidance in all cases . 
in 78 patients , 135 pvp were performed using single - slice spiral ct ( picker pq5000 , cleveland , oh , usa ) combined with conventional radiofluoroscopy ( siremobil iso - c , siemens , erlangen , germany )  . 
in 28 patients , 47 pvp were performed using multislice spiral ct alone ( sensation 16 , siemens , erlangen , germany ) with the following ct - fluoroscopy equipment : an additional 17 - liquid - crystal monitor , placed inside the ct room and moveable to be well visualised by the operator , with identical capabilities to the monitor of the main console . 
this monitor allows real - time display of axial ct - fluoroscopy images and visualisation of axial images acquired on the volume and / or reconstructed with multiplanar reformatting ( mpr ) in the sagittal and coronal planes . 
the operator could thus follow the most delicate phases of the procedure ( needle placement in the vertebral body , cement injection ) on the axial ct - fluoroscopy images in real time to evaluate cement distribution in the vertebra and identify immediately even the slightest cement leak , which requires slowing or temporary interruption of the injection . 
the craniocaudal extent of possible cement leaks identified on the axial ct - fluoroscopy images can be precisely defined by visualising the sagittal and coronal mpr images acquired on the vertebral volume during or after the procedure . 
 a control joystick to move the ct table a floor pedal to control the scan alla effettuazione della vpp stato globalmente di 11 , 65 , 2 giorni , lievemente inferiore nei pazienti affetti da osteoporosi ( 10 , 52 , 6 giorni ) rispetto a quelli con metastasi ( 13 , 57 , 6 giorni )  . 
 materiali per quanto riguarda il materiale impiegato , abbiamo utilizzato prevalentemente il kit simco ( optimed , etlingen , germania ) composto di aghi con mandrino a punta conformata a becco di flauto / diamante , del calibro di 15 g , 13 g , 10 g e della lunghezza di 1015 cm , di siringa con iniettore manuale in metallo e raccordi per laspirazione / iniezione del cemento acrilico . 
abbiamo sempre utilizzato il cemento acrilico radio - opaco mendec spine ( tecres spa , sommacampagna , verona , italia ) costituito principalmente da poli - metil - meta - acrilato ( pmma ) caratterizzato da tempo di polimerizzazione ( indurimento ) inferiore ai 10 min ; la preparazione del cemento acrilico stata effettuata mediante la miscelazione della durata di 30 s del solvente ( 9 , 4 g composti di mma , n , n - dimetil - p - toluidina , idrochinone ) con la polvere ( 20 g composti di pmma , solfato di bario al 30% , perossido di benzoile ) in flacone chiuso per evitare lesalazione che pu risultare potenzialmente tossica per il personale [ 9 ]  . 
abbiamo inoltre utilizzato una siringa da 10 cc per liniezione di anestetico locale , aghi inclusi nel kit oppure aghi chiba ( 1819 g ; lunghezza 20 cm ) sia per lanestesia in profondit , sia come guida sulla quale far avanzare coassialmente lago della vpp dalla cute alla corticale ossea della vertebra da trattare , previo taglio dellestremit esterna dellago con tronchese , quando necessario ( presenza di raccordo di plastica negli aghi chiba )  . 
infine , bisturi per lincisione della cute nella sede di accesso e martello ortopedico del peso di 3 hg per agevolare la penetrazione ossea dellago . metodologia per quanto riguarda la metodologia i pazienti sono stati preliminarmente informati dei benefici e dei rischi dellintervento per la firma del consenso informato . 
per ridurre al minimo i rischi di infezione , cos come suggerito in letteratura [ 4 , 10 ] , i pazienti immunodepressi per terapie oncologiche sono stati sottoposti a preventivo trattamento con antibiotici 3gg prima dellintervento . la procedura stata condotta in tutti i casi con guida tc . 
in 78 pazienti sono state effettuate 135 vpp utilizzando tc spirale monostrato ( picker pq5000 , cleveland , ohio ) associata a radio - fluoroscopia tradizionale ( siemens siremobil iso - c ; erlangen , germania )  . 
a , b at the l5 level , computed tomography ( ct ) - fluoroscopy - guided insertion of the cannula ( a ) for cement injection ( b ) in the body ; during the injection , small venous anterior leakages of cement ( arrows ) are seen , without clinical symptoms . 
a , b guida con tc - scopia a livello di l5 della introduzione dellago cannula ( a ) per la iniezione del cemento acrilico ( b ) nel soma ; durante la iniezione piccole fughe venose anteriori ( frecce ) del cemento , senza sintomatologia . 
c controllo tc dopo la procedura : nella immagine sagittale ottenuta con tecnica multi planar reformatting ( mpr ) , si riscontra omogenea distribuzione del cemento e piccola fuga venosa anteriore ( freccia ) , a direzione craniale . radiol med ( 2008 ) 113 : 114133 fig . 
vpp multi - livello con approccio dorsale inter - costo - trasversario ( d8 , d11 ) e lombare trans - mono - peduncolare ( l1 , l3 )  . 
the surgical field was prepared by accurately sterilising the skin over a surface of approximately 80 cm2 and delimiting the needle entry point with large sterile drapes to minimize risks of infection . 
in tal modo loperatore ha potuto seguire sul piano assiale con tc - scopia in tempo reale le fasi pi critiche della procedura ( posizionamento dellago nel soma vertebrale ; iniezione del cemento ) , per valutare la diffusione intra - somatica del cemento e , nello stesso tempo , identificare immediatamente anche le minime fughe extra - vertebrali di cemento , ci che richiede limmediato rallentamento e / o interruzione temporanea delliniezione . 
needle advancement through the cortical and trabecular bone was achieved with the aid of the surgical hammer under radiofluoroscopic guidance in a lateral projection or with ct fluoroscopy in the axial plane . 
once the needle was positioned in the vertebral body , after removing the stylet , in some cases we injected iodinated water - soluble contrast medium into the vertebral body through the cannula ( venous vertebrogram ) to visualise the basivertebral venous plexus and its branches into the epidural plexuses and inferior caval systein agreement with other authors [ 3 ] , we performed a vertebrogram only when , after removing the stylet , we noted blood flowing out of the external tip of the cannula . 
this occurred in four pvp procedures for the treatment of metastases . before injection of the acrylic cement , a biopsy was obtained with a core biopsy needle introduced coaxially into the pvp cannula , but this was done only when the initial diagnostic assessment had failed to identify the nature of the vertebral alteration ( 14 patients )  . 
the amount of acrylic cement injected in each vertebra ranged from 2 cc to 9 cc ( mean 5.7 cc / pvp )  . e per il contenimento della dose di esposizione radiante ( hand - care )  . una volta posizionato il paziente in decubito prono nel modo pi confortevole possibile stata effettuata la preliminare acquisizione di un pacchetto di scansioni tc per la visualizzazione delle immagini assiali e / o ricostruite con tecnica mpr nei piani sagittale e coronale . 
la preparazione del campo stata effettuata disinfettando accuratamente la cute per un area di circa 80 cm2 , delimitando la sede di introduzione dellago / aghi con ampi teli sterili per ridurre al minimo i rischi di infezione . 
a guide needle ( chiba ) insertion into the periosteum and cutting of its external tip . b on the guide needle , coaxial introduction of the cannula ( with bevelled distal end ) and insertion into the bone cortex . 
with the bevel tip oriented laterally , the needle avoids the spinal canal , whereas with the bevel tip oriented medially , the needle approaches the centre of the body ( arrows )  . 
a infissione dellago guida ( chiba ) sul periostio e taglio della sua estremit esterna . b avanzamento coassiale dellago cannula ( punta a becco di flauto ) sullago fino alla corticale ossea . 
d la direzione della penetrazione dellago dipende dallorientamento della punta del tagliente ottenuto ruotando ( freccia curva ) la porzione esterna dellago : con punta rivolta verso lesterno lago avanza evitando il canale spinale , mentre con punta rivolta allinterno lago avanza avvicinandosi al centro del soma vertebrale ( frecce )  . 
e una volta posizionato lago e sfilato il mandrino , viene lentamente iniettato il cemento acrilico . monitoring the cement injection to check its distribution in the vertebral body and / or identify possible leakages was done under radiofluoroscopic guidance in 135 pvp . 
to avoid the risk of spreading the cement in the soft tissues [ 3 , 10 ] , approximately 10 min after the injection , the needle was slowly removed by rotating and withdrawing it gently . 
where pulmonary complidellago attraverso la corticale e nella tela spongiosa del soma vertebrale stato effettuato con lausilio del martello ortopedico , sotto il controllo radio - fluoroscopico nella proiezione laterale o sul piano assiale con tc - scopia . 
posizionato lago nel soma vertebrale , una volta tolto il mandrino , in alcuni casi stata effettuata iniezione di mdc organoiodato idro - solubile nel soma vertebrale attraverso lagocannula ( vertebrogramma venoso ) in modo da visualizzare il plesso venoso basi - vertebrale e le sue efferenze nei plessi epidurali e nel sistema cavale inferiore . 
in accordo con altri autori [ 3 ] , abbiamo ritenuto opportuno eseguire il vertebrogramma venoso solo quando , rimuovendo il mandrino , abbiamo visto refluire sangue dalla estremit esterna dellagocannula ; ci si verificato in 4 vpp per il trattamento di metastasi . prima di iniettare il cemento acrilico la biopsia ossea stata effettuata con ago da carotaggio introdotto coassial124 radiol med ( 2008 ) 113 : 114133 fig . 
postprocedural chest ct , performed owing to mild dyspnoea after the procedure , demonstrates small emboli of cement ( white arrows ) in some distal arterial branches of the right lower lobe . 
after ct assessment , patients were instructed to get off the table and maintain an upright position for about 1 min to check their clinical condition immediately after pvp before transferring them to a stretcher . mente nellago - cannula della vpp , solo nei casi in cui ( 14 pazienti ) , nella fase di selezione , la valutazione diagnostica non ha stabilito la natura dellalterazione vertebrale . 
una viscosit troppo bassa aumenta il rischio di fuga extra - ossea del cemento , mentre una viscosit troppo elevata pu causare difficolt di iniezione e quindi di riempimento del soma vertebrale . 
ad evitare il rischio di disseminare il cemento nelle parti molli [ 3 , 10 ] , lestrazione dellago stata sempre effettuata a circa 10 min dal termine della iniezione , lentamente e progressivamente con movimenti combinati di rotazione e dolce trazione dellago . 
completata la valutazione tc , ciascun paziente stato fatto scendere dal lettino mantenendo la stazione eretta per circa un minuto prima di radiol med ( 2008 ) 113 : 114133 patients lay in a supine position for about 3 h after the procedure . 
most patients were discharged from hospital within 24 h ( 104 patients ) ; two patients remained in hospital for 3 days after the procedure because of severe complications requiring treatment and a period of observation . follow - up follow - up of all 106 patients was performed by the internist . 
because the length of follow - up could not be predicted for each patient , during the first follow - up visit , patients were administered the same questionnaire as used for patient selection and consisting of an assessment of pain ( 10 - point vas ) , functional mobility ( 4 - point scale ) , analgesic use ( 3 - point scale )  . 
 complications were divided into mild ( conditions requiring bland therapy and / or a 24 - h observation period in hospital ) and severe ( conditions requiring more aggressive treatment and / or hospitalisation for more than 24 h )  . 
 extravertebral cement leakages were not considered complications unless they were accompanied by clinical symptoms ; therefore , for the purposes of statistical analysis , all cement leakages , whether mild or severe , were classified according to their site : paravertebral , intradiscal , epidural , foraminal and vascular . recurrences were subdivided into osteoporotic vertebral collapse or metastases appearing in other dorsolumbar vertebrae following pvp . data were entered in a database and processed for the whole series and for the two patient groups separately ( osteoporosis , metastases )  . 
statistical analysis was carried out by the medical physicist ( gb ) who used students t test for unpaired data to derive the p value from two sets of mean values . farlo coricare sulla barella per verificare immediatamente le condizioni cliniche dopo la vpp . dopo il trattamento il paziente ha mantenuto il decubito supino per circa 3 h . 
le dimissioni dallospedale sono avvenute entro le 24 h nella maggioranza dei casi ( 104 pazienti ) ; 2 pazienti sono stati trattenuti dopo lintervento con un ricovero di 3 giorni per complicanze pi gravi che hanno richiesto terapia con periodo di osservazione . follow - up il follow - up stato effettuato dallinternista in tutti i 106 pazienti . 
non potendo prevedere la durata del follow - up in ciascun paziente , nel corso della prima visita di controllo stato utilizzato il medesimo questionario della selezione dei pazienti con scale per la valutazione del dolore ( scala vas di 10 punti ) , dellautonomia motoria ( scala di 4 punti ) , delleventuale terapia antalgica farmacologica ( scala di 3 punti )  . 
il tempo medio intercorso fra il trattamento e la prima visita di controllo stato di 1 , 71 , 6 mesi nella serie totale , superiore nei pazienti osteoporotici ( 1 , 81 , 4 mesi ) rispetto ai pazienti con metastasi ( 1 , 31 , 2 mesi )  . 
la durata complessiva media del follow - up stata variabile : pi breve ( 3 , 39 mesi ) nei pazienti con metastasi ( intervallo : 0 , 311 , 5 mesi ) in rapporto alla progressione neoplastica , rispetto a quella ( 3 , 92 mesi ) dei pazienti con osteoporosi ( intervallo : 0 , 223 , 4 mesi )  . outcomes lanalisi dei risultati del trattamento stata condotta in tutti i pazienti entro le 24 h dallintervento e nel follow - up , confrontando i dati dei questionari raccolti prima e dopo la effettuazione della vpp . 
pertanto i risultati clinici fanno riferimento alle scale di valutazione del dolore , dellautonomia motoria e delleventuale terapia antalgica farmacologica . le complicanze sono state suddivise in lievi ( condizioni che hanno richiesto blanda terapia e / o periodo di osservazione di 24 h in ospedale ) e gravi ( condizioni che hanno richiesto terapia pi aggressiva e / o ricovero ospedaliero oltre le 24 h )  . 
 se non accompagnate a sintomatologia clinica , le fughe extra - vertebrali di cemento non sono state considerate complicanze ; pertanto , per la loro valutazione statistica , tutte le fughe extra - vertebrali di cemento acrilico , indipendentemente dalla loro entit moderata o severa , sono state classificate per sede : paravertebrale , intradiscale , epidurale , foraminale , vascolare . le recidive sono state suddivise in cedimenti osteoporotici o localizzazioni secondarie comparsi in altre vertebre dorso - lombari dopo vpp . 126 radiol med ( 2008 ) 113 : 114133 table 2 results of the clinical evaluation . 
mean values with standard deviation ( ) of the three clinical evaluation score systems [ visual analogue scale ( vas ) , functional mobility , analgesic use ] observed before percutaneous vertebroplasty ( pre - pvp ) and after treatment ( post - pvp ) are shown for the whole series ( 106 ) , for patients with osteoporosis ( 67 ) and for those with metastases ( 39 )  . 
sono riportate le medie dei punteggi con le deviazioni standard ( ) relative alle tre scale di valutazione clinica ( vas ; autonomia motoria ; terapia farmacologica antalgica ) rilevate prima ( pre - vpp ) e dopo ( post - vpp ) il trattamento , nella serie totale dei pazienti ( 106 ) , nei pazienti con osteoporosi ( 67 ) , nei pazienti con metastasi ( 39 )  . 
the results of the assessment of pain , functional mobility and analgesic use before and after pvp , in the whole patient series ( 106 ) , in those with osteoporosis ( 67 ) and in those with metastases ( 39 ) are summarised in table 2 . 
statistical analysis indicated a significant improvement ( p < 0.001 ) in pain , functional mobility i dati , raccolti su un database , sono stati elaborati per la serie complessiva e distinguendo i due gruppi di patologie ( osteoporosi ; metastasi )  . 
le valutazioni statistiche sono state effettuate dal fisico sanitario ( gb ) utilizzando il test t di student per dati non appaiati per ricavare il p - value fra due serie di valori medi . risultati tutti i pazienti nei quali la selezione clinica e i risultati dellimaging hanno confermato le condizioni per effettuare la vpp , sono stati sottoposti allintervento per un totale di 182 vertebre trattate . 
per ciascun paziente in una singola procedura sono state trattate da un minimo di una a un massimo di quattro vertebre con una media di 1 , 7 vertebre / paziente . 
il tempo medio totale per il trattamento di un paziente stato di 57 , 520 min ( range : 21 min per una vertebra , 128 min per quattro vertebre ) ; il tempo medio per il trattamento di una singola vertebra stato lievemente superiore nelle metastasi ( 35 , 5 min ) rispetto ai cedimenti osteoporotici ( 31 , 6 min )  . 
 per quanto riguarda la risposta clinica , in 104 pazienti ( 98% ) la riduzione del dolore entro le 24 h dal trattamento stata significativa o completa ; 2 pazienti affetti da metastasi , radiol med ( 2008 ) 113 : 114133 fig . 
three groups of patients are distinguished on the basis of the interval ( in months ) between pvp and completion of the second questionnaire ( range 01 months 52 patients , range 13 months 32 patients , range > 3 months 22 patients )  . 
nel grafico sono riportati i valori medi del punteggio vas prima ( pre - vpp ) e dopo ( post - vpp ) trattamento , con i rispettivi intervalli di confidenza . 
vengono distinti tre gruppi di pazienti a seconda dellintervallo ( in mesi ) fra vpp e compilazione del secondo questionario ( range 01 mese : 52 pazienti ; range 13 mesi : 32 pazienti ; range > 3 mesi : 22 pazienti )  . 
il p value calcolato dal confronto delle serie dei valori di vas pree post - vpp < 0 , 001 nei tre gruppi di pazienti . and analgesic use after pvp . 
in order of frequency , the leaks occurred in veins of the perivertebral ( 33 ) , epidural ( 17 ) , intradiscal ( 17 ) , paravertebral soft tissue ( 10 ) , and foraminal ( 3 ) plexuses . 
intradiscal leakages predominated ( 16 ) in patients with osteoporosis , whereas venous ( 23 ) and epidural ( 13 ) leakages were more frequent in patients with metastasis . following pvp , in osteoporotic patients receiving antiboneresorption agents , recurrences of structural collapse in vertebrae other than those treated were identified in eight cases ( 11.9% ) , half of them symptomatic . 
i risultati relativi alle scale di valutazione del dolore , dellautonomia motoria e della terapia antalgica farmacologia prima e dopo vpp , nella serie totale dei pazienti sottoposta a follow - up ( 106 ) , nei pazienti con osteoporosi ( 67 ) e in quelli con metastasi ( 39 ) sono riassunti nella tabella 2 . 
 per quanto riguarda le complicanze , nella nostra esperienza 3 sono risultate gravi ( 2 , 8% ) in quanto hanno richiesto trattamento e ricovero ospedaliero di 3 gg dopo la vpp : 1 pneumotorace nel corso di un approccio inter - costo - trasversario che ha richiesto apposizione di drenaggio pleurico , 2 fughe extra - vertebrali rispettivamente in sede epidurale e foraminale con sintomatologia clinica che ha richiesto trattamento farmacologico e periodo di osservazione con risoluzione della sintomatologia , senza necessit di intervento chirurgico . 
le complicanze lievi che hanno richiesto periodo di osservazione di 24 h dopo la vpp sono state 2 ( 1 , 8% ) , rappresentate da piccole embolie polmonari di cemento 128 radiol med ( 2008 ) 113 : 114133 months ( 2 )  . 
more recently , pvp has been considered effective not only for pain relief but also for augmenting vertebral height as an alternative to kyphoplasty [ 15 ]  . among the selection criteria adopted , concordance of the clinical assessment ( pain site ) and imaging findings ( structural alteration level ) is the most important indication [ 3 , 4 , 7 ]  . 
osteolysis of the posterior wall and / or pedicles with involvement of the epidural tissue has recently been considered a relative contraindication for pvp , as some authors [ 20 , 21 ] have reported good results in the treatment of vertebral malignancies even in the presence of these alterations . in our personal experience , patients were selected in a multidisciplinary manner with two ( clinical and imaging ) selection levels and a single coordinator ( the internist ) who supervised the collection of questionnaires before and after pvp . all pvp procedures were conducted under ct guidance . in particular , the first 135 pvp ( 74% ) were performed with ct in combination with radiofluoroscopy , as this was believed to be safer and more precise compared with radiofluoroscopic guidance alone , as suggested by previous reports [ 3 , 22 , 23 ]  . 
le fughe si sono manifestate in ordine di frequenza in sede vascolare venosa nei plessi perivertebrali ( 33 ) , epidurale ( 17 ) , intra - discale ( 17 ) , paravertebrale nelle parti molli ( 10 ) , foraminale ( 3 )  . 
nei pazienti affetti da osteoporosi le fughe sono risultate prevalenti in sede intra - discale ( 16 ) , mentre nei pazienti con metastasi sono prevalse in sede vascolare venosa ( 23 ) ed epidurale ( 13 )  . dopo la vpp , nei pazienti osteoporotici in terapia con farmaci ad effetto anti - riassorbitivo osseo , le recidive di cedimento strutturale in altre vertebre diverse da quelle gi trattate sono state rilevate in 8 pazienti ( 11 , 9% ) , la met delle quali sintomatica ; le recidive si sono verificate entro 6 mesi ( 2 ) , entro 12 mesi ( 4 ) e oltre 12 mesi ( 2 )  . 
seguendo questa indicazione , sono stati trattati in prevalenza i cedimenti osteoporotici ( 63 , 2% ) , rispetto ai coinvolgimenti neoplastici secondari a carcinomi ( 33% ) o a mieloma ( 3 , 8% )  . 
pi recentemente la vpp viene ritenuta efficace non solo per il trattamento del dolore , ma anche per aumentare laltezza del soma vertebrale , in alternativa alla cifoplastica [ 15 ]  . fra i criteri di selezione da noi utilizzati la concordanza tra il quadro clinico ( sede del dolore ) e quello imaging ( livello somatico dellalterazione strutturale ) rappresenta lindicazione pi importante [ 3 , 4 , 7 ]  . 
nella sezione sagittale rm ( a ) ottenuta con sequenza turbo spin echo t1 dipendente e sagittale tc ( b ) ottenuta con tecnica multi planar reformatting ( mpr ) , effettuate a distanza di 4 mesi dalla vpp del soma di d11 ( freccia vuota ) , comparsa di nuova metastasi osteolitica al soma di d8 ( freccia ) , con interruzione del muro posteriore che controindica leffettuazione di nuova vpp . ered safe and effective in guiding percutaneous procedures since 1996 [ 2427 ]  . 
da ricordare che la lisi del muro posteriore e / o dei peduncoli vertebrali con coinvolgimento del tessuto epidurale sono state recentemente considerate contro - indicazioni relative alla effettuazione della vpp , in quanto alcuni autori [ 20 , 21 ] hanno riportato buoni risultati nel trattamento di lesioni vertebrali maligne anche in presenza di queste alterazioni . nella esperienza personale , la selezione dei pazienti stata effettuata in modo multidisciplinare seguendo due livelli rispettivamente clinico e imaging , con un unico referente ( linternista ) che ha coordinato la raccolta dei questionari prima e dopo il trattamento . la totalit delle vpp da noi effettuate stata condotta con guida imaging tcassistita . 
in particolare , inizialmente 135 vpp ( 74% ) sono state guidate con impiego combinato della tc e della radio - fluoroscopia ritenendolo pi sicuro e preciso rispetto alla sola guida radio - fluoroscopica in accordo con altri autori [ 3 , 22 , 23 ]  . 
successivamente , disponendo di una tc - multistrato dotata della strumentazione per tc - scopia , le restanti 47 vpp ( 26% ) sono state guidate esclusivamente con la tc . 
gli accessi sono stati in prevalenza unilaterali ( 97 , 8% ) in quanto meno invasivi e ugualmente efficaci per la distribuzione del cemento e per il suo effetto stabilizzante sul soma vertebrale trattato [ 2830 ]  . 
le vie di introduzione dellago preferite sono state trans - peduncolare ( 61% ) prevalentemente a livello lombare ed inter - costo - trasversaria ( 30 , 7% ) prevalentemente a livello dorsale . 
 la iniezione del cemento rappresenta il passaggio pi importante della procedura e richede il monitoraggio in tempo reale con radio - fluoroscopia o tc - scopia al fine di controllare la distribuzione del cemento nel soma vertebrale e di identificare le eventuali fughe extra - vertebrali . 
per tale motivo , le casistiche pi recenti che hanno utilizzato la guida tc riportano incidenza maggiore di piccole fughe asintomatiche extra - vertebrali di cemento [ 13 , 26 , 31 ]  . 
 leffetto meccanico del cemento si svolge mediante la stabilizzazione delle microfratture del soma vertebrale e ha il 130 radiol med ( 2008 ) 113 : 114133 cal characteristics and dorsolumbar vertebral alteration proved to be more reliable . 
the approaches used were predominantly unilateral ( 97.8% ) , as these are less invasive and equally effective for distribution of cement and its stabilizing effect on the vertebral body [ 2830 ]  . 
 cement injection is the most important step in the procedure and requires real - time monitoring by radiofluoroscopy or ct fluoroscopy to check cement distribution within the vertebra and identify possible leakages . 
for this reason , the more recent studies carried out with ct guidance have reported a higher incidence of small , asymptomatic cement leakages [ 13 , 26 , 31 ]  . 
 the mechanical effect of cement is to stabilize vertebral microfractures and , more importantly , to relieve pain [ 32 ]  . as there is no correlation between the amount of acrylic cement injected and symptoms remission [ 4 , 10 , 19 ] , we aimed to achieve a good central distribution of cement within the vertebral body , taking care to avoid leakages , above all in the posterior direction . 
therefore , the mean quantity of cement used in each vertebra was 5.7 cc , similar to the amount used by others ( 6 cc ) [ 8 ] and within the recommended range ( 2cc9cc ) [ 19 ]  . 
 the use of ct with or without radiofluoroscopy allowed easier targeting of the vertebral body and enabled multiplanar evaluation of the vertebra before and after pvp in a single session lasting on average 57 min , with a mean time per vertebra only slightly longer for metastases compared with osteoporotic collapse . with regard to clinical response , because cement polymerization and consequently vertebral stabilization occurs within minutes , pain reduction was recorded in 98% of patients within 24 h of treatment , to their general satisfaction . in the literature , the results of pvp on pain reduction have been presented in widely differing series in terms of sample size , lesion type , results analysis and follow - up duration , such that comparisons are impossible . 
nonetheless , in studies on the treatment of metastases , pain disappearance or reduction was reported in 75%82% of patients [ 20 , 21 , 33 ] , whereas in the treatment of osteoporotic collapse , it was reported in 73%97% [ 7 , 8 , 22 , 29 ]  . 
in mixed series including both metastases and osteoporosis more similar to our series pain disappearance or reduction was reported in 75%100% of cases within 1 week [ 3 , 14 , 23 , 3236 ]  . 
in our study , clinical results were based on the comparison between data collected before pvp and at the first follow - up visit after pvp , with a mean interval of 1.7 months from the procedure . 
poich non esiste correlazione fra la quantit di cemento acrilico iniettata e la remissione della sintomatologia [ 4 , 10 , 19 ] , si cercato di ottenere una buona distribuzione centrale del cemento nel soma vertebrale , evitando le fughe soprattutto con direttrice posteriore . 
pertanto , la quantit media di cemento acrilico iniettato in ciascuna vertebra stata di 5 , 7 cc , simile a quella ( 6 cc ) riportata da altri autori [ 8 ] e comunque entro il range ( 2 cc9 cc ) indicato in letteratura [ 19 ]  . 
 limpiego della tc in associazione o meno alla radiofluoroscopia ha agevolato le fasi di centratura del soma vertebrale e consentito la valutazione multiplanare della vertebra prima e dopo la vpp , in ununica seduta la cui durata media stata di circa 57 min , con un tempo medio per il trattamento di una singola vertebra lievemente superiore nelle metastasi rispetto ai cedimenti osteoporotici . per quanto riguarda la risposta clinica alla vpp , poich la stabilizzazione del corpo vertebrale avviene in pochi minuti per il rapido consolidarsi del cemento , la riduzione del dolore nel punto trattato stata riscontrata nel 98% entro le 24 h dal trattamento ; ci ha determinato soddisfazione generale nei nostri pazienti . 
nella letteratura i risultati della vpp sul dolore sono presentati in casistiche molto varie per numero di pazienti , tipologia di lesioni trattate , analisi dei risultati e durata del follow - up , tali da inficiare la comparazione dei dati tra loro . 
comunque , nelle serie riguardanti il trattamento di metastasi la scomparsa / riduzione del dolore stata rilevata nel 75%82% dei pazienti [ 20 , 21 , 33 ] , mentre in quelle relative al trattamento di cedimenti osteoporotici stata rilevata nel 73%97% [ 7 , 8 , 22 , 29 ]  . 
nelle casistiche miste per trattamento di pazienti con metastasi e osteoporosi pi simili alla nostra la scomparsa / riduzione del dolore stata rilevata nel 75%100% nella prima settimana [ 3 , 14 , 23 , 3236 ]  . 
nel nostro studio i risultati clinici si riferiscono alla comparazione dei dati raccolti nella fase di selezione e nella prima visita di controllo dopo vpp con un intervallo medio di 1 , 7 mesi dalla procedura . 
anche la riduzione delluso di farmaci analgesici e il miglioramento dellautonomia motoria rilevati nel nostro studio , conferma come la vpp abbia in assoluto giovato sulla qualit della vita , con verosimile riduzione della spesa sanitaria . 
peraltro , da ricordare che il periodo complessivo del follow - up stato breve , soprattutto nei pazienti oncologici ( 3 , 39 mesi ) ; ci , anche nella nostra esperienza come in quella di altri autori [ 3 , 8 , 14 , 2023 , 29 , 3236 ] , rappresenta il punto critico . come riportato recentemente [ 4 ] auspicabile vengano effettuati studi prospettici su trials controllati che confermino i risultati riscontrati nel breve periodo dopo la vpp , riguardanti non solo la sintomatologia e le eventuali recidive , ma anche il destino del cemento introdotto nella vertebra . radiol med ( 2008 ) 113 : 114133 treatment , and the results remained constant over time ( fig . 8 ) , confirming that the efficacy of pvp is long lasting . 
even reduction in analgesic use and improvement in functional mobility observed in our study confirmed that pvp had an overall positive effect on quality of life , with a probable reduction of health care costs . 
as recently reported [ 4 ] , prospective controlled trials are required to validate the long - term outcomes of pvp with regard not only to symptom relief and recurrences but to the fate of the cement introduced into the vertebra . if patient selection is accurate and the procedure technique is meticulously followed , complications are rare [ 37 ] and more common in metastases ( 5% ) than in osteoporotic collapse ( 1% )  . 
in our opinion , ct guidance helped limit the incidence of severe ( 2.8% ) and mild ( 1.8% ) complications reported in other studies [ 19 , 3438 ] , such as spinal cord or nerve root compression due to excessive epidural and / or foraminal leakage of the injected cement , pulmonary embolism due to venous leakage , haematomas along the needle track , costal or pedicular fractures and pneumothorax . 
infections are avoided by antibiotic prophylaxis in immunocompromised patients , accurate sterilization of the surgical field , and a rigourously aseptic technique [ 19 , 16 , 37 ]  . 
the reported incidence of leakages varies in relation to the number and type of lesions treated and ranges from 9% to 88% [ 3 , 8 , 13 , 23 , 31 , 33 , 36 ]  . 
in osteoporotic patients , the prevalence of intradiscal leaks is due to the frequent formation of cavities or clefts in the disc endplate as a result of structural collapse and does not alter spine biomechanics or increase the risk of disc degeneration [ 37 , 39 , 40 ]  . 
anterior leaks follow the anastomoses of the basivertebral vein in the perivertebral venous plexuses , which empty into the caval system , with a resulting risk of pulmonary embolisposterior leaks occur in the epidural and periradicular venous plexuses where cement accumulation may become symptomatic owing to spinal cord or nerve root involvement . 
in general , extravertebral leaks rarely become symptomatic if care is taken to interrupt the injection as soon as the leakage is detected on the monitor and allowing the cement to harden for a few seconds . 
 as reported in the literature [ 41 , 42 ] , fracture recurrences within 1 year following pvp are frequent in osteoporotic patients ( 12.4%21.7% ) and explained by increased stiffse la selezione dei pazienti accurata e se viene rigorosamente rispettata la metodologia della procedura , le complicanze sono rare [ 37 ] , con prevalenza nel trattamento delle metastasi ( 5% ) rispetto ai cedimenti osteoporotici ( 1% )  . nellopinione personale la guida tc ha contribuito a mantenere bassa lincidenza di complicanze gravi ( 2 , 8% ) e lievi ( 1 , 8% ) , riscontrate in altre esperienze riportate in letteratura [ 19 , 3438 ] quali le compressioni mielo - radicolari da eccessiva fuga epidurale e / o foraminale del cemento acrilico , lembolia polmonare da fuga venosa del cemento acrilico , gli ematomi lungo il tragitto dellago , le fratture costali / peduncolari , il pneumotorace . 
le infezioni vengono evitate grazie alla somministrazione preventiva di antibiotici nei pazienti a rischio per immunodeficienza , alla accurata disinfezione del campo di intervento , al rigoroso mantenimento della asepsi durante tutta la procedura [ 19 , 16 , 37 ]  . 
in nessuno dei nostri pazienti stata riscontrata spondilodiscite infettiva dopo vpp , peraltro segnalata sporadicamente in letteratura [ 4 , 37 ]  . anche nella nostra esperienza le fughe extra - vertebrali del cemento acrilico asintomatiche sono risultate frequenti ( 43 , 9% )  . 
in letteratura la incidenza variabile in rapporto al numero e al tipo di lesioni trattate , compresa fra il 9% e il 88% [ 3 , 8 , 13 , 23 , 31 , 33 , 36 ]  . 
nei pazienti osteoporotici , la prevalenza delle fughe in sede intra - discale dovuta alla frequente discontinuit della limitante osteo - discale in seguito al cedimento strutturale e non altera la biodinamica del rachide n aumenta il rischio di degenerazione discale [ 37 , 39 , 40 ]  . 
la prevalenza delle fughe in sede vascolare venosa ed epidurale nei pazienti con metastasi dovuta alla maggior vascolarizzazione delle lesioni maligne per i fenomeni di neo - angiogenesi [ 34 ]  . 
la via di fuga segue le anastomosi della vena basi - vertebrale in sede anteriore nei plessi perivertebrali che si scaricano nel sistema cavale con rischio di embolia polmonare ; in sede posteriore , la fuga avviene nei plessi venosi epidurali e peri - radicolari dove laccumulo del cemento pu divenire sintomatico per il coinvolgimento delle strutture mielo - radicolari . 
in generale , difficilmente le fughe extra - vertebrali di cemento divengono sintomatiche se si ha lavvertenza di interrompere la iniezione del cemento lasciandolo consolidare per poche decine di secondi non appena la fuga viene riconosciuta sul monitor . come riporta la letteratura [ 41 , 42 ] , le recidive di frattura nei pazienti osteoporotici entro lanno dopo la vpp sono frequenti ( 12 , 4%21 , 7% ) e giustificate dallincremento della rigidit del soma trattato rispetto a quelli contigui , alla progressione della osteoporosi e al miglioramento dellattivit motoria con aumento del rischio di nuova frattura . 
pur tenendo conto del follow - up breve , il nostro studio ha fatto rilevare recidiva di frattura nel 11 , 9% 132 radiol med ( 2008 ) 113 : 114133 ness of the vertebral body with respect to adjacent ones , osteoporosis progression and increased mobility that predisposes the patients to a higher risk of new fractures . 
despite the short follow - up period , we found fracture recurrences in 11.9% of osteoporotic patients and new symptomatic vertebral metastases in 5.1% of oncological patients ; most recurrences occurred within 1 year following treatment . 
 conclusioni dei pazienti osteoporotici e di nuova localizzazione secondaria vertebrale sintomatica nel 5 , 1% dei pazienti oncologici ; la maggior parte delle recidive si manifestata entro lanno dal trattamento . 
 conclusions in conclusion , our experience suggests that patient selection should be preferably carried out by a multidisciplinary team to ensure an optimal level of accuracy that only the combination of specialist competence in the clinical and imaging fields can guarantee . 
therefore , our selection process involves an oncologist , an orthopaedic surgeon , a radiologist and an internist to coordinate diagnostic investigations and collect the data before and after pvp . 
in our opinion , performing pvp in a radiology department equipped with the best imageguiding technology ( radiofluoroscopy and / or ct ) and where the competence of other specialists as well as the radiologist can come together represents the optimal solution to ensure the best chances of success and reduce the risk of complications . in conclusione , la nostra esperienza suggerisce che la selezione dei pazienti va affrontata preferibilmente in chiave multidisciplinare al fine di ottenere un buon livello di accuratezza che solo le competenze specialistiche garantiscono nei rispettivi campi di interesse clinico e imaging . 
pertanto , il nostro modello di selezione coinvolge i profili professionali delloncologo , dellortopedico , del radiologo e dellinternista , questultimo dedicato al coordinamento degli accertamenti diagnostici e alla raccolta dei dati prima e dopo la vpp . 
limpiego della guida tc nella effettuazione della vpp rende pi sicure e precise le manovre di centratura e di iniezione del cemento , riducendo i rischi di complicanze ; ci assume importanza particolare quando un team inizia la propria esperienza con questa procedura e deve ridurre al minimo i rischi e gli inconvenienti legati alla curva di apprendimento . 
leffettuazione della procedura in anestesia locale nella sala tc consente di effettuare tutte le valutazioni pree post - vpp senza la necessit di dover spostare il paziente da una sala allaltra ; in tal modo , il tempo medio totale della procedura con i relativi controlli pi contenuto ( circa 57 min nellesperienza personale )  . 
rasori 10 , 43100 parma , italy 2dipartimento di scienze radiologiche , sezione di diagnostica per immagini , ospedale maggiore - universit degli studi di parma , via gramsci 14 , 43100 parma correspondence to : a . 
in all subjects , hrct scanning , at suspended end - expiratory volume , was performed at rest and during ventilation with 6 and 12 cmh2o by nasal insufflation with continuous positive airway pressure ( ncpap ) , both at baseline and after inhalation of 200 g oxitropium bromide metered dose inhaler ( mdi )  . 
abbiamo studiato 7 pazienti ( 2 maschi , range di et : 3669 anni ) con asma cronica in condizioni cliniche stabili ( fev1 range : 30%87% del valore predetto ; fev1 / fvc range : 48%75% del valore predetto ) e 6 controlli sani ( 3 maschi , range di et : 2950 anni )  . 
in tutti i soggetti sono state effettuate scansioni hrct a fine espirazione a riposo e durante ventilazione mediante cpap con 6 e 12 cmh2o , sia in condizioni basali , sia dopo inalazione di 200 g di oxitropio bromuro mdi . 
nei pazienti asmatici , linsufflazione con la pressione di 12 cmh2o ha cambiato in modo significativo il diametro di base del lume ( 3 , 30 , 7 mm vs 3 , 80 , 6 mm ; p < 0 . , 01 ) e il diametro esterno ( 6 , 20 , 9 mm vs 6 , 70 , 8 mm ; p < 0 , 05 ) mentre nei controlli sani , linsufflazione con la pressione di 6 cmh2o e di 12 cmh2o ha prodotto cambiamenti significativi a carico del diametro basale del lume ( 4 , 01 , 6 mm vs 4 , 81 , 6 mm e 4 , 71 , 7 mm ; p < 0 , 01 )  . nei pazienti asmatici , linalazione di oxitropio bromuro ha cambiato significativamente il diametro di base del lume ( 3 , 30 , 7 mm vs 4 , 40 , 6 mm ; p < 0 , 05 ) mentre radiol med ( 2008 ) 113 : 4355 the application of 6 or 12 cmh2o insufflation did not modify any bronchial diameters . 
nei controlli sani linalazione di oxitropio bromuro ha modificato in modo significativo il diametro di base del lume ( 4 , 01 , 6 mm vs 5 , 01 , 5 mm ; p < 0 , 05 )  . 
i nostri risultati dimostrano che nei pazienti asmatici il grado di distensibilit delle vie aeree , misurato mediante hrct , pu essere diverso se comparato a quello dei controlli sani . 
la hrtc pu fornire informazioni utili sulla distensibilit delle vie aeree . parole chiave asma imaging del torace tc ad alta risoluzione introduction introduzione asthma is an inflammatory lung disease characterised by increased airway reactivity to various stimuli and airflow obstruction that is at least partially reversible [ 1 ]  . 
whereas acute inflammation is a beneficial nonspecific response of tissues to injury that generally leads to repair and restoration of normal structure and function , asthma represents a chronic inflammatory process followed by healing , the end result of which is characteristically an altered structure referred to as airway remodelling [ 2 ]  . 
the subgroup of asthmatic subjects with irreversible airflow obstruction is of importance because these subjects experience considerable morbidity and account for a high percentage of asthma - related health costs [ 4 ]  . 
early markers of airway remodelling might be important for managing asthmatic patients . we used high - resolution computed tomography ( hrct ) to examine the ability of mechanical pressures via nasal insufflation to distend the airways of subjects with chronic asthma , who were compared with healthy subjects at baseline and after reducing airway tone with an anticholinergic drug . 
 materials and methods six healthy controls and seven individuals with asthma were lasma una malattia infiammatoria dei polmoni che caratterizzata da uniper - reattivit delle vie aeree verso vari stimoli e da unostruzione al flusso parzialmente reversibile [ 1 ]  . 
mentre linfiammazione acuta una risposta non specifica dei tessuti che generalmente conduce alla riparazione strutturale e al ripristino funzionale nei confronti di un meccanismo lesivo , lasma rappresenta un processo infiammatorio cronico delle vie aeree il cui risultato finale caratteristicamente unalterazione strutturale definita come rimodellamento [ 2 ]  . 
importante tenere in considerazione il sottogruppo di pazienti asmatici con ostruzione irreversibile a carico delle vie aeree , perch questi pazienti sono affetti da una considerevole morbilit e sono rappresentano unalta percentuale dei costi in termini di salute dovuti allasma [ 4 ]  . 
marcatori precoci di rimodellamento delle vie aeree potrebbero essere importanti per il management dei pazienti asmatici . in questo studio abbiamo utilizzato la tc ad alta risoluzione ( hrct ) per esaminare la capacit delle pressioni meccaniche , attraverso linsufflazione nasale , di distendere le vie aeree dei soggetti affetti da asma cronica rispetto a controlli sani in condizioni basali e dopo riduzione del tono delle vie aeree mediante un farmaco anti - colinergico . radiol med ( 2008 ) 113 : 4355 enrolled in the study . 
the seven patients affected by chronic asthma ( two men , age range 3669 years ) had a diagnosis of asthma according to the american thoracic society criteria [ 5 ] for at least 5 years , and they had no acute exacerbation within the preceding 3 months . 
 spirometry spirometry was measured by a flow - sensing spirometer connected to a computer for data analysis ( koko spirometer , ferraris respiratory , louisville , co , us )  . 
each time , fev1 values were recorded as the highest of three readings made at 1min intervals . ct and airway analysis all patients underwent thin - section ct examination of the entire thorax using a 16 - slice scanner ( sensation 16 - siemens medical solutions , foreheim , germany ) without i.v. 
injection of contrast mediuthe scanning parameters were : 120 kvp , 100 mas , rotation time 0.5 s , feed / rotation 18 mm , the smallest possible field of view ( fov ) covering both lungs , bone filter , collimation 0.75 mm with 1 - mm reconstruction . 
ai sette pazienti affetti da asma cronico ( 2 maschi , range det : 3669 anni ) era stata fatta diagnosi di asma , in accordo con i criteri della american thoracic society [ 5 ] , da almeno 5 anni ed essi non avevano presentato riesacerbazioni nei tre mesi antecedenti . 
anche i pazienti hanno rilasciato il loro consenso informato allo studio . spirometria la spirometria stata effettuata mediante un respiratore connesso ad un computer per lanalisi dei dati ( koko spirometer , ferraris respiratory , louisville , usa )  . 
sono stati misurati i valori di base del fev1 e dopo 15 minuti di inalazione di 200 g di oxitropio bromuro . ogni volta , i valori di fev1 sono stati registrati come il pi alto valore delle tre letture fatte ad intervalli di un minuto . 
 tc del torace e protocollo di studio tutti i pazienti sono stati sottoposti a scansioni del torace con tc a strato sottile mediante tc multidetettore a 16 strati ( sensation 16 - siemens medical solution , foreheim , germania ) senza somministrazione ev di mezzo di contrasto . 
i parametri di scansione sono stati : 120 kvp , 100 mas , tempo di rotazione di 0 , 5 s , feed / rotation pari a 18 mm , il pi piccolo campo di vista possibile ( fov ) in grado di coprire entrambi i polmoni , un filtro per losso , una collimazione pari a 0 , 75 mm con ricostruzioni di 1 mm . dopo alcuni respiri in condizioni di stabilit , i soggetti sono stati chiamati ad effettuare una inspirazione massimale seguita immediatamente dallespirazione . 
2a - c le scansioni tc dimostrano la tecnica di misurazione del diametro bronchiale del bronco segmentale apicale del lobo superiore destro nei soggetti sani a riposo ( a ) , dopo cpap con 6 cmh2o ( b ) e dopo cpap con 12 cmh2o ( c ) , prima della somministrazione di oxitropio bromuro . ated all ct scans , measuring both internal and external diameters of the apical bronchus of the right upper lobe . 
questi dati sono stati utilizzati per calcolare laccordo interosservatore . la media dei valori misurati dai due osservatori stata considerata come valore di riferimento finale delle misurazioni . analisi statistica i valori sono stati rappresentati come mediadeviazione standard ( sd )  . 
le differenze fra i dati di base e i dati post - inradiol med ( 2008 ) 113 : 4355 table 1 characteristics of asthmatic subjects and healthy nonsmoking volunteers asthmatic subjects ( n = 7 ) healthy subjects ( n = 6 ) tervento sono state esaminate attraverso lanalisi della varianza e il test di comparazione multipla di dunnett . 
stato considerato significativo un valore di p < 0 , 05 . age ( years ) gender ( f / m ) disease duration ( years ) fev1 ( % predicted ) fev1 / fvc ( % ) 4711 6718 * 6710 * 378 11115 1045 risultati fev1 , forced expiratory volume in the first second ; fvc , forced vital capacity . 
values are expressed as meanstandard deviation ; * p < 0.05 tabella 1 caratteristiche dei soggetti asmatici e dei volontari sani non fumatori pazienti asmatici ( n = 7 ) soggetti sani ( n = 6 ) et ( anni ) sesso ( f / m ) durata malattia ( anni ) fev1 ( %vp ) fev1 / fvc ( % ) 4711 6718 * 6710 * 378 11115 1045 fev1 , volume di aria espirata nel primo secondo ; fvc , capacit vitale forzata . 
i valori sono stati espressi come mediasd ; * p < 0 , 05 the baseline fev1 and fev1 / forced vital capacity ( fvc ) among the two groups , as expected from our stratification ( table 1 )  . 
after administration of the bronchodilator , we found a significant difference in the change of both baseline fev1 and fev1 / fvc in asthmatic patients only ( p < 0.05 , table 2 )  . le caratteristiche dei soggetti sono mostrate in tabella 1 . 
dopo la somministrazione del broncodilatatore , abbiamo riscontrato un cambiamento significativo dei valori basali di fev1 e fev1 / fvc solo nei soggetti asmatici ( p < 0 , 05 , tabella 2 )  . laccordo interosservatore nelle misurazioni ct stato buono sia per il diametro interno ( ri = 0 , 67 ) che per quello esterno ( ri = 0 , 75 )  . 
la somministrazione di una pressione di 12 cmh2o ha modificato significativamente entrambi i diametri bronchiali nei pazienti asmatici , mentre nei controlli sani cambiato in modo significativo solo il diametro interno ( tabella 3 )  . 
we show that only administration of 12 cmh2o pressure modified airway diameters in asthmatic patients , but positive pressures did not further modify airway diameters after the addition of the bronchodilator . 
by contrast , in healthy subjects , administration of both 6 cmh2o and 12 cmh2o positive pressure , with and without oxitropium bromide inhalation , significantly changed airway diameters ( tables 4 and 5 )  . 
usando questo metodo innovativo , essenzialmente basato sullinsufflazione nasale a pressione positiva continua , abbiamo rilevato che la distensibilit delle vie aeree nei pazienti con asma cronico risultata diversa se paragonata con quella dei soggetti sani . 
abbiamo mostrato che nei pazienti asmatici solo la somministrazione di una pressione di 12 cmh2o ha modificato il calibro delle vie aeree , ma le pressioni positive non hanno modificato i diametri delle vie aeree dopo laggiunta del broncodilatatore . 
al contrario , nei soggetti sani sia la somministrazione di una pressione di 6 cmh2o sia di 12 cmh2o , con e senza linalazione di oxitropio bromuro , ha modificato significativamente i diametri delle vie aeree ( tabella 4 e 5 )  . 
questi reperti indicavano che le vie aeree dei pazienti con asma cronica erano risultate pi rigide di quelle dei soggetti sani . esistono diversi cambiamenti strutturali , tutti inclusi nel termine di rimodellamento delle vie aeree . 
lispessimento della membrana basale reticolare , lipertrofia del muscolo liscio e la fibrosi sub - epiteliale sono i markers probabilmente pi utili e rilevanti [ 6 , 7 ]  . 
6 valori individuali e valore medio del lume bronchiale del bronco segmentale apicale del lobo superiore destro a riposo e dopo insufflazione di una pressione di 6 cmh2o e di 12 cmh2o nei pazienti asmatici . post 6 cmh2o post 12 cmh2o after oxitropium post 6 cmh2o post 12 cmh2o p < 0.01 condizioni basali post 6 cmh2o post 12 cmh2o dopo oxitropio post 6 cmh2o post 12 cmh2o radiol med ( 2008 ) 113 : 4355 table 4 values of external and lumen diameters at baseline and after oxitropium bromide in asthmatic subjects pre and post 6 and 12 cmh2o pressure insufflation study population baseline after oxitropium external diameter lumen diameter external diameter lumen diameter gender pre post 6 post 12 post 6 post 12 post 6 post 12 post 6 post 12 asthmatic subjects mean standard deviation soggetti asmatici pz 1 pz 2 pz 3 pz 4 pz 5 pz 6 pz 7 media tabella 4 valori del diametro esterno e del diametro interno in condizioni basali e dopo oxitropio bromuro nei soggetti asmatici pree post - insufflazione a pressione positiva con 6 e 12 cmh2o studio sulla popolazione condizioni basali dopo oxitropio diametro esterno diametro interno diametro esterno diametro interno sesso post 6 post 12 post 6 post 12 post 6 post 12 post 6 post 12 a number of structural changes are grouped together under the umbrella term airway remodelling . 
it has been demonstrated in dogs that even relatively high levels of positive end - expiratory pressures cannot always prevent airway closure when there is sufficient stimulation of the airway smooth muscle [ 9 ]  . 
stato dimostrato che , anche nei cani , livelli relativamente alti di pressioni positive di fine espirazione non possono sempre prevenire la chiusura delle vie aeree in presenza di una sufficiente stimolazione della muscolatura liscia delle vie aeree [ 9 ]  . 
inducendo il rilassamento della muscolatura liscia ( mediante un broncodilatatore anti - colinergico , come loxitropio bromuro ) , abbiamo riscontrato che la somministrazione di pressioni positive non incrementa ulteriormente la dilatazione bronchiale nei soggetti asmatici in paragone con i controlli . 
kasahara and colleagues reported a significant negative correlation between postbronchodilator fev1 and both bronchial - wall thickening on hrct and reticular basement membrane thickness in endobronchial biopsy [ 10 ]  . 
however , other cross - sectional studies failed to demonstrate an association between fev1 and either bronchial - wall thickening or reticular basement membrane thickness [ 4 , 11 , 12 ]  . airway diameters measured on axial images depend on the lung volume and angle between the airway central axis and the plane of section [ 13 ]  . 
 [ 10 ] hanno riportato una significativa correlazione negativa fra i valori di fev1 dopo broncodilatatore , lispessimento della parete bronchiale alla hrct e lispessimento della membrana basale reticolare alla biopsia endobronchiale . 
comunque altri studi trasversali non sono stati in grado di dimostrare unassociazione fra fev1 , lispessimento della parete bronchiale e lo spessore della membrana basale reticolare [ 4 , 11 , 12 ]  . 
 i diametri delle vie aeree misurati sul piano assiale dipendono dal volume polmonare e dallangolo compreso fra lasse centrale della via aerea ed il piano di sezione [ 13 ]  . abbiamo estratto le misure dei diametri da quelle del tronco del bronco apicale del lobo superiore destro , il quale viene di solito sezionato nelle scansioni assiali ed facilmente identificato alla tc . 
il mantenimento di un volume polmonare relativamente costante fra le scansioni hrct un aspetradiol med ( 2008 ) 113 : 4355 surements from the trunk of the apical bronchus of the right upper lobe , which is usually sliced in cross - section and easily identified on ct scans . 
most recent software may overcome some limitations related to the use of two - dimensional planar data for airway analysis , as it can depict a three - dimensional airway skeleton and measure airway luminal and wall areas very precisely at any site in the lungs [ 14 , 15 ]  . 
therefore , we hope that future studies with more advanced techniques can verify our results . however , this study is the first to provide a dynamic measure of the airways obtained by ncpap . 
this is a new method that may have important clinical implications , as hrct might be used to measure dynamic changes in airway diameter in vivo that may be not detectable by conventional global lung measurements . 
anche se non abbiamo fatto uso di una regolare sincronizzazione respiratoria , il monitoraggio delle curve flusso - volume ci ha permesso di ottenere questo risultato con una buona affidabilit . 
la potenziale variabilit interosservatore nella misurazione dei diametri bronchiali mediante calibri elettronici ha portato allo sviluppo di metodi computerizzati per determinare le dimensioni della parete delle vie aeree . anche se abbiamo garantito un adeguato livello di concordanza fra gli osservatori nellanalisi semiquantitativa , lutilizzo di dati planari bidimensionali per lanalisi delle vie aeree presenta tuttavia alcuni limiti . 
molti softwares pi recenti possono superare qualche limite legato alluso di dati planari bidimensionali , dal momento che sono in grado di rappresentare uno scheletro tridimensionale delle vie aeree e misurarne larea endoluminale e larea di parete in maniera molto precisa e a qualsiasi livello dei polmoni [ 14 , 15 ]  . 
dunque , ci auguriamo che ulteriori indagini con tecniche pi avanzate possano verificare i nostri risultati . questo studio comunque il primo a fornire dati sulla misurazione dinamica delle vie aeree , ottenuta attraverso linsufflazione nasale a pressione continua . 
il metodo innovativo e pu avere importanti implicazioni cliniche , visto che la hrct pu essere utilizzata per misurare cambiamenti dinamici del calibro in vivo , che non possono essere individuati attraverso misurazioni convenzionali globali del polmone . 
in 4 / 20 patients , all with wegeners granulomatosis , cxr was negative or demonstrated only nodular opacities ; in two of these cases , ct revealed ground - glass opacities . 
a complete follow - up was available for ten patients : initially , they showed consolidation opacities in 36 / 60 zones , which persisted in 16 / 60 after 7 days and in 11 / 60 after 15 days . 
studio retrospettivo di 23 episodi di ead in 20 pazienti , 17 con eziologia identificata , 3 senza causa specifica , studiati tutti con rx torace e 15 con tc . 
la tc , pi sensibile dellrx nel riconoscere opacit ground - glass , indispensabile in pazienti con possibile ead e quadro rx negativo . parole chiave polmone , emorragia radiografia , toracica polmone , tc radiol med ( 2008 ) 113 : 1628 introduction diffuse alveolar haemorrhage ( dah ) is a rare clinicopathological syndrome characterised by diffuse intra - alveolar bleeding , which may have an insidious chronic course or may present as an acute event in subjects of any age , including children [ 1 , 2 ]  . 
the fundamental pathogenetic mechanisms are deposition of immune complexes formed in the bloodstream or in situ on the vessel endothelium or walls , production of antineutrophil cytoplasmic antibodies ( anca ) and production of antiglomerular basement membrane ( anti - gbm ) antibodies [ 5 ]  . the most frequent histopathological finding ( an almost constant finding in systemic vasculitis ) is pulmonary capillaritis characterised by fibrin thrombi in the interalveolar capillaries and septa , fibrinoid necrosis of capillaries , granulocyte infiltrates , erythrocytes and haemosiderin in the interstitiuin the absence of damage to the alveolar interstitium , there may be mild alveolar haemorrhage ; in the case of recurring haemorrhage , interstitial fibrosis and tissue haemosiderosis may develop [ 6 ]  . 
a less frequent histological pattern is diffuse alveolar damage ( dad ) characterised by interstitial and alveolar oedema , capillary congestion with microthrombi and , above all , intra - alveolar hyaline membranes [ 6 ]  . dah may develop in a number of systemic diseases , as a result of coagulation disorders , inhaled toxins or infections ( table 1 ) , but it may even have no specific cause [ 5 , 6 ]  . 
in the acute phases , it is characterised by the presence of dyspnoea with hypoxaemia , haemoptysis ( in 70% of cases ) and sideropenic anaemia [ 1 ]  . 
anaemia is the most constant finding in patients with pulmonary haemorrhage and is present in virtually all patients with goodpastures syndrome [ 1 ]  . haemoptysis is the most striking symptom and may be present intermittently for weeks before the acute event or , more commonly , it may manifest or worsen dramatically and suddenly over a few days or even hours . 
other symptoms include cough , fever and chest pain . the radiographic pattern of dah is characterised by consolidation or ground - glass alveolar - filling opacities of extremely varying size that are usually bilateral and prevalently distributed in parahilar regions . 
in chronic or recurrent dah , persistent fibrotic interstitial involvement may develop in the later phases [ 4 ]  . introduzione lemorragia alveolare diffusa ( ead ) una rara sindrome clinico - patologica caratterizzata da sanguinamento intraalveolare diffuso , che pu avere un decorso insidioso e cronico o presentarsi come un evento acuto in soggetti di qualsiasi et , compresi pazienti in et pediatrica [ 1 , 2 ]  . 
lead deve essere distinta dallaspirazione alveolare diffusa di sangue proveniente da lesioni focali del polmone ( es . : bronchiettasie , tumori , infezioni ) , che sono di solito radiograficamente individuabili [ 3 , 4 ]  . 
i meccanismi patogenetici fondamentali sono : la precipitazione di immunocomplessi , formati o in circolo o in situ , a livello dellendotelio o delle pareti vasali ; la produzione di anticorpi diretti contro componenti citoplasmatici dei neutrofili ( anca ) ; la produzione di anticorpi anti - membrana basale ( ambg ) [ 5 ]  . 
 il quadro istopatologico pi comune ( pressoch costante in corso di vasculite sistemica ) la capillarite polmonare , caratterizzata da trombi di fibrina nei capillari e nei setti interalveolari , necrosi fibrinoide dei capillari , infiltrati granulocitari , eritrociti ed emosiderina nellinterstizio . 
pi raro il riscontro del pattern istologico del danno alveolare diffuso ( dad ) , caratterizzato da edema interstiziale ed alveolare , congestione capillare con microtrombi e , soprattutto , presenza di membrane ialine intra - alveolari [ 6 ]  . lead pu comparire nel corso di numerose malattie sistemiche , in seguito a disordini coagulativi o inalazione di tossine o infezioni ( tabella 1 ) , ma pu anche rimanere senza una causa specifica [ 5 , 6 ]  . 
lemottisi il sintomo pi eclatante , e pu presentarsi in modo intermittente per settimane prima della presentazione dellevento acuto o , pi spesso , manifestarsi o aggravarsi in maniera drammatica e improvvisa nel corso di pochi giorni o addirittura di alcune ore . 
altri sintomi sono la tosse , la febbre e il dolore toracico . il quadro radiografico tradizionale dellemorragia alveolare diffusa caratterizzato da opacit da occupazione alveolare , abitualmente bilaterali , di tipo consolidativo o ground glass , di estensione assai variabile ; spesso la distribuzione predominante in sede parailare . 
nelle forme croniche , o recidivanti di emorragia table 1 main causes of diffuse alveolar haemorrhage vasculitis connectivitis drugs other vasculiti connettiviti farmaci varie tabella 1 principali cause di ead wegeners disease micropolyangiitis churg strauss syndrome idiopathic pulmonaryrenal syndromes systemic lupus erythematosus rheumatoid arthritis polydermatomyositis scleroderma penicillamine cytarabine bleomycin goodpastures syndrome idiopathic haemosiderosis antiphospholipid antibody syndrome coagulation disorders bone marrow transplantation morbo di wegener micropoliangioite sindrome di churg strauss sindromi nefro - polmonari idiopatiche lupus eritematoso sistemico artrite reumatoide polidermatomiosite sclerodermia penicillina citarabina bleomicina sindrome di goodpasture emosiderosi idiopatica sindrome da anticorpi antifosfolipidi coagulopatie trapianto di midollo radiol med ( 2008 ) 113 : 1628 alveolare diffusa , pu comparire tardivamente un quadro di persistente impegno interstiziale di natura fibrotica [ 4 ]  . in tc , lead in fase acuta si presenta con opacit ground glass o consolidative che spesso risparmiano il mantello polmonare e gli apici [ 9 ]  . 
nelle forme pi blande o in fase subacuta possono associarsi ai quadri di ground glass tenui opacit pseudo - nodulari , senza distribuzione preferenziale [ 10 ] ; infine pu essere osservato il pattern del crazy paving caratterizzato da opacit ground glass sovrapposte a una fine trama reticolare . 
le opacit lineari che producono il pattern reticolare non sono dovute a inspessimento dei setti lobulari secondari , ma a deposito di materiale emorragico in alveoli alla periferia del lobulo [ 9 ]  . 
la tc , soprattutto se eseguita con tecnica ad alta risoluzione , ritenuta pi sensibile dellrx standard per individuare focolai circoscritti di ead , specie con pattern ground glass , ma non risulta comunque pi specifica . il sospetto clinico - radiografico di ead impone lesecuzione di una broncoscopia con bal , con evidenza della presenza nelle vie aeree di sangue rosso vivo o a lavatura di carne proveniente da sedi multiple , e riscontro microscopico di macrofagi alveolari che contengono emosiderina ( siderofagi ) in quantit crescente in relazione alla cronicit della patologia [ 2 , 11 ] ; in alcuni casi pu per essere indispensabile il ricorso alla biopsia . 
 scopo del lavoro descrivere i reperti della ead in unampia casistica di pazienti sottoposti a esami rx e tc . quando disponibili sono state valutate anche le indagini eseguite nel follow - up ravvicinato , per meglio caratterizzare il decorso radiologico della malattia . 
si sono poi confrontate la sensibilit e la specificit dei radiogrammi standard del torace e della tc convenzionale o a alta risoluzione per meglio definirne il rispettivo ruolo nella diagnosi della malattia . on computed tomography ( ct ) , dah presents with ground - glass or consolidation opacities in the acute phases , often with sparing of the subpleura and apices [ 9 ]  . 
in milder forms or in the subacute phase , slight pseudonodular opacities without preferential distribution [ 10 ] may be associated with ground - glass findings ; finally , a crazy - paving pattern characterised by ground - glass opacities over a thin reticular pattern may be observed . 
the linear opacities producing the reticular pattern are not related to thickened secondary lobular septa but to the deposition of haemorrhagic material inside the alveoli at the lobule periphery [ 9 ]  . 
ct , in particular high - resolution ct ( hrct ) , is considered more sensitive than standard x - ray in identifying limited foci of dah , especially with ground - glass patterns , but it is no more specific . clinical and radiographic suspicion of dah requires confirmation by bronchoscopy with bronchoalveolar lavage ( bal ) , with demonstration of bright red blood from multimateriali e metodi stato eseguito uno studio retrospettivo multicentrico , reclutando un totale di 20 pazienti affetti da emorragia alveolare diffusa , giunti allosservazione tra il 1991 e il 2004 . 
una diagnosi eziologica precisa stata ottenuta in 17 / 20 integrando i dati clinico - anamnestici , bioptici e laboratoristici specifici ( canca , panca , ambg , sierologia per il lupus eritematoso sistemico , anticorpi antifosfolipidi ) : 8 pazienti risultavano affetti da granulomatosi di wegener ( gw ) , 3 da micropoliangioite ( mpa ) , 2 da sindrome di goodpasture ( gp ) , 3 da emosiderosi polmonare idiopatica ( eip ) , 1 da sindrome da anticorpi antifosfolipidi ( aps )  . 
b quasi completa risoluzione delle lesioni a un mese di distanza con persistenza di pattern reticolo - nodulare medio - basale . ple sites in the airways and microscopic evidence of alveolar haemosiderin - containing macrophages ( siderophages ) whose number increases in proportion to the chronicity of the disease [ 2 , 11 ]  . 
in a few cases , the use of biopsy may be indispensable . the purpose of this paper is to describe dah findings in a large series of patients studied by cxr and ct . 
sensitivity and specificity of standard cxr and conventional or high - resolution ct were then compared to establish the respective roles of the two modalities in the diagnosis of the disease . materials and methods a retrospective multicentric study was conducted on 20 patients with dah who presented between 1991 and 2004 . the diagnosis of dah was established on the basis of clinical findings of anaemia ( haemoglobin less than 10 mg / dl ) in 20 / 20 patients , dyspnoea ( 20 / 20 ) , haemoptysis ( 13 / 20 ) and the results of bronchoscopy ( 20 / 20 ) , bal ( 20 / 20 ) and biopsy ( 12 / 20 )  . 
an accurate aetiological diagnosis was achieved in 17 / 20 cases after integrating specific clinical , biopsy and laboratory data [ cytoplasmic - staining antineutrophil cytoplasmic antibodies ( c - anca ) , perinuclearstaining anca ( p - anca ) , antiglomerular basement membrane ( anti - gbm ) antibodies , serology for systemic lupus erythematosus , antiphospholipid antibodies ]  . 
 erano disponibili controlli radiografici in tutti i 20 pazienti , ed esami tc in 15 / 20 , di cui 14 in fase acuta ed uno in corso di follow - up ; gli esami tc sono stati eseguiti con tecniche ed apparecchiature diverse . 
per la valutazione degli esami rx e tc ognuno dei due polmoni stato diviso in tre regioni : una zona superiore , compresa fra gli apici e la carena , una zona intermedia , fra la carena e le vene polmonari , e una regione inferiore , dalle vene polmonari ai diaframmi , per un totale di sei zone . 
in ciascun settore dei due polmoni si ricercata la presenza di consolidamenti o di opacit ground glass ( a vetro smerigliato ) , registrando quale regione fosse pi interessata e se venissero risparmiati gli apici e le regioni mantellari . 
veniva inoltre registrata la presenza di reperti patologici non strettamente correlati alla ead : opacit nodulari , pattern interstiziali reticolonodulari , strie fibrotiche o segni di honeycomb , versamento pleurico . 
episodi ripetuti di ead in un singolo paziente sono stati considerati separatamente e sono stati quindi valutatati complessivamente 23 episodi . risultati la distribuzione delle opacit dimostrate radiograficamente nei 23 episodi di ead riassunta nella tabella 3 . radiol med ( 2008 ) 113 : 1628 were affected by wegeners granulomatosis , three by micropolyangiitis , two by goodpastures syndrome , three by idiopathic pulmonary haemosiderosis and one by antiphospholipid antibody syndrome . 
patient demographic data are shown in table 2 . cxr studies were available for all 20 patients and ct scans for 15 / 20 , 14 of which were in the acute phase and one from the follow - up . 
to evaluate the cxr and ct studies , each lung was divided into three regions upper zone , from the apices to the carina ; middle zone , between the carina and the pulmonary veins ; and lower zone , from the pulmonary veins to the diaphragm for a total of six zones ( three on each side )  . 
repeated dah episodes in a single patient were considered separately , resulting in a total of 23 episodes . results the distribution of opacities shown radiographically in the 23 dah episodes is summarised in table 3 . dah in wegeners granulomatosis eight patients presented with one dah episode each , at the onset of wegeners granulomatosis . 
un esame tc era disponibile in 7 / 8 pazienti , di cui 6 / 8 al momento dellepisodio di ead e 1 / 8 eseguito in follow - up . valutazione rx quattro / 8 presentavano allesordio un quadro rx compatibile con ead , caratterizzato da opacit ground glass o consolidative , con un numero medio di zone coinvolte di 4 , 6 / 6 . in 2 pazienti si apprezzavano esclusivamente opacit di tipo consolidativo diffuse a tutte e sei le zone polmonari , negli altri 2 , meno gravi , erano presenti entrambe le lesioni . 
in 3 casi stato possibile valutare levoluzione radiografica in follow - up : in 2 / 3 si assisteva ad una rapida regressione delle lesioni sin dai primi controlli successivi , con scomparsa delle opacit consolidative ( eventualmente dopo una modificazione in pattern ground glass ) entro 15 giorni . 
in 1 / 3 si osservava inizialmente un aggravamento del quadro con sostituzione delle opacit ground glass con opacit consolidative , e a partire dallottava giornata miglioramento con risoluzione a radiol med ( 2008 ) 113 : 1628 table 3 results diagnosis wegeners granulomatosis micropolyangiitis goodpastures syndrome idiopathic haemosiderosis antiphospholipid syndrome other total tabella 3 risultati diagnosi granulomatosi di wegener micropoliangioite sindrome di goodpasture emosiderosi polidiopatica s . 
one of the eight patients had completely negative cxr . ct evaluation three of four patients with cxr findings typical of dah also underwent ct , which proved to be more accurate in defining the zones involved and the extent of the groundglass pattern , although it provided no significant additional elements . 
in 2 / 3 patients with cxr evidence of nodular lesions but no consolidation or ground - glass opacities , ct documented the presence of ground - glass opacity in one zone in one case but failed to reveal typical findings of dah in the other and only confirmed the existence of nodular lesions . 
tre / 8 dimostravano esclusivamente lesioni nodulari a volte cavitate , caratteristiche della granulomatosi di wegener , senza opacit consolidative o ground glass . uno / 8 presentava un reperto rx totalmente negativo . valutazione tc in 3 / 4 pazienti con reperti radiografici caratteristici di ead veniva eseguita anche la tc , che risultava pi accurata nel definire le zone interessate e lestensione del pattern ground glass , ma nel complesso non forniva elementi aggiuntivi significativi . 
in 2 / 3 pazienti con rx positivo per lesioni nodulari , ma negativo per opacit consolidative o ground glass la tc documentava in un caso la presenza di ground glass in ununica zona , mentre nellaltro non permetteva di evidenziare gli aspetti tipici delle ead , confermando la presenza di lesioni nodulari . 
nel caso con quadro rx completamente negativo la tc documentava un pattern di tipo ground glass nelle 2 zone intermedie ( parailari )  . ead in corso di micropoliangioite di tutti e 3 i pazienti erano disponibili controlli rx e tc . 
un paziente presentava un unico episodio di ead con opacit consolidative inizialmente monolaterali ( 2 / 6 ) , che si erano radiol med ( 2008 ) 113 : 1628 poi diffuse a 6 / 6 dopo tre giorni . 
i restanti pazienti hanno presentato rispettivamente due e tre successivi episodi di ead , prima che fosse possibile stabilire la diagnosi corretta e impostare una terapia adeguata . il primo paziente esordiva con un reperto rx di opacit di tipo consolidativo in 5 / 6 zone e , dopo un netto miglioramento senza reliquati , presentava dopo un anno un ulteriore episodio di ead con opacit consolidative in 5 / 6 zone . la completa normalizzazione si aveva dopo appena una settimana . 
nel secondo paziente il radiogramma mostrava un addensamento consolidativo nella zona inferiore di destra , mentre allindagine tc si osservava un quadro di opacit prevalentemente ground glass in 4 / 6 zone . 
nel terzo si apprezzava un impegno tipo ground glass in tutte le zone con risparmio mantellare e dellapice sinistro . ead in corso di sindrome da anticorpi antifosfolipidi lunico paziente della nostra casistica mostrava al radiogramma del torace delle opacit consolidative perilari e medio - basali ( 4 / 6 zone ) , con estensione a 6 / 6 dopo solo poche ore . 
lhrct documenta opacit prevalentemente di tipo ground glass ( freccia ) , con zone di pattern crazy paving ( frecce doppie )  . dah in micropolyangiitis cxr and ct studies were available for all three patients . one patient presented with a single episode of dah with initially unilateral consolidation opacities ( 2 / 6 ) , which had spread to 6 / 6 zones 3 days later . 
ct performed after the first episode confirmed the ground - glass pattern in 6 / 6 zones , with additional areas of crazy - paving patterns . dah in idiopathic pulmonary haemosiderosis in one patient , a ground - glass pattern was observed in 2 / 6 zones in the middle field on both sides . 
in the second patient , cxr showed a dense consolidation in the lower right zone , entrambi i pazienti presentavano opacit diffuse a 6 / 6 zone , con aspetto prevalentemente ground glass in un paziente e consolidative nel secondo . 
in the third patient , a ground - glass pattern was observed in all zones , with sparing of the subpleura and left apex . dah in antiphospholipid antibody syndrome the only patient with this syndrome showed perihilar and middle - basal consolidation opacities on cxr ( 4 / 6 zones ) , which extended to 6 / 6 zones after only a few hours . 
solo di questo paziente stata valutato un esame tc , che presentava anchesso un pattern di tipo ground glass in 4 / 6 zone , ma in sedi diverse rispetto al reperto dellrx standard . risultati complessivi complessivamente opacit consolidative o ground glass caratteristiche di ead erano dimostrate allrx standard in 16 / 20 pazienti . 
 nei 23 episodi di ead risultavano interessate allesordio 84 / 138 zone ( 60 , 8% ) , con opacit consolidative in 53 / 138 ( 38% ) , e ground glass in 31 / 138 ( 22% )  . 
le zone superiori erano interessate nel 43% , le zone intermedie nel 73% e le zone inferiori nel 65% . in 10 pazienti stato valutato il follow - up rx ( tabella 4 )  . 
le opacit ground glass inizialmente aumentavano ( 14 / 60 ) per lattenuazione delle opacit consolidative , riducendosi dopo 15 giorni a 5 / 60 ( 8% ) ; in soli due casi da causa ignota , per i quali non fu instaurata terapia eziologica , le lesioni persistevano oltre un mese . 
come reperti associati sono stati apprezzati noduli in 5 casi , strie fibrotiche in 2 , versamento pleurico in 6 ( in un caso anche pericardico ) , incremento delle dimensioni cardiache in 4 pazienti . radiol med ( 2008 ) 113 : 1628 picture improved after 24 h and normalised completely after 15 days . 
 dah in goodpastures syndrome both patients presented with opacities extending to 6 / 6 zones , with a prevalently ground - glass appearance in one patient and a consolidation appearance in the other . 
the ct available for one patient demonstrated limited sparing of the apical regions . dah of unknown cause in three patients with a single dah episode , the aetiological diagnosis could not be established with certainty . 
ct was performed on this patient only : it demonstrated a ground - glass pattern involving 4 / 6 zones as well , but in different sites compared with cxr findings . 
 in the 23 dah episodes , 84 / 138 zones ( 60.8 % ) were affected at onset , with consolidation opacities in 53 / 138 ( 38% ) and ground - glass opacities in 31 / 138 ( 22% )  . 
 follow - up cxr was evaluated in ten patients ( table 4 )  . at onset , 35 / 60 ( 58% ) zones were involved by consolidation opacities and 11 / 60 ( 18% ) were affected by ground - glass opacities . 
after 1 week , consolidation opacities persisted in 16 / 60 ( 26% ) , whereas 15 days later , they persisted in 11 / 60 ( 18% )  . 
ground - glass opacities initially increased ( 14 / 60 ) as a result of the regression of consolidation opacities but decreased after 15 days to 5 / 60 zones ( 8% )  . 
b alla hrct evidenza di aree di opacit ground glass da ead confermata dal lavaggio bronco - alveolare . discussione lead una sindrome clinico - patologica piuttosto rara , caratterizzata da sanguinamento alveolare diffuso , che si manifesta con emottisi , tosse , dispnea ed ipossiemia fino allinsufficienza respiratoria , anemia sideropenica ed opacit radiografiche da occupazione alveolare [ 1 ]  . 
lemottisi , sintomo cardine , di enradiol med ( 2008 ) 113 : 1628 table 4 progression of lesions in 10 patients consolidations ground - glass opacities 36 / 60 11 / 60 onset 7 days later 16 / 60 14 / 60 15 days later 11 / 60 5 / 60 table 5 comparison between chest x - ray ( cxr ) and computed tomography ( ct ) in 14 patients consolidations ground - glass opacities 30 / 84 ( 37% ) 14 / 84 ( 16% ) 32 / 84 ( 38% ) 36 / 84 ( 43% ) tabella 4 evoluzione delle lesioni in 10 pazienti tabella 5 confronto rx / tc in 14 pazienti esordio 7 giorni dopo 15 giorni dopo opacit consolidative opacit ground glass 30 / 84 ( 37% ) 14 / 84 ( 16% ) 32 / 84 ( 38% ) 36 / 84 ( 43% ) opacit consolidative opacit ground glass 36 / 60 11 / 60 16 / 60 14 / 60 11 / 60 5 / 60 in one case a patient with dah in micropolyangiitis ct demonstrated a crazy - paving pattern . 
associated findings included nodules in five cases , fibrotic streaks in two , pleural effusion in six ( in one case also pericardial effusion ) and enlarged heart in four . discussion dah is a rare clinicopathological syndrome characterised by diffuse alveolar bleeding accompanied by haemoptysis , cough , dyspnoea and hypoxaemia , respiratory failure , sideropenic anaemia , and cxr opacities due to alveolar filling [ 1 ]  . 
other signs and symptoms frequently associated with dah are fever , chest pain , elevated erythrocyte sedimentation rate ( esr ) and joint pain [ 11 ]  . in the diagnosis of dah , the following factors are essential : complete blood count , bal ( not always feasible in more acute or severe forms ) , coagulation tests and autoantibody tests ( anca , anti - gbm antibodies )  . 
respiratory function tests , which may indicate increased lung diffusion capacity for carbon monoxide ( dlco ) are not usually possible in the acute phases , whereas they may be helpful in milder forms and during the follow - up . 
in doubtful cases , renal or pulmonary biopsy with surgical or transbronchial sampling may prove useful . the histological pattern , which is almost constant in systemic vasculitis or autoimmune processes , is marked by capillarity [ 12 ]  . 
the essential pathogenetic mechanisms are the precipitation of immunocomplexes on the vessel walls and the production of anca or anti - gbm antibodies tit molto variabile e manca in 1 / 3 dei casi , mentre lanemia pi costante [ 1 ]  . 
altri segni e sintomi che si associano allemorragia alveolare diffusa sono la febbre , le toracoalgie , il rialzo dei valori della eritrosedimentazione ( ves ) , le artralgie [ 11 ]  . per la diagnosi di ead sono fondamentali : lemocromo , il bal , non sempre eseguibile nelle forme pi acute e severe , i test della coagulazione e la ricerca di diversi tipi di autoanticorpi ( anca , ambg )  . 
le prove di funzionalit respiratoria , che possono evidenziare un incremento dei valori della diffusione polmonare del co ( dlco ) , non sono di solito utilizzabili in fase acuta , mentre possono risultare utili nei casi pi lievi e nel follow - up . 
nei casi dubbi pu essere utile lesecuzione di una biopsia renale o polmonare , con prelievo chirurgico o transbronchiale . il quadro istologico , pressoch costante in presenza di vasculite sistemica o di processi autoimmuni , quello della capillarite [ 12 ]  . 
i meccanismi patogenetici fondamentali sono la precipitazione di immunocomplessi a livello delle pareti vasali , la produzione di anca o di anticorpi anti - mb [ 5 , 13 ]  . 
il quadro radiologico dellead caratterizzato da opacit parenchimali da occupazione alveolare , bilaterali , diffuse , di tipo consolidativo o ground glass , con distribuzione predominante in sede perilare ( ad ali di farfalla ) , e risparmio di apici e seni costofrenici . 
 la diagnosi differenziale va posta con le altre cause di opacit da occupazione alveolare come ledema cardiogeno , abitualmente associato a versamento pleurico bilaterale e cardiomegalia o non cardiogeno , e con lessudato inradiol med ( 2008 ) 113 : 1628 fig . 
5a - d diffuse alveolar haemorrhage in micropolyangiitis : chest xray obtained a at onset , b at 24 h and c at 36 h show bilateral consolidations spreading rapidly . 
the radiological pattern of dah is characterised by diffuse , bilateral consolidation or ground - glass opacities due to alveolar filling , predominantly distributed in the perihilar regions ( butterfly wings ) and sparing of the apices and costophrenic angles . 
the parenchymal opacities often appear suddenly , with major changes of site , extension and density observed at short - term follow - up studies [ 7 , 8 ]  . 
in the event of recurrences , incomplete resolution of the opacities evolving into fibrosis may be identified [ 4 ]  . dah needs to be differentiated from other causes of opacity due to alveolar filling , such as cardiogenic oedema usually associated with bilateral pleural effusion and cardiomegaly or noncardiogenic oedema , and from the inflammatory exudate from infectious or eosinophilic pneumonia [ 1 ]  . 
in addition to ground - glass or consolidation opacities , ct may also reveal crazy - paving patterns . our retrospective study reviewed the cxr and ct images of 20 patients with dah . 
specific causes wegeners granulomatosis in eight cases , goodpastures syndrome in two , miidiopathic pulmonary croscopic polyangiitis three , fiammatorio caratteristico delle polmoniti infettive o eosinofile [ 1 ]  . 
in tc si osservano , oltre alle opacit ground glass o consolidative , anche quadri di pattern crazy paving . nel nostro studio retrospettivo sono stati revisionate le indagini radiografiche e tc di venti pazienti affetti da emorragia alveolare diffusa . 
le specifiche cause della emorragia alveolare diffusa erano : in otto casi la granulomatosi di wegener , in due la sindrome di goodpasture , in tre la poliangioite microscopica , in tre lemosiderosi polmonare idiopatica e in uno la sindrome da anticorpi antifosfolipidi . 
in dieci pazienti era possibile valutare levoluzione del quadro radiologico nel follow - up ravvicinato . tipico della ead allesame rx standard , in accordo con i dati della letteratura , la presenza di opacit parenchimali da occupazione alveolare , che si presentano con aspetto di tipo consolidativo o ground glass , diffuse e bilaterali , pi frequenti nei campi polmonari medi con maggioradiol med ( 2008 ) 113 : 1628 haemosiderosis in three and antiphospholipid antibody syndrome in one case . 
 a finding typical of dah on standard cxr , in agreement with the literature , is the presence of diffuse and bilateral parenchymal opacities due to alveolar filling , with a consolidation or ground - glass appearance , more frequent in the middle fields and more evident in perihilar sites ( 75% )  . in our study , the finding was moderately less frequent in the lower zones ( 65% ) and markedly less so in the upper zones ( 43% )  . 
in seven cases with complete or almost complete extension of parenchymal opacities over both lung fields , there was at least partial sparing of the apices or subpleura in five , in agreement with the literature . in patients ( 10 / 20 ) for whom short - term follow - up studies were available , we almost constantly observed a rapid improvement , with findings normalising in 20% after 1 week and in 60% after 2 weeks . 
this result differs slightly from previous studies that report complete normalisation occurring after only 7 days . ct and hrct can confirm the possible presence of consolidation opacities and can detect ground - glass zones more easily . 
ct also identified a single case of crazy - paving pattern , which is characteristic though not pathognomonic of dah [ it may also appear in acute respiratory distress syndrome ( ards ) or acute interstitial pneumonia ]  . 
cxrct correlation was not always possible , as ct studies are difficult to perform in the acute stage when respiratory impairment is most severe . during the follow - up , ct showed no particular advantages over cxr in documenting the evolution of dah . conclusions dah is a relatively rare syndrome characterised by nonspecific radiological patterns of alveolar filling , which usually do not allow for a firm radiological diagnosis . 
a diagnosis or suspicion of dah requires correlation with clinical data that support the diagnostic hypothesis : episodes of haemoptysis or , more importantly , rapid - onset anaemia . the diagnosis of suspected alveolar haemorrhage , if supported by clinical data , may also be established by the radiologist based on the finding of diffuse alveolar - filling opacities , especially if a rapid change of parenchymal opacities is observed . 
the radiological suspicion may often prompt the clinician to rapidly order further imaging and laboratory re evidenza in sede perilare ( 75% ) ; una frequenza modicamente inferiore stata rilevata dal nostro studio nelle zone inferiori ( 65% ) , mentre nettamente inferiore nelle zone superiori ( 43% )  . 
in sette casi , in cui era presente un completa o quasi completa diffusione delle opacit parenchimali su entrambi i campi polmonari , ben 5 presentavano un risparmio almeno parziale degli apici o della regione mantellare , in accordo con quanto riportato in letteratura . dei pazienti ( 10 / 20 ) di cui era disponibile un follow - up ravvicinato si osservato pressoch costantemente rapido miglioramento , con normalizzazione del quadro nel 20% dopo una settimana e nel 60% dopo due settimane . 
ci differisce lievemente dai dati della letteratura che riportano in media una completa normalizzazione gi dopo 7 giorni . lindagine tc e hrtc in grado di confermare la eventuale presenza di opacit consolidative e di evidenziare pi facilmente le zone di ground glass . 
non sempre stato possibile comunque correlare strettamente i quadri rx con quelli tc e hrtc per la difficolt ad effettuare uno studio tc nelle fasi acute di pi severa compromissione respiratoria dei pazienti . 
nel follow - up la tc non ha dimostrato particolari vantaggi rispetto allesame rx per documentare levoluzione della ead . conclusioni lead una sindrome piuttosto rara , con aspetti radiologici aspecifici , di occupazione alveolare che non consentono , di solito , ununivoca diagnosi radiologica . 
per la diagnosi o il semplice sospetto di ead indispensabile la correlazione con i dati clinico - anamnestici che supportino lipotesi diagnostica : episodi di emottisi o , ancora pi importante , una condizione di anemia insorta rapidamente . la diagnosi di sospetto di emorragia alveolare , se supportata dalla clinica , pu essere posta anche dal radiologo sulla base del reperto di opacit diffuse da occupazione alveolare , a maggior ragione se si riscontra una rapida modificazione delle opacit parenchimali ; il sospetto radiologico pu spesso indirizzare il clinico alla rapida esecuzione delle ulteriori indagini strumentali e laboratoristiche indispensabili al definitivo inquadramento della patologia . radiol med ( 2008 ) 113 : 1628 studies , which are vital for the definitive diagnosis . ct , especially hrct , can better evaluate the extent of disease and are definitely more sensitive than cxr , in particular in identifying ground - glass opacities . 
the higher sensitivity of hrct supports its use in patients with possible dah and a negative cxr , such as patients with connectivitis , vasculitis or bone marrow transplant presenting with haemoptysis and mild anaemia . 
the hrct finding of ground - glass areas , although not entirely specific , can guide investigations towards subsequent bronchoscopy and biopsy . la tc e meglio la hrtc consentono di meglio valutare lestensione della patologia e sono sicuramente pi sensibili dellrx , in particolare nel riconoscimento di opacit ground - glass , ma non pi specifiche . 
la maggior sensibilit della hrtc impone il ricorso a questa metodica in pazienti con possibile ead e quadro radiografico negativo , quali pazienti affetti da connettiviti , vasculiti o sottoposti a trapianto di midollo che presentino emottisi e lieve anemia . 
this study was performed to clarify the role of perfusion - weighted imaging ( pwi ) at 3 tesla in the characterisation of haemodynamic heterogeneity within gliomas and surrounding tissues and in the differentiation of high - grade from low - grade gliomas . 
pwi was performed by first - pass gadopentetate dimeglumine t2 * - weighted echo - planar images , and cerebral blood volume ( cbv ) maps were computed with a nondiffusible tracer model . 
oedematous - appearing areas were divided in two groups according to signal intensity on t2 - weighted images : tumour with lower ( nearly isointense to grey matter ) and oedema with higher ( scarcely isointense to cerebrospinal fluid ) signal intensity . 
il pwi stato ottenuto mediante immagini eco - planari t2 * - pesate con primo passaggio di gadopentetato di dimeglumina , e le mappe di volume ematico cerebrale ( cbv ) sono state elaborate con il modello del tracciante non diffusibile . 
nei gliomi di alto grado , lrcbv appariva marcatamente incrementato nella massa ( mediasd , 4 , 31 , 2 ) ed ai margini ( 4 , 01 , 1 ) , e ridotto nelle aree necrotiche ( 0 , 30 , 3 )  . 
le regioni apparentemente edematose sono state divise in due gruppi sulla base dellintensit di segnale nelle immagini pesate in t2 : tumore con pi basso segnale ( quasi isointenso alla sostanza grigia ) ed edema con segnale pi elevato ( quasi isointenso al liquido cefalorachidiano )  . 
esso facilita la caratterizzazione in rm dei gliomi cerebrali e fornisce utili informazioni per la pianificazione del trattamento chirurgico e radiante . parole chiave tumori cerebrali risonanza magnetica volume ematico cerebrale imaging pesato in perfusione introduction introduzione gliomas account for approximately 51% of all central nervous system tumours , and their incidence is increasing , especially among the oldest patients [ 1 ]  . 
therapeutic management and prognosis depend on the reliable distinction between high - grade and low - grade gliomas , and a variety of imaging modalities have been proposed for accurate identification of tumour grade [ 2 ]  . 
the combination of t1and t2weighted and contrast - enhanced magnetic resonance ( mr ) imaging is considered the gold standard for diagnosis of cerebral gliomas , but discrepancies between mr imaging findings and pathologic reports have been encountered [ 3 ]  . 
 perfusion - weighted imaging ( pwi ) is a fast and powerful mr technique that is increasingly used in the study of intracranial mass lesions [ 2 , 4 , 5 ]  . 
numerous techniques have been proposed to measure perfusion - related parameters , such as blood volume , transit time , clearance , extraction fraction , blood flow and permeabilitysurface area product , in the brain [ 6 ]  . 
however , dynamic susceptibilityweighted bolus - tracking method , using an exogenous endovascular tracer such as gadopentetate dimeglumine , and cerebral blood volume ( cbv ) , within haemodynamic parameters , have been widely used in clinical settings [ 717 ]  . this pwi method can depict areas of varying haemodynamic activities within tumours and surrounding tissue and can help grade cerebral gliomas [ 717 ]  . 
several studies have demonstrated that the quantitative estimate of cbv reflects tumour microvasculature and angiogenesis [ 79 ]  . the degree of vascularity is directly correlated with malignancy , and the density of microvessels is a prognostic indicator in patients with gliomas [ 18 ]  . 
however , low - grade gliomas , most notably oligodendrogliomas , can present high relative cbv ( rcbv ) foci not reflective of malignancy and may confound the accuracy of rcbv mapping in glial tumour grading [ 19 ]  . i gliomi rappresentano circa il 51% di tutti i tumori del sistema nervoso centrale ( snc ) e la loro incidenza sta aumentando particolarmente fra i pazienti pi anziani [ 1 ]  . limpostazione terapeutica e la prognosi dipendono dalla accurata distinzione tra tumori di alto e di basso grado , e sono state proposte diverse modalit di imaging per permettere laccurata identificazione del grado di malignit [ 2 ]  . 
lutilizzo di immagini rm pesate in t1 , prima e dopo mezzo di contrasto , e in t2 considerato il gold standard per la diagnosi dei tumori cerebrali , ma sono state segnalate alcune discrepanze tra reperti rm e referti anatomo - patologici [ 3 ]  . limaging pesato in perfusione ( pwi ) una tecnica rm veloce ed efficace che viene sempre pi spesso utilizzata nello studio delle neoformazioni cerebrali [ 2 , 4 , 5 ]  . 
numerose sono le tecniche proposte per misurare parametri di perfusione cerebrale quali il volume ematico , il tempo di transito , la clearance , la frazione di estrazione , il flusso ematico e il prodotto permeabilit - area di superfice [ 6 ]  . 
nella pratica clinica , comunque , la metodica che stata pi largamente utilizzata quella dinamica basata sulla suscettibilit magnetica da iniezione in bolo di un mezzo di contrasto endovascolare esogeno , quale il gadopentetato di dimeglumina , ed il parametro emodinamico pi misurato stato il volume ematico cerebrale ( cbv ) [ 717 ]  . 
tale metodica consente di individuare , nel contesto della massa tumorale e dei tessuti circostanti , aree con diverse caratteristiche emodinamiche e pu aiutare nellidentificazione del grado di malignit dei gliomi [ 717 ]  . 
il grado di vascolarizzazione di un tumore correlato direttamente col suo grado di malignit , e la densit dei microvasi tumorali un importante indice prognostico in pazienti con glioma [ 18 ]  . 
tuttavia , i gliomi di basso grado quali gli oligodendrogliomi possono pre136 radiol med ( 2008 ) 113 : 134143 with the integration of 3 - tesla ( 3t ) imagers into clinical practice , there is growing interest in the diagnostic performance of mr imaging techniques at 3t with respect to the established magnetic field strength of 1.5 t [ 2022 ]  . 
mr performed at a higher magnetic field strength has the advantages of higher signal - to - noise ratio ( snr ) and therefore of improved spatial and temporal resolution . 
these gains , however , can be partially lost because of several limitations , such as changes in relaxation times , increase in chemicalshift artefacts and magnetic susceptibility effects and security issues [ 21 , 23 , 24 ]  . 
histopathologic assessment according to the criteria of the revised world health organization ( who ) classification revealed two grade i gangliogliomas , three grade ii astrocytomas , four grade ii oligodendrogliomas , two grade ii oligoastrocytomas , two grade iii oligodendrogliomas , two grade iii anaplastic astrocytomas and 21 grade iv glioblastomas . 
for statistical purposes , grades i and ii gliomas ( 11 patients ) were designed as low grade , and grades iii and iv ( 25 patients ) as high grade . 
the local institutional review board approved the retrospective study . imaging mr examinations were performed using a 3 - t system ( ge medical systems , milwaukee , wi , usa ) with standard quadrature head coil prior to stereotactic biopsy or open surgery . 
tali vantaggi possono essere in parte perduti per effetto di alcune limitazioni , quali le modificazioni dei tempi di rilassamento , laumento degli artefatti da chemical shift e da suscettibilit magnetica e le problematiche inerenti la sicurezza [ 21 , 23 , 24 ]  . lo scopo di questo studio stato quello di caratterizzare leterogeneit spaziale dellemodinamica nei gliomi e nei tessuti peritumorali mediante pwi a 3t , e di valutare il ruolo di questo approccio nella differenziazione dei glomi di alto grado da quelli di basso grado . materiali e metodi pazienti sono stati studiati retrospettivamente 36 pazienti con glioma non trattato ( 22 uomini e 14 donne ; et mediasd , 56 anni12 ; range di et , 2976 anni )  . 
le diagnosi istopatologiche , effettuate secondo la classificazione proposta dallorganizzazione mondiale della sanit ( who ) , includevano : 2 gangliogliomi di i grado , 3 astrocitomi di ii grado , 4 oligodendrogliomi di ii grado , 2 oligoastrocitomi di ii grado , 2 oligodendrogliomi di iii grado , 2 astrocitomi anaplastici di iii grado e 21 glioblastomi di iv grado . 
per lanalisi statistica , i gliomi di grado i e ii ( 11 pazienti ) sono stati considerati tumori di basso grado e i gliomi di grado iii e iv ( 25 pazienti ) tumori di alto grado . 
lo studio retrospettivo stato approvato dalla commissione etica locale . imaging gli esami rm sono stati effettuati con unapparecchiatura a 3 tesla ( ge medical systems , milwaukee , wi ) con bobine in quadratura standard per encefalo , prima della biopsia stereotassica o dellintervento chirurgico . 
after the first ten acquisitions , a bolus of gadopentetate dimeglumine ( 0.07 mmol / kg ) was injected with a mechanical injection pump ( 3 ml / s ) through an 18or 20 - gauge intravenous catheter , followed by a 20 - ml saline flush . 
images were inspected for overall image quality and motion artefacts and transferred to a workstation for postprocessing with a dedicated software package ( functool performance , ge medical systems )  . 
the software calculated , on a voxel - by - voxel basis , curves of signal intensity changes over time , t2 * relaxation rate ( r2 * ) , the baseline to be subtracted to the r2 * curve , and area under the fitted r2 * curve . 
the r2 * was calculated by the equation r2 * = ln ( st / s0 ) / te , where st is the signal intensity at time t , s0 is the precontrast signal intensity ( excluding the first one to two images acquired while reaching of the steady - state mr signal ) and te is the echo time . baseline was estimated by calculating the average background intensity prior to onset and after completion of the transient signal intensity change . 
cbv maps were generated by the numerical integration of r2 * for the first - pass bolus through each pixel on the basis of kinetic principles for nondiffusible tracers [ 6 ] , and the relative cbv ( rcbv ) was calculated by rcbv = cbv [ tumour ] / cbv [ contralateral normal white matter ]  . 
 regions of interest ( rois ) were selectively drawn in the necrotic or cystic regions of the tumour , the apparently nonnecrotic mass , the margins , the oedematous - appearing areas and the surrounding normal - appearing tissue . 
areas of altered signal outside the enhanced margins were taken as apparently oedematous , and areas surrounding the tumours without enhancement or signal alteration in all sequences were considered as apparently normal . 
 il pwi stato ottenuto con sequenze echo - planari ad impulso singolo di tipo gradient - echo ( spessore 5 mm , gap 1 mm , tr 1700 ms , te 48 ms , fa 90 , fov 22 , matrice 164164 , nex 1 , n di fette 12 , tempo di acquisizione 1 min )  . 
dopo le prime 10 acquisizioni , stato somministrato un bolo di gadopentetato di dimeglumina ( 0 , 07 mmol / kg ) con un iniettore automatico ( 3 ml / s ) attraverso un catetere endovenoso di 1820 gauge , seguito immediatamente dalla somministrazione di 20 ml di soluzione fisiologica . 
le immagini ottenute sono state prima visionate per valutare la loro qualit e la eventuale presenza di artefatti da movimento , e poi sono state trasferite su una workstation per lelaborazione mediante un software dedicato ( functool systems , performance , general electric medical milwaukee , wi )  . 
il software calcolava , per ogni voxel : le curve di variazione nel tempo dellintensit di segnale , il tasso di rilassamento t2 * ( r2 * ) , la linea di base da sottrarre alla curva di r2 * , e infine larea sottesa alla curva r2 *  . 
il valore di r2 * stato calcolato con la seguente equazione : r2 * = ln ( st / s0 ) / te , dove st lintensit di segnale al tempo t , s0 lintensit di segnale prima del contrasto ( escludendo le prime 12 immagini acquisite durante il raggiungimento dello stato stazionario del segnale rm ) e te il tempo di eco . 
le mappe di cbv sono state generate attraverso lintegrale numerico del r2 * al primo passaggio del bolo , in ogni pixel , sulla base dei principi cinetici dei traccianti non diffusibili [ 6 ] , e il valore di rcbv stato calcolato con la formula : rcbv = cbv [ tumore ] / cbv [ sostanza bianca normale controlaterale ]  . 
 le roi sono state tracciate nelle regioni tumorali necrotiche o cistiche , nella massa tumorale apparentemente non necrotica , nei margini tumorali , nelle regioni apparentemente edematose e in quelle apparentemente sane . 
le aree di alterato segnale che circondavano i margini neoplastici impregnati sono state considerate come apparentemente edematose , mentre quelle che non presentavano alterazioni di segnale o impregnazioni patologiche sono state considerate come apparentemente normali . 
1a - c conventional t1 - weighted contrast - enhanced ( a ) and t2 - weighted ( b ) images and cerebral blood volume ( cbv ) map ( c ) in a patient with a temporal glioblastoma . 
margins ( d ) : area nearly isointense to grey matter ( tumour ) ( e ) and area scarcely isointense to cerebrospinal fluid ( oedema ) ( f ) surrounding the tumour , and contralateral normal white matter ( g )  . 
1a - c immagini rm pesate in t1 dopo mezzo di contrasto ( a ) e in t2 ( b ) , e mappa di volume ematico cerebrale ( cbv ) ( c ) in un paziente con glioblastoma temporale . 
margini ( d ) ; area quasi isointensa alla sostanza grigia ( tumore ) ( e ) e area quasi isointensa al liquor ( edema ) ( f ) circostanti il tumore , e sostanza bianca normale controlaterale ( g )  . 
le differenze tra i gruppi sono state valutate utilizzando lanalisi della varianza e il test t di student post hoc a due code con un livello di significativit di p < 0 , 05 , dopo correzione secondo bonferroni . 
le valutazioni statistiche di massa e margini tumorali sono state effettuate separatamente perch in 8 casi il glioma era ridotto a un sottile anello di impregnazione intorno ad unarea centrale necrotica . two - tailed students t test with a bonferroni corrected significance level of p < 0.05. 
oedematous - appearing rois were divided in two groups according to signal intensity on t2weighted images : tumour , with relatively lower signal intensity ( nearly isointense to grey matter ) ; and oedema , with relatively higher signal intensity ( scarcely isointense to cerebrospinal fluid )  . 
 discussion in this study , pwi performed at 3 t provided results similar to those previously reported at 1.5 t , as it allows differentiation of high - grade from low - grade gliomas and the distinction of different tumour structures . 
2a - c conventional t1 - weighted contrast - enhanced ( a ) and fluid - attenuated inversion recovery ( b ) images , and cerebral blood volume ( cbv ) map ( c ) in a patient with a grade ii temporoparietooccipital oligoastrocytoma . 
2a - c immagini rm pesate in t1 dopo mezzo di contrasto ( a ) e flair ( b ) , e mappa di volume ematico cerebrale ( cbv ) ( c ) in un paziente con oligoastrocitoma temporo - parieto - occipitale di ii grado . 
tale reperto pu essere spiegato dallosservazione che 140 radiol med ( 2008 ) 113 : 134143 table 1 rcbv [ meanstandard deviation ( sd ) ] in the selected regions of interest ( rois ) of high - grade and low - grade gliomas rcbv , relative cerebral blood volume ; rois , regions of interest . 
observations that the average vessel size of a tumour is greater than that of capillaries and that the ge - epi technique is highly sensitive to those larger vessels in contrast to se - epi that have higher sensitivity to capillaries may explain this finding [ 8 ]  . 
consequently , temporal changes of signal amplitude during the first passage of the contrast bolus are dominated by t2 * effects , and difference in t1 - weighting due to variations in tr can be neglected . 
in contrast , glioblastomas typically demonstrate a breakdown of the il calibro medio dei vasi tumorali maggiore di quello dei capillari e che le sequenze ge - epi sono pi sensibili ai vasi di calibro maggiore , al contrario delle sequenze se - epi pi sensibili ai capillari [ 8 ]  . 
di conseguenza , le variazioni temporali dellintensit di segnale al primo passaggio del bolo di contrasto sono determinate principalmente dagli effetti t2 * ed eventuali differenze di pesatura in t1 , legate ai diversi tr , possono essere trascurate . 
di conseguenza , il decremento del segnale t2 * pu essere parzialmente compensato da un aumento del segnale t1 e ci pu condurre ad una sottostima dell rcbv [ 4 , 11 ]  . 
altri autori hanno usato tr lunghi e / o flip angle ridotti per diminuire la pesatura in t1 [ 4 , 9 , 13 ] , o la tecnica del double - echo [ 25 ]  . 
therefore , the t2 * - related signal decrease can be partly compensated for by a t1 - related signal increase , which may lead to an underestimation of rcbv [ 11 , 4 ]  . 
others used long tr and / or a small flip angle to reduce t1 weighting [ 4 , 9 , 13 ] , and others used the doubleecho technique [ 25 ]  . 
correction of rcbv maps for contrast - agent extravasation by means of a linearfitting algorithm is a new , promising method that allows rcbv values significantly correlated with glioma tumour grade [ 16 ]  . the different doses and infusion rates of contrast agent , which were used by the different authors , can also explain the discrepancies . 
in any case , high - grade gliomas present a marked heterogeneity of histologic composition , including varying degrees of vascularity and frequent areas of necrosis , which can account for the large range of rcbv values [ 4 ]  . in this study performed at a higher magnetic field , we used ge - epi with a relatively long te , lower contrast dose and infusion rate and did not research maximum rcbv values . 
the lower contrast agent dose and infusion rate and the lack of predose injection are the more likely explanations for the lower rcbv values we found in high - grade gliomas . pwi takes advantage of increased susceptibility effect at 3 t , resulting in higher sensitivity to transitory t2 * changes due to the bolus of contrast medium [ 23 ]  . 
in our study , in fact , no patient complained of unpleasant feelings of warmth and / or nausea , symptoms often reported by patients when we previously tried to use higher infusion rates . 
however , increased susceptibility effect also has some disadvantages , such as t2 * shortening and stronger distortion artefacts , particularly close to bone and air spaces at the skull base [ 23 ]  . 
geepi , in particular , can potentially show increased ghosting and shearing effects , which may compromise image quality presenta specifici vantaggi e svantaggi [ 2 , 26 ]  . 
la correzione delle mappe di rcbv per lo stravaso di mezzo di contrasto con lutilizzo di un algoritmo di fitting lineare rappresenta un nuovo promettente metodo che permette di avere rcbv che correlano significativamente con il grado di malignit del glioma [ 16 ]  . 
inoltre , in molti studi le roi sono state posizionate nel contesto delle aree tumorali con pi alti valori di rcbv , misurandone in tal modo soltanto i valori massimi [ 4 , 8 , 9 , 11 , 14 , 15 ]  . 
in ogni modo , i gliomi di alto grado presentano una notevole eterogeneit istopatologica , con differenti gradi di vascolarizzazione e frequenti aree di necrosi , caratteristiche che possono in parte spiegare la vasta gamma di valori di rcbv riportati [ 4 ]  . in questo studio realizzato a pi alto campo magnetico , abbiamo utilizzato sequenze ge - epi con un te relativamente lungo , dosi di contrasto e velocit di infusione pi basse e non abbiamo ricercato valori massimi di rcbv . luso di basse dosi di contrasto e di ridotte velocit di infusione e la mancanza di uniniezione pre - dose di contrasto rappresentano la spiegazione pi probabile per i bassi valori di rcbv che abbiamo rilevato nei gliomi di alto grado . 
il pwi trae vantaggio dallaumento della suscettibilit magnetica a 3t , risultando in una pi alta sensibilit alle variazioni transitorie di t2 * legate allarrivo del bolo di contrasto [ 23 ]  . 
 [ 28 ] hanno dimostrato che il pwi a 3t pu essere praticabile anche a basse dosi di contrasto come 0 , 05 mmol / kg . un altro vantaggio , derivante dallutilizzo di dosi e velocit di infusione pi basse , il miglior comfort dei pazienti . 
nel presente studio , infatti , nessun paziente ha lamentato sgradevole sensazione di calore e / o nausea , sintomi spesso manifestati quando precedentemente avevamo utilizzato pi alte velocit di infusione . 
tuttavia , laumentata suscettibilit magnetica presenta anche alcuni svantaggi , quali la riduzione del t2 * e i pi evidenti artefatti da distorsione , specialmente in vicinanza delle strutture ossee ed degli spazi aerei della base del cranio [ 23 ]  . 
lutilizzo delle sequenze ge - epi , in particolare , pu potenzialmente causare un aumento degli effetti di shearing e ghosting , che possono compromettere la qualit delle immagini e linterpretazione diagnostica [ 23 ]  . 
from the histopathological point of view , regions of altered signal outside the enhancing margins of high - grade gliomas represent a variable combination of vasogenic oedema and infiltrating tumour cells [ 29 ]  . 
in our study , areas nearly isointense to grey matter ( tumour ) on t2 - weighted images showed high rcbv , suggesting incremented size and / or number of vessels and hence tumour angiogenesis . 
on the contrary , areas scarcely isointense to cerebrospinal fluid ( oedema ) presented low rcbv , suggesting a reduction of microvessel density due to the increase of interstitial water . the finding that perienhancing regions of metastasis , containing pure vasogenic oedema , showed rcbv lower than those of high - grade gliomas , containing infiltrating tumour cells , supports our hypothesis [ 30 , 31 ]  . 
a larger study population including a balanced number of patients with different who grades and a trial to correlate mr and histopathological findings will be useful to further support the results of this study . istopatologico , le regioni di alterato segnale esterne ai margini impregnati dei gliomi di alto grado rappresentano una combinazione variabile di edema vasogenico e di cellule tumorali infiltranti [ 29 ]  . 
in tale studio le aree approssimativamente isointense alla sostanza grigia nelle immagini t2 - pesate ( tumore ) mostrano alti valori di rcbv , suggerendo un incremento del calibro e / o del numero dei vasi e , quindi , una angiogenesi tumorale . 
al contrario , le aree quasi isointense al liquido cerebrospinale ( edema ) presentano bassi valori di rcbv , suggerendo una riduzione di densit microvascolare legata allaumento di acqua interstiziale . 
il rilievo che le aree circostanti le aree di impregnazione delle metastasi , contenenti edema vasogenico puro , presentano valori di rcbv pi bassi di quelli delle aree peritumorali dei gliomi di alto grado , caratterizzate oltre che da edema anche da cellule tumorali infiltranti , di supporto alla nostra ipotesi [ 30 , 31 ]  . 
 il presente studio ha due rimarchevoli limiti : il ristretto numero di pazienti con astrocitoma anaplastico , che pu aver influenzato i risultati statistici , e la mancanza di conferme istopatologiche . 
uno studio su una popolazione pi ampia di pazienti , con una distribuzione pi bilanciata di gliomi con diverso grado who , e un trial per correlare i reperti rm con quelli istopatologici potrebbero essere utili per supportare ulteriormente i risultati di questo studio . conclusioni conclusions pwi at 3 t helps distinguish necrosis from tumour mass , infiltrating tumour from oedema and high - grade from lowgrade gliomas . 
riconoscendo i suoi vantaggi ed i potenziali svantaggi e adattando le procedure di imaging alle modificazioni indotte dallalto campo , il pwi a 3t pu essere utilizzato come parte integrante dellesame rm di routine delle lesioni espansive intracraniche per migliorare laccuratezza diagnostica , la valutazione pre - trattamento ed il follow - up dei pazienti con glioma cerebrale . acknowledgement the authors are grateful to piero ghedin and fred frigo ( ge healthcare ) for expert technical assistance . 
fugazzola1 1vascular and interventional radiology , department of radiology , 2department of oncology , 3department of anaesthesiology , university of insubria , viale borri 57 , 21100 varese , italy correspondence to : d . 
this study was done to assess the effectiveness and advantages of computed tomography ( ct ) fluoroscopy as a guide for locating and treating lesions that are not amenable to ultrasound ( us ) guidance , and to evaluate the ct signs of immediate technical success and the shortterm results . 
over the past year , we selected 14 patients ( four women and ten men ; mean age 73 , range 6183 years ) out of 103 candidates for hepatic radiofrequency ablation ( rfa )  . 
the 14 lesions comprised seven residual tumours after combined embolisation and us - guided rfa of a large hepatocellular carcinoma ( hcc ) , which were indistinguishable from necrosis or surrounding healthy parenchyma ; two hcc nodules in locations that were inaccessible by us ; five metastases ( two from renal carcinoma , two from colorectal adenocarcinoma and one from lung carcinoma ) , of which one could not be distinguished from the surrounding healthy parenchyma on us and four were inaccessible by us . 
nellultimo anno abbiamo selezionato 14 / 103 pazienti ( 4 femmine e 10 maschi ) candidati a un trattamento di radiofrequenza ( rf ) epatica , et media 73 anni ( range 6183 ) portatori di 14 lesioni epatiche : 7 residui di grosso hcc , esito di terapia combinata mediante embolizzazione e rf eco - guidata non distinguibili dalla necrosi o dal parenchima epatico sano circostante ; 2 noduli di hcc non raggiungibili con guida ecografica per sede ; 5 metastasi ( 2 da carcinoma del rene , 2 da adenocarcinoma del colon - retto e 1 da carcinoma del polmone ) , di cui 1 non distinguibile dal parenchima sano circostante allecografia e 4 non raggiungibili per sede . 
le lesioni presentavano diametro compreso tra 1 , 4 e 3 , 5 cm . le procedure sono state espletate in sala tc in assistenza anestesiologica con ago elettrodo di leveen coassiale ( 14 gauge , diametro apertura uncini da 2 a 4 cm )  . 
nelle 3 lesioni metastatiche a prevalente vascolarizzazione veno - portale si documentato successo tecnico immediato e assenza di radiol med ( 2008 ) 113 : 87100 observed disease progression , with the appearance of additional nodules at 6 months . 
the two metastases with arterial supply showed no signs of recurrence at 3 months ; one case developed a recurrence along the ablation margin , with the appearance of satellite nodules at 6 months . 
ct fluoroscopy is overcoming the limitations of ct in locating and treating lesions with different hepatic vascularisation and those unamenable to us ; furthermore , it reduces the length of the procedure , thanks to the faster and more accurate placement of the needle electrode . 
le 2 metastasi a prevalente vascolarizzazione arteriosa , non hanno evidenziato a 3 mesi segni tc di recidiva ; a 6 mesi in 1 caso si documentata una recidiva lungo il margine di ablazione e comparsa di microlesioni satelliti . 
la guida fluoro - tc ha attualmente superato i limiti della tc nel localizzare e trattare lesioni a differente vascolarizzazione epatica e quelle non fattibili sotto guida ecografica ; inoltre ha ridotto i tempi di procedura per il pi veloce ed accurato posizionamento dellago - elettrodo . 
la tcms si dimostrata metodica affidabile nella valutazione dei risultati della rf immediati e a breve distanza . parole chiave radiofrequenza mdct fluoro - tc introduction introduzione the indications and limitations of treating primary and secondary liver tumours with radiofrequency ablation ( rfa ) have been extensively debated and are now well established [ 13 ]  . 
although ultrasound ( us ) guidance is the fastest , it is unfeasible in several cases ; for example , when the lesion has an echogenicity that does not permit differentiation from the surrounding parenchyma or when its location renders the lesion inaccessible . 
in particular , ct - fluoroscopy guidance combines the high spatial resolution and good contrast resolution inherent to contrast - enhanced ct [ 4 ] with the immediacy of fluoroscopic monitoring [ 5 ]  . 
nonetheless , ct guidance is limited in centring hypervascular lesions because of the short duration of arterial enhancement . the purpose of this study was to assess the effectiveness of ct - fluoroscopy guidance in the location and treatment of lesions with arterial or portal vein supply and unamenable to us because of their location , and to assess ct signs of immediate and short - term technical success . le indicazioni ed i limiti del trattamento dei tumori primitivi e secondari del fegato mediante ablazione con radiofrequenza ( rf ) sono stati ampiamente discussi e ben codificati [ 13 ]  . 
la guida ecografica sicuramente la pi veloce ma in alcuni casi non fattibile , qualora la lesione abbia unecogenicit non distinguibile dal parenchima circostante o non sia raggiungibile per la sua sede . 
in tali casi la guida mediante tomografia computerizzata ( tc ) offre una valida alternativa ; in particolare la guida fluorotc somma lalta risoluzione spaziale della tc e la buona risoluzione di contrasto ottenibile mediante linfusione di mezzo di contrasto ( mdc ) [ 4 ] con limmediatezza del controllo fluoroscopico [ 5 ] ; la guida tc presenta comunque dei limiti nella centratura di lesioni ipervascolari in relazione alla breve durata dellenhancement arterioso . scopo del lavoro valutare lefficacia dellulteriore vantaggio della guida fluoro - tc nel localizzare e trattare lesioni a differente vascolarizzazione epatica non fattibili o non raggiungibili per sede con guida ecografica e valutarne i segni tc di successo tecnico immediato e a breve distanza di tempo . radiol med ( 2008 ) 113 : 87100 materials and methods between october 2005 and october 2006 , 103 hepatic rfa procedures were carried out at our institute : 89 / 103 were performed under us guidance , whereas 14 lesions in 14 patients ( 4 women and 10 men ) , mean age 73 ( range 6183 years ) were treated under ct - fluoroscopy guidance ( aquilian 64 - slice ct , toshiba europe medical systems )  . 
of the four patients with metastasis , 2 / 4 , with metastasis from colorectal cancer , presented high carcinoembryonic antigen ( cea ) levels ( 75 ng / ml and 104 ng / ml ) , whereas 1 / 4 , with metastasis from squamous cell lung carcinoma , had elevated cytokeratin 19 fragment ( cyfra 21 - 1 ) levels ( 3.2 ng / ml )  . 
seven patients ( with residual tumour from hcc ) had previously undergone liver rfa ; the remaining 7 / 14 had undergone no previous surgical or percutaneous treatment on the liver . 
 the procedure was carried out in the ct room with anaesthesiological assistance ( patient sedated with 12 mg of midazolam , 13 mg of alfentanil , 50150 mg of propofol intravenously , and oxygen by face mask )  . 
 in all cases , we used a coaxial 14 - gauge leveen needle electrode ( boston scientific , san jos , ca , usa ) , with a 2to 4 - cm array diameter , connected to a 200 - w generator ( rf 300 , boston scientific )  . 
le lesioni presentavano diametro compreso tra 1 , 4 e 3 , 5 c undici lesioni avevano una prevalente vascolarizzazione arteriosa quindi caratterizzate da una fugace iperdensit nella sola fase arteriosa e 3 lesioni invece vascolarizzazione portale , quindi a marcata ipodensit nella sola fase veno - portale . 
dei 4 pazienti con metastasi , 2 / 4 con metastasi da colonretto presentavano un incremento dei valori del cea ( 75 ng / ml e 104 ng / ml ) in 1 / 4 con metastasi da carcinoma spinocellulare del polmone un aumento del cyfra 21 - 1 ( 3 , 2 ng / ml ) ; il paziente con metastasi da carcinoma del rene non presentava alterazione dei marcatori tumorali . 
sette pazienti ( con residuo di hcc ) erano stati sottoposti in precedenza a rf epatica ; i rimanenti 7 / 14 non avevano subito pregressi trattamenti chirurgici o percutanei a livello epatico . 
 le procedure sono state espletate in sala tc in assistenza anestesiologica ( paziente in sedazione ottenuta con somministrazione endovenosa di midazolam 12 mg , alfentanyl 13 mg , propofol 50150 mg , associata ad ossigeno in maschera ) ; stata inoltre praticata anestesia locale lungo il sito daccesso mediante 5 ml carbocaina 2% ( carbocaina , astrazeneca , basiglio , italia )  . in tutti i pazienti stata inoltre effettuata una profilassi antibiotica . 
mean hospital stay was 2.3 ( range 15 ) days . tanea di mdc solo per le lesioni ipervascolarizzate con rapido wash - out ( 12 boli da 50 ml a 4 ml / s , concentrazione 400 mgi / ml seguita da 30 ml di fisiologica a 4 ml / s ; la dose massima complessiva di mdc somministrata stata , come raccomandato , di 2 ml per kg di peso del paziente )  . 
b , c due to its size , the lesion was treated with embolisation ( b ) ( black arrow ) combined with radiofrequency ablation ( c ) ( white arrow )  . 
d mdct at 1 month , arterial phase : a marginal residual nodule is seen ( black arrow ) ; small lipiodol residues from the previous embolisation can be seen close to the residual tumour . 
f , g mdct at 3 months : no signs of recurrence along the ablation margins ; small lipiodol residues persist inside the ablation area ( black arrow ) ; the size of the ablation area is unchanged . 
h , i mdct at 12 months : no signs of recurrence , and ablation area unchanged in size ; disease progression with the appearance of satellite micronodules ( black arrow )  . 
b , c le dimensioni fanno optare per il sinergismo della terapia combinata della lesione mediante embolizzazione ( b ) ( freccia nera ) e rf ( c ) ( freccia bianca )  . 
marcatamente aumentato in dimensioni il nodulo da insemenzamento sottocutaneo ( freccia bianca )  . risultati stato ottenuto successo tecnico immediato in 13 / 14 pazienti , valutato mediante tcms come assenza di residuo per mancata impregnazione della lesione a prevalente vascolarizzazione arteriosa e in tutti i casi per margini di ablazione che comprendevano e superavano la lesione . 
nelle 3 lesioni metastatiche a prevalente vascolarizzazione veno - portale ( 2 da adenocarcinoma colon - rettale e 1 da carcinoma spinocellulare polmonare ) , si documentato successo tecnico immediato e assenza di recidiva a 3 e 6 mesi in tutti i 3 casi . 
larea di ablazione presentava ridotta densit a margini ben definiti con cercine di granulazione assente e dimensioni superiori alla lesione trattata a 3 mesi e pressoch immodificata per dimensioni e caratteristiche al controllo a 6 mesi ; laltra ha avuto una ripresa di malattia a 6 mesi per comparsa di ulteriori noduli epatici . 
b ricostruzioni mpr con finestra da polmone : riconoscibile lungo tutto il decorso lago elettrodo avanzato mediante approccio trans - polmonare con dispiegamento degli uncini nel contesto della lesione sottodiaframmatica . 
 d tcms a 6 mesi : area di ablazione di ridotta densit a grossolana morfologia semilunare con dimensioni nettamente superiori rispetto alla lesione trattata ; assente il cercine denso marginale di granulazione . results immediate technical success was achieved in 13 / 14 patients , defined as mdct absence of residual tumour based on lack of enhancement of lesions with arterial supply and ablation margins comprising and extending beyond the lesion in all cases . 
in the three metastatic lesions with portal vein supply ( two from colorectal adenocarcinoma and one from squamous cell carcinoma of the lung ) , mdct demonstrated immediate technical success and no recurrence at 3 and 6 months . 
the ablation area showed low density , well - defined margins and absence of granulation riit appeared larger than the treated lesion at 3 months and remained unchanged in size and shape at 6 months . 
3 a multidetector computed tomography ( mdct ) at 1 month , arterial phase : near the low - density area ( black arrow ) , the outcome of an ultrasoundguided radiofrequency ablation , a crescent - shaped , hyperdense area due to residual hepatocellular carcinoma can be seen ( white arrow )  . 
b postprocedural mdct , arterial phase : the hypervascular lesion has disappeared and has been replaced by a rounded hypodense ablation area with a dense marginal rim produced by inflammation ( black arrow )  . 
within the ablated area , the hooks of the needle electrode can be clearly seen , with their typical umbrella - like shape ( white arrow ) c , d mdct at 3 months ( c arterial phase ; d portal phase ) : the dense marginal rim has disappeared ; it is partially recognisable as a thin rim in the portal phase only ( black arrow ) ; the ablation area is well delimited and appears smaller . 
e , f mdct at 6 months : further shrinkage of the ablation area without signs of recurrence along the ablation margins ( black arrow )  . fig 3 a tcms a 1 mese , fase arteriosa : a ridosso di area di ridotta densit ( freccia nera ) esito di rf con guida ecografia ; riconoscibile area iperdensa semilunare con significato di residuo di hcc ( freccia bianca )  . 
b tcms post - procedura , fase arteriosa : non pi riconoscibile la lesione ipervascolarizzata sostituita da area tondeggiante di ablazione di ridotta densit con spesso cercine denso marginale di tipo infiammatorio ( freccia nera )  . 
c , d tcms a 3 mesi ( c fase arteriosa ; d fase veno - portale ) : assente il cercine denso marginale riconoscibile a tratti nella sola fase veno - portale ( freccia nera ) come sottile orletto . 
the granulation rim can be distinguished from residual tumour in that it is concentric , has regular margins , appears hypervascular in the arterial and / or portal phase and never shows portal - phase washout , which is typical of viable tumour . 
it was later applied to primary and secondary lesions of the liver and lung and less commonly to renal , adrenal , and bone neoplasms , to thyroid and parathyroid nodules and to breast and prostate cancers [ 812 ]  . rfa is based on the generation of heat inside the lesion , with temperatures exceeding 50c . 
if that temperature is maintained for more than 3 min , intracellular proteins are denatured and membrane lipids dissolved , resulting in cell death by coagulation necrosis [ 1015 ]  . 
the availability of a coaxial system is especially useful for needle placement under ct guidance : this system allows preliminary positioning of a needle discussione la termoablazione percutanea con rf una tecnica mini - invasiva che stata inizialmente proposta per il trattamento delle anomalie della conduzione cardiaca , della nevralgia del trigemino [ 6 ] e dellosteoma osteoide [ 7 , 8 ] ; successivamente stata applicata alle lesioni primitive e secondarie del fegato e del polmone e , pi raramente , alle neoplasie renali , surrenali , ossee , ai noduli tiroidei e paratiroidei , nonch ai tumori della mammella e della prostata [ 812 ]  . la tecnica di rf si basa sullo sviluppo di calore allinterno della lesione con temperature superiori ai 50c . 
il mantenimento di tale temperatura per pi di 3 minuti determina la denaturazione delle proteine intracellulari e la dissoluzione dei lipidi di membrana con conseguente morte cellulare per necrosi coagulativa [ 1015 ]  . 
lago - elettrodo di leveen ( 14 g ) utilizzato nel nostro studio dotato di 10 uncini retrattili che una volta aperti vanno ad assumere la tipica configurazione ad ombrello . 
particolarmente utile per il posizionamento mediante guida tc la disponibilit di un sistema coassiale che consente il preliminare posizionamento di un ago - trocar , con inserimento successivo dellago elettrodo e apertura degli uncini ; il materiale del trocar non trasmette il calore lungo il suo decorso garantendo quindi un sicuro approccio anche trans - polmonare [ 17 ] e inoltre , in questi , casi retraendo la cannula , al termine della procedura , possibile aspirare eventuali falde di pneumotorace . per quanto riguarda le indicazioni , la rf epatica attualmente proposta come terapia curativa , con il vantaggio , rispetto alla chirurgia , di preservare pi parenchima epatico sano , nella lesione singola primitiva epatica con dimensioni non superiori ai 4 cm in relazione alle attuali dimensioni dellago . 
in pazienti con cirrosi epatica compensata ( child a / b ) possibile effettuare lablazione di un massimo di 3 lesioni di hcc , se confinati ad un singolo lobo epatico , con diametro non superiore ai 4 cm [ 18 ]  . 
possibile effettuare un trattamento con pi infissioni o pi sedute e ripetere ulteriormente il trattamento quando compare una nuova lesione , come accade nella maggior parte dei pazienti cirrotici entro 5 anni . 
parimenti indicata in pazienti con metastasi epatiche anche se interessano entrambi i lobi epatici , fino ad un massimo di 5 lesioni con diametro non superiore ai 4 cm , secondarie a qualunque neoplasia primitiva precedentemente trattata radicalmente , nei confronti delle quali la chirurgia non attuabile , controindicata o non tollerata dal paziente [ 3 ]  . radiol med ( 2008 ) 113 : 87100 trocar , with subsequent insertion of the needle electrode and deployment of the hooks . 
in addition , in these cases , on removing the cannula at the end of the procedure , possible areas of pneumothorax can be aspirated . hepatic rfa is currently indicated as a curative procedure for single primary liver lesions up to 4 cm in diameter in relation to the size of current needles . 
in patients with compensated liver cirrhosis ( child a / b ) , as many as three hcc lesions up to 4 cm can be ablated if they are confined to a single hepatic lobe [ 18 ]  . treatment with multiple electrode placements or over multiple sessions is also possible , and the same treatment can be repeated when a new lesion appears , as occurs within 5 years in most cirrhotic patients . 
rfa is also indicated for liver metastases affecting both hepatic lobes : in particular , up to five lesions 4 cm or less in diameter secondary to cancers that have been resected , in which surgery is impossible , contraindicated or not tolerated by the patient [ 3 ]  . today , size is no longer an absolute limitation of rfa of neoplastic lesions , thanks to the development of larger needle electrodes of varying shape producing a 4to 5 - cm area of necrosis per placement , the possibility of multiple needle placements and the local infusion of hypertonic saline solution , which would increase the volume of necrosis by increasing tissue impedance [ 10 , 16 ]  . 
currently , most primary and secondary hepatic lesions are treated under us guidance , as the method is widely available , inexpensive , allows virtually unlimited viewing angles even with the transcostal approach and is carried out in real time . 
the procedure is markedly operator dependent , as success is influenced by the operators promptness in locating and penetrating the lesion at the passage of the us contrast agent , and the treatment can only be performed on lesions that are isoechoic to the surrounding parenchyma [ 19 ]  . ct - fluoroscopy guidance , in our experience , is indispensable , as it is the only technique capable of reaching the lesion and it is useful when the lesion , although visualised on us , cannot be accessed with us because of its location . furthermore , as sporadically reported in the literature [ 17 , 18 , 20 ] , ct guidance allows transpulmonary access to subdiaphragmatic hepatic lesions , which are usually inaccessible under us guidance . 
attualmente la maggior parte delle lesioni primitive e secondarie del fegato vengono trattate sotto guida ecografica , poich questa metodica ampiamente disponibile , a basso costo , le angolazioni possibili sono virtualmente illimitate , anche mediante approccio trans - costale , e la procedura viene eseguita in tempo reale . 
inoltre possibile lutilizzo del mdc ecografico che ha il solo limite della singola dose e della fugacit che comporta un limitato tempo di azione ; pertanto il successo del trattamento dipende dalla velocit e dalla rapidit delloperatore nel localizzare e penetrare la lesione al passaggio del mdc ecografico , quindi molto operatore dipendente e attuabile chiaramente solo nelle lesioni che presentano una diversa ecogenicit rispetto al parenchima circostante [ 19 ]  . la guida fluoro - tc , nella nostra esperienza , ha dimostrato di essere una alternativa indispensabile quando la sola tecnica capace di raggiungere la lesione e diviene utile quando la lesione , pur essendo identificabile con lecografia , non aggredibile con tale metodica a causa della sua localizzazione . 
inoltre la guida tc permette laccesso trans - polmonare per le lesioni epatiche localizzate in sede sottodiaframmatica generalmente inaccessibili con guida ecografia come riportato in letteratura in casi sporadici [ 17 , 18 , 20 ]  . 
da una revisione della letteratura [ 4 , 17 , 18 , 2023 ] di alcuni autori che hanno utilizzato la guida tc quale alternativa allecografia risultano trattate con guida tc 49 lesioni ( 2 delle quali mediante fluoro - tc ) ; di queste lesioni , 34 / 49 sono hcc mentre le rimanenti sono metastasi con una netta prevalenza di lesioni secondarie ad adenocarcinoma colon - rettale . 
 la rapida identificazione di lesioni a differente vascolarizzazione e della punta / direzione dellago il sicuro vantaggio della guida fluoro - tc dovuto al tempo di scansione tanto breve quanto sufficiente per la ricostruzione dellimmagine . 
questo combina lelevata risoluzione spaziale sul piano assiale tipica della tc , con lelevata risoluzione temporale della fluoroscopia , permettendo la visualizzazione in tempo reale della lesione , della punta e della direzione dellago durante tutta la procedura . 
 prompt visualisation of lesions with arterial or portal supply and of the tip / direction of the needle is a major advantage of ct fluoroscopy , resulting from a scan time that is as short as needed for reconstruction . 
this combines the high spatial resolution in the axial plane of ct with the high temporal resolution of fluoroscopy , allowing real - time visualisation of the lesion , and the tip and direction of the needle throughout the procedure . 
from the control console , the operator can independently move the table , tilt the tube and acquire fluoroscopic images that can be viewed on the control monitor next to the ct table . therefore , the procedure is performed during the simultaneous assessment of three contiguous scan planes displayed on the monitor : the plane of the lesion and the planes immediately above and below . 
this increases significantly the longitudinal resolution along the z axis and consequently the systems reliability , as the actual direction of the needle is more accurately defined in the craniocaudal direction . 
if , as the needle advances , the tip is no longer visualised in the lesion plane but in the plane above the lesion , it means that the needle is being tilted too cranially ; if , conversely , the tip appears in the plane below , its direction will be too caudal . ct fluoroscopy can be used with three operational modes : continuous fluoroscopy , used from the moment the needle is inserted to when the lesion is reached ; spot - check fluoroscopy , to confirm the position of the tip and ensure direction is maintained after a short advancement of the needle ; mixed continuous and spot check , where the continuous mode is used only to overcome particularly difficult anatomical and procedural situations [ 24 ]  . 
 when rfa is performed under continuous ct - fluoroscopy guidance , one needs to take into account the possible consequences of exposure of the operators hands to the direct beam and therefore to higher radiation doses [ 25 ]  . dose measurements for the operators hand carried out by irie et al . 
given these dose rates , the operator may be forced to limit the number of procedures done each year to keep within the dose limits of 20 msv / year for the entire body and of 500 msv / year for the hands . 
pertanto la procedura viene effettuata mediante la simultanea valutazione di una triplice immagine fluoroscopica , vale a dire che sul monitor vengono visualizzati contemporaneamente 3 piani contigui di scansione : il piano della lesione e i piani adiacenti sopra e sottostanti . 
questa opportunit incrementa notevolmente la risoluzione longitudinale lungo lasse z e quindi laffidabilit del sistema , in quanto viene pi dettagliatamente definita leffettiva direzione in senso cranio - caudale dellago . 
se , infatti , durante lavanzamento dellago si nota che la punta non viene pi visualizzata nel piano centrale ma in quello soprastante si intuisce che si sta imprimendo allago uninclinazione troppo craniale , se viceversa si visualizza la punta nel piano sottostante la direzione sar troppo caudale . sono possibili 3 modalit operative : la fluoroscopia continua durante linserimento dellago fino al raggiungimento della lesione ; la fluoroscopia di rapido controllo o spot caratterizzata da avanzamento per breve tratto dellago e successivo spot di scopia , il pi breve possibile , per la verifica della posizione della punta e del mantenimento della direzione programmata ; da ultimo possibile una modalit mista , sia continua che spot , riservando la modalit continua al superamento di situazioni anatomiche ed operative particolarmente problematiche [ 24 ]  . 
 quando il trattamento di rf viene condotto sotto guida fluoro - tc continua , bisogna considerare anche le possibili conseguenze derivate dallesposizione delle mani delloperatore al fascio diretto quindi a dosi di radiazione pi elevate [ 25 ]  . 
con queste misurazioni pu accadere che loperatore deve limitarsi a realizzare solo un certo numero di interventi per anno considerando la limitazione della dose a 20 msv / anno per lintero corpo e 500 msv / anno per le mani . 
una significativa riduzione della dose per loperatore pu essere ottenuta utilizzando solo dei sottili guanti di protezione in piombo , i quali riducono del 77% la dose sulla mano delloperatore . 
pi lungo il supporto dellago minori sono le radiol med ( 2008 ) 113 : 87100 operators from scattered radiation consists in placing lead drapes under and over the patient , close to the access site , as indicated by previous studies [ 29 ]  . 
finally , the use of needle supports ( either long or short ) allows the hands to be kept away from the direct beathe longer the needle support , the lower the radiation doses to the hand . 
nonetheless , needle supports cannot be used in all cases because of the difficulty in manoeuvring the needle , especially when the force applied is not sufficient to reach deep lesions . 
the combination of lead drapes , bismuth gloves and needle supports proved to be the most effective solution , with almost 100% dose reduction [ 30 ]  . in the assessment of immediate and long - term results , contrast - enhanced us has been proposed to determine the extent of the ablation area and the absence of residual tumour [ 19 ]  . 
ct is , however , the most widely used technique for the assessment of long - term results in lesions treated with rfa , even though mri according to some authors is more accurate in monitoring the acute effects of the treatment [ 10 , 15 , 31 ]  . 
an advantage of mri is its ability to assess the volume of coagulation necrosis in real time during the application of energy [ 16 , 32 ]  . postprocedural ct shows a hypodense area often containing numerous , irregularly distributed , small air inclusions of varying size , which indicate that coagulation necrosis has taken place . 
two minutes after rfa , attenuation of the treated tissue decreases by 14 hu compared with the healthy liver , a difference that increases to 22 hu after 8 min [ 33 ]  . 
the ablated area appears rounded , with well - defined borders and surrounded by a thick , relatively hyperdense , rim representing an inflammatory reaction , and larger than the initial lesion . 
in contrast , in the case of incomplete ablation , the borders are ill defined , and the peripheral viable tumour shows similar enhancement to that of the initial lesion [ 16 , 37 ]  . 
minor complications include haemobilia , asymptomatic pleural effusion , cholecystitis ( with lesions adjacent to the gallbladder ) , abdominal pain caused by peritoneal irritation , shoulder pain from diaphragmatic irritation , fever due to treatment - induced necrosis , abscesses and biliary fistula [ 39 , 40 ]  . 
tuttavia , non in tutti i casi pu essere utilizzato il supporto , a causa delle difficolt nel manovrare lago , specialmente quando viene esercitata una forza di penetrazione insufficiente per raggiungere lesioni profonde . 
la combinazione di teli di piombo , guanti di bismuto , ed il supporto per lago si dimostrata la soluzione pi efficace con una riduzione di circa il 100% [ 30 ]  . nella valutazione dei risultati immediati e a distanza lecografia con mdc stata proposta per determinare lestensione dellarea di ablazione e lassenza di residui [ 19 ] ; comunque la tc la tecnica maggiormente utilizzata per la valutazione dei risultati a distanza delle lesioni sottoposte a rf , bench la rm secondo alcuni autori sia pi accurata per il monitoraggio degli effetti acuti del trattamento [ 10 , 15 , 31 ]  . 
a 2 minuti dalla rf il tessuto trattato mostra unattenuazione inferiore di 14 uh rispetto al tessuto epatico sano , e questa differenza aumenta a 22 uh dopo 8 minuti [ 33 ]  . 
dopo somministrazione di mdc , la differenza di attenuazione tra il tessuto sottoposto ad ablazione con rf e il tessuto epatico sano aumenta a 55 uh [ 3436 ]  . 
larea di ablazione appare a morfologia tondeggiante con profili ben definiti per spesso cercine marginale di relativa iperdensit espressione di avvenuta reazione infiammatoria , di dimensioni maggiori rispetto al nodulo di partenza . 
nel caso di ablazione parziale , invece , i profili risultano mal definiti e il tessuto tumorale marginale vitale mantiene un enhancement analogo a quello della lesione iniziale [ 16 , 37 ]  . 
tra le complicanze minori sono stati descritti : emobilia , versamento pleurico asintomatico , colecistite ( in caso di lesione localizzata a ridosso della colecisti ) , dolore addominale da irritazione peritoneale , dolore alla spalla da irritazione diaframmatica , iperpiressia dovuta ai fenomeni necrotici indotti dal trattamento , ascessi , fistola biliare [ 39 , 40 ]  . 
this might be caused , as postulated by various authors [ 41 ] , by a previous biopsy of the lesion or by multiple placements of the needle cannula or needle electrode inside the lesion before the ablation . in addition to the postprocedural assessment of the immediate technical success to differentiate residual tumour from the dense inflammatory rim , further evaluations need to be performed after some time . 
this time interval allows identification of possible nodular recurrences along the ablation margins , which can be distinguished from the thin , dense peripheral granulation rim that is absent or discontinuous after 3 months . 
the ablation area , or scar , is larger than the treated lesion , as it includes the lesion and a safety margin of at least 0.51 cif treatment is successful , after 6 months or sometimes longer the scar shrinks , with complete disappearance of the peripheral granulation rim and unchanged hypodensity ( 22 hu )  . the world health organisation or response evaluation criteria in solid tumours ( recist ) dimensional criteria [ 42 ] , therefore , cannot be used to document response to ablation therapies , at least not in the immediate posttreatment period . 
based on these criteria , the effectiveness of cancer treatment is assessed by measuring the extent of tumour shrinkage , a parameter that cannot be applied to thermal ablation procedures . 
however , the most common criterion to assess the procedures effectiveness on ct , mri or contrast - enhanced us is the absence of enhancement in the treated tissue , although this may change with the introduction of routine positron emission tomography ( pet )  . 
questo possibile che si realizzi , come da pi autori ipotizzato [ 41 ] , per pregressa biopsia della lesione o per pi posizionamenti dellago cannula o dellagoelettrodo allinterno della lesione prima dellablazione . oltre alla valutazione del successo tecnico immediato post - procedura che differenzia il residuo dal cercine denso marginale di tipo infiammatorio necessario eseguire una valutazione a distanza ; questo intervallo di tempo consente di identificare leventuale recidiva nodulare generalmente lungo i margini di ablazione gi distinguibile dallesile cercine denso marginale di granulazione assente o riconoscibile solo a tratti ai 3 mesi . 
larea di ablazione o scar ( cicatrice ) risulta pi grande della lesione trattata , includendo la lesione e un margine di sicurezza di almeno 0 , 51 ca 6 mesi se il trattamento ha avuto successo , questa cicatrice diminuisce di dimensioni , anche se questo pu avvenire pi lentamente , con completa scomparsa del cercine di granulazione marginale e mantenendo immodificata lipodensit ( 22 uh )  . i criteri dimensionali della who o del recist [ 42 ] , pertanto , non possono essere applicati per documentare la risposta alle terapie ablative almeno non nellimmediato periodo post - trattamento . 
quindi sono necessari altri metodi per accertare lefficacia della rf ; attualmente non c un chiaro consenso su quali metodiche di imaging siano pi appropriate per il follow - up post - ablazione . 
in ogni caso il criterio pi comunemente utilizzato per valutare lefficacia delle procedura attraverso la tc , la rm o lecografia con mdc lassenza dellenhancement del tessuto trattato in attesa di poter utilizzare la pet di routine . oggi nella valutazione dei risultati il ricorso alla pet o alla pet - tc da riservare , secondo alcuni , ai casi dubbi ; la proposta di impiegare tale metodica conseguente ai buoni risultati ottenuti nella valutazione dei risultati di lesioni trattate con rf anche in altri distretti [ 43 ]  . 
limaging per la valutazione dei risultati viene poi necessariamente integrato con un controllo clinico e bioumorale specifico [ 10 ]  . conclusions conclusioni ct guidance has always proved to be a valid percutaneous approach to rfa of primary and secondary liver tumours that cannot be accessed under us guidance owing to their location . 
real - time ct - fluoroscopy guidance has overcome the limitations of ct in the localisation and treatment of lesions that are inaccessible to us guidance , even when the lesions are small and have a transient and rapid enhancela guida tc ha da sempre dimostrato di essere un valido approccio percutaneo al trattamento mediante rf dei tumori primitivi e secondari del fegato non raggiungibili sotto guida ecografia per sede con le medesime indicazioni e risultati . 
la guida fluoro - tc in tempo reale ha attualmente superato i limiti della tc nel localizzare quindi trattare lesioni non fattibili sotto guida ecografica anche di piccole radiol med ( 2008 ) 113 : 87100 ment in the arterial phase alone . 
gandini universit degli studi di torino , dipartimento discipline medico - chirurgiche , sezione di radiodiagnostica , cattedra di radiologia , via genova 3 , 10026 torino , italy correspondence to : g . 
mattone , istituto di radiologia delluniversit di torino , via genova , 3 , 10026 torino , italy , tel . : + 39 - 011 - 6335964 , fax : + 39 - 011 - 6960310 , e - mail : giorgiomatto@alice.it received : 11 december 2006 / accepted : 4 april 2007 / published online : 25 february 2008 springer - verlag 2008 abstract purpose . 
follow - up clinico : mediante scala vas si indagato il dolore percepito dai pazienti immediatamente dopo la procedura e dopo 1 , 15 , 30 , 90 , 180 e 270 giorni . 
il follow - up clinico - strumentale consente di monitorare efficacemente i pazienti individuando precocemente le eventuali complicanze . parole chiave verteroplastica follow - up crolli vertebrali osteoporosi embolia polmonare 102 introduction percutaneous vertebroplasty is an interventional procedure consisting of the injection , under fluoroscopic or computed tomographic ( ct ) guidance , of radiopaque bone cement into a diseased vertebral body to obtain pain relief and possible vertebral stabilisation . 
the treatment is indicated in subjects with osteoporotic vertebral collapse refractory to conservative management and in malignancies with severe pain related to destruction of the vertebral body ( osteolytic metastasis and myeloma )  . 
 the aim of this paper is to present our experience with a series of patients treated at our institute and to describe patient selection criteria and the technique and its possible complications . 
with regard to complications , we propose adoption of a clinical and imaging follow - up protocol designed to identify both early ( extravertebral cement leaks and pulmonary embolism ) and late ( collapse of adjacent vertebrae ) complications . materials and methods patient selection criteria radiol med ( 2008 ) 113 : 101113 introduzione la vertebroplastica percutanea una procedura di radiologia interventistica , consistente nelliniezione , sotto guida radioscopica o combinata radioscopica e tomodensitometrica , di cemento osseo radiopaco in un corpo vertebrale affetto da differenti patologie , allo scopo di ottenere un effetto antalgico e la sua eventuale stabilizzazione . 
il trattamento indicato nei soggetti affetti da crolli somatici su base osteoporotica refrattari alla terapia medica conservativa e nelle neoplasie maligne con dolore severo correlato alla distruzione del corpo vertebrale ( metastasi osteolitiche e mieloma )  . 
 lo scopo di questo lavoro presentare lesperienza maturata su un gruppo di pazienti trattati presso il nostro istituto , descrivendo i criteri di selezione dei candidati , la tecnica di esecuzione e le possibili complicanze : a proposito di queste ultime , si propone ladozione di un protocollo di follow - up clinico e strumentale che si avvalga della radiologia tradizionale finalizzato allindividuazione di quelle precoci ( i cosiddetti leak , fughe paravertebrali di cemento e le embolie polmonari ) e di quelle tardive ( come il crollo di vertebre adiacenti )  . in agreement with the guidelines of the society of interventional radiology [ 1 ] and american college of radiology [ 2 ] , the following conditions were considered indications for percutaneous vertebroplasty : 1 . 
allergy to any materials used during the procedure before the procedure , patients underwent clinical assessment to evaluate the site and intensity of pain , which had to be : severe , focal , located along the midline , exacerbated by palpation of the spinous process of the involved vertebra and by spinal flexion , and in the absence of radicular symptoms [ 3 , 4 ]  . preliminary two - view spinal radiographs were obtained to establish correspondence between pain site and fracture site . 
a magnetic resonance imaging ( mri ) study was used materiali e metodi criteri di selezione dei pazienti in accordo con le linee guida della society of interventional radiology [ 1 ] e dellamerican college of radiology [ 2 ] , si sono considerate indicazioni alleffettuazione della vertebroplastica percutanea : 1 . 
lallergia ai materiali utilizzati durante la procedura . prima dellintervento i pazienti sono stati sottoposti a visita medica per valutare la sede e lintensit del dolore , il radiol med ( 2008 ) 113 : 101113 to distinguish among acute , subacute and chronic ( where more than one vertebra was involved ) fractures and to exclude other possible causes of pain , such as herniated disc or narrow vertebral canal . 
 technical aspects all patients received adequate information about the procedural aspects , benefits and risks of vertebroplasty and were asked to give written informed consent for the procedure . the procedures were performed without general anaesthesia , as we believe the patient should remain alert to be able to report the onset of pain or radicular symptoms . 
local anaesthesia of the skin , subcutis and periosteum was achieved by administering 23 ml of 1% lidocaine for each vertebra being treated . the bone cement used in all procedures was polymethylmethacrylate ( pmma ) with the addition of barium sulphate , tungsten or zirconium dioxide . 
the injection was made via a 10to 15 - gauge steel needle cannulas 100to 150 - mm long . all procedures were done in the ct room , after positioning of a c - arm with digital fluoroscopy , under combined ct and fluoroscopic guidance . 
the quantity of cement required was determined intraprocedurally by the operator on the basis of the residual size of the vertebra and the degree of filling obtained ( mean injected volume per vertebra : 2 ml )  . 
a postprocedural ct scan , if necessary with three - dimensional reconstruction , allowed us to verify the correct distribution of cement within the vertebral body . at the end of the procedure , patients remained in a supine position for at least 60 min after application of a flat dressing and ice over the needle entry point . 
where medical conditions permitted , patients were discharged the following day after a final assessment . personal case series between 23 october 2003 and 15 january 2007 , we performed percutaneous vertebroplasty on 101 patients 30 men and 71 women aged from 37 to 87 ( mean 71.4 , median 74 ) years . 
 quale doveva avere determinate caratteristiche : essere severo , focale , localizzato lungo la linea mediana , esacerbato dalla compressione del processo spinoso della vertebra interessata e dalla flessione della colonna , in assenza di sintomi radicolari [ 3 , 4 ]  . i pazienti sono stati studiati preliminarmente eseguendo radiogrammi della colonna nelle due proiezioni di base , per accertare la corrispondenza fra sede del dolore e sede della frattura . 
uno studio con risonanza magnetica stato necessario per distinguere le fratture acute da quelle subacute e croniche ( in caso di interessamento di pi metameri ) e per escludere altre possibili cause di dolore quali unernia discale o un canale vertebrale stretto . 
un approfondimento con tomografia computerizzata servito per individuare le sedi di potenziali fughe di cemento , come in caso di discontinuit del muro somatico posteriore [ 3 , 5 ]  . aspetti tecnici tutti i pazienti sono stati preventivamente informati sugli aspetti procedurali , sui benefici e sui rischi correlati alla vertebroplastica , ed stato loro richiesto per iscritto il consenso allesecuzione del trattamento . 
lanestesia locale di cute , sottocute e periostio , stata ottenuta mediante la somministrazione di 23 ml di lidocaina all1% per ogni metamero da trattare . il cemento osseo impiegato in tutti i trattamenti il polimetilmetacrilato ( pmma ) con laggiunta di solfato di bario , di tungsteno o di ossido di zirconio . 
liniezione avvenuta mediante aghi - cannula in acciaio di 1015 g , lunghi dai 100 ai 150 mtutte le procedure sono state eseguite in sala tc , previo posizionamento di un arco a c con fluoroscopia digitale , sotto controllo combinato tomodensitometrico e radioscopico . 
parapeduncolare : vertebre toraciche e lombari . per lavanzamento degli aghi da vertebroplastica nei corpi vertebrali stato utilizzato un martello ortopedico . prima di procedere alliniezione del cemento stata sempre eseguita una biopsia con ago tranciante coassiale , utile per avere conferma della diagnosi radiologica . 
la quantit di cemento da inoculare stata decisa dalloperatore in corso di procedura in base alle dimensioni residue del metamero da trattare e al grado di riempimento ottenuto ( il volume iniettato stato in media di 2 ml per metamero )  . una scansione tc di controllo a fine procedura con eventuale ricostruzione tridimensionale ha consentito di verifi104 radiol med ( 2008 ) 113 : 101113 a total of 173 vertebral bodies were treated , distributed as follows : t5 ( 4 ) , t6 ( 4 ) , t7 ( 4 ) , t8 ( 6 ) , t9 ( 7 ) , t10 ( 10 ) , t11 ( 23 ) , t12 ( 27 ) , l1 ( 36 ) , l2 ( 20 ) , l3 ( 16 ) , l4 ( 14 ) , l5 ( 2 )  . 
a total of 114 treatment sessions was performed ; in nine patients , the procedure was repeated once or twice to treat new compression fractures at levels adjacent to treated vertebrae or to treat previously diagnosed compression fractures that had not been treated during the first session . 
in only one case was the procedure repeated on an vertebra treated in the first session : the patient was affected by a lung carcinoma metastasis involving l4 and had not experienced any improvement after the first vertebroplasty procedure . the second procedure was successful in relieving pain . in 64 patients ( 120 treated vertebrae ) , indication for the procedure was an osteoporotic compression fracture . 
in 37 patients ( 53 treated vertebrae ) , the indication was neoplastic disease , namely , bone metastasis from bronchial carcinoma ( 7 cases ) , melanoma metastasis ( 5 cases ) , multiple myeloma ( 6 cases ) , non - hodgkins lymphoma of bone ( 5 cases ) , prostate carcinoma metastasis ( 3 cases ) , pancreatic exocrine carcinoma metastasis ( 1 case ) , gastric carcinoma metastasis ( 1 case ) , renal carcinoma metastasis ( 1 case ) , medullary thyroid carcinoma metastasis ( 1 case ) , breast carcinoma metastasis ( 3 cases ) , colon carcinoma metastasis ( 2 cases ) , vertebral angiosarcoma ( 1 case ) and vertebral haemangioma ( 1 case )  . 
the mean age of these patients at the time of treatment was 63.7 ( median 64 ) years . in 49 patients , more than 1 vertebra was treated during the same session : 2 vertebrae in 36 patients , 3 in 11 and 4 in 2 . 
only 1 vertebra was treated in all the remaining sessions . assessment of results the patient population was divided into two groups : patients with osteoporotic compression fractures and patients with neoplastic vertebral involvement . 
pain relief was assessed in all patients immediately after the procedure , at 24 h , at 15 days and at 1 month . at the end of the study , we were able to extend the followup period to 9 months for 65 patients ( 41 osteoporotic and 24 neoplastic ) , to 6 months for 14 ( 9 osteoporotic and 5 neoplastic ) and to 3 months for 11 ( 7 osteoporotic and 4 neoplastic )  . 
five patients were considered lost to followup : these were subjects receiving a different antalgic treatment simultaneously or subjects who died from intervening causes . during the follow - up visits , patients were asked whether the pain had disappeared , was significantly or only moderately less , had remained unchanged or had worsened comcare la corretta diffusione del cemento allinterno del corpo vertebrale . al termine dellintervento i nostri pazienti sono rimasti in decubito supino per almeno 60 minuti , previa medicazione a piatto ed applicazione di ghiaccio sulla cute nel punto di ingresso dellago . 
i pazienti , ove consentito dalle condizioni cliniche , sono stati dimessi il giorno seguente dopo una visita di controllo . casistica personale nel periodo compreso tra il 23 / 10 / 2003 ed il 15 / 01 / 2007 sono stati sottoposti a vertebroplastica percutanea 101 pazienti , 30 maschi e 71 femmine , di et compresa , al momento del trattamento , fra i 37 e gli 87 anni ( media 71 , 4 anni , mediana 74 anni )  . 
sono state effettuate in totale 114 sessioni di trattamento ; in 9 pazienti , infatti , la procedura stata ripetuta una o due volte a distanza di tempo per il verificarsi di nuovi crolli vertebrali a livelli limitrofi a quelli precedentemente trattati o per il trattamento di crolli gi diagnosticati ma sui quali non si era intervenuti nella prima sessione terapeutica . 
in un solo caso si intervenuti nuovamente sulla stessa vertebra gi trattata nel corso della prima seduta : il paziente in questione era affetto da metastasi di carcinoma polmonare a livello del soma di l4 e non aveva tratto alcun beneficio dalla prima vertebroplastica . 
la ripetizione del trattamento ha consentito un miglioramento della sintomatologia algica . in 64 pazienti ( per un totale di 120 metameri trattati ) la patologia di base che ha posto indicazione alla procedura stata una frattura somatica da compressione su base osteoporotica . 
in 37 pazienti ( per un totale di 53 metameri trattati ) si trattato di patologia neoplastica e precisamente di metastasi ossea da carcinoma bronchiale ( 7 casi ) , metastasi ossea da melanoma ( 5 casi ) , mieloma multiplo ( 6 casi ) , localizzazione di linfoma non hodgkin ( 5 casi ) , metastasi ossea da carcinoma prostatico ( 3 casi ) , metastasi ossea da carcinoma del pancreas esocrino ( 1 caso ) , metastasi ossea da carcinoma gastrico ( 1 caso ) , metastasi ossea da carcinoma renale ( 1 caso ) , metastasi ossea da carcinoma midollare tiroideo ( 1 caso ) , metastasi ossea da carcinoma mammario ( 3 caso ) , metastasi ossea da carcinoma del colon ( 2 casi ) , angiosarcoma vertebrale ( 1 caso ) , emangioma vertebrale ( 1 caso )  . let media di questi pazienti era , al momento del trattamento , di 63 , 7 anni ( mediana 64 anni )  . in 49 pazienti si intervenuti su pi metameri nella stessa sessione di trattamento : in 36 pazienti su 2 metameri , in radiol med ( 2008 ) 113 : 101113 pared with before vertebroplasty . 
responses were scored from 1 to 5 , where 1 indicates complete pain relief , 2 significant pain reduction , 3 moderate reduction , 4 no change and 5 worsening . 
in addition , we calculated the incidence of intraprocedural cement leaks in the two groups of patients ( osteoporotic and neoplastic ) ; application of the 2 test to the results enabled us to analyse the relation between vertebral collapse aetiology and complication onset . starting with the 51st patient , we integrated clinical and imaging follow - up and studied all patients treated with radiography of the spine and chest : two - view spinal radiography and posteroanterior chest radiography were performed 24 h after the procedure ; only the spinal study was repeated 30 days later . 
spinal radiography at 24 h allows identification of the presence and location of possible bone - cement leaks ; repetition of the examination after 30 days allows further assessment of cement stability and detection of possible secondary vertebral collapse in adjacent vertebrae . 
the chest radiograph at 24 h investigates the presence of pmma pulmonary emboli , a rare but possible and potentially fatal event . results in 88% and 84% of the procedures performed on osteoporotic and neoplastic patients , respectively , we achieved pain disappearance or significant reduction . 
all patients who reported significant pain reduction or pain disappearance also experienced an improvement in mobility , unless this was affected by concurrent diseases , and were able to discontinue or reduce their use of analgesic agents . 
no patient reported pain worsening following treatment . among patients with osteoporotic vertebral collapse , five developed pain at another level , leading to a second procedure , which was successful . 
nelle restanti sessioni terapeutiche si proceduto al trattamento di un singolo metamero . valutazione dei risultati la popolazione di pazienti stata suddivisa in due gruppi : pazienti affetti da crollo vertebrale osteoporotico e pazienti affetti da localizzazione neoplastica vertebrale . 
considerata la finalit antalgica della vertebroplastica percutanea , il parametro fondamentale di valutazione dei risultati stato in entrambi i gruppi lefficacia della procedura in termini di riduzione / scomparsa del dolore . 
leffetto analgesico stato verificato in tutti i pazienti immediatamente dopo la procedura , a 24 ore , 15 giorni ed 1 mese ; al momento della chiusura del lavoro stato possibile estendere il follow - up a 9 mesi per 65 pazienti ( 41 osteoporotici e 24 neoplastici ) , a 6 mesi per 14 ( 9 osteoporotici e 5 neoplastici ) , a 3 mesi per 11 ( 7 osteoporotici e 4 neoplastici )  . 
cinque pazienti sono stati considerati persi al follow - up : si tratta di soggetti sottoposti ad una simultanea differente terapia antalgica oppure deceduti per cause intercorrenti . in occasione delle visite di controllo si domandato ai pazienti se , rispetto a prima della vertebroplastica , il dolore fosse scomparso , si fosse ridotto in maniera significativa o solo modesta , fosse rimasto invariato o fosse invece peggiorato . 
si assegnato un punteggio da 1 a 5 , ove 1 sta per completa remissione del dolore , 2 per sua significativa riduzione , 3 per modesta riduzione , 4 per non variazione ed infine 5 per peggioramento dopo la procedura . 
 i dati ottenuti sono stati elaborati ed stata calcolata la percentuale di successo del trattamento , considerando come successo terapeutico unicamente la significativa riduzione del dolore o la sua totale scomparsa ( punteggio 1 e 2 )  . 
stata inoltre calcolata lincidenza delle fughe di cemento osseo intraprocedurali nei due gruppi di pazienti osteoporotici e neoplastici ; lapplicazione del test del 2 ai risultati ottenuti ci ha consentito di studiare la correlazione tra leziologia di un crollo e linsorgenza di complicanze . a partire dal cinquantunesimo paziente , si integrato il follow - up clinico con quello radiologico , sottoponendo tutti i pazienti trattati con vertebroplastica ad un esame radiografico del rachide e del torace : il radiogramma della colonna nelle due proiezioni e quello del torace in proiezione postero - anteriore sono stati eseguiti 24 ore dopo al trattamento ; il solo studio del rachide stato ripetuto dopo 30 giorni . 
la radiografia della colonna a 24 ore consente di individuare la presenza e la posizione di eventuali leak di cemento osseo ; lo stesso esame ripetuto dopo 30 giorni costi106 radiol med ( 2008 ) 113 : 101113 fig . 
1a , b fuga di cemento nei tessuti molli ( a ) e intradiscale ( b )  . tuisce una verifica della stabilit del cemento iniettato e permette di accertare eventuali crolli secondari nelle vertebre adiacenti a quelle trattate . 
il radiogramma del torace a 24 ore indaga la presenza di emboli polmonari di pmma : evento fortunatamente raro , ma possibile e potenzialmente letale . risultati l88% e l84% dei trattamenti effettuati rispettivamente su pazienti affetti da crollo vertebrale osteoporotico e su pazienti affetti da localizzazione neoplastica stato seguito da scomparsa o significativa riduzione del dolore . 
nelle sedi trattate , il livello di analgesia raggiunto entro le prime 24 ore si mantenuto in entrambi i gruppi di pazienti pressoch costante per la durata del follow - up . 
nei casi ad esito positivo , tutti i pazienti , a seguito della riduzione o scomparsa del dolore , hanno beneficiato di un miglioramento della capacit deambulatoria , quando non impedita da patologie concomitanti , ed hanno potuto sospendere o ridurre sensibilmente lassunzione di farmaci analgesici . 
nel 12% dei pazienti osteoporotici trattati e nel 16% di quelli affetti da patologia neoplastica , si avuta solo una modesta regressione della sintomatologia a seguito della procedura , senza miglioramento nel follow - up . 
in nessun caso si registrato un peggioramento della sintomatologia dolorosa a seguito del trattamento . nel gruppo di pazienti affetti da crollo osteoporotico la presentazione del dolore ad un altro livello si verificata in 5 casi . 
approximately 20% of patients complained of mild pain arising at the treatment site immediately after the procedure , which was associated with haematoma in only one fifth of cases , and resolved rapidly and spontaneously in all cases . radiol med ( 2008 ) 113 : 101113 fig . 
3a , b fuga di cemento in una vena perivertebrale , immagine tc ( a )  . rilievo radioscopico durante la procedura ( b )  . discussion pain relief is the main goal of vertebroplasty . 
although the injected cement does not restore the collapsed vertebra to its original volume , it modifies the vertebras biomechanical characteristics , making it more resistant to compressive forces [ 68 ] and preventing further collapse . 
the resulting internal stabilisation is probably related to the mechanism responsible for complete or partial pain relief , as it reduces stimulation of the intraosseous and periosteal nerve endings by preventing micromotions of the fracture fragments [ 9 , 10 ]  . 
circa il 20% dei pazienti , infine , ha lamentato linsorgenza di una lieve dolenzia in sede di trattamento nellimmediato periodo post - procedurale , associata ad ematoma solo in un quinto dei casi e sempre di rapida e spontanea risoluzione . discussione leffetto antalgico il primo obiettivo della vertebroplastica . 
il cemento iniettato , pur senza restituire loriginario volume al corpo vertebrale collassato , ne modifica le caratteristiche biomeccaniche , conferendogli maggior resistenza alle forze di compressione [ 68 ] e prevenendone un ulteriore crollo : la stabilizzazione interna che ne deriva verosimilmente allorigine della scomparsa o riduzione del dolore , poich riduce la stimolazione delle terminazioni nervose intraossee e periostali impedendo i micro movimenti reciproci dei frammenti di frattura [ 9 , 10 ]  . 
quindi utile disporre di metodiche di imaging che permettano di datare lepoca di insorgenza di una frattura oltre che di porne diagnosi : nel nostro studio ci si avvalsi della risonanza magnetica , sfruttando i cambiamenti di segnale della spongiosa ossea in base allet della frattura [ 11 ] : le fratture acute e quelle subacute con meno di 30 giorni sono ipointense nelle sequenze t1 pesate ed iperintense in quelle t2 pesate e stir ( short t inversion recovery )  . 
 abbiamo fatto ricorso ad uno studio tc in tutte le occasioni in cui si ritenuto utile indagare lintegrit del muro somatico posteriore ( specie nelle localizzazioni vertebrali neoplastiche ) : la sua discontinuit , specie se associata alla retropulsione di un frammento osseo , aumenta il rischio di leak e di conseguente compressione delle strutture midollari nel canale vertebrale [ 12 ]  . 
in ununica occasione il trattamento percutaneo si svolto con la sola guida radioscopica con arco a c in sala angiografica , a causa di un guasto del macchinario tc durante la procedura : trattandosi del penultimo metamero lombare , il rischio di paraplegia era nullo . 
diversamente , se lavaria allimpianto tc si fosse verificata durante il trattamento di una vertebra cervicale o toracica , non avremmo ritenuto prudente proseguire sotto il solo controllo fluoroscopico , essendo la probabilit di generare complicanze neurologiche permanenti molto pi alta : non sono a noi noti casi di complicanze neurologiche permanenti segnalati in letteratura verificatisi a seguito di procedure effettuate con lausilio della guida tc , che pertanto noi riteniamo preferibile . 
 peraltro doveroso segnalare come oggi , nella maggioranza dei centri , la sola guida fluoroscopica sia considerata sufficiente nella maggior parte dei trattamenti , riservando la guida tc a soli casi selezionati ( vertebre cervicali , toraciche alte o significative alterazioni morfologiche o rotoscoliotiche del segmento scheletrico da trattare ) [ 1316 ]  . 
il monitoraggio fluoroscopico resta comunque insostituibile nel controllo real time delliniezione e progressione del cemento , consentendo il precoce riconoscimento di eventuali leak venosi o paravertebrali che potrebbero rendere necessaria una rapida interruzione o sospensione del trattamento . 
il cautelativo utilizzo della guida tc nelle sole circostanze sopra citate consente inoltre di ridurre la dose raggi al paziente , i tempi ed i costi della procedura . nella nostra esperienza , su 173 vertebre trattate si sono osservate fughe di pmma in 34 casi ( tabella 1 ) : 21 di questi leak hanno interessato i plessi venosi paravertebrale o epidurale , costituendo una potenziale origine di emboli polmonari ( che tuttavia si possono verificare anche in assenza di evidente leak venoso ) , mentre in 13 casi si trattato di fughe nei tessuti molli paravertebrali o intersomatiche . 
ordinando i leak osservati in funzione della patologia che aveva posto indicazione per il trattamento con vertebroplastica ed elaborando i dati ottenuti , ricaviamo i seguenti dati : nelle fig . 
acute and subacute fractures ( less than 30 days old ) are hypointense in t1 - weighted sequences and hyperintense in t2 - weighted and short tau inversion recovery ( stir ) sequences . 
approxiradiol med ( 2008 ) 113 : 101113 mately 1 month after a fracture , the majority of lesions becomes isointense to normal bone in both t1 and t2 sequences . 
 we used ct in all cases in which we felt it necessary to investigate posterior wall integrity ( especially in neoplastic vertebral lesions ) : posterior wall discontinuity , above all when associated with a retropulsed bone fragment , increases the risk of leakage and subsequent compression of medullary structures in the spinal canal [ 12 ]  . 
in one case only did we perform the procedure in the angiography suite using fluoroscopic c - arm guidance alone ; this was due to a breakdown of the ct unit during the procedure . however , as the vertebra being treated was l4 , the risk of paraplegia was nonexistent . 
in contrast , if the ct breakdown had occurred while treating a cervical or thoracic vertebra , we would not have considered it safe to proceed under fluoroscopic guidance alone , as the likelihood of permanent neurological complications would have been much higher . 
we therefore consider ct guidance advisable . it should , however , be noted that most centres consider fluoroscopic guidance alone sufficient in most procedures and reserve ct for selected cases ( cervical , high thoracic vertebrae or significant morphological or rotoscoliotic alterations of the skeletal segment being treated ) [ 1316 ]  . 
fluoroscopic imaging remains irreplaceable for real - time monitoring of cement injection and distribution , allowing early detection of venous or paravertebral leaks requiring prompt interruption or suspension of the procedure . 
conservative use of ct guidance limited to the cases described above , however , allows for lower doses and reduced procedure time and costs . in our experience , out of 173 vertebrae treated , pmma leaks occurred in 34 cases ( table 1 ) : 21 involved the paravertebral or epidural venous plexuses , creating a potential source of pulmonary emboli ( which may , however , arise also in the absence of evident venous leaks ) , whereas in 13 cases , they involved the paravertebral or intersomatic soft tissue . 
by ordering the leaks observed according to the indication for vertebroplasty , we derived the following data : of 120 treated osteoporotic vertebrae , 23 cases developed leaks , equal to 19% of procedures ; of these , 14 were venous ( 61% ) and nine paravertebral or discal ( 39% )  . 
of the 53 treated neoplastic vertebrae , 11 cases had leaks , equal to 21% of procedures , of which seven were venous ( 64% ) and four paravertebral ( 36% )  . 
consequently , the results of our study are in disagreement with those re120 vertebre osteoporotiche trattate si sono verificati leak in 23 casi , pari al 19% delle procedure , dei quali 14 venosi ( 61% ) e 9 paravertebrali o discali ( 39% )  . 
tra le 53 vertebre affette da patologia neoplastica e sottoposte a procedura sono state accertate fughe di cemento in 11 casi , pari al 21% dei trattamenti , delle quali 7 venose ( 64% ) e 4 paravertebrali ( 36% )  . la differenza nellincidenza dei leak accertati tra i pazienti affetti da crollo osteoporotico rispetto a quelli verificatisi nei pazienti affetti da frattura su base neoplastica , valutata con il test del 2 , non statisticamente significativa ( p > 0 , 05 )  . 
i risultati del nostro studio , quindi , sono in disaccordo con quelli di altri autori [ 12 , 17 ] che associano alla natura tumorale di un crollo vertebrale sottoposto a vertebroplastica un aumentato rischio di fughe di cemento osseo , identificandone la causa nellazione erosiva della neoplasia sulla limitante somatica . nonostante la ricca vascolarizzazione delle lesioni vertebrali neoplastiche , la natura dei crolli trattati anche risultata statisticamente ininfluente nella determinazione di un leak venoso piuttosto che paravertebrale / discale non venoso . i risultati del nostro studio dimostrano come la vertebroplastica percutanea sia efficace nel ridurre il dolore provocato da localizzazione neoplastica e da fratture osteoporotiche . 
i pazienti che abbiamo sottoposto alla procedura hanno riferito la scomparsa o la significativa riduzione del dolore immediatamente dopo la procedura e dopo 24 ore nel 88% dei casi quando colpiti da crollo osteoporotico , e nel 84% quando affetti da localizzazione neoplastica . 
in nessun soggetto si avuto un peggioramento della sintomatologia , mentre i pazienti che non hanno tratto sollievo in maniera significativa dal trattamento erano affetti da fratture datate oltre sei mesi . il nostro follow - up clinico ha previsto controlli a 15 e 30 giorni , ripetuti a 3 , 6 e 9 mesi . 
la riduzione del dolore ottenuta nella sede trattata immediatamente dopo la procedura si mantenuta costante per la durata del follow - up in tutti i pazienti . nei pazienti neoplastici la ricomparsa del dolore nella sede trattata o in altri livelli condizionata dalla progressione della malattia . 
la recidiva non controindica peraltro la ripetizione della procedura ; nella nostra esperienza , 3 dei 37 pazienti neoplastici trattati sono stati sottoposti con successo ad una nuova procedura in seguito allestensione della malattia ad altri metameri o a recidiva nello stesso gi trattato . 
recidive del dolore in pazienti colpiti da crolli osteoporotici possono essere causate dalla frattura di metameri adiacenti : alcuni studi ipotizzano una relazione tra le rinvigorite caratteristiche biomeccaniche della vertebra trattata ed il crollo dei metameri osteopenici adiacenti [ 22 , 23 ]  . 
la naturale tendenza della malattia osteoporotica a produrre fratture vertebrali multiple in metameri adiacenti 110 radiol med ( 2008 ) 113 : 101113 table 1 venous and paravertebral leaks observed in our study , grouped by primary disease treated vertebrae venous leaks paravertebral / discal leaks osteoporotic vertebrae neoplastic vertebrae total leaks total vertebrae vertebre osteoporotiche vertebre neoplastiche totale leak totale vertebre tabella 1 leak venosi e paravertebrali occorsi nella nostra casistica , raggruppati per patologia di fondo vertebre trattate leak venosi leak paravertebrali / discali ported by other authors [ 12 , 17 ] who found vertebroplasty of neoplastic vertebral collapse to be associated with a higher risk of cement leakage , attributing the cause to end - plate erosion by the neoplasm . despite the rich vascularity of neoplastic vertebral lesions , the nature of the vertebral fractures treated was not found to correlate statistically with venous or nonvenous paravertebral / discal leaks . the results of our study demonstrate the efficacy of percutaneous vertebroplasty in reducing pain induced by neoplastic lesions and osteoporotic compression fractures . 
patients treated with the procedure reported complete or partial pain relief immediately after the procedure : 24 h after in 88% of cases of osteoporotic fractures and in 84% of cases of neoplastic fractures . 
no patient reported pain worsening , whereas patients who failed to benefit significantly from the procedure were affected by fractures more than 6 months old . clinical follow - up involved visits at 15 and 30 days and at 3 , 6 and 9 months . 
recurrence is not , however , a contraindication for repeat procedures ; in our experience , three out of 37 neoplastic patients were treated successfully with a second procedure following disease extension to other vertebrae or recurrence in a treated vertebra . 
pain recurrence in patients with osteoporotic vertebral collapse may be related to the fracture of adjacent vertebrae : some studies have hypothesised a relationship between the strengthened biomechanics of a treated vertebra and the collapse of adjacent osteoporotentro un breve spazio di tempo osservata da altri autori [ 24 ] , associata alla perdita di sostanza ossea che si verifica nei corpi vertebrali adiacenti a quelli interessati da un crollo [ 25 ] , tenderebbe a minimizzare il ruolo della vertebra sottoposta a vertebroplastica nella patogenesi di queste nuove fratture . 
nella nostra esperienza , in 8 dei 64 pazienti ( pari al 12 , 5% ) sottoposti a vertebroplastica per il trattamento di una frattura osteoporotica si sono verificati nuovi crolli in metameri limitrofi , sempre entro 30 giorni dallesecuzione della procedura . 
in tutti i casi il trattamento delle nuove fratture ha consentito di risolvere la sintomatologia algica . il riscontro di 3 casi asintomatici di embolia polmonare da polimetilmetacrilato , diagnosticati casualmente in pazienti trattati con vertebroplastica che si erano successivamente sottoposti al routinario controllo radiografico del torace in vista di un intervento chirurgico , unitamente al crescente numero di casi analoghi segnalati in letteratura [ 2630 ] , ci ha fatto sentire la necessit di adottare un sistema di follow - up radiologico , da affiancare a quello clinico gi in corso , capace di individuare precocemente questo tipo di complicanza . 
si cos deciso di sottoporre a radiografia del torace tutti i pazienti trattati con vertebroplastica 24 ore dopo la procedura ; nella stessa occasione si effettua un radiogramma del rachide , da ripetersi poi a 30 giorni in concomitanza con la visita di controllo . il nostro follow - up strumentale si pone cos i seguenti scopi : il riconoscimento precoce delle embolie polmonari da pmma ; il controllo della disposizione del cemento iniettato ; radiol med ( 2008 ) 113 : 101113 ic vertebrae [ 22 , 23 ]  . 
the natural tendency of osteoporosis to produce multiple fractures in adjacent vertebrae within a short time interval noted by other authors [ 24 ] , associated with the bone loss occurring in vertebrae adjacent to those affected by collapse [ 25 ] , would tend to minimise the role of the treated vertebra in the pathogenesis of these new fractures . 
in all cases , treatment of the new fracture achieved pain relief . the finding of three asymptomatic cases of pulmonary embolism due to pmma , incidentally detected in patients who subsequently underwent routine preoperative chest xray , combined with the growing number of similar cases reported in the literature [ 2630 ] , prompted us to add radiological follow - up to the clinical follow - up already in place to ensure early detection of this type of complication . 
we thus decided to perform chest radiography 24 h after vertebroplasty on all treated patients ; on this occasion , we also obtained a spinal radiograph , which was repeated at the follow - up visit at 30 days . 
 our imaging follow - up has the following aims : to detect pmma pulmonary emboli early on to check distribution of the injected cement to search for secondary fractures involving other vertebral levels the sensitivity of the adopted protocol has been confirmed by one of the 51 patients included in the radiological follow - up who showed small high - density nodules ( higher than the density of normal bone ) in the left subclavian pulmonary region , referable to pmma emboli . 
the frequent reports of frankly symptomatic cases , some with negative outcome , should not , however , lead us to underestimate this complication [ 27 , 28 ] , above all in consideration of the high prevalence of chronic bronchopulmonary disease among our patients ( on average aged over 70 )  . our decision to use conventional radiology for the follow - up provides the protocol with the basic features of quality : effectiveness and efficiency . 
a patient undergoing the same number of follow - up ct studies of the same body districts would absorb an 8.5 - times higher dose . finally , none of the patients in our series experienced symptomatic complications other than temporary discomfort at the site of percutaneous access , which was reported table 2 absorbed radiation dose during radiographic and computed tomography ( ct ) exams , and ct / radiography absorption ratio for equivalent districts chest dorsal spine lumbar spine torace rachide dorsale rachide lombosacrale x - rays 0.02 0 , 02 tabella 2 dose assorbita ( msv ) nel corso di indagini rx e tc e rapporto assorbimento tc / rx per distretti equivalenti ct / x - rays 3.9 tc / rx la ricerca di fratture secondarie alla procedura , eventualmente verificatesi ad altri livelli . a conferma della sensibilit del protocollo adottato , in uno dei 51 pazienti gi inclusi nel follow - up radiologico sono state identificate piccole formazioni nodulari a densit elevata ( superiore a quella dellosso normale ) in sede polmonare subclaveare sinistra , attribuibili ad embolizzazione da polimetilmetacrilato . 
anche questo paziente , come quelli oggetto di diagnosi occasionale , non lamentava sintomi riferibili ad embolia polmonare ; il riscontro in letteratura di alcuni casi francamente sintomatici , talora ad evoluzione infausta , non ci deve per far sottovalutare questa complicanza [ 27 , 28 ] , soprattutto in considerazione dellalta prevalenza di broncopneumopatie croniche tra i nostri pazienti ( mediamente ultrasettantenni )  . la scelta della radiologia tradizionale quale metodica di imaging da utilizzare nel follow - up dei pazienti trattati fa acquisire al nostro protocollo le caratteristiche fondamentali della qualit : efficacia ed efficienza . 
esso efficace per la sua sensibilit , mentre efficiente in termini di costo , inteso sia come spesa sanitaria , sia come irradiazione del paziente ( tabella 2 ) : lesecuzione dei tre controlli radiografici in questione comporta lassorbimento di una dose media di 2 , 02 msv . 
un paziente sottoposto allo stesso numero di controlli tc dei medesimi distretti assorbirebbe una dose 8 , 5 volte superiore . infine , nella nostra casistica non si presentata alcuna complicanza sintomatica , fatta eccezione per il transitorio fastidio nella zona dellaccesso percutaneo , riferito da circa il 20% dei pazienti e associato ad ematoma in un quinto dei casi . 112 radiol med ( 2008 ) 113 : 101113 by approximately 20% of patients and associated with haematoma in one fifth of cases . conclusioni conclusions percutaneous vertebroplasty is a minimally invasive and effective procedure for relieving pain associated with osteoporotic or neoplastic vertebral collapse . 
complications are rare and generally well tolerated ; for this to remain true , it is important to select patients accurately , use combined fluoroscopic and ct guidance to check the needle route and monitor the injection in real time , and to carefully establish the volume of cement to be injected . 
pain relief is independent of the amount of cement injected , which is , in contrast , directly related to the risk of leakage and complications . our radiological follow - up aims to detect cement pulmonary emboli early on , which is an uncommon but possible and potentially fatal complication . 
other follow - up imaging modalities have already been reported in the literature , but their use is aimed at studying the treated spine only [ 31 ]  . la vertebroplastica percutanea una procedura poco invasiva e di provata efficacia nella terapia antalgica dei crolli vertebrali su base osteoporotica o neoplastica . 
le complicanze sono rare e generalmente ben tollerate , ma per mantenerle tali importante selezionare accuratamente i pazienti , usufruire della doppia guida radioscopica - tomodensitometrica per controllare il tragitto dellago e monitorare in tempo reale la fase di iniezione , stabilire con attenzione il volume di cemento da iniettare . 
lelevata sensibilit della metodica di imaging prescelta e il suo basso costo in termini economici e di irradiazione , giustificherebbero ladozione del follow - up presso i vari centri che praticano la vertebroplastica , semplificandone inoltre lapplicazione presso qualsiasi altra unit di radiologia . 
the aim of this study was to evaluate the role of [ 18f ] fluorodeoxyglucose positron emission tomography / computed tomography ( fdg - pet / ct ) in the staging of hodgkins and aggressive non - hodgkins lymphoma ( hl and nhl ) , comparing it with conventional diagnostic methods , i.e. 
there was complete concordance in 54 / 65 patients ( 83.1% ) ; among the remaining 11 cases , pet upstaged eight patients ( seven true positive and one false positive ) , and downstaged three ( all false negative )  . 
lesame pet ha consentito di stadiare correttamente 61 / 65 pazienti ( 93 , 8% ) , le metodiche convenzionali 58 / 65 ( 89 , 2% ; p = ns , test 2 )  . 
nella stadiazione , entrambe le tecniche risultavano concordare in 54 / 65 casi ( 83 , 1% ) ; nei restanti 11 casi , lesame pet ha determinato una sovrastadiazione in 8 pazienti ( 7 veri positivi ed 1 falso positivo ) e una sotto - stadiazione in 3 casi ( tutti falsi negativi )  . 
fdg - pet / ct should therefore be used routinely in the initial evaluation of both patient subgroups . keywords fdg - pet / ct hodgkins lymphoma aggressive non - hodgkins lymphoma disease staging diagnostica dellesame fdg - pet / tc nella stadiazione dei lh e lnh . 
questo ne suggerisce un uso di routine nelliter di stadiazione . parole chiave fdg - pet / ct linfoma di hodgkin linfoma non hodgkin stadiazione introduction introduzione despite several attempts to improve the efficiency of treatment regimens , in only 50% of patients diagnosed with aggressive non - hodgkins lymphoma ( nhl ) and 80% of those with hodgkins lymphoma ( hl ) is the event - free survival prolonged [ 14 ]  . 
the international prognostic index ( ipi ) and the hasenclever score , including histopathological and clinical features as prognostic factors , are well - established predictors of treatment outcome and survival [ 5 , 6 ]  . 
furthermore , in patients with malignant lymphoma , accurate staging is mandatory to plan an effective chemotherapy regimen and to minimise treatment side effects and toxicity [ 7 ]  . 
conventional staging techniques , considered the reference standard , include neck , chest , abdomen and pelvic contrast - enhanced computed tomography ( ce - ct ) , uni / bilateral bone marrow biopsy ( bmb ) and in some cases magnetic resonance imaging ( mri )  . 
at present , mri is considered to be a complementary technique to ce - ct and bmb , allowing , in some anatomical districts , further and more specific information [ 11 , 12 ]  . the recent introduction of whole - body [ 18f ] fluorodeoxyglucose positron emission tomography ( fdg - pet ) scan and the use of the combined pet / ct tomographs has added a new strategic tool to this scenario , allowing abnormal metabolic tissue changes to be correlated with anatomic structures defined at ct imaging . 
in particular , fdg - pet , by studying tissue glycolytic activity , allows metabolic characterisation of morphological indeterminate nonostante i numerosi tentativi fatti per migliorare lefficacia dei protocolli terapeutici , attualmente solo il 50% dei pazienti con diagnosi di linfoma non - hodgkin aggressivo ( nhl ) e l80% di quelli con linfoma di hodgkin ( hl ) hanno una risposta completa e definitiva al trattamento [ 14 ]  . 
linternational prognostic index ( ipi ) e lo hasenclever score sono i due score pi utilizzati per predire la risposta al trattamento e la sopravvivenza di questi pazienti [ 5 , 6 ]  . 
tuttavia , permangono importanti differenze nella risposta e nella sopravvivenza di soggetti inclusi nello stesso gruppo di rischio . attualmente , lo stadio di malattia al momento della diagnosi ritenuto elemento di fondamentale importanza , sia dal punto di vista prognostico che per impostare un piano terapeutico efficace , riducendo al minimo gli effetti collaterali e la tossicit del trattamento [ 7 ]  . 
le tecniche convenzionali di stadiazione considerate il gold standard includono la tomografia computerizzata con mezzo di contrasto ( tc mdc ) delle regioni cervicale , toracica e addomino - pelvica , la biopsia osteo - midollare ( bmb ) monoe / o bilaterale della cresta iliaca e , solo in alcuni casi , la risonanza magnetica ( mri )  . 
tuttavia , ognuna di queste metodiche presenta limiti che ne riducono laccuratezza diagnostica ; in particolare la tc con mdc non consente di differenziare piccoli linfonodi tra benigni e maligni , n di differenziare il tessuto fibrotico residuo dalleventuale persistenza di malattia dopo il trattamento [ 8 ]  . 
daltra parte la bmb oltre ad essere una metodica invasiva , presenta alcuni limiti legati sia ad errori di campionamento che alla modalit di presentazione della malattia ( come nel caso dellinteressamento midollare di tipo patchy ) [ 9 , 10 ]  . 
infine la mri che attualmente utilizzata solo in alcuni casi come metodica complementare rispetto alla tc con mdc o alla bmb ; ha elevata sensibilit ma limiti di specificit [ 11 , 12 ]  . la recente introduzione della tomografia ad emissione di positroni con 18f - fluorodesossiglucosio ( fdg - pet ) e quella dei tomografi ibridi pet / tc ha aggiunto , nel campo diagnostico oncologico , uno strumento essenziale in grado di correlare le caratteristiche metaboliche specifiche dei diffe580 radiol med ( 2008 ) 113 : 578590 findings , detection of early disease before morphological changes occur and differentiation of residual tumour from scar / necrotic tissue . 
in fact , it is useful for assessing partial or complete response and differentiating residual disease from therapyinduced fibrosis and / or necrosis after completion of chemoradiotherapy [ 1719 ]  . 
a new and interesting use for fdg - pet is related to the early evaluation of chemotherapy response to identify patients not responding to treatment and who are thus candidates for different therapeutic strategies [ 20 , 21 ]  . however , the role of whole - body fdg - pet in the staging of patients with lymphoproliferative disease and its real impact on clinical outcome and treatment planning remains to be determined . 
several studies on this topic report a high diagnostic accuracy of this technique when compared with the standard staging methods [ 2225 ] both in nodal and extranodal disease and in localised bone marrow disease . 
the aim of this study was to evaluate the role of whole - body fdg - pet / ct compared with conventional staging techniques ( ce - ct and bmb ) and to evaluate its clinical impact in patients with hl and aggressive nhl . materials and methods patients population we included in our study 65 consecutive patients : 42 men , 23 women , with a median age of 46.7 ( range 1783 ) years . there were 35 cases of aggressive nhl ( 25 diffuse large b cell , six follicular grade iii , two mantle cell and two anaplastic ) and 30 cases of hl . 
fifty - two of 65 patients were at first diagnosis of disease ( 32 aggressive nhl and 20 hl ) and 13 were being evaluated for disease relapses ( three nhl and ten hl ; table 1 )  . 
all selected patients were evaluated and treated in the same haematology oncology department ; all underwent disease staging , treatment and restaging at the end of the treatment . staging procedures the clinical stage of disease was assessed according to the ann arbor classification . 
la fdg - pet / tc si dimostrata essere la pi accurata delle metodiche di stadiazione in numerosi tumori ; essa infatti consentendo di studiare lattivit glicolitica tessutale , che particolarmente incrementata nei tessuti neoplastici , permette di caratterizzare modificazioni strutturali di dubbia natura ( ad esempio il nodulo polmonare di ndd ) , identificare la presenza di cellule neoplastiche prima che queste abbiano determinato modificazioni morfologiche ( ad esempio in linfonodi di dimensioni normali ) e di differenziare la persistenza di tessuto tumorale dalla necrosi e dalla fibrosi . 
in questo campo lesame pet considerato essenziale per valutare la risposta al trattamento ( risposta parziale vs risposta completa , caratterizzazione metabolica di masse residue [ 1719 ] )  . 
un nuovo interessante uso della pet con fdg la valutazione della risposta precoce al trattamento nei linfomi di hodgkin ( ma anche nei nhl aggressivi ) con lobiettivo di identificare precocemente i pazienti non responder da candidare a trattamenti pi aggressivi [ 20 , 21 ]  . tuttavia il ruolo dellesame fdg - pet / tc nella stadiazione dei pazienti con malattia linfoproliferativa ed il suo impatto reale sulloutcome clinico e sulle strategie terapeutiche rimane da determinare . 
diversi studi su questo argomento riportano unaccuratezza diagnostica della pet pi elevata rispetto alle metodiche di stadiazione convenzionali [ 2225 ] , sia per quanto riguarda lidentificazione della malattia a livello linfonodale , sia per linteressamento degli organi parenchimatosi , sia per lidentificazione di malattia osteo - midollare . 
quindi lo scopo di questo studio quello di valutare il ruolo dellesame fdg - pet / tc nella stadiazione di pazienti con hl e nhl aggressivo , confrontandolo con le metodiche di standard ( tc mdc e bmb ) e valutandone limpatto clinico . materiali e metodi popolazione dei pazienti abbiamo incluso in questo studio 65 pazienti consecutivi : 42 maschi e 23 femmine , di et media 46 , 7 anni ( range 1783 anni )  . 
cinquantadue pazienti erano alla prima diagnosi ( 32 nhl e 20 hl ) mentre i restanti 13 presentavano ricaduta di malattia ( 3 nhl e 10 hl ; tabella 1 )  . 
tutti i pazienti inclusi sono stati studiati e trattati presso la stessa struttura complessa di ematologia ; tutti hanno eseguito stadiazione di malattia , trattamento e rivalutazione alla fine dello stesso . stadiazione lo stadio di malattia stato valutato secondo la classificazione di ann arbor . 
patients were instructed to fast for at least 6 h before the scan ; at the time of tracer injection , all patients presented a blood glucose level < 200 mg / dl . 
whole - body emission scans ( eight to nine bed positions , 2.5 min per position for the gemini ; and six to seven bed positions , 3.5 min per position for the discovery st ) were acquired beginning 60 min after the intravenous injection of fdg ( dose range 222370 mbq )  . 
the acquisition protocol started with a scout view ( a ct bidimensional projection of the patient ) , which was used to define the body axial extension ( start and end position ) over which to acquire the ct and pet data . 
once the scan range had been defined , from the base of the skull to the proximal femur , a ct scan was performed ( voltage 140 kv and tube current of 60 ma for discovery st , and 120 kv , 80 ma for gemini )  . this scan lasted approximately 1 min and was used for both anatomical localisation and attenuation correction of pet emission data . 
pet data of the whole - body distribution of the tracer were acquired in 3d mode ( from the pelvis to the neck )  . coronal , sagittal and transverse data sets were reconstructed . 
at the end of the cluso : anamnesi , esame obiettivo , esami ematologici di routine , studio ecocardiografico , tc con mdc delle regioni cervicale , toracica e addomino / pelvica , biopsia osteo - midollare bilaterale ed esame fdg - pet / tc total body . 
gli esami pet / tc sono stati acquisiti in due centri pet , utilizzando due differenti tomografi pet / tc : un gemini ( philips medical systems , cleveland , ohio , usa ) e un discovery st ( general electric medical systems , waukesha , wisconsin , usa )  . 
per lo studio pet con fdg , i pazienti sono rimasti a digiuno per almeno sei ore prima delliniezione del tracciante ; tutti prima della somministrazione presentavano livelli glicemici inferiori a 200 mg / dl . 
lesame emissivo pet ( che consisteva nella acquisizione di 89 field of view fov della durata di 2 , 5 minuti ciascuno nel caso del tomografo gemini e di 67 fov della durata di 3 , 5 minuti ciascuno nel caso del discovery st ) stato acquisito 60 minuti dopo la somministrazione endovenosa di fdg ( dose compresa tra 222 e 370 mbq )  . 
il protocollo di acquisizione dellesame pet / tc prevede inizialmente lesecuzione di uno scout view ( una proiezione bidimensionale del paziente ) che permette di definire la parte del corpo ( posizione iniziale e finale ) su cui acquisire lesame tc e quello pet . 
una volta stabilita lestensione di scansione ( normalmente tra la porzione prossimale del femore e la base cranica ) , viene acquisito lesame tc a basso dosaggio ( ld tc : 120 kv , 80 ma / s per la gemini e 140kv , 60 ma / s per la discovery st )  . 
questa scansione , della durata di circa 1 minuto , viene utilizzata sia per la correzione 582 radiol med ( 2008 ) 113 : 578590 treatment , all 65 patients underwent a second whole - body pet / ct study and ce - ct scan . standard reference all study results were subsumed in a reference standard , as there is no gold standard to confirm thepositive findings at whole - body pet and ce - ct or bone marrow biopsy were interpreted as pathologic , whereas discordant findings between pet and conventional techniques were further investigated . 
in particular , concordance between conventional diagnostics methods ( ce - ct and bmb together ) and fdgpet / ct was rated if both procedures provided the same disease stage . 
the were then investigated with further techniques [ ultrasonography ( us ) for abdominopelvic and inguinal evaluation and mri for bone marrow evaluation ] or evaluated by clinical follow - up , comparing pet and ce - ct scans acquired at staging and at the end of treatment . 
in all discordant cases , a final consensus was achieved . statistical analysis differences between disease stage with fdg - pet / ct and conventional imaging techniques were evaluated with the chi - square test , which was also used to analyse change in disease stage in patients with hl and aggressive nhl . results clinical characteristics of the 65 patients are reported in table 1 . 
whole - body fdg - pet / ct correctly staged 61 / 65 patients ( 93.8% ) , whereas conventional staging techniques correctly staged 58 / 65 cases ( 89.2% ; p = ns , chi - square test )  . in 54 out of 65 patients ( 83.1% ) , we obtained concordance on disease stage between whole - body fdg - pet / ct scan and standard staging techniques ; in the 11 remaining cases ( 11 / 65 ; 16.9% ) , there was discordance . 
eight of these 11 discordant cases were upstaged by the fdg - pet / ct scan . further studies and / or clinical follow - up confirmed this result in seven cases ( four aggressive nhl and three hl )  . 
in particular , in two patients ( one b - cell nhl and one hl ) , pet showed abdominal lymph node involvement ( lymph nodes with ct diameter < 15 mm ) , which was no longer evident in the pet / ct images acquired at the end of the treatment . 
al termine della scansione tc , la posizione del lettino viene traslata nel fov della pet per lacquisizione di questultimo . lesame pet emissivo viene acquisito in modalit 3d ( dalla pelvi alla base cranica )  . 
tutti gli esami pet / tc sono stati valutati dagli stessi due medici nucleari che hanno firmato congiuntamente tutti i referti senza essere a conoscenza dei risultati della tc mdc e della bmb . 
alla fine del trattamento tutti i 65 pazienti hanno ripetuto lesame fdg - pet / tc total body e la tc mdc . valutazione dei risultati dal momento che non esiste un gold standard di riferimento che consente di confermare i risultati dei singoli esami di stadiazione eseguiti , abbiamo proceduto come segue . 
abbiamo considerato concordanti le metodiche convenzionali ( tc mdc e bmb ) e lesame fdg - pet / tc quando entrambe le procedure hanno identificato lo stesso stadio di malattia . 
daltro lato le abbiamo considerate discordanti quando lo stadio di malattia identificato risultato essere diverso . tutti i casi discordanti sono stati rivalutati da un gruppo interdisciplinare di medici dei dipartimenti di ematologia , radioterapia , medicina nucleare e radiologia , ed investigati con ulteriori metodiche ( ecografia per la valutazione delle regioni addomino - pelvica e di quella inguinale , mri per la valutazione del midollo osseo ) o valutati con follow - up clinico ( confrontando lo studio pet / tc e quello tc mdc eseguiti al momento della stadiazione ed alla fine del trattamento )  . 
in tutti i casi discordanti , il gruppo interdisciplinare ha raggiunto un accordo finale . analisi statistica le differenze tra lo stadio di malattia identificato con la fdg - pet / tc e quello identificato con le tecniche di stadiazione convenzionale sono state valutate con il test del chi quadro ; lo stesso test stato utilizzato per analizzare il cambio di stadio di malattia nel gruppo dei pazienti con hl ed in quello con nhl aggressivo . risultati le caratteristiche cliniche dei 65 pazienti inclusi in questo studio sono riportate nella tabella 1 . 
la fdg - pet / tc total body ha consentito di studiare correttamente 61 / 65 pazienti ( 93 , 8% ) , mentre le tecniche di stadiazione convenzionali ( tc mdc e bmb ) 58 / 65 ( 89 , 2% ; p = ns , test 2 )  . 
in 54 dei 65 pazienti ( 83 , 1% ) , risultata concordanza tra lo stadio di malattia identificato col solo esame fdg - pet / ct e quello con le metodiche convenzionali ; nei restanti 11 casi ( 11 / 65 ; 16 , 9% ) discordanza . 
the remaining three out of the 11 discordant cases ( all aggressive nhl ) were erroneously downstaged by pet / ct scan ( in all of these cases , bone marrow involvement < 20% was found on bone marrow biopsy )  . 
therefore , seven out of 65 patients ( 10.7% ) were correctly upstaged by pet / ct scan : 6 / 30 ( 20% ) with initial disease stage and 1 / 35 ( 3% ) with advanced stage . 
in particular , due to the pet scan findings , six cases shifted from an initial stage ii ( five iia and one iib ) stated by conventional techniques to an advanced stage iii ( n = 4 ) and iv ( n = 2 ) ; one case shifted from an initial stage iiia to a final stage iva . in five out of the seven upstaged patients ( 5 / 65 , 7.7% ) , oncological treatment was modified ( table 2 )  . 
in patients presenting with hl , there was complete agreement in disease stage between standard techniques and fdg - pet / ct in 26 cases ( 86.7% ) ; in three cases ( 10% ) , pet / ct correctly upstaged the disease , and in one case ( 3.3% ) , the pet / ct finding was false positive . 
ulteriori approfondimenti diagnostici e / o il follow - up clinico hanno confermato il dato pet / tc in 7 pazienti ( 4 con nhl aggressivo e 3 con hl )  . 
tre degli 11 casi discordanti ( tutti nhl aggressivi ) sono stati erroneamente sotto - stadiati dalla fdgpet / tc ( in tutti la bmb ha dimostrato la presenza di un infiltrato midollare linfomatoso inferiore al 20% )  . 
pertanto in 7 su 65 pazienti ( 10 , 7% ) la pet / tc ha correttamente portato ad una sovra - stadiazione della malattia rispetto a tc mdc e bmb . 
in particolare , in seguito ad esame pet , 6 casi sono passati dallo stadio ii ( 5 iia e 1 iib ) allo stadio iii ( n = 4 ) o iv ( n = 2 ) , mentre 1 paziente passato dallo stadio iiia a quello iva . il protocollo di trattamento stato modificato in 5 dei 7 pazienti sovrastadiati ( 5 / 65 , 7 , 7% ; tabella 2 )  . 
in 2 pazienti con localizzazione di malattia a livello osteo - midollare stato aggiunto al trattamento chemioterapico , un trattamento radioterapico sulla lesione ; in altri 3 pazienti ( 2 casi con interessamento di linfonodi inguinali e splenico ed 1 caso con interessamento epatico ) vi stato un cambiamento del protocollo chemioterapico . 
nei restanti due pazienti il trattamento oncologico non stato modificato sulla base dei risultati dellesame fdg - pet / tc , poich nel primo caso , trattandosi di una recidiva della malattia , era gi stato pianificato un trapianto di cellule staminali , mentre nel secondo caso era gi stato previsto un protocollo adeguato per il trattamento di una massa bulky a livello orofaringeo . sottogruppi : hl e nhl aggressivi lesame fdg - pet / ct total body ha consentito di stadiare correttamente 29 / 30 pazienti con hl e 32 / 35 con nhl ( rispettivamente 96 , 7% e 91 , 4% ; p = ns , test 2 )  . 
nel gruppo dei pazienti con hl ( n = 30 ) stato riscontrato completo accordo nella stadizione di malattia tra tecniche convenzionali e fdg - pet / tc in 26 pazienti ( 86 , 7% ) ; in 3 casi ( 10% ) lesame pet / ct ha correttamente sovra - stadiato la malattia , mentre in un caso ( 3 , 3% ) il reperto pet / ct risultato essere falso positivo . 
nel gruppo dei pazienti con nhl aggressivo ( n = 35 ) stato riscontrato completo accordo nella stadizione di malattia tra tecniche convenzioradiol med ( 2008 ) 113 : 578590 fig . 
 [ 18f ] fluorodeoxyglucose positron emission tomography / computed tomography scan correctly identified ( and ultrasonography confirmed ) the presence of disease at the level of the inguinal lymph nodes and the spleen ( stage iiias )  . 
2 la presenza di malattia osteo - midollare evidenziata dallesame fdg - pet / tc ( e confermata dal successivo esame di mri ) , a livello del femore sinistro . the end of the staging workup , 13 of 65 patients ( 20% ) were judged to have bone marrow disease by the interdisciplinary group of physicians . 
in particular , in the six pet + / bmb cases , we had five cases of bone marrow involvement confirmed with mri and one mastocytosis ( pet false positive )  . 
published a meta - analysis of 20 nali e fdg - pet / ct in 28 pazienti ( 80% ) ; lesame pet / ct ha correttamente sovra - stadiato la malattia in 4 casi ( 11 , 4% ) , mentre i restanti 3 casi sono risultati falsi negativi ( 8 , 6% )  . malattia osteo - midollare linteressamento osteo - midollare stato valutato con lesame fdg - pet / tc total body e con la bmb ; la mri stata utilizzata in caso di discordanza . 
in particolare nei 6 casi pet + / bmb sono stati riscontrati : 5 casi di malattia midollare confermati dalla mri ed un caso di mastocitosi ( falso positivo pet )  . 
the pooled true positive value of fdg - pet was found to be 90% , with an upstaging rate ranging from 8% to 17% and a downstaging rate ranging from 2% to 23% . 
in fact , in our patient population , fdg - pet / ct correctly upstaged seven of 65 patients , but in particular , six of 30 ( 20% ) with limited disease stage . 
in contrast with isasis meta - analysis [ 26 ] , our study did not show significant differences in pet / ct diagnostic accuracy between hl and aggressive nhl subgroups . 
this finding was probably due to the fact that in the meta - analysis , several studies included patients with low - grade nhl , which is known to have a low uptake of fdg , with the risk of false negative results [ 27 ]  . fdg - pet / ct is therefore a diagnostic tool that improves the accuracy of disease staging in patients with lymphoma when compared with standard techniques . at present , in most pet centres , combined pet / ct scanmili : rispettivamente 69 , 2% vs 61 , 5% , 91 , 1% vs 100% , e 92 , 3% vs 92 , 3% . 
tuttavia , dei 13 pazienti con malattia osteo - midollare , lesame pet ha consentito di identificarne 5 negativi alla bmb . discussione nel gennaio del 2005 , isasi et al . 
 [ 26 ] hanno pubblicato una meta - analisi di 20 studi nella quale si valutava laccuratezza diagnostica della pet con fdg nella stadiazione dei linfomi di hodgkin e non - hodgki risultati di questa meta - analisi mettono in evidenza la relativa superiorit dellesame pet rispetto alle metodiche convenzionali di stadiazione ( tc mdc , bmb e / o mri )  . 
in questo lavoro , il valore predittivo positivo complessivo dellesame pet risulta essere del 90% , con una percentuale di sovra - stadiazione compresa tra 8% e 17% , ed una di sotto - stadiazione compresa tra 2% e 23% . 
i risultati del nostro studio sono in accordo con quelli di questa meta - analisi , confermando una maggiore accuratezza diagnostica dellesame fdg - pet / tc total body rispetto alle metodiche di stadiazione convenzionali ( 94 , 3% vs 89 , 2% ) , in una popolazione di pazienti con hl e nhl aggressivo . 
nel presente studio , lesame pet / tc ha portato a sovra - stadiare correttamente la malattia in 7 pazienti dei 65 ed in particolare in 6 dei 30 ( 20% ) con stadio di malattia iii . 
tuttavia , a differenza di quanto riportato nella meta - anaradiol med ( 2008 ) 113 : 578590 table 3 comparison between positron emission tomography ( pet ) and bone marrow biopsy ( bmb ) in detecting bone marrow disease bmb + bmb total * one false positive ( see text ) ; + positive ; negative table 3 confronto tra tomografia ad emissione di positroni ( pet ) e biopsia osteo - midollare ( bmb ) nellidentificazione di malattia ossea bmb + bmb totale pet + pet total pet + pet totale * un falso positivo ( vedi testo ) ; + positivo ; negativo ners are available . 
the fact that patients undergoing pet are simultaneously imaged by ct ( even though at low resolution and without contrast enhancement ) should lead us to reconsider the best diagnostic workup for staging patients with lymphoma . 
in particular , could whole - body fdg - pet / ct alone be sufficient for staging patients with malignant lymphoma , or are bmb and ce - ct still necessary ? if we take into consideration bone marrow disease , it is our opinion that pet / ct scan cannot replace bmb . 
in fact , in our patient population , although fdg - pet / ct showed similar sensitivity , specificity and accuracy to bmb , we observed a concordance between the techniques in only four cases . 
on the other hand , we had four fdg - pet / ct false negative cases ( in all of them , bmb reported a bone marrow involvement less than 20% ) and five bmb false negative cases ( fdg - pet / ct showed , and mri confirmed , a focal , patchy , nondisseminated bone marrow involvement )  . 
therefore , even if the role of fdg - pet / ct in bone marrow evaluation has yet to be defined , these results and those reported by other studies [ 28 ] suggest that the diagnostic role of the two techniques has to be considered complementary . 
in particular , pet / ct may improve the sensitivity of bmb , especially in the presence of focal ( patchy ) nondisseminated bone marrow presentation , whereas bmb alone can detect minimal bone marrow disease [ 29 , 30 ]  . 
it is also our opinion that the pet / ct scan should be the first step in lymphomastaging workup so that it could be used to guide bmb in the presence of patchy bone marrow disease . on the other hand , considering disease identification at the lymph node and parenchymal level , is fdg - pet / ct lisi di isasi , il nostro studio non ha posto in evidenza significative differenze dellaccuratezza diagnostica dellesame pet / tc tra il gruppo di pazienti con hl e quello con nhl aggressivo . 
verosimilmente questo risultato da imputare al fatto che nella meta - analisi di isasi , numerosi studi includevano pazienti con nhl a basso grado , linfomi per i quali , attualmente , nota una bassa fissazione del 18f - fluorodesossiglucosio , e dunque unalta prevalenza di casi falsi negativi [ 27 ]  . 
dunque lesame fdg - pet / tc total body un esame in grado di incrementare laccuratezza diagnostica nella stadiazione dei linfomi maligni , rispetto alla tc mdc e alla biopsia osteo - midollare . attualmente , nella maggior parte dei centri pet , vengono utilizzati tomografi ibridi pet / tc . 
per questo motivo , tenendo in considerazione il fatto che un paziente che si sottopone ad un esame pet esegue contemporaneamente un esame tc ( sia pure a bassa risoluzione e senza mezzo di contrasto ) e osservando i risultati di questo studio e quelli derivanti dalla letteratura , dovremmo forse rivalutare quale sia il migliore percorso diagnostico per la stadiazione dei linfomi di hodgkin e dei non hodgkin aggressivi . 
in particolare , possiamo pensare di utilizzare da solo lesame pet / tc con fdg oppure lesame tc mdc e la biopsia osteo - midollare sono tuttora necessari e vanno utilizzati con quello pet ? iniziando dalla biopsia osteo - midollare nostra opinione , basata sullesperienza personale ma anche su recenti pubblicazioni , che questo esame sia assolutamente necessario . in effetti , nella presente esperienza bmb e pet hanno presentato valori simili di sensibilit , specificit ed accuratezza diagnostica ; tuttavia la concordanza nei pazienti con malattia osteo - midollare stata sorprendentemente bassa ( solo 4 dei 13 pazienti con malattia osteo - midollare erano infatti positivi ad entrambe le metodiche )  . 
daltra parte , abbiamo avuto 4 casi falsi negativi allesame pet ( in tutti questi casi la bmb risultava positiva , evidenziando per uninfiltrazione midollare inferiore al 20% ) e 5 casi falsi negativi alla bmb , nei quali la pet ha mostrato e , la mri ha confermato , la presenza di interessamento midollare patchy . 
infatti la pet potenzialmente in grado di migliorare la sensibilit della biopsia osteo - midollare in quei casi in cui linteressamento midollare patchy , mentre solo la bmb in grado di identificare un diffuso interessamento midollare anche quando minimo ( e dunque non rilevabile dalla pet [ 29 , 30 ] )  . 
tutto questo porta per a suggerire , nella stadiazione del paziente con linfoma maligno , lesecuzione dellesame pet in prima battuta , in modo che le sue immagini possano eventualmente essere utilizzate come guida successiva per la biopsia osteo - midollare nel caso sia risultata la presenza di un interessamento midollare di tipo patchy . per quanto riguarda invece , la stadiazione di malattia a livello di stazioni linfonodali ed organi parenchimatosi , lesame fdg - pet / tc sufficiente da solo , oppure la tc con mdc sempre necessaria ? dai dati disponibili in letteratura , lintroduzione del tomografo ibrido pet / tc consen588 radiol med ( 2008 ) 113 : 578590 alone sufficient ? from the literature data , the availability of morphological images coregistered with functional ones seems to improve the diagnostic accuracy of pet , allowing better functional characterisation of abnormal pathological findings [ 3134 ]  . 
in particular , the introduction of combined pet / ct scanners has improved the identification and characterisation of lesions in anatomically complicated districts , such as head and neck , and / or in the abdominalpelvic region , where physiological tracer uptake may be confused with pathological lesions . 
on the utility of pet / ct with fdg in the staging patients with hl and aggressive nhl , to the best of our knowledge , there are only few papers available . 
they showed that pet / ct is more sensitive and specific than ce - ct [ 36 ] and suggested that pet / ct performed without intravenous contrast media is sufficient for staging patients with hl and aggressive nhl . 
it is our opinion that pet / ct interpreted in conference by both the nuclear medicine physician and the radiologist could replace ce - ct in most cases . in fact , fdg - pet has a high accuracy level ( the same or higher than ce - ct ) , and the evaluation of low - dose ct by an experienced reader can highlight the presence of abnormal findings in complex districts on pet , such as kidney and / or bowel , and / or lead to further investigation with cect . 
however , although our data are in agreement with other papers on pet / ct , some limitations of our study do not permit a definitive conclusion on this topic . 
furthermore , we only compared the final disease stage on pet / ct and conventional staging techniques and did not perform a lesion - by - lesion evaluation . in conclusion , our data confirm the high accuracy of fdg - pet / ct in staging hl and aggressive nhl , thus emphasising that it must be considered a standard diagnostic procedure in the initial evaluation of both patient subgroups . further studies are required to identify the best diagnostic staging technique . 
however , the combination of bmb and fdg - pet / ct , with an integrated interpretation of pet and ct findings by a nuclear medicine physician and a radiologist , should be considered the best first approach . tendo la co - registrazione di immagini funzionali ed anatomiche , migliora laccuratezza diagnostica dellesame pet , portando ad una miglior caratterizzazione funzionale dei reperti morfologici dubbi [ 3134 ]  . 
in particolare la co - registrazione di immagini pet / tc migliora lidentificazione e caratterizzazione di lesioni situate a livello di distretti anatomicamente complessi come il distretto testa - collo , o a livello della regione addomino - pelvica , dove la presenza fisiologica di accumuli di fdg pu essere confusa con quella di malattia . 
 [ 35 ] , del gruppo di essen , riportano che lesame pet / tc ha una migliore sensibilit ( 93% ) se confrontato con quello tc ( 78% ) o pet da solo ( 86% )  . 
nel loro lavoro gli autori evidenziano una maggiore sensibilit e specificit dellesame pet / tc rispetto a quello tc mdc e suggeriscono che lesame pet / tc sia sufficiente da solo per la stadiazione dei linfomi maligni.. pi recentemente raanani et al . 
 nostra opinione che la refertazione congiunta di questo esame da parte degli specialisti medico nucleare e radiologo possa , nella maggioranza dei casi , sostituire lesame tc con mezzo di contrasto . 
infatti lo studio fdg - pet ha unelevata accuratezza diagnostica ( maggiore o uguale a quella dellesame tc mdc ) , e la valutazione della tc da parte di un radiologo esperto pu evidenziare alterazioni morfologiche in distretti complicati dal punto di vista pet come quello renale o intestinale e / o richiedere luso di ulteriori indagini come quella ecografia e / o la tc con mezzo di contrasto . 
inoltre nel nostro studio abbiamo confrontato soltanto lo stadio complessivo di malattia ottenuto con lesame pet / tc a quello ottenuto con le tecniche convenzionali e non abbiamo eseguito un confronto lesione per lesione . in conclusione i nostri dati confermano lelevata accuratezza diagnostica dellesame pet / tc con fdg nella stadiazione dei pazienti con linfoma di hodgkin e in quella di pazienti con linfoma non - hodgkin aggressivo . 
simonetti dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy correspondence to : a . 
conventional breast mri consisted of the following sequences : t1 ( matrix , 288512 ) ; t2 ( matrix 225512 ) ; short tau inversion recovery ( stir ) ( matrix 320224 ) and dynamic t1 [ 2d fast - field echo ( ffe ) ] ( matrix 256512 ; temporal resolution 80 s )  . 
the sense technique included the following sequences : t1 ( matrix 512512 ) ; t2 ( matrix 512512 ) ; short - tau inversion recovery ( stir ) ( matrix 320224 ) ; dynamic t1 ( 3d ffe ) ( matrix 512512 , with a temporal resolution 70 s )  . 
confrontare in termini di qualit di immagine e analisi cinetica lesame di risonanza magnetica ( rm ) mammaria convenzionale con lesame rm acquisito con la tecnica dellimaging parallelo con scanner rm 1 , 5 t nello stesso gruppo di pazienti . 
lesame convenzionale era caratterizzato dalle seguenti sequenze : t1 ( matrice 288512 ) ; t2 ( matrice 225512 ) , da una short tau inversion recovery ( stir ) ( matrice 320224 ) e da una sequenza t1 ( 2d ffe ) dinamica post contrasto ( matrice 256512 ; risoluzione temporale 80 s )  . 
lesame acquisito con il sense era costituito da una sequenza t1 ( matrice 512512 ) , t2 ( matrice 512512 ) , stir ( matrice 320224 ) e una sequenza dinamica t1 ( 3d ffe ) ( matrice 512512 , con una risoluzione temporale 70 s )  . 
la qualit dellimmagine stata valutata assegnando a ciascuna sequenza un punteggio da 1 a 4 e i valori medi assegnati a ciascuna sequenza sono stati comparati tra i due protocolli . 
our data suggest that the sense imaging protocol applied in our study is superior to conventional imaging with regard to image quality , especially for t1 postcontrast and stir images . 
al contrario una differenza statisticamente significativa stata dimostrata tra i due protocolli per quanto riguarda la qualit delle immagini delle sequenze stir e di quelle t1 dopo contrasto acquisite con tecnica sense , rispetto a quelle acquisite con il protocollo convenzionale ( p < 0 , 001 )  . 
i risultati del nostro studio suggeriscono che il protocollo sense da noi utilizzato , mostrando una qualit di immagine superiore rispetto al protocollo convenzionale soprattutto per le sequenze stir e t1 dopo mezzo di contrasto , possa essere considerato una valida alternativa ai protocolli di imaging tradizionale nella rm mammaria effettuata con scanner rm 1 , 5 t . parole chiave carcinoma mammario rm dinamica con mdc sense imaging parallelo introduction introduzione over the past decades , important advances have been made in the field of magnetic resonance imaging ( mri ) of the breast up to more recent experience that has demonstrated not only that breast cancer can be visualised on mr images but also that mammographically and clinically occult breast cancer can be detected on mr images [ 13 ]  . 
it has become increasingly clear that the diagnostic criteria for breast lesion characterisation are based either on morphologic features and enhancement kinetics using contrast - enhanced dynamic mr images [ 46 ]  . 
the aim of our study negli ultimi decenni , sono stati compiuti numerosi progressi nel campo della risonanza magnetica ( rm ) delle mammelle , fino alle pi recenti esperienze che hanno dimostrato come la rm , oltre ad essere un esame diagnostico complementare allimaging convenzionale nella diagnosi del carcinoma mammario , consente di evidenziare lesioni occulte alle indagini mammografiche ed ecografiche [ 13 ]  . 
 ormai consolidato che i criteri diagnostici per la caratterizzazione rm delle lesioni mammarie si basino sulla valutazione congiunta della morfologia e del pattern cinetico di enhancement che le lesioni presentano allo studio rm dinamico con mezzo di contrasto [ 46 ]  . 
risoluzioni spaziali elevate devono essere acquisite in intervalli di tempo breve , per poter caratterizzare con accuratezza il pattern cinetico di enhancement delle lesioni . tuttavia risoluzione spaziale e temporale sono in conflitto e nuove strategie rm sono necessarie al fine di ottimizzare i protocolli rm [ 9 ]  . 
recentemente , sono stati compiuti numerosi progressi nella tecnologia delle bobine di superficie che hanno portato allo sviluppo di nuovi e pi efficaci protocolli dacquisizione con un conseguente incremento della risoluzione spaziale ed una riduzione dei tempi di acquisizione [ 10 ]  . 
il pi recente sviluppo tecnologico per la riduradiol med ( 2008 ) 113 : 465476 was to compare conventional breast mri and breast mri acquired with the sense technique on a 1.5 t scanner in the same patients , on the basis of image quality and kinetics analysis . materials and methods patients the study group included 31 patients ( mean age 53 years ; age range 4074 ) with x - ray mammography and ultrasonography ( us ) suspicious for malignancy . 
all lesions classified as benign at core biopsy and lesions with a low level of suspicion on conventional imaging and mri were followed up by mri and mammography for at least 12 months . 
the study was approved by our institutional review board , and all patients gave their written informed consent . magnetic resonance technique all mri examinations were performed on a 1.5 - t wholebody mri system ( intera , philips medical systems , best , the netherlands ) twice : once with the standard dynamic protocol , and once with the use of sensitivity - encoding ( sense ) technology . 
lo scopo del nostro studio stato quello di confrontare , in termini di qualit di immagine e di analisi cinetica , limaging rm convenzionale delle mammelle con limaging rm acquisito con tecnica sense , nello stesso gruppo di pazienti utilizzando uno scanner rm a 1 , 5 t . 
le lesioni che sono state classificate come benigne alla core biopsy o che allimaging convenzionale e rm mostravano un basso sospetto di malignit , sono state sottoposte a follow - up rm e mammografico con cadenza annuale . 
tutte le pazienti hanno firmato un consenso informato allo studio . tecnica rm gli esami rm sono stati eseguiti con unapparecchiatura rm a 1 , 5 t ( intera , philips medical systems , best , olanda )  . tutte le pazienti sono state sottoposte allesame rm due volte , una volta utilizzando una tecnica standard e laltra utilizzando la tecnologia sense . 
all t1 dynamic sequences were acquired after a bolus injection of 0.1 mmol / kg of gadolinium dimeglumine ( magnevist ; schering , berlin , germany ) at an injection rate of 2 ml / s , followed by a 20 - ml saline flush . 
each observer recorded morphological characteristics such as lesion shape ( round , oval , irregular or stellate ) , margins ( smooth , irregular or spiculated ) and internal architecture ( homogeneous , heterogeneous , enhancement or low - signal intensity internal septations )  . 
quantitative assessment of lesion relative enhancement rates were calculated according to the pattern : [ ( post - contrast signal intensity ( si ) precontrast si ) / pre - contrast si ] 100 ( % )  . 
the qualitative features of the si / time curves , such as the presence of persistent enhancement ( type 1 ) , plateau ( type 2 ) or washout ( type 3 ) , were analysed as described elsewhere [ 12 ]  . mri findings , according to the fisher score , were classified into breast imaging - reporting and data system ( bi - rads ) categories [ 12 ]  . 
images were displayed in a pairwise fashion to allow direct comparison of images obtained with the standard protocol and the sense protocol . readers were blinded to the protocol with which the respective images were acquired . 
image quality was subjectively rated on a scale of 1 ( poor image quality ) to 4 ( excellent ) on the basis of the presence or absence of radiofrequency ( rf ) inhomogeneity artefacts , motion and susceptibility artefacts . rf inhomogeneity artefacts were defined as the presence of an undesired variation in signal intensity across the image due to a nonuniform b1 field or an nonuniform sensitivity in the receive - only coil . 
successivamente allacquisizione della survey e della reference scan , sono state acquisite le seguenti sequenze : t1 ( tse ) ( tr / te 6 , 8 / 3 , 3 ms ; spessore , 2 , 5 mm , gap 0 ; matrice , 512512 ) ; t2 ( tse ) ( tr / te 3800 / 140 ms ; spessore , 2 , 5 mm , gap 0 ; matrice , 512512 ) ; una sequenza short tau inversion recovery ( stir ) ( tr / te / ti / 4 , 000 / 42 / 155 ms ; 2 , 5 mm spessore , gap 0 ; 320224 matrice ) ed unacquisizione dinamica t1 ( 3d ) ( ffe ) ( tr / te 7 , 9 / 3 , 9 ms ; flip angle , 25 ; matrice 512512 ; spessore , 2 , 5 mm ; 8 dinamiche ; con una risoluzione spaziale 70 s per ciascuna dinamica )  . tutte le sequenze t1 dinamiche sono state acquisite previa iniezione a bolo di gadolinio ( acido gadopentetico e sale dimegluminico , magnevist ; schering , berlino , germania ) 0 , 1 mmol / kg somministrato ad un flusso di 2 ml / s , seguito da un bolo di 20 ml di soluzione fisiologica . 
sono state valutate da ciascun osservatore le caratteristiche morfologiche della lesione , quali , la forma ( rotonda , ovale , irregolare , o stellata ) , i margini ( regolari , irregolari , o spiculati ) e larchitettura interna ( enhancement omogeneo , eterogeneo , o presenza di setti interni ipointensi )  . 
per la valutazione del rapporto intensit segnale / tempo ( is / t ) sono state disegnate manualmente delle regioni di interesse ( roi ) ( 33 pixels ) allinterno delle lesioni sospette in corrispondenza dellarea di maggior enhancement . 
le caratteristiche delle curve is / t , come la presenza di enhancement persistente ( tipo 1 ) , plateau ( tipo 2 ) o wash - out ( tipo 3 ) , sono state analizzate come descritto altrove [ 12 ]  . 
 analisi della qualit delle immagini per lanalisi prospettica della qualit delle immagini , tutte radiol med ( 2008 ) 113 : 465476 the imaging sequence or as the movement of a small portion of the imaged object . 
susceptibility artefacts were defined as microscopic gradients or variations in the magnetic field strength that occur near the interfaces of substances , with different magnetic susceptibility causing dephasing of spins and frequency shifts of the surrounding tissues . 
 statistical analysis owing to the nonnormal distribution of most variables , nonparametric statistical methods ( pairwise wilcoxon test ) were used to compare both the image quality scores and the relative enhancement rates obtained with the two imaging protocols . 
for statistical evaluation of differences between the qualitative features of the si / time curves achieved with the two protocols an exact wilcoxon signed rank test for dependent samples was performed . 
la qualit delle immagini stata soggettivamente valutata attraverso lattribuzione di un punteggio da 1 ( qualit delle immagini scarsa ) a 4 ( qualit delle immagini eccellente ) in base alla presenza o allassenza di artefatti da disomogeneit del campo magnetico , movimento e artefatti da suscettibilit magnetica . 
gli artefatti da disomogeneit del campo magnetico sono definiti come la presenza di una indesiderata variazione dellintensit di segnale nellimmagine dovuta a non uniformit del campo b1 o a non uniforme sensibilit della bobina di ricezione . 
gli artefatti da movimento ( come il movimento della paziente , movimenti respiratori o da battito cardiaco e pulsazioni vascolari ) sono state definite sia come il movimento dellintero oggetto durante lacquisizione della sequenza sia come il movimento di parte di esso . 
gli artefatti da suscettibilit sono stati definiti come gradienti microscopici o variazioni nellintensit del campo magnetico che si verificano a livello delle interfacce di tessuti aventi differente suscettibilit magnetica , causando un defasamento degli spins e uno shift nelle frequenze di risonanza dei tessuti circostanti . 
of the 27 malignant lesions , 16 were infiltrating ductal carcinomas , five invasive lobular cancer , three mixed ductal / lobular carcinomas and three were ductal carcinoma in situ . 
for the benign lesions , the patients were 1854 years old , and the lesion dimension ranged from 15 mm to 53 mm ( mean diameter 24 mm )  . 
three lesions identified with both the standard protocol and the sense protocol in three patients , who had fibrocystic disease with focal adenosis at final diagnosis , yielded three false - positive ( bi - rads 4 ) results . 
i risultati ottenuti sono stati confrontati . analisi statistica per confrontare sia la qualit delle immagini che le percentuali relative di enhancement nonch le caratteristiche qualitative delle curve is / t dei due protocolli stato utilizzato il test non parametrico wilcoxon dei ranghi con segno . 
le pazienti con carcinoma mammario avevano unet compresa tra 33 e 77 anni e le dimensioni del tumore variavano tra 4 mm e 42 mm ( diametro medio 13 mm )  . 
relativamente alle lesioni benigne , le pazienti presentavano et compresa tra 18 e 54 anni e dimensioni delle lesioni comprese tra 15 mm e 53 mm ( diametro medio 24 mm )  . 
queste lesioni sono state prospetticamente e indipendentemente identificate mediante protocollo sense . due ulteriori lesioni sono state individuate utilizzando immagini ottenute con tecnica sense in una donna di 63 anni che presentava una lesione sospetta al seno destro . 
tuttavia , la dimostrazione di queste due foci additivi mediante lutilizzo del protocollo sense non ha modificato il trattamento della paziente poich una malattia multicentrica era gi stata diagnosticata con il protocollo di imaging convenzionale . 
a dynamic subtraction magnetic resonance ( mr ) image of first postcontrast acquisition of conventional 2d gradient echo , ( matrix , 256256 , temporal resolution 80 s )  . 
b dynamic subtraction mr image of first postcontrast acquisition of sensitivity - encoding ( sense ) imaging examination protocol ( matrix , 512512 with temporal resolution 70 s )  . 
nella sequenza sense si riconoscono , oltre queste lesioni , ulteriori focolai neoplastici ( b , frecce )  . inoltre i margini spiculari sono meglio definiti nellimmagine acquisita con il protocollo sense ( d , testa di freccia )  . 
le categorie bi - rads , assegnate per lesione e non per seno , sono risultate identiche nei due protocolli in 62 / 64 lesioni ( 97% )  . analisi cinetica discussion in our study , we compared conventional breast mri with breast mri acquired with the sense technique with a 1.5 - t scanner in the same patients on the basis of image quality non sono state osservate significative differenze tra le percentuali relative medie di enhancement ( protocollo standard vs protocollo sense , 99 , 80 , 6 vs 101 , 30 , 6 , p > 0 , 05 )  . le caratteristiche qualitative della curva is / t , quali persistente enhancement , plateau e washout determinate per 472 radiol med ( 2008 ) 113 : 465476 fig . 
b dynamic subtraction mr image of first postcontrast acquisition of sensitivity - encoding ( sense ) imaging examination protocol ( matrix , 512512 with temporal resolution 70 s )  . 
c , d particolari ingranditi della lesione , rispettivamente di a e b . il tipico aspetto rm del fibroadeonoma , con margini ben definiti e setti interni che non mostrano incremento dellintensit del segnale , appaiono meglio riconoscibili sullimmagine ottenuta con protocollo di studio sense ( b e d , frecce )  . 
3a - d axial precontrast t1 magnetic resonance ( mr ) images and corresponding subtracted images for a 44 - year - old woman with previous breast cancer who underwent mr imaging for follow - up . 
a , b standard dynamic protocol ( matrix , 256256 , temporal resolution 80 s ) : the lesion appear as a nodular mass with smooth borders on the precontrast image ( a ) ; first postcontrast subtracted image ( b )  . 
3a - d immagini rm assiali t1 - dipendenti pre e post - contrastografiche di una donna di 44 anni , gi operata di carcinoma mammario , che ha effettuato lesame per controllo . 
la lesione appare come una massa nodulare con margini lisci sia nellimmagine pre - contrastografica ( a ) , sia in quella dopo mezzo di contrasto ( b )  . 
breast mri is increasingly used in addition to ciascuna lesione , sono risultate simili nei due protocolli ( p > 0 , 05 )  . qualit dellimmagine il punteggio complessivo assegnato alla qualit complessiva dellimmagine ottenuto con il protocollo sense risultato superiore rispetto al protocollo convenzionale ( protocollo standard vs protocollo sense , 2 , 70 , 5 vs 3 , 20 , 5 , p < 0 , 05 )  . 
 discussione in questo studio abbiamo confrontato in termini di qualit di immagine e analisi cinetica dellenhancement , limaging rm convenzionale delle mammelle con limaging rm ottenuto mediante limpiego della tecnica sense nello stesso gruppo di pazienti utilizzando uno scanner rm 1 , 5 t . 
in particolare , differenze significative sono state osservate nei punteggi assegnati alle immagini t1 post contrasto ( p < 0 , 001 ) e alle immagini stir ( p < 0 , 001 )  . 
le percentuali medie relative di enhancement e le caratteristiche qualitative delle curve is / t , ottenute con i due diversi protocolli desame sono risultate sovrapponibili ( p > 0 , 05 )  . 
la rm della mammella sempre pi frequentemente utilizzata in associazione alle modalit di imaging convenzionale quale la mammografia e lecografia mammaria per la diagnosi del carcinoma della mammella [ 1315 ]  . 
un esame rm dinamico della mammella per essere affidabile dal punto di vista diagnostico deve essere acquisito con una elevata risoluzione spaziale in un intervallo di tempo compreso tra 60120 s . 
a differenza della risoluzione temporale ( per cui unulteriore incremento della risoluzione temporale al di sotto di 60 s non comporta alcuna informazione diagnostica aggiuntiva ) , lincremento della risoluzione spaziale estremamente vantaggioso , purch si mantengano accettabili valori di snr [ 1719 ]  . 
con la tecnica sense , a differenza di quanto avviene utilizzando bobine phased array , i singoli elementi del474 radiol med ( 2008 ) 113 : 465476 conventional breast imaging modalities , such as mammography and breast us [ 1315 ]  . 
unlike temporal resolution ( in which a further increase beyond the 60 - s limit does not bring any additional diagnostic information ) , improving spatial resolution is highly advantageous provided acceptable snr levels are maintained [ 1719 ]  . 
with the sense technique , unlike what happens with phased - array coils , the coil elements are not used to cover separate anatomical regions to increase the snr but are used to simultaneously measure the same region , with an increase in scan speed [ 20 , 21 ]  . 
the sense reconstruction algorithm separates the superimposed signals using information on the individual coil sensitivities and restores the full fov image . in general , sense reduces scanning time at the expense of a decrease in snr that is equivalent to reducing the number of excitations . 
 [ 22 ] using sense combined with a 2d gradient echo dynamic pulse sequence with a 1.5t scanner were able to increase the spatial resolution to a 400 / 512 imaging matrix , keeping the temporal resolution at 1 min and without affecting image contrast . 
indeed , compared with 2d sequences , 3d pulse sequences offer a higher snr , which can be traded for improving spatial resolution ( increased thinner section thickness or higher matrix )  . 
this is because 3d imaging has a lower temporal resolution and suffers significantly more from image degradation due to all kinds of artefacts , including field inhomogeneities and motion artefacts [ 19 ]  . 
indeed , in our study , by using the sense technique combined with 3d pulsed sequences , while preserving kinetic data , we were able to obtain images with a higher quality score compared with the standard 2d protocol without sense . 
in their conclusions , they state that the sense technique has resulted in fewer recalls for breathing la bobina non sono utilizzati per coprire differenti regioni anatomiche per incrementare il rapporto segnale - rumore ( snr ) , ma sono utilizzate per campionare il segnale proveniente dalla stessa area , con il conseguente aumento della velocit di acquisizione [ 20 , 21 ]  . 
van den brink et al . [ 22 ] utilizzando la tecnica sense associata a sequenze pulsate 2d gradient echo dinamiche con uno scanner a 1 , 5 t , sono stati in grado di aumentare la risoluzione spaziale utilizzando una matrice pari a 400 / 512 , mantenendo la risoluzione temporale 1 minuto senza modificare il contrasto dellimmagine . 
nel nostro studio il guadagno in termini di rapidit di acquisizione ottenuto mediante lutilizzo della tecnica sense stato impiegato per aumentare la risoluzione spaziale utilizzando sequenze 3d con matrice elevata e con spessore di strato sottile . 
le sequenze 3d offrono , rispetto alle sequenze 2d , un maggiore snr , che pu essere sfruttato per migliorare la risoluzione spaziale ( riduzione dello spessore di strato o matrice pi elevata )  . 
questo perch limaging 3d ha una minore risoluzione temporale e risente in misura significativamente superiore della degradazione della qualit dellimmagine dovuta a qualunque tipo di artefatto , compresi gli artefatti da disomogeneit del campo magnetico e gli artefatti da movimento rispetto alle sequenze 2d [ 19 ]  . 
infatti , come dimostrato nel nostro studio , limpiego della tecnica sense in associazione a sequenze pulsate 3d , preservando i dati cinetici , ha permesso di ottenere immagini di qualit superiore in confronto a quelle ottenute con protocollo 2d standard senza sense . 
questi autori hanno valutato laccuratezza diagnostica di tre differenti protocolli dinamici 3d per lo studio rm della mammella acquisiti con tecnica sense ed eseguiti con apparecchiatura rm 1 , 5 t . 
nelle loro conclusioni hanno riportato che lutilizzo della tecnica sense ha diminuito il numero dei richiami delle pazienti per esami rm inadeguati grazie alla diminuzione della presenza di artefatti da movimento legati alla respirazione ed al battito cardiaco o alla cattiva visualizzazione dei cavi ascellari . 
in the time period when the background signal crosses zero , more data can be obtained with sense , resulting in a better background suppression [ 20 ]  . nel nostro studio , abbiamo inoltre osservato che la qualit delle immagini stir acquisite con il protocollo sense risultato significativamente superiore rispetto al protocollo standard ( p < 0 , 001 )  . 
nellintervallo di tempo in cui il segnale di base oltrepassa lo zero , con la tecnica sense si possono ottenere molti pi dati , con una conseguente migliore soppressione di fondo [ 20 ]  . 
this study was undertaken to evaluate the accuracy of contrast - enhanced magnetic resonance angiography ( ce - mra ) in detecting renal artery stenosis using intra - arterial digital subtraction angiography ( dsa ) as the gold standard . 
results were compared with dsa , and sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy of mra were determined . 
dsa showed 51 main renal arteries ( one patient had a single kidney ) and six accessory arteries ( total number of arteries 57 ) in the 26 patients considered . 
when the presence of stenosis was considered , the readers results , respectively , were as follows : sensitivity 77% and 72% , specificity 69% and 69% , ppv 86% and 85% , npv 55% and 50% and diagnostic accuracy 75% and 71% . 
when the detection of significant stenosis was considered , the results , respectively , were : sensitivity 83% and 83% , specificity 73% and 78% , ppv 60% and 65% , npv 90% and 91% , and diagnostic accuracy 76% and 80% . 
i due lettori hanno fatto registrare , considerando la presenza di stenosi , una sensibilit del 77% / 72% , una specificit del 69% / 69% , un vpp dell86% / 85% , un vpn del 55% / 50% e unaccuratezza diagnostica del 75% / 71% , rispettivamente . 
quando si consideri invece la presenza di stenosi emodinamicamente significativa i risultati ottenuti erano i seguenti : sensibilit 83% / 83% , specificit 73% / 78% , vpp 60% / 65% , vpn 90% / 91% , accuratezza diagnostica 76% / 80% . 
la concordanza interosservatore risultava buona per la presenza di stenosi ( = 0 , 69 ) e eccellente per la presenza di stenosi significativa ( = 0 , 85 )  . 530 radiol med ( 2008 ) 113 : 529546 conclusions . 
moreover , all of the missed significant stenoses were distally located , and therefore , the failure to detect them might be related to the suboptimal spatial resolution of mra . 
la spiegazione non appare univoca , ma va rilevata in particolare let media dei pazienti indagati , superiore a quella riportata dalla maggior parte degli altri autori , che potrebbe aver giustificato una minor collaborazione dei pazienti , e la sede distale delle stenosi emodinamicamente significative non identificate , il cui mancato riconoscimento potrebbe essere legato alla risoluzione spaziale non ottimale dellangio - rm . 
va comunque rilevato che langio - rm ha dimostrato un elevato valore predittivo negativo per la presenza di stenosi significativa , aspetto di particolare rilievo clinico in quanto ci permette ai pazienti con angio rm renale normale di evitare ulteriori indagini pi invasive . parole chiave stenosi dellarteria renale ipertensione nefrovascolare angio - rm angiografia digitale introduction introduzione the term renovascular hypertension denotes the causal relationship between a renal artery stenosis and its clinical consequences , such as hypertension , ischaemia and renal failure . 
renal artery stenosis underlies hypertension in 1%5% of hypertensive patients [ 1 , 2 ] and in 5%15% of those with end - stage renal failure entering dialysis programmes each year . 
a large autopsy study has shown renal artery stenosis to be present in 10% of patients with diabetes mellitus and hypertension , in 22% of those with abdominal aorta aneurysm and in 45% of those with peripheral artery disease [ 3 ]  . the main causes of renal artery stenosis are atherosclerosis and fibromuscular dysplasia and , less commonly , arteritis , arterial thrombosis and aortic dissection . 
more than 90% of cases of stenosis are caused by atherosclerosis and the remaining 10% by fibromuscular dysplasia [ 4 ] , which affects predominantly women younger than 50 years of age and tends to involve the distal main renal artery and segmental renal arteries [ 5 ]  . 
atherosclerotic renal artery stenosis typically affects the proximal renal artery , in particular the ostium , and its prevalence increases with age , as demonstrated by a recent study that reported a 6.8% incidence of significant stenoses among the general population older than 65 years of age [ 6 ]  . 
 the prevalence is higher in patients with other concomitant conditions , such as diabetes , lower - limb arterial disease and coronary artery disease [ 7 , 8 ]  . 
moreover , it has been calculated that the mean age at onset of atherosclerotic renal artery stenosis is 77.2 years [ 6 ]  . several studies have shown that at least 30%50% of pail termine ipertensione nefrovascolare riflette la relazione causale tra una stenosi dellarteria renale ( ras ) e le sue conseguenze cliniche quali lipertensione , lischemia e linsufficienza renale . 
nei pazienti affetti da ipertensione arteriosa solo l1%5% presenta unipertensione di tipo secondario determinata da una stenosi dellarteria renale [ 1 , 2 ] , mentre nei pazienti con insufficienza renale terminale che entrano in dialisi ogni anno la ras la principale responsabile nel 5%15% dei casi . 
un ampio studio autoptico ha dimostrato unincidenza del 10% di stenosi dellarteria renale nei pazienti con diabete mellito e ipertensione , del 22% nei pazienti con aneurisma dellaorta addominale e nel 45% nei pazienti con arteriopatia periferica [ 3 ]  . le principali cause di ras sono larteriosclerosi e la displasia fibromuscolare , meno frequentemente le arteriti , la trombosi arteriosa e la dissezione aortica . 
larteriosclerosi determina poco pi del 90% dei casi di stenosi mentre la displasia fibromuscolare poco meno del 10% [ 4 ] ; questultima colpisce prevalentemente il sesso femminile in et inferiore ai 50 anni e frequentemente coinvolge la porzione distale dellarteria renale principale e i suoi rami segmentari [ 5 ]  . 
la ras su base arteriosclerotica invece colpisce le porzioni prossimali dellarteria , in particolare il tratto ostiale , e la sua prevalenza aumenta con let come dimostra un recente studio condotto in north carolina che ha riportato unincidenza del 6 , 8% di stenosi significative nella popolazione generale con pi di 65 anni [ 6 ]  . 
 la prevalenza aumenta nei gruppi di pazienti che sono affetti da altre patologie concomitanti quali il diabete , larteriopatia degli arti inferiori e la patologia coronaria [ 7 , 8 ]  . stato inoltre calcolato che let media di insorgenza di tale patologia di 77 , 2 anni [ 6 ]  . 
 radiol med ( 2008 ) 113 : 529546 tients with a haemodynamically nonsignificant stenosis ( < 60% ) will progress to a significant stenosis ( > 60% ) within 1 year of diagnosis [ 9 , 10 ] , with up to 16% total occlusions at 5 years [ 7 , 911 ]  . 
more than 20% of patients develop a shrunken kidney if stenosis is > 60% [ 7 , 11 ]  . after revascularisation , hypertension improves in two thirds of patients with significant renal artery stenosis , and in 27%80% of them [ 4 , 1116 ] renal function improves or stabilises . 
in this selected population , noninvasive modalities are preferred , which include colour - doppler ultrasound [ 17 ] , angiotensin - converting enzyme ( ace ) - inhibitor renal scintigraphy and the more recent magnetic resonance angiography ( mra ) [ 18 ] and spiral multidetector computed tomography ( ct ) angiography . the more invasive intra - arterial digital subtraction angiography ( dsa ) , regarded as the gold standard for the diagnosis of renovascular hypertension [ 3 , 13 , 1921 ] , is reserved for patients eligible for interventional endovascular treatment . the main objective of this study was to compare mr angiography and intra - arterial dsa in terms of sensitivity , specificity , negative predictive value ( npv ) , positive predictive value ( ppv ) and diagnostic accuracy . 
 materials and methods patients between october 2003 and june 2005 , 35 consecutive patients ( 18 men , 17 women ; age range 3187 years ; mean age 66.5 years ) with suspected renovascular hypertension based on clinical , laboratory and imaging findings were referred to our division for investigation . 
twenty - six of the 35 patients underwent mra of the renal arteries followed by dsa performed within 6 months ( range 1185 days ; mean 42 days ) ; in one case only was dsa performed > 3 months after mra . 
seven out of 35 patients were studied with mra of the renal arteries but did not undergo dsa because of patient refusal ( three cases ) or the nephrologists advice ( four patients with multivessel arterial disease at high risk of cholesterol embolism )  . two of the 35 patients underwent dsa only , as they had pacemakers ( absolute contraindication for mri )  . 
our study considered the group of patients ( n = 26 ) who underwent both mra and dsa . molteplici studi hanno dimostrato che almeno il 30%50% dei pazienti con una stenosi non emodinamicamente significativa ( < 60% ) progredisce verso una stenosi significativa ( > 60% ) entro un anno dalla diagnosi [ 9 , 10 ] , con un tasso di occlusione totale fino al 16% a cinque anni [ 7 , 911 ]  . 
inoltre , in pi del 20% dei pazienti si verifica una evoluzione verso il rene grinzo se la stenosi superiore al 60% [ 7 , 11 ]  . dopo rivascolarizzazione due terzi dei pazienti con stenosi renale significativa mostrano un miglioramento dello stato ipertensivo e nel 27%80% [ 4 , 1116 ] un miglioramento o una stabilizzazione della funzione renale . 
in questa popolazione selezionata dal punto di vista diagnostico attualmente si prediligono le tecniche non invasive quali leco - color doppler ( ecd ) [ 17 ] , la scintigrafia renale con ace - inibitore e le pi recenti angiografia con risonanza magnetica ( angio - rm ) [ 18 ] e angiografia con tc spirale multistrato ( angio - tc ) , riservando langiografia digitale per via arteriosa ( dsa ) , che attualmente rappresenta ancora il gold standard nella diagnostica dellipertensione nefrovascolare [ 3 , 13 , 1921 ] , ma che costituisce una tecnica invasiva , ai casi passibili di trattamento di tipo interventistico endovascolare . 
 lo scopo principale del nostro studio stato quello di confrontare in termini di sensibilit , specificit , valore predittivo negativo , valore predittivo positivo e accuratezza diagnostica langio - rm con la dsa per via arteriosa . materiali e metodi pazienti nel periodo compreso tra ottobre 2003 e giugno 2005 sono stati indagati nella nostra unit clinico operativa 35 pazienti consecutivi , 18 maschi e 17 femmine , di et compresa tra 31 e 87 anni ( media : 66 , 5 anni ) , con sospetto di ipertensione nefrovascolare su base clinica , laboratoristica o strumentale ; 6 di questi erano affetti da insufficienza renale cronica . 
ventisei su 35 pazienti sono stati sottoposti ad angio - rm delle arterie renali e successivamente , in un arco di tempo di sei mesi ( min : 1 giorno ; max : 185 giorni ; valore medio : 42 giorni ) , a dsa dello stesso distretto , che ha costituito il gold standard per il nostro studio . 
the surface coil was placed around the patient in such a way as to enable studying the vascular tree from the proximal abdominal aorta down to the iliac arteries . after a t1 - weighted balanced turbo spin - echo ( b - tse ) localising sequence and a t1 - weighted real - time 2d fastfield echo ( ffe ) sequence , images were obtained with a t1weighted 3d ffe breath - hold sequence in the coronal plane . 
we used the following technical parameters , adapted to the individual patient to ensure full coverage of the vascular territory of interest and keep acquisition times as short as possible : coil sense - body , tr 4.25.0 ms , te 1.41.6 ms , matrix 512512 , flip angle 40 , field of view 370450 mm , slice thickness 3 / 4 mm with interslice gap of 1.5 / 2 mm , 50 slices . 
the sequence was acquired before and after administration of intravenous paramagnetic contrast material to enable subsequent image subtraction and generation of 3d maximum intensity projection ( mip ) reconstructions in the coronal and sagittal plane . paramagnetic contrast material was injected through a 20 - gauge needle cannula in a peripheral vein of the arm using an mr - compatible automatic injector ( spectris ; medrad , indianola , ia , usa )  . 
fourteen of the 26 patients received 0.1 mmol / kg of a 0.5 - m contrast medium ( gadodiamide , omniscan , ge medical systems , milwaukee , wi , usa ) at a flow rate of 2 ml / s , followed by a 20 - ml saline flush at the same rate . 
in agreement with the literature [ 2225 ] , stenoses were graded according to the following classification : radiol med ( 2008 ) 113 : 529546 pazienti hanno eseguito unicamente la dsa in quanto portatori di pacemaker ( controindicazione assoluta allesecuzione della rm )  . 
la nostra analisi stata effettuata sul gruppo di pazienti ( 26 ) sottoposti ad angio - rm e dsa . procedure diagnostiche e analisi delle immagini angio - rm lesame rm stato condotto mediante limpiego di un magnete superconduttivo da 1 , 5 t ( philips gyroscan intera , best , olanda ) con gradienti da 30 mt / m e velocit di raggiungimento del picco pari a 150 mt / m / s , utilizzando la bobina per il corpo ( q - body ) e la bobina di superficie phased array ( sense - body )  . 
la bobina di superficie stata posizionata intorno al paziente in modo da poter indagare lalbero vascolare dallaorta addominale prossimale fino alle arterie iliache comprese . dopo una sequenza di centratura balanced turbo spin echo ( b - tse ) pesata in t1 e una sequenza 2d fast field echo ( ffe ) pesata in t1 real time , le immagini sono state ottenute con sequenza 3d ffe pesata in t1 acquisita sul piano coronale , in apnea respiratoria , utilizzando i seguenti parametri tecnici , modulati sul singolo paziente in modo da coprire lintero territorio vascolare di interesse e ridurre il pi possibile la durata della scansione : bobina selezionata = sense - body , tr = 4 , 25 , 0 ms , te = 1 , 41 , 6 ms , matrice 512512 , flip angle 40 , campo di vista 370450 mm , spessore di strato 3 / 4 mm con gap di 1 , 5 / 2 mm , 50 strati . 
la sequenza stata acquisita anche prima delliniezione di mezzo di contrasto paramagnetico per via endovenosa per permettere la successiva sottrazione di immagine e quindi le ricostruzioni 3d utilizzando lalgoritmo mip sul piano coronale e sagittale . il mezzo di contrasto paramagnetico stato iniettato con lausilio di un iniettore automatico rm - compatibile ( spectris ; medrad , indianola , usa ) attraverso un ago - cannula da 20 gauge posizionato in una vena periferica dellarto superiore ; in 14 / 26 pazienti stato somministrato un mdc 0 , 5 m ( gadodiamide , omniscantm , ge medical systems , milwaukee , wisconsin , usa ) nella dose di 0 , 1 mmol / kg ad una velocit di 2 ml / s , seguito dallinfusione di 20 ml di soluzione fisiologica alla stessa velocit . 
nei rimanenti 12 pazienti stato iniettato un mdc 1 m ( gadobutrolo , gadovisttm , schering , berlino , germania ) nella dose di 0 , 2 mmol / kg ad una velocit di 1 , 8 ml / s , seguito dallinfusione di 20 ml di soluzione fisiologica sempre a 1 , 8 ml / s . 
il mdc stato somministrato con tecnica di sincronizzazione bolus tracking mediante una sequenza fluoroscopica coronale gradient echo 2d ( gre 2d t1 real time ) effettuata durante la somministrazione del mdc con controllo visivo da parte delloperatore e partenza della sequenza di acquisizione non appena il segnale avesse documentato larrivo del mdc in aorta addominale . due radiologi con esperienza angiografica ( rispettivamente di 9 e 13 anni ) e di rm hanno valutato in doppio cieradiol med ( 2008 ) 113 : 529546 1 . 
occlusion ( absence of vessel enhancement ) additionally , both readers were asked to rate their confidence by adding definitely or probably to their diagnoses , resulting in an 8 - point grading scale : 1 . 
definitely occluded artery dsa all dsa examinations were performed with an integris allura system for diagnostic angiography and interventional radiology ( philips medical systems , eindhoven , the netherlands ) , which uses a digital imaging chain with charge - coupled device ( ccd ) camera technology and 1 , 0241 , 024 pixel matrix . 
for each series , an average of 30 ml of nonionic iodinated contrast medium ( iopromide 370 mgi / ml , ultravist , schering , berlin , germany ) was injected with an automatic injector ( medrad mark v , indianola , ia , usa ) at a flow rate of 1520 ml / s , for a total of approximately 90 ml . 
selective catheterisation of the renal arteries was only performed if considered necessary to establish the diagnosis . images were evaluated on screen or on film by two experienced radiologists unaware of the results on mra . 
the evaluation was carried out in a similar manner to mra , and cases of disagreement were resolved by consensus . statistical analysis co le immagini mip e le immagini di partizione . 
occlusione ( assenza di opacizzazione del vaso )  . stato inoltre chiesto ad entrambi i lettori di precisare il livello di confidenza nel giudizio espresso in termini di sicuramente o probabilmente ; ci ha portato ad ampliare la scala di valutazione come segue : 1 . 
sono state acquisite una proiezione antero - posteriore e una proiezione obliqua di circa 2030 per ogni arteria renale principale ; per ogni serie , mediante iniettore automatico ( medrad mark v , indianola , usa ) , sono stati iniettati in media 30 ml di mdc organoiodato non ionico ( iopromide 370 mgi / ml , ultravist , schering , berlino , germania ) ad un flusso di 1520 ml / s , per un totale di 90 ml circa . 
 we evaluated the sensitivity , specificity , ppv , npv and diagnostic accuracy of mra in detecting stenosis of any severity and identifying significant stenoses ( > 50% ) without considering the level of diagnostic confidence expressed by the readers . 
of the six accessory renal arteries seen on dsa , only one was identified by both readers on mra , whereas reader 2 identified two , probably lumbar , arteries as accessory renal arteries ( false positives )  . 
to summarise , 52 out of 57 arteries ( 91% ) were identified on mra . dsa : nei 26 pazienti esaminati , la dsa ha rilevato 51 arterie renali principali ( 1 paziente era nefrectomizzato ) e 6 arterie polari per un totale di 57 arterie . 
multiple arterie renali sono state identificate in quattro pazienti ; angio - rm : in tutti i pazienti , langio - rm stata considerata diagnostica da entrambi i lettori che hanno identificato tutte le 51 arterie renali principali . 
delle 6 arterie renali polari viste in dsa , solo unarteria stata identificata allangio - rm da entrambi i lettori , mentre il lettore 2 ha identificato due vasi arteriosi , verosimilmente lombari , come arterie renali polari ( falsi positivi )  . 
 presence of stenosis presenza di stenosi dsa : among the 57 renal arteries identified , dsa demonstrated 20 normal arteries ( 16 main renal arteries and four accessory arteries ) and 37 pathological arteries ( 35 main renal and two accessory arteries ) , three of which showed double stenosis . 
 occlusa totale no stenoses stenoses occlusion total overall total dsa , digital subtraction angiography stenosi assente stenosi presente occlusione totale dsa , angiografia digitale radiol med ( 2008 ) 113 : 529546 fig . 
1a - d digital subtraction angiography in a patient with two renal arteries on both sides : a , b double significant stenosis of the left main renal artery ( arrows ) , proximal stenosis of the left accessory artery ( arrowhead ) and distal stenosis of the right main renal artery ( empty arrow )  . 
1a - d angiografia digitale di paziente con due arterie renali bilateralmente : a , b doppia stenosi significativa dellarteria renale principale sinistra ( frecce ) , stenosi prossimale dellarteria accessoria sinistra ( punta di freccia ) e stenosi distale dellarteria principale destra ( freccia vuota )  . 
tre stenosi severe e 6 stenosi lievi sono state table 2 detection of stenoses and occlusions by contrast - enhanced magnetic resonance angiography ( reader 2 ) definitely probably normal normal probably definitely probably mild severe mild definitely severe probably occluded definitely occluded total radiol med ( 2008 ) 113 : 529546 dsa , digital subtraction angiography tabella 2 risultati angio - rm per la presenza di stenosi e occlusioni ( lettore 2 ) mra / sicur . 
2a - d digital subtraction angiography in a patient with two renal arteries on the right and one on the left : a nonsignificant stenosis of the right renal artery ( arrow ) and b severe stenosis of the origin of the anterior branch of the left renal artery . 
c , d magnetic resonance angiography detects both stenoses ( arrows ) and additionally shows more distal flow void , misdiagnosed as stenosis ( arrowhead ) ( false positive ) of the anterior branch of the left renal artery . 
2a - d angiografia digitale di paziente con due arterie renali a destra e una a sinistra : a stenosi lieve del tratto prossimale dellarteria principale di destra ( freccia ) e b stenosi severa allorigine del ramo prepielico di sinistra . 
langio - rm ( c , d ) documenta entrambe le stenosi ( frecce ) ed inoltre fa rilevare assenza di segnale interpretata come stenosi ( punta di freccia ) al terzo medio del ramo prepielico sinistro ( falso positivo )  . radiol med ( 2008 ) 113 : 529546 table 3 detection of significant stenoses and occlusions by contrast - enhanced magnetic resonance imaging ( reader 1 ) mra / dsa definitely probably normal normal probably definitely mild mild probably severe definitely severe probably occluded definitely total occluded stenoses 50% stenoses > 50% occlusion total dsa , digital subtraction angiography tabella 3 risultati angio - rm per la presenza di stenosi significative e occlusioni ( lettore 1 ) mra / sicur . 
 occlusa totale 25 25 15 55 stenosi 50% stenosi > 50% occlusione totale dsa , angiografia digitale stenoses and six mild stenoses were classified as normal arteries , whereas three normal arteries were judged as severe stenoses and two as mild stenoses . 
three severe stenoses and eight mild stenoses were considered as normal arteries , whereas two normal arteries were graded as mild stenoses , two as severe stenosis and one as an occlusion . 
two occlusions were correctly identified , whereas three severe stenoses were graded as occlusions . in the identification of stenosis of any severity , the two mra readers showed substantial agreement , with a value of 0.69. 
three normal arteries and seven mild stenoses were judged as severe stenoses . the results for reader 2 were as follows : 29 true - negative , 15 true - positive , three false - negative and eight false - positive findings ( table 4 )  . 
tre stenosi severe e 8 stenosi lievi sono state considerate come arterie normali , mentre due arterie normali sono state classificate come stenosi lievi , due come stenosi severe e una come occlusa . 
una ulteriore valutazione stata effettuata rifacendosi al significato clinico , considerando quindi insieme i vasi normali e i vasi con una stenosi non emodinamicamente significativa ( < 50% )  . 
il lettore 2 ha individuato correttamente 29 casi negativi e 15 positivi , mentre in 3 casi ha espresso un giudizio falso - negativo e in 8 casi un falso - positivo ( tabella 4 )  . 
3a - d selective digital subtraction angiography of both renal arteries : a , b nonsignificant stenosis on the right ( arrow ) and severe stenosis on the left ( arrowhead )  . 
c , d magnetic resonance angiography shows the right stenosis ( arrow ) and the poststenotic dilatation , which induced the readers to consider it as significant ( overestimation )  . 
3a - d angiografia digitale selettiva delle due arterie renali : a , b stenosi lieve dellarteria renale destra ( freccia ) e severa della sinistra ( punta di freccia )  . 
langio - rm ( c , d ) conferma la stenosi a destra ( freccia ) ben documentando la dilatazione poststenotica che ha indotto i lettori a giudicarla severa ( sovrastima )  . 
la stenosi a sinistra ( punta di freccia ) stata ritenuta lieve verosimilmente per la non ottimale opacizzazione del vaso ( sottostima )  . stenoses were classified as normal arteries ; five mild stenoses were graded as severe , two normal arteries were judged as significantly stenotic and one as occluded . 
in the identification of significant stenosis , interobserver agreement between the two mra readers was nearly perfect , with a value of 0.85. table 5 reports the sensitivity , specificity , ppv , npv and diagnostic accuracy that emerged from the two readers observations in identifying the presence of stenosis of any severity and of haemodynamically significant stenosis only . evaluation of lesions in relation to diagnostic confidence tables 1 and 2 show that out of 55 observations recorded , reader 1 was confident in the interpretation of 40 cases cinque stenosi lievi sono state giudicate come severe , due arterie normali sono state date come significativamente stenotiche e una come occlusa . 
nella identificazione delle stenosi significative la concordanza interosservatore tra i due lettori dellangio - rm risultata eccellente con un pari a 0 , 85 . dai rilievi dei due osservatori emergono quindi i valori di sensibilit , specificit , valore predittivo positivo e negativo e accuratezza diagnostica riportati nella tabella 5 sia nella valutazione di presenza di stenosi che di stenosi emodinamicamente significativa . valutazione delle stenosi in relazione alla confidenza diagnostica in base alle tabelle 1 e 2 si evince che , su 55 rilevazioni , il lettore 1 ha valutato con sicurezza 40 casi ( 73% ) mentre ha espresso delle riserve nel giudicare i rimanenti 15 casi radiol med ( 2008 ) 113 : 529546 table 4 detection of significant stenoses and occlusions by contrast - enhanced magnetic resonance imaging ( reader 2 ) mra / dsa definitely probably normal normal probably definitely mild mild probably severe definitely severe probably occluded definitely total occluded stenoses 50% stenoses > 50% occlusion total dsa , digital subtraction angiography tabella 4 risultati angio - rm per la presenza di stenosi significative e occlusioni ( lettore 2 ) mra / sicur . 
if we consider only confident diagnoses , the sensitivity , specificity , ppv , npv and diagnostic accuracy are those reported in table 6 . ( 27% ) ; il lettore 2 si dimostrato confidente nella diagnosi in 39 casi ( 71% ) e incerto nei restanti 16 ( 29% )  . 
considerando solamente le valutazioni certe di ogni lettore emergono i valori di sensibilit , specificit , valore predittivo positivo e negativo e accuratezza diagnostica riportati nella tabella 6 . discussion renal artery stenosis is the most common cause of secondary hypertension . 
its detection , and above all the correct evaluation of the degree of stenosis , are crucial for establishing the most appropriate treatment : antihypertensive agents , angioplasty or in rare cases surgery [ 13 , 16 ]  . noninvasive diagnostic techniques such as ultrasound , ct angiography and mra have proved to be accurate in evaluating renovascular hypertension , allowing reduction in the number of diagnostic angiograms [ 13 , 20 , 22 , 2630 ]  . 
la sua identificazione , ed in particolare la corretta valutazione del grado di stenosi , risulta di fondamentale importanza per una corretta pianificazione del trattamento : terapia farmacologica antiipertensiva , angioplastica o , raramente , trattamento chirurgico [ 13 , 16 ]  . 
tecniche diagnostiche non invasive come lecografia , langio - tc e langio - rm , si sono dimostrate accurate nella valutazione dellipertensione nefrovascolare con lo scopo di ridurre il numero di angiografie diagnostiche [ 13 , 20 , 22 , 2630 ]  . lecografia di solito utilizzata come tecnica di prima istanza per la valutazione della stenosi dellarteria renale radiol med ( 2008 ) 113 : 529546 assessing renal artery stenosis [ 27 , 31 ]  . 
the main limitations of the technique lie in the difficult acoustic window in a large number of patients , operator dependence and relatively low sensitivity and specificity in visualising accessory renal arteries [ 22 ] , which may be responsible for renovascular hypertension in a limited number of cases [ 32 ]  . ct angiography has developed considerably in recent years , thanks to technological advances and the advent of multislice technology ( multislice ct )  . 
recent reports [ 29 , 30 ] maintain that multislice ct scanners have increased the sensitivity and specificity of ct to levels similar to those of dsa and considerably improved the evaluation of the more distal vessels and accessory arteries . 
the use of ionising radiation and iodinated contrast media causing possible adverse reactions and the risk of nephrotoxicity in patients at risk make this technique potentially less advantageous than mra . contrast - enhanced mra ( ce - mra ) , first described by prince in 1993 , has rapidly become the primary method for vascular imaging [ 3335 ] , and numerous efforts have been made to refine the examination technique , especially for studying renal arteries [ 32 , 3641 ]  . 
over the years , these studies have demonstrated the value of the technique , with reported sensitivity and specificity values up to 100% . the results obtained by us in terms of sensitivity and specificity are not , however , as encouraging as those reported in the literature . 
sensitivity and specificity in our study were 72%77% and 69% , respectively , for the detection of stenosis of any severity and only a little higher without , however , reaching the values reported in the literature when considering its ability to identify significant stenoses ( sensitivity 83% , specificity 73%78% )  . 
given that our findings were in contrast with those in the international literature , it is natural to consider whether they are the result of inadequate study design or execution or whether the role of mra in the study of patients with renovascular hypertension should in fact be reconsidered . 
however , the technical parameters of the sequences used in our study were essentially identical to those used in many other studies [ 32 , 35 , 39 , 40 , 42 ] , so we believe this hypothesis to be unfounded . 
on the other hand , it is also true that on reviewing their errors in the light of dsa results , both readers recognised a less - than - perfect technique in all cases of significant stenosis found to be false negative ( three for both readers )  . 
il limite principale di tale tecnica rappresentato dalla difficile finestra acustica in un ampio numero di pazienti , dalloperatore dipendenza e da una relativa bassa sensibilit e specificit nella visualizzazione delle arterie renali accessorie [ 22 ] che possono essere responsabili , anche se in un limitato numero di pazienti , di ipertensione nefrovascolare [ 32 ]  . langio - tc una metodica che si sviluppata sensibilmente negli ultimi anni grazie ai notevoli progressi della tecnologia , in particolare con lavvento della tomografia computerizzata a strato multiplo ( tc multistrato )  . 
pubblicazioni recenti [ 29 , 30 ] sostengono che con questo tipo di apparecchiatura la sensibilit e specificit di questindagine risulta pressoch sovrapponibile a quella della dsa e che la valutazione dei vasi pi distali e delle arterie accessorie risulta notevolmente migliorata . 
lutilizzo di radiazioni ionizzanti e di un mezzo di contrasto iodato con possibili reazioni e con il rischio di nefrotossicit in pazienti a rischio rendono questa tecnica potenzialmente meno vantaggiosa rispetto allangio - rm . langio - rm con mezzo di contrasto ( ce - mra ) , descritta per la prima volta da prince nel 1993 , diventata in breve tempo lindagine di riferimento nellimaging del sistema vascolare [ 3335 ] e numerosi sforzi sono stati compiuti per migliorare la tecnica desame , soprattutto a livello delle arterie renali [ 32 , 3641 ]  . 
questi studi hanno dimostrato nel corso degli anni la validit di questa tecnica riportando valori di sensibilit e specificit fino al 100% . i risultati da noi ottenuti in termini di sensibilit e specificit , per , non sono incoraggianti come quelli della letteratura : nel nostro studio questi parametri si attestano rispettivamente sul 72%77% e sul 69% nella valutazione della presenza di stenosi e poco migliorano , senza arrivare mai ai valori della letteratura , quando si considera la capacit di individuare le stenosi significative ( sensibilit 83% , specificit 73%78% )  . 
sulla base di questi risultati , discordanti rispetto alla letteratura internazionale , viene spontaneo chiedersi se il dato ottenuto frutto di una errata conduzione dello studio o se effettivamente il ruolo di questa tecnica nello studio dei pazienti con ipertensione nefrovascolare debba essere riconsiderato . 
i parametri tecnici delle sequenze da noi impiegate sono sostanzialmente sovrapponibili a quelli utilizzati da molti autori [ 32 , 35 , 39 , 40 , 42 ] per cui non riteniamo questa ipotesi abbia fondamento . 
entrambi i lettori , comunque , rivalutando i propri errori alla luce dei dati emersi dalla dsa , hanno in effetti ravvisato una tecnica non perfetta in tutti i casi di stenosi significative risultati falsi negativi ( 3 per entrambi i lettori )  . 542 radiol med ( 2008 ) 113 : 529546 in one case of a severely stenotic renal artery judged as normal by both readers , it was stressed that enhancement of vascular structures was low , making detection of stenosis , which was also distal , very difficult . 
suboptimal enhancement was also responsible for some false - positive cases , in which normal arteries were judged as stenotic ( three cases for reader 1 ; two cases for reader 2 ) or even occluded ( one case for reader 2 )  . 
it is crucial that mra be performed during breath - holding [ 22 , 37 , 38 , 41 , 42 ] to prevent motion from further reducing the techniques suboptimal spatial resolution , especially at the level of smaller vessels . 
because the majority of renal artery stenoses are atherosclerotic and thus detected in elderly patients who are unable to hold their breath for the time required , the examination should be performed with sequence parameters optimised to reduce acquisition time as much as possible . 
 the advanced age of the patients included in our series ( mean age 66.5 years ) may be another factor that negatively affected mra image quality and consequently diagnostic performance . 
in fact , many studies that reported higher sensitivity and specificity [ 20 , 22 , 32 , 4448 ] were conducted on younger and therefore presumably more cooperative patients . finally , in one case , a stenosis at the origin of the retropelvic branch of the renal artery was missed because the readers suspected that the signal loss seen at that level was artefactual . 
it should , however , be emphasised that all these errors concerned the failure to detect distal stenoses ; this fact is not surprising in that many authors [ 21 , 42 , 4851 ] have stressed that mra is limited in depicting distal stenoses because of its suboptimal spatial resolution . even the visualisation of accessory renal arteries is affected by this limitation , as the frequently small calibre of these vessels can preclude adequate depiction . 
in letteratura , in effetti , sono pochi i lavori [ 22 , 37 , 38 , 43 , 44 ] che utilizzano una concentrazione inferiore a 0 , 2 mmol / kg , che considerata , dalla maggior parte degli autori , la concentrazione ottimale per una buona opacizzazione vasale . 
in questo caso il paziente era stato arruolato anche per un altro studio che prevedeva lutilizzo del mezzo di contrasto ad una concentrazione di 0 , 1 mmol / kg . 
lopacizzazione non ottimale stata responsabile anche di alcuni casi falsi positivi , dove arterie normali sono state date come stenotiche ( 3 casi per il lettore 1 ; 2 casi per il lettore 2 ) o perfino occluse ( 1 caso per il lettore 2 )  . 
questi 6 falsi positivi si distribuivano in numero eguale ( 3 ciascuno ) tra i due gruppi di pazienti in cui erano stati somministrati i due mezzi di contrasto diversi . in altri due pazienti non sono state individuate due stenosi distali in quanto gli artefatti da movimenti respiratori hanno ridotto la qualit dellimmagine determinando una sfumatura dei profili vasali . 
fondamentale quindi che lesame di angio - rm venga condotto in apnea respiratoria [ 22 , 37 , 38 , 41 , 42 ] per evitare che il movimento riduca ulteriormente la non ottimale risoluzione spaziale della rm , soprattutto a livello dei rami con calibro pi piccolo . 
poich la maggior parte delle lesioni stenotiche a carico dellarteria renale sono di natura arteriosclerotica e quindi si riscontrano in pazienti anziani che spesso non sono in grado di mantenere unapnea prolungata , auspicabile eseguire lesame con unottimizzazione dei parametri della sequenza in modo da ridurre al minimo la durata dellacquisizione . 
 let avanzata dei pazienti della nostra casistica ( et media 66 , 5 anni ) pu quindi essere un altro fattore che ha influenzato negativamente la qualit delle immagini di angio - rm e conseguentemente la performance diagnostica dellesame . 
in effetti in letteratura in diversi studi [ 20 , 22 , 32 , 4448 ] con risultati migliori in termini di sensibilit e specificit , il campione preso in esame era composto da pazienti pi giovani e presumibilmente pi collaboranti . in un ultimo caso , infine , non stata individuata una stenosi allorigine del ramo retropielico dellarteria renale , in quanto stata sospettata lorigine artefattuale della diminuzione dellintensit di segnale evidente a tale livello . 
bisogna sottolineare , comunque , che tutti questi errori riguardavano il mancato riconoscimento di stenosi distali ; questo dato non sorprende in quanto in letteratura molti autori [ 21 , 42 , 4851 ] hanno sottolineato come langio - rm abbia una capacit limitata nel visualizzare le stenosi distali a causa della risoluzione spaziale non ottimale . 
anche la visualizzazione delle arterie renali accessorie risente di questa limitazione della tecnica , in quanto il calibro ridotto che spesso questi vasi hanno non ne permette sempre una adeguata visualizzazione . 
in fact , although ce - mra is not so heavily affected by flow artefacts , as are non - contrast - enhanced techniques ( time of flight and phase contrast ) , it is not , however , totally free of thefor this reason , signal loss due to turbulent flow at the stenosis and downstream from it may be confused with a higher grade of stenosis [ 22 , 30 , 52 ]  . the level of diagnostic confidence recorded by the two readers in evaluating the images may have influenced sensitivity and specificity values . 
in recent years , some authors [ 26 , 59 ] noted that dsa may be an imperfect reference standard and proposed replacing it with the degree of arterial revascularisation after angioplasty . thus , the fact of using a test that is sometimes unreliable as a gold standard may in part account for our results with mra . 
the lower sensitivity of our study in comparison with previous reports may also be justified by this aspect . we believe that no single explanation exists for the low sensitivity and specificity recorded in our study ; additionally , a study conducted in 2004 [ 21 ] on a much larger patient population reported sensitivity and specificity values comparable with ours , invoking similar reasons to account for the discrepancy in results in comparison with most other reports in the literature . moreover , from a clinical point of view , it is important to know both the ppv and npv , as these two statistical indexes can assist in clinical decision making . 
la bassa risoluzione spaziale [ 52 , 53 ] , inoltre , pu giustificare la tendenza alla sovrastima delle stenosi ( 2 stenosi severe date come occluse dal lettore 2 ) e la tendenza a considerare stenotiche ( 2 casi per entrambi i lettori ) o occluse ( 1 caso per il lettore 2 ) arterie in realt normali . 
 nel nostro studio abbiamo avuto 5 casi falsi - positivi per entrambi i lettori nella diagnosi della presenza di stenosi e 10 ( lettore 1 ) e 8 ( lettore 2 ) casi falsi - positivi nella valutazione delle stenosi superiori al 50% . 
infatti langio - rm con contrasto , pur non risentendo tanto come le tecniche non contrastografiche ( tof e pc ) degli artefatti da flusso , non ne completamente indipendente . 
per tale motivo , la mancanza di segnale dovuta al flusso turbolento a livello e a valle della stenosi pu essere confusa con un grado maggiore di stenosi [ 22 , 30 , 52 ]  . 
peraltro escludendo tutti i casi in cui il grado di valutazione non era sicuro , sia per la presenza di stenosi che per le stenosi significative si ottengono dei valori di sensibilit e specificit solo modicamente migliori . bisogna inoltre tener conto che la nostra casistica non numericamente particolarmente consistente e lesiguit del campione pu aver in parte condizionato i risultati . unulteriore argomentazione che la dsa un gold standard imperfetto ; infatti alcuni lavori riportano per la dsa un valore di correlazione interosservatore nella diagnosi delle stenosi significative non ottimale , con un range che va da 0 , 65 a 0 , 68 e un altro studio dimostra che la dsa imprecisa nel grading della stenosi a causa della sua natura bidimensionale [ 21 , 5458 ]  . 
alcuni autori [ 26 , 59 ] negli ultimi anni hanno supposto che la dsa non sia un perfetto test di riferimento , proponendo come gold standard il grado di rivascolarizzazione dellarteria dopo trattamento mediante angioplastica ; il fatto , quindi , di prendere come gold standard un test che talvolta non attendibile , potrebbe in parte spiegare i risultati da noi ottenuti nellangio - rm . infine nel nostro studio le immagini angio - rm sono state valutate da osservatori esterni coinvolti a posteriori nella sola analisi delle immagini . 
questo dato differisce dalla maggior parte degli studi ufficiali in cieco in cui i lettori erano direttamente coinvolti nella gestione del paziente e quindi inevitabilmente a conoscenza di informazioni cliniche rilevanti per una diagnosi pi accurata . 
 riteniamo quindi che i bassi valori di sensibilit e specificit da noi rilevati non trovino una spiegazione univoca ; un lavoro del 2004 [ 21 ] , peraltro , riporta valori di sensibilit e specificit simili ai nostri , determinati su una casistica ben pi ampia , adducendo motivazioni simili alle nostre per spiegare la difformit dei risultati nei confronti della letteratura . va peraltro considerato come dal punto di vista clinico sia importante conoscere il valore predittivo sia positivo che negativo , perch questi due indici statistici sono utili nel pro544 radiol med ( 2008 ) 113 : 529546 mra yielded results comparable with the literature , with a ppv of 86% and npv of 55% in detecting stenoses and a ppv of 60% and npv of 90%91% in identifying significant stenoses . 
this implies that although mra tends to underestimate the number of stenoses , it is nonetheless able to correctly identify patients without significant stenoses and thus spare them further diagnostic and interventional procedures first and foremost dsa . 
da questo punto di vista langiorm presenta nella nostra casistica risultati conformi alla letteratura con un valore predittivo positivo dell86% e un valore predittivo negativo del 55% nella capacit di discriminare la presenza di stenosi e un vpp del 60% e un vpn del 90%91% nella capacit di diagnosticare stenosi significative . 
da ci si deduce che pur essendo langio - rm un esame che tende a sottostimare il numero delle stenosi , in grado tuttavia di individuare correttamente i pazienti non affetti da stenosi significative e quindi permette loro di evitare ulteriori indagini diagnostiche e interventistiche , in primis la dsa . 
da sottolineare che nella nostra casistica il numero maggiore di stenosi non diagnosticate erano stenosi lievi e quindi non rilevanti dal punto di vista clinico . conclusions conclusioni our results suggest that , despite the less - than - optimal sensitivity and specificity values that were , in our opinion , mainly due to the characteristics of our study population and the distal location of some significant stenoses , mra remains a useful diagnostic test in evaluating patients with suspected renovascular hypertension . 
it has a high level of accuracy in ruling out significant renal artery stenosis and thus spares the patient additional , more invasive , procedures . i nostri risultati suggeriscono che , nonostante valori non ottimali di sensibilit e specificit , dovuti a nostro giudizio essenzialmente alle caratteristiche della popolazione in esame ed alla sede distale di alcune stenosi significative , langio - rm rimane comunque un test diagnostico utile nella valutazione dei pazienti con sospetta ipertensione su base nefrovascolare in quanto lelevata capacit di escludere con sicurezza la presenza di una stenosi renale significativa permette al paziente di evitare ulteriori indagini pi invasive . 
di radiologia , istituto nazionale di riposo e cura dellanziano ( inrca ) , roma , italy 3istituto di medicina legale , universit degli studi di genova , genova , italy 4servizio di radiologia , azienda ospedaliera g . 
through analysis of several cases derived from legal or insurance proceedings brought against radiologists , the most common forms of error are described , and their implications for criminal and civil liability are illustrated , although it is emphasised that the existence of an error does not always translate into the presence of malpractice . keywords radiology error criminal liability civil liability malpractice lawsuit riassunto la valutazione della rilevanza medico - legale dellerrore in radiologia e , quindi , della responsabilit penale e civile nellesercizio della professione impone lanalisi di come radicalmente sia modificata nellopinione pubblica la percezione del diritto alla tutela della salute e , da questo , siano nate una medicina e , quindi , anche una radiologia sempre pi facilmente orientate a principi cautelativi o difensivi , con proliferare di accertamenti e procedure spesso inutili . 
tramite casi esemplificativi tratti da procedimenti giudiziari o assicurativi ormai risolti contro radiologi , larticolo descrive le pi comuni forme di errore e ne illustra le ricadute in sede penale e civile , evidenziando comunque che lerrore non sempre configura lesistenza di una responsabilit ovvero di una colpa , in particolare in ambito penalistico . parole chiave radiologia errore responsabilit penale responsabilit civile procedimenti giudiziari introduction introduzione the medicolegal relevance of error has recently been emphasised by the media , which riding the usually shortla rilevanza medico - legale dellerrore stata negli ultimi anni senzaltro accentuata dallinfluenza dei media che , 600 radiol med ( 2008 ) 113 : 599608 lived emotional wave of the countless real or supposedly real episodes of medical malpractice report alarming figures based on statistics considered to be reliable . 
on the basis of these figures , it is estimated that 4% of patients admitted to hospital each year in italy are victims of injury caused by avoidable infections , diagnostic errors or treatment errors . the consequences are an estimated 2.5 billion euro in additional costs to the health care system and some 15 , 000 cases of malpractice lawsuits filed by patients [ 1 ]  . 
contributing to the growth of medical litigation is a changed perception by the general public of the right to health care , with heightened expectations regarding what medicine can achieve . 
patients are reluctant to accept their disease and / or disability as a biological event , whereas at the same time , there is the growing conviction of the omnipotence of medicine , which is often fuelled by the scientific community and physicians themselves , who emphasise achievements while glossing over the risks and side effects of the procedures used . 
this leads to deteriorating doctorpatient relationships , which in the event of real or alleged treatment failure contributes to set off litigation mechanisms ( which in as many as 2 / 3 of cases are unfounded ) that are supported by a new understanding of clinical risk and professional liability [ 2 ]  . as in other branches of medicine ( which is not , it should be emphasised , an exact science ) , in radiology , errors inevitably occur , generally due to omission in diagnostic radiology ( a false negative leads to delayed treatment and thus harm to the patient ) and to commission in interventional radiology , in a fashion similar to surgery . 
through the examination of a series of cases derived from legal proceedings or insurance claims , we describe the types and characteristics of radiological error and illustrate the criminal and civil implications . error type and characteristics in diagnostic activity , errors occur as a consequence of inappropriate organisation or management processes ( latent error ) or in the perception or interpretation of diagnostic images ( human error ) [ 3 ]  . 
both types of error can result in litigation on the basis of apparently obvious considerations : a cavalcando londa emotiva quasi mai durevole degli ennesimi , reali o supposti tali , episodi di mala sanit , divulgano dati allarmanti basati su statistiche ritenute attendibili : sulla base di tali dati si stima che il 4% dei pazienti ricoverati ogni anno in italia sia vittima di danni conseguenti ad infezioni , errori diagnostici o terapeutici che potrebbero essere evitati ; il costo aggiuntivo conseguente valutato in circa 2 , 5 miliardi di euro ; si calcola , inoltre , che vi siano 15000 ricorsi giudiziari promossi dai pazienti [ 1 ]  . 
un contributo allesacerbazione del contenzioso medico - legale dato altres dalla modificata percezione del concetto di diritto alla tutela della salute , con crescenti aspettative sui risultati della medicina : sempre pi i pazienti sono portati alla non accettazione della malattia e / o dellinvalidit come evento propriamente biologico mentre di pari passo cresce la convinzione della medicina onnipotente , spesso grazie anche al contributo delle societ scientifiche e dei medici stessi i quali enfatizzano i risultati raggiunti , sottacendo i rischi e gli effetti collaterali delle procedure adottate . 
in tale nuovo scenario si aggiunge una medicina sempre pi facilmente orientata a principi cautelativi o difensivi pi che di bioetica ; da ci discende un rapporto medicopaziente freddo che contribuisce , in caso di vero o presunto insuccesso , allinsorgenza di meccanismi di rivalsa e a rivendicazioni , addirittura nel 2 / 3 dei casi non fondate ma che trovano sponda in un mutato modo di intendere o accettare lalea terapeutica ed il concetto di colpa professionale [ 2 ]  . in radiologia , come in altre discipline della medicina ( che , giova sempre ricordarlo , non una scienza esatta ) si commettono inevitabilmente errori , che generalmente sono di tipo omissivo nellattivit diagnostica ( il falso negativo causa un ritardo da cui deriva un danno per il paziente ) e di tipo commissivo nellattivit interventistica , analogamente a quanto avviene in chirurgia . 
larticolo descrive tramite casi esemplificativi tratti da procedimenti giudiziari o assicurativi le tipologie e le caratteristiche dellerrore in radiologia e le sue conseguenze penali e civili . tipologie e caratteristiche dellerrore : casistica nellattivit diagnostica gli errori si verificano quale conseguenza di un sistema organizzativo non idoneo ( errore latente ) o nella percezione o interpretazione del documento iconografico ( errore umano ) [ 3 ]  . 
1a , b preoperative chest radiograin the upper lobe of the right lung ( a ) , there is evidence of a small pulmonary nodule that was missed by the radiologist . 
il paziente , costretto in sedia a rotelle , denuncia il radiologo e , in sede civile , risarcito con 900000 milioni di lire ( 465000 )  . lesion that the specialist should have identified or that even a layperson can see was missed ; a sign was misinterpreted that would have led to a different diagnosis . 
this kind of simplification is fed by hindsight , a ubiquitous phenomenon based on the belief that past events were predictable , and were often the inevitable consequence of preexisting conditions . 
the radiologist reports mediastinal haemorrhage but does not think it necessary to complete the study with contrast media ; 48 h after the ct scan and after surgery for femoral fracture , the patient suddenly dies . 
indeed , it has been known for some time that individuals with knowledge of the outcome tend to give a higher estimate of the predictability of that event than they would have given they not had advance knowledge [ 4 , 5 ]  . 
in the study , participants with prior knowledge of the diagnosis felt that a certain diagnosis was more likely than did those in the control group , who were presented with a list of symptoms compatible with the disease in question but also compatible with other possibilio che addirittura un profano era in grado di vedere ; stato interpretato scorrettamente un segno che doveva orientare in modo diverso . 
tale semplificazione alimentata inevitabilmente dal senno di poi ovvero dal quel fenomeno particolarmente pervasivo nella vita quotidiana basato sul pensiero che un certo evento non avrebbe potuto non verificarsi : spesso i fatti accaduti sono descritti come conseguenze ritenute per lo pi inevitabili di condizioni che erano presenti gi allinizio . 
poich tali valutazioni si riferiscono abitualmente ad eventi incerti e dato che ex ante per questi possibile soltanto stimare la probabilit con cui potranno verificarsi , ne consegue che la valutazione generalmente espressa , dopo che il fatto si verificato , riradiol med ( 2008 ) 113 : 599608 sulta sistematicamente distorta . 
stato gi da tempo , infatti , accertato come individui , informati che un fatto si verificato , assegnino ad esso una stima di probabilit maggiore di quella prevista in assenza della suddetta informazione [ 4 , 5 ]  . 
in particolare , in ambito medico una ricerca ormai ritenuta classica pone in evidenza come anche medici esperti possano essere esposti allinfluenza del senno di poi : molti partecipanti allesperimento ritennero pi probabile una certa diagnosi sapendo , prima della valutazione acritica dei sintomi , che si trattava della descrizione di quella malattia rispetto ad un gruppo di controllo cui fu presentata una lista di sintomi compatibili con la patologia in oggetto ma anche con altre [ 6 ]  . 
 il senno di poi stato segnalato anche nella pratica radiologica clinica osservandone le conseguenze [ 7 , 8 ]  . linteresse relativo risulta evidente poich questa distorsione cognitiva pu avere conseguenze assolutamente gravi in sede di valutazione di responsabilit per ci che non si fatto o non si potuto fare e per ci che si fatto alla luce di ci che effettivamente accaduto . 
la ricerca delle tipologie e delle caratteristiche dellerrore pu svolgere questo importante compito , iniziando dallanalisi delle quote di ineluttabilit dellerrore stesso , come dimostrato dalla variabilit delle osservazioni intrae inter - osservatore . 
 la valutazione degli aspetti propri dellatto medico - radiologico pone in evidenza il significato rilevante di altre condizioni che hanno uninfluenza determinante sugli errori radiologici quali lanamnesi , lurgenza e lemergenza , le fig . 
5 a patient with a prosthetic aortic valve is admitted to the emergency room for sudden acute chest pacardiac computed tomography ( ct ) is requested for suspected acute coronary syndrome . 
he fails to remark on the ct findings indicated by the arrowheads , which he interprets as a result of the previous surgical intervention instead of intimal flaps in type a aortic dissection , as confirmed by subsequent transoesophageal ultrasonography . 
nel sospetto di sindrome coronarica acuta richiesto uno studio tc urgente delle coronarie che sono descritte come normali ; interpretandoli come esiti del precedente intervento chirurgico , il radiologo non segnala neppure i reperti evidenziati dalle punte di freccia e che sono piuttosto da riferire a flap dellintima in dissezione tipo a dellaorta ascendente ; successiva conferma mediante ecografia transesofagea . 
this phenomenon , therefore , reflects a sort of determinism with respect to the past and is the unconscious and misleading result of a retrospective evaluation of events . hindsight bias has also been reported in clinical radiological practice [ 7 , 8 ]  . 
the relevance is obvious , as this kind of cognitive bias can have serious effects on the assessment of liability for what was done or not done in the light of the eventual outcome . 
in realt , anche nei casi in cui le attribuzioni siano previste da una norma , le ipotesi di responsabilit professionale non sono chiaramente definibili anche in funzione del bene tutelato , la salute del paziente . 
 evidente che lattivit medico - legale per laccertamento delle responsabilit muove dal presupposto che le indagini radiologiche non possono non essere considerate come parti integranti della cartella clinica e / o della documentazione sanitaria . 
e come tali , divengono spesso elemento di tutela , oltre che di garanzia , sia per la salute del paziente sia per la difesa della dignit e onorabilit del rafig . 
the patient is taken to the thoracic surgery operating theatre , where surgery with access at the level of the iv left intercostal space is performed and multiple fractures of the ribs are reported ; conspicuous bleeding from intercostal arteries and bleeding pulmonary parenchymal lacerations are identified . 
trasferimento nella sala operatoria della chirurgia toracica : intervento con accesso a livello del iv spazio intercostale sinistro e reperto di multiple fratture costali con cospicuo sanguinamento da vasi intercostali e lacerazioni parenchimali polmonari . 
 analysis of the various aspects of radiological practice highlights the significance of other factors that heavily affect radiological error , such as patient history , urgency and emergency , sensitivity of screening examinations , clinical tradeoff between false positives and false negatives , available technology , setting , work hours and time dedicated to reporting . medicolegal implications of error in radiological examinations it is often believed that specific existing norms can help settle issues of professional liability . 
in practice , even where regulations do exist that outline the radiologists competences , professional liability cannot be easily established , in part because of the nature of the right being protected that is , the health of the patient . 
however , it is also known that it is easier to judge a radiologists performance than to judge that of any other physician , precisely because consultants or expert witnesses can verify the professional conduct of radiologists a posteridiologo . 
daltra parte , altrettanto noto come sia pi facile giudicare loperato di un radiologo che non di un qualsiasi altro medico grazie proprio alla possibilit di verificare latto professionale del primo tramite il referto radiologico , alla luce della documentazione iconografica ( comunemente denominata reperto ) ovvero di quelle immagini certe che possono essere ben esaminate a posteriori da parte di consulenti o periti . lattivit del radiologo , come quella di chiunque , esposta ad una possibile valutazione penale e / o civile , in tema di responsabilit professionale , per eventuali conseguenze di danno derivanti da comportamenti incongrui ovvero da un errore nella risposta al quesito diagnostico oltre che , in taluni casi , per il mancato riconoscimento di quadri rilevabili anche extra quesito diagnostico . 
pur essendo molto diversi i presupposti per il riconoscimento della responsabilit penale rispetto a quella civile , dal punto di vista medico - legale vi in ogni caso la necessit di definire la prevedibilit , levitabilit , la rilevabilit e leventuale emendabilit del comportamento errato . 
 la valutazione della colpa in radiologia non presenta , sul piano giuridico , aspetti diversi e peculiari rispetto ai criteri ordinari che la giurisprudenza applica allattivit 606 radiol med ( 2008 ) 113 : 599608 ori , by reviewing the radiological report and relevant imaging findings . the radiologists activity , like that of any other person , is subject to possible criminal and / or civil evaluation to establish professional liability in the event of harm deriving from inappropriate conduct , an error in responding to a diagnostic query or failure to detect pathological signs not related to the diagnostic query . 
the criminal and civil aspect of technical - professional liability , therefore , presumes the real or alleged occurrence of personal harm . although criminal and civil liability are established on the basis of very different criteria , from the medicolegal point of view , there is in either case a need to establish foreseeability , avoidability , certainty and the possible ability to rectify the misconduct . determination of fault in radiology is characterised by the same criteria that the law applies to all medical activity . these criteria are imprudence , negligence and inexperience , as well as failure to abide by possible precautionary regulations . 
a judgement of liability naturally contemplates even slight fault but becomes more benevolent and understanding in the context of inexperience , as long as this case is characterised by a special difficulty . 
it should also be borne in mind that , beyond incorrect medicolegal methodological practices , judgment of liability must take place from an ex ante perspective , with reference to the situation present and known at the time of the alleged misconduct . in criminal proceedings , medicolegal evaluation of liability in the case of harm ( slight , severe or very severe ) or of manslaughter is based on assessment of supposedly incorrect technical - professional conduct and causation . 
it is precisely the meaning attributed to the error of conduct ( and to its consequences ) that renders the sense of professional liability of the physician in italy completely different from that in other countries , such as the united states [ 13 ]  . 
indeed , in italy , error alone is not enough to substantiate a hypothesis of a criminal offence , and to be precise , not even the occurrence of a harmful event is sufficient . 
an indispensable feature is the relationship ( chronological , topographical , commensurate harm , phenomenological continuity , exclusion ) between the error ( or misconduct ) and the harm , which must be directly caused by the medical act with an uninterrupted causal link and not from contingencies rootmedica . 
la colpa accertata secondo un giudizio che d naturalmente rilievo anche alla forma lieve ma che diventa maggiormente benevolo e comprensivo in materia di imperizia , purch in questa evenienza sia insita una speciale difficolt . 
bisogna , inoltre , ricordare che , al di l di erronee prassi metodologiche medico - legali , il cosiddetto vaglio di colpa deve svolgersi secondo giudizio ex ante , con riferimento alla situazione presente e nota al momento della condotta incriminata . 
 in ambito penalistico laccertamento medico - legale nel caso di lesione ( lieve , grave o gravissima ) o di omicidio colposo si basa sulla valutazione della condotta tecnicoprofessionale supposta erronea e sulla ricostruzione del nesso di causalit . 
proprio il significato attribuito al cosiddetto errore di condotta ( ed alle sue conseguenze ) che rende completamente differente il senso di responsabilit professionale del medico in italia rispetto ad altre realt come , ad esempio , quella statunitense [ 13 ]  . 
nel nostro paese , infatti , non basta lerrore a definire il riconoscimento di unipotesi di delitto e , per la precisione , potrebbe non essere sufficiente neppure il verificarsi dellevento dannoso . 
risulta indispensabile la definizione di un rapporto ( cronologico , topografico , di adeguatezza lesiva , continuit fenomenologica , esclusione ) tra lerrore ( o il comportamento non adeguato ) e il danno che deve discendere , con ininterrotto legame causale , dallatto medico e non da contingenze connaturate al mero andamento patologico n da cause sopravvenute assolutamente estranee . 
occorre acquisire la prova di tale nesso in termini di certezza processuale , ossia oltre ogni ragionevole dubbio ; cio necessario dimostrare ( come attesta la suprema corte di cassazione , sezioni unite penali , 10 luglio 2002 , n 27 ) con elevato grado di probabilit prossimo alla certezza che levento dannoso non si sarebbe verificato ovvero si sarebbe verificato ma in epoca significativamente posteriore o con miradiol med ( 2008 ) 113 : 599608 ed in the disease itself or intervening extraneous causes . proof needs to be acquired of such a link in terms of legal certainty , i.e. 
of demonstrating that no error was committed or that the harm was not the result of his or her actions , lies with the physician and , in our case , the radiologist , who acts on behalf of the public health care system that takes on contractual liability in regard to its clients . 
assessment of professional liability , which usually follows termination of the criminal phase , places medical misconduct in the context of the obligation to award damages when a patient unjustly suffers injury due to an illicit action ( inexperience , imprudence , negligence ) or a harmful event derived from breach of contract due to failed or inadequate commitment of the physician with respect to his or her obligation to perform well . 
8826 of 13 april 2007 . the proliferation of civil liability cases brought against physicians and radiologists , which imply ( when established ) the awarding of damages to the patient , results in a need for broad insurance coverage , even though this is not compulsory . nor intensit lesiva se il medico avesse agito diversamente . 
 in ambito civilistico , al medico pubblico dipendente , e nella fattispecie al radiologo , agendo egli per conto dellazienda sanitaria che assume una responsabilit contrattuale nei confronti degli assistiti , imposto lonere della prova cio la dimostrazione di non aver sbagliato ovvero che il danno non deriva da suo operato . 
la valutazione della responsabilit professionale , che abitualmente subentra una volta esaurita la fase penale , riconduce la cattiva condotta del medico nel quadro dellobbligo del risarcimento che interviene quando si realizzi nel paziente un danno ingiusto prodotto da fatto illecito ( imperizia , imprudenza , negligenza ) oppure un evento dannoso derivante da violazione del contratto per mancato o difettoso impegno del medico nei confronti della sua obbligazione di ben operare . 
nel primo caso violata una responsabilit extracontrattuale , nel secondo caso una responsabilit contrattuale ; le due possono essere invocate separatamente ovvero in concorso , in dipendenza delle variabili caratteristiche del rapporto . 
 importante ricordare che la prestazione medica e , quindi , anche radiologica non comporta unobbligazione di risultato ma semplicemente di comportamenti e mezzi anche se il risultato positivo una conseguenza statisticamente fisiologica della prestazione professionale diligente , come attesta la sentenza 13 aprile 2007 , n . 
il proliferare delle cause legali , che implicano il risarcimento del danno patito dal paziente ( qualora la responsabilit civile del medico e del radiologo sia accertata ) , costringe ad unampia copertura assicurativa , anche se non obbligatoria . conclusioni conclusions the radiologist must be aware that sensory , cognitive , processing and decision - making errors generate false negatives and false positives and can translate into real or presumed harm for the patient , with related legal consequences . 
it is , nonetheless , certain that a critil radiologo deve prender atto che errori sensoriali , mentali , elaborativi e decisionali , generando falsi negativi e positivi , possono tradursi in un danno reale o presunto per il paziente , con relative conseguenze medico - legali . 
cirillo unit operativa complessa di diagnostica per immagini , presidio ospedaliero dei pellegrini ; asl napoli 1 , via portamedina alla pignasecca 41 , 80134 napoli , italy correspondence to : l.c. 
cirillo , via manzoni 19 , 80123 napoli , italy , tel . : + 39 - 081 - 2543323 , fax : + 39 - 081 - 2543307 , e - mail : lc.cirillo@libero.it received : 7 march 2007 / accepted : 24 august 2007 / published online : 20 may 2008 springer - verlag 2008 abstract purpose . 
ct therefore provides an important contribution to preoperative selection of patients , assisting in directing those with < 20% bone loss towards arthroscopic capsular repair . keywords glenohumeral instability glenohumeral ct bony bankart riassunto obiettivo . 
la valutazione quantitativa ha permesso di calcolare con esattezza il deficit osseo del bordo glenoideo antero - inferiore in termini di area ( espressa in mm2 ) o di percentuale di superficie . 
la metodica da noi utilizzata rende possibile quantificare con estrema precisione il deficit osseo , con una tecnica semplice , rapida e facilmente riproducibile , fornendo cos un contributo fondamentale nella selezione pre - operatoria dei pazienti , indirizzando verso lintervento di capsuloplastica artroscopica i pazienti con un difetto osseo inferiore al 20% . parole chiave instabilit gleno - omerale tc glenoomerale lesione di bankart ossea radiol med ( 2008 ) 113 : 496503 introduction introduzione shoulder instability is a subjective and objective condition that manifests as a sensation of joint laxity associated with pa the disorder may result from traumatic injuries or from congenital malformations or abnormal glenoid orientation [ 1 ]  . 
posttraumatic instability is the most common type , frequently occurring among athletes , and presents as anteroinferior instability ( 95% of cases ) or , less commonly as posterior instability [ 2 ]  . 
the complexity of the disorder requires the integration of different imaging modalities [ conventional radiology , conventional arthrography , computed tomography ( ct ) arthrography , magnetic resonance imaging ( mri ) , mr arthrography ] , to better define the anatomicalpathological changes [ 3 , 4 ]  . in recent years , the assessment of skeletal damage has aroused much interest , particularly in bone defects of the anteroinferior glenoid expressed both as acute fractures ( bony bankart lesions ) and as chronic bone deficiency [ 57 ]  . 
it has been shown that the presence of a significant amount of bone loss from the anteroinferior glenoid is a predisposing factor for recurrent instability and a negative prognostic factor for arthroscopic capsular repair [ 813 ]  . this implies a need to identify and quantify glenoid bone loss in the delicate preoperative stage [ 1417 ]  . 
the aim of this study was to evaluate this method not only as an aid to surgical planning but also in the postoperative follow - up . materials and methods between january and november 2006 , 93 patients ( 83 male and ten female subjects ) aged 1670 years ( mean 27 years ) were studied with ct . 
patients were divided into two groups on the basis of clinical findings : group 1 comprised 80 patients on the waiting list for stabilisation surgery , 74 of whom suffered posttraumatic recurrent anteroinferior instability and six chronic multidirectional instability , referred to us for traumatic injuries to lax shoulders . 
 all patients underwent simultaneous assessment of both shoulders from a plane passing 1 cm above the acromioclavicular joint to the inferior aspect of the glenoid cavity with a general electric hi - speed ( two - slice ) ct scanner . the following scanning parameters were used : reconstruction thickness 2 mm with 1 - mm gap , 140 kv , 60 ma , with linstabilit di spalla una condizione soggettiva ed obiettiva che si manifesta con una sensazione di perdita di contatto articolare associata a dolore . 
linstabilit post - traumatica la pi frequente , una patologia molto ricorrente tra gli atleti e si presenta spesso ( 95% dei casi ) come instabilit antero - inferiore , meno frequentemente come instabilit posteriore [ 2 ]  . 
la complessit di questa patologia richiede unintegrazione di diverse metodiche di imaging ( radiologia tradizionale , artrografia tradizionale , artro - tc , rm , artrorm ) , al fine di caratterizzare con maggiore esattezza le alterazioni anatomo - patologiche [ 3 , 4 ]  . negli ultimi anni ha assunto notevole rilevanza la valutazione dei danni scheletrici ed in particolare i difetti ossei della rima glenoidea antero - inferiore , espressi sia come fratture acute ( bony - bankart ) che come deficit ossei cronici [ 57 ]  . 
stato dimostrato che la presenza di una significativa perdita di sostanza ossea a livello della rima glenoidea antero - inferiore rappresenta una condizione predisponente allinsorgenza di un quadro di instabilit ricorrente , ed un fattore prognostico negativo ai fini di una capsuloplastica artroscopica [ 813 ]  . 
nata pertanto la necessit non solo di individuare , ma anche e soprattutto di quantificare il deficit osseo glenoideo nella delicata fase preoperatoria [ 1417 ]  . di recente , stato elaborato un metodo di misurazione mediante tc [ 18 ] in grado di quantificare il deficit osseo glenoideo in termini di area ( espressa in mm2 ) o di percentuale di superficie . 
lobiettivo del nostro studio di esporre la validit di tale metodo , non solo nella pianificazione pre - operatoria , ma anche nei controlli post - intervento . materiali e metodi da gennaio a novembre 2006 , sono stati sottoposti ad esame tc spirale 93 pazienti ( 83 uomini e 10 donne ) di et compresa tra i 16 e 70 anni ( et media 27 anni )  . 
i pazienti sono stati suddivisi dal punto di vista clinico - anamnestico in due gruppi : i gruppo : 80 pazienti posti in lista dattesa per intervento di stabilizzazione , di cui 74 per instabilit recidivante post - traumatica antero - inferiore , e 6 per instabilit cronica multidirezionale , giunti alla nostra osservazione per eventi traumatici avvenuti su spalle lasse ; ii gruppo : 13 pazienti con episodi di recidiva di lussazione di spalla dopo intervento di stabilizzazione , di cui 7 operati per via artroscopica e 6 mediante trasposizione coracoidea secondo latarjet - patte . 
 in tutti pazienti stato eseguito lo studio comparativo del498 radiol med ( 2008 ) 113 : 496503 bone reconstruction algorithm , and subsequent off - centre back reconstruction of the healthy shoulder first and then of the pathological shoulder with a smaller fov ( approximately 15 cm )  . 
starting from the geometric assumption [ 6 , 15 ] that all glenoids can be inscribed in a circle , a circle was drawn based on the inferior part ( 3 oclock to 9 oclock ) of the contour of the healthy glenoid to obtain the normal glenoid area expressed in mm2 to be used as a reference value . 
thus , the percentage of bone loss is provided by the simple equation : normal glenoid area : 100 = pathological glenoid area : x results among the 80 patients in group 1 with recurrent glenohumeral dislocation , we observed a glenoid rim lesion in 64 patients ( 80% ) , 24 ( 30% ) of whom had a bony bankart lesion and 40 ( 50% ) a bone deficiency of the anteroinferior glenoid . 
mpr mediante assi paralleli alla rima glenoidea ( a ) ; immagine frontale della cavit glenoidea ( b )  . le spalle , da un punto passante 1 cm sopra larticolazione acromion - claveare , fino a coprire interamente la cavit glenoidea , mediante tc general electric hi - speed ( double slice )  . 
sono stati utilizzati i seguenti parametri di acquisizione volumetrica : spessore di ricostruzione 2 mm con intervallo di 1 mm , 140 kv , 60 ma , con algoritmi di ricostruzione per osso , e successiva retroricostruzione off center prima della spalla sana e poi della spalla patologica con un fov ridotto rispetto a quello dellacquisizione ( circa 15 cm )  . 
la percentuale del deficit osseo viene ottenuta mediante una semplice equazione : area glenoidea normale : 100 = area glenoidea patologica : x nel primo gruppo di 80 pazienti con lussazione gleno - omerale recidivante , stata osservata una lesione della rima glenoidea in 64 pazienti , di cui 24 presentavano una bonyradiol med ( 2008 ) 113 : 496503 fig . 
area di riferimento della superficie glenoidea della spalla sana ( 580 mm2 ) ( a ) ; area della superficie glenoidea della spalla patologica con valutazione del deficit osseo glenoideo ( 99 mm2 ) ( b )  . tion after stabilisation surgery , we observed no bone defect in six patients , a small ( < 15% ) glenoid bone deficiency in six patients ( 46% ) , and a large ( > 20% ) bone defect in one case only ( 8% )  . 
 discussion the glenohumeral joint is a highly complex anatomical system , the stability of which depends equally on static factors , such as capsular - ligamentous and bony structures , and dynamic factors , such as tendinous - muscular structures . 
even though joint stability is dependent on a combination of interacting factors rather than on a single factor , in recent years , the role of bony alterations has been emphasised , particularly the role of lesions of the glenoid rim , the incidence bankart , e 40 un deficit osseo del bordo glenoideo anteroinferiore . 
 the first to introduce the notion of glenoid rim lesion was bigliani et al . , who in 1998 [ 7 ] classified lesions of the anteroinferior glenoid rim into three types , defining the bone fragment bony bankart : type i : displaced bone fragment with attached rim ( bony type ii : consolidated displaced bony fragment with detype iiia : anterior glenoid erosion < 25% of the total surbankart ) tached rim face radiol med ( 2008 ) 113 : 496503 fig . 
3a - c paziente con grossolana bankart ossea ; area della superficie glenoidea di riferimento 776 mm2 ( a ) ; valutazione del deficit osseo glenoideo ( 201 mm2 pari al 26 % ) ( b ) e della bankart ossea ( 76 mm2 pari al 10% ) ( c )  . to complesso , alla cui stabilit concorrono in maniera sinergica sia fattori statici come le strutture capsulo - legamentose ed ossee , che fattori dinamici come le strutture teno - muscolari , che svolgono invece una funzione attiva . 
sebbene nessun fattore sia singolarmente responsabile della stabilit articolare , ma una combinazione di differenti fattori che interagiscono fra loro , negli ultimi anni stato enfatizzato il ruolo delle alterazioni ossee , ed in particolare le lesioni del bordo glenoideo , la cui incidenza nellinstabilit gleno - omerale ricorrente sembra essere molto elevata ( 90% ) [ 5 , 6 ]  . 
nelle mpr sul piano coronale ( a ) e sagittale ( b , c ) si apprezza la completa lisi dellinnesto osseo con evidenza di un esteso deficit osseo del bordo antero - inferiore della glena pari al 29% . 502 radiol med ( 2008 ) 113 : 496503 type iiib : anterior glenoid erosion > 25% of the total surface . 
 it is commonly believed that the presence of a large avulsed fragment or a bone loss sufficient to give the glenoid the shape of an inverted pear leads to a mechanical inability to contain the humeral head , and these conditions therefore predispose to recurrent dislocations and risk factors for recurrences even after stabilisation surgery [ 8 , 9 ]  . these important clinical and statistical data have originated the need for early detection and precise quantification of glenoid bone defects , as this will influence decisions about whether to treat arthroscopically or with coracoid transfer surgery according to latarjet - patte . 
 although the choice of treatment depends on several variables , according to the majority of authors a glenoid bone defect involving > 18%25% of the total surface seems to contraindicate arthroscopic treatment [ 7 , 1013 ]  . 
among them , sugaya et al . , in 2003 [ 6 ] , succeeded in calculating the percentage of bone defect by using ct with 3d reconstructions and elimination of the humeral head , demonstrating that the inferior half of the glenoid can be approximated to a circle , the diameter of which is a line between 3 oclock and 9 oclock . 
this important intuition is the basic assumption underlying the method used [ 18 ]  . given that in the same individual the surface of the two glenoids is identical , by calculating the circumferential area of the inferior half of the healthy glenoid one can evaluate the shape of the pathological glenoid and measure the bony defect in terms of area ( mm2 ) or percentage of surface , simply by drawing the contour of the fragment of the defective area . 
 from the analysis of the results achieved to date we can state that the method is fast , simple , easy to reproduce and capable of providing precise quantification of the bone defect of the anteroinferior glenoid . 
it could therefore become a necessary step in preoperative planning in patients with anterior glenohumeral instability . sa , inducano unincapacit meccanica al contenimento della testa omerale , e quindi rappresentino una condizione predisponente a lussazioni ricorrenti ed un fattore di rischio per linsorgenza di recidive anche dopo intervento di stabilizzazione [ 8 , 9 ]  . 
sulla base di queste importanti indicazioni clinico - statistiche nata la necessit di individuare precocemente e di quantificare esattamente il deficit osseo glenoideo in quanto influenza la scelta del trattamento , che pu essere di riparazione artroscopica o di trasposizione coracoidea secondo latarjet - patte . 
 sebbene la scelta del trattamento dellinstabilit dipenda da numerose variabili , per la maggior parte degli autori un deficit osseo glenoideo che coinvolga pi del 18%25% della superficie totale sembra controindicare un trattamento artroscopico [ 7 , 1013 ]  . 
alcuni autori , hanno cercato di quantificare il deficit osseo glenoideo , proponendo metodi eterogenei , sia radiologici che artroscopici [ 9 , 10 , 1417 ]  . tra questi sugaya et al . 
nel 2003 [ 6 ] riuscito a calcolare la percentuale del deficit osseo mediante un metodo tc con ricostruzioni 3d e sottrazione della testa omerale , dimostrando come la met inferiore della glena possa essere considerata con buona approssimazione una circonferenza che ha come diametro una linea passante da ore 3 a ore 9 . questa importante intuizione , rappresenta il presupposto fondamentale della metodica utilizzata [ 18 ]  . poich in un stesso individuo la superficie delle due glene identica , calcolando prima larea circonferenziale della met inferiore della glena sana , possibile valutare la morfologia della glena patologica e calcolare il deficit osseo in termini di area ( espressa in mm2 ) o in percentuale di superficie , semplicemente disegnando il contorno del frammento o larea deficitaria . 
40773 - 1 published online : 20 june 2008 springer - verlag 2008 this book adds to those dedicated to paediatric radiology in the medical radiology / diagnostic imaging series directed by professors baert , knauth and sartor . 
authors represent a team of wellestablished , experienced and well - known paediatric radiologists from large paediatric radiology departments in hospitals in europe and the united states . the aim of the book is not only to review the old imaging techniques , which are the daily diagnostic bread in this field , but also to document , present and discuss the increasing and important role of other cross modalities , such as ultrasound , computed tomography ( ct ) and magnetic resonance imaging ( mri ) ( increasingly important in this field )  . all authors have clearly discussed their topics with appropriate reference to recent literature , adding as much as possible their how i do it approaches to diagnostic problems , stressing , among the others points , what kind of contrast medium is to be used according to the problem to be solved . 
important is the discussion , in the chapter on gastrointestinal interventions , addressing how to prepare the child who is to undergo it , in regard , as well , to sedation and anaesthesia . 
the same refers to intussusception diagnosis and reduction techniques dealt , with at large , in all their different modalities , in two different separate chapters . due to the fact that subject matter starts from the oesophil volume in questione si aggiunge a quelli dedicati alla radiologia pediatrica nella collana medical radiology / diagnostic imaging diretta dai professori baert , knauth and sartor . 
lelenco degli autori rappresenta un gruppo di radiologi pediatri esperti , ben conosciuti nel loro campo e di riconosciuta fama provenienti da importanti reparti di radiologia pediatrica in europa e negli stati uniti . scopo principale del volume era di rivedere non solo vecchie e note immagini e tecniche che sono alla base dellattivit giornaliera dei reparti di radiologia pediatrica , ma anche di documentare , presentare , discutere e far conoscere il sempre pi importante ruolo di altre modalit di studio quali gli ultrasuoni , la tc e la rm ( questultima con ruolo sempre pi importante in questo campo )  . tutti gli autori hanno discusso la parte loro assegnata con chiarezza e con riferimenti bibliografici quanto pi possibile aggiornati , soprattutto cercando di mettere in luce il proprio metodo di approccio ( how i do it ) ai problemi diagnostici , discutendo in particolar modo il tipo di mezzo di contrasto da impiegare a seconda dei problemi da affrontare . 
lo stesso discorso valido riguardo alle metodiche di diagnosi e terapia dellinvaginazione intestinale , trattati ampiamente in due differenti capitoli . 609 - 610 recensione1 1 - 09 - 2008 10 : 03 pagina 610 radiol med ( 2008 ) 113 : 609610 agus and continues all the way to the rectum , including the accessory organs of digestion , the reader will find some overlap between chapters ( appendicitis , intussusception , necrotizing enterocolitis , for example )  . 
in my opinion , this is not a drawback ; on the contrary , it is a bonus , giving the reader the opportunity to understand how the same problem can be dealt with in different hospital situations . the images contained in this book are of the highest quality , some of them in colour ( impressive are the intraoperative and clinical images to be found and enriching the first chapter about gastrointestinal emergencies )  . 
blickman and devos refer to complications in preparation of the volume , due to some authors dropping out due to illness or because of changes in employment situation precluding them from contributing . 
going through the book , however , these complications are not evident , and the endresult is more than rewarding and satisfactory . this book , which is easy to read , will be much appreciated by radiologists ( both paediatric radiologists and those dealing with adults ) , paediatricians and paediatric surgeons and adds substance to the existing knowledge of the subject matter . 
i am sure this book will be much appreciated by trainees in radiology , for whom it is warmly recommended . malposizione delle figure nel 2 capitolo e meno nel 1 . nella loro prefazione i curatori del volume , i professori blickman e devos fanno riferimento a complicanze insorte nella preparazione del volume , dovute a rinunce a causa di malattia o dovute a cambiamenti nelle condizioni di impiego che hanno impedito ai possibili autori di farlo . leggendo il volume , per , non si ha segno di queste complicanze ed il risultato finale pu essere considerato pi che soddisfacente . questo volume sar sicuramente apprezzato dai radiologi ( siano essi pediatrici o delladulto ) , dagli specializzandi in radiologia cui lo raccomando vivamente , dai pediatri e dai chirurghi pediatrici , fornendo materia alla conoscenza dellargomento , soprattutto per la utile ricaduta nei confronti dai bambini che soprattutto beneficeranno dallo stesso . 
one hundred and twenty children ( 68 boys and 52 girls aged between 1 month and two years ) with a clinical suspicion of gastro - oesophageal reflux ( postprandial vomiting , weight loss , failure to thrive , anaemia , night - time coughing and crying , regurgitation , etc . ) were studied by contrast - enhanced cdus and subsequently by 24 - hour ph - metry . 
in consideration of the results obtained and particularly of the low level of invasiveness , contrastenhanced cdus could be used to monitor children undergoing medical or surgical treatment for the complications of gastro - oesophageal reflux disease . keywords colour doppler us gasro - oesophageal reflux ph - metry contrast media riassunto obiettivo . 
centoventi bambini , 68 maschi e 52 femmine , con et compresa tra 1 mese e 2 anni , con sospetto di reflusso gastro - esofageo allesame clinico ( vomito post - prandiale , perdita di peso , ritardo di crescita , anemia , tosse e pianto notturno , rigurgiti , ecc . ) , sono stati sottoposti ad esame con eco - color doppler con mdc e successivamente con ph - metria nelle 24 ore . 
il color doppler ha evidenziato in tutti i casi di reflusso il passaggio del mdc dallo stomaco nel tratto addominale e nel terzo medio e distale del tratto toracico dellesofago permettendo la valutazione della porzione di esofago interessata dal reflusso . 
in base ai risultati ottenuti e soprattutto in virt della scarsa invasivit , la suddetta metodica ecografica potrebbe essere utilizzata nel monitoraggio dei bambini con malattia da reflusso gastro - esofageo sottoposti a terapia medica o chirurgica delle complicanze del reflusso gastro - esofageo . parole chiave color doppler ecografia reflusso gastro - esofageo ph - metria mezzo di contrasto 592 introduction gastro - oesophageal reflux disease ( gord ) [ 1 , 2 ] refers to the involuntary return of gastric contents into the oesophagus . 
gord should be promptly diagnosed to prevent complications such as peptic oesophagitis , ulcers and strictures [ 3 ] , above all in symptomatic children , in whom the incidence of such complications is higher . commonly used techniques for diagnosing and classifying gord are 24 - hour ph - metry [ 46 ] , oesophageal manometry [ 7 , 8 ] , endoscopy [ 9 ] , barium swallow [ 1012 ] , scintigraphy [ 1315 ] and gastroscopy [ 16 ]  . 
the use of noninvasive techniques is especially desirable in newborns and infants , lending support to methods such as ultrasound ( us ) [ 1721 ] , colour - doppler us ( cdus ) [ 22 , 23 ] and pulseddoppler us [ 24 ] for the diagnosis and follow - up of gord . ph - metry , considered the reference standard , is invasive , not always available in paediatric units , and often requires hospitalisation with resulting higher health care costs . 
sonographic contrast material has recently been successfully employed in endocavitary imaging , for example , for studying vesicoureteral reflux , where it yielded results almost identical to voiding cystourethrography but with the advantage of sparing the patient exposure to ionising radiation [ 25 ]  . 
 the aim of this study was to evaluate the diagnostic accuracy and sensitivity of contrast - enhanced cdus in detecting gord and to identify sonographic patterns on which to base a sonographic classification of the disease . 
in the study , we employed cdus with sonographic contrast material , shu 508 a ( levovist , schering ) a suspension of galactose , air microbubbles and palmitic acid [ 26 ] for diagnosing gord in symptomatic children < 2 years of age , and we compared the results with those of 24 - hour phmetry . materials and methods over the past six years , 120 infants ( 68 boys and 52 girls ; age range 1 month to 2 years ; mean age 12 months ) presenting with postprandial vomiting ( 32 ; 26.6% ) , weight loss and failure to thrive ( 30 ; 25% ) , anaemia , night - time coughing and crying , regurgitation , melaena , pneumonia , cyanosis , asthma , night - time awakening and head rotation ( 58 ; 48.3% ) ( table 1 ) were studied by contrast - enhanced colourdoppler us followed by 24 - h ph - metry . 
the examinations were performed after obtaining the parents informed consent . twenty - four - hour ph - metry was conducted the day after the sonographic study to improve patient compliance , and radiol med ( 2008 ) 113 : 591598 introduzione il reflusso gastro - esofageo ( ger ) [ 1 , 2 ] consiste nellinvolontario passaggio di contenuto gastrico nellesofago . 
il ger deve essere diagnosticato precocemente per prevenire in tempo complicanze quali lesofagite peptica , ulcere , stenosi [ 3 ] sopratutto nel bambino sintomatologico dove lincidenza pi elevata . gli strumenti generalmente usati per la diagnosi e la classificazione del ger sono : la ph - metria nelle 24 ore [ 46 ] , la manometria esofagea [ 7 , 8 ] , lendoscopia [ 9 ] , il pasto baritato [ 1012 ] , la scintigrafia [ 1315 ] e la gastroscopia [ 16 ]  . 
luso di tecniche non invasive molto importante specie nei neonati e nei lattanti ; ci favorisce dunque lutilizzo di metodiche quali lecografia [ 1721 ] , il color doppler [ 22 , 23 ] e il doppler pulsato [ 24 ] , nella diagnosi e nel follow - up del ger . 
recentemente il mdc ecografico gi stato utilizzato con successo per via endocavitaria come ad esempio nellapparato urinario per lo studio del reflusso vescico - ureterale ; ottenendo risultati pressoch sovrapponibili a quelli della cistografia , con il vantaggio dellassenza dellimpiego di metodiche con radiazioni ionizzanti [ 25 ]  . 
 lobiettivo di questo lavoro la valutazione dellaccuratezza diagnostica e della sensibilit del color doppler con mdc nella diagnosi del ger nonch lindividuazione di reperti ecografici finalizzata allindividuazione di uneventuale classificazione ecografica del ger . 
patients ( % ) sintomi numero pazienti ( % ) postprandial vomiting weight loss and failure to thrive anaemia regurgitation and belching crying refusal to eat hiccups melaena asthma , pneumonia , cyanosis , nocturnal coughing nocturnal awakening head rotation 32 ( 26.6 ) 30 ( 25 ) 8 ( 6.6 ) 2 ( 1.6 ) 4 ( 3.3 ) 6 ( 5 ) 2 ( 1.6 ) 1 ( 0.8 ) 24 ( 20 ) 7 ( 5.8 ) 4 ( 3.3 ) vomito post - prandiale perdita di peso e ritardo di crescita anemia rigurgiti ed eruttazioni pianto rifiuto di alimentarsi singhiozzo melena asma , polmoniti , cianosi , tosse notturna risvegli notturni rotazione del capo 32 ( 26 , 6 ) 30 ( 25 ) 8 ( 6 , 6 ) 2 ( 1 , 6 ) 4 ( 3 , 3 ) 6 ( 5 ) 2 ( 1 , 6 ) 1 ( 0 , 8 ) 24 ( 20 ) 7 ( 5 , 8 ) 4 ( 3 , 3 ) the two tests were conducted in a double - blind fashion . cdus was performed with a au - 5 idea unit ( esaote biomedica , genoa , italy ) and a 3.5 mhz probe , using a pulse repetition frequency ( prf ) of 6 khz . 
after a 4 - h fast , all patients were administered 7.5 ml of contrast suspension ( 400 mg / ml ) ( maximum osmolarity at 37c = 2 , 894 mmol / kg ) mixed with milk to reproduce a normal feed ( 15 ml / kg )  . 
at the end of the feed , patients were given a small amount of milk without contrast ( 10 ml ) to cleanse the oesophagus from residual contrast material and avoid false positive results . 
the anatomical landmarks used to identify the oesophageal segments were the portion located between the abdominal aorta and left liver lobe for the cardia and abdominal oesophagus on the transverse subxiphoid scans ; the portion between the left liver lobe , the abdominal aorta and the heart for the thoracic oesophagus on longitudinal subxiphoid scans . 
the electrodes were secured to the nose to reduce motion artefacts to the minimuat the end of the recording , the electrodes were removed and the output data analysed by appropriate software . 
the catheters were inserted through the nose and positioned under the guidance of an image intensifier : the compilazione del consenso informato da parte dei genitori , i pazienti sono stati sottoposti allo studio ecografico e successivamente allo studio ph - metrico . 
 lecografo utilizzato era lau - 5 idea ( esaote biomedica , genova , italia ) equipaggiato con sonda da 3 , 5 mhz , utilizzando una ripetizione degli impulsi ( prf ) di 6 khz . 
a tutti i pazienti , a digiuno da quattro ore , sono stati somministrati 7 , 5 ml di sospensione ( 400 mg / ml ) ( max osmolarit a 37c = 2894 mmol / kg ) di mezzo di contrasto integrati al latte in modo da riprodurre il normale pasto ( 15 ml / kg )  . 
alla fine della somministrazione del pasto stata somministrata una piccola quantit di latte senza mdc ( 10 ml ) per lavare lesofago dai residui di mdc per evitare falsi positivi . 
sono state eseguite con pazienti in decubito supino scansioni trasverse e longitudinali sotto - xifoidee per evidenziare il mdc nello stomaco e nellesofago intratoracico ed addominale . le indagini ecografiche sono state eseguite dallo stesso operatore . 
come punti di repere anatomici del cardias e dellesofago addominale sono stati considerati : il tratto compreso tra laorta addominale e il lobo sinistro del fegato nelle scansioni sotto - xifoidee traverse e come repere per lesofago toracico stato considerato il tratto compreso tra lobo sinistro del fegato , aorta addominale e cuore visualizzati con la scansione longitudinale sottoxifoidea . 
gli elettrodi sono stati ancorati al naso in modo da ridurre al minimo gli artefatti da movimento du594 radiol med ( 2008 ) 113 : 591598 first probe was positioned in the gastric body and the second about 5 cm above the lower oesophageal sphincter ( los )  . impedance changes were recorded 2 , 4 , 6 , 8 and 10 cm above the los . 
we considered the total number of reflux episodes and the percentage of time of oesophageal ph < 4 . the number of reflux episodes and time percentage of ph < 4 were analysed every 2 h . 
a diagnosis of gord was established when the total number of reflux episodes during 24 h was > 50 and / or the percentage of time of ph < 4 was > 6% . the sonographic classification of gord consisted of two grades : abdominal oesophagus ( grade 1 reflux ) and abdominal oesophagus + thoracic oesophagus ( grade 2 )  . 
there were no reactions or side effects to the sonographic contrast material . the contrast material was successfully administered to all children , including those who were poorly cooperative . twenty - four - hour oesophageal ph - metry confirmed the presence of reflux in the 84 patients with positive cdus findings and detected reflux in two additional patients with negative cdus findings . 
comparison of oesophageal ph - metry and cdus revealed a diagnostic accuracy of 94% and a sensitivity of 98% with a statistically significant difference ( p < 0.0001 ) at mcnemars test . discussion sonographic contrast material within the stomach and oesophagus appears polychromatic at cdus and is easily distinguished from monochromatic vascular signals ; in addition , if the prf is increased , the vascular signals will disappear , allowing selective visualisation of the contrast material . 
i cateteri sono stati introdotti per via nasale e posizionati sotto la guida di un intensificatore di brillanza : la prima sonda stata posizionata nel corpo gastrico e laltra stata posizionata 5 cm circa sopra lo sfintere esofageo inferiore ( les ) ; i cambi di impedenza sono stati registrati a 2 , 4 , 6 , 8 e 10 cm sopra il les . 
la diagnosi di ger stata posta quando il numero totale di reflussi nelle 24 ore era maggiore di 50 e / o la percentuale giornaliera di ph < 4 era pi del 6% . la classificazione eseguita con lindagine ecografica , stata suddivisa in due gradi : esofago addominale ( i grado di reflusso ) ; esofago addominale + esofago toracico ( ii grado )  . 
la ph - metria nelle 24 ore ha confermato la presenza del reflusso negli 84 pazienti positivi allindagine ecografica ed ha dimostrato la presenza di reflusso in altri 2 pazienti che erano risultati negativi allindagine ultrasonografica . 
a a large amount of us contrast agent is seen in the abdominal oesophagus ( short arrow ) ; us contrast agent inside the stomach ( long arrow )  . 
aorta , freccia corta ; l , fegato . 596 radiol med ( 2008 ) 113 : 591598 unaccuratezza del 94% e una sensibilit del 98% e una significativit statistica ( p < 0 , 0001 ) al mcnemar test . discussione il mdc ecografico nello stomaco e nellesofago appare policromatico con il color doppler ed facilmente distinguibile dai segnali vascolari monocromatici , inoltre aumentando la prf si pu ottenere la scomparsa dei segnali vascolari permettendo la visualizzazione selettiva del mdc . 
nel nostro studio due falsi negativi riscontrati con lecografia hanno mostrato il reflusso alla ph - metria tardivamente oltre 30 minuti dopo il pasto , quindi lassenza di reflusso riscontrata con lesame ecografico dovuta probabilmente alla limitata durata delleffetto cromatico del mdc nellesofago e nello stomaco , tale dato rappresenta quindi un limite della metodica ecografica . stata riscontrata piena corrispondenza con la ph - metria nella determinazione della porzione di esofago interessato dal reflusso ; ci ha permesso di formulare una classificazione ecografica distinta in due gradi di reflusso : i grado ( reflusso nella porzione addominale dellesofago ) e ii grado ( reflusso nella porzione addominale e intratoracica dellesofago )  . 
la suddetta classificazione potrebbe essere rapportata alla gravit legata al danno procurato alla mucosa dell esofago ; tali gradi potrebbero essere utilizzati per una eventuale stadiazione ecografica del reflusso . in questo lavoro il color doppler ha dimostrato sensibilit elevata , maggiore rispetto allecografia b - mode [ 27 , 28 ] , al pasto baritato con fluoroscopia [ 29 ] e al color doppler senza mdc [ 30 , 31 ]  . 
essa presenta numerosi vantaggi : assenza di reazioni ed effetti collaterali ; scarsa influenza dalla mancata collaborazione del paziente ; minore invasivit rispetto agli altri test ; facile esecuzione , riproducibilit . un altro importante vantaggio dellutilizzo dellshu 508 a quello della riproduzione di un pasto fisiologico non alterando dunque i fisiologici meccanismi prandiali cos come fig . 
this enables us to formulate a sonographic classification consisting of two grade of reflux : grade 1 ( reflux in the abdominal oesophagus ) and grade 2 ( reflux into the abdominal and thoracic oesophagus )  . 
this classification could correlate with the degree of damage sustained by the oesophageal mucosa , and the grades could be used for a sonographic staging of reflux . in our study , contrast - enhanced cdus proved to have high sensitivity , greater than that of b - mode sonography [ 27 , 28 ] , barium swallow fluoroscopy [ 29 ] and cdus without contrast agent [ 30 , 31 ]  . 
the technique has numerous advantages : no adverse reactions or side effects , limited influence of poor patient cooperation , less invasiveness with respect to other tests , easy performance and reproducibility . another major benefit of the use of shu 508 a is that it reproduces a physiological meal without affecting normal prandial mechanisms , in contrast to the barium swallow , which should be reserved for identifying anatomical abnormalities in selected cases . 
for this reason , for diagnosing gord , we propose a diagnostic workup with other tests in symptomatic patients with negative contrastenhanced cdus results ( approximately 30% of patients in our sample )  . 
 given the importance of the early diagnosis of gord in symptomatic patients , contrast - enhanced cdus could be proposed as an alternative to oesophageal ph - metry in centres lacking ph - metry equipment . 
in addition , in view of its limited invasiveness compared with other methods , the technique could be indicated for monitoring patients after surgical or medical treatment . table 3 reflux grade on color - doppler ultrasonography gord grade number of patients gord , gastro - oesophageal reflux disease tabella 3 grado di reflusso con lesame ecografico grado ger numero di pazienti i grado ii grado ger , reflusso gastro - esofageo succede per esempio per lesame radiologico con pasto baritato ; questultimo infatti dovrebbe essere riservato solo nei casi selezionati per la ricerca di anomalie anatomiche . gli svantaggi della metodica ecografica sono rappresentati essenzialmente dalla durata limitata delleffetto cromatico del mdc ; per questo motivo per la diagnosi del ger proponiamo lapprofondimento diagnostico con altre metodiche nei pazienti sintomatici negativi allesame ecografico con mdc ( circa il 30% dei pazienti del nostro campione )  . 
 data limportanza della diagnosi precoce del ger nei pazienti sintomatologici , nei centri che non dispongono dellattrezzatura per la ph - metria , il color doppler con mdc potrebbe essere proposto in alternativa alla suddetta . inoltre questa metodica potrebbe trovare indicazione nel monitoraggio dopo la terapia chirurgica o medica grazie alla scarsa invasivit rispetto alle altre metodiche . diagnostica per immagini in geriatria e . 
and the fact that he did so a few decades ago in a predominantly hedonistic society focused on the potential benefits and future prospects of the technological revolution rather than on social issues , a society where the elderly were still marginalised eloquently testifies to his far - sightedness and future orientation . in 1996 , together with his pupil teresa cammarota , he published lezioni di diagnostica per immagini in geriatria ( lectures in diagnostic imaging in geriatrics ) to share the content of his lessons at the school of specialisation in gerontology and geriatrics of turin with the entire radiological community . 
beautifully presented , the first edition provided not only a stimulus for others to learn more about the subject , but a valuable , quick - reference guide for daily practice , with elderly people being then , as now , the most regular users of radiology services . this second edition has more ambitious goals , as thanks to the impetus given by comino other texts have been produced and the interest within the italian society of radiology ( sirm ) has increased . 
if the first edition aimed primarily to promote interest in the elderly patient by introducing the novice to the basics of geriatric imaging , the new edition has taken a leap in quality by revisiting the issues in a more complete , modern and indepth fashion . 
if the first edition was deliberately basic and spartan in appearance , the layout here is more elegant and polished , and generally better suited to a book providing trained radiologists with an in - depth overview of the elderly patient . edmondo comino stato il primo cultore della radiologia geriatrica in italia : esserlo diventato qualche decennio fa , in una societ tendenzialmente edonistica concentrata di pi sulle potenzialit del boom tecnologico e dei suoi sviluppi futuri e meno sui propri aspetti sociali ove lanziano era ancora un emarginato dimostra ampiamente la sua lungimiranza e preveggenza . 
 nel 1996 assieme alla sua allieva teresa cammarota diede alle stampe le lezioni di diagnostica per immagini in geriatria mettendo a disposizione di tutti i radiologi quelle che erano delle semplici lezioni tenute alla scuola di specializzazione di gerontologia e geriatria di torino : la veste editoriale era gi eccellente , e per chi voleva quel testo era non solo uno stimolo ad approfondire largomento , ma anche una preziosissima guida ( un bignami , per chi se lo ricorda ! ) nella pratica quotidiana , visto che gi allora lanziano era il pi assiduo frequentatore dei nostri servizi . 
 questa seconda edizione nasce con pi ambiziosi traguardi , perch nel frattempo proprio grazie allimpulso di comino qualche altro testo stato prodotto e il fermento in seno alla sirm aumentato . 
se la prima edizione aveva soprattutto lo scopo di suscitare linteresse per lanziano , introducendo il neofita ai principali argomenti , questa consente di fare davvero un salto di qualit , rivisitandoli in modo pi approfondito , completo e moderno . 
cos , ogni capitolo viene corredato da ricca iconografia e da schemi e tabelle esplicativi ed sempre affiancato da un inquadramento clinico , in modo da rendere pi efficace ed integrata la trattazione . 
ancora , se la prima edizione aveva anche volutamente una veste tipografica essenziale e spartana , questa invece ne presenta una pi pretenziosa ed elegante , del tutto adeguata alla finalit di approfondire lo studio dellanziano per il radiologo formato . 
libro consigliabile a tutti , ai radiologi esperti ma radiol med ( 2008 ) 113 : 611612 this book is recommended reading for expert radiologists and especially for young radiologists , partly on account of the sensitivity ( a highly treasured quality nowadays ! ) shown by comino and his team of authors and collaborators from the turin school , a school well known for its humanity as well as for its scientific achievements . soprattutto ai giovani ; anche perch largomento viene trattato con quel giusto grado di sensibilit ( valore da tener ben presente oggigiorno ! ) , che contraddistingue comino e che coinvolge gli altri autori e i collaboratori , provenienti tutti dalla scuola torinese , nota anche per i contenuti umani oltre che scientifici . francesco schiavon dipartimento di radiologia ospedale s . 
midiri1 1dibimel , sezione di scienze radiologiche , universit degli studi di palermo , via del vespro 127 , 90127 palermo , italy 2centro medico mantia , via de spuches 22 , 90100 palermo , italy correspondence to : f . 
the aim of this study was to assess the reliability of perifascial oedema as a sonographic criterion for selecting the most appropriate treatment ( ultrasoundguided corticosteroid injection or ultrasound - guided extracorporeal shock wave therapy ) of idiopathic plantar fasciitis ( ipf )  . 
sixty - four patients with a clinical diagnosis of unilateral refractory ipf , treated conservatively for at least 8 weeks , were studied with highresolution ultrasound ( hrus )  . 
patients with an hrus diagnosis of ipf were grouped according to the presence ( a ) or absence ( b ) of perifascial oedema and then randomly allocated to treatment with corticosteroid injection ( 1 ) or extracorporeal shock wave therapy ( 2 )  . 
i pazienti con diagnosi hrus di fpi sono stati suddivisi in ( a ) presenza e ( b ) assenza di edema perifasciale e poi suddivisi random in trattati con ( 1 ) infiltrazione di corticosteroidi e ( 2 ) eswt . 
la presenza delledema perifasciale potrebbe essere un efficace criterio nellindirizzare la terapia verso le iniezioni di corticosteroidi con guida hrus . keywords plantar fasciitis sonography corticosteroid injection shock waves foot parole chiave fascite plantare ecografia iniezioni di corticosteroidi onde durto piede radiol med ( 2008 ) 113 : 486495 introduction introduzione the plantar fascia is a band of fibrous tissue extending from the lower margin of the calcaneus to the plantar surface of the metatarsophalangeal joints and the bases of the proximal phalanges of the toes [ 1 , 2 ]  . 
because of its significant biomechanical role , the plantar fascia is subjected to recurrent microtraumas at the calcaneal insertion , perpetuated by repeated strain through weight bearing and the resulting inflammatory response . 
imaging plays a fundamental role in the diagnosis of ipf as it provides confirmation of the clinical suspicion and helps in differential diagnosis and planning the most appropriate treatment [ 4 ]  . 
therapy is primarily conservative , and although effectiveness varies with the type of treatment ( or combination treatment ) , positive results have been reported in 90% of patients [ 5 ]  . 
a number of studies have also reported highly positive results for eswt with or without us guidance in treating plantar fasciitis [ 7 , 9 ]  . high - resolution us ( hrus ) is very reliable in the diagnosis of ipf , with a sensitivity of 80% and a specificity of 88.5% compared with the reference standard , magnetic resonance imaging ( mri ) [ 5 ]  . 
the purpose of this study was to evaluate the role of perifascial oedema as a sonographic criterion to assist in the choice between us - guided eswt or us - guided steroid injection for treating ipf , with clinical and hrus follow - up 6 weeks after treatment . materials and methods over a period of 18 months , 87 patients with a clinical diagnosis of unilateral heel pain treated conservatively ( nonsteroid anti - inflammatory drugs and heel cup ) for at least 8 weeks with unsatisfactory results were referred for physiatric assessment ( t0 )  . 
assessment included a detailed history of the heel pain , with special reference to duration and la fascia plantare una banda di tessuto fibroso che si estende dal margine inferiore del calcagno alla superficie plantare delle articolazioni metatarso - falangee e alla base della falange prossimale delle dita del piede [ 1 , 2 ]  . 
in relazione al suo importante ruolo biomeccanico prona a ripetuti traumi , pi propriamente microtraumi , perpetuati dalla ripetuta tensione esercitata sotto carico dal peso corporeo ( weight - bearing ) , in corrispondenza della sua inserzione calcaneare , a cui consegue una risposta infiammatoria . 
il ruolo delle metodiche di imaging nella diagnosi della fpi di fondamentale importanza poich consente la verifica del sospetto clinico , la diagnosi differenziale e la corretta pianificazione terapeutica [ 4 ]  . 
la terapia di scelta conservativa e la sua efficacia varia in funzione della tipologia adottata , a volte con terapie combinate , potendo raggiungere , come riportato in alcune casistiche , risultati efficaci nel 90% dei pazienti [ 5 ]  . 
alternative alle terapie conservative non invasive e ai trattamenti invasivi chirurgici sono le tecniche mini - invasive come le iniezioni di corticosteroidi e le onde durto ( eswt )  . 
anche per leswt , senza o con puntamento ecografico , sono stati riportati in diversi studi sono stati riportati risultati molto efficaci nel trattamento della fascite plantare [ 7 , 9 ]  . 
lecografia ad alta risoluzione ( hrus ) si dimostrata una metodica molto affidabile nella diagnosi della fpi presentando , rispetto alla risonanza magnetica ( rm ) , ritenuta il gold standard , una sensibilit del 80% e una specificit del 88 , 5% [ 5 ]  . 
scopo dello studio stato valutare il ruolo del segno ecografico edema perifasciale nella scelta del trattamento mini - invasivo ( eswt sotto puntamento ecografico o iniezioni ecoguidate di corticosteroidi ) nella terapia della fpi con una rivalutazione clinica ed hrus a 6 settimane dalla fine dei trattamenti . 488 radiol med ( 2008 ) 113 : 486495 pattern of onset , and a clinical examination with determination of body mass index ( bmi )  . 
heel pain was estimated by using a 10 - point visual analogue scale ( vas ) ranging from 1 ( no pain ) to 10 ( maximal pain )  . all patients underwent hrus on the same day as the clinical examination . 
hrus aimed to confirm the clinical diagnosis of ipf and exclude other possible diagnoses and was performed by the same radiologist ( ai ) , who was blinded to the clinical findings , in particular to the side affected and vas score . 
in patients with an hrus diagnosis of ipf , we also evaluated the presence of perifascial oedema , which is characterised by loss of definition of the fascial borders and hypoechogenicity of the neighbouring soft tissues . all patients gave their written informed consent after receiving information about the purposes of the study and a detailed explanation of the procedures involved . 
 patients with an hrus diagnosis of plantar fasciitis who gave their informed consent were divided into two groups according to the presence ( a ) or absence ( b ) of perifascial oedema . 
the two groups were then further subdivided on the basis of the treatment performed : ( 1 ) us - guided corticosteroid injection and ( 2 ) us - guided eswt . 
four subgroups were thus obtained : a1 , ipf with perifascial oedema treated with corticosteroid injection ; a2 , ipf without perifascial oedema treated with eswt ; b1 , ipf without perifascial oedema treated with corticosteroid injection ; and b2 , ipf with perifascial oedema treated with eswt . 
durante questa sono stati effettuati la raccolta dellanamnesi mirata al sintomo dolore , con particolare riferimento alla sua durata e modalit di comparsa , e lesame clinico con la determinazione dellindice di massa corporea ( bmi )  . 
il dolore stato quantizzato attraverso una visual analogue scale ( vas ) facendo indicare al paziente su una scala suddivisa in 10 punti , da 1 ( nessun dolore ) a 10 ( dolore massimo ) , lentit del dolore recepito . tutti i pazienti per validare la diagnosi clinica specialistica sono stati sottoposti ad hrus nella medesima giornata della visita fisiatrica . 
lo studio hrus mirato alla detezione dei pazienti con fpi e alla diagnosi differenziale stato eseguito in cieco dallo stesso radiologo ( a.i. ) non a conoscenza della clinica ed in particolare del lato affetto e del punteggio vas . 
normalmente la fascia plantare si presenta come una banda iperecogena a struttura fibrillare , con margini netti e regolari rappresentati da due bande iperecogene , e uno spessore inferiore a 4 mm [ 11 ]  . 
 [ 11 ] , i quali hanno osservato nel piede asintomatico di pazienti con fpi monolaterale uno spessore della fascia plantare di 3 , 830 , 72 mm [ 12 ]  . 
we used a 20 - gauge spinal needle connected to a 5 - ml syringe filled with 1 ml of methylprednisolone ( depo - medrol 40 mg , pharmacia nv / sa , puurs , belgium ) mixed with 0.6 ml of mepivacaine hydrochloride ( carbocaine 3% , astra - zeneca , milan , italy )  . 
the tip of the needle was inserted in the plantar fascia , and the corticosteroid was slowly injected within the fascia and , after partially withdrawing the needle tip , between the fascia and the fat pad . 
four sessions of eswt were carried out at weekly intervals with delivery of 2 , 000 shock waves of 0.03 mj / mm2 to the affected area via a piezoelectric device ( piezoson 100 , richard wolf , knittlingen , germany ) provided with a cylindrical probe and parabolic focus . 
us equipment was the same as that used for diagnosis and guidance . sonograms were assessed for changes in fascial thickness and echostructure and the development of complications ( fascial rupture ; fat pad atrophy )  . 
clinical improvement was defined as a significant reduction in vas score to values lower than 40.5. results all patients presented with the typical symptoms of heel pain during the first few steps after rest or on rising in the morning , which worsens progressively with increased activity . 
 i pazienti con diagnosi hrus di fascite plantare che hanno aderito ai propositi dello studio sono stati suddivisi in due gruppi in base alla presenza ( a ) o assenza ( b ) di edema perifasciale . 
sono stati ottenuti quindi 4 sottogruppi : a1 , fpi con edema perifasciale trattata con iniezione di corticosteroidi ; a2 , fpi senza edema perifasciale tratta con eswt ; b1 , fpi senza edema perifasciale trattata con iniezione di corticosteroidi ; e b2 , fpi con edema perifasciale tratta con eswt . 
 stato usato un ago spinale da 20 g connesso ad una siringa da 5 ml con 1 ml di sospensione acquosa di metil - prednisolone acetato ( depo - medrol 40 mg , pharmacia nv / sa , puurs , belgio ) misto a 0 , 6 ml soluzione iniettabile di mepivacaina cloridrato ( carbocaina 3% , astra - zeneca , milano , italia )  . 
stato impiegato un approccio plantare con inclinazione dellago obliqua caudo - craniale e antero - posteriore e sono stati utilizzati la guida connessa alla sonda ecografica e la traccia elettronica della guida da biopsia visualizzata sul monitor dellecografo . 
il trattamento eslw stato eseguito dopo puntamento ecoguidato fina490 radiol med ( 2008 ) 113 : 486495 lizzato alla localizzazione della regione inserzionale calcaneare della fascia plantare e alla focalizzazione della profondit di trattamento . 
sono state effettuate 4 sedute , una alla settimana , somministrando 2000 impulsi con una media di 0 , 03 mj / mm2 nellarea del trattamento utilizzando un apparecchiatura piezoelettrica ( piezoson 100 , richard wolf , knittlingen , germania ) con sonda cilindrica e fuoco parabolico . 
la rivalutazione strumentale stata effettuata , dopo la visita fisiatrica , con lhrus eseguita in cieco dal medesimo operatore ( a.i. ) non a conoscenza delleventuale miglioramento clinico , con la medesima apparecchiatura ecografica , precedentemente utilizzata per la diagnostica e la guida ai trattamenti , valutando la variazione dello spessore e dellecostruttura della fascia plantare e la comparsa di eventuali complicanze ( rottura della fascia ; atrofia del cuscinetto adiposo plantare )  . 
il miglioramento clinico stato giudicato efficace per riduzioni significative del vas con valori inferiori a 40 , 5 . risultati tutti i pazienti riferivano una sintomatologia tipica , caratterizzata da dolore al tallone con i primi passi dopo il riposo o insorgente al mattino ; questo inoltre si acuiva durante lattivit motoria in modo esponenziale alla durata della stessa . 
il lato affetto era il destro in 33 pazienti ( 55% ) ed il sinistro in 27 pazienti ( 45% ) , il vas medio era di 7 , 20 , 7 e lo spessore della fascia plantare nel lato affetto era di 5 , 80 , 7 mm . nei 27 / 87 pazienti ( 31 , 03% ) in cui non stata posta allhrus diagnosi di fascite plantare in 15 casi allhrus stata evidenziata una entesopatia inserzionale del tendine achilleo associata a borsite retrocalcaneare ; nei restanti 12 casi stata posta una diagnosi eziologia solo ricorrendo allintegrazione rm che ha evidenziato in 8 casi una osteocondropatia della sottoastragalica , in 2 casi una flogosi del cuscinetto adiposo calcaneare e in 2 casi una frattura da stress del calcagno . 
nei quattro sottogruppi ( a1 , a2 , b1 e b2 ) non sono state evidenziate differenze significative di et , bmi , vas e spessore della fascia plantare nel lafig . 
plantar fasciitis with thickening ( crosses ) and heterogeneous hypoechogenicity ( asterisks ) of the plantar fascia , perifascial oedema with loss of distinction of margins and hypoechogenicity of the surrounding soft tissues ( arrows ) is also seen . 
fascite plantare , caratterizzata da ispessimento ( croci ) e disomogenea ipoecogenicit ( asterischi ) della fascia plantare , coesiste edema perifasciale , caratterizzato da sfumatura dei margini e ipoecogenicit dei tessuti molli limitrofi ( frecce )  . 
mean vas score was 7.20.7 , and mean fascial thickness on the affected side was 5.80.7 mamong the 27 / 87 patients ( 31.03% ) without hrus confirmation of plantar fasciitis , the examination showed achilles tendon enthesopathy associated with retrocalcaneal bursitis in 15 cases . 
in the remaining 12 cases , the diagnosis was established with mri , which revealed osteochondropathy of the subastragalar joint in eight cases , inflammation of the calcaneal fat pad in two cases and a calcaneal stress fracture in two cases . 
there were no significant differences in age , bmi , vas score or plantar fascia thickness on the symptomatic side among the four subgroups ( a1 , a2 , b1 and b2 )  . 
fascite plantare con edema perifasciale a prima e b 6 settimane dopo trattamento ecoguidato con iniezioni di corticosteroidi : riduzione dello spessore e dellipoecogenicit della fascia plantare con scomparsa della sfumatura dei margini fasciali e dei tessuti molli limitrofi . 
among patients without perifascial oedema , clinical improvements were seen in 5 / 15 cases ( 35.71% ) in subgroup b1 with significant reduction in vas scores ( 3.80.6 ) , and in 13 / 15 cases ( 92.85% ) in subgroup b2 with vas scores of 3.20.7. 
no significant clinical improvement was obtained in 12.5% of patients in subgroup a1 , in 62.5% of those in a2 , in 64.29% of those in b1 and in 7.15% of those in b2 . 
nei pazienti senza edema perifasciale , nel sottogruppo b1 stato evidenziato un miglioramento clinico con riduzione del vas ( 3 , 80 , 6 ) in 5 / 15 casi ( 35 , 71% ) e nel sottogruppo b2 stato evidenziato in 13 / 15 casi ( 92 , 85% ) con vas di 3 , 20 , 7 . 
fascite plantare con edema perifasciale a prima e b 6 settimane dopo trattamento ecoguidato con eswt : modesta riduzione dello spessore e dellipoecogenicit della fascia plantare con riduzione della sfumatura dei margini fasciali e dei tessuti molli limitrofi . 
fascite plantare senza edema perifasciale a prima e b 6 settimane dopo trattamento ecoguidato con iniezione di corticosteroidi : modesta riduzione dello spessore dello spessore e dellipoecogenicit della fascia plantare . 
hrus is an inexpensive , dynamic and noninvasive modality that does not use ionising nel 7 , 15% di quelli del gruppo b2 non stato ottenuto un significativo miglioramento clinico . 
 discussione la fascite plantare la flogosi della fascia plantare e delle strutture limitrofe ; pu essere idiopatica o correlata a patologia sistemica ( artrite reumatoide , spondiliti sieronegative , ecc . ) o a trauma [ 13 ]  . 
listologia ha mostrato alterazioni abbastanza varie come la necrosi delle fibre collagene , la metaplasia condroide e la calcificazione della matrice , che suggeriscono il ripetersi di tensione e processi degenerativi [ 15 ]  . 
la diagnosi differenziale comprende la borsite sottocalcaneare , la frattura da stress del calcagno , la sindrome del tunnel tarsale e losteomielite del calcagno [ 12 ]  . lhrus una metodica dinamica , a basso costo , non invasiva , che non utilizza radiazioni ionizzanti , molto affidabile nellidentificazione della fpi . 
nel nostro studio stata posta la diagnosi hrus di fascite plantare in 60 su 87 pazienti ( 68 , 97% ) e nel 53 , 33% di essi stata evidenziato un edema perifasciale . 
 in letteratura ad oggi non sono stati codificati precisi criteri hrus che indirizzino , nei casi recalcitranti alla terapia conservativa , la scelta verso uno dei trattamenti miniinvasivi ( iniezioni di corticosteroidi o eswt )  . 
le iniezioni di corticosteroidi nel tallone sono utilizzate abitualmente per la terapia della sintomatologia algica e i trattamenti possono essere eseguiti con tecnica palpatoria o ecoguidata [ 2 , 9 ]  . 
questultima presenta una minore percentuale di ricaduta , 1 caso su 12 contro i 6 / 13 della tecnica palpatoria , con ridotta ricorrenza del dolore e riduzione della necessit di ripetere il trattamento [ 9 ]  . 
nel nostro studio abbiamo utilizzato un approccio plantare con inclinazione dellago obliqua caudo - craniale e antero - posteriore , inoltre abbiamo impiegato la guida connessa alla sonda ecografica e la traccia elettronica della guida da biopsia visualizzata sul 494 radiol med ( 2008 ) 113 : 486495 radiation and is very reliable in identifying ipf . 
in our study , hrus confirmed the diagnosis of plantar fasciitis in 60 out of 87 ( 68.97% ) patients , and in 53.33% of them , it revealed perifascial oedema . to date , no definite sonographic criteria have been identified to assist in selecting between steroid injection and eswt in patients not responding to conservative therapy . corticosteroid injection into the heel is commonly employed for pain control , and the injection may be carried out under palpation or us guidance [ 2 , 9 ]  . 
us - guided procedures are associated with lower recurrence rates ( 1 / 12 vs . 6 / 13 for palpation ) , with reduced pain recurrence and less need for repeat procedures [ 9 ]  . 
in our study , we used a plantar approach with oblique caudocranial and anteroposterior needle inclination , with the guide connected to the us transducer and on - screen tracking of the biopsy guide . several authors have emphasised the effectiveness of corticosteroid treatment with us guidance , with significant reduction in vas scores and thickness of the plantar fascia seen at follow - up at 3 months [ 2 , 9 ]  . 
in our study , 87.5% of patients in subgroup a1 with perifascial oedema responded well to the treatment , showing reduced mean vas score and reduced fascial thickness , whereas only 35.71% of patients in subgroup b1 without perifascial oedema responded positively . 
treatment with corticosteroid injection thus proved to be more beneficial in subgroup a1 as a result of the anti - inflammatory action of corticosteroids helping reduce the perifascial oedema caused by the chronic inflammation underlying fascial hypertrophy . a number of studies have investigated the effectiveness of eswt , with conflicting results . 
in our study , 92.85% of patients in subgroup b2 ( without perifascial oedema ) showed a good response to the treatment , with reduced mean vas scores and thinning of the plantar fascia , whereas only 37.5% of those in group a2 ( with perifascial oedema ) responded well . 
 the mechanism of action of eswt in musculoskeletal disorders is still uncertashock waves are thought to act by stimulating or reactivating the healing process , probably by disrupting avascular or hypovascular tissues to encourmonitor dellecografo . 
molti autori hanno evidenziato lefficacia del trattamento con corticosteroidi eseguito con tecnica ecoguidata con significativa riduzione del vas e dello spessore della fascia plantare alla rivalutazione a 3 mesi [ 2 , 9 ]  . 
nel nostro studio , nel sottogruppo a1 , con edema perifasciale , abbiamo evidenziato una buona risposta al trattamento con riduzione del vas medio e dello spessore della fascia plantare nel 87 , 5% dei casi mentre nei pazienti del gruppo b1 , senza edema perifasciale , abbiamo evidenziato una buona risposta al trattamento con riduzione del medio e dello spessore della fascia plantare soltanto nel 35 , 71% . 
pertanto il trattamento con iniezioni di corticosteroidi si mostrato di maggiore utilit nel sottogruppo a1 , ci da attribuire allazione antinfiammatoria dei corticosteroidi che operano nella riduzione delledema perifasciale espressione del processo flogistico cronico alla base dellipertrofia della fascia . sono stati effettuati vari studi sullefficacia del trattamento con eswt con risultati contrastanti . 
in uno studio a doppio cieco controllato randomizzato , buchbinder et al . [ 7 ] affermano la mancata evidenza di risultati che supportino lefficacia delleswt nel trattamento della fascite plantare alle rivalutazioni a 6 e 12 settimane . 
nel nostro studio , nel gruppo b2 , senza edema perifasciale , abbiamo evidenziato una buona risposta al trattamento con riduzione del vas medio e dello spessore della fascia plantare nel 92 , 85% dei casi mentre nei pazienti del gruppo a2 , con edema perifasciale , abbiamo evidenziato una buona risposta al trattamento con riduzione del vas medio e dello spessore della fascia plantare soltanto nel 37 , 5% . 
si suppone che esse agiscano stimolando o riattivando i processi di guarigione , probabilmente attraverso la rottura di aree tissutali avascolari o ipovascolari incoraggiandone la rivascolarizzazione , il rilascio locale di fattori di crescita e il reclutamento di appropriate cellule staminali che contribuiscono a una pi normale guarigione tissutale [ 16 ]  . 
lhurs un efficace strumento diagnostico per la patologia della fascia plantare e diventa fondamentale quando si deve avviare il paziente ad una delle due tecniche terapeutiche mini - invasive , leswt e le infiltrazioni con corticosteroidi . 
 radiol med ( 2008 ) 113 : 486495 age revascularisation , releasing local growth factors and recruiting appropriate stem cells conducive to more normal tissue healing [ 16 ]  . 
 our study has some limitations : ( 1 ) small size of the study population , which does not allow for statistical validation , ( 2 ) the assumption , shared by other authors , that steroid injection is effective even though , as noted by wong et al , [ 17 ] , there is no evidence of its therapeutic effect in ipf and ( 3 ) the absence of a control group receiving only conservative therapy to demonstrate that the clinical improvements were the effect of the minimally invasive treatments rather than part of the natural history and evolution of the disease . 
cataldo20 1istituto nazionale di fisica nucleare , via amendola 173 , 70126 bari , italy 2universit di bari , dipartimento di fisica , italy 3tires , center of innovative technologies for signal detection and processing , bari , italy 4saris , bari , italy 5asl , bari , italy 6dipartimento di fisica delluniversit di pisa e infn sezione di pisa , italy 7asl pisa , italy 8infn , sezione di torino , torino , italy 9infn , sezione di genova , genova , italy 10ceaden , habana , cuba 11ospedale valdese di torino and infn , sezione di torino , torino , italy 12universit di napoli federico ii , dipartimento di scienze fisiche , e istituto nazionale di fisica nucleare , sezione di napoli , napoli , italy 13asl napoli 14universit di palermo , palermo , and infn , sezione di catania , italy 15asl palermo , italy 16universit di siena , siena , e istituto nazionale di fisica nucleare , sezione di cagliari , italy 17universit di sassari , e istituto nazionale di fisica nucleare , sezione di cagliari , italy 18asl sassari , italy 19dipartimento di fisica universit di lecce and infn , lecce , italy 20dipartimento di scienza dei materiali , universit di lecce e infn , lecce , italy correspondence to : s . 
the digitised images were collected beginning in 1999 by a community of physicists in collaboration with radiologists in several italian hospitals as a first step in developing and implementing a computer - aided detection ( cad ) systeall 3 , 369 mammograms were collected from 967 patients and classified according to lesion type and morphology , breast tissue and pathology type . 
le immagini sono state raccolte dal 1999 da un gruppo di fisici in collaborazione con radiology di alcuni ospedali italiani , come primo passo dello sviluppo e implementazione di un sistema di computer aided detection ( cad )  . 
una interfaccia grafica opportunamente progettata stata sviluppata per la visualizzazione e lelaborazione delle mammografie digitalizzate al fine di 478 radiol med ( 2008 ) 113 : 477485 point for developing other medical imaging applications , such as a breast cad , currently being upgraded and optimised for use in a distributed environment with grid services , in the framework of the instituto nazionale di fisicia nucleare ( infn ) - funded medical applications on a grid infrastructure connection ( magic ) - 5 project . keywords database mammography medical image processing grid poter supportare direttamente una diagnosi medica su monitor ad alta risoluzione . 
il database ha rappresentato il punto di partenza per lo sviluppo di altre applicazioni di imaging medicale come il cad mammografico costantemente ottimizzato e aggiornato con luso di un ambiente distribuito che dispone di servizi grid , nel framework del progetto magic - 5 , finanziato dellinfn . parole chiave database mammografia elaborazione di immagini mediche grid introduction introduzione a medical image data set is the starting point for important epidemiological and statistical studies . 
usually , it is used to develop and test algorithms for computer - aided detection ( cad ) systems but it is used also for teaching and training medical students or as an archive of rare cases . 
presently , many large data sets of digitised mammograms are available on the web [ 3 , 4 ]  . other grid - based databases are described in the literature [ 5 , 6 ]  . 
the development of a cad system is strictly tied to collection of a large data set of selected images . in this paper , a full description of the medical application on a grid infrastructure connection ( magic ) - 5 database , whose collection started in a previous project , grid platform for computer aided library in mammography ( gpcalma ) , is given . 
 un dataset di immagini cliniche la base per importanti studi epidemiologici e statistici : di norma , esso usato per sviluppare e testare algoritmi per sistemi cad , ma anche per linsegnamento e laddestramento di studenti di medicina o come archivio di casi rari . 
pi recentemente il progetto medical imaging resource center ( mirc ) dellrsna [ 2 ] ha proposto un sistema molto generale per immagazzinare e pubblicare immagini mediche , innanzitutto per supporto di ricerca e di studio , che potesse mettere insieme un gran numero di database remoti e renderli accessibili come un tuttuno . 
altri database basati su grid sono descritti in letteratura [ 5 , 6 ]  . lo sviluppo di un sistema cad strettamente legato alla raccolta di un ampio dataset di immagini selezionate . in questo lavoro viene data una completa descrizione del database di magic - 5 ( medical application on a grid infrastructure connection ) , la cui raccolta cominciata in un progetto precedente ( gpcalma , grid platform for computer aided library in mammography )  . materials and methods materiali e metodi images were acquired in various mammographic centres using different mammographic screen / film systems and settings ( all with molybdenum anode ) in the framework of different applications , including both clinical routine carried out on symptomatic women and screening programmes addressing asymptomatic women . 
a workstation , composed of a personal computer ( pc ) runle immagini sono state acquisite in vari centri di mammografia usando differenti sistemi e settaggi mammografici di tipo screen / film ( tutti con anodo di molibdeno ) , nellambito di varie applicazioni , incluse sia procedure cliniche su donne sintomatiche , sia programmi di screening rivolti a donne asintomatiche . 
una stazione di radiol med ( 2008 ) 113 : 477485 ning the linux operating system , a film scanner and a dedicated disk , was installed at each site involved in the programme . 
each image was initially saved in a file with a special format ( called calma ) consisting of a header including the information on row and column number and a sequence of bytes with pixel intensity . 
these numbers are used to transform the vector in a matrix : each pixel of the image can be represented by a triplet ( r , c , i ) where r is the row number , c is the column number and i is the intensity of the pixel ranging from 0 ( black ) to 4 , 095 ( white )  . 
in sites where clinical studies were performed , the pc was connected to a high - resolution and high - luminosity black - and - white liquid crystal display ( lcd ) monitor . 
all mammograms in the calma database that were digitised with a scanner are available in digital imaging and communications in medicine ( dicom ) file format [ 8 ]  . 
data are not stored as dicomdir , as we want to preserve the granularity at the level of the single image to be able to process each image individually and to run parallel analysis on distributed data . each exam is stored in a directory , which contains one dicom file per image , including a collection of tags , values , types , length and value fields describing patient information , imaging procedure information and other image related information . 
the diagnosis is provided according to classification criteria proposed by the american college of radiology [ 9 ] and , if required , is available as a text file . the patient related information includes an identification string uid gender and birth date . 
 the image - related information includes image type ( scanned / digital ) , study date , study identification ( id ) , series description , image laterality , view position , series number , pixel pitch and name and address of the institution where taken . 
when available , information about the device manufacturer , acquisition and calibration parameters ( model name , tube voltage and current , anode features ) is also provided . the database is still growing , mostly including new cases that are now mainly from digital mammograms : in that case , the information tags of the dicom file are all those provided by the acquisition device . database description the database is composed of 3 , 369 mammographic images , each including data and clinical information . 
i parametri degli scanner ccd usati sono stati [ 7 ] : la misura del pixel di 85 m e una profondit di 12 bit ( 4096 livelli di grigio )  . 
ciascuna immagine stata inizialmente salvata in uno speciale formato ( chiamato formato calma ) , che consiste in un header che include le informazioni su numero di riga e colonna e una sequenza di bytes con lintensit del pixel . 
questi numeri sono usati per trasformare il vettore in una matrice : ciascun pixel dellimmagine pu essere rappresentato da una tripletta ( r , c , i ) , dove r il numero di riga , c il numero di colonna e i lintensit del pixel , che varia tra 0 ( nero ) a 4095 ( bianco )  . 
i dati non sono stati conservati come dicomdir poich volevamo preservare la granularit a livello di singola immagine , in modo tale da poter processare ciascuna immagine individualmente e gestire analisi parallele su dati distribuiti . 
ciascun esame archiviato in una directory , che contiene un file di tipo dicom per immagine , con un insieme di etichettte , valori , tipi , lunghezze e valori di campi che descrivono informazioni del paziente , informazioni sulle procedure di imaging e altre informazioni sullimmagine . 
il nome in chiaro solo se lo si richiede allo scopo di uniformarsi alle richieste di privacy : la correlazione tra lesame uid e lidentit del paziente conservata in un database locale privato su ciascun sito . 
 linformazione relativa allimmagine include il tipo di immagine ( scansionata / digitale ) , la data dellesame , lid dellesame , la descrizione della serie , il lato dellorgano indagato , la vista , il numero di serie , il passo del pixel , il nome e lindirizzo dellistituto dove stato effettuato lesame . 
quando disponibile , vengono forniti anche linformazione sulla casa costruttrice dello strumento , i parametri di acquisizione e calibrazione ( nome del modello , alimentazione del tubo e corrente , caratteristiche dellanodo )  . il database tuttora in crescita , vengono inclusi nuovi casi che sono adesso per la maggiore parte provenienti da mammografi digitali : in questo caso le informazioni del file dicom sono quelle provenienti dallo strumento di acquisizione . 480 radiol med ( 2008 ) 113 : 477485 age40 years age > 70 years 1 image 6 images 40 years < age50 years 60 years < age70 years 2 images 3 images 50 years < age60 years 5 images 4 images fig . 
the repartition of the database in left / right breast images is 1 , 835 ( 51% ) and 1 , 734 ( 49% ) , respectively , whereas for the craniocaudal / oblique / lateral views , it is 1 , 601 ( 48% ) , 1 , 456 ( 43% ) and 312 ( 9% ) , respectively . 
all mammographic images with extra information related to the patient ( follow - up , age , and interesting cases ) were collected in the italian hospitals involved in the collaboration from 1997 to 2002 . 
 prior to being processed , all images were anonymised . all the images containing one ( or more ) lesions were classidescrizione del database il database composto da 3369 immagini mammografiche , ciascuna delle quali include dati e informazioni cliniche . 
la ripartizione delle immagini in destre / sinistre 1835 ( 51% ) and 1734 ( 49% ) rispettivamente , mentre la ripartizione cranio - caudale / obliqua / laterale 1601 ( 48% ) , 1456 ( 43% ) e 312 ( 9% ) rispettivamente . 
la dimensione delle immagini 20672657 pixels , 85 m di passo ( 300 punti / pollice ) ; la dimensione di ogni file , nel formato calma , circa 11 mbytes . 
tutte le immagini mammografiche , con le relative informazioni extra ( follow - up , et del paziente e casi di interesse ) , sono state raccolte dal 1997 al 2002 negli ospedali italiani coinvolti nella collaborazione . 
tutte le immagini del database , contenenti una o pi lesioni sono state classificate secondo il tipo di lesione ( massa o microcalcificazione ) , il suo grado di malignit , il tipo di tessuto della mammella , ecc . nel database ci sono 306 ( 32% ) immagini provenienti da soggetti definiti normali ( bi - rads r1 ) ovvero senza alcuna evidenza di lesione ( confermato da tre anni di follow - up radiologico )  . 
la distribuzione reradiol med ( 2008 ) 113 : 477485 table 1 histotypes as classified in the database tabella 1 istotipi presenti nel database histotype number istotipo numero invasive lobular carcinoma lobular carcinoma in situ ductal invasive carcinoma ductal in situ carcinoma papilloma intraductal dysplasia fibrosis fibroadenoma fibrocystic disease sclerosing adenosis epithelial hyperplasia adenosis tubular carcinoma mucinous carcinoma total carcinoma lobulare invasivo carcinoma lobulare in situ carcinoma duttale invasivo carcinoma duttale in sito papilloma intraduttale displasia fibrosi fibroadenoma malattia fibrocistica adenosi sclerosante iperplasia epiteliale adenosi carcinoma tubulare carcinoma mucinoso totale fied according to the kind of lesion ( mass or microcalcification ) , malignancy grade , breast texture type , etc . 
 in this database , there are the images from 306 ( 32% ) patients who were defined as normal [ breast imaging reporting and data system ( bi - rads ) r1 ] when there was no evidence of any lesion ( confirmed by 3 years of radiological follow - up )  . 
the remaining images are from 661 ( 68% ) abnormal patients : when a suspicious lesion was found by the radiologist in these images , it was classified as suspicious , benign or malignant . 
 there are 1 , 062 images containing at least one region of interest ( roi ) with a massive lesion and 304 images containing at least one roi with microcalcifications . 
in total , there are 1 , 296 ( 38% ) abnormal images containing at least one lesion ( massive or microcalcification or both ) and 2 , 073 ( 62% ) normal images with no lesions . 
each image can also contain more than one lesion , so the total number of rois is 1 , 620 ( 1 , 236 massive and 384 microcalcification )  . 
we adopted the scheme of lattanzio and guerrieri [ 10 ] , which has been recognised as a satisfactory reference framework by a national panel of radiologists , with more than 20 years of experience in mammography , who identified and localised each lesion according to this classification . 
each abnormal image comes with a description of the lesion , as shown in lativa del grado di malignit delle lesioni : 560 ( 35% ) sospette , 468 ( 29% ) benigne e 592 ( 37% ) maligne . 
le immagini contenenti almeno una massa o un cluster di microcalcificazioni , secondo la diagnosi del radiologo , sono considerate anormali . il database contiene 1062 immagini con almeno una regione di interesse ( roi ) con una lesione massiva e 304 images con almeno una roi contenente un cluster di microcalcificazioni . 
in totale ci sono 1296 ( 38% ) immagini patologiche contenenti almeno una lesione ( massa o microcalcificazione o entrambi ) e 2073 ( 62% ) immagini normali , senza lesione alcuna ; unimmagine pu contenere anche pi di una lesione , per cui il numero totale di roi 1620 ( 1236 masse e 384 micro calcificazioni )  . ciascuna di queste principali classi di lesioni ( cluster di microcalcificazioni e lessioni massive ) viene ulteriormente classificata secondo le caratteristiche morfologiche . 
nel nostro database viene adottato lo schema di lattanzio e guerrieri [ 10 ] , che stato riconosciuto come un valido schema di riferimento da un certo numero di radiologi italiani , con pi di 20 anni di esperienza , che identificano e localizzano le lesioni secondo tale classificazione . 
ciascuna immagine patologica contiene una descrizione delle lesioni come mostrato nelle tabelle 2 e 3 , in cui riportata la suddivisone delle roi per diversi tipi di massa e di microcalcificazione , con il corrispondente numero di immagini che presentano quel dato tipo di lesione . la posizione e la grandezza della massa sono definite da un cerchio tracciato dal radiologo , con le coordinate del centro { xrad ; yrad } e il raggio { rrad } , contenente per intero la massa . 
i raggi delle masse variano da 3 , 1 mm a 47 , 2 mm , con una media di 11 , 7 mm , mentre il raggio delle microcalcificazioni varia da 1 mm a 72 , 8 mm con una media di 11 , 9 mm . 482 radiol med ( 2008 ) 113 : 477485 table 2 different kinds of masses present in the database ; others includes a combination of the types mentioned in the text . 
riportato il numero di immagini contenente ciascun tipo di massa regions of interest images regioni di interesse immagini masse tipo massive lesions type irregular roundish opacity spiculated opacity regular roundish opacity parenchymal distortion blurred roundish opacity fibroadenoma others total 1 , 236 1 , 062 opacit rotonda irregolare opacit spiculata opacit rotonda regolare distorsione parenchimale opacit rotonda sfumata fibroadenoma altre totale 1236 table 3 different kinds of microcalcifications present in the database . 
riportato il numero di immagini contenente ciascun tipo di lesione microcalcifications type regions of interest images regioni di interesse immagini microcalcificazioni tipo glandular mixed lobular scattered ductal teacup eggshell tubular total ghiandolare misto lobulare sparso duttale teacup eggshell tubulare totale 1062 tables 2 and 3 , in which the partition of the rois for different kind of massive lesions and microcalcifications , with the corresponding number of images from which each kind of lesions comes , is reported . 
 mass location and size is defined by a radiologist - drawn circle , characterised by centre coordinates ( xrad ; yrad ) and radius ( rrad ) , which fully contains the mass . 
as far as the breast background is concerned , in the magic - 5 database , we adopt a tissue classification recognised as a standard by many italian radiologists [ 11 , 12 ] : 1 . 
ai radiologi della collaborazione stato chiesto di identificare il tessuto mammario per una completa caratterizzazione dellimmagine mammografica . per quanto riguarda il tessuto mammario presente nel database magic - 5 , la classificazione adottata quella riconosciuta come standard da molti radiologi italiani [ 11 , 12 ] : 1 . 
tessuto denso : indica un parenchima mammario denso ( percentuale di tessuto denso > 75% )  . la classificazione del tessuto mammario basata solo sullapparenza del parenchima , senza tener conto del tipo di pelle , della vascolarit , della presenza / assenza di masse e / o calcificazioni , dei linfonodi , n della corrispondenza , della storia della malattia , dellet e della storia familiare . radiol med ( 2008 ) 113 : 477485 dense ; 135 ; 4% fibroadipose ; 1179 ; 35% glandular ; 2055 ; 61% fig . 
dense tissue indicates a dense breast parenchyma . ( dense tissue percentage > 75% ) breast background classification is based only on the appearance of the parenchyma , without any reference to skin , vascularity , presence / absence of masses , calcifications or lymph nodes or to parity , history of breast disease , age and family history . 
most of the images are glandular like : the detection of pathological structures in this kind of image is a relatively hard task , as the target is surrounded by a noisy environment . 
images were collected in different clinical and screening conditions , so they do not represent a typical distribution of masses and microcalcifications in terms of ratio of benign to malignant cases ; moreover , they were collected from different centres and were acquired with different mammography units under different conditions . 
however , the uniformity of the digitisation makes the database technically suitable for research studies devoted to the application of cad procedures and also in a epidemiologically heterogeneous scenario . the database represents the largest italian sample of digitised mammograms . 
it has been successfully used for developing and testing the magic - 5 cad system [ 7 , 13 , 14 ] , and integrated into a grid environment [ 15 ] so that distributed data can be remotely accessed and analysed . 
it has been the basis of an experimental study about the peculiarities of computer display for reporting [ 16 ] , and it has been used to test the performance of different cad systems as second readers [ 17 ]  . 
la maggioranza delle immagini sono di tipo ghiandolare , cosa che rende particolarmente difficile la rilevazione delle strutture patologiche dal momento che le stesse sono circondate da un fondo rumoroso . linformazione sul tessuto mammario trasferita da ciascun paziente a ciascuna immagine estratta da quel paziente per lanalisi poich il cad testato su questo database analizza ogni singola vista indipendentemente . il database presenta alcune limitazioni , specialmente dal punto di vista epidemiologico : le immagini sono state raccolte in condizioni cliniche differenti , per cui non riproducono la tipica distribuzione di masse / microcalcificazioni in termini di rapporto benigne / maligne ; inoltre , essendo state raccolte in differenti centri , le immagini sono state acquisite con diversi mammografi e in differenti condizioni . 
in ogni caso , luniformit del processo di digitalizzazione rende il database adatto a studi di ricerca focalizzati allapplicazione di cad anche in presenza di uno scenario eterogeneo dal punto di vista epidemiologico . il database rappresenta il pi ampio campione di immagini mammografiche in italia ed stato utilizzato con successo per lo sviluppo e il test dei sistemi cad della collaborazione magic - 5 [ 7 , 13 , 14 ] , nonch integrato in un ambiente grid [ 15 ] , in modo che sia possibile laccesso e lanalisi in remoto delle immagini e dei dati distribuiti . 
il database stato alla base degli studi sperimentali circa le peculiarit della refertazione a video [ 16 ] ed stato usato per verificare lefficacia di diversi cad come secondo lettore [ 17 ]  . 
inoltre stato utilizzato con successo [ 18 ] per lo sviluppo di un sistema cad per lidentificazione di cluster di microcalcificazioni allinterno di un database distribuito europeo di immagini mammografiche nellambito del progetto mammogrid [ 1921 ] , dopo aver riscalato le immagini in termini di passo e range dimanico , nella fase di training di una classificazione neurale . lapproccio grid al crescere delle dimensioni del database la natura distribuita della collaborazione pone un ulteriore problema : analogamente a quanto avviene in un programma di screening , i dati sono raccolti in siti geograficamente separati e generalmente non replicati tra un sito e laltro . 
nel paradigma della grid ( spostare i programmi invece dei dati ) un sito che ospita una frazione del database distribuito deve fornire una certa quantit di potenza di calcolo condivisa oltre alle risorse di storage . 
le tecnologie grid non rendono pos484 the grid approach the growth of the database and the distributed nature of the collaboration raises a problesimilarly to what happens in a screening programme , data are collected from several geographically remote sites and are generally not replicated between sites . 
in the grid paradigm ( move code rather than data ) , a site hosting a fraction of the distributed database should provide not only storage resources but also some shared computational power . 
grid technologies thus allow not only interactive online diagnosis , but also image analysis locally with respect to the data , with a relevant reduction of the delays presently associated with the diagnosis in screening programmes . 
also , they can , for example , allow researchers with limited access to computational resources or network bandwidth to remotely process a large database , possibly with some degree of parallelisprivacy policies are easily enforced , as in some use cases , the original images never leave the local network of the site . 
from the grid point of view , it is based on the aforementioned model in which input data are not moved and their analysis is run in parallel on the nodes where they are stored and , if possible , interactively . 
from this point of view , the collaboration can be seen as a vo with common services ( data and metadata catalogue , job scheduler , information system ) running on a central server and a number of distributed nodes ( clients ) providing computing and storage resources . integration of tools for remote disk storage access into the cad system has successfully been tested : a prototype that makes it possible to share data between the different sites of the research and to run cad from remote sites has been built [ 8 , 15 ]  . 
the next step is to transfer the prototype into a clinical environment , involving radiologists collaborating in the project , to implement telediagnosis and telescreening . conclusions the database collected represents a useful archive of digitised mammographic images . 
it can be a valuable tool to the scientific community for different tasks such as training and radiol med ( 2008 ) 113 : 477485 sibile solo la diagnosi interattiva on - line , ma anche lesecuzione asincrona di analisi di immagini localmente rispetto ai dati , potenzialmente riducendo i tempi di attesa per la diagnosi nei programmi di screening ; o possono permettere a ricercatori con limitato accesso a risorse di calcolo o di rete , ad esempio , di processare remotamente un database di grandi dimensioni , eventualmente anche con qualche grado di parallelismo . 
inoltre , limplementazione di criteri di privacy e riservatezza pu essere semplificata , dato che in alcuni use case le immagini originali non escono mai dalla rete locale del sito che le ospita . questo approccio , che contraddistingue i progetti basati sulle tecnologie grid , li differenzia dai progetti orientati alla sola raccolta e pubblicazione di database , come liniziativa mirc del rsna [ 2 ] , che offre una piattaforma per organizzare e rendere accessibili on - line raccolte di immagini mediche digitali , ma richiede sempre il download completo dei file da esaminare . per la realizzazione dellinfrastruttura grid stata creata una virtual organization ( vo ) , i cui membri possono essere autorizzati a condividere dati e risorse per implementare use case di screening , tele - diagnosi e tele - training in ambito mammografico . 
il prototipo implementa il menzionato modello in cui a spostarsi da un sito allaltro il codice eseguibile invece delle immagini , che vengono analizzate in parallelo e , quando possibile , interattivamente , nei diversi siti in cui sono conservate . 
da questo punto di vista , la collaborazione pu essere vista come una vo con servizi comuni ( data e metadata catalogue , job scheduler , information system ) ospitati su un server centrale ed un certo numero di nodi distribuiti ( client ) che forniscono le risorse di storage e calcolo . 
 lintegrazione nella stazione cad delle funzionalit per laccesso alle risorse grid stata realizzata in un prototipo che rende possibile la condivisione di dati tra i siti che compongono linfrastruttura e lesecuzione remota da un sito allaltro di algoritmi cad [ 8 , 15 ]  . 
il passo successivo sar linstallazione del prototipo in ambiente clinico , con il coinvolgimento dei radiologi che partecipano alla collaborazione , per implementare gli use case di tele - diagnosi e telescreening . conclusioni il database raccolto rappresenta un utile archivio di immagini mammografiche digitalizzate , che pu efficacemente essere usato dalla comunit scientifica per svariati scopi come laddestramento di strumenti di classificazione basati su reti neurali [ 2325 ] , per uso didattico e per studi statistici ed epidemiologici . radiol med ( 2008 ) 113 : 477485 testing of neural - network - based classification tools [ 2325 ] , for retrieval use and for statistics and epidemiology studies . 
its integration in a grid computing environment makes possible the implementation of several remote - analysis - use cases , in which we demonstrate functionalities that can prove useful in screening programmes and teletraining . analogamente a quanto avviene nei programmi di screening , i dati sono raccolti e conservati in siti geograficamente distinti . 
lintegrazione del database in un ambente grid ha reso possibile limplementazione di alcuni use case di analisi remota , con i quali sono dimostrate funzionalit utili in programmi di screening e tele - training . acknowledgements this work was made in the framework of the magic - 5 collaboration . 
bellomi1 , 3 1divisione di radiologia , 2divisione di urologia , istituto europeo di oncologia irccs , via ripamonti 435 , 20141 milano , italy 3facolt di medicina e chirurgia , universit degli studi di milano , via festa del perdono 7 , 20122 milano , italy 4divisione di anatomia patologica e medicina di laboratorio , istituto europeo di oncologia irccs , via ripamonti 435 , 20141 milano , italy correspondence to : g . 
transverse , sagittal and coronal t2 - weighted and t1 - weighted ( before and after intravenous gadolinium injection ) images were obtained with a four - channel phased - array coil . 
confrontare la stadiazione locale del tumore del pene definita con la risonanza magnetica abbinata allerezione farmacologicamente indotta con iniezione intracavernosa di prostaglandine ( rm con test di farmacoinfusione intracavernosa , rm - tfi ) con lesame clinico e con lanatomia patologica . 
tredici pazienti con tumore del pene mai trattato sono stati esaminati con rm - tfi ( ottenuta con iniezione intracavernosa di 10 g di prostaglandine e1 )  . sono state acquisite immagini assiali , coronali e sagittali pesate in t2 e t1 ( prima e dopo iniezione endovenosa di gadolinio ) , utilizzando una bobina phased - array a quattro canali . 
la rm - tfi si dimostrata superiore allesame clinico e ha modificato la strategia terapeutica in tre pazienti . 517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 518 radiol med ( 2008 ) 113 : 517528 keywords penile cancer magnetic resonance imaging intracavernosal injection of prostaglandin e1 ( pge1 ) tunica albuginea preoperative local staging parole chiave tumore del pene risonanza magnetica iniezione intracavernosa di prostaglandine e1 ( pge1 ) tonaca albuginea stadiazione locale pre - operatoria introduction introduzione penile cancer is extremely rare in europe and north america , where it accounts for 0.4%0.6% of all malignancies in men . 
it is , however , a major health problem in developing countries , and in some countries of south america , asia and africa , it constitutes 10%20% of all male malignancies [ 1 , 2 ]  . although partial or total penectomy is the treatment of choice in that it allows long - term palliation and good survival , even in patients with advanced disease , the anatomical disfigurement and the psychological morbidity resulting from penile amputation have encouraged the use of organsparing strategies , such as external beam radiation therapy , brachytherapy , cryotherapy , mohs microsurgery , laser ablation or partial excision . 
however , the success of these procedures was found to be satisfactory when the patients were correctly selected and the lesion confined to the tunica albuginea without involvement of the corpora cavernosa or corpus spongiosum ( stage tis and t1 tumours ) [ 3 ]  . 
patients with tumours confined to the tunica albuginea ( tis , t1 ) can be treated by organ - sparing surgery , whereas those with tumours involving the tunica albuginea and invading the corpus spongiosum or corpora cavernosa ( t2 ) , the urethra or the prostate ( t3 ) , or adjacent structures ( t4 ) require conventional surgery , that is , partial or total penectomy . clinical examination , urethrography , cavernosography and ultrasound [ 47 ] are the most commonly used techniques in local staging . 
few studies have investigated the use of mri in conjunction with pharmacologically induced penile erection ( pipe ) [ 2 , 8 ] , though the technique has been proposed in selected cases [ 911 ]  . the aims of our study were to compare the local staging of penile cancer by mri with artificial erection induced by intracavernosal prostaglandin e1 ( pge1 ) injection ( mripipe ) with the clinical examination and pathology and to verify whether mri - pipe led to changes in the choice of treatment strategy . il tumore del pene estremamente raro in europa e negli usa , dove rappresenta lo 0 , 4%0 , 6% di tutti i tumori maligni maschili ; al contrario esso un problema sanitario rilevante nei paesi in via di sviluppo : rappresenta il 10%20% dei tumori maligni maschili nei paesi dellamerica del sud , dellasia e dellafrica [ 1 , 2 ]  . sebbene la penectomia parziale o totale rappresenti la terapia di elezione , consentendo una buona palliazione a lungo termine e una buona sopravvivenza anche in pazienti con malattia in stadio avanzato , la menomazione anatomica e la morbilit psicologica derivanti dallamputazione del pene hanno indirizzato verso trattamenti conservativi , come la radioterapia con fasci esterni , la brachiterapia , la crioterapia , la chirurgia sotto controllo microscopico secondo mohs , lablazione laser o lescissione . 
gli studi pubblicati sulla chirurgia conservativa descrivono per lo pi esperienze con pochi pazienti provenienti da un singolo istituto , ma il successo di queste procedure stato soddisfacente quando i pazienti erano selezionati correttamente e la lesione era confinata alla tonaca albuginea e non coinvolgeva i corpi cavernosi o il corpo spongioso ( stadio t in situ e stadio t1 ) [ 3 ]  . 
la determinazione del coinvolgimento della tonaca albuginea perci il criterio fondamentale per la decisione terapeutica : i pazienti con tumore confinato alla tonaca albuginea ( tis , t1 ) possono essere trattati con chirurgia conservativa , mentre i pazienti con tumore che ha coinvolto la tonaca albuginea , invadendo il corpo spongioso o i corpi cavernosi ( t2 ) , luretra o la prostata ( t3 ) , o le strutture adiacenti ( t4 ) devono essere trattati con chirurgia convenzionale , con la penectomia parziale o totale . lesame clinico , luretrografia , la cavernosografia e lecografia [ 47 ] sono le tecniche pi spesso utilizzate per la stadiazione locale . 
la risonanza magnetica ( rm ) ha dimostrato grandi potenzialit , con unaccuratezza superiore all80% nel determinare lestensione locale del tumore [ 1 ]  . in letteratura , la rm associata allerezione peniena farmaco indotta stata poche volte sperimentata [ 2 , 8 ] o proposta in casi selezionati in poche rassegne sul tema [ 911 ]  . obiettivi del nostro studio sono : confrontare la stadiazione locale del tumore del pene con rm abbinata allerezione farmacologicamente indotta con iniezione intracavernosa di prostaglandine ( rm - tfi ) con lesame clinico e con lanatomia patologica e verificare se la rm - tfi abbia determinato cambiamenti nella scelta della strategia terapeutica . 517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 519 radiol med ( 2008 ) 113 : 517528 materials and methods the study was approved by the institutional ethics committee . 
between june 2001 and october 2006 , we prospectively enrolled 13 consecutive patients ( age range , 4779 years , mean age 55.4 years ) with untreated penile cancer after having obtained patients written informed consent . 
a urologist with 20 years of experience in penile cancer carried out all clinical examinations , establishing tumour extent and invasion of the penile structures to stage the tumours in accordance with the tnm criteria of the american joint committee on cancer of 2002 . 
mri - pipe was performed within 10 days of the clinical examination . all patients received premedication with intracavernosal injection of 10 g of pge1 2030 min before the beginning of the mri examination . 
the penis was dorsiflexed against the abdomen , wrapped in folded gauze to avoid direct contact with the coil or abdomen and immobilised with adhesive tape fixed to the abdomen and lateral support structures ( mri spacer pads ) to avoid longitudinal and lateral movements due to involuntary contractions of the bulbocavernosal muscles during erection . 
in addition , patients were instructed to breathe regularly and avoid any voluntary contraction of the penile muscles . mri was performed with a 1 - tesla magnet ( signa horizon lx , general electric , milwaukee , wi , usa ) using a phased - array coil . 
images were obtained in the axial , coronal and sagittal planes using the following sequences : t1weighted two - dimensional spin echo ( se ) [ tr 380 ms , te 14 ms ( 3 , 500 / 104 ) , echo train length 12 , slice thickness 3 mm , gap 0.3 mm , five averages , matrix 320224 , fov 240 mm ] and t2 - weighted two - dimensional fast spin echo ( fse ) [ tr 3 , 500 ms , te 104 ms ( 380 / 14 ) , echo train length 12 , slice thickness 3 mm , gap 0.3 mm , five averages , matrix 320224 , fov 240 mm ]  . 
after an initial t1 - weighted axial acquisition without contrast administration , t2 - weighted sagittal images were acquired to plan the t2 - weighted paracoronal and para - axial images to be obtained parallel and perpendicular to the long axis of the penis , respectively . further t1 - weighted sagittal , paracoronal and para - axial images , superimposable to the t2 - weighted images , were also acquired before and after the intravenous injection ( 0.2 ml / kg ) of contrast material [ gadolinium diethylene triamine pentaacetate acid ( gd - dtpa ) ]  . one radiologist , with 10 years of experience in urological imaging and unaware of the results of the clinical examination , performed the mri staging in accordance with the tnm classification of the american joint committee on cancer of 2002 . 
as reported in the literature [ 9 , 11 ] , these apmateriali e metodi lo studio stato approvato dal comitato etico istituzionale . tra giugno 2001 e ottobre 2006 , sono stati arruolati in maniera prospettica 13 pazienti consecutivi ( range di et 4779 anni ; et media 55 , 4 anni ) con tumore del pene non trattato , dopo aver ottenuto un consenso informato scritto . in tutti i pazienti sono stati eseguiti esame clinico ed rmtfi per la stadiazione locale del tumore . 
un urologo , con 20 anni di esperienza nei tumori del pene , ha effettuato lesame clinico , definendo lestensione del tumore e linfiltrazione delle diverse strutture del pene , proponendo una stadiazione in accordo con i criteri tnm dellamerican joint committee on cancer del 2002 . 
tutti i pazienti sono stati sottoposti a premedicazione , tramite iniezione intracavernosa di 10 g di prostaglandine , 2030 minuti prima dellorario fissato per linizio dellesame rm . tutti i pazienti sono stati posizionati sul lettino della rm in posizione supina e con i piedi rivolti in avanti . 
il pene stato dorsiflesso sulladdome , avvolto in garze ripiegate per evitarne il contatto diretto con la bobina o laddome e immobilizzato tramite cerotti fissati alladdome e alle strutture laterali di sostegno ( cuscini distanziatori da rm ) , per evitare movimenti longitudinali e laterali , dovuti ad eventuali contrazioni involontarie dei muscoli bulbo - cavernosi durante lerezione . 
i pazienti , inoltre , sono stati istruiti ad effettuare atti respiratori regolari e ad evitare ogni contrazione volontaria della muscolatura del pene . limaging rm stato ottenuto con un magnete da 1 t ( signa horizon lx , general electric , milwaukee , wi , usa ) , utilizzando una bobina phased - array . 
le immagini t1 pesate , spin echo ( se ) bidimensionali ( tr 380 ms ; te 14 ms [ 3500 / 104 ] ; echo train lenght 12 ; spessore di fetta 3 mm ; gap 0 , 3 mm ; 5 medie , matrice 320224 ; fov 240 mm ) e t2 pesate , sequenze fast spin echo ( fse ) bidimensionali ( tr 3500 ms ; te 1o4 ms [ 380 / 14 ] ; echo train lenght 12 ; spessore di fetta 3 mm ; gap 0 , 3 mm ; 5 medie , matrice 320224 ; fov 240 mm ) , sono state acquisite nei piani assiali , coronali e sagittali . 
dopo unacquisizione t1 pesata senza mezzo di contrasto secondo il piano assiale , sono state acquisite immagini t2 pesate sagittali , per unaccurata pianificazione di immagini para - coronali e para - assiali t2 pesate , rispettivamente parallele e perpendicolari allasse maggiore del pene . 
inoltre sono state acquisite ulteriori immagini t1 pesate sagittali , para - coronali e para - assiali , sovrapponibili alle immagini t2 pesate , prima e dopo liniezione ( 0 , 2 ml / kg ) endovenosa di mezzo di contrasto ( gd - dtpa )  . un radiologo , con dieci anni di esperienza in radiologia urologica , ignaro dei risultati dellesame clinico , ha effettuato la stadiazione rm , in accordo con la classificazione tnm dellamerican joint committee on cancer del 2002 . 
 nella interpretazione delle immagini , dapprima sono state identificate le normali strutture anatomiche , che , in accordo con quanto riportato in letteratura [ 9 , 11 ] , sono vi517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 520 radiol med ( 2008 ) 113 : 517528 table 1 normal penile anatomy on magnetic resonance imaging anatomical structures t2 signal intensity hyperintense skin hypointense dartos subepithelial connective tissue hyperintense colles and bucks fascia and tunica albuginea hypointense hyperintense corpus spongiosum or corpora cavernosa tabella 1 anatomia normale rm del pene strutture anatomiche intensit di segnale t2 cute dartos tessuto connettivo sottoepiteliale fascia di colles e buck e tunica albuginea corpo spongioso o corpi cavernosi iperintenso ipointenso iperintenso ipointenso iperintenso pear on axial t2 - weighted images as well - distinct concentric layers representing hyperintense skin , hypointense dartos , hyperintense subepithelial connective tissue , colles and buck fasciae and the tunica albuginea as a single hypointense rim , and hyperintense corpus spongiosum and corpus cavernosum ( table 1 )  . 
because neoplastic tissue has intermediate signal intensity on t2 - weighted images , it appears hypointense relative to the corpus spongiosum and cavernosum [ 9 , 11 ] and to the subepithelial connective tissue but hyperintense relative to the dartos and tunica albuginea . 
stage t1 tumours : invasion of the subepithelial connective tissue , which appears as a mass of relative hypointensity protruding into the ( hyperintense ) subepithelial connective tissue but not infiltrating the tunica albuginea , which preserves homogeneous thickness and signal intensity throughout its circumference , without frank interruptions 2 . 
stage t2 tumours : invasion of the tunica albuginea or corpus spongiosum or cavernosum , which is visualised as a mass causing a thinning or an interruption of the tunica albuginea circumference or as a mass of relative hypointensity protruding into the corpus spongiosum or cavernosum ( both hyperintense ) 3 . 
t4 tumours : invasion of adjacent anatomical structures , which appears as the loss of fat cleavage planes , associated with altered signal intensity or neoplastic strands within the invaded structure sualizzate nelle immagini assiali pesate in t2 come strati concentrici , ben distinti tra loro , che dallesterno allinterno si presentano : la cute iperintensa , il dartos ipointenso , il tessuto connettivo sottoepiteliale iperintenso , le fascia di buck e di colles e la tonaca albuginea come un unico anello ipointenso , i corpi spongioso e cavernoso iperintensi ( tabella 1 )  . dopodich , stata identificata la sede del tumore , che , caratterizzato da una intensit di segnale intermedia in t2 , risulta ipointenso rispetto ai corpi spongioso e cavernoso [ 9 , 11 ] e al tessuto connettivo sottoepiteliale , ma iperintenso rispetto al dartos e alla tonaca albuginea . 
linvasione di strutture anatomiche adiacenti , che si visualizza come la perdita dei piani adiposi di clivaggio , associata ad alterata intensit di segnale o gettoni neoplastici nel contesto della struttura invasa : tali tumori sono stadiati come t4 . 
 la scelta del trattamento stata effettuata sulla base della sede e dellestensione del tumore , definita dalla stadiazione della rm - tfi e dellesame clinico : i pazienti con tumore in stadio t1 sono stati sottoposti allablazione laser , mentre quelli tumore in stadio t2 o maggiore alla penectomia parziale o totale . 
la stadiazione locale di malattia eseguita con la rm - tfi stata confrontata con quella dellesame clinico e dellanatomia patologica . risultati lesame clinico stato concorde con lanatomia patolo gica in 8 casi su 13 : 5 pazienti in stadio t2 e 3 pazienti in stadio t1 . 
negli altri 5 casi , lesame clinico ha sovrastadiato la malattia in due pazienti ( un carcinoma in situ come t1 ed un t1 come un t2 ) e ha sottostadiato la malattia in tre pazienti ( due pazienti con tumore t2 come t1 e uno con tumore t3 come t2 ) ( tabella 3 )  . la rm - tfi stata eseguita con successo in tutti i pazienti , in dieci con unerezione ottimale , in tre con unere517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 521 radiol med ( 2008 ) 113 : 517528 table 2 magnetic resonance imaging semiological criteria for local staging of penile tumours in t2 sequences signal intensity relative signal intensity of tumour semiological criteria for invasion t stage subepithelial connective hyperintense tissue tunica albuginea hypointense corpus spongiosum or corpora cavernosa urethra or prostate hyperintense hyperintense hypointense hyperintense hypointense hypointense adjacent structures hypointense , hyperintense hypointense , hyperintense hypointense mass invading hyperintense tissue hyperintense mass interrupting hypointense rim hypointense mass invading hyperintense tissue hypointense mass invading hyperintense tissue loss of fat planes and neoplastic strands tabella 2 criteri semeiologici rm per la stadiazione locale del tumore del pene nelle sequenze pesate in t2 intensit segnale intensit di segnale relativa del tumore criteri semeiologici di invasione stadio t tessuto connettivo sottoepiteliale tunica albuginea corpo spongioso o cavernoso uretra o prostata iperintenso ipointenso iperintenso iperintenso ipointenso iperintenso ipointenso ipointenso strutture adiacenti iper - , ipointenso ipo - , iperintenso massa ipointensa invade tessuto iperintenso massa iperintensa interrompe anello ipointenso massa ipointensa invade tessuto iperintenso massa ipointensa invade tessuto iperintenso perdita piani di clivaggio e gettoni neoplastici treatment was determined by tumour site and extent as defined by mri - pipe and clinical staging . 
local staging of disease obtained with mri - pipe was compared with that of the clinical examination and pathological assessment . results clinical staging and pathological staging coincided in eight cases out of 13 : five patients with stage t2 disease and three with stage t1 disease . 
in the other five cases , the clinical examination overstaged the tumours in two patients ( one tis was staged as t1 and one t1 staged as t2 ) and understaged them in three ( two t2 staged as t1 and one t3 staged as t2 ) ( table 3 )  . mri - pipe was performed successfully in all patients . optimal erections were achieved in ten patients and suboptimal erections in three ; nonetheless the erections lasted until the end of the examination ( up to 30 min ) in all cases . one patient developed priapism secondary to the intracavernosal pge1 injection , which was resolved by aspiration of the corpora cavernosa ; no patient complained of pain or diszione subottimale ; in tutti i casi comunque lerezione durata fino al termine dellesame ( fino a 30 minuti )  . 
la rm - tfi ha correttamente stadiato 12 su 13 pazienti ; solo in un paziente ( con carcinoma in situ del solco coronale ) essa non stata in grado di riconoscere la presenza del tumore ( tabella 3 )  . il trattamento terapeutico stato adeguato per tutti i pazienti , come pianificato sulla base della valutazione collegiale dei reperti dellesame clinico e della rm - tfi : 6 pazienti ( 5 con carcinoma t1 e uno con carcinoma in situ ) sono stati sottoposti ad ablazione laser ; i rimanenti 7 pazienti hanno subito un intervento chirurgico convenzionale : penectomia parziale in sei pazienti ( cinque t2 e un t3 ) e penectomia totale nel paziente con sarcoma t2 dellasta del pene . 
laggiunta della rm - tfi nella stadiazione pre - operatoria ha cambiato la strategia terapeutica in tre pazienti : i pazienti 1 e 9 sarebbero stati sottotrattati con unablazione laser e il paziente 13 sarebbe stato sovratrattato con una penectomia parziale . i tumori del pene sono risultati 12 carcinomi squamocellulari e un sarcoma ; essi erano localizzati a livello del glande in sette pazienti , a livello del glande e del prepuzio in due , a livello del solco coronale in due e a livello dellasta del pene in un paziente ( sarcoma ) ( tabella 3 )  . 517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 522 table 3 site of penile cancer and t stage defined by both clinical examination and magnetic resonance imaging combined with pharmacologically induced penile erection compared with the final pathological stage obtained after surgery in the 13 patients in this series patient site t stage by clinical examination mr - pipe pathology surgery radiol med ( 2008 ) 113 : 517528 tabella 3 sede , stadio e tipo di chirurgia effettuata nei pazienti con tumore del pene . 
la tabella descrive la sede del tumore del pene , la stadiazione del t secondo lesame clinico , la rm - tfi , e la stadiazione definitiva dellanatomia patologica dopo chirurgia , nei 13 pazienti di questa casistica paziente sede stadio t esame clinico rm - tfi anatomia patologica chirurgia glans and prepuce glans shaft prepuce coronal sulcus coronal sulcus glans and prepuce glans glans prepuce glans glans coronal sulcus glande e prepuzio glande asta prepuzio solco coronale solco coronale glande e prepuzio glande glande prepuzio glande glande solco coronale partial penectomy laser ablation total penectomy partial penectomy partial penectomy laser ablation partial penectomy partial penectomy partial penectomy laser ablation laser ablation laser ablation laser ablation penectomia parziale ablazione laser penectomia totale penectomia parziale penectomia parziale ablazione laser penectomia parziale penectomia parziale penectomia parziale ablazione laser ablazione laser ablazione laser ablazione laser comfort during the examination . 
mri - pipe correctly staged 12 out of 13 patients ; in one patient only ( with carcinoma in situ of the coronal sulcus ) did it fail to detect the presence of the tumour ( table 3 )  . treatment planning , defined on the basis of the joint evaluation of the clinical examination and mri - pipe , proved adequate for all patients : six patients ( five with t1 and one with tis disease ) underwent laser ablation . 
the remaining seven patients underwent conventional surgery : partial penectomy in six patients ( five t2 and one t3 ) and total penectomy in the patient with t2 sarcoma of the penis shathe addition of mri - pipe to preoperative staging changed the treatment strategy in three patients : patients 1 and 9 would have been undertreated by laser ablation , and patient 13 would have been overtreated by partial penectomy . histologically , the penile cancers were 12 squamous cell carcinomas and one sarcoma . 
lesions involved the glans in seven patients , the glans and prepuce in two , the coronal discussione la scadente performance dimostrata dallesame clinico nei nostri pazienti ( solo 8 pazienti su 13 stadiati correttamente ) concorde con i dati della letteratura : solitamente lesame clinico sottostima lestensione del tumore del pene [ 5 ]  . 
solo uno studio descrive lesame clinico come una metodica affidabile nel determinare le dimensioni del tumore e linfiltrazione dei corpi cavernosi , ma raccomanda comunque luso dellimaging nei casi in cui linfiltrazione dei corpi cavernosi non possa essere determinata in modo appropriato con il solo esame obiettivo [ 12 ]  . 
i tumori non stadiati correttamente dallesame clinico erano localizzati a livello del glande ( due pazienti ) , a livello del glande e del prepuzio ( un paziente ) e a livello del solco coronale ( due pazienti )  . 
in accordo con quanto riportato in letteratura [ 5 ] , anche nella nostra coorte di paziente stata documentata una maggiore difficolt di stadiazione dei tumori del pene che interessano il glande con lesame clinico . 517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 523 radiol med ( 2008 ) 113 : 517528 sulcus in two and the shaft in one patient ( sarcoma ) ( table 3 )  . discussion the poor performance of the clinical examination in our series ( only eight out of 13 patients were staged correctly ) confirms previous reports that the clinical examination tends to underestimate the extent of penile cancer [ 5 ]  . 
only one study describes the clinical examination as a reliable method for determining tumour size and infiltration of the corpora cavernosa , even though it recommends the use of imaging in tumours for which the physical examination alone cannot properly determine infiltration of the corpora cavernosa [ 12 ]  . 
the tumours incorrectly staged by the clinical examination involved the glans ( two patients ) , the glans and prepuce ( one patient ) and the coronal sulcus ( two patients )  . 
in agreement with the literature [ 5 ] , we found that tumours involving the glans were more difficult to stage clinically . mri - pipe had better accuracy than the clinical examination in preoperative local staging , enabling correct staging of 12 out of 13 penile cancers . 
these results are in agreement with those of a recently published study [ 8 ] that reports a good correlation ( k = 0.75 , p < 0.001 ) between histological staging and staging by mri - pipe . 
 la rm - tfi ha dimostrato unaccuratezza migliore dellesame clinico nella stadiazione locale pre - operatoria dei tumori del pene , permettendo una stadiazione corretta in dodici pazienti su tredici . 
tali risultati sono in accordo con uno studio pubblicato di recente [ 8 ] , che riporta una buona correlazione ( k = 0 , 75 , p < 0 , 001 ) tra stadiazione istologica e radiologica con rm - tfi . 
 la sede della lesione non ha influenzato laccuratezza della rm - tfi nella stadiazione del tumore al pene , dal momento lunica lesione non correttamente stadiata era un carcinoma in situ del solco coronale , mentre le lesioni stadiate correttamente erano indifferentemente localizzate nel glande ( 5 pazienti ) , nel glande e nel prepuzio ( 2 pazienti ) , nel prepuzio ( 2 pazienti ) , nel solco coronale ( 2 pazienti ) e nellasta del pene ( un paziente )  . la somministrazione di mezzo di contrasto non ha migliorato la performance della rm - tfi nellunico paziente non correttamente stadiato ( con carcinoma in situ ) , n ha aggiunto informazioni rilevanti negli altri 12 pazienti correttamente stadiati . 
questo probabilmente dovuto alla mancanza nella nostra casistica di pazienti con tumore del pene in stadio t4 , per i quali il contrasto avrebbe potuto giocare un ruolo nel dimostrare linvasione delle strutture anatomiche adiacenti secondo la nostra opinione , la elevata accuratezza difig . 
c il paziente stato selezionato per una chirurgia conservativa ( ablazione laser ) , che risultata il trattamento pi adeguato , come confermato dallanatomia patologica ( stadio pt in situ )  . 517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 524 radiol med ( 2008 ) 113 : 517528 tumour location did not affect the accuracy of mripipe staging given that the only lesion staged incorrectly was a carcinoma in situ of the coronal sulcus . 
all correctly staged lesions involved the glans ( five cases ) , the glans and prepuce ( two cases ) , prepuce ( two cases ) , the coronal sulcus ( two cases ) and the shaft ( one case ) without distinction . administration of contrast material did not improve the performance of mri - pipe in the only patient staged incorrectly ( with carcinoma in situ ) , nor did it provide important additional information in the 12 patients correctly staged . 
this is probably due to the absence of patients with stage t4 disease , in whom contrast administration might help to demonstrate invasion of the adjacent anatomical structures . in our opinion , the high level of accuracy demonstrated by mri - pipe in our study is the result of the high - contrast resolution achieved between the hypointense tunica albuginea and markedly hyperintense corpora cavernosa and spongiosum in t2 during penile erection . 
conventional mri is reported to be limited in distinguishing penile cancers confined to the tunica albuginea mostrata dalla rm - tfi nel nostro studio merito dellelevata risoluzione di contrasto che stato possibile raggiungere tra tonaca albuginea ipointensa e corpi cavernosi e spongioso marcatamente iperintensi in t2 nel pene eretto . 
sono riportate limitazioni di questa tecnica nel distinguere i tumori del pene confinati alla tonaca albuginea ( stadio t1 ) da quelli che invadono il corpo spongioso o i corpi cavernosi ( stadio t2 ) [ 13 ]  . 
a sagittal t2 - weighted images demonstrate clear interruption of the hypointense rim of the tunica albuginea of the corpora cavernosa due to a bulky tumour of the glans ( relatively hyperintense mass )  . 
a le immagini sagittali pesate in t2 dimostrano una evidente interruzione del profilo della tunica albuginea ( ipointensa ) dei corpi cavernosi , da parte di un voluminoso tumore che interessa il glande ( massa di iperintensit di segnale relativa ) : tale reperto ha portato ad una stadiazione preoperatoria di tumore del pene in stadio t2 . 
le immagini di macroistologia dimostrano una corrispondenza con le immagini della rm - tfi . 517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 525 radiol med ( 2008 ) 113 : 517528 fig . 
a sagittal t2 - weighted images demonstrated a small interruption of the low - signal - intensity rim of the tunica albuginea ( arrows ) of corpora cavernosa , which indicates a stage t2 tumour . 
a le immagini sagittali pesate in t2 dimostrano una piccola interruzione dellanello ipointenso della tunica albuginea ( frecce ) dei corpi cavernosi , che indica uno stadio t2 del tumore . 
b nelle immagini sagittali pesate in t2 senza test di farmacoinfusione intracavernosa ( tfi ) linterruzione della tunica albuginea dei corpi cavernosi non facilmente identificabile , a causa della minore distensione e della minore risoluzione di contrasto tra lanello ipointenso della tunica albuginea e la iso - / ipointensit dei corpi cavernosi , rispetto alle immagini dopo lerezione indotta mediante iniezione intracavernosa di prostaglandine . ( stage t1 ) from those invading the corpus spongiosum or the corpora cavernosa ( stage t2 ) [ 13 ]  . 
had clinical staging alone been used to determine the choice of surgery , treatment would have remained unchanged for only two of the five patients with incorrect clinical staging : patient 6 ( overstaged as t1 ) would have undergone laser ablation in any case , even if he had been correctly staged as tis of the coronal sulcus , and patient 8 ( understaged as t2 ) would have been treated by partial penectomy even if he had been correctly staged as t3 carcinoma of the glans . 
clinical staging alone would have led to the undertreatment of two patients : patients 1 and 9 would have undergone laser ablation , as they had been clinically understaged as t1 , whereas mri - pipe demonstrated invasion of the corpus spongiosum dellesame clinico , non ci sarebbero stati cambiamenti solo in due dei cinque pazienti nei quali lesame clinico aveva fatto una stadiazione scorretta : il paziente 6 ( sovrastadiato come t1 ) sarebbe stato sottoposto ugualmente ad ablazione laser ed il paziente 8 ( sottostadiato come t2 ) avrebbe subito una penectomia parziale , anche se fossero stati correttamente stadiati , rispettivamente , come carcinoma in situ del solco coronale e come carcinoma del glande allo stadio t3 . 
due pazienti sarebbero stati sottotrattati sulla base del solo esame clinico : i pazienti 1 e 9 sarebbero stati sottoposti allablazione laser , dal momento che erano stati sottostadiati come t1 dallesame clinico , mentre la rm - tfi ha evidenziato linvasione del corpo spongioso ( stadio t2 ) e ha correttamente selezionato questi pazienti per una penectomia parziale . 
va sottolineato che la rmtfi ha permesso di evitare una chirurgia mutilante in que517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 526 radiol med ( 2008 ) 113 : 517528 fig . 
a axial t2 - weighted images demonstrated an intact tunica albuginea ( arrows ) , which indicates stage t1 tumour . b coronal t2 - weighted images confirmed the presence of an intact tunica albuginea ( black arrowheads ) , indicating stage t1 tumour of the coronal sulcus ( white arrow )  . 
b le immagini coronali pesate in t2 confermano la presenza di una tunica albuginea integra , ( punte di freccia nere ) , indicativa di un tumore del solco coronale ( freccia bianca ) in stadio t1 . 
c il paziente stato correttamente selezionato per una chirurgia conservativa ( ablazione laser ) , come confermato dallanatomia patologica ( stadio pt1 )  . ( stage t2 ) and correctly selected these patients for partial penectomy . 
the role of mri - pipe proved especially important for evaluating the tunica albuginea ; a finding of an intact tunica albuginea at preoperative staging justifies conservative surgery , such as laser ablation . 
in our series , we identified no distinctive features of squamous cell carcinomas and sarcoma , either on clinical examination or at mri - pipe . there are some limitations to our study . 
the accuracy of mri - pipe was not compared with that of conventional mri , nor could the literature data be used as a basis for sto paziente , che ha invece potuto beneficiare di un intervento conservativo , con eccellenti risultati funzionali ed estetici . 
il ruolo della rm - tfi , in particolare , stato cruciale nella valutazione della tonaca albuginea , la cui integrit dimostrata nella stadiazione pre - operatoria consente il ricorso ad una chirurgia conservativa , come lablazione laser . 
nella nostra casistica non sono state trovate caratteristiche differenti , n nellesame clinico n nella rm - tfi tra i carcinomi squamocellulari e il sarcoma . il nostro studio ha alcuni limiti . 
laccuratezza della rmtfi non stata confrontata con quella dellesame rm convenzionale , n stato possibile utilizzare come confronto i dati riportati in letteratura , per il numero ridotto di studi pubblicati . 
ulteriori studi possibilmente multicentrici , con un numero pi elevato di pazienti , dovrebbero paragonare queste due tecniche desame , al fine di quantificare il reale vantaggio ottenuto con lerezione peniena , che pu comportare complicanze , come descritto in un paziente della nostra casistica , che ha sviluppato priapismo . 
questa non pu essere considerata una complicanza minore , poich ha 517 - 528 rame254_petralia 9 - 07 - 2008 16 : 40 pagina 527 radiol med ( 2008 ) 113 : 517528 comparison given the small number of studies published on the subject . 
further , possibly multicentric studies on larger patient populations should compare these two examination techniques to quantify the true gain of imaging with artificial erection , given that this can cause priapism , as seen in one of our patients . 
priapism cannot be regarded as a minor complication , as it requires additional treatment and causes the patient considerable discomfort ; we recommend that outpatients be observed until the erection has subsided . 
in contrast , the remaining 12 patients tolerated the pharmacologically induced erection well , with none reporting discomfort . erection was suboptimal in only three out of 13 patients ; however , this did not affect the accuracy of mri - pipe , as the t2 hyperintensities and tunica albuginea distension were in any case greater than achievable in an examination with the penis in flaccid state . 
the use of a stronger magnet ( 1.5 t or even greater ) than used in our study ( 1 t ) could theoretically improve the results thanks to better spatial and contrast resolution ; however , field strength has been shown to have no influence on the techniques diagnostic accuracy [ 6 ]  . we were unable to compare the results of mri - pipe with those of ultrasound performed with high frequency linear - array probes , which afford excellent spatial resolution [ 14 ] , even higher than that of mri . 
 conclusions in conclusion , although mri - pipe has no role in the diagnosis of penile cancers , which is established by the clinical examination , it does have good potential in local staging and may lead to major changes in treatment planning if correctly performed and interpreted . 
the accuracy of the examinations performed in our series indicates that good results can be achieved , and time can be saved , by acquiring only t2 - weighted sequences in the sagittal , para - axial and paracoronal planes , reserving the preand postcontrast t1 - weighted sequences for staging tumours invading the adjacent anatomical structures ( t4 )  . 
al contrario , i rimanenti 12 pazienti hanno accettato di buon grado la procedura dellerezione farmacoindotta , senza riferire alcun fastidio . solo in tre dei tredici pazienti si ottenuta unerezione subottimale ; tuttavia questo non ha influenzato laccuratezza della rm - tfi , perch sono state comunque raggiunte maggiori iperintensit nelle immagini t2 pesate e distensione della tonaca albuginea , rispetto a quelle di un esame condotto con pene flaccido . 
lutilizzo di un magnete di maggior intensit ( 1 , 5 t o ancora maggiore ) , rispetto a quello utilizzato nel nostro studio ( 1 t ) , in teoria , potrebbe migliorare i risultati della nostra esperienza , per la migliore risoluzione di spaziale e di contrasto ; tuttavia , uno studio ha dimostrato come lintensit del campo non influenzi laccuratezza diagnostica dellesame [ 6 ]  . non stato possibile comparare i risultati della rm - tfi con quelli della ecografia eseguita con sonde lineari a elevata frequenza , le quali permettono una eccellente risoluzione spaziale [ 14 ] , superiore a quella della rm ; lo sviluppo di tali sonde ha consentito alla ecografia di avere potenzialit paragonabili a quelle della rm nella stadiazione locale dei tumori del pene [ 7 ]  . 
 conclusioni in conclusione , rm - tfi non riveste alcun ruolo nella diagnosi dei tumori del pene , la quale gi clinica , ma dimostra un elevato potenziale nella stadiazione locale e pu determinare importanti cambiamenti nella pianificazione della terapia , se correttamente eseguita e interpretata . 
per limitare il tempo - macchina a circa 30 minuti , necessario premedicare con pge1 il paziente con adeguato anticipo ( 2030 minuti ) ; sulla base della valutazione dellaccuratezza degli esami eseguiti nella nostra casistica , riteniamo che risultati ottimali possano essere ottenuti gi con la sola esecuzione di sequenze pesate in t2 secondo i piani sagittale , para - assiale e para - coronale , con un conseguente significativo risparmio di tempo , riservando lesecuzione di sequenze pesate in t1 prima e dopo la somministrazione di mezzo di contrasto solo per la stadiazione di tumori che invadono le strutture anatomiche adiacenti ( t4 )  . 
this study was done to evaluate the midand long - term patency rates of complete ( from the origin to hunters duct ) chronic occlusions of the superficial femoral artery ( sfa ) treated by angioplasty and / or stenting . 
from february 2002 to march 2005 , 21 patients with complete occlusion of the sfa and good distal runoff ( two or three patent vessels ) were treated with endovascular recanalisation . 
in all cases , recanalisation was performed with a contralateral approach by percutaneous transluminal angioplasty ( pta ) , with stenting only when pta provided unsatisfactory results ( due to elastic recoil and complications such as dissection )  . in the case of calcified occlusions and when the true lumen of the sfa could not be crossed , subintimal angioplasty was performed . 
lo studio include 21 pazienti con occlusione completa dellafs e buon run - off distale ( 2 o 3 vasi pervi ) sottoposti a ricanalizzazione endovascolare nel periodo compreso tra febbraio 2002 e marzo 2005 . 
in tutti questi casi la ricanalizzazione stata effettuata con approccio controlaterale cross - over mediante angioplastica transluminale ( pta ) e stenting solo nelle evenienze in cui la pta ha fornito risultati insoddisfacenti , per ritorno elastico di parete ( recoil ) e complicanze tipo dissezione ; nelle occlusioni in prevalenza calcifiche e nei casi in cui non si guadagnato il lume vero dellafs , stata utilizzata la tecnica di angioplastica subintimale . 
il tasso di perviet primaria a 6 , 12 , 24 , 32 e 44 mesi stato , rispettivamente , del 93 , 3% , 69 , 2% , 72 , 7% , 62 , 5% e 40% ; il tasso di perviet secondaria a 6 , 12 e 24 mesi del 100% , 84 , 6% e 81 , 8% . 568 radiol med ( 2008 ) 113 : 567577 occlusions of the sfa showed good midand long - term primary patency rates , with few periprocedural complications . 
la ricanalizzazione percutanea delle occlusioni croniche complete dellafs , nella nostra serie , ha mostrato buoni tassi di perviet primaria e secondaria a medio e lungo termine con un basso tasso di complicanze periprocedurali ; le ri - occlusioni possono essere trattate con tecnica percutanea , che garantisce un soddisfacente tasso di perviet secondaria . parole chiave arteria femorale superficiale occlusione angioplastica stent introduction introduzione arterial insufficiency of the lower extremities is a very common disorder that affects 20% of the population older than 75 years of age . 
the main cause of peripheral arterial occlusive disease is atherosclerotic disease , with lesions located in the femoropopliteal segment in more than half of cases . chronic occlusion of the superficial femoral artery ( sfa ) causes claudication and may lead to chronic critical limb ischaemia [ 1 ]  . 
in view of the high morbidity and mortality of peripheral arterial disease , different treatment options have been proposed , including femoropopliteal bypass surgery , combined thromboendarterectomy techniques using wollmar ring strippers with optional stenting [ 2 , 3 ] and percutaneous revascularisation . 
whereas in the past it was used to treat only short stenoses and occlusions , nowadays , longer lesions are also eligible for treatment [ 4 ]  . this study evaluated the midand long - term patency rates of percutaneous recanalisation of complete chronic occlusions of the sfa , extending from the origin to hunters canal , for which surgical treatment is usually indicated [ 5 ]  . 
in considerazione degli elevati tassi di morbidit e mortalit correlati a questa patologia , sono state proposte differenti opzioni terapeutiche , rappresentate dagli interventi chirurgici di by - pass femoro - popliteo , dalle tecniche combinate di tromboendoarteriectomia mediante anelli di wollmar associate o meno allo stenting [ 2 , 3 ] e dalla rivascolarizzazione percutanea . 
questultima , grazie anche ai vantaggi della minore invasivit e morbilit , ha ampliato le proprie indicazioni : infatti , mentre in passato venivano sottoposte a questa procedura solo steno - occlusioni brevi , attualmente sono suscettibili di trattamento anche lesioni ostruttive pi estese in lunghezza [ 4 ]  . questo studio si propone di valutare la perviet a medio e lungo termine della ricanalizzazione mediante tecnica percutanea delle occlusioni croniche complete dellafs , estese dallorigine sino al canale di hunter , che usualmente costituiscono indicazione chirurgica [ 5 ]  . 
 between february 2002 and march 2005 , 33 patients ( 22 men and 11 women ; mean age 73.6 years ; range 5885 years ) with complete chronic occlusion of the sfa ( from origin to hunters canal ) were treated with percutaneous transluminal angioplasty ( pta ) or pta and stenting . 
inclusion criteria were complete sfa occlusion , patency of the popliteal artery and at least two lowermateriali e metodi da febbraio 2002 a marzo 2005 sono stati sottoposti a pta o pta e stenting 33 pazienti ( 22 maschi e 11 femmine ; et media 73 , 6 anni ; range da 58 a 85 anni ) , tutti con occlusione cronica completa dellafs ( dallorigine sino al canale di hunter ) ; di questi 33 pazienti vengono presi in considerazione i 21 che presentavano run - off distale con due o tre vasi pervi . 
sono stati quindi esclusi dallo studio 12 pazienti con scarso run - off periferico ( definito come locclusione o la stenosi emodinamicamente significativa di almeno due vasi tibioperoneali ) [ 6 ] ; i criteri di inclusione sono stati pertanto : radiol med ( 2008 ) 113 : 567577 limb arteries . 
all patients were symptomatic and had severe claudication ( rutherford stage iii ) or critical limb ischaemia ( rutherford stages ivvi )  . contralateral access with the crossover technique was used in all patients to reduce the risk of retroperitoneal bleeding ( more common with the antegrade approach in the case of high femoral artery bifurcation ) , to better assess the femoral artery bifurcation and to avoid postinterventional compression of the puncture site on the treated side and thus reduce the risk of acute sfa occlusion . 
the crossover technique involved retrograde access of the contralateral common femoral artery and placement of a 5 - f valved introducer sheath ( terumo , tokyo , japan ) and a 5 - f hook simmons 1 catheter ( cordis , warren , nj , usa )  . 
the lumen of the contralateral external iliac artery was reached with a 0.035hydrophilic guidewire ( terumo , tokyo , japan ) , which was then exchanged for a superstiff guidewire ( amplatz , boston scientific , natick , ma , usa )  . 
the catheter and introducer were then removed , and a 6 - f 45 - cm - long introducer sheath ( cordis , warren , nj , usa ) was positioned . the occlusion was crossed with a straight or angled hydrophilic guidewire ( glidewire terumo , tokyo , japan ) and 5 - f straight or vertebral catheter ( cordis , miami , fl , usa )  . recanalisation was achieved by pta with 6 mm10 cm balloons ( cordis , warren , nj , usa )  . 
this involved placing a 45 - cm - long 6 - f introducer sheath ( cordis , warren , nj , usa ) with the distal tip just above the femoral bifurcation and traversing the length of the occlusion through the subintimal space until the true lumen was re - entered in the popliteal artery , generally above the knee joint , with a 5 - f vertebral catheter ( cordis , warren , nj , usa ) and 0.035 - hydrophilic guidewire ( terumo , tokyo , japan )  . 
in the remaining 12 cases , unsatisfactory results due to elastic recoil with > 30% residual stenosis or complications such as dissection with flow - limiting flap called for repeat angioplasty with the balloon inflated at low pressure to secure the dissection flap , followed by stenting . 
in cases of calcified occlusion , we employed a nitinol stent having high radial force and open - cell design ( luminexx - bard , karlsruhe , germany ) , 6 or 7 mm in diameter , 10 or 12 cm in occlusione completa dellafs , perviet dellarteria poplitea e di almeno due arterie di gamba . 
tre pazienti , inoltre , presentavano anche il coinvolgimento dellasse iliaco : in tutti e tre i casi si trattava di occlusioni dellarteria iliaca esterna . tutti i pazienti erano sintomatici con claudicatio severa ( stadio iii della classificazione di rutheford ) o ischemia critica ( stadi iv - vi della classificazione di rutheford )  . in tutti i pazienti stato effettuato un approccio controlaterale con tecnica cross - over per ridurre il rischio di ematoma retroperitoneale ( pi frequentemente correlato alla puntura anterograda in caso di biforcazione femorale alta ) , per una migliore valutazione della biforcazione femorale e per evitare , al termine della procedura , la compressione nel sito di puntura in corrispondenza del lato trattato , riducendo cos il rischio di occlusione acuta dellafs . 
il cross - over stato effettuato mediante puntura retrograda dellarteria femorale comune controlaterale ove stato posizionato introduttore valvolato da 5f ( terumo , tokyo , giappone ) e mediante lutilizzo di catetere tipo hook o tipo simmons 1 da 5 f ( cordis , warren , nj , usa ) ; guadagnato il lume dellarteria iliaca esterna controlaterale con guida idrofilica 0 , 035 ( terumo , tokyo , giappone ) , si sostituita la guida stessa con guida super - stiff ( amplatz , boston scientific , natick , ma , usa ) e , rimossi il catetere e lintroduttore , si posizionato introduttore lungo 45 cm da 6f ( cordis , warren , nj , usa )  . 
locclusione stata valicata mediante supporto di guida idrofilica rigida retta od angolata ( glidewire terumo , tokyo , giappone ) e catetere retto o vertebrale 5f ( cordis , miami , fl , usa )  . 
la ricanalizzazione stata effettuata mediante angioplastica transluminale ( pta ) con cateteri forniti di pallone dilatatore del calibro di 6 mm e della lunghezza di 10 cm ( cordis , warren , nj , usa ) ; nelle complicanze o nel risultato insoddisfacente della pta stata posta lindicazione allo stenting . 
nelle occlusioni in prevalenza calcifiche , e nei casi in cui non si guadagnato il lume vero dellafs , stata utilizzata la tecnica di pta subintimale ( 7 casi )  . 
la tecnica prevede il posizionamento di un introduttore del calibro di 6f lungo 45 cm ( cordis , warren , nj , usa ) con estremo distale in prossimit della biforcazione femorale ; quindi , mediante il supporto di catetere di tipo vertebrale da 5f ( cordis , warren , nj , usa ) e guida idrofilica 0 , 035 ( terumo , tokyo , giappone ) , locclusione stata valicata sino al rientro nel lume vero in arteria poplitea , generalmente in sede sovra - articolare . 
 in 9 casi la pta stata sufficiente alla ricanalizzazione del vaso ; nei rimanenti 12 casi il risultato insoddisfacente , con ritorno elastico di parete ( recoil ) condizionante stenosi residua superiore al 30% , e complicanze tipo dissezione con flap stenosante o occludente hanno imposto lutilizzo dello stent , previa esecuzione di una seconda angioplastica con dilatazione del palloncino a bassa pressione per tentare di riaccollare il flap . 
to avoid plaque protrusion in noncalcified occlusions , we preferred to use an 8 mm8 cm closed - cell metal alloy stent ( wallstent - boston scientific , natick , ma , usa ) ; when dilated to 6 mm , the stent covers 10 cm of artery , thanks to its elasticity and flexibility . 
five patients were treated with one stent only , five with two stents and two with three stents . patients treated with pta and stenting received the following postprocedural medical treatment : heparin for 48 h ( 5 , 000 iu in 250 ml saline solution at a flow rate of 20 ml / h ) ; an anticoagulation dose of fraxiparin for 30 days , followed by double antiaggregant therapy ( clopidogrel + low - dose aspirin )  . 
the three external iliac artery occlusions were treated by pta with a 7 mm10 cm balloon in one case and by pta ( 7 mm10 cm balloon ) and stenting ( 10 mm6 cm ; smart , cordis , miami , fl , usa ) in the other two cases . 
in 5 pazienti stato utilizzato solo uno stent , in 5 pazienti sono stati impiegati 2 stents e in 2 pazienti sono stati utilizzati 3 stents . nei casi di pta e stenting stata suggerita la seguente terapia medica post - trattamento : eparina per 48 h ( 5000 ui in 250 ml di fisiologica a 20 ml / h ) ; fraxiparina a dose scoagulante per 30 giorni , poi doppio antiaggregante ( clopidogrel + cardioaspirina )  . 
le 3 occlusioni dellarteria iliaca esterna sono state trattate in un caso mediante pta con pallone del calibro di 7 mm e lunghezza di 10 cm , in due casi mediante pta ( pallone 7 mm10 cm ) e stenting ( 10 mm6 cm ; smart , cordis , miami , fl , usa )  . 
 il follow - up stato condotto mediante valutazione clinica ed eco - color doppler a 6 e 12 mesi , e successivamente annualmente ( range da 6 a 55 mesi , valore medio : 23 mesi )  . 
al follow - up a 12 mesi ( range da 9 a 15 mesi , valore medio : 12 , 2 mesi ) , disponibile per 13 pazienti , sono state riscontrate 4 occlusioni : 1 paziente ha subito lampuradiol med ( 2008 ) 113 : 567577 fig . 
1a - e preprocedural angiography : complete occlusion of the left superficial femoral artery ( sfa ) from the origin ( a ) , with recanalisation at the level of the femoropopliteal junction through collateral vessels ( b )  . 
1a - e angiografia pre - procedura : occlusione completa dellarteria femorale superficiale ( afs ) sinistra dallorigine ( a ) con ricanalizzazione del passaggio femoro - popliteo tramite circoli collaterali ( b )  . 
of the two stent occlusions that developed at 14 and 15 months , one was recanalised by cutting balloon and in - stent stenting because of associated tazione dellarto ( dopo 12 mesi ) , 1 stata convertita in bypass femoro - popliteo ( 9 mesi dopo il trattamento ) ; le 2 occlusioni di stent , verificatesi rispettivamente dopo 14 e 15 mesi dal trattamento , sono state ricanalizzate luna tramite cutting balloon e stenting in stent in quanto associata a frattura di stent , laltra mediante trombectomia meccanica ( rotarex , straub medical ag , wangs , svizzera ) e pta . 
2a - f preprocedural angiography : complete occlusion of the left superficial femoral artery ( sfa ) from the origin ( a ) , with recanalisation at the level of the femoropopliteal junction through collateral vessels ( b )  . percutaneous transluminal angioplasty ( pta ) of the sfa with 6 - mm10 - cm balloon ( c )  . 
post - pta angiography : recanalisation of the sfa ( d ) with dissection flap just beyond its origin , better depicted in the detail enlargement ( arrow ) ( e )  . 
2a - f angiografia pre - procedura : occlusione completa dellarteria femorale superficiale ( afs ) sinistra dallorigine ( a ) con ricanalizzazione del passaggio femoro - popliteo tramite circoli collaterali ( b )  . 
angiografia post - pta : ricanalizzazione dellafs ( d ) con flap di dissezione a valle dellorigine dellafs , meglio evidente nellimmagine di particolare ingrandita ( freccia ) ( e )  . 
angiografia dopo posizionamento di stent in nitinol di 7 mm di calibro e 12 cm di lunghezza , al terzo prossimale dellafs : completa ricanalizzazione dellafs ( f )  . stent fracture , and the other by mechanical thrombectomy ( rotarex , straub medical ag , wangs , switzerland ) and pta . 
thus , the primary patency rate at 1 year was 69.2% ( 9 / 13 patients ) , whereas the secondary patency rate was 84.6% ( 11 / 13 patients )  . 
nove pazienti hanno effettuato il follow - up a 24 mesi ( range da 18 a 26 mesi , valore medio : 24 mesi ) : in 1 caso stata riscontrata locclusione dellafs , trattata mediante pta intra - stent ; il tasso di perradiol med ( 2008 ) 113 : 567577 table 1 follow - up : primary and secondary patency rates no . 
the 24 - month primary patency rate was therefore 72.7% ( 8 / 11 patients , including the two cases of failure at 12 months ) , and the secondary patency rate was 81.8% ( 9 / 11 patients )  . 
in five cases , the sfa was patent , whereas in one case , the artery had reoccluded ( at 31 months , subsequently converted to femoropopliteal bypass grafting )  . 
the sfa was patent in both cases , leading to a primary patency rate of 40% ( 2 / 5 patients including the previous failures )  . discussion the treatment of choice for complete sfa occlusions is surgery with femoropopliteal bypass grafting [ 7 ]  . 
endovascular treatment may be conducted via a contralateral approach with the crossover technique in order to prevent retroperitoneal bleeding , more common with antegrade access in cases of high femoral - artery bifurcation , to achieve better control of the femoral bifurcation and to viet primaria a 24 mesi , pertanto , del 72 , 7% ( 8 / 11 pazienti , inclusi i due casi di insuccesso a 12 mesi ) ; il tasso di perviet secondaria dell81 , 8% ( 9 / 11 pazienti )  . 
sei pazienti hanno effettuato il follow - up a 32 mesi ( range da 28 a 36 mesi , valore medio : 32 mesi ) ; in 5 casi lafs risultata pervia ; in 1 caso stata riscontrata la ri - occlusione del vaso arterioso ( a 31 mesi , poi convertita in by - pass femoropopliteo )  . 
per 2 pazienti disponibile il follow - up oltre 32 mesi ( range da 40 a 55 mesi , valore medio : 44 mesi ) : in entrambi i casi lafs risultata pervia , con un tasso di perviet primaria del 40% ( 2 / 5 pazienti , includendo gli insuccessi precedenti )  . 
il trattamento endovascolare unalternativa che presenta il vantaggio della minore invasivit ; inoltre non preclude la terapia chirurgica , che pu essere dilazionata [ 8 ]  . il trattamento endovascolare pu essere effettuato mediante approccio controlaterale con tecnica cross - over per ovviare allematoma retroperitoneale , pi frequentemente correlato alla puntura arteriosa anterograda nei casi di biforcazione femorale alta , per ottenere un miglior controllo della biforcazione femorale e per evitare , al termine della procedura , la compressione in corrispondenza del sito di puntura , che potrebbe causare locclusione acuta dellafs trattata . 
nei casi in cui la guida guadagni il lume vero dellafs e dellarteria poplitea , si procede alla ricanalizzazione mediante pta , che viene integrata dallo stenting , qualora il ri574 radiol med ( 2008 ) 113 : 567577 fig . 
3a - d preprocedural angiography : reocclusion of the left superficial femoral artery ( sfa ) from the origin , 15 months after treatment [ percutaneous transluminal angioplasty ( pta ) plus stenting ] with recanalisation of the popliteal artery through collateral vessels ( a )  . 
3a - d angiografia pre - procedura : ri - occlusione dellafs sinistra dallorigine , a 15 mesi dal trattamento ( pta e stenting ) con ricanalizzazione dellarteria poplitea tramite circoli collaterali ( a )  . 
where the true lumen of the sfa and popliteal artery is accessible to the guidewire , pta recanalisation is performed , with optional stenting if the pta results are haemodynamically inadequate [ 7 , 9 ]  . 
where the guidewire fails to reach the true lumen , subintimal pta can be used [ 10 ] ; however , this technique produces a narrowed recanalisation lumen due to elastic recoil and flow - limiting spiral dissection flap , which requires stenting . several studies have evaluated the treatment of sfa stenoses and occlusions with a mean lesion length of 16 cm [ 4 , 8 , 10 , 1123 ] , reporting mean primary patency rates at 6 , sultato emodinamico della pta non sia adeguato [ 7 , 9 ]  . 
nei casi in cui la guida non abbia guadagnato il lume vero , si utilizza la tecnica di pta subintimale [ 10 ] ; tale procedura tuttavia , realizza un lume ridotto di ricanalizzazione , per il ritorno elastico e il flap di dissezione spiroide , talvolta stenosante o occludente , che impone lo stenting . in letteratura esistono diversi studi che riguardano il trattamento delle steno - occlusioni dellafs , con una lunghezza media delle lesioni di 16 cm [ 4 , 8 , 10 , 1123 ] , e con tassi di perviet primaria a 6 , 12 e 24 mesi in media del 71% ( range : 48%97% ) , 51 , 8% ( range : 22%86% ) e del 57% ( range : 36%84% )  . 
in alcuni casi stata utilizzata solo la tecnica di pta [ 8 , 1518 , 20 ] con un tasso radiol med ( 2008 ) 113 : 567577 12 and 24 months of 71% ( range 48%97% ) , 51.8% ( range 22%86% ) and 57% ( range 36%84% ) , respectively . 
in other cases , stenting was added to pta [ 4 , 10 , 1114 , 19 , 2123 ] , reaching a mean 12 - month primary patency rate of 55% . 
the follow - up period in these studies , no longer than 12 months , demonstrated primary patency rates of 49%50% and 22%35% at 6 and 12 months , respectively . 
our study reported better results , with primary patency rates of 93.3% ( 14 / 15 patients ) at 6 months and 69.2% ( 9 / 13 patients ) at 12 months . 
the follow - up period was longer , even though with a small number of patients . primary patency rate was 72.7% ( 8 / 11 patients ) at 24 months , 62.5% ( 5 / 8 patients ) at 32 months and 40% ( 2 / 5 patients ) beyond 32 months . 
the secondary patency rate was 100% ( 15 / 15 patients ) at 6 months , 84.6% ( 11 / 13 patients ) at 12 months , and 81.8% ( 9 / 11 patients ) at 24 months . 
it is important to emphasise that in cases of failure of the percutaneous techniques , we were nonetheless able to perform femoropopliteal bypass surgery ( in two patients ) ; only one case had to undergo an amputation . 
 our results with percutaneous revascularisation techniques are very similar to those reported for femoropopliteal bypass surgery , with a 1 - year primary patency rate of 68% [ 24 ]  . 
moreover , percutaneous recanalisation is associated with less morbidity in terms of both number and severity of complications , and may represent a valuable alternative for patients at high surgical risk [ 8 ]  . 
we recorded none of the other complications reported in the literature , and in particular , thanks to the use of the crossover technique , no cases of retroperitoneal bleeding . 
in altri casi , alla pta stato aggiunto luso dello stenting [ 4 , 10 , 1114 , 19 , 2123 ] ; stato cos ottenuto un tasso di perviet primaria a 12 mesi in media del 55% . 
le complicanze riscontrate sono state : lembolia distale ( 2%5 , 4% ) , lematoma nel sito di puntura ( 2%14% ) , lo pseudoaneuriil sanguinamento retroperitoneale sma ( 1 , 6%4 , 5% ) , ( 1 , 6%13% ) e la perforazione arteriosa ( 1%6 , 7% )  . delle serie rammentate , che hanno impiegato la pta associata eventualmente a stenting , solo due riportano anche casi di occlusioni complete dellafs [ 10 , 19 ] ( mentre nellesperienza personale tutti i pazienti erano affetti da lesioni occludenti a carico di tutto lasse femorale ) ; tali studi dispongono di un follow - up condotto non oltre 12 mesi e mostrano tassi di perviet primaria a 6 e a 12 mesi rispettivamente del 49%50% e 22%35% . 
opportuno sottolineare che , in caso di insuccesso delle procedure percutanee , stato comunque possibile effettuare lintervento chirurgico di by - pass femoro - popliteo ( in 2 pazienti ) ; solo uno , invece , stato il caso esitato in amputazione . 
 i risultati da noi riportati impiegando le tecniche di rivascolarizzazione percutanea sono sovrapponibili a quelli ottenuti con lintervento di by - pass femoro - popliteo il cui tasso di perviet primaria a 1 anno pari al 68% [ 24 ] ; inoltre la ricanalizzazione percutanea si associa ad una minore morbilit , per quanto riguarda sia il numero che la gravit delle complicanze , e pu essere una valida alternativa per i pazienti che presentano un alto rischio chirurgico [ 8 ]  . 
le complicanze correlate al trattamento sono state solo le embolie distali ( 2 / 21 , pari al 9 , 5% ) , trattate con successo mediante trombolisi loco - regionale ; peraltro non si sono osservate le altre complicanze riportate in letteratura , in particolar modo , non si sono osservati casi di sanguinamento retroperitoneale grazie allimpiego della tecnica crossover . 
la pi alta incidenza di embolia distale osservata nella nostra casistica correlabile alla maggior indaginosit della procedura di ricanalizzazione , collegata alla maggior estensione in lunghezza delle lesioni , rispetto ai casi riportati in letteratura . negli ultimi anni due contributi hanno valutato la possibilit di trattare le occlusioni dellarteria femorale superficiale ( con una lunghezza media delle lesioni di 12 , 2 e 6 , 9 cm rispettivamente ) tramite direct stentingcon stent in nitinol [ 25 , 26 ] : il follow - up disponibile fino a 24 mesi , con un tasso di perviet primaria a 12 mesi del 76%84% e a 24 576 radiol med ( 2008 ) 113 : 567577 follow - up lasted 24 months , with a primary patency rate of 76%84% at 12 months and of 60%84% at 24 months . this technique avoids the trauma of predilatation and thus reduces myointimal proliferation , a cause of delayed restenosis . 
moreover , our study demonstrated that in complete sfa occlusions , pta alone was often inadequate to ensure patency , and in > 50% ( 12 / 21 ) of cases , it had to be combined with the placement of one or more stents owing to elastic recoil with > 30% residual stenosis and flow - limiting spiral dissection . 
moreover , in the treatment of complete chronic occlusions of the sfa , it remains to be demonstrated that direct stenting is superior to the more commonly used techniques of predilatation or pta catheter dilatation followed by secondary stenting in the case of inadequate angioplasty results only . 
lo studio randomizzato di schillinger , condotto su pazienti con claudicatio severa e ischemia critica dovuta a stenosi o occlusione dellafs , ha confermato la superiorit del primary stenting con stent in nitinol nei confronti della pta eventualmente associata a stenting [ 27 ]  . conclusioni in base allesperienza personale , la ricanalizzazione percutanea delle occlusioni croniche complete dellarteria femorale superficiale con pta eventualmente associata a stenting fattibile nella maggior parte dei casi , con tassi soddisfacenti di perviet primaria a medio e lungo termine e un basso tasso di complicanze periprocedurali ; i buoni risultati ottenuti sono senzaltro correlati ad unaccurata selezione dei pazienti , con particolare attenzione alle condizioni dei vasi di out - flow . 
lo studio ha inoltre evidenziato che spesso la pta da sola , in caso di occlusioni complete dellafs , non sufficiente a garantire la perviet del vaso trattato e in pi del 50% ( 12 / 21 ) dei casi stata associata , per il ritorno elastico di parete , condizionante stenosi residua superiore al 30% , e per la presenza di complicanze tipo dissezione con flap spiroide stenosante od occludente , al posizionamento di uno o pi stent . 
 sono peraltro necessari , per validare la metodica endovascolare percutanea , studi basati su casistiche numericamente pi consistenti e con un follow - up pi protratto nel tempo ; inoltre va dimostrata , nel trattamento delle occlusioni croniche complete dellafs , la superiorit della tecnica di direct stenting nei confronti di quelle , sinora pi spesso impiegate , di predilatazione o dilatazione con catetere da pta seguite da stenting solo nei casi di insoddisfacente risultato dellangioplastica ( secondary stenting )  . 
we studied both wrists in 18 healthy volunteers ( ten men , eight women , age range 1858 years , mean age 34 years ) with a philips iu22 us scanner equipped with a high - resolution linear - array broadband transducer ( 517 mhz )  . 
abbiamo studiato entrambi i polsi di 18 soggetti volontari sani ( 10 maschi , 8 femmine , range 1858 anni , et media 34 anni ) mediante un apparecchio philips iu22 con trasduttore lineare ad alta risoluzione ( 517 mhz )  . 
lecografia ad alta risoluzione ci permette di studiare i legamenti estrinseci del carpo con un buon dettaglio anatomico ma il ruolo dellecografia nelliter terapeutico delle patologie da instabilit del carpo rimane da dimostrare . radiol med ( 2008 ) 113 : 504516 keywords us wrist carpal joint ligaments anatomy parole chiave ecografia polso carpo legamenti anatomia introduction introduzione chronic wrist pain is a common clinical query in referrals for musculoskeletal disorders . 
in this type of instability , there may be pathological involvement of many of the anatomical structures of the wrist [ triangular fibrocartilage complex ( tfc ) , intrinsic and extrinsic ligaments , muscles , and tendons ] , but in most cases , the symptoms are related to traumatic involvement of the extrinsic ligaments [ 2 , 3 ]  . 
the function of the palmar and dorsal ulnotriquetral ligaments and of the ulnolunate is to stabilise the distal radioulnar joint during wrist pronosupination and to prevent ulnar dislocation of the wrist bones . 
furthermore , these ligaments , along with other components of the triangular fibrocartilage ( tfc ) and the remaining ligaments of the radiocarpal joint , prevent ulnar dislocation of the ends of the carpal bone [ 4 , 5 ]  . 
therefore , knowledge of the anatomy of the carpus and in particular of the extrinsic ligaments is extremely important . the introduction into clinical practice of sonographic equipment with high - resolution transducers , together with the development of new , increasingly sophisticated postprocessing algorithms to optimise image resolution , has led to an increased use of high - resolution ultrasound ( hrus ) in the study of small joints . 
 the purpose of this study was to elucidate the potential of hrus in the study of extrinsic carpal ligaments and describe the imaging technique adopted and the sonographic appearance of the ligaments and their course using magnetic resonance ( mr ) arthrography as a reference standard . materials and methods we examined a group of 18 asymptomatic healthy volunteers with no history of wrist trauma . 
the group comprised ten men and eight women ( mean age 34 years , range 1858 ) referred for musculoskeletal disorders not involving the wrist and enrolled in the study after providing explicit written informed consent . 
two radiologists with more than 10 years experience in musculoskeletal us assessed both wrists ( 36 ) using a us scanner ( iu22 , koninklijke philips electronics , eindhoven , the netherlands ) equipped with a broadband linear - array transducer ( 517 mhz ) with compound imaging and software based on algorithms for optiil dolore cronico di polso rappresenta un quesito comune nellambito della patologia muscoloscheletrica . 
nella maggior parte dei casi , esso pu essere ricondotto ad eventi di tipo traumatico ed , in particolare , a lesioni che determinano un quadro di instabilit carpale [ 1 ]  . 
in questo tipo di instabilit , vi pu essere un coinvolgimento patologico di molte delle strutture anatomiche del polso ( complesso della fibrocartilagine triangolare ( tfc ) , legamenti intrinseci ed estrinseci , muscoli e tendini ) , ma in molti casi la sintomatologia pu essere essenzialmente ricondotta allinteressamento traumatico dei legamenti estrinseci [ 2 , 3 ]  . 
la funzione del legamento ulnopiramidale palmare e dellulnopiramidale dorsale , unitamente allulnolunato , quella di stabilizzare larticolazione radioulnare distale durante i movimenti di pronosupinazione del polso e di prevenire la dislocazione ulnare delle ossa del carpo . 
inoltre , questi legamenti , insieme alle altre componenti della tfc e dei restanti legamenti dellarticolazione radiocarpica , prevengono la dislocazione ulnare dei capi ossei carpali [ 4 , 5 ]  . 
pertanto , molto importante conoscere lanatomia del carpo e , in particolare , quella dei legamenti estrinseci . lintroduzione nelluso clinico di apparecchiature ecografiche provviste di trasduttori ad elevata definizione , unitamente allo sviluppo di nuovi e sempre pi sofisticati algoritmi di post - processing mirati alla ottimizzazione della risoluzione di immagine , ha determinato un aumento dellutilizzo di tali sistemi nello studio delle piccole articolazioni . essi forniscono la possibilit di analizzare con elevato dettaglio anatomico strutture tendinee e legamentose superficiali , anche di piccole dimensioni [ 68 ]  . 
 lobiettivo dello studio stato quello di chiarire le potenzialit applicative dellecografia ad alta risoluzione nello studio delle componenti legamentose estrinseche del carpo descrivendo la tecnica di studio , laspetto ecografico dei legamenti e di descriverne il decorso , utilizzando lartrografia a risonanza magnetica ( artro - rm ) come metodica di riferimento . materiali e metodi stato esaminato un gruppo di 18 soggetti volontari sani , asintomatici , con anamnesi negativa per traumi a livello del polso . 
i soggetti sono stati 10 maschi e 8 femmine con unet media di 34 anni ( range 1858 anni ) , giunti allos506 radiol med ( 2008 ) 113 : 504516 mising image resolution . 
after identifying the ligament on us , the scan plane was optimised to enable visualisation of the entire course of the ligament , and accurate assessment of its echostructure and thickness ; thickness was measured at the middle third portion of the ligament . ten subjects also underwent mr arthrography of the wrist to obtain accurate anatomical data uninfluenced by the us operator . 
mr arthrography of the wrist involves a freehand intra - articular injection of 7 ml of 0.0025 mmol / ml gadoteric acid in 0.9% saline ( dotarem prefilled syringes , guerbet s.a. , villepinte , france ) into the radiocarpal joint . mr imaging was performed using a dedicated c - scan system with a low magnetic field ( 0.2 t ) ( esaote biomedica , genoa , italy ) with t1 - weighted gradient echo ( ge ) and spin echo ( se ) sequences in the three orthogonal planes . statistical analysis statistical analysis was used to calculate the mean thickness of ligaments and assess interobserver variability with cohens kappa value . 
in the coronal plane , the study was always performed in a neutral position , except for the radial collateral ligament , which was evaluated in ulnar deviation of the wrist . 
from a biomeservazione per patologie di tipo muscolo - scheletrico non coinvolgenti il carpo e reclutati per lo studio in oggetto , previo ottenimento di esplicito consenso informato scritto riguardante lintero studio . 
due medici radiologi , con esperienza ultradecennale in ecografia muscoloscheletrica , hanno valutato entrambi i polsi ( 36 ) dei soggetti reclutati , utilizzando un apparecchiatura ecografica ( iu22 , koninklijke philips electronics , eindhoven , olanda ) provvista di trasduttore lineare elettronico a larga banda da 517 mhz con sistema compound e software con algoritmi di ottimizzazione della risoluzione di immagine . 
le scansioni sono state effettuate prendendo come marcatori anatomici le superfici delle ossa carpali nelle sedi di inserzione e decorso dei legamenti estrinseci . una volta individuato ecograficamente il legamento , si provveduto ad ottimizzare il piano di scansione in modo da visualizzarlo lungo tutto il suo decorso , valutandone accuratamente anche ecostruttura e spessore ; le misurazioni dello spessore sono state effettuate al iii medio del legamento . inoltre , in 10 casi , stato eseguito un esame artro - rm di polso , al fine di ottenere informazioni anatomiche precise e non influenzabili dalloperatore ecografico . 
la tecnica artro - rm di polso prevede liniezione intrarticolare a mano libera , a livello dellarticolazione radiocarpica , di 7 ml di una soluzione di 0 , 0025 mmol / ml di acido gadoterico in soluzione fisiologica di sodio cloruro 0 , 9% ( dotarem siringhe preriempite , guerbet s.a. , villepinte , francia )  . 
il livello di concordanza per il valore di stato fissato secondo i limiti seguenti : 00 , 20 scarsa ; 0 , 210 , 40 modesta ; 0 , 410 , 60 moderata ; 0 , 610 , 80 sostanziale ; maggiore di 0 , 81 quasi perfetta [ 9 ]  . radiol med ( 2008 ) 113 : 504516 table 1 mean ligament visualisation rates and interobserver agreement ( value ) risultati palmar side dorsal side radial side radioscaphocapitate 79% , 0.77 radiotriquetral 96% , 0.95 radial collateral 31% , 0.80 radiolunotriquetral 89% , 0.82 ulnotriquetral 63% , 0.58 ulnolunate 65% , 0.69 ulnotriquetral 88% , 0.79 ulnolunato 65% , 0 , 69 ulnopiramidale 88% , 0 , 79 tabella 1 percentuale media dei pazienti in cui il legamento risultato visibile e valore di concordanza interosservatore ( ) versante palmare versante dorsale versante radiale radioscafocapitato 79% , 0 , 77 radiopiramidale 96% , 0 , 95 collaterale radiale 31% , 0 , 80 radiolunopiramidale 89% , 0 , 82 ulnopiramidale 63% , 0 , 58 chanical point of view , the extrinsic dorsal ligaments are tensed during flexion , whereas the extrinsic volar ligaments are tensed during extension . 
as is known , these artefacts are caused by the predominance of diffraction over reflection of the ultrasound beam when the angle of incidence is not perpendicular to the structure being examined . 
the normal us anatomy of the single extrinsic wrist ligaments , the scans and the anatomical landmarks used are described below : radioscaphocapitate ( rsc ) ligament : the rsc ligament arises from the radial aspect of the wrist and extends obliquely to the palmar aspect of the distal scaphoid pole where it attaches with a fibrous band . 
non stato possibile studiare i legamenti radioscafolunato e collaterale ulnare in nessuno dei 36 polsi esaminati . tutti i legamenti si presentano come strutture caratterizzate da elevata ecogenicit , di aspetto fibrillare , con ecostruttura interna molto simile a quella tendinea e sono riconoscibili nel contesto dei tessuti molli circostanti . 
sul piano coronale , lo studio dei legamenti stato effettuato sempre in posizione neutra , eccetto per il legamento collaterale radiale che stato valutato con il carpo in deviazione ulnare . 
lanalisi ecografica effettuata su legamenti in tensione ha consentito di apprezzare il loro decorso e lecostruttura con migliore dettaglio e con una conseguente riduzione degli artefatti legati allanisotropia ; come noto , la comparsa di tali artefatti legata alla prevalenza dei fenomeni di diffrazione del fascio ultrasonoro rispetto a quelli di riflessione , quando langolo dincidenza non ortogonale alla struttura in esame . 
le immagini artro - rm hanno evidenziato correttamente in tutti i casi i legamenti estrinseci del carpo , ad eccezione del legamento collaterale ulnare che non stato dimostrato in nessun paziente . 
2 legamenti estrinseci dorsali : 5 radiolunopiramidale dorsale ( rlpd ) , 6 ulnopiramidale dorsale ( upd ) , 7 collaterale radiale ( rc )  . arises from the palmar aspect of the radial styloid process , passes over the scaphoid bone and inserts onto the lunate . 
in realt , questa struttura anatomica viene considerata pi propriamente un ispessimento della capsula articolare che si estende dal processo stiloideo ulnare fino al piramidale e al pisiforme , piuttosto che un legamento vero e proprio [ 13 , 14 ]  . 
mechanical instability of the radius is thus contained by the extrinsic ligaments , mainly by the rsc and by the rlt , which , with their oblique orientation , contain the radiocarpal joint in all directions [ 11 , 12 ]  . 
attualmente , i legamenti estrinseci del carpo hanno acquisito una importanza rilevante nello studio del polso traumatico ; essi sono infatti coinvolti nella patogenesi dellinstabilit carpale , che in passato si pensava ascrivibile unicamente ai legamenti intrinseci scafolunato e lunopiramidale [ 16 ]  . 
 table 3 ultrasound assessment of the radiolunotriquetral ligament tabella 3 valutazione ecografica del legamento radiolunopiramidale radiolunotriquetral ligament legamento radiolunopiramidale thickness bony landmarks wrist position probe orientation 2.10.7 mm palmar side of the styloid process , triquetrum slight dorsiflexion axial oblique scan with a 1015 medial inclination spessore riferimenti ossei posizione del polso orientamento della sonda 2 , 10 , 7 mm lato palmare processo stiloideo , piramidale leggera dorsiflessione scansione assiale obliqua con 1015 di inclinazione mediale radiol med ( 2008 ) 113 : 504516 fig . 
in fact , this anatomical structure is more appropriately considered as a thickening of the joint capsule extending from the ulnar styloid process to the triquetrum and the pisiform rather than a ligament proper [ 13 , 14 ]  . 
the ratable 4 ultrasound assessment of the palmar ulnolunate ligament palmar ulnolunate ligament thickness bony landmarks wrist position probe orientation 1.90.7 mm ulna , lunate slight dorsiflexion longitudinal oblique scan with a 510 craniocaudal lateral inclination tabella 4 valutazione ecografica del legamento ulnolunato palmare legamento ulnolunato palmare spessore riferimenti ossei posizione del polso orientamento della sonda 1 , 90 , 7 mm ulna , semilunare leggera dorsiflessione scansione longitudinale obliqua con 510 di inclinazione laterale craniocaudale sono state proposte diverse metodiche di imaging per la valutazione diagnostica delle componenti legamentose estrinseche ed intrinseche del carpo . 
molti autori concordano nel considerare lartro - rm lesame di riferimento nella diagnostica per immagini delle patologie del carpo . nellartro - rm , infatti , liniezione intrarticolare di una miscela di soluzione fisiologica e gadolinio in grado di distendere le strutture capsulari articolari permettendone una visualizzazione ottimale con unaccuratezza diagnostica pari al 95% [ 1719 ]  . 
 [ 20 ] , la percentuale di visualizzazione completa dei legamenti stata di 73% per il legamento radiolunopiramidale , 62% per il radioscafocapitato , 74% per lulnopiramidale palmare ed il 93% per il radiopiramidale dorsale . 
nel nostro studio , stato possibile identificare i legamenti radiolunopiramidale ( 89% dei casi esaminati ) , radioscafocapitato ( 79% ) , ulnopiramidale palmare ( 88% ) e radiopiramidale dorsale ( 96% ) con unottima concordanza tra i due osservatori ( tabella 1 ) , con unaccuratezza diagnostica superiore a quanto riportato nello sturadiol med ( 2008 ) 113 : 504516 fig . 
b ultrasound anatomy scheme ( p , triquetrum ; u , ulna ; tfc , triangular fibrocartilage ; pup , palmar ulnotriquetral ligament ; fpd , flexor digitorum profundis )  . 
b schema dellanatomia ecografica ( p , piramidale ; u , ulna ; tfc , fibrocartilagine triangolare ; pup , legamento ulnopiramidale palmare ; fpd , flessore profondo delle dita )  . 
currently , the extrinsic carpal ligaments have become very important in the study of the traumatised wrist , given their involvement in the pathogenesis of carpal instability , which in the past was thought to be ascribable to the intrinsic scapholunate and lunotriquetral ligaments alone [ 16 ]  . 
necessario tuttavia sottolineare che il lavoro citato stato condotto con una sonda ecografica a minor frequenza ( 12 mhz contro 17 mhz del nostro studio ) e con operatori di minor esperienza in ecografia muscoloscheletrica ( operatori con 4 e 7 anni di esperienza in ecografia muscolo - scheletrica , contro radiologi che eseguono questo tipo di esami da oltre 10 anni )  . 
i rimanenti legamenti sono stati pi difficili da visualizzare ( con un valore basso di ) ed , in particolare , il collaterale ulnare e il radiolunato non stati mai individuati , sia per le ridotte dimensioni sia per il decorso irregolare rispetto alla superficie cutanea . 
le corrispondenti immagini di artrorm ci hanno permesso di confrontare le principali caratteristiche anatomiche dei legamenti , con una coerente correlazione anatomica tra ecografia e risonanza , sia nei valori table 5 ultrasound assessment of the palmar ulnotriquetral ligament tabella 5 valutazione ecografica del legamento ulnopiramidale palmare palmar ulnotriquetral ligament legamento ulnopiramidale palmare thickness bony landmarks wrist position probe orientation 2.10.4 mm ulna , triquetrum slight dorsiflexion pure longitudinal scan spessore riferimenti ossei posizione del polso orientamento della sonda 2 , 10 , 4 mm ulna , piramidale leggera dorsiflessione scansione longitudinale pura radiol med ( 2008 ) 113 : 504516 fig . 
b ultrasound anatomy scheme ( r , radius ; l , lunate ; p , triquetrum ; rpd , dorsal radiotriquetral ligament ; ecd , extensor digitorum communis )  . 
b schema dellanatomia ecografica ( r , radio ; l , semilunare ; p , piramidale ; rpd , legamento radiopiramidale dorsale ; ecd , tendini estensori comuni delle dita )  . 
 [ 20 ] reported a rate of complete visualisation of 73% for the radiolunotriquetral , 62% for the radioscaphocapitate , 74% for the palmar ulnotriquetral and 93% for the dorsal radiotriquetral ligament . 
a litable 6 ultrasound assessment of the dorsal radiotriquetral ligament tabella 6 valutazione ecografica del legamento radiopiramidale dorsale dorsal radiotriquetral ligament legamento radiopiramidale dorsale thickness bony landmarks wrist position probe orientation 2.60.4 mm radium , triquetrum slight palmar flexion oblique axial scan with a 2030 craniocaudal medial inclination spessore riferimenti ossei posizione del polso orientamento della sonda 2 , 60 , 4 mm radio , piramidale leggera flessione palmare scansione assiale obliqua con 2030 di inclinazione mediale craniocaudale radiol med ( 2008 ) 113 : 504516 fig 8a - c dorsal ulnotriquetral ligament . 
b ultrasound anatomy scheme ( p , triquetrum ; l , lunate ; u , ulna ; upd , dorsal ulnotriquetral ligament ; fuc , flexor carpi ulnaris )  . 
b schema dellanatomia ecografica ( p , piramidale ; l , semilunare ; u , ulna ; upd , legamento ulnopiramidale dorsale ; fuc , flessore ulnare del carpo )  . 
the remaining ligaments were more difficult to visualise ( low values ) and , in particular , the collateral ulnar and the radiolunate were never identified , owing both to their small size and irregular course relative to the skin surface . 
the corresponding mr arthrography images enabled us to compare the main anatomical features of ligaments , with a good anatomical vello carpale , infatti , lecografia non consente una valutazione ottimale delle componenti ossee e si rivela solo parzialmente utile nella caratterizzazione delle superfici cartilaginee e delle strutture intrarticolari [ 7 ]  . lecografia richiede una lunga curva dapprendimento e , se eseguita con apparecchiature di vecchia generazione , possiede unaccuratezza diagnostica inferiore rispetto allartro - rm . 
tuttavia , allo stato dellarte , non esiste alcuno studio scientifico che dimostri che le tecniche ecografiche ad alta risoluzione con macchine di nuova generazione siano inferiori allartro - rm relativamente allaccuratezza diagnostica . 
ad ogni buon conto , lecografia ad alta risoluzione da considerarsi come una metodica emergente , a table 7 ultrasound assessment of the dorsal ulnotriquetral ligament tabella 7 valutazione ecografica del legamento ulnopiramidale dorsale dorsal ulnotriquetral ligament legamento ulnopiramidale dorsale thickness bony landmarks wrist position probe orientation 2.20.5 mm ulna , triquetrum wrist in slight dorsiflexion and in ulnar deviation pure longitudinal scan 2 , 20 , 5 mm ulna , piramidale spessore riferimenti ossei posizione del polso polso in flessione dorsale e deviazione ulnare orientamento della sonda scansione longitudinale pura della sonda radiol med ( 2008 ) 113 : 504516 fig . 
 [ 13 ] and course . mr arthrography and us images were not compared in terms of diagnostic accuracy , as the purpose of our study was to evaluate the ability of us to identify normal extrinsic ligaments of the wrist . 
further limitations to the study are related to the intrinsic limits of the modality used . at the carpal level , us does not allow optimal assessment of the bony components and is only partially useful for characterising cartilage surfaces and intra - articular structures [ 7 ]  . us has a long learning curve and , if performed with oldgeneration equipment , it has lower diagnostic accuracy than mr arthrography . 
diagnostic imaging based on ultrasound ( us ) , computed tomography ( ct ) , magnetic resonance imaging ( mri ) and digital subtraction angiography ( dsa ) has a fundamental role in detecting visceral involvement in hht patients and is therefore crucial for the prognostic assessment and therapeutic approach . 
mri and ct angiography are the methods of choice for diagnosing cerebral involvement , and it is debated whether mri could be considered as a screening examination on account of its noninvasiveness . 
pulmonary arteriovenous malformations , diffuse telangiectases or high - flow , low - pressure shunts between pulmonary arteries and veins can be studied with contrast - enhanced us , but multidetector ct seems to provide the most comprehensive evaluation of their angioarchitecture , whereas angiography has a predominant role in treatment . 
us is useful for detecting hepatic lesions but should be completed by more accurate imaging methods such as multidetector ct and mri . riassunto la telangiectasia emorragica ereditaria ( hht ) , o malattia di rendu - osler - weber , un disordine vascolare ereditario , caratterizzato dalla comparsa di lesioni angiodisplasiche mucocutanee e viscerali , la cui diagnosi si basa esclusivamente su criteri clinici . 
la diagnostica per immagini , mediante gli ultrasuoni ( us ) , la tomografia computerizzata ( tc ) , la risonanza magnetica ( rm ) e la angiografia ( dsa ) , ha un ruolo cruciale nella diagnosi del coinvolgimento viscerale nei pazienti affetti da hht ed , pertanto , fondamentale nella valutazione prognostica e nella impostazione terapeutica . 
la rm e la angio - tc sono le metodiche di scelta nella diagnosi dellinteressamento cerebrale , ed dibattuto se , per la scarsa invasivit , la rm sia da proporre come metodica di screening . 
le malformazioni arterovenose polmonari , telangiectasie diffuse o fistole tra arterie e vene polmonari , possono essere ricercate con us con mdc , ma la tc multidetettore appare lindagine pi completa per la valutazione della loro angioarchitettura mentre langiografia mantiene un ruolo prevalentemente terapeutico . 
gli us sono utili nella ricerca delle lesioni epatiche , ma devono essere integrati da indagini pi accurate quali la tc multidetettore e la rm . 548 radiol med ( 2008 ) 113 : 547566 keywords hereditary hemorrhagic telangiectasia renduosler - weber disease cerebral arteriovenous malformations pulmonary arteriovenous malformations intrahepatic shunts parole chiave telangiectasia emorragica ereditaria malattia di rendu - osler - weber malfomazioni arterovenose cerebrali malformazioni arterovenose polmonari fistole intraepatiche introduction introduzione hereditary haemorrhagic telangiectasia ( hht ) , also known as rendu - osler - weber disease , is a hereditary autosomaldominant vascular disorder that occurs with an estimated frequency of 1020 cases / 100 , 000 [ 1 , 2 ]  . 
pathological hallmarks of the disease are mucocutaneous and visceral angiodysplastic lesions ( telangiectases and arteriovenous shunts ) variously distributed throughout the cardiovascular systethe nasal mucosa and the skin are the most frequent sites of telangiectases , although a significant proportion of hht patients has pulmonary , cerebral or hepatic involvement [ 3 , 4 ]  . 
less commonly reported sites include the gastrointestinal tract and other abdominal organs , such as the pancreas . hht diagnosis is based on the identification of at least three of the four curaao criteria : presence of mucocutaneous telangiectases , recurrent spontaneous episodes of epistaxis , visceral involvement and a family history of the disease [ 57 ]  . 
although clinical assessment has a fundamental role in detecting the disease , diagnostic imaging , especially thanks the technological advances in computed tomography ( ct ) and magnetic resonance imaging ( mri ) , is indispensable for identifying vascular abnormalities and establishing disease severity . this paper provides a general outline of the possibilities of diagnostic imaging in the study of visceral involvement in hht . 
it draws on the experience of the diagnostic imaging division of the interdepartmental centre for the study of hht of our teaching hospital , which , within the framework of an hht screening programme , started approximately 6 years ago and has studied 167 patients to date . 
the first level consists of ultrasound ( us ) completed by colour - doppler us ( cdus ) of the upper abdomen , and contrast echocardiography ( ce )  . the second level consists of a multiphase ct study of the chest and abdomen for simultaneous assessment of pulmonary and hepatic involvement . 
the abdomen is scanned during a dual arterial phase ( early and delayed ) to assess the hepatic parenchyma , and the scans are extended to the chest during the portal phase to screen for pulmonary fistulas . patients with treatable pulmonary vascular malformations , that is , malformations amenable to embolotherapy , are followed up at yearly intervals . 
patients with small pulla telangiectasia emorragica ereditaria ( hht ) , nota come malattia di rendu - osler - weber , un disordine vascolare a trasmissione ereditaria autosomica dominante che si manifesta con una frequenza stimata intorno a 1020 / 100000 [ 1 , 2 ]  . 
da un punto di vista anatomo - patologico le alterazioni caratteristiche di tale patologia sono rappresentate da lesioni angiodisplasiche mucocutanee e viscerali ( telangiectasie e malformazioni arterovenose ) , variamente distribuite lungo tutto il sistema cardiovascolare . 
la mucosa nasale e la cute sono le sedi pi frequentemente interessate dalle telangiectasie , ma un numero significativo di pazienti con hht presenta un interessamento polmonare , cerebrale o epatico [ 3 , 4 ]  . 
meno frequente , anche se riportato in letteratura il coinvolgimento del tratto gastroenterico e di altri visceri addominali , quali il pancreas . la diagnosi di hht si basa sul riconoscimento di almeno tre dei quattro criteri diagnostici di curaao : presenza di telangiectasie mucocutanee , comparsa di episodi spontanei e ricorrenti di epistassi , identificazione di un coinvolgimento viscerale e familiarit per la malattia [ 57 ]  . 
sebbene la valutazione clinica abbia un ruolo fondamentale nel riconoscimento di tale patologia , la diagnostica per immagini , soprattutto grazie allevoluzione tecnologica delle apparecchiature di tomografia computerizzata ( tc ) e di risonanza magnetica ( rm ) appare indispensabile nellidentificazione delle alterazioni vascolari e nella definizione della gravit della patologia . il presente lavoro , il cui scopo fornire un quadro generale delle attuali possibilit della diagnostica per immagini nello studio del coinvolgimento viscerale di tale rara patologia , il risultato dellesperienza della sezione di diagnostica per immagini del centro interdipartimentale per lo studio della hht del nostro policlinico alla quale sono afferiti ad oggi , nellambito di un programma di screening della malattia iniziato circa 6 anni fa , 167 pazienti . 
 nello studio del coinvolgimento epatico e polmonare tale programma si articola su due livelli di esami diagnostici eseguiti indipendentemente luno rispetto allaltro : il primo livello prevede lesecuzione dello studio ecografico delladdome superiore , completato dallesame color - doppler , e di uno studio ecocardiografico con mdc ( mdc - ec )  . 
in patients showing only hepatic involvement , the 2 - year follow - up consists of ct of the abdomen with scans extended to the chest to identify the possible presence of pulmonary fistulas . digital subtraction angiography ( dsa ) of the pulmonary vasculature , besides being used to evaluate pulmonary fistulas prior to endovascular treatment , is reserved for cases with discordant ce and pulmonary ct findings . since september 2006 , the evaluation of abdominal visceral involvement has been completed with contrast - enhanced mri of the abdomen . 
moreover , 30%50% of hht patients have multiple lesions [ 9 , 11 ] , whereas the incidence of multifocal lesions is only 0.7%3% in cerebral avms that are not associated with hht [ 9 , 12 ]  . 
cvms are classified based on the affected vascular district into aneurysms , arteriovenous shunts , capillary malformations ( telangiectases ) , venous malformations ( cavernomas ) and venous developmental abnormalities ( venous angiomas ) [ 13 ]  . 
qualora il paziente sia risultato portatore di piccole fistole polmonari che non necessitano di trattamento , il protocollo prevede lesecuzione di un nuovo esame tc del torace , senza iniezione di mdc , a distanza di due anni . 
nei pazienti in cui le alterazioni vascolari polmonari si associano al coinvolgimento epatico , il controllo a 2 anni viene effettuato con iniezione di mdc ed esteso anche alladdome con protocollo multifasico . nei pazienti con esclusivo coinvolgimento epatico il controllo tc a due anni comprende anche lo studio del torace per la ricerca di una eventuale comparsa di fistole polmonari . langiografia a sottrazione dimmagine ( dsa ) della vascolarizzazione polmonare viene riservata , oltre che nella valutazione pre - trattamento endovascolare delle fistole polmonari , solo ai casi in cui esiste una discrepanza tra il risultato della mdc - ec e quello della tc polmonare . a partire dal settembre 2006 , la valutazione del coinvolgimento viscerale addominale integrata dallesecuzione di un esame rm addominale con somministrazione di mdc ( cerm )  . 
dei 167 pazienti studiati sono stati complessivamente riconosciuti affetti da malformazioni arterovenose epatiche 116 pazienti , 92 da malformazioni arterovenose polmonari e 8 da malformazioni vascolari cerebrali . malformazioni vascolari cerebrali la presenza di malformazioni cerebrovascolari ( cvms ) , in associazione ad hht , stata descritta soltanto nel 5%10% dei casi [ 8 , 9 ] , ma si ritiene che la reale prevalenza sia pi alta . 
infatti lesecuzione di una rm cerebrale come esame di screening in pazienti affetti dalla malattia ha consentito di identificare la presenza di cvms in circa il 23% dei casi [ 10 ]  . 
inoltre in tali pazienti , il riscontro di lesioni multiple stato descritto nel 30%50% dei casi [ 9 , 11 ] , mentre nei soggetti portatori di malformazioni arte550 radiol med ( 2008 ) 113 : 547566 normal communication between arteries and veins . 
this communication , through one or more feeding artery and one or more draining vein , may occur via an interposed abnormal vascular network ( nidus ) , in which case it is defined as a true avm , or directly , through a high - flow channel without the interposition of vessels . 
on the basis of their angiographic appearance , avms are classed into micro - avms when the feeding arteries and draining veins have normal dimensions and the nidus is < 1 cm in diameter , and macro - avms , in which the arteries and veins appear generally enlarged and the nidus is > 1 cm in diameter [ 1517 ]  . 
venous angiomas , considered developmental venous abnormalities [ 18 ] , are characterised by venous ectasia , usually with subcortical location ( periventricular white matter , midbrain , cerebellum ) in the absence of arterial ectasia . 
imaging procedures used to establish a diagnosis of cvm in patients affected by hht are ct angiography , mr angiography and dsa . on ct , avms generally appear isohyperdense in the baseline scans , with a nodular or serpiginous appearance , at times associated with calcification . 
these lesions enhance rapidly after contrast injection , revealing a mulberry - like appearance , which is rounded in intraparenchymal lesions and triangular in sulcal lesions , that is , lesions lodged in a cortical sulcus . 
the use of contrast material helps in the morphological assessment of the disease and thus in the diagnosis [ 10 ] , especially in the case of lowflow avms . on ct , cavernous malformations are rounded and often appear slightly hyperdense , with a cloud - like appearance rovenose cerebrali non associate ad hht , la plurifocalit incide soltanto nel 0 , 7%3% dei pazienti [ 9 , 12 ]  . 
le cvms sono genericamente classificate , in base al distretto vascolare interessato , in aneurismi , shunt arterovenosi , malformazioni capillari ( telangiectasie ) , venose ( malformazioni cavernose ) ed anomalie dello sviluppo venoso ( angiomi venosi ) [ 13 ]  . 
tutti tali tipi di malformazioni , anche se con varia incidenza , sono riportati in associazione alla hht [ 14 ]  . gli shunt arterovenosi costituiscono la malformazione vascolare di pi frequente riscontro nei pazienti affetti dalla hht e consistono in una anomala connessione tra vasi arteriosi e venosi . 
tale connessione attraverso una o pi arterie afferenti ed una o pi vene di drenaggio pu avvenire con linterposizione di una rete vascolare anomala ( nidus ) , ed in tal caso si parla di malformazioni arterovenose propriamente dette ( avms ) , oppure in maniera diretta , ad alto flusso , senza interposizione di vasi . 
in base al loro aspetto angiografico le avms si classificano in micro - avms , quando le arterie afferenti e le vene efferenti hanno normali dimensioni ed il nidus ha diametro < 1 cm , e macro - avms , in cui i vasi arteriosi e venosi appaiono generalmente dilatati ed il nidus ha diametro > 1 cm [ 1517 ]  . 
sono comunemente definite cavernomi e sono veri e propri laghi vascolari , generalmente venosi , spesso circondati da una pseudocapsula costituita da un vallo gliotico , ricco di depositi di emosiderina e spesso calcificazioni . 
gli angiomi venosi , considerati anomalie dello sviluppo venoso [ 18 ] , sono rappresentati dalla ectasia di un vaso venoso , abitualmente a localizzazione sottocorticale ( sostanza bianca periventricolare , mesencefalo , cervelletto ) , in assenza di dilatazione arteriosa . 
per porre diagnosi di malformazioni vascolari cerebrali nei pazienti affetti da hht le procedure diagnostiche abitualmente utilizzate sono rappresentante dalla tc ( angio - tc ) , dalla rm ( angio - rm ) e dallangiografia . alla tc le avms appaiono generalmente iso - iperdense nelle sequenze di base , con aspetto nodulare o serpiginoso , talora con associate calcificazioni . 
tali lesioni subiscono un marcato incremento di densit dopo iniezione del mdc che ne svela laspetto moruliforme , rotondeggiante nel caso di localizzazione intraparenchimale , triangolare in quelle sulcali , cio indovate in un solco corticale . 
computed tomography angiography , coronal maximum intensity projection reconstruction ( a ) , t1weighted inversion recovery magnetic resonance image ( mri ) in the axial plane ( b ) and selective digital subtraction angiography ( dsa ) of the left carotid artery ( c )  . 
la dsa definisce con esattezza lemodinamica della avm , le afferenze provenienti dallarteria silviana ( punte di freccia piene ) , il nidus ( freccia ) e gli scarichi venosi drenanti in collettori corticali ( punte di freccia vuote )  . that mimics a recent brain haematoma . 
lutilizzo del mezzo di contrasto facilita lanalisi morfologica della patologia e quindi la diagnosi [ 10 ] specie per le avms a basso flusso . le malformazioni cavernose alla tc hanno forma rotondeggiante ed appaiono spesso tenuemente iperdense , con aspetto nubecolare che simula un ematoma cerebrale recente . 
la iniezione del mdc determina una scarsa e sfumata modificazione del quadro [ 19 ]  . 552 radiol med ( 2008 ) 113 : 547566 vein and the small orthogonal tributaries with the typical caput medusae appearance on contrast - enhanced images . 
 in some cases , mri demonstrates only indeterminate changes that do not fit into any of the categories of arteriovenous ( avms and avfs ) or venous ( venous angiomas and cavernomas ) malformations and are characterised by variable signal intensity and enhancement [ 10 ]  . 
these lesions may , in fact , be depicted as small punctate or curvilinear hypoor hyperintense areas 1015 mm in diameter , without a nidus , without evident enlargement of adjacent arteries or veins and with variable signal intensity on t1and t2 - weighted sequences . 
the use of thinner sections , background suppression and administration of contrast material might improve the mri sensitivity in these cases [ 10 ]  . dsa is considered the diagnostic gold standard in studying cvthis examination allows one to analyse the angioarchitecture of avms and avfs by depicting the feeding arteries , the nidus and shunt points , the draining veins , haemodynamics and possible associated malformations ( arterial and venous aneurysms ) and provides accurate information on lesion size and location , which is crucial for treatment planning . 
 finally , dsa is more accurate in establishing the nature of malformations classified as indeterminate at mri , revealing , in most cases , small avms with abnormal angioarchitecture [ 10 ]  . 
in general , the prevalence of neurological disorders in hht patients ranges from 8% to 27% ; in 61% of cases , these disorders are caused by embolic complications of pulmonary arteriovenous fistulas , but in around 28% of cases , they are caused by intracerebral haemorrhage secondary to cvms [ 10 ]  . according to some authors , the reported very low rate of haemorrhage from cerebral avms in hht [ 10 , 14 , 20 ] makes routine screening for these malformations unnecessary [ 14 ]  . 
according to others , because the vascular lesions in hht tend to enlarge over time and are often multiple [ 14 , 21 , 22 ] , mri should be used as a screening tool in asymptomatic patients [ 10 ]  . treatment options for cvms depend on the size and angioarchitecture of the malformation , on their location and on the possible symptoms . 
large lesions , especially high - flow lesions with a high risk of rupture , require treatment , and alla rm , che molto pi sensibile e specifica nel loro studio , presentano un caratteristico cercine ipointenso nelle sequenze a lungo tr che sembra allargarsi nelle sequenze ge per la presenza di emosiderina . 
la lesione ha una zona centrale di aspetto settato multilobulare e disomogeneamente reticolare nelle sequenze t2 - pesate , per la presenza di aree ipoed iperintense , e talora mostra incremento di intensit dopo utilizzo del mezzo di contrasto per la presenza di sinusoidi [ 10 ]  . nel caso delle anomalie dello sviluppo venoso ( angiomi venosi ) sia la tc che la rm , dopo la somministrazione del mezzo di contrasto , consentono di identificare il vaso dilatato sottocorticale e le piccole vene tributarie , con decorso ortogonale e caratteristico aspetto a caput medusae . in alcuni casi il reperto rm consiste nella dimostrazione di alterazioni indeterminate , che non rientrano nelle categorie descritte delle malformazioni arterovenose ( avms e avfs ) o venose ( angiomi venosi e cavernomi ) e sono caratterizzate da intensit di segnale ed enhancement variabile [ 10 ]  . 
tali lesioni possono , infatti , essere rappresentate da piccole aree puntiformi o curvilinee ipood iperintense , con diametro di 1015 mm , prive di nidus , senza evidente dilatazione dei vasi arteriosi o venosi circostanti e con varia intensit di segnale nelle sequenze t1 e t2 . 
in tali casi luso di sezioni sottili , la tecnica di soppressione dello sfondo e liniezione del mezzo di contrasto possono incrementare la sensibilit della rm [ 10 ]  . attualmente il gold standard diagnostico per la studio delle cvms considerata la dsa . 
questo esame consente di analizzare langioarchitettura delle avms e avfs , evidenziando le arterie afferenti , il nidus ed i punti di fistola , le vene efferenti , lemodinamica e le malformazioni eventualmente associate ( aneurismi arteriosi e venosi ) ed inoltre fornisce precise informazioni sulla loro dimensione e localizzazione , fondamentali nella pianificazione terapeutica . 
gli angiomi venosi sono caratterizzati da piccoli vasi venosi di vario diametro che confluiscono in una vena pi larga [ 9 , 10 ]  . la dsa , infine , dimostra una maggiore accuratezza nella definizione delle alterazioni cerebrali classificate come indeterminate alla rm , rivelando , nella maggior parte dei casi , che si tratta di piccole avms con angioarchitettura anomala [ 10 ]  . 
la presenza di cvms pu determinare la comparsa di differenti disturbi neurologici , che vanno dalla semplice cefalea ad una sintomatologia acuta legata alla comparsa di crisi convulsive o di emorragie intraparenchimali e subaracnoidee . 
in generale , nei pazienti affetti da hht , la prevalenza dei disturbi neurologici compresa tra l8% ed il 27% ; tali disturbi nel 61% dei casi sono legati a complicanradiol med ( 2008 ) 113 : 547566 endovascular embolisation is proposed as a valuable alternative to surgical excision or radiotherapy . 
the latter tend to be high - flow , low - pressure fistulas that consist of direct communications between enlarged feeding arteries and draining veins , often with an interposed aneurysmal sac [ 23 ]  . 
detection of these malformations should therefore always prompt careful evaluation in the attempt to identify other diagnostic criteria for hht and the extension of diagnostic tests to the patients family members . left untreated , approximately 50% of patients with pavms will develop disabling or fatal complications . 
approximately 10% of patients develop pleural or pulmonary haemorrhage caused by bleeding of the abnormal vessels in a bronchus or the pleural cavity or rupture of the aneurysmal nidus , which may prove fatal [ 26 ]  . 
bypass of the pulmonary capillary bed resulting from the direct communication between the pulmonary and systemic circulation due to arteriovenous shunts leads to hypoxia , and more than 45% of patients with hht and pavms present with exercise intolerance , dyspnoea and cyanosis [ 23 ]  . 
severe neurological complications affect about 40% of hht patients either in the form of stroke ( 30% ) or brain abscess ( 10% ) [ 27 ]  . surgical treatment of pavms , consisting of the resection of the larger lesions , has been long considered the treatment of choice , capable of producing a temporary remission of symptoms . 
enlargement of the smaller lesions , however , leads to recurrence [ 28 ] so that nonsurgical procedures have recently been proposed that have shown satisfactory results in large patient series . 
transcatheter embolisation of all pavms with a feeding artery at least 3 mm in diameter [ 29 ] is considered the most appropriate treatment because it is effective and can be repeated whenever necessary . given that adequate treatment reduces the risk of serious complications , detection of pavms is very important in both symptomatic and asymptomatic patients . 
diagnostic ze emboliche in rapporto alla presenza di fistole arterovenose polmonari , ma in circa il 28% dei casi sono legati ad emorragia intracerebrale secondaria a cvms [ 10 ]  . la constatazione che nei pazienti con hht riportata una percentuale molto bassa di emorragie da avms cerebrali [ 10 , 14 , 20 ] , farebbe venir meno , secondo alcuni , la necessit di uno screening routinario di tali malformazioni [ 14 ]  . 
secondo altri autori , al contrario , dal momento che le alterazioni vascolari in tale malattia presentano un progressivo incremento volumetrico e sono spesso multiple [ 14 , 21 , 22 ] , opportuna lesecuzione di un rm , come metodica di screening nei pazienti asintomatici [ 10 ]  . le opzioni terapeutiche in presenza di cvms dipendono dalle dimensioni e dallangioarchitettura , ed anche dalla loro localizzazione ed eventuale sintomatologia . 
le lesioni voluminose , specie se ad alto flusso ed elevato rischio di rottura , devono essere trattate ed attualmente lembolizzazione per via endovascolare si propone come valida alternativa allasportazione chirurgica o alla radioterapia . 
le lesioni di piccole dimensioni possono invece essere soltanto monitorate nel tempo per controllore un eventuale incremento volumetrico e la comparsa di alterazioni emodinamiche . malformazioni arterovenose polmonari pi del 30% dei pazienti affetti da hht sviluppano malformazioni arterovenose polmonari ( pavms )  . 
in tal caso si tratta di fistole ad alto flusso e bassa pressione , che consistono in connessioni dirette tra arterie afferenti dilatate e vene di drenaggio spesso con linterposizione di una sacca aneurismatica [ 23 ]  . 
circa il 95% delle arterie afferenti origina dalla circolazione polmonare piuttosto che sistemica [ 24 ]  . le pavms rappresentano un marker della malattia ; la recente letteratura , infatti , riporta che il 90% dei pazienti con pavms affetto da hht e nel restante 10% si tratta di casi sporadici [ 23 , 25 ]  . 
il riconoscimento di tali malformazioni dovrebbe , pertanto , indurre sempre ad unattenta valutazione del paziente alla ricerca degli altri criteri diagnostici della hht ed anche , eventualmente , allestensione delle indagini diagnostiche ai famigliari . qualora non sottoposti a trattamento , circa il 50% dei pazienti con pavms destinato a sviluppare complicanze disabilitanti e talora fatali . 
in circa il 10% di tali pazienti , infatti , possono comparire emorragie pleuriche o polmonari generate dal sanguinamento dei vasi anomali in un bronco o nella cavit pleurica o dalla rottura del nidus aneurismatico che pu causare lexitus del paziente [ 26 ]  . 
il bypass del letto capillare polmonare , conseguente alla diretta comunicazione tra le circolazioni polmonare e sistemica dovuta alla presenza degli shunts , determina la comparsa di ipossia , ed infatti pi del 45% dei pazienti con hht e pavms presenta intolleranza allesercizio fisico , dispnea e cianosi [ 23 ]  . 
la scomparsa del filtro capillare polmonare 554 radiol med ( 2008 ) 113 : 547566 imaging thus plays the crucial role of identifying and characterising pavms and guiding treatment decisions . 
different noninvasive imaging techniques have been proposed for studying pavms : chest x - ray ( cxr ) , contrast echocardiography ( ce ) , ct and mri [ 30 ]  . on cxr , pavms appears as rounded , noncalcified lesions that are generally peripheral , well circumscribed and with regular margins , often connected to the hilum by radiopaque bands that represent the enlarged feeding and draining vessels . 
sensitivity of the technique is , however , so low ( approximately 60% ) [ 31 ] that a two - view chest radiogram is unable to rule out the presence of pavms [ 32 ]  . 
 ce , performed with agitated saline as a contrast agent , is recognised as a highly accurate method in diagnosing pavms , with a sensitivity of 93% and a specificity 62% [ 33 ] ; it is also very useful for evaluating clinical outcome after embolotherapy [ 34 ]  . 
in addition , it is the only method capable of demonstrating the presence of right - to - left shunting and characterising it as intracardiac or intrapulmonary [ 31 ]  . the method is based on the observation that microbubbles introduced in a peripheral vein are able to produce intracardiac sonographic contrast [ 35 , 36 ]  . 
thus , when a solution of agitated saline ( or polygelin colloid ) is injected into the peripheral vein of a healthy subject , the contrast rapidly appears in the right atrium and then dissipates and is not seen in the left heart . 
ce is a quantitative method that assesses the presence of haemodynamically significant shunts , but its main limitation is the lack of qualitative information about the number , size , location and angioarchitecture of the lesions . ct , in particular spiral multidetector ct ( mdct ) , provides a three - dimensional ( 3d ) , multiplanar ( mpr ) angiography - like ( mip , volume rendered ) study with a high level of anatomical detail , even without the use of contrast material , and it is fundamental in the detection and morphological assessment of pavms [ 30 , 39 , 40 ]  . 
it offers a more accurate anatomical depiction of pavms than do other noninvasive imaging modalities , it is considered complementary to angiography in the study of pavms before treatment and it is fundamental during follow - up . 
complicanze neurologiche serie colpiscono , infatti , circa il 40% dei pazienti affetti da hht e sono rappresentate da ictus ( 30% ) e da ascessi cerebrali ( 10% ) [ 27 ]  . la terapia chirurgica delle pavms , che consiste nella resezione delle lesioni di maggiori dimensioni , stata a lungo considerata il trattamento di scelta , in grado di produrre una remissione temporanea dei sintomi . 
lingrandimento delle malformazioni pi piccole induce , per , la ricorrenza dei sintomi [ 28 ] cosicch , negli anni recenti , sono state proposte procedure non chirurgiche che hanno mostrato risultati soddisfacenti in larghe serie di pazienti . 
attualmente , lembolizzazione transcatetere di tutte le pavms con arteriola afferente di almeno 3 mm di diametro [ 29 ] considerata il trattamento pi opportuno poich efficace e ripetibile ogni qualvolta sia necessario . dal momento che un adeguata terapia in grado di ridurre il rischio di insorgenza di complicanze serie , la diagnosi della presenza di pavms molto importante sia nei pazienti sintomatici che asintomatici . 
differenti metodiche di imaging non invasivo sono state proposte nello studio delle pavms : radiografia del torace ( rt ) , mdc - ec , tc e rm [ 30 ]  . alla rt le pavms appaiono come lesioni rotondeggianti non calcifiche , generalmente periferiche , ben circoscritte , a margini regolari , spesso raggiunte da bande ilari radiopache che rappresentano i vasi afferenti ed efferenti dilatati . 
la sensibilit di tale metodica comunque bassa ( intorno al 60% ) [ 31 ] per cui attualmente acclarato che un radiogramma in duplice proiezione del torace non in grado di escludere la presenza di pavms [ 32 ]  . 
 lmdc - ec , eseguita utilizzando come mezzo di contrasto una soluzione salina agitata , riconosciuta come metodica altamente accurata nella diagnosi delle pavms , mostrando una sensibilit del 93% ed una specificit del 62% [ 33 ] , ed assai utile nella valutazione del decorso clinico dopo trattamento embolizzante [ 34 ]  . 
pertanto , quando una soluzione agitata di soluzione salina ( o di poligelina colloidale ) iniettata in una vena periferica di un soggetto sano il contrasto rapidamente visualizzato a livello di atrio destro e quindi dissipato e non visibile nel cuore sinistro dal momento che le microbolle di maggiori dimensioni ( > 8 m ) rimangono intrappolate nei capillari polmonari , mentre le microbolle pi piccole si dissolvono nel circolo polmonare [ 37 ]  . 
ra - rv , atrio e ventricolo destro ; la - lv , atrio e ventricolo sinistro . position of lesions in axial ct scans explains the greater accuracy ( 98% vs 60% ) of ct compared with dsa in detecting pavms , even though dsa is considered more appropriate for depicting the angioarchitecture of individual lesions [ 30 ]  . 
the possibility of obtaining high - quality angiographic reconstructions addresses the limitations of axial scans in identifying the course of pulmonary vessels , which may be variously oriented in space . 
although nonenhanced scans are generally sufficient to reach a diagnosis , in lesions larger than 10 mm in diameter , injection of contrast material can help confirm the vascular nature of the lesion by demonstrating the sequential increase in attenuation of the feeding artery , aneurysmal sac and draining vein [ 30 ]  . 
furthermore , the strong enhancement of the lesion after contrast injection , comparable with that of other vascular structures [ 41 ] , allows for a confident diagnosis . mri is considered less effective than ct or dsa for detecting pavms , above all , small pavms with high flow [ 23 ]  . 
in fact , the rapid blood flow results in an absent or minimal mri signal , known as a signal void , so the pavm may be indiscernible from the surrounding air - filled lung on se sequences [ 42 ]  . 
si tratta di una metodica quantitativa che valuta la presenza di shunt emodinamicamente significativi , ma il cui limite principale lassenza di informazioni qualitative circa il numero , le dimensioni , la localizzazione e langio - architettura delle lesioni . tridimensionale la tc , utilizzando apparecchiature dotate di tecnologia spirale multidetettore ( tcmd ) , in grado di fornire una ( 3d ) , multiplanare rappresentazione ( mpr ) e di tipo angiografico ( mip , vr ) di elevato dettaglio anatomico , anche se eseguita senza lutilizzo del mdc , ed fondamentale nella ricerca delle pavms e nella valutazione della loro morfologia [ 30 , 39 , 40 ]  . 
essa fornisce un quadro anatomico pi preciso rispetto ad altre modalit di imaging non invasivo ed ha assunto un ruolo complementare a quello dellangiografia nello studio pre - trattamento di tali malformazioni e fondamentale nel loro follow - up . 
lassenza di sovrapposizione di lesioni nelle scansioni tc assiali spiega la maggiore accuratezza ( 98% vs 60% ) della tc rispetto alla dsa nel riconoscimento delle pavms sebbene questultima metodica sia considerata pi appropriata per dimostrare langio - architettura della singola lesione [ 30 ]  . 
some parenchymal nodules with regular multilobulated margins are evident peripherally in the left upper lobe ( arrow ) , the middle lobe ( thick empty arrow ) and right lower lobe ( empty arrow )  . 
the feeding artery ( arrowhead ) and draining vein ( empty arrowhead ) are well appreciable in the 3d angiography detail ( f ) of the pavm of the left upper lobe ( arrow )  . 
in corrispondenza del lobo superiore sinistro ( freccia sottile piena ) , del lobo medio ( freccia vuota ) e del lobo inferiore destro ( freccia sottile vuota ) , in sede mantellare , sono evidenti dei noduli parenchimali a margini regolari e polilobati . 
nel particolare 3d - angio ( f ) della pavm del lobo superiore sinistro ( freccia sottile piena ) appaiono bene evidenti larteria afferente ( testa di freccia piena ) e la vena efferente ( testa di freccia vuota )  . 
according to their angiographic appearance , pavms are classified into simple or complex . tro quando le immagini assiali e le ricostruzioni angiografiche sono analizzate in concomitanza laccuratezza della tc nella caratterizzazione delle lesioni si accresce enormemente , passando dal 76% al 95% [ 40 ]  . alla tc la pavm pu apparire come un nodulo omogeneo , circoscritto e non calcificato , delle dimensioni anche di alcuni centimetri , o come una massa serpiginosa connessa ai vasi [ 30 ]  . 
sebbene le scansioni senza mezzo di contrasto siano generalmente sufficienti per arrivare ad una diagnosi , in caso di lesioni pi grandi di 10 mm di diametro , liniezione di mezzo di contrasto utile per accertare la natura vascolare della lesione polmonare in base alla dimostrazione dellincremento sequenziale di densit dellarteria afferente , del sacco aneurismatico e della vena efferente [ 30 ]  . 
inoltre il marcato incremento di densit della lesione dopo iniezione di mezzo di contrasto , comparabile a quello di altre strutture vascolari [ 41 ] , consente una diagnosi certa . la rm stata a lungo considerata meno efficace della tc e della dsa nel riconoscimento delle pavms , specialmente se piccole e ad alto flusso [ 23 ]  . 
computed tomography maximum intensity projection reconstruction in the sagittal plane ( a ) ; superselective digital subtraction angiography of the right pulmonary branch feeding the pavm ( b )  . 
larteriola afferente ( testa di freccia piena ) e la venula efferente ( testa di freccia vuota ) sono ben evidenti . completa corrispondenza tra i reperti riconoscibili nelle due indagini . simple pavms have a single feeding artery connected to a single draining vein via a nonseptate aneurysmal communication . 
the simple type is the most common type and occurs in 80% of cases [ 28 ]  . the main limitations of angiography are its laboriousness , invasiveness and cost , so its use should be limited to to vuoto di segnale , e pertanto una pavm pu non essere distinguibile dalladiacente parenchima polmonare pieno daria con le sequenze spin - echo [ 42 ]  . 
attualmente per , con lintroduzione di apparecchiature rm pi avanzate e lutilizzo della angio - rm con mezzo di contrasto ( cemr ) e in apnea [ 43 ] , diventato possibile diagnosticare tutte le pavms clinicamente significative . 
infatti , anche se in letteratura esistono pochi lavori riguardanti lutilizzo della rm nello studio del coinvolgimento polmonare in pazienti con hht , risultati preliminari indicano che langio - rm tridimensionale con gadolinio metodica utile e dotata di una buona sensibilit generale ( 78% ) ed elevata specificit ( 100% ) nella diagnosi di pavms ; la sensibilit raggiunge il 100% quando vengono considerate lesioni vascolari > 5 mm ed un diametro dellarteriola afferente > 3 mm [ 43 ]  . nonostante gli avanzamenti nelle metodiche di imaging non invasivo , comunque la dsa continua ad essere considerata il gold standard nella valutazione delle pavms prima della embolizzazione terapeutica o del trattamento chirurgico [ 23 ]  . 
gli shunt arterovenosi sono , al contrario , classificati come di tipo complesso , quando esistono comunicazioni tra multipli vasi afferenti ed efferenti con linterposizione di dilatazioni sacciformi spesso settate e suddivise in un reticolo di piccoli vasi . 
il tipo semplice il pi frequente e compare nell80% dei casi [ 28 ]  . il limite principale degli studi angiografici risiede nella loro laboriosit , invasivit e nel costo , cosicch il loro uso dovrebbe essere riservato a quei pazienti nei quali la presenza di pavms da sottoporre a trattamento endovascolare sia stata riconosciuta con le metodiche non invasive . numerosi protocolli di screening sono stati proposti per la ricerca di un eventuale coinvolgimento polmonare nei pazienti affetti da hht ed ulteriori ricerche sono necessarie per definire quale sia lapproccio diagnostico pi adeguato , considerando accuratezza , costo - beneficio ed utilit clinica . attualmente la mdc - ec , grazie alla sua eccellente sensibilit , superiore a quella dellossimetria e della dsa [ 44 , 45 ] , nonch alla facilit di esecuzione e disponibilit , pu essere considerata indagine proponibile nello screening iniziale . 
la mdc - ec non , comunque , una metodica qualitativa , pertanto il paziente che risulti positivo a tale esame deve essere avviato alla tc , che deve prevedere ricostruzioni mpr e 3d , e successivamente alla dsa in presenza di pavms suscettibili di trattamento endovascolare [ 46 ]  . 558 radiol med ( 2008 ) 113 : 547566 patients in whom noninvasive diagnostic tests have detected the presence of pavms requiring endovascular treatment . numerous screening protocols have been proposed for assessing pulmonary involvement in patients with hht , and further studies are required to identify the best approach in terms of accuracy , cost - effectiveness and clinical benefit . due to its excellent sensitivity ( higher than that of pulse oximetry and dsa [ 44 , 45 ] ) , ease of use and availability , ce can be considered the best initial screening test . 
ce is not , however , a qualitative method , so the patient with positive findings should be studied by ct with mpr and 3d reconstructions , followed by dsa whenever ct has identified significant pavms requiring endovascular treatment [ 46 ]  . 
although the hepatic vascular alterations associated with hht tend to be asymptomatic , some authors have reported severe complications , such as congestive cardiac failure , portal hypertension , portosystemic encephalopathy , cholangitis and atypical cirrhosis [ 4750 ]  . 
this explains why all hht patients should be screened for possible liver involvement . three types of shunts between the major hepatic vessels are possible [ 51 ] : arterioportal ( hepatic artery to portal vein ) , arteriosystemic ( hepatic artery to portal veins ) and portosystemic ( portal vein to hepatic veins or vena cava )  . intrahepatic arterioportal shunts consist of abnormal communications between the hepatic arteries and portal veins . 
although this type of shunt may occur in benign liver neoplasms or be the consequence of traumas or biopsy procedures , they are typically associated with cirrhosis and hepatocellular carcinoma ( hcc ) as a result of the tendency for this tumour to grow in the portal veins [ 51 ]  . 
in hht these shunts are congenital and represent the most common type of shunting , which may manifest in isolation or in association with arteriosystemic shunts [ 4 ]  . arteriosystemic shunts , abnormal communications between the hepatic arteries and hepatic veins , are rare and generally associated with benign or malignant liver neoplasms [ 51 ]  . 
in hht they are not an uncommon finding , occurring in 50%64% of cases , especially in association with arterioportal shunts [ 4 , 48 , 52 , 53 ]  . portosystemic shunts are frequent in patients with cirrhosis and are related to the increased portal pressure that causes the development of a myriad of extraand intrahepatic portosystemic anastomoses [ 4 , 50 ]  . 
only a few cases of spontaneous intrahepatic portosystemic shunts have been remalformazioni arterovenose epatiche il riconoscimento di fistole arterovenose intraparenchimali epatiche il reperto di pi comune riscontro in associazione con lhht . 
recentemente la loro ricerca sistematica nei pazienti con tale malattia ha evidenziato una frequenza , intorno al 75% , molto superiore , rispetto a quanto precedentemente segnalato in letteratura [ 4 ]  . 
sebbene le alterazioni vascolari epatiche correlate alla malattia siano generalmente asintomatiche , alcuni autori hanno riportato complicanze gravi quali scompenso cardiaco congestizio , ipertensione portale , encefalopatia portosistemica , colangite e cirrosi atipica [ 4750 ]  . 
questo spiega perch appare opportuno ricercare sempre nei pazienti affetti da tale malattia leventuale interessamento epatico . tra i maggiori distretti vascolari epatici sono possibili tre tipi di shunt [ 51 ] : arteroportali ( tra arteria epatica e vasi portali ) , arterosistemici ( tra arteria epatica e vene sovraepatiche ) , e portosistemici ( tra vasi portali e vasi sovraepatici o vena cava )  . gli shunts intraepatici arteroportali consistono in comunicazioni anomale tre arterie epatiche e vene portali . 
questo tipo di comunicazione si associa tipicamente alla cirrosi ed al carcinoma epatocellulare ( hcc ) , in rapporto alla tendenza di questa neoplasia a svilupparsi ed accrescersi nei vasi portali [ 51 ] , ma pu manifestarsi anche in associazione a neoplasie epatiche benigne o essere conseguenza di traumatismi o procedure bioptiche . 
nella hht questi shunts sono congeniti , rappresentano la forma pi comune e possono manifestarsi in forma isolata o in associazione a quelli arterosistemici [ 4 ]  . gli shunts arterosistemici , anomale comunicazioni tra arterie e vene epatiche , sono considerati rari e si associano , generalmente , alla presenza di neoplasie epatiche benigne o maligne [ 51 ]  . 
nei pazienti affetti da hht non rappresentano un reperto infrequente , potendosi riscontrare dal 50% al 64% dei casi , specie in associazione con quelli arteroportali [ 4 , 48 , 52 , 53 ]  . gli shunts portosistemici sono un reperto comune in pazienti affetti da cirrosi e sono correlati allincremento della pressione portale che provoca lo sviluppo di una miriade di anastomosi portosistemiche extraed intraepatiche [ 4 , 50 ]  . in letteratura sono riportati solo pochi casi della forma spontanea intraepatica e pochissimi quelli evidenziati in pazienti con hht [ 50 ]  . il gold standard per diagnosticare il coinvolgimento epatico nella hht considerata la dsa selettiva dellarteria epatica . 
con questo esame possibile dimostrare la dilatazione di tale arteria e la precoce opacizzazione dei rami venosi ( portali in caso di fistole arteroportali ed epatici in caso di fistole arterosistemiche ) [ 54 ]  . 
pi difficoltosa lidentificazione degli shunt portosistemici , specie nei soggetti in cui predominano shunt di tipo arterosistemico , sebbene i reperti angiografici di tale tipo di shunt siano stati descritti in letteratura e consistono nella diretta evidenziazione di una connessione tra vasi portali e venosi epatici o sistemici spesradiol med ( 2008 ) 113 : 547566 ported in the literature , and even fewer are those reported in patients with hht [ 50 ]  . the gold standard for diagnosing liver involvement in hht is selective dsa of the hepatic artery . 
this examination can demonstrate enlargement of the hepatic artery as well as the early opacification of venous branches ( portal in the case of arterioportal fistulas and hepatic in arteriosystemic fistulas ) [ 54 ]  . 
however , the angiographic features of such shunts have been described and consist of the direct visualisation of a communication between enlarged portal veins and hepatic or systemic veins [ 55 ]  . 
angiography is , moreover , an invasive and expensive procedure whose use should be limited to selected cases , especially in consideration of the fact that liver involvement is benign and asymptomatic in most cases [ 54 ]  . 
therefore , minimally invasive modalities such as us in association with cdus , ct and mri have assumed a central role in the visualisation of hepatic alterations [ 4 , 52 , 54 ]  . us and cdus have been proposed for screening hepatic vascular involvement because they are noninvasive , widely available and inexpensive , and they provide a qualitative and quantitative evaluation of the arterial , portal and venous flow [ 50 , 5658 ]  . major and minor sonographic criteria for liver involvement in hht have been proposed , though these were based on small series of patients [ 48 , 53 , 54 , 5764 ]  . 
dilatation of the common hepatic artery ( > 7 mm inner diameter ) and intrahepatic arterial hypervascularisation are the two major criteria , with 100% specificity , and a sensitivity of 100% and 88% , respectively [ 54 ]  . 
minor criteria are increased flow velocity in the hepatic artery ( > 110 cm / s ) and portal vein ( > 25 cm / s ) , resistance in the hepatic artery < 0.6 and tortuous course of the extrahepatic hepatic artery [ 54 ]  . 
inversion or pulsatility of the portal flow and the presence of a high - pressure arterial flow originating from the hepatic artery in the hepatic veins , leading to disruption of their normal cdus pattern of triphasic heartbeat - modulated waves , have been described in arterioportal and arteriosystemic shunts , respectively [ 53 , 54 , 58 ]  . 
the diagnosis of intraparenchymal portosystemic fistulas is based on direct visualisation of a dilated portal vein communicating directly with a hepatic vein [ 62 ]  . the high accuracy of the major criteria for detecting intrahepatic shunts has led some authors to consider cdus sufficient for a diagnosis in asymptomatic subjects , with more invasive tests , such as ct , mri or dsa being reserved for symptomatic subjects [ 53 ]  . 
langiografia , inoltre , un esame invasivo e costoso , per cui il suo impiego pu essere riservato a casi selezionati , specie in considerazione del fatto che il coinvolgimento epatico nella maggior parte dei casi benigno ed asintomatico [ 54 ]  . 
la dilatazione dellarteria epatica comune ( > 7 mm di diametro interno ) e lipervascolarizzazione arteriosa intraepatica rappresentano i due criteri ecografici maggiori , con specificit del 100% e sensibilit del 100% e del 88% rispettivamente [ 54 ]  . 
i criteri minori sono lincremento della velocit di flusso nellarteria epatica ( > 110 cm / s ) e nella vena porta ( > 25 cm / s ) , una resistenza nellarteria epatica < 0 , 6 e il decorso tortuoso del tratto extraepatico dellarteria epatica [ 54 ]  . 
linversione o la pulsatilit del flusso portale e la presenza nelle vene sovraepatiche di un flusso arterioso ad alta pressione ad origine dallarteria epatica , con conseguente alterazione del loro pattern cdus normalmente caratterizzato da onde trifasiche modulate dal battito cardiaco , sono descritti in associazione a shunt arteroportali e arterosistemici , rispettivamente [ 53 , 54 , 58 ]  . 
reperti considerati non significativi sono la dilatazione della vena porta ( > 13 mm ) e delle vene sovraepatiche ( > 11 mm ) , lepatomegalia e i margini nodulari . 
lidentificazione di fistole portosistemiche intraparenchimali si basa sulla identificazione diretta di un vaso portale dilatato in diretta comunicazione con una vena sovraepatica [ 62 ]  . la elevata accuratezza dei criteri maggiori nellidentificazione di shunt intraepatici fanno ritenere , secondo alcuni , il cdus sufficiente per la diagnosi in soggetti asintomatici , mentre esami pi invasivi , quali la tc , la rm o la dsa dovrebbero essere riservati ai soggetti sintomatici [ 53 ]  . 
la visualizzazione delle alterazioni vascolari epatiche con le vecchie apparecchiature tc convenzionali o rm era inusuale poich tali alterazioni sono correlate a fenomeni di modificazione dellemodinamica epatica riconoscibili esclusivamente nelle fasi precoci dellenhancement vascolare . 
la tc riconosciuta quale valido strumento per diagnosticare il coinvolgimento epatico e sono ormai codificati il ruolo e le modalit di esecuzione dello studio multifasico del fegato , che prevede lacquisizione delle 560 radiol med ( 2008 ) 113 : 547566 fig . 
early arterial phase ( a , d ) : simultaneous opacification of left portal branches ( white arrowheads ) and hepatic artery ( black arrowheads ) with no opacification of the main portal vein ( arrow ) and its left branch ( empty arrow )  . 
late arterial phase ( b , e ) : the opacification of left portal branches persists and the main portal vascular district ( arrow and empty arrow ) becomes more visible . 
scansioni tc assiali su due differenti livelli : fase arteriosa precoce ( a , d ) : evidente la simultanea opacizzazione dei rami portali di sinistra ( teste di freccia bianche ) e dellarteria epatica ( teste di freccia nera ) in assenza di opacizzazione del tronco portale principale ( freccia piena ) e del suo ramo sinistro ( freccia vuota )  . 
fase arteriosa tardiva ( b , e ) : persiste lopacizzazione di rami portali di sinistra ed inizia la visualizzazione del distretto portale principale ( freccia piena e freccia vuota )  . 
fase portale ( c , f ) : i distretti vascolari portale ( teste di freccia bianche , freccia piena e freccia vuota ) e venoso ( teste di freccia vuote ) sono ben opacizzati . unusual because the changes are related to hepatic haemodynamic phenomena that can only be appreciated in the early phases of vascular enhancement . 
the role , examination protocol consisting of an early and delayed arterial phase and a portal phase and significant findings for identifying the typical hepatic vascular malformations of hht and differentiating the various types of shunts have been standardised [ 4 ]  . 
on the other hand , few studies have investigated the use of mri in these patients , even though the opportunities offered by the fast modern scanners and the use of contrast material have provided diagnostic findings comparable to those of ct [ 65 ]  . on multiphase mdct and dynamic mri , the diagnosis of arterioportal shunts relies on indirect signs , and particularly on the early , prolonged enhancement of the portal vessels during the early arterial phase . 
as scansioni in una doppia fase arteriosa , precoce e tardiva , ed in fase portale , nonch i reperti significativi per identificare le alterazioni vascolari epatiche tipiche dellhht e per differenziare le varie forme di shunt [ 4 ]  . 
in maniera analoga ad altri tipi di shunts arteroportali non associati a masse neoplastiche questo tipo di shunt tipicamente periferico o sottocapsulare . la presenza di unarteria epatica tortuosa e dilatata ( diametro > 7 mm ) e di una vena porta dilatata ( diametro > 13 mm ) , spesso associata a circoli collaterali e splenoradiol med ( 2008 ) 113 : 547566 fig . 
computed tomography with coronal maximum intensity projection reconstructions on different levels in the early arterial phase ( a , d ) , the late arterial phase ( b , e ) and the portal phase ( c , f )  . 
the early venous drainage with the simultaneous opacification of the right and inferior hepatic veins ( empty arrowheads ) and the hepatic artery ( black arrowheads ) is evident during both arterial phases . 
the hepatic parenchyma is inhomogeneous due to the presence of several millimetric hypervascular images , related to telangiectases , and of a large area of transient hepatic parenchymal enhancement ( thpe ) ( * ) of the sixth segment . 
visualizzazione in entrambe le fasi arteriose del precoce drenaggio venoso con contemporanea opacizzazione delle vene sovraepatiche destra e inferiore ( teste di freccia vuote ) e dellarteria epatica ( teste di freccia nere )  . 
il parenchima appare disomogeneo per la presenza di numerose multiple immagini puntiformi ipervascolarizzate , di pochi millimetri di diametro , riferibili a telangiectasie e di una estesa area di arterializzazione parenchimale ( transient hepatic parenchymal enhancement , thpe ) ( * ) a livello del vi segmento . 
in fase portale ( c , f ) tali disomogeneit parenchimali non sono pi evidenti . with other types of nontumoural arterioportal shunts , these shunts are typically peripheral or subcapsular . further common ct findings in this type of shunt are a tortuous and dilated hepatic artery ( diameter > 7 mm ) and a dilated portal vein ( diameter > 13 mm ) , often associated with collateral circulations and splenomegaly ( longitudinal spleen diameter > 130 mm ) [ 7 ]  . 
the latter findings may be suggestive of portal hypertension , which should , however , also be confirmed clinically or through the direct measurement of portal pressure [ 4 , 65 ]  . arteriosystemic shunts may occur as an isolated finding or more frequently in association with arterioportal shunts . again , multiphasic ct and dynamic mri provide only indirect signs for the detection of these shunts . 
a severe complication of these intrahepatic left - to - right shunts is high - output cardiac failure . ct and mri diagnosis of intrahepatic portosystemic shunts is still a challenge . 
in fact , whereas it is easy to distinguish the early and late arterial phases from the portal - venous phase with a fast multiphasic study , it is difficult megalia ( diametro splenico longitudinale > 130 mm ) , sono altri reperti tc comuni nei pazienti con tale tipo di shunt [ 7 ]  . 
tali shunt sinistro - destro intraepatici , per lalto flusso che generano , possono determinare come complicanza severa la comparsa di uno scompenso cardiaco . la diagnosi tc e rm di shunts portosistemici intraepatici rimane pi difficoltosa . 
mentre , infatti , semplice distinguere le fasi arteriose precoce e tardiva da quella porto - venosa attraverso un veloce studio multifasico , difficile separare chiaramente le fasi portale pura da quella venosa . pertanto lunico reperto tc la visualizzazione diretta durante la fase porto - venosa di vasi portali dilatati in comunicazione con vene epatiche o sistemiche anchesse dilatate . 562 radiol med ( 2008 ) 113 : 547566 fig . 
dynamic contrastenhanced magnetic resonance imaging , coronal maximum intensity projection reconstruction : time t = 0 from the arrival of the contrast bolus in the aorta ( a ) , time t = 5 s ( b ) , time t = 10 s ( c ) and time t = 15 s ( d )  . 
the hepatic parenchyma is diffusely inhomogeneous due to the presence of several millimetric hypervascular images , related to telangiectases ( arrowheads ) , and a transient hepatic parenchymal enhancement ( thpe ) ( * )  . 
il parenchima epatico appare diffusamente disomogeneo per la presenza di numerose immagini puntiformi ipervascolarizzate , di pochi millimetri di diametro , riferibili a telangiectasie ( punte di freccia ) , e di una area di arterializzazione parenchimale ( transient hepatic parenchymal enhancement , thpe ) ( * )  . 
arteria epatica ( freccia ) e tronco portale ( freccia vuota )  . to clearly separate the portal phase from the venous phase . thus , the only ct sign is the direct visualisation , during the portal - venous phase , of dilated portal veins communicating with hepatic or systemic veins , which are also enlarged . sometimes , the communication appears as a dilated paraumbilical vein with a intrahepatic course [ 66 ]  . 
 intrahepatic perfusion disorders , in the form of transient hepatic parenchymal enhancement ( thpe ) , are frequent in hht patients and are often associated with the presence of arterioportal shunts , of which they may represent a further indirect sign [ 4 ]  . 
sometimes , they exhibit rounded or pseudorounded shape and may not be discernible from other lesions , especially small foci of hepatocellular carcinoma ( hhc ) [ 52 ]  . disorders of angiogenesis control mechanisms , typical of hht , may account for the finding of other intraparenchymal vascular abnormalities appearing as pseudolesions , such as telangiectases and large confluent vascular masses ( lcvms ) [ 4 , 52 ]  . 
 disordini perfusivi intraepatici , che si manifestano sotto forma di differenze transitorie nellattenuazione / intensit epatica ( transient hepatic parenchymal enhancement , thpe ) , sono frequenti nei pazienti con hht e sono spesso associati alla presenza di shunts arteroportali rappresentandone , talora , un ulteriore segno indiretto [ 4 ]  . 
talvolta esse presentano una morfologia rotondeggiante o pseudorotondeggiante non facilmente distinguibile da altre patologie , soprattutto piccoli foci di hcc [ 52 ]  . i disordini nei meccanismi di controllo dellangiogenesi , tipici dellhht , possono spiegare la comparsa di altre anomalie vascolari intraparenchimali che possono assumere aspetti di pseudo - lesioni , come telangiectasie e larghe masse vascolari confluenti ( lcvms ) [ 4 , 52 ]  . 
during the arterial phases , the hepatic parenchyma is disseminated with several millimetric hypervascular images , referring to telangiectases , that are no longer evident during the portal phase ( c )  . 
a strongly enhancing subcapsular area with irregular shape , relating to an area of transient hepatic parenchymal enhancement ( thpe ) ( * ) , is evident in the seventh segment . 
il parenchima epatico nelle fasi arteriose appare disseminato di multiple immagini puntiformi ipervascolarizzate di pochi millimetri di diametro riferibili a telangiectasie , non pi evidenti nella fase portale ( c )  . 
in sede subcapsulare , in corrispondenza del vii segmento , evidente unarea a morfologia irregolare ed elevato enhancement ( * ) , riferibile ad una area di arterializzazione parenchimale ( transient hepatic parenchymal enhancement , thpe )  . 
modern techniques allow rapid and accurate depiction of cerebral , pulmonary and hepatic alterations , providing valuable tools for prognostic assessment and treatment planning . us combined with colour - doppler imaging , in part thanks to advances in sonographic contrast media , appears to constitute the best modality to screen patients for hepatic and pulmonary fistulas and can provide useful information lari caratterizzati , dopo liniezione del mdc , da un incremento di densit precoce e persistente durante le fasi arteriose . 
le moderne metodiche consentono una rapida e precisa visualizzazione delle alterazioni cerebrali , polmonari ed epatiche , fondamentale nella valutazione prognostica e nella impostazione terapeutica di tali pazienti . gli us in associazione col color doppler e grazie ai miglioramenti nel campo dei mezzi di contrasto sembrano essere la migliore modalit di screening nella ricerca delle fistole epatiche e polmonari e possono fornire utili informazioni sul decorso clinico dopo trattamento embolizzante delle pavms . 564 radiol med ( 2008 ) 113 : 547566 on clinical outcome after embolotherapy of pavms . ct and mri , with their high - quality , 3d angiographic reconstructions , are the most accurate modalities for the morphological study of lesions , and they have replaced angiography as a diagnostic procedure . 
qualitative ct evaluation included the following parameters : ( a ) location ; ( b ) tumor edges ; ( c ) necrosis ; ( d ) pleural effusion ; ( e ) metastases ; ( f ) chest wall infiltration ; ( g ) tumor margins . 
qta included evaluation of mean ( m ) , standard deviation ( sd ) , kurtosis ( k ) , skewness ( s ) , entropy ( e ) , shape from texture ( tx_sigma ) and average of positive pixels ( mpp )  . 
pearsonrho test was used to evaluate the relationship of continuous non - dichotomic parameters , whereas mannwhitney test was used for dichotomic parameters . results histological evaluation demonstrated thymoma in 12 cases and thymic carcinoma in 4 cases . 
this approach has been recently applied to various tumors , such as glioblastoma [ 24 ] , clear - cell renal carcinoma [ 5 , 6 ] , breast , rectal and lung adenocarcinoma [ 711 ]  . 
recent studies also demonstrated how quantitative texture analysis ( qta ) may be used to complement conventional imaging features [ 1217 ] ; however , further investigations are needed to deepen the knowledge on the relationship between radiological and biological phenotypes and to enlarge the role of radiomics in clinical practice . 
the last national cancer institute ( nci ) workshop report [ 1 ] proposed several fields of application vol . : ( 0123456789 ) 1 3 346 la radiologia medica ( 2018 ) 123 : 345350 for radiomics , identifying lung ct as the first research area in the priority list , but even less common lesions , such as thymic tumors , can represent interesting fields of application . 
the primary objective of this study was to evaluate the potential relationship between ct features , qta data , histologic grading and tumor staging in patients with thymic tumors [ 18 ] ; secondly , we assessed the ability of ct and qta to predict the development of a myasthenic syndrome and serological positivity of anti - achr antibodies . image analysis two radiologists with 8years and 2years of experience in chest ct , blinded to personal , clinical and histological data , independently performed a qualitative evaluation of the images . 
qta was performed by a third independent radiologist with 3years of experience in advanced oncologic imaging . materials andmethods qualitative evaluation patient population this retrospective study received local institutional review board approval ; informed consent was obtained for all patients or relatives . 
data from sixteen patients affected by thymic neoplasm were retrospectively retrieved from our local clinical database , according to the following inclusion criteria : ( a ) histologic diagnosis of thymic tumor obtained with percutaneous image - guided biopsy , mediastinoscopy or surgery ; ( b ) tumor classification according to who and masaoka systems ; ( c ) ct scan data available for qualitative and qta analysis ; ( d ) no previous chemotherapy or radiation therapy ; and ( e ) available clinical information including data on potential myasthenic syndrome and anti - achr antibodies . ct scan protocol all ct scans were performed with a 64 - slice ct scanner ( somatom definition , siemens , forchheimgermany ) before and after intravenous administration of iodinated contrast agent ( 0.2mg / kg of iomeron 400mgi / mlbracco spaitaly ) in the venous phase ( 60s delay after contrast injection )  . 
regions of interest ( rois ) were manually delineated around the thymic tumor on axial contrastenhanced ct images , enclosing only tumor tissue [ 17 , 19 ] as previously described . 
the in - plane filtration step utilized a laplacian of gaussian spatial band - pass filter to produce a series of derived images highlighting features at different anatomic spatial scales varying from fine texture ( ssf2 , 2mm in radius ) , medium texture ( ssf3 , 3mm in radius ) and coarse texture ( ssf4 , 4mm in radius )  . 
1 roi positioning on cect and texture elaboration with different spatial scale filter ( ssf ) : fine texture , medium texture and coarse texture 1 3 la radiologia medica ( 2018 ) 123 : 345350 mean ( m ) , which measures the average brightness in selected pixels . standard deviation ( sd ) , which measures variation or dispersion that exists from the mean . kurtosis ( k ) : from the greek kyrtosis , convexity , which measures peakedness and tailedness inversely related to the number of features highlighted ( whether bright or dark ) ; it increases by intensity variations in highlighted features . skewness ( s ) , which measures asymmetry in pixel distribution related to the average brightness of the highlighted features ( predominantly bright features give positive values , predominantly dark objects give negative values ) ; it tends to zero with increasing number of features highlighted and moves away from zero with density variation in highlighted features . entropy ( e ) , which measures texture irregularity in terms of randomness of gray - levels distribution inside the roi . shape from texture ( tx_sigma ) : parameter dealing with information on the geometric surface of the lesion . mpp , average of positive pixels . i : 3 patients ; masaoka ii : 7 patients ; masaoka iii : 2 patients ; masaoka iv : 4 patients . 
myasthenic syndrome was present in 7 out of 16 patients ( 5 who b2 , 1 b3 and 1 c ) , with 6 of them being positive for anti - achr antibodies ; among the remaining 9 patients , one was positive for anti - achr antibodies . qualitative analysis tumor location was in the upper mediastinum in 13 cases and lower mediastinum in 3 cases lesion . 
due to the small sample size included in this preliminary study , necrosis was the only parameter which could be analyzed for relationship with the qta data using the mannwhitney test , ( table1 )  . statistical analysis quantitative analysis in this study , the normality of each continuous variable group was tested using the kolmogorovsmirnov z test . 
4 relationship data between qta and lesion size discussion the objective of this study was to evaluate the potential relationship of qta with several clinical and imaging parameters in patients with thymic neoplasthe identification of these relationships could derive noninvasive prognostic information before treatment and predict the occurrence of certain clinical scenarios , with possible impact on treatment decisions and patient management . 
qualitative imaging features may represent immediate tools , potentially useful for the radiologist during reporting ; unfortunately , in this preliminary study , the small number of patients enrolled allowed only a partial analysis , concerning only one qualitative parameter ( necrosis )  . 
in particular , the association between necrosis and qta parameters , such as kurtosis and skewness , was expected , since these two parameters represent the lack of homogeneity of the pixels and the deviation from normality , respectively . 
in any case , the finding of significant associations in this preliminary analysis looks promising ; in the next future , a more extensive analysis including a higher number of patients and ct features is likely to reveal further associations . 
on the other hand , several significant relationships were demonstrated between qta parameters , classification systems used for thymic lesions ( who and masaoka ) , tumor size and clinical condition ; these associations can be explained basing on intrinsic features of tumors ; for example , basing on entropy , whose values increase as size increases , we can infer that larger tumors have a less homogeneous pixel distribution ; this observation is confirmed by the trend of mpp , which decreases with increasing tumor size , indicating a more homogeneous appearance in smaller tumors . 
these associations , particularly between qta data and classification systems , seem also to indirectly suggest a relationship with prognosis , since these classifications have prognostic significance , especially the masaoka system , already validated as independent prognostic factor [ 18 ]  . 
even in this case , the enrollment of more patients in a further study could allow a survival analysis , with the aim to assess the presence of an effective direct relationship between qta parameters and clinical outcome . 
the relationship between qta parameters and histology also represents an incentive for further studies , with the aim to correlate phenotypic and genotypic features of the tumor , as already done for other cancers , such as glioblastoma multiforme or lung adenocarcinoma . 
furthermore , the ability to differentiate different components of the tumor through imaging analysis could also encourage the use of these techniques of radiomics and quantitative analysis as biopsy guidance , in order to identify the most suitable areas of the tumor to be sampled . 
for each patient , the epicardial contour of the single ventricle was manually segmented on cine images by two readers and an automated bt algorithm was independently applied to calculate end - diastolic volume ( edv ) , end - systolic volume ( esv ) , stroke volume ( sv ) , ejection fraction ( ef ) , and cardiac mass ( cm )  . 
 constant advances in cardiac magnetic resonance ( cmr ) techniques and equipment in the last decade now grant adequate anatomical detail in addition to the accurate and not operator - dependent functional assessment of ventricular chambers ( main and accessory ) , cardiac valves , and intraor extracardiac shunts and conduits . 
in addition , contrast - enhanced cmr could allowthe detection of the myocardial fibrotic evolution , an evaluation still not clinically feasible with computed tomography [ 11 ]  . non - invasive imaging techniques play a major role in the follow - up of patients with fc . 
in particular , cmr is emerging as the leading modality for pre - / post - surgical assessment of congenital heart disease ( chd ) as well as for early diagnosis of cardiac and systemic complications , clarifying cardiovascular anatomy and physiology [ 7 , 1215 ]  . 
several studies have progressively asserted the correlation between the prognosis of patients with fc and their ventricular size and function calculated with analysis and segmentation of cmr images , showing it to be equally or more accurate than echocardiographic assessment and distinctly more reproducible [ 8 , 16 , 17 ]  . in literature , there is limited experience regarding the volume analysis of fc patients . 
a study [ 18 ] showed that the inclusion of the hypoplastic chamber during the segmentation of cine images of fc patients has no effect on the quantification of cardiac volumes , but may result in a less accurate measurement of the ejection fraction . the aim of our study is to validate the blood - threshold ( bt ) segmentation algorithm in cmr cine images for the evaluation of cardiac function in patients with fuh . materials andmethods study population the ethics committee approval was obtained for this retrospective study ( ethics committee of the university la radiologia medica ( 2018 ) 123 : 331337 hospital san raffaele ; protocol code uh_01 ; approved on july 14th , 2016 )  . 
 the inclusion criteria for the re - assessment of the images were : ( 1 ) complete acquisition of cardiac volume with cine images ; ( 2 ) acquisition of through - plane images of flow in the ascending aorta ; and ( 3 ) the absence of atrialventricular valve insufficiency.therefore , 15 examinations were excluded , and a total of 55 examinations , belonging to 44 patients ( 7 patients were scanned 2 times and 2 patients 3 times ) , were included . 
in case of repeated examinations on the same patient , the time interval was at least 12months . the 44 patients included 30 males and 14 females , with a mean ageand its corresponding standard deviation ( sd ) at the first examination of 258years ( mean standard deviation , sd )  . 
the youngest patient was 7 - year - old at the time of examination , and the oldest patient was 41 - year - old . image acquisition all cmr examinations were performed with a 1.5 - t unit ( magnetom sonata maestro class or magnetom aera , siemens medical solutions ) with 40or 45 - mt / m gradient power , respectively , using a 4or 18 - channel surface phased - array coil placed over the thorax and with the patient in a supine position . 
thus , the blood - threshold technique ( mass - k mode ) was applied using a 50% bt and the end - diastolic volume index ( edvi ) , end - systolic volume index ( esvi ) , stroke volume ( sv ) , ejection fraction ( ef ) , and cardiac mass values were calculated in a totally automated way . for the segmentation of flow images of the ascending aorta , in each session each oneof the two readers positioned a region of interest on the vessel boundary of a selected slice . 
subsequently , each reader propagated the segmentation through the remaining slices , the software proposed an automated adjustment , and the reader was allowed to manually correct the adjusted contours . 
for each session , forward flow and backward flow measurements were obtained . statistical analysis data were reported as meansd or median and interquartile range ( iqr ) according to normal distribution or nonnormal distribution , respectively . the wilcoxon test and spearman correlation were used to compare and correlate the median value of sv and aortic forward flow , respectively . the blandaltman method was used to estimate the intra and inter - reader reproducibility . 
the intra - reader reproducibility was performed only for r1 with at least a 10 - day interval between the two sessions . the coefficient of repeatability ( cor ) was calculated as 1.96 sd of differences of the two datasets . 
bias ( mean of the differences of the two datasets ) and 95% limits of agreement ( bias2 sd ) were plotted as well . results the image analysis was feasible in all patients and no artifacts prevented readers from performing the segmentation . 
we found no significant difference ( p = 0.123 ) , but a significant correlation ( r = 0.789 , p < 0.001 ) between mean sv and aortic forward flow . 
all ventricle and aortic functional parameters are shown in table1 . the bias between the sv values measured by r1 was 0.12ml , accompanied by a cor of 8.1ml , corresponding to an intra - reader reproducibility of 86% . 
 an example of segmentation of cinecmr images with the bt technique is shown in fig.3. discussion in cmr , ventricular volume and function assessment is achieved through the segmentation of cine images . 
this post - processing technique , initially exclusively manually performed by trained readers , implies the recognition of the difference between the blood pool in the ventricular cavity , of other anatomical structures normally in the ventricular chamber such as trabeculae and papillary muscles ( tpm ) as well as of the ventricular walls . 
1 blandaltman plot for intra - reader reproducibility of stroke volume measurement ( a ) ; blandaltman plot for aortic forward flow measurement ( b ) la radiologia medica ( 2018 ) 123 : 331337 analysis , to obtain a proper estimate of the ventricular volume and mass with minimal manual input [ 2225 ]  . 
in this technique , after the reader has manually traced only the epicardial contours on the end - systolic and enddiastolic phases of the cine images , the software calculates a blood percentage for each pixel inside the contoured area , considering the different signal intensity of the blood and myocardiuafter visual inspection , the reader can freely alter , in any slice and phase , the default bt value of signal intensity discrimination . 
moreover , semi - automated detection of the epicardial margin can be used , requiring only small manual adjustments on good quality images , further curtailing the time required for the post - processing stage [ 29 ]  . 1 3 la radiologia medica ( 2018 ) 123 : 331337 fig . 
2 blandaltman plot for inter - reader reproducibility of stroke volume measurement ( a ) ; blandaltman plot for aortic forward flow measurement ( b ) the mass - k mode algorithm has been validated for clinical routine application , showing both accurate and reproducible evaluation of ventricular mass and volume and reduced time of analysis , by jaspers etal . 
 [ 25 ] on 137 patients with a broad range of cardiac diseases not including chd . the results of our study validate the use of this bt technique in patients with an abnormal cardiac anatomy , such as the one that is found in patients with fc . 
in the absence of other reference tools to validate ventricular volume assessments , we choose to use aortic flow measurements as an independent benchmark for sv , since previous studies showed it to be a solid and reproducible standard . 
b , d , f the same images after manual epicardial volume analysis with blood - threshold mode activation based on a single - center historical series of fc patients ; however , fuv patients are a very small population and usually referred to a single center . 
second , it is possible that , due to the retrospective design of our study , even small differences in the acquisition parameters , reasonably likely to happen in the absence of astandardized cmr acquisition protocol , may have negatively influenced the quality of cine images and therefore the performance of the bt technique . 
finally , we should consider the possibility of obtaining the same volume analysis with different softwares ; this new function could be integrated in future softwares to be used in fuh patients . to summarize , we successfully validated the use of a bt technique for the segmentation of cine images in patients with fc . 
we observed a high intraand interreader reproducibility for the assessment of ventricular sv and excellent agreement with aortic flow values used as a benchmark . funding this study was supported by local research funds of the irccs policlinico san donato , a clinical research hospital partially funded by the italian ministry of health . compliance with ethical standards ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . ethical approval the ethical committee of irccs ospedale san raffaele approved the protocol uh_01 on july 14 , 2016 . 
the final size change of the hemangioma was categorized into three groups compared with the initial diameter ( increased , > 120% ; no change , 80120% ; decreased , < 80% )  . results among the 101 hemangiomas , 32 lesions ( 31.7% ) were enlarged and 21 lesions ( 20.8% ) were shrunken during intervals of 60157 ( median , 81 ) months . 
only a minor proportion ( 1% , n = 1 ) of the lesions showed size fluctuation during follow - up . conclusion during the long - term ( 513years ) follow - up , about 50% of the hepatic hemangiomas were enlarged or shrunken to > 20% of the initial diameter . 
aside from the cirrhosis and aging factors , the size changes seemed sporadic . keywords hepatic hemangioma interval change computed tomography magnetic resonance imaging liver cirrhosis introduction hepatic hemangioma is one of the most common benign lesions of the liver , detected in 0.420% of cases in autopsy series [ 1 , 2 ]  . 
once a hepatic * jeong - sik yu yjsrad97@yuhs.ac 1 department ofradiology , gangnam severance hospital , yonsei university college ofmedicine , 211 eonju - ro , gangnam - gu , seoul06273 , southkorea hemangioma is properly diagnosed , it rarely causes problems in the future management of the disease . 
some hemangiomas have been incidentally recognized during modern health - care programs or serial imaging studies for the follow - up of other diseases , and the natural history of hepatic hemangioma was recently reported considering the surgical management depending on the speed of tumor growth [ 3 , 4 ]  . 
the studies found that nearly half of the hemangiomas increased in size by up to 2mm / year during a mean followup period of 3.7years [ 3 ] , and that the growth rate decreased rapidly when the diameter of the lesions became > 10cm or in patients older than 50years during a median follow - up period of 4years , obviating the need for preventive treatment even in patients with large lesions [ 4 ]  . meanwhile , several prior studies reported that hepatic hemangiomas tended to enlarge during pregnancy or vol . : ( 0123456789 ) 1 3 324 la radiologia medica ( 2018 ) 123 : 323330 estrogen treatment , suggesting a role for female sex hormones in hemangioma growth [ 5 , 6 ]  . 
this study was conducted to investigate the long - term changes of hepatic hemangiomas during a follow - up period of > 5years , and to determine the intrinsic or extrinsic determinants for the size changes of hepatic hemangiomas . as pseudo - washout appearance on mri using liver - specific contrast agent present study [ 12 ]  . 
the size of the lesions was also checked for the remaining 129 patients in the imaging reports , and 19 patients having only tiny ( < 6mm ) lesions on the initial and follow - up images were also excluded owing to the difficulty of recognizing the typical findings of hemangiomas . 
during the review of imaging features , two patients who underwent liver transplantation and partial hepatectomy were also excluded because the involved segments of the liver containing the hemangioma were resected . 
 seven patients who underwent transarterial chemoembolization for the treatment of hepatocellular carcinomas after the initial study were also excluded because of the possible compromise of the supplying hepatic artery branches . 
 the medical records of underlying diseases and drug history were available for all patients . materials andmethods imaging protocols precontrast and postcontrast ct examinations were performed with one of two scanners : a 16 - slice or a 64 - slice multidetector ct scanner ( somatom sensation 16 or somatom sensation 64 ; siemens medical solutions , erlangen , germany )  . 
 for dynamic ct , the average start times for the arterial and portal venous phases were 34 ( 3038s ) and 70s , respectively , after the initiation of contrast medium injection . 
in the non - dynamic imaging patients research approval was obtained from the institutional review board of our hospital , and the requirement for informed consent was waived for this retrospective study . 
 from january 2006 to december 2010 , a total of 1115 consecutive patients were recognized to have suggestive features of hepatic hemangiomas on contrast - enhanced computed tomography ( ct ) or magnetic resonance imaging ( mri ) at our institution . 
on the picture archiving and communication system ( pacs ) , patients having one or more prior or further follow - up ct or mri examinations with an interval of > 5years were sorted ( n = 136 )  . 
hepatic hemangiomas were diagnosed with the use of the combination of pre - established typical imaging features , including the gradually centripetal globular enhancement during the multiphasic dynamic imaging with sustaining enhancement on delayed phase similar to the intrahepatic vasculature on ct or mri . 
at mr imaging , a lesion was considered to be a hemangioma if it was well - demarcated and notably hyperintense on t2 - weighted fast spin - echo images in addition to the dynamic imaging features [ 10 ]  . 
for small lesions with early strong enhancement of entire lesion , the presence of arterioportal shunts combined with the typical imaging features in the delayed phase images and t2 - weighted mri were helpful in the imaging diagnosis of hemangiomas [ 11 ]  . 
moreover , all of the subjected lesions have very long - term follow - up imaging data that confirmed the benignity of the lesions even in the patients showing atypical postcontrast imaging features such fig . 
enlarged , not - changed , and shrunken lesions were defined as the final diameter larger than 120 , 80120% , and < 80% of the initial diameter , respectively 1 3 la radiologia medica ( 2018 ) 123 : 323330 protocol of single - phase ct , the postcontrast scan was performed at the timing around the portal venous phase . mri was performed using 1.5 - t systems ( magnetom vision or avanto ; siemens , erlangen , germany )  . 
after acquiring localizer images in the supine position , spectrally fat - suppressed breath - hold t2 - weighted turbo spin echo images or half - fourier single - shot turbo spin - echo images were acquired on the axial plane . 
after a double - echo chemical shift gradient - echo technique for opposedand in - phase images was performed , contrast - enhanced imaging was done using three - dimensional gradient - echo sequences on the axial plane during about 20 - s breath - holding periods . 
the dynamic series consisted of one precontrast scan followed by three sequential postcontrast series ( early arterial , late arterial , and portal phase ) with 34 - s intervals ( 20s for image acquisition with breath holding and 14s for re - breathing )  . 
 the postcontrast series were performed after a bolus injection of gadopentetate dimeglumine ( 0.1mmol / kg ) ( magnevist ; bayer healthcare , berlin , germany ) or gadoxetic acid disodium ( 0.1ml / kg ) ( primovist ; bayer healthcare , berlin , germany ) at a rate of 2 or 1ml / s , respectively , followed by a saline flush using a power injector . 
delayed phase images were acquired at 5min , and hepatobiliary phase images were obtained additionally at 20min for the patients using gadoxetic acid disodium , respectively , after the contrast agent injection . 
as our institution is a tertiary referral hospital , there were numerous imaging data from other institutions , and those images were also used for data analysis if the digital image was available for lesion comparison on pacs . data analysis two radiologists ( one with 10 years experience with abdominal imaging and the other a second - year radiology resident ) reviewed the images independently and recorded the size of each hepatic hemangioma . 
the selection of imaging slices and the contrast - enhanced phase depended on the largest lesion diameter and the most conspicuous lesion - to - liver contrast in each patient , regardless of the enhancement pattern of the lesion . 
if the measured values differed by 3mm for the same lesion in the same imaging session between the two radiologists , the size was measured again during a conference to minimize the measurement error . 
the change in size was categorized into three groups : enlarged , with a final size > 120% of the initial size ; not - changed , with a final size 80120% of the initial size ; shrunken , with a final size < 80% of the initial size . 
furthermore , imaging data on the closest to the median date between the initial and final examinations were also reviewed to reveal possible fluctuations in size . the study coordinator ( 20years experience of abdominal imaging ) recorded the background hepatic condition of each case to determine the underlying liver problethe presence of liver cirrhosis was determined according to relevant hepatic contour changes and portal hypertensive stigmata in the imaging studies , in addition to the patients medical records . 
hepatic steatosis was defined as the liver showing lower attenuation than that of the spleen on nonenhanced ct based on rather specific criteria ( liverspleen , < 1 hounsfield unit ) [ 13 ]  . 
the medical records of all cases were reviewed for medication history , including steroids , female hormones , and chemotherapy for controlling malignancy . statistical analysis the relationship between the initial diameter and size change ratio ( the final diameter divided by the initial diameter ) was estimated by pearson correlation test . 
to determine the relationship between the age of the patients and the size change of the lesions , a correlation coefficient between the age of the patients and the diameter change ratio of the lesions was also calculated . 
all statistical analyses were performed with spss statistics version 23 ( ibm corp . , armonk , ny , usa )  . results of the 101 patients , 15 patients had underlying cirrhosis and 29 patients had fatty liver . 
of the 26 patients with chemotherapy for various malignancies , 24 patients used at least one antiangiogenic agent , while two patients had only chemotherapeutic agents without antiangiogenic effects ( table1 )  . 
 the mean ages of the three patient groups according to size change were 47.3years ( enlarged ) , 52.8years ( no change ) , and 57.1years ( shrunken ) , suggesting a higher tendency of lesion enlargement in younger patients ( p = 0.003 ) ( table1 )  . 
other factors including background fatty liver or chemotherapeutic drug history for various malignancy ( table2 ) showed no statistical significance on univariate and multivariate analyses ( p > 0.05 ) ( table1 )  . 
logistic regression test showed that patients in the shrunken group were older ( univariable , p = 0.017 ; multivariable , p = 0.046 ) than the remaining patients , and the incidence of background cirrhosis was higher ( univariable , p = 0.011 ; multivariable , p = 0.031 ) in these patients than in those in the no change and enlarged groups . discussion hemangioma is considered a type of congenital vascular anomaly rather than a tumorous condition ; thus , it is expected to show no remarkable change in size over time . 
 [ 3 ] reported that nearly 40% of 163 hepatic hemangiomas in 123 patients grew by > 5% of the initial diameter over time ( meanstandard deviation , 3.71.9years ) at a modest rate ( 2mm / year in linear dimension and 17.4% per year in volume )  . 
 [ 4 ] during a median follow - up period of 4years , 144 of 220 patients ( 65% ) had hemangiomas that increased in size , whereas 20 patients ( 9% ) had hemangiomas that decreased in size . 
in their study , the peak growth was found in young ( age < 30years ) patients and the growth rate was significantly decreased in older ( age > 50years ) patients [ 4 ]  . for the growth rate of each hemangioma , we found no significant correlation between the initial size and the size change ratio . 
regardless of the length of the follow - up period , patients with a 20% increase in diameter were significantly younger than the other patients in the present study , consistent with the prior report [ 4 ]  . 
moreover , there was no predilection for the female sex in the incidence of 1 3 la radiologia medica ( 2018 ) 123 : 323330 hemangiomas in the cirrhotic liver are likely to decrease in size , probably owing to progressive fibrosis [ 9 ]  . 
these findings suggest that liver cirrhosis may cause obliteration of hepatic hemangiomas in the process of fibrosis , which could explain the shrunken lesions for nearly one - half of the hepatic hemangiomas in cirrhotic livers in the present study . 
in this patient , there was no remarkable enlargement on earlier follow - up ct ( from 0.4cm at 15months to 0.7cm at 6years ) , which suggested that the gradual enlargement was not influenced by the early hemodynamic changes in the remaining hepatic parenchyma and surrounding parenchymal hyperplasia just after the partial hepatic resection . 
the age of this patient was 42years , younger than the mean age of all patients , and the size change also seemed to be rather sporadic except for the age factor when the background fibrosis was not severe enough to obliterate the cavernous channel of the hemangiomas . 
 the degree of intracellular fatty deposit in the surrounding hepatic parenchyma is not likely to induce any hemodynamic changes in intrahepatic vascular lesions . we presumed that if the hemangioma is a real vascular neoplasm [ 18 ] , the antiangiogenic effect would induce the shrinkage of hepatic hemangiomas in patients with cancer treated with relevant chemotherapeutic agents ( table2 )  . 
this finding could support the concept that hepatic hemangioma is a kind of vascular malformation or hamartoma rather than a true neoplasm [ 19 ] , and its enlargement or shrinkage might be related to the expansion or narrowing of the cavernous vascular space rather than cellular proliferation or necrosis . 
however , the result of the present study suggested that even if there was chemotherapy - induced vasculitis , the degree of the inflammatory process would not be severe enough to induce shrinkage of the cavernous vascular spaces in the hemangiomas . 
besides the direct vascular occlusion of supplying hepatic artery branches from chemoembolization [ 20 ] , which was excluded from the present study , there have been no data showing that intrahepatic vasculitis could induce the regression of hemangiomas . use of steroid agents is another possible contributing factor to the size change in hepatic hemangiomas ; however , the effect is still under debate [ 21 , 22 ]  . 
a an axial image of portal venous phase post - contrast ct shows a 2.6 - cm hemangioma in s6 liver with strong contrast enhancement in most of the lesion volume ( arrow )  . 
b the lesion looks enlarged to 6.4cm in the longest diameter after 6years and 4months interval growth of hepatic hemangiomas in the present study , like in the previous report [ 4 ]  . despite the presence of a statistical significance , only a minor proportion of patients ( 23% ) with hormone therapy showed growing hemangiomas compared with the control group ( 10% incidence of growing hemangiomas ) in the report by glinkova etal . 
according to the results of the present study , only senile change seemed to nonspecifically affect the long - term interval change of the hemangiomas . with regard to background liver changes , dodd etal . 
a axial images of arterial ( left ) and portal phase ( right ) post - contrast ct show a 2.1 - cm hemangioma in the right hepatic lobe with peripheral globular and centripetal enhancement ( arrowheads )  . 
b the lesion looks shrunken to 1.1cm ( arrow ) in the longest diameter after 11years on axial t2 - weighted ( left ) and portal phase of postcontrast t1 - weighted mri ( right ) combined with peripheral parenchymal retraction steroids on hepatic hemangiomas . 
while herbal medicine is an important source of steroid intake in the far east asian region , it was difficult to gain information on exact usage , duration , or type of such medications from our hospitals medical records . 
therefore , we decided to exclude the use of steroid agents in the data analysis of this study . this study is one of the largest studies with a long - term follow - up of hepatic hemangiomas . 
in the statistical analysis of several possible factors responsible for the size change of hepatic hemangiomas , only the patients age and underlying liver cirrhosis showed statistical significance in univariable and multivariable analyses . 
moreover , there was one patient who showed fluctuation in the size of hemangioma : the hemangioma decreased from 1.7 to 1cm during the first 5years of follow - up , and then enlarged to 1.3cm in diameter during the next 5years . 
although we reviewed the medical record of this patient again , we could not find any medical history of the possible factors that we considered in the present study . this study has some limitations . 
during the long - term follow - up interval , the patients were mostly outside of the 1 3 la radiologia medica ( 2018 ) 123 : 323330 hospital , and it was impossible to obtain a timely history of medication , which could directly affect the size change . 
 third , for patients with cirrhosis , it was also difficult to quantify the histologic background of fibrosis with the size change of each hemangioma owing to the retrospective study design . 
finally , hepatic hemangiomas were not the major targets for imaging studies in most patients , and the ct or mri protocols were not standardized depending on the underlying disease problems of the patients . 
regardless of the variable imaging protocols used in the various ct and mri devices , there was no problem in sizing the lesions that indicated hemangiomas at multiple imaging sessions during the very long - term follow - up time . in conclusion , during the long - term ( 513years ) follow - up period , about half of the hepatic hemangiomas showed either an increase or a decrease in size . 
sixteen patients used two or more different drugs during the follow - up periods including two patients who used non anti - angiogenic drugs only 1 3 330 la radiologia medica ( 2018 ) 123 : 323330 compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
patients were randomly assigned to three different operators , including a junior supervisor and two first - year residents in radiology who never performed an intra - articular injection of the knee before the present study . 
lateral position does not require a supplementary irradiation and does not increase the procedural papersonal operators skill is an independent factor in determining the success of the training . keywords knee injections , intra - articular / methods arthrography fluoroscopy reproducibility of results interventional humans introduction intra - articular injections of the knee are commonly used in clinical practice by physician like rheumatologists , orthopedic surgeons and general practitioners . 
intra - articular needle * paolo simoni paoloemiliosimoni@gmail.com reine fabiola childrens university hospital , universit libre de bruxelles ( ulb ) , 15 , avenue jean joseph crocq , 1020brussels , belgium 2 radiology department , chu de lige , chu du sart tilman , bt . 
35 , 4000lige , belgium placement can be required to treat various knee joint disorders including rheumatoid arthritis ( ra ) and osteoarthritis ( oa ) [ 1 ]  . 
in radiology practice , fluoroscopy is currently used to guide the intra - articular placement of the needle into the knee joint space , especially to carry out computed tomography arthrography ( cta ) [ 2 ] or magnetic resonance arthrography ( mra ) [ 3 , 4 ] of the knee . in the absence of a knee effusion , needle placement into the intra - articular space presents a challenge to the clinician [ 5 ]  . 
without imaging guidance , the placement of the needle in the knee joint can be only indirectly verified by the backflow of the liquid [ 6 ] or when audible squishing sounds are heard after injection of a mixture of liquid and air [ 7 ]  . some studies have evaluated the accuracy of needle placement into the intra - articular space of the knee joint vol . : ( 0123456789 ) 1 3 360 la radiologia medica ( 2018 ) 123 : 359366 without imaging guidance in the absence of an effusion and revealed that at least 1020% of the injections are not intraarticular [ 5 , 8 , 9 ]  . incorrect placement of extra - articular hyaluronic ( ha ) injection causes discomfort to the patient and declination of the effect of the ha [ 10 ]  . 
intra - articular needle placement is more accurate when performed under imaging guidance using ultrasound ( us ) or fluoroscopy [ 11 ]  . us - guided intra - articular knee injection improves the accuracy of intra - articular needle placement [ 4 ] and the short - term outcome after corticosteroid injection in knees with [ 12 ] and without [ 11 ] joint effusion . iodinate contrast [ 2 , 3 , 6 , 7 , 13 ] or air [ 8 ] can be used to check the intra - articular position of the needle . under fluoroscopic guidance , in the superolateral approach , the patient lies supine on the x - ray table [ 14 ]  . 
 the intra - articular position of the needle can be checked by injecting some milliliters of iodinate contrast and observing the filling of the joint space . in clinical practice , we observed that the superolateral approach could easily be performed also with the patient in lying on the side opposite to the target knee . 
the aim of the present study was to evaluate the learning curves of beginner operators performing the superolateral approach under fluoroscopic guidance using the supine and lateral position . materials andmethods all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . the study was approved by the local institutional ethics committee , and an informed consent was obtained from all individual participants included in the study . 
one hundred and seventy - seven consecutive patients scheduled for a computed tomography ( ct ) arthrography of the knee joint were enrolled in the study , between june and november 2012 , including 72 females ( 40.7% ) and 105 males ( 59.3% ) , mean age 42.215.0years. patients with evidence of joint effusion into the suprapatellar pouch on lateral x - rays view of the knee were excluded . 
patients with a metallic hardware in the knee , including joint prosthesis , were also excluded . all the patients underwent a standard arthrography of the knee under fluoroscopic guidance to prepare the ct arthrography . three different operators , including two first - year residents in musculoskeletal imaging and a junior supervisor , performed the injection under fluoroscopic guidance . 
the junior supervisor had performed a 6 - month training in interventional radiology . for the intra - articular injections , the operator was chosen using a table of randomization [ 15 ]  . injection positions two positions ( supine and lateral position ) were used for the intra - articular injection . 
 the intra - articular position of the needle was confirmed by the contrast ( hexabrix 320 , guerbet , villepinte , france ) filling the suprapatellary pouch . data collection the height and weight of patients were noted , and body mass index ( bmi ) was calculated . the presence or the absence of a previous knee trauma and / or knee surgery was also recorded . the administration of non - steroidal anti - inflammatory ( nsaid ) drugs on the same day of the injection was noted . the knee pain level was measured just before the injection and during the injection by the 10 - point visual analogue scale ( vas ) [ 16 ]  . 1 3 la radiologia medica ( 2018 ) 123 : 359366 fig . 
 the patella is slightly subluxated externally , and the needle approaches the knee superolaterally in the skin notch between the lateral patella and the lateral femur condyle ( b )  . 
the diffusion of iodinated contrast into the anteromedial recess of the articular space ( black arrowheads ) confirms the intra - articular position of the needle ( d ) the vas before the injection was named vaspre , while the vas measured during the injection was named the vasinjection . 
the comparison of mean values between different groups was made using the analysis of variance ( anova ) , while the comparison of proportion was made using the 2 . the modification of the vas was assessed using the students t test for paired samples . 
the learning curves were determined by a logistic regression . the dependence of success of intra - articular injection and extravasation on other variables was studied using univariate and multivariate logistic regression models . 
under fluoroscopic guidance ( b ) the needle is placed immediately behind the upper pole of the patella , in the presumptive location of the suprapatellar pouch ( c )  . 
the opacification of the suprapatellar pouch confirms the intra - articular position of the needle ( d ) ( or ) , their 95% confidence intervals ( 95% ci ) and p values were calculated . in order to assess the influence of co - variables on procedural pain and on the time of fluoroscopy , a multiple regression analysis was used . for each model , the mean valuesd or the correlation ( r ) was used . 
the needle is placed far from the cartilage , thus minimizing the occurrence of cartilage damage by the needle . the present study was , to the best of our knowledge , the first evaluating learning curves , procedural pain and extravasation rate of intra - articular injection of the knee under fluoroscopic guidance . 
therefore , lateral position could be proposed to beginners to improve the rate of successful intra - articular knee injection . second , the rate of successful injections depended on the personal skill of the operator . 
further studies in other populations of patients are needed to confirm an influence of the sex on the success of the knee intra - articular injection . fourth , learning curves indicated that for operators 2 and 3 , there was a significant learning effect for the supine and lateral positions together and for the supine position alone , while there was no significant learning effect for the lateral position alone . 
the three operators have statically equally used the two different positions of injection ( supine position 101 patient ( 57% ) and lateral position 76 patients 42.9 ( p = 0.92 ) ) ( table1 )  . there was a significant learning effect for the supine and lateral positions together ( fig.4 ) and for the supine position alone ( fig.5 ) for operator 2 and operator 3 . 
lateral position and the placement of needle directly in the presumptive location of the suprapatellar pouch may help beginners to avoid injecting contrast in the nearby soft tissues , namely the prefemoral fat pad and the hypodermic soft tissues of the anterolateral aspect of the knee . this study has some limitations . first , we did not evaluate the grade of osteoarthritis of the lateral patellofemoral joint . second , we did not quantify the extent of the contrast extravasation . 
contrast extravasation may be minimal in some cases and not clinically relevant . third , the lateral radiographs of the knee were used to exclude patients with intra - articular fluid collection . 
 this method could be ineffective in patients with a small amount of intra - articular fluid , and we may have failed to exclude this subset of patients . fourth , we used the bmi and not the knee circumference to assess knee dimensions . 
therefore , our analysis could be ineffective to reveal a higher rate of failed injection in patients with a knee with a large abdominal circumference . 1 3 la radiologia medica ( 2018 ) 123 : 359366 fig . 
5 learning curves for the supine position alone : there is a significant learning effect for operators 2 and 3 finally , we did not compare the lateral and supine position under fluoroscopic guidance with the blind superolateral position for operators in training . 
this could be assessed in another perspective study . in conclusion , the superolateral injection of the knee under fluoroscopic guidance with the patient in lateral position may be proposed as easy technique to perform a successful intra - articular injection without extravasation for operators in training . the lower rate of extravasation of this technique may be particularly relevant in case of contemporary injection of hyaluronic acid and corticosteroid . lateral position does not require a supplementary irradiation and does not increase the pain related to the procedure . 
personal operators skill is an independent factor in determining the learning curve . acknowledgements adelin albert , phd , and laurence seidel , phd , are kindly acknowledged for the statistical analysis . funding therefore , no fund was granted to the authors to perform this study . compliance with ethical standards conflict of interest the authors declare no conflicts of interest to declare . ethical standards no animals were involved in the present study . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent the local institutional ethics committee approved the study , and an informed consent was obtained from all individual participants included in the study . 1 3 366 la radiologia medica ( 2018 ) 123 : 359366 5 . 
sibbitt wl jr , kettwich lg , band pa etal ( 2012 ) does ultrasound guidance improve the outcomes of arthrocentesis and corticosteroid injection of the knee ? scand j rheumatol 41 : 6672 13 . 
messina c etal ( 2016 ) ultrasound guidance to perform intra - articular injection of gadolinium - based contrast material for magnetic resonance arthrography as an alternative to fluoroscopy : the time is now . 
messina c etal ( 2017 ) do we still need to take fluoroscopical guidance into account when injecting joints ? semin arthritis rheum 46 ( 4 ) : e16 20 . 
in more recent times , post - mortem ct ( pmct ) and post - mortem ct - angiography ( pmcta ) have become an established practice in numerous forensic units , because of the undeniable advantages these diagnostic instruments can offer : data acquisition times are increasingly fast , costs have become lower and , once acquired , data can be re - utilized and re - evaluated at any given time . 
this review aims to chart the history of post - mortem cardiac imaging , highlighting its evolution both in terms of methodology and technology as well as the contribution that forensic radiology has been able to offer to forensic pathology , not as an alternative to autopsy but as a guide and aid when performing one . 
 finally , the latest advances in the study of cardiac deaths are explored , namely by cardiac post - mortem mri ( pmmr ) , able to visualize all the various stages of a myocardial infarction , post - mortem mri - angiography ( pmmra ) , useful in investigating coronary artery pathology and post - mortem cardiac micro - ct , able to provide near - histological levels of myocardial , coronary and valvular detail . keywords post - mortem angiography post - mortem computed tomography post - mortem computed tomography angiography post - mortem magnetic resonance imaging post - mortem magnetic resonance angiography post - mortem micro computed tomography introduction post - mortem imaging is a powerful tool in forensic sciences , its importance is widely recognized and its application increasingly common in forensic practice . 
on the other hand , following the advances in clinical and forensic radiology , current post - mortem imaging has become an increasingly helpful tool in the study of the coronary arteries and the myocardiuautopsy is , in fact , the established gold standard for the investigation of cause of death , however , because of religious , cultural , economic , and workforce reasons , replacement of the invasive component of these investigations has become preferable in some circumstances . based on the above mentioned , post - mortem coronary imaging has become an added tool to diagnose scds , as vol . : ( 0123456789 ) 1 3 352 la radiologia medica ( 2018 ) 123 : 351358 an adjunct to gross and histological - immunohistochemical examination [ 5 ]  . since the 1970s , various techniques for post - mortem selective coronary arteriography have been experimented . 
 subsequently , post - mortem imaging for the cardiac study has been introduced , becoming noticeably widespread and a tool of customary use in various forensic units worldwide [ 6 ]  . however , only in recent times , pmct with intravascular contrast agent infusion ( pmct angiography ; pmcta ) has become an established practice [ 79 ]  . therefore , the aim of this review is to chart the history of post - mortem coronary imaging , highlighting its evolution both in terms of methodology and technology as well as the contribution that forensic radiology has been able to offer to forensic pathology , not as an alternative to autopsy but as a guide and aid when performing one . early stages ofpostmortem coronary imaging multiple approaches topostmortem selective coronary angiography in the 1970s , post - mortem coronary angiography was introduced for the investigation of scd related to cad and ihd . 
 introduction of post - mortem selective coronary arteriography came from the need to provide a rapid and precise explanation for scd , by evaluation of myocardial modifications and of vascular patterns and alterations . 
the easiness of execution together with wealth and clarity of data gathered in this new way , allowed for a quick and precise overview of the anatomical conditions of entire coronary arterial tree , especially the end - branches that are difficult to examine in autopsy [ 10 ]  . first approaches included selective coronary incannulation and subsequent administration of contrast agents , to provide opacification of entire coronary arterial tree . 
this result was achieved by imaging study with the organ removed from the body ( by ex situ cardiac angiography ) , rather than by performing a whole body angiography ( by insitu cardiac angiography ) , because of the lack of an active circulation to deliver contrast agent . ex situ cardiac angiography provided , as a preparatory phase , en - bloc removal of heart and thoracic organs , and successive cardiac isolation , transecting the aortic root just above the coronary ostia . 
an angiocatheter was then inserted in the ostia and a contrast agent injected . numerous contrast agents were available , in particular semi - solid compounds mixed with barium sulfate or lead oxide [ 11 , 12 ] , or also a high viscosity watery solution made by 41% of iodamide , as in the experience of institute of forensic medicine in naples , italy [ 13 ]  . 
as an alternative to these semi - solid contrast agents , characterized by laborious and expensive procedures , especially due to the use of pressure regulators , alternative contrast agents were introduced [ 14 ]  . 
in particular , with diatrizoate meglumine and diatrizoate sodium , a low cost contrast agent , it was possible to achieve an excellent opacification of the coronary arterial tree . revolution ofpostmortem computed tomography angiography ( pmcta ) introduction of pmct has radically changed the post - mortem study of coronary arteries and myocardiuin the last 20years , in fact , post - mortem cardiac imaging has seen a remarkable growth because of the undeniable advantages ct scan offer : data acquisition times are increasingly fast , costs have become lower and , once acquired , data can be re - utilized and re - evaluated at any given time . 
the speed of execution , the high definition of the anatomy that can be achieved for any vascular region of the body , the possibility to directly acquire entire volumes , the capacity to easily achieve 3d reconstructions through rendering software , have made pmct the most used investigative method today to support an autopsy in the post - mortem examination of cases of scd [ 1517 ]  . volume acquisition and scan times have forced a rigorous streamlining of method and choice of contrast agents . 
 in this regard , two different techniques were developed : the first aims at the study of the sole coronary arteries by an insitu selective coronary ct - angiography [ 18 ] , while the other encompasses the evaluation of the vascular system of the entire body ( whole - body pmcta ) [ 19 , 20 ]  . modern insitu selective coronary ct - angiography is performed by inserting a catheter in the lumen of the left carotid artery , inflating a balloon catheter in the ascending aorta and injecting contrast agent in the aortic root to opacify the coronaries . 
in particular , the oxford approach [ 21 ] entails the manual administration of a sole contrast agent , while the leicester method entails the administration of both air ( negative contrast that can highlight possible calcified plaques or coronary stents ) and a contrast agent through a machine - run injector [ 22 , 23 ]  . 
moreover , since these approaches use only a small amount of contrast , the risk of edema to tissues ( that might jeopardize further investigations such as histological analyses ) is staved off . nowadays , whole - body pmcta is the most commonly used technique , because it allows the view of the whole vascular system of head and neck , chest , abdomen and extremities [ 1 , 24 ]  . 1 3 la radiologia medica ( 2018 ) 123 : 351358 different pmcta techniques are currently available , each with its own variations , elaborated by working groups also as part of the multi - centric research trial project for validation of post - mortem ct - angiography ( twgpam technical working group post - mortem angiography methods )  . conventional technique [ 2527 ] has been utilized for the first time in 2004 as part of the virtopsy project . 
 according to this approach , a minimally invasive study of the entire body is achieved by cannulating the femoral vessels and injecting an oily liquid solution since oily liquids can remain intravascular through a heart lung machine . 
this approach is of considerable value , because groin region is easily accessible , its vessels are fairly superficial and thus easier to cannulate , coronaries are not touched and perfusion pressure can remain low ( 1200ml per 90s for the arterial phase )  . 
post - mortem circulation is determined through a perfusion device with controlled pressure that injects a mixture of 6% oily contrast agent and paraffin oil , in the femoral vessels that have been cannulated on one side of the body using a 510cm skin incision . 
the procedure entails a basic ct scan followed by three post - contrastographic phases where standardized injection parameters are used ( injection time , pressure and flow - speed )  . 
 [ 29 ] , using the same approach in the cannulation of the femoral vessels , but different perfusion device ( using a modified heartlung machine and different perfusion protocol ) and contrast agents ( watery solutions and different combinations of polyethylene glycol )  . 
 [ 31 ] proposed a variation of the conventional technique , by cannulating the artery and vein in the armpit region , instead of the groin , to get an excellent view also of the vascular system in the legs . 
 [ 32 , 33 ] introduced an alternative technique , by injecting a contrast agent into a peripheral vein after the patient has been pronounced dead , directly after in - hospital death on the clinical ct table , while performing the same pressure on the chest as the cardiopulmonary resuscitation ( cpr ) , to increase blood pressure and generate small cardiac output . 
 [ 34 ] proposed a different approach involving cardiac left ventricle , by a percutaneous puncture through the intercostal under ct guidance and manual injection of diatrizoate meglumine and normal saline . pmcta is a minimally invasive procedure , able to show direct and indirect evidence of serious pathologies affecting the coronaries . 
subsequently , with more than one phase , it is suggested to interpret the changes as diagnostic if they are visible in at least two . among the direct evidence , coronary stenosis or occlusions are worth mentioning [ 35 ] , while among the indirect evidence myocardial enhancement is a sign of ischemic necrosis . 
in fact , through the use of lipophilic contrast agents , normal myocardial tissue shows no impregnation from the contrast , while damaged myocardium appears as contrast - enhanced areas perfectly coinciding with infarcted myocardium [ 25 , 36 , 37 ]  . post - mortem ct - angiography is extremely useful to detect coronary stenosis and to quantify the degree of occlusion , without alteration of the anatomical structures examined , as inevitably happens with autopsies [ 38 , 39 ]  . 
moreover , preparation and examination of cardiovascular bypass surgeries is usually difficult and can require a long time during an autopsy , due to the presence of scar tissue around bypass area and of vascular anastomoses . 
a post - mortem ct - angiography allows for a 3d visualization and evaluation of cardiovascular bypass , supporting the forensic pathologist in the detection of any potentially relevant finding during the autopsy . a comparison between selective incannulation of the coronary arterial tree with the organ removed from the body ( by ex situ cardiac angiography ) and a whole - body pmcta approach with 3d cardiac volume rendering is provided in figs.1 , 2 and 3 . limitations in ct scan without contrast agent are determined mainly by the possibility to show only certain signs of myocardial ischemia such as the myocardial thickening ( in chronic infarction ) , cardiac tamponade ( in case of trauma or rupture of a myocardial ischemic scar ) or hemothorax ( in case of aortic dissection )  . 
contrast agent injection , conversely , leads to optimal opacification of the coronary lumen , thus showing potentially fatal anomalies such as stenosis [ 40 , 41 ]  . pmcta findings usually well correlate with autopsy findings . 
pmcta is advantageous compared to autopsy in the study of calcified plaques , since anatomical structure can be permanently altered by coronary and myocardial section , and false - positives can be created giving 1 3 354 la radiologia medica ( 2018 ) 123 : 351358 fig . 
sections on aortic valve level demonstrating b the entire coronary tree and c lca with the critical stenosis of the lumen ( arrows ) such as traumatic lacerations or scars . 
myocardial ruptures and lacerations of the coronary arteries are easily revealed by the extravasation of contrast agent . on the other hand , a ct scan can present some limitations compared to histological study , mainly represented by the defect in visualization in the downstream post - stenotic portion of vessels and by the difficulty to establish the nature of stenosis , whether chronic or acute caused by a plaque rupture . however , a definitive diagnosis of myocardial ischemia is based on anatomical and pathological criteria and can be carried out in two different ways : in a minimally invasive way through image - guided biopsy of the most affected area , or through histopathological study of samples taken during an autopsy . finally , pmcta has shown great potential to increase the quality of post - mortem investigations , especially in the field of scd . 
a post - mortem ct scan together with a ct - guided biopsy could also be a valid alternative in those communities where , for ethical or religious reasons , minimally invasive investigations are preferred to the autopsies . 
a selective image of the left anterior descending artery ( lad ) with critical stenosis of the lumen in the middle tract at d2 level ( red arrows )  . 
contrast agent injection allows also a better evaluation of pathological conditions of the myocardium , 1 3 la radiologia medica ( 2018 ) 123 : 351358 most recent advances cardiac postmortem mri ( pmmr ) andpostmortem mriangiography ( pmmra ) from the 1990s , post - mortem mri ( pmmr ) has garnered an increasingly important role as an adjunct in diagnosis and a helpful tool to complement an autopsy , especially in cases where certain communities objected to autopsies on religious grounds and asked for less invasive techniques to investigate the causes of death [ 27 , 43 ]  . in particular , pmmr is the method of choice in cases of sudden cardiac death , showing the myocardium and eventual lesions within it , eventually associated to pmcta , which permits a detailed investigation of stenosis or other lesions of the coronary arteries . cardiovascular imaging is a core area of pmmr imaging and growing evidence indicates that pmmr is able to detect ischemic injury ( acute , subacute and chronic infarction ) , according to the intensity in t1 and t2 sequences , at an earlier stage than traditional autopsy and routine histology [ 44 ]  . 
on the other hand , myocardial alterations in hyperacute phase are not detectable at autopsy , even if in presence of coronary stenosis , or other causes of scd such as myocardial hypertrophy or cocaine intoxication . for these reasons , post - mortem 3 - tesla mri is an effective and helpful support in visualizing and differentiating myocardial infarction in acute , subacute and chronic phases , including hyperacute phase not clearly visible at autopsy or histological examination ( first histological signs of myocardial infarction appear approximately after 24h )  . 
 pmmr above all , in selected cases , can be altogether an alternative minimally invasive method to conventional autopsy , especially for subjects who cannot undergo traditional autopsy for logistical , cultural or personal reasons . as an adjunct , a combination of the soft tissue detail provided by mri and the information afforded by angiography is useful in investigating vascular pathology and solid organ laceration [ 45 ]  . basic evaluation of the coronary arteries on non - contrast t2 weighted pmmr imaging is difficult and lack of missing , and the assessment of coronary artery disease problematic , so pmmra fat - saturated t1 weighted images offer good images . 
peg - diluted contrast agent , hyperintense in t1wimages and hypointense in t2w - images , provides , in fact , visualization of vascular pathologies [ 46 ]  . overall , all vascular pathology identified at pmmra can also be seen at pmcta , so that its diffusion and utilization remains again limited . cardiac microct post - mortem micro - ct ( pmmct ) is a tool in the investigation of scd , using pmct at an improved resolution down to micrometers . 
micro - imaging had already been experienced ( mainly in the study of calcified tissues , dental matrices and bone specimens ) [ 4751 ] , also in fetal imaging [ 52 ] , highlighting its specific preclinical role and its application on specific types of samples ( e.g. , fetal ) according to the model of the device . 
micro - ct , in fact , can provide a highly accurate three - dimensional rendering of cardiac structure , after extracting and fixing tissue in a solution of 10% formalin and potassium triiodide to preserve cellular architecture and provide optimal contrast . 
furthermore , micro - ct represents a well - consolidated technique and confirms the capacity of this technology for non - invasive examination , enabling nondestructive inspection and providing very high - resolution images ( micrometer resolution ) without the need for the injected contrast agent . 
surprisingly , the resolution obtained by pmmct seems able to provide near - histological levels of myocardial , coronary and valvular detail , so that histology compared to micro - ct does not provide additional useful information . 
in this way , micro - ct scans can provide the necessary level of detail to make this approach even superimposable to histological study and able to conduct to an accurate morphological diagnosis without the need for further dissection [ 53 ]  . conclusions the use of pmcta has become customary in the investigation of scd because of the undeniable advantages these diagnostic instruments can offer : data acquisition times are increasingly fast and , once acquired , can be accessed at any given time , even after cremation or burial . 
on the other hand , there are some disadvantages that need mentioning : performing certain 1 3 356 la radiologia medica ( 2018 ) 123 : 351358 procedures requires equipment and necessity to employ specialized staff , leading to costs that small units cannot always afford . 
another relevant aspect is the need for radiologists to specifically train for post - mortem examinations . the latest advances in the study of cardiac deaths are represented by cardiac post - mortem mri ( pmmr ) , the method of choice in cases of sudden cardiac death , showing the myocardium and eventual ischemic injury ( acute , subacute and chronic infarction )  . 
besides , post - mortem mri - angiography ( pmmra ) is useful in investigating coronary artery pathology and post - mortem cardiac micro - ct ( pmmct ) is able to provide near - histological levels of myocardial , coronary and valvular detail . in this way , as each technique has its own advantages and limitations , it is essential to select the right method among available different procedures . 
the diagnostic capability of all these various techniques of post - mortem imaging compared to a full autopsy has been widely demonstrated [ 5759 ]  . nowadays , it does not seem possible for post - mortem imaging to ever replace conventional autopsy , but it can be a valid complementary tool with encouraging future perspectives . 
in fact , the combination of post - mortem imaging and conventional autopsy is actually the gold standard in the evaluation of death when the suspected cause is ischemic cardiomyopathy . 
for these reasons , post - mortem imaging has to be considered an aid in the forensic investigations , rather than an alternative to conventional post - mortem procedures [ 60 , 61 ]  . compliance with ethical standards conflict of interest the authors have no conflicts of interest to disclose . ethical standards this article does not contain any studies with human participants performed by any of the authors . ethical approval the present article obtained approval by ethics committee . 
clinical outcomes and mortality were evaluated after the treatment , and follow - up was carried out after hospital discharge . results atcdt was technically successful in 93.7% ( 36 / 37 ) patients , with one case died from respiratory failure during procedure . 
three cases died of respiratory failure caused by pte , and two cases died of diseases unrelated to pte ( lung carcinoma / hemoptysis ) during a 201524days of follow - up . conclusion atcdt may be a feasible , effective , and safe treatment for normotensive patients with acute pte . keywords pulmonary thromboembolism agitation thrombolysis catheter - directed thrombolysis thrombolysis follow - up introduction pulmonary thromboembolism ( pte ) is a common lifethreatening disease with a wide spectrum of clinical presentation , from asymptomatic embolism to massive embolism with sudden death [ 1 ]  . 
1 , east jian she road , zhengzhou450052 , china interventional institute ofzhengzhou university , zhengzhou , china interventional therapy andclinical research center ofhenan province , zhengzhou , china tomographic angiography in patients without hemodynamic shock or instability is not termed massive pte [ 2 ]  . 
the optimal management of normotensive patients with acute pte is controversial , whether thrombolysis decrease mortality and morbidity remains questionable , and even it is not warranted [ 4 ]  . the catheter fragmentation by rotatable pigtail catheter underwent successful experimental assessment [ 5 ] and clinical application for massive pte patients [ 6 , 7 ] , which facilitates at least partial recanalization of a central embolic occlusion [ 7 ]  . 
previous research indicated that agitation thrombolysis ( at ) is also a safe and feasible approach for treatment of buddchiari syndrome patients with inferior vena cava thrombosis with or without balloon dilation [ 8 , 9 ]  . 
the contraindications to lysis included active internal hemorrhage , aortic dissection , pregnancy , cerebrovascular accident , or history of surgery or trauma within 2weeks . agitation thrombolysis andcatheterdirected thrombolysis procedure the vital signs and bleeding complications were monitored continuously prior to and during the interventional fig . 
stars indicates thrombosis in right superior pulmonary artery ( r - spa ) , right inferior pulmonary artery ( r - ipa ) , right middle pulmonary artery ( r - mpa ) , left superior pulmonary artery ( l - spa ) and left inferior pulmonary artery ( l - ipa )  . 
thrombolysis treatment terminates once patient is clinical cured and no symptom of pte with no thrombosis was confirmed by ct angiography ; otherwise , treatment should be maintained for 7days in the absence of improvement . anticoagulation andfollowup five milligrams of warfarin was taken orally once a day from the beginning of the second day until 6months after the procedure , and 5000iu of low molecular weight heparin was hypodermically injected twice a day until international normalized ratio reached 23 . 
the follow - up protocols were performed 1 , 3 , 6 , and 12months after procedure and then annually by computed tomographic angiography , which has the greatest sensitivity and specificity for detecting emboli in pulmonary artery [ 2 ]  . statistical analysis data were presented as meanstandard deviation . 
venous thrombosis was the risk factor for thromboembolic disease in these patients ; 21 patients have deep venous thrombosis , with 6 in right , 7 in left , and 8 in both legs . 
 the survival rate is 73.4% 6331524days after operation during follow - up . discussion massive pte is one of the most frequent noncardiac causes of cardiac arrest [ 12 , 13 ] , which caused an incidence of cardiac arrest of 18% [ 14 ]  . 
treatments for massive pte include systemic or local thrombolysis , percutaneous mechanical thrombectomy , and open surgical embolectomy , besides implantation of inferior vena cava filter to prevent further pte [ 1 ]  . 
percutaneous mechanical thrombectomy , a reliable therapeutic option of pte , provides rapid clearance of occlusive thrombus in pulmonary artery , decreasing pulmonary artery pressure and improving hemodynamics [ 15 , 16 ] , and reducing dose and time of pharmacologic thrombolysis , which offers an alternative to surgical thrombectomy and pharmacologic thrombolysis , especially when there are contraindications to thrombolytic drugs [ 17 ]  . 
whether thrombolysis decrease mortality and morbidity remains questionable , and even it is not warranted [ 4 ]  . previously studies indicated that at is a safe and feasible approach for treatment of fresh inferior vena cava thrombosis occurred naturally or iatrogenically in buddchiari syndrome patients [ 8 , 9 ]  . 
two patients died after the operation , with a mortality rate of 6.9% , which was lower than the reported mortality rate in untreated patients ( 2565% ) [ 14 ] ; however , a total of seven patients ( 24.1% ) died during follow - up . 
3 postoperative ct examination shows no thrombosis in right superior pulmonary artery ( r - spa ) , right inferior pulmonary artery ( r - ipa ) , right middle pulmonary artery ( r - mpa ) , left superior pulmonary artery ( l - spa ) and left inferior pulmonary artery ( l - ipa ) la radiologia medica ( 2018 ) 123 : 338344 for at , the pigtail tip is a safe configuration and is easy to navigate into and within the pulmonary artery without perforation [ 7 ]  . 
the unobstructed area is relatively increased after fragmentation of central emboli and dislocation of the fragments to peripheral pulmonary arteries , and the increased total surface area of the fragments may result in accelerated efficacy of thrombolysis compared to local thrombolysis [ 7 ]  . 
secondary end - point : control of pain and functional / compressive disorders during follow - up ( 27years )  . results procedure was performed bilaterally in 250 patients ( 98% )  . 
for long - term evaluation we used the follow - up data of 176 patients of premenopausal age who have been treated in a period of time included between january 2001 and december 2010 , and monitored for up to a maximum of 2years . 
all patients included in such study were women with symptomatic uterine fibroids with surgical indications ( hysterectomy or laparoscopic myomectomy ) , hopeful in uterus preservation and / or avoid surgery therapy . 
the patients were included on the basis of clinical and instrumental criteria . the study has been approved by ethical committee of catholic university of sacred heart of rome . clinical criteria consisted in the presence of at least one of the following symptoms : hypermenorrhea and / or menometrorrhagia , relapsing and unresponsive to medical therapy , with or without anemia ; pelvic pain and / or compressive disturbances ( pollakiuria , urinary retention , abdominal distension , feeling of weight in the lower abdomen , constipation or tenesmus )  . 
instrumental criteria consisted of ultrasound diagnosis of single or multiple fibroids in transmural location , intramural , subserosal , intramural / subserosal , intramural / submucosal and / or transmural . 
no restrictions were applied on maximum size of uterus and fibroids and number of fibroids within uterus . exclusion criteria from the study are the following : presence of pelvic inflammatory disease or endometritis ; presence of subserosal pedunculated fibroids , a pedicle measuring less than 50% of the maximum diameter of the same fibroid ; presence of submucosal fibroids removable by hysteroscopic operation ; suspicion of pelvic malignancy ; concomitant gynecological pathologies with surgical indications ; contraindication to arteriography ( hypersensitivity to contrast medium , severe coagulopathies la radiologia medica ( 2018 ) 123 : 385397 and renal failure ) ; desire to increase fertility : considering that data on the impact of reproductive capabilities are still contrasting , patients whose only disturbance was represented by infertility were not included unless specific exceptions : ( 1 ) patients who had already undergone hormonal therapies or myomectomy without achieving results ; ( 2 ) when location , number and / or size of fibroids allowed hysterectomy as the only therapeutic option . 
 patients were subjected to medical - gynecological examination with a detailed clinical history ; pap test if needed ; transabdominal and transvaginal pelvic ultrasound , including fluximetric evaluation ; hysteroscopy with endometrial biopsy if needed ; mri of the pelvis in selected cases ; normal hematochemical tests ; plasma dosage of fsh and estradiol on the third day of menstrual cycle for premenopausal patients ; microscopic examination of fresh and cultured vaginal secretion ; urine culture . 
after a verification of preliminary investigations outcome , patients were informed in detail on the potential benefits and risks of the procedure , its implementation rules , possible side effects and complementary drug therapy , and a written informed consent to treatment was acquired . the patients were hospitalized 1day before the procedure beginning . 
for premenopausal patients the treatment was planned within the first 10days of menstrual cycle . on admission , each patient received a questionnaire for evaluation of menstrual cycle features ( time , interval and quantity of flow ) , type and severity of the symptoms . 
the intensity of disturbances was expressed using a descending numerical scale from 3 ( severe symptoms ) to 1 ( mild symptoms )  . all embolization procedures have been performed by an interventional radiologist , following a standard protocol : vital signs monitoring , peripheral venous access for infusion of fluids and medicines , urinary catheter positioning , intravenous antibiotic prophylaxis ( cefotaxime 1g ) 1h before procedure beginning . 
after positioning the tip of the coaxial microcatheter in the third distal of uterine artery ( fig.3 ) , we proceeded with injection , under fluoroscopic control , 1 3 la radiologia medica ( 2018 ) 123 : 385397 fig . 
2 selective angiography of internal iliac artery ( right ) , with evidence of uterine artery , its ascendent portion and beginning of vascular design of fibroid ( simmons 2 catheter 5f ) fig . 
patency of main trunk of uterine artery of the embolic material : particles of polyvinyl alcohol ( pva ) from 150 to 500m ( contour , target therapeutics , fremont , ca , usa ) in 237 patients , and calibrated microparticles of increasing size from 200 to 900m ( embosphere , biosphere medical , rockland , ma ) in 18 patients . 
 1 3 388 la radiologia medica ( 2018 ) 123 : 385397 in the first 12h pain was controlled with epidural anesthesia ( 15ml ropivacaine 0.2% and morphine 3mg , immediately after the conclusion of the procedure ) in the first 28 patients , and with intravenous analgesia ( 20mg morphine infusion at a rate of 2ml / h ; paracetamol every 6h and ketorolac if needed ) in other 227 patients . 
the severity of post - procedural pain was evaluated at 2 , 6 and 24h through a visual analogue scale ( vas ) , that envisages a score from 0 ( no pain ) to 10 ( unbearable pain )  . 
the established follow - up for all patients included a clinical monitoring and ultrasound at 1 , 3 , 6 , 12 , 18 , and 24months after the execution of the procedure and , afterwards , a yearly checkup for those patients chosen for long - term evaluation . at each checkpoint , routine hemochemical tests , plasmatic assay of fsh and estradiol were performed , and a written questionnaire was handed to patients for the evaluation of symptoms modifications , features of the menstrual cycle and degree of satisfaction about treatment results . 
embolization procedure has been performed bilaterally in 250 patients ( 98% ) and in 4 cases unilaterally , 3 for congenital absence of uterine contralateral artery , and 1 for the presence of a not catheterizable uterine stenotic artery . 
after the procedure , all patients complained painful pelvic cramps of varying intensity with an average vas rating of 5.6 ( range 110 ) at 2h , 4.6 ( range 1 3 la radiologia medica ( 2018 ) 123 : 385397 110 ) at 6h and 2.2 ( range 09 ) at 24h from the treatment . 
114 patients ( 45% ) complained of nausea and / or vomiting in the first 12h and 98 patients ( 38.6% ) experienced a slight rise in body temperature ( 37.038.0 c ) from the day of surgery . 
after discharge ( table2 ) , 67 patients ( 26.4% ) reported intermittent fever ( body temperature > 38c for 23h per day ) with an average duration of 2.4days ( range 110days ) , 226 ( 89% ) complained pelvic pain caused by cramps , average duration of 5.2days ( range 130days ) , and 203 ( 80% ) reported spotting occurrence , which lasted an average time of 9.9days ( range 060days )  . 
in 6 of these cases amenorrhea was transient , with spontaneous return flow for 2 patients within 3 months after the procedure , and within 4 months for the remaining 4 patients . 
we experienced one case of permanent amenorrhea with premenopausal hormonal values and no climacteric symptoms in a woman of 44years , who was carrier of 4 massive submucosal fibroids in which hysteroscopy ( performed 3 months after the procedure ) documented endometrial atrophy . 
9 of these patients had a pre - procedure ultrasound diagnostic table 2 clinical disorders after ufe symptoms after treatment ( within 1224h ) nausea / vomiting fever ( > 38 ) slight rise in body temperature ( 3738 ) symptoms after discharge intermittent fever ( temperature > 38 for 23h / day ) pelvic pain ( cramps ) spotting occurrence 114 ( 45% ) 36 ( 14% ) 98 ( 38.6% ) 67 ( 26.4% ) 226 ( 89% ) 203 ( 80% ) of intramural fibroid with submucosa component , while 5 patients had one massive intramuralsubserosalsubmucosal fibroid . 
in the remaining 11 ( 4.3% ) patients the expulsion occurred on an average of 4.3 ( range 26 ) months after embolization and in only 1 case a vaginal myomectomy was needed . 
from a clinical point of view , the revision of questionnaires to evaluate symptom modifications , has shown a rapid improvement of all those disorders caused by fibroids , with statistically significant results from the first post - embolization month ( table3 )  . 
for menstrual disorders we noticed a complete resolution in 56% of cases at 1year , in 78% at 2years , and a marked improvement in 32% at 1year , and 14% at 2years . 
in the specific case of menstrual symptoms , subjective perception of disorders improvement has been supported by statistically significant enhancement of menstrual flow characteristics ( table3 ) and by significant increase in hemoglobin and hematocrit levels ( table4 )  . 
during the follow - up period ( 1284months ) , disorders occurrence ( that is meant as recurrence of initially controlled symptoms ) was found in only 18 patients after a median of 36months ( range 384months ) from embolization therapy . 
the recurrent symptomatology consisted of multiple symptoms ( menstrual and / or pain and / or compressive disorders ) in 7 of these patients , and in a single one for 11 of them ( menometrorrhagia in 9 , pelvic pain in 1 , compressive disorders in 1 )  . 
 of the 18 patients who experienced a return of symptoms , 11 had a new surgery performed after a 56 - month median ( range 1584 months ) from embolization treatment , 6 patients underwent a definitive hysterectomy operation and 4 a myomectomy one . 
in addition , 9 of 18 patients with symptomatic recurrence had further hormonal therapies ( progestin , estoprogestinics , medicated spiral ) in an attempt to control symptoms ; of these ones , three then had a surgery treatment . 
 for the other cases of pregnancies : 6 ( 60% ) hesitated in miscarriage ( mean age at conception 40.5years , range 3445 ) and in one case ( woman with previous multiple myomectomy ) there was an ectopic pregnancy . discussion the results of our clinical experience show that uterine arteries embolization is a well - tolerated procedure , safe and highly effective in the treatment of symptomatic uterine fibroids . 
it is almost constant but the intensity is variable : usually severe immediately after embolization , it tends to decrease after 68h , persisting in some cases with variable intensity and frequency for 45days . 
usually pain is accompanied by fever , referable 1 3 392 la radiologia medica ( 2018 ) 123 : 385397 table 5 characteristics of patients that underwent ufe ( successes and failures ) characteristics successes failures age at procedure ( years ) < 35 3539 4044 4549 50 bmi ( kg / m2 ) < 20 2024 2529 30 children 1 smokers yes / ex systemic diseases yes adenomyosis concurrent yes previous medical therapy every type gnrh - agonist previous myomectomy hysteroscopy laparoscopy laparotomy symptoms menstrual disorders pelvic pain compressive disorders anemia number of fibroids 24 5 site of dominant fibroid subserosal intramuralsubserosal intramuralsubmucosal transmural tendency [ 13 ]  . 
nausea and vomiting are relatively frequent in the first hours after procedure , usually linked , at least in part , to the administration of opiates [ 2 ]  . 
the symptomatologic chain just described is defined as postembolization syndrome and is found in 1550% of patients , it is usually solved in less than a week [ 2 , 4 ]  . 
 the majority of patients who undergoes embolization , despite the presence of side effects , can be discharged within 2436h with prescription of oral analgesic therapy for some days and is generally able to resume normal activities within 810days after the procedure [ 1 , 5 , 6 ]  . in our experience , the mean length of hospital stay was 24h and the recovery period was on average 9 - day ( range 130 )  . 
these results are superimposable to those reported in literature , and obviously much lower than those of laparotomic myomectomy ( 3 and 44days , respectively ) [ 7 ] and hysterectomy ( 46 and 60days , respectively ) [ 8 , 9 ]  . 
even if our study was not focused on economic implications of this therapeutic modality , it must be observed that reducing hospitalization and convalescence time can positively affect social and individual costs of fibromatosis pathology . 
 results among largest international case studies have shown the therapeutic efficacy of embolization in reducing treated fibroids size ( estimated averagely between 50 and 60% ) and improving of menstrual disorders and all those symptoms related to fibroids , with success rates between 85 and 95% in the short and medium term [ 5 , 1013 ]  . 
all these studies also report a high rate ( 8797% ) of satisfaction among patients , due to procedure results . embolization is particularly effective in treating menometrorrhagia as suggested by the observation of an immediate resolution or from a marked improvement of this symptom in 8692% of treated patients [ 14 ]  . 
the resolution or improvement of compressive disorders as well as painful symptoms requires a longer time and is documented in 4070 and 6490% of patients , respectively [ 14 ]  . 
the effect demonstrated on the global dimensions of uterus and fibroids is important tooin fact a mean volumetric decrease of uterus of 5060% , and of the dominant fibroid of 3086% is documented in literature [ 5 , 1012 , 15 ]  . in agreement with literature data we have observed an improvement of all disorders in more than 90% of cases , with more than 80% of long - term patients satisfied . 
the great variability of dimensional reduction depends essentially on the structure of fibroids , in particular on the relationship between vascular and stromal component and / or on the amount of extracellular matrix . 
we have observed , as already pointed out by previous studies [ 12 ] , the lack of correlation between symptomatologic response and extent of size reduction in fibroids , demonstrated by acknowledgment of a good symptomatic control in many patients who experienced a relatively small and / or late dimensional reduction of uterus and fibroid . 
studies with a 2 - year follow - up reported an incidence of procedural failure in controlling symptoms , with the resulting need for new treatments , calculated between 9 and 23% [ 4 , 1618 ]  . 
long - term studies with follow - up from 3 to 6years also reported a failure of the procedure and the following need for a treatment in 1328% of patients [ 1922 ]  . 
 firstly , categorization difficulties regarding fibromatosis pathology severity , heterogeneity of criteria used to define procedure failure , and variability in follow - up duration make difficult to compare the results of different studies . 
 moreover , in our study , unlike many others conducted retrospectively , patients were followed prospectively with regular clinical and instrumental controls in order to identify promptly the onset of new diseases and the exact reason and chronological history of any additional treatment needed . 
in addition to this , selection of patients for treatment and subsequent clinical follow - up have been realized by a gynecologist experienced in this therapeutic alternative , and this makes it possible to minimize risks either of inappropriate treatment indication ( concurrent pathologies ) , or of an incorrect symptoms evaluation that can onset during follow - up period : in many cases these symptoms can be attributed to different causes , not related to fibroids ( e.g. , dysfunctional metrorrhagia of perimenopausal period )  . according to literature data , the main causes of treatment failure are represented by the development of new fibroids , regrowth of myomas not completely avascularized and concomitant presence of adenomyosis [ 2325 ]  . 
in line with these data , we observed the growth of new fibroids in 7 ( 38.8% ) of 18 patients within our cases who showed a symptomatic recurrence , while in the other 7 we have verified 1 3 394 la radiologia medica ( 2018 ) 123 : 385397 the reappearance of vascularization , with resulting fibroid regrowth , expression of initial incomplete devascularization . 
one possible explanation is that , as previously mentioned , the volumetric reduction of dominant fibroid and uterus is not always connected to an improvement of symptoms [ 12 ]  . 
this information is in contrast with previous studies on factors influencing the procedure outcome [ 17 , 21 , 2631 ] , but is in harmony with some data related to outcome of laparotomic myomectomy [ 3234 ]  . 
this could be explained by the fact that women who have symptomatic uterine fibroids during younger age may have a more active form of disease , and thus be exposed to a greater risk of recurrence either after embolization , or after myomectomy . 
a further explanation could be that young women ( after every conservative treatment ) have a greater amount of time to develop new ailments until the beginning of menopause . moreover , we have observed that women with a laparoscopic myomectomy history have an increased risk of procedure clinical failure , about 4 times higher if compared to women without previous surgery . 
 furthermore , considering the acknowledgement of high - frequency utero - ovarian anastomoses ( which can fuel fibroid vascularization ) in women who have already performed a pelvic surgical treatment [ 36 ] , we can assume that this group of patients can show incomplete embolization with a higher frequency . 
in the matter of our study the overall complication rate , equal to 7.4% , is comparable to that reported in other cases [ 23 ] and confirms that the morbidity of this procedure is inferior to that reported in myomectomy ( 38.6% ) and hysterectomy ( 40.1% ) literature [ 38 ]  . 
 specifically , we found 17 ( 6.7% ) cases of fibroid expulsion , 3 during the first month after the procedure , 11 in the first 6months , 3 after the second year of follow - up . 
the expulsion of fibroid is the most frequent complication after ufe , and is reported in more than 10% [ 11 , 23 ] of patients , recognizing as pathogenic mechanism , a drastic size reduction of lesions , and their subsequent protrusion into the uterine cavity . 
the phenomenon is most common in the case of submucosal fibroids or intramural fibroids with a remarkable submucosa component [ 23 ]  . small submucosal fibroids can be spontaneously expelled through vaginal way , while removal would be required in cases of partial ejection of intramural / submucosal or transmural voluminous fibroids , by resectoscopy or vaginal myomectomy treatment [ 23 , 29 ]  . 
considering our clinical records , 17 fibroids were expelled , 2 of which were submucosal , intramural / submucosal ones were 9 , and 6 fibroids completely affected the uterine wall . 
imaging studies ( pelvic ultrasound , mri and diagnostic hysteroscopy ) performed on 17 patients after the expulsion , have shown a rapid reactivation of normal myometrial and endometrial architecture . 
 this confirms , in agreement with what has been already highlighted by some studies in literature [ 18 , 40 , 41 ] , that the expulsion of embolized fibroid , if not complicated by superinfection , represents a stage of uterine wall structural rearrangement process in response to received treatment and as such can be considered a real cure . 
on 24 patients in our study who had one or more pedunculated fibroids , there was only one case ( 4.2% ) of acute pelvic pain onset for a partial detachment of a fibroids pedicle that required an urgent laparoscopic myomectomy 5months after the procedure . the presence of pedunculated fibroids ( fibroids with a diameter of less than 50% of the maximum diameter of a fibroid ) was considered , until a couple of years ago , a contraindication for procedure execution , in relation to potential risks of torsion of pedicle fibroids and following ischemic necrosis , and possible detachment of fibroid from uterus , with the necessity of urgent surgery [ 42 , 43 ]  . 
however , the increased morbidity associated with pedunculated fibroids presence has been recently proved to be wrong by results coming from several case studies , which have noticed no significant differences in post - procedural complication rates between women with and without subserosal pedunculated fibroids [ 4345 ]  . in our batch we had no infectious complications , no bleeding and no potentially mortal event . the possible impact of this procedure on reproductive potential is a topic of particular relevance especially because most of the potential female candidates for embolization are aged between 30 and 40years . 1 3 la radiologia medica ( 2018 ) 123 : 385397 an important aspect in such context is radiation exposure during the procedure , keeping in mind that ovaries are among the most radiosensitive organs . the radiation exposure varies according to fluoroscopy duration , operators experience , number of angiographic sequences performed [ 46 , 47 ]  . 
one of the first studies on the dosimetric evaluation of ovarian radiation exposure during the embolization procedure , had documented an average fluoroscopy time of 21.89min and a mean ovarian dose of about 22 : 34cgy [ 48 ] , comparable to that needed for lower gastrointestinal series and for iliac angioplasty , but greater than that observed for an abdominal ct scan , or for common fluoroscopic procedures ( hysterosalpingography , tubal recanalization )  . 
however , the main lines of literature report amenorrhea onset ( transient or permanent ) , associated with other symptoms of ovarian failure in more than 5% of cases [ 12 , 51 ]  . 
almost all of these cases are reported in women older than 45 , but have also been reported episodic cases of ovarian failure in younger patients [ 19 , 5254 ]  . 
the most valid etiopathogenetic hypothesis is that of a secondary ovarian hypoperfusion to nontarget embolization [ 54 , 55 ] through collateral uterine ovarian cycle or a flow inversion in ovarian arteries after uterine arteries bilateral occlusion . 
 many literature studies have tried to evaluate ovarian function through plasma fsh dose ( on the third day of menstrual cycle ) before and after treatment in groups of women with different age . 
most of these studies have not found changes in fsh levels after treatment [ 5658 ] and reduced reproductive potential was attested only in few cases [ 59 ]  . 
two casecontrol studies ( prospective and long - term ones ) have confirmed with a combined evaluationultrasound ( ovarian volume and follicular count ) and clinical ( fsh and estradiol plasma dose on the third day of menstrual cycle ) of ovarian functionality changes , that : the procedure does not have effects on ovarian reserve in women under 40years of age and does not accelerate menopausal process in older women [ 60 , 61 ]  . 
moreover , post - embolization amenorrhea may be due to a massive ischemic injury found at endometrial level , which can cause atrophy [ 62 ] or formation of secondary intrauterine synechiae to chronic inflammation processes associated with tissue necrosis [ 6365 ]  . 
in one case , a woman of 44years with normal fsh and lh levels , a hysteroscopic and histologic diagnosis of endometrial atrophy was made , 3months after the procedure . 
in the second case , a woman of 48years who experienced the onset of chronic pelvic pain , 10months after the treatment , the hysteroscopic examination revealed the presence of intrauterine synechiae , which were lysed with consequential symptoms remission . 
it must be observed that only for two of the 67 patients in our clinical record , who had fibroids with an important submucosal component , we detected endometrial damage after the procedure . 
these two cases can be dated back to earlier stages of our clinical trial , when pretreatment direct evaluation ( hysteroscopic ) of endometrial cavity was not routinely performed yet . subsequently , hysteroscopy has become a crucial survey of our pretreatment diagnostic procedure either to exclude concurrent endometrial pathologies ( polyps , hyperplasia , etc . ) , or to have more accurate determination of adverse effects probability ( spotting , ejection ) after the procedure , to provide adequate counseling to women wishful of becoming pregnant . there are numerous series in literature showing uncomplicated pregnancies after embolization [ 52 , 6671 ]  . 
 these reports demonstrate the possibility of spontaneous conception and pregnancy complete development ( after embolization ) , but also suggest an increased miscarriage risk ( 2760% ) , premature birth ( over 28% ) , fetal malposition ( 17% ) , caesarean section ( over 50% ) , low birth weight ( 7% ) , abnormalities in implantation and placentation processes ( 7% ) and also a higher risk of postpartum hemorrhage ( 1320% ) if compared to general population tendency . 
this rate , in first hypothesis , can be mostly linked to a higher maternal age at the time of birth ( 40.5years , range 3445 ) than to procedure execution . we had three successful pregnancies ; patients age at conception was 30 , 31.6 and 39years , respectively . 
we have not detected the appearance of fibroids - related symptoms either during pregnancy period ( threatened abortion , threatened premature delivery , pain 1 3 396 la radiologia medica ( 2018 ) 123 : 385397 symptoms , untimely placental abruption and / or abnormal bleeding ) or in postpartum ( uterine atony , postpartum bleeding )  . conclusions our experience in ufe leads us to conclude that for the vast majority of women with symptomatic uterine fibroids , this procedure is an excellent alternative to traditional surgical therapy , not only for its safety and tolerability but also for its high effectiveness in short , medium and long term . moreover , as already documented in literature , this therapeutic modality offers objective and significant socioeconomical benefits if compared to traditional surgical therapies , especially in reducing hospital stay and convalescence period , with a resulting faster recovery of patients daily activities . 
even if data on reproductive potential effects of this therapy are still clashing , the number of pregnancies without complications is increasing , both spontaneous or secondary with assisted reproductive techniques , and is reported in women who underwent embolization therapy . 
 this data give us a wide margin for such treatment extension to those women wishful of future pregnancy chance . funding the authors state that this work has not received any funding . compliance with ethical standards guarantor the scientific guarantor of this publication is alessandro cina , md . conflict of interest the authors of this manuscript declare no relationships with any companies , whose products or services may be related to the subject matter of the article . statistics and biometry one of the authors has significant statistical expertise . 
causes of vascular injury were divided in high - energy trauma ( n = 6 ) , iatrogenic ( n = 3 ) and penetrating injuries ( n = 3 )  . 
imaging findings included active haemorrhage , pseudoaneurysm and focal dissection . results embolization was performed with microcoils in all patients ; complete thrombosis was obtained in four patients by additional injection of spongostan pledgets and in two patients with 300500m particles . 
no patient required emergency surgery or subsequent surgical treatment . conclusion transcatheter embolization offers an effective , efficient and safe alternative to conventional surgical management of ima injuries . keywords internal mammary artery arterial injury angiography transcatheter embolization introduction internal mammary artery ( ima ) injuries are rarely reported in literature ; however , its lesions are capable of causing massive intrathoracic bleeding and life - threatening events . 
the leading cause of ima injuries is trauma [ 1 ] ; however , a clear majority ima injuries are iatrogenic , caused by , for instance , central venous catheterization [ 2 ] , pericardiocentesis [ 3 ] or sternotomy [ 4 ] or secondary to a systemic disease ( connective tissue disease or inflammatory vasculitis ) [ 5 ]  . imaging findings of ima injuries are often non - specific and include anterior mediastinal haemorrhage , possibly * fabio corvino effecorvino@gmail.com interventional radiology department , aorn a . 
cardarelli 9 , 80131naples , italy 2 department ofradiology , university ofnaples parthenope , naples , italy with evidence of active bleeding , hemothorax , pseudoaneurysm , arteriovenous fistula and associated fracture of the ribs , clavicle or sternuto avoid potential complications , urgent diagnostic setup to localize the source of bleeding and subsequent appropriate therapy is necessary when such patients present to the emergency room [ 6 ]  . control of bleeding can be achieved either by surgery ( surgical ligation ) or minimally invasive transarterial embolization . 
informed consent for data collection was obtained from all conscious patients . preprocedural imaging ima injuries were initially identified on computer tomography angiography ( cta ) in 11 patients and in 1 patient the diagnosis was suggested by an ultrasound study with colourpower doppler . cta ( lightspeed vct 64 slice ct , ge healthcare , milwaukee , us ) imaging was obtained both before and after intravenous administration of 120ml of 300 mgi / ml iodinated contrast medium ( ultravist , guerbet , roissy , france ) using an automatic injector at a flow rate of 4ml / s , followed by 40ml saline solution at the same injection rate . 
arterial phase was performed with bolustracking technique , placing the region of interest ( roi ) on descending aorta ( at the supradiaphragmatic level ) with a 100 hu threshold higher than baseline density . 
indirect diagnostic findings suggestive for ima injury were anterior mediastinal hematoma , haemothorax , extra - pleural hematoma , pneumothorax , rib fractures , sternum fracture , hemopericardium and cardiac tamponade . 
moreover , these findings can be combined with each other . in one case that developed haemodynamic instability immediately after a central vein catheterization done in our department , the diagnosis was suggested on us study with colour doppler , confirming the presence of a pseudoaneurysm characterized by typical appearance of swirl pattern of blood flow in the lumen on colour imaging ( the typical yinyang sign ) [ 9 ]  . technique all procedures were performed by interventional radiologists . 
ima embolization procedure was carried out under continuos cardiovascular and respiratory monitoring assisted by an anaesthesiologist in the angiography suite ( artis zee , siemens healthcare , enlangen , germany )  . 
after obtaining a vascular access by placing a femoral 5f sheath , selective catheterization and angiography of the subclavian artery omolateral to ima vascular injury were obtained using a sim - 2 , h - 1or ver - type catheter . 
the microcatheters were inserted as near as possible to the vascular lesion performing embolization more distally to minimize devascularization . selection of embolic agents was based on the physicians personal experience and preference . 
the main embolic material consisted in 0.018 - inch platinum microcoils ( cook medical , bloomington , in , usa ) used in 12 patients ( fig.1 ) ; the size of the coils were chosen so that they would be slightly larger ( e.g. , 23mm coil for a diameter of vessel of 23mm )  . 
moreover in 4 of 12 patients , the complete thrombosis was obtained by additionally injection of spongostan pledgets ( spongostan , johnson & johnson , usa ) ( fig.3 ) ; in other 2 patients , in addition to microcoils , the procedure was completed by injection of 300500m embosphere particles ( merit medical systems , south jordan , ut , usa )  . 
spongostan pledgets and embosphere particles was additionally injected to secure coil - induced thrombosis . the success of procedure was defined as complete conclusion of blood flow into the lesion with cessation of the haemorrhage on post - embolization angiography . 
a chest ct demonstrated a mixed density right - side anterior mediastinal haematoma compressing right heart with an internal focus of active bleeding ( circle ) , haemorrhagic pleural effusion ( arrowhead ) and haemopericardium ( arrow ) ; b superselective acute angiogram of right ima demonstrated an active bleeding from a penetrating branch ; c final angiogram demonstrated complete exclusion after coil embolization of active bleeding observation was performed for all the patients after the procedure . study endpoints anddefinition study endpoint includes technical success , clinical success , assessment of minor or major complications . 1 3 la radiologia medica ( 2018 ) 123 : 369377 fig . 
c coil embolization with back - door front - door technique with complete exclusion of source of bleeding technical success was defined as complete cessation of contrast extravasation and disappearance of pseudoaneurysm or arteriovenous fistula after embolization procedures . clinical success was defined as clinical and radiographic absence of bleeding ; in cases where there is no available follow - up imaging , no recurrent decrease of haemoglobin , no need for blood transfusion , haemodynamic stabilization , no 1 3 374 la radiologia medica ( 2018 ) 123 : 369377 fig . 
a mpr sagittal ct image demonstrate sternum fracture ( arrow ) and a central anterior mediastinal hematoma with an internal focus of active bleeding ( circle ) ; b , c selective angiogram of left ima confirms extravasation of contrast , successfully embolized with coils and additionally injection of spongostan pledgets ; d , e superselective angiogram of right ima demonstrate a focal dissection ( arrowhead ) with severe vasospasm , successfully embolized with coils need for subsequent surgical treatment and being discharged after recovery were defined as clinical success . late success was defined as the absence of repeat bleeding during follow - up , without the need for a repeat endovascular procedure or a subsequent surgical operation . complications were classified as minor or major , according to the definition of complications established by the cardiovascular and interventional radiology society of europe [ 10 ]  . results high - energy trauma ( n = 6 ) , iatrogenic ( n = 3 ) and penetrating injuries ( n = 3 ; two gunshot injuries and one stab wound ) were the causes of ima injuries . 
two blunt trauma victims had bilateral ima injury ; thus , there were a total of 14 ima injuries in 12 patients . diagnostic ct demonstrates direct sign of ima injuries in 13 cases ( actively bleeding vessel in 8 cases , pseudoaneurysms in 4 cases , focal dissection in 1 case )  . 
indirect ct findings were anterior mediastinal hematoma ( seven patients ) , hemothorax ( six patients ) , extra - pleural hematoma ( four patients ) , pneumothorax ( two patients ) , hemopericardium ( two patients ) , rib fractures ( one patient ) , sternum fracture ( one patient ) , and cardiac tamponade ( one patient )  . 
 in one case , us study , carried out immediately in a patient that developed haemodynamic instability after a central vein catheterization , suggested the presence of a pseudoaneurysm on swelling cutaneous tissue next to puncture site . diagnostic ima angiography confirmed the pre - procedural imaging findings ; all the patients underwent transcatheter embolization . 
of 12 patients , 6 had left ima injury , 4 right ima injury and in 2 bilateral injury . technical success was obtained in all patients ( 100% ) demonstrated by complete occlusion of vascular lesion on post - embolization angiography . the overall clinical success rate was 83.3%. 
 no minor complication was registered . no one of 12 patients presented a new episode of bleeding during follow - up , without the need for a repeat endovascular procedure or a subsequent surgical operation . evaluation of length hospital stay was impossible due to coexisting injuries ( especially in the blunt trauma group )  . discussion ima injuries are a tricky problem because they are rare , hard to diagnose and open to different treatment options . 
on ima injury post - blunt trauma yielded 49 cases being reported over 37years [ 1 ]  . the first report describing a case of ima injury dates to the 1930s [ 13 ] and the first case treated with gianturco coils 1 3 la radiologia medica ( 2018 ) 123 : 369377 embolotherapy is believed to be in 1982 described by smith etal . 
 [ 14 ] , a case of ima injury after high - energy trauma . the ima arises from the concavity of the first part of the subclavian artery and immediately passes downwards , forwards and medially , lying upon the pleura in the upper intercostal spaces up to the third costal cartilage ; subsequently , it continues anterior to the transversus thoracic muscle ending in the sixth intercostal space by dividing into musculophrenic arteries and the superior epigastric [ 115 ]  . 
in its course , ima passes lateral to the sternum and for this reason is subject to injury by blunt trauma cases that involve sternal fractures or by penetrating parasternal injuries [ 6 , 7 ]  . 
moreover , also iatrogenic cause of ima injury are related to its anatomically course : inadvertent puncture of ima for insertions of central venous catheters in non usguided access to the subclavian vein [ 2 ] ; aesthetic surgery , especially in breast augmentation where hematoma is a selflimiting common adverse event , but when , large diameter of ima perforators has been injured , conservative management cannot control massive continuous bleeding [ 16 ] ; pericardiocentesis , pacemaker lead insertion or thoracic major surgery can injury ima directly [ 3 , 4 ]  . ima is characterized by a rich potential collateral network with thoracic cavity , especially with mediastinum and pericardium , and with chest wall , maintaining communication to the distal part of the superior epigastric artery , the anterior intercostal branches and the musculophrenic artery . 
 this network allow to produce , in cases of its injury , a variety of clinical symptoms ranging from hemothorax , pericardial effusion / tamponade to mediastinal or extra - pleural hematoma rendering the vessel expendable without risk of ischemia / infarction following embolization [ 17 ]  . 
to prevent retrograde filling of ima pseudoaneurysms from collaterals , we employed the technique back - doorfront - door consisting of vessel occlusion both distal and proximal to the injury . the ima is small in size ( mean size : 23mm ) , but its average blood flow is of 60ml / min , which under different conditions can increase to as much as 150ml / min , resulting in a potentially 1 - l blood loss in a few minutes [ 18 , 19 ]  . multidetector ct angiography provides a time - efficient method for planning therapy in patients with acute bleeding , showing accurately the anatomic location of bleeding and the probable vascular origtherefore , diagnostic ct must be used as a guide for angiographic or surgical intervention ; additional information provided by ct angiography leads to faster catheterization of bleeding vessel and subsequent embolization [ 21 ]  . digital subtraction angiography ( dsa ) has been considered the gold standard for the detection of ima injuries ; moreover , if a haemorrhage source is identified , dsa allows to treat by superselective embolization minimizing potential complications [ 722 ]  . 
in cases where dsa show an ima truncated ( as in focal dissection ) and not actively bleeding , the decision whether to embolize is very tricky ; in our study and experience , we have an aggressive approach toward these types of arterial injuries because of the unpredictable nature and natural history of arterial injuries [ 23 , 24 ]  . 
 in acute phase , an ima injury can potentially retract itself achieving temporary hemostasis connected to hypotension and arterial spasm ; however , delayed bleeding may ensue once the patient is resuscitated with severe consequences as lethal shock in 45% of patients [ 1 ]  . besides the potential complications inherent in any embolization procedure , embolization of a non - bleeding but transected ima may have negative consequences for the patients later on the life . 
the ima is the preferred conduit for coronary artery by - pass grafting because of its patency rates at 10years is about 90% [ 25 ]  . the alternative treatment method to transcatheter embolization is emergent open surgical thoracotomy with artery ligation [ 26 ] ; in our series , we reported a high rate of technical and clinical success , with a very low complication rate , and surgical approach was not performed in any patient . 
reported a series of 19 ima injuries in 18 patients , with 12 patients underwent transcatheter embolization and 6 surgically managed ; the success rates for the patients were 91.6 and 66% , respectively , demonstrating the effectiveness of transcatheter embolotherapy of ima injuries [ 7 ]  . 
reported a series of five patients with iatrogenic ima injuries successfully treated by microcoils embolization in the absence of procedure - related complications or surgical exploration needing [ 2 ]  . 
subsequently , several articles , only case reports , exist , all of that treated successfully by coils transcatheter embolization [ 3 , 4 ]  . considering that for efficient treatment of vascular injuries , the choice of embolization material is important , the material should be chosen according to the site , size and flow pattern of the vessels to be occluded , material availability , and the experience of the interventionalist . 
the main disadvantage of coil embolization is that usually more than one coil is required for adequate occlusion , which increases the cost and time of the procedure [ 27 ]  . 
moreover , if the source of bleeding is close to the subclavian artery , to avoid coil migration it is possible to use detachable coils , which are removable if they dislocate into the subclavian artery . additionally , we used spongostan pledgets in four patients and embosphere particles in two patients to promote rapid thrombosis within the coils . 
we preferred to occlude 1 3 376 la radiologia medica ( 2018 ) 123 : 369377 ima with coils and subsequently , injection of liquid embolic agents at the end of the procedure for extra safety . 
 spongostan is a temporary embolic agent , with recanalization usually occurring within 520days ; its use alone is not preferable because of the high risk of recurrence of haemorrhages at multianastomosis sites [ 28 , 29 ]  . 
 therefore , we use it in combination with coils and not as single embolic material for the risk of bleeding recurrence . no papers in literature have reported the use of n - butylcyano - acrylate ( nbca ) in treatment of ima injuries . 
the use of nbca is largely described in treatment of spontaneous hematomas with high technical and clinical success rate [ 32 ] ; its use can be proposed so in the treatment of ima injuries , especially in cases when microcatheters cannot be navigated to reach distal targets . complications related to interventional embolization procedure are rare [ 1 ]  . 
we did not encounter any of these ones in our series . the limitations of our study are the small number of patients , its retrospective design and the lack of a control group treated surgically ; because this type of lesions is rare and surgical treatment is more invasive , it is impossible to conduct a prospective randomized trial with a high number of patients to compare outcomes of the percutaneous and open approaches . 
percutaneous angiography with selective embolization is associated with high technical and clinical success rates allowing direct identification of the bleeding vessel , immediate control of the source of bleeding and replacement of the need for open surgical thoracotomy with artery ligation , avoiding general anaesthesia and enabling immediate recovery of the patient . 
a summary of these recommendations is here reported . materials and methods a multidisciplinary approach was used to establish the working group by involving radiologists , interventional radiologists , neuroradiologists , interventional cardiologists , occupational health specialists , medical physicists , radiation protection experts , radiographers and nurses . 
three main topics have been addressed : patient radiation protection ( summarized in ten golden rules ) ; staff radiation protection ( summarized in ten golden rules ) ; and education / training of interventional radiology professionals . results in the golden rules , practical and operational recommendations were provided to help the professionals in optimizing dose delivered to patients and reducing their own exposure . 
operative indications dealt also with continuing education and training , and recommendations on professional accreditation and certification . conclusions the consensus conference was the methodology adopted for the development of these recommendations . 
orsola - malpighi university hospital , via massarenti 9 , 40138bologna , italy 2 abdus salam international centre fortheoretical physics , trieste , italy 3 department ofmedicine epidemiology andenvironmental sanitation , istituto nazionale perlassicurazione contro gli infortuni sul lavoro ( inail ) , rome , italy 4 national centre forinnovative technologies inpublic health , istituto superiore di sanit ( iss ) , rome , italy introduction the number of fluoroscopically guided interventional ( fgi ) procedures is increasing as they may offer advantages compared with clinical interventions , such as surgical , aiming at the same medical outcome : shorter stays in hospital ; less risks and discomforts for the patients ; general anaesthesia usually not needed ; and last but not least in the current strong budget - controlled healthcare systems , less costs . the fgi practices comprise both diagnostic and interventional procedures , usually performed by percutaneous access and under local anaesthesia and / or intravenous sedation , where fluoroscopic and fluorographic images are used for : localizing the lesion or treatment site , monitoring the procedure , and controlling and documenting the therapy [ 1 , 2 ]  . 
due to the widespread diffusion of fgi procedures and , in some of them , to the high radiation doses delivered to patients and / or the vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 378384 staff , the related dose management and radiation protection are strictly controlled by law . 
 187 / 2000 [ 3 ] , transposition of the european commission ( ec ) directive 97 / 43 / euratom [ 4 ] , specifies that the interventional radiology ( ir ) procedures are special practices involving high doses to the patient . 
the council directive 2013 / 59 / euratom [ 5 ] , states that member states shall ensure that appropriate medical radiological equipment , practical techniques and ancillary equipment is used in medical exposure involving high doses to the patient which may be the case in interventional radiology special attention shall be given to quality assurance programmes and the assessment of dose . 
 as this directive will repeal the directive 97 / 43 / euratom with effect not later than 6 february 2018 , the need for national and international guidelines is pressing . 
the referral guidelines for medical imaging taking into account the radiation doses are expressly requested by the law to comply with the justification principle , while the agreed standards for good medical radiological procedures , with modification of practices where appropriate are auditable criteria for reviewing medical radiological procedures to improve the quality and outcome of patient care [ 5 ] to comply with the optimization principle . in italy , the national institute of health ( istituto superiore di sanit , iss ) is the public advisory body of the ministry of health for radiation protection regulation of aspects related to the risk of ionizing radiation in medical fields , whereas the national workers compensation authority ( istituto nazionale per lassicurazione contro gli infortuni sul lavoro , inail ) guarantees the radiation protection of the workers also in the medical field . 
those two authorities already cooperated in the past for addressing reference documents for the radiology practices [ 6 , 7 ] and recently proposed to establish an italian working group on interventional radiology ( iwgir ) to develop national recommendations for the optimization of patients and operators exposures , tightly related in fgi procedures . 
the proposal was fully accepted by all italian scientific / professional societies and competent authorities involved in the fgi practices , selecting qualified members for the iwgir . the recommendations are here presented and commented as a summary representing an example of national indicative operations from relevant medical scientific societies and the competent authority [ 5 ] as requested by the european legislation . materials andmethods the iwgir was composed of professionals working in the field of interventional radiology and interested , as stakeholders , to radiation protection of patients and staff . 
 the represented scientific and professional associations were : the italian society of medical and interventional radiology ( societ italiana di radiologia medica e interventistica , sirm ) , the italian association of diagnostic and interventional neuroradiology ( associazione italiana di neuroradiologia diagnostica e interventistica , ainr ) , the italian society of interventional cardiology ( societ italiana di cardiologia interventistica , gise ) , the italian association arrhythmology and cardiostimulation ( associazione italiana di aritmologia e cardiostimolazione , aiac ) , the italian association of medical radiation protection ( associazione italiana di radioprotezione medica , airm ) , the italian association of medical physics ( associazione italiana di fisica medica , aifm ) , the national professional association of qualified experts ( associazione nazionale professionale esperti qualificati , anpeq ) , the italian association of radiation protection ( associazione italiana di radioprotezione , airp ) , the national federation professional colleges of radiographers ( federazione nazionale collegi professionali tecnici sanitari di radiologia medica , fncptsrm ) , the italian association of interventional radiographers ( associazione italiana tecnici di radiologia interventistica , aitri ) and the national federation nursing colleges ( federazione nazionale collegi infermieri , ipasvi )  . the working group , operating as a consensus conference , started from both a critical revision of the literature and the results of previous surveys coordinated by iss [ 8 ] and inail [ 9 ] , and then developed the recommendations [ 10 ] where the role of various professionals in fgi , the recommendations for patients and staff dosimetry , radiation protection and optimization of exposures , and the content of the necessary second level education and training of professionals were described . 
the iwgir achieved consensus through six facilitated consensus meetings , attended by all of the above stakeholders , from september 2013 to june 2015 . the subject was divided into three main topics : radiation protection of patients , radiation protection of operators , and education and training of ir professionals . 
the first and second sections were then summarized in a few recommendations provided in the form of ten short and practical golden rules . the use of diagnostic reference levels ( drls ) to reduce the stochastic risk of patient exposures and the trigger of alert levels to prevent skin burns from radiation was introduced and recommended in fgi procedures . 
suggested numerical values were derived from the international literature and national surveys , but , due to the presence of a widespread range of doses in interventional radiology even for the same procedure [ 1114 ] , the recommendations [ 10 ] provided references for each given value and technique as a tool for referrers in systematic comparisons . 1 3 380 results informed consent an informed consent , specifically for ir procedures , is suggested in the document [ 10 ] and shortly described and commented in table1 . 
the fgi procedures could deliver high skin doses and be repeated in short period of time on the same patient ; therefore , the informed consent should include the information on potential skin tissue reactions ( skin burns ) with the recommendation of consulting the medical specialist if erythema and / or epilation appears . golden rules forpatient exposure optimization the golden rules for patient radiation protection were divided into four subtopics : general , before , during and after procedure . 
the ten main golden rules for patients ( grp ) provided by the document [ 10 ] are shown in table2 . in particular , as italian legislation does not provide drls for interventional procedures yet , the iwgir suggests a comparison of local patient doses with the literature data , national survey data or international diagnostic reference levels , some of them being reported in tables3 , 4 . 
moreover , the procedure complexity is influenced by patients anatomy and lesion severity and could strongly affect the patient exposure : thus , a complexity index that could scale appropriately the drl has been introduced , and iwgir is proposing possible multiplication factors as a function of the procedure complexity for some interventions ( table5 ) , derived from the literature [ 15 , 16 ]  . 
because conventional approach can be particularly difficult in fgi procedures where several types la radiologia medica ( 2018 ) 123 : 378384 of images and cine frame are used ( such as fluoroscopy , planar , digital subtraction angiography and cone beam ct images ) , the iwgir suggests an image quality criteria approach , based on the literature [ 17 ]  . 
quality criteria can include both clinical criteria , related to the level of visualization of anatomical markers in the images , and technical criteria , based on operational aspects influencing both patient exposure and image quality . 
as an example , in the case of coronary angiography , visualization of collateral circulation when present and simultaneous and full opacification of the vessel lumen at least until the first flow - limiting lesion ( in general > 95% by visual estimation ) are clinical and technical criteria , respectively . golden rules forstaff exposure optimization as far as the golden rules for operator ( gro ) radiation protection are concerned , the priority was given to practical and operational recommendations that could help the professionals to reduce the dose to themselves by reducing , in many instances , the dose to patients too . 
a selection of the ten main golden rules for operators is reported in table2 . from an italian survey about the interventional cardiology procedures [ 9 ] ceiling shields , table curtain shields and protective eye lens glasses were pointed out as the less used radiation protection tools by operators : that would be a major critical issue in radiation safety as glasses and ceiling shields can reduce the eye lens dose from 5 to 33 times and from 1.2 to 33 times , respectively [ 18 ] ; then , their usage is mandatory ( as recommended by the gro#10 in table2 ) due to the much lower occupational eye lens dose limit for workers included in the new ec directive . 
indeed for the lens of the eye , the new limit on the equivalent dose shall be 20msv in a single year [ 5 ] vs the current italian legislation limit that is 150msv . 
in particular , the iwgir provides transmission factors for taking into account for the use of protective eye lens glasses : those factors shall be multiplied table 1 features of informed consent in interventional radiology procedures features comments 1 . 
the patient is not an expert in medicine and , based on his / her education and understanding , the information shall make clear the predictable risks in a way true and emotionally well balanced 2 . 
referred only to the procedure proposed to patient 1 3 la radiologia medica ( 2018 ) 123 : 378384 table 2 golden rules for radiation protection of patients and staff ( downloadable at : ry / publ / cont / 15_41_web.pdf ) patients general 1 . 
before to use an angiographic equipment make the optimization of the technical protocols selecting , for each protocol , the necessary and sufficient image quality to perform the clinical task 2 . 
for high - dose interventional procedures adopt alert ( trigger ) levels of the cumulative air kerma ( ck ) or of the kerma area product ( kap , dap ) to inform operator when in a complex procedure the skin dose can have reached a threshold for skin injuries ; make the follow - up of patients that may have received high skin doses ( > 3gy ) before an ir procedure 5 . 
acquire the exposure history of the patient to recognize previous high - skin - dose ir procedures and , in the case , make an effort to modify x - ray beam incidences to spare yet exposed skin areas during the ir procedure also image and pulse rate 6 . 
maximize distance between the x - ray tube and the patient to the extent possible and minimize distance between the patient and the image receptor : for a frontal projection , keep the x - ray tube under the patient table 2 . 
use pulsed fluoroscopy ( with the lowest frame rate possible to obtain images of acceptable quality ) rather than continuous and low - dose fluoroscopy ( if possible ) ; in the case of children , remove the antiscatter grid where appropriate 4 . 
use collimation : collimating properly the x - ray beam to the area of interest both reduces the patient dose and improves the image quality due to the less scattered radiation 8 . 
when using lateral angulated projections , stand on the side of the transmitted beam ( that is , by the image receptor , not by the x - ray tube ) , if possible 10 . 
use properly : personal radiation protective devices ( apron , thyroid collar , leaded glasses with side protection as appropriate ) ; fixed / mobile radiation protective shields ( table curtain , ceiling suspended screens with repositioning when projection is changed ) ; personal dosimeters by the appropriate operational quantity for eye lens dosimetry , e.g. 
hp ( 3 ) [ 19 ]  . education andtraining ofir staff finally , continuous education , theoretical / practical training and information of medical staff ( as well as relevant competence in radiation protection ) , specific for different professionals , are mandatory in ir [ 5 ] according to national and ec regulations . 
a second level of education for practitioners shall include both radiation management of patient and staff and , due to the complexity of radiological equipment used in ir , equipment - specific training ( even in other facilities ) as appropriate . 
 [ 28 ] biliary drainage iliac artery angioplasty ft : 30min kap : 100gycm2 number of images : ft : 30min kap : 250gycm2 number of images : ft : 20min kap : 250gycm2 number of images : ft : 20min kap : 200gycm2 number of images : transcatheter arterial chemoembolization13 / embolization28 ft : 25min kap : 400gycm2 number of images : ft : 20min kap : 300gycm2 number of images : tips ( transjugular intrahepatic portosystemic shunt ) ft : 60min kap : 525gycm2 number of images : ft : 40min kap : 350gycm2 number of images : ft fluoroscopy time kap kerma area product table 5 complexity index and respective fluoroscopy time , number of images and kap values for percutaneous coronary interventions ( pci ) procedures complexity index [ ci ] kap [ gycm2 ] fluoroscopy time [ min ] number of images 1500 1700 2300 simple ( ci = 1 ) medium complex ( 1 < ci2 ) complex ( ci > 2 ) kap kerma area product discussion some of the golden rules for patients and operators are in a certain way overlapping as the patient is the main source of the scattered radiation for the staff , and therefore , limiting the patient dose will contribute to limit operator exposure as well . the introduction of drl in projection radiology , ct and nuclear medicine was a long and not easy process [ 4 , 21 ] : in a similar way , and likely even more , the use of drl in interventional radiology will require appropriate diligence for not being in times of trouble . 
therefore , drl in interventional radiology are likely to be introduced carefully : the range of values quoted by the iwgir is fairly extended ; thus , they may be adapted to different facilities and used as a benchmark , due to the lack of drls provided by law . the present methods for the maximum skin dose ( msd ) assessment are not providing real - time information to the operator : thus , alternative methods using the cumulative kerma area product ( kap ) or , better , the cumulative air kerma ( cak ) at the interventional point [ 22 ] are recommended . 
moreover , the ec directive defines interventional radiology as the use of x - ray imaging techniques to facilitate the introduction and guidance of devices in the body for diagnostic or treatment purposes : following that definition the iwgir used the same terminology , although well aware of how much these procedures are nowadays performed by physicians in many medical specialties and not only by radiologists [ 2 ] , requiring therefore specific education and training in radiation protection for ir after specialization as the basic courses were not equivalent or totally absent in several medical specialization schools . 
 the iwgir therefore stressed the value of continuing education and theoretical / practical training to provide further knowledge , competence and skills in radiation protection for ir healthcare professionals [ 10 ]  . a milestone of the evidence - based medicine is the hierarchical system of classifying evidence , also known as the levels of evidence [ 24 ] : the document of iwgir would be an evidence level 5 study , i.e. 
the proposed methodology proved to be both robust and reproducible for achieving 1 3 la radiologia medica ( 2018 ) 123 : 378384 the consensus in document development where so many different medical specialties are involved . 
the resulting standards for radiation protection in image - guided procedures should be implementable in the daily medical practice as in - the - field professionals agreed on them . future trends can be related to spreading the recommendations of iwgir throughout the country in order to develop more a patient / operator radiation protection culture and to have feedbacks by the physicians , medical physicists , radiographers and other professionals communities : even to this purpose , present version of the document ( in italian ) is currently available online at : / / www.iss.it / bina ry / publ / cont / 15_41_web.pdf , and an english version is expected within 2018 . 
scientific and professional societies are also distributing online the document and two posters containing grp and gro , respectively . conclusions in the medical use of ionizing radiation , continuous performance monitoring together with education and training programmes represents an essential process for promoting organizational , professional and patient - oriented practice improvement , besides fulfilling national and european legislations . 
this safety culture is even more needed in interventional radiology due to the potential high doses delivered to patient and staff , and to the wide spread of these miniinvasive technique in all fields of medicine . the methodology adopted for the development of this document with the contribution and agreement of all ir actors could provide a cross - specialty advice and thus can be seen as the winning approach for the distribution and practical implementation of the recommendations to reach a real impact on the optimization of the ir practices . italian working group on interventional radiology carlo bergamini , aou di bologna , retired since 2009 ; guglielmo bernardi , ao santa maria degli angeli , pordenone ; corrado bibbolino , irccs spallanzani , roma , retired since 2011 ; loredana dercole , fondazione irccs policlinico san matteo , pavia ; antonio donofrio , aorn dei colli ospedale v . 
monaldi , napoli ; maurizio isalberti , ospedale regionale di lugano , svizzera ; roberto moccaldi , consiglio nazionale delle ricerche , roma ; antonio orlacchio , universit degli studi di roma tor vergata , roma ; simone panci , ospedale san giovanni di dio , firenze ; emanuela piccaluga , ospedale niguarda c granda , milano ; ennio c . 
pathological animal and human post - mortem studies have confirmed the relationship between this radiological finding and the presence of gadolinium accumulation in vulnerable brain regions in patients with normal renal function . 
in this short communication , we report the case of a 15 - year - old patient affected by b - cell acute lymphoblastic leukemia ( ball ) who developed a hyperintense signal in the dentate nuclei following multiple administrations of a macrocyclic gbca . 
bufalini hospital , cesena , italy imaging department , bambino ges childrens hospital , rome , italy administrations , particularly following the exposure to linear gbcas [ 15 ]  . 
pathological animal and human post - mortem studies have confirmed the relationship between this radiological finding and the presence of gadolinium accumulation in vulnerable brain regions in patients with normal renal function [ 69 ]  . 
in this short communication , we report the case of a 15 - year - old patient affected by b - cell acute lymphoblastic leukemia ( ball ) who developed a hyperintense signal in the dentate nuclei following multiple administrations of a macrocyclic gbca . the purpose of this report is to discuss possible differential diagnoses of this radiological finding with special focus on the differentiation between iron or manganese accumulation , post - irradiation changes and gbca - related gd deposition , highlighting the importance of the acquisition of accurate clinical data to improve our scientific knowledge . case report a 15 - year - old boy first accessed our department in may 2013 for right lower limb paresthesia and strength deficit . 
 he had been diagnosed with b - cell acute lymphoblastic vol . : ( 0123456789 ) 1 3 470 la radiologia medica ( 2018 ) 123 : 469473 leukemia ( ball ) in 2010 in another hospital and was treated with chemotherapy until 2012 . 
during this period , according to patients clinical reports , he did not undergo any mr examination . the first mr scan was performed in our institution and revealed presence of central nervous system ( cns ) involvement within the left fronto - parietal cortex , which required mr follow - up . a total of 9 consecutive mr examinations were performed during the follow - up period between may 2013 and february 2016 , with a 3t scanner ( siemens skyra , erlangen , germany )  . the standard brain mr protocol with contrast administration included pre - contrast axial turbo spin echo t1 - weighted sequence ( repetition time / echo time : 500600ms / 9.96.4ms ; section thickness : 3mm ; spacing : 0.3mm ; field of view : 220mm ; matrix size : 256256 , flip angle : 138 and echotrain : 42 ) and axial t2 - weighted sequence ( repetition time / echo time : 8600 ms / 122 ms ; section thickness : 3mm ; spacing : 0.6mm , field of view : 220mm and matrix size : 384324 )  . the mean time interval between contrast administrations was 5months ( range : 116months )  . 
each mr examination was performed exclusively with the injection of the macrocyclic gbca gadoterate dimeglumine ( dotarem , guerbet , villepinte , france ) at a standard dose of 0.1mmol / kg body weight . 
in total , 100ml of gadoterate dimeglumine was administered . all mr images were visually inspected by two neuroradiologists and the dentate nucleus / pons signal intensity ratio was calculated on unenhanced t1 - weighted images with a roi - based method as previously reported [ 10 ]  . 
at visual inspection a bilateral and symmetrical hyperintensity of the dn is slightly visible at the 5th mr ( b ) and more clearly appreciable at the 8th ( c ) and 9th ( d ) mr examination . 
t2 - weighted images show no significant visible alterations of si during the entire follow - up ( eh ) 1 3 la radiologia medica ( 2018 ) 123 : 469473 fig . 
bmt : bone marrow transplantation a few months after the 9th mr examination , the patient was hospitalized for sepsis ; his clinical conditions worsened by developing respiratory failure , septic shock and heart failure which finally led to his decease in march 2016 . discussion over the past 2years , several studies have investigated t1 hyperintensity in deep brain gray matter nuclei , particularly the dentate nucleus ( dn ) and globus pallidus ( gp ) , following multiple administrations of linear gadolinium - based contrast agents ( gbcas ) [ 15 ]  . 
however , only few studies have provided histological proof confirming gd deposits in the brain tissue of human adults despite normal renal function and intact blood brain barrier [ 8 , 9 ]  . regarding the pediatric brain , only one study investigated the gbca deposit in brain samples , identifying heavy deposition of gadolinium within the dentate nucleus and throughout the cerebellar cortex after 4 injections of linear gbcas , without any visible dn hyperintensity on mri [ 11 ]  . macrocyclic gbcas have been also widely studied in this panorama , confirming their higher kinetic and thermodynamic stability compared to linear ones [ 12 , 13 ]  . 
although the brain deposit of gd has been demonstrated in human specimens even after the exposure to macrocyclic gbca injection [ 14 ] , the lack of visible dn hyperintensity afterthe administration of this class of contrast agentsis still debated . a possible explanation of the different signal intensities shown by macrocyclic and linear contrasts can be speculated based upon the different chemical forms of the gd deposit , as shown in the results of a recent study on rats [ 7 ]  . 
in this study , the residual gd found in the rat brain after repeated administration of linear gbcas was present to a large extent in insoluble form , which is most likely responsible for the brain hyperintensities observed in mr images . 
on the other hand , after administration of macrocyclic gbcas , the gd was only present in soluble small molecules [ 7 ] , which may lead to a different t1 signal intensity . our case involves a 15 - year - old boy who demonstrated bilateral and symmetrical dn hyperintensity following multiple injections of the macrocyclic agent gadoterate meglumine . 
our patient underwent a craniospinal irradiation for relapsing ball in the cns in 2013 , and the dn hyperintensity was visible on the 5th mr in october 2013 at first , so that a possible contribution may be speculated . 
these results seem to suggest a marginal role of radiotherapy in causing dn hyperintensity , although a possible compounding effect cannot be completely excluded . 1 3 472 la radiologia medica ( 2018 ) 123 : 469473 manganese accumulation must also be considered as a possible differential diagnosis for deep brain nuclei t1 hyperintensity , since our patient underwent parenteral nutrition during 2weeks in 2014 for an episode of acute pancreatitis . 
in fact , manganese deposition has been reported in association with parenteral nutrition and liver failure , showing bilateral hyperintensity of the gp on unenhanced t1 - weighted images as the most frequent cns localization [ 19 ]  . 
 [ 21 ] demonstrated significantly increased gadolinium liver concentrations ( glc ) in pediatric recipients of allogeneic hematopoietic stem cell transplants who underwent multiple mr examinations enhanced with gadoterate meglumine . 
although a reduction of glc was noted in patients that underwent deferoxamine chelation therapy , the authors hypothesized that in case of siderosis a possible interaction may occur between ferric ion and gadoterate meglumine [ 21 ]  . 
based on these results , we can similarly speculate that the findings shown in the case above could represent the result of possible interaction between the gbca and increased levels of ferric iron resulting from multiple transfusions , leading to gbca - related retention in a high - relaxivity form , thus explaining imaging findings on the 8th and 9th mr . the main limitation of this report is the absence of postmortem data : lacking of pathologic proofs , we cannot draw definite conclusions as to what the visible dn hyperintense signal represents in our patient . so far , the clinical impact of gadolinium - related retention in the brain tissues not associated with nsf has not been cleared , as well as the processes contributing to gadolinium accumulation . recently , the pharmacovigilance risk assessment committee ( prac ) of the european medicines agency ( ema ) issued a statement recommending the suspension of marketing authorizations for four linear gbcas [ 22 ]  . 
food & drug administration ( fda ) subsequently issued statements disagreeing with the prac recommendation [ 23 , 24 ] and emphasizing the absence of discernable clinical signs or symptoms associated with t1 hyperintensity or gd retention . 
despite these criticalities , emas final opinion confirmed the restrictions on use of linear gadolinium agents in body scans [ 25 ]  . in our patient , a clearly visible t1 hyperintensity was noted in the dn following 4 close injections of gadoterate meglumine . 
the patient never presented any cerebellar symptoms , which is in agreement with all published findings to date . in conclusion , regardless of the reasons for the hyperintense signal , this case should lead us to reflect on the limitations of our knowledge about gd pharmacokinetic and the possible role of the individual phenotype and susceptibility in the development of deep brain nuclei hyperintensities . compliance with ethical standards conflict of interest author l.p declares that he has no conflict of interest . 
 size - specific conversion factors were used to translate the recorded ctdivol into ssde according to the procedure described in the american association of physicists in medicine ( aapm ) report 204 . 
high dose levels and dose variations among hospitals reveal the need for standardization of scanning protocols and staff training on adoption of scanners dose reduction techniques . keywords size - specific dose estimates ( ssde ) computed tomography volume ct air kerma index introduction according to unscear global survey of medical radiation usage and exposures , ct scanning accounts for 43% of the total collective effective dose due to diagnostic medical radiology [ 1 ]  . 
ct scanning accounts for 7.9% of the total number of diagnostic medical examinations in health - care level i countries , just over 2.0% in health - care level ii countries and just under 14% in health - care level iii / iv countries * einas h . 
box3001 , 11111khartoum , sudan 2 department ofphysics , committee onradiation andenvironmental pollution protection , college ofscience , al imam mohammad ibn saud islamic university ( imisu ) , riyadh , saudiarabia [ 1 ]  . 
 epidemiological studies have failed to answer the various questions regarding cancer risk related to low radiation levels ; nonetheless , the data were robust and the topic is challenging [ 2 ]  . 
 accurate dose estimates are , therefore , essential for better protection of the patient receiving ct examination as well as other medical procedures utilizing ionizing radiation . in the european guidelines for ct , two quantities are proposed for setting diagnostic reference levels : ct dose index ( ctdivol ) per slice ( serial scanning ) or per rotation ( helical scanning ) and the dose length product ( dlp ) per complete examination [ 3 ]  . 
the ctdivol estimates the average dose within a scan volume from dose measurements made in a standard 16 - cm ( head ) or 32 - cm ( body ) ct phantodlp vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 424431 accounts for the total radiation dose delivered to the scanned region of the body , defined as the product of ctdivol and the scan length [ 3 , 4 ]  . the recommendations by the international electrotechnical commission ( iec ) in 2002 made it mandatory for all manufacturers to display both ctdivol and dlp on the screens of their ct devices [ 4 ]  . 
moreover , using ctdivol , the dose to patients smaller than the acrylic ct body phantoms ( 32cm ) is underestimated by as much as a factor of three [ 79 ]  . concerns over using ctdivol as a dose metric has led the american association of physicist in medicine to develop and recommend size - dependent conversion factors , which can be used to determine size - specific dose estimate ( ssde ) values from ctdivol values [ 10 ]  . 
the ssde corrects for the difference between the patient size and the acrylic ct phantom and offers an improved metric for expressing the average absorbed dose . at the national level , ct patient dose data are available in sudan in terms of ctdivol and dlp dose indices [ 11 , 12 ]  . 
 thus , it was the aim of this study to update the radiation exposure for adult patients undergoing multi - detector ct examinations at sudanese hospitals using size - specific dose estimates ( ssde )  . 
 the hospitals were in khartoum and medani states , representing the largest states in terms of population density and provide diagnostic services for a wide area around thethese hospitals were selected because these are among the largest in terms of workload . 
survey data were collected from the following hospitals : advance diagnostic center ( adc ) ; al - amal hospital ( amh ) ; antalia private clinic ( apc ) ; medani hospital ( mh ) ; ribat university hospital ( ruh ) ; national armed force hospital ( afh ) ; royal care hospital ( rch )  . 
due to the retrospective nature of the study , formal consents from the examined individuals were waived . dose determination dose information and scan parameters pertaining to the studied patients were retrospectively collected from the dicom header , including patient information ( age , gender ) , tube voltage , tube current , rotation time ( s ) , pitch value and ctdivol . for ssde calculations , we measured the diameter of the patients images using digital calipers on the scanner console . 
measurements were done for anteriorposterior diameter ( hereafter , dap ) and lateral diameter ( hereafter , dlat ) from the mid - slice location on the transverse ct image and dlat on scout images . 
next , the ssde was calculated by multiplying the console - displayed ctdivol with the size - specific conversion factors ( f ) given in the aapm report 204 [ 10 ] : ssde = ctdivol f  . descriptive statistics was used to analyze the study results . 
the correlation was considered statistically significant at p value less than 0.05. quality control measurements the parameters , which best characterize the image quality , were assessed by catphan 504 ct quality assurance phantom ( the phantom laboratory ltd , ny , usa )  . 
the survey showed that some centers use the protocols provided by the vendors and others use manual settings for the examinations , which could explain the variation in mas values recorded in the study ( table3 )  . 
also , it appeared that radiographers lacked training on how to deal with dose reduction techniques of the scanners . as detailed above , ssde was estimated via two ways : ( 1 ) from transverse images ( hereafter , ssdetrans ) using dap + lat as patient size ; ( 2 ) from scout images ( hereafter , ssdesco ) using dlat as patient size . 
the later correlation was statistically insignificant at p = 0.05. in table5 , a statistical summary is given for the studied ct doses [ mean , , range ( minmax ) , third quartile ] and max / min ratios . significant dose variations were presented , reflected by the maximum to minimum ratio of 11.04 ( chest ct ) and 18.62 ( abdominal ct ) , which is a clear indication that scan protocols were not standardized . discussion ctdivol provides a useful way to compare radiation output levels among different scanners . 
both patient body characteristics and the radiation output are better described by the ssde . performance ofmsct image quality assurance tests were performed , and the results were compared with the tolerance limits specified by the international electrotechnical commission [ 4 ]  . 
the equipment was not covered under regular qa program and thus baseline data for the tested qa parameters do not exist . concerning dose performance , ctdivol can be used as a suitable dose descriptor for ct scanner output . 
with the exception of 16 - slice ct at rch , one would conclude that multi - slice ct scanners tend to provide lower patient dose compared to the same type of ct with lower multi - detectors in a row . 
definite conclusions on performance of different types of msct could not be feasible in this study due to the limited number of scanners per model studied . ctdivol vs ssde as seen ( figs.1 , 2 ) , ssde values from transverse ct images and scout radiographs were significantly different compared to ctdivol . 
they agreed that for a given ct technique , patient dose decreases as patient size increases because there is more attenuation of the incident x - ray beam by surrounding soft tissues , necessitating adjustment according to patient size for appropriate ct dosimetry [ 15 , 16 ]  . 
the result was an increase in patient organ dose as a function of patient size , which was ascribed to the aec system that attempts to maintain constant image noise for all patient sizes [ 17 , 1921 ]  . on the other hand , the relation between the patient size and dose in chest ct scanning showed a different trend . 
in chest ct scanning and generally when scanning tissues having different density from water or pmma , ssde considerably underestimates the absorbed dose due to the much lower density of lung tissues in chest [ 23 ]  . to overcome this problem , the water equivalent diameter ( dw ) has been proposed that considers both the geometrical size of the patient and the inhomogeneity of the patients tissues [ 24 ]  . 
thus , further studies are needed to further improve current patient dose data using dw . comparison withtheliterature anddose optimizations to optimize the radiation dose delivered to patients during radiological procedures , estimated radiation doses should 1 3 430 la radiologia medica ( 2018 ) 123 : 424431 be compared against established diagnostic reference levels ( drls ) [ 25 , 26 ]  . 
examples of drls for abdominal ct are those recommended by the american college of radiology in the usa ( 25.0mgy ) , the health protection agency in the uk ( 14.0mgy ) [ 25 , 26 ] and the italian nationwide survey ( 18mgy ) [ 27 ]  . 
when our results ( 22.8mgy ) were compared with these drls , the current doses were comparable to the us drls . as seen ( table4 ) , inter - hospital dose ratiosmaximum to minimumare as high as 11.04 ( chest ct ) and 18.62 ( abdominal ct )  . 
survey results revealed an important room for dose optimization ; however , lack of proper training and inexperienced technologists are major obstacles to the full utilization of these features . conclusions to provide more accurate estimations of patient doses , the ssde metric was used in this study instead of ctdivol . 
in this study , we evaluated the safety in terms of toxicity and efficacy of using of 810 fractions schedules with helical tomotherapy ( ht ) for primary and metastatic lung lesions . methods between march 2014 and may 2016 , a total of 39 patients ( median age 72years , range 2691 ) were treated with ht - sbrt for malignant lung lesions : 22 patients with early stage nsclc , 17 with oligometastases . 
local control ( lc ) , overall survival ( os ) and toxicity rates were prospectively collected . results median duration of rt was 15days ( range 1026days ) and no interruption occurred . 
with a median follow - up of 13months ( range 329 ) , we reported one g2 pneumonitis ( 2.6% ) and one g2 chest pain ( 2.6% ) ; nog2 esophagitis was registered . 
stereotactic body radiation therapy ( sbrt ) has allowed an improvement of oncological outcomes with negligible toxicity , compared to conventional rt , specifically for medically inoperable early stage nsclc * francesco cuccia f.cuccia1@virgilio.it extended author information available on the last page of the article patients [ 26 ]  . 
the efficacy and safety of sbrt have also been documented in patients affected by oligometastatic disease , i.e. , the presence of 15 lesions [ 7 ]  . sbrt is typically delivered in a limited number of fractions over the course of 12 weeks [ 8 ]  . 
based on the toxicity data following sbrt for centrally located lesions [ 9 ] , a strategy of risk - adapted dose prescription was proposed to minimize sbrt - related adverse events , depending on the localization of target volumes within the lungs and proximity to mediastinal organs at risk ( oars ) [ 10 , 11 ]  . recent developments in lung sbrt , such as intensitymodulated rt ( imrt ) and image - guided rt ( igrt ) , have allowed a high accuracy of dose distribution to the target volumes and a more precise assessment of tumor volume changes during the course of treatment by means of imaging vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 406414 on - board , lowering high doses to nearby normal tissues [ 12 , 13 ]  . helical tomotherapy ( ht ) is a platform that combines imrt with in - built image guidance using megavoltage ( mv ) ct scanning . we report a single - center experience of 810 fractions schedule ht - sbrt for primary and single metastatic lung lesion . materials andmethods this is a retrospective mono - institutional study that received the ethics approval from our institutional ethic committee ; informed consent was acquired from all participants enrolled in this series . primary endpoint of the present study is the feasibility of ht - sbrt for primary and secondary lung malignancies ; local control ( lc ) , disease - free survival ( dfs ) and overall survival ( os ) are secondary endpoints . 
sbrt was indicated when the following criteria were satisfied : medically inoperable early stage nsclc , the presence of a single lung metastasis for oligometastatic patients , tumor size5cm , karnofsky perfomance status70 , a life expectancy of at least 6 months . early stage nsclc patients were staged with bronchoscopy , enhanced computed tomography ( ct ) scan of the lung and upper abdomen with contrast - medium and 18 - fluorodesossiglucose positron emission tomography ( pet )  . 
the biopsy was avoided in the presence of severe comorbidities ; in this scenario , the metabolic imaging was considered a surrogate of malignancy , according to the literature [ 14 ]  . 
the clinical target volume ( ctv ) , equal to the gross tumor volume ( gtv ) , was defined merging the treatment planning ct with a megavolt computed tomography ( mvct ) scan [ 1517 ]  . mvct is a free breathing slow ct able to give information relative to the full extent of target motion during respiratory movement , as recommended by aapm task group 101 report [ 16 ]  . 
different dose schedules were used according to the tumor site ( central or peripheral ) and maximum diameter of lesion : 6070gy in 810 fractions for peripheral lesions , 5060gy in 10 fractions for central lesions , 40gy in 10 fractions for ultra - central lesions . 
also patients frailty , tumor size and location ( especially for lesions whose ptv touches or extends into the ribs / pleura , or unable to meet the 3 or 5 fractions schedules constraints ) had an impact in fractionation selection process [ 18 , 19 ] , leading to schedules with bed10 > 100gy administered in 39% of cases , and schedules with bed10 < 100gy in 61% . 
dose constraints for oars were derived from peer - reviewed literature [ 8 , 10 , 20 ] : volume of the lung , excluding ptv , receiving 20gy ( v20 ) and 5gy ( v5 ) to 10 and 35% , respectively ; mean lung dose ( mld ) 9gy ; dmax28gy on spinal cord ; central airways , brachial plexus and esophagus dmax were limited to 40gy . 
all statistical analyses were carried out using stata / se 14.1 ( stata , corp lp , texas , usa )  . toxicity andfollowup adverse events were assessed according to the ctcae version 4.0. 
concerning pulmonary toxicity , patients who were asymptomatic with radiologic changes were not considered to have toxicity . contrast - enhanced chest ct was performed every 3months from the end of sbrt for the first 2years . 
percist criteria were used to evaluate the metabolic response [ 23 ]  . results between march 2014 and may 2016 , a total of 39 consecutive patients ( median age 72years , range 2691 ) were treated with ht - sbrt for malignant lung lesions : 22 patients were treated for early stage nsclc , 17 for metastatic disease ( table1 )  . in early stage nsclc , pathological confirmation was obtained for 17 patients ( 77% )  . 
in - field irradiation failures were observed in 2 ( 5.1% ) patients , one in the nsclc group and one in the oligometastatic group . acute adverse events were registered as follows ( table2 ) : g2 chest pain in one ( 2.6% ) patient with peripherally located tumor ; no rib fractures were recorded . 
no patient developedg3 radiation - induced pneumonitis , reporting only one g2 pneumonitis ( 2.6% ) , successfully treated with steroids , in a patient who concomitantly underwent erlotinib after progression through platinum - based chemotherapy . 
linacs equipped with flattening filter free delivery allow to reduce the treatment time and , probably , uncertainties related to organ motion during irradiation [ 24 , 25 ]  . 
cyberknife system offers a precise tracking during breathing and adjustment to moving targets [ 26 , 27 ] in order to compensate uncertainties related to the long treatment delivery time . 
ht could be largely criticized due to the relatively long treatment delivery in the absence of a lesion tracking systeactually , on the basis of clinical evidence , this technology is safe for treating moving tumors considering that interplay of breathing and tomotherapy delivery motions did not affect significantly plan delivery accuracy [ 28 ]  . to date , a bed10100gy remains a strong predictive factor of long - term lc [ 29 ]  . 
this could be explained with experimental and clinical data supporting the role of the total dose as a more crucial factor comparing to bed10 , based on the hypothesis that a moderate protracted schedule fractionation could improve re - oxygenation and , consequently , increase the tumor response [ 30 , 31 ]  . 
apart from the present experience , other studies reported valuable results both in terms of lc and safety profile by means of ht - sbrt in lung malignancies ( table4 ; [ 15 , 18 , 3238 ] )  . 
similar to our experience , 12 - months lc was superior to 90% . an italian study [ 15 ] , enrolling 56 patients with lung primary or secondary cancer , evaluated clinical outcomes of ht - sbrt in two different subgroups : ablative sbrt for 27 patients with t12 nsclc and palliative sbrt for 29 patients with oligometastases . 
in fact , several authors [ 3941 ] identified dosimetric parameters that might be useful as predictors of radiation pneumonitis , such as the mean lung dose , v20 and v5 . 
in the present study , ht allowed to respect available lung dose constraints in the majority of cases : mean lung dose < 9gy was respected in 97.4% of cases , v20 < 10% in 92.3% , v5 < 35% in 79.5%. 
in the present study population , only one patient in the metastatic group with slightly higher values of v20 and mld underwent steroid treatment for respiratory symptoms due to a g2 rp ; this patient was concomitantly treated with target agent anti - epidermal growth factor receptor ( erlotinib ) after first - line platinum - based chemotherapy and , after a short course period of steroids treatment , continued erlotinib . 
according to the data derived from few clinical trials , an increased toxicity is possible when targeted therapy is combined with sbrt [ 43 ]  . it is also well recognized that lung lesions located in the so - called no - fly - zone are at particular risk of complications [ 12 ]  . 
in this last clinical scenario , mediastinal oars sparing , in addition to a more fractionated regimen , is crucial to minimize the risk of adverse events , especially in the challenging situation of ultra - central located lesions . 
these findings reinforce patient selection as a crucial factor in the decision - making process for lung oligometastatic disease . 1 3 la radiologia medica ( 2018 ) 123 : 406414 1 3 412 la radiologia medica ( 2018 ) 123 : 406414 tumor while sparing nearby oars offering a safe treatment option , despite the relatively higher low dose to the normal lung remains an issue of debate [ 18 , 44 ]  . 
in our series , the three ultra - central patients reported no significant toxicity . in conclusion , the present study has several limitations such as : ( 1 ) the retrospective nature of the analysis ; ( 2 ) the heterogeneity of the population ( primary and metastatic lesions ) here analyzed ; ( 3 ) the limited follow - up . 
however , although the limitations abovementioned could affect the robustness of the present results , lc and os rates here reported seem comparable to available clinical data , both for primary lung tumors as well as lung oligometastases after sbrt . a longer follow - up and a wider sample size are advocated for more mature results both in terms of oncological outcomes and toxicity rates . 
this paper aims to report a single - center experience of direct puncture sclerotherapy of peripheral lfvms , focusing on technical aspects and clinical outcome in mid - term follow - up . materials and methods 16 patients have been treated for peripheral lfvms ( mean age 36.1years ) , complaining mild pain , swelling of the region of interest , and cosmetic nuisance . 
standard procedure consisted of direct puncture of the nidus using 2023 gauge needles under us guidance and injection of up to 15ml foam of sodium tetradecyl sulphate under fluoroscopic guidance . 
clinical and radiological follow - up were assessed at 1 , 3 , and 6 months . results lesions were localized : 8 in the upper and 5 the in lower limbs , 2 in the cheeks , and 1 in the vaginal labia . 
at 6 month follow - up , technical and clinical success were obtained in all cases , while radiological follow - up showed 81.2% ( 13 patients ) complete vessels thrombosis after multiple sclerotherapy sessions . 
no major complications have been recorded ; five patients ( 31.2% ) referred minor complications . conclusions sclerotherapy via direct puncture of lfvms is a clinically effective procedure , well tolerated by patients , with reduced costs and mild minor complications rate ; interventionalists should always clarify to the patients that multiple sessions would be performed and recurrences are expected at imaging follow - up despite clinical improvement . keywords vascular malformation low flow peripheral sclerotherapy direct puncture introduction vascular malformations ( vms ) are divided in high - flow and low - flow vascular malformations ( lfvms ) , with or without arterial components , respectively . according to the localization in or outside the central nervous system , they are distinguished in central or peripheral . lfvms are rare lesions with a global incidence of approximately 1 / 10 , 000 [ 1 ]  . 
cardarelli 9 , 80131naples , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 474480 lymphatic components according to the glowacki and mulliken classification [ 2 ]  . 
these lesions are congenital with a varied clinical presentation but usually are diagnosed in adult age as focal mass with intermittent swelling and pa symptoms can vary from asymptomatic , with or without cosmetic impairment , to pain , functional limitations ; they can be accentuated by physical activity , temperature variation , and specific positioning . the therapeutical management is challenging because of the high recurrence rate [ 3 ] ; therefore , different surgical and percutaneous approaches have been proposed , adopting multiple agents . 
 patient preparation consisted of preprocedural 6h fasting and hydratation . the standard procedure consisted of direct puncture of the nidus using 2023 gauge butterfly needles or 2021 gauge micropuncture needles under us guidance , depending on the size and on the position of the lesion ( fig.2 ) ; after blood aspiration confirming nidus puncture , contrast injection under fluoroscopic guidance was performed to opacify the vm nidus corresponding to the mr findings . 
the foam was prepared using two 10ml luer lock syringes via a three - way tap and mixed 1 : 1 with air , according to the technique described by tessari [ 6 ] ; the total amount was not pre - established , but the rule was to fulfill the lesion with foam until all the iodine contrast washed away . 
1 mr t1 - weighted sequences before ( a ) and after contrast injection ( b ) in coronal plane showing a vascular malformation in the left cheek ( black arrow )  . 
this 59 - year - old woman referred chewing defects and cosmetic discomfort ; the lesion maximum diameter was 3.4cm ( see also pt 15 in table1 ) 1 3 476 table 1 sample characteristics according to sex , age , lesion site and size , lymphatic component , and puig and dubois classification pt sex age ( years ) site size ( cm ) lymphatic component p & d classification la radiologia medica ( 2018 ) 123 : 474480 2 m 56 3 m 33 4 m 37 9 m 36 10 f 11 f 12 f 13 m 24 14 f 15 f 16 f left arm left leg left forearm left arm right arm right leg left vaginal labia right cheek left forearm right thigh left hand ( 2nd metacarp ) 1.2 right arm right leg left foot ( plantar ) left cheek right hand ( 3rd finger ) none none none microcystic none none none none none microcystic none microcystic microcystic none none none pt patient , p & d : puig and dubois classification type i type ii type iii type ii type iii type iii type i type ii type ii type ii type i type ii type ii type i type ii type i the postprocedural management consisted of clinical observation for 3 h during analgesic ( 1000mg paracetamol ) infusion ; a us was performed before patient dismission to exclude possible local complications . 
patients were recommended to assume antibiotics therapy for the following 3 days and analgesic in case of pain and fever [ 8 ] ; daily activities were restored the day after the procedure . clinical and radiological follow - up ( us and / or mr ) ( fig.4 ) were assessed at 1 and 6 months . technical success in this study was considered a complete fluoroscopic fulfilling of the lfvm nidus according to the previous acquired mr data ; clinical success was defined as a functional and cosmetic improvement of the initial conditions following the percutaneous treatment . results all vms included in this series were lfvms with dominant venous component of soft tissues ; in 4 cases , mr showed a concomitant lymphatic microcystic ( < 2cm ) component too . 
according to the puig and dubois classification system , they appeared 5 type i , 8 type ii , and 3 type iii ( table1 )  . 14 patients have been treated on a day - hospital basis without overnight stay , while 2 patients required one night hospital stay , because a diagnostic arteriography via femoral access was needed to clarify contrast - enhanced mr findings ; in those latter cases , no arterial inflow was detected . lesions were localized : 8 in the upper limbs ( 4 arms , 2 forearms , 2 hands ) , 5 the in lower limbs ( 1 thigh , 3 legs , 1 foot ) , 2 in the cheeks , and 1 in the vaginal labia . the procedures have been always technically accomplished ( 100% ) ; in 9 cases ( 56.2% ) , two different needles were required to be positioned into the nidus to fulfill the lesion . at 1 month follow - up , 13 patients referred clinical improvement ( 81.2% ) with reduction of pain and palpable mass , while in 3 cases ( 18.8% ) , the symptoms remained stable . 
in all cases , a us study showed enlarged and stiffened serpiginous vessels , partially thrombosis with reduced but persistent amount of venous flow signal into the lesion . fifteen patients were available to repeat the treatment , one patient was lost to follow - up ; at 3 months , all referred clinical improvement ( 100% )  . 
imaging follow - up showed disappearance of the flow signal with complete thrombosis in 8 patients ( 53.3% ) , while in 7 patients ( 46.7% ) , further reduction but with small amount of persistent flow signal was still appreciable . 
the 7 patients with residual flow were treated a third time with the same protocol ; after 3 more months , complete thrombosis was evident at mr follow - up in 4 cases ( 57.1% ) , while in 3 ( 42.8% ) reduced but persistent amount of venous flow signal was still evident . 
these latter patients preferred to suspend the treatment because referred clinical success in terms of symptomatic and cosmetic improvement despite the residual flow . overall , at 6 month follow - up , technical and clinical success were obtained in all cases and imaging ( us and / or mr ) showed 81.2% ( 13 patients ) complete vessels thrombosis after multiple sclerotherapy sessions . according to cirse classification system for complications [ 9 ] , no major complications requiring prolonged hospital stay ( grade iiv ) were observed ; however , five patients ( 31.2% ) referred minor complications ( grade i ) in terms of 1 3 la radiologia medica ( 2018 ) 123 : 474480 fig . 
usguided local anesthesia using a 25 gauge needle ( a ) ; preparation of the foam of sodium tetradecyl sulphate ( fibro - vein 3% , mac pharma srl , italy ) using two 10ml luer lock syringes via a three - way tap and mixed 1 : 1 with air , according to the technique described by tessari ( b ) ; after puncture of the nidus using a 23 gauge butterfly needle under us guidance , a 10ml luer lock syringe is connected and used to aspire blood confirming the correct positioning of the needle ( c ) ; slow flow manual foam injection through the butterfly needle under fluoroscopic guidance ( d ) 1 3 la radiologia medica ( 2018 ) 123 : 474480 478 fig . 
 foam injection under fluoroscopic guidance in oblique coronal plane , fulfilling the vascular malformation ( white arrow indicating the 23 gauge butterfly needle into the nidus ; black arrow indicating the foam distribution into the lesion ) ( b ) fever during the 2 days following the procedure ( 2 ) and / or skin erythema ( 3 ) , successfully managed with paracetamol and resolving within the first 2 weeks after treatment . discussion the treatment of vascular malformations is difficult and its goal should be to eliminate the nidus . sclerotherapy is the obliteration of a peripheral vascular malformation through the injection of an aggressive sclerosing agent causing instant precipitation of the endothelial cell proteins by denaturation and cellular dehydration and finally results in endothelial destruction and thrombosis [ 10 ]  . numerous sclerotherapy agents have been reported for treating low - flow vascular malformations , including sodium tetradecyl sulphate , ethanol , polidocanol , and bleomycin [ 11 ] ; however , no prospective randomised studies have compared these agents and there is no consensus as to which sclerosant agent is best [ 3 ]  . recently , foam of sodium tetradecyl sulphate has become the standard treatment with some evidence suggesting superior sclerotherapy [ 12 ] , where microbubbles of air are coated with sodium tetradecyl sulphate creating enormous increase in the surface area , displacing blood from the lesion and permitting better contact of the agent to the endothelium [ 13 ] ; indeed , it is the contact with the endothelium that is important to damage . in accordance with the literature data [ 3 ] , in this study , sclerotherapy with foam of sodium tetradecyl sulphate has fig . 
mr t1 - weighted sequence after contrast injection in coronal plane showing volumetric reduction of the vascular malformation in the left cheek ( black arrow ) at 6 month follow - up after three treatment sessions 1 3 la radiologia medica ( 2018 ) 123 : 474480 proven to be safe without major complications and mild rate of minor complication ( cirse classification system for complications : grade i )  . 
indeed , it should be noted that foam of sodium tetradecyl sulphate is deactivated by a relatively small volume of blood ; 0.5ml of blood will deactivate 1ml of 3% sodium tetradecyl sulphate significantly reducing the systemic effects [ 14 ]  . concerning the injection technique , it should be underlined that all liquid sclerosant agents are radiolucent and , therefore , not visible on fluoroscopy . 
there are a number of ways to identify the sclerosant agent and contrast can be added to facilitate visualization ; however , this will lead to some sclerosant dilution and may reduce effectiveness [ 15 ] ; in this study , the vascular malformations were first opacified by contrast and so during foam injection contrast outflow revealed sodium tetradecyl sulphate distribution . different classification systems have been proposed , which categorizes lfvms , by their mr morphology [ 16 , 17 ] and drainage characteristics [ 4 , 5 ] ; in this study , the puig and dubois classification has been adopted , because it correlates well with clinical outcomes [ 3 ]  . according to the literature data [ 3 ] , in this sample , sclerotherapy has proven to be an effective technique ; however , it is crucial to underline to the patients the concept that multiple treatment sessions are required and that is rare the lesion itself is definitely ablated , because longterm recurrences are frequent ; therefore , the aim of the intervention should be the clinical success based on patient satisfaction and symptoms improvement rather than imaging success intended as total disappearance of the lesion at us and / or mr follow - up . furthermore , it should be noted that sclerotherapy via direct puncture is a convenient procedure in terms of hospital expense , adopting low - cost materials ( butterfly / micropuncture needles and sodium tetradecyl sulphate ) , and being usually performed without overnight stay . this study presents some limitations . 
patients population was subdivided into three groups according to the organ failure : ( a ) chronic kidney failure ( n = 8 ) , ( b ) restrictive cardiomyopathy undergoing heart transplantation ( n = 1 ) , and ( c ) end - stage liver failure undergoing liver transplantation ( n = 6 )  . 
fifty - nine cmbs lesions ( 64.8% ) had supratentorial lobar distribution , 17 cmbs lesions ( 18.8% ) had supratentorial non - lobar distribution and the remaining 15 cmbs lesions ( 16.4% ) were infratentorial distributed . 
the improved detection of cmbs with swi sequences may contribute to a more accurate identification of patients with cerebral risk factors to prevent complications during or after the organ transplantation . keywords cerebral microbleeds susceptibility - weighted imaging magnetic resonance imaging end - stage organ failure transplantation introduction cerebral microbleeds ( cmbs ) consist of small cerebral hemosiderin deposits surrounded by macrophages that result from previous microhemorrhages , usually asymptomatic due to the rupture of small arteries , arterioles , and / or capillaries [ 1 , 2 ]  . 
 as a result , cmbs are more sensitively detected by swi compared to t2 * - weighted gre [ 3 , 8 , 1114 ]  . the presence of cerebral microbleeds was found in up to 5% of healthy adults , but they were most commonly correlated with aging , hypertension , cerebral amyloid angiopathy , ischemic stroke , intracerebral hemorrhage , and cognitive disorders [ 1 , 12 , 15 ]  . 
moreover , the presence of cmbs is an independent risk factor for subsequent larger intracerebral hemorrhages , and they are also associated with higher incidence of cognitive decline [ 18 , 19 ]  . regarding the localization , cerebral microbleeds can be classified in supratentorial lobar , supratentorial deep ( or non - lobar ) , infratentorial , and mixed distributed . the lobar distribution involves the cortex and the subcortical white matter . 
the infratentorial pattern includes the brainstem and cerebellufinally , mixed cmbs are a combination of both cortical and deep localization [ 20 ]  . the distribution of cmbs could be correlated to the systemic disease of the patient . a supratentorial lobar pattern was associated with the presence of cerebral amyloid angiopathy [ 21 ] and with degenerative brain disease , most commonly alzheimer disease [ 11 , 22 , 23 ]  . 
a distribution of cmbs in the deep white matter or in the infratentorial structure was significantly higher in patients with hypertension [ 16 ]  . patients with end - stage organ failure share several risk factors strongly associated with the presence of cerebral microbleeds , such as cardiovascular risk factors , low glomerular filtration rate , and platelet dysfunction . 
moreover , advanced hepatic failure , such as in childpugh class c , or fulminant hepatitis , are associated with hepatic coagulopathy due to decreased liver production of coagulation proteins [ 24 ]  . cerebral microbleeds have also an increased incidence in patients who underwent anticoagulation therapy due to chronic heart disease that finally brings to end - stage heart failure [ 25 ]  . as the presence of cmbs is considered a risk factor for future development of cmbs , and it may predict the development of ischaemic stroke and secondary intracranial hemorrhage [ 26 , 27 ] , it has become of fundamental relevance to assess the number and distribution of cmbs by mr imaging [ 36 ]  . the aim of this study was to review the distribution of cerebral microbleeds in patients with end - stage organ failure and their association with specific end - stage organ failure risk factors as a neuroimaging biomarker for the underling disease . materials andmethods patient population our retrospective cohort study was reviewed and approved by the institutional research review board ( irrb ) of our institution , and informed consent form was waived ; however , informed written consent to the mr was obtained in all patients . we examined 79 patients candidate for liver , kidney or heart transplantation between august 2015 and june 2017 as a part of a research protocol aimed to assess preexistence of cerebral risk factor in patients candidate for organ transplantation at our institution . 
drug therapy , which could increase bleeding risk , such as aspirin , clopidogrel , and warfarin , was reported for each patient . exclusion criteria were the presence of acute or chronic ischemic or hemorrhagic stroke , intracranial hemangioma , cerebral cavernous malformation , arteriovenous malformations , cerebral aneurysm , alzheimers disease , intracerebral lesions with a hemorrhagic component associated with tumors and abscesses . patients with unavailable swi images ( n = 8 ) , or poor image quality ( n = 6 ) were excluded from the study . ultimately , the study population consisted of 15 patients ( mean age 63.5years , age range 4882years , 9.15 ) , 9 males ( 60% ) and 6 females ( 40% )  . 1 3 la radiologia medica ( 2018 ) 123 : 441448 patients population was subdivided into three groups according to the organ failure : patients with end - stage kidney failure ( n = 8 ) , a patient undergoing heart transplantation due to restrictive cardiomyopathy ( n = 1 ) , and patients with end - stage liver failure undergoing liver transplantation ( n = 6 )  . 
data are summarized in table1 . mr examination the mr exams were performed on a 3t mr scanner ( discovery 750w , general electric , healthcare , milwaukee , usa )  . mr imaging protocol included axial and sagittal fast - spin echo ( fse ) t2w ( 8000 / 90 [ tr / te ] ) images , axial fluidattenuated inversion - recovery ( flair ) ( 9000 / 150 / 2250 [ tr / te / ti ] ) images , along with axial , sagittal and coronal non - enhanced and contrast - enhanced ( 0.1 mmol / kg gadobutrolgadovist , bayer , germany ) , fse t1w ( 600 / 20 [ tr / te ] ) images with a field of view ( fov ) of 24 cm , matrix 320320 , slice thickness 4mm , intersection gap 1mm , number of excitations 1 . the swi images ( 3d gre 48 / 23ms [ tr / te ] , flip angle 10 ) were obtained with a fov of 24cm , matrix 256256 , slice thickness 2.5mm , gap 1mm , number of excitations 1 , and acquisition time 4 : 04min . the swi images were also post - processed with the minimum intensity projection ( minlp ) algorithm in the axial plane with a slice thickness of 310mm to better visualize signal void of the vessels structures . image analysis the images were analyzed in consensus by two neuroradiologists , each with at least 10years of experience , who were unaware of the patients clinical information . 
any disagreement about image assessment was resolved in consensus by the two radiologists by discussion . swi images , presented in random order on a picture archiving and communication system ( pacs ) ( agfa healthcare gmbhbonn , germany ) , were analyzed by the two neuroradiologists for the presence and localization of the cmbs lesions . cerebral microbleeds were defined as small , hypointense , rounded lesions within the brain parenchyma that measured less than 10mm on the swi images [ 29 ]  . using the swi - filtered phase images , cortical calcifications , as well as choroid plexus , globus pallidum , and pineal calcifications , were easily identified as they appear with the oppositesign phase compared to hemosiderin [ 30 ]  . 
hypointense lesions in the basal ganglia , not clearly identified as calcifications , were excluded as most likely they represent iron deposits . hypointense spots near the neurocranium and the splanchnocranium were not considered because of their vicinity to the bone and their consequent uncertain artifact nature . to better differentiate between cmbs and blood vessels , the minimum intensity projection ( minip ) post - processed swi images were used as they are able to demonstrate the signal void of the vessels structures [ 5 ]  . number and distribution of cerebral microbleeds were recorded based on their location as supratentorial lobar ( strictly cortical and subcortical ) , supratentorial non - lobar ( in deep regions including the basal ganglia , thalamus , internal capsule , external capsule , corpus callosum , deep and periventricular white matter ) , and infratentorial ( brainstem , cerebellum ) as previously reported in the literature [ 29 ]  . statistical analysis continuous variables are presented as meanstandard deviation ( sd ) and compared using two - tailed , unpaired students t test . 
axial minimum intensity projection ( minip ) susceptibility - weighted imaging ( swi ) image shows two small , rounded , hypointense cerebral microbleeds in the left parietal lobe , and other smaller microbleeds in both frontal and parietal lobes of the right and left hemispheres fig . 
age and hypertension are also significantly correlated to the presence of cmbs as demonstrated in this study and as reported in the literature [ 19 ]  . cerebral microbleeds , according to guideline proposed in the literature [ 36 ] , are defined as round or ovoid lesions , that appear hypointense and with a blooming effect 1 3 la radiologia medica ( 2018 ) 123 : 441448 fig . 
axial minimum intensity projection ( minip ) susceptibility - weighted image shows a small , rounded , hypointense , brainstem microbleed imaging ( swi ) on t2 * - gre and swi sequences . 
in recent years , with the introduction of susceptibilityweighted imaging sequences , and with the wider availability of 3t mr units , there was an increased sensitivity of detection of small cerebral microbleeds [ 7 , 8 , 19 ]  . supratentorial lobar distribution of cerebral microbleeds was the most typical distribution founded in our series of end - stage organ failure patients ( 64.8% ) , and it was characterized by the presence of multiple cortical and subcortical white matter cmbs ( range 226 cmbs )  . 
this association was not related to the presence of other cmb risk factors such as other neurological diseases [ 32 ]  . the incidence of microbleeds in hemodialysis patients is significantly higher compared with the general population without a history of chronic kidney failure or stroke . 1 3 446 la radiologia medica ( 2018 ) 123 : 441448 in the chronic kidney failure population , diminished estimated glomerular filtration rate has been found to be a risk factor for cmbs [ 31 ]  . 
moreover , chronic kidney failure is correlated with the number of cmbs , thus , the number of cmbs can provide an indirect estimation of chronic kidney failure severity [ 3336 ]  . in our patient who underwent heart transplantation , a predominance of supratentorial lobar distribution of cmbs was found . 
 [ 38 ] found that the presence of cerebral microbleeds was more commonly found in patients with warfarin - related intracerebral hemorrhage when compared to anticoagulated patients without intracerebral hemorrhage . in end - stage liver failure patients studied in our series , the most common complication of the disease was the hepatic encephalopathy , which is an important prognostic factor of the disease [ 39 ]  . hepatic encephalopathy is characterized by high signal intensity in the globus pallidum on t1 - weighted mr images , likely a reflection of increased tissue concentrations of manganese , and white matter abnormality [ 40 ]  . however , hepatic failure is also associated with coagulopathy due to decreased liver production of coagulation proteins . 
the presence of cmbs on swi images was reported in patients with hepatic coagulopathy in the corpus callosum and in the paraventricular white matter , and they may arise from rupture of small penetrating arterial vessels [ 41 ]  . cerebral microbleeds were related to the degree of liver fibrosis , with a significantly increased number of cerebral microhemorrhages in case of advanced fibrosis [ 42 ]  . in our series , supratentorial lobar distribution of cmbs was the most commonly reported location in end - stage liver disease patients with a significant positive correlation with platelet dysfunction and hepatic coagulopathy due to decreased liver production of coagulation proteins in advanced hepatic failure . there is clinical evidence for the role of cerebral microbleeds in cognitive decline and for the correlation between cmbs and small vessel disease , cerebral stroke , and increase mortality . 
particularly , there is strong evidence that higher number of cmbs is associated with a more severe cognitive dysfunction , which comprises impaired executive function , and decreased attention and processing speed [ 7 , 11 , 34 ]  . 
the development of novel imaging technique and large prospective studies is expected to better understand the pathogenesis of cmbs and the clinical implication of this currently underdiagnosed clinical entity . limitations of this study are the relatively small group of patients , the lack of randomization of groups , the prevalence of end - stage kidney failure patients over other end - stage organ failure , particularly to the only one end - stage heart failure patient , and the retrospective nature of the study . another limitation was due to the fact that patient image analysis was limited by the lack of swi images ( n = 8 ) or poor image quality ( n = 6 ) due to the motion artifact . conclusions the use of swi sequences in a more widely available very high field strength mr units ( 3t ) has increased the detection of cmbs underlying an emerged new important imaging biomarker of cerebral involvement in a variety of diseases and syndromes . cerebral microbleeds are mostly founded in supratentorial lobar localization in end - stage organ failure patients and they are associated to several specific risk factors related to endstage organ failure . the radiologist involved in brain imaging in end - stage organ failure patients should be aware of the evidence that the presence of cmbs might identify patients at risk of future cerebral stroke , intracranial hemorrhage , and cognitive impairment , which in turn represents risk factor for complication during or after the transplantation . funding the authors state that this work has not received any funding . compliance with ethical standards conflict of interest the scientific guarantor of this publication is gianvincenzo sparacia , md . 
the remaining prior contrast - enhanced carotid cta studies were regarded as a potentially incidental ipe when a filling defect was found in one or more pulmonary arteries and subjected to the other two thoracic radiologists independently for reviewing and assessing for characteristics of the ipe and the image quality of the pe . 
characteristics of the patients with ipe were also studied in terms of gender , age , as well as clinical indication . results the prevalence of ipe among these suspected stroke patients was 0.8% on carotid ct angiography , and 24 ( 96% ) of all ipes had not been previously diagnosed by the original reporting radiologists . 
radiologists should check the higher pulmonary arterial vasculature carefully on the contrastenhanced carotid cta scans . keywords computed tomography angiography incidental pulmonary embolism carotid angiography suspected stroke introduction pulmonary embolism ( pe ) remains a major challenge to public health due to its high mortality [ 4 ] , which may exceed that of myocardial infarction and stroke in usa [ 11 ]  . 
 although pe is less prevalent in china , with an estimated annual incidence of 3.9 cases per 100 , 000 persons / year , the hospital mortality rate of pulmonary embolism - related * dong - hui shen dawnshen@sina.com 1 department ofradiology , fujian medical university union hospital , no . 
ipe is deemed to be a filling defect of one or more pulmonary arteries occurring on imaging ordered for indications other than suspected pe [ 18 ] and has been reported in many contrast - enhanced chest ct scans [ 26 ]  . fortunately , thanks to the rapid advancement of multidetector computed tomography ( mdct ) and its thin detector thickness and rapid acquisition , the peripheral pulmonary vessels are better visualized with exceptional spatial and temporal resolution . 
consequently , the contrast - enhanced ct examinations involving portions of the chest may detect the presence of ipe . carotid cta covers from the base of the heart through to the cerebral vertex and unavoidably includes the upper vol . : ( 0123456789 ) 1 3 400 la radiologia medica ( 2018 ) 123 : 399405 portions of the chest . 
it is a stratification tool for the evaluation of carotid atherosclerosis , which is a potential embolic source , especially in patients with symptoms of stroke [ 8 ]  . 
 presumably , ipe might be found on carotid cta images , however , due to the emergency of stroke or other preexisting conditions , the evidences of ipe on carotid cta scans were often overlooked . 
the current study attempted to determine the prevalence of ipe in suspected stroke patients undergoing carotid cta and to evaluate its characteristics in clinical scenarios . materials andmethods patient inclusion our institutional ethics committee approved this retrospective study , and the requirement for informed consent was waived . 
one attending thoracic radiologist with 8years of experience from department of radiology , fujian medical university union hospital , retrospectively and independently reassessed all carotid cta cases which were performed between january 2013 and december 2016 . 
the cases were identified by searching our picture archiving and communication systems ( pacs ) ( designed by ylz healthcare , fujian , china ) using the keyword carotid cta . 
participants were excluded from the study for any of the following conditions : ( 1 ) non - suspected stroke patients ; ( 2 ) known or suspected pe ; ( 3 ) poor or absent contrast enhancement of relevant pulmonary arteries ; ( 4 ) apparent substantial artifact ; or ( 5 ) irretrievable images . if a filling defect was found in one or more pulmonary arteries , the case was recorded as a potentially incidental pe and subjected to the evaluation from the other two thoracic radiologists with 9 and 25years of experience , respectively , and independently . 
otherwise , it was excluded from the ipe group . cta technique the carotid cta studies were performed on two 64 - slice ct scanners ( revolution and hd - 750 ) ( ge healthcare , milwaukee , wisconsin , usa ) in our imaging center . 
first , the anteroposterior and lateral position of the two positioning images were acquired to determine the scanning range : from the base of the heart through to the cerebral vertex . 
a caudocranial scanning direction was selected , and the imaging parameters were 0.625 - mm slice thickness , 0.5 - mm reconstruction interval , 120 kv , auto ma and a rotation time of 0.5s. evaluation ofimages andclinical findings in addition to the original axial images , coronal and sagittal multiplanar reformations ( mpr ) were also reformed to observe the characteristics of ipe , which included the presence , the site , the laterality , and the proximal extension . 
the latter was used to evaluate the quality of the contrast enhancement by means of a 3 - grade scale using the following criteria : 1 = poor [ < 150 ( hounsfield unit , hu ) ] , 2 = limited ( 150250 hu ) , and 3 = good ( > 250hu )  . 
as noted , the attenuation of most proximal pulmonary artery < 150 hu ( 1 ) was excluded . additionally , semi - quantitative likert scales were used for the assessment of the conspicuity of the pe ( 1 = very subtle , i.e. , the filling defect was evident only in retrospect and would not be expected to be identified during primary interpretation ; 2 = subtle , i.e. , the filling defect was difficult to visualize , but would likely be identified by careful inspection during primary interpretation ; 3 = evident , i.e. , the filling defect was clearly visible in retrospect )  . 
these included , but not limited to , pneumonia , lung nodules , and ground - glass opacities . clinical information suspected stroke patients who had been hospitalized were classified as inpatients and others who had only ambulatory visits and emergency room visits were categorized as outpatients . 
patient characteristics were noted for accessing demographic information and symptoms from the hospital database , pacs , request card and logbooks . statistical analysis the data were collected and analyzed using spss 16.0 software ( spss , inc . , chicago , il , usa )  . 
p value less than 0.05 was considered statistically significant . results a total of 4873 consecutively registered cases undergoing carotid cta between september 1 , 2013 , and august 31 , 2016 were identified from pacs . 
the remaining 3160 cases ( 64.8% ) were derived from 3144 patients ( 1786 men and 1358 women , at an average age of 60.910.2years from an age range of 3594years )  . 
filling defects were found in one or more pulmonary arteries in 25 patients , with a total incidence rate of 0.8% , in which pe was not mentioned in the carotid cta scan reports of 24 patients . 
among these patients , 13 ( 52% ) had a final diagnosis of ischemic stroke , 11 ( 44% ) had transient ischemic attack and 1 ( 4% ) had hemorrhagic stroke , and the most common comorbid condition was hypertension ( n = 20 )  . 
the demographic and clinical details of these patients were summarized in table1 . in terms of patient classification , ipes were found in 23 inpatients and 2 outpatients and the respective incidence rate was 1.0% ( 23 / 2249 ) and 0.2% ( 2 / 895 )  . 
thus , the incidence of ipe in the inpatient group was significantly higher than in the outpatients ( 2 = 5.18 , p = 0.024 , fishers exact test )  . 
of patients ( % ) age , mean ( sd ) male , n ( % ) past history , n ( % ) hypertension smoking hyperlipidemia malignancy coronary artery disease diabetes heart disease chronic obstructive lung disease stroke type , n ( % ) ischemic transient ischemic attack hemorrhagic n = 25 61.311.6 14 ( 64 ) 20 ( 80 ) 17 ( 68 ) 11 ( 44 ) 8 ( 32 ) 7 ( 28 ) 5 ( 20 ) 5 ( 20 ) 2 ( 8 ) 13 ( 52 ) 11 ( 44 ) 1 ( 4 ) in terms of age , patients aged < 50years accounted for less than one - twentieth ( 4% ) of all ipe cases , and those aged 6069 accounted for three - fifths ( 60% ) , and elderly people aged 70 or over one - third ( 36% )  . 
in this patient population , most ipe instances were reported in patients aged 6069 and the highest incidence rate of ipe was found in the group aged 70 and over . 
other most common incidental findings in these ipe positive patients were pneumonia ( n = 4 ) , followed by lung nodules ( n = 2 ) and ground - glass opacities ( n = 1 )  . discussion the current study conducted a retrospective investigation into a four - year clinical data pool of 3144 suspected stroke patients . 
almost table 2 age distribution of patients with ipe age ( years ) < 60 6069 7079 > 80 1706 n ( % ) positive 7 ( 0.4% ) 9 ( 1.1% ) 6 ( 1.3% ) 3 ( 2.8% ) ipe incidental pulmonary embolism , sd standard deviation ipe incidental pulmonary embolism 1 3 402 la radiologia medica ( 2018 ) 123 : 399405 fig . 
 b coronal image shows filling defect ( arrow ) in subsegmental branch of left upper lobe pulmonary artery all the ipes had a high conspicuity and satisfied the requirement of pe evaluation . the wide use of mdct is increasing the rate of detection of asymptomatic pe in patients undergoing contrastenhanced ct scanning even for reasons other than detection of pe [ 5 , 7 , 9 ]  . 
the clot has been labeled as silent pe [ 10 , 12 , 16 , 25 , 27 ] or unsuspected pe [ 1 , 23 , 24 ] or missed pe [ 15 , 17 , 29 ] , and in the interest of uniformity , we like to use the term incidental pe in this article following the recommendation of the international society on thrombosis and hemostasis ( isth ) in 2012 [ 14 ]  . ipe cases are described as those identified on contrastenhanced ct scans of partial or the whole chest other than those to rule out pe . 
the prevalence of ipe reached 32% in patients with deep venous thrombosis [ 25 ]  . according to the literature available , no existing studies have reported the prevalence of ipe in suspected stroke patients undergoing carotid cta . 
however , carotid cta only involves part of the upper part of lung and pe has a predilection for lower lung lobes [ 21 ] ; therefore , we speculate that the actual prevalence of ipe in patients afflicted with suspected stroke is probably underestimated and the potential hazard to patients has not been 1 3 la radiologia medica ( 2018 ) 123 : 399405 fig . 
b coronal image shows that filling defects are also seen in segmental branch of right upper lobe pulmonary artery ( wide arrow ) and lobe branch of the left lower lobe pulmonary artery ( narrow arrow ) table 3 characteristics of ipes no . 
of ipes n ( % ) single multiple site of thrombus right upper lobe right lower lobe left upper lobe bilateral upper lobe right upper and lower lobe bilateral upper lobe and left lower lobe bilateral upper and lower lobe most proximal location subsegmental segmental lobar attenuation of ipe attenuation of pulmonary artery pulmonary artery enhancement score pe conspicuity score 18 ( 72 ) 7 ( 28 ) 10 ( 40 ) 2 ( 8 ) 6 ( 24 ) 3 ( 12 ) 2 ( 8 ) 1 ( 4 ) 1 ( 4 ) 2 ( 8 ) 5 ( 20 ) 17 ( 68 ) 3 ( 12 ) 33.219.8 ( hu ) 326.641.5 ( hu ) ipe incidental pulmonary embolism ; hu hounsfield unit fully appreciated . 
moreover , the overall pe rate among these patients may be even higher , because patients with a history of pe or suspected pe were excluded from the current study . of note , in our study , nearly all ipes had not been reported in the initial radiological reports . 
one possible explanation is that the identification of pe on carotid cta scans seems more challenging than on pulmonary cta images , because pulmonary vessels are not a primary focus of image interpretation . 
meanwhile , only a small portion of the pulmonary vessels is involved in carotid cta and the conspicuity of pulmonary vessels derived in this manner is not as good as that from pulmonary cta . 
therefore , it is recommended that the radiologists should assess the upper chest in examinations by carotid cta , even though the primary purpose of the examination is not to exclude thoracic diseases . our study has shown that ipe was most commonly located in the segmental pulmonary artery , which is consistent with the findings of tresoldi etal . 
 however , one study , which employed a pe - computer - aided detection program ( pe - cadx ) to evaluate pe , reported that over half of pe was found in the subsegmental artery 1 3 404 la radiologia medica ( 2018 ) 123 : 399405 [ 15 ]  . 
the possible explanation for this inconsistency is due to the use of a latest - generation pe - cadx program and dedicated pulmonary cta , which can precisely pinpoint the location of pe . 
moreover , because only a limited part of the lung was included in the carotid cta cases enrolled in the current study and most ipes occurred in the right upper pulmonary lobe and were single pes in nature , the findings in our study are not likely to accord with those reported in other studies [ 7 , 15 ]  . our study showed that pe had a higher prevalence in inpatients than in outpatients . 
the result of our study is consistent with that of a previous study [ 3 ]  . age is known as independent risk factor for pe and the incidence of pe increases dramatically with advancing age [ 13 , 22 , 28 ]  . 
the mean age of patients with ipe in this study was 61.3years , which was lower than 68.5years reported in the literature [ 13 ]  . several artifacts , such as breathing motion artifact and beam - hardening artifact , may lead to an incorrect interpretation of pe , which has been systematically reported [ 19 ] , remains a challenge in our study . 
although ct protocol used in our study is not the pulmonary angiographic protocol , the short acquisition time and high concentration of the contrast media in carotid cta protocol also achieved adequate contrast enhancement of the pulmonary artery mostly . 
the average attenuation of the most proximal pulmonary was 326.6 hu with optimal enhancement , and only 19.4% of patients reported inadequate vessel enhancement . in our study , however , several limitations should be considered . 
first , as this study is a single - centre retrospective analysis and lacks standard pulmonary cta studies for comparison , we cannot evaluate the accuracy , the sensitivity and specificity of carotid cta in predicting ipe . 
second , it is possible that some ipe instances may actually be overlooked , as the ipe diagnostic criteria used in the current study were relatively strict : three thoracic radiologists retrospectively and independently assessed every case and ipe was confirmed only when all of them reached an agreement . 
 moreover , this study did not record the levels of d - dimer and evaluate the clinical diagnostic value of d - dimer for ipe in patients with suspected stroke . 
finally , we did not assess the benefits of treating ipe . in summary , the current study documents that ipe was present in up to 0.8% of suspected stroke patients undergoing carotid cta , and the incidence was higher in inpatients or elder patients . 
the cranial mri examinations including swi acquired on the same day of siebcg detection and serial cus to assess the progress of siebcg lesions in the following 6month period were retrospectively evaluated and compared for the presence of germinal matrix hemorrhage . results on swi , solely one patient ( 7 , 1% ) had signal alteration on caudothalamic groove compatible with grade 1 germinal matrix hemorrhage . 
seven patients ( 50% ) had signs of presumptive hypoxic insult including hyperintense dots on centrum semiovale and periventricular white matter in five , and increased signal intensity on the globus pallidi in two , on t1 - weighted images . 
of these , 10 patients became normal on follow - up cus at postterm - equivalent age , whereas four were missing . conclusion symmetrical increased echogenicity of bilateral caudothalamic grooves seen on newborn cus may be the indicator of other pathologies as ischemic insult or focal parenchymal hemorrhage . 
murat state hospital , edirne22030 , turkey 2 faculty ofmedicine , department ofradiology , erciyes university , kayseri , turkey 3 faculty ofmedicine , department ofradiology , trakya university , edirne , turkey 4 faculty ofmedicine , department ofpediatrics , erciyes university , kayseri , turkey 5 neonatology clinic , malatya state hospital , malatya , turkey vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 434440 introduction germinal matrix hemorrhage ( gmh ) is one of the most crucial complications encountered in preterm neonates that usually occurs during the first week of the life and tends to be unilateral [ 13 ]  . 
however , increased echogenicity of the caudothalamic groove detected following first week of the life has been suggested to be an isolated finding or associated with non - hemorrhagic factors , as infection , prematurity , intrauterine growth retardation , and asphyxia . 
 however , the data of non - hemorrhagic origin have not been studied on a wide study group . magnetic resonance imaging ( mri ) is considered as the gold - standard imaging method for evaluation of prematurity associated cranial pathologies . 
to our knowledge solely in one article , addressing this issue , four infants who were detected to have such lesions were examined by mri including t2 * weighted gradient - echo sequence and subependymal hemorrhage was excluded [ 8 ]  . though seldom , we came across symmetrical increased echogenicity of bilateral caudothalamic grooves ( siebcg ) on cus examinations performed in our neonatal intensive care unit ( nicu )  . 
we aimed to retrospectively investigate whether siebcg is of hemorrhagic origin or associated with other intracranial pathologies by evaluating swi with the contribution of other mri sequences . materials andmethods the current study was institutional review board approved and compliant with the declaration of helsinki . 
eventually , a total of 14 newborns [ 8 girls , 12 premature with gestational age between 26 to 35weeks and 3days ( mean 30weeks and 5days ) , 2 mature with gestational age of 37weeks and 6days , 39weeks ] with the overall mean birth weight of 1532g ( range 8002650g ) who were detected to have siebcg on cus and underwent mri on the same day of siebcg detection were included in the study . in our nicu as a part of routine practice , serial cuss were performed beginning from the first week of life until discharge . 
as the routine cus protocol , sequential images were obtained on both sagittal and coronal planes via the anterior fontanel by using both of aforementioned sector and linear transducers . routine cranial mri examinations were carried out on 1.5 tesla mri device ( siemens aera ; siemens medical systems , germany )  . 
images of swi ( b ) and phase map ( c ) revealed right cerebellar millimetric hemorrhagic focus ( arrows ) la radiologia medica ( 2018 ) 123 : 434440 results 12 newborns out of 14 were admitted to the nicu due to prematurity and associated clinical problems . 
these problems are listed as follows : respiratory distress ( n = 7 , respiratory distress syndrome ( rds ) in 6 , transient tachypnea of the newborn and pneumothorax in 1 newborn ) , retinopathy of prematurity ( rop , n = 6 ) , patent ductus arteriosus ( pda , n = 5 ) , sepsis ( n = 4 ) , pneumonia ( n = 2 ) , necrotizing enterocolitis ( nec , n = 2 ) , seizure ( n = 2 ) , patent foramen ovale ( pfo , n = 2 ) , coarctation of aorta ( n = 1 ) , ventricular septal defect ( vsd , n = 1 ) , supraventricular tachycardia ( n = 1 ) , disseminated intravascular coagulation ( dic , n = 1 ) , and duodenal web ( n = 1 )  . 
remaining two mature neonates were referred to the nicu with the diagnosis of meconium aspiration syndrome ( mas ) , small for gestational age ( sga ) , and hypoglycemic seizure in one and congenital pneumonia and pneumothorax in other neonate . 
five newborns had surgical operation due to duodenal web ( n = 1 ) , pda ( n = 1 ) , aorta coarctation ( n = 1 ) , and rop ( n = 3 )  . symmetrical increased echogenicity of bilateral caudothalamic grooves was detected by cus on 2nd to 65thdays of life , with a mean age of 28 , 6days , and 36th gestational weeks . 
seven patients ( 50% ) had signs of probable hypoxic insult including hyperintense dots on centrum semiovale ( fig.4 ) and periventricular white matter in five , and subtle increased signal intensity on the globus pallidi in two on t1 - weighted images . 
swi ( b ) and phase map ( c ) showed bilateral hemorrhage on caudothalamic grooves ( arrows ) 1 3 la radiologia medica ( 2018 ) 123 : 434440 fig . 
3 siebcg ( arrows ) with a millimetric cyst ( dashed arrow ) was shown on 31th day of life in patient eleven on right parasagittal image ( a )  . 
no evidence of hemorrhage was seen at the region of caudothalamic grooves on swi ( b ) , whereas focal millimetric areas of hemorrhage detected on left parietal white matter ( c , d , arrows ) on swi and phase map images fig . 
4 siebcg was seen on coronal cus ( arrows ) in premature newborn ( patient five ) ; microcyst was also noted on left caudothalamic groove ( a , dashed arrow )  . 
there were millimetric hyperintense foci on centrum semiovale on t1 - weighted image ( c , arrows ) had normal cus scans on follow - up at postterm - equivalent age , whereas four were missing . 
detailed clinical characteristics and imaging findings are given in table1 . discussion our results showed that siebcgs detected on cus in all patients , but one was not compatible with gmh on swi . 
in the literature , there have been several studies addressing siebcg with different nomenclature as hyperechoic caudate nuclei , late germinal matrix hemorrhage - like lesions , and non - hemorrhagic germinal matrix echogenicity [ 68 ]  . 
however , we detected siebcg lesions on the second day of life in two patients ( patient 10 and patient 14 ) with the gestational age of 32weeks and 2days ; 39weeks and 2days ; respectively . 
in the literature , the overall mean detection time of the lesions was reported as near - term - equivalent period rather than early preterm period in terms of corrected gestational age [ 68 ]  . 
 in our study , siebcg was detected with a mean age of 28 , 6days ( range 265days ) and 36th gestational weeks ( range 31weeks and 2days41weeks )  . 
 [ 10 ] reported the evolution steps of late neonatal onset subependymal echogenicities in the order of hyperechogenic stage , cyst formation , and disappearance on the follow - up cus examinations . 
on followup cus of ten patients at postterm - equivalent age , siebcg lesions disappeared consistent with the evolution steps in the literature . the etiology of the siebcg lesions still remains unclear . 
 [ 8 ] speculated that the etiology of subventricular echogenicities is more likely ischemic rather than hemorrhagic origin that led to germinolysis and gliosis . magnetic resonance imaging was reported to be more sensitive than cus to detect white matter injury in preterm newborns [ 11 , 12 ]  . 
we encountered accompanied hyperintense dots on centrum semiovale and periventricular white matter in five patients and subtle increased signal intensity on the globus pallidi in two patients on t1 - weighted mr images . 
however , there was no evidence of such problems in both patients with increased signal intensity on the globus pallidi ; nevertheless , rds and nec in one , and vsd in the other one were noted as the clinical evidence of probable ischemia . 
 medical history of our patients revealed clinical evidence of possible ischemia such as rds , sepsis , seizures , nec , dic , pda , vsd , sga , and mas , and mechanic ventilator support . 
therefore , in the presence of clinical signs of hypoxia , those signal alterations may be attributed to presumptive ischemic insult . to our knowledge , this study evaluates the largest group of newborns with siebcg who were investigated by mri 1 3 la radiologia medica ( 2018 ) 123 : 434440 and is the first study to investigate siebcg by using swi . 
 swi is an advanced mri technique , established based on a high - resolution , three - dimensional , gradient - echo sequence , utilizing both magnitude and phase images . 
in addition to the conventional mri sequences , swi has been shown to have the potential of providing further precious information about parenchymal microhemorrhages , gmh , intraventricular hemorrhage , and dilated prominent intramedullary veins [ 16 ]  . 
the study [ 17 ] comparing two groups of neonates with and without subependymal lesions , matched for gestational age , with chronic lung disease , concluded that these lesions have no major impact on neurodevelopmental outcome . 
prospectively designed studies with larger study groups and long - term follow - up should be performed to determine interval imaging findings and clinical outcome of siebcg in the future . conclusion we indicate that siebcg detected on newborn cus is generally not a manifestation of gmh by using swi . 
knowledge about characteristic imaging features of siebcg is important in daily cus practice , and if it exists , further examination with swi should be performed . acknowledgements none of the authors involved in this study received financial support . funding source no fund used for our writing . compliance with ethical standards conflicts of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments . 
published a clinical study on the effects of multiple injections of the macrocyclic gbcas gadoterate meglumine and gadobutrol on dentate nuclei t1 - weighted signal intensities ( si ) in patients with multiple sclerosis [ 1 ]  . 
therefore , it is likely that the values within these intervals did not follow a normal gaussian distribution and that the statistical tests used for comparisons were not appropriate . furthermore , the authors compared their results with those of radbruch etal . 
the data reported in this article confirm the previous studies , showing no evidence of gadolinium retention in brain after multiple injections of the macrocyclic gbcas . compliance with ethical standards conflict of interest j.s. 
the aim of this study is to evaluate parotid gland texture analysis ( ta ) combined with formal dosimetry as a factor for predicting severe late xerostomia in patients undergoing radiation therapy for head and neck cancers . methods we performed a retrospective analysis of patients treated at our radiation oncology unit between january 2010 and december 2015 , and selected the patients whose normal dose constraints for the parotid gland ( mean dose < 26gy for the bilateral gland ) could not be satisfied due to the presence of positive nodes close to the parotid glands . 
ta parameters included features of grey - level co - occurrence matrix ( glcm ) , neighbourhood grey - level dependence matrix ( ngldm ) , grey - level run length matrix ( glrlm ) , grey - level zone length matrix ( glzlm ) , sphericity , and indices from the grey - level histogra we performed a univariate and multivariate analysis between all the texture parameters , the volume of the gland , the normal dose parameters ( v30 and mean dose ) , and the development of severe chronic xerostomia . results seventy - eight patients were included and 25 ( 31% ) developed chronic xerostomia . 
paris - sud , universit paris saclay , cea - shfj , 91400orsay , france 5 department ofmedical , surgical andneuro sciences , diagnostic imaging , university ofsiena , azienda ospedaliera universitaria senese , siena , italy 6 unit ofradiation oncology , university hospital offlorence , florence , italy 7 department ofbiology , college ofscience andtechnology , 3 sbarro health research organization , temple university , temple university , philadelphia , pa , usa vol . : ( 0123456789 ) 1 3 416 introduction radiation therapy ( rt ) , with or without chemotherapy and / or surgery , represents the standard of care for the majority of head and neck cancer patients . for many years , rt has evolved with better target definitions and healthy tissue avoidance criteria , resulting in an improvement of loco - regional control and overall survival [ 13 ]  . in particular , the introduction of intensity - modulated radiation therapy ( imrt ) , which allows for the simultaneous delivery of different fractional doses to the various planned target volumes ( ptvs ) , has led to improved target irradiation , while limiting doses to normal tissues , thus reducing side effects and morbidity [ 47 ]  . the most common side effect of head and neck rt is xerostomia , which results from permanent damage to the salivary glands , particularly the parotids , thus leading to a major impairment of the patients quality of life [ 8 , 9 ]  . 
 dosimetric studies have shown that , in this setting , imrt may be useful for protecting the parotids against excessive radiation [ 47 , 10 , 11 ] , and have shown that a mean radiation dose of 26gy is the threshold for preserving stimulated salivary flow [ 6 , 10 ]  . 
a clear benefit was also obtained in terms of quality of life ( qol ) after the parotidsparing effect of imrt was demonstrated [ 4 , 12 ]  . however , this approach cannot be applied to a subset of patients in everyday clinical practice due to the presence of gross tumour or nodal disease close to the parotid glands [ 13 , 14 ]  . 
yet , despite this , only a certain percentage of head and neck patients , whose dose constraints could not be satisfied , develop radiation - induced xerostomia due to the sensitivity and specificity of normal tissue complication probability ( ntcp ) models at the clinic [ 15 ]  . these data suggest that , in addition to a formal dosimetric analysis , other parameters are required to obtain a more accurate prediction of xerostomia . image texture analysis ( ta ) is a heterogeneity quantifying approach that cannot be appreciated by the naked eye , and early evidence suggests that ta has a great potential in the field of oncology [ 1618 ]  . this analysis refers to numerous mathematical methods , which are used to evaluate the grey - level intensity and position of the pixels within an image to derive the so - called texture features , which in turn provide for a measure of heterogeneity [ 19 , 20 ] , and has already been applied to the parotid gland in terms of radiation - induced structural modifications and diagnostic power [ 2123 ]  . la radiologia medica ( 2018 ) 123 : 415423 materials andmethods patient series we performed a retrospective analysis of head and neck patients treated at our radiation oncology unit between january 2010 and december 2015 , and selected the patients whose normal dose constraints for the parotid gland ( mean dose < 26gy for bilateral gland ) could not be satisfied due to the presence of positive nodes close to the parotid glands . all of the patients clinical and pathological data were recorded before rt was begun . 
this study has been authorized by the institutional review board . radiotherapy andchemotherapy treatment rt was delivered with a 6 mv photons linear accelerator , using the intensity - modulated radiation therapy technique ( imrt )  . 
chemotherapy ( cisplatinum 40mg / m2 , weekly ) was accordingly prescribed following the national cancer network ( nccn ) guidelines . ct acquisition andsegmentation planning cts were acquired in our department , according to the scanning protocol , using a ge lightspeed ct scanner ( ge medical system , milwaukee , wi , usa )  . the parotid gland that showed a higher v30 was contoured by an expert radiation oncologist ( gr , pt ) , taking into consideration both the diagnostic ct and mri , and eventually using image fusion [ 13 , 24 ]  . the impact of the variations on the contouring was analysed by having two delineations performed on each patient by different radiation oncologists ( vn , pp ) , and the ta parameters were tested for reliability with the intra - class coefficient correlation method ( icc )  . the aim of this study is to evaluate parotid gland ta as feature extraction andtexture analysis a factor for predicting xerostomia . all the analysis for this work was carried out using lifex software  . 
the selected parotid gland ( i.e. , as above , the 1 3 la radiologia medica ( 2018 ) 123 : 415423 parotid that showed a higher v30 ) was used as the region of interest ( roi )  . 
the prediction results were further interpreted using the receiver operating characteristic ( roc ) curve . the entire statistical analysis was conducted using spss after the rt was completed , the patients began a scheduled followup programme , with repeated ct and mri scans , to assess the recurrence of the pathology , at 4weeks , 1216weeks , and every 3months thereafter for the first 2years , or , in the event that any clinical signs arose suggesting progressive disease ( pd )  . 
 roc curves were then generated for the known dosimetric parameters ( volume , mean dose , v30 ) , and for the integrated analysis of these known parameters with the ta parameters . to validate the models performance , the cohort was randomly separated into four partitions , with three partitions used as the training data sets , and the remaining one as the testing set ( k - fold validation )  . 
the training and testing were run four times , and the main characteristics of our patient cohort are summarized in table2 . seventy - eight patients were included , and 25 ( 31% ) developed severe chronic xerostomia . out of 78 patients , 54 ( 69% ) were male and 24 ( 31% ) were female . 
forty - one patients ( 53% ) underwent concomitant chemo - radiation with cisplatinum 40mg / m2 , weekly . during the observation period , 20 patients ( 25% ) showed evidence of disease recurrence , and 14 patients ( 18% ) died due to the progression of the disease . 
 the k - fold validation was successful , as the auc calculated on the four training sets were within the 95% confidence interval of the auc calculated on the original population , both for the prediction of acute and chronic xerostomia ( see table6 )  . number and percentage 54 ( 69% ) 24 ( 31% ) 14 ( 18% ) 64 ( 72% ) 12 ( 15% ) 28 ( 36% ) 38 ( 49% ) 4 ( 5% ) 48 ( 61% ) 16 ( 20% ) 10 ( 14% ) 20 ( 25% ) 22 ( 29% ) 34 ( 43% ) 2 ( 3% ) 53 ( 69% ) 25 ( 31% ) discussion radiation - induced xerostomia is the most common side effect suffered by head and neck cancer patients . 
the use of imrt has been shown to be useful for protecting the parotids against excessive radiation [ 47 , 10 , 11 ] , even in prospective trials [ 36 ]  . in this context , the texture analysis of the parotid gland has been recognized as a useful tool , even potentially correlated with the changes induced by radiation therapy [ 21 , 37 ] , and diagnostic discrimination of parotid lesions on mri [ 22 ]  . a study of radiation - induced parotid injury in head and neck patients has also been conducted , which analyses the ultrasound glcm texture parameters [ 23 ]  . these previous studies showed a decrease in mean , entropy , and fractal dimension between the start and the end of the radiation treatment , supposedly due to the loss of acinar cells and the increase in the adipose ratio , as also demonstrated by comparing ct images with histopathological slides [ 38 ]  . texture analysis allows for the identification of other textural features that characterize the structure of the parotid glands with respect to simple mean density , and provides for a greater exploitation of the ct images information content . 
if the motivation for the dosimetric parameter v30 is intuitive [ 3335 ] , rlnu refers to the length of the homogeneous run , and belongs to the grey - level run length matrix ( glrlm ) , which provides the size of the homogeneous runs for each grey - level with the same matrix as the sre parameter , which refers to the distribution of the short homogeneous runs in an image . 
surgery is the elective treatment , but , especially in high - risk patients , it is important to prevent the re - formation of ho and , in these cases , radiotherapy ( rt ) can play an important role . materials and methods we retrospectively analyzed a mono - institutional casistic of 30 patients ( 31 sites ) at high risk for ho development , treated with surgery and preor postoperative rt . 
radiological studies and clinical examination were performed in all patients during the follow - up period to evaluate both treatment efficacy and acute or late toxicity . results with a median follow up of 67months , 23 patients had a complete response ( cr ) with excellent results in term of joint mobility . 
no acute or late reactions have been reported . conclusion our data confirm safety and efficacy of rt in preventing ho , especially in high - risk patients , preferring a single fraction of 7gy . keywords heterotopic ossifications radiotherapy prophylaxis arthroplasty introduction heterotopic ossification ( ho ) is defined as the abnormal formation of lamellar bone in soft tissue , such as muscle , nerves and connective tissues . 
different causes of ho have been identified : trauma with subsequent fractures , dislocations and surgical procedures are the most frequent etiologies , but neurologic injuries related to spinal cord and brain injury as well as severe burns have also been recognized [ 1 , 2 ]  . even though the most frequently involved joints are hip , elbow , knee , shoulder and ankle , all major joints can * lavinia bianco lavinia.bianco@tin.it 1 department ofoncology , radiation oncology , school ofmedicine , azienda ospedaliera ordine mauriziano umberto i , university ofturin , turin , italy be affected ; temporo - mandibular joints ho has also been reported [ 3 ]  . ho pathogenesis is probably related to an inappropriate differentiation of pluripotential mesenchymal cells into osteoblastic stem cells , but certain causal factors remain unknown . 
furthermore , in the acute phase after trauma , there is evidence of infiltration by round cells with edema , muscle degeneration and inflammation , which are replaced with cartilage and bone after a few weeks [ 13 ]  . regarding clinical presentation of ho , it is typically silent and is frequently detected as incidental findings on imaging . 
when symptomatic , ho can cause motion limitation at involved joint , pain , and even complete bony vol . : ( 0123456789 ) 1 3 464 la radiologia medica ( 2018 ) 123 : 463468 ankylosis in severe cases ; other rare symptoms are localized warmth , mild edema , swelling and erythema [ 4 ]  . according to brooker classification ( which is reported below ) , hip ho are divided into four classes : grade 1 and 2 are usually asymptomatic , while grade 3 and 4 are frequently clinically symptomatic ( figs.1 and 2 , 35 , 6 )  . 
 grade 1 grade 2 grade 3 grade 4 islands of bone within the soft tissues about the bone spurs in the pelvis or the proximal end of the femur with at least 1cm between the opposing bone surfaces bone spurs from the pelvis or proximal end of the femur with < 1cm between opposing bone structures radiographic ankylosis [ 5 ] in patients with clinically significant ho , management often includes surgery excision , associated with prophylactic measures , such as external beam radiation therapy ( eb - rt ) or non - steroidal anti inflammatory drugs ( nsaids ) as indomethacin [ 6 ]  . in a meta - analysis published by vavken etal . 
in 2009 , 634 patients treated with rt were compared with 661 treated with nsaids ( indometacin , diclofeac or aspirin ) ; both risk ratios for ho and for complications were analyzed and there was no evidence of statistically significant or clinically important difference in the two arms [ 7 ]  . on the contrary , the two different therapies differ in terms of cost effectiveness . 
furthermore we tried to select a subset of patients where rt could be more appropriate than other therapies . materials andmethods from october 2005 to september 2012 , 30 patients ( 31 sites ) presenting ho received a prophylactic rt in our department of radiation oncology . 
indeed , nsaids have been frequently be reported as associated with many side effects , such as gastrointestinal ulceration , decreased platelet aggregation and renal toxicity which could lead to a low compliance and discontinuation of therapy [ 8 , 10 , 11 ]  . 
at last , nsaids can be even used in combination with rt : in 2015 cihan and arslan reviewed data of 12 patients treated with rt for ho and 7 of those received indomethacin together with rt . 
they concluded that rt in combination with nsaids was safe and an effective therapy for ho prophylaxis [ 12 ]  . regarding rt , in 1958 cooley and gross demonstrated that a dose of 30gy rt could prevent bone repair in a fracturated rat bone if performed in the first week of healing ; otherwise , the same treatment carried out of that time window was not efficient anymore [ 13 ]  . this concept was confirmed in humans since 1952 , when it was demonstrated that doses greater than 20gy could inhibit bony growth . 
therefore , previous experience of rt in ho prevention was performed with doses of about 20gy . anyway , since ho frequently affects young and nononcological patients , in the subsequent years the authors postulated the need of decreasing rt doses , to reduce the potential risk of secondary malignancies . 
6 the same patient after surgical intervention followed by radiotherapy 1 3 466 la radiologia medica ( 2018 ) 123 : 463468 mobilization after surgery , rt was generally performed before surgery . all patients were submitted to preliminary simulation using x - rays or ct images ; after treatment planning , the irradiation was delivered by varian dhx linear accelerator , with antero - posterior and postero - anterior fields conformed to site of ho , using 6 mv or 18 mv photon energies . 
the great majority of our patients ( 29 out of 32 sites ) were treated with a total dose of 7gy in a single fraction . all the patients received an x - ray examination the day after treatment . 
in case of persistence of pain or not complete response , patients were also followed during subsequent months or years with x - rays or ct and clinical visits . complete response was defined as no more evidence of ho in radiological studies during 6months after surgical intervention and rt , and as complete resolution of presenting symptomatology ( pain , motion reduction ) which was evaluated with orthopedic clinical visits ; partial response was identified as an improvement but not a complete resolution of symptoms or new development of broker grade iii ossification , which is usually considered as not clinically significant [ 13 , 19 ]  . 
with a median follow up of 67months ( range 19102months ) no acute or late reactions have been reported ( table2 )  . discussion the elective treatment of heterotopic ossifications remains surgery , but especially in high - risk patients , it is important to prevent the re - formation of ho . different possible risk factors for ho have been reported . 
sex , patients height 170cm , hypertrophic osteoarthritis of higher degree , size of femoral component of the prosthesis , previous ipsior contralateral ho and short course of non - steroidal anti - inflammatory drug ( diclofenac ) therapy significantly influenced the rate of ho in univariate analysis ; in particular , ho were 6.9% higher in men than in women . 
anyway , even though in the multivariate analysis prosthesis size , sex and height where found to have an interdependence , only prosthesis size had a statistically significant influence on ho ( p = 0.004 ) [ 20 ]  . from 1958 , when cooley and goss demonstrated the effect of radiation on bone repair process , several studies have demonstrated the efficacy of rt in ho prevention [ 21 ]  . the majority of our patients were successfully treated with a total dose of 7gy in a single fraction . in a recent metanalysis written by milakovic etal . 
this effect seemed to be an independent contribution , considering that , in the same meta - analysis , biologically effective dose ( bed ) did not affect ho progression . 
therefore , considering that single fraction rt could reduce the number of visits of the department and may be easier for the patient , despite that evidence the author suggested that a single fraction rt could be better in case of patients with advance disease or with a poor performance status [ 9 ]  . furthermore , in the same journal an editorial was published where the authors reported some mistakes in the above - mentioned article ( such as incorrect fractionation for two trials or some incorrect calculation of the bed ) ; anyway , they corrected the data and finally confirmed that treatment in a single 78gy fraction seems optimal [ 19 ]  . table 2 results patient n ( % ) sites n ( % ) previous rt response relapse acute toxicity late toxicity 23 ( 76% ) 24 ( 77.4% ) complete 2 ( 6.5% ) 7 ( 23.3% ) 7 ( 22.6% ) partial time of relapse ( months ) 1 3 la radiologia medica ( 2018 ) 123 : 463468 one of our patients experienced a retreatment of the same site ; in some patients , retreatment of the hip with a history of radiation for heterotopic ossification could be indicated , considering that , as written above , one of risk factors of ho reported in literature is represented by a history of ho in the ipsilateral or contralateral hip . lo and healy described four patients who were successfully re - irradiated after repeated hip surgery , without side effects [ 22 ]  . even the patient of our clinical case has not reported any toxicity . regarding pre - operative versus post - operative rt , seegenschmiedt etal . 
this finding was important because it was one of the first analyses in literature of rt performed in trauma setting instead of as an elective treatment [ 25 ]  . anyway , preoperative rt more advantages comparing to postoperative setting : there is not risk of luxation of prosthesis , any possible pain of the patient caused by transport is avoided and it provides lower costs as patients can be transported by car and do not need an ambulance [ 20 ]  . furthermore , it spares prosthetic material from irradiation and avoids interference with bony ingrowth into porous surfaces [ 13 ]  . nsaids , particularly indomethacin , have been widely used in alternative to rt with similar success rates . 
furthermore , as reported in the introduction , nsaids were more cost - effective than rt ( 8 )  . none of our patients developed acute or late toxicity . in literature there are not many findings about acute or subacute side effects associated with rt . 
few cases of pancytopenia after rt have been described , but blood cell count always normalized after only 1month [ 26 ]  . in a review written more than 10years ago the risk of trochanteric nonunion in case of trochanteric osteotomy was reported , which had a rate of about 1230% after rt versus 215% in other patients ; anyway just because of both highrisk rates , this technique has been performed very rarely in recent years , in favor of extended trochanteric osteotomy with allows easier bony union . another possible risk is due to the radiation dose to the testes because it can lead to reduction in sperm counts and furthermore in radiation - induced hereditary effects . 
testicular shielding has been reported to reduce dose to the testis by about 54% , leading to an average dose of 11.3cgy , thus this technique is strongly recommended [ 5 ]  . finally a potential risk in terms of secondary malignancies related to rt is well known ; however , we must consider that the total dose which is commonly prescribed to prevent ho is very low . in 2012 , farris etal . 
purpose of this study was to evaluate effectiveness and safety of endovascular treatment with flowdiverting stents ( fd ) in unruptured intracranial aneurysms . methods from may 2009 and may 2014 , we treated 49 patients with a total of 58 aneurysms , with fd technique . 
fifteen of the patients were asymptomatic , eight had headache , thirteen patients presented symptoms due to mass effect of the aneurysm on cns structures , twelve were treated due to a post - surgical relapse and one patient presented relapsing tias due to distal embolization from the aneurysm dome . 
we considered a dome / neck ratio > 2 as the only exclusion criteria . results successful stent deployment was achieved in 50 procedures out of 52 ( 94.34% ) while overall mortality was 2% ( 1 / 49 )  . 
at 3months , follow - up 75% ( 42 / 56 ) of the aneurysms were excluded from intracranial circulation , at 6months 80.35% ( 45 / 56 ) and at 12months 84% ( 47 / 56 )  . 
according to isuia study ( international study of unruptured intracranial aneurysms ) [ 5 ] , the risk of rupture of unruptured intracranial aneurysms varies according to aneurysm dimensions and localization in willis circulation , with higher chance of rupture in large / giant aneurysms of posterior circulation . intracranial aneurysms can be treated with either neurosurgical or endovascular approach . according to recent studies , neurosurgical treatment should be preferred in young patients , with aneurysms located in the anterior circulation and with low surgical risk [ 6 ] ; surgical treatment , although more invasive , is usually definitive [ 68 ] with lower chance of relapse in aneurysm neck region ( 1.58% ) , affected by a morbidity of 2022% and mortality of 810% . endovascular treatment can be achieved with different kinds of approaches and techniques such as 1 . 
parent artery occlusion [ 15 ] which could be achieved with different materials such as spirals , balloons or liquid embolic agents to treat mainly giant aneurysms with wide neck and impossibility to spare the vessel ; 6 . 
flow diversion stenting used to treat large , giant , fusiform or large - necked intracranial aneurysms , which , if treated with traditional endovascular technique , have a high rate of relapses and periprocedural complications . 
 the aim of this treatment is reconstruction of the parent artery wall , creating a biological seal to the aneurysm [ 16 , 17 ]  . after fd stent deployment , different degrees of contrast stasis are witnessed at angiographic controls ; usually aneurysms progress to a complete thrombosis within 12months with complete wall reconstruction , nevertheless the rate at which this process happens is hard to predict [ 17 ]  . as reported in the literature and case series of patients treated with fd stenting , an antiplatelet therapy is necessary before and after the deployment of the device , increasing risk of hemorrhagic complications . 
therefore , the use of these stents is greatly limited in patients that must be treated in emergency settings due to a subarachnoid hemorrhage ; safety of these stents in this kind of patient is still to be assessed [ 18 ]  . our study is a retrospective analysis of patients with unruptured intracranial aneurysm , treated with flow diversion technique in our interventional radiology department ; we reviewed our data collected over 5years of activity to assess the device effectiveness , safety and midterm followup results in treating unruptured intracranial aneurysms . materials andmethods we retrospectively evaluated 49 patients , who underwent endovascular treatment with fd stenting for unruptured intracranial aneurysms from may 2009 and may 2014 . 
a total of 59 aneurysms were treated . indication of fd stenting was given according to aneurysm morphology ( fusiform over saccular ) , the absence of a narrow neck ( dome / neck ratio < 2 ) and whenever traditional endovascular approach ( such as unassisted or assisted coiling ) appeared difficult due to complex vascular anatomy resulting in difficult sac catheterization ( table1 )  . 
exclusion criteria for the treatment were the presence of a narrow neck ( dome / neck ratio > 2 )  . the evaluation of anatomical characteristics of the aneurysms was performed with ct - angio , using a 64 slice ct lightspeed vct 64 ( ge , boston ma , usa ) and / or angio - mri using an achieva 1.5t ( philips , amsterdam , nl ) , using tof and / or ce - mra techniques ; since 2012 all preoperative evaluations were performed with mippr reconstruction to better analyze vessel anatomy . 
no antiplatelet resistance test was performed at our institution . all patients underwent ct - angio study at 37 days after the treatment to assess deployment and stability of the device . follow - up was performed at our institution provided digital subtraction angiography ( dsa ) at 3 , 6 , 12 and 24months after the procedure ( fig.1 ) , replaced by ctangio , whereas the patient could not perform or refused to undergo the invasive examination . 
aneurysm filling and contrast stasis at follow - up dsa were evaluated with the okelly - marotta ( okm ) grading scale [ 19 ] , which has been reported to have good intraand interobserver agreement [ 20 ]  . 
at each angiographic control , every treated aneurysm was graded with a letter according to the initial degree of filling ( a : total filling , b : subtotal filling , c : entry remnant , d : no filling ) and with a number which represents the degree of stasis observed through the angiographic phases ( 1 : stasis in arterial phase , 2 : stasis in capillary phase , 3 : stasis in venous phase )  . 
we considered a complete occlusion as a grade d aneurysm . clinical evaluation was performed at baseline before the procedure , at discharge and at each angiographic control with modified rankin scale ( mrs )  . we analyzed different parameters as primary outcome , according to the literature : aneurysm occlusion , stent patency , patency of the covered vessel and of collateral branches as secondary outcome we evaluated short - term mortality , long - term morbidity with mild or severe deficit at follow - up . results we performed a total of 52 procedures in 49 different patients ; two patients required a second treatment at 3months due to incomplete coverage of the neck , one patient was retreated due to disease progression at 6months . 
1 dsa imaging of a large saccular aneurysm of the ophthalmic tract of right internal carotid artery with wide neck : a imaging before the procedure , b angiographic image after stent deployment , ( c , d ) angiography at 3 months in lateral and a - p views : the aneurysm is completely excluded ( grade d of okm scale ) 12.7mm ( range , 640mm ) ( table1 )  . 
regarding aneurysm morphology , 46 of 58 ( 79.3% ) were saccular and 12 of 58 ( 20.7% ) were fusiform ( table1 )  . successful stent deployment was achieved in 50 of 52 procedures ( 96.15% ) ; no additional endovascular treatment ( such as deployment of coils inside aneurysm dome or balloon angioplasty inside the stent ) was performed . 
procedural complications occurred in only one case , in a patient that was being treated for middle cerebral artery aneurysms with pipeline - ped ( 1 / 49 ; 2% )  . 
we performed various attempts of retrieving the stent using alligator retrieval device ( ev3 , irvine , causa ) , although unsuccessful , with perforation of middle cerebral artery ; ct scan performed after the procedure showed the presence of sah associated with a large intraparenchymal hematoma and severe midline shift leading to the death of the patient 24h later . 
in the other case of failure 1 3 la radiologia medica ( 2018 ) 123 : 449455 of stent deployment , the length of the device was underestimated , therefore , it was not possible to achieve complete coverage of the aneurysm neck ; stent was then retrieved before deployment and was replaced with a longer device with a good final angiographic result . 
short - term morality was 2% ( 1 / 49 )  . we enrolled a total of 48 patients in our follow - up , for a total of 56 treated aneurysms , follow - up ranged from 12 to 40months with a mean follow - up time of 33months . 
 we registered a complete occlusion at 3months in 75% of the aneurysms ( 42 / 56 ) , at 6months in 80.35% ( 45 / 56 ) and at 12months in 84% ( 47 / 56 )  . 
out of the forty patients , which had an angiographic follow - up at 3years , we registered a complete occlusion in 90% of the aneurysms ( 38 / 42 ) ( table2 )  . 
the other four patients ( treated with two pipeline - peds , one silk and one fred ) had a delayed and partial opacification of the aneurysms dome confirming a partial thrombosis of the sac [ 19 , 20 ] ( table3 )  . 
patients who showed an unchanged perfusion of the aneurysm during follow - up were retreated ( grade 1a of okm scale ) ; two patients , both treated with pipeline - ped for giant aneurysm of ica , were retreated at 3months due to an incomplete coverage of the neck . 
no aneurysm rupture was registered in our patients during follow - up . in all the cases evaluated at follow - up , a complete stent patency was witnessed at 3 , 6 and 12months , without any signs of intra - stent thrombosis . 
two patients presented a mild intimal hyperplasia , without signs of hemodynamic stenosis or clinical symptoms , one was treated with pipeline - ped stent while the other with silk . 
both patients presented a complete occlusion of the aneurysm at 12months , suggesting that prolonged antiplatelet therapy does not affect significantly aneurysm occlusion rate . in only one patient , treated for an aneurysm of ica at cavernous tract with pipeline - ped , we registered a partial reduction of caliber of the ophthalmic artery at 6months follow - up , with occlusion of collateral orbital vessel , causing a mild symptomatology ( scotoma ) ; these findings were present also at 12months ( table2 )  . four patients , treated due to the presence of giant or large aneurysm causing mass effect symptoms , presented mild and temporary worsening of the symptoms , with complete remission of the symptoms at 12months . 
one patient , treated with pipeline - ped flex for a giant basilar aneurysm , had a severe worsening of the symptoms 4 months after the treatment , without registering any complications at angiographic and mri controls . 
long - term mortality due to aneurysm related causes and intracranial bleeding was 0% at follow - up . table 2 primary outcomes primary outcomes aneurysm occlusion ( okm scale grade d ) : at 3months at 6months at 12months at 3years parent vessel patency at 12months collateral vessels patency at 12months stent patency at 12months table 4 complications , morbidity and mortality complications , morbidity and mortality technical procedural complications parent vessel thrombosis ischemic complications hemorrhagic complications short - term mortality long - term morbidity collateral vessel occlusion with scotoma mass effect symptoms long - term mortality 75% ( 42 / 56 ) 80.35% ( 45 / 56 ) 84% ( 47 / 56 ) 90% ( 38 / 42 ) 100% ( 48 / 48 ) 98% ( 47 / 48 ) 100% ( 48 / 48 ) 1 / 49 ( 2% ) 0 / 49 ( 0% ) 0 / 49 ( 0% ) 1 / 49 ( 2% ) 1 / 49 ( 2% ) 2 / 48 ( 4% ) 1 / 48 ( 2% ) 1 / 48 ( 2% ) 0 / 48 ( 0% ) 1 3 454 discussion flow - diverting stents are an important evolution of endovascular approach for the treatment of intracranial aneurysms , shifting the aim of the procedure from occluding the aneurysms dome to repairing the parent vessel wall [ 17 , 2124 ]  . 
when comparing traditional endovascular techniques with fd stenting , we must take into account that the literature data regarding conventional endovascular embolization are results of over 30years of studies and publications , while fd stents are quite new devices ; therefore , the literature data available were collected on preliminary experiences [ 2528 ]  . even though our study presents some limitations , such as the restricted number of patients treated and the retrospective evaluation of the collected data , our results are in agreement with the ones reported in the current fd literature [ 2124 ] , which show how fd stenting for intracranial aneurysms is a safe and effective treatment ( especially in large necked and fusiform aneurysms ) granting a high percentage of occlusion of the dome , with low risk of complications [ 2527 ]  . a recent meta - analysis of 18 studies from briganti f etal [ 29 ] reported how fd stenting of intracranial aneurysms presents a good rate of aneurysms occlusion with low incidence of major complications ( ranging from 023.1% , with mean incidence of 8.3% ) such as occlusion or severe intra - stent stenosis , ischemic complications and hemorrhagic complications . 
mortality rate was also reported ranging from 0.5 to 8% ( mean rate 3.4% ) ; permanent morbidity related to the procedure was reported , with a mean rate of 3.5%. 
complication , morbidity and mortality rates reported in our study were comparable to the one reported in the meta - analysis . thrombosis of the aneurysm is a gradual and predictable result of correct fd deployment ; therefore , when treating large or giant aneurysms causing mass effect symptoms , this phenomenon could lead to a temporary worsening of the symptoms , due to an increased compression of surrounding cns structure . 
only after complete occlusion of the dome , we witnessed shrinking of the aneurysm , but this effect seemed still unpredictable and uncontrollable . bhogal etal [ 30 ] recently reported a large case series of patients treated with fd stenting , and analyzed the rate of partial or complete occlusion occurring in side branches covered by the device . 
 la radiologia medica ( 2018 ) 123 : 449455 in our case series , we only reported one case of branch caliber reduction ( 1 / 56 , 2% ) involving the ophthalmic artery and causing occlusion of collateral orbital vessel . the okm scale grading system [ 19 ] is a viable tool to assess the degree of aneurysm filling and contrast stasis , and it helps understanding the rate at which the aneurysm thrombosis occurs in different patients . 
this finding could hint that the process of aneurysm thrombosis , even if delayed , is always present after the deployment of fd stents ; moreover , the high rate of interand intra - observer agreement helps in evaluating aneurysm thrombosis evolution since controls are not always performed by the same operator [ 20 ]  . since our study reported a few number of cases treated with different kind of stents , we could not obtain homogeneous groups to assess whether aneurysm exclusion was faster and more definitive with one brand than with another . 
 [ 18 ] reported how current practice regarding antiplatelet therapy after intracranial stent deployment is heterogeneous , and in the literature , there is a lack of clinical trials that compare different medications for this kind of patients and procedure . 
most common treatment regimen for patient undergoing elective treatments was acetylsalicylic acid 325mg and clopidogrel 75mg daily ( for 7days before the procedure ) , while for maintenance regimen treatment the most common association was acetylsalicylic acid 325mg daily for life and clopidogrel 75mg daily for 3months . 
we did not report any event of occlusion of the stent , while we witnessed only two cases of patients presenting asymptomatic mild neointimal hyperplasia that spontaneously resolved at follow - up , after 6months of double antiplatelet therapy . conclusions in our study , fd stenting of unruptured intracranial aneurysm seems to be an effective and safe treatment , especially in selected patients with aneurysm presenting specific anatomical characteristic ( large neck , fusiform )  . 
this treatment leads to high rate of complete occlusion of the aneurysm in most patient at 1year after the procedure and is associated with low incidence of periand post - procedural complications . 
however , thrombosis and occlusion of the aneurysm could still be delayed in some patients ; still no predictors of aneurysm occlusion rate are known and the exact timing 1 3 la radiologia medica ( 2018 ) 123 : 449455 of this phenomenon could not be predicted . 
 however , association with the subsequent occurrence of major adverse cardiovascular events ( mace ) has not yet been evaluated . purpose this study aimed at evaluating the association of icac with subsequent mace and overall mortality . methods in this retrospective , irb approved study , we included 175 consecutive patients ( 89 males , mean age 78.38.5years ) of age > 60years who underwent an unenhanced ct of the head due to minor trauma or neurological disorders . 
 mace was defined as myocardial infarction or revascularization , stroke or death due to cardiovascular event . results mean follow - up time was 39.87.8months , resulting in 579.7 patient - years of follow - up . 
therefore , icac might be a prognostic factor to determine the risk for these events in older patients . keywords ct calcification cardiovascular event introduction arterial calcification is an integral part in the process of atherosclerosis and has been reported to be present in up to 90% of atherosclerotic plaques and lesions [ 13 ]  . 
15 , 81377munich , germany internal medicine iv , division ofrheumatology , ludwig - maximilians - university hospital munich , munich , germany 3 department ofdiagnostic andinterventional radiology , university hospital tuebingen , tuebingen , germany tomography ( ct ) in various regions of the body . 
the quantitative measurement of the burden of calcification in coronary arteries by ct has been shown to have a prognostic value in symptomatic and asymptomatic patients [ 58 ] and has been linked to the risk of the subsequent occurrence of major adverse cardiovascular events ( mace ) [ 9 ]  . intracranial arterial calcifications ( icac ) are often detected on unenhanced ct of the brain in elderly patients , especially in patients with vascular risk factors [ 1013 ]  . 
 in addition , two studies showed that the presence of icac vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 456462 in patients with acute stroke increases the risk for future vascular events [ 15 , 16 ] , the risk of subsequent downstream microemboli [ 17 ] and that icac is an indicator for incomplete arterial revascularization and poorer functional outcome after interventional stroke treatment [ 18 ]  . unlike in coronary arteries , the impact of presence and amount of icac on the subsequent occurrence of mace , which comprises the leading causes of death in the western world , has not yet been evaluated in an asymptomatic population . therefore , the purpose of this study was to evaluate the association of intracranial arterial calcifications , as detected with unenhanced ct of the head , and the subsequent occurrence of major adverse cardiovascular events and overall mortality . materials andmethods patients in this retrospective study in a first step all consecutive patients aged > 60years who were examined with an unenhanced ct of the head at our institution between 2005 and 2006 were extracted from our radiology information syste in a second step , we performed a full - text search in all these patients and filtered out the examinations with the following keywords in the clinical information section of the examination : fall , trauma , headache , dizziness , accident . 
in a third step , we reviewed the ct reports of the remaining patients and excluded all patients with an acute pathological finding such as bleeding , acute ischemia , fracture or malignant cerebral lesion as well as old ischemic lesions . 
a complete follow - up could be obtained for 175 patients ( men age 78.38.5years ; 89 males , 86 females ) , consistent with the cohort of this study . assessment ofoccurrence ofmace andmortality all patients were contacted with a letter , which included a structured questionnaire in which patients were explicitly asked about their clinical course in the years since they underwent unenhanced ct at our department . 
in cases with insufficient patient information , their general practitioners were contacted to provide information about the occurrence of mace or mortality of the patient . a board - certified radiologist reviewed the clinical course of all cases with the occurrence of mace ; if the mace was treated in our hospital , the clinical course of the event was reviewed in our hospital database . 
if the mace was treated in another hospital , medical reports were requested and reviewed as well . ct acquisition all unenhanced ct examinations were performed on 64or 128 - row scanners from different manufacturers ( somatom sensation 64 , somatom definition flash , both siemens ; aquilion , toshiba ; light speed vct , ge )  . 
in all patients , axial images were reconstructed in a bone window with slice thickness of 2mm and a soft tissue cerebral window with slice thickness of 3mm . calcified plaque score two radiologists with 4 and 13years of experience in crosssectional imaging performed a blinded consensus reading of the ct examinations . 
a grade was determined for each of the following arteries : both internal carotid arteries ( ica ) , both middle cerebral arteries ( mca ) , both vertebral arteries ( va ) , basilar artery ( ba )  . 1 3 458 la radiologia medica ( 2018 ) 123 : 456462 fig . 
a cps 1 : dot < 10 circumference , b cps 2 : 1090 circumference , c cps 3 : 90270 circumference , d cps 4 : 270360 circumference in each patient , the grades of each artery were then added statistical analysis to result in the calcified plaque score ( cps ) : cps = left ica + right ica + left mca + right mca + left va + right va + ba . comparisons ofthestudy to assess the influence of the cps on the occurrence of mace and all - cause mortality the patients were first divided in two groups : patients without calcified plaque ( cps = 0 ) , and patients with any calcified plaque ( cps1 )  . 
in addition , we performed a second division into two groups by grouping the patients according to the median cps into a low - cps and high - cps group . variables with normal distribution are presented with mean and standard deviation ; comparisons were performed with a 2 - sided t test . 
variables with non - normal distribution are presented with median and minimum / maximum ; comparisons were performed with a wilkoxon rank - sum - test . the influence of the cps on the occurrence of mace or all - cause mortality and the difference of the groups were tested with kaplanmeier - analysis ; significance was tested with log - rank - test . 
statistical analyses were performed with spss version 22 ( ibm , armonk , ny , usa )  . ethical standards our institutional review board gave approval for this study under the number 448 - 12 . 
all patients or their relatives gave informed consent prior to inclusion in this study . results patients a complete follow - up could be obtained for 175 patients ( men age 78.38.5years ; 89 males , 86 females ) , which is consistent with the cohort of this study . 
 kaplanmeier analysis showed that patients with a cps of 0 had a significantly lower risk for the occurrence of mace during follow - up ( p = 0.036 ) ; this is visualized in fig.2. 
highcps group the study population was divided by the median of the calcified plaque score ( cps = 5 ) into a group with a low - grade plaque burden ( cps < 5 ) and a group with a high - grade plaque burden ( cps5 )  . 
3 kaplanmeier - analysis of no plaque versus any plaque on the occurrence of all - cause mortality 1 3 460 la radiologia medica ( 2018 ) 123 : 456462 intracranial arterial calcification . 
therefore , intracranial artery calcifications , which can be easily detected on noncontrast - enhanced ct scans of the head , might be a prognostic factor to determine the risk for a future cardioor cerebrovascular events in older patients . the selection of the cohort was performed according to clearly defined inclusion and exclusion criteria . 
 [ 21 ] with cohorts consisting of 65 and 319 patients , respectively . the evaluation of icac was performed in unenhanced ct images of the head , which had been acquired in a clinical setting . 
 all examinations were standardized to a slice thickness of 2mm in the bone reconstructions and 3mm in the soft tissue reconstructions ; this ensured a reproducible , standardized analysis of the images . 
arterial calcifications are clearly detectable as hyperdense spots or lesions in unenhanced ct , which can be detected more sensitive by non - enhanced ct than by ct - angiography . 
this is probably due to the fact that subtle calcifications are masked by contrast media during ct - angiography [ 21 ]  . for grading of icac we used the scale proposed by babiarz etal . 
in a recent study this scale has been reported to be associated with the best inter - reader and intra - reader reproducibility when compared to other semi - quantitative scales [ 10 ]  . 
another possibility to quantify icac is with semi - automatic computer - assisted volumetry ; feasibility and a good reproducibility of different methods have been reported [ 10 , 22 ]  . 
however , in order to perform volumetric assessment of icac , acquisition of data with a very thin slice thickness ( < 1mm ) is necessary , which , due to the retrospective design of this study , was not available . 
it has been shown that these plaque components can be visualized very well using high - resolution mri without the need for radiation exposure [ 24 , 25 ]  . 
however , hr - mri is more time - consuming , more expensive and is , therefore , in most cases not yet performed in clinical workup of patients comprising our study cohort . 
5 kaplanmeier - analysis of cps < 5 versus cps 5 on the occurrence of all - cause mortality discussion in this retrospective study , we included 175 patients older than 60years who were examined with an unenhanced ct scan of the head due to minor trauma or neurological disorders . 
 furthermore , patients with a low burden of intracranial arterial calcification had a significant longer event - free and overall survival than patients with a high burden of 1 3 la radiologia medica ( 2018 ) 123 : 456462 has difficulties to depict and quantify calcifications . 
yet it has been shown that plaque calcification is a good indicator of the total underlying atherosclerotic burden [ 4 , 26 ] and that a calcified plaque represents an advanced plaque stage [ 27 ]  . 
we think that a prospective trial , which evaluates the association of ct and high - resolution plaque imaging mri of the intracranial and extracranial arteries on the occurrence of mace would be of scientific interest . in our asymptomatic cohort of older patients , presence of intracranial arterial calcification was high . 
similarly , presence of icac ranged from 72 to 83% in other studies , which examined patients with a history of stroke [ 15 , 21 , 28 ]  . the main findings of our study are that asymptomatic patients with a high burden of icac have a significantly increased risk for the subsequent occurrence of mace and all - cause mortality , independent of age and sex of the patients . 
the large population - based rotterdam cohort study comprised 2323 stroke - free patients and showed a significant relation of icac volume on the subsequent occurrence of stroke [ 12 ]  . 
another study examined the association of icac and the occurrence of mace and mortality in patients with stroke after hospital discharge [ 15 ] ; these patients were excluded in our study . 
together with the presented studies our findings underline that presence of icac might serve as a marker for the future risk of cardiovascular events , which can be easily detected and graded semi - quantitatively without the use of a contrast agent . 
given the fact that mace comprises the leading causes of death and disability in the western world , earlier recognition of high - risk patients is crucial to optimize therapy and risk - factor profile and thus reduce the risk for future events . 
asymptomatic patients with a high burden of icac could then be referred for therapy and risk factor optimization . there are also several potential limitations of our study that should be taken into account . 
 furthermore , we adjusted our main findings only to age and gender but not to other established cardiovascular risk factors such as arterial hypertension , hyperlipidemia , obesity or smoking . 
therefore , our study reflects a realistic clinical setting in which radiologists can recommend further work - up often only based on a limited amount of clinical information . in the future , larger prospective cohort studies should evaluate and confirm our findings with adjustment for all established cardiovascular risk factors . 
in addition , it might be of interest to perform evaluation of icac on different points during follow - up , to evaluate whether a more aggressive anti - atherosclerotic therapy and risk factor optimization will help to stabilize the amount of icac and lower the risk of cardiovascular events in patients with high icac burden . in conclusion , we could show that patients with a high burden of icac , as detected in unenhanced ct of the head , have a significantly increased risk for the subsequent occurrence of mace and mortality . 
therefore , presence and grade of icac might be a simple marker for the risk of mace and a statement on presence / absence of icac andif presenta semi quantitative grading such as mild / moderate / severe should be included in radiological reports of unenhanced cts of the head . 
thus , it might help the referring clinicians to identify patients at high risk for cardiovascular events , who might profit by a more aggressive medical therapy and risk factor optimization . funding this research received no specific grant from any funding agency in the public , commercial , or not - for - profit sectors . compliance with ethical standards conflict of interest all authors declare that there is no conflict of interest . ethical standards our institutional review board gave approval for this study under the number 448 - 12 . 
all patients or their relatives gave informed consent prior to inclusion in this study . la radiologia medica ( 2018 ) 123 : 554560 radiotherapy radiation therapy insmall cell lung cancer : anational italian survey patriziaciammella1 giorgiatimon1 alessiobruni2 davidefranceschini3 paoloborghetti4 nicolgiajlevra5 carlogreco6 vieriscotti7 marcotrovo8 on the behalf of associazione italiana radioterapia oncologica ( airo ) received : 11 december 2017 / accepted : 15 february 2018 / published online : 13 march 2018 italian society of medical radiology 2018 abstract introduction radiation therapy plays an important role in the management of sclc both in curative and palliative setting , however , conflicting data from clinical trials incite debate over the appropriate use of radiation therapy regarding prophylactic cranial irradiation ( pci ) and / or thoracic consolidative in extensive - stage sclc ( es - sclc )  . 
this survey is conducted to evaluate the current pattern of care among italian radiation oncologists . methods in june 2016 , all italian radiation oncologists were invited to a web - based survey . 
questions pertaining the role of rt in the clinical management of both limited - stage ( ls ) and es - sclc were included . results we received 48 responses from italian radiation oncologists . 
preferred management of ls - sclc favored primary concurrent chemoradiotherapy ( 89% ) , even if the 36.9% usually delivered rt during or after the cycle 3 of chemotherapy , due to organizational issues . 
pci was recommended in es - sclc patients with thoracic complete remission ( 63% of respondents ) , with thoracic partial response ( 45% ) and with thoracic stable disease ( 17% ) after first - line chemotherapy . 
lastly , the thoracic consolidative rt was recommended by 51% of respondents in patients with es - sclc in good response after first - line chemotherapy and a great variability was shown in clinical target volume definition , doses and fractionation schedules . conclusions our analysis showed a high adherence to current guidelines among the respondents in regard to chemoradiation approach in ls - sclc patients and to pci indications and doses . 
future clinical trials are needed to standardize these treatment approaches to improve treatment outcomes among patients with es - sclc . keywords radiation therapy small cell lung cancer national italian survey * patrizia ciammella patrizia.ciammella@asmn.re.it 1 radiation therapy unit , department ofoncology andadvanced technology , azienda ospedaliera arcispedale s maria nuova , istituto di ricovero e cura acarattere scientifico , viale risorgimento 80 , 42123reggioemilia , italy 2 uoc radioterapia oncologica , aou policlinico di modena , modena , italy 3 radiotherapy andradiosurgery department , humanitas cancer center andresearch hospital , milan , italy 4 radiation oncology department , spedali civili brescia , p.le spedali civili , 1 , brescia , italy 5 radiation oncology , sacro cuore don calabria cancer care center , negrar , verona , italy 6 radiotherapy unit , campus bio - medico university , rome , italy 7 department ofradiation oncology , azienda ospedaliero - universitaria careggi , university offlorence , florence , italy 8 radiation oncology department , cro aviano , aviano , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 554560 introduction small cell lung cancer ( sclc ) accounts for about 1015% of all lung cancer cases . 
it is usually related to smoking habits and it tends to show a rapid systemic spread , meaning it is often diagnosed in advanced stages [ 1 ]  . radiation therapy ( rt ) plays an important role in the management of sclc , both in curative and palliative setting . 
concurrent chemoradiotherapy ( ccrt ) in limited - stage sclc ( ls - sclc ) is widely adopted due to the strong evidence supporting the use of thoracic rt concurrently with platinumbased chemotherapy to improve overall survival ( os ) [ 14 ]  . 
 although the role of thoracic rt is well - established in the management of ls - sclc , the optimal radiation dose and fractionation schedule is still under investigation [ 5 , 6 ] , as well as target delineation and optimal timing of concurrent chemotherapy . on the other hand , chemotherapy is the cornerstone treatment for extensive stage ( es - sclc ) and four to six cycles of platinum - based systemic therapy represent the current standard of care [ 2 , 3 ]  . 
 consolidative thoracic radiotherapy ( ctrt ) seems to be beneficial in patients with es - sclc who achieved a response after primary chemotherapy , as shown by a recently published phase iii randomized trial conducted on 498 adults with advanced sclc from 42 hospitals [ 8 ]  . in addition , prophylactic cranial irradiation ( pci ) following response to induction chemotherapy provided a survival benefit in a phase iii trial [ 9 ] and it is currently recommended for responders with either lsor es - sclc [ 2 , 3 ]  . 
however , the risk for late radiation effects and other clinical factors might impact on its routinary use [ 6 , 10 , 11 ]  . for all these reasons , the management of lsand es - sclc can be highly variable between different oncology centers and it is likely to be guided by clinician experience and local patterns of practice . the aim of this survey was to evaluate the current management of sclc in italy and to highlight areas of potential improvement , if needed . 
in particular , we designed this survey to assess italian radiation oncologists attitude regarding both pci and ctrt in ls - sclc and es - sclc , and what factors influence physicians clinical recommendations . methods the study was approved by associazione italiana di radioterapia oncologica ( airo )  . 
a first call was originally sent on june 6 2016 , and a reminder 1month later , to maximize response rate . the survey contained 34 questions regarding the management of sclc , and particularly the role of ctrt and pci in es - sclc . 
physicians were first asked details about demographics and clinical experience : years since residency completion , number of patients affected with sclc treated in the past years , practice setting and basic knowledge . 
factors influencing the use of pci , the timing and choice of rt regimens , the role of multidisciplinary case discussion and rt planning techniques and delivery were also evaluated . 
forty - eight responses were received , representing 6% of all italian radiation oncologists registered as member of airo . the level of experience of the respondents varied : three radiation oncologists ( 6% ) have been working in a radiation oncology department for less than 5years , 15 ( 32% ) for 510years and 29 ( 61.7% ) for more than 10years . 
the median number of newly diagnosed sclc patients seen annually was more than 20 for only 4 ( 8.33% ) radiation oncologists , less than 10 for 19 ( 39.58% ) and between 10 and 20 for over half of respondents . 
55% are subspecialists in lung cancer . the rate of multidisciplinary case - discussion was 82.98%. management oflimitedstage sclc radiation oncologists were asked to select the chemoradiation approach in fit patients with ls - sclc . 
we asked to define the cause of radiation delay : more than half of the respondents declared to have organizational issues . 1 3 556 la radiologia medica ( 2018 ) 123 : 554560 table 1 survey questions posed to respondents . 
the distribution of recommended schedule by survey respondents was showed in fig.1. discussion the results of this radiation oncology italian survey show the variability of practice occurring in the treatment of both ls and esslcl . 
 [ 15 ] have conducted a systematic review and literature - based meta - analysis to establish the most effective way of combining chest rt with chemotherapy for patients with ls - sclc . 
 thirty - four percent recommends pci also in patients with stable disease after first - line chemotherapy ; regarding essclc , 63.83% suggests pci in patients with complete thoracic remission after chemotherapy , 44.68% also in patients with partial thoracic response and 17.02% in patients with stable thoracic disease too . 
pci schedule is 25gy in 10 daily fractions for the majority of respondents . role ofthoracic consolidative rt inessclc almost all clinicians ( 97.87% ) recommend 6 cycles ( 46.7% ) or 45 cycles ( 48.89% ) of cisplatin and etoposide as first - line chemotherapy in patients with es - sclc . among respondents , 51% estimated a frequency of radiotherapy consultation for ctrt in more than 70% of patients with es - sclc responding to systemic therapy , as shown in table2 . moreover , we asked to estimate the number of patients with es - sclc undergoing ctrt . 
the majority of radiation oncologists ( 71.7% ) treats on average less than 10 patients per year ; only 6.52% , as showed in table3 , treats more than 20 patients per year . fifty - one percent would offer ctrt in all es - sclc patients with good response ( complete or partial ) after firstline chemotherapy . 
respondents were allowed to choose more than one option for this question . regarding the definition of clinical target volume ( ctv ) , 8.89% of respondents asserted that they would include the entire pre - chemotherapy thoracic disease extent in the ctv , 55.56% would treat only the post - chemotherapy residual disease and 35.56% would define the ctv somewhere in between the pre - chemotherapy and the residual disease , with two separated volumes and different dose levels . 
the intergroup 0096 trial showed that 45gy / 1.5gy per fraction , delivered twice - daily over 3weeks with concurrent cisplatinetoposide , was superior to 45gy / 1.8gy per fraction , once a day over 5weeks [ 20 ]  . 
oneyear survival was 83% for the twice - daily rt arm and 76% for the daily arthese inconclusive results suggest that both the schedules can be used in this setting . 
a more recent retrospective study of a large number of patients with ls - sclc suggests that elderly patients with large tumors may not benefit from pci in terms of os , even after a complete response to definitive chemoradiation therapy [ 25 ]  . most italian radiation oncologists ( 97 , 96% ) would offer pci not only in patients in complete remission , but even in patients with partial or stable response after chemotherapy and dose and fractionation schedule was almost unanimously 25gy in 10 daily fractions . the use of pci has been evaluated in patients with essclc who responded to initial chemotherapy . 
the earliest meta - analysis [ 22 ] included 14% of patients with stage iv disease and showed a benefit that was similar to that of limited - stage disease , but only in patients with complete response to systemic treatment . as clearly reported by kim , to date , there have been two clinical trials with opposite results regarding pci for patients with es - sclc [ 26 ]  . 
a phase iii study from european organization for research and treatment of cancer ( eortc ) randomized 286 patients to either pci or no radiation after any response to chemotherapy [ 9 ]  . 
this trial showed a statistically significant improvement in median os in the pci group , but it was recently debated , because routine pre - pci brain imaging was not performed , and concerns about long - term neurocognitive dysfunction arose [ 27 ]  . 
a japanese trial , presented to the 2016 asco annual meeting , randomized patients with es - sclc and a negative magnetic resonance of the brain to pci or no radiation after any response to chemotherapy [ 28 ]  . 
also , a recent analysis of practice pattern among us radiation oncologists revealed that 98% offers pci to patients with es - sclc after a response to systemic chemotherapy , according to current national comprehensive cancer network guidelines [ 30 , nccn ]  . the use of thoracic consolidation rt for patients with es - sclc who achieved clinical response to chemotherapy is supported by current nccn guidelines , but patient selection and rt doses and volumes are not well - defined in literature . 
patients with es - sclc who achieved any response to 46 cycles of platinumetoposide chemotherapy were randomized to receive either thoracic rt ( 30gy in 10 fractions ) and pci or pci alone . 
a more recent seer ( surveillance , epidemiology , and end results program ) database analysis showed an improvement in 2 - year os from 2.5 to 6% and median os from 4 to 7months with thoracic rt in patients with es - sclc [ 36 ]  . additional analysis on the crest data demonstrated that only patients with residual intrathoracic disease following chemotherapy had a benefit from thoracic rt [ 37 ]  . 
in our survey , 51% of respondents would offer thoracic rt in all es - sclc patients with good response ( complete or partial ) after first - line chemotherapy , despite the crest trial results . the major limit of the present study is the low response rate ( 6% ) , although this is similar to other oncology surveys ( 10% ) [ 38 , 39 ]  . 
as a matter of fact , when we asked if in the rt center , clinicians were divided into anatomical district - based groups , > 55% answered they were dedicated ( also ) to lung cancer , 36% that they were not dedicated to any disease , and only 9% of respondents was not involved in lung tumor treatment . 
moreover , young specialists or in training clinicians might be hesitant to answer questionnaires about such a specific topic : only 6% of respondents have less than 5years of experience in rt . 
secondary objectives were to calculate the effective dose , to establish the number of positive ct and to analyze which of the risk factors are correlated with positivity at ct ; finally , to calculate sensitivity and specificity of nice and cchr in our population . materials and methods we retrospectively evaluated 493 ct scans of patients aged 1845years , collecting the following parameters from ed medical records : patient demographics , risk factors indicating the need of brain imaging , trauma mechanism , specialty and seniority of the referring physician . 
for each ct , the effective dose and the negativity / positivity were assessed . results 357 / 493 ( 72% ) and 347 / 493 ( 70% ) examinations were not in line with the cchr and nice guidelines , respectively . 
in our series , cchr showed sensitivity of 100% , specificity of 74% ; nice showed sensitivity of 100% , specificity of 72% . conclusion we observed an important overuse of head ct scans in mhi ; the main promoting factor for inappropriate was injury mechanis2% of head ct were positive , correlating with signs of suspected skull fracture and motor vehicle accident with high energy impact . keywords minor head injury computed tomography head ct emergency department clinical decision rules ct overuse introduction * michaela cellina michaela.cellina@asst - fbf - sacco.it 1 asst fatebenefratelli sacco , piazza principessa clotilde 3 , 20121milan , italy irccs san raffaele hospital , via olgettina 60 , 20132milan , italy head trauma is a frequent cause for emergency department ( ed ) access ( 1.72million / year in us ) [ 1 ] and is considered a public health concern , with a major economic burden on health care services [ 2 ]  . 
more than 75% of head trauma arriving at ed are classified as minor head injury ( mhi ) [ 3 ] , which is defined as a history of loss of consciousness , vol . : ( 0123456789 ) 1 3 508 la radiologia medica ( 2018 ) 123 : 507514 amnesia , or disorientation , with glasgow coma scale ( gcs ) from 13 to 15 [ 3 ]  . 
head ct is considered the gold standard for the evaluation of head trauma , due to its high sensitivity for detecting brain hemorrhage and skull fractures [ 4 ] , but the dramatic increase in its use has raised some concerns about its applicability , cost burden , ionizing radiation exposure , especially in the emergency setting [ 5 , 6 ]  . since < 1% of mhi needs surgical interventions [ 3 , 7 , 8 ] , the execution of head ct in all mhi patients would not be fully justifiable economically and would expose patients to an unjustified radiation dose . 
the most used clinical decision rules are : national institute for health and clinical excellence ( nice ) [ 9 ] , canadian computed tomography head rules ( cchr ) [ 3 ] , american college of emergency physician ( acep ) [ 10 ] , neurotraumatology committee of the world federation of neurosurgical societies ( ncwfns ) [ 11 ] , national emergency x radiography utilization study ( nexus - ii ) [ 12 ] , new orleans criteria ( noc ) [ 7 ] , and scandinavian clinical decision rules [ 13 ]  . 
their main goal is to reduce costs and exposure to ionizing radiation [ 14 ]  . nice and cchr proved to have high value of specificity in detecting intracranial lesions needing neurosurgical intervention [ 3 , 4 , 15 ]  . despite these guidelines , the overuse of head ct in mhi still remains a diffuse problem both for patients - related and non - clinical human factors [ 16 ]  . therefore , our aim was to assess the amount of ct scans for mhi performed in relatively young patients in our ed that are not recommended by nice and cchr guidelines , and to analyze factors contributing to unnecessary examinations . secondary objectives were : to calculate the effective dose of head ct scans , to establish the rate of positive ct scans in our population and to analyze which of the risk factors , included in the clinical decision rules selected in our study , are correlated with ct positivity in our series . materials andmethods patient population institutional review board approval was granted for this study with a waiver of the requirement to obtain written informed consent from each patient . we choose to study a relatively young population of patients , as more sensitive to radiation exposure . we retrospectively evaluated head ct scans of consecutive patients aged 1845years from january 1 to june 30th 2016 , presented for mhi to the emergency department of an urban hospital of milan ( northern italy ) with a number of access to the ed of 100 , 000 / year . our exclusion criteria were : patients aged < 18years or > 45years , trauma occurred > 24h before the access in ed , gcs < 13 , missing clinical data , refusal to undergo head ct scan , head ct scan performed at the request of the patient , unreliable history provided by the patient , and head trauma resulting from syncope or seizure . 
we performed group comparison using pearson 2 test for categorical variables and mannwhitney u test for continuous variables to identify any risk factor with statistically significant correlation with positive head ct . 
 [ 18 ] , in a study on 400 patients with mhi , reported that 36.8% patients had no indication for the execution of the ct scan , according to a list of ct indications created by a panel of experts from a revision of the literature . 
 [ 19 ] considering cchr as reference , observed 10.9% of ct scans non - appropriate in the population study in general , and 37.3% of non - indicated examinations , when analyzing patients younger than 65years . 
 [ 19 ] showed a significant higher tendency of the neurologists to request non - indicated ct . no type of seniority was statistically significant as a risk factor , as also reported by klang etal . 
in our study , only specialized physicians work in our emergency room , and the level of experience of our first aid physicians can be considered more homogeneous . significant correlation between patient age and unwarranted ct was not observed in our group , unlike other series [ 19 ] and this can be explained by the fact that we considered a restricted age range of young patients . when analyzing the mechanism of head trauma , motor vehicle accidents with high - energy impact was found to be a significant risk factor for non - indicated ct for both nice and cchr ; these findings are in line with klang etal . 
other proposed non - clinical factors related to the inappropriate / different use of head ct in ed were race / ethnicity [ 21 ] and patient economic factors [ 22 ]  . 
the differences between our data and those reported in the literature can be largely explained by the different models of health organization in the various countries : given that in italy the access to the exams is not bound to the presence of a patients insurance , the use of the ct scan in the emergency department is more widespread than in other countries and not limited by patient social or economic factors . in our case series , we found only 10 positive ct ( about 2% ) and this is less than what reported by lee [ 23 ] , who observed an important increase of the use of head ct in head trauma from 2001 to 2007 with a constant rate of detected intracranial hemorrhages ( that is 3% ) and by sadegh etal . 
in our group of abnormal ct scans , we did not observe a significant prevalence of brain contusions , as previously reported [ 3 , 7 , 8 , 24 , 25 ] , while subarachnoid hemorrhage was the most frequent finding . 
 analyzing the correlation between trauma mechanisms , risk factors and ct positivity , at univariate analysis we observed a significant correlation between abnormal ct scan , and well - evident head wound , signs of suspected skull fracture , hemotympanum , raccoon eyes , motor vehicle accident with high energy impact , and sport injuries . 
at multivariate analysis , we found a correlation with only two variables : signs of suspected skull fracture and motor vehicle accident with high - energy impact . the evidence that suspected skull fracture is correlated with ct abnormal findings has already been reported [ 18 ] , as well as the presence of hemotympanum and raccoon eyes , that are both signs of basal skull fracture [ 3 , 7 , 8 , 18 , 26 ]  . as in other studies , headache and amnesia did not have a significant association with positive ct scan [ 3 , 7 , 8 , 24 ]  . 
 previous studies demonstrated a correlation between abnormal 1 3 la radiologia medica ( 2018 ) 123 : 507514 ct and various risk factors , such as focal neurological deficit [ 8 , 2527 ] , loss of consciousness [ 28 ] , and gsc [ 8 , 29 ]  . in our study , the majority of risk factors did not show a significant correlation with abnormal head ct , and this can be explained by the fact that in our series only a reduced number of patients had a positive ct scan . in our case series , only 1 / 493 patient needed a neurosurgical intervention , and this rate is below the data reported in the literature ; sadegh etal . , in a study on mhi including patients who had at least one risk factor according to clinical decision rules reported a rate of mhi patients needing neurosurgery of 1% [ 8 ] , stiell etal . 
individual cancer risk is a multifactorial entity that is difficult to estimate ; however , age , sex and delivered examination dose are important contributing factors [ 3234 ]  . 
2msv is a relatively low dose of radiation exposure , anyway , the risk from repeated low - dose exposure need to be considered [ 24 , 31 , 32 ]  . 
in our case series , we observed two patients with abnormal ct whose ct scan was not required according to both cchr and nice , and one patient with intracranial post traumatic lesions with ct scan indicated by nice but not by cchr ; therefore , on the one hand we can consider that a close adhesion to the guidelines would have resulted in missing post - traumatic findings , on the other hand , none of the patients with a ct scan not in line with the clinical guidelines required a neurosurgical intervention . this is a retrospective study ; we carefully analyzed patient medical records for any sign and symptoms , but we have to consider the possibility that patients who underwent ct scan had signs / symptoms that could justify the execution of brain imaging but were not reported in the medical records and this fact can lead to an overestimation of the rate of non - indicated ct , even if we can suppose that severe signs or symptoms have been registered . moreover , this study was conducted in a single institution with a particular organization and may not be generalizable to another ed . conclusions in conclusion , we observed an overuse of ct scan in mhi in young patients according to both cchr and nice guidelines . 
the main contributing factor for over - referral was injury mechanism . in our case series , 2% of positive ct scans were observed , and a correlation between ct positivity and signs of suspected skull fracture and motor vehicle accident with high - energy impact . the overuse of head ct scan in mhi is the cause of unnecessary radiation exposure and health care cost . 
an analysis of the causes for overuse should be carried out in every ed to target specific interventions , education of the staff , compliance with the guidelines , and revision of the management protocols . funding no funding has been received for this study . compliance with ethical standards conflict of interest authors declare no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
data were compared between nodules that became hccs at follow - up ( hcc ) and those that did not ( no - hcc )  . results on follow - up , 5 / 69 nodules became hccs and 64 / 69 showed indeterminate characteristics . 
multivariate regression analysis showed that increase in size ( or 10.48 ; sensitivity , 100% ; specificity , 81.2% ; p < 0.001 ) and hepatobiliary phase hypointensity ( or 1.02 ; sensitivity , 100% ; specificity , 78.1% ; p < 0.001 ) was associated with hcc development . conclusion indeterminate hepatocellular nodules at gd - eob - dpta - enhanced mri in cirrhotic patients rarely became hccs . 
hepatobiliary phase hypointensity had a weak association with hcc development . keywords hcc indeterminate hepatocellular nodule cirrhosis gd - eob - dtpa liver mri introduction current diagnosis and management of hepatocellular carcinoma ( hcc ) are largely guided by imaging results . 
the american association for the study of liver disease ( assld ) 2010 guidelines recommend that a non - invasive diagnosis of hcc in patients with chronic * francesco agnello fra.agnello@libero.it 1 department ofradiology , university ofpalermo , via xii gennaio 1 / g , 90141palermo , italy 2 department ofsciences forhealth promotion andmother andchild care g . 
dalessandro , university ofpalermo , palermo , italy liver disease can be done at contrast - enhanced computed tomography ( ct ) or magnetic resonance imaging ( mri ) if a nodule larger than 1cm in diameter shows enhancement on hepatic arterial phase with subsequent wash - out on portal venous and / or delayed phase [ 1 ]  . 
these differences are related to vascular tumor changes during hepatocarcinogenesis , which result in an initial decrease in normal portal and arterial supply , subsequently followed by an increase in abnormal arterial supply via newly formed , abnormal , arteries [ 5 ]  . 
hepatocellular nodules without typical imaging features of hcc are considered indeterminate by assld 2010 guidelines , and a second study ( the other of ct or mri ) or nodule biopsy is recommended [ 1 ]  . 
with the advent of gd - eob - dtpa , the ability of mri to detect hcc nodules has increased , but in parallel , a growing number of hepatocellular nodules with indeterminate characteristics vol . : ( 0123456789 ) 1 3 490 la radiologia medica ( 2018 ) 123 : 489497 are being detected in the cirrhotic liver [ 68 ]  . 
have found 60 benign lesions , 41 premalignant lesions ( high - grade dysplastic nodules / early hcc ) , and 10 hccs , and concluded that hepatobiliary phase hypointensity is the stronger marker of malignancy [ 9 ]  . 
the latter observation is in accordance with a paper by kumada etal . , which have reported that approximately one quarter of gd - eob - dtpa hepatobiliary phase hypointense hepatocellular nodules became hypervascular hccs at follow - up [ 10 ]  . 
have found that hyperintensity on diffusion - weighted ( dw ) images in hypovascular hepatobiliary phase hypointense nodules increased the risk of progression to hypervascular hccs [ 11 ]  . 
to the best of our knowledge , there is only one study , which had specifically investigated the significance of hyperintense nodules on t1 - weighted images [ 12 ]  . thus , the purpose of this study was to retrospectively analyze the evolution of indeterminate hepatocellular nodules of any type on serial gd - eob - dpta - enhanced mri in cirrhotic patients , and to identify nodule characteristics that allow prediction of hcc development . materials andmethods study population this retrospective study was performed in a large , referral hospital for hepatobiliary diseases ( policlinico paolo giaccone , university of palermo )  . 
institution review board of our hospital approved this study , and waived the need for patient informed consent because of the retrospective nature of the study . the study coordinator ( f.a. , a radiology fellow with 8 years of experience ) searched our radiology database to identify all cirrhotic patients who underwent gdeob - dpta - enhanced mri of the liver between january 2009 and april 2015 . 
of the 10 who had less than 24 - month follow - up , no nodule become hypervascular hcc at at multi - detector row ct or mri follow - up or was proved to be hcc at pathology . 
the etiology of cirrhosis was hepatitis c infection in 27 patients ( 82% ) , hepatitis b infection in three patients ( 10% ) , and both in three patients ( 10% )  . 
the diagnosis of cirrhosis was made on the basis of histological findings in eight patients and combined clinical features and laboratory results in 25 patients . mr imaging protocol mr imaging was performed on one of the two 1.5t mr scanners available at our institution ( signa excite , general electric , healthcare ; intera achieva , philips healthcare ) equipped with a body - phased array coil . 
the imaging protocol for both scanners included axial t2 - weighted turbo or fast spin - echo ( with and without fat saturation ) sequences , axial dual gradient - recalled echo ( gre ) t1 - weighted sequence , axial diffusion - weighted ( dw ) sequence using three b values ( 0 , 150 , and 800s / mm2 ) , and axial contrastenhanced three - dimensional t1 - weighted gre sequence with fat suppression . 
 contrast - enhanced images are obtained immediately before and after contrast injection , on late hepatic arterial phase at 2035s , portal - venous phase at 80s , 3 - min late , and 20 - min hepatobiliary phases . 
an automated bolus 1 3 la radiologia medica ( 2018 ) 123 : 489497 detection algorithm ( mr smart prep ; ge medical systems , milwaukee , wi , usa ) or a fluoroscopic triggering ( bolus - trak ; philips medical systems , best , the netherlands ) was used to obtain an optimal hepatic arterial phase [ 13 ]  . 
nodule signal intensity was evaluated on unenhanced t1and t2 - weighted sequences , as well as on high - b - value dw and contrast - enhanced sequences , and was classified as hypointense , isointense , or hyperintense to the surrounding liver . 
on the basis of signal intensity at baseline mri , each nodule was classified into one of the following six groups ( hereafter called baseline groups ) : 1 , hypointense on hepatobiliary phase ; 2 , hyperintense on hepatobiliary phase ; 3 , hypointense on 3 - min late and hepatobiliary phase ; 4 , hyperintense on t1 - weighted and hypointense on hepatobiliary phase ; 5 , hypointense on portal - venous , 3 - min late and hepatobiliary phase ; and 6 , hyperintense on t1 - weighted phase . the coexistence of other ( at least three ) nodules with the same imaging appearance of the selected nodule at baseline mri was recorded . diagnosis of hcc was done according to the assld 2010 guidelines criteria that require a minimum size of 10mm , and a typical enhancement pattern ( i.e. , arterial enhancement followed by venous wash - out ) [ 1 ]  . medical charts were reviewed to determine whether any hcc exceeded the aasld 2010 criteria for curative treatment , which include a single hcc more than 5cm in diameter or 3 hccs less than 3cm [ 1 ]  . statistical analysis statistical analysis was performed at per nodule level . 
the dependency among nodules observed within the same patient was explicitly considered in the analysis . data were compared between nodules that became hccs at follow - up ( hereafter called hcc nodules ) and those that did not ( hereafter called no - hcc nodules ) using the fishers exact test for categorical variables and the generalized estimating equations model ( gee ) , with binomial family and logit link , for continuous variables . 
age , cirrhosis etiology , and history of hcc before the baseline mr examination were also considered as a variable . data were reported as count and percentage for qualitative variables and as mean and standard deviation for continuous variables . 
the adjusted odds ratios ( ors ) with respective 95% confidence intervals ( cis ) , sensitivity , specificity , positive predictive value ( ppv ) , and negative predictive value ( npv ) were reported . 
the hcc nodules had a greater mean baseline diameter than non - hcc nodules , and these differences were statistically significant . the mean tumor diameter doubling time of hcc nodules was 595.25days. 
among 12 no - hcc nodules with increased size at follow - up , 10 of 12 ( 83% ) were high - grade dysplastic nodules and 2 of 12 ( 17% ) were low - grade dysplastic nodules . diagnosis of no - hcc was confirmed by means of surgical resection ( two high - grade dysplastic nodules ) and fineneedle biopsy ( eight high - grade dysplastic nodules and two low - grade dysplastic nodules )  . hcc nodules had a significantly greater mean change in size than no - hcc nodules . 
b , c on 15 - month mr follow - up , the nodule shows enhancement on hepatic arterial phase ( b ) and wash - out on portalvenous phase ( b ) 1 3 la radiologia medica ( 2018 ) 123 : 489497 nodules that showed hypointensity on 3 - min late phase . 
we found that increase in size [ or 10.48 ( 95 cis 2.9936.74 ) ; sensitivity , 100% ; specificity , 81.2% ; ppv , 31.3% , npv , 100% ; p < 0.001 ] , and hypointensity on hepatobiliary phase [ or 1.02 ( 95 cis 0.215.05 ) ; sensitivity , 100% ; specificity , 78.1% ; ppv , 16.7% ; npv , 100% ; p = < 0.001 ] , were associated with hcc development . 
other variables failed to achieve a statistical significance . discussion in this study , we have analyzed the evolution of indeterminate hepatocellular nodules in cirrhotic patients in serial gdeob - dpta - enhanced mri . 
we found that only few nodules became hypervascular hccs at follow - up , and the majority of nodules showed indeterminate findings or disappeared at follow - up . the frequency of hcc transformation of indeterminate hepatocellular nodules was in line with the previous results [ 1719 ]  . 
have reported that 15 of 634 ( 2.4% ) non - hypervascular , hypoattenuating , and hepatocellular nodules transformed into hypervascular hccs on serial imaging follow - up [ 17 ]  . 
the observation that indeterminate hepatocellular nodules rarely become hypervascular hccs is also supported by a study by seki etal . , which have reported that most dysplastic nodules disappeared ( 15 of 33 , 45% ) or remained unchanged ( 14 of 33 , 42% ) at follow - up [ 18 ]  . 
in a study using a rat model [ 19 ]  . the hcc nodules had a slow grow on a serial imaging follow - up , suggesting that a 612 - month follow - up is the best option for the management of indeterminate hepatocellular nodules detected at gd - eob - dtpa - enhanced mri . 
of note , in our series , all nohccs with increased size at follow - up were highor lowgrade dysplastic nodules at pathology analysis . since the goal of screening cirrhotic patients is to detect hcc at an early stage , the second purpose of our study was to identify nodule characteristics that can predict hcc development [ 1 , 22 , 23 ]  . 
b on 18 - month hepatobiliary phase mr image , the nodule is not appreciable signal intensity characteristics hypointensity on hepatobiliary phase was significantly more common in hcc than in no - hcc nodules . 
hepatobiliary phase hypointensity was attributed to decreased organic anion - transporting polypeptide ( oatp8 ) expression , which occurs during the multistep hepatocarcinogenesis in parallel with elevation of nodule malignancy grade , before the reduction of normal arterioportal inflow and elevation of abnormal arterial inflow [ 24 ]  . 
this allowed us to speculate that hepatobiliary phase hypointense nodules , which subsequently became hccs , might be high - grade dysplastic nodules or early hccs [ 25 , 26 ]  . 
however , in our series , hepatobiliary phase hypointensity had a specificity of 78% and a very week or ( 1.2 ) , because most hepatocellular nodules showing hepatobiliary phase hypointensity remained indeterminate , or disappeared at follow - up . 
this is supported by the fact that hepatobiliary phase hypointensity was considered by the liver imaging reporting and data system ( lirads ) as an ancillary feature that favors the diagnosis of hcc and not a major feature of hcc [ 28 ]  . 
the fact that the hepatobiliary phase hypointensity can be found in any non - hepatocyte containing lesion ( e.g. , cysts and hemangiomas ) further limits its application as an independent predictor for hcc development [ 2830 ]  . 
no - hcc nodules showing hepatobiliary phase hypointensity are likely regenerative or dysplastic nodules . another interesting result of our study was that , although hcc nodules had a greater mean baseline diameter than nohcc nodules , the baseline size was not a predictive factor for hcc development . on the other hand , nodule increase in size significantly correlated with hcc transformation , and represented an independent predictor of hcc development . 
thus , it is crucial to pay particular attention and carefully observe those hepatocellular nodules , which show hepatobiliary phase hypointensity and increase in size . this study had some limitations that should be pointed out . 
however , this reflects our clinical practice , in which imaging follow - up is performed with different modalities and suspicious nodules are treated as soon as possible to prevent the development of untreatable hccs . 
however , the probability that a no - hcc nodule with stable or decreased size at follow - up was an hcc was extremely low because of a long follow - up [ 31 , 32 ]  . 
data in parentheses are ranges si signal intensity , other nodules other nodules with the same imaging appearance of the selected nodule at initial mri , w weighted , dw diffusion weighted , hap hepatic arterial phase . 
pvp portal - venous phase , hb hepatobiliary phase a data are mean standard deviation could help to identify those patients at higher risk for hcc development . in conclusion , this study demonstrated that indeterminate hepatocellular nodules in cirrhotic patients rarely progress into hypervascular hccs . 
639 , zhi zao ju road , shanghai200011 , china vol . : ( 0123456789 ) 1 3 562 la radiologia medica ( 2018 ) 123 : 561562 table 1 comparison of the datasets presented in solitary fibrous tumours in the extracranial head and neck region : correlation of ct and mr features with pathologic findings . 
it seems that more often than not whenever a study is published that describes signal increases in the dentate nuclei and globus pallidi on unenhanced t1 - weighted images following the exclusive administration of macrocyclic gbcas , there is immediately a response either from the contrast manufactures [ 2 , 3 ] or from other interested parties considered experts in the field [ 4 ]  . 
the fact that our results differ from those of others should not draw unwarranted criticism and invalidate the study but instead should draw attention to the complexity of the issues involved . 
a first report by stojanov [ 5 ] in patients with relapsingremitting multiple sclerosis ( rrms ) was heavily criticized in part because of the methodological design ( lack of control for previous administrations of gbcas other than gadobutrol prior to consecutive gadobutrol administrations ) and in part because of the lack of visible t1 - hyperintensity on the images presented [ 2 ]  . 
it is strange that our study in patients with rrms should now be criticized even though the patients received exclusively either gadoterate or gadobutrol and despite clear visible evidence of t1 - hyperintensity with both of these gbcas . 
it should be noted that clear visible * alessandra splendiani alessandra.splendiani@cc.univaq.it 1 biotechnological andapplied clinical sciences department , university oflaquila , laquila , italy t1 - hyperintensity has recently also been demonstrated by bjrnerud etal . 
it should be pointed out that not all of the patients evaluated showed increases in t1 - hyperintensity but that some did ( approximately one - third , as stated )  . 
they then go on to state that the example shown in figure4a , b is from a patient who received the highest level of injections , and the signal was already visible in the dn prior to injection of gadoterate meglumine . 
regarding the latter comment , first , it is curious that the authors of the letter should themselves note t1 - signal yet later conclude that our data show no evidence of gadolinium retention in brain after multiple injections of the macrocyclic gbcas . 
while it is true that other pathologic conditions may lead to t1 - signal increases in the dn , t1 - hyperintensity following multiple gbca administrations has invariably been taken as being at least suggestive of gadolinium retention . 
ignoring the visible t1 - signal in our study while taking it as indicative of gd retention in others suggests the authors of the letter are being highly selective in how they define evidence . 
this points to a lack of impartiality on the part of certain investigators and brings into question the motivations for their criticisms . the authors final comment : the data reported in this article confirm the previous studies , showing no evidence of gadolinium retention in brain after multiple injections of the macrocyclic gbcas is absurd . 
furthermore , the statement not only ignores studies in autopsy series that have unequivocally shown gadolinium retention in brain after multiple injections of macrocyclic gbcas [ 9 ] but also ignores the considered opinion of respected american college of radiology ( acr ) experts who recently issued the following statement : while less sensitive studies that rely upon visually observable changes in t1 - weighted mri signal do not suggest macrocyclic agents deposit gadolinium within brain tissue , more quantitative mass spectrometry data from multiple sources have confirmed that they do , albeit at lower levels [ 10 ]  . the concluding comment that our data show no evidence of gadolinium retention in brain after multiple injections of the macrocyclic gbcas is akin to saying if you cant see it , its not there . 
 [ 11 ] found comparable amounts of the intact chelate for macrocyclic and linear agents in the brain but gadolinium bound to macromolecules resulting in high relaxivity molecules that are supposedly causing the signal intensity increase exclusively for linear and not for macrocyclic gadolinium - based contrast agent . 
both our data and those of stojanov provide evidence that gadolinium retention in the brain occurs after multiple injections of macrocyclic gbcas . in conclusion , we feel our results are consistent with the currently available information that suggests gadolinium retention in the brain for all gbcas irrespective of their molecular structure . 
however , in common with all retrospective analyses of t1 - signal changes after gbca administration , it suffers from intrinsic study design and methodology limitations which are evident in all studies of this type . 
treatment response was monitored by diffusion - weighted magnetic resonance imaging ( dw - mri ) and dynamic contrast - enhanced mri ( dce - mri ) obtained 1day before , 14 and 60days after treatment . 
this paper shows an original project concerning about a possible palliative treatment not only in a murine model ( preclinical setting ) but also in humans . keywords iodine - 125 seeds brachytherapy pancreatic ductal adenocarcinoma xenografts diffusion and perfusion imaging introduction pancreatic ductal adenocarcinoma ( pdac ) is one of the most malignant tumors , which mostly originates from pancreatic ductal epitheliuits incidence and mortality have increased significantly in recent years . 
639 , zhizaoju road , shanghai200011 , china institute ofmedical imaging andengineering , university ofshanghai forscience andtechnology , shanghai , china 3 hainan west central hospital , danzhou , hainan , china treatment of pdac is early surgical resection . 
however , there is still controversial about the efficacy of 125i seeds brachytherapy for the unresectable pdac . to accelerate elucidation of the efficacy of 125i seeds permanent brachytherapy in pdac , there is a need for a method to evaluate therapy response . 
therefore , multiparametric mr imaging based on adc and perfusion parameters would provide full evaluation of response to 125i seeds brachytherapy for pdac . in this study , we intend to evaluate efficacy of 125i seeds brachytherapy for pdac xenografts . 
furthermore , we investigated treatment response to 125i seeds brachytherapy with dwi and dce - mri in a pdac xenograft model . materials andmethods this study was approved by the institutional animal care and use committee of the shanghaininth peoples hospital affiliated to shanghaijiao tong university school of medicine . cell culture andreagents to establish pdac xenografts in nude mice , human sw - 1990 pdac cells were obtained from the chinese academy of science . 
the cell suspension was prepared for injection into the nude mice . pdac xenograft model twenty 4 - week - old balb / c male nude mice weighing 1820g were bought from the shanghai jiao tong university school of medicine experimental animal center . 
imaging studies were conducted before therapy initiation ( baseline ; day 0 ) , 14 , and 60days after therapy . single shot echo - planar sequences were used to perform dwi with fat suppression and b - values ( 0 ; 500s / mm2 ) in three orthogonal gradient directions ( x , y , and z )  . 
the acquisition parameters are as follows : repetition time ms ( tr ) / echo time ms ( te ) , 2200 / 75.8 ; diffusion separation time , 16ms ; diffusion gradient duration , 6ms ; matrix , 6464 ; field of view ( fov ) , 8040mm ; slice thickness , 1.8mm , and slice gap , 0.2mthe mr functool 2 analysis software was used to calculate the adc maps in an offline workstation ( adw 4.4 , ge healthcare , usa )  . 
 regions of interests ( rois ) , respectively , enveloped the entire tumor , peripheral zone , and central zone without seeds . the dce - mri protocol included the precontrast t1 - weighted images ( t1wi ) and a dynamic enhanced series of 288 t1wi using a rapid phase gradient echo sequence ( fspgr ) - lava flex . 
ktrans ( volume transfer constant , ml / mlmin ) , v e ( extravascular extracellular volume fraction ) , k ep ( rate 1 3 la radiologia medica ( 2018 ) 123 : 481488 constant , min1 ) , and timeintensity curves were calculated based upon the tofts model [ 10 ]  . tumor volume was measured on postcontrast t1wi . 
 each section of tumor was manually delineated by two observers ( kaicheng li , 20years of experience in clinical mr imaging ; yu liu , 8years of experience in experimental mr imaging ) in consensus . 
and all sections were summed afterward . histological analysis at day 60 , all survival invivo tumors were collected , and hematoxilin and eosin ( h&e ) staining , terminal deoxynucleotidyl transferase mediated dutp nick end labeling ( tunel ) , and cd31 staining were performed . immunohistochemical analysis was performed according to the same procedure with reported previously [ 11 ]  . 
 the percentage of positive staining cells was defined as the ratio of positive staining cells to total cells . statistical analysis statistical analysis was performed with spss 13.0 software ( spss inc . , chicago , il , usa )  . 
one - way analysis of variance ( anova ) was performed to compare the adc values and perfusion parameters among the different treatment periods ( day 0 , 14 , and 60 ) within the experiment and control group . 
although the mean tumor volumes in both groups continued to increase at 14 and 60days after therapy initiation , most notably , 125i seeds were able to inhibit tumor growth effectively . 
the baseline perfusion parameters ( ktrans , ve , and kep ) did not reach a significant difference between the 125i seeds group and control group ( wholetumor rois )  . 
to our knowledge , this is the first report on dwi and dce - mri study evaluating therapeutic efficacy of 125i seeds brachytherapy in a pdac xenograft model . our results showed that 125i seeds brachytherapy could inhibit tumor growth and angiogenesis and promote cell apoptosis and necrosis in pdac xenografts . 
other studies also demonstrated a similar result that 125i seeds brachytherapy showed obvious apoptosis and more potent antitumor activity accompanied by the radiation dose increase [ 11 ]  . tumor adc has been reported to be a sensitive imaging biomarker for detecting treatment response in various tumors , including breast cancer , sarcoma , brain tumors , and lung cancer [ 1317 ]  . 
our study results indicated that early and long response to 125i seeds brachytherapy in pdac xenografts could be detected by adc values , and the adc values increased in sequence in the 125i seeds group . 
this result is consistent with other results that a significant adc increase in orthotopic pancreatic tumors was detected after anti - dr5 therapy , prior to visible change in tumor morphology [ 18 ]  . dce - mri provides some parameters that can reflect tumor neoangiogenesis and microvasculature . 
images showed the ktrans maps and timeintensity curves ( tics ) of the entire tumor regions ( white line ) at baseline ( a , b ) , 14 days ( c , d ) , and 60 days ( e , f ) after treatment with 125i seeds . 
and the perfusion parameters were listed under the tics similar to other study about dce - mri of pdac treated with cetuximab and irinotecan , in which the ktrans decreased and the ve changes showed no statistical difference in the entire tumor region [ 9 ]  . 
 second , the use of untreated mice as control group , though adequate for efficacy study , might suffer from bias related to the influence of the insertion procedure in particular for the study of tumor vascularization and necrosis . 
representative microphotographs of h&e ( 100 original magnification ) ( a ) , tunel ( 400 original magnification ) ( b ) , and cd31 ( 400 original magnification ) ( c ) staining of tumors in the 125i seeds group collected at day 1 3 488 la radiologia medica ( 2018 ) 123 : 481488 in conclusion , 125i seeds brachytherapy can effectively inhibit the cell proliferation of pdac and lead to higher degree of necrosis and necroptosis and lower microvessel density . 
there was a significant global effect size ( r2 = 0.934 ; p < 0.001 ) , which yielded a total variance of 93.4%. conclusions our findings support researchers decision to stop the misuse of if alone to evaluate radiologists and other researchers should review journals bibliometrics for their decision - making during the manuscript submission phase . 
cuauhtemoc , 06726mexicocity , mexico 2 magnetic resonance unit , medica sur clinic andfoundation , mexicocity , mexico 3 departamento de neuroquimica , instituto nacional de neurologia y neurocirugia , mexicocity , mexico introduction the impact factor ( if ) reflects the relative importance of a journal within its field and quantifies the frequency with which the average article in a journal has been cited in a particular period [ 1 ]  . 
if for a given indexed journal is calculated dividing the number of times the articles published in a journal are cited during the two previous years , by the number of articles published by that journal in the same interval [ 2 ]  . 
although if has become the leader metric for consideration of tenure and promotion , and for budget and resource planning in most of the universities , research institutions , and colleges [ 3 ] , contradictory opinions are stating that the if is not a perfect metric and has severe limitations [ 47 ]  . recently , the american society for cell biology , with journal editors , publishers , and other stakeholders , issued a pledge to move away from an over - reliance on journal vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 524534 impact factor and to seek new ways of assessing research output [ 8 ] ; a similar opinion appeared in an editorial of bmc medicine [ 9 ]  . 
furthermore , recent articles in journals of the radiology , nuclear medicine and medical imaging category , written by editors and authors , commented on several aspects of the if and its association with concurrent bibliometrics [ 1 , 7 , 1012 ]  . alternative bibliometrics from the impact factor ( if ) , all of them reported annually by the web of knowledge managed by thomson reuters [ 13 ] have been claimed to improve the esteem of journals in specific categories [ 14 , 15 ]  . 
of articles [ published ] , cited halflife , eigenfactor score ( es ) , and article influence score . to further analyze the relationship between citations and bibliometrics of radiology , nuclear medicine and medical imaging journals which are reported annually by the web of knowledge , we assessed the bibliometrics from these journals and calculated their annual predictive ability for total - cites calculation in a 7 - year period . 
our findings might help authors to understand which bibliometrics offer a better ranking of journals before submission . materials andmethods study design a retrospective study to evaluate the performance of journals in the radiology , nuclear medicine and medical imaging category from the web of knowledge [ 13 ] recorded the values of eight selected bibliometrics listed in the journal citations reports ( jcr ) [ 16 ] in a 7 - year period . 
definitions of each used bibliometric from the web of knowledge have been recently published [ 15 ]  . definitions of the alternative bibliometrics from the web of knowledge : 1 . 
eigenfactor score ( es ) is considered an indicator of the global influence or repercussion of manuscripts published online in journal citation reports ( jcr ) as part of the web of knowledgesm . 
article number ( an ) is the number of articles published during the selected year . journal selection andmeasured periods we chose the bibliometrics values of journals in the radiology , nuclear medicine and medical imaging category of the jcr science edition . 
we assembled five sets of bibliometrics for each journal and for each selected year that matched to its total citations 2 - year ahead : set 1 : 2007 bibliometrics vs . 
even with different n and only a few dependent variables ( dvs ) , a sample size of about 20 in the smallest cell should ensure robustness ; we got a total of 124 measurements per bibliometric included in our assessment . 1 3 526 la radiologia medica ( 2018 ) 123 : 524534 table 1 list of journals in the radiology , nuclear medicine and medical imaging category source : journal citation report , science edition ; 20072013 1 . 
a linear mixed effects model with random slopes and intercepts was used to test the hypothesis that alternative bibliometrics of the web of knowledge surpasses the if as predictors of a total - cite calculation . 
level 1 , the selected bibliometrics ( continuous variables ) consecutively measured during 5 years ; level 2 , the year of citation ( that is time , the repeated measures ) ; and level , 3 the journal id ( levels 1 and 2 are nested within each journal )  . 
the 2 - years ahead total citations was the dependent variable . mixedmodel effects analysis data were analyzed using maximum likelihood ( ml ) estimation ; it is considered an appropriate approach for studying individual change , besides ml , focuses on the entire model ( both fixed and random effects ) ; for our data , it created a hierarchical model that nested repeated measures at six consecutive years within to specify the within - individual error covariance structure that best fits the data and protects the precision of estimates for the appropriate model , we evaluated the most common covariance matrixes types reported in the literature ( unstructured , scaled identity , compound symmetry , diagonal ) [ 23 ] ; then , each matrix type generated a different model . 
 the fitness of the models was assessed with the 2 - log likelihood ( i.e. , likelihood ratio test / deviance test ) , akaikes information criterion ( aic ) , and bayesian information criterion ( bic )  . our model considered the fixed effects of the selected independent variables . 
we added a random effect for the repeated measures , which allowed us to resolve the nonindependence of data by assuming a different baseline of the continuous independent variables values for each journal . 
this effect characterizes the characteristic variation due to individual differences ; the model design expected multiple responses per journal , and these reactions would depend on each journals baseline level [ 24 ]  . 
graphical representation of the fitting of the data was performed using scatter plot of the predicted versus the observed values of total citations for the whole model , labeled by subgroups ( year of citations )  . 
linear regression ( lr ) analysis allowed the measurement of r2 and p values [ 25 ]  . 1 3 528 la radiologia medica ( 2018 ) 123 : 524534 measure oftheeffect size results we computed a pseudo - r2 as a measure of global effect size statistic , even though the response variable variance was partitioned into five levels in our model . 
as previously described , we use the predicted score for each participant in the sample , calculate the correlation between the observed and predicted scores , and squared that correlation [ 22 ]  . 
we plotted the selected bibliometric values from 2007 to 2013 and performed a split - plot factorial anova . displacement oftheranking place to show a graphic representation of how alternative bibliometrics could reorder the top 25 journal initially ranked by the if after the analysis , we present a simple graph line connecting the rankings of the 25s top journals with their most significant predictive metrics . we performed separate analyses using the most common covariance matrixes types ; the unstructured matrix type represented the best model by depicting the smallest values in the information criteria table . 
this matrix type has been reported to offer the best fit and is most commonly found in longitudinal data as it is the most parsimonious , which requires no assumption in the error structure [ 27 ]  . 
table2 shows the assessment of the overall fit of the multivariate models . significant predictors oftotal citations andbeta coefficients oftheregression model all independent variables were included : impact factor , 5year impact factor , immediacy index , no . 
figure2 shows graph lines identifying each selected journal in the final model ; the existence of random slopes and intercepts is evident . and es nor a main effect of time ( p > 0.05 in both analyses )  . 
 for those journals with an if > 3.0 , there was a continuous growing trend from 2007 to 2013 ; journals with an if between 2 and 3 decrease in their value after 2010 ; and those below 2.0 if remained stable after that date . 
figure4a , b shows the if and es trends plotting the split - plot anova . global effect displacement ofjournals previously ranked bytheif the global effect size ( pseudo - r2 correlation between the observed and predicted scores ) for the whole model depicted an r2 value = 0.934 , p < 0.001 ; this value corresponds to a large effect size . 
figure3 illustrates the regression line between the observed and predicted values for total citations . evolution ofifandes overtime the split - plot anova showed no significant interaction between time and if ( p > 0.05 ) , but a main effect of time ( p < 0.001 ) ; there was neither an interaction between time there was a significant re - ranking among the top 25s journals initially listed by the if ( the year 2013 )  . 
after we had reclassified the journals based on their es , only 16 journals remained in the top 25 , some were demoted , but the rest climbed higher ; some examples include : jaac - cardiovas imag moved from 1st to 20th , and med phys jumped from 25th to 6th position . 
figure5 depicts the ranking displacements based on if , es , and chl . table 3 significant predictors of total cites for selected bibliometrics f ratio intercept impact factor 5 - year impact factor immediacy index no . 
usually , researchers look for journals with the highest impact factor instead of journals with the best audience for their research [ 4 ]  . the success of researchers is nowadays judged by the number of publications they have published in high if journals [ 28 ]  . 
the assessment of the scientific impact of journals evaluated by bibliometrics is a complex , multi - dimensional construct and therefore the use of a single bibliometric index is inappropriate to rank , evaluate , and value table 4 directions of the relationship between each predictor and the outcome ( total citations ) are represented by a positive or negative regression coefficient ( b value ) ; it is evident the large beta coefficient of the eigenfactor score signaling it as the most influential predictor of total citations ivs ( bibliometrics ) se b 95% confidence interval lower bound upper bound intercept impact factor 5 - year impact factor immediacy index no . 
lines represent the predicted values of total citations ( number ) at each year of measurement ; the existence of random slopes and intercepts among the journals is evident readers should look beyond the impact factor and assess scientific articles individually [ 29 ]  . 
preferably , the use of multiple metrics with complementary features provides a more comprehensive view of journals and their relative placements in their fields [ 30 ]  . our study shows additional evidence to numerous reports about the apparent limitations of the if as a significant predictor of total citations [ 5 , 3133 ]  . 
the use of mixed - models analyses allowed us to study intraand interindividual differences in the curve parameters ( slopes and intercepts ) [ 23 ] ; this assessment dismisses the assumption of homogeneity of regression slopes , cast aside the assumption of independence ( between cases ) , and expect the presence of missing data [ 24 ]  . 
our results evince the es as the bibliometric which captures best the prestige of a journal , this fact has been previously compared with the ability of the if [ 34 ]  . 
however , our data are limited to state if the es can assess the actual dissemination of an article ( i.e. , its use , as well as the category of journals which include it in their reference lists ) [ 20 ]  . 
we consider our finding that journals with es values higher than 0.01201 showing a decreasing trend from 2007 to 2011 and then a growing recovery continued until 2013 , depicts a real pattern in the data , as this was a subgroup analysis not observed with lower es values . our findings agree with a similar study in the gastroenterology and hepatology category [ 14 ]  . 
on the other hand , es is a per - journal measure that represents each journal size , based on its total citations ; therefore it is considered superior for evaluating the quality of journals [ 34 ]  . 
the non - significance of the if is explained as it measures citations per article , then , is a poor indicator of total citations given that scholarly journals vary in size over multiple orders of magnitude . the es is gaining traction , because it focuses on the impact of particular articles , but dependence solely on citations still limits it . 
the rest of bibliometrics is less well - known as predictors of citations , for example , the number of articles at least scales with a journal size , but does not account at all for quality ; this left the es as a winner in an unbalanced competition [ 14 ]  . 
4 graphical representation of the if and es trends over time ( from 2007 to 2013 ) in the radiology , nuclear medicine and medical imaging category using a split - plot anova with a 5 - level rank . 
b , regarding es , journals with values higher than 0.01201 , showed a decreasing trend from 2007 to 2011 with an increasing trend continued until 2013 1 3 532 la radiologia medica ( 2018 ) 123 : 524534 fig . 
5 graphical representation of displacements in the ranking order of the top 25 journals ; after re - ranking the journals by their es , only 16 chronicles remained in the top 25 , the rest were demoted ; in a second re - ranking by chl , only 3 of the first top 25 if journals stayed within the top 25 positions with a positive correlation to the if ( r = 0.94 ) , however , we did not find an analysis of ais similar to our study [ 36 ]  . readers should be aware that even though the number of citations has been widely used as a metric to rank papers , recently some iterative processes are considering new approaches , such as the pagerank algorithm which has been applied to the citation networks [ 37 ]  . 
moreover , more modern usage - based article - level metrics are being also explored such as the usage factor , publisher and institutional repository usage statistics ( pirus2 ) , and the y - factor [ 30 ]  . additional factors are worth mentioning : each medical specialty depicts different if threshold , for example , a journal in the oncology field might have an if up to 30 times as high as the corresponding figure in the forensic medicine category [ 3 ]  . 
that is , citations are not equally distributed , with fewer than 20% of the articles accounting for more than 50% of the total number of citations [ 39 ]  . 
despite these facts , the misuse of the if for judging the value of science persists , because it confers significant benefits to individual scientists and journals [ 40 ]  . several limitations of this study need to be addressed : a detailed explanation of each bibliometric is beyond the scope of this article ; our analysis was not a conventional regression model , but a linear mixed effects design . 
part of the benefits of a study of this kind is that the assumption of independence ( between cases ) is cast aside , and correlation among variables in the model is expected [ 24 ]  . 
after our previous articles on this topic were published in 2015 and 2018 , we looked forward to being consistent our previous reports [ 14 , 15 ]  . additional factors , such as longer time frames , the number of articles published in each issue , circulation of each journal , host of factors impacting citation ( self - citation , semi - mandatory , and mandatory citation ) might all influence citation calculations . 
we did not include these possible confounding factors , as the web of knowledge does not consider thewe acknowledge that normalization of journal citations by its article count is desirable . 
also , a factor that may affect author where to submit 1 3 la radiologia medica ( 2018 ) 123 : 524534 their work were outside the scope of this study : topic , affiliation with society , geography , rejection by earlier submission , familiarity with the submission and revision process , turnaround time and invitation by editors . 
we do not consider this study a case of self - plagiarism finding the similarities in the used methodology , but a needed proof - ofconcept ( poc ) ; we mean the attainment of a specific method to demonstrate its feasibility . 
because a poc aim assesses the real potential of a method for its clinically meaningful effects in the intended population [ 41 ] , we repeat the same methodology ( linear mixed model design ) to our target journal category and were able to obtain similar results . 
readers should be aware that the jcr includes approximately 171 categories in the sciences and 54 in the social sciences ; then , publication of future studies validating our model in other specialties would be desirable . in conclusion , impact factor and immediacy index shows no ability to predict 2 - year ahead annual - citations , our findings support researchers decision to stop the misuse of if alone to evaluate a re - ranking of journals using eigenfactor score , article influence score , and cited halflife provides a better assessment of the significance and importance of scientific journals in particular disciplines . 
 radiologists and other researchers should review these scores for their decision - making during the manuscript submission phase ; they may even become a new standard of the quality and validity of the research . acknowledgements ulises orbe - arteaga , msc , was a research fellow at the mri unit of medica sur clinic and foundation during 2014 2015 . 
us and ct images in each case were retrospectively reviewed by a radiologist at each institution , and classified into one of the following four categories based on us and ct features : no dtd ; indeterminate ; suspicious for dtd ; and dtd . 
the diagnostic accuracy of us and ct were calculated at each institution by comparison with histopathological results . results respective us and ct classifications in the 177 patients were no dtd in 75 and 71 , indeterminate in 46 and 34 , suspicious for dtd in 28 and 31 , and dtd in 28 and 41 . 
among the histopathological results , 113 patients had normal thyroid parenchyma , 23 had hashimoto thyroiditis , 36 had non - hashimoto lymphocytic thyroiditis , and 5 had diffuse hyperplasia . 
 nodular thyroid disease is a localized form , whereas diffuse thyroid disease ( dtd ) is characterized by involvement of the entire thyroid gland , and is a main cause of thyroid dysfunction [ 2 ]  . 
accordingly , the purpose of the present study was to compare the diagnostic performance of ct and us for the detection of incidental dtd using static us and ct images , multicenter data , and histopathological results as a reference standard . materials andmethods patients the present retrospective analysis was based on patient data collected from four university - affiliated hospitals . 
between july and december 2016 , patients who met the following criteria at each institution were included : underwent thyroid surgery for the treatment of nodular thyroid lesions ; received at least one preoperative thyroid us examination ; and underwent preoperative neck ct for tumor staging . 
faculty radiologists specializing in head - and - neck imaging or supervised board - certified radiologists participating in head - and - neck radiology fellowship training performed all us examinations . four board - certified radiologists ( with 5 , 6 , 10 , and 15years experience with thyroid us examination after obtaining board certification ) performed retrospective analyses of us images using a picture - archiving and communication systeeach radiologist analyzed the us findings from study patients at each institution , and was blinded to the ct diagnosis , clinico - serological information , and patient medication history for dtd . 
based on the literature [ 4 , 7 ] , the following features were investigated in the static us images : echogenicity ( iso - , low , or high ) ; echotexture ( fine , coarse , or micronodulative ) ; anteroposterior diameter of the thyroid gland [ normal ( 12cm ) , increased ( > 2cm ) , or decreased ( < 1cm ) ] ; glandular margin ( smooth or lobulated ) ; and vascularity ( normal , decreased , or increased )  . based on the us features , the enrolled patients were classified into four categories , as follows : those without abnormal us features were classified as no dtd ; those with 1 abnormal us feature were classified as indeterminate ; those with 2 abnormal us features were classified as suspicious for dtd ; and those with 3 abnormal us features were classified as dtd . neck ct andretrospective image analysis for tumor staging before thyroid surgery , neck ct ( slice thickness , 3mm ; reconstruction increment , 3mm ) was performed using contrast medium ( 23ml / s and 40s delay time ) and a 64 - channel multi - detector ct scanner ( brilliance 64 ; philips medical systems , cleveland , oh , usa and discovery ct 750hd sp 64 ; ge medical systems , milwaukee , wi , usa ) or a 128 - channel multi - detector ct scanner ( lightspeed ; ge medical systems and somatom definition as + ; siemens healthcare , forchheim , germany )  . 
non - enhanced axial , contrast - enhanced axial , and contrast - enhanced coronal reformatted ct images were acquired in all cases . four board - certified radiologists ( with 4 , 6 , 10 , and 15 years experience with neck ct interpretation after obtaining board certification ) performed the retrospective analyses of ct images using a picture - archiving and communication systeeach radiologist analyzed the ct findings from study patients at each institution , and was blinded to the us diagnosis , clinico - serological information , and patient medication history for dtd . 
based on the literature [ 5 , 6 ] , the ct features of the thyroid gland were retrospectively analyzed in terms of the degree and pattern of parenchymal attenuation in the non - enhanced ct images , glandular size and margin in the contrast - enhanced ct images , and degree and pattern of parenchymal 1 3 la radiologia medica ( 2018 ) 123 : 515523 enhancement in the contrast - enhanced ct images as follows : degree of parenchymal attenuation was divided into iso - , low , or high ; patterns of both glandular attenuation and enhancement were categorized into homogeneous or inhomogeneous ; anteroposterior diameters of both lobes of the main thyroid were measured , averaged , and classified into 1 of 3 categories : 12cm ( normal ) , < 1 , or > 2cm ; margin of the thyroid was classified as smooth or lobulated ; degree of parenchymal enhancement was classified as normal , decreased , or increased . based on the ct features , the enrolled patients were classified into four categories , as follows : those without abnormal ct features were classified as no dtd ; those with 1 abnormal ct feature were classified as indeterminate ; those with 2 abnormal ct features were classified as suspicious for dtd ; and those with 3 abnormal ct features were classified as dtd . histopathology histopathological findings from the thyroid gland were classified by board - certified pathologists from each of the affiliated hospitals . 
non - hashimoto lymphocytic thyroiditis exhibited diffuse infiltration of the thyroid gland with lymphocytes and other inflammatory cells but none of the typical histopathological features of hashimoto thyroiditis such as oxyphilic metaplasia , follicular atrophy , or follicular disruption . 
the thyroid gland was considered to be normal thyroid parenchyma ( ntp ) when there was no visual evidence of coexisting dtd . statistical analysis to evaluate the differences in ct and us features between dtd and ntp , independent t tests were used for continuous variables and the pearsons 2 test or , for small cell values , fishers exact test for categorical variables . 
all statistical analyses were performed using spss version 24.0 ( ibm corporation , armonk , ny , usa ) and medcalc version 14.10 ( medcalc , belgium ) ; p < 0.05 was considered to be statistically significant . results patient characteristics based on the histopathological results from 177 patients , 64 ( mean age of 45.3years with an age range of 2175years ; male : female = 8 : 56 ) were subsequently classified as dtd and 113 ( mean age 45.6years [ range 1579years ] ; 25 male , 88 female ) as ntp . 
after thyroid surgery , papillary thyroid carcinoma [ 163 / 177 ( 92.1% ) ] , follicular thyroid carcinoma [ 2 / 177 ( 1.1% ) ] , follicular adenoma [ 4 / 177 ( 2.3% ) ] , and nodular hyperplasia [ 8 / 177 ( 4.5% ) ] were identified . 
on histopathological analysis , ntp [ 113 / 177 ( 63.8% ) ] , hashimoto thyroiditis [ 23 / 117 ( 13.0% ) ] , non - hashimoto lymphocytic thyroiditis [ 36 / 177 ( 20.3% ) ] , and diffuse hyperplasia [ 5 / 177 ( 2.8% ) ] were found . 
in the comparison of us classification and histopathological results , the 75 cases assigned to the no dtd category included hashimoto thyroiditis ( n = 2 ) , non - hashimoto lymphocytic thyroiditis ( n = 4 ) , diffuse hyperplasia ( n = 0 ) , and ntp ( n = 69 )  . 
the 28 cases assigned to the suspicious for dtd category included hashimoto thyroiditis ( n = 8 ) , non - hashimoto lymphocytic thyroiditis ( n = 12 ) , diffuse hyperplasia ( n = 1 ) , and ntp ( n = 7 )  . 
the 28 cases assigned to the dtd category included hashimoto thyroiditis ( n = 10 ) , non - hashimoto lymphocytic thyroiditis ( n = 11 ) , diffuse hyperplasia ( n = 4 ) , and ntp ( n = 3 )  . comparisons of individual ct features between ntp and dtd are summarized in table2 . 
in data presented in parentheses are percentage of each item ct computed tomography , dtd diffuse thyroid disease the comparison of ct classification and histopathologic results , the 71 cases assigned to the no dtd category included hashimoto thyroiditis ( n = 2 ) , non - hashimoto lymphocytic thyroiditis ( n = 2 ) , diffuse hyperplasia ( n = 0 ) , and ntp ( n = 67 )  . 
the 34 cases assigned to the indeterminate category included hashimoto thyroiditis ( n = 1 ) , nonhashimoto lymphocytic thyroiditis ( n = 5 ) , diffuse hyperplasia ( n = 0 ) , and ntp ( n = 28 )  . 
the 31 cases assigned to the suspicious for dtd category included hashimoto thyroiditis ( n = 6 ) , non - hashimoto lymphocytic thyroiditis ( n = 11 ) , diffuse hyperplasia ( n = 0 ) , and ntp ( n = 14 )  . 
1 ultrasonography ( us ) and computed tomography ( ct ) images from a 32 - year - old woman diagnosed with hashimoto thyroiditis on histopathological examination , which was determined to be diffuse thyroid disease ( dtd ) category on both us and ct ( papillary thyroid carcinoma in the right thyroid )  . 
in the longitudinal gray - scale ( a ) and color doppler ( b ) sonograms , the thyroid gland ( arrows ) exhibits hypoechogenicity , coarse echotexture , anteroposterior diameter > 2cm , lobulated margin , and increased vascularity . 
in the nonenhanced ( c ) and contrast - enhanced ( d ) axial ct images , the thyroid gland ( arrows ) shows low , but homogeneous attenuation , anteroposterior diameter > 2cm , smooth margin , and normal but inhomogeneous enhancement diagnostic performance ofus andct classifications in roc curve analyses , the classification of 2 features of dtd was to be the best predictor of dtd on both of us and ct diagnoses . 
there were no statistically significant differences in all values between us and ct diagnoses [ p > 0.05 ( mcnemar test ) ]  . analyses ofus andct diagnoses according toindividual institution us classifications for detecting dtd at each institution are summarized in table3 . 
 in all institutions , the prevalence of the indeterminate category was 39.0% ( 46 / 177 ) , ranging from 17.1% ( 7 / 41 ) to 37.5% ( 15 / 40 )  . 
when the indeterminate category cases were excluded , the prevalence of false - negative diagnosis for detecting dtd was low ( mean 4.6% [ 6 / 131 ] ; range 0% [ 0 / 25 ] to 8.8% [ 3 / 34 ] ) and the prevalence of false - positive diagnosis was variable [ mean 7.6% ( 10 / 131 ) ; range 2.9% ( 1 / 34 ) to 14.3% ( 5 / 35 ) ]  . ct classifications for detecting dtd at each institution are summarized in table4 . 
in all institutions , the prevalence of the indeterminate category was 19.2% ( 34 / 177 ) , ranging from 12.2% ( 5 / 41 ) to 35.6% ( 16 / 45 )  . 
among the four institutions , three demonstrated higher sensitivity in ct and higher specificity in us , whereas one demonstrated similar sensitivity and specificity between ct 1 3 520 la radiologia medica ( 2018 ) 123 : 515523 fig . 
2 ultrasonography ( us ) and computed tomography ( ct ) images from a 36 - year - old woman diagnosed with non - hashimoto lymphocytic thyroiditis on histopathological examination , which was determined to be no diffuse thyroid disease ( dtd ) category on us , but dtd category on ct ( papillary thyroid carcinoma in the left thyroid )  . 
in the longitudinal gray - scale ( a ) and color doppler ( b ) sonograms , the thyroid gland ( arrows ) demonstrates isoechogenicity , fine echotexture , anteroposterior diameter of 12cm , smooth margin , and normal vascularity . 
in the non - enhanced ( c ) and contrast - enhanced ( d ) axial ct images , the thyroid gland ( arrows ) exhibits low and inhomogeneous attenuation , anteroposterior diameter of 12 cm , smooth margin , and decreased but homogeneous enhancement and us . 
in the literature , us features of dtd include low echogenicity , coarse or micronodulative echotexture , lobulated margin , and increased parenchymal vascularity [ 4 , 7 ] , whereas ct features of dtd include low and inhomogeneous attenuation , increased gland size , and increased and inhomogeneous enhancement [ 5 , 6 ]  . 
 similar to previous studies , normal gland size and smooth margin were commonly observed in dtd on both us and ct [ 47 ]  . in the present study , 2 features of dtd demonstrated the highest diagnostic value in both us and ct , similar to 1 3 la radiologia medica ( 2018 ) 123 : 515523 fig . 
3 comparisons of receiver operating characteristic ( roc ) curves representing the diagnostic performance of ultrasonography and computed tomography classifications as the best independent predictor for differentiating diffuse thyroid disease from normal thyroid parenchyma . 
diagonal line = 50% of the area under the roc curve ( auc ) , and also refers to a hypothetical marker that has no discriminatory power for differentiating diffuse thyroid disease from normal thyroid parenchyma : us [ auc 0.866 ( 95% ci 0.8070.912 ) ] and ct [ auc 0.893 ( 95% ci 0.8380.935 ) ] previous us studies reported in the literature [ 4 , 5 ]  . 
to clarify the cut - off number of abnormal ct features for detecting dtd , further study may be required . to our knowledge , only one comparative study of us and ct for detecting dtd has been reported [ 5 ]  . 
the reason for this is unclear ; however , a possible explanation is that our results correspond with results from a previous study in that real - time us was superior to static us for detecting incidental dtd [ 7 ] , and that real - time us and ct demonstrated similar diagnostic values [ 5 ]  . 
furthermore , the prevalence of the indeterminate category was higher for us [ 26.0% ( 46 / 177 ) ] than for ct [ 19.2% ( 34 / 177 ) ]  . 
 1 3 522 la radiologia medica ( 2018 ) 123 : 515523 thus , we believe that ct is a useful tool for differentiating dtd from ntp . this study had several limitations , the first of which was the small sample size at each institution . 
finally , there were differences among the affiliated hospitals with regard to us and ct modalities , and ct protocols . in conclusion , both us and ct demonstrated similar diagnostic value for differentiating dtd from ntp . 
 giaccone - university ofpalermo , via del vespro 129 , 90127palermo , italy 2 department ofradiology , oncology , andanatomy pathology , policlinico umberto - university sapienza , rome , italy 3 department ofsciences forhealth promotion andmother , child care , policlinico p . 
giaccone - university ofpalermo , via del vespro 129 , 90127palermo , italy malignant lesions initially assigned to bi - rads category 3 at conventional mammographic interpretation [ 8 ]  . more recently , shen etal . 
we also performed inter and intra - observer analysis to assess operators variability . materials andmethods study design the whole study has been carried out in accordance with the code of ethics of the world medical association ( declaration of helsinki )  . 
no fbls were excluded due to us imaging being not appropriate for s - detect evaluation . image analysis s - detect is a built - in , commercially available dedicated software installed and running on the ultrasound system rs80a . 
features used for us feature analysis in s - detect are as follows : shape differences , echo and texture features using spatial gray - level dependence matrices , intensity in the mass area , gradient magnitude in the mass area , orientation , depthwidth ratio , distance between mass shape and best t ellipse , average gray changes or histogram changes between tissue / mass area , comparison of gray value of left , posterior , and right under the lesion , the number of lobulated areas / protuberances / depressions , lobulation index , and elliptic - normalized circumference [ 11 ]  . one week before starting the image analysis process , all the readers involved in this study had to attend a separate 5 - h training session and all readers had to evaluate individually and separately by means of s - detect further 20 fbls ( encompassing both benign and malignant mass ) not included in the final study . onsite evaluation two experienced radiologists ( more than 20years of breast us ) subjectively classified by consensus the 300 fbls into 4 categories prospectively : ( 1 ) bi - rads 2 : benign ; ( 2 ) birads 3 : probably benign ; ( 3 ) bi - rads 4 : suspicious ; ( 4 ) birads 5 : highly suggestive of malignancy . 
the analysis of us features was based on the fourth edition of the bi - rads lexicon , which was the only one available on our system at the time of the study . in the same session , the two experienced radiologists choose the most representative image for each of the same 300 fbls and evaluated this image by means of s - detect . 
 the lesions were randomly and independently assessed in separate sessions , to avoid recall bias . information about patients age , family or personal history of breast cancer and previous us investigations were available to the two investigators to better reproduce a real clinical setting and for a meaningful comparison with consensus analysis . 
reviewers were blinded to pathologic findings . standard ofreference ( sor ) to the purpose of this study , us - guided core - biopsy was considered as sor for all the fbls classified as bi - rads 3 , 4 or 5 either before or after s - detect assessment . 
for all lesions classified as bi - rads 2 both before and after s - detect assessment , us findings at 6 , 12 and 24months follow - up have been available at moment of evaluation and considered as sor . 
the difference between sensitivity and specificity is judged to be statistically significant in case of non - overlapping confidence intervals . the improvement in diagnostic confidence was assessed at receiver operating characteristic ( roc ) curve analysis using the response from the five - point grade scale and by plotting the sensitivity ( i.e. , true - positive fraction ) against 1 - specificity ( i.e. , false - positive fraction )  . 
for all tests , p < 0.05 was considered to indicate a statistically significant difference . for retrospective analysis , kappa statistics were calculated to assess inter - operators and intra - operator agreement , between the baseline and after 3months . 
agreement was graded as poor ( 0.20 ) , moderate ( 0.200.40 ) , fair ( 0.400.60 ) , good ( 0.600.80 ) , or very good ( 0.801.00 ) [ 14 ]  . results overall , according to the sor 120 / 300 ( 40% ) fbls were malignant , 2 / 300 ( 0.7% ) fbls were lesions of uncertain malignant potential / b3 ( atypical ductal hyperplasia ) and 178 / 300 ( 59.3% ) fbls were benign ( table1 )  . image analysis : onsite evaluation a not statistically significant increase of fbls correctly characterized by the two experienced radiologists was registered with the use of s - detect when compared to the baseline , with a reduction in the number of both false - negative ( n = 3 vs n = 10 ) and false - positive ( n = 24 vs n = 33 ) cases ( table2 )  . 
65 / 84 ( 77.4% ) fbls were confirmed as bi - rads 3 after the use of s - detect : this confirmation was correct in all 65 cases . 
57 / 77 ( 74% ) fbls were confirmed as bi - rads 5 : this confirmation was correct in 55 / 57 cases and not correct in 2 / 57 cases ( one xanthogranulomatosis showing microlobulated margins and irregular shape and one fibrosis with irregular shape , microlobulated margins and not parallel orientation ) , respectively . twenty - seven out of 300 ( 9% ) fbls remained incorrectly characterized even after the use of s - detect fig . 
dotted blue line , dashed red line , and green line indicate area under the roc curve of the radiologists without s - detect , with s - detect and reference line , respectively . 
right : with s - detect ( green line contour ) margins were classified as microlobulated and partially angular and the lesion was correctly upgraded from bi - rads 3 to bi - rads 4b . 
3 in a 34 - year - old - woman , b - mode us shows a 9 mm slightly hypoechoic , oval shaped and with parallel orientation left breast lesion ( arrow )  . 
4 in a 30 - year - old - woman with mastodynia , b - mode us depicted a 15 mm hypoechoic right breast mass , with parallel orientation ( arrow )  . 
right : with s - detect ( green line contour ) margins were classified as circumscribed : the lesion was incorrectly downgraded from bi - rads 4a to bi - rads 3 . 
however , breast us requires extensive experience , considering that it as an operator - dependent procedure and presents lower reproducibility , specificity and positive predictive value than mammography [ 16 ]  . 
the introduction of a categorization system based on sonographic criteria , such as the breast imaging reporting and data system ( bi - rads ) , has proved useful for describing and classifying both benign and malignant breast lesions [ 1 ]  . 
however , the limited reproducibility of the system in determining the exact likelihood of malignancy of suspicious breast lesions ( category 4 ) , with variability ranging from 3 to 94% , leaves unchanged the need for more invasive and expensive diagnostic procedures , such as biopsy [ 17 ]  . as an attempt to overcome these drawbacks at least in part , image analysis systems have been introduced in mammographic breast cancer screening , aiming at lesion detection [ 18 ]  . 
therefore , a novel and more interactive approach to image analysisaiming at helping radiologist more with decision - making than with simple lesion detectionhas been developed for mammography , showing sensitivity comparable to that of human readers [ 20 ]  . our data confirm that the use of a computer - aided decision - making support can led to an increase of the number of correctly characterized breast masses , both benign and malignant , in the sonographic assessment of fbls , as carried out by experienced radiologists . 
who reported a statistically significant higher area under the roc curve ( 0.725 ) for s - detect guided assessment of a series of 192 fbls in comparison with an experienced radiologist ( 0.653 ) ( p = 0.038 ) [ 10 ]  . 
on the other hand , such an improvement may be still of clinical relevance , considering that , in the present study , s - detect - aided evaluation has led to a change in the initial bi - rads classification in more than one - fifth of fbls , with a statistically significant rate of correct re - classification ( 81% )  . 
5 dotted blue line , dashed red line , and green line indicate area under the roc curve of without s - detect , with s - detect and reference line ( a ) for resident #1 and ( b ) for resident #2 , respectively . 
although this incorrect up - grade would cause unnecessary tissue sampling , increasing cost and discomfort for the involved patients , from the clinical point of view , there is no increased risk of missing malignancies . 
on the other hand , among the 120 malignant fbls studied in our series , only two fbls ( 1.2% ) were erroneously interpreted as probably benign ( bi - rads 3 ) by the s - detect - guided expert radiologists . 
both of them are quite rare breast tumors and , in our series , they showed some us signs of benignity , such oval shape and circumscribed margin , respectively [ 21 , 22 ]  . 
among the two high - risk fbls studied in our series , one atypical ductal hyperplasia , initially missed by the two expert reviewers , was correctly recognized as suspicious by s - detect - assisted reading , whereas the second one was erroneously downgraded to bi - rads 3 category due to the presence of oval shape and circumscribed margin . in our series , the three main us descriptors misleading the classification were , in order of frequency , margin , shape and orientation . 
in addition , lazarus and coworkers have found only a moderate agreement ( k = 40 ) for margin evaluation and even less for echo pattern ( fair : k = 0.29 ) [ 23 ]  . 
in the study by kim etal . , only moderate agreement ( k = 0.58 ) was seen in the final assessment between the radiologist and s - detect [ 10 ]  . 
this increase could be a result of the fact that an image analysis system brings more sonographic features to the attention of the resident , as it has been already reported for computer - aided detection in breast mri [ 25 ]  . 
our experience suggests a possible role of s - detect as useful adjunct tool for physicians or sonographers not expert in breast ultrasound . there are some limitations to this study . 
first , the analysis of us features was based on the fourth edition of the bi - rads lexicon , since s - detect implemented the descriptors of the fourth edition in its analysis . 
hence doppler analysis , which might have helped the readers , was not included in the present study . third , our study is a single - institution study and our series does not necessarily reflect a general population screened for breast cancer , with different values of prevalence of malignancy . 
 clinical presentation included intermittent mild pain associated with a soft tissue swelling / palpable mass in all patients , chronic pain and increased local heat in 29 patients , local swelling and decreased range of motion of the adjacent joint in 45 patients , and all the above symptoms in 23 patients . 
 histologic examination of the remaining five lesions showed nodular fasciitis ( two lesions ) , endometriosis ( one lesion ) , hemangioendothelioma ( two lesions ) ; us of these lesions showed variable size , irregular margins , and deep - seated location . 
shape was most commonly oval ( fusiform ) , margins were most commonly not well defined ( irregular , hazing but circumscribed ) , phleboliths were more common in deep - seated lesions , echo structure was heterogeneous , and echogenicity was most commonly hyperechogen and involuting . conclusion clinical presentation and typical b - mode and color doppler us findings are adequate for the diagnosis of soft tissue hemangiomas without the need for biopsy and histologic analysis . 
if any clinical or us doubt , an us - guided biopsy should be performed . keywords hemangiomas soft tissue ultrasonography diagnosis biopsy introduction soft tissue hemangiomas are benign soft tissue tumors that closely resemble normal vessels [ 1 ]  . 
they account for approximately 7% of all benign soft tissue tumors , may arise at various anatomic locations , and are much more commonly superficial than deep - seated [ 14 ]  . 
diagnosis is usually easy for typical superficial lesions ; however , atypical and deepseated hemangiomas cannot be distinguished from malignant soft - tissue tumors without appropriate imaging studies [ 58 ]  . the imaging modality of choice for the diagnosis of soft tissue hemangiomas is magnetic resonance ( mr ) imaging . 
however , soft tissue hemangiomas most commonly show typical clinical and ultrasonography ( us ) findings that may allow for an accurate and easy diagnosis [ 14 , 1624 ]  . 
in this scenario , us can be used successfully in the same setting to guide biopsy for tissue sampling [ 2124 ]  . the purpose of this study is to describe the clinical and us findings of soft tissue hemangiomas , and to compare with the results of histologic diagnosis . 
our hypothesis was that us is appropriate as a single diagnostic method for these tumors without the need for a biopsy . materials andmethods we performed an observational study on 97 patients with soft tissue hemangiomas admitted and treated at the authors institution from 2004 to 2011 . 
no patient was lost to follow - up ; all patients or their relatives gave written informed consent for their data to be included in this study . clinical findings at presentation included ( 1 ) intermittent mild pain associated with a soft tissue swelling / palpable mass in all patients , ( 2 ) chronic pain and increased local heat in 29 patients , ( 3 ) local swelling and decreased range of motion of the adjacent joint in 45 patients , and ( 4 ) all the above symptoms in 23 patients . 
no patient of these series had an mr imaging examination ; in all these patients the diagnosis was assumed based on typical clinical and us findings , as previously described [ 14 , 2027 ]  . 
us examination was done using a acuson antares premium us device ( siemens ultrasound , mountain view , ca ) from 2004 to 2009 , and a hi vision preirus device ( hitachi medical corporation , japan ) from 2009 to 2011 with a multifrequency ( 512mhz ) linear array transducer . 
the b - mode us protocol evaluated the site and location ( superficial , 74 lesions ; deep - seated , 23 lesions ) , size , shape , margins , presence of calcifications , echo structure ( homogenous or heterogeneous ) , and echogenicity ( hyper , iso or hypo - echogenicity )  . 
 the vascularity and flow were evaluated in power doppler us ( pdus ) with scanning the entire lesion and setting the parameters at the lowest doppler gain to prevent aliasing . 
based on the clinical and us findings , as reported above , a diagnosis of soft tissue hemangioma was made in all patients . after us examination , all patients had us - guided biopsy of their lesions using a 14 - gauge , 100150mm biopsy needle ( biopsy bell , mirandola , mo , italy ) ; biopsies in adults were done under local anesthesia ( 2% mepivacaine , 68ml ) , while in children were done under general anesthesia . 
a direct approach to the tumor was used in all cases after consultation with orthopaedic oncology surgeons ( afm and ce ) so that the biopsy tract was put in line with the incision of an anticipated surgical excision of the tumor . 
us findings were suggestive of a soft tissue hemangioma that was confirmed with us - guided biopsy and histologic examination 1 3 540 la radiologia medica ( 2018 ) 123 : 538544 fig . 
2 a b - mode us shows a deep - seated solid lesion with heterogeneous echo structure , mainly hypoechoic with peripheral hyperechoic rib pdus shows vascularity of the lesion . 
us of these lesions showed variable size , irregular margins , and deep - seated location . histologically documented soft tissue hemangiomas were most commonly superficial ( 74 lesions ) compared to deep - seated ( 18 lesions )  . 
the most common type of hemangiomas was arteriovenous ( 45 lesions ) , followed by cavernous intramuscular ( 37 lesions ) , and capillary ( 10 lesions ) ( table1 )  . 
shape was most commonly oval ( fusiform ) , margins were most commonly not well defined ( irregular , hazing but circumscribed ) , echo structure was heterogeneous , and echogenicity was most commonly hyperechogen ( presence of fat ) and involuting ( table2 )  . 
 no us differences were observed between superficial and deep - seated hemangiomas with respect to site , size , shape , margins , echo structure and echogenicity ; phleboliths were more common in deep - seated lesions ( 11 lesions ) compared to superficial lesions ( 2 lesions )  . 
us findings were suggestive of a soft tissue hemangioma but us - guided biopsy and histologic examination showed endometriosis discussion the diagnosis of soft tissue hemangioma is based on clinical history , physical examination , symptoms , and imaging findings [ 820 ]  . 
typical clinical findings include a smooth and soft palpable mass , particularly superficial , painless or painful during activity , slow - growing or constant in time [ 14 ]  . 
 typical us findings include small size ( usually less than 5cm ) , subcutaneous location , heterogeneous echotexture with multiple regular cystic or tubular spaces and echogenicity depending on the prevalent tissue in the lesion ( most commonly hyperechogenicity due to presence of fat ) , hazing margins ( not completely well - defined ) , intralesional regular vascular formations of different caliber and regularly distributed , calcifications ( phleboliths ) , good compressibility , 1 3 la radiologia medica ( 2018 ) 123 : 538544 the present study did not evaluate a control group but was based on observational ( clinical and imaging ) findings of a single center physicians . 
however , the observed high diagnostic accuracy and the findings based on the experience of a large tertiary tumor center as the authors own center increase the power of our analysis and conclusions . 
however , we did not compare to a control group of patients with soft tissue tumors to evaluate the diagnostic accuracy of us , but we shorted our analysis only in patients with the clinical diagnosis of soft tissue hemangiomas to evaluate in these patients the diagnostic accuracy of us . 
we believe that in this setting , a statistical analysis is not applicable in the present study . typical us findings of soft tissue hemangiomas were observed in the patients included in this series using combined b - mode us and pdus [ 16 , 2527 ]  . 
b - mode us provided for evaluation of the site , size , margins and echostructure ( liquid or mixed ) of the lesion , and presence of plebolithes and any vascular structures . 
shape of the lesions was most commonly oval / fusiform , mean longitudinal diameter was 5cm , lesions were most commonly superficial , margins were most commonly not well - defined , and phleboliths were rare , most commonly in deep - seated lesions . 
echogenic pattern depends on the presence of fat , muscle and fibrous tissue ; presence of fat shows a hyperechogenic pattern , while presence of muscle and fibrous tissues shows a mixed hypo - iso echogenic pattern . 
hypoechogenic tubular or cystic / alveolar formations with good compressibility and light attenuation are common because of intralesional vascular formations [ 4 , 16 , 1820 , 26 , 28 , 29 ]  . 
heterogeneity shows a prevalent hyperechogenic pattern with a prominent fatty component , while when a mixed fatty , muscular and fibrous component is present the echo structure is not hyperechogenic but mixed ( hyper - hypo - iso ) echogenic [ 4 , 16 , 1820 , 26 , 28 , 29 ]  . 
in the present series , most soft tissue hemangiomas ( 69% ) were hyperechogenic with a heterogeneous echo structure secondary to the presence of fat ( most common ) , muscle , fibrous tissue , and tubular or cystic regular or irregular vascular formations . 
there was always some compressibility and most lesions showed increased color flow and a high flow pattern with an arterial and venous component flow signal , modified during both systole and diastole , in power and color doppler . 
us findings were suggestive of a soft tissue hemangioma but us - guided biopsy and histologic examination showed hemangioendothelioma increased flow signal during compression , tubular and cystic structures [ 4 , 2024 ]  . 
a high vessel density ( > 5 / cm2 ) and a high doppler shift ( > 2khz ) has been associated with a sensitivity of 84% and a specificity of 98% for the diagnosis of hemangiomas [ 20 ]  . 
most important , it is based on non - ionizing radiation , therefore , it can be repeated as many times as necessary , and can be used to guide biopsy [ 1620 ]  . 
 based on the results of the present series , the diagnostic accuracy of us for soft tissue hemangiomas is high ( 94.8% ) ; therefore , us diagnosis of soft tissue hemangiomas should be considered accurate without the need for biopsy and histologic analysis . 
additionally , us provides guidance for preoperative needle biopsy , perioperative guidance for lesion resection by localizing leading margin , and guidance for needle placement during minimally invasive treatments such as percutaneous sclerosis [ 31 ]  . 
it has been reported that us depiction of abundant low - flow vascular channels is a predictor for the potential success of percutaneous sclerosis [ 31 , 32 ]  . 
computed tomography ( ct ) angiography provides comprehensive 1 3 la radiologia medica ( 2018 ) 123 : 538544 information on long - standing lesions , lesions in adolescent and adult patients , and lesions involving osseous structures [ 31 ]  . 
the differential diagnosis should include venous malformations , arteriovenous malformations , lymphatic malformations , rapidly involuting congenital hemangioma , noninvoluting congenital hemangioma , capillary malformation , tufted angioma , kaposiform hemangioendothelioma , and fibrosarcoma [ 3439 ]  . 
 doppler us of malformations shows sponge - like anechoic vessels with arterial and / or venous wave form , or a poorly defined collection of cystic spaces with a high mean restrictive index . 
mr imaging may be considered as first line modality in superficial lesions with atypical clinical presentation , deep lesions difficult to evaluate with clinical examination , large lesions , complex combined vascular malformations , and to evaluate the deep extent in areas difficult to evaluate with us . continuous dull pain , large deep - seated lesions , increase in size during time , irregular infiltrating margins , highly heterogeneous echo structure , and irregular mixed tubular and alveolar vascular formations are clinical and us findings that should increase the awareness of the treating physician for another diagnosis than a hemangioma . 
 intralesionally , all lesions showed alveolar ( endometriosis ) or tubular ( fasciitis , hemangioendotelioma and endometriosis ) vascular structures of different caliber . in conclusion , clinical presentation and typical us findings are adequate for the diagnosis of soft tissue hemangiomas without the need for a biopsy and histologic analysis . 
in this study , we investigated the ability of dynamic susceptibility contrast ( dsc ) perfusion in differentiating necrotic changes from pathological angiogenesis and compared measurements of relative cerebral blood volume ( rcbv ) , relative cerebral blood flow ( rcbf ) and k2 , using a dedicated software . methods twenty - nine patients with secondary brain tumors were included in this retrospective study and underwent dsc perfusion mri with a 3 - month follow - up imaging after chemoor radiation - therapy . 
relative cbv using a cut - off value of 2.1 proved to be the most accurate and reliable parameter . keywords functional magnetic resonance imaging perfusion brain neoplasm metastases cerebral blood volume introduction brain metastases affect 2040% of patients with cancer and represent the second most common cerebral neoplasm , after meningiomas , in adults [ 1 ]  . 
stereotactic radiosurgery ( srs ) has become an increasing noninvasive treatment option for the original version of this article was revised : the name of the last author was incorrect . 
metastatic tumor recurrence and radiation necrosis have a similar appearance on conventional mri [ 4 ] and it is often difficult to distinguish which entity is responsible for a progressively enhancing lesion after chemo and / or radiation - therapy [ 5 , 6 ]  . 
in the presence of progressively enhancing lesions we are facing the decision whether to proceed to a salvage treatment or to wait and see , with conservative medical care [ 4 ]  . 
histology remains the reference standard to confirm or refute tumour recurrence but this vol . : ( 0123456789 ) 1 3 546 la radiologia medica ( 2018 ) 123 : 545552 requires ideally a resection of the lesion rather than biopsy because of spatial tumour heterogeneity . pseudoprogression represents an exaggerated response to an effective therapy [ 7 ] and can be misinterpreted as tumor progression on conventional mri . 
apparent tumor progression on mri may actually represent pseudoprogression in 64% of cases [ 8 ]  . at present , perfusion - weighted mr - imaging ( pwi ) using a dynamic susceptibility contrast ( dsc ) technique is one of the most clinically relevant physiological mri methods . 
pwi has also shown promising results for diagnosis of pseudoprogression , which is often not possible on conventional t2 - weighted and contrast - enhanced t1 - weighted mr sequences . the aim of this study is to assess how measurements of rcbv , rcbf and k2 ( a marker of vascular permeability ) derived from dsc perfusion mri can help distinguishing between recurrent neoplasm and treatment - related changes in patients with brain metastases . 
moreover , we set out to determine an optimum rcbv cut - off value for the differentiation between the two entities . materials andmethods patient sample from march 2013 to april 2016 , 29 patients ( mean age 53 , range 33 - 79years ; 11 males , 18 female ) with secondary brain tumors ( 13 breast , 12 lung , 2 bladder , 2 colon ) were retrospectively included in the study . 
image processing was performed with a dedicated software package ( olea sphere , olea medical , la ciotat , france )  . after radiotherapy , mri was obtained after 45days in all patients and at 3 - month interval follow - up thereafter in patients who survived . on conventional mri , diagnosis of recurrent disease was based on the presence of nodular highly vascularized areas within the contrast - enhanced lesion , irrespective of areas indicative of necrosis . 
on the other hand , diagnosis of stable disease was made in the absence of any highly vascularized areas and / or absence of lesion increment . on the basis of both clinical and radiological follow - up , diagnosis of pseudoprogression was made if an initial increase in contrast - enhancing lesion size was followed by stabilization or resolution on conventional mri follow - up in patients without progressive deterioration of neurological condition . reference standard a definitive diagnosis ( standard of reference ) of recurrent disease ( neoangiogenesis ) was made by pathological examination in 3 cases and clinico - radiological follow - up in the remaining patients . 
patients were retrospectively divided in the two groups based on the definitive diagnosis . 1 3 la radiologia medica ( 2018 ) 123 : 545552 cbv , cbf andk2 measurements the rcbv maps were generated using established tracer kinetic models applied to the first - pass data . 
the region - of - interest ( roi ) placed on the lesions included all enhancing tissue and excluded nonenhancing necrotic areas and the surrounding edema ; roi had a size of at least 20 pixels in all examined patients and was centred on the peak cbv values on the parametric map for each lesion to minimize confounding factors in rcbv analysis . 
our software automatically generated a corrected cbv map derived from k2 permeability map . statistical analysis the patients of our cohort were dichotomized in two groups : cases with recurrent disease ( n = 25 ) and cases with stable disease ( n = 53 )  . 
all cases in which diagnosis of pseudoprogression was made were included in stable disease group . comparison oftheparameters ofinterest betweendisease andnodisease descriptive statistics which included mean , standard deviation ( sd ) , minimum and maximum values for parameters of fig . 
1 dcs perfusion mri obtained in a 75 - year - old woman with cerebral metastasis from breast cancer with tumor recidive ( recurrent disease ) 6months after chemoand radiation - therapy . 
 the differences in values were statistically significant for rcbv and rcbf but not for k2 . the distribution of these three parameters for both patients with recurrent and stable disease is summarized in fig.2 ; box and whisker plot are also reported . 
however , difference in rcbv values between patients with pseudoprogression and stable disease was not significantly different . cutoff ofrcbv andcalculation ofsensitivity , specificity anddiagnostic accuracy sensitivity , specificity and diagnostic accuracy obtained using three different cut - off values for the rcbv are shown in table2 . 
2 the distribution of all values for the three parameters of interests ( rcbv , rcbf , k2 ) and for both patients with recurrent and stable disease are reported . 
physiological imaging techniques , such as t2 * - weighted dsc - pwi have substantially advanced the clinical use of mri for differentiating recurrent cerebral tumors from the radiation necrosis [ 15 ]  . 
 in the present study , first pass bolus tracking technique with t2 * - weighted images ( dsc ) was used as perfusion imaging technique , which is the fasted and presently the clinically most widely used perfusion techniques with mr . with a dedicated analysis software , we extracted the following perfusion parameters from dsc imaging : rcbv , rcbf and k2 [ 16 ]  . 
a number of studies have reported that the degree of capillary permeability varies markedly between recurrent intra - axial metastatic tumor and radiosurgery - induced necrosis [ 1722 ]  . 
dsc may also be helpful in the ongoing evaluation of patients with known brain tumors , as recurrent or residual tumor has been shown to have higher rcbv than pseudoprogression or radiation necrosis , both in the setting of gliomas and metastases [ 11 , 23 ]  . in the present study , we compared rcbv , rcbf and k2 in patients with recurrent disease and with stable disease ( cases of necrosis or pseudoprogression ) ; we found that mean values of the rcbv , rcbf and k2 were lower in patients with stable disease compared to patient with recurrent disease . 
 these results are in line with previous studies on cerebral metastases treatment - related changes , which have recommended a rcbv cut - off between 1.85 [ 24 ] and 2.6 , the latter consisting predominantly of lung and breast primary tumors [ 12 ]  . 
3 pseudoprogression in a 53 - year - old woman with occipital right lobe metastasis ( white arrow ) from lung cancer , 3 months ( a ) and 9 months ( b ) after radiation therapy . 
a on conventional mr sequences ( flair and t1 - post - contrast ) , ring enhancement with increment of lesion dimension was interpreted as tumor progression ( recurrent disease ) , while perfusion map recorded a rcbv value of 0.22. 
 the three continuous line shows the cut - off values chosen for rcbv ( red , blue and black for rcbv = 2.6 , rcbv = 2.1 , and rcbv = 1.6 , respectively ) la radiologia medica ( 2018 ) 123 : 545552 in the evaluation of 51 patients with cerebral metastases , rizzo etal . 
in comparison with the previous studies , the main result of the proposed study is that sensitivity , specificity and diagnostic accuracy of 100% could be archived with a rcbv cut - off value of 2.1. sensitivity and specificity values can vary according to chosen parameters due to the existence of a border area in which necrotic tissue and tumor recurrence coexist and that dsc - pwi can prevalently guide towards one type of pathogenesis , but not in absolute terms [ 25 ]  . previous studies indicate that the development of pseudoprogression seems to result in a better outcome and overall survival [ 26 ]  . 
pseudoprogression is likely to result from treatment - related cellular hypoxia , which induces expression of hypoxia - regulated molecules from tumor and surrounding cells , with a consequent increase in vascular permeability and enhancement [ 27 , 28 ]  . accurate selection of roi within the lesion are essential to calculate pwi parameters for differentiating recurrent metastatic tumor from dominating radiation effects ; in fact the areas of recurrent tumor may not always consist of the tumor cells but may coexist with necrosis and hypovascular areas caused by occlusive vasculopathy induced by radiation . our study had some limitations : first of all , we obtained a pathological diagnosis of cerebral metastasis in only three cases . 
histology obtained by biopsy or limited resection represents the current reference standard for confirmation of neoplastic disease , even if the most malignant portion of a tumor may not be included in the sample . 
moreover , the risk of possible complications of a biopsy may outweigh the benefits of a confirmative tissue diagnosis . further limitation of this study isa subject sample too small to draw any definite conclusions about its use for patient management . 
moreover , it is important to underline that a threshold cbv value of 2.1 cannot be applied universally , for it was derived from 1 3 la radiologia medica ( 2018 ) 123 : 545552 results from specific mr instrument and software in a singular institute . in conclusion , dsc perfusion imaging appears to be a highly useful advanced mrl method for the differentiation between tumor recurrence , tumor necrosis and pseudoprogression in patients with treated cerebral metastases . 
 relative cbv proved to be the most reliable parameter to determine the presence or absence of recurrent tumor , and a cut - off value of 2.1 yielded a high diagnostic accuracy in our cohort . 
we recommend that further prospective evaluation should be undertaken with a larger sample - size and imageguided histopathological sampling to confirm the efficacy of the technique described in this retrospective study . funding the authors declare that this study has not received any funding . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
however , because of the wide availability and high diagnostic performance of ct examinations , assessment of radiation dose to individual organs during diagnostic thoracic mdct has been primarily focused on the breast , lungs , and bone marrow because * shujie cheng shujiecheng@yeah.net 1 department ofradiology , the affiliated hospital ofhebei university , 212 yuhua road , lianchi district , baodingcity , hebeiprovince300072 , peoplesrepublicofchina of their relative high sensitivity to radiation compared with other organs in the thorax [ 35 ]  . 
thus , reducing the radiation dose in ctpa studies has become a priority for radiologists . several available techniques have been shown to reduce radiation dose during mdct imaging , including reduction in tube output , reduction in tube voltage , reduction in z - axis coverage , and variation in pitch [ 612 ]  . 
currently , the only available organ dose modulation ( odm ) technique is a new technique of radiation dose reduction that modulates tube current by reducing the tube current over a prescribed 120 radial arc over the anterior aspect of the body . 
the organ dose modulation technique aimed vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 676685 at reducing the absorbed breast dose during ctpa is the use of bismuth shields , which has shown maximal dose reduction to the breast [ 14 ]  . 
3d smart ma modulation for ct has been one of the most important technological developments in ct radiation dose reduction , and it yields excellent image quality while reducing the tube current [ 15 , 16 ]  . 
adaptive statistical iterative reconstruction ( asir - v ) is an effective and widely used algorithm for reducing noise and maintaining image quality [ 1719 ]  . to our knowledge , no previous study has compared the image quality and radiation dose of organ dose modulation and 3d smart ma modulation by using the asir - v algorithm in ctpa . 
the patient characteristics are shown in table1 . ct scan protocols all 300 patients underwent ctpa with the gemstone detector to derive 128 slices per rotation on a high - definition discovery ct750 hd ( hdct ; ge healthcare , wisconsin , usa )  . 
the scan parameters were as follows : helical , 0.5 - s tube rotation time , pitch factor of 0.984 : 1 , 50 - cm sfov , 78.75 - mm / s table speed , and 120 - kvp tube voltage . 
the scan parameters were as follows : helical , 0.5 - s tube rotation time , pitch factor of 0.984 : 1 , 50 - cm fov , 78.75 - mm / s table speed , and 120 - kvp tube voltage . 
the technique is intended to achieve the desired image quality as specified by the user in the form of a ni with a user - selected minimum and maximum ma range , which extended from 30 to 360ma , and ni value was 25 . 
for the 3d smart ma technique , tube current was modulated to achieve an image noise of 25hu in images of uniform object at image slice thickness of 5mm . all images were reconstructed with 50% asir - v [ 20 , 21 ] , which implied 50% filtered back projection blending with 50% asir in the reconstructed images . 
the scan area extended from 1cm below the clavicle to the diaphrag the axial length ranged from 295 to 335mall patients were trained how to breathe before the examination and were required to hold their breath during the examination . 
 therefore , we used a 45 - ml bolus of pure contrast medium , followed by 30ml of a mixed phase with 40% contrast medium and 60% nacl , and finally , a 50 - ml chaser bolus of pure nacl in all groups . 
the thickness of the reconstructed images was 0.625mm , at an interval of 0.6ma circular region of interest ( roi ) with an area of 10 1.0mm2 was placed at different spots to measure the mean ct values and image noise as shown in fig.1. 
 for all measurements , the size , shape , and position of the rois were kept constant among the image sets by applying a copy - and - paste function on the workstation . the cnr of all the images was calculated according to t he following for mula [ 21 , 22 ] : cnr = ( ct main pulmonary trunk cterector spinae muscle ) / sdchest wall fat , where ctmain pulmonary trunk denotes the mean ct value of the main pulmonary trunk , cterector spinae muscle denotes the mean ct value of the erector spinae muscle in the same slice , and sdchest wall fat denotes the mean noise generated by chest wall fat . 
the signal - to - noise ratio ( snr ) was calculated according to the following formula [ 22 , 23 ] : snr = ctmain pulmonary trunk / sdmain pulmonary trunk , where sdmain pulmonary trunk denotes the mean noise generated by the main pulmonary trunk . 
the cnr and snr measurements were taken from the images for the objective evaluation of image quality . all images were interpreted by two independent radiologists with at least 20years experience in ct pulmonary angiography . 
the two radiologists evaluated the overall diagnostic image quality on a diagnostic pacs workstation with the same brightness and resolution settings of the same viewing monitor over a period of 2weeks . 
the overall diagnostic image quality of ctpa was assessed using the following 5 - point scale , and the 5 - point rating scales for the images of ctpa are shown in table1 [ 12 , 24 , 25 ]  . 
all the images were randomized , and the readers were blinded to the scan modes ( i.e. , odm combined with asir - v scan mode and 3d smart ma scan mode )  . 
 the characteristics of the six patient subgroups ( age , height , and weight ) , image quality scores ( subjective image quality ) , ma values , ctdivol , dlp , and ed were compared using one - way analysis of variance ( anova )  . 
a , b give an example for image impression achieved with the odm with a 29.92 kg / m2 ( a ) , the 3d smart ma modulation with a 19.18 kg / m2 ( b ) section thickness is 0.625 mm for image a and b . 
signal intensity was measured with a roi tool as ct value of pulmonary trunk , main left and right pulmonary arteries , and image noise as standard deviation of pulmonary trunk , main left and right pulmonary arteries . 
there was a significant difference in signal intensity values between the two ct scan protocols ( p < 0.01 ) subjective evaluation ofimage quality intraobserver variability ( k ) was 0.81 ( 95% ci 0.531.00 ) for observer 1 and 0.76 ( 95% ci 0.390.88 ) for observer 2 ; these results indicated a good agreement . 
the study performed with the odm demonstrated segmental pe in the right and left pulmonary artery and different segment of right lung and left lung with ct value from 409 to 419 hu ( white arrow )  . 
in this study , we evaluated and compared the radiation dose and image quality between organ dose modulation and 3d smart ma modulation at different bmis , as well as organ dose modulation combining asir - v . 
organ dose modulation is a new technique for msct scanning that reduces the tube current over a predefined region of the body and is of specific interest in ctpa imaging to reduce absorbed breast dose . 
this technique decreases the tube current of the scan over an anterior 120 arc of the patient while it relatively increases the tube current over the remaining 240 to prevent the deterioration of image quality at the center . 
 in ctpa imaging , this technique aims to take into account the anatomical location of breast tissue to reduce the tube current in a predefined angle volume of the anterior rotation . 
it is a reconstruction technique that enables reduction in image noise ( standard deviation ) , streak artifact at low signal condition and improvement in low - contrast detectability , while preserving the structure details in the image , it contains more advanced noise modeling and object modeling , and also added some physics modeling , which offers further promise toward the aim of acquiring low - dose ct exams at lower radiation dose to patients , while preserving or even enhancing diagnostic value . 
in the higher bmi group ( 29.9kg / m2 bmi 34.9kg / m2 ) , the average radiation dose with organ dose modulation technique was reduced by 38.22% compared to that of 3d smart ma technique for ctpa , but the image quality had no statistically significant difference . 
the results indicate that using organ dose modulation in patients with higher bmis can reduce more radiation dose than patients with small bmis , that is why the organ dose modulation technique can reduce more ma value in patients with higher bmis than small bmis . prior studies have shown that a maximum 47% decrease in thoracic organ dose using organ dose modulation compared with tube current modulation for thorax ct scan [ 30 , 31 ]  . 
however , the results of this study show that organ dose modulation combined with the asir - v technique reduces the radiation dose by an average of 35.91% , compared to 3d smart ma modulation for ctpa in different bmi group ( 18.5kg / m2 bmi < 34.9kg / m 2 ) , the difference was that prior studies focused on the differences in imaging quality and radiation dose in thorax ct scan by organ dose modulation and auto ma modulation . 
this study focused on comparing the image quality and radiation dose of organ dose modulation and 3d smart ma modulation by using the asir - v in ctpa , the goal of 3d smart ma is to make reconstructed images contain x - ray quantum noise at a same level desired by the user , and independent of patient size and / or anatomy . 
4 graph showing the comparisons of signal - to - noise ratio ( snr ) , contrast - to - noise ratio ( cnr ) , and ct dose index of volume ( ctdivol ) between odm and 3d smart ma modulation in different body mass index ( bmi ) values . 
no statistical differences in snr and cnr between the odm with asir - v and the 3d smart ma modulation in 18.5 kg / m2 bmi 34.9 kg / m2 ( p > 0.05 ) , but there was a significant difference noted in the ctdivol value between the odm and 3d smart ma modulation . 
that because organ dose modulation provides a mode to reduce x - ray tube current ( ma ) in anterior direction of the patient where the most radiation - sensitive organs ( breast tissue ) are located while maintaining overall diagnostic image quality by modulating x - ray tube current according to the x - ray tube angle . 
that why odm can modulate tube current along the z - axis , also modulates the x - ray beam in the xand y - plane output for a constant 120 of the gantry rotation , and centrally located organs have a constant radiation exposure while superficially located organ ( breast tissue ) experience reduced exposure within the prescribed 120 radial arc . 
we also found that the mean ct values of the pulmonary arteries , erector spinae muscle , and chest wall fat were affected by the measurement area size and location of the measurement area , especially in the erector spinae muscle and chest wall fat . 
first , the patients in all of the groups were not scanned consecutively ; nevertheless , there were no significant differences in patient characteristics 1 3 684 la radiologia medica ( 2018 ) 123 : 676685 ( age , height , and weight ) among the groups . 
however , our ct scanner was not equipped with the veo . in conclusion , this study set out to determine that the radiation dose was significantly lower for odm combined with the asir - v technique than for 3d smart ma modulation . 
the aims of this study were to explore the association of the od and ssc - ild on chest high - resolution computed tomography ( hrct ) , and to establish a cutoff point for the od suggestive for the presence of a significant lung involvement . methods the widest oesophageal diameter ( wod ) was obtained on axial hrct images . 
 although the pathologic mechanisms underlying ild are not yet fully elucidated , there is evidence that oesophageal motility disturbances and gastro - oesophageal reflux ( ger ) are implicated in ild development in several lung conditions , including ssc . 
it is assumed that both abnormalities of oesophageal peristalsis and decreased low oesophageal sphincter pressure may lead to repeated microaspirations of gastric acid content into the respiratory tract , with consequent and progressive airway damage [ 810 ]  . od detected on chest hrct is frequently associated with an extensive ild , as well as with low pulmonary performance [ 4 , 5 ]  . 
the coexistence of ild and ger disease ( gerd ) in patients with connective tissue diseases ( ctds ) [ 6 ] and the evidence that ctd patients with ild have a higher incidence of pathologic reflux reinforce the assumption that gerd may play a role in the natural history of lung disease in subjects with ctd [ 9 ]  . several studies have reported the prevalence of od on chest hrct in ssc , using empirical cutoff values to define od without regard to normal standards [ 3 , 4 , 1113 ]  . the purposes of this study were to confirm the association of od and ild on chest hrct in patients with ssc , and to identify the oesophageal diameter cutoff value with the best association ( higher sensitivity and specificity ) with ssc - ild . materials andmethods study population from january 2016 to december 2017 , consecutive ssc patients , defined by the american college of rheumatology classification criteria [ 14 ] , were included from the rheumatological clinic and the medical clinic of the universit politecnica delle marche . 
 the modified rodnan skin score ( mrss ) ( score 051 , where lower values represent a better condition ) was employed to assess skin damage [ 16 ]  . the presence of autoantibodies , including anti - topoisomerase i and anti - centromere , was also assessed . the exclusion criteria were represented by : current or recent ( within 3months ) respiratory infection , severe pulmonary hypertension requiring specific treatment , uncontrolled congestive heart failure , and clinically significant abnormalities other than ild identified on chest hrct . 
echocardiography and right heart catheterization were examinations not included in the evaluation for this study . patientcentred measures the patient - centred measures were collected to evaluate dyspnoea , physical function , and ger symptoms , respectively , employing the borg dyspnea index ( borg score ) [ 17 , 18 ] , the health assessment questionnaire - disability index ( haq - di ) [ 19 , 20 ] , andthe gerdq questionnaire [ 21 ]  . the borg score assesses the perceived dyspnoea ( breathing discomfort ) with a numerical scale from 0 to 10 ( 0 = no breathlessness at all , 0.5 = very very slight ( just noticeable ) , 1 = very slight , 2 = slight breathlessness , 3 = moderate , 4 = somewhat severe , 5 = severe breathlessness , 7 = very severe breathlessness , 9 = very , very severe ( almost maximum ) and 10 = maximum ) [ 22 ]  . the haq - di is a tool to measure the functional status ( evaluating activities of daily living ) , and is calculated as an ordinal variable ( from 0 = no disability , to 3 = severe disability )  . the intended use of haq - di is for arthritis [ 19 ] ; however , it was shown to correlate with visceral and cutaneous involvement in ssc and to detect deterioration of function in these patients [ 20 , 23 ]  . the gerdq questionnaire is a simple six - item self - administered tool [ 24 ]  . 
four items assess the symptoms and situations considered as positive predictors for gerd diagnosis : heartburn , regurgitations , disorders related to sleep , and use of over - the - counter products . 
the other two questions evaluate symptoms considered negative predictors for reflux , such as nausea and epigastric pathe patient answers each question about symptom frequency during the last week using a likert - like scale from 0 to 3 for positive features , and from 3 to 0 for negative attributes [ 21 ]  . 
gerdq cutoff 9 gave the best balance with regard to sensitivity [ 66% ; 95% confidence interval ( ci ) : 5874 ] and specificity ( 64% ; 95% ci 4183 ) for gerd . pulmonary function tests ( pfts ) pfts were carried out within 2weeks from the chest hrct assessment , with a spirometry using a computerized lung analyser ( masterscreen diffusion , jaeger gmbh , hchber , germany )  . 
forced vital capacity ( fvc ) , first second forced expiratory volume ( fev1 ) , and the single breath carbon monoxide diffusing capacity of the lung ( dlco ) were recorded . 
at least three measurements were taken for each variable to guarantee repeatability . parenchymal abnormalities onhrct all hrct examinations were performed according to a standard protocol , using a ct 64ge light speed vct power scanner with a rotation tube scanning time of 0.65s. 
scans 1 3 la radiologia medica ( 2018 ) 123 : 655663 were acquired in full inspiration from the apex to the lung base in supine position , at 120kv and 300mas , and slice thickness and spacing of scans of 1.25 and 7mm , respectively . 
for a detailed description of the warrick scoring , the reader can refer to the original article [ 25 ]  . oesophageal diameter measurement inhrct in this study , the widest oesophageal diameter ( wod ) was used as a measure of od . 
the oesophageal axial diameter in hrct was measured by osirix md 7 ( fig.2 ) , a dicom viewer software ( osirix md version 7 , 64 - bit format ) on a mac mini ( 2.8ghz intel core 2 duo desktop computer , 16gb random - access memory ; apple computer , cupertino , ca , usa ) running mac operating system macos high sierra , version 10.13.2. interobserver agreement for the oesophageal axial diameter measurement in hrct was tested in 20 examinations . 
 [ 5 ] , the three oesophageal diameter measurements were performed : above the aortic arch ( a ) , between the right inferior pulmonary vein and the aortic arch ( b ) , and between the diaphragmatic hiatus and the right inferior pulmonary vein ( c )  . 
baseline study cohort characteristics are shown intable1 . the results of the analyses of the relationships among wod , patient - centred measures , warrick score , and pfts results are shown in fig.3. 
covariates considered in the model included : age , gender , disease duration , anti - topoisomerase antibodies , mrss , borg score , gerdq , haq - di , fvc , and dlco . 
a warrick score of 7 was employed as cutoff point to consider the presence of a significant ssc - ild [ 27 ]  . results overall , 126 ssc patients were included in the study . 
moreover , there is a clinically significant association between od and hrct findings of ild : oesophageal diameter positively correlates with patient - centred measures of dyspnoea , gastro - oesophageal symptoms and functional disability , and is negatively correlated with dlco . 
furthermore , od is more prevalent in subjects with longer disease duration and is significantly more correlated with the presence of anti - topoisomerase i serum autoantibodies . additionally , to the best of our knowledge , it is the first research that defines a cutoff point for od associated with ssc - ild using roc curve analysis . the mechanisms underlying ssc - ild are not yet completely known . 
some evidences suggest that both cell - mediated and humoral immunity play a role in the pathogenesis of ild [ 2832 ]  . oesophageal motor alterations have also been considered as contributing factors of ssc - ild [ 810 ]  . 
the changes in oesophageal peristalsis and decreased low oesophageal sphincter tone may induce a predisposition to ger [ 810 , 33 ]  . many investigators have described how ger can be one of the initiating factors of a variety of respiratory disorders ( e.g. , asthma , bronchiectasis , and recurrent acute pneumonia ) [ 3437 ]  . 
concluded that there was no association between od and ild , it is possible that the size of the cohort or the cutoff point of 9mm may account for the lack of association . 
interestingly , the authors noted a statistically significant reduction in dlco and a non - significant trend towards reduction in total lung capacity in those patients with oesophageal diameters > 9mthis finding may suggest that dlco is a more sensitive marker of lung injury related to silent aspiration as has been shown in other forms of lung injury . in 2012 , patiwetwitoon et al . 
 the circle on the curve shows the optimal cutoff point , corresponding with the maximum sum of sensitivity and specificity out that ger therapy could potentially improve symptoms and pft parameters in these patients [ 34 , 37 , 38 ]  . several studies have reported the prevalence of od on chest ct scans in ssc patients . 
revealed that in ssc patients , the presence of hypomotility or aperistalsis detected on oesophageal manometry is associated with lower lung volumes and reduced dlco values [ 33 ]  . 
 revealed that an augmented oesophageal diameter on hrct in ssc patients is associated with more severe ild , lower lung volumes , and worse co diffusion [ 5 ]  . although our study does not demonstrate a causal relationship between oesophageal diameter and ssc - ild , our findings are consistent with the results of previous studies corroborating the hypothesis that ger and microaspiration may be involved in the ssc - ild pathogenesis . three potential limitations to our study have to be mentioned . 
firstly , there were some intrinsic issues : the nature of this study was cross - sectional , and the information on risk factors for ssc - ild progression was not available to our cohort . 
thirdly , we had no control group or patients with other causes of oesophageal dysfunction to compare with ssc patients . in conclusion , our findings confirm that patients with ssc - ild had more dilated oesophagus on chest hrct compared with patients with ssc and no significant lung disease . 
future longitudinal studies to determine whether a dilated oesophagus is a risk factor for ild progression should be designed to include careful assessment of the ssc 1 3 662 la radiologia medica ( 2018 ) 123 : 655663 subset , quantitative changes on hrct scan of the lungs [ 18 ] , and objective reference criteria for gerd diagnosis . compliance with ethical standards conflict of interests the authors declare that they have not conflict of interests . ethical approval all applicable international , national , and institutional guidelines for the care and use of animals were followed . 
to categorize the angiogenesis around the fracture site , the microvascular blood flow from ceus was classified into four categories , depending on the portion of the investigated area that was involved in the neovascularization process : grade 0 = 0% ; grade 1 = 030% ; grade 2 = 3070% ; grade 3 = 70100% . 
vascularity significantly increased over time ( p < 0.001 ) , namely : 1 ( 25th75th percentile = 12 ) at 7days ; 2 ( 12 ) at 4weeks ; 3 ( 02 ) at 8weeks . 
 all patients but one showed early progressive increase in neovascularization well identified with ceus at the fracture site . conclusion ceus is a feasible method to monitor healing in patients with long bone nonunion . keywords ultrasound contrast - enhanced ultrasound long bone nonunion mesenchymal stem cells platelet - rich plasma * domenico albano albanodomenico@me.com 1 department ofimaging , azienda ospedaliera universitaria citt della salute e della scienza , cto hospital , via zuretti 29 , 10126turin , italy 2 department ofimaging , ospedale humanitas gradenigo , c.so regina margherita 8 , 10153turin , italy 3 department ofradiology , di.bi.med. , university ofpalermo , via del vespro 127 , 90127palermo , italy institute ofmolecular genetics , national research council ofitaly , via ferrata , 27100pavia , italy 5 department oforthopedics andtraumatology , santandrea hospital , c.so abbiate 21 , 13100vercelli , italy 6 unit ofdiagnostic andinterventional radiology , irccs istituto ortopedico galeazzi , via r . 
 several factors are involved in the development of nu , such as infection , mechanical stability , growth factors , local environment , and the quality of the underlying bone matrix . 
 however , previous studies underlined the central role of vascularity in the healing process [ 2 ] ; hypoxia at the site of fracture seems to be one of the main predisposing factors for nu [ 3 ]  . the treatment of long bone nu is still a major issue , with different operative and non - operative available treatments . 
indeed , radiographs and computed tomography are used to diagnose fractures [ 5 ] and monitor bone healing [ 6 ] , but their main limitation is the low sensitivity for the healing process during the early phases [ 6 ]  . 
as the role of angiogenesis in bone fracture healing is crucial , ultrasound ( us ) with color and power doppler , and contrast - enhanced ultrasound ( ceus ) might be helpful to determine the vascularity of bone callus in the first few weeks of healing providing useful information , besides avoiding radiation exposure . 
 to the best of our knowledge , a single paper [ 8 ] used ceus in the preoperative analysis of infected nu , but nothing is published about longitudinal evaluation of these patients . the aim of our study was to assess the technical feasibility of ceus in the monitoring of non - infected long bone nu healing . materials andmethods study population ceus is a standard procedure at our institution ; thus , no institutional review board approval was needed for the present study , but approval was obtained for retrospective publication of data and patients informed consent was waived . patients aged 18years and over , with clinical and radiological diagnosis of a non - infected long bone nu at least 9months after a fracture , who underwent surgery and intraoperative administration of mesenchymal stem cells ( msc ) and platelet - rich plasma ( prp ) were included in the present study . 
the treatment of infected nu included deep - tissue sampling for both microscopic and histological examination , taking care to avoid contact of the clean instruments with the skin in order to prevent contamination . 
after initial baseline us examination , 2.4ml of us contrast agent consisting of sulfur hexafluoride microbubbles ( sonovue , bracco , italy ) was administered as a bolus in a peripheral vein , followed by a 5 - ml saline flush . 
at the end of the injection , a timer was started and evaluation of contrast agent was carried on up to 3mthe presence of hyperechoic spots within the bone callus allowed verifying the contrast medium arrival at the site of fracture . 
all disagreements were resolved in consensus . to categorize the angiogenesis process around the fracture site , the assessment of microvascular blood flow from ceus imaging was classified into four categories . 
the observers visually assigned values ranging from 0 to 3 depending on the portion of the investigated area that was involved in the vascularization process : grade 0 = 0% ; grade 1 = 030% ; grade 2 = 3070% ; and grade 3 = 70100% , respectively . 
the latter was obtained with external fixation ( 17 / 25 ) , internal fixation ( 7 / 25 ) , or both external and internal fixation ( 1 / 25 )  . the angel bone marrow kit system is used intraoperatively at the point of care for the safe and rapid preparation of concentrate bone marrow ( cbm ) from a small sample of autologous bone marrow ( abm )  . 
in brief , 60cc of anticoagulated bm ( 12cc anticoagulant citrate dextrose 1 3 la radiologia medica ( 2018 ) 123 : 703709 solution + 48cc bm ) is harvested from the anterior iliac crest using a five - hole needle provided with the kit that withdraws in different directions to reduce the risk of bm dilution with whole blood . 
the bm is then introduced in the system , and the automated process of preparation is started . the first component to be collected is platelet - poor plasma ( ppp )  . 
angel system adjusts the valve position to collect prp , white blood cells and cell precursors like mscs until red blood cells are detected by the absorption of the 940nm wavelength of light . 
around 2cc of cbm is dispensed into the collection syringe , and the volume is adjusted to 5cc with ppp simply pulling back the plunger of the syringe without opening the closed circuit . 
the product contains eightfold concentrated precursor cells ( msc , hematopoietic cell phosphatase , endothelial precursor cell ) , platelets , and white blood cells that can be directly injected in the nu site to stimulate the local environment and induce tissue regeneration . it is known that increased vascularity positively influences nu healing [ 8 ]  . 
 conversely , in patients where no vascularization was seen at ceus before treatment , mscs and prp were administered with an osteoinductive scaffold composed by mineralized bone matrix ( chips , fibers , and powder )  . 
at these time points , the operator assessed both the vascularization of the callus and also the potential presence of complications . all patients also underwent routine radiographic evaluation at 3 and 6months after the procedure . statistical analysis the nonparametric friedman test was used to compare neovascularization at four time points when ceus evaluation table 1 data of 25 patients with long bone nonunion repaired using autologous mesenchymal stem cells and platelet - rich plasma no . 
sex age bone additional findings type of fixation baseline 7days 4weeks 8weeks hematoma hematoma hematoma fluid collection hematoma fluid collection tibia femur tibia femur tibia tibia tibia tibia tibia femur tibia tibia femur femur tibia tibia tibia tibia tibia 1 m 47 3 m 25 4 m 52 7 m 53 9 m 59 13 m 54 14 m 51 15 m 32 17 m 33 18 m 45 19 m 44 20 m 20 humerus 21 m 21 22 m 31 24 m 50 25 m 52 tibia tibia tibia femur tibia internal external external internal external external external external external internal external external external internal external internal external external internal internal external external external external + internal 1 external 1 3 706 la radiologia medica ( 2018 ) 123 : 703709 was performed : surgery , 1 , 4 , and 8weeks after surgery . 
at subsequent time points , vascularity significantly increased over time ( p < 0.001 ) , namely at 7days it was 1 ; 12 ; at 4weeks it was 2 ; 12 ; and at 8weeks it was 3 ; 02 . at evaluation performed at 7days after the procedure , in 4 / 25 ( 16% ) patients a small subcutaneous hematoma was detected , defined as an ovoid hypoechoic area around the site of administration , which spontaneously resolved at subsequent evaluations . 
in 2 / 25 ( 8% ) patients , a fluid anechoic collection around the callus was detected , still visible at 4 and 8 - week follow - up . 
in one of these cases , vascularization did not change between 7 - day and 8 - week follow - up . at 6 - month evaluation , standard radiographs showed complete fracture healing in all patients and complete bone consolidation . figures1 , 2 , and 3 show a representative case of our study population . discussion our main finding is that ceus is feasible in the evaluation of bone callus after autologous mscs and prp implantation . 
 in all cases but one , ceus was able to demonstrate progressive increase in vascularization of the bone callus . the treatment of long bone nu is still challenging in clinical practice . 
over the last years , focus of clinicians and researchers has been placed on the role of mscs in regenerative medicine as a potential source for the regeneration of bone [ 4 ]  . 
the arrow indicates the area imaged using contrast - enhanced ultrasound in fig.2 even prp autologous nature guarantees the lack of significant side effects [ 12 , 13 ] , thus allowing for deliver insitu bioactive molecules [ 14 ]  . 
in previous works performed on patients with tendinopathy , prp has demonstrated to determine an early increase in the vascularization at the site of injection [ 15 , 16 ] , probably induced by the vascular endothelial growth factor present in prp [ 17 ]  . fracture healing is a complex process that requires some steps and implicates several factors . 
it is the result of interactions between the osteogenic cells , the osteoinductive stimulants , and the osteoconductive scaffolds , to obtain a condition of mechanical stability [ 2 ]  . 
in this setting , angiogenesis at the site of bone fracture is crucial to promote the regenerative process , especially allowing the endochondral ossification through the transformation of avascular cartilaginous tissue in vascular osseous tissue [ 2 ]  . 
in the early phase of bone healing , plain films and computed tomography are useful to assess the alignment of bone fragments but definitely do not enable to monitor the neovascularization of bone callus . 
a baseline evaluation : no contrast uptake is seen in the area surrounding the fracture ( arrows ) ; t = tibia ; double - headed arrow = bony breach . 
b seven - day evaluation : in the area of treatment ( arrows ) , a small amount of peripheral contrast uptake is seen ( asterisks ) ; however , the central part is still avascular ( circles )  . 
c four - week evaluation : contrast uptake is seen in most of the treated area ( arrows , asterisks ) , and a central robust vessel is seen ( arrowheads )  . 
d eight - week evaluation : the whole treated area is homogeneously vascular ( arrows ) advantage from the intrinsic property of us contrast agents to remain within the vessels , thereby providing useful information regarding small microvascular structures [ 19 , 20 ]  . 
however , their results are scarcely comparable with ours , as we only included aseptic nu only and we did not perform any quantitative evaluation . in our series , all patients but one showed a significant increase in neovascularization at the site of bone fracture at the various time points well identified with ceus . 
however , it is worth saying that this reduced vascularization did not affect the radiographic healing of the fracture , thus making the correlation between vascularization and healing somewhat uncertain . in our study , we performed the ceus examinations with these precise time points to better follow the bone healing process . 
the baseline ceus was performed before treatment to demonstrate the absent or poor vascularization at the site of bone fracture to choose the treatment option : in patients with no pre - treatment vascularization , an osteoinductive scaffold composed by mineralized bone matrix was added to the standard treatment . 
at 7days from surgery , ceus allowed the identification of the beginning of reparative neoangiogenesis during the inflammatory phase characterized by the release of growth factors mainly by the mscs and prp and the formation of hematoma rapidly replaced by granulation tissue [ 22 ]  . 
for more difficult locations , one good method to improve anatomic correlation might be the use of fusion imaging , using preoperative computed tomography or magnetic resonance images [ 29 ]  . 
last , all patients included in our series had a good outcome at 3 and 6 - month follow - up and all but one showed progressively increasing neovascularization over time . 
thus , the real predictive role and diagnostic performance of ceus in these patients cannot be evaluated , as also patients with bad results should have been included . in conclusion , ceus is fully feasible to monitor patients with long bone nu repaired using autologous mscs and prp implantation . 
future larger studies should be performed to better understand the predictive role of ceus in this setting . acknowledgements at the moment the work was conducted , domenico aloj was affiliated with the department of orthopedics and traumatology , i clinic , azienda ospedaliera universitaria citt della salute e della scienza , cto hospital , via zuretti 29 , 10126 turin , italy . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
the fracture is almost consolidated ( arrow ) during the reparative phase , after 4weeks , during which the formation of soft callus with woven bone is promoted by osteoblasts and macrophages from the blood supply , and at 8weeks , during which the woven bone is replaced by lamellar bone [ 22 ]  . 
after that , during the remodeling phase , the calcification of bone callus makes difficult the evaluation of the site of fracture with the ceus , but the callus becomes sufficiently dense to be assessed through radiography and computed tomography [ 7 ]  . 
however , the role of ceus in the correct therapeutic planning of these patients should be further addressed in future prospective trials . the reliability of us in the diagnosis of bone fractures [ 2426 ] , especially in pediatric patients [ 27 ] , and in the evaluation of bone healing [ 28 ] is well known . 
the most common cause of as in adults is the calcification of trileaflet or congenital bicuspid valve apparatus . in patients with as , the precise determination of disease severity is of utmost importance for its management and therapeutic decision - making [ 25 ]  . 
given that as should be intended as a disease continuum and no single vol . : ( 0123456789 ) 1 3 644 la radiologia medica ( 2018 ) 123 : 643654 parameter alone should define severity , grading of as is usually performed on the basis of a spectrum of non - invasive hemodynamic measurements , i.e. , peak aortic jet velocity , mean pressure gradient , and aortic valve area ( ava )  . 
current acc / aha [ 5 ] and esc [ 4 ] guidelines recommend eoa < 1.0 cm2 and mpg > 40mmhg as the main criteria to define severe as . 
although the invasive quantification of as severity by catheter - based hemodynamic techniques has been proposed as the gold standard for the grading of as severity , it is rarely performed today because it is time - consuming , costly , and entailing substantial risk . 
in addition , it is well known that the use of the gorlin equation to estimate the ava is associated with several sources of error , as being directly influenced by cardiac output , blood viscosity , and flow turbulence [ 6 ]  . 
further , the original purpose of the gorlin equation was to give an estimate of the anatomical ava , but what our eyes see is not necessarily what our heart feels , and eoa by continuity equation better represents the hemodynamic burden caused by the stenosis . 
in daily clinical practice , transthoracic echocardiography ( tte ) is the recommended imaging modality for the initial assessment of suspected aortic valve disease and for the evaluation of eoa and ava ( class i , level of evidence : b ) [ 4 , 5 , 7 ]  . assessment of anatomical ava by direct planimetry ( avapl ) of the valve orifice is often necessary in questionable casesimportantly when assessment of eoa is unreliable due to poor transthoracic acoustic windows and / or suboptimal doppler angle alignment with flow direction and this is usually done by transesophageal echocardiography ( tee ) , ormore recentlyby cardiac magnetic resonance ( cmr )  . 
mr planimetry does not rely on blood flow velocity quantification , pressure gradients or geometrical assumptions , thus , cmr may provide valuable information , especially in patients with reduced cardiac output or other table 1 demographic , anatomic and hemodynamic data of the study population conditions affecting measured parameters [ 8 ]  . 
cmr may also be used to assess the functional degree of as severity , by using velocity - dependent analyses based on the continuity equation [ 9 ]  . to date , only few studies have been performed to evaluate the accuracy of cmr for planimetric and continuity equation measurements of ava in comparison with tte and tee . 
therefore , in the present two - center study we performed a direct comparison between planimetric and continuity equation measurements of ava as assessed by cmr , tte and tee , in a series of patients undergoing valve surgery , and examined inter - modalities diagnostic agreement and precision . methods patient population this is a retrospective observational study with a two - site chieti , italy and bristol , ukenrollment of 31 consecutive patients ( 21 men , 10 women , mean age 69 10years , 20 in chieti , 11 in bristol ) with symptomatic moderate - to - severe aortic valve stenosis first assessed by tte , and scheduled for elective aortic valve replacement . 
pts patients , lvef left ventricular ejection fraction , tte transthoracic echocardiography , cmr cardiac magnetic resonance , tee transesophageal echocardiography , ava aortic valve area , eoa effective orifice area according to established and standardized protocols by qualified observers aware of patients medical history , suspected underlying disease and major comorbidities , but who were blinded to the results of other examinations . 
imaging and acquisition protocols were in agreement with recommendations from the society for cardiovascular magnetic resonance board of trustees task force on standardized protocols [ 10 ] and with the american society of echocardiography recommendations for quality echocardiography laboratory operations [ 11 ]  . 
patients informed consent for the performance of the here - reported diagnostic examinations was obtained from all individual participants included in the study . transthoracic doppler echocardiography ( tte ) tte was performed using conventional ultrasound systems ( philips sonos 5500 and philips ie33 x5 - 1 , philips healthcare , best , the netherlands ) attached to 15mhz transducers . 
details of the methods here used are provided in the online supplemental material . transesophageal echocardiography ( tee ) 2d - tee was performed using conventional ultrasound systems ( philips sonos 5500 and philips ie33 x7 - 2t ) attached to 27mhz transducers . 
after the tee probe was positioned in the esophagus at the level of the aortic valve , the transducer was rotated from 0 to 3045 to obtain a short - axis cross - sectional view of the aortic valve . 
after selecting one frame , in which the maximum aortic valve opening was observed , with fine adjustments of the cutting plane to delineate the smallest aortic valve orifice , the inner borders of the valve leaflets were traced manually using a magnified view to measure the ava . 
final measurements were averaged in at least 3 cardiac cycles . 1 3 646 cmr imaging cmr imaging was performed on 1.5 tesla mr scanners ( achieva ; philips medical system , best , the netherlands , for the chieti patients ; and avanto , siemens , enlargen , germany , for the bristol patients ) , each using a dedicated 8 - element phased - array cardiac synergy coil for signal reception . 
after localization of the heart using three - plane and oblique survey images , cine - imaging was performed with a balanced steady - state free - precession ( bssfp ) technique at 30 phases per cardiac cycle ( by vectorcardiographic gating ) in 814 parallel short axis , and two chamber and four chamber ( 8mm thickness , 0mm gap )  . 
 a three - chamber view ( for the lvot ) and an oblique coronal view cine - image ( for the aortic outflow tract of the left ventricle ) were also acquired . 
mr ( vti and v ) data acquired at this level are most strongly correlated with the ultrasound measures ( vti and v ) in the lvot and at the aortic valve [ 12 , 13 ]  . 
for each patient , peak aortic jet velocity measured by tte was used to define cmr encoding velocity ( cmr velocity encoding ( venc ) = ( 1.251.5 ) peak jet velocity ) to optimally define resolution . 
importantly , our phase mapping protocol included preliminary in - plane phase - contrast ( pc ) analysis aimed at imaging transaortic flow direction and to assist in planning the appropriate location of subsequent perpendicular through - plane slabs [ 14 ]  . 
as the first venc range is subjectively set depending on the expected velocity of the jet and in order to speed up the scouting process , we ran flow mapping by selecting the venc range based on transvalvular aortic peak velocity as measured by cw doppler on tte . 
 for this purpose , regions of interest ( rois ) were drawn on each of the 24 phases of magnitude images to include the lumen of the lvot ( 10mm below the aortic valve annulus ) and of the aorta ( 10mm above the annulus ) , and peak velocities were computed ( v )  . 
oblique coronal ( a ) and three - chamber long - axis view ( b ) of the aortic outflow tract with slice position for planimetry indicated by white lines parallel to the aortic annulus . 
 cross - sectional bssfp image ( c ) shows a stenotic tricuspid valve 1 3 la radiologia medica ( 2018 ) 123 : 643654 10mm below the aortic valve annulus , manually delineating the inner borders of the lvot lumen . 
in addition , for each modality , the valve morphology was defined by two reviewers , in consensus , as bicuspid or tricuspid . method pl - cmr ce - cmr statistical analysis normal distribution was described as mean , standard deviation ( sd ) or 95% confidence interval ( ci )  . 
the pearson correlation coefficient measures how far each observation deviates from the best - fit line and is a measure of precision ; bias correction factor measures how far the best - fit line deviates from the 45 line through the origin and is a measure of accuracy . 
linear regression ( c ) and blandaltman analysis ( d ) illustrating the agreement between ava assessed by planimetric measurements after exclusion of patients with extensive thickening and heavy calcification of all cusps . 
also , we here demonstrate the increased agreement of cmr - derived planimetry after excluding patients with thickened and moderately / heavy calcified valves , which is one limitation to bear in mind when performing cmr analyses . 
in such cases , the continuity equation - derived evaluation appears to be the strategy of choice for cmr in grading the severity of isolated as . echocardiographic assessment ofasseverity byuse ofthesimplified continuity equation orplanimetry the 2d transesophageal planimetric method is known to be more accurate than the similar 2d transthoracic method . 
it indeed requires a precise positioning of the transducer to obtain the correct crosssectional view at the level of the edges of the aortic cusps at their maximum opening , which can be quite challenging due to the aortic root anterior and superior movement during the cardiac cycle . 
based on this principle , to calculate the eoa one needs to perform 3 measurements : the vti of the lv outflow tract using pw doppler , the vti through the aortic valve using cw doppler , and the cross - sectional area of the lvot , which is calculated from the measured lvot diameter by assuming a circular shape . 
calculation 1 3 650 la radiologia medica ( 2018 ) 123 : 643654 of the eoa by using the simplified continuity equation has some disadvantages , as it may not be feasible in a significant proportion of patients due to poor acoustic window and / or subvalvular flow acceleration . 
moreover , given that the calculation of ava requires the inclusion of 3 measurements ( the lvot diameter , the lvot peak velocity and the aortic peak velocity ) in the simplified continuity equation , this method may involve relatively large measurement errors . 
 the precise estimation of lvot diameter is the most critical parameter for an accurate estimation of the eoa and is difficult in patients with poor acoustic windows or severe calcifications of the aortic valve and of the outflow tract . 
 in addition , measurement of the peak flow velocity in the lvot may be distorted in patients with high or low left cardiac output or associated valvular insufficiency , because it is susceptible to changes in flow dynamics . 
this highlights the important need for additional noninvasive and accurate methods for the fine assessment of stenosis severity in the presence of possible discordances between tte - eoa measurements , transvalvular gradients , dimensionless velocity ratio , and eventually clinical findings . assessment ofasseverity bycmr because of the aforementioned limitations of echocardiography , several investigators have recently proposed to grade the severity of as by using cmr . 
indeed , with the introduction of ssfp , cmr allows high - quality cine - short - axis images of the aortic valve , and therefore to obtain accurate direct planimetry of its maximum opening area . several recent studies have compared the measurements of ava obtained by this planimetric approach with those obtained by tee . 
potential limitations of cmr planimetry are difficulties in the precise visualization of the aortic cusps due to partial volume effects , the presence of calcifications , or flow - related artefacts . 
ssfp sequences are generally preferred because of their superior signal - to - noise ratio , clear - cut blood - tissue contrast , and high spatial and temporal resolutions , making the accurate identification of the fast - moving valve cusps easier [ 24 ]  . 
 [ 25 ] have demonstrated that also cmr planimetry of aortic bioprosthetic orifice area correlates highly with data obtained by tte ( r = 0.82 ) and tee planimetry ( r = 0.92 ) despite artefacts caused by the presence of surgical foreign bodies , such as sternal wires and the struts of stented prostheses . as shown in table4 , the agreement between cmr and tee to assess native aortic valves in our study ( ccc = 0.85 ) is as high as those reported by debl etal . 
this result highlights a potential limitation of the cmr planimetric techniques , as diffuse valvular calcifications may hamper the correct delineation of the leaflets and the estimation of the valve area . besides the direct planimetry of the aortic valve opening , cmr also allows the eoa calculation by use of the continuity equation . 
as with doppler echocardiography , this requires the obtainment of 2 different sets of data , i.e. , supra and subvalvular flow velocity data , which can be obtained by the use of velocity - encoded phase - contrast images , and anatomical information on the dimensions of the lvot , which requires multislice cine - imaging . multidetector computed tomography is a powerful imaging modality to measure dimensions , surfaces and volumes of cardiac chambers . 
 [ 27 ] , we measured the lvot area on the through - plane phase - contrast images acquired at 10mm below the aortic valve annulus , manually delineating the inner borders of the lvot lumen and not the lvot diameter . 
thanks to this method , we show that the lvot cross - section is typically elliptical and not circular ; as a consequence , tte underestimates the lvot area calculated assuming a circular geometry . 
indeed , given there is a small but actual augment in cancer risk from exposure to ionizing radiation in children , it is important to understand what the risk of alternative techniques could be . 
the main concerns can be summarized in : ( 1 ) biological effects of non - ionizing electromagnetic fields ( emf ) employedwhose mechanisms of interaction with human tissues are polarization , induced current , and thermal heating , respectively . 
 ( 5 ) risks related to gadolinium - based contrast agents , especially considering the newly reported brain deposition . keywords mr safety paediatric population introduction current radiological literature is strongly focussed on radiation imaging risks [ 1 ] ; it may be worthwhile to assess the safety of alternative imaging modalities used in the paediatric population . 
since it is a small but actual augment in cancer risk from exposure to ionizing radiation in children , it is important to understand what the risks of alternative techniques could be . methods therefore , the aim of this article was to make a risk / benefit analysis of avoiding the use of x - rays in favour of other imaging modalities , focusing our attention on mr imaging ( mri )  . 
search results for ( ( gadolinium [ mesh terms ] or gadolinium [ all fields ] ) and deposition [ all fields ] and ( brain [ mesh terms ] or brain [ all fields ] ) ) were 142 papers . lastly , searching for ( magnetic resonance imaging [ mesh ] and safety [ mesh ] and sedation ) we obtained 22 papers . 
fda has approved exposure of adults to 7t fields and exposure of neonates to 4t fields . usually , institutional review boards ( irbs ) define mri as a minimal risk technique so it is approved for numerous research protocols , including in children [ 3 ]  . 
anyway , the genetic damage should be reversible : after 48h , the mn number returned to that of the controls , suggesting that two cell divisions are enough to eliminate thein conclusion , the authors suggested prudent use to avoid superfluous examinations , according to the precautionary principle . 
simi [ 8 ] reported a dose - dependent ( 1.5t scanner , with a maximum gradients strength of 50mtm1 , and a maximum gradients speed of 150mtm1s1 ) increase of mn frequency invitro that returned to control values after 24h when the exposure was within diagnostic levels . 
besides , in everyday life , we are subjected to a series of environmental insults that cannot be genotoxic in themselves , but may increase the negative effects of other biological , chemical and / or physical agents [ 8 ]  . 
in a study by magin [ 14 ] on ( sub ) chronicle exposures , no statistically significant changes were observed in foetal growth in animals ( mice ) exposed to only mr or ultrasound fields . 
luckily , analysis of cognitive and biometric data from a decade - long longitudinal fmr study of normal language development in a small , longitudinal sample of healthy children who received up to 10 mr scans provided evidence of minimal ( if any ) risk [ 3 ]  . 
 demonstrated the effect on human lymphocyte activation cytokine release by smf in 0.5t mr [ 15 , 16 ]  . the most common / known biological problem during mr is that of heating , due to rf fields [ 17 ]  . 
the rf power absorbed per unit of mass of an object is defined specific absorption rate ( sar ) and is measured in watts per kilogram ( wkg1 )  . 
many technical issues cause an increase of examination time , such as smaller coils to maximize local signal ( enclosing a larger portion of the body , and augmenting rf heating in turn ) , 1 3 la radiologia medica ( 2018 ) 123 : 695702 respiratory triggering and cardiac gating , and controlled ventilation [ 20 ]  . during sedation / anaesthesia , which limits intrinsic thermoregulation , body temperature is the result of a sum of factors : the cool environment , hypothermia because of passive heat loss ( large surface area - to - body weight ratio ) , heating due to rf fields [ 21 ]  . 
conversely , a case of iatrogenic hyperthermia occurring in a 16 - month - old infant during anaesthesia for cardiac mr ( fentanyl , rocuronium , sevoflurane ) was reported [ 23 ]  . 
other series of infants propofolsedated do not confirm hypothermia , reporting a prevalence of heating : probably , the depth of sedation may influence the degree of thermoregulatory impairment [ 24 ]  . 
this could augment the chance of hearing loss and could have an adverse effect on neurosensory and physiologic short - term and long - term natural growth and development of the neonate [ 26 ]  . 
another source of acoustic noise is the so - called rf hearing ( click , buzz , chirp , or knocking noise ) [ 25 ]  . time - varying magnetic fields also induce electric fields in patients , stimulating nerves or muscles . 
safety standards avoid cardiac stimulation [ 28 ]  . risks fromferromagnetic external objects andimplanted devices the risk of ferromagnetic projectiles unintentionally carried inside the scanning room of an mr setting is greater in children ( especially in the newborns and infants ) than in adults . 
as synthesized by arthur [ 17 ] : proper requirements must be accessible when sick young children are in the mr environment : mr - compatible fibre - optic temperature monitoring , pulse oximeter , ecg leads . 
as well as longer - term central venous catheters , implanted programmable cerebrospinal fluid ( csf ) shunts ( to be resected after imaging ) , implanted cardiac devices and cochlear implants are typical of paediatric patients . 
the fdas centre for devices and radiological health ( cdrh ) proposes terms to be used to label mr information for medical devices [ 29 ] : mr safe : an item that poses no known hazards in all mr environments ; fig . 
1 ct angiography sagittal reconstruction of a 1 - year - old female with congenital heart disease with berlin heart , a paediatric mechanical ventricular assist device ( arrow ) ; in these cases , magnetic resonance ( mr ) imaging is contraindicated 1 3 698 la radiologia medica ( 2018 ) 123 : 695702 mr conditional : an item that has been demonstrated to pose no known hazards in a specified mr environment with specified conditions of use ; mr unsafe : an item that is known to pose hazards in all mr environments . owing to the complexity of the conditions faced and the heterogeneity of the implanted devices , in our hospital we identified a flow chart that has the justification of the examination as starting point and subsequently advises that the physician retrieves the information on the device from the manufacturer , identifying the degree of mr safety . 
 the increasing amount of data on all specific devices will ultimately allow to build a database , enabling real - time decisions . risks associated withsedation andanaesthesia the most common cause of artefacts on mr images is patient motion . 
in mr performed in paediatric patients , spatial resolution is crucial , but unfortunately there is an inverse relationship between spatial resolution and signal - to - noise ratio ( snr ) , which is proportional to the square root of the acquisition time [ 30 ]  . nice guidelines suggest [ 31 ] : for children and young people [ ] during diagnostic imaging consider either chloral hydrate for children under 15kg , or midazolaif these are not suitable , consider one of the following drugs ministered by a specialist healthcare professional with a narrow margin of safety : propofol , sevoflurane . 
 in children with congenital cardiac diseases , the frequency of adverse events was estimated to be between 0 and 10.4% [ 33 ] and direct patient observation is prevented by physical separation . 
according to edwards [ 32 ] , feed and wrap is ideal for children younger than 1year , oral or intravenous sedation between 1 and 5years , and distraction therapies for > 6year olds . 
there is a need to balance the choice between the risk of failing the exam , the use of alternative techniques such as ct ( considering any diagnostic limits ) , and performing anaesthesia directly ( if the organization allows it ) [ 35 ]  . in any case , intensive use of techniques to reduce artefacts , such as respiratory gating ( or triggering ) , respiratory compensation ( or phase re - ordering ) , navigator echoes , ecg gating , contributing to long acquisition times , is required in children . risks associated withgadoliniumbased contrast agents ( gbca ) gbcas can increase the accuracy of mr examinations , but many risks associated with the administration of exogenous contrast media must be taken into account [ 36 ]  . 
macrocyclic agents have a complete ring encasing the ion of gd in a structure which tends to hold it more firmly , thus being more resistant to its release [ 37 ]  . 
in healthy individuals , the half - life of gbcas is usually 1.5h , while in severely impaired renal function patients the half - life is increased up to approximately 30h [ 39 ]  . 
seventeen of these children had documented exposure to gbcas [ 40 ]  . the association of brain mr abnormalities ( abnormal t1 shortening in deep brain areas ) with a history of linear gbca administration was firstly reported by kanda [ 41 ]  . 
the studies have been focused in three directions : ( 1 ) detection of increased t1 - weighted signal intensity ( si ) or r1 relaxation rate in deep grey matter structures ; ( 2 ) direct detection of gd and measurement of gd concentration in human tissues ( brain , other organs ) [ 45 ] [ 5457 ] ; ( 3 ) animal studies ( detection and measurement of gd levels , imaging investigations , gd deposit speciation ) [ 5860 ]  . 
0.18% for iodinated contrast agents [ 5 , 6466 ]  . conclusions the main role of imaging is to help patients by influencing clinical management , simultaneously reducing imagingrelated risks without negative consequences on efficacy as much as possible . 
in detail , it can create a variety of tissues contrasts that can even be coregistered , increasing lesion conspicuity [ 30 , 67 ]  . unfortunately , mr is also somewhat operator dependent in its execution and , to be effective , time consuming . 
 conversely , ct is faster , cheaper , and much easier to perforas arthurs stated [ 5 ] : a well - performed ct will yield better diagnostic information than a poorly performed mr . 
syndrome associated with paediatric tumours , such as beckwithwiedemann syndrome and , even more , dna repair diseases ( fanconi anaemia , ataxiatelangectasia , etc . ) , which are characterized by immunodeficiency and / or predisposition to cancer development , need a screening by imaging [ 6870 ]  . 
despite the presumed genotoxicity , mr is considered the technique of choice in this case : many cancer - prone diseases have been shown to be radiosensitive due to pitfalls in the mechanisms of repair of induced dna lesions . up to date there is not yet an adequate consensus about the mr - related cancer risks and the world health organization affirmed that the carcinogenicity of static magnetic fields to humans is not at present classifiable . 
the limits of wb - mr are poor sensitivity ( motion artefacts , partial volume planes ) and poor specificity ( pitfalls due to growth variants ) [ 73 ]  . 
2 a , b pre - contrast t1 - weighted images of a 13 - year - old girl affected by suprasellar germinoma treated with chemotherapy and radio - therapy . 
a clear dentate nucleus hyperintensity ( arrows ) is visible after 6th from previous mr ( b ) ; only a macrocyclic gbca was used after repeated gbca administration have been found . 
for all these reasons , emas committee for medical products for human use ( chmp ) has recently published several precautions and recommendation on the use of gbcas for mr [ 61 ]  . esur contrast medium safety committee recommends avoiding unnecessary exposure of children to gbcas , especially in neonates and infants . 
contrast agents with highest risk of nsf ( linear ) are contraindicated in neonates and should be used with caution in children aged less than 1year [ 62 ]  . 
however , bedoya [ 63 ] investigated the effect of intravenous contrast material ( linear ) on renal function in a large population of neonates and concluded that , in the absence of known renal failure , neonates receiving standard patient care do not appear to be at increased risk for developing renal toxicity due to the administration of intravenous iodineor gadolinium - based contrast media . 1 3 700 la radiologia medica ( 2018 ) 123 : 695702 besides , technological advancements in ct ( reduced radiation doses in sub - second scan times ) improve the potentials of ct and we should re - evaluate its use in at - risk paediatric patients . 
a typical example is cardiac ct [ 33 ]  . in summary , particularly in young children , the choice between ct and mr should be decided on a case - by - case basis , considering efficacy first and avoiding radio - phobic attitudes . 
of course , the costs , the urgency , and the availability of machines also play a primary role . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants performed by any of the authors . 
particular attention has been given to detection of early symptoms [ 1 ]  . nevertheless , a large number of patients with sudden cardiac death or non - fatal myocardial infarction did not experience prior symptoms of chest pain or exertional dyspnoea . 
 this emphasizes the importance of early detection and * ernesto di cesare ernesto.dicesare@cc.univaq.it 1 dipartimento di scienze cliniche applicate e biotecnologiche , universit degli studi di laquila , via vetoio 1 , 67100laquila , italy treatment of underlying subclinical coronary atherosclerosis [ 2 ]  . at present time , traditional risk factors are used for the cardiovascular management of asymptomatic subjects . 
 patients without symptoms or signs of coronary artery disease ( cad ) , but with familial hypercholesterolemia ( fh ) , severe hypertension , smoking habits , and obesity are considered at risk . 
the identification and quantification of coronary artery calcium ( cac ) , a marker of subclinical atherosclerosis , may provide adjunctive prognostic information in the assessment of conventional risk factors [ 5 ]  . 
 however , cac does not represent the whole spectrum of vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 686694 atherosclerosis and has limitation to diagnose obstructive cad . coronary computed tomography angiography ( ccta ) has instead the ability to provide information regarding localization , extent and tissue component of atherosclerotic plaques . 
none of the other non - invasive techniques has shown similar capability to evaluate coronary lumen patency and to identify thickening of the wall [ 9 , 10 ]  . however , screening of asymptomatic patients with intermediate - to - high risk of cad by ccta is currently under debate and , according to the current guidelines [ 68 , 11 , 12 ] , considered as an uncertain but potentially useful clinical application . in this retrospective study , the prevalence of subclinical coronary atherosclerosis was evaluated and the composition of the plaque was studied in a group of asymptomatic patients who underwent ccta . the purpose was to assess the prevalence of coronary artery disease , as detected by cta , in asymptomatic patients with an intermediate risk of cad . the appropriate institutional review board committees approved the study protocol . methods andmaterials study population from january 2015 to august 2016 , we retrospectively enrolled 621 patients . 
from a total population of 621 patients , we excluded : poor ct image quality due to motion artefacts ( n = 3 ) , chest pain or discomfort before cardiac ct ( n = 30 ) , known coronary artery disease including artery bypass graft surgery and stent ( n = 353 ) , previous mi ( n = 34 ) , previous stroke ( n = 2 ) , previous transient ischemic attack or peripheral artery disease ( n = 11 ) , age under 35 ( n = 1 ) , high risk according to the frc ( n = 2 )  . 
 as a result , we analyzed 185 cardiac ct of asymptomatic intermediate risk subjects . in the presence of motion artefacts or inappropriate contrast delivery , resulting in non - diagnostic image quality of > 1 coronary artery or important proximal segments , the entire scan was considered non - diagnostic . the patients examined in our institution included : fiftynine patients after uncertain stress test , 10 after positive stress test , 11 after submaximal stress test and the remaining for preoperative cardiac clearance . 
the risk factors were calculated according to frc [ 3 ] and the patients were divided into three categories of risk for adverse coronary events : low ( risk < 10% at 10years ) = 08 points ; intermediate ( risk between 1020% at 10years ) = 915 points ; high ( risk > 20% at 10years ) 16 points . 
we excluded lowand high - risk patients . acquisition techniques image acquisition was made using a 640 - slice ct ( toshiba aquilion one 320 - row detectors ) that acquires a volume up to 16cm allowing the study of the entire heart in a single heartbeat , with a significant radiation dose reduction . 
the acquisition of images in the ct scan was synchronized to the heartbeat and performed with sequential scan and prospective ecg - gating . one hour before imaging , patients blood pressure and heart rate were recorded . 
to avoid movement artefacts on the images and acquire the entire heart in a single heartbeat , an heart rate < 65bpm , spontaneous or pharmacologically induced using - blockers , was necessary . 
 the acquisition was obtained in two heartbeats when it was impossible to reduce the cardiac heart rate below 65b / m just before the acquisition , 5mg of sublingual nitro - glycerine ( isosorbide , carvasin , wyeth lederle ) was administered in all patients . fifty millilitres of non - ionic contrast material ( iomeron 400 , bracco diagnostic , milan , italy ) was injected into the antecubital vein at 5ml / s , followed by 40ml of saline solution at the same flow rate , using a dual power injector ( stellant , medrad , indianola , pa , usa )  . the right time to start acquisition was determined using bolus tracking ( sure start ) in the descending aorta with a scan threshold of 300 hu . 
by means of this 1 3 688 la radiologia medica ( 2018 ) 123 : 686694 system , a tube power ranging from 50 to 500ma was established , based on the data received from the scanograa medium fov was selected to allow correct visualization of all cardiac structures in each patient . 
we employed iterative reconstruction : the aidr - 3d which operates in both the row data and the image doma the target noise value expressed as standard deviation was 33 . 
for each patient , the phase with the least artefacts was automatically determined by the systewe chose the one with the least movements ( phasexact , toshiba medical system , tochigi , japan )  . 
the radiation dose absorbed by the patient was evaluated . image analysis all scans were carefully analyzed for the presence of atherosclerotic plaques . subjective evaluation of the images was carried out by two cardiac radiologists with at least 15 ( edc ) and 5 ( lp ) years of experience , respectively . 
issues such as motion and poor gating were not taken into account in the subjective assessment , as they could not be ascribed to the reconstruction algorithm . the images were evaluated with multiplanar reconstruction technique ( mpr ) , maximum intensity projection ( mip ) and volume rendering ( vr ) through the study of a coronary segment . 
the intermediate artery , when present , was designated as segment 16 [ 13 ]  . image quality was assessed and classified as good ( no artefacts ) , adequate ( presence of image - degrading artefacts but feasible for evaluation with a moderate confidence ) , or poor ( presence of image - degrading artefacts and feasible for evaluation only with a low confidence )  . plaques were defined as structures > 1mm2 within and / or adjacent to the vessel lumen , which could be clearly distinguished from the lumen and surrounding pericardial tissue . 
 the possible presence of plaques , the number of affected vessels and the degree of stenosis that they determine were described . the presence of myocardial bridging and coronary abnormalities was also reported . we used commonly applied methods to measure extent of cad . 
the severity of stenosis was assessed by the percentage of luminal narrowing and classified , according to the 2012 aha guidelines for stable ischemic heart disease , as mild ( < 50% ) , moderate ( 5070% ) , and severe ( > 70% ) [ 14 ]  . patients were also classified according to the number of coronary arteries with obstructive cad as 3 - vessel or left main obstructive cad , 2 - vessel obstructive cad , single vessel obstructive cad , non - obstructive cad or absence of cad . patient followup the primary endpoint was major adverse cardiovascular events ( mace ) , defined as the combination of death , nonfatal myocardial infarction , unstable angina requiring hospital stay , and vessel revascularization . 
the diagnosis of myocardial infarction was based on the presence of new q waves in at least 2 contiguous leads or an elevation of creatine kinase or its mb isoenzyme . 
revascularization was performed in the presence of stenosis of at least 70% of diameter with a positive stress test or an ffr < 0.80. the second endpoint was subsequent imaging diagnostic test ( i.e. , myocardial perfusion scintigraphy or coronary angiography [ cag ] )  . the third endpoint was evaluation of changes after modification of patient management ( i.e. , lifestyle modification , changes in pharmacological therapy )  . follow - up data were obtained by a review of medical records or telephone interviews using trained personnel blinded to coronary ccta results . 
data are expressed in numerical value and in brackets , in % characteristics in positive cases for atherosclerotic plaques total ( n = 112 ) mild stenosis moderate stenosis severe stenosis indeterminate stenosis number of affected vessels 1vessel 2vessels 3vessels 4vessels diameter of stenosis on the main plaque 49% 5069% > 70% blooming effect ( poorly quantifiable ) features of the main plaque calcified mixed non calcific 56 ( 30.2% ) 49 ( 26.5% ) 3 ( 1.6% ) 4 ( 2.2% ) 50 ( 44.6% ) 33 ( 29.5% ) 22 ( 19.6% ) 5 ( 4.5% ) 56 ( 30.3% ) 49 ( 26.5% ) 3 ( 1.6% ) 4 ( 2.2% ) 55 ( 49.1% ) 21 ( 18.8% ) 36 ( 32.1% ) positive in 10 ( 5.4% ) , and negative in 30 ( 16.2% ) and 11 ( 5.9% ) did not carry out stress tests at all . 
the ccta documented the presence of moderate stenosis in 4 out of the 30 st negative patients , while out of the 59 patients with uncertain st , 14 showed moderate stenosis . the correlation between st and cta results is described in table3 . 
most cardiac events ( 87% ) ( i.e. , revascularization procedures ) occurred , on the basis of ccta results , within 120days of cta . 1 3 la radiologia medica ( 2018 ) 123 : 686694 fig . 
heavy calcification of the left descending coronary artery makes not quantifiable the degree of the stenosis for blooming effect in both proximal and distal coronary artery table 3 correlation between st and cta results uncertain st ( n = 59 53.6% ) positive stb ( n = 10 9.1% ) negative st ( n = 30 27.3% ) submax sta ( n = 11 10% ) results of cta coronary stenosis absent or < 50% 44 ( 40% ) 2 ( 1.8% ) undeterminate 13 ( 11.8% ) coronary stenosis 50% 1 ( 0.9% ) 9 ( 8.2% ) 26 ( 23.6% ) 4 ( 3.6% ) 3 ( 2.7% ) 1 ( 0.9% ) 6 ( 5.5% ) values are expressed as n ( % ) data are expressed in numerical value and , in brackets , in % st stress test a st inconclusive ( e.g. , inability to achieve adequate maximal heart rate in response to exercise , st depression < 1 mm ; left ventricular hypertrophy with repolarization abnormalities ; rapid resolution < 1 min - of ecg changes ; appearance of angina typical during exercise in a patient at high risk , but no modification of the ecg ; pressure response inadequatee.g. , increase in systolic blood pressure < 25 mm hg - in the absence of valve disease or heart failure , etc . ) [ 11 ] b st depression 1mm the remaining 12 patients with moderate cad on ccta underwent therapy changes : 4 introduced statins and 8 introduced antiplatelet agent . in those patients with mild stenosis ( 563.2% ) at ccta , only 2 patients ( 1.1% ) underwent revascularization procedures ( 2 pci ) within 120days , due to ffr < 0.80. 
the remaining 54 subjects ( 29.1% ) underwent additional diagnostic testing on the basis of cta results within 120days of cta : myocardial perfusion scintigraphy in 35 patients ( 18.9% ) ; 19 ( 10.2% ) underwent adenosine stress cardiac magnetic resonance . 
as a result , all patients 1 3 692 la radiologia medica ( 2018 ) 123 : 686694 were submitted to therapy changes : antiplatelet agent or statin in all patients , and none of these treatments were discontinued . at the spearmans rank correlation , older age ( rho coefficient = 0.43 ; p = 0.034 ) and cad ( rho coefficient = 0.26 ; p = 0.023 ) found by means of cta were associated with a greater risk of adverse events . 
all these patients benefit from medical treatment and coronary risk control management to reduce progression of total atherosclerotic plaque burden . the current knowledge regarding the prevalence of occult cad in asymptomatic patients is limited . 
the confirm study highlights a discrepancy between the clinical assessment of cad and the presence and extent of cad demonstrated by ccta , which is potentially particularly pronounced in individuals without traditional modifiable risk factors . 
they also demonstrated an incremental value of coronary cta for predicting ( mace ) [ 15 , 16 ]  . up to now , one of the methods used routinely to diagnose the presence of stable coronary artery disease are the stress tests [ 4 , 17 , 18 ]  . 
the ccta documented the presence of moderate stenosis in 4 out of the 30 st negative patients , while out of the 59 patients with uncertain st , 14 showed moderate stenosis . 
in addition , in our series ccta identified a good percentage of non - calcified plaques providing useful data in the identification of unstable coronary lesions that are prone to rupture and may cause acute coronary events . 
 ccta is a non - invasive imaging method able to quantify the degree of stenosis and to detect the plaque components ; the only potential risks are represented by the possibility of adverse events related to the use of iodinated contrast agents . 
in fact , although coronary angiography represents the gold standard in clinical diagnosis of cad cannot be used as a screening test in asymptomatic patients because of its invasiveness and related risks . in this study , atherosclerotic plaques were identified in many of the asymptomatic individuals . 
nevertheless , with respect to the published guidelines [ 68 ] , it seems today inadequate to suggest ccta as screening tool in the asymptomatic patients . in our experience , we found significant differences when the patients were stratified by cholesterol , hypertension and smoking habits . 
we observed that cad was much more frequent in patients with elevated values of systolic blood pressure than in those with normal values and in smokers with respect to non - smoker patients and in the patients with higher level of total cholesterol if compared to those with normal values ( pr > f 0 , 001 , 0 , 004 and 0 , 003 )  . 
these data confirm the high correlation with hypertension , cholesterol high levels and smoking in the genesis of the atheroma [ 19 ] , the need of adequate therapy and the dangerous effect of smoking as principal aspects in the primary prevention . it is also interesting to underline that , in more than 50% of individuals with coronary stenosis , the plaques were located in the left anterior descending coronary artery . 
the current evidence supporting the use of various tests for the detection of cad is based on meta - analyses and multicentre studies [ 9 ]  . multi - detector computed tomography ( mdct ) can detect coronary atherosclerosis and stenosis and is reliable for ruling out significant cad in patients with low - to - intermediate probability of cad . 
ischemia imaging has been regarded as the most appropriate in symptomatic patients with intermediate pre - test probability ( 1585% ) of significant cad , while in asymptomatic patients or in those with low or high pre - test probability , the tests are generally not recommended . invasive coronary angiography has been regarded as the reference standard for detection and assessment of cad severity , but , as an invasive procedure , it is associated with specific procedure - related adverse events . 
when non - invasive stress imaging is contraindicated , non - diagnostic , or unavailable , the measurement of fractional flow reserve ( ffr ) or coronary flow reserve is helpful during diagnostic coronary angiography . 
in fact , our study demonstrates that 1 3 la radiologia medica ( 2018 ) 123 : 686694 significant stenosis was found among the stratified patients according to frs [ 3 ]  . in the current study , we are in line with previous experiences although they support the possibility to introduce ccta also in asymptomatic patients . 
we strongly believe , however , that ccta must be narrowed down to specific populations to avoid unnecessary examinations . impact ofcta onadditional tests andrisk ofradiation exposure although the current guidelines [ 710 ] do not recommend the use of multidetector ct as a screening procedure in asymptomatic patients , this technique is expanding more and more in this field increasing its use in the clinical practice . the food and drug administration agency announced that there is a small chance ( 1 in 2000 ) to develop a cancer following ct studies that give a radiation dose of 10msv [ 21 ]  . 
based on the recent study beir - vii ( biological effects of ionizing radiation ) , the first generation of 64 - row detector ct is associated with a high risk of cancer , especially in women and in younger patients [ 22 , 23 ]  . 
in this study , ccta was performed with the use of a wide detector ct able to acquire the entire heart volume in a single heartbeat with a heart rate < 65b / min and in two heart beats when the heart rate was 6575b / min particular , in 39% of the studied patients we were unable to reach an heart rate below 65b / min also after - blockers administration and the acquisition was obtained in two heartbeats . 
such findings suggest that that risks related to the x - ray exposure are really limited . on the other hand , previous multicentre studies carried out with 64 - slice ct units demonstrated sensitivities of 9599% and specificities of 6483% as well as negative predictive values of 9799% for the identification of individuals with at least one coronary artery stenosis by ica [ 2628 ]  . meta - analyses of smaller trials confirm high sensitivity ( 9899% ) and negative predictive value ( 99100% ) , paired with lower specificity ( 8289% ) and positive predictive value ( 9193% ) [ 26 ]  . in a multicentre study , which included patients with previously known cad , pci and mi , diagnostic accuracy was lower ( sensitivity 85% and specificity 90% )  . 
severe coronary calcium negatively impacts the accuracy of coronary cta [ 2931 ]  . study limitations costs represent one of the main limitations to the use of cta as a screening tool in the routine clinical practice . nevertheless , the major limitation is that there are still insufficient data concerning the follow - up of patients and the clinical course post - ccta . 
for all these reasons , additional studies are needed to confirm the results obtained . in conclusion , the prevalence of cad in asymptomatic patients was not negligible ; nevertheless , the medium - term prognosis still needs to be confirmed . a significant number of individuals with occult cad may be misclassified by the traditional methods of risk and diagnostic stratification commonly used in clinical practice . 
 ccta has the ability to correctly identify these patients , even though the relationship between risks and benefits and the cost problem remain to be assessed . it seems reasonable now that also asymptomatic patients be evaluated with ccta . 
hemoptysis is their principal complication and is a potentially fatal condition . purpose to illustrate the causes , multidetector ct angiography ( mdcta ) findings and differential diagnosis of acquired ppaa . materials and methods the institutional review boards approved this study . 
we conducted a retrospective review of the demographic data and the results of clinical and laboratory examinations , and imaging studies of patients managed between january 2012 and january 2017 in two institutions . results a total of 19 patients had acquired ppaa that were detected at mdcta , 9 patients with normal pulmonary artery pressures and 10 with pulmonary hypertension . 
further clarification of the natural history of these rare arterial aneurysms is needed . keywords aneurysm pulmonary artery blood vessels multidetector computed tomography endocarditis hemoptysis * tullio valente tullio.valente@gmail.com 1 department ofdiagnostic imaging , section ofgeneral radiology , azienda ospedali dei colli , p.o. 
a true aneurysm is a focal dilatation of a blood vessel bound by all three layers of the vessel wall , whereas pseudoaneurysms or false aneurysms are the result of a breach in the vessel wall contained by the adventitia or surrounding perivascular soft tissue [ 24 ]  . 
fusiform aneurysms consist vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 664675 table 1 anatomical classification and distribution of pulmonary artery aneurysms table 2 etiological classification of pulmonary artery aneurysms central ( main trunk and major branches ) versus peripheral ( or parencongenital ( > 50% usually central and fusiform ) heart defects persistent ductus arteriosus ventricular septal defects atrial septal defects hypoplastic aortic valve bicuspid aortic valve pulmonary valve stenosis pulmonary regurgitation absent pulmonary valve connective tissue abnormalities prenatal varicella ehlersdanlos syndrome marfan syndrome ( usually true ) cystic medial necrosis ( usually true ) acquired ( < 50% ) infectious ( usually false ) syphilis tuberculosis pyogenic bacteria ( often in drug abusers ) septic embolisms ( often in endocarditis ) bacterial and fungal pneumonia lung abscess and bronchiectasis vasculitis ( usually true ) behet syndrome hughesstovin syndrome takayasu arteritis pulmonary arterial hypertension ( usually true ) chronic pulmonary embolism connective tissue diseases neoplasm primary lung cancer primary right atrial cancer pulmonary metastasis iatrogenic ( usually false and saccular ) cardiac surgery catheters chest tubes angiography surgical resection biopsy trauma pregnancy idiopathic ( usually true ) chymal ) true versus false fusiform versus saccular solitary versus multiple of diffuse circumferential dilation of a long segment of the vessel . 
 the normal pulmonary circulation is a low - pressure system that has approximately one - tenth the flow resistance of the systemic circulation as well as a high capacitance [ 5 , 6 ]  . 
 most of the pulmonary aneurysms are located in a major pulmonary artery such as the pulmonary trunk ( defined as a diameter of over 4cm ) and major branches ( defined as central or proximal aneurysms ) [ 5 , 7 ] , whereas only a small percentage ( about 2030% ) is localized in the peripheral pulmonary divisions usually lobar , segmental and subsegmental branches ( defined as peripheral or intraparenchymal aneurysms or ppaa ) [ 710 ] ( table1 )  . 
of the few reported ppaa cases in the literature , more than 50% are described as being associated with congenital heart disease including patent ductus arteriosus , ventricular septal defect or bicuspid aortic valve [ 1 , 5 , 710 ]  . 
in the other half of cases , acquired pathologies are found to be the underlying etiology [ 1 , 4 , 5 , 810 ]  . ppaa may occur when any two of the following three conditions exist : ( 1 ) infection , ( 2 ) pulmonary hypertension and ( 3 ) a congenital or acquired defect of the vascular wall [ 1315 ]  . 
greene and baldwin have defined four pathological criteria for an idiopathic paa : simple dilatation of the pulmonary trunk with or without involvement of the remainder of the arterial tree , the absence of intracardiac or extracardiac shunts , the absence of chronic cardiac or pulmonary disease and the absence of arterial disease such as syphilis or more than minimal atheromatosis or arteriosclerosis of the pulmonary vascular tree [ 18 ]  . 
acquired pathologies include pulmonary arterial hypertension ( defined as an increase in mean pulmonary arterial pressure ( pap ) to 25mmhg at rest as assessed by right heart catheterization ) [ 19 ] , vasculitis ( i.e. , behets disease ) [ 20 ] , infection , neoplasm , connective tissue disease ( i.e. , marfan syndrome , scleroderma ) or trauma ( including iatrogenic injuries ) [ 1 , 5 , 810 , 13 , 2124 ] ( table2 )  . 
other risk factors and causes for developing paa include degenerative changes of the elastic media , long - term steroid use and age older than 60years [ 7 , 9 , 13 , 25 ]  . 
in general , the clinical manifestations of ppaa often remain inconsistent and nonspecific , whereas most patients have no complaints and many cases with ppaa may be present but undiagnosed ; clinical symptoms include dyspnea , chest pain , hoarseness , palpitation and syncope [ 1 , 710 ]  . 
e mip oblique sagittal reformatted image shows a simple type of left lower lobe pulmonary arteriovenous malformations ( pavm ) consisting of direct connection between a feeding pulmonary artery and a draining vein through an aneurysm ( right to left shunt ) ( arrow )  . 
hemoptysis due to pulmonary arterial origin is quite rare ( estimated to occur in less than 10% of cases ) and requires specific diagnostic and therapeutic approach [ 28 ]  . 
recently , reports and identification of these clinical entities have increased owing to advances in diagnostic imaging modalities such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) and echocardiography [ 9 , 10 , 34 ]  . 
multidetector ct angiography ( mdcta ) yields high - resolution angiographic studies complemented by highquality reformatted mediastinal window images allowing the identification of the origin and course of the pulmonary arteries . 
 by employing a large radiologic two institutions database to capture the greatest number of these rare focal vascular dilatations , the objective of this article is to provide accurate mdcta findings of the size , presentation , risk stratification and differential diagnosis of ppaa . 1 3 la radiologia medica ( 2018 ) 123 : 664675 fig . 
a mdcta axial image ( lung window ) of mycotic peripheral aneurysms appears as multiple small vascular opacities ( arrow ) surrounded by ground - glass halos caused by perilesional hemorrhage ( arrowheads )  . 
 b mdcta oblique sagittal mip reconstruction ( lung window ) shows focal iatrogenic ( swan - ganz catheter ) aneurysm of medial segment of middle lobe artery in severe acute hemoptysis ; note perianeurysmal parenchymal hemorrhagic ground - glass opacity and gas ( white arrow )  . 
c follow - up chest x - ray ( cxr ) and d axial unenhanced mdcta after endovascular treatment ( coil embolization ) of a mycotic inferior lingular segment ppaa appearing as a lung nodule on cxr ( arrows )  . 
e mdcta sagittal reformatted image and f axial pet / ct image demonstrate multiple peripheral hyperenhancing and hypermetabolic nodules ( arrows ) surrounded by ground - glass opacity areas ( arrowheads ) in both lungs . 
bacterial cultures of blood grew staphylococcus aureus materials andmethods this study was approved by the institutional review boards at our tertiary referral cardiothoracic and emergency hospital for retrospective review of patients records and imaging . 
all multidetector computed tomographic angiograms with the diagnosis of peripheral pulmonary artery , aneurysm , dilatation , dissection or rupture present in the radiologists final report at our institutions were retrospectively identified in radiology information system from january 2012 to january 2017 . 
mdcta examinations were performed with 16 - slice ( brilliance ct , philips medical systems ) or 64 - slice ( lightspeed vct , ge healthcare ) scanners with intravenous injection of nonionic iodinated contrast medium , volumes ranging from 60 to 130ml and injection rates ranging from 2.5 to 5ml / s . 
however , with fast mdcta ( scan duration < 10s ) , the contrast administration protocols have become unified with the prevailing use of a faster injection of a smaller amount of contrast mediusaline flush was used for all patients . 
 although axial sections are still the mainstay of interpretation , two - dimensional and three - dimensional reformatting techniques such as maximum intensity projection ( mip ) , curved planar reformation ( cpr ) , multiplanar reformation ( mpr ) and volume rendering ( vr ) may facilitate interpretation and improve communication with the referring physicians 1 3 668 la radiologia medica ( 2018 ) 123 : 664675 table 3 characteristics of patients with ppaa ( 19 cases ) cause patients ( no ) gender age ( mean and range ) clinical history pahb hemoptysis infectious bacterial endocarditis pulmonary tb fungal pn . 
by using this model , we have estimated the presence of correlation between the variables and its intensity ( related to the value of the beta estimated ; the intensity explains the change in value of diameters as consequence of a unit variation of the number of aneurysm ) using the ordinary least squares ( ols ) method . 
b mip coronal reformatted image shows a partially thrombosed left descending pulmonary artery pseudoaneurysm and thrombosed aneurysms in the segmental branches of the left lower lobe ( arrow )  . 
d after massive hemoptysis , a followup mdcta axial image shows a mycotic ( rasmussen ) false aneurysm ( arrow ) resulting from caseous necrosis of a pulmonary artery branch . 
e mdcta axial image shows impending rupture findings in a large rasmussen false aneurysm of the segmental branch of right descending pulmonary artery ( arrow ) with high attenuation in the thrombus ( asterisk ) ; f multiple centrilobular and tree - in - bud parenchymal nodules and y - , v - shaped branching opacities from active tb disease are better showed at lung window results nineteen patients with ppaa were diagnosed by mdcta from january 2012 to january 2017 at our institution . 
ten of our patients ( 52.6% ) with ppaa had associated pulmonary arterial hypertension ( pah ) , 7 into group 1 ( related to idiopathic , heritable , drug induced and other causes of pah ) , 1 into group 3 ( related to lung diseases and / or hypoxia ) and 2 into group 5 ( pah with unclear and / or multifactorial mechanisms ) of the updated pah clinical classification [ 19 ]  . 
despite the limited number of patients in our database , likely due to the rarity of the disease , we found a 1 3 670 la radiologia medica ( 2018 ) 123 : 664675 fig . 
ad axial and oblique coronal mip reformatted images show right atrium tumor ( black arrows ) , multiple pulmonary metastatic lesions , tumoral bilateral thromboembolic disease ( arrowheads ) and partially thrombosed right lower lobe pulmonary artery pseudoaneurysm ( white arrow )  . 
a 78 - year - old man with metastatic renal cell carcinoma ( mrcc ) , pulmonary hypertension and hemosputum , treated with sunitinib , a multitargeted tyrosine kinase inhibitor . 
ef mdcta axial images show a small right lower lobe ppaa that increases in diameter at follow - up ct ( arrows ) certain negative relationship ( = 0.30cm ) between the diameter and number of aneurysms with a higher number of aneurysms per patient correlating with a smaller diameter . 
the mechanism of aneurysm formation lies in the vessels wall destruction and replacement by granulomatous , neoplastic or fibrotic tissue causing thickening and weakening of the outer arterial wall and then extending to the inner wall [ 3 , 25 ]  . 
most infected or mycotic aneurysms arise in peripheral pulmonary arteries , usually as complications of right heart infective endocarditis , mainly seen in the elderly and immunocompromised patients , intravenous drug users , native or prosthetic valve endocarditis or in cardiac device holders [ 21 , 4146 ]  . 
 they may arise through hematogenous seeding from distant septic foci , septic microemboli to the vasa vasorum or neighboring infected lesions and have a high mortality rate approaching 80% [ 9 , 44 ]  . 
characteristic mdcta findings include a lobulated vascular mass with irregular wall , a perivascular soft tissue mass , ground - glass opacification and / or parenchymal consolidation , cavitary nodules , pulmonary artery embolization , infarcts , stranding and pleural fluid . 
 ac mdcta axial ( parenchymal window ) , oblique coronal ( parenchymal window ) and oblique sagittal ( mediastinal window ) images show a iatrogenic pseudoaneurysm in medial segmental artery of middle lobe ( black arrows )  . 
e mdcta axial images parenchymal window and ( f ) mediastinal window show a posterior subsubsegmental ppaa of right lower lobe ( arrows ) branch by a tuberculous cavity [ 36 , 47 ] , and it usually involves the upper lobes or the superior segment of a lower lobe in the setting of reactivation tuberculosis . 
rasmussen aneurysms can vary in size and number but most commonly present as small ( < 1cm ) solitary lesions surrounded by a parenchymal opacity / consolidation [ 49 ]  . 
signs of pulmonary arterial source of hemoptysis seen on mdcta include direct visualization of a focal contrast - enhancing dilation , an outpouching arising from the pulmonary artery ( 75% ) or the presence of a pulmonary artery in the inner wall of a pulmonary cavity ( 25% ) [ 4850 ]  . 
a study of 50 individuals with marfan syndrome identified an enlarged pulmonary artery root in 74% [ 62 ] , while only one case of large main pulmonary trunk aneurysm was published [ 63 ]  . 
impending rupture in a large mycotic pseudoaneurysm of the lateral segmental middle lobe artery in a 67 - year - old man with massive hemoptysis and methicillin - resistant staphylococcus aureus sepsis . 
a unenhanced mdcta axial image shows a curvilinear area of higher attenuation ( arrowheads ) in a large middle lobe aneurysm , corresponding to hemorrhage insinuating into the mural thrombus ( crescent sign ) with associated pleural effusion . 
d mdcta delayed phase axial image shows a serpiginous enhancing wall vessel rim ( curved arrow ) that may reflect adventitial inflammation or vasa vasorum congestion of the vasa vasorum causing vascular wall ischemia [ 65 ]  . 
to our knowledge , there are no reports in the literature of association between sunitinib cancer therapy and peripheral pulmonary artery aneurysms and between fibrotic lung pattern ( uip ) and pulmonary artery dilatation . 
in the last case , it is possible to think that the fibrotic retraction can also be exercised on peripheral 1 3 674 la radiologia medica ( 2018 ) 123 : 664675 vascular branches as well as on the small airways . 
the differential diagnosis of ppaa includes other rare causes of vascular mass - like lesion such as venous varix , congenital or acquired that involves pulmonary venous structures , the high - flow pulmonary carcinoids and some arteritis with a rare pulmonary arteries involvement such as takayasus arteritis . 
similar to aortic aneurysms , the risk of rupture of ppaa increases with the size of the aneurysthis is in accordance with laplace law , which states that wall tension increases with the diameter of the vessel and with an increased transmural pressure such as in pulmonary hypertension [ 35 , 9 , 10 ]  . 
endovascular coil ( and / or balloon ) embolization is currently preferred as it is less invasive with fewer complications observed over surgical intervention which poses a very high risk of increased morbidity and mortality , especially for patients with severe pah [ 15 ]  . 
there are no treatment guidelines because of low disease incidence , but treatment is generally recommended for aneurysms progressively increasing in size and in the presence of clinical ( abrupt chest pain ) and ct findings indicative of impending rupture . 
we also define the degree of vascularity using superb microvascular imaging ( smi ) , power doppler ( pd ) , and color doppler ( cd ) and compare smi with cd and pd . materials and methods a total of 100 cases , comprising 50 girls and 50 boys , with ages ranging from 3 to 17years were included in this prospective study . 
swe , smi , pd , and cd measurements were taken from both parotid glands , and the relationships with sex , age , and body mass index ( bmi ) were determined . 
the median values obtained with smi were significantly higher than the median values obtained with both pd and cd . conclusion this study determined the reference swe , smi , pd , and cd values for normal parotid glands in healthy children and adolescents . 
no : 369 , konya , turkey 3 department ofradiology , istanbul faculty ofmedicine , turgut ozal street , fatih , istanbul , turkey introduction ultrasound elastography is a noninvasive method used to measure the stiffness of tissuethat is , it can obtain a quantitative estimation of the elasticity of different tissues . 
as a result , normal elasticity values for the parotid gland may be a marker for diagnosis of infectious diseases like parotitis , inflammatory diseases like juvenile sjogren syndrome , and neoplastic diseases like lymphoma . 
additionally , the vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 710718 normal values for the same organ may vary with age or bmi [ 3 , 4 ]  . 
in the literature , the reference values for various tissues ( e.g. , liver , spleen , thyroid , breast , muscle and tendon , and kidney ) in adults and children have been reported using different devices that employ se , arfi , or swe techniques [ 57 ]  . 
though the normal swe elasticity values for parotid gland tissue have been defined in previous studies , these studies only include the adult population [ 8 , 9 ]  . 
 [ 10 ] published a study defining the normal elasticity values for the parotid gland in pediatric patients using se ; however , to the best of our knowledge , there is no study available that has determined the normal elasticity values with swe . the use of doppler methods for the parotid gland is important in diffuse diseases and tumors [ 11 ]  . 
as in adults , increased or reduced tissue vascularity of the parotid gland in children may be helpful in identifying infectious , autoimmune , or neoplastic diseases [ 12 ]  . 
however , no study has measured or determined the normal vascularity of parenchyma using the smi technique for normal parotid glands in children . the aim of our study is to investigate elasticity values with swe for parotid gland parenchyma in healthy tissue and to define the degree of vascularity using smi , pd , and cd techniques . 
 exclusion criteria were age younger than 3years , insufficient cooperation , rejecting participation in the study , fever during evaluation , acute parotitis , and tumor , trauma , and surgical history related to the parotid gland . 
all cases included in the study had sufficient image quality and employed an appropriate technique , so no case was excluded from the study . elastography and doppler measurements were completed by common consensus between two experienced pediatric radiologists with more than 2years of elastography experience . 
all measurements were taken with an aplio 500 platinum ultrasound device ( toshiba medical systems , japan ) with a high - frequency linear probe ( frequency range 514mhz )  . 
1 shear wave elastography and doppler techniques were performed while each child remained calm and motionless with their head turned to the side that was opposite of the investigated parotid gland . 
three valid measurements were taken in two modes ( kpa and m / s ) a mode in which reliable data are obtained when the lines are parallel and smooth , and the increase in distance between the lines is parallel to the increase in elasticity . 
subsequently , a 5 - mm - diameter region of interest ( roi ) was used to take measurements at three different points within homogeneous parenchyma that did not contain vascular structures and lymph nodes . 
 smi is an advanced application of scattering suppression to subtract flow signals with high frame rates displayed as a colored image ( color smi ) or a gray - scale image of flow ( monochrome smi ) [ 17 ]  . 
3 two vascular spot flows using color doppler imaging ( a ) , three vascular spot flows using power doppler imaging ( b ) , five vascular spot flows using superb microvascular imaging ( c ) left parotid gland were compared to determine their respective normal elasticity values . 
 variables were investigated at the 95% confidence interval , and p values below 0.05 were accepted as significant . results the descriptive analysis of age , bmi as well as the elasticity ( kpa ) and shear wave velocity ( m / s ) values of the right and left parotid glands from swe and the vascular counts from within the fixed window using smi , cd , and pd are given in table1 . 
there were no significant differences between smi , cd , and pd for above and below the age of 10 or for right and left parotid glands ( p > 0.05 ) ( table5 )  . 
 in pediatric patients , the majority of parotid gland diseases comprise viral infections ( e.g. , mumps , cmv , and hiv ) , bacterial infections ( e.g. , staphylococcus aures , gram - positive cocci , gram - negative rods , and anaerobic bacteria ) , and sialadenitis [ 12 ]  . 
in children and adults , early identification and beginning appropriate treatment is very important in terms of preventing complications like sialectasis , cervical , or supraglottic edema from spreading to other organs and abscesses . 
other more rarely observed diseases in children are juvenile sjogren syndrome , hemangiomas and vascular malformations , and lymphomas [ 18 ]  . though imaging methods like magnetic resonance imaging ( mri ) , computed tomography ( ct ) , mri sialography , and angiography may be used in the diagnosis of these diseases , ultrasound scanning is an excellent method , especially in children since it is noninvasive , comfortable , easily accessible , and free of ionizing radiation [ 19 ]  . 
 [ 20 ] reported that parotid glands showed normal echotexture with multiple hypoechoic intraparenchymal lymph nodes on gray - scale ultrasound in the diagnosis of post - pubertal epidemic parotitis . 
4 below 10years of age ( 10 ) , elasticity values ( in kpa and m / s ) significantly increased in the bilateral parotid gland compared to above 10years ( < 10 ) the cd mode is beneficial to identify parenchyma and mass vascularization or non - perfused cysts [ 12 ]  . 
smi is a more recent method compared with elastography , and its greatest advantage is that it can show very fine vascular structures more successfully than cd and pd [ 21 ]  . 
normal elasticity and vascularity values for the parotid gland may help as a marker for diagnosis of infectious diseases like parotitis , inflammatory diseases like juvenile sjogren syndrome , and neoplastic diseases like lymphoma . 
this study is unique because it investigates the normal parotid glands of children and adolescents using swe and smi methods . there may be differences in the elasticity values of organs between children and adults . 
5 the median number of vascular spots obtained by superb microvascular imaging was significantly higher than the median number of vascular spots obtained by both color doppler imaging and power doppler imaging transition from childhood ( under 10years ) to adolescence ( above 10years )  . 
 [ 10 ] , in a study using the se elastography method on a total of 54 children , determined the normal strain index value for the parotid gland and found no significant difference between male and female children , age , and bmi . 
moreover , the higher number of patients in our study may have changed the statistics and results . identification of increased vascular flow in soft tissues is accepted as showing active inflammation and parenchymal remodeling in the parotid gland , as in other organs [ 2224 ]  . 
 [ 23 ] reported that vascularization in the parotid gland increased due to benign lymphoepithelial lesions in hiv infections , and mixed nodules were more hypervascular compared to cyst - like 1 3 la radiologia medica ( 2018 ) 123 : 710718 nodules . 
within a fixed window with 1.5 1cm dimensions , smi imaged 5 1.70 vascular spots in the right parotid gland and 4 1.70 vascular spots in the left parotid gland . 
the basal vascularity values for children found in this preliminary study may be beneficial in terms of identifying sialadenitis , autoimmune , and neoplastic diseases . among the limitations of our study are the low number of patients , the exclusion of children younger than 3years of age , counting of vascular structures within a fixed window instead of the whole surface of the parotid lobe , and a lack of deep - lobe measurements . conclusion this preliminary study determined the reference swe , smi , pd , and cd values for the parotid gland in pediatric patients . 
thirteen out of 40 were addressed to gallium68psma - 11 ( hbed - cc ) - pet / ct for a biochemical relapse after rp , 14 / 40 after a salvage rt and 13 / 40 after salvage or adjuvant adt . 
gallium68psma - 11 ( hbed - cc ) - pet / ct data changed the therapeutic approach in 28 patients ( 70% )  . conclusions gallium68psma - 11 ( hbed - cc ) - pet / ct can be a useful tool in the restaging of post - rp , rt or adt patients presenting biochemical relapse of pc and it could change the decision - making process in up of 70% of these patients . 
giglio , cefal , italy 4 medical oncology , sacro cuore don calabria hospital , 5 division ofurology , sacro cuore don calabria hospital , negrar , verona , italy negrar , verona , italy 6 nuclear medicine , sacro cuore don calabria hospital , negrar , verona , italy 7 university ofbrescia , brescia , italy the results of the available randomized controlled trials ( rcts ) showed that 3752% of prostate cancer ( pca ) patients will present a biochemical relapse of the disease after radical prostatectomy ( rp ) [ 13 ]  . 
the same rcts showed that adjuvant radiotherapy has a well - established role in the treatment of biochemical recurrence ( bcr ) , allowing an increase of biochemical - free survival rates [ 13 ] or overall survival [ 1 ]  . 
 bcr after rp or rt usually precedes the clinical evidence metastases by several years : the role of conventional imaging techniques ( bone scintigraphy , computed tomography ) is poor in asymptomatic patients [ 4 ]  . 
moreover , new imaging techniques , as ( 18f o 11c ) choline pet / ct , have been vol . : ( 0123456789 ) 1 3 720 la radiologia medica ( 2018 ) 123 : 719725 recently introduced in the clinical approach of relapsing pca patients , and these tools allow a more precise identification of intraprostatic , nodal and / or systemic disease [ 5 ]  . 
these new techniques of imaging not only allow the identification of macroscopic relapses , but also an earlier identification of failure sites , thus allowing the identification of oligometastatic patients who could benefit from local approaches [ 6 , in the setting of psa relapse after surgery , choline pet / ct has been recognized as a potential diagnostic exam widely used with different intents : ( 1 ) to detect loco - regional relapses or distant metastasis ; ( 2 ) to support the decisionmaking strategy in rt treatment planning [ 5 , 8 , 9 ]  . 
recently , 68 - ga psma ligand pet / ct has been more and more evaluated as alternative to choline pet / ct , as it seems to be more accurate in the identification of macroscopic relapses at lower levels of psa [ 1012 ]  . aim of this retrospective study is to analyze the changes in the therapeutic approach to pca patients presenting a bcr based on the results of gallium68psma - 11 ( hbed - cc ) - pet / ct . materials andmethods since june 2016 , gallium68psma - 11 ( hbed - cc ) - pet / ct is available in the nuclear medicine department of the sacro cuore don calabria hospital ( negrar , italy )  . 
since then , to assess its role in the diagnostic approach of relapsing pca patients , we decided , in agreement of the nuclear medicine department , to include in a database all pca patients presenting a bcr discussed in our multidisciplinary tumor board ( mtb ) and a potential indication of gallium68psma - 11 ( hbed - cc ) - pet / ct . 
the results of the gallium68psma - 11 ( hbed - cc ) - pet / ct were presented to the mtb , who decided whether to confirm or not the initial treatment . 
all patients undergoing to gallium68psma - 11 ( hbed - cc ) - pet / ct signed a specific informed consent . in the present analysis , we also created three classes of patients : watch and wait group ( group 1 , n = 6 ) , curative group ( group 2 , n = 12 ) and palliative group ( group 3 , n = 22 )  . 
moreover , we divided our population of study using percentiles - based criteria for psa rising to evaluate potential correlations with gallium68psma - 11 ( hbed - cc ) - pet / ct findings . gallium68psma11 ( hbedcc ) pet / ct acquisition procedure gallium68psma - 11 ( hbed - cc ) - pet / ct scans were performed in accordance with the standard whole - body oncological protocol following the guidelines of the european association of nuclear medicine ( eanm ) [ 13 ]  . 
all gallium68psma - 11 ( hbed - cc ) - pet / ct scans were obtained with a hybrid pet / ct tomography ( siemens mct , global siemens healthcare germany )  . 
the pet / ct acquisition protocol consisted of a one - phase procedure : whole - body scan 60min after injection from the base of the skull to the superior portion of the thighs ( 89 bed positions , 2min per bed or flow - motion technology ) with patient positioned supine with arms crossed above head . 
mim maestro software is a constrained , intensity - based free form deformable registration algorithm ; it uses the entire contrast window of the ct for matching the two scans . population from 06 / 2016 to 04 / 2017 , a total of 40 consecutive patients received a gallium68psma - 11 ( hbed - cc ) - pet / ct . 
thirteen out of forty were addressed to gallium68psma - 11 ( hbed - cc ) - pet / ct for a bcr after rp only , 14 / 40 presented a bcr after a salvage 1 3 la radiologia medica ( 2018 ) 123 : 719725 rt post - rp and 13 / 40 after adjuvant or salvage adt postrp . 
adt was delivered after surgery and / or after radiotherapy , depending on the clinical situation of the patient and the clinical judgment of the surgeon or the radiation oncologist . 
table3 gives an insight into the types of changes that have been proposed . before gallium68 psma - 11 ( hbed - cc ) - pet / ct , 6 patients would be classified in the group 1 , 12 in the group 2 and 22 in the group 3 . 
after gallium68psma - 11 ( hbedcc ) - pet / ct , 4 / 6 group 1 patients ( 67% ) and 17 / 22 group 3 patients ( 77% ) finally received a treatment . 
after gallium68psma - 11 ( hbed - cc ) - pet / ct , 14 / 22 finally received only loco - regional treatments ( 63% ) , delivered with stereotactic body radiotherapy ( sbrt , n = 11 ) or pelvic irradiation ( n = 3 , table3 )  . 
in conclusion , based on the results of gallium68psma - 11 ( hbed - cc ) - pet / ct , 17 / 22 patients ( 77% ) initially candidates to adt finally received a local treatment instead or with adt . six patients were candidates to no treatments before gallium68 psma - 11 ( hbed - cc ) - pet / ct : of them , three finally received sbrt and one sbrt + adt . 
in 67% of these patients , gallium68psma - 11 ( hbed - cc ) - pet / ct changed the treatment . gallium68 psma - 11 ( hbed - cc ) - pet / ct showed an impact also in the patients who already had an indication for local treatments . 
based on the results of gallium68psma - 11 ( hbed - cc ) - pet / ct , 4 received also a boost on the positive pelvic nodes identified at gallium68psma - 11 ( hbed - cc ) - pet / ct , 1 finally received sbrt and 1 palliative bone rt . 
globally , gallium68psma - 11 ( hbed - cc ) - pet / ct changed the therapeutic strategy in 54% of this last subset of patients . discussion to the best of our knowledge , this is one of the largest studies exploring the impact of gallium68psma - 11 ( hbedcc ) - pet / ct in the decision - making process of a pcaspecialized mtb dealing with pca patients presenting a bcr [ 14 ]  . 
our results show that in this clinical setting , gallium68psma - 11 ( hbed - cc ) - pet / ct results could influence the clinical decision in 70% of patients . 
noteworthy , more than 70% of the cases moved from palliative to curative approaches , with 80% of them finally avoiding the adt that was initially prescribed . some important limitations of this study should be acknowledged , as they could influence the results . 
 the lack of comparison of other standard imaging modalities could potentially be considered a bias , but the available literature seems to support our assumption about the superiority of gallium68psma - 11 ( hbed - cc ) - pet / ct in terms of accuracy in this setting [ 15 ]  . 
anyway , we can agree that from a methodological point of view the possibility of having the results of other standard imaging modalities ( for example , 11cor 18f - choline pet / ct ) would add further interesting information . 
moreover , we analyzed a quite heterogeneous population with 27 / 40 patients who received some forms of local ( n = 14 ) or systemic treatments ( n = 13 ) after rp . 
to date , choline pet / ct remains the most used examination in patient with prostate cancer relapse , despite its low sensibility for low psa levels [ 5 ]  . 
 in their study , roc analysis showed thatpet / ct - positive andpet / ct - negative patients could be distinguished better using a psa cut - off value of 1.4ng / ml [ 16 ]  . 
differently , gallium68psma - 11 ( hbed - cc ) - pet / ct shows better pathology - proven sensibility and specificity rates when compared to radio - choline pet / ct , as demonstrated also in a recent surgical series by pfiser etal . 
in our experience , 32 / 40 patients ( 80% ) presented positive findings in gallium68psma - 11 ( hbed - cc ) - pet / ct , thus confirming the high diagnostic value of this technique . 
patients receiving only systemic treatments for their bcr were classified into group 3 1 3 724 la radiologia medica ( 2018 ) 123 : 719725 potential impact of gallium68psma - 11 ( hbed - cc ) - pet / ct in changing the therapeutic approach . 
in our study , for example , 4 / 6 group 1 patients ( 66% ) and 17 / 23 group 3 patients ( 74% ) finally received a curative treatment . 
although whether this improves patient outcomes still remain unclear , the impact of potentially avoiding adt and all the potential adt - related toxicities is noteworthy [ 27 , 28 ]  . conclusions in conclusion , therapeutic strategy based on the gallium68psma - 11 ( hbed - cc ) - pet / ct was changed in 70% of patients analyzed compared to the strategy that would have been proposed in case pet was not available and / or not strictly indicated . 
its role in improving the selection , and then the outcomes , of patients who would be treated with curative intent deserves further prospective evaluations . funding this research did not receive any specific grant from funding agencies in the public , commercial , or not - for - profit sectors . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standard all procedures were in accordance with the ethical standards and the helsinki declaration . 
this series aims to describe an initial single - center experience examining intraprocedural safety and technical success of mvp . materials and methods ten patients ( mean age 55.1years ) have been treated for arterial embolization using mvp ; eight extracranial and two intracranial arterial embolizations have been performed . 
the embolizations were because of : four bleedings , three aneurysms , two pseudoaneurysms , and one presurgical nephrectomy . results mvp3 was used in five cases , mvp5 in four cases , and mvp 7 once . 
in all cases , the mvp was successfully released in < 1min six patients , the mvp was the sole embolizing agent employed , while in four subjects , it was positioned complementary after coils . 
cardarelli 9 , 80131naples , italy 2 radiology department , universit campus bio - medico di roma , via alvaro del portillo 200 , 00198rome , italy 3 neuroradiology department , aorn cardarelli di napoli , via a . 
cardarelli 9 , 80131naples , italy vol :  . ( 1234567890 ) 1 3 radiol med ( 2018 ) 123 : 236243 multiple pathologies , accounting mainly from : hemorrhages , aneurysms , pseudoaneurysms , and artero - venous malformations . 
ptfe polytetrafluoroethylene in all cases , a thin slice ( 0.65 mm ) contrast - enhanced computed tomography ( cect ) was acquired before the procedure to plan the embolization ( see figs.2 , 3 , 4 , 5 , 6 , 7 )  . once recognized the target vessel of embolization at cect , a diagnostic digital subtraction angiography ( dsa ) was performed using a 5fr catheter with a tip curve that better fits the vessel anatomy ; this confirmed the site to embolize and the size of the vessel to occlude . 
a cect scan in arterial phase , 0.65mm slice thickness , sagittal reconstruction , maximum intensity projection : bleeding from the right facial artery with cutaneous fistula ( white arrow ) ; b dsa in sagittal projection confirming the cect findings ( white arrow ) after catheterization of the external carotid artery ; c dsa in sagittal projection showing coils embolization ( white arrow ) of the bleeding after superselective microcatheterization of the facial artery statistical analysis all data analyses were performed in a matlab environment ( mathworks , inc , natick , massachusetts , usa )  . results in eight patients , the mvp was adopted in extracranial arterial vessels , while in two cases , the carotid syphon was embolized . in all cases , the mvp was successfully released in < 1min . four cases were treated because of bleedings ( see table2 : cases 1 , 3 , 5 and 8 ) : one traumatic , one neoplastic , and two iatrogenic . 
the iatrogenic hemorrhages occurred after positioning of an abdominal drainage and a nephrostomy . in two patients ( see table2 : cases 2 and 7 ) , an intrahepatic and a descendent genicular arteries iatrogenic pseudoaneurysms were embolized . finally , in 3 subjects ( see table2 : cases 6 , 9 , and 10 ) , the mvp was released to occlude a true aneurysm , one of which was a recurrence of a previously pluriembolized carotid syphon giant aneurysm . the mvp3 was used in five cases : segmental branch of right hepatic artery ( case 2 ) , left epigastric artery ( case 5 and 8 ) , descendent genicular artery ( case 7 ) , and carotid syphon ( case 10 ) ; the mvp5 was chosen in four cases : external carotid artery ( case 1 ) , intraparenchymal branch of the right renal artery ( case 3 ) , splenic artery ( case 6 ) , and carotid syphon ( case 9 ) ; the mvp7 was adopted once in the left renal artery ( case 4 )  . in six patients , the mvp was the primary and sole embolizing agent employed ( cases 1 , 2 , 3 , 5 , 7 , and 8 )  . 
in four subjects ( cases 4 , 6 , 9 , and 10 ) , the mvp was positioned complementary after coils to definitely seal the target artery just proximally to the lesion ; this approach was chosen in three patients affected by aneurysms where coils were used to fill the sac and in one case of preoperative embolization for surgical nephrectomy of a renal malignancy . in one case ( see table2 : case 4 ) , a preoperative occlusion of the left renal artery was performed propaedeutics to surgical nephrectomy because of a large renal malignancy . the technical and clinical success was obtained in 100% ; hemorrhages were interrupted , and aneurysms and pseudoaneurysms did not show recanalization at follow - up . 1 3 radiol med ( 2018 ) 123 : 236243 fig . 
it was so planned external carotid artery embolization with a mvp5 , the vessel having a caliper of 4.1 m dsa ( a ) confirmed bleeding recurrence ; the mvp5 was positioned into the external carotid artery in correspondence of the origin of the facial artery . 
a dsa in sagittal oblique projection showing bleeding recurrence : the 5 fr catheter ( dotted black arrow ) in correspondence of the carotid bifurcation , 2.7 fr microcatheter into the origin of the external carotid artery ( black arrow ) , hemorrhagic recurrence with extraluminal contrast agent ( white arrow ) , and previous coils embolization ( dotted white arrow ) ; b dsa in sagittal projection demonstrating successful embolization with bleeding resolution after positioning of a mvp5 : distal and proximal radiopaque markers of the mvp5 positioned into the external carotid artery in correspondence of the origin of the facial artery ( white arrows ) ; previous coils embolization ( dotted white arrow ) the radiological follow - up ( range 2weeks to 10months ) showed no mvp migrations . discussion interventional radiologists can choose between a wide spectrum of devices when facing arterial embolization , including liquids , particles , and metallic agents ; each product presents its advantages and limits ; therefore , the appropriate choice is made patient by patient . liquids and particles are not controllable agents as detachable metallic devices , and therefore , distal extension and migration are risks that should be contemplated . 
furthermore , for the same reason , it has been reported a reduced delayed recanalization through the device thanks to the ptfe coating compared to the amplatzer plug and coils [ 4 ]  . its successful use has been described in small series in visceral [ 1 , 35 ] , cervical [ 6 ] , and cerebral [ 710 ] districts on both adult [ 1 , 3 , 4 , 6 , 7 , 9 ] and pediatric patients [ 5 , 8 , 1014 ] , including also cardiac interventions [ 1114 ]  . 
 the ptfe coating allows fast embolization onset , because it immediately occlude the vessel after mvp release if the right device caliper has been selected ; on the other hand , longer procedural time frequently occurs when using coils , 1 3 240 radiol med ( 2018 ) 123 : 236243 fig . 
cect showed a 19mm pseudoaneurysm refurnished by the descendent genicular artery ( a ) , in correspondence of the point of entrance of an arthroscopic trocar ; the endovascular embolization was planned . 
dsa confirmed cect findings ; with a left femoral access , a 5fr catheter ( mp a1 , merit medical , usa ) was positioned in cross into the right superficial femoral artery ( b ) and a 2.7 microcatheter ( progreat , terumo , japan ) was advanced in proximity of the pseudoaneurysm ( c ) ; other refurnishing vessels were excluded . 
a cect scan in arterial phase , 0.65 mm slice thickness , coronal reconstruction , maximum intensity projection : pseudoaneurysm ( white arrow ) of the right descendent genicular artery ( white dotted arrow ) ; black asterisk indicates the medial femoral condyle . 
 b diagnostic dsa in postero - anterior projection confirming cect findings : pseudoaneurysm ( white arrow ) of the right descendent genicular artery ( white dotted arrow ) ; the black arrow shows the right superficial femoral artery , the grey arrow indicates the tip of the 5fr diagnostic catheter . 
c superselective dsa with microcatheter ( grey arrow ) positioned into the distal segment of the descendent genicular artery ( white dotted arrow ) showing the pseudoaneurysm filled by the contrast agent ( white arrow ) because these have no coating and so release of multiple coils is often required . the mvp should not be considered as an alternative to coils ; it is instead a device with different features that could be used apart from or together with coils as complementary agent for backward sealing , as occurred in four patients in this series ( cases 4 , 6 , 9 , and 10 ) where mvp was released at the side of coils . in this sample , the mvp has been safely employed for body and neurodistricts in adults patients ; the technical success has been obtained in 100% for both primary and complementary release of the device . based on the reported experience , the mvp presents the following advantages : the nitinol skeleton is soft and so the device is able to easily navigate in tortuous and twisted vessels ; mvp3 and mvp5 can be released through a 0.027 microcatheter , allowing distal embolization in small arteries ; the detachable system permits to retract and repositioning mvp multiple times and landing in the preferred site safely when the operator is satisfied . 
in this series , no difficulties were encountered in withdrawing the mvp within the microcatheter and repositioning thanks to the nitinol skeleton softness . main limitations of mvp are related to the visibility of only the distal and proximal radiopaque markers ; the correct deployment of the central portion can be assessed indirectly , after contrast agent injection . 
furthermore , operators should always assess the availability of a sufficient straight landing zone able to receive the unconstrained length of the mvp ( 12mm for mvp3 and mvp5 ; 16mm for mvp7 ) before releasing the device . 
finally , as for all plugs , the diameter of the vessel to embolize has to be precisely measured to adopt the correct mvp size and avoid device migration and unsuccessful procedures . even if the reported experience is limited because of the retrospective design and small size sample and further larger studies are required , according to the proposed data , the mvp seems to be a safe embolizing device ; 1 3 radiol med ( 2018 ) 123 : 236243 fig . 
a postero - anterior projection fluoroscopy showing the mvp3 immediately after release : proximal and distal radiopaque extremities of the mvp3 ( white arrows ) , tip of the pusher wire after mvp detachment ( dotted white arrow ) , and tip of the 2.7fr microcatheter ( grey line )  . 
b postero - anterior projection fluoroscopy after mvp3 embolization demonstrating successful vessel occlusion without pseudoaneurysm filling : proximal and distal radiopaque extremities of the mvp3 ( white arrows ) , tip of the 2.7 fr microcatheter ( grey line ) ; the orthopedical screw is also appreciable on the lateral femoral condyle ( white dotted line ) fig . 
6 asymptomatic 57 - year - old woman presenting with a unruptured , strict neck , giant aneurysm ( 43mm ) of the left carotid syphon ( a ) ; the lesion was treated by a stent - assisted coils embolization ; however , after 1year , the aneurysm recurred ( b )  . 
b aneurysm recurrence after stent - assisted coils embolization 1 year later , with enlargement of the proximal portion of the neck ; coils ( black asterisk ) , recurrence with contrast agent filling the sac ( white asterisk )  . 
eight months later , a second recurrence was evident ( a ) at dsa ; after a balloon occlusion test demonstrating a good rightleft anterior circle communication ( b ) , it was decided to definitely occlude the left internal carotid with a mvp5 ( c )  . 
b postero - anterior projection dsa shows left balloon occlusion test demonstrating a good rightleft anterior circle communication ; balloon occlusion catheter into the left internal carotid ( white dotted arrow )  . 
the doses to uterus and ovaries for each phase were calculated with the ctexpo software , taking into consideration the sizespecific dose estimate ( ssde ) after measuring the size of every single patient . results the final cohort was composed of 76 female patients with an average age of 30 ( from 19 to 40 years )  . 
 unindicated scans were most frequent for appendicitis and unlocalized abdominal pathe excesses of mean radiation doses to the uterus and ovaries due to unindicated phases were , respectively , of 38 and 33msv per patient . conclusion in our experience , unindicated additional ct phases were numerous with a significant excess radiation dose without an associated clinical benefit . 
high levels of ionizing radiation exposure are known to increase the risk of cancer [ 7 , 8 ] , but the data for lower doses of radiation are not as clear and remain controversial [ 9 , 10 ]  . in line with this trend , the role of ct in the evaluation of acute abdominal and pelvic conditions continues to expand . 
in this anatomical region , there are organs , such as female gonads , that are sensitive to radiation exposure with the potential risk of carcinogenesis / mutagenesis [ 5 ]  . quantitative human data on the risks of genetically transmissible diseases and cancer induction following the exposure of female germ cells to ionizing radiation are scarce [ 11 ]  . in the absence of clarity on this topic , the acr , the health physics society ( hps ) , and other interested organizations have adopted the alara principle : physicians should minimize the amount of radiation exposure to only what is medically necessary [ 12 , 13 ]  . most strategies to reduce radiation associated with ct have focused on vetting ct as the appropriate diagnostic test , limiting the examination to the anatomic area in question and optimizing scanning parameters ( particularly in pediatric patients ) [ 14 ]  . 
an important but potentially overlooked source of medically unnecessary radiation is the use of multiphase examinations when a single or lesser number of phases would suffice [ 14 ]  . 
the acr has developed evidence - based appropriateness criteria describing scanning protocols for various clinical conditions [ 15 ]  . the purpose of this study is to determine the frequency of unindicated ct phases , according to these criteria and evidence - based data from the literature [ 16 , 17 ] and to evaluate the resultant excess absorbed radiation doses to the uterus and ovaries in women of reproductive age who have undergone ct for non - traumatic abdomino - pelvic emergencies . 
our results could inspire other authors to verify the excess of radiation dose in their clinical practice and promote the use of ct protocols tailored to the clinical indications . radiol med ( 2018 ) 123 : 185190 materials andmethods study design andsetting this is a retrospective and descriptive study . 
for this study , we used visipaque 320mgi / ml ( ge healthcare , united states ) , iopamiro 370 mgi / ml ( bracco , italy ) , and iomeron 400mgi / ml ( bracco , italy )  . the contrast - enhanced acquisition in the arterial phase was performed with bolus tracking after 20s by the recognition of a density of 100hu , in a region of interest ( roi ) , 1 3 radiol med ( 2018 ) 123 : 185190 usually localized in the aorta at the level of the celiac artery . 
acr appropriateness criteria and evidence - based data from the literature [ 16 , 17 ] were used as the gold standard . for the ct examination , acr appropriateness criteria enable radiologists to establish if the ct examination should be done without the contrast injection , or only with the contrast injection , or both with and without the contrast injection , for a given clinical indication . one ct protocol used ( unenhanced , contrast - enhanced or unenhanced , and contrast - enhanced ) was considered appropriate if the acr appropriateness criteria score was equal or higher than 4 ( on a scale ranging from 1 to 9 , scores of 46 indicate that studies may be appropriate , and scores of 79 indicate that studies are usually appropriate ) and unindicated if the score was less than 4 . each examination that had more than one contrastenhanced phase was analyzed by the authors in consensus , who judged an unindicated phase according to the evidencebased data from the literature [ 16 , 17 ]  . 
unindicated phases were reviewed to determine if there was an incidental finding on the scan that could justify additional scanning for further characterization ( e.g. , incidental liver mass necessitating delayed imaging )  . 
the dosimetric data collected were then corrected by a factor , f204 , to obtain the size - specific dose estimate ( ssde ) according to aapm204 [ 18 ] , as dosimetric data provided by the equipment are referred to a cylindrical phantom with a diameter of 3232cm , and there is a need of scaling the data to the actual size of the single patient to have a more accurate evaluation of the doses . 
 between june 2012 and january 2015 , we found 82 women of reproductive age ( 40years or less ) , who had undergone an abdomino - pelvic ct for an abdominal emergency . 
six of these patients were excluded , because acr appropriateness criteria for their clinical indication were not found ( hemoperitoneum in two patients , intestinal bleeding in one patient , fistula of abdominal wall in one patient , exacerbation of crohns disease in one patient , and ischemia of cecum in another patient )  . 
the final cohort was then composed of 76 female patients with an average age of 30 ( from 19 to 40years )  . among these 76 patients , 18 had undergone ct for appendicitis , 17 for unlocalized abdominal pain , 8 for bowel obstruction , 6 for lithiasis , 6 for urinary infection , 6 for renal colic , 4 for salpingitis , 3 for pelvic mass , 3 for cholecystitis , 2 for pancreatitis , 1 for bowel perforation , 1 for diverticulitis , and 1 for upper abdominal mass . 
 1 3 188 radiol med ( 2018 ) 123 : 185190 table 1 ct phases used for each clinical indication with the correlation to acr score clinical indication number of patients acr score number of ct phases number of unindicated ct phases unindicated unenhanced phase unindicated arterial phase unindicated portal phase unindicated delayed phase appendicitis unlocalized abdominal pain 17 bowel obstruction lithiasis urinary infection renal colic salpingitis cholecystitis pelvic mass pancreatitis bowel perforation diverticulitis upper abdominal mass fig . 
precontrast ( a ) , arterial ( b ) , venous ( c ) , and delayed ( d ) ct acquisitions show a dilated appendix with thickened and enhancing walls and stranding of the adjacent fat ( arrows )  . 
only one phase is diagnostic population from medical imaging , despite accounting for only 17% of all imaging procedures [ 20 ]  . given that the majority of radiation exposure is now from man - made sources and that the majority of this exposure originates from medical imaging , it is important to understand the possible effects and risks of this radiation exposure to the human body . 
radiation effects can be divided into two general types : deterministic effects and stochastic effects . 1 3 radiol med ( 2018 ) 123 : 185190 deterministic effects are the result of the excessive cell death that can occur following ionizing radiation exposures and have a known radiation exposure threshold below which their occurrence can be avoided . 
inadvertent deterministic effects have recently been reported in patients following ct [ 21 ]  . radiation to the pelvis can damage uterus and uterine vessels and affect the ability of a woman to carry a pregnancy to term [ 22 ]  . 
the threshold value of absorbed doses for ovarian failure is of 2.56.0gy for single exposure and > 0.2 for a long - term exposure ( yearly or repeated for many years )  . 
it has been found that the same dose of radiation is more likely to cause ovarian failure in older patients ( late 40s ) than in younger patients ( late 20s ) [ 25 ]  . 
the gravid uterus is a radiosensitive organ owing to the developing fetus , and theoretic effects from radiation ( based on animal and human studies ) include prenatal death , growth retardation , mental retardation , and childhood cancer [ 2628 ]  . 
the threshold value for malformation in the conceptus ( i.e. , embryo or fetus ) in the period of organogenesis ( 38weeks of pregnancy ) is 100200mgy , so doses under 50mgy ( 50msv ) have not been associated with an increase in fetal anomalies or pregnancy loss [ 29 ]  . 
this is reassuring , given that an estimated dose to the conceptus from an abdomino - pelvic ct is approximately one - half this amount [ 28 ]  . in addition , evaluating the radiation risk in women of reproductive age , an important parameter to be considered is the ovarian radiosensitivity to genetic damage and its transmission to progeny . 
however , various considerations suggest that extrapolating the data for mice to humans , the sensitivity of follicle / oocyte to radiationinduction of atresia clearly differs between species and follicular stages , and this adds to the difficulty of correctly estimating the genetic hazard of radiation in humans [ 11 ]  . in our study , the effective dose per patient to the ovaries was 70.5msv , less than 100msv , responsible for carcinogenesis , and much less than the 1gy dose that , according to the literature [ 11 ] , could cause chromosomal damage also in human oocytes . we had a total of 93 unindicated phases , a high number in 76 women , with an average of 1.2 inappropriate phases per patient , with an excess dose to the ovaries , for unjustified ct phases , of about 33msv per patient . this dose is high , especially in cases of an exposition for a short period of time , not an infrequent situation in women admitted in the emergency department with complicated abdomino - pelvic emergencies or for complications after surgery ( with the possibility of a cumulative dose superior to 100msv )  . among strategies to manage dose exposure : justification of examination , optimizing scanning parameters , limiting the examination to the anatomic area in question , and avoiding multiphase examinations , we emphasize in particular the last aspect that in our study determined a high dose . acr appropriateness criteria are a good strategy to avoid multiphase examinations , because most of the clinical emergency indications for ct are comprised of a suggested scanning protocol . 
in our study , only a few clinical indications were not included ( hemoperitoneum , intestinal bleeding , fistula of abdominal wall , exacerbation of crohns disease , and ischemia of cecum )  . 
to limit unjustified ct phases , it is helpful to follow evidence - based ct scanning protocols from scientific literature , for different emergency clinical conditions . the limits of our experience are that this is a monocentric study with a relatively low number of women , with no pediatric patients , and our data could be local results that show our experience , focusing the problem of high radiation dose in young female patients as we know that in many countries , there is not a standardization of ct protocols . our results could inspire other authors to verify the excess of radiation dose in their clinical practice and promote european guidelines for ct protocols tailored to the clinical indications . we aim to promote multicentric prospective studies , with trained radiologists and tailored protocols and to observe if retesting them in different clinical indication , there would be a reduction in the excess of ct radiation dose . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
 we evaluated the intraand inter - observer reproducibility of a semi - automatic tool for bac quantification on digital mammograms . materials and methods a multivendor image dataset of 212 mammographic views , 106 cranio - caudal ( cc ) and 106 medio - lateral oblique ( mlo ) , were retrospectively selected from 53 subjects if bac were seen in at least one view . 
further research is needed to translate bac quantification into clinical practice . keywords breast arterial calcifications ( bac ) cardiovascular risk mammography reproducibility * rubina manuela trimboli trimboli.rm@gmail.com integrative biomedical research phd program , department ofbiomedical sciences forhealth , universit degli studi di milano , via mangiagalli , 31 , 20133milan , italy 2 unit ofradiology , irccs policlinico san donato , via morandi 30 , 20097sandonatomilanese , italy 3 kiwifarm s.r.l. , frazionerivalta69 , 12064lamorra , italy 4 postgraduate school inradiodiagnostics , universit degli studi di milano , via festa del perdono 7 , 20122milan , italy 5 u.o. 
c , viale verona 210 , 38123trento , italy 6 division ofmolecular andgender imaging , department ofbiomedical imaging andimage - guided therapy , medical university ofvienna / general hospital vienna , waehringer guertel 18 - 20 , 1090vienna , austria 7 u.o. 
radiologia senologica , irccs ospedale san raffaele , via olgettina 60 , 20132milan , italy 8 department ofexperimental medicine , dimes , institute ofanatomy , university ofgenoa , via de toni 14 , 16132genoa , italy 9 department ofbiomedical sciences forhealth , universit degli studi di milano , via morandi 30 , 20097sandonatomilanese , italy vol :  . ( 1234567890 ) 1 3 radiol med ( 2018 ) 123 : 168173 introduction cardiovascular ( cv ) disease , including coronary artery disease and stroke , still represents the main cause of death in the world [ 1 ]  . 
any preventive strategy needs a correct risk assessment aiming at personalized and appropriate interventions to reduce morbidity and premature mortality as well as to increase quality of life and duration [ 2 ]  . established scores based on traditional risk factors such as the framingham risk score [ 3 ] and the systematic coronary risk evaluation [ 4 ] have limitations and should be further improved [ 1 ]  . 
new methods for the assessment of cv risk have been advocated and studied , including those derived from imaging such us coronary artery calcium score , carotid intima - media thickness , epicardial adipose tissue and breast arterial calcifications ( bac )  . 
variable results have been obtained on the associations of these predictive methods with cv events and the added value on improving risk assessment as an adjunct to the traditional scores is discussed [ 5 ]  . 
thus , the clinical applicability is still challenging , especially when considering potential limitations of imaging - based methods such as lack of standardization and suboptimal reproducibility . in particular , bac , well recognized as not clinically relevant findings on about 12% of routine screening mammograms of women in their fifth to seventh decade of life [ 6 ] , received attention as being strongly associated with coronary artery disease [ 7 ] [ 6 ]  . 
 consider reasonable to recommend further risk assessment of bacpositive women [ 8 ]  . unfortunately , consistent and reliable methods for bac estimation on mammograms are lacking , making difficult their clinical use for cv prevention . 
previous studies mainly reported bac as present or absent , limiting the discriminant power of a measure on a continuous scale . in this scenario , we evaluated the intraand inter - observer reproducibility of a specifically developed semi - automatic tool for bac quantification on digital mammograms . materials andmethods image selection this retrospective study was approved by the local ethical committee . 
each case had to show in at least one projection in one breast a finding diagnosed as per bac by a radiologist with at least 5 - year experience in mammography . 
such manual bac segmentation represented the reference standard for the training of the semi - automatic system . the algorithm segmented and quantified bac , by providing an estimate of the image surface area occupied by bac , starting from rectangular regions of interest ( rois ) drawn by radiologists . 
the bac surface area was expressed in mm2 , and to help the study logistics , the system allowed radiologists to visualize the mammograms and draw the rois online , through a simple ad - hoc web - based interface . 
inside the rois , the segmentation was fully automatic , so that the only possible source of variability was the rois selection by radiologists . reproducibility assessment ( testing phase ) two residents in radiodiagnostics with more than 6 - month experience in mammography independently positioned the rois to identify the image portions where they recognized bac . 
to standardize the human component of the segmentation method , both operators were intensively trained ( total training time 5h for each of the two residents ) by a radiologist with a 9 - year experience in mammography and by a bioengineer with a 5 - year experience in image segmentation . 
data are reported for the first measurements of observer1 ( o1 , 1 ) and observer2 ( o2 , 1 ) and for the second measurement of observer1 ( o1 , 2 ) where baccc , l and baccc , r represent the respective segmented bac surface on the cc view of the left ( l ) and right ( r ) breasts . 
in the same way , bacmlo , l and bacmlo , r represent the segmented bac surface on the mlo view of the left ( l ) and right ( r ) breasts . statistical analysis shapirowilk test was used to assess the normal distribution of data . 
processed corresponding views with manually positioned rectangular rois containing breast arterial calcifications ( bac ) ( right ) the total bac burden of each analyzed subject , the total bac surface ( bactot ) was calculated as : bactot = baccc , l + bacmlo , l baccc , r + bacmlo , r results 1 3 radiol med ( 2018 ) 123 : 168173 the intra - observer blandaltman analysis showed a bias of 11.9mm2 , a coefficient of repeatability equal to 32.7mm2 for an average bactot measurement equal to 72.8 mm2 and a corresponding reproducibility value of 55% . 
on the other hand , the inter - observer analysis showed a bias of 7.0mm2 , a coefficient of repeatability equal to 61.4mm2 for an average bactot measurement equal to 63.4mm2 and a corresponding reproducibility value of only 3% . 
blandaltman plots are depicted in fig.3. discussion bac are a common finding on mammograms where they appear as linear , parallel opacities , typically described as a tram - track appearance [ 10 ]  . 
although an overall bac prevalence up to 29% has been reported [ 7 ] , they are not commonly described by radiologists in their reports being considered neither suggestive of nor a risk factor for breast cancer . 
the dotted line represents the bias that affects measurement process and the dashed lines represent the limits of agreements between different repetitions ( intra - observer analysis ) or observers ( inter - observer analysis ) a secondary finding on mammograms , no big efforts have been made for standardizing their quantitative evaluation similar to mammographic density . as previously mentioned , a strong association between bac and cv disease has been demonstrated , related to a distinct pathophysiological pathway from the intimal atherosclerotic process [ 12 ]  . 
 [ 7 ] analyzed 10 cross - sectional studies for a total of 3 , 952 women and found a 3.86 odds ratio ( or ) for cad in those with bac versus those without bac . 
considering the established role of screening mammography as a method to reduce breast cancer mortality by over 40% in women who attend a screening program [ 13 ] , a reliable quantification of bac used for cv risk estimation could be an important additional value of screening mammography . 
only results from analyses using a dichotomic ( present / absent bac ) scale were used because quantification methods adopted were largely heterogeneous and not comparable [ 1418 ]  . 
 [ 20 ] developed a technique for quantification of bac using standard full - field digital mammography , demonstrating the feasibility of quantifying vascular calcium mass using densitometry upon calcium calibration on phantom , with an excellent inter - observer agreement . in this study , bac were detected by human readers who selected encompassing rois within mammographic images . 
 being the segmentation within the rois fully automatic , the only possible source of variability of this process was the rois selection and positioning , entirely depending on the reader . 
we can speculate that bac recognition is not a mere matter of higher density findings on the background of breast 1 3 172 radiol med ( 2018 ) 123 : 168173 parenchyma and / or fat . 
as a consequence , developing a computed algorithm for bac detection and quantitative estimation is far from easy . to standardize and reduce operator - dependency , two strongly different strategies are possible . 
 on the other hand , radiologists may define semi - quantitative ordinal scales for severity of bac , similar to the four acr classes for breast density [ 10 ]  . 
moreover , preliminary first attempts for testing this method through long - experienced breast radiologists as observers were made , and a reproducibility even lower ( unpublished data ) resulted . 
in addition , for the specific aim of the experience here described , the two residents underwent an intensive training under a double supervision ( a breast radiologist and a bioengineer , as described in methods ) , with the specific aim of optimizing their reproducibility . in conclusion , our experiment showed a poor reproducibility of a semi - automatic operator - dependent tool for bac quantification . 
however , the apparent association seen between adc values and pmi may be due to contribution of high adc values of mri - invisible tumors rather than reflecting their relationship . keywords cervical cancer parametrial invasion magnetic resonance imaging diffusion - weighted imaging apparent diffusion coefficient likert scale introduction cervical cancer is the second most common cancer in women worldwide [ 1 ]  . 
therefore , several investigators have tested and identified several predictors of pmi ( i.e. , tumor size , depth of stromal invasion , presence of lymph node metastasis ) ; however , most are postoperative pathological variables that are not provided in the preoperative setting [ 3 ]  . 
especially , mri findings such as the intactness of the cervical stromal rim on t2 - weighted imaging ( t2wi ) , known as the hypointense rim sign has shown excellent negative predictive value , ranging from 90 to 100% [ 47 ]  . recently , the apparent diffusion coefficient ( adc ) derived from diffusion - weighted imaging ( dwi ) on mri is gaining interest in oncological imaging . 
up to date , only two studies have addressed the association between adc of cervical cancer and pmi in which it was shown that adc value is significantly lower in cervical cancer with pmi than in cervical cancer without pmi [ 5 , 9 ]  . 
however , adc itself does not directly provide morphological information ( i.e. , extent of parametrial invasion using t2wi ) but rather reflects a functional aspect of the tumor ( i.e. , tissue cellularity and integrity of cell membranes ) [ 11 ]  . 
for example , patients with overt radiological pmi on t2wi , such as nodular extension of tumor into the parametrium , will likely harbor pathological pmi , while those who have an intact cervical stroma on t2wi , are very unlikely to have pmi , no matter how high or low the adc value is . therefore , the purpose of our study was to re - evaluate the value of adc for determining pmi in patients with cervical cancer , by stratifying them into subgroups based on a likert scale using t2wi . materials andmethods patient population we received approval from the institutional review board from our institution with waiver of informed consent . 
using a computerized search of electronic medical records , we identified patients who met the following inclusion criteria : ( 1 ) patients with newly diagnosed cervical cancer , ( 2 ) with figo stages ia2iib , ( 3 ) who underwent preoperative pelvic mri examination , ( 4 ) followed by radical hysterectomy with lymph node dissection from 2010 to 2013 at our institution . 
among the 147 patients initially identified , we excluded the following : ( 1 ) previously underwent conization ( n = 39 ) , ( 2 ) mri protocol did not include dwi ( n = 7 ) , or ( 3 ) dwi performed with b values700s / mm2 ( n = 14 )  . 
prior to image acquisition , 20mg of hyoscine butyl bromide ( buscopan , boehringer ingelheim pharma , ingelheim am rhein , germany ) was intramuscularly injected for bowel motion suppression . 
only the t2wis and dwi with adc maps were analyzed as part of the current study , which were acquired using the following parameters : at 1.5 - tesla , ( a ) t2wi with tr / te , 32174733 / 100108ms ; field of view ( fov ) , 22cm ; slice thickness , 5mm ; intersection gap , 1mm ; matrix , 384224 ; number of excitations ( nex ) , 2 and ( b ) dwi using fat - saturated echo - planar technique with three b values ( b = 0 , 600 , and 1000s / mm2 ) and tr / te , 64508200 / 73100ms ; fov , 30cm ; slice thickness , 5mm ; intersection gap , 1mm ; matrix , 160 160 ; and nex , 24 , and at 3 - tesla , ( c ) t2wi with tr / te , 31194460 / 9095ms ; fov , 2225cm ; slice thickness , 5mm ; intersection gap , 01mm ; matrix , 312307364 ; nex , 12 and ( d ) dwi using fat - saturated echo - planar technique with three b values ( b = 0 and 1000s / mm2 ) and tr / te , 50006250 / 6377ms ; fov , 2530cm ; slice thickness , 5mm ; intersection gap , 01mm ; matrix , 128128192192 ; and nex , 45 . image analysis all images were assessed at a commercial pacs system ( infinitt co , ltd , seoul , korea ) by a radiologist ( syk ) with 10years of experience in pelvic mri , blinded to the clinical information . 
cervical cancer was defined as a focal lesion showing high signal intensity ( si ) on t2wi compared with the normal myometrium corresponding to an area with high si on dwi ( b 1000s / mm2 ) and low si on the adc map [ 5 ]  . 
 the likelihood of pmi was graded on a six - point likert scale based on the intactness of the cervical stromal ring and other ancillary findings ( spiculated tumorparametrial interface , soft tissue extension into the parametrium , encasement of periuterine vessels ) [ 6 , 12 ]  . 
when an apparent tumor was visible on mri , they were given the following scores : 1 , no pmi ; 2 , probably no pmi ; 3 , possible pmi ; 4 , probable pmi ; and 5 , definite pmi . 
after selecting the plane with the largest cross - sectional area of the tumor , a free - drawn region of interest ( roi ) was traced manually on the adc map to include as much of the tumor as possible . 
in patients with no identifiable tumor , rois were carefully placed on the axial plane including the anterior and posterior epithelial linings of the cervix [ 13 ]  . clinical andpathologic data collection the patients electronic medical records and pathology database were reviewed to assess the preoperative and postoperative pathological findings including age , figo stage , histologic subtype , serum squamous cell carcinoma ( scc ) antigen level , and parametrial invasion at final surgical specimens . 
all pathological analysis was performed by two faculty gynecologic pathologists . statistical analysis statistical analysis was performed using spss ( version 21.0 ; spss , inc . , chicago , il , usa )  . 
mri findings ( likert scale for radiological pmi and adc values ) were compared between patients with and without pmi using the linear - by - linear association and mannwhitney u test . 
then , the mannwhitney u test was used to assess whether there were differences in adc between patients with and without pmi stratified to each score group according to the likert scale . 
in addition , to ascertain for the effects of mri magnet strength , we compared the adc values between patients that underwent mri at 1.5and 3 - t scanners with mannwhitney u test in the whole study group and in each subgroup stratified to the presence of pmi . results clinical andsurgical findings of the 87 patients , 19 ( 21.8% ) were identified to have pmi at pathological analysis . 
however , when stratified to the likert scale , no significant differences ( p = 0.1800.857 ) in adc were shown between patients with and without pmi within each score group ( table3 )  . 
especially , when regarding only the 72 patients in which the tumor was visible on mri ( likert scores of 15 ) and , therefore , adc was measured on the visible tumor , there was no significant difference 1 3 212 radiol med ( 2018 ) 123 : 209216 fig . 
on axial t2 - weighted image no definite tumor with high signal intensity is seen in the cervix , whereas the whole hypointense cervical stromal ring ( arrow ) is intact . 
although clinical examination still remains the reference standard for figo staging , the results of the current study further add evidence for mri as a useful tool to identify patients without pmi and , therefore , strengthen the current recommendations that encourages mri in the preoperative assessment of cervical cancer when possible [ 12 ]  . 
because pmi is well known to be associated with clinical features of disease recurrence and survival , assessment of radiological pmi using t2wi will help stratify patients with cervical cancer to receive proper management ( surgery , primary chemoradiation , or adjuvant therapy after surgery ) and help the clinician in predicting postoperative outcomes and counseling the patient [ 2 , 14 ]  . the results of our study demonstrated that the adc value of cervical cancer was significantly different in patients with and without pmi as has been shown in two previous studies [ 5 , 9 ]  . 
 especially , there was no significant difference in the adc values between patients with and without pmi in the patients where adc values were measured on visible tumors , that is , patients with scores of 15 . 
we speculate that this discrepancy can be explained by the following : the inclusion of patients with a score of 0 ( mri - invisible tumor ) , in which none were proven to have pmi on pathology , significantly increased the mean adc values of pmi - negative patients , therefore , rendering a difference in adc values between those with and without pathological pmi . 
the adc values in the subgroup of patients with a likert score of 0 , in fact , are in within the reported ranges adc values of the normal cervix derived using high b values of 800s / mm2 or more ( 1.411.769103mm2 / s ) [ 13 , 15 , 16 ]  . 
in a study of 346 cervical cancer patients with figo stage ib1 , none of those with mri - invisible cancers had pmi at pathological analysis [ 17 ]  . 
furthermore , the quantitative assessments of dwi in terms of adc values have been shown to be comparable when using scanners of different magnet strengths [ 19 , 20 ]  . 
however , the size of the study population is within the sizes of the two previous studies studying the relationship between adc and pmi in cervical cancer : 49 and 117 in the studies by micco etal . 
furthermore , even with this limited number of patients , we were able to raise questions regarding the role of adc as a potential biomarker of pmi in cervical cancer . 
yet , our study is exploratory in nature and , therefore , additional studies , preferably , with a larger number of patients ( especially , those with pmi on pathology ) would be needed to derive more robust conclusions . 
third , our mri protocol at the time of this study did not include an axial oblique which is currently recommended for assessing the local extent of cervical cancer [ 21 ]  . 
however , a recent meta - analysis suggested that the diagnostic performance of mri for parametrial invasion was not significantly different between mri protocols that included axial oblique and sagittal versus protocols that did not include them ; therefore , it is uncertain how this may have affected our study [ 22 ]  . 
in addition , although it was not the primary goal of our study to assess the accuracy of t2wi in determining pmi , using simply t2wi in three orthogonal planes may have affected the proportion of patients within each subgroup of the likert scale . 
although we found no significant differences that may have occurred from different magnet strength ( 3vs 1.5 - t ) , we were unable ascertain the effect of scanner difference ( vendor ) on the value of adc and image quality . 
although this may mirror our clinical practice in the real world , this variability may have affected the results of our study , as some investigators found that adc values can differ when using scanners from different vendors at identical magnet strength [ 23 ]  . in conclusion , a likert scale based on t2wi and adc values showed a significant association with the presence of pmi at pathology . 
however , as there was no significant difference in adc values between tumors with and without pmi in patients with a visible tumor on mri , the apparent association seen between adc and pmi in the whole study population may in fact be due to the contribution of mriinvisible tumors rather than reflect the relationship of adc with pmi . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the aim of this study is to evaluate which haralicks features are the most feasible in predicting tumor response to neoadjuvant chemoradiotherapy ( crt ) in colorectal cancer . materials and methods after mri and histological assessment , eight patients were enrolled and divided into two groups based on response to neoadjuvant crt in complete responders ( cr ) and non - responders ( nr )  . 
a dedicated statistical analysis was performed to evaluate distribution of the extracted haralicks features computing mean and standard deviation . results pretreatment mri examination showed significant value ( p < 0.05 ) of 5 over 14 computed haralick texture . 
 hospital , via franco faggiana 1668 , 04100latina , italy 2 department ofengineering , university ofroma tre , via vito volterra 62 , 00146rome , italy 3 department ofradiological sciences , aoup , via savi 10 , 56126pisa , italy conclusions five haralicks features showed significant relevance in the prediction of response to therapy in colorectal cancer and might be used as additional imaging biomarker in the oncologic management of colorectal patients . keywords t2 - weighted mri colorectal cancer haralicks texture analysis response to therapy introduction early diagnosis and accurate staging of rectal cancer are raising an essential role in the oncologic patients management particularly in personalized treatment strategies . 
the validation of the technique for this purpose has been based on the ability to distinguish normal rectal wall from pathologic tissues on the basis of the high contrast resolution achievable on t2 - weighted sequences [ 3 ]  . 
however , its role in the evaluation of response to therapy is challenging due to the difficulty in discriminating fibrotic to viable residual tissue after neoadjuvant chemoradiotherapy ( crt ) through morphologic approach with t2 - weighted image [ 4 ]  . visual assessment has several limitations compared to quantitative measurements , such as inferior inter - reader agreement due to human eye error [ 5 ]  . 
to overcome this issue , a multiparametric approach [ 6 , 7 ] including t2 - weighted , diffusion - weighted images ( dwi ) [ 810 ] and dynamic contrast - enhanced mri ( dce - mri ) have been proposed [ 11 , 12 ] with improved results but not already optimal to assure a personalized treatment to patients . 
in literature , texture parameters derived from t2 - weighted images of rectal cancer have the potential role as imaging biomarkers of tumoral response to neoadjuvant crt [ 15 ]  . 
 it is possible to extract texture parameters using statistical ( first - order , second - order , and high - order ) , model - based or transform methods [ 16 ]  . 
thus , the purpose of this paper was to determine which of the quantitative parameters extrapolated from haralicks texture analysis most suitable in predicting complete tumor response to neoadjuvant therapy and to evaluate the possible correlation among these parameters . materials andmethods population study this retrospective study involved a sub - cohort of prospectively enrolled patients involved in the italian association for cancer research ( airc ) trial study mr imaging biomarkers in response evaluation to neoadjuvant chemoradiotherapy in rectal cancer i.g. 
all patients had histologically proved colorectal adenocarcinoma and locally advanced tumor stage from ii ( ct3 - 4 , n0 , m0 ) to iii ( ct24 , n + , m0 ) following the uicc 2009 . 
1 flow chart of methodology : data were organized into two categories by visual inspection of radiologists ( 1a and 1b ) ; manual segmentation of complete responder ( 2a , green line ) and non - responder ( 2b , red line ) was performed ; after manual segmentation , each mri was elaborated to extrapolate haralicks texture data ( from 3 to 6 ) 1 3 radiol med ( 2018 ) 123 : 161167 study protocol all patients underwent 3 mri examinations , as have been already extensively described in another study [ 14 ]  . 
due to the specific purpose of this study , we have focused our analyses only on pretreatment oblique axial t2 - weighted mri examinations for the assessment of imaging biomarkers capable to discriminate from responder and non - responder patients prior to the beginning of neoadjuvant therapy . mri examination all mri acquisitions were performed using a 3t scanner ( discovery mr750 , general electrics , milwaukee , wisconsin , usa )  . 
a standard clinical imaging protocol used for rectal cancer study was performed including routinely and dedicated sequences , such as t1 and t2 - weighted with fat saturation / suppression , dwi , adc and dynamic contrastenhanced sequences as described in another study [ 15 ]  . 
for the specific purpose of our study , we analyzed high - resolution t2 - weighted fast recovery fast - spin echo ( 2d frfse ) sequence ( tr , 20864172ms ; te , 11.4122.3ms ; nex , 2 ; slice thickness , 4mm ; matrix , 512512 ) acquired angled to the axial planes orthogonal to the long axis of the rectum to obtain an oblique axial t2 - weighted planes [ 1921 ]  . 
highresolution t2 - weighted images grant an optimal morphologic evaluation by allowing a precise tumor segmentation ; additionally , the texture parameters have a good reproducibility on t2 - weighted as described in literature [ 19 , 22 ]  . texture analysis haralicks texture analysis is a statistical technique , known as the spatial gray - level dependence matrix method . 
as freeborough and fox demonstrated [ 23 ] , a texture discriminant function derived from mri brain scans using a spoiled gradient - echo technique on a 1.5t system gave significantly different values for alzheimer sufferers compared to normal controls [ 17 ]  . two radiologists ( xxx and xxx ) with 7 and 11years of experience in rectal cancer mri evaluation , respectively , performed the segmentation step in consensus . 
 the tumor region has been manually drawn from pre - crt oblique axial t2 - weighted mri image , slice by slice for the entire tumor volume by means of a free open - source segmentation platform ( itk - snap version 4.11.0 ; itk - snap.org ) [ 24 , 25 ]  . 
glcm can be mainly described as an histogram in two dimension that assesses the co - occurrence frequency of two pixel intensities at a specified offset compared to each other over the region where the texture is computed . 
in detail , energy provides knowledge about uniformity of image with a 01 range ( the highest value 1 expresses low variation in image with respect to intensity )  . 
at last , inverse difference moment is referred to as uniformity quantifying the affinity of cooccurrence gray levels [ 26 ]  . table 1 14 haralicks texture features analyzed are described in table1 haralicks texture features energy contrast sum of squares correlation sum average inverse difference momentorhomogeneity entropy sum variance sum entropy difference variance difference entropy information measure correlation1 information measure correlation2 maximum correlation in bold are reported the 5 over 14 features that shown significant results 1 3 164 statistical analysis to evaluate distribution of the extracted haralicks features , statistical analysis was performed computing mean and standard deviation using statistical analysis with spss ( 21.0 ; spss , chicago , il , usa ) and medcalc version 12.7.2 ( medcalc software , ostend , belgium )  . 
dedicated engineers performed a normalization of the glc matrices by taking the neighbor pixel values and reference pixel values paying attention to probability rather than just counting of co - occurrences as suggested wibmer and colleagues [ 27 ]  . 
the wald test from the regression model was performed and p values0.05 were considered statistically significant . results from a total of 90 consecutive patients enrolled in the aforementioned trial , 82 patients were excluded due to : ( a ) histological partial response to therapy ( n = 21 ) ; ( b ) non - completion of the neoadjuvant treatment at the time of the present study ( n = 46 ) ; ( c ) lack of surgical treatment ( n = 2 ) ; and ( d ) lack of histological results at the time of patient selection ( n = 13 )  . thus , the final population consisted of eight patients ( two females , six males , median age 65.5years , range 5878 years ) with locally advanced colorectal adenocarcinoma at tumor stages ii ( ct3 - 4 , n0 , m0 ) and iii ( ct2 - 4 , n + , m0 ) confirmed by preliminary biopsy . 
all patients follow a neoadjuvant crt and after a time - span of 6 - 8weeks , they underwent total mesorectal excision surgery ( tme ) followed by the histological assessment performed by an expert gastrointestinal pathologist . preliminary results on haralicks texture analysis has shown that 5 over 14 features could hire an important role as mri biomarker to differentiate between complete responder and non - responder patients affected by rectal cancer ( all p < 0.05 ) : energy , contrast , correlation , entropy , inverse difference moment . 
2 comparison between complete responder and non - responder haralicks features discussion this paper represents a preliminary technical study on haralicks textural features and the possibly to evaluate the prognostic trend of colorectal cancer with mri semi - automatic image analysis . the t2 - weighted colorectal mri of cr patients showed less disorder and randomness than nr patients imaging . 
 moreover , t2 - weighted images of cr patients have higher energy , inverse difference moment and correlation values , indicating uniformity in image , as well as lower entropy and contrast values , revealing lower randomness and dissimilarity in their gray levels in comparison with nr patients . 
contrariwise , t2 - weighted images of nr patients have higher entropy and contrast , representing higher randomness or disorder and dissimilarity in image gray levels . texture analysis can be included in a wider field of research called radiomics that has the aim to exploit the full potential of medical imaging [ 28 ]  . 
moreover , with the integration of genomics and microarray could built the basis of a wider diagnostic branch called radiogenomic [ 30 ] , a potential powerful tool for clinical decision able to assess , with higher accuracy than each single diagnostic tool , the response to neoadjuvant therapy or the tailored treatment based on the tumor phenotype leading to an overall improvement of patient management . as demonstrated by ng etal . 
recent studies demonstrated that texture parameters derived from t2 - weighted images of rectal cancer potentially might assume a role as imaging biomarkers in detecting tumoral response to neoadjuvant crt [ 14 ]  . 
their capability on reflecting tumor heterogeneity may be further used in clinical practice , integrated to the other diagnostic tools , to improve the selection of tailored patients therapy to avoid under / over treatment that could slow down the care process . 
 haralick analysis has been preferred in our study for the reasons as follow : first , fractal - based texture models are computationally intensive as the model is estimated during the texture extraction process ; second , there is a lack in orientation sensitivity and these models are not suitable for describing local image structures [ 27 ]  . our study has several limitations . 
third , we did not perform a proper 3d volumetric texture evaluation because the software available allows only a single - slice evaluation contrarily to the texture analysis described by wibmer etal . 
more studies are encouraged for a deeper analysis of the topic . conclusion our preliminary results showed that energy , contrast , correlation , entropy and inverse difference moment , are the 1 3 166 radiol med ( 2018 ) 123 : 161167 haralicks features that may have a significant relevance in predicting the response to therapy in patients with colorectal cancer . 
in particular , the association of such imaging features with additional genomics and microarray data can potentially provide a comprehensive overview of tumor characteristics , allowing for an effective targeted therapy and moving towards a personalized treatment in patients with rectal cancer . 
moreover , significant difference ( p < 0.001 ) was shown on comparing the mean volume of the cervical lymph nodes on both sides of the neck in the studied groups . 
no significant differences emerged between the drug - free and treated patients . conclusion the abnormalities shown by ultrasound in cervical lymph nodes are related to deep ones and independent of the ongoing treatment , suggesting a relationship between lymphatic drainage and disease pathology . keywords cervical lymph nodes multiple sclerosis ultrasound introduction the central nervous system ( cns ) has long been considered an privilegedimmunesite or immunologically unique organ , due to the existence of its tight junction - based on bloodbrain barrier . 
however , the studies performed during the last decade have revealed a functional meningeal lymphatic system that drains fluid , macromolecules and immune cells from the cerebrospinal fluid ( csf ) into the regional lymph nodes . 
given this background , cervical lymph nodes are the first drainage stations of the brain and therefore play a key role in both tolerance to self - antigens and adaptive immunological responses in the cns , particularly in vol :  . ( 1234567890 ) 1 3 radiol med ( 2018 ) 123 : 202208 neuroinflammatory disorders such as multiple sclerosis ( ms ) [ 13 ]  . medical history of neurologic disorders ( 10 males and 10 females ; mean age 40.30years ; age range 2763years )  . several neuropathological abnormalities , including brain water edema , swollen axons , degeneration of ganglia , and proliferation of glia , were reported when all cervical lymph nodes were resected and the deep cervical lymphatic vessels were ligated in experimental models of ms [ 4 ]  . 
furthermore , surgical removal of the cervical and lumbar lymph nodes in experimental autoimmune encephalomyelitis ( eae ) of animals reduces brain inflammation and also relapse burden , indicating that lymph nodes may contribute to disease pathology [ 5 ]  . no systematic studies have examined the structural characteristics and clinical correlates of cervical lymph nodes in patients with ms . 
this is quite important considering that some of the most effective ms therapies work by inhibiting lymphocyte transmigration into the cns ( i.e. , natalizumab ) or sequestering them to the lymph nodes ( i.e. , fingolimod ) , suggesting that these lymphatic structures may represent an extension of the brains immunological milieu [ 6 ]  . in the present study , we aimed to characterize invivo cervical lymph nodes in patients with relapsingremitting ms , using ultrasound imaging , and to ascertain if patients have any corresponding and distinguishing clinical features . materials andmethods study design between september 2015 and june 2016 , 52 patients affected by relapsingremitting ms ( rrms ) were recruited by the neurological clinic and had ultrasound examination of the deep cervical lymph nodes at the department of diagnostic imaging . the inclusioncriteria were : males or females between 18 and 50years , with confirmed and documented diagnosis ofrrms according to the revised mcdonald criteria , in treatment with natalizumab or fingolimod ( dmt - treated ms group ) for at least 6 months ordrug - nave . exclusion criteria included patients who had : ms relapse or treatment with corticosteroids within 30days prior to neuroradiological examination ; symptoms and signs of acute / recent infections ; previous history of neck pathology or any other known disease that might affect the lymphatic tissue . in accordance with the above - mentioned criteria , the patient group was composed of 43 patients , of whom 22 ms patients were drug free ( 11 males and 11 females ; mean age 39.68years ; age range 2759years ) and 21 were in the dmt - treated ms group ( 10 males and 11 females ; mean age 40.05years ; age range 2554years )  . the demographic and clinical data of the enrolled subjects are reportedin table1 . at the time of enrollment , all subjects underwent a clinical and neurological evaluation that included the expanded disability status scale ( edss ) , a ten - point disease severity derived from nine ratings for individual neurological domains . 
on the basis of ongoing therapy , patients with ms were divided into two subgroups : drug - free patients ( f - ms ) and dmt - treated ones ( t - ms )  . this observational and retrospective study was approved by the institutional review board ; moreover , it was in accordance with the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . 
all the ultrasound data in this study were collected by the same neuroradiologist ( fdg ) with more than 5years of experience in ms and ultrasound imaging , following standardized protocols for data acquisition under the supervision of sm ( 25years of experience in ultrasound imaging andms )  . all levels of both sides of the neck were fully examined for the presence of lymph nodes , which were classified by site following robbins level . the morphology , diameters [ axial , longitudinal and anteroposterior ( ap ) ] and volume of the lymph nodes visible on us were measured . 
also , we calculated an average index of the lymph nodes short axis ( anteroposterior diameter ) and volumes ( on right and left side ) ( figs.2 , 3 , respectively ) , which are more significant measurements in accordance with literature . 
in the 1980s suggested the hypothesis of a physical connection between the csf and the perivascular space in the cns , by injecting a tracer into the csf [ 7 , 8 ]  . 
demonstrated the presence of a particular kind of system that they named glymphatic system , which seems to clear interstitial solutes in the brain through the exchange of csf and isf along the pathway composed of vein walls and astrocytic cells [ 10 , 11 ]  . 
in the early twentieth century , it was demonstrated that the csf drains into the deep cervical lymph nodes via the cribriform plate into the lymphatic system of the nasal mucosa [ 1217 ]  . louveau and aspelund in 2015 discovered the existence of the functional lymphatic system located in the dura mater which is ableto drain fluids , macromolecules and immune cells to deep cervical lymph nodes [ 18 , 19 ]  . 1 3 radiol med ( 2018 ) 123 : 202208 fig . 
1 ultrasound examination of lymph node in robbins level iia in patient with multiple sclerosis : note the increased volume of the lymph node with recognizable hilus on the right ( a ) and left side ( b )  . 
ltc laterocervical region in experimental animals with resected lymph nodes , or ligated lymphatic vessels in the neck , were associated with several neurological abnormalities such as increased csf pressure , hydrocephalus , swollen axons and degeneration of ganglia such as those of the optic nerve [ 4 ]  . 
these results seem to reinforce the hypothesis that a communication probably exists between the cns structures and the lymph nodes of the neck region . moreover , two independent studies have demonstrated the presence of a functioning conventional lymphatic vasculature in the meninges , which is able to drain macromolecules and immune cells from the meningeal spaces and brain parenchyma into the deep cervical lymph nodes [ 20 , 21 ]  . these lymphatic vessels , along the dural sinuses , have similar characteristics to the known lymphatic vessels in the rest of the human body , but , at the same time , have a different anatomical distribution probably attributable to the high csf pressure in the cns with respect to the interstitial fluid pressure of the other regions of the body . this new kind of lymphatic vessels seem to be able to carry fluids and immune cells from the cerebrospinal fluid to the deep lateral cervical lymph nodes , as shown in rats by injecting a dye that was subsequently detected both in the 1 3 206 radiol med ( 2018 ) 123 : 202208 lymphadenopathy could influence the physiopathology of neuroinflammatory disorders such as multiple sclerosis . the current therapeutic protocols in ms are focused on the immunomodulatory action of drugs such as natalizumab and fingolimod . therefore , the aim of our study was to evaluate if there were any differences in the morphology and size of the lymph nodes in the two groups of ms patients ( naive and dmt )  . 
no statistically significant difference was detected in the volume and the short axis of lymph nodes between the two groups , while there was a significant difference in volume and short axis between patients with ms and the control group . 
this result seems to confirm the hypothesis that somehow there could be a particular connection between the cns and laterocervical lymph nodes , in particular with the iia level of robbins . 
this seems to reinforce the hypothesis of the role of lymphatic drainage in the physiopathology of neuroinflammatory disorders such as ms . in particular , we found a statistically significant increased volume of the first lymph node in iia level of robbins bilaterally . in addition , the solitary increased volume of the first lymph node at level iia , and not in the remaining axillary and inguinal lymph nodes , underlines the specific role of the deep laterocervical lymph nodes in the lymphatic drainage of the brain and probably in the pathogenesis of the disease . this resultissupported and reinforced by the analysis of the axial ( ap diameter ) of the lymph node , because the short axis of the lymph node is considered more indicative of the pathophysiological changes according to literature [ 22 ] and it is increased in our patients with ms . moreover , our results are consistent with those of o . 
this seems to be in agreement with the presence of cns antigens in deep cervical lymph nodes also in experimental autoimmune encephalomyelitis as well as in stroke , so that it can be argued that cervical lateral lymph nodes represent a site of activation of cns specific t cells [ 28 ]  . another characteristic data , evidenced by our study , is the increased hypoechoicity of lymph node at level iia that could be referred to greater cellularity , as well as to increased inflammatory activity . on further evaluation with the color doppler module , all the lymph nodes that we examined had a recognizable hilus . the present study has few limitations . 
2 the box - and - whisker plots show the distribution and median value of the anteroposterior diameter of the lymph nodes , respectively , at level iia of robbins on the left side in the case and control groups fig . 
3 the box - and - whisker plots show the distribution and median value of the anteroposterior diameter of lymph nodes , respectively , at level iia of robbins on the right side in the case and control groups meningeal vessels and in the cervical lymph nodes [ 18 ]  . 
for that reason , the meninges seem to be essential immunological sites that allow cns immune surveillance to function correctly [ 13 , 20 , 21 ]  . all these discoveries have paved the way for new research studies to assess how the lymphatic system and 1 3 radiol med ( 2018 ) 123 : 202208 fig . 
this value was higher in drug - free patients with ms than those under treatment conclusion our study provides the first invivo evidence of subtle cervical lymph node enlargement in patients with ms compared to ageand sex - matched controls , using ultrasound evaluation . 
moreover , these abnormalities are specifically related to the deep cervical nodes and independent of the ongoing treatment , suggesting a strong relationship between disturbed cns lymphatic drainage and disease pathology . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . funding this study has not received grant or funding . informed consent vidual participants included in the study . informed consent was obtained from all indifig . 
5 the box - and - whisker plots show the distribution and the median value of lymph nodes in our studied groups split up by category and side the second limitation concerns the ultrasound examination which is related to the performer : however , we have overcome this limitation by performing the ultrasound examination by the same physician . nevertheless , on the other hand , this is the first study which has showed , in vivo , that deep cervical lymph nodes have increased volume and anteroposterior diameter . 
all scan data were retrieved by our pacs ( picture archiving and communication system ) by means of a dose monitoring software . results among the variables we considered , no significant difference of radiation dose was observed among patients of different ages nor concerning tube voltage . 
we quantified and analyzed the most relevant variables in order to provide a useful tool to manage properly ct dose variability , estimating the amount of additional radiation dose for every single significant variable . 
additional scans , incorrect scan length and incorrect usage of aec system are the most relevant cause of patient radiation exposure . keywords computed tomography radiation exposure lymphoma dose optimization surveillance radioprotection introduction ct scanning represents a fundamental diagnostic tool for radiologists and its utilization has become ubiquitous in medicine [ 1 ]  . 
many technical developments , such as faster scan times , improved spatial resolution , and multiplanar and tridimensional reconstruction techniques , have increased the usefulness of ct for almost every anatomical disease [ 2 ]  . 
as a consequence of the increased use of computed tomography , the average radiation dose in the population is dramatically increased over the last three decades , with an approximately sevenfold increase in radiation exposure [ 3 ]  . 
hence , there is a rising concern about the risks for patients undergoing multiple ct examinations and other x - ray imaging modalities , with a specific attention to young adults and children who are much more vol . : ( 0123456789 ) 1 3 192 radiol med ( 2018 ) 123 : 191201 sensitive to the radiation damage [ 46 ]  . 
to contain this raising trend in radiation dose , many initiatives have been taken by different national and international organizations , institutions and radiological societies [ 79 ]  . the attention must be paid in particular on oncologic imaging : patients are often exposed to multiple whole - body ct examinations , which are justified by the medical need to stage the tumor , to assess the response to treatment and to promptly identify malignant tumor recurrence . 
whereas these multiple ct examinations are not a cause of concern for patients with advanced cancers , the appropriate use of ct and related risk in patients affected by cancers with favorable prognosis and with a long life expectancy , is under debate . 
in addition to appropriateness considerations about the use of ct examinations in oncology , specific attention must be paid to the choice of the right timing of the repeat examinations . 
indeed , depending on the clinical protocol , many oncologic patients may be exposed to several ct examinations every year , which causes an increase of the cumulative radiation amount they are exposed to [ 13 , 14 ]  . 
another important issue is the utilization of optimized technical parameters such as limiting the examination to the involved anatomic area , choosing the right value of the tube current and the tube voltage . 
previous papers have demonstrated that the lack of optimization criteria as well as the lack of knowledge about radiation protection issues and technical procedures can cause an unjustified radiation overexposure in patients who undergo ct examinations [ 1518 ]  . 
despite several studies that compare the role of the different approaches for follow - up in patients affected by lymphomas [ 19 ] , use of ct in follow - up of lymphomas remains largely diffuse . 
the identification of the best approach to identify tumor spread or recurrence in lymphomas is still under debate and it is beyond the objectives of this article . the aim of our study is to assess the radiation dose indices of ct imaging studies , performed in a group of young adults patients affected by lymphoma , by detecting the influence of different scan parameters during repeat ct examinations , and by considering which technicians and radiologists behaviors might be involved . materials andmethods patient enrollment informed consent was obtained from all participating patients . 
for each patient we considered only the repeat ct examinations , which were performed during treatment and follow - up , excluding the first staging exaonly patients who underwent three or more repeat ct examinations on the same ct equipment were included in the study . ct equipment all ct examinations were performed on a 16 - raw detector ct scanner ( toshiba medical system ) at the same radiological institution . 
ct examinations were performed by six different technologists ( i.e. , radiographers ) supervised by five different radiologists . study design the study was pilot and observational ( cohort type ) in a repeated measures framework . 
primary outcome was the radiation index , i.e. , the dose length product ( dlp ) of entire ct examination ( measure ) , while the secondary outcome was the dlp concerning only a venous phase for each ct examination . 
in addition , other variables such as sex , age , scan length , abdominal diameter , tube voltage ( kv ) , use of aec system and numbers of acquired scans were revealed . 
the blocks of the ct examinations were unbalanced , that is , not all subjects were submitted to six examinations . data collection data were retrieved from our picture archiving and communication system ( fujifilm , synapse 4.0 , japan ) using a radiation dose monitoring software ( total quality monitoring system , qaelum , belgium )  . 
for each patient , age at the time of performed exam , sex , computed tomography dose index ( ctdivol ) , dlp , kv value , use of aec system , scan length , number of performed scans , and abdominal diameter were recorded . 
the dose monitoring software tool was also used to verify the constant patient positioning inside the gantry throughout the repeat ct examinations . 1 3 radiol med ( 2018 ) 123 : 191201 statistical analysis descriptive statistics are expressed as mean standard deviation for continuous variables and frequencies for categorical variable . 
concerning that , we performed two kruskalwallis tests on both total dlp and dlp of a venous phase , to assess the variability due to the technologists behavior , for each block of ct examination . 
in these tests , statistical significance was set at p value < 0.05 and non - normality distributions were checked by shapirowilk tests . thus , to evaluate the fixed effects ( ) of each potential involved factor ( predictors ) , detached linear mixed models ( lmm ) were fitted on both outcomes ( i.e. , total dlp and dlp venous phase ) [ 20 ]  . 
two hierarchical random effects ( intercept type ) , on the subjects and nested on the technologists , were also included in the models to manage the hierarchical data structure due to the repeated measures and technologists rotation across the ct examinations . 
because both outcomes did not follow a normality distribution ( checked by shapirowilk test ) , bootstrap estimations were used and the model coefficients ( ) were tested by bootstrap 95% confidence intervals ( percentile type ) ( 95%cib ) , i.e. , when = 0 was not included in the intervals , the coefficient was significant . 
in this way , the coefficient was more significant when 95% cib was more distant from 0 . moreover , to detect multicollinearity and potential measured confounders , the pairwise associations between potential involved factors were also evaluated through linear regression models or fishers exact test , as appropriate if response variables were continuous or dichotomous . 
 regarding the former , bootstrap estimations were performed , whereas for the latter odds ratios ( or ) for small samples ( or achieved by conditional maximum likelihood estimation ) [ 21 ] , p values and 95% cis were computed . 
statistical significance was set at p value < 0.05. we also performed two detached multivariable lmms on both outcomes to evaluate the conditional effects ( ) of the potential involved factors . 
at this stage , the fixed effects of the predictors on the outcome variables were conditional , that is , we obtain the expected outcome variation per unit increase of predictor , keeping fixed the others in the built - in model . 
for each multivariable lmm , coefficients of determination ( r2 ) were also computed ( as goodness of fit measure ) as 1 minus fraction of residual variance ( i.e. , bootstrap residual variance divided by outcome total variance )  . 
the analysis was performed on r 3.2.2 [ 22 ] using the r / lme4 [ 23 ] and r / boot [ 24 ] packages . results preliminary analysis in table1 descriptive statistics concerning the observed variables are reported , which were sex , age , scan length , abdominal diameter measurement , kv selection , utilization of current modulation and number of acquired scans . 
in the lower section of the table are reported the outcomes of the study which are the radiation dose indices concerning a single venous phase and the entire ct examination . 
moreover , table2 highlights that , within each measure , the kruskalwallis tests on both total dlp and venous phase dlp returned non - significant results , i.e. , there were no differences across technologists . 
in other words , on both total dlp and dlp venous phase , the dose delivered to the patient is the same whatever the technologist performed in the ct examinations ( 1st ct , 2st ct , 3st ct , 4st ct , 5st ct or 6st ct )  . table3 shows the effects of potential involved factors on the dlp values , in terms of crude bootstrap ( or md ) , adjusted only for the subject and technologist random effects . 
notably , the number of scans factor was not considered for venous phase as it was the only phase performed . we also considered the association among predictors , which are shown in table3 . 
these are included following a model selection procedure and using a forward strategy by adding predictors with significant effects to the null model . table4 shows the fitted models , the final model is considered that model where all remaining variables are statistically significant . 
at this stage , the effects of the predictors on the outcome variable are conditional , i.e. , expected outcome variation per unit increase of predictor , keeping fixed the others in the built - in model . 
therefore , we note that modulation , sex , number of scans , abdominal diameter and scan length continued to be significantly involved factors in the multivariable lmm , too . 
therefore , a model selection procedure like before has been performed . table5 shows the fitted models , the final model is considered that model where all remaining variables are statistically significant . 
these new directives aim to reduce the increasing population dose and to permit a better consciousness and communication between radiologists and patients , and finally to guarantee a better patient care . 
particularly , this has to be done in those patients who are young at the time of the diagnosis and undergo multiple ct examinations , 1 3 radiol med ( 2018 ) 123 : 191201 such as patients affected by lymphoma . 
although it is still controversial , some authors also demonstrated that patients affected by lymphoma , especially the ones with low - grade disease and long life expectancy , have an increased risk to develop a second solid tumor due to the radiation dose received in the occasion of the performed radiological imaging procedures [ 25 , 26 ]  . 
some other recent studies show that patients receiving eight or more cts have a twofold increase in secondary primary malignancies and this risk is dose - dependent [ 27 ]  . 
considering that these patients often undergo procedures such as radiotherapythat surely have a more important role in terms of absolute dose administeredthe imaging radiation dose is not probably the predominant increasing risk factor ; however , it is definitely one of them on which we could effectively intervene . 
therefore , this study aims to provide some useful tools to acquire more consciousness about how radiologists ( and consequently technologists ) behavior might affect the final radiation dose of the single exam to obtain a good optimization . our results clearly demonstrate a variability of the radiation dose delivered to patients affected by lymphoma during repeat ct examinations . 
accounting for this , to the best of our knowledge , our work is the first study that intends to measure how the behavior of technologists and radiologists may affect the radiation dose delivered to oncologic patients . 
in fact , several strategies can be adopted to reduce radiation associated with ct , such as limiting the examination to the requested anatomic area , optimizing scanning parameters and avoiding multiple scans when clinically unnecessary [ 28 , 29 ]  . 
this aspect is definitively important when patients undergo repeat ct examinations , as one of the main goals should be avoiding unjustified variability in radiation exposure . although it was expected that young patients were exposed to a lower radiation dose as a consequence of a specific attention of the operators when performing ct exams , no significant difference was observed concerning different ages of patients . 
thus , it is mandatory to persist in educating the entire radiological team to adapt the scan technique to the patients age for their well - known higher vulnerability due to their more radiosensitive tissues [ 30 , 31 ]  . in our study the preliminary results obtained through a univariate analysis anticipate the evidence emerging from the final models presented in fig.1 , which schematically summarizes the significant study results . 
despite several physics and clinical studies have demonstrated various levels of dose reduction using lower tube voltage [ 32 , 33 ] , on the basis of the multivariate analysis we found no significant difference of the radiation dose indices depending on the tube voltage ( 100 and 120kv )  . 
this probably is due to the specific automated exposure control ( aec ) system available on our ct scanner : reducing tube voltage from 120 to 100kv results in an increase of the ma value which tends to keep almost unchanged the overall radiation dose index . 
nevertheless , it is important to emphasize that the reduction of kv settings might be also useful to limit the amount of administered contrast medium and this aspect is also particularly relevant in oncologic patients who undergo several contrast - enhanced ct examinations [ 34 ]  . there are different factors that mostly vary the dose delivered to the patients . 
some of them are independent from the radiological teams behavior , such as sex and abdominal size ; others might be influenced by the settings of protocol and the scan parameters , and they are scan length , usage of aec system and number of performed scans . 
they tend to receive more radiation dose due to the longer scan length , the greater body mass and the larger abdominal size , which determines a higher ma value automatically set by the aec system . with our analysis , we are able to quantify the increase of the dlp value for each centimeter added to the scan length . 
 a previous work published by zanca and co - workers showed that in a substantial number of patients ( about 80% ) , ct data are acquired beyond the real area of interest , leading to excessive effective and organ doses [ 35 ]  . 
this information must be carefully taken into consideration by radiographers and it outlines how important it is to limit the scan length to the anatomic boundaries , avoiding unnecessary radiation exposure . concerning the abdominal size , it markedly influences the amount of the radiation dose delivered to the patient . 
despite this aspect is largely dependent on the body dimension of the patient , radiographers can limit the radiation exposure of bigger patients by choosing the most appropriate parameters settings , i.e. , assessing together with radiologist if it is possible lowering the radiation dose and accepting a higher image noise . 1 3 200 radiol med ( 2018 ) 123 : 191201 on the basis of our results , it is evident that deactivating aec system causes a significant increase of the radiation exposure . 
in fact , when aec is switched on and properly adjusted , it leads to a significant reduction of the radiation dose ( 731.29 mgyxcm for total examination and 307.95 mgyxcm for single venous phase )  . 
it is mandatory to emphasize the importance of centering the patient accurately within the ct gantry , as a miscentering may impair a correct functioning of the aec software [ 36 , 37 ]  . 
we strongly encourage users to take advantage of these technical tools for reducing radiation dose while maintaining diagnostic image quality . we found that the most significant variable influencing the radiation dose during repeat ct examinations was the number of performed scans for each ct examination . 
taking into account that all exams included in this study have been performed in the same institution and on the same ct equipment , there is an unjustified excess of variability of ct scanning protocols adopted by the different radiologists . 
part of this radiation dose variability can be partially explained by the complexity of the clinical situations and also by the different confidence of the single radiologist in detecting recurrence or relapse disease only by means of the venous phase . 
however , it is fundamental to ponder properly the necessity of eventual additional phases and consider carefully the riskbenefit balance taking into account the amount of additional dose that a new scan adds to final radiation exposure as shown in our results , especially in younger patients . 
so , it is mandatory to find a standardized and shared ct protocol to avoid unnecessary phases , and the consequent increase of radiation - related risks . finally , in this study we did not find any significant difference in radiation dose delivered by the different technologists within each measure , while the observed dose variability is highly influenced by the radiologists behavior in terms of number of scans performed . our work has some limitations . 
then , the small population and the restricted area ( a single institution ) we considered may represent a limitation of our work . conclusions in summary , our findings demonstrate that patients affected by lymphoma who undergo repeat whole - body ct examinations may receive unnecessary radiation dose due to an incorrect settings of ct protocols . 
in this study , we quantified and analyzed the radiation dose identifying its most relevant variables to provide a useful tool to manage properly ct dose variability , estimating the amount of additional radiation dose for every single significant variable , including specific settings of each scan parameters . 
such considerations are increasingly relevant given the growing attention on general population dose , the new euratom directives about radioprotection and underline the fundamental need of shared and standardized ct protocols . 
in our experience , cases with atypical pulmonary sarcoidosis patterns evaluated in the study are consistent with similar cases described in the literature , both in lymph node and atypical parenchymal involvement . 
all the atypical characteristics of the work should alert the radiologist to consider sarcoidosis among the possible differential diagnoses , always correlating the results of the computed tomography examination with appropriate clinical - laboratory evaluations . keywords sarcoidosis high - resolution computed tomography diagnosis atypical manifestations differential diagnosis introduction sarcoidosis is an idiopathic systemic granulomatous disease of unknown aetiology and it is characterized by noncaseous epithelioid cell granulomas and fibrotic changes in tissue architecture . 
in 90% of patients , there is a pulmonary involvement associated with mediastinal hilar lymph node enlargement , but the disease may also involve skin , eyes , liver , heart , and brathe diagnosis is based on a correct clinicalradiological evaluation and histological demonstration of non - necrotizing , non - caseous epithelioid granulomas . 
 the sarcoidosis differential diagnosis includes all principal granulomatous disorders such as tuberculosis , leishmaniosis , whipple disease , tularaemia , fungal disease , and non - infective granulomatous diseases ( hodgkin and non - hodgkin lymphomas , sarcomas , silicosis , berylliosis , hypersensitivity pneumonitis , vasculitis , blau syndrome , and others )  . 
although the diagnosis of sarcoidosis generally requires histological confirmation , in patients with suspect sarcoidosis , the high - resolution computed tomography ( hrct ) of the chest plays a relevant role to identify the lung involvement , with a higher sensitivity and specificity than chest x - ray ( cxr ) [ 3 , 4 ]  . the classical staging of the disease , developed by siltzbach , was developed before computed tomography ( ct ) introduction [ 5 ]  . 
nowadays , hrct is the gold standard for the detection and characterization of parenchymal abnormalities and it helps to better characterize the interstitial pulmonary involvement . pulmonary sarcoidosis may manifest with various radiological patterns : a typical pattern consists of small nodules along the lymphatics in the peribronchovascular interstitial space and in the interlobular septa ( with peri - lymphatic distribution ) , evolving in interstitial lung involvement [ 2 , 6 , 7 ]  . the typical radiological hrct manifestations of sarcoidosis include hilar and mediastinal lymphadenopathies , usually symmetrical , bilateral ( with sub - carinal involvement ) , and well defined ; in addition , nodules are commonly rounded , well defined , and measure 25mm in size . 
fibrotic alterations may occur in 2025% of cases : classic fibrotic changes include linear opacities and reticulation , interlobular septa thickening , bronchovascular distortion ( traction bronchiectasis ) , and reduction of lung volumes . hrct of chest helps to reach a diagnosis of sarcoidosis in typical clinical contexts , such as in case of lfgren syndrome , where there is the triad of intrathoracic lymphadenopathy , erythema nodosum , and arthritis . 
 it can differentiate reversible and irreversible sarcoidosis abnormalities that may represent different phases and activity levels in the disease ( irreversible fibrotic alterations , such as honey combing , express a chronic persistent fibrotic process rather than an acute inflammation ) [ 4 , 8 ]  . usually , 2530% of patients develop an unusual sarcoidosis with non - specific radiological pattern . 
these patterns are various and the signs are reported with different frequencies in the literature [ 2 , 4 , 6 , 7 , 9 , 10 ] ( table1 )  . the aim of this study was to report some atypical hrct patterns of sarcoidosis evidenced in our population of patients , focusing on the differential diagnosis to contribute to the difficult role of the radiologist in the disease identification and to help the clinicians to reach the diagnosis . materials andmethods we retrospectively reviewed the imaging of 308 patients referred to a regional referral centre for interstitial lung diseases since january 2016 . 
all these patients were table 1 typical and atypical patterns in pulmonary sarcoidosis at hrct typical features nodules with lymphangitic spread in the peribronchovascular interstitial space and in the interlobular septa bilateral , symmetric hilar and mediastinal lymphadenopathy fibrotic alterations : linear opacities and reticulation , interlobular septa thickening , bronchovascular distortion ( traction bronchiectasis ) and reduction of lung volumes predominant upper - middle lobes atypical features atypical patterns of lymphadenopathy : isolated , unilateral , with calcifications pulmonary nodules and masses : confluent alveolar opacities , mass - like opacities interstitial fibrotic alterations and fibrocystic changes : bullae , cysts , honey - comb opacities in the upper - middle lung zones , emphysema ground - glass opacities pleural involvement : pneumothorax , effusion , pleural thickening linear opacities : interlobularintralobular septal thickening halo - sign airway involvement : atelectasis , mosaic - attenuation pattern , tracheo - bronchial alterations 1 3 176 radiol med ( 2018 ) 123 : 174184 diagnosed according to international ats / ers / wasog criteria [ 11 ]  . 
inclusion criteria were a diagnosis of sarcoidosis established by histopathology , an hrtc study performed at the time of diagnosis , and a 6 - month / 1 - year clinical and radiological follow - up . 
according to the hrct pattern , three single experienced radiologists classified the patients into two different groups as being affected by typical or atypical pulmonary sarcoidosis ( see table1 ) and they radiologically define the predominant pattern of presentation : in case of discordance , a consensual agreement was reached . results in total , 47 patients were enrolled : 29 ( 61.7% ) showed a typical pulmonary pattern and 18 ( 38.3% ) an atypical pattern . 
only one patient ( 5.5% ) had fibrocystic changes ( bullae , pulmonary cysts , and paracicatricial emphysema ) , 1 patient ( 5.5% ) had halo - sign , 1 patient ( 5.5% ) presented itself with diffuse and bilateral ground - glass opacities , and 1 patient ( 5.5% ) had an isolated lung mass . 
moreover , three patients ( 16.6% ) with atypical lymph node pattern ( such as asymmetric - isolated lymphadenomegaly or egg - shell - like lymph nodes calcification ) were also found . hrct atypical patterns atypical patterns oflymphadenopathy asymmetric , isolated , or unilateral lymph nodes are uncommon in sarcoidosis , especially in young patients . 
since 1967 , when jacobsen and felson established the criteria for diagnosing of egg - shell - like calcifications , more and more diseases have been described presenting this manifestation , especially silicosis , histoplasmosis , and tuberculosis [ 12 ] ( table2 )  . 
microcalcifications of hilar lymph nodes are also rare and they express a chronic disease . in our population , all the patients presented chronic persistent sarcoidosis and it was observed one or more extrapulmonary localization . 
pulmonary lesions and mediastinal lymph node interest were present at the onset , while the egg - shell - like lymph node calcifications were observed after 6years from the diagnosis . 
the disease required at the beginning an immunosuppressive therapy ( methotrexate ) , but recently , low - dose steroid therapy is sufficient to obtain a control . pulmonary nodules andmasses sarcoidosis can involve alveoli and airspaces determining lung consolidations and conglomerate masses distributed table 2 egg - shell - like calcifications : diseases and differential diagnoses disease presenting thoracic egg - shell - like calcifications silicosis sarcoidosis sclerodermia blastomycosis differential diagnosis of thoracic egg - shell - like calcifications aneurysms pulmonary arteries thyroid tumours treated lymphoma pneumoconiosis amyloidosis histoplasmosis parathyroid tumours thymic cysts multinodular goitre 1 3 radiol med ( 2018 ) 123 : 174184 represent reversible lesions that sometimes can improve after therapy ; they correspond to the confluence of numerous micronodules and they are associated with acinar or alveolar sarcoidosis . 
 the lesion was positive at radionuclide imaging ; in this case , 18f - fluorodeoxyglucose positron emission tomography ( 18fdg - pet ) and the biopsy demonstrated nonnecrotizing granulomatous inflammation compatible with sarcoidosis . 
1 enlarged lymph nodes with egg - shell - like mediastinal calcifications in a patient with pulmonary chronic sarcoidosis ( maximum intensity projectionmip - coronal reconstruction ) in the peribronchovascular areas of the upper and middle lung . 
the lesion was positive at radionuclide imaging ; in this case , 18f - fluorodeoxyglucose positron emission tomography ( 18fdg - pet ) and lung biopsy demonstrated non - necrotizing granulomatous inflammation compatible with sarcoidosis . 
the honey - combing - like cysts in a patient with stage iv sarcoidosis , with a radiol med ( 2018 ) 123 : 174184 ct pattern mimicking chronic hypersensitivity pneumonia ( hp ) pattern , were evidenced in the figure and they were associated with an asymmetric lung involvement . 
 however , the same pattern can be seen in bronchiolo - alveolar carcinoma , lymphoma , pneumoconiosis , pneumonia , and bronchiolitis obliterans organizing pneumonia ( boop ) [ 6 ]  . the patient represented in fig.6 has a diffuse and symmetric ggo in both lungs . 
the patient in this case is a ceramist smoker man : his diagnosis was made when he was 50years , pft showed mild obstruction associated to a mild decrease of dlco . 
a , b sagittal reconstructions of right and left lung ; c axial ct scan of both apexes 1 3 179 radiol med ( 2018 ) 123 : 174184 fig . 
5 a axial and b coronal ct scans show diffuse fibrotic alterations without predominance of upper - middle lobes , associated with areas of oligoemia ( that is called mosaicattenuation pattern )  . 
axial and coronal ( d ) ct follow - up after 1month of steroid therapy cough and dyspnoea , and she presented normal pft with a mild decrease of dlco . 
serum chitotriosidase was highly increased , and an invasive diagnosis ( ebus - tbna ) allowed to exclude cryptogenic organizing pneumonia ( cop ) and infective disease . fibrocystic changes cystic pattern is composed by round air - containing parenchymal spaces with a well - defined wall ( usually the wall is thin , < 2mm ) [ 15 ]  . 
fibrotic alterations coexisted in this patient with consolidate areas and bilateral bronchiectasis . linear opacities in some patients with sarcoidosis ( 50% of cases ) , an isolated linear reticular thickening involving the subpleural areas of the upper - middle lung can be observed [ 6 ]  . 
7 axial ct scan in a woman with stage iv sarcoidosis shows a large cystic space in left lower lobe pleural involvement in a limited patients population ( approximately 14% ) [ 10 , 17 ] , sarcoidosis can determine pleural involvement with inflammatory thickening and calcifications as well as with bilateral plaque - like opacities formed by conglomerations . 
8 this young woman has an end - stage sarcoidosis with diffuse fibrocystic changes ( cysts , bullae , and honeycombing ) associated with confluent opacities corresponding with airspace consolidation . 
10 axial ct scans in a and b show an interlobular intralobular septal thickening determining a diffuse reticular pattern in both lungs , with no predominance of upper and middle lobes . 
in fact , aspergillus ( or other saprophytic fungi ) can colonize these parenchymal cavitations in less than 5% of patients with advanced fibrotic involvement [ 2932 ]  . 1 3 radiol med ( 2018 ) 123 : 174184 182 fig . 
12 a axial and b coronal ct reconstructions show a patchy fibrotic involvement in peribronchovascular zones and middle - upper lobes , associated with mosaic - attenuation pattern and ground - glass opacities . 
this patient was a 68 - year - old neversmoker woman with a restrictive pulmonary syndrome : the severe reduction of dlco required prolonged methotrexate and steroid treatment discussion the atypical radiological findings in patients affected by sarcoidosis represent a diagnostic challenge for the radiologist as well as for the clinicians . 
sarcoidosis may simulate different lung diseases on ct imaging such as lymphangitis carcinomatosis , hypersensitive pneumonia ( hp ) , pulmonary langerhans cell histiocytosis ( plch ) , or uip : such variable radiological characteristics of pulmonary involvement should alert the radiologist to consider sarcoidosis in the differential diagnosis . 
in fact , sarcoidosis is considered the great mimic [ 7 ] , because its uncommon radiological features may be mistaken with other lung disease such as tuberculosis , pneumoconiosis , cancer , or metastatic disease . atypical manifestations , such as honey - comb - like cysts and fibrocystic changes , halo - sign , mosaic - attenuation pattern , military opacities , or pleural disease ( pneumothorax , effusion , and pleural thickening ) , have been reported mainly associated with a peculiar clinical phenotype . 
hrct atypical features have been associated with older age ( patients with more than 50years ) and smoking history [ 34 ]  . hrct of the chest plays a fundamental role in the diagnostic work - up and in the follow - up of patients with sarcoidosis . 
the imaging plays an important role also in the identification of high - yield sites for trans - bronchial or surgical lung biopsy , to guide the bronchoscopist [ 4 , 6 , 8 ]  . 
high - resolution computed tomography ( hrct ) is the gold standard for the detection and characterization of parenchymal abnormalities and it helps to better characterize the interstitial pulmonary involvement . 
 furthermore , hrct helps to differentiate an active inflammation ( reversible abnormalities , such as consolidation , nodules , and septal thickening ) from an irreversible lung fibrosis ( honeycombing , cysts , and traction bronchiectasis ) and helping to choose the appropriate therapy especially in patients with stage 2 or 3 sarcoidosis [ 4 ]  . 
radionuclide imaging , especially 18f - fluorodeoxyglucose positron emission tomography ( 18fdg - pet ) , is recently required in many cases and may be helpful to assess the activity of the disease [ 37 ]  . the imaging plays a fundamental role in the diagnosis and management of patients with pulmonary sarcoidosis . 
the detection of ground - glass opacities , nodules , and thickening of the interlobular septa suggests a possible resolution , whereas honeycombing and an advanced fibrotic pattern indicate an irreversible course and an end - stage disease . 
 it is not clear whether the evolution of the typical and atypical patterns is influenced by sarcoidosis therapy and whether the finding of specific patterns can guide to start immunosuppressive - steroid treatment . 
nowadays , treatment decisions tend to depend on the clinical symptoms and on extrapulmonary involvement , but not on the radiological signs , even if imaging plays a fundamental role in the diagnosis [ 38 , 39 ]  . 
furthermore , hrct should not be used in the routine follow - up for patients with stable disease and it should be considered in case of worsening of clinical conditions . 
atypical radiological patterns are always a challenge even for the experienced radiologists . in conclusion , the cases with atypical pulmonary sarcoidosis patterns evaluated in the study are consistent with similar cases described in the literature [ 2 , 4 , 6 , 7 , 9 , 10 , 4042 ]  . 
all the atypical characteristics described in this study should alert the radiologist to even consider sarcoidosis among the possible differential diagnoses , always correlating the hrct results with appropriate clinical and laboratory evaluations . 1 3 radiol med ( 2018 ) 123 : 174184 compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . ethical approval all procedures performed in studies involvement human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
 the interplay of genetic susceptibility , infection by epsteinbarr virus and environmental factors ( diet , smoke , alcohol , wood dust - related occupations ) is recognized to be important for the occurrence of the disease . 
since the 5 - year survival ranges from 72% for stage i to 38% for stage iv , the quality of life of survivors has been recognized as an important issue [ 3 , 4 ]  . 
however , the disease has been characterized by early lymphatic spread and relatively frequent hematological dissemination compared to other head and neck carcinomas . radiotherapy is a basic form of local therapy being applied as the exclusive treatment for stage i and with concomitant chemotherapy in other stages of disease without distant metastases . 
thanks to technological progress , new radiotherapy techniques have been developed with the intention not only of improvement of tumor coverage , but also of better spearing oars reducing thus xerostomia , hearing loss , temporal lobe injury , and damage to the spinal cord , brain stem and optic chiasma in comparison to the vol . : ( 0123456789 ) 1 3 218 radiol med ( 2018 ) 123 : 217226 traditional 2 - dimensional radiotherapy ( 2drt ) [ 58 ]  . 
in the treatment of npc , the 3 - dimensional conformal radiotherapy ( 3d - crt ) was first reported by the memorial sloan - kettering cancer center in 1991 and the intensity modulated radiation therapy ( imrt ) by university of california san francisco in 2000 [ 9 , 10 ]  . 
recently , imrt has become the optimal radiation technique to be performed in the treatment of npc due to its better protection of adjacent healthy tissue and significant reduction of side - effects , especially xerostomia , in comparison to 2drt and 3d - crt techniques . 
however , for the time being there is no undisputed evidence that the imrt is superior to 3d - crt regarding overall survival ( os ) , disease - free survival ( dfs ) and locoregional control ( lrc ) [ 1114 ]  . 
conformal parotid - sparing radiotherapy ( conpas ) , a more advanced 3d - crt technique , has been developed with the aim to spare parotid glands and spinal cord when imrt is not available [ 15 ]  . 
conpas employs two pairs of full - length parallel opposed oblique beams that are turned into half - beams by closing the collimators on the side of the spinal cord . 
three randomized studies compared imrt versus 2d radiotherapy [ 5 , 7 , 8 ] and four non - randomized studies compared imrt versus 3d radiotherapy [ 1114 ]  . 
the imrt - sib technique allows the simultaneous delivery of different dose levels to different target volumes within a single treatment fraction enabling the shortening of treatment duration and enhancing biologically equivalent dose ( bed )  . 
to the best of our knowledge there is no study comparing conpas 3d - crt and imrt - sib in the treatment of nasopharyngeal carcinoma . therefore , the objective of the present study was to compare the two above - mentioned radiation techniques that previously proved to be effective in parotid gland sparing , with respect to the treatment outcome , tumor coverage and dose distribution to the organs at risk . patients andmethods at our department of oncology 2drt was the standard of treatment of npc until may 2009 when conpas 3d - crt was introduced . 
in july 2012 , we started to gradually implement imrt - sib instead of 3d - crt . a total of 24 consecutive patients with histologically proven npc treated with conpas 3d - crt or imrt - sib between may 2009 and december 2016 were retrospectively enrolled in the study . 
only patients treated by physicians who applied both radiation techniques were included in the study for the purpose of reducing potential variability in contouring target volumes and oars . the pretreatment evaluation included the patients history , physical examination , direct flexible fiberoptic nasopharyngoscopic examination , chest x - ray , computed tomography or magnetic resonance imaging scans of head and neck . 
 the high risk clinical target volume ( ctv1 ) was defined as gtv plus 510mm margctv2 covered potential sites of microscopic disease including the entire nasopharynx , retropharyngeal lymph nodes , skull base , clivus , pterygoid fossae , parapharyngeal space , posterior third of the nasal cavity and maxillary sinus , sphenoid sinus and neck nodal regions of intermediate risk . 
in both techniques planning target volumes ( ptvs ) were generated with an isotropic expansion of 5mm from corresponding ctvs except in the proximity of critical oars where the margin was reduced to 03m for conpas 3d - crt in 8 patients 3 ptvs were determined : ptv1 70gy , 2gy / fraction ( high risk ) , ptv2 60gy , 2gy / fraction ( intermediate risk ) and ptv3 54gy , 2gy / fraction ( low risk )  . 
 for imrt - sib in all patients 3 ptvs were defined : ptv1 66gy , 2.2gy / fraction ( high risk ) , ptv2 60gy , 2gy / fraction ( intermediate risk ) and ptv3 54gy , 1.8gy / fraction ( low risk )  . 
the radiation plans were made using the xio ( elekta , sweden ) planning systethe conpas 3d - crt planning was done according to previously published technical recommendations [ 15 ]  . 
conpas 3d - crt was performed with a 6 mv photon beam delivered with a primus plus linear accelerator ( siemens , germany ) with 82 - leaf multileaf collimator ( mlc )  . 
for each imrt plan , patient - specific quality assurance ( qa ) was performed . delineation of oars ( spinal cord , brain stem , parotid glands , optic chiasma , optic nerves , cochlea , lens , temporal lobe and posterior fossa of the brain ) was done according to previously reported guidelines [ 21 , 22 ]  . 
standard dose constraints were adapted [ 23 ]  . chemotherapy the chemotherapy consisted of 3 cycles of cisplatin 80mg / m2 , 5 - fluorouracil 1000mg / m2 administered before or after radiotherapy and 3 cycles of concurrent cisplatin 100mg / m2 every 3weeks . 
one patient in the imrt - sib had stage i disease while all other patients who did not receive chemotherapy were older than 75years of age . followup patients characteristics ( table1 )  . 
more patients in the conpas 3d - crt group received concomitant chemotherapy compared to the imrt group , while there was a somewhat higher rate of stage 1 and 2 in the imrt group compared to the 3d group , 23 versus 9% , respectively . 
in the imrt - sib group , 5 patients received 3 cycles of concurrent chemotherapy and 5 patients received 2 cycles . four patients , two in each group , had a partial response to the treatment while all others had a complete response . 
the overall survival ( os ) and disease - free survival ( dfs ) were estimated using the kaplanmeier method and the differences were assessed by the log rank test . 
 the median value of dose applied to 50% volume of the left parotid gland was 4205cgy in the conpas 3d - crt group and 2219 cgy in the imrt - sib group while the median value of dose applied to 50% volume of the right parotid gland was 4100cgy in the conpas 3d - crt group and 2580cgy in the imrt - sib group . 
comparison of dose distribution at parotid level of two representative patients treated with different radiation techniques is presented in fig.3. the median value of maximal dose to the spinal cord was 4423cgy in the conpas 3d - crt group and 3837cgy in the imrt - sib group . 
in the multivariate analysis age , gender , stage , t , n , radiation technique and application of chemotherapy were not significant predictor factors of dfs . the percentage volume covering 95% of the prescribed dose ( v95% ) of all ptvs was significantly better in the recently , imrt has become the standard treatment for nasopharyngeal cancer applied alone in stage i and with concurrent chemotherapy for stages ii to ivb . 
better spearing of surrounding oars was well recognized as the main advantage of imrt resulting in lower toxicity of the treatment and better quality of life when compared with 3d - crt and 2drt [ 5 , 6 , 8 , 1113 ]  . 
in case of unavailability of imrt , conpas 3d - crt technique showed the best dose - volume values for parotid glands and spinal cord in comparison to other more advanced 3d - crt techniques [ 15 , 29 ]  . in our study , the os for the whole cohort of patients was in accordance with the results of other studies [ 12 , 30 ] while dfs was lower than reported by kunag etal . 
 [ 31 ] which could be possibly explained by the learning curve at our department and by small number 1 3 ptv95 iii wilcox p : 0.0032434 * * ptv95 ii wilcox p : 0.0249163 * ptv95 i wilcox p : 3.4963e06 * * * 3dcrt imrt 3dcrt imrt 3dcrt imrt protocol ptv107 iii wilcox p : 1 ptv107 ii wilcox p : 0.0299608 * ptv107 i wilcox p : 0.0574565 radiol med ( 2018 ) 123 : 217226 fig . 
2 comparison of the dosimetric results obtained with conpas 3 - dimensional conformal radiotherapy ( conpas 3d - crt ) and intensity modulated radiotherapy with simultaneous boost ( imrt - sib ) for planning target volumes ( ptvs ) : a the percentage volume covering 95% of the prescribed dose ( v95% ) ; b the percentage volume covering 107% of the prescribed dose ( v107% )  . 
 [ 30 ] noted that local failure - free rate ( l - ffr ) in the imrt era did not show further improvement as compared with the 3d - crt era . 
however , steady increase in 5 - year os and disease - specific survival ( dss ) for npc has been observed from 1960s and 2drt era to 1990s [ 30 ]  . 
 [ 30 ] reported that both 3d - crt and imrt were independent significant factors for local control . the results of this study proved a more conformal dose distribution and better coverage of all ptvs in the imrt - sib 1 3 222 fig . 
3 comparison of isodose distribution in a ct slice of two representative patients : a conpas 3 - dimensional conformal radiotherapy ( conpas 3d - crt ) ; b intensity modulated radiotherapy with simultaneous boost ( imrt - sib ) radiol med ( 2018 ) 123 : 217226 than in the conpas 3d - crt group without increase of the v107% which was consistent with other studies [ 6 , 32 , 33 ]  . 
as was previously reported that radiation doses to most oars were associated with t or n stage and gtv [ 34 , 35 ] , we checked if there were any differences between the groups in patients characteristics and found none . 
 [ 11 ] reported much higher doses applied to the parotid glands when compared imrt and 3d - crt [ left parotid gland : mean 46.84 gy ( range 21.4464.37 gy ) and mean 59.48 gy ( range 40.1470.37gy ) , respectively ]  . 
their total prescribed dose was higher , up to 72.075.6gy for t3 - 4 tumors , with a daily fraction 1.8gy while we applied 70gy with a daily fraction 2gy in the conpas 3d - crt group and 66gy with a daily fraction 2.2gy to the ptv1 in the imrt - sib group . 
the results of our study proved that better sparing of the parotid glands was achieved with imrt than with 3d - crt which was in concordance with the results of numerous other studies [ 6 , 8 , 11 , 31 , 3739 ] although in our study conpas 3d - crt was performed which previously proved to be better protection of parotid glands than conventional 3d technique . however , although lee etal . 
 [ 30 ] found a reduction of neurological damage from 2drt era to 3d - crt era and further to imrt era , there were reports of significantly higher maximum and mean doses for the posterior fossa of the brain , brain stem and cerebellum contributing to the higher incidence of acute fatigue during imrt than during 3d - crt [ 40 , 41 ]  . 
in our study , both maximal and mean doses to the posterior fossa of the brain and brain stem were also higher in the imrt - sib group than in the conpas 3d - crt group but that was not statistically significant . 
the lack of significant differences in dose distribution of abovementioned organs at risk between the two studied radiotherapy techniques in our study could be possible explained by different orientation of fields in conpas 3d - crt plans than in conventional 3d techniques used in other studies . the limitations of the study are a low number of patients , the retrospective study design and relatively short follow - up time . in conclusion , the results of this study proved that imrtsib was significantly better than conpas 3d - crt in terms of parotid glands and spinal cord sparing as well as ptvs coverage . 
however , there were no survival advantages . 1 3 radiol med ( 2018 ) 123 : 217226 left parotid 50% volume dose wilcox p : 0.0010405 * * left parotid mean dose wilcox p : 0.0225002 * 6000 5000 4000 3000 2000 1000 6000 5000 4000 3000 2000 1000 4000 3000 2000 1000 right parotid 50% volume dose wilcox p : 0.0317437 * right parotid mean dose wilcox p : 0.0256783 * 3dcrt imrt 3dcr protocol medula maximal dose wilcox p : 0.00196463 * * medula mean dose wilcox p : 0.0629178 medula minimal dose wilcox p : 0.0596533 3dcrt imrt 3dcrt imrt 3dcr imrt protocol fig . 
4 comparison of the dosimetric results obtained with conpas 3 - dimensional conformal radiotherapy ( conpas 3d - crt ) and intensity modulated radiotherapy with simultaneous boost ( imrt - sib ) for organs at risk ( oars ) : a parotid glands ; b spinal cord ; c temporal lobes and posterior fossa of the brain ; d cochlea . 
the black horizontal line represents the median value of dose for each organ of risk 1 3 224 radiol med ( 2018 ) 123 : 217226 posterior fossa mean dose wilcox p : 0.231578 left temporal lobe mean dose wilcox p : 0.409952 right temporal lobe mean dose wilcox p : 0.283929 3dcrt imrt 3dcrt imrt 3dcrt imrt protocol left cochlea dose wilcox p : 0.927375 right cochlea dose wilcox p : 0.648162 3000 2000 1000 6000 4000 2000 3dcrt imrt 3dcrt imrt protocol fig . 
all patients without significant alteration patterns at mpmri have been referred for follow - up at 1year . results 91 / 108 patients showed on the mpmri highly suspicious lesions ( pirads 4 and 5 ) ; the remaining 17 / 108 patients revealed no significant alteration consistent with pca ( pirads 3 )  . 
however , the cdr rises significantly , up to 77% , after the 53 initial consecutive biopsies that were performed ( p < 0 , 05 ) and thus identified as part of the learning curve . 
patients of the second group ( 17 / 108 ) have been followed with serial psa assessments , clinical reevaluation , and follow - up mpmri . conclusion performing exclusively targeted mr / ultrasound fusion - guided biopsies for the diagnosis of pca in patients with suspicious psa levels ( > 4ng / ml ) increases the detection rate of clinically significant cancer , changing both the therapeutic options and the prognosis . keywords prostate cancer multiparametric magnetic resonance targeted biopsy the original version of this article was revised : the first and last names of the second author were interchanged . 
to diagnose pca , the european association of urology ( eau ) guidelines [ 2 ] recommend , as - ine tools , the psa level evaluation , the digital rectal examination , and the pathologic evidence provided by trans - rectal ultrasound guided random biopsy ( trus - guided biopsy )  . however , the literature has demonstrated that trusguided biopsy has a high percentage of false - negative results vol . : ( 0123456789 ) 1 3 228 la radiologia medica ( 2018 ) 123 : 227234 ( 47% ) [ 3 ] , that 5080% of clinically significant neoplastic lesion is missed , and that the potential to differentiate lesions varies from 11 to 35% [ 4 , 5 ]  . given the promising results found in the literature [ 6 ] , multiparametric mri of the prostate ( mpmri ) has been introduced in the eau and european society of urogenital radiology guidelines ( esur ) [ 2 ] as the second level ( 2b ) of investigation , specifically following random negative biopsy [ 7 , 8 ] the introduction of mpmri in the diagnostic work - up for pca has improved biopsy accuracy and cdr , given its negative predictive value ( npv ) of 86.298.6% for clinical significant cancer [ 9 , 10 ] ( 10% of which , even if not identified , represent small low - grade lesions that , as such , would undergo active surveillance program anyway ) and positive predictive value ( ppv ) of 5296% [ 6 , 11 ]  . 
nevertheless , despite the demonstrated validity of the mri multiparametric approach to diagnose prostate cancer , recent papers showed that a biparametric approach ( t2wi and dwi ) may be sufficient for routine prostate imaging [ 13 ] .cdr is up to 40% in the cognitive approach , which is based on the execution of random sampling of previously identified lesions on mr images [ 24 , 11 , 1416 ]  . 
the best outcomes have been obtained in pinpointing small foci ( < 1cm ) ; after fusion biopsy , the cdrs of the aforementioned go up to 31% more than the one after biopsy based on the cognitive approach [ 5 , 1922 ]  . 
in view of the background , the goal of our study is to validate the role of pca diagnosis by mr / ultrasound fusion - guided targeted biopsy alone , in individuals with suspected pca . materials andmethods patients population andstudy design for this prospective study , approved by our institutional review board , between january 2015 and november 2016 , a cohort of 108 patients , aged from 46 to 78years , was recruited . 
patients were eligible to participate in the trial if they were older than 18years of age , had high suspicion for pca following digital rectal examination ( dre ) , and had a psa density > 0.20 , psa velocity > 0.75ng / ml / year and total psa > 4ng / ml ( > 2.5 in patients with family history )  . 
 the examinations have been acquired at 3.0 tesla mpmri ( discovery 750 ge , italy ) , using a 32 - channel phased - array surface coil ( torsopa )  . 
the morphologic images have been obtained using propeller fast spin echo ( frfse ) multiplanar t2w sequences ( sagittal , axial , and coronal planes ) ( tr : 4500ms ; te : 120ms ; average : 4 ; slice thickness : 3mm ; tim ; matrix : 352352 ; fov : 22cm ; scan time : 3 , 30min ) with optimization of the parameters , yielding a higher spatial resolution . 
 once the analysis of the images had been performed according to piradsv2 score [ 23 , 24 ] , in case the same patients showed more than one lesion that the index lesion was chosen considering the highest pirads assessment category or , alternatively , the largest lesion , if there was more than one of the same category . 
piradsv2 score allows the stratification of patients adopting a 5 - point scale based on the likelihood ( probability ) that a combination of mpmri findings on t2w , dwi , and dce correlates with the presence of a clinically significant cancer for each lesion in the prostate gland [ 24 , 25 ]  . 
patients displaying suspicious mr 1 3 la radiologia medica ( 2018 ) 123 : 227234 patterns or reports consistent with high probability of neoplastic disease ( pirads 4 and 5 ) have undergone targeted biopsy . 
ugeo h60 3d , that allows the 3d reconstruction of prostatic volumes by means of a particular endorectal probe known as end fire . the fusion software enables the acquisition of a volumetric image of the prostate , obtained by fusing mr and us , by means of a co - registration method . 
by doing so , the registration becomes resistant to the movement and to the deformation of the prostate , caused by the probe or by the movement of the patient [ 26 ]  . the 3dtrus trace of the prostate is an automatic registration based on the position of the organ over the image . 
in our protocol , the maximum number of lesion undergoing biopsy was 3 , and the maximum number of biopsy samples , for each lesion , was 2 and 4 for small and large lesions , respectively . 
the fusion biopsies have been performed by experienced radiologist on the field with 3 - year training and by a younger radiologist with 2 - year training , who has also performed trus - guided biopsies for 1year . 
 to our knowledge , we represent one of the first radiological teams performing the procedure on his own , suggesting that being confident with images modality is the major issue on performing target biopsy technique . patient preparation no local anesthesia was offered prior to the procedure except for the administration of endorectal lidocaine gel ( 10ml )  . 
discrepancies were resolved by consensus , assuming the most experienced readers opinion as the definitive one . results the 108 patients with a psa mean value of 7 , 62ng / ml underwent mpmri with the following results : 91 patients with suspect lesions classified as pirads 4 and 5 ; 17 patients classified as pirads 3 . the first group of patients ( pirads 4 and 5 ) was referred to undergo fusion targeted biopsy . 
specifically , 33 patients underwent radical prostatectomy that showed positivity for pca at the pathology report as the needle core biopsy did ; 10 have been treated with radiotherapy , and 15 have been referred to active surveillance protocols . 
in addition , we want to specify that the mri index lesion , according to piradsv2 , not always corresponded to the index tumor of radical prostatectomies ; 1 3 230 la radiologia medica ( 2018 ) 123 : 227234 fig . 
a mpmri t2w sequence ; b adc sequence ; c dwi sequence ; dg index lesion sampling and prostate 3d reconstruction made by the software ; h radical prostatectomy macro - section fig . 
a mpmri t2w sequence ; b adc sequence ; c dwi sequence ; d prostate ultrasound and target sampling ; e 3d reconstruction made by the software ; f radical prostatectomy macro - section 1 3 la radiologia medica ( 2018 ) 123 : 227234 table 1 start table showing patients characteristics men included in the study , n age median ( iqr ) pre - biopsy psa level , ng / ml , median men with pirads = 3 lesions on mpmri , n men with pirads = 4 lesions on mpmri , n men with pirads = 5 lesions on mpmri , n patients undergoing to fusion biopsy , n targeted biopsies per patient and per lesion , median 62 ( 4678 ) 7 , 62ng / ml 3 ( 23 ) , 2 ( 14 ) ( iqr ) patients with positive biopsy , n biopsy result gs 6 ( 3 + 3 ) , n biopsy result gs 7 ( 3 + 4 ) , n biopsy result gs 7 ( 4 + 3 ) , n biopsy result gs 8 ( 4 + 4 ) , n biopsy result gs 9 ( 5 + 4 ) , n negative biopsy , n ior interquartile range , psa prostate - specific antigen , gs gleason score specifically , the mpmri index lesion corresponded to the lesion with the highest gleason score ( index tumor ) in 64% of cases ; in 15% , the mri index lesion had the same gs of another lesion , and in the remaining 21% , the mri index was found to have a lower gs of a non - index lesion . 
patients of the second group ( pirads 3 ) were followed with serial psa assessments at 3months , clinical reevaluation at 6months , and follow - up with mpmri ( 8 - 12months )  . 
 among the aforementioned 17 patients , one of them , given the rapid increase in psa ( 4 , 5ng / ml in january , 5 , 98ng / ml in may , and 8 , 32ng / ml in july ) , underwent a second random biopsy , which resulted to be positive for prostate adenocarcinoma ( gs6 3 + 3 in 18% of 1 / 12 samples )  . 
instead , the remaining 16 had stable clinical findings ( dre ) , laboratory findings ( psa / psa density ) , and imaging report ( mri pattern )  . 
there were only four cases in which there was disagreement between readers . recorded complications are urosepsis in two patients , which resolved in the 5days and moderate hematuria in three patients . 
according to the calvin dindo classification , both complications are classified as grade i . discussion the introduction of mpmri has modified significantly the diagnostic algorithm and the therapeutic planning of pca [ 17 ] ; in fact , mpmri can combine the high spatial resolution of t2wi to dwi and dce sequences which evaluate cellular proliferation and angiogenesis , respectively . 
matching anatomic and functional information provided by mpmri , with respect to the simple morphologic representation of the lesion on t2wi , designates the mpmri as the most promising technique to increase sensitivity , specificity , and diagnostic accuracy in the diagnosis of pca , as it has been validated by the previous experience [ 11 ] , [ 27 , 28 ]  . 
in addition , decreasing the number of samples allows for a greater patient compliance , reducing discomfort , and concerns . in our study , we have obtained a cdr of 63% in 108 individuals with gs6 examined by mri - trus - guided biopsy . 
furthermore , analyzing 1 3 232 table 2 study flowchart la radiologia medica ( 2018 ) 123 : 227234 patients with suspect mpmri lesion ( n = 108 ) enrolled between january 2015 to november 2016 excluded : patients ( n = 17 ) without clinically significant mpmri lesion ( pirads = 3 ) follow up : - serial psa ( 3 m ) , - clinical reevaluation ( 6m ) - mpmri . 
consequently , we identified 6months that , in our experience , correspond to 53 biopsies , as part of the necessary individual learning process of radiologists performing targeted fusion biopsies . 
these findings may have implications for further studies aimed at evaluating prostate targeted biopsy long - term effectiveness in terms of follow - up and the possible involvement of the technique learning curve . furthermore , it is necessary to compare mri - trusguided biopsy results with in - bore mri guided biopsy scan which offers the possibility of more precise targeting with the chance to perform even fewer core biopsies [ 37 ]  . 
 however , this approach has limitations , being a high cost in terms of spending review , an intrinsic elevated technical difficulty which makes it eligible only for highly trained radiologists and the general contraindication of mri study [ 3840 ]  . despite the good results obtained in this study , it is necessary to evaluate a standardized method for a correct selection of patients that are possible candidates for targeted biopsy , specifically for those in which lesions are identified by mpmri as being pirads 3 . further studies focused on a per core basis analysis are warranted to achieve more detailed results in terms of cdr . 
an oral contrast iodine concentration of 5.827.77mgi / ml most closely approximated a target oral contrast density of 200 hu . conclusions oral contrast density is strongly influenced by kvp , supporting use of more dilute oral contrast when using lower - kvp techniques . keywords oral contrast kvp ct dose introduction reduced voltage ( lower kvp ) ct scanning techniques have become increasingly popular in abdominopelvic imaging as a means to both reduce effective radiation dose and increase iodinated intravenous contrast conspicuity [ 13 ]  . 
 the most commonly utilized positive oral contrast agents are comprised of mixtures of either iodine or barium which result in attenuation of incident x - rays , increasing visualized * andrew d . 
with reduced voltage ct , the attenuation of oral contrast increases as the x - ray energy levels approach the k - edge of iodine or barium , resulting in greater bowel contrast [ 4 , 5 ]  . 
while the clinical benefits of increased contrast conspicuity with reduced voltage ct ( including the potential for using decreased intravenous contrast volumes ) have been well established for iv contrast agents , less attention has been paid to increased oral contrast conspicuity [ 68 ]  . 
while increased intravascular contrast from intravenous contrast agents is generally considered desirable , increasing apparent intraluminal contrast could obscure pathology for oral contrast agents with low - kvp ct . water - soluble iodine - based oral contrast agents in clinical use are diluted per manufacturer guidelines in radiology departments prior to patient ingestion . 
in this study , an initial retrospective assessment investigated clinical abdominopelvic ct scans acquired with either reduced or higher - voltage protocols , but which used oral contrast concentrations that were unchanged from prior higher - voltage ct protocols . 
 this initial subjective reader assessment was performed to establish whether or not the oral contrast density was optimized , as evidenced by the need to adjust window and level settings from default pacs levels . 
of the 100 clinical ct scans performed , 95 were sect acquisitions ( 95 datasets ) and 5 were dual - source dect acquisitions ( 10 datasets ; each dual - source ct included highand lowenergy images )  . 
for the purposes of this study , all datasets acquired using kvp settings of 120 or higher were considered high - energy acquisitions ( n = 32 ) and 110kvp or less were considered low - energy acquisitions ( n = 63 )  . 
 eighty - two percentage of patients also received iv contrast with protocol specific , weight - based contrast volume and injection rates . 100 oral contrast cts 95 sect acquisi ( cid : 31 ) ons 5 dect acquisi ( cid : 31 ) ons 63 datasets at 110 kvp 32 datasets at 120 kvp 5 datasets at 90 kvp 5 datasets at 150 kvp fig . 
2 commercially available cirs phantom was utilized to scan 10 - cc syringes filled with premixed barium oral contrast material and various dilutions of iodinated contrast material using single - energy and dual - energy techniques on a third - generation dual - source ct scanner phantom study a commercially available cirs tissue equivalent phantom ( fig.2 ) was utilized to image oral contrast materials using kvp settings ranging from 90 to 140kvp with single energy and at 90 and 150kvp with dect techniques . 
 all ct imaging was performed on the same third - generation dual - source ct scanner ( force , siemens healthcare , erlangen , germany ) using routine clinical protocols ( table1 )  . two commercially available positive oral contrast agents were used , including barium sulfate and iohexol . 
additionally , however , in the five cases performed with dect , using default window / level settings , readers were also asked to choose which of the three dect datasets ( low - energy , high - energy , and 0.6 blended datasets ) were optimal for bowel assessment . 
due to the low incidence of bowel pathology in our patient cohort , readers were not asked to assess for specific bowel pathology . quantitative analysis quantitative analysis on both the phantom and clinical examinations was performed by one fellowship - trained abdominal imager with 19years of post - fellowship experience reading ct . 
for the phantom study , a single region of interest ( roi ) measuring 105mm2 was placed centrally within the contrast sample , taking care to avoid the walls and to center within the z - axis volume . 
for the patient study , three rois were placed on axial images , within opacified jejunal loops in the left upper abdomen , and ileal loops in the pelvis or right lower quadrant . 
 care was taken to place the roi centrally within representative loops of well - opacified bowel , using corresponding sagittal or coronal reconstructed series to avoid volume - averaging effects . 
contrast - to - noise ratio ( cnr ) was calculated with the following formula : cnr = huoral contrastu huretroperitoneal fat retroperitoneal fat syringes , which were capped and then inserted into one of 6 channels within the phantom , which was then centered in the gantry of the ct scanner and imaged . after ct acquisitions , routine clinical reconstructions of the dataset were performed at the scanner for singleenergy ct images . 
for dual - energy ct acquisitions , 0.6 blended and single - tube ( 90 and 150kvp ) datasets were reconstructed on a vendor - specific workstation ( syngovia , siemens healthcare , erlangen , germany )  . 
 to assess differences in attenuation based on weight ranges , a one - way anova test determined significance within the ranges < 100 , 100200 , and > 200lb , and a student t test was used for a separate comparison of thin patients ( 100lb ) compared to average or large patients ( > 100lb )  . 
for optimal oral contrast dilution assessment , a value of 200hu was chosen based on the results of prior studies [ 14 , 15 ] as well as consensus among the study readers based on assessment of the phantom images . results in the clinical study , three subjects received barium as the oral contrast agent with the remaining 97 subjects ( 97% ) receiving iodine - based oral contrast . 
when bowel segment oral contrast density was stratified by patient weight ( < 100 , 100200 , and > 200lb ) , gastric contrast attenuation was uniform across weight classes ( p = 0.48 ) , but decreased in the jejunum ( p = 0.33 ) and ileum ( p = 0.19 ) as patient weight increased categorically ( table3 )  . 
 no artifacts related to oral contrast material were reported by any reader . our results confirm that with reduced voltage ct , oral contrast density increases , affecting clinical image appearance and requiring greater window and level changes . 
regardless of potential negative clinical impact , our results highlight the opportunity to significantly lower iodine concentrations in oral contrast agents when used with reduced voltage ctwhich has potential to increase patient tolerance and decrease department cost . 
a similar trend was seen in the subset of patients imaged with dual - energy ct ( dect ) ; however , small numbers likely precluded reaching statistical significance 1 3 la radiologia medica ( 2018 ) 123 : 918925 fig . 
5 clinical studydual - energy oral and iv contrast materialenhanced ct in a 46 - year - old female with abdominal pa the 100 kvp image ( a ) , 150 kvp image ( b ) , and 0.6 blended dect image ( c ) are displayed at standard 350 / 50 abdominal window / levels . 
6 phantom studyoral contrast density ( hu ) versus kvp at single - energy ct ( sect , left ) and dual - energy ct ( dect , right )  . 
dotted line shows the historic target oral contrast density of 200hu contrast agents cannot be as readily diluted , they are likely less desirable for use in reduced voltage ct . our study suggests that an iodinated contrast dilution of as low as 6mgi / ml may be optimal for 100kvp voltage level scans , which was approximately 33% lower than that used in our clinical practice at the time of this study . 
this is in line with findings of [ 8 ] who suggested that 9mgi / ml , and potentially as low as 3mgi / ml , may be appropriate for reduced voltage dual - energy ct acquisitions . 
as many radiology departments dilute oral iodinated contrast agents immediately prior to use , these studies highlight both the potential for patient - specific oral contrast dosing and potential impact of non - tailored dilutions that could result in contrast densities that are too high or low . it is important to acknowledge that oral contrast material is being less utilized in many practices and for many 1 3 924 la radiologia medica ( 2018 ) 123 : 918925 indications [ 1719 ]  . 
however , despite this trend , in certain patient populations , including patients with little intra - abdominal fat [ 20 ] , cases of suspected leak , fistula or abscess [ 21 ] , patients with prior gastric bypass surgery , and in patients with peritoneal disease or in whom iv contrast cannot be utilized [ 20 , 21 ] , oral contrast material may remain an important tool to optimize diagnostic ability of ct imaging . 
 of particular note is that thinner patients ( who are more likely to receive oral contrast material in many practices ) are also more likely to be scanned with lower - voltage techniques ( in order to optimize radiation dose )  . 
however , use of oral contrast complicates radiation dose optimization : when automated tube modulation techniques are used , the presence of oral contrast material may increase patient radiation dose [ 22 ]  . 
therefore , particularly in thinner patients , the use of lower concentrations of oral contrast material has the potential not only to optimize bowel opacification but also to decrease radiation dose . 
beyond improved contrast density and optimized radiation dose , use of lower concentrations of oral contrast agents not only decreases cost but also increases patient acceptance due to less objectionable taste [ 23 , 24 ]  . to our knowledge , no prior studies evaluating effects of different voltage settings on oral contrast density assessed optimal window and level settings . 
our results suggest that if oral contrast dilutions are not optimized for low - kvp techniques , substantial adjustments to window and level settings are required to compensate for high contrast density . 
 as our readers reported needing window and level adjustment in 86% of cases , including those scanned with higher energies , this suggests that contrast densities used during our study might need to be adjusted even for high - energy scans . 
although our dataset included relatively few dualenergy acquisitions , readers uniformly favored high - energy datasets for evaluation of the bowel , over low - energy and blended datasets when standard windows were utilized , due to reduced opacity of the oral contrast agent . 
while use of high - energy datasets from dect acquisitions as a substitute for optimized contrast dilution could be considered , as these datasets are not routinely available in clinical practice , their use may not be practical in most settings . this study has some limitations , including a small population size . 
as cost and radiation dose would likely preclude scanning patients with and without oral contrast material ( particularly with multiple dilutions ) , such an investigation would likely require a multiinstitutional approach . 
we believe that our study represents an important step toward oral contrast optimization , identifying a suitable oral contrast dilution for use at low - energy techniques that replicates the density of oral contrast dilutions used with traditional high - energy techniques . in conclusion , when utilizing reduced voltage ct , changes in the methods for administration oral contrast are likely warranted . 
specifically , iodinated contrast agents should be diluted in relationship to the expected kvp setting in order to maintain a clinically acceptable appearance and prevent the need for extensive changes to window and level settings . 
while individually tailored oral contrast dilutions are unrealistic in most practice settings , iodine concentrations of 6mg / ml may be reasonable in thin - to - average - sized patients when low - energy scanning techniques are utilized . 
 as premixed barium - based positive oral contrast agents are not as readily diluted , iodinated agents may be preferable for low - energy techniques . authors contributions dh sheafor acts as the guarantor of integrity of the entire study . 
an activity - based cost analysis was performed to evaluate potential savings due to the introduction of ceus as an alternative to ct , after the first year of postoperative negative controls . results ceus reported accuracy , sensitivity , specificity , positive predictive values , negative predictive values of 97.4 , 96 , 100 , 100 and 93.1% in the detection and characterization of endoleaks . 
however , endovascular procedure is more expensive than traditional surgery , with higher frequency of re - interventions to treat complications , such as endoleak , endograft occlusion , migration and post - implantation rupture [ 1 ]  . endoleak is defined as incomplete exclusion of aneurysm sac due to persistent blood flow outside a graft and within the sac itself . 
scuro , 37134verona , italy diagnosis is crucial for preventing the risk of aneurysm sac enlargement and rupture [ 2 ]  . according to eurostar guidelines ( european collaborators on stent / graft techniques for aortic aneurysm repair ) , computed tomography angiography ( cta ) is an established gold standard and noninvasive method to evaluate these patients during follow - up . 
during the first year , follow - up observations should be performed at 3 , 6 and 12months after procedure , with successive annual checks for an average period of 6years [ 3 ]  . several studies have already shown that alternative imaging techniques ( mr , eco - color - doppler ) and contrastenhanced ultrasonography ( ceus ) permit increased recognition and characterization of endoleak [ 415 ]  . after 1year of negative ct exams , use of ceus as an alternative investigation method could lead to substantial cost savings , related to its lower costs . 
all ceus examinations were recorded on dvd to review the dynamic study . materials andmethods patients , inclusion andexclusion criteria this single - center retrospective study received irb approval , and informed consent was obtained from all the patients enrolled . 
the study population included 157 patients treated with evar in clinicalradiological follow - up over a period of 6years between 2011 and 2016 . exclusion criteria consisted of the presence of insufficient image quality or the lack of any imaging study . twenty patients were excluded because of the lack of one of the imaging methods . 
therefore , we included 137 patients treated with evar ( 122 males and 15 females , mean age 70.3years , range 5490years ) , 69 with zenith endograft , cook medical and 68 with excluder , gore medical : all patients underwent endoprosthesis evaluation with ceus and cta , both performed within 1week ( average 4.3days , range 27days )  . 
none of the patients had allergic diathesis after iodinated contrast injection . twenty - three of 137 patients had a history of ischemic heart disease ( with only one case of previous myocardial infarction ) : this was not an exclusion criterion , because it occurred 6months before ceus examination . 
in 9 out of 137 patients was performed an angiographic study with femoral artery approach , based on previous ultrasound or ct findings , in order to characterize and possibly treat endoleaks . imaging technique in ceus , all ultrasound examinations were performed by the same operator on a sequoia 512 6.0 ultrasound system ( acuson , mountain view ca , usa ) , with harmonic microbubble - specific imaging , convex probes and low acoustic ultrasound pressure ( 24mhz cadence contrast pulse sequencing ; 0.2 mechanical index ; 1213 frames a second )  . 
the exam was completed after intravenous administration of 2.4ml bolus of second - generation contrast agent ( sonovue , bracco , milan , italy )  . ct angiography abdominal aorta ct study was performed with a 64 - row scanner ( brilliance ct - 64 ; philips , eindhoven , the netherlands ) before and after intravenous administration of 1.5ml / kg of water - soluble iodine contrast agent ( ultravist 370 , bayer schering pharma , germany ) at a flow rate of 4.5ml / s by automatic power injectors , followed by a bolus 50ml of saline solution . 
patients underwent a cranio - caudal scan from the diaphragm to the symphysis pubis , with triphasic protocols including unenhanced acquisitions , arterial contrast - enhanced acquisitions ( timed with a bolus - tracking technique , performed with a 4 - s delay from 150 - hu threshold of enhancement ) and venous contrast - enhanced acquisitions ( 60s later )  . 
for arterial contrastenhanced phases , parameters were : 0.8mm slice thickness ; 0.4mm pitch ; 120kv ; and 310mas . image analysis both cta and ceus images were double - blinded analyzed by two radiologists ; in case of doubt ( n = 7 ) , discrepancies were subsequently resolved by consensus . 
 ceus examination lasted 4min after contrast administration , in order to detect also late type endoleaks ( in particular type ii ) [ 13 ]  . ct images were analyzed on a dedicated workstation in order to generate multi - planar two - dimensional reconstructions ( mpr ) , mip ( maximum intensity projections ) and 3d reconstructions ( volume rendering )  . 
 1 3 906 la radiologia medica ( 2018 ) 123 : 904909 endoleaks were diagnosed in the case of persistent contrast flow inside the excluded sac . statistical analysis sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy of ceus were calculated as compared to cta , representing the reference standard . 
after the first year with negative cta , starting from the second year , cost savings due to the introduction of ceus as an alternative to cta in the annual routine examinations were assessed . 
for the entire surveillance period , we assumed that no patient should be re - operated . for economic analysis , differential costs of ceus and cta were considered ( defined as the sum of equipment , materials and staff costs ) according to the modalities of examinations in our institute based on the activity - based costing ( abc ) method and similarly as other papers in the literature [ 1719 ]  . 
medical staff cost estimated at 1.02 per minute , depending on the time required for each examination ( medical history , informed consent , examination and report ) , and obtained from the sirm document determining activity volumes of radiologists [ 16 ]  . 
after the first year , main causes of failure of evar procedure are endoleaks , a reperfusion of the excluded aneurysm sac , and endotension , defined as high pressure within the aneurysm sac [ 1 , 3 ]  . although mechanisms underlying these complications are unclear and there is no agreement on the therapeutic approach , radiologists play a crucial role in endoleak diagnosis and treatment . 
1 at ceus , in the axial ( a ) and sagittal scans ( b ) , an endoleak of type ii ( arrow ) is depicted posteriorly to the right branch of the endoprosthesis . 
 in the same site ( arrow ) , a leak of iodinated contrast material is demonstrated by means of ct angiography in the mip images on the axial ( c ) and coronal planes ( d ) results confirm the accuracy in post - evar follow - up ; the failure to identify three endoleaks was correlated with intrinsic limitations , such as patients constitution or intestinal interposition . 
it must be underlined that the average bmi of patients enrolled was not far from reference values , allowing the radiologist to easily perform a reliable ceus exam in the majority of cases . however , cta can not correctly diagnose all endoleaks , as the hypodynamic ones , due to slow flow of exile lumbar arteries . 
correct evaluation of the diameters of excluded aneurysm sac is decisive because an increase in pressure inside the excluded bag , and consequently an increase in its caliber , may confirm the suspicion of endoleak . 
in this regard , despite the sample is relative small , we found a nonsignificant difference between ceus and cta in diameters determination , both for correctly excluded sacs and for those with endoleak . our activity - based cost analysis showed that ceus could provide significant savings compared to cta for the management of these patients and could make the basis for an alternative follow - up protocol in the future . as previously suggested [ 17 19 ] , it is clear that activity - based cost analysis is merely the first step in a cost - effectiveness analysis that encompasses diagnostic benefits , including effects on treatment and biological costs . the economic factor along with advantages of ceus ( low invasiveness , high tolerance , absence of ionizing radiation and safety in subjects with renal insufficiency ) makes it an alternative to cta for post - procedural follow - up [ 15 ]  . however , cta offers some advantages : relatively nonoperator dependent , not conditioned by physical constitution , provides information on endograft implantation , integrity , migration , distortion , length and diameter of the neck ; it remains the gold standard examination for first year of postevar follow - up . 
consequently , in a reasoned follow - up , cta should be performed only in patients with the increase in sac diameter or for the detection of endoleak before surgery [ 14 ]  . 
on the opposite , cta has some drawbacks including radiation exposure , that may represent a problem in long - term follow - up , and iodine contrast material administration that could represent a contraindication in patients with renal impairment . this study suffers from several limitations . 
second , activity - based costing ( abc ) analysis is only a part of the health tecnology 1 3 la radiologia medica ( 2018 ) 123 : 904909 908 fig . 
 for example , it may be difficult to observe deeply situated lesions , in particular in obese patients ; moreover , bowel gas interposition and the presence of diffuse mural calcification could obscure the penetration of ultrasound beam resulting in a poor acoustic window . 
second , compared with ct or mri , the performance of ceus is more strongly influenced by the experience of the investigator and by patient - related factors ( cooperativeness )  . it should be noted that in our study , we recorded a higher incidence of endoleak than the literature ( 1540% ) conclusions in conclusion , ceus is an accurate and a cheap imaging method in post - evar follow - up patients , and it could be considered as a valid alternative to cta , after the first year of negative controls , reducing the number of unnecessary ct examinations . 1 3 la radiologia medica ( 2018 ) 123 : 904909 compliance with ethical standards conflict of interest all the authors declare that he / she has no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent for ceus , ct and mr was obtained from all individual participants included in the study . 
based on dicom standard , the dose information of digital radiological equipment can be collected in various ways , for example , by analysis of dicom headers , by optical character recognition of the patient record , by dicom - modality performed procedure steps ( mpps ) or by dicom - radiation dose structured report ( rdsr )  . 
the rdsr in particular is a hierarchically structured document encoding all relevant radiation exposure information , both for accumulated and per single irradiation event ; it enables easy and universal comprehensive dose monitoring for dicom modalities [ 1 , 2 ]  . 
brotzu , cagliari , italy 5 medical physics department , usl toscana nord ovest , 6 medical physics unit , european institute ofoncology , lucca , italy milan , italy be defined as dose archive and communication system ( dacs )  . italian law requires the recording of all imaging and treatment procedures performed with ionising radiation [ 3 ]  . 
the latest eu council directive 2013 / 59 / euratom ( bss ) [ 4 ] strengthens requirements for recording and reporting doses from radiological procedures ; it states that member states shall ensure that information relating to patient exposure forms part of the report of the medical radiological procedures . 
likewise , the alara ( as low as reasonably achievable ) principle for dose optimization must be applied in all cases and the diagnostic reference levels ( drls ) [ 5 , 6 ] have to be regularly reviewed . 
with rdim , statistical analysis of dosimetric indices can be performed 7 medical physics department , istituto scientifico san raffaele , milan , italy 8 medical physics department , a.u.s.l. 
piacenza , piacenza , 9 medical physics unit , ats - assl sassari aou sassari , italy sassari , italy 10 medical physics department , fondazione irccs policlinico san matteo , pavia , italy 11 radiation diagnostics department , a.o.u. 
mauriziano , turin , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 944951 effortlessly , for example , to comply with the methodology of drls . 
similarly , the dose outliers can be immediately detected and investigated . from a healthcare management perspective , collecting patient dose data on a large scale could be conceived as the keystone for a medical radiation dose registry , which could be used for risk assessment and epidemiological studies . 
 the international atomic energy agency ( iaea ) initiated the smart card project in 2006 [ 8 ] to develop a template for tracking the number and type of radiological procedures and , wherever possible , dose for individual procedures . 
in italy , to the authors knowledge , no similar initiative is present . it has been proven that sharing the analysis of dose indices within a multi - institutional environment can be effective for dose optimization [ 9 ]  . 
to that purpose , the rdim systems are valuable tools to easily obtain statistical indices and dose distributions based on a large number of data . this work reports the first results of a project promoted by the italian association of medical physics ( aifm ) aimed to test , in a multicentric context , the efficacy of using rdim software in pointing out the needs for dose optimization . 
 although the project involved different radiological modalities , this paper concerns ct data only . materials andmethods rdim system through the aifm network of medical physicists , a commercial company ( tecnologie avanzate , turin , italy ) promoted a limited number of trial versions of a rdim software to thirteen centers for 6months . 
 the software version that was used at the time of the project provided the following metrics : ctdivol , dlp , ssde ( for body protocols ) at scan level ; total dlp , namely dlptot , and effective dose e at study level . 
the dose indices include ctdivol weighted by scan length , namely ctdivol w / acq , an examination - level dose index useful to compare studies with multiple series , and it coincides with ctdivol for studies with one scan or multiple scans with equal length . 
a tool is available for the user to manually merge protocol names into master protocols , to bypass the problem of protocol name variability , due to the lack of a standard nomenclature . 
several statistical tools are available to filter and analyze data on the basis of multi - criteria searches , for example by protocol , procedure , equipment , date range , user , etc . 
the histogram bin - width is user - defined ; it cannot be lower than a minimum of 1mgy for ctdivol , and a minimum of 50mgycm or 100mgycm for dlptot , depending on the amount of data . 
these reference values can be automatically assigned on the basis of the statistical distribution ( for example , above maximum , above average , etc . ) or they can be configured by the user . data collection andanalysis centers were located in a wide geographical area of northern and central italy , and sardinia ( 9 , 2 and 2 , respectively )  . 
 within the limit of the number of available licenses of the rdim system , 19 ct scanners were selected to be representative of all major vendors and different years of installation ( see table1 )  . 
the accuracy of the ctdivol values displayed by the ct console was verified in each center to be within the maximum tolerance value ( < 20% ) [ 13 ]  . 
a list of common ct examinations performed on adult patients ( > 18years old ) for most frequently scanned anatomical regions ( head , chest , abdomen ) was selected . 
protocols included were : head ct ( routine head , brain , head for trauma ) , chest ct ( routine thorax , high resolution lung hrct , pulmonary angiography ) , abdomen ct ( single phase and multiphase , colonography , kidneyureterbladder ) , spine ( cervical , lumbar , lumbar - sacral )  . 
feedback reports were then provided to centers to compare their performance against the overall dose index distributions and against other participants . although the drl definition was not a priority of the project , the mean , median and 75th percentile of ctdivol and dlptot were evaluated from the overall distributions , based on the anatomical regions of the head , chest and abdomen and compared with recently published values . results the results of the software testing process were successful in each institution . 
a small percentage of spurious cases ( less than 2% on average ) had to be manually excluded from analysis , due , for example , to examinations performed under wrong protocol definitions , or outliers of dose indices related to special cases ( for example test images )  . 
given the large amount of data to be checked in each institution , some spurious cases were overlooked during data collection , while a tukeys test was performed to detect outliers to be reviewed . a large variability between ctdivol distributions was generally observed among the ct units , both for median values , ranges and shapes . 
it is worth observing that in fig.1b the minimum and maximum correspond to the newest ( 2015 ) and oldest ct ( 2006 ) equipment , respectively . figure2a , b shows the ctdivol boxplots for hrct and ct for pulmonary embolism , respectively . 
for hrct in particular , the lowest ctdivol values were observed for one scanner ( ct7 ) , which was unequipped with iterative reconstruction algorithnevertheless , the effect of iterative vs fbp reconstruction algorithm could be recognized . 
the acquisition protocols of these cts were similar except for the image reconstruction algorithm , which resulted in a statistically significant ctdivol reduction ( about 40% ) , as proved by a wilcoxon rank test . the overall distribution of ctdivol and dlptot for the examinations of head , thorax and abdomen is shown in fig.4 , where the mean , median , 25th and 75th percentiles are reported . 
table2 summarizes the observed values for ctdivol and dlptot , in comparison with published values from a previous italian survey [ 14 ]  . discussion significant work is required to manage the large amount of data collected by rdim software . 
to ensure data consistency , a preliminary standardization of ct acquisition protocols is needed to avoid errors and misinterpretation of results , as recently pointed out [ 15 ]  . 
despite protocol standardization , a certain amount of inconsistencies are nevertheless to be expected , due , for example , to mistakes in loaded protocols or last minute changes of the ct scanning parameters . 
on the other hand , a few of these anomalous events do not have the potential to significantly affect the large set of data collected by rdim software and the related statistical indices . a large variability of ctdivol for similar acquisition protocols was observed , especially for examination of the head ( fig.1a ) which resulted in a range of about one order of magnitude . 
1 boxplot intercomparison of ctdivol distributions from different ct scanners , head ( a ) and thorax ( b ) acquisition protocols ( distributions with less than 50 cases are not shown ) reported from a multicentric study [ 16 ]  . 
 this is related both to patient attenuation and to the way the current is modulated over the scan range , which ultimately depends on the atcm technique implemented by the manufacturer [ 18 ]  . 
indeed , comparing dose distributions of different equipment can in principle be useful to test atcm on a real anthropomorphic basis . in this investigation , the intercomparison between centers was able to trigger dose optimization . 
the age of the equipment generally affects dosimetric performance , as apparent in fig.1b , where the highest and lowest ctdivol median values are related to the oldest and newest ct units , respectively . 
2 boxplot intercomparison of ctdivol distributions from different ct scanners , hrct ( a ) and pulmonary embolism ( b ) acquisition protocols ( distributions with less than 50 cases are not shown ) la radiologia medica ( 2018 ) 123 : 944951 the urinary tract , as shown in fig.3 , where a dose reduction of about 40% , was found , in agreement with recent literature [ 19 ]  . not only technological but also human factors play an essential role in reducing exposure . 
in particular , this was observed in thorax hrct ( fig.2a ) , where the lowest exposure values were related to one ct unit ( ct7 ) not equipped with iterative algorithms . 
in fact , in this case , the radiologists had heavily reduced mas , while preserving a diagnostic quality , in order to reduce radiation risk for patients with lung disease undergoing follow - up scans . for head examinations , results for ctdivol and dlptot are in substantial agreement , although slightly lower , with published drls [ 14 ]  . 
for single - phase abdomen protocol , the median ctdivol was in perfect agreement with that published in the italian survey ( 18mgy ) , while it was not possible to compare dlptot , because of inconsistencies in the number of phases ( one phase for our study , all phases for [ 14 ] )  . 
for thorax cts , the 75th percentile of ctdivol ( 11mgy ) was about 27% lower than the value found in the italian study ( 15mgy ) , but it is similar to the value of 10mgy recently found from data collected by four ct scanners [ 20 ]  . 
indeed , the italian survey was based on data collected in 2010 , while in our investigation more than half ( 57% ) of the involved ct units were installed after 2010 . 
3 boxplot intercomparison of ctdivol distributions from two equal manufacturer / model ct scanners , without and with iterative reconstruction algorithm ( ct17 and ct6 , respectively ) for kidneyureter bladder acquisition protocols atcm systems , which could be particularly effective for the low - density lung region , although further analysis is needed to confirm this assumption . this study proved the feasibility of setting up an italian multi - institutional network aimed at dose optimization in ct and showed that sharing statistics of dose indices in a multi - equipment context can be useful for dose optimization at an institutional level . only a limited number of ct units could be monitored for a limited time , due to software license restrictions ; thus , the variability of dose indices could not be further investigated . 
due to lack of connection with ris and the hospital informative system , detailed information about the procedures and the patients ( i.e. , clinical indications or bmi ) were not available . 
moreover , at the time of data collection , the software version did not provide organ dose and water equivalent - based ssde [ 21 ] ; therefore , patientspecific dose analysis was not possible . conclusions rdim systems are valuable tools for dose optimization in radiology departments . 
on the other hand , to be fully effective , rdim systems require accurate management of acquisition protocols and data analysis by an expert multiprofessional team ( radiologists , technologists , medical physicists )  . 1 3 950 la radiologia medica ( 2018 ) 123 : 944951 fig . 
4 overall distributions of ctdivol and dlptot for common examinations of standard head , thorax and abdomen acquisition protocols ( all data ) 1 3 la radiologia medica ( 2018 ) 123 : 944951 table 2 comparison of the results of this study and drls from an italian survey [ 14 ] ctdivol ( mgy ) dlptot ( mgycm ) mean median 75th mean median 75th head thorax abdomen 61.8 ( 64 ) 9.1 ( 12 ) 14.3 ( 15 ) 58 ( 60 ) 8 ( 12 ) 12 ( 14 ) 66 ( 69 ) 11 ( 15 ) 18 ( 18 ) 1201 ( 1223 ) 451 ( 620 ) 893 ( 653 ) 1100 ( 1041 ) 350 ( 416 ) 700 ( 580 ) 1300 ( 1382 ) 550 ( 754 ) 1100 ( 843 ) acknowledgements the authors would like to thank guido catolla , barbara mongero , enrico rinaldi of tecnologie avanzate ( turin , italy ) for providing the rdim software to participants of the study . 
 the authors also express their appreciation for the support given by aifm presidents , luisa begnozzi and michele stasi for the initiative . collaborators pintacuda giovanna ( 14 ) , aliberti camillo ( 15 ) , andreini daniele ( 16 ) , argiolas giovanni maria ( 17 ) , bassani laura ( 18 ) , dedola giovanni luca ( 19 ) , fasolini giorgio ( 20 ) , figoli davide ( 21 ) , gallo teresa ( 22 ) , gigliotti carmen rosaria ( 7 ) , lafe elvis ( 23 ) , loria alessandro ( 7 ) , profili stefano ( 24 ) , rosenberg ilan ( 25 ) , scomazzoni francesco ( 26 ) , solitro federica ( 27 ) , stefanini teseo ( 28 ) ( 14 ) veneto institute of oncology iov - irccs , padua , italy , radiology department ; ( 15 ) azienda ospedaliera universit di padova , s.c. 
 brotzu , radiology department , cagliari , italy ; ( 18 ) usl toscana nord ovest , radiation diagnostics department , lucca , italy ; ( 19 ) usl toscana centrofirenze s.o.c. 
radiologia san giovanni dio digd , firenze , italy ; ( 20 ) asst papa giovanni xxiii bergamo , dipartimento immagini , bergamo , italy ; ( 21 ) a.u.s.l. 
two radiologists with different experience performed a double - blind retrospective evaluation of the images , classifying the patients in the two groups by using only single specific signs ; then , the images were reviewed in consensus with a third radiologist and sensitivity and specificity were calculated . 
subsequently , the frequency of every single sign and of every possible combination of nonspecific signs in the two groups was registered , to find combinations present only in the surgical group ; sensitivity and specificity were calculated by using even those specific combinations . results at the first consensual evaluation , sensitivity and specificity were 75 and 100% , respectively . 
two combinations of nonspecific signs ( focal wall thickening + extraluminal air ; focal wall thickening + seat belt sign ) were found only in surgical patients that did not present any single specific sign : sensitivity calculated adding those two combinations was 95% , without a decrease in specificity . conclusions mdct is an accurate technique in the evaluation of blunt surgically relevant bmis . 
nevertheless , they present high morbidity and mortality rates , which may vary depending on the association with other solid abdominal organ lesions , severity and on the involved hollow viscera [ 13 ]  . 
the mortality is higher in case of perforation of hollow viscera that can complicateif not correctly diagnosedwith peritonitis , acute renal failure , ards and sepsis [ 1 ]  . 
in patients with isolated lesion of hollow viscera , the mortality increases with the delay of their arrival into the operating theater ( within 8h , 2% ; 816h , 9.1% ; 1624h , 16.7% ; more than 24h , 30.8% ) [ 1 , 2 ]  . abdominal pain due to peritoneal irritation is the most frequent clinical sign , although it is not a specific finding and may not be present during the clinical examination of the patient , since clear signs of peritonitis may not appear for hours [ 4 ]  . 
moreover , in patients with concomitant head or spinal injury , it can be difficult to evaluate its presence [ 4 , 5 ]  . clinical management of polytrauma patients depends on their hemodynamic stability or instability [ 6 , 7 ]  . 
computed tomography ( ct ) due to its accessibility , rapid image acquisition and accurate assessment of multiorgan lesionshas established itself since the 1980s as the first choice imaging technique in evaluating hemodynamically stable polytrauma patients [ 8 , 9 ]  . ct is regarded as highly accurate in depicting abdominal solid organs injuries . 
however , the diagnostic potential of ct in revealing bowel and mesenteric injuries remains controversial [ 1013 ] with a sensitivity that varies from 55 to 87% [ 11 , 14 ] and specificity between 88 and 92% [ 10 , 11 ]  . 
nowadays , ct examinations can not only correctly identify bowel and mesenteric lesions , but can also discriminate injuries that need immediate surgical attention ( major lesions : full thickness laceration of bowel wall , la radiologia medica ( 2018 ) 123 : 891903 laceration that involves the serosa and muscularis propria but not the mucosa , active mesenterial bleeding , vessel injury with ischemic bowel lesions ) from injuries that can be managed conservatively ( minor lesions : mesenteric hematoma without active bleeding , bowel wall hematoma , laceration of the serosa ) [ 3 , 14 ]  . multiple ct signs of bowel and mesenteric injuries have been described in the literature [ 3 , 4 , 6 , 1421 ]  . 
some of them ( bowel wall discontinuity , the cutoff sign , active bleeding and vascular signs ) [ 3 , 4 , 6 , 1423 ] are specific of surgical injuries ; however , they have a low sensitivity . 
other findings , that are more frequent ( extraluminal air , focal bowel wall thickening , focal bowel wall enhancement changes , mesenteric hyperdensity , seat belt sign and free abdominal fluid ) [ 3 , 4 , 6 , 1425 ] , have a low specificity , since they may be observed also in case of nonsurgical injuries . as the presence of a combination of signs increases the likelihood of clinically important injuries that necessitate surgical management [ 4 , 26 ] , the aim of this paper was to identify combinations of nonspecific signs useful for the diagnosis of major lesions in patients that do not have any single specific sign . materials andmethods patients the surgical group patients were selected upon review of the records of all patients who underwent surgery for traumatic abdominal injury from january 2005 to october 2014 at the department of general surgery of our university hospital . 
 twenty - two patients with surgically proven bowel and / or mesenteric injuries were included in this group : two of them were taken directly to operating room due to the severity of the clinical conditions without first having a mdct ( both of them died during intervention ) ; the remaining 20 patients had first a mdct followed by laparotomic surgery ( 19 male and 1 female , mean age 47.4years , range 1887years )  . 
we included all the digestive tract injuries from the stomach to the rectum ( table1 )  . table 1 localization of bowel and / or mesenteric surgical injuries ( 20 patients ) bowel mesentery bowel and mesentery ileal loop = 2 iv part of duodenum = 1 jejunum = 1 ileal loop + sigma transection - 1 transverse mesocolon = 7 sigma mesentery = 2 ileal mesentery = 1 tot = 5 patients tot = 10 patients mesocolon + colon splenic flexure = 1 ileal mesentery + jejuneal loop + descending colon transection = 1 sigma mesentery + left colon = 1 ileal mesentery + ileal loop = 1 ileal mesentery + last ileal loop + right colon = 1 tot = 5 patients 1 3 la radiologia medica ( 2018 ) 123 : 891903 the control group was selected from ct images of 96 patients that arrived at the emergency department of our hospital after a blunt abdominal trauma : it encompasses 34 patients ( 29 male and 5 female , mean age 44.8years , range 1592years ) , without bowel or mesenteric injuries that needed surgery at the ct exam and during clinical follow - up but presenting with other organ injuries . 
we used high - concentration cm ( iobitridol 350mg i / ml , xenetix 350 , guerbet , villepinte , france ) administered with an automatic injector having a constant infusion velocity of 2.53ml / s ; a flush of 40ml of saline solution with the same infusion velocity followed the cm injection . 
arterial phase was acquired at 3540s after cm injection , venous phase at 90s and delayed phase at 5mfive of the 20 patients in the surgical group had a repeat ct , in 3 / 5 cases after 68h and in 2 / 5 cases after 3days , for a total of 25 examinations : in 12 / 25 cases , a four - phase examination was performed in basal , arterial , venous and delayed phase ; in 9 / 25 fig . 
1 study flowchart 1 3 894 la radiologia medica ( 2018 ) 123 : 891903 cases , a three - phase examination was performed in basal , arterial and venous phase ; and in 4 / 25 cases , a basal phase was followed by a venous and delayed phase . 
in the control group , 16 / 34 patients had a four - phase examination , 15 / 34 had a three - phase examination , 2 / 34 had a basal and venous phase scanning , and in one case a basal , venous and delayed phase scanning was performed . 
oral contrast medium was not administered [ 6 ]  . in the surgical group , the ct examination was performed on average 6h after the patients arrival at the emergency room ( range 15min48h )  . 
only in one case , which was actually transferred from another hospital , the trauma occurred 10days before the ct examination . images analysis two radiologists with different experience in abdominal imaging retrospectively and independently reviewed the ct examinations of the 54 patients : a staff radiologist with an 8years of experience in abdominal imaging ( expert radiologist ( er ) ) and a iv year resident ( r )  . 
 the observed signs were then reviewed in consensus with a third radiologist to resolve possible disagreements . subsequently , the frequency of each single specific or nonspecific sign in the two groups was evaluated in consensus . 
finally , the frequency of the various pairs of nonspecific signs was also computed , in order to assess their distribution and identify possible specific combinations ( i.e. , present only in patients of the surgical group )  . statistical analysis first , sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy for both the individual reviews of the two radiologists ( er ; r : table2 ) and the consensus review with the third radiologist ( table3 ) according to the presence of single specific signswere calculated . after the consensus evaluation , sensitivity , specificity and accuracy of each ct sign ( table4 ) and of all the possible pair combinations of the nonspecific signs ( table5 ) were computed . 
 finally , sensitivity , specificity , ppv , npv and accuracy derived from the images review integrating single specific signs with specific pair combinations were calculated ( table6 )  . furthermore , the chi - square test was used to evaluate the statistical significance of the presence of free fluid in the surgical group and the control group . 
the t student test was used to evaluate the statistical significance of the different free fluid mean density between the two groups . results in the group of 20 patients with bowel and / or mesenteric injuries that needed surgical treatment , 5 / 20 had a bowel lesion , 10 / 20 had a mesenteric injury , 5 / 20 a combined bowel and mesenteric injury , and 3 / 20 had a double bowel lesion ( in two different locations of the intestinal tract ) for a total of 28 lesions ( 13 bowel lesions and 15 mesenteric lesions )  . 
the values refer to identifying patients with bowel and / or mesenteric injuries that required urgent surgery ( 20 ) , patients with bowel injuries ( 10 ) and patients with mesenteric injuries ( 15 )  . 
 moreover , the nonspecific signs ( specificity < 100% : pneumoperitoneum , bowel wall enhancing pattern , focal bowel wall thickening , mesenteric hyperdensity , free abdominal fluid , seat belt sign ) presented a higher sensitivity ( range between 20 and 90% )  . 
2 ct after cm administration ( venous phase ) , coronal oblique mpr image : cutoff sign caused by a complete transection of descending colon with segment diastasis ( arrows ) ; thin hematoma between the proximal and the distal segment ( asterisk ) 1 3 la radiologia medica ( 2018 ) 123 : 891903 fig . 
c repeated contrast - enhanced ct , performed after 8h ( venous phase ) , axial mpr image : thickening and hyperdensity of the cecum wall ( arrows ) associated with multiple mesenteric air bubbles ( arrowheads )  . 
transection of the ileocolic vascular peduncle causing double transmural ischemic lesion of the distal ileum ( not seen at ct ) and of the cecum was found at surgery a statistically significant difference between the mean density value of free fluid in the two groups was registered using the t student test : 27.7 hu in the surgical group versus 16 hu in the control group ( p = 0005 )  . some pairs of nonspecific signs were identified as specific pairs ( table5 ) , since they were present only in the surgical group patients . 
some of themextraluminal air + contrast enhancement variations , extraluminal air + seat belt sign , contrast enhancement variations + seat belt sign were associated with single specific signs ; other pairsfocal bowel wall thickening + extraluminal air ( fig.6 ) and focal bowel wall thickening + seat belt sign ( fig.7 ) were found in patients requiring surgery which did not have any single specific sign . 
furthermore , the other 4 / 5 cases showed , at the retrospective evaluation , signs of major trauma on the first ct examination , which were not interpreted correctly at the prospective evaluation by the radiologists on duty . in the era of mdct , all exams must be performed with a high - resolution protocol , with slice thickness and reconstruction interval values equal to 1mm and completed by multiplanar reconstructions [ 22 ]  . generally , a pre - contrast medium phase is useful to evaluate the attenuation values of abdominal organs , in order to identify or rule out active bleeding and assess any abnormal changes of attenuation values in the subsequent phases after cm injection [ 15 , 16 ]  . a two - phase ct examination after cm injection , in arterial and venous phase , is advisable , in order to identify the presence of active bleeding or a major vessel injury [ 15 , 16 , 28 , 29 ]  . 
if a minor vessel injury or a slow flow bleeding is suspected , a delayed phase acquisition should be added to the ct exam protocol [ 6 , 30 ]  . 
5 ct after cm administration ( venous phase ) , axial mpr image : wall thickening of the ascending colon ( arrow ) associated with free fluid in the lateroconal fascia and retro colonic fascia ( arrowhead ) ; free fluid can also be seen in the ileal mesentery ( empty arrow )  . 
as the ct pattern was compatible with an intramural hematoma of the right colon , the patient was treated conservatively with resolution of the clinical symptoms ( pain on the right side ) and of the radiological signs discussion bowel wall defect . 
if this particular combination had been used as a discriminating factor between patients that were candidates to surgery and those that were not , it would have led to the correct placement of the false - negative patient reported in table6 , thus fig . 
6 a , b ct after cm administration ( venous phase ) , consecutive axial mpr images : thickening of ileal loops , showing a fair contrast enhancement ; air bubbles are seen nearby ( the extraluminal air can be recognized better in the cranial scan )  . 
jejunal perforation was found at surgery 1 3 la radiologia medica ( 2018 ) 123 : 891903 finally in some cases , although the patients have a negative ct or a ct suggesting minor trauma upon arrival in the emergency room , a second ct exam should be performed if the clinical conditions worsen . 
it is useful to repeat the ct examination after 68h to evaluate the evolution of signs , especially in bowel trauma [ 16 ] , since a longer delay can jeopardize the patients outcome ; oral cm is also recommended when an intestinal perforation is suspected . ct signs of bowel or mesenteric injuries after blunt abdominal trauma have already been described in various papers and reviews [ 3 , 4 , 6 , 1421 ]  . 
more recently , a few papers have analyzed the meaning of several signs like free fluid [ 35 , 36 ] , extraluminal air [ 24 , 25 , 27 ] or described new sings indicating transection of hollow viscera [ 23 ]  . 
moreover , the radiologist not only identifies the trauma signs , but also provides an estimation of its severity for an adequate treatment planning , surgical or conservative [ 14 , 22 ]  . 
we can distinguish between signs indicating bowel trauma or mesenteric trauma , both specific and nonspecific of surgical injuries . bowel signs specific signs it is well known that the most specific diagnostic sign for a perforation of hollow viscera is the bowel wall discontinuity ( and in case oral cm is being used the extravasation of the latter )  . 
in our series , a wall laceration was found in 15% of the cases . the paper published by cho [ 23 ] mentions also the cutoff sign , expression of a complete bowel transection : in their series , 8 cases of transection were described and the sign was present in all cases , having a 100% sensitivity . 
our series encompasses two cases of bowel transection , but the cutoff sign was present in only one case ( left colon lesion ) on ct , having a sensitivity of 5% ( 1 / 20 ) when considering the whole 20 patients in the surgical group , but of 50% when we consider only the patients with a complete transection . nonspecific signs extraluminal air has been considered for years as a feature for hollow viscera injury , having sensitivity values ranging from 20 to 75% [ 3 , 4 , 15 , 20 ]  . 
7 ct after cm administration ( venous phase ) , axial mpr image : distal ileal loop showing a thickened and hyper - dense wall associated with free mesenteric fluid showing a triangular morphology ( asterisk )  . 
8 ct after cm administration ( venous phase ) , axial mpr image : emphysematous bubbles ( long arrows ) inside the muscles leaning against the inferior right ribs , caused by an important thoracic trauma , associated with a small gas bubble along the liver margin ( short arrow )  . 
the thoracic trauma combined with the absence of bowel wall lesion signs allowed to classify the air along the liver margin as benign extraluminal air [ 31 ] have argued against the usefulness of a delayed phase , concluding that it should not be inserted in the routine ct protocol of polytrauma patients , but should be acquired only in the suspicion of abdominal injury in the previously acquired phases , in order to detect vascular and urinary tract injuries . 
in our series , it was necessary for the diagnosis in only 5% of cases ( 1 / 20 )  . the use of oral cm has been an ongoing debate argument for years [ 3034 ]  . 
nowadays , because it is believed that the disadvantages are greater than the advantages ; therefore , it should be used only in selected cases . 1 3 900 la radiologia medica ( 2018 ) 123 : 891903 [ 4 ]  . 
it is important to accurately evaluate all the acquired scans in the less striking cases , as the presence of extraluminal air may not be evident at the basal phase but can accumulate in time , therefore becoming evident in the venous or delayed phase [ 4 ]  . however , in the recent years its specificity has been disputed , due to the presence of free peritoneal air coming from other districts , especially in patients with rib fractures , major subcutaneous emphysema of the thoracic wall , diaphragm lacerations , pneumothorax or pneumomediastinum , intraperitoneal rupture of the urinary bladder with an indwelling foley catheter . 
air coming from these districts can reach the peritoneal cavity , causing false - positive cases [ 4 , 33 ]  . thus , it is not possible to consider extraluminal air as only present or absent : in a recent study of 74 patients with free extraluminal air on ct , 38 of them were referred to surgery and 11 laparotomic surgeries were not necessary , whereas the remaining 36 had conservative treatment [ 25 ]  . 
 therefore , other evaluations are necessary : some authors think that the amount of extraluminal air is not as important as the location and dimension of the air bubbles for differential diagnosis between benign air and injury - predicting air ; particularly , the presence of air bubbles in front of the liver is a sign of benign air [ 25 ]  . 
moreover , hefny [ 24 ] underlines the air bubble dimensions : if they are less than 10mm , they predict benign air ; in this paper , only two patients from 21 that presented extraluminal air on ct had a bowel injury and they both presented multiple air bubbles ( 10mm or more in diameter )  . 
therefore , authors of the above - mentioned papers conclude that extraluminal air alone is not a sign that requires an urgent laparotomic surgery but should be correlated with other clinical signs [ 24 ] , or associated with other ct signs of bowel injury , free fluid ( in the absence of solid organ injury ) and the clinical and / or radiological seat belt sign [ 25 ]  . another potential error can be the presence of pseudopneumoperitoneum , that is , when the air is trapped between the abdominal wall and the parietal peritoneum , mimicking a true pneumoperitoneum [ 22 ]  . 
pseudopneumoperitoneum may be found in patients with injuries to the extraperitoneal segments of the rectum , rib fractures , pneumothorax or pneumomediastinum [ 4 ]  . on the other hand , the absence of free air does not exclude an intestinal perforation ; henfy reports in his paper that of the 398 patients that did not present with extraluminal air only two had a laceration of a bowel loop . 
this can occur for many reasons : the perforation may be contained or may partially seal spontaneously , developing ileus prevents passage of gas into abdominal cavity , or small gas collections may rapidly be reabsorbed through the peritoneal lining . in our series , the sensitivity of the extraluminal air sign was 40% . 
on the other hand in the nonsurgical group , extraluminal air was identified in 3 / 34 cases ( table4 ) : the gas bubble morphology , their location , the presence of thoracic injuries ( pulmonary contusions , rib fractures ) and especially the lack of other ct signs indicating bowel injuries ( in particular the absence of focal bowel wall thickening ) allowed a correct diagnosis of benign air . focal bowel wall thickening it can suggest the presence of a complete transection or a lesion that does not require surgery ( a wall hematoma ) [ 20 ]  . 
moreover , there does not exist an absolute cutoff value that is considered pathological ( generally 34mm ) [ 5 ] , due to the lack of distension of jejuno - ileal loops . 
therefore , a comparative analysis of the bowel loops located near the suspicious - looking loop is imperative in order to evaluate the difference in thickness . furthermore , a diffused thickening of small bowel wall can be an expression of wall edema due to a systemic water overload ( after hemodynamic stabilizing maneuvers ) , or due to splanchnic hypoperfusion ( shock bowel )  . 
other signs of hypoperfusion ( reduced vena cava diameter , adrenal hemorrhage , peri - pancreatic edema ) or hyperhydration signs ( peri - portal edema ) are also present [ 3 , 4 , 37 ]  . 
in our series , focal wall thickening was observed in 55% of cases in the surgical group and in 5.8% of cases in the nonsurgical group . focal bowel wall enhancement changesincreased or decreased indicates a vascular involvement . 
the increase in enhancement , if diffuse , can also be part of the shock bowel complex [ 3 , 4 , 37 ]  . in our series , focal changes in enhancement were identified in 30% of cases in the surgical group versus 5.8% of cases in the nonsurgical group . cho [ 23 ] described another sign called the janus sign thatassociated with the cutoff signis highly suggestive of bowel wall transection . 
this sign , that is the presence in the same bowel loop of increased and decreased bowel wall enhancement , was not observed in our series in the two cases of complete bowel transection . 1 3 la radiologia medica ( 2018 ) 123 : 891903 mesenteric signs specific signs the diagnosis of a hematoma with active bleeding is quite simple , even more when all the phases are acquired on the ct scan ( basal , arterial , venous , delayed ) , making it possible to identify an arterial and sometimes a venous vessel laceration [ 38 ] causing progressive cm collection inside the hematoma [ 28 , 29 ]  . 
this ct sign was present in 50% of cases in our surgical group . the vascular signs ( beaded appearance and abrupt vessel termination ) were first described by atri etal . 
 [ 14 ] that considered them as having a reasonable sensitivity ( 60% ) and specificity for mesenteric vascular involvement , but also as predictive signs for an ischemic bowel wall lesion [ 3 , 5 , 14 , 35 ]  . 
abrupt vessel termination can be caused by a traumatic dissection or a direct vessel laceration ; also , beaded appearance or mural irregularities , usually surrounded by mesenteric stranding , indicate injury of the vessel wall [ 14 , 39 ]  . however , the frequency of these signs reported by atri etal . 
in our experience , conducted with a 40 - row scanner associated with mpr and mip reconstructions of high quality , their frequency was not so high ( 25% )  . 
in our series , the association of these signs was observed in only one case in the control group , having a good specificity ( 97% ) but a low sensitivity ( 25% )  . 
we discuss mesenteric hyperdensity combined with abdominal free fluid in the next paragraph . bowel andmesenteric signs the radiologic seat belt sign , especially when associated with extraluminal air , is highly predictive of a major abdominal injury . 
in mareks series [ 25 ] , its frequency was reported in 24% of the 38 / 74 patients that had surgery and in none of the patients in the control group ( 36 / 74 that had conservative treatment with a specificity of 100% )  . 
in our series , the seat belt sign was observed in 4 / 20 patients of the surgical group and in 13 / 34 patients in the control group , having a sensitivity of 20% and a specificity of 61.7% , rather lower compared to mareks data [ 25 ]  . 
on the other hand in our series , the association of this sign to other nonspecific signs of loop injury ( especially focal bowel wall thickening ) although rare ( 20% ) proved to be specific for a major loop lesion . 
 the same result was also reported by marek [ 25 ]  . free abdominal fluid is the less specific sign in the diagnosis of bowel and / or mesenteric lesions but also the most sensitive one ( sensitivity 100% , specificity 26% [ 14 , 40 ] )  . 
 [ 35 ] analyzed the amount and density of free fluid in bowel trauma comparing it to the same data in a trauma patient group that did not have a reason for the free fluid ascertainable on ct . 
in our series , which is not comparable to yus study due to a different composition of the control group , a statistically significant difference was found between the mean density value of the free fluid in surgical patients ( 27.7 uh ) and the control group patients ( 16 uh ) ; we did not find a significant difference when comparing the amount of free fluid in the two groups . we can conclude that free abdominal fluid , especially when located among the bowel loops ( triangle sign [ 4 ] ) in patients without solid organ injury , must raise suspicion of a bowel and / or mesenteric lesion . 
nevertheless , its presence should be associated with other signs in order to guide the diagnosis [ 4 ] ; furthermore , it does not necessarily suggest a major trauma : in our series , free fluid was present in 3 of the 4 patients with bowel and / or mesenteric trauma that were treated conservatively . 
therefore , this ct sign suggests a watchful waiting and , in case the patients clinical conditions worsen , a ct exam should be repeated after 6 / 8h [ 24 ]  . 
on the other hand , the absence of free fluid strongly suggests the absence of surgically important bowel or mesenteric injuries [ 14 ]  . in our experience , the free fluid and mesenteric hyperdensity association had a moderate sensitivity ( 75% ) and specificity ( 73.5% ) in distinguishing between surgical and nonsurgical patients . 
this association to select surgical patients would have made possible the correct diagnosis as a surgical patient of the fn case by both radiologists , but with a decrease in specificity from 100 to 73.5%. msct has an established high reliability in depicting abdominal organs injuries . 
however , the diagnostic potential of ct in revealing bowel and mesenteric injuries remains controversial , especially in the discrimination of major 1 3 902 la radiologia medica ( 2018 ) 123 : 891903 lesions that need surgery from minor ones which can be treated conservatively , with variable sensitivity values ranging from 53% up to 8795% [ 1114 ]  . 
among the data published in the literature , the sensitivity values are very different , in relation to the use of different ct scans but also depending on the type of lesions . 
in fact , there are a higher number of false - negative cases in patients with ischemic bowel injuries that have greater risk of delayed diagnosis with consequent poorer outcome [ 41 ]  . the results of our series show a sensitivity of 75% , a specificity of 100% and an accuracy of 91% in the consensus review obtained by using only single specific signs ( bowel wall discontinuity with the cutoff sign , active bleeding and vascular signs )  . although le bedis [ 4 ] and soto [ 26 ] state that the association of more ct signs can be useful to detect major trauma , to our knowledge there is no paper that evaluates the diagnostic gain provided by using combined signs . 
in this paper , we analyzed also every possible pair of nonspecific signs , in order to find pair combinations that could be useful for the diagnosis of major trauma . 
in particular , two of them ( focal bowel thickening + extraluminal air and focal bowel thickening + bowel wall hematoma ) were found in patients without any single specific sign , being reliable for the diagnosis of surgically relevant lesions . indeed , sensitivity and accuracy values are higher ( 95 and 98% , respectively ) , without a decrease in specificity , when for the diagnosis the specific pairs of nonspecific signs are used along with the single specific signs , especially in case of bowel injuries . our study has some limits . 
second of all , we did not include all patients that had an abdominal trauma during this period of time , since it is a casecontrol study in which the positive patients were recovered from the surgical records . 
third of all , only four minor injuries that were treated conservatively were present in the control group ; this certainly influenced the specificity values that would have been lower if there had been more minor injuries in the control group , as is the case of atris study [ 14 ]  . 
finally , radiological and clinical correlation was poor ; in fact , it was difficult to establish an association between the imaging and the clinical data ( abdominal pain , acute abdomen , etc . ) , because the clinical data were gathered retrospectively from the clinical files . in conclusion , even with the above - mentioned limits , our study demonstrates that mdct is an accurate imaging technique in detecting patients with surgically relevant bowel and / or mesenteric injuries . 
the most frequent abnormality at chest x - rays was bronchial wall thickening , observed in 88.5% of the cases ; radiological findings are faint in the 25% of the cases ( 29 / 114 patients )  . 
in nine subjects with a normal chest x - ray , unenhanced ct with a quantitative analysis was performed , and depicted features consistent with constrictive bronchiolitis . conclusion measles may produce bronchiolitis and pneumonia . 
in the cases in which involvement of pulmonary parenchyma is not sufficient to result in radiological abnormalities , ct used with a dedicated postprocessing software package , provides an accurate lungs and airways analysis , also determining the percentage of lung involvement . keywords measles pneumonia bronchiolitis conventional radiography computer tomography computer tomography quantitative airway analysis introduction measles is one of the most highly contagious , directly transmitted viral disease caused by a single - strand rna virus , member of the morbillivirus genus in the family paramyxoviridae , more frequent in children , usually associated with permanent immunity . 
it is mainly spread by direct contact with airborne respiratory droplets , and is transmitted normally from 4days before to 4days after the onset of rash , with an incubation period of 1014days . 
between 1 march 2017 and 28 february 2018 , 28 european union ( eu ) member states reported 14 , 813 cases of measles ; most of the cases were reported by italy ( 5039 ) , romania ( 4481 ) , greece ( 1851 ) and france ( 1175 ) , accounting for 34 , 30 , 12 and 8% , respectively , of all cases reported by eu countries [ 7 ]  . 
complication of measles include pneumonitis , encephalitis , super - imposed bacterial infections and , later , subacute sclerosing panencephalitis [ 9 ]  . pulmonary disease is one of the most common complications , its occurrence is reported between 3 and 57% [ 1217 ] , and accounts for most measles - associated deaths [ 1 ]  . 
demographic data , vaccination status , clinical features and laboratory values of the patients were extracted from medical records . patients underwent postero - anterior and lateral chestx rays , because of clinical reasons ( dyspnea , shortness of breath , cough )  . computed tomography ( ct ) scans were obtained without intravenous contrast material , using a 16detector row helical ct system ( bright speed ; ge medical systems , milwaukee , wis ) with the following parameters : 70120kv , 80120ma , a table speed of 5mm per rotation , a pitch of 1.378. 
the nonenhanced scans were reconstructed at collimations of 1.5mm , and reviewed on a picture archiving and communication system workstation ( agfa healthcare )  . the spectrum of conventional radiographic and ct findings evaluated encompasses : ground glass opacity ; consolidation ; nodules , micronodules , and tree - in - bud opacities ; interlobular septal thickening ; bronchial and / or bronchiolar wall thickening . a ground - glass opacity is an increased lung attenuation in which vessels remain visible , due to coexisting thickening of the interstitium and partial filling of the airspaces ; consolidation is complete filling of the airspaces which results in obscuration of vessels . nodules are small mass rounded , 110mm in diameter , interstitial nodules are soft tissue attenuation with well - defined borders ; alveolar nodules are centrilobular dense attenuation or ground - glass opacity with ill - defined borders . the tree - in - bud finding reflects the presence of dilated and impacted centrilobular bronchioles . 
bronchiolar wall thickening may result in smooth , nodular or irregular thickening of the peribronchovascular interstitium , with a ratio of the bronchial wall thickness to the bronchus diameter > 0.2 or in comparison of another lung region . furthermore , all ct raw data was transferred to advantage workstation ( aw ) , where thoracic vcar imaging software ( ge medical systems , milwaukee , wis ) was used for lungs and airways analysis . 
this advanced tool provides quantification of hounsfield units ( hu ) and a color - coded display of the thresholds within the lungs , automatically producing quantitative measurements of the involvement . 
in this way , the extent of ground glass opacities and the bronchiolar involvement were evaluate and were quantified on each ct section using an automated density mask technique in which voxels with attenuation values between specific thresholds are highlighted . the cut - off levels between normal lung density and abnormal attenuation lung was defined as 742 and 381hu . 
the percentage of high attenuation was automatically calculated for the whole lung . patients were considered to have pulmonary involvement if they had any of the following features : bronchial wall thickening , parenchymal attenuation disturbances , ground - glass attenuation , air - space consolidation , small centrilobular nodules , and / or pleural and mediastinal lymph node involvement . all images were independently analyzed by two boardcertified radiologists ( vs , fa , with 30 and 6years of experience in chest imaging ) ; disagreements in image interpretation were resolved by consensus . results two hundred ninety patients with clinical diagnosis of measles confirmed by serological assays were admitted to our hospital in the study period . 
most cases were observed in the 1830years old bracket ( 45% )  . among these patients , 97% had not been vaccinated or have received only one dose of vaccination , nobody referred to have had measles during childhood . 
two patients were immunocompromised , due to leukemia and to immunosuppressive therapy with biologic agents for crohn disease , two patients were infected with hiv , six patients presented a chronic liver dysfunction , two patients presented a rheumatological disease ( lupus erythematosus and rheumatoid arthritis ) , one had multiple myeloma and one presented multiple sclerosis and high blood pressure . 
six patients were diabetic ( three patients have also blood hypertension ) , one was obese , six have blood hypertension . one hundred fifty patients ( 52% ) underwent chest - x rays for clinical reasons ( dyspnea , shortness of breath , cough )  . chest imaging allowed the diagnosis of pulmonary involvement in 114 of 150 patients ( 76% ) , in 30 out 39 ( 74% ) of the patients with immunocompromission or comorbidities . the most frequent radiological features were bronchial / bronchiolar wall thickening , observed in 88.5% of the case ( 101 / 114 patients ) , with or without centrilobular nodules ; ground glass opacities ; interlobular septal thickening ; parenchymal consolidation ; pleural effusion . 
in 29 of these 101 patients ( 29% ) , chest - x ray findings were very faint and a consensus reading made the diagnosis . in detail we observed : diffuse bronchial / bronchiolar wall thickening ( fig.1 ) in 53 patients ( faint in 25 subjects , moderate in 21 , severe in 7 ) ; diffuse bronchial / bronchiolar wall thickening with centrilobular nodules ( fig.2 ) and tree in bud in 13 patients ( faint in 5 and severe in 8 subjects ) ; bronchial / bronchiolar wall thickening in the lower lobes in 15 patients ( faint in 11 subjects and moderate in 4 subjects ) , associated with smooth interlobular septal thickening ; patchy ground glass opacities with centrilobular nodules of ground glass in 6 patients ( fig.3 ) ; combination of both , interstitial and alveolar disease with focal parenchymal consolidation in 14 patients ( 6 with associated pleural effusion )  . 
in eight of the latter patients pneumonia / bronchopneumonia involved the left lower lobe , in three subjects the left upper lobe , in one in the upper lobes , in one lower lobes and in one patient there was patchy air - space consolidation throughout the lungs . in the remaining 13 patients , chest x - rays showed multiple focal parenchymal consolidations , scattered throughout the lungs . we observed mediastinal lymph node enlargement in two patients . among the 150 patients with chest imaging , 17 patients ( 11% ) , with rapidly progressive respiratory illness , underwent volumetric thin - section ct to determine whether and / fig . 
 among those patients , 9 ( 6% ) presented normal findings at chest radiography . in eight patients , ct confirmed chest - x ray findings , with focal parenchymal consolidations involving lower lobes , and bilateral pleural effusion . among the 9 cases with normal chest - x rays ( fig.4ac ) , ct depicted moderate lower lobes bronchial / bronchiolar wall thickening in 4 cases , and faint bronchiolar wall thickening and diffuse lung lucency only in the remaining 5 1 3 938 la radiologia medica ( 2018 ) 123 : 935943 volume hu interval value gamma right lung volume left lung volume total - 950 hu - 1024 / - 742 hu 71 , 78% 73 , 04% 72 , 36% / 2 , 43 l > - 950 hu - 742 / - 381 hu 21 , 92% 20 , 02% 21 , 05% / 0 , 70 l - 381 / 3071 hu 6 , 29& 6 , 92% 6 , 58% / 0 , 22 l 1 3 la radiologia medica ( 2018 ) 123 : 935943 fig . 
d thoracic vcar imaging software : quantitative analysis shows the percentage of high attenuation ( > 950 hu ) automatically calculated for the whole lung in patient with diffuse involvement consistent with bronchiolitis and normal chest x rays patients . 
in these latter four patients thoracic vcar imaging software , used on post processing , demonstrated diffuse involvement consistent with bronchiolitis ( fig.5 ) , characterized by a wall thickening due to inflammation around bronchioles , without tree in bud opacities , centrilobular nodules or mosaic perfusion . discussion pneumonia is one of the most common measles complications , and its occurrence is reported between 3 and 57% [ 1217 ]  . 
in our series , 52% ( 150 / 290 ) of the patients diagnosed of measles presented respiratory symptoms , so that underwent chest imaging which allowed pneumonia diagnosis in 82% of these cases ( 123 / 150 patients ) , 42% of the whole study patients ( 123 / 290 ) , with a higher percentage of compared to the literature data . the prevalence of measles virus pneumonia is higher in pregnant women and patients who are immunocompromised due to leukemia or lymphoma , acquired immunodeficiency syndrome ( aids ) , or immunosuppressive therapy [ 18 ]  . in our measles series , most of the patients have not been vaccinated or experienced measles during childhood ; 39 patients presented immunocompromission or comorbidities , among these patients 30 ( 74% ) were affected by lung involvement . measles pneumonia accounts for most measles - associated deaths and the reported mortality rates in adult measles pneumonitis vary considerably , from 1% up to 36% [ 1 , 19 ]  . 
various histopathologic patterns of lung injury have been described in viral pneumonia , more often nonspecific . most respiratory viruses produce cytopathic effects , and in severe cases necrotizing bronchitis / bronchiolitis characterized by exudates within bronchiolar lumen , or even bronchiectasis , and diffuse alveolar damage , which can be hemorrhagic ; the histologic features are epithelial necrosis of the airways with mononuclear infiltration of alveolar walls , and fibrinous exudates in the alveoli [ 2426 ]  . histologically measles virus pneumonia is characterized by multinucleated giant cells in the alveolar air spaces and within the bronchiolar and tracheobronchial epithelium [ 24 ]  . epithelial hyperplasia and diffuse alveolar damage , with air spaces filled with fluid and cellular inflammatory infiltrations produce the radiological features of primary measles pneumonia [ 25 , 26 ]  . the radiologic findings reflect the variable extent of these histopathologic features , and are dependent on several host factors , including age and underlying immune status ; risk factors associated with increased frequency and severity of viral infections include very young and old age , malnutrition , and immunologic disorders [ 27 , 28 ]  . based on imaging features it can be difficult to differentiate viral pneumonia , as a measles lung involvement , from other pathological processes , above all infectious . 
however , radiographic findings in combination with clinical findings improve the accuracy of diagnosis in viral lung involvement . the spectrum of radiological findings encompasses ground glass opacity and consolidation ; nodules , micronodules , and tree - in - bud opacities ; interlobular septal thickening ; and bronchial and / or bronchiolar wall thickening . 
because of the associated bronchiolitis , hyperinflation is commonly present [ 2023 , 29 , 30 ]  . when there is high clinical suspicion of pneumonia , and chest radiographs demonstrate normal or questionable radiographic findings , patients undergo ct , which can be more sensitive and specific than chest radiographs , depicting even very faint abnormalities , like the parenchymal attenuation disturbances , recognized in some viral infections [ 2831 ]  . the parenchymal attenuation disturbances are seen on ct scans as mosaic attenuation pattern , that refers to the presence of areas of varying decreased attenuation [ 31 ] in this cases caused by alveolar hypoventilation because the bronchioles inflammation produces obstruction , which leads to secondary vasoconstriction and under perfused lung . the differential diagnosis of viral lung involvement is broad and includes many causes of pulmonary diseases , even noninfectious [ 3238 ]  . 
ground - glass opacity and consolidation may be observed in patients with fungal or bacterial infection , in pulmonary edema , pulmonary hemorrhage , hypersensitivity pneumonitis , respiratory bronchiolitis , organizing pneumonia , and alveolar proteinosis . 
a tree - in bud appearance is more often associated with airways infection , including tuberculosis , nontuberculous mycobacteria bronchopneumonia , however , there are several noninfectious causes of tree in bud appearance . 
b thoracic vcar imaging software color - coded display , shows interstitial thickening 1 3 la radiologia medica ( 2018 ) 123 : 935943 mucoid impaction in asthma , allergic bronchopulmonary aspergillosis , and aspiration . 
the parenchymal attenuation disturbances may also be observed with bacterial and fungal pneumonia , and in noninfectious disease including vascular disease and some diffuse infiltrative diseases . atypical measles pneumonia occurs after exposure to natural measles virus in patients with previous measles immunization which killed measles virus vaccine [ 39 ]  . 
in these case is a presumed hypersensitivity response in incomplete immunized patient or may be due to a superimposed bacterial process [ 39 , 40 ] ; however , some cases were also reported in patients without previous measles immunization [ 40 ]  . atypical measles pneumonia is more severe and shows a lobular or segmental infiltration with hilar lymphadenopathy and frequently pleural effusion [ 41 ]  . 
in our series , we did not observe . although measles virus can cause pneumonia in a significant percentage of infected patients , pneumonia is often due to bacterial infection that occurs because of the immune suppression induced by measles [ 15 , 16 ]  . 
haemophilus influenzae is the most common organism of the secondary bacterial infection in typical measles cases [ 13 ] , usually associated with lobar pneumonia . chest - x ray is the diagnostic tool of choice for determining measles pulmonary involvement , and findings of primary measles virus pneumonia are mixed reticular opacities and air - space consolidation . ct plays a supportive role in its diagnosis and helps to exclude other causes . the spectrum of ct findings encompasses the classical viral pneumonia features , including bronchial wall thickening , patchy inhomogeneities in the attenuation of lung parenchyma , caused by hypoventilation of alveoli distal to bronchiolar obstruction due to inflammation , and the socalled parenchymal attenuation disturbances , ground - glass attenuation , air - space consolidation , and small centrilobular nodules [ 2031 ]  . however , radiological abnormalities that reflect airwaycentric disease are non - specific and must be interpreted in conjunction with clinical information . 
in our series , 6% of the cases ( 9 / 15 ) , all with progressive respiratory illness , chest - x rays was normal . in these 7 patients , we used ct not only for pneumonia assessment but , coupled with sophisticated postprocessing technology , also for the functional quantitative assessment of lung density , to emphasize and quantify even the most subtle bronchiolar or alveolar abnormalities . any cellular and / or fluid content increase in the interstitial or in the lung parenchyma , results indeed in increased attenuation of pixels relative to the low attenuation of air , and in hypoventilation of alveoli distal to bronchiolar inflammatory obstruction . however , when this involvement is very faint , the use of a ct program density mask , suitable to indicate areas of ground glass and bronchiolar wall thickening , improves the imaging performance , because the software is able to provide measures that reflect changes in attenuation , indirect measures of the parenchymal changes [ 4244 ]  . 
our results showed that adult patients with measles , who had normal chest radiographs , had ct density features which could be related to a constrictive bronchiolitis . radiological evidence of lymph node enlargement in adults is uncommon and according with the literature data , in our series we rarely observed lymphoadenomegalies in two patients . this study has several limitations ; foremost because only 150 patients underwent chest imaging , some patients with lung involvement may have been missed . 
on the other hand , all the patients with respiratory distress , clinically evaluated , underwent chest x - ray . furthermore , there are inherent limitations due to the lack of transtracheal aspiration . 
in the cases , in which the microbiological culture of sputum was performed , it was negative and also the urinary pneumococcal and legionella tests were negative in all but one patient who was affected by pneumococcal pneumonia . 
moreover , a pre - existing pulmonary disease was documented in ten patients , but we cannot exclude that more patients presented an unaware pulmonary disease that could have affected the lung imaging . 
in conclusion , because pneumonia is the most common serious complication of measles and respiratory failure , the most common cause of death , it is important to determine the degree of involvement in all adults with measles , even those with normal pulmonary auscultation findings . it is possible that measles can diffusely involve the lung parenchyma , but not sufficiently to result in radiological abnormalities . 
we found both an obstructive cad at ca and myocardial edema at cmr in 53.2% of patients , while 8.5% of patients had a non - obstructive cad and no edema . 
furthermore , in 6 of the edema - positive patients with multi - vessels obstructive cad , cmr identified myocardial edema in a vascular territory different from that of the lesion supposed to be the culprit at ca . conclusions in a non - negligible percentage of nstemi patients , t1 and t2 mapping detect myocardial edema without significant stenosis at ca and vice versa . 
however , these sequences have well - recognized limitations , including incomplete blood suppression along the subendocardium , regional variations in signal intensity due to phased array coil inhomogeneities and signal dropout due to myocardial motion , and rely on subjective visual interpretation [ 13 ]  . recently , t1 and t2 mapping have demonstrated a better performance than traditional stir sequences in myocardial edema identification [ 2 , 47 ]  . the prevalent mechanism underlying the increase in myocardial t1 and t2 values in acute myocardial infarction ( mi ) is likely related to the increase in tissue mobile water content ( i.e. , myocardial edema ) that involves the ischemic as well as the infarcted myocardium [ 8 , 9 ]  . the majority of t1 / t2 mapping studies in ( mi ) were focused on st - segment elevation myocardial infarction ( stemi ) patients [ 4 , 10 ]  . 
however , in non - st - segment elevation myocardial infarction ( nstemi ) , myocardial changes are expected to be milder than in stemi , and the performance of t1 and t2 mapping sequences might be lower in this clinical setting . 
moreover , in acute nstemi patients without high - risk features , invasive management is often postponed for up to 72h [ 1113 ] and cmr can be obtained within this interval . 
cmr may play an important role in confirming the diagnosis and may identify the culprit territory as well as the presence of large non - viable myocardiu this unique information can be useful for a correct planning of the percutaneous coronary intervention ( pci )  . in a recent study [ 14 ] , t1 and t2 mapping have demonstrated higher diagnostic performance than stir sequences in the identification of the culprit lesion in a cohort of nstemi patients . in this study , the vast majority of patients were imaged after coronary angiography ( ca )  . 
moreover , recent studies have suggested that the extent of edema may change during the first week after mi [ 16 , 17 ] , with an initial reperfusion - related wave of edema that decreases at 24h followed by a second wave , related to healing processes , in the succeeding days . 
consequently , data obtained days after the invasive management might differ from those obtained in an earlier phase , when cmr might be utilized in the clinical decisional process . materials andmethods study population fifty - four patients who met the standard diagnostic criteria for acute nstemi [ 13 ] , awaiting early ca and showing a rise in high - sensitivity cardiac troponin t ( hs - ctn - t ) level above the 99th percentile , were enrolled from january 2013 to may 2018 . 
a clinical history of previous mi was not an exclusion criterion . four patients were subsequently excluded because cmr evidenced an imaging pattern suggestive of acute myocarditis ( n = 3 ) and takotsubo cardiomyopathy ( n = 1 )  . 
t1 mapping was performed utilizing a modified look - locker inversion recovery ( molli ) pulse sequence [ 3 ] with a 3 - 3 - 5 pattern ( three images in the first two look - locker segments and five images for the third inversion , with three recovery heartbeats between acquisition episodes )  . 
truefisp cine images were evaluated regarding wall motion abnormalities ( 1 , normal ; 2 , hypokinesia ; 3 , akinesia ; 4 , dyskinesia ) , and the wall motion score index ( wmsi ) was calculated as the sum of segmental scores divided by 17 . 
the transmural extent of contrast enhancement within each segment was defined visually according to the following scheme : 0 = no enhancement , 1 = 125% , 2 = 2650% , 3 = 5175% , 4 = 76100% enhancement extent referred to the myocardial wall thickness [ 20 ]  . 
furthermore , one reader ( c.t. ) measured t1 and t2 values in both the infarcted myocardium ( im ) and the remote myocardium ( rm ) , defined as the unaffected segment contralateral to the im , by drawing regions of interest ( rois ) over the maps . 
myocardial edema in the inferobasal segment ( arrow ) is clearly demonstrated in t2 map obtained in 2ch view ( a ) as well as in t1 ( b ) and t2 ( c ) maps obtained in short - axis view . 
coronary angiography ( e ) shows a subocclusive stenosis of the right coronary artery ( arrow ) 1 3 la radiologia medica ( 2018 ) 123 : 926934 im to specific coronary artery territories according to standardized criteria [ 19 ] and taking into account the coronary anatomy evidenced at ca . coronary angiography ca was performed using standard techniques . 
no significant differences were found in ventricular function parameters and hs - ctn - t peak level neither between edema - positive and edema - negative patients nor between patients with and without an obstructive cad . 
it was subocclusive ( i.e. , > 90% ) in 25 of35 patients and critical ( > 80% ) in the other 10 subjects . pci was performed in 21 patients and coronary artery bypass graft surgery in 3 patients . 
in thirteen of them we found some segments with lge but without edema in t1 / t2 maps ; in agreement with clinical history and ca findings , lge in these segments was considered as being due to the previous infarcts . 
in the remaining 4 patients we found both lge and edema in segments that , accordingly to clinical history , had been previously infarcted . 1 3 930 la radiologia medica ( 2018 ) 123 : 926934 we also identified patients with myocardial edema without irreversible injury at lge : 3 ( 20% ) out of 15 lge - negative patients showed edema on t1 and / or t2 maps . cmr findings : acute myocardial injury int1 andt2 maps we judged 14 / 2% of all myocardial segments as non - analyzable in t1 / t2 maps , respectively , because of motion or off - resonance artifacts . edema was detected in 31 patients ( 65.9% ) when evaluating t2 maps and in 24 patients ( 51.1% ) when evaluating t1 maps . 
 in 6 of these patients ( 12.8% ) , all with multi - vessels disease , cmr identified myocardial edema in a vascular territory different from that of the lesion supposed to be the culprit at ca . 
furthermore , there were 12 patients ( 25.5% ) with obstructive cad and no edema at cmr , while in 6 ( 12.8% ) patients we found myocardial edema at cmr despite a non - obstructive cad at ca ( table2 )  . discussion in this study , we found that both t1 and t2 mapping enable the identification of myocardial edema in the majority of patients with nstemi , although some myocardial diseased segments were non - analyzable in t1 maps due to artifacts . 
2 boxplot of t2 ( a ) and t1 ( b ) values in the infarcted myocardium ( im ) , remote myocardium ( rm ) and in previously infarcted segments . 
furthermore , t2 values were significantly higher in acute infarct versus previously infarcted segments ( p < 0.001 ) , while the difference in t1 values between acute and chronic infarcts was not significant , and there was an overlap in t1 values between acute and chronic infarcts 1 3 la radiologia medica ( 2018 ) 123 : 926934 fig . 
coronary angiography reveals multi - vessel critical cad , involving both the left anterior descending artery ( subocclusive stenosis of the mid segment , followed by a complete occlusion of the apical segment ) ( arrows ) and the second diagonal ( proximal occlusive stenosis ) ( arrowhead ) ( a )  . 
in t1 map , on the contrary , t1 values were similar in acute ( 1154ms ) and chronic infarct ( 1151ms ) ( arrows ) ( d ) table 2 myocardial edema and obstructive cad in nstemi patients obstructive edema no edema cad coronary artery disease ; nstemi non - st - segment elevation myocardial infarction of patients there was an agreement between ca and cmr findings . 
 [ 14 ] in 73 patients , t1 and t2 maps evidenced myocardial edema in 88 / 86% of subjects , respectively . we found myocardial edema in a lower percentage of patients . 
these differences are likely to depend on the imaging protocol utilized . we have applied a classic molli sequence [ 3 ] and a widely used truefisp sequence [ 1 ] , and our results are in agreement with layland etal . 
on the contrary , fibrosis has only a minor effect on myocardial t2 [ 34 ]  . in a recent study [ 31 ] , both t1 and t2 maps provided excellent performance in discriminating between acute and chronic mi . 1 3 932 la radiologia medica ( 2018 ) 123 : 926934 in this study a mixed cohort of reperfused stemi and nstemi patients were evaluated at four time points from 8days to 6months after mi . 
however , in our opinion , data obtained when evaluating the evolution of a mi from the acute to the chronic phase may not necessarily be congruent with findings obtained when comparing different acute and old infarcts of varying levels of severity that coexist in a same patient . actually , t1 values in acute and chronic mi are expected to depend on the degree of edema and replacement fibrosis , respectively , and therefore , it is conceivable that t1 values in a small acute nstemi may be similar to t1 values in an old severe mi [ 35 ]  . 
accordingly , although mean t1 values were higher in acute than in previous mi , we found that in 3 patients with widespread previous mi , there was an overlap of t1 values in acute and old infarcts . in our cohort , the number of patients with previous infarcts is small ; however , our results highlight a possible limitation of t1 mapping in a real clinical scenario . although the majority of patients had both obstructive cad and myocardial edema , in a non - negligible percentage of patients ( 25.5% ) we found significant coronary stenosis without myocardial edema . 
embolization , resolution of thrombus before cmr or vasospasm can be speculated in these subjects . further studies are necessary to evaluate the long - term benefit of an early revascularization in patients without edema , as well as the possible role in risk stratification of myocardial edema when detected in patients without significant coronary stenosis . 
however , our results suggest that ca and t1 / t2 mapping might provide complementary information in the evaluation of nstemi patients , further supporting the role of cmr as an adjunctive tool , potentially useful in the clinical decisional process in this clinical setting . furthermore , we found that in some patients with multivessel disease , t1 / t2 maps evidenced myocardial edema outside the distribution of the coronary artery showing the most severe stenosis and supposed to be the culprit at ca . 
 this could suggest a potential role of t1 and t2 mapping in the invasive management of nstemi patients with multiple coronary stenosis , in which might be difficult to identify the culprit with ca [ 25 ]  . this study has some limitations . first , we enrolled a relatively small number of patients and we had to exclude high - risk patients , in whom immediate ca is mandatory . second , we did not include stir sequences in our standard protocol , given that it was already extensive for acute patients . 
however , previous studies have consistently found that t1 and t2 maps have a better performance than stir sequences in myocardial edema detection [ 2 , 47 , 14 ]  . furthermore , although we performed a thorough evaluation of all myocardial segments , we did not obtain t1 / t2 maps in contiguous short - axis slices . 
in our opinion and in line with previous studies [ 2 , 7 , 14 , 32 , 36 ] , our choice is a good compromise between the need to obtain a full coverage of the ventricles and an excessive lengthening of the examination time in acute patients . 
however , we cannot exclude that the performance of the maps in the detection of subtle myocardial edema might further ameliorate by increasing the number of slices . this also prevented us from computing volume and mass of myocardial edema , given that there are significant cautions regarding the accuracy of this quantification when utilizing non - contiguous slices [ 37 ]  . finally , during ca we did not utilize functional tests like fractional flow reserve ( ffr ) to determine the likelihood that coronary stenosis caused myocardial ischemia . 
moreover in our series all culprit lesions are subocclusive or critical , and correlation between ca and ffrisstrong in such severe stenosis [ 38 ]  . conclusions in a non - negligible percentage of nstemi patients , t1 and t2 mapping detect myocardial edema without significant stenosis at ca and vice versa , and in some cases with multi - vessel disease cmr may better specify the infarctrelated artery territory . 
therefore , t1 and t2 mapping might provide information complementary to ca in the evaluation of acute nstemi . compliance with ethical standards conflicts of interest authors carlo tessa , jacopo del meglio , alessio lilli , stefano diciotti , luca salvatori , marco giannelli , claudio vignali and giancarlo casolo declare that they have no conflict of interest . 
however , at least one gadoxetate disodium arterial phase without motion artifacts and adequate for acquisition timing , was acquired in all mr examinations . conclusion the incidence of breath - hold failure and acute transient dyspnea after gadoxetate disodium administration increased during the third arterial phase only . 
multiarterial phase imaging has been shown able to improve the detection and differential diagnosis of hypervascular focal liver lesions [ 3 ]  . gadoxetate disodium and gadobenate dimeglumine are widely used in liver mr for their added value in hepatobiliary phase imaging [ 2 ]  . 
the key advantage of gadoxetate disodium is the acquisition of hepatobiliary phase within vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 910917 20min after intravenous administration , compared to the time 90 to 120min necessary for hepatobiliary phase imaging after gadobenate dimeglumine administration [ 4 ]  . on the other hand , the clinical practice and some observational studies reported an increased incidence of artifacts in the arterial phase due to breathing difficulties after gadoxetate disodium administration . 
 [ 5 ] firstly reported an association between gadoxetate disodium and an acute self - limiting dyspnea that can have a deleterious effect on arterial phase mr image quality ; other authors defined that phenomenon transient severe motion [ 6 ] or breathlessness due to long breath - time [ 7 ]  . 
irrespective of its definition , this event can even lead to severely degraded gadoxetate disodium arterial phase images in 18% of mr examinations , resulting in some cases in nondiagnostic imaging [ 5 ]  . 
many studies investigated the causes of this phenomenon [ 811 ] , and several approaches have been applied to reduce motion artifacts : ( a ) lowering the contrast injection rate [ 12 ] , ( b ) using multiple arterial phase technique [ 6 ] , ( c ) shortening the scanning time [ 7 , 13 ] , ( d ) using a modified breathing command [ 14 ] , and ( e ) diluting contrast medium [ 15 , 16 ]  . 
 [ 17 ] recently reported a reduced arterial phase breath - holding duration in healthy volunteers administered with gadoxetate disodiubased on these contradictory data and on the fundamental importance of gadoxetate disodium as contrast agent in liver mr , we designed an observational prospective interindividual study to evaluate the incidence of motion artifacts , breath - hold failure and acute transient dyspnea , and the variation of clinical parameters [ oxygen saturation ( sato2 ) and heart rate ( hr ) ] , in patients undergoing liver mr with the multiarterial phase ( controlled aliasing in parallel imaging results in higher accelerationcaipirinha algorithm ) technique . materials andmethods this observational prospective single - site study was approved by the institutional review board , and it was compliant with the health insurance portability and accountability act . 
written informed consent was obtained from all subjects prior to study initiation . subjects data were collected from 250 consecutive patients who underwent gadoxetate disodium - enhanced liver mr , according to current medical practice and inclusion criteria , from july 2014 to march 2015 . 
in total , 128 of them were cirrhotic patients , 73 were patients who developed liver lesions during the follow - up for oncologic diseases , and 49 were patients with incidental hepatic lesions . 
the multiarterial phase image acquisition has been started 810s after the visual detection of contrast material at the celiac artery with the real - time bolus display method ( care bolus ; siemens healthcare ) : the celiac artery was visualized about 15 s after injection ; then , the first , the second , and the third arterial phases were acquired 2328 , 2934 , and 3539s after injection , respectively , anyhow defining an appropriate arterial phase acquisition . 
during saline injection , the arterial phase acquisition has been started 15s after the start of the injection . for each patient , the examination included a saline arterial phase followed by a gadoxetate disodium arterial phase . 
in the present study , we took advantage of this procedure by also collecting the subjective feelings and analyzing the image quality of the saline arterial phase , in order to evaluate whether the injection procedure itself can lead to a discomfort and / or motion artifacts . 
in this way , we were able to evaluate the effect of gadoxetate disodium on 1 3 912 la radiologia medica ( 2018 ) 123 : 910917 occurrence of adverse events ( in particular breathing difficulties ) , motion - related artifacts , and image quality in comparison with saline injection in an observational prospective interindividual study . clinical parameters andselfevaluation questionnaire sato2 and hr were measured by using a peripheral pulse oximeter prior , during , and after mr examination . 
for each imaging phase , the lowest sato2 and the highest hr were recorded . breath - hold during arterial phase acquisition was assessed by using the prospective acquisition correction technique ( pace ) monitors . 
the presence of sudden pronounced oscillations was considered indicator of poor breath - hold ( pace + ) , whereas graphs having a straight or slowly varying trend were considered physiological ( pace )  . after each injection ( saline and contrast medium ) , the radiologist asked to the patients whether they experienced any difficulties during the procedure and , if so , to briefly describe thethen , the radiologist reported the responses in the questionnaire . 
respiratory motion artifacts were classified by using the following 5 - point scale , as previously described [ 5 , 9 ] : 1 , no artifact ; 2 , minimal artifact with no effect on diagnostic quality ; 3 , moderate artifact with some effect but no severe effect on diagnostic quality ; 4 , severe artifact but images were still interpretable ; and 5 , extensive artifact and images nondiagnostic . 
we considered images with artifacts from 1 to 3 as good or degraded but still interpretable and images with artifacts from 4 to 5 as nondiagnostic images [ 5 ]  . statistical analysis continuous variables were tested for normality with the shapirowilks test : normal variables were expressed as mean standard deviation ; not normal variables were expressed as median plus interquartile range ( iqr 25th and 75th percentile )  . 
binary and categorical variables , reported as counts and percentages , were studied with the chi - square test ( with yates correction for 2 2 ) or with fishers exact test . 
 the average values of hr and sato2 during saline arterial phase and gadoxetate disodium arterial phase were also similar to the basal values ( fig.1 ) , with no statistical difference between saline and contrast agent ( table1 )  . the calculation of the fleiss kappa coefficient resulted in k = 0.82 , which indicates an almost perfect agreement between readers . 
for these patients , the radiologists reported either chronic cough , poor collaboration , poor breath - hold , or irregular breath - hold . among patients having both breath - hold failure and selfreported respiratory problems ( 6 of 250 ) , 2 patients ( 2 of 6 , 33% ) experienced transient dyspnea and 3 patients ( 3 of 6 , 50% ) had motion artifacts . 
although artifacts increased in the third phase of both pace + and pace patients , pace + patients had more artifacts than pace ones figure3 shows triple arterial phase imaging , with and without artifacts . discussion in this observational prospective interindividual study , we evaluated the incidence of acute transient dyspnea , breathhold failure , variation of clinical parameters ( sato2 and hr ) , and motion artifacts in patients undergoing gadoxetate disodium liver mr with multiarterial phase ( caipirinha algorithm ) technique . 
we also evaluated whether the procedure itself can affect the incidence of acute transient dyspnea and severe motion - related artifacts by comparing the gadoxetate disodium arterial phase with a saline arterial phase ; the acquisition of the saline arterial phase allows to reproduce the same sensation than contrast administration in terms of cooling / warming , noise during the real - time bolus display method , and duration of apnea during acquisition . 
although several studies have already investigated the association of gadoxetate disodium with motion artifacts and dyspnea , in the present work we hypothesized that the use of an optimized protocol ( including a multiple parallel acquisition technique ) in conjunction with a systematic comparison between data obtained after gadoxetate disodium administration and those observed after saline injection , could further elucidate the cause and rate of this phenomenon . caipirinha is a multiple parallel acquisition technique enabling shortened acquisition times while still maintaining adequate spatial resolution [ 18 , 19 ]  . 
 we found a similar rate of artifacts in the first ( p = 0.28 ) and second ( p = 0.09 ) arterial phase , whereas a significant difference between contrast agent and saline was found in the 1 3 la radiologia medica ( 2018 ) 123 : 910917 table 3 summary of the relevant data and results of the questionnaire for the 16 pace + patients . 
in the first table , we reported the data concerning the 10 patients who did not experience any difficulty during mr examination ( negative questionnaire ) age - sex duration of apnea ( s ) gadoxetate disodium dose ( ml ) phase motion artifacts ( presence and affected phase ) notes of the radiologist 75 - f 60 - m 70 - f 78 - m 68 - f 73 - f 74 - f 65 - m 61 - m 54 - m 45 - f 46 - f 64 - m 39 - m 56 - m 57 - m yes , 2nd yes , 3rd yes , 3rd yes , 3rd yes , 3rd yes , 1st yes , 3rd yes , 3rd restlessness no apnea ( hr > 90bpm ) chronic cough poor collaboration chronic cough poor breath - hold irregular breath - hold tachycardia ( hr > 110bpm ) poor breath - hold poor breath - hold ( hr > 85bpm ) yes , 3rd yes , 2nd and 3rd yes , 3rd transient dyspnea difficulty in breath - holding till the end of the acquisition transient dyspnea difficulty in breath - holding till the end of the acquisition nausea and difficulty in breath - holding hand burning sensation , fear age - sex duration of the apnea ( s ) gadoxetate disodium dose ( ml ) phase motion artifacts problems reported by patients for these patients , a brief note of the radiologist is reported in the last column . 
3 examples of triple arterial phase mr imaging without artifacts ( a ) and with artifacts in the third phase ( b ) 1 3 916 la radiologia medica ( 2018 ) 123 : 910917 last arterial phase ( p < 0.0001 ) , as some patients were unable to hold their breath for 1618s after gadoxetate disodium administration . 
we did not observe any variation of sato2 and hr in patients with breath - hold failure and / or self - reported respiratory problems either , confirming previous findings [ 11 , 17 , 20 , 21 ]  . 
therefore , these clinical parameters do not seem to be related to acute transient dyspnea and / or to severe motion artifacts . respiratory monitoring with pace system demonstrated that imaging artifacts were associated with breathhold failure ( p < 0.0001 ) in the third arterial phase only . 
therefore , acute transient dyspnea seems to be associated with breath - hold failure , but it does not necessarily lead to imaging artifacts . in previous studies [ 5 , 7 , 8 , 11 , 13 , 22 ] severe motion artifacts were found even in 17% of gadoxetate disodium arterial phase imaging , while breath - hold failure and / or acute transient dyspnea was observed even in 39% of gadoxetate disodium - enhanced mr examinations . 
furthermore , one placebocontrolled trial reported that 80% ( 35 of 44 ) of subjects had reduced maximal hepatic arterial phase breath - holding duration when administered gadoxetate disodium compared with both saline and gadoterate meglumine , and 27% ( 12 of 44 ) was unable to hold their breath for at least 20s after gadoxetate disodium administration [ 17 ]  . our results showed lower rates of breath - hold failure ( 6.4% ) and acute transient dyspnea ( 0.8% ) during gadoxetate disodium mr examinations . 
a possible explanation of these discrepancies could be the use of a lower dose of gadoxetate disodium in comparison with most of studies conducted in the usa [ 5 , 9 , 22 ] , where gadoxetate disodium is often administered at a higher , off - label dose . 
furthermore , we could not evaluate the impact of our protocol on gadoxetate disodium arterial phase in comparison with other contrast agents . in conclusion , by using caipirinha multiarterial technique , the incidence of motion - related artifacts increased during the third arterial phase only , thus allowing the acquisition of at least one arterial phase not compromised by motion artifacts and adequate for acquisition timing , in all patients . 
 nowadays , new specific receptor targeted pet tracers in prostate cancer imaging have been introduced ; one of the most used is 68ga - psma , that evaluates the expression of prostate - specific membrane antigen ( psma )  . 
the aim of this review article is , in the first part , to give an overview of the main indications and future development of 68ga - psma imaging , using pet / ct or pet / mri , according to the clinical course of the disease and in view of the current use of multiparametric mri ( mpmri ) and choline pet in the management of pca . 
in the second part , a brief overview of the promising 18f - labelled psma tracers and the current use of psma radionuclide therapy will be provided . keywords prostte cancer positron emission tomography magnetic resonance imaging prostate - specific membrane antigen introduction 18f - fdg is a well - known and established radiotracer used in oncology . 
however , when it comes to prostate cancer ( pca ) , an increase in glucose metabolism may be observed [ 1 ] only in rare cases , such as aggressive and undifferentiated pca . * angelo del sole angelo.delsole@unimi.it 1 residency programme innuclear medicine , university ofmilan , milan , italy 2 turku pet centre , turku university hospital , turku , 3 medical oncology unit , istituto scientifico romagnolo perlo studio e la cura dei tumori ( irst ) irccs , meldola , italy 4 department ofhealth sciences , university ofmilan , milan , finland italy 5 nuclear medicine unit , istituto scientifico romagnolo perlo studio e la cura dei tumori ( irst ) irccs , meldola , italy 6 nuclear medicine unit , ospedale san paolo , milan , italy pet tracers that target lipid metabolism , such as 18f or 11c - choline and 11c - acetate , whose incorporation into cell membranes is associated with the cell proliferation that occurs in pca , are currently considered accurate probes widely used in staging or in detecting biochemical recurrence , with a strict correlation with psa values [ 2 ]  . 
however , due to a limited sensitivity of 18f / 11c radiolabelled choline pet in patients with serum psa levels below 1.51ng / ml [ 3 ] , over the last few years there has been a shift in focus towards the development of more sensitive diagnostic imaging strategies based on the development of radiopharmaceuticals targeting the prostate - specific membrane antigen ( psma )  . psma is a transmembrane folate hydrolase protein that is overexpressed in the cell membrane of nearly all cases of pca and generally correlates with the gleason score , stage and tumour grade [ 1 ] , thus it may represent an ideal target for a radiopharmaceutical . 
the radiopharmaceutical production requires a 68ge68ga generator and can be performed easily through a fast complexing reaction that yields a stable product , without the need of an on - site cyclotron [ 4 ]  . 68gapsma pet inthedetection ofprimary tumour the standard workup to reach the initial diagnosis of pca is a digital transrectal exam followed by non - targeted multicore transrectal ultrasound ( trus ) - guided biopsy . 
this technique is associated with low diagnostic yield and limited sensitivity ( 48% ) in detection of clinically significant pca [ 7 ]  . moreover , the false negative rate is relevant ( 2147% ) [ 8 ] and the risk of overdiagnosis and therefore overtreatment of indolent pca is increased while up to 50% of clinically significant pca might be undetected [ 9 ]  . 
1 physiological distribution of 68ga - psma in a maximum intensity projection ( mip ) image image courtesy of turku pet centre , turku university hospital , turku , finland multiparametric - mri ( mp - mri ) , which is defined as a set of images with at least one more sequence in addition to the anatomical t1 and t2 - weighted images , such as diffusion weighted imaging ( dwi ) + apparent diffusion coefficient ( adc ) map and contrast - enhanced ( dce ) sequence , has demonstrated high specificity and variable but quite high npvs and sensitivity in the detection of pca , especially involving the transitional zone ( tz ) [ 1113 ]  . 
prostate imaging reporting and data system ( pi - rads ) was developed by the european society of urogenital radiology ( esur ) in 2012 to provide standardized guidelines for image acquisition and interpretation of mp - mri . 
the currently used pi - rads v.2 ( 2015 ) consists of a 5 - point scoring system based on selected criteria derived from an mpmri exam and assesses the probability of clinically significant pca [ 14 ]  . in the pi - rads version 2 , t2w imaging and dwi in combination with adc map are considered the central core in the mpmri examination , with dce sequence findings mostly used as a confirmation in equivocal cases . 
using this method , score 3 patients are dived in two sub - categories ( 3a and 3b ) according to the volume ( cut - off of 0.5cm3 ) in order to decide which lesion should be biopsied . even if mpmri remains the cornerstone in detecting and local staging of pca , the diagnostic performance of mpmri does not completely fulfil expectations in the initial diagnosis of clinically significant pca . 
in fact , the accuracy , sensitivity , and specificity ranges reported are very variable ( 4487% , 5896% , and 2387% , respectively ) [ 16 ]  . pet / ct with choline tracers has a limited value in the diagnosis of pca and most of the data in recent literature have demonstrated controversial results . 
some early studies have reported high sensitivity values of choline pet ( 98100% ) in pca detection and localization on a patientbased analysis [ 17 , 18 ] , but other studies have oppositely reported lower and limited sensitivities ( 6679% ) [ 19 , 20 ]  . 
 after performing invivo pet imaging , specimens of prostatectomy of 9 patients were scanned exvivo and the tracer distribution was compared after a 3 - dimensional voxel - wise with histopathology in localized pca . 
as the literature regarding this topic is still limited , new studies are needed to clarify the issue . 68gapsma pet inguiding biopsy procedures in recent years , biopsy performed with the combination of fused transrectal ultrasound and mpmri ( mpmri / trus ) has been increasingly used [ 25 ]  . 
axial t2 w , dwi , pet , and combined pet / mri images show the primary tumour of the right transitional zone ( a ) , with an extension to the seminal vesicles ( b )  . 
in fact cases of mri - undetected clinically significant pca ( around 20% ) have been reported [ 29 ] along with false negative results , especially when a mucinous component is present [ 30 ]  . a recent prospective trial [ 31 ] has evaluated the added value of pet / mri with 18f - choline for pet / mri / trus guided biopsy in 36 patients with suspected or known localized pca . 
in a study by storzt etal . , 16 patients with previous negative prostate biopsy underwent a fusion - guided transrectal biopsy of suspicious lesions detected with 68ga - psma - pet / mr [ 33 ]  . 
hopefully , in the near future , this application will be explored further with larger studies . 68gapsma intreatment planning ofprimary tumour establishing the extension of the primary tumour is crucial for treatment planning , such as surgery or radical radiotherapy . 
today , the use of intensity - modulated radiotherapy ( imrt ) an accurate tool with high sensitivity and specificity and promising low toxicity levels , and the simultaneous integrated boost ( sib ) for primary tumour and lymph node metastasishas increased [ 35 ]  . 
although ct is a well - established method in rt planning , mpmri is increasingly utilized today for radiotherapy planning in order to contour the primary tumours of patients before imrt [ 36 , 37 ]  . 
in this phase , the chance of the so - called oligometastatic disease should also be considered , which requires selected treatments as patients with oligometastatic disease can benefit from a metastasisdirected therapy , such as target rt for bone lesions or node metastasis [ 43 ]  . 
mpmri can be used in the local staging of suspect lymph nodes , despite its limitations , as almost 80% of metastatic lymph nodes in pca have a threshold diameter < 8mm , which is smaller than the one used in ct or mri to determine pathological lymph nodes ( 10mm ) [ 44 ]  . in this scenario , pet provides an additional value in primary nodal staging , particularly in patients with high - risk disease ( gleason score > 7 , psa > 20ng / ml , clinical stage t2c - 3a )  . the role of choline tracers in nodal staging of pca has been investigated , but the clinical application is impaired by its poor sensitivity ( range 3345% ) , even if associated with an excellent specificity ( over 95% ) [ 45 , 46 ]  . 
 68gapsma pet has shown higher pooled sensitivity at 70% ( 95% ci 5383% ) , and pooled specificity at 84% ( 95% ci : 2499% ) compared to conventional imaging with ct or mpmri [ 44 , 48 ]  . 
18f - sodium fluoride pet / ct can be used in the clinical practice to increase the accuracy , although it has been shown that the advantages of this method are poor [ 52 ]  . mpmri can be used in the evaluation of bone tissue involvement , especially because it provides a better spatial and contrast resolution within bone marrow than ct , so that metastasis may be identified before the osteoblastic reaction occurs [ 53 ]  . 
nearly 17% of pca patients after surgical treatment have a biochemical relapse , and psa serum valuethough commonly used as the first biomarker of biochemical recurrenceis not reliable enough because of its low specificity [ 59 ]  . detecting and recognizing the type of recurrence is crucial as it can guide different types of salvage treatments , such as lymphadenectomy or radiotherapy for loco - regional disease or adt and chemotherapy in a widespread disease [ 60 ]  . 
the patient then underwent salvage radiotherapy image courtesy of turku pet centre , turku university hospital , turku , finland 1 3 la radiologia medica ( 2018 ) 123 : 952965 fig . 
in the ct images , there are no morphological signs of the pathological lesion ( a ) image courtesy of turku pet centre , turku university hospital , turku , finland fig . 
for this reason , the analysis of the restriction of water diffusion in dwi imaging and even more the contrast enhancement on dce sequences are considered more reliable mri techniques in detecting local recurrence [ 63 ]  . 1 3 958 la radiologia medica ( 2018 ) 123 : 952965 choline pet / ct can increase the detection of relapse and provide better results than conventional imaging [ 64 ]  . 
they analysed 155 pca patients , who were referred to restaging , and observed that psa levels and psa doubling time ( higher serum psa values and short psadt ) are independent determinants of overall scan positivity and of detection of extra - pelvic lymph node metastasis . 
interestingly , the authors demonstrated that for psa values < 0 , 5ng / ml , a detection rate of 50% for 68ga - psma versus 12 , 5% for 18f - fluoromethylcholine , 69% versus 31% for psa values 0.52ng / ml and 86% versus 57% for psa values > 2ng / ml were recorded . 
the authors performed prostate - segment - based analysis specifically regarding the primary cancer lesion for four of such studies , and patient - based analysis specifically regarding pelvic lymph node metastases for four other studies . 
certain data comparing the performance of the two methods have suggested a more accurate lesion detection of 68gapsma pet / mri in suspected recurrent pca compared to pet / ct [ 72 ]  . 68gapsma pet inplanning salvage treatment afterrecurrence the assessment of biochemical relapse may lead to different types of therapy such as salvage radiotherapy or salvage lymphadenectomy , in case of local recurrence or isolated oligometastatic disease , and androgen deprivation therapy or chemotherapy in case of metastatic disease . as mpmri alone is not a valuable primary tool in guiding local salvage treatment with the limitations already mentioned , pet / ct and potentially pet / mri play a lead role in detecting recurrence in order to plan and monitor treatment , even if there is currently no consensus regarding the use of this imaging technique for salvage treatment guidance . choline pet has a limited sensitivity in the detection of biochemical recurrence , and is not considered useful to guide salvage treatment . 
besides , in the era of theranostics , reliable staging of pca with precise characterization of the extent of the disease and a differentiation of oligofrom poli - metastatic diseases would improve the treatment management of the patient . different types of adt therapy are currently used : surgical ( orchiectomy ) , medical , with lhrh agonist ( leuprolide , goserelin ) , with lhrh antagonist ( degarelix ) , or with antiandrogens ( flutamide , bicalutamide , enzalutamide )  . furthermore , other prognostic and predictive biomarkers and probes are also important due to the high heterogeneity of the disease at clinical and biomolecular levels [ 78 , 79 ]  . 
 over the last 5years , there has been a research boom on biomarkers and targeted therapies in pca including androgen receptor ( ar ) directed therapies such as abiraterone and enzalutamide with biomarkers of resistance such as ar mutations , splice variants or copy number variations in mcrpc [ 80 , 81 ] , olaparib for pca with defects in dnarepair genes [ 82 ] , and ipatasertib for pten loss disease . 
 there is a growing clinical need for new targeted therapies for pca , which may help maximize the effect on tumour cells and avoid major toxicities in healthy organs [ 83 ]  . studies have evaluated the role of choline pet / ct in the treatment response to second - line adt or chemotherapy in crpc patients with extended bone metastases but have given mostly unsatisfying results [ 8486 ]  . 
at present , a number of small sample studies and case reports have been published , and show promising results [ 90 , 91 ]  . 18flabelled psma tracers recently , the labelling of psma with 18f is gaining attention , and certain 18f - labelled psma tracers have been developed to be used both for diagnostic and therapeutic purposes [ 92 ]  . 
the limit of 68ga - psma is its restricted availability due to the need of local and cost - intensive 68ge68ga generators that require separate synthesis in a radiopharmacy facility , which can provide only few elutions per day . 
another challenge concerns the pharmacokinetic characteristics , as 68ga - psma has a prevalent urinary excretion , which may , in certain circumstances , hinder the evaluation of the prostate bed and pelvic lymph nodes . 
 additionally , the authors reported that in a separate cohort of 25 patients that underwent both examinations , 18f - dcfpyl was able to detect additional lesions in 36% of the pet positive scans . 
however , the study did not consider psa values < 0.5ng / ml , where 68ga - psma has already shown consistent results , and the different time of acquisition ( 1h after injection for 68ga - psma and 2h for 18f - dcfpyl ) may have resulted in the better sensitivity of 18f . 
given this , the optimal acquisition protocol and timing remain under debate for both 68ga - psma and 18f - dcfpyl , [ 97 ]  . finally , another 18f - labelled radiopharmaceutical is 18f - psma - 1007 , which has shown performance comparable to 68ga - psma - 11 , with a good tumour - to - background ratio and reduced urinary excretion . 
the future direction may be to increase the use of hybrid imaging with pet / mri also for 18f - labelled psma tracers . in terms of new developments , a psma ligand also suitable for spect imaging - 99mtc - mip - 1404is now under investigation in a phase iii clinical trial and has showed good sensitivity in detection of pca and lymph node invasion so far [ 99 ]  . psma radionuclide therapy inthetheranostics era in line with the aim of developing new therapies , it is noteworthy that besides being an imaging biomarker , psma can also be a therapeutic target . 
in fact , 177lu - psma therapy appears as a potent and novel option in patients with metastatic castration - resistant pca , based on exciting preliminary data on the safety and efficacy in reducing tumour burden [ 67 , 100 ]  . 
several retrospective safety , efficacy and dosimetry data guiding current clinical protocols have been reported , although the most effective and tolerable doses and co - medications to maximize the efficacy with minimal side effects has not yet been clearly defined . 1 3 la radiologia medica ( 2018 ) 123 : 952965 the administration of this treatment requires high expertise , in order to support the rapid clearance of free 177lupsma to reduce side effects . 
although at present radionuclide therapy using beta - emitters has been assessed as the principal option for late - stage castration - resistant metastatic pca [ 104 , 105 ] , certain studies have shown an overall biochemical response rate of 45% after 14 cycles of 177lu - psma therapy and a percentage of 40% of patients that do not respond at all to the therapy [ 106 ]  . in view of this , during the last years , the use of alphaemitting psma tracers has been considered as an option for radionuclide therapy for pca . 
223ra therapy has been already used as alpha therapy in the treatment of castration - resistant pca , but mostly with a palliation aim in symptomatic bone metastases [ 107 ]  . a new therapy with 225ac - psma seems to be promising in breaking radio - resistance to 177lu - psma , having certain advantages over beta - emitters : first of all , the very short range of alpha particles ( 50100m ) enable a more targeted and cell - specific therapy ; secondly , the alpha therapy microdosimetry could spare healthy tissue more accurately and have less toxicity , especially to the bone marrow , enabling therapy in patients with bone marrow infiltration , a contraindication to beta - emitter therapy [ 108 ]  . the use of 225ac - psma alpha therapy has demonstrated , in a number of preliminary studies , a promising response rate in skeletal and extra - skeletal disease , which is correlated with a metabolic response at the follow - up 68ga - psma - 11 pet / ct and a decrease in the psa values [ 109 , 110 ]  . 
the only adverse clinical event reported was a prolonged xerostomia , as salivary glands , together with kidneys and red marrow , are dose limiting targets of psma labelled radionuclide therapies . nevertheless , the limited availability of 225ac , although different alternative methods of production have been already proposed , remains one of the major limits for clinical use . 
procedures were categorized into two different grades of complexity , standard and complex , intended as fenestrated / chimney / snorkel and evar plus additional embolization to prevent endoleak type ii . 
we evaluated patient demographics , air kerma ( ak ) , dose area product ( dap ) , and procedural data ( fluoroscopy time , number of fluorographies , and iodinated contrast )  . 
staff radiation dose was measured with film badge dosimeter on c - arm . results the eco - dose protocol witnessed a dap reduction of 53% in standard evars and of 57% in complex evars and an ak reduction of 45% in standard and 57% in complex evar . 
the image quality in 2016 was perceived acceptable , as proven by the fact that fluoroscopy time , number of fluorographies , and contrast medium volumes did not have to be increased . 
in particular , endovascular aortic procedures expose patients and staff to significant doses of ionizing radiation , with a potential risk of radiation - induced skin damage and subsequent malignancy [ 3 ]  . 
virtually , all patients undergoing abdominal aortic aneurysm repair ( evar ) need a preoperative ct scan , intraoperative fluoroscopic and fluorography imaging , and lifelong surveillance imaging . the european directive 2013 / 59 / euratom of december 5 , 2013 emphasized the need for justification of medical exposure and strengthened the requirements on the information to be provided to patients , the recording and reporting of doses from medical procedures , the use of diagnostic reference levels , and the availability of doseindicating devices [ 4 ]  . 
as of now , radiation exposure in patients who undergo medical imaging procedures is not typically monitored , but member states must transpose the directive into national legislation by february 6 , 2018 . a lower radiation dose to the patient will result in a lower radiation dose also to the staff [ 5 ] , dose that can be further lowered by taking protective measures , such as various forms of x - ray shielding and lead aprons , collars , and glasses . 
recent technical innovation managed to reduce the entrance dose , while maintaining the image quality , by exploiting advanced real - time image - processing algorithms and hardware changes , such as thicker copper filtration , shorter pulse duration , smaller focal spot size , and a more sensitive detector [ 6 ]  . 
in centers where this technology is not yet available , it is essential to work on the optimization of the existing angiography system for improving patients safety , as well as on the education of operators about the most appropriate use of the imaging equipment [ 7 ]  . well - known strategies to reduce radiation exposure during endovascular procedures are maximizing the distance between the x - ray source and the patient , minimizing the distance from the patient to the detector [ 8 ] , applying low fluoroscopy settings and an appropriate field of view [ 9 ] , and using road mapping functionalities [ 10 ]  . 
other useful tips have been proposed in the literature : the operator should not activate the fluoroscopy unit when not viewing the monitor and should make use of the last - imagehold feature [ 11 ] , redundant views should be avoided , and the operator should note the number of 5 - min fluoroscopic notifications alarms [ 12 ]  . 
in addition , all forms of magnification , either decreasing the field of view ( fov ) or increasing the distance between the patient and the detector , increase the radiation dose and should thus be minimized as much as possible [ 13 ]  . 
a good collimation decreases scatter radiation , by eliminating the more divergent rays , upgrades image quality , and reduces radiation exposure by eliminating x - rays not converging on the area of interest and thus not useful to imaging . 
the change of projection can spare the skin from the harmful effects of radiation , but care must be exercised to use this method intelligently because steeply angled oblique images result in more tissues to be traversed by the x - ray beam and in compensation by the automatic brightness control system , resulting in an increased radiation dose [ 14 ]  . 
in addition , radiation dose can be reduced by increasing awareness among personnel and implementing standardized x - ray exposure protocols [ 6 ]  . the impact of the more recent technical innovations in reducing the entrance dose was well demonstrated in a wide spectrum of procedures , like pacemaker and implantable cardioverter defibrillator ( icd ) implantations [ 15 ] , transcatheter aortic valve implantations [ 16 ] , aortoiliac endovascular procedures [ 6 ] , lower extremity interventions [ 17 ] , and endovascular aneurysm repair too [ 18 ]  . 
to the best of our knowledge , however , there are no studies in the literature that used a reconfiguration of the angiographic system to reduce the radiation dose during endovascular procedures . aim ofthestudy the aim of our study was to evaluate the radiation dose reduction during evar after the reconfiguration of the philips ( eindhoven , the netherlands ) alluraxper fd20 x - ray system present in our hybrid roothe estimate was made by comparing data on a sample of patients treated before the reconfiguration ( year 2012 ) with data on an equivalent sample of patients treated after the reconfiguration ( year 2016 )  . the primary endpoint was confirming the patients dose reduction . 
the details of the reconfiguration are summarized in table1 . the entire staff ( doctors , radiographers , and nurses ) were extensively trained in the use of the new protocol . 
specific emphasis was placed on radiation protection awareness , from the common procedures for the reduction of the radiation dose to the safest and most proficient ways for adopting , whenever possible , the eco mode and not going over the number of fluorographies necessary for the best outcome of evar . study design andsamples the aim of the study was to test whether the implementation of the eco - dose protocol fostered a decrease in the dose received by the patients without unacceptable cuts in the image quality . to this end , evar procedures were categorized into two different grades of complexity : standard evars ; complex evars , including evar plus additional embolization to prevent endoleak type ii and fenestrated / chimney / snorkel evars . two samples , each composed of 25 consecutive standard and 25 consecutive complex evars , were compared . 
 the first sample included the last 50 procedures performed before the optimization ( normal - dose sample ) , whereas the second one included the first 50 procedures performed after no exclusion criteria were applied to patients as to age , gender , and body mass index ( bmi )  . the patient radiation dose was obtained by evaluating the air kerma ( ak ) and the dose area product ( dap ) , as proposed in 2009 by the society of interventional radiology [ 12 ]  . 
the total ak is the procedure cumulative air kerma at the interventional reference point ( defined at 15cm on the tube side of the isocenter ) and is measured in gray ( gy )  . 
 dap is defined as the integral of ak across the entire x - ray beam emitted from the x - ray tube and is a surrogate measurement for the entire amount of energy delivered to the patient by the beam ( gy cm2 )  . 
all patients at the time of the procedure had been informed about the possible use of their data for study purposes and signed an informed consent for patients information was anonymized prior to the analysis . statistical analysis continuous variables were checked for normality with the shapiro - wilks test . 
 normality was rejected for all other variables , which are reported as median , first quartile q1 ( 25th percentile ) and third quartile q3 ( 75th percentile )  . 
data were compared with mannwhitneys nonparametric test and displayed graphically by box plots , which allow visualizing sample mean , median , and the upper and lower ( first and third ) quartiles . 
 correlations between variables were expressed by pearsons linear correlation coefficient r . categorical variables , reported as counts and percentages were arranged in 2 2 contingency tables and studied with the chi - square test with yates correction . statistical significance was set at two - tail p < 0.05. 
the variables considered were : age , gender , bmi , ak , total dap , fluoroscopy time , number of fluorographies , and volume of contrast medium injected . to shield the possible confusing effect of the reduction of the number of performed fluorographies consequent to the staffs training , we report for each evar the value of the fluorography - related dap ( dapf ) normalized to the number of performed fluorographies ( nf )  . the outcome of the two comparisons is shown in table2 for standard evars and table3 for complex evars . 
1 box plot of ak ( a ) and dap ( b ) for standard ( normal and eco protocol ) and complex ( normal and eco protocol ) evar procedures . 
the bottom and top hinges of the boxes are the first ( q1 ) and third ( q3 ) quartiles ; the blue band inside the box is the second quartile ( median ) , and the red line is the sample mean fig . 
2 box plot of the fluoroscopy time ( a ) and of the number of fluorographies ( b ) for standard ( normal and eco protocol ) and complex ( normal and eco protocol ) evar procedures . 
 the bottom and top hinges of the boxes are the first ( q1 ) and third ( q3 ) quartiles ; the blue band inside the box is the second quartile ( median ) , and the red line is the sample mean 1 3 la radiologia medica ( 2018 ) 123 : 966972 fig . 
 the bottom and top hinges of the boxes are the first ( q1 ) and third ( q3 ) quartiles ; the blue band inside the box is the second quartile ( median ) , and the red line is the sample mean discussion evar procedures may be highly irradiating for patients , possibly leading to skin injuries , as well as to stochastic effects . 
 [ 6 ] registered over all evars a 56% reduction in ak and 57% in dap , after the implementation of the allura clarity fd20 systethis study did not distinguish between standard and complex evar , making difficult a direct comparison with our series , but the figures are consistent . 
de ruiter and colleagues [ 18 ] evidenced a reduction in dap of about 36% for not - complex evars and 32% for complex evars performed with a fixed c - arm equipped with allura clarity image - processing technology . 
 in that study , a median dap of 157.0gycm2 and a median ak of 600mgy in not - complex evar and a median dap of 598.2gycm2 , with a median ak of 3700mgy , in complex evar were , respectively , registered . 
another study [ 17 ] showed a dose reduction of about 60% in complex endovascular procedures [ cep ] after the implementation of the allura clarity image - processing system ; the reduction was more effective in lower extremity interventions , up to 70% in fluorography and 47% in fluoroscopy , than in complex evars ( up to 44% in fluorography and 37% in fluoroscopy )  . 
absolute x - ray doses in simple evar procedures were 157gycm2 ( dap ) and 560mgy ( ak ) , while they were 372gycm2 ( dap ) and 2580mgy ( ak ) in complex evar procedures . 
both these studies , however , considered as complex only fenestrated evar and do not mention any embolization performed to prevent type ii endoleaks . it is important to remember that while the recent technical innovations attempt to maintain or enhance the image quality , the eco dose achieves a lower dose irradiation at the expenses of some clinical image quality loss . 
granted that the image quality is necessarily higher when using high radiation doses , the eco - dose protocol has , however , been successfully optimized to obtain an acceptable image quality with the lowest possible dose according to the various procedures , as proven by the fact that fluoroscopy times , number of fluorographies , and contrast medium volumes did not have to be increased , with the latter two actually significantly decreasing . 
the normalized variable dapf / nf was introduced to enhance the effect of the eco protocol , independently from the reduction in the number of fluorographies achieved thanks to the staffs training ; of course , it was the synergy between machine reconfiguration and staff training that allowed a reduction close to 60% for complex evars . table 4 overview of clinical studies on allura clarity technology in evar procedures : comparison with the current study dapstandard ( % ) akstandard ( % ) dapcomplex ( % ) akcomplex ( % ) de ruiter etal . 
 ( 2016 ) ( allura clarity ) current study ( 2017 ) ( eco - dose mode ) ( 36% ) ( 21% ) ( 53% ) ( 57% ) ( 49.5% ) ( 45% ) 598.2 ( 32% ) ( 38.1% ) ( 57% ) 3700 ( 57% ) 2580 ( 48.1% ) 1236 ( 57% ) 1 3 972 la radiologia medica ( 2018 ) 123 : 966972 the exposure dose reduction for the patients was paralleled by a decrease in the staff exposure , quantified in 26% . 
it must be remembered that the operator is typically exposed to a dose rate approximately 0.1% the entrance skin exposure dose rate to the patient 1m from the center of the fluoroscopic field [ 11 ]  . this study has some limitations . 
second , while other studies considered as complex evars only chimney / fenestrated / branched evar , we classified as complex evars also the intraoperative embolizations to prevent endoleak type ii , usually performed at our institution . 
third , we evaluated the impact of the reconfiguration on the image quality only indirectly , through surrogate measurements as fluoroscopy time , number of fluorographies , and volume of iodinated contrast injected . 
histological analysis included : histological features ( histological type , necrosis , vascular invasion and mib1 ) , immunohistochemical characterization ( immunophenotype , receptor status , her2 - neu and grading ) and loco - regional characteristics ( t and n )  . 
radiologia , universit politecnica delle marche , ancona , italy 2 disco , universit politecnica delle marche , ancona , italy 3 azienda ospedaliero universitaria ospedali riuniti clinica di oncologia , universit politecnica delle marche , ancona , italy 4 azienda ospedaliero universitaria ospedali riuniti clinica di radiologia , universit politecnica delle marche , ancona , italy 5 dipartimento radiologia clinica , ospedali riuniti azienda ospedaliero universitaria ospedali riuniti , via tronto 10 , 60126ancona , an , italy introduction breast cancer ( bc ) is currently regarded as a highly heterogeneous disease . 
molecular subtype classification is based on immunohistochemical surrogates for the hormonal receptors ( er and pr ) , the overexpression of her2 ( human epidermal growth factor receptor ) and the proliferation index ( mib1 ) , which represent biomarkers with prognostic and predictive value in bc . 
each molecular subtype correlates with vol . : ( 0123456789 ) 1 3 754 la radiologia medica ( 2018 ) 123 : 753764 different biological behavior and clinical outcome , response to hormonal treatment ( ht ) and / or chemotherapy ( ct ) [ 2 ]  . dynamic contrast - enhanced magnetic resonance ( dcemr ) imaging of the breast is increasingly used as an adjunct to mammography and ultrasonography ( us ) to improve the detection and characterization of primary and recurrent breast cancers . 
correlation between morphological features , kinetic parameters of dce - mri and prognostic factors of bc has been previously analyzed , providing conflicting results [ 3 , 4 ]  . there are many differences between the two major histotypes of bc , in particular in the biological characteristics : invasive lobular carcinoma ( ilc ) express most of the time er and pr , with a lower proliferation index compared to invasive ductal carcinoma ( idc ) [ 6 ]  . 
moreover , they present two different patterns of angiogenesis ( based on multiple angiogenic factors ) in terms of vascular density , which influences the enhancement [ 7 ]  . 
it has been shown [ 811 ] that the different immunophenotypes correlate with specific vascular characteristics , such as angiogenesis , capillary density and vascular endothelial growth factor ( vegf ) expression , which reflect the dynamic contrast - enhanced images [ 10 ]  . aim of the study is to expand the evaluation of the dynamic characteristics of breast magnetic resonance ( bmr ) , analyzing some not taken into account in previous studies , and to seek a correlation between these and the histopathologic and immunohistochemical characteristics of breast cancer to orient the subsequent clinical and therapeutic management of patient . there are several studies in the literature that correlates biological characteristics of the bc with contrast enhancement curves [ 4 , 10 ] , adc values [ 12 ] and multifocality [ 13 ] ; in comparison with these studies , this one focuses on contrast enhancement kinetics of malignant lesions and in particular on the quantitative parameters that can be obtained from the timesignal intensity curve ( tic )  . materials andmethods patients a retrospective analysis was conducted from january 2012 to june 2016 ; a total of 149 consecutive patients were selected that performed breast mr for loco - regional staging purposes with histopathologically confirmed invasive breast carcinoma . forty patients were excluded for having undergone mr imaging more than 2weeks before surgery and / or initiation of neoadjuvant chemotherapy ; other 14 patients were excluded because were diagnosed with bc histotype different from idc or ilc . 
with the inclusion and exclusion criteria described in table1 , the final cohort was table 1 inclusion and exclusion criteria inclusion criteria surgery exclusion criteria infiltrative ductal and lobular cancer ( idc and ilc ) early breast cancer undergone mr imaging within 2 weeks prior to locally advanced breast cancer undergone mr imaging within 2 weeks prior to chemotherapy with neoadjuvant intent ductal or lobular cancer insitu ( dcis and lcis ) histotype different from idc and ilc ( i.e. , apocrine , medullary , mucinous carcinoma ) patients undergone breast mr imaging with a different protocol from the standard one in use at our institution local disease recurrence mrs different from rm philips achieva ( 1.5 t ) composed of 95 patients ( age range 2975years , mean 48years )  . 
the institutional review board of our institution approved the study . histological analysis all patients underwent to core needle biopsy ( 16 g needle ) , stereotactic or ultrasound guided , before surgery and / or chemotherapy . in all 95 cases were analyzed : histological features : histological type ( idc , ilc or mixed type ) , the presence of necrosis and / or vascular invasion ( v1 ) and mib - 1 ( 20% / > 20% ) ; [ 14 , 15 ] based on who classification , the most common histotypes ( idl and ilc ) were selected , and additionally mixed type neoplasms were included ( ductal / lobular ) [ 16 ]  . immunohistochemical characterization ( ihc ) : immunophenotype ( luminal a , luminal b , her2 + and triple negative tn ) , receptor status ( hr ) , her2 - neu ( herceptest - test immunocytochemical semiquantitative ) , grading ; er , pr , and her2 were examined by ihc staining of formalin - fixed , paraffin - embedded tissues . 
gallen [ 18 ] , molecular subtypes were classified considering the status of er , pr and her2 : subtypes were classified as luminal a ( er or pr positive , her2 negative ) , luminal b ( er or pr positive , her2 positive ) , her2 type ( hormone receptor negative , her2 positive ) , or triple negative ( hormone receptors and her2 negative )  . 1 3 la radiologia medica ( 2018 ) 123 : 753764 loco - regional characteristics : t and n ( according to who classification )  . 
each sequence lasts 1min and 17s , for a total duration of the kinetic mr study of 8min and 5s . postprocessing andmri enhancement analysis in order to evaluate the characteristics of the tic , the images were processed in a dedicated workstation software ( philips quantitative analysis )  . 
wash - in rate : maximum slope between t0 and time of peak intensity , which determines the maximum rate of contrast agent uptake during the acquisition and can adequately estimate the degree of early strong enhancement of tumoral tissue ; 4 . 
wash - out rate : absolute value of maximum slope between time of peak intensity and last measurement point , which determines the maximum rate of contrast agent outflow during the acquisition ; 5 . 
1 maximum enhancement ; 2 time to peak ; 3 wash - in rate ; 4 wash - out rate ; 5 brevity of enhancement ; 6 area under curve 1 3 756 la radiologia medica ( 2018 ) 123 : 753764 6 . 
type of curve in relation to the histological , immunohistochemical and loco - regional features of bcs . based on the type of the tic , patients were classified into three groups : nine patients with type i curve , 40 with type ii curve and 46 with type iii curve . 
dynamic parameters in relation to the histological , immunohistochemical and loco - regional features of bcs . tables7 , 8 and 9 show the extrapolated parameters from the tic in relation to the histological , immunophenotypic and loco - regional features of the examined tumors . there is a big amount of evidence in the literature regarding the correlation between mr images and invasive and / or insitu tumor . 
recent studies showed that mri is likely to predict the clinical , histological and molecular features of tumoral lesion , which represents one of the major prognostic factors for bc patients . 
according to the literature [ 7 , 26 , 27 ] , this finding may be associated with necrosis , due to the aberrant and chaotic angiogenesis of lobular cancers . 
this could explain the typical mr image of ilc , characterized by low and slow in - flow and release of the contrast from the lesion . in table5 , type iiiii curves are associated with luminal her2tumors ( 24.4% of cases ) , which represent the 42% of our series , and with tnbc , which is in line with data from lee etal . 
moreover , type iiiii curves are likely to be related to poorly differentiated lesions ( g2g3 ) [ 5 ]  . in table6 , type ii and type iii curves were found to be associated with the absence ( n0 ) or limited ( n1 ) lymph node involvement . 
in fact , an intense and early enhancement after administration of contrast is due to the increased vascular density of high - grade lesions [ 28 , 29 ]  . interestingly , our study showed a statistically significant correlation between bc immune profile and the following mr kinetic parameters : absolute maximum enhancement , time to peak and wash - in rate ( table8 )  . 
these data are in line with those previously presented by lee etal . , in which less steep enhancement curves are characteristics of high - grade lesions ( g2g3 ) [ 5 ]  . 
conversely , time to peak in tnbc and her2 + have significantly higher values compared to luminals ( table8 )  . furthermore , our study showed a correlation between er staining and multiple mr kinetic parameters , supporting previously published data [ 4 ]  . 
 diffusion - weighted imaging ( dwi ) evaluation may help to establish prognostic factors : the apparent diffusion coefficient ( adc ) is a helpful parameter for predicting low - risk tumors [ 33 ]  . 
texture analysis ( a mathematical method that analyzes spatial location and signal intensity characteristics of pixels ) is an adjunctive method that can help to discriminate breast cancer subtypes [ 34 ]  . 
 the expanding number of potential imaging and molecular biomarkers could improve the management of breast cancer but , at the same time , has the potential to produce lists of random statistical parameters , disperse scientific efforts , and drive up the cost of health care [ 36 ]  . this study has some limitations : this is a retrospective analysis with a number of patients included unbalanced compared to the number of factors considered . 
in order to find further correlations between mri characteristics and tumoral biological parameters , it could be useful to combine our findings with other mri features not evaluated in the present study such as lesion size , shape and adc values . 1 3 la radiologia medica ( 2018 ) 123 : 753764 fig . 
2 this post - contrast image a shows a mass lesion in the right breast which demonstrates a low time to peak value ( b ) : this lesion reported vascular invasion at the histological analysis . 
in another patient , mri post - contrast image c depicts a smaller mass lesion that demonstrates a higher ttp value ( d ) : in this case vascular invasion was not reported at the histological analysis . 
in this study , a correlation between ttp and vascular invasion was shown : low ttp values are frequently associated with the presence of neoplastic vascular invasion ( v1 ) ( p = 0.02 ) 1 3 762 la radiologia medica ( 2018 ) 123 : 753764 fig . 
3 mri image a , a large lesion is demonstrated that shows a curve with a less steep slope related to a low wash - in rate ( b )  . 
in our study , wash - in rate was higher in tumors with er + ( p = 0.0018 ) pr + ( p = 0.05 ) associated with a steep initial slope 1 3 la radiologia medica ( 2018 ) 123 : 753764 fig . 
transient elastography could not differentiate between group 1 and group 2 patients ( p = 0.12 ) , whereas point and 2d elastography examinations could distinguish patients in group 1 from group 2 ( p < 0.01 for both stq and ste )  . 
 administration of combined three elastography techniques showed the best diagnostic accuracy ( 90.1% ) for liver fibrosis , which was confirmed with hepatic biopsy examination . conclusion point and 2d elastography were superior to transient elastography to detect liver fibrosis and guide clinical anti - viral treatment . 
analysis of combined transient , point , and 2d elastography techniques showed the better diagnostic accuracy for liver fibrosis . keywords chronic hepatitis b liver fibrosis transient elastography point elastography two - dimensional elastography introduction chronic hepatitis b is a global health problem with the prevalence close to 4% worldwide [ 1 ]  . 
thus , accurate assessment of hepatic fibrosis grades is very helpful in evaluating the treatment and prognosis [ 6 ]  . hepatic biopsy has been the gold standard to assess the severity of liver fibrosis [ 7 ]  . 
recently , ultrasound elastography , which measures the propagation velocity of shear waves to estimate the liver stiffness , has been applied to quantitatively assess the severity of liver fibrosis [ 8 ]  . 
ultrasound elastography could be performed with different techniques , including transient , point , and two - dimensional ( 2d ) shear wave elastography [ 9 ]  . transient elastography is the first shear wave vibroacoustic technique used in the clinic , but has limitations when applied to patients with obesity or ascites . 
point and 2d shear wave elastography could allow the examiner to select vol . : ( 0123456789 ) 1 3 736 la radiologia medica ( 2018 ) 123 : 735741 a sampling area and obtain real - time images , but are relatively new techniques and require more studies before they could be widely applied in the clinical [ 9 , 10 ]  . 
previous studies comparing these different elastography techniques also reported controversial results , some showing better diagnostic values for point and 2d elastography , and others demonstrating no difference between transient and point / 2d techniques [ 1114 ]  . 
in fact , detection of mild and moderate fibrosis is more important , since early diagnosis and treatments to patients with early stages of fibrosis might reverse the progression of the disease [ 35 ]  . in the current study , we performed transient , point , and 2d elastography examinations in patients with chronic hepatitis b and in different stages of hepatic fibrosis , and compared diagnostic values of three elastography techniques for hepatic fibrosis . materials andmethods study design andparticipants patients with viral b hepatitis , who visited the ultrasonic department , ruijin hospital ( shanghai , china ) between january and july 2017 , were prospectively and continuously screened for the study . 
the study protocol was approved by the hospital ethics committee , and all the study participants signed the informed consent . the exclusion criteria were : ( 1 ) concurrent other liver disorders , such as drug - induced liver injury , autoimmune hepatitis , schistosomiasis , alcohol abuse , or infections from other virus diseases , including cytomegalovirus and human herpes virus ; ( 2 ) the levels of serum alanine aminotransferase and / or aspartate aminotransferase were 5 times higher than the normal ranges ; ( 3 ) the heart , brain , and kidney disease or diabetes ; ( 4 ) conventional ultrasound showed moderate - to - severe fatty liver , which could affect elastography examination . study protocol study instruments andexaminers transient elastography was performed with fibroscan device and m or l probe ( supersonic imagine , france )  . 
 point ( stq ) and 2d ( ste ) elastography were performed with the mindray resona 7 ultrasound system and l5 - 1 probe ( mindray , china )  . fibroscan examination was conducted by one sonographer with > 5years of experience . 
both sonographers were blinded to the liver biopsy results . patients position andpreparation forexamination based on the recommendation from european federation of societies for ultrasound in medicine and biology ( efsumb ) [ 8 ] , all participants were required to have a 2h of fasting time before the examination . 
patients were asked to breathe normally ( fibroscan ) or hold breath for 34s ( stq and ste ) to obtain stable images . ultrasound elastography examination first , routine ultrasound was performed to measure the width of the main portal vein ( mpv ) and spleen vein ( spv ) , and the maximal diameter ( sp1 ) and thickness ( sp2 ) of the spleen . 
images were selected when the uniform color filled more than 90% of the sampling area at a detection depth of 37cthen , the images were switched to quality control mode ( rlb map added )  . 
1 a reliable image was obtained when uniform color filled > 90% of sampling area and pr > 95% under rlb map , b after a reliable image was obtained , quantitative measurement was performed in the region of interest ( roi ) with the probe perpendicular to the skin fig . 
2 when two - dimensional grayscale image was obtained , elastography measurements were performed 5 times with final standard deviation < 2.0 as the quality control while avoiding large blood vessels and bile ducts liver biopsy after the ultrasound examination , liver biopsy was performed with a mn 1620 biopsy needle ( magnum biopsy gun , bard , usa )  . 
the scheuer criteria are : g0 : no inflammation ; g1 : mild inflammation ; g2 : moderate inflammation ; g3 : moderate - to - severe inflammation ; and g4 : severe inflammation . 
fibrosis grades are : s0 : no fibrosis ; s1 : enlarged fibrotic portal tracts ; s2 : portal fibrosis with rare septa ; s3 : fibrosis with architectural distortion , but no obvious cirrhosis ; and s4 : numerous fibrous septal with pseudolobule formation . 
based on the liver biopsy and pathological examination results , patients were assigned into group 1 ( either g or s classification < 2 ) or group 2 ( either g or s classification 2 )  . 
this g / s classification was used since it was general agreement that 1 3 738 la radiologia medica ( 2018 ) 123 : 735741 patients with either g or s classification 2 require antiviral treatment . 
two senior pathologists who were blinded to the elastography results reviewed the biopsy specimens and provided the histopathological reports . statistical analysis data were presented as mean standard deviation or median with 95% confidence interval when appropriately . 
ste included mean ( e1 ) , maximum ( e2 ) , and minimum ( e3 ) values elastography measurements , the calculated sensitivities were higher than the calculated specificities . 
analysis of combined three techniques could achieve the highest diagnostic accuracy . previous studies demonstrated that ultrasound elastography could provide quantitative information on the severity of liver fibrosis , though the results were controversial [ 1114 ]  . 
 in the current study , transient elastography examination did not show a statistical significant difference between the group 1 and group 2 patients who suffered from different severity in liver fibrosis . 
 this suggested that accurate diagnosis , which could identify the grades of hepatic fibrosis and decide treatment plan , was better with point and 2d elastography than with transient elastography . diagnostic performances of combined techniques are shown in table4 . 
e1 mean ste value 1 3 740 la radiologia medica ( 2018 ) 123 : 735741 current study , our transient elastography was conducted with fibroscan which was widely used to diagnose liver fibrosis . 
the 2d elastography ( ste ) examination used a multi - wave imaging platform that applies ultra - high - speed ultrasound wave to track the displacement of shear wave propagation paths at various points in different depths in the tissue . 
this resulted in a mach cone phenomenon , which could greatly enhance the production of the shear waves and increase the shear wave propagation efficiency in the tissue , and reduced the focused ultrasound energy to avoid negative biological effects . 
we tested segments 5 and 6 of the liver since the ultrasound beam was vertical to the intercostal space at this area and could also avoid the large blood vessels and bile duct , less affected by the breathing , and easy for biopsy . 
our results showed that point and 2d elastography provide better diagnostic accuracy compared to transient elastography . there was no previous study which investigated the combined analysis results from the transient , point , and 2d elastography . 
our results showed that combined analysis of multiple techniques could increase the accuracy to evaluate liver fibrosis . previous studies to calculate the diagnostic performance of elastography examinations showed that both sensitivity and specificity varied approximately 6090% , with some studies reporting higher sensitivity than specificity and others reporting opposite results [ 2022 ]  . 
our results suggested that elastography technique might be used to screen patients with possible liver fibrosis , but its finding should be confirmed by other diagnostic test , such as newly developed magnetic resonance elastography [ 23 ]  . limitations of the current study included small sample size and single - center study . 
future studies with a large sample size and focused on different stages of liver fibrosis should be performed . in conclusion , our results showed that point and 2d shear wave elastography had better diagnostic performances than transient elastography in detecting liver fibrosis . 
aim of our study was to evaluate patients perception of radiation exposure related to routine ct and their understanding after communication of their dose exposure . materials and methods a survey , investigating patients knowledge of radiation dose , was given to all adult patients ( > 18years ) undergoing a ct examination both before and after ct scan . 
 after ct scan , a second questionnaire was administered ( after receiving the ct dose bill report and medical written and / or explanation about ionizing radiation risk )  . 
results of the preand post - ct questionnaires responses were compared according to demographics characteristics and among the four post - ct groups . results for some questions , statistically significant differences were found between the two centres . 
however , there is not a standardized better way of communicating information on ionizing radiation risks due to ct . keywords radiation dose dose bill ionizing radiation risk questionnaire computed tomography * chiara tudisca chiaratudisca@gmail.com 1 department ofbiopathology andmedical biotechnology , section ofradiological sciences , dibimed university ofpalermo , via del vespro 127 , 90127palermo , italy 2 department ofexperimental andclinical biomedical sciences , radiodiagnostic unit n . 
dalessandro , university ofpalermo , palermo , italy introduction the legislation senate bill 1237 signed in california in september 2010 and applied since july 1 , 2012 , prescribed the duty for radiologist of recording ct dose parameters , as volume ct dose index ( ctdivol ) and dose - length product ( dlp ) , for each patient , placing these values in the radiology report ( the so - called dose bill information )  . 
initial experience on the consequences of this law and on radiologist compliance has been published [ 1 , 2 ]  . according to the euratom directive 59 / 2013 , in europe patients will receive dose bill in the radiological report starting from february 2018 [ 3 ]  . 
nevertheless , the international atomic energy agency ( iaea ) has stated that there is a need for improved communication , between vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 788798 professionals and patients . 
iaea basic safety standards stated that the patient has to be informed of the potential benefit of the radiological procedure , as well as radiation risks [ 4 ]  . misunderstood information can cause misinformed widespread panic and fear . 
thus , the next step should be to understand how to provide this information to patients , and which additional information patients would like to receive and need [ 59 ]  . we chose ct as diagnostic tool since it exposes to higher levels of ionizing radiation ( ir ) compared to conventional x - rays examinations [ 1013 ] , and it is more widely used in both oncologic and non - oncologic patients compared to other imaging techniques using ionizing radiations [ 14 , 15 ]  . on this background , the endpoints of our prospective study were : 1 . 
to tailor type of information according patients sex , age and scholarship level . method andmaterials this prospective cross - sectional study was carried out at the diagnostic radiology departments of the university hospital paolo giaccone in palermo ( coordinating centre ) and at the careggi hospital university of firenze . 
all patients that underwent a ct examination from may to september 2016 were consecutively recruited in the two centres ( somatom definition as 128 slices , siemens - healthcare , erlangen , germany for palermo ; light - speed , ge medical systems , milwaukee , wis and somatom plus 64 slices , siemenshealthcare , erlangen , germany for firenze )  . 
the study was approved by both the ethical committee ( ec ) of palermo and firenze ( reference number ec palermo 11 / 2015 ; ec firenze 16204 / 2016 )  . 
written informed consent stating that the patient voluntarily participated in this survey study and containing the contact information for the human investigation committee was administered and signed by all the patients . 
patients refusing to sign this informed consent were excluded . survey structure two different structured questionnaires were administered to the patient , one before ct scan and the other after ct scan ( most of the questions were the same in both questionnaires )  . the first survey was the same for all patients . 
it included both personal patients data and questions aimed at assessing patients perception and knowledge about ir and related risks , also comparing ct scan with generic x - ray and other cancer risk factors , and their opinion on the utility of the knowledge of ct dose parameters . immediately after ct scan , patients were provided their ct dose report , which was represented by ctdi and dlp derived from the scanner console and / or picture archiving and communication system ( pacs )  . 
after dose bill communication , patients were split in 4 groups , and a second questionnaire was administered as follows : group i a paper reporting a numerical ct dose parameters expressed in ctdi and dlp , without any other information or explanation ( only - bill - no explanation group ) ; group ii a paper reporting ct dose parameters and a written explanation ( written - explanation group ) on the risks related to ionizing radiation exposure due to medical uses , without additional oral information . 
this group was divided into two subgroups : ii - a a short written explanation , ii - b an extended written explanation ; group iii a paper reporting ct dose parameters and extensive oral explanation ( given by radiology residents ) on the risks related to ir exposure due to medical reasons ( oral / written - explanation group )  . the second survey was aimed at understanding : if the ct dose bill has been understood ( group i ) ; if the patients perception / knowledge of risks due to ir was changed after receiving the ct dose bill and medical written and / or explanation ( groups ii and iii )  . outcomes since our objective was to determine patients knowledge and / or awareness about radiation exposure due to ct scans , as well as their understanding of risks of radiation - induced possible damages , the primary outcome measure was the proportion of correct answers to each question on the survey . 
then , both the rate of correct questions in the second survey and the 1 3 790 la radiologia medica ( 2018 ) 123 : 788798 differences between the groups were evaluated . 
moreover , the relationship between primary and secondary outcomes and demographic information were investigated . results statistical analysis the sample size was calculated assuming that the probability to know the risks of possible radiation - induced damages and to be aware about radiation exposure due to ct scans increases linearly with increasing the information provided to patients of groups i , ii and iii . 
a sample size of at least 64 patients for each group of each radiological centre was calculated to test the null hypothesis h0 : p1 = p2 = p3 against the one - sided alternative h1 : p1 = 0.20 ; p2 = 0.30 ; p3 = 0.40. 
the cochranarmitage trend test was used , assuming a type - 1 error rate equal to 0.05 and statistical power equal to 0.80. all questions included in both surveys were treated as categorical variables , and they were expressed as counts and percentages . 
to adjust the above statistical association with respect to age , gender and education , the multilevel logistic regression models were estimated for each question and adjusted odd ratio ( or ) and 95% confidence intervals were calculated . 
for all questions , it was modelled the probability for each respondent to give the correct answer related to give the wrong answer or to do not know the answer . 
the z test for proportions was used to assess statistical significance of the difference between the perceived general knowledge about risk factors for healthincluding irbefore and after dose bill communication . for each analysis , a p value < 0.05 was considered to be statistically significant . 
 all statistical analyses were performed using stata / se 14.1 ( statacorp lll , texas usa ) a total of 430 questionnaires were administered to 430 patients consecutively recruited from may to september 2016 . 
eighteen patients declined to fill in the questionnaire ; the major reasons were the absence of interest in performing the questionnaire and the patients worry concerning the examination they had to undergo . 
group i , iia , iib and iii included 114 , 87 , 86 and 125 patients , respectively . a statistically significant difference concerning patients age was found among the groups , with group iib being younger than the others despite the casual distribution of the questionnaires ( table1 )  . 
 no difference in other patients demographics among the different groups was found ( table1 )  . main findings from overall data extracted after post - ct survey were the following ( table3 ) : 66% of the patients wrote that they had not understood the provided numerical ct dose parameters ; 87% were aware that performing more ct or x - ray examinations raises the risk of radiation - induced malignancies ; 64% were aware of the low risk of a single x - ray exami59% felt that performing a single ct scan is quite or nation ; highly dangerous . comparing the answers in the post - ct survey given by the patients in the different groups , just a significant difference in the perception of the comprehension of ct dose parameters was found ( table3 )  . 
results of multivariate analysis showed that age , sex and education did not affect the answers ( table4 )  . to determine the better communication form of the dose bill to patients , the answers given to seven questions common to both pre - ct and post - ct surveys were compared ( table5 ) : in all groups , it was found in post - ct survey an increased awareness of radiation exposure , which is administered through ct than through x - ray . 
the majority preferred symbols to indicate dose and verbal scales to indicate risks , and the preferred source of information was the prescriber or information letter [ 16 ]  . the hypothesis , we and ukkola etal . 
 [ 16 ] started from , was that there was a growing trend in patient learning on the topic of ir and radiation protection , depending on how the explanation was given to patients . 
providing ct dose parameters accompanied by information on the risks related to ir exposure due to medical reasons in an extensive written / oral form ( oral / written - explanation group ) , compared to providing ct dose bill without additional information ( only - bill - explanation group ) , makes the patient feel he / she has better understood ct dose parameters [ 17 ]  . 
 moreover , patients who just received concise written information ( group iia ) , when compared to group i , were those who believed that being submitted to one or multiple ct examinations do not change the probability of having irrelated damages ( table4 , question 2 )  . patients who received written ( either concise or extensive ) information , more frequently said they would accept to undergo ct examinations also when it is not clinically relevant . 
however , these data were not extensively explained either written or orally , thus giving us a first base to hypothesize that patients answered randomly to the surveys , as it will be better elucidated throughout the discussion . 
we can infer that the decision to participate the study for almost all of the respondents was probably not so much the desire to deepen their knowledge about radioprotection or to participate in a useful scientific work , but the willingness to please physicians working in the department where they were doing their own diagnostic examination . our starting hypothesis was that the extensive oral explanation was the best way to give the patient explanations . 
regarding the question related to bigger dose given by ct compared to x - ray ( table6 , question 1 ) , it can be noted an improvement about the percentage of the right answers in the second survey for the group iii . 
in fact , a significant subset of patients of the group i answered correctly to the same questions in the second survey , even if they got it wrong in the first survey and did not receive any kind of explanation between the first and second surveys . finally , when patients were asked about how did they feel with the fact that in the next future ( 2018 , february ) ct dose parameters will be registered in the ct report , a significant increase in the perception of the usefulness of these parameters was registered just in group 1 ( table5 , point 6 ) ; at multivariate analysis , groups iia , iib and iii did not perform better than group 1 ( table6 , point 6 ) , thus underlining the possible scarcity of interest on the topic in these groups , even in group iii after having had a dedicated physician talking with them . even if nearly half of all the patients answered they were interested on the topic , we cannot demonstrate an increasing interest on the topic in the second survey , in any of the groups . moreover , patients of group i improved their answers in the second survey , sometimes better than the other groups , and the additional increasing information provided , either written or oral , did not significantly improve patients awareness , knowledge and interest in radiation protection issues . this was underlined by the fact that a third of patients claimed to have understood , without any extensive explanation , the meaning of two technical terms such as dlp and ctdi ( table3 ) not so well understandable by many physicians [ 6 , 16 , 18 ]  . all what emerged from the analysis of the results is supported by the experience of investigators dealing with the administration of the survey themselves . 
patients , as perfectly understandable , were afraid for the examination result and showed less interest to radiation protection issues . this impression cannot be statistically expressed , but it finds its concretization in the answers given by the patients . 
 these , in some cases , were explicitly given randomly as demonstrated in those who completely changed the categorization of health risk factors in the second survey , when compared to the first one . 
conversely , they did not consider ir as one of the two most dangerous factors in either the first or the second survey , how it is proved by the little amount of patients putting exposure to nickel / asbestos / cobalt among 1 3 la radiologia medica ( 2018 ) 123 : 788798 the health risk factors . 
in general , there is a significant gap in patient awareness about ir risk and there is a need to address this deficiency , as also seen in ria etal . 
similar results were found between the current paper and ria etals paper since in both studies the communication of ct dose bill to patients was not enough to ensure the awareness of the sense of the dosimetric values written in the radiology report . 
this was an obvious sign of lack of interest by patients about this topic . considering that in none of the forms of the communication the other health risk factors were taken into account , the change experienced cannot be otherwise explained than with random assignment of the categories [ 7 , 8 ]  . 
also this evidence made us understand that although almost all the respondents have decided to join the surveys , they probably just wanted to please the physician , but they were not really interested in doing it . all the above discussed points , as 1 . 
however , it would be not easy to collect valid answers , because probably influenced by the results and implication of the diagnostic examination . indeed , the stress condition of the patients should be considered as a limitation for a correct , conscious and reasoned response to the surveys . moreover , the assessment of the effect of reading ct dose parameters under stress - free conditions for the patient could be of great usefulness , because starting from february 2018 the euratom will oblige the radiologist to write them , presumably as ctdi and dlp , in the ct report . 
once the stress conditions are over , the patient may be prompted to ask for the meaning of these parameters and consult certain websites and mobile applications that infer data population on tumour - risk to the individual ct examination without giving any scientific explanation . 
the information provided by those website or apps could raise an unmotivated concern in the patient and the patient could be wrongly pushed in the decision of not performing clinically indicated or follow - up necessary examinations [ 20 ]  . 
in order to avoid the recent messy in the public opinion concerning vaccinations in italy , it is mandatory to find the right ways to include the raw ctdi and dlp data in the most adequate context ( patient , family doctor , radiologist ) that will induce the comprehension of the data and topic without causing undue worries that would prevent patients from necessary follow - up examinations or any kind of unmotivated panic [ 21 ]  . a limitation of this study was represented by the enrolment of patients in two different hospitals , in which statistically significant differences between the answers of the patients were pointed out . 
however , data were adjusted in the multivariate analysis . another limitation of the study concerns estimates precision , which is not completely satisfactory for some questions , as suggested by quite large confidence intervals . 
there is room for improvement in this study by increasing the effective sample size in order to increase precision . the conception of this study was related to the fact that dlp and ctdi will be mandatory and important to help reduce population ir dose and , implicitly , also the number of required cts . 
the importance of this topic in our opinion will be essentially perceived by the medical staff , but it does not seem to be perceived by the patient according to our results . concerning the way of communication to the patient , it seems that the information provided both in a concise and extended form , neither written nor oral , increases the patients knowledge . from our study , we can understand that the awareness of the patient increases just to be submitted to the examination ; therefore , no different type of either written or oral explanation changes patients knowledge about radiation risk . conclusion the euratom directive requires the ct dose parameters to be reported for each examination in the report starting in february 2018 . 
this remains very valuable for doctors dealing with the patient , because this way they can easily control the total patient dose in case of multiple examination , so avoiding to exceed threshold values . 
the other aim of the ct dose parameters communication is to make patients aware of the radiation protection issue as also suggested by aiea and who [ 22 , 23 ] , but relying just on dlp and ctdi is probably not the best solution to reach the goal ; beyond all the 1 3 798 la radiologia medica ( 2018 ) 123 : 788798 considerations made , we must remember that just 34% of the total patients said they had understood ct dose parameters . 
prostate volume and the apparent diffusion coefficient ( adc ) were measured at an average of 10days post - pae and at 1 , 3 , 6 , and 12months post - pae . 
after pae , ultrahigh b value diffusion - weighted imaging ( dwi ) can show early infarction better than lower b value dwi . keywords magnetic resonance imaging prostatic hyperplasia embolization therapeutic diffusion magnetic resonance imaging infarction introduction approximately 50% of men with a clinical and radiological diagnosis of benign prostatic hyperplasia ( bph ) have moderate to severe lower urinary tract symptoms ( luts ) [ 1 ]  . 
 although both medical and surgical therapies for bph are effective , they are associated with significant morbidity rates and some degree of sexual dysfunction [ 3 , 4 ]  . 
recently , prostatic arterial embolization ( pae ) for bph has been shown to be a safe and effective procedure that improves luts related to bph [ 5 , 6 ]  . magnetic resonance imaging ( mri ) is the most adequate imaging technique for the prostate [ 7 ] , and it is also the best suited imaging method for evaluating the prostate after pae [ 8 ]  . 
some clinical indexes are also used in the evaluation of symptoms after pae , such as the international prostate symptom score ( ipss ) , quality of life ( qol ) , and peak urinary flow rate ( qmax )  . 
written informed consent was obtained from each patient . thirty - five patients with severe luts attributable to bph that was refractory to medical treatment who underwent pae at our institution between january 2014 and may 2017 were screened for study enrollment . 
a total of 28 consecutive patients ( mean age 70.6years ; age range 5884years ) who underwent pae at our institution and followed up with imaging for at least 12months were eligible for study participation . 
seven patients were excluded from the study for the following reasons : surgery or repeated pae before completing 12months of follow - up and / or any missed mris before or after pae . the baseline characteristics of the 28 patients are shown in table1 . 
all prostate volumes were greater than 50ml according to measurements taken using mri . patients underwent angiography and pae in a therapeutic angiography unit equipped with a digital flat - panel detector system ( innova 4100 iq ; ge healthcare ) with nonionic contrast medium ( visipaque 320 mgi / ml ; ge healthcare )  . 
we started the pae with smaller pva particles ( 50 m ; polyvinyl alcohol foam embolization particles ; cook incorporated , bloomington , in , usa ) for la radiologia medica ( 2018 ) 123 : 727734 the distal or intraprostate embolization and ended with larger particles ( 100m ; cook incorporated ) for more proximal prostatic arterial embolization . 
each vial of pva ( 1ml ) was diluted in a 40 - ml solution of nonionic contrast medium ( iodixanol 320 mgi / ml ; visipaque ; ge healthcare )  . 
the endpoint of embolization was near stasis ; after it was achieved , a waiting time of 45min followed for the particles to be redistributed in the feeding vessels ; and then , more embolic material was injected until complete stasis of the feeding artery was seen fluoroscopically . 
after pae , angiography was carried out using the power injector , with the 4 - fr catheter at the anterior branch of the internal iliac artery to check for any further blood supply to the prostate . 
in all individuals , antibiotics were given to prevent infection at 2days before the procedure and continued for 7days following the pae . operative success was defined as completing the unilateral or bilateral pae . 
axial diffusion - weighted imaging ( dwi ) using four b values of 0 , 1000 , 2000 , and 3000s / mm2 was performed to aid in the consistency of slice placement with the axial t2wi . 
dce - mri was performed in the transverse plane at baseline ( pre - contrast ) and at six time points after the administration of the contrast material , using a transverse three - dimensional fat - suppressed t1 - weighted gradient - echo sequence . 
a total of 15ml of gadobenate dimeglumine ( multihance ; bracco sine , shanghai , china ) was injected intravenously at a rate of 3ml / s using a power injector ( spectris ; medrad , 1 3 la radiologia medica ( 2018 ) 123 : 727734 warrendale , pa ) , followed by a 20 - ml saline flush . 
the mr imaging parameters are shown in table2 . statistical analysis mr image analysis we evaluated prostatic mri examinations before embolization ( within 2weeks of the procedure ) , at 10days ( mean 10days ; range 618days ) , and 1 , 3 , 6 - , and 12months after the procedure . 
after embolization , the infarcted area was defined as the region displaying no evident enhancement after contrast agent administration , and signal characteristics of the prostatic infarction region were observed . 
all data were measured by two radiologists , and the average of the two measurements was considered the final prostatic volume . the si of the infarcted area was observed on dwi ( different b value ) , and the adc value was measured on adc maps . 
correlations between the changes in prostatic volumes and clinical and imaging indexes before and 12months after embolization were analyzed by multiple linear correlation analysis . results operative success was achieved in all patients ( 100% ) , including 26 ( 92.9% ) patients with bilateral prostatic arterial embolization and 2 ( 7.1% ) patients with unilateral embolization . 
other minor complications ( e.g. , transient hematuria , hematospermia , and a small amount of rectal bleeding ) were self - limiting and disappeared during the first week after pae . 
twelve months after embolization , the mean ipss , qol score , qmax , pvr , and psa improved significantly compared with baseline values , but the mean iief - 5 score was not significantly different from the baseline value ( table1 )  . infarcts were observed after embolization in all patients ( 100% ) and occurred exclusively in the transition zone . 
however , we did not measure the volume of the infarct due to limitations of the post - processing software . the si of the dwi can reflect changes in the course of prostatic infarction . 
when b = 1000 and 2000s / mm2 , the adc values of the prostate pre - embolization were not significantly different from those at average of 10days post - embolization , but the adc values of the fig . 
when the age was older and the pvr value was smaller , the prostatic volume reduction was more obvious . discussion in our study , patients showed operative success and significant clinical improvement in terms of ipss , qmax , pvr , qol , and psa 12 months after embolization compared with baseline values . 
 decreased testosterone uptake in prostate cells after embolization could lead to the inhibition of prostate growth , and a possible decrease in the number of 1 - adrenergic receptors could lead to decreased muscle tone and urine outflow obstruction [ 11 , 12 ]  . although most of the previous studies focused on the clinical efficacy of pae , we preferred to concentrate on the changes in the infarcts and their imaging characteristics . 
at an average of 10days after embolization , prostatic infarct occurred and was observed clearly on the post - enhancement scan and appeared as symmetrical patchy necrosis on both sides of the prostate midline [ 13 ]  . 
this may be due to hemorrhagic necrosis with the presence of proteinaceous content and blood breakdown products , especially methemoglobin , and their associated t1 - shortening effects [ 14 , 15 ]  . 
contrast enhancement was lower in the peripheral zone compared to that in the transition zone [ 1720 ]  . on dwi ( b = 1000 or 2000s / mm2 ) , we did not observe the presence and extent of the prostatic infarct at an average of 10days after embolization . 
when b = 3000s / mm2 , the adc value of the prostate before embolization was significantly different from that obtained at every time interval after embolization ( p < 0.05 ) [ 22 , 23 ]  . 
for both signal observation and adc measurements , an ultrahigh b value ( b = 3000s / mm2 ) was better than other b values , because dwi can reflect more effective movement of water molecules inside and outside the cells as the b value increases [ 24 ]  . the prostate volume decreased with time after embolization . 
ten days after embolization , the prostate volume of 3 of the 28 patients increased slightly , which may be due to hemorrhage and edema formation after prostatic infarction that resulted in a temporary enlargement of the prostate volume [ 27 ]  . no statistically significant difference was observed in volumes before and 10days after embolization . 
we performed mri 10days after surgery to exclude complications , especially severe complications , and to observe the effect of prostatic infarction ; however , the change in prostatic volume was not obvious . 
della misericordia , 15 , 33100udine , italy 3 department ofoncologic radiation therapy anddiagnostic imaging , centro di riferimento oncologico , via franco gallini , 2 , 33081aviano , italy introduction external beam radiation therapy ( ebrt ) is increasingly used as definitive treatment of non - metastatic prostate cancer ( pca ) [ 1 , 2 ]  . 
since pca ranges from biologically indolent to aggressive , locally advanced disease , proper stratification of the risk of biochemical recurrence is of pivotal importance in predicting patients outcome and planning the most appropriate ebrt regimen in terms of dose , fractionation , volumes of irradiation and association with adjuvant androgen deprivation therapy ( adt ) [ 25 ]  . available risk stratification systems , e.g. , the national comprehensive cancer network ( nccn ) one [ 5 ] , define patients risk based on the combination of prostatic specific antigen ( psa ) level , gleason score ( gs ) and the t stage vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 778787 as defined by digital rectal examination ( dre ) [ 2 , 4 , 6 ]  . 
 recently , multiparametric magnetic resonance imaging ( mpmri ) has been advocated as a more reliable tool to provide the t stage for the purpose of risk stratification [ 3 , 7 , 8 ]  . 
the use of mpmri - derived t stage ( mpmrit ) showed a prevalent effect of risk upgrading compared to clinical staging , thus influencing the choice of the ebrt regimen and / or duration of adjuvant adt [ 3 , 7 , 8 ]  . however , uncertain cost - effectiveness is still concern for a more systematic use of staging mpmri , especially in lower - risk patients [ 2 ]  . 
popular nomograms such as partin tables ( pt ) [ 9 ] and the memorial sloan - kettering cancer center nomogram ( mskccn ) are cheaper and readily available tools to predict pathological t stage , and in turn to define patients risk before ebrt . 
however , mpmri was shown to predict the pathological t stage better than pt [ 1012 ] and / or mskccn [ 13 ] , thus emphasizing the problem of whether mpmri - derived or nomogram - derived t stage should be used to assess patients risk before ebrt planning . the purpose of this study was then to assess whether the agreement between mpmri , pt and mskccn in defying patients risk category is high enough to use them interchangeably in the risk stratification process of patients with pca referred to ebrt . materials andmethods study population this study was performed in two centres as a branch of larger trials investigating the role for 3.0t mpmri in the management of pca , as approved by the referring ethical committees of both participating institutions . 
enrolled subjects expressed informed consent to participation . during the period january 2013october 2016 , we prospectively addressed to staging mpmri all patients with biopsy - proven pca addressed to ebrt by a pool of referring radiation therapy oncologists ( 1020years of experience in treating pca )  . 
for the purpose of analysis , clinical risk stratification was assessed according to the nccn criteria [ 5 ] , using psa level , gs and the t stage as resulting from 2011 - updated pt ( ptt ) and mskccn ( mskccnt )  . 
in particular , ptt and mskccnt were defined in accordance with the tnm classification [ 14 ] as 100 probability of organ conned disease on nomogram ( % ) , dichotomizing the results as organ - confined disease ( oc ) ( stage t2 ) versus non - organ - confined disease ( noc ) ( stage t3 ) for a resulting probability < 50% and 50% , respectively . 
before the examination , patients voided the rectum with a cleansing enema in both centers , and received i.administration of a spasmolytic agent ( 20mg hyoscine butylbromide , buscopan , boehringer ingelheim gmbh , ingelheim , germany ) in center 1 . the mpmri protocols are illustrated in table1 . 
apparent diffusion coefficient ( adc ) maps were obtained with the vendors software ( extended mr workspace , philips medical system , the netherlands in center 1 ; ge funtool 14.3.1 , general electrics , milwaukee , usa in center 2 ) , using linear regression of signal intensity versus b values according to a mono - exponential fitting model . image analysis image analysis was performed in consensus by two readers ( 3 and 13years of experience in urogenital radiology ) , using a dedicated workstation ( olea sphere , olea medical , la ciotat , france )  . 
detection and staging of pca were performed in accordance with the prostate imaging reporting and data system ( pi - rads ) version 1 [ 15 ] and version 2 [ 16 ] before and after mid - 2015 , respectively . 
when using pi - rads version1 , such a classification was obtained if the sum of individual sequences scores was 10 according to the rules detailed elsewhere [ 17 ]  . 
in particular , readers scored : ( 1 ) the probability of extracapsular extension ( ece ) as 1 for tumor - to - capsule abutment , 3 for irregular capsule profile , 4 for neurovascular bundle thickening and / or bulge with loss of capsule and / or tumor - to capsule contact > 10mm , and 5 for measurable extracapsular disease ; ( 2 ) the probability of seminal vesicle invasion ( svi ) as 1 for expansion , 2 for low t2 signal , 3 for filling of an angle , 4 for enhancement and restricted diffusion , and 5 for measurable solid tissue . 
though associated with increased detection of ece in patients with broad tumor - to - capsule contact [ 18 ] , cancer adc values were not used in the staging process , given well - known problems of inter - scanner reproducibility . 
this translated into poor agreement , with k values of 0.16 ( standard error 0.11 ) for mpmri versus pt , and 0.16 ( standard error 0.10 ) for mpmri versus mskccn . 
most discrepancies between mpmri and nomograms occurred in classifying intermediate risk category , with 17 / 30 discrepant assignments ( 56.7% ; 95% ci 38.974.4 ) compared to pt and 24 / 28 discrepant assignments ( 85.7% ; 95% ci 72.898.7 ) compared to mskccn . there was moderate agreement between nomograms ( k = 0.58 , standard error 0.08 ) , with mskccn upgrading the risk compared to pt ( 12 / 80 intermediate risk cases and 7 / 80 low - risk cases moving towards high - risk category )  . examples of mpmri - induced downgrading are illustrated in figs.1 , 2 , while mpmri - induced upgrading is shown in fig.3. 
 discussion pt and mskccn are of widespread use in radiation therapy departments to refine clinical t staging and treatment decisions [ 2 ] , given the capability of the t stage alone ( being equal psa level and gleason score ) to change patients risk assignment and in turn recommended ebrt regimens [ 5 ]  . 
1 mpmri - induced risk downgrading in a 74 - year - old man with a gleason score 3 + 4cancer and psa level 7.20ng / ml ( ct2a ) , showing risk of non - organ - confined disease of about58% and 62% , according to pt andmskccn , respectively.mpmrishowed a small left peripheral zone lesion with restricted diffusion on thehigh b - value image and adc map , respectively ( white arrow in a and b )  . 
the lesion was visible as a hypointense focus on transverse ( c ) and sagittal ( d ) turbo spin echo t2 - weighted images and showed moderate focalenhancement aftergadolinium administration on subtracted 3d gradient echot1 - weighted imaging ( e )  . 
2 risk downgrading related to staging mpmri in a 77 - year - old patient with a gleason score 3 + 4 cancer ( psa level 13.1ng / ml , ct3a )  . 
mpmri found a focus of restricted diffusion in the left peripheral zone at the midglandular level , with hyperintensity on high b - value transverse image ( arrow in a ) , and hypointensity on the adc map ( arrow in b )  . 
on t2 - weighted transverseimaging ( c ) , the lesion was found as a slightly hypointense focus far from the capsule ( arrow ) , showing focal contrast enhancement on dynamic contrast imaging ( arrow in d )  . 
mpmri results reclassified nccn risk from high to intermediate patients referred to ebrt , we observed moderate agreement between the two nomograms in assessing oc versus noc ( k = 0.51 ) , with pt downstaging 25% of patients assessed as t3 stage with the mskccn . 
this translated into moderate agreement only ( k = 0.58 ) in risk category assessment , with a tendency of mskccn to upgrade the risk compared to pt ( 12 / 80 intermediate risk cases and 7 / 80 low - risk cases moving towards high - risk category )  . 
however , we believe that this observationfurther emphasizes the need to rely on mpmri rather than nomograms in case of discrepancies in staging pca , given the capability to provide more objective anatomical information on a patient - by - patient basis [ 4 , 7 , 8 ] , including lesion size , laterality , location of prostatic and extraprostatic disease . 
 moreover , mpmri was shown to assess oc better as a standalone technique ( auc 0.88 ) than in combination with pt ( auc 0.63 ) [ 12 ]  . mpmri staging had a relevant effect in terms of risk stratification in our series . 
3 mpmri - induced upgrading of prostate cancer in a 76years - old man with a gleason score 3 + 4 cancer , psa level 4.77ng / ml , ct1c , showing risk of stage t3 of about36% according to pt.mpmri showed left peripheral zone to bealmost completely affected bya large lesion with restricted diffusion on transverse high b - value image and adc map , respectively ( white arrow in a and b )  . 
the lesion was markedly hypointense on transverse ( c ) and sagittal ( d ) turbo spin echo t2 - weighted images ( arrows ) , and showed focal enhancement aftergadolinium administration on 3d gradient echot1 - weighted imaging ( e ) , with a definite wash - in / washout time - intensitycurve ( f )  . 
 capsular profile was irregular and thinned on turbo spin echo t2 - weighted images , with a tumor - to - capsule contact > 1 cinitial extension towards the left seminal vesicle was seen on the same images ( arrow in d ) , suggestingextraprostaticdisease ( stage t3 )  . 
however , a similar effect was shown in a previous study comparing mpmri versus a different nomogram ( roach equations ) [ 4 ] , suggesting a possible tendency of some nomograms to overstage pca compared to mpmri , and in turn overestimate patients risk . 
 of note , all previous works comparing mpmri versus drebased risk stratification ( with or without the complement of trus and / or computed tomography ) [ 4 , 7 , 8 , 20 ] were concordant in showing a prevalent mpmri - related effect of risk upgrading , as expected by low reliability of dre in predicting noc compared to pt and mskccn [ 22 , 23 ]  . 
 in our series , mpmri reclassified more than one - third of patients initially assessed as being at higher risk ( 35.9% with pt and 37.9% with mskccn , respectively ) , or lower risk ( 40.9% with pt and 40.0% with mskccn , respectively )  . 
 assuming that mpmri acts as a reasonable surrogate standard for pathology , our results suggest a potential role for refining the assessment of intermediate risk patients , since the majority of reclassifications occurred towards this risk category , with relevant consequences on patients management ( e.g. , adding adt in the case of upgrading and reducing the duration of adt in the case of downgrading ) [ 5 ]  . one might argue that a systematic use of mpmri as a risk stratification tool is potentially cost - ineffective . 
4 concordance betweenmpmri and nomograms in assessing the riskin a 73 - year - old patient with gleason score 4 + 3 cancer ( psa level 10.69ng / ml , ct2a ) , showing a pt and mskccn risk of extraprostatic disease 74% and 67% , respectively . 
mpmri showed a pi - rads 5 focus ( arrow ) of restricted diffusion in the right peripheral zone at midglandular level , with hyperintensity on transverse high b value image ( a ) , and hypointensity on the adc map ( b )  . 
on transverse ( c ) and coronal ( d ) t2 - weighted imaging , the lesion appeared markedly hypointense , with broad ( > 1cm ) tumor - tocapsule contact ( arrows ) , suggesting microscopic extracapsular extention . 
the patient was classified at high risk according to nccn categories is reasonable to assume that mpmri - based risk reclassification might compensate for the costs induced by overor under - treatment . 
of note , there is increasing evidence on combined positron emission tomography and computed tomography imaging ( pet - ct ) as a tool to assist in targeted biopsies in the setting of hybrid imaging with mpmri [ 24 , 25 ] or identify intermediateand high - risk cancers [ 26 ]  . 
 while 18f - fdg , 11c - acetate , 18f - choline , and 18f - facbc ( fluciclovine ) were shown to have limited use in localized pca and a high false - positive rate , prostate - specific membrane antigen ( psma ) - targeted agents such as ( n - [ n - [ ( s ) 1 , 3 - dicarboxypropyl ] carbamoyl ] - 4 - 418f - fluorbenzyl - lcysteine ) ( 18f - dcfbc ) showed higher positive predictive value for index lesions than mpmri [ 26 ]  . 
while mpmri is not associated with radiation exposure , pet - tc has the advantage of a panoramic evaluation of extraprostatic disease , including the detection of metastases [ 27 ]  . 
however , microscopic t3a stage has a reasonably limited effect on ebrt planning , because it is generally accepted that an additional margin of treatment for 1 3 786 la radiologia medica ( 2018 ) 123 : 778787 microscopic ece is unnecessary or can be adjusted based on unfavorable psa level and / or gs [ 29 ]  . 
importantly , microscopic ece can be missed by pt and mskccn as well [ 912 ] , emphasizing that overlooking microscopic t3a stage is an intrinsic risk in the ebrt scenario , in which final pathological proof of cancer extension lacks by definition . 
second , we used anarbitrary threshold ( 50% ) to define noc based on the nomograms results , given the impossibility to establish a populationbased cutoff in patients without final pathology . 
on the other hand , we believe that establishing a reasonable cutoff for nomograms is arelatively important task if more objective information on noc is provided at a glance by mpmri , thus further emphasizing our results . in conclusion , we showed that mpmri provides substantially different risk stratification than nomograms in patients with pca referred to ebrt , so that they cannot be used interchangeably . 
assuming that mpmri acts as a reasonable surrogate standard of reference for pathology , our results suggest that this technique can refine or replace pt and / or mskccn as tool for risk stratification purposes . compliance with ethical standards conflict of interest the authors declare that they have conflict of interest to disclose . ethical standards all the procedures performed in the study were in accordance with the ethical standards of the institutional research committee and with the 1964 helsinki declaration and its later amendments . 
this study aimed to review the published evidence on effective dose of non - dental cbct for diagnostic use by focusing on dosimetry system used to estimate dose . materials and methods a systematic review of the literature was performed on 12 november 2017 . 
studies were screened for inclusion based on defined inclusion and exclusion criteria according to the preferred reporting items for systematic reviews . results fifteen studies met the inclusion criteria and were included in our review . 
effective dose was estimated by different methods : ( i ) rando phantom associated with thermoluminescent dosimeters ( 6 ) , metal oxide semiconductor field - effect transistor dosimeters ( 3 ) , and optically stimulated luminescent dosimeters ( 1 )  . 
 ( iii ) monte carlo simulations ( 2 )  . conclusion cbct of extremities , cervical spine , ears and paranasal sinuses was found to be a low - dose volumetric imaging technique . 
2 , university offlorence azienda ospedaliero - universitaria careggi , largo brambilla 3 , 50134florence , italy 2 department ofradiology , university hospital paolo giaccone ofpalermo , via del vespro 127 , 90127palermo , italy 3 skanray europe , via cicogna , 38 , 40068sanlazzarodisavena , bologna , italy 4 department ofexperimental andclinical medicine , section ofrespiratory medicine , university offlorence azienda ospedaliero - universitaria careggi , largo brambilla 3 , 50134florence , italy vol . : ( 0123456789 ) 1 3 766 introduction cone beam computed tomography ( cbct ) is a volumetric imaging technique extensively used and well established in all areas of dental diagnostics [ 15 ]  . 
nevertheless , cbct is not used for contrast - enhanced examinations , does not have a high contrast resolution [ 15 ] , and the scan time is long with non - negligible motion artefacts [ 16 ]  . x - ray imaging for diagnostic purposes has gradually increased , which may have led to an increase in radiationinduced health risks [ 1719 ]  . 
for this reason , both in the usa ( senate bill 1237 ) and europe ( euratom directive 59 / 2013 ) legislations have been published that intensely request from operators to record the estimated patient dose of each radiation exposure in every radiology report [ 20 , 21 ]  . 
this may be useful not only for estimating the potential risk of radiation exposure but also for assessing protocol optimisation , standardisation , and quality assurance [ 22 ]  . currently , effective dose is the most commonly metric used to track patient dose and represents the stochastic health risk to the whole body , which is the probability to induce cancer and / or genetic damage from ionising radiation . 
it involves comparing dosimetric values from different examinations and modalities [ 23 ]  . radiation dose of cbct in dental use was already discussed by different papers [ 24 ]  . 
an additional purpose is to analyse the methods used to measure and estimate the effective dose . la radiologia medica ( 2018 ) 123 : 765777 materials andmethods literature searches the literature review was carried out in conformity with the preferred reporting items for systematic reviews ( prisma ) statement for studies focused on the dosimetric evaluation of cbct , except in dental applications . 
 prisma is an evidence - based minimum set of items that helps authors to improve the reporting of systematic reviews , although it is not a quality assessment tool to estimate the merit of a research [ 25 ]  . the search strategy was restricted to english - language papers via the pubmed and web of science databases . 
the following combined terms were investigated : radiation dosage , radiation protection , dose , effective dose , absorbed dose , and cone beam computed tomography ( table1 )  . 
 for the aims of this review , these terms were defined as follows : radiation dosage and radiation protection according to medical subject headings ( mesh )  . dose a generic term including all kinds of doses described by the international commission on radiological protection ( icrp ) [ 26 ]  . effective dose the sum of the products of the tissue weighting factors and the absorbed dose within the exposed tissues and organs of the bodyestablished by the icrp . absorbed dose the quantity of ionising radiation absorbed by a body , measured as the energy absorbed per unit massestablished by the icrp . cone beam computed tomography a volumetric imaging technique with a conic / pyramidal x - ray beam of radiation . the search in pubmed included both mesh and freetext terms , whereas the searches in web of science included only free - text terms . 
the searches were conducted on 12 november 2017 . inclusion andexclusion criteria we included studies published in international peer - reviewed journals that examined effective dose of non - dental cbct for diagnostic use . 
data were individually extracted from each study on ( 1 ) the type of endpoint , ( 2 ) the anatomical area , ( 3 ) the physical and technical features of cbct - units , especially scanning protocols , ( 4 ) the method to measure and estimate radiation dosage , ( 5 ) the features of dosimeters and phantoms , and ( 6 ) the effective dose . in case of disagreement over the study selection or data extraction , the issue was solved by consensus discussion among the reviewers . fifteen studies met our inclusion criteria . 
among the 15 papers selected ( 14 original papers [ 2740 ] and 1 conference proceeding [ 41 ] ) , two of them analysed two anatomical areas ; all the others analysed only one anatomical area ( table2 )  . 
one study [ 31 ] used a modified specific acquisition system that involved a pause during each exposure of the multiple frames to reduce potential motion artefacts generated by the rotating c arno physical / technical parameter was referred to in the three studies [ 34 , 37 , 41 ]  . 
 the tube voltage was mentioned in all the other studies , whereas some of them did not report field of view ( fov ) [ 28 , 29 ] , mas [ 30 , 38 , 39 ] , and voxel size [ 27 , 28 , 40 ]  . features ofdosimetry systems forcalculating effective dose the studies analysed in the current review measured or estimated the effective dose by using the following methods ( table3 ) : rando phantom associated with three different kinds of dosimeters thermoluminescent dosimeter ( tld ) [ 2729 , 32 , 33 , 41 ] , metal oxide semiconductor fieldeffect transistor ( mosfet ) dosimeter [ 31 , 35 , 40 ] , and optically stimulated luminescent dosimeter ( osld ) [ 36 ]  . 
all the others are older . the large variability in both the physical / technical features of the cbct - unitsespecially tube voltage , tube current , exposure time , and fovand the different methods used to measure or estimate the effective dose produced significant differences in the dosimetric values , thus making analysis of the results somewhat difficult . 
furthermore , since the description of the exposure parameters and scanning protocols was often incomplete , realising the reasons for the different results on the effective dose was hard . analysis ofdosimetry systems forcalculating theeffective dose tlds inserted in a rando phantom represent the conventional reference method for assessing the effective dose . 
nevertheless , tlds need to be replaced within the phantom after every exposure . 1 3 6 la radiologia medica ( 2018 ) 123 : 765777 1 3 la radiologia medica ( 2018 ) 123 : 765777 770 1 3 la radiologia medica ( 2018 ) 123 : 765777 since several exposures are recommended to attain more reliable dosimetric values , measuring the effective dose by tld is very laborious , time - consuming , and prone to mistakes . 
they can perform multiple real - time measurements without having to repeatedly disassemble and reposition the phantothe drawback of mosfets is that they are visible on the radiographs and produce a heel effect [ 42 , 43 ]  . oslds consist of crystals whose electrons collect the energy released from x - rays . 
at the dosimeter readout , the crystal is stimulated with a light - emitting diode , allowing the electrons to fall back to their original energy state while emitting a characteristic light proportional to the amount of the absorbed radiation dose . 
oslds have a small size and can be positioned on the patient sk although several considerations and conditionssuch as beam energy and spectrum , dose range , geometrical arrangement , and reading protocoltheoretically warrant the use of specific correction factors , these factors and the related uncertainties are mostly in the single - digit per cent in the typical conditions of medical diagnostic ct . 
 contrary to the perception by some , signal fading is not a significant issue over a period of several days or weeks if the oslds are handled properly [ 44 , 45 ]  . ctdi and dap are radiation dose outputs that indicate the amount of radiation directed towards the patient and allow one to compare the radiations of different ct systems . 
the dap measures the radiation dose to air ( without backscatter ) multiplied by the area of the x - ray field . the monte carlo simulation is a software - based technique used to simulate photon interactions with living matter since it tracks the trajectories of each individual photon and calculates the amount of energy released point by point . 
although up to 109 photons can typically be simulated with the computing power of current hardware and software resources , ct examinations involve a larger number of photons ( up to 1016 photons )  . 
the only paper [ 27 ] which compared monte carlo simulations and tld , while keeping unchanged all cbct - unit scanning parameters , found that monte carlo simulations underestimated the effective dose by more than 50% in the ears study and by 10% in the paranasal sinuses study , with respect to tld . radiation dose ofextremities andcervical spine knee ankle wrist koivisto etal . 
 [ 29 ] examined the ear by using tlds inserted in an alderson - rando phantothe resulting effective doses were 400 , 361 , 110 , and 80sv , respectively . 
the 1 3 772 la radiologia medica ( 2018 ) 123 : 765777 1 3 la radiologia medica ( 2018 ) 123 : 765777 1 3 774 la radiologia medica ( 2018 ) 123 : 765777 first two aforementioned authors [ 27 , 32 ] used a large fov including both ears , whereas the other two authors [ 28 , 29 ] did not mention the size of the fov . 
 [ 27 ] measured the effective dose via a specific fov ( 15 12cm ) for the paranasal sinuses study using both tlds inserted in an alderson - rando phantom and monte carlo simulations . 
in fact , each physical / technical parameter of every cbct - unit must be optimised in order to limit the exposure , reach a diagnostically acceptable image quality in relation to the clinical query , and allow the comparison of doses using different imaging techniques . the ear study requires a high resolution to detect the tiny structures of which it is constituted ; consequently , a high radiation dosage is needed [ 32 ]  . 
the dose can be generally reduced in the paranasal sinuses , cervical spine , and extremities studies , where the image quality is adequate even with low - dose protocols [ 32 , 33 , 50 ]  . 
low - dose protocols should be set in all imaging techniques with ionising radiation , especially in cbct , because of several units with extremely variable acquisition parameters and therefore very different exposures , as shown in the current review . 
furthermore , although cbct is considered to be a low - dose volumetric imaging technique , in clinical practice the repetition rate of examinations due to motion artefacts is not insignificant ( 0.95.4% ) [ 12 , 51 , 52 ] ; this increases the mean radiation dose administered to patients . overall , the mean cbct effective dose for the extremities ( 7.1sv ) was a little more than double and seven times the amount of one projection x - ray effective dose for the knee ( 3.0sv ) [ 40 ] and the footankle ( 1.0sv ) region [ 35 , 36 ] , respectively . 
the study of extremities by radiographs needs more than one plain film , and a bone fracture is not always detectable by two - dimensional medical imaging because of the geometric distortion effect and the superimposition of three - dimensional complex skeletal structures [ 53 , 54 ]  . 
therefore , we suppose that cbct may sometimes replace a conventional x - ray examination in extremity bone trauma turned into a first - level imaging since cbct assures high diagnostic accuracy in the detection of bone fractures [ 5558 ] with an acceptable radiation dose . using a standard rando phantom or a computational patient model has important limitations because neither system takes into account the constitutional nature of any individual patient and the wide range of scan protocols . 
in fact , a typical adult phantom does not represent an individual patient - specific habitus ; consequently , it will underestimate the dose for a paediatric patient and overestimate the dose for an obese patient because the x - ray beam is attenuated to a greater extent in large patients than in small patients [ 59 ]  . we noticed that the physical / technical parameters necessary to make the value of an effective dose meaningful were reported more thoroughly in the studies in which the primary endpoint was represented by a dosimetric study . 
we firmly believe that an accurate report of the effective dose must always be combined with a detailed description of both the physical / technical parameters of any unit and the dosimetry system adopted . 
similarly , reporting only the scanner output value is not appropriate since scanner outputs are not a real measurement of the patient dose , not unless they are combined with the conversion factors , taking into account the patients size / age / gender , irradiated organ , body composition , scan range , mas , and tube voltage [ 6062 ]  . currently , there are no conversion factors for non - dental cbct . 
 even more so , it is debatable to use the conversion factors of different technology systems as conventional x - rays or 1 3 la radiologia medica ( 2018 ) 123 : 765777 multislice ct . 
for that reason , future investigations on non - dental cbct conversion factors are recommended . we wonder whether it is proper to report the scanner output value for the estimation of patient dose in the radiology report as required by the latest international provisions . 
we think that mentioning the scanner output value in the radiology report is just the first step towards monitoring both the exposure to the population and the dose to the individual patient . 
it is desirable for the future to achieve a fast , easy , accurate , cost - effective , and unambiguous system for estimating the effective dose since dosimeters cannot be placed within the organs of a human being . 
the ideal solution to ensure reliable patient dose measurements would be to have every ctunit displaying the effective dose directly on the computer screen at the end of each examination by innovative software monte carlo simulation - like or reliable conversion factors in combination with scanner outputs . 
this is a hard challenge for research . the main limitation of our study was the impossibility of making a meta - analysis because of both the heterogeneity of the methods used to estimate the dose and the limited papers available on the various non - dental cbct applications . 
furthermore , although effective dose represents the most reliable metre used to track the dose for individual patients , effective dose is believed not to be an excellent parameter of patient risk per se [ 6365 ] and the stochastic radiation damage may be underestimated [ 66 , 67 ]  . conclusions the current review proved that cbct of the extremities , cervical spine , ears , and paranasal sinuses was a low - dose volumetric imaging technique . 
they can cause hematuria , anemization and flank paendovascular treatment is recommended due to its effectiveness . objective to assess the potential difference between the embolization of iatrogenic renal psa and iatrogenic renal psa + avf , in terms of technical and clinical success rate , procedure complexity and impact on the renal function . methods we retrospectively reviewed 30 embolization procedures of iatrogenic renal psa and renal psa + avf in 27 patients in two centers between december 2006 and february 2017 , comparing technical and clinical success rate , total procedural time , creatinine before and after the procedure and parenchymal ischemic area after the procedure . 
all patients underwent ct before embolization procedure and different embolization materials were used . results we identified 15 iatrogenic renal psa and 15 iatrogenic renal psa + avf ( causes : 23 nephron - sparing surgery , 2 nephrostomies , 1 lithotripsy , 1 ureteroscopic pyelolithotomy , 1 renal biopsy )  . 
microcoils were used in 21 cases , microcoils and spongostan in 3 cases , microcoils and controlled - release microcoils in 4 cases and controlled - release microcoils in 1 case . 
no significant statistical differences were found in the comparison of technical and clinical success rate , total procedural time , creatinine and parenchymal ischemic area after the procedure . conclusions transarterial embolization can be considered as the first - line treatment for renal artery iatrogenic lesions , considering its effectiveness . 
the image shows a renal artery pseudoaneurysm ( long white arrow ) in the third medium of the right kidney with simultaneous opacification of the renal vein ( short white arrows ) with arteriovenous fistula . 
b dsa before the embolization confirming an oval - shape pseudoaneurysm ( white arrow ) at the superior renal third without opacification of the renal vein nor of the inferior vena cava complexity of the procedure was evaluated by the total procedural time . 
3 box plot showing the comparison between the maximum diameter of the pseudoaneurysmal sac in the psa group ( blue ) and in the psa with arteriovenous fistula group ( pink ) ( p = 0.12 ) table 3 embolization materials materials no . 
4 graphic showing the comparison of the technical success ( p = 1.00 ) and the clinical success ( p = 0.59 ) in the psa group ( blue ) and in the psa with arteriovenous fistula group ( orange ) fig . 
5 box plot showing the comparison of the procedural time in the psa group ( blue ) and in the psa with arteriovenous fistula group ( pink ) ( p = 0.50 ) it was 105mol / l ( 60194mol / l ) in the group a and 100mol / l ( 49194mol / l ) in the group b . 
in group a , the post - procedural renal ischemic area was < 20% in 83.3% of cases ( 10 / 12 patients ) and between 20 and 40% in 16.7% of cases ( 2 / 12 patients )  . 
in group b , the post - procedural renal ischemic area was < 20% in 50.0% of cases ( 7 / 14 patients ) , between 20 and 40% in 21.4% of cases ( 3 / 14 patients ) and between 40 and 60% in 28.6% of cases ( 4 / 14 patients )  . 
there was no 1 3 la radiologia medica ( 2018 ) 123 : 742752 of the potential difference of technical and clinical success rate , renal function and kidney ischemia after the treatment . most psa are small and asymptomatic , and spontaneously disappeared ; in most cases , a conservative management is usually preferred . 
a strategy of treatment is considered mandatory for all psa regardless of their size or symptomatology ( anemization , flank pain , renal disfunction ) , due to the risk of rupture and bleeding [ 14 ]  . 
endovascular treatment by microcoils or stent graft has become the first choice of management of the renal psa because superselective catheterization enables successfully embolization with a minimum loss of normal renal parenchyma and has reduced invasiveness , high success rate and lower risk of complications . iatrogenic renal psa can be associated with avf and this , theoretically , increase technical difficulty of their endovascular embolization due to the risk of distal dislodgement of the embolization material as coils and particles . complications related to endovascular procedures are rare and the most frequent are nonselective embolization , nontarget occlusion , and additional arterial trauma . 
these can lead to a parenchymal loss , hypertension or renal failure . to the best of our knowledge , this is one of the largest series reported in the literature today and it was consecutively performed in two different centers , but a team member and the strategy of treatment were the same ( between 2006 and 2012 , center a , n = 6 cases ; between 2012 and 2015 , center b , n = 21 cases )  . in comparison with ierardi etal . 
 [ 13 ] reported 86 / 144 cases ( 69 psa and 17 psa + avf ) and 30 / 50 cases ( 21 psa and 9 psa + avf ) , respectively , but these studies were not targeted for evaluation of the results of the transarterial embolization . in our experience , high technical ( 90.0% overall ) and clinical ( 88.9% overall ) success were possible because of the fast clinical evaluation and multidisciplinary management of the symptoms and signs at debut . 
gross haematuria , acute flank pain , anemization and recent history of invasive and / or mini - invasive renal procedures are crucial for suspicion of iatrogenic renal vascular injuries . doppler ultrasound ( us ) , colour - doppler us , contrastenhanced us ( ceus ) and contrast - enhanced ct were evaluated and compared in previous studies to evaluate sensitivity and specificity . 
ct has the advantage to image the entire urinary tract and to exam even the urinary phase of the contrast - enhancement enabling to detect eventually an arterialurinary fistula ( auf )  . 
psa can be associated with avf , but a comparison of the results of theirs endovascular treatment is missing in the literature . to the best of our knowledge , this is the first large study of comparison of the endovascular treatment of iatrogenic renal psa ( n = 15 ) and psa with avf ( n = 15 ) , in terms 1 3 750 la radiologia medica ( 2018 ) 123 : 742752 in the literature , the reported technical success was until 100.0% [ 25 ] , but in our series the only 2 cases of partial embolization had a spontaneous complete clinical resolution . the clinical success reported in literature was until 95.0% [ 4 , 10 ] and similar to our study in which the only 2 cases of rebleeding were successfully treated by a second embolization procedure . technical ( psa group 86.7% , psa + avf group 93.3% ) and clinical ( psa group 84.6% , psa + avf group 92.9% ) success rates were not statistically different ( p > 0.05 ) , despite the hypothesis of major complexity of the iatrogenic renal psa embolization when associated with an avf . an explication can be the same technical procedure of embolization of a psa with or without avf ; the only additional risk factor for the embolization of an avf is the distal migration of the embolization material , but the detachable microcoils were used in few cases of psa ( 2 / 15 cases ) and psa + avf ( 3 / 15 cases ) with no statistical difference ( p > 0.05 ) , and no cases of distal embolization . in case of iatrogenic vascular renal injuries as psa or avf , there are two options of treatment : surgical or endovascular management . 
in recent years , transarterial embolization ( tae ) is became the first and effective method to control the hemorrhagic urological emergency ; previous studies have shown that the embolization of iatrogenic renal arterial injuries is a safe , tissue preserving treatment method , associated with high clinical and technical success rate , using different embolic agents [ 1517 ]  . in the endovascular management , the choice of the embolic material is important for a superselective and complete embolization of the target lesion and the material should be chosen according to the its characteristics ( size , flow , material availability , experience of the interventionalist and , last but not least , costs )  . 
coils , detachable coils , vascular plugs , stent grafts or liquid agents are the possible choices of treatment . our treatment preferred material was microcoils that allow a superselective embolization as distally as possible , to have a minimal parenchymal loss and are more controllable in particular in small vessels [ 18 ]  . the embolization using coils is not disadvantage - safe ; often more than a coil is required to have a complete embolization , and it is time - consuming . in two cases , we used spongostan to complete the sac embolization , because the coils were not enough to have a complete embolization ; as seen in most recent cases , it was not needful . 
an explication can be the proximal site of the avf when associated with psa , resulting in a proximal embolization of a larger renal artery branch and then in a greater renal parenchyma loss . in two patients only partial psa exclusion was obtained at the first endovascular treatment , but in oneof these hematuria spontaneously stopped and no psa was observed at 1 week ct study of follow up ; the other patient had rebleeding 22days after the first successful embolization , but a second tae of the reperfused psa sac was successful and uneventful . in one case , there was vasospasm during the procedure , unfortunately followed by a technical problem ; because of that the patient underwent the procedure in another hospital . a significantly impairment of the renal function was not observed ; in almost all cases , we observed a transient increase in the serum creatinine ( 1day after the procedure ) [ 19 ] followed by a non - significant decrease 3days after the procedure , as reported in the literature [ 20 ]  . 
transient elevation of the serum creatinine level is probably due to the amount of contrast material used during the procedure and before that in ct diagnosis [ 21 ]  . our technical success rate ( 90.0% ) was quite similar and comparable to that reported by other authors and our complication rate was much better than that reported by guneyli etal . 
 [ 22 ] , who has a higher number of cases , but not as large as in our study after nephron sparing surgery . other complications reported in the literature such as perirenal hematoma and surgical conversion [ 23 , 24 ] have not been noted in our study ; this indicates a limited parenchymal or renal function loss . no local complications in the puncture site occurred , even using mechanical hemostasis devices . complexity of the procedure was evaluated by the total procedural time . 
the fluoroscopy time was not available for the majority of patients and then we used the total procedural time that may be affected by other factors ( such as vasospasm and difficult anatomy ) that may dilate the procedural time but not necessarily the fluoroscopy time . there were no statistical significant differences of the total procedural time between the two groups but this does not allow to state no statistical significant differences of the procedural complexity . 
assumption of a greater complexity of the embolization of a psa with avf versus a psa cannot be confirmed from our study ; no study in literature 1 3 la radiologia medica ( 2018 ) 123 : 742752 evaluated this aspect nor the comparison of the procedural and fluoroscopy time in the two groups [ 2426 ]  . serum creatinine was assumed as an indicator of the renal function . 
the serum creatinine after 3days was considered a good index to evaluate the recovery of the renal function after the procedure because it allows the intravascular volume recovery and the contrast agent elimination . 
 we noted a transitory increase of the serum creatinine 1day after the procedure , due to impairment of the renal function caused by the contrast agent used during the preliminary ct study and during embolization procedure [ 19 , 21 ]  . 
the serum creatinine 3days after the procedure was similar to the base creatinine and there were no statistical significant differences between the two groups . the post - procedural renal ischemic area was considered a good index of the superselectivity of the embolization because the procedural goal was a peripheral embolization to minimize the renal parenchymal loss . 
our post - procedural renal ischemic area was similar to other study in the literature [ 3 ] , but we at first tried a stratification of the patients by the type of iatrogenic lesion . 
despite there was no statistical significant difference between the two groups ( p > 0.05 ) , the renal tissue sacrifice seems to be greater in psa + avf group . 
another study [ 25 ] examined the change in renal parenchymal volume before and after procedure by quantitative evaluation of the renal volume , but the mean loss of volume of 25.2% was determined in a small subgroup ( 10 / 25 , 40% ) of the patients . the main limitations of our study are the small sample size , the retrospective study nature instead of a randomized prospective trial , and the absence of a surgical control group ; these are due to the rarity of this type of lesions and because the nephron sparing surgery is a relative new surgical approach . 
because of that we decided to make a retrospective multicenter study to collect a number as large as possible of cases . recently , a larger study in a single center including 27 patients with iatrogenic renal arterial psa ( n = 16 ) , avf ( n = 7 ) or psa + avf ( n = 4 ) was reported [ 26 ] , but no comparison between the three subgroups of lesions was performed . in conclusion , the percutaneous embolization of the iatrogenic renal artery psa without or with an avf is safe and effective ; these iatrogenic renal artery injuries can be embolized with coils spongostan with a minimal renal tissue loss . 
psa with avf could be most challenging to embolize in comparison with only psa and require advanced technical skills and detachable embolization materials because they can determine a major renal tissue loss . acknowledgements the authors wish to acknowledge elisabetta balestro for english assistance . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
data on the baseline characteristics , technical success , clinical success , and long - term outcomes were collected and analyzed retrospectively . results the technical success rate of endovascular treatment was 100% . 
if it is applicable , ahv recanalization should be considered prior to treatment in order to achieve a longer patency . keywords endovascular treatment buddchiari syndrome hepatic vein accessory hepatic vein introduction buddchiari syndrome ( bcs ) is a rare disorder defined by hepatic venous outflow obstruction at any level of the hepatic vein ( hv ) and / or the inferior vena cava ( ivc ) that results in portal hypertension [ 14 ]  . 
at * yu li ssyuss@126.com 1 department ofinterventional radiology , pingliang peoples hospital , 296 east kongtong road , pingliang , gansu , china 2 department ofinterventional radiology , xuzhou central hospital , 199 south jiefang road , xuzhou , jiangsu , china 3 department ofradiology , xuzhou central hospital , 199 south jiefang road , xuzhou , jiangsu , china present , bcs can be divided into three types according to the different sites of obstruction [ 1 ] : hv - type bcs is defined as obstruction of three hvs ( left , middle , and right hvs ) ; ivc - type bcs is defined as ivc obstruction with at least one patent hv ; and combined - type bcs is defined as obstruction of both ivc and three hvs . different types of bcs require different treatment strategies . 
ivc recanalization is also well suited for most combined - type bcs disorders , since approximately 8689% of patients with combined - type bcs have the benefit of the compensatory and patent accessory hv ( ahv ) [ 1 , 4 ]  . 
 endovascular recanalization should be performed first , followed by trans - jugular intrahepatic portosystemic shunt vol . : ( 0123456789 ) 1 3 800 la radiologia medica ( 2018 ) 123 : 799807 ( tips ) if endovascular recanalization fails [ 515 ]  . 
most studies to date have focused on tips as the primary management of hv - type bcs [ 915 ] , and some recommend that tips should be its first - line treatment [ 15 ]  . 
previous studies have demonstrated that the cumulative 5 - year primary patency rates after endovascular treatment for hv - type bcs ranged from 60 to 90% [ 58 ]  . in this study , we aimed to determine the clinical effectiveness and long - term outcomes of endovascular treatment for hv - type bcs . materials andmethods the present single - center , retrospective study was approved by our institutional review board . 
informed consent for the procedure and clinical data management was obtained from each study patient . study design from june 2011 to august 2016 , 68 consecutive patients with symptomatic hv - type bcs underwent endovascular treatment in our center . 
patients were excluded if they had any of the following conditions : diffuse obstruction of three hvs without a compensatory ahv , asymptomatic bcs due to well - established intrahepatic collateral vessels , or bcs secondary to a malignant tumor . target vein selection diagnosis of hv - type bcs was established by reviewing the patients history and findings from abdominal ultrasound and abdominal magnetic resonance angiography ( mra )  . 
if the patient had the compensatory ahv and its obstruction length was shorter than that of all of the three main hvs ( left , middle , and right hvs ) , then the ahv was chosen as the target vein . procedures were performed by two interventional radiologists under fluoroscopic guidance . recanalization of the hv was performed using a right jugular vein approach . 
 the diameter of the stent or balloon needed to be 2mm larger than the hv / ahv diameter . if hv / ahv recanalization failed via the ivc approach , then an ultrasound - guided percutaneous trans - hepatic route was used to access the hv / ahv . 
a 21g chiba needle ( cook , bloomington , in , usa ) was punctured into the target hv / ahv , a 6f sheath and a 4f ver catheter were placed into the target hv / ahv , and a guide wire was sent through the catheter to detect the obstructed site . 
when the guide wire passed through the obstructed site , the distal tip of the guide wire was pulled out of the right jugular / femoral vein using a vascular snare ( atrieve vascular snare kit , medical device technologies , inc . , gainesville , fl , usa )  . 
patients were monitored for inr every week until a stable inr was achieved in the therapeutic range , and further monitoring was done once a month . endovascular treatment assessment oftreatment all patients were placed in the supine position . 
the follow - up ended if the patient died , underwent tips , surgical shunt , or liver transplant , or at end of the study period ( march 2017 )  . 
 the covariates incorporated into the multivariate analysis were variables found to be significant at p < 0.1 in the 1 3 802 la radiologia medica ( 2018 ) 123 : 799807 fig . 
the baseline data of the 68 patients are demonstrated in table1 . technical success endovascular treatment for hv - type bcs was technically successful in all 68 patients ( table2 )  . 
the diameter of the balloons ( cook , bloomington , in , usa , bard , murray hill , nj , usa , or cordis ) ranged from 10 to 16mthe stents used were 1014 - mm - diameter zilver stents ( cook ) or luminexx stents ( bard )  . 
these satisfactory results may indicate that endovascular treatment is effective for hv - type bcs . a step - wise procedure , according to the sequence of medical treatment - endovascular treatment - tips - liver transplantation , is recommended for treating bcs [ 16 ]  . 
if the preoperative radiological examination reveals a diffuse obstruction of the hv , tips can be performed directly [ 14 ]  . the strategy of endovascular treatment for hv - type bcs is recanalization of one hv with the shortest obstruction length [ 58 ]  . 
dilation of the obstructed hv with a large balloon catheter can provide sufficient radial mechanical force to disrupt the fibrotic and organized structure of the vascular wall [ 8 ]  . 
therefore , it is reasonable that the cumulative 5 - year primary patency rate in this study was lower than that in dings study . the type of bcs is an important risk factor for recurrence of bcs after endovascular treatment [ 20 ]  . 
among the patients with hvtype bcs , segmental obstruction ( > 1cm ) of the target vein was considered an independent risk factor of recurrence after endovascular treatment [ 6 ]  . in this study , we found that the primary patency duration of the ahv was significantly longer than that of the hv . 
these findings may explain why ahv had a longer primary patency duration than did the hv after endovascular treatment . on the other hand , the mechanism of obstruction between hv and ahv may be different . 
however , ahv obstruction occurs because the ostium of the ahv is restricted by the ivc wall and does not dilate along with the ahv stem dilation [ 17 ]  . 
third , although we found that ahv recanalization may achieve a longer patency duration , not all patients had the compensatory ahv ; thus , use of the ahv is only suitable for selected patients . in conclusion , endovascular treatment is an effective method that resulted in excellent long - term patency and survival in patients with hv - type bcs . 
if patients have the compensatory ahv , ahv recanalization can be considered in order to achieve a longer patency duration . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical statement all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
in one patient , proximal cuff insertion was previously performed , in three patients proximal cuff was urgently inserted but t1a el persisted ; one patient , previously treated with ovation abdominal stent graft system , was directly proposed for endovascular treatment . 
in all cases , endovascular embolization was successfully performed and the transfemoral approach was always chosen ; in one case it failed and translumbar approach by direct puncture of the sac was required . 
used embolization agents were glue , ethylenevinyl alcohol copolymer ( onyx ) and coils in three cases , n - butyl cyanoacrylate and onyx in one case , onyx and coils in the last case . results technical success rate was 100% as well as clinical success . 
clinical success was 100% until today and the sac diameter remained stable in four patients and decreased in one . conclusions onyx may be considered a suitable embolic agent in the treatment of patients with type ia endoleaks after evar , after failure of conventional treatments such as prolonged balloon inflation of the aortic neck or deployment of large bare stent . keywords endovascular treatment type ia endoleak embolization ethylenevinyl alcohol copolymer * gianpaolo carrafiello gcarraf@gmail.com 1 diagnostic andinterventional radiology department , san paolo hospital , university ofmilan , milan , italy 2 vascular surgery department , university ofinsubria , viale borri , 57 , 21100varese , va , italy interventional radiology , department ofradiology , insubria university , viale borri , 57 , 21100varese , va , italy 4 vascular surgery unit , department ofsurgery , san paolo hospital , university ofmilan , milan , italy 5 department ofradiology , caldarelli hospital , naples , italy introduction endovascular aortic aneurysm repair ( evar ) has been accepted as a standard procedure for an anatomically suitable infrarenal abdominal aortic aneurysm ( aaa ) [ 1 ]  . 
although evar is less invasive and can be the treatment of choice for high - risk patients , it might lead to a great number of complications and reinterventions [ 2 ]  . 
the prognosis of vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 638642 type ia endoleaks depends on the possibility of sealing the stent graft , proximally . 
an alternative approach , generally considered when the previously mentioned ones are unsuccessful or infeasible , is transcatheter embolization , which is a wellestablished treatment option for type 2 endoleaks [ 6 ]  . 
in the literature , short reports have described this technique : embolic agents used are coils or liquids agents [ n - butyl 2 - cyanoacrylate ( nbca ) or ethylenevinyl alcohol copolymer ( onyxcovidien , irvine , california , usa ) ] [ 69 ]  . we present eight cases of proximal type i endoleak with radiological evidence of expanding sac size , five of them had a contained rupture . 
the aim of this study was to evaluate the safety , technical success , and clinical success of embolization of type t1a el after evar using ethylenevinyl alcohol copolymer as an embolic agent alone or in combination with other materials . materials andmethods our internal review board approved the study . informed consent was obtained from all individual participants included in the study . 
from august 2013 to august 2015 , eight patients who presented with a type ia endoleak after evar [ six men and two women , average age 72.5years old ( range 6583years old ) ] were studied ( table1 )  . the treatment indications for exclusion of the el were : expansion and rupture of the sac ( five cases ) and increasing of sac size ( three cases )  . 
in this last case a 18 g ( biopsybell , mirandola ( mo ) , italy ) needle was used for the table 1 patients , indications , and technical aspects pts , age indications approach embolic agents follow - up efficacy complications onyx ( [ ] ; volume ) sac size ( mm ) pre post ag , 70yo transfemoral nbca + onyx 18 ; 1.5ml 24m , died none due to ima completely embolized fa , 83yo transfemoral coils + onyx 34 ; 1ml 12m , died of none ab , 70yo expanding transfemoral nbca + coils + onyx 18 , 34 ; 2ml none stroke 30m , alive cvb , 77yo expanding transfemoral nbca + coils + onyx 34 ; 3ml 18m , alive none mi , 77yo translumbar nbca + coils + onyx 18 , 34 ; 3.2ml 12m , alive none ds , 67yo transfemoral nbca + onyx 34 ; 2.8ml 12m , alive none ah , 65yo transfemoral nbca + onyx 18 , 34 ; 3ml 12m , alive none fg , 71yo transfemoral nbca + onyx 18 ; 2ml 15m , alive none pts patients , yo years old , nbca n - butyl cyano - acrylate , m months ; mm millimeters , pre pretreatment , post post - treatment expanding sac and rupture expanding sac and rupture expanding sac and rupture expanding sac and rupture expanding sac and rupture expanding completely embolized completely embolized completely embolized completely embolized completely embolized completely embolized completely embolized 1 3 la radiologia medica ( 2018 ) 123 : 638642 640 fig . 
1 contrast - enhanced ct revealed type ia endoleak ( a ) ; angiogram performed with angiographic catheter located in the access to the aneurysmal sac ( b ) ; angiogram performed with the microcatheter in the sac ( c ) ; image acquired at the end of the procedure , shows ethylene vinyl alcohol copolymer in the sac ( d ) percutaneous puncture performed under cone beam computer tomography ( cbct ) guidance with dedicate software ( xperguide , philips healthcare ) ; the microcatheter was introduced through the needle . 
used embolization agents were glue ( glubran ii , n - butyl - 2 - cyanoacrylate ( nbca ) ; gem s.r.l. , viareggio , italy ) , ethylenevinyl alcohol copolymer ( onyxcovidien , irvine , california , usa ) , and coils ( concertotm detachable coil system ; irvine , ca , usa ) in three cases , nbca and onyx in four cases , and onyx and coils in the last case ( table1 )  . 
embolization was stopped when the sac was filled completely ; final arteriogram confirmed complete embolization of the el . coils used presented a diameter of 20mm and a length of 40mm . patients were routinely monitored at our institution and follow - up included contrast - enhanced ultrasound ( ceus ) before discharge , computed tomography angiography ( cta ) at 30days , cta or ceus at 6months , and cta at 12months postoperatively , and annually thereafter . 
2 ruptured abdominal aorta aneurysm ( a ) ; persistent type ia endoleak after deployment of proximal cuff ( b ) ; angiogram performed after percutaneous puncture of the aneurysmal sac confirmed that there was an endoleak ( c ) ; embolization performed with coils , nbca and ethylenevinyl alcohol copolymer with the aim of filling remaining supplied gaps ( d ) ; minimum intensity projection ( mip ) reconstruction confirmed complete embolization : embolic agents ( coils , nbca , and ethylenevinyl alcohol copolymer ) take the conformation of the endoleak ( e ) completion angiography . 
safety was defined on the basis of minor or major complications related to the procedure [ 10 ]  . results technical success was 100% , with complete exclusion of the el being reached in all cases . 
follow - up did not show the reappearance of el type ia in any case ; in particular , one patient had a recurrence - free follow - up of 24months ( death due to myocardial infarction ) , and another patient had a follow - up of 12months ( death due to stroke )  . 
there were no procedure - related complications such as intraperitoneal bleeding , ischemic bowel injury , bowel perforation , or infection in the aneurysm sac or graft . discussion the incidence of type i proximal endoleak is more frequent in anatomically difficult situations , such as short neck diameter ( < 15mm ) , large neck diameter ( > 32mm ) , tapered necks , increased angulations ( > 60 ) , and landing zones with calcifications , thrombus , or uneven size [ 11 ]  . 
if an endoleak persists despite these measures , definitive therapy may require conventional open surgery , visceral artery bypass combined with stentgraft extension , or the use of chimney or periscope grafts to extend proximal and distal landing zones . patients not eligible for these more complicated procedures because of severe comorbidities or adverse anatomical factors may be treated by transcatheter embolization of the endoleak itself [ 9 ]  . 
there is limited published experience on type 1 endoleak embolization , and previous reports have involved coils and n - butyl 2 - cyanoacrylate ( nbca ) [ 8 , 11 ]  . 
 ethylenevinyl alcohol copolymer ( onyx , ev3 , irvine , ca , usa ) is a relatively novel nonadhesive liquid embolic agent , which is most commonly used to treat intracranial arteriovenous malformations [ 9 , 12 ]  . 
the authors described a reperfusion of the endoleak in one case that occurred 2days after the procedure ; in a second case , they showed an occluded endoleak but a small trace of contrast between the aortic wall and the stent - graother studies of a small series of patients [ 7 , 14 ] reported 100% technical success , although there were early occlusions of renal artery chimney grafts in one patient , and another patient experienced late stent - graft migration resulting in fatal aneurysm rupture at 18months post - embolization [ 14 ]  . 
our series presents a longer followup period , 16.5months ( range 1230months ) without any 1 3 642 la radiologia medica ( 2018 ) 123 : 638642 complication related to the procedure or to the embolic agent used and no el recurrences ; moreover , all type ia endoleaks of the series followed evar . 
 the vessels embolized with onyx are completely filled by the embolic agent , and they are less fragile because of the lower inflammatory reaction and the absence of polymerization heat when compared with nbca - embolized ones [ 15 ]  . 
in our experience , considering also endovascular embolization of type ii endoleak [ 16 ] , onyx could be useful to fill the remaining gaps of the sac filled with other embolic agents and to create a proximal cap . in our opinion , the advantage to use onyx in combination with other embolic agents is twofold : to limit expenditure , and most important , to exploit its characteristics , in particular the creation of a proximal cap is safer on the basis of the possibility to control injection . 
to this last point , the injection may be performed slowly and stopped when the desired embolization was reached . in conclusion , onyx may be considered a useful embolic agent in the treatment of patients with type 1 endoleaks after evar that are not suitable for standard therapeutic options . our results , in accordance with a few other publications , are promising . 
cohen kappa statistic was computed to estimate the reproducibility in correctly identifying lesions ; for multi - reader - multi - case ( mrmc ) analysis , weighted jackknife alternative free - response receiver operating characteristic ( wjafroc ) statistical tools was applied . results the intra - radiologist and inter - observer reproducibility values were the highest for the 0.165mm size pixel at 500cd / m2 display , for both chest lesions and bone fractures evaluations . 
as regards chest lesions , observer performances were significantly greater with 0.165mm size pixel display at 500cd / m2 than with lower maximum luminance and / or larger pixel pitch displays . 
concerning bone fractures , the performance obtained with 0.212mm size pixel display at 250cd / m2 was statistically lower than that obtained with 0.165mm sixe pixel display at 500cd / m2 . conclusion our results indicate that an increased maximum luminance level and a decreased pixel pitch of medical - grade display improve the accuracy of detecting both chest lesions and bone fractures . keywords digital radiography images roc curve radiographic image interpretation liquid crystal display medical grade display * manuela lualdi manuela.lualdi@istitutotumori.mi.it introduction 1 department ofradiology , fondazione irccs istituto nazionale dei tumori , via venezian 1 , 20133milan , italy 2 department ofradiology , ospedale san bassiano , via dei lotti 40 , 36061bassanodelgrappa ( vi ) , italy 3 medical physics unit , fondazione irccs istituto nazionale dei tumori , via venezian 1 , 20133milan , italy 4 medical statistics , biometry andbioinformatics unit , fondazione irccs istituto nazionale dei tumori , via venezian 1 , 20133milan , italy information andcommunication technology unit , fondazione irccs istituto nazionale dei tumori , via venezian 1 , 20133milan , italy regardless of how a digital radiography image is produced , the information content conveyed to the eye of the observer depends on how faithfully and reliably the image is displayed . 
medical - grade displays used for the interpretation of plain radiography images should meet the american college of radiology ( acr ) , the american association of physicists in medicine ( aapm ) and the society for imaging informatics in medicine ( siim ) technical standard for electronic practice of medical imaging 2012 guidelines [ 1 ]  . 
 according to these recommendations , the pixel size of a diagnostic display should be about 0.200mm and not longer vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 586592 than 0.210mm , the maximum luminance , lmax should be at least 350cd / m2 and the minimum luminance in the presence of ambient light , lmin should be at least 1cd / m2 . 
furthermore , to the best of our knowledge , only three studies [ 57 ] have investigated the role of maximum luminance in the evaluation of radiographic images , but the reported results may have a bias because of the different technology and panel of the analyzed displays . the purpose of this study was to investigate the effect of both pixel pitch and maximum luminance of medical grade displays on observer performance for detection of bone fractures and chest lesions depicted in digital radiography images . 
medical - grade displays produced by a single manufacturer were utilized , in order to rule out any manufacturing difference from the experimental setting and so to ensure that the feedback on the two selected parameters , pixel pitch and luminance , were not influenced by other factors such as different white point or different reflection coefficient . materials andmethods this study consists of a retrospective interpretation of chest and bone digital radiography images provided by two research institutions ; the protocol of the study was approved by the ethics committee of the lead institution . 
the procedure of the chest study is described in details ; for the bone study , only discrepancies are highlighted with respect to the chest study . equipment four liquid crystal display ( lcd ) monochrome medicalgrade displays of the same vendor ( nec display solutions ltd , tokyo , japan ) were used for this study ; the technical characteristics of the selected displays , labeled in this paper by letters from a to d , are summarized in table1 . the stock faceplate of the displays was covered so that no textual information or model number was visible to the observers . 
each display was initially calibrated according to the dicom part 14 gsdf and accounting for the ambient light of the reading room they were used in ( less than 25lx )  . 
 all the chest images were acquired using a fdr velocity - u digital radiography device ( fujifilm medical system , ct , usa ) , with a pixel pitch of 0.100mexposure parameters were 115120kvp and 58mas with a 180 - cm source to detector distance . the images selection was performed using the 0.165mm size pixel display at 500cd / m2 ( display c in table1 ) by a senior radiologist with more than 30years experience in the interpretation of chest images . 
the selection was made on the basis of different levels of interpretative difficulty in terms of lesions features and sizes as well as background pattern in order to reflect the spectrum and complexity of the diagnoses encountered in the daily practice ; accordingly , for each of the three subsets of images the requirement was to have one - third of easily assessable images , one - third of intermediate difficulty and one - third of higher interpretative difficulty . 
cases of micronodules and pneumothoraces were selected on the basis of confirmation with computed tomography ( ct ) findings ; negative images were confirmed on the basis of the existence of a minimum diseasefree period following either a negative biopsy result or a negative radiological finding . images were anonymized and blindly evaluated on the considered displays by radiologists with varying degrees of expertise : one senior radiologist with more than 30years experience in the interpretation of chest images and two junior radiologists with 1 ( junior 2 ) and 5years experience ( junior 1 )  . 
all observers have reviewed all of the images twice ( in the following , first and second reading sessions ) ; this allowed us to verify an appropriate intra - observer reproducibility . 
the first reading of the senior is the one that has led to the selection of cases and in the following will be referred to as reference evaluation ( ref )  . the reading sessions were held between november 2015 , first evaluation , and december 2015 , second evaluation , with the second session being held at least 2weeks after the first reading session . 
to rule out adaptation and visual fatigue effect , every observer was required to examine the images in their own time , restricting to a maximum of five consecutive images on a certain display . 
the observers were asked to complete an evaluation module for each image , rating the presence of the selected chest lesions on a five - point confidence level ( percentage cl ) : 20 , 2040 , 4060 , 6080 and greather than 80 , with100 percentage indicating absolute certainty the lesion was present or absent . 
the localization of each abnormality was indicated by the area of the chest with suspected lesion ( upper left , upper right , lower left , lower right )  . 
the observers were unaware of the number of potential findings , so they were free to report more than one finding per subject . bone study thirty - two bone digital radiography images were selected among those performed from august 2012 to october 2015 . 
 all the bone images were acquired using an eidos 3000 digital radiography device ( mecall srl , milan , italy ) , with a pixel pitch of 0.143mexposure parameters were 4680kvp and 6180mas with a 110 - cm source to detector distance . in the selection phase ( october 2015 ) , the 0.165 - mm size pixel display at 500cd / m2 ( display c in table1 ) was used by a senior radiologist with more than 20years experience in the interpretation of bone images . 
 in most cases , the presence or the absence of the fractures was confirmed by means of computed tomography ( ct ) or magnetic resonance imaging ( mri ) findings . 
only in few cases the confirmation of the diagnosis was obtained by retrieving the results from follow - up procedures . the reading sessions were held between october 2015 and may 2016 . 
one senior radiologist with more than 20years experience in the interpretation of bone images and two junior radiologists with 1 ( junior 2 ) and 3years experience ( junior 1 ) were the observers . 
all observers have reviewed all of the images twice ( in the following , first and second reading sessions ) ; overall , 32 ( cases ) 4 ( displays ) 3 ( observers ) 2 ( sessions ) = 768 readings were made . statistical analysis concordance analysis was performed in order to estimate the different patterns of agreement , such as the intra - observer and inter - observer agreement . 
due to the nature of the variables involved in this analysis the cohens kappa statistic ( kc ) [ 10 ] and its 95% confidence interval were computed ; kc values were interpreted in a qualitative manner on the basis of the landis and koch classification criteria [ 11 ]  . 
specifically , for the inter - observer agreement ( each radiologist vs each other and each radiologist vs the reference evaluation ) only data arising from the second reading were used . subsequently , data were also analyzed by applying the well - defined statistical tool developed within the multireader - multi - case ( mrmc ) scheme [ 12 , 13 ]  . 
the developed five - point score and the reference evaluation were used to investigate the performance of each medical display and of each observer in terms of alternative free - response receiver operating characteristic analysis ( afroc ) by considering the data arising from the second reading session only . 
specifically , the weighted jackknife afroc ( wjafroc ) [ 14 ] figure of merit ( fom ) was computed by using the obuchowskirockette ( or ) procedure with hillis improvement as significance - testing method [ 15 ]  . 
the jafroc paradigm were chosen in order to take into consideration both the detection and localization of the suspected abnormalities . all statistical analyses were performed using the sas ( version 9.2 , sas institute inc . , cary , nc ) and r software ( version 3.3.0 ; r foundation for statistical computing , vienna , austria )  . results to evaluate the different pattern of concordance ( intraand inter - observer agreement ) , a single pivotal variable was created by jointly considering the type of lesion and its localization , if present . 
similarly , for the bone study , the highest intra - observer reproducibility values were obtained for display c ( kc : 0.900 and kc : 0.717 for junior - 1 and junior - 2 , respectively ) , and the lowest ones on display b and d ( kc : 0.685 and kc : 0.450 for junior - 1 and junior - 2 , respectively )  . as far as the inter - observer agreement , table2 reports the kc values obtained in the chest study ( section a ) and bone study ( section b )  . 
for both chest and bone studies , the highest kc values were observed for display c in all the performed comparisons , except for the junior - 1 versus senior comparison in the bone study , where the highest kc value was obtained for display d . 
moreover , by looking at the junior - 1 vs senior comparison at least a moderate agreement was obtained with all the displays ( kc range 0.5160.770 for chest study and kc range 0.7230.850 for bone study ) , whereas by looking at the junior - 2 vs senior results , lower kc values were observed . 
on the contrary , junior - 1 judged all the images as sub - optimal or optimal with all the displays , with the exception of four images evaluated as excellent with display a . 
as far as the bone study , the majority of the images were evaluated as optimal by the senior with all the displays , with a small predominance for the display b , that is the one in use in daily clinical practice . 
very few images ( maximum 3 for each observer and monitor ) were considered of excellent quality . 1 3 la radiologia medica ( 2018 ) 123 : 586592 finally , with concern to the reading times of chest images , a median value of 1min was registered for all the displays within each observer . 
for the bone study , the reading time ranged from 1 to 4min , with an overall median value of 2min . discussion the smaller the pixels and the greater their number , up to a point , the more faithfully can a representation capture the original . 
for a 6075cm typical viewing distance , the best visibility is no better than 0.2mm and , with close viewing from half that distance , 0.1msince technology should not restrict the ability of the observer , for the presentation of 5mp digital radiography images acquired with a detector pixel pitch of about 0.1000.200mm , it is desirable to use medical displays with similar pixel pitch to ensure that spatial details in the acquired image are preserved onto the medical display in use and to require less zoom / pan adjustment when the observer desires to view the full resolution image dataset . 
furthermore , as the number of just noticeable differences ( jnd ) is a function of display luminance , it is also desirable to use displays with a high maximum luminance value to achieve a high luminance ratio , by not lowering below 1cd / m2 the minimum luminance value in the presence of ambient lighting . in this work we evaluated 0.165mm size pixel displays , conventionally used in mammography , in comparison with 0.212mm size pixel displays typically used for plain radiography . 
for each of the two selected pixel pitches , the effect of two maximum luminance values was investigated : 500cd / m2 , that is the calibration value proposed by most medical displays manufacturers , and 250cd / m2 , that is the average residual luminance after about 10 , 000 backlight hours of our medical - grade displays . 
a luminance value of 250cd / m2 is lower than the minimal requirement indicated in the acr guidelines ( 350cd / m2 ) but higher than that reported in the iec 62563 - 1 recommendations ( 170cd / m2 ) and implemented by standard protocols for medical display quality control ; displays with a luminance value of about 250cd / m2 are routinely used for reporting . 
the results of our study suggest that an increased maximum luminance level and a decreased pixel pitch of medical - grade display improve the accuracy of detecting both chest lesions and bone fractures . 
from the data concerning the perceived image quality , we point out that both senior radiologists evaluated as optimal or excellent , the images reproduced by the display used in daily clinical practice : 0.165mm pixel size display at 500cd / m2 for chest images , with which the best performance results were also obtained , and 0.212mm pixel size display at 250cd / m2 for bone images , with which , interestingly , the worst performance results were obtained . 
these findings suggest that radiologists get used to the instrument routinely utilized and perceive as optimal the images that are represented in the way they are accustomed and not those actually ; display technology , on the other hand , seems to affect diagnostic performance regardless of device habit and image quality perception . finally , some notes about the possible limitations of the current study should be mentioned . 
this choice was made to ensure that the feedback on the two selected parameters , pixel pitch and luminance , was not influenced by other technical factors related to the manufacturing of the displays . 
the replication of the study on displays from other brands with different panel characteristics could be of interest and it was partially accomplished with a pilot study on the subject , carried out at the same time of our research work . 
however , according to both the overall number of cases evaluated by the senior radiologists during their routine clinical activity and the time interval occurred between case selection and case evaluation ( more than 2months ) we are confident in the generated results . 
finally , although our analysis outcome has some limitations because of the small number of digital radiography images utilized , the evidence gathered in this study corroborates the findings of other studies [ 7 , 17 ] about the impact of luminance levels and pixel pitch on the observers performance . 
the data generated from this study , as well as those generated by our other studies focused on different radiological modalities [ 18 ] , can be viewed as exploratory , aiming at a deeper evaluation of the impact of the physical parameters of medical displays in the interpretation process of radiological images . this study has potential for a clinical effect by providing an estimate of the influence of medical - grade displays with different pixel pitch and luminance on the correct evaluation of digital radiography images . 1 3 592 la radiologia medica ( 2018 ) 123 : 586592 funding the authors state that this work has not received any funding . compliance with ethical standards conflict of interest the authors of this manuscript declare no relationships with any companies , whose products or services may be related to the subject matter of the article . 
the patients were divided into three subgroups according to the cardiac t2 * values as the high - risk group ( t2 * mri < 10ms ) , mediumrisk group ( t2 * mri 10 - 20ms ) , and the low - risk group ( t2 * mri > 20ms )  . results the majority of patients used dfx ( deferasirox ) ( 79% ) and deferiprone ( dfp ) ( 17% )  . 
thalassemia syndromes are divided into two groups according to transfusion requirement , non - transfusion - dependent ( ntdt ) and transfusion - dependent ( tdt ) thalassemia [ 1 ]  . 
although most clinics use iron - chelating agents to prevent iron accumulation in the heart and liver , congestive heart failure is still a leading cause of death in patients with tdt [ 2 ]  . 
after the introduction of t2 * mri assessments in the 2000s , this technique has shown to be a consistent indicator for iron deposition and important guidance for planning of chelation therapies [ 6 , 7 ]  . the aim of this study was to assess the cardiac and liver iron depositions of patients with tdt using mri , and also to screen the relationship between t2 * mri values with serum ferritin levels and chelation therapy . materials andmethods design ofstudy this research was designed as a retrospective , singlecentered study , conducted in istanbul university , istanbul medical faculty thalassemia center , which is the one of the oldest and largest thalassemia centers in turkey . 
 one hundred patients were followed up by other centers and admitted to our radiology center for mri examinations only . finally , a total of 106 patients , who were followed up in istanbul medical faculty thalassemia center , were evaluated for this study . 
forty - eight patients had more than one follow - up mri examination obtained after approximately every 2.7years. when the second mri measurements were analyzed , patients in the high - , medium - , and low - risk patients underwent repetitive mri tests ( two - thirds of lowand high - risk hepatic groups , and three out of four medium - risk cardiac groups according to t2 * level )  . 
further investigation into why some highand medium - risk group patients did not undergo second mris was performed , which revealed that these patients were recruited for other clinical and international studies conducted in our center . 
seventy - nine percent of patients used deferasirox ( dfx ) as an oral chelator , 17% used deferiprone ( dfp ) , 2% used deferoxamine ( dfo ) , and 2% used combined therapy ( dfo + dfx )  . 
forty - three percent of patients with tdt underwent splenectomy . magnetic resonance imaging the t2 * mri assessments of patients were performed on a 1.5 tesla mri ( achieva , philips medical systems , best , the netherlands ) and conducted at the department of radiology . 
acquisition parameters were as follows : repetition time 400ms , flip angle 45 degrees , matrix 120 93 pixels , field of view 35cm , sampling bandwidth 1082hz , and 21s of breath - hold in each slice . in myocardial imaging , a mid - ventricular short - axis slice was acquired at six different echo times with delta te of 2.2ms. 
acquisition parameters were as follows : repetition time of radiofrequency pulses 15ms , flip angle 30 , matrix 128176 pixels , field of view 35cm , sampling bandwidth of 2777hz . 
the repetition time was adjusted according to the patients heart rate as displaying a gating delay time of 0ms after the r - wave in order to reduce motion artifacts . 
left ventricular dimensions and function were assessed by long - axis cines and shortaxis cines . background noise was subtracted from the signal intensity of the selected region of interest and calculated in each image using thalassemia tools ( a plug - in of cmr tools , cardiovascular imaging solutions , london , uk )  . 
t2 * was calculated automatically using the formula : y = kete / t2 * , where ke is a constant , te and y represent the echotime and image consecutive signal intensities . 
the patients were classified as high risk if their myocardial t2 * mri values were < 10ms , medium risk if they were between 10 and 20ms , and low risk if they were > 20ms in terms of cardiac complications [ 9 ]  . participants data analysis one hundred six patients with tdt ( mean age : 21.9years ; range 846years ) were evaluated for this study between data were collected retrospectively from laboratory results , radiology reports , and patient files . 
the sociodemographic and general characteristics of the patients are demonstrated in table1 . serum ferritin levels were significantly correlated with lics ( rs = 0.63 , p < 0.001 ) , hepatic t2 * values ( rs = 0.58 , p < 0.001 ) , but not with cardiac t2 * values ( rs = 0.20 , p = 0.07 ) in patients with tdt . 
risk groups classified according to cardiac t2 * values as described in methods section showed no significant differences in terms of serum ferritin levels , lic , and hepatic t2 * values . 
the lic significantly reduced and hepatic t2 * values significantly increased , whereas cardiac t2 * values did not change in the second mr measurements of patients with tdt ( p = 0.01 , p = 0.05 , p = 0.12 , respectively ) ( table3 )  . 
the ratio of the sum of the highand medium - risk groups to the total , according to cardiac t2 * and hepatic t2 * values , was significantly diminished in the second mri results ( p < 0.01 ) ( table4 )  . 
therefore , ferritin may be a poor indicator of total body iron [ 14 ]  . in the 2000s , cardiac and liver mri techniques were developed [ 8 , 15 ] for detection of body iron overload . 
however , patients using the dfx chelator demonstrated a dramatic reduction in lic in follow - up . the repetition of mri evaluations at regular intervals could be performed for efficient monitoring of total body iron content . 
in a comparative study , it has been shown that dfp was efficient in reducing cardiac iron burden , and dfo was effective for decreasing liver iron deposition [ 13 ]  . the consistency of these mri results reveals an important guidance for chelation therapy in patients with beta thalassemia because cardiomyopathy and heart failure due to iron overload is reversible by the selection of effective chelation therapy [ 4 ]  . approximately three in four patients in our study group were in the safe zone in terms of cardiac iron burden . 
 moreover , the second mr results after a mean 2.7 - year follow - up period showed a significant decrease in the ratio of mediumand high - risk groups to the total in terms of liver and cardiac iron deposition . 
this high rate in the low - risk group and decrease in the high - risk group could be a result of good clinical follow - up , effective chelation therapy regimen , and good adherence to chelator treatment . the limitations of this study are the retrospective design , omission of drug interaction and antioxidant status , the 1 3 576 la radiologia medica ( 2018 ) 123 : 572576 relatively small sample size , and non - equal chelator groups . 
wood jc , enriquez c , ghugre n etal ( 2005 ) mri r2 and r2 * mapping accurately estimates hepatic iron concentration in transfusion - dependent thalassemia and sickle cell disease patients . 
the aim of this study was to investigate the role of alberta stroke program early ct score based on diffusion weighted imaging ( mr - aspect ) in the assessment of brain damage pre - evt , patient selection for evt and outcome . materials and methods we included in this study patients with national institute of health stroke score ( nihss ) at admission 8 , mr - aspect 5 and anterior ais , who were treated with evt in our hospital . 
we evaluated aspect score at admission ( ct - aspect - in ) , 24h after evt and at discharge , nihss , modified ranking scale ( mrs ) , thrombolysis in cerebral infarction scale ( tici ) , onset - to - intervention - delay ( otid ) and collateral circulation score ( ccs )  . results 68 patients ( mean age 78 11.9years ) were included in this study . 
mr - aspect score correlated with post - evt outcome better than ct - aspect - in scores . conclusion mr - aspect score based on diffusion weighted imaging is useful for the selection of patients with ais that can have a favourable outcome from evt . 
before evt , non - contrast head ct and ct - angiogram are usually acquired and the alberta stroke program early ct ( aspect ) score [ 6 ] is computed on noncontrast ct scan ( ct - aspect )  . 
in patients with ais with an unclear vol . : ( 0123456789 ) 1 3 610 la radiologia medica ( 2018 ) 123 : 609617 time of onset , mr imaging , based on dwi / flair mismatch , is safe and efficient for patient selection [ 8 ]  . 
indeed , a favourable outcome [ i.e. , modified ranking scale ( mrs ) 02 ] was found in the 61% of patients with unclear - onset stroke , an mr - aspect score 5 and a clinical - diffusion mismatch [ 8 ]  . 
recent evidences suggest that large dwi lesions ( 70100ml ) ( i.e. , a low mr - aspect score ) , are highly predictive of poor outcome after reperfusion [ 6 , 813 ]  . 
as a standard protocol in our hospital , these patients were labelled as stroke code patients and a dedicated expert stroke neurologist performed national institute of health stroke score ( nihss ) evaluation . 
all patients with nihss 8 , mraspect 5 and with major vessel occlusion , were selected for evt . imaging acquisition parameters ct scan was performed using a multidetector scanner ( somatom definition as 64 , siemens healthcare , germany )  . 
ct scans were acquired using contiguous axial images , acquired on standard orbitomeatal plane from foramen magnum to vertex ( 1mm3 isotropic voxel ; kvp = 120 , mas = 360 )  . 
a 8 - fr guiding catheter ( neuron max 088 penumbra ) or a 9 - fr balloon - guiding catheter ( merci concentric , boston scientific ) was placed in the common / internal carotid artery . an intermediate catheter ( ace 64 penumbra ) and a microcatheter ( headway , terumo microvention ) were used to perform intracranial thrombectomy with stent retrievers ( solitaire fr medtronic )  . 
in case of thromboaspiration , a 5max , ace , ace64 ( penumbra ) or a sofiatm plus ( terumo microvention ) were advanced over a microcatheter ( headway terumo microvention ; 3 max penumbra ) to the occlusion site . 
evt were performed in conscious sedation or in general anaesthesia . data collection for each patient we collected the following data : 1 3 la radiologia medica ( 2018 ) 123 : 609617 1 . 
dwi based aspect score ( mr - aspect ) and ctaspect score were retrospectively computed on admission ct ( ct - aspect - in ) and on a ct scan performed 24h after intervention ( ct - aspect - 24 ) ; 3 . 
collateral circulation score ( ccs ) [ 18 ] , which describes the ability of collateral circulation to supply the area involved in the ischemic stroke , and has a value range between 0 and 5 ( where 5 is the best collateral condition and 0 the worst one ) ; 5 . 
thrombolysis in cerebral infarction scale ( tici ) [ 19 ] , which consists of 5 items : 0 , 1 , 2a , 2b and 3 ( where 0 represents the absence of recanalization and 3 a complete one )  . 
mrs [ 20 ] , a scale used to calculate the clinical outcome , was calculated at 3 - month follow - up after discharge ( mrs - 3m )  . 
asymptomatic haemorrhagic transformation revealed by a ct examination 24h after evt ; our final study population included 68 consecutive patients ( 37m , 31 f , mean age 78years 11.9years ) who underwent evt due to an ais over 1 - year period . 
concerning nihss at discharge , 55 of the 68 ( 80.9% ) patients had an improvement of their neurological status compared to admission , no improvement was registered in 1 patient ( 1.5% ) , and a neurological worsening was observed in 12 of the 68 patients ( 17.6% ) , with 8 patients deceased at discharge . the nihss - 24 correlated with ccs and tici class . 
complications occurred during evt ( if any ) , namely perforation and embolic occlusion of new territories . statistical analysis statistical analyses were conducted to understand which factors better help to predict patient outcomes , according to nihss - 24 and mrs - 3moreover , we tested if there was any difference between the mrand ct - aspect scores at admission . 
non - parametric friedmans test for paired samples was used ; in addition , non - parametric spearmans correlation coefficient as well as non - parametric mannwhitney tests for independent samples , kruskallwallis and fishers exact tests were employed when required . 
significant cutoff was set to 0.05 , and bonferroni corrected when necessary . the outcome at 3months evaluated with the disability scale ( mrs - 3m ) correlated with recanalization after evt ( tici ) ( table2 )  . 
patients with poor recanalization reported the most severe disabilities ; conversely , patients with good recanalization had a favourable outcome at 3 - month follow - up ( table3 )  . 
a significant negative correlation was found between ct - aspect - 24 and mrs - 3m our study suggests that mr - aspect score based on dwi applied to patients with ais strongly correlates with ctaspect score calculated 24h after evt . 
indeed , by means of a retrograde flow , collateral circulation temporarily vascularizes the involved brain areas preventing cell death and sustaining penumbra [ 21 , 22 ] , thus mitigating neurological deficits and influencing aspect score . 
in our study , in patients with high ccs ( 3 and 4 ) , mr - aspect scores 1 3 la radiologia medica ( 2018 ) 123 : 609617 fig . 
a box plots show the distribution of differences between ct - aspect - 24 scores and aspect at admission ( ct - aspect - in and mraspect ) for tici - c class : ct - aspect data are shown in dark gray ( light gray for ct - aspect - in data )  . 
positive correlations were observed only in subjects falling in tici - c class ; however , the correlation was higher when considering mr - aspect scores , as it can be evinced from the slopes . 
this result may be explained by the fact that collateral circles likely sustain penumbra and prevent ischemic core enlargement until complete recanalization is achieved , and reperfusion occurred . most of the patients that underwent evt had a decrease of the neurologic deficit , as demonstrated by longitudinal nihss analysis . 
hence , ccs and tici scores can help clinicians to predict patient recovery after intervention . we also observed a systematic nihss - 24 decrease for patients with a complete vascular recanalization ( tici score = 3 )  . 
it is worth mentioning that ct - aspect - 24 showed a clear negative correlation with mrs - 3m , thus highlighting the fact that ct - aspect - 24 score may help clinicians to predict patients long - term recovery . 
this correlation is most likely due to the fact that ct - aspect - 24 shows irreversible brain damages that define permanent neurological deficits . nonetheless , evt recanalization does not correspond always to reperfusion , since reperfusion can occur only in penumbra , which is still vital and rescuable brain tissue . 
the extend - ia trial [ 2 ] showed an nihss reduction > 8 points or nihss in range 01 at 72h was observed in 80% of patients with thrombectomy vs 37% observed in control group . 
moreover , mrs - 3m falling in 02 range was found in 71% of 1 3 la radiologia medica ( 2018 ) 123 : 609617 thrombectomy patients vs 40% observed in controls [ 2 ]  . 
in our institution , all patients with a clinical suspicion of ais were labelled at admission as stroke code patients and a dedicated expert stroke neurologist performed a clinical examination in the emergency rooa brain ct was performed immediately after on each stroke code patient . 
this allows a timely diagnosis and treatment for our stroke code patients . after the ct scan , if no haemorrhage was proved , mri evaluation was performed in all patients with a nihss 8 , with no age cutoff . 
 for the ischemic core evaluation , we preferred the use of mr imaging than perfusion - ct ; indeed , our perfusionct protocol is able to acquire only a limited brain slab , which is a suboptimal condition to a proper evaluation of the ischemic penumbra . 
for this reason and for the strict closeness of the mr unit to digital angiography room , we used this approach . mr imaging was performed with 8 - min and 45 - s scan protocol that allowed the assessment of the ischemic core wideness and the site of vessel occlusion . 
ischemic brain damage was visualized on a dwi based adc map ( b = 1000s / mm 2 ) and evaluated by means of aspect score ( mr - aspect ) [ 6 ]  . 
to save more time ( 102s ) in the mr acquisition , we may speculate that b = 0s / mm2 images of dwi could be used in further studies as t2 - weighted images . 
indeed , vo and colleagues [ 13 ] proved that dwi is the best technique to identify hyperacute infarction within 6h and true diffusion lesion reversal is rare and not clinically significant . 
a score of 10 corresponds to absence of impaired brain areas , and 1 point is later on subtracted for each ischemic area ( i.e. , mass effect , abnormally low attenuation in white matter , loss of demarcation of the gray / white junction )  . 
it is worth remarking that an early start of evt is crucial for patients prognosis . neurological deficits in ais are due to the involvement of two distinct regions , namely the ischemic core and the penumbra [ 26 , 27 ]  . 
indeed , selected patients showed a small ischemic lesion on mr - aspect despite high nihss , meaning that involved , but still rescuable , areas were wider than the ischemic core found on dwi . moreover , the use of mr allow a reliable timing of ais onset with an earlier detection of brain damage with dwi / adc , followed by flair and t2 [ 30 ]  . 
further , flair sequences may show collateral circulation with the well - known spaghetti sign that is an early sign of acute ischemic stroke and correlates with the dwi / pwi mismatch [ 31 , 32 ]  . fast imaging protocol and fast evt are necessary . 
particular attention was given in our study to the aspect evaluation through ct or mr - dwi before evt , to identify patients with a small infarct core that could really benefit from revascularization and reperfusion . we observed that ct based aspect scores were always higher than those measured via mr - aspect based on dwi . 
 this result was not unexpected , since it is known that dwi sequences are able to precociously detect irreversible alterations of brain , which become evident only at a later stage with ct . the main limitation of our study is the small number of patients related to the fact it is based on a single - centre experience . conclusion mr - aspect score based on dwi is useful for patient selection for evt and correlates with outcome , as demonstrated through the evaluation of mrs - 3m and nihss24 . 
our results confirm that a timely performed evt is an important factor for a good clinical outcome in stroke patients . 1 3 616 la radiologia medica ( 2018 ) 123 : 609617 compliance with ethical standards conflict of interest antonio pitrone declares unrelated conflict of interest : consultancy : medtronic . 
in case of suspected vascular malformations time - resolved mr angiography might add important information for therapeutic decisions and follow - up . objective the objective of our study was to assess the usefulness and diagnostic performance of time - resolved imaging of contrast kinetics sequence in the evaluation of peripheral vascular anomalies . subjects and methods sixty - six patients ( 23 pediatric , 43 adult ; mean age 26 ) affected by upper or lower limb vascular anomalies and studied using time - resolved imaging of contrast kinetics sequence were prospectively evaluated . 
all studies were performed on a 1.5 - t whole - body mr systetwo independent readers tried to categorized the suspected vascular anomalies in pre - contrast and post - contrast mr sequences and assessed the overall tricks image quality . 
in 11 patients , the diagnostic performance comparability between tricks sequence and digital subtraction angiography was evaluated . results on the basis of time - resolved imaging of contrast kinetics , 31 of the vascular anomalies were classified as high - flow vascular malformations , 29 as low - flow vascular lesions and 6 as hemangiomas . 
the vascular anomalies characteristics provided by moderate , good or excellent quality tricks images were confirmed by digital subtraction angiography . conclusion time - resolved imaging of contrast kinetics sequence let the radiologist to acquire useful temporal information to correctly evaluate vascular anomalies components , adding more data to those provided by conventional mr sequences , especially in case of arteriovenous malformation . 
forty percent of them are located in the head and neck , 40% in the extremities , and 20% in the trunk [ 5 ]  . every part of the body could be affected , and many lesions affect the head , neck and extremities , so psychological morbidity caused by disfigurement is an important problethey could appear as red , blue or skin color lesions that modify the normal anatomic profiles . 
 high - flow vascular malformations could also cause a palpable bruit or thrill and high - output cardiac failure . there are many different types of vascular anomalies and during the last decades there has been a progressive improvement in their classification . 
the last issva classification was published in 2014 , in which vascular malformations are subdivided into simple and combined , and a section on the association with other anomalies and syndromes has been introduced , among others . 
capillary ( cms ) , lymphatic ( lms ) , and venous malformations ( vms ) or mixed lesions are classified as low - flow malformations , whereas any malformation with an arteriovenous shunt without an intervening capillary bed is classified as a high - flow malformation , including arteriovenous malformations ( avms ) , arteriovenous fistulas ( avfs ) and combined vascular lesions such as capillaryarteriovenous malformations ( cavms ) or capillarylymphaticarteriovenous malformations ( clavms ) [ 6 ]  . dermatologic findings are often the first clinical manifestation of vascular anomalies , but it is frequently not possible to distinguish with certainty between the various subcategories only on the basis of physical examination and clinical history . high - frequency grey - scale and doppler us is the first imaging modality to be considered [ 7 ] , displaying a turbulent multidirectional flow within the nidus , characteristic of avm , and enabling the distinction between macrocystic lymphatic malformations and venous malformations by flow signal detection within the lesion in the la radiologia medica ( 2018 ) 123 : 563571 latter [ 8 ]  . 
 digital subtraction angiography ( dsa ) it is still today the gold standard imaging modality for the hemodynamic evaluation of vascular anomalies , especially in the case of high - flow vascular malformations . 
most of lowflow vascular anomalies and haemangiomas are isointense or hypointense with respect to muscle on t1 - weighted and hyperintense on t2 - weighted or short tau inversion recovery ( stir ) images . 
the latter cannot be easily detected with unenhanced mr imaging ; however , an abnormal proximity and contact between arterial and venous vessels as well as flow - voids , ectasia and tortuosity identified in the surrounding veins could raise the suspect of this vascular pathology . 
macrocystic lymphatic malformations ( lms ) present as septated masses with ring enhancement within cyst walls ; microcystic lms dont have clearly recognizable cystic spaces and do not show significant enhancement [ 10 ]  . 
avms and avfs show early enhancement of the drainage veins ; a nidus could be identified in avhemangiomas present as welldefined , noninfiltrating lesions with fast - flow vessels at the periphery of the mass [ 7 , 9 ] and strong enhancement after contrast administration . 
mr - angiography ( mra ) is the preferred imaging modality for vascular anomalies evaluation and should be considered as a fundamental diagnostic tool when there are equivocal findings at us . 
unfortunately , the temporal resolution of conventional mra does not enable a satisfactory 1 3 la radiologia medica ( 2018 ) 123 : 563571 assessment of high - flow vascular malformations , making it difficult to identify with certainty a high - flow component within the lesion . 
only the high temporal resolution of 3d time - resolved mra allow the correct evaluation of the feeding arteries , the nidus and the drainage veins , enabling the characterization of a avm or a av fistula . 
nowadays , technological progress allows patients with vascular anomalies to undergo only noninvasive vascular imaging without radiation exposure for treatment planning purpose . the objective of this study is to evaluate image quality , inter - observer diagnostic variability and the added value of 3d time - resolved mra to reach the right diagnosis in peripheral vascular anomalies compared to unenhanced and conventional enhanced mri . subjects andmethods patient population a prospective study was performed in 95 patients who were clinically suspected of having a peripheral vascular anomaly ( upper or lower extremities ) after a dermatological examination , a us scan or , in some cases , after the evaluation of a previous unenhanced mr study . 
patients whose vascular anomaly had already been diagnosed or treated were excluded ( 21 patients ) , as well as those who undergone mri in a scanner different from the ge one described below ( 5 patients )  . 
the study population consisted , therefore , of 66 patients ( mean age 26 , range 0.575 ) who underwent a tricks - mra study between january 2004 and december 2016 . 
some patients ( 7 ) had done a previous unenhanced mr study in other institutions , usually undergone to exclude orthopedic disorders , and they required a more detailed mra study . 
dsa was performed in 11 patients 115months after mra , because endovascular treatment was considered . the study was approved by the institutional review board and ethics committee of our institution . 
after , 1 3 566 la radiologia medica ( 2018 ) 123 : 563571 using tricks - mra sequence , they independently randomly classified vascular anomalies and graded the overall image quality and the ability of this sequence to show the vascular anomaly components ( feeding arteries , av fistula , nidus , drainage veins , vm , lm cysts walls or haemangioma ) using a five - point scale scores ( 5 , excellent ; 4 , good ; 3 , moderate or satisfactory ; 2 , poor ; 1 , non - diagnostic ) ( table1 )  . 
in eleven patients who underwent dsa , dsa images , considered as the standard of reference , were reviewed by an experienced interventional radiologist ( with 10years of experience in interventional radiology ) , who was unaware of the tr - mra findings , and the dsa diagnosis was compared with that made using tr - mra to assess the two modalities comparability . statistical analysis interobserver agreement for the image quality grading , as well as the diagnosis of avm were assessed by kappa - statistics ( k < 0 less than chance agreement , 0.010.20 slight agreement , 0.210.40 fair agreement , 0.410.60 moderate agreement , 0.610.80 substantial agreement , 0.810.99 almost perfect agreement , k = 1 perfect agreement )  . results image assessment the two radiologist independently tried to classify the suspected vascular anomalies on pre - contrast images , and they both affirmed 6 patients seem to have lm ( 1 in pediatric and 5 in adult patients ) and a patient with a very enlarged venous vessel with flow - void seemed to have a avf ( table2 )  . after the independent and random evaluation of postcontrast lava sequence the two classification were identical and they classify one adult patient as avf , 6 as lm ( 1 in pediatric and 5 in adult patients ) , 14 as suspected vm ( 6 in pediatric and 8 in adult population ) , 6 as hemangiomas ( 5 in pediatric patients and 1 adult ) and 39 lesion as suspected vascular anomalies not otherwise specified ( 11 pediatric ; 28 adult )  . the two independent vascular anomalies diagnosis after tr - mra images assessment were almost identical ( table3 )  . 
30 vascular anomalies were classified as highflow vascular malformations by reader 1 , and 31 by reader 2 ( 5 avfs , 1 in pediatric patients , 4 in adult ; 25 avms by reader 1 , 26 by reader 2 , 19 in adult patients and , in the pediatric subgroup , 6 by reader 1 and 7 by reader 2 )  . 
as regards interobserver agreement for image quality assessment , it was almost perfect for excellent ( k = 0.91 , both in pediatric and adult patients ) , good ( k = 0.93 , both in pediatric and adult patients ) and moderate scale scores ( k = 0.88 in pediatric patients ; k = 0.86 in adult patients )  . 
interobserver agreement for vascular anomaly subtype diagnosis on tr - mra was perfect for suspected avf diagnosis ( k = 1 ) and for suspected diagnosis of avm and vm in adult patients . 
the sensitivity of tr - mra to diagnose an avm was 100% and the positive predictive value was 100% for reader 1 and 91% for reader 2 . discussion conventional mr imaging provide useful information about vascular anomalies anatomic extension and relationship to surrounding structures . 
in the past , when tricks sequence was still not available in our medical institution , if a patient was clinically suspected of having a peripheral vascular anomaly , conventional mra sequence was used . 
nowadays , the 3d fat - suppressed t1 - weighted gre sequences ( vibe , siemens healthcare ; lava , ge healthcare ; thrive , philips healthcare ) allow short acquisition times with a high - spatial - resolution images of both the vascular system and the surrounding soft tissues , but they could not accurately demonstrate all the components of high - flow vascular malformations . 
currently , there are many innovative mra sequences [ e.g. , tricks ( ge healthcare , milwaukee , wis ) , 4dtrak ( philips healthcare , bothell , wash ) , twist ( siemens healthcare , malvern , pa ) , freeze frame ( toshiba medical systems , tustin , calif ) , and traq ( hitachi medical systems , twinsburg , ohio ) ] which spatial resolution has been improved by segmenting 3d k - space into a central region and one or more peripheral regions and by sampling the center of k - space more frequently than the periphery , which is updated only periodically [ 12 , 13 ] , resulting in high temporal resolution with appropriate spatial resolution for vascular imaging . 
therefore , to obtain a good hemodynamic evaluation of the lesions its necessary to take advantage of this high temporal resolution of 1 3 568 la radiologia medica ( 2018 ) 123 : 563571 fig . 
as a result tr - mra could be the reference imaging modality for pretreatment evaluation , and patients could undergo dsa only when an endovascular treatment is necessary , avoiding catheter angiography for diagnostic purpose . 
this article confirms the results of other similar studies in this field [ 14 , 15 ] , as the high comparability between dsa and tr - mra diagnosis , the 1 3 la radiologia medica ( 2018 ) 123 : 563571 high interobserver agreement about overall tr - mra image quality evaluation and tr - mra capability to reach a proper vascular anomaly diagnosis [ 1416 ]  . 
in our experience , the more frequent obstacles that prevented good or excellent image quality were small sudden movements during the early tr - mra acquisition phases , which occurred both in pediatric and adult patients . 
 tr - mra diagnostic failure of a reader in one case could be easily explained by the poor quality of that tr - mra examination , due to a sudden movement of the limb in a child . 
an useful information that can be drawn from the results of this study is that a radiologist with ten years experience in cardiovascular imaging can evaluate conventional mr and tr - mra vascular anomaly images almost as a radiologist with decades of experience . 
 the almost identical diagnosis reached by the two readers allows us to hypothesize that when a vascular anomaly mr diagnosis is possible , based on acquired sequences and adequate image quality , classify the anomaly rightly is definitely not an impossible goal . 
as a result , we can say that the diagnostic capacity of tr - mra is almost identical in both pediatric and adult patients for mri cardiovascular experts . our study has several limitations . 
 second , only 11 patients underwent the reference standard , dsa , at our medical institution , and this is mainly due to the use of tr - mra as a non - invasive first level and sometimes conclusive investigation , especially in the last decade . 
nevertheless , this is one of the few reports evaluating tr - mra in this field . compliance with ethical standards conflict of interest the authors declared no potential conflicts of interests associated with this study . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the purpose of this study was to identify and describe the prevalence of mandibular canal branching ( mcb ) using cone beam computer tomography ( cbct )  . methods seven hundred standardized cbcts were selected . 
pathologies found in the molar region were frequently connected with mcb ( 77.8% ) , and the most common pathology related to branches was periapical lesion . conclusions mandibular canal branching presented a high prevalence in cbct imagery , more frequently located in regions of the premolar and retromolar . 
an adequate diagnosis of the mcb is necessary to perform dental procedures and verify possible associated pathologies . keywords cone beam computed tomography mandibular canal mandible inferior alveolar nerve bifid mandibular canal * smila gonalves barra samilagbarra@gmail.com 1 school ofdentistry , federal university ofminas gerais , antonio carlos ave . , 6627 - pampulha , belohorizonte , mg31270 - 010 , brazil 2 school ofdentistry , federal university ofminas gerais , antonio carlos ave . , 6627 - pampulha , belohorizonte31270 - 010 , brazil 3 university ofalberta , 5 - 524 echa , 11405 - 87th ave , edmontont6g1c9 , canada 4 department ofcommunity andpreventive dentistry , school ofdentistry , federal university ofminas gerais , av . 
pampulha , belohorizonte , mg31.270 - 010 , brazil introduction the mandibular canal is an important anatomical structure to be considered in dentistry , and branching has been reported in the prior literature [ 13 ]  . 
it is necessary to understand its anatomy in order to avoid injuries of the alveolar inferior neurovascular bundle , such as peri - implant fibrous tissue formation , sensory disturbances , traumatic neuroma , or bleeding [ 410 ]  . 
studies have reported no difference in gender and age in the occurrence of mcb [ 6 , 12 , 13 ] , while others have found a higher prevalence of bifid canals in males [ 9 , 14 ]  . the location and prevalence of mcb is variable depending on the type of diagnostic method . 
 [ 18 ] have considered 2d imaging as having good diagnostic accuracy for detecting mcb , there was no diagnostic agreement between panoramic radiographs and computed tomography [ 9 , 19 ]  . 
other studies have demonstrated that 3d imaging is more adequate to detect mcb and analyze their characteristics , such as locations and direction , as well as whether they are unilateral or bilateral [ 3 , 4 , 7 , 10 , 20 ]  . 
it has been stated that the improvements provided by 3d imaging make it possible to find branches not yet identified [ 2 , 10 , 21 ]  . the large number of procedures performed in the posterior region of the mandible implies that the mandibular canal deserves attention from clinicians . 
the anatomical variations of the mandibular canal must be considered as an important anatomical structure in the surgical planning of the procedures , such as implant insertions , extractions of included teeth , biopsies , enucleations and curettage of pathologies , apical surgical interventions , harvesting of block bones , as well as anesthetic procedures [ 13 , 6 , 7 , 10 , 15 ]  . 
thus , considering the higher diagnostic accuracy of cbct in identifying and depicting mcb , the purpose of this study was to identify and describe the prevalence of this mandibular canal alteration in a canadian sample consisting of patients who received dental care at the university of alberta . materials andmethods ethics approval was obtained from the university of alberta for this study ( pro00050422 )  . 
as the main clinical reasoning for the examinations arose from orthodontic recommendations , the cbcts included had a large field of view and a voxel size of 0.3mm. cbct images were analyzed by creating panoramic views ( 5.2510.25mm thickness ) and multiplanar sectional slices ( 1mm thickness and 1mm spacing ) , using xoran software ( xoran technologies , ann arbor , usa )  . 
examinations that did not show the entire mandible or that presented artifacts derived from patients movements were excluded . assessments of images were performed by an oral and maxillofacial radiologist ( maac ) , a specialist with 10years experience , using a 20 led monitor with 1600 900 pixel resolution ( flatron e2442tc model , lg electronics , seoul , south korea )  . 
the kappa test revealed almost perfect agreement of the intraexaminer in the detection of mcb ( 0.842 ) [ 22 ]  . the variables analyzed were gender , occurrence of mcb located between the mandibular foramen and mental foramen , pattern of occurrence ( number of branches in each patient ) , region of mcb origin ( ramus , retromolar , molar , premolar , or mental foramen ) , the presence and localization of foramina at the end of the branches , location of the foramina , images of pathologies located between the mandibular foramen and mental foramen , connection between mcb and pathologies , kind of pathology connected to mcb , and the region of connection between mcb and pathology . 
 the variables were recorded on a spreadsheet . the number of branches was referred to the total number of branches that emerged from both sides of each patient : singleone branch , or multipletwo or more branches . 
the branches that emerged from the mental foramen region were considered to be mental foramen branches . when mcb emerges in its own foramen , which is not the mental foramen , the secondary foramen were called foramina . 
the kolmogorovsmirnov and chi - squared tests were used to verify the distribution of the sample , compare the sides of each patient , and evaluate associations of mcb with other variables . results after evaluating the database , 700 cbcts were included in the study ( 279 male and 421 female ; mean age = 20.97years ; median = 16years )  . 
3 single mandibular canal branching in retromolar region ( black arrows ) with foramina ( white arrow ) seventeen cases ( 8.72% ) were found to have multiple branches affecting the same side , including one case with three branches and another with five . 
there was a statistically significant difference ( p < 0.05 ) between mcb and pathologies in this region , which was not observed in the other regions ( table3 )  . twenty - five tomographic images of pathologies were connected to mcb . 
the secondmost frequent lesion was pericoronitis in seven cases . discussion mandibular canal branching has presented a prevalence ranging from 0.08% [ 17 ] to 65% [ 6 ] , depending on the diagnostic tool used . 
thus , based on these findings , it can be concluded that the findings obtained by cbcts are reliable , since this method is able to improve detection and show the features of the mandibular canals and their variations , compared with 2d exams [ 3 , 4 , 7 , 10 ]  . the occurrence of mcb was not related to gender . 
 [ 15 ] , which found a statistical association with males , it is in accordance with the majority of studies that have also found no difference with respect to gender [ 3 , 6 , 12 , 13 ]  . regarding the affected sides , most of the mcb found were unilateral . 
hence , the larger number of females , when compared to males , with mcb is due to their higher proportion in the sample . regarding the cases with multiple branches affecting the same side of each patient , muinelo - lorenzo etal . 
the high number of unilateral mcb found in the present study does not permit the confirmation of a systemic effect from a prenatal factor and opens a new perspective about the influence of a local postnatal causal factor . a higher number of mcb has emerged from the mandibular canal in the premolar region . 
 [ 13 ] reported no premolar branches and found retromolar branches to be the most common mcb . the branches detected in the premolar region were frequently toward the lingual region and had a high prevalence of lingual foramina . 
since some anatomical studies have shown that this nerve has branches entering the mandible through the lingual surface , including the premolar region [ 2326 ] , premolar branches may represent an evidence of the supplementary innervation from the mylohyoid 1 3 606 la radiologia medica ( 2018 ) 123 : 601608 fig . 
5 sequence of cross sections showing a branch located in the right side of the mandibular body ( yellow arrowhead ) , which emerges in foramina located in the lingual cortical ( white arrow ) and returns to the mandible entering lingual foramina located in the retromolar region ( black arrow ) , merging again to the mandibular canal nerve , forming an anastomosis with the inferior alveolar neurovascular bundle , according to krasny etal . 
in this way , the occurrence of premolar mcb could help explain difficulties with anesthetic procedures [ 15 ]  . the most common tomographic image of pathology found overall was apical lesions . 
this happened in a pronounced way in the molar region , where most of the pathologies were in contact with mcb , and represents an additional reason for the suspicion of a local action of a postnatal causal factor . 
this physiological mechanism has already been proven and may possibly occur in maxillofacial structures [ 28 , 29 ]  . the large field of view and voxel size may have an effect on the identification of mcb , since these can vary in size . 
monoenergetic reconstructions were extrapolated at 64 , 69 , 88 , 105 , 110 , 120 , 140 , 170 , and 190 kilo - electron volts ( kev ) and the optimal energy was manually selected . 
nevertheless , because of the high number of pairwise comparisons , no differences were found in the post hoc analysis except for a trend toward statistical significance when comparing the 170 and 64kev doses . conclusions dect with specific post - processing may reduce metal artifacts and significantly enhance the image quality and diagnostic value when evaluating metallic implants . keywords hip metallic prostheses knee metallic prostheses dect artifact beam hardening photon beam * giammaria marziali giammaria.marziali@gmail.com institute ofradiology , catholic university school ofmedicine , fondazione policlinico universitario a . 
gemelli , rome , italy introduction in patients with joint prosthesis or other metallic orthopedic devices , it is important to accurately evaluate the boneprosthesis interface , the adjacent bone and soft tissues , and the device itself . 
radiologists are frequently asked to verify correct positioning of the prosthesis relative to the hip and to exclude device ruptures or fractures of the bone tissue and hematomas or inflammation / infection within the surrounding soft tissues [ 2 ]  . 
some of these techniques modify ct acquisition parameters , reducing pitch or increasing tube voltage or current ; while , others change the ct image visualization by using an extended ct scale , maximum intensity projection ( mip ) , or ct reconstruction parameters , or by increasing the slice thickness [ 69 ]  . 
dual - energy ct ( dect ) is a relatively new imaging tool that allows image acquisition at two different energy levels , with different vendors offering different techniques [ 10 ]  . 
dect enables the generation of images through monoenergetic extrapolations from two different energy spectra , resulting in higher metallic artifact reduction compared with filtered back projection [ 1113 ]  . 
monoenergetic reconstructions can also be time - consuming , since they must be reconstructed at the workstations after the acquisition of raw data and can slow down the workflow . however , syngo dual energy software ( siemens medical solutions , erlangen , germany ) has recently introduced an application called de - composition , which works on the same principles of monoenergetic reconstructions , using the raw data from both tubes , but with an additional noisereduction filter . 
the aim of this work was to assess the image quality and diagnostic value using dect to reduce metallic artifacts in subjects with knee and hip prostheses . materials andmethods this prospective , single - center study evaluating patients with painful prostheses was performed in agreement with the 1990 declaration of helsinki and subsequent amendments . 
patients provided written informed consent . patients from march 2015 to july 2016 , 31 patients ( 22 knee and 10 hip prostheses ) with pain were enrolled in this study . 
as that this is a perspective observational study , we included all the patients with painful hip and knee prostheses having a ct examination in our institution . ct data acquisition all exams were performed on a dual source ct ( somatom definition flash , siemens medical , forchheim , germany )  . 
the dect scans parameters were : slice acquisition , 2 32 0.6mm ; pitch , 0.5 ; rotation time , 0.5s and tube voltage , 100 for tube a and 140 kvp for tube b , respectively . 
the relationship between the tube currents was approximately 3 : 1 in favor of the high potential to produce as many high - energy photons as possible and still get a sufficient low - energy image for dual - energy image production [ 15 ]  . 
tube current modulation was activated to keep the dose at a minimum . ct image reconstruction ct images were reconstructed with a slice thickness of 1.5mm and an increment of 1mm , using a fixed field of view ( fov ) of 200 mm ( image matrix 512 512 ) , and a sharp convolution kernel ( d30 )  . 
post - processing of monoenergetic images was performed using commercially available software ( syngo , software va31 , monoenergetic application ) installed on a leonardo workstation ( siemens healthcare , forchheim , germany )  . 
some energy levels were chosen to match the mean energies of standard 120 kvp ( 64kev ) and 140 kvp ( 69kev ) spectra and a 140 kvp spectrum with an additional 0.1 - mm - thick tin filter ( 88kev )  . 
a 79 - year - old man with a painful knee prosthesis ; dect reconstructions of the knee prosthesis at 64 , 69 , 88 , 105 , 120 , 140 , 170 and 190 kev ; optimal kev ; b6 - 140kev and fast de . 
note the extensive metal artifacts secondary to beam hardening and photon starvation at 64kev and dramatic improvements at 190kev and opt kev levels were chosen on the basis of previous published works on metallic orthopedic devices [ 1517 ]  . 
 for the quantitative analysis , a circular region of interest ( roi ) was placed by a third radiologist ( with 3years of experience in musculoskeletal imaging ) , within the most evident streak artifacts on every image . 
 an ai formula was then used to quantify the severity of metal artifacts ( ai = sda sdb ) , where sda is the standard deviation in artifacts and sdb is the standard deviation in the reference region without artifacts [ 19 ]  . statistical analysis to describe quantitative and categorical variables , the mean standard deviation and frequencies or percentages were used . 
a 76 - year - old woman with a painful hip prosthesis ; dect reconstructions of the hip prosthesis at 64 , 69 , 88 , 105 , 120 , 140 , 170 and 190kev ; optimal kev ; b60140kev and fast de . 
to compare the image quality among the different monoenergetic images ( 64 , 69 , 88 , 105 , 120 , 140 , 170 , 190 , opt kev , b60140 and fast de ) , the mantelhaenszel 2 - test was carried out . 
pairwise comparisons of both qualitative and quantitative assessment scores ( 64 , 69 , 88 , 105 , 120 , 140 , 170 , 190 , b60140 , fast de , opt kev ) were made using bonferroni correction . 
the image quality scores were significantly ( p < 0.001 ) different between fast de and monoenergetic images at 64 , 69 , 88 , 105 , 120 , 140 , 170 and 190kev . 
there was also significant difference between fast de and opt kev ( p value < 0.001 ) , but not between fast de and b 60 - 140 . the number of ct artifacts was significantly different between monoenergetic images ( p = 0.004 between groups , table3 )  . 
nevertheless , because of the high number of pairwise comparisons , no differences were found in the post hoc analysis except for a trend toward statistical significance in the comparison between the 170 and 64kev monoenergetic doses . discussion for patients with metallic orthopedic implants , optimal visualization of bony structures and implants , as well as the interface between the implant and bone and the surrounding soft tissues , is key to rule out complications such as implant loosening or fractures . 
in recent years , dect with monoenergetic reconstructions has emerged as a novel imaging technique that is able to significantly reduce metallic artifacts with a dramatic improvement in image quality . 
 [ 13 ] accurately used a dect protocol on a standard hip phantom with a titanium and steel hip prosthesis ; then , they demonstrated effective reduction of metallic artifacts using monoenergetic reconstruction with a dual source scanner on a total of 22 adults with various metallic implants . 
4 the graph shows the percentages of the image quality as the percentages for the five points of the likert scale for all the monoenergetic doses following settings that were used in our study : slice acquisition 2 32 0.6mm ; pitch , 0.5 ; rotation time , 0.5s ; tube voltage : 100 kvp for tube a and 140 kvp for tube b with a tin filter applied to the tube b for better energy spectrum separation . 
 [ 14 ] similarly demonstrated a significant reduction in metallic artifacts of monoenergetic reconstructions ( 130kev ) in 47 patients treated with various implanted metal orthopedic devices ; however , using a slightly different dect protocol . 
 [ 12 ] evaluated the potential of mar in a phantom study with titanium and stainless steel plates using a single - source ct system at 80kev for titanium plates and 110kev for stainless steel plates [ 1 , 12 ]  . in our study , we demonstrated that the fast de , b60140 and the opt kev reconstructions had the best overall image quality . 
we also should point out that in our experience the fast de and b60140 techniques led to similar dect images , which were automatically reconstructed by the ct scan software . 
therefore , we demonstrated that the dect images are the best choice for optimizing artifacts and , at the same time , the workflow . there were several limitations to our study . 
also , the knee and hip prostheses were all the same type and were evaluated using a single kind of ct equipment . in conclusion , dect with specific post - processing could be a valid tool to reduce metal artifacts and may significantly enhance the image quality when evaluating metallic implants . 1 3 la radiologia medica ( 2018 ) 123 : 593600 1 3 600 la radiologia medica ( 2018 ) 123 : 593600 compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the acronym child ( childhood interstitial lung disease ) commonly defines these disorders , although air spaces , airways , alveolar epithelium , vasculature , pleura , and pleural spaces can also be involved , besides the pulmonary interstitiuchild can be caused by diffuse developmental disorders , alveolar growth abnormalities , surfactant dysfunction disorders , and other specific conditions of poorly understood etiology . 
the aim of this article is to review the ct patterns of lung involvement in a series of infants with child . keywords interstitial lung disease diffuse lung disease computed tomography infant introduction diffuse lung disease in infancy includes a wide range of very rare and peculiar pulmonary conditions with an incidence ranging from 0.13 / 100 , 000 [ 1 ] to 16 / 100 , 000 [ 2 , 3 ]  . these conditions may present with unexplained progressive respiratory distress in full term babies shortly after birth [ 4 ] or , later in life , in the first 2years of age with tachypnoea , hypoxia , failure to thrive , dry cough and wheezing in the absence of respiratory tract infection [ 5 ]  . 
more rarely , diffuse lung disease can be diagnosed in older children * claudio granata cgranata@sirm.org 1 department ofimaging , irccs bambino ges childrens hospital , rome , italy 2 pulmonary andallergy disease unit andcystic fibrosis center , department ofpediatrics , irccs istituto giannina gaslini , genoa , italy 3 paediatric pulmonology andsleep andlong term ventilation unit , irccs bambino ges childrens hospital , rome , italy 4 department ofpediatric radiology , irccs istituto giannina gaslini , genoa , italy presenting with unexplained exercise - induced breathlessness and digital clubbing [ 6 ]  . 
in the older age group diffuse lung diseases usually have much greater overlap with adult disorders [ 7 ] , whereas they are substantially different and peculiar in younger children [ 8 ]  . 
therefore , the american thoracic society ( ats ) introduced the acronym child ( childhood interstitial lung disease ) [ 9 ] and developed [ 4 ] a dedicated classification system of interstitial lung disease which subdivided them in two categories : disorders more prevalent in infancy , and disorders not specific to infancy . 
in full term newborns with respiratory failure of unknown origin , genetic testing for both disorder of surfactant metabolism and alveolar capillary dysplasia with pulmonary vein misalignment should be performed and precede a lung biopsy [ 7 ]  . as to chest imaging studies , in some conditions imaging findings can be specific , thus making it possible to avoid further testing . 
child disorders remain unrecognized on imaging studies , as they are very rare . chest x - ray is routinely performed as first imaging modality in children presenting with signs and symptoms suggesting interstitial lung disease . 
 hyperinflation is the most common finding , although findings can be initially normal . ct is certainly the best modality for evaluating the lungs , thanks to its capability to define precisely the involvement of interstitium , air spaces , or airways with better characterization of the various forms of child . 
a volumetric , thinsection high resolution scanning of the entire chest can be performed in few seconds with multidetector ct scanners , which makes it possible to avoid sedation in most cases . 
therefore , the aim of this article is to review the ct patterns of lung involvement in a series of patients with child . imaging technique in our institutions , ct studies were performed with two different scanners . the first one was a second - generation dual source ct system ( siemens somatom definition flash , siemens erlangen , germany ) , with two x - ray tubes and two detector systems settled at an angular offset of 95 . 
 sinogram - affirmed iterative reconstruction ( safire ) filter , strength of 1 , was employed . the second scanner was a single source somatom sensation 64 ( siemens medical solutions , erlangen , germany )  . 
ct axial ct ( a ) and coronal ( b ) images in an 8 - year - old girl show hyperinflation and hyperlucency due to alveolar simplification , mainly located in the upper lobes , middle lobe , and lingula with peripheral pulmonary vascular attenuation . 
the left lower lobe is hypoplastic ( white arrow ) with hypoplasia of the vein imaging findings diffuse developmental disorders acinar dysplasia , congenital alveolar dysplasia ( cad ) and alveolar capillary dysplasia with misalignment of pulmonary veins ( acd / mpv ) are included in this subgroup of child . acinar dysplasia is caused by growth arrest of the lung during the pseudoglandular stage of development at 616 gestational weeks , whereas cad results from growth arrest during the canalicular stage at 1626 gestational weeks [ 13 ]  . acd / mpv is characterized by muscular hypertrophy of the intralobular pulmonary arterioles , underdevelopment fig . 
coronal ct image in a 30 - month - old boy shows diffuse subpleural anteromedial cysts 23 mm in diameter in the upper lobes ( arrows ) 1 3 580 la radiologia medica ( 2018 ) 123 : 577585 of the pulmonary lobules associated with reduced capillary vascularisation , and misplacement of the pulmonary veins adjacent to the pulmonary arteries . 
 the outcome is unfavourable , with death occurring within 1month of presentation in almost 100% of cases . imaging findings are poorly known in this subgroup of patients , because of the rapid demise and of the rarity of these conditions . 
on chest radiographs , non - specific findings of diffuse hazy pulmonary opacification were reported in both lungs [ 10 ]  . alveolar growth abnormalities in this subgroup of child , the abnormal development of the lungs is a consequence of superimposed conditions or events . 
alveolar growth abnormalities ( aga ) includes pulmonary hypoplasia , chronic neonatal lung disease , and structural pulmonary changes related to chromosomal abnormalities or associated with congenital heart disease in chromosomally normal children . 
histological features include deficient alveolar development , with air space widening and simplification ( poor alveolar septation )  . pulmonary hypoplasia is most often secondary to intrauterine restriction of thoracic space , due to oligohydramnios , diaphragmatic hernia , or thoracic skeletal dysplasia ( fig.1 ) [ 17 ]  . chronic neonatal lung disease is typically represented by bronchopulmonary dysplasia , which represents the most common cause of child in infants . 
a further ct study performed 5years later c shows middle lobe and lingula largely replaced with cysts : some of these cysts may represent traction bronchiectasis 1 3 la radiologia medica ( 2018 ) 123 : 577585 the prolonged oxygen supply with mechanical ventilation in preterm newborns , which may lead to a varying degree of peribronchial fibrosis , obliterative bronchiolitis , and epithelial squamous metaplasia [ 18 ]  . 
imaging findings on chest x - ray show interstitial thickening , bands of atelectasis , and patchy or generalised hyperinflation of the lungs , whereas on chest ct areas of ground glass opacity , septal thickening and overinflated / simplified lobules can be observed . on chest ct , chromosomal disorders such as trisomy 21 appears with reduced alveolar number and surface in association with cysts along the lung periphery , fissures , and vascular bundles ( fig.2 ) [ 19 , 20 ]  . the main symptom in this subgroup of patients is respiratory distress , which may vary greatly according to causative conditions and associated anomalies . recently , impaired lung growth due to defective alveolarization has been linked to mutations of the filamin a ( flna ) x - linked gene [ 2124 ]  . 
axial ct images in a 7 - year - old girl ( ac ) show small cysts with subpleural and interlobular distribution ( black arrows ) , possibly representing traction bronchiectasis . 
axial ct image in a 14 - year - old girl d shows typical pulmonary alveolar proteinosis with a crazy - paving pattern 1 3 582 la radiologia medica ( 2018 ) 123 : 577585 fig . 
in these 1 3 la radiologia medica ( 2018 ) 123 : 577585 ct findings not known table 3 summary of the most frequently observed ct findings diffuse developmental disorders alveolar growth abnormalities pulmonary hypoplasia prematurity - related chronic lung disease chromosomal - anomaly - associated pulmonary structural changes trisomy 21 surfactant function disorders spftb , spftc , abca3 mutations lysinuric protein intolerance specific conditions of unknown or poorly understood etiology neuroendocrine cell hyperplasia of infancy ground - glass opacity , septal thickening , overinflated lung parenchyma subpleural cysts along lung periphery , fissures , and bronchovascular bundles diffuse ground - glass opacity , consolidations , septal thickening septal thickening , subpleural cysts , nodules , parenchymal bands hyperinflation , ground - glass opacity in the paramediastinal region , middle lobe , and lingula tered cysts pulmonary interstitial glycogenosis patchy or diffuse ground - glass opacity , interlobular septal thickening , scatpatients , diffuse or patchy ground - glass opacities and septal thickening with architectural distortion can be observed on chest ct [ 22 , 29 ]  . other rare genetic abnormalities , such as mutation of thyroid transcription factor 1 ( ttf1 ) [ 30 ] and lysinuric protein intolerance can cause surfactant dysfunction . 
in lysinuric protein intolerance septal thickening , subpleural cysts , and nodules followed by parenchymal bands at later stages can be observed ( fig.6 ) [ 10 , 31 ]  . surfactant dysfunction disorders can be diagnosed with genetic testing , making lung biopsy unnecessary in most cases . pulmonary interstitial glycogenosis ( pig ) is characterized by an increased number of glycogen - laden mesenchymal cells in the lobular interstitium [ 9 ]  . 
pig is often associated with disorders of alveolarization causing lung growth abnormality : in these patients , ct may show patchy areas of ground - glass opacity , interlobular septal thickening , and cystic changes [ 13 , 37 ]  . more rarely , pig is a primary disorder not associated with growth abnormalities : in such cases , the above ct findings appear diffuse within the lungs . 
steroid treatment is usually beneficial in patients with severe symptoms . specific conditions ofunknown orpoorly understood etiology conclusions in neuroendocrine cell hyperplasia of infancy , the neuroendocrine cells normally present in the alveolar epithelium are more numerous than normal . 
this is a relatively common interstitial lung disorder of infancy , which presents with persistent tachypnoea , retractions , and hypoxemia with air - trapping and restriction [ 32 ]  . 
 therefore , lung biopsy could be avoided in those patients with typical symptoms and characteristic ct findings [ 36 ]  . the outcome is generally favourable and self - limiting with supportive therapy addressing the hypoxemia [ 13 ]  . symptoms of child are non - specific and they are mainly represented by a varying degree of respiratory distress and hypoxaemia . 
the probability of reaching a diagnosis can be increased with a structured diagnostic approach . once child is suspected , chest ct should always be performed to confirm the presence of disease and to evaluate its extension [ 6 ]  . 
actually , ct scanning is rarely able to make a specific diagnosis among the conditions included in child group , because of the non - specific findings usually observed ( table3 ) [ 6 ]  . 1 3 584 la radiologia medica ( 2018 ) 123 : 577585 genetic abnormalities are frequently present in child . 
 therefore , genetic testing should be carefully considered according to the clinical situation . if treatment has to be changed accordingly , lung biopsy should be considered in patients with no evidence of known genetic abnormalities and non - specific imaging findings . 
the aim of our study is to assess the incidence of pelvic lymph nodal relapse and outcome in prostate cancer patients receiving poi . materials and methods data from 207 consecutive patients were collected . 
 biochemical relapse - free survival ( brfs ) , pelvic nodal relapse - free survival ( pnrfs ) , distant metastasis - free survival ( dmfs ) , disease - specific survival ( dss ) and overall survival ( os ) were calculated ; analysis of prognostic variables was performed . results five - year brfs , pnrfs , dmfs , dss and os were , respectively , 90 , 98 , 96 , 97 and 91% . 
pelvic nodal relapse was not correlated to impaired outcome . conclusions lymph nodal pelvic relapse occurs in 2% of patients at 5years and does not correlate with impaired outcome , suggesting the lack of theoretical benefit of a prophylactic nodal irradiation . 
tumor biology and response to treatment are the main determinants of outcome . keywords prostate cancer definitive radiotherapy whole pelvic irradiation prostate - only irradiation introduction whole pelvic irradiation ( wpi ) in prostate cancer patients has been extensively investigated with the aim of preventing metastatic spread of cancer cells through lymphatic drainage , following data from surgical cohorts that reported improved biochemical relapse in patients undergoing prostatectomy with extended pelvic lymphadenectomy [ 14 ]  . 
evidences from non - randomized trials supported the use of 4050gy wpi followed by a radiation boost to * mauro loi mauro.loi82@gmail.com 1 radiation oncology unit , university offlorence , l.go brambilla 3 , florence , italy 2 radiotherapy department , erasmus mc hospital , groene hilledijk 301 , 3075earotterdam , thenetherlands the prostate in patients at high risk of locoregional relapse due to advanced local stage [ 5 , 6 ] or biological risk of nodal involvement 15% calculated by the roach formula : 2 / 3 ( initial psa ) + 10 ( score gleason 6 ) [ 7 ]  . 
wpi did not confer any survival advantage compared to prostateonly irradiation ( poi ) in a large series of 14 , 817 patients [ 10 ] and might result in additional toxicity despite use of modern techniques [ 11 ]  . 
three randomized trials ( rtog 7706 , rtog 9413 , getug 01 ) substantially failed to prove a superiority of wpi over poi in prostate cancer patients [ 1214 ]  . 
radiation therapy was delivered in daily fractions of 2gy , 5days per week , either by intensity - modulated radiotherapy ( imrt ) or by conformal 3d radiotherapy up to a median dose of 50gy ( 4060gy ) followed by an imrt boost . 
indication for androgen deprivation therapy ( adt ) was discussed at the multidisciplinary tumor board and offered to patients with known negative prognostic features , ( intermediatehigh damico risk stage ) before poi initiation and after the radiation course as adjuvant treatment . 
imaging was systematically performed in patients experiencing bf with contrastenhanced ct or 18f - choline - positron emission tomography ( pet ) to exclude presence of bone or visceral metastases . 
biochemical relapse - free survival ( brfs ) , pelvic nodal relapse - free survival ( pnrfs ) , distant metastasisfree survival ( dmfs ) , disease - specific survival ( dss ) and overall survival ( os ) were calculated from the last day of radiotherapy until the event occurrence or the last followup visit . 
this study has been authorized by the institutional review board . statistical analysis was carried out with spss statistical package version 21 ( ibm corp . ) to perform outcome analysis and asses the predictive value of patient ( tumor stage , gs , pretreatment psa , damico risk class , rni ) and treatment - related variables ( total dose , use of imrt , use and duration of adt )  . 
staging ct scan and pelvic mri were performed in 176 ( 86% ) and 134 ( 65% ) case , respectively ; 9 patients ( 4% ) underwent staging choline - pet at diagnosis . 
adt was administered to 131 ( 63.3% ) patients : in all cases it consisted of a neoadjuvant treatment prior to the radiation course and continued throughout and after radiotherapy for a median overall duration of 21 ( range 336 ) months . 
at the time of our analysis , 28 ( 14% ) patients were dead ; among them , 9 ( 4% ) died as a result of progressive metastatic disease . 
limited lymph nodal pelvic relapse was observed in four cases ( 2% ) : obturator , common iliac and internal iliac chain were involved in two , one and one case , respectively . 
 at univariate analysis , gs 7 ( p = 0.00003 ) , rni 15% ( p = 0.002 ) and intermediate / high damico risk category ( p = 0.043 ) were correlated with metastatic recurrence . 
no patient or treatment variable showed any influence on overall survival . discussion in this retrospective study we report the results of a single institution cohort of non - metastatic prostate cancer patients treated by definitive poi to analyze patterns of failure and their impact on outcome . 
the choice of this time window was motivated by the need to obtain adequate follow - up and , on the other hand , to select a consecutive series of patients homogeneously treated according to modern practice after integration in clinical management of appropriate stratification , dose escalation and availability of imrt , integration of adt and consistent criteria for definition of biochemical relapse . according to our experience pnr is an uncommon event , occurring in 2% of patients and accounting for 13% of cases of bf : this result is in line with historical data from surgically treated patients undergoing standard lymphadenectomy [ 17 ] , though lower than expected if compared to modern surgical series of operated , clinically 1 3 la radiologia medica ( 2018 ) 123 : 631637 fig . 
right : kaplanmeier plots for dss according to gs < 7 [ 2 ] versus 7 [ 1 ] node - negative prostate cancer that reports a rate of 630% occult nodal metastasis after prostatectomy plus extended lymphadenectomy [ 18 ]  . 
common sense might suggest that , if treatment failure can result from lymphatic dissemination , eradication of microscopic foci of disease by encompassing the lymphatic drainage in the treatment volume might improve efficacy and prevent further cancer cell scattering , at the expense of a complex and more toxic treatment [ 11 ]  . 
on the other hand , in patients who ultimately developed distant relapse , subclinical systemic disease might be already established at the time of the primary treatment ; hence these patients would not draw any benefit from nodal drainage irradiation . 
it should be also pointed out that until recent years , the detection of pnr would not have changed the medical management , consisting of watchful waiting until initiation of systemic treatment by adt . 
however , in the last decade , availability of metabolic imaging techniques favored in recent years the emergence of focal nodal stereotactic radiation therapy ( sbrt ) as a promising treatment option in patients with limited sites of recurrence . 
sbrt is an innovating modality of treatment that allows delivering ablative radiation dose with precise target definition : in a recent multi - institutional retrospective study , sbrt for oligometastatic prostate cancer relapse resulted in a 3 - year disease progression - free survival of 31% , comparable with results of salvage lymph node dissection [ 19 ]  . 
therefore , sbrt could be proposed to treat the isolated site ( s ) of recurrence , delaying or avoiding the use of adt [ 19 , 20 ]  . in our cohort the 5 - year brfs was 89% . 
previous reports confirmed the role of dose escalation in improving patient outcome [ 2226 ] , and in particular in patients with rni 15% the administration of a total dose of 77gy was a major predictor of response to treatment , resulting in a 74% 5 - year brfs [ 27 ]  . 
additional benefit from this association was though lost at the 7 - year analysis , suggesting that the combination only delayed progression in those patients who already carried a subclinical extraprostatic burden of disease [ 13 ]  . 
it is noteworthy that adt was administered in the majority of high - risk patients ( both according to damico classification and roach rni formula , in 78 and 89% of patients , respectively )  . 
it is on the other hand possible , since we did not observe any influence of risk category on outcome , that adt improves outcome by acting on determinants of risk groups other than gs that might influence the success of poi such as tumor stage ( i.e. , by 1 3 636 la radiologia medica ( 2018 ) 123 : 631637 downstaging disease when administered before rt , allowing for better target coverage )  . in our series , the main determinant of outcome was gs : data from historical series reported impaired outcome in patients with gs 7 even after adjustment for other known prognostic factors [ 28 , 29 ]  . 
secondarily , due to presumed enhanced radioresistance , further advancement in dose escalated protocols , altered fractionation schedules and combinational treatment could be advocated to improve radiation therapy efficacy [ 31 ]  . 
finally , as stated above , the possible role of adt in mitigating tumor burden , despite low tumor differentiation before primary treatment and its influence on long - term outcome should be taken into account when designing future experimental trials . the independent predictive impact of psa nadir in determining the risk of biochemical failure in patients treated by external - beam rt has been demonstrated by previous reports , proposing a threshold of 0.2ng / ml as a predictor of biochemical relapse - free survival [ 32 ]  . 
nevertheless interpretation of these values might be confounded by late onset of cytotoxic effects of rt over months , persistence of radio - resistant benign prostatic tissue and concomitant use of adt [ 34 ]  . 
therefore the use of a threshold of 0.08ng / ml should not be recommended . together , these data suggest that use of wpi in the whole high - risk population might not be worth the risk of overtreatment ; conversely , the emergence of sbrt and the improvement of metabolic imaging may shift the paradigm of treatment from a cautionary primary preventive attitude ( use of prophylactic wpi in the majority of high - risk patients ) to a secondary prevention based on early detection of oligorecurrent site of disease and locoregional treatment by sbrt . 
in summary , due to uncertainty in the identification of patients drawing a clear benefit from wpi and the emergence of novel locoregional modalities of treatment for oligorecurrent disease such as sbrt , the use of prophylactic wpi should be limited to selected cases . there are several limitations in our retrospective study . 
 despite a long 71months follow - up and a consistent clinical management , the study population is a small cohort from a single institution , resulting in a limited number of events that may affect the reliability of our results . 
the duration of androgen deprivation in patients with known negative prognostic features ( in particular , intermediatehigh damico risk stage ) was influenced by a certain number of confounders ( tolerance to treatment , patients compliance , institutional practices before availability of consensus statements ) and is probably a source of moderate bias , as expected in a retrospective study where no relative dose intensity can be prespecified . 
due to retrospective design , missing information on pretreatment variables such as percentage of positive cores at diagnosis did not allow the use of more updated lni - risk calculators as compared to the roach formula : future trials based on more accurate pretreatment classification of patients through novel nomograms should be encouraged to define a clear subset of patients that could definitely benefit from wpi [ 35 ]  . conclusions pelvic lymph nodal relapse was found in 2% of patients at 5years and was not significantly correlated with distant metastatic dissemination or impaired outcome . 
the linear no - threshold hypothesis dates back to 70years and has not been scientifically validated , yet it remains the driving force behind current regulatory policies concerning radiation exposure . 
 in 2006 , the biological effects of ionizing radiation ( beir ) viicommittee , a committee of the united states nuclear regulatory commission ( usnrc ) , published a report based on the 19581999 lss data for acute exposure to low doses of radiation . 
revealed the reason for this support of the lnth hypothesis as being related to the abundance of financial support from government entities and the numerous government and private - industry jobs that depend on the acceptance of the lnth . 
the authors thereafter mentioned the findings of the 2005 french academy of sciences report reaching a contrasting conclusion , which proves a lack of evidence supporting any harm below 100mgy and findings of adaptive responses for that range [ 4 ]  . 
it urges making every effort to maintain infrared exposures as far below dose limits as possible , which translates to lowering doses in nuclear medicine images , computed tomography ( ct ) , and x - ray studies . 
not only does the lowered dosage affect the quality of the image used for diagnosis , but this policy reinforces a phobia of radiation for authorized physician users , technologists , and patients [ 3 ]  . 
this fear of ionizing radiation affects the diagnosing and , therefore , the proper treatment of patients , and many patients decline any exposure to radiation and treatment , sometimes resulting in premature death . 
evaluation of the evidence presented by the author deems the lnth a non - sequitur and advocates rational thoughts and benefits of medical imaging . lower radiation doses have the potential to improve cancer therapy results in a subset of patients who are candidates for tumor irradiation . 
it should be noted that this benefit and risk - oriented approach might raise concern in cancer patient management , where low - dose irradiation ( ldi ) , especially when repeated over various cycles , may not be as beneficial as image - guided radiotherapy ( igrt ) and periodic imaging in cancer survivors . 
igrt is valuable for sensitive healthy tissues ; however , tumors requiring direct visualization ( i.e. , palliative radiotherapy involving large fields and superficial tumors ) will least likely benefit from igrt , and instead require ldi [ 6 ]  . various factors must be taken into consideration , including the type and stage of the cancer , patient history , length of treatment , and organ mass . 
diagnostic imaging techniques should implement doses that can help diagnose and treat patients while not harming thebenefits and risks should be considered from various angles before a treatment plan is devised for patients to obtain successful health outcomes . author contributions ap and bv drafted and critically revised the letter . 
this is because the distention of the glenohumeral joint following intra - articular injection of the diluted mr contrast media allows for better delineation of the anatomy of the articular surfaces , especially the capsulolabral complex , cartilage , and capsule in younger patients [ 1 ]  . 
although it is feasible to use multiple techniques ( i.e. , fluoroscopyguided , ultrasound - guided , computed tomography - guided , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 620630 and mr - guided ) to administer mr contrast media into the shoulder , fluoroscopy - guided techniques are common . 
 recently , however , ultrasound - guided intra - articular injection has been increasingly used for mra [ 2 , 3 ]  . a three - dimensional ( 3d ) imaging sequence known as t1 high - resolution isotropic volume excitation mr ( thrive ) has recently been developed and is used not only in the abdomen and but also in musculoskeletal areas [ 48 ]  . 
 thrive , which uses t1 - weighted gradient sequence with a dual half - scan , improves fat suppression and enables fast dynamic scanning with submillimeter in - plane resolution , resulting in high contrast resolution [ 4 , 5 ]  . 
in addition , 3d mr imaging with isotropic resolution can be used to create multi - planar reformatted images , enabling the creation of similar sequences with different image planes and resulting in decreased scan time [ 6 , 7 ]  . 
3d isotropic mr can also minimize partial volume artifacts , as it uses thin slices that allow lesions to be analyzed without inter - slice gaps [ 8 ]  . 
we hypothesized that thrive images are more effective than two - dimensional three - plane ( axial , coronal , sagittal ) proton - density fat - suppressed ( 2d - pd - fs ) images in diagnosing superior labral anterior - to - posterior ( slap ) and bankart lesions . 
to the best of our knowledge , there have been no other reports comparing the usefulness of thrive images obtained during direct shoulder mra and 2d - pd - fs images for the evaluation of the capsulolabral complex and the articular surface of the glenohumeral joint . 
we thus compared the diagnostic performance of the thrive sequence with that of a standard protocol for direct shoulder mra for the detection of slap and bankart lesions , using arthroscopy findings as a reference standard . materials andmethods study population in an effort to improve imaging sequence quality in our institution , we used a modified shoulder direct mra imaging protocol , which includes the axial plane of a thrive sequence . 
our institutional review board approved the retrospective analysis of this data and waived informed consent for this analysis . at our institution , patients ( < 40years old ) younger than 40years of age are usually referred to our department for direct shoulder mra if they have symptoms of instability , a suspected slap , and a history of recurrent shoulder dislocation . 
the inclusion criteria for this study were ( 1 ) direct shoulder mra performed at our institution between january 2016 and july 2016 using a fluoroscopic - guided anterior approach , ( 2 ) the presence of both thrive and 2d - pd - fs images , ( 3 ) subsequent arthroscopy within 3months of the mra , and ( 4 ) availability of a detailed arthroscopic report . 
eight of the 92 patients were excluded from this study because they had either undergone shoulder surgery before the direct shoulder mra ( n = 5 ) , undergone repeated direct shoulder mra of the same shoulder for follow - up ( n = 2 ) , or undergone direct shoulder mra due to the presence of intra - articular tumors ( synovial osteochondromatosis , n = 1 )  . 
 a 22 - gauge , 3.5 - inch - long spinal needle was used to target the middle to inferior portion of the anterior glenohumeral joint space , and approximately 1 ml of the iodinated contrast agent iopromide ( ultravist 370 ; bayer schering pharma ; berlin , germany ) was injected to confirm position of the intra - articular needle . 
ten milliliters of this solution were mixed with 5ml of iodinated contrast agent ( omnipaque ( 300mg / ml ) ; nycomed ; princeton , nj , usa ) and 5ml of 1% lidocaine , resulting in a final gadolinium dilution of 1 : 250 ( 2mmol / l of gadolinium )  . 
the axial thrive images were additionally obtained using the following parameters : repetition time / echo time , 16 / 8ms ; flip angle , 10 ; matrix , 180 178 pixels ; field of view , 16cm ; slice thickness , 2mm ; inter - slice gap , 0mm ; echo train length , 1 ; number of acquisitions , 1 ; and scan time , 2min and 40s . 
this procedure took approximately 2min . image analysis quantitative image quality was evaluated by assessing the contrast - to - noise ratio ( cnr ) of the intra - articular ( glenohumeral joint ) signal . 
 signal intensity was assessed by measuring regions of interest ( rois ) in the joint space ( intra - articular fluid ) and adjacent muscle tissue ( deltoid muscle ) at each time point using both thrive and 2d - pd - fs axial images . 
signal intensity of the intra - articular fluid was measured in the axillary recess of the shoulder adjacent to the articular surface of the humeral head [ 9 ]  . 
to avoid volume artifacts , the joint space and deltoid muscle signal intensities and sd of the background air were measured three times , and the average values were used . 
the cnr of the intra - articular signal was calculated using the following equation [ 10 ] : cnrintraarticular signal = ( siintraarticular joint uid sideltoid muscle ) sdbackground air . to compare the qualitative image quality and diagnostic performance of the two sequences , 84 direct shoulder mra images were independently reviewed by two boardcertified radiologists with 6 and 9years of experience who were blind to patient history , arthroscopic findings , and final fig . 
axial proton - density fat - suppressed ( pd - fs ) ( a ) and t1 highresolution isotropic volume excitation ( thrive ) ( b ) images show homogenous fat saturation in the entire shoulder . 
to diagnose slap or bankart lesions , the reviewers evaluated the type of slap lesion ( type iiv ) [ 11 ] and the bankart lesion , checking for the presence of osseous fractures of the anterior inferior glenoid rim which indicates bony bankart lesions , while their absence indicates cartilaginous bankart lesions ( table2 ) [ 12 ]  . 
all mr diagnoses were compared the reports of a shoulder arthroscopy performed by an orthopedic shoulder surgeon , which served as a reference . statistical analysis all data were analyzed using medcalc ( version 12.3.0 ; mariakerke , belgium )  . 
there were three components to the statistical analysis : ( 1 ) comparison of image quality between the two mr sequences using a wilcoxon rank sum test , ( 2 ) comparison of diagnostic performance between the two mr sequences using delongs test [ 13 ] , and ( 3 ) the assessment of inter - observer agreement using an intraclass correlation coefficient ( icc ) with a 95% confidence interval ( ci )  . 
the mean interval between the direct shoulder mra and arthroscopy was 29.7days ( range 1759days )  . image assessment the total time required for the thrive scan was about 2min and 40s , while the total time required for the three sequences of 2d - pd - fs was about 8min and 40s . 
the median value for image sharpness was 1 ( interquartile range 0.4 ) for the thrive images and 2 ( interquartile range 0.6 ) for the 2d - pd - fs images . 
these findings suggest that using thrive may contribute to a higher correlation between direct shoulder mra and arthroscopic findings as well as a reduction in the discrepancies between radiological findings . we found that thrive images have meaningfully higher quantitative and qualitative image quality than 2d - pdfs images . 
axial ( a ) and coronal ( b ) proton - density fat - suppressed images show curvilinear high signal intensity ( arrows , a and b ) from the superior to anteroinferior labru both reviewers diagnosed the patient with a superior labral anterior - to - posterior ( slap ) type ii lesion . 
axial t1 highresolution isotropic volume excitation images show a tear ( open arrowheads , c and d ) and the disruption of the capsulolabral complex ( arrowhead , c )  . 
hh humeral head 1 3 628 la radiologia medica ( 2018 ) 123 : 620630 spectral attenuated inversion recovery fat suppression using sensitivity encoding ( sense ) [ 15 ]  . 
 thrive sequences also use dual half scanning , which is particularly appropriate for scans with large fields of view and relatively thick slices , as well as 3d scans with many slices . 
 in addition , there is the potential to reformat images in any plane including non - standard planes , such as those with double obliquity or curved planes , without compromising image resolution . 
together , this can help simplify imaging protocols and reduce acquisition time when multi - planar imaging is required . using 3d isotropic imaging of the shoulder , previous studies [ 16 28 ] have exhibited similar sensitivity and specificity values for detecting rotator cuff and labral tears relative to 2d conventional sequences , with shorter scan times . 
among these studies , four [ 19 , 2123 ] performed indirect ( intravenous contrast - enhanced ) shoulder mri , while the other studies [ 1618 , 20 , 2428 ] , including our own , performed direct ( intra - articular contrast - enhanced ) shoulder mra . 
importantly , no study has investigated and compared the diagnostic performance of 3d isotropic imaging and 2d conventional sequences in patients with or without various types of slap ( type iiv ) and bankart ( cartilaginous , osseous bankart ) lesions , though some studies evaluated solely slap lesion [ 17 , 18 ] , labral tear [ 2123 , 2528 ] , or labral defect [ 16 ]  . 
thus , our study is clinically meaningful for not only patients with suspected labral tear , but also those with shoulder dislocation [ 29 ]  . the ability to have shorter scanning times is especially important for direct shoulder mra , as the arthrography procedure is painful for most patients . 
 [ 32 ] demonstrated that the 3d shoulder mra with compressed sensing was feasible because it showed higher snr and cnr with similar diagnostic performance and shorter scan time ( 2min 22s ) compared to 3d shoulder mra without compressed sensing ( 3min 23s )  . 
by applying compressed sensing techniques , 3d thrive imaging may show higher image quality and diagnostic performance with a shorter scan time compared to routine 2d - pd - fs sequences . 
although in the present study we evaluated the thrive images on a workstation , as long as the purpose of the direct shoulder mra is to diagnose slap or bankart lesions , reconstructing the axial thrive images and transferring them to the pacs may be a substitute for the three sequences of the 2d - pd - fs imaging . 
according to our protocols , if we replace routine 2d - pd - fs with thrive sequences , we would decrease our scan time by 69% . we used the fluoroscopic guidance technique for intraarticular injection of the contrast media in the present study . 
accordingly , we have made the effort to change our shoulder mra technique from fluoroscopic to ultrasound guidance , which does not restrict one to a specific diagnostic procedure and thus can be applied to therapeutic procedures in the musculoskeletal system , such as joint injections of various drugs ( i.e. , steroids , lidocaine or hyaluronic acid ) [ 36 , 37 ]  . our study has several limitations . 
 second , although we evaluated overall subjective image noise and sharpness as qualitative image quality measures , our study lacked image quality analysis for each anatomical structure ( e.g. , labrum , ligament , cartilage )  . 
this is because in our institution , 1 3 la radiologia medica ( 2018 ) 123 : 620630 unenhanced shoulder mr imaging was performed for these conditions rather than invasive direct shoulder mra . 
if we reconstructed the images and used non - standard planes , such as those with double obliquity or curved planes , on 3d thrive images , the difference in diagnostic performance between 3d thrive and 2d - pd - fs might increase . 
the benefits of basing treatment decisions on thrive should be further assessed in future clinical studies by examining the imaging - pathology correlation . in conclusion , the thrive sequences on 3t direct shoulder mra have higher image quality , less motion artifacts , and similar diagnostic performance to 2d - pdfs imaging for slap and bankart lesions . 
 consequently , we believe that the use of thrive may be helpful for patients with slap and bankart lesions , and may be routinely obtained during direct shoulder 3t mra . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
patients were divided into two groups : transfemoral approach ( group a , n = 15 patients ) and transradial approach ( group b , n = 15 patients )  . 
after procedure , patients were questioned about the compliance using the questionnaire at 24h and vas rating at 6 , 12 , 18 and 24h . results the average of vas in group b was lower than in group a in each evaluation at 6h ( p < 0.20 ) , 12h ( p < 0.07 ) , 18h ( p < 0.02 ) and 24h ( p < 0.22 ) on the basis of mannwhitney u test , however , without a clear scientific evidence . 
on the basis of this background , our hypothesis is that tr approach can modify the compliance and pain feeling of patients undergone to uae . the aim of our study is then to verify vas and patient compliance in the immediate ( 24h ) post - procedural time , comparing patients undergoing uae through tr approach versus patients undergoing standard tf procedure . methods institutional review board ( irb ) approval was obtained . 
 between january and september 2017 , 30 consecutive patients were enrolled in two european centers with more than 10years experience of uae , one performing procedures through tf approach ( group a , n = 15 patients ) and the other through tr approach ( group b , n = 15 patients )  . 
the data of patients and treated fibroids are summarized in table1 ( group a ) and in table2 ( group b . ) the procedures were performed by two experienced interventional radiologists , one for each center . 
patients with absolute contraindications to any endovascular procedure ( inr 1.5 , platelet value < 50.000 , ecog stage 34 ) or patients unable to answer to vas have been considered unsuitable and excluded from the study . 
the analgesia protocol was as follows : ( a ) pre - procedure : 100mg ranitidine ; 10mg metoclopramide ; 30mg ketorolac ; ( b ) during the procedure : 2mg midazolam ; 150mg fentanyl ; 4mg morphine ; 1g paracetamol ; ( c ) post - procedure 12 / 24h : e.v. 
infusion ( 2ml / h ) ; morphine 2mg / h + physiological saline ; paracetamol 1g every 6h ; on the basis of the need , ketorolac was given , max 90mg / day . 
d - type wave and diameter less than 2mm were considered technical exclusion criteria for tr 1 3 la radiologia medica ( 2018 ) 123 : 885889 table 2 summary of patients population ( group b ) age of patient number type of fibroids fibroid size ( cm ) of fibroids treated access . 
a local anesthetic mixture of 100mcg nitroglycerine and 9ml of 1% lidocaine in a 10ml syringe was injected along the length of ra under palpation for length of needle at the wrist ( about 4cm )  . 
under us guidance by using a micropuncture set , a single - wall 21 - gauge needles puncture was achieved , and then a 4 - french sheath ( prelude ease , merit medical system inc , europe ) was inserted . 
 catheterization of both internal iliac artery and then of the descendent portion of uterine arteries was obtained by using a 4 - french , 125 - cm angled berenstein catheter ( merit medical system inc . , europe ) and a 2.8 - french , 150 - cm microcatheter ( direxion hi - flo , boston scientific corporation , europe )  . 
in case of radial spasm or in case of painful movement of the catheter , a solution of 100300mcg of nitroglycerine was injected through sheath ( repeated as much as two times )  . 
 sheath removal was performed after saline flushing ; then , a radial pressure - assisted compression device ( safeguard , merit medical system inc . , europe ) was inflated ( 7ml of air ) for about 30min , reducing 1ml every 5min . transfemoral access local anesthesia was obtained injecting 5ml of 3% lidocaine unilaterally or bilaterally in case of double access . 
 a 5 - french sheath was then inserted , and different types of diagnostic catheters were used to catheterize the internal iliac arteries ( sim 1 , cobra c2 )  . 
then , microcatheters were used to distal catheterization of the uterine arteries ( direxion hi - flo , boston scientific corporation , europe )  . embolisation after the catheterization of the descendent portion of the uterine arteries , microparticles were injected . 
we used two types of microparticles ranging in size between 500 and 900 micron ( embozene , boston scientific corporation , europe and embospheres , merit medical system inc , europe )  . 
in addition , patients undergone to tr access were asked to give their opinion on how much the possibility to bend the legs influenced pain relief as reported in table4 . 
a p value smaller that 0.05 was considered significant , and the difference between the two groups regarding vas and compliance questionnaire data was evaluated by using a statistical test ( mannwhitney u test )  . 
in group a , we treated unique fibroid in three patients ( 20% ) up to four in nine patients ( 60% ) and more than four in three patients ( 20% )  . 
regarding the questionnaire of table4 in group b , seven patients ( 46.6% ) strongly considered the impact of bending legs on pain relief , other seven considered it of some impact ( 46.6% ) , while only one patient ( 6.6% ) considered it indifferent . 
there were three self - limiting groin hematomas in tf group and one case of radial spasm in group b ; the latter was successfully treated with pharmacological protocol . another aspect that we analyzed is the cost - effectiveness between tr approach and femoral one : although the cost of the vascular introducer sheath catheters utilized for arterial puncture in tr approach is more expensive than tf approach , the earlier ambulation and recovery related to tr approach led to significant reductions in bed and total hospital costs . discussion several studies have compared the with tf versus tr access for coronary endovascular procedures , assessing the superiority of tr approach in terms of lower rates of vascular 1 3 la radiologia medica ( 2018 ) 123 : 885889 complications and mortality , with an earlier ambulation , recovery and improved patient satisfaction [ 2 , 7 , 8 ]  . 
 there was a strong patient preference for tr catheterization , and this is probably due to the fact that , as opposed to the tf approach , the former procedure allows patients to either freely bend their legs , or walk and sit because they are not obliged to absolute post - procedural bed rest . 
tr catheterization led also to significant reductions in bed , pharmacy and total hospital costs . recently , tr approach has been proposed for peripheral interventions including vascular procedures , chemoembolization and uae [ 3 , 9 , 10 ]  . 
in 2014 [ 3 ] ; the authors presented their experience on 29 consecutive patients with a technical success rate of 100% , with no immediate major or minor complications . 
 [ 11 ] reported a retrospective analysis on 1.531 consecutive tr access for noncoronary procedures , in particular with 116 cases of uae without major complications . pain management is very important in uae procedures , and particular attention is given to investigate new protocols to ensure patient comfort after the intervention . 
in our opinion , the importance of tr access is even more important in uae and it is also due to the possibility of bending legs ; the latter maneuver is considered to relief visceral abdominal pain as assessed by the carnetts sign , a recognized medical test [ 12 ]  . 
this is confirmed by the fact that in our study more than 90% of patients undergone to tr access consider the bending legs to have an impact on pain relief . our study has some limitations ; in particular , it is not randomized and the procedures are not done by the same operators ; furthermore , the patient compliance is assessed by a questionnaire built by an institutional consensus . 
between january 2012 and october 2016 , 108 consecutive oncologic patients ( 59 males , 49 females , mean age 52.6years ; 129 diagnosed lesions ) underwent multiphasic ct protocol including unenhanced ( ue ) , arterial ( ae ) , portal ( pe ) , 5 - min ( de - 5 ) and the 15 - min ( de - 15 ) delayed phases of adrenal glands . 
the best overall accuracy in diagnosing adenomas ( 97.6% ; 126 / 129 lesions correctly diagnosed ) was obtained using 40% threshold for calculating pwo from peak to de - 15 scan . conclusions if only an intermediate phase is available , the 15 - min delayed scan should be acquired to avoid any drop in diagnostic accuracy . 
delayed contrast material - enhanced wash - out parameters were proposed for separating benign lesions ( lipid - poor adenomas ) , usually presenting fast wash - out , from malignant ones ( mainly represented by metastases ) , vol . : ( 0123456789 ) 1 3 834 la radiologia medica ( 2018 ) 123 : 833840 frequently characterized by slow wash - out of contrast material [ 718 ]  . 
in order to easy ct schedule , recent studies proposed the possibility to maintain high diagnostic accuracy in distinguishing adenomas from nonadenomas using a 10 - min [ 8 ] and also a 5 - min delayed acquisition [ 16 , 19 , 20 , 23 ]  . 
 however , a retrospective study on a large cohort of patients concluded that the 10 - min delayed adrenal enhancement wash - out test has reduced sensitivity for the characterization of adrenal adenomas compared with results from prior studies [ 17 ]  . 
the possibility to increase the diagnostic accuracy of wash - out test using multiple intermediate scans ( namely arterial and portal enhanced scans ) was also recently proposed [ 20 ]  . 
with two intermediate scan available , a possible increase in absolute attenuation could be obtained , with subsequent increase of wash - out , independently from the time of acquisition for the delayed scan . 
calculating the wash - out from the peak enhancement phase could allow to reduce the protocol time , avoiding the need to wait for a further delayed scan . the primary aim of this paper is to calculate the diagnostic accuracy of wash - out parameters using multiple intermediate ( arterial and portal phases ) and multiple delayed ( 5and 15 - min delay ) acquisitions , secondarily to depict the best combination of intermediate and delayed scan for the calculation of wash - out parameters . materials andmethods patient population this prospective study had institutional review board approval and informed consent was obtained from all patients enrolled . 
inclusion criteria were : presence of 1 eligible adrenal mass ; multiphasic ct protocol including unenhanced scan of upper abdomen ( ue ) , followed by arterial phase ( ae ) of the chest ( with adrenal glands included in the field of view ) , portal enhanced ( pe ) phase of the abdomen , the 5 - min and the 15 - min delayed phases of adrenal glands . 
exclusion criteria were : incomplete ct protocol ( n = 5 ) ; final diagnosis of the adrenal mass not established ( n = 40 ) ; non - eligible adrenal mass ( n = 6 )  . 
 therefore , the study population consisted of 108 patients ( 59 males , 49 females , mean age 52.6years , range 3488 ) , presenting a total of 129 adrenal lesions ( 72 left , 57 right )  . 
 the final diagnosis was achieved by means of percutaneous biopsy ( n = 13 ) , surgery ( n = 17 ) , imaging follow - up of at least 1year ( range 1224months ; n = 99 )  . 
in case of lack of histological diagnosis , the absence of size change on follow - up ct determined the diagnosis of adenoma ( lipid - poor for ue attenuation > 10 hu and lipid - rich for ue attenuation 10 hu )  . 
1 flowchart showing inclusion and exclusion criteria and lesions classification 1 3 la radiologia medica ( 2018 ) 123 : 833840 and exclusion criteria and lesions included are described in fig.1. ct protocol all the examinations were performed with a commercially available ct scanner ( somatom sensation 64 , siemens medical solution , forchheim , germany ) with the following imaging parameters : fov 360 , slice thickness 1mm , 1 : 1 table pitch , 120kvp , variable tube current depending on patient size ( 150250mas )  . 
after the intravenous administration of 1.5ml / kg of iopromide ( ultravist 370 , bayer - schering , germany , 370mg of iodine / ml ) with a power injector , at a flow rate of 3ml / s , two intermediate enhanced scans were acquired for staging purposes with 35 - s delay ( ae ) , including chest and upper abdomen , and 80 - s delay ( pe ) including the whole abdomen . 
the wash - out is relatively fast , with more than 46% pwo at the time of the 5 - min delayed scan ( d ) , that is consistent with the diagnosis of adenoma . 
on the section with the largest surface area , a circular or ovoid region of interest ( roi ) was used to measure average ct attenuation values , including one - half to two - thirds of the area of the mass to reduce partial volume effects . 
wash - out parameters were also calculated for all lesions starting from peak attenuation ( considered as the highest attenuation achieved for each lesion with both ae and pe available ) to de - 5 and de - 15 , respectively . statistical analysis receiver operator curves ( roc ) analysis was performed for all the imaging parameters calculated : the thresholds yielding the best accuracy in differentiating adenomas from nonadenomas were retrospectively determined on the basis of roc curves . 
the corresponding sensitivity ( se ) , specificity la radiologia medica ( 2018 ) 123 : 833840 ( sp ) , positive predictive value ( ppv ) , negative predictive value ( npv ) and overall accuracy ( acc ) were calculated . 
all the 62 lipid - rich adenomas were correctly diagnosed as benign lesions on the basis of their ue attenuation < 10 hu . the peak enhancement phases in each subgroup of lesions are reported in table2 . 
the average difference of attenuation between ae and pe scan was 9 hu ( 11 hu for adenomas and 8 hu for nonadenomas , respectively )  . roc curves of each best wash - out parameters are reported in fig.3. 
the large majority of the 67 lesions with baseline attenuation > 10 hu were correctly characterized on the basis of absolute and relative wash - out parameters , as in previous reports . 
 [ 22 ] concluded that the quantitative evaluation of wash - out parameters at mri could not be used to characterize lipid - poor adrenal adenomas . in previous papers , the entity of intermediate attenuation and the time of intermediate scan adopted varied widely [ 616 ]  . 
 [ 10 ] , evaluating a triphasic ct protocol , ae phase attenuation of adenomas and nonadenomas was 86 hu and 67 hu , respectively , whereas attenuation was 89 hu and 71 hu during pe phase , respectively . 
according to our results , pe scan should be preferred to ae scan in case of a dedicated adrenal study for the subsequent calculation of wash - out parameters . our results are consistent with a previous study demonstrating a significant increase of wash - out parameters la radiologia medica ( 2018 ) 123 : 833840 calculated from the peak attenuation when compared to those calculated from ae or pe scans [ 20 ]  . 
a little increase in diagnostic accuracy was obtained by calculating wash - out from peak to de - 15 for all the imaging parameters ( pwo > awo > pew )  . 
two nonadenomas ( 1 metastasis from renal clear cell carcinoma and a 1 from melanoma ) showed a wash > 40% and were misdiagnosed as adenomas on the basis of wash - out curves ; however , the qualitative assessment ( hypervascular pattern at the time of ae scan ) and the other clinical and imaging findings ( presence of a hypervascular renal tumor ) may help in the differential diagnosing [ 23 , 24 ]  . 
even with a little drop in overall diagnostic accuracy , these results corroborated our hypothesis that pe phase represents the best single intermediate scan for the subsequent calculation of wash - out . 
for this reason , we believe that a 15 - min delayed scan should be obtained in case only ae phase available . the pwo parameter did better than pew parameter : a possible explanation is that the pew accuracy may decrease in case of low baseline attenuation . 
the mean radiation doses of the whole abdomen in our study ( 6.6msv ) were relatively low , being similar to that reported for the low dose scan of the abdomen in the study by gervaise etal . 
for this reason , the availability of multiple intermediate scan may allow the radiologists to shorter ct protocol , especially when sufficient wash - out can be demonstrated , reducing examination time and radiation exposure . this study has several limitations . 
individual matching for gender ( 53% female ) , age ( 53 19years ) , body height , weight , anteriorposterior and transverse diameters of chest and lung ruled out pre - test confounders . 
two - tailed t test and chi - square test were significant for p < 0.05. results measurable lymph nodes delineated equally in cases ( 261 / 372 iaslc zones , 70% ; 280 / 372 , 75% ) and controls ( 528 / 744 , 71% ; 519 / 744 , 70% ; no significant differences , power 90% )  . 
one observer delineated significantly more peripheral zone lymph nodes in cases ( 35 / 62 ) than in controls ( 43 / 124 ) ; there were no significant differences otherwise . 
common indications include the investigation of benign and primary or metastatic malignant disease of the lung parenchyma and mediastinum and cardiovascular disease , particularly pulmonary embolism [ 15 ]  . 
in turn , diagnostic radiation exposure is the leading contributor to non - natural radiation dose [ 6 ]  . improved ct technology , such as multi - detector row ct ( mdct ) , automatic exposure control ( aec ) , or iterative image reconstruction ( iir ) , increases dose efficiency , particularly in lung disease , due to the high intrinsic contrast between air and soft tissue [ 3 , 79 ]  . 
for general medical purposes within the same purview , standard - dose chest ct ( sdct ) ranges from 4 to 6msv ( formerly , 47msv ) , as elsewhere in the european union [ 1 , 2 , 4 , 1113 ]  . ldct provides diagnostic image quality , without significant loss of anatomic detail , in the lung and pleura [ 810 ] and in the thoracic skeleton [ 14 , 15 ]  . 
however , ldct also depicts thoracic soft tissue structures , including hilar and mediastinal lymph nodes that play a role in both benign and malignant lung disease [ 16 , 17 ]  . 
in principle , however , intravenous contrast enhancement ( ce ) , which is frequently used to improve delineation of thoracic lymph nodes at sdct , can also be applied at ldct for the same purpose [ 18 ]  . ldct examinations , as recommended for occupational medicine , have been offered in our institution in conjunction with ce upon special request by chest physicians . 
we hypothesized that there was no significant difference in the delineation of thoracic lymph nodes between ce - ldct and ce - sdct . materials andmethods data were organized and presented in this manuscript in accordance with the strobe statement [ 19 ]  . ethical considerations , study design , setting , andstudy population a prospective study design was dismissed and a retrospective casecontrol design favoured because ce - ldct examinations had previously been performed in our institution upon special request . 
based on the world medical association declaration of helsinki , the institutional ethics committee for human studies approved of our retrospective , monoinstitutional , matched casecontrol study of ce - ldct ( cases ) and ce - sdct ( controls ) examinations performed within a 20 - month time period ( fig.1 ) in the city - centre division for internal medicine of our department under stable scan conditions , and waived individual patient consent . 
 patients whose chest cts were retrospectively analysed were legally able to consent to the examination , had signed the respective forms , could follow breathing instructions , did not have contraindications for ce , were examined supine , in the arterial phase of ce , and had a body mass index ( bmi ) not exceeding 30kg / m2 . 
exclusion criteria were deviations from those inclusion criteria , previous radiotherapy of the mediastinum , severe motion artefacts per the original ct report , or incomplete or interrupted ct scan . 
based on institutional radiology files , two control patients of the same gender with ce - sdct during the study period were matched to each patient case , per body weight , body height , bmi , sagittal and lateral chest diameter , and sagittal and lateral lung diameter , such that there were 124 controls ( table1 ) , and a test power of 90% for all and 80% for each of six different thoracic lymph node zones was reached ( see study size section )  . variables lymph node delineation in each of six different thoracic lymph node zones was the primary variable of interest in this study . 
the outcome was either positive , if at least one lymph node in an individual lymph node zone delineated such that its long and short axis could be reproducibly measured with electronic callipers , or negative , if such delineation was impossible . 
secondary variables of interest included ct dose index ( ctdi ) and dose length product ( dlp ) , which were individually provided for each patient by the ct scanner as a mandatory requirement . 
besides matching criteria , short - axis diameter of the largest lymph node delineated in an individual lymph node zone was a potentially confounding variable whose outcome was either large , if short - axis diameter exceeded 1cm , or small otherwise . 
 two independent observers evaluated all ce - ldct and ce - sdct images to assess variability of perception as a potential effect modifier . data sources andmeasurements ce - ldct and ce - sdct images were retrieved from the institutional picture archiving and communication system ( pacs , syngo studio vb36c , siemens medical solutions , erlangen , germany ) and displayed in stack mode on a clinically certified 21 - inch 5k greyscale monitor . 
observer 2 was a cross - sectional imaging attending with more than 10years of post - fellowship clinical work experience in chest ct . six different lymph node zones were evaluated , based on the seventh edition of the international association for the study of lung cancer ( iaslc ) map , including the upper zone ( lymph node stations 2r , 2l , 3a , 3p , 4r , and 4l ) , aortopulmonary zone ( lymph node stations 5 and 6 ) , subcarinal zone ( lymph node station 7 ) , lower zone ( lymph node stations 8 and 9 ) , hilar / interlobar zone ( lymph node stations 10 and 11 ) , and peripheral zone ( lymph node stations 12 , 13 , and 14 ) , respectively [ 2123 ]  . 
the iaslc map was available to each independent observer [ 2123 ]  . previously , all patients underwent chest ct from the apex to the base of the lungs in supine position , arms above the head , on the same clinical whole - body 64 - detector row ct scanner ( optima 660 , ge healthcare europe , garching , germany )  . 
ce - ldct cases were examined at 100 kvp , with tube current ranges of 1040ma ( bmi up to 25kg / m2 ) or 1060ma ( bmi more than 25kg / m2 )  . 
twodimensional iir ( asir , ge healthcare europe , garching , germany ) was applied at levels of 70% for cases and 40% for controls , respectively , per institutional protocols . bias to clarify observer tasks prior to the study , the two observers jointly assessed three ce - sdct scans which had been screened for but excluded from the controls . 
to rule out potential effects of learning or memory , all ct scans in the study were anonymized jointly , by randomly assigning a five - digit number to each , put in sequence from the lowest to the highest random number , and grouped into six different packages , which were evaluated in individually randomized order by each observer . 
individual indications for chest ct were retrieved from the radiology information system and summarized for each of the celdct cases and ce - sdct controls as representing either non - neoplastic or neoplastic / presumably neoplastic disease . study size where n is the total sample size , p1 the expected delineation rate among cases , p2 the expected delineation rate among controls , q1 the proportion of cases , q2 the proportion of controls , p = q1 * p1 + q2 * p2 , za the standard normal deviate for alpha ( 1.96 for an alpha error of 0.05 ) , and zb the standard normal deviate for beta ( 1.284 for a test power of 90% ) , calculated sample size [ 24 ]  . the number of eligible ce - ldct cases was 62 ( 372 iaslc lymph node zones )  . 
for an expected delineation rate of p1 = 0.750 , p2 should be either 0.834 or higher ( n > 1093 ) or 0.655 or smaller ( n > 1103 ) to conclude that there was a significant difference [ 24 ]  . 
for an expected delineation rate of p1 = 0.750 , p2 should be either 0.909 or higher ( n > 184 ) or 0.541 or smaller ( n > 185 ) to conclude that there was a significant difference in an individual zone , while any other p2 would be insignificant , with zb = 0.840 ( power 80% ) [ 24 ]  . quantitative variables andstatistical methods dichotomous variables were recorded in two - by - two contingency tables , separately for the two independent observers , and subjected to two - tailed chi - square testing [ 25 ]  . 
averages standard deviation ( sd ) were calculated for quantitative measures of radiation exposure , including ctdi and dlp , and ed , as based on a conversion factor ( ek ) of 0.017 for adults [ 20 ]  . 
measures of radiation exposure and quantitative matching variables ( potential confounders ) were subjected to two - tailed students t test for unpaired data and uneven variance [ 27 ]  . 
there were no statistically significant differences between ce - ldct cases ( n = 62 , observer 1 , dark grey bars , observer 2 , light grey bars ) and matched ce - sdct controls ( n = 124 , observer 1 , light grey hatched bars , observer 2 , dark grey hatched bars ) after correction for multiple testing , except for peripheral ( pulmonary ) zone lymph node delineation in observer 2 1 3 la radiologia medica ( 2018 ) 123 : 818826 fig . 
observer 1 delineated lymph nodes in approximately 70% of all lymph node zones together in both ce - ldct cases and ce - sdct controls , with ranges between individual lymph node zones of 4090% in cases and 4398% in controls , and no significant differences ( table2 , figs.2 , 3 , 4 )  . 
observer 2 delineated lymph nodes in approximately 75% of all iaslc lymph node zones together in ce - ldct cases and 70% in ce - sdct controls , with ranges between individual lymph node zones of 5290% in cases and 3593% fig . 
when based on individual estimates of patient dose as provided by the ct scanner and documented in pacs as a mandatory requirement , average ed of ce - ldct was approximately 30% of average ed of ce - sdct per eur - 16262 - en calculation [ 20 ]  . 
first , it was monoinstitutional and limited to one specific 64 - detector row ct scanner , such that it remains unclear whether radiation dose could be similarly reduced ( or even further ) on other ct scanners . 
however , similar dose reduction options can be expected elsewhere , because the ct technology applied here is ubiquitously available and currently in widespread clinical use [ 1 , 7 , 8 ]  . 
it has been shown for pulmonary embolism ct protocols , though , that radiation doses are lower with 64 - detector row ct scanners than with less detector rows [ 28 ]  . 
fifth , the study exclusively analysed mediastinal , hilar , and pulmonary lymph nodes , while it left out others , such as supraand infra - clavicular , axillary , chest wall , retro - crural , or diaphragmatic lymph node stations . 
however , in clinical practice , lymph node size , particularly with a short - axis diameter exceeding 1cm , lymph node clustering , and uptake of contrast media into lymph nodes are criteria applied to detect potentially malignant lymphadenopathy [ 29 ]  . 
however , it has previously been shown that highly dose - saving ct protocols provide diagnostic image quality , 1 3 la radiologia medica ( 2018 ) 123 : 818826 without significant loss of anatomic detail , in the thoracic skeleton [ 14 , 15 ]  . 
tenth , due to inclusion criteria , inference from the study population to the general population is limited to patients with a bmi of 30kg / m2 or less . difficult task , secondary findings in this study imply that decreasing radiation dose as investigated here decreases neither thoracic lymph node delineation nor inter - observer agreement . interpretation conclusion within the limits of this study , the hypothesis that there was no significant difference in the delineation of thoracic lymph nodes per the iaslc map between ce - ldct , at an average of 30% of standard dose , and ce - sdct , should be accepted as true , with a test power of 90% , based on joint evaluation of six different lymph node zones , and with reproducible results between two independent observers [ 1 , 2 , 4 , 11 , 12 , 2123 ]  . 
it can be ruled out therefore neither that increasing radiation dose beyond ce - sdct would improve lymph node delineation , nor that decreasing radiation dose below ce - ldct would still yield acceptable lymph node delineation . 
in fact , a preliminary study in ten patients on sub - milli - sievert chest ct with different iir techniques reported promising delineation of mediastinal structures [ 31 ]  . 
small - scale studies imply that custom - made ce - ldct protocols might be suitable to follow - up patients with specific malignant diseases [ 32 , 33 ]  . 
in contrast to those studies , however , our study had a large sample size with high statistical power , included non - oncological patients , and applied chest ct protocols previously recommended by authorities [ 1 , 2 , 4 , 1012 ] , and the iaslc map as an established and generally accepted localization tool [ 21 ]  . further analyses revealed that although inter - observer agreement was high on lymph node delineation , agreement beyond chance was moderate in both ce - ldct cases and ce - sdct controls , unlike previously observed [ 18 ]  . 
this has previously been observed in delineation of lymph node compartments , gross target volume , and planning target volume in patients with non - smallcell lung cancer scheduled for radiotherapy [ 34 ]  . 
while it appears that delineation of thoracic targets represents a in conclusion , it appears that ce chest ct can be performed at much lower radiation exposure to the individual patient than currently accepted , with unchanged thoracic lymph node delineation . 
this implies that large - scale reduction in radiation dose is possible in routine clinical care , since lymph node delineation is crucial for both diagnosis and follow - up of different benign and malignant diseases . 
currently , inference to the general population is limited to dosereduced chest ct as recommended by governing bodies for occupational medicine , to the iaslc lymph node zones investigated here , and to patients with a bmi of 30kg / m2 or less . 
further studies should demonstrate whether investigation of other thoracic soft tissue structures will be limited by dose reduction and whether radiation dose can be reduced in patients with higher bmi . acknowledgements this manuscript includes results of doctoral thesis work in preparation by larissa marwitz at the faculty of medicine of the university of munich ( ludwig - maximilians - universitt , lmu ) , germany . 
reiser and jens ricke , directors of the department of radiology of the faculty of medicine of the university of munich ( ludwig - maximilians - universitt , lmu ) , germany . compliance with ethical standards conflict of interest all authors declare that there is no conflict of interest . ethical standards this was a retrospective study . 
ct allows excellent visualisation of typical bony vol . : ( 0123456789 ) 1 3 852 la radiologia medica ( 2018 ) 123 : 851859 landmarks to guide the procedure [ 8 , 9 ]  . 
these methods achieved optimal results but expose the patient to high radiation dose above all in cases of repeated interventional sessions [ 10 , 11 ]  . ultrasound ( us ) guidance could be considered as an option [ 1216 ] ; however , it is limited by poor visualisation of the target due to its deep location , frequent presence of bone spurs , and greater difficulty of interpretation by physicians who are not familiar with spine us anatomy [ 17 ]  . magnetic resonance ( mr ) imaging guidance has the advantage of guiding injection without radiation , but it has substantial limitations . 
mr guidance is troublesome and time - consuming , also requiring the use of expensive mr compatible needles [ 1820 ]  . in this tangled panorama , fusion - imaging technology has been proposed to enhance difficult clinical procedures [ 2123 ]  . 
fusion - imaging technology couples real - time us with the corresponding ct or mr image obtained from a previous diagnostic examination and reformatted in real time according to the ultrasound scanning plane [ 24 , 25 ]  . 
this allows combining the panoramic view and elevated anatomical detail of mr , or ct , with the ease of use of ultrasound without exposing the patient to additional ionising radiations [ 2629 ]  . the aims of the current study are : ( 1 ) to present our experience in procedures of fj injections ( fji ) performed with a newly developed multimodal echo - navigator ( masmec , modugno , italy ) which enables probe - oriented or needleoriented procedures ; ( 2 ) to evaluate short - term clinical outcomes of a consecutive series of patients affected by fjd treated with steroid and anaesthetic injection with this new device ; ( 3 ) to compare the obtained results with a cohort of patients affected by fjd treated with steroid and anaesthetic injection with ct - guided injection . materials andmethods patients this is a monocentric retrospective study based on prospectively collected data . 
two patients from control group were lost at final follow - up . clinical data are recorded and summarised in table2 . post - procedural patients satisfaction , rated as bad ( no change of complaints ; even worse ) , moderate ( fji helped me but i wont let this procedure again ) , good ( most of the complaints are relieved and i would again let this procedure if my complaints reappear ) , perfect ( fji satisfied me and fulfilled my expectations ) , was recorded at the end of followup in all patients . fusionimaging guided fji technique in the study group , we used a newly eco - nav multimodality navigation system ( masmec , modugno , italy ) , equipped with an electromagnetic ( em ) needle tracking system , in which a magnetic sensor is embedded in the needletip . 
the echo - navigator integrates the ultrasound machine with a low - intensity magnetic field generator docked by wire to the ultrasound machine . the previously acquired mr ( 12 ) or ct ( 16 ) dataset , which served as the imaging modality of reference , was loaded using standard dicom format on the us machine through cd - rom device or usb . 
 the radiation dose was 41 , 8 mgycm for each acquisition . the mr protocol used is a volumetric hybrid contrast enhancement sequence ( hyce ) , ( tr 10ms , te 5ms , st 0 , 4mm , fov 220 220 300mm , flip angle 70 , scan time 56 min ) , performed on an mri dedicated system ( s - scan , esaote biomedica , italy )  . 
 in this case , we could fuse any ct dataset ( better if images were reconstructed with 0 , 625mm effective slice thickness ) and any volumetric mri sequence with slice thickness thinner than 4mm . the imaging techniques were combined using image fusion technology ( econav ; masmec , modugno , italy )  . 
for correct superimposition of ultrasound and mr / ct images , the defined body landmarks were bony contours of spinous process of the second , third , fourth and fifth lumbar vertebra , posterior superior iliac spine , first sacral foramen , and the sacroiliac joint . 
during navigation , the distance between the tracking transmitter and the receiver did not have to not exceed 70cm , but this did not represent a limitation for lumbar joint injections . 
when the mr / ct scanning plane corresponded to the ultrasound scanning plane and the operator provides the confirmation input , the software connected the mr / ct image to the ultrasound picture , allowing a synchronous motion , consistent with movements and rotations of the probe , displaying both images on the screen . 
econav represented on the screen two images , respectively , on the left and on the right of the operative 1 3 854 la radiologia medica ( 2018 ) 123 : 851859 fig . 
on the left were reported the real - time images oncoming from the us scanner ( real - time window ) , in the right were reported pre - acquired images captured from us scanner or other sources like ct , mr , or mr / ct / us fused images ( virtual window )  . 
in the probeview mode , the virtual window reports 2d images that represent the cut planes passing through the us probe scanning direction ( b mode image and his orthogonal ) and the trajectory of the needle as dashed line that becomes full on the passing through zone of the b mode virtual planes . 
 the first ( a ) is the probe - oriented modality and second ( b ) the needle - oriented modality 1 3 la radiologia medica ( 2018 ) 123 : 851859 all study and control group fji were performed by the same musculoskeletal radiologist ( p.c. ) with more than 10years of experience in spine interventional procedures . statistical analysis continuous variables were reported as mean sd and compared using the independent student t test or mannwhitney u test . 
categorical variables were expressed as the number of cases or percentage and compared with chi - square test or fisher exact test . all demographic and clinical data were compared at baseline and at different time points . 
5 procedural time reduction during the learning curve comparing both groups , no statistically significant difference could be detected neither at baseline conditions nor during the follow - up period as reported in table2 . 
 [ 32 ] performed mr fusion - assisted ultrasound - guided injections 1 3 la radiologia medica ( 2018 ) 123 : 851859 on 38 patients ( 112 facet joints ) with accuracy in target achievement of 85.7%. 
however no comparisons with gold standard have been reported . in this setting , the first aim of our study was to present our experience in procedures of fj injections performed with a newly developed multimodal echo - navigator , compared with the results of a control group of patients that received ctguided fji . em tracking has been shown to improve targeting accuracy during interventional procedures . 
inside this volume , the accuracy of the tracker is 1.1mm ( root - mean - square error - rms within a 95% confidence interval ) as summarised in table3 . 
first of all , the presence of patient sensor localised on the skin near the target area allows to overcome the need of recalibration if a displacement of the generator occurs . 
furthermore , the presence of sensor embedded in the stylet tip allows to show the tip of the needle in the foreground and to choose the trajectory before inserting the needle . since econav does not require the use of ct or mri scans during the procedure , the daily diagnostic workflow is not impaired . 
this patient was affected by multilevel degenerative disc disease with instability . the third endpoint was to compare the obtained results with a cohort of patients affected by fjd treated with steroid and anaesthetic injection with ct - guided injection . 
we do not observe 1 3 858 la radiologia medica ( 2018 ) 123 : 851859 any statistically significant difference between fusion and guided cohort of patients and the ct - guided group in facet joint injection . 
the multimodal navigation system allows combining the panoramic view and elevated anatomical detail of mr , or ct with the ease of use of ultrasound without patient exposure to additional ionising radiations . 
 an example patient that receives a complete low - dose ctguided fji treatment ( two acquisitions for three injections ) will receive a global dose of ( ( 41.8 2 ) 3 ) = 250 , 8mgyc starting from comparable baseline conditions , no significant differences in clinical results between groups have been reported during the follow - up period . 
we reached a greater satisfaction rate in fusion - imaging group ( even if not statistically significant ) ; this could be partially explained by the fact that patients are aware of ionising radiation avoidance with this new device . although no statistical difference in fusion - guided and ct - guided procedure time was observed , we reported a significant time reduction for fusion procedures during the learning curve . 
this could be partially explained with the increased global expertise of operators but also with the improved automation of the fusion system currently in use . finally , although the number of obese patients treated with fusion guidance is limited ( three patient ) , the procedure was feasible in all patients and no outcome differences were observed . 
first of all , our trial was performed with different diagnostic mr or ct scans acquired in different hospitals and with different protocols , with patients lying in the supine position . 
 this choice introduces several biases but is able to recreate a practical clinical routine scenario , in which patients perform the examination for diagnostic purposes , with no expectation of any interventional procedure . 
the vertebrae of the lumbar spine will have slightly different position between supine and prone position but the real - time calibration corrections and the use of multiple bony landmarks at each vertebra before the introduction of the needle bypass the problem . although the satisfactory results , our findings should be confirmed by larger prospective studies aimed to demonstrate the non - inferiority of fusion - guided procedures compared to gold standard also for challenging locations around the spine . in conclusion , econav fusion - imaging guided system is a safe , feasible , effective and reproducible option in fjd infiltration procedures . 
multivariate analysis was conducted to identify association between clinical ( age , family or personal history of breast cancer , symptoms ) , diagnostic findings ( imaging modality , lesion size , final bi - rads category ) and final excision outcome . results eleven ( 7% ) of 153 b3a lesions were upgraded to malignancy . 
lesion size > 10mm ( or = 9.3832 ; 95% ; p = 0.0398 ) and bi - rads category 45 ( or = 12.6004 ; 95% ; p = 0.0006 ) were found to be independent predictors of upgrade to malignancy . conclusions b3a lesions are associated with low risk of malignancy at excision . 
lesion size > 10mm and bi - rads 45 category may represent useful predictors of upgrade to malignancy . keywords b3a lesions core biopsy excisional biopsy positive predictive value breast cancer introduction percutaneous imaging - guided needle core biopsy ( ncb ) and vacuum - assisted biopsy ( vab ) have become standard minimally invasive tool for the diagnosis of breast lesions . 
 the true benefit of ncb / vab in the clinical routine is the improvement of the preoperative diagnosis rate of screendetected breast cancers , thus reducing the number of surgical procedures for diagnostic purposes in breast cancer management [ 1 , 2 ]  . the b - coding system employed by the nhs breast cancer screening program classifies ncb / vab specimen into * iliana bednarova iliana.bednarova@gmail.com 1 department ofmedical area , institute ofdiagnostic radiology , university ofudine , azienda ospedalierouniversitaria , s . 
maria della misericordia , 33100udine , italy five categories as follows : b1 , normal tissue / non - diagnostic ; b2 , benign ; b3 , uncertain malignant potential ; b4 , suspicious for malignancy ; or b5 , malignant [ 3 ]  . 
 this category comprises a broad spectrum of lesions including atypical ductal hyperplasia ( adh ) , lobular neoplasia ( alh , lcis ) , flat epithelial atypia ( fea ) , radial scar / complex sclerosing lesions ( rs ) , papillary lesions ( pl ) and fibro - epithelial lesions ( fel )  . 
although the b3 category represents a relatively small proportion of all image - guided biopsies , in large series published so far , its prevalence ranges between 5 and 10% [ 4 , 5 ]  . 
several authors have suggested that certain subgroups of patients with b3 lesions at ncb / vab might avoid excisional biopsy ; however , currently there is no universal consensus on reliable clinical , histologic or radiologic criteria to identify these patients [ 10 ]  . the primary aims of our study were to determine the ppv for malignancy in cases of b3a lesions diagnosed at ultrasound - guided ncb or mammographic vab and to attempt to identify specific clinical characteristics and imaging features that might be predictors of upgrade to malignancy . 
the secondary objective was to identify the group of patients who might become candidates for follow - up ( fu ) rather than surgical excision ( se )  . materials andmethods this retrospective study was approved by the institutional review board with waiver of patient informed consent . study population from january 2010 to december 2016 , after a systematic review of pathologic results , a total of 339 patients with b3 diagnosis were identified on core biopsy . 
of these biopsies , 295 ( 87% ) were performed under ultrasound ( us ) guidance and 44 ( 13% ) were performed under stereotactic or digital breast tomosynthesis ( dbt ) guidance . 
 furthermore , b3a lesions were subclassified according to histopathologic parameters into papillary lesions ( pl ) , radial scars / complex sclerosing lesions ( rs ) and fibro - epithelial lesions ( fel )  . 
b3b lesions were subclassified into atypical ductal hyperplasia ( adh ) , lobular intraepithelial neoplasia ( ln / lin ) and flat epithelial atypia ( fea )  . the inclusion criteria for this study were , ( 1 ) b3a subcategory lesion at pathologic evaluation of biopsy specimens in the absence of any other associated high - risk lesion ( i.e. , atypical ductal hyperplasia or lobular neoplasia ) , dcis or invasive carcinoma ; ( 2 ) diagnostic surgical excision performed in our institution ( surgical removal is recommended for the management of all b3 lesions without atypia at our institution , independently of radiologic appearance and biopsy techniques ) [ 3 , 6 ] ; ( 3 ) pathologic analysis of percutaneous biopsy and surgical specimens performed at the department of pathology at our hospital ; ( 4 ) available radiologic images and clinical data from patients electronic records , including : demographic data such as age , family or prior personal history of breast cancer ( invasive carcinoma or dcis ) , data about clinical findings ( palpable nodule / nipple discharge ) , radiologic data regarding the reasons for biopsy such as ultrasound findings ( mass or nodule / architectural distortion ) and mammographic findings ( mass , microcalcification , architectural distortion )  . 
there were sixteen patients ( 10.7% ) who had a prior history of breast cancer and 29 patients ( 19.3% ) with first - degree family history of breast cancer . imaging andimageguided biopsy techniques of 149 patients , 121 ( 80.2% ) underwent mammographic ( mmg ) examination using dedicated full - field equipment ( digital device , giotto ims srl ) or dbt system ( selenia dimensions , hologic ) , acquired in two standard planes : mediolateral oblique and craniocaudal . 
whole - breast ultrasound ( us ) was performed in 145 ( 96.3% ) women using one of two different systems : ( 1 ) linear - array 517mhz transducer iu22 ( philips medical system ) or ( 2 ) linear - array fig . 
twentyfive of 149 patients ( 16.8% ) did not undergo mmg examination due to their young age , and 4 / 149 patients ( 2.7% ) had undergone the us examination in another hospital , which revealed no suspicious findings . 
all examinations and biopsy procedures were performed by one of four radiologists with experience of more than 10years in breast imaging and biopsy with us or stereotactic / dbt guidance . percutaneous biopsy procedures were performed using mammographic or ultrasound guidance according to the lesion type and judgment of the radiologist . 
us - guided procedures were performed using an automated biopsy gun ( magnum biopsy instrument , bard ) or a semi - automated biopsy gun ( precisa , hospital service spa ) with a 14 - gauge tru - cut , 15 - cm - long needle ( throw of the biopsy needle was 23mm )  . 
 according to our institutions protocol , amagnetic titanium clip was left to mark the site of biopsy in all cases in which the biopsy procedures were performed under mammography guidance and in cases of us - ncb in which the lesion size was < 5mm or when the lesion was seen with much difficulty after the biopsy procedure . image analysis to collect mmg and us variables , all images were reviewed retrospectively in consensus by two radiologists from breast imaging group ( 4 and more than 10years of experience in breast imaging , respectively ) who were blinded to the final histopathologic diagnosis . 
quadrantectomy was performed for 11 ( 7% ) lesions , which were upgraded to cancer at the excisional biopsy , and se was performed for 142 ( 93% ) lesions . finally , we reviewed the surgical pathology report of each lesion and classified it according to the highest - grade lesion in the following categories : malignant ( invasive carcinoma or dcis ) , high - risk b3 lesions without or with associated atypia ( pl , rs , fel , adh , ln ) , or benign ( proliferative changes without atypia , other benign lesions )  . 
the excision histology result was considered as the standard of reference . definition ofpositive predictive value formalignancy positive predictive value ( ppv ) for malignancy was defined when patients were found to have cancer ( invasive or dcis ) at final histology after se ( ppv = number of malignant cases / total number of lesions 100 )  . data analysis all eligible patients with b3a lesions were included in the statistical analysis . 
the outcome upgrade to malignancy of b3a lesions was correlated with selected clinical and radiologic predictors using the chi square or fishers exact test for categorical variables and t test for continuous variables . 
the level was set 0.05. 1 3 812 results final histology results of 153 b3a lesions diagnosed at us - guided ncb ( 134 / 153 , 87.6% ; 67 pl , 39 rs , 28 fel ) or mammographic vab ( 19 / 153 , 12.4% ; 7 pl and 12 rs ) , 11 / 153 lesions ( 6 pl , 5 rs ) were upgraded to non - invasive cancer ( dcis ) at surgical excision resulting in an overall ppv for malignancy of 7.2%. 
the ppv for 73 patients diagnosed with 74 pl was 8.1% ( 6 / 74 ) and showed no significant difference compared to that of 48 patients diagnosed with 51 rs ( 9.8% , 5 / 51 )  . 
 of the 125 / 153 ( 81.7% ) histologically confirmed high - risk lesions , 63 ( 50.4% ) were pl , 42 ( 33.6% ) were rs and 20 ( 16% ) were fel . 
seventeen ( 17 / 153 , 11.1% ) lesions were categorized as benign at final histology , and of these , la radiologia medica ( 2018 ) 123 : 809817 there were 5 ( 30% ) fibrocystic changes , 4 ( 23% ) sclerosing adenosis and 8 ( 47% ) fibroadenomas . association betweenclinical findings andfinal histology results the results of comparing clinical variables between patients with benign outcome and those with upgrade to malignancy are summarized in table3 . 
a , b digital breast tomosynthesis images in both cc and mlo view demonstrate architectural distortion with long , thin , radiating spicules in the upper outer quadrant of the left breast ( red circle )  . 
d subtracted axial t1 - weighted spoiled gradient - recalled echo ( spgr ) fat - suppressed image shows a pattern of an irregular , spiculated tumor - like mass ( red arrow )  . 
of 153 lesions , 20 ( 13.1% ) were detected by mmg only , 90 ( 58.8% ) were detected by us only and 43 ( 28.1% ) were detectable by both mmg and us . 
a gray - scale ultrasound image shows a solitary mural - based 9 5mm hypoechoic lesion ( long white arrow ) within dilated duct ( short white arrows ) in the para - areolar region . 
because of the heterogeneity of b3 lesions and their different risk of associated malignancy , two recent studies [ 8 , 9 ] emphasize the importance of further subclassification of b3 lesions according to the absence ( b3a ) or presence ( b3b ) of epithelial atypia as proposed by ibrahim [ 7 ]  . 
 [ 9 , 18 ] , also recommending the use of subcategorization into b3a and b3b , reporting a higher malignancy rate in b3b ( ppv : 23.3% ) compared to b3a ( ppv : 5.8% ) category and a higher rate of invasive carcinomas in b3b ( 70% ) versus b3a ( 10% ) category . 
on the basis of these results and recommendations , we have chosen to focus our study on b3a lesions ( including pl , rs and fel ) diagnosed at imaging - guided ncb / vab , in which final excision histology was available . 
the aim of our study was to evaluate if it would be possible to predict which b3a lesions are likely to be associated with malignancy , in order to select patients in whom imaging fu rather than se might be adopted . in the current study the overall ppv for malignancy among b3a lesions was 7% ( 11 / 153 ) , value that is consistent with the findings of the majority of previous studies [ 8 , 9 , 17 , 18 ]  . papillary lesions were the most frequently identified lesion in our b3a series , with a ppv for malignancy of 8% ( 6 / 74 ) after se . 
radial scars / complex sclerosing lesions represented 33.3% of our b3a cases series , where 9.8% ( 5 / 51 ) of these patients with rs were found to have a malignant lesion on se . 
studies in the literature report percentage of dcis or invasive carcinomas after a ncb diagnosis of rs ranging from 0 to 34% [ 20 ] , but the values decrease to 012% in case of rs without atypia [ 21 , 22 ]  . 
in our study , there were 28 cases of fibro - epithelial lesions and none of these was upgraded to malignancy at final excision histology . in our series , all eleven malignancies detected after b3a diagnosis were ductal carcinomas insitu and were all nonhigh grade ( 9 low - grade and 2 intermediate - grade dcis )  . 
as previously reported , it is well known that malignant lesions detected after a b3 ncb / vab diagnosis show favorable histologic features , compared with carcinomas after a b5 diagnosis [ 8 , 23 ]  . in most studies , neither clinical , nor imaging or biopsy features alone or in combination can correctly identify b3 lesions with less than 2% chance of carcinoma at se , which , according to the acr recommendations , can be managed with short - term fu . 
in agreement with previous studies [ 18 , 24 ] , our results showed that clinical findings ( palpable nodule or nipple discharge ) were not associated with malignancy on excision histology . 
this observation was supported by the results of hoffmann who did not find an association between mammographic features and subsequent diagnosis of cancer in excision biopsy [ 29 ]  . 
on contrary , in the study of rakha [ 8 ] , microcalcifications as the main 1 3 816 la radiologia medica ( 2018 ) 123 : 809817 radiologic abnormality were more likely to be associated with upgrade to malignancy compared to mass lesions or architectural distortions . 
in 16 ( 16 / 23 , 70% ) cases with b3a lesions , the microcalcifications were removed completely and partial removal was assessed in 7 ( 7 / 23 , 30% ) cases . 
 another limitation is that we used heterogeneous biopsy techniques : 19 ( 12.4% ) lesions were biopsied with a 911gauge vacuum - assisted device , and 134 ( 87.6% ) with a 14 - gauge automated or semi - automated needle biopsy . 
in addition , our b3a series included only three histologic subtypes and only lesions for which the final pathology of surgical specimen was available were included . in our study , we did not consider the role of contrastenhanced breast mri in the evaluation of high - risk lesions . 
 according to few previous studies [ 30 , 31 ] , which investigated the potential of this imaging technique in high - risk lesions , the negative predictive value of mri ( 9698% ) , might be very useful in identifying patients who could potentially avoid surgery , reducing associated costs and time as well as patient anxiety . 
consequently , today , the most common clinical practice is to perform se in the majority of b3 lesions , in order to rule out malignancy ( this can be achieved by examining the entire lesion histologically ) , which leads to unnecessary surgery in most cases . b3a lesions demonstrate a low ppv , which might reinforce the practice of obviating se in selected patients and further refines the current b3 subclassification with possible implications in clinical management [ 9 ]  . 
however , according to recent consensus recommendations [ 16 ] for most of the b3 lesions with low ppv for cancer ( pl , rs , fel ) , se could be avoided and therapeutic excision with vab might represent a sufficient alternative . nowadays , further data are becoming available in order to move toward more conservative approach , particularly in cases of b3 lesions without atypia , where management of these lesions with surgery may be potentially avoided . it is important to underline that every patient and each case should be discussed on a singular basis with a multidisciplinary team , taking into consideration patients demographic and clinical factors , imaging features , lesion size , possibility of non - surgical minimally invasive management as well as patient preference . 
in fact , we might assume that , when there is a low imaging suspicion for malignancy , when enough tissue has been sampled and there is no atypia found within the lesions , the surgery could be avoided and a very careful follow - up should be recommended instead [ 32 , 33 ]  . 
additional studies , looking at radiologic and morphological parameters , may be useful for a better assessment of malignant potential of different b3 entities , thus minimizing unneeded surgery in the majority of patients with a b3 diagnosis on ncb and a benign diagnosis on se [ 17 ]  . in conclusion , more comprehensive examination of b3 category lesions is mandatory in order to achieve acceptable balance between the risk of underestimation of b3 lesions with associated malignancy and overtreatment of benign b3 lesions . 
in contrast to strokes , seizure - related cerebral cortical lesions ( sccls ) usually show hyperperfusion , and therefore , cerebellar perfusion patterns are expected to be different from those of strokes . 
with arterial spin labelling ( asl ) , we evaluated the cerebellar perfusion status in patients with sccls . materials and methods using a search of the recent database over the last 31months , 26 patients were enrolled in this study . 
the inclusion criteria were as follows : ( 1 ) a history of seizures , ( 2 ) mr examination taken within 24h from the last seizure , ( 3 ) the presence of sccls on t2 / flair or dwi , ( 4 ) hyperperfusion in the corresponding areas of sccls on asl , and ( 5 ) no structural abnormality in the cerebelluthe perfusion status in the contralateral cerebellum was evaluated and categorized as hyper - , isoand hypoperfusion . 
because each cerebellum is connected with the contralateral cerebral hemisphere through the cortico - ponto - cerebellar ( cpc ) projecting fibres , a functional disruption of the cpc pathways is the underlying pathophysiologic mechanism of ccd [ 1 , 2 ]  . 
seizure - related cerebral cortical lesions ( sccls ) are characterized by hyperintensity on the t2 / flair image vol . : ( 0123456789 ) 1 3 844 la radiologia medica ( 2018 ) 123 : 843850 and restricted diffusion on dwi and can mimic acute ischaemic stroke in clinical and radiologic findings . 
therefore , cerebellar perfusion patterns are expected to be different from those of strokes . the arterial spin labelling ( asl ) technique is a noninvasive tool used to measure the cerebral blood flow ( cbf ) without administering a radiopharmaceutical or contrast agent and can be used repeatedly . 
compared to pet and spect , asl perfusion mr imaging has several advantages , including high availability , low cost , short scan time and lack of radiation hazard [ 710 ]  . there have been several reports that sccls show hyperperfusion on asl in patients with acute seizures [ 1113 ]  . 
the purpose of this study was to evaluate the cerebellar perfusion status in patients with acute seizures and sccls using asl perfusion mr imaging . materials andmethods patients this study was approved by our institutional review board . 
 informed consent was waived due to the retrospective nature of the study design . from a database search of our institution during the last 31months ( between august 2014 and march 2017 ) , twentysix patients were enrolled in this study . 
the inclusion criteria were as follows : ( 1 ) a history of seizures in the patients medical record , ( 2 ) an mr examination within 24h of the last seizure , ( 3 ) the presence of sccls on t2 / flair or dwi in the unilateral cerebral hemisphere or bilateral hemispheres with unilateral predominance , ( 4 ) hyperperfusion in the corresponding areas of sccls on asl and ( 5 ) no structural abnormalities in the cerebellum . an experienced neurologist reviewed all of the patient eeg data and clinical information , including any abnormalities in seizure - related data . mr imaging protocol mr examinations were performed using a 3.0 - tesla scanner ( ingenia ; philips healthcare , best , netherlands ) with a 32 - channel head coil . 
t2 - weighted and preand postcontrast t1 - weighted images were also acquired to assess the presence of structural alterations . image analysis all mr images were reviewed by two neuroradiologists with 3 and 25years of experience on a picture archiving and communication systefirst , we evaluated the location and extent of sccls on t2 / flair and dwi and evaluated perfusion abnormalities on asl without knowledge of the clinical information except for the presence of a current clinically and / or electrophysiologically confirmed seizure . second , a qualitative analysis ( visual assessment ) was performed to evaluate the cerebellar perfusion status on the asl rcbf colour map . 
each reviewer who was blinded to the presence and location of sccls independently assessed the perfusion status of each cerebellar hemisphere from the bottom to the top and classified these as symmetric ( isoperfusion ) or asymmetric perfusion . 
finally , the ccp was classified as hyper - , isoor hypoperfusion compared to the ipsilateral cerebelluin cases in which there was a discrepancy , two reviewers later reached a consensus . third , a quantitative analysis was also performed . 
the asymmetric index ( ai ) of cerebellar perfusion was calculated by measuring the rcbf in each cerebelluon a slice of an axial scan representing the greatest perfusion asymmetry , roi circles measuring 1530mm in diameter were manually drawn on the affected and mirrored cerebellar hemispheres ( fig.1 ) [ 14 , 15 ]  . 
the ai of cerebellar perfusion was calculated by using the following formula [ 15 , 16 ] : ai = 100 ( rcbfcontralateral rcbfipsilateral ) ( rcbfipsilateral ) positive and negative ai values indicate the relative hyperperfusion and hypoperfusion of the contralateral cerebellum , respectively . 
the calculated asymmetry index was a positive value statistical analysis to assess the interobserver agreement for ccp ( hypoperfusion , isoperfusion , hyperperfusion ) in the qualitative analysis , the kappa statistic was used [ 15 ]  . 
the differences in the ai values according to the ccp status were analysed by using the analysis of variance ( anova ) test . regarding the location of the sccls , the patients were divided into frontal - positive and frontal - negative groups according to the presence or absence of frontal lobe involvement . 
statistical analysis was performed to determine the difference in the frequency of cc hyperperfusion and ai values between the groups by using the fishers exact test and the mannwhitney u test . 
the significance level for the test was p < 0.05. 1 3 846 la radiologia medica ( 2018 ) 123 : 843850 1 3 la radiologia medica ( 2018 ) 123 : 843850 results the baseline characteristics of the patients and their results are provided in table1 . 
b on the adc map image , the lesions of the frontoparietal lobes reveal restricted diffusion ( arrows ) and the parietal lobe lesion reveals increased water diffusion ( arrow head ) , respectively . 
the interruption of cpc pathways causes a remote functional deactivation with reduced excitatory input and 1 3 la radiologia medica ( 2018 ) 123 : 843850 decreased cerebellar blood flow [ 1 , 2 ]  . 
this phenomenon is commonly observed on perfusion mr imaging , including asl as well as pet and spect , in stroke patients [ 14 , 16 , 17 , 20 , 21 ]  . 
in contrast to stroke , during seizure activity , ccd is believed to arise from excessive excitatory input along the cpc pathways , which produces a phenomenon similar to the deafferentation syndrome observed after stroke [ 3 ]  . 
the presence of cc hyperperfusion in seizure patients may be helpful for the lateralization of epileptic foci in clinical situations [ 22 ]  . in our patients , all the 7 cases of cc hypoperfusion were in the left cerebellar hemisphere with a consequent sccl in the right cerebral hemisphere . 
however , we could not find any differences in the cerebellar perfusion patterns according to whether the location of sccls was the right cerebral hemisphere or the left cerebral hemisphere . 
further studies with a large number of patients are needed . a seizure can mimic an acute stroke , and a stroke can also present with a seizure [ 26 ]  . 
nonetheless , an acute infarction showing focal hyperperfusion ( luxury perfusion ) or reperfusion with spontaneous recanalization of a clot on mr is challenging to differentiate from sccls [ 27 ]  . 
this finding is different from an acute stroke , which shows hypoperfusion or isoperfusion of the contralateral cerebellum rather than cc hyperperfusion . another advantage of this study is the use of the asl method , which does not require the administration of an exogenous tracer or contrast agent . 
the asl technique has been shown to be beneficial in many clinical trials , especially for paediatric patients , patients with impaired renal function or patients who need periodic follow - up perfusion studies . 
in addition , the ccp status on asl was determined with excellent interobserver agreement and was quantified using ai with excellent reproducibility . in our study , comparing the results of qualitative analysis ( visual assessment ) and quantitative analysis , the ai demonstrated general agreement with the ccp status of the visual assessment . 
considering the results of visual assessment and quantitative analysis , it seems that the cerebellar perfusion asymmetry can be visually distinguished when the ai value differs by 10 or more . the present study has several limitations . 
nonetheless , cc hyperperfusion was also observed in four patients ( 50% ) ( fig.3 ) , but the frequency was slightly lower than the average . second , because the number of subjects was relatively small , we did not find a statistically significant difference between the two groups according to the presence or absence of frontal lobe involvement . 
further studies with a larger number of patients will be needed . third , we could not determine the evolution of the cerebellar perfusion status because follow - up examinations were not performed in most cases . 
further studies with serial follow - up are needed . 1 3 850 la radiologia medica ( 2018 ) 123 : 843850 in conclusion , with asl perfusion mr imaging , we evaluated the cerebellar perfusion status in acute seizure patients with sccls . 
ih are usually not present at birth , become apparent at 24weeks of age , they follow a phase of rapid growth until 69months of age ( proliferative phase ) and then they spontaneously involute ( involutive phase ) until disappearing ( most often ) or leaving fibro - fatty remnants . very interestingly , in the methods section , the authors report that the age range of their patients is 489 with an average age of 34 . in this cohort , they found various features to what they define : arteriovenous / cavernous intramuscular and capillary hemangiomas . 
issva classifies vascular anomalies in two main branches : tumors and malformations ( issva classification of vascular anomalies 2014 international society for the study of vascular anomalies available at issva .org / class ifica tion )  . 
among tumors , there are infantile hemangioma and congenital hemangioma , the * giacomo colletti giacomo.colletti@gmail.com 1 maxillo facial surgery , san paolo hospital , university ofmilan , via a . 
then , there are vascular malformations that can be further sub - classified but that , for sake of simplicity , can be divided into capillary , lymphatic , venous and arteriovenous . 
thus , arteriovenous , venous and capillary are nosographies referring to vascular malformations and not hemangiomas [ 4 ]  . moreover , the literature agrees on the need to abandon the term cavernous hemangioma because it is wrong and misleading [ 1 ]  . in fact , all cavernous hemangiomas appeared to be venous malformations [ 5 ]  . also , many of the features that the authors describe in their paper are typical for vascular malformations : phleboliths and compressibility for instance , are typical of venous malformations . 
 the purpose of this study is to evaluate the need for iterative reconstruction software in ct - guided periradicular infiltration therapy with an ultra - low - dose protocol . materials and methods one hundred patients underwent ct - guided periradicular infiltration therapy of the lumbar spine using an ultra - low - dose protocol with adaptive iterative dose reduction 3d ( aidr 3d ) for image reconstruction . 
 while limiting acquisitions needed for planning purposes have shown to be effective [ 2 ] , reduction and modulation of tube voltage and tube currenttime product are options prior to image acquisition [ 3 ]  . 
additionally , software tools such as enhanced filtered back - projection and the more advanced iterative reconstruction algorithms aim at retaining image quality while dose id reduced [ 4 ]  . 
iterative reconstruction algorithms may iterate in the raw data , the image domain , vol . : ( 0123456789 ) 1 3 828 la radiologia medica ( 2018 ) 123 : 827832 or both , and numerous vendor - specific approaches exist . 
 one such algorithm is adaptive iterative dose reduction 3d ( aidr 3d , canon medical systems , otawara , japan ) , which was cleared by the fda in april 2012 [ 5 ] , and iterates in both the raw data and the image data domain ( reconstruction in three dimensions )  . 
aidr 3d significantly reduces image noise , while the slight improvement in spatial resolution claimed by the vendor still needs to be verified [ 6 , 7 ]  . several recent studies comparing the image quality and dose reduction potential of fbp and aidr 3d in different diagnostic ct applications [ 812 ] consistently report aidr 3d to significantly reduce the mean required overall dose by 3650% while maintaining or even improving image quality [ 1315 ]  . 
to the best of our knowledge , no research has been conducted so far investigating the potential of iterative reconstruction algorithms in the context of ct - guided interventions . this study aims at investigating whether the use of iterative reconstruction software is mandatory for implementing ultra - low - dose protocols with adequate image quality for ct - guided lumbar periradicular infiltration therapy . materials andmethods patients this study included 100 patients ( 58 females and 42 males , median age 62years ) undergoing single - site ( 52 right side , 48 left side ) periradicular infiltration therapy of the lumbar spine for pain relief . 
segments targeted were l1 / l2 ( 1 ) , l3 / l4 ( 12 ) , l4 / l5 ( 30 ) , and l5 / s1 ( 57 )  . inclusion criteria were patients aged 18 and over presenting with acute or chronic nerve root irritation and focal neurologic symptoms and a history of inadequate response to conservative measures including drug treatment . 
the study was approved by the institutional review board ( irb )  . intervention protocol interventions were performed on an 80 - slice ct scanner ( aquilion prime , canon medical systems , otawara , japan )  . 
the radiologist performing the intervention monitored stepwise needle advancement with acquisition of single - slice images staying next to the patient ( step - and - shoot technique )  . 
ct parameters were a tube voltage of 100kv , tube currenttime product of 5mas ( rotation time of 0.5s , 10ma ) , and a slice thickness of 8m before therapeutic injection of triamcinolone acetonide ( volon a , dermapharm ag , germany ) and bupivacaine hydrochloride ( carbostesin , astrazeneca , uk ) , a test injection of contrast medium ( imeron 300 , bracco , germany ) was performed . image evaluation for our retrospective analysis , images were independently evaluated by four experienced radiologists focusing on the conspicuity of the needle tip , visibility of the neuroforamen , and delineation of contrast medium distribution . 
additionally , image noise was quantified by measuring the standard deviation in a standardized region of interest ( roi ) of air in the field of view ( fov )  . three images per intervention and reconstruction type were analyzed . 
each of the three images was rated for needle and neuroforamen conspicuity and the third image additionally for contrast medium distribution , resulting in a total of seven ratings per patient and reconstruction type and a total of 1400 ratings for each reader . conspicuity was assessed using a numeric rating scale with scores from 1 ( poor ) to 4 ( excellent )  . 
the radiologists rated images in four sessions with 25 patients each . data analysis statistical analysis including generation of graphs was performed using r ( version 3.2.3 , r foundation for statistical computing , vienna , austria ) , a gnu project with copyright by the r foundation . 
as apparent from table1 , there was a significant difference in image noise between the average of the three images to be rated per patient with each of the two reconstruction algorithms investigated . taking the results for all features together , the four raters assigned 81.3% identical scores ( table2 ) , as also reflected in the bar charts presented in fig.1. 
these are the images depicting the needle close to the bony structures of the neuroforamen , which degrades its conspicuity compared with its visibility in subcutaneous fat or muscle tissue , where contrast is high . 
the overall average scores also indicate that both reconstruction algorithms , aidr 3d and fbp , provide sufficient image quality . the two algorithms have intrinsic features which might have influenced ratings . 
the standard aidr 3d level was chosen in order not to eliminate the needle tip artifact , 1 3 la radiologia medica ( 2018 ) 123 : 827832 which is desirable here to assess the needle position . 
conversely , the higher image noise of fbp reconstruction makes it more difficult to identify the needle tip artifact on these images . iterative reconstruction algorithms require powerful hardware to reconstruct images within a reasonable time . 
it should be part of future studies to evaluate the contribution of aidr 3d to ultra - low - dose ct protocols for interventions in low - contrast anatomy such as abdominal drainage . there is also use of ultrasound to perform spinal interventions which excellently visualizes soft tissue and avoids exposure to ionizing radiation [ 21 , 22 ]  . 
it should be considered as a rational alternative to ct guidance when no bony barriers as caused by degenerative changes are expected . conclusion in conclusion , ultra - low - dose protocols can be used for periradicular infiltration therapy on ct scanners even when no iterative reconstruction software is available . 
 fbp provides sufficient image quality with only slightly lower ratings than iterative reconstruction in our analysis . acknowledgements this research did not receive any specific grant from funding agencies in the public , commercial , or not - for - profit sectors . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
seventy - five percent of responders reported that , every year , visited < 50 gu patients ( pts ) , 18.1% visited 50100 pts and 6.9% visited > 100 pts . 
in case of tc , the prescription of rt was limited ( < 10 patients per year ) due to the low incidence of disease and recent shift to surveillance as a first option in stage i seminoma . conclusions our survey showed that radiation oncologists are rarely involved in the decision making strategy of gu cancer , despite many clinical trials support rt use . 
these patients probably deserve a more uniform approach based on updated , detailed and evidence - based recommendations . keywords genito - urinary cancer radiotherapy italian survey introduction genito - urinary ( gu ) malignancies include prostate , urinary bladder ( and urothelial cancers of urethra and upper gu tract ) , renal cell carcinoma , penis , and testicle cancers . 
sempreboni 5 , 37024negrar , verona , italy 2 radiation oncology department , azienda ospedaliera san camillo - forlanini , rome , italy 3 european institute ofoncology , university ofmilan , milan , italy 4 department ofradiation oncology , campus biomedico university , rome , italy 5 genito - urinary group ofairo italian association forradiation oncology , rome , italy 6 radiosurgery andradiotherapy department , istituto clinico humanitas cancer center andresearch hospital , rozzano , milan , italy 7 department ofradiation oncology , university andspedali civili hospital , brescia , italy 8 department ofradiation oncology , irccs san martino - ist national cancer research institute anduniversity , genoa , italy 9 university ofbrescia , brescia , italy vol . : ( 0123456789 ) 1 3 880 la radiologia medica ( 2018 ) 123 : 879884 urological cancers constitute 26% of all patients undergoing radiotherapy ( rt ) in the uk [ 4 ]  . 
these data are not available for italy ; however , similar incidence of urological tumors in italy and the uk makes suppose that the percentages are not different . bc includes two main categories : non - muscle - invasive and muscle - invasive bladder cancer . 
a nonsurgical option is represented by a strategy of bladder preservation that includes combination of transurethral resection of bladder tumor ( turbt ) , chemotherapy and radiotherapy ( rt ) [ 6 ]  . 
bladder preservation with trimodality therapy has been included as a standard option in the majority of guidelines , but this conservative approach is still rarely used in clinical practice in italy , whereas in some countries is largely practiced [ 79 ]  . renal cell carcinoma ( rcc ) accounts for about 3.8% of all new cancer , while testicular cancers are relatively uncommon and represent 1% of all male tumors [ 1 ]  . historically , rcc has been considered a radioresistant tumor and , for this reason , rt has been used mainly to treat metastatic sites with a palliative intent . however , in the past decade , evidence has grown that a high dose given in one or a few fractions by virtue of stereotactic ablative radiotherapy ( sabr ) can overcome resistance [ 10 ] in a safe and effective way . in addition , higher doses per fraction seem to induce microvascular damage , thus increasing the direct cytotoxic effect of rt [ 11 ]  . overall , these new applications of rt in primary and oligometastatic rcc remain under investigation because no randomized trials have so far been published , but they are increasingly adopted in the clinical arena . despite emerging data in the use of rt and the large number of patients treated for gu cancer , the role of radiation oncologist in the decision strategy remains to be fully exploited . the aim of the present survey is thus to investigate the actual attitude of the italian radiation oncologists in the management of these types of gu cancer ( excluding prostate , penile and other - than - bladder - urothelial cancer ) and their propensity to treat them with rt . materials andmethods in june 2017 , a survey including 16 items was sent to all italian radiation oncologists using the mailing list of airo . 
 the items of the questionnaire were defined over a multistep process by a panel of experts in gu working group of the italian association of radiation oncology ( airo )  . 
a multidisciplinary gu tumor board met regularly in 64 ( 73.6% ) out of 88 centers and 54 ( 68.3% ) of the respondents affirmed to be a member of this board . 
importantly , postoperative rt for highrisk bladder cancer has also recently raised attention and the results of the ongoing studies might change the treatment strategy in the future [ 17 , 18 ]  . discussion as the complexity of cancer care for the management of the remaining gu malignancies grows , a multidisciplinary approach is increasingly important [ 12 , 13 ] although the treatment of gu cancer is commonly based on a combined modality approach including surgery , chemotherapy and rt , our survey showed that there is place for improvement in the attitudes of the italian radiation oncologists toward this group of diseases . our survey shows that the majority of the italian radiation oncologists participate actively in the multidisciplinary gu tumor boards ; however , few non - prostate gu tumors are then treated with rt in italy . 
most probably , the attention of the multidisciplinary gu tumor boards is given to prostate cancer and other gu malignancies are not yet managed in the real multidisciplinary way [ 14 ]  . 
such approach is somehow contrary to the recommendations of all national and international guidelines for gu malignancies . bladder radical cystectomy represented for many years the only therapeutic option for muscle - invasive bc . 
nevertheless , to date , the strategy of bladder preservation by means of turbt followed by radio - chemotherapy is a valid option supported by several international guidelines [ 15 , 16 ]  . but , contrary to what might be expected , our findings are similar to those published by jereczek - fossa etal . 
as a matter of fact , a bladder sparing strategy is slow to be adopted and may account for a certain degree of undertreatment of many patients with muscleinvasive bc . 
two main reasons can explain the underutilization of trimodality treatment : ( 1 ) the choice of therapy is still extremely affected by the single specialists background , the use of primary tumor directed rt in rcc reported in our survey was higher than expected : specifically , 2.4% cases ( 1020 patients per year ) and 7% ( > 20 patients per year )  . 
preliminary results deriving from studies evaluating the efficacy and safety of sabr for primary rcc show excellent early outcomes in terms of tumor response with acceptably low toxicity rates [ 20 ]  . 
according to the survey in lombardy region of italy , 6% of all rt treatments for oligometastatic cancer in 2016 was delivered to rcc oligometastatic tumors [ 21 ]  . several studies on the efficacy of multidisciplinary care teams for rcc have demonstrated improved results . 
however , since there are no other published reports on this issue , the results of our survey reflect the pattern of practice in italy . another limitation is the lack of crude numbers of all gu cancer patients treated in italy with rt and the scarce information on the adherence to the guidelines . 
the aim of 1 3 la radiologia medica ( 2018 ) 123 : 879884 our survey was to give a snapshot data on the case - volume regarding non - prostate gu tumors referred to the italian radiation oncologists . 
our survey may serve as a basis to investigate the barriers to the radiotherapy access in gu tumors in italy . in summary , there are increasing evidences , to support the benefits of multidisciplinary approach for urologic malignancies , where the role of radiation oncologist should be part of the decision making process . 
more specifically , multidisciplinary management of gu cases allows patients to meet with clinicians from different oncologic disciplines , including radiation oncology , and better consider the relative advantages and disadvantages of each therapeutic approach , with the ultimate goal of a deeper understanding and identification of the best treatment modality . the impact of team - based management clearly extends beyond the diagnosis and can positively impact the treatment morbidity and mortality . 
although a more effective communication and coordination of the attending physicians seems to be the most obvious gain , multidisciplinary care might have a potential role in influencing practice patterns and improving patient outcomes . 
moreover , several authors have confirmed that multidisciplinary team implementation would dramatically reduce overall patient care costs by decreasing treatment - associated side effects , length of hospital stay , and various other hypothesized savings [ 26 ]  . thus , excluding prostate cancer , multidisciplinary team in other gu cancer still remains in practice poorly developed from an organizational point of view . 
more comprehensive , and more specialized multidisciplinary teams , including specialists like dedicated radiation oncologists with specific skills in gu cancer , are requested to discuss all therapeutic alternatives before treatment is selected . 
from five identified subtypes , especially the somatostatin type 2a receptor can be used for diagnostic imaging in positron emission tomography ( pet ) by ssrspecific radiolabelled peptides ( e.g. , 68ga - dotatate ) but also for peptide receptor radionuclide therapy ( prrt ) [ 3 , 4 ]  . 
this , in turn , implies that in high grade tumor types , ssr - specific vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 860870 radiotracers might come with a limited detection rate which can be enhanced by combining pet with contrast - enhanced ct [ 6 ]  . 
contrast media in mri bear the risk of nephrogenic systemic fibrosis in patients with impaired renal function [ 11 ] and , moreover , the recently discovered phenomenon of retained gadolinium in the brain raises the question about long - term harm of repeated injections [ 12 ]  . 
combining the advantages of high soft tissue contrast together with superior alignment quality , fully integrated pet / mri systems represent a promising alternative to pet / ct for patients with net [ 15 , 16 ]  . 
yet , the examination time of a whole - body pet / mri can sum up to over 1hour which is associated with higher patient discomfort and potential non - compliance , as compared to pet / ct [ 17 ]  . 
to improve clinical schedules and patient compliance , examination times can be reduced using accelerating mr sequence techniques [ 18 ] or by optimizing mr protocols focussing on the clinical question [ 19 ]  . the aim of our study was to evaluate fast non - enhanced examination protocols in abdominal pet / mri in direct comparison to multiphase contrast - enhanced pet / ct with ssr - specific radiotracers regarding the effectiveness of lesion detection for follow - up examinations in patients with unresectable metastasized nets . materials andmethods patient cohort we performed a retrospective evaluation of 29 patients who underwent a pet / mri at the same day immediately after a clinically indicated pet / ct between january 2012 and august 2014 . 
the remaining tracer activity from pet / ct was sufficient for the subsequently performed pet / mri examination , so no additional tracer injection ( and additional radiation exposure for the patient ) was necessary . 
patient and tumor characteristics are given in table1 . inclusion criteria were net in patients history a multiphase contrast - enhanced pet / ct with ssr - specific radiotracers and a pet / mri protocol which covered at least abdomen and pelvis with an axial t2 half fourier acquisition single shot turbo spin echo ( t2 haste ) and diffusion fig . 
 finally , 29 patients with proven net were included in our evaluation weighted imaging ( dwi ) as well as an axial t2 - weighted fast spin - echo sequence ( t2 tse ) with fat saturation the patient population included 9 patients as a part of a larger , prospectively conducted study which was designed as a feasibility study for pet / mri . 
regarding the retrospective scientific evaluation of the pseudonymized data , the local ethics committee waived informed consent . pet / ct tracer injection took place before the pet / ct examination . 
the multiphase ct protocol consists of a bolus - triggered arterial phase scan from the cranial base to the pelvis and a subsequent portovenous phase scan from the upper abdomen to the upper thighs after the intravenous application of 120ml iodinated contrast agent ( flow rate : 3ml / s , ultravist 370 , 1 3 862 table 1 patient and primary tumor characteristics patient primary tumor location grading therapy la radiologia medica ( 2018 ) 123 : 860870 appendix pancreas small bowel small bowel appendix small bowel small bowel small bowel small bowel lung appendix pancreas pancreas small bowel pancreas pancreas small bowel pancreas pancreas small bowel pancreas small bowel stomach ovary surgery surgery surgery , prrt , sandostatin surgery surgery surgery surgery prrt surgery surgery surgery surgery , prrt surgery , sandostain surgery surgery , prrt surgery surgery surgery , sandostatin sandostatin surgery prrt , sandostatin surgery prrt , sandostatin surgery surgery cup cancer of unknown primary , prrt peptide receptor radionuclide therapy bayer healthcare , germany )  . 
pet was iteratively reconstructed using the manufacturers software ( 3d ordinary poisson ordered subset expectation maximization ) including point - spreadfunction algorithm and time of flight image reconstruction using the following parameters : 2 iterations , 21 subsets , gaussian filtering of 2mm , matrix size 400 . 
a dose of 2040mg butylscopolamine butylbromide ( buscopan , boehringer ingelheim , ingelheim , germany ) was intravenously injected right before the examination to reduce bowel movement . mean injection dose of 68ga - high - affinity ( ha ) dotatate ( n = 1 ) or 68ga - dotatate ( n = 28 ) was 157 14mbq and the mean uptake time was 21mboth 68ga - ha - dotatate and 68ga - dotatate are radiolabelled somatostatin analogs with comparable tissue distribution , tracer uptake and lesion detectability [ 20 ]  . 
 examination time per bed position was 4min . a whole - body multiphase contrast - enhanced pet / ct scan takes about 30min in our facility . pet / mri after the pet / ct , patients were transferred to the pet / mri facility . 
the pet / mri scanner is a fully integrated 3t - system which can acquire pet and mri simultaneously ( biograph mmr , siemens healthineers , erlangen , germany )  . 
for attenuation correction , a 3d t1 - weighted spoiled gradient - echo sequence in endexpiratory breath - hold with dixon - based fatwater separation was used as provided by the vendor . 
a focal tracer uptake exceeding regional background together with a morphologic correlate in mri ( e.g. , a lymph node or a parenchymal lesion ) was considered as a malignant lesion . 
focal tracer uptakes in regions with known physiological uptake , e.g. , in the uncinate process or the small bowel wall , were not rated as malignant lesions [ 2325 ]  . 
bulky metastatic lymph nodes and 1 3 864 la radiologia medica ( 2018 ) 123 : 860870 confluent peritoneal metastases were each counted as one lesion . reference standard andstatistical analysis to define a reference standard , the pet / ct and pet / mri examinations were evaluated together in a final consensus reading . 
for the consensus reading , a focal tracer uptake exceeding regional background together with a morphologic correlate in mri and / or multiphase ct was considered as a malignant lesion . 
lesions visible in mri or ct only were defined as malignant according to the clinically established morphological criteria ( e.g. , infiltrative growth , increased / decreased perfusion , diffusion restriction )  . 
follow - up examinations were available in 18 / 29 patients : 7 patients with pet / ct only , 5 patients with pet / ct and pet / mri , 5 patients with pet / ct and mri and 1 patient with mri only . 
to compare the results obtained by the four different setups with pet / ct , a mcnemar test with continuity correction for binary outcome data with dependent samples was used . 
the statistical evaluation was performed with the software jmp ( version 11 , sas institute , cary , ny )  . in a patient - based analysis , a patient was rated as positive / negative if the evaluated setup or pet / ct revealed / did not reveal a metastasis of any kind . results oncologic evaluations malignant lesions were found in 21 / 29 patients ( 72% )  . 
of those , 157 lesions were located in the liver ( 16 patients ) , 40 lesions in the skeleton ( 5 patients ) , 4 lesions in the pancreas ( 4 patients ) , 4 lesions in the small bowel ( 1 patient ) and 18 metastatic lymph nodes ( 10 patients )  . 
previously conducted studies [ 14 , 16 ] with contrast - enhanced mri protocols of the liver and no dwi could show a superiority of mri ( or pet / mri , respectively ) as compared to a multiphase contrast - enhanced pet / ct . 
this is in accordance with our results : the multiphase contrastenhanced imaging in pet / ct was inferior to a pet / mri containing t2 haste , t2 tse and dwi . 
multiphase contrast - enhanced ct reveals some of the metastases ( white arrows ) ; in dwi additional liver metastases could be identified ( dotted arrows ) 1 3 866 la radiologia medica ( 2018 ) 123 : 860870 fig . 
the highlighted lesion is located closely to the vena cava and is not visible in pet of pet / mri ( c ) most probably due to the longer uptake time compared to pet of pet / ct ( a )  . 
in mri , however , it is hard to recognize in t2 tse ( d ) and dwi provided low signal intensity ( e ) in the area leading to low image quality in the adc map ( d )  . 
 this lesion was overlooked in pet / mri 1 3 la radiologia medica ( 2018 ) 123 : 860870 1 3 la radiologia medica ( 2018 ) 123 : 860870 868 fig . 
5 example of a patient with small lymph node metastases in the upper abdomen in pet / mri ( upper row ) and pet / ct ( lower row )  . 
the perfect alignment of pet and ct allowed to correlate the punctual tracer uptake in the pet image to a small lymph node close to the duodenu in pet / mri , a punctual tracer uptake can be seen in the pet image but , however , no distinct morphologic correlate was found in the corresponding t2 tse image ct , especially for dwi at 3t due to the echo - planar imaging technique [ 27 , 28 ]  . 
a reason for that might on the one hand be found in delayed data acquisition in pet / mri as compared to pet / ct and on the other hand in the technique of the attenuation correction in the biograph mmr ( segmentationbased method ) which is based on an mri sequence [ 30 ]  . 
atlas - based methods are implemented in recent updates of vendors software which might improve conspicuity of bone lesions [ 32 ]  . the diagnostic performance of pet / mri in our study was lowest for lymph node metastases as compared to pet / ct . 
bowel movement between the acquisition of pet and mri can , therefore , lead to an imperfect alignment of pet and mri in small mesenteric lymph nodes as shown in fig.5. 
with a patients preparation as it was performed for the pet / ct ( by drinking mannitol and injecting butylscopolamine right before the examination ) , an improved detection rate of mesenteric lymph nodes in pet / mri can be expected . 
moreover , some lymph node metastases in the hilum of the liver were falsely rated as metastatic liver lesions from reader i ( less experienced ) which cannot be interpreted as a general limitation of pet / mri . previously conducted studies could show that pet / mri is sensitive in detecting peritoneal carcinomatosis [ 33 ] which could also be seen in our study . especially with setups ii and iii , the overall lesion detection rate of reader ii ( more experienced ) showed no significant difference to the detection rate of pet / ct , while the detection rate of reader i ( less experienced ) was inferior . 
 less experienced readers might , therefore , benefit from more sequences as provided in setup iv . it should be emphasized that the proposed mr protocol is aimed to serve for a fast staging protocol together with pet and cannot , therefore , replace a dedicated mr examination , e.g. , of the liver ( including , e.g. , t1 - weighted sequences )  . 1 3 la radiologia medica ( 2018 ) 123 : 860870 our study has several limitations . 
neuroendocrine tumors are rare entities and our study design ( pet / ct and pet / mri at the same day ) only allowed to include a relative low number of patients . 
however , previously conducted studies could demonstrate a remarkable similarity of 68ga - ha - dotatate and 68ga - dotatate regarding tissue distribution , tracer uptake and lesion detectability [ 20 ]  . 
therefore , we do not expect significant differences in the diagnostic efficiency between both substances in our study . finally , the chosen reference standard was image based although image parameters were investigated . 
therefore , imaging information of all available modalities including follow - up examinations seems a reliable alternative . in conclusion , the results of our study assume that a protocol containing t2 haste , t2 tse and dwi for nonenhanced pet / mri with ssr - specific radiotracers of the abdomen can be performed in a comparable time and with comparable effectiveness in lesion detection as a multiphase contrast - enhanced pet / ct . 
it might , therefore , serve as a contingent alternative , e.g. , for follow - up examinations in patients with unresectable metastasized neuroendocrine tumors and impaired kidney function . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent the patient population included 9 patients as a part of a larger , prospectively conducted study which was designed as a feasibility study for pet / mri . 
regarding the retrospective scientific evaluation of the pseudonymized data , the local ethics committee waived informed consent . la radiologia medica ( 2018 ) 123 : 871878 radiotherapy stereotactic body radiotherapy foroligometastatic soft tissue sarcoma mauroloi1 marloesduijm1 sarahbaker1 lindarossi1 dirkgrunhagen2 cornelisverhoef2 joostnuyttens1 received : 13 february 2018 / accepted : 12 june 2018 / published online : 19 june 2018 italian society of medical radiology 2018 abstract background stereotactic body radiotherapy ( sbrt ) is emerging as a novel treatment option in metastatic soft tissue sarcoma ( sts )  . 
the aim of our study was to evaluate the effectiveness of exclusive sbrt on disease control and survival in oligometastatic ( 3 synchronous lesions ) sts . materials and methods in total , 16 consecutive patients , accounting for 26 metastases ( including 21 lung and 5 lymph node or soft tissue metastases ) , were treated at our institution with sbrt . 
local control ( lc ) , overall survival ( os ) , distant metastases - free survival ( dmfs ) , and time to initiation of chemotherapy or best supportive care ( corrected disease - free survival , cdfs ) were assessed . results four - year os was 54% and median os was 69months [ 95% confidence interval ( ci ) 20118months ]  . 
increased time from primary tumor to first metastasis identifies patients with potentially greater benefit from sbrt . keywords stereotactic body radiotherapy oligometastases soft tissue sarcoma radiotherapy introduction soft tissue sarcomas ( stss ) are a heterogeneous and rare group of mesenchymal malignancies of connective tissue , encompassing 50 distinct histologic subtypes and accounting for an estimated 25 , 000 new cases per year in europe [ 1 ]  . 
 in early - stage sts , surgery with or without ( neo ) adjuvant radiotherapy is the cornerstone of clinical management and may result in cure [ 2 ]  . 
however , in advanced or recurrent disease , therapeutic options are limited due to poor responsiveness to standard chemotherapy , with an expected median survival of 15months [ 3 ]  . 
in select patients with limited * mauro loi m.loi@erasmusmc.nl 1 department ofradiation oncology , erasmus mc cancer institute , po box2040 , 3000carotterdam , thenetherlands 2 department ofsurgical oncology , erasmus mc cancer institute , rotterdam , thenetherlands metastatic disease , local treatments such as metastasectomy can improve disease control and survival . 
an increasing use in recent years of stereotactic body radiotherapy ( sbrt ) , a highly focused extremely hypofractionated ablative radiotherapy technique , has challenged this preconception [ 7 ]  . 
its applicability to sts metastases has been tested in a small number of monocentric retrospective studies and showed promising local control rates which depend on the treated site [ 816 ]  . 
 this approach may prove particularly beneficial in patients with oligometastatic disease ( an intermediate state between localized and widespread metastatic disease ) [ 17 ] and in patients with the common histologic subtypes of liposarcomas and leiomyosarcoma ( collectively called l - sarcomas ) which share a similar response profile to agents like trabectedin and eribulin and a relative radiosensitivity [ 18 , 19 ]  . 
interpretation of results from previous retrospective series may be limited by a number of confounders , including the inclusion of patients with polymetastatic disease [ 8 , 10 , 12 , 14 ] or bone - derived sarcomas [ 9 , 11 , 15 ] , use of palliative radiation schedules [ 8 , 10 ] , and concurrent administration of other treatment modalities [ 8 , 9 , 16 ]  . 
the aim of our study was to evaluate the effectiveness of exclusive sbrt on disease control and survival in a cohort of oligometastatic sts patients . death from any cause or last follow - up . 
in order to assess the impact of sbrt on disease control and the need for subsequent therapy , a secondary analysis was carried out : distant metastasis - free survival ( dmfs ) was measured from start of radiation therapy to occurrence of new metastases outside the irradiated field . 
a corrected dfs ( cdfs ) as a surrogate indicator of chemotherapy - free survival was calculated as time until development of a new metastasis requiring systemic treatment / supportive care or resulting in death , censoring any distant progression which was effectively treated by repeated sbrt or surgery . materials andmethods statistical analysis patient selection , treatment procedures , andfollowup eighteen consecutive sts patients were treated with sbrt at our institution between may 2005 and september 2016 . 
planning target volume ( ptv ) was obtained by isotropic expansion of 27mm around the macroscopic lesion ( gross tumor volume , gtv ) delineated on a 1.5 - mm - thick slice simulation ct scan . 
clinical evaluation with physical examination and ct scan was performed at 3 and 6months and subsequently every 6months until 5years after the treatment or until disease progression . definition oftheendpoints local failure ( lf ) was defined as an increase of at least 20% in diameter of the treated volume . 
the kaplanmeier method was applied to estimate survival curves , and the log - rank test was used to compare curves of dichotomized categorical and continuous ( cutoff : median value ) variables . 
variables analyzed for lc were tumor site , histologic subtype ( l - sarcomas versus other ) , prior use of chemotherapy in the metastatic setting , time from primary treatment to first relapse , length of tumor ( major axis ) on planning ct , gtv volume size , dose prescribed to the ptv , and maximum point dose to the ptv as expressed in equivalent 2 - gy dose ( eqd2 ) for / = 10 . 
for patient - based endpoints ( dmfs , cdfs , os ) , variables analyzed included age , gender , histologic subtype ( l - sarcomas versus other ) , time from primary treatment to metastases , number of concurrently treated metastases at first sbrt , and prior use of chemotherapy in the metastatic setting . 
histologic subtypes included 3 dedifferentiated liposarcomas ( ls , 19% ) , 1 malignant peripheral nerve sheet tumors ( mpnst , 6% ) , 2 leiomyosarcomas ( lms , 13% ) , 2 rhabdomyosarcomas ( rs , 13% ) , 1 synovial sarcoma ( ss , 6% ) , 1 solitary fibrous tumor ( sft , 6% ) , and 1 myxofibrosarcoma ( mfs , 6% )  . 
in order of incidence , lms ( 7 metastases ) , nos ( 6 metastases ) , ls ( 4 metastases ) , rs ( 4 metastases ) , mfs ( 2 metastases ) , mpnst ( 1 metastasis ) , ss ( 1 metastasis ) , and sft ( 1 metastasis ) accounted for , 1 3 la radiologia medica ( 2018 ) 123 : 871878 respectively , 27 , 23 , 14 , 7 , and 5% of treatments . 
therefore , sbrt was the upfront treatment in 9 ( 56% ) patients and was iteratively performed ( > 1 consecutive treatment ) in 4 patients ( 25% )  . 
at 2 and 4years , dmfs was , respectively , 41 and 33% , median 17months ( 95% ci 530months ) ( fig.2a ) : no correlation with patientrelated variables was found on univariate analysis . 
c overall survival following sbrt stratified by disease - free interval from primary tumor treatment less than 24months ( dashed line ) and greater than 24months ( solid line ) fig . 
late toxicity consisted of grade 1 and 2 chest pain ( n = 3 and 1 , respectively ) , grade 2 cough ( n = 2 ) , and grade 1 chronic diarrhea ( n = 1 ) , while no grade 3 toxicity was reported after a median follow - up per treatment of 43months ( iqr 2270months )  . discussion due to poor prognosis in advanced sts , and limited effectiveness of chemotherapy , local ablative treatments and their possible survival benefit have been extensively studied in recent years , particularly in the oligometastatic setting [ 21 ]  . 
an overview of current literature is summarized in table3 . in our study , we report outcome and adverse events in oligometastatic sts patients undergoing sbrt for both lung and lymph node / soft tissue metastases . 
in general , our 76% 4 - year lc rate is slightly inferior to lc rates reported for lung metastases treated with sbrt [ 11 , 13 , 14 ]  . 
no data on local control are reported in the only study that examined stereotactic treatment of sts metastases of miscellaneous localizations . in our series , median os was 69months , which is comparable to survival following metastasectomy [ 4 , 5 ]  . 
we included only oligometastatic sts patients , as we aimed to determine the specific effect of sbrt without the confounding effect of concurrent or adjuvant ( post - sbrt ) systemic treatment . 
another remarkable point in our study population is that 10 out of 16 patients received sbrt as the first treatment for metastases , while an additional 5 patients received exclusive surgery at first metastatic failure . 
it is likely that these features ( limited oligometastatic disease burden , receiving upfront ablative therapy ) may identify patients at an early phase of cancer progression who may draw the highest benefit from sbrt [ 7 ]  . sbrt in patients with a controlled primary tumor led to a median distant disease control of 17months . 
of note , one patient who received 4 courses of sbrt to lung metastases over a period of 3years was disease free at the time of analysis , 12years after treatment of the primary tumor . 
the treatment strategy of prescribing 1 3 876 la radiologia medica ( 2018 ) 123 : 871878 table 3 summary of published studies on stereotactic body radiotherapy for sarcoma study site prior treatment n patients n metastases follow - up from toxicity dhakal [ 8 ] chang [ 9 ] lung chemotherapy : surgery : 31% spine surgery : 9 / 32 3years : 82% median : g3 : 0 events 1year : 78% median : 25months 29months stragliotto [ 10 ] mixed n / a median : 22months median : 26months g12 : 39 events g3 : 2 events mehta [ 11 ] 4years : 94% 4years : 73% g1 : 24 events folkert [ 12 ] spine n / a 1year : 88% median : acute g12 : 100 ( chemotherapy post - sbrt : 10 / 32 ) ( more than half pretreated with chemotherapy ) lung chemotherapy : surgery : 38% ( chemotherapy post - sbrt : 94% ) ( unspecified number with chemotherapy post - sbrt ) soyfer [ 13 ] lung n / a navarria [ 14 ] lung chemotherapy : surgery : 61% frakulli [ 15 ] lung surgery : 70% lc local control , os overall survival 17months events acute g3 : 1 event chronic g3 : 4 events 100% at analymedian 60months 5years : 96% median g12 : 18 events 70months 2years : 86% 2year : 66% g3 : 0 events metastases occurrence median : 11months median : 22months median : 20months median : 12months median : 95months median : 39months median : 17months median : 16months baumann [ 16 ] lung chemotherapy : 1year : 94% 2years : 43% g3 : 3 events subsequent sbrt courses delayed further progression requiring chemotherapy or supportive care for a median interval of 28months . interestingly , the only predictive factor for lc , os , and cdfs was a disease - free interval from initial diagnosis of less than 24months . 
 [ 14 ] reported a poorer survival in sts patients experiencing metastatic relapse within 24months , showing a 5 - year os of 33% compared to 88% in patients with late - onset metastatic dissemination . 
theoretical models postulate that the interval between primary tumor removal and the appearance of oligometastases is inversely correlated to the scattering phase of malignant cells from the primary tumor [ 22 ]  . 
regarding the correlation between lc and time to metastases , it could be hypothesized that early relapsing tumors may be characterized by higher doubling time and increased resistance to hypofractionated schedules due to fast repopulation [ 23 ]  . 
further research on oligometastatic disease and clinical validation of theoretical principles are needed to guide clinical decision making . in line with previously published studies , sbrt was well tolerated irrespective of the treated site . 
most interestingly , despite a median follow - up time of 36months , no chronic toxicities were observed , confirming the favorable toxicity profile of sbrt . 1 3 la radiologia medica ( 2018 ) 123 : 871878 there are several limitations of our study . 
the patient population is relatively small , and hence , our study may not have detected differences in treatment response between histologic subtypes ( in particular l - sarcomas ) according to differing intrinsic radiosensitivities . 
referral for sbrt may select for less fit patients who are ineligible for surgical metastasectomy ( negative bias ) and , on the other hand , positively select patients with favorable prognostic features , such as a single metastasis . 
 due to the rarity of the disease , large multicentric studies should be undertaken [ 16 ]  . conclusions sbrt in oligometastatic disease results in durable local control in the majority of patients , with a favorable toxicity profile . 
 in patients with controlled primary tumor , median time to distant failure was 17months , while median time to further medical interventions ( chemotherapy or supportive care ) was 28months . 
the role of sbrt in sts oligometastatic patients warrants further evaluation . funding this research received no specific grant from any funding agency in the public , commercial , or not - for - profit sectors . compliance with ethical standards conflict of interest all the authors listed ( mauro loi , marloes duijm , sarah baker , linda rossi , dirk grunhagen , cornelis verhoef , joost nuyttens ) report no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
sensitivity , specificity , positive / negative predictive value and inter - observer agreement ( using cohens ) were calculated to compare diagnostic performance . results lesions were benign in 87 and in 23 cases malignant . 
some studies predicted an increased incidence of salivary gland tumors as high as 5% per year [ 22 ]  . therefore , a correct pre - operative diagnosis of salivary gland tumors is particularly important for a correct , appropriate and instant treatment [ 12 ]  . 
since early diagnosis improves the prognosis of salivary gland tumors [ 17 ] , it is essential for successful treatment of malignant salivary gland tumors of the first degree ( low grade ) with a 5 - year survival rate of up to 90% . 
the 5 - year survival rate in patients with high - grade tumors reaches 50% [ 11 , 26 ]  . the methods of diagnosis primarily depend on the location of lesions , and thus , fine - needle aspiration cytology ( fnac ) and ultrasound are mainly applied to lesions of the superficial glands . 
one of the advantages of mri and ct techniques is the ability to gauge the extent and invasion of the tumor , which can be additionally used for diagnosis [ 5 , 6 , 20 ]  . 
when a tumor is suspected , however , mri should be preferred as it allows a more accurate assessment of the extent of infiltration and tumor demarcation [ 35 ]  . the value of the diagnostic methods ( mri , ct ) in the diagnosis of salivary gland tumors was determined in several studies [ 18 , 30 ] , as well as the importance of multidetector ct ( mdct ) for better assessment and investigation of inflammatory pathologies and tumor extension [ 24 , 25 ]  . 
however , the influence of radiological experience on the diagnostic accuracy and inter - observer agreement has not been investigated to date . in the current era of oncology , salivary gland tumors are interdisciplinarily treated . 
as ear , nose and throat ( ent ) physicians with varying amounts of experience in radiology have access to imaging data , ct and mr scans are routinely reviewed before surgery . 
furthermore , experience levels of the initially reporting radiologists in radiology departments differ considerably . this retrospective study includes the radiological evaluation of mr / ct images by three radiologists with differing radiol med ( 2018 ) 123 : 105116 experience in order to determine the influence of experience on the radiological diagnosis of salivary gland tumors . materials andmethods patients this study was approved by the local ethics committee with a waiver for written informed consent . 
from 2006 to 2012 , 203 patients were examined at our institute with suspected salivary gland tumors ; 75 of those were excluded either due to missing histopathological findings or because of conspicuous features in mri / ct images resulting from a prior iatrogenic procedure . 
the average time between radiological examination and surgery was 28days ( range 1243days )  . magnetic resonance imaging ( mri ) mri examinations were performed using a head and neck coil combination with 1.5tesla units ( magnetom avanto , siemens , erlangen , germany )  . 
turbo spin - echo ( tse ) ( tr / te 539 / 13 ms ) and spin - echo ( se ) ( tr / te 600 / 17 ms ) table 1 histological findings , with morphology codes of international classification of diseases for oncology ( icd - o ) [ 14 ] medical findings cases squamous cell carcinoma ( scc ) 8070 / 3 other malignant tumors adenoid cystic carcinoma ( acc ) 8200 / 3 adenocarcinoma ( nos ) 8140 / 3 non - hodgkins lymphomas ( nhls ) 9680 / 3 , 9699 / 3 melanoma 8720 / 3 pleomorphic adenoma 8940 / 0 warthins tumor 8561 / 0 other benign tumors cystadenoma 8440 / 0 hemangioma 9120 / 0 neurofibroma 9540 / 0 oncocytoma 8290 / 0 diseases without neoplasm cyst sialadenitis lymphadenitis sialadenosis no pathological finding 1 3 radiol med ( 2018 ) 123 : 105116 sequences of t1 - weighted images in transverse direction were acquired before and after contrast administration . 
 the t2 - weighted images ( tse ) with fat suppression were included in transverse plane ( tr / te 4200 / 110ms ) ; 113 of 116 patients received gd - dota as contrast agent ( dotarem , guerbet , france ) with 0.1ml / kg of body weight . 
in three cases , no contrast agent was administered . computed tomography ( ct ) the ct examinations were performed with a dual - source ct scanner ( somatom definition flash , siemens healthcare , forchheim , germany )  . 
if incorrectly affected glands or localization were reported , the diagnosis was considered wrong . statistical analysis statistical evaluation of the results was performed using commercially available software ( medcalc statistical software version 12.7.2 ; medcalc software bvba , ostend , belgium , and bias 8.6.0 , epsilon verlag , frankfurt am main , germany )  . 
the values for sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) of the three raters ( r1 , r2 , r3 ) were calculated regarding dignity and entity . 
the first radiologist ( r1 ) had more than 20years of experience , the second radiologist ( r2 ) 11years , and the third radiologist ( r3 ) 7years of experience in head and neck imaging . 
to provide a better comparability of readouts , observers were allowed to evaluate each case for a maximum time of 10min . results dignity image analysis evaluation of imaging data was performed on regular pacs workstations ( centricity 4.2 , ge healthcare , dornstadt , germany ) ; 116 ( 91% ) mri and 12 ( 9% ) ct scans were diagnosed . to determine malignancy or benignity , reviewers rated tumor dignity on the basis of presented images . 
the differentiation between malignant or benign lesions was made based on criteria that have been thoroughly described elsewhere [ 2 , 8 , 16 , 23 , 27 , 36 ]  . 
the evaluation sheets contained free description text for diagnosis without any predefined diagnoses and fields with pre - defined values for localization and affected glands . for tumor classification , the entity was regarded as correct when the radiological diagnosis corresponded to histopathological findings . 
differential diagnoses were r1 achieved the highest values of all raters for malignancy / benignity assessment , both using mri and ct with values of 100% for sensitivity , specificity , npv and ppv . 
in the classification of squamous cell carcinomas ( scc ) by mri / ct , r1 achieved 100% for all values and r2 and r3 had the same results for sensitivity . 
this might be explained by the fact that both r2 and r3 had the same number of false diagnoses , however , for 1 3 radiol med ( 2018 ) 123 : 105116 1 3 110 radiol med ( 2018 ) 123 : 105116 1 3 radiol med ( 2018 ) 123 : 105116 1 3 112 fig . 
1 calculated values for dignity for mri ( a ) and ct ( b ) sorted by observers ( r1 > 20 , r2 = 11 , r3 = 7years of radiological experience ) radiol med ( 2018 ) 123 : 105116 fig . 
2 inter - observer agreement regarding classification and dignity for mri / ct , assessed by cohens kappa k for the most experienced observer r1 ( > 20years ) , the less experienced r2 ( 11years ) and the least experienced r3 ( 7years ) different cases . 
in our study , however , there was always a difference ( 633% ) between r1 and the other two reviewers . 1 3 radiol med ( 2018 ) 123 : 105116 for malignancy assessment using mri , r2 and r3 achieved the same sensitivity and almost the same values for specificity . 
furthermore , the results of our study are based on histopathology , resulting in a higher accuracy of the reference standard [ 32 ]  . for tumor classification using mri , we noted a confusion of warthins tumors with pleomorphic adenomas . 
4 mri of pleomorphic adenoma on the left parotid gland of a 35 - year - old woman correctly diagnosed by r1 and incorrectly diagnosed by r2 as a cyst and by r3 as a warthins tumor . 
a axial turbo spin - echo ( tse ) t1 ; b sagittal t2w tse and c axial contrastenhanced spin - echo sequence 1 3 114 radiol med ( 2018 ) 123 : 105116 fig . 
these results are comparable with other studies [ 38 ]  . an according observation can be made for the groups other benign tumors and diseases without neoplas all three reviewers partially diagnosed some cases of other benign tumors incorrectly as warthins tumor ( r1 : 1 of 5 ; r2 and r3 : 2 of 5 )  . 
in the group diseases without neoplasm this was even more pronounced , where r1 misdiagnosed 1 of 13 cases in mri as warthin ( r2 : 6 ; r3 : 9 )  . similar to other studies , the most common benign tumor in our study was pleomorphic adenoma [ 33 ]  . 
however , the most common malignant tumor in our study was scc , which is in contrast to other studies where this is the mucoepidermoid carcinoma or adenocystic carcinoma [ 28 ]  . 
none of the healthy patients without neoplasm were correctly diagnosed by r3 . the highest inter - observer agreement was documented between r1 and r2 , reaching from moderate to substantial agreement . 
another limitation is the ratio of mri and ct being 1 : 10 , thus the results regarding ct have limited reliability and should be verified in a larger study . 
the selection of the reviewing radiologists could also be extended with an exacter gradation of radiological experience of the observers . in conclusion , our results indicate that increasing levels of radiological experience leads to a higher accuracy in classification of salivary gland tumors using both ct and mri . 
the following voxel - wise enhancement parameters were extracted : ( 1 ) time to peak enhancement ; ( 2 ) signal intensity at peak ( sip ) ; ( 3 ) peak enhancement percentage ( pep ) ; ( 4 ) post - initial enhancement percentage ( piep )  . 
the following pathological prognostic factors were considered for potential correlation : tumor ( pt ) and nodal ( pn ) stage , grading , perivascular / perineural invasion , estrogen / progesterone receptor status , ki - 67 proliferation , and her2 expression . 
 angiogenesis is the process by which , as the tumor grows , hypoxic stress on tumor cells , caused by the increasing gap between demand and supply of oxygen and nutrients through the normal vessels , leads to the formation of new vessels and / or the sprouting of existing capillaries in the peritumoral stroma through the release of growth factors , particularly the vascular endothelial growth factor ( vegf )  . 
the large endothelial fenestrations of the new capillary system , no longer controlled by regular physiologic mechanisms , give rise to increased capillary leakage of contrast material that can be appreciated on magnetic resonance imaging ( mri )  . 
 this is the pathophysiologic basis for bc detection and differential diagnosis with breast mri [ 6 , 7 ] , that currently represents the most sensitive method [ 8 ]  . dynamic contrast - enhanced ( dce ) - mri allows to extract local perfusion parameters that permit to quantify the angiogenetic activity of breast lesions . 
so far , perfusion parameters have been correlated with pathological prognostic factors such as grading , tumor size , human epidermal growth factor receptor 2 ( her2 ) overexpression , hormonal receptors expression , and ki67 - positive cells percentage , with local recurrences , metastatic spread , and overall survival as well as response to neoadjuvant therapy , with conflicting results [ 9 , 10 ]  . 
patients were imaged in prone position with a dedicated bilateral breast surface coil , on days 714 of the menstrual cycle in premenopausal women and without scheduling limitations in postmenopausal women . 
after a three - plane scout view , the imaging protocol started with a bilateral axial t2 - weighted shorttau inversion recovery sequence and an axial diffusionweighted echo - planar sequence , both of them not considered for the current study . 
at first , spatial resolution was doubled using super sampling tool in order to minimize partial volume effect ; secondarily , the volume was outlined through constraints on consecutive slices . 
we retrospectively reviewed clinical and imaging records of newly diagnosed bc cases surgically treated at our institution from january 2011 to december 2013 , who also had preoperative breast mri performed at our department of radiology . 
the following voxel - wise semi - quantitative enhancement parameters were extracted : ( 1 ) time to peak enhancement ; ( 2 ) signal intensity at peak ( sip ) ; ( 3 ) peak enhancement percentage ( pep ) ; and ( 4 ) post - initial enhancement percentage ( piep )  . pep and piep were computed on three time points : the baseline point ( t0 ) , the end of wash - in phase ( t1 ) , and the post - bolus point ( t2 )  . 
axial t1 - weighted subtracted images show the application of the semi - automatic three - dimensional volume segmentation ( olea medical , la ciotat , france ) of an invasive ductal carcinoma on the right breast . 
segmentation was obtained by selecting a single seed that propagates through slices , using an isointensity algorithm pep = 100 st1 st0 the piep describes in percentage the post - initial behavior of the concentration time curve : st2 st1 piep = 100 based on the pep value , the initial signal increase of the pixel intensity curve has been classified between three wash - in types : slow ( less than 50% increase in signal intensity compared with pre - contrast signal intensity ) , intermediate ( between 50 and 100% increase in signal intensity compared with pre - contrast signal intensity ) , and fast ( over than 100% increase in signal intensity compared with pre - contrast signal intensity )  . 
similarly , based on the piep value , the post - initial signal course of the pixel intensity curve has been classified in : persistent ( signal increase over 10% peak signal intensity ) , plateau ( constant signal intensity10% ) and washout ( signal decrease over 10% peak signal intensity )  . as time to peak enhancement and corresponding peak are independently reached by each voxel also pep and piep were computed taking this into account . 
histological features , including grading , estrogen receptor ( er ) and progesterone receptor ( pr ) status , her2 expression , ki - 67 proliferation , vascular and neural invasion , tumor and axillary nodal stage were obtained from the pathology reports . 
correlations among enhancement parameters and pathological prognostic factors were evaluated using , respectively , spearman ( ) correlation coefficient for pt , pn , histologic grade and ki67 proliferation or phi ( ) correlation coefficients in case of vascular / neural invasion , er expression , pr expression , her2 expression ( positive vs negative )  . 
statistical significance level was set at p < 0.05. results overall , 76 consecutive women were identified in the database ; 56 women were excluded from the analysis for having ductal carcinoma insitu ( 1 ) , multifocal ( 20 ) , multicentric ( 15 ) , non - mass enhancement lesions ( 8 ) or bilateral cancers ( 8 )  . 
they found a significant correlation between model - based and model - free parameters and concluded that general information about tumor vascularization and pathologic prognostic factors may be obtained by routine acquisitions analyzing timesignal intensity curve [ 12 ]  . 
however , dedicated mri protocols aiming at deriving model - based perfusions parameters require t1 mapping and arterial input function favoring high temporal resolution with the sacrifice of high spatial resolution , the latter being indeed necessary for lesion morphology characterization . 
accordingly , our study demonstrated that model - free enhancement parameters obtained from a routine acquisition protocol of breast mri correlate with histological prognostic factors . important to note , her2 gene product is a trans - membrane receptor protein that plays an important role in regulating cell growth and differentiation . 
amplification or overexpression of this oncogene occurs in approximately 1530% of bcs and is relevant for the development and progression 1 3 radiol med ( 2018 ) 123 : 9197 of certain aggressive bcs , being strongly associated with increased disease recurrence and a poor prognosis [ 13 ]  . 
previous studies showed that the vegf expression , related to angiogenesis and microvessel density of bc , is positively correlated with her2 expression in human breast carcinomas [ 15 ]  . 
thus , the increased vascularization revealed by high perfusion indices on mri well addresses the poor prognosis of her2 - positive bcs . tumor stage at diagnosis still influences bc overallsurvivalsignificantly in the current era of effective systemic therapy [ 16 ] , representing a strong predictor of a poor prognosis [ 17 ]  . 
we found that sip and pep , which are indices of high vascularization , correlated with pt ( figs.2 , 3 ) , and may potentially serve as predictive imaging biomarkers [ 17 ]  . 
our results are in line with previous studies reporting an association between increased vascularization and higher histological grading with larger tumor size [ 10 , 19 ]  . lymph node metastases are well - recognized prognostic indicators . 
axial t1 - weighted subtracted images ( above ) and corresponding pep distribution ( below ) of a pt1 ( left ) and a pt2 ( right ) invasive ductal carcinoma . 
representative parametric color - coded maps of sip showing lower values in a pt1 invasive ductal carcinoma ( left ) compared with a pt4 invasive ductal carcinoma ( right ) 1 3 96 radiol med ( 2018 ) 123 : 9197 as expected , the intraand inter - reproducibility of volume segmentation proved to be suboptimal . 
in fact , as it derives from the euclidean geometry , greater the number of considered dimensions , greater the error and lower the reproducibility of the measurement [ 21 ]  . 
automatic segmentation systems are advocated to solve this geometrical difficulty . a growing interest is in the use of mri as a prognostic tool helping to define prognosis and also for a better planning of therapies . 
this is particularly true in patient candidates to neoadjuvant therapies where mri could help to optimize the treatment in non - responders and in patients not suitable for surgery , such as elderly patients , where breast mri could help understand hallmarks of cancers in a non - invasive way . 
the strength of the present study is that it applies a semi - quantitative analysis using data derived from routine clinical acquisitions of breast mri , differently from what has been done in previous perfusion studies using dedicated acquisitions [ 10 , 22 ]  . 
notably , 73% of identified patients was excluded for multifocal , multicentric , bilateral , or non - mass lesions , as however expected in a population of women newly diagnosed with breast cancer requested with mri . 
thus , in order to definitively ascertain the relation between enhancement parameters and pathological prognostic factors of bc , larger prospective studies are needed to figure out the applicability of routine mri acquisitions in a prognostic potential for a predictive , personalized , preventive , participatory ( p4 ) medicine [ 23 ]  . in conclusion , our study showed that voxel - wise enhancement parameters of invasive bcs derived from a routine clinical dce - mri protocol correlated with her2 , pt and pn . 
this supports considering breast mri as a promising tool to improve bc patient management . compliance with ethical standards conflict of interest daniela casolino is product manager for olea sphere software at mts s.r.l. 
other authors declare that they have no conflict of interest . ethical standards the work has been approved by the local ethical committee , protocol code olea_01 on june 2 , 2016 . 
a. , genova , italy 4 diagnostic andinterventional radiology , university ofpisa , via paradisa 2 , 56100pisa , italy 5 department ofsurgical , medical andmolecular pathology andcritical care medicine , university ofpisa , pisa , italy different materials mimicking the appearance of various focal lesions . 
later , the specimen was dissected to set a benchmark for size assessment . results us was able to identify all the simulated lesions within the tongue , resulting in one case more accurate than ct . 
however , further research is mandatory to assess the reliability of invivo us in the detection and characterization of tongue lesions as well as of other oral soft tissue alterations . keywords mouth tongue ultrasound imaging feasibility study introduction oral cancer represents one of the most frequent neoplasms worldwide , being the sixth most common cancer in the world [ 1 ] , with over 450.000 new cases diagnosed each year worldwide . nine out of ten of these neoplasms are oral squamous cell carcinoma ( oscc ) , which may affect every site of the mucosal tissue linings of the mouth , such as tongue , palate , cheeks , lips and mouth floor . 
the tongue is the most common site of oral cancer , with a reported incidence of 17.852% with squamous cell carcinoma accounting for over vol . : ( 0123456789 ) 1 3 136 radiol med ( 2018 ) 123 : 135142 changes during the scans , we brought the specimen to room temperature 4h before scanning . 
prior to introducing the simulated lesions , we defined five parts on the tongue surface for each side considering anatomical landmarks , such as the lingual terminal transverse sulcus and the lateral margin of the tongue . 
historically , oscc has a low survival rate ( < 50% after 5years ) , due to late diagnosis [ 4 ] ; in fact , oscc is often discovered only when the cancer has invaded deep structures and metastases are present , most likely in the cervical lymph nodes , with a significantly worst prognosis . currently , the diagnostic techniques employed in the diagnosis of oral lesions are computed tomography ( ct ) and magnetic resonance ( mr )  . 
ct is a widely available imaging modality , but involves the use of ionizing radiations and contrast agents and may be limited by the presence of streak artefacts due to high - attenuating intraoral material . 
on the other hand , mr is less promptly available and may be limited by the presence of ferromagnetic materials , pacemaker , and the possibility of motion artefacts during the rather lengthy examination [ 5 ]  . ultrasonography ( us ) is extensively used in head and neck applications , for the evaluation of salivary gland , lymph nodes , and subcutaneous tissue . 
advanced applications include us - guided fine - needle aspiration , measurement of tongue cancer thickness for the evaluation of tumour extension and deep infiltration , and diagnosis of metastasis to cervical lymph nodes [ 6 ]  . most us studies of head and neck are currently performed by placing a transducer on the skin surface . 
the study of superficial soft tissue masses with high - resolution grayscale and colour doppler us in some cases may be helpful to distinguish benign from malignant diseases on the basis of ultrasonographic patterns [ 7 ]  . 
however , intraoral us studies performed by placing the transducer directly on the mucosal surface hold the promise to improve the lesions conspicuity ( higher detection rate ) and to lead to a better differential diagnosis by evaluating in greater detail echogenicity , margin , shape , structure , size , and vascularity of the lesions . until now , intraoral us has been hindered by the anatomical constraints that limit the accessibility of conventional us probes in the oral cavity . 
in this preclinical study , we evaluated the advantages of placing an 8mhz transducer directly on an exvivo calf tongue to detect and characterize simulated lesions at different depths within the specimen , using ct as a benchmark for the determination of lesions position . materials andmethods a freshly extracted calf tongue was acquired en bloc from a commercial slaughterhouse within 2h of slaughter . 
1 calf tongue specimen : a right side , view of the defined areas ; the vertical lines divide the specimen into three segments ( tip , anterior part , and posterior part ) , while the horizontal line separates the dorsal and ventral aspects of the tongue ; b ct localization of the lesions , sagittal view ; it is possible to recognize the round - shaped inclusions mimicking capsulated lesions and the materials used to perform tissue alterations ; c ct localization of the lesions , axial view 1 3 radiol med ( 2018 ) 123 : 135142 different appearance at us and ct . 
no simulated lesion was localized in the dorsal portion of the tongue , which is the least involved area affected by squamous cell carcinoma [ 8 ]  . the calf tongue was imaged using a us scanner equipped with a prototype broadband linear array probe ( l8 - 20 , esaote , firenze , italy ) with very high spatial images were obtained using the probe at a mean frequency of 8mhz , both in the sagittal and coronal scanning planes . 
after selecting the b - mode , the probe was placed perpendicular to the dorsal part of the tongue to preliminarily identify the simulated lesions and then rotated 90 clockwise to evaluate all the aspects of the lesions . 
scanning parameters were the following : detector configuration 640.625mm , tube voltage 80140kv via fast kv switching , tube current 600ma , tube rotation time 1s , detector collimation 0.625mm , reconstruction interval 0.625mm , beam pitch 0.516 : 1 and standard reconstruction kernel . 
a stack of monochromatic images with the same slice thickness ( 0.625mm ) and an energy level of 65kev was generated using an iterative reconstruction algorithm ( 30% asir , ge healthcare ) to maximize contrast - tonoise ratio for optimal assessment of both normal tongue tissue and simulated lesions . 
orthogonal and oblique multiplanar reformatted ( mpr ) views and volume rendering ( vr ) images were produced for localization and threedimensional depiction of each simulated lesion . after the ct acquisition , we dissected the specimen and extracted the materials used to create the lesions . 
non - parametric rank correlation was performed using spearmans rho to assess the relationship between the variables using a monotonic function and kendalls tau to evaluate whether the ranks between observations were equal or not . 
finally , regression analysis was carried out to estimate the relationships among the variables . results all 14 simulated lesions introduced in the specimen were easily detectable using our us equipment . 
in particular , us was able to visualize even the finest insertions ( like the 3 - 0 suture thread ) and provided a clear distinction between normal tissue and the areas where the silicone rubber and toothpaste were injected . 
a 3 - 0 suture thread : it is possible to recognize the sinusoidal pattern through the tissue ; b vaseline inclusion : it is possible to appreciate the knot used to seal the inclusion ; c inclusion of silicone rubber ; d wax cone inserted longitudinally with the major axis oriented parallel to the dorsal surface of the tongue analysed using volume reconstructions as well as coronal , axial , and sagittal reconstructions to optimize the visibility of the lesions , to highlight their structure and ct attenuation , and to differentiate them from normal tissue and air . 
the only simulated lesion that was not identifiable at ct was the one produced with the monopolar electrosurgical unit . the comparison between the size of the simulated lesions measured at us and their actual size in the dissected specimen as measured using a boley - gauge orthodontic caliper is reported in table2 . 1 3 radiol med ( 2018 ) 123 : 135142 discussion in this preclinical study , we used a prototype us system for detecting and characterizing tongue - simulated lesions on an exvivo specimen . 
our experimental setting presented the advantage of placing the transducer directly on the surface of the tongue , providing a clear depiction of superficial lesions as well as relatively deeper tissue alterations . previous clinical studies have investigated the effectiveness of intraoral us for the diagnosis of oral cancer and proved that us performed well in the evaluation of tumour depth , which is an important prognostic factor related to lymph node metastasis [ 914 ]  . 
 started from a histopathological diagnosis of oscc and then compared us imaging data with the surgical findings in terms of tumour thickness and presence of neck metastases [ 15 ]  . 
found that intraoral us delineated the extent of the lesion of the oral cavity in all the enrolled patients , presented strong correlation with the histological sections , and could identify most tumours less than 5.0mm in thickness unlike ct and mr [ 2 ]  . 
us can identify lesions up to 1.0mm , while ct and mr could not differentiate various tissues within millimetres and are limited by distortions from dental fillings , x - ray beam hardening , and insufficient tissue contrast in case of very small lesions [ 16 ]  . 
show that us images reflect the actual tumour thickness more precisely than the measurements obtained using histological sections , due to formalin tissue fixation and slide preparation [ 9 ]  . the status of resection margins is an important prognostic factor for oscc , as achieving tumour clearance of 5mm or more at the primary site can decrease the incidence of locoregional recurrence , also obviating the need for adjuvant radiotherapy . 
a three - dimensional volume rendering ; b coronal reconstruction ; c axial reconstruction ; d sagittal reconstruction the mean difference between the us measurements and the caliper measurements was 0.18cm , with a statistically significant correlation between the two measurements ( pearson correlation coefficient 0.609 , p < 0.05 , kendalls tau - b coefficient 0.593 , p < 0.01 , spearmans coefficient 0.733 , p < 0.01 ) ( tables3 , 4 )  . 
 ( 2 - tailed ) * * correlation is significant at a level of 0.01 ( 2 - tailed ) of reliability with histological measurements for tumour thickness [ 10 ] , and us has also been used for the detection of recurrent tumours and post - treatment changes after radical radiotherapy , confirming clinical findings and increasing the confidence in making early detection of recurrence [ 11 ]  . 
some authors have tried to identify the risk related to tumour volume and lymph node metastasis , since the oral cancer tnm staging system presents limited prognostic significance as it considers the two - dimensional aspect alone for t1t3 and defines deep or extrinsic muscles infiltration to categorize oral tongue and floor of mouth squamous cell carcinoma as t4a [ 12 ]  . 
showed that in 88% , us was able to distinguish between the tissue lesions and the normal tongue parenchyma and demonstrated the reliability radiol med ( 2018 ) 123 : 135142 fig . 
the plotted points were close to the regression line , suggesting a strong relationship between the variables under study of us for the evaluation of tumour thickness against histological measurement [ 17 ]  . 
found a correlation between the quantitatively analysed invasive front in tongue cancer on us images and the histological malignancy grade groups , providing a non - invasive and valuable diagnostic modality , which can predict cervical lymph node metastasis preoperatively and thereby assist in preoperative evaluation of tongue lesions and surgical planning [ 14 ]  . together with colour doppler us , vascularity in oral masses can be shown , helping to differentiate malignant masses from benign ones [ 13 ]  . 
some authors set 7mm as a cutoff measure for risk of lymph node metastases ( 7mm 12% risk , > 7mm 57% risk ) and recommend regular followup [ 15 ]  . 
moreover , high - resolution diagnostic intraoral us works excellently for real - time examination of soft tissues to assess tumour thickness and surgical clearance just after resection [ 20 ]  . 
in case of head and neck cancer of unknown primary site , us is a feasible means to identify primary oropharyngeal tumours , even of small dimensions , making patients eligible for less invasive treatment [ 19 ]  . 
moreover , intraoral us can be routinely used for suspected peritonsillar abscess diagnosis and drainage treatment [ 21 ] , presenting 1 3 radiol med ( 2018 ) 123 : 135142 from 90 to 100% sensitivity and allowing guided needle puncture for aspiration [ 22 ]  . therefore , us could provide the possibility of better understanding of the three - dimensional anatomy of oral mucosal lesions , defining the patterns of neoplastic locoregional spread and adding important diagnostic information on treatment and prognosis . the results of our study suggest that intraoral us may be effectively used to detect tongue lesions and possibly other lesions of the oral cavity with relative ease and is capable of measuring them very precisely . 
we also showed that us performs better than ct , in terms of lesion identification , but it must be noted the experimental setting did not allow us to benefit from the contrast enhancement that is achievable in the clinical setting . 
another limitation of the study was the lack of comparison with mr , which has a better contrast resolution in soft tissues : further research has to be conducted using mr - compatible materials to simulate lesions without significant artefacts . 
the use of an exvivo specimen with simulated lesions aiming to resemble oral diseases , but different in their pattern , highlights the actual need of further studies to thoroughly assess the accuracy of intraoral us in a clinical setting . acknowledgements the support of the staff in the radiology institute of the university hospital , cisanello at the university of pisa , is gratefully acknowledged . 
group 4 was scanned as standard radiation dose ( srd ) group : 120kvp , automatic tube current modulation ( atcm ) technique with an image quality index of 20 , and filtered back projection ( fbp ) algorithtube voltage for three rrd groups was 80 kvp in group 1 , 100kvp in group 2 , and 120kvp in group 3 , and all three groups were with image quality index of 18 and imr algorithimage noise , signal - to - noise ratio ( snr ) , and contrast - to - noise ratio ( cnr ) were measured . 
on top of that , lower tube voltage tended to be more optimal . keywords radiation dose iterative model reconstruction ct angiography renal artery image quality introduction renal artery computed tomography angiography ( cta ) as a noninvasive method has been widely used to investigate renal vascular diseases such as atherosclerotic renal artery stenosis ( ras ) [ 13 ]  . 
although catheter - based arteriography still represents the gold standard for diagnosing ras , previous studies have reported that renal artery cta also had high sensitivity ( 94100% ) and specificity ( 7997% ) [ 4 , 5 ]  . 
however , concerns over radiation exposure of cta still remain due to their potential risks for cancer [ 6 ]  . recently , some scanning strategies including low tube voltage , tube current modulation and adaptation and highpitch data acquisition allowed cta to be done with lower radiation doses [ 79 ]  . 
however , only optimization of scan parameters may be accompanied with deteriorated diagnostic quality of ct images due to substantial increases of image noise and / or beam - hardening artifacts , especially for low tube voltage . 
for the sake of comprising lower image quality ( iq ) brought by low tube voltage and / or high pitch , iterative reconstruction ( ir ) algorithms were introduced vol . : ( 0123456789 ) 1 3 84 radiol med ( 2018 ) 123 : 8390 to help reduce the quantum noise associated with standard filtered back projection ( fbp ) reconstruction algorithms , which was able to address increased image noise in reduceddose ct scans [ 1012 ]  . 
in the last decade , hybrid - type ir ( hir ) algorithm was demonstrated facilitating dose reductions of 2366% depending on the proportion of iteration blending with fbp [ 13 ]  . 
nowadays , a more advanced ir algorithm known as iterative model reconstruction ( imr ) with a knowledge - based approach that yields improved image quality and virtually noise - free images has been introduced to enable further dose reduction and image - quality improvement [ 6 , 12 ]  . 
imr turns out to be a promising technique in the population of young patients or those who need to receive repeated ct examinations [ 14 , 15 ]  . to the best of our knowledge , this is the first article about the application of imr in renal artery cta . 
thus , we primarily aimed to investigate whether reduced radiation dose ( rrd ) protocols reconstructed with imr could offer better iq than standard radiation dose ( srd ) protocol with fbp . 
 furthermore , by comparing several rrd protocols with different tube voltage , we also tried to find the optimal rrd scanning parameters for imr algorithm . materials andmethods study population this study was approved by the institutional review board , with waiver of patient informed consent . 
patients who were allergic to iodinated contrast agent , had a history of renal surgery or intervention treatment of renal artery were excluded , and those who had a bmi over 30kg / m2 were also ruled out to eliminate the poor iq brought by extremely large shape . ct acquisition andimage reconstruction patients were randomly assigned into 4 groups ( 20 for group 1 , 24 for group 2 , 20 for group 3 , and 20 for group 4 ) according to their scan date . 
detailed acquisition parameters were as follows : collimation , 1280.625mm ; pitch , 0.914 ; gantry rotation time , 0.4s ; fov , 350mm ; slice thickness , 1.0mm ; slice increment , 1.0mm ; matrix , 512512 ; tube voltage , 80 kvp for group 1 , 100kvp for group 2 , 120kvp for group 3 and 4 ; tube current products , automatic tube current modulation ( atcm , doseright , philips heathcare ) represented as doseright index was used to reduce or raise tube current to maintain constant radiation dose . 
 the injection protocol for all groups were identical : 0.8ml / kg of contrast at injection rate of 3.5ml / s followed by a saline chaser of 20ml at the same rate . 
raw data from group 1 , 2 and 3 were reconstructed with imr technique ( level 1 , soft tissue ) , while images from group 4 were reconstructed with conventional fbp technique . radiation dose the radiation dose information of all ct examinations was expressed as volume ct dose index ( ctdivol , mgy ) and dose length product ( dlp , mgy cm ) obtained from the exam summary page of each mdct scan . 
effective dose ( e , msv ) was calculated using the following equation : e = edlpdlp , and edlp was a conversion factor equal to 0.015 taken from normalized value of effective dose per dose - length product for the abdomen [ 16 ]  . image quality evaluation all images were reviewed and interpreted on a commercially available workstation ( intellispace portal version 6.0 , philips healthcare )  . 
multiplanar reformations ( mpr ) , maximal intensity projection ( mip ) images and volume render ( vr ) images were also reconstructed as accessory modalities for determining vascular stenosis . a senior radiologist with more than 5years of experience in abdominal radiology blinded to scanning protocols performed objective image assessment on reconstructed 1.0mm thick axial images , and the following findings were recorded : ( 1 ) transverse diameter of the abdominal circumference was measured on the slice with largest anteriorposterior diameter . 
 ( 2 ) mean ct attenuation values ( in hounsfield units ) of abdominal aorta , right renal artery and left renal artery were measured in region of interest ( roi ) s on abdominal aorta at the level of renal hilum and on bilateral renal artery trunk 1cm from their origins , respectively . 
 ( 3 ) standard deviation ( sd ) , which stood for image noise , 1 3 radiol med ( 2018 ) 123 : 8390 was measured in a roi of 50mm2 drawn in a homogeneous region of the subcutaneous fat of the anterior abdominal wall . 
 ( 4 ) the signal - to - noise ratio ( snr ) and contrast - tonoise ratio ( cnr ) of abdominal aorta and renal arteries were calculated using the following formulas : snr = mean attenuation / image noise ; and cnr = ( mean attenuationmean muscle attenuation ) / image noise , where mean attenuation referred to the mean ct attenuation of the aortic and bilateral renal artery rois respectively , and mean muscle attenuation was the mean attenuation of psoas muscle roi [ 8 ]  . 
 snr and cnr were used to minimize bias from the single measurement . for subjective image quality assessment , available images included axial source images , mpr , mip and vr images . 
diagnostic confidence was rated : 1 = unacceptable , completely non - diagnostic ; 2 = poor , only suggesting lesion , 3 = good , diagnostic , 4 = better , diagnostic confidence , 5 = excellent , fully diagnostic confidence . 
vessel artifact was scored : 1 = severe noninterpretable artifacts ; 2 = very artifactual under limited conditions ; 3 = moderately artifactual not interfering with evaluation of anatomic structure ; 4 = slightly artifactual ; 5 = optimal or indicated no artifacts . 
intravascular contrast was also scored : 1 = unacceptable ; 2 = poor contrast with obscured contour ; 3 = fair contrast with the contour slightly obscured but without impacting of diagnosis ; 4 = good contrast ; and 5 = excellent . 
scores by the more experienced observer 1 were used to be compared . statistical analysis all statistical analyses were performed by commercially available statistical product and service solutions ( spss ) software , version 22.0 ( ibm , new york , united states )  . 
there was no statistical difference among four groups of sex , age , height , weight , bmi and abdominal circumference diameter ( table1 )  . dose radiation ctdi , dlp and e showed statistical differences among four groups ( p < 0.05 ) ( table2 )  . 
 vessels were well demonstrated on axial ( a ) , mip ( b ) and vr ( c ) images reconstructed by imr algorith another 62 - year - old man ( bmi 23.7 kg / m2 , perimeter 331.4 mm ) of group 1 also underwent renal artery cta for hypertension . 
axial ( d ) , mip ( e ) and vr ( f ) images all clearly confirmed the severe stenosis of the proximal portion of right renal artery renal arteries were detected in right renal arteries and 11 in left renal arteries . 
four patients were diagnosed of slight stenosis with no plaque . discussion our study demonstrated that rrd - protocol renal artery cta reconstructed with imr algorithm could provide better iq than that of fbp images with srd protocol . 
what is more , lower tube voltage was proved to be optimal rrd scanning parameters for imr algorithm in renal artery cta . this study was designed to decrease peak voltage in two rrd groups compared with srd group , and adopt doseright function in three rrd groups to ensure approximate 40% reduction of radiation dose . 
thus , we did not reduce the overall radiation dose of rrd groups to the level of previous reports so as to detect the small mural plaque on renal arteries and make precise decision of stenosis . as shown by both objective and subjective evaluation in current study , images reconstructed with imr algorithm in these three rrd groups led to perceivably better iq than that of fbp algorithm in srd group . 
reported that low - dose protocol using iterative model - based reconstruction in abdominal cta could provide high iq and improve vascular contrast compared with fbp [ 21 ]  . 
indicated that even with 12.5% - dose , modelbased iterative images of upper abdomen could yield comparative objective image noise and snr to fbp images with control - dose [ 22 ]  . 
however , imr algorithm based on structural knowledge models could produce the truest and most superior images by repeatedly decreasing differences between ideal models and acquisition data [ 12 , 24 ]  . 
this mechanism permits imr to be an effective method to lower image noise which could be much helpful when determining vascular enhancement , border and stenosis , especially with rrd protocol . 
but we had the opposite view that it was confident to evaluate the stenosis of renal arteries and its associated 1 3 88 radiol med ( 2018 ) 123 : 8390 fig . 
although with reduced radiation dose , a , b reconstructed with imr showed conspicuously better intravascular enhancement , smoother border and lesser noise of bilateral renal arteries than c and d reconstructed with fbp . 
one possible reason for the better iq of 80 and 100kvp protocols might be that the lower tube voltage was , the higher the attenuation of arteries would be under the circumstances of similar patient bmi and contrast injection volume . 
because only if the mean effective energy of the polychromatic x - ray approaches 33.2kvp , reducing tube voltage would increase the absorption of iodinated contrast [ 26 ]  . 
however , our subjective scores revealed that when with imr reconstruction , diagnostic confidence was similar in these three groups , while artifact evaluation was even better with 100kvp than with 120kvp , suggesting its reduction of beam hardening . 
 also supported our results that in abdominal ct examinations , low - tube - voltage scanning with model - based iterative reconstruction would be able to provide less artifact streak and superior diagnostic acceptability [ 19 ]  . 
improving vascular enhancement and lowering tube voltage would generally increase image noise , but imr algorithm would still be capable of reducing noise by obtaining more precise noise model and utilize scan data more efficiently [ 27 ]  . our study had some limitations . 
last but not the least , the overall radiation dose of our three rrd groups were similar , and we lack a stepwise gradation of radiation dose levels to seek the lowest dose level with which imr reconstruction could provide diagnostic iq . in conclusion , imr images in renal artery cta with rrd protocols could provide clinically significantly better iq in terms of both objective and subjective evaluation than fbp images with srd protocols . 
on top of that , lower tube voltage protocols were proved to be optimal rrd scanning scheme in renal artery cta for clinical work . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
a review of our pacs database for the period from march 1 , 2007 to july 31 , 2016 revealed 158 confirmed ms patients who received exclusively either gadoterate meglumine ( n = 81 ) or gadobutrol ( n = 77 ) for diagnosis and follow - up . 
si measurements on unenhanced t1 - weighted images were performed on all scans of all patients and at regions of interest ( rois ) positioned on the dentate nucleus ( dn ) and pons . 
although brain t1 hyperintensity may occur for a variety of reasons unrelated to gbca exposure [ 1923 ] , retention of gadolinium ( gd ) either as intact gbca or as released gd bound to macromolecules is now recognized as a principal cause of recent observations . 
nevertheless , imaging studies have focused primarily on the dentate nucleus ( dn ) and globus pallidus ( gp ) , since these are the brain areas in which visible t1 hyperintensity is most evident . 
these studies have primarily reported visible t1 hyperintensity after the cumulative administration of linear gbcas but not after the cumulative administration of macrocyclic gbcas [ 59 ] , even though gd presence has been confirmed after the administration of both classes of gbca [ 26 ]  . 
to date , studies that have demonstrated quantitative t1 signal increases after the administration of macrocyclic gbcas [ 17 , 18 ] , have been criticized [ 2729 ] in part due to the lack of conspicuous visible t1 hyperintensity . 
although accurate speciation analysis is vol . : ( 0123456789 ) 1 3 126 radiol med ( 2018 ) 123 : 125134 currently lacking , the observed differences between linear and macrocyclic gbcas are widely assumed , rightly or wrongly , to reflect differences in chelate stability , with the greater t1 hyperintensity seen with linear gbcas reflecting greater release of gd than is the case with the more stable macrocyclic gbcas . patients with multiple sclerosis ( ms ) undergo frequent contrast - enhanced mr examinations and thus receive numerous gbca administrations over the course of a lifetime . 
studies that have looked at t1 signal changes in these patients have consistently demonstrated increased t1 - signal in the dn after administration of the linear gbcas gadopentetate and gadodiamide [ 2 , 30 , 31 ] but have produced conflicting results for the macrocyclic gbcas with some authors reporting no t1 signal changes after administration of gadobutrol or gadoterate [ 3133 ] and others reporting significant quantitative increases after administration of gadobutrol [ 17 ]  . 
the aims of our study were to assess changes in dn signal intensity on unenhanced t1 - weighted mr images after multiple administrations of the macrocyclic gbcas gadobutrol and gadoterate , and to compare our findings with findings from previous studies with the linear agents gadopentetate and gadobenate . materials andmethods patients this single - center retrospective study was approved by the institutional review board and the need for patient informed consent was waived . 
we reviewed our pacs database for patients with rr - ms who underwent repeat mri of the brain during the period from march 1 , 2007 to july 31 , 2016 . 
for inclusion in the study patients were required to have had : ( 1 ) a minimum of at least four consecutive mri examinations enhanced exclusively with the macrocyclic gbcas gadoterate meglumine ( dotarem ; guerbet , aulnay - sous - bois , france ) or gadobutrol ( gadovist ; bayer healthcare , berlin , germany ) ; ( 2 ) rr - ms diagnosed and followed up at mri performed exclusively at our institution ; ( 3 ) an egfr of 60ml / min / 1.73m2 or above , on the basis of the chronic kidney disease epidemiology collaboration formula [ 42 ] , based on a blood sample taken close to the date of the last mr examination . 
exclusion criteria were : ( 1 ) cerebrovascular events including hemorrhage , stroke , or brain ischemia ; ( 2 ) previous cerebral neurosurgical treatments or radiation therapy ; ( 3 ) intraaxial brain tumor or other lesions such as vascular malformations located in the cerebellum or pons ; ( 4 ) history of intracranial infection , such as meningitis or encephalitis ; ( 5 ) abnormal liver function or hepatic deficiency ; ( 6 ) alternate use of the two gbcas in the same patient or unclear documentation of the gbca used . 
the final patient cohort comprised 158 patients of which 81 received exclusively gadoterate and 77 exclusively gadobutrol . for all included patients , the age , sex , number of gbca administrations and accumulated dose were recorded ( table 1 )  . 
the dn - to - pons ( dnp ) t1 - si ratio was then calculated for each mr examination . statistical analysis statistical analyses were carried out using dedicated software ; ( stata - corp , version 8.2 ; college station , tx , usa ) and a priori significance level was set to p < 0.01. 
unpaired t tests were used to determine if the mean change in dnp t1 - si ratio ( obtained by subtracting mean dnp t1 - si ratio determined for the first mri examination from the mean dnp t1 - si ratio determined for the last mri examination ) was different from 0 . 
 linear regression analysis revealed no significant influence ( p > 0.01 ) of age , sex or kidney function on the observed dnp t1 - si ratio differences for either gadoterate or gadobutrol ( table3 )  . comparison withliterature findings we compared our results with those of radbruch etal . 
no significant differences ( p > 0.01 ) in first - to - last dnp t1 - si ratios were noted between our findings for gadoterate and gadobutrol and those of radbruch etal . 
conversely , our firstto - last dnp t1 - si ratios for gadoterate and gadobutrol were both significantly lower ( p < 0.01 ) than those determined by radbruch etal . 
for gadopentetate and gadobenate , respectively . the effect of accumulated dose on mean first - to - last dnp t1 - si ratios as assessed using linear regression analysis is shown in table5 . 
linear regression revealed a significant difference between linear and macrocyclic gbcas in terms of quantitative data across different publications and revealed overall similarity between our findings and those of other authors regarding macrocyclic gbcas . discussion the relative molecular stabilities of gbcas and their potential to release gd have been a major concern since the first association between gbca administration and the occurrence of nephrogenic systemic fibrosis ( nsf ) [ 45 ]  . 
a consequence of nsf in europe ( unlike elsewhere in the world ) was that the european medicines agency ( ema ) classified gbcas according to their invitro stability constants as being of low , intermediate , or high risk of inducing nsf [ 46 ] , with the macrocyclic gbcas ( gadoterate , gadobutrol , gadoteridol ) classified as low risk , the simple linear gbcas ( gadodiamide , gadoversetamide , gadopentetate ) classified fig . 
2 axial t1 image shows two regions of interest ( rois ) positioned on the right dentate nucleus and the central part of the pons for assessing the dentate nuclei - to - pons ( dnp ) t1 - si ratio unpaired t tests were also used to determine whether statistical differences exist between our findings and findings published previously for linear gbcas [ 9 , 10 ]  . 
despite these quantitative findings , visible t1 hyperintensity was noted in approximately onethird of all patients in both groups that received at least five administrations of with gadoteridol or gadobutrol . 
4 a , b unenhanced axial t1 - weighted image a of the first exam shows substantial homogeneous signal intensity of the dentate nuclei compared to pons area ; after 11 administrations of gadoterate the unenhanced axial t1 - weighted image , b shows a marked increase of the dn signal intensity relative to the mean signal value determined in the first exam 1 3 130 radiol med ( 2018 ) 123 : 125134 fig . 
although this classification is incongruous in that no cases of nsf have ever been reported after the sole administration of any intermediate risk gbca [ 4749 ] while confirmed cases of nsf have been reported 1 3 radiol med ( 2018 ) 123 : 125134 table 5 results of linear regression analyses of the mean si ratio differences considering different groups of contrast agents and respective accumulated doses criterion parameter regression coefficient 95% ci standardized regression coefficient gadoterate meglumine vs . 
imaging studies that have investigated the propensity of gbcas to cause si increase in the dn and gp on unenhanced t1 - weighted images have further cemented this perception ; invariably , t1 - signal increases have been extensively reported after serial administrations of linear gbcas while studies that demonstrate quantitative si increases after serial administration of macrocyclic gbcas have been less frequent [ 27 , 28 ]  . our findings are consistent with those of previous studies and yet offer new insights into t1 - signal changes in the dn following serial macrocyclic gbca administration . 
 [ 9 ] who also demonstrated a small but non - significant increase in dnp t1 - si ratio ( 0.00160.0266 ) in 50 patients with mainly glioma / glioblastoma following serial administrations of gadoterate . 
 comparison with previous findings for the linear gbcas gadopentetate [ 9 ] and gadobenate [ 10 ] confirmed that significantly lower t1 - signal increases in the dn are noted with the macrocyclic gbcas gadoterate and gadobutrol . 
on the other hand , at variance with previous studies performed with macrocyclic gbcas [ 59 ] , we noted visible t1 hyperintensity in the dn in approximately one - third of patients in each subgroup that received at least five administrations of either gadoterate or gadobutrol . 
although detailed analysis of these qualitative findings was beyond the scope of this initial study , specific evaluation of these patients is currently underway . we administered a standardized dose of 0.1mmol / kg of bodyweight of either gadoterate or gadobutrol for all mr examinations . 
given that significant negative correlations between the mean time interval between exams ( 115.07.4weeks for gadoterate ; 123.63.3weeks for gadobutrol ) and the dnp t1 - si ratio increases were not observed , our results confirm that short injection intervals should not lead to significant changes in t1 hyperintensity in the dentate nuclei . our findings differ from those of stojanov etal . 
 [ 18 ] in that , whereas we also noted small increases in dnp t1 - si ratios following multiple administrations of gadoterate and gadobutrol , the changes we observed were not significant . 
 [ 17 ] enrolled fewer patients ( n = 58 ) which may have affected the statistical analysis and that the first enhanced mri exam in their analysis was not necessarily the first enhanced mri exam the patient received . 
 [ 10 ] in 1 3 132 radiol med ( 2018 ) 123 : 125134 their analyses of the linear gbca gadopentetate and the substituted linear gbca gadobenate , respectively . although the patient inclusion and exclusion criteria for our study were largely identical to those of radbruch etal . 
however , whereas the different pathologies might be considered a potential confounding factor , evidence to date suggests that gd entry into the brain occurs primarily by the glymphatic pathway [ 51 ] and that the specific type of pathology is only minimally relevant , if at all . a potential drawback of dnp ratio determinations to assess possible gd retention is that gd presence is observed throughout the brain including the pons , as well as in other body organs [ 2426 ]  . 
however , whereas this might imply systematic underestimation of the amount of gd retained based on dnp ratios , it has been shown that the amount retained in the dn is 22 times higher than that in the pons [ 24 ]  . 
however , this approach is limited due to motion and pulsation artifacts caused by the physiologic flow of csf during systole and diastole [ 52 ] which potentially leads to inhomogeneous signal measurements and thus artifactual variations in dn - to - csf ratio . a final consideration concerns the form of gd potentially retained in the dn and elsewhere and whether this reflects the retention of intact gbca molecule or gd released from the gbca molecule and subsequently bound to macromolecules . 
currently , it is widely presumed that t1 - signal increases reflect gd released from the gbca molecule possibly through gbca dissociation and transmetallation with competing endogenous metals , such as zinc , copper , calcium , and iron [ 5355 ]  . 
a recent study performed in animals [ 56 ] suggests marked differences between the three available macrocyclic gbcas implying that future investigation should focus on each gbca individually rather than considering gbcas within each class to be equivalent . limitations of our study are that we did not correlate the different clinical manifestations of ms with the possible presence of gd in the dn as performed elsewhere [ 17 , 57 ]  . 
 [ 58 ] observed possible t1 signal increases in the dn of ms patients suffering of secondary progressive disease , although at the time of the study ( 2009 ) no association with retained gd was made . 
nevertheless , given that only approximately 1015% of ms cases is affected by secondary progressive disease [ 59 ] this may not have been a contributory factor in our study . in conclusion , we found small first - to - last increases in dnp t1 - si ratios in patients with ms following multiple administrations of the macrocyclic gbcas gadoterate and gadobutrol . 
although the changes were minimal and lower than those observed with linear gbcas , our findings confirm that t1 hyperintensity in the brain , potentially indicative of gd retention , occurs after serial injections macrocyclic gbcas . author contribution statement splendiani is the principal investigator . 
other authors have equally contributed in drafting / revising the manuscript for content , including medical writing for content , study concept or design , and analysis or interpretation of data . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards and patient consent we declare that all human and studies have been approved by the local ethics committee and have therefore been performed in accordance with the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . 
 mbir images were also compared with the images of 21 standard - dose paranasal sinus patients reconstructed with adaptive statistical iterative reconstruction ( asir ) algorithin the second phase , 14 pediatric tumors patients ( images with asir in the initial scan ) who came for followup paranasal sinus ct scan were prospectively enrolled with reduced radiation and mbir algorithin both study phases , image noise and the contrast noise ratio ( cnr ) of sphenoid was measured ; and subjective image quality was evaluated . 
56 , nanlishi road , xicheng district , beijing100045 , china vol . : ( 0123456789 ) 1 3 118 radiol med ( 2018 ) 123 : 117124 keywords children paranasal sinus model - based iterative reconstruction algorithm ( mbir ) low - dose ct radiation dose based on the first phase study and reconstructed using mbir algorithm to further validate its clinical applicability . introduction ct is an excellent imaging modality for displaying bony structures and has become a routine imaging examination of the paranasal sinuses [ 15 ]  . 
however , due to scan region overlap between sinus and eye , the potential damage to vitreous body of the eye when imaging sinus is always a concern [ 612 ]  . 
although sinus mri has an excellent contrast resolution for sinus mucosa and soft tissue lesions , it is inferior to ct in evaluating sinus walls and bony structures in paranasal sinus to completely replace ct . 
on the other hand , there has been a lot of effort both in hardware and software to reduce radiation dose while maintaining clinically acceptable image quality in ct [ 4 , 13 , 14 ]  . 
recently , a full model - based iterative reconstruction ( mbir ) algorithm ( commercial name is veo ( r ) , ge healthcare , waukesha , wi ) that incorporates the noise model and the optical model of the whole detection system for significantly decreasing image noise and improving spatial resolution at the same time has been introduced [ 15 , 16 ]  . 
the purpose of this study was to evaluate the clinical application of mbir algorithm in the 80kvp low potential and the ultra - low - dose paranasal sinus ct imaging of children . materials andmethods this study was approved by the ethics committees of our hospital , and written consent was obtained from the parent of each patient in the second phase . 
the first phase was to evaluate the noise reduction capability and the clinical acceptability of mbir images in ultra - low - dose ct imaging using the existing ultra - low - dose ct dacryocystography ( dcg ) scan data reconstructed using both mbir algorithm and traditional filtered back - projection ( fbp ) algorithm , and comparing their image noises . 
the mbir images were also compared with the images of 21 standard - dose paranasal sinus ct patients reconstructed with adaptive statistical iterative reconstruction ( asir ) algorithm for objective and subjective image quality measurements in paranasal sinus . 
in the second phase , 14 tumor patients who came for follow - up sinus ct scan were prospectively enrolled with reduced radiation patient selections andct examinations feasibility study ofmbir inultralowdose ct ofparanasal sinuses we retrospectively selected 16 children ( male : female = 12 : 4 ; age 2321months , range 4months8years ) who suffered from nasolacrimal duct obstruction and underwent ultra - low - dose ct dacryocystography from may 2012 to june 2013 in our institution . 
meanwhile , 21 paranasal sinus patients ( male : female = 10 : 11 ; age 6634months , range 12months12years ) who underwent the standarddose ct and adaptive statistical iterative reconstruction ( asir ) from may 2012 to august 2012 were used as control group for comparison . scan parameters for the ultra - low - dose ct dacryocystography ( dcg ) group were as follows : tube voltage of 80kv , fixed tube current of 80ma , gantry rotation speed of 0.8s , and pitch of 1.375 , beam collimation of 640.625mm for a 40mm total coverage in a single rotation . 
scan parameters for the standard - dose paranasal sinus group were as follows : tube voltage of 120kv , automatic tube current modulation ( atcm ) of 10350ma for obtaining a noise index ( ni ) of 14hu , gantry rotation speed of 0.8s , and pitch of 1.375. 
the standard reconstructions kernel was used in both the fbp and asir reconstructions , without any additional filters . validation withfollowup scans fourteen pediatric patients ( male : female = 9 : 5 ; age range 211years ; median age , 7years ) with tumors ( lymphoma , n = 12 ; langerhans cell histiocytosis , n = 2 ) for follow - up paranasal sinus ct from july , 2013 to june , 2014 in our institute were prospectively enrolled with reduced radiation for ct scans and image reconstruction with mbir algorithm ( group a )  . 
observers were allowed to adjusting the window width and level based on their own viewing habits . subjective image quality assessment a 5 - point scale ranging from 1 ( worst ) to 5 ( best ) was used . 
 overall image quality was subjectively assessed in terms of the subjective image noise , low contrast resolution of sinus mucosa , and the ability to display ostiomeatal complex and sinus bone walls ( 5 : minimum noise , excellent contrast , clearly displayed bony structures , and walls with sharp boundary ; 4 : low noise , good contrast , well - displayed bony structures , and walls with good boundary ; 3 : moderate noise , good contrast , recognizable bony structures , and walls with acceptable boundary ; 2 : high noise , low contrast , bony structures , and walls are with blurred boundary and cannot be easily identified ; 1 : severe noise , low contrast , structures , and walls cannot be identified )  . 
images with scores equal or greater than 3 were considered acceptable . objective image noise measurement ct number and its standard deviation ( sd ) on the sphenoid and the adjacent temporal muscle were measured using a centrally located circular region of interest ( roi ) with areas of 2030mm2 . 
the weighted sum of the standard deviations of the sphenoid and the temporal muscle was used to represent image noise , contrast noise ratio ( cnr ) was calculated as follows : cnr = ( ctnumber ( bone ) ctnumber ( muscle ) ) sqrt ( ( sd ( bone ) 2 + sd ( muscle ) 2 ) 2 )  . for tumor patients , the thickness of maxillary sinus was measured by the two radiologists together . radiation dose the displayed dose indicators : volumetric ct dose index ( ctdivol ) and dose length product ( dlp ) were recorded at the end of each examination . 
unfortunately , we do not have the data for the accuracy of ctdivol measurement , the accuracy of the reported ctdivol values was verified using the latest quality check report . 
the actual measured ctdivol value was 6.0% higher for the conventional ct scans using 120kv , and 1.2% higher for the ultra - low - dose ct scans using 80kv . 
other quantitative measurements were compared using the independent samples t test , and qualitative measurements using mannwhitney test to determine the significance of differences between groups and differences were assumed significant only when the p value < 0.05. 
 mbir increased subjective image quality especially in ostiomeatal complex , providing excellent contrast between turbinate structures and surround mucosa , compared with the fbp reconstruction for the same data set . 
there was good agreement in terms of the subjective image quality scores between the two doctors with kappa = 0.67 , p < 0.05. bone and soft tissue compared with the asir reconstruction in the standard - dose group ( p < 0.05 ) , cnr increased by 80.0% and provided the same thickness measurement of 1.50.2mm for the maxillary sinus wall as the standarddose group . 
various dose reduction methods , such as the use of high pitch value [ 18 ] , low tube voltage and tube current [ 19 ] , and iterative reconstruction algorithms [ 20 , 21 ] , have all been evaluated . 
1 a , b axial and coronal views of the mbir images of a 7 - year - old girl with left lacrimal duct obstruction , respectively , acquired using - dose scan parameters of 80kv / 80ma / 0.8s / and pitch of 1.375 with ctdivol of 1.09mgy ; c , d axial and coronal views of the fbp reconstructions acquired using the same scan protocol as a , b . 
 e , f axial and coronal views of the 30%asir images of a 7 - year - old boy with headache for 10days ; standard scan parameters were as follows : 120kvp , automatic tube current modulation for a noise index of 14hu , gantry rotation speed of 0.8s , and helical pitch of 1.375 with ctdivol of 3.2mgy. 
in a , b , contrast agent is visible in the left lacrimal sac on the left side , and entering into the right nasal meatus through the nasolacrimal duct . 
c , d have worse than acceptable image noise and the structures of ostiomeatal complex are not clear enough model - based iterative reconstruction ( mbir ) algorithm produced excellent image quality in terms of low image noise and high spatial resolution under extremely low radiation dose ( < 0.1msv ) for paranasal sinus ct imaging of children . with the average photon energy closer to the k - edge of contrast medium ( iodine ) and bones , low tube voltage ( 80kvp in our system ) is advantageous in bringing out the contrast between bony structures and surrounding tissues , and is one of the ways to reduce radiation dose requirement while maintaining adequate contrast - to - noise ratio for bony structures . 
in the mbir images , noise in the soft tissue is decreased ( arrow head ) , and tiny bones with osteoclasia ( b with two arrows ) are displayed more clear than in d we first evaluated the low - dose performance of mbir algorithm using the existing extremely low - dose scan data from ct dacryocystography examination of pediatric patients in our hospital . 
 due to its unique clinical purpose , extremely low - dose ct scans are normally applied , providing us with an excellent opportunity to evaluate paranasal sinuses in extremely lowsignal imaging conditions , and used as sample for assessing the methodology , implying the use of contrast obviously may allow low dose for the difference in density of soft tissue and opacified tissue . 
by comparing the mbir images of the ct dacryocystography scans with that of the standard - dose paranasal sinus examination , we demonstrated that even with 63.9% lower radiation dose ( ctdivol ) , mbir further reduced images noise by 39.9% and increased cnr by 63.6% with clear boundaries for bony structures . the ability of mbir algorithm to reduce image noise and improve spatial resolution in an extremely low - dose imaging situation was further validated using the scan data of followup paranasal sinuses patients who were in a stable period after chemotherapy that required follow - up examination . 
mbir images from the extremely low - dose scan fully satisfied the diagnostic needs , and judging from the significant image noise reduction with mbir algorithm , combine with low tube voltage , we speculate that it is possible to further reduce the required radiation dose in paranasal sinus ct scan . our study did have limitations . 
first , the sample size was relatively small and the age distribution was skewed , due to the fact that ct dacryocystography examination only applies to patients with no obvious effect under treatment , and the extreme - low - dose follow - up scans were only given to tumor patients who were in stable period after chemotherapy to avoid misdiagnosis and wrong diagnosis , future studies should use more detailed radiation group based on the age of children [ 22 ]  . 
second , the spectrum of disease was limited , and we did not consider the impact of sinusitis , rhino polypus , or other diseases on the display of sinus . 
third , some new ct scanners offer 70kv tube voltage ; it may be more suited for pediatric para - sinus exafourth , this research was aimed to the application of 80kv low - dose scan combined with mbir , but did not pay close attention to the routine asir reconstruction protocol for diagnostic centres with equipment without mbir . 
increasing the asir percentage or the noise index and lowering the maximum ma value are some of the options to further reduce radiation dose without adversely affecting image diagnosis . finally , because there was no recon kernel in mbir algorithm , and higher spatial resolution reconstruction options were not explored , the impact of applying additional highresolution enhancement on images and clinical diagnosis needs to be investigated further . acknowledgements we are grateful to all subjects and their family members for their cooperation in providing clinical information for the study . 
we would like to express our sincere thanks to jianying li and ning guo for their technical support in understanding the model - based iterative reconstruction algorithm and in editing the manuscript . compliance with ethical standards funding this study was supported by the beijing childrens hospital young investigator program ( grant numbers bch - yipb - 2016 - 06 ) and clinical technology innovation project of beijing municipal commission ( grant numbers xmlx201407 )  . conflict of interest the authors declare that they have no conflict of interest . ethical approval the present study was approved by the ethics committee of beijing childrens hospital . 
severe outcomes may be observed even in the face of negative cts . keywords baggie body stuffer abdominopelvic ct methamphetamine poisoning abbreviation met methamphetamine computed tomography emergency department gastrointestinal introduction drug smuggling has nowadays increased worldwide compared to previous decades [ 13 ]  . 
body stuffing and packing are emergencies in general medicine accompanying with a rather high mortality and morbidity , especially if the diagnosis is not made in time and treatment given is not appropriate [ 4 , 5 ]  . the term body packers is used for the individuals who smuggle illicit drugs using their body cavities . 
therefore , on - time diagnosis of the patients with history of ingestion of amphetamines / met may affect their prognosis [ 8 , 9 ]  . due to relatively large size and number of packets in the body packers , even the plain abdominal radiograph may be diagnostic in up to 80% of the cases [ 10 , 11 ]  . 
however , in body stuffers , the baggies are less in number and smaller in size limiting the efficacy of abdominal radiography in diagnosis and mandating more evaluation with abdominopelvic computed tomography ( ct ) scanning . 
apart from variable and relatively low sensitivity and specificity of ct in detecting body stuffers , clinical significance of observing one or more foreign bodies or a questionable leak in the gi tract in ct scan of the suspects is rather unknown [ 9 ]  . 
to the best of our knowledge , no study has evaluated the relation between ct findings and patients clinical manifestations in met body stuffers which was the main goal of the current study . materials andmethods study design andsettings in a routine data base census study , hospital files of the patients referring with the history of met body stuffing ( solely or in combination with other drugs ) between december 2012 and july 2014 were evaluated in the biggest academic tertiary poison hospital of the world with an annual ed census of more than 24 , 00028 , 000 and nearly 12 , 00014 , 000 hospital admissions [ 1315 ]  . 
a data sheet containing demographic characteristics ( age and gender ) , time of ingestion and amount of the substance in the baggie , history of addiction , signs and symptoms on presentation , lab test results ( on - arrival and maximum measures during hospitalization ) , urine screening tests , results of abdominopelvic ct , number and place of the packs in ct , treatment performed , hospitalization period , and final outcome was filled for every single patient . 
all recorded complications including brain hemorrhage and mortality were also searched . selection ofparticipants diagnosis was made based on the patients self - claim and confirmed by positive urine test results ( if any ) or expulsion / removal of the baggies / their covers . 
those with hypertensive urgency ( systolic blood pressures above 180mmhg or diastolic blood pressure above 120mmhg ) and any end organ damage were put in the severe - outcome group . 
end organ damage was defined as seizure , decreased level of consciousness mandating intubation , rhabdomyolysis [ creatine phosphokinase ( cpk ) > 5000 u / l ] , increased troponin ( > 0.1ng / ml ) , doubling of the level of creatinine , increased liver transaminases ( > 1000 u / l ) , hyperthermia ( t > 40c ) , [ 16 ] or death . study protocol the patients had undergone abdominopelvic ct without contrast using a 16 - row ct scanner ( activion 16 , toshiba , japan ) , with following parameters : automated ma tube charge , tube potential of 120kv and pitch factor of 1.4. 
 images were reviewed in a local pacs ( picture achieving and communication system ) software ( medal electronic workstation , tehran , iran ) in abdominal and lung windows by a board - certified radiologist with 4years of experience in abdominal imaging and a senior radiology resident with focused training on abdominal ct of suspected drug smugglers , who were blinded to the clinical results . 
in cases of non - agreement , the cts were double - checked and a consensus was finally made . suspected body smuggling n = 149 suspected body stuers n = 124 conrmed body stuers n = 113 conrmed met body stuers n = 70 body packers / pushers n = 25 not conrmed n = 11 other stuers except met n = 43 fig . 
 compliance withethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
irb of institution waived the requirement for informed consent in data base studies . the data were analyzed using statistical package for social sciences ( spss ) version 18 and stata software ( version 6.0 ) using mannwhitney u test , t test , chi - square test , z test , and fishers exact test . 
a p value less than 0.05 was considered to be statistically significant . results in a total of 70 patients , mean age was 31.79.1years ( range 1563years ) and 95% were male . 
thirty - six ( 51.4% ) had been referred by police force and the remainder had referred themselves due to fear of toxicity after they had hidden baggies and misled police but had not expelled their baggies . 
2 axial ct section in abdominal window ( a ) depicts a round mildly hyperdense baggie in gastric antrusurrounding hypodense halo secondary to trapped air underneath the cover is better appreciated in lung window ( b ) statistical analysis fig . 
ct study in next day ( b ) confirms the passage of packet to distal bowel loops in right pelvis study outcome computed tomography results were reported to be positive in the presence of well - defined baggies with ( fig.2 ) or without ( fig.3 ) surrounding air halo . 
in 40 ct - negative patients , four reported expulsion of the baggies , five mentioned that they had not expelled their baggies , and 31 did not give reliable history on the subject . 
 baggies were retrieved in one while in the other one , surgical intervention was unsuccessful . in total , 63 patients were discharged symptom - free ( 27 with positive and 36 with negative cts )  . 
in the 30 patients with positive cts , number of the baggies was determined in 21 and there was evidence of baggies leakage in nine cases . eight , six , three , one , and three patients were diagnosed to have one , two , three , four , and six baggies , respectively . 
detecting swallowed baggies even by the costly imaging techniques ( i.e. , abdominopelvic ct scan ) is difficult because they are usually very small , radiolucent , and obscured by food in the gastrointestinal tract . 
using amphetamines may result in euphoria , anxiety , psychosis , muscular stiffness , mydriasis , fever , perspiration , tachycardia , hypertension , seizure , and cardiovascular collapse [ 17 ]  . 
a thorough physical examination is , therefore , recommended in the body stuffers [ 18 , 19 ]  . ct findings of the met body stuffers are seldom reported [ 20 ]  . 
the onset of clinical toxicity is usually rapid following ingestion of poorly packaged substance ; this is in contrast to the body packers whose symptoms may take a long time to manifest . 
 although the risk of radiation due to ct imaging and clinical benefit are challenging in body stuffers , diagnosis of body stuffers from packers is a difficult task in patients who even deny ingestion of the pack / baggie . 
in nine patients , no obvious packet was detected but hyperdense content mixed with food material was revealed which might imply leakage and rupture of the baggies due to their loose coverage . 
it is also concluded that small isodense pellets may be missed in ct scan due to lack of clear surrounding bag and similarity to the normal contents of the abdomen . 
experience of the radiologists , team work between the radiologist and toxicologist , using advanced equipments , grade of compression , substance form , coating , and packing process are the main factors affecting the detection rate [ 21 ]  . physicians are usually interested in following the baggies by serial x - rays or cts to be assured about their safe passage . 
most patients have met packets either in their stomach ( and perhaps treatable with activated charcoal ) or in the large intestine , and therefore close to expulsion and perhaps treatable with polyethylene glycol . 
serial cts may assist them in determining the best method of treatment including whole bowel irrigation , activated charcoal or even endoscopy for rapid retrieval of the baggies [ 22 ]  . 
no statistically significant difference was detected between the two ct - positive and ct - negative groups regarding their 1 3 radiol med ( 2018 ) 123 : 98104 period of hospitalization , time and amount of the ingested substance , clinical findings , intubation , vital signs , lab test results , and urine screening tests . 
surgical intervention is less common in body stuffers in comparison to packers , although fatal complications may occur even through inhalation as well as ingestion [ 3 , 24 ]  . as shown , severe - outcome patients had more negative ct results . 
this means that ruptured baggies are less likely to be detected by the radiologist while they make the patient symptomatic and put him / her in the severe - outcome group , although we could not prove this hypothesis by statistical analysis . 
this is in accordance with our previous studies which showed a sensitivity of 37.555% for ct without contrast in detection of the body stuffers [ 17 , 25 , 26 ]  . 
 we could find pulse rate as a correlating factor like they found , but we also found ldh , hco3 , be , agitation and loss of consciousness as other probable effective factors in univariate analysis . 
they believed that detecting the ingested baggies using imaging modalities might not be a reliable end point for treatment [ 10 ]  . almost 37% of our patients were in the severe - outcome group which is a higher proportion in comparison with the previous studies [ 10 , 24 , 26 , 27 ]  . 
we are working in a main referral center with more complicated patients referring from other hospitals defining the fact that most of our cases were in the severe - outcome group [ 13 ]  . some studies have introduced ct as a sufficient method of diagnosis in the body stuffers . 
in machine packaging , halos are formed around the packets making detection easier and more reliable while in our cases , baggies were packed manually and covered by a thin plastic sheet making the diagnosis difficult or impossible especially in hypoor iso - dense packets and the baggies prone to leak or rupture . 
our patients , therefore , presented with more severe clinical symptoms albeit with negative ct results . it seems that many factors including ct type and window level may affect the results of ct in these patients . 
in the current study , content of the baggies was methamphetamine solely or in combination with other illicit drugs with a wide range of density ( 12670hu )  . limitations the few sample size and retrospective nature of the study were definitely major limitations of the current study . 
also we would not expect heroin , opium , methadone and other substances which were found to be ingested by some met body stuffers to have the same symptoms . ct scans had been performed with slice thickness of 10 and 7mm which limits the detection of sub - centimeter baggies and partially explain our low sensitivity in body stuffers compared to other limited studies with higher sensitivity . 
 although our study is the first one to evaluate the relationship between the ct findings and clinical manifestations of the methamphetamine body stuffers , future studies on larger sample sizes are warranted . 
the type and total dose of the drug ( s ) , the time from stuffing to presentation and the type of packing ( i.e. , secure bag vs no wrapping or loose plastic ) were not available in recorded documents in which they may influence outcome . there is no gold standard test or method to detect baggies in body stuffers . 
lack of confirmatory assays for methamphetamines in 83% of the patientsbased on the histories that can be unreliableis another limitation , although urine toxicology screening tests are also fraught with positive results . 
the clinical effect of the drug ingested ( i.e. , sympathomimetic ) may describe ct findings in these patients and provide a correlation between ct imaging and severe clinical outcomes . conclusion it seems that there is no relation between ct findings and clinical manifestations of the methamphetamine body 1 3 104 radiol med ( 2018 ) 123 : 98104 stuffers . 
also , ct scanning cannot be relied on for diagnosis and determination of the prognosis in body stuffers . acknowledgements this article has been extracted from the thesis written by hedie zamini in school of medicine , shahid beheshti university of medical sciences ( registration no 340m - 2015 )  . 
pi - rads score was correlated with the histological results , divided in three groups ( benign tissue , atypia and carcinoma ) and with gleason groups , divided in four categories considering the new grading system of the isup 2014 , using t test . 
the first application technique , introduced for the first time in 1989 [ 4 ] , was a single biopsy of a target nodule identified by ultrasound examination [ 5 ]  . 
the current standard technique for a prostate biopsy is random transrectal ultrasound ( trus ) - guided needle insertion , which consists of taking from 10 to 14 cores ; this approach leads to a cancer detection rate that ranges from 27 to 40.3% [ 6 , 7 ]  . however , this methodology is not completely accurate and presents several limitations . 
trus biopsy yields upgrading of pca in at least 25% of patients : identification of microfocal cancers of little clinical significance determines a potential problem in men with suspect pca , which could undergo unnecessary surgical treatment [ 8 , 9 ]  . 
on the other hand , standard trus biopsy undersamples sites far from the needle access ( anterior gland ) , and false negatives are represented by nearly 35% of cases [ 10 ] [ 11 ]  . magnetic resonance imaging ( mri ) [ 12 , 13 ] is recommended by the european association of urology ( eau ) , national comprehensive cancer network ( nccn ) and european society of urogenital radiology ( esur ) guidelines in patients with persistently elevated or incremented psa levels , and / or previous negative biopsies . 
the aim is to evaluate the gland and identify lesions which could undergo target biopsy [ 14 , 15 ] , in a population including men in active surveillance programs ( as )  . 
on the other hand , with mri - targeted biopsies , the detection rate of insignificant cancers , are lower than with systematic blind biopsy [ 20 ]  . the combination of mp - mri images with ultrasound real - time techniques allows for the integration of the high radiol med ( 2018 ) 123 : 143152 sensitivity and negative predictive value given by mp - mri with the advantages of transrectal ultrasound [ 20 ]  . despite the large volume of literature describing the different techniques used to detect and confirm prostate cancer , there continues to be great attention on how to obtain optimal results by selecting the most suitable diagnostic tool . 
in this sense , the aim of this study was to evaluate the performance of mp - mri in the detection of prostate lesions and the characterization of the malignant ones , as determined by correlating such data with histological findings obtained through ultrasound fusion biopsy . 
we also performed prostatic sampling through trus - guided random biopsies to analyze false - negative cases and identify in which cases mpmri could be inaccurate . materials andmethods in this retrospective study , approved by the ethical committee of the campus bio - medico university where patients were tested , we evaluated 96 prostate mp - mri examinations which were performed at the department of radiological sciences for biochemical or clinical suspects of pca , between october 2015 and june 2016 . 
all patients were biopsy nave . mp - mri examinations were performed using a 1.5t scanner ( magnetom aera siemens erlangen , germany ) by positioning a dedicated six - channel body coil over the pelvis , with the patient in the supine position . 
the contrast agent , gadobenate - dimeglumine ( multihance ; bracco imaging , milan , italy ) , was administered in a concentration of 0.2mmol / kg ; it was injected with an automatic injector through a 20 1 3 radiol med ( 2018 ) 123 : 143152 g intravenous cannula at the rate of 4ml / s , followed by infusion of 15ml saline solution at the same speed . 
axial t1 - weighted vibe fat suppressed sequence . technical parameters for each sequence are summarized in table1 . each exam had a duration of 31.467.2min. following image acquisition , the exams were transferred to a dedicated workstation ( syngo.via , siemens , erlangen , germany ) ; each mp - mri exam was preliminarily evaluated by two experienced radiologists , and the prostate suspicious lesions were identified . all lesions were classified using the pi - rads version 2 lexicon [ 21 ] , on the basis of morphological and functional findings . pi - rads version 2 uses a 5 - point scale based on the likelihood that a combination of mp - mri findings on high resolution t2 - weighted ( t2w ) , diffusion - weighted mri ( dwi ) , and dynamic contrast - enhanced mri ( dce ) correlates with the presence of a clinically significant cancer for each lesion in the prostate gland [ 18 , 22 ]  . all the patients with a suspicious prostate cancer lesion ( pi - rads 4 and 5 and pi - rads 3 , sustained by significant clinical data ) underwent mri - trus fusion biopsy . 
following assessment by dedicated radiologists , the mp - mri exams were stored in a cd - rom , imported on the navigation system ( urostation koelis , grenoble , france ) and fused with real time ultrasound images . during trus scanning , an acquisition of a transverse section of the prostate was locked and the corresponding axial mp - mri image was identified , using three anatomical target points as reference : prostate apex , base and posterior edge . 
the movement of the us endorectal probe was synchronized with the mp - mri images which could also be adjusted in the 3d volume to correspond to us images even in oblique plans . the biopsies were performed on the mri / us fusion target lesions , previously identified on mp - mri images , and on other 12 random cores ( cranial right , basal right , equator 1 right , equator 2 right , caudal right , apex right , cranial left , basal left , equator 1 left , equator 2 left , caudal left , apex left ) an average of four cores were obtained for each target lesion biopsy . 
the obtained samples were analyzed by a pathologist with at least 10years of experience . based on cell morphology and dysplasia grading , lesions were histopathologically classified in three groups : malignant lesions , atypia or high - grade prostatic intraepithelial neoplasia , and benign prostate tissue [ 3 , 23 ]  . for the histological pattern classification of malignant lesions , we considered the international society of urological pathology ( isup ) 2014 consensus conference on gleason grading of prostatic carcinoma , which split the gleason score of 7 into two groups , 3 + 4 ( called group grade 2 ) versus 4 + 3 ( called group grade 3 ) ; we based this criteria on the current data which indicate a worse prognosis for the second group [ 24 ]  . 
student t test was used to compare psa values , lesions maximum dimensions and lesions gleason median value of this group with psa value , lesions maximum dimension and lesions gleason median value of pca identified by mp - mri ( true - positives )  . statistical significance was set at p < 0.05. 
the mean value of pi - rads was 4.41 ( sd = 0.60 ) for group a , 3.61 ( sd = 0.87 ) for group b , and 3.24 ( sd = 0.81 ) for group c , as shown in fig.1. the differences between group a and group b , between group b and group c , and between group a and group c were statistically significant . the median gleason score of cancer - positive targets was 3 + 4 ( range , 3 + 3 to 4 + 5 ) in group a . 
the only statistically significant difference was found between group 1 and group 4 . for carcinoma lesions , the median psa correlated to the gleason score as follows : 5.65ng / ml ( range 1.110.5ng / ml ) in gleason group 1 ; 6.15ng / ml ( range 2.411.2ng / ml ) in gleason group 2 ; 6.72ng / ml ( range 0.2916.3ng / ml ) in gleason group 3 ; and 13.19ng / ml ( range 4.0735.5ng / ml ) in gleason group 4 . the only two groups of patients showing a significantly different median value of pi - rads were the ones with a low psa level and gs7 , and with high psa levels and gs > 7 . 
no statistically significative difference was observed in pi - rads median value between the group with low psa and gs > 7 and other groups , neither was it found between groups with high psa and gs7 and other groups . 
therefore , in the past couple of decades , in literature , a tendency to increase the number of cores was expressed , to sample undetected foci of carcinoma and reduce the false - negative rate . 
yet the evaluation of detection rates of 18 - , 20and 24 - random cores prostatic biopsies , besides the advantage of a more accurate cancer detection rate [ 2628 ] , demonstrated an increase of risks and complications ( such as bleeding , urinary obstruction , vasovagal reaction and infection )  . 
 the population marginal means of groups 0 , 0 and 1 , 1 were significantly different ( bonferroni test ) score as follows : 11.94mm ( range 620mm ) in gleason group 1 ; 13.22mm ( range 527mm ) in gleason group 2 ; 15.57mm ( range 730mm ) in gleason group 3 ; and 20mm ( range 935mm ) in gleason group 4 . the only two groups showing a statistically significant different pi - rads median value were the groups with a smaller diameter and gleason7 and the group with a larger diameter and gleason > 7 . 
no statistically significant difference was observed in pi - rads median value between the group with smaller diameter and gleason > 7 and other groups , or between the group with larger lesions and gleason7 and other groups . 
the lesion demonstrates high si on the high - b - value image of the dwi ( b ) ( arrow ) , low adc value ( c ) ( arrow ) , strong contrast enhancement ( d ) with early and high peak enhancement with washout on the dce curve ( e )  . 
the histological result of mp - mri / us guided biopsy of target lesion confirmed a gleason 8 ( 4 + 4 ) pca we also demonstrated that the pi - rads scores correlate with microscopic features of cancer lesions , based on gleason classification , with the best capability to distinguish very aggressive lesions ( gleason > 7 ) from slightly aggressive lesions ( gleason < 7 )  . 
the performance of mpmri , expressed in term of pi - rads score , decreases in the evaluation of carcinoma with intermediate behaviour , classified as gleason 7 ( group grade 2 and group grade 3 )  . 
in agreement with the literature [ 3133 ] , gleason 7 carcinoma harbors an element of high - grade pattern carcinoma , and it is intermediate in clinical aggressiveness between patterns group grade 1 and group grade 4 and 5 . 
6 mri prostate exam in a 64 - year - old man with a psa of 3.5ng / ml ( increasing from 1.1 in 1year ) and two negative prior biopsies . 
the histological result confirmed a gleason 6 ( 3 + 3 ) pca demonstrated that all men with gleason less than 7 and many men with gleason 7 ( 3 + 4 ) could be considered low grade cancer and could be object of active surveillance or radical prostatectomy without requiring pelvic lymph node removal , due to low risk of diffusion . 
on the other hand , men with a gleason greater than 8 have been considered high risk patients , with higher recurrence percentage , requiring a more aggressive therapeutic choice , such as radioor 1 3 150 radiol med ( 2018 ) 123 : 143152 chemotherapy . 
we investigated the cause of mp - mri limits and the cases in which mp - mri missed pca lesions identification . therefore , once mp - mri detectability was assessed and true positives were analyze , histological results by mp - mri / us guided target biopsies and histological results by us random sampling core biopsies were compared and mp - mri false negative lesions behaviour were analyzed . several studies have found that mri / us - fusion biopsy detect pca in 3437% of patients with prior negative trus biopsies , with one - third of these patients harboring highgrade cancer as defined by a gleason score > 7 [ 36 ]  . prostate cancer is considered multifocal , small , intermingled with benign stroma , and not uniformly distributed within the gland cancer . 
demonstrated that the combination of random us - guided and target mp - mri / us fusion - guided biopsies doubled the detection of insignificant pca , when compared to target mp - mri / us fusion - guided alone [ 29 ] , on the other hand , bjurlin etal . 
showed that a biopsy strategy combining random us - guided with mp - mri / us - fusion biopsies can also increase the detection rate of significant pca , when compared to mp - mri / us - fusion biopsy alone [ 37 ]  . 
in our study , 40 / 1152 ( 3.49% ) cores of the random sampling usguided biopsies showed the presence of carcinoma , that was otherwise missed on mp - mri examination . 
the data analysis from this group of patients , showed that only one target lesion was identified at mp - mri exam , and a lower psa value and lower target lesion maximum diameter were demonstrated , compared to psa level and target lesion maximum diameter of the rest of the population . in agreement with a recent review , our results showed that mp - mri detectability is higher for more clinical aggressive lesions [ 37 ] , since these have a higher metabolism as well as speed of growth , which are parameters directly related to psa serum level increase and lesion dimension . analyzing histologic behaviour of these microfoci of carcinoma , undetected on mp - mri exams , we demonstrated that they did not have a gleason score greater than the gleason of mp - mri identified lesions . 
this data is consistent with recent findings from a large prospective study which showed that mri / us - fusion biopsy can detect as many gleason 7 or greater tumors , while simultaneously avoiding the detection of 44% of lower grade disease [ 29 ]  . this study has some limitations . 
second , the study population was relatively small and the gleason subgroups were not equal in number , with a greater number of lesions in the patient group with a gleason score of 7 and this may have influenced the accuracy of pi - rads statistics . 
however , patients rate for each group is representative of general population and in accordance with other recent works . our findings suggest that us / mp - mri fusion biopsy represents the elective method to perform prostatic biopsy in a safe and efficacy way and that the pi - rads score significantly correlates with prostatic lesions aggressiveness . 
type 1 and 2 cysts were treated using pair ( puncture , aspiration , injection , respiration ) and single puncture catheterization methods ; type 3 lesions were treated using a modified catheterization technique . 
 alcohol was used as a scolicidal and sclerosing agent in all procedures . results after excluding three lesions ( 0.5% ) because of lack of parenchymal support during catheterization , 274 ( 49.7% ) , 250 ( 45.3% ) , and 27 ( 4.9% ) of 551 lesions were treated with pair , single puncture catheterization , and modified catheterization techniques , respectively . 
ce generally targets the liver ( 5070% ) and may occasionally affect other organs such as the lungs ( 530% of cases ) , spleen , kidneys , bones , brain , heart , adrenal gland , ovary , and thyroid gland [ 2 , 4 ]  . ce is mainly treated with surgery , which is invasive and associated with high morbidity and mortality rates and longer hospital stays [ 1 , 5 ]  . 
however , minimally invasive approaches have been developed within the last 2 decades ; these include percutaneous treatments with excellent results and lower mortality and morbidity rates [ 510 ]  . 
forty - two hydatid cysts in thirty - four patients were excluded , because the patients follow - up duration was shorter than 6months . all hydatid cysts were evaluated using ultrasonography ( us )  . 
both criteria used for cyst hydatid lesions are described in table1 . preprocedure evaluation after obtaining written informed consent , albendazole was orally given at a dose of 10mg / kg / day for 10days before and 2weeks after the percutaneous procedure as prophylaxis to decrease the risk of secondary dissemination . 
diphenhydramine hcl ( 20mg ) and methylprednisolone ( 1mg / kg ) were administered intravenously to all patients to prevent allergic reactions and decrease the risk of anaphylaxis . radiol med ( 2018 ) 123 : 153160 procedure all nonvascular interventional procedures were performed by two interventional radiologists with 8 - year experience . 
 percutaneous treatments were performed under us and c - arm fluoroscopy guidance ; specifically , after administering local anesthesia ( prilocaine hydrochloride ) under locally sterilized conditions , targeted lesions were determined and punctured under us guidance . 
ce type 1 ( gharbi type 1 ) and type 3a ( gharbi type 2 ) hydatid cysts < 6cm were treated via pair ( puncture , aspiration , injection , and respiration ) , whereas cysts > 6cm were treated via single puncture catheterization ( spc )  . 
all ce type 2 and 3b ( gharbi type 3 ) cysts underwent the modified catheterization ( mocat ) technique . during pair , ce lesions were punctured with 18 - g needles , and nearly 50% ( calculated from us measurements ) of the fluid volume were aspirated from the cyst pouch . 
cyst completeness and associations with adjacent structures were then evaluated by injecting contrast agent ( sodium amidotrizoate , urografin , bayer ) as much as 1020% of volume ( calculated from us measurements ) into the cyst cavity under fluoroscopic guidance until the cyst contours became definite . 
the cavity was re - aspirated and filled with a mixture of absolute alcohol ( 98% alcohol , approximately 3050% of aspirated cavity volume ) and contrast agent ( approximately 1020% of the aspirated cavity volume )  . 
 after waiting for 710min to observe endocyst detachment from the pericyst , the injected alcohol was re - aspirated . for spc , the cyst was punctured through an 8f catheter ( bioteq , taipei , taiwan ) using a trocar method under us guidance . 
the cavity was reaspirated and filled with a mixture of absolute alcohol ( 98% alcohol , approximately 3050% of aspirated cavity volume ) and contrast agent ( 10% cyst volume )  . 
after 710min , the cyst cavity was re - aspirated , and a catheter was affixed to the skin . table 1 world health organization and gharbi classifications of hydatid cysts who classification describing features gharbi classification ce type 1 ce type 2 ce type 3a ce type 3b ce type 4 ce type 5 type 2 type 3 type 2 type 3 type 4 type 5 univesicular cyst with visible cyst wall , mobile echogenicities ( hydatid sand ) multivesicular and multiseptated cyst containing daughter cysts , honeycomb pattern univesicular cyst with unattached and loose membranes ( water - lily sign ) cyst containing daughter cysts in solid matrix cyst containing hypoechoic / hyperechoic partially solid matrix , no daughter cysts cyst containing solid matrix with thick and calcified wall who world health organization - informal working group , ce cystic echinococcosis status active active transitional transitional inactive inactive 1 3 radiol med ( 2018 ) 123 : 153160 for mocat , the lesion was punctured with a 14f catheter ( bioteq , taipei , taiwan ) via the trocar method under us guidance . 
after nearly 20min , the cyst cavity was re - aspirated , and the catheter was affixed to the skhowever , if residual daughter vesicles were detected on cavitographic images , irrigationaspiration procedures were repeated the following day until these vesicles were completely eliminated . 
 catheters were removed when the amount of fluid drained from the cavity decreased to < 10ml per day . followup all patients were subjected to follow up us at the 1st , 3rd , 6th , 9th , and 12th months after the first procedure and annually thereafter . 
decreased cyst size and volume , increased cyst wall thickness and echogenicity , complete endocyst detachment from the pericyst , decreased fluid content , and a heterogeneous / pseudotumor remnant appearance were considered positive indicators of healing [ 2 ]  . 
recurrence was defined as the absence of a decrease in treated ce lesion size and the formation of new daughter cysts [ 10 ]  . statistical analysis the statistical analysis system 9.4 ( sas university edition version 9.4 ) was used for statistical analyses . 
mean ce lesion diameter was 75.637.5mm ( range : 8260mm ) , and 397 ( 71.6% ) and 157 ( 28.3% ) lesions were localized in the right and left lobes , respectively . 
lesions were detected in the liver only in 323 patients ( 93% ) , whereas extrahepatic organ involvement was present in 24 patients ( 6.9% ; lungs : 18 , spleen : 5 , and uterus - right ovary : 1 )  . percutaneous treatments were successfully applied to 551 lesions ( 99.5% ) , and no percutaneous treatment was administered to three lesions ( 0.5% ) in two patients because of a lack of parenchymal support during catheterization . 
local recurrences were detected in 19 patients ( 5.4% ) within 1year after the treatment and in 17 lesions of 17 patients ( ce type 1 : 15 patients and ce type 3a : 2 patients )  . 
only two major complications , anaphylaxis , were observed in two cases ( 0.5% ) and quickly resolved via immediate intervention by the anesthesiology teano deaths or abdominal dissemination related to percutaneous treatment per se or its complications were recorded . 
 three patients with high - output ( > 300ml / day ) fistulas for > 1week with no sign of reduction were exposed to endoscopic treatment , and endoscopic retrograde cholangiopancreatography was performed in one patient developing hemobilia . 
a 6 - year - old boy developing methemoglobinemia from the local anesthetic agent ( prilocaine hydrochloride ) was treated intravenously with methylene blue . the median duration of catheterization in 250 patients treated with spc was found as 2days ( mean , 3.57.9days ; range , 171days )  . 
the median duration of catheterization in 27 patients treated with the mocat was detected as 2days ( mean , 3.37days ; range , 134days ) , and the median duration in all catheterized patients was found as 2days ( mean , 3.57.8days ; range , 171days )  . mean overall hospital stay was 1.552.3days ( range : 023days )  . 
patients treated with catheterization had hospital stays between 1 and 2days in general , whereas those treated with pair were discharged on the same day after 5or 6 - h observation period . 
follow - up ultrasonography examination at the 6th month after the single puncture catheterization procedure demonstrates complete endocyst detachment from the pericyst , decreased fluid content , and reduction in size ( b )  . 
ultrasonography obtained at the 28th month follow - up after the procedure shows the appearance of pseudotumor number of patients 2 ( 0.5% ) 2 ( 0.5% ) 8 ( 2.3% ) 19 ( 5.4% ) 7 ( 2% ) 1 ( 0.2% ) 1 ( 0.2% ) 36 ( 10.3% ) table 3 type of complications complications major anaphylaxis total minor urticaria biliary fistulas abscess hemobilia methemoglobinemia total discussion percutaneous treatments are more noninvasive and reliable modalities , associated with lower rates of postoperative complications , recurrences and shorter hospital stays should be preferred in treating liver ce lesions [ 2 , 5 , 8 ]  . 
yet , 20% hypertonic saline is recommended not to be used in patients with cysts communicating with biliary tree because of the danger of causing sclerosing cholangitis [ 13 ]  . in percutaneous treatment of hydatid cysts , the scolicidal and sclerosing effect of alcohol that we used as an only endocavitary agent is well known [ 14 , 15 ]  . 
absolute alcohol , known to have a stronger scolicidal and sclerosing effect than 20% hypertonic saline , can be used as a scolicidal agent [ 14 , 16 ]  . 
therefore , we consider that the sclerosing effect of alcohol led to no cholangitis in patients in whom clear cystic content was aspirated during the first puncture , and no biliary leakage was detected during the cavitogram . cyst rupture , leakage , and spillage may lead to allergic reactions most frequently characterized by urticaria , flushing , and swelling of mucous membrane [ 18 ]  . 
in a study performed by kabaalioglu etal . , it was reported that an intercostal approach via liver tissue was used for all right lobe cysts so as to minimize the risk of leakage [ 6 ]  . 
in another study by corona etal . , for decreasing the risk of leakage , a coaxial system composed of a 20 - cm - long fine needle with an outer 10 fr sheath was reported to be used to puncture the cystic cavity [ 20 ]  . 
in our study , among catheterization methods , we use the trocar technique of direct catheterization into the cyst to avoid the risk of the fluid leakage and spillage to the adjacent tissues or abdomen . percutaneous treatments of liver ce can be performed using different methods . 
in our study , depending on the type , size , and location of each lesion , we used different percutaneous treatment methods so as to achieve the highest therapeutic success and lowest complication and recurrence rates . 
we used pair for all ce type 1 ( gharbi type 1 ) and ce type 3a ( gharbi type 2 ) hydatid cysts smaller than 6cm , whereas bigger than 6cm were treated via spc . 
all ce type 2 and 3b ( gharbi type 3 ) cysts were treated mocat technique . the success of percutaneous treatments may vary depending on the type and size of the lesions . 
in that study , the treatment success rates were higher for ce type 1 ( gharbi type 1 ) and ce type 3a ( gharbi type 2 ) lesions than for ce type 2 and 3b ( gharbi type 3 ) and ce type 4 ( gharbi type 4 ) lesions [ 6 ]  . 
we expect that further large - series studies will be performed to clarify the outcomes of percutaneous treatment for ce type 2 and 3b ( gharbi type 3 ) lesions . 
we note that mean initial size of the cysts treated via percutaneous intervention in our study was 75.637.5mm ( range : 8260mm ) , while mean initial size of the cysts was 4.8mm ( range : 2.8200mm ) in the study performed by giorgio etal . 
while a statistically significant decrease was obtained in the size of lesions through all three percutaneous treatment modalities , the decrease in the size of lesions obtained through spc and mocat techniques was higher , compared with that via pair technique . 
 we consider that the reason why the decrease in the size of lesions in pair technique rather than spc and mocat techniques was lower arose from the fact that we used pair for lesions < 6cm . surgical treatments currently remain the standard therapeutic option for such lesions [ 18 , 23 , 24 ] , despite the disadvantages of an invasive method with higher rates of morbidity and mortality , poor cost - effectiveness , associated trauma [ 25 , 26 ] , and contraindications for patients with cardiac or pulmonary disorders [ 24 ]  . 
in a meta - analysis of 769 patients with liver hydatid cysts treated with pair plus albendazole and 952 matched , surgically treated control subjects , smego and sebanegoin found that pair plus chemotherapy was associated with greater clinical efficacy , as well as lower rates of morbidity , mortality , disease recurrence , and shorter hospital stays [ 27 ]  . 
in our study , recurrences were detected in 19 ce lesions ( 5.4% ) , and 17 of 19 lesions were successfully treated following additional interventional procedures ; the remaining two lesions were also surgically treated . 
currently , medical treatment with albendazole and mebendazole is mostly performed to prevent abdominal dissemination and recurrence before surgical or percutaneous treatments ; however , the use of these agents alone provides insufficient outcomes [ 2 , 22 , 24 ]  . 
similarly , all patients in our study were orally administered albendazole at a dose of 10mg / kg / day for 10days before and 2weeks after the percutaneous procedure . 1 3 radiol med ( 2018 ) 123 : 153160 in conclusion , alcohol appears to be safe and effective as a scolicidal and sclerosing agent during the percutaneous treatment of liver hydatid cysts . 
the suspected diagnosis of placental implant anomalies was obtained before surgery because it was based on us and mr acquired in each case ; the post - surgical evaluation gave the confirmation of placental anomalies . 
furthermore , patients with placenta previa major without accretism were involved in the study as reported in table1 and in the results section . regarding the second observation ( secondless effective . ) , it is well known that patients affected by placenta percreta clearly presents higher pph risks and , therefore , the standard surgical approach consider hysterectomy ; indeed in our sample 19 out of 21 patients with this placental anomaly required uterus removal . 
however , as clearly assessed in the introduction section and in our previous published papers [ 3 , 4 ] , the primary goal of this interventional protocol is blood loss reduction and avoidance of the consequential catastrophic events ( as disseminated intravascular coagulation occurring after massive transfusions ) ; uterus preservation is the secondary endpoint and this is also explained to the patients into the informed consent that we submit the day before the procedure . 
so , hysterectomy absolutely does not represent failure of the protocol . finally , as assessed in the manuscript conclusions , we aim that this protocol may represent a technical alternative that interventional radiologists could consider when facing this challenging scenario . 
however , there is still a lack of consensus on which method is preferable in terms of efficacy and costbenefit . purposes we , therefore , asked whether ( 1 ) the benefits in terms of sensitivity and specificity and ( 2 ) the costs were comparable between fluoroscopyand ultrasound - guided joint aspirations in a suspicious of hip pji . methods between 2013 and 2016 , 52 hip aspirations were performed on 49 patients with clinical , radiological , or serological suspicion of pji , waiting for a revision surgery . 
donato milanese , milan , italy results ( 1 ) ultrasound - guided aspiration revealed valid sensitivity ( 89% vs 60% ) and specificity ( 94% vs 81% ) in comparison with fluoroscopic - guided aspiration . 
 the musculoskeletal infection society ( msis ) recently developed a definition for pji based on different criteria [ 1 ]  . in this setting , the role of hip aspiration is of paramount importance for the management of pji . 
hip aspiration can be performed under fluoroscopy ( f ) [ 223 ] , ultrasound ( us ) [ 2426 ] , or , less commonly , computed - tomography ( ct ) guidance [ 27 ]  . 
fluoroscopyguided hip aspiration is the most common and described procedure worldwide ; nevertheless , ultrasound aspiration is gaining popularity , especially for patient safety , because of the absence of x - rays and iodinated contrast agents . 
however , there is still a lack of consensus on which vol :  . ( 1234567890 ) 1 3 radiol med ( 2018 ) 123 : 2835 method is preferable in terms of diagnostic efficacy and riskbenefit for patients . the main purpose of this retrospective study was to compare the diagnostic characteristics ( sensitivity and specificity ) between fluoroscopy and ultrasound - guided hip aspirations in a suspicious of pji . 
because of this primary objective , we compared the results of these preoperative hip aspirations with the results of cultures from multiple intraoperative tissue samples obtained during revision surgery , together with all the other msis criteria , to evaluate the accuracy of these two radiological techniques . 
the costs and pros / cons of these two procedures were also analyzed and discussed . methods a retrospective cohort study comparing two different aspiration techniques for pji diagnosis was performed in collaboration between hip and radiology departments at our institution . patients who underwent hip aspiration between january 2013 and august 2016 before total hip arthroplasty revision ( rtha ) were studied . 
the inclusion criteria were defined as : clinical , radiological , or serological suspicion of pji ; antibiotics suspension at least 3weeks before hip aspiration and revision surgery ; revision surgery after hip aspiration ; informed consent for hip aspiration and revision surgery . all procedures followed were in accordance with the 1975 declaration of helsinki , as revised in 2000 and 2008 . 
 details that might disclose the identity of the subjects under the study were omitted , in accordance with hipaa . fluoroscopy was mostly performed until 2015 ; then , due to different management and policy of health resources at our institutions , ultrasound has been especially used . the patients were so divided in two groups on the basis of the used radiological technique : ( 1 ) fluoroscopyvs ( 2 ) ultrasound - guided hip aspiration . 
each patient of the fluoroscopy or ultrasound group was defined infected ( pji ) or control ( non - infected ) using the msis criteria selected as the gold standard for pji diagnosis . 
based on these criteria , a patient was defined as affected by pji when at least one of the major criteria or four of the minor criteria were satisfied [ 1 ]  . major criteria : revision ; or 1 . 
greater than five neutrophils per high - power field in five high - power fields observed from histologic analysis of periprosthetic tissue at 400magnification . a patient who fulfilled the criteria was considered infected ( pji group )  . 
 therefore , matching the aspiration technique and the presence or absence of infection , each procedural group was subdivided in two subgroups : fluoroscopy - pji group , fluoroscopy - control group , ultrasound - pji group , and ultrasoundcontrol group . the preoperative aspiration of each patient was then compared to the definitive intraoperative multiple cultures ( one of the two major criteria ) and all the other msis criteria to determine the rate of true positive , false positive , true negative , and false negative of both radiological groups ( table1 )  . 
the patient was described as false table 1 correspondence between preoperative hip aspirations and msis criteria for infection after revision group confirmed pji definitive msis criteria positivea control definitive msis criteria negative positive preoperative true + hip aspiration negative preoperative false hip aspiration false + true a patients in the pji group had at least one of the msis major criteria or four of the minor criteria satisfied preoperatively 1 3 30 radiol med ( 2018 ) 123 : 2835 negative if bacterial growth was not reported after preoperative aspiration , but then , the multiple intraoperative cultures or the other msis criteria reported the presence of infection . fluoroscopic aspiration the patient was admitted for a day - hospital procedure for local regulatory laws . 
once the fluoroscopic position of the needle was considered satisfactory , the inserter was removed from the needle and then the vacuum phenomenon caused by the negative intracapsular pressure was appreciated , indicating the intra - articular position . because of its bacteriostatic effect , injection of contrast media ( arthrogram ) was not performed to confirm the intraarticular position of the needle [ 28 ]  . 
routinely , the aspirated fluid was inoculated into two culture blood bottles and two swabs ( containing aerobic or anaerobic liquid enrichment medium ) in sterile conditions . ultrasound aspiration the ultrasound investigation was performed by radiologists with at least 5years of musculoskeletal experience , using a 5 - mhz convex ultrasound probe with puncture guide . 
all samples ( two blood bottles and two culture swabs ) were sent to laboratory for culture . revision surgery during revision surgery , three - to - five samples were obtained from the hip joint and nearby tissues and then transferred to microbiology and cultured for a minimum of 15days . 
 standard microbiological techniques were performed to identify the possible pathogen and determine antibiogram , screening for aerobic , anaerobic , acid - fast bacillus , and fungal microorganisms . costs any surgical procedure comprises direct costs , measurable , such as operating room and surgical performance , and indirect costs , not so easily quantifiable , such as social costs , loss of work , or salary [ 30 ]  . 
the costs of hip aspiration were calculated by summing the costs of operating room , performance , and microbiological culture . the cost of the operating room was calculated per hour of procedure ( 1000 / h ) ( region of lombardy , italy ) , considering the start of the procedure as the moment of making the first insertion of the needle and the end as when the procedure was completed . 
the collection extends from superficial ( s ) to deep ( d ) soft tissues showing multiloculated aspect with thick synovial walls ( yellow arrow ) and septa ( white arrow )  . 
the needle ( arrows ) is advanced with an in - plane approach up to reach a small fluid collection ( white asterisk ) surrounding the hyper - echoic surface of hip prosthesis ( arrowhead )  . 
the costs of the ambulatorial ultrasound procedure were on charge of both the ssn and the patient , with the payment of a co - pay fee ( ticket ) , except for those who were entitled to exemptions . statistical analysis continuous variables were expressed as mean and standard deviation ( sd )  . 
specifically , each test is represented according to its sensitivity and 1 - specificity and connected to the point ( 0 , 0 ) and ( 1 , 1 ) through two lines . 
the slope of the two lines represents the likelihood ratio positive and negative of the test . results fifty - two hip aspirations were performed on forty - nine patients ( 23 men and 26 women )  . 
there were no statistically significant differences when comparing the mean age of patients ( p = 0.93 ) and the mean wait time for revision surgery ( p = 0.20 ) of the two groups . in the fluoroscopy group , ten patients ( 38.5% ) were considered infected ( fluoroscopy - pji group ) ( table2 )  . 
after the revision surgery , of these 10 infected hips , 6 patients ( 60% ) had positive preoperative hip aspiration ( true positive ) and 4 patients ( 40% ) had negative preoperative hip aspiration ( false negative )  . 
in the fluoroscopy - control group , three positive hip aspirations ( 18.8% ) were considered false positive , because the msis was not satisfied even after revision surgery . the sensitivity of hip aspiration in the fluoroscopy group was 60% ( 95% ci 2688% )  . 
the specificity was table 2 fluoroscopy aspiration hip aspiration pji group control group positive culture negative culture 1 3 32 table 3 ultrasound aspiration hip aspiration pji group control group positive culture negative culture table 4 fluoroscopy pji group case age msis diagnosis hip aspiration revision cultures culture 81 minor criteria sinus tract culture culture 89 minor criteria 79 minor criteria sinus tract culture cultures e . 
hip aspiration under fluoroscopy guidance required an average time of 176.7min. in the ultrasound group , nine patients ( 34.6% ) were diagnosed septic after msis criteria ( ultrasound - pji group ) ( table3 )  . 
fluoroscopy - guided aspiration with or without injection of iodinated contrast ( hip arthrography ) is the most commonly technique published in the literature ( table6 ) [ 223 ]  . 
it appears to be an effective and reproducible procedure , but there are risks derived from doses of radiations and the potential adverse reactions against iodinated contrast . in this retrospective study , ultrasound - guided aspiration showed good and superior outcomes in comparison with fluoroscopy - guided procedure evaluating sensitivity ( 89% vs 60% ) and specificity ( 94% vs 81.3% ) , even if the difference was not statistically significant . in our study , a low sensitivity was found for fluoroscopy . 
this rate of false - negative outcomes could be explained by the incapability of fluoroscopy to drive the needle toward a fluid collection , collecting potentially less fluid to cultivate than us . 
scarce fluid for culture and consequentially low table 5 ultrasound pji group case msis diagnosis hip aspiration cultures revision cultures culture culture culture culture culture culture culture culture culture s . 
the main limitation of this study is the small sample size that does not permit the detection of a statistical difference in terms of sensibility and specificity , even if the main purpose of the study was to show us as valid as fluoroscopy in detecting pji . 
larger randomized controlled clinical trials are needed to confirm and validate these clinical results and to draw the future role of the radiologist and ultrasound in the preoperative management of pji . a first question dealing with effectiveness of a diagnostic procedure in pji is how this procedure may resemble fluoroscopy - guided aspiration results . 
us has been reported an excellent modality to visualize the soft tissues surrounding the hip ( greater trochanteric bursa , iliopsoas tendon / bursa , gluteal tendons , and iliotibial band ) , cystic or solid soft - tissue masses [ 34 ] , and extra - articular fluid collections communicating with the joint : these structures , undetectable with fluoroscopy , can be possible locations of pathologies after hip arthroplasty and may be passible of aspiration [ 35 , 36 ]  . 
us provide theoretical advantages also considering needle insertion , which can be more precise and safer , monitoring continuously on the screen the tip of the needle , to avoid accurately heterotopic ossifications or septic extraarticular collections , with the potential risk of introducing infective microorganisms into a sterile joint [ 38 ]  . there are few studies about the accuracy of ultrasoundguided aspiration for hip pji diagnosis [ 2426 ]  . 
 [ 26 ] compared the clinical outcomes of ultrasound vs fluoroscopy hip aspiration , reporting similar results to our study , but different statistical comparison was performed . the cost analysis of our study showed an average difference of 218.28. 
usually , in the literature , the intraoperative culture results obtained during revision surgery were considered as the gold standard for the attestation of pji : this methodology does not appear completely reliable to differentiate pji from aseptic failure in our case series and in literature , due to possibility to underestimate the presence of pji . 
we had 4 patients in 19 infected ( 21% ) that presented intraoperative negative cultures : with the use of other major ( sinus tract ) or minor criteria , we were able to differentiate the septic failure of the prosthesis and better investigate the accuracy of the radiological techniques in managing pji . conclusions preoperative hip aspiration is a useful diagnostic tool for detection of pji . 
the standard of care for endometrial cancer patients with a good performance status and resectable tumor is surgical removal that may include hysterectomy , bilateral oophorectomy , pelvic and lombo - aortic lymphadenectomy , omental and peritoneal biopsies . lymph node metastasis , related to deep invasion ( > 50% ) of the myometrium , is the most common form of extrauterine disease spread and the strongest predictor for recurrence . 
for patients with low - risk endometrioid carcinoma ( grade 1 or 2 and superficial myometrial invasion < 50% ) , lymphadenectomy is not recommended , and only hysterectomy with bilateral oophorectomy is performed . 
for intermediate - risk patients ( deep myometrial invasion > 50% or grade 3 superficial myometrial invasion < 50% ) and high - risk vol . : ( 0123456789 ) 1 3 14 radiol med ( 2018 ) 123 : 1319 patients ( grade 3 with deep myometrial invasion > 50% ) , lymphadenectomy can be considered for staging purposes ( intermediate - risk ) or even recommended ( high - risk ) , along with omental and peritoneal biopsies [ 2 ]  . according to the european society of urogenital imaging guidelines for staging endometrial cancer [ 2 , 3 ] , the indications for mr , as helpful imaging for local staging , include : high grade , serous or clear cell adenocarcinomas , suspicion of deep myometrial invasion , and screening for lymphadenopathy . 
a prospective collaborative trial comparing mri and ultrasonography ( us ) , reported that the accuracy of us is comparable to that of mri for local staging [ 4 ]  . 
 recently introduced dual - energy ct ( dect ) scanners use more than one energy peak for fast image acquisition and depict the interaction of tissues and materials with x - ray beams at different energies [ 5 , 6 ]  . 
dect also yields processed images that increase iodine conspicuity ( enhancement ) in parenchymal tissue or vascular structures , and help to differentiate materials according to the different energies of the x - ray beam ( so - called material decomposition )  . since ct is frequently recommended for distant staging ( not only for n staging , but also for m staging ) , ct assessment of deep myometrial invasion would allow patients to avoid an additional examination for local staging , and could represent a one - stop radiological examination for staging endometrial cancer . to the best of our knowledge , no study has hitherto evaluated the performance of dect in evaluating deep myometrial infiltration by endometrial cancer . 
the objective of this study was a retrospective assessment of deep ( > 50% ) myometrial invasion in patients with a diagnosis of endometrial cancer who underwent dect for staging . materials andmethods patient selection patients with a diagnosis of endometrial cancer who underwent ct with spectral imaging before surgery between 28 / 10 / 2015 and 28 / 04 / 2017 ( 18months ) were retrospectively selected for inclusion in this study . 
exclusion criteria were : acquisition of ct scan without the use of spectral imaging , extensive pelvic artifacts caused by metallic hip prostheses , and surgery performed at other institutions . 
written informed consent to ct examination , and to the use of anonymized clinical and imaging data for scientific and / or educational purposes was obtained from all patients at first access in our institution . ct imaging technique all ct examinations were performed on a discovery ct750 hd scanner ( general electric healthcare , milwaukee wi , usa )  . 
all scans extended in a cranio - caudal direction from the lung apices or from the liver dome to the pubis in the portal venous phase ( 90120s after iv administration of contrast medium )  . 
all images were archived in digital format . scans were acquired during a single breath - hold with the following parameters : tube rotation time : 0.5s ; spiral pitch factor : 0.984 ; standard algorithm reconstruction ; total collimation width 40mm ( 640.625mm ) ; slice thickness 2.5mm ; reconstruction interval 2.5mm ; display field of view 330400mm ; tube voltage 80 and 140kv ; fixed tube current 630ma . evaluation ofct images each examination was evaluated using the gsi viewer - gsi liver and kidney tool on the aw server ( ge medical systems ) , where images were reconstructed at different kev levels and evaluated in the axial , sagittal and coronal planes by a radiologist with 12years of experience in gynecological imaging ( sr )  . 
evaluation of ct images included : assessment of deep ( > 50% ) myometrial invasion in the following three sets of images : 70kev ( corresponding to usual ct images ) , 50kev , and iodine material decomposition images . 
 at the time of ct scan assessment , the radiologist was aware of the diagnosis of endometrial cancer , but was blind to the results of surgery and the pathology report . on the three sets of images the radiologist described endometrial cancer as : not assessable ( na ) ; stage ia , if the tumor was confined to the endometrium or invaded the inner half ( < 50% ) of the myometrium ; stage ib , if the tumor invaded the outer half ( > 50% ) of the myometrium [ 7 ]  . ultrasound all patients underwent gynecological transvaginal us as part of their standard presurgical local staging when evaluation of myometrial invasion was always performed and recorded . 1 3 radiol med ( 2018 ) 123 : 1319 the reference gold standard ( gs ) for comparison of the radiological assessment was the pathological examination after surgery . statistical analysis the agreement between the three sets of ct images ( 50 , 70kev and iodine ) , the us and the gs for evaluation of deep myometrial invasion was estimated by the cohens kappa statistic ( k ) and tabulated with 95% confidence intervals ( ci )  . 
the power of the observed agreement for each set vs the null hypothesis of k = 0.50 using a two - sided significance test at the 5% level was also calculated . 
summary statistics ( counts , mean , median , min and max as well as percent ) for patients age , days from ct / us to surgery and grading were also produced . based on the comparison with the gs , sensitivity , specificity and accuracy of images at 50 , 70kev , iodine material decomposition and us were evaluated and tabulated with the proper 95% ci . results the study included 39 patients with a median age of 61years ( 4789 )  . 
all the histological examinations showed endometrioid adenocarcinomas ; 11 / 39 ( 28% ) with a differentiation grade 1 ; 15 / 39 ( 38% ) with a differentiation grade 2 ; 13 / 39 ( 33% ) with a differentiation grade 3 ( table1 )  . 
median time between ct scan and surgery was 23days ; median time between us and surgery was 18days ( table1 )  . among the three sets of ct images , myometrial invasion was not assessable in 24 / 39 ( 61% ) patients at 70kev , in 1 / 39 ( 2% ) patients at 50kev , and in 14 / 39 ( 35% ) in the iodine material decomposition images . the agreement between evaluation of myometrial infiltration and the gs at 50 , 70kev , iodine reconstructions and us is summarized in table2 . 
however , the post hoc power calculation showed that among the three sets of ct images , only those at 50kev had enough power ( 88% ) to test the hypothesis of no difference with respect to the gs ( power for 70kev , iodine reconstruction and us agreement with the gs were 7 , 16 and 21% , respectively )  . 
a combination of preoperative imaging and intraoperative evaluation is considered helpful to determine if this surgical procedure is necessary in each patient [ 10 ]  . specifically , for patients with low - risk endometrial cancer and for endometrial cancer patients in childbearing age , pre - operative assessment of myometrial invasion might be considered [ 2 , 11 , 12 ]  . 
according to this time delay , ct scans were acquired in our cohort during the portal venous phase , between 90 and 120s after contrast medium injection . many centers , including ours , stage endometrial cancer patients by second - level us ( for local staging ) and ct scan ( for distant staging )  . 
if a ct scan could assess myometrial invasion , it might offer additional information for local staging , especially in case of doubtful results , and serve for distant staging . ct scanning has never been considered reliable for local staging of endometrial cancer because it is not sensitive or specific enough to assess the depth of myometrial or cervical involvement , due to the poor contrast difference between tumor and myometrium [ 14 ] , the tumor itself being barely visible on ct images . 
indeed , conventional ct uses a single energy x - ray beam to acquire images , where the pixel values and hu are based on how many photons reach the detectors and how many are absorbed by the different tissues compared to those absorbed by water . 
this traditional limit of ct in evaluating the local extent of endometrial cancer was confirmed in our series , where the tumor itself was barely visible in the 70kev images , corresponding to the routine images acquired at 100kv . 
accordingly , on virtual monochromatic images at 70kev , myometrial invasion could only be assessed in 39% of patients , and the consequent agreement with surgery was as low as 0.43. dect may overcome this limitation because an additional attenuation measurement is obtained at a second energy , allowing the differentiation of two materials and quantification of their mass density . 
this approach is currently implemented with different methods : fast kvp switch between high and low energy ( from 140 to 80kev ) , dual x - ray sources and a multilayer detector , in which the innermost layer collects the low - energy data , while the high - energy data are collected by the outermost layer . 
the ct device used in this study adopted the fast kvp switch solution : a complete description of the advantages and disadvantages of each technique is provided by mccollough etal . 
specifically , low - energy virtual monochromatic images provide higher contrast between adjacent structures because of higher beam attenuation by iodine ; the drawback is that these images show more noise , particularly in heavier patients . 
virtual monochromatic images generated at 6077kev are reported to have optimal peak contrast - tonoise ratio for soft tissue evaluation , while those generated at 5055kev are optimal for evaluating blood vessels and depicting slow flow [ 6 ]  . accordingly , in addition to the 70kev images , we evaluated virtual monochromatic images at 50kev , as well as images reconstructed according to the material decomposition amplifying the presence of iodine ( iodine reconstructions )  . 
second , we did not compare the results of ct scan with mr as our institution prefers the approach of second - level us combined with a ct scan for distant staging . 
since we had no previous evidence of dect performance in the evaluation of myometrial invasion , we decided not to alter the usual local management of endometrial cancer patients by adding an mr examination . 
third , the number of cases evaluated in this study is relatively small ( n = 39 ) to determine the accuracy of dect as a pre - operative imaging modality for local staging of endometrial cancer patients . 
these encouraging results suggest that dect may be considered for assessment of deep myometrial invasion at first as an adjunct to other assessments and , after further validation , as an alternative to other pre - operative imaging examinations . 
the small lesion was well depicted on the axial ct images at 50kev ( a ) and iodine reconstructions ( b ) , where it was delineated by a subtle rim of contrast enhancement , showing that the myometrium was infiltrated < 50% ; the lesion was also clearly visible in ultrasound ( c ) , whereas its outer margins were difficult to see on the 70kev images ( d ) 1 3 radiol med ( 2018 ) 123 : 1319 fig . 
the lesions margins , which infiltrated the myometrium > 50% , especially on the right side , are better visible in the ct coronal reconstruction at 50kev ( a ) , although these images show more artifacts , and iodine reconstructions ( b ) , whereas it is less delineated on the 70kev images ( c )  . 
the same lesion was also seen and measured in us ( d ) lastly , the selection of patients was retrospective , depending on the performance of dect and tvus at our institution . 
alberto mauro , an employee of ge healthcare , helped the authors in setting up the ct protocol and had no influence on the data collected for this study . ethical approval this article does not contain any studies with animals performed by any of the authors . 
all procedures performed in this study involving human participants , were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent vidual participants included in the study . informed consent was obtained from all indiradiol med ( 2018 ) 123 : 4862 radiotherapy hypofractionated radiotherapy withsimultaneous integrated boost ( sib ) plustemozolomide ingood prognosis patients withglioblastoma : amulticenter phase ii study bythebrain study group oftheitalian association ofradiation oncology ( airo ) marcokrengli2 liviamarrazzo3 stefanomariamagrini4 beatricedetti1 silviascoccianti1 vincenzofusco5 luigipirtoli6 danieladoino7 albafiorentino8 lauramasini2 danielagreto1 michelabuglione4 giovannirubino6 federicolonardi9 fernandamigliaccio10 salvinomarzano11 riccardosantoni12 umbertoricardi13 lorenzolivi1 received : 14 july 2017 / accepted : 23 august 2017 / published online : 6 september 2017 italian society of medical radiology 2017 abstract introduction a multicenter phase ii study for assessing the efficacy and the toxicity of hypofractionated radiotherapy with sib plus temozolomide in patients with glioblastoma was carried out by the brain study group of the italian association of radiation oncology . methods twenty - four patients with newly diagnosed glioblastoma belonging to recursive partitioning analysis classes iii and iv were enrolled . 
one patient out of 24 ( 4.2% ) developed radionecrosis that required surgical resection with no evidence of disease in the surgical specimen . conclusions this trial confirms that hypofractionated radiotherapy with sib and association with temozolomide may be a reasonable and feasible option for good prognosis patients with gbm . keywords glioblastoma intensity modulated radiotherapy simultaneous integrated boost temozolomide hypofractionated radiotherapy * silvia scoccianti silvia.scoccianti@unifi.it 1 radiation oncology unit , azienda ospedaliera universitaria careggi , florence , italy 2 radiotherapy unit , department oftranslation medicine , university ofpiemonte orientale , novara , italy 3 medical physics unit , azienda ospedaliera universitaria careggi , florence , italy istituto del radio o . 
hypofractionated radiotherapy might be an option also for good prognosis patients considering that a shorter duration of the treatment leads to advantages from a quality of lifes perspective for the patients and cost savings in terms of machine time [ 4 ]  . moreover , intensity modulated radiotherapy ( imrt ) provides the chance to administer a simultaneous integrated boost ( sib ) , using different doses per fraction in different areas of the target . the current multicentric phase ii study was proposed by the brain working group of the italian association of radiation oncology ( airo )  . 
the study aimed at evaluating the efficacy in terms of overall survival ( os ) and progression - free survival ( pfs ) and toxicity of a hypofractionated schedule with sib in association with concomitant and sequential temozolomide ( tmz ) in patients with relatively good prognosis ( rpa classes iii and iv [ 6 ] )  . this trial was opened on september 2009 and , then , it was closed early on november 2014 , due to poor accrual . methods study design the brain , previous malignancies except for carcinoma insitu of the cervix or basal cell carcinoma , pregnant or lactating woman , and psychiatric disturbances . local institutional review board of each participating institution approved the study protocol . database development , central data management , statistical analysis , safety management and trial management were done at the department of radiation oncology in florence . all procedures performed in this study were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent was obtained from all individual participants included in the study . the primary aim of the study was the evaluation of actuarial os at 12months ( 12 - month os )  . 
the study was designed to detect an advantage in terms of survival at 12months from 0.61 , ( 12 - month os reported for patients enrolled in the eortc / ncic trial [ 1 ] ) , to 0.78 with statistical power at 80% and alpha = 0.05. 
the sample size needed was estimated to be 66 patients . survival rates were calculated according to kaplanmeier analysis , starting from the day of surgery to the day of last follow - up or death for os and to the day of evidence of radiological progression or to the day of last follow - up for pfs . univariate and multivariate analysis were conducted with the main prognostic factors using log - rank test and cox regression model , respectively , for assessing the prognostic value of different factors in terms of os and pfs . 
the following prognostic factors were evaluated : gender , age ( 65 vs > 65 ) , preoperative kps ( 80 vs > 80 ) and postoperative kps ( 80 vs > 80 ) , extent of surgery ( gross total resection vs subtotal resection vs biopsy ) , maximum diameter of preoperative gross tumor ( 3 vs > 3cm ) , and o6 - methylguanin - dna - methyltransferase ( mgmt ) promoter methylation status ( methylated vs not methylated )  . this multicentre trial was undertaken in nine radiotherapy departments in italy . patients were eligible for inclusion in the trial if they were newly diagnosed with histologically proven glioblastoma ; were at least 18years of age ; belonged to recursive partitioning analysis ( rpa ) class iii ( age < 50 , kps 90100 ) or iv ( age < 50 , kps < 90 ; age50 , surgical resection , good neurologic function ) ; had preoperative mri scan showing a lesion with maximum diameter 4cm in contrast - enhanced t1 - weighted sequences ; had availability of postoperative mri scan ; had adequate bone marrow , renal , and liver function ; agreed to use effective contraception if women of childbearing potential . exclusion criteria were lesions sited in the brainstem or infiltrating the spinal cord , previous radiation treatment to radiotherapy patients were immobilized with an individualized thermoplastic mask or with other devices with < 3 mm of uncertainty . slice thickness of the simulation computed tomography ( ct ) was 3mco - registration with postoperative mri was mandatory . the gross tumor volume ( gtv ) was defined on contrastenhanced t1 - weighted sequences and it included the operative bed and any residual contrast enhanced lesion . the clinical target volume for the sib ( ctv67.5gy ) was defined as the gtv + 5mm margin , whereas the clinical target volume for the lower - dose volume ( ctv52.5gy ) was obtained by adding a 10mm margin to the ctv67.5gy. 
considering an alpha / beta ratio equal to 10 for glioblastoma , the biologically effective dose ( bed ) of this schedule was equal to 97.8gy for the sib and to 70.8gy for the lower - dose volume . such a schedule was defined considering the data published by iuchi etal . 
 [ 7 ] who found that bed96gy in the boost volume was related to better outcomes in terms of both local control and overall survival . furthermore , a schedule for the lower - dose volume corresponding to a bed equal to 70.8gy was chosen in order to prescribe a dose similar to that commonly administered during the standard treatment . 
it is in fact noteworthy that the standard treatment consisting in 60gy in 30 fractions corresponds to a bed of 72gy for an alpha / beta ratio of 10gy . prescription was defined following the icru 50 and icru 62 guidelines [ 8 , 9 ]  . 
different priorities for each region of interest ( roi ) were suggested for the inverse planning . secondary dose constraints criteria were proposed both for oars and target volumes in case of critical location and extent of ptv . treatment was performed with imrt or other highly conformal techniques allowing meeting the critical organs constraints . 
verification was performed at least for the first three fractions and , then , on a weekly basis . chemotherapy radiotherapy was associated with concomitant chemotherapy with temozolomide ( tmz ) 75mg / m2 / day , 7days / week , from the first day until the end of radiotherapy . 
blood count was monitored throughout treatment weekly or more frequently , if needed . four weeks after completing the concomitant phase , chemotherapy with tmz was administered for additional 6 cycles of maintenance treatment . 
starting from the second cycle , the dose was escalated to 200mg / m2 in the absence of toxicity . tmz was administered daily , in the morning , on an empty stomach , preferably 1h before radiation treatment . 
1 protocol flowchart toxicity assessment side effects of radiotherapy were evaluated according to radiation therapy oncology group ( rtog ) scale [ 18 ]  . acute toxicity of chemotherapy was assessed according to common terminology criteria for adverse events v4.0 ( ctcae ) [ 19 ]  . chemotherapy was continued throughout the concomitant period if all of the following conditions were met : absolute neutrophilic count 1.5109 / l , platelet count 100109 / l , common toxicity criteria ( ctc ) non - hematological toxicity less than or equal to grade 1 ( except for alopecia , nausea and vomiting )  . during the sequential treatment a complete blood count was obtained 21days after the first dose . 
treatment - related 1 3 chronic toxicity was scored according to rtog / eortc scale for late toxicity [ 18 ]  . toxicity followup patients were followed with clinical assessment and mri scans after 3 and 6 chemotherapy cycles , and , thereafter , every 3months ( or earlier if clinically indicated )  . progressive disease was defined as a 25% increase in the size of one or more measurable lesions or the appearance of new lesions [ 20 ]  . in case of clinical worsening before the first planned response assessment , the mri scan was moved up . 
in case of apparent progression within 3months from the end of concomitant treatment , the patient underwent spectroscopy and / or perfusion mri to differentiate pseudo - progression from relapsing tumor . 
in case of lack of evidence of progressive disease , patients continued temozolomide until the following evaluation . in case of progression , patients received salvage chemotherapy or best supportive care . for each patient , day of last follow - up , day of evidence of progression disease and day of death were recorded . results efficacy between september 2009 and november 2014 , 24 patients were enrolled . 
all the other parameters ( gender , age , preoperative and postoperative kps , extent of surgery , maximum diameter , ptv volume ) were not significantly related to os . no prognostic factor resulted to have an impact on pfs . radiol med ( 2018 ) 123 : 4862 radiotherapy - related acute toxicity was no relevant . 
there were four chemotherapy interruptions ( 16.6% ) during the concomitant phase , all lasted 5days : 2 patients had an interruption for myelosuppression ( n = 1 g2 thrombocytopenia and n = 1 g2 neutropenia ) , one for g2 fatigue and another one for g2 impairment of liver function . 
six out of 24 patients required an increasing dose of antiedemigen drugs during rt for worsening of neurological symptoms . a case of g3 neutropenia and 2 cases of g3 thrombocytopenia occurred during the chemotherapy maintenance phase and caused a dose reduction for the following cycles . 
among patients who had maintenance tmz , 3 had more than 6 cycles . all the radiotherapy plans met the dose constraints for the organs at risk defined for the hypofractionated schedule . 
 during the long - term follow - up , there was no toxicity to the organs at risk for which constraints had been set , except for a case of g4 radionecrosis of the brain parenchyma : the patient required to be operated and there was no evidence of disease in his pathology specimen . discussion rationale from a radiobiological point of view , hypofractionation may lead to increased cell killing and reduction of tumor repopulation [ 2123 ]  . 
remarkably , the reduction of overall treatment time in hypofractionated regimens may represent a significant benefit in terms of quality of life for patients with such a severe prognosis [ 2426 ]  . 
the introduction in the clinical practice of imrt is related to a better conformity in dose release with advantages in terms of potential treatment - related toxicity [ 22 ]  . 
another benefit of imrt is the possibility of administering a sib with differentiated doses within the target volume [ 17 ]  . literature analysis there are several studies reporting the use of imrt with sib in high grade gliomas ( table3 )  . 
the interpretation of the findings in literature is not easy because the existing studies included a limited number of patients and some series included also who grade iii gliomas , introducing an important bias for understanding the efficacy of the 1 3 radiol med ( 2018 ) 123 : 4862 table 2 patients characteristics age ( years ) median range <= 65years > 65years 7080 90100 craniotomy stereotactic biopsy neuronavigation guided biopsy radical excision partial excision not available methylated not methylated <= 80 <= 80 phenytoin valproic acid levetiracetam unknown 4378 17 ( 71% ) 7 ( 29% ) 4 ( 17% ) 20 ( 83% ) 15 ( 62.5% ) 9 ( 37.5% ) 8 ( 33% ) 16 ( 67% ) 13 ( 54% ) 11 ( 46% ) 19 ( 79% ) 3 ( 12% ) 2 ( 8% ) 17 ( 71% ) 7 ( 29% ) 8 ( 33% ) 4 ( 17% ) 12 ( 50% ) 1 ( 4% ) 23 ( 96% ) 7 ( 29% ) 17 ( 71% ) 7 ( 29% ) 17 ( 71% ) 9 ( 37.5% ) 15 ( 62.5% ) 20 ( 83% ) 4 ( 17% ) 4 ( 17% ) 20 ( 83% ) 6 ( 25% ) 4 ( 17% ) 4 ( 17% ) 7 ( 29% ) 3 ( 12% ) 1 ( 4% ) 23 ( 96% ) preoperative intracranial high pressure preoperative focal neurological symptoms preoperative seizures preoperative kps surgery mgmt extent of surgery according to postoperative imaging postoperative intracranial high pressure postoperative focal neurological symptoms postoperative seizures postoperative kps postoperative preradiotherapy barthel index preradiotherapy use of steroids preradiotherapy use of aeds rpa class treatment . 
importantly , the interpretation of the results in terms of outcome is limited by significant heterogeneities in the definition of the target and in the employed radiation schedules . target definition the definition of target volumes varied very widely both for the lower - dose volume and for the boost volume . 
for the lower - dose volume , some authors included the peritumoral edema [ 7 , 22 , 32 ] or even the peritumoral edema with the addition of heterogeneous anisotropic margin [ 28 , 29 ] , while others chose as ctv for the lower - dose volume an isotropic expansion of the gross tumor volume ranging from 1.5 [ 23 , 27 ] to 2cm [ 30 , 33 , 34 ]  . 
for the sib volume , most authors chose to administer the boost on the gtv , defined as surgical cavity plus any enhancing lesion [ 22 , 23 , 27 , 28 , 30 , 32 , 33 ] , while others prescribed the boost dose to an isotropic expansion of gtv ranging from 0.5cm [ 7 ] to 1cm [ 29 ]  . 
for the lower - dose volume , the majority of studies used a conventional fractionation [ 23 , 2729 , 34 ] , whereas some authors used a dose for fraction > 2 and 3gy [ 22 , 30 , 32 , 33 ] and only a study [ 7 ] , besides the current one , opted for fraction size > 3gy . 
for the sib volume , some authors chose a moderate hypofractionation ( 2.43gy per fraction ) [ 23 , 2729 , 34 ] , whereas other authors tested a hypofractionation with doses for fraction 4gy , as in the current study [ 7 , 22 , 30 , 32 , 33 ]  . 1 3 radiol med ( 2018 ) 123 : 4862 1 3 56 radiol med ( 2018 ) 123 : 4862 1 3 radiol med ( 2018 ) 123 : 4862 1 3 58 radiol med ( 2018 ) 123 : 4862 1 3 radiol med ( 2018 ) 123 : 4862 1 3 60 radiol med ( 2018 ) 123 : 4862 biologically effective dose andoutcome in table3 , the biologically effective dose ( bed ) relative to the different radiation schedules is shown . 
bed of the schedules employed in the existing literature series ranged between 74.4 [ 29 , 32 ] and 125.8gy [ 7 ] for the sib volumes and between 39 [ 22 , 3033 ] and 67.2gy [ 34 ] for the lower - dose volumes . in the current study , the choice of the fractionation to use had a rationale : bed for the sib volume was 97.8gy for the sib volume , relying on the results of iuchi etal . 
on the other hand , bed for the lower - dose volume was 70.8gy in order to have a bed similar to the standard treatment . results in terms of efficacy of the existing studies in literature are very heterogeneous ( table3 )  . 
despite the limited number of the patients enrolled in the present trial , it seems interesting that no late toxicity occurred to the organs at risk for which dose constraints had been set . addition oftmz the most recent trials added tmz to the hypofractionated schedules [ 2732 ]  . 
interestingly , from literature data the addition of concomitant and sequential chemotherapy seems to have a slight but significant impact on os , although toxicity might increase , mainly in terms of myelotoxicity . prognostic factors in the present series , only the mgmt promoter status was found to be related to os . 
age [ 23 , 28 ] , kps [ 23 , 28 , 33 ] , rpa class [ 23 , 27 , 28 ] , extent of surgery [ 7 , 23 , 27 , 30 ] , and multifocality [ 33 ] resulted to have an impact on prognosis in patients with glioblastoma treated with sib technique in other literature studies but not in the present series , maybe due to the limited number of patients . advantages andpitfalls ofthestudy this study is a rare phase ii trial evaluating the role of sib in gbm but it is limited by a small number of patients , although , to our knowledge , the maximum number of patients ever included in a prospective series assessing the role of sib in gbm is 40 [ 28 , 29 ]  . 
 the low rate of the observed severe late toxicity related to radiotherapy in our series , in spite of the high bed of the chosen schedule and the use of temozolomide as a radiosensitizer , might highlight the importance to define and meet dose constraints . lastly , this series confirms that concomitant and sequential temozolomide is feasible also in hypofractionated schedules . conclusions the hypofractionated schedule with sib employed in this trial had comparable results in terms of efficacy with other studies in literature that used a sib . 
the severe toxicity rate was limited in spite of the high bed of the chosen schedule and it might be due to the adoption of strict dose constraints . 1 3 radiol med ( 2018 ) 123 : 4862 this trial confirms that hypofractionated radiotherapy with sib and association with temozolomide may be a reasonable and feasible option for good prognosis patients with gbm . 
 this new ultrasonography technique separates the moment of image acquisition ( that may be performed also by a technician ) from that of its interpretation , increasing reproducibility , reducing operator - dependence and physician time . 
abus , with those advantages , has the potential to be used as an adjunctive tool to screening mammography , especially in the dense breast , where mammography has a relatively low sensitivity . 
womens awareness of risks related to breast density is a hot topic , especially in the usa where legislative breast density notification laws increase the demand for supplemental ultrasound screening . 
the purpose of this article is to present a summary of current state - of - the - art of abus technology and applications , with an emphasis on breast cancer screening . 
this article discusses also how to overcome some abus limitations , in order to be familiar with the new technique . keywords automated breast ultrasound screening breast cancer ultrasonography * martina zanotel martina.zanotel@gmail.com 1 department ofmedical area , institute ofdiagnostic radiology , university ofudine , azienda sanitaria universitaria s . 
maria della misericordia , p.le santa maria della misericordia , 15 , 33100udine , italy introduction breast cancer is the most common malignant disease of the female population [ 1 ] and mammographic screening is an effective proven method for reducing mortality , through early diagnosis [ 2 ]  . 
for this reason and because of breast density has been established as an independent risk factor for breast cancer , the need for an additional tool is gaining ever greater interest [ 4 ]  . 
this study , however , revealed some weak points of hhus screening , such as the high number of false positives ( fp ) and the considerable effort in terms of physician time for exam execution and interpretation [ 5 ]  . 
automated breast ultrasound ( abus ) , also known as automated volumetric scanner ( abvs ) , depending on the vendor , was introduced with the purpose to overcome the operator - dependence of hhus , increasing the reproducibility of the examination . 
abus is a technological advance , which provides ultrasonography 3d representation of the breast tissue , with the advantage of multiplanar reformations and the capability to review images retrospectively once the examination has been acquired [ 4 , 10 ]  . 
the concept of automated breast ultrasound dates back to the 70s [ 11 ] ; however , old generation scanners had transducers with relatively low frequency ( 47mhz ) and image quality was not sufficiently good . 
interest in abus research further increased with the vol . : ( 0123456789 ) 1 3 2 radiol med ( 2018 ) 123 : 112 development of modern scanners , provided with high - frequency transducers [ 12 ]  . 
therefore , several studies were performed mostly for the evaluation of abus as a supplemental screening tool [ 1315 ] and in recent years some studies also considered its use in the clinical setting [ 12 , 1619 ]  . in the present review , we performed a computerized search by using the pubmed database ( gov / pubmed / ) , including articles listed up to 30 april 2017 . 
a hydrogel nipple pad is applied to allow proper contact with the skin and a trained operator is responsible for appropriate vertical orientation of the probe and adequate contact pressure with the skoverall examination time is about 2030min ( 1020min for scanning , 510min for preparing the patient ) [ 13 ]  . 
initially , such systems did not allow 3d reconstructions of the row data [ 4 ] ; however , new 3 - d whole breast multiplanar reconstruction software has recently been announced . modern automated breast scanners were subsequently developed ( somo - v , ge healtcare ; acuson s2000 , siemens medical solutions ) ; both received fda clearance in 2012 [ 21 ] and operate differently from previous hybrid machines . 
those systems are provided with special high - frequency and large footprint transducers ( 1517cm ) , similar in size to a mammography compression paddle and mounted on a mechanical arone of those modern systems is provided with a curved transducer designed to follow the contour of the breast [ 4 ]  . 
of note , learning to perform abus , with correct positioning and adequate compression power , requires time ; therefore , training is a relevant part for image quality [ 22 ]  . 
 after image acquisition , row data are stored on the systems hard disk and then transferred to a dedicated workstation , where images , displayed both in the native axial plane of acquisition and reformatted coronal and sagittal planes , can be reviewed for further interpretation and analysis . 
the coronal plane , also known as the surgical view ( in which the breast is positioned in the same way that it is oriented on the surgical table ) , introduces new diagnostic information , i.e. 
the main limitations of abus systems are exclusion of axillary regions from the field of view and the absence of tools to assess vascularity and tissue elasticity [ 4 ]  . prone - type scanners are still under development ; however , one of these systems received fda clearance in 2014 [ 21 ]  . 
a circumferential transducer performs the scan with the patient lying prone on the table with the breast suspended in a warm - water bath beneath an opening in the table top [ 22 , 24 ]  . 
after acquisition , data are processed and reconstructed to allow volumetric rendering [ 22 , 24 ]  . abus interpretation automated breast ultrasound technology allows the radiologist to interpret ultrasonography images in a separate time after acquisition . 
different interpretation times have been reported , ranging from 5 to 10min [ 14 , 23 , 2529 ] , probably according to differences in readers experience and complexity of each case . regarding the reading technique there is no uniform protocol : some authors used a reading protocol starting from transverse plane [ 26 ] , while other authors preferred starting from coronal plane [ 28 , 30 , 31 ]  . 1 3 radiol med ( 2018 ) 123 : 112 fig . 
1 artifacts : nipple shadowing ( arrow ) and dense breast parenchyma artifacts ( asterisk ) displayed on automated breast ultrasonography using siemens abvs ( a axial view , b coronal view , c sagittal view )  . 
re - scanning the same patient and increasing scanning pressure , these artifacts were eliminated ( d axial view , e coronal view , f sagittal view ) allowing to obtain an optimal visualization of the entire breast parenchyma clinical applications screening the application of automated breast ultrasound was initially focused on the screening setting and first works aimed to test the new technique in dense breast . 
interest has continued to increase in past years due to a greater awareness for the problem of breast density , especially in the usa where legislative breast density notification laws increase the demand for supplemental us screening [ 22 , 26 ]  . first screening works were performed using a hybrid system [ 13 , 25 ]  . 
 [ 13 ] , in a multicenter study , compared mammography alone versus automated whole breast ultrasound ( awbu ) plus mammography in 4419 women with dense breasts and / or at elevated risk of breast cancer . 
 the detection of invasive ductal cancers and smaller lesions ( 10mm ) was significantly higher for awbu alone than mammography ( sensitivities for cancers 10mm of 81 and 33% , respectively ) [ 13 ]  . 
by adding awbu to mammography , the sensitivity of breast cancer detection increased from 50 to 81% and all readers in this study significantly improved the identification of asymptomatic cancers [ 25 ]  . 
indeed , the cancer detection for true positive cases showed an increase of 63% , with only a 4% decrease in correct identification of the true negative cases [ 25 ]  . 
of note , mean interpretation time per awbu was 7min 58s [ 25 ] , shorter than the time reported in the acrin 6666 trial regarding hhus screening ( 19min ) [ 5 ]  . in the past years other important studies have been published using modern automated ultrasound systems [ 14 , 15 , 32 ]  . 
recall rates increased by 9.0 per 1000 ( 13.8 per 1000 for mammography alone and 1 3 4 radiol med ( 2018 ) 123 : 112 22.8 for the combined imaging approach ) and specificity decreased by 0.7% when abus was added to mammography [ 14 ]  . 
 specificity decreased non - significantly ( from 78.1% for mammography alone to 76.2% for the combined modalities ) due to a robust training program [ 32 ]  . table1 presents the results of above presented screening studies . 
on the other hand , an increase of recall rates was reported [ 1315 ] , a problem which emerged also from studies considering screening with hhus [ 36 , 37 ]  . 
 [ 38 ] evaluating abus as a screening tool in women with dense breasts , reported an overall recall rate of 19% during the 3 - month study time period . 
 of note , recall rate trended down from 24.7% in the first studys month to 12.6% in the third studys month showing the clinical implication that abus has a learning curve [ 38 ]  . 
therefore , such a problem could be overcome improving readers experience and by providing radiologists training programs to help minimize false positives [ 32 , 38 ]  . table 1 results of studies comparing screening mammography alone versus mammography plus abus study kelly etal . 
 most of the studies compared abus with hhus in terms of detection [ 23 , 28 , 31 , 3942 ] and characterization [ 12 , 4348 ] of breast lesions , while others evaluated the diagnostic performance of abus [ 23 , 29 , 30 , 39 , 41 , 4346 , 49 , 50 ]  . 
 some publications focused on the inter - observer agreement of abus [ 12 , 16 , 26 , 30 , 39 , 41 , 43 , 51 ] and others evaluated abus in the pre - operative setting [ 1719 , 52 ] , in the assessment of response to neoadjuvant chemotherapy [ 53 ] and as a second look procedure [ 10 , 54 , 55 ]  . 
furthermore , imaging - histologic correlation between abus semeiotics and molecular subtypes of breast cancer has been investigated [ 56 ]  . detection detection of breast lesions was reported to be similar between the two us modalities for most of the authors [ 23 , 3941 ] , even if some studies reported higher detection rates for abus than hhus ( table2 ) [ 31 , 42 ]  . 
 1 3 radiol med ( 2018 ) 123 : 112 table 2 results of studies comparing abus and hhus in breast lesion detection study number ( patients , lesions ) hhus detection rate ( % ) abus detection rate ( % ) wang etal . 
 [ 43 ] found fair agreement between abus and hhus in the comparison of bi - rads scores ( k = 0.34 ) , but dichotomizing bi - rads categories into suspicious ( bi - rads 4 - 5 ) vs . 
the same authors , 2years later , performed another study on 983 patients showing fair agreement ( k = 0.31 ) between abus and hhus in assigning bi - rads scores ( dichotomized as benign for bi - rads 1 - 2 and unclear / suspicious for bi - rads 0 , 4 and 5 ) [ 44 ]  . 
those results were caused probably by imbalanced blinding of readers ( hhus readers had clinical information and availability of mammography while abus readers did not ) [ 44 ]  . 
retraction phenomenon is a peculiarity of coronal plane , unique of abus , with high diagnostic accuracy for breast malignancy [ 31 , 39 , 40 , 48 ]  . 
2 a case of 48 - year - old woman with invasive ductal carcinoma ( idc ) of the right breast , diagnosed on us - guided core needle biopsy . 
in this study 31 of 119 malignant lesions were rated as bi - rads 1 - 2 by abus ; of those , 12 lesions were seen after re - reading abus examinations and 8 lesions were primarily seen with mri or mammography , therefore found on second look [ 44 ]  . 
 relevant problems concerning the image quality emerged from the study , such as the presence of artifacts and lacking data due to inadequate contact between the transducer and the skin [ 44 ]  . most of published studies did not find significant differences between hhus and abus in diagnostic performance ( table3 ) [ 23 , 39 , 41 , 45 , 49 ]  . 
one of the fn of hhus ( misinterpreted as adenosis ) was a 6.5cm invasive ductal carcinoma , presenting as an extensive hypoechoic area but correctly detected by abus , thanks to its wide scanning area [ 23 ]  . 1 3 radiol med ( 2018 ) 123 : 112 fig . 
automated breast ultrasonography detected a small ( 8 mm ) hypoechoic mass presenting the retraction phenomenon , which is a useful feature visible on coronal plane ( a , b , c three contiguous coronal images , d axial view )  . 
tomosynthesis ( e mlo view , f cc view ) showed a small spiculated opacity interobserver reliability inter - observer reliability has a fundamental role in determining the diagnostic accuracy of abus with a significant impact on its clinical practice [ 50 ]  . 
key results from main studies are summarized in table4 . data regarding the agreement in assigning bi - rads scores were heterogeneous , ranging from slight to substantial [ 12 , 26 , 30 , 39 , 41 , 43 , 51 ]  . 
agreement proved to increase by dichotomizing bi - rads scores into benign and suspicious groups [ 30 , 43 ] and also by adding mammography to abus [ 26 ]  . 
 [ 16 ] analyzing 24 patients with abus two times before biopsy or surgery ( within a mean interval of 1.3days ) found that the different values of depth were probably related to variations in positioning and scanning pressure of the probe . 
az for hhus and abus were not statistically significant for each reader ( n = 3 ) , but the mean az values were significantly different other applications ofabus in the preoperative setting , one of the preliminary studies for abus , which was performed in a population of 40 patients including both insitu and invasive cancers , showed promising results in the extent of cancer assessment [ 19 ]  . 
 [ 18 ] , analyzing 33 patients with histologically proven dcis , found that abus assessed the extent of disease better than hhus ( compared to histopathology ) and that mean lesion size assessed by abus did not differ significantly from that determined by histopathology . 
 [ 52 ] focusing on the pre - operative assessment of dcis , found that abus is superior to hhus in the detection of malignancies and it is also more accurate in the tumor largest diameter assessment . considering 3d evaluation of 51 invasive ductal carcinomas , xu etal . 
 [ 17 ] assessed largest tumor diameter , tumor volume and tumor surface area on hhus and abus and 1 3 radiol med ( 2018 ) 123 : 112 1 3 10 radiol med ( 2018 ) 123 : 112 compared these with tumor size and volume on pathology specimen after surgical excision ( gold standard )  . 
furthermore , volumetric measurements determined by abus had significantly higher accuracy than those determined by hhus [ 17 ]  . automated breast ultrasound has been also evaluated in the assessment of response to neoadjuvant chemotherapy [ 53 ]  . 
the product change of two largest perpendicular diameters ( pc ) in axial and coronal planes and the longest diameter change in axial and coronal planes were the four prediction methods examined in the study [ 53 ]  . 
the overall performance of abus in predicting complete response after four cycles of chemotherapy was high ( area under the receiver operating characteristic curve [ auc ] : 0.830.85 ) and all four prediction methods revealed high sensitivities ( 85.788.1% ) while specificity was high only for pc ( 81.585.1% ) [ 53 ]  . 
 [ 56 ] demonstrated that the luminal - a , luminal - b , her2 and triple - negative subtypes have specific predictive factors ( luminal - a : retraction phenomenon , post - acoustic shadowing , echogenic halo , absence of calcifications ; luminal - b : presence of calcifications , absence of retraction phenomenon ; her2 : presence of calcifications , absence of retraction phenomenon , non - mass lesions , absence of echogenic halo , post - acoustic enhancement ; triple negative : absence of retraction phenomenon , post - acoustic enhancement , absence of echogenic halo , absence of calcifications , regular shape )  . 
automated breast ultrasonography ( a coronal view , b axial view , c sagittal view ) detected two hypoechoic lesions with retraction phenomenon on the upper quadrants of the left breast , well represented on coronal reconstruction ( index lesions : thin arrow ; multifocality : arrowhead )  . 
another small hypoechoic area ( circle on coronal , axial and sagittal views ) was detected on automated ultrasonography secondlook examination performed after staging breast mri , due to the presence of suspicious mass like enhancement on the inferior - outer quadrant of the same breast ( d large arrow )  . 
 coronal view well depicts all three neoplastic lesions in the same image 1 3 radiol med ( 2018 ) 123 : 112 independent predictor for the luminal - a subtype when present and for the triple negative subtype when absent [ 56 ]  . conclusion automated breast ultrasound is an emergent ultrasonography technique , developed to support screening mammography , especially in dense breast , where mammographys sensitivity is relatively low . 
however , abus presents some limitations because of the lack of tools to assess vascularity and tissue elasticity ; another possible limitation is the exclusion of axillary regions from the field of view . 
with the increase of screening demand , abus has the potential to be the method of choice as an adjunctive tool to screening mammography in women with dense breast tissue . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval this article does not contain any studieswithhuman participants or animals performed by any of the authors . informed consent the images of automated breast volumetric scanner ( abvs ) and mri shown in the figures were retrospectively selected among examinations previously performed according to an ethical committee approved trial investigating the role for abvs in clinical practice , with informed consent obtained from all individual participants . funding no funding was received . radiol med ( 2018 ) 123 : 4447 radiotherapy xerostomia quality oflife scale ( xeqols ) questionnaire : validation ofitalian version inhead andneck cancer patients lucianalastrucci1 robertademajo1 andrearampini1 pietrogiovannigennari1 paolapernici1 silviabertocci1 vittoriobini2 simonaborghesi1 received : 16 june 2017 / accepted : 4 august 2017 / published online : 31 august 2017 italian society of medical radiology 2017 abstract aim to translate the xerostomia quality - of - life scale ( xeqols ) into italian language ( xeqols - it )  . 
the xeqols consists of 15 items and measures the impact of salivary gland dysfunction and xerostomia on the four major domains of oral health - related qol . methods the xeqols - it was created through a linguistic validation multi - step process : forward translation ( tf ) , backward translation ( tb ) and administration of the questionnaire to 35 italian patients with head and neck cancer . 
radiotherapy ( rt ) has an essential role in the management of hnc , yet it produces considerable acuteand long - term side effects to the oral cavity [ 2 ]  . 
xerostomia is the most prominent complication in patients with hnc : in the first week of conventional rt , salivary flow decreases from 50 to 60% , after 7weeks it diminishes to approximately 20% and continues to decline for up to several months after rt , depending on the dose received by the salivary glands and the volume of the gland tissue included in the irradiation fields [ 46 ]  . 
many patients have difficulty eating dry or hard food and are forced to adjust their vol :  . ( 1234567890 ) 1 3 radiol med ( 2018 ) 123 : 4447 diet . 
a variety of methods are currently available for the evaluation of radiation - induced xerostomia , however , dry mouth is a subjective experience and its assessment should rely on patient self - reports [ 9 ]  . 
 xerostomia - related quality of life scale ( xeqols ) is a validated questionnaire developed on 15 items , grouped into 4 domains ( physical functioning , personal / psychological functioning , social functioning , pain / discomfort issues ) [ 2 ]  . 
each items are formed on a likert scale : the first 14 items asking how mouth dryness affects life in specific ways using the ordinal response categories of not at all , a little , somewhat , quite a bit , and very much ; the 15th item asks if you were to spend the rest of your life with your dry mouth / throat dryness just the way it is now , how would you feel about this ? using likert responses ranging from delighted to terrible . 
the aim of this study is to validate the italian translation of xeqols ( xeqols - it )  . materials andmethods the items of xeqols were translated into italian language performing a process taking into account the recommendations by the european organization for research and treatment of cancer quality of life group guidelines for translation [ 11 ]  . 
hypothesizing an expected prevalence of comprehension problems < 10% with a precision of confidence limits 10% , we recruited 35 italian patients affected by hnc receiving radical or postoperative rt or radiochemotherapy or in follow - up after radical treatment . 
table1 table 1 characteristics of subjects at study male female 1850years 5165years 6683years ecog 0 ecog 1 patients in radiotherapy treatment patients in follow - up lower secondary education secondary education retirees / not workers workers smokers no smokers drinkers no drinkers patients with partner ( wife , husband , mate ) patients without partner 29 ( 82.8% ) 6 ( 17.2% ) 1 ( 2.8% ) 17 ( 48.6% ) 17 ( 48.6% ) 24 ( 68.6% ) 11 ( 31.4% ) 8 ( 22.9% ) 27 ( 77.1% ) 23 ( 65.7% ) 12 ( 34.3% ) 24 ( 68.6% ) 11 ( 31.4% ) 24 ( 68.6% ) 11 ( 31.4% ) 9 ( 25.7% ) 26 ( 74.3% ) 29 ( 82.8% ) 6 ( 17.2% ) describes patients features . 
to evaluate v2 , patients completed the xeqols - it and also a cognitive debriefing about the clarity of instructions , the easiness to complete the items and any recommendable changes . 
 the cognitive debriefing consisted in 6 points : debriefing 1 , the clarity of instructions and of the items on a five - point likert scale ( 1 = not at all ; 2 = somewhat ; 3 = moderately ; 4 = very ; 5 = completely ) ; debriefing 2 , the ease to complete the items on a five - point likert scale ( 1 = not at all ; 2 = somewhat ; 3 = moderately ; 4 = very ; 5 = completely ) ; if it was easy to answer the items using the proposed rating scale with yes / no answer format ; if there were difficulties , they were asked to indicate which ones ; if any word of the instructions and of the items was unclear , indicate which ones ; if any item was redundant , should be deleted or added ; if they had any suggestion to improve any item , instruction and response scales . time to compilation was recorded for each patient . 
 patients demographic , clinical , and treatment details were recorded and correlated with the items , the four domains of hrqol and the debriefing score . 1 3 46 statistical analysis to describe the extent to which all items measure the same concept or construct , we used the cronbach alpha coefficient to assess internal consistency [ 12 ]  . 
in our study , we found that this discomfort is predominant in 1850 aged . in conclusion , the italian version of xeqol is linguistically valid , future research should explore feasibility and utility for clinicians and patients . compliance with ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . conflict of interest the authors declare that they have no conflict of interest . 
the first - order adc histogram parameters at the intra - treatment time - point were compared to the baseline time - point in the metastatic lymph nodes ( lns )  . 
this was followed by txt9percentile75pre , txt1meanpre , and txt2standard deviationpre . conclusions our results suggest that heterogeneity metrics extracted from adc - maps in metastatic lymph nodes , before and after ic , can be used as supplementary ic response indicators . keywords nasopharyngeal cancer lymph node induction chemotherapy diffusion - weighted mri introduction nasopharyngeal carcinoma ( npc ) originates from epithelium of the nasopharynx . 
the use of ic prior to chemo - radiation therapy reduces the rate of distant metastasis , especially for patients with a gap between diagnosis and the start of chemo - radiation therapy [ 2 ]  . if outcome can be predicted during an early treatment stage , patients could be spared from ineffective treatment toxicity [ 35 ]  . 
studies have shown that computed tomography ( ct ) has a high negative predictive value ( npv ) of up to 95% , with a low positive predictive value ( ppv ) of 35% , for assessing the lymphadenopathy response to chemo - radiation therapy [ 6 ]  . 
ultrasound ( us ) is preferred for evaluation of intra - nodal architectural changes , but unreliable information of deeper lymph nodes is a major challenge of us [ 7 ]  . 
 other imaging modalities ( e.g. , single photon emission - ct ( spect ) and positron emission tomography ( pet ) ) are limited by low spatial resolution for treatment response , especially shortly after initiation of treatment [ 8 ]  . conventionally , assessment of treatment outcome in lymphadenopathy by ct and conventional magnetic resonance imaging ( cmri ) is based on measurement of short axis of the lymph nodes , according to recist criteria . 
this method cannot be used within a short duration after the start of treatment , because morphological changes have not occurred yet [ 9 ]  . diffusion - weighted ( dw ) magnetic resonance imaging ( mri ) and its derived apparent diffusion coefficient ( adc ) map provide physiological information about tumorous tissues [ 10 ]  . 
by quantifying water diffusivity within the tumor , changes in tumor cellularity , which may occur due to chemotherapy , radiotherapy or adjuvant chemo - radiation therapy , can be traced by dwi [ 1013 ]  . in this study , a heterogeneity analysis was applied on an adc - map of the metastatic nodes at the baseline , after one cycle of ic and after two cycles of ic , with the aim of establishing two hypotheses : firstly , pretreatment heterogeneity measures have potential to classify complete response ( cr ) patients from partial response ( pr ) patients , and secondly , the alterations of lns internal microenvironment after one cycle of ic could be detected by the heterogeneity parameters . 
the present study was performed to test the defined hypotheses in ten patients . materials andmethods patients institutional review board ( irb ) approval was obtained from the local institution at shahid beheshti university of medical science for performing serial mri acquisitions on patients with nasopharyngeal cancer who showed lymph node involvement . 
twenty patients with histologically confirmed primary nasopharyngeal cancer who were treated between jan 2013 and july 2014 at our institution ( jorjani radiotherapy center , imam hosein hospital ) participated in this study . 
among the enrolled patients , 10 patients were excluded for the following reasons : ( 1 ) one patient had claustrophobia and could not continue the serial mri examination ; ( 2 ) the image quality of three patients was poor and not sufficient for the analysis ; ( 3 ) two patients didnot have a metastatic lymph node ; and ( 4 ) four patients decided to continue with their treatment at another institution . 
full mr imaging sessions were carried out on the 10 patients who filled out the informed consent fortable1 summarizes the patient demographics . treatment protocol included two cycles of ic ( cisplatin : 75mg / m2 in day 1 and 5 - fu : 1000mg / m2 in days 14 ) , followed by a full dose of radiotherapy ( 70gy ) to the primary and gross nodal disease and a prophylactic dose to the uninvolved neck regions ( 60gy ) using a three - dimensional conformal technique ( 3dcrt )  . 
conventional images included t1 - weighted images ( tr / te = 692 / 8ms ) and t2 - weighted spin - echo images ( tr / te = 4550 / 116ms ) in axial planes , with slice thickness = 6mm , spacing between slices = 6.6mm , field of view ( fov ) = 256256mm2 and flip angle = 90  . 
diffusionweighted images were obtained using a spine echo - planar table 1 patients demographics patient tumor staging response t2n3 t1n1 t2n3 t2n1 t2n3 t1n2 t1n2 t1n2 t2n1 t2n2 1 3 38 radiol med ( 2018 ) 123 : 3643 imaging ( epi ) pulse sequence in the axial plane before contrast administration , with slice thickness = 5mm , fov = 192192mm2 , and tr / te = 1020 / 88ms . 
the diffusion sensitizing gradients were applied in all three orthogonal planes ( x , y , z ) with three b - values ( 0 , 500 , and 1000 ) s / mm2 . imaging time points were 1 week before , 10 days after the initiation of injection in first cycle of ic and 2 days after the end of second cycle of ic . 
the regions of interest ( roi ) were then overlaid on the corresponding adc - maps with a visual guide reference of ce - t1 images using image - j software at three time points : before treatment ( adcpre ) , after one cycle of ic ( adcintra ) , and at the end of ic ( adcpost )  . 
in addition , other sets of rois were drawn on ce - t1 images at three time points ( i.e. , ce - t1pre , ce - t1intra , and ce - t1post ) to measure the whole ln volume . 
the parameters were calculated as follows : ( 1 ) meanthe mean of the tumor histogram , ( 2 ) standard deviationthe average contrast , ( 3 ) normalized variancethe measure of smoothness , ( 4 ) skewnessthe third moment , ( 5 ) energya measure of uniformity or homogeneity , ( 6 ) entropya statistical measure of irregularities , ( 7 ) kurtosisthe fourth moment , ( 8 ) 25th percentilethe smallest scores that are greater than , or equal to 25% , ( 9 ) 75th percentilethe smallest scores that are greater than , or equal to 75% , and ( 10 ) 95th percentilethe smallest scores that are greater than , or equal to 95% . 
the definitions of the quantitative parameters ( qp ) are presented in table2 . to assess whether the pretreatment ln volume ( lnv ) and their changes can be used as a macroscopic predictive marker ( based on anatomical images ) or not , the entire ln volume was calculated by multiplying the voxel size with the number of voxels , slice thickness , and inter - slice gap within specified rois . results qps were compared between pretreatment ( qppre ) and after one cycle of ic ( qpintra ) using paired sample t tests for all patients . 
the evolution of these parameters before , intra ( 10 days after first injection ) and post ic ( after the end of two cycle of ic ) was depicted for all patients ( fig.3a , c , e )  . 
a discriminant analysis was used to build a predictive model , based on a linear combination of the pretreatment parameters that provides the best discrimination between the cr and pr groups . 
images in each row are from three measurement time points : a cet1pre , b ce - t1intra , c ce - t1post , d adcpre , e adcintra , f adcpost . 
previous studies investigated the role of adc parameters in predicting the treatment response to therapy in head and neck squamous cell carcinoma ( hnscc ) [ 6 , 13 ]  . 
 [ 2 ] reported that pretreatment adc and t - stage are associated with the local failure of chemoradiotherapy or radiotherapy in hnscc and achieved a significant positive correlation between t - stage and adc . 
changes in the meanadc 3 weeks after chemoradiotherapy , in comparison with the corresponding values before treatment , were reported as an indicator for loco - regional failure and loco - regional control by matoba etal . 
 [ 2 , 3 ]  . the results of our study will be discussed from the following two points of view : extraction ofquantitative texture parameters fromtheadcmap forearly detection ofmicrostructural changes andtreatment response ofinvolved lns toone cycle ofic most investigators extracted the meanadc to evaluate the early changes of tumor cellularity . 
therefore , the focus of this study was to evaluate 1 3 40 mean - adc max - adc min - adc median - adc txt1 - mean txt2 - std txt3 - nv txt4 - skewness txt5 - energy txt6 - entropy txt7 - kurtosis table 2 definitions of heterogeneity quantitative parameters quantitative parameters definition radiol med ( 2018 ) 123 : 3643 the average of adc - values within the roi the maximum adc - value within the roi the minimum adc - value in the roi the median of adc - values in the roi the mean of the tumor histogram the amount of variation from the mean of histograthis feature is a measure of average contrast within the roi the mean of the normalized squared distances of each of adc - values within the roi from histogram mean . 
this feature demonstrates the amount of dispersion of adc - values around the mean and is a measure of smoothness within the image the amount of asymmetry between values of adc - values around the mean . 
if the tail is longer on the left side than the right side , the histogram is negatively skewed and if the right - side tail is elongated , the histogram is positively skewed the sum of squared adc - values within the roi , which is a measure of homogeneity within the roi . 
higher energy denotes higher homogeneity and lower energy represents heterogeneity the average amount of information within the roi : more uncertainty requires more information for encoding ad has higher entropy . 
higher kurtosis reflects more distribution of the values towards the tails rather than the mean and lower kurtosis shows that the adc - values are more concentrated around the mean txt8 - percentile25 the point on the horizontal axis such that 25% of the area under the histogram lies to the left of that point ( and 75% to the right ) txt9 - percentile75 txt10 - percentile95 the point on the horizontal axis such that 75% of the area under the histogram lies to the left of that point the point on the horizontal axis such that 95% of the area under the histogram lies to the left of that point metastatic lymph node changes using heterogeneity analysis to reveal their physiological behavior early after one cycle of ic . in summary , there are two major differences between this ongoing study and the previous studies : first , the use of heterogeneity analysis for ln response assessment , and second , different mri data acquisition time points and evaluation of response after one cycle of ic . 
to the best of our knowledge , the employment of texture analysis on adc - maps for assessing lns response to just one cycle of ic has yet to be documented . 
for this purpose , several quantitative metrics were explored to obtain the most accurate feature ( s ) as potential predictive biomarkers for the early response of the ln to ic . 
the initial results showed that some of these parameters could detect early changes in the intra - nodal microstructure . in most studies , effective treatment is reflected by an increase in adc - values . 
 however , there was no correlation between the mean , txt1 mean , and txt5energy with the cr or pr groups , possibly due to the small number of patients . 
these results suggest that the previously - mentioned quantitative parameter could be used as a predictive biomarker for the therapeutic response in the early phase ( only one cycle of ic ) of the treatment in a larger number of patients . the results of the volumetric measurements were indicative of the inability of lnvs changes to detect a response to one cycle of ic . 
3 comparable evolution in mean adc , txt1meanadc , txt5 energy , and ln volume following one ( intra ) and two ( post ) cycle of ic for all patients ( a , c , e , and g ) , cr and pr patients ( b , d , f , and h ) quite distinct from each other , which was indicative of the potential of txt5energy to classify cr from pr group . 
a smaller wilks lambda and the coefficients with large absolute values corresponded 1 3 42 radiol med ( 2018 ) 123 : 3643 our preliminary results suggest that a heterogeneity analysis on metastatic ln before and early after ic yields valuable information about effect of ic . acknowledgements this work was fully supported by a grant from the shahid beheshti university of medical science ( grant number : 5232 ) , tehran , iran . 
this study aimed to assess ct features of the msgs after ria in patients with papillary thyroid carcinoma ( ptc )  . methods the study population comprised consecutively registered ptc patients who had undergone total thyroidectomy , ria , follow - up neck ultrasonography ( us ) , and neck ct . 
post - ria changes were determined by comparisons between follow - up neck us results ( main reference ) and between preoperative and post - ria neck ct features . results of the 28 patients , 13 ( 46.4% ) showed post - ria changes in the parotid glands ( n = 8 ) , submandibular glands ( n = 0 ) , or both ( n = 5 ) on neck ct . 
the common ct findings of postria changes in the parotid gland included low parenchymal attenuation , decreased glandular size , a lobulated margin , decreased or increased parenchymal enhancement , and an inhomogeneous enhancement pattern , whereas common ct findings of post - ria changes in the submandibular gland included decreased glandular size , a lobulated margin , * dong wook kim dwultra@nate.com 1 department ofradiology , busan paik hospital , inje university college ofmedicine , 75 , bokji - ro , busanjin - gu , busan47392 , southkorea iso - enhancement , and an inhomogeneous enhancement pattern . conclusion the common ct features of post - ria changes in msgs include decreased glandular size , a lobulated margin , and an inhomogeneous enhancement pattern . keywords computed tomography papillary thyroid carcinoma major salivary gland radioactive iodine ablation introduction radioactive iodine ablation ( ria ) is commonly used for the complete removal of remnant papillary thyroid carcinoma ( ptc ) after total thyroidectomy [ 1 ]  . 
in the literature , radiotherapy or ria may change the echotexture , echogenicity , and margins of the major salivary glands , and may reduce the glandular size on ultrasonography ( us ) [ 46 ]  . 
in a previous study , common us features of post - ria changes in msgs included a coarse echotexture , decreased echogenicity , a lobulated margin , and decreased glandular size [ 6 ]  . 
in particular , the history of ria and comparison of us features before and after ria can differentiate post - ria changes in msgs from other msg diseases [ 6 ]  . computed tomography ( ct ) is a popular imaging tool for evaluating various neck lesions because it has many advantages , such as a wide field of view , objectivity , and detailed display of bone or air - containing organs [ 7 ]  . 
1 a 57 - year - old woman who underwent total thyroidectomy and a single session of radioactive iodine ablation ( ria ) for papillary thyroid carcinoma in the left thyroid lobe . 
before total thyroidectomy and ria , both parotid ( a ) and submandibular ( b ) glands on contrast - enhanced , axial computed tomography ( ct ) image show a smooth margin , a normal gland size , and homogeneous parenchymal enhancement ( arrows )  . 
on the contrast - enhanced , axial ct images of both parotid ( c ) and submandibular ( d ) glands at 44months after ria , both parotid ( arrows ) and right submandibular ( arrowheads ) glands show a decreased glandular size , a lobulated margin , decreased parenchymal enhancement , and an inhomogeneous enhancement pattern ( suggestive of post - ria changes ) , whereas left submandibular gland ( arrows ) shows a smooth margin , a normal gland size , and homogeneous parenchymal enhancement ( suggestive of normal gland )  . 
on the longitudinal sonograms of both parotid ( e ) and submandibular ( f ) glands at 42 months after ria , both parotid ( right : arrowheads , left : arrows ) and right submandibular ( arrowheads ) glands show a coarse echotexture , decreased echogenicity , a lobulated margin , and decreased glandular size ( suggestive of postradioactive iodine ablation change ) , whereas left submandibular gland ( arrows ) shows a fine echotexture , iso - echogenicity , a smooth margin , and normal glandular size ( suggestive of normal gland ) changes in msgs may be helpful in the ct evaluation of msg lesions . 
therefore , this study aimed to evaluate ct features of post - ria changes in msgs in ptc patients who had undergone total thyroidectomy and postoperative ria . radiol med ( 2018 ) 123 : 2027 materials andmethods patients this study was approved by the appropriate institutional review board , and the need for informed consent was waived due to its retrospective nature . 
among them , 30 patients who did not undergo 1 or more follow - up us examinations of the neck and 244 patients who did not undergo at least 1 ct examination of the neck in our hospital after ria ( over a period of approximately 7years ) were excluded . 
after radioactive iodine administration , the patients were instructed to consume sour juice or candies as frequently as possible for 2days to increase salivation . for all the study patients , 2 radiologists performed follow - up neck us using a high - resolution ultrasound scanner ( iu 22 ; phillips medical systems , bothell , wa , usa ) with a 512 - mhz linear probe . 
at this institution , follow - up neck us examinations are routinely performed for 1 ( 4.3 ) 5 ( 21.7 ) 0 ( 0 ) 17 ( 73.9 ) 1 ( 4.3 ) 5 ( 21.7 ) 17 ( 73.9 ) 7 ( 30.4 ) 0 ( 0 ) 16 ( 69.6 ) 16 ( 69.6 ) 7 ( 30.4 ) 8 ( 34.8 ) 6 ( 26.1 ) 9 ( 39.1 ) 5 ( 21.7 ) 18 ( 78.3 ) neck ct andimage analysis neck ct was conducted using a contrast medium ( slice thickness , 3mm ; reconstruction increment , 3mm ) and a 64 - channel multi - detector ct scanner ( aquilion one ; toshiba medical systems , otawara , japan ) or a 128 - channel multi - detector ct scanner ( lightspeed ; general electric medical systems , milwaukee , wi , usa )  . 
at our hospital , neck ct was performed in the axial planes from the skull base to the upper mediastinum , whereas the upper level of the ct scan in non - enhanced ct was the skull base or mandibular angle , depending on the clinical reasons for neck ct . in may 2017 , the same radiologist with 16years of experience in head and neck ct interpretation retrospectively analyzed the ct images using a picture archiving and communication system , while blinded to the us data . 
the following features were retrospectively investigated on the basis of subjective evaluation by the investigator : degrees and patterns of parenchymal attenuation and enhancement , the size of msgs , and glandular margthe degrees of parenchymal attenuation were classified as iso - , low , or high on non - enhanced images . 
hu values of msgs were not considered in the determination of parenchymal attenuation and enhancement , because of the lack of a reference hu value . determination ofpostria change post - ria changes were determined by comparisons between follow - up neck us results ( main reference ) and between preoperative and post - ria neck ct features : ( 1 ) when newly developed us features of post - ria changes in msgs ( including a coarse echotexture , decreased echogenicity , a lobulated margin , and decreased glandular size ) were detected on follow - up us after ria , the presence of postria change was determined . 
2 a 41 - year - old man who underwent total thyroidectomy and a single session of radioactive iodine ablation ( ria ) for papillary thyroid carcinoma in the right thyroid lobe . 
before total thyroidectomy and ria , non - enhanced ( a ) and contrast - enhanced ( b ) , axial computed tomography ( ct ) images show normal parotid glands with mild fat degeneration ( arrows )  . 
at 38 months after ria , nonenhanced ( c ) and contrast - enhanced ( d ) , axial ct images of both parotid glands show normal findings with mild fat degeneration . 
on the longitudinal sonograms ( e ) of both parotid glands at 42 months after ria , the left parotid gland ( arrowheads ) shows a coarse echotexture , decreased echogenicity , a lobulated margin , and decreased glandular size ( suggestive of post - radioactive iodine ablation change ) , whereas right parotid gland ( arrows ) shows a fine echotexture , isoechogenicity , a smooth margin , and normal glandular size ( suggestive of normal gland ) msgs between preoperative neck ct and neck ct after ria was detected in a patient with negative follow - up us results and no clinical suspicion of other msg disease , the presence of post - ria change was determined . 
however , image analysis for the sublingual gland was not performed . 1 3 radiol med ( 2018 ) 123 : 2027 table 3 frequency analysis of computed tomography features of eight submandibular glands with post - radioactive iodine ablation change after radioactive iodine ablation in five patients ct features degree of parenchymal attenuation isolow high pattern of attenuation homogeneous inhomogeneous glandular size normal increased decreased margin smooth lobulated degree of enhancement isodecreased increased pattern of enhancement homogeneous inhomogeneous data are number of items , with percentage in parentheses ct computed tomography results of the 28 patients , the initial ria dose ranged from 100 to 180mci ( meansd , 157.524.4mci ) as follows : 100mci ( n = 3 ) , 150mci ( n = 11 ) , 160mci ( n = 3 ) , and 180mci ( n = 11 )  . 
of the 28 patients , all underwent 1 or more sessions of follow - up neck us ( mean session 3.61.5 ; range 16 ; mean interval 40.719.2months ; range 670months )  . 
based on comparison of the us and ct features of the parotid glands , 23 parotid glands in 13 patients ( mean age 49.214.7years ; age range 1770years ) were found to show post - ria changes ( mean interval 37.926.7months ; range 1283months )  . 
the mean hu value of parotid parenchyma with post - ria changes on nonenhanced and enhanced ct was 26.5 ( range from 63 to 15 ) and 24.2 ( range from 59 to 109 ) , respectively . 
mean hu values of the parotid parenchyma without post - ria changes on non - enhanced and enhanced ct were 20.1 ( range from 45 to 10 ) and 35.6 ( range from 25 to 95 ) , respectively . 
of the ten parotid glands in six patients with positive us and negative ct features , nine parotid glands in five patients had a short interval between ria and neck ct examination ( mean 10.47.0months ; range 119months ) , whereas for one parotid gland in one patient , there was a 38 - month - interval between these examinations . 
of the two patients with negative us and positive ct features , one parotid gland in one patient showed only increased parenchymal enhancement on a short - interval ct ( 9months after ria ) , whereas one parotid gland in the other patient revealed only a lobulated margin on ct . 
based on the us and ct features , the former case was determined as an early stage of post - ria changes , whereas the latter case was determined as representing a normal parotid gland . of the 56 submandibular glands in 28 patients , 8 submandibular glands in 5 patients ( mean age 48.614.6years ; age range 2664 years ) showed post - ria changes . 
the common ct features of post - ria changes in the submandibular gland included isoand homogeneous parenchymal attenuation , decreased glandular size , a lobulated margin , iso - enhancement , and an inhomogeneous enhancement pattern . 
the mean hu value of the submandibular parenchyma with post - ria changes on non - enhanced 1 3 26 radiol med ( 2018 ) 123 : 2027 and enhanced ct was 32.811.0 ( range from 15 to 45 ) and 121.040.7 ( range from 34 to 162 ) , respectively . 
the mean hu value of the submandibular parenchyma without post - ria changes on non - enhanced and enhanced ct was 39.411.6 ( range from 4 to 67 ) and 129.023.2 ( range from 84 to 211 ) , respectively . 
however , a cutoff hu value between submandibular glands with post - ria changes and normal submandibular glands was not determined , due to a considerable overlap . discussion all msgs are involved in the transport of radioactive iodine into the saliva [ 1 ]  . 
the parotid gland is the most active , and its serous cells apparently have a greater capacity for concentrating radioiodine than mucous cells [ 1 , 8 , 9 ]  . 
in the current study , the prevalence of post - ria changes in the parotid glands was much higher than that in the submandibular glands on both us and ct . 
furthermore , bilateral gland involvement was more common than unilateral involvement . in the literature , the common us features of post - ria changes included a coarse echotexture , decreased echogenicity , a lobulated margin , and a decreased glandular size [ 6 ]  . 
in the current study , the common ct features of post - ria in the parotid gland included low parenchymal attenuation , decreased glandular size , a lobulated margin , decreased or increased parenchymal enhancement , and an inhomogeneous enhancement pattern . 
this may be correlated with pathological findings of post - ria changes , including the initial radiation - induced duct damage , subsequent acinar destruction , and combined fatty degeneration . 
in the current study , glandular atrophy was observed in the chronic phase , whereas normal glandular size or mild glandular enlargement was found in the acute phase . senile msgs may have characteristics similar to those of msgs showing post - ria changes on ct . 
in the current study , post - ria changes tend to involve a marked decrease in the glandular size , whereas senile msgs without postria changes tended to have a normal glandular size . 
however , the author hypothesized that post - ria changes showed moderate glandular atrophy because of profuse fatty degeneration after the initial radiation - induced duct damage and subsequent acinar destruction , unlike senile msgs . 
in practice , the coexistence of a history of ria after total thyroidectomy and the presence of ct features of post - ria changes in msgs can allow differentiation from senile msgs and other glandular diseases . this study has several limitations . 
third , the author could not investigate the degree and pattern of parenchymal attenuation in 26 parotid glands because of lacking ct images ( a ct scan level from the mandibular angle to the sternum on non - enhanced ct )  . 
 in particular , a single radiologist subjectively determined the glandular size on the basis of a comparison between ipsilateral and contralateral msgs or the interval change in glandular size between preoperative and post - ria neck cts . in conclusion , the common ct features of post - ria changes in msgs include decreased glandular size , a lobulated margin , and an inhomogeneous enhancement pattern . 
 thus , awareness for ct features of post - ria changes in msgs may be helpful for differentiating post - ria changes from senile msg or other msg disease on ct . author contributions concept and design : dwk . 
hereafter , i use the term abnormally invasive placenta ( aip ; accreta , increta , percreta ) instead of accretism and total placenta previa instead of major placenta previa , according to the world standard nomenclature . first , uae may be an over - treatment for patients with total placenta previa without suspicion of aip . 
their inclusion criteria were radiological diagnosis of placental anomalies ( previa or aip ) and risk factors for peri / postpartum hemorrhage ( previous cesarean deliveries , uterine curettage , and advanced age )  . 
previous studies indicated that bleeding amount was large in some total placenta previa even without aip , anterior placental location [ 2 ] or short cervical length [ 3 ] is its example . 
without some such criteria , we cannot determine for whom predelivery uae is effective . second , forcible removal of the placenta followed by some hemostatic procedures in aip , referred to as extirpative approach , is now almost abandoned at least for planned surgery because it caused marked bleeding and hysterectomy [ 4 ]  . 
employed intrauterine - hemostatic balloon after placental removal ; however , forcible placental removal is technically impossible , or at least very difficult , in percreta , and hemostatic balloon may not be useful since the uterine wall is usually ruptured / torn off . 
this may be due to marked heterogeneity of placenta previa and vol . : ( 0123456789 ) 1 3 80 radiol med ( 2018 ) 123 : 7980 aip , which giurazza etal . 
mean bedvh for both bladder * paolo borghetti paolobor82@yahoo.it 1 radiation oncology department , spedali civili hospital andbrescia university , piazzale spedali civili 1 , it - 25123brescia , italy 2 medical physics department , spedali civili hospital , brescia , italy ( p < 0.01 ) and rectum ( p < 0.05 ) were also significantly better for volumetric modulated arc therapyimage guided radiotherapy ( vmatigrt ) plans than for 3dcrt plans . conclusion art is better than srt in terms of brfs and os , particularly for more aggressive cases , advanced t stage and higher gleason score . 
in the usa , this has contributed to the release of joint guidelines by urologists and radiation oncologists aimed at sharing recommendations based on evidence in this context [ 4 ]  . 
art should be offered to patients with adverse pathological findings at prostatectomy , including seminal vesicles invasion ( svi ) , positive surgical margins ( psm ) or extracapsular extension ( ece )  . 
salvage postoperative radiotherapy ( srt ) should be considered in case of biochemical or local recurrence , without evidence of metastatic disease , in patients with confirmed prostatic specific antigen ( psa ) at 0.2ng / ml or higher or local recurrence . despite these recommendations [ 46 ] , debate continues on the role and timing of postoperative radiotherapy in prostate cancer , fueled by the risk of overtreatment or of excess of toxicity . 
 however , this meta - analysis presented limitations , due to the heterogeneous inclusion of retrospective and randomized studies , different doses and modality of radiotherapy compared to recent practice , insufficient information about adverse events and , finally , different combinations with androgen deprivation therapy ( adt ) [ 7 ]  . to date is possible to stratify patients for disease recurrence after prostatectomy , e.g. , using kattan nomograms , to identify the cases that could really benefit of art . 
this nomogram is based on a scoring system considering surgical margin status , svi , ece , lymph node invasion , primary and secondary gleason score ( gs ) and preoperative psa level to predict 10 - year biochemical progression - free rate [ 8 ]  . in addition , since the majority of prostate cancer patients have a good prognosis , much attention has been devoted to the toxicity profile of adjuvant treatment and quality of life . 
 different highly conformal radiotherapy techniques such as intensity modulated radiotherapy , volumetric modulated arc therapy , helical tomotherapy [ 9 ] and image guided radiotherapy ( igrt ) [ 1012 ] seem to provide an advantage in sparing rectum and bladder with a significant reduction of toxicity . aim of the present analysis is to evaluate biochemical relapse - free survival ( brfs ) , overall survival ( os ) , late rectal and bladder toxicities in a retrospective single institution series , also by applying an in - house software able to import all the individual dose - volume histogram ( dvh ) in a database and to perform descriptive and inferential statistical analysis of mean dvhs pertaining to the different techniques and for the different volumes of interest . materials andmethods from 1999 to 2012 , 508 consecutive patients were submitted to radiotherapy after radical prostatectomy at our institution . 
in addition , for 102 more cases , dvh were missing , because many of the oldest patient files were stored in a treatment planning system no longer used and were often corrupted or not retrievable . 
postoperative radiotherapy was defined as adjuvant ( art ) when the psa level was undetectable ; on the contrary it was defined as salvage ( srt ) when psa resulted 0.2ng / ml or higher . 
 physical examination and psa measurements were regularly carried out during follow - up ; late rectal and bladder toxicities were registered according to common terminology criteria for adverse effects ( ctcae ) , version 4.0. 
in particular proctitis , colitis , diarrhea , non - infective cystitis , urinary incontinence and retention were considered but only proctitis and non - infective cystitis were analyzed because more frequent and clinically relevant . 
data on toxicities were obtained from medical records of patients that include routinely urinary and gastrointestinal symptoms reported by patients ( and their severity ) at each follow - up visit . 
timing of follow - up was usually every 3months the first year , every 6months for further 3years and every year for the rest of follow - up ; patients that reported toxicities had personalized follow - up . for this analysis , biochemical relapse - free ( brfs ) and overall survival ( os ) were calculated from the radical prostatectomy date to that of biochemical relapse ( psa confirmed higher than 0.2 ng / ml in at least two subsequent measurements ) , or to the date of death for any cause , respectively . differences between groups were calculated using the log - rank test . 
however , thanks to the prodvh software , we tried to identify more subtle differences in the bedvh profile , possibly originating differences in clinical toxicity not otherwise explainable . mean bedvhs of rectum and bladder were elaborated and analyzed within clinically relevant groups , such as rectal and bladder toxicities grade ( g0g1 vs g2g3 ) , to assess possible relationships with dosimetric data , dose prescription ( 66gy vs 70gy ) and radiotherapy technique ( 3dcrt vs vmatigrt ) because these factors could affect dvhs . 
bedvhs obtained with the prodvh software were compared with anova test for three group comparisons and t student test for two group comparisons ; a p value < 0.05 was considered statistically significant . 
prodvh software collects bedvhs of every single plan to generate an average bedvh resulting in a distribution of data comparable point by point with statistical tests along the whole bedvh profile and not only according to specific points . all the plans analyzed were within the dose constraints applied at our institution ( for bladder : v6550% , v7035% ; for rectum : v50 < 60% , v70 < 20% )  . 
it is worth noting that only 4 of the patients experienced g3 proctitis and 5 g3 noninfective cystitis . prodvh although all the plans we analyzed comply with the institutional constraints without major violations , we compared mean bedvhs ( the mean was calculated on volume values for each dose )  . 
the thick lines represent the average dvhs the thin lines are average 1 sd group ( g0g1 vs g2g3 ) did not show any statistically significant difference . mean bedvhs of bladder , rectum and ptv were also evaluated in terms of radiotherapy technique ( 3dcrt vs vmatigrt )  . 
likewise , in terms of rectum mean bedvhs , vmatigrt resulted significantly better ( p < 0.05 ) throughout all the dose spectrum ( except an inversion between 39 and 44gy )  . 
bladder bedvh profile was significantly different from low doses up to 38 gy and from 45 gy up to 65 gy ( p < 0.05 ) ; in both dose regions vmatigrt plans allowed to obtain the inclusion of a smaller bladder volume . 
since a recent debate in the literature raised the issue that this result might be biased because of lag time bias , survivals were calculated from surgery , to assess the real benefit of postoperative radiotherapy [ 18 , 19 ]  . 
doses ( in the range 1 3 radiol med ( 2018 ) 123 : 6370 6670gy ) and ptv volume did not result significantly linked to late toxicity . this study is flawed because of its retrospective nature ; however , the results presented confirm the data derived from three randomized controlled trials [ 13 ] and from a recent meta - analysis [ 5 ]  . 
despite this , a gap between evidence and practice in this setting is noted [ 20 , 21 ] and one reason could be related to the worries about toxicities . in terms of dose constraints , several data are available to predict toxicity grade [ 2225 ] , but they remain a relatively broad suggestion , often unable to explain specific trends in selected subgroups . 
in this study , prodvh was applied to a retrospective analysis to test its reliability to investigate correlations between clinically relevant features ( toxicity grade , ptv volume , dose level and radiotherapy technique ) and mean bedvh . although all treatments were planned according to our institutions dvh constraints , as already stated , the actual patients plans had different dosimetric outcome . 
the use of prodvh , and particularly of the tool to evaluate and compare mean bedvh , allowed to compare the whole dvh profile , thus overcoming the limits of a comparison merely considering differences in standard dvh points . 
the statistically significant differences outlined in fig.2 demonstrate that reducing dose to rectum gives a benefit in terms of toxicity reduction , regardless of whether all plans were within dose constraints . the results , as reported in fig.2 , show that mean rectum bedvh , across the whole dose range ( 472gy ) , was significantly related to the grade of rectal toxicity ( g0g1 vs g2g3 )  . 
bedvhs for organs at risk seemed significantly related to radiotherapy technique ; vmatigrt technique obtained better planning and clinical results regardless of the dose level ( 6670gy ) and when the comparison with 3dcrt plans was restricted to patients with similar ptv volume to avoid the possible bias represented by a smaller set up margin applied when igrt was used . 
this minimal difference could , however , be attributed to a different modality of elaboration and optimization of plans , based on the choice of the 95% isodose as the minimum isodose covering ptv in 3dcrt technique rather than accepting the mean dose closer to dose prescription for vmat plans . this experience demonstrates the importance of combining clinical results extrapolated by retrospective databases with dvh data . 
however , the data obtained with the average dvh analysis also support the conclusion that a further improvement of the cost / benefit ratio of the treatments is possible . conclusions the results of this study on postoperative prostate cancer radiotherapy are twofold : a reappraisal of the differences in outcome between art and srt and an evaluation , in this clinical model , of a new modality of treatment plan evaluation and comparison . the study data , although limited by their retrospective nature , support the conclusion that postoperative prostate cancer radiotherapy should be applied as soon as possible after surgery , since the policy of deferring treatment until a biochemical relapse is evident might be related with worse survival results . the prodvh software allows to identify average or reference dvhs , representative of dvh families with peculiar clinical correlates . 
a proof of principle has been , therefore , obtained that such reference dvh could be compared to that of the individual patient in the attempt of more efficiently predicting ( and avoiding ) toxicity . 
this could be helpful also in the setting of postoperative prostate cancer radiotherapy , where the toxicity of treatment should be carefully balanced against the expected advantages in outcome . compliance with ethical standards conflict of interest statement all authors disclose any actual or potential conflict of interest including any financial , personal , or other relationships with other people or organizations within 3years of beginning the submitted work that could inappropriately influence , or be perceived to influence , their work . ethical standards this article does not contain any studies with animals . 
cardarelli 9 , 80131naples , italy 4 biomedical instrumentation andmeasurements lab , universit campus bio - medico di roma , via alvaro del portillo 200 , 00100rome , italy 5 physic department , aorn cardarelli di napoli , via a . 
cardarelli 9 , 80131naples , italy vol . : ( 0123456789 ) 1 3 72 radiol med ( 2018 ) 123 : 7178 procedure ; this may represent a technical alternative that interventional radiologists can consider when facing this challenging scenario . keywords uterine arteries embolization predelivery placental implant anomalies microparticles mri introduction in the last decades , the rate of cesarean deliveries has continuously increased in western countries [ 1 , 2 ] ; as a consequence , the rate of placental implant abnormalities is increasing because of the anomalous implant point of the following pregnancies on the previous uterine scar [ 3 ]  . these pathological implants , whether concerning the site ( placenta previa ) or the depth ( placenta accreta ) , are a blown risk factor in severe bleeding during the delivery , because the placenta is richly vascularized and does not completely detach . therefore , abnormally invasive placenta is now considered one of the leading causes of severe post - partum hemorrhage and emergency hysterectomy ; it has been associated with maternal morbidity and mortality rates up to 60 and 7% , respectively [ 4 ]  . it has longly been accepted that only hysterectomy could be the definitive treatment [ 57 ] ; however , in the last decade , innovative approaches have been developed to attempt a conservative uterine management and especially reduce blood loss by combining surgery and endovascular techniques . 
on the basis of the technical knowledge previously acquired from fibroids [ 8 ] and post - partum hemorrhage embolizations [ 9 ] , in the obstetrical environment , the prophylactic role of interventional radiology procedures is rapidly gaining interest in facing these challenging clinical conditions [ 7 , 1019 ] ; different methods have been reported : predelivery uterine arteries ( ua ) catheterization , balloon catheter positioning , preor post - delivery prophylactic embolization . 
until now , a univoque protocol has still not been accepted . the aim of this paper is to report on a single center experience of managing patients affected by abnormal placental implants by embolizing ua immediately before the scheduled cesarean delivery : the main goal was to reduce the blood loss ; the secondary goal was to reduce the rate of hysterectomies . materials andmethods inclusion criteria were radiological diagnosis of placental anomalies and risk factors for peri / postpartum hemorrhage ( previous cesarean deliveries , uterine curettage , and advanced age )  . 
subsequently , the contralateral hypogastric artery was catheterized with the same 5fr cobra catheter and another small bolus ( 35ml ) of diluted contrast agent was injected to visualize the origin of the uterine artery . 
1 30 - year - old woman at the 32nd week of pregnancy , one previous cesarean delivery ; coronal ( a ) and sagittal ( b ) t2 - weighted fast spin echo sequences showing placenta previa maior ( white continuous arrows ) and accreta ( white dotted arrows ) fig . 
2 36 - year - old female affected by placenta accreta , one previous cesarean delivery ; right ( a ) and left ( b ) uterine artery embolization ; the arrows show the tip of the 5fr catheter ( black ) , the tip of the 2.7 fr microcatheter ( grey ) and the embolizing agent ( white )  . 
3 33 - year - old female affected by placenta previa maior and percreta , two previous cesarean deliveries ; left ( a ) and right ( b ) uterine artery embolization ; the arrows show the tip of the 5fr catheter ( black ) , the tip of the 2.7fr microcatheter ( grey ) , and the embolizing agent ( white )  . 
 this patient underwent to hysterectomy 1 3 74 radiol med ( 2018 ) 123 : 7178 deep placental accretism , massive bleeding , severe uterine atony , or organ compromise . and t1 - weighted fat - suppressed sequences preand postcontrast injection . after the delivery , the intrauterine hemostasis balloon all data analyses were performed in a matlab enviwas positioned in all patients preserving the uterus . ronment ( mathworks , inc , natick , massachusetts )  . blood units transfusions were performed for hemoglobin values < 7g / dl and / or pronounced pallor . the femoral introducer was removed the day after the results delivery . sir and cirse guidelines for the use of radiations during pregnancy [ 20 ] were strictly followed and the fluoroscopy protocol was standardized to obtain the best compromise between image quality and radiation dose : low - dose rate pulsed fluoroscopy with a low pulse rate ( 7.5pulses / s ) ; no angiography exposure ; last image hold technique to plan the embolization ; no enlargement of the field of view ; half - dose filter ; single postero - anterior beam projection ; maximal distance of the x - ray tube from the patient ( 40cm ) ; tube current as low as possible by keeping the tube potential as high as possible . 
 the mean time occurring between the end of the endovascular procedure and the accomplishment of the cesarean delivery was 6 min ( range 4 min 38 s7 min 17s )  . no ph anomalies were measured from the umbilical cord blood ; the apgar score at 5min was 8 . neonatologists evaluated the children 6 months after the delivery by applying the bayley - iii scale test . 
the analysis of the neurodevelopmental milestones showed normal cognitive development in all children . the uterine wall enhancement was evaluated in the subgroup of 10 patients analyzed with contrast - enhanced mri 6 months after the embolization procedure . 
 to prevent this challenging scenario , different endovascular approaches have been reported in patients considered at high risk of post - partum bleeding because of concomitant placental implant anomalies ( table 2 )  . 
diagnostic angiography ( a ) of the left hypogastric artery ( black arrow showing the tip of the 5fr catheter ) showed bleeding from the stumps of the uterine artery . 
in addition , the right side ( c ) was evaluated ( black arrow shows the tip of the 5fr catheter distally positioned into the anterior branch of the hypogastric artery ) and contrast agent extravasation was appreciable ( white arrow )  . 
the patient required transfusion of eight blood units and was transferred to the intensive care unit 1 3 76 radiol med ( 2018 ) 123 : 7178 table 2 comparison with the previous published studies about predelivery approach in patients with placental implant anomalies authors year sample embolization technique blood loss / transfusions hysterectomies ( % ) izbizky etal . 2015 95 pts with suspected accretism bd : ua catheterization 14% large - volume blood loss dsouza etal . 
 [ 14 ] treated 95 patients with suspected placenta accrete by predelivery bilateral uterine artery catheterization and embolization after delivery : they reported 14% of the patients receiving large - volume blood transfusions and 83% hysterectomies . 
described another approach consisting of positioning an aortic balloon before the delivery and then to proceed with embolization of ua after delivery [ 13 ] on 42 patients with placenta praevia and accreta ; they reported only one case of hysterectomy and an average amount of blood transfusion of 42283ml . in a recent study , niola etal . 
 [ 15 ] first reported on predelivery embolization with reabsorbable agent ( spongel ) just before the cesarean delivery in a cohort of patients affected by placenta previa or accretism : in this study , 64% of the patients did not require transfusions with an overall mean rate of 0.7 blood units transfused ; hysterectomy was performed in 26% of the sample . 
because of the wide uterine arteriosus collateral flow in pregnancy [ 26 ] , the risk of uterine necrosis is avoided as confirmed on the subsample of patients evaluated at 6months with mri . 
furthermore the embolization is intended to reduce the blood flow into the uterine artery and not to completely stop it , compared to fibroids treatment technique [ 8 ] : this is a crucial aspect to avoid foetal hypoxia in the time occurring between the end of the endovascular procedure and the cesarean delivery . balloon occlusal catheters in the hypogastric arteries have not been considered in this study according to the controversial and mixed results reported in the literature in this category of patients ; balloon occlusal catheters do not appear to reduce operative time or length of hospital stay [ 25 ]  . 
in addition , as reported by pelage , fohlen , and le pennec [ 9 ] , the systematic preoperative placement of arterial occlusion balloons is not recommended in the management of abnormal placentation . experienced operators ( > 5years in the field of endovascular and surgical management of obstetrical pathologies ) , both interventionalists and surgeons , performed these procedures : indeed , this study was performed in a tertiary care 1 3 radiol med ( 2018 ) 123 : 7178 center in the italian region with the most elevated rate of cesarean deliveries ( 59.5% of all deliveries in 2012 ) [ 27 ]  . the monolateral femoral approach has been privileged , because it implies one arterial puncture and an easier management of the patient , both during surgical manipulation in course of the cesarean delivery and during the postprocedural recovery : in the study protocol , the introducer has been removed only the day after . 
in the literature , studies reporting both monolateral and bilateral femoral approaches have been described , but no data to discern the best technique are available according to our knowledge . the most commonly adopted curve to catheterize the hypogastric artery in this study has been the cobra curve ; other curves are available and the choice mainly depends on the operator personal confidence . 
the robert uterine catheter curve in this scenario has been avoided because of the long loop of its shape : this would imply moving the c - arm on the abdominal aorta during the procedure with consequent prolonged fluoroscopy time . according to the cirse guidelines for fibroids embolization [ 8 ] , to reduce the risk of arteriosus spasms , a microcatheter has been always adopted to catheterize the horizontal portion of the uterine artery ; the 5 fr catheter was positioned into the hypogastric or at the origin of the ua . even if the risk of developing hypothyroidism in newborns has been suspected , no consensus is present in the literature and published studies reported no ill effects on neonatal thyroid function [ 2931 ] ; the iodinated contrast agent injected has been carefully reduced as much as possible . a relevant issue of all the predelivery approaches is the radiation dose to the foetus . 
at the end of the third trimester , the lifetime cancer risk after an in utero radiation dose of 100 mgy is the same as for a child exposed to similar radiation levels up to the age of 10years [ 32 , 33 ] ; the risk of childhood cancer increases after a dose of 10mgy , and therefore , this should be reduced as much as possible . 
for this purpose , in this study , the cirse guidelines for the use of radiation during pregnancy [ 20 ] have been strictly followed . patients with placental implant anomalies are usually candidate to hysterectomy ; a recent literature review examining 34 studies published between 1977 and 2012 reported that blood transfusions may be required in 2070% of cases with similar values for hysterectomies performed after delivery [ 34 ]  . in this study , only patients at high risk for post - partum hemorrhage have been enrolled . 
in terms of blood units transfused and hysterectomies , patients affected by placental accretism presented a worst outcome compared to patients only affected by placenta previa maior . furthermore , the prophylactic approach has already proven to be a cost - effective strategy according to the italian national health service budgets , with reduced hospital stay and intensive units recoveries [ 35 ] ; this should be another aspect to consider . this study presents some limitations . 
first of all , the sample is small ( 69 patients ) , and from a single center with miscellaneous severe placental anomalies and because of this , no subgroup analysis for specifical placental anomaly neither a comparison with a control group of patients not embolized before predelivery has been conducted . 
 this approach requires that the embolization procedure is strictly performed in a gynecological operating room , because the cesarean delivery must be performed immediately after the endovascular procedure to avoid foetal hypoxia ; therefore , the operative setting requires mandatorily the availability of a c - arexperienced operators and a strong multidisciplinary partnership with gynecologists and neonatologists are crucial elements . 
before attempting this technique , operators should be confident with uterine arteries microcatheterization and microparticles injection in the field of gynecological and obstetric endovascular procedures ; embolization first of uterine leiomyomata and then of post - partum hemorrhages should be part of the learning curve as well as ease with low - dose fluoroscopic images . 
fetal mri plays an increasingly important role in the prenatal diagnosis of fetal neck , chest and abdominal malformations , even if its role has been amply demonstrated , especially , in the field of fetal cns anomalies . 
 due to its multiparametricity and multiplanarity , mri provides a detailed evaluation of the whole fetal respiratory , gastrointestinal and genitourinary systems , especially on t2 - weighted ( w ) images , with a good tissue contrast resolution . 
in the evaluation of the digestive tract , t1 - w sequences are very important in relation to the typical hyperintensity of the large intestine , due to the presence of meconiuthe objective of this review is to focus on the application of fetal mri in neck , chest and abdominal diseases . keywords fetal mri prenatal diagnosis body malformation neck malformation chest malformation abdominal malformation urogenital malformation introduction us is the first imaging modality of investigation , but as well - known it has some limitations , in particular , when there are such factors as oligo - / anhydramnios , gestational age , maternal obesity and complex malformations . 
in this regard , fetal mri finds its application , and its role has been amply demonstrated , especially , in the field of fetal cns anomalies [ 1 , 2 ]  . fetal mri is a level iii diagnostic tool , performed subsequently as a level ii prenatal ultrasound ( us )  . 
some scientific societies have recently published guidelines regarding fetal mri , based on clinical and scientific evidences [ 4 ]  . the objective of this review is to focus on the application of fetal mri in neck , chest and abdominal diseases . search criteria a structured pubmed search was performed starting in december 2016 including all relevant original and review articles published in and after year 2000 . 
a total of 420 papers on human subjects published in english were included and then evaluated for their content and relevance ; case reports were excluded . 92 articles were used as the literature basis of this review . 
 we describe imaging techniques , recent developments , common clinical indications and safety issues about mri of the fetal body . technique andprotocols the study protocol includes primarily t2and t1 - weighted ( w ) sequences ; names and acronyms for these sequences vary among the mr manufacturers ( table1 )  . 
t2 - w fast or turbo spin - echo sequences represent the standard sequence for a fetal mri examination using single repetition time ( tr single shot ) acquiring a single slice . 
commercially , this sequence is known as half - fourier acquisition single - shot turbo spin echo ( haste ) ( tr 1000ms , te 119ms , slice thickness 3mm , fov 203270mm , matrix 256134 , flip angle 150 ) or single - shot fast spin echo ( ssfse ) or single - shot turbo spin echo ( sstse )  . 
the slice must be thin ( 34mm ) with axial , sagittal and coronal orientations orthogonal to the organ / area of interest to provide detailed evaluation of fetal anatomy [ 5 ]  . thanks to single - slice acquisition , artifacts related to fetal motion are reduced . 
in particular , this kind of sequence enhances the static fluid signal and focuses on fluid anatomical structures ( fetal nasal and oral cavities , pharynx , trachea , stomach , proximal intestine , urinary tract , gallbladder , lungs and amniotic fluid ) [ 6 ]  . breath - hold gradient - echo ( ge ) sequences with the ssfp ( steady - state - free - precession ) ( true - fisp ) ( tr 3ms , te 1ms , slice thickness 4mm , fov 400300mm , matrix 256144 , flip angle 60 ) are frequently employed in all cases of excessive fetal motion causing artifacts . 
t1 - w imaging with and without fat suppression ( fs ) are acquired during breath - holding ( tr 6ms , te 3ms , slice thickness 3.5mm , fov 500313mm , matrix 256112 , flip angle 10 )  . 
two different types of t1 - w sequences are generally used : ge with short tr and timeecho ( te ) and fast spin echo ( fse - t1 )  . 
these sequences provide information about the microscopic brownian motion of free and bonded water molecules in biological tissues , thus are useful to study pulmonary and renal maturity on late gestational age . apparent diffusion coefficient ( adc ) maps are reconstructed and adc values are measured in correspondence to the region of interest ( roi )  . 
this is helpful to display ectopic kidneys , small kidneys , bilateral renal agenesis and to evaluate normal renal growth [ 8 ]  . neck anomalies the most common fetal neck abnormalities are , according to frequency , teratoma , cystic lymphatic malformation and hemangioma ; the differential diagnosis should include less frequent lesions such as cervical thymic cyst and neuroblastoma . 
fetal mri is crucial to study the nature of the lesion ( cystic , vascular , neoplastic , etc . ) and its extension : in fact , it is a significant diagnostic tool because it can determine the severity of the malformation studying its extension and visualizing if the lesion is confined to the neck or it invades the mediastinum . furthermore , it is decisive to discriminate if those neck lesions compress important anatomical structures such as trachea or esophagus . 
thus , through the assessing of the invasion or compression severity , fetal mri is important to assess prognosis and to plan a consequent in uteroor postnatal treatment [ 9 , 10 ]  . the extension of a neck mass and the visualization of the upper airway may be difficult on us . 
t2 - w fetal mr imaging shows the typically hyperintense fluid - filled airway and could help in the correct assessment of the severity of the obstruction , its extension into mediastinum and eventually detecting esophageal and / or vascular compression which could impair prognosis [ 11 ]  . lazar described the tracheoesophageal displacement index ( tedi ) to provide a score to classify fetal airway displacement and found out that a tedi > 12mm is associated to a poorer prognosis at birth . 
on mr images , ch may have areas of heterogeneity and flow voids [ 17 ]  . heart pathologies congenital heart disease ( chd ) : echocardiography represents the gold standard examination for fetal heart disease [ 18 , 19 ]  . 
however , american heart association included its application in the diagnostic routine of chd [ 20 ] ; in fact , recent studies suggested that fetal mri can identify hemodynamic change in case of chd through t2 mapping of venous blood on umbilical vein [ 21 ]  . the standard fetal heart protocol is different from the one applied on lung and abdomen and includes two phases : static and dynamic phases . 
direct signs are cardiac situs , cardiothoracic index , volume and conformation of chambers , myocardial anomalies , malposition of the cardiac axis ( normal : 45 ) , septal defects and vascular abnormalities . 
indirect signs are the absence of anatomical structures such as valves and the presence of cardiomegaly and / or pericardial effusion ; in particular , the last two signs refer to pathologies that could also origin from systemic diseases . 
coronal ( a ) and axial ( b ) haste t2 - weighted images of a fetus with left cystic lymphatic malformation of the neck ( white arrowhead ) with extension to the mediastinuthe trachea is dislocated but patent ( b , white arrow )  . 
coronal ( d ) haste t2 - weighted image shows a hypo - / isointense teratoma of the neck , which is hyperintense on dwi ( e ) and hypointense on adc map ( f )  . 
a sagittal t2 - weighted image shows the mass inside the oropharynx with a patent trachea ( g ) prenatal echocardiography , even though mri with the flow void sign could be helpful [ 23 , 24 ]  . crucial to select fetuses for the ex utero intrapartum therapy ( exit ) procedure [ 31 ]  . in addition , fetal brain evaluation should be proposed in fetuses affected by chd because recent studies have suggested an association between severe chd index of altered brain growth and enlarged cerebrospinal fluid spaces [ 25 ]  . chest pathologies fetal mri is a useful tool in the assessment of chest malformation , because mr imaging can study lung parenchyma using t2 - wi to visualize the anatomy and morphology . 
in the last years , the role of mri is gaining importance with dw imaging because through this sequence it is possible to evaluate lung physiological parenchymas maturation in different gestational ages , considering that evidences suggest that adc values increase with the aging of the pregnancy [ 2629 ]  . most of chest malformations that we are going to describe have a characteristic particular hyperintense signal on t2 - wi . 
several methods have been suggested to measure fetal lung volumes on mri [ 3638 ] , but the most common is tracing the region of interest ( roi ) around the residual lung , usually on the axial plane [ 32 , 39 , 40 ] and then multiply it by the slice thickness . 
however , the most recognized approach to determine outcome prediction for fetuses with cdh is the measurements ratio , the observed fetal lung volume ( oflv ) or the expected fetal lung volume ( eflv ) [ 31 , 32 ]  . 
some authors proposed standardized measurements of the lung volume and its correlation to outcome for other thoracic abnormalities such as cpam , creating the cpam volume ratio ( volume of the mass divided by the fetal head circumference ) , based on us measurements [ 41 ] , and the mri lung mass volume ratio [ 38 , 42 ]  . congenital pulmonary airway malformation ( cpam ) ( fig.3 ) : known as congenital pulmonary adenomatoid malformation ( cpam ) is the most common lung malfor1 3 la radiologia medica ( 2018 ) 123 : 271285 fig . 
the lesion has heterogeneous signal intensity , with internal flow voids due to the presence of vessels surrounded by solid hyperintense component , leading to the diagnosis of a neck hemangioma . 
coronal ( c ) and axial ( d ) true - fisp images show dilation of the subarachnoid spaces ( c ; black arrows ) severe dilation and wall thickening of the right sided cardiac chambers ( d ; black arrowheads ) , due to the presence of an arteriovenous fistula inside the neck hemangioma . 
it is classified into five types going from hyperintense unilocular or multilocular region with thin wall ( type ione or more cysts > 2cm , or type iimultiple cysts ranging from 0.5 to 2cm ) to an homogeneous solid mass ( type iiimicrocystic / solid type , with cysts < 0.5cm ) [ 44 , 45 ]  . 
bronchogenic cysts are typically isolated close to the mediastinum but in some cases the cyst is intra - parenchymal ; in these cases a correct differential diagnosis may not be possible in the prenatal period . 
the vascularization is an important factor to differentiate between cpam type i ; and bps : bps is supplied from the systemic circulation cpam type i by pulmonary artery branches . bronchopulmonary sequestration ( bps ) : it is the second most frequent lung malformation and it is characterized by the presence of abnormal pulmonary tissue not connected to the tracheobronchial tree . 
 it appears as a well - defined homogeneous solid mass , hyperintense on t2 - w [ 50 , 51 ]  . congenital lobar overinflation ( clo ) : ( fig.4 ) it is an overinflation of a lung segment or lobe , caused by a bronchial obstruction , of intrinsic or extrinsic origin that leads to severe alveolar overdistension [ 52 ]  . 
 usually a dilated tubular structure at the hilum on mri consistent with a dilated bronchus is a typical finding of this condition [ 53 , 54 ]  . congenital bronchogenic cyst : on mri it appears as a fluid lesion with thin walls , usually located near the tracheal carina . 
it is similar to ccam type i and the signal intensity depends on the cystic content and it is usually hyperintense on t2 - wi and variable on t1 - wi [ 35 ]  . congenital high airway obstruction syndrome ( chaos ) : it is caused by obstruction of the larynx or trachea , which could be of intrinsic or extrinsic origin , leading to the trapping of lung fluids and tracheal dilatation [ 55 ]  . 
sagittal t2 - w image ( a ) shows a marked hyperintensity and enlargement of the superior lobe of the left lung ( back arrowhead , a ) , excluding the apical segment ( white arrow ; a ) , which determines right shift of the mediastinum ( b , white arrowhead ) ; axial true - fisp image ( c ) shows normal inferior left lobe ( seen posteriorly , c ) , hyperintensity and enlargement of the superior left lobe and mediastinal shift ( white arrowhead , c )  . 
t2 - weighted haste images on axial ( a ) , sagittal ( b ) and coronal ( c ) planes showing enlargement of the right lung ( r ) with solid appearance . 
in the first one , the abnormality is usually located at the level of the mainstem with dilation of the distal lung [ 59 ] , which can compress the mediastinum and the contralateral normal lung . 
posterolateral hernias are the most common types ( 7075% ) , the majority occurring on the left side ( 85% ) ; in this case , the thorax may contain small and large bowels , spleen , stomach , left lobe of the liver , and occasionally , homolateral kidney . 
less frequently , hernias occur on the right side and usually contain part of the right lobe of the liver and sometimes the bowel and / or the right kidney ( 13% )  . 
cdh is associated with various degrees of pulmonary hypoplasia and severe persistent pulmonary hypertension of the newborn with high risk of mortality [ 66 ]  . in addition , other malformations that further complicate the clinical course may be present . 
 coronal ( a , b ) and axial ( c ) haste t2 - weighted images show herniation of abdominal structures ( white arrowhead ) on the left hemithorax ; the left lung is reduced in volume and compressed ( white circle )  . 
the liver and stomach are not herniated ( white arrow ) , whereas the spleen ( black circle ) is dislocated inside the thorax along with small bowel loops and the colon , which is hyperintense on t1 - weighted image ( black arrows , d ) due to the presence of meconiucoronal ( e ) and sagittal ( f ) haste t2 - weighted images of another fetus with cdh which show herniation of the left lobe ( white circle ) of the liver ( liver up ) inside the thorax . 
t1 - weighted image shows hyperintensity in the left hemithorax due to the presence of colon ( black arrows , g ) 1 3 278 la radiologia medica ( 2018 ) 123 : 271285 malformations , including atrial septal defects and the coarctation of the aorta , are the most frequent anomalies observed in fetuses and newborns with cdh ; gastrointestinal malformations , such as meckel diverticulum and anal atresia , are the second largest group of malformations in neonates with cdh . 
cdh is also associated with musculoskeletal and craniofacial malformations , such as auricular dysplasia , aplasia of the radius , and cleft lip and palate ; anomalies of the central nervous system , including cases of cerebellar hypoplasia , hydrocephalus , and partial agenesis of the corpus callosum ; bronchopulmonary malformation , that mainly consisted of pulmonary sequestrum ; genetic aberrations [ 67 ]  . fetal mri should provide information regarding location ( right , left ) , herniated organs , and in particular bowel , liver ( liver - up and liver - down ) and kidneys ; lung volume measurements of the residual and contralateral lung and the indices of fetal lung maturity [ 31 , 68 , 69 ] ; signal intensity analysis as a possible expression of lung maturity , possible mediastinal shift , polyhydramnios and hydrops fetalis and other associated conditions . 
by evaluating these parameters , high - risk fetuses [ 70 ] ( with liver herniation and / or delayed lung maturity ) can be identified [ 71 ]  . 
low - risk fetuses ( liver down and normal lung parameters ) can be undergone to elective post - natal surgical reduction . abdominal pathologies fetal mri has an important role in particular in fetuses co - affected by both genitourinary and gastrointestinal malformations , such as cloacal malformations , abdominal wall defects and cloacal exstrophy . 
indications to fetal mri in case of abdominal disorders , include renal or bowel abnormalities , retroperitoneal masses or the presence of severe oligohydramnios , which impairs us evaluation of the fetus . 
 in addition , fetal mri may add diagnostic information in anhydramnios or oligohydramnios , because in these cases us examination is technically difficult ; it may provide adjunctive information about lung development [ 76 , 77 ]  . renal anomalies : renal hypoplasia : it represents the failure of the kidney to develop to normal size , usually associated to hypertrophied contralateral kidney ; renal agenesis ( fig.7 ) : bilateral agenesis is incompatible with life ; unilateral agenesis is uncommon . 
 diffusion - weighted imaging plays an important role in the suspect of renal agenesis , thanks to its high sensitivity in the detection of renal parenchyma [ 78 , 79 ] ; in fact , dwi is helpful in the diagnosis of ectopic kidneys , small kidneys , bilateral renal agenesis and also to evaluate normal renal development [ 7 ]  . polycystic kidney disease : mri shows enlargement of both kidneys , which appear hyperintense on t2 - w due to the presence of numerous small cysts uniformly distributed in the parenchyma [ 80 ]  . congenital kidney tumors ( fig.7 ) : the most frequent congenital kidney neoplasm is mesoblastic nephroma ( or fetal renal hamartoma ) , which unless complicated necrosis and hemorrhage , is iso to hypointense on t1 - w and variable on t2 - w images with restriction on dwi . ureteric anomalies : hydronephrosis : it is clearly visualized on t2 - weighted images . 
the most common cause of fetal hydronephrosis is a pyeloureteral junction stenosis ; duplicated ureters ( fig.8 ) : mri can be helpful in the diagnosis of a complete or incomplete duplex system , and eventually of the ectopic drain usually affecting the upper ureter , which may present an associated ureterocele [ 81 ]  . suprarenal masses : this group includes adrenal , genitourinary or non - genitourinary masses ( gastrointestinal or spleen ) [ 82 , 83 ]  . 1 3 la radiologia medica ( 2018 ) 123 : 271285 fig . 
sagittal haste t2 - w image ( a ) shows the presence of an anterior abdominal wall defect ( white arrow ) with herniation in the amniotic cavity of abdominal content , covered by peritoneum ( a , b ; black arrowhead ) ; same findings on axial true - fisp image ( b ) , showing the presence of bowel loops ( b ; black arrow ) inside the covering membrane of the omphalocele . 
the loops are hyperintense on t1 - w image ( c ; white arrowhead ) due to the presence of meconiu anterior abdominal wall defect ( a ; black arrowhead )  . 
 the bowel loops ( white arrowhead ) are hyperintense on t1 - w ( f ) , due to the presence of meconium neuroblastoma : it is the most common malignant newborn tumor . 
it usually appears as a complex cystic mass , but it can also have a solid component with low signal on t1 - w images and moderately increased signal on t2 - w images . 
it has a better prognosis compared to the pediatric type [ 80 ]  . abdominal extralobar sequestration : it should be considered in the differential diagnosis of suprarenal masses ; mri helps to distinguish the normal adrenal gland separated from the mass , which usually has a higher signal intensity compared to the lung , similar to the signal intensity of the stomach . 
the feeding vessel is not often seen on mri ; on the contrary , color doppler us may identify it [ 84 ]  . gastric duplication cysts and spleen cysts : often localized on the greater curvature . 
they are unilocular cysts with hyperintense content on t2 - w sequences and low signal on t1 - w sequences ; if they have hemorrhagic content , they can also be hyperintense on t1 - w images [ 80 , 85 ]  . prune belly syndrome : mri findings in this rare malformation are severe bilateral hydronephrosis , urethral dilatation and absent genitalia ; anhydramnios may be present [ 86 ]  . gastrointestinal malformations proximal gi malformations : there is no evidence in the guidelines about the role of magnetic resonance in the study of these pathologies ; in fact , isolated cases of atresia and stenosis of the upper gi do not represent an indication to mri . 
the most frequent are [ 87 ] : esophageal atresia : due to an abnormal development of the tracheoesophageal septuit is suspected when a dilated esophageal pouch , hyperintense on t2 - w images , is seen in the thorax , and if it is associated to a persistent small or absent stomach ; however , esophageal atre1 3 280 la radiologia medica ( 2018 ) 123 : 271285 of duodenal atresia , fetal mri show both dilated fluidfilled stomach and proximal duodenum with a typical double bubble sign on t2 - w images ; it is often associated to polyhydramnios [ 89 ]  . malposition or abnormal size of the stomach : persistent small stomach with normal amniotic fluid should raise the suspect of congenital microgastria , often associated to a dilated esophagus . 
in this last case , large bowel has a reduced caliperwith absent or low meconium content . intestinal cystic disease : less frequently affecting the distal bowel . large bowel disorders : distal large bowel obstruction : on t1 - w images it can be visualized as a dilated tubular structure with hyperintense content ; proximal tubular bowel loops are usually dilated and have a hyperintense signal on t2 - w images . 
a different situation is represented by megacystis microcolon intestinal hypoperistalsis syndrome ( mmihs ) , which is a rare cause of gastrointestinal and genitourinary obstructions ; in this condition the distal colon presents a reduced caliber . meconium peritonitis : it is as a complication of intestinal atresia ; meconium pseudocyst is a common complication in these cases . 
it is a complication of intestinal atresia and may evolve in meconium pseudocyst that usually presents internal septa with a hyperintense signal on t2 - w images and an hypointense signal on t1 - wi [ 80 ]  . complex malformations cloacal malformation : a rare and complex disorder resulting in the lack of compartmentalization of the urinary , genital and intestinal tract . 
in fact , this group of malformations range from an ectopic anteriorly positioned anus to the complete persistent cloaca , which only affects female fetuses and occurs when the vagina , urinary tract and the rectum are fused fig . 
7 two different fetuses with kidney and bladder agenesis ( ab ; 19 weeks of gestation ) and congenital mesoblastic nephroma ( cf ; 27 weeks of gestation )  . 
t2 - weighted haste images on coronal ( a ) and sagittal ( b ) planes showing a fetus with mri findings of anhydramnios ( white arrowheads ) , the absence of both kidneys ( white arrows ) and bladder ( black arrowhead )  . 
axial t2 - weighted ( c ) and t1 - weighted ( d ) images of a fetus with mesoblastic nephroma ( white arrowhead ) of the right kidney which appears as a solid mass with some cystic components ( white arrow )  . 
the mass is hyperintense on dwi ( e ) and hypointense on adc map ( f ) sia may be suspected also in case of polyhydramnios , a small stomach and absent visualization of esophageal lumen on t2 - w images [ 88 ]  . 
when an esophageal atresia is suspected , it is necessary to search for other gi , renal and vertebral malformations . duodenal atresia : it may have intrinsic or extrinsic ( often due to the presence of a choledochal cyst ) origin case 1 3 la radiologia medica ( 2018 ) 123 : 271285 fig . 
fetus at 29weeks of gestation with duplex collecting system of the left kidney on coronal t2 - w image ( d ) , which shows a dilated upper pelvis ( black asterisk ) , and a not dilated compressed inferior pelvis ( black arrowhead )  . 
true - fisp images show that the outlet of the superior dilated ureter ( f , white arrow ) is more distal and abnormal ( probably in vagina ) compared to the outlet of the inferior ureter ( g , black arrow ) , which is in the bladder fig . 
we also calculated the concordance between fna and core biopsy by lesion appearance , lesion ct attenuation , lesion histology , lesion location and fna needle gauge size . results core biopsy alone provided the diagnosis in 207 / 215 cases ( 96.3% ) , however , the fna provided the diagnosis in the remaining 8 / 215 cases ( 3.7% ) where the core biopsy was non - diagnostic . 
there were 154 ( 71.6% ) lytic lesions , 21 ( 9.8% ) blastic lesions , 25 ( 11.6% ) mixed lytic and blastic lesions and 15 ( 7.0% ) lesions that were neither lytic nor blastic . 
the concordance between fna and core biopsy is higher for lytic lesions than for blastic lesions ; and higher for low - attenuation lesions than for high - attenuation lesions . keywords osseous lesions lytic blastic metastases fine - needle aspiration fna bone lesions ct attenuation introduction fine - needle aspiration ( fna ) is often used for the diagnosis of soft tissue lesions from several sites , including the thyroid , lung , breast and pancreas [ 14 ]  . 
for these sites , fna * ronnie sebro ronnie.sebro@uphs.upenn.edu 1 department ofradiology , university ofpennsylvania , 3400 spruce street , philadelphia , pa19104 , usa 2 department ofpathology , university ofpennsylvania , 3400 spruce street , philadelphia , pa19104 , usa 3 department oforthopedic surgery , university ofpennsylvania , 3400 civic center blvd , perelman center south tower , room 10 - 179 , philadelphia , pa19104 , usa has high sensitivity and specificity [ 14 ]  . 
fna for evaluation of osseous lesions has been debated because of reported lower sensitivity and higher non - diagnostic rate compared to those of concurrent core biopsies [ 57 ]  . 
there are also numerous problems that may occur when using solely fna for evaluation of osseous lesions including : difficulty obtaining fna specimens with adequate cellularity [ 7 , 8 ] , and difficulty in making a definitive diagnosis due to similarities between the cytomorphological features of different lesions in bone [ 7 , 8 ]  . 
special immunohistochemical stains may help diagnosis from fna ; however , these require special processing [ 8 ]  . osseous lesions may be lytic , blastic , mixed lytic or blastic or neither . 
core biopsy is more accurate than fna for evaluation of osseous lesions [ 8 ] , however , core biopsy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 254259 accuracy has been shown to decrease with increase in computed tomography ( ct ) attenuation of a lesion ( more blastic lesions ) [ 9 , 10 ]  . 
it is unknown if the accuracy of fna is affected by whether the lesion is lytic , blastic or mixed lytic and blastic ; or whether the accuracy of fna is affected by lesion ct attenuation . we hypothesized that fna in conjunction with core biopsies of osseous lesions is more likely to be diagnostic than core biopsies only . 
we also hypothesized that the concordance between fna and core biopsy would be higher for low - attenuation lesions ( 100 hu ) than for high - attenuation lesions ( > 100 hu )  . 
therefore , the aims of this study are to compare the diagnostic rate of fna performed in conjunction with core biopsy compared to core biopsy alone ; and to assess the concordance between fna and core biopsy for lytic , mixed lytic and blastic , and blastic osseous lesions . 
we also assessed whether the concordance between fna and core biopsy varied based on a number of other factors , including the lesion histology , lesion location and fna needle gauge size . with expertise in bone lesions independently of the fna diagnosis . radiographic evaluation musculoskeletal radiologists determined whether the osseous lesions were lytic , blastic , mixed lytic and blastic , or neither lytic nor blastic on unenhanced computed tomography ( ct ) studies or radiographs . 
there were a few ( n = 15 ) lesions that were neither lytic nor blastic lesions and were fractures or lesions that looked neither lytic nor blastic on ct . 
the ct attenuation of a lesion was obtained from ct studies of the untreated lesions performed within 2weeks of biopsy in patients who underwent ultrasound - guidedor fluoroscopy - guided biopsy . materials andmethods statistical analysis this retrospective study was approved by the local institutional review board ( irb ) , and is compliant with the health insurance portability and accountability act of 1996 ( hipaa )  . 
 we retrospectively reviewed patients who underwent simultaneous fna and core biopsies of osseous lesions at our institution over a 6 - year period ( january 1st , 2011 through december 31st , 2016 )  . 
soft tissue lesions that extended into the bone , i.e. , lesions not originating from the bone were excluded . cytologic andhistopathologic evaluation fnas were performed using 2025g westcott or chiba needles and 15 passes were made . 
the cytopathologist evaluated these lesions and rendered a diagnosis independent of the core biopsy performed . core biopsies were performed concurrently with the fna and obtained using a bone core biopsy needle ranging in size from 11 to 15g , depending on lesion size and location . 
we also assessed the concordance between fna and core biopsy for low - attenuation lesions ( 100 hu ) and for high attenuation lesions ( > 100 hu )  . 
finally , we assessed the concordance between fna and core biopsy based on a number of other factors , including the lesion histology ( whether the lesion was metastatic versus non - metastatic in nature ) , lesion location and fna needle gauge size . 
we found 68 / 215 ( 22.3% ) patients had benign osseous lesions / findings ( aneurysmal bone cysts , giant cell tumors , chondroblastomas , inflammation / infection , fibrosis or normal findings ) ; 29 / 215 ( 13.5% ) patients had primary malignant osseous lesions ( lymphomas , plasma cell neoplasms , pecomas , chondrosarcomas , leiomyosarcomas , osteosarcomas ) ; and 118 / 215 ( 54.9% ) patients had osseous metastatic lesions ( carcinomas from primary sites such as breast , kidney , lung , and prostate ; melanomas and 1 3 la radiologia medica ( 2018 ) 123 : 254259 table 2 concordance between fna and core biopsy by lesion imaging appearance table 3 concordance between fna and core biopsy by lesion histolcomparison concordance ( % ) comparison concordance ( % ) lytic lesions blastic lesions mixed lytic and blastic lesions attenuation attenuation100 hu ( low attenuation ) attenuation > 100 hu ( high attenuation ) 180 / 215 ( 83.7 ) 136 / 154 ( 88.3 ) 13 / 21 ( 61.9 ) 18 / 25 ( 72.0 ) 110 / 126 ( 87.3 ) 58 / 77 ( 75.3 ) benign osseous lesions malignant primary osseous lesions of the bone metastases 54 / 67 ( 80.6 ) 24 / 29 ( 82.8 ) 102 / 119 ( 85.7 ) table 4 concordance between fna and core biopsy by lesion location lymphomas )  . 
as expected , there was a slight increase in the proportion of men with blastic osseous lesions , likely due to prostate cancer . there were 180 / 215 ( 83.7% ) cases where the diagnosis from the fna was concordant with the core biopsy diagnosis ( table2 )  . 
we identified eight cases ( 3.72% ) where fna yielded the diagnosis and the core biopsy did not / was non - diagnostic . the concordance between fna and core biopsy in diagnosing osseous lesions by imaging appearance ( lytic , blastic , mixed lytic and blastic or neither lytic nor blastic ) was evaluated . 
this concordance was 136 / 154 ( 88.3% ) for lytic osseous lesions ; 13 / 21 ( 61.9% ) for blastic osseous lesions ; 18 / 25 ( 72.0% ) for mixed lytic and blastic lesions ; and 13 / 15 ( 86.7% ) for neither lytic nor blastic lesions . 
there were 12 subjects who underwent ultrasound / fluoroscopyguided biopsies and had no unenhanced ct studies of the untreated lesions within 2weeks of biopsy , so the attenuation of the biopsied lesions could not be measured . 
there was no significant difference in the concordance between fna and core biopsy by lesion location ( p > 0.05 for all comparisons )  . the concordance between fna and core biopsy was analyzed by fna needle gauge size ( table5 )  . 
there was no difference between the concordance between fna and core biopsy by fna needle gauge size ( p > 0.05 for all comparisons )  . discussion we showed that fna in conjunction with core biopsy is more likely to be diagnostic than core biopsy alone . 
the concordance between fna and core biopsy was higher for the evaluation of lytic osseous lesions compared to blastic lesions ; and higher for low - attenuation ( 100 hu ) lesions 1 3 258 la radiologia medica ( 2018 ) 123 : 254259 than high attenuation ( hu > 100 ) lesions . 
we also think it is reasonable to attempt fna for blastic lesions , however , we note a lower concordance rate with core biopsy , and therefore , a likely lower diagnostic rate . 
we found no statistically significant association between gauge size and the concordance between fna and core biopsy . previous studies have shown that fna is useful for the diagnosis of lesions at numerous sites [ 14 ]  . 
our data support the fact that core biopsy is generally more diagnostic than fna , but our data also showed that fna was diagnostic and the core biopsy was non - diagnostic in 3.72%. 
the diagnostic accuracy of combining both fna and core biopsy are quite high , and therefore , higher than either technique used in isolation . utilizing fna in addition to core biopsy is useful for a number of reasons . 
the biopsy needle can be repositioned to a different location within the lesion to increase the likelihood of obtaining a diagnostic sample if the fna shows predominantly bloody , acellular or necrotic material . 
fna may show the presence of an infectious organism or evidence of acute or chronic inflammation , and in that case , this should direct the musculoskeletal radiologist to obtain gram stains and microbiology cultures . 
the musculoskeletal radiologist should obtain flow cytometry and molecular testing and the core biopsy samples should be placed in sterile saline rather than formalin if the fna shows the presence of a lymphoproliferative process . 
we also could not determine the true accuracy , sensitivity and specificity of fna relative to core biopsies because not all cases underwent open biopsy ( the gold standard )  . in summary , we have demonstrated that fna with concurrent core biopsy has superior diagnostic accuracy compared to core biopsy alone . 
we also demonstrated that the concordance between fna and core biopsy for lytic osseous lesions is higher than that of blastic osseous lesions and is a useful technique for musculoskeletal radiologists . acknowledgements the article is not under consideration for publication elsewhere . 
the shielding of testes and the exclusion of eyes from the scan could allow to further reduce the dose . keywords scoliosis eos system organ doses lifetime attributable risk introduction the radiological investigation of spinal and bone structure deformity is an essential tool for the identification of pathological changes and to guide the surgeon in choosing the best and least invasive treatments . 
the commonly used imaging modalities for monitoring these pathologies are digital radiography ( dr ) and computed radiography ( cr ) thanks to the high bone structures contrast that permits to acquire images with low - dose patient techniques . 
the use of ct permits to obtain detailed information about malformations of the spine , but the patient , which should normally be subjected to * marco branchini branchini.marco@gmail.com 1 department ofmedical physics , san raffaele scientific institute , via olgettina 60 , 20132milan , italy 2 chief department ofradiology , irccs istituto ortopedico galeazzi , via riccardo galeazzi 4 , 20161milan , italy frequent examinations , is exposed to higher doses of radiation [ 1 , 2 ] and , moreover , the spine cannot be imaged in load because of the patientposition being supine or prone . 
 new low - dose ct protocol , however , has been developed to reduce patient exposition to dose level comparable with radiography [ 3 ]  . in recent years , the eos imaging system ( eos imaging , paris , france ) has been introduced specifically for the imaging of particular musculoskeletal pathologies . 
the eos scanner is a bi - planar x - ray scanning system that allows acquiring images of the lower extremities and column in load , with patient in vertical position or , if it is not possible , sitting down in the machine . 
furthermore , it allows to obtain high - quality images [ 410 ] using very short acquisition times providing also 3d reconstructions of the skeleton , useful in many clinical applications [ 1114 ]  . 
nonetheless , the issue of dose delivered by the vol . : ( 0123456789 ) 1 3 306 la radiologia medica ( 2018 ) 123 : 305313 table 1 investigated organs at risk and the corresponding number of tlds no . 
of tld last generation of radiological machines is still of primary importance especially for young patients who underwent several examinations and dose reduction is a fundamental factor in the assessment of wide scoliosis diagnostic screenings introduction . in this study , in order to assess the diagnostic procedure for scoliosis imaging by using the eos system in adolescent patients , we focused in its dosimetric performance evaluating organ doses and effective dose . 
the aim of this study is to compare organ dose and effective dose between cr and eos and compute the lifetime attributable risk ( lar ) of cancer incidence and cancer mortality due to a full spine examination in an adolescent standard patient . position colon bone marrow ( iliac crest ) lungs stomach small intestine oesophagus liver thyroid testicles eyes abdomen skin dose pelvis skin dose materials andmethods the eos imaging systems the eos low - dose 2d / 3d is an xray system used for imaging of the spine . 
 sixty tlds , type gr200a ( lif : mg , cu , p ) , were placed internally and externally to the phantom , in correspondence with the most important organs at risk , as reported in table1 . 
in particular , we locally positioned at least three tlds for each internal organ at risk ( oar ) and a tld card , consisting of three tlds with different shieldings , for the external oar . 
tld dosimeters were calibrated in dose to tissue : a total number of 18 tlds were exposed to different values of tube current and kvp ( 90 and 109kv )  . 
the uncertainty in the leastsquares calibration coefficient was computed and combined together with the standard unfors and tld uncertainties calculated following gum procedures [ 20 ] ( 3% for both dosimeters , as derived from unfors specifications and tld reproducibility measurements ) and with the estimated standard uncertainty in dosimeters positioning during calibration ( 1% ) for an overall relative standard uncertainty equal to 5% . the experimental measurements the phantom underwent a radiological examination in the same position of patients ( fig.1 ) and using the total rachis protocol as in clinical setting at the irccs orthopaedic institute riccardo galeazzi ( milan , italy ) for an adolescent patient with weight of about 60kg ( manufacturers exposure parameters for medium morphotype )  . 
in table2 , we reported the parameters setting and the corresponding dose area product ( dap ) value for the protocol used for the measurements and for the protocol with a speed 4 , as an example , for which we observe a dap reduction of about 40% . 
expositions consisted in an antero - posterior ( ap ) and a lateral ( lat ) projection with the left side of the phantom nearer to the tube , as for the eos . 
 also in this case , we selected routine settings used for a standard adolescent patient ( ap projection : ssd = 179cm , 90kv , 80mas ; lat projection : ssd = 172cm , 95kv , 100mas ) with weight of around 60kg . 
the following approximations were adopted for estimating the dose to the remainder organs specified in icrp 103 : heart dose same as oesophagus dose , right kidney dose same as liver dose , dose to left kidney , pancreas , spleen and gall bladder same as dose to stomach . 
the external dosimeters are clearly visible 1 3 308 la radiologia medica ( 2018 ) 123 : 305313 the inferred dose and consequently added to the calibration standard uncertainty ( see tld calibration )  . 
in particular , mean breast dose ( both male and female ) was approximated to the average value between dose to stomach and dose to liver consistently to the data reported in the study of damet etal . 
 [ 15 ] which found breast dose equal to about 100 and 85% of the average dose to liver and stomach in the examinations performed with eos and cr systems , respectively . 
the last value was taken as equal to the average value of stomach and liver doses . results organ doses andeffective dose the images from ap and lat projections obtained with the eos and with cr systems are shown in fig.2. 
 the lower values obtained with the computed radiography for testes and eyes are due to the fact that they were outside the fields during our experimental measure mimicking the routine examinations . 
used eos scanning speed 3 , instead of our choice of scanning speed 7 , but higher ma values compared to our protocol , thus resulting in similar dap for the ap view and around 10% lower for lat view . 
thus , we could argue that the effective dose value that we found could be reduced to about 0.26msv at scanning speed 4 , a result similar to that of lou etal . 
the lower values found by gialuosis can be explained by the low mas values ranging between 18 and 30 used in their hospital ( 11 and 18mas for ap and lat )  . 
 [ 27 ] , authors achieved a consistent decrease in dose level to 0.08msv with pa / lat projections using cr system and the air - gap technique instead of the anti - scatter grid for 13to 17 - year - old patients . 
for example , using a wedge - shaped filter can greatly decrease patient exposure , but it is more difficult and less reproducible than eos as reported by radiology technicians [ 16 ]  . 
other techniques to decrease radiation exposure are employment of copper filtration in ap projections [ 29 ] , posterioranterior ( pa ) projection in place of ap [ 15 , 16 ] and air - gap substituting anti - scatter grid [ 27 ]  . 
at the moment , we are optimizing the scoliosis procedure performed with cr to further decrease dose values still considering image quality . it is evident that , both in eos and in cr , the dose difference between left / right and front / back organs is a consequence of the ap and lat ( field from left to right ) directions of irradiation . 
 some authors [ 30 , 31 ] argued that lar should be more defensible than effective dose for measuring the risk because the latter is defined independently of age and sex but should be representative of all the following effects : carcinogenesis , hereditary effects , life shortening and loss of quality of life . 
 in any case , we must emphasize that both effective dose and lar are referred to an abstract standard individual ( a particular age and sex group in the case of lar ) and should not be exactly attributed to a real person . scoliosis patients who require surgery are imaged regularly , and the number of radiographies examinations could be consistent : hansen et al . 
 [ 27 ] registered an average value of seven examinations and the society on scoliosis orthopaedic and rehabilitation treatment stated that x - ray examination should be repeated every 612months [ 32 ]  . 
 considering a mean number of seven examinations would result in a lar ( beirvii ) of induction for all cancers in a 15 - year - old male patient of 0.5 / 1000 and 0.8 / 1000 with eos and cr / grid ( approximately 0.8 / 1000 and 1.3 / 1000 for a 15 - year - old female )  . 
moreover , considering the large variability of dose values reported in bibliography , an international standardization of procedures would be beneficial to minimize the risk in scoliosis patients . this study has several limitations . 
experimental measurements were taken from a normal adult male rando alderson phantoeven if an adult female alderson rando ( 160cm , 55kg ) would have been more suitable to approximate weight and dimensions of an adolescent patient , our measurement can be considered a reasonable approximation of organ doses to a late adolescent male especially considering that the parameters were tuned for a 60kg patient : the mean weight for 16and 18 - year - old male are about 61 and 67 kg as derived from thewho data [ 33 ] of bmiand height - forage . 
as a first approximation , the same experimental data were employed to estimate the dose and lar for a female patient ( average weight for 16and 18 - year - old girl equal to around 55 and 57 kg [ 33 ] ) to investigate ionizing radiation risk as a function of sex . 
these limitations could be acceptable when considering that same measurement setting was employed for both eos and cr scanners and one of the aims of this 1 3 312 la radiologia medica ( 2018 ) 123 : 305313 study was to assess the relative patient exposure between two modalities . 
moreover , considering the european directive 2013 / 59 euratom [ 34 ] that has highlighted the relevance of the medical exposures justification process , the results here included may facilitate referrers and practitioners in risk / benefit evaluations , especially for repeated examinations of younger patients . conclusions one of the aims of this paper was to assess organ doses for a scoliosis examination with the eos imaging system and comparing them to doses received in the same examination performed with a computed radiography systethis kind of investigation allows to gain useful information for patient dose and protocols optimization . 
as expected , the comparison with other studies in literature revealed that eos system has a narrow exposition range than cr and conventional radiography , mainly because of its standardized examination settings . 
 although cancer induction probability is limited for both eos and cr systems , it is highly recommended to optimize exposition dose especially for young patients considering the large number of diagnostic examinations during follow - up . 
 another important finding of the study was the higher dose values for the eos examinations in the eyes and testicles because of eyes inclusion in the field and lack of testicle shielding as standard practice . 
therefore , an improvement in the eos examination procedure is warranted . acknowledgements the authors would like to thank simonetta brambilla , matteo giagnorio , gianpaolo pallazzi and michele ieraci for the kind and competent collaboration in the experimental measurements . 
this article is an open access publication abstract objectives to apply the delphi exercise with iterative involvement of radiologists and pulmonologists with the aim of defining a structured reporting template for high - resolution computed tomography ( hrct ) of patients with fibrosing lung disease ( fld )  . methods the writing committee selected the hrct criteriathe delphi itemsfor rating from both radiology panelists ( rp ) and pulmonology panelists ( pp )  . 
the remaining 17 / 27 ( 63.3% ) items were rated by the pp in round 3 , with 2 / 17 items ( 11.7% ) rated essential by the pp . 
orsola - malpighi , university ofbologna , bologna , italy 8 department ofradiology , azienda unit sanitaria locale di bologna , bologna , italy 9 department ofradiology , gb morgagni hospital , forl , italy 10 department ofradiological sciences , institute ofradiology , universit cattolica del sacro cuore , rome , italy vol . : ( 0123456789 ) 1 3 246 introduction the radiology report is an essential part of the service that radiologists provide to both patients and referring physicians , in any field of medicine . 
the radiology reports structure and content may vary according to several factors , including the clinical inquiry , and the radiologists expertise and education . free text reporting is still the most common format in clinical radiology . 
however , free text clinical reports may heterogeneously render the core information ( e.g. , language and cultural variability ) , making it difficult to compare reports or find specific details [ 2 , 3 ]  . 
this is particularly true for diffuse lung disease ( dld ) , which is often a challenging diagnosis and prone to variable description by high - resolution computed tomography ( hrct )  . 
for instance , reporting enlarged lymphnodes might result misleading in patients with fibrosing lung disease ( fld ) because these abnormalities frequently coexist without specific clinical implication . a number of initiatives are being promoted by the major international societies of radiology to disseminate the use of structured reporting [ 4 ]  . 
 however , it seems that most radiologists are encouraging and appreciating the use of structured reporting , especially in among subspecialist radiologists [ 8 ]  . to our knowledge , there is no proposed structured reporting template for hrct scans of subjects with dld to guide radiologists in the systematic reporting in the framework of findings andsynthesize a final clinical hypothesis . 
following debates between expert pulmonologists and chest radiologists at the italian national meetingsnational meetings , respectively , from the italian societies of respiratory medicine and the italian society of medical radiology ( sirm ) , we hypothesized that a structured report might be particularly helpful for hrct of patients with fld . within the reference standard of multidisciplinary discussion , the radiology report remains the primary method of communication between radiologists and clinicians , particularly in non - referral centers . 
in la radiologia medica ( 2018 ) 123 : 245253 fact , reducing the chance of omitting important findings ( e.g. , traction bronchiectasis or pulmonary emphysema ) , or supplying an interpretation of the radiological pattern , would be paramount to guide the referring physician in critical clinical decisions for patients with fld . this study was undertaken to enact critical shared discussion between chest radiologists and pulmonologists by means of multi - round consensus - building delphi exercise , to develop a comprehensive focused structured reporting template for hrct of patients with fld . 
the study objectives were to develop a list of hrct criteria to describe fld , to learn the most relevant parameters according to the point of view of pulmonologist , and to assess the agreement among experts on the proposed criteria . materials andmethods a six members writing committee proposed the hrct criteria and parametersthe delphi items to the panelists rating . 
the writing committee members had at least 10years of experience and authored at least 10 studies in imaging of dld and they did not participate in the following delphi survey . 
the list of delphi items was based on the evidence from the literature in fld and the experience of each writing committee member . selection ofthedelphi domains anditems a literature search was performed in medline to identify publications relevant to the hrct features of flds from 2002 idiopathic interstitial pneumonia classification document to january 2016 [ 10 ]  . 
the full text of the selected studies was reviewed by two out of six members of the writing committee , who developed and shared the initial list of delphi items with the other writing committee members via emails and teleconferences . the structured report was divided into three domains according to the american college of radiology handbook for residents : ( a ) initial considerations , ( b ) hrct findings , ( c ) conclusions [ 11 ]  . 
furthermore , hierarchy of hrct findings description was investigated with particular emphasis on the key components of the fld , namely honeycombing , traction bronchiectasis , and signs of volume loss [ 9 ]  . 
it was also investigated the relevance of disclosure of the confidence in diagnosing and differentiating honeycombing and traction bronchiectasis , which is a critical task even among expert chest radiologists [ 12 ]  . quantitative information was also among the items of hrct findings , namely the relevance of reporting the extent of fibrosis and emphysema in the structured report . 
 1 3 248 la radiologia medica ( 2018 ) 123 : 245253 furthermore , the format of preferred visual scoring was proposed as either continuous variable ( e.g. , percentage ) or as category ( e.g. , mild , moderate , or severe )  . 
of note , no cut - off values were a priori set to define the categories of disease extent ( e.g. , the category should be assigned according to radiologist subjective impression )  . 
in addition , it was investigated whether extent should be provided for any fld or only for individual disorders ( e.g. , sarcoidosis , systemic sclerosis ) for which literature supported the prognostic value of such data at the time of the present study [ 13 , 14 ]  . 
scientific references were supplied to the panelists for informed review of the aforementioned items . the domain conclusions was meant to investigate the relevance of reporting the hrct pattern ( e.g. , usual interstitial pneumonia , uip ; non - specific interstitial pneumonia , nsip , etc . ) , of proposing further diagnostic evaluation , and of indicating the timing for hrct follow - up . selection ofthestudy panelists the italian chest imaging subspecialty society indicated a list of 53 expert radiologists ( 38 males , age range 3072years , median age 43years , median years of experience in dld 11years ) , all active members of the section of thoracic imaging of the sirm , to participate in the delphi survey ( i.e. , the radiology panelistsrps )  . 
selection criteria for rps were as follows : ( a ) 5years of experience in imaging of dld ( as reported in the society database ) ; ( b ) authorship of3 articles on dld in peer - reviewed journal . 
likewise , 18 pulmonologists ( 13 males , age range 38 - 61years , median age 53years , median years of experience in dld 15 ) panelist ( pp ) were selected according to the following selection criteria : ( a ) 10years of experience in dld ; ( b ) authorship of10 articles on dld in peer - reviewed journal . 
the selected rps and pps were contacted by email , informed about the aims and methodology of the study . overview ofthedelphi exercise the delphi exercise was run by a biostatistician ( with 5 years of experience ) , through emails exchange . first , rps were asked to classify delphi items into three categories , as follows : ( a ) essential ; ( b ) optional ; or ( c ) not relevant for the hrct structured reporting . 
items rated essential were further classified according to the format of reporting into free text or outlined ( i.e. , by a fixed check - list of descriptors or categories )  . 
furthermore , all panelists were allowed to suggest additional items to be included in the item list for the subsequent round ; this fostered the open discussion that this inter - specialty consultation was meant for . in addition , pps were also asked to judge the delphi items that had been rated essential by the rps , as follows : agree or disagree . 
likewise , this cut - off value was also used to select the most appropriate format of reporting of each retained item ( e.g. , to be given as free text or to be outlined )  . results four delphi rounds were performed to obtain the final structured report . 
a total of 12 / 18 ( 66.7% ) pulmonologists agreed to participate as pps and completed one delphi round ( i.e. , the third round )  . the result of each round is given in supplementary tables14 and summarized in fig.1. 
in particular , total or nearly total agreement was reached for the following items : presence of prior hrct scans for comparison , initial description of the variation of hrct findings as compared to prior scans , and assessment of the disease distribution . 
a number of panelists expressed no preference for the format of reporting as outlined in supplementary tables . in round 2 , 17 / 27 ( 63% ) items were re - rated by the rps . 
a 80% consensus was not reached for any of thea consensus greater than 80% was recorded upon the outline format for four out of 10 ( 40% ) items that had been judged essential in round 1 . 
ten out of 42 ( 24% ) rps suggested to add an item for ancillary findings ( e.g. , pleural plaques , dilated esophagus , etc . ) , and report it as free text . in round 3 , pps rated essential the extent of the visual scoring of both fld ( expressed as percentage lung volume involvement ) and emphysema ( expressed as categories )  . 
furthermore , three ( 25% ) pps suggested to expand on the conclusions domain by including a more detailed list of hrct patterns and potential association or cause ( e.g. , unknown connective tissue disease , asbestosis , etc . ) of fld predictable from the hrct findings . 
 this was regarded as worth of rating by the radiologists writing committee that agreed upon a list of both hrct patterns and associations of fld . in round 4 , rps chose between including only the hrct patterns list or also suggesting any association or cause of the fld in the structured report . 
the format of each item included in the final template was chosen by the writing committee by taking into account the preferences of the majority of the rps and pps . 
the iterative structure of the delphi exercise showed a substantial agreement on the items progressively proposed for inclusion by each 1 3 250 la radiologia medica ( 2018 ) 123 : 245253 ideally , the radiologic report should address both clinical and radiological needs , with a direct and easy format . 
on the clinical side , there is no official recommendation about the mandatory features of a radiological report , notably about suggesting association between hrct pattern and cause of dld . 
this study was indeed driven by the need for practical interaction to improve the usefulness of the basic communicating system within multidisciplinary management of the patient , namely the radiologic report . 
therefore , pulmonologists were involved in this study to integrate their needs in a shared structured report , and to rate the relevance of items selected by radiologists . interestingly , pulmonologists agreed on the choice of radiologists and suggested to include information on the extent of both fld and emphysema , which were not rated essential by a sufficient proportion of radiologists . 
furthermore , pulmonologists proposed an additional item for the conclusions , namely the suggestion of possible cause or association of the fld , which might be particularly useful to define the clinical choice for subsequent diagnostic work - up or management . 
for example , the compulsory radiological suggestion of a potential cause of fld ( e.g. , asbestosis , connective tissue disease , etc . ) rather than the sole hrct pattern ( e.g. , uip or nsip ) , might encourage both radiologists to systematically look for important ancillary findings ( e.g. , pleural plaques , dilated esophagus , etc . ) and pulmonologists to seek clinical investigation for the proposed association [ 23 ]  . the delphi exercise is one of the strengths of the present study . 
noteworthy , the anonymity of panelists reduces the potential influence of strong opinion leaders on other participants and , thereby , the results of the survey [ 24 ]  . 
the specific design of our delphi survey was meant to first gather the opinion of radiologists , and then to investigate agreement of pulmonologists , especially on topics that are essential to the majority of expert radiologists . 
 the unanimous agreement of pulmonologists on items retained by radiologists suggests that all those items were clinically necessary , but allegedly they were not sufficient . there are multiple formats for structured report , with no one being absolutely preferable over the other . 
the proposed template for structured report of fld comes as the first multidisciplinary example in the field . the glossary of terms for thoracic imaging as well as the classification documents have both improved the interpretation of the fld [ 1820 ]  . 
therefore , as for other specific topics , a structured report may well fit the fld [ 21 ]  . 1 3 la radiologia medica ( 2018 ) 123 : 245253 asked to choose their preferred format for each itethere was poor consensus ( threshold for consensus80% ) on the format for structured report . 
both radiologists and pulmonologists did not consider essential the reporting style of hrct findings , particularly the avoidance of over - description and the disclosure of confidence on interpretation of key hrct findings ( e.g. , honeycombing vs reticular abnormalities superimposed to emphysema )  . 
therefore , the format of each item included in the final template was chosen by the writing committee by taking into account the preferences of the majority of the rps and pps . 
we think that a combination of free text and outlined items may be helpful to either systematically disclose key unequivocal hrct features ( e.g. , honeycombing ) or describe the meaning of individual abnormalities that otherwise would be difficult to capture using a fixed check - list . further items included in the final structured report template are worth of discussion . 
notably , the structured description of hrct signs of fld allows the list of potential diagnoses of dld to be narrowed from over a hundred disorders to a handful of diseases [ 9 ]  . radiologists did not reach a consensus on the format of preferred visual scoring for emphysema extent . 
this was probably due to the current lack of clarity about the best method to be applied for that purpose , indeed the visual score is affected by quite an inter - observer variation . 
furthermore , the utility of semi - automatic software for emphysema quantitation in routine activity has yet to be clarified , especially for emphysema in fld [ 26 ]  . 
 this method is not suitable for quantification of patients with emphysema and fld because it cannot discriminate between low density areas due to emphysema or associated with honeycomb cysts or traction bronchiectasis [ 27 ]  . 
in our survey , the radiologists did not reach a consensus on that [ 13 , 14 ] , whilst the pulmonologists preferred to include specific description of disease extent for any fld as well as emphysema . 
this request from the pulmonologists is likely related to the need to get additional instruments to improve their interpretation of the patient clinico - functional profile . the inclusion of air trapping in fld seemed also concerning for structure report . 
furthermore , air trapping may be independent from specific association with fld ( e.g. , it has been reported in up to 32% of ipf cases ) [ 28 ]  . 
in a recent study , diffuse air trapping was the source of ct - pathologic discordance in 71.8% in ipf [ 29 ]  . in the conclusions domain , neither radiologists nor pulmonologists agreed upon suggesting specific diagnostic work - up because it was likely perceived as potentially misleading , allegedly beyond the radiologists knowledge ( e.g. , radiologists have often limited information about the patient clinical condition and indeed cannot figure out what would be best for him )  . this study has some limitations . 
this issue will be discussed by forthcoming studies . in conclusion , this study provides a template for structured report of fld that features essential items as agreed by thoracic radiologists and their main speaker , the pulmonologists . 
the multidisciplinary methodology strengthens the structured report utility for daily practice . acknowledgements carlo agostini 1 , carlo albera2 , domenico attin3 , giuseppe battista4 , elena bertelli5 , giuseppina bertorelli6 , claudio bn7 , martina bonifazi8 , lorenzo bonomo9 , andrea borghesi 10 , lucio calandriello9 , antonella caminati11 , diana capannelli3 , stefania cerri12 , federica ciccarese3 , davide colombi13 , marco confalonieri14 , annaemilia del ciello9 , giovanni della casa15 , roberto dore16 , fabio falaschi17 , alessandra farchione9 , beatrice feragalli18 , paola franchi9 , giampaolo gavelli19 , sergio harari11 , fabrizio luppi12 , fabio maggi20 , maria antonietta mazzei21 , manuela mereu22 , gianluca milanese23 , stefano palmucci24 , rosa lucia patea22 , alberto pesci25 , marco piolanti26 , venerino poletti27 , gaetano rea28 , luca richeldi29 , paola rogliani30 , chiara romei17 , paola rottoli31 , alessandro sanduzzi - zamparelli32 , alfredo sebastiani33 , gianluigi sergiacomi34 , gian alberto soardi35 , lucia spaggiari36 , paolo spagnolo37 , sara tomassetti27 , rocco trisolini38 , adele valentini16 , carlo vancheri39 , valentina vespro40 , luca volterrani21 1clinical immunology , department of medicine ( dimed ) , padua university , padua , italy ; 2department of clinical and biological 1 3 252 la radiologia medica ( 2018 ) 123 : 245253 sciences , university of turin , turin , italy ; 3radiology unit , cardiothoracic - vascular university hospital s . 
orsola - malpighi , bologna , italy ; 5radiologia , ospedale careggi , firenze , italy ; 6respiratory disease and lung function unit , department of medicine and surgery , university of parma , italy ; 7radiology , poliambulanza foundation hospital , brescia , italy ; 8department of biomedical sciences and public health , universit politecnica delle marche , ancona , italy ; 9institute of radiology , department of radiological sciences , universit cattolica del sacro cuore , rome , italy ; 10department of radiology , university and spedali civili of brescia , italy ; 11u.o. 
di pneumologia e terapia semi - intensiva respiratoria servizio di fisiopatologia respiratoria ed emodinamica polmonare , ospedale san giuseppe multimedica irccs , milan , italy ; 12center for rare lung diseases , university hospital policlinico di modena , italy ; 13department of radiology , guglielmo da saliceto hospital , piacenza , italy ; 14pulmonology department , university hospital of cattinara , trieste , italy ; 15radiology , university hospital policlinico di modena , italy ; 16unit of radiology , irccs policlinico san matteo , pavia , italy ; 17second radiology unit , university hospital of pisa , pisa , italy ; 18department of medical , oral and biotechnological sciences , university g . 
dannunzio , chieti , italy ; 19radiology unit , irccs istituto scientifico romagnolo per lo studio e la cura dei tumori ( irst ) , meldola ( fc ) , italy ; 20azienda sanitaria locale n . 
1 , avezzano , sulmona , laquila , italy ; 21department of medical , surgical and neuro sciences , diagnostic imaging , azienda ospedaliera universitaria senese , university of siena , siena , italy ; 22department of neuroscience and section of integrated imaging and radiological therapies , university of chieti , italy ; 23section of radiology , unit of surgical sciences , department of medicine and surgery ( dimec ) , university of parma , italy ; 24department of medical and surgical sciences and advanced technologies - radiodiagnostic and radiotherapy unit , university hospital policlinico - vittorio emanuele , catania , italy ; 25department of health science , pulmonology unit , university of milan bicocca , san gerardo hospital , monza , italy ; 26radiologia , azienda unit sanitaria locale di bologna , italy ; 27department of diseases of the thorax , azienda usl romagna , gb morgagni hospital , forl , italy ; 28department of diagnostic imaging , monaldi hospital , naples , italy ; 29unit operativa complessa di pneumologia , universit cattolica del sacro cuore , fondazione policlinico a . 
gemelli , rome , italy ; 30university of rome tor vergata , department of systems medicine , rome , italy ; 31department of medical and surgical sciences and neurosciences , respiratory diseases unit , university of siena , italy ; 32respiratory medicine section , department of clinical medicine and surgery , federico ii university of naples , naples , campania , italy ; 33interstiziopatie polmonari dipartimento medico - chirurgico dei percorsi integrati . 
azienda ospedaliera san camillo - forlanini di roma , italy ; 34department of diagnostic and molecular imaging , radiation therapy and interventional radiology , university hospital tor vergata , rome , italy ; 35uoc radiologia , ospedale maggiore di borgo trento , aoui verona , verona , italy ; 36radiologia , arcispedale s . 
maria nuova azienda - ospedaliera di reggio emilia , italy ; 37section of respiratory diseases , department of cardiac , thoracic , and vascular sciences , university of padua , padua , italy ; 38interventional pulmonology unit , policlinico s . 
orsolamalpighi , bologna , italy ; 39department of clinical and experimental medicine , regional centre for interstitial and rare lung diseases , university of catania , catania , italy ; 40dipartimento di diagnostica per immagini , uoc di radiologia , fondazione irccs ca granda , ospedale maggiore policlinico , milan , italy . compliance with ethical standards conflict of interest the authors state that this study was not funded . 
 albera reports grants , personal fees and non - financial support from roche , during the conduct of the study ; personal fees and non - financial support from roche , personal fees and non - financial support from boehringer ingelheim , personal fees and non - financial support from fibrogen , personal fees and non - financial support from gsk , personal fees and non - financial support from sanofi aventis , outside the submitted work . 
harari reports personal fees from roche , grants and personal fees from intermune , grants and personal fees from boehringer ingelheim , outside the submitted work.luppi reports personal fees from boehringer ingelheim , grants and personal fees from roche , during the conduct of the study . 
dwi with short tau inversion recovery ( stir - dwi ) and that with spectral attenuated inversion recovery ( spair - dwi ) were performed using 3.0 - t magnetic resonance imaging , and the obtained snrs and adcs were compared . 
adcs were also compared between the right and left breast phantoms . results for samples 3 and 4 , snrs obtained using stir - dwi were lower than those obtained using spair - dwi . 
for all samples , stir - dwi demonstrated slightly larger percentage differences in adcs between the right and left phantoms than spair - dwi . conclusion snrs and adcs obtained using stir - dwi are influenced by the t1 value ; a shorter t1 value decreases snrs , overestimates adcs , and induces the measurement error in adcs . 
stir - dwi showed a larger difference in adcs between the right and left phantoms than spair - dwi . keywords diffusion - weighted imaging signal - to - noise ratio apparent diffusion coefficient short tau inversion recovery * tsukasa yoshida ts.yoshida@scchr.jp 1 department ofdiagnostic radiology , shizuoka cancer center , 1007 , shimonagakubo , nagaizumi , sunto , shizuoka411 - 8777 , japan 2 department ofradiation science , hirosaki university graduate school ofhealth sciences , 66 - 1 hon - cho , hirosaki036 - 8564 , japan 3 division ofmedical life sciences , department ofradiological life sciences , hirosaki university , 66 - 1 hon - cho , hirosaki036 - 8564 , japan introduction diffusion - weighted imaging ( dwi ) combined with dynamic contrast - enhanced magnetic resonance imaging ( mri ) improves the diagnostic accuracy of breast lesions [ 1 , 2 ]  . 
the previous studies have indicated that dwi is useful for detecting and differentiating malignant breast lesions as well as for evaluating the therapeutic response to neoadjuvant chemotherapy [ 36 ]  . echo - planar imaging ( epi ) is often used for dw image acquisition , because its rapid acquisition provides robustness to the motion artifact . 
however , several artifacts vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 296304 related to an epi sequence degrade image quality and impair the accuracy of adc measurements [ 7 ]  . 
spectral attenuated inversion recovery ( spair ) is preferred for high - field breast mri , because its inversion pulse is robust to b1 inhomogeneity [ 9 ] ; however , it is sensitive to b0 inhomogeneity caused by air around the breast [ 9 ]  . 
therefore , fat suppression using frequency - selective type is still challenging in breast dwi . short tau inversion recovery ( stir ) is an alternative fat suppression technique for regions that suffer from b0 inhomogeneity . 
the present study aimed to compare snrs and adcs obtained using the two different fat suppression techniques in breast dwi of a phantom . materials andmethods breast phantom design we prepared a homemade phantom with commercially available agar and granulated sugar . 
the breast phantom comprised four cylindrical plastic bottles ( diameter : 25mm , height : 55mm ) and a plastic container ( diameter : 120mm , height : 140mm )  . 
1 photograph ( left ) and schema ( right ) of the breast phantofour cylindrical plastic bottles ( 25 - mm diameter and 55 - mm height ) were filled with agar gels containing different concentrations of granulated sugar . 
the t1 and t2 values were 223955 and 682ms for sample 1 , 167133 and 733ms for sample 2 , 131326 and 703ms for sample 3 , and 92116 and 711ms for sample 4 , respectively . 
imaging parameters were as follows : field of view , 330mm ; acquisition matrix , 112112 ; reconstruction matrix , 448448 ; parallel imaging technique , sense ; acceleration factor , 2.0 ; slice thickness , 3.0mm ; slice interval , 0.6mm ; phase - encoding direction , anteriorposterior ; repetition time , 10 , 000ms ; echo time , shortest ( 70ms for stir - dwi and 69ms for spair - dwi ) ; inversion time , 240ms for stir - dwi and shortest for spair - dwi ; band width , 35.7hz / pixel for stir - dwi and 25.8 hz / pixel for spair - dwi ; number of acquisitions , one ; half scan factor , 0.8 ; and acquisition time , 120s . 
 the shim volume covered the entire region of the bilateral breast phantom to improve the main field inhomogeneity , as previously described [ 20 ] , and a multi - transmit technique was used to achieve b1 field homogeneity . 
phantoms were left at room temperature to minimize the variation in adcs based on temperature . image analysis image analysis was performed using imagej version 1.45 ( national institutes of health , bethesda , md , usa )  . 
the subtraction method , which uses two images with identical parameters [ 21 ] , was applied to calculate snr using the following equation : snr = 2 where s is the averaged signal intensity in the two images with identical parameters and is the standard deviation fig . 
the 2020 - pixel rois were placed in the identical position for b = 0 ( left ) , b = 1000 ( center ) , and adc maps ( right ) obtained from the subtracted image . 
the percentage difference in adcs between the right and left breast phantom was calculated using the following equation : dierence = adcright adcleft adcright 100 , where adcright and adcleft represent mean adcs obtained in the right and left breast phantom , respectively . 
moreover , the percentage differences between stir - dwi and spair - dwi for each sample were calculated and compared . statistical analysis the statistical analysis was performed using r software ( version 3.2.3 ; r project for statistical computing , vienna , austria )  . 
a p value of < 0.05 was considered statistically significant . results table1 shows snr obtained using stir - dw and spairdw images at b = 0 and b = 1000 . 
for samples 1 and 2 , snrs obtained using stir - dwi were comparable to those obtained using spair - dwi , whereas for samples 3 and 4 , snrs obtained using stir - dwi were much lower than those obtained using spair - dwi . figure4 shows dw images and adc maps obtained using stir - dwi and spair - dwi . 
4 dw images and apparent diffusion coefficient ( adc ) maps obtained using diffusion - weighted imaging ( dwi ) with short tau inversion recovery ( lower row ) and dwi with spectral attenuated inversion recovery ( upper row )  . 
the bias of adcs were 0.00068103 mm2 / s for sample 1 , 0.024103 mm2 / s for sample 2 , 0.041103 mm2 / s for sample 3 , and 0.13103 mm2 / s for sample 4 . 
5 blandaltman plots of adcs obtained with two fat suppression techniques for sample 1 ( a ) , sample 2 ( b ) , sample 3 ( c ) , and sample 4 ( d )  . 
the vertical scales in all graphs are the same for comparison and 0.34% for sample 1 , sample 2 , sample 3 , and sample 4 , respectively . table 4 shows the percentage differences in adcs obtained using stir - dwi and spair - dwi . 
therefore , variations in snrs and adcs should be assessed using a phantom or standard material to optimize scan parameters and produce reliable protocols for dwi ( table5 )  . snrs obtained using stir - dwi depend on relaxation properties of the sample . 
lower snrs for samples 3 and 4 obtained using stir - dwi are explained by the inversion pulse and t1 value ( 131326ms for sample 3 and 92116ms for sample 4 )  . 
in stir , the inversion pulse is typically a non - frequency - selective pulse that partially saturates the water as well as the fat proton [ 8 ]  . 
a low snr occurs when the t1 value of a measurement object is similar to the inversion delay time , because the la radiologia medica ( 2018 ) 123 : 296304 longitudinal magnetization of the water proton cannot completely recover . 
therefore , the diagnostic performance of stir in breast dwi can be maintained regardless of its low snr if performed at high - field strength , i.e. , at 3 t or above . in the sample with a shorter t1 value , overall adcs obtained using stir - dwi were significantly higher than those obtained using spair - dwi . 
these results are explained by the t1 - weighted effect of the stir technique and are consistent with those obtained in the previous studies [ 10 , 11 ]  . 
our results indicated that stir - dwi might overestimate adcs of lesions containing blood and portentous components . the gadolinium contrast medium also exhibits the t1 - shortening effect and hence has the potential to overestimate adcs in stir - dwi . 
furthermore , such a delay may reduce the perfusion effect caused by gadoliniutherefore , we believe that stir - dwi provides accurate adc measurements , even following contrast administration . in this study , the relaxation properties of sample 2 , which did not include any fat components , were similar to those of the fibroglandular tissue [ 18 , 26 ]  . 
hence , adc measurements of the fibroglandular tissue depend on the fat suppression technique used , because it is difficult to eliminate the effect of the fat component . blandaltman analysis provides important feature of reproducibility between two fat suppression techniques . 
these results indicate that stir - dwi could overestimate adcs and induce the measurement error in adcs of the sample with a shorter t1 value . the cvs of adcs in both fat suppression techniques suggest the good repeatability , as shown in the previous study [ 27 ]  . 
therefore , stir - dwi may provide better cvs of adcs than those provided by spair - dwi owing to the ability to achieve uniform fat suppression in breast dwi . stir - dwi demonstrated larger differences in adcs between the right and left breast phantoms than spairdwi . 
our results suggested that the difference in adcs obtained using stir - dwi is problematic when adcs between the lesion and contralateral sides are compared , as described in a previous report [ 28 ]  . this study has several limitations . 
adcs vary among different mri systems ; therefore , differences in adcs between stir - dwi and spair - dwi found in this study may not be the same when using other vendors . in conclusion , snrs and adcs obtained using stirdwi are influenced by t1 values in samples ; shorter t1 values decrease snrs overestimate adcs and induce the measurement error in adcs . 
the model was elaborated considering the patients treated in two institutions : fondazione policlinico universitario agostino gemelli of rome ( 173 cases , training set ) and university medical centre of maastricht ( 25 cases , validation set )  . 
this study suggests that the fractal analysis can play an important role in radiomics , providing valuable information not only about the gtv structure , but also about its inner subpopulations . keywords radiomics fractals rectal cancer predictive model magnetic resonance imaging introduction the use of biomedical imaging for diagnosis and therapy purposes in oncology has exponentially increased in the last few decades . 
approximately 1142% of these patients show a pathological complete response vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 286295 ( pcr ) after crt ; different studies demonstrated that patients showing pcr usually have a better prognosis in terms of local failure , metastases - free survival and overall survival [ 12 , 13 ]  . 
recent studies have proposed more conservative surgical approaches , such as local excision or wait and see , to reduce morbidities related to tme in patients , in which complete response is observed [ 14 , 15 ]  . elaborating predictive models that are able to identify which patients could result to be clinical complete responders therefore gained great importance for their correct multidisciplinary management . the model developed in this investigation aims to predict the pcr probability analysing pre - treatment t2 - weighted mr images . 
magnetic resonance imaging ( mri ) represents the gold standard in rectal cancer diagnosis , as it provides excellent soft tissue contrast and high spatial resolution [ 16 ]  . because of these characteristics , this imaging modality can describe with high precision the heterogeneity of the tumour , which is considered today as an important biomarker for response prediction . 
recent studies have demonstrated that tumour sensitivity to treatments could be linked to tumoral spatial organisation , which reflects its heterogeneous cellular population [ 17 ]  . fractal analysis is considered a reliable method to quantify the tumour heterogeneity [ 18 ]  . 
fractals are structures that display a repeating pattern at different size scales ; this property is quantified by a parameter named fractal dimension that measures the self - similarity grade of the structure under analysis [ 19 ]  . 
an image processing procedure that combines fractal and segmentation analysis has been proposed to investigate cancer heterogeneity on mr images , similar to the approach described by szigeti etal . , for studying lung tumour heterogeneity on mice ct scans [ 20 ]  . we first identified different tumour subpopulations through an intensity - based segmentation applied on normalised values and then their spatial organisation has been described using fractal dimensions . 
the aim of this study was to implement our fractal - based approach in a radiomic analysis to quantify the rectal cancer heterogeneity in patients affected by larc and to elaborate a predictive model able to esteem the pcr probability of a patient by analysing the pre - treatment mr . materials andmethods patients this study was conducted on the pre - treatment mr images of the patients treated in two hospital centres : fondazione policlinico universitario agostino gemelli ( rome , italy ) and maastro clinic ( grow , mumc , maastricht , the netherlands )  . policlinico gemelli retrospectively collected 173 patients among those treated between may 2008 and december 2014 . 
maastro clinic prospectively collected 25 patients considering the thunder trial ( theragnostic utilities for neoplastic diseases of the rectum , nct 00969657 )  . the enrolled patients had a pathological diagnosis of larc and they were older than 18years , when the disease was diagnosed . 
all the patients signed informed consent for data collection and they were treated with neo - adjuvant chemo - radiotherapy followed by total mesorectal excision 68weeks after the end of crt . the pathological post - operative data included histology , grading and tumour regression grade ( trg ) according to mandard classification [ 21 ]  . 
pathological complete response was defined in case of ypt0n0 or ypn0 / ypnx . image analysis the mr images analysed were obtained following a protocol that considers t2 - weighted fast spin - echo 2d images acquired in a plane orthogonal to the tumour longitudinal axis [ 16 ]  . 
the box - counting method was applied slice by slice to estimate the fractal dimension of the subpopulations identified where min [ i ( x , y ) ] and max [ i ( x , y ) ] are , respectively , the 1st and the 99th percentile of the grey - level histograms representing the gtv , to minimise the influence linked to the spike pixels . fractal analysis similar intensity levels were gathered and considered as new structures , here defined as subpopulations . subpopulations identification different clusters were identified in the gtv slices containing the normalised intensity values . 
the segmentation was automatically performed considering the pixels whose intensities were included between two threshold levels defined as percentages of the gtv maximupixels with the spatial organisation of these subpopulations was quantified , calculating the fractal dimension of the border including the analysed subpopulation . the fractal dimension was calculated using the software developed in r and c environment implementing the boxcounting method . 
the 1 3 la radiologia medica ( 2018 ) 123 : 286295 number of counts as a function of the side square was plotted on a loglog graph and a linear fit is applied . 
the angular coefficient of the linear fit was an estimation of the fractal dimension [ 25 ]  . this software was validated comparing its results with those obtained using the imagej software [ 26 ] on simple geometries with known fractal dimensions ( line , square , koch curve )  . for each individuated subpopulation , the fd calculation was performed on all gtv slices ; mean , median , maximum and minimum fd distribution values were considered as parameters representing the spatial organisation of the subpopulation . feature extraction three types of features were automatically calculated by means of moddicom : ( 1 ) fractal features , considered as parameters quantifying the tumour heterogeneity . ( 2 ) morphological features , describing the tumour geometry and gtv shape ( surface and volume , surface / volume ratio , eccentricity )  . ( 3 ) statistical features , describing the behaviour of greylevel histogram representing the gtv volume ( entropy , skewness and kurtosis )  . cian of gaussian ( log ) filter to the raw images . this filter consists of an implemented convolution kernel that applies the following equation to the original pixels : x2 + y2 log ( x , y ) = 2 [ e x2 + y2 22 ] where x and y represent the coordinates of pixels surrounding the central one ( on which equation is used to calculate the convolution ) and is the size of standard deviation in the log equation , expressed in mm [ 27 ]  . this filter , adopted by ng etal . 
highly relevant features were identified as a first step for data analysis using the wilcoxon test method . this test was recently addressed as the most reliable and accurate method for feature selection in radiomics by parmar etal . 
the statistical tests performed confirmed the heterogeneity of the cohorts adopted . pathologic complete response ( trg = 1 ) was reached in 47 patients of rome ( pcr occurrence rate equal to 27% ) and in 7 patients of maastricht ( pcr occurrence rate equal to 28% )  . 
the proportions observed between positive and negative outcomes were consistent with clinical literature data [ 12 ]  . the majority of the rome patients ( 83.3% ) had a prescription dose of 55gy . 
 [ 7 ] have recently proposed a strategy to normalise the mr signal in brain , dividing each voxel intensity by the standard deviation of the whole brain signal . this methodology was applied to the mr images of 81 glioblastoma patients and a predictive model was then proposed to identify patients with poor prognosis at the time of tumour diagnosis . 
in particular , the authors quantified tumour heterogeneity , creating different radiomic profiles originating from the combination of the information extracted from four different mr contrasts . in this investigation , we presented a new approach to process the mr signal , consisting in the normalisation of each pixel inside the gtv in reference to the 1st and 99th percentile of the overall gtv intensity level histogram , to eliminate spike signals and focus on the informative content of the analysed gtv . potentialities offractal analysis inradiomics after the normalisation , we evaluated the tumour heterogeneity analysing the spatial organisation of the pixel clusters with common intensities by means of fractal dimensions , as performed by szigeti etal . , on lung cancer ct images [ 20 ]  . the results obtained in the feature selection process showed that the fractal parameters related to tumour subpopulations have higher performance in predicting pcr than statistical and morphological features . the high informative content of the fractal dimension was also confirmed in the elaboration of the predictive model , where the maximum fd of the subpopulation with pixel intensity higher than 40% appeared to be the most significant parameter of the model . 1 3 292 la radiologia medica ( 2018 ) 123 : 286295 fig . 
3 nomogram of the predictive model developed 1 3 la radiologia medica ( 2018 ) 123 : 286295 the proposed statistical model predicts with high accuracy ( auc = 0.78 in training set and 0.80 in validation set ) whether pcr will be obtained for a specific patient , starting from the analysis of the staging mr . a predictive model for pcr starting from 18fdg petct images was recently proposed by van stiphout etal . 
 [ 37 ] proposed a model to evaluate treatment response after crt in larc patients , by analysing different mr sequences ( t2w volumetry , dw - mri and dce - mri ) acquired before and after crt . 
in their explorative study ( 55 analysed patients ) , they observed that a significant increase in the apparent diffusion coefficient ( adc ) after crt was correlated to non - responder patients . one of the most significant advantages offered by our model is represented by the fact that only mr images acquired before treatment are required to calculate the pcr probability . 
4 gtv slice where the maximum fd was calculated for a patient who experimented pcr ( left ) and for a patient who did not show pcr ( right ) .in the red scales , the pixel values with normalised intensities higher than 40% are reported conclusion the possibility to provide spatial information related to tumour sub - regions can furthermore open important scenarios in biophysics and radiotherapy planning . 
in fact , assuming that the pixel clusters with shared intensity levels correspond to cell groups with individual physical and radiobiological characteristics , the possibility to detect these clusters could allow dose modulation within the tumour through dose - painting protocols . in conclusion , the method proposed in this work is able to detect from mr images , valuable information about the rectal tumour heterogeneity , to predict the pcr probability after crt in case of larc patients . funding this study was not funded by any company . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
 we want to prospectively investigate the use of additional superb microvascular imaging ( smi ) and strain elastography to b - mode ultrasound in thyroid nodules in distinguishing benign from malignant thyroid nodules . methods we analyzed 52 thyroid nodules ( malignant = 26 , benign = 26 ) and reviewers scored the likelihood of malignancy for three data sets ( i.e. , b - mode ultrasonography alone , b - mode ultrasonography + smi , and b - mode ultrasonography + strain elastography )  . 
the area under the receiver - operating characteristic curve ( az ) values , sensitivities , and specificities were compared . results a comparison of the data sets revealed that area under the receiver - operating characteristic curve values were similar without statistical difference . 
several suspicious ultrasonographic features predict thyroid cancer , including hypoechogenicity , a spiculated or microlobulated margin , microor macro - calcifications , and a taller - thanwider shape [ 2 , 3 ]  . 
in addition , none of these ultrasonographic findings has sufficient specificity to classify a lesion as malignant [ 68 ]  . doppler ultrasonography is widely used for evaluating vascularity of thyroid nodules . 
rationale for studying vascularity of thyroid nodules is the observation that cellular proliferation correlates with increased vascularization that vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2018 ) 123 : 260270 may lead to anarchical angiogenesis present in malignancy [ 9 , 10 ]  . 
although several studies have revealed that presence of intranodular vascularity may increase risk of malignancy [ 11 , 12 ] , the association between intranodular vascularity and risk of malignancy has not been consistently proven [ 6 , 7 , 13 ]  . 
 [ 12 ] described color doppler characteristics that may be useful in distinguishing malignant from benign nodules and may facilitate selection of the lesion to sample in patients with many thyroid nodules . 
 superb microvascular imaging ( smi ) , developed by toshiba medical systems , is a new microvascular flow imaging mode implemented on the aplio 500 ultrasound system ( toshiba medical systems , tokyo , japan )  . 
smi uses advanced clutter suppression to extract flow signals from large to small vessels and depicts this information at high frame rates as a color overlay image ( color smi ) or as a grayscale map of flow ( monochrome smi )  . 
in a recently published article , the authors demonstrated that smi could depict perinodular and intranodular vascular flow with greater detail than color doppler imaging and power doppler imaging [ 14 ]  . ultrasound elastography is a non - invasive technique that can provide an objective evaluation of tissue stiffness , and it is useful in differentiating benign from malignant thyroid nodules [ 15 , 16 ]  . 
malignant thyroid nodules are much harder than benign ones at palpation ; therefore , these malignancies are often associated with changes in mechanical properties of a tissue , and ultrasound elastography has been used to differentiate cancers from benign lesions . 
two kinds of elastography techniques ( strain and shear waves ) are currently used in clinical practice , and both techniques differ in terms of the forces measured and imaging methods [ 17 ]  . 
fine - needle aspiration ( fna ) is the standard tool for determining if a thyroid nodule is malignant , but it is invasive and may cause minor complications [ 21 ]  . 
compared with acoustic radiation force impulse imaging , that can measure average shear - wave velocity in a small region of interest ( roi ) for short durations ( less than 1ms ) , strain elastographic images are acquired by displacing tissue under stress by repeated manual compression of the transducer . 
in this technique , malignant nodules , typically denser than benign nodules , are less responsive to applied stress than the surrounding normal thyroid parenchyma . these above - mentioned techniques can improve diagnostic performance of conventional ultrasonography and be beneficial in decision - making for management of thyroid nodules ; therefore , they could contribute to decrease overtreatment . 
therefore , the purpose of this study was to prospectively investigate use of additional superb microvascular imaging ( smi ) and strain elastography to b - mode ultrasound in thyroid nodules in distinguishing benign from malignant thyroid nodules . materials andmethods patients andlesions this prospective study was conducted with institutional review board approval of chung - ang university hospital , and informed consent for ultrasound elastography and smi was obtained from patients . 
according to the consensus statement and recommendation of the korean society of thyroid radiology ( ksthr ) , thyroid nodules were categorized into three groups according to features on b - mode ultrasonographysuspicious malignant , probably benign , and indeterminate nodules [ 3 ]  . 
mean ultrasonography follow - up duration was 314days ( range 240348days ) in included cases . ultrasonographic examinations andultrasoundguided procedures the conventional thyroid ultrasonographic examinations were conducted by one of three radiologists with 510years of experience in thyroid ultrasonography . 
after b - mode ultrasonography , only patients scheduled to undergo ultrasound - guided fna underwent smi and strain elastography , conducted by one radiologist with 5years of experience in thyroid ultrasonography using a high - resolution ultrasound device with a 14 - mhz probe ( aplio 500 , toshiba medical systems )  . first , b - mode ultrasonographic images were acquired , and then , the smi and strain elastographic images were 1 3 262 la radiologia medica ( 2018 ) 123 : 260270 acquired in the same plane , without changing patients position . 
color and monochrome smi were obtained for nodules and focal zone , by maintaining a constant scanning depth and time - gain compensation throughout the study duration to optimize visualization of the target region . 
after adjusting the pressure and speed of manual compression to reveal the muscle as a mix of red and green for the reference area , representative strain elastographic images were acquired . ultrasound - guided fna was conducted using a 23 - gauge needle attached to a 5 - ml syringe . 
repeat biopsy was conducted when cytological findings of nodules were non - diagnostic or revealed atypia of undetermined significance or follicular lesion of undetermined significance ( aus / flus )  . 
 ultrasound - guided core - needle biopsy was conducted using a free - hand technique with an 18 - gauge dual - action semiautomatic core biopsy needle having a 22 - mm throw . 
 specimens from fna and biopsy were analyzed by a thyroid pathologist with 15years of experience . data andstatistical analysis still images and cine loops of thyroid nodules from the ultrasonographic examinations , including the smi and strain elastographic images , were analyzed by two experienced radiologists that did not perform the smi and strain elastography ( i.e. , they were blinded to cytology results )  . 
the result was accepted when scores provided by both reviewers were the same ; otherwise , the score provided by the reviewer with 10years of thyroid imaging experience was accepted . 
a score of 1 indicated the absence of intranodular or perinodular vascularity ( no vascularity ) ; a score of 2 indicated the presence of circumferential vascularity at the margin of the nodule ( perinodular vascularity ) ; a score of 3 indicated intranodular vascularity with or without perinodular vascularity , less than 50% ( mild intranodular vascularity ) ; and a score of 4 indicated marked intranodular vascularity with or without perinodular vascularity , greater than 50% ( marked intranodular vascularity )  . 
color - coding of elastographic images was conducted according to the scoring system recommended by asteria etal . , and red / green and blue represented soft and hard tissues , respectively ( fig.2 ) [ 16 ]  . 
a score of 1 indicated nodules that presented elasticity in the whole examined area ( homogeneously green ) ; a score of 2 indicated nodules that presented elasticity in a large portion of the examined area ( almost the whole tumor is light green and red with some peripheral and / or central blue areas ) ; a score of 3 indicated nodules with stiffness in a large portion of the examined area ( almost the whole tumor is in hard blue with some light green and red areas ) ; and a score of 4 indicated non - elastic nodules ( homogenously hard blue )  . to evaluate the diagnostic performance of the three data sets ( i.e. , b - mode ultrasonography alone , b - mode ultrasonography + smi , and b - mode ultrasonography + strain elastography ) in distinguishing benign from malignant thyroid nodules , two reviewers scored the likelihood of malignancy ( 0100 ) for each data set , respectively . 
 according to this , probably benign nodules were scored from 0 to less than 10 , indeterminate nodules were scored from 10 to less than 50 , and suspicious malignant nodules were scored from 50 to 100 . 
in the second and third reading sessions , the reviewer was asked to consider a change in the scoring of likelihood of malignancy , according to the findings of smi and strain elastography . 
 reader agreement between the two radiologists in evaluating diagnostic performance of data sets was estimated using intraclass correlation coefficient ( icc ) [ 26 ]  . in addition to determining sensitivity and specificity of b - mode ultrasonography for each data set , sensitivity and specificity were compared with those of nodules downgraded or upgraded using mcnemars test based on the binary management decision of whether to perform fna [ 27 ]  . 
if an elasticity score of 4 or an smi score of 4 was assigned , the category of the nodule was selectively upgraded from 1 ( probably benign ) to 2 ( indeterminate to suspicious )  . 
 among the other 9 nodules , 7 were proven as aus / flus on the initial fna and repeat biopsy and two were proven as follicular neoplasms after repeat biopsy . 
surgical confirmation was conducted for 18 nodules ; the malignant lesions comprised papillary carcinoma ( n = 15 ) , and benign lesions comprised follicular adenoma ( n = 2 ) and nodular hyperplasia ( n = 1 )  . 
in terms of auc values , compared with b - mode ultrasonography alone , combined use of ultrasonography with strain elastography or smi improved performance of both reviewers in distinguishing benign from malignant nodules . 
 excellent agreement was observed between the reviewers for b - mode ultrasonography alone , b - mode ultrasonography + smi , and b - mode ultrasonography + strain elastography ( table1 )  . after selectively upgrading or downgrading the nodule category based on elasticity and smi scores , seven nodules were downgraded from category 2 ( indeterminate to suspicious ) to category 1 ( probably benign )  . 
however , most studies analyzed diagnostic performance of the combined set ( b - mode ultrasonography + strain elastography ) as well as strain elastography alone as an ultrasonographic finding . 
the reason for this result is unclear ; however , we used a malignancy likelihood ranging from 0 to 100 for comparing data sets , different from that used in the previous reportsthey used 4to 5 - point scoring scales or a strain ratio . 
 [ 14 ] described that smi demonstrated microvascular flow with significantly higher image scores and provided a better depiction of vessel branching details than did color doppler imaging or power doppler imaging in all thyroid nodules . 
3 results of the area under the receiver - operating characteristic curve ( auc ) of the malignancy likelihood of thyroid nodules for differentiating benign from malignant nodules ( reviewers 1 and 2 ) discussion in our study , all data sets ( b - mode ultrasonography , b - mode ultrasonography + smi , and b - mode ultrasonography + strain elastography ) revealed statistically significant differences between benign and malignant nodules assessed by both reviewers . 
therefore , according to our results , smi could have similar or better ability than b - mode ultrasonography alone in differentiating benign and malignant thyroid nodules . to our knowledge , this was the first study to compare the performance of b - mode ultrasonography with a combination of other techniques ( strain elastography and smi ) using multiple cases of thyroid nodules consecutively encountered in real clinical practice . 
recent studies using ultrasound elastography have focused on its potential in reducing the odds of fna or biopsy with benign results because of further discrimination of low suspicion lesions [ 27 , 28 ]  . 
according to the ksthr guideline , indeterminate nodules larger than 1 cm and suspicious nodules larger than 0.5cm should be candidates for ultrasound - guided fna [ 3 ]  . 
in this study , mean nodule size was 1.27cm , and five of seven nodules , downgraded based on elasticity and smi scores , were larger than 1cwe suggested the standard of corrected category 1 ( probably benign nodule ) and corrected category 2 ( indeterminate to suspicious nodule ) for binary management decision - making , and it could be acceptable . 
moreover , all seven downgraded nodules were initially categorized as indeterminate nodules ; therefore , combined use of strain elastography and smi may be beneficial in correctly classifying indeterminate nodules on b - mode ultrasonography . 
some reports have suggested that doppler ultrasonography was not beneficial in differentiating benign from malignant thyroid nodules [ 3 , 7 , 13 ] , because internal vascularization can be detected in hyperplastic follicular proliferation or granulation tissues in large nodules of colloid goiter [ 29 ]  . 
on fna , the nodule was confirmed as papillary thyroid cancer table 2 characteristics of seven nodules that were downgraded based on the elasticity and smi scores initial category on b - mode ultrasonography downgraded category based on management decision elasticity score smi score size on b - mode ultrasonography ( cm ) final diagnosis indeterminate indeterminate indeterminate indeterminate indeterminate indeterminate indeterminate smi superb microvascular imaging 21 21 21 21 21 21 21 benign benign benign malignant benign benign benign ultrasonography has been constantly assessed for the evaluation of thyroid nodule , because increase of vascularity is usually related to cellular proliferation in a neoplastic condition [ 30 ]  . 
in addition , proportion of malignancy of included nodules was relatively high ; this study was prospectively conducted in a tertiary university hospital ; therefore , most of our patients were referred from local clinics or screening centers when they had suspicious findings . 
nine nodules were excluded , because repeat biopsy revealed aus / flus or follicular neoplasaccording to the bethesda system [ 24 ] , malignancy risk of these categories was 515 and 1530% , respectively . 
second , duration of imaging follow - up in cases of imagingpathologic concordant benign lesions after fna was relatively insufficient in our study to eliminate the issue of sampling error . 
however , if we had conducted quantitative analysis , results may have varied , because it would have involved use of continuous variables . in conclusion , additional use of smi and strain elastography revealed similar diagnostic performance to the conventional thyroid ultrasonography in distinguishing benign from fig . 
when a nodule with indeterminate ultrasonographic features demonstrates no stiffness on strain elastography or no vascularity on smi , we recommend follow - up rather than fna , without a significant change in sensitivity . 
this could potentially lead to an increase in specificity on thyroid ultrasonography . compliance with ethical standards conflict of interest author hye shin ahn declares that he has no conflict of interest . 
subgroup analysis was performed between general and orthopaedic hospitals with mannwhitney u and 2 statistics . results a total of 129 / 2405 answers ( 5.4% of members ) were included in our analysis . 
the percentage of procedures and the use of autologous preparations were significantly higher in orthopaedic hospitals than in general hospitals . keywords joint injection bursa tendon calcific tendinopathy interventional musculoskeletal procedures ultrasound * luca maria sconfienza io@lucasconfienza.it introduction 1 unit ofradiology , ospedale evangelico internazionale , piazzale gianasso 5 , 16100genoa , italy 2 department ofbiotechnology andapplied clinical science , university oflaquila , laquila , italy 3 department ofradiology , di.bi.med. , university ofpalermo , via del vespro 127 , 90127palermo , italy 4 unit operativa di radiologia diagnostica ed interventistica , irccs istituto ortopedico galeazzi , via riccardo galeazzi 4 , 20161milan , italy 5 dipartimento di scienze biomediche perla salute , universit degli studi di milano , via festa del perdono 7 , 20122milan , italy 6 s.c. 
diagnostica perimmagini e ecografia interventistica , ospedale evangelico internazionale di genova , salita superiore san rocchio 31 / a , 16122genoa , italy over the past years , therapeutic musculoskeletal procedures have become widely diffuse in both public and private institutions , with increasing indications over time [ 16 ]  . 
hence , ultrasound has emerged as a cheap , quick , and reliable tool for real - time guidance of the needle during procedures , avoiding vascular and nervous structures and ensuring the correct achievement of the injection site , as well as to detect potential complications [ 811 ]  . 
however , to our knowledge , there are no published papers on the real diffusion of therapeutic musculoskeletal procedures . thus , the aim of our study was to perform an online survey among all members of the musculoskeletal section of the italian society of medical and interventional radiology to understand how therapeutic musculoskeletal procedures are performed in daily practice in italy . materials and methods study design institutional review board approval was not required because this paper does not involve patient data . 
the list of questions is reported in table1 . on october 2nd , 2017 , an email was sent out to all members , inviting them to participate in this report . 
they were informed that completion of the questionnaire would have required not more than 5min and that the survey was anonymous and data would be managed in aggregated form to ensure anonymity . 
participants were also asked to talk to other colleagues working in the same institution to avoid data duplication . members could provide their name and email address , which were not linked to the data . 
the link to participate in the poll remained open for 20days and was closed on october 22nd , 2017 . data analysis once received , the database was analysed for further analysis . 
joint injections were performed in 88.9% of institutions , whereas bursal / tendon injection , and percutaneous irrigation of calcific tendinopathy were performed in 74 and 58% of the hospitals , respectively . 
full data regarding subgroup analysis are reported in table3 . discussion our main findings were that the most common therapeutic musculoskeletal procedures performed in 2016 were joint injection , bursal / tendon injection , and percutaneous irrigation of calcific tendinopathy , arthropathic pain being the main indication . 
further , the number of procedures performed in orthopaedic hospitals was significantly higher than in general hospitals , as well as for the use of autologous 1 3 la radiologia medica ( 2018 ) 123 : 314321 preparations such as platelet - rich plasma or mesenchymal stem cells . our survey found that joint injection and bursal / tendon injections are the most frequent procedures , as indirectly proved by the wide literature published on this topic [ 6 , 10 , 27 , 28 ]  . 
as an example , injections in the glenohumeral and knee joint [ 27 ] , the scaphotrapeziotrapezoid joint [ 28 ] , the tendon sheath of the long head of the biceps [ 29 ] , have shown to be significantly more accurate when guided by ultrasound rather than by the palpation of anatomical landmarks . 
according to our data , it is the second most common interventional musculoskeletal procedure in orthopaedic hospitals , with calcific tendinopathy being the second most common indication for imaging - guided interventions in these institutions . 
at first , it was a fluoroscopic procedure , although ultrasound has clearly replaced fluoroscopy as a more reliable , safer , and easier guidance in this setting [ 3032 ]  . ultrasound has several well - established advantages in comparison with fluoroscopy , among which it does not use ionizing radiations , it is widely available and provides highquality real - time imaging of soft tissues [ 33 , 34 ]  . 
furthermore , a crucial point is the preservation of antisepsis through careful and precise measures , which can be guaranteed also in ultrasonography rooms . conversely , the percentage of fluoroscopic procedures performed in interventional radiology rooms is higher in orthopaedic hospitals than in general hospitals . 
at any rate , these data could be explained by the fact that in orthopaedic hospitals there is a significantly higher request and amount of interventional musculoskeletal procedures to be performed , as demonstrated by our data . 
this result could be explained not only by the direct cooperation between radiologists and orthopaedists , but also by the greater availability of the required equipment and higher experience in this setting of musculoskeletal radiologists working in orthopaedic hospitals . 
these autologous preparations have demonstrated promising results in several pathologic conditions , since they provide several molecules capable to promote healing mechanisms and reducing degenerative processes , with no significant side effects due to their autologous nature [ 18 , 3537 ]  . 
however , it is important to know how and when to use them , to achieve the best cost - effectiveness for our patients , since some controversial results have been achieved using these relatively newer treatments , especially in osteochondral lesions and tendinopathies [ 3842 ]  . regarding major spinal treatments , such as vertebroplasty or discal interventions , a relatively low number of answers might have been obtained because some interventional radiologists are not registered with the italian college of musculoskeletal radiology but only to the italian college of interventional radiology . 
furthermore , we did not include in our survey more advanced procedures , such as thermal or high - intensity focused ultrasound ablations , which are performed by a limited number of centres [ 1 , 3 , 24 ]  . 
this certainly reflects the different local 1 3 320 la radiologia medica ( 2018 ) 123 : 314321 situations in terms of health policy , relationships between radiologists and other physicians , and education . in conclusion , our report reveals that the most common interventional musculoskeletal procedures performed in italy in 2016 by the members of the italian college of musculoskeletal radiology were joint injections , bursal / tendon injection , and percutaneous irrigation of calcific tendinopathy , arthropathic pain being the main indication . 
authors want to thank all members who completed the survey in full and gave their consent to publish their names : alessio angileri , francesco arrigoni , angelo asciano , raffaele averna , francesco bartelli , alberto bellelli , massimo giuliano bonetti , mario canepari , rinaldo capoccia , cristian caporali , emanuele ciarci , federico ciolina , paolo comes , armando conchiglia , luca de flaviis , pierluigi de matteis , paola erra , gianluigi di giulio , marilene eccher , carlo faletti , giampiero feltrin , gisella ferretti , giovanni foti , michele liotti , alessandro lupi , nicola magarelli , daniele maiettini , giorgia manfredonia , sabino mangino , fabio melchiorre , davide monti , giovanni musella , alessandro napoli , mauro niccolini , dario notaro , giulio pasquotti , luciano perini , caterina peroni , lucia pinali , vincenzo pipitone , stefano romiti , domiziana santucci , giancarlo sarnelli , giuseppe sarti , germano scevola , marco scrocca , casimiro simonetti , michele solarino , giulio vallati , carlo zanolini . compliance with ethical standards ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
 for this type of study ethical approval and patients consent were not required . funding no funding was obtained for the present study . conflict of interest all authors are members of the musculoskeletal college of the italian society of medical and interventional radiology . 
mariani springer milan dordrecht heidelberg london new york , 2013 isbn : 978 - 88 - 470 - 2762 - 6 e - isbn : 978 - 88 - 470 - 2763 - 3 published online : 16 march 2013 springer - verlag 2013 the authors of this 331 - page case - based atlas , published under the aegis of the study group of inammation / infection of the italian association of nuclear medicine ( aimn ) , aim to present the reader with an overview of the use and results of nuclear medicine in the eld of infection and inammation . after clearly dening inammation and infection , the thirteen chapters of the book provide examples of imaging and practical clinical cases in order to properly evaluate the problem / s under discussion . the opening chapter which claries normal ndings covers different radiopharmaceuticals and techniques including the ever increasing use of multimodality fusion imaging ( spect / ct and pet / ct ) , with its variants and pitfalls . 
chapters on various infection and inammation sites follow : tissues ; bone and joints ; joint prosthesis ; vascular prosthesis ; nonorthopaedic or cardiovascular implantable devices ; central nervous system , head and neck structures ; infective endocarditis and cardiovascular implantable electronic devices ; fever of unknown origin ; abdomen ; diabetic foot ; lung ; chronic inammatory diseases . 
 in each chapter , examples and clinical cases are introduced by a few pages of background material and a thorough presentation of the sites of infection or inammation . all of the contributing authors , from different italian and spanish centres , have masterfully treated the different topics enriching them with a large cohort of clarifying , and very useful images ( beware : ct images in one case are presented as mri scans ; aortography as a selective right renal arteriography in another )  . 
 the book will be very useful as a teaching aid for trainees in nuclear medicine and radiology as well as clinicians who are often unaware of the diagnostic opportunities gli autori di questo atlante di 331 pagine , basato sulla casistica , pubblicato sotto legida del gruppo di studio inammazione / infezione della associazione italiana di medicina nucleare ( aimn ) , ha lo scopo di presentare al lettore una panoramica sullimpiego ed i risultati della medicina nuclea re nei riguardi dei processi infettivi ed inammatori . dopo aver ben chiaramente denito i termini inammazione ed infezione , i 13 capitoli del volume presentano esempi , mediante immagini e casi clinici pratici allo scopo di poter valutare in modo corretto il / i problema / i in discussione . 
 il capitolo di apertura , oltre a specicare i reperti normali , tratta dei differenti radiofarmaci e delle tecniche , includendo le sempre pi usate tecniche multimodali di fusione delle immagini ( spect / ct e pet / ct ) , comprese le varianti e le difcolt delle stesse . 
poi seguono i capitoli dedicati alle possibili sedi di infezione ed inammazione : tessuti ; ossa ed articolazioni ; protesi articolari ; protesi vascolari ; mezzi non - ortopedici o cardiovascolari di impiantologia ; sistema nervoso centrale , strutture della testa e del collo ; endocardite infettiva ed impianti elettronici cardiovascolari ; febbre di origine sconosciuta ; malattie inammatorie croniche . in ciascun capitolo , alcune pagine descrittive dellargomento in esame ed una precisa presentazione delle sedi di infezione ed inammazione trattati nello stesso , fanno da introduzione ai relativi esempi e casi clinici . tutti gli autori del volume , provenienti da differenti centri in italia e spagna , hanno trattato magistralmente i diversi argomenti , arricchendoli con una larga messe di immagini puntuali e molto utili ( attenzione per : immagini ct sono presentate come esempio di rm , in un caso ; una aortograa , come unarteriograa selettiva renale , in un altro )  . questo testo sar assai utile , quale strumento di apprendimento , sia per gli specializzandi in medicina nucleare e in radiologia , che per i clinici , spesso alloscuro delle possibiradiol med ( 2013 ) 118 : 898899 offered by radionuclide imaging , which offers benet to the patient , sometimes overrunning other radiological modalities . in my opinion , unexplained acronyms and the lack of an index at the end of the book are only small drawbacks to this otherwise instructive text . lit diagnostiche che lo studio per immagini con radionuclidi offre quali beneci al paziente , essendo spesso superiori ad altre modalit radiologiche . secondo il mio punto di vista , la presenza di acronimi non deniti per esteso e la mancanza di un indice nale sono piccole manchevolezze di questo volume , per il resto istruttivo . 
del vescovo , campus bio - medico , university of rome , via alvaro del portillo , 200 trigoria , rome , italy , tel . : + 39 - 06 - 225411633 , e - mail : r.delvescovo@unicampus.it received : 26 february 2011 / accepted : 4 december 2011 / published online : 17 september 2012 springer - verlag 2012 abstract purpose . 
prima del trattamento , le lesioni intra - ghiandolari ipointense nelle sequenze pesate in t2 ed iperintense nelle sequenze post - contrastograche pesate in t1 sono state interpretate come sospette per localizzazione di neoplasia per poi essere state confermate , come sede di adenocarcinoma prostatico , con il psa e con lesame istologico in tutti e 25 i pazienti ( rho = 1 e p < 0 , 001 )  . 
as the volume of tissue destroyed is generally small ( 13 mm in depth ) , it is necessary to carry out several local adjoining treatments to create a sufciently large area of necrosis [ 2 ]  . 
various causes have been proposed , including patient movement during treatment , untargeted tumour sites , complex lesions or differences in perfusion patterns due to the neoplasm [ 6 , 7 ]  . intratumoral haematic ow is notoriously inuential on the effects of hyperthermia . 
treatment of murine livers with ultrasound equal to 67425 w / cm2 with exposure times of 320 s revealed that the area of necrosis induced in vivo is directly dependent on us intensity and exposure duration [ 7 ]  . 
it remains unclear how hifu - induced ablation alters prostate perfusion at the tumour site [ 7 ]  . dynamic contrast - enhanced magnetic resonance ( dcemr ) imaging , which requires the activity of gadolinium chelates ( molecules of low molecular weight ) , is the noninvasive method of choice for evaluating glandular microcirculation [ 9 ]  . 
the aim of this study was to evaluate , using quantitative analysis , the diagnostic performance of dcemr imaging in prostate adenocarcinoma before and after transrectal hifu . lhigh intensity focused ultrasounds ( hifu ) trans - rettale un trattamento innovativo , minimamente invasivo , riservato a pazienti non chirurgici , affetti da adenocarcinoma della prostata localizzato [ 1 ]  . 
il volume di distruzione tissutale mediamente di piccole dimensioni ( 13 mm in profondit , 520 mm in altezza ) [ 2 ] e pertanto , al ne di determinare unampia area di necrosi , necessario indurre multipli trattamenti locali , limitro . 
tuttavia , anche se larea di termoablazione generalmente omogenea , sono stati riportati in letteratura casi di persistenza di cellule tumorali successivamente al trattamento [ 4 , 5 ]  . 
il perch si registrino queste precoci riprese di malattia non risulta legato ad ununica motivazione ; in letteratura vengono descritte diverse cause tra cui il movimento del paziente in corso di trattamento , foci di tumore non bersagliati , lesioni complesse o la presenza di aree con differente perfusione nel contesto della neoplasia [ 6 , 7 ]  . 
 [ 7 ] , trattando fegato di topi per mezzo di intensit di ultrasuoni pari a 67425 w / cm2 con tempi di esposizione compresi tra 320 secondi , hanno dimostrato che larea di necrosi indotta in vivo direttamente dipendente dallintensit degli ultrasuoni e dalla durata di esposizione , e che le lesioni si riducono no al 40% delle dimensioni iniziali , variando tali parametri indipendentemente dal fatto che il tessuto sia o meno perfuso . 
leffetto che ha lalterata perfusione della ghiandola prostatica nella sede del tumore nei riguardi dellablazione indotta dellhifu non ancora chiaro . la risonanza magnetica perfusionale ( rm - p ) , prevedendo limpiego di chelati del gadolinio ( molecole con basso peso molecolare ) , la metodica non - invasiva di scelta per radiol med ( 2013 ) 118 : 851862 materials and methods patients and treatment between may and october 2009 , we prospectively analysed 25 consecutive patients affected by prostate cancer and diagnosed with intraglandular adenocarcinoma ( t1t2 ) , with an average age [ standard deviation ( sd ) ] of 706 ( range , 5583 ) years ; median , 71 , an average prostate - specic antigen ( psa ) value ( sd ) of 9.05.3 ng / ml ( range , 0.3028.6 ng / ml ; median , 8.2 ng / ml ) and an average prostate volume ( sd ) of 2813 cm3 ( range , 1654 cm3 ; median , 28 cm3 )  . 
 the study was approved by the institutional review board , and patients gave oral and written informed consent . all patients , before us treatment , underwent transurethral resection of the prostate ( turp ) .treatment required the use of the ablatherm device : the patient was positioned on an ablatherm bed lying on their right side . 
the device consisted of an endorectal probe composed of two different transducers : one 7.5 mhz to plan treatment , and the other 3 mhz for the actual treatment , with a length of 40 mm ( ultrasonic intensity in situ equals 1 , 500 w / cm2 )  . 
the operator , once focused on the intraglandular lesion , determined a series of adjoining treatments , from the top to bottom , with a thickness of 1.7 mtotal treatment duration was approximately 2 h , with each shot lasting 5 s and a 5 - s interval to allow heat dissipation of heat , for a total of 400600 shots . 
psa value was evaluated at 1 , 4 and 6 months after treatment . dynamic contrast - enhanced magnetic resonance ( dce - mr ) imaging the mr examination was carried out with a 1.5 - tesla magnet ( symphony , siemens medical systems , erlangen , germany ) with a phased - array coil . 
dce - mr imaging was performed the day prior to and 1 , 4 and 6 months after hifu treatment using the following sequences : t2 - weighted turbo spin - echo ( tse ) at high resolution [ time to repetition ( tr ) 6.130 ms , effective time to echo ( te ) 109 ms , slice thickness 4 mm , eld of view ( fov ) 180180 mm , matrix 256192 , three excitations , echo train length 21 ] in the axial , coronal and sagittal planes ; t1 - weighted turbo fast low - angle shot ( flash ) with fat suppression ( tr / te 838 / 2.75 ms ; inversion time 500 ms ; ip angle 10 ; fov 2438 cm ; matrix 160256 voxels ; slice thickness 5 mm ; slice number three ; 25 images per slice at intervals of 2.5 s ) in the axial plane before and during intravenous administration of the contrast medium . paramagnetic contrast agent ( dotarem ; guerbet laboratories , aulnay - sous - bois , france ) was administered intravenously by an automatic injector at a rate of 4 ml / s with a la valutazione della microcircolazione ghiandolare [ 9 ]  . 
 obiettivo del nostro studio stato , dunque , quello di valutare , per mezzo di unanalisi quantitativa , la performance diagnostica della rm - p nelladenocarcinoma della prostata prima e dopo hifu trans - rettale . materiali e metodi pazienti e trattamento abbiamo analizzato 25 pazienti affetti da neoplasia della prostata con diagnosi di adenocarcinoma intra - ghiandolare ( t1 - t2 ) , con unet media [ deviazione standard ( ds ) ] di 706 anni ( range 5583 anni ; mediana = 71 anni ) , valori dellantigene prostatico specico ( psa ) medi ( ds ) di 9 , 05 , 3 ng / ml ( range 0 , 3028 , 6 ; mediana = 8 , 2 ) e volume prostatico medio ( ds ) di 2813 cm3 ( range1654 ; mediana = 28 )  . 
il device costituito di una sonda endorettale che contiene due differenti trasduttori : uno da 7 , 5 mhz volto a pianicare il trattamento , un altro da 3 mhz per il trattamento vero e proprio , con una profondit di lunghezza ssa pari a 40 mm ( intensit ultrasonora in situ pari a 1500 w / cm2 )  . 
loperatore , una volta ssato il punto della lesione focale intra - ghiandolare , determinava una serie di trattamenti , limitro , dallapice alla base , con spessore pari a 1 , 7 mla durata complessiva del trattamento era di circa 2 h : ogni shot era pari a 5 s , con un intervallo di altri 5 s volto a consentire la dissipazione del calore , per un totale di circa 400600 shots . 
il dosaggio del psa avvenuto ad intervalli regolari di 1 mese , 4 mesi e 6 mesi successivi al trattamento . risonanza magnetica perfusionale lesame rm stato condotto con magnete da 1 , 5 tesla ( symphony , siemens medical systems , erlangen , germania ) mediante impiego di bobina di supercie pelvica phased - array . 
la rm - p veniva effettuata il giorno prima dellhifu e ad 1 mese , 4 mesi e 6 mesi dopo il trattamento mediante impiego di sequenze : turbo spin - echo ( tse ) pesate in t2 ad alta risoluzione [ tempo di ripetizione ( tr ) 6 , 130 ms , tempo di eco ( te ) effettivo 109 ms , slice thickness 4 mm , campo di vista ( fov ) 180180 mm , matrice 256192 , 3 excitations , echo train length 21 ] , su piano di scansione assiale , coronale e sagittale ; 854 radiol med ( 2013 ) 118 : 851862 turbo - fast low - angle shot ( flash ) pesate in t1 con soppressione del segnale del grasso ( tr / te : 838 / 2 , 75 ms ; tempo di inversione : 500 ms ; ip angle : 10 ; fov : 2438 cm ; matrice : 160256 voxels ; slice thickness : 5 mm ; slice number : 3 ; 25 images per slice ad intervalli di 2 , 5 s ) su piano di scansione assiale prima e durante somministrazione di mezzo di contrasto endovena . 
 larea sospetta per neoplasia veniva indicata sulla base del risultato di rm ; pertanto , considerando il preciso numero di sezione come per la biopsia , lhifu veniva effettuata a tale livello . il volume della ghiandola prostatica stato valutato prima e 1 mese , 4 mesi e 6 mesi dopo il trattamento sulla base delle sole sequenze pesate in t2 , su piano di scansione assiale , per mezzo di un software di post - processing dedicato ( osirix , apple , macintosh ) prevedendo sezioni contigue con spessore massimo di 3 mm . analisi quantitativa manuale ( aqm ) per ogni paziente , prima del trattamento , in ogni sequenza t1 pesata dinamica , stato registrato il valore dellintensit di segnale ( is ) a livello della sospetta sede di neoplasia e della porzione controlaterale normale . 
 areas suspicious for neoplasm were indicated on the basis of mr evidence , and , considering the specic number section as in prostate biopsy , hifu was performed in that area . prostate gland volume was evaluated 1 , 4 and 6 months after treatment based on t2 - weighted sequences , in the axial plane , using dedicated postprocessing software , which required contiguous sections with a maximum thickness of 3 mm . manual quantitative analysis ( mqa ) before treatment , si was recorded on each t1 - weighted dce sequence at the level of the suspicious sites and control tissue . 
in corrispondenza della base , a livello dellemiporzione destra , si evidenzia una focale immagine ipointensa che mostra poi ( b ) precoce e signicativo potenziamento nelle acquisizioni post - contrastograche come evidenziato in questimmagine turbo - flash t1 - pesata . snr = sd of background per ogni paziente , stata calcolata la media aritmetica dei valori di snr ottenuti in ciascuna fase dinamica ; da tali valori stato creato un graco contenente due curve che illustravano la variazione nel tempo del snr della porzione ghiandolare sede di neoplasia e di tessuto normale . 
regions of interest ( rois ) are drawn at the level of the suspected site of neoplasm ( green circle ) and at an equivalent contralateral site in the apparently normal gland ( red circle )  . 
a region of interest ( roi ) to measure the standard deviation of the background noise is drawn in a region outside the patients body ( pink circle )  . 
intensit del segnale in corrispondenza dellarea sospetta sede di neoplasia ( cerchio verde ) ; intensit del segnale in corrispondenza della regione ghiandolare controlaterale sana ( cerchio rosso ) ; deviazione standard del rumore di fondo ( cerchio rosa )  . signal - to - noise ratio ( snr ) was calculated from si values by dividing the si by the sd of the background noise : snr = sd of background for each patient , arithmetic average values were calculated for the snr obtained in each dynamic phase . 
a diagram was drawn using these values , with two curves that illustrated the variations in time of the snr at the sites of neoplasm and in the healthy tissue . 
 il numero di campioni ottenuti dipendeva molto dalle caratteristiche della ghiandola e variava da 4 a 10 ( media 7 )  . analisi statistica al ne di calcolare la differenza statistica esistente tra la mediana dei valori di snr nel tempo ottenuti prima e dopo il trattamento ( ad 1 mese , 4 mesi e 6 mesi ) , stato effettuato il test di mann - whitney ( analisi intragruppo )  . lanalisi statistica utilizzata per confrontare il risultato della rm - p con i dati strumentali ( psa ed istologia ) , ha previsto limpiego di un test non parametrico ( correlazione di spearman con valori considerati signicativi con p < 0 , 05 )  . risultati prostate biopsies valutazione delle immagini rm transrectal prostate biopsies were obtained at the time of diagnosis and 6 months after treatment using an 18 - gauge needle and us guidance . 
the number of samples obtained depended on the characteristics of the gland and varied from four to ten ( average seven )  . lindagine stata eseguita correttamente in tutti e 25 i pazienti . 
prima del trattamento , le lesioni intra - ghiandolari ipointense nelle sequenze pesate in t2 ed iperintense nelle sequenze post - contrastograche pesate in t1 sono state interpretate come sospette per localizzazione di neoplasia radiol med ( 2013 ) 118 : 851862 statistical analysis the mann - whitney test ( intragroup analyses ) was used to evaluate statistical signicance between the mean snr values obtained before and after treatment . 
after hifu treatment , dce - mr imaging displayed 100% sensitivity and 96% specicity . analysis of the dce - mr imaging data before treatment , the prostate gland displayed intraparenchymal areas that in the dynamic postgadolinium ce sequences showed a progressive and increased contrast uptake with respect to the remaining glandular parenchyma , indicative of neoplasm ; at 1 , 4 and 6 months after treatment , no areas of hyperenhancement were observed either in the parenchyma or bordering the hifu - induced areas of necroper poi essere state confermate , come sede di adenocarcinoma prostatico , con il psa e con l esame istologico in tutti e 25 i pazienti ( rho = 1 e p < 0 , 001 )  . 
un solo paziente , nel controllo a 6 mesi , ha mostrato , perifericamente allarea di necrosi indotta , una focale immagine di alterato potenziamento post - contrastograco interpretata come residuo di malattia ma poi rivelatasi negativa allesame istologico ; in questo paziente il psa era inferiore ad 1 e dunque laboratoristicamente libero da malattia ( rho = 0 , 92 e p < 0 , 001 )  . prima del trattamento , la rm - p , considerando gold standard il dato istologico , mostra sensibilit = 100% , specicit = 100% , valore predittivo positivo ( vpp ) = 100% e valore predittivo negativo ( vpn ) = 100% ; dopo il trattamento hifu , presenta sensibilit = 100% e specicit = 96% . analisi dei dati di rm - p ( aqm ) la ghiandola prostatica ha mostrato , prima del trattamento , focali aree intraparenchimali che , nelle sequenze post - contrastograche ottenute dinamicamente , presentavano un progressivo ed aumentato potenziamento rispetto al restante parenchima ghiandolare ed erano indicative di neoplasia ; tale condizione non si vericava nelle porzioni ghiandolari limitrofe allarea di necrosi indotta dallhifu nei controlli condotti ad 1 mese , 4 mesi e 6 mesi dopo il trattamento , conducendo al risultato che il potenziamento post - contrastograco dinamico del parenchima ghiandolare risultava complessivamente omogeneo . prima del trattamento , nelle aree intra - ghiandolari con maggiore potenziamento post - contrastograco , i valori medi di snr nel tempo denivano una curva con rapida ascesa , picco a circa 48 s e successiva lenta discesa ; tale condizione non si vericava nella controlaterale porzione ghiandolare sana , i cui valori medi di snr nel tempo denivano una curva indice di un lento e graduale potenziamento post - contrastograco . 
a distanza di 4 mesi e 6 mesi dal trattamento la prostata mostrava un potenziamento postcontrastograco del parenchima complessivamente omogeneo ( all interno della linea rossa )  . sis , with the glandular parenchyma enhancement appearing completely homogeneous . before treatment of the intraglandular areas that exhibited the greatest contrast uptake , the average values of the snr over time dened a curve with a rapid rise , a peak of enhancement at 48 s and a subsequent slow drop . 
in particular , in the intraglandular areas with greater contrast enhancement , before - treatment average snr values over time dened a curve with a rapid rise , a peak of enhancement and a subsequent slow decrease . 
in particolare , prima del trattamento , nelle aree intra - ghiandolari con maggiore potenziamento post - contrastograco , i valori medi di snr nel tempo denivano una curva con rapida ascesa , picco di potenziamento e successiva lenta discesa ; tale condizione non si vericava nella controlaterale porzione ghiandolare sana , i cui valori medi di snr nel tempo denivano una curva indice di un lento e graduale potenziamento post - contrastograco . 
lanalisi statistica ha mostrato una differenza signicativa nellandamento delle due curve ( p < 0 , 03 )  . nei controlli rm - p condotti ad 1 mese , 4 mesi e 6 mesi successivamente al trattamento , i valori medi di snr nel tempo denivano curve pressoch analoghe nel contesto del parenchima ghiandolare limitrofo allarea di necrosi indotta e nella controlaterale sana ; pertanto lana lisi statistica condotta non ha mostrato differenze signicative nell andamento delle curve nei rispettivi periodi ( p > 0 , 01 )  . radiol med ( 2013 ) 118 : 851862 fig . 
in corrispondenza della neoplasia si evidenzia una curva con rapida ascesa , picco a circa 48 s e successiva lenta discesa ; tale condizione non si verica nella controlaterale porzione ghiandolare sana , i cui valori medi di snr nel tempo deniscono una curva indice di un lento e graduale potenziamento post - contrastograco . 
 such ndings were not observed in the control region of the healthy gland , for which the average snr values over time dened a curve indicating gradual and slow contrast enhancement . 
such an increase could be the principle factor responsible for the rapid rise of the curve and the subsequent peak in contrast uptake in neoplastic tissue . we also observed several morphological and postgadolinium modications in the dce - mr imaging evaluation after hifu treatment . 
we observed the rim of enhancement in the perinecrotic area in all patients 1 month discussione i nostri risultati dimostrano che la rm - p pu essere impiegata come ottimo strumento per la visualizzazione delladenocarcinoma della prostata ; tale condizione si verica in virt dellaumentato apporto di usso vascolare presente in corrispondenza della neoplasia rispetto al tessuto ghiandolare normale [ 11 ]  . 
 , infatti , ampiamente dimostrata lesistenza di un incremento del volume di distribuzione interstiziale ( ve ) in corrispondenza dei tessuti neoplastici legato alla distruzione dellendotelio delle cellule della ghiandola da parte della neoplasia [ 12 ] ; tale incremento potrebbe essere il principale fattore responsabile della rapida ascesa della curva e del conseguente picco di potenziamento postcontrastograco presente in corrispondenza del tessuto neoplastico . abbiamo , inoltre , osservato diverse modicazioni morfostrutturali e post - contrastograche ai controlli rm - p successivi al trattamento hifu . 
in letteratura sono presenti diversi lavori che trattano delle modcazioni rm successive a trattamento termoterapico ( laser ) [ 13 , 14 ] o con radiofrequenze [ 15 ] e crioterapico [ 16 ] che si instaurano nella prostata ed in altri organi . 
il rim di potenziamento presente nella zona perinecrotica , che abbiamo osservato in tutti i pazienti a distanza di 1 mese dalla procedura , un reperto riscontrato costantemente anche in altri tessuti ( fegato , rene ed encefalo ) nel periodo successivo al trattamento ; studi presenti in letteratura , condotti sul fegato e sul rene , hanno dimostrato che tale rim spesso molto sottile ( 1 mm ) e che , nella maggior parte dei casi , scompare a distanza di 2 mesi dalla procedura di ablazione [ 17 ]  . 
8 nei controlli rm - p condotti ad 1 mese , 4 mesi e 6 mesi successivamente al trattamento , i valori medi di snr nel tempo deniscono curve pressoch analoghe nel contesto del parenchima ghiandolare limitrofo allarea di necrosi indotta e nella controlaterale sana . after the procedure , which is consistent with that in other tissues ( liver , kidney , brain ) in the same period after treatment . 
 studies on the liver and kidney demonstrate that this rim is often very thin ( 1 mm ) and that , in the majority of cases , it disappears 2 months after the ablation procedure [ 17 ]  . in the prostate , similar ndings have been demonstrated after laser ablation for benign prostate hypertrophy and after hifu treatment [ 13 , 14 , 18 ]  . 
histological evaluation of such conditions , performed on pig and rabbit livers , shows that such a zone corresponds to an area subjected rst to inammation and subsequently to brosis [ 19 ] : the corresponding zone in humans is unknown . prostata tale condizione stata dimostrata successivamente ad ablazione laser per il trattamento dellipertroa prostatica benigna ( ipb ) e a trattamento hifu [ 13 , 14 , 18 ]  . 
 la valutazione istologica di tale condizione , condotta su fegato di coniglio e di suino , ha dimostrato che tale zona corrisponde ad unarea soggetta prima ad inammazione e successivamente a brosi [ 19 ] ; quale sia il corrispettivo sulluomo non al momento noto . ulteriore dato interessante risultato linversione del rapporto perfusionale tra il tessuto ghiandolare perinecrotico ed il parenchima controlaterale sano , con curve che mostravano un andamento omogeneo , regolare , senza raradiol med ( 2013 ) 118 : 851862 another point of interest is the perfusion ratio inversion between perinecrotic glandular tissue and healthy , control parenchyma , with curves that show a homogeneous , regular trend , with no rapid rise or peak of enhancement in the 1 - , 4and 6 - month mr imaging evaluation . 
histological results after hifu treatment demonstrated that the following changes occur according to the time of the follow - up ( 1 ) necrosis , which corresponds to the area of the prostate lacking contrast enhancement ; ( 2 ) areas of normal glandular tissue with greater expression of the connective ( brosis ) and inammatory tissue corresponding to the perinecrotic area ; and ( 3 ) normal glandular tissue . the trend in our perfusion curves was largely comparable with that of follow - up evaluations obtained at 1 , 4 and 6 months . 
thus , we present evidence that the inammatory tissue , which in the rst month following treatment constituted the rim of enhancement , did not signicantly inuence postcontrast graphic kinetics of the perinecrotic area of the gland . 
 the follow - up mr investigation proved to be indispensable , as evidenced by the 61% total reduction in glandular volume , as parenchymal evaluation with transrectal us could be very difcult . 
in addition , the excellent correlation between psa values and dce - mr imaging after treatment ( rho = 0.92 and p < 0.001 ) allowed us to hypothesise that only the post - hifu 6 - month follow - up is needed ( with psa < 1 )  . 
 a limitation of the study was that we did not routinely perform diffusion - weighted imaging ( dwi ) for neoplasm diagnosis , an essential component of the multiparametric evaluation of prostate neoplasm . despite the excellent results obtained in this study , it is necessary to evaluate a larger number of patients to establish with greater accuracy the real efcacy of hifu treatment and dce - mr imaging in the follow - up of patients with prostate adenocarcinoma . 
 pida ascesa n picchi di potenziamento nei controlli ad 1 mese , 4 mesi e 6 mesi ; tale evidenza non mai stata riscontrata nei lavori presenti in letteratura di nostra conoscenza . 
i risultati istologici , ottenuti successivamente al trattamento , dimostravano , in misura variabile a seconda del tempo di controllo : ( 1 ) necrosi , che corrispondeva allarea della prostata priva di potenziamento alla rm - p ; ( 2 ) foci di tessuto ghiandolare normale con maggiore espressione di tessuto connettivale ( brosi ) ed inltrati inammatori corrispondenti alle aree perinecrotiche ; ( 3 ) tessuto ghiandolare normale . landamento delle nostre curve di perfusione risultato essere sostanzialmente sovrapponibile nei controlli ad 1 mese , 4 mesi e 6 mesi , testimonianza che linltrato inammatorio , che nel primo mese costituisce il rim di po tenziamento , non inuisce in maniera signicativa sulla cinesi contrastograca della porzione ghiandolare perinecrotica . 
 la riduzione complessiva del 61% del volume ghiandolare rende quasi indispensabile il follow - up mediante indagine rm , in quanto risulta particolarmente difcoltosa la corretta valutazione parenchimale con esame ecotomo graco transrettale ; inoltre , lottima correlazione riscontrata tra psa e rm - p successivamente al trattamento ( rho = 0 , 92 e p < 0 , 001 ) , consente di ipotizzare il control lo post - hifu esclusivamente a 6 mesi ( se psa < 1 )  . 
limi te del nostro studio quello di non aver effettuato lin dagine con diffusion - weighted imaging ( dwi ) al ne di considerare larea sospetta per neoplasia , elemento essenziale per una corretta valutazione multiparametrica di malattia . nonostante gli ottimi risultati ottenuti , necessario valutare un pi ampio numero di pazienti al ne di poter stabilire con maggiore accuratezza la reale efcacia dellhifu e della rm - p nel follow - up . 
this observational study considered the bedside chest x - rays performed on 258 consecutive patients ( 160 men , 98 women ; mean age , 58 years ) admitted to intensive care units . 
si tratta di uno studio osservazionale sugli rx torace a letto effettuati su 258 pazienti consecutivi ( 160 maschi / 98 femmine ; et media 58 anni ) ricoverati presso i reparti di terapia intensiva . 
stata effettuata una straticazione dei pazienti in base al motivo del ricovero ed analisi sui motivi che hanno portato agli esami rx torace al ne di valutarne lefcacia diagnostica ( ed )  . 
 parole chiave terapia intensiva radiogramma del torace efcacia diagnostica introduction introduzione despite the technological advances in radiological imaging , chest x - ray ( cxr ) remains the most frequently ordered exnonostante il progresso tecnologico dellimaging radiologico , lrx torace rimane , ancora oggi , lesame pi richiesto radiol med ( 2013 ) 118 : 744751 amination for studying pulmonary disease in patients admitted to the intensive care unit ( icu ) , where it is performed at the bedside [ 15 ]  . 
clinical assessment of pulmonary diseases in critically ill patients admitted to icu or those in whom the function of one or more organs is so compromised that they require continuous monitoring of vital functions , and often pharmacological and mechanical support , is heavily dependent on imaging [ 1 ]  . intensivists can rely on increasingly advanced imaging techniques for diagnosis and follow - up of critically ill patients . 
computed tomography ( ct ) provides a detailed study of all thoracic structures with very short imaging times ; at the same time , however , it involves exposure to high doses of ionising radiation [ 6 ] and is associated with possible complications due to iodinated contrast agents and risks related to patient transport to the radiology department [ 7 , 8 ]  . 
a modality gaining an increasing role in this respect is pulmonary ultrasound ( us ) , which often enables a timely bedside diagnosis , with low costs , no invasiveness , and no ionising radiation . 
however , it remains a complementary modality limited to preliminary assessment of certain conditions affecting the pleura and subpleural regions ( pneumothorax , effusion , atelectasis , consolidation ) , which requires extensive operator experience and is therefore only performed in a small number of centres [ 9 , 10 ]  . the purpose of our study was to analyse the frequency of bedside cxr in the icu and verify its clinical value by using one of the efcacy indexes dened by the american college of radiology committee on efcacy to assess the costbenet ratio associated with radiological imaging : diagnostic efcacy ( de ) [ 11 ]  . materials and methods we retrospectively reviewed a consecutive series of 258 patients ( 160 men , 98 women ; mean age , 58 years ) admitted to an icu during the rst semester of 2010 in order to study the reasons for admission and the length of hospital stay . 
 cxr and radiology reports of patients enrolled in the study on the basis of the lists provided by the hospital wards were retrieved from the radiology information systempicture archiving and communications system ( ris / pacs ) and reviewed . 
seven subgroups were identied : patients per lo studio della patologia polmonare nei pazienti ricoverati in reparti di terapia intensiva , dove viene eseguito direttamente a letto del malato [ 15 ]  . 
la valutazione clinica delle patologie polmonari in pazienti critici ricoverati presso reparti di terapia intensiva , ovvero pazienti in cui la funzionalit di uno o pi organi cos compromessa da richiedere il monitoraggio continuo delle funzioni vitali e spesso , il loro supporto farmacologico e meccanico , fortemente condizionata dalle metodiche di imaging [ 1 ]  . attualmente , il medico rianimatore pu avvalersi di metodiche sempre pi allavanguardia per la diagnosi e il follow - up in pazienti critici ; prima fra tutte la tomograa computerizzata ( tc ) che permette , in tempi molto brevi , uno studio accurato di tutte le strutture toraciche , ma , allo stesso tempo , esposizione ad alte dosi di radiazioni ionizzanti [ 6 ] , a possibili complicanze legate alluso del mezzo di contrasto iodato e a rischi implicati nel trasporto dei pazienti presso il reparto di radiologia [ 7 , 8 ]  . 
una metodica che sta acquisendo un ruolo sempre maggiore lecograa polmonare , che spesso offre la possibilit di porre diagnosi con rapidit al letto del malato , a basso costo , in assenza di invasivit , senza lutilizzo di radiazioni ionizzanti . 
rimane comunque un esame marginale , limitato alla valutazione preliminare di alcune situazioni patologiche riguardanti la pleura ed il mantello polmonare sub - pleurico ( pneumotorace , versamento , atelettasia , consolidazione ) che richiede una grande esperienza da parte del radiologo e che quindi viene eseguito in un numero limitato di centri [ 9 , 10 ]  . lo scopo del nostro lavoro stato quello di valutare la frequenza dellutilizzo dellrx torace a letto eseguito in reparti di terapia intensiva e vericarne la validit clinica utilizzando uno degli indici di efcacia deniti dallamerican college of radiology committee on efcacy , per la valutazione del rapporto costo benecio associato alle metodiche radiologiche : lefcacia diagnostica ( ed ) [ 11 ]  . materiali e metodi stata effettuata unanalisi retrospettiva su una serie consecutiva di 258 pazienti ( 160 maschi e 98 femmine ; et media di 58 anni ) degenti nel primo semestre del 2010 presso i reparti di terapia intensiva al ne di valutare il motivo del ricovero e il tempo di degenza . 
utilizzando il sistema radiology information system ( ris ) / picture archiving and communication system ( pacs ) , sono stati rivalutati i radiogrammi e il relativi referti dei pazienti arruolati in relazione allelenco fornito dai reparti di degenza . 
we calculated the de , dened as the number of cxr showing new ndings or changes to known ndings divided by the total number of il numero totale di esami valutati stato 933 , eseguiti su 258 pazienti , con una degenza media di 12 , 7 giorni ( deviazione standard 12 , 14 )  . 
il numero medio di rx del torace effettuati nelle diverse condizioni cliniche , stato di 4 nei pazienti ir , 5 nei pazienti pt , 2 nel po , 3 , 5 in caso di neuro , 2 di po vasc , 3 in pazienti in po neuro e 7 in pazienti trap ( tabella 2 )  . 
1 paziente con emorragia subaracnoidea ( esa ) , versamento pleurico bilaterale ( a ) e suo miglioramento ad un controllo eseguito dopo 3 giorni ( b )  . radiol med ( 2013 ) 118 : 744751 fig . 
the mean number of cxr obtained in the different clinical conditions was four in rf , ve in pt , two in the po , 3.5 in neuro , two in po vasc , three po neuro and seven in transp ( table 2 )  . 
la differenza di ed nei diversi sottogruppi di pazienti esaminati , valutata con il metodo del chi - quadro , non risultata statisticamente signicativa ( p > 0 , 05 )  . discussione il radiogramma del torace permette di avere una buona rappresentazione sia del mediastino sia del parenchima polmonare ed quindi , senza dubbio , la base necessaria e spesso sufciente per supportare diverse decisioni terapeutiche , per rilevare alterazioni sospettate clinicamente o sconosciute e per monitorarne levoluzione nel tempo . 
una tecnica rigorosa e un giusto numero dinformazioni cliniche pertinenti consentono cos di valutare i volumi ematici circolanti , la distribuzione del usso , le anormalit pleuriche e del parenchima polmonare , lo stato del mediastino e del cuore . 
5 analisi degli addensamenti polmonari , versamenti pleurici , pneumotoraci in base al fatto che siano stati riscontrati al momento del ricovero o in seguito durante il ricovero . ten sufcient evidence to support treatment decisions , reveal clinically suspected or unknown abnormalities and monitor their evolution over time . 
a scrupulous technique and adequate number of relevant clinical data allow assessment of circulating blood volume , ow distribution , pleural and pulmonary abnormalities and state of the mediastinum and heart . 
patient transport within the hospital is often laborious and not free from potential complications ( displacement of drainage tubes and / or other mechanical devices ) , and correct orthogonal positioning is difcult . in the light of the above , cxr should be preferably performed only when clinically indicated , as this could help limit both costs and operator and patient radiation exposure . 
diversi studi hanno valutato la rilevanza clinica delluso del radiogramma del torace di routine versus quello on demand ( secondo indicazione clinica ) : in un ampio studio prospettico di graat et al . 
 [ 12 ] si visto che il 5 , 8% dei radiogrammi del torace di routine hanno mostrato nuovi o inaspettati reperti , ma solo il 2 , 2% ha portato a modicazioni della terapia ; un ulteriore studio di controllo randomizzato di krivopal et al . 
6 efcacia diagnostica dellrx torace per singolo gruppo di pazienti straticati in base al motivo di ricovero . % diagnostic efcacy several studies have investigated the clinical value of routine versus on - demand cxr ( based on clinical indication ) : a large prospective study by graat et al . 
 [ 12 ] demonstrated that 5.8% of routine cxr showed new or unexpected ndings , but only 2.2% resulted in changes in therapy ; a randomised controlled study conducted by krivopal et al . 
 a prospective observational study analysing 1 , 780 routine cxr in 559 icu patients [ 14 ] concluded that the diagnostic and therapeutic value of routine cxr was limited , leading the authors to recommend abandoning this practice in the icu . 
at the same time , the american college of radiology appropriateness criteria recommend daily cxr in patients with acute cardiopulmonary disease and in mechanically ventilated patients [ 15 ]  . our experience shows that the number of cxr obtained in the group of critically ill patients was indeed very high , especially in some subgroups , such as transplant patients , who routinely undergo daily cxr examination . 
on the other hand , given the high de in this group , this practice seems to be justied by the clinical condition and the possibly rapid progression of complications and cardiovascular instability of these patients . 
 in conclusion , despite practical difculties and technical problems often related to the patients condition , bedside cxr remains the most accessible and commonly used imaging modality in the icu , as it provides constant patient monitoring and a high de . 
as a result , the radiologist should maintain familiarity with the interpretation of cxr , radiogrammi con risultati signicativi ( che richiedevano quindi un intervento ) nel gruppo di pazienti che ricevevano rx torace su indicazione clinica ( 26 , 5% ) rispetto quelli del gruppo in cui il radiogramma del torace veniva fatto di routine ( 13 , 3% )  . 
 un recente studio osservazionale prospettico che ha analizzato 1780 rx torace di routine in 559 ricoveri ospedalieri in terapia intensiva [ 14 ] ha concluso che il valore diagnostico e terapeutico del radiogramma del torace di routine basso , e gli autori raccomandano quindi di abbandonare tale pratica in terapia intensiva . 
allo stesso tempo i criteri dappropriatezza dellamerican college of radiologist raccomandano lesecuzione giornaliera del radiogramma del torace in pazienti con problemi cardio - polmonari acuti ed in pazienti sottoposti a ventilazione meccanica [ 15 ]  . la nostra esperienza dimostra che il numero rx torace eseguiti nel gruppo di pazienti critici osservato obbiettivamente molto elevato , soprattutto in determinate categorie di pazienti , come i trapiantati , che vengono sottoposti di routine ad un radiogramma del torace al giorno ; tale modus operandi appare peraltro , data la comunque elevata ed in questa classe di pazienti , giusticato dalla situazione clinica e dalla possibile rapida evolutivit delle complicanze e mutabilit dello status cardiocircolatorio di tali pazienti . 
 possiamo concludere quindi affermando che il radiogramma del torace a letto , nonostante le difcolt pratiche per la sua esecuzione e le imprecisioni tecniche , spesso legate alle condizioni del paziente , rimane la metodica pi accessibile ed utilizzata in reparti di terapia intensiva , poich permette un monitoraggio costante del paziente con , allo stesso tempo , un elevata ed . 
brittenden and tolan , the reader will understand why this book was conceived and consequently written by the contributors ( heavily involved in this problem ) who report on expertise gained over the years in their dedicated departments . post surgical abdominal radiology is not a simple subject , due sometimes to poor information provided by the surgeons about the performed procedure / s and its / their endresults , as well as little knowledge on the part of the radiologist concerning the complexity of abdominal anatomical surgical changes . questions abound about post surgical bowel anatomy and functions , possible anatomical leaks , and severe complications very often present in old and frail patients which are difcult to correctly evaluate . 
which radiological modality is best ? plain x - ray lm ? contrast examination by barium or water - soluble contrast media ? us ? ct ? mri ? each modality offers pros and cons in their performance thus the radiologist must face the question : how can he / she properly and correctly report the obtained images without being exposed to surgeons blame ? the aim of this book is to give the reader a thorough answer to all the above questions , aided by radiological images coupled with and made easier to understand by many anatomical drawings of the performed surgical procedure / s . 
 these drawings are a strong - point of the book : once they have been understood and digested the related radiological images will be more easily understood . the content of the book is divided into 9 parts : introduction to the post surgical abdomen ; the esophagus ; the stomach and duodenum ; the pancreas ; the biliary tree ; the liver ; the small bowel ; the colon ; genitourinary system , all enriched by a very precise index . 
 nellintroduzione da parte del halligan e nella prefazione da parte dei curatori del volume , i dottori brittenden e tolan , il lettore si render conto del perch questo volume stato concepito e conseguentemente scritto dai vari collaboratori ( ampiamente coinvolti in questo problema ) , che descrivono lesperienza guadagnata nel corso degli anni nei loro specici reparti . la radiologia delladdome post - chirurgico non un argomento semplice , in parte , talvolta , a causa dei pochi dati forniti dai chirurghi sullintervento / i eseguito / i e sul risultato nale , e , in parte per la poca dimestichezza da parte del radiologo riguardo alla complessit delle modiche anatomiche post - chirurgiche delladdome . 
 molte e numerose sono le domande circa lanatomia e la funzionalit post - chirurgica delle anse intestinali , le possibili perdite / deiscenze e le importanti complicanze che sono spesso presenti nei pazienti anziani e deboli che sono anche difcili da studiare . 
cos meglio eseguire da un punto di vista radiologico ? esami diretti delladdome ? indagini con mezzi di contrasto , impiegando il bario o mezzi di contrasto idrosolubili ? ecograa ? tac ? rm ? ciascuna di queste modalit possiede pro e contro alla sua esecuzione , cosicch il radiologo si trova ad affrontare la seguente domanda : come refertare in modo corretto ed adeguato le immagini ottenute , senza incorrere in rimbrotti da parte del chirurgo ? scopo del volume di fornire al lettore una risposta adeguata a tutte le domande di cui sopra , aiutato da immagini radiologiche associate , rese di pi facile comprensione , da un numero notevole di disegni anatomici delle procedure chirurgiche eseguite . 
 il contenuto del volume diviso in 9 parti : introduzione alladdome post - chirugico ; lesofago ; lo stomaco ed il duodeno ; il pancreas ; il sistema biliare ; il fegato ; il piccolo intestino ; il colon , il sistema genito - urinario , il tutto arricchito da un indice molto preciso . ciascun capitolo arricchito da immagini molto precise radiol med ( 2013 ) 118 : 896897 each chapter is enriched by very precise , well reproduced images , explanations about the surgical technique / s employed ( sometimes too detailed for the overworked radiologist ) and an updated reference list . 
one will also nd a list of abbreviations , unfortunately not reporting all those to be found throughout the text . quite an impressive book to be recommended to surgeons ( to familiarize them with the radiological images , with the hope that they will be more thorough and precise about the performed intervention when lling in request forms for their patients ) and to radiologists ( who have to answer surgeons requests in the best and most precise way ) a book to be kept at hand and used in the daily routine in any department . 
 e ben riprodotte ; spiegazioni circa la / e tecnica / che chirurgiche impiegate ( talvolta troppo dettagliate per un radiologo molto impegnato nel lavoro ) e da un elenco bibliograco aggiornato . 
il lettore trover anche un elenco di abbreviazioni , purtroppo non completo rispetto a tutte quelle rintracciabili nel testo . un volume piuttosto importante , da raccomandare ai chirurghi ( per familiarizzarli con le immagini radiologiche , in modo che gli stessi possano essere pi accurati e precisi in merito allintervento eseguito , nel momento della compilazione delle richieste per i loro pazienti ) ed ai radiologi ( che debbono rispondere ai quesiti del chirurgo nel modo migliore e pi preciso ) , un volume da avere a disposizione e da utilizzare in ogni reparto radiologico nello svolgimento della pratica quotidiana . 
this study was undertaken to analyse the clinical characteristics and computed tomography ( ct ) imaging features of patients with pancreatic acinar cell carcinoma and to clarify characteristic imaging features . 
clinical and ct imaging records of ten patients with pancreatic acinar cell carcinoma ( three women and seven men ; mean age , 58 years ) examined using multidetector ct scanners were retrospectively studied . 
seven tumours appeared as enhanced solid pancreatic masses , with the large masses having hypodense areas ; three had > 75 % cystic component ; seven ( 70% ) , including four solid and three cystic masses , had wellcircumscribed or partially well - dened thin , enhanced encapsulation . 
lo scopo di questo studio stato quello di analizzare le caratteristiche cliniche e di imaging tc dei pazienti con carcinoma a cellule acinari del pancreas e di chiarire le caratteristiche imaging del carcinoma a cellule acinari . 
sono stati retrospettivamente esaminate gli aspetti clinici e di imaging tc di 10 pazienti con diagnosi di carcinoma a cellule acinari del pancreas ( tre femmine e sette maschi , et media 58 anni ) sottoposti ad esame tc multidetettore . 
sette tumori sono risultate lesioni solide del pancreas , con aree ipodense contestuali ; tre presentavano componenti cistica superiore al 75% ; sette tumori ( 70% ) , di cui quattro solidi e tre con componente cistica , presentavano pareti sottili ben circoscritte o pazialmente sottile , vascolarizzata . 
la diagnosi di carcinoma a cellule acinari dovrebbe essere presa in considerazione nel caso di lesioni pancreatiche solide di grandi dimensioni con caratteristiche imaging tipiche e presenza di aree centrali cistiche di dimensioni variabili . parole chiave tc carcinoma a cellule acinari pancreas massa cistica noduli murali 724 introduction acinar cell carcinoma ( acc ) is a rare neoplasm of the pancreas originating from acinar elements of the exocrine pancreas , accounting for approximately 1 % of nonendocrine tumours [ 1 , 2 ]  . 
given its rarity , the clinical and imaging appearance , treatment and outcome of this disease have not been fully investigated ; case reports , multicentre studies , small - scale studies and relatively limited literature reviews represent the available literature on this disease [ 37 ]  . 
thus , imaging features and clinical characteristics of ten patients with acc , including both solid and cystic masses veried by surgery and pathology , are delineated and discussed to help radiologists become more procient with recognising acc and thus providing more accurate diagnosis . materials and methods clinical data the protocol for this study was approved by the institutional review board of our institution , and informed consent for this retrospective study was acquired from the patients . 
after their operations , patients were assessed clinically and with ultrasonography ( us ) , as well as with multidetector computed tomography ( mdct ) on follow - up , which ranged from 2 to 58 ( mean , 30 ) months . 
all patients were administered 500800 ml of water 30 min prior to ct scan and an additional 250300 ml immediately prior to the study to achieve adequate gastric and duodenal distension . 
a total of 80130 ml of nonionic iodinated contrast material ( omnipaque 300 mg i / ml , ge healthcare ) was injected intravenously at a rate of 2.53.5 ml / s with a power injector ( ulrich medical , gerradiol med ( 2013 ) 118 : 723731 many ) through an 18 - gauge intravenous catheter inserted into the antecubital vethe volume of contrast material delivered was 1.52 ml / kg body weight . 
three patients underwent dual - phase ct scans during the unenhanced , pancreatic and hepatic venous phases , whereas the other seven underwent triple - phase ct during the same phases . 
imaging features comprised : location ( head , neck , body , tail ) ; size ; shape ; margin and enhanced capsule ; fraction composed of solid versus cystic material ( greater or less than 50 % solid ) ; internal attenuation characteristics on enhanced arterial and pancreatic phase images compared with surrounding pancreatic tissue ( hypoattenuation , isoattenuation or hyperattenuation ) ; enhancement pattern ( peripheral , complete , mural nodule ) ; calcication ( present or absent ) ; biliary and pancreatic ductal dilatation . 
haematoxylin and eosin ( h&e ) staining was performed , and macroscopic appearances of each resected segment were analysed with photomacrographs ; analysis comprised location , size , shape and edge . radiol med ( 2013 ) 118 : 723731 results clinical analysis patients comprised seven men and three women with a mean age of 58 ( range , 3871 ) years . 
in three patients ( 3 / 10 ) , masses were found incidentally at routine physical examination , one of whom showed an abdominal mass at the beginning of the physical examination . 
 serum carbohydrate antigen ( ca ) 19 - 9 was increased in four patients , with levels four to six times the normal level , whereas alpha - fetoprotein ( afp ) was increased mildly in one patient . 
median survival time was 35 ( 570 ) months ; two patients died from disease recurrence during follow - up . image analysis table 2 summarises ct features with respect to lesion location , size , shape , margin and encapsulation , composition , calcication and enhancement pattern . 
all six solid tumours and the small solid or mural nodules in the three cystic lesions appeared with a progressively lled - in enhanced pattern during dual - phase scans ; however , enhancement in tumours was less than that of adjacent normal pancreatic parenchyma . 
a la tomograa computerizzata ( tc ) in fase precontrastograca mostra una massa ipodensa nella testa del pancreas , b le immagini post - contrastograche mostrano una sottile capsula vascolarizzata ( freccia ) ; c la ricostruzione coronale mostra chiaramente la capsula vascolarizzata . 
d a basso ingrandimento ( ingrandimento originale 100 ) , apprezzabile la struttura acinare del tumore con le cellule neoplastiche disposte in piccole unit ghiandolari ; e a maggior ingrandimento ( ingrandimento originale 200 ) , apprezzabile labbondante citoplasma eosinolo rosa con granuli . 
the bile duct , including the intrahepatic bile duct , ductus choledochus and pancreatic duct , were dilated in one lesion , located in the uncinate of the pancreatic head . 
a la tc in fase precontrastograca mostra una massa di circa 4 , 5 cm4 , 1 cm di diametro nella coda del pancreas con componenti cistiche con piccoli noduli solidi parietali . 
b allesame tc in fase precontrastograca non si evidenzia enhancement a carico della zona necrotica cistica , mentre la sottile parete cistica ( freccia nera ) e i noduli parietali ( freccia bianca ) appaiono vascolarizzati . radiol med ( 2013 ) 118 : 723731 fig . 
b in the portal phase , the tumour was continuously enhanced , becoming isodense in the portal venous phase ; many small lymph node metastases were found around the lesion . 
la lesione invade la milza e la sua origine risulta difcile da riconoscere . brous bands separate tumour cells into lobules ; the tumour is encapsulated and highly cellular with stroma under light microscope ( fig.1 d , e )  . discussion pancreatic ductal adenocarcinoma ( dac ) is the most common pancreatic neoplasm , comprising > 90 % of all pancreatic neoplasms . 
it is dened as a carcinoma that exhibits pancreatic enzyme production by neoplastic exocrine cells , and its clinical presentation is usually related to either the local effects of the tumour or to metastases [ 8 ]  . 
acc has nonspecic clinical symptoms , with 55% of patients presenting abdominal pain , weight loss , nausea and vomiting , and some patients with a palpable abdominal mass [ 13 ]  . 
the clinical presentation is generally nonspecic , but in 16 % of cases , systemic manifestations related to the liberation of lipase , such as panniculitis and polyarthralgia , may occur [ 15 , 16 ]  . 
no patient in our study had the corresponding systemic symptoms . a recent study provided evidence of male predominance in acc patients and a mean age of 59.6 years , which is consistent with our results , which found seven of the ten fig . 
histopathologically , a pure acc has two predominant patterns of growth : an acinar pattern , consisting of cells growing in well - formed acini ; and a solid pattern , characterised by sheets and cords of cells in a brovascular stroma . 
the microscopic appearance of acc is distinctive : acinar structures are the hallmark of this neoplasm ; thick , 730 radiol med ( 2013 ) 118 : 723731 patients were men , with an average age of 58 years . 
seven tumours ( 70% ) either had well - circumscribed , thin enhanced capsules ( n = 5 ) or were partially encapsulated ( n = 2 ) on ct imaging . 
 in our study , radiological manifestations of acc were clearly claried as a large , solid mass with a varying proportion of cystic components , which represented necrosis and haemorrhage . 
 in a previous study of ours , cystic degeneration occurred in small tumours ( up to 2.5 cm in diameter ) , which is inconsistent with results of this study . 
in contrast , the average diameter of dac is 23 cm [ 20 ]  . considering the intraductal epithelial origin of dac , pancreatic duct obstruction is usually present , even with small tumours ; hence , dual - duct symptoms are used as specic features to diagnose dac . 
dac could also be differentiated from acc by indirect signs , such as atrophic distal parenchyma , interrupted duct sign , inltration of the peripheral nerve and encasement of an artery and / or vein [ 21 ]  . the majority of authors describe acc as a hypovascular mass on ct , typically heterogeneously enhanced , but less so than the surrounding pancreatic parenchyma [ 6 , 7 ]  . 
 however , some authors report hypervascular acc in the pancreatic phase that then become isodense in the portal venous phase ; tumours that present this enhancement pattern may mimic a neuroendocrine neoplasm [ 22 , 23 ]  . 
 when acc is considered as a diagnosis , solid masses with cystic necrosis should be differentiated from solid pseudopapillary tumours ( spts ) of the pancreas , which easily produce intratumoural haemorrhage . 
cystic acc lesions could sometimes be misdiagnosed as mucinous cystadenomas of the pancreas , which occurs predominantly in perimenopausal women ( average age at presentation , 47 years ) [ 24 ]  . 
the mucinous cyst content also aids in the differential diagnosis . in conclusion , ct imaging may be a useful tool for diagnosing pancreatic acc based on the following characteristics : larger size ; solid or cystic masses with well - circumscribed , thin , enhanced encapsulation and hypovascular mass on ct ; solid masses with hypodense area in large masses ; cystic lesions with mural nodules or a small solid component ; enhancement in the cystic wall ; mural nodules ; and solid component . acknowledgements hu shengping was supported by shanghai science and technology committee . 
favrel1 1service de radiothrapie oncologie , centre hospitalier lyon - sud , chemin du grand - revoyet , 69495 pierre benite cedex ( france ) and ea 3738 2istituto del radio o . 
craniocaudal ( cc ) , anteroposterior ( ap ) and laterolateral ( ll ) displacements were measured during the rst 3 days of treatment and then weekly by comparing two orthogonal images obtained by an electronic system of portal imaging with digitally reconstructed radiographs ( drrs )  . 
setup margins ( sm ) were dened according to the international commission on radiation units ( icru ) - 62 formula , the stroom equation and the van herk equation . 
gli spostamenti cranio - caudali ( cc ) , antero - posteriori ( ap ) e latero - laterali ( ll ) sono stati misurati durante i primi 3 giorni di trattamento e poi settimanalmente comparando due immagini ortogonali ottenute da un sistema elettronico di portal imaging e le digitally reconstructed radiographs ( drrs )  . 
 lerrore sistematico ( ) e random ( ) della popolazione sono stati calcolati rispettivamente come deviazione standard della media della popolazione e come media delle deviazioni standard per ogni paziente . 
la imrt una tecnica di trattamento altamente sosticata che necessita di una denizione 864 radiol med ( 2013 ) 118 : 863869 keywords pituitary adenomas radiotherapy imrt setup margins igrt precisa ed ottimizzata degli errori di setup locali e , quindi , dei volumi da irradiare . 
 parole chiave adenomi iposiari radioterapia imrt margini di setup igrt introduction pituitary adenomas are classied as benign intracranial tumours and constitute 10% of all tumours in the adult population [ 1 ]  . 
they are asymptomatic in the majority of the cases , but might have a signicant impact on health in the late course of the disease , either because of clinical syndromes due to hormonal imbalance and / or because of the local mass effect on the surrounding structures [ 2 ]  . 
in the last two decades , many noninvasive or minimally invasive procedures have been developed for treating pituitary adenomas , including microsurgery , stereotactic radiosurgery ( srs ) , hormonal therapy and fractionated external - beam radiation [ 3d - conformal radiotherapy ( crt ) ] [ 24 ]  . 
throughout this period , many techniques have been described in the literature for conventional fractionated rt : two opposed lateral beams , a three - eld technique adding a coronal eld , moving - arc elds , 360 rotational elds , and 3d - crt [ 6 ]  . 
considering the benign nature of this disease , its good prognosis and potential curability , the dose delivered and the denition of planned target volume ( ptv ) must be carefully and precisely identied to spare organs at risk ( oars ) in this territory , namely , optic nerves and the optic chiasma . 
 as has been shown in treating tumours of other anatomical sites , imrt can obtain better dose distribution , avoiding critical structures and decreasing morbidity without compromising , and even improving , local control [ 810 ]  . 
considering the highly conformed dose distribution of imrt , while preserving critical structures in proximity or even in contact with the target volume , dening margins in these kinds of treatment is crucial to avoid geographic omission because of their potential impact on local control . 
whereas analysis of setup errors is already published for other tumour sites [ 11 , 12 ] , including brain tumours [ 13 ] , data about this issue in treating pituitary adenomas are lacking in the literature . 
we present a retrospective analysis of imrt setup errors in patients treated for pituitary adenomas . patients and methods a retrospective analysis of patients treated with imrt for a pituitary adenoma from january 2009 was conducted . 
the aim was to evaluate setup uncertainties in order to dene optimal margin around the gross tumour volume ( gtv ) , or clinical target volume ( ctv ) if the tumour was completely removed before rt , in order to obtain the ptv . 
following our internal protocols , ptv was dened as ctv + isotropic margin of 3 mtotal dose of rt was 54 gy ( 2 - gy / daily fractions )  . 
radiation therapy ( rt ) was radiol med ( 2013 ) 118 : 863869 delivered by a linear accelerator ( varian accelerator clinac 2100 c / d ) equipped with a mini - multileaf collimator ( mmlc , 120 leaves )  . setup verication the isocentre was chosen and placed following the indications of the international commission on radiation units and measurements ( icru ) reports no . 
 verication of the isocenter position was performed by a 2d2d comparison of two orthogonal portal images ( 0 and 90 ) by manual realignment , which was then retrieved by an electronic system of portal imaging ( varian portal vision ) to be nally compared with the digitally reconstructed radiographs ( drrs ) obtained from the simulation ct scans . 
 denition of displacement craniocaudal ( cc ) , anteroposterior ( ap ) and laterolateral ( ll ) displacements between drr isocentre and portal imaging isocentre were measured and analysed twice by two different radiation oncologists . 
8.6 ( varian medical system )  . statistical evaluation of setup margins differences between planned irradiation geometry during a treatment session may be systematic or randoif the mean irradiation geometry in the fractionated treatment differs from the geometry in the treatment plan , a systematic error occurs . 
as described by stroom and heijmen : for systematic uncertainties , such a population standard deviation ( often denoted by ) indicates the patient - to - patient variation in the systematic deviation from the planning situation . 
finally , geometric uncertainties of a specic patient group can normally be characterized by the sd of the distribution of systematic deviations in the patient group ( ) and by the average sd of the distribution of random deviations ( ) [ 17 , 18 ]  . 
the resultant values were incorporated into the formulas proposed by the icru [ 14 ] , by stroom and heijmen [ 16 ] and by van herk [ 19 ] , in order to derive ctv - to - ptv margins in the ll , cc and ap planes . 
statistical analyses were performed using the medcalc software ( medcalc version 9.2.0.1 , medcalc software , belgium )  . results patients from january 2009 to april 2010 , 20 patients were treated with imrt for pituitary adenomas . 
table 2 summarises systematic and random errors and setup margins ( in millimetres ) calculated by the icru - 62 method , by strooms formula and by van herks formula ; table 1 describes data for every patient . discussion radiation therapy has a well - established role in the multidisciplinary treatment of pituitary adenomas [ 20 ]  . 
the denition of target volumes has a major role in the workload of radiation oncologists and should take into account clinical and / or radiological criteria , natural history of the tumour and also errors that could be related to physiological movement of organs and / or disease and setup errors [ 19 ]  . 
positive values correspond to anterior , caudal and right error direction in the ap , cc and ll direction , respectively tabella 1 caratteristiche dei pazienti ed errori di setup : valori positivi corrispondono ad una variazione in direzione anteriore , caudale e a destra rispettivamente nella direzione ap , si and rl patient no . 
moreover , to ensure that the evolution towards a programme of frameless igrt for treating pituitary adenomas initiated in our department would perform within a framework of quality assurance , we decided also to verify the margins used in our daily practice ( 3 mm ) before using them in the new context . the problem of correct setup is a challenge in this kind of patient , particularly considering that pituitary adenomas are benign diseases , and so the risk of late side effects of rt , such as secondary tumours , should be taken into account . 
 moreover , if modern irradiation techniques , such as imrt , volumetric arc rt and proton - beam therapy ( pbt ) allow highly shaped dose distributions with a rapid fall - off of dose out of the ptv , the correct denition of margins and treatment volumes is crucial . 
 radiol med ( 2013 ) 118 : 863869 if organ motion has a minimal impact in intracranial tumour treatment , the problem of patient setup has been extensively studied in this kind of disease due to the presence of critical intracranial structures and / or functional pathways [ 13 , 21 , 22 ]  . 
looking at the available literature on setup margins in rt for brain tumours , our results do not signicantly differ from published reports about setup verication by electronic portal imaging . 
as holds true for all studies approaching the problem of setup margins in rt , this analysis is interesting but has only local value and should be done in all rt centres treating this type of patient . in our experience , we interestingly found a more important setup error in the cc direction , which means that probably the chiasma could receive an increased dose compared with the dose that we accepted on the basis of dose distributions and dose - volume histograms . 
considering the level of dose that we deliver in our daily practice ( 54 gy ) , this might not be a problem : in fact , a recent study stated that the maximal acceptable dose could be 55 gy [ 26 ]  . 
in any case , our department quite recently implemented the exactrac xray image - guidance system with 6 degrees of freedom and a cone - beam ct systealso on the basis of data presented in this article , analysis of the impact of these new techniques in our daily practice is now underway . 
 conversely , the problem should be considered in the context of srt or , more generally , of higher biological delivered doses , where the impact of random and systematic setup errors would be more important . 
moreover , it is accepted that for higher doses per fraction and / or in new methods of dose delivery ( imrt , srt , proton therapy... ) , the formula of biological equivalent dose ( bed ) might not be reliable , and its application in these contexts should therefore be carefully evaluated [ 27 ]  . 
it means that all modern techniques for setup control that could be based on bony references ( tomotherapy , cone - beam ct , exactrac ) , with the possibility of verication of the interand intra - fraction variability , can assure a setup error < 3 mwang et al . 
evaluated patient setup of an optically guided , kv image - based frameless system : in 87.5 % of patients in the study , treatments were completed under optical guidance with a maximum setup error of 2 mm and a median setup error of 0 m for the remaining 12.5% of patients , isodisplacements were > 2 mm , and treatment records showed that those patients were repositioned guided by the orthogonal kv images [ 30 ]  . 
reported that after a frame - guided setup , conebeam ct acquired before each fraction showed setup errors for biteblockand mask - based treatments smaller ( 2.91.3 mm ) than those for thermoplastic - mask - alone - based treatments ( 3.21.5 mm ) , but the difference was not signicant . 
our study also gave us the possibility of critically emphasising differences between the three proposed methods . as shown in table 2 , differences can be observed using different methods to calculate setup errors . 
in our opinion , this approach is not realistic , and the dosimetric study by stroom and heijmen [ 16 ] conrms our idea that an error that is repeated during all the treatment does not have the same dosimetric meaning as a random error . 
in fact , the nal result of systematic uncertainties is a relatively small volume that is largely underdosed , whereas random errors yield a larger volume that is only underdosed a little . 
so , in our opinion , as the icru - 62 formula does not take into account these situations , it is not well adapted to the aim of our study and , more generally , to the study of setup errors . conversely , the stroom formula correctly takes into account the different , greater , impact of systematic errors . 
 it should be noted that in their formula , rotational deviations 868 radiol med ( 2013 ) 118 : 863869 were included , so the resulting margins could be anisotropic . 
although the stroom formula appears to be suitable for clinical application , we prefer to use the van herk formula , which gives margins calculated analytically for a perfect sphere with a perfectly conformal dose distribution that is similar to those obtained with imrt . 
it should be noted that the results obtained with formulae are comparable and both methods are , in our opinion , suitable for use in clinical practice . conclusions imrt is a highly sophisticated treatment technique that requires precise denition and optimisation of the irradiated volumes . 
beomonte zobel department of radiology , campus bio - medico school of medicine , university of rome , via alvaro del portillo 200 , 00128 rome , italy correspondence to : r . 
this study was undertaken to assess the reliability of the posterior approach under ultrasonographic guidance ( pauga ) , with the arm abducted , before performing direct magnetic resonance ( mr ) arthrography of the shoulder . 
patients were enrolled because of glenohumeral instability ( n = 71 ) , chronic shoulder pain ( n = 25 ) , suspicion of rotator cuff tear ( n = 13 ) and adhesive capsulitis ( n = 2 )  . 
patients were placed in the lateral position , on the contralateral side to that being examined ; the arm of the shoulder undergoing the examination was placed in slight internal rotation with the hand under the contralateral armpit . 
for each patient , the number of injection attempts , room time , complications and pain , as recorded on a 10 - point visual analogue scale ( vas ) , were noted . 
i pazienti sono stati arruolati a causa di instabilit gleno - omerale ( n = 71 ) , dolore di spalla cronico ( n = 25 ) , sospetto di lesioni della cufa dei rotatori ( n = 13 ) e capsulite adesiva ( n = 2 )  . 
 i pazienti sono stati disposti in decubito clinostatico laterale , sul anco controlaterale rispetto a quello coinvolto nellesame ; il braccio della spalla esaminata stato posto in lieve rotazione interna , con la mano al di sotto dellascella controlaterale . 
 per ciascun paziente sono stati registrati i seguenti dati : numero di tentativi di puntura , tempo - sala necessario per liniezione , complicanze e dolore , valutato mediante una scala visuale analogica ( vas ) , con punteggio da 0 a 10 . 
quattordici radiol med ( 2013 ) 118 : 806815 the injection was successful at the rst attempt , whereas in the remaining nine cases ( 8% ) , needle repositioning without any additional puncture was required to obtain clear sonographic depiction of the position of the needle tip . 
pauga is a reliable and rapid technique that is well tolerated by patients and easy for the radiologist to perfor keywords shoulder direct mr arthrography shoulder us guidance pazienti ( 12 , 6% ) hanno mostrato una temporanea ed autolimitantesi difcolt nei movimenti dellarto interessato e tredici pazienti ( 11 , 7% ) hanno mostrato una reazione vagale che non ha richiesto il ricorso a farmaci . 
in 102 casi ( 92% ) liniezione stata eseguita con successo al primo tentativo , mentre nei restanti ( 8% ) casi , stato necessario eseguire un riposizionamento dellago senza necessit di punture addizionali , al ne di ottenere un chiaro riscontro ecograco della posizione della punta dellago . 
pauga una tecnica afdabile e veloce , ben tollerata dai pazienti e veloce da essere eseguita dal radiologo . parole chiave spalla rm artrograca diretta guida ecograca introduction introduzione assessing injuries affecting tendinous and brocartilaginous structures of the shoulder requires sophisticated diagnostic tools . 
direct mr arthrography was developed to overcome such problems and to provide a clear depiction of intra - articular structures with the aid of iatrogenic joint effusion ( arthrogram effect ) [ 1 ]  . 
direct mr arthrography involves the intra - articular injection of either normal saline or diluted paramagnetic contrast agent , with the latter being the method of choice in most institutions [ 1 ]  . 
 our objective was to assess the reliability of the posterior approach under us guidance ( pauga ) with the patients arm in the abduction position before performing direct mr arthrography of the shoulder in terms of number of injection attempts , room time , complications and pa la valutazione delle lesioni tendinee e bro - cartilaginee della spalla richiede strumenti diagnostici sosticati . 
la rm artrograca diretta stata sviluppata per superare tali problematiche e per investigare con chiarezza le strutture intra - articolari per mezzo della distensione articolare iatrogena ( effetto artrograco ) [ 1 ]  . 
la rm artrograca diretta richiede liniezione intra - articolare di soluzione salina o di una soluzione diluita di mezzo di contrasto paramagnetico , con la seconda preferita in molti istituti [ 1 ]  . 
al contrario , nella rm artrograca indiretta , liniezione di mezzo di contrasto viene eseguita per via endovenosa e si attende la sua successiva diffusione nello spazio articolare [ 2 ]  . sono stati descritti diversi approcci di somministrazione intra - articolare di mezzo di contrasto , sia sotto guida uoroscopica che ecograca . 
 il nostro obiettivo stato quello di valutare lafdabilit dellapproccio posteriore sotto guida ecograca e con arto in abduzione ( pauga ) prima dellesecuzione di una rm artrograca diretta della spalla , in termini di numero di materials and methods 808 patients between january 2008 and november 2010 , 111 consecutive patients ( 82 men , 29 women ; mean age , 24 years ) underwent direct mr arthrography of the shoulder under us control . 
inclusion criteria were : glenohumeral instability ( n = 71 ) , chronic shoulder pain ( n = 25 ) , suspicion of rotator cuff tear ( n = 13 ) and adhesive capsulitis ( n = 2 )  . 
a gadolinium - based solution was prepared by mixing 0.1ml gadolinium ( prohance ; bracco , milan , italy ) , 20 ml of saline , and 5 ml of 2% lidocaine [ 4 ]  . 
1 decubito del paziente mentre riceve liniezione della spalla : il paziente sdraiato sul anco opposto rispetto a quello coivolto nellesame ; il braccio della spalla in esame posizionato in lieve intra - rotazione , con la mano dello stesso lato posizionata al di sotto dellascella controlaterale . radiol med ( 2013 ) 118 : 806815 tentativi di puntura , tempo - sala necessario per liniezione , complicanze e dolore . materiali e metodi pazienti da gennaio 2008 a novembre 2010 , 111 pazienti ( 82 maschi , 29 femmine , et media 24 anni ) sono stati consecutivamente arruolati per essere sottoposti a rm artrograca diretta della spalla sotto guida ecograca . 
il gruppo dei pazienti stato composto come segue : instabilit gleno - omerale ( n = 71 ) , dolore di spalla cronico ( n = 25 ) , sospetta lesione della cufa dei rotatori ( n = 13 ) , capsulite adesiva ( n = 2 )  . 
i pazienti sono stati esclusi dallo studio in caso di frattura a carico delle componenti articolari della spalla , terapie anticoagulati o diatesi emorragiche , allergia o anamnesi positiva per allergia al mezzo di contrasto , infezione o inammazione articolare . 
una soluzione acquosa a base di gadolinio ( prohance , bracco , milano , italia ) stata preparata secondo la seguente diluizione : 0 , 1 ml di gadolinio addizionati a 20 ml di soluzione salina e a 5 ml di lidocaina al 2% [ 4 ]  . 
lago stato inserito con direzione latero - mediale , parallelamente allasse lungo della sonda ed avanzato nello spazio articolare , tra la testa omerale e la parte posteriore del labbro glenoideo . 
il mandrino dellago spinale da 22 gauge stato rimosso non appena ottenuto laccesso intra - articolare e quindi , lago connesso ad una siringa contente la soluzione a base di gadolinio . 
per ottenere unottimale distribuzione del mezzo di contrasto nello spazio intra - articolare , stato sempre ottenuto un controllo della posizione della punta dellago a forma di becco di auto , prima della somministrazione . 
2a posizione della punta dellago vericata sotto guida ecograca ; b controllo ecograco mediante color - doppler eseguito per escludere eventuali sanguinamenti dopo la puntura . anaesthesia was obtained before each injection . 
 the 22 - gauge spinal needle stylet was removed as soon as the access was gained , and the needle was subsequently connected to a syringe containing the gadolinium - based solution . 
le immagini sono state ottenute su piani di scansione assiali , coronali e sagittali ; le immagini sono state ottenute anche in posizione di abduzione e rotazione esterna [ 5 ]  . 
le immagini sono state valutate da un radiologo con 10 anni di esperienza nellambito della radiologia muscolo - scheletrica . imaging technique dati all mr examinations were performed with a 1.5 - t unit ( magnetom symphony ; siemens medical solutions , germany )  . 
t1 - weighted fat suppressed sequences were acquired ( repetition time ms / echo time ms , 440 / 9 ; two signals acquired ; eld of view , 16 cm ; imaging matrix , 256160 ; section thickness , 4 mm ; no intersection gap )  . 
 data collection for each patient , the following parameters were recorded : number of attempts needed to ll the joint space with contrast medium solution , room time ( time elapsing from the moment the patient entered the room to receive the injection and the moment the patient left the room to go to the mr unit ) , complications such as burning sensation , altered or reduced sensitivity , movement compromise , early fatigue , vagal reaction or bleeding at the puncture site . 
finally , pain intensity was recorded on a 10 - point visual analogue scale ( vas ) , where 0 indicates no pain and 10 indicates the worst possible pain . statistical analysis for quantitative parameters ( room time , pain intensity ) , usual parameters were calculated as mean and standard deviation ( sd )  . results direct mr arthrography examinations were performed successfully in all patients , and no major immediate or late complications were observed . 
inne , lintesit del dolore avvertito dal paziente stata valutata mediante il ricorso alla scala analogico visuale ( vas ) , con punteggi da 0 a 10 : 0 signicava assenza di dolore e 10 il peggior dolore mai avvertito . per i parametri quantitativi ( tempo - sala ed intensit dolorica ) sono stati calcolati media e deviazione standard ( ds )  . analisi statistica risultati le rm artrograche dirette sono state eseguite con successo in tutti i casi , e non si sono registrate complicanze maggiori immediate o tardive . 
in 102 casi ( 92% ) liniezione stata di successo al primo tentativo , mentre nei restanti nove casi ( 8% ) stato necessario eseguire un riposizionamento dellago senza necessit di una seconda puntura , al ne di valutare ecogracamente lesatta posizione della punta della ago . 
3a , b immagine di rm artrograca diretta t1 - pesata ottenuta sul piano di scansione assiale ; si noti la lassit dei legamenti gleno - omerale ( a ) medio ed ( b ) inferiore ( rispettivamente , freccia lineare e curva )  . 
5a , b immagine di rm artrograca diretta t1 - pesata ottenuta sul piano di scansione coronale ; si noti linpingment cronico del tendine sovraspinoso ( freccia lineare ) ( a ) ; il tendine del capo lungo del bicipite appare normale nel medesimo paziente ( freccia curva ) ( b )  . was successful at the rst attempt , whereas in the remaining nine cases ( 8% ) , needle repositioning without a second puncture was necessary to obtain a clear sonographic assessment of the position of the needle tip . 
indicazioni allesecuzione di tale metodica sono : instabilit gleno - omerale dovuta a lesioni del complesso labro - legamentoso , rico812 table 1 results observed in our study cohort attempts , n ( % ) successful at rst attempt required needle repositioning without additional puncture mean room time ( min ) observed complications , n ( % ) temporary compromise of movements self - limiting vagal reaction pain ( vas scale ) vas , visual analogic scale tabella 1 risultati osservati nella popolazione in studio numero di tentativi di puntura , n ( % ) successo la primo tentativo necessario riposizionamento dellago senza puntura addizionale tempo - sala medio ( min ) complicanze osservate , n ( % ) compromissione temporanea nei movimenti reazione vagale autolimitantesi dolore ( vas ) vas , scala visuale analogica within the infraspinatus occurred . 
indications are glenohumeral instability due to lesions to the labral - ligamentous complex , failed surgical capsular reconstruction [ 1 ] and suspected partial - thickness rotator cuff tears [ 2 ]  . 
 this safe and relatively easy technique signicantly enhances the changes of diagnosing intra - articular and rotator cuff disorders because it allows capsular distension and separation of intra - articular structures [ 6 ]  . 
in addition , intracapsular contrast medium administration is an excellent method for achieving optimal contrast resolution , thus making direct mr arthrography far more effective than conventional mr imaging in the evaluation of glenohumeral joint disorders . 
however , factors inuencing the preference of direct mr arthrography rather than conventional mr imaging seem to be the presence of an experienced radiologist performing and interpreting the images and the orthopaedic surgeons and radiologists belief that the use of direct mr arthrography can effectively alter patient management [ 1 ]  . several different approaches and techniques have been described for administering the contrast medium into the joint space . 
tale metodica appare sicura e relativamente semplice da eseguire , aumentando la probabilit diagnostica di disordini intra - articolari o legati ad alterazioni delle strutture della cufa dei rotatori , grazie alla possibilit di separare le strutture intra - articolari [ 6 ]  . 
 inoltre , liniziezione intra - capsulare un eccelente metodo per ottenere unottimale risoluzione di contrasto , rendendo , pertanto , la rm artrograca diretta molto pi performante da un punto di vista diagnostico rispetto alla rm convenzionale , nella diagnostica gleno - omerale . 
tuttavia , i fattori che sembrano far preferire la rm artrograca diretta rispetto alla rm convenzionale , sono la disponibilit di radiologi esperti , capaci di eseguire e refertare lesame e soprattutto la ferma convinzione sia del radiologo che dellortopedico che il ricorso a tale metodica possa effettivamente cambiare in senso positivo la gestione clinica del caso [ 1 ]  . diversi approcci e tecniche sono stati descritti per ottenere la somministrazione intra - articolare di mezzo di contrasto . 
pertanto , lapproccio dovrebbe essere scelto in base alla sospetta lesione sottostante ( per esempio , pazienti con sospetta instabilit anteriore dovrebbero ricevere lapproccio posteriore e pazienti con sospetta instabilit posteriore dovrebbero ricevere lapproccio anteriore )  . 
 radiol med ( 2013 ) 118 : 806815 the anterior approach raises concerns due to the possible distortion of healthy anatomical structures as the needle traverses the anterior stabilising complex of the glenohumeral joint [ 6 ]  . 
 [ 4 ] that the posterior approach should be preferred , as it does not interfere with the delicate glenohumeral stabilising structures , such as the anterior band of the inferior glenohumeral ligament and the anteroinferior portion of the labru in addition , as most of the direct mr arthrograms are performed for suspected anterior instability far more frequent than the posterior form the anterior approach could affect diagnostic performance . 
in this perspective , we agree with koivikko and mustonen [ 7 ] , who considered the posterior approach to be superior because if leakage occurs into and through the infraspinatus muscle , artefacts are easier to recognise . 
even though the posterior approach has been related to vasovagal collapse [ 7 ] , in our experience , we solved the problem by having the patient lie on the contralateral side . with regard to the technique , in 1975 , schneider et al . 
this method is still widely used , although many others have been described [ 9 , 10 ] ; however , the approach under us guidance is less time consuming and does not require ionising radiation [ 6 ]  . in our institution , a posterior approach under us guidance has always been applied because of the aforementioned advantages and the possibility of avoiding radiation exposure and saving resources related to the use of the angiographic suite ( especially costs connected to devices and staff )  . 
in our experience , the us - guided approach represents an excellent technique because it is fast ( estimated room time of 7.21.4 min , 92% of injections successful at the rst attempt )  . 
this happened because the needle tip bevel was angled against the humeral head ; as a result , repositioning of the needle meant slightly withdrawing the needle and rotating the tip to avoid contact with the humeral head and facilitate administration of intracapsular contrast mediuin our opinion , this manoeuvre should not be consebbene la proposta di chung et al . 
 [ 4 ] , secondo cui sarebbe opportuno ricorrere allapproccio posteriore per preservare le delicate strutture stabilizzati anteriori , come la banda anteriore del legamento gleno - omerale inferiore e la porzione antero - inferiore del labbro glenoideo . inoltre , poich , la gran parte delle rm artrograche dirette sono eseguite per sospetta instabilit anteriore , di gran lunga pi frequente rispetto alla posteriore , il ricorso allapproccio anteriore potrebbe alterare la performance diagnostica . 
 [ 7 ] , i quali considerano superiore lapproccio posteriore rispetto allanteriore poich in caso di stravaso di mezzo di contrasto nel contesto delle strutture del muscolo infra - spinato , gli artefatti che ne deriverebbero sarebbero morofologicamente pi facilmente riconoscibili . 
ancora , sebbene lapproccio posteriore sia stato correlato ad una maggiore incidenza di reazioni vagali [ 7 ] , nella nostra esperienza , tale problematica stata risolta ricorrendo al decubito clinostatico del paziente , sul anco opposto rispetto a quello coinvolto nello studio . 
tale metodica ancora ampiamente utilizzata , sebbene molte altre sono state descritte [ 9 , 10 ] ; tuttavia , lapproccio ecograco si dimostrato essere meno dispendioso rispetto al uoroscopico in termini di tempo , senza ricorso a radiazioni ionizzanti [ 6 ]  . nel nostro istituto , lapproccio posteriore sotto guida ecograca stato sempre applicato per via dei suddetti vantaggi , per la possibilit di non irradiare il paziente e per il risparmio delle risorse collegate allimpiego della sala angiograca ( soprattutto costi legati ai materiali ed allo staff )  . 
 nella nostra esperienza , lapproccio ecograco rappresenta una tecnica eccelente poich rapida ( tempo - sala stimato 7 , 21 , 4 min , 92% di inieizioni eseguite con successo al primo tentativo )  . 
nel nostro studio , l8% dei casi ha necessitato di un riposizionamento dellago senza punture addizionali ; ci accaduto perch la punta dellago a forma di becco di auto era inclinata contro la testa omerale ; di conseguenza , il riposizionamento dellago altro non stato se non un minimo indietreggiamento dellago associato ad un piccolo movimento di rotazione della punta dello stesso , cos da evitare il contatto con la testa omerale e permettere una pi agevole somministrazione intra - articolare del mezzo di contrasto . 
secondo la nostra opinione , tale manovra non dovrebbe essere interpretata come un secondo tentativo di puntura , perch non stata eseguita una nuova puntura . 814 radiol med ( 2013 ) 118 : 806815 sidered a second injection attempt , as it did not involve a second puncture . 
in this context , we found a vas score of 3.20.4 , which does not seem to be completely in line with previous results [ 7 , 11 ]  . 
 however , this small discrepancy could be explained by the fact that other studies used a more accurate vas scale with a score from 0 to 100 , rather than the 10 - point scale used by us . we had a low rate of extracapsular contrast leakage compared with rutten et al . 
 there were no severe complications in our study , as only 14 ( 12.6% ) patients had some temporary movement discomfort , which resolved spontaneously in < 30 min , and 13 ( 11.7% ) patients had a self - limiting vagal reaction ; the latter problem can easily be avoided by having patients lie on the side contralateral to the one being examined , rather than sit with their back to the radiologist . 
in our opinion , the sitting position is not safe , because in the event of a vagal reaction arising during the puncture , the radiologist cannot assist the patient promptly , as he or she is busy handling the probe and the needle . our study contains no estimation of radiologist time that is , the time needed by the physician to perform the contrast medium injection ( 1518 s )  . 
 in conclusion , we found that systematic use of the pauga technique is reliable , fast , well tolerated by patients and easy for the radiologist to perfor lapproccio posteriore sotto guida ecograca si dimostrato ben tollerabile dal paziente ; in tale ottica , abbiamo riscontrato un punteggio di 3 , 20 , 4 sulla scala vas che non sembra perfettamente in accordo con quanto riportato da altri studi [ 7 , 11 ]  . 
tuttavia , tale disaccordo sebbene minimo , potrebbe essere giusticato dal fatto che negli altri studi stata utilizzata una scala vas sicuramente risulta pi accurata , con punteggio da 0 a 100 . nel nostro studio , abbiamo avuto un basso tasso di stravaso extra - capsulare di mezzo di contrasto rispetto a rutten et al . 
tuttavia , se consideriamo che nella nostra casistica abbiamo avuto solo minimi stravasi , i dati diventano pi omogenei . il nostro studio non ha mostrato serie complicanze poich solo 14 ( 12 , 6% ) pazienti hanno mostrato impaccio nei movimenti , autolimitantesi in meno di 30 minuti e 13 ( 11 , 7% ) pazienti hanno avuto una reazione vagale , anchessa autolimitantesi ; tale complicanza stata facilmente gestibile da un punto di vista clinico , come dimostrato dalla nostra casistica , facendo assumere il decubito clinostatico sul anco al paziente , piuttosto che il decubito seduto con le spalle rivolte al radiologo . 
secondo la nostra opinione , la posizione da seduto del paziente non risulta sicura , poich in caso di reazione vagale , il radiologo sarebbe nellimpossibilit di prestare rapidamente soccorso in quanto con le mani impegante con la sonda ecograca e con lago . il nostro lavoro manca di una valutazione del tempo - radiologo che il tempo necessario al clinico per eseguire la somministrazione intra - articolare di mezzo di contrasto ( circa 1518 secondi )  . 
recursive partitioning analysis ( rpa ) class and national cancer institute common toxicity criteria ( nci - ctc ) version 3 were used to classify patients and evaluate acute toxicity , respectively . 
our data suggest that rct with tmz seems to produce a better outcome with a mild toxicity prole in elderly patients affected by gbm . keywords glioblastoma radiotherapy elderly chemotherapy riassunto obiettivo . 
la radiochemioterapia ( rtcht ) il trattamento standard nei pazienti affetti da glioblastoma ( gbm ) , ma a causa della mancanza di evidenze nei pazienti anziani , la radioterapia e la chemioterapia possono essere utilizzate singolarmente o integrate . 
la tossicit acuta , durante rtcht , stata accettabile ( 11 , 43% di trombocitopenia g3 - 4 ; 8 , 57% di tossicit neurologica g3 - 4 )  . 
i nostri dati suggeriscono che nei pazienti anziani lassociazione di radioterapia e temozolomide sembra essere efcace e sicura . parole chiave glioblastoma radioterapia pazienti anziani chemioterapia radiol med ( 2013 ) 118 : 870881 introduction introduzione high - grade gliomas ( hgg ) are the most common primary brain tumours in adults . 
predictors of outcome include not only tumour characteristics ( histology and genetics ) , extent of surgical excision and karnofsky performance status ( kps ) are predictors of outcome , but so is age at diagnosis , which is recognised as a predictor of poor prognosis [ 3 , 4 ]  . 
 [ 3 ] , using a recursive partitioning analysis ( rpa ) , evaluated 1 , 578 patients enrolled in three malignant glioma trials of the radiation therapy oncology group ( rtog ) from 1974 to 1989 and observed that patient age > 50 years was an important prognostic factor for survival , together with kps , neurological function and type of surgery ; these factors were used to dene six prognostic classes [ 3 ]  . 
as a result , few data on outcomes and toxicity are present in the literature , and treatment in this group of patients varied from observation to a radical approach [ 7 ]  . 
in an analysis conducted by scott et al . , elderly patients with gbm who underwent radiation therapy ( rt ) had improved cancer - specic survival ( css ) and os compared with patients not receiving rt [ 8 ] , and several studies emphasise that standard / aggressive approaches are possible in the elderly also [ 9 , 10 ]  . 
 the aim of this retrospective study was to evaluate acute toxicity and outcome in elderly patients affected by gbm treated with rct with tmz . i gliomi di alto grado ( gag ) sono i tumori cerebrali pi comuni nelladulto . 
il glioblastoma ( gbm ) , rappresentando il 75% di tutti i gag , una eteroplasia devastante che , nonostante i trattamenti aggressivi , ha una mediana di sopravvivenza globale ( os ) di circa un anno [ 1 ]  . 
il numero dei pazienti anziani affetti da gbm in aumento e , sfortunatamente , la loro aspettativa di vita di gran lunga pi breve rispetto ai pazienti pi giovani [ 2 ]  . 
tra i fattori predittivi per la sopravvivenza vi sono , non soltanto le caratteristiche tumorali ( istologia e genetica ) , lestensione dellescissione chirurgica ed il karnofsky performance status ( kps ) , ma anche let alla diagnosi stata riconosciuta come un fattore prognostico negativo [ 3 , 4 ]  . 
 [ 3 ] usando il recursive partitioning analysis ( rpa ) , hanno valutato 1578 pazienti arruolati in 3 studi sui gliomi maligni del radiation therapy oncology group ( rtog ) dal 1974 al 1989 ed hanno osservato che let superiore ai 50 un fattore correlato alla sopravvivenza insieme al kps , alle funzioni neurologiche ed alla chirurgia utilizzata ; questi fattori sono stati utilizzati per denire 6 classi prognostiche [ 3 ]  . 
i pazienti pi anziani , a causa della scarsa tolleranza e del rischio elevato di effetti collaterali , sono esclusi dai trials clinici : in letteratura ci sono pochi dati clinici sulla sopravvivenza e tossicit e perci il trattamento per questi pazienti varia dallosservazione allapproccio radicale [ 7 ]  . 
 [ 8 ] ha mostrato che i pazienti anziani con gbm sottoposti a radioterapia ( rt ) hanno una sopravvivenza cancro correlata migliore rispetto a i pazienti che non sono stati sottoposti ad rt [ 8 ] ed altri studi hanno sottolineato che lapproccio standard / aggressivo anche possibile negli anziani [ 9 , 10 ]  . 
 lo scopo di questo studio retrospettivo di valutare la tossicit acuta e loutcome nei pazienti anziani affetti da gbm trattati con rtcht con tmz . materials and methods 872 eligibility radiol med ( 2013 ) 118 : 870881 materiali e metodi elegibilit we retrospectively evaluated patients > 65 years with newly diagnosed and histologically proven gbm , kps > 60 , white blood cell count ( wbc ) > 3.5109 / l , platelet count > 150109 / l , bilirubin and creatinine levels < 1.5 times the upper limit of normal , aspartate aminotransferase ( ast ) , alanine aminotransferase ( alt ) and alkaline phosphatase < 2.5 times upper limit of normal who were treated at our institution . 
after surgery , patients received rt plus concomitant and adjuvant tmz , if feasible [ 5 ]  . sono stati inclusi pazienti con et superiore a 65 anni e con diagnosi istologica di gbm ; kps > 60 ; globuli bianchi3 , 5109 / l ; conta piastrinica150109 / l ; livelli di bilirubina e creatinina no a 1 , 5 volte superiore al normale ; aspartato aminotransferase ( ast ) , alanina aminotransferasi ( alt ) e fosfatasi alcalina no a 2 , 5 volte superiore alla normalit , sono stati trattati presso il nostro istituto e valutati retrospettivamente . 
tutti i pazienti sono stati sottoposti a resezione chirurgica denita , dal neurochirurgo e dal confronto degli esami di imaging pree post - operatori , come resezione completa , parziale o biopsia . 
dopo il trattamento chirurgico i pazienti hanno ricevuto rt con tmz concomitante e , se fattibile , adiuvante [ 5 ]  . radiotherapy radioterapia patient immobilisation was obtained using a thermoplastic mask . 
clinical target volume ( ctv ) was dened as tumour lesion and / or surgical bed plus oedema plus 0.5 - cm margins ; or if oedema was small or absent , ctv was dened by an expansion of tumour lesion and / or surgical bed plus 23 c the planning target volume ( ptv ) was created by adding 0.7 - cm margins to the ctv . 
il clinical target volume ( ctv ) stato denito come la lesione tumorale e / o il letto chirurgico con ledema e 0 , 5 cm di margine ; in assenza di edema , il ctv stato denito espandendo la lesione tumorale e / o il letto chirurgico di 23 cil planning target volume ( ptv ) stato creato espandendo il ctv di 0 , 7 cla dose totale al ptv stata di 60 gy ( 2 gy / die )  . 
dallinizio della rtcht , i pazienti hanno ricevuto terapia con 24 mg di desametasone al giorno per os . chemotherapy chemioterapia concomitantly , tmz was administered ( 7 days per week ) at a daily dose of 75 mg / mq ; after 4 weeks from the end of rt , patients underwent six cycles of tmz at a dose of 150200 mg / mq / day5 days every 28 days . 
anticonvulsants and antiemetics were administered , if necessary , during rt ; thereafter , antiemetic prophylaxis was used during adjuvant tmz . la tmz concomitante alla rt stata somministrata ( 7 giorni a settimana ) a dose giornaliera di 75 mg / mq e a 4 settimane dalla ne della radioterapia , i pazienti sono stati sottoposti a 6 cicli di tmz con dose di 150200 mg / mq / day5 giorni ogni 28 giorni . 
 radiol med ( 2013 ) 118 : 870881 surveillance and follow - up sorveglianza e follow - up baseline examination included postoperative gadolinium magnetic resonance imaging ( mri ) or ct , complete blood counts and blood chemistry . 
dalla ne della rt , la rm stata ripetuta ogni 3 mesi e la risposta al trattamento stata valutata secondo i criteri response evaluation criteria in solid tumors ( recist ) [ 11 ]  . 
 statistical analysis os was measured from the date of diagnosis to the date of death or last follow - up ; progression - free survival ( pfs ) was dened as the time from diagnosis to tumour progression / relapse or last follow - up . 
 analisi statistica la sopravvivenza globale ( os ) stata misurata dalla data della diagnosi alla morte o allultimo follow - up e la sopravvivenza libera da progressione ( pfs ) stata denita dalla diagnosi alla data della recidiva / progressione o allultimo follow - up . 
 sixteen of 35 patients ( 45.71% ) underwent six cycles of adjuvant tmz : six did not complete the planned treatment due to disease progression or toxicity ; 19 of 35 did not start chemotherapynine ( 25.71% ) due to disease progression , ve to age ( > 75 years ) and major comorbidity or neurothrombocytopaenia and ve ( 14.28% ) because they refused . 
sedici / 35 pazienti ( 45 , 71% ) hanno eseguito i cicli di tmz adiuvante : 6 pazienti non sono riusciti a completare il trattamento per progressione o tossicit . 
19 / 35 non hanno iniziato la chemioterapia adiuvante : 9 pazienti ( 25 , 71% ) per progressione di malattia , 5 pazienti per et ( maggiore di 75 anni ) per comorbilit maggiori o per neutropenia / trombocitopenia mentre 5 ( 14 , 28% ) pazienti hanno riutato il trattamento . 
durante la tmz concomitante , la trombocitopenia g3 - 4 stata riscontrata in 4 pazienti ( 11 , 43% ) , mentre non stata riscontrata nessuna neutropenia g3 - 4 . 
 overall survival at the moment of this analysis , three patients ( 8.57% ) were alive without evidence of disease , nine ( 25.71% ) were alive with disease and 23 ( 65.72% ) had died due to the disease . 
 sopravvivenza libera da progressione con un follow - up mediano di 11 mesi ( range 341 ) , 29 / 35 pazienti ( 82 , 85% ) hanno sviluppato una progressione di malattia documentata alla rm . 
 sopravvivenza al momento dellanalisi , 3 pazienti ( 8 , 57% ) sono vivi senradiol med ( 2013 ) 118 : 870881 za malattia , 9 ( 25 , 71% ) sono vivi con malattia e 23 pazienti ( 65 , 72% ) sono morti . 
 discussione attualmente il trattamento riconosciuto come standard per il gbm consiste nella resezione chirurgica seguita dalla rtcht con tmz adiuvante [ 5 ] , ma sfortunatamente nei pazienti anziani lapproccio terapeutico appropriato sconosciuto . 
 nei pazienti con et superiore ai 65 anni , la resezione aggressiva ha mostrato un incremento della sopravvivenza se comparata alla sola biopsia o alla resezione parziale senza aumentare il rischio di morbilit chirurgica [ 12 , 13 ]  . 
dopo il trattamento chirurgico , i pazienti anziani vanno incontro a diverse tipologie di trattamen to : rtcht o radioterapia oppure chemioterapia o best supportive care [ 7 ]  . 
secondo le linee guida , la rtcht , incrementando la sopravvivenza [ 5 , 1419 ] , rientra nella categoria 1 di raccomandazione per i pazienti giovani , ma per i pazienti over 70 , rientra nella categoria 2b : stupp et al . 
 [ 5 ] hanno riportato una os mediana di 14 , 6 mesi ( range 13 , 216 , 8 ) con una sopravvivenza ad 1 e 2 anni del 61 , 1% e 26 , 5% , rispettivamente [ 5 ] , escludendo da que sto studio i pazienti con unet superiore ai 70 anni . 
 attualmente il termine anziano si riferisce allet pensionabile ( 65 anni ) anche se in letteratura vengono utilizzati diversi cut - off ( 60 , 65 , 70 o 75 anni ) [ 2022 ]  . 
i pazienti over 70 presentano diverse comorbilit , che presumibilmente , potrebbero rendere difcile la tolleranza alla radiochemioterapia , anche se questa correlazione non stata ancora denita [ 23 ]  . 
nonostante il ruolo della rtcht nei pazienti anziani sia incerto , nella nostra istituzione , let non considerata un fattore limitante nella scelta del trattamento , perci il regime terapeutico di stupp et al . 
 aggressive resection in patients > 65 did not increase surgical morbidity and was found to prolong survival compared with needle biopsy or partial resection [ 12 , 13 ]  . 
adjuvant rct improves survival [ 5 , 1419 ] and is a category 1 recommendation for younger patients but a category 2b in patients > 70 years : stupp et al . 
an update of this trial with 5 - years follow - up showed the benet of rct also in patients 6570 years [ hazard ratio ( hr ) for death , 0.7 , with 95% condence interval ( ci ) 0.50.97 ] [ 14 ]  . 
 the term elderly is often linked to the age of eligibility for retirement benets ( 65 years ) , but different cutoff ages ( 60 , 65 , 70 or 75 years ) are used in the literature [ 2022 ]  . 
 patients > 70 years have an increased number of comorbidities , which presumably makes it difcult to tolerate rct 876 radiol med ( 2013 ) 118 : 870881 even if this is not dened [ 23 ]  . 
although the role of rct in the elderly is uncertain , at our institution , age was not considered a limiting factor in the choice of treatment approach , and the stupp regimen was used in all gbm patients , with a good performance status [ 5 ]  . 
la compliance al trattamento concomitante stata del 94 , 3% : nessun paziente ha interrotto la rtcht per tossicit e solo 2 pazienti hanno interrotto il trattamento per progressione di malattia . 
i dati preliminari di uno studio retrospettivo ( 305 pazienti affetti da gbm con et superiore a 60 anni , trattati con la sola rt o con rt e tmz ) , presentato al meeting annuale dellassociazione americana di oncologia clinica ( asco ) del 2010 , ha mostrato una os mediana di 12 mesi nel gruppo della radiochemioterapia [ 21 ]  . 
la tossicit e loutcome della presente analisi sono paragonabili agli altri studi pubblicati ( tabelle 2 e 3 ) e mostrano come table 2 published data on acute haematological toxicity during radiochemotherapy ( rct ) with temozolomide ( tmz ) in elderly patients patients ( n ) acute neutropaenia g34 , % ( n ) acute thrombocytopaenia g34 , % ( n ) author brandes et al . 
toxicity and outcome of our analysis compared favourably with other published studies ( tables 2 and 3 ) and showed that rct plus tmz la radiochemioterapia con tmz sia fattibile ed efcace nei pazienti anziani , con una os mediana variabile dai 10 ai 15 mesi . 
although the prognostic prole of our patients was not favourable ( 68.57% of cases > 70 years , 100% of cases in rpa class vvi , 68.57% of cases with partial resection or biopsy ) , our survival data were consistent with those of the subgroup of patients aged 6070 years treated in the eortc / ncic study ( median os 10.9 months ) [ 5 ]  . 
 adjuvant tmz was administered to 16 patients , and only 10 / 35 ( 28.57% ) completed the planned treatment , so that no statistical analysis was performed to evaluate the impact of adjuvant tmz . 
dropping out of chemotherapy is frequently observed , and in fact , about 20% of elderly patients completed adjuvant tmz [ 24 , 25 , 27 ]  . there is as yet no comparison of the standard stupp regimen and rt or tmz alone in the elderly , even though combined therapy offered better results , as shown in table 4 . 
 when we compared our results with those reached with a single - modality approach , we observed an increase in sur6070 trattati nello studio eortc / ncic ( os mediana di 10 , 9 mesi ) [ 5 ]  . 
 la chemioteraia con tmz adiuvante stata somministrata a 16 pazienti e solo 10 ( 28 , 57% ) hanno completato il trattamento pianicato , per questa ragione non stata eseguita nessuna analisi statistica per valutare lefcacia del tmz adiuvante . 
frequentemente si osserva linterruzione della chemioterapia , infatti circa il 20% degli anziani riesce a completarla [ 24 , 25 , 27 ]  . al momento non ci sono studi comparativi tra il regime di trattamento standard e la sola rt o chemioterapia con tmz , nonostante la terapia combinata offra migliori risultati come mostrato in tabella 4 . 
confrontando i nostri risultati con quelli raggiunti con la sola rt o tmz , abbiamo osservato un aumento della sopravvivenza con la radiochemioterapia ( tabella 3 e 4 )  . 
nei pazienti over 65 , il trattamento radiante standard o ipofrazionato da solo o la chemioterapia con tmz da sola , hanno riportato una sopravvivenza mediana di circa 6 mesi [ 2833 ] e per detable 4 published data on outcome in elderly patients with glioblastoma author therapy patients ( n ) median kps median age ( years ) median os ( months ) chamberlain et al . 
 [ 27 ] ( pts > 65 years ) rct , radiochemotherapy ; tmz , temozolomide ; kps , karnofsky performance status ; pfs , progression - free survival ; gbm , glioblastoma ; nr , not reported ; os , overall survival ; adj , adjuvant ; n , number ; pts , patients 11.5 radiol med ( 2013 ) 118 : 870881 tabella 4 dati di sopravvivenza sui pazienti anziani affetti da glioblastoma ( gbm ) autore terapia pazienti ( n ) kps mediano et mediana ( anni ) os mediana ( mesi ) tmz week on - off 178 ( 155 gbm ) 193 ( 178 gbm ) chamberlain et al . 
 [ 27 ] ( pts65 anni ) kps , karnofsky performance status ; os , sopravvivenza globale ; rt , radioterapia ; tmz , temozolomide ; rpa , recursive partitioning analysis ; adj , adiuvante ; pts , pazienti ; nr , non riportato 11 , 5 vival time if the elderly patients received the stupp regimen ( table 3 and 4 )  . 
 the neuro - oncology working group of the german cancer society randomised patients > 65 years to either tmz or rt alone and , based on preliminary data , showed the superiority of rt [ 34 ]  . 
the nordic brain tumor study group randomised gbm patients > 60 years to standard rt ( 60 gy ) , hypofractionated rt ( 34gy ) and tmz alone , showing an advantage of chemotherapy [ 35 ]  . 
 in conclusion , the stupp regimen [ 5 ] remains the standard treatment approach in patients < 70 , and although there terminare il ruolo della rt e del tmz , nel 2005 iniziato larruolamento per due studi randomizzati di phase ii i cui dati preliminari sono stati presentati allasco nel 2010 . 
il neuro - oncology working group della german cancer society ha randomizzato pazienti over 65 a ricevere o tmz o rt e , i dati preliminari , hanno mostrato la superiorit della rt [ 34 ]  . 
il nordic brain tumor study group ha randomizzato pazienti over 60 a ricevere rt standard ( 60 gy ) , rt ipofrazionata ( 34 gy ) oppure tmz , mostrando un vantaggio della chemioterapia [ 35 ]  . 
 [ 5 ] rimane il trattamento standard nei pazienti under 70 e nonostante non ci sia un livello di evidenza 1 nei pazienti anziani , lapproccio combinato ( rt e tmz ) sembra 880 radiol med ( 2013 ) 118 : 870881 is no level 1 evidence in elderly patients , combined modality ( rt plus tmz ) seems to produce a better outcome than the single modality in this group [ 36 ]  . 
despite the limitations of this analysis [ retrospective , small sample size and absence of the methyl - guanine methyltransferase ( mgmt ) test that has only recently become available at our centre ] , our data agree with the literature and suggest that the association of rt with tmz could be considered a safe and effective strategy for treating gbm in elderly patients , showing a better survival with mild toxicity than the single - modality approach . 
considerando i limiti di questa analisi ( dati retrospettivi , ridotto campione e assenza della valutazione del mgmt test , recentemente disponibile nel nostro istituto ) , i nostri dati sono in accordo con la letteratura e suggeriscono che lassociazione di rt e tmz potrebbe essere considerata una strategia sicura ed efcace nel trattamento degli anziani con gbm , mostrando una migliore sopravvivenza con tossicit lieve rispetto allapproccio terapeutico in singola modalit . 
ten cases have been chosen for each section , simple as well as complicated or unusual cases highlighting the topic , cases which should and could be of practical use to both physicians in training as well as expert radiologists . each case is presented following a xed framework which presents on the rst page radiological images , primarily ct , mri or us and on the facing page a very short clinical history , extended comments about the condition and pertinent imaging ndings . 
this layout makes one wonder : why do comments anticipate the imaging ndings ? it would have been better at least in my opinion exactly the contrary . at the end of each ten - case section one will nd one page of selected references ( books ; websites ; articles ) in order to expand the readers knowledge on the topic . images are of the highest quality and properly chosen however , sometimes arrows are missing . 
 intenzione di questo volume nelle sue 256 pagine di offrire al lettore una serie di casi interessanti lo studio per immagini delladdome , divisi in dieci sezioni dedicate : fegato , colecisti ed albero bilaire ; pancreas ; milza ; peritoneo ; esofago ; stomaco e duodeno ; intestino tenue ; colon ; retto ed ano . 
 per ogni sezione sono stati selezionati dieci casi , sia semplici che complicati od inusuali , ben illustranti largomento , casi che dovrebbero e potrebbero essere di utilit pratica sia ai medici in tirocinio che ai radiologi esperti . ogni caso presentato seguendo uno schema determinato , caratterizzato da una prima pagina con le immagini radiologiche , fondamentalmente tc , rm o us e , sulla pagina a fronte , da una storia clinica molto succinta ed unampia epicrisi corredata da immagini diagnostiche pertinenti . 
di fronte a questa impostazione ci si chiede : perch i commenti precedono i reperti per immagini ? sarebbe stato meglio , almeno secondo la mia opinione , disporre esattamente del contrario . 
 al termine dei dieci casi di ogni sezione , si trova una pagina di riferimenti selezionati ( libri , websites , articoli ) , in modo tale da poter ampliare le conoscenze del lettore sullargomento . le immagini sono della pi elevagta qualit e scelte con cura : tuttavia , talvolta , mancano delle opportune frecce indicatrici . 
vulpio , tel : + 39 - 06 - 30155485 , fax + 39 - 06 - 30155491 , e - mail : c.vulpio@alice.it received : 2 december 2011 / accepted : 29 february 2012 / published online : 22 october 2012 springer - verlag 2012 abstract purpose . 
in 85 hdp , we evaluated the following us parameters of all and of the largest ptgs : number , maximum longitudinal diameter ( mld ) , structural ( hypoechoic , heterogeneous , nodular ) and vascular ( nonhypovascular , intermediate , hypervascular ) echo - pattern scores . 
in the 41 ( 59% ) responders , number ( 01 ) , mld ( < 10 mm ) and structural and vascular scores ( 12 ) of the largest ptg were signicantly lower than in nonresponders . 
receiver operating curve ( roc ) curve analysis showed high sensitivity and specicity ( 90% and 73% , respectively ) of the mld ( < 10mm ) of the largest ptg in the predicting therapeutic outcome . 
i 69 hdp sono stati classicati responders ( r ) [ mediana ormone paratiroideo intatto ( ipth ) 300 pg / ml durante follow - up ] o nonresponders ( nr ) ( ipth > 300 pg / ml )  . 
in 41 ( 59% ) r il numero ( 01 ) , il mld ( < 10 mm ) e gli score strutturali e vascolari ( 12 ) della ptg maggiore erano signicativamente inferiori rispetto ai nr . 
lanalisi della curva receiver operating curve ( roc ) dimostra unelevata sensibilit e specicit del mld [ 90% / 73% ] della ptg maggiore ( < 10 mm ) nel predire la risposta terapeutica . 
 correlati alla gravit del shpt ed al tipo di iperplasia paratiroidea e predicono la risposta alla terapia medica . keywords ultrasonography secondary hyperparathyroidism parathyroid glands vitamin d cinacalcet parole chiave ecograa iperparatiroidismo secondario paratiroidi vitamina d cinacalcet introduction introduzione ultrasonography ( us ) of the parathyroid glands ( ptgs ) was introduced in the diagnosis of secondary hyperpara thyroidism ( shpt ) in haemodialysis patients ( hdp ) many years ago [ 19 ]  . 
most authors believe that us is an indispensable tool for the surgeon to identify ptg number , size and site before surgery and to correctly plan the surgical procedure [ 10 , 11 ]  . 
nevertheless , us is largely used in clinical practice as it is noninvasive , easily repeatable and has acceptable sensitivity and specicity ( 8095% in primary hpt and 4580% in shpt ) [ 1420 ]  . 
 indeed , it has been recently suggested that us is not only the most effective method for detecting the number and site of ptgs in candidates for parathyroidectomy , but also the most appropriate tool to dene size , shape and echostructural and vascular patterns in shpt patients [ 2123 ]  . 
 patients and methods population lecograa ( us ) delle ghiandole paratiroidee ( ptg ) stata introdotta da diversi anni nella diagnosi delliperparatiroidismo secondario ( shpt ) dei pazienti emodializzati ( hdp ) [ 19 ]  . 
la maggior parte degli autori ritiene che lus sia uno strumento diagnostico indispensabile al chirurgo per identicare il numero , le dimensioni , e la sede delle ptg prima dellintervento e pianicare correttamente la procedura chirurgica [ 10 , 11 ]  . 
ciononostante lus diffusamente utilizzata nella pratica clinica in quanto non - invasiva , facilmente ripetibile e dotata di una sensibilit e specicit accettabili ( 80%95% nel iperparatiroidismo primario e 45%80% nel shpt ) [ 1420 ]  . 
in realt recentemente stato suggerito che lus non soltanto il mezzo pi efcace per evidenziare il numero e la sede delle ptg nei pazienti candidati a patiroidectomia , ma anche lo strumento pi appropriato per denire la loro dimensione , forma , eco - struttura e vascolarizzazione nei pazienti con shpt [ 2123 ]  . 
la presenza di nh il principale fattore determinante dellirreversibilit del shpt e del fallimento della terapia medica [ 2729 ] e la sua tempestiva dimostrazione utile per denire la strategia terapeutica [ 30 ]  . nel presente studio , abbiamo misurato i parametri us ( numero , dimensioni , eco - patterns strutturali e vascolari ) delle ptg riscontrate negli hdp con shpt e valutato come essi differiscono in relazione al grado di shpt , la risposta terapeutica e il tipo istologico diperplasia ghiandolare . we retrospectively examined us ndings of ptgs of 85 hdp from the hemodialysis service of the department of surgery , catholic university , rome . 
the study objective was to dene : ( 1 ) the possible correlation between biochemical markers of calciumphosphorus ( capi ) metabolism and us parameters of ptgs ; ( 2 ) us parameters of ptgs of patients who responded to medical therapy compared with those who did not ; ( 3 ) possible correlations between us parameters / patterns and type of hyperplasia assessed by pathology . 
 we dened ptgs as nodules placed posterior to the thyroid capsule , with a longitudinal diameter parallel to that of the thyroid , with an independent afferent artery and hypoechoic or heterogeneous / nodular echostructural pattern . 
sin da gennaio 2004 , tutti i hdp vengono sottoposti a us delle ptg quando viene diagnosticato un shpt [ ormone paratiroideo intatto ( ipth ) > 300 pg / ml ] e prima di essere avviati alla terapia medica o chirurgica . 
lobiettivo dello studio stato denire : ( 1 ) le possibili correlazioni tra i markers biochi mici del metabolismo calcio - fosforico ed i parametri us delle ptg ; ( 2 ) i parametri us delle ptg dei pazienti che avevano risposto alla terapia medica rispetto a quelli che non avevano risposto ; ( 3 ) le possibili correlazioni tra i parametri e patterns us ed il tipo di iperplasia denito dallistologia . 
il livello di ipth stato determinato mediante dosaggio immunologico con electrochemiluminescenza ( roche modular e 170 , roche diagnostics ltd , svizzera ; range di normalit 1065 pg / ml )  . 
 abbiamo denito ptg quei noduli situati posteriormente alla capsula tiroidea , con diametro longitudinale parallelo a quello della tiroide , con una arteria afferente indipendente ed una eco - struttura ipoecogena o eterogenea / nodulare . 
1a - f score degli eco - patterns strutturali ( a ipoecogeno omogeneo o lievemente eterogeneo ; b altamente eterogeneo , c nodulare ) e vascolari ( d ao ipo - vascolarizzato : segnale di usso sanguigno assente o singolo e minuto spot periferico o centrale ; e score intermedio : minuti e multipli spot di segnale di usso sanguigno interessanti meno del 30% della circonferenza o supercie della ptg ; f ipervascolarizzato : multipli e marcati segnali di usso centrali e periferici coinvolgenti pi del 30% della circonferenza e della supercie della ptg )  . radiol med ( 2013 ) 118 : 707722 fig . 
b nodular ( score 3 ) echo pattern and corresponding vascular ow signal : frequently in cases of adenoma - like hyperplasia , the intraglandular arterial branches surround the hyperplastic nodule . 
 circumference and / or < 30% of surface ; ( 3 ) hypervascular multiple high peripheral and central blood - ow signal taking up > 30% of ptg surface and circumference . 
 pathology ptg size was assessed in the operating room immediately after resection , and type of glandular hyperplasia was dened by a single experienced pathologist ( fg ) according to tominaga et al . 
abitualmente nello stesso paziente sono presenti simultaneamente i tipi diversi di iperplasia poich laccrescimento delle ptg asincrono ed asimmetrico . statistical analysis istologia data were analysed by medcalc software ( belgium version 12 for microsoft windows xp )  . 
the appropriate test was used when comparing group means [ t test , analysis of variance ( anova ) studentnewmankeuls post hoc comparison ] or median and frequencies ( mannwhitney , chi - square , kruskalwallis tests )  . 
 [ 10 ] come segue : ( 1 ) iperplasia diffusa , ( 2 ) iperplasia iniziale o micro - nodulare , ( 3 ) iperplasia macro - nodulare e simil - adenomatosa ( adenomalike )  . analisi statistica i dati sono stati analizzati mediante il software medcalc ( belgio versione 12 , per microsoft windows xp )  . 
of these , 39 ( group a ) underwent conventional therapy with vitamin d alone ( before 2006 ) , 30 ( after 2006 ) were treated with vitamin d ( paricalcitol ) and cinacalcet ( group b ) and 16 ( referred to our centre from other dialysis units of our region ) underwent parathyroidectomy ( group c )  . 
 the hdp of group a underwent therapy with intravenous calcitriol ( meansd dose 3.21.7 g / week , range 16 ) or paricalcitol ( meansd 12.74.6 g / week , range 525 ) according to national kidney foundation kidney disease outcomes quality initiative ( nkf - kdoqi ) guidelines and to the manufacturers posology [ 30 ]  . 
in group b , paricalcitol ( 10.45.7 g / week ) was associated with the maximal tolerated dose of cinacalcet ( 52.315.2 mg / die )  . hdp of groups a and b were treated and followed up at our dialysis centre for 31.718.7 ( range , 1360 ) months . 
 hdp were classied as responders if median ipth serum level during treatment and follow - up was 300 pg / ml ( maximum ipth level recommended by the nkf - kdoqi guidelines ) and as nonresponders if median ipth was > 300 pg / ml or parathyroidectomy was performed . 
 in nonresponders of groups a and b with high levels of ipth ( > 800 pg / ml ) , ca and pi after at least 6 months of medical treatment with the maximum doses of drugs permitted , parathyroidectomy was proposed . 
at pathological examination , 15 ( 15.2% ) ptgs showed diffuse , 60 ( 60.6% ) micronodular and 24 ptgs ( 24.2% ) macronodular / adenoma - like hyperplasia . us ndings and clinical outcome table 2 shows the number of ptgs , mld and structural and vascular echo patterns of all ptg and of the largest ptg detected in group a , b and c hdp . 
as shown in table 2 , median [ interquartile range ( iqr ) ] number and mean mld of all and largest ptgs of responders in group a or group b were signicantly lower than that of nonresponders . 
interestingly , mld and number of ptgs of nonresponders in groups a and b were similar to those of surgical patients in group c . us showed no ptg in 12 ( 29% ) of 41 responders ( nine patients of group a and three of group b ) and at least one ptg in the remaining 29 hdp . 
le correlazioni tra due variabili sono state calcolate con test parametrico ( test di correlazione di pearson ) o test non parametrico ( test di correlazione di spearman )  . 
la capacit diagnostica nel discriminare i casi responders ( r ) da quelli non responders ( nr ) dei diversi punti di cut - off dei parametrici biochimici ed us stata valutata mediante lanalisi della curva receiver operating curve ( roc )  . 
trentanove ( gruppo a ) sono stati sottoposti a terapia convenzionale con la sola vitamina d ( prima del 2006 ) ; 30 ( dopo il 2006 ) sono stati trattati con vitamina d ( paracalcitolo ) e cinacalcet ( gruppo b ) mentre 16 ( inviati al nostro centro da altre unit di dialisi della nostra regione ) sono stati sottoposti a paratiroidectomia ( gruppo c )  . 
 gli hdp del gruppo a sono stati sottoposti a terapia endovenosa con calcitriolo ( dose mediads dose 3 , 21 , 7 g / settimana , range 16 ) o paracalcitolo ( mediads 12 , 74 , 6 g / settimana range 525 ) nel rispetto delle linee guida national kidney foundation kidney disease outcome quality initiative ( nkf - kdoqi ) e della posologia del produttore [ 30 ]  . 
 la paratiroidectomia stata proposta ai nr dei gruppi a e b con livelli elevati di ipth ( > 800 pg / ml ) , calcio e fosforo dopo almeno 6 mesi di terapia medica con le massime dosi permesse dei farmaci . 
allesame istologico , 15 ( 15 , 2% ) ptg mostravano iperplasia diffusa , 60 ( 60 , 6% ) micro - nodulare e 24 ptg ( 24 , 2% ) iperplasia macro - nodulare e adenoma - like . 714 radiol med ( 2013 ) 118 : 707722 table 1 demographic , clinical and laboratory characteristics of responders ( r ) and nonresponders ( nr ) of each group . 
some patients with moderate concentrations of baseline ipth ( 400700 pg / ml ) associated with mld > 10 mm were nonresponders to therapy ; conversely , patients with higher baseline ipth concentrations ( > 800 pg / ml ) associated with mld < 10 mm were responders . 
the ipth , serum ca and alp levels were signicantly correlated with ptg number and mld , which are structural and vascular echo patterns of the risultati della us e risposta clinica la tabella 2 mostra il numero di ptg , il mld e i patterns eco - strutturali e vascolari di tutte le ptg e di quella maggiore riscontrate nei hdp dei gruppi a , b e c . 
come mostrato in tabella 2 , il numero mediano ( range interquartile ) e il mld medio di tutte le ptg e di quella maggiore dei pazienti r sia del gruppo a che del gruppo b erano signicativamente minori rispetto ai pazienti nr . 
in modo interessante , il mld ed il numero di ptg dei pazienti nr del gruppo a e b erano simili a quelli dei pazienti chirurgici del gruppo c . lus non ha mostrato nessuna ptg in 12 ( 29% ) dei 41 responders hdp ( 9 pazienti del gruppo a e 3 del grup po b ) e almeno una ptg nei rimanenti 29 hdp . 
in groups a and b , roc curve analysis showed a high sensitivity and specicity of mld of the largest ptg ( 90% and 73% respectively ; cutoff 10 mm , auc 0.9 , p < 0.0001 ) and ipth concentration ( 83% and 82% , respectively ; cutoff 750 pg / ml , auc 0.8 , p < 0.0001 ) in predicting therapeutic outcome . 
 us ndings and pathology twenty - six parathyroidectomies were performed , and 99 ptgs were removed : 84 ( 85% ) in orthotopic and 15 ( 15% ) in ectopic sites . 
prendendo in considerazione tutte le 140 ptg riscontrate , si dimostrata una correlazione signicativa tra il mld ed il punteggio del pattern eco - struturale ( coefciente di correlazione di spearman 0 , 736 , p < 0 , 0001 ) e vascolare ( coefciente di spearman 0 , 710 , p < 0 , 0001 )  . 
questi due parametri erano anche tra loro correlati ( coefciente di spearman 0 , 724 , p < 0 , 0001 ) : con laumentare del mld prevalgono i patterns ecograci pi gravi . 
us detected only four of 14 ptgs with diffuse hyperplasia , and the small sample did not allow statistical comparison between structural and vascular echo patterns and type of ptg hyperplasia . 
anche i livelli di ipth e il mld della ptg maggiore erano signicativamente correlati ( coefciente di correlazione di person 0 , 529 , p < 0 , 0001 )  . 
nel gruppo a e b , lanalisi della curva roc ha dimostrato unalta sensibilit e specicit del mld della ptg maggiore ( 90% e 73% rispettivamente ; cut - off10 mm , auc 0 , 9 , p < 0 , 0001 ) e della concentrazione del ipth ( 83% e 82% rispettivamente cut - off750 pg / ml , auc 0 , 8 , p < 0 , 0001 ) nel predire la risposta terapeutica . 
 risultati della us ed istologia sono state eseguite 26 paratiroidectomie e sono state rimosse complessivamente 99 ptg : 84 ( 85% ) in sede ortotopica e 15 ( 15% ) in sede ectopica . 
indeed , the study showed that us detection of ptg was negative in 12 ( 29% ) of 41 responders to medical treatment and that in the remaining 29 responders , us usually detected one or two small ptgs ( mld < 10mm ) associated with low structural and vascular pattern scores . 
lanalisi della 718 radiol med ( 2013 ) 118 : 707722 curva roc ha dimostrato che il mld istologico > 8 mm predice liperplasia nodulare ( microe macro - nodulare ) con 83% e 78% di sensibilit e specicit rispettivamente ( auc 0 , 78 , p < 0 , 0001 )  . 
 escludendo le 15 ptg ectopiche , lus ha evidenziato 56 su 84 ptg ortotopiche , : solo 4 ( 36% ) su 14 ptg ortotopiche con iperplasia diffusa , 34 ( 68% ) su 50 ptg con iperplasia micro - nodulare e 18 ( 80% ) su 20 ptg con iperplasia paratiroidea macro - nodulare e adenoma like ( 2 14 , 1 p < 0 , 001 )  . 
lus ha evidenziato solo 4 su 14 ptg con iperplasia diffusa ed il campione limitato di ptg con iperplasia diffusa non ha permesso un confronto statistico tra gli eco patterns strutturali e vascolari ed il tipo di iperplasia delle ptg . 
 il presente studio dimostra che nei pazienti emodializzati con shpt i parametri ecograci delle ptg sono correlati con la gravit del shpt e sono predittivi della responsivi t alla terapia medica in quanto indicativi del tipo diperplasia ghiandolare . 
in effetti , il presente studio ha evi denziato che la ricerca ecograca di ptg era negativa in 12 ( 29% ) su 41 hdp responders alla terapia medica e che nei rimanenti 29 responders lus generalmente ha visualizzato una o due piccole ptg ( mld < 10 mm ) con bassi punteggi degli eco - patterns strutturali e vascolari . 
lus delle ptg dei pazienti nr , invece , ha visualizzato almeno una ptg ma abitualmente pi di una ptg con un mld > 10 mm ed eco - patterns con pi alti punteggi . 
 [ 17 , 18 ] hanno riferito che i pazienti con almeno una ptg pi grande di 0 , 5 cm3 o 10 mm di diametro generalmente risultavano refrattari alla terapia con calcitriolo . 
4 correlazione tra diametro longitudinale massimo ( mld ) ecograco e istologico ( equazione di regressione y = 4 , 1 + 0 , 6x ; coefciente di determinazione r2 0 , 4 , p < 0 , 0001 )  . 
 [ 21 ] showed that the suppressive effect of a single oral dose of 8 g of calcitriol on ipth concentration was reduced in patients with us evidence of enlarged ptgs . 
overall , our results suggest that long - term medical treatment may be helpful in patients with ptg < 10 mm and useless in patients with ptg > 10 m another interesting result of our study is that mld of ptgs evaluated by us was signicantly correlated with mld determined by histology and predictive of nodular hyperplasia . 
in this regard , it is well known that the presence of nodular hyperplasia is commonly recognised as the most important cause of medical therapy failure because of the down - regulation of the vitamin d receptor ( vdr ) and calcium - sensing receptor ( casr ) [ 35 ]  . 
moreover , the mld of ptg with diffuse hyperplasia was 7.13.1 mthese data conrm that diffuse hyperplasia is an initial stage of ptg hyperplasia and that us does not always detect ptg at this stage , possibly because of the small size and shape . 
conversely , ptgs with advanced stage of growth present with an echogenic capsule distinct from the thyroid capsule and a hypoechoic shape due to hypercellularity and progressive disappearance of the fatty area . 
 [ 21 ] hanno dimostrato che leffetto soppressivo sulle concentrazioni di ipth di una singola dose orale di 8 g di calcitriolo era ridotta nei pazienti con evidenza ecograca di ptg ingrandite . 
nel complesso , i nostri risultati suggeriscono che la terapia medica a lungo termine pu essere utile nei pazienti con ptg < 10 mm e inutile nei pazienti con ptg > 10 mm . un altro risultato interessante del presente studio che il diametro delle ptg misurato con lecograa e quello misurato con listologia erano strettamente correlati e predittivi della iperplasia nodulare . 
infatti lanalisi della curva roc ha dimostrato che un mld istologico > 8 mm predice con accuratezza la presenza di iperplasia nodulare con una sensibilit e specicit del 83% e 78% . 
a questo riguardo ben risaputo che la presenza di iperplasia nodulare comunemente riconosciuta come lorigine pi importante del fallimento della terapia medica a causa della down - regulation dei recettori della vitamina d ( vdr ) e del calcio ( calcium sensing receptor , casr ) [ 35 ]  . 
 nel presente studio abbiamo dimostrato che lus non ha evidenziato alcuna ptg nel 29% dei hdp responders e che ha documentato solo il 36% delle 14 ptg ortotopiche con iperplasia diffusa . 
il mld delle ptg con iperplasia diffusa era 7 , 13 , 1mquesti dati confermano che liperplasia diffusa rappresenta uno stadio iniziale della iperplasia delle ptg e lus non sempre in grado di evidenziare le ptg in questo stadio , probabilmente a causa delle piccolo dimensioni e della forma della ptg . 
viceversa le ptg con un grado di avanzato accrescimento presentano una capsula ecogena distinta da quella tiroidea ed un aspetto ipoecogeno dovuto allipercellularit ed alla progressiva scomparsa delle aree di tessuto adiposo . 
6a , b la gura mostra 2 casi di iperplasia macro - nodulare ( a ) e adenoma - like ( b ) delle ptg : eco - pattern strutturale ( in alto ) , esame macroscopico della sezione longitudinale ( nel mezzo ) e istologia ( in basso )  . 
however , sometimes it may be difcult to distinguish the heterogeneous and nodular patterns because there are intermediate pictures between the two scores and a clear distinction of two patterns can be difcult , especially without the aid of cdus imaging . simultaneously to ptg growth , vascular blood supply increases [ 3638 ]  . 
cdus will demonstrate a peripheral vascular arc arising from the incomunque in alcuni casi pu essere difcile distinguere il pattern eterogeneo da quello nodulare poich vi sono quadri intermedi tra i due scores ed una chiara distinzione dei due patterns pu essere difcile specialmente senza lausilio del color doppler . in simultanea allaccrescimento della ptg , aumenta anche lafusso ematico vascolare [ 3638 ]  . 
una volta che larteria nutritiva entra nella ghiandola iperplastica , essa si ramica verso la periferia prima che le diramazioradiol med ( 2013 ) 118 : 707722 ferior thyroidal artery branch and encircling the ptg . 
these results suggest that us of ptgs may play an important role in staging renal shpt and consequently dene the most appropriate therapeutic strategy . ni pi piccole penetrino in profondit [ 39 ]  . 
i linfonodi potranno in modo caratteristico mostrare una vascolarizzazione centrale ed ilare ed un ilo centrale adiposo e i noduli tiroidei non hanno una afferenza vascolare propria [ 15 ]  . 
agolli , santandrea hospital , via di grottarossa 1035 - 1039 , 00189 rome , italy , tel . : + 39 - 06 - 33776160 / 06 - 33776164 , fax : + 39 - 06 - 33776608 , e - mail : lindaagolli@yahoo.it received : 2 november 2011 / accepted : 20 march 2012 / published online : 29 november 2012 springer - verlag 2012 abstract purpose . 
the inuence of the prognostic factors on overall ( os ) , disease - free ( dfs ) , disease - specic ( dss ) , colostomy - free ( cfs ) and metastasis - free ( mfs ) survival was evaluated . 
stato valutato limpatto dei fattori prognostici su sopravvivenza globale ( os ) , sopravvivenza libera da malattia ( dfs ) , sopravvivenza specica di malattia ( dss ) , sopravvivenza libera da colostomia ( cfs ) e sopravvivenza libera da metastasi ( mfs )  . 
 dovremmo considerare il t e ln come importanti fattori prognostici per la sopravvivenza . parole chiave cancro anale radioterapia chemioterapia fattori prognostici radiol med ( 2013 ) 118 : 882894 introduction anal cancer is a relatively rare disease with a good prognosis , constituting 4% of all lower gastrointestinal tract and 1.6% of all digestive system malignancies [ 1 , 2 ]  . 
three randomised trials established radiotherapy and concurrent chemotherapy regimen with 5 - uoruracil ( 5 - fu ) and mitomycin c ( mmc ) as the gold standard for treating anal carcinoma ; however , these studies also reported signicant acute toxicity rates . 
patients treated with curative radiochemotherapy presented locoregional failure rates of approximately 30% , with disease - free survival ( dfs ) rates of 5070% and overall survival ( os ) rates of 6075% [ 11 13 ]  . 
 the purpose of this retrospective analysis was to evaluate disease control after radiation therapy with or without concurrent chemotherapy in terms of os , dfs and colostomy - free survival ( cfs ) .in patients with anal cancer treated at a single institute . 
we also sought to determine acute and late toxicity rates and prognostic factors . materials and methods between may 2002 and november 2010 , 42 patients with anal cancer were treated at our department of radiation oncology with primary radiotherapy with or without concurrent chemotherapy and were included in this retrospective analysis . 
pretreatment evaluation included history , physical examination , total - body computed tomography ( ct ) , colonoscopy and proctoscopy examination and endorectal ultrasound ( us ) and / or magnetic resonance imaging ( mri ) of the pelvis . 
all primary tumours were histologically proven by introduzione il cancro anale una patologia relativamente rara associata a una buona prognosi e rappresenta il 4% di tutti i tumori del tratto gastrointestinale inferiore e l1% di quelli di tutto lapparato digerente [ 1 , 2 ]  . 
la terapia richiede un approccio multidisciplinare ma , al momento , la chirurgia rappresenta solo un trattamento di salvataggio in caso di malattia persistente o localmente recidivante [ 68 ]  . 
 [ 9 , 10 ] hanno ottenuto una risposta completa dopo radiochemioterapia con un elevato tasso di controllo locale in aggiunta al vantaggio di poter preservare la funzionalit dello sntere anale . 
tre studi randomizzati hanno stabilito che la radioterapia associata a chemioterapia concomitante con 5 - uorouracile ( 5 - fu ) e mitomicina c ( mmc ) rappresenta il gold standard nel trattamento del carcinoma anale [ 1113 ] ; comunque , questi studi hanno anche riportato un tasso signicativo di tossicit acuta . 
i pazienti trattati con la radio - chemioterapia curativa hanno presentato tassi di ricaduta locoregionale intorno al 30% con una sopravvivenza libera da malattia ( disease - free survival , dsf ) del 5070% e una sopravvivenza globale ( overall survival , os ) del 6075% . 
laggiunta della chemioterapia ha aumentato la sopravvivenza libera da malattia ma non ha inuito sulla sopravvivenza globale . lobiettivo di questa analisi retrospettiva stato quello di valutare , in termini di sopravvivenza globale , sopravvivenza libera da malattia e sopravvivenza libera da colostomia ( colostomy - free survival , cfs ) , il controllo di malattia dopo radioterapia con o senza chemioterapia concomitante in pazienti con cancro anale trattati in una singola istituzione . 
sono stati anche valutati la tossicit acuta e cronica e i fattori prognostici . materiali e metodi tra maggio 2002 e novembre 2010 , 42 pazienti con cancro anale sono stati trattati presso il nostro dipartimento di radioterapia oncologica con radioterapia associata o meno a chemioterapia concomitante e sono stati inclusi in questa analisi retrospettiva . 
nine patients were treated with radiotherapy alone because of age ( n = 3 ) , comorbidities ( n = 4 ) and hiv status ( n = 1 ) , and one patient refused chemotherapy . 
radiotherapy consisted of external - beam radiation therapy ( ebrt ) of the lower pelvis and nodes , with cranial margin at the bifurcation of the common iliac nodes and lower margin encompassing the anal margin and lower limit of the inguinal nodes . 
different types of regimens were administered as follows : 14 ( 33% ) patients had 5 - fu alone , seven ( 17% ) had 5 - fu and mitomycin c , six ( 14% ) had 5 - fu and cisplatin , four ( 10% ) had capecitabine and mitomycin c and two ( 5% ) had capecitabine and cisplat in two patients , chemotherapy ( one receiving 5 - fu alone and one capecitabine and mitomycin c ) was interrupted due to high - grade gastrointestinal toxicity . 
la valutazione pretrattamento comprendeva lanamnesi del paziente , lesame sico , una tomograa computerizzata ( tc ) total - body , colonscopia e proctoscopia , ecograa transrettale o risonanza magnetica della pelvi . 
da notare che un paziente presentava una storia di sindrome da immunodecienza acquisita ( aids )  . trattamento tutti i pazienti sono stati sottoposti a trattamento radiante con nalit curativa . 
nove pazienti sono stati trattati con radioterapia esclusiva a causa dellet ( n = 3 ) , di comorbidit ( n = 4 ) , dello stato hiv ( n = 1 ) e un paziente ha riutato la chemioterapia . 
il trattamento radioterapico stato effettuato con radioterapia a fasci esterni ( ebrt ) sulla pelvi inferiore e sui linfonodi , col margine craniale posizionato alla biforcazione dei linfonodi iliaci comuni e il margine inferiore che includeva il margine anale e il limite inferiore dei linfonodi inguinali . 
i pazienti sono stati posizionati in posizione supina in modo da evitare disomogeneit al perineo e sono stati utilizzati sistemi di immobilizzazione personalizzati . lo schema di trattamento radioterapico utilizzato pi frequentemente stato di 59 , 4 gy in 33 frazioni con una dose di 1 , 8 gy per frazione . 
in tutti i casi stato effettuato un sovradosaggio sul gross tumor volume ( gtv ) che comprendeva il tumore primitivo ( gtv1 ) o i linfonodi clinicamente positivi ( gtv2 )  . 
il planning target volume ( ptv1 ) comprendeva la pelvi e ha ricevuto 36 gy in 20 frazioni nei pazienti t1 e t2 , n0 seguiti da 23 , 4 gy in 11 frazioni da 1 , 8 gy sul ptv2 che comprendeva il ctv con laggiunta di un margine di 1015 mi pazienti con malattia t3 e / o n + hanno ricevuto 45 gy in 25 frazioni sulla pelvi ( ptv1 ) e 14 , 4 gy in 8 frazioni sul ptv2 che comprendeva il ctv pi un margine di 1015 mtutti i linfonodi positivi hanno ricevuto la dose totale di 59 , 4 gy . trentatre pazienti ( 79% ) sono stati sottoposti a trattamento chemioterapico concomitante durante la terapia radiante . 
i diversi schemi utilizzati sono stati : 5 - uorouracile radiol med ( 2013 ) 118 : 882894 follow - up the rst follow - up evaluation for tumour response was 68 weeks after the end of radiation treatment . 
late toxicities were recorded and assessed on follow - up examination after 90 days from rt completion using rtog late morbidity scoring criteria [ 15 ]  . statistical analysis statistical analysis was performed using statistical package for social science ( spss ) version 13.0. 
cfs was calculated from the rst day of radiation therapy to the day of surgery in patients who needed a permanent colostomy due to tumour persistence / recurrence or therapy - induced gastrointestinal complications . 
a p value < 0.05 was considered statistically signicant . in 14 ( 33% ) pazienti , 5 - uorouracile e mitomicina c in 7 ( 17% ) pazienti , 5 - uorouracile e cisplatino in 6 ( 14% ) pazienti , capecitabina e mitomicina c in 4 ( 10% ) pazienti e capecitabina e cisplatino in 2 ( 5% ) pazienti . 
il trattamento chemioterapico stato interrotto in 2 pazienti ( uno trattato con 5 - uorouracile e uno con capecitabina e mitomicina ) a causa di elevata tossicit gastrointestinale . follow - up la prima valutazione di follow - up della risposta tumorale stata effettuata 68 settimane dopo la ne del trattamento radioterapico . 
le tossicit tardive sono state valutate e registrate allesame di follow - up dopo 90 giorni dal termine della radioterapia utilizzando i criteri di morbilit tardiva rtog [ 15 ]  . analisi statistica tutte le analisi statistiche sono state effettuate utilizzando il software statistical package for social science ( spss ) versione 13.0. 
la sopravvivenza libera da colostomia stata calcolata dal giorno di inizio della radioterapia no al giorno dellintervento chirurgico nei pazienti che necessitavano una colostomia permanente a causa della persistenza / recidiva tumorale o di complicanze gastrointestinali indotte dalla terapia . 
at 68 weeks after radiation therapy with or without chemotherapy , complete response was obtained in 32 of 42 patients ( 76% ) ; eight responsive patients received radiotherapy alone . 
in six patients ( 14% ) , partial response was achieved ; after 46 months , two of them presented complete remission ( total complete response , 81% )  . 
death occurred in eight patients ( 19% ) : four ( 9.5% ) died from tumour and four ( 9.5% ) from intercurrent causes without evidence of disease ( one from late radiochemotherapy complications ; he always had negative biopsies on follow - up )  . 
one patient with stable stage iiib ( t4 n2 ) disease refused salvage surgery and died 8 months after completion of radiotherapy alone because of advanced age ( 86 years )  . 
two ( 5% ) of 42 patients developed distant metastases during follow - up : one presented distant metastases ( abdominal and pelvic lymph nodes ) 36 months and the other distant relapse ( lung , bone and nodes ) 24 months after the conclusion of radiotherapy . 
 six patients ( 14% ) underwent salvage surgery with curative intent : four underwent apr for tumour progression / persistence , one underwent apr for late chemoradiation complications and one underwent colectomy for local recurrence 20 months after completion of radiation treatment . 
le caratteristiche cliniche dei pazienti sono riassunte nella tabella 1 . risposta , follow - up e recidive quarantadue pazienti con cancro anale senza metastasi a distanza hanno ricevuto radioterapia curativa con o senza chemioterapia concomitante . 
a 68 settimane dal trattamento radioterapico + / chemioterapico stata ottenuta una risposta completa in 32 pazienti su 42 ( 76% ) ; otto di questi pazienti avevano ricevuto radioterapia esclusiva . 
in 6 pazienti ( 14% ) , stata ottenuta una risposta parziale ; dopo 46 mesi , due di loro presentavano remissione completa di malattia ( risposta totale completa 81% )  . 
quattro pazienti ( 10% ) presentavano malattia stabile dopo 68 settimane dal termine del trattamento . il follow - up medio e mediano osservato stato di 31 , 5 e 23 , 5 mesi , rispettivamente ( range 398 mesi )  . 
la morte avvenuta in 8 pazienti ( 19% ) ; quattro di questi pazienti ( 9 , 5% ) sono morti a causa del tumore , e quattro ( 9.5% ) per cause intercorrenti senza evidenza di malattia ( uno di questi pazienti morto per complicanze tardive del trattamento radio - chemioterapico , in presenza di biopsie negative al follow - up )  . 
un paziente con malattia stabile ha riutato la chirurgia di salvataggio ed morto 8 mesi dopo il termine della radioterapia ; presentava una malattia di stadio iiib ( t4 n2 ) e aveva ricevuto radioterapia esclusiva a causa dellet avanzata ( 86 anni )  . la persistenza / progressione tumorale si osservata in 5 pazienti ( 12% )  . 
due pazienti ( 5% ) su 42 hanno sviluppato metastasi a distanza durante il follow - up : un paziente ha presentato metastasi a distanza ( linfonodi addominali e pelvici ) dopo 36 mesi , e laltro paziente ha sviluppato metastasi su polmone , ossa e linfonodi 24 mesi dopo il termine della radioterapia . sei pazienti ( 14% ) sono stati sottoposti a chirurgia di salvataggio con intento curativo . 
un paziente ha subito una colectomia per recidiva locale 20 mesi dopo il completamento del trattamento radiante . sopravvivenze e fattori prognostici il tasso di sopravvivenza a 2 anni e 5 anni stato del 78 , 8 e del 72 , 7% , rispettivamente . 
lo stadio globale e la tossicit cutanea sono risultati fattori prognostici postivi solo per la dss ( p = 0 , 028 e p = 0 , 039 , rispettivamente )  . 
allanalisi multivariata , solo lo stadio t stato identicato come fattore prognostico signicativo per los ( p = 0 , 018 ) e la cfs ( p = 0 , 026 )  . 
tutti i pazienti hanno presentato una reazione cutanea durante il trattamento radiante : in 30 pazienti ( 71 , 4% ) stata di grado 12 ; in 11 pazienti ( 26 , 2% ) di grado 3 . 
la tossicit acuta gastrointestinale stata osservata in 26 pazienti ( 62% ) : in 22 ( 52% ) pazienti stata di grado 12 , in 4 pazienti ( 10% ) di grado 34 ( due pazienti hanno presentato diarrea di grado 3 , un paziente ha sviluppato una stola retto - vaginale di grado 4 , un paziente ha presentato disidratazione e diarrea di grado 4 )  . 
le tossicit acute genito - urinarie sono state riportate in 17 pazienti ( 40% ) : in 16 di questi pazienti sono state di grado 12 e una paziente ha sviluppato mucosite vaginale e dolore di grado 3 . 
le tossicit ematologiche si sono vericate durante il trattamento radio - chemioterapico come segue : anemia di grado 12 si vericata in 2 pazienti , mentre non stata osservata alcuna anemia di grado 34 ; leucopenia di grado 12 si vericata in 4 pazienti , leucopenia di grado 34 si vericata in 2 pazienti ; trombocitopenia di grado 1 si vericata in 1 paziente e di grado 4 in un altro paziente . 
2 sopravvivenza libera da malattia ( dfs ) , sopravvivenza libera da colostomia ( cfs ) e sopravvivenza libera da metastasi ( mfs )  . from univariate and multivariate analysis are reported in table 2 . toxicity rates overall therapy was moderately well tolerated . 
acute gastrointestinal toxicities were observed in 26 patients ( 62% ) : 22 ( 52% ) had grade 12 , four ( 10% ) had grade 34 ( two grade 3 diarrhoea , one grade 4 rectovaginal stula , one grade 4 dehydration and diarrhoea )  . 
acute genitourinary toxicities were seen in 17 patients ( 40% ) : 16 with grade 12 and one with grade 3 vaginal mucositis and pahaematological toxicities occurred during radiochemotherapy , as follows : grade 12 anaemia in two patients ( no grade 34 anaemia was observed ) ; grade 12 leukopenia in four , grade 34 leukopenia in two ; thrombocytopenia grade 1 in one and grade 4 in another . 
 eight patients ( 19% ) developed mild to moderate late toxicities : one grade 2 faecal incontinence , one grade 1 bleeding , one grade 1 anal pain , one grade 1 subcutaneous brosis , two rectal discharge ( one grade 1 ; one grade 2 ) and two grade 1 proctitis . 
 fecale di grado 2 , un paziente ha avuto sanguinamento di grado 1 , un paziente ha avuto dolore anale di grado 1 , un paziente ha sviluppato brosi sottocutanea di grado 1 , due pazienti hanno avuto tenesmo rettale ( grado 1 : un paziente ; grado 2 : un paziente ) , e due pazienti hanno avuto proctite di grado 1 . 
un solo paziente ( 2 , 3% ) ha sviluppato tossicit tardiva di grado 4 ( stola retto - vaginale ) ed morto a causa delle complicanze di questo effetto collaterale indotto dal trattamento . 
il tasso di tossicit acuta e tardiva riportato in tabella 3 . discussione il trattamento radio - chemioterapico concomitante rappresenta attualmente lo standard per il cancro anale localizzato con un controllo locale e una sopravvivenza simili a quelli riportati con la chirurgia radicale , permettendo cos di riservare la resezione chirurgica come strategia di salvataggio solo in caso di malattia persistente o di recidiva locale . 
lo studio randomizzato della european organization for research and treatment of cancer ( eortc ) [ 13 ] ha confrontato la radioterapia da sola con il trattamento tabella 2 analisi univariata e multivariata ( p ) pz . 
the united kingdom coordinating committee on cancer research ( ukccr ) randomised trial [ 11 ] comprised 585 patients and compared radiation treatment alone and chemoradiation with 5 - fu and mmc . 
after long - term follow - up , results from the same trial conrmed that lower local control rates and improvements of rfs for anal cancer following chemoradio - chemioterapico con 5 - fu - mmc . 
dopo follow - up a lungo termine , i risultati dallo stesso studio hanno confermato che con il trattamento chemio - radioterapico viene mantenuto un maggior controllo locale e si ottengono miglioramenti nella sopravvivenza libera da recidiva [ 17 ]  . 
 [ 19 ] showed complete response in 78% of patients treated with radiotherapy with concurrent 5 - fu and cisplatthe 5 - year pfs and os were 55% and 69% , respectively . 
 [ 20 ] reported a 5 - year os of 85.7% and a complete response in 93.1% of patients treated with pelvic radiotherapy concurrent to continuous - infusion 5 - fu plus cisplatin for at least 2 cycles . 
 [ 21 ] showed complete remission in 72% of patients treated with radical chemoradiation , with 2 - year dfs , dss , os and cfs of 67% , 87% , 76% and 85% , respectively . 
our current practice is to biopsy all cases suspicious for disease persistence who are likely to benet from salvage treatment , despite the well - known risk of stula associated pazienti trattati con radioterapia pelvica e 5 - uorouracile e cisplatino concomitante in infusione continua per almeno 2 cicli . 
 [ 21 ] ha mostrato remissione completa nel 72% dei pazienti trattati con radiochemioterapia radicale con una dfs , dss , os e cfs a 2 anni del 67 , 87 , 76 e 85% , rispettivamente . 
la nostra pratica comune quella di valutare la biopsia in tutti i casi sospetti per persistenza di malattia che potrebbero beneciare da un trattamento di salvataggio , nonostante il ben noto rischio di indurre la formazione di stole associato a tale procedura . 
in the eortc randomised trial [ 13 ] , patients with no nodal involvement had signicantly higher rates of local control ( p = 0.0017 ) and os ( p = 0.045 ) than did patients with nodal involvement . 
preliminary results were presented from the rtog 98 - 11 trial [ 25 , 26 ] , which randomised 682 patients to receive radiotherapy with concurrent 5 - fu and mmc or induction chemotherapy with 5 - fu and cisplatin followed by radiotherapy with concurrent 5 - fu and cisplatmultivariate analysis demonstrated that clinical node - positive status and tumour size > 5 cm ( p < 0.0001 and p = 0.005 , respectively ) were independent predictive factors for worse dfs . 
no other factors , including sex , age , histological type , chemotherapy and overall treatment time , showed impact on survival or local control . acute side effects reported in our study are similar to the results of other authors [ 31 , 32 ] , with grade 34 radiodermatitis , which occurred in 28.6% patients , being the most frequent toxic event . 
literature reports indicate late toxicity rates from 4% to 50% , depending on followup length , radiotherapy technique , dose per fraction and combination of chemotherapeutic agents [ 33 ]  . 
in one patient ( 2.3% ) , rectovaginal stula led to death ; this was the only death attributable to treatment - related complications . in letteratura , pochi studi hanno analizzato limpatto dei fattori prognostici sulla sopravvivenza e sul controllo locoregionale in pazienti con cancro anale . 
alcuni studi hanno identicato la dimensione del tumore e lestensione del coinvolgimento linfonodale come i pi importanti fattori prognostici per il cancro anale [ 2224 ] e il nostro studio ha confermato questi dati . 
nello studio randomizzato eortc [ 13 ] , i pazienti senza coinvolgimento linfonodale avevano dei tassi signicativamente pi alti di controllo locale ( p = 0 , 0017 ) e di sopravvivenza globale ( p = 0 , 045 ) rispetto ai pazienti con coinvolgimento linfonodale . 
sono stati presentati i risultati preliminari dello studio rtog 98 - 11 [ 25 , 26 ] , in cui 682 pazienti sono stati randomizzati a ricevere radioterapia con 5 - fu e mitomicina c concomitante , o chemioterapia di induzione con 5 - fu e cisplatino seguita da radioterapia associata a 5 - fu e cisplatino . 
lanalisi multivariata ha mostrato che il coinvolgimento linfonodale e le dimensioni del tumore > 5 cm ( p < 0 , 0001 e p = 0 , 005 , rispettivamente ) erano fattori predittivi indipendenti per una peggiore sopravvivenza libera da malattia . 
 allanalisi univariata , lo stadio t era associato in maniera signicativa con los , dss , cfs e dfs , mentre lo stadio n ha mostrato correlazione signicativa solo con la dss . 
 nessun altro fattore , incluso il sesso , let , il tipo istologico , la chemioterapia e la durata totale del trattamento , ha mostrato impatto sulla sopravvivenza o sul controllo locale . gli effetti collaterali acuti riportati nel nostro studio sono simili ai risultati di altri autori [ 31 , 32 ]  . 
la letteratura riporta tassi di tossicit tardiva compresi tra il 4 e il 50% a seconda della durata del follow - up , della tecnica radioterapica , della dose per frazione e della combinazione di agenti chemioterapici [ 33 ]  . 
questa stata lunica morte attribuibile a complicanze correlate al trattamento . radiol med ( 2013 ) 118 : 882894 conclusions conclusioni in conclusion , we acknowledge that our study is limited because of its retrospective design and consequential inherent biases , and that it comprised a small number of patients and a short follow - up . 
future research should also focus on developing new cytotoxic agents or targeted drugs . in conclusione , siamo consapevoli che la nostra serie limitata , in quanto si tratta di uno studio retrospettivo e quindi ne presenta i bias inerenti , a causa del numero ridotto di pazienti e del breve follow - up . 
comunque , i nostri dati supportano che la radio - chemioterapia combinata nel trattamento del cancro anale fattibile e pu portare a beneci in termini di sopravvivenza e con un tasso accettabile di effetti collaterali . 
 ulteriori studi , soprattutto studi prospettici e randomizzati di fase iii , sono necessari per valutare la dose ottimale di irradiazione utile per ottenere un adeguato controllo locale e per denire il miglior trattamento combinato . 
this was a prospective study of 28 consecutive patients with multiple myeloma ( 19 men , nine women ; age range , 5173 years ; mean age , 60 years ) who underwent wb - mdct and conventional radiography ( cr ) of the skeleton . 
we conclude that wb - mdct has an impact on treatment planning and prognosis in patients with multiple myeloma , as it has high rate of detecting cortical and medullary bone lesions , spinal fracture and extraosseous riassunto obiettivo . 
in questo studio prospettico sono stati arruolati consecutivamente 28 pazienti ( 19 maschi , 9 femmine ; et compresa tra 5173 anni ; et media , 60 anni ) che sono stati sottoposti a tcms total - body e radiograa dello scheletro . 
 la tcms total - body ha determinato un aumento dello stadio 14 pazienti , con una differenza signicativa nella stadiazione ( p = 0 , 002 ) tra tcms total - body e rc . 
il coinvolgimento midollare , sia focale ( n = 6 ) che diffuso ( n = 3 ) ha mostrato una correlazione positiva con il punteggio complessivo ( r = 0 , 790 ) e lo stadio di malattia ( r = 0 , 618 )  . 
la tcms total - body incide nella pianicazione del trattamento e nella prognosi dei pazienti con mieloma multiplo , avendo un alto grado di individuazione delle lesioni ossee corticali e midollari , delle lesioni spinali e di quelle extraossee . 
queste informazioni possono determinare una variazione del piano terapeutico nel mieloma multiplo , in seguito ad un aumento dello stadio di malattia e alla individuazione di fratture spinali o lesioni spinali extraossee . parole chiave mieloma osso colonna vertebrale tc total - body radiograa stadiazione introduction multiple myeloma is the most common primary bone malignancy and accounts for 10% of all haematological malignancies and 1% of all cancers . 
patients diagnosed as having stage i multiple myeloma require conservative therapy , whereas patients at stage ii and iii may benet from high - dose chemotherapy and stem - cell transplant , depending on eligibility . 
additional therapy in the form of radiotherapy and vertebroplasty are indicated in the presence of paraspinal mass and compressed vertebra , respectively [ 16 ]  . different imaging modalities have been used to stage multiple myeloma : conventional skeletal survey and low - dose whole - body radiography has relatively high false - negative rates ( 3070% ) , leading to understaging [ 10 ]  . 
fluorodeoxyglucose positron emission tomography ( [ 18f ] fdg - pet ) and 99mtc - sestamibi scintigraphy may be associated with false results due to infection or inammation and have limited spatial resolution that hinders the detection of small lesions [ 13 , 14 ]  . 
technological advances have enabled the application of whole - body computed tomography ( wbct ) , allowing examination of the entire body to diagnose the spread of disease in the appendicular skeleton . 
wb - mdct enables high - resolution imaging of cortical and trabecular bone within a short acquisition time ( 1 min ) with thin - slice collimation and multiplanar reconstructions ( mpr )  . 
 materials and methods this prospective study comprised 28 consecutive patients ( 19 men , nine women ; age range , 5173 years ; mean age , 60 years ) with newly diagnosed , untreated multiple myeloma . 
 all patients were examined with a 64 - mdct scanner ( brilliance 64 , philips medical systems , cleveland , oh , usa ) with the patients lying supine with arms along the body . 
scanning extended from the top of the skull to the knee joints , with an average scan length of 150 ca convolution kernel ( b 70f ) for bone and ( b 35f ) soft tissue were used . 
 all images were reconstructed in overlapping technique in the axial plane with an effective slice thickness of 2 mm and a reconstruction increment of 1 m mprs in the sagittal and coronal planes with a section thickness of 4 mm were reconstructed . 
radiation dose was calculated directly by the machine . image analysis was performed by two radiologists ( ea , nt ) with 10 and 2 years experience in ct scan imaging , respectively . 
the skeleton was divided into six anatomical regions : skull , vertebral column ( spine ) , pelvic bones , thoracic cage ( ribs and sternum ) and upper and lower extremities . 
 each region was scored from 03 ( 0 = normal , 1 = 14 lesions , 2 = 520 lesions , 3 20 lesions / diffuse disease ) to correspond with the new durie - salmon plus staging system [ 26 ]  . 
 hyperattenuating medullary lesions , either focal ( welldened nodular mass < 3 cm ) or diffuse ( diffuse mass involving the bony canal ) inltrations of the femoral , tibial and humeral bony canal , as well as of the pelvic bones , were assessed . 
to differentiate marrow inltration from physiological residual haematopoietic red marrow , a threshold of 0 hu was set , considering all lesions lying above it as pathological [ 21 ]  . 
students t test was carried out to study the difference between two groups , and one - way analysis of variance ( anova ) was used to test the difference between more than two groups . 
correlation coefcient ( r ) and p value were calculated ; p value was considered signicant if 0.05 at a condence interval ( ci ) of 95% . results wb - mdct detected more bony lesions than did cr ( table 1 )  . 
the compressed vertebral body was in the dorsal ( n = 1 ) and lumbar ( n = 3 ) regions and showed decreased height with no adjacent soft tissue mass . 
extraosseous lesions appeared only at wb - mdct and were in the form of pleural effusion ( n = 3 ) , pulmonary inltrates ( n = 2 ) , hepatic lesions ( n = 2 ) , lymphadenopathy ( n = 1 ) and paraand intraspinal soft tissue mass with spinal cord compression ( n = 2 )  . 
the higher detection rate of wb - mdct was more evident in the vertebral body and thoracic cage , whereas the difference between the two modalities was much lower in pelvic bones and upper and lower extremities . 
this may be explained by the fact that bone marrow inltration of the axial skeleton leads to early bone destruction in myeloma because of the dense trabecular architecture of the vertebral bodies and pelvic bones . 
in contrast , the long bony canals of the appendicular skeleton lack trabecular parts , so that inltration by myeloma cells can reach large dimensions before causing bone destruction and becoming visible at cr [ 14 ]  . treatment regimens for multiple myeloma differ depending primarily on disease stage and presence of extraosseous lesions and spinal fracture . 
patients diagnosed with stage i without any detectable bone involvement do not require therapy , whereas patients in stage ii and iii prot from therapy in terms of quality of life and survival [ 37 ]  . 
in this study , mdct upstaged 7 / 28 ( 25% ) patients : one from stage i to stage iii and six from stage i to stage ii , with subsequent changes in treatment planning . 
seven patients were upstaged from stage ii to stage iii , which did not affect treatment planning . frequency of medullary lesions in the femoral , humeral and pelvic bones of myeloma patients is high ( 3446% )  . 
there was a positive correlation between medullary lesions and overall myeloma score and stage . pathological fracture is seen within the rst year ( 45% ) of diagnosis and during the course ( 65% ) of disease [ 27 ]  . 
an important advantage of mdct over cr is the delineation of extraosseous ndings , which can lead to a change in disease stage or therapy regimen [ 19 , 30 , 31 ]  . 
 in this study , extraosseous lesions were detected in seven ( 25% ) patients , two of whom had paraspinal and intraspinal soft tissue masses on mdct , leading to mr imaging of the spine and urgent radiotherapy . 
using a low - dose protocol , the radiation dose is slightly higher than that of a skeletal survey with x - rays and varies between 3 and 4 msv depending on patient weight [ 14 ]  . 
 tcms total - body secondo ricostruzioni sagittali a e coronali b che mostrano numerose lesioni osteolitiche coinvolgenti sterno , vertebre , ossa pelviche e femori prossimali . 804 radiol med ( 2013 ) 118 : 799805 fig . 
axial multidetector computed tomography ( mdct ) image of proximal femora showing hyperdensity ( 95 hu ) in the medullary cavity of the left femur and normal density in the medullary cavity of the right femur ( 40hu )  . 
immagine assiale tcms dei femori prossimali che evidenzia uniperindensit ( 95 hu ) della midollare del femore di sinistra e normale densit della midollare del femore di destra ( 40hu ) tion of fdg - pet alone , as it combines the high contrast resolution ( sensitivity ) of pet with the high spatial resolution ( anatomy ) of ct . 
fdg - pet / ct can signicantly contribute to an accurate wb evaluation of multiple myeloma patients , as fdg - pet uptake indicates active myeloma and ct shows bone destruction . 
la scansione assiale mostra multiple lesioni litiche coinvolgenti la colonna , le coste e le scapole , con associata massa dei tessuti molli intraspinali e paraspinali . conclusions there are several limitations to this study . 
first , it involved the use of mdct alone , whereas combined imaging modalities such as low - dose wb - mdct and pet may be valuable fdg - pet / ct overcomes the low spatial resoluwe conclude that wb - mdct has an impact on treatment planning and prognosis in patients with multiple myeloma as it has a high detection rate for cortical and medullary bony lesions , spinal fractures and extraosseous lesions . 
natale18 1dipartimento di scienze cliniche applicate e biotecnologiche , universit di laquila , italy 2cardio - vascular imaging unit , giovanni xxiii hospital , monastier di treviso ( tv ) , italy and erasmus medical center university , rotterdam , the netherlands 3dipartimento di scienze radiologiche , oncologiche e anatomo - patologiche , universit sapienza di roma , italy 4istituto di radiologia , diagnostica e interventistica , universit a avogadro , novara , italy 5dipartimento di radiodiagnostica , apss di trento , trento , italy 6department of radiology and experimental imaging center , san raffaele hospital and vita - salute san raffaele university , milan , italy 7dipartimento di radiologia ospedale san gennaro asl napoli 1 centro , napoli , italy 8uoc radiologia , ospedale fatebenefratelli isola tiberina , roma , italy 9istituto di radiologia , universit di torino , italy 10us radiologia cardiovascolare , dipartimento cardiotoracovascolare , policlinico s . 
orsola , bologna , italy 11dipartimento di radiologia , universit degli studi di ancona , ancona , italy 12sezione di scienze radiologiche , dipartimento di biopatologia e biotecnologie mediche e forensi , aoup paolo giaccone , universit degli studi di palermo , italy 13radiologia 1 , dai servizi diagnostici e per immagine , azienda ospedaliero - universitaria , policlinico di modena , italy 14us radiologia cardiovascolare , dipartimento cardiotoracovascolare , policlinico s . 
gemelli hospital , catholic university , rome , italy 16dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e terapia radiante della fondazione policlinico universitario tor vergata roma , italy 17servizio di radiologia , dipartimento di scienze biomediche per la salute , universit degli studi di milano , irccs policlinico san donato , san donato milanese , milano , italy 18mri dept . , catholic university of sacred heart , c / o centro oncologico fiorentino , sesto fiorentino ( fi ) , italy correspondence to : e . 
de roos , lumc - leiden university medical center leiden , the netherlands received : 17 may 2012 / accepted : 6 june 2012 / published online : 29 november 2012 springer - verlag 2012 abstract cardiac magnetic resonance ( cmr ) is considered an useful method in the evaluation of many cardiac disorders . 
 synthetically we describe different cardiac disorders and express for each one a classication , i to iv , depending on the signicance of diagnostic information expected . riassunto la risonanza magnetica cardiaca ( rmc ) considerata oggi utile nella valutazione di numerose cardiopatie . 
in modo sintetico si descrivono le differenti cardiopatie e si esprime per ciascuna una classe di indicazione , da i a iv , in funzione della rilevanza delle informazioni diagnostiche aspettate . radiol med ( 2013 ) 118 : 752798 keywords heart magnetic resonance parole chiave cuore risonanza magnetica introduction introduzione continuous improvements both in hardware and software , initiated in the early 1990s , have made cardiac magnetic resonance ( cmr ) a particularly interesting noninvasive imaging modality to diagnose numerous cardiac disorders . cardiology and radiology scientic societies have , therefore , spent considerable effort dening guidelines , consensus reports , and appropriateness criteria , based on the opinion of experts and evidence published in literature . two main documents have guided the clinical application of cmr in recent years : the consensus panel report of 2004 , published in the journal of cardiovascular magnetic resonance and in the european heart journal [ 1 ] , and the document on appropriateness criteria for cardiac computed tomography and magnetic resonance , published in 2006 [ 2 ] and revised in 2010 [ 3 ]  . 
the purpose of the two documents was different : the rst established the diagnostic relevance of cmr in the study of congenital and acquired cardiac disorders with regard to other diagnostic modalities , while the latter dened the appropriateness of indications , identifying numerous clinical scenarios in the context of various disorders . the aim of this document is to reconcile these two approaches , providing the imaging diagnostician with an update of both the general indications and the specic appropriateness for the clinical use of cmr in the different cardiac disorders . in light of this , we have maintained the structure in classes of indications , as used in the consensus panel report of 2004 . class i : provides clinically relevant information and is usually appropriate ; may be used as a rst - line imaging technique ; usually supported by substantial literature . class ii : provides clinically relevant information and is frequently useful ; other techniques may provide similar information ; supported by limited literature . class iii : provides clinically relevant information but is infrequently used because information from other imaging techniques is usually adequate . class inv : potentially useful , but still investigational . technical aspects requisites lo sviluppo tecnologico , hardware e software , delle apparecchiature di risonanza magnetica avvenuto nellultimo decennio ha reso la risonanza magnetica cardiaca ( rmc ) una tecnica di imaging non invasivo particolarmente utile nella denizione e nellinquadramento diagnostico di molte cardiopatie . le societ scientiche cardiologiche e radiologiche hanno pertanto compiuto un importante sforzo per denire linee di indirizzo , consensi e criteri di appropriatezza , basati dapprima su pareri di esperti e poi sui dati dellevidenza dettati dalla letteratura . in rmc , due sono i documenti principali sui quali ci si basati nella pratica clinica degli ultimi anni : il consensus panel report del 2004 , pubblicato sul journal of cardio vascular magnetic resonance e sulleuropean heart journal [ 1 ] , e il documento sui criteri di appropriatez za di tc e rm , pubblicato nel 2006 [ 2 ] e revisionato nel 2010 [ 3 ]  . 
i documenti hanno due obiettivi differenti in quanto il primo stabilisce quando la rm pu essere in dicata , fornendo elementi diagnostici pi o meno rilevan ti in base alla relativa patologia cardiaca , mentre il secondo denisce lappropriatezza dellindicazione congurando molteplici scenari clinici nellambito delle varie patologie . lo scopo di questo documento di conciliare , sulla base della nostra esperienza , le due impostazioni , fornendo al diagnosta per immagini sia lindicazione generale , che lappropriatezza specica dello scenario clinico nelle diverse patologie cardiache . in considerazione di ci , abbiamo mantenuto limpostazione in classi di indicazioni del consensus panel report del 2004 : classe i : fornisce informazioni clinicamente rilevanti ed solitamente appropriata ; pu essere utilizzata come indagine di prima istanza ; supportata da cospicui dati della letteratura . classe ii : fornisce informazioni clinicamente rilevanti ed spesso utile ; altre metodiche possono fornire analoghe informazioni ; supportata da dati della letteratura limitati . classe iii : fornisce informazioni clinicamente rilevanti , ma utilizzata poco frequentemente perch le informazioni ottenute con altre metodiche sono solitamente adeguate . classe inv : potenzialmente utile ma ancora applicata a cardiac mri is commonly performed with 1.5 tesla eld strength magnets . 
in general , images acquired with higher eld strengths together with dedicated multichannel phased - array coils provide a higher signal to noise ratio , useful for producing images with smaller voxels and consequently higher spatial resolution . 
however , increasing eld strength augments motion and susceptibility artefacts , especially at the thoracic level . high - eld gradients and slow rates are required in order to allow fast imaging . 
parallel imaging techniques introduced in the last decade can shorten cmr examinations , halving the acquisition time . cardiac gating is mandatory for all acquisitions and is obtained by means of vectorcardiogram , now considered the choice modality to synchronise radiofrequency pulses with the cardiac cycle , better than electrocardiographic gating . respiratory movements must be controlled ; breath - hold sequences have almost completely replaced free breathing and conventional respiratory - gated acquisitions . 
nevertheless , navigator echo techniques have been developed in order to allow high - quality 3d imaging . different sequences provide various informations : morphology , function , ow and tissue characterization . sequences morphology both black - blood and bright - blood sequences may be useful for morphological evaluation . 
they are used to obtain a morphological evaluation of the heart and great vessels , providing optimal delineation of fat ( bright signal ) , cardiac muscle ( medium signal ) , pericardium ( dark signal ) and blood ( dark signal )  . 
a development of conventional spin echo and fast spin echo is breath - hold double inversion recovery multi - shot fast spin echo ( ir - fse ) , which allows better owing blood signal nulling , without any respiratory artefacts . 
a development of conventional gradient echo sequence is the steady - state free precession ( ssfp ) technique , which allows higher contrast to noise and higher spatial resolution , and is considered the technique of choice among the bright - blood sequences . function bright - blood sequences are used to evaluate cardiac funaspetti tecnici requisiti la risonanza magnetica cardiaca ( rmc ) generalmente eseguita mediante magneti da 1 , 5 tesla . 
in generale , immagini acquisite con pi alto campo magnetico e con bobine multicanale dedicate producono un migliore rapporto segnale / rumore utile a generare immagini con voxel pi piccoli e , conseguentemente , con maggiore risoluzione spaziale . 
comunque , incrementando lintensit di campo aumentano gli artefatti da movimento e da suscettibilit , specialmente a livello toracico . sono necessari elevati gradienti e slow rate per produrre acquisizioni veloci . 
la tecnica di imaging parallela introdotta nellultima decade pu ridurre il tempo di acquisizione , dimezzandolo . la sincronizzazione cardiaca necessaria per tutte le acquisizioni del cuore ed ottenuta con vectorcardiograa , considerata oggi la modalit di scelta per sincronizzare gli impulsi di radiofrequenza con il ciclo cardiaco , superiore alla sincronizzazione elettrocardiograca . i movimenti respiratori possono essere controllati ; sequenze a respiro sospeso hanno rimpiazzato quasi completamente le acquisizioni convenzionali a respiro libero . 
 tuttavia , la tecnica navigator echo stata sviluppata per ottenere elevata qualit nellimaging 3d . sequenze differenti producono informazioni diverse : morfologia , funzione , usso e caratterizzazione tissutale . sequenze morfologia sequenze a sangue nero e sequenze a sangue bianco possono essere utili nella valutazione morfologica . 
sono utilizzate per ottenere una valutazione morfologica del cuore e dei grossi vasi , producendo unottima delineazione del grasso ( segnale brillante ) , del muscolo cardiaco ( segnale intermedio ) , del pericardio e del sangue ( segnale scuro e assente )  . 
unevoluzione delle convenzionali sequenze spin echo e fast spin echo la double inversion recovery multi - shoth fast spin echo ( ir - fse ) , che produce annullamento del segnale del usso ematico senza alcun artefatto respiratorio . le sequenze a sangue chiaro producono alta intensit di segnale dal usso ematico rispetto al muscolo cardiaco , che appare di segnale intermedio . 
generally 2530 cardiac phases per each slice are acquired ; nine to twelve 8 mmthick contiguous slices are generally required to encompass the left ventricle in short axis , allowing global assessment of systolic function parameters of both ventricles with high reproducibility . 
 single breath - hold 3d acquisition is now available , to cover the entire heart in a single breath - hold of 2030 seconds . flow to assess and quantify blood ow , phase - contrast sequences are used ; these sequences give two sets of images : an amplitude or module set , similar to conventional gradient echo , and another one dened as phase images where the signal is given only by owing spins , while stationary spins are nulled . 
images can be acquired in 3d or 2d mode : 3d acquisitions are used for angiographic imaging , while 2d images are acquired in cine technique and are aimed at velocity and ow measurements . tissue characterisation non - contrast - enhanced sequences and contrast - enhanced sequences ( perfusion and delayed enhancement ) are used . 
 non - contrast - enhanced sequences black - blood sequences : these provide differentiation of fat ( bright signal ) , cardiac muscle ( medium signal ) , pericardium ( dark signal ) and owing blood ( no signal )  . 
fat saturated acquisitions are available to distinguish bright signal due fat or haemorrhage . oedema - weighted sequences : fat - saturated double inversion recovery fast spin echo with long echo time ( 80100 ms ) or triple inversion recovery fast spin echo sequences are useful to identify the presence of oedema ( bright signal ) within the myocardial wall ( low signal )  . 
different readout techniques can be used zione morfologica di numerose strutture cardiache . unevoluzione della sequenza gradient echo la tecnica steady state free precession ( ssfp ) , che mostra pi elevato contrasto / rumore e risoluzione spaziale ed considerata la tecnica di scelta tra le sequenze a sangue bianco . funzione le sequenze a sangue bianco sono utilizzate per valutare la funzione cardiaca . 
 generalmente si acquisiscono 2530 fasi cardiache per ogni strato : sono generalmente necessari da 9 a 12 strati contigui , di spessore di 8 mm , per acquisire il ventricolo sinistro in asse corto , rendendo possibile la valutazione dei parametri di funzione sistolica di entrambi i ventricoli con elevata riproducibilit . 
attualmente , disponibile anche una singola sequenza 3d in grado di coprire lintero cuore in una singola apnea di 2030 secondi . flusso per valutare e quanticare il usso ematico si utilizzano sequenze phase contrast ; queste producono due set di immagini , un set di ampiezza o modulo , simile alle sequenze convenzionali gradient - echo , e un altro denito come immagini di fase dove il segnale prodotto solamente dagli spin in movimento , mentre gli spin stazionari vengono annullati . 
le immagini possono essere acquisite in 3d o 2d : le acquisizioni 3d si impiegano per limaging angiograco , mentre quelle 2d si acquisiscono in tecnica cine e sono indirizzate alla misure di usso . caratterizzazione tessutale si utilizzano sequenze non contrastograche e sequenze contrastograche ( perfusione e delayed enhancement )  . sequenze non contrastograche sequenze a sangue nero : permettono la differenziazione del grasso ( segnale elevato ) , del muscolo cardiaco ( segnale intermedio ) , del pericardio ( segnale basso ) e del usso ematico ( assenza di segnale )  . 
sono disponibili sequenze con saturazione del grasso , utili a distinguere lelevato segnale dovuto al grasso o a emorragia . sequenze pesate per ledema : sequenze double inversion recovery fast spin echo con lungo te ( 80100 ms ) o sequenze triple inversion recovery fast spin echo sono utili a identicare la presenza di edema ( segnale elevato ) nella parete miocardica ( segnale basso )  . 
inoltre , 756 radiol med ( 2013 ) 118 : 752798 ( fast gradient echo , hybrid echo - planar technique , steady - state free precession ) after a saturation recovery pulse to null the blood pool and myocardium signal . early and delayed enhanced sequences : these are used to detect the presence of necrosis or brosis at the myocardial walls . 
inversion recovery fast gradient echo ( irfgre ) are commonly used ; the inversion recovery prepulse is used to null the signal intensity of non - enhanced myocardium , while the evidence of enhanced areas within the myocardium 10 to 20 minutes after contrastmedium injection is related to myocardial cell death or scarring . 
early acquisition ( 23 minutes after contrast injection ) is useful to assess microvascular damage in acute myocardial infarction . finally , conventional spin echo or fast spin echo sequences can be used to assess and quantify contrast enhancement in myocardial inammation . congenital heart diseases advantages and limitations one of the strongest indications for cmr imaging is the study of congenital heart diseases , both because of the accurate morphological and functional evaluation that the method can provide , even in the presence of complex congenital anomalies , and because of its non - invasiveness , which is a fundamental advantage when studying paediatric or juvenile patients and patients requiring repeated follow - up examinations over time [ 46 ]  . general indications routine clinical use of cmr in newborns and in small children is hampered by the need for anaesthesia [ 7 , 8 ]  . 
for that reason , cmr is limited to those in whom cardiac ultrasound does not provide substantial information , such as patients with an inadequate acoustic window ( extracardiac anomalies ) or for assessment of complex forms of congenital heart disease [ 9 ]  . 
on the contrary , in older children , in adults , and in subjects who have undergone surgery , the quality of echocardiography may be limited by anatomical factors or by the sequelae of the surgery . 
for these reasons cmr has become a rst - level investigation for numerous indications and especially in the follow - up of surgical patients and in the evaluation of complex anomalies [ 10 ]  . 
cardiac computed tomography ( ct ) is used instead of cmr in only a few specic clinical situations ( claustrophobia , patients with a permanent pace - maker or debrillator , presence of ferromagnetic metal materials such as coils or other devices )  . 
however , the combination of low - radiation protocols and ultrafast scanning makes ct attractive to study possono essere facilmente identicate lesioni di elevato segnale ( ad esempio , angiomi cardiaci )  . accumulo di ferro : sequenze a sangue scuro o a sangue bianco t2 * fast gradient sono utili a identicare e quanticare laccumulo cardiaco di ferro attraverso lanalisi della riduzione del rilassamento t2 *  . sequenze contrastograche sequenze di perfusione ( rst pass ) : vengono utilizzate sequenze fast gradient echo t1 pesate ; si acquisiscono almeno tre strati in asse corto ( basale , intermedio , apicale ) ad ogni battito cardiaco durante la somministrazione di un bolo di un chelato di gadolinio . 
possono essere utilizzate differenti tecniche ( fast gradient , hybrid echoplanar , steady - state free precession ) dopo un impulso di saturazione utile ad annullare il segnale del sangue e del miocardio . delayed end early enhanced sequences : sono utilizzate per identicare la presenza di necrosi o brosi a livello della parete miocardica . 
comunemente si utilizzano inversion recovery fast gradient echo ( ir - fgre ) ; il preimpulso dinversione utilizzato per annullare il segnale del miocardio non contrastato , mentre levidenza di aree con accumulo di contrasto nel miocardio 1020 minuti dopo liniezione del mezzo di contrasto correlato a necrosi cellulare o alla presenza di cicatrice . 
lacquisizione precoce ( 23 minuti dopo liniezione del mezzo di contrasto ) utile per valutare il danno microvascolare nellinfarto miocardico acuto . inne , possono essere utilizzate sequenze spin echo convenzionali o fast spin echo per valutare e quanticare lenhancement contrastograco nellinammazione miocardica . cardiopatie congenite vantaggi e limiti lo studio delle cardiopatie congenite ( cc ) rappresenta una delle indicazioni cliniche pi solide della rmc , sia per laccurata valutazione morfo - funzionale che la metodica in grado di fornire , anche in presenza di anomalie congenite pi complesse , che per la sua non invasivit , che rappresenta vantaggio fondamentale quando si studiano pazienti in una fascia di et pediatrica o giovanile e che necessitano di ripetuti follow - up nel tempo [ 46 ]  . indicazioni generali limpiego clinico della rmc nei reparti di terapia intensiva , in et neonatale e della prima infanzia , reso difcoltoso dalla necessit dellanestesia [ 7 , 8 ]  . 
 cmr is particularly accurate in identifying malformations and assessing the systemic venous return [ 14 ]  . solamente nei casi dinadeguata nestra acustica ( anomalie extracardiache ) o per specici quesiti anatomici o funzionali nelle cc pi complesse [ 9 ]  . 
pertanto la rmc acquista valore di indagine di primo livello in numerose indicazioni e , in particolare , nel follow - up dei pazienti operati e nella valutazione delle anomalie complesse [ 10 ]  . 
solamente in poche situazioni cliniche speciche ( claustrofobia , pazienti portatori di debrillatore o pace - maker non temporaneo , presenza di materiale metallico ferromagnetico come coil o altri device ) la tc sostituisce la rm . 
comunque , i protocolli a bassa dose di radiazione e le acquiszioni ultraveloci rendono la tc attraente per studiare pazienti giovani , ovviando alla necessit di procedure invasive . lapplicazione della rm in et fetale , inne , per quanto attraente , ancora oggi limitata allambito sperimentale ( tabella 1 ) [ 11 ]  . 758 radiol med ( 2013 ) 118 : 752798 atrial anomalies and anomalies of pulmonary veins indicazioni speciche per le cardiopatie congenite cmr is very reliable in the diagnosis and overall assessment of atrial septal defects and correlates very well with transoesophageal echocardiography ( gold standard for the study of morphology and measurement of atrial septum defects [ 15 , 16 ] ) and for the invasive quantication of shunts [ 17 ]  . however , from a clinical point of view cmr may provide limited additional information to echocardiography in describing isolated atrial septal defects , such as ostium primum and ostium secundu cmr is of great help in quantifying the degree of right ventricular volume overload and calculating the severity of the intracardiac shunt . 
additionally , in cases of atypical defects , in particular sinus venosus atrial septal defects , and for assessment of abnormal pulmonary venous return , cmr is unquestionably the reference technique [ 18 , 19 ]  . 
moreover , cmr is indicated in patients with isolated right ventricular dilatation in order to exclude , among other causes , partial anomalous pulmonary venous return or an atrial septal defect [ 20 ]  . 
cmr is of limited clinical utility in the evaluation of foramen ovale , in which this imaging technique is inferior to both transoesophageal and transthoracic echocardiography [ 21 ]  . anomalies of atrio - ventricular connections , atrio - ventricular valves , and ventricles cmr is useful in the study of discordant atrio - ventricular ( av ) connections , valve atresia , av defects [ 22 ] , and ventricular septal defects [ 23 ] , in order to identify the ventricular septal defects associated with complex anomalies [ 24 , 25 ] and , in particular , recognising venous return , systemicpulmonary collaterals [ 26 ] , and biventricular function [ 27 ]  . 
 among the av anomalies , in ebsteins disease , cmr may give additional information to the one provided by echocardiography ( associated lesions , ventricular brosis ) and may be indicated in the follow - up of right ventricular function [ 28 ]  . anomalies of the great vessels cmr is an extremely accurate method for studying all the diseases of the aorta . 
mr angiography is useful for studying anomalies of the aortic arch [ 29 ]  . aortic coarctation : in aortic coarctation , location and severity of narrowing are determined accurately by cmr [ 30 ] , while ow sequences are used to measure the severity of the stenosis by calculating ow velocities and the transisthmic gradient . 
the multiplanar orientation of the mr ow sequences overcomes the limitations of echocardiography , due to the tortuosity of the aorta and sequeanomalie del situs e delle vene sistemiche lanalisi del situs ( solitus , inversus , ambiguus ) e lanatomia sequenziale , che il cardine sistematico di approccio alle cc , sono facilmente ottenibili con lecocardiograa ma , in presenza di anomalie complesse associate particolarmente frequenti nei siti ambigui ( eterotassie ) [ 12 ] , la rmc superiore allecocardiograa [ 13 ] , soprattutto per la multiplanariet e lelevato campo di vista che le consentono di visualizzare in poche immagini linsieme delle strutture toracoaddominali . 
la rmc particolarmente accurata nellidenticare le malformazioni e i ritorni venosi sistemici [ 14 ] ed frequentemente utile nella valutazione pre - chirurgica . anomalie atriali e delle vene polmonari la rmc molto afdabile nella diagnosi e nella valutazione globale dei difetti interatriali ( dia ) , correla ottimamente con lecograa transesofagea ( ecote ) , gold standard per lo studio della morfologia del setto interatriale [ 15 ] , nella misurazione dei dia [ 16 ] e con il cateterismo cardiaco nella quanticazione degli shunt [ 17 ]  . 
 nonostante ci , la rmc clinicamente aggiunge limitate informazioni addizionali allecograa nei dia isolati tipo ostium primum e secundunei difetti atipici , invece , in particolare il dia tipo seno venoso , la rmc di grande aiuto nel quanticare il grado del sovraccarico volumetrico destro e nel calcolare la gravit degli shunt cardiaci . 
in caso di difetti atipici , in particolare nei difetti atriali tipo seno venoso e per la valutazione del ritorno venoso polmonare anomalo , la rmc indubbiamente la tecnica di riferimento [ 18 , 19 ]  . 
 inoltre , la rmc indicata nei pazienti con dilatazione isolata del ventricolo destro per escludere , tra le altre cause , un anomalo parziale ritorno venoso polmonare ( rvpap ) o un dia [ 20 ]  . 
di scarsa utilit clinica la valutazione del forame ovale , dove lrmc inferiore allecote e allecograa transtoracica [ 21 ]  . anomalie delle connessioni atrio - ventricolari , delle valvole atrio - ventricolari e dei ventricoli nello studio delle connessioni atrio - ventricolari ( av ) discordanti , delle atresie valvolari , dei difetti av [ 22 ] e interventricolari ( div ) [ 23 ] , la rmc utile nellidenticare i div associati ad anomalie complesse [ 24 , 25 ] e , in particolare , per lidenticazione dei ritorni venosi , delle collaterali sistemico - polmonari [ 26 ] e della funzione biventricolare [ 27 ]  . 
tra le anomalie av , nella malattia di ebstein la rmc pu fornire informazioni aggiuntive allecocardiograa ( lesioni associate , brosi ventricolare ) ed essere indicata nel follow - up della funzione ventricolare destra [ 28 ]  . radiol med ( 2013 ) 118 : 752798 lae of surgery . 
the only limitation of cmr may be in evaluating aortic stents , because the artefacts from stent struts may impede the visualisation of phenomena such as stent restenosis or fractures . 
 patent ductus arteriosus ( botallos duct ) : cmr is of greater value when the patent ductus arteriosus is associated with complex congenital anomalies [ 33 ] , in adults , in whom the open duct may be more difcult to identify by echocardiography , and , nally , in pre - operative assessment , which requires precise quantication of the shunt . pulmonary arteries : cmr is very accurate in the study of pulmonary arteries and their main branches . 
determining the morphology of these vessels is an essential part of the pre - operative and post - operative assessments of numerous congenital heart diseases , such as tetralogy of fallot , pulmonary atresia , and univentricular heart [ 34 ]  . 
mr angiography is the main technique for evaluating the pulmonary arteries , measuring their dimensions , identifying any stenoses , but also for a precise denition of the systemic - pulmonary collaterals , outcomes of unifocalisation procedures , and systemic - pulmonary shunts [ 35 ]  . 
flow sequences can be used to estimate the severity of one or more of pulmonary stenoses in the main branches [ 36 ]  . post - operative evaluation of congenital heart diseases this is the most well - established indication for cmr , given its high reproducibility in studying biventricular function [ 37 ] and considering that serial functional evaluation has an essential role in the follow - up of these patients . 
in particular , evaluation of right ventricular function , which is difcult with echocardiography , is crucial in the followup of surgically managed congenital heart diseases , such as tetralogy of fallot , pulmonary atresia with ventricular septal defects , transposition of the great vessels treated with atrial switch and double - outlet right ventricle . 
other information exclusively provided by cmr is the depiction of myocardial brosis by late enhancement imaging , which contributes to stratify the risk of arrhythmias in these patients [ 38 ]  . among the surgically managed congenital heart diseases , cmr is particularly important in the follow - up of tetralogy of fallot and associated anomalies [ 39 ]  . 
cmr allows assessment of the entire right ventricle , including the outow tract which is often the site of complications ( e.g. , pseudoaneurysms , residual stenoses ) , as well as quantication of pulmonary regurgitation and identication of residual pulmonary stenoses and shunt . 
langio - rm utile nello studio delle anomalie dellarco aortico [ 29 ]  . coartazione aortica : la rmc denisce accuratamente sede ed estensione della stenosi nella coartazione aortica [ 30 ] , mentre con le sequenze di usso misura la severit della stenosi attraverso il calcolo delle velocit di usso e il gradiente transistmico . 
lunico limite di tale metodica pu essere la valutazione degli stent aortici , per gli artefatti del materiale che limitano la visualizzazione di reperti come la ristenosi e le fratture di stent . perviet del dotto di botallo : la rmc acquista maggiore valore quando il botallo associato ad anomalie congenite complesse [ 33 ] negli adulti , dove pu essere di pi difcile identicazione allecocardiograa , e inne nello studio pre - chirurgico , dove richiesta la precisa quanticazione dello shunt . arterie polmonari : la rmc molto accurata nello studio dellarteria polmonare e delle sue diramazioni principali la cui denizione morfologica essenziale nella valutazione pree post - operatoria di numerose cc come la tetralogia di fallot ( tdf ) , latresia polmonare ( ap ) , i cuori univentricolari [ 34 ]  . 
langio - rm la tecnica principale per valutare le arterie polmonari , misurarne le dimensioni , identicarne una stenosi , ma anche per unaccurata denizione di collaterali sistemico - polmonari , degli esiti di interventi di unifocalizzazione e degli shunt sistemico - polmonari [ 35 ]  . 
lutilizzo delle sequenze di usso pu stimare la gravit di una o pi stenosi polmonare a livello delle diramazioni principali [ 36 ]  . valutazione post - operatoria delle cardiopatie congenite rappresenta lindicazione maggiormente consolidata della rmc , in relazione allelevata riproducibilit nello studio della funzione biventricolare [ 37 ] , la cui valutazione sequenziale nel tempo uno degli elementi fondamentali del follow - up . 
in particolare , lo studio della funzione ventricolare destra , molto difcile con esame ecocardiograco , di cruciale importanza nel follow - up delle principali cc operate come la tdf , lap con div , le trasposizioni dei grandi 760 radiol med ( 2013 ) 118 : 752798 dality , cmr is particularly interesting in dening the optimal time to perform surgical replacement of the pulmonary valve through serial monitoring of cardiac volumes [ 40 ]  . in patients with atrial switch procedure ( e.g. , senning , mustard operation ) for transposition of the great arteries , cmr is important in evaluating the morphology of the venous bafes and to quantify stenoses or shunts in case of bafe stenosis or leakage , respectively . 
furthermore , cmr is the most accurate method in studying the function of the systemic right ventricle and the degree of myocardial brosis , in order to stratify prognostic risk . 
in particular , cmr ow sequences enable the quantication of ow patterns through the anastomosis and ow distribution to the right and left lung , and are helpful in quantifying shunts in case of systemic - pulmonary collaterals [ 42 ]  . finally , angiographic cmr sequences ne - tuned for coronary artery imaging allow an accurate depiction of the origin and proximal course of the coronary arteries [ 43 , 44 ]  . 
other indications in childhood are the depiction of coronary artery aneurysm formation in patients with kawasakis disease , and , as mentioned above , in patients with coronaries arteries reimplantation [ 41 ]  . 
it should be emphasised that , because of the increased survival rate of patients with congenital heart disease , an larger number of these will present acquired cardiac disease , such as ischaemic heart disease . cmr will most likely have an important role in the diagnosis of mixed congenital and acquired cardiac disorders . acquired disorders of the aorta cmr is widely used in clinical practice to study aortic disorders [ 46 ] , enabling a simultaneous evaluation of the vessels lumen and wall , the characterisation of plaques and vasi ( tga ) operate con switch atriale e i ventricoli destri a doppia uscita . 
unaltra informazione unica della rmc la valutazione della brosi miocardica con le sequenze di late enhancement , che contribuiscono a straticare il rischio aritmico di questi pazienti [ 38 ]  . tra le cc operate , il ruolo della rmc particolarmente importante nel follow - up della tetralogia di fallot ( tdf ) e delle anomalie associate [ 39 ]  . 
la rmc visualizza ottimamente il ventricolo destro , incluso il tratto di efusso ventricolare destro , sede spesso di complicanze ( ad esempio , pseudoaneurismi e stenosi residue ) , quantica lentit del rigurgito polmonare e dei ussi polmonari , identica shunt e stenosi polmonari residue . 
come modalit di imaging non invasiva , la rmc di particolare interesse per denire lottimale timing chirurgico per la sostituzione valvolare polmonare attraverso monitoraggio seriato dei volumi cardiaci [ 40 ]  . nei pazienti con procedura di scambio atriale ( ad esempio , intervento senning , mustard ) per la trasposizione delle grandi arterie ( tga ) operate , la rmc importante per valutare sia la morfologia dei condotti venosi che per quanticare le stenosi o gli shunt in caso di leakage dei bafe chirurgici . 
nei pazienti con procedura di switch arterioso , possono essere accuratamente visualizzate complicanze come la compressione delle arterie polmonari dallaorta ascendente o problemi correlati al reimpianto di arterie coronarie , come il restringimento delle arterie coronarie o linfarto miocardico [ 41 ]  . nei pazienti con ventricolo unico ( ad esempio , sindrome del ventricolo sinistro ipoplastico o del ventricolo destro ipoplastico ) trattato con anastomosi cavale - polmonare ( procedura di fontan ) , la rmc ideale nel delineare la morfologia complessa di questi pazienti con lausilio dellangio - rm con mezzo di contrasto e delle sue ricostruzioni , o in alternativa con la sequenza 3d steady - state free precession ( ssfp )  . 
 in particolare , le sequenze rmc di usso si utilizzano per quanticare i pattern di usso attraverso lanastomosi e la distribuzione del usso attraverso i polmoni destro e sinistro e sono utili per quanticare shunt in caso di collaterali sistemico - polmonari [ 42 ]  . 
 inne , le sequenze rmc angiograche messe a punto per le arterie coronarie sono in grado di dimostrare accuratamente lorigine e il decorso prossimale delle arterie coronarie [ 43 , 44 ]  . 
altre indicazioni pediatriche sono lidentiradiol med ( 2013 ) 118 : 752798 table 2 specic indications for mr in congenital heart disorders indications class in ebsteins disease isolated ventricular septal defects ( vsd ) isolated situs anomalies or situs anomalies associated with simple congenital heart disorders 1 . 
in patients with severe renal failure , in whom the use of gadolinium is contraindicated , unenhanced bright - blood ssfp sequences are a valuable alternative to contrast - enhanced 3d mr angiography . cazione di aneurismi delle coronarie nella malattia di kawasaki e , come menzionato precedentemente , nei pazienti con reimpianto delle coronarie [ 41 ]  . deve essere enfatizzato che , in considerazione dellaumentata sopravvivenza dei pazienti con cardiopatie congenite , un crescente numero di questi presenter patologie cardiache acquisite come la cardiopatia ischemica . the spectrum of clinical indications for which the use la rmc ricoprir verosimilmente un importante ruolo tabella 2 indicazioni speciche per la rm nelle cardiopatie congenite 762 indicazioni radiol med ( 2013 ) 118 : 752798 classe nella malattia di ebstein stenosi e displasia polmonare e stenosi aortica isolata stenosi sottovalvolare aortica stenosi sopravalvolare polmonare stenosi sopravalvolare aortica 1 . 
anomalie del situs viscero - atriale anomalie del situs isolate o associate a cc semplici anomalie del situs associate a cc complesse denizione dellanatomia delle vene sistemiche nel sospetto di situs ambiguus 2 . 
anomalie delle valvole atrio - ventricolari ( av ) e dei ventricoli anomalie anatomiche e funzionali isolate delle valvole av anomalie delle valvole av , delle connessioni av e difetti settali av che si associano a malformazioni complesse ( atresie delle valvole av , ventricoli destri a doppia entrata - uscita , criss - cross heart , trasposizioni dei grandi vasi ) anomalia di ebstein quanticazione della funzione ventricolare destra , del danno miocardico ( brosi ) , denizione di lesioni associate difetti settali ventricolari ( div ) isolati div sopracristale div associati a cc complesse quanticazione volumi e massa ventricolare dx e sn diverticoli e aneurismi ventricolari 5 . 
for nella diagnosi di patologie cardiache miste congenite e acquisite . patologie acquisite dellaorta la risonanza magnetica ( rm ) largamente utilizzata nella pratica clinica per lo studio delle patologie dellaorta [ 46 ] , radiol med ( 2013 ) 118 : 752798 these purposes , the results of cmr and ct are essentially equivalent , the only limitation being that cmr cannot identify intramural calcication directly . cmr can also be used in the follow - up of surgical or endovascular aortic repair ( evar ) , to evaluate all types of leaks , although with the relevant limitation that some endoprostheses cannot be well assessed because of magnetic susceptibility artefacts . 
cmr is therefore used less frequently than ct or contrast - enhanced ultrasound techniques [ 47 ]  . in the overall assessment of aortic dissection an additional value of cmr may be provided by ow mapping sequences , which can be used to quantify the degree of aortic valve regurgitation , and to assess the ow patterns in the true and false lumen . even though cmr is highly accurate in the diagnosis and detection of complications of aortic emergencies , such as acute aortic syndromes ( penetrating ulcer , intramural haematoma , and dissection ) , most often the diagnosis is made by multidetector ct or echocardiography : this because most cmr facilities do not offer 24 hour access . 
 indeed , it is the only method able to date the haematoma , through the use of t1 and t2 black - blood fast spin echo sequences , evaluating signal changes over time in relation to different products of degradation of haemoglobcmr can , therefore , distinguish an acute intramural haematoma from a subacute one or from a wall thrombus [ 49 ]  . in contrast to its limited contribution in acute aortic syndromes , cmr plays a prominent role in the assessment of chronic diseases of the aorta . 
the high reproducibility of aortic measurements , added to the non - invasive nature of the technique , and the high diagnostic accuracy in identifying potential complications , make cmr an ideal method for the follow - up of aortic aneurysms and dissections [ 5052 ]  . 
in particular , cmr , compared to ct , is fundamental in the evaluation of aneurysms in patients with marfans syndrome , turners syndrome and bicuspid aortic valve , which are essentially diseases of young adults or even the paediatric population . 
these morphological and functional abnormalities can be studied using a multiparametric cmr approach . cmr plays a key role in the diagnosis and follow - up of aortitis [ 53 ]  . 
in fact , mr angiography affords an accurate 3d luminographic view of the aorta and its main branches and , like ct angiography , enables the identication of stenoses or aneurysms secondary to processes of inammation and reparative brosis . 
in addition , cmr is also accurate in consentendo la simultanea valutazione di lume e parete vasale , la caratterizzazione di placca e la quanticazione dei ussi grazie alla combinazione di sequenze angio - rm gradient echo ( gre ) 3d , morfologiche ( spin - echo black - blood e gradient - echo steady - state free precession ) e di ow mapping o velocity encoding ( venc )  . 
nei pazienti con grave insufcienza renale e nei quali controindicato luso del gadolinio , possono essere inoltre acquisite sequenze unenhanced a sangue chiaro ssfp che rappresentano una valida alternativa allangiograa rm 3d contrastograca . lo spettro di indicazioni cliniche in cui lutilizzo della rmc pu essere considerato appropriato quanto mai ampio e comprende la patologia steno - aneurismatica con relativa valutazione post - chirurgica / interventistica , le sindromi aortiche acute e le aortiti . nella patologia steno - aneurismatica , la rmc consente unaccurata valutazione morfo - funzionale delle sacche aneurismatiche e delle apposizioni parietali contestuali e il loro relativo monitoraggio evolutivo con risultati sostanzialmente sovrapponibili alla tc , con la sola limitazione di non consentire lidenticazione diretta della calcicazioni parietali . la rmc pu essere anche utilizzata nel follow - up chirurgico o post - endovascular aortic repair ( evar ) ove consente di valutare tutti i tipi di leak , ma con il rilevante limite che alcune endoprotesi risultano mal valutabili per gli artefatti da suscettibilit magnetica associati . 
pertanto , la rmc viene utilizzata meno frequentemente rispetto alla tc o alle tecniche di eco - contrastograa [ 47 ]  . nella valutazione globale della dissezione aortica , un valore aggiunto della rmc pu essere dato dalle sequenze con ow mapping , che possono quanticare il grado di insufcienza valvolare aortica o visualizzare la turbolenza di usso nel vero e falso lume . nella patologia aortica acuta ( ulcera penetrante , ematoma intramurale e dissezione ) , la rmc estremamente accurata per la diagnosi e lidenticazione delle complicanze di queste emergenze , ma pi spesso la diagnosi ottenuta con tc multidetettore o ecocardiograa , poich molti impianti rmc non offrono un accesso nelle 24 ore [ 48 ]  . 
infatti lunica metodica capace di datare lematoma attraverso luso delle sequenze ( black blood fast spin echo ) bbfse t1 e t2 , valutando la variazione di segnale nel tempo in rapporto ai differenti prodotti di degradazione dellemoglobina . 
la rm pu quindi distinguere un ematoma intramurale acuto da uno subacuto o da un trombo parietale [ 49 ]  . la rmc gioca invece un ruolo determinante nella patologia cronica dellaorta . 
lelevata riproducibilit delle misure aortiche , alla quale si aggiungono la non invasivit e lelevata accuratezza diagnostica nellidenticare potenziali complicanze , rendono tale metodica ideale nel follow764 radiol med ( 2013 ) 118 : 752798 the diagnosis of aortitis in its early stages , using a combination of t2 - weighted and t1 - weighted contrast - enhanced black - blood fast spin echo ( bbfse ) images . 
these allow the assessment of the degree of disease activity , and can be used to monitor the efcacy of treatment . another application of cmr is the characterisation of atherosclerotic plaques . 
in this context , information can be provided on the content ( with potential differentiation between stable and unstable lesions ) and volume of the atherosclerotic plaque ( with the possibility of monitoring the response to pharmacological treatments ) [ 54 , 55 ]  . 
also molecular imaging ( which exploits the binding of gadolinium or other mr contrast agents to specic molecular constituents of the plaque , in order to identify or highlight some plaque characteristics , such as inammatory components ) is still in an experimental , not clinical stage , although it is potentially interesting for the future of plaque imaging [ 56 ]  . pulmonary arteries the most common acquired pathology of the pulmonary arteries is thromboembolism , both in its acute and chronic forms . 
though mr angiography provides excellent images of the pulmonary artery tree and can be used to diagnose pulmonary emboli , in clinical routine the diagnosis of acute thromboembolism is most often made by ct angiography [ 57 , 58 ]  . 
not only has ct angiography a higher spatial resolution , enabling in particular identication of peripheral defects , but the restricted availability of mr units limits the use of cmr in clinical practice . 
on the other hand , cmr has an increasingly important role in assessing patients with chronic pulmonary hypertension , both in the detection of pulmonary chronic thromboembolism , for the evaluation of the devastative effects of increased pulmonary pressures on the right ventricular function , and for the assessment of reversed cardiac remodelling after pulmonary thromboendarterectomy [ 59 ]  . 
 for this reason , the use of cmr in chronic thromboembolic pulmonary hypertension certainly offers a more complete approach than ct ( table 3 )  . up degli aneurismi e delle dissezioni aortiche [ 5052 ]  . 
in particolare , rispetto alla tc la rmc fondamentale nel valutare gli aneurismi nei pazienti con sindrome di marfan , sindrome di turner , valvola aortica bicuspide , che costituiscono sostanzialmente una popolazione giovane - adulta o addirittura pediatrica e dove il coinvolgimento riguarda soprattutto la porzione prossimale dellaorta , con un interessamento frequente della funzione valvolare e un impatto sul ventricolo sinistro . 
queste anomalie morfologiche e funzionali possono essere studiate utilizzando un approccio multiparametrico . la rmc gioca un ruolo di primo piano anche nella diagnosi e nel follow - up delle aortiti [ 53 ]  . 
infatti , langio - rm consente unaccurata valutazione luminograca 3d della morfologia dellaorta e dei suoi principali vasi analogamente alla tc e consente lidenticazione di stenosi o aneurismi secondari alla patologia inammatoria e alla riparazione . 
in aggiunta , la rmc si dimostrata accurata nella conferma diagnostica delle aortiti anche nelle fasi precoci , attraverso limpiego combinato delle sequenze bbfse t2 pesate e t1 pesate dopo mezzo di contrasto , valutando il grado di attivit della malattia e rappresentando un utile mezzo per monitorare lefcacia delle terapie . la caratterizzazione della placca aterosclerotica unaltra applicazione della rm , che sfrutta anchessa lalta risoluzione di contrasto di alcune sequenze e la non invasivit della metodica . 
la rmc fornisce informazioni sul contenuto ( con potenziale differenziazione tra lesioni stabili e instabili ) e sulla volumetria della placca aterosclerotica [ 54 , 55 ] con possibilit di monitorare la risposta alla terapia farmacologica . 
limpiego clinico per ancora limitato a pochi centri specializzati , soprattutto perch richiede un supporto tecnico elevato in termini di sequenze dedicate , hardware e software ( rm ad alta risoluzione ) , ma anche per la necessit di disporre di un maggior numero di studi clinici che confermino lefcacia della metodica . 
di contro , le potenzialit dimpiego della rmc sono in incremento nel cuore polmonare tromboembolico cronico per la valutazione dei devastanti effetti dellincrementata pressione polmonare sulla funzione ventricolare sinistra e per la valutazione del rimodellamento inverso dopo tromboendoarteriectomia polmona766 radiol med ( 2013 ) 118 : 752798 refore , currently considered the gold standard ; in fact , it is not affected by the geometric assumptions used in 2d echocardiography for the left ventricle ( such as the area / length method )  . 
although these assumptions dont limit the study of healthy subjects ventricles , they represent a problem in dilated and / or remodelled ventricles , in which the geometric shape is not preserved . 
furthermore , the 3d mr approach is the only one that can be used to calculate the indices of global systolic function of the right ventricle , which as is known , cannot be linked to any geometric shape [ 60 , 61 ]  . measurements have been validated ex vivo and in vivo , for both ventricles , with high intraand inter - observer reproducibility ; furthermore , as mentioned above , the reproducibility is better than the one achieved with echocardiocardiography [ 62 , 63 ]  . ssfp sequences are considered the reference for cine imaging with 1.5 t scanners , because they offer better intrinsic contrast than spoiled gradient echo sequences , thus improving the recognition of the endocardial border . alternatively , stroke volumes can be calculated for both ventricles using phase - contrast cine sequences , which , by measuring the ow velocity and the blood output through the thoracic aorta and pulmonary artery immediately above the valve plane , provide similar values as the stroke volume calculated using 3d cine imaging . the same 3d approach is used to evaluate both left and right ventricular masses ; the method has been validated ex vivo . in addition to the assessment of ventricular volumes , mass and global function , cine imaging provides accurate data regarding regional systolic function , usually expressed in terms of wall motion and wall thickening . 
both can be evaluated visually , semi - quantitatively ( e.g. , normokinetic , hypokinetic , akinetic , or dyskinetic for wall motion ) or quantitatively ( e.g. , amount of wall thickening in millimetres or as a percentage )  . 
cmr myocardial tagging techniques and variants ( e.g. , strain - encoding cmr ) allow the calculation of myocardial wall strains and shear strains . these techniques show excellent reproducibility compared to tissue doppler and speckle tracking techniques , and have the advantage of assessing the strain in the entire ventricle [ 62 , 64 , 65 ]  . 
unfortunately strain analysis is still time - consuming and its use is not part of routine clinical assessment . evaluation of inducible ischaemia / risk stratication the detection of signicant coronary artery disease is bare [ 59 ]  . 
pertanto , lutilizzo della rm nel cuore polmonare tromboembolico cronico permette un approccio completo rispetto alla tc ( tabella 3 )  . cardiopatia ischemica la rm cardiaca ormai entrata nella pratica clinica in numerosi aspetti della cardiopatia ischemica ; infatti in grado di fornire informazioni in ambito diagnostico e prognostico non ottenibili o solo parzialmente ottenibili dalle altre metodiche non invasive ( ecograa e scintigraa miocardica ) , che da molti sono ancora considerate lo standard clinico - strumentale di riferimento . le principali applicazioni della rmc sono rappresentate dalla valutazione degli indici di funzione ventricolare , dalla valutazione dellischemia inducibile / straticazione del rischio e dalla valutazione dellinfarto acuto e cronico . valutazione degli indici di funzione ventricolare lo studio della funzione sistolica globale ventricolare ( calcolo dei volumi , della gittata sistolica e cardiaca , della frazione di eiezione ) si avvale dellapproccio 3d della cinerm ed pertanto oggi considerato il gold standard ; essa infatti non risente di assunti geometrici utilizzati in ecocardiograa 2d per il ventricolo sinistro ( come il metodo area / lunghezza ) , che non costituiscono un limite nei ventricoli di soggetti sani , ma lo diventano nei ventricoli dilatati e / o rimodellati , nei quali la forma geometrica non conservata . 
inoltre , lapproccio 3d della rm lunico utilizzabile per il calcolo degli indici di funzione sistolica globale del ventricolo destro che , come noto , non assimilabile ad alcuna gura geometrica [ 60 , 61 ]  . le misure sono state validate ex - vivo e in - vivo per entrambi i ventricoli , con riproducibilit intrae inter - osservatore elevate e superiori a quelle delecocardiocardiograa [ 62 , 63 ]  . la tecnica di riferimento in cine - rm sugli attuali scanner a uso clinico da 1 , 5 t la ssfp , che rispetto alla gradient echo convenzionale presenta un miglior contrasto intrinseco , con conseguente migliore riconoscibilit del prolo endocardico . alternativamente , la gittata sistolica pu essere calcolata per ciascun ventricolo mediante sequenze cine - phase contrast , che misurando velocit di usso e portata attraverso aorta e arteria polmonare subito al di sopra del piano valvolare , che producono valori simili rispetto a quelli calcolati con il metodo 3d suddetto . radiol med ( 2013 ) 118 : 752798 sed on a double mr approach for assessment of inducible ischaemia : the study of changes in myocardial contractility and the analysis of myocardial perfusion . 
in both cases , physical exercise , considered a more physiological method of inducing ischaemia , is impractical within the magnet and so pharmacological stress is commonly used . changes in regional contractility are evaluated with cinemr , using dobutamine as stress - inducing agent : dobutamine is a sympathomimetic amine that increases the strength and frequency of cardiac contractions and has been shown to be more sensitive than the vasodilating agents , such as dipyridamole and adenosine . 
cine - mr with dobutamine is more accurate than echocardiography with dobutamine : nevertheless , mr is only indicated in patients with a poor acoustic window , due to the difcult management of the stress , and to the greater availability and lower cost of dobutamine - induced echocardiographic stress . 
stress testing can also be used with a tagging technique , in order to calculate wall strain under stress [ 66 , 67 ]  . myocardial perfusion is studied using various types of t1 - weighted , rst - pass sequences during a bolus intravenous administration of a gadolinium chelate ( max 0.1 mmol / kg ) , with the greatest possible coverage of the left ventricle , and at least three slices in the short axis together with one long axis view if possible , in order to evaluate the apex [ 68 , 69 ]  . 
 the standard protocol is to study stress - induced perfusion rst , followed by regional and global systolic function , and then resting perfusion ; the last examination can , however , be replaced by delayed enhancement images ( see below ) , capable of identifying any irreversible myocardial lesions . 
 however , the dual stress / resting study is easier to compare to medical nuclear examinations , which use this methodological approach ; furthermore , the use of a quantitative method allows calculating the myocardial perfusion reserve , which correlates well with the data from positron emission tomography ( pet )  . the results of mr perfusion studies , using both qualitative and semiquantitative methods , correlate very well with those of quantitative invasive coronary angiography , pet and single photon emission computed tomography ( spect ) ; compared to the medical nuclear imaging techniques , mr has indubitable advantages , which are not limited to the absence of ionising radiation , but also include greater spatial resolution ( < 3 mm in plane ) : this enables the detection of any subendocardial ischaemia that could go undetected [ 7072 ]  . the high negative predictive value of mr in stress perfusion studies is of particular importance ; the examination is , therefore , indicated in subjects with an intermediate risk of coronary artery disease , in those with an equivocal or nonlo stesso approccio 3d viene utilizzato per il calcolo della massa ventricolare , sia sinistra che destra ; il metodo stato validato ex - vivo . in aggiunta alla valutazione dei volumi ventricolari , massa e funzione globale , la cine - rm produce accurati dati relativi alla funzione sistolica regionale che usualmente espressa in termini di cinesi e ispessimento parietale . 
entrambe possono essere valutate visualmente , in modo semiquantitativo ( ad esempio , normo - , ipo - , a - , dis - cinetico ) o quantitativamente ( ad esempio , entit dellispessimento espresso in millimetri o in percentuale )  . 
queste tecniche mostrano uneccellente riproducibilit rispetto ai dati del tissue doppler e dello speckle tracking e risultano vantaggiose nella valutazione dello strain dellintero ventricolo [ 62 , 64 , 65 ]  . 
sfortunatamente , lanalisi dello strain ancora lunga nei tempi di esecuzione e il suo utilizzo non fa parte della valutazione clinica di routine . valutazione dellischemia inducibile / straticazione del rischio lindividuazione di una patologia coronarica signicativa si avvale di un duplice approccio rm allinduzione di ischemia : lo studio delle alterazioni della contrattilit e quello della perfusione miocardica . 
in entrambi i casi , lo stress sico , considerato pi siologico , difcilmente eseguibile nel magnete , per cui si utilizza lo stress farmacologico . la valutazione delle alterazioni della contrattilit regionale si esegue con cine - rm , utilizzando come agente di stress la dobutamina , amina simpaticomimetica che incrementa contrazione e frequenza cardiaca e che si dimostrata pi sensibile degli agenti vasodilatatori , dipiridamolo e adenosina . 
la cine - rm con dobutamina risultata pi accurata delleco - dobutamina , ma la difcolt di monitoraggio del paziente durante lo stress insieme alla maggior disponibilit e al minor costo dellecodobutamina rendono indicata la rm solo nei pazienti con cattiva nestra acustica . 
lo stress pu inoltre essere utilizzato anche con la tecnica del tagging , al ne di calcolare lo strain parietale sotto stress [ 66 , 67 ]  . lo studio della perfusione miocardica si ottiene utilizzando vari tipi di sequenze di primo passaggio , t1 dipendenti durante somministrazione ev in bolo di un chelato di gadolinio ( max 0 , 1 mmol / kg ) , con copertura pi ampia possibile del ventricolo sinistro , in asse corto con almeno tre strati associati , se possibile , a un asse lungo per la valutazione dellapice [ 68 , 69 ]  . 
il protocollo convenzionale prevede dapprima lo studio di perfusione da stress , cui segue lo studio della funzione sistolica regionale e globale e poi uno 768 radiol med ( 2013 ) 118 : 752798 interpretable exercise ecg , and in those with previously discordant tests [ 73 ]  . evaluation of myocardial infarction the reference mr technique for the study of myocardial infarction is the so - called delayed - enhancement technique using inversion recovery gradient echo sequences acquired 1020 minutes after intravenous administration of a gadolinium chelate ( 0.10.2 mmol / kg )  . 
as a consequence , spect , by not identifying small ischaemia - related myocardial injury such as subendocardial infarctions , which are an important prognosticator of future ischaemic events , underscores the crucial role of cmr both in diagnosis and risk stratication . 
in patients presenting with severe coronary artery disease and chronic ventricular dysfunction , the probability of functional recovery after coronary revascularisation is determined by the viability of the dysfunctional myocardiuthe latter is inversely related to the transmural infarct extent . 
additional low - dose dobutamine cmr can be used to determine the contractility reserve of viable myocardium in infarcts with an intermediate infarct transmurality [ 74 ]  . in general , the intraand inter - observer reproducibility is very high compared to that of nuclear medicine techniques ; the correlation with pet is good , while cmr is more accurate than spect [ 72 ]  . cmr has proved to be particularly sensitive in acute coronary syndromes , both with t2 - weighted sequences , to identify ischaemia - induced myocardial oedema , and with the delayed - enhancement technique , to depict irreversibly damaged myocardium ; furthermore , it predicts future events better than the conventional risk factor assessment . 
moreover , stress perfusion cmr enables the depiction of a signicant coronary artery disease , and cmr allows the differentiation from disorders , such as acute myocarditis and tako - tsubo ( or stress ) cardiomyopathy , that clinically may simulate an acute coronary syndrome . 
because of these strengths , cmr is increasingly used in the emergency setting . cmr performed early after reperfused st - segment elestudio di perfusione a riposo ; tuttavia questultimo pu essere sostituito anche dalla sola sequenza di delayed enhancement ( vedi oltre ) , in grado di identicare le eventuali lesioni miocardiche irreversibili . 
esso inoltre rende possibile , utilizzando un metodo quantitativo , il calcolo della riserva di perfusione miocardica , che correla bene con i dati della pet . i risultati rm di perfusione , sia con valutazione qualitativa che semiquantitativa , correlano molto bene con la coronarograa invasiva quantitativa , con la pet e con la spect ; rispetto alle tecniche medico - nucleari , la rmc presenta indubbi vantaggi , non solo per la mancata somministrazione di radiazioni ionizzanti , ma anche per la maggior risoluzione spaziale ( < 3 mm nel piano ) , il che permette di identicare uneventuale ischemia subendocardica non riconosciuta [ 7072 ]  . di particolare rilievo lelevato valore predittivo negativo della rmc di perfusione da stress ; lesame risulta pertanto indicato nei soggetti con rischio intermedio di malattia coronarica , in presenza di ecg da sforzo dubbio o non interpretabile , oppure con test precedenti discordanti [ 73 ]  . valutazione dellinfarto miocardico la tecnica rm di riferimento nello studio dellinfarto quella cosiddetta del delayed enhancement ; si tratta di unacquisizione inversion recovery gradient echo , ottenuta 1020 minuti dopo la somministrazone ev di un chelato del gadolinio ( 0 , 10 , 2 mmol / kg )  . 
paragonato ad altre tecniche come la spect , il delayed enhancement ha il vantaggio di unelevata risoluzione spaziale , consentendo una precisa valutazione dellestensione dellinfarto con numerose varianti tecniche , in apnea o a respiro libero con tecnica navigator - echo , che identica linfarto acuto e cronico come area iperintensa , rispetto allassenza di segnale del miocardio non infartuato . 
la tecnica stata validata nellanimale da esperimento in numerosi studi e costituisce oggi il gold standard , in quanto dotata di maggior risoluzione spaziale rispetto alle indagini medico - nucleari comunemente utilizzate . 
la necrosi o la brosi miocardica piccola di radiol med ( 2013 ) 118 : 752798 vation myocardial infarction ( stemi ) yields notable prognostic information , such as microvascular obstruction and haemorrhage , salvageable myocardium , transmural infarct extension and involvement of the right ventricle , which affect ventricular remodelling and increase the risk of major adverse cardiac events [ 75 , 76 ]  . finally , cmr is currently the best technique to detect infarct - related complications , such as pseudo - aneurysm formation , thrombus formation , and pericardial pathology ( e.g. , infarct - related pericardial inammation ) [ 77 ]  . coronary arteries assessment coronary artery mr angiography has not reached the high standards of coronary ct because of the well - known technical limitations of mri ( diameter of distal arteries , systolic - diastolic movements , tortuous course , respiratory artefacts )  . 
the technique cannot , therefore , be used to exclude coronary artery disease , even though recent technological developments in single centres have provided encouraging results , approaching those of ct . 
given the completely non - invasive nature of the investigation compared to ct or coronarography , mr is particularly relevant in young subjects with such anomalies ( table 4 ) [ 78 ]  . cardiomyopathies according to the revised aha and esc classications , cardiomyopathies are dened as myocardial diseases associated with electrical and / or mechanical dysfunction , which can lead to inappropriate hypertrophy or dilation , due to numerous , frequently genetic , causes . 
they are classied as primary and secondary , with the primary divided into genetic , mixed and acquired . dilated cardiomyopathy in dilated cardiomyopathy , cmr represents the gold standard technique in quantifying volumes and ejection fractions of both ventricles , and with its high reproducibility it is suitable in monitoring any changes in cardiac function over time [ 6063 ]  . thanks to its unique tissue characterisation , cmr can be dened as the imaging technique of choice ( class i ) in the differential diagnosis between post - ischaemic and nonischaemic forms of dilated cardiomyopathy : in the former , delayed - enhancement sequences document an ischaemictype pattern characterised by constant involvement of the subendocardial side with variable transmural extension [ 79 ]  . 1 gr possono essere identicate con rmc , mentre il limite inferiore della spect circa 10 volte pi basso . 
come conseguenza , la spect , non potendo rilevare piccoli danni miocardici correlati allischemia , come gli infarti subendocardici che sono importanti fattori prognostici di futuri eventi ischemici , rende evidente il ruolo cruciale della rmc sia nella disgnosi che nella straticazione del rischio . 
unulteriore rmc con dobutamina a bassa dose , pu essere usata per determinare la riserva contrattile del miocardio vitale in infarti con intermedia transmuralit [ 74 ]  . in generale , la riproducibilit intrae inter - osservatore molto elevata e , rispetto alle tecniche medico - nucleari , la correlazione con la pet buona , mentre la rmc risulta pi accurata della spect [ 72 ]  . nelle sindromi coronariche acute , la rmc si dimostrata particolarmente sensibile sia con le sequenze t2 dipendenti per lidenticazione delledema indotto dallischemia , che con la tecnica di delayed enhancement per identicare irreversibilmente il miocardio danneggiato ; inoltre , ha mostrato maggior predittivit di eventi futuri rispetto alla valutazione dei fattori di rischio convenzionali . 
inoltre , la rmc con perfusione da stress consente di identicare una coronaropatia signicativa e la rmc in grado di differenziare disordini come la miocardite acuta e la tako - tsubo ( o cardiomiopatia da stress ) , che clinicamente pu simulare una sindrome coronarica acuta . 
for example , a non - ischaemic pattern of enhancement ( usually meso - epicardial ) more frequently occurs in cases of post - myocarditis cardiomyopathy [ 80 ]  . 
the so - called scar - imaging ( late enhancement ) is currently used in the assessment of post - ischaemic dilated cardiomyopathy , also as part of the pre - procedure evaluation of patients who are candidates for cardiac resynchronization therapy with an implantable cardiovascular device . 
knowledge of the site and extension of the irreversible tissue damage ( dened by the same late - enhancement sequences ) in these patients is very important , in order to assess the potential response to treatment and the after treatment prognosis [ 81 ]  . 
la metodica non pu essere quindi utilizzata per escludere la malattia coronarica , anche se i recenti sviluppi tecnologici in singoli centri hanno mostrato risultati promettenti , prossimi a quelli della tc . 
 lunica indicazione in classe i rappresentata dalla ricerca di anomalie di origine e decorso delle coronarie prossimali , solitamente ben studiabili , data la totale non invasivit della metodica rispetto alla tc o alla coronarograa , di particolare rilievo in soggetti giovani ( tabella 4 ) [ 78 ]  . cardiomiopatie in accordo con le classicazioni rivisitate aha e esc , le cardiomiopatie sono denite come patologie del miocardio radiol med ( 2013 ) 118 : 752798 stratication , as documented in the literature , late - enhancement imaging can also supply important prognostic information about the risk of death and major cardiovascular events , even though the effective role of cmr in this specic clinical setting should still be considered as investigational ( table 5 ) [ 82 ]  . associate a disfunzioni elettriche e / o meccaniche che possono condurre a uninadeguata ipertroa o dilatazione dovuta a diverse cause frequentemente genetiche . 
affected subjects may be asymptomatic or present with breathlessness on exertion , chest pain , pre - syncopal or syncopal episodes , or sudden death . frequently found electrocardiographic alterations are electrical signs of left ventricular hypertrophy ( high voltage qrs , left axis deviation , etc . ) , ventricular repolarisation abnormalities , and pathological q waves . the diagnosis of hypertrophic cardiomyopathy can be made through echocardiographic and echo - doppler examinations , which can detect left ventricular wall thickening ( diastolic thickness 15 mm )  . 
echocardiography also accurately documents the diastolic dysfunction associated with the cardiomyopathy and any dynamic obstruction of ventricular outow caused by anomalous movements of the anterior leaet of the mitral valve [ 85 ]  . cmr has a class i indication in several situations , the most common being the diagnostic conrmation of asymmetric forms of hypertrophy , particularly those involving the left ventricular apex , which may not be well assessed by echocardiography [ 86 ]  . 
in cine - mri the strong contrast between ventricular cavity , cardiac muscle and epicardial fat enables accurate measurement of the myocardial thickness also in regions where echocardiographic assessment is limited , such as the right ventricle in cases of biventricular involvement . 
furthermore , cmr is considered the gold standard for the measurement of ventricular mass . in concentric forms of hypertrophic cardiomyopathy , which can usually be well evaluated with echocardiography , the use of cmr is fundamental to make the differential diagnosis from other types of cardiomyopathy with a clinically similar presentation , such as non - compaction cardiomyopathy or storage cardiomyopathies : these include the ones occurring in cardiac amyloidosis and fabrys disease in which there are specic late - enhancement patterns different from those typical of hypertrophic cardiomyopathy [ 87 ]  . 
the pattern of enhancement most frequently found in hypertrophic cardiomyopathy is mesocardial , with cardiomiopatia dilatativa nella cardiomiopatia dilatativa ( cmp ) , la rmc rappresenta il gold standard di riferimento per quanticare con elevata riproducibilit i volumi e la frazione di eiezione di entrambi i ventricoli e monitorare quindi nel tempo le eventuali modicazioni dei parametri di funzionalit cardiaca [ 6063 ]  . la metodica , grazie alle sue uniche capacit di caratterizzazione tissutale , pu essere denita come limaging di scelta ( classe i ) nella diagnosi differenziale tra forme dilatative post - ischemiche e forme non ischemiche ; nelle prime , le sequenze inversion - recovery dopo gadolinio documentano un pattern di late enhancement di tipo ischemico , caratterizzato da interessamento costante del versante subendocardico , con variabile estensione transmurale e identicativo del fronte di necrosi [ 79 ]  . nellambito delle forme non ischemiche , la diagnostica differenziale dei vari tipi di late enhancement pu fornire informazioni utili per differenziare quadri a eziologia postmiocarditica dalle forme puramente primitive in base , ad esempio , alla presenza delle strie di potenziamento con pattern non ischemico ( in genere meso - epicardico ) che caratterizzano pi frequentemente le prime [ 80 ]  . 
il cosidetto scarimaging trova attualmente impiego nelle forme dilatative post - ischemiche , anche nella valutazione pre - procedurale dei pazienti candidati a terapia di resincronizzazione cardiaca con impianto di icd ( implantable cardiovascular device ) , in cui la conoscenza di sede ed estensione del danno tissutale irreversibile ( denito dalle stesse sequenze di late enhancement ) molto importante per valutare la potenziale risposta alla terapia e la prognosi dei pazienti trattati [ 81 ]  . 
 in ambito di straticazione del rischio , come documentato in lettaratura , il late enhancement imaging pu fornire anche importanti informazioni prognostiche relative al rischio di mortalit o di eventi cardiovascolari maggiori associati , anche se il ruolo effettivo della rmc in questo setting clinico specico da considerarsi ancora in fase investigazionale ( tabella 5 ) [ 82 ]  . cardiomiopatia ipertroca la cardiomiopatia ipertroca la malattia cardiovascolare pi comune tra quelle su base genetica e interessa tra lo 0 , 1 e lo 0 , 2% della popolazione [ 83 ] ; essa inoltre rappresenta la pi frequente causa di morte improvvisa nella popolazione giovanile [ 84 ]  . 
dal punto di vista clinico , i soggetti table 5 indications for mr in cardiomyopathies : dilated cardiomyopathy 772 indications differential diagnosis between ischaemic and non - ischaemic forms pre - implantation of icd ( for scar identication and site ) intracavity thrombi global biventricular systolic function ( pre - treatment and follow - up ) non - ischaemic forms : differential diagnosis prognostic stratication icd , implantable cardioverter debrillator tabella 5 indicazioni alla rm nelle cardiomiopatie : cardiomiopatia dilatativa indicazioni diagnosi differenziale tra forme ischemiche e non ischemiche pre - impianto icd ( per identicazione e sede scar ) trombosi endocavitaria valutazione funzione sistolica globale biventricolare ( pre - trattamento e follow - up ) forme non ischemiche : diagnosi differenziale straticazione prognostica icd , implantable cardioverter debrillator radiol med ( 2013 ) 118 : 752798 class inv classe a patchy distribution in the areas of greatest hypertrophy , and reects one of the anatomical substrates of the disease ( the disarray that causes expansion of the extracellular space )  . 
mr perfusion studies may also supply information on ischaemic phenomena that reect microvascular damage with possible implications for risk stratication in patients with known hypertrophic cardiomyopathy [ 89 ]  . 
cmr is also indicated in the follow - up of subjects who have undergone surgical treatment , such as subaortic myomectomy , or percutaneous alcohol septal ablation [ 90 ]  . 
 cmr techniques for ow quantication ( phase - contrast methods ) are useful in recognising high resting gradients below the aortic valve in subjects with obstructive disease ; however , the main limitation of cmr is its limited ability to evaluate dynamic changes in these gradients , which represent echocardiographic markers of the disease . the accuracy of cmr in identifying myocardial hypertrophy is useful in family screening ( table 6 ) [ 91 ]  . restrictive cardiomyopathy restrictive cardiomyopathy comprises a heterogeneous group of myocardial and endocardial diseases that lead to inadequate ventricular relaxation during diastole , with a consequent increase in ventricular lling pressure . 
echocardiography is the initial imaging technique of choice and is often useful to identify morphological alterations of the affetti possono essere asintomatici o presentare dispnea da sforzo , dolore toracico , episodi sincopali e pre - sincopali , o morte improvvisa . 
anche alterazioni elettrocardiograche sono di frequente riscontro , consistenti in segni elettrici di ipertroa ventricolare sinistra ( alti voltaggi del qrs , deviazione assiale sinistra ecc . ) , anomalie della ripolarizzazione ventricolare e onde q patologiche . la diagnosi di malattia pu essere posta mediante esame ecocardiograco ed ecodoppler , che consente di individuare lispessimento parietale del ventricolo sinistro ( spessore diastolico 15 mm )  . 
lecocardiograa documenta in modo accurato anche la disfunzione diastolica associata alla cardiomiopatia e leventuale ostruzione dinamica dellefusso ventricolare con lanomalo movimento del lembo anteriore della mitrale [ 85 ]  . la rmc trova indicazione di i classe in differenti situazioni , la pi frequente delle quali rappresentata dalla conferma diagnostica delle forme asimmetriche , specie di quelle a localizzazione apicale che sono mal valutabili ecogracamente [ 86 ]  . 
nelle sequenze cine - rm , lelevato contrasto tra cavit ventricolare , muscolo cardiaco e grasso epicardico permette di misurare accuratamente lo spessore del miocardio , anche in regioni dove la valutazione ecocardiograca limitata ( ventricolo destro nelle forme con coinvolgimento bi ventricolare )  . 
 nelle forme concentriche , usualmente ben valutabili con esame ecocardiograco , lutilizzo della rmc fondamentale per porre diagnosi differenziale nei confronti di altre radiol med ( 2013 ) 118 : 752798 table 6 indications for mr in cardiomyopathies : hypertrophic cardiomyopathy indications apical type asymmetric type differential diagnosis of myocardial hypertrophies ( athletes heart , fabrys disease , amyloidosis ) evaluation of global biventricular systolic function and myocardial mass evaluation of left ventricular outow obstruction prognostic stratication ( myocardial brosis ) follow - up biopsy guide tabella 6 indicazioni alla rm nelle cardiomiopatie : cardiomiopatia ipertroca indicazioni forma apicale forma asimmetrica diagnosi differenziale delle ipertroe miocardiche ( cuore datleta , fabry , amiloidosi ) valutazione funzione sistolica globale biventricolare e massa miocardica valutazione ostruzione efusso ventricolare sn straticazione prognostica ( brosi miocardica ) follow - up guida alla biopsia class classe cardiac chambers and functional modications of diastolic lling , which indicate a pathological scenario compatible with restrictive cardiomyopathy . however , echocardiography often fails in differentiating restrictive cardiomyopathy from constrictive pericarditis , whereas these two conditions are correctly distinguished by cmr , thanks to the combined assessment of different elements including pericardial thickness , interventricular septal motion during the phases of breathing , and the pattern of myocardial or pericardial late enhancement [ 9294 ]  . 
 furthermore , once the restrictive cardiomyopathy has been diagnosed , cmr can often identify the aetiology and guide the therapeutic approach , through the identication of specic distribution patterns of late enhancement depending on the different mechanisms underlying the formation of brosis ( amyloidosis , sarcoidosis , anderson - fabry disease , endomyocardial brosis / hypereosinophilia syndrome ) [ 95100 ] or detection and quantication of myocardial iron load [ 101 , 102 ]  . 
 the simple evaluation of diastolic function and functional monitoring during the follow - up is adequately performed by echocardiography ; so the use of cmr in these cases is limited to those patients in whom the echocardiography is difcult and unreliable because of a poor acoustic window ( table 7 )  . forme di miocardiopatia che si manifestano con fenotipo simile , ad esempio cardiomiopatia da miocardio non compatto o cardiomiopatie da accumulo , come lamiloidosi cardiaca o la malattia di fabry , dove si osservano pattern di enhancement tardivo specici , differenti da quello tipico della miocardiopatia ipertroca [ 87 ]  . 
il pattern di enhancement di pi frequente riscontro nella miocardiopatia ipertroca di tipo mesocardico , a chiazze nelle zone di maggiore ipertroa e riette uno dei substrati anatomici della patologia , cio il cosiddetto disarray che determina espansione dello spazio extracellulare . 
lesame rm di perfusione pu fornire anche informazioni riguardo fenomeni di ischemia che riettono danno microvascolare con possibili ricadute sulla straticazione del rischio del paziente con nota miocardiopatia ipertroca [ 89 ]  . 
la metodica rmc inoltre indicata per il follow - up dei soggetti sottoposti a terapia chirurgica mediante miomectomia subaortica o ad alcolizzazione del setto per via percutanea [ 90 ]  . 
 le tecniche rmc di quanticazione dei ussi ( metodiche a contrasto di fase ) sono utili per il riconoscimento di gradienti elevati a riposo in sede sottovalvolare aortica nei soggetti con forma ostruttiva della malattia ; tuttavia , il li774 left ventricular non - compaction this form of cardiomyopathy derives from an embryonic development disorder of the endomyocardium , characterised by the persistence of multiple , prominent ventricular trabeculae separated by deep intertrabecular recesses . 
furthermore , the use of contrast agents can demonstrate the presence of brosis in non - compacted areas of the myocardium [ 103 ]  . arrhythmogenic right ventricular cardiomyopathy arrhythmogenic right ventricular cardiomyopathy ( arvc ) is an entity of unknown origin in the classication of cardiomyopathies . 
also known as right ventricular dysplasia , it is a primary disease of the hearts muscle , characterised by broadipose atrophy mainly involving the right ventricle and responsible for severe ventricular arrhythmias and sudden death also in young people . 
the pathological diagnosis of arvc is accomplished on the basis of the evidence of fatty or brofatty replacement of the myocardium mostly at the right ventricle in absence of other cardiac and non - cardiac causes of death . cmr is considered the best imaging technique in the assessment of arvc [ 104 ]  . 
cine mr enables calculation of the right heart volumes and ejection fraction : this is useful since patients with this form of cardiomyopathy develop progressive right ventricular dilatation and impaired systolic function ( pathological values are considered to be a body surface - adjusted right ventricular volume of > 110 ml / m in males or > 100 ml / m in females and a right ventricular ejection fraction 40% ) , as stated by the task force on arvc [ 105 ]  . cmr analysis of regional wall motion is extremely useful and better than any other technique to detect any areas of akinesia / dyskinesia / bulging , which can be interpreted as a consequence of the cell death underlying the disease . 
 morphological imaging ( black - blood ) is able to demonstrate fatty inltration within the myocardial tissue , which occurs through an ex vacuum mechanism after the death of the cardiac muscle cells . 
images acquired using late enhanradiol med ( 2013 ) 118 : 752798 mite principale della rm rappresentato dallestrema difcolt di valutare le variazioni dinamiche di tali gradienti che rappresentano uno dei marker ecograci di malattia . laccuratezza della rmc nellidenticare lipertroa miocardica utile , inoltre , nello screening familiare ( tabella 6 ) [ 91 ]  . cardiomiopatia restrittiva la cardiomiopatia restrittiva comprende un eterogeneo gruppo di patologie miocardiche o endocardiche che comportano un inadeguato rilasciamento ventricolare durante la diastole con conseguente incremento delle pressioni di riempimento ventricolare . 
lecocardiograa rappresenta la tecnica di imaging iniziale , spesso utile a identicare quelle modicazioni morfologiche delle camere cardiache e funzionali della fase di riempimento diastolico che suggeriscono un quadro compatibile con cardiomiopatia restrittiva . 
tuttavia , lecocardiograa spesso fallisce nel differenziare la cardiomiopatia restrittiva dalla pericardite costrittiva , che invece vengono correttamente differenziate dalla rmc grazie alla valutazione combinata di differenti elementi fra cui lo spessore del pericardio , il movimento del setto interventricolare durante le fasi del respiro , il pattern di late enhancement miocardico o pericardico [ 92 94 ]  . 
inoltre , diagnosticata la cardiomiopatia restrittiva , la rmc consente spesso di identicare il substrato eziologico e quindi di guidare lapproccio terapeutico , attraverso lidenticazione di pattern specici di distribuzione del late enhancement , dipendenti da diversi meccanismi di creazione della brosi ( amiloidosi , sarcoidosi , malattia di anderson - fabry , brosi endomiocardica / sindrome da ipereosinolia ) [ 95100 ] o lidenticazione e quanticazione dellaccumulo di ferro cardiaco [ 101 , 102 ]  . 
la semplice valutazione della funzione diastolica e il monitoraggio funzionale durante il follow - up sono compiti che lecocardiograa svolge adeguatamente , quindi il ricorso alla rmc in questi casi limitato a quei pazienti in cui la valutazione ecocardiograca difcoltosa e inafdabile per problemi di scarsa nestra acustica ( tabella 7 )  . non compattazione ventricolare sinistra questa cardiomiopatia deriva da un disordine della morfogenesi endomiocardica caratterizzato dalla persistenza di multiple trabecolature ventricolari prominenti , separate da profondi recessi intertrabecolari . 
generalmente , colpisce la parete laterale e lapice del ventricolo sinistro , quei segmenti cio che durante lembriogenesi vanno pi tardivaradiol med ( 2013 ) 118 : 752798 cement technique after administration of a contrast agent can show areas of enhancement within the myocardium , indicating sites of brotic repair . 
the reproducibility of the mr technique enables comparison of wall motion changes , replacement and late enhancement sector by sector , increasing the diagnostic value in the case of concomitant presence of these features . 
 cmr is also useful in the follow - up of patients with arvc [ 106 ]  . other cardiomyopathies haemochromatosis haemochromatosis - related cardiomyopathy is due to the accumulation of iron in cardiac myocytes responsible for both systolic and diastolic dysfunction . 
 myocardial t2 * is correlated to the amount of cardiac iron determined in myocardial biopsies [ 24 ] and a t2 * value < 20 ms is considered to indicate iron overload in patients with - thalassaemia major . 
cmr is the only method capable of non - invasive monitoring of the trend and efcacy of ironchelating therapy over time . sarcoidosis sarcoidosis is a systemic granulomatous disease involving the heart in up to 50% of cases . 
cmr is proposed as the diagnostic investigation in studying the heart of patients with sarcoidosis , in the follow - up and assessment of cardiac morphology and function and in determining the disease extension [ 109 , 110 ]  . 
finally , analysis of late - enhancement sequences plays a very important role [ 111 , 112 ] ; late enhancement seems to localise to the basal parts of the heart , in particular in the interventricular septum and the lateral wall , with a characteristic distribution ( focal or with striae sparing the subendocardium ) or , in more advanced cases , with a transmural pattern . mente incontro al processo di compattazione . 
luso del mezzo di contrasto pu dimostrare , inoltre , la brosi presente nelle zone di miocardio non compatto [ 103 ]  . cardiomiopatia aritmogena del ventricolo destro la displasia del ventricolo destro unentit di origine sconosciuta nella classicazione delle cardiomiopatie . 
anche conosciuta come cardiomiopatia aritmogenica del ventricolo destro ( cavd ) una malattia primitiva del muscolo cardiaco caratterizzata da atroa broadiposa prevalentemente coinvolgente il ventricolo destro e responsabile di aritmie ventricolari severe e morte improvvisa anche nei giovani . 
la diagnosi patologica di cavd basata sullevidenza di sostituzione adiposa o broadiposa del miocardio prevalentemente a livello del ventricolo destro , in assenza di altre cause di morte cardiache e non cardiache . la rmc considerata la migliore tecnica di imaging nello studio della cavd [ 104 ]  . 
lo studio 3d cine - rm permette il calcolo dei volumi destri e della frazione deiezione ; tale dato risulta utile in quanto nei pazienti affetti si osserva una progressiva dilatazione della camera ventricolare e riduzione della funzione sistolica ( viene considerato patologico un volume ventricolare destro per supercie corporea > 110ml / m nei maschi o 100 ml / m nelle donne e fe ventricolare destra 40% ) come riportato dalla task force sulla cavd [ 105 ]  . 
lanalisi della cinesi regionale risulta estremamente utile nel denire , meglio di ogni altra tecnica , la presenza di aree di acinesia / discinesia / bulging interpretabili come esiti della morte cellulare che sta alla base della malattia . 
le acquisizioni morfologiche ( a sangue nero ) sono in grado di dimostrare linltrazione di tessuto adiposo in sede intramiocardica riferibile a meccanismo ex vacum dopo la morte delle miocellule . 
la riproducibilit propria della tecnica rm permette la comparazione delle alterazioni cinetiche , della sostituzione e del late enhancement settore per settore , incrementando il valore diagnostico nel caso di copresenza di tali elementi . 
il coinvolgimento ventricolaradiol med ( 2013 ) 118 : 752798 class classe table 7 indications for mr in cardiomyopathies : restrictive cardiomyopathies 776 indications differential diagnosis from constrictive pericarditis differential diagnosis and characterization of restrictive forms evaluation of global biventricular systolic function and myocardial mass evaluation of diastolic function follow - up biopsy guide tabella 7 indicazioni alla rm nelle cardiomiopatie : cardiomiopatie restrittive indicazioni diagnosi differenziale con la pericardite costrittiva diagnosi differenziale e caratterizzazione forme restrittive valutazione funzione sistolica globale biventricolare e massa miocardica valutazione funzione diastolica follow - up guida alla biopsia fabrys disease and amyloidosis about 4% of patients with a morphological diagnosis of hypertrophic cardiomyopathy ( on the basis of increased wall thickness ) have fabrys disease [ 113 ]  . 
other patients with a morphological diagnosis of myocardial hypertrophy show an amyloid restrictive cardiomyopathy characterised by diastolic dysfunction , ventricular hypertrophy and thickening of the interatrial septuthe distinction from other forms of cardiac hypertrophy may be difcult in the early stages of amyloidosis . 
however , the pattern of distribution of the late enhancement in amyloidosis is distinctive ; widespread , global , and mainly subendocardial , with a transmural tendency in more severe cases ( table 8 ) [ 117 ]  . myocarditis the clinical onset of acute myocarditis may produce extremely variable and non - specic signs , including typical heart attack - like signs ( acute chest pain , increased troponin and st segment elevation ) and atypical ones including new - onset arrhythmias , rapidly evolving dilated cardiomyopathy , and acute heart failure [ 118 ]  . from a diagnostic point of view , traditional investigations are not very accurate in this condition , which usually sarcoidosi re sinistro presente generalmente nelle forme avanzate e la rmc produce informazioni simili a quelle del ventricolo destro . 
la rmc inoltre utile nel follow - up di tali pazienti [ 106 ]  . altre cardiomiopatie emocromatosi dovuta allaccumulo di ferro a carico dei miociti cardiaci , responsabile di disfunzione sia sistolica che diastolica . 
la determinazione dei livelli di ferro a livello cardiaco gioca un ruolo molto importante nei pazienti con tale patologia , essendo linsufcienza cardiaca la prima causa di mortalit in questi pazienti . 
la determinazione dellaccumulo di ferro cardiaco oggi possibile con la misurazione del tempo di rilassamento t2 * mediante lutilizzo di sequenze multi - echo t2 * [ 107 , 108 ]  . 
il t2 * miocardico correla con la concentrazione di ferro cardiaco ottenuta da campioni di biopsie miocardiche [ 24 ] e un valore di t2 * < 20 ms considerato positivo per accumulo nei pazienti affetti da - talassemia major . 
la rmc lunica metodica in grado di monitorare in modo non invasivo landamento e lefcacia della terapia chelante nel tempo . una malattia granulomatosa sistemica che pu coinvolgere il cuore dei pazienti che ne sono affetti no al 50% dei radiol med ( 2013 ) 118 : 752798 table 8 indications for mr in cardiomyopathies : other cardiomyopathies indications arrhythmogenic right ventricular disease right ventricular global and regional systolic evaluation tissue characterisation ( bro - adipose replacement ) aetiological and differential diagnosis of complex ventricular arrhythmias differential diagnosis of isolated dilatation of the right ventricle left ventricular non - compaction isolated form ( not associated with other cardiomyopathies ) suspected endoventricular thrombi primary and secondary haemochromatosis ( diagnosis and follow - up ) fabrys disease ( diagnosis and follow - up ) sarcoidosis tabella 8 indicazioni alla rm nelle cardiomiopatie : altre cardiomiopatie malattia aritmogena del ventricolo destro valutazione sistolica regionale e globale del ventricolo destro caratterizzazione tissutale ( sostituzione bro - adiposa ) diagnosi eziologica e differenziale delle aritmie ventricolari complesse diagnosi differenziale delle dilatazioni isolate del ventricolo destro non compattazione ventricolare sinistra forma isolata ( non associata ad altre cardiomiopatie ) sospetto di trombosi endoventricolare emocromatosi primitiva e secondarie ( diagnosi e follow - up ) malattia di fabry ( diagnosi e follow - up ) sarcoidosi class indicazioni classe presents with non - specic imaging and laboratory features . 
these consist of changes in troponin and inammation markers in absence of coronary lesions documented by selective catheterisation and non - specic electrocardiographic changes , such as sinus tachycardia with nonspecic st - segment changes , new - onset bundle branch block , and infarct - like pictures with t - wave inversion and st - segment elevation . although endomyocardial biopsy is the diagnostic gold standard , it does have relevant limitations . 
the most important are the invasiveness of the procedure , which leads to complications in about 6% of cases ( severe complications , 0.5% ) , and its low diagnostic sensitivity due to the possibility of sampling error ( samples of healthy myocardium ) : this is related to the typically focal nature of the process which predominantly involves the epicardial wall , an area difcult to sample due to the risk of wall perforation [ 119 ]  . given its non - invasiveness and unique capacity for tissue characterisation , cmr may be considered appropriate and clinically relevant ( class i ) in all possible manifestations of the onset of myocarditis , from infarct - like forms in patients with healthy coronary arteries , to those with new - onset arrhythmias , and in patients with acute heart failure typical of the fulminating or rapidly progressive forms . the standard cmr technique is based on the combicasi . 
la rmc viene proposta come indagine diagnostica per lo studio cardiaco dei pazienti con sarcoidosi , nel follow - up e nella quanticazione dei parametri morfo - funzionali cardiaci e dellestensione della malattia [ 109 , 110 ]  . 
gli inltrati sarcoidotici focali e diffusi , responsabili di edema e inammazione , vengono visualizzati come aree di iperintesit delle sequenze t2 pesate con saturazione del segnale del tessuto adiposo . 
inne , un ruolo molto importante spetta allanalisi del late enhancement ( le ) [ 111 , 112 ] , che sembra avere in questa patologia specica localizzazione interessando le porzioni basali , in particolare in corrispondenza del setto interventricolare , e la patere laterale , con un pattern di distribuzione caratteristico ( focale o con strie che risparmiano il subendocardio ) o , nei casi pi avanzati , con un pattern transmurale . malattia di fabry e amiloidosi circa il 4% dei pazienti con diagnosi morfologica di cardiomiopatia ipertroca ( sulla base dellaumento degli spessori ) presenta la malattia di fabry [ 113 ]  . 
in questi pazienti 778 table 9 indications for mr in myocarditis indications class acute coronary syndrome - like presentation in patient with lesion - free coronary arteries new onset arrhythmias acute heart failure of unknown cause chronic heart failure of unknown cause ( not secondary to valve disease ) aetiological diagnosis follow - up ( steroid therapy ) prognostic stratication biopsy guide tabella 9 indicazioni alla rm nelle miocarditi indicazioni classe presentazione simil - sindrome coronarica acuta a coronarie indenni aritmie di nuova insorgenza scompenso acuto di ndd scompenso cronico ( non secondario a valvulopatia ) di ndd diagnosi eziologica follow - up ( terapia steroidea ) straticazione prognostica guida alla biopsia ndd , natura da determinare nation of functional ssfp sequences and morphological imaging with early and late enhancement and short - tau inversion recovery ( t2 - stir ) , which can identify the various tissue characteristics present in myocarditis : active hyperaemia , myocite necrosis ( with a meso - epicardial pattern of late enhancement ) , and oedema [ 120 , 121 ]  . in chronic myocarditis , cmr can be used to assess chronic heart failure in order to differentiate the dilated cardiomyopathies with a post - myocarditis aetiology from the post - ischaemic forms , characterised by subendocardial or transmural late enhancement , with obvious consequences for the clinical - therapeutic management of the patient [ 120 , 121 ]  . it has also been proposed that cmr with late - enhancement imaging could be used as a guide when taking endomyocardial biopsies ( table 9 ) [ 120 , 122125 ]  . heart transplantation in patients who have received a heart transplant , early recognition of organ rejection ( before the functional deterioration of allogeneic tissue ) is a relevant diagnostic and clinical problethe current gold standard is endomyocardial biopsy . 
cmr , particularly with t2 - weighted stir sequences , radiol med ( 2013 ) 118 : 752798 lattivit dellenzima - galattosidasi ridotta e ci determina un accumulo dei glicosngolipidi gl3 . 
in molti casi la rmc permette di evidenziare unarea di late enhancement ( le ) intramiocardico a carico della parete basale - laterale [ 114 , 115 ] , sede non tipica per la diagnosi di cardiopatia . 
la rmc pu valutare lefcacia del trattamento terapeutico con lenzima sostitutivo [ 116 ]  . altri pazienti con diagnosi morfologica di ipertroa miocardica sono in realt affetti da cardiomiopatia restrittiva amiloidotica , caratterizzata dalla presenza di disfunzione diastolica , ipertroa ventricolare e ispessimento del setto interatriale . 
tuttavia , il pattern di distribuzione del le nellamiloidosi distintivo ; diffuso , globale e prevalentemente subendocardico , nei casi pi gravi pu avere andamento transmurale ( tabella 8 ) [ 117 ]  . miocarditi lesordio clinico della miocardite acuta pu essere estremamente aspecico e variabile , comprendendo sia forme tipiche con manifestazioni simil - infartuali ( dolore toracico acuto , movimento troponinico e sovraslivellamento del tratto st ) , che forme atipiche caratterizzate da aritmie di nuovo riscontro o da quadri rapidamente evolutivi con cardiopatia dilatativa e scompenso acuto [ 118 ]  . dal punto di vista diagnostico , i test tradizionali sono poco accurati per linquadramento clinico della malattia , che si presenta in genere con quadri strumentali e laboratoristici aspecici . 
essi sono consistenti in movimento troponinico e degli indici di ogosi in assenza di lesioni coronariche documentabili con cateterismo selettivo e modicazioni elettrocardiograche aspeciche tipo tachicardia sinusale con alterazioni aspeciche del tratto st , blocchi di branca di nuova insorgenza o quadri simil - infartuali con inversione dellonda t e sovraslivellamento del tratto st . anche la biopsia endomiocardica , pur rappresentando il gold standard diagnostico , ha delle rilevanti limitazioni date in primo luogo dallinvasivit della procedura che presenta un rischio di complicanze del 6% circa ( 0 , 5% complicanze gravi ) e dalla sua ridotta sensibilit diagnostica che dipende dal rischio di prelevare campioni di tessuto miocardico sano ( il cosiddetto sampling error ) in un processo che , almeno nelle fasi iniziali , assume carattere tipicamente focale con coinvolgimento prevalente del versante epicardico , che risulta poco esplorabile dal punto di vista istologico per il rischio di perforazione [ 119 ]  . in questambito clinico , sia per la sua non invasivit che per le sue uniche capacit di caratterizzazione tissutale , lutilizzo della rmc pu essere considerato appropriato e cliradiol med ( 2013 ) 118 : 752798 can be useful in this clinical situation ; in fact , myocardial oedema can be an early marker of acute rejection , since it depends on both inammatory phenomena that precede organ rejection and presence of interstitial oedema caused by altered absorption of uids , which occurs in the early stage of microcirculation congestion [ 126 ]  . cardiac masses cardiac mri is considered a powerful tool in the evaluation of patients with suspected pericardial or cardiac masses . 
angiosarcomas and undifferentiated sarcomas are the two most common primary malignancies . some normal structures can mimic true cardiac tumours : prominent eustachian valves , chiari network , crista terminalis , lipomatous interatrial septum , pleuro - pericardial cysts , and large hiatal hernias . 
cmr can easily recognise these structures , which often remain undened with other non - invasive cardiac imaging . moreover , differential diagnosis with intracardiac thrombi can be easily dened by cmr ; cardiac thrombi can occur in the left atrial appendage in patients with atrial brillation , while left ventricular thrombi often be detected in patients with dilated ischaemic cardiomyopathy . 
cine mr and contrast - enhanced cardiac mri allow the differentiation between thrombus and neoplastic masses , due to the absence of vascularisation and , consequently , of contrast enhancement in the thrombus , where it may be observed at the most peripheral uptake . in patients with cardiac neoplastic masses , variable extents of contrast enhancement are generally observed . 
cmr can be employed to characterise tissue within the mass . with regard to benign tumours , the most common is atrial myxoma , which is easily recognised with mr , but is often identied already with traditional trans - thoracic echocardiography . 
the most common site is the left atrium ( 7580% ) , in the interatrial septum , especially near the fossa ovale , but it may also occur in the right atrium ( 1020% ) and occasionally in both atria , growing through the foramen ovale , in case of patency [ 127 ]  . 
mr examination is usually nicamente rilevante ( classe i ) in tutte le possibili manifestazioni di esordio della malattia , dalle forme simil - infartuali in pazienti a coronarie sane a pazienti con aritmie di nuovo riscontro , no ai quadri di scompenso acuto tipici delle forme fulminanti o rapidamente progressive . la tecnica di studio rmc standard si basa sulla combinazione di sequenze funzionali ssfp e di imaging morfologico con tecnica di early e late enhancement e t2 - stir ( short - tau inversion recovery ) che consentono di identicare le diverse componenti tissutali presenti nella patologia rappresentate rispettivamente da iperemia attiva , brosi interstiziale ( con pattern meso - epicardico di late enhancement ) ed edema [ 120 , 121 ]  . nella miocardite cronica la rmc pu essere impiegata nellinquadramento dello scompenso cronico per differenziare le cardiomiopatie dilatative a eziologia post - miocarditica rispetto alle forme post - ischemiche caratterizzate da late enhancement di tipo subendocardico o transmurale , con ovvie ripercussioni sulla gesione clinico - terapeutica del paziente [ 120 , 121 ]  . lutilizzo della rmc con tecnica di late enhancement stato inoltre proposto come guida per la biopsia endomiocardica ( tabella 9 ) [ 120 , 122125 ]  . trapianto cardiaco nei pazienti sottoposti a trapianto cardiaco , la diagnosi precoce di rigetto dorgano ( prima cio che si alteri la funzionalit del tessuto allogenico stesso ) rappresenta una rilevante problematica diagnostica e clinica , in quanto il gold standard attuale la biopsia endomiocardica . 
 la rmc , in particolare con le sequenze t2 - stir pesate , pu essere utile in questa situazione clinica ; ledema miocardico , infatti , pu rappresentare un marker precoce di rigetto acuto , potendo dipendere sia dai fenomeni ogistici che precedono il rigetto dorgano che dalla presenza di edema interstiziale da alterato riassorbimento di uidi , che si evidenzia in fase precoce per congestione del microcircolo [ 126 ]  . masse cardiache la risonanza considerata una valida tecnica nello studio di pazienti con sospette masse cardiache e paracardiache . 
il primo 780 radiol med ( 2013 ) 118 : 752798 requested after echocardiographic studies , in order to plan a possible surgical intervention ( class ii )  . a benign tumour for which cmr is not indicated is papillary broelastoma , since this lesion is usually small ( normally less than 1 cm ) , and generally formed of ne growths attached to the endocardium by a pedicle [ 128 , 129 ]  . 
typically , they arise from the left interventricular septubecause of the risk of sudden death , removal is recommended also in asymptomatic patients . both rhabdomyomas and bromas are well - dened lesions , showing medium signal intensity and limited uptake of contrast mediufibromas often show central calcication . 
the disadvantage of cmr is related to the inability to detect calcication , useful in the differentiation between bromas and rhabdomyomas . malignant tumours although mr does not always enable tissue characterisation of the malignant lesion , it does play a very important role in pre - operative evaluation , allowing accurate loco - regional staging by revealing extension towards surrounding organs and inltration of vascular structures , cardiac chambers and the pericardial serosa ( table 9 ) [ 130 , 131 ]  . angiosarcoma angiosarcomas arise most frequently from the left atriu they often show pericardial involvement . 
high conelemento da considerare , in presenza di una sospetta lesione cardiaca , riguarda il riconoscimento e la differenziazione tra le cosiddette masse e pseudomasse e , in questo ambito , il contributo diagnostico della rm assolutamente rilevante ( classe i )  . alcune strutture normali possono mimare veri tumori cardiaci : una prominente valvola di eustachio , la rete di chiari , la cresta terminale , il setto interatriale lipomatoso , la cisti pleuro - pericardica e ampie ernie iatali . 
inoltre , la diagnosi differenziale con trombi intracardiaci facilmente ottenuta dalla rmc : trombi cardiaci possono facilmente organizzarsi a livello dellauricola sinistra nei pazienti con brillazione atriale , mentre trombi del ventricolo sinistro spesso si osservano in pazienti con cardiomiopatia dilatativa ischemica . 
cine - rm e rmc contrastograca permettono la differenziazione tra trombo e masse neoplastiche , in relazione allassenza di vascolarizzazione e , conseguentemente , di potenziamento contrastograco nel trombo , dove al massimo pu essere osservato un accumulo periferico . nei pazienti con masse neoplastiche cardiache viene evidenziata una variabile quantit di presa contrastograca . 
la rmc pu essere utilizzata per caratterizzare il tessuto allinterno della massa . nellambito dei tumori benigni , la lesione pi frequente il mixoma atriale , ben riconoscibile con rm , ma spesso identicato gi con esame ecocardiograco transtoracico tradizionale . 
la sede pi comune latrio sinistro ( 75 80% ) , specialmente a livello del setto interatriale nei pressi della fossa ovale , ma possono presentarsi anche nellatrio destro ( 1020% ) e occasionalmente in entrambi gli atri , crescendo attraverso il forame ovale in caso di perviet [ 127 ]  . 
lesame rm viene in genere richiesto dopo esame ecocardiograco per leventuale planning dellintervento chirurgico ( classe ii )  . tra i tumori benigni , una delle lesioni per le quali non vi indicazione alla cardio - rm il broelastoma papillare , in quanto una lesione di solito piccola , abitualmente inferiore al cm e generalmente costituita da ni escrescenze attaccate allendocardio attraverso un sottile peduncolo [ 128 , 129 ]  . 
questa lesione generalradiol med ( 2013 ) 118 : 752798 trast enhancement is also observed , due to the high degree of vascularisation . sarcoma liposarcoma lymphoma undifferentiated sarcomas , brosarcomas , leiomyosarcomas have a similar appearance to angiosarcomas with varying degrees of vascularisation . liposarcomas are extremely rare and may occur at any cardiac level . 
malignant cardiac masses angiosarcomi once a cardiac mass has been identied , the presence of heterogeneous inltration of the myocardium , vascular invasion , or other signs of metastasis ( e.g. , metastatic pleural effusion and / or mediastinal adenopathy ) can be used to differentiate benign vs malignant tumours . 
first - pass imaging through a cardiac mass may help distinguish vascularised lesions , such as renal carcinoma metastases , from other nonvascular lesions ( table 10 )  . sarcomi pericardial diseases liposarcomi langiosarcoma origina pi frequentemente dallatrio sinistro e mostra spesso invasione pericardica . 
elevata presa di contrasto spesso presente in relazione allelevata vascolarizzazione . sarcomi indifferenziati , brosarcomi e leiomiosarcomi hanno aspetti simili allangiosacoma con vari gradi di vascolarizzazione . cmr represents an ideal method in the study of the pericari liposarcomi sono estremamente rari . 
possono essere preradiol med ( 2013 ) 118 : 752798 table 10 indications for mri in cardiac masses 782 indications differential diagnosis between mass , thrombus or artifact ( from slow ow or by poor acoustic window ) at echocardiography intracardiac mass : differential diagnosis between benign and malignant lesions and characterization intracavitary cardiac mass differentiation in suspect of myxoma cardiac pseudomass characterization staging malignant tumors : evaluation of extension to surrounding organs , vascular structures , cardiac chambers and pericardium ; judgement of operability and therapy planning assessing valvular aps suspected lesion , like broelastoma tabella 10 indicazioni alla rm nelle masse cardiache indicazioni diagnosi differenziale tra massa , trombo o artefatto ( da usso lento o da cattiva nestra acustica ) allecocardiograa massa intracardiaca : diagnosi differenziale fra lesione benigna e maligna ed eventuale tipizzazione tipizzazione massa cardiaca endocavitaria in sospetto mixoma caratterizzazione pseudomasse cardiache staging tumori maligni : valutazione estensione verso organi circostanti , strutture vascolari , camere cardiache e pericardio ; giudizio di operabilit e pianicazione terapeutica valutazione sospetta lesione lembi valvolari , tipo broelastoma class iii classe dium , thanks to the strong natural contrast existing between the serous membranes distended by a physiological amount of uid and the adipose tissue present on both the mediastinal and subepicardial aspects , and to the possibility of combining precise morphological and functional evaluations [ 132134 ]  . 
however , the left pericardium is often not visible because of the lack of surrounding fat and the contiguity to the left lung . echocardiography , nonetheless , remains the method to be used rst and is very often satisfactory in a large number of clinical situations , given its relative inexpensiveness , speed of performance and widespread availability . 
la maggior parte delle metastasi mostra segni di vascolarizzazione dopo iniezione di mezzo di contrasto . masse cardiache maligne verso benigne una volta che la massa stata identicata , la presenza di inltrazione del miocardio , linvasione vascolare o altri seradiol med ( 2013 ) 118 : 752798 pericardial effusion echocardiography is the rst level method in the evaluation of simple uid collections ( homogeneously anechoic serous effusions )  . cmr may be useful in the characterisation of complex effusions ( haemopericardium or myopericardial massesassociated effusions ) or in the evaluation of the impact of large effusions on diastolic function , in cases in which the large effusion and a poor acoustic window prevent accurate echocardiographic evaluation of morphology and function ( class i ) [ 132134 ]  . cmr has a limited role in cardiac tamponade , given the acute nature of this condition and the need of emergency intervention ( class iii ) [ 133 ]  . congenital anomalies congenital anomalies of the pericardium are rare and due to abnormal intrauterine embryonic development of the pericardiucmr is the rst choice imaging method for characterisation and diagnosis of these anomalies . partial and complete defects can generally be well evaluated by using both cine ssfp and tse images , visualising both the extent of serosal defect and the degree of cardiac herniation into the left hemithorax frequently associated with these disorders . 
more challenging could be the detection of partial defects involving the left ventricle lateral wall , since mr visibility of this segment of pericardium is worse . in congenital defects , mr also enables a global evaluation of the often associated complex anomalies involving both the heart ( tetralogy of fallot , atrial septal defects , patent ductus arteriosus , etc . ) and non - cardiac structures ( hiatal hernia , bronchogenic cysts , pulmonary hypoplasia ) [ 2 , 3 ]  . pericardial diverticula , which are extremely rare , are focal herniations of the visceral layer of the pericardial membrane through the parietal layer . 
cmr can provide useful support in the diagnosis and pre - operative evaluation of these diverticula [ 2 ]  . cmr should be considered the imaging method of choice for pleuro - pericardial cysts , given its ability to characterise tissues and resolve differential diagnoses , thanks to the combination of t1and t2 - weighted tse sequences . 
the cysts are easily recognised because of their site ( the right cardiophrenic angle being much more frequently affected than the left one ) and signal characteristics ( hypointense in t1 , hyperintense in t2 without contextual solid elements ) , and can almost always be distinguished from other masses and similar pseudomasses ( echinococcal cysts , mediastinal teratomas , bronchogenic cysts , etc . ) [ 2 , 3 ]  . gni di metastasi ( ad esempio , versamento pleurico metastatico e / o adenopatia mediastinica ) possono essere utilizzati per differenziare neoplasie benigne da quelle maligne . 
limaging di primo passaggio di una massa cardiaca pu aiutare a distinguere tra lesioni vascolarizzate , come metastasi da carcinoma renale , dalle altre lesioni avascolari ( tabella 10 )  . malattie del pericardio la rm rappresenta la metodica ideale per lo studio del pericardio , grazie allelevato contrasto naturale esistente tra i foglietti sierosi distesi da una siologica quota di uido e il tessuto adiposo presente sia sul versante mediastinico che subepicardico e alla possibilit di combinare unaccurata valutazione morfologica e funzionale [ 132134 ]  . 
tuttavia , il pericardio sinistro spesso non visibile a causa dellassenza di grasso paracardiaco e della contiguit del polmone . lecocardiograa rimane la metodica di prima istanza e molto spesso risolutiva in un ampio numero di situazioni cliniche grazie alla sua relativa economicit , rapidit di esecuzione e ampia diffusione sul territorio . 
 the use of paramagnetic contrast agents with the late - enhancement technique shows any enhancement of the serosal layers , an expression of active inammation , after administration of gadolinium . one particular situation is post - infarction pericarditis , both epistenocardiac or autoimmune ( dresslers syndrome )  . 
 in this condition , the late - enhancement pattern of the infarct is associated with intense enhancement of the pericardial layers together with a peculiar clinical picture , characterised by chest pain , electrocardiographic changes and alterations in serum inammatory markers . 
often no further imaging besides transthoracic echocardiography is required [ 133 ]  . constrictive pericarditis constrictive pericarditis is a chronic pathological process characterised by fusion of the parietal and visceral layers of the pericardium , with transformation of the pericardial sac into a relatively non - expandable brous or brocalcied rind that encloses the heart muscle , thereby causing severe impairment in diastolic lling . 
therefore , a correct denition of this condition requires combined morphological and functional studies . in the typical forms with thickened pericardium , the diagnosis can be made by combining the clinical data with the classic echocardiographic ndings of thickening of the serosal pericardium ( > 5 mm ) , paradoxical motion of the interventricular septum and a variable degree of diastolic dysfunction [ 132136 ]  . the diagnostic contribution of cmr in the classic forms of pericardial thickening is therefore the same as that of echocardiography , providing conrmation of the ultrasound radiol med ( 2013 ) 118 : 752798 sulla funzione diastolica di versamenti cospicui , in cui la presenza di abbondante versamento con nestra acustica non ottimale non consente in alcuni casi unaccurata valutazione morfo - funzionale ecocardiograca ( classe i ) [ 132134 ]  . nel tamponamento cardiaco , tuttavia , la rmc ha un ruolo limitato in considerazione della natura acuta e della necessit di rapido intervento ( classe iii ) [ 133 ]  . 
 anomalie congenite complessivamente rappresentano entit rare dovute allanomalo sviluppo embriogenico intrauterino del pericardio in cui la rmc rappresenta la metodica di prima scelta per la caratterizzazione e la diagnosi . i difetti parziali o completi sono in genere ben valutabili sia con le sequenze cine - ssfp che tse , con cui possibile visualizzare sia lestensione del difetto sieroso che lentit dellerniazione cardiaca nellemitorace sinistro , che spesso si associa a tali alterazioni . 
una relativa difcolt pu presentarsi nei difetti parziali che interessano la parete laterale ventricolare sinistra , ove il pericardio risulta meno visualizzabile in rm . in aggiunta , nei difetti congeniti , la metodica pu consentire di valutare in modo combinato anche le anomalie complesse spesso associate , sia cardiache ( tetralogia di fallot , difetti interatriali , perviet del botallo ecc . ) che extracardiache ( ernia iatale , cisti broncogene , ipoplasia polmonare ) [ 2 , 3 ]  . i diverticoli pericardici , estremamente rari , sono estroessioni focali del foglietto viscerale attraverso difetti del foglietto parietale , in cui la rmc pu fornire un utile supporto per la diagnosi e la valutazione pre - operatoria [ 2 ]  . nelle cisti pleuro - pericardiche , la rmc dovrebbe essere considerata la metodica di riferimento per la caratterizzazione e la diagnosi differenziale , grazie alla combinazione di sequenze tse pesate in t1 e t2 . 
the transthoracic approach is usually sufcient , but when inadequate , transoesophageal echocardiography overcomes the limits of a poor acoustic window [ 137 ]  . cmr is complementary to echocardiography ; it is used in particular when there is an inadequate transthoracic acoustic window and transoesophageal echocardiography cannot necessita in genere di integrazione con esami di ii livello nelle forme con quadro tipico . la rmc invece pu essere utile nella caratterizzazione tissutale dei versamenti complessi , non anecogeni e per lidenticazione di eventuale tessuto solido presente allinterno dei foglietti . 
la metodica consente di identicare ledema e gli ispessimenti dei foglietti sierosi associati alla ogosi sia con le sequenze tse - stir che in cine - ssfp , in cui possibile valutare anche la mobilit dei foglietti sierosi [ 132134 ]  . 
 una situazione clinica peculiare riguarda le pericarditi post - infartuali , sia epistenocardiche che nella forma autoimmune ( sindrome di dressler ) , in cui il pattern di late enhancement dellinfarto si associa a un intenso potenziamento dei foglietti pericardici e con un un quadro clinico peculiare , che spesso non necessit di ulteriore imaging oltre lesame ecocardiograco transtoracico , e caratterizzato da dolore toracico , modicazioni ecg e movimento sierologico degli indici di ogosi [ 133 ]  . pericardite costrittiva la pericardite costrittiva ( pc ) un processo morboso cronico , caratterizzato dalla fusione dei foglietti parietale e viscerale , con trasformazione del sacco pericardico in una cotenna brosa o brocalcica , relativamente inestensibile , che avvolge il muscolo cardiaco determinando grave decit del riempimento diastolico . 
furthermore , the introduction of ssfp sequences , now commonly used in cine mr , has further improved the contrast as well as the spatial resolution , given that the shorter acquisition times enable the use of higher matrices , with consequent increased in - plane resolution . 
overall , the level of indication for mr studies of valve morphology , la disfunzione diastolica e la modicazione delle velocit di riempimento possono essere valutate con le sequenze venc in rmc . la rmc rappresenta invece indicazione clinica di i classe nelle forme costrittive con pericardio non ispessito ( < 5 mm ) , in cui la metodica pu essere di notevole supporto rispetto allecocardiograa documentando con elevato dettaglio morfologico anche piccoli ispessimenti focali , poco identicabili con ultrasuoni , potenzialmente responsabili di quadri clinici anche rilevanti [ 133 , 134 , 137 ]  . una situazione clinica peculiare , in cui emerso il ruolo della rmc , riguarda la differenziazione tra pc e cardiomiopatia restrittiva ( cmr ) , in cui presente una ridotta distensibilit dei ventricoli , che presentano dimensioni normali e con dinamica sistolica normale o poco alterata con un quadro funzionale sostanzialmente sovrapponibile tra le due condizioni ; la diagnosi differenziale tra le due condizioni patologiche tuttavia di grandissima importanza , in quanto i pazienti con pc giovano della terapia chirurgia con pericardiotomia , a differenza di quelli con cmr [ 4 , 5 ]  . in questa situazione clinica lutilizzo di sequenze ssfp con tecnica real - time consente di visualizzare lalterata motilit del setto interventricolare durante la respirazione con movimento paradosso tipico nella pc e conservata convessit nella cmr ( tabella 11 ) [ 135 , 136 ]  . valvulopatie lo studio delle valvole cardiache appannaggio , in prima istanza , dellecocardiograa , data la sua ampia disponibilit , il basso costo e il superiore dettaglio morfologico , che consente unottimale denizione dei lembi valvolari ; il completamento doppler consente di ottenere le informazioni funzionali necessarie allinquadramento clinico del paziente . 
normalmente lapproccio transtoracico sufciente ma , ove carente , laccesso transesofageo consente di superare i limiti della scarsa nestra acustica [ 137 ]  . la rmc complementare allecocardiograa ; a essa , in particolare , si ricorre in caso di insufciente nestra acustica transtoracica e accesso transesofageo non eseguibile , non disponibile o riutato dal paziente [ 138 ]  . le sequenze a sangue nero in apnea permettono una visualizzazione dei lembi valvolari in circa l85% dei casi , data la limitata risoluzione spaziale e di contrasto della tecnica . 
this is important in cases of valve disease in which a precise evaluation of systolic ventricular function is clinically indicated , as for example in patients with aortic regurgitation ; in these cases , as stated in the above - cited document , the indication for mr studies is class i . however , poor ow sensitivity is one limitation of ssfp sequences : proton dephasing , caused by the ow turbulence resulting from the valve disease , produces a net signal intensity decrease in the ow - void phenomenon , which is known to occur with traditional cine mr techniques . 
for a long time , evaluation of the ow void has been the main method in estimating valve dysfunction , although it is exclusively a qualitative method . consequently , a method that is nding wide indications in the study of valve diseases is cine phase - contrast imaging , which enables calculation of the ow velocity and , in a plane perpendicular to the ow , of output . 
these data can then be used to calculate the regurgitant volume and fraction , comparing the stroke volumes of the two ventricles in the case of a regurgitant valve and the pressure gradient in the case of a stenotic one ( table 12 ) [ 139 , 140 ]  . left atrium and pulmonary veins cardiac veins left atrium pulmonary vein complex the electrophysiological procedures of transcatheter ablation of the pulmonary veins [ 141 , 142 ] to eliminate the trigger of atrial brillation require precise knowledge of the complex and extremely variable anatomy of the region [ 143145 ]  . 
 post - processing ( mpr / mip , 3d epicardial and endocardial volume rendering ) of mr angiography images enables identication of many variants of pulmonary vein drainage into the left atrium ( supranumerary veins and common trunks ) [ 143 , 147 ] , branching of the conuence of the piano . 
tuttavia , unimportante indicazione rappresentata dallo studio della valvola aortica bicuspide , specie se associata a dilatazione del bulbo aortico e dellaorta ascendente , essendo la rm pi accurata dellecocardiograa in tale misurazione ; in questo caso lindicazione viene posta in classe i . come noto , la superiore risoluzione di contrasto delle sequenze ssfp alla base dellottimale visualizzazione dei contorni endoed epicardico , vantaggio che alla base della denizione della cine - rm come gold standard per il calcolo della funzione sistolica segmentaria e globale e della massa . 
tale aspetto risulta quindi importante quando , in caso di valvulopatia , sia clinicamente indicata una precisa valutazione della funzione ventricolare sistolica , ad esempio nei pazienti con insufcienza aortica ; ne consegue , in accordo con il documento succitato , lindicazione in classe i . una limitazione delle sequenze ssfp comunque rappresentata dalla scarsa sensibilit al usso , per cui il defasamento protonico causato dalle turbolenze di usso indotte da una valvulopatia determina una netta riduzione del fenomeno di ow void ben noto con le tecniche di cine - rm convenzionali . 
la valutazione del ow void ha per lungo tempo costituito il principale metodo di stima del vizio valvolare , ma esso rappresenta esclusivamente un metodo qualitativo . conseguentemente , una sequenza che trova ampia indicazione nello studio delle valvulopatie la cine phase contrast , che consente di calcolare la velocit di usso e , in un piano perpendicolare alla direzione del usso , la portata . 
 ci permette quindi il calcolo del volume e della frazione di rigurgito , comparando le gittate sistoliche dei due ventricoli , in caso di insufcienza valvolare , e del gra diente pressorio in caso di stenosi valvolare ( tabella 12 ) [ 139 , 140 ]  . atrio sinistro e vene polmonari vene cardiache complesso atrio sinistro vene polmonari le procedure elettrosiologiche di ablazione transcatetere delle vene polmonari ( vp ) [ 141 , 142 ] , responsabili dellinnesco della brillazione atriale ( fa ) , richiedono una precisa conoscenza della complessa anatomia di questa regione , caratterizzata da unestrema variabilit [ 143145 ]  . 
la rmc , al pari della tcmd ( tc multidetettore ) , in grado di fornire una dettagliata road map per le procedure di ablazione , indispensabile per migliorarne lefcacia terapeutica , ridurne la durata e limitare le possibili complicanze 788 radiol med ( 2013 ) 118 : 752798 table 12 indications for mr in patients with cardiac valve disease indications class valve morphology : bicuspid aortic valve valve morphology : vegetations , papilloma , paravalvular abscesses quantication of global right and left ventricular systolic function quantication of left ventricular mass quantication of valve regurgitation quantication of valvular stenosis planimetry of the aortic valve tabella 12 indicazioni alla rm nelle valvulopatie indicazioni classe morfologia valvolare : valvola aortica bicuspide morfologia valvolare : vegetazioni , papillomi , ascessi paravalvolari quantizzazione funzione sistolica globale ventricolare destra e sinistra quantizzazione massa ventricolare sinistra quantizzazione insufcienza valvolare quantizzazione stenosi valvolare planimetria valvola aortica iii veins , morphology of the ostia [ 148 ] , and calculation of the atrial volumes [ 149 ]  . 
according to some authors , cmr is less accurate than echocardiography in detecting the presence of any thrombi in the left atrial appendage , a condition which contraindicates an ablation procedure [ 151 ]  . 
cmr is also useful in the followup of patients who have undergone an ablation procedure : a follow - up examination 3 months after the procedure will easily show any narrowing of the lumen of the vein [ 152 ]  . 
the possibility of integrating images produced by cmr with electro - anatomical maps , derived from navigation systems used by the electrophysiologists during the ablation procedures , further improves the interventions , also in terms of reducing radiation dose by shortening uoroscopy time [ 153156 ]  . 
recently published articles suggest that late - enhancement techniques could play a role in identifying the formation of post - ablation atrial brosis , with the purpose of verifying the efcacy of the ablation procedure [ 157159 ]  . 
le sequenze angio - rm forniscono immagini il cui post - processing ( mpr / mip , volume rendering 3d epicardico ed endocardico ) consente lidenticazione delle numerose varianti di conuenza delle vp nellatrio sinistro ( vene sovrannumerarie e tronchi comuni ) [ 143 , 147 ] , del branching di conuenza delle vene , della morfologia degli osti [ 148 ] e il calcolo dei volumi atriali [ 149 ]  . 
secondo alcuni autori , la rmc meno accurata rispetto allecocardiograa nel rilevare la presenza di eventuali trombi dellauricola sinistra , condizione che controindica la procedura di ablazione [ 151 ]  . 
inoltre , la rmc utile anche nel follow - up dei pazienti sottoposti alla procedura di ablazione : lesame eseguito dopo 3 mesi permette di riconoscere agevolmente eventuali restringimenti del lume venoso [ 152 ]  . 
la possibilit di integrare le immagini realizzate mediante rmc con le mappe elettro - anatomiche , derivate dai sistemi di navigazione utilizzati dagli elettrosiologi durante le procedure di ablazione , consente di ottimizzare ulteriormente le procedure interventistiche , anche in termini di riduzione di dose radiante , stante la contrazione dei tempi di uoroscopia [ 153156 ]  . 
recentemente sono comparsi in letteratura alcuni articoli che suggeriscono come la tecnica del late enhancement ( lge ) possa avere un ruolo nellidenticazione della formazione della brosi atriale post - ablazione , allo scopo di vericare lefcacia della procedura interventistica [ 157159 ]  . 
le sequenze di lge potrebbero essere utili anche nella straticazione dei pazienti da candidare allablazione [ 160 ]  . vene cardiache la precisa conoscenza anatomica delle vene cardiache , caratterizzata da una discreta variabilit [ 161 , 162 ] , di grande importanza negli interventi di resincronizzazione cardiaca ( pacing biventricolare o crt ) , riservata ad alcuni pazienti affetti da scompenso cardiaco [ 163 , 164 ] , in grado di fornire un considerevole benecio sui sintomi e di ridurre la mortalit . 
nel pacing biventricolare , oltre al posizionamento di un elettrodo stimolatore a livello della supercie endocardica dellapice del ventricolo destro , si inserisce un secondo elettrodo epicardico a livello del ventricolo sinistro , generalmente in corrispondenza della parete postero - laterale , la porzione ventricolare che si attiva pi tardivamente , pertanto responsabile della desincronizzazione intra - ventricolare , cui consegue una riduzione della frazione di eiezione . 
in biventricular pacing , besides placing a stimulating electrode in the endocardial surface of the apex of the right ventricle , a second epicardial electrode is introduced into the left ventricle , generally in the postero - lateral wall , which is the part of the ventricle that is activated later and is therefore responsible for the intraventricular desynchronisation , that causes a reduction in ejection fraction . 
in over 90% of patients the left ventricular electrode can be placed using a transvenous approach , trying to introduce the stimulator into a postero - lateral branch or target ve the success of the procedure is dependent on the knowledge of the cardiac veins anatomy : retrograde venography is diagnostic in only 67% of patients , either because the coronary sinus cannot be cannulated or because of inadequate occlusion of the vessel by the balloon , that prevents backwash of the contrast agent injected countercurrent in order to opacify the cardiac veins ( table 13 ) [ 161 ]  . 
there are some recent reports of studies on the possible role of mr in the evaluation of the cardiac venous system , using whole - heart angiographic - like sequences with or without the administration of contrast agents [ 165169 ]  . 
combining the study of the cardiac veins with an evaluation of myocardial motion and viability through mr could be extremely useful in patients with heart failure who are candidates for cardiac resynchronisation therapy . spectroscopy magnetic resonance spectroscopy ( mrs ) is the only technique that can open a non - invasive window on myocardial metabolism , without using ionising radiation and external rale o vena target . 
il successo della procedura vincolato alla conoscenza dellanatomia delle vene cardiache : la venograa retrograda risulta diagnostica solo nel 67% dei pazienti a causa dellimpossibilit di incannulare il seno coronarico o dellinadeguata occlusione vasale da parte del palloncino che impedisce il lavaggio ( backwash ) del mezzo di contrasto iniettato controcorrente per lopacizzazione delle vc ( tabella 13 ) [ 161 ]  . 
recentemente alcuni lavori della letteratura hanno indagato il possibile ruolo della rm nella valutazione del sistema venoso cardiaco , attraverso lutilizzo di sequenze simil - angiograche whole - heart con o senza somministrazione di mezzo di contrasto [ 165 169 ]  . 
lassociazione dello studio delle vene cardiache con la valutazione della motilit e della vitalit miocardiche mediante rm potrebbe rivelarsi estremamente utile nei pazienti con scompenso cardiaco candidati alla crt . spettroscopia la spettroscopia a risonanza magnetica ( magnetic resonance spectroscopy , mrs ) apre una nestra non invasiva sul metabolismo miocardico , senza utilizzare radiazioni ionizzanti o traccianti esogeni . 
in mrs il segnale origina dai nuclei di idrogeno ( 1h ) o da altri nuclei con momento magnetico diverso da zero , come il fosforo 31 ( 31p ) o il carbonio 13 ( 13c )  . la 13c - mrs valuta dinamicamente i ussi dei substrati miocardici e il metabolismo del ciclo di krebs , come dimostrato in studi sperimentali preclinici [ 170 ]  . 
tuttavia , lapplicazione clinica della 13c - mrs stata nora ostacolata dalla bassa sensibilit e , quindi , dalla necessit di somministrare precursori esogeni arricchiti di 13c o di 2 - 13c iperpolarizzato . 
it detects signals from hydrogen nuclei ( 1h ) or from other nuclei with magnetic moments different from zero , such as 31phosphorus ( 31p ) or 13carbon ( 13c )  . preclinical studies have shown that 13c - mrs provides a real - time assessment of myocardial substrate selection and krebs cycle metabolism [ 170 ]  . 
however , no clinical cardiac studies have been performed using 13c - mrs so far , due to the low sensitivity and the need to administer exogenous 13c - enriched or hyperpolarised [ 2 - 13c ] - enriched precursors . conversely , 1h - mrs has been applied in both animal models and humans . 
1h - mrs based measurements of the local concentration of the creatine pool in the myocardium [ 171 , 172 ] can differentiate viable ( total creatine 26 mol / g ) from infarcted non - viable myocardium ( total creatine 10 mol / g ) [ 171 ]  . 
myocardial creatine depletion has also been found in patients with dilated and hypertrophic cardiomyopathy with a signicant association with other markers of the severity of heart failure [ 173 ]  . 
moreover , the possibility of quantifying intramyocardial mobile lipids through 1h - mrs has recently attracted growing interest because of the popularity of theories about lipid overstorage and lipotoxic injury to myocytes in the pathogenesis of cardiac dysfunction in type - 2 diabetes and obesity [ 174176 ]  . however , the majority of human cardiac mrs studies have been focused on metabolites including a 31p nucleus as the molecular target ( high - energy phosphates )  . 
a typical 31p - spectrum from a human heart shows beta - , alphaand gammaadenosine triphosphate ( atp ) , phosphocreatine ( pcr ) , phosphodiesters , phosphomonoesters , and inorganic phosphates . 
the heart is the organ which needs the greatest amount of energy per mass unit : in the pathogenesis of cardiac dysfunction in several diseases , a mismatch between energy demand and supply is involved [ 179 ]  . 
pcr is a sort of cellular reservoir of energy : when atp demand exceeds atp synthesis , such as in ischaemic conditions , pcr is consumed to maintain the atp concentration constant , resulting in a decreased pcr / atp ratio [ 180 ]  . 
la misurazio ne del pool totale di creatina attraverso 1h - mrs [ 171 , 172 ] consente di differenziare il miocardio vitale ( creatina totale 26 mol / g ) dal miocardio infartuato non vitale ( creatina totale 10 mol / g ) [ 171 ]  . 
la deplezione della creatina miocardica stata dimostrata anche in pazienti con cardiomiopatia dilatativa e ipertroca , con signicati va correlazione con altri marker di gravit dello scompenso cardiaco [ 173 ]  . 
inoltre , la possibilit di quanticare i lipidi mobili intramiocardici attraverso l1h - mrs ha recentemente suscitato crescente interesse data la popolari t delle teorie riguardanti loverstorage di lipidi e il dan no miocitario lipotossico nella patogenesi della disfunzione cardiaca in pazienti con diabete di tipo 2 e obesit [ 174176 ]  . tuttavia , la maggior parte degli studi di mrs cardiaca nelluomo ha avuto come target il 31p ovvero i fosfati ad alta energia . 
il tipico spettro miocardico del 31p , ottenuto per la prima volta nelluomo negli anni ottanta [ 177 ] , consente di riconoscere : beta - , alfae gammaadenosina trifosfato ( atp ) , fosfocreatina ( pcr ) , fosfodiesteri , fosfomonoesteri , e fosfato inorganico . 
un parametro metabolico ampiamete utilizzato in 31p - mrs il rapporto fosfocreatina / adenosina trifosfato ( pcr / atp ) [ 178 ] , il cui signicato deriva dal ruolo della reazione creatina - chinasi ( ck ) nel controllo termodinamico dei miociti . 
il cuore lorgano dellorganismo che richiede il maggior apporto di energia per unit di massa e uno squilibrio fra richiesta e apporto di energia coinvolto nella patogenesi della disfunzione cardiaca in molte patologie [ 179 ]  . 
la ck mantiene bassa la concentrazione delladenosina difosfato ( adp ) intorno ai mitocondri , convertendo adp in atp . latp costituisce il carburante di tutte le attivit delle miobrille , prime fra tutte il rilasciamento diastolico e la contrazione sistolica . 
la pcr una sorta di riserva energetica cellulare : quando la richiesta di atp eccede la sua sintesi , come in condizioni dischemia , la pcr consumata per mantenere costante la concentrazione di atp , con conseguente decremento del rapporto pcr / atp [ 180 ]  . 
il rapporto pcr / atp pu anche ridursi in caso di decremento del pool totale di creatina , come accade nello scompenso cardiaco [ 173 ]  . nel vasto capitolo dellipertroa cardiaca , il rapporto pcr / atp permette di differenziare lipertroa compensatoria del cuore datleta ( normale rapporto pcr / atp ) [ 181 , 182 ] dalla cardiopatia ipertroca ipertensiva [ 183 ] o dalla cardiomiopatia ipertroca ( ridotto rapporto pcr / atp ) [ 184 , 185 ]  . 
 in the broad context of cardiac hypertrophy , 31p - mrs can be used to differentiate the adaptive hypertrophy of differenti studi hanno dimostrato che la 31p - mrs pu identicare le conseguenze biochimiche delle prime fasi radiol med ( 2013 ) 118 : 752798 the athletes heart ( normal pcr / atp ratio ) [ 181 , 182 ] from hypertensive hypertrophy [ 183 ] or hypertrophic cardiomyopathy [ 184 , 185 ] ( impaired pcr / atp ratio )  . 
the stress - induced reduction of the pcr / atp contributed to the suggestion of microvascular ischaemia as a pathogenic mechanism of chest pain in syndrome x , indicating a potential important diagnostic and prognostic role for 31p - mrs in this disease [ 187 , 188 ]  . a decreased pcr / atp ratio is also a characteristic feature of heart failure [ 189 ] , although pcr / atp underestimates the true impairment of cardiac energy metabolism in these patients . 
in fact , absolute quantication studies by 31p - mrs performed using the sloop technique demonstrated a 51% decrease in pcr levels associated with a 35% reduction in atp , resulting in a limited decrease ( 25% ) in the pcr / atp ratio [ 190 ]  . 
nevertheless , a decreased pcr / atp had a strong prognostic value in dilated cardiomyopathy , being able to predict either total or specic mortality better than both new york heart association ( nyha ) functional class and left ventricular ejection fraction [ 191 ]  . 
finally , a pathogenic role of impaired energy metabolism in the determination of cardiac dysfunction in patients with type - 1 and type - 2 diabetes has been suggested from 31p - mrs studies [ 193 , 194 ]  . in conclusion , despite the relevance of the diagnostic and prognostic information provided by 1h - mrs and 31p - mrs , as well as the lack of other techniques able to offer the same non - invasive evaluation , cardiac mrs is currently still limited to the research setting and is not included in protocols for routine clinical use , mainly because of methodological complexity , technical limitations , and lack of standardisation [ 178 ]  . 
however , there are still some signicant limitations , such as the low spatial resolution , hindering the possibility of detecting regional metabolic myocardial inhomogeneities , relatively long acquisition times , the need for a dedicated coil for 31p - mrs and , nally , the variability of measurements making data obtained in different mr laboratories not comparable [ 195 ]  . 
ultrahigheld magnets ( 7 t or higher ) will provide improvements in signal - to - noise ratio , and spatial and spectral resolution of myocardial mrs . conict of interest none della cascata ischemica miocardica . 
la riduzione del rapporto pcr / atp durante stress ha anche contribuito a suggerire la patogenesi ischemica microvascolare del dolore precordiale nella sindrome x , patologia nella quale la 31p - mrs potrebbe rivestire un importante ruolo diagnostico e prognostico [ 187 , 188 ]  . 
infatti , studi di quanticazione assoluta mediante 31p - mrs con tecnica sloop hanno evidenziato una riduzione del 51% nei livelli di pcr associata a una riduzione del 35% dellatp , con conseguente limitato decremento ( - 25% ) del rapporto pcr / atp [ 190 ]  . 
la riduzione di tale rapporto ha comunque un forte valore prognostico in pazienti con cardiomiopatia dilatativa essendo un predittore indipendente di mortalit totale e di mortalit specica , migliore di quanto lo siano la classe funzionale della new york heart association ( nyha class ) e la frazione deiezione del ventricolo sinistro [ 191 ]  . 
inoltre , unapplicazione rilevante della 31p - mrs la valutazione della risposta miocardica in pazienti sottoposti a modulazione farmacologica del metabolismo cardiaco [ 192 ]  . inne , studi di 31p - mrs hanno suggerito come lalterazione del metabolismo energetico svolga un ruolo patogenetico nel determinare la disfunzione cardiaca in pazienti con diabete di tipo 1 e 2 [ 193 , 194 ]  . in conclusione , nonostante la rilevanza delle informazioni diagnostiche e prognostiche ottenibili attraverso 1hmrs e 31p - mrs e la non disponibilit di altre tecniche non invasive alternative , la mrs cardiaca rimane connata nellambito della ricerca e non inclusa nella routine clinica , principalmente a causa della complessit metodologica , dei limiti tecnici e della carenza di standardizzazione [ 178 ]  . 
permangono tuttavia limitazioni rilevanti quali la bassa risoluzione spaziale , che ostacola lidenticazione di disomogeneit regionali del metabolismo miocardico , i tempi di acquisizione relativamente lunghi , la necessit di utilizzare bobine dedicate per la 31p - mrs e , inne , la variabilit delle misurazioni , che rende poco confrontabili i risultati ottenuti con apparecchiature diverse [ 195 ]  . 
miglioramenti in termini di rapporto segnale / rumore e di risoluzione spaziale e spettrale della mrs miocardica saranno possibili con limpiego di apparecchiature operanti a 7 t e oltre . 792 radiol med ( 2013 ) 118 : 752798 8 . 
cova1 1uco di radiologia , dipartimento di scienze mediche , chirurgiche e della salute , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , trieste , italy 2uco di chirurgia plastica , dipartimento di scienze mediche , chirurgiche e della salute , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , trieste , italy correspondence to : a . 
diep were always depicted ( n = 81 ) and subdivided according to taylors classication into type i ( 65% ) , type ii ( 28% ) , and type iii ( 7% )  . 
le angio - tc sono state effettuate con una tc a 64 - detettori durante liniezione di 100 ml di mezzo di contrasto ( mdc ) con usso di 4 , 5 ml / s . 
le arterie epigastriche inferiori profonde sono state sempre visualizzate ( n = 81 ) , classicate secondo taylor in : tipo i 65% , tipo ii 28% , tipo iii 7% . 
la qualit dellopacizzazione vascolare stata ottimale in 30 casi su 41 , mentre si registrata sovrapposizione venosa per fase arteriosa tardiva in 8 indagini su 41 ed opacizzazione subottimale per radiol med ( 2013 ) 118 : 732743 requires careful optimisation owing to the critical timing of opacication typical of that vascular district . 
lo studio dei vasi perforanti con angiotc rappresenta un utile supporto per la pianicazione dellintervento di ricostruzione mammaria , ma richiede unottimizzazione dellindagine per la tempistica di opacizzazione critica di tali vasi . 
a variety of different donor sites and surgical techniques have been described for autologous tissue transplantation . the use of a deep inferior epigastric perforator ( diep ) ap is the most appropriate surgical option for autologous breast reconstruction provided that a team with experience in microsurgical techniques is available . 
compared with the traditional myocutaneous technique , diep involves the use of cutaneous and subcutaneous tissues , with sparing of the muscle layers and less morbidity at the donor site , less postoperative pain and shorter recovery times [ 3 ]  . 
in agreement with the moon and taylor classication [ 7 ] , the branching pattern of collateral vessels may be classied as type i ( single trunk ) , type ii ( bifurcation into two trunks ) and type iii ( division into more than two trunks )  . the supercial inferior epigastric artery ( siea ) ap is a good alternative to the diep ap in autologous tissue reconstruction . 
clinical studies show that the siea can be identied in 1015% of the population , even though small - scale anatomical studies report a higher prevalence [ 4 , 8 ]  . previous studies demonstrated that computed tomography angiography ( cta ) of the abdominal wall is a highly accurate method for studying abdominal perforator arteries , having 96100% sensitivity and 95100% specicity [ 9 11 ]  . 
the use of preoperative cta shortens operative time , reduces postoperative complications [ 12 ] , depicts perforala ricostruzione mammaria una tappa fondamentale nel trattamento delle pazienti affette da carcinoma mammario . 
 lintervento di ricostruzione per tecnicamente pi complesso rispetto al semplice impianto di una protesi ed i rischi di complicanza post - operatoria sono maggiori [ 1 , 2 ]  . 
 sono stati descritti una variet di differenti siti donatori per effettuare il trapianto autologo , utilizzando svariate differenti tecniche chirurgiche . lutilizzo del lembo con rami perforanti dellarteria epigastrica inferiore ( diep ) risulta lopzione chirurgica ottimale per la ricostruzione di mammella autologa , sempre che sia disponibile un team in grado di utilizzare tecniche microchirurgiche . 
paragonata alla tecnica tradizionale miocutanea la diep prevede lutilizzo di cute e sottocute , con risparmio dei piani muscolari , con minor morbilit del sito donatore , minor dolore post - operatorio e tempi di recupero minori [ 3 ]  . 
in accordo con moon e taylor [ 7 ] la disposizione dei rami collaterali si pu classicare nel tipo i ( branca singola ) , tipo ii ( tronco biforcato ) e tipo iii ( con pi di 2 divisioni )  . il lembo confezionato con larteria epigastrica inferiore superciale ( siea ) una valida alternativa al lembo con diep negli interventi di ricostruzione con tessuto autologo . 
da studi clinici risulta come la siea sia osservata nel 10%15% della popolazione , anche se studi anatomici su piccola scala riportano prevalenze superiori [ 4 , 8 ]  . studi precedenti dimostrano come langio - tomograa computerizzata ( tc ) della parete addominale rappresenti una tecnica dotata di elevata accuratezza per lo studio delle 734 fig . 
cta of the abdominal wall for vascular mapping has been described in detail , and its superiority over other imaging techniques , in particular , colour doppler ultrasound , has been demonstrated [ 14 ]  . 
mean patient age was 57 [ range , 3774 ; radiol med ( 2013 ) 118 : 732743 arterie perforanti addominali , presentando una sensibilit del 96%100% ed una specicit del 95%100% [ 911 ]  . 
lindagine angio - tc in grado di individuare le arterie perforanti sino ad un calibro di 0 , 3 mm , di fornirne una precisa localizzazione e di indicarne con precisione il decorso intra - muscolare ed a livello del sottocute [ 13 ]  . 
tutte le pazienti avevano indicazione allintervento di mastectomia per neoplasia mammaria : in 32 / 41 pazienti ( 78% dei casi ) stato previsto un intervento combinato con un solo tempo chirurgico , mentre nelle restanti 9 pazienti ( 22% dei casi ) si preferito eseguire la ricostruzione in un secondo tempo . 
la ricostruzione stata in un solo caso bilaterale , mentre nei restanti 40 casi stato effettuato un intervento monolaterale . tecnica tc per poter fornire al chirurgo sulle immagini tc i reperi anatomici a livello della parete addominale necessari per il confezionamento del lembo , risultato necessario che la posizione della paziente sul lettino tc riproducesse quanto pi possibile quella assunta sul tavolo operatorio ; per tale motivo si evitato di posizionare la paziente con le braccia sollevate sopra le spalle , al ne di evitare che la cute addominale fosse stirata cranialmente e che la cicatrice ombelicale ( utilizzata come sede di repere ) venisse dislocata . 
the indication for mastectomy was breast cancer in all patients : in 32 / 41 patients ( 78% ) , mastectomy and reconstruction were performed in a single surgical session , whereas in the remaining nine patients ( 22% ) , reconstruction was performed at a later date . 
reconstruction was bilateral in one case only and unilateral in the remaining 40 . ct technique to provide the surgeon with ct images showing the anatomical landmarks necessary to harvest the ap , the patients position on the ct bed must simulate her position on the operating table . 
for this reason and to prevent abdominal skin from being stretched cranially and the umbilical scar ( used as a landmark ) from being dislocated , the patient was not placed with arms raised above the shoulders . 
the examination was performed after removal of all clothing from the chest and abdomen to avoid macroscopic compression and distortion of the subcutaneous soft tissues , which would produce errors in the reference coordinate system used for marking vessel position . 
breath - holding instructions were clear and repeated several times to limit motion artefacts due to subcutaneous tissues of the abdominal wall being more mobile than the intra - abdominal structures . 
 cta was performed using a 64 - slice multidetector - row ct scanner ( aquilion 64 , toshiba medical systems , tokyo , japan ) with the following scan parameters : slice thickness , 640.5 mm ; rotation time , 0.4 s ; pitch , 1.66 ; x - ray tube parameters , 120 kv , 300 ma . 
le istruzioni alla paziente riguardo al mantenimento dellapnea sono state chiare e ripetute pi volte , al ne di limitare gli artefatti da movimento dovuti al fatto che i tessuti sottocutanei della parete addominale sono pi mobili rispetto alle strutture endo - addominali . 
 le indagini di angio - tc sono state eseguite mediante apparecchiatura tc multislice a 64 strati ( aquilion 64 ; toshiba medical systems , tokyo , giappone ) , utilizzando i seguenti parametri di scansione : spessore di strato 640 , 5 mm , tempo di rotazione 0 , 4 s , pitch 1 , 66 ; parametri del tubo radiogeno 120 kv , 300 ma . 
il volume acquisito comprendeva una regione limitata superiormente da un piano passante circa 5 cm cranialmente rispetto alla cicatrice ombelicale e inferiormente da un piano passante subito al di sotto del piccolo trocantere . 
 il dataset di immagini stato analizzato in consenso da due radiologi con almeno 5 anni esperienza di imaging vascolare mediante una workstation dedicata ( vitrea 2 , vital images , usa )  . 
sono state eseguite le seguenti ricostruzioni : ricostruzione maximum intensity projection ( mip ) sul piano coronale con spessore di 25 mm , posizionata anteriormente , con il ne di includere completamente il decorso della diea , dalle arterie iliache cranialmente sino al medio addome . 
tale ricostruzione utile per visualizzare posizione , calibro e disposizione delle branche laterali di entrambe le diea , nonch la presenza di rami siea incostanti ; mip assiale , sagittale e coronale da 5 mm con marcatura 736 radiol med ( 2013 ) 118 : 732743 figure 2a - c a 5 - mm maximum intensity projection ( mip ) reconstruction in axial , sagittal and coronal planes . 
 the image data set was analysed consensually on a dedicated workstation ( vitrea 2 , vital images , usa ) by two radiologists with at least 5 years of experience in vascular imaging . 
the following reconstructions were obtained : 25 - mm - thick coronal maximum intensity projection ( mip ) reconstruction : performed in the anterior position with the aim of including the entire diea course from the iliac arteries to the middle abdomen . 
lutilizzo di immagini riformattate con tecnica mip consente di valutare oltre al calibro del vaso perforante , anche la lunghezza del suo decorso intramuscolare ; 3d surface rendering : la ricostruzione 3d della superradiol med ( 2013 ) 118 : 732743 cie cutanea , nella quale sono stati precedentemente evidenziati i siti di emergenza delle arterie perforanti , consente una loro precisa localizzazione sul piano cutaneo . 
un preset specico di impostazioni di visualizzazione ( window / level , transparency e color look up table ) sulla console consente di annullare il tessuto adiposo del sottocute per dimostrare in 3d unicamente i rami sottocutanei delle arterie perforanti . 
 le immagini assiali sono state poi valutate per la ricerca di eventuali reperti collaterali . i vasi perforanti utilizzati per il confezionamento dei lembi sono risultati sempre visibili e correttamente riconosciuti , eccetto in un singolo caso in cui il vaso perforante utilizzato per confezionare il lembo non stato evidenziato dallindagine tc ; la revisione delle immagini ha mostrato come tale struttura fosse in realt visibile , ma non adeguatamente valorizzata in fase di documentazione / refertazione . 
le diea sono state chiaramente visibili in 81 / 82 casi e la distribuzione dei rami collaterali secondo taylor stata la seguente : tipo i 65% ( n = 46 ) ; tipo ii 28% ( n = 20 ) ; tipo iii 7% ( n = 5 )  . 
 in una paziente , la diea destra non era visualizzabile ed erano apprezzabili circoli anastomotici con larteria epigastrica superiore profonda ; tale paziente , precedentemente appendicectomizzata , presentava verosimilmente danno iatrogeno di tale vaso . 
in 12 pazienti sono stati identicati reperti collaterali , consistenti in : angioma epatico ( 1 caso ) , adenoma surrenalico ( 1 caso ) , cisti renale semplice ( 2 casi ) , cisti renale a densit elevata ( 1 caso ) , idronefrosi monolaterale per sindrome del giunto pielofig . 
mip reformatted images provide an assessment of perforator calibre and length of its intramuscular course ; 3d surface rendering : the 3d reconstruction of the skin surface , on which the point of perforator surfacing has previously been identied , allows precise localisation of these points on the skin surface . 
specic visualisation settings ( window / level , transparency and colour look - up table ) on the console can cancel subcutaneous fat to depict only subcutaneous branches of the perforating arteries . axial images were subsequently analysed to identify any collateral ndings . 738 radiol med ( 2013 ) 118 : 732743 fig . 
c three dimensional volume rendered ( vr ) reconstruction of images acquired in the optimal arterial phase ( a ) only shows perforator arteries ; window / level and colour look - up table are set to exclude subcutaneous fat and unenhanced vessels . 
4a ricostruzione mip assiale di 5 mscansione acquisita nella fase arteriosa ottimale : le arterie perforanti ( freccia ) presentano densit molto pi alta delle vene , e possono essere facilmente differenziate dalle vene di accompagnamento ( punta di freccia )  . 
d ricostruzione mip 3d della scansione acquisita in fase arteriosa tardiva ( b ) : sono visibili vasi venosi prominenti , a rischio di essere scambiati per grosse arterie perforanti . results diea perforators used to harvest the aps were always visible and correctly identied on ct , except for a single case . 
on average , three perforating branches were ureterale ( 1 caso ) , leiomioma uterino ( 5 casi ) , disseminazione metastatica scheletrica ( 1 caso ) ( tabella 1 )  . 
nel caso di disseminazione metastatica scheletrica tale reperto ha comportato la sospensione dellintervento e ha indirizzato la paziente ad una chemioterapia neoadiuvante . discussione langio - tc pre - operatoria della parete addominale si rivelata una ottima tecnica per la pianicazione pre - operatoria negli interventi di ricostruzione mammaria mediante lembo confezionato con diep [ 1017 ]  . 
in linea con i dati della letteratura , che documentano una sensibilit dellangio - tc nello studio delle arterie perforanti addominali pari al 96%100% [ 911 ] , nella nostra esperienza le diea sono radiol med ( 2013 ) 118 : 732743 fig . 
b nelle immagini 3d volume rendering le perforanti acquisite in una fase arteriosa troppo precoce appaiono insufcientemente opacizzate . identied on the right ( range , 15 ; sd1 mm ) and two on the left ( range 15 ; sd1 mm )  . 
in 12 patients , additional incidental ndings were identied , namely : hepatic angioma ( one case ) ; adrenal adenoma ( one case ) ; simple renal cyst ( two cases ) ; high - density renal cyst ( one case ) ; unilateral hydronephrosis secondary to ureteropelvic junction obstruction ( one case ) ; uterine leiomyoma ( ve cases ) ; disseminated skeletal metastases ( one case ) ( table 1 )  . 
in this latter case , nding led to surgery being postponed to allow the patient to undergo adjuvant chemotherapy . discussion preoperative cta of the abdominal wall proved to be an excellent technique in the preoperative planning of breast reconstruction surgery with diep ap [ 1017 ]  . 
consistent with previous reports , which indicate 96100% cta sensitivity in studying abdominal perforating arteries [ 911 ] , in our experience , diea were clearly visible in all 41 patients , with bilateral visualisation in 40 patients , whereas siea , which have been reported in 1015% of the overall population [ 4 , 8 ] , were identied in 6 / 41 patients ( 15% ) , with bilateral visualisation in three cases . accessibility of multislice scanners , present in most mistate chiaramente visualizzate in tutte le 41 pazienti , con visualizzazione bilaterale in 40 pazienti , mentre le siea , presenti nella popolazione in una percentuale pari al 10% 15% , [ 4 , 8 ] sono state evidenziate in 6 / 41 pazienti ( 15% ) , con visualizzazione bilaterale in 3 casi . la disponibilit di apparecchiature multistrato , presenti nella maggior parte dei centri di riferimento per la chirurgia microvascolare , ne fa una tecnica ottimale e di facile accesso . 
tuttavia , per il raggiungimento di un risultato ottimale , questo tipo di esami richiede una conduzione tecnica rigorosa che prevede un posizionamento preciso della paziente sul lettino dellapparecchiatura tc ( supina a braccia conserte ) , lutilizzo di protocolli di acquisizione e di ricostruzione dedicati , nonch uninterpretazione accurata delle immagini . 
 nel nostro studio il posizionamento della paziente a braccia conserte e la rimozione di tutti gli indumenti al livello toraco - addominale hanno consentito di acquisire in tutti i casi immagini prive di artefatti da movimento e in grado di fornire al chirurgo i reperi anatomici a livello della parete addominale necessari per il confezionamento del lembo cutaneo . 
la rimozione sistematica degli indumenti stata suggerita solo recentemente da alcuni autori riguardo allesecuzione di angio - tc della parete addominale [ 15 ] , mentre in altre esperienze non vi si fa menzione [ 9 , 16 ]  . per quanto riguarda lesecuzione dellesame , se da una parte la modalit di iniezione del mezzo di contrasto non dissimile da quella delle angio - tc convenzionali , dallaltra la tempistica di acquisizione delle immagini per evidenziare i vasi perforanti addominali di difcile impostazione . 
 lacquisizione , infatti , deve avvenire in una fase arteriosa 740 finding table 1 incidental ndings observed in computed tomography angiography ( cta ) patients ( n ) further investigation radiol med ( 2013 ) 118 : 732743 fibromas simple renal cyst hepatic angioma adrenal adenoma high - density renal cyst hydronephrosis , ureteropelvic junction 1 disseminated bone metastases none none ultrasound additional scan phase obtained during same examination additional scan phase obtained during same examination ultrasound follow - up bone scan tabella 1 reperti collaterali osservati in corso di angio - tomograa computerizzata ( angio - tc ) reperto pazienti ( n ) indagini successive fibroma cisti renale semplice angioma epatico adenoma surrenalico cisti renale densa idronefrosi ; sindrome del giunto metastasi ossee disseminate nulla nulla approfondimento ecograco ulteriore scansione tc effettuata contestualmente allindagine ulteriore scansione tc effettuata contestualmente allindagine follow - up ecograco scintigraa ossea crovascular surgery referral centres , makes cta an excellent , readily available technique . 
however , achieving optimal results is dependent upon scrupulous technique , which consists of precise patient positioning on the ct bed ( supine with arms folded ) , dedicated acquisition and reconstruction protocols and accurate image interpretation . 
 in our study , patient positioning with arms folded and removal of all clothing at the thoracoabdominal level allowed acquisition of images unaffected by motion artefacts in all cases , with identication of the abdominal wall landmarks needed to harvest the cutaneous ap . 
the systematic removal of clothing for abdominal - wall cta has only recently been suggested [ 15 ] and was not mentioned in other studies [ 9 , 16 ]  . regarding image acquisition , although the technique for contrast - agent injection was similar to that used in conventional cta , the acquisition time needed to depict abdominal perforators is difcult to determine . 
in fact , images must be acquired during a later arterial phase compared with cta optimised for opacication of the main abdominal vessels , but just before venous return from the supercial and deep abdominal plexuses . 
these prerequisites limit the time window for optimal acquisition , and a delay of few seconds is often sufcient to obtain images spoiled by venous contamination . another parameter difcult to determine in advance is the time needed for opacication of peripheral abdominal vessels . 
if opacication time of the iliac vessels relative to the abdominal aorta can be estimated before the acquisition pi tardiva rispetto ad unangio - tc ottimizzata per lopacizzazione dei principali vasi addominali , ma comunque poco prima del ritorno venoso da parte dei plessi venosi addominali superciali e profondi . 
questi pre - requisiti limitano la nestra temporale per unacquisizione ottimale e spesso bastano pochi secondi di ritardo per ottenere delle fasi inciate da contaminazione venosa . un altro parametro di difcile determinazione prima dellacquisizione il tempo di opacizzazione dei vasi periferici addominali . 
se il tempo di opacizzazione dei vasi iliaci rispetto allaorta addominale pu essere valutato prima dellacquisizione mediante unoperazione di bolus tracking , il tempo di opacizzazione delle arterie epigastriche ed in particolare dei vasi perforanti non di facile determinazione . 
per tale motivo nella nostra esperienza abbiamo deciso di impostare sempre la roi del bolus tracking a livello dellaorta addominale e di regolare il ritardo dellacquisizione basandoci sui parametri clinico - anamnestici del paziente , in particolare sullet e sui fattori di rischio cardiovascolari riferiti in anamnesi che comprendono spesso informazioni riguardanti la funzione di pompa cardiaca ; una paziente anziana , con anamnesi di cardiopatia e con ridotta gittata cardiaca presenter un tempo di circolo pi lento , richiedendo un ritardo di scansione maggiore rispetto ad una paziente giovane con regolare funzione di pompa cardiaca o con tachicardia , spesso presente e legata alla componente emotiva insita nellesecuzione dellindagine , anche in relazione alla patologia di base . 
 radiol med ( 2013 ) 118 : 732743 by using the bolus tracking method , the opacication timing of epigastric arteries and , in particular , perforators , is not easy to calculate . 
for this reason , we always decided to place the bolus tracking roi over the abdominal aorta and calculate the scanning delay on the basis of the patients clinical data and history , in particular , her age and reported cardiovascular risk factors , which often include information on cardiac pump function . 
an elderly patient , with a history of heart disease and reduced cardiac output , will have a slower circulation time and require a longer delay compared with a young patient with normal cardiac pump function or tachycardia , which is often present due to the stress of the examination and the underlying disease . 
delayed acquisition occurred in eight cases in our study . in consideration of the above , although delayed arterial acquisition does not necessarily involve repeat examination , acquisitions obtained too early produce nondiagnostic images and the examination needs to be repeated , with increased radiation dose to the patient . 
the mean dose delivered is limited ( approximately 6 msv ) , lower than the dose delivered in many other conventional ct studies of the abdomen [ 18 ]  . 
 postprocessing using mip , 3d surface - rendering and 3d volume - rendering reconstructions allowed for excellent visualisation of the diea and siea and denition of their position , calibre and arrangement . 
in our study protocol for preoperative planning , the venous system was not included , even though recent studies suggest the possibility of considering assessment of the number and course of abdominal wall veins when studying perforator arteries [ 16 ]  . 
however , in our opinion , the study of the venous system should not focus on the venous perforator system , as perforating arteries are always accompanied by a homonymous vein draining at the level of the deep inferior epigastric veins . 
rather , we believe it should focus on the subcutaneous venous plexus , which seems to play an important part in the supercial venous drainage of the free ap transplanted in the breast area . conclusions abdominal wall cta is gaining ground as the standard of reference in preoperative localisation of abdominal perfosolitamente i vasi addominali superciali arteriosi risultano distinguibili da quelli venosi sulla base del diverso grado di opacizzazione dopo liniezione di mezzo di contrasto . 
in questi casi il riconoscimento della natura arteriosa del vaso si basa sul calibro e sul diverso decorso allinterno del pannicolo adiposo : ci rende il processo di riconoscimento pi lento e aumenta il tempo necessario alla ricostruzione su console , rendendola inoltre meno precisa . 
unacquisizione tardiva si vericata in 8 casi nel nostro studio . considerando quanto detto sopra , se unacquisizione arteriosa tardiva pu non richiedere necessariamente la ripetizione dellindagine , unacquisizione effettuata in una fase arteriosa troppo precoce si traduce in unindagine non diagnostica che impone la ripetizione della scansione aumentando di fatto la dose di esposizione della paziente . 
 il post - processing , con ricostruzioni mip , 3d surface rendering e 3d volume rendering , ha consentito di visualizzare in modo ottimale le diea e le siea e di denirne la posizione , il calibro e la disposizione . 
nel nostro protocollo di studio per la pianicazione pre - operatoria il sistema venoso non stato incluso , anche se recenti lavori hanno ipotizzato la possibilit di considerare nello studio della localizzazione dei vasi arteriosi perforanti anche una valutazione del numero e del decorso delle vene della parete addominale [ 16 ]  . 
a nostro avviso , tuttavia , lo studio del versante venoso andrebbe focalizzato non tanto sul sistema venoso perforante , in quanto solitamente le arterie perforanti sono sempre accompagnate in parallelo da unomonima vena che drena a livello delle vene epigastriche inferiori profonde , quanto piuttosto sul plesso venoso sottocutaneo , che sembra svolgere un ruolo importante nel successivo drenaggio venoso superciale del lembo libero trasposto in sede mammaria . conclusioni langio - tc della parete addominale si sta imponendo come esame di riferimento nello studio pre - operatorio di localizzazione dei vasi perforanti addominali . 
la precisa localizzazione di questi vasi consente al chirurgo di effettuare la dissezione della parete addominale con maggior sicurezza , riducendo di conseguenza i tempi di allestimento del lembo libero addominale [ 13 , 19 ]  . 
secondo la nostra esperienza lo studio ottimale dei vasi perforanti si ottiene mediante una conduzione tecnica rigorosa dellesame tc in termini di posizionamento della paziente , somministrazione del mezzo di 742 radiol med ( 2013 ) 118 : 732743 rators . 
the exact localisation of these vessels allows for a safer abdominal - wall dissection , with shorter operative time for harvesting the abdominal free ap [ 13 , 19 ]  . 
in our experience , optimal study of perforators is obtained by applying scrupulous cta technique in terms of patient position , contrast administration , volume acquisition timing and image reconstruction . 
reporting must be standardised and focus on information that may be useful to the surgeon in the operating roo timing of volume acquisition after contrast administration is crucial to achieving optimal perforator depiction . 
however , timing may vary widely , as it depends on each patients circulation ; this makes it difcult to obtain perfect synchronisation and acquisition of an optimally delayed arterial phase , even when using automatic bolus tracking . 
for this reason , in our experience , it is advisable to preset a second scan to be used only in the event that the images obtained from the rst scan were acquired too early . 
 in the future , increasingly delayed acquisitions may be needed due to the greater surgical interest in the anatomy of the supercial venous draining system [ 19 ]  . contrasto , tempistica di acquisizione del volume e ricostruzione delle immagini . 
 essa risulta tuttavia molto variabile in quanto dipende dalla dinamica circolatoria di ogni singolo paziente ; ci rende difcile una perfetta sincronizzazione e lottenimento di una fase arteriosa tardiva ottimale , anche utilizzando il sistema di bolus tracking automatico . 
per tale motivo secondo la nostra esperienza risulta auspicabile impostare preventivamente una seconda scansione pi tardiva , da utilizzare unicamente nel caso in cui le immagini ottenute dalla prima risultassero troppo precoci . 
rossi2 1scienze radiologiche , azienda ospedaliero - universitaria di parma , via gramsci 14 , padiglione barbieri , 43100 parma , italy 2dipartimento clinico di scienze radiologiche e istocitopatologiche , via massarenti 9 , bologna , italy correspondence to : m . 
although urological ( stricture , urinary stulas , vesico - ureteral reux ) and lymphatic complications ( lymphocoele ) have a high incidence , they only rarely lead to graft loss . 
by contrast , vascular complications ( stenosis , arterial and venous thrombosis , arterio - venous stulas , pseudoaneurysms ) are relatively rare , but potentially serious and may affect graft survival . 
the purpose of this pictorial review is to illustrate the increasingly signicant contribution of magnetic resonance angiography ( mra ) in the management of complications of kidney transplantation , and emphasise how this method should now be considered a mandatory step in the diagnostic workup of selected cases . 
moreover , the application and role in this setting of new magnetic resonance imaging ( mri ) techniques , such as diffusion - weighted and blood oxygen level - dependent ( bold ) mri , are also discussed . riassunto il trapianto di rene rappresenta attualmente la terapia delezione nella maggior parte dei pazienti con insufcienza renale cronica terminale per gli eccellenti risultati di sopravvivenza dellorgano e del paziente nonostante le complicanze chirurgiche siano tuttora abbastanza frequenti . 
le complicanze urologiche ( stenosi , stole urinose , reussi vescico - ureterali ) e linfatiche ( linfocele ) , pur avendo unincidenza signicativa , raramente determinano la perdita del graft , mentre le complicanze vascolari ( stenosi , trombosi arteriose e venose , stole artero - venose , pseudo - aneurismi ) , relativamente rare , sono potenzialmente gravi e possono compromettere la sopravvivenza dellorgano . 
lo scopo di questo pictorial review quello di illustrare il contributo sempre pi signicativo della risonanza magnetica angiograca ( mra ) nel management delle complicanze del trapianto renale , ritenendo ormai questa metodica step obbligato nelliter diagnostico di casi selezionati . 
verr anche discusso il ruolo delle nuove tecniche di risonanza magnetica ( mr ) , diffusione e blood oxygenation level dependent ( bold ) , in questo ambito . keywords magnetic resonance imaging renal transplant ultrasound parole chiave risonanza magnetica trapianto renale ecograa 838 introduction kidney transplantation is currently the treatment of choice for most patients with end - stage chronic renal failure owing to its excellent results in terms of patient and graft survival , and despite the fact that surgical complications are still relatively frequent [ 1 ]  . even though the incidence of urological ( stenosis , urinary stulas , vesico - ureteral reux ) and lymphatic complications ( lymphocoele ) is signicant , these complications rarely lead to graft loss ; by contrast , vascular complications ( stenosis , arterial and venous thrombosis , arteriovenous stulas , pseudoaneurysms ) are relatively rare , but are potentially serious and may affect graft survival [ 2 , 3 ]  . 
 ultrasound ( us ) and colour doppler us ( cdus ) are currently used as routine diagnostic techniques since they are readily available , repeatable , safe and inexpensive ; on the other hand , they are also closely dependent on operators skill and poorly specic , especially as concerns certain complications such as uid collections , acute rejection and neoplasms [ 46 ]  . 
 digital subtraction angiography with selective arterial catheterisation ( dsa ) is the diagnostic gold standard for the study of vascular complications , but it is an invasive procedure which uses potentially nephrotoxic iodinated contrast agents [ 4 , 5 ]  . 
alcune di queste complicanze possono presentarsi con un quadro clinico subdolo e aspecico ; si rende pertanto necessario il ricorso a esami strumentali per una precoce e precisa diagnosi e , quindi , un tempestivo trattamento . 
 lecograa e leco color - doppler ( ecd ) vengono attualmente utilizzate come tecniche diagnostiche di routine in quanto facilmente fruibili e ripetibili , sicure ed economiche , ma strettamente legate allesperienza delloperatore e poco speciche , soprattutto per alcune complicanze , quali raccolte , rigetti acuti e neoformazioni [ 46 ]  . langiograa digitale a sottrazione con cateterismo arterioso ( dsa ) rappresenta il gold standard diagnostico per lo studio delle complicanze vascolari , ma una procedura invasiva che utilizza mezzi di contrasto ( mdc ) organo - iodati , potenzialmente nefrotossici [ 4 , 5 ]  . la tomograa computerizzata multidetettore ( tcmd ) una tecnica non invasiva e accurata , ma richiede anchessa limpiego di mdc organo - iodato e lesposizione del paziente a radiazioni ionizzanti . 
the protocol used at our centre involves the acquisition of axial and coronal t2 - weigthed turbo spin - echo ( tse ) sequences with and without fat suppression , axial t1 - weighted se sequences , a bolus - timing sequence after i protocolli applicati nello studio mra nei pazienti sottoposti a trapianto renale variano a seconda dei sistemi hardware e software utilizzati . 
il nostro protocollo prevede sequenze turbo spin echo ( tse ) t2w senza e con la soppressione del grasso sul piano assiale e coronale , sequenze se t1 sul piano assiale , una sequenza di bolus - timing dopo sommiradiol med ( 2013 ) 118 : 837850 nistrazione di 0 , 2 ml / kg di mezzo di contrasto paramagnetico mediante iniettore automatico alla velocit di 2 ml / s e sequenze tridimensionali ad alta risoluzione spaziale ( 3d hi - res ) acquisite in breath - holding nella fase arteriosa , venosa e tardiva . complicanze vascolari stenosi arteria renale le stenosi nei pazienti trapiantati possono interessare sia le arterie iliache del ricevente sia larteria renale , sino alle diramazioni intraparenchimali del graft . le stenosi si localizzano pi frequentemente in sede anastomotica ( figg . , 2 , 3 )  . 
 lecd rappresenta attualmente lesame di prima istanza nel sospetto clinico di stenosi dellarteria renale , in particolare quando vi sia unipertensione arteriosa difcilmente controllabile con i farmaci e / o un peggioramento della funzionalit renale [ 14 , 15 ]  . qualora lecd avvalori tale sospetto clinico , consigliabile una successiva valutazione strumentale . 
in this context , mra represents a useful level - two diagnostic technique which provides , in a noninvasive manner , a panoramic view of the 840 radiol med ( 2013 ) 118 : 837850 fig . 
marked stenosis of the transplanted renal artery at the anastomosis ( arrow ) , digital subtraction angiography ( dsa ) ( b , c ) conrms the approximately 70% stenosis ( arrow )  . 
3a , b paziente maschio di 70 anni , mra addome , ricostruzione mip in coronale ( a ) con evidenza di stenosi del 50% circa dellarteria iliaca esterna di sinistra in sede pre - anastomotica ( freccia )  . 
 lecd , nel caso di fav , evidenzia una visualizzazione precoce della fase venosa mentre nello pseudoaneurisma mostra la presenza di ussi turbolenti [ 18 , 19 ]  . a differenza dellecd , la mra in grado di caratterizzare con precisione la lesione indicandone la sede anatomica ( renale o extrarenale ) , le dimensioni e i rapporti con le strutture contigue , permettendo un corretto planning preoperatorio . complicanze urologiche le complicanze urologiche rappresentano circa il 39% di tutte le complicanze [ 20 ]  . 
 ostruzione ureterale circa il 90% delle ostruzioni ureterali determinato da una stenosi o da unischemia ureterale che coinvolge nella quasi totalit dei casi il tratto ureterale distale , in prossimit della giunzione vescico - ureterale . 
il gold standard rappresentato dalla nefrostograa anterograda , una pratica invasiva che permette di individuare la natura e la sede esatta dellostruzione , garantendo nel contempo il ripristino immediato della funzionalit renale grazie allaccesso per eventuali drenaggi [ 22 ]  . nello studio sulle cause di unostruzione ureterale la mra , completata con la fase urograca , da considerarsi una valida alternativa sia alla uro - tc che alla nefrostograa anterograda perch priva rischi procedurali , nefrotossicit e radiazioni ionizzanti . 
stenosi emodinamicamente signicativa con aspetto liforme di unarteria interlobare superiore ( freccia ) linfocele renal artery thrombosis this a rare complication ( < 1% ) which tends to present in the immediate postoperative period as a consequence of surgical errors in graft harvesting or transplantation , severe hypotension in the immediately after surgery , arteriosclerosis involving the main renal artery and / or its branches . the rst - level imaging study is cdus , which demonstrates an absence of ow downstream from the thrombosis . 
 rispetto allesame ecograco , lmra permette una pi precisa localizzazione anatomica della lesione e dei suoi rapporti con le strutture contigue ; caratteristicamente , lintensit di segnale di tipo francamente uido , iperintenso nelle sequenze tse t2w e ipointenso nelle sequenze se radiol med ( 2013 ) 118 : 837850 fig . 
 ipointensit di segnale del polo inferiore del rene trapiantato in fossa iliaca sinistra senza signicativa retrazione della capsula per esiti di infarto cronico ( frecce )  . mra enables an accurate diagnosis of renal vein thrombosis ( t2 - weighted double inversion recovery haste sequences ) , as well as evaluation of the possible extension to the iliac vessels and exclusion of other possible causes of graft dysfunction [ 13 , 14 , 17 ]  . ascessi t1w , con impregnazione del mezzo di contrasto nelle fasi urograche tardive . arteriovenous stulas and pseudoaneurysms arteriovenous stulas ( avf ) are almost exclusively due to graft biopsy , whereas pseudoaneurysms generally form at the anastomoses as a result of technical errors or infection at the level of the surgical sutures . 
 in avf , cdus provides early visualisation of the venous phase , whereas in pseudoaneurysms it shows the presence of turbulent ows [ 18 , 19 ]  . unlike cdus , mra is able to precisely characterise the lesion indicating its anatomical location ( renal or extrarenal ) , size and relations with adjacent structures , thus allowing correct preoperative planning . urological complications urological complications account for approximately 3 - 9% of all complications [ 20 ]  . 
 us is the rst - level examination which , in the case of urinary obstructions , can reveal the presence and degree of hydronephrosis , generally associated with a high resisqualunque tipo di raccolta peri - trapianto pu evolvere in un ascesso , complicanza relativamente rara ma gravata da una elevata mortalit se non correttamente diagnosticata e tempestivamente trattata . lmra rappresenta in questi casi lesame di prima scelta , permettendo una diagnosi differenziale con gli altri tipi di raccolte ( linfoceli e urinomi ) in quanto mostra un tipico alone di edema inammatorio perilesionale francamente iperintenso nelle sequenze tse t2w con soppressione del grasso ( fat - sat )  . ematomi le caratteristiche del segnale dellematoma variano in relazione ai diversi stati di ossidazione dellemoglobina . 
pi frequenti nellimmediato postoperatorio ( fase acuta ) , gli ematomi presentano elevato segnale nelle sequenze pesate in t1 ( tabella 1 )  . allesame ecd possono presentarsi come raccolte semplici o settate , indistinguibili ecogracamente da altri tipi di raccolte . complicanze mediche necrosi tubulare acuta e rigetto acuto nel trapianto da donatore cadavere , la necrosi tubulare acuta rappresenta la causa pi frequente di una ritardata ripresa funzionale dellorgano . 
the gold standard is antegrade nephrostography , an invasive test that permits identication of the nature and precise site of the obstruction , while allowing immediate recovery of renal function by providing access routes for urinary drainage [ 22 ]  . in the study of the causes of a ureteral obstruction , mra , complete with a urographic phase , is to be considered a valuable alternative to both ct urography and antegrade nephrostography as it is free of procedural risks , nephrotoxicity and ionising radiation . 
in addition , mra is particularly sensitive in distinguishing transient hydronephrosis , a frequent occurrence in the immediate postoperative period , from a true obstruction [ 14 ]  . lymphocoele lymphocoele refers to a collection of lymph more frequently located between the bladder , the transplanted kidney and the iliac vessels . 
 del rene , un cambiamento dellecogenicit delle piramidi renali e della corticale e un incremento dellir . lmra evidenzia un normale enhancement della corticale , un marcato ritardo della perfusione midollare e una funzione di ltrazione glomerulare gravemente compromessa [ 8 ]  . 
nei pazienti con atn , dopo somministrazione di mdc si osserva un normale enhancement della corticale , seguito da un marcato ritardo nellescrezione renale , mentre nei pazienti affetti da rigetto acuto sono compromessi sia la perfusione corticale che il gfr [ 9 , 24 ]  . 
 il gold standard rimane comunque lesame bioptico che consente una diagnosi sicura e una quanticazione della gravit del rigetto , pur essendo una procedura non scevra da complicanze [ 25 , 26 ]  . rigetto cronico il rigetto cronico si manifesta tardivamente dopo il trapianto e rappresenta tuttora la causa pi comune di perdita dellorgano trapiantato . lesame ecd pu mostrare reperti di normalit o segni aspecici come un assottigliamento della corticale e incremento dellecogenicit parenchimale . lmra mostra una ritardata impregnazione ed escreradiol med ( 2013 ) 118 : 837850 abscesses any type of peri - graft uid collection may become an abscess , a relatively rare complication which carries a high mortality unless correctly diagnosed and promptly treated . mra is the investigation of choice in the differential diagnosis with other types of collection ( lymphocoele and urinoma ) , as it shows a typical halo of peri - lesional inammatory oedema which is frankly hyperintense in t2 - weighted tse sequences with fat suppression ( fat - sat )  . haematomas the signal characteristics of haematoma vary depending on the oxidation state of haemoglob more common in the immediate postoperative period ( acute phase ) , haematomas present with high signal intensity in t1 - weighted sequences ( table 1 )  . on cdus they may appear as simple or septated uid collections , sonographically indistinguishable from other types of collection . medical complications acute tubular necrosis and acute rejection in transplants from cadaver donors , acute tubular necrosis ( atn ) is the most frequent cause of delayed functional recovery of the gra cdus shows nonspecic ndings such as enlargement of the kidney , a change in echogenicity of the renal pyramids and cortex and increased resistive index ( ri )  . 
after contrast material administration , patients with atn show normal cortical enhancement followed by markedly delayed renal excretion , whereas in patients with acute rejection both cortical perfusion and gfr are compromised [ 9 , 24 ]  . 
9 paziente maschio di 62 anni , mr addome inferiore senza mdc , sezione coronale t2 - pesata : raccolta uida saccata ( linfocele ) , medialmente al rene trapiantato in fossa iliaca destra ( frecce )  . zione di mdc e un rapporto cortico - midollare alterato . 
gli esami di laboratorio e la clinica non sono sempre sufcienti a porre una diagnosi di certezza ; , pertanto , necessario un approccio diagnostico clinico - strumentale integrato [ 7 ]  . chronic rejection is a late complication of renal transplannello studio delle complicanze del trapianto di rene lin846 radiol med ( 2013 ) 118 : 837850 tation and still represents the most common cause of graft loss . cdus may show normal ndings or nonspecic signs , such as cortical thinning and increased parenchymal echogenicity . 
 , isointense ; + , hyperintense ; , hypointense stage days hyperacute acute subacute ( early ) subacute ( late ) chronic 12 27 7 to 1428 > 1428 t1w + + + + + + tabella 1 stadi evolutivi dei sanguinamenti , correlazione tra et dellematoma e intensit di segnale in mr nelle pesature t1 e t2 . 
 , isointenso ; + , iperintenso ; , ipointenso stadio giorni t1w iperacuto acuto subacuto ( precoce ) subacuto ( tardivo ) cronico 12 27 + + + 7 sino a 1428 + + + > 1428 + + + discussion the diagnostic approach to the complications of kidney transplantation is complex ; laboratory tests and clinical presentation may not be sufcient to establish a rm diagnosis , which therefore requires a combination of clinical and imaging assessments [ 7 ]  . in the study of kidney transplant complications , cdus is the level - one diagnostic investigation [ 2 , 6 , 10 ]  . 
the sensitivity of this technique may , however , be heavily limited by the patients habitus ( obesity ) , by the presence of bowel gas or by poor compliance . 
in vascular complications , cdus suffers some limitations such as difcult depiction of mild or moderate renal artery stenoses and a fair rate of false negative results ( sensitivity and specicity of 71% and 76% , respectively ) [ 1113 ]  . numerous authors agree that mra tends to overestimate arterial stenosis because of the ow void ; it is therefore unlikely that an arterial stenosis < 50% detected on mra will prove to be haemodynamically signicant on dsa [ 1517 ]  . 
 in addition , mra is very useful for revealing other aspects that may be associated with the arterial stenosis : poststenotic arterial dilatation , enhancement differences in the renal parenchyma up to parenchymal atrophy . as regards diagnostic suspicion of acute rejection , despite its role as the standard investigation , cdus is unable to differentiate rejection from the other parenchymal complications , and in particular from atn with which it may co - exist [ 23 ]  . dagine diagnostica di primo livello lecd [ 2 , 6 , 10 ]  . 
 lecd per le complicanze vascolari presenta alcuni limiti quali la difcile visualizzazione di stenosi lievi o moderate delle arteria renale e una discreta percentuale di falsi negativi ( sensibilit e specicit rispettivamente del 71 e del 76% ) [ 1113 ]  . numerosi autori concordano nel ritenere che la mra tenda a sovrastimare le stenosi arteriose per la presenza del ow void ; pertanto poco probabile che una stenosi arteriosa inferiore al 50% rilevata allmra possa essere emodinamicamente signicativa alla dsa [ 1517 ]  . 
lmra inoltre molto utile nellevidenziare altri aspetti che possono associarsi alla stenosi arteriosa ; la dilatazione arteriosa post - stenotica , i gradienti di impregnazione di mdc del parenchima renale no allatroa parenchimale . per ci che attiene al sospetto diagnostico di rigetto acuto dorgano , pur essendo lecd lindagine di riferimento , questultima non in grado di differenziarlo da altre complicanze parenchimali , in particolare rispetto alla atn con la quale , peraltro , pu coesistere [ 23 ]  . nel lavoro di kalb et al . 
nei pazienti con atn si osserva un normale enhancement contrastograco della corticale con un marcato ritardo nellescrezione renale , nei pazienti affetti da rigetto acuto sono comproradiol med ( 2013 ) 118 : 837850 fig . 
abdominal mra : coronal t2weighted se ( a ) and axial t1 - weighted high - resolution isotropic volume examination ( thrive ) with contrast medium ( b )  . 
mra addome in sezione coronale , se t2 - pesata ( a ) e sezione assiale t1 - pesata high resolution isotropic volume examination ( thrive ) con mdc ( b )  . 
formazione a margini netti ( a , frecce ) a struttura mista caratterizzata da una componente tissutale solida eccentrica e multipli sottili sepimenti che si impregnano di mdc ( b , frecce )  . 
in patients with atn there is normal cortical enhancement with heavily delayed renal excretion , whereas in patients with acute rejection cortical perfusion and gfr are both impaired [ 9 , 24 ]  . 
diffuse oedema is present in acute rejection but not in atn ; however , we believe that , although highly sensitive , this sign is nonspecic so that further studies are needed to understand the real clinical usefulness of mra in this setting [ 23 ]  . the use of mra is particularly useful in the study of peri - graft uid collections , which are seen in the immediate postoperative period in around 14% of cases [ 5 ]  . 
 the cdus appearance of a peri - graft uid collection is completely nonspecic , and the mra ndings may help to characterise it , particularly if the time of onset is also taken into account [ 11 ]  . 
 haematomas are more frequent in the immediate postoperative period and in this phase they are typically hyperintense on t1 - weighted images ; unlike all the other types of collection , abscesses show a rim of peri - lesional inammatory oedema , which is also appreciable on noncontrast - enhanced scans . new interesting applications of mra are diffusionweighted ( dw - mri ) and blood oxygenation level - dependent ( bold ) imaging [ 27 ]  . 
by using sequences that are particularly sensitive to proton movements such as single - shot echo - planar imaging ( ss - epi ) , diffusion imaging allows measurement of the diffusion of water molecules within tissue ; application of additional dephasing gradients capable of causing a drop in signal intensity proportional to the movement of water molecules through tissue allows for quantication of the apparent diffusion coefcient ( adc ) of water protons [ 27 ]  . bold imaging permits measurement of the degree of oxygenation of tissues by exploiting the paramagnetic properties of deoxyhaemoglobin [ 27 ]  . 
the presence of deoxyhaemoglobin in the capillaries produces microscopic magnetic eld inhomogeneties , which increase dephasing of the spins of the hydrogen protons and thus reduce signal intensity on t2 - weighted sequences [ 28 , 29 ]  . the conicting results reported in the literature with regard to dw - mri and bold imaging in the transplanted kidney currently do not justify their clinical use , considering that they prolong examination time without adding signicant information to the standard mra technique [ 29 ]  . despite its potential mra suffers limitations related to the examination technique and patient type ; an acquisition performed too early or too late during the dynamic phase may lead to false positive results in the assessment of the renal artery . 
with the recent introduction of the mr uoroscopy technique , timing of the contrast bolus can now be optimised so as to substantially minimise this problem ; messi sia la perfusione corticale che il gfr [ 9 , 24 ]  . 
edema diffuso presente nel rigetto acuto e non nella atn tuttavia , a nostro avviso , questultimo segno s molto sensibile ma altrettanto aspecico , e pertanto ulteriori studi sono necessari per comprendere la reale utilit clinica della mra in questo ambito [ 23 ]  . 
 limpiego della mra particolarmente utile nello studio delle raccolte peri - trapianto , presenti nellimmediato postoperatorio in circa il 14% dei casi [ 5 ]  . laspetto ecd delle raccolte uide peri - trapianto del tutto aspecico ; gli aspetti mra possono permettere un orientamento sulla caratterizzazione della raccolta stessa , tenendo conto anche del timing di insorgenza [ 11 ]  . 
gli ematomi sono pi frequenti nellimmediato post - intervento e in questa fase sono caratteristicamente iperintensi nelle sequenze pesate in t1 ; gli ascessi presentano , a differenza di tutte le altre raccolte , un alone di edema inammatorio perilesionale , evidenziabile anche senza lutilizzo del mdc . nuove interessanti applicazioni della mra sono rappresentate da tecniche di diffusione ( mr - dw ) e dalla tecnica blood oxygenation level dependent ( bold ) [ 27 ]  . 
la tecnica di diffusione consente , attraverso luso di sequenze particolarmente sensibili ai movimenti protonici come le echo - planar single - shot ( ss - epi ) , di misurare la diffusione delle molecole dacqua a livello tissutale ; lapplicazione di gradienti aggiuntivi di defasamento in grado di determinare una riduzione dellintensit di segnale proporzionale al movimento delle molecole dacqua nel tessuto permette di ottenere una quanticazione del coefciente di diffusione dei protoni dacqua ( adc ) [ 27 ]  . la tecnica bold permette di misurare il grado di ossigenazione dei tessuti , sfruttando le propriet paramagnetiche della desossiemoglobina [ 27 ]  . 
la presenza di desossiemoglobina nei capillari produce microscopiche disomogeneit magnetiche , che aumentano lo sfasamento degli spin dei protoni degli atomi di idrogeno e quindi riducono lintensit di segnale nelle sequenze t2 - pesate [ 28 , 29 ]  . la non univocit dei risultati riportati nella letteratura riguardo le tecniche mr di diffusione e bold nel rene trapiantato , attualmente non giusticano la loro applicazione clinica , considerando che i tempi desecuzione dellesame sono allungati senza aggiungere signicative informazione alla tecnica mra standard [ 29 ]  . lmra , nonostante le grandi potenzialit , presenta alcuni limiti legati alla tecnica desame e alla tipologia di paziente ; unacquisizione troppo precoce o troppo tardiva durante la fase dinamica pu essere causa di falsi positivi nella valutazione dellarteria renale . 
con la recente introduzione della tecnica uoro - rm , oggi possibile ottimizzare il timing del bolo del mdc , cos da ridurre sensibilmente tale problematica ; inoltre , le sequenze a singolo breath - hold con apnee di massimo 2530 s , possono ridurradiol med ( 2013 ) 118 : 837850 moreover , single breath - hold sequences with maximum breath - hold time of 2530s can reduce the incidence of artefacts caused by respiratory movements [ 30 ]  . 
a further limitation of mra is the difculty depicting thin polar arteries because of poor spatial resolution [ 17 ]  . on the basis of recent literature reports , brief mention should be made of the correlation between the development of nephrogenic systemic brosis ( nsf ) and exposure to some paramagentic contrast media used in mra [ 31 ]  . 
 although there is no absolute certainty as to the cause - andeffect relationship between nsf and gadolinium - based contrast agents , the italian society of medical radiology recommends caution in patients with kidney transplant and renal failure stages 3 - 4 and 5 ( gfr 3059 ml / min and creatinine > 4.0 mg / dl ) and the use of prophylactic hydration and a low dose of contrast medium ( 0.4 mmol / kg ) so as to reduce the risk of nephrotoxicity [ 31 , 24 ]  . re lincidenza degli artefatti legati alla respirazione [ 30 ]  . 
 linadeguata apnea , la claustrofobia sofferta da alcuni pazienti , la presenza di pacemaker , di clip o di stent rappresentano limiti legati al paziente [ 17 , 13 ]  . 
in base alle recenti segnalazioni in letteratura , un breve accenno merita la correlazione tra lo sviluppo di brosi sistemica nefrogenica ( nsf ) e lesposizione ad alcuni mezzi di contrasto paramagnetici utilizzati nella mra [ 31 ]  . 
nonostante non sia stato dimostrato con assoluta certezza il nesso di causalit tra fsn e agenti di contrasto a base di gadolinio , la societ italiana di radiologia medica raccomanda cautela nei pazienti con trapianto renale e con insufcienza renale in stadio 3 , 4 e 5 ( gfr 3059 ml / min e creatinina > 4 , 0 mg / dl ) e lutilizzo di misure prolattiche di idratazione e bassa dose di mdc ( 0 , 4 mmol / kg ) al ne di ridurre il rischio di nefrotossicit [ 31 , 24 ]  . conclusions conclusioni in conclusion , the diagnostic approach to conditions affecting the transplanted kidney is complex and requires the combination of several imaging modalities . 
 mra is a noninvasive , accurate and repeatable leveltwo investigation which provides useful anatomical and functional information about the transplanted kidney and is especially indicated after inconclusive or positive cdus ndings . 
 mra limits the use of dsa to the study of vascular complications thanks to its good diagnostic accuracy ; it is a valuable diagnostic aid in urological complications and in the study of peri - graft uid collections . 
in selected cases , mra limits the use of biopsy which , although the gold standard in the diagnosis of rejection , atn and neoplasms , is not free of possible complications ( arteriovenous stula , pseudoaneurysms and haemorrhage )  . lmra una tecnica diagnostica di secondo livello non invasiva , accurata e ripetibile che fornisce utili informazioni anatomiche e funzionali del rene trapiantato , indicata soprattutto nei casi dubbi o positivi allecd . 
risultati incoraggianti sono stati ottenuti nella diagnostica differenziale del rigetto acuto e dellatn . lmra limita il ricorso alla dsa per lo studio delle complicanze vascolari per la sua buona accuratezza diagnostica ; un valido supporto diagnostico nelle complicanze urologiche e nello studio delle raccolte peritrapianto . 
sixty - seven were placed through the jugular vein , 61 through the brachial vein and 63 through the femoral vein 109 patients , the vcf was placed for absolute indications , in 77 for relative indications , and in 15 for temporary ltration . 
vcf was removed 6 months after deployment in 11 patients , 12 months in eight , 24 months in four after 36 months in three ( range , 1801 , 155 days . ) there were no periprocedural complications . 
in 109 / 201 pazienti il fc stato posizionato con indicazioni assolute , in 77 / 201 pazienti il fc stato posizionato con indicazioni relative e in 15 / 201 pazienti il fc stato posizionato per ltrazione temporanea . 
le indicazioni alla rimozione del fc sono state : non pi evidenza di controindicazioni alla terapia anticoagulante in assenza di nuovi episodi di embolia polmonare e perviet dellasse venoso iliaco - cavale . 
of the 186 vcf placed for permanent use , with absolute and relative indications , 14 were removed ( 4 / 109 and 10 / 77 , respectively )  . 
technical failure of the removal procedure is directly proportional to the vcf tilt , and the vcf is as yet unable to ensure absolute removal safety , with the result that failure may occasionally occur . 
the morphological and structural features of permanent / retrievable vcf allow for unlimited time from placement to removal , documented to be up to 3 years after placement . keywords vena cava lter pulmonary embolism removable vena cava lter periprocedurali . 
 sono stati rimossi 12 dei 15 fc posizionati con indicazione temporanea ; nei restanti 3 pazienti , nefrectomizzati per neoplasia renale , non si proceduto alla rimozione del fc per persistenza del trombo neoplastico . 
le caratteristiche morfologiche e strutturali del fc denitivo tipo removibile ne consentono comunque la rimozione illimitata nel tempo , almeno documentata a 3 anni . parole chiave filtro cavale embolia polmonare filtro cavale removibile introduction introduzione the use of vena cava lters ( vcf ) to prevent pulmonary embolism ( pe ) in patients with deep vein thrombosis ( dvt ) is recognised as a reliable approach when anticoagulation therapy is contraindicated or ineffective , even though their placement is still problematic in young patients or cases requiring temporary ltration , as in multiple trauma , pregnancy or prior to procedures involving vena cava ( vc ) manipulation [ 13 ]  . 
it is therefore necessary to dene when a vcf placed for permanent indications may be removed , even several years later , and to establish whether a permanent / retrievable vcf may also be used for temporary ltration [ 610 ]  . the purpose of our work was to evaluate the safety of removing shortand long - term permanent / retrievable vcf ( aln implants chirurgicaux , ghisonaccia , france )  . limpiego dei ltri cavali ( fc ) per la prevenzione della embolia polmonare ( ep ) nei pazienti affetti da trombosi venosa profonda riconosciuto valido quando la terapia anticoagulante sia controindicata o inefcace , ma risulta ancor oggi problematico quando il posizionamento del fc riguardi pazienti in giovane et o situazioni di temporanea ltrazione , quali possono realizzarsi nel politrauma , nella gravidanza o in previsione di particolari interventi che comportino la manipolazione della vena cava ( vc ) [ 13 ]  . 
the approach was transjugudal 2002 al 2010 , nel nostro centro , sono stati posizionati 201 fc di tipo denitivo / removibile aln in 201 pazienti ( et media 53 anni ; range 1880 anni ) ; sessantasette sono 818 radiol med ( 2013 ) 118 : 816825 fig . 
1a cavography performed at the end of the procedure shows the extremity of the vena cava lter ( vcf ) at the renal vein conuence , projected against the lower end plate of the t12 vertebra . 
b follow - up at 36 months with abdominal x - ray during breath - holding demonstrates the cranial end of the vcf projected against the body of t12 with a slight cranial shic contrast - enhanced computed tomography ( ct ) during the portalvenous phase before vcf removal shows penetration of the hooks and their escape from the posterior wall of the vena cava ( arrows )  . 
b il follow - up a 36 mesi espletato con rx delladdome in apnea respiratoria , dimostra lestremo craniale del fc che si proietta al corpo d12 con lieve slittamento craniale . 
c la tc con mdc effettuata in fase veno - portale , prima della rimozione del fc dimostra la penetrazione degli uncini e la loro fuoriuscita dalla parete posteriore della vena cava ( frecce )  . 
in 109 patients with proven pe , the vcf was placed for absolute indication for permanent use ; in 43 for contraindications to anticoagulation therapy , in 29for haemorrhagic complications during anticoagulation therapy and in 37 for failure of anticoagulation treatment . 
in 109 / 201 pazienti con ep documentata il fc stato posizionato con indicazioni assolute di tipo denitivo ; in 43 / 109 per controindicazioni alla terapia anticoagulante , in 29 / 109 per complicanze emorragiche in corso di terapia anticoagulante e in 37 / 109 per insuccesso della terapia anticoagulante . 
in 77 / 201 pazienti , in assenza di ep , il fc stato posizionato con indicazioni relative con intento denitivo per trombo ottante iliaco aggettante in cava e / o in vena renale . 
2a cavography performed at the end of the procedure shows correct vena cava lter ( vcf ) placement in the infrarenal position , with its axis parallel to the longitudinal axis of the vc . 
lapice del fc viene svincolato dalla vena renale mediante lutilizzo di un pallone dilatatore ( frecce ) gonato tra le maglie del fc e sospinto verso lalto ( c ) ; successivamente , il fc viene agganciato ( teste di frecce ) e rimosso ( d ) senza complicanze procedurali . rary ltration and thus for short - term use : these comprised seven cases of multiple trauma and eight requiring prophylaxis before caval manipulation . 
then , using a curved hydrophilic guidewire ( 0.035glidewire , terumo , tokyo , japan ) , a 5 - f vascular introducer sheath was positioned ( cordis , miami , fl , usa )  . 
cavography was then performed with a straight or pigtail diagnostic catheter ( cordis ) to idenporanea , quindi con intenzione di rimuovere il fc : in 7 per politrauma e in 8 per prolassi preoperatoria in manipolazione cavale . 
in tutti i casi stato utilizzato lapproccio percutaneo con tecnica di seldinger mediante ago cannula da 19 g e , successivamente , con guida idrolica curva ( 0 , 035 , glidewire , terumo , tokyo , giappone ) , stato posizionato un introduttore vascolare da 5 f ( cordis , miami , usa ) ; successivamente , mediante catetere diagnostico retto o pigtail ( cordis , miami , usa ) stata effettuata una cavograa per individuare la conuenza delle vene renali , le eventuali ano820 radiol med ( 2013 ) 118 : 816825 fig . 
mediante doppio approccio ( femoralegiugulare ) un catetere pigtail , avanzato per via transfemorale , viene posizionato tra gli steli del fc ; con movimenti di torsione del catetere si orienta il fc lungo lasse della vci ( c )  . 
successivamente , il fc viene agganciato dallalto dal sistema estrattore avanzato per via giugulare e rimosso ( d )  . tify the conuence of the renal veins , possible caval abnormalities and diameter of the vc . 
access from above was preferred ( brachial and / or jugular ) , as it ensures less vcf tilting with respect to vc longitudinal axis . in 179 patients , the vcf was placed infrarenally and suprarenally in the remaining 22 . 
si preferito laccesso dallalto ( brachiale e / o giugulare ) in quanto riduce il tilting del fc , cio langolazione dellasse del fc rispetto allasse longitudinale della vena cava . in 179 / 201 pazienti il fc stato posizionato in sede sottorenale , nei rimanenti 22 / 201 in sede sovrarenale . 
in 19 of these 26 patients , removal was performed exclusively via the right transjugular approach using a straight 7 - f extraction system equipped with a pincer that grasps the vcf and draws it back into the device . 
in seven patients , a double right jugular and femoral approach with four - handed technique was required to alter , from below , orientation of the vcf cranial end by afxing a pigtail catheter stiffened by an inner guidewire between the vcf struts . 
i 26 / 201 pazienti candidati alla rimozione sono stati indagati mediante angio - tc , per escludere la presenza di ep e documentare la perviet dellasse venoso iliaco - cavale ed eventuali complicanze . 
in 19 / 26 la rimozione stata effettuata esclusivamente per via trans - giugulare destra , mediante sistema estrattore da 7 f a morfologia retta provvisto di pinza al suo estremo distale che aggancia e ringuaina il fc allinterno del dispositivo . 
in 7 / 26 stato necessario un doppio approccio giugulare e femorale destro , con tecnica a quattro mani per modicare , dal basso , lorientamento dellestremo craniale del fc mediante linssione tra gli steli del fc di un catetere pigtail irrigidito con un guida al suo interno . 
 in two transfemoral approaches ( 0.99% ) , the vcf was excessively tilted ( > 15 ) with respect to the longitudinal vc axis ; in both cases , the vcf was not retrieved immediately , as ltration was considered adequate at follow - up cavography . 
a few caudal , gravity - related migrations by half a vertebral body , of no practical consequence , were detected that may have been caused by the lack of downward - directed hooks . 
twenty - six of 201 il rilascio con normo - posizionamento del fc si realizzato con successo tecnico ( tilting non superiore ai 15 gradi ) nel 99 , 01% dei casi . 
in due casi ( 0 , 99% ) , per via femorale , si realizzata uneccessiva inclinazione ( superiore ai 15 gradi ) del fc rispetto allasse longitudinale della vc ; in entrambi i casi non si proceduto alla rimozione immediata del fc in quanto si ritenuta sufciente la ltrazione al controllo dopo cavograa . 
sono state documentate alcune cadute caudali , sino a mezzo corpo vertebrale , favorite dalla gravit , ma senza pratica importanza , forse dovute alla mancanza di uncini rivolti verso il basso . 
sono stati rimossi 26 / 201 fc con un successo tecnico 822 radiol med ( 2013 ) 118 : 816825 vcf were removed , with a 99% technical success rate . 
retrieval was performed through a transjugular approach at 6 months from placement in 11 patients , 12 months in eight , 24 months in four and 36 months in three , with a maximum indwelling time of 1 , 155 days . 
twenty - one of 26 removed vcf were infrarenal and , ve were suprarenal . twelve of the 15 vcf deployed for temporary use were removed : in three patients who had undergone nephrectomy for renal cancer , vcf was removed due to persistent neoplastic caval thrombus . fourteen ( 14 / 186 ) vcf deployed with absolute and relative indications for permanent use were removed ( 4 / 109 and 10 / 77 , respectively )  . 
of these , only one vcf was occluded by thrombi . discussion data on the incidence of pe are controversial , as it is a rarely diagnosed emergency that carries a high risk of death . 
 autopsy studies indicate pe as the cause of death in 214% of cases , with peaks of 60% in elderly and at - risk patients ( cardiac , chronic obstructive pulmonary disease , trauma patients )  . 
 because of the close relationship between pe and dvt , the term thromboembolic venous disease has been coined to refer to the predominant aetiopathogenesis of the disease [ 12 ]  . 
congenital factors include antithrombin iii deciency , hyperhomocysteinaemia , protein c and protein s deciency , prothrombin mutation , activated protein c resistance ( apc - r ) and consequences of factor v leiden mutation . 
in a minority of cases , there may be complete haemodynamic and anatomical resolution , whereas in most cases , resolution is partial and associated with a normal clinical condition . 
in a minority of cases , recurrent or silent pe leads to pulmonary hypertension ; untreated pe leads to death within 3 years from diagnosis . the purpose of treating pe is to reduce mortality and prevent recurrences and late complications , namely , postphlebothrombotic syndrome and chronic pulmonary hypertension . 
la rimozione stata effettuata per via trans - giugulare : a 6 mesi dal posizionamento in 11 pazienti , a 12 mesi in 8 , a 24 mesi in 4 e a 36 mesi in 3 casi , con tempo massimo di permanenza di 1155 giorni . 
ventuno ( 21 / 26 ) fc rimossi erano stati posizionati in sede sottorenale e 5 / 26 in sede sovrarenale . sono stati rimossi 12 dei 15 fc posizionati con indicazione temporanea ; in 3 pazienti , nefrectomizzati per neoplasia renale , per persistenza del trombo neoplastico cavale . quattordici ( 14 / 186 ) fc posizionati con indicazioni assolute e relative con intento denitivo sono stati rimossi , rispettivamente 4 / 109 e 10 / 77 ; di questi un solo fc presentava trombi inclusi . discussione i dati sulla incidenza dellep sono controversi , in quanto questa patologia rappresenta unemergenza poco diagnosticata e a rischio di morte elevato . 
studi autoptici indicano lep come causa di morte variabile tra il 2 e il 14% ; in gruppi di pazienti anziani e a rischio ( cardiopatici , bpco , traumatizzati ) , la percentuale pu giungere al 60% . 
lep e la trombosi venosa profonda ( tvp ) sono strettamente correlate ; di qui il termine unicante di malattia tromboembolica venosa che si riferisce al momento eziopatogenetico prevalente della malattia [ 12 ]  . 
tra i primi , i pi comuni : decit di antitrombina iii , iperomocisteinemia , decit di proteina c o proteina s , mutazione della protrombina , resistenza alla proteina c attivata ( apc - r ) , conseguenza della mutazione del fattore v di leiden . 
pu evolvere , in una minoranza di casi , nella completa risoluzione emodinamica e anatomica ; nella maggior parte si assiste alla parziale risoluzione associata a uno stato clinico normale . 
in una minoranza , lep recidivante o silente procede verso lipertensione polmonare ; lep , se non trattata , porta al decesso nei tre anni successivi alla diagnosi . gli obiettivi della terapia della tromboembolia polmonare sono la riduzione della mortalit , la prevenzione delle recidive e delle complicanze tardive rappresentate innanzitutto dalla sindrome post - ebotrombotica e dallipertensione polmonare cronica . 
 selecting the vcf to be used is more complex when pe prevention is expected to be short term : when anticoagulation therapy must be suspended because of surgery in patients with proximal dvt that developed < 1 month previously , as a preventive measure in high - risk patients before major orthopaedic surgery , in elderly patients with a positive history of thromboembolic disease , in patients with limited cardiopulmonary reserve and / or pulmonary hypertension and in rare cases of protected thrombolysis . temporary vcf have less denite and less well - accepted indications . 
currently available devices are reluctantly used on account of complications due to thrombogenicity , infections , often inadequate indwelling time , difcult and costly management and frequent migration and kinking . 
in addition to the properties of permanent vcf ( biocompatibility , absence of thrombogenicity , resistance to degradation , maintenance of a constant caval ow , stability in relation to the caval wall ) these devices also offer the advantage of possible removal . 
in the rst published studies , several authors expressed concern because of the frequent retrieval failures due to the straight shape of the extracting device and the almost constantly tilted position of the vcf , which made grasping difcult [ 1517 ]  . 
improved knowledge of the device and the experience gained by operators have signicantly reduced retrieval failures : vcf tilting with respect to the longitudinal axis of the vc may be prevented by positioning the vcf through the transjugular or brachial approach . 
 [ 16 ] reported four cases of failure among 55 retrievals out of 220 vcf placed ( 121 placed for pe ) , with an average indwelling time of 51 ( range , 6352 ) days . 
 [ 17 ] reported four cases of failure among 18 retrievals out of 30 vcf placements , with a mean indwelling time of 123 ( range , 30345 ) days . 
the frequency of retrieval and short vcf indwelling time ( 36 months ) in these studies are probably linked to the relative indication for positioning ( no cases of pe )  . 
conversely , in most series , vcf are placed for absolute indications related te : la controindicazione , linsuccesso o le complicanze della terapia anticoagulante in pazienti con documentata tvp prossimale e ep . 
 pi problematica la scelta del fc da utilizzare quando la protezione embolica si prevede limitata nel tempo : quando sia necessario sospendere la terapia anticoagulante in previsione di un intervento chirurgico in paziente con tvp prossimale comparsa da meno di 1 mese , nella prolassi dei pazienti ad alto rischio prima di intervento ortopedico maggiore , in soggetti anziani con anamnesi positiva per malattia tromboembolica , in pazienti con minima riserva cardiopolmonare e / o ipertensione polmonare o nei rari casi di trombolisi protetta . il fc temporaneo ha indicazioni attualmente meno certe e condivise . 
i dispositivi in commercio vengono utilizzati malvolentieri per le complicanze legate alla trombogenicit , alle infezioni , al tempo di permanenza spesso insufciente , per la loro gestione difcile e costosa e a causa della frequenza delle migrazioni - inginocchiamenti dei fc . 
per questi motivi stato proposto , quale alternativa al fc temporaneo , lutilizzo del fc denitivo di tipo removibile [ 14 ] che somma alle qualit del fc denitivo ( biocompatibilit , assenza di trombogenicit , resistenza alla degradazione , mantenimento di un regolare usso cavale , stabilit rispetto alla parete cavale ) la possibilit di essere rimosso . 
nelle prime esperienze pubblicate , pi autori esprimevano perplessit derivate dai frequenti fallimenti nella rimozione , dovuti alla morfologia retta del dispositivo estrattore e alla posizione quasi sempre inclinata del fc che ne rendeva problematico laggancio [ 1517 ]  . 
 [ 16 ] , in 55 rimozioni su 220 fc ( 121 posizionati con ep ) riportano 4 insuccessi con un tempo medio di permanenza di 51 giorni ( range 6352 giorni ) ; imberti e colleghi [ 17 ] , su 30 impianti con 18 tentativi di rimozione riportano 4 insuccessi con un tempo di permanenza medio di 123 giorni ( range 30345 giorni )  . 
la frequenza di rimozione e il tempo breve di permanenza ( 36 mesi ) del fc in questi lavori sono probabilmente legati alla indicazione relativa al posizionamento ( assenza di ep )  . 
nella maggioranza delle casistiche i fc vengono invece posizionati con indicazioni assolute ove giocano un ruolo importante fattori congeniti e acquisiti che solo in minima percentuale regrediscono , consentendone la rimozione . 
in fact , the double approach proved to be decisive in all cases of disproportionate tilting , as described in a case of atrial migration with upside - down lter rotation [ 22 ]  . 
our experience conrms the safety of vcf retrieval up to 1 , 155 days after implantation and conrms that the nitinol structure of the vcf , thanks to its shape memory , allows for unlimited retrieval , with failures being related only to vcf tilting and not to endothelialisation . dio multicentrico francese [ 22 ] ha documentato lestrazione di 123 fc con un solo caso di insuccesso e tempo di permanenza massimo di 722 giorni . 
 infatti , il doppio approccio si rilevato determinante in tutti i casi di estremo tilting , come descritto in un caso di dislocazione in atrio con ltro ruotato di 180 [ 22 ]  . 
la nostra esperienza ha documentato la sicurezza dellestrazione del fc con permanenza massima di 1.155 giorni ; la struttura in nitinol del fc , pertanto , in relazione alla sua memoria di forma , permette una rimozione illimitata e linsuccesso legato solo ed esclusivamente al tilt del fc e non a processi di endotelizzazione . conclusions retrieving permanent vcf proved to be more difcult than placement . 
filter placement from above ( via the jugular and brachial approaches ) prevents disproportionate vcf tilt , as the hooks are extracted rst and the lter is thus coaxially stabilised with respect to the vc . 
therefore , the use of permanent / retrievable vcf can be more safely suggested in all young patients with absolute indications for vcf placement and in all clinical situations requiring temporary ltration . conclusioni la rimozione del fc denitivo si rilevata sicuramente pi difcile del posizionamento . 
linsuccesso della procedura di rimozione direttamente proporzionale al tilt del fc . il posizionamento dallalto ( giugulare e brachiale ) previene leccessivo tilting del fc poich gli uncini sono i primi a uscire stabilizzando il ltro coassialmente rispetto alla vc . 
il fc denitivo di tipo removibile , tuttavia , ancora non possiede gli estremi di sicurezza assoluta alla rimozione e , anche se in rari casi , ne contemplato linsuccesso . 
the parameters analysed were : technical success , preand posttreatment serum creatinine ( scr ) and blood pressure ( bp ) , average number of antihypertensive drugs administered before and after treatment and vessel patency on colour doppler ultrasound ( cdus ) at 1 , 3 , 6 and 12 months and once a year thereafter . 
consistent with the literature data , our experience shows that endovascular treatment with pta / stenting is a safe and effective option for managing tras and can thus be considered the method of choice . keywords transplanted renal artery stenosis endovascular treatment pta / stenting riassunto obiettivo . 
da gennaio 2005 a dicembre 2010 , 17 pazienti ( 4 femmine e 13 maschi ; et media 60 , 9 anni ) affetti da tras sono stati sottoposti a pta / stenting . 
il successo tecnico stato del 100% ; ad un followup medio di 28 , 318 , 7 mesi , si osservata una riduzione statisticamente signicativa dei valori di creatinina sierica e di pressione arteriosa . 
allecd nel 18% dei casi si riscontrata re - stenosi di grado moderato ( < 60% ) , non associata ad alterazioni della funzionalit dorgano e non meritevole di nuovo trattamento . 
nella nostra esperienza , in linea con i dati della letteratura , il trattamento endovascolare mediante pta / stenting rappresenta una opzione sicura ed efcace nella gestione delle tras , costituendo la prima scelta terapeutica . parole chiave stenosi arteria renale trapiantata trattamento endovascolare pta / stenting radiol med ( 2013 ) 118 : 826836 introduction introduzione renal transplantation is the treatment of choice in patients with chronic end - stage kidney failure , as it improves the recipients quality of life and ensures long - term survival [ 1 ]  . 
the effectiveness of renal transplantation depends on the long - term function of the graalthough the development of increasingly effective immunosuppressive therapies has reduced the incidence of acute and chronic organ rejection , 1220% of transplanted patients developed either vascular or extravascular complications that may undermine long - term effectiveness [ 2 ]  . 
the majority of these complications are transplanted renal artery stenosis ( tras ) , arteriovenous stulas , intraor extrarenal pseudoaneurysms and thrombosis of the renal artery and / or vesince tras was rst described in 1966 , it has increasingly been reported as the main cause of refractory hypertension and kidney transplant failures [ 4 ]  . 
the incidence of tras ranges from 1% to 23% [ 5 ] , depending on the diagnostic criteria adopted in each centre and the routine use of colour doppler us ( cdus )  . 
the rapid development of endovascular techniques in the past 10 years has also involved this clinical area , and endovascular surgery has become the treatment of choice for atherosclerotic renovascular conditions , including tras , as it ensures high technical success rates using a minimally invasive approach and provides adequate long - term patency and a lower complication rate compared with open surgery [ 8 ]  . the purpose of this retrospective analysis of our experience was to evaluate the effectiveness of endovascular treatment of tras with percutaneous transluminal balloon angioplasty ( pta ) and stenting using latest - generation materials and then compare it with data reported in the literature . materials and methods between january 2005 and december 2010 , 17 patients with tras ( 13 men , 4 women ) underwent endovascular treatment . 
the diagnosis of tras was based on : ( 1 ) new onset of arterial hypertension > 140 / 90 mmhg unresponsive to medical therapy with two or more antihypertensive agents ; ( 2 ) 20% increase of post - transplantation creatinine ( cr ) levels ; ( 3 ) cdus abnormalities consisting of peak systolic velocity ( psv ) > 200 cm / s or > 50% compared with the il trapianto renale il trattamento di scelta in pazienti con insufcienza renale cronica terminale , migliorando la qualit della vita ed assicurando sopravvivenza a lungo termine nei riceventi [ 1 ]  . 
lefcacia del trapianto renale dipende dalla funzionalit a lungo termine del graft : lo sviluppo di sempre pi efcaci terapie immunosoppressive ha ridotto lincidenza di rigetto acuto e cronico dorgano , tuttavia in circa il 12%20% dei pazienti trapiantati insorgono complicanze , vascolari o extra - vascolari , che possono inciarne lefcacia a lungo termine [ 2 ]  . 
le complicanze pi frequenti sono quelle vascolari , che hanno incidenza del 3%15% in pazienti trapiantati [ 2 ] e possono causare perdita della funzionalit dorgano [ 3 ] ; esse sono rappresentate principalmente da stenosi dellarteria renale trapiantata ( tras ) , stola artero - venosa , pseudoaneurisma intrarenale o extrarenale e trombosi dellarteria e / o vena renale . 
dalla prima descrizione nel 1966 , la tras stata sempre pi frequentemente riportata come la principale causa di ipertensione refrattaria alla terapia medica e di insuccesso del trapianto renale [ 4 ] : fondamentale pertanto la diagnosi precoce seguita da trattamento adeguato della patologia per assicurare la sopravvivenza del graft e del paziente stesso . 
 lincidenza di tras oscilla tra l1% ed il 23% [ 5 ] a seconda dei criteri diagnostici impiegati in ogni istituto e luso routinario delleco - color doppler ( ecd ) ; lintroduzione nella pratica clinica della risonanza magnetica ( rm ) [ 6 ] ne ha consentito una diagnosi sempre maggiore e precoce . 
nel passato il trattamento standard di tale complicanza era rappresentato dallintervento chirurgico , con una efcacia dello stesso del 63%92% [ 7 ] ; nellultimo decennio il rapido sviluppo delle tecniche endovascolari si affermato anche in questo ambito , diventando il trattamento di scelta nella patologia aterosclerotica renovascolare e quindi anche della tras , in quanto assicura , in modo mini - invasivo , alto successo tecnico con adeguata perviet a distanza a fronte di una riduzione delle complicanze rispetto allintervento chirurgico standard [ 8 ]  . 
 obiettivo del nostro studio valutare lefcacia del trattamento endovascolare mediante angioplastica percutanea transluminale ( pta ) e stenting delle tras con impiego di materiali di ultima generazione , effettuando unanalisi retrospettiva della nostra esperienza e confrontandola con i dati della letteratura . materiali e metodi da gennaio 2005 a dicembre 2010 , 17 pazienti affetti da tras ( 13 maschi , 4 femmine ) sono stati sottoposti a trattamento endovascolare . 
lesame angiograco documenta la presenza di stenosi di grado severo in corterzo medio rispondenza del dellarteria renale trapiantata ( a ) , trattata mediante posizionamento di stent balloon - expandable con ripristino di buon calibro vasale ( b )  . downstream ow ; presence of jet aliasing and a resistive index ( ri ) > 0.8 [ ri = ( sv / dv ) / sv , where sv = maximum systolic velocity and dv = minimum diastolic velocity ]  . our case series comprised 4 women ( 23.5% ) and 13 men ( 76.5% ) with a mean age of 60.9 ( range , 3274 ) years ( table 1 )  . 
all patients received kidneys from cadaveric donors ( 100% ) , transplanted in nine cases in the left iliac fossa ( 53% ) and in eight cases in the right iliac fossa ( 47% ) , with end - to - side anastomoses in the external iliac artery ( 100% )  . 
low - osmolar , water - soluble nephrotropic iodinated contrast material ( visipaque 270 mg / ml , ge healthcare as , oslo , norway ) was used after dilution to 50 % with saline solution to prevent contrast - induced nephrotoxic damage . 
bolus of sodium heparin ( 50 ui / kg ) was administered . osa > 140 / 90 mmhg refrattaria alla terapia medica con due o pi farmaci anti - ipertensivi ; ( 2 ) incremento del 20% dei valori di creatinina post - trapianto ; ( 3 ) alterazioni allecd rappresentate da velocit di picco sistolico ( vps ) > 200 cm / s o > 50% rispetto al vaso a valle , presenza di fenomeno di jet aliasing ed indice di resistenza ( ir ) > 0 , 8 [ ir = ( vs / vd ) / vs dove vs = massima velocit sistolica e vd = minima velocit diastolica ]  . la nostra casistica ha compreso 4 femmine ( 23 , 5% ) e 13 maschi ( 76 , 5% ) con et media di 60 , 9 anni ( range : 3274 ) ( tabella 1 )  . 
tutti i pazienti hanno ricevuto lorgano da cadavere ( 100% ) , trapiantati in 9 casi in fossa iliaca sinistra ( 53% ) ed in 8 in fossa iliaca destra ( 47% ) con anastomosi termino - laterale nellarteria iliaca esterna ( 100% )  . 
preliminary angiography shows the presence of severe stenosis of the transplanted renal artery ( a ) , which was treated with a balloon - expandable stent , with restoration of vessel diameter ( b )  . 
lesame angiograco documenta la presenza di stenosi di grado severo dellarteria renale trapiantata ( a ) , trattata mediante posizionamento di stent balloon - expandable con ripristino di buon calibro vasale ( b )  . 
collateralmente si documenta presenza di ramo polare . under uoroscopy , an introducer was placed , with its distal end near the origin of the renal artery , through a hydrophilic guide with a 0.035 - j - tip ( terumo corp , tokyo , japan )  . 
with the aid of a 5 - f guidewire ( vertebral , terumo corp ) , the stenosis was crossed with a 0.018 - guidewire ( thruway , boston scientic , natick , ma , usa )  . 
these were tsunami ( terumo corp ) in ten cases and express vascular ( boston scientic ) in seven ; mean diameter was 5.35 mm ( 11 / 17 5 mm ; 6 / 17 6 mm ) and mean length 17.1 mm ( 12 / 17 18 mm ; 5 / 17 15 mm )  . haemostasis was obtained with the perclose proglide system ( abbott vascular inc . , redwood city , ca , usa ) in 11 / 17 cases ( 56% ) and with manual compression in 6 / 17 cases ( 44% )  . 
stato impiegato mezzo di contrasto organo - iodato idrosolubile , nefrotropico a bassa osmolarit ( visipaque 270 mg / ml , ge healthcare as , oslo , norvegia ) , diluito al 50% con soluzione siologica per prevenire danni nefrotossici correlati al mezzo di contrasto ( mdc )  . 
prima di effettuare il trattamento stato somministrato un bolo endovena ( ev ) di eparina sodica ( 50 ui / kg )  . sotto controllo uoroscopico mediante lausilio di guida idrolica con punta j 0 , 035 inch ( terumo corp , tokyo , giappone ) si proceduto a posizionamento di introduttore con estremo distale in prossimit dellorigine dellarteria renale . 
con lausilio di catetere guida 5 f ( vertebral , terumo corp , tokyo , giappone ) stata valicata la stenosi mediante una guida di 0 , 018 inch ( thruway , boston scientic , natek , na , usa )  . 
follow - up was performed by clinicallaboratory assessment with determination of serum creatinine ( scr ) and blood pressure ( bp ) and cdus at 1 , 3 , 6 and 12 months and yearly thereafter . preand posttreatment scr and bp values were compared using the t test , with p < 0.05 being considered a statistically signicant difference . 
mean number of drugs administered before and after treatment and degree of residual stenosis were compared with cdus , considering stenosis < 60% , tsunami ( terumo corp , tokyo , giappone ) ed in sette casi di tipo express vascular ( boston scientic , natek , na , usa )  . 
stata impostata doppia terapia antiaggregante con acido acetil - salicilico ( asa ) ( 100 mg / die ) e clopidogrel ( 75 mg / die ) per 30 giorni , quindi asa a tempo indenito . 
 stato eseguito follow - up mediante esami clinico - laboratoristici con controllo della creatinina e della pressione arteriosa ed esame ecd ad 1 , 3 , 6 , 12 mesi e successivamente una volta lanno . sono stati confrontati i valori di creatinina sierica e di pressione arteriosa pree post - trattamento mediante test t di student , considerando una differenza statisticamente signicativa il riscontro di valori di p < 0 , 05 . 
sono stati inoltre confrontati il numero medio di farmaci somministrati prima e dopo il trattamento ed il grado di stenosi residua mediante ecd , considerando come non emodinamicamente signicativa una stenosi < 60% , con riscontro di vps < 160 cm / s e ir compreso tra 0 , 56 e 0 , 7 . risultati periodo considerato osservazionale nel ( gennaio 2005 - dicembre 2010 ) presso il nostro ospedale sono stati effettuati 472 trapianti renali , di cui 15 da donatore vivente ; di questi , il 3 , 6% ( 17 pazienti ) ha sviluppato tras , trattata per via endovascolare mediante pta / stenting dellarteria renale trapiantata . 
il tempo medio intercorso tra il trapianto e la diagnosi di tras stato di 9 , 3 mesi ( range : 143 mesi ) ; la sede pi frequente di stenosi ( 88% ) era quella anastomotica ( 15 / 17 pazienti ) , solo nel 12% dei casi ( 2 / 17 ) era localizzata al tratto medio dellarteria renale . 
abbiamo avuto solo una complicanza peri - procedurale rappresentata dallo sviluppo di pseudoaneurisma nella sede di puntura ( trattato con successo mediante compressione eco - guidata dello stesso )  . durante il follow - up in un caso si osservato il decesso a distanza di 48 mesi dalla procedura per patologia non inerente al trattamento o per insufcienza renale . 
due pazienti , a 24 e 29 mesi dal posizionamento dello stent , hanno sviluppato insufcienza renale ( in un caso per ripresa della malattia antecedente il trapianto e nel restante caso per rigetto cronico del graft ) e hanno ripreso il trattamento emodialitico : dopo tale termine sono stati pertanto esclusi dal follow - up . 
ad un follow - up medio di 28 , 318 , 7 mesi , abbiamo riscontrato in tutti i casi una riduzione dei valori di creatinina sierica , con diminuzione del valore medio da 2 , 52 mg / ml pre - procedura a 1 , 7 mg / ml post - trattamento ; tale differenza risultata statisticamente signicativa ( p < 0 , 05 )  . 
the most common site of stenosis ( 88% ) was the anastomosis ( 15 / 17 patients ) ; only in 12% of cases ( 2 / 17 ) did stenosis develop in the middle portion of the renal artery . 
the technical success rate was 100% , with only one periprocedural complication , which consisted of the development of a pseudoaneurysm at the puncture site ( treated successfully by us - guided compression )  . 
two patients , 24 and 29 months after stent placement , developed kidney failure ( in one case due to disease relapse before transplantation and in the other to chronic graft rejection ) ; these patients resumed haemodialysis and were excluded from further follow - up . 
during an average follow - up of 28.318.7 months , scr values fell in all cases , the mean value decreasing from 2.52 mg / ml to 1.7 mg / ml after treatment . 
in 82% of cases ( 14 / 17 patients ) , cdus revealed an absence of haemodynamic stenosis ; in the remaining 18% ( 3 / 17 ) , it identied moderate restenosis ( around 60% ) with psv ( < 200 cm / s ) , which were not associated with abnormalities in organ function and therefore not deserving of new endovascular treatment . 
the onset of arterial hypertension is , in fact , associated with renal hypoperfusion , with consequent organ ischaemia which , if not promptly corrected , may irreversibly compromise graft function [ 10 ]  . the incidence of tras is extremely variable : humar et al . 
alla valutazione ecd abbiamo evidenziato nell82% dei casi ( 14 / 17 pazienti ) lassenza di stenosi emodinamica ; nel restante 18% ( 3 / 17 ) si riscontrata la presenza di re - stenosi di grado moderato ( 60% circa ) con riscontro di vps ( < 200 cm / s ) , non associate ad alterazioni della funzionalit dorgano e pertanto non meritevoli di nuovo trattamento endovascolare . 
si passati da una terapia medica costituita dallassunzione media di 3 , 50 , 5 a 1 , 50 , 5 farmaci anti - ipertensivi ( tabella 2 )  . discussione la tras la pi frequente complicanza vascolare del trapianto renale , responsabile dell1%5% dellipertensione refrattaria post - trapianto [ 8 ] la cui diagnosi precoce fondamentale per un tempestivo ed efcace trattamento . 
 lo sviluppo di ipertensione arteriosa si associa infatti ad ipoperfusione renale con conseguente sofferenza ischemica dorgano che , se non prontamente corretta , pu compromettere in maniera irreversibile la funzionalit del trapianto stesso [ 10 ]  . lincidenza di tras estremamente variabile : humar et al . 
 [ 12 ] hanno evidenziato un incremento della diagnosi con incidenza passata dal 2 , 4% al 12 , 4% dallintroduzione routinaria dellecd come metodica diagnostica , analogamente a mammer et al . 
nella nostra esperienza , con impiego routinario dellecd nella valutazione diagnostica di pazienti trapiantati , abbiamo evidenziato unincidenza di tras del 3 , 6% , in linea con i dati riportati in letteratura [ 5 , 1114 ]  . 
 nella nostra esperienza tutti i casi di tras sospetti in base al riscontro allecd di caratteristiche indicative di stenosi emodinamicamente signicative sono stati confermati allangiograa diagnostica eseguita prima del trattamento , a testimoniare lafdabilit di tale metodica nella diagnosi di tras , come riportato in letteratura [ 1619 ]  . 
 [ 20 ] il riscontro isolato di alterazioni ecd in assenza di modicazioni dei parametri clinico - laboratoristici , non di per s indicativo di tras da trattare : nel nostro follow - up abbiamo infatti riscontrato tre casi di re - stenosi di grado moderato non associati ad aumento della creatinina o della pressione arteriosa che non sono stati trattati nuovamente , senza che ci inciasse lefcacia del trapianto a lungo termine . radiol med ( 2013 ) 118 : 826836 cdus into clinical practice . 
in our experience , routine use of cdus in the diagnostic assessment of transplant patients yielded an incidence of tras of 3.6% , consistent with the literature [ 5 , 1114 ]  . 
hence , we believe diagnostic assessment with cdus is a valuable and important addition to clinicallaboratory parameters for identifying the condition [ 15 ]  . in our experience , all cases of suspected tras on the basis of cdus evidence of haemodynamically signicant stenosis were conrmed at diagnostic angiography performed prior to treatment , thus proving cdus reliability in tras diagnosis , as reported in the literature [ 1619 ]  . 
 [ 20 ] , an isolated nding of cdus abnormalities without corresponding clinicallaboratory changes is not indicative per se that tras is deserving of treatment : in our follow - up , there were three cases of moderate restenosis not associated with elevated scr or bp and which were not retreated . 
this did not affect the long - term effectiveness of the transplantation . in our experience , all cases of tras occurred in cadaveric transplants , as also reported in the literature [ 12 ] , which suggests that immunological factors and prolonged ischaemia of the donor kidney are implicated in the aetiopathogenesis . 
the most frequent site of stenosis , as observed in our study , is the proximal portion of the artery [ 21 ] , and this is related to myointimal hyperplasia at the site of the surgical anastomosis . 
the mean interval between renal transplantation and tras diagnosis was 9.34.5 months , in keeping with the literature data [ 7 ] , which report the frequent early onset of tras . standard treatment of tras was surgery , with anastomosis resection and revision , stenotic segment bypass with autologous vein or endarterectomy and with a technical success rate of 6392% and a recurrence rate of 12% [ 7 ]  . 
this option was , however , burdened by a high risk of complications , such as loss of the transplanted kidney ( 1520% ) , ureteral damage ( 14% ) , reoperation for suboptimal outcome ( 13% ) and death ( 5% ) [ 22 ] ; it was , therefore , rapidly replaced with endovascular treatment as the approach of choice , with surgery being reserved for cases of repeated failure of the endovascular approach or severe stenosis not amenable to pta [ 23 ]  . initially , the endovascular treatment of choice for tras was pta , which ensured clinical success with normalisation of scr in 8593% of cases and of arterial pressure in 63 83% of cases and a risk of complications such as arterial dissection , thrombosis or anastomosis rupture of 4% [ 24 ] and an incidence of restenosis between 5% and 30% [ 25 ]  . in recent years , the combined use of pta and stenting has established itself as the treatment of choice , as it ensures greater immediate and mediumto long - term success ( 90 100% ) than pta alone , with a low rate of complications in the transplanted renal artery [ 26 ]  . 
 [ 27 ] nella nostra esperienza tutti i casi di tras si sono vericati in trapianti da cadavere : ci in linea con quanto pubblicato in letteratura [ 12 ] e sembra far propendere per un ruolo eziopatogenetico giocato da fattori immunologici e dalla prolungata ischemia del rene donatore . 
la sede pi frequente di stenosi , come osservato nel nostro studio , quella prossimale [ 21 ] e ci da mettere in relazione ad iperplasia miointimale nella sede di anastomosi chirurgica . 
abbiamo riscontrato un intervallo medio tra trapianto renale e diagnosi di tras di 9 , 34 , 5 mesi , in accordo con i dati della letteratura [ 7 ] che documentano la frequente insorgenza precoce di tale patologia dopo il trapianto stesso . nel passato il trattamento standard di tale patologia era rappresentato dallintervento chirurgico , con resezione e revisione dellanastomosi , by - pass con vena autologa del tratto stenotico o endoarterectomia , con successo tecnico del 63%92% e tasso di recidiva del 12% [ 7 ]  . 
tale opzione , gravata da alti rischi di complicanze , come la perdita del rene trapiantato ( 15%20% ) , danno ureterale ( 14% ) , re - intervento per risultato non ottimale ( 13% ) e mortalit ( 5% ) [ 22 ] , stata rapidamente sostituita dal trattamento endovascolare come approccio di scelta e rappresenta oggi un intervento di seconda istanza in caso di ripetuto fallimento dellapproccio endovascolare o in caso di stenosi severe inaccessibili alla pta [ 23 ]  . il trattamento endovascolare effettuato inizialmente per la tras stata la pta , che assicurava un successo clinico con normalizzazione dei valori di creatinina sierica nell85%93% dei casi e della pressione arteriosa nel 63%83% dei casi , con un rischio di complicanze quali dissezione arteriosa , trombosi o rottura dellanastomosi del 4% [ 24 ] ed incidenza di re - stenosi del 5%30% [ 25 ]  . negli ultimi anni si affermato come opzione di scelta per il trattamento della tras lapproccio combinato pta / stenting , che assicura un maggior successo immediato e a medio - lungo termine ( 90%100% ) rispetto alla sola pta , con una ridotta incidenza di complicanze a livello dellarteria renale trapiantata [ 26 ]  . 
 [ 27 ] hanno riscontrato che la sopravvivenza a 5 anni dei pazienti con tras trattati mediante pta / stenting era del 76 , 3% , maggiore di quella dei pazienti sottoposti a trapianto renale che non avevano sviluppato tras ( 72 , 9% ) , a sottolineare lefcacia di tale trattamento . sono pochi gli studi che hanno valutato il trattamento della tras mediante stent [ 2736 ] e tutti ne hanno documentato lefcacia in termini di successo tecnico immediato e a lungo termine e di miglioramento clinico - laboratoristico , indicando tale approccio come opzione di scelta nella gestione terapeutica della tras . 
 nella nostra esperienza , in linea con i dati della letteratura [ 3036 ] , il trattamento della tras mediante predilatazione della lesione stenosante e successivo stenting 834 radiol med ( 2013 ) 118 : 826836 reported that patients with tras treated with pta / stenting had a 5 - year survival rate of 76.3% , that is , higher than kidney transplant patients who had not developed tras ( 72.9% ) , emphasising the effectiveness of the treatment . only a few studies have assessed stenting in the treatment tras [ 2736 ] , and all documented its effectiveness in terms of immediate and long - term technical success and improvement in clinicallaboratory parameters , suggesting this approach as the treatment of choice for managing tras . in our experience , as reported in the literature [ 3036 ] , treating tras by predilatation and subsequent stenting has proved to be a safe and effective option : technical success was achieved in all cases treated , with restoration of vessel diameter and improvement of renal haemodynamics . our results are consistent with the literature and document the effectiveness of endovascular treatment of tras with stenting : valpreda et al . 
 [ 35 ] , in a retrospective evaluation of 30 cases of tras treated with pta / stenting , achieved 100% technical success with , a signicant reduction in bp and scr , at a mean follow - up of 7.1 years , without any difference in survival between patients with tras treated with stenting and transplanted patients without tras . 
 [ 36 ] , in a retrospective study of eight patients with tras , found a statistically signicant improvement in renal function and bp after stent placement , with reduction of antihypertensive drugs , documenting the long - term effectiveness ( mean follow - up 42.59 months ) of endovascular treatment . in our experience , cdus revealed no restenosis in 82% of cases and only moderate restenosis ( approximately 60% ) not associated with graft function deciencies and thus not requiring further treatment in the remaining 18% . 
 [ 35 ] , who observed a restenosis incidence of 15.6% ( 5 / 30 patients ) , which was not haemodynamically signicant in most cases , and requiring further endovascular pta in one case only . drawing on the experience gained in cardiac settings , the use of drug - eluting stents ( des ) could alleviate the issue of restenosis : however , though promising , the few reports refer to small case series with limited follow - up periods [ 37 , 38 ]  . 
 consistent with the literature [ 2836 ] , our study documents the effectiveness of endovascular treatment of tras with pta / stenting , which ensures adequate recovery of kidney function in the absence of major complications . 
in patients with clinicallaboratory parameters suspicious for tras , integration with cdus is important , as , in experienced hands , it has high sensitivity and specicity for diagnosing this condition . 
based on our experience , we believe pta / stenting to be the rst - line treatment in managing tras , as it ensures good immediate and mediumto longterm results . della stessa si rivelata unopzione sicura ed efcace : in tutti i casi da noi trattati abbiamo ottenuto successo tecnico , con ripristino di un buon calibro vasale e miglioramento dellemodinamica renale . i risultati da noi ottenuti sono in linea con i dati della letteratura e documentano lefcacia del trattamento endovascolare delle tras mediante posizionamento di stent : valpreda et al . 
 [ 35 ] , nella loro valutazione retrospettiva di 30 pazienti affetti da tras trattati mediante pta / stenting , hanno ottenuto un successo tecnico del 100% , con riscontro , ad un follow - up medio di 7 , 1 anni , di una riduzione statisticamente signicativa dei valori di pressione arteriosa e di creatinina sierica , in assenza di differenza in termini di sopravvivenza tra i pazienti con tras trattati mediante stenting rispetto ai pazienti trapiantati non affetti da tras . 
 [ 36 ] , in un recente studio retrospettivo di 8 pazienti affetti da tras , hanno riscontrato un miglioramento statisticamente signicativo della funzionalit renale e della pressione arteriosa dopo posizionamento di stent , con riduzione dei farmaci anti - ipertensivi impiegati , documentando lefcacia a lungo termine ( follow - up medio di 42 , 59 mesi ) del trattamento endovascolare in tale patologia . 
 nella nostra esperienza nell82% dei casi non abbiamo avuto riscontro ecd di re - stenosi , riscontrate invece nel restante 18% , ma di grado moderato ( 60% circa ) e non associate ad alterazioni della funzionalit dorgano e pertanto non meritevoli di ri - trattamento . 
 [ 35 ] , che hanno riscontrato unincidenza di re - stenosi del 15 , 6% ( 5 / 30 pazienti ) nella maggior parte dei casi non emodinamicamente signicativa e solo in un caso meritevole di ulteriore trattamento endovascolare mediante pta . mutuando lesperienza accumulata in ambito cardiologico , limpiego di stent a rilascio di farmaci ( des ) potrebbe in futuro ridurre il problema della re - stenosi : tuttavia gli scarsi dati bibliograci , pur con risultati promettenti , si riferiscono a casistiche poco numerose e con breve follow - up [ 37 , 38 ]  . il nostro studio , in linea con i dati della letteratura [ 2836 ] , documenta lefcacia del trattamento endovascolare mediante pta / stenting nel trattamento della tras che garantisce un adeguato recupero della funzionalit renale in assenza di complicanze maggiori associate . 
importante in pazienti con parametri clinico - laboratoristici sospetti per tras , lintegrazione con lesame ecd che presenta , in mani esperte , alta sensibilit e specicit nella diagnosi di tale patologia . 
dewey springer heidelberg dordrecht london new york , 2011 isbn : 978 - 3 - 642 - 14021 - 1 e - isbn : 978 - 3 - 642 - 14022 - 8 published online : 25 july 2013 springer - verlag 2013 this book is impressive . 
 importantly , due to the increased spatial and temporal resolution of 64 - row and 320 - row scanners and their dual source technology , it is now possible to study with great care and precision the coronary arteries , through non invasive ct angiography or coronary ct angiography . 
 the reader is guided through technical and personnel requirements ( how long for instance training should take to properly report the obtained images ) , how to purchase these wonderful machines , how profound the knowledge of coronary anatomy and their variants must be to make useful connections with cardiology knowledge . 
the reader will also receive precise details on patient preparation ( medication , breath - hold instructions etc . ) as well as useful information on the radiation protection issues related to this sort of procedure . the authors also discuss the different types of ct machines now available on the market , highlighting their pros and cons and different capabilities offered by the vendors to operators in the eld . the application of coronary ct angiography in plaque and calcication imaging is well described , as well as assessment of cardiac functions and valves . 
hints are also provided on the evaluation of stent lumen patency or patency reduction in patient follow - up ( at the present time still a source of debate due to device blooming artefacts )  . 
one will learn how one heart - beat ( one second scanning time ! ) and ensuing contrast medium reduction is affordable with 320row scanners at the expense of increased scattered radiation and ensuing image noise . all throughout the book there are plentiful and very beautiful ct images covering the technical spectrum , in impressionante , questo volume ! nel testo sar possible trovare tutte le possibili informazioni sulla tomograa computerizzata ( tc ) indirizzata alla valutazione delle coronarie e delle malattie congenite del cuore . 
fatto veramente importante , dato laumento della risoluzione spaziale e temporale offerte dalle attrezzature a 64 e 320 detettori ed alla tecnologia a doppia sorgente , ora possibile studiare con grande accuratezze e precisione le arterie coronarie mediante la tecnica angio - tc non invasiva o la coronarograa tc . 
 il lettore viene guidato attraverso i requisiti tecnici e personali ( per esempio , quanto a lungo deve essere il periodo di apprendimento prima di poter refertare corretamente le immagini ottenute ) , su come acquistare queste mecchine meravigliose e su quanto profonda debba essere la conoscenza dellanatomia delle coronarie e delle loro varianti per poter instaurare utili raffronti con le rispondenze cardiologiche . 
il lettore trover anche precise informazioni sulla preparazione del paziente ( premedicazione , istruzioni su come trattenere il respiro , etc . ) , nonch utili informazioni sulle problematiche della radioprotezione correlate a questa tipologia di indagine . gli autori presentano anche una digressione relativa alle diverse tipologie di attrezzature oggi disponibili sul mercato , mettendone in evidenza i pro ed i contro nonch le differenti opzioni operative offerte dai costruttori agli utilizzatori delle stesse . lutilizzo della coronarograa tc nella valutazione per immagini delle placche e delle calcicazioni coronariche ben descritta , come la valutazione della funzionalit sia cardiaca che valvolare . 
sono inoltre forniti suggerimenti sulla valutazione della perviet del lume degli stent o sulla riduzione del loro calibro nei controlli dei pazienti ( argomento allo stato attuale fonte di discussione a seguito degli artefatti da blooming )  . 
sar possibile imparare come si possa ottenere una riduzione ad un solo battito cardiaco ( un solo secondo per la ripresa ! ) con conseguente riduzione del mezzo di contrasto con gli apparecchi a 320 detettori , a scapito per di una maggior radiazione diffusa e conseguente maggior rumore dellimmagine . 
 il volume corredato da numerose immagini tc qualitativamente apprezzabili documentanti lo spettro tecnico , in 1070 radiol med ( 2013 ) 118 : 10691070 correlation , when necessary , with angiographic images ( coronary angiography is still an important tool in the evaluation of some of the presented and discussed conditions )  . 
 one will nd a very long chapter devoted to clinical cardiac ct cases in order to become properly familiar with them . in this book chapter titles , abstracts , tables , listings are not in the usual springer pale - blue style but in a sort of oldfashioned rose colour . 
 this is a book to be treasured by the radiologists and cardiologist who discover a mint of wise and precise information in their daily practice . correlazione , se e quando necessario , con immagini angiograche tradizionali ( la coronarograa ancora un importante strumento nella valutazione di alcune delle situazioni presentate e discusse )  . 
il lettore trover inne un lungo capitolo dedicato a casi clinici di cardio - tc allo scopo di familiarizzarsene . in questo volume , titoli dei capitoli , abstract , tabelle , elenchi non sono evidenziati con lusuale stile blu tenue delleditore springer , ma con un pallido rosa antico . 
we detected 31 superior labral anterior posterior ( slap ) lesions , all conrmed on arthroscopy with three cases of underestimation : in the detection of slap lesions , the sensitivity , specicity , accuracy , positive predictive value ( ppv ) and negative predictive value ( npv ) of mr arthrography were 100% ; in the evaluation of the type of slap lesion , sensitivity was 100% , specicity was 78.5% , accuracy was 92.8% , ppv was 71.7% and npv was 100% . 
all cases of capsular laxity ( 13 / 42 ) and biceps tendon lesions ( 3 / 42 ) were conrmed on arthroscopy with sensitivity , specicity , accuracy , ppv and npv of 100% . 
 eleven cuff lesions were detected on mr arthrography , 10 of which conrmed at arthroscopy : sensitivity was 100% , specicity was 96.8% , accuracy was 97.6% , ppv was 90.9% and npv was 100% . 
the role of mr arthrography is to describe the key features of lesions affecting the superior portion of the shoulder , including location , morphology , extent , and associated injuries and riassunto obiettivo . 
abbiamo riscontrato 31 lesioni del labbro glenoideo superiore da anteriore a posteriore ( slap lesions ) , tutte confermate allesame artroscopico con 3 casi di sottostima del grado di lesione : nella individuazione delle slap lesions la sensibilit , specicit , accuratezza , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) dellartro - rm sono risultati del 100% ; nella valutazione del tipo di slap lesion la sensibilit stata del 100% , la specicit del 78 , 5% , laccuratezza del 92 , 8% , il vpp del 71 , 7% e il vpn del 100% . 
tutti i casi di lassit capsulo - legamentosa ( 13 / 42 ) e di lesione del tendine del capo lungo del bicipite ( 3 / 42 ) sono stati confermati allartroscopia con sensibilit , specicit , accuratezza , vpp e vpn del 100% . 
delle 11 lesioni dei tendini della cufa dei rotatori diagnosticate con artro - rm , 10 sono state confermate artroscopicamente con sensibilit del 100% , specicit del 96 , 8% , accuratezza del 97 , 6% , vpp del 90 , 9% e vpn del 100% . 
lesioni associate sono state diagnosticate in 38 / 42 pazienti . radiol med ( 2013 ) 118 : 10221033 1023 anatomical variants and to correlate these features with clinical symptoms . keywords shoulder mr arthrography instability superior instability slap lesion conclusioni . 
il ruolo dellartro - rm quello di valutare le caratteristiche delle lesioni della porzione sovraequatoriale della spalla , descrivendone la sede , la morfologia e lestensione e di identicare e descrivere la presenza di lesioni e varianti anatomiche associate . parole chiave spalla artrograa - rm instabilit instabilit superiore slap lesion introduction introduzione glenohumeral instability is a common cause of shoulder pain and loss of shoulder function and refers to the symptomatic subluxation or dislocation of the humeral head in relation to the glenoid fossa [ 1 ]  . 
among them , the most commonly adopted by orthopaedic surgeons is the matsen - snydercastagna classication which includes traumatic unidirectional instability with bankart lesion and requiring surgery ( tubs ) , atraumatic multidirectional bilateral instability responsive to rehabilitation , inferior capsular shift and interval closure ( ambrii ) , and a group of subtle conditions of minor instability secondary to repeated microtraumas and known as acquired instability from overstress usually treated with surgery ( aios ) [ 24 ]  . labral position is located by superimposing the face of a clock onto the surface of the glenoid , and by convention 12 oclock is superior and 6 oclock is inferior ; the 9 to 3 oclock position of the glenoid fossa corresponds to the superior zone of the glenoid labrum or supraequatorial area , 3 oclock is the anterior portion and 9 oclock the posterior portion [ 5 ]  . 
the supraequatorial region includes structures that have an important role in static and dynamic stabilisation of the glenohumeral joint ( rotator interval , long head of the biceps brachii , superior glenoid labrum , superior and middle glenohumeral ligaments and tendons of rotator cuff )  . 
lesions or anatomical variants of these structures are related to shoulder instability [ 610 ]  . evaluation of the superior zone is diagnostically challenging from an imaging standpoint because of the large number of normal variations which occur in this location and the difculty in accurately assessing superior labral injuries . 
the purpose of this study was to evaluate the role of the mr arthrography in the identication and classication of lesions that support superior instability , comparing imaging ndings with the data from arthroscopic surgery . linstabilit gleno - omerale una causa comune di dolore e perdita della funzionalit della spalla ed responsabile di sublussazioni sintomatiche o lussazioni della testa omerale rispetto alla fossa glenoidea [ 1 ]  . 
esistono molte classicazioni delle instabilit di spalla , tra queste la pi adottata dai chirurghi ortopedici quella di matsen - snyder - castagna che include le traumatic unidirectional bankart lesions , responds to surgery ( tubs ) , che vanno incontro a trattamento chirurgico , le atraumatic multidirectional bilateral responds to rehabilitation inferior capsular shift , and interval closure ( ambrii ) , che giovano solitamente di un trattamento conservativo riabilitativo e le acquired instability overstress surgery ( aios ) caratterizzate da microinstabilit acquisita secondaria ad eventi microtraumatici ripetuti [ 24 ]  . la regione sovra - equatoriale , o superiore , di spalla unarea anatomica dellarticolazione gleno - omerale che si pu denire come la regione della glenoide che va da ore 9 ad ore 3 , considerando il quadrante di un orologio sulla supercie della glena , dove ore 12 il nord , ore 6 il sud , ore 3 la porzione anteriore e ore 9 la porzione posteriore [ 5 ]  . 
la regione sovra - equatoriale include alcune strutture anatomiche che hanno un ruolo fondamentale nella stabilizzazione statica e dinamica dellarticolazione gleno - omerale ( intervallo libero dei rotatori , tendine del capo lungo del bicipite brachiale , cercine glenoideo superiore , legamenti gleno - omerali superiore e medio e i tendini della cufa dei rotatori )  . 
lesioni o varianti anatomiche di queste strutture sono correlate con linsorgenza di instabilit superiore di spalla [ 610 ]  . la valutazione della regione superiore ( sovra - equatoriale ) della spalla difcoltosa sia a causa del numero elevato di varianti anatomiche presenti in questa zona , sia a causa della difcolt nella precisa stima delle lesioni labrali superiori . 
lartro - risonanza magnetica ( rm ) sembra essere la tecnica di imaging migliore attualmente disponibile per la valutazione della regione gleno - omerale superiore [ 11 13 ]  . 
lo scopo del nostro studio quello di valutare il ruolo dellartro - rm nellidenticazione e classicazione delle le1024 materials and methods from january 2007 to january 2010 , we retrospectively reviewed 42 patients ( 30 men and 12 women ; mean age , 36 years ; age range , 1962 years ; median age , 33 ) who underwent mr arthrography of the shoulder followed by arthroscopic surgery . 
 all patients had clinical signs of chronic supraequatorial instability of the shoulder , with diffuse , difcult to pinpoint , shoulder pain radiating to the arm , exacerbated by external rotation and arm extension and associated with weakness . 
exclusion criteria were : a history of recent traumatic events ( within the last year ) or surgical procedures on the shoulder and clinical signs of primary rotator cuff disease . the mean interval between mr arthrography and arthroscopy was 3 months ( 15 months )  . all mr studies were performed with a dedicated shoulder coil using a 1.5 - t scanner [ eclipse , picker - marconi ( unit 1 ) and avanto , siemens ( unit 2 ) ]  . 
the intraarticular injection was done without uoroscopic guidance using a 19.5 - gauge spinal needle and with the administration of 20 ml of paramagnetic contrast agent ( magnevist 2 mmol / l , bayer - schering , berlin , germany ; dotarem 2.5 mmol / l , guerbet , france )  . 
 materiali e metodi nel periodo compreso tra gennaio 2007 e gennaio 2010 , abbiamo valutato retrospettivamente 42 pazienti ( 30 maschi e 12 femmine ) con et media di 36 anni ( range : 1962 anni , mediana : 33 anni ) sottoposti ad artro - rm di spalla e successiva chirurgia artroscopica . tutti i pazienti presentavano clinicamente segni di instabilit sovra - equatoriale cronica di spalla con dolore aspecico , irradiato allarto omolaterale , spesso esacerbato dallextrarotazione e associato a decit di forza . 
i sintomi erano presenti da un periodo di 36 mesi e tutti i pazienti erano stati trattati conservativamente , senza benecio , con farmaci antiinammatori non steroidei ( fans ) e siochinesiterapia ( fkt )  . sono stati esclusi dallo studio i pazienti con anamnesi positiva per eventi traumatici recenti ( nellultimo anno ) , i pazienti con quadro clinico riconducibile alla presenza di patologia della cufa dei rotatori ed i pazienti con pregresso intervento chirurgico alla spalla . lintervallo medio tra lesame artro - rm e lartroscopia di spalla stato di 3 mesi ( 15 mesi )  . tutti gli esami sono stati eseguiti utilizzando una bobina dedicata essibile per la spalla con magnete da 1 , 5 t : eclipse , picker - marconi ( unit 1 ) and avanto , siemens ( unit 2 )  . 
liniezione dellarticolazione stata eseguita senza guida scopica , con ago spinale 19 , 5 g e successiva iniezione intra - articolare di 20 ml di contrasto paramagnetico ( magnevist 2 mmol / l ; bayer - schering berlino , germania ; dotarem 2 , 5 mmol / l , guerbet , francia )  . 
 nel protocollo dellunit 1 venivano utilizzate sequenze spin echo ( se ) t1 pesate [ tempo di ripetizione ( tr ) 500 ms , tempo di eco ( te ) 12 ms , matrice 256512 , number of signal averages ( nsa ) 1 , thickness 3 , 54 mm ] per ottenere immagini nei piani sagittale , coronale ed assiale . 
field of view ( fov ) varied from 16 to 20 cm . the mr arthrograms were retrospectively assessed for the presence of three parameters : slap lesions , capsular laxity of the rotator interval , and abnormalities of the long head of the biceps tendon . 
identied associated lesions were gleno - labral articular disruption ( glad ) ; anterior labroligamentous periosteal sleeve avulsion ( alpsa ) ; glenohumeral ligament lesions ; bankart or bony bankart lesions ; partial or complete rotator cuff tears ( supraspinatus tendon ) ; ambrii and anatomical variations [ buford complex ; foramen sublabralis ; hypotrophic or hypertrophic bid middle glenohumeral ligament ( mgh ) ; accessory glenohumeral ligament ( ghl ) ]  . 
all cases of abnormality of the long head of the biceps tendon were associated with rotator cuff lesions . in t2 con saturazione del segnale del grasso [ dp / t2 fatsat , tr 4000 ms , te 19 / 96 ms , ip angle ( fa ) 90 , matrice 256256 , nsa 2 ; thickness 4 mm ] sul piano coronale e sequenze 3d fse con soppressione del grasso pesate in t1 ( tr 31 ms , te 7 ms , fa 90 , matrice 256256 , nsa 2 , thickness 0 , 50 mm ) per ottenere immagini assiali . 
il campo di vista ( fov ) era variabile da 16 a 20 cm . gli esami artro - rm sono stati revisionati retrospettivamente , sono stati ricercati tre parametri : la presenza di lesioni del labbro glenoideo superiore da anteriore a posteriore ( slap lesions ) , di lassit capsulare dellintervallo libero e di lesioni del capo lungo del bicipite . 
 alterazioni documentabili del capo lungo del bicipite ( clb ) sono state evidenziate solo in 3 casi ( 7 , 1% ) : 1 pazien1026 radiol med ( 2013 ) 118 : 10221033 table 1 comparison between mr arthrography and arthroscopy pt . 
 le lesioni del clb descritte in 3 pazienti allindagine in rm sono state tutte confermate allartroscopia ( 3 vp , 0 fp , 39 vn , 0 fn ) con sensibilit , specicit , accuratezza , vpp e vpn del 100% . 
lassit capsulare dellintervallo libero ( freccia bianca vuota )  . thrography , and all lesions were conrmed at arthroscopy ( 13 tp , 0 fp , 29 tn , 0 fn ) , resulting in 100% sensitivity , specicity , accuracy , ppv and npv . 
 the biceps tendon lesions detected in three patients on mr arthrography were all conrmed at arthroscopy ( 3 tp , 0 fp , 39 tn , 0 fn ) resulting in 100% sensitivity , specicity , accuracy , ppv and npv . 
il mdc opacizza larea di lesione del tendine ( freccia )  . discussion superior instability is an important cause of chronic pain and is difcult to diagnose with physical examination only , so that the support of imaging is fundamental [ 14 , 15 ]  . 
the in 2 / 42 ( 4 , 7% ) casi si osservata discordanza tra i reperti artroscopici ed i reperti artrograci per quanto riguarda le lesioni associate ; in 1 paziente lindagine artro - rm aveva permesso di evidenziare una lesione osteocartilaginea 1030 radiol med ( 2013 ) 118 : 10221033 di bankart che la revisione artroscopica classicava come semplice distacco capsulo - labrale brocartilagineo ; in un altro caso non stata dimostrata con lartroscopia la tendinopatia degenerativa del tendine del sovraspinato e la borsite sub - acromion deltoidea . 
la sensibilit dellartro - rm nellidenticazione di lesioni associate stata del 93 , 5% . discussione linstabilit superiore unimportante causa di dolore cronico , questa condizione molto difcile da diagnosticare solo sulla base del solo esame obiettivo e quindi risulta fondamentale il supporto dellimaging [ 14 , 15 ]  . 
le patologie che interessano la porzione sovra - equatoriale di spalla sono responsabili di instabilit e comprendono le lesioni dellintervallo libero dei rotatori ( ilr ) , le lesioni del clb e le slap lesions [ 5 , 16 , 17 ]  . 
 la difcolt di identicazione pu essere spiegata con il tipo di approccio scelto per lartroscopia , il portale anteriore , in presenza di aspetto lasso della capsula anteriore , non ha la profondit necessaria a esplorare lilr [ 18 , 19 ]  . 
 [ 20 ] hanno studiato la complessa anatomia e limportante ruolo svolto dallilr nella stabilizzazione dellarticolazione gleno - omerale ; lanatomia normale dellilr stata correttamente dimostrata con lartro - rm , metodica che si rivelata superiore allimaging rm non artrograco nella identicazione delle strutture che compongono lilr , in particolare utilizzando piani di studio orientati in base allanatomia della struttura da esaminare [ 20 ]  . 
si deve infatti tenere in considerazione che la patologia sovra - equatoriale di spalla e quindi dellilr raramente si manifesta isolata , come dimostrato anche nella nostra serie , e quindi il solo esame basale indurrebbe alla riparazione chirurgica delle sole alterazioni diagnosticate [ 17 , 21 , 22 ]  . unaccurata diagnosi e descrizione di queste anomalie pu aiutare lortopedico [ 23 ] , infatti descritto in letteratura che le lesioni dellilr e linstabilit bicipitale con o senza danno strutturale del tendine , non riparate durante lartrofig . 
il mdc imbibisce larea di lesione del tendine ( freccia nera vuota )  . commonest causes of shoulder pain are abnormalities of the rotator interval or long head of the biceps tendon , and slap lesions [ 5 , 16 , 17 ]  . 
the term refers to the awkward identication at arthroscopic investigation , probably explainable by the anterior arthroscopic approach that makes it difcult to explore the free interval [ 18 , 19 ]  . 
they suggest that the rotator cuff interval can be best outlined by mr arthrography using both conventional and dedicated imaging planes [ 20 ]  . in a series of patients studied by le heuc et al . 
the failed recognition is explained by the need for capsule distension ( achievable with intra - articular contrast agent injection ) that makes possible a better visualisation of all the anatomical structures . 
it is , in fact , radiol med ( 2013 ) 118 : 10221033 1031 important to underline that shoulder conditions causing superior instability rarely occur in isolation , as suggested in our study , and that a baseline examination alone would result in incomplete surgical repair [ 17 , 21 , 22 ]  . accurate diagnosis of these anomalies can further aid the surgeon [ 23 ] , as there is evidence that rotator interval lesions , with or without biceps tendon damage , not repaired during rotator cuff arthroscopy may cause persisting pain after surgery [ 17 , 2426 ]  . the impact of accurate imaging investigation on the diagnosis of glenohumeral instability is highly important ; the results of mr imaging can guide the surgeon towards arthroscopic or open treatment for recurrent instability [ 8 , 10 , 12 , 27 ]  . mr images without intra - articular contrast are usually adequate for the investigation of rotator cuff abnormalities . 
 however , for evaluating glenohumeral instability , an mr arthrography with the intra - articular injection of gadolinium with diethylenetriamine - pentaacetic acid ( gd - dpta ) can ensure joint distension and therefore a comprehensive visualisation of all major anatomical structures as well as subtle labral abnormalities , thereby heightening diagnostic accuracy [ 10 , 2830 ]  . 
intra - articular contrast has been shown to be particularly useful for differentiating slap lesions and anatomical variants such as sublabral recess and foramen [ 5 ]  . in his study , magee et al . 
conventional mr sensitivity and specicity compared with arthroscopy were as follows : anterior labral tear , 83% sensitivity and 100% specicity ; slap tear 84% and 100% , supraspinatus tendon tear 92% and 100% . 
at mr arthrography , sensitivity and specicity compared with arthroscopy changed as follows : anterior labral tear , 98% sensitivity and 100% specicity ; slap tear 98% and 99% , supraspinatus tendon tear 100% and 100% [ 31 ]  . 
several studies have conrmed the value of mr arthrography in detecting slap lesions , reporting sensitivity ranging from 82% to 100% , specicity between 71% and 98% and accuracy between 83% and 94% [ 5 , 3235 ]  . 
 [ 29 ] , reported a sensitivity of mr arthrography in recognising slap lesions of 92% in 25 patients ; in our study , the sensitivity , specicity , accuracy , ppv and npv in the detection of slap lesions were 100% ; in the evaluation of the real type of slap lesions , the sensitivity was 90.3% , specicity was 78.5% , accuracy was 92.8% , ppv was 71.7% and npv was 100% . 
 low - grade slap lesions ( type i and ii ) are more difscopia per patologia della cufa dei rotatori , possono essere causa della persistenza della sintomatologia dolorosa dopo chirurgia [ 17 , 2426 ]  . limpatto di accurate indagini di imaging nella diagnosi dellinstabilit gleno - omerale di fondamentale importanza , i risultati della rm possono indirizzare il chirurgo verso il trattamento artroscopico o quello aperto in caso di instabilit recidivante [ 8 , 10 , 12 , 27 ]  . 
la rm senza mdc solitamente utilizzata nella diagnosi di lesioni della cufa dei rotatori e nellimpingement acromion - omerale , mentre nella valutazione dellinstabilit gleno - omerale lesame rm dopo somministrazione intra - articolare di gadolinio con acido dietilenetriamine - pentaacetico ( gd - dtpa ) assicura ladeguata distensione articolare che consente un ottimo dettaglio anatomico e quindi potenzia il valore diagnostico della metodica [ 10 , 2830 ]  . 
i valori di sensibilit e specicit della rm convenzionale sono stati i seguenti : per le lesioni del cercine glenoideo anteriore 83% di sensibilit e 100% di specicit ; per le slap lesions rispettivamente 85% e 100% ; per le lesioni del tendine del sovra spinato rispettivamente 92% e 100% . 
con lartro - rm i valori di sensibilit e specicit comparati con lartroscopia sono risultati i seguenti : 98% e 100% per le lesioni del cercine anteriore , 98% e 99% per le slap lesions ; 100% sia di sensibilit che di specicit per le lesioni di cufa [ 31 ]  . 
i nostri risultati sulle slap lesions sono simili a quelli comparsi in letteratura , anche nella nostra serie la lesione pi frequente stata quella di tipo ii [ 3034 ]  . 
molti studi hanno confermato la validit dellartro - rm nellidenticazione delle slap lesions , riportando un range di sensibilit dall82% al 100% , di specicit tra il 71% e il 98% e di accuratezza tra l83% e il 94% [ 5 , 3235 ]  . 
 [ 29 ] hanno riportato una sensibilit dellartro - rm nella diagnosi di slap lesion del 92% in 25 pazienti , nel nostro studio sensibilit , specicit , accuratezza , vpp e vpn nella identicazione delle slap lesions stata dal 100% , mentre nella denizione del tipo di slap lesion la sensibilit stata del 90 , 3% , la specicit del 78 , 5% , laccuratezza del 92 , 8% , il vpp del 71 , 7% e il vpn del 100% . le slap lesions di basso grado ( tipo i e ii ) sono pi difcili da diagnosticare quando la distensione capsulare ottenuta dalliniezione del mdc non sufciente a dimostrare la profondit della lesione [ 31 , 32 ]  . 
recenti studi 1032 radiol med ( 2013 ) 118 : 10221033 cult to diagnose since the capsular distension obtained by the contrast agent injection may not be sufcient to demonstrate the depth of the lesion [ 31 , 32 ]  . 
recent studies have shown that the commonest cause of false positive results in suspected slap lesion is the inltration of contrast agent within the sublabral recess or sulcus , and sublabral foramen , as these anatomical variants can mimic a slap lesion [ 5 , 28 ]  . 
in our series , no case of anatomical variant was observed and therefore there were no differential diagnosis issues . in conclusion , clinical assessment of supra - equatorial shoulder instability is difcult and imaging plays a key role in the diagnosis . 
supra - equatorial instability is isolated in only a few cases , and more frequently different abnormalities are associated including labrocapsular abnormality , subequatorial labral disease , slap lesions , disorders of the rotator interval and long head of the biceps tendon or complex anatomical variants of the capsular ligaments . the role of mr arthrography is to describe the key features of the supra - equatorial labral lesion , including the location , morphology , and extent of the abnormality and associated injuries , and to correlate these features with the clinical symptoms . hanno dimostrato che la pi comune causa di falso positivo nei casi di sospetta slap lesions rappresentata dallinltrazione del mdc nel recesso o solco sublabrale o nei casi di foramen sublabrale , queste normali varianti anatomiche possono mimare una slap lesion [ 5 , 28 ]  . 
tamburrini , e - mail : tamburrini@unicz.it received : 13 july 2012 / accepted : 17 august 2012 / published online : 25 june 2013 springer - verlag 2013 abstract purpose . 
the aim of our study was to estimate the diagnostic accuracy of wholebody magnetic resonance imaging ( wb - mri ) and positron emission tomography / computed tomography ( pet / ct ) in mm patients studied before and after treatment . 
we considered 22 consecutive patients ( 10 males , 12 females ; age range , 4883 years ) with newly diagnosed mm ( ndmm group ) , and the same 22 patients underwent at least one re - assessment after treatment ( previously treated mm , ptmm group )  . 
la diagnostica per immagini svolge un ruolo centrale nella stadiazione , nella denizione prognostica oltre che nella pianicazione e nel monitoraggio della terapia in pazienti con mieloma multiplo ( mm )  . 
wb - rm e tc / pet sono state effettuate a breve distanza tra loro sia nel gruppo ndmm ( 22 esami ) che nel gruppo ptmm ( 29 esami )  . 
accounting for 1% of all malignancies and 10%15% of haematopoietic disorders , it is rare before the 5th decade of life ( the mean age of affected patients is 6070 years )  . 
the disease is histopathologically characterised by the inltration or replacement of the normal cellular components of bone marrow by myeloma cells producing osteoclastic - activating factor ( oaf )  . 
most often death occurs as a result of bacterial infection , renal failure and thromboembolisthe diagnosis of mm relies on clinical , laboratory and imaging ndings : diagnostic imaging plays a crucial role in staging the extent , severity and progression of disease , as well as in planning treatment and assessing its effects . available imaging modalities are conventional radiology , nuclear medicine , multidetector computed tomography ( mdct ) and whole - body magnetic resonance imaging ( wb - mri ) [ 47 ]  . conventional radiology remains useful despite its limitations : in 30% to 70% of cases it fails to detect any focal abnormality and a nding of diffuse osteoporosis may be impossible to distinguish from osteoporosis from other causes . 
 in practice , the radiographic skeletal survey has low sensitivity , especially in the study of some skeletal districts ( ribs , scapulae , sternum ) [ 5 ]  . 
the classic appearance of the basic lesion is single or multiple punched - out lytic lesions with well - dened nonsclerotic margins and variable diameter . nuclear medicine with cellular [ methoxy isobutyl isonitrile ( mibi ) 99mtc - 67ga citrate ] and osteotropic [ 99mmethylene - diphosphonate ( mdp ) ] radiopharmaceuticals has a very limited role due to its low sensitivity , as the classic lesions are essentially the result of an osteoclastic process . 
 by contrast , positron emission tomography with computed tomography ( pet / ct ) has such an important role that it is currently included in the recent mm staging criteria , and has shown considerable value in the follow - up after chemo il mieloma multiplo ( mm ) una gammopatia monoclonale ad elettiva localizzazione nel midollo osseo , caratterizzata dalla proliferazione di un singolo clone di plasmacellule , in grado di produrre , nel 90% dei casi , elevate concentrazioni di unimmunoglobulina presente nel sangue , nelle urine , o in entrambe , con associate lesioni litiche dellosso . 
rappresenta l1% dei tumori maligni ed il 10%15% delle malattie del sistema ematopoietico ed rara prima della v decade di vita ( let media dei pazienti affetti di 6070 anni )  . 
questa malattia caratterizzata , dal punto di vista anatomopatologico , dallinltrazione o dalla sostituzione dei costituenti cellulari del midollo normale da parte di cellule mielomatose con produzione dellosteoclastic activating factor ( oaf ) con esaltazione dellattivit osteoclastica . 
la diagnosi di mm clinico - laboratoristicostrumentale : la diagnostica per immagini contribuisce in modo determinante alla stadiazione della patologia per denirne la diffusione , la gravit e levoluzione , ed utilizzata anche al ne di orientare la terapia e valutarne gli effetti . le metodiche di imaging disponibili sono la radiologia tradizionale , la medicina nucleare , la tomograa computerizzata multidetettore ( tcmd ) e la risonanza magnetica whole body ( wb - rm ) [ 47 ]  . la radiologia tradizionale , pur con i suoi limiti , mantiene tuttora una sua utilit : si segnala comunque che in una percentuale oscillante dal 30% al 70% dei casi non si rilevano alterazioni focali allesame radiologico e che laspetto osteoporotico diffuso pu non essere distinguibile dallosteoporosi di altra natura . 
laspetto classico della lesione elementare di osteolisi pura , a stampo , a margini netti non sclerotici , di diametro variabile , solitaria o multipla . la medicina nucleare con lutilizzo di radiofarmaci di cellularit [ metossi isobutil isonitrile ( 99mtc - mibi ) e 67gallio - citrato ] , ed osteotropi [ 99tc - metilen difosfonato ( mdp ) ] ha un ruolo molto limitato per la bassa sensibilit , poich le lesioni classiche sono determinate da un processo essenzialmente osteoclastico . 
al contrario la tc / tomograa ad emissione di positroni ( pet ) ha un ruolo importante 932 radiol med ( 2013 ) 118 : 930948 and / or radiotherapy [ 8 , 9 ]  . 
in addition to uoro - deoxy - glucose pet / ct , other radiotracers such as 11c - choline [ 10 , 11 ] and 11c - methionine [ 12 , 13 ] have been used experimentally in mm patients , showing a good level of accuracy for the diagnosis of both bone marrow and extramedullary involvement . 
that said , a role appears to be emerging for whole - body low - dose ct ( wb - ldct ) in the assessment of lytic lesions , such that in some centres it has come to replace the radiographic skeletal survey [ 14 ]  . 
mdct can be of assistance in guiding biopsy procedures . wb - mri , now a widely used technique not only in haemato - oncology [ 3 , 1517 ] , is pivotal to mm imaging , as it is able to demonstrate focal or diffuse , homogeneous or heterogeneous ( salt and pepper ) signal intensity changes with extremely high sensitivity , even though its specicity is limited : like pet / ct , wb - mri has also been included in the most recent staging criteria , as it correlates well with the clinical and laboratory data [ 1821 ]  . 
however , it should be noted that , in the case of low - grade ( < 20% ) bone marrow inltration , the mri ndings may be completely normal . 
 on the basis of these premises , we compared the diagnostic performance of wb - mri and pet / ct with the ndings of the bone marrow aspirate in mm patients , in order to dene the role of the two modalities at diagnosis and after treatment and establish whether they provide complementary or overlapping results . 
even though these modalities enable panoramic views and are highly sensitive , they are both associated with signicant costs , both economic and biological ( pet / ct ) , uneven availability and long examinations times . 
the patients in our study were staged by applying the durie and salmon plus staging system [ 20 ] : stage ia ( no lesion or single lesion on mri ) ; tanto da essere attualmente inserita nei pi recenti criteri di stadiazione del mm , mostrando inoltre notevole valore nel follow - up della malattia dopo chemioe / o radioterapia [ 8 , 9 ]  . 
oltre alla tc / pet con uor - deossiglucosio ( fdg ) , altri radiofarmaci quali la 11c - colina [ 10 , 11 ] e la 11c - metionina [ 12 , 13 ] sono stati impiegati sperimentalmente in pazienti con mm , dimostrando una buona accuratezza sia per la diagnosi dellinteressamento midollare che extra - midollare . 
 la tcmd in concreto non di impiego routinario nel mm , fatto salvo lo studio mirato di determinati distretti ( rachide , massiccio facciale ) : comunque , attualmente , appare emergente il ruolo della tcmd whole body a bassa dose ( wb - ldct ) nella valutazione delle lesioni litiche , tanto che in alcune istituzioni tende a sostituire lesame radiologico dello scheletro [ 14 ]  . 
comunque la tcmd pu essere di ausilio per prelievi bioptici . la rm con la tecnica wb , oggi ampiamente diffusa , e non solo in oncoematologia [ 3 , 1517 ] , rappresenta un cardine fondamentale nellimaging del mm , potendo documentare alterazioni di intensit di segnale focali o diffuse , omogenee o variegate con aspetto a sale e pepe con altissima sensibilit , seppure con contenuta specicit : anche la wb - rm come la tc / pet rientra nei pi attuali criteri di stadiazione , correlandosi bene con i dati clinico - laboratoristici [ 1821 ]  . 
va peraltro segnalato sin da ora che il reperto rm , in caso di inltrazione di basso grado ( < 20% ) del midollo osseo , pu apparire del tutto normale . 
 sulla base di queste considerazioni e per denire il ruolo della wb - rm e quello della tc / pet sia alla diagnosi che dopo la terapia e con lobiettivo di comprendere se le metodiche siano tra loro complementari o sovrapponibili , abbiamo confrontato le performance diagnostiche dellimaging con wb - rm e con tc / pet con i risultati dellaspirato midollare nei pazienti con mm . 
pur considerando che entrambe risultano panoramiche ed altamente sensibili , va segnalato che le stesse hanno signicativo costo , non solo in senso economico ma anche biologico ( tc / pet ) , non uniforme disponibilit e tempi desecuzione lunghi . materiali e metodi pazienti sono stati prospetticamente arruolati nel nostro studio tutti i pazienti con diagnosi di mieloma multiplo inviati al dipartimento di diagnostica per immagini a partire da luglio 2006 sino a marzo 2010 . 
 a total of 22 consecutive patients ( 10 males and 12 females ; age range , 4483 years ) with a diagnosis of mm were enrolled and staged in this way ; these patients were entered in the newly diagnosed mm group ( ndmm )  . 
this group of patients with previously treated mm ( ptmm ) underwent at least one whole - body imaging study after an interval of 2 months from the end of the last treatment cycle . 
 thus a total of 29 whole - body imaging studies ( wb - mri and pet / ct ) were carried out in the ptmm group underwent to establish response to treatment . table 1 shows the general characteristics of the patients enrolled in the ndmm and ptmm groups . 
 treatment response was dened in accordance with the criteria of the international myeloma working group ( imwg ) [ 2224 ] as complete response ( cr ) , near complete response ( ncr ) , very good partial response ( vgpr ) and partial response ( pr )  . 
for patients to be considered responders , the bone marrow aspirate or biopsy had to be negative stadiazione con il sistema durie e salmon plus ha inserito nei criteri di stadiazione anche la rm e la tc / pet . 
sulla base di questi criteri abbiamo arruolato 22 pazienti consecutivi ( 10 maschi e 12 femmine , di et compresa tra 4483 anni ) alla diagnosi ( gruppo ndmm )  . i medesimi pazienti sono stati successivamente seguiti nel tempo con imaging , dopo essere stati sottoposti a terapia ( gruppo ptmm ) per valutare lefcacia del trattamento . 
nel gruppo ptmm sono stati effettuati 29 esami di imaging whole body ( wb - rm e tc / pet ) , per denire lentit della risposta al trattamento . la tabella 1 mostra le caratteristiche generali dei pazienti arruolati sia nel gruppo ndmm che ptmm . 
all cases of bone marrow inltration greater than 5% were considered persistence of disease ( sd or dp )  . the study protocol was approved by our universitys ethics committee , and the study was performed in accordance with the helsinki guidelines . 
all patients were duly informed about the study and provided their formal consent to participate . assessment in all patients pet / ct and wb - mri were performed within 2 weeks from each other . 
for each patient we considered initial disease stage , myeloma type , and laboratory parameters ( serum and urine proteins , haemoglobin levels , 24 - hour urinary protein excretion , serum 2 - microglobulin , and urine protein electrophoresis )  . 
 whole - body morphological imaging with both pet / ct and wb - mri was always evaluated blinded to bone marrow cellularity and laboratory ndings ; the pet / ct studies were evaluated jointly by one radiologist and one nuclear physician . wb - mri examination technique all whole - body mr images were acquired using a 1.5 tesla scanner ( achieva , eindhoven , philips medical system , the netherlands ) equipped with a mobile table extender and an integrated q - body coil , with the lying patient supine in a feetrst position and with arms along the sides of the body . 
we acquired t1 - weighted short tau inversion recovery ( stir ) images for seven different body stations using the combination of the sliding patient support , table extender and image fusion ( mobyview software , philips medical system , best , the netherlands )  . 
 ( imwg ) [ 2224 ] : risposta completa ( cr ) , risposta quasi completa ( ncr ) , risposta parziale molto buona ( vgpr ) e risposta parziale ( pr )  . 
al contrario in tutte le altre condizioni in cui si dimostrata la presenza di malattia stazionaria ( sd ) o la progressione di malattia ( pd ) abbiamo classicato il paziente come non responsivo . 
in ogni caso la presenza di inltrazione midollare superiore al 5% stata considerata persistenza di malattia ( sd e pd )  . il protocollo stato approvato dal comitato etico della nostra universit . 
tutti i pazienti sono stati inoltre debitamente informati dello studio , fornendo un formale consenso di adesione . metodi in tutti i pazienti arruolati tc / pet e wb - rm sono state acquisite a breve distanza tra loro con un intervallo massimo di 2 settimane . 
per ogni paziente sono stati considerati lo stadio iniziale , il tipo di mieloma , e parametri laboratorio ( proteine seriche ed urinarie , livelli di emoglobina , escrezione proteica urinaria delle 24 ore , 2 - microglobulina sierica , ed i risultati del quadro proteico elettroforesico )  . 
 limaging morfologico wb , sia tc / pet che wb - rm stato valutato non conoscendo i risultati della cellularit midollare e dei dati di laboratorio , e per quanto riguarda la tc / pet , congiuntamente da un medico radiologo e da un medico nucleare . tecnica desame wb - rm tutte le immagini whole - body sono state acquisite usando uno scanner whole - body rm a 1 , 5 t ( achieva , eindhoven , philips medical system , olanda ) dotato di prolunga mobile del tavolo ed utilizzando una bobina di acquisizione q - body integrata , con paziente posizionato sul tavolo porta - paziente in posizione piede - testa , supino e con le braccia posizionate ai lati del corpo . 
sono state acquisite immagini t1 - pesate e short tau inversion recovery ( stir ) per sette differenti stazioni corporee dalla testa ai piedi usando la radiol med ( 2013 ) 118 : 930948 the images were rapidly re - aligned by means of dedicated software to facilitate instantaneous image review at the workstation . 
image interpretation was simplied by scrolling each single image at the workstation , and generally took 1015 minutes . pet / ct examination technique all patients underwent uor - deoxyglucose ( fdg ) - pet / ct performed with a discovery st8 hybrid scanner ( general electric , milwaukee wi , usa )  . 
 they received 370 mbq of 18f - fdg intravenously and after approximately 60 minutes a whole - body scan from head to toe was obtained using 9 to 12 consecutive elds of view . areas of heightened metabolism were analysed by manually drawing regions of interest ( roi ) over the brighter pixels . 
then the maximum standardised uptake value ( suvmax ) within the roi was calculated according to the following equation : suv = tissue concentration ( mbq / g ) / [ injected dose ( mbq ) / body weight ( g ) ] image analysis for each patient , the pattern of bone marrow inltration was analysed on both pet / ct and wb - mri . 
at mri we dened ve different patterns in agreement with baur - melnyk [ 19 ] : normal , focal inltration , multifocal inltration ( > 10 focal areas ) , diffuse inltration ( no areas of normal bone marrow ) and mixed inltration , where focal and diffuse aspects coexist . 
 similarly , at fdg - pet / ct we dened the following pet criteria : negative in the absence of areas of pathological uptake , positive for focal or multifocal lesions depending on number of foci detected ( > 10 focal areas was considered multifocal )  . 
the criteria for a positive pet nding were preliminarily dened as the presence of an area of focal uptake showing greater intensity than the surrounding tissue , regardless of its suv . 
a diffuse pattern at pet was instead dened as the nding of a diffuse increase in glucose metabolism as measured at the lumbar spine , and increased uptake at hepatic level . 
 in our experience , the ct component of the examination served to guide evaluation of the pet study by considering the following aspects : absence of focal lesions ; combinazione del tavolo porta - paziente in movimento , table extender e fusione delle immagini ( mobyview software , philips medical system , best , olanda )  . 
per ogni stazione corporea sono state acquisite 36 slices usando scansioni con la sincronizzazione del respiro per i distretti toracici ed addominali ( 18 slices / sincronizzazione del respiro )  . 
il tempo di scansione stato di circa 35 minuti incluso il posizionamento del paziente . le immagini sono state riallineate rapidamente usando software dedicati per facilitare la rivisitazione istantanea alla workstation . 
linterpretazione stata semplicata dallo scorrimento delle immagini singole alla workstation e generalmente avviene in uno spazio di tempo di circa 1015 minuti . tecnica desame tc / pet tutti i pazienti arruolati hanno effettuato la scansione tc / pet con fdg con uno scanner tomograco ibrido discovery st8 ( general electric , milwakee wi , usa )  . 
sono stati somministrati 370 mbq di 18f - fdg per via endovenosa e dopo circa 60 minuti stata effettuata una scansione whole body dal vertice ai piedi impiegando da 9 a 12 campi di vista consecutivi . le aree di incremento del metabolismo sono state analizzate denendo manualmente delle regioni di interesse ( roi ) sui pixel di maggiore intensit . 
successivamente stato calcolato il valore di uptake standardizzato ( suv ) massimo ( max ) allinterno della roi in accordo alla seguente equazione : suv = tissue concentration ( mbq / g ) / [ injected dose ( mbq ) / body weight ( g ) ] analisi delle immagini per ogni paziente stato analizzato il pattern di inltrazione midollare allimaging whole body sia tc / pet che rm . 
 alla rm abbiamo denito 5 differenti pattern di inltrazione midollare in accordo con quanto riportato da baur - melnyk [ 19 ] : normale , inltrazione focale , inltrazione multifocale ( > 10 aree focali ) , inltrazione diffusa ( assenza di aree di midollo normale ) e misto dove coesistono aspetti focali e diffusi . 
 in modo analogo allesame tc / pet con fdg sono stati deniti i seguenti criteri pet : negativo in assenza di aree di patologica ipercaptazione , positivo per lesioni focali o mul936 radiol med ( 2013 ) 118 : 930948 table 2 relation between disease stage and whole - body imaging patterns stage ( n ) pet pattern ( n ) mri pattern ( n ) stage ib ( 5 ) stage ii ( 10 ) stage iii ( 7 ) f ( 5 ) f ( 2 ) ; mf ( 8 ) mixed ( 3 ) ; negative ( 4 ) mixed ( 5 ) ; diffuse ( 2 ) f ( 5 ) mf ( 7 ) ; mixed ( 3 ) pet , positron emission tomography ; mri , magnetic resonance imaging ; f , focal ; mf , multifocal tabella 2 relazione tra stadio di malattia e pattern riscontrato allimaging wb stadio ( n ) pet pattern ( n ) rm pattern ( n ) stadio ib ( 5 ) stadio ii ( 10 ) stadio iii ( 7 ) misto ( 3 ) ; negativo ( 4 ) misto ( 5 ) ; diffuso ( 2 ) f ( 5 ) mf ( 7 ) ; misto ( 3 ) f ( 5 ) f ( 2 ) ; mf ( 8 ) pet , tomograa ad emissione di positroni ; rm , risonanza magnetica ; f , focale ; mf , multifocale lytic lesion ( s ) without sclerotic rim ; signs of diffuse osteopoenia ; ( possible ) fractures ; expansile bone lesions with cortical destruction and involvement of surrounding soft tissues . finally , the imaging studies were assessed for concordance or discordance with regard to number of lesions and disease pattern . 
of these , seven showed a focal pattern ( ve stage ib , two stage ii ) , eight a multifocal pattern ( stage ii ) , and three a mixed pattern ( stage iii )  . 
conversely , only 3 / 7 patients with stage iii disease exhibited pathological fdg uptake , characterised by a mixed pattern due to the coexistence of focal lesions and diffuse inltration ( suvmax range , 4.79.2 ) on both pet and ct . 
in the remaining four patients with ndmm stage iii , pet failed to show focal areas of intifocale in funzione del numero di focalit riconoscibili ( 10 aree focali multifocale )  . 
i criteri di positivit in pet sono stati preventivamente deniti come la presenza di unarea di captazione focale di intensit maggiore rispetto al tessuto circostante , indipendentemente dal valore di suv . 
 la coesistenza di pattern diffuso e focale stata denita pattern misto , analogamente a quanto stabilito per la rm . nella nostra esperienza , la componente tc servita come guida per la valutazione del reperto pet e gli aspetti considerati sono stati di : assenza di lesioni focali ; lesione / i litica / che senza orletto sclerotico ; segni di osteopenia diffusa ; ( eventuali ) fratture ; lesioni ossee espansive con distruzione corticale e impegno dei tessuti molli circostanti . inne gli esami di imaging sono stato giudicati in accordo o in disaccordo per numero di lesioni e per il loro pattern di malattia . 
i criteri di analisi delle immagini sono stati applicati sia nelle acquisizioni alla diagnosi e che in quelle dopo trattamento . risultati whole body imaging in ndmm la tc / pet con fdg risultata positiva in 18 / 22 pazienti ndmm . 
in questa metodica stato riscontrato nei 18 / 22 pazienti positivi , un pattern focale in 7 ( 5 stadio ib , 2 stadio ii ) , multifocale in 8 ( stadio ii ) , misto in 3 ( stadio iii )  . 
nei 5 pazienti con stadio ib stata evidenziata dalla pet alme no una lesione avida di fdg con range di suvmax compreso tra 2 , 48 , 7 e con aspetto tc di lesione litica . 
in tutti i 10 pazienti con stadio ii sono state correttamente evidenziate multiple aree di intensa ipercaptazione focale del radiofarmaco ( suvmax 4 , 313 , 1 ) corrisponden ti ad alterazioni litiche alla tc . 
al contrario solo in 3 dei 7 pazienti con stadio iii si segnalava la presenza di patologica captazione di fdg mostrando un pattern di tipo misto per la coesistenza di lesioni focali ed inltrazione diffusa ( range di suvmax 4 , 79 , 2 ) sia in pet che in tc . 
nei restanti 4 pazienti affetti da ndmm in stadio iii , la pet non mostrava aree focali di ipercaptazione sebbene laspirato midollare evidenziasse uninvasione plasmacellulare superiore al 40% , con reperto tc di osteopenia diffusa . 
sulla base di tale reperto abbiamo considerato questi pazienti pet negativi . in tutti i 22 pazienti la wb - rm risultata positiva , moradiol med ( 2013 ) 118 : 930948 fig . 
1a - d coronal wb - mri ( a , b ) : t1 - weighted sequence shows diffuse hypointensity of the bone marrow ; stir sequence shows marked and diffuse high signal intensity due to diffuse bone marrow inltration in a patient with > 60% plasma cells on bone marrow biopsy . 
on the basis of this nding , we considered these patients to be pet - negative . wb - mri was positive in all 22 patients , showing abnormal bone marrow signal due to focal , diffuse or mixed inltration , consistent with the results of the bone marrow aspirate . 
a mixed pattern was seen in eight patients ( three in stage ii and ve in stage iii ) , whereas a diffuse pattern was seen in two cases ( both stage iii )  . 
considering pattern as a function of the extent of bone marrow inltration , there was concordance between the pet and mri pattern in ve ( four focal and one multifocal ) out of six patients with 20% inltration , and discordance in one case . 
in termini di pattern , la rm ha evidenziato un pattern focale in 5 pazienti , tutti con stadio ib , di tipo multifocale in 7 , tutti in stadio ii . 
il pattern misto era presente in 8 ( 3 in stadio ii e 5 in stadio iii ) , mentre quello diffuso in 2 casi , tutti in stadio iii . 
la correlazione tra stadio di malattia e pattern dellimaging riportata in tabella 2 . limaging wb risultato concordante fra tc / pet e rm in 18 dei 22 pazienti con ndmm , in termini di presenza di malattia , ma discordante per pattern in 5 / 18 . 
in funzione dellinltrazione plasmacellulare abbiamo inoltre riscontrato in 6 pazienti con inltrato 20% , un pattern pet ed rm concordante in 5 casi ( di tipo focale in 4 e multifocale in uno ) , discordante in un caso . 
nel gruppo di 11 pazienti con inltrazione midollare compresa tra 20%40% , i pattern risultavano concordanti in solo 7 casi ( malattia mf in 4 , mista 2 , focale in 1 )  . 
bar graph of the distribution of the different patterns recorded at wb - mri ( a ) and pet ( b ) as a function of the extent of plasma cell inltration in the group of patients with ndmm ( newly diagnosed multiple myeloma )  . 
2a , b graco a barre della distribuzione dei diversi pattern riscontrati alla wb - rm ( a ) ed alla pet ( b ) in funzione dellinltrazione plasma - cellulare nel gruppo di pazienti ndmm . 
 938 the group of 11 patients with 20%40% bone marrow inltration , the patterns were concordant in seven cases only ( multifocal in four , mixed in two , focal in one )  . 
four of the ve patients with > 40% inltration showed no areas of increased radiotracer uptake on pet with signs of diffuse osteopoenia on ct , whereas one case showed positive pet / ct with mixed pattern . 
nel gruppo di 5 pazienti con inltrazione > 40% abbiamo inne riscontrato assenza di aree di ipercaptazione in pet con segni tc di osteopenia diffusa in 4 casi , mentre in 1 caso la pet / tc era positiva con un pattern misto . 
the overall results of imaging in the patients with ndmm are reported in table 3 . whole - body imaging in ptmm the same 22 patients ( examinations 122 in table 4 ) were followed up during the course of the disease , after at least one complete chemotherapy cycle or after autologous bone marrow transplantation . 
because seven patients ( patients 2 , 4 , 5 , 11 , 13 , 17 , 20 corresponding to examinations 2329 in table 4 ) underwent a second whole - body assessment at a later date , a total of 29 examinations were performed to evaluate the patients response to treatment . 
in 7 pazienti riportati consecutivamente in tabella 4 ( pazienti 2 , 4 , 5 , 11 , 13 , 17 , 20 corrispondenti ad esami 2329 in tabella 4 ) , una rivalutazione con imaging whole body stata ripetuta anche in una ulteriore occasione . 
le caratteristiche dei pazienti arruolati al momento della rivalutazione ed i risultati dellimaging sono riportate in tabella 4 . venti / 29 esami sono stati effettuati in pazienti considerati come responsivi al trattamento ( 7 con cr , 4 con ncr , 2 con vgpr , 7 con pr ) in base ai risultati dellaspirato midollare e dei parametri di laboratorio . 
in 16 di 20 con risposta al trattamento , la tc / pet mostrava la persistenza delle alterazioni strutturali gi segnalate allesordio dalla tc , in assenza di una corrispondente ipercaptazione di fdg . 
 by contrast , wb - mri was negative in only 12 / 20 responders ; in the eight cases of positive wb - mri , the pattern was diffuse in six patients , multifocal in one and focal in one . 
 likewise , four responders were positive at pet / ct , with focal pattern in two cases and diffuse pattern in two , and evidence of lytic lesions at ct . 
in two la wb - rm risultata negativa solo in 12 dei 20 responder ; in questi 8 casi con wb - rm positiva , stato osservato un pattern diffuso in 6 , multifocale e focale in 1 paziente . 
in the seven true positive cases with progressive disease pet / ct showed a multifocal ( n = 4 ) or mixed ( n = 2 ) pattern , and a focal pattern in one case only . 
of the six discordant cases , two were due to false negative pet results in nonresponders , who showed a focal or diffuse pattern on wb - mri consistent with the laboratory and aspirate ndings ; four were due to false positive mri results in responders with negative pet ndings consistent with the laboratory ndings . 
in particular , in the latter four patients , wb - mri showed a diffuse pattern in three cases and a multifocal pattern in one , which after 6 months showed a substantial reduction in bone marrow cellularity ( table 5 )  . 
the available modalities are the radiographic skeletal survey , low - dose mdct , wb - mri and pet / ct [ 2 , 46 , 14 , 2528 ]  . 
clearly , an investigation is considered useful when its result negative or positive affects patient management . mm accounts for approximately 10% of all haematological malignancies , and signicant progress has recently been made in the diagnosis , staging and treatment of this disease . 
 because mm is a diffuse process a wide eld of view is indispensable [ 29 ] for the simultaneous assessment of bone marrow and possible extraosseous foci , reported in 10% za in 23 / 29 in termini di capacit di riconoscere la persistenza o meno di malattia . 
dei 6 pazienti discordanti , 4 erano dovuti ad una falsa positivit rm in pazienti responder , mente in 2 casi alla falsa negativit della pet in pazienti non responder , che mostravano alla wb - rm pattern focale o diffuso in accordo con quanto evidenziato dai dati laboratorio e dallaspirato midollare . 
negli altri 4 casi discordanti , nel gruppo responder era legato alla presenza di positivit rm e negativit pet ; questo ultimo dato era in accordo con quanto segnalato dagli esami di laboratorio . 
in particolare in questi 4 pazienti la wb - rm mostrava un pattern diffuso [ 3 ] e multifocale in un caso , che ripetuto a 6 mesi mostrava una netta riduzione della cellularit midollare . discussione limaging diagnostico svolge un ruolo fondamentale nel management del mm , tanto alla diagnosi che nella valutazione durante e dopo la terapia . 
le metodiche disponibili sono lesame radiologico sistemico dello scheletro , la tcmd a bassa dose , la wb - rm e la tc / pet [ 2 , 46 , 14 , 2528 ]  . 
certo che unindagine viene considerata utile allorch il suo risultato , negativo o positivo che sia , inuenza il management del paziente . il mm rappresenta circa il 10% delle malattie oncoematologiche e , negli ultimi anni , signicativi progressi sono stati compiuti nella diagnosi , nella stadiazione e nel trattamento di questa entit . 
essendo la malattia un processo diffuso indispensabile un ampio fov [ 29 ] per la simultanea valutazione del midollo osseo e di eventuali foci extraossei , riportati , secondo alcuni autori , nel 10%16% dei pazienti con mieloma multiplo [ 30 , 31 ]  . 
extraosseous localisations may be present in especially aggressive forms of mm characterised by a very poor prognosis . even considering that the radiographic skeletal survey remains the rst - line staging modality in several centres and acknowledging that it suffers limitations [ 18 ] to the point that there is a tendency to replace it with low - dose mdct there is an emerging role for wb - mri and pet / ct in the staging and follow - up of mm patients [ 19 , 20 , 25 , 27 ]  . 
these modalities have in fact been incorporated into the more recent durie and salmon plus staging system , whereas the radiographic skeletal survey is part of the classic durie - salmon systeit should , however , be noted that the comparison between the two staging systems is still the subject of debate as the inclusion of the appendicular skeleton in the durie - salmon plus system may lead to overstaging , with an impact of treatment and prognosis [ 32 ]  . the recent guidelines of the international myeloma working group [ 3335 ] underline the importance of accurate whole - body imaging of these patients . 
some authors recommend the use of wb - mri in patients with suspected mm but no bone lesion on radiography and in those with apparent solitary plasmacytoma [ 27 ] and do not recommend the routine use of pet / ct . 
however , the use of pet / ct for disease staging has been shown to provide complementary information to wb - mri [ 8 , 9 , 28 , 36 , 37 ]  . 
in addition , low - dose ct is believed [ 14 ] to have extensive potential for use , with a signicant increase in sensitivity and reduction in radiation dose . the combined use of the two modalities , according to the literature , does not yield false positive results , achieving a specicity and positive predictive value of 100% [ 15 , 38 ]  . 
contrast agents ( whole - body dynamic contrast - enhanced mri ) are not routinely used in these patients for a number of reasons , including the fact that lesions undergoing treatment have an extremely variable appearance and the examinations times are signicantly longer . 
despite these problems some authors [ 4143 ] have proposed the use of contrast - enhanced imaging to monitor response to treatment . according to recently published studies , diffusionweighted sequences ( diffusion - weighted imaging with background suppression , dwibs ) [ 4449 ] appear to signicantly increase the value of mri not only in staging ni extraossee possono essere presenti in forme mielomatose particolarmente aggressive , caratterizzate da una prognosi molto severa . pur considerando che lesame radiologico dello scheletro in alcune istituzioni resta tuttora la prima indagine ai ni della stadiazione e ribadendo i limiti dello stesso [ 18 ] , tanto che , come gi detto , la tcmd a bassa dose tende a sostituirlo , appare emergente limpiego della wb - rm e della tc / pet nella stadiazione e nel follow - up di questi pazienti [ 19 , 20 , 25 , 27 ]  . 
va peraltro sottolineato che il confronto tra i due sistemi di stadiazione rappresenta tuttora motivo di dibattito poich linclusione dello scheletro appendicolare nel sistema durie e salmon plus pu causare una sovra - stadiazione della malattia , inuenzando il trattamento e la prognosi [ 32 ]  . le recenti linee guida dellinternational myeloma working group [ 3335 ] sottolineano limportanza della accurata valutazione total body di questi pazienti . 
alcuni autori consigliano limpiego della wb - rm nei pazienti con sospetto mm ma con esame sistemico dello scheletro negativo per lesioni ossee e nei pazienti con apparente plasmocitoma solitario [ 27 ] e non raccomandano limpiego routinario della tc / pet . 
nella stadiazione , comunque secondo altri autori la tc / pet pu fornire informazioni complementari alla wb - rm [ 8 , 9 , 28 , 36 , 37 ]  . 
va peraltro segnalato che la tc / pet a bassa dose presenta , secondo alcuni autori [ 14 ] , ampie prospettive di impiego con signicativo aumento della sensibilit e riduzione della dose radiante . lutilizzo combinato delle due metodiche , dai dati della letteratura , non fornisce falsi positivi con una specicit ed un valore predittivo positivo ( ppv ) pari al 100% [ 15 , 38 ]  . 
limpiego in questi pazienti di agenti di contrasto ( whole - body dynamic contrast - enhanced rm ) non routinario per una serie di fattori tra cui si segnala che le lesioni in corso di trattamento hanno un aspetto estremamente variabile , con signicativo prolungamento del tempo di indagine . 
nonostante tali considerazioni alcuni autori [ 4143 ] ne propongono limpiego per monitorare la risposta al trattamento . da segnalare che le sequenze in diffusione ( dwibs ) [ 44 49 ] da recenti segnalazioni in letteratura paiono aumentare signicativamente il valore della rm non solo nello staging , ma anche nel follow - up dei pazienti con mm , avendo inoltre 944 radiol med ( 2013 ) 118 : 930948 fig . 
3a - h assessment before and six months after treatment ( velcade , thalidomide , dexamethasone ) of a patient with a focal mm lesion at t8 level , with obvious signs of pathological fracture and spinal canal involvement ( a , b ) on wb - mri . 
3a - h valutazione pree post - trattamento a sei mesi ( velcade , talidomide , desametasone ) in mm con lesione focale a carico di d8 , segni di frattura patologica con evidente impegno nello speco vertebrale ( a , b ) in wb - rm . 
nel controllo post - terapia , alla wb - rm ( e , f ) , netta riduzione nellimpegno dello speco e perivertebrale con persistenza di alterato segnale a carico del soma interessato ; in g e h ( tc / pet ) non evidenti aree di attivit , con persistenza dellalterazione strutturale litica . radiol med ( 2013 ) 118 : 930948 but also in the follow - up of mm patients , with a potential for monitoring the disease during treatment [ 50 ]  . 
however , despite the extremely encouraging results , the authors state that a larger study is required to dene the true clinical impact of diffusion - weighted imaging with calculation of the apparent diffusion coefcient [ 48 ]  . 
 for the purposes of planning treatment and predicting prognosis , the overall assessment of disease status does not rely solely on the results of diagnostic imaging ( clearly fundamental for both the diagnosis and the follow - up ) , but requires integration of imaging with the clinical and laboratory ndings . the intensive use of whole - body imaging in staging is currently mandatory in view of the fact that the number of lesions and consequently the disease stage will signicantly inuence the patients prognosis . 
in practice , the haemato - oncologist relies on imaging to help select those patients with a worse prognosis and greater risk of recurrence who will need close and constant disease monitoring , so as to be able to promptly address recurrences . 
in this respect , it is important to remember that mri and targeted biopsy are the only techniques capable of providing information about bone marrow cellularity in a specic skeletal district ; this fact explains some of the discrepancies between the presence of active focal areas and normal iliac crest aspirate . 
it should be considered that none of our patients had extramedullary lesions , which constitute a particularly favourable setting for pet imaging according to the literature [ 9 ]  . re - evaluation following treatment is an even more complex scenario owing to the co - existence of at least two factors : effects of treatment on the nonpathological osteomedullary compartment and on the transformed cells and their metabolisin our series , consistent with the literature [ 5 , 7 , 16 ] we noted that bone marrow cellularity , as assessed by mri , showed changes related to the administration of bone marrow growth factors , leading to a near - physiological hypercellularity which should be borne in mind when reevaluating disease status in patients affected by mm . 
similarly , we found that with regard to the imwg criteria for treatment response , pet / ct was positive with active focal lesions in two patients classied as responders . 
comunque , per quanto i risultati siano estremamente incoraggianti , viene suggerita una esperienza pi ampia per denire il reale impatto clinico delle sequenza in diffusione con il calcolo del coefciente di diffusione apparente ( adc ) [ 48 ]  . 
 la valutazione complessiva dello stato di malattia , al ne della pianicazione terapeutica e della prognosi , non si fonda esclusivamente sui risultati dellimaging diagnostico , peraltro fondamentale tanto allesordio che nel follow - up , ma dalla sintesi di questi con i dati clinici e laboratoristici . al momento si impone nella stadiazione un uso intensivo dellimaging whole body , in considerazione del fatto che il numero di lesioni e quindi lo stadio della malattia , inuenza signicativamente la prognosi del paziente . 
dal punto di vista pratico lonco - ematologo chiede allimaging , di selezionare quei pazienti a prognosi pi sfavorevole e con un maggiore rischio di recidiva , che richiederanno una pronta e continua valutazione dello stato di malattia , per poter trattare in modo tempestivo la recidiva . 
a tal ne opportuno ricordare che lrm e la biopsia mirata sono le sole metodiche in grado di fornire informazioni circa la cellularit midollare in un specico distretto scheletrico ; tale considerazione spiega talora le discrepanze tra presenza di aree focali attive ed aspirato midollare da cresta iliaca siologico . 
nella nostra casistica , per quanto limitata , la tc - pet ha dato informazioni integrative , spesso grazie allausilio della componente tc dellesame , senza tuttavia modicare la stadiazione del paziente . 
opportuno considerare che in nessuno dei nostri pazienti stata riscontrata la presenza di lesioni extramidollari , che rappresentano un contesto favorevole alla pet da quanto emerge dalla letteratura [ 9 ]  . la rivalutazione dopo trattamento invece uno scenario ancor pi complesso per la coesistenza di almeno due fattori : gli effetti della terapia sul compartimento osteo - midollare non patologico e gli effetti sulle cellule trasformate e sul loro metabolismo . 
nella nostra casistica abbiamo notato , come confermato dalla letteratura [ 5 , 7 , 16 ] , che la cellularit midollare valutata in rm subisce delle variazioni legate soprattutto allassunzione di fattori di crescita e di stimolazione del midollo , inducendo una parasiologica ipercellularit , aspetto questo da tenere in considerazione nella rivalutazione dello stato di malattia in pazienti affetti da mieloma . 
allo stesso modo abbiamo riscontrato che in relazione ai criteri imwg di risposta al trattamento , la tc / pet risultava positiva con lesioni focali attive in 2 pazienti classicati come responder . 
in uno di questi pazienti abbiamo ri946 radiol med ( 2013 ) 118 : 930948 patients was found to have disease recurrence at the site of the pet / ct abnormalities . 
this anecdotal nding prompts some considerations regarding the absolute value of the response criteria and the effects of treatment on the relationship between viable , metabolically active cells and lesion volume , as a potential confounding factor . 
questo dato aneddotico apre lo spazio per alcune considerazioni sul valore assoluto dei criteri di risposta e sugli effetti del trattamento sul rapporto tra cellule vitali , metabolicamente attive e volume della lesione , quale potenziale fattore confondente . 
 conclusions conclusioni with regard to the simultaneous or sequential use of the two examinations it is clear that an extensive routine use of wbmri and pet / ct at diagnosis and after treatment cannot be considered feasible in all patients affected by mm . 
in the previously - treated setting , in particular in aggressive forms with a poor prognosis , a combined use of the two modalities should be preferred if compatible with the local organisational setup or , alternatively , pet / ct should only be used in cases of discrepancy between the laboratory and mri ndings . circa la contemporaneit e la sequenzialit delle metodiche chiaro che un impiego estensivo e routinario di wb - rm e tc / pet in tutti pazienti con mieloma , alla diagnosi e dopo trattamento , non appare praticabile . 
nel primo caso ragionevole ritenere la wb - rm metodica di primaria importanza , rimandando alla tc / pet i casi di mielomi microo non secernenti , e con localizzazioni extra - midollari . 
 nel contesto post - trattamento , specie per forme aggressive ed a prognosi sfavorevole , auspicabile limpiego combinato delle metodiche wb - rm e tc / pet dove possibile in funzione dello scenario organizzativo in cui si opera , o in alternativa eseguire la tc / pet solo in caso di discrepanza tra laboratorio ed imaging rm . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
a case - based atlas springer new york dordrecht heidelberg london , 2011 isbn : 978 - 1 - 4419 - 0430 - 0 ( hardcover ) e - isbn : 978 - 1 - 4419 - 0431 - 7 isbn : 978 - 1 - 4614 - 0949 - 6 ( softcover ) published online : 25 july 2013 springer - verlag 2013 this book , in its 151 page case - based layout , is intended to present the reader with an overview of possible results in the eld of coronary artery ct angiography ( ccta )  . one will nd six sections : coronary anatomy ; congenital coronary and other anomalies ; coronary artery disease ; percutaneous coronary intervention ; postsurgical revascularization ; and extracoronary abnormalities . sections open with an introduction , followed by interesting case presentations ( history ; ndings ; diagnosis ; discussion ; pearls of wisdom and pitfalls ) and close with a list of suggested readings ( noteworthy are citations of papers published in la radiologia medica )  . each case shows how a ccta examination has to be reviewed and studied at the workstation by the use of source images , multiplanar reformat , curved multiplanar , maximum intensity projection , 3d volume rendered , visual analysis and virtual endoscopy images ( sometimes followed by the related coronary angiography ) , in order to reach the correct diagnosis or suggest to the angiographist the need for an invasive procedure . images are of the highest quality , easily understandable , but , in a few cases missing proper arrow size . this is an atlas which will be much appreciated by radiologists , cardiologists and cardiac surgeons as well as by trainees starting work and study in this eld . 
 questo volume , impostato nelle sue 151 pagine come presentazione di casi , ha lo scopo di offrire al lettore una disanima di quanto ottenibile nel campo dellangio - tc delle arterie coronarie ( ccta )  . vi si troveranno sei sezioni : anatomia coronarica ; anomalie congenite delle coronarie e non solo ; malattie delle arterie coronarie ; interventi percutanei ; rivascolarizzazione post - chirurgica ; anomalie extracoronariche . ogni sezione si apre con una introduzione seguita da una presentazione ( storia clinica ; reperti ; diagnosi ; discussione ; spunti di saggezza e insidie ) di casi clinici di interesse e si chiude con un elenco di letture suggerite ( notevoli le citazioni di lavori pubblicati su la radiologia medica )  . ciascun caso dimostra come ogni esame di ccta debba essere rivisto e studiato alla consolle impiegando le immagini di origine , quelle di riformattazione multiplanare e curva , di proiezione di massima intensit , di volume 3d , nonch di analisi visiva e di endoscopia virtuale ( cui fa seguito , talvolta , la relativa angiograa coronarica ) , in modo tale da porre una diagnosi corretta o suggerire allangiograsta la necessit di una procedura invasiva . 
morphological measurements of residual renal function , such as renal length ( p = 0.004 ) , renal width ( p = 0.004 ) , renal thickness ( p = 0.008 ) , and renal size ( p = 0.004 ) were signicantly higher in nonanuric than anuric patients . 
 riassunto obiettivo questo studio ha valutato se una corticale renale sottile oppure qualsiasi misurazione morfologica del rene possano essere predittivi di funzionalit renale dopo nefrostomia percutanea ( pcn ) , riducendo , in questo modo , la necessit di tale procedura . materiali e metodi tutti i pazienti sono stati sottoposti a pcn unilaterale eseguita sotto guida ecograca e uoroscopica . 
successivamente sono state eseguite misurazioni morfologiche del rene per valutare la funzionalit renale residua ; una corticale renale sottile stata denita alla tomograa computerizzata ( ct ) mostrando uno spessore corticale < 10 mla produzione di urina stata misurata giornalmente e i pazienti sono stati suddivisi in due gruppi : anurici e non anurici . 
 risultati misurazioni morfologiche della funzionalit renale residua , quali lunghezza renale ( p = 0 , 004 ) , larghezza renale ( p = 0 , 004 ) , spessore renale ( p = 0 , 008 ) e dimensione renale ( p = 0 , 004 ) sono risultate signicativamente pi elevate nei pazienti non anurici rispetto ai pazienti anurici . 
la produzione di urina risultata aumentata di 85 , 47 ml / die per ogni millimetro di incremento della larghezza renale ( p = 0 , 026 ) e di 65 , 31 ml / die per ogni millimetro di incremento dello spessore renale ( p = 0 , 024 )  . 
le analisi di regressione lineare semplice hanno mostrato che i malati di cancro hanno una 910 radiol med ( 2013 ) 118 : 909916 keywords percutaneous nephrostomy renal cortex urine output kidney produzione di urina signicativamente pi bassa ( 358 , 73 ml / die , p = 0 , 046 ) rispetto ai pazienti sani . conclusioni questo studio ha mostrato che la produzione di urina e altri dati clinici possono fornire un indice per valutare la funzionalit renale residua prima di decidere sulla esecuzione di procedure di pcn . parole chiave nefrostomia percutanea corticale renale produzione di urina rene to december 2009 . 
in this group , 49 procedures had concomitant computed tomography ( ct ) images performed within one month of the pcn procedure and a renal cortex thickness that measured less than 10 mm on ct scans . 
 our institute approved the study protocol and all patients gave informed consent for use of their medical records individuals were assessed by multiple clinical characteristics including age , gender , emergent haemodialysis ( + / - ) , urinary tract infection ( + / - ) , indication for pcn ( for infection or obstruction ) , renal length , renal width ( anterior - posterior ) , renal width ( left - right ) , renal cortex thickness on ct scan , kidney volume ( length * width [ anteriorposterior ] * width [ left - right ] ) , pre - pcn and post - pcn serum estimated glomerular ltration rate ( egfr ) , and average daily urine output from pcn . inclusion and exclusion criteria all patients underwent unilateral pcn . 
there also may be noninvasive indicators which can help to avoid pcn altogether . previous studies have used magnetic resonance imaging ( mri ) [ 1 ] or radionuclide renography [ 911 ] to estimate the residual renal function . 
the most common indication for pcn is to recover the function of the obstructed kidney ; however , other indications for the procedure include infection control , urine diversion , and access for urolithiasis [ 16 ]  . the function of kidneys with a thin cortex has not been well investigated . 
 materials and methods study design this was a retrospective review of medical records from 42 patients covering a four - year period from january 2006 all pcn procedures were performed under both sonographic and uoroscopic guidance , either by a staff radiologist or by a radiology resident under direct supervision of a staff radiol med ( 2013 ) 118 : 909916 radiologist . 
 clinical physicians followed up the drainage tube function at the patient bedside ; the drainage tubes were replaced or removed if obstructed . urine output urine output from the nephrostomy tube was recorded daily . 
the urine output amount on the procedure day was excluded , since it was assumed to be residual urine from the obstructed collecting system rather than true daily urine output from the drained kidney . 
anuria of the drained kidney was dened as < 100 ml / day urine output from pcn [ 13 ]  . measuring renal size by ct concomitant ct images within one month of pcn were subsequently reviewed . 
for the reconstructed axial and coronal images , we used both a 5 mm slice thickness and a 5 mm interval . renal thickness was measured at the kidney midpoint on axial images . 
if more than one dilated renal calyx was visible in the same kidney midpoint axial image , the measurements from the renal capsule to each of the dilated calyces were then averaged . 
simple and multiple linear regression analyses were performed to evaluate whether the renal size was an independent inuence on urine output , and summarised by the weight coefcient ( ) using a 95% condence interval ( ci )  . 
in order to present the differences between the two groups divided by urine output , the continuous and categorical data were presented using a median with inter - quartile range ( iqr ) and respective percentages . 
a receiver operating characteristic ( roc ) analysis was performed to detect the size of nonfunctional obstructed kidneys , and the area under the curve was formulated to determine the accuracy of the kidney size . 
all statistical assessments were two sided and evaluated at the 0.05 level of signicance using spss 15.0 statistical software ( spss inc , chicago , il , usa )  . results general characteristics the study cohort included 42 patients . 
in the 42 patients , 16 ( 38.1% ) were diagnosed with urinary tract infections ( uti ) , 17 ( 40.5% ) had a diagnosis of renal stones , 15 ( 35.7% ) had cancer , and 8 ( 19% ) underwent chronic haemodialysis . 
with a controlling for pre - pcn creatinine , the urine output increased 66.02 ml / day for every millimetre increase in renal thickness ( p = 0.025 ) ( table 2 )  . 
1 correlazione tra dimensioni renali , spessore della corticale renale , e produzione di urina . gfr was not measured adequately in our study , a true comparison of this parameter was therefore limited . 
in 1999 [ 15 ] concluded that factors such as duration of obstruction and the functionality of the contralateral kidney play roles in determining renal recoverability , believing nonsurgical management or nephrectomy may be preferable with irreversible kidney function damage . 
upon performing pcn procedures , we found the increased level of urine output to be a good indicator for improved kidney function . our study aimed to prevent unnecessary pcn procedures ; proper patient assessment can greatly assist the role of pcn for treating obstructed kidney diseases and improving post - procedure renal function . 
 [ 17 ] also documented a correlation between careful pre - procedure patient assessment and procedure outcomes . some disagreement remains regarding which pre - procedure parameters determine optimal patient management post - pcn . 
in 1999 [ 15 ] and 2002 [ 18 ] found that younger patient age , smaller duration of obstruction , improved contralateral kidney function , and decreased pyelolymphatic backow increased renal function more than those individuals not possessing those characteristics . 
other studies have shown that greater cortical thickness and improved gfr correlate with stronger renal function [ 16 , 17 ] ; gender and diet may also be implicated in recovery of renal function [ 17 ]  . 
while it would appear that healthier individuals had a greater chance for improvement from obstructive kidney disease , our study showed no clinical differences between outcomes of anuric and nonanuric patient groups , in age , gender , or other clinical characteristics . 
the reasons for this remain uncertain , and may point to a role of diagnostic imaging to assess differences in patient outcomes . thus , our study focused on other parameters , such as renal measurements for assessing the role of pcn . 
dynamic contrast - enhanced mri , in comparison to nuclear studies , also provided equivalent information about renal function but superior information regarding morphology [ 10 , 23 ]  . 
 judging preserved renal function by using only renal length , width , thickness , and cortex thickness gives a relatively rough estimate , but is easy to perform compared to other invasive or non - invasive studies . 
these measurements may still serve as a quick pre - pcn estimation of preserved renal function , although they are less accurate . hence , pcn has continued to show its importance for assessing outcomes in the obstructed kidney , and remains a practical clinical method . 
in view of other inaccurate assessment methods , pcn was considered to be the most accurate predictive test available [ 5 , 6 , 24 ]  . our study focused on daily amount of nephrostomy urine output . 
noted that digital scintillation cameras and scintigrams of technetiumlabelled tubular agents such as 99mtc mercaptoacetyltriglycine ( mag3 ) provide functional assessment and even some anatomical information [ 19 ]  . 
these studies showed a positive correlation between renal morphology measurements and urine output which was similar to the results in our study . ultrasonography has been another noninvasive diagnostic imaging method for estimating renal function . 
in comparison to 916 radiol med ( 2013 ) 118 : 909916 conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
we emphasise the role of computed tomography and magnetic resonance imaging , which allow recognition of early alterations . keywords stress injuries stress fractures mr imaging computed tomography leg riassunto le lesioni da stress , la cui incidenza in aumento nella popolazione sportiva , in ambito sia competitivo che amatoriale , rappresentano una risposta patosiologica dellosso a modicazioni della normale stimolazione meccanica . 
in particolare , si enfatizza il ruolo dellimaging con tomograa computerizzata e con risonanza magnetica che permettono di riconoscere le alterazioni precoci . parole chiave lesioni da stress fratture da stress risonanza magnetica tomograa computerizzata gamba introduction introduzione the incidence of stress - related injuries is increasing among both competitive and amateur athletes [ 1 ]  . 
these injuries represent a response of the bone to changes in the normal mechanical environment : a continuum that spans from normal bone remodelling to accelerated remodelling with early damage up to frank fracture . in the human body , the bone most frequently affected by stress - related injury is the tibia ( 49.1% ) , followed by the tarsal bones ( 25.3% ) , metatarsals ( 8.8% ) , femur ( 7.2% ) , bula ( 6.6% ) , pelvic bones ( 1.6% ) , sesamoid bones ( 0.9% ) , and spine ( 0.6% ) [ 2 ]  . 
esse rappresentano una risposta dellosso a modicazioni della normale stimolazione meccanica : un continuum dal normale rimodellamento osseo a un rimodellamento accelerato , con danni precoci , no alla frattura franca . nel corpo umano , losso pi frequentemente colpito da lesioni da stress la tibia ( 49 , 1% ) , seguita dalle ossa del tarso ( 25 , 3% ) , metatarso ( 8 , 8% ) , femore ( 7 , 2% ) , perone ( 6 , 6% ) , ossa della pelvi ( 1 , 6% ) , ossa sesamoidi ( 0 , 9% ) e rachide ( 0 , 6% ) [ 2 ]  . 
le lesioni da stress della gamba coinradiol med ( 2013 ) 118 : 10341044 1035 and more rarely the bula ; they are responsible for pain on exertion in over 75% of cases [ 1 , 2 ] and are slightly more frequent in runners . volgono la tibia e , pi di rado , il perone ; sono responsabili di oltre il 75% dei casi di dolore da sforzo [ 1 , 2 ] e sono lievemente pi frequenti nei corridori . 
 the initial diagnostic approach is always conventional radiology , which is inexpensive , widely available , and quick to perfordespite the low sensitivity , radiography can reveal frank fractures or even abnormalities such as bone tumours and calcications of the soft tissues . 
although bone scintigraphy was previously considered the standard investigation for stress injuries of bone , today there is evidence that it has limited sensitivity in early stages , as well as poor specicity . 
 this paper describes the entire spectrum of stress injuries affecting the leg , with special emphasis on the role of mr imaging and ct . il primo momento diagnostico sempre la radiologia convenzionale , indagine di basso costo , ampia accessibilit e breve tempo dindagine . 
nonostante in passato la scintigraa ossea fosse considerata la metodica di riferimento per la valutazione delle lesioni ossee da stress , vi oggi evidenza di una limitata sensibilit in fase precoce ; essa inoltre gravata da bassa specicit . 
in questo lavoro verr esaminato lintero spettro delle lesioni da stress della gamba , enfatizzando il ruolo della rm e della tc . pathophysiology mechanical stress applied to bone leads to physiological remodelling , a result of reabsorption and repair processes [ 68 ]  . 
if the bone has undergone excessive stress , repair mechanisms are overwhelmed by the accumulation of microinjuries : this leads to the development of stress - related injuries and fractures [ 911 ]  . the application of load causes axial , bending or torsional stress [ 7 ]  . 
in cancellous bone , microfractures involve the trabeculae ; in cortical bone , they rst affect the bone interposed between the osteons and then the osteons themselves . fisiopatologia le sollecitazioni meccaniche cui losso sottoposto ne determinano un siologico rimodellamento , risultato di processi di riassorbimento e conseguente riparazione [ 68 ]  . 
se si va incontro a sollecitazioni eccessive , il meccanismo di riparazione sopraffatto dallaccumulo di microdanni : ci conduce allinsorgenza di lesioni e fratture da stress [ 911 ]  . lapplicazione di un carico determina sollecitazioni assiali , in essione o in torsione [ 7 ]  . 
nellosso spugnoso le microfratture coinvolgono le trabecole ; nellosso corticale interessano inizialmente losso interposto tra gli osteoni e solo successivamente questi ultimi . risk factors the risk factors associated with tibial stress injuries can be divided into two main groups : overload ( or training errors ) and biomechanical inefciency [ 11 ]  . the causes of overload include : exercising on hard ( like concrete ) and / or uneven surfaces , starting a training programme after a long period of inactivity , increasing intensity or duration of exercise too quickly , using worn - out or ill - tting shoes , running uphill or downhill . 
the major biomechanical inefciency which contributes to stress injuries of the leg is at feet ; at feet also predispose to overpronation , in which the excessive inward rotation of the foot and ankle cause the tibia to twist : this accentuates the strain placed on the leg bones and muscles . fattori di rischio i fattori di rischio associati alle lesioni da stress della tibia possono essere suddivisi in due gruppi principali : sovraccarico ( o errori di allenamento ) e inefcienza biomeccani ca [ 11 ]  . le cause di sovraccarico includono : svolgimento di attivit su superci dure ( come il cemento ) e / o irregolari , inizio di un programma di allenamento dopo un lungo periodo di inattivit , aumento dellintensit o della durata dellallenamento in maniera troppo rapida , utilizzo di scarpe logore o inadeguate , corsa in salita o discesa . 
la principale inefcienza biomeccanica che contribuisce a determinare le lesioni da stress della gamba il piede piatto ; esso prediradiol med ( 2013 ) 118 : 10341044 1036 site and symptoms the most common site of bone stress injuries is the cortical bone of the tibial diaphysis [ 11 ] and , in particular , the middle and distal third [ 2 ]  . 
the anterior cortex is more frequently involved than the posterior cortex , as the former is exposed to tensile forces which are more damaging compared to the compressive forces that act on the latter . 
the medial and lateral cortex are only rarely involved . the anatomical region of the tibia most frequently involved by cancellous bone stress fractures is the medial tibial plate [ 1217 ]  . 
around 6% of stress injuries affect the bula , most commonly the middle and distal third [ 12 , 18 ]  . clinically , stress injuries of the tibial diaphysis cause a painful syndrome known as the medial tibial stress syndrome ( mtss ) or shin splint . 
computed tomography ( ct ) is the best tool for the diagnosis of stress - related osteopoenia , and the only one able to detect it at an early stage . 
only rarely does prolonged stress induce osteopoenia detectable with conventional radiology ; in these cases the cortical bone appears thin and ill - dened ( grey cortex sign ) [ 20 ]  . 
advanced osteopoenia is usually associated with other stress injuries , known as cavitations and striations . la corticale diasaria della tibia il sito pi comune di lesioni ossee da stress [ 11 ] , in particolare il suo terzo medio e distale [ 2 ]  . 
la corticale anteriore pi frequentemente coinvolta da lesioni da stress rispetto alla corticale posteriore , poich sulla prima agiscono forze tensive , pi dannose rispetto a quelle compressive che agiscono sulla seconda . 
le corticali mediale e laterale sono interessate solo raramente . la parte anatomica della tibia pi frequentemente coinvolta nel caso di lesioni da stress della spongiosa il piatto tibiale mediale [ 1217 ]  . 
circa il 6% delle lesioni da stress coinvolge il perone , pi frequentemente a livello del terzo medio e del terzo distale [ 12 , 18 ]  . clinicamente , le lesioni da stress della corticale diasaria tibiale causano una sindrome dolorosa nota come sindrome tibiale mediale da stress ( mtss ) o shin - splint . 
quando si realizza una frattura da stress , il dolore non si riduce pi con il riposo e diventa costante . radiol med ( 2013 ) 118 : 10341044 1037 fig . 
a in a 20 - year - old asymptomatic male runner three regions of interest ( roi ) ( 1 , 2 , 3 ) placed over the tibial cortical bone show mean density values ranging between 1755 to 1658 hu , with a difference < 10% . 
a in un corridore maschio di 20 anni , la misurazione mediante tre regioni di interesse ( roi ) posizionate sulla corticale tibiale mostra un valore medio di densit compreso tra 1755 e 1658 hu , con una differenza < 10% . 
b in un corridore maschio di 20 anni con sindrome tibiale mediale da stress la misurazione con roi ( 1 , 2 , 3 ) mostra normali valori di densit della corticale mediale ( 2205hu ) e osteopenia delle corticali anteriore ( 1446hu , - 35% ) e posteriore ( 1887hu , - 14% ) ( 1 , 2 , 3 )  . cavitations and striations imaging the appearance of cavitations and striations in the bone cortex is correlated to osteoclastic proliferation [ 4 ]  . 
 [ 4 ] reported that the presence of changes affecting simultaneously the anterior and posterior cortices is highly specic for stress injury and allows the differentiation from other bone conditions , such as neoplasms and infections . 
whereas t1weighted images have low sensitivity for detecting these lesions , t2 - weighted and short - tau inversion - recovery ( stir ) sequences provide a clear depiction . fractures fractures almost exclusively occur in the anterior or posterior tibial cortex . 
solo raramente lo stress prolungato induce osteopenia individuabile con radiologia convenzionale ; in questi casi la corticale appare sottile e mal denita ( segno della corticale grigia ) [ 20 ]  . 
b scansione rm assiale , ottenuta con sequenza turbo spin echo ( tse ) t2 - pesata a un livello pi craniale rispetto alla scansione tc , che mostra cavitazioni e strie iperintense sia nella corticale anteriore che in quella posteriore ( segno della doppia corticale )  . tion of stress fractures affecting either the cortical or cancellous bone [ 22 , 23 ]  . 
 [ 4 ] hanno evidenziato come la presenza di alterazioni che coinvolgono simultaneamente la corticale anteriore e posteriore sia altamente specica per lesioni da stress e permetta una diagnosi differenziale con altre patologie dellosso , come neoplasie e infezioni . 
mentre le immagini pesate in t1 hanno una bassa sensibilit nellidenticare queste lesioni , esse sono facilmente visibili nelle sequenze t2 - pesate e in quelle short - tau - inversion - recovery ( stir )  . fratture le fratture si realizzano quasi esclusivamente nella corticale anteriore o posteriore della tibia . 
4a - c thirtyfour - year - old male runner with medial tibial stress syndrome lasting six months and 1 - month onset of intractable paa 1 - mm - thick high - resolution ct slice with 1 - mm - thick slices shows a longitudinal posterior tibial fracture ( arrowhead ) and calcic periosteal reaction ( arrow )  . 
a scansione tc ad alta risoluzione con spessore di 1mm che mostra una frattura longitudinale tibiale posteriore ( testa di freccia ) con reazione periostale calcica ( freccia )  . 
b immagine tse t2 - pesata con spessore di 3mm che mostra una rima di frattura iperintensa ( testa di freccia ) e periostite calcica ipointensa ( freccia )  . 
the presence of typical stress injuries and the absence of pathological tissue allow the differentiation from other causes of bone marrow oedema ( e.g. , infections , bone tumours )  . 
la rm consente una migliore valutazione delle alterazioni dei tessuti molli ( edema del periostio o del midollo osseo ) associate alle fratture da stress [ 4 , 23 ]  . 
nelle immagini assiali , le fratture orizzontali , a causa della non perfetta complanariet con il piano di scansione , appaiono tipicamente come lesioni osteolitiche ovali o rotondeggianti e possono simulare radiol med ( 2013 ) 118 : 10341044 1040 fig . 
b sagittal stir ( short - tau inversion recovery ) image depicts hyperintense fracture cleft ( arrow ) , as well as periosteal and endosteal oedema ( arrowheads )  . 
c t1 - weighted fat - saturated tse image obtained 5 min after contrast medium injection demonstrates enhancement of the fracture ( arrow ) and of the periosteal oedema ( arrowheads )  . 
c immagine tse t1 - pesata con saturazione del segnale del grasso ottenuta cinque minuti dopo liniezione del mezzo di contrasto che dimostra enhancement della frattura ( freccia ) e delledema periostale ( teste di freccia )  . 
lindividuazione di una massa di tessuto molle che inltra ed erode losso la chiave diagnostica per la diagnosi delle fratture patologiche [ 32 ]  . lesioni della spongiosa tibiale la diagnosi precoce delle lesioni da stress dellosso trabecolare raramente possibile con lesame radiograco convenzionale . 
sia nelle sequenze t1 pesate che in quelle t2 pesate , una frattura dellosso spugnoso appare come una linea ipointensa circondata su entrambi i versanti da edema del midollo osseo . 
6 twenty - year - old male runner with a 5 - week history of lower leg pastir image shows tibial periostitis ( arrowheads ) and bone marrow oedema ( b )  . 
 anche visibile edema del midollo osseo del canale diasario peroneale ( freccia ) per unassociata lesione da stress del perone . injuries is the presence of a fracture line [ 35 ]  . 
both coronal t1 - weighted tse ( a ) and t2 - weighted fat - saturated tse ( b ) images show a band of oedema in the medial tibial metaphysis . 
entrambe le immagini coronali , ottenute sia con sequenza tse t1 - pesata ( a ) che tse t2 - pesata con saturazione del segnale del grasso ( b ) , mostrano una banda di edema nella metasi tibiale mediale . 
presente edema muscolare ( freccia ) che potrebbe far sospettare la presenza di una lesione ossea biologicamente aggressiva ; lassenza di una massa di tessuto con segnale delle parti molli esclude una frattura patologica . 
dopo due settimane di riposo , la radiograa ( c ) mostrava una banda di osteosclerosi riparativa ( freccia )  . nidus ; however , the nidus may not be apparent on radiography and ct , if it is located in the periostium or endostium [ 36 , 37 ] , even in the presence of intense bone marrow oedema . 
in these cases , the key elements for the differential diagnosis are : the absence of the typical cortical bone stress injuries and the enhancement pattern on contrast - enhanced mr imaging [ 29 ]  . brodies abscess is a chronic osteomyelitis characterised by the presence of an infectious osteolytic focus surrounded by reactive osteosclerosis . 
ct demonstration of an abscess cavity surrounded by serpiginous radiolucencies allows the diagnosis of brodies abscess to be established . ribbings disease is a rare , painful condition , which present during the third or fourth decade of life and involves ma osteoide , facilmente caratterizzabile in presenza di un nidus corticale ; tuttavia lesame radiograco e la tc possono non individuare il nidus se localizzato nel periostio o nellendostio [ 36 , 37 ] , pur in presenza di intenso edema del midollo osseo . 
in questi casi gli elementi chiave per la diagnosi differenziale sono : lassenza delle tipiche lesioni corticali da stress e il comportamento contrastograco allesame rm con mezzo di contrasto [ 29 ]  . 
la dimostrazione con la tc di una cavit ascessuale e di immagini serpiginose circostanti ne consente la diagnosi . la malattia di ribbing una patologia rara , causa di dolore , che si presenta nella terza o quarta decade di vita e radiol med ( 2013 ) 118 : 10341044 1043 the tibial diaphysis . 
lesame radiograco , la tc e la rm possono rilevare ispessimento della corticale e sclerosi endostale con obliterazione del canale midollare ; mentre la rm pu mostrare ledema del midollo osseo nella cavit diasaria [ 38 ]  . conclusions conclusioni conventional radiology , always used as the rst - line imaging technique , may allow the detection of frank fractures . 
 mr imaging is the technique of choice for depicting the entire spectrum of stress injuries , allowing also the exclusion of other pathological conditions responsible for leg pact is useful , when mr imaging is negative , to depict very early changes in cortical bone . la radiologia convenzionale , sempre impiegata come metodica di prima istanza , consente talora di evidenziare la presenza di fratture franche . 
la tc utile , qualora lesame rm sia negativo , per dimostrare alterazioni corticali in fase estremamente precoce . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
malatesta , corso mazzini 18 , 28100 novara ( no ) , italy , tel . : + 39 - 347 - 1593684 , fax : + 39 - 0321 - 3733579 , e - mail : malatestaemanuele@hotmail.it preliminar results of this study were presented at the 26th national congress ainr , 19 - 22 october 2011 , padua , italy and at the 45th national congress sirm , 1 - 5 june 2012 , turin , italy . 
from may 2009 to april 2012 , 28 patients ( 6 men and 22 women ; mean age , 54 years ) with a total of 35 aneurysms were treated with fds . 
we evaluated postprocedural technical success and long - term efcacy , with follow - up examinations performed at 37 days [ computed tomography ( ct ) / magnetic resonance ( mr ) angiography ] and at 3 , 6 and 12 months ( digital subtraction angiography , dsa )  . 
da maggio 2009 ad aprile 2012 sono stati trattati mediante fd 28 pazienti ( 6 maschi e 22 femmine ; et media 54 anni ) portatori di 35 aneurismi cerebrali . 
abbiamo valutato il successo tecnico procedurale e lefcacia a distanza mediante angiotomograa computerizzata ( tc ) o angio - risonanza magnetica ( rm ) a 37 giorni , quindi angiograa digitale a sottrazione ( dsa ) a 3 , 6 e 12 mesi . 
i risultati da noi ottenuti , in linea con i dati della letteratura , documentano che il trattamento degli aneurismi cerebrali mediante fd rappresenta unopzione sicura ed efcace in casi selezionati ( aneurismi a largo colletto , fusiformi , blister - like ) , con buoni risultati nel tempo . parole chiave stent a diversione di usso aneurismi intracranici silk stent pipeline stent trattamento endovascolare introduction introduzione the treatment of brain aneurysms represents a major challenge for specialists in the eld . 
since then , the inventiveness of the pioneers coupled with the remarkable technological advances in materials have allowed the endovascular treatment of intracranial aneurysms to shift from the occlusion of the parent artery to the occlusion of the aneurysm dome [ 2 ]  . 
with the rening of techniques and the introduction of coils , endovascular treatment gradually established itself , in part thanks to the stability of the results obtained [ 3 ]  . recently , in an effort to further improve the endovascular technique , alternative devices have been developed such as ow diverters ( fd ) ( pipeline - ped , ev3 neurovascular irvine california ; silk , balt extrusion , montmorency , france ) and meshed stents , which cover the aneurysm neck and modify haemodynamic ow within the aneurysm and parent artery to induce thrombosis , while preserving the patency of covered side branches [ 46 ]  . the primary purpose of this paper is to report our preliminary experience with the treatment of intracranial aneurysms with fd , in terms of complete exclusion of the aneurysm dome and patency of the stent and covered branches . 
dal 1974 , epoca in cui serbinenko [ 1 ] descrisse per primo il trattamento di aneurismi cerebrali per via endovascolare mediante luso di un palloncino di lattice , in pochi anni linventiva dei pionieri di tale metodica , associata al notevole sviluppo tecnologico dei materiali , ha consentito il passaggio del trattamento endovascolare degli aneurismi intracranici dallocclusione del vaso portante al trattamento selettivo endosacculare [ 2 ]  . 
 con lafnamento delle tecniche e lintroduzione delle spirali , il trattamento endovascolare andato sempre pi affermandosi grazie anche alla stabilit dei risultati ottenuti [ 3 ]  . nel tentativo di migliorare ulteriormente la tecnica endovascolare , negli ultimi anni , sono stati sviluppati device alternativi alle spirali quali gli stent a diversione di usso ( fd ) ( pipeline - ped , ev3 neurovascular irvine california , usa ; silk , balt extrusion , montmorency , francia ) , stent a maglie strette , che posizionati a copertura del colletto aneurismatico , modicano lemodinamica del usso nella sacca e nel vaso portante , assicurando la trombosi dellaneurisma , con conservata perviet del vaso dorigine e dei suoi rami collaterali ricoperti [ 46 ]  . scopo primario del lavoro riportare la nostra preliminare esperienza nel trattamento di aneurismi intracranici con fd , in termini di esclusione completa della sacca aneurismatica dal circolo , perviet dello stent e dei vasi ricoperti . 
 twenty eight consecutive patients ( 6 men and 22 women ; mean age , 54 years ) with 35 aneurysms , were treated with fd between june 2009 to and april 2012 . 
six patients were treated for asymptomatic ( incidental ) aneurysm , seven because of headaches , ve due to mass effect ( brainstem and cranial nerves ) , nine due to recanalisation following previous endovascular / surgical repair , one for a subarachnoid haemorrhage ( sah ) due to ruptured blister - like aneurysm ( table 1 )  . 
the indication for treatment with fd was conmateriali e metodi nel nostro istituto , da maggio 2009 ad aprile 2012 , sono stati trattati consecutivamente mediante fd 28 pazienti ( 6 maschi e 22 femmine ; et media 54 anni ) , portatori complessivamente di 35 aneurismi ( tabella 1 ) , previa approvazione del comitato etico del nostro istituto . 
in sei casi i pazienti erano asintomatici ( aneurisma incidentale ) , in 7 presentavano cefalea , in 5 sintomi da effetto massa sulle strutture cerebrali limitrofe ( tronco encefalo e nervi cranici ) , in 9 casi abbiamo radiol med ( 2013 ) 118 : 971983 table 1 study population , clinical presentation and distribution of treated aneurysms according to location , morphology , type and size tabella 1 popolazione di studio , presentazione clinica e suddivisione degli aneurismi trattati in base alla sede , morfologia , tipo e dimensioni . 
lindicazione al trattamento con fd stata posta in base alla morfologia dellaneurisma ( fusiforme o sacciforme ) , allassenza di colletto ( dome / neck ratio < 2 ) e quando il trattamento con tecniche convenzionali ( spirali e stent ) sembrava essere difcoltoso ( alta probabilit di fallimento , di complicanze o recidiva )  . 
tutti i trattamenti sono stati eseguiti su angiografo monoplano philips integris v5000 ( philips medical sciences , best , olanda ) , apparecchiatura non dotata di tecnica 3d rotazionale o software per neuronavigazione . 
lo studio stato effettuato in modo prospettico . valutazione pre - operatoria tutti i pazienti hanno eseguito , nella fase pre - operatoria , uno studio angio - tomograa computerizzata ( tc ) o angio974 radiol med ( 2013 ) 118 : 971983 fig . 
1a - d aneurisma sacciforme dellarteria basilare : dsa pretrattamento ( iniezione in vertebrale sinistra ; visione laterale ) ( a ) ; il follow - up dsa a 4 mesi ( iniezione in vertebrale sinistra ; visione laterale ) ( b ) , eseguito al momento del peggioramento clinico , mostra lesclusione dellaneurisma dal circolo ( trattamento con ped , solitaire e spirali axium ) ; lo studio rm a 4 mesi [ uid attenuated inversion recovery ( flair ) coronale ] evidenzia la trombosi della sacca con effetto massa sul tronco encefalico ( c ) ; lo studio rm a 12 mesi ( flair coronale ) documenta la stabilit del trattamento con persistenza delleffetto massa sul tronco encefalico , senza sostanziali modicazioni dei reperti ( d )  . cording to the diameter of the parent artery and extension of coverage . 
nel post - processing sono state realizzate ricostruzioni mippr ( multiplanar reconstruction based on maximum intensity projection images ) , per poter scegliere la misura pi appropriata dello stent ( diametro e lunghezza ) in base al valore del diametro del vaso da ricostruire e dellestensione della copertura . 
 stato inoltre utilizzato un algoritmo di ricostruzione analisi vaso , presente nel software del nostro sistema di archiviazione immagini ( pacs kodak carestream ; easteam kodak company ) , in grado di creare immagini lineari del vaso di interesse e di calcolarne il reale diametro assiale . materiali impiegati sono stati impiegati i due tipi di fd in commercio , posizionando complessivamente 43 fd , 36 ped ( diametro da 2 , 5 a 4 , 5 mm , lunghezza da 16 a 20 mm ) e 7 silk ( diametro da 3 , 5 a 4 , 5 mm , lunghezza da 25 a 50 mm )  . radiol med ( 2013 ) 118 : 971983 fig . 
 protocollo procedurale prima dellintervento tutti i pazienti sono stati informati del tipo di trattamento programmato , dei beneci e dei rischi as976 radiol med ( 2013 ) 118 : 971983 was performed using a 4 fr diagnostic catheter ( cordis corp , johnson and johnson , miami lakes , fl , usa ) and a 0.035 inch hydrophilic guidewire ( terumo corp , tokyo , japan ) ; subsequently , a carrier catheter ( 6 fr envoy , corp , johnson and johnson ; 6 fr penumbra neuron , penumbra inc , harbor bay pkwy alameda , ca , usa ) was inserted to reach a suitable location in the cavernous segment of ica or the v3 segment of the vertebral artery . 
 in all cases , transend 205 ex floppy ( boston scientic , natek , na , usa ) or synchro 14 ( boston scientic ) microguides were used . then , the fd system was pushed through the delivery microcatheter and aligned with the distal tip of the microcatheter ; the microcatheter was retracted slowly to unsheathe the stent , while a forward tension was maintained on the stent to keep it in place , with a push and pull technique . 
 after placement of the stent , angiography was performed to evaluate technical success , intended as covering the aneurysm neck and proper distention of the stent within the vessel lumen . medical therapy all patients were pretreated with 250 mg of ticlopidine twice daily for 5 days . 
only in one of the patients , treated as an emergency for a ruptured aneurysm , was a bolus of 300 mg of clopidogrel administered 6 hours before the procedure . 
 at the beginning the procedure all patients received heparin ( 50 iu / kg + 1000 iu / h ) while a bolus of acetylsalicylic acid ( 500 mg ) was administered when releasing the stent . 
 after the procedure and during the rst 3 months , dual antiplatelet therapy ( 250 mg of ticlopidine twice daily and 300 mg of acetylsalicylic acid once daily ) was prescribed ; single antiplatelet therapy with 300 mg of acetylsalicylic acid once daily was then continued for 3 to 6 months . clopidogrel was not used because of the high percentage of drug resistance and because at the time of treatment this drug was not reimbursed by the italian national health system . sociati ed hanno rmato un consenso informato . 
 tutti gli interventi sono stati eseguiti in sala angiograca , mediante angiografo monoplano philips integris v5000 ( philips medical sciences , best , olanda ) , in anestesia generale , previa puntura percutanea trans - femorale comune , con accesso vascolare 6 fr ; stato eseguito un esame diagnostico preliminare mediante lutilizzo di catetere 4 fr ( cordis corp , johnson and johnson , miami lakes , fl , usa ) e guida idrolica 0 , 035 inch ( terumo corp , tokyo , giappone ) ; successivamente stato posizionato un catetere portante ( envoy 6 fr , corp , johnson and johnson ; penumbra neuron 6 fr , penumbra inc , harbor bay pkwy alameda , ca , usa ) nel vaso di interesse in una sede adeguata al trattamento . 
in tutti i casi trattati con ped stato impiegato un microcatetere marksman ( ev3 neurovascular ) o in alternativa rebar ( ev3 neurovascular irvine ) ; nei pazienti trattati con silk sono stati usati un microcatetere vasco + 21 e vasco + 25 ( balt extrusion )  . 
in tutti i casi sono state impiegate microguide transend 205 ex floppy ( boston scientic , natek , na , usa ) o synchro 14 ( boston scientic )  . il fd stato quindi inserito allinterno del microcatetere , sino ad allinearlo allestremo distale del microcatetere ; lo stent stato poi rilasciato , a cavallo del colletto aneurismatico , con una combinazione tra retrazione del micro catetere e spinta della guida di rilascio , in tecnica di push and pull . 
dopo il posizionamento dello stent , sono stati eseguiti i controlli angiograci per valutare il successo tecnico , inteso come copertura del colletto aneurismatico e la corretta distensione dello stent allinterno del lume vasale . terapia medica tutti i pazienti hanno assunto ticlopidina 250 mg2 / die da 5 giorni prima dellintervento . 
nel solo caso di trattamento di aneurisma blister - like rotto , trattato in urgenza , stato somministrato un bolo di clopidogrel 300 mg , 6 ore prima della procedura . 
dopo il trattamento e per i primi 3 mesi stata impostata una duplice terapia antiaggregante ( ticlopidina 250 mg2 / die + acido acetilsalicilico 300 mg1 / die ) ; dal 3 al 6 mese stata proseguita la singola terapia antiaggregante con acido acetilsalicilico 300 mg1 / die . eccetto che in un caso non abbiamo utilizzato clopidogrel a causa dellalta percentuale di resistenza e la non mutuabilit del farmaco . follow - up follow - up all patients underwent follow - up by ct or mr 3 to 7 days after treatment to assess correct positioning of the stent . 
 tutti i pazienti hanno eseguito follow - up mediante angio - tc o angio - rm a 37 giorni dallintervento per valutare il corradiol med ( 2013 ) 118 : 971983 fig . 
3a - d liniezione in carotide interna destra mostra la presenza di un aneurisma blister - like rotto del tratto carotido - oftalmico ; proiezione obliqua destra a 45 : immagine sottratta ( a ) , non sottratta ( b ) ; ricostruzione del sifone carotideo con 2 ped embricati ( c ) a copertura del blister ; ( d ) la ricostruzione mippr dello studio angio - tc eseguito a 7 giorni dallintervento , mostra la sovrapposizione dei 2 ped con corretta copertura del blister . follow - up with digital subtraction angiography ( dsa ) or alternatively ct was performed at 3 , 6 and 12 months . 
il follow - up a lungo termine ha previsto una dsa di controllo a 3 , 6 e 12 mesi dallintervento o in alternativa uno studio angio - tc cerebrale . 
sono stati analizzati i seguenti parametri : esclusione della sacca aneurismatica dal circolo ; perviet dello stent ; perviet del vaso ricostruito e dei vasi arteriosi originanti dal tratto ricoperto , in accordo con i dati della letteratura [ 7 , 8 ]  . results risultati thirty treatments were performed in 28 patients ( two cases were retreated at 3 months because of partial coverage of the aneurysm neck )  . 
the patient died in intensive care 21 days after the procedure abbiamo effettuato complessivamente 30 interventi in 28 pazienti ( due ritrattamenti a 3 mesi per copertura parziale del colletto aneurismatico )  . 
in one case of a dissecting middle cerebral aneurysm we had a defect of ped distal opening , with locking and distal migration of the system in the parent artery . 
attempts to recover the system ( snareandra andramed gmbh germany , ev3 neurovascular hyperform balloon ; ev3 neurovascular retriever alligator ) were not effective , with subsequent vessel perforation and death of the patient after 24 hours . 
we therefore had an overall mortality of 7% ( 2 / 28 patients )  . il successo tecnico ( adeguata copertura del colletto aneurismatico in assenza di complicanze intra - procedurali ) si ottenuto in 29 / 30 interventi ( 96 , 6% ) ; in un caso ( 3 , 4% ) di aneurisma della cerebrale media si vericata la difettosa apertura distale dello stent ( ped ) con incarceramento e migrazione distale dello stesso nel vaso parente . 
sono stati effettuati numerosi tentativi di recupero dello stent ( snareandra andramed gmbh , germania ; ev3 neurovascular hyperform balloon ; ev3 neurovascular retriever alligator ) risultati tuttavia infruttuosi , con successiva perforazione della cerebrale media e decesso del paziente a distanza di 24 ore . 
abbiamo pertanto osservato una mortalit complessiva del 7% ( 2 / 28 pazienti )  . aneurysm occlusion rate at follow - up esclusione dal circolo dellaneurisma table 2 shows the occlusion rate of treated aneurysms according to size . 
in the remaining cases minimal opacication of a residual sac was seen , with persistence of the contrast medium in the venous phase of the study , interpreted as a partial thrombosis of the aneurysm dome [ 6 ]  . patency of the stent , parent artery and covered side branches parent artery patency was observed in 100% at 3 , 6 and 12 months , without any occurrence of acute stent thrombosis . intrastent intimal hyperplasia , with haemodynamically nonsignicant stenosis and without symptoms , was observed at 3 months follow - up of two carotid ophthalmic aneurysms treated with ped implantation . 
a 3 mesi abbiamo osservato complessivamente un tasso di esclusione dal circolo del 60% ( 18 / 30 aneurismi ) , a 6 mesi del 73% ( 19 / 26 ) ed a 12 mesi dell89% ( 16 / 18 )  . 
nei restanti casi si osservava alla dsa unopacizzazione parziale e tardiva della sacca aneurismatica indicativa di trombosi incompleta [ 6 ]  . perviet dello stent , dei vasi parenti e delle branche collaterali ricoperte dallo stent in tutti i casi abbiamo osservato completa perviet dello stent a 3 , 6 e 12 mesi , in assenza di trombosi intra - stent . al follow - up a 3 mesi abbiamo riscontrato due casi di iperplasia intimale intra - stent determinanti stenosi non emodinamicamente signicative , in assenza di sintomatologia clinica associata ( trattamento di due aneurismi del tratto carotido - oftalmico della carotide interna con ped )  . 
4a - d liniezione in carotide interna destra , eseguita a distanza di 3 mesi dal trattamento con ped di un aneurisma del tratto carotido - oftalmico , mostra la presenza di iperplasia intimale intrastent , determinante stenosi < 40% : ( proiezione obliqua ) immagine sottratta ( a ) e non ( b ) ; il controllo dsa a 12 ( c ) e 24 mesi ( d ) dallintervento documenta la progressiva riduzione delliperplasia e della stenosi . 
there were no other cases of occlusion of the covered side branches . outcome clinico vato nessun altro caso di steno - occlusione dei vasi collaterali ricoperti dagli stent . clinical outcome clinical follow - up was performed with a modied rankin scale ( mrs ) in 26 patients . 
we observed four cases of transient , self - limited worsening of neurological symptoms in the immediate postprocedural period : three of these patients had giant / large aneurysm with mass effect . 
abbiamo osservato 4 casi di peggioramento transitorio del quadro clinico neurologico , autolimitatisi nellimmediato post - trattamento : di questi 3 pazienti erano portatori di aneurismi giant / large con effetto massa sulle strutture limitrofe . 
in un paziente ( con aneurisma giant dellarteria basilare ) si vericato un importante peggioramento clinico 980 radiol med ( 2013 ) 118 : 971983 them ( with a giant basilar artery aneurysm ) experienced a major clinical deterioration 4 months after treatment . 
although surgery has a lower relapse rate in the region of the aneurysm neck ( 1.4%8% ) [ 1012 ] compared to endovascular treatment ( 9%59% ) [ 10 , 13 , 14 ] , it is associated with higher morbidity and mortality rates , especially in cases of large / giant or wide neck aneurysms [ 1012 ]  . 
endovascular treatment of cerebral aneurysms with a conventional device ( coils with the possible association of a stent ) represents an effective option which is , however , associated with a risk of failure in cases of unfavorable anatomy , difculty obtaining a total lling of the aneurysm with coils [ 15 , 16 ] , and difculty achieving complete coverage of the neck , with a high risk of recurrence [ 3 ]  . the use of fd changes the treatment approach from intrasaccular to parent artery reconstruction , obtaining greater neck coverage than with coils alone [ 6 ]  . 
this new type of stent , by reconstructing the parent artery , determines a reduction of the whirling ow within the sac , inducing thrombosis and simultaneously ensuring patency of the covered side branches . in our experience , we achieved technical success in 29 / 30 treatments ( 96.6% ) , with adequate coverage of the aneurysm neck , without intraprocedural complications . 
in one case ( 3.8% ) technical failure occurred leading to the patients death ( treatment - related mortality , 3.5% ) , in line with the literature data [ 8 , 17 ]  . there was one additional death in a case of a ruptured blister - like aneurysm that was treated with ped implantation in an emergency setting . 
 in un caso di aneurisma del tratto cavernoso della carotide interna , il paziente ha lamentato a 3 mesi dallintervento , la comparsa di scotomi intermittenti , senza decit del campo visivo : la sintomatologia poi regredita completamente al controllo a 12 mesi dal trattamento . discussione il trattamento endovascolare degli aneurismi cerebrali rappresenta attualmente una valida alternativa alla chirurgia [ 9 ] ; questultima presenta un pi basso grado di recidiva nella regione del colletto ( 1 , 4%8% ) [ 1012 ] a confronto con il trattamento endovascolare ( 9%59% ) [ 10 , 13 , 14 ] ma associata ad un maggior tasso di mortalit e morbilit , particolarmente in aneurismi large / giant o con ampio colletto [ 1012 ]  . 
il trattamento endovascolare degli aneurismi cerebrali con device convenzionali ( spirali con eventuale associazione di stent ) rappresenta unopzione efcace , associata tuttavia a rischio di fallimento terapeutico in caso di anatomia sfavorevole , difcolt nellottenere un riempimento totale dellaneurisma con spirali [ 15 , 16 ] , difcolt nella copertura completa del colletto , con alto rischio di recidive [ 3 ]  . lutilizzo dei fd ha cambiato lapproccio del trattamento endovascolare dalla tecnica classica endosacculare a quella innovativa endoluminale , con ricostruzione del vaso dorigine e con una maggiore copertura del colletto aneurismatico rispetto a quella ottenuta con tecniche convenzionali [ 6 ]  . 
questo tipo di stent , ricostruendo il vaso da cui origina laneurisma , determina una riduzione del usso vorticoso allinterno della sacca , inducendone la trombosi e garantendo contestualmente la perviet dei vasi arteriosi collaterali . nella nostra esperienza abbiamo ottenuto un successo tecnico in 29 / 30 interventi ( 96 , 6% ) , con adeguata copertura del colletto aneurismatico , in assenza di complicanze intraprocedurali . 
in un solo caso ( 3 , 8% ) si vericato insuccesso tecnico con decesso del paziente ( mortalit intervento - correlata : 3 , 5% ) , in linea con i dati della letteratura [ 8 , 17 ]  . 
 the treatment of ruptured blister - like aneurysms with fd is an option reported in the literature [ 1820 ] : in fact , this type of aneurysm has a fragile and poorly dened wall , without a recognisable neck , which makes surgical and endovascular treatment very difcult . 
fd currently represents the only therapeutic option that allows a quick and safe endovascular repair of the diseased vessel , in both elective and emergency settings [ 18 - 20 ]  . 
sah is still the greatest limit to the use of fd , given the need for dual antiplatelet therapy : in the cases of ruptured blister - like aneurysms , however , the need for immediate treatment overcomes this limitation . 
in our experience , we administered a bolus of 300 mg of clopidogrel 6 hours before the procedure and continued with the usual dual antiplatelet therapy postoperatively , in the absence of bleeding complications . 
the literature shows a different therapeutic management with administration of dual antiplatelet therapy only in the postoperative period [ 1820 ]  . we observed complete occlusion of the aneurysm in 60% of cases at 3 months , 73% at 6 months , 89% at 12 months ( table 2 )  . 
these data are in agreement with the current literature , as in the pipeline intracranial treatment of aneurysms ( pita ) trial [ 21 ] , which showed complete aneurysm occlusion in 93% and 97% at 6 and 12 months , respectively , or the buenos aires [ 17 ] and budapest experiences [ 8 ]  . 
these results demonstrate the effectiveness of the fd in the treatment of intracranial aneurysms , with a high rate of complete occlusion of the aneurysm sac at follow - up . these innovative devices preserve the patency of covered side branches , as demonstrated in preclinical [ 4 ] and clinical studies [ 7 ]  . 
we experienced one case of steno - occlusion of the orbital branches of the ophthalmic artery and il trattamento di aneurismi blister - like rotti con fd unopzione riportata in letteratura [ 1820 ] : questo tipo di aneurismi presenta , infatti , una parete fragile e non ben denita , in assenza di colletto riconoscibile , che rende difcile il trattamento sia chirurgico che endovascolare con tecniche convenzionali . 
lesa rappresenta ancora oggi la maggiore controindicazione allutilizzo del fd , data la necessit della doppia terapia antiaggregante : negli aneurismi blister - like rotti tuttavia la necessit di un immediato trattamento supera questa controindicazione . 
nella nostra esperienza abbiamo somministrato un bolo di 300 mg di clopidogrel 6 ore prima dellintervento e proseguito poi con la consueta doppia terapia antiaggregante nel post - operatorio , in assenza di complicanze emorragiche . 
in letteratura riportato un differente management terapeutico con somministrazione della doppia terapia antiaggregante solo nel postoperatorio [ 1820 ]  . abbiamo osservato una completa esclusione degli aneurismi dal circolo del 60% a 3 mesi , del 73% a 6 mesi e dell89% a 12 mesi ( tabella 2 )  . 
tali risultati sono in accordo con i dati della letteratura , come dimostrato dallo studio pipeline intracranial treatment of aneurysms ( pita ) [ 21 ] che riporta tassi di occlusione a 6 e 12 mesi , rispettivamente del 93% e 97% e dalle esperienze preliminari di buenos aires [ 17 ] e di budapest [ 8 ]  . 
questi risultati documentano lefcacia dei fd nel trattamento degli aneurismi intracranici con alto tasso di completa occlusione della sacca aneurismatica al follow - up . tali innovativi device preservano la perviet delle branche collaterali ricoperte , come dimostrato da studi preclinici [ 4 ] e clinici [ 7 ]  . 
nella nostra esperienza abbiamo osservato un solo caso di steno - occlusione delle branche orbitali dellarteria oftalmica e riduzione di calibro di questultima , con comparsa di scotomi intermittenti , risoltisi poi nel tempo . 982 radiol med ( 2013 ) 118 : 971983 reduction of the arterys caliber with intermittent scotomas , which resolved over time . the risk of thrombosis and intrastent stenosis is a problem related to the use of intracranial stents ; hence the need for dual antiplatelet therapy . 
probably the peculiarity of the antiplatelet regimen used , different from that used in the major studies in the literature [ 8 , 17 , 21 ] , contributed to this result . fd stents were introduced for the treatment of fusiform , saccular , large , giant or wide - neck aneurysms [ 5 , 7 , 17 ]  . 
large and giant aneurysms , which manifest primarily through a mass effect on the surrounding anatomical structures , can be treated with conventional devices , but the results are unsatisfactory [ 10 , 13 , 14 ]  . 
the fd progressively excludes the aneurysm from the circulation , eliminating the risk of rupture and providing thrombus resorption ( shrinkage of the aneurysm ) , with reduction of the mass effect . 
 i nostri risultati sono in linea con i dati della letteratura : nel trial pita [ 21 ] stato osservato solo un caso di stenosi moderata e szikora et al . 
 [ 6 ] hanno riportato la presenza di stenosi emodinamicamente signicative nel 33% dei casi trattati , la maggior parte delle quali brevi e localizzate nella porzione distale dello stent , soprattutto nei casi in cui il diametro del vaso distalmente al colletto dellaneurisma era molto minore rispetto a quello prossimale . 
probabilmente la peculiarit dello schema terapeutico antiaggregante da noi adottato , differente da quello dei maggiori studi della letteratura [ 8 , 17 , 21 ] , ha contribuito ad ottenere tale risultato . gli stent fd sono stati introdotti per il trattamento di aneurismi fusiformi , sacciformi , di grandi dimensioni o senza colletto [ 5 , 7 , 17 ]  . 
gli aneurismi large e giant , che si manifestano primariamente con leffetto massa sulle strutture anatomiche limitrofe , possono essere trattati con device convenzionali , con risultati tuttavia insoddisfacenti [ 10 , 13 , 14 ]  . 
 il fd escludendo completamente dal circolo laneurisma , ha come obbiettivo lannullamento del rischio di rottura e il riassorbimento del trombo endosacculare , con riduzione delleffetto massa ; linduzione della trombosi pu tuttavia aggravare leffetto massa stesso , con esacerbazione della sintomatologia clinica [ 5 ]  . 
the results obtained are in agreement with those reported in the literature [ 6 8 , 1721 ] , and in particular with the recently published french multicentre study [ 22 ] and german single - centre i limiti del nostro studio sono rappresentati dal basso numero di pazienti e dal breve follow - up . 
granata , e - mail : effegranata@alice.it received : 29 february 2012 / accepted : 23 may 2012 / published online : 27 may 2013 springer - verlag 2013 abstract purpose . 
between december 2010 and december 2011 , we prospectively observed 32 patients ( 30 with trigeminal neuralgia and two with hemifacial spasm ) , with a suspected clinical diagnosis of neurovascular conict . 
to assess the contact between nerve and vessel , magnetic resonance imaging ( mri ) by three - dimensional ( 3d ) constructive interference in steady state ( ciss ) and high - resolution mr angiography ( mra ) were performed in all cases . 
advanced virtual mri techniques , such as image fusion and virtual cisternography , are able to depict the complex anatomical relationships between neural and vascular structures within the cisternal spaces of the skull base . 
tra dicembre 2010 e dicembre 2011 , sono stati prospetticamente arruolati 32 pazienti ( 30 con nevralgia trigeminale e 2 con emispasmo faciale ) , con diagnosi clinica di conitto neuro - vascolare . allo scopo di denire il contatto anomalo tra una struttura vascolare e il nervo cranico , i pazienti sono stati sottoposti a risonanza magnetica ( rm ) con tecnica 3d - constructive interference in steady - state ( ciss ) , e a studio angio - rm ad alta risoluzione . 
in tutti i pazienti , inoltre , abbiamo realizzato una simulazione pre - chirurgica dellintervento di decompressione microvascolare utilizzando la tecnica di fusione di immagine bidimensionale e la cisternograa virtuale . 
le tecniche di fusione di immagine bidimensionale e la cisternograa virtuale si sono dimostrate adeguate nella valutazione dei complessi rapporti anatomici tra strutture nervose e strutture vascolari nel contesto degli spazi cisternali della 1046 radiol med ( 2013 ) 118 : 10451054 keywords neurovascular conicts mr cisternography image fusion base cranica . 
esse costituiscono un ottimo strumento pre - chirurgico in grado di migliorare la tradizionale valutazione rm di questa regione . parole chiave conitto neuro - vascolare cisternograa rm fusione di immagine introduction introduzione neurovascular conicts are cranial nerve dysfunctions caused by an abnormal contact between cranial nerves and arterial or venous vessels [ 1 ]  . 
neurovascular compression syndrome includes trigeminal neuralgia ( tn ) and hemifacial spasm ( hfs ) , related to involvement of the 5th and 7th cranial nerves [ 24 ]  . 
less common are glossopharyngeal neuralgia , sensorineural hearing loss [ 5 ] or hypoglossal paralysis [ 6 ]  . first neurosurgical attempts , starting in the 1930s , were realised in the absence of radiological assessment , only relying on previous reports of nerve compression supported by vascular structures . the microvascular decompression technique was proposed by dandy in l932 [ 7 ] , later rediscovered by gardner , and nally fully implemented by jannetta in the 1970s [ 8 ]  . 
 modern neurosurgical techniques are widely supported by magnetic resonance imaging ( mri ) , which allows a clear visualisation of the complex neurovascular anatomy within the cisternal spaces of the skull base [ 9 , 10 ]  . 
in particular , three - dimensional ( 3d ) constructive interference in steady state ( ciss ) and mr angiography ( mra ) by means of 3dtime - of - ight ( tof ) sequences provide an excellent multiplanar depiction of nervous and vascular structures inside the cerebrospinal uid ( csf ) [ 1 , 3 , 1012 ]  . the aim of the study was to evaluate advantages and limits of advanced virtual mri techniques , such as 3d - ciss and 3d - tof image fusion and mr cisternography , in planning surgery in patients with neurovascular conicts . 
to this end , we performed a presurgical simulation of microvascular decompression using virtual mri techniques and compared the surgical ndings with the radiological patterns . materials and methods patient population and mri study protocol the whole study was approved by the university ethics committee prior to patient recruitment ; written informed consent of all patients was obtained . 
between december 2010 and december 2011 , 32 consecutive patients ( 30 with tn and two with hfs ; 22 women and 10 men ; mean age , 427 years ; age range , 2368 ) , admitted to the neurosurgical centre of our institution with a suspected clinical diagnosis of neurovascular conict , underwent presurgical mri examination with conventional sequences . 
the clinical diagnostic criteria were observed in all cases . la sindrome da conitto neuro - vascolare legata a un anomalo contatto tra un nervo cranico e un vaso arterioso o venoso , in grado di determinare una disfunzione attiva del nervo [ 1 ]  . 
le sindromi da compressione neuro - vascolare includono la nevralgia trigeminale e lemispasmo facciale , espressione del coinvolgimento rispettivamente del v e del vii nervo cranico [ 24 ]  . 
meno comuni sono , per converso , la nevralgia glossofaringea , lipoacusia neurosensoriale [ 5 ] o la paralisi del nervo ipoglosso [ 6 ]  . i primi tentativi neurochirurgici , n dagli anni trenta , furono realizzati in assenza di valutazione radiologica e si basavano solo su precedenti esperienze di casi di compressione nervosa sostenuta da strutture vasali . 
 la tecnica di decompressione microvascolare fu proposta da dandy nel 1932 [ 7 ] , in seguito riscoperta da gardner e , inne , perfezionata da jannetta negli anni settanta [ 8 ]  . 
 le tecniche neurochirurgiche moderne sono ampiamente supportate dalla valutazione di risonanza magnetica ( rm ) che consente una chiara denizione della complessa anatomia neuro vascolare , nel contesto degli spazi cisternali della base cranica [ 9 , 10 ]  . 
in particolare , le sequenze 3d constructive interference in steady - state ( ciss ) e lo studio angio - rm ( mra ) consentono di ottenere uneccellente denizione multiplanare delle strutture nervose e vascolari contenute nel liquor cefalo - rachidiano [ 1 , 3 , 1012 ]  . scopo del nostro lavoro stato la valutazione delle possibilit e dei limiti di tecniche avanzate virtuali di risonanza magnetica , quali la fusione di immagine bidimensionale e la cisternograa virtuale , nella pianicazione pre - chirurgica in pazienti con conitto neuro - vascolare . 
in the 3d - ciss and 3d - tof fusion images , the nervous structures were automatically displayed in blue and the arterial vessels in deep red . virtual cisternography relies on volume rendering reconstruction of the 3d ciss images . 
the position of the virtual camera is indicated on multiplanar reconstruction images as the intersection of two perpendicular lines , and the projection and viewing angle is indicated as a pyramid - shaped beain virtual cisternography , the anatomical structures closer to the virtual camera eye are displayed in the foreground , whereas those more distant from the virtual eye are displayed in the background [ 1 , 12 , 13 ]  . results in all operated patients , virtual presurgical simulation with mri was consistent with the intraoperative ndings . 
ventuno pazienti sono stati inne sottoposti a intervento di decompressione microvascolare presso il dipartimento di neurochirurgia del policlinico universitario di messina . protocollo rm lo studio di rm stato realizzato con un magnete superconduttore da 1 , 5 t ( magnetom , siemens medical solutions , erlangen , germania ) , intensit di risalita dei gradienti di 26 mt / m , slew rate 200 t / m / ms e bobina dellencefalo . 
tr : 39 ms ; te : 6 , 5 ms ; ip angle : 20 gradi ; fov : 200 mm ; matrice : 192 ( cid : 31 ) 512 ; spessore di fetta : 0 , 88 mm ; una acquisizione . in tutti i pazienti sono state quindi realizzate la fusione di immagine bidimensionale e la cisternograa virtuale . realizzazione della fusione di immagine bidimensionale e della cisternograa virtuale i dati delle sequenze 3d - ciss e 3d - tof sono stati trasferiti su una workstation indipendente ( leonardo workstation , vd 30b , siemenserlangen , germany )  . 
nelle immagini di fusione bidimensionale delle sequenze 3dciss e 3d - tof , le strutture nervose sono state automaticamente rappresentate in blu , mentre i vasi arteriosi in rosso intenso . la cisternograa virtuale basata sulla tecnica di ricostruzione volume rendering delle immagini 3d - ciss . 
questa funzione consente di creare una visione tridimensionale dinamica utilizzando i dati volumetrici in una vera e propria videocamera virtuale che pu essere traslata e ruotata anche con ni movimenti . 
la posizio ne della videocamera virtuale viene indicata sulle imma gini della ricostruzione multiplanare come lintersezione di due rette perpendicolari ; la proiezione e langolo di vi suale sono indicati come un cono a forma di piramide . 
 nella cisternograa virtuale , le strutture anatomiche pi vicine allocchio della videocamera virtuale sono rappresentate in primo piano , mentre le strutture pi distanti dallocchio virtuale sono visualizzate in secondo piano [ 1 , 12 , 13 ]  . discussion risultati neurovascular conict syndrome is due to abnormal contact between cranial nerves and arterial or venous vessels , causin tutti i pazienti operati , la simulazione virtuale pre - chiradiol med ( 2013 ) 118 : 10451054 1049 fig . 
 larteria cerebellare antero - inferiore ( freccia rossa ) impatta il prolo inferiore del nervo ( freccia nera ) ( a ) , immagine di sorgente sagittale 3d - tof . 
 ing an active cranial nerve dysfunction . the incidence of neurovascular conict is 4.5 / 100 , 000 / year for trigeminal neuralgia [ 14 ] , 0.8 / 100 , 000 / year for hemifacial spasm [ 15 ] and for 0.8 / 100 , 000 / year for glossopharyngeal neuralgia [ 6 ]  . several factors , congenital or acquired , can determine the development of an abnormal contact between cranial nerves and vessels , such as the small size of the posterior fossa , elongation of the arteries and the aging - related brain sag phenomenon characterised by a progressive downward displacement of the nervous structures [ 9 ]  . the repeated pulsation of the offending vessel damages the myelin sheath of the nerve . 
damage to the insulating coating leads to direct contact between neurites , with the genesis of an ephaptic synapse , a short circuit in which the impulses proceed towards the periphery and the centre of the nerve . 
the generation of potential ectopic action in the sensory root of the nerve may be responsible for the typical , episodic , electric , lancinating pain of trigeminal neuralgia [ 4 ]  . mri has a fundamental role in the neuroradiological diagnosis of neurovascular conict . 
larteria cerebellare antero - inferiore ( freccia rossa ) impatta il vii nervo cranico in corrispondenza della rez ( freccia gialla ) ( a ) , immagine di sorgente assiale 3d - tof . 
visualizzazione obliqua anteriore dellimpatto ( d ) ( v : vaso ; rez : root exit zone )  . ing tools for assessing the anatomical relationships between cranial nerves and vessels within the cisternal spaces of the skull base . 
the source images , acquired in the axial plane , are routinely postprocessed with multiplanar reconstruction ( mpr ) with good sagittal , coronal and oblique reformatting [ 13 , 10 , 11 , 16 ]  . 
new possibilities are related to virtual mr techniques , such as 2d fusion imaging and cisternography , which have profoundly changed the diagnostic approach to neurovascular conicts [ 12 ]  . in the present study , these advanced virtual mri techniques were used to presurgically simulate microvascular decompression in patients with neurovascular conict syndromes . 
il dan neggiamento del rivestimento isolante del nervo determina la formazione di un contatto diretto tra i neuriti , con la geradiol med ( 2013 ) 118 : 10451054 1051 fig . 
sca ( red arrow ) impacts the upper prole of the nerve ( black arrow ) ; aica ( yellow arrow ) impacts the lower prole of the nerve ( black arrow ) ( a ) , sagittal 3d - tof source image . 
4a - e conitto a sandwich tra arteria cerebellare antero - inferiore ( aica ) e arteria cerebellare superiore ( sca ) v nervo cranico in paziente con nevralgia trigeminale . 
larteria cerebellare superiore ( freccia rossa ) impatta il prolo superiore del nervo ( freccia nera ) ; larteria cerebellare antero - inferiore ( freccia gialla ) impatta il prolo inferiore del nervo ( freccia nera ) ( a ) , immagine di sorgente sagittale 3d - tof . 
larteria cerebellare superiore ( freccia rossa ) e larteria cerebellare antero - inferiore ( freccia gialla ) sono visibili ( b ) , immagine di fusione sagittale ciss - tof . 
in patients with trigeminal neuralgia , nesi di una efapsi , un vero e proprio corto circuito elettrico in cui gli impulsi nervosi procedono verso la perife ria e il centro della struttura nervosa . 
la genesi di po tenziali di azione ectopici nel contesto della radice sensitiva del nervo pu essere responsabile del dolore tipico , episodico , elettrico e lancinante della nevralgia trigeminale [ 4 ]  . la rm svolge un ruolo fondamentale nella diagnosi neuroradiologica di conitto neuro - vascolare . 
le sequenze 3d - ciss e 3d - tof possono essere modernamente considerate come strumenti di imaging tradizionale per determinare i rapporti anatomici tra i nervi cranici e le strutture vascolari nel contesto degli spazi cisternali della base cranica . 
larteria cerebellare superiore ( freccia rossa ) impatta il prolo superiore del nervo che appare distorto ( freccia nera ) ( a ) , immagine di sorgente coronale 3d - tof . 
 visualizzazione dallalto dellimpatto ( d ) ( n : nervo ; v : vaso )  . radiol med ( 2013 ) 118 : 10451054 ratterizzate da alta risoluzione spaziale e di contrasto . 
le immagini di sorgente acquisite sul piano assiale vengono normalmente rielaborate mediante ricostruzioni multiplanari ( mpr ) , con buona riformattazione secondo i piani sagittale , coronale e obliquo [ 13 , 10 , 11 , 16 ]  . le tecniche virtuali di rm , quali la fusione di immagine bidimensionale e la cisternograa , hanno profondamente modicato lapproccio diagnostico al conitto neuro - vascolare [ 12 ]  . 
nel presente studio , queste tecniche virtuali avanzate di rm sono state utilizzate in fase pre - operatoria per simulare lintervento di decompressione microvascolare in pazienti con sindrome da conitto neuro - vascolare . 
 in tutti i pazienti abbiamo ottenuto una chiara denizione del contatto tra il nervo cranico e la struttura vascolare responsabile della compressione con unottima correlazione con i rilievi intra - operatori . 
hanno studiato 10 pazienti con nevralgia del trigemino e 7 pazienti con emispasmo facciale e hanno dimostrato una buona cor . rispondenza tra le immagini rm pre - operatorie e i risul tati post - chirurgici . 
nei pazienti con nevralgia del trigemino , gli autori hanno dimostrato un contatto patologico sca - nervo in 2 / 10 pazienti ( 20% ) e un contatto a sandwich in 2 / 10 pazienti ( 20% )  . 
hanno studiato 12 pazienti con nevral gia trigeminale , mostrando un contatto patologico con la sca in 8 / 12 casi ( 66 , 6 ) , con laica in 1 / 12 casi ( 8 , 4% ) e la presenza di compressioni multiple in 3 / 12 casi ( 25% ) [ 13 ]  . 
 in conclusione , lindagine rm , la cui sensibilit appare radiol med ( 2013 ) 118 : 10451054 1053 they demonstrated a pathological sca - nerve contact in 6 / 10 patients ( 60% ) , aica - nerve contact in 2 / 10 patients ( 20% ) and a sandwich contact in 2 / 10 patients ( 20% )  . 
in patients with hemifacial spasm , they showed pica - nerve contact in 5 / 7 patients ( 71.4% ) , and aica - nerve contact in 2 / 7 patients ( 28.6% ) [ 1 ]  . 
studied 12 patients with trigeminal neuralgia , showing a pathological contact with sca in 8 / 12 patients ( 66.6% ) , with aica in 1 / 12 patients ( 8.4% ) , and multiple compressions in 3 / 12 patients ( 25% ) [ 13 ]  . in conclusion , mri examination , implemented with virtual techniques , can be considered an optimal tool for the neurosurgeon , as it is able to simulate the surgical approach and limit cerebellar injury by predicting the position of critical structures such as the petrosal vein , the vertebral artery or the cerebellar occulus [ 10 ]  . 
the ability to view this complex anatomical region in a coloured image increases , in our opinion , the diagnostic condence in patients affected by this functional pathology [ 1 , 1113 ]  . incrementata dalle tecniche virtuali , pu essere considerata strumento ideale per il neurochirurgo , in grado di simulare lapproccio chirurgico e limitare il possibile danno cerebellare , individuando in via preventiva la posizione di strutture critiche come le vene petrosali , larteria ver tebrale o il occulo cerebellare [ 10 ]  . 
in questo caso , infatti , la scarsa rappresentazione di liquor cefalo - rachidiano pu essere responsabile di una navigazione difcile nel contesto delle cisterne con una non chiara denizione dei rapporti anatomici tra nervi cranici e vasi . 
per converso , la tecnica di fusione di immagine tra sequenze 3d - ciss e 3d - tof sembra dimostrarsi pi maneggevole , anche per radiologi non esperti o per i clinici . 
 la possibilit di visualizzare la complessa regione anatomica in questione in immagini colorate automaticamente , secondo il nostro parere , aumenta la sicurezza diagnostica nellapproccio al paziente con conitto neuro - vascolare [ 1 , 1113 ] conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
ma ( co - eds . ) springer , heidelberg , dordrecht , london , new york , 2012 isbn : 978 - 3 - 642 - 11494 - 6 e - isbn : 978 - 3 - 642 - 11495 - 3 published online : 25 july 2013 springer - verlag 2013 when a patient is informed by his urologist / physician that he is affected by prostate cancer , he is confronted with the numerous treatment at his disposition . they include surgery and external - beam radiation as utilized in the past ; intensity modulated radiation therapy , brachytherapy ( low and high dose rate ) , laparoscopic or robotic prostatectomy , cryoablation , high intensity focused ultrasound , and , recently the latest radiosurgery or stereotactic body radiation therapy ( cyberknife system )  . some of the above radiation regimens involve a daily session schedule lasting for many weeks and are not devoid of toxicities ( to seminal vesicles , testicles , bladder , and rectum ) ; surgery requires anaesthesia and a hospital stay . 
esse includono la chirurgia e la terapia radiante esterna , come utilizzate in passato ; la terapia radiante ad intensit modulata , la brachiterapia ( a bassa ed alte dosi ) , la prostatectomia laparoscopica o robotica , la crioablazione , lecograa focalizzata ad alta intensit e , recentemente , la radiochirurgia o terapia radiante corporea stereotactica ( sistema cyberknife )  . alcuni dei regimi di trattamento con radiazioni prevedono delle sedute giornaliere della durata di non poche settimane e non sono scevri da tossicit ( a vescicole seminali , testicoli , vescica e retto ) ; la chirurgia richiede unanestesia ed un ricovero ospedaliero . 
al contrario la radiochirurgia offre ipofrazionamento della dose e piano di terapia della durata di 5 o di un solo giorno , essendo inoltre indolore per il paziente . uno dei principali problemi del cancro della prostata rappresentato dalla mobilit sia del paziente che della prostata durante il trattamento : da ci deriva un conseguente non corretto carico di radiazioni a tessuti ed organi circostanti . al contrario la radiochirurgia , mediante luso di reperi inseriti accuratamente nella prostata , controllati e localizzati continuamente mediante la ripresa con immagini durante la somministrazione della dose , permette una precisa localizzazione e conseguente eradicazione del tumore nello stadio t1 e t2 . 
consequently , over time , the frequency of detected pulmonary emboli has signicantly increased . the typical prevalence of the ct pulmonary angiography ( ctpa ) is 1 positive ct exam per 20 performed and the incidence of isolated sspe is between 5%15% , depending on the population investigated . until today , the treatment is substantially the same for large , central emboli and for small , peripheral sspe . 
on the other hand , every year , 3% of treated patients develop a major bleeding event , requiring medical care ( cerebral haemorrhage , gastrointestinal bleeding or bleeding following trauma )  . an increasing number of investigators dont think that treating all these small emboli in the pulmonary arteries is worth the risk of bleeding due to treatment . 
di conseguenza , negli ultimi anni , notevolmente aumentata la frequenza di embolia polmonare rilevata nel corso di indagini diagnostiche . la prevalenza di embolia polmonare ( ep ) nelle angio - tc polmonari ( ctpa ) di un esame positivo ogni 20 eseguiti e lincidenza di epss isolata tra il 5% ed il 15% , a seconda della popolazione in esame . attualmente il trattamento dellembolia polmonare sostanzialmente lo stesso sia per i grandi emboli centrali sia per i piccoli epss periferici . 
daltra parte , ogni anno , il 3% dei pazienti trattati sviluppa un evento di sanguinamento maggiore , con necessit di cure mediche ( emorragia cerebrale , emorragia gastrointestinale o sanguinamento a seguito di traumi )  . un crescente numero di autori non ritiene necessario il trattamento di questi piccoli emboli polmonari periferici proprio a causa dellaumentato rischio di sanguinamento secondario al trattamento stesso . 
in altre parole , il punto : 902 radiol med ( 2013 ) 118 : 901908 massive emboli were found intra vitam [ 3 ] and the disease was considered nearly always fatal , with a mortality estimate ranging from 30% to 80% . 
 the development of progressively more effective therapies and the introduction of modern imaging techniques ( initially ventilation - perfusion scan , then spiral ct , that superseded scintigraphy as the most used imaging modality to assess for suspected pulmonary embolism about ten years ago ) corresponded to a decrease in mortality rate to less than 3% , but the therapeutic success was probably overrated , because the treated emboli changed from those detected on the basis of clinical ndings ( large , central ) to those detected using ctpa . 
their view was famously anticipated by a classical paper by robin in 1977 with the evocative title : overdiagnosis and overtreatment of pulmonary embolism : the emperor may have no clothes [ 4 ]  . a number of radiological studies , both prospective and retrospective , assessed the prevalence of pulmonary embolism , previously unsuspected and incidentally detected on routine spiral ct exams [ 57 ]  . 
among the patients with cancer , about 10% had ct unsuspected emboli , and 30% of these emboli were not reported at the time of initial reading [ 7 ]  . 
 [ 8 ] found incidental pulmonary emboli in 4% of oncology patients undergoing ct , with a higher prevalence among patients with gynaecological malignancies and those with melanoma . asymptomatic deep venous thrombosis ( dvt ) has also been reported during cancer staging . 
 [ 9 ] , for example , reported a 3.3% incidence of unsuspected pe and found that incidental dvt was present in 8% of patients undergoing staging pelvic ct . in cancer patients , the presence of unsuspected sspe , not associated with any symptoms or clinical and laboratory specic parameters , as demonstrated by oconnell et al . 
on the contrary , unsuspected pe involving major vessels have poorer prognosis , with a long - term mortality rate similar to that of symptomatic pe patients [ 11 ]  . 
there remains , however , the question of whether the sspe represents an early manifestation of hypercoagulable state , which is associated with an increased tutti gli emboli polmonari sono uguali ? possiedono tutti le stesse caratteristiche ? qual lembolo che necessita di essere trattato per prevenire nuovi episodi o il decesso ? un tempo , nel periodo precedente la terapia anticoagulante , solo le embolie massive venivano scoperte in vita [ 3 ] e la malattia era considerata molto spesso fatale , con una stima della mortalit variabile dal 30% all80% . lo sviluppo di terapie sempre pi efcaci e lintroduzione di moderne tecniche di imaging ( inizialmente la scintigraa ventilo - perfusionale , quindi la tc spirale , che ha superato da una decina danni la scintigraa come modalit di imaging pi utilizzata nella valutazione della sospetta ep ) , hanno portato ad una riduzione del tasso di mortalit a meno del 3% , ma il successo terapeutico probabilmente sovrastimato poich si passati dal trattare solamente gli emboli rilevati sulla base dei dati clinici ( emboli centrali e di grandi dimensioni ) , al trattare tutti gli emboli rilevati con la ctpa . le considerazioni suddette hanno recentemente indotto prasad et al . 
la loro visione stata notoriamente anticipata da uno storico articolo di robin del 1977 , dal titolo suggestivo : sovradiagnosi e sovratrattamento dellembolia polmonare : limperatore potrebbe essere nudo [ 4 ]  . numerosi studi radiologici , sia prospettici sia retrospettivi , hanno valutato la prevalenza di embolia polmonare non sospettata e rilevata incidentalmente in indagini tc di routine [ 57 ]  . 
lembolia come reperto incidentale stata riscontrata nell1 , 5%3 , 4% dei casi , soprattutto nei soggetti di et oltre 60 anni , con una prevalenza ospedaliera dal 4% al 5% e prevalenza ambulatoriale dallo 0 , 6% al 2 , 2% . in base allesperienza di farrell et al . 
 [ 8 ] hanno trovato emboli polmonari incidentali nel 4% degli studi tc di pazienti oncologici , con una maggiore prevalenza tra pazienti con tumori ginecologici e con melanoma . anche la trombosi venosa profonda ( tvp ) asintomatica viene spesso riscontrata durante le stadiazioni oncologiche . 
 [ 9 ] , ad esempio , hanno osservato una incidenza del 3 , 3% di ep non sospettata ed hanno scoperto che la tvp incidentale era presente nell8% dei pazienti sottoposti a stadiazione pelvica tc . nei pazienti con cancro , la presenza di epss di riscontro occasionale , non associata ad alcuna sintomatologia n a parametri clinico - laboratoristici specici , come dimostrato da oconnell et al . 
al contrario , embolie polmonari inciradiol med ( 2013 ) 118 : 901908 dentali che coinvolgono rami maggiori hanno una prognosi peggiore , con una mortalit a lungo termine che si avvicina a quella dei pazienti con embolia sintomatica [ 11 ]  . 
 [ 10 ] , non vi unopinione condivisa sulla necessit di trattamento delle epss asintomatiche in pazienti con cancro [ 12 ] , bench in questi pazienti il rischio di sanguinamento maggiore secondario alla terapia anticoagulante possa essere superiore a quello di unembolia polmonare . le epss sono piuttosto comuni anche nei pazienti non oncologici [ 13 ] e possono presentarsi isolatamente , in assenza di difetti di riempimento centrali o di maggiori dimensioni ( probabilmente il 5% di tutte le ep rilevate [ 2 ] )  . 
 nel 1993 gurney [ 14 ] si chiese : se gli emboli di piccole dimensioni sfuggono allangiograa polmonare , quali sono le conseguenze per il paziente ? e nel 2005 goodman [ 15 ] aggiunse che non sempre chiaro se lep di piccole dimensioni , in assenza di trombosi venosa profonda , giustichi il costo , la mortalit e la grave morbilit associate alla terapia anticoagulante . la fleischner society [ 16 ] ha poi osservato che la rilevanza clinica delle piccole ep periferiche e la necessit di somministrare anticoagulanti in tali casi rimangono un argomento di dibattito . 
dopo lintroduzione della ctpa , lincidenza di ep aumentata a 112 , 3 casi ogni 100000 abitanti ( aumento dell81% ) e la mortalit si leggermente ridotta a 11 , 9 casi ogni 100000 , ma le complicanze emorragiche dovute ad anticoagulanti sono passate da 3 , 1 a 5 , 3 casi ogni 100000 abitanti ( aumento del 71% )  . 
 nel complesso , lintroduzione della ctpa stata associata con una crescente incidenza di ep e solo una minima variazione della mortalit ( peraltro non signicativa )  . queste osservazioni sembrano dimostrare lesistenza di una importante quota di sovradiagnosi ( cio riscontro di emboli clinicamente irrilevanti )  . 
 [ 10 ] , there is no shared opinion on the need for treatment of asymptomatic sspe in cancer patients [ 12 ] , even though in these patients the risk of bleeding due to anticoagulation may outweigh the risk of fatal pulmonary embolism . sspe are rather common even in non - cancer patients [ 13 ] and can occur in isolation , in the absence of central or larger lling defects ( probably 5% of all detected pe [ 2 ] )  . in 1993 gurney [ 14 ] asked : if small emboli are missed at pulmonary angiography , what are the consequences for the patient ? and in 2005 , goodman [ 15 ] stated that : it is not always clear whether small pe , in the absence of deep venous thrombosis , justify the expense , mortality and serious morbidity associated with anticoagulation . the fleischner society [ 16 ] added that the clinical relevance of small peripheral pe and the need to administer anticoagulants in such cases remain a subject of debate . the clinical evidence was recently analysed by wiener et al . 
all in all , the introduction of ctpa 904 radiol med ( 2013 ) 118 : 901908 was associated with a rising incidence of pe and a minimal change in mortality ( not signicant )  . these observations seem to demonstrate the existence of a signicant component of overdiagnosis ( i.e. , nding clinically unimportant emboli )  . 
for example , a person with discharge diagnosis codes for pe and intracranial haemorrhage could have been admitted with primary intracranial bleeding and developed a pe as a complication of the hospitalisation . nevertheless , evidence that overdiagnosis represents a real problem continued to increase . in a retrospective review of their experience , suh et al . 
 [ 21 ] reported on the prevalence of pe , lower extremity dvt and anticoagulation therapy of 50 patients , selected from 1273 consecutive ctpas performed over a 6 - month period . 
the authors concluded that we need further studies to determine the signicance of such dots , considering the risk of anticoagulation , because the risk can outweigh the benets . another problem not easy to resolve is the high ctpa interobserver variability for sspe diagnosis with ctpa , which is greatly inuenced by the level of experience of the radiologist [ 22 ]  . 
 [ 23 ] in a study involving radiologists with different experience showed that 11% of ctpas with an initial diagnosis of sspe , re - interpreted by a highly experienced thoracic radiologist , were later proved negative . 
therefore , many of the sspe diagnosed with ctpa may be actually false positive results , due to a misinterpretation of the operator , to motion artefacts or to poor opacication of the vessel . 
 [ 24 ] state that all ctpa scans positive for isolated sspe should be reviewed by an experienced thoracic radiologist as a second opinion . besides , not only the presence but also the number , size and position of the emboli and the whole clinical scenario should be taken into due consideration . in some cases , isolated sspe without dvt could be even considered a para - physiological , incidental nding , to be left alone . 
ad esempio , una persona con codici di dimissione per diagnosi di ep ed emorragia intracranica avrebbe potuto essere stata ricoverata per una iniziale emorragia intracranica ed aver sviluppato successivamente una ep come complicanza durante il ricovero . tuttavia , levidenza che la sovradiagnosi rappresenti un problema reale continua a crescere . in una revisione retrospettiva della loro esperienza , suh et al . 
 [ 21 ] hanno riportato la prevalenza di ep , tvp degli arti inferiori e terapia anticoagulante di 50 pazienti , selezionati tra 1273 ctpa consecutive eseguite nel corso di un periodo di 6 mesi . 
dei 50 pazienti con ctpa positiva , 17 ( 34% ) avevano dots , cio piccole e periferiche epss , con unestensione del coagulo minimale e senza alcun segno di tvp . 
gli autori hanno concluso che sono necessari ulteriori studi per determinare limportanza di tali dots , considerando il rischio della terapia anticoagulante , poich i rischi possono superare i beneci . un altro problema di non facile soluzione quello dellelevata variabilit interosservatore nella diagnosi di epss alla ctpa , che notevolmente inuenzata dal livello di esperienza del radiologo [ 22 ]  . 
 [ 23 ] in uno studio che coinvolgeva radiologi con diversa esperienza , hanno evidenziato che l11% delle ctpa con diagnosi iniziale di epss , reinterpretate da un radiologo toracico con elevata esperienza , si sono poi rivelate negative . 
pertanto , molte delle epss diagnosticate alla ctpa potrebbero essere in realt dei falsi positivi dovuti ad un errore di interpretazione delloperatore , ad artefatti da movimento o a scarsa opacizzazione del vaso . 
 [ 24 ] affermano che tutte le ctpa positive per epss isolata dovrebbero essere reinterpretate da un radiologo toracico esperto , sotto forma di consulto interno o second opinion . inoltre , non solo la presenza , ma anche il numero , la dimensione e la posizione degli emboli , oltre allintero scenario clinico , dovrebbero essere presi in debita considerazione . in alcuni casi , epss isolate , senza tvp , potrebbero essere considerate reperti incidentali parasiologici e non essere trattate . goodman [ 15 ] ha osservato infatti che una normale funzione del letto capillare polmonare quella di ltrare piccoli grumi di sangue per proteggere la circolazione sistemica . 
 perci , come possiamo determinare quali pazienti con piccole ep dovrebbero essere trattati ? tapson [ 25 ] ha suggerito che in questi casi lo studio degli arti inferiori potrebbe probabilmente essere utile . 
questo autore ha riconosciuto che la sovradiagnosi di ep un fenomeno reale , ma ha dichiarato che probabile che un sottogruppo di pazienti con ep incidentale tragga comunque benecio dalla terapia . lep acuta potrebbe essere in realt un fenomeno sia soradiol med ( 2013 ) 118 : 901908 monary capillary bed is to lter small clots to protect the systemic circulation . 
so , how do we determine which patients with small pe should be treated ? tapson [ 25 ] suggested that examining the legs would likely be useful in these cases . 
the authors concluded that the shift in imaging from scintigraphy to ctpa resulted in increased diagnosis of a less fatal spectrum of emboli , raising the possibility of over diagnosis . 
 of course , these conclusions dont take into consideration other important factors , such as the ct capability to offer an alternative diagnosis in patients with acute chest pain ( e.g. , aortic dissection ) , which clearly is not in the realm of scintigraphy . 
a retrospective study revealed that ctpa , performed for a clinical suspicion of acute pe , showed other clinically relevant ndings , requiring immediate and specific intervention , in 27.5% of cases [ 27 ]  . 
benet - to - risk ratios were calculated by dividing the mortality benet of preventing a fatal pe by the risk of radiation - induced cancer from the ct scan . 
of course , the benet - to - risk ratio could be and probably will be decreased very soon by further optimising the radiation dose delivery , due to technology evolution . 
nella loro esperienza , dal 2000 al 2007 , lincidenza di ep aumentata da 0 , 69 a 0 , 91 casi ogni 100 ricoveri , in forte correlazione con lutilizzo maggiore della ctpa . 
non vi stato alcun cambiamento nella mortalit , ma il tasso di casi fatali diminuito dal 5 , 7% al 3 , 3% . in media , gli emboli letali rilevati con la ctpa erano la met di quelli diagnosticati con la scintigraa . 
gli autori hanno concluso che il passaggio nel campo dellimaging dalla scintigraa alla ctpa ha portato ad un aumento di diagnosi di uno spettro meno fatale di emboli , aumentando cos la possibilit di sovradiagnosi . ovviamente , queste conclusioni non tengono in considerazione altri fattori importanti , come la capacit della tc di offrire una diagnosi alternativa nei pazienti con dolore toracico acuto ( es . : dissezione aortica ) , che chiaramente non ottenibile con la scintigraa . 
uno studio retrospettivo ha dimostrato che la ctpa eseguita in pazienti con sospetta ep acuta , nel 27.5% dei casi evidenziava altri reperti clinicamente rilevanti che necessitavano di un intervento immediato e specico [ 27 ]  . lesposizione a radiazioni della tc si progressivamente ridotta , ma ancora superiore a quella della scintigraa . 
 il rapporto rischio - benecio stato calcolato dividendo il benecio sulla mortalit dato dalla possibilit di prevenire un ep fatale con il rischio di cancro indotto dalle radiazioni della scansione tc . 
sia i pazienti ricoverati che i pazienti del pronto soccorso hanno mostrato tassi signicativamente pi elevati di ep rispetto a pazienti ambulatoriali ( rispettivamente 14% e 14 , 5% versus 6 , 8% )  . 
gli uomini hanno ricevuto una dose di radiazioni signicativamente superiore rispetto alle donne ( 9 , 7 vs 8 , 4 msv ) , ma gli uomini hanno unaspettativa di vita signicativamente pi bassa rispetto alle donne , con ridotta mortalit per cancro attribuibile alle radiazioni . 
 [ 28 ] hanno concluso che , a seconda di molteplici fattori , quali dati anagraci del paziente e la dose di radiazioni erogata , i beneci dellutilizzo della ctpa per sospetta ep variano da 25 a 187 volte i rischi . inoltre , i rischi secondari alla diagnosi ed al trattamento dellep devono essere confrontati con il rischio della mancata diagnosi e del non - trattamento . 
questi rischi sono certamente difcili da stimare , in quanto dipendono da molteplici fattori , variano da caso a caso e dovrebbero essere valutati su base individuale [ 29 , 30 ]  . 906 radiol med ( 2013 ) 118 : 901908 ment . 
these risks are certainly difcult to estimate , as they depend on multiple factors , but they vary by case and should be evaluated on an individual basis [ 29 , 30 ]  . 
 [ 31 ] suggested withholding treatment of sspe , after fully informing patients , provided that ( a ) pulmonary reserve is good ; ( b ) there is no evidence of dvt on serial testing ; ( c ) major risk factors for pe are no longer present ; ( d ) there is no history of central venous catheterisation or atrial brillation ; ( e ) there is a willingness to return for serial venous ultrasound . under these conditions , patients diagnosed with isolated sspe have favourable 3 - month outcomes with a recurrence rate < 1% and no pe - attributed deaths . 
d - dimer testing is also less sensitive for sspe versus segmental or larger emboli ( 76% sensitivity versus 98% ) [ 32 ] ; this implies that many symptomatic patients with a negative d - dimer result may actually be affected from isolated sspe . 
given that the combination of a negative d - dimer result and a non - high pre - test probability can , with reasonable safety , exclude a major pe without the use of ctpa , a greater use of these diagnostic algorithms is likely going to reduce the overdiagnosis of sspe . considering the absence of prospective data demonstrating the benets of treating sspe and the risks associated with anticoagulant therapy , the results of the ongoing clinical trial [ 1 ] are expected in the scientic community to determine if and how patients with symptomatic sspe should be treated . another potential future direction of research could be the proposal of a model of multiparametric scoring for symptomatic isolated sspe based on the integration of the ctpa results with other clinical and laboratory parameters ( d - dimer , doppler lower limbs , pao2 , signs of right heart overload on echocardiography ) in order to identify the categories of patients who can really benet from a specic therapy . in conclusion , the availability of modern ctpa obviously simplies the diagnosis but it creates new , previously unknown problems . 
 single - photon emission computed tomography ( spect ) , ventilation - perfusion scintigraphy and magnetic resonance ( mr ) may play a major role in the near future but the diagnosis of sspe requires a very high spatial resolution and probably will remain a ct diagnosis . besides , based on prospective investigation of pulmonary embolism diagnosis ( pioped ) ii data ( sensitivity 83% , specicity 96% ) [ 34 ] , at a disease prevalence of approximately 5% , the number of false positive patients approaches the number of true positive ctpa studies for the detection of acute pe , and this problem is probably even nel frattempo , stein et al . 
 [ 31 ] hanno suggerito di sospendere il trattamento in caso di epss , dopo aver pienamente informato i pazienti , nel caso in cui sussistano : ( a ) una buona riserva funzionale polmonare ; ( b ) nessuna evidenza di tvp nelle indagini di controllo ; ( c ) nessun fattore di rischio maggiore per ep ; ( d ) non storia di cateterismo venoso centrale o di brillazione atriale ; ( e ) disponibilit del paziente a ritornare per un controllo mediante ecograa venosa . in queste condizioni , i pazienti con diagnosi di epss isolata hanno un outcome favorevole a 3 mesi , con un tasso di recidiva < 1% e assenza di decessi attribuibili alla ep . 
anche il test del d - dimero meno sensibile per lepss rispetto alle embolie segmentarie o maggiori ( 76% di sensibilit rispetto al 98% ) [ 32 ] ; ci implica che un certo numero di pazienti sintomatici ma con d - dimero negativo potrebbero in realt essere affetti da epss isolata . 
dal momento che la combinazione di un test del d - dimero negativo e una probabilit pre - test non alta possono con ragionevole sicurezza escludere una ep maggiore senza ricorrere alla ctpa , un maggiore utilizzo di questi algoritmi diagnostici auspicabile per ridurre la sovradiagnosi di epss . 
 considerando lassenza di dati prospettici che dimostrino i beneci del trattamento delle epss ed i rischi legati alla terapia anticoagulante , i risultati dello studio in corso [ 1 ] sono attesi della comunit scientica , per determinare se e come i pazienti con epss sintomatica debbano essere trattati . unaltra possibile futura direzione della ricerca potrebbe essere quella di proporre un modello di scoring multiparametrico per le epss sintomatiche isolate che preveda lintegrazione del dato ctpa con altri dati clinico - laboratoristici ( d - dimero , eco - doppler arti inferiori , pao2 , segni di sovraccarico del cuore destro allecocardiograa ) allo scopo di individuare le categorie di pazienti che possano realmente beneciare di una terapia specica . in conclusione , la disponibilit della moderna ctpa , ovviamente , semplica la diagnosi , ma crea nuovi problemi , in precedenza sconosciuti . 
la necessit di ulteriori informazioni ovvia , perch molte domande relative allep acuta e in particolare allepss isolata risultano ancora senza risposta . tomography ( spect ) , la scintigraa ventilo - perfusionale e la risonanza magnetica ( rm ) possono giocare un ruolo importante nel prossimo futuro , ma la diagnosi di epss richiede una risoluzione spaziale molto alta e probabilmente rimarr una diagnosi esclusiva della tc . single - photon emission computed inoltre , sulla base dei dati dello studio prospective investigation of pulmonary embolism diagnosis ( pioped ) ii ( 83% sensibilit , specicit 96% ) [ 34 ] , con una prevalenza di malattia di circa il 5% , il numero degli studi ctpa per il rilevamento di ep acuta che risultano falsi positivi si avvicina molto a quello dei veri positivi e questo problema probabilmente ancora pi importante in caso di epss . 
 [ 2 ] at the end of their article , rightly stated that pe captures all the complexity of medicine in the evidence - based era . they argue ( and we agree ) that outcome - based clinical trials with long - term follow - up would be helpful to further guide management but trial funding should move away from industry - sponsored studies , which continue to test triviality , alluding to the raging debate regarding the so called disease mongering [ 36 ] , one of the greatest problems of the modern medicine . 
regarding response to stereotactic radiotherapy , we recorded one ( 6% ) complete response ( cr ) , six ( 37% ) partial responses ( pr ) , ve ( 32% ) stable disease ( sd ) and four ( 25% ) local failures . 
scopo di questo lavoro valutare la tossicit acuta e il controllo locale nel trattamento di pazienti sottoposti a radioterapia stereotassica extracranica ( sbrt ) per lesioni metastatiche paracardiache e cardiache , denite come tali se localizzate entro 1 cm dal cuore o nel contesto del suo parenchima materiali e metodi . 
per quanto concerne la risposta alla radioterapia stereotassica , stata registrata 1 ( 6% ) risposta completa ( cr ) , 6 ( 37% ) risposte parziali ( pr ) , 5 ( 32% ) stabilit di malattia ( sd ) e 4 ( 25% ) progressioni locali . 
 keywords cardiac metastases paracardiac metastases oligometastases stereotactic body radiotherapy radiotherapy parole chiave metastasi cardiache metastasi paracardiache oligometastasi radioterapia stereotassica radioterapia 1056 introduction the occurrence of lung metastases represents an unfavourable event that takes place in up to one third of all patients affected by malignant neoplasms [ 1 ]  . 
when systemic disease is diagnosed , chemotherapy is the mainstay of treatment : on the whole , it exerts an impact on prognosis that is highly dependent on tumour histotype and cancer biological behaviour , but most patients gain little or no improvement in terms of long - term survival [ 2 ]  . 
 however , in the last two decades in the oncological community , many attempts have been made to try to single out metastatic patients who might theoretically benet from a more aggressive , multimodal approach [ 3 ]  . 
however , it is still a matter of debate as to how to properly stage and dene an oligometastatic patient ( how many sites of involvement or how many lesions should be present at the same time )  . 
 in this framework , in the context of secondary lung lesions , two main therapeutic nonsurgical approaches have been brought forward next to or mostly as an alternative to metastasectomy : stereotactic body radiotherapy ( sbrt ) and radiofrequency ablation ( rfa )  . 
by denition , extracranial sbrt delivers a high biologically effective dose ( bed ) to a small target , ultimately aiming at ablation of tumour cells with minimal toxicity to the surrounding normal tissue . 
growing evidence is accumulating on the great potential of improved therapeutic index inherent to this radiation technique , particularly in the setting of early - stage primitive lung cancers and lung metastases [ 4 ]  . 
on the other hand , some experiences have raised concern on the safe use of sbrt for central lesions [ 5 ] , the latter generally being dened as targets placed within 2 cm of the proximal bronchial tree , critical mediastinal vascular structures and vertebral bodies [ 6 ]  . 
at the present time , no denite indications exist on how to safely irradiate central lung metastases with sbrt , especially when target lesions are in close proximity to the heart or within its wall . 
 in this dual - institution ( santa chiara radiotherapy unit and azienda ospedaliero universitaria careggi radiotherapy unit , university of florence ) , retrospective analysis , we report our experience with patients who underwent sbrt for paracardiac and cardiac metastatic lesions , dened as such when located at a maximum distance of 1 cm from the heart or inside its parenchyma , in order to evaluate acute toxicity and local control ( lc )  . 
 radiol med ( 2013 ) 118 : 10551065 introduzione la comparsa di metastasi polmonari rappresenta un evento sfavorevole nella storia naturale di circa un terzo dei pazienti affetti da neoplasia maligna [ 1 ]  . 
nel momento in cui la malattia viene diagnosticata in fase sistemica , la chemioterapia la principale arma terapeutica : nel complesso , essa esercita un impatto sulla prognosi dei pazienti che altamente dipendente dallistotipo tumorale e dal comportamento biologico della neoplasia in atto , ma sfortunatamente la maggior parte dei pazienti non ottiene beneci sensibili per quanto concerne la sopravvivenza a lungo termine [ 2 ]  . 
nelle ultime 2 decadi , tuttavia , nella comunit oncologica si cercato di individuare , nellambito di pazienti con malattia metastatica , situazioni nelle quali potesse derivare un benecio , perlomeno teorico , da un approccio terapeutico multimodale pi aggressivo rispetto alla sola terapia sistemica [ 3 ]  . 
in tal senso , veniva riconosciuta la presenza di uno stato di malattia oligometastatica , implicante la presenza di una patologia con un grado di diffusione sistemica ancora limitato ; ancora oggi motivo di dibattito , tuttavia , quali possano essere i criteri pi adeguati per denire un paziente oligometastatico ( quanti organi debbano essere coinvolti in uno stesso momento o che numero massimo di lesioni debbano essere contemporaneamente presenti )  . 
la radioterapica stereotassica extracranica ( sbrt ) una tecnica in grado di erogare unelevata dose biologica efcace ad un target di piccole dimensioni , in ultima istanza con lobiettivo di eradicare le cellule tumorali e di esporre ad una tossicit minima il tessuto sano circostante . 
numerose evidenze hanno dimostrato la possibilit di ottimizzare lindice terapeutico con questa tecnica , particolarmente nellambito di tumori primitivi polmonari in fase precoce e di metastasi polmonari [ 4 ]  . 
daltro canto , alcune esperienze hanno evidenziato potenziali criticit nellutilizzo di sbrt per lesioni centrali [ 5 ] , questultime denite come target localizzati entro una distanza di 2 cm dallalbero bronchiale prossimale , dalle strutture vascolari mediastiniche e dai corpi vertebrali [ 6 ]  . 
attualmente , non sono disponibili indicazioni denite su come irradiare con sbrt in maniera sicura le metastasi radiol med ( 2013 ) 118 : 10551065 materials and methods sbrt technique : planning and delivery computed tomography ( ct ) scans were acquired with a 16 - slice ct scanner in helical modality ( lightspeed 16 ge medical systems , wi , usa ) at three different breathing phases : a noncontrast free - breathing acquisition with 3.75 - mm slice thickness , and two contrast - enhanced scans ( 2.5 - mm slice thickness ) at end - exhale and end - inhale . 
patients were trained to keep a shallow physiological breathing cycle , and thresholds for ct scan acquisitions were set using an active breathing coordinator spirometer ( abc elekta , crawley , uk )  . 
the gross tumour volume ( gtv ) was contoured using the information from both scans in order to obtain an internal target volume ( itv ) [ 8 ] ; no margins were added from the gtv to the clinical target volume ( ctv )  . 
 for patients treated at the santa chiara radiotherapy unit , a treatment plan was created on the end - exhale ct scan employing a dynamic arc technique ( ergo planning system , elekta ) : coplanar arcs were shaped by means of a dynamic external micro - multileaf collimator ( micro - mlc ) with a 5 - mm leaf width at the isocenter ( elekta )  . 
a negative leaf margin for ptv conformation was usually employed to allow prescription to isodoses lower than 90% , and an inverse optimisation module ( amoa ) was used when necessary to reduce doses to oars . 
for patients treated at the careggi radiotherapy unit , a plan with ve to seven noncoplanar beams was created on the end - exhale ct scan using the pinnacle treatment planning system ( philips , version 8.0 m ) , and a collapsed cone convolution type of algorithm was performed for dose calculation . 
as for dosage specication , in 15 of 16 patients , the prescription dosage was 36 gy in three fractions ( 70% isodose ; 17.14 gy per fraction at the isocenter )  . 
 materiali e metodi tecnica sbrt : planning e delivery le scansioni di tomograa computerizzata ( tc ) sono state acquisite in modalit elicoidale mediante un multidetettore tc a 16 strati ( lightspeed 16 ge medical systems , wi , usa ) in 3 differenti fasi del respiro : unacquisizione a respiro libero , senza mezzo di contrasto , con uno spessore di 3 , 75 mm ; 2 scansioni ( spessore di 2 , 5 mm per strato ) con mezzo di contrasto acquisite in fasi di espirio ed inspirio . 
i pazienti sono stati istruiti a mantenere un pattern respiratorio siologico e sono state determinate speciche soglie del respiro per lacqusizione tc mediante lutilizzo di uno spirometro abc ( active breathing coordinator ; abc elekta crawley , regno unito )  . 
il gross tumor volume ( gtv ) stato contornato utilizzando le informazioni di entrambe le scansioni tc per ottenere un internal target volume ( itv ) [ 8 ] ; non stata effettuata unespansione tra gtv e clinical target volume ( ctv )  . 
chiara , stato prodotto un piano di trattamento sulla tc in espirio utilizzando una tecnica ad arco dinamico ( ergo planning system , elekta crawley , regno unito ) : archi coplanari sono stati conformati mediante lausilio di un micro multileaf collimator ( mlc ) esterno con unapertura di 5 mm per lamella allisocentro ( elekta crawley , regno 1058 radiol med ( 2013 ) 118 : 10551065 isocenter )  . 
the heart dosimetric features are summarised in table 1 . image - guided radiotherapy before each fraction , a kilovolt cone - beam ct ( cbct ) was acquired for correcting patient setup and tumour position using the xvi system implemented on the synergy linear accelerator . 
un margine negativo a livello lamellare stato solitamente adottato per la conformazione del ptv per consentire prescrizioni ad isodosi inferiori al 90% , ed un modulo di ottimizzazione inversa ( amoa ) stato utilizzato quando necessario per ridurre le dosi agli oars . 
 heart dmax ( gy ) heart dmean ( gy ) heart v30gy ( cc ) heart irradiated volume ( cc ) distance ptv - heart ( mm ) apatient with cardiac lesion ptv , planning target volume ; v30gy , heart voluime receiving a dosage of 30 gy tabella 1 caratteristiche dosimetriche cardiache paziente no . 
as a second step , tumour positioning was checked and corrections performed when necessary according to manual alignment between the cbct tumour image and the planned itv [ 7 ]  . clinical examination , follow - up and evaluation of toxicity and response patients were evaluated until disease progression after completion of sbrt to the paracardiac and cardiac metastases using the response evaluation criteria in solid tumors ( recist ) on a thorax ct or positron emission tomography ( pet )  . 
a thorough cardiological examination including echocardiography was performed on the day before treatment and on the last day of therapy , and subsequently , clinical and cardiological follow - up were scheduled at 1 , 3 , 6 and 12 months after the end of treatment . 
survival and control times were calculated from the end of sbrt . results patient characteristics between january 2009 and may 2011 , 16 patients with paracardiac and cardiac lesions were treated with sbrt at the university of florence in two different institutions : seven patients were planned and treated at the santa chiara radiotherapy unit and nine at the azienda ospedaliera universitaria careggi radiotherapy unit . 
median age of the patient population was 67.1 ( range , 3781 ) years ; median follow - up was 6.5 months ( range , 3 months to 2.3 years ) ; 15 of 16 patients had paracardiac lesions and one patient a cardiac lesion . 
the latter was a 73 - year - old patient previously operated on for a well - differentiated brosarcoma of the achilles tendon in 2009 who underwent a thorax ct scan in february 2011 , which revealed the presence of suspicious bilateral lung nodules . 
a following uorodeoxyglucose positron emission tomography ( fdg - pet ) scan conrmed ct ndings , showing a pathological uptake of tracer at two distinct nodules in the left lung ( one in the upper lobe and the other in the lower lobe ) and a smaller one in the right upper lobe : all three nodules were located peripherally in the lung parenchyma and were all subsequently treated with sbrt . 
 moreover , a sharp area of hypermetabolism was seen at the to con 57 fasci non coplanari sono strati elaborati sulla base della tc in espirio mediante il sistema di treatment planning pinnacle ( philips , version 8.0 m ) ed un algoritmo di tipo collapsed cone convolution stato adottato per il calcolo della dose . 
per quanto concerne la dose erogata , in 15 pazienti su 16 la dose di prescrizione stata di 36 gy in 3 frazioni ( allisodose del 70% ; 17 , 14 gy per frazione allisocentro )  . 
in un paziente la lesione target era localizzata nel contesto del parenchima cardiaco , e la dose prescritta stata pari a 30 gy in 3 frazioni ( allisodose del 70% ; 14 , 28 gy per frazione allisocentro )  . 
le caratteristiche dosimetriche cardiache sono riassunte nella tabella 1 . radioterapia image guided prima di ciascuna frazione , stata acquisita una conebeam tc ( cbct ) a kv per la correzione del setup del paziente e della posizione tumorale utilizzando il sistema xvi implementato sullacceleratore lineare synergy ( elekta , crawley , regno unito )  . 
in secondo luogo , la posizione del tumore veniva controllata e venivano effettuate correzioni , se necessarie , secondo lallineamento manuale tra limmagine del tumore alla cbct e litv pianicato [ 7 ]  . 
 valutazione clinica , follow - up ed analisi di tossicit e risposta al trattamento i pazienti sono stati valutati , una volta completato il trattamento sbrt sulle metastasi paracardiache e cardiache , sino a progressione di malattia . 
la valutazione della risposta stata elaborata in base ai response evaluation criteria in solid tumors ( recist ) mediante esame tc torace o tomograa ad emissione di positroni ; la rivalutazione mediante imaging stata eseguite non prima di 2 mesi dal completamento della radioterapia e preferibilmente a 3 mesi da essa . 
valutazioni cardiologiche approfondite , comprendenti esame ecocardiograco , sono state effettuate il giorno precedente allinizio del trattamento , in coincidenza dellultimo giorno di terapia e susseguentemente i controlli clinici e cardiologici di follow - up sono stati stabiliti a distanza di 1 , 3 , 6 e 12 mesi dalla ne del trattamento . 
il fallimento a distanza stato denito in base allo 1060 radiol med ( 2013 ) 118 : 10551065 sviluppo di nuove metastasi e / o di progressione di metastasi non trattate in pazienti sottoposti a sbrt . 
gli intervalli di sopravvivenza e controllo di malattia sono stati calcolati dalla ne della sbrt . risultati caratteristiche dei pazienti fra gennaio 2009 e maggio 2011 , sono stati trattati con sbrt 16 pazienti affetti da lesioni paracardiache e cardiache presso luniversit di firenze in 2 differenti istituti : 7 pazienti sono stati pianicati e trattati presso lunit di radioterapia s . 
let mediana della casistica stata di 67 , 1 anni ( range 3781 anni ) ; il follow - up mediano di 6 , 5 mesi ( range 329 mesi ) ; 15 pazienti su 16 presentavano una lesione paracardiaca mentre 1 paziente aveva una lesione cardiaca . 
in questultimo caso si trattava di un paziente di 73 anni , precedentemente sottoposto ad intervento chirurgico di asportazione di un brosarcoma ben differenziato del tendine dachille , che era stato sottoposto ad un esame tc torace a febbraio 2011 con riscontro di noduli polmonari bilaterali di natura sospetta . 
un successivo esame in tomograa ad emissione di positroni ( pet ) con uorodesossiglucosio ( fdg ) confermava il sospetto dei reperti tc mostrando una captazione patologica del radiofarmaco a livello di 2 distinti noduli nel polmone sinistro ( uno nel lobo superiore ed un altro nel lobo inferiore ) ed un altro nodulo di dimensioni minori nel lobo superiore destro : tutti e 3 i noduli erano localizzati perifericamente nel parenchima polmonare e sono stati sottoposti a trattamento con sbrt . 
tutti i pazienti trattati erano oligometastatici : sono stati deniti come tali i pazienti caratterizzati dalla presenza di massimo 5 lesioni in non pi di due organi , al tempo del trattamento radioterapico ; la malattia primitiva era stata precedentemente asportata chirurgicamente o era stabile al momento della sbrt . 
2 risonanza magnetica cardiaca ( immagini in t2 ) che conferma la presenza di lesione metastatica di 15 mm localizzata nella parete anterosettale del ventricolo sinistro nel foglietto subepicardico . radiol med ( 2013 ) 118 : 10551065 1061 table 2 patient characteristics tabella 2 caratteristiche dei pazienti feature patients , n ( % ) caratteristiche pazienti , n ( % ) gender male female age ( years ) mean range primary tumour lung colon - rectum liver kidney soft tissue interval from primary diagnosis to paracardiac metastases ( months ) median range 12 ( 75 ) 4 ( 25 ) 67.1 3781 8 ( 50 ) 5 ( 32 ) 1 ( 6 ) 1 ( 6 ) 1 ( 6 ) 53.8 0138 sesso maschi femmine et ( anni ) media range tumore primario polmone colon - retto fegato rene tessuti molli intervallo tra la diagnosi iniziale e la comparsa di metastasi paracardiache ( mesi ) media range 12 ( 75 ) 4 ( 25 ) 67 , 1 3781 8 ( 50 ) 5 ( 32 ) 1 ( 6 ) 1 ( 6 ) 1 ( 6 ) 53 , 8 0138 the main series features are reported in table 2 . 
a clinical decision was taken on an individual - patient basis to evaluate whether all or most disease sites were amenable to sbrt , taking into account the feasibility of the treatment , the performance status of the patient and the availability of other therapeutic options , such as chemotherapy . 
one patient was disease free after > 2 years from sbrt of a solitary lung paracardiac metastasis , whereas in two cases , the oligometastatic burden of disease remained stable . 
regarding response to sbrt , we recorded one ( 6% ) complete response ( cr ) , six ( 37% ) partial responses ( pr ) , ve ( 32% ) stable disease ( sd ) , and four ( 25% ) local failures . 
a mild , clinically irrelevant , pericardial effusion ( pce ) was o la maggior parte dei siti di malattia fossero candidabili a sbrt , tenendo conto della fattibilit del trattamento , del performance status del paziente e della disponibilit eventuale di altre opzioni terapeutiche quali la chemioterapia . 
 outcome clinico complessivamente , la casistica dei pazienti in esame stata seguita in follow - up per un tempo mediano di 6 , 7 mesi ( range 329 )  . 
nella quasi totalit dei pazienti trattati , si sviluppata , successivamente alla sbrt , progressione a distanza di malattia ; un paziente libero da malattia dopo oltre 2 anni dal trattamento stereotassico di una metastasi solitaria paracardiaca , mentre in 2 casi la diffusione oligometastatica di malattia rimasta stabile . 
per quanto concerne la risposta al trattamento stereotassico , abbiamo registrato una ( 6% ) risposta completa , 6 ( 37% ) risposte parziali , 5 ( 32% ) stabilit di malattia e 4 ( 25% ) fallimenti locali . 
per quanto riguarda la tossicit , la compliance al trattamento stata ottimale ; nella nostra casistica nessun paziente ha sviluppato sintomi di natura cardiologica n ha presentato alterazioni signicative elettrocardiograche o ecocardiograche , anche a mesi di distanza da sbrt . 
abbiamo osservato un caso di esofagite g2 a 10 giorni dal trattamento con completa regressione della sintomatologia dopo appropriata terapia antinammatoria discussione stato ampiamente dimostrato che sbrt rappresenta un approccio terapeutico non invasivo ed efcace se impiegata per lesioni periferiche a livello polmonare : il suo utilizzo quale alternativa allintervento chirurgico stato dimostrato in pazienti affetti da tumori polmonari primitivi in stadio precoce non operabili per comorbilit ed elevati tassi di risposta sono stati riportati a confronto di quanto ottenibile mediante radioterapia a frazionamento standard [ 10 ]  . 
daltro canto , lutilizzo di radioterapia ipofrazionata per target centrali , siano essi tumori polmonari primitivi o lesioni secondarie , devessere preso in considerazione con cautela , dal momento che rimangono incertezze circa la esatta tolleranza ad alte dosi di radioterapia degli organi a rischio localizzati nella cosidetta no - y zone . 
 [ 11 ] , i quali hanno affermato che i tassi di controllo locale e sopravvivenza sono migliori con una dose biologica efcace ( bed ) 100 gy ( considerando un rapporto alfa / beta di 10 ) rispetto a valori < 100 gy . 
abbiamo selezionato questa schedula di frazionamento in quanto , come indicato in altri lavori [ 12 ] , una dose biologica efcace superiore ai 100 gy uno dei parametri pi importanti nellottenere un incremento in termini di controllo locale . 
 [ 6 ] hanno trattato 70 pazienti affetti da lesioni polmonari primitive periferiche e centrali con una dose totale di 60 / 66 gy allisodose dell80% , erogate in 3 frazioni , con intento radicale . 
 stata registrata una differenza sostanziale in termini di assenza di tossicit severa ( 83% vs 54% a 2 anni , rispettivamente ) in dipendenza della posizione del target : nei pazienti con lesioni centrali , un danno rilevante alle vie aeree stato registrato in 8 pazienti con tossicit g3 / g4 e 5 pazienti sono deceduti in conseguenza della tossicit subita . 
3 tc - pet di rivalutazione post - sbrt che evidenza captazione aspecica del tracciante fdg nel ventricolo sinistro , con completa scomparsa del nodulo metastatico . seen in one patient at echocardiography at 3 months and disappeared at subsequent follow - up examinations . 
 discussion it has been extensively shown that sbrt is an effective , noninvasive therapeutic approach when used for peripheral lesions in the lungs : robust evidence has validated its use as a possible alternative to surgery in patients affected by early - stage lung tumours not amenable to operation due to comorbid conditions , and high response rates are reported compared with data obtained with standard fractionated radiotherapy [ 10 ]  . 
on the other hand , the use of hypofractionated radiotherapy for central targets , whether primary lung tumours or secondary lesions , must be considered with caution , as tolerance to high - dose radiation of organs at risk lying in the so - called no - y zone remains uncerta the effect of dose escalation or fraction size is important for local control , as reported in a review by onishi et al . 
 [ 11 ] , who showed local control and survival rates were better with a bed 100 gy ( alpha / beta of 10 ) compared with < 100 gy . 
we chose this schedule beradiol med ( 2013 ) 118 : 10551065 1063 cause , as indicated by other published data [ 12 ] , a bed > 100 gy is one of the most important parameters by which to obtain an increase in local control . 
 [ 6 ] treated 70 patients with both peripheral and central primary lung lesions to a total dose of 60 / 66 gy to 80% isodose delivered in three fractions with radical intent . 
 [ 13 ] reported a case of a 75 - year - old man with a pulmonary artery sarcoma , recurrent after surgical resection , treated with cyberknife stereotactic radiosurgery , resulting in clinical and radiographic complete remission . 
 [ 14 ] reviewed clinical data of the oslo and stockholm trials on postoperative radiotherapy in women affected by early breast cancer : they provided a quantitative description of the doseresponse relationship for excessive cardiac mortality found in the two cohorts as a result of heart irradiation . 
according to the authors opinion , this would mean that to reduce the probability of long - term cardiac damage , it would be more important to decrease the dose to the heart than to restrict the irradiated volume . 
as for sbrt , additional work is clearly needed to evaluate the potential impact of high - dose , hypofractionated radiotherapy on the heart [ 18 ] , and further observation is required to correlate the dose to subvolumes of the heart to potential late consequences , such as valvular abnormalities and coronary artery disease ( cad ) [ 19 ]  . 
 [ 13 ] hanno riportato il caso di un paziente di 75 anni con un sarcoma dellarteria polmonare recidivato dopo resezione chirurgica e trattato mediante radiochirurgia cyberknife con successiva evidenza di remissione completa clinica e radiologica . 
 [ 14 ] hanno effettuato una review dei dati clinici relativi ai trials di oslo e stoccolma sulla radioterapia post - operatoria in donne affette da neoplasia mammaria in stadio precoce : hanno fornito una descrizione quantitativa della relazione dose - risposta per leccessiva mortalit cardiaca riscontrata nelle 2 coorti di pazienti come risultato dellirradiazione collaterale del cuore . 
secondo lopinione degli autori , questo dato potrebbe signicare che per ridurre la probabilit di un danno cardiologico a lungo termine , potrebbe essere pi rilevante mirare a ridurre la dose al cuore piuttosto che minimizzare il volume irradiato . 
lincidenza di versamento pericardico era del 27 , 7% ( 28 pazienti su 101 ) ed il tempo mediano per la comparsa di tale alterazione era di 5 , 3 mesi ( range 116 , 7 ) dopo il trattamento radiante . 
nessuno dei fattori clinici analizzati stato riscontrato essere in grado di inuenzare signicativamente il rischio di versamento pericardico post - attinico ; allanalisi multivariata la v30 cardiaca veniva selezionato come unico parametro signicativamente associato con tale evento avverso . 
per quanto concerne sbrt , studi aggiuntivi sono chiaramente necessari per valutare il potenziale impatto sul cuore di un trattamento radioterapico ipofrazionato a dosi elevate [ 18 ] ed ulteriori dati sono richiesti per correlare la dose depositata su subvolumi dellorgano cardiaco a potenziali conseguenze tardive , quali patologie valvolari e vasculopatie coronariche [ 19 ]  . 
 nella nostra casistica , 16 pazienti affetti da lesioni cardiache o paracardiache sono strati trattati con sbrt ed in nessun caso stato riscontrata la presenza di sofferenza cardiaca valutata clinicamente o mediante ecocardiogramma ; solo in un caso si sviluppata unesofagite g2 , regredita prontamente mediante terapia medica , ed in nessun caso si sono avute complicanze acute polmonari . 
per quanto concerne lefcacia del trattamento , il controllo locale 1064 radiol med ( 2013 ) 118 : 10551065 in our series , we treated 16 patients with cardiac or paracardiac lesions , and in none of them was heart discomfort seen ( clinically or with echocardiography ) after treatment ; only one patient experienced grade ii acute oesophagitis , with prompt recovery after medical therapy , and none developed pulmonary side effects . 
sbrt represents a valid option for treating metastatic lesions , even those in close proximity to the heart , as shown in our series where the mean distance of ptv from the pericardium was 1.8 mas observed in other experiences [ 20 , 21 ] , satisfactory local control might translate into improved survival . 
 limitations of our study are the retrospective nature of the analysis and the need for longer follow - up in order to evaluate late toxicity as well , specically in terms of adverse cardiac events . 
nevertheless , we think our data are encouraging in terms of efcacy and feasibility regarding the use of high - dose radiotherapy in this difcult situation where the target volume is in close proximity to the heart . 
 our treatment intent was palliative , but we believe that oligometastatic patients might truly benet from low - toxicity , aggressive local therapies in terms of disease control . risultato essere pari al 75% . 
sbrt pu rappresentare una valida opzione per trattare lesioni metastatiche , anche se estremamente vicine al cuore , come dimostrato nella nostra esperienza in cui la distanza media del ptv dal pericardio pari a 1 , 8 mcome dimostrato in altri lavori [ 20 , 21 ] , un controllo locale di malattia soddisfacente pu tradursi in un miglioramento della sopravvivenza . 
 i limiti del nostro studio sono costituiti dalla natura retrospettiva dellanalisi e dalla necessit di un maggiore tempo di osservazione in modo da poter valutare adeguatamente anche la tossicit tardiva , specicatamente in termini di eventi avversi cardiologici . 
ciononostante , riteniamo che i nostri dati siano incoraggianti in termini di efcacia e fattibilit in relazione alluso di radioterapia ad alte dosi in una situazione a rischio in cui il volume bersaglio paracardiaco . 
lintento del nostro trattamento stato palliativo , ma riteniamo che pazienti oligometastatici selezionati possano realmente beneciare in termini di controllo di malattia dallimpiego di terapie locali aggressive e con pochi effetti collaterali . 
 conclusions conclusioni results of our retrospective study show that sbrt represents a safe and effective option for treating cardiac and paracardiac metastases . i risultati del nostro studio retrospettivo mostrano che sbrt rappresenta una opzione sicura ed efcace nel trattamento di metastasi cardiache e paracardiache . 
of these , seven patients ( 44% ) were successfully treated with percutaneous drainage alone , whereas ve patients ( 31% ) required placement of a covered stent due to incomplete resolution of the collection . 
da giugno 2004 a gennaio 2010 , 16 pazienti con gl post sl sono stati trattati dal nostro teatutti i pazienti sono stati sottoposti a transito con mezzo di contrasto per os ( gastrogran ) e tomograa computerizzata ( ct )  . 
di questi in 7 ( 44% ) pazienti il drenaggio percutaneo stato lunico presidio terapeutico ; 5 pazienti ( 31% ) hanno richiesto stents per la mancata risoluzione del gl . 
dopo 1009 , 8456 , 7 giorni di follow - up : 1 paziente morto per evento cardiovascolare e 2 pazienti sono stati sottoposti a bypass bilio - pancreatico - digestivo . 
la presenza di sepsi corrobora questo approccio rispetto al tradizionale trattamento chirurgico . radiol med ( 2013 ) 118 : 962970 condition and in particular the presence of sepsis supports the value of this approach in preference to the conventional surgical approach . parole chiave fistola gastrica sleeve gastrectomy drenaggio percutaneo stent ricoperto trattamento non chirurgico keywords gastric leak sleeve gastrectomy percutaneous drainage stent graft non - surgical management introduction introduzione obesity is a leading problem in western countries , with a prevalence which increased by 1.1% between 2007 and 2009 [ 1 ]  . 
 laparoscopic sleeve gastrectomy ( sg ) is the most commonly used therapy for obesity , and gastric leak ( gl ) is one of the most frequent complications [ 3 ]  . 
 the denition of anastomotic leak has been provided by the uk surgical infection study group as the leak of luminal contents from a surgical join between two hollow viscera [ 4 ]  . 
a leak may also be an outow of gastrointestinal content through a suture line around an organ or a luminal content collection next to the anastomosis [ 7 ]  . 
leaks have been classied according to time of onset : early ( between the rst and third day after surgery ) , intermediate ( between the fourth and seventh day after surgery ) , late ( more than 8 days after surgery ) [ 4 ]  . 
 based on pathophysiology , gastric leak is related to a high value of intraluminal pressure that exceeds the resistance of the suture line , thereby causing the stula [ 8 ]  . 
 classic stulas tend to appear between 5 and 6 days after surgery , but when there is a mechanical - tissular cause , stulas are usually discovered within the rst 2 days after surgery [ 8 ]  . the typical location of gl is the proximal third of the stomach , close to the gastro - oesophageal junction : burgos et al . 
we report our experience with the nonsurgical treatment of gl , based on the patients eligibility for drainage placement . lobesit uno dei principali problemi dei paesi occidentali , con una prevalenza aumentata di 1 , 1% tra il 2007 e il 2009 [ 1 ]  . 
questi dati hanno portato alcuni studiosi a ipotizzare che nel 2050 gran parte degli americani probabilmente circa il 100% sar in sovrappeso [ 2 ]  . lintervento chirurgico laparoscopico di sleeve gastrectomy ( sg ) una delle tecniche pi utilizzate per la cura dellobesit e la stola gastrica ( gl ) una delle sue complicanze principali [ 3 ]  . 
una stola pu anche essere denita come perdita del contenuto gastrointestinale attraverso la linea di sutura intorno un organo o come una raccolta accanto alla anastomosi [ 7 ]  . 
le stole sono state classicate in base al tempo di insorgenza in : precoci ( tra la prima e la terza giornata post - operatoria ) , intermedie ( tra la quarta e la settima giornata post - operatoria ) e tardive ( oltre lottava giornata post - operatoria ) [ 4 ]  . dal punto di vista siopatologico , la stola gastrica dovuta ad un alto valore di pressione intraviscerale che supera la resistenza della linea di sutura causando perdita di materiale [ 8 ]  . 
le stole tendono a comparire tipicamente in quinta - sesta giornata post operatoria , ma nel caso di un danno meccanico - tissutale possibile identicare la stola anche in seconda giornata post operatoria [ 8 ]  . la tipica localizzazione del gl il terzo prossimale dello stomaco , a livello della giunzione gastro - esofagea : burgos et al . 
 [ 7 ] riportano una percentuale dll85 , 7% per le stole a livello del terzo prossimale dello stomaco e solo il 14 , 3% a livello del terzo distale dello stomaco ; stroh et al . 
 [ 9 ] riportano il 7% delle stole a livello della giunzione gastroesofagea . nonostante il gl aumenti la morbilit e la mortalit dei pazienti dopo sg , non stato ancora denito un consenso internazionale per il management del gl . 
riportiamo 964 materials and methods patient population radiol med ( 2013 ) 118 : 962970 la nostra esperienza nel trattamento non chirurgico di gl , incentrato principalmente sulla possibilit di utilizzare il drenaggio come trattamento di scelta . this retrospective study was conducted with institutional review board approval with waiver of informed consent . 
 from july 2004 to december 2010 , 16 patients ( three male , 13 female ; mean age , 437 years ) with gl following sg were referred to our department . 
all patients underwent clinical examination both before and 3 , 6 , 12 months after sg ; after the rst year post sg , a yearly visit is strongly recommended but not compulsory . 
ct scan , with oral contrast medium ( gastrogran ) was used to conrm the contrast swallow ndings , determine the size and the number of collections , and to guide the percutaneous drainage procedure , if required . 
sepsis was dened as fever > 38c and elevated inammation markers ( white cell count , creactive protein and erythrocyte sedimentation rate ) ; tachycardia conrmed the presence of sepsis . 
 patients eligible for percutaneous drainage were treated with flexima ( boston scientic , natick , ma , usa ) and malecot ( cook medical , limerick , ireland ) catheters with a calibre between 10 f and 14 f , depending on the size of the abdominal collection . 
the percutaneous drainage procedures were performed under ct and uoroscopy guidance , materiali e metodi popolazione di pazienti questo studio di tipo retrospettivo stato condotto con lapprovazione del comitato di revisione del nostro istituto ( irb )  . 
nel periodo da luglio 2004 a dicembre 2010 , 16 pazienti ( 3 maschi , 13 femmine , et media 437 anni ) con gl post - sg , sono stati trattati dalla nostra unit operativa . 
tutti i pazienti avevano effettuato un esame clinico prima e dopo 3 , 6 e 12 mesi post - sg ; dopo il primo anno post - sg , una visita annuale altamente raccomandata ma non obbligatoria . valutazione del gl il gl stato denito come perdita di mezzo di contrasto ( gastrogran ) evidenziato con rx dellapparato digerente . 
 la tomograa computerizzata ( ct ) con mezzo di contrasto ( gastrogran ) per os , stata poi utilizzata per confermare la stola , per determinare la dimensione e il numero di raccolte e per guidare il drenaggio percutaneo , se necessario . 
la sepsi stata denita come febbre > 38c e aumento degli indici della inammazione ( globuli bianchi , proteina c - reattiva e velocit di sedimentazione eritrocitaria ) ; la tachicardia ha confermato la presenza di sepsi . management dei pazienti tutti i pazienti sono stati indirizzati al team di nutrizionisti dellobesity unit del nostro ospedale . 
patients not responding to drainage were treated with a covered stent ( wallex fully covered esophageal stent , boston scientific , natick , ma , usa ) , placed at the level of the stula , as shown in figure 3 . sono state : la mancanza di un sicuro tramite percutaneo no alla raccolta e pazienti non collaboranti . 
controindicazioni relative sono state : coagulopatie , che hanno richiesto correzione con emoderivati prima della procedura , raccolta sterile e procedura con passaggio attraverso la pleura . i pazienti eleggibili a drenaggio percutaneo sono stati trattati con flexima ( boston scientic , natick , ma , usa ) e malecot ( cook medical , limerick , irlanda ) con un calibro compreso tra 10 e 14 f , a seconda della dimensione della raccolta addominale . 
associated conditions were diabetes mellitus ( 5 / 16 , 38% ) , hypertension ( 6 / 16 , 37% ) and obstructive sleep apnoea syndrome ( osas ) ( 5 / 16 , 31% )  . 
in 15 / 16 patients ( 94% ) the contrast leak was located at the gastro - oesophageal junction ; only one case ( 6% ) presented a leak in the mid - gastric region . all collections were located at the level of the left hypogastric region . 
la risoluzione del gl stata denita mediante uoroscopia con mezzo di contrasto per os come riduzione della dimensione / risoluzione di raccolta addominale o assenza di spandimento del mezzo di contrasto . 
i pazienti non - responder al drenaggio sono stati trattati con stent ricoperto ( wallex fully covered esophageal stent , boston scientic , natick , ma , usa ) posizionato a livello della stola , come mostrato in figura 3 . risultati popolazione di pazienti nella tabella 1 sono riassunte le caratteristiche della nostra popolazione di pazienti prima di sg . 
in 3 / 16 ( 19% ) patients , the leak was associated with bleeding , and in 1 / 16 ( 7% ) with haematemesis . patient management twelve / 16 ( 75% ) patients required a single percutaneous drainage , whereas 2 / 16 ( 13% ) required two percutaneous drainages because of two different noncommunicating abdominal collections . 
in 15 / 16 pazienti ( 94% ) il gl era localizzato a livello della giunzione esofago - gastrica , solo in un caso ( 6% ) stata evidenziata la stola a livello della regione medio - gastrica . tutte le raccolte erano localizzate a livello dellipogastrio sinistro . 
in 3 / 16 ( 19% ) pazienti la stola era associata a sanguinamento e un paziente ( 1 / 16 , 7% ) ha presentato ematemesi . management del paziente dodici / 16 ( 75% ) pazienti hanno richiesto il drenaggio percutaneo , mentre in due pazienti ( 2 / 16 , 13% ) sono stati necessari due drenaggi percutanei a causa di due raccolte addominali non comunicanti tra loro . 
tra i pazienti eleggibili per drenaggio percutaneo : cinque ( 5 / 12 , 42% ) presentavano stola precoce ( range 17 giorni ) di cui 3 ( 3 / 5 , 60% ) febbrili e sette ( 7 / 12 , 58% ) presentavano stola tardiva ( range 1130 giorni )  . 
il drenaggio stato la sola procedura terapeutica in 7 pazienti ( 7 / 12 , 58% ; 7 / 16 , 43% ) che hanno presentato risoluzione della raccolta addominale ( n = 4 ) , valutati da ascessogramma con uoroscopia e sollievo dei sintomi ( n = 3 )  . 
percutaneous drainage proved to be a valid stand - alone procedure in seven patients ( 7 / 12 , 58% ; 7 / 16 , 43% ) , who achieved resolution of the abdominal collection ( n = 4 ) , as evaluated by uoroscopic abscessogram , and symptom relief ( n = 3 )  . 
five patients ( 5 / 12 , 42% ) required placement of a covered stent due to incomplete resolution of the abdominal collection ( n = 4 ) and worsening of symptoms ( n = 1 )  . 
one patient ( 1 / 16 , 6% ) needed a covered stent because he was unt for surgery and ineligible for drainage due to a small stula located on the posterior wall of the gastro - oesophageal junction . 
total parenteral nutrition was administered in ve patients and enteral nutrition in ve patients . no patient necessitated surgical re - intervention . other procedures one patient required double vascular embolisation for pseudoaneurysms due to pancreatitis . 
embolisation of the left gastro - epiplipoic artery was achieved with coils ( balt extrusion , montmorency , france ) whereas embolisation of the splenic artery required the use of coils and onyx 34 ( ev3 , micro - therapeutics inc , irvine , california , usa )  . follow - up after a mean follow - up of 1009.8456.7 days ( range , 5782001 days ) , we recorded the death of one patient due to cardiovascular failure . 
two patients necessitated a biliopancreatic - digestive bypass ( bpd - bp ) due to unchanged bmi : the rst patient had a bmi of 50 and the second of 51.5. 
 twelve patients ( 12 / 16 , 75% ) were in good health with a signicant reduction in bmi ( p < 0.05 ) and without any recurrence of stula ; additionally , one girl successfully completed a pregnancy . 
stato osservato un caso di migrazione dello stent che ha richiesto un riposizionamento ; non sono state evidenziate altre complicanze ( stent kinking , infezione stent ) nella nostra popolazione . 
la durata della permanenza dello stent oscillata tra 7 e 45 giorni con una durata media di 29 , 815 , 6 giorni . tre ( 3 / 16 , 19% ) pazienti , valutati come non idonei al drenaggio e / o non candidabili a stent , sono stati trattati con la sola terapia medica . 
nella nostra popolazione cinque pazienti sono stati sottoposti a nutrizione parenterale totale ( tpn ) e 5 pazienti a nutrizione enterale ( en )  . in nessun paziente stato necessario un successivo reintervento chirurgico . altre procedure in un paziente con pancreatite stata necessaria una doppia embolizzazione di pseudo - aneurismi . 
larteria gastroepiploica sinistra stata embolizzata con spirali ( estrusion balt , montmorency , francia ) mentre per larteria splenica stato utilizzato anche onyx 34 ( ev3 , micro - therapetics inc , irvine , california , usa )  . follow - up dopo un follow - up medio di 1009 , 8456 , 7 giorni ( range 5782001 giorni ) abbiamo registrato la morte di un paziente per evento cardiovascolare maggiore . 
due pazienti sono stati sottoposti a bypass bilio - pancreatico - digestivo ( bpdbp ) per mancata riduzione del bmi : primo paziente presentava bmi di 50 e secondo paziente di 51 , 5 . 
un paziente , con bmi iniziale di 55 , 5 , ha avuto un aumento di peso ( 15 kg / 3 mesi ) , ma ha riutato altri trattamenti . 
dodici pazienti ( 12 / 16 , 75% ) hanno presentato un buono stato di salute con una riduzione signicativa del loro indice di massa corporea ( p < 0 , 05 ) senza alcuna recidiva di stola ; inoltre una ragazza ha portato a termine la gravidanza . nella nostra popolazione il periodo di degenza media stato di 55 , 336 , 8 giorni , con un massimo di 134 giorni e un minimo di 7 giorni . discussione il gl uno delle pi frequenti complicanze della chirurgia bariatrica ed associato ad un aumento dei tassi di morbilit , mortalit e degenza ospedaliera [ 3 , 10 ]  . 
la gestione del gl ancora empirica e basata sullesperienza , dal momento che non esistono linee guida per il manageradiol med ( 2013 ) 118 : 962970 discussion gl is one of the most frequent problems complicating bariatric surgery and is associated with increased rates of morbidity , mortality , and prolonged hospital and intensive care unit stay [ 3 , 10 ]  . 
in the last few years , several authors have described their experience with the management of gl after sg but , to the best of our knowledge , nobody has proposed exclusively nonsurgical management . 
described a ow - chart algorithm for gl after sg based on a multidisciplinary approach considering time of leak onset ( early / late ) and patient condition ( sepsis / no sepsis ) [ 6 ]  . 
 [ 10 ] reported their experience with 16 patients with gl , who were treated with surgical therapy in the case of early leak and with medical management in the case of late leak . 
classic gl management can be summarised as follows : early stula ( < 3 days after surgery ) is eligible for a primary repair but a high percentage of recurrence is present [ 6 ] ; late stula can be managed conservatively by placing drainage and / or with parenteral or enteral nutrition , highdose proton pump inhibitors , and antibiotics . 
the defect could be closed using biological glue ( seamguard , tissucol , and brin sealant ) or a covered stent used as a temporary stula bypass [ 10 , 1217 ]  . in line with the literature , we used percutaneous drainage to treat seven late leaks as well as ve early leaks , because of the patients general condition . 
our algorithm for gl management is based on the patients eligibility for percutaneous drainage , because of the high rate of gl recurrence after a second surgical procedure [ 11 ]  . 
in our population , 75% of patients were eligible for drainage , and in more than half of the patients drainage placement proved to be a valid stand - alone procedure ; ve nonresponders to drainage therapy necessitated stent placement . 
our study was retrospective but the survival rate observed justies the enrolment of a larger number of patients in order to dene , prospectively , an algorithm for the nonsurgical management of gl . 
negli ultimi anni alcuni autori hanno descritto la loro esperienza nella gestione di gl , ma nessuno ha proposto una terapia esclusivamente nonchirurgica per la gestione di gl dopo sg . 
 [ 6 ] hanno descritto un algoritmo per il management del gl con un approccio multidisciplinare basato sul tempo di insorgenza della stola ( precoce / tardiva ) e sulle condizioni cliniche del paziente ( sepsi / non sepsi )  . 
la gestione classica del gl pu essere riassunta come segue : stola precoce ( < 3 giornata post operatoria ) pu beneciare di un re - intervento , gravato per da un alta percentuale di recidiva [ 6 ] ; stola tardiva sottoposta a terapia conservativa con drenaggio e / o nutrizione parenterale o enterale , alte dosi di inibitori della pompa protonica , e antibiotici . 
il gl pu essere passibile di riparazione con colla biologica ( seamguard , tissucol , colla di brina ) o stent ricoperto [ 10 , 1217 ]  . in linea con la letteratura , nella nostra popolazione di studio abbiamo trattato sette stole tardive con drenaggi percutanei , ma anche cinque pazienti con stola precoce sono stati sottoposti a drenaggio a causa della loro condizione generale . 
il nostro algoritmo per il management del gl basato sulleleggibilit del paziente al trattamento con drenaggio percutaneo , dato lalto tasso incidenza di recidiva dopo una seconda procedura chirurgica [ 11 ]  . 
nella nostra esperienza nessun paziente stato sottoposto ad altro intervento chirurgico per la gestione gl . i limiti del nostro studio sono legati alle piccole dimensioni del campione preso in esame e al disegno dello studio . 
 il nostro studio infatti di tipo retrospettivo , ma il tasso di sopravvivenza dei nostri pazienti incoraggia larruolamento di nuovi pazienti per denire prospetticamente un algoritmo per la gestione non chirurgica del gl . possiamo concludere che la gestione mini - invasiva di gl possibile e particolarmente utile nei pazienti con fattori di rischio chirurgico . 970 radiol med ( 2013 ) 118 : 962970 conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
twenty - ve patients ( 17 men , 8 women ) with 31 liver metastases > 3 cm or located near vessels ( > 3 mm ) were treated in a total of 29 sessions . 
follow - up was performed with computed tomography ( ct ) scan at 1 , 3 , 6 and 12 months after treatment ; mean follow - up period was 12.04 ( range , 336 ) months . 
percutaneous mwa of liver metastases > 3 cm or located near vessels ( > 3 mm ) can be considered a valid and safe option , probably preferable to rfa . 
lo scopo del nostro studio stato quello di valutare il successo tecnico , lefcacia e la sicurezza della ablazione con microonde ( mwa ) di metastasi epatiche inoperabili , nei casi in cui la radiofrequenza ( rfa ) presenta alcuni limiti . 
venticinque pazienti ( 17 uomini , 8 donne ) , con unet media di 65 , 9 anni ( range 4983 ) , sono stati sottoposti ad ablazione percutanea con microonde ( mwa ) eco - guidata di 31 metastasi epatiche con un diametro medio maggiore di 3 cm e / o situate in prossimit di grossi vasi ( diametro > 3 mm )  . 
i tumori erano cos suddivisi : metastasi da carcinoma del colon - retto ( n = 21 ) e metastasi da carcinoma non del colon - retto ( n = 10 )  . 
il followup stato eseguito con la tomograa computerizzata ( tc ) a 1 , 3 , 6 e 12 mesi dopo il trattamento ; il periodo medio di follow - up di 12 , 04 mesi ( range 336 mesi )  . 
la mwa percutanea di metastasi epatiche con diametro maggiore di 3 cm e / o localizzate in siti critici , in vicinanza di vasi di grosse dimensioni e / o di organi cavi , pu essere considerata una opzione valida e sicura , probabilmente preferibile alla rfa , in questi casi . 
over the years , various ablation techniques have been developed , including ethanol ablation , laser ablation , cryoablation and radiofrequency ablation ( rfa ) [ 47 ] ; the most widely used technique is radiofrequency ablation [ 8 ]  . 
factors that signicantly correlate with increased failure rates are metachronous occurrence of liver metastases , large mean lesion size and central tumour location [ 11 , 12 ]  . microwave ablation ( mwa ) therapy is a relatively new technique that can be applied to different types of tumours [ 13 ]  . 
comparing mwa and rfa , the size and shape of the mwa zone may be more consistent and less dependent on the heat - sink effect from vascular structures or large bile ducts in proximity of the lesion [ 13 , 14 ]  . 
 the aim of this study was to demonstrate the efcacy and safety of mwa to overcome the limits of rfa . materials and methods patients this was a prospective , nonrandomised controlled study . 
 ad oggi la chirurgia ancora il trattamento di scelta per le metastasi epatiche [ 1 ] , tuttavia solo il 20% delle lesioni , al momento della diagnosi , sono suscettibili di trattamento chirurgico [ 2 , 3 ]  . 
questo ha dirottato negli anni lattenzione verso tecniche alternative alla chirurgia , prime fra tutte le tecniche ablative , al ne di consentire un controllo locale di un tumore non pi resecabile ; ne sono state proposte diverse , lalcolizzazione , lablazione con laser , la crioablazione , lablazione con radiofrequenza ( rfa ) o con microonde ( mwa ) [ 47 ]  . 
la rfa si rivelata una opzione di trattamento promettente per le metastasi epatiche , sebbene il suo ruolo necessiti tuttora di essere stabilito con maggiore precisione ; gli studi disponibili dimostrano che la rfa pu essere molto utile , ma vi sono alcune considerazioni di cui tenere conto [ 7 ]  . 
le complicanze perie post - procedurali , seppur non frequenti ( 7 , 1%9 , 5% ) [ 9 , 10 ] , possono risultare gravi e richiedere un trattamento ; ci limita lutilizzo della rfa solo in centri specializzati . 
i principali fattori che inuiscono negativamente sul successo locale della rfa sono le dimensioni della lesione , il numero e la localizzazione di queste [ 11 , 12 ]  . 
 la termo - ablazione con mw invece una tecnica relativamente nuova , applicabile a differenti tipologie di neoplasie [ 13 ] , in grado di offrire tutti i beneci della rfa a cui sembrano aggiungersi alcuni vantaggi . 
al confronto con la rfa , la mwa determina delle aree di necrosi coagulativa pi uniformi e di maggiori dimensioni , meno sensibile allheat sink effect garantendo un risultato migliore nelle lesioni localizzate in prossimit dei vasi o dei dotti biliari di grosso calibro [ 13 , 14 ]  . le nostra serie interamente costituita da lesioni con diametro maggiore di 3 cm e / o localizzate in sedi critiche ; lobiettivo di questo studio quello di dimostrare lefcacia e la sicurezza della mwa nelle lesioni con queste caratteristiche e quindi la possibilit di superare i limiti della rfa . radiol med ( 2013 ) 118 : 949961 between may 2008 and september 2011 , 25 patients ( 17 men , 8 women ) , mean age 65.9 ( range , 4983 ) years , underwent percutaneous mwa of intraparenchymal liver metastases with a mean diameter of 3.7 ( range , 1.17 ) cm ( table 1 )  . 
distribution was as follows : 21 metastases from colorectal cancer , two from breast cancer , one from cancer of the pharynx , two from oesophagus carcinoma , one from retroperitoneal leiomyosarcoma , two from gallbladder carcinoma , one from renal cell carcinoma and one from pancreatic carcinoma . 
inclusion criteria were : absence of extrahepatic disease or stable extrahepatic disease for at least 3 months inoperable lesions tumour size ( > 3 cm ) lesions located near vessels ( with a diameter > 3 mm )  . one week prior to the ablation treatment , patients with materiali e metodi pazienti questo uno studio di tipo osservazionale retrospettivo non randomizzato . 
nel periodo compreso tra maggio 2008 e settembre 2011 , 25 pazienti ( 17 uomini , 8 donne ) con unet media di 65 , 9 anni ( range 4983 ) , sono stati sottoposti a mwa percutanea eco - guidata di 31 lesioni epatiche secondarie con un diametro medio di 3 , 7 cm ( range 1 , 17 ) ( tabella 1 )  . 
le 31 metastasi trattate erano cos suddivise : 21 metastasi da carcinoma del colon - retto , 2 metastasi da carcinoma della mammella , 1 da carcinoma della faringe , 2 da carcinoma dellesofago , 1 da leiomiosarcoma retroperitoneale , 2 da carcinoma della colecisti , 1 da carcinoma del rene , 1 da table 1 characteristic of patients and lesions ( maximum diameter , location , residual tumour and recurrence ) pt no . 
porta iv - vi 2 ; 2 3 ; 2 m , maschio ; f , femmina ; k , carcinoma ; v . , vena ; tc , tomograa computerizzata 30 ( no recidiva ) 36 ( no recidiva , progressione malattia ) 12 ( no recidiva ) 8 ( no recidiva ) 12 recidiva 12 ( no recidiva ) 12 ( no recidiva ) 8 ( no recidiva ) 8 recidiva 7 ( no recidiva ) 6 ( no recidiva ) 6 ( no recidiva , progressione malattia ) 6 ( no recidiva ) 6 ( no recidiva ) 14 ( no recidiva ) 18 ( no recidiva ) 12 ( no recidiva ) 27 ( no recidiva ) 24 ( no recidiva , progressione malattia ) 13 ( no recidiva , progressione malattia ) 8 ( no recidiva , progressione malattia ) 6 recidiva 4 ( no recidiva ) 3 ( no recidiva ) 3 ( no recidiva , progressione malattia ) metachronous metastases underwent percutaneous biopsy performed under ultrasound ( us ) guidance ( philips iu22 , best , the netherlands ) , with histological conrmation for all lesions . 
le principali indicazioni per linclusione al trattamento comprendevano : assenza di malattia extraepatica o malattia extraepatica stabile da almeno 3 mesi ; lesioni non trattabili chirurgicamente ; dimensioni del tumore ( diametro maggiore di 3 cm ) ; lesioni localizzate nelle adiacenze di grossi vasi ( diametro maggiore di 3 mm )  . nella settimana precedente il trattamento , tutti i pazienti sono stati sottoposti a biopsia percutanea sotto guida ecograca ( philips iu22 , best , paesi bassi ) con conferma istoradiol med ( 2013 ) 118 : 949961 logica di tutte le lesioni . 
i pazienti con metastasi sincrone suscettibili di mwa sono stati sottoposti a cicli di chemioterapia adiuvante ( i protocolli sono cambiati pi volte negli ultimi dieci anni ) dopo la procedura ; i pazienti con metastasi metacrone non sono stati uniformemente trattati con chemioterapia adiuvante ( 5 fu e leucovorin in combinazione con irinotecano e / o oxaliplatino )  . baseline imaging limaging pre - trattamento comprendeva lindagine in tomograa computerizzata ( tc ) multistrato addominale ( mdct , aquilon 64 , toshiba , giappone ) senza e con somministrazione di mezzo di contrasto ( mdc ) organo - iodato . 
ogni scansione tc stata acquisita con uno spessore di 0 , 5 mm , tensione di 120 kv , 250 ma , previa iniezione di 100 ml di mezzo di contrasto iodato ( visipaque 320 , ge healthcare , usa ) ad una velocit di 3 ml / s , seguita da iniezione di 40 ml di soluzione salina ad una velocit di 2 ml / s . trattamento pre - operatorio il prolo della coagulazione era nel range di normalit per tutti i pazienti . 
unadeguata prolassi antibiotica stata ottenuta mediante la somministrazione endovenosa di 1 g di cefazolina sodica ( ancef , smithkline beecham pharmaceuticals , philadelphia , usa ) , somministrata ogni 8 ore per tre giorni prima della procedura no a 2 giorni dopo . trattamento intraoperatorio prima dellinizio di ciascuna procedura stata eseguita unanestesia locale nella sede dingresso dellantenna attraverso iniezione sottocutanea di una soluzione di 10 ml al 2% di mepivacaina . 
ciascun paziente stato mantenuto in regime di sedazione moderata per tutta la durata del trattamento , condizione ottenuta mediante somministrazione endovenosa di propofol ( 0 , 52 , 0 mg / kg / h ) , alfentanyl ( 12 mg / kg ) e mydazolam ( 0 , 070 , 08 mg / kg )  . 
1 algoritmo per il trattamento delle metastasi epatiche non trattabili chirurgicamente [ 1 ]  . baseline imaging pretreatment imaging consisted of abdominal multidetectorrow computed tomography ( mdct ) ( aquilion 64 , toshiba , japan ) with and without contrast medium administration . 
the contrast - enhanced scans were acquired after injection of 100 ml of iodinated contrast agent ( visipaque 320 , ge healthcare , usa ) at an injection rate of 3 ml / s , followed by injection of 40 ml saline at a rate of 2 ml / s . preoperative treatment the coagulation prole was in the normal range for all patients . 
adequate antibiotic prophylaxis was achieved with intravenous administration of 1 g of cefazolin sodium ( ancef , smithkline beecham pharmaceuticals , philadelphia , pa , usa ) given every 8 h for 3 days before the procedure until 2 days afterwards . 954 intraoperative treatment local anaesthesia at the antenna entrance site was achieved with subcutaneous injection of a 10 - ml solution of 2% mepivacaine . 
in all patients , mwa was performed under moderate sedation , through intravenous administration of propofol ( 0.52.0 mg / kg / h ) , alfentanil ( 12 g / kg ) and midazolam ( 0.070.08 mg / kg )  . 
during the entire ablation session , patients were monitored by an anaesthesiologist . equipment imaging guidance the procedures were performed under us guidance ( philips iu22 , best , the netherlands )  . percutaneous microwave ablation procedure the ablation system consists of a microwave generator ( evidenttm mw ablation system , covidien ltd , usa ) capable of producing a power of 45 w at 915 mhz , connected by coaxial cable to a 14.5 - gauge straight microwave antenna with a total length of 12 or 17 cm ( vt 1237 and vt 1737 evidenttm mw ablation percutaneous antenna ) with a 3.7or 2 - cm radiating section . 
according to manufacturer specications , ablation was performed by inserting the antenna within the lesion and maintaining a power of 45 w for a total ablation time of 10 min in order to obtain the optimal necrosis volume . 
all lesions in our series , presenting a maximum diameter > 3 cm , were treated with two or three antennas simultaneously positioned at a distance of 1 cm from each other to achieve adequate necrosis ; in particular , lesions with a diameter between 3 and 4 cm were treated with two antennas and lesions with a diameter 4 cm with three antennas with cluster arrangement . follow - up follow - up was carried out by ct scan after 1 , 3 , 6 and 12 months in combination with complete blood and metabolic tests . 
local disease control was assessed on the basis of the lesions contrast enhancement ( ce ) : the absence of ce in the ablation zone indicated a complete response , the presence of a thin peripheral rim of ce with a thickness < 5 mm at follow - up > 3 months was radiol med ( 2013 ) 118 : 949961 equipaggiamento guida imaging le procedure sono state eseguite sotto guida ecograca ( philips iu22 , best , paesi bassi )  . procedura di ablazione percutanea con microonde il sistema di ablazione utilizzato include un generatore di microonde ( evidenttm sistema di ablazione a mw , covidien ltd . , usa ) in grado di produrre una potenza di 45 w / 915 mhz , collegato tramite cavo coassiale a unantenna di 14 , 4 g con una lunghezza totale di 12 o 17 cm ( antenna per mwa , vt 1237 e vt 1737 evidenttm , covidien ltd . , usa ) con una sezione radiante di 3 , 7 cm o 2 cle antenne sono state continuamente perfuse con una soluzione salina a temperatura ambiente ad una velocit di 60 ml / min , come indicato dalla casa costruttrice , al ne di prevenire eventuali danni termici . 
 il trattamento ablativo stato eseguito inserendo lantenna allinterno della lesione e mantenendo una potenza di 45 w per un tempo di ablazione totale di 10 minuti al ne di ottenere un volume di necrosi ottimale . 
tutte le lesioni della nostra serie con un diametro massimo superiore ai 3 cm sono state trattate ricorrendo a due o tre antenne simultaneamente , posizionate a una distanza di 1 cm luna dallaltra per ottenere una necrosi adeguata ; in particolare le lesioni con un diametro tra 3 e 4 cm sono state trattate con 2 antenne , le lesioni con diametro maggiore di 4 cm sono state trattate con 3 antenne posizionate con disposizione a cluster . follow - up tutti i pazienti sono stati sottoposti a follow - up mediante tc eseguita dopo 1 , 3 , 6 e 12 mesi dal trattamento in combinazione con indagini bioumorali complete . 
il controllo locale della malattia stato valutato mediante il contrast enhancement ( ce ) della lesione : lassenza di ce nella zona di ablazione indica una risposta completa , la presenza di un sottile margine periferico di ce con uno spessore < 5 mm al follow - up > 3 mesi stato considerato un segno negativo ( assenza di tessuto vitale ) , un ce focale irregolare stato considerato come un segno di malattia residua . 
il follow - up totale stato registrato in tutti i pazienti in un arco di tempo che va dalla data della procedura ( primo o secondo trattamento ) no allindagine tc pi recente . clinical outcomes : successo clinico , sopravvivenza libera da malattia , sicurezza ed efcacia della tecnica il successo tecnico stato denito come il corretto posizionamento delle antenne nel contesto della lesione . radiol med ( 2013 ) 118 : 949961 considered a negative sign ( absence of viable tissue ) and focal irregular ce was regarded as a sign of residual disease . 
the total follow - up was recorded in all patients over a period of time between the date of the procedure ( rst or second treatment ) until the most recent ct survey . clinical outcomes : technical success , disease - free survival , safety and efcacy technical success was dened as the correct positioning of the antennas within the lesion . disease - free survival ( dfs ) was dened as the length of time after treatment during which a patient survives with no sign of disease . safety was dened as the frequency of complications . 
major complications were dened as those that , if untreated , might threaten the patients life , lead to substantial morbidity and disability , result in hospital admission or substantially lengthen hospital stay , as described by the international working group on image - guided tumour ablation [ 16 ]  . 
complications were further divided into two causal categories : those secondary to mw antenna placement ( pneumothorax , infection and bleeding ) and those secondary to thermal injury ( damage to adjacent organs ) [ 17 ]  . 
moreover , values of laboratory tests ( white cell count , serum bilirubin , alkaline phosphatase , aspartate aminotransferase , alanine aminotransferase ) were evaluated before and after the ablation session . efcacy of the technique was dened on the basis of the percentage of tumour recurrence . 
local recurrence was dened as the presence of viable tissue around ( < 5 mm ) and / or in the context of the treated nodule at ct performed at least after 3 months . 
 the total follow - up period was recorded in all patients as the time from the date of the procedure ( rst or second treatment ) to the most recent ct scan . statistical analysis la sopravvivenza libera da malattia stata denita come lintervallo di tempo , successivo al trattamento , durante il quale il paziente sopravvive senza alcun segno della malattia . la sicurezza stata denita come la frequenza di complicanze . 
tutte le complicanze sono state registrate e classicate come minori e maggiori , valutate in base ai criteri common terminology criteria for adverse events ( ctcae ) [ 15 ]  . 
sono state denite complicanze maggiori quelle che , se non trattate , potrebbero minacciare la vita del paziente , portare a morbilit importanti e disabilit , condurre ad un ricovero ospedaliero o allungare la degenza in ospedale , cos come descritto da international working group of image guided tumor ablation [ 16 ] ; per complicanze minori , invece , si intende la sindrome post - ablazione associata a una sintomatologia simil inuenzale ( febbre , dolore , nausea e vomito ) che si protrae per pi di 4 giorni dopo la procedura . 
 le complicanze sono state ulteriormente suddivise in due categorie : complicanze legate al posizionamento dellantenna ( pneumotorace , infezione e sanguinamento ) e complicanze da danno termico ( danni agli organi adiacenti ) [ 17 ]  . 
gli indici di laboratorio ( conteggio dei globuli bianchi , bilirubina sierica , fosfatasi alcalina , aspartato aminotransferasi , alanina aminotransferasi ) sono stati valutati prima e dopo la sessione di ablazione . lefcacia tecnica stata valutata in base alla percentuale di recidive locali . 
la recidiva locale stata denita come la presenza di tessuto vitale ( < 5 mm ) intorno e / o nel contesto della lesioni trattate , visibile alla tc eseguita almeno dopo 3 mesi dalla procedura . 
lefcacia tecnica stata valutata sulla base delle caratteristiche di imaging utilizzando i response evaluation criteria in solid tumors ( recist ) [ 18 ]  . il follow - up totale in tutti i pazienti stato registrato a partire dalla data dellultima procedura ( primo o secondo trattamento ) no alla scansione tc pi recente . analisi statistica per lanalisi statistica dei dati stato utilizzato il software medcalc ( broekstraat 52 , 9030 mariakerke , belgio )  . 
per la valutazione del tempo libero da malattia stato applicato il metodo kaplan - meier . the medcalc software ( broekstraat 52 , 9030 mariakerke , belgium ) was used for statistical analysis , and the kaplan meyer method was applied for evaluation of dfs . il successo tecnico stato del 100% : in tutti i casi le antenne sono state posizionate correttamente allinterno della risultati 956 radiol med ( 2013 ) 118 : 949961 lesione . 
nessuna complicanza maggiore insorta nel periodo intra - , peri - , post - procedurale , le complicanze registrate possono essere classicate nello stadio 1 secondo i criteri ctcae [ 15 ]  . 
in 7 pazienti sono stati registrati valori alterati di bilirubina sierica nel post - trattamento ( in media 1 , 73 mg / dl ; range 0 , 83 , 6 mg / dl )  . 
si ricorsi ad una seconda sessione di ablazione per trattare il tessuto residuo a distanza di 3 mesi dal trattamento iniziale ; questo ha prodotto una necrosi completa del tessuto neoplastico ancora vitale . 
in 3 delle 31 lesioni trattate ( 9 , 6% ) stata osservata una recidiva durante il periodo di follow - up . non stata evidenziata nessuna correlazione statisticamente rilevante tra sesso , et del paziente e incidenza di recidiva o residuo . 
inne , in 6 dei 25 pazienti sottoposti a mwa ( 19 , 3% ) stata registrata durante il follow - up la comparsa di nuove lesioni alla tc indicative di una progressione della malattia nonostante in questi pazienti lablazione della lesione target risultasse completa . discussione la chirurgia resettiva considerata , se realizzabile , il trattamento prioritario nella terapia delle metastasi epatiche ed la sola ad intento curativo [ 2 , 19 ]  . 
diversi studi effettuati dai centri pi importanti hanno dimostrato che la resezione di ben l80% del parenchima epatico pu essere eseguita con un tasso di mortalit operatoria inferiore al 5% [ 2 , 20 ] , ma solo per il 5%10% dei pazienti , al momento della diagnosi , possibile il trattamento chirurgico [ 3 , 21 ] con una fig . 
eseguita dopo un mese dalla procedura di ablazione documenta la presenza di unarea periferica a morfologia semilunare compatibile con residuo di malattia . there was no statistical correlation between sex , age and incidence of residual tumour or tumour recurrence . 
six of the 25 patients who underwent mwa ( 19.3% ) developed disease progression with the appearance of new lesions on follow - up ct ; in these patients , the ablation of target lesions was complete . discussion when feasible , surgical resection is considered the treatment of choice for liver metastases and is the only treatment with curative intent [ 2 , 19 ]  . 
several studies from major hospitals have shown that resection of as much as 80% of the liver can be performed , with an operative mortality rate of < 5% [ 2 , 20 ]  . 
however , only 510% of patients are suitable for surgical treatment , with a resulting 5 - year survival rate of 2040% , depending on tumour location , type , number and size [ 3 , 21 ]  . 
among these predictors , the number of hepatic metastases and tumour - free surgical margins remain the most important determinants of survival [ 23 ]  . although hepatic resection can be performed relatively easily for a solitary tumour , and survival rate is high , treatment is highly invasive . 
moreover , in patients potentially suitable for surgery , metastases may be located in sites not radically resectable , such as adjacent to the gastrointestinal tract , important vessels or gallbladder . 
these limitations have prompted the search for alternative therapies to surgery , such as ablative techniques , to allow local control of unresectable tumours [ 7 , 23 ]  . 
various ablation techniques have been developed , including ethanol ablation , laser absopravvivenza a 5 anni del 20%40% variabile a seconda della posizione , del tipo , del numero e delle dimensioni delle lesioni . 
tra questi determinanti , il numero delle metastasi e la possibilit di ampi margini di exeresi allatto chirurgico sono da considerarsi i fattori prognostici pi importanti per la sopravvivenza [ 23 ]  . anche se la resezione epatica pu essere eseguita in modo relativamente agevole per un tumore solitario e comporta un tasso di sopravvivenza alto , il trattamento da considerarsi altamente invasivo . 
inoltre , nei pazienti potenzialmente candidati alla chirurgia , le metastasi possono localizzarsi in siti difcilmente raggiungibili o non suscettibili di unexeresi completa per la vicinanza di strutture importanti come il tratto gastrointestinale , vasi di grosso calibro , la colecisti . 
 tutto ci ha dirottato lattenzione verso tecniche alternative alla chirurgia , quali le tecniche ablative , per consentire il controllo locale di un tumore non resecabile [ 7 , 23 ]  . 
questi hanno riconosciuto la rfa come metodica fattibile e relativamente sicura , con tassi di risposta tumorale del 52%95% e una sopravvivenza mediana di 3037 mesi [ 7 , 25 ]  . 
 la disponibilit di follow - up pi prolungati e di serie di pazienti numericamente pi consistenti , tuttavia , ha reso manifesta la possibile insorgenza di gravi complicanze e il 958 radiol med ( 2013 ) 118 : 949961 lation , cryoablation and rfa [ 47 ]  . 
the most widely used technique is rfa [ 24 ] , which has emerged as a promising treatment option for liver metastases , although its exact role in the treatment of nonresectable metastases needs to be established . 
several studies have proved rfa to be feasible and relatively safe , with tumour response rates of 5295% and median survival of 3037 months [ 8 , 27 ]  . with increasing follow - up time and the availability of larger patient groups , however , the occurrence of serious complications and the high number of local rfa failures emphasise the need for a more precise identication of risk factors for both occurrence of complications and local tumour growth after rfa treatment [ 9 ]  . 
the authors dened as central those lesions located in direct contact with or abutting a large vessel measuring at least 3 mm . mwa is able to offer all the benets of rfa as well as some substantial advantages [ 8 , 28 ]  . 
mwa zone size and shape may be more consistent and less dependent on the heat - sink effect from vascular structures in proximity to the lesion [ 13 , 14 ]  . 
 [ 29 ] , in a review covering the last 10 years , analysed the safety and efcacy of mwa of liver metastases , particularly from colorectal cancer , and concluded that it may be considered a safe treatment modality . 
 laparoscopic and surgical approaches are used to ablate lesions that cannot be reached percutaneously or in patients who may benet at the same time from other abdominal operations [ 30 , 31 ]  . 
in our series , we selected only metastases > 3 cm and located close to vessels ( with a diameter > 3 mm ) ; they were treated using percutaneous mwa so that a large ablation area could be obtained easily by several needle antenna insertions into the target neoplasm under us guidance within a relatively short period . non trascurabile numero di fallimenti della rfa , sottolineando la necessit di una pi precisa identicazione dei fattori di rischio da correlare alle complicanze ed allefcacia del trattamento [ 9 ]  . 
 [ 27 ] ha concluso che i fattori che inuiscono sul successo locale della rfa nel trattamento della metastasi epatiche sono la dimensione della lesione , il numero e la loro ubicazione ; nel suo studio infatti , la recidiva risultata pi frequente per le metastasi con diametro superiore ai 3 cm ( 19 , 5% e 41 , 2% in clm con diametro di 35 cm e > 5 cm rispettivamente , contro il 5 , 6% delle lesioni con diametro inferiore a 3 cm ) e nelle lesioni in posizione centrale rispetto a quelle periferiche ( 21 , 4% contro 6 , 5% )  . 
sono denite centrali le lesioni in contatto diretto o adiacenti a vasi di grosse dimensioni con diametro di almeno 3 mm . la mwa in grado di offrire tutti i beneci della rfa oltre a sostanziali vantaggi [ 8 , 28 ]  . 
la mwa garantisce un migliore prolo convettivo , temperature pi elevate e costanti allinterno della lesione , riduzione dei tempi di procedura , possibilit di utilizzare pi antenne simultaneamente per il trattamento di lesioni multiple . 
le dimensioni e la forma dellarea di ablazione ottenuta con le microonde risultano essere pi conformi alle reali caratteristiche della lesione tumorale , inoltre le mw risentono meno delleffetto di dissipazione del calore legato alla presenza di strutture vascolari in prossimit della lesione [ 13 , 14 ]  . 
 [ 29 ] in una recente revisione che copre gli ultimi 10 anni , ha analizzato la sicurezza e lefcacia delle mw nel trattamento ablativo delle metastasi epatiche , in particolare nelle metastasi colorettali ( clm ) , concludendo che tale metodica pu essere considerata una modalit sicura di trattamento . 
 come le altre tecniche ablative , la mwa offre differenti tipi di approccio : percutaneo , laparoscopico , laparotomico [ 30 ] ; lapproccio laparoscopico , e in misura maggiore quello laparotomico , vengono utilizzati per lablazione di lesioni che non possono essere raggiunte attraverso la via percutanea oppure nel caso di pazienti che possono beneciare , nel medesimo tempo operatorio , di altri interventi addominali [ 30 , 31 ] ; nel nostro studio , in cui sono state selezionate solo lesioni con diametro superiore ai 3 cm e / o localizzate in prossimit di strutture vascolari con diametro > 3 mm , il trattamento con una o pi antenne , inserite per via percutanea sotto guida ecograca , ha permesso lablazione delle lesioni con una durata complessiva del trattamento relativamente breve . nello studio di lorentzen et al . 
 [ 11 ] suggested that lesions > 5 cm and those located close to great vessels or adjacent organs should be treated with open rfa , thus allowing vascular inow occlusion and complete mobilisation of the liver . 
 in conclusion , however , the most important aspect emerging from our small series is the possibility of performing mwa of metastases located at critical sites where literature data reveal that other ablative techniques , such as rfa , may be neither radical nor completely safe . 
it also shows the possibility of treating large lesions simultaneously by using multiple antennas ( average diameter of lesions treated in our series is lower than that found in the literature )  . 
mwa seems technically preferable in selected cases : lesions with diameter > 3cm lesions close to large - calibre vessels > 3 mm lesions close to important structures ( gallbladder , right exure of the colon ) ta del 100% con una ablazione completa della lesione target valutata nellimmediato post - procedura tramite controllo ecograco con mdc . 
il tasso di recidiva della nostra casistica ( 9 , 6% ) , confrontato con i dati della letteratura , pu essere considerato accettabile tenendo conto delle caratteristiche delle metastasi trattate . 
 [ 11 ] hanno suggerito che le lesioni con diametro > 5 cm e quelle localizzate vicino a vasi di grosso calibro o in prossimit di organi importanti , devono essere trattate con rfa a cielo aperto , cos da mobilizzare il fegato ed ottenere locclusione del usso epatico in entrata . 
nel nostro studio , la sindrome post - ablazione , identicata con uno stato simil febbrile associato a malessere generale , stata registrata in 6 ( 21% ) delle 29 sessioni di ablazione eseguite . lesperienza presentata uno studio non randomizzato ; lassenza di un confronto con una metodica di ablazione alternativa rappresenta un limite . 
altri limiti possono essere identicati nel limitato numero di pazienti inclusi nello studio , e nel periodo di follow - up relativamente breve ( 12 , 04 mesi )  . 
inoltre i pazienti della nostra serie non hanno ricevuto una chemioterapia adiuvante in modo uniforme dunque non possono essere considerati un gruppo omogeneo . tuttavia , laspetto pi rilevante che emerge dal nostro studio , seppure numericamente limitato , la possibilit di eseguire la mwa anche su metastasi epatiche che si localizzano in siti critici , laddove i dati della letteratura rivelano come altre tecniche ablative , prima fra tutte la rfa , risultano essere non radicali n completamente sicure , inoltre dimostra la possibilit di trattare lesioni di grosse dimensioni simultaneamente grazie allimpiego di pi antenne ( il diametro medio delle lesioni trattate nella nostra serie superiore a quello che si trova in letteratura )  . 
inclusion criteria were patients with 2 dilated side branches involving any site of the parenchyma ; presence of communication with the main pancreatic duct and previous investigations by mri / mrcp within at least six months . 
patients with a follow - up period shorter than 12 months ( n = 33 ) and those with a diagnosis of multifocal ipmn of the side branches without any follow - up ( n = 14 ) were excluded from the study . 
the quantitative image analysis included : number of dilated side branches in the head - uncinate process and body - tail ; maximum diameter of lesions in the head - uncinate process ; maximum diameter in the body - tail ; maximum diameter of the main pancreatic duct in the head and body - tail . 
the qualitative image analysis included : presence of malformations or anatomical variants of the pancreatic ductal system ; site of the lesions ( head - uncinate process , body - tail , ubiquitous , bridge morphology ) ; presence of gravity - dependent intraluminal lling defects ; presence of enhancing mural nodules . 
lobiettivo che il nostro studio si propone quello di seguire levoluzione nel tempo delle neoplasie multifocali mucinose intraduttali papillari ( ipmn ) dei rami collaterali per mezzo della risonanza magnetica ( rm )  . 
criteri di inclusione : pazienti con 2 rami collaterali dilatati che coinvolgono qualunque sito del parenchima pancreatico ; presenza di comunicazione con il dotto pancreatico principale , 2 esami precedenti rm / cprm a distanza di almeno sei mesi . 
criteri di esclusione : pazienti con un periodo di osservazione inferiore ai 12 mesi ( n = 33 ) , ed i pazienti con diagnosi di ipmn multifocale dei dotti di ii ordine che non hanno un follow - up ( n = 14 )  . 
 lanalisi quantitativa comprendeva : numero delle ectasie cistiche dei dotti collaterali nella testa - processo uncinato e nel corpo - coda ; diametro massimo delle lesioni nella testa - processo - uncinato ; diametro massimo nel corpocoda , diametro massimo del dotto pancreatico principale nella testa e nel corpo - coda . 
lanalisi qualitativa comprendeva : presenza / assenza di malformazioni / varianti anatomiche del sistema duttale pancreatico , localizzazione delle lesioni nel parenchima pancreatico , presenza di difetti endoluminali declivi , presenza di noduli parietali 918 radiol med ( 2013 ) 118 : 917929 results . 
the mean diameter of the cystic lesions was 13.7 mthe mean diameter of the main pancreatic duct was 3.6 mat follow - up , the mean number of cystic lesions was 7.76. 
il diametro medio delle ectasie cistiche era di 13 , 7 mil diametro medio del dotto pancreatico principale era di 3 , 6 mal follow - up il numero medio di ectasie cistiche era di 7 , 76 . 
il diametro medio del dotto pancreatico principale era di 3 , 7 min 18 / 108 pazienti ( 16 , 6% ) sono stati osservati difetti di riempimento intraluminali nei dotti pancreatici secondari , mentre sono stati riscontrati noduli murali in 3 / 108 pazienti ( 2 , 7% )  . 
 keywords pancreas intraductal papillary mucinous tumours mr imaging parole chiave pancreas tumori intraduttali papillari mucino - secernenti risonanza magnetica introduction introduzione intraductal papillary mucin - secreting neoplasms ( ipmns ) of the pancreas may originate in the epithelium of the main pancreatic duct ( mpd ) and of the side branches ( sb ) and are thus classied morphologically into mpd - ipmn , sbipmn , and mixed forms [ 1 , 2 ]  . 
the risk of malignant transformation varies by site of onset of ipmn : it was observed that tumours originating from branch ducts have a malignancy rate of 25% ( 6%46% ) , while ipmn of the mpd have a malignancy rate of 70% ( 57%92% ) [ 3 ]  . 
 for this reason , the international guidelines consider ipmn of the mpd or mixed forms to be an indication for surgery , while clinical and radiological follow - up is indicated in sb - ipmn [ 3 ]  . the biological behaviour of ipmn varied from papillary intraductal mucinous adenoma , ipmn with moderate dysplasia ( borderline ) and intraductal papillary mucinous carcinoma , noninvasive ( in situ ) or invasive ; different degrees of dysplasia can also be found within the same tumour [ 4 , 5 ]  . 
with the growing use of imaging techniques , these cystic pancreatic lesions are detected incidentally with increasing frequency [ 6 ]  . studies on the evolution of ipmn , especially of the side branches , with magnetica resonance imaging ( mri ) and mr cholangiopancreatography ( mrcp ) are still limited in number and with mixed results [ 6 ]  . the goal of imaging is to detect malignant forms and the i tumori intraduttali papillari mucino - secernenti ( ipmn ) del pancreas possono originare dallepitelio del dotto pancreatico principale ( dpp ) e da quello dei dotti secondari ( dii ) ; pertanto sono stati classicati morfologicamente in ipmn del dpp , ipmn dei dii e forme miste [ 1 , 2 ]  . 
il rischio di trasformazione maligna varia in base alla sede di insorgenza degli ipmn : stato infatti osservato che tumori che si originano dai dotti pancreatici secondari hanno una frequenza di malignit del 25% ( 6%46% ) mentre gli ipmn del dpp hanno una frequenza di malignit del 70% ( 57%92% ) [ 3 ]  . 
 per tale ragione , le linee guida internazionali pongono indicazione allintervento chirurgico per gli ipmn del dotto pancreatico principale o le forme miste , mentre per gli ipmn dei dotti secondari viene indicato il follow - up clinico - radiologico [ 3 ]  . 
 il comportamento biologico degli ipmn variabile da adenoma mucinoso papillare intraduttale , ipmn con moderata displasia ( borderline ) e carcinoma mucinoso papillare intraduttale , non invasivo ( in situ ) o invasivo ; inoltre i diversi gradi di displasia si possono ritrovare anche nello stesso tumore [ 4 , 5 ]  . 
 gli studi sullevoluzione degli ipmn in particolare dei radiol med ( 2013 ) 118 : 917929 initial stages of malignant transformation of ipmn from adenoma to borderline lesion to cancer [ 7 ]  . 
the present experience continues a previous study by extending the observation window and the population examined , in order to follow the evolution over time of side branch ipmns and to gain insight into their natural history , a prerequisite for the diagnosis and management of these patients [ 8 ]  . materials and methods an analysis of the archives of surgery , pathology and radiology of our institute revealed 155 patients eligible for inclusion in this retrospective study : all patients had a diagnosis of multifocal ipmn of the side branches and underwent mri and mrcp . the inclusion criteria were the presence of two or more dilatations of the side branches , involving any location of the pancreatic parenchyma ; at least two lesions communicating with the main pancreatic duct ; two or more mri / mrcp studies performed at our centre at least six months apart ; a follow - up period exceeding 12 months . the exclusion criteria were lesions involving both the side branches and the main pancreatic duct ( mixed ipmn ) ; imaging studies performed elsewhere ; follow - up period less than 12 months ( n = 33 ) ; patients with a diagnosis of multifocal ipmn of second - order ducts without follow - up ( n = 14 ) ( which we intend , however , to follow up and monitor over time )  . the nal population included in the study thus comprised 108 patients . 
the average age of patients at diagnosis was 63.4 years ( range , 2884 )  . at the time of observation 82 / 108 patients ( 75.9% ) were asymptomatic , so the detection of multifocal ipmn of the side branches occurred incidentally during radiological tests carried out for other indications . 
the remaining 26 / 108 ( 24.1% ) patients were symptomatic : 16 / 108 patients ( 14.8% ) had diabetes , with previous episodes of acute and chronic pancreatitis ; 5 / 108 patients ( 4.6% ) had abdominal pain ; 2 / 108 patients ( 1.8% ) had episodes of acute pancreatitis . 
in the patient population studied , 2 / 108 patients ( 1.85% ) had abnormal cancer antigen ( ca ) 19 - 9 values and 1 / 108 ( 0.92% ) patient had increased carcinoembryonic antigen ( cea ) values . from the time of diagnosis , all patients were examined periodically with mri / mrcp on a quarterly or annual basis over a follow - up period exceeding 12 months ( mean , 34.6 months ; median , 25.8 months ; range , 12217 months ) and with a mean number of investigations of 3.8 ( range , 211 )  . the follow - up examinations performed 6 months conrmed the mri / mrcp diagnosis of multifocal ipmn of the dotti collaterali con risonanza magnetica ( rm ) e colangiopancreatograa rm ( cprm ) sono ancora in numero limitato e con risultati non univoci [ 6 ]  . 
 obiettivo della diagnostica per immagini quello di identicare le forme maligne e le fasi iniziali della trasformazione degli ipmn nel loro processo carcinogenetico da adenoma a lesione border - line no al carcinoma [ 7 ]  . 
questo lavoro riprende uno studio precedente ampliando la nestra di osservazione e la popolazione presa in esame , al ne di seguire levoluzione nel tempo degli ipmn dei dotti secondari e di conoscerne la storia naturale , presupposto utile e fondamentale per la diagnosi e la gestione di questi pazienti [ 8 ]  . materiali e metodi da unanalisi dellarchivio della chirurgia , anatomia patologica e radiologia del nostro istituto , sono stati identicati 155 pazienti potenzialmente candidati per inclusione in questo studio retrospettivo con diagnosi di ipmn multifocali dei dotti pancreatici secondari , sottoposti ad esami di rm / cprm . i criteri di inclusione dello studio hanno compreso i pazienti con presenza di due o pi ectasie dei dotti pancreatici secondari , coinvolgenti qualsiasi sede del parenchima pancreatico ; presenza di comunicazione di almeno due lesioni con il dotto pancreatico principale e due o pi esami rm / cprm a distanza di almeno sei mesi effettuati presso il nostro istituto , pazienti con un periodo di osservazione superiore ai 12 mesi . i criteri di esclusione dello studio sono stati : lesioni coinvolgenti sia i dotti secondari che il dotto pancreatico principale ( ipmn misti ) ; esami effettuati in sedi diverse dal nostro istituto ; pazienti con un periodo di osservazione inferiore ai 12 mesi ( n = 33 ) ed i pazienti con diagnosi di ipmn multifocale dei dotti di ii ordine che non hanno un follow - up ( n = 14 ) , che comunque ci proponiamo di seguire e monitorare nel tempo . quindi la popolazione di pazienti inclusa nello studio stata di 108 pazienti . 
gli ipmn periferici multifocali sono stati riscontrati in 76 soggetti di sesso femminile ( 70 , 3% ) e solo in 32 pazienti di sesso maschile ( 29 , 6% )  . 
 al momento dellosservazione 82 / 108 pazienti ( 75 , 9% ) erano asintomatici , per cui il riscontro di ipmn multifocali dei dotti secondari stato occasionale , osservato durante esami di radiologia svolti con altre indicazioni . 
mentre i restanti 26 / 108 ( 24 , 1% ) pazienti sono risultati sintomatici : 16 / 108 pazienti ( 14 , 8% ) erano diabetici , con pregressi episodi di pancreatite acuta e cronica ; 5 / 108 pazienti ( 4 , 6% ) presentavano dolore addominale , e 2 / 108 pazienti ( 1 , 8% ) 920 radiol med ( 2013 ) 118 : 917929 side branches , and were used as a screening test for further investigations in the same patient . examination technique and protocol mr examinations were performed using a 1.5 - tesla superconducting magnet ( magnetom symphony , siemens , erlangen , germany ) , with a 4 - channel coil placed over the upper abdomen . 
before the investigation , all patients were requested to fast for 4 - 6 hours ; then , 10 - 20 minutes before the examination they were given 50150 ml of superparamagnetic contrast agent ( lumirem , guerbet , paris , france ) orally in order to cancel the signal from the gastroduodenal uid on the t2 - weighted sequences . 
the dynamic study was performed with t1 - weighted volumetric gre sequences , with selective fat saturation ( volume interpolated breath - hold examination , vibe ) acquired in the axial plane . 
nella popolazione di pazienti studiati 2 / 108 pazienti ( 1 , 85% ) presentavano valori alterati di cancer antigen ( ca ) 19 - 9 e 1 / 108 ( 0 , 92% ) paziente valori aumentati di carcinoembryonic antigen ( cea )  . dal momento della diagnosi , tutti i pazienti sono stati sottoposti a controlli periodici con rm / cprm , a cadenza semestrale e / o annuale , per un periodo di osservazione superiore ai 12 mesi per una media di 34 , 6 mesi ( mediana 25 , 8 ; intervallo 12217 mesi ) , con un numero di indagini medio di 3 , 8 ( intervallo 211 )  . la conferma del quadro rm / cprm negli esami di controllo , eseguito 6 mesi , ha confermato la diagnosi di ipmn multifocali dei dotti di ii ordine ed ha rappresentato un esame di controllo per gli esami successivi nello stesso paziente . tecnica e protocollo desame gli esami di rm sono stati eseguiti mediante unapparecchiatura con magnete superconduttivo da 1 , 5 tesla ( magnetom symphony , siemens , erlangen , germania ) , con bobina multicanale ( 4 canali ) posizionata sulladdome superiore . 
 prima dellesecuzione dellindagine a tutti i pazienti stato richiesto il digiuno ( 46 ore ) ; sono stati somministrati 50 150 ml di mezzo di contrasto ( mdc ) superparamagnetico ( lumirem , guerbet , parigi , francia ) per os , 1020 minuti prima dellesame , al ne di annullare lintensit di segnale del uido gastroduodenale nelle sequenze t2 - dipendenti . 
tale sequenza stata condotta secondo diverse angolazioni ( da 3 a 10 acquisizioni ; media : 6 ) , rispetto allasse maggiore del pancreas al ne di ottimizzare la visualizzazione del sistema duttale pancreatico . radiol med ( 2013 ) 118 : 917929 was performed randomly , whereas the follow - up images were always reviewed in comparison with the diagnostic examination in order to detect any changes . 
variations in the number of cystic dilatations of the side branches at the head - uncinate process and body - tail , as well as variations in the mean diameter of the largest cystic lo studio dinamico stato ottenuto durante la somministrazione di 0 , 1 mmol / kg di peso corporeo di chelati del gadolinio ( multihance , bracco , milano , italia ) a 2 , 5 ml / s con tecnica quadrifasica : pre - contrasto , fase pancreatica ( 3545 s ) , venosa portale ( 8590 s ) , e tardiva ( > 180 s ) , a cui ha fatto seguito iniezione di soluzione salina ( 1525 ml )  . 
lo studio dinamico stato eseguito mediante sequenze in eco di gradiente , t1 - dipendenti , volumetriche , con saturazione selettiva del grasso volume interpolated breathold examination ( vibe ) secondo il piano assiale . 
 analisi delle immagini lanalisi delle immagini stata eseguita da 2 osservatori ( rm , 15 anni di esperienza ; fc , 4 anni di esperienza ) , in maniera indipendente , alla workstation di refertazione . 
lanalisi delle immagini di rm / cprm stata eseguita alla diagnosi in maniera randomizzata ; mentre i successivi controlli a confronto con lesame della diagnosi , al ne di evidenziare eventuali variazioni . 
 stata eseguita unanalisi delle immagini sia di tipo qualitativo che di tipo quantitativo . lanalisi qualitativa ha previsto i seguenti parametri : presenza di malformazioni / varianti anatomiche del sistema duttale pancreatico : pancreas normalmente fuso / pancreas divisum ; sede della lesione : testa - processo uncinato , corpo - coda , ubiquitario o a ponte ( coinvolgimento della testa e della coda con risparmio del corpo ) ; presenza di difetti di riempimento endoluminali declivi allinterno delle ectasie cistiche nelle sequenze t2 - dipendenti ( haste ) suggestivi di presenza di mucina ; presenza di noduli parietali ( denendo come tali qualsiasi escrescenza papillare o protuberanza evidenziabile nel contesto delle singole ectasie cistiche , purch in posizione antideclive ) con impregnazione di mdc nella fase venosa dopo somministrazione di chelati del gadolinio . lanalisi quantitativa delle immagini stata effettuata da un osservatore non coinvolto nellanalisi qualitativa , ed ha preso in considerazione i seguenti parametri : numero delle ectasie cistiche dei dotti pancreatici secondari nella testa - processo uncinato ed a livello del corpocoda ; diametro massimo della ectasia cistica dei dotti secondari di maggiori dimensioni , a livello della testa - processo uncinato ed a livello di corpo - coda ; diametro massimo del dotto pancreatico principale nella testa e nel corpo - coda . 922 radiol med ( 2013 ) 118 : 917929 table 1 multifocal intraductal papillary mucinous neoplasms ( ipmn ) of the side branches : mri / mrcp pattern at diagnosis and follow - up . 
qualitative analysis qualitative analysis diagnosis , n ( % ) k statistic follow - up , n ( % ) ipmn of the branch ducts in the head - uncinate process ipmn of the branch ducts in the body - tail ubiquitous ipmn of the branch ducts ipmn of the branch ducts with bridge morphology gravity - dependent lling defects contrast - enhanced mural nodules 10 / 108 ( 9.2 ) 9 / 108 ( 8.3 ) 83 / 108 ( 76.8 ) 6 / 108 ( 5.5 ) 18 / 108 ( 16.6 ) tabella 1 neoplasie intraduttali papillari mucino - secernenti ( ipmn ) multifocali dei dotti secondari : caratteristiche rm / cprm alla diagnosi e loro evoluzione . 
la correlazione inter - osservatore stata considerata scarsa per un valore k < 0 , 20 ; sufciente per 0 , 21 < k < 0 , 40 ; moderata per 0 , 41 < k < 0 , 60 ; buona per valori 0 , 61 < k < 0 , 80 e molto buona per valori 0 , 81 < k < 1 , 00 . il test t di student per dati appaiati stato applicato per analizzare la variazione del numero delle ectasie cistiche dei dotti pancreatici secondari sia nella testa - processo uncinato che nel corpo - coda , la variazione del diametro massimo della lesione cistica dei dotti secondari di maggiori dimensioni e del calibro medio del dotto pancreatico principale , nella testa - processo uncinato e nel corpo - coda , alla diagnosi ed ai controllo controlli successivi . 
in 13 / 108 ( 12% ) pazienti stata osservata la variante anatomica del pancreas divisum , mentre nei restanti 95 / 108 ( 88% ) pazienti la congurazione duttale pancreatica risultata normale . 
 the ndings regarding the quantitative analysis of comparisons between the last follow - up examination and the examination at diagnosis are shown in table 4 . discussion ipmns represent approximately 25% of cystic neoplasms of the pancreas but their precise prevalence is not known [ 6 ]  . 
 these tumours are characterised by a papillary proliferation with excessive production of extracellular mucin which can lead to occlusion of the pancreatic ducts , with the possible occurrence of pawith the passing of time the continued growth of the ipmn leads to a bulging of the wall of the affected duct , giving the neoplasm the typical appearance of a pancreatic cystic lesion [ 9 ]  . 
on diagnostic imaging , ipmns of the side branches appear as cystic dilations of the ducts , in communication with the main pancreatic duct that presents normal calibre [ 10 ]  . in relation to the different morphology of ipmn , which correlates to a different biological behaviour , international guidelines consider ipmn of main pancreatic duct or mixed forms to be an indication for surgery , whereas clinicalradiological follow - up is indicated for ipmn of the side branches , especially when lesions are < 3 cm in asymptomatic patients [ 11 , 12 ]  . the risk of invasive cancer is less than 30% , but is not i dati relativi alla localizzazione degli ipmn , alla rilevazione di difetti di riempimento declivi allinterno del lume delle ectasie dei dotti pancreatici secondari , dovuti alla mucina ed alla presenza / assenza di noduli parietali in posizione anti - declive con impregnazione di mdc in fase post - contrastograca sono riportati nella tabella 1 . la variabilit inter - osservatore risultava avere un buon grado di correlazione per la rilevazione di possibili varianti anatomiche ( k = 0 , 77 ) , della localizzazione delle ectasie cistiche ubiquitarie ( k = 0 , 68 ) , a livello della testa - processo uncinato ( k = 0 , 73 ) e corpo - coda ( k = 0 , 78 )  . 
il grado della correlazione invece era sufciente per losservazione della disposizione delle ectasie cistiche a ponte ( k = 0 , 39 ) e per la rilevazione dei difetti di riempimento declivi ( k = 0 , 22 )  . 
inne scarso risultato il grado di correlazione per lidenticazione dei noduli murali con impregnazione di contrasto ( k = 0 , 20 )  . le rilevazioni riguardanti lanalisi quantitativa alla diagnosi sono riportate nella tabella 2 . 
abbiamo riscontrato un aumento della frequenza degli ipmn con laumentare dellet dei pazienti , come calcolato dalla frequenza relativa ed assoluta dellet dei pazienti suddivisi per gruppi di et riportata nella tabella 3 . osservazioni allultimo controllo lanalisi qualitativa delle immagini di ogni paziente non ha fatto rilevare alcuna modica rispetto ai risultati della diagnosi se non per la comparsa in 3 / 108 pazienti ( 2 , 7% ) radiol med ( 2013 ) 118 : 917929 fig . 
therefore these patients should be monitored over time in order to detect early signs of progression or degeneration [ 15 ]  . monitoring of ipmn is necessary for the risk of malignant transformation which , although low , is still present . 
questi tumori sono caratterizzati da una proliferazione di tipo papillare con una produzione eccessiva di mucina extracellulare che pu portare allocclusione del lume dei dotti pancreatici , con possibile comparsa di dolore . 
con il passare del tempo la continua crescita dellipmn porta ad uno sancamento della parete del dotto coinvolto , conferendo alla neoplasia il tipico aspetto di neoformazione cistica pancreatica [ 9 ]  . 
 pertanto tali pazienti devono essere controllati nel tempo , al ne di rilevare precocemente segni di progressione o di degenerazione [ 15 ]  . il monitoraggio degli ipmn si rende necessario per il rischio di trasformazione maligna che sebbene basso comunque presente . 
questo dato , tuttavia , non deve far aumentare il sospetto in questi pazienti , in quanto non rappresenta un segno suggestivo di trasformazione maligna e , in considerazione dei lunghi tempi di crescita , non richiede un cambiamento del programma di controllo nel tempo [ 17 ]  . nella nostra serie , invece , non abbiamo rilevato un aumento signicativo del diametro medio delle ectasie cistiche n del calibro del dpp a livello della testa - processo uncinato , che potrebbe essere indicativo di estensione e progressione della neoplasia , dai dotti secondari al dpp . 
 una crescita del diametro del dotto sarebbe stato sospetto in quanto il coinvolgimento del dpp si associa ad un aumentato rischio di trasformazione maligna , come ben noto nelle forme centrali e miste [ 18 ]  . 
al contrario il calibro del dpp aumentato in modo signicativo a livello del corpo - coda ; questo potrebbe essere dovuto alla continua deposizione di mucina nella porzione prossimale del dotto fig . 
limmagine t2 - dipendente di cprm sul piano coronale , dimostra unectasia cistica di multipli dotti pancreatici secondari con conformazione a ponte , a livello della testa e della coda ( frecce )  . other studies [ 4 ]  . 
this nding , however , is not a sign of malignant transformation so it should not increase the level of suspicion nor does it require any change in the follow - up programme in consideration of the long growth times [ 17 ]  . in our series , we did not detect any signicant increase in the average diameter of the cystic dilatations or in the calibre of the mpd in the head - uncinate process , which could be indicative of the extension and progression of cancer from the side branches to the mpd . 
le due immagini t2 - dipendenti di cprm sul piano coronale , dimostrano multiple ectasie cistiche dei dotti pancreatici secondari ; si nota un aumento del diametro della lesione di maggiori dimensioni a livello della testa allultimo controllo ( b ) rispetto alla diagnosi ( a )  . 
questi pazienti , tuttavia , non hanno manifestato contemporaneamente altri criteri di ma928 radiol med ( 2013 ) 118 : 917929 cess , even though the absence of parietal nodules is not an indication that the tumour is benign [ 20 ]  . 
therefore it was decided not to subject them to pancreatic resection , but to intensify the follow - up ( every 6 months instead of every year )  . recently , as a result of the lower incidence of invasive cancer , it has been proposed that selected patients with ipmn of the side branches should undergo observation if the cystic dilatation has a diameter smaller than 3 cm and there are no mural nodules or dilatation of the mpd [ 21 , 22 ]  . 
 [ 20 ] have reported that ipmns with a diameter less than 25 mm have a low incidence of malignant lesions compared to ipmns with a diameter greater than 3 ca close follow - up with mri / mrcp can be performed in these patients , particularly in those who are not candidates for surgery . 
these patients are assessed for any increase in tumour size , possible changes in radiological aspects and the appearance of symptoms [ 2326 ]  . our study had some limitations concerning the evaluation of ipmn : the lack of histological conrmation , in that the indication for surgery is increasingly limited to those patients who show signs of malignant degeneration , the retrospective nature of the study and the fact that both radiologists were aware of the diagnosis . 
as reported in the literature , in certain cases mri may underestimate the disease stage by not recognising a diffuse extension of ipmn , or , conversely , it may overestimate the presence of cystic dilatations , in that the distal dilatation secondary to mucin secretion in the pancreatic ducts and / or ductal alterations associated with chronic pancreatitis can mimic the presence of ipmn [ 27 ]  . 
finally , the major limitation of mri is the recognition of forms characterised by a high degree of dysplasia [ 28 ]  . lignit n hanno accusato alcuna sintomatologia clinica . 
 pertanto stato deciso di non sottoporli ad intervento di resezione pancreatica , ma a controlli periodici pi frequenti ( ogni 6 mesi anzich un anno )  . recentemente stato proposto in pazienti selezionati con ipmn dei dotti secondari , in relazione alla minor incidenza di carcinoma invasivo , una strategia di osservazione se la ectasia cistica ha un diametro inferiore ai 3 cm e se non sono presenti noduli murali o dilatazione del dpp [ 21 , 22 ]  . 
 [ 20 ] hanno riportato che ipmn con diametro inferiore ai 25 mm hanno una bassa incidenza per lesioni maligne rispetto agli ipmn con diametro superiore ai 3 c un follow - up seriato pu essere eseguito in questi pazienti con rm / cprm , soprattutto nei soggetti che non sono candidati alla chirurgia . 
 il nostro studio ha avuto alcune limitazioni nella valutazione degli ipmn : la mancanza di riscontro istologico , in quanto lindicazione chirurgica sempre pi limitata a quei pazienti che presentano segni di degenerazione maligna , inoltre stato condotto in maniera retrospettiva ed entrambi i radiologi erano al corrente della diagnosi . 
come riportato in letteratura , la rm pu in taluni casi sottostimare la patologia , misconoscendo unestensione diffusa degli ipmn , viceversa pu sovrastimare la presenza delle ectasie cistiche , in quanto la dilatazione distale secondaria alla secrezione di mucina nei dotti pancreatici e / o le alterazioni duttali associate con la pancreatite cronica possono mimare la presenza di ipmn [ 27 ] ; inne il maggior limite della rm il riconoscimento delle forme caratterizzate da un alto grado di diplasia [ 28 ]  . conclusioni conclusions ipmns of the side branches tend to evolve very slowly , which is why they are managed successfully with conservative therapy , through observation and monitoring . 
our ndings lead us to believe that an mri / mrcp follow - up with an interval of 6 months for the rst two years and annually thereafter is a valid strategy . 
in addition , it is desirable to use a simplied mri / mrcp protocol , with a smaller number of sequences . gli ipmn dei dotti secondari tendono ad avere unevoluzione molto lenta nel tempo , il che spiega perch vengano gestiti con successo con una terapia conservativa , attraverso losservazione ed il monitoraggio di queste lesioni . 
le nostre osservazioni ci portano a ritenere valido un controllo con rm / cprm del paziente con un intervallo di 6 mesi per i primi due anni ed annuale successivamente . 
verosimile che per ectasie molto piccole si possa ulteriormente ridurre la frequenza dei controlli rm / cprm ed anche auspicabile lutilizzo di un protocollo rm / cprm semplicato , con un minor numero di sequenze . radiol med ( 2013 ) 118 : 917929 conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
after preliminary examination with conventional ultrasound ( us ) and colour doppler us , the patients were examined with elastosonography , using high - level equipment ( toshiba aplio xg ) and quantitative software ( elasto - q )  . 
 sensitivity and specicity of the us score were about 56% and 72% , respectively , whereas those of the strain ratio were 93% and 89% , using a cut - off of 2 obtained with receiver operating characteristic ( roc ) curve analysis . 
si sono ottenuti valori di sensibilit e specicit rispettivamente 56% e 72% per leco - score e 93% e 89% per lo strain ratio , utilizzando un cut - off pari a 2 , con un valore predittivo positivo del 55% e dell82% rispettivamente . 
quantitative elastosonography is a useful diagnostic tool in the evaluation of thyroid lesions , and can be used to limit ne - needle aspiration cytology and improve the selection of patients for thyroidectomy . 
 keywords thyroid nodule quantitative elastosonography color doppler ultrasound tiroidei , utile per ridurre il ricorso allagoaspirato , in particolare nei casi incerti . parole chiave nodulo tiroideo elastosonograa quantitativa eco - color doppler introduction introduzione thyroid nodules are extremely common ndings during routine clinical examinations . 
physical examination can direct the diagnostic hypothesis towards malignity if the nodule has greater stiffness than the healthy thyroid and if it is xed to the surrounding tissue planes , particularly in the case of a single lesion . conventional ultrasonography provides useful information for the characterisation of thyroid nodules , such as echogenicity , size , borders , perilesional rim , microcalcications and vascularisation [ 1 ]  . 
changes in these parameters have been demonstrated in thyroid cancer , even though the sensitivity and specicity of the modality are not sufcient to differentiate benign and malignant lesions , needing further diagnostic investigations . 
fine - needle aspiration cytology ( fnac ) is considered the gold standard in characterising nodules that show clinical and ultrasonographic features of malignancy , in particular in the case of single nodules of at least 1 cthe sensitivity of thyroid fnac is between 65% and 98% , while its specicity varies between 72% and 100% [ 2 , 3 , 5 ]  . 
however , it is an invasive technique , and the material sampled is nondiagnostic ( thy1 ) or inconclusive / undetermined ( thy3 ) [ 6 , 7 ] according to the 2011 thyroid bethesda system ( tbs ) classication in 20% of cases ( table 1 ) [ 8 ]  . malignant nodules are characterised by a greater consistency than benign ones , while the latter show a density similar to healthy tissue [ 9 ]  . 
according to the principle for which elastic tissues , when compressed by an external force , are deformed more easily in comparison to harder ones , elastosonography provides a rapid and noninvasive evaluation of the parenchyma . 
 [ 11 ] , elastosonography was developed with the aim to complete the ultrasonographic examination by evaluating the degree of deformability of the analysed structures . most of the literature refers to the qualitative evaluation il riscontro di noduli tiroidei estremamente comune durante lesame obiettivo di routine . 
la semplice palpazione pu gi in alcuni casi indirizzare lipotesi diagnostica verso la malignit , se si individua allesame obiettivo un nodulo di consistenza aumentata rispetto alla tiroide sana e se questo appare ipomobile rispetto ai piani sottoe sovrastanti , ancor pi se si tratta di una lesione singola . lecograa convenzionale fornisce una serie di informazioni utili per quanto concerne la caratterizzazione del nodulo tiroideo , quali ecogenicit , dimensioni , denizione dei margini , orletto peri - lesionale , microcalcicazioni e vascolarizzazione [ 1 ]  . 
lalterazione di tali parametri nel carcinoma tiroideo stata ampiamente dimostrata , bench la sensibilit e la specicit della metodica non sono tali da permettere una differenziazione denitiva tra lesioni benigne e maligne , necessitando quindi di ulteriori approfondimenti diagnostici . 
attualmente lagoaspirato considerato il gold standard per la caratterizzazione delle lesioni clinicamente o ecogracamente sospette per patologia maligna , in particolare per i noduli solitari di almeno 1 cm di diametro , poich permette di porre indicazione per la tiroidectomia . 
la sensibilit dellago - aspirato della tiroide compresa tra il 65% e il 98% , mentre la specicit oscilla tra il 72% e il 100% [ 2 , 3 , 5 ]  . 
tuttavia si tratta di una tecnica invasiva , oltretutto nel 20% dei casi il materiale prelevato risulta essere non diagnostico ( thy1 ) e in una percentuale analoga inconclusivo / indeterminato ( thy3 ) [ 6 , 7 ] , secondo la classicazione thyroid bethesda system ( tbs ) del 2011 ( tabella 1 ) [ 8 ]  . 
basata sul principio che i tessuti pi elastici , quando compressi da una forza esterradiol med ( 2013 ) 118 : 10111021 1013 table 1 bethesda classication ( 2011 ) for thyroid cytopathology cytological result bethesda classication of thyroid nodules thy1 thy2 thy3 thy4 thy5 thy6 nondiagnostic or unsatisfactory cyst uid only virtually acellular specimen other ( blood , clotting artefact , etc . ) benign benign follicular nodule ( adenoma , colloid nodule ) hashimoto thyroiditis in the proper clinical context granulomatous ( subacute ) thyroiditis other atypia or follicular lesion of undetermined signicance follicular neoplasm or suspicious for a follicular neoplasm specify presence of hurthle cells suspicious for malignancy suspicious for papillary carcinoma suspicious for medullary carcinoma suspicious for metastatic carcinoma suspicious for lymphoma other malignant papillary carcinoma poorly differentiated carcinoma medullary carcinoma anaplastic carcinoma squamous cell carcinoma carcinoma with mixed features metastatic carcinoma non - hodgkin lymphoma other of tissue elasticity , focusing in particular on the colour map as the reference parameter in the characterisation of thyroid lesions . 
however , the evaluation of stiffness with colour maps is inuenced by considerable interobserver variability , in both the acquisition and interpretation of data . recently , the introduction of new software has enabled the use of a quantitative parameter , the so - called the strain ratio between the elastic distortion of normal surrounding parenchyma and of the nodular lesion , expressed as a numeric value . 
the aim of this study was to assess the value of the strain ratio in comparison with multiparametric ultrasonography analysis in the characterisation of thyroid nodules . materials and methods from july 2009 to september 2011 , we enrolled 123 patients ( 96 women and 27 men ; age range , 16 to 73 years ; average age , 39 ) with nodular thyroid disease and eligible for total thyroidectomy . 
of these patients , 109 has a single suspicious nodule according to ultrasonographic ndings , na , si deformano pi facilmente rispetto a quelli caratterizzati da maggiore durezza , lelastosonograa permette una valutazione rapida e non invasiva dei parenchimi . 
 [ 11 ] , lelastosonograa nasce come metodica che ha lobiettivo di completare lanalisi ecograca della lesione , valutando il grado di deformabilit ed elasticit delle strutture in esame . la maggior parte dei dati esistenti in letteratura fa riferimento alla valutazione qualitativa dellelasticit tissutale , ponendo particolare enfasi sulla mappa colorimetrica quale parametro di riferimento per caratterizzare le lesioni tiroidee . 
tuttavia , la valutazione del grado di rigidit , cos stimata , inuenzata da una notevole variabilit interosservatore , tanto nellacquisizione dei dati quanto nellinterpretazione degli stessi . recentemente lintroduzione di nuovi software ha consentito limpiego di un parametro quantitativo , pertanto facilmente confrontabile e standardizzabile , il cosiddet to strain ratio o rapporto di deformabilit tra la distorsio ne elastica del parenchima normale circostante e quella della lesione nodulare , espresse secondo parametri nu merici . 
lo scopo dello studio stato quello di confrontare la validit dello strain ratio rispetto allanalisi multiparametrica ecograca nella caratterizzazione del nodulo tiroideo . materiali e metodi nel periodo compreso tra luglio 2009 e settembre 2011 sono stati arruolati 123 pazienti ( 96 femmine e 27 maschi , di et compresa tra 16 e 73 anni ; et media 39 ) candidati allintervento di tiroidectomia totale per la presenza di patologia nodulare tiroidea . 
dunque sono stati prospetticamente esaminati 147 noduli tiroidei , con dimensioni comprese fra 5 mm e 60 mm . tutti i pazienti sono stati sottoposti ad esame ecograco ed eco - color doppler ( ecd ) , successivamente sono stati valutati mediante elastosonograa , con apparecchiatura ecograca di alta fascia aplio xg ( toshiba medical systems , osaka , giappone ) , sonda lineare a matrice da 137 mhz e software dedicato elasto - q ( elastosonograa quantitativa )  . 
i risultati dellesa me istologico sono stati utilizzati come parametro di rife1014 thy1 thy2 thy3 thy4 thy5 thy6 tabella 1 classicazione di bethesda del 2011 per la citopatologia tiroidea classicazione risultato citologico tbs noduli tiroidei tessuto non diagnostico o insoddisfacente cisti completamente uida campione virtualmente acellulare altro ( artefatti da sangue , vestiti , ecc ) benigno nodulo follicolare benigno ( adenoma , nodulo colloidale ) tiroidite di hashimoto in un corretto contesto clinico tiroidite granulomatosa ( subacuta ) altro atipia o lesione follicolare di signicato indeterminato neoplasia follicolare o sospetta neoplasia follicolare specicare presenza di cellule di hurthle sospetto per malignit sospetto per carcinoma papillare sospetto per carcinoma midollare sospetto per metastasi sospetto per linfoma altro maligno carcinoma papillare carcinoma poco differenziato carcinoma midollare carcinoma anaplastico carcinoma a cellule squamose carcinoma con caratteristiche miste carcinoma metastatico linfoma non - hodgkin altro tbs , thyroid bethesda system and the remaining 14 patients showed compressive multinodular goitre . 
therefore 147 thyroid nodules , measuring between 5 mm and 60 mm , were prospectively examined . all patients underwent us and colour doppler us ( cdus ) , and were subsequently examined by elastosonography , with high level equipment ( aplio xg , toshiba medical systems , osaka , japan ) , with linear matrix 137 mhz probe and dedicated elasto - q software ( quantitative elastosonography )  . 
ciascun nodulo esaminato sta to descritto dapprima in base alle caratteristiche ecograche , che hanno permesso di identicare i noduli sospetti , anche nel contesto del gozzo multinodulare , e successivamente secondo i parametri elastosonograci . 
sensibilit e specicit sono state confrontate con test statistico del kappa per la valutazione della concordanza . lecograa ha permesso lanalisi di morfologia , ecostruttura , orletto , margini e rapporti con le strutture circostanti , microcalcicazioni e pattern di vascolarizzazione . 
 per meglio confrontare i dati forniti dallecograa tradizionale e quelli elastosonograci , stato utilizzato , come parametro di sintesi , leco - score , ossia una variabile dicotomica ottenuta in base alle caratteristiche esaminate , da noi introdotta in questo studio per permettere un pi agevole confronto con i dati elastosonograci . per il calcolo delleco - score ( 0 / 1 ) sono stati considerati : lecogenicit , assegnando un valore uguale a 1 nel caso di noduli ipoo isoecogeni e 0 per formazioni iperecogene ; i margini , attribuendo un valore di 1 nel caso fossero irregolari e 0 se regolari ; la vascolarizzazione , considerando i pattern 1 e 2 indicativi di benignit ed il pattern 3 di malignit ; inne le microcalcicazioni , con lausilio del software micropure , dando un valore di 1 se presenti e 0 se assenti . 
dalla sommatoria dei punteggi assegnati agli elementi presi in considerazione , stato ricavato un parametro quantitativo facilmente confrontabile con il rapporto di deformabilit , permettendo unanalisi della lesione pi rapida e diretta . 
ai noduli che presentavano da 0 a 2 caratteristiche sospette , in base alla classicazione sopra descritta , stato attribuito un eco - score uguale a 0 ; a quelli che invece presentavano almeno tre elementi di sospetta malignit , con un punteggio pari o superiore a 3 , stato attribuito un eco - score uguale a 1 . allesame ecograco ha fatto seguito quello elatosonograco , basato sulla compressione del tessuto tiroideo sede di lesione nodulare con la stessa sonda ecograca e sulla visualizzazione della dinamica della compressione , registrata su curva compressione / tempo . 
ogni valutazione ha richiesto circa 38 minuti , con un numero medio di 8 compressioni ripetute per 5 volte . la sonda , posizionata in orientamento trasversale , stata appoggiata sulla tiroide del paziente supino con il capo iperesteso . 
ogni valutazione elastosonograca doveva visualizzare nella stessa immagine sia il diametro radiol med ( 2013 ) 118 : 10111021 1015 values , using histopathological data , were measured in order to evaluate accuracy of the two methods . 
the us score , a resumptive parameter that was used for a better comparison between the us and elastosonography data , is a dichotomous variable obtained from the features analysed and introduced in this study to facilitate the comparison with the elastosonography data . to calculate the us score ( 0 / 1 ) we considered : echogenicity , assigning a value of 1 to hypoechoic or isoechoic nodules and a value of 0 to hyperechoic ones ; borders , assigning a value of 1 to irregular borders and 0 to regular ones ; vascularisation , considering patterns 1 and 2 to indicate benignity and pattern 3 malignity ; microcalcications , using micropure software and assigning a value of 1 to their presence and of 0 to their absence . 
the nodules presenting up to 2 suspicious features were assigned a us score of 0 , while those presenting at least 3 suspicious features were scored 1 . after the us examination , elastosonography was performed by compressing , with the same us probe , the site of the nodular lesion and visualising the compression dynamics recorded on a compression / time curve . 
each evaluation took approximately 38 minutes , with an average of 8 compressions repeated 5 times . patients lay supine with hyperextended head , and the probe was positioned , with a transverse orientation , over the thyroid lobe . 
each elastosonography examination had to show both the maximum diameter of the nodule and the surrounding healthy tissue in the same image , to enable a comparison of stiffness . data were acquired and memorised as raw data for the following off - line analysis . 
 maggiore del nodulo sia una quota di tessuto sano , utilizzata per il confronto della deformazione . i dati sono stati acquisiti e memorizzati in forma di dati grezzi ( raw data ) , per la successiva valutazione off - line . 
i noduli con uno strain ratio inferiore a 2 sono stati valutati come benigni , quelli con un valore maggiore di 2 sono stati considerati maligni . risultati sono stati analizzati i dati relativi ai 147 noduli esaminati , valutati in 123 pazienti candidati alla tiroidectomia . 
in base alle caratteristiche ecograche ( eco - score ) , 26 noduli sono stati classicati erroneamente come negativi , mentre 27 sono risultati falsamente positivi . esaminando i dati elastosonograci , le 11 lesioni , erroneamente classicate come maligne sono risultate essere 7 noduli iperplastici e 2 adenomi follicolari , mentre i falsi negativi sono stati 5 , di cui 4 carcinomi papilliferi e 1 carcinoma midollare . radiol med ( 2013 ) 118 : 10111021 1016 fig . 
the nodules with a strain ratio < 2 were evaluated as benign , the ones with a value > 2 were considered malignant . results we analysed the data of 147 nodules , evaluated in 123 patients eligible for thyroidectomy . 
leco - score nel nostro studio ha dimostrato sensibilit del 56% e specicit del 72% , con valore predittivo positivo ( vpp ) del 55% e valore predittivo negativo ( vpn ) del 70% . lo strain ratio elastosonograco , invece , ha presentato sensibilit del 93% e specicit dell89% , con vpp dell82% e vpn del 94% . 
 stato analizzato il grado di concordanza diagnostica tra valutazione elastosonograca ed eco - score , che ha documentato una superiorit statisticamente signicativa ( p = 0 , 002 ) dellelastosonograa . numerosi studi riguardanti la caratterizzazione ecograca radiol med ( 2013 ) 118 : 10111021 1017 fig . 
at ultrasound ( a ) the lesion appears hypoechoic with irregular borders ; colour doppler ( b ) shows a type iii vascular pattern ; the elastosonographic ( c ) strain ratio is 2.90 , consistent with the diagnosis of malignancy . 
on the basis of the us features ( us score ) , 26 nodules were erroneously classied as negative , while 27 were considered falsely positive . examining the elastosonography data , the 11 lesions erroneously classied as malignant turned out to be seven hyperplastic nodules and two papillary adenomas , while the false negatives were four papillary carcinomas and one medullary carcinoma . the data obtained therefore appear to indicate a higher accuracy of elastosonography compared to the ultrasonographic examination . 
the us score in our study showed a sensitivity of 56% and a specicity of 72% , with a positive predictive value of 55% and a negative predictive valued of 70% . the elastosonography strain ratio , instead , showed a sensitivity of 93% and a specicity of 89% , with a positive predictive value ( ppv ) of 82% and a negative predictive value ( npv ) of 94% . 
in particolare , lo studio ha dimostrato come i noduli benigni non possano essere differenziati da quelli maligni solo in base al pattern eco - color doppler [ 13 ] ed agli altri parametri ecograci , come i margini lesionali e le microcalcicazioni . 
questultima , descritta per la prima volta circa 20 anni fa , una tecnica dinamica che valuta il grado di distorsione dei tessuti presi in esame , basandosi sul principio che , in risposta ad una compressione esterna , le porzioni molli si deformano pi facilmente rispetto a quelle dure [ 15 ]  . 
in particular , one study found that benign nodules cannot be differentiated from malignant ones according to their us features , such as lesion borders , microcalcications and colour doppler us pattern [ 13 ]  . 
however , it is necessary to keep in mind that the degree of tissue deformation is also closely correlated to the features of the surrounding structures . elastosonography was developed as a method for the study of the breast and prostate [ 1619 ] ; only later was its use extended to the analysis of the thyroid , a supercial gland easy to investigate with us and a frequent site of nodular disease . 
many recent studies have focused on its possible application in the characterisation of thyroid lesions and as a technique complementary to us , showing highly encouraging results . the most comprehensive studies on this topic [ 12 , 20 22 ] assess the colour map as the main elastosonographic parameter , and perform a qualitative analysis on the basis of the ueno - itoh classication [ 20 ]  . 
they used qualitative elastosonography to evaluate 195 thyroid nodules , of which 142 were undetermined and 53 nondiagnostic , and the scoring was classied with values 1 ( high ) , 2 ( intermediate ) 3 ( low )  . 
 [ 24 ] subsequently carried out a large study that compared the scoring and strain index cut - off values in the differential radiol med ( 2013 ) 118 : 10111021 ni sulle propriet elastiche dei parenchimi , riettendo la composizione e lorganizzazione architetturale degli stessi . 
tuttavia necessario tenere presente che il grado di deformazione di un tessuto strettamente correlato anche alle caratteristiche delle strutture circostanti . lelastosonograa nasce come metodica per lo studio della mammella e della prostata [ 1619 ] ; solo successivamente stata estesa anche allanalisi della tiroide , ghiandola superciale , facilmente indagabile con gli ultrasuoni , frequente sede di patologia nodulare . 
negli ultimi anni , lelastosonograa stata oggetto di numerosi studi di ricerca , che hanno portato a risultati fortemente incoraggianti sulla possibilit di introdurre lesame elastosonograco come strumento diagnostico valido nella caratterizzazione delle lesioni tiroidee e come tecnica complementare a quella ecograca . gli studi pi esaustivi in materia [ 12 , 2022 ] valutano come principale parametro elastosonograco la color - map , effettuando pertanto unanalisi qualitativa e basandosi sulla classicazione di ueno - itoh [ 20 ]  . 
essi hanno valutato 195 noduli tiroidei , di cui 142 indeterminati e 53 non diagnostici , con elastosonograa qualitativa , e lo scoring stato classicato con i valori 1 ( elevato ) , 2 ( intermedio ) , 3 ( basso )  . 
 [ 24 ] hanno realizzato un ampio studio , nel quale sono stati presi in considerazione e confrontati i valori di scoring e di strain index cut - off per la diagnosi differenziale tra no duli tiroidei benigni e maligni . 
questi lavori hanno dimostrato lutilit dellelastosonograa nella diagnosi differenziale . nel nostro studio preliminare [ 13 ] , abbiamo raggiunto risultati fortemente positivi sulla validit dello strain ratio , variabile quantitativa , e pertanto abbiamo ritenuto utile ampliare la casistica per avere dati di maggiore rilievo . 
 mediante lanalisi statistica , confrontando i valori ottenuti allesame elastosonograco con i parametri ecogra ci , considerando un valore di cut - off pari a 2 , lelastosonograa ha dimostrato avere sensibilit e specicit maggiori , con una concordanza statisticamente signicativa rispetto alleco - score . 
these studies demonstrated the usefulness of elastosonography in the differential diagnosis . in our preliminary study [ 13 ] , we obtained highly positive ndings of the validity of the strain ratio quantitative variable , and therefore considered it useful to extend our series to strengthen our ndings . 
by comparing the results of elastosonography and us parameters through statistical analysis , with a cut - off equal to 2 , elastosonography showed higher sensitivity and specicity with a signicant statistical agreement compared to the us score . 
our preliminary study had suggested , as a potential goal of the elastosonography technique , the possibility of collecting further differential information also in cases of nonindicated or unfeasible fnac , in agreement with the current guidelines . all these results were conrmed by the present study in which the us score showed a sensitivity of 56% and a specicity of 72% , with a 55% ppv and a 70% npv the elastosonographic strain ratio showed a sensitivity of 93% and a specicity of 89% , with a ppv of 82% and a npv of 94% . 
moreover , since the npv and sensitivity were higher than 90% , a nodule with a strain ratio > 2 , even without other suspicious features , should be investigated with fnac . 
the patients enrolled in our study had a much higher prevalence of cancer compared to the general population , as they were considered eligible for thyroidectomy for multinodular goitre or for lesions suspicious for malignant thyroid disease . 
regarding the method , the main limits were the need to maintain a correct probe / tissue angle , the unavailability of a real - time evaluation , the presence of uid areas or coarse calcications [ 22 ] , and an insufcient amount of healthy parenchyma contiguous to the lesion , as in the case of multinodular goitre [ 21 ]  . 
in the present study , however , interobserver variability was not taken into consideration ; this important factor reduces the reproducibility of compressive methods , as previously reported [ 25 ]  . 
 in a future study , we therefore plan to analyse the data relating to this variable and those resulting from the different levels of operator experience , in the light of the encouraging results obtained by merino et al . 
 [ 26 ] who recently reported a interobserver agreement of over 80% . sonograca , la possibilit di fornire ulteriori informazioni differenziative anche in quei casi in cui lagoaspirato non appare indicato o effettuabile , in accordo con le correnti linee guida . 
 tutto ci stato confermato dal presente studio in cui leco - score ha mostrato sensibilit del 56% e specicit del 72% , con valore predittivo positivo ( vpp ) del 55% e valore predittivo negativo ( vpn ) del 70% . lo strain ratio elastosonograco , invece , ha presentato sensibilit del 93% e specicit dell89% , con vpp dell82% e vpn del 94% . 
 stato analizzato il grado di concordanza diagnostica tra valutazione elastosonograca ed eco - score , che ha documentato una superiorit statisticamente signicativa ( p = 0 , 002 ) dellelastosonograa . 
inoltre , poich il vpn e la sensibilit sono risultate superiori al 90%% , un nodulo con strain ratio maggiore di 2 , anche senza altri parametri di sospetto , dovrebbe comunque essere sottoposto ad agoaspirato . 
i pazienti arruolati nel nostro studio presentavano una prevalenza signicativamente maggiore di cancro rispetto alla popolazione generale , poich gi candidati alla tiroidectomia per gozzo multinodulare o per lesioni sospette per patologia tiroidea maligna . 
per quanto concerne la metodica , la necessit di mantenere un corretto angolo sonda / tessuto , limpossibilit di una valutazione in realtime , la presenza di aree uide o grossolane calcicazioni [ 22 ] , una quota insufciente di parenchima sano adiacente alla lesione , come nel caso di gozzo multinodulare [ 21 ] , sono stati i principali limiti . 
inoltre ai ni di una buona esecuzione della tecnica , in base ai nostri dati , loperatore deve essere sufcientemente esperto in quanto , sia per la corretta visualizzazione ecograca del nodulo sia per la standardizzazione delle compressioni , necessario che lesecutore abbia effettuato un cospicuo numero di esami . 
 ci proponiamo pertanto di analizzare in ulteriori ricerche future i dati relativi a tale variabile e quelli derivati dalla differente esperienza delloperatore , alla luce dei risultati incoraggianti ottenuti da merino et al . 
 [ 26 ] che in un recente lavoro hanno riportato una concordanza interosservatore di oltre l80% . 1020 conclusions radiol med ( 2013 ) 118 : 10111021 conclusioni the results of our study showed that the strain ratio , obtained by quantitative elastosonography , is more accurate than the us score , and that this technique appears to have sufcient sensitivity and predictive value to reduce the use of fnac , with a consequent better selection of patients eligible for surgery . 
in the future , the implementation of the quantitative evaluation system with a real - time elastosonography image , will make the performance of elastosonography examination faster and easier . i risultati ottenuti dimostrano che lo strain ratio , ottenuto con lelastosonograa quantitativa , pi accurato delleco - score e , sebbene siano necessari ulteriori studi su una popolazione non selezionata di pazienti , questa tecnica appare caratterizzata da sufciente sensibilit e valori predittivi tali da ridurre il ricorso allagoaspirato , con conseguente migliore selezione dei pazienti candidati alla chirurgia . 
we considered all the requests for breast imaging ( mammography , ultrasound and magnetic resonance imaging ) received by our radiology department between october 2010 and december 2010 , and assessed their appropriateness based on the patients age and the clinical question , if present . 
out of a total of 1500 requests for ultrasound examination , the request was appropriate in 855 ( 57% ) cases ; out of a total of 2350 requests for mammography , the request was appropriate in 493 ( 21% ) cases ; out of a total of 100 requests for magnetic resonance imaging , the request was appropriate in 83 ( 83% ) cases . 
improving the timeliness of diagnosis is an important goal to be pursued by enhancing the available health services , improving communication and coordination of the different professionals involved and optimising diagnostic pathways in order to reduce healthcare spending . keywords breast cost analysis breast imaging breast cancer riassunto obiettivo . 
per quanto concerne lecograa mammaria , abbiamo riscontrato che , su un totale di 1500 esami richiesti , in 855 casi ( 57% ) la richiesta risultava inappropriata ; delle 2350 richieste di mammograe il 21% ( 493 esami ) risultato inappropriato ed inne per gli esami di rm , delle 100 richieste ricevute , l83% risultavano inappropriate . 
il miglioramento della tempestivit della diagnosi un obiettivo rilevante da perseguire attraverso un potenziamento dei servizi sanitari a disposizione , tale da migliorare la comunicazione ed il coordinamento tra le diverse gure professionali specialistiche interessate , al ne di ottimizzare i percorsi diagnostici con conseguente diminuzione della spesa sanitaria . 
 parole chiave mammella analisi dei costi diagnostica senologica tumore della mammella radiol med ( 2013 ) 118 : 984994 introduction introduzione in recent years , the correct use of available diagnostic tools and the increasingly earlier diagnosis [ 1 , 2 ] , allowing for the optimisation of therapeutic strategies , have resulted in an approximately 45% reduction in mortality rates from breast cancer [ 3 ]  . 
the inappropriate use of available technologies is not only associated with adverse diagnostic and therapeutic consequences , but can also result in rising costs , an important factor in a eld characterised by an increasing reduction in resources [ 4 , 5 ]  . nowadays , clear guidelines suggest the correct sequence of diagnostic procedures for women in different age and risk groups [ 610 ]  . 
improved optimisation of diagnostic pathways combined with the heightened sensitivity of women who spontaneously refer for diagnostic monitoring and widespread awareness campaigns have already led to a progressive increase in the number of correct diagnoses of nonpalpable lesions and consequently to a signicant improvement in long - term prognosis [ 11 ]  . 
however , further improvements would be possible if women were not confused about the correct combination of imaging modalities that should be applied : this confusion has been shown to inuence prevention and treatment in the eld of breast imaging and it often concerns both the choice of the most appropriate investigation based on age and specic clinical question [ mammography , ultrasound , magnetic resonance imaging ( mri ) ] , and the correct sequence of investigations [ 1217 ]  . the aim of this study was to evaluate the inuence of inappropriate requests on the diagnostic pathway and diagnosis and the resulting healthcare expenditure . we analysed and classied all optimal diagnostic pathways as being consistent and nonconsistent and all requests for diagnostic investigations ( mammography , ultrasound and mri ) received by our radiology department between october 2010 and december 2010 as appropriate and inappropriate . 
 diagnostic pathways negli ultimi anni , grazie ad un corretto utilizzo degli strumenti diagnostici a nostra disposizione e ad una diagnosi sempre pi precoce [ 1 , 2 ] , che a sua volta permette lottimizzazione delle strategie terapeutiche , abbiamo assistito ad una riduzione della mortalit per cancro della mammella di circa 45% [ 3 ]  . 
lelevata disponibilit di diverse tecniche diagnostiche daltra parte pu comportare il rischio del ricorso non giusticato alle stesse ed il non rispetto di una loro applicazione clinica razionale ed appropriata . 
un ricorso non appropriato alle tecnologie disponibili oltre ad avere conseguenze negative diagnostiche e terapeutiche porta anche spesso ad un incremento dei costi , fenomeno questo rilevante in una realt caratterizzata da sempre minori risorse in ambito sanitario [ 4 , 5 ]  . oggigiorno chiare linee guida dettano liter che le donne nelle diverse fasce di et e di rischio dovrebbero seguire [ 610 ]  . 
il miglioramento nellottimizzazione dei percorsi diagnostici , unitamente alla sensibilit delle donne , che spontaneamente si sottopongono a controlli strumentali periodici , ed alla maggiore diffusione delle campagne di sensibilizzazione , hanno gi determinato un progressivo aumento delle diagnosi corrette di lesioni non palpabili con conseguente signicativo miglioramento della prognosi a distanza [ 11 ]  . 
ulteriori miglioramenti sarebbero per possibili se si riuscisse ad eliminare quella confusione sulliter diagnostico da seguire , da noi riscontrata , e che spesso contraddistingue lattivit di prevenzione e cura in ambito senologico . 
tale confusione pu riguardare sia la scelta dellesame pi appropriato in relazione allet ed allo specico quesito clinico [ mammograa , ecograa , risonanza magnetica ( rm ) ] sia la corretta successione cronologica degli esami [ 1217 ]  . obiettivo del nostro studio quello di valutare come una non corretta indicazione ad un esame possa inuire sul percorso diagnostico , sulla diagnosi e sulla spesa sanitaria che ne deriva . abbiamo osservato e catalogato come coerenti e non coerenti i percorsi diagnostici ottimali , e quindi appropriate o non appropriate , tutte le richieste di esami diagnostici ( mammograa , ecograa e rm ) , giunte presso il dipartimento di diagnostica per immagini dello ircs , policlinico universitario di tor vergata roma , nel periodo compreso tra ottobre 2010 e dicembre 2010 . according to the european and usa guidelines [ 610 ] , when studying breast disease , women are divided into two categories depending on their age and the presence or absence of clinical signs ( asymptomatic and symptomatic patients ) ; moreover , women with a high risk of developing breast cancer who require specic surveillance programmes are classied as a separate category [ 610 ]  . 
 based on the guidelines [ 610 ] , we summarise the different diagnostic pathways to be undertaken , according to the percorsi diagnostici nello studio della patologia mammaria , in accordo con le linee guida europee e degli stati uniti [ 610 ] , si distinguono le donne in categorie in funzione dellet e della presenza o assenza di segni clinici ( pazienti asintomatiche e sintomatiche ) ; vengono inoltre classicate in una categoria distinta le donne ad alto rischio di sviluppo di carcinoma mammario , le quali necessitano di specici programmi di sorveglianza diagnostica [ 610 ]  . 
 986 radiol med ( 2013 ) 118 : 984994 patients category , which have been dened to achieve an early diagnosis and correct therapeutic planning . in asymptomatic patients aged < 40 years , regular screening tests are not indicated , except in case of breast cancer antigen ( brca1 , brca2 ) carriers who require specic surveillance programmes . 
in the case of the patients request , clinical examination is recommended as the rst - line investigation ; where physical signs suggest a need for further investigations , the patient should undergo ultrasound and , if the diagnostic doubts are still not solved , mammography and cytological - histological characterisation , if deemed necessary . 
mammography offers an overview of the breasts , but needs to be completed by ultrasound in the case of predominantly glandular component of the breast ; however , it is important to respect the time sequence of these two investigations . 
besides being complementary to mammography , ultrasound is essential whenever there is any doubt about the diagnosis or to dene the nature of lesions ( liquid and / or solid ) detected during mammography [ 1214 ]  . 
the time interval between examinations ranges from 12 to 18 - 24 months depending on the patients age and the mammographic ndings ; in particular , for patients with ndings falling under r3 category ( very probably benign ) , a time interval shorter then 12 months is recommended [ 610 ]  . symptomatic patients are investigated according to two different pathways depending on age . 
 suspicious ndings detected by conventional imaging need further diagnostic investigation , including mri or cytological - histological characterisation under imaging guidance [ 610 , 17 ]  . materials and methods from october 1st , 2010 to december 31th , 2010 we studied all requests for breast imaging received by the department of diagnostic imaging , molecular imaging , interventional radiology and radiotherapy of the ircs tor vergata university hospital in rome , and evaluated their appropriateness according to the patients age and the clinical hypothesis , whenever available . 
the patients enrolled in our study were aged 25 to 80 years , 68% of them were asymptomatic come in accordo con le linee guida [ 610 ] riportiamo brevemente quali siano i diversi percorsi diagnostici da considerare , in relazione alla categoria di appartenenza , deniti al ne di poter effettuare una tempestiva diagnosi ed un corretto planning terapeutico . nelle pazienti asintomatiche con et inferiore ai 40 anni , non c indicazione ad eseguire dei controlli periodici , tranne nei casi in cui queste presentino un rischio genetico di carcinoma della mammella [ breast cancer antiger ( brca1 , brca2 ) ] , che necessita di specici programmi di sorveglianza diagnostica . 
in caso di richiesta da parte della paziente comunque consigliato in prima istanza lesame clinico ; in caso di segni obiettivi che meritino un ulteriore accertamento diagnostico quindi necessario procedere con un esame ecograco e , se persiste il dubbio diagnostico , con mammograa ed eventuale prelievo citoistologico . 
la mammograa offre una valutazione panoramica delle mammelle , ma necessita di un completamento diagnostico ecograco nei casi in cui queste siano prevalentemente rappresentate da componente ghiandolare ; tuttavia importante che nel percorso diagnostico sia rispettata la successione temporale tra i due esami . 
lesame ecograco , oltre ad essere complementa re al controllo mammograco , si rende indispensabile ogni qualvolta si presenti un dubbio diagnostico o per denire la natura liquida e / o solida di una lesione apprezza bile allesame mammograco [ 1214 ]  . 
la periodicit dei controlli varia tra i 12 ed i 1824 mesi in funzione dellet della donna e del quadro mammograco ; in particola re nelle pazienti con riscontro di reperti deniti nella categoria r3 molto probabilmente benigni si consigliano controlli con intervallo di tempo inferiore ai 12 mesi [ 610 ]  . lo studio delle pazienti sintomatiche prevede due differenti percorsi diagnostici in relazione al dato anagraco . 
 nei casi di donne con et inferiore ai 40 anni trova indicazione lesame ecograco eventualmente integrato con proiezioni mammograche . le donne sintomatiche con et maggiore ai 40 anni devono essere necessariamente studiate con la mammograa e solo successivamente con lecograa . 
reperti sospetti individuati allimaging convenzionale necessitano di ulteriori approfondimenti diagnostici come la rm ovvero caratterizzazione cito - istologica sotto guida strumentale [ 610 , 17 ]  . materiali e metodi nel trimestre dal 1 ottobre 2010 al 31 dicembre 2010 abbiamo preso in considerazione tutte le richieste di esami radiol med ( 2013 ) 118 : 984994 and 32% symptomatic ( secretion , palpable nodules , retracted nipples , altered skin prole )  . 
 overall , 1 , 758 ultrasound examinations were performed , including additional investigations when missing , those repeated in the same patient due to mammography - ultrasound discrepancies resulting from incorrect diagnostic pathway , and second - look ultrasound ; 2 , 387 mammographic examinations were performed , including additional investigations when missing ; 133 mri studies were performed , also including 6 - month follow - up examinations ; nally , 46 cytological and 14 histological characterisations were performed on suspicious lesions . 
le pazienti arruolate nel nostro studio erano di et compresa tra i 25 ed gli 80 anni , asintomatiche nel 68% dei casi e sintomatiche nel 32% ( secrezione , noduli palpabili , retrazione capezzolo , alterazioni del prolo cutaneo )  . 
gli esami di rm sono stati sempre eseguiti ad eccezione dei casi in cui erano presenti delle importanti controindicazioni ( pacemaker , claustrofobia , rischio di motilit di corpi estranei metallici )  . 
al ne di completare o riordinare il corretto iter diagnostico sono stati effettuati gli esami aggiuntivi quando mancanti , in base a quanto affermato dalle linee guida [ 610 ]  . 
 per quanto riguarda gli esami ecograci , compresi quelli aggiunti quando mancanti , quelli ripetuti nella stessa paziente per discordanza mammo - ecograca conseguente ad un iter diagnostico errato e gli esami ecograci di second look , sono stati eseguiti complessivamente 1758 esami ; per quanto riguarda gli esami mammograci sono stati effettuati 2387 esami compresi i controlli aggiunti quando mancanti ; sono stati effettuati 133 esami rm , considerati anche i controlli a 6 mesi ; inne sono state eseguite su lesioni sospette 46 caratterizzazioni citologiche e 14 istologiche . 
 tutte le indagini effettuate sono state valutate da un medico radiologo con almeno 10 anni di esperienza il quale ha valutato ed interpretato le indagini eseguite in conformit e secondo quanto raccomandato sia in ambito europeo sia negli stati uniti classicando in 5 classi di categorie le conclusioni diagnostiche [ 10 , 18 , 19 ] le indagini strumentali previste ed effettuate comprendono esami convenzionali ( mammograa ed ecograa ) , esami di secondo livello ( rm ) , e la caratterizzazione citoistologica delle lesioni eseguita mediante procedure interventistiche condotte con lausilio della guida ecograca , mammograca e / o di rm . le indagini mammograche sono state effettuate con mammografo digitale ge senographe 2000 d , mediante 3 proiezioni : cranio - caudale , medio - laterale - obliqua e medio - laterale ; qualora necessarie , sono state acquisite proiezioni aggiuntive , in compressione mirata e / o ad ingrandimento diretto di immagine . gli esami ecograci sono stati realizzati con ecografo philips iu22 e sonde lineari small part dedicate per lo studio delle strutture di supercie , con frequenza compresa tra 7 , 5 e 12 mhz . gli esami rm , qualora possibile , sono stati effettuati tra il 6 ed il 15 giorno del ciclo mestruale . 
the images acquired were post - processed with image subtraction algorithm , assessment of time / intensity curves , maximum intensity projection ( mip ) and multiplanar reconstruction ( mpr )  . determination of examination - related costs for the italian national health service economic analysis of the healthcare costs that could have been avoided if the correct diagnostic procedure had been followed was made based on costs listed in the national health service ( nhs ) regional tariff for specialist outpatient examinations , as established by regional council resolution no . 
562 of lazio region dated september 2006 . table 1 reports operational codes for mammographic , ultrasound and mri procedures , cytological and histological characterisation , and interventional procedures , with the corresponding ofcial tariffs . 
sono state eseguite sequenze morfologiche t2 turbo spin echo ( tse ) pesate , sequenze t2 a soppressione selettiva del segnale del tessuto adiposo e nove sequenze dinamiche t1 fast field echo gradientecho [ tempo di ripetizione ( tr ) / tempo di eco ( te ) 5 , 1 / 2 , 3 ms , ip angle ( fa ) 20 , spessore 2 mm , senza intervallo gap , matrice di 512512 ] , di cui una basale e le altre dopo la somministrazione di mezzo di contrasto ( mdc ) gadolinioacido dietilen - triamino - pentacetico ( dtpa ) ad una dose di 0 , 10 , 2 mmol / kg ( 2 ml / s ) per via endovenosa . 
le immagini acquisite sono state sottoposte a post - processing con algoritmo a sottrazione dimmagine , valutazione delle curve intensit / tempo , ricostruzioni maximum intensity projection ( mip ) e rielaborazioni multiplanar reconstruction ( mpr )  . identicazione del costo ad esame per il sistema sanitario nazionale al ne di determinare la valutazione del costo per il sisteradiol med ( 2013 ) 118 : 984994 table 2 inappropriateness of requests for ultrasound examinations ultrasound : 855 ( 57% ) inappropriate requests out of 1500 analysed 530 ( 62% ) : rst - line examination 250 ( 30% ) : additional diagnostic test after mammography performed at another centre ( after 6 to 8 months ) 75 ( 8% ) : not indicated following mammography ( fatty breasts ) tabella 2 inappropriatezza degli esami ecograci e sua origine ecograa : 855 ( 57% ) richieste inappropriate su 1500 valutate 530 ( 62% ) : ecograa in prima istanza 250 ( 30% ) : integrazione diagnostica di mammograa di altra sede ( dopo 68 mesi da questultima ) 75 ( 8% ) : ecograa non indicata dopo mammograa ( mammelle adipose ) results we selected inappropriate requests from among all those received by our department ( tables 24 )  . 
we then analysed the causes for inappropriateness by examination method and we re - organised and added further examinations to the patients diagnostic pathways as necessary . out of a total of 1 , 500 requests for breast ultrasound , 855 ( 57% ) were inappropriate because 62% of them ( 530 exams ) had been requested as a rst - line assessment when mammography would have been more appropriate ; 30% ( 250 examinations ) had been requested in addition to mammography carried out at another centre , but the patients had obtained an appointment through the central booking service ( cup ) after 6 to 8 months only ; nally , 8% of the mammographic assessments ( 75 examinations ) showed fatty breasts without any signicant mammographic ndings , so that the diagnostic pathway could be considered complete ( table 2 )  . out of 2 , 350 requests for mammography , 21% ( 493 examinations ) were inappropriate because 76.2% ( 375 examinations ) were yearly follow - up examinations , but were performed before the end of 12 - month time period , probably because of difculties obtaining an appointment ; in 9.52% of cases ( 47 examinations ) , mammography was requested in asymptomatic patients aged < 35 years ; in 14.28% of the cases ( 71 examinations ) the patients had a request for a 6 - month ultrasound follow - up but replaced it with mammography because no appointment could be obtained through the cup ( table 3 )  . of the 100 mri referrals , 83% were inappropriate . 
inappropriateness was due to the fact that in 35% of the cases the mri had been requested as an additional investigation following negative mammography + ultrasound in patients with particularly dense breasts ; 25% were inappropriate due to the fact that the examinations were requested in order to assess known and stable nodules ( in morphology and size ) , which had already been detected on conventional imaging ma sanitario nazionale ( ssn ) degli esami che si potevano evitare se si fosse percorso il corretto iter diagnostico sono state prese in considerazione le tariffe stabilite dal nomenclatore tariffario regionale delle prestazioni specialistiche ambulatoriali , approvato con deliberazione giunta regionale del lazio n . 
 risultati dalla valutazione delle richieste giunte al dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia dello ircs , policlinico di tor vergata , abbiamo selezionato quelle inappropriate ( tabelle 24 )  . 
in 135 patients ( 25% ) , the request for an ultrasound examination was unnecessary since mammography had shown fatty breast , and this resulted in an unnecessary bilmente sempre per problemi legati agli appuntamenti dati dal cup ; nel 9 , 52% dei casi ( 47 esami ) veniva richiesta una mammograa in pazienti con et inferiore ai 35 anni non sintomatiche ; nel 14 , 28% dei casi ( 71 esami ) le pazienti di fronte ad una richiesta di controllo ecograco a 6 mesi non trovando disponibilit presso il cup per effettuare unecograa lavevano sostituita di loro iniziativa personale con una mammograa ( tabella 3 )  . per quanto concerne gli esami di rm , delle 100 richieste ricevute , l83% risultavano inappropriate . 
linappropriatezza deriva per il 35% da richieste di rm come esame aggiuntivo oltre alla combinazione convenzionale mammograa + ecograa , risultate negative , perch le pazienti presentavano mammelle particolarmente dense ; per il 25% deriva da esami richiesti per valutare noduli apprezzabili e stabili ( per morfologia e dimensioni ) nel tempo , individuati allimaging convenzionale e / o gi sotradiol med ( 2013 ) 118 : 984994 cost of 4 , 845.15 euros , while in the remaining 148 patients ( 27.9% ) a mammography - ultrasound discrepancy was shown which led to repetition of the ultrasound examination for a cost of 5 , 311.72 euros , which could have been avoided if the correct diagnostic pathway had been followed ; in this case , rst - line mammography should have been prescribed . of the 250 requests for additional ultrasound following mammography but after a 6to 8 - month period , in 27 cases ( 10.8% ) suspicious lesions were detected which led to cytological characterisation in all cases , which conrmed malignancy in 12 cases ( 48% )  . 
costs associated with this pathway were not considered an unnecessary expenditure since the diagnostic pathway was considered to be correct , even though it should be highlighted that the long waiting lists resulted in a delay in diagnosis of 6 to 8 months . 
 of the 100 mri requests received by our department , in 4 / 100 cases the examination was not carried out due to the existence of major contraindications ( pacemaker , claustrophobia , risk of dislodgement of metallic foreign bodies ) ; in 13 / 100 cases the request was considered appropriate and therefore the associated costs were not considered unnecessary . 
 the 83 inappropriate rmi examinations carried out showed that 44 ( 53% ) patients had negative ndings which resulted in discontinuation of the diagnostic workup , so that the overall expenditure of 10 , 975.80 euros incurred until then was unnecessary . 
the remaining 39 ( 47% ) patients showed ndings which required further diagnostic investigation by means of second - look ultrasound : of these , 34 cases showed enhancement areas which were not related to bilateral masses ; four patients had a nodular area of less than 1 cm in diameter , which was hypointense in t2 - weighted sequences and characterised by contrast enhancement following contrast administration , with no signicant enhancement pattern ; one case showed a nodular area larger than 1 cm in diameter which was hypointense in t2 - weighted sequences , with a malignant enhancement pattern . 
in 135 pazienti ( 25% ) si dimostrata linutilit dellesame ecograco richiesto sulla base di un quadro mammograco a prevalente componente adiposa della mammella , determinando una spesa superua di 4845 , 15 euro , mentre nelle rimanenti 148 pazienti ( 27 , 9% ) stata riscontrata una discordanza mammo - ecograca che ha portato alla ripetizione dellesame ecograco con un costo di 5311 , 72 euro che si sarebbe potuta evitare rispettando liter diagnostico corretto , che nel caso specico , prevedeva lesecuzione dellesame mammograco in prima istanza . delle 250 richieste dintegrazione diagnostica ecograca , successiva ad una mammograa , ma a distanza di 68 mesi da questa : in 27 casi ( 10 , 8% ) sono state evidenziate lesioni sospette , pertanto stata effettuata in tutti i casi una caratterizzazione citologica , che in 12 casi ( 48% ) ne ha confermato la malignit . 
i costi relativi a questo percorso non sono stati considerati inutili e dunque non costituiscono una spesa superua poich liter diagnostico che li ha originati stato considerato corretto , va per sottolineato come i lunghi tempi dattesa abbiano determinato un ritardo nella diagnosi di 68 mesi . 
allo stesso modo non sono stati considerati inutili i 223 casi in cui lesame ecograco risultato negativo , ma comunque necessario per integrare lindagine mammograa . delle 75 richieste desame ecograco in presenza di un precedente esame mammograco con esito negativo , rispettivamente 6 pazienti ( 8% ) presentavano un reperto ecograco che ha reso necessaria una valutazione citologica risultata poi negativa , determinando nel complesso una spesa superua ( ecograa + ago aspirato eco guidato + esame citologico ) pari a 639 , 24 euro ; in 69 pazienti ( 92% ) lesame ecograco non ha riscontrato reperti sospetti determinando una spesa di 2476 , 41 euro . delle 100 richieste di rm a noi pervenute , in 4 / 100 casi lesame non stato effettuato in relazione alla presenza di importanti controindicazioni alla sua esecuzione ( pacemaker , claustrofobia , rischio di motilit di corpi estranei metallici ) ; in 13 / 100 casi la richiesta di esame rm stata considerata appropriata e quindi i costi relativi a questo percorso non sono stati considerati inutili e dunque non costituiscono una spesa superua . degli 83 esami inappropriati di risonanza magnetica che sono stati eseguiti si riscontrato che in 44 ( 53% ) pazienti table 5 cost of diagnosis . 
for the remaining 13 women with echostructural changes in the possible area of the nding ( s ) shown on second - look ultrasound , it was necessary to continue the diagnostic pathway with cytological characterisation of the area of interest . 
the overall cost incurred from october 2010 to december 2010 for ultrasound and mri examinations only was 51 , 235.04 euros ( table 5 )  . radiol med ( 2013 ) 118 : 984994 c stato un esito negativo , che ha permesso la ne degli accertamenti diagnostici facendo ritenere di conseguenza inutile la spesa complessiva sostenuta pari a 10975 , 8 euro . 
 nelle rimanenti 39 ( 47% ) pazienti sono stati riscontrati reperti che hanno reso necessario un approfondimento diagnostico mediante un second look ecograco : di queste , 34 pazienti hanno presentato aree di enhancement non correlate a massa bilaterali ; 4 hanno presentato unarea di diametro inferiore ad 1 cm a morfologia nodulare , ipointensa nelle sequenze t2 pesate , caratterizzata da contrast enhancement dopo somministrazione di mdc con prolo cinetico non signicativo ; in 1 caso si riscontrata la presenza di unarea di diametro maggiore ad 1 cm a morfologia nodulare , ipointensa nelle sequenze t2 pseudonodulare di enhancement , con cinetica di enhancement di tipo maligno . 
 nel second look ecograco effettuato su 39 pazienti , in 26 non sono state evidenziate formazioni sospette , la rm stata ripetuta a distanza di circa 6 mesi ( stabiliti in base alle caratteristiche della lesione ed al quadro iconograco ) , e dopo il successivo follow - up a distanza risultato negativo . 
linappropriatezza delle richieste iniziali ha determinato quindi lesecuzione di tre esami inutili : una prima rm , seguita da un second look ecograco e , a distanza di sei mesi , una successiva rm determinando una spesa sanitaria superua di 13904 , 54 euro . 
le rimanenti 13 donne hanno presentato alterazioni ecostrutturali nella verosimile sede del reperto / i riscontrato al second look ecograco ed stato necessario pertanto proseguire il percorso diagnostico mediante una caratterizzazione citologica nella sede dinteresse . 
c stato un riscontro citologico negativo in 11 pazienti confermato da una rivalutazione rm a distanza di 6 mesi che non ha evidenziato aree di particolare interesse ; il percorso diagnostico di queste pazienti stato di un esame rm , seguito da un esame ecograco di second look , unecograa con prelievo citologico mediante ago aspirato ( vab ) e dalla relativa spesa per lanalisi presso il dipartimento di anatomia patologica di esame citologico ed inne un secondo esame rm per un costo totale di 6659 , 84 euro . 
le rimanenti 2 pazienti hanno avuto un riscontro citologico positivo , ci ha reso necessario proseguire il percorso diagnostico tramite la valutazione istologica del reperto sospetto , mediante un prelievo ( vab ) dal quale si riscontrava un carcinoma in situ che veniva inviato allintervento chirurgico . 
in 1 caso non veniva confermata la positivit del reperto con una spesa di 1110 , 62 euro considerando che la paziente stata sottoposta ad un esame ecograco , una rm seguita da una valutazione ecograca e citologica e , successivamente , caratterizzazione istologica . la spesa superua che abbiamo calcolato in questo studio relativa alle richieste desame di rm di 32650 , 8 euro . 
la spesa globale evidenziata nel periodo intercorso da ottobre 2010 a dicembre 2010 relativa alle sole richieste desame di ecograa e di rm stata di 51235 , 04 euro ( tabella 5 )  . radiol med ( 2013 ) 118 : 984994 discussion discussione in this study we found that approximately 21% ( 493 examinations ) of mammography requests were inappropriate , and in particular that 375 / 493 examinations ( 76.2% ) had been requested as a yearly follow - up examination , but the patients had referred to the centre before the recommended 12 - month period had elapsed . 
for 71 patients ( 14.4% ) , a 6 - month follow - up ultrasound scan had been requested , but the patients had booked a mammography either by mistake or because they had been unable to obtain an appointment for ultrasound examination . ultrasound is the most commonly misinterpreted imaging test after mri , both by patients and by requesting physicians . 
a total of 250 out of 855 examinations ( 30% ) were requests for ultrasound to complete the diagnostic pathway after mammography , which , however , the patients succeeded in booking only 6 to 8 months after mammography . 
in 530 / 855 ( 62% ) cases , the request was for a rst - line ultrasound examination , that is , the patients had no previous recent mammogram , or the gynaecologist requested mammography for regular breast screening alternating it with breast ultrasound in the following years . 
in 75 cases ( 8% ) the ultrasound examination was not indicated since a recent mammogram had shown negative ndings within predominantly fatty breasts . among the mri examinations , a high number of inappropriate requests was found equal to 83% ( 83 exams ) ; in 29 cases ( 35% ) mri was requested as an additional diagnostic investigation following negative results of mammographic or ultrasound examinations in dense breasts . 
moreover , 11 requests ( 13% ) were made by nonradiologists in replacement of mammography + ultrasound or in order to clarify diagnostic doubts resulting from misinterpretation of conventional images . conclusions in recent years , the demand for diagnostic imaging has increased exponentially but it is virtually impossible to meet this demand despite efforts to optimise use of human and technological resources and implement innovative organisatra gli esami mammograci abbiamo potuto constatare che circa il 21% ( 493 esami ) delle richieste risultava non appropriato , in particolare 375 esami ( 76 , 2% ) erano stati richiesti come controllo annuale , ma le pazienti , seppur non trascorsi i 12 mesi consigliati , si erano presentate in anticipo presso il centro . 
in 47 casi ( 9 , 52% ) lesame era stato richiesto in modo non appropriato in relazione alla giovane et delle pazienti ( inferiore ai 35 anni ) ed allassenza di sintomatologia clinica . 
in 71 pazienti ( 14 , 4% ) era stato richiesto un controllo ecograco a distanza di 6 mesi , ma per errore avevano prenotato lesame mammograco o non avevano trovato disponibilit di prenotazione per lesame richiesto . per quanto riguarda gli esami ecograci , rappresentano lindagine strumentale pi frequentemente mal interpretata dopo la rm , sia dalla donna stessa che dai medici richiedenti . 
a 250 ( 30% ) pazienti era stato richiesto un completamento diagnostico dellesame mammograco con lecotomograa , che le stesse erano riuscite a prenotare solo a distanza di 68 mesi dalla mammograa . 
 in 530 ( 62% ) richieste , lesame ecograco risultava di prima istanza ovvero le pazienti non avevano precedentemente effettuato uno studio mammograco recente , oppure il ginecologo richiedeva come indagine strumentale di controllo periodico della mammella una mammograa alternandola con lecograa nei controlli successivi a cadenza annuale . 
 in 75 casi ( 8% ) lecograa non era indicata a seguito di un recente esame mammograco negativo in un quadro di mammelle a prevalente componente adiposa . nella rm stato riscontrato un elevato numero di richieste inappropriate con valori dell83% ( 83 esami ) : in 29 casi ( 35% ) lesame era stato richiesto come ulteriore accertamento diagnostico , a fronte di esami mammograci ed ecograci negativi in quadri di mammelle dense ; in 20 casi ( 25% ) lesame era stato richiesto per la caratterizzazione di noduli evidenziati allecograa . 
inoltre 11 richieste ( 13% ) erano state effettuate da medici non radiologi in sostituzione di mammograa + ecograa o per chiarire dubbi diagnostici dovuti ad una non corretta interpretazione delle immagini di imaging convenzionale da parte dei medici stessi . conclusioni negli ultimi anni abbiamo assistito ad una crescita esponenziale della domanda di esami diagnostici alla quale pressoch impossibile fornire una tempestiva risposta , nonostante gli sforzi di adeguamento delle risorse umane , tecnologiche e di innovativi modelli organizzativi . 
le conseguenze sono rappresentate da una crescita incontrollata della spesa sanitaria , lallungamento dei tempi di attesa , e da un incremento 994 radiol med ( 2013 ) 118 : 984994 tional models . 
as a consequence , healthcare expenditure is rising dramatically , the waiting lists are growing , and many diagnostic tests performed in healthcare facilities are not always justied from a professional and technological point of view . the use of shared guidelines [ 610 ] , known to referring physicians and giving radiologists the opportunity to manage the complete diagnostic pathway , would signicantly reduce the number of inappropriate investigations . patients survival is mostly associated with early diagnosis [ 3 , 11 ]  . 
if the disease is detected at an early stage , when the tumour is still small , the likelihood of cure is very high : in the case of small lesions ( less than 1 cm in diameter ) , 15 - year survival is higher than 90% as compared to the diagnosis of a later - stage tumour , which is larger and has a considerably lower likelihood of long - term survival [ 2022 ]  . 
 this study shows that improving the timeliness of diagnosis is an important objective to be pursued by enhancing the available health services and improving communication and coordination among the different specialists involved , in order to optimise diagnostic pathways and consequently reduce healthcare expenditure . 
 delle prestazioni diagnostiche rese in ambienti sanitari non sempre qualicati sia dal punto di vista professionale che tecnologico . il ricorso alle linee guida [ 610 ] , condivise con i medici che richiedono gli esami , e la possibilit di afdare ai medici radiologi la completa gestione delliter diagnostico , ridurrebbe in maniera signicativa il numero di indagini inappropriate . la possibilit di sopravvivenza delle pazienti in gran parte legata alla diagnosi precoce [ 3 , 11 ]  . 
se la malattia viene scoperta in una fase iniziale , quando le dimensioni del tumore sono ridotte , le probabilit di guarigione sono molto alte : in caso di una piccola lesione , inferiore ad un centimetro di diametro , la sopravvivenza a 15 anni superiore al 90% rispetto ad una diagnosi del tumore in una fase pi avanzata , ovvero quando ha gi raggiunto certe dimensioni e le possibilit di sopravvivenza a distanza si riducono considerevolmente [ 2022 ]  . 
 emerge da questo studio che il miglioramento della tempestivit della diagnosi un obiettivo rilevante da perseguire attraverso un potenziamento dei servizi sanitari a disposizione , tale da migliorare la comunicazione ed il coordinamento tra le diverse gure professionali specialistiche interessate , al ne di ottimizzare i percorsi diagnostici con conseguente diminuzione della spesa sanitaria . 
the area under the receiver operating characteristic ( auroc ) curve for the diagnosis of cirrhosis ( f4 ) with asq was 0.77 , whereas for the diagnosis of any degree of brosis ( f1 ) it was 0.71. 
the auroc for the diagnosis of cirrhosis ( f4 ) with fibroscan was 0.98 , while for the diagnosis of any degree of brosis ( f1 ) it was 0.94. 
asq is a promising new ultrasound software programme which offers encouraging results in the diagnosis of both liver cirrhosis ( f = 4 ) and brosis ( f1 )  . 
larea sottesa alla curva receiver operating characteristic ( auroc ) per diagnosi di cirrosi ( f4 ) con asq risultata 0 , 77 mentre per diagnosi di brosi di qualsiasi grado ( f1 ) stata 0 , 71 . 
lauroc per la diagnosi di cirrosi ( f4 ) con fibroscan risultata 0 , 98 mentre per la diagnosi di brosi di qualsiasi grado ( f1 ) stata 0 , 94 . 
lasq un nuovo e promettente software ecograco che presenta risultati incoraggianti sia nella diagnosi di cirrosi epatica ( f = 4 ) che nella diagnosi di brosi ( f1 )  . 
attualmente tuttavia ancora non sono state raggiunte le performance diagnostiche del fibroscan . parole chiave acoustic structure quantication fibrosi epatica fibroscan 996 introduction hepatic brosis represents the main characteristic of most chronic diseases of the liver [ 1 ]  . 
however , it is an invasive procedure that can cause complications , it is expensive and its diagnostic accuracy may be inuenced by possible sampling errors and interand intraobserver variability . 
moreover , biopsy is able to evaluate only 1 / 50 , 000 of the whole liver parenchyma [ 2 ] and , especially in case of undersized or fragmented samples , it may underestimate hepatic brosis [ 3 ]  . 
in this context , the development of a noninvasive , accurate and consistent test for the diagnosis and grading of hepatic brosis has great importance . transient elastography ( fibroscan , echosens , paris , france ) is without doubt the most commonly used method . 
fibroscan uses an ultrasound impulse to evaluate parenchymal response through the registration of the return echo , thus allowing measurement of the rigidity of hepatic tissue in kpa , which is an indirect index of hepatic brosis . 
these are based on magnetic resonance imaging ( mri ) ( double contrast mri , mr elastography , diffusionweighted imaging or dwi , and perfusion mri ) and on ultrasonography , such as acoustic radiation force impulse or arfi ( siemens , erlangen , germany ) , real - time tissue elastography ( hi - rte ) ( hitachi medical systems europe , zurich , switzerland ) and acoustic structure quantication ( asq ) software ( toshiba medical systems , osaka , japan )  . the aim of our study was to assess the diagnostic accuracy , sensitivity and specicity of asq sonographic software in the assessment of the degree of hepatic brosis in patients with chronic hepatitis c virus ( hcv ) or hepatitis b virus ( hbv ) - related hepatitis , in comparison to fibroscan . materials and methods preliminary evaluation radiol med ( 2013 ) 118 : 9951010 introduzione la brosi epatica rappresenta la caratteristica principale della maggior parte delle epatopatie croniche [ 1 ]  . 
la biopsia epatica viene tuttoggi considerata il gold standard per la valutazione della brosi epatica ; essa tuttavia una procedura invasiva possibile causa di complicanze , una metodica costosa e la sua accuratezza diagnostica pu essere inuenzata da possibili errori di campionamento e dalla variabilit di interpretazione intere intra - osservatore . 
il fibroscan una tecnica che mediante un impulso ultrasonoro permette di valutare la risposta parenchimale attraverso la registrazione delleco di ritorno , consentendo quindi di misurare la rigidit in kpa del tessuto epatico , indice indiretto della brosi epatica . 
recentemente alcune tecnologie emergenti sono state proposte per la diagnosi non invasiva e la classicazione della brosi epatica , basate sulla risonanza magnetica ( rm ) ( doppio contrasto , elasto - rm , diffusion weighted imaging o dwi e rm perfusionale ) , e sullecograa , quali lacoustic radiation force impulse o arfi ( siemens , erlangen germania ) , la real - time tissue elastography o hi - rte ( hitachi medical systems europe , zurigo , svizzera ) ed inne il software ecograco acoustic structure quantication o asq ( toshiba medical systems , osaka , giappone )  . 
 scopo del nostro studio stata la valutazione dellaccuratezza , della sensibilit e della specicit del software ecograco asq nella stima del grado di brosi epatica in pazienti affetti da epatite cronica correlata la virus dellepatite c ( hcv ) o al virus dellepatite b ( hbv ) , ed il confronto con fibroscan . 
all individuals signed an informed consent forthe volunteers were enrolled with the following inclusion criteria : no history of diffuse or focal liver disease assessed through history taking , laboratory examinations [ values in the normal range for serum glutamic oxaloacetic materiali e metodi valutazione preliminare tra giugno e luglio 2010 abbiamo arruolato 20 volontari sani di et compresa tra 27 e 42 anni ( et media 35 ) , radiol med ( 2013 ) 118 : 9951010 transaminase ( sgot ) , serum glutamic pyruvic transaminase ( sgpt ) , - glutamil - transferase ( gt ) , bilirubinaemia , international normalized ratio ( inr ) , serum albumin and cholinesterase and negative for anti - hcv , hcv - rinonucleic acid ( rna ) , hepatitis b antigens ( hbsag ) and hbv - deoxyribonucleic acid ( dna ) ] and standard ultrasound ( us ) examination . 
all volunteers underwent conventional abdominal us and asq with dedicated equipment and 75 mhz convex probe ( aplio xg , toshiba medical systems , osaka , japan ) for the evaluation of the best liver acoustic window for asq assessment . 
 in particular , we captured two images with a right subcostal approach at the level of segments 7 and 8 , one in the best possible axial plane and the second in a sagittal plane , and two images of the left lobe ( orthogonal to each other , axial and sagittal )  . 
subsequent processing of the raw data , done off - line with integrated software , showed that the best asq evaluations with the lowest number of invalid measurements were at the level of segments 7 and 8 with the axial approach , whereas the data obtained with other scans did not provide the same reproducibility . the right segments have , in fact , a higher proportion of parenchyma free of great vascular structures ( vessels easily detectable during a conventional us examination ) and perivascular connective tissue , which are responsible for a remarkable variation in results , not only between different individuals but also within a single patient , as stated in toyoda et al.s [ 4 ] previous experience with asq . 
all the images obtained were used in the asq analysis , by drawing a single region of interest ( roi ) that included the widest portion of hepatic parenchyma free of great vascular structures and calculating the mode , mean and standard deviation ( sd )  . 
the roi was positioned at a depth of 46 cm depending on the dimensions of the liver , as reported in the literature , selecting an area sufciently distant from glissons capsule . before drawing the roi , we consulted the parametric map of each image to make sure it covered an area of hepatic parenchyma representative of the whole echostructure of the liver . 
in addition to the grayscale images , asq is in fact able to provide colour maps based on the distribution of the amplitude of echoes and especially on the scatter , i.e. , the deection of ultrasound wave , produced by different interfaces . 
on the basis of a red to green colour scale , high values of cm2 ( statistical parameter deriving from the different distribution of the amplitude of echoes ) are associated 9 maschi e 11 femmine . 
i volontari sono stati arruolati in considerazione dei seguenti criteri di inclusione : assenza di pregressa storia di malattia diffusa o focale a carico del fegato , valutata tramite anamnesi , esami di laboratorio [ valori nei range di normalit per transaminasi glutammicoossalacetico ( got ) , transaminasi glutammico - piruvica ( gpt ) , - glutammil - transferasi ( gt ) , bilirubinemia , international normalized ratio ( inr ) , albuminemia e colinesterasi ed inoltre negativit per anticorpi anti - hcv , hcv - acido ribonucleico ( rna ) , antigene per lepatite b ( hbsag ) ed hbv - acido deossiribonucleico ( dna ) ] ed esame ecograco standard . 
tutti i volontari sono stati sottoposti ad ecograa convenzionale delladdome e con asq con apparecchiatura dedicata e sonda convex da 75 mhz ( aplio xg , toshiba medical systems , osaka , giappone ) al ne di valutare la migliore nestra acustica epatica per la valutazione con asq . 
 in particolare sono state acquisite due immagini con approccio sottocostale destro a livello dei segmenti vii e viii , una su un piano il pi possibile assiale , laltra su un piano sagittale , e due immagini a livello del lobo sinistro ( sempre ortogonali tra loro , assiale e sagittale )  . 
la successiva elaborazione dei dati grezzi , che viene effettuata off - line con software integrato nellapparecchio , ha dimostrato che le migliori valutazioni asq con il pi basso tasso di misurazioni non valide sono state eseguite al livello dei segmenti vii ed viii con approccio assiale , mentre i dati ottenuti mediante le altre scansioni non permettevano unanaloga riproducibilit . 
nei segmenti di destra infatti maggiore la quota di parenchima scevra da grandi strutture vascolari ( vasi facilmente evidenziabili allesame ecograco convenzionale ) e da connettivo perivasale che determina una notevole variabilit dei risultati non solo tra soggetti diversi , ma anche nel singolo paziente , in accordo con quanto affermato dalla precedente esperienza asq di toyoda et al . 
inne , le valutazioni , effettuate a questo livello , correlano meglio con i risultati della biopsia epatica e del fibroscan , anchessi effettuati a carico dei segmenti vii ed viii . stata anche eseguita una scansione della milza posizionando il paziente in decubito destro per ottenere unimmagine secondo lasse longitudinale . 
lanalisi asq stata condotta su tutte le immagini acquisite , disegnando una singola regione di interesse ( roi ) selezionata in modo da comprendere la pi ampia area di parenchima epatico senza includere grossolane strutture vascolari , per i motivi precedentemente illustrati , calcolando moda , media e deviazione standard ( sd )  . 
1a , b asq examination in an f0 patient , right lobe : a shows an asq ultrasound image of the right hepatic lobe , with a roi already drawn . 
il parenchima mostra bassi valori di cm2 ed una colorazione verde tipica di un parenchima epatico abbastanza omogeneo , mentre il letto vascolare dei vasi epatici leggermente rosso ( valori di cm2 pi elevati )  . with red , while low values of cm2 correspond to green . 
 al ne di includere allinterno della roi unarea di parenchima epatico rappresentativa dellintera ecostruttura del fegato , prima di disegnarla , abbiamo consultato la mappa parametrica di ogni singola immagine . 
parallelamente alle immagini in scala di grigi , infatti , lasq in grado di fornire mappe colorimetriche , basate sulla distribuzione di ampiezza degli echi e soprattutto sullo scatter , cio sulla deessione dellonda ultrasonora , prodotto dalle diverse interfacce . 
basandosi su una scala colorimetrica dal rosso al verde , ad elevati valori di cm2 ( parametro statistico che deriva dalla differenza di distribuzione di ampiezza degli echi ) corrisponde una colorazione rossa , mentre a ridotti valori di cm2 corrisponde una colorazione verde . 
 protocollo di studio e valutazione bioptica tra settembre 2010 e giugno 2011 , 77 pazienti ( 43 maschi e 34 femmine , con un intervallo det compreso tra 27 e 75 anni e con et media 59 anni ) affetti da epatite virale b e c con indicazione alla biopsia epatica per la valutazione della brosi sono stati arruolati nel nostro studio ( tabella 1 )  . 
tutti i pazienti sono stati sottoposti ad ecograa standard delladdome e con asq con apparecchiatura dedicata e sonda convex da 75 mhz ( aplio xg , toshiba medical systems , osaka , giappone ) , a fibroscan ed inne a biopsia epatica nel corso di una settimana . 
 lanalisi del fegato mediante il software asq stata eseguita , in accordo con i risultati della valutazione preliminare sui volontari sani , con un approccio assiale a livello dei segmenti vii ed viii ; mentre la milza stata valutata secondo lasse longitudinale , facendo assumere al paziente decubito laterale destro . 
la fase successiva di posizionamento della roi sulle immagini acquisite stata condotta avendo cura di selezionare unampia area di parenchima priva di grossolane strutture vascolari , per i motivi precedentemente illustrati , calcolando moda , media e sd . 
all patients underwent a standard abdominal us examination and asq with dedicated equipment and 75 mhz convex probe ( aplio xg toshiba medical systems , osaka , japan ) , fibroscan and nally a liver biopsy within a week . 
the bioptic evaluation was used as the gold standard of the diagnostic protocol . letteratura per il corretto posizionamento della stessa [ 4 ]  . entro i sette giorni successivi i pazienti hanno effettuato lelastometria ad impulsi ( fibroscan ) e la biopsia epatica . 
il grado di necroinammazione epatica e lo stadio di brosi sono stati valutati secondo lo score di ishak ( tabella 2 )  . la brosi stata valutata al fibroscan secondo il grading metavir . 
stata quindi utilizzata una scala di conversione per distribuire i pazienti in quattro gruppi , accorpando i gradi f1 e f2 ( metavir ) nel gruppo 2 ( tabella 3 )  . inne , stata effettuata unanalisi statistica tramite lutilizzo del software spss versione 19.0 ( spss inc , chicago , il ) e del software r versione 2.4.1 ( r foundation , vienna , austria )  . acoustic structure quantication il software ecograco asq effettua unanalisi di tipo qualitativo ( mediante lutilizzo di mappe colorimetriche ) e di tipo quantitativo ( mediante calcoli statistici ) per determinare il grado di brosi epatica . 
in condizioni di normalit ( assenza di distorsioni macromolecolari ) lo scatter dellonda ultrasonograca risulta essere minimo o del tutto assente , mentre quando viene distorta larchitettura parenchimale di un organo , come nella brosi epatica , lo scatter risulta aumentato . 
il software asq analizza lo speckle artifact ( traduzione letterale : macchiolina ) prodotto dal fenomeno sico dello scatter attraverso i differenti tessuti ; lo speckle viene rappresentato da numerosi pixel in scala di grigi ed analizzati come dati grezzi . 
 subsequent positioning of the roi on the acquired images was done taking care to select a wide parenchymal area free of great vascular structures , for the reasons previously discussed , calculating mode , mean and sd . 
the roi was positioned at a depth of 46 cm depending on the organ dimensions , referring to the literature for its correct positioning [ 4 ]  . during the following seven days patients underwent transient elastography ( fibroscan ) and liver biopsy . 
queste misurazioni vengono effettuate allinterno di speciche roi disegnate dalloperatore su unimmagine in scala di grigi [ 4 , 5 ]  . fibroscan lelastometria ad impulsi , cio il fibroscan , rappresenta una metodica non invasiva di misurazione della rigidit del tessuto epatico espressa in kpa . 
questo sistema costituito da una sonda ecograca modicata che contiene un vibratore che genera onde elastiche , e un trasduttore ecograco utilizzato sia come emittente che come ricevente di ultrasuoni . 
ad una maggiore velocit di propagazione dellonda elastica corrisponde una maggiore rigidit del tessuto esaminato [ 6 ]  . risultati i 20 volontari arruolati per la valutazione preliminare sono stati inseriti nel gruppo dei pazienti sani . 
scatter or deection of the ultrasound wave is determined by propagation through tissues and it varies according to the acoustic interfaces it encounters . in normal conditions ( absence of macromolecular distortions ) , scatter of ultrasound wave is minimum or completely absent , while it increases when the parenchymal architecture of the organ is distorted , as in hepatic brosis . 
 asq measures the difference ( cm2 ) between a theoretical distribution of echo amplitudes obtained by the statistical analysis of 2 ( result of mean of speckles of healthy livers ) and the real distribution of echo amplitudes recorded in the case under examination . 
the system consists of an ultrasound probe modied in order to contain a vibrator that generates elastic waves and an ultrasonic transducer that is used both as a transmitter and receiver . 
the vibrator transmits , through the ultrasound transducer , vibrations to the hepatic tissues , genle differenze statistiche tra i quattro gruppi di pazienti epatopatici sono state valutate con il coefciente di correlazioni per ranghi di spearman come mostrato in figura 7 . 
 negli stessi pazienti , i valori risultanti dalle misurazioni effettuate con il fibroscan correlavano molto bene con il grado di brosi ( coefciente di correlazione di spearman ( cid : 29 ) = 0 , 88 ; p < 0 , 01 ) come mostrato in figura 7b . laccuratezza diagnostica dellasq rispetto al fibroscan nella stadiazione della brosi epatica stata valutata calcolando la differenza delle aree sottese alla curva receiver operating characteristic ( roc ) ed risultata statisticamente signicativa ( p < 0 , 05 )  . 
considerando questo valore come cut - off per la diagnosi di cirrosi epatica , la sensibilit e la specicit dellasq sono risultate essere 68 , 8% e 62 , 3% , rispettivamente . 
in questo caso , con il cut - off suddetto , la sensibilit e la specicit dellelastometria epatica nella diagnosi di cirrosi epatica sono risultate essere 93 , 8% e 88 , 5% , rispettivamente . 
in b la corrispondente mappa colorimetrica asq evidenzia un lieve aumento del letto vascolare e quindi delle colorazioni in giallo ed in rosso . erating an elastic wave that propagates through the tissue . 
to a higher propagation velocity of the elastic wave corresponds a greater rigidity of the examined tissue [ 6 ]  . results the 20 volunteers enrolled in the preliminary evaluation were entered in the group of the healthy patients . 
in b la corrispondente mappa colorimetrica asq evidenzia elevati valori di cm2 e quindi un aumento della colorazione rossa , tipica della brosi severa . considerando questo valore come cut - off , la sensibilit e la specicit dellasq nella diagnosi di brosi sono risultate essere 71 , 4% e 71 , 4% rispettivamente . 
in questo caso , con il cut - off suddetto , la sensibilit e la specicit dellelastometria epatica nella diagnosi di brosi sono risultate essere 85 , 7% e 82 , 1% , rispettivamente . 
il parenchima mostra bassi valori di cm2 e presenta una colorazione tendente al verde tipica dei tessuti omogenei , con una colorazione tendente al rosso in sede perivasale ( valori di cm2 pi elevati )  . broscan measurement on the hepatic lobe for each group are summarised in table 4 . statistical analysis the statistical differences between the four groups of patients with liver disease were evaluated with spearmans rank correlation coefcient as shown in figure 7 . 
laccuratezza diagnostica della biopsia epatica , inoltre , pu essere inuenzata da possibili errori di campionamento , strettamente correlati alla non uniforme distribuzione del danno epatico , e dalla variabilit dinterpretazione intere intra - osservatore . 
in b la corrispondente mappa colorimetrica asq mostra in verde laspetto omogeneo del parenchima splenico con la presenza di alcuni spot gialli e rossi ( che rappresentano valori di cm2 pi elevati )  . discussion histological evaluation of liver biopsy samples is the only reliable and accepted method for the evaluation of hepatic brosis . 
furthermore , these limits make liver biopsy inappropriate for the questi limiti , rendono la biopsia epatica inadatta per diagnosi e monitoraggio longitudinale nella popolazione generale [ 3 ]  . 
daltra parte rimane insostituibile nei pazienti che necessitano di terapia farmacologica e che si giovano di una stadiazione non solo del grado di brosi epatica , ma anche del grado di inammazione . per tutte queste ragioni negli ultimi anni la ricerca di nuove metodiche non invasive per la determinazione della brosi epatica ha avuto un grande sviluppo , ed in questo contesto sono state descritte diverse metodiche elastograche per la valutazione della rigidit del fegato che si basano su ultrasuoni ad onde trasversali , ed alcune di queste metodiche sono in uso per la valutazione non invasiva della brosi epatica . 
the groups of patients , distinguished by increasing degrees of brosis ( f0 - f4 ) , are represented on the horizontal axis , while the cm2 average ( a ) and kpa ( b ) values are represented on the vertical axis . 
the yellow box represents the values between the rst and third quartile of each group , while the black vertical line represents the extension to the maximum and minimuthe black horizontal line represents the average value . 
i gruppi di pazienti , distinti per gradi crescenti di brosi ( f0 - f4 ) sono rappresentati sullasse delle ascisse , mentre i valori di cm2 average ( a ) e di kpa ( b ) sono rappresenti sullasse delle ordinate . 
il riquadro giallo rappresenta i valori compresi tra il primo e il terzo quartile di valori di ogni gruppo , mentre la linea nera verticale rappresenta lestensione ai valori massimi e minimi . 
nevertheless , liver biopsy remains irreplaceable in patients who necessitate pharmacological therapy and benet from the staging of the degree of hepatic brosis and inammation . for the above mentioned reasons , in recent years there has been a great development of research on new noninvasive methods for the assessment of hepatic brosis . 
we have here described many elastographic techniques for the todica non di imaging , che stata ampiamente studiata e presenta una buona correlazione con la biopsia epatica in termini di specicit e sensibilit , in particolar modo nella brosi hbv / hcv correlata . 
laccuratezza del fibroscan stata valutata in una meta - analisi che riporta sensibilit e specicit della metodica nella diagnosi di brosi signicativa , rispettivamente del 70% e dell84% [ 7 ]  . 
b curva roc per la diagnosi di brosi ( f1 ) con asq ( in blu ) e fibroscan ( in verde )  . evaluation of liver rigidity based on transverse ultrasound waves , some of which are used for the noninvasive evaluation of hepatic brosis . 
it has been studied in depth and presents a good correlation , in terms of specicity and sensitivity , with liver biopsy , in particular in hbv / hcv - correlated brosis . 
 the accuracy of fibroscan has been calculated with a meta - analysis which reported sensitivity and specicity values in the diagnosis of brosis equal to 70% and 84% , respectively [ 7 ]  . 
 among other limitations , it is important to consider that fibroscan is a one - dimensional technique that does not allow assessment and selection , through sonographic images , of the best portion of hepatic parenchyma where to perform measurements . 
moreover , the association of the histological degree of necroinammatory activity and the results of hepatic elastography in patients suffering from chronic viral hepatitis is still controversial [ 8 , 9 ]  . 
some of them are based on the use of contrast medium , such as double contrast mri and perfusion mri ; among the mri techniques that do not use contrast agents , dell87% , e una specicit del 91% . 
tra le altre limitazioni va ricordato che si tratta di una tecnica monodimensionale , che non permette di valutare e scegliere tramite immagini ecograche la porzione di parenchima epatico pi adeguata per effettuare la misurazione . 
inoltre nei pazienti con epatiti virali croniche lassociazione tra il grado istologico di attivit necroinammatoria epatica e il risultato dellelastometria epatica un argomento ancora controverso [ 8 , 9 ]  . 
inne , lesecuzione dellesame difcoltosa nei pazienti obesi o con spazi intercostali stretti ed impossibile nei pazienti con ascite . i maggiori sforzi nel campo della ricerca sono stati fatti sia in rm che in ultrasonograa , ed in particolare si sono focalizzati sulle metodiche elastograche . 
di queste alcune tecniche si basano sullutilizzo dei mezzi di contrasto , come la rm a doppio contrasto e la rm di perfusione ; tra le tecniche di rm non contrastograche le pi interessanti sono lelasto - rm e la rm con sequenze pesate in diffusione . lelasto - rm una promettente tecnica di imaging , non invasiva , che quantica la rigidit del fegato , analizzando la propagazione delle onde meccaniche attraverso il tessuto . 
 [ 11 ] che hanno condotto uno studio su 88 pazienti , la performance diagnostica dellelasto - rm nella stima della brosi epatica , valutata calcolando larea sottesa alla curva roc ( auroc ) risultata essere compresa tra 0 , 91 ( f1 secondo la classicazione di desmet ) e 0 , 99 ( f = 4 secondo desmet ) aumentando quindi allincremento del grado di brosi . 
una migliore capacit predittiva nella distinzione degli stadi di radiol med ( 2013 ) 118 : 9951010 1007 the most important ones are mr elastography and dwi . mr elastography is a promising noninvasive imaging technique that quanties liver rigidity by analysing the propagation of mechanical waves through tissue . 
 [ 11 ] conducted a study on 88 patients and the diagnostic performance of mr elastography in the estimation of hepatic brosis , evaluated by calculating the area under the roc curve ( auroc ) , was between 0.91 ( f1 according to desmets classication ) and 0.99 ( f = 4 according to desmets classication ) , and therefore increased with increasing degrees of brosis . 
he reported 91%95% of sensitivity and 87%95% of specicity for mr elastography in the diagnosis of hepatic brosis , while the dwi sensitivity and specicity results were less signicant ( 84%88% and 68%82% , respectively )  . as far as the ultrasonographic investigations are concerned , the acoustic radiation force impulse ( arfi ) has been used for many years in the evaluation of hepatic brosis . 
arfi , an elastography technology , uses the physical principle by which propagation velocity of ultrasound is proportionally related to the elastic properties of the penetrated medium regardless of wave amplitude [ 13 , 14 ]  . 
 [ 18 ] indicated that real - time tissue elastography did not conrm the diagnostic performance of transient elastography ( fibroscan ) , with auroc values between 0.69 ( for f2 ) and 0.65 ( in the diagnosis of cirrhosis f = 4 )  . these elastography techniques are unable to provide evaluations on the properties of the tissue or information on the heterogeneity of the hepatic structure , even though they can be used to assess its rigidity . 
 asq aims to demonstrate that an increase of the cm2 average value is associated with the increase of the degree of hepatic brosis , making the evaluation of the degree of brosi dellelasto - rm rispetto alla dwi stata dimostrata nel recente studio di wang et al . 
 [ 12 ] che ha riportato una sensibilit della prima del 91%95% e una specicit dell87%95% nella diagnosi di brosi epatica , rispetto a valori di sensibilit e specicit della tecnica dwi relativamente meno signicativi ( rispettivamente 84%88% e 68%82% )  . 
larfi , metodica elastograca , sfrutta il principio sico secondo il quale la velocit di propagazione degli ultrasuoni proporzionale alle propriet elastiche del mezzo attraversato ed indipendente dallampiezza dellonda [ 13 , 14 ]  . 
 [ 15 ] , hanno evidenziato una correlazione signicativa tra la metodica arfi e il grado di brosi , riportando valori di auroc di 0 , 82 e di 0 , 91 nella diagnosi di brosi moderata e di cirrosi . 
 [ 16 ] hanno registrato , invece , unaccuratezza dellarfi nella diagnosi di cirrosi compresa tra 0 , 94 ( sensibilit 93 , 0% , specicit 85 , 1% ) e 0 , 91 ( sensibilit 81 , 5% , specicit 88 , 4% ) utilizzando come reference standard , rispettivamente , il fibroscan e la biopsia epatica . unaltra metodica per la valutazione della brosi epatica lelastosonograa tissutale in real - time come dimostrato da koizumi et al . 
 [ 18 ] avevano affermato che la realtime elastography non replicava la performance diagnostica della transient elastography ( fibroscan ) , con valori di auroc compresi tra 0 , 69 ( per f2 ) e 0 , 65 ( nella diagnosi di cirrosi f = 4 )  . queste metodiche elastograche non possono fornire stime sulle propriet del tessuto o informazioni sulleterogeneit della struttura epatica , nonostante possano essere utilizzate per valutarne la rigidit . 
lasq si propone di dimostrare che un incremento del valore di cm average associato ad un aumento del grado di brosi epatica , rendendo possibile la valutazione del grado di brosi mediante lanalisi delle immagini ecograche bmode . 
queste misurazioni , effettuate a livello del lobo destro , correlano con i risultati della biopsia epatica e del 1008 radiol med ( 2013 ) 118 : 9951010 brosis through the use of b - mode ultrasonography images possible . 
for the patients with chronic liver disease enrolled in our study , the cm2 average values were signicantly correlated to the degree of brosis ( spearmans correlation coefcient = 0.56 ; p < 0.01 ) , and increased linearly with increasing metavir scores . cm2 average measurements obtained at the splenic level did not show signicant changes with increasing degrees of liver brosis . 
this could be due to the moderate but not excellent diagnostic sensitivity of the technique , in particular in comparison to fibroscan , especially in the presence of intermediate degrees of brosis in which the spleen undergoes only limited structural changes . 
moreover , in our preliminary evaluation on healthy volunteers we found that the estimation of brosis depends on the selection of the roi , because inclusion of parenchymal areas rich in vessels , even if small in size , leads to unreliable results related to perivascular brosis or the vacuum effect of the vessel lumen . 
the best correlations are obtained by selecting a roi in parenchymal areas free of evident vessel structures , at an adequate depth ( 46 cm )  . on the other hand , in evaluating our results we must consider that the histological ndings on biopsy samples do fibroscan . 
nei pazienti con epatopatia cronica reclutati nel nostro studio , i valori di cm average sono risultati signicativamente correlati al grado di brosi ( coefciente di correlazione di spearman ( cid : 29 ) = 0 , 56 ; p < 0 , 01 ) , aumentando di pari passo con laumento dello score di metavir . 
questo potrebbe essere spiegato dalla discreta ma non ottima sensibilit diagnostica della tecnica di studio , in particolare rispetto al fibroscan , soprattutto nei gradi intermedi di brosi epatica , in cui la milza subisce modicazioni strutturali di lieve entit . 
ulteriori studi su una pi vasta scala potrebbero essere utili per confermare o smentire il presente risultato . per quanto riguarda laccuratezza dellasq nella diagnosi di brosi il valore di cut - off pi accurato e atto a discriminare pazienti con un grado di brosi maggiore o uguale allo score f1 ( secondo la scala metavir ) risultato essere 135 cm average con una sensibilit del 71 , 4% ed una specicit del 71 , 4% ( auc = 0 , 71 intervallo di condenza 0 , 600 , 83 )  . 
per ci che concerne laccuratezza della metodica nella diagnosi di cirrosi risulta che il valore di cut - off pi accurato e discriminante nel quarto gruppo ( f4 score metavir ) sia 138 cm average con una sensibilit pari al 68 , 8% ed una specicit pari al 62 , 3% ( auc = 0 , 77 ; 95% intervallo di condenza 0 , 650 , 89 )  . i pazienti sono stati arruolati e distinti nei gruppi di appartenenza tenendo conto della valutazione bioptica del grado di brosi , e non sono state valutate le possibili differenze tra i pazienti con epatite hcv e i pazienti con epatite hbv correlata . 
inoltre dalla nostra valutazione preliminare effettuata su volontari sani , risultato che la valutazione della brosi dipende dalla scelta della roi , in quanto linclusione di aree di parenchima ricche di vasi , anche se di piccole dimensioni , determina risultati non attendibili , legati alleffetto di vuoto del lume vasale o alla brosi peri - vasale . 
le migliori correlazioni si ottengono ponendo la roi in aree di parenchima scevre da strutture vasali evidenti , mantenendo sempre una profondit adeguata ( 46 cm )  . daltra parte nella valutazione dei nostri risultati bisogna anche tenere conto che lesito dellesame istologico nei campioni bioptici non sempre rappresenta accuratamente il grado di brosi dellintero fegato . 
sebbene la biopsia epatica sia lo standard di riferimento , i campioni bioptici hanno radiol med ( 2013 ) 118 : 9951010 1009 not always accurately represent the degree of brosis of the whole liver . 
even though liver biopsy is the gold standard , the biopsy samples are small sized and can determine biases in the histological diagnosis of hepatic brosis [ 2 ]  . the diagnostic accuracy of asq in comparison to fibroscan in the staging of hepatic brosis was evaluated by calculating the difference between the areas under the roc curve . 
a statistically signicant difference was detected between the two areas ( p < 0.05 ) , so that asq cannot yet be proposed as a valid diagnostic alternative in the study of hepatic brosis . piccole dimensioni , e possono determinare bias nella diagnosi istologica di brosi epatica [ 2 ]  . laccuratezza diagnostica dellasq rispetto al fibroscan nella stadiazione della brosi epatica stata valutata calcolando la differenza delle aree sottese alla curva roc ed stata rilevata una differenza statisticamente signicativa tra le due aree ( p < 0.05 ) , per cui allo stato attuale lacoustic structure quantication non pu essere ancora proposto come valida alternativa diagnostica nello studio della brosi epatica . conclusions our preliminary experience with asq shows encouraging results in the diagnosis of patients with cirrhosis and in the distinction between patients with and without brosis . 
use of the software during routine ultrasonographic examinations of patients with chronic liver disease makes it possible to combine ultrasonography with a qualitative and quantitative evaluation of hepatic brosis , resulting in a reduction of follow - up time and costs . currently , asq does not equal the diagnostic performance of fibroscan . 
however , we believe that the combined analysis of the several parameters provided by the software ( sd , mode , symmetry in the form of cm2 histogram and peak value of the histogram ) , together with the recent availability of asymmetric rois ( more appropriate for delimiting parenchymal areas free of vessels ) , of the possibility of positioning the roi directly on the parametric map and , nally , of an algorithm for the automatic removal of small vessels included in the roi could improve the diagnostic sensitivity and accuracy of the asq technique . conclusioni la nostra esperienza preliminare con asq dimostra risultati incoraggianti per quanto concerne la diagnosi dei pazienti con cirrosi e nella distinzione tra i pazienti senza brosi dai pazienti con brosi . 
il software utilizzato durante il controllo ecograco routinario dei pazienti epatopatici cronici , consente di combinare studio ecograco e valutazione qualitativa e quantitativa della brosi epatica , con riduzione dei tempi e dei costi del follow - up . 
riteniamo per che lanalisi combinata dei molteplici parametri forniti dal software ( ds , moda , simmetria della forma dellistogramma cm e valore di picco dellistogramma ) , come anche la recente disponibili t di roi asimmetriche , che potrebbero essere pi idonee alla delimitazione di aree di parenchima libere da vasi , della possibilit di posizionare la roi direttamente sulla mappa parametrica e di un algoritmo di rimozione automatica di piccoli vasi inclusi nella roi , potrebbero migliorare la sensibilit e laccuratezza diagnostica della metodica asq . 
giannoni piccin nuova libraria s.p.a. , padova , 2013 isbn : 978 - 88 - 299 - 2219 - 2 published online : 25 july 2013 springer - verlag 2013 when one gets to the last page of this book he is confronted with some questions . 
has he learned from this concise , explanatory text , rich in anatomic references divided into 3 sections ( skull , neurocranium , splanchnocranium ) and 9 chapters ? has he appreciated the rich number of images intended to cover most of the text details ? has he reached throughout the reference lists at the end of each of the nine chapters checking their layouts and correctness ? giunto al termine di questo volume il lettore si pone alcune domande . 
practical and useful hints unable the reader to differentiate between what is normal , variant or pathologic when confronted with skull ct images . all these hints are well illustrated and exemplied by the very large number of images which are the backbone and strength of the book . 
these very beautiful images are made even clearer and understandable by the very clever use of arrows , explanatory words on the images and by their concise captions . then one gets to the references and should feel unsatised and lets say upset , at least if he is as pernickety as i am on this point : references hectic in their layout , inconsistent also in the same journal citation , missing important data such as printers cities , using capital letters for books as well as article citations , reporting also in italian an article published in the ajnr ! typos that we hope to be surely corrected in a second , possible , and well - earned edition . forgetting the above point ( which is in any case a signicant part of the book , as well as a few misprints in the text ) , this book will be appreciated by radiologists and trainees in radiology as well as by those clinicians and staff physicians il testo necessita che il lettore ( se non familiare od aggiornato sullargomento ) ritorni con la mente ai giorni in cui da studente era di fronte al libro di anatomia , in modo tale da rinfrescare le sue conoscenze ed essere in grado di apprezzare in pieno ci che gli autori desiderano rendere noto . suggerimenti pratici ed utili mettono in grado il lettore di differenziare tra ci che normale , variante del normale o patologico quando sia messo di fronte ad immagini tc del cranio . tutti questi suggerimenti sono ben illustrati ed esemplicati da un gran numero di immagini che rappresentano lasse portante e la forza del volume . 
queste bellissime immagini sono rese ancora pi chiare e comprensibili mediante luso assai intelligente di frecce , termini esplicativi direttamente sulle immagini e dalle concise didascalie . quando tuttavia si giunge ai riferimenti bibliograci , ci si sente insoddisfatti se non diciamolo pure innervositi , almeno per chi pignolo come me : voci bibliograche fantasiose nella impostazione , inomogenee anche nella citazione della medesima rivista , che non riportano riferimenti importanti come il nome della citt delleditore , che usano lettere maiuscole per la citazione di volumi ed anche degli articoli , riportando persino in italiano un articolo pubblicato sullajnr ! errori che auspichiamo verranno di sicuro corretti in una ben meritata possibile seconda edizione . non tenendo conto di quanto sopra ( che in ogni caso una parte importante del volume ) come anche di alcuni errori di stampa , questo testo sar apprezzato dai radiologi e dagli specializzandi in radiologia , come anche dai clinici radiol med ( 2013 ) 118 : 12541255 1255 confronted with skull ct images , most of all in the emergency rooms setting where a diagnosis between a variant of the normal or a fracture can have signicant importance to the patient . 
in any case , in the daily work - ow in order to properly diagnose what is normal , variant or pathologic , each diagnosis requiring to having at its base a profound and proper knowledge of the radiological anatomy of the skull which is well illustrated all throughout the books pages . e medici di reparto che si confrontano frequentemente con immagini tc , soprattutto nei reparti di urgenza , dove una diagnosi tra una variante del normale ed una frattura possono essere di importanza signicativa per il paziente . 
between january 2006 and april 2011 , 70 foetuses with a mean gestational age of 28 weeks and 4 days ( range , 1836 ) weeks with vm on foetal mri were assessed in this prospective study . 
half - fourier rapid acquisition with relaxation enhancement ( rare ) t2 - weighted , t1 - weighted and diffusion - weighted ( dwi ) images along the three orthogonal planes according to the longitudinal axis of the mother , and subsequently of the foetal brain , were acquired . 
among them , 11 ( 69% ) had mild ( eight isolated and three associated ) , one ( 6% ) had moderate associated and four ( 25% ) had severe associated vm . 
tra gennaio 2006 e aprile 2011 , 70 feti di et gestazionale media di 28 settimane e 4 giorni ( range 1836 settimane ) con vm alla rm fetale sono stati inclusi in questo studio prospettico . 
sono state eseguite immagini t2 - dipendenti half fourier rare lungo i tre piani ortogonali allasse longitudinale materno e allencefalo fetale , immagini t1 - dipendenti e sequenze in diffusione . 
in 11 / 16 ( 69% ) neonati la rm fetale aveva mostrato vm lieve ( 8 / 11 isolata , 3 / 11 associata ) , 1 / 16 ( 6% ) neonato vm moderata associata , 4 / 16 ( 25% ) neonati vm severa 1200 radiol med ( 2013 ) 118 : 11991211 conclusions . 
lassenza di anomalie associate alla vm e la presenza di una vm di basso grado sono fattori prognostici favorevoli per levoluzione della vm . parole chiave imaging fetale rm diagnosi intrauterina congenito feto introduction introduzione ventriculomegaly ( vm ) represents the most frequent encephalic anomaly seen at foetal magnetic resonance imaging ( mri ) , with an incidence varying between 0.5 and 2 per 1 , 000 births per year [ 1 , 2 ]  . 
prognosis of isolated severe vm is slightly better , with a 33% survival rate at 2 years and normal neurological and physical development in 1062.5% of cases , depending on the study [ 3 , 68 ]  . 
regarding the prognosis of isolated forms , a delay in neurological development can be found in 25% of cases of moderate and in up to 7% of cases of mild vm [ 1 , 6 , 915 ]  . 
progression is associated with a 22% rate of chromosomal anomalies and with a negative prognosis in 44% of cases in comparison with 1% and 7% , respectively , of the forms that do not progress ( stabilisation or regression ) [ 1618 ]  . this study evaluated the evolution of vm diagnosed using foetal mri and compared results with those seen at la ventricolomegalia ( vm ) rappresenta lanomalia encefalica fetale di pi frequente riscontro alla risonanza magnetica ( rm ) fetale , con unincidenza variabile tra 0 , 52 / 1000 nati / anno [ 1 , 2 ]  . 
la diagnosi di ventricolomegalia viene posta quando il diametro atriale ( da ) di uno o entrambi i ventricoli 10 mm ( corrispondente a 4 deviazioni standard sopra la media ) , dalla 14 settimana di gestazione no al termine della gravidanza [ 3 ]  . 
la prognosi per le vm severe isolate , invece , leggermente migliore , con un tasso di sopravvivenza a due anni del 33% e uno sviluppo neurologico e sico normale in percentuali variabili dal 10% al 62 , 5% nei diversi studi [ 3 , 68 ]  . 
per quello che riguarda la prognosi della forma isolata , si pu riscontrare un ritardo nello sviluppo neurologico nel 25% dei casi di vm moderata e nello 07% dei casi di vm lieve [ 1 , 6 , 915 ]  . un altro fattore che inuenza la prognosi della vm isolata , sia moderata che lieve , levoluzione della dilatazione nel corso del tempo . 
la progressione associata a un tasso di anomalie cromosomiche del 22% e ad una prognosi negativa nel 44% dei casi , in confronto con l1% e il 7% rispettivamente delle forme che non progrediscono ( stabilizzazione o regressione ) [ 1618 ]  . radiol med ( 2013 ) 118 : 11991211 1201 postnatal diagnostic imaging , such as transcranial ultrasound ( us ) and encephalic mri . 
 materials and methods patient population between january 2006 and april 2011 , we studied with mri 165 pregnant women ( age range , 1744 years ; mean age , 32 years ) , three of whom had twin pregnancy , for a total of 168 foetuses . 
fifty - ve of 70 ( 78% ) patients ( one twin pregnancy , for a total of 56 foetuses ) agreed to give information about the course of the pregnancy , the delivery and the newborn . 
fifty - three of 55 ( 96% ) pregnancies were brought to ter the twin pregnancy was interrupted owing to the death of one foetus and the nding of cerebral haemorrhage in the other one . 
at birth , 49 / 53 ( 92% ) newborns were alive ; four ( 8% ) died ( one due to bilateral renal agenesis , one due to crouzon syndrome , one due to hydrocephaly and one due to multifactorial causes )  . 
in particular , of the 49 living newborns , 31 ( 63% ) underwent one or more transcranial us , ten ( 20% ) underwent encephalic mri and eight ( 17% ) underwent no postnatal imaging . thirty - four foetuses were assessed in this prospective study on the basis of the following criteria : ( a ) foetal mri nding of either unilateral or bilateral vm ( transverse diameter at the atrial level 10 mm ) ; ( b ) possibility of obtaining information about the pregnancy , the delivery and the newborn from the patient ; ( c ) performance of postnatal diagnostic imaging studies such as transcranial us and / or encephalic mri . 
 vm was considered unilateral when the atrial diameter of a single lateral ventricle was 10 mm with the contralateral ventricle within the normal range of values and bilateral when the atrial diameter of both lateral ventricles was 10 m exclusion criteria were : ( a ) foetal mri diagnosis other than vm ; ( b ) unavailability of the patient ; ( c ) voluntary termination of pregnancy ; ( d ) death of the newborn ; ( e ) lack of postnatal diagnostic imaging studies . foetal mri ndings were then compared with the following postnatal diagnostic imaging studies to evaluate the lobiettivo di questo lavoro stato quello di valutare levoluzione della vm diagnosticata mediante rm fetale , confrontando i risultati ottenuti in rm fetale con le indagini diagnostiche post - natali , come ecograa transfontanellare e rm encefalo . materiali e metodi popolazione dei pazienti nel periodo compreso fra gennaio 2006 e aprile 2011 , abbiamo sottoposto a rm 165 donne in stato di gravidanza ( et materna compresa fra 17 e 44 anni , et media 32 anni ) , 3 delle quali con gravidanza gemellare , per un totale di 168 feti , di et gestazionale ( eg ) compresa fra 18 e 37 settimane ( eg media 28 settimane e 4 giorni )  . 
 cinquantacinque ( 78% ) delle 70 pazienti ( 1 in gravidanza gemellare , per un totale di 56 feti ) hanno fornito informazioni sullandamento della gravidanza , del parto e sul nascituro ; 53 / 55 ( 96% ) gravidanze sono state condotte a termine . 
alla nascita i neonati vitali sono stati 49 / 53 ( 92% ) , 4 / 53 ( 8% ) sono deceduti ( 1 per agenesia renale bilaterale , 1 per sindrome di crouzon , 1 per idrocefalia e 1 per cause multifattoriali )  . 
in particolare su 49 neonati vitali , 31 / 49 ( 63% ) hanno eseguito 1 o pi ecograe transfontanellari , 10 ( 20% ) hanno eseguito la rm encefalo , 8 ( 17% ) neonati non hanno eseguito indagini diagnostiche post - natali . 
le indagini post - natali sono state effettuate entro sei mesi dalla nascita per lesecuzione della ecograa transfontanellare ed entro un anno dalla nascita per lesecuzione della rm post - natale . sono stati inclusi in questo studio prospettico 34 feti secondo i seguenti criteri : ( a ) riscontro mediante rm fetale di ventricolomegalia monolaterale o bilaterale ( diametro trasversale a livello dellatrio 10 mm ) ; ( b ) rintracciabilit delle pazienti al ne di ottenere informazioni sullandamento della gravidanza , sul parto e sul nascituro ; ( c ) esecuzione di indagini diagnostiche post - natali ( eco transfontanellare e / o rm encefalo )  . 
we distinguished the evolution of ventricular dilatation as : progression if postnatal diagnostic imaging studies showed a higher grade of vm compared with the foetal mri ; stability if postnatal diagnostic imaging studies showed a vm of the same grade compared with the foetal mr ; normalisation if postnatal diagnostic imaging studies showed lateral ventricles within normal limits . magnetic resonance technique mr examination was performed with a 1.5 - tesla system ( magnetom symphony , siemens , erlangen , germany ) using a multichannel phased - array surface coil . 
 the examination protocol involved the acquisition of t2weighted half - fourier acquired single - shot turbo spin - echo ( haste ) images along the three planes orthogonal to the maternal longitudinal axis : axial , sagittal and coronal . 
the following parameters were used : time to repetition ( tr ) / time to echo ( te ) / 95 ms , slice thickness 68 mm , matrix 256224 , eld of view ( fov ) 3842 cthese sequences had the main aim of analysing relations between maternal foetal structures and placental characteristics . 
t2 - weighted haste images of the foetal brain where then obtained in the axial , coronal and sagittal planes with the following parameters : tr / te / 95 ms , slice thickness 3 mm , matrix 256256 , fov 3335 cm , with each sequence used as a spatial reference for the subsequent sequence . 
administered. image analysis mr images were independently analysed by two radiologists ( rm , sm ) with obstetric mri experience ; in case of disagreement , the nal decision was reached by consensus . 
 quantitative image analysis was performed at a workstation on the axial and coronal images by a radiologist ( aa ) not involved in the qualitative analysis . quantitative image analysis was performed on axial and la vm stata considerata monolaterale quando il diametro dellatrio ventricolare laterale di un solo ventricolo risultato maggiore / uguale a 10 mm , con il controlaterale compreso nellintervallo dei valori normali ; bilaterale quando il diametro di entrambi gli atri era maggiore / uguale a 10 mm . i criteri di esclusione sono stati : ( a ) diagnosi in rm fetale diversa dalla vm ; ( b ) irreperibilit delle pazienti ; ( c ) interruzione volontaria di gravidanza ; ( d ) decesso del neonato ; ( e ) mancata esecuzione di indagini diagnostiche postnatali . i reperti della rm fetale sono stati quindi confrontati con le successive indagini diagnostiche post - natali al ne di valutare levoluzione della vm . 
abbiamo distinto levoluzione della dilatazione ventricolare in : progressione , se le indagini diagnostiche post - natali mostravano una vm di grado maggiore rispetto alla rm fetale ; stabilit , se le indagini diagnostiche post - natali mostravano una vm dello stesso grado rispetto alla rm fetale ; normalizzazione , se le indagini diagnostiche post - natali mostravano ventricoli laterali nei limiti della norma . risonanza magnetica la rm stata effettuata con un magnete a 1 , 5 tesla ( magnetom symphony , siemens , erlangen , germania ) con limpiego di una bobina multicanale . 
per ridurre la peristalsi intestinale , tutte le donne hanno ricevuto uniniezione intramuscolo di butilscopolamina ( buscopan , schering , germania ) 10 minuti prima dellinizio dellesame . il protocollo desame prevedeva immagini t2 - dipendenti half - fourier acquired single - shot turbo spin - echo ( haste ) lungo i tre piani ortogonali allasse longitudinale materno : assiale , sagittale e coronale . 
i parametri impiegati sono stati : tempo di ripetizione ( tr ) / tempo di eco ( te ) / 95 ms , 68 mm di spessore di scansione , matrice 256224 e 3842 cm di campo di vista ( fov )  . 
 successivamente sono state ottenute immagini t2 - dipendenti haste sullencefalo fetale lungo i piani assiale , coronale e sagittale , mediante i seguenti parametri : tr / te / 95 ms , 3 mm di spessore di scansione , matrice 256256 e 3335 cm di fov ; con ogni sequenza usata come riferimento spaziale per la sequenza successiva . 
il protocollo desame inoltre prevedeva immagini true - fisp , sullencefalo fetale lungo i piani assiale , coronale e sagittale ; i parametri impiegati sono stati : tr / te 4 , 3 / 2 , 1 ms , 5 mm di spessore di scansione , matrice 400400 e 400512 di fov . radiol med ( 2013 ) 118 : 11991211 1203 coronal images and included measuring the transverse diameter of the lateral cerebral ventricles at the atrial level . 
the classication adopted to dene dilatation grade , in accordance with the literature [ 2 , 3 ] , was the following : mild vm : 10 mmad12 mm ; moderate vm : 13 mmad15 mm ; severe vm : ad > 15 mm . qualitative analysis included focal or diffuse alterations in signal intensity of the encephalic tissue ( present / absent ) , presence of corpus callosum , cortical thinning , presence of other intraor extra - axial encephalic malformations , and posterior fossa evaluation . results quantitative analysis qualitative analysis at foetal mri , of 34 newborns with postnatal imaging studies , vm was mild in 25 , moderate in four and severe in ve . we evaluate the presence / absence of associated intraand extra - axial malformations in infants with vm ( table 1 ) : 21 / 25 mild cases were isolated at foetal mri ; four were associated ( one with dandywalker syndrome ; one with corpus callosum complete agenesis and two with alteration of signal intensity due to haemorrhage ) ; 2 / 4 moderate cases were isolated at foetal mri ; two were associated ( one with corpus callosum complete agenesis and one with dandywalker syndrome and alteration of signal intensity by haemorrhage ) ; 5 / 5 severe cases had associated anomalies at foetal mri ( two with corpus callosum complete agenesis ; one with corpus callosum complete agenesis and bilateral alteration of cortical signal intensity ; one with a variant of dandywalker syndrome , alteration of signal intensity and cortical thinning by haemorrhage and one with cortical thinning )  . vm evolution we compared foetal mri to postnatal imaging surveys to evaluate vm evolution . 
foetal mri showed the presence of mild vm in 13 of 16 ( 81% ) newborns , 12 of which were isolated and one associated with alteration of signal intensity by haemorrhage . 
 in nessun caso stata eseguita sedazione materna e fetale n somministrazione endovenosa di chelati del gadolinio . analisi delle immagini le immagini di rm sono state analizzate da due radiologi ( rm e sm ) con esperienza di rm ostetrica , in maniera indipendente ; in caso di discrepanza di interpretazione , la decisione nale stata presa per consenso . 
lanalisi quantitativa delle immagini di rm stata eseguita su workstation da un radiologo ( aa ) non coinvolto nellanalisi qualitativa . lanalisi quantitativa delle immagini stata eseguita su scansioni assiali e coronali e ha compreso la misura del diametro trasversale dei ventricoli cerebrali laterali a livello dellatrio . 
la classicazione adottata per stabilire il grado di dilatazione stata denita in accordo con la letteratura [ 2 , 3 ] : vm lieve : 10 mmda12 mm ; vm moderata : 13 mmda15 mm ; vm severa : da > 15 mm . lanalisi qualitativa ha compreso : alterazioni dellintensit di segnale , focali o diffuse , del tessuto nervoso encefalico ( presenti / assenti ) , la presenza del corpo calloso , di aree di assottigliamento corticale , di eventuali altre malformazioni encefaliche intraed extra - assiali e la valutazione della fossa cranica posteriore . 
in eight of those 11 ( 72% ) cases , vm was isolated , two ( 18% ) had associated anomalies ( one cerebral haemorrhage outcome , one corpus callosum agenesis ) and one ( 10% ) had mild isolated vm with postnatal cerebral mri revealing the presence of lissencephaly not evident on foetal mri . 
nessuno dei casi di vm associata presentava anomalie extra - assiali . evoluzione della vm abbiamo confrontato le rm fetali con le indagini post - natali , al ne di valutare levoluzione della vm . 
la rm fetale di 13 / 16 ( 81% ) neonati aveva mostrato la presenza di vm lieve , 12 delle quali isolate , mentre 1 con associata alterazione dellintensit di segnale da sanguinamento . 
1a - d case of normalisation : foetus 23 weeks and 5 days gestation with isolated mild vm : right lateral ventricle with a maximum diameter of 10 mm ( arrow ) on coronal t2 - weighted haste image ( a )  . 
case of stabilisation : foetus of 31 weeks and 5 days gestation with mild vm ( left lateral ventricle 11 mm ) , as shown on coronal t2 - weighted haste image ( arrow ) ( c )  . 
feto di epoca gestazionale 23 settimane + 5 giorni con ventricolomegalia lieve isolata : ventricolo laterale destro con un diametro massimo di 10 mm ( freccia ) nellimmagine t2 - dipendente haste coronale ( a )  . 
feto alla 31 settimana + 5 giorni di epoca gestazionale con ventricolomegalia lieve isolata ( ventricolo laterale sinistro 11 mm ) , come mostrato nellimmagine t2 - dipendente coronale ( c , freccia )  . 
il complesso ventricolare in asse , lievemente asimmetrico per maggiore evidenza del corno frontale del ventricolo laterale sinistro che presenta diametro trasversale di 4 m tal mri , however , overestimated the situation , giving a nding of complete agenesis of the corpus callosupostnatal mri also detected an arachnoid cyst in the posterior cranial fossa . 
this arachnoid cyst was not identied during the foetal period and was still not retrospectively recognisable in the transverse t2 - weighted haste or diffusion - weighted images ( dwi )  . 
in 1 / 11 ( 10% ) casi di vm lieve isolata , la rm encefalo post - natale ha evidenziato la presenza di lissencefalia , non evidente alla rm fetale . 
quattro su 16 ( 25% ) neonati presentavano vm severa , 2 / 4 ( 50% ) con associata agenesia del corpo calloso , 1 / 4 ( 25% ) con associato assottigliamento corticale . 
in 1 / 4 ( 25% ) la rm encefalo post - natale ha aggiunto , alla diagnosi di vm severa associata ad agenesia del corpo calloso e alterazioni 1206 radiol med ( 2013 ) 118 : 11991211 fig . 
in tal caso la rm encefalo postnatale ha evidenziato il corpo calloso anche se molto assottigliato , laddove la rm fetale invece aveva sovrastimato il quadro dando unagenesia completa del corpo calloso . 
 inoltre , nellindagine post - natale stata diagnosticata una cisti aracnoidea in fossa cranica posteriore , misconosciuta in epoca fetale e non sicuramente individuabile nemmeno retrospettivamente nelle immagini t2 - dipendenti haste e nelle sequenze in diffusione . 
3a - d case of stabilisation : foetus of 30 weeks gestation with severe vm : diameter of the lateral ventricles 17 maxial ( a ) and sagittal ( b ) t2 - weighted haste images show complete agenesis of the corpus callosum with increased depth of interhemispherical ssure , which is separated from the third ventricle only by choroid tela ( arrows )  . 
 the encephalic mri at 3 months of life shows parallel ventricular conguration , suggestive of corpus callosum agenesis , as shown on axial t2 - weighted haste image ( c )  . 
feto alla 30 settimana di epoca gestazionale con ventricolomegalia severa , ventricoli laterali 17 mle immagini assiale ( a ) e sagittale ( b ) t2 - dipendenti mostrano unagenesia completa del corpo calloso , con un maggior approfondimento della scissura interemisferica , che viene separata dal terzo ventricolo solamente dalla tela corioidea . 
 rm a 3 mesi di vita : nellimmagine assiale t2 - dipendente ( c ) si apprezza il tipico aspetto dei ventricoli a decorso parallelo compatibile con lagenesia completa del corpo calloso ; si nota asimmetria per maggior ampiezza del ventricolo laterale di sinistra . 
per quello che riguarda la vm severa ( da > 15 mm ) la prognosi infausta , con un tasso di sopravvivenza a due anni che non supera il 16% nel caso della forma associata e del 33% nella forma isolata [ 3 , 68 ]  . 
in questultimo caso stato riportato uno sviluppo sico e neurologico normale in percentuali variabili dal 10% al 62 , 5% nei diversi studi [ 3 , 68 ]  . nel caso della vm moderata e lieve , il pi importante fattore prognostico lassociazione con altre anomalie . 
5a - f case of progression : foetus of 31 weeks and 5 days gestation with mild vm ( right 11 mm , left 12 mm ) , as shown in axial t2 - weighted haste image ( b )  . 
hypoplastic corpus callosum ( arrow ) is shown on sagittal t2 - weighted rare image ( f ) , in contrast to what is documented on foetal mri ( c )  . 
feto alla 25 settimana + 5 giorni di epoca gestazionale con ventricolomegalia lieve ( destro 11 mm , sinistro 12 mm ) , come mostrato nellimmagine assiale t2 - dipendente ( b )  . 
nellimmagine sagittale t2 - dipendente ( f ) si apprezza iposviluppo del corpo calloso ( freccia ) , che risulta assottigliato ma presente , a differenza di quanto osservato nella rm fetale ( c ) , concomita stenosi dellacquedotto di silvio in rapporto a lieve ipertroa della lamina quadrigemina ( testa di freccia )  . 
nellimmagine assiale t2 - dipendente sulla fossa cranica posteriore ( d ) si apprezza una cisti aracnoidea con ampliamento degli spazi liquorali cisternali della base di sinistra , con minima ipoplasia dellemisfero cerebellare corrispondente . 
 tale cisti aracnoidea stata misconosciuta in epoca fetale e non riconoscibile anche retrospettivamente nellimmagine t2 - dipendente assiale ( a )  . 1208 radiol med ( 2013 ) 118 : 11991211 fig . 
a focal lesion , hyperintense on t2 - weghted images , located in the left temporaloccipitalparietal lobes , is seen in coronal ( a ) and axial ( b ) images . 
catheter draining cerebrospinal uid is seen on the right side ( black arrow ) , with its distal end inside the occipital horn of the same side ( d , e )  . 
nelle immagini t2 - dipendenti haste coronale ( a ) e assiale ( b ) si apprezza una lesione focale , con struttura disomogeneamente iperintensa , con epicentro nei lobi temporo - occipito - parietale di sinistra . 
nelle immagini t2 - dipendenti assiale ( e ) e coronale ( f ) non sono pi apprezzabili i focolai emorragici precedentemente visibili e si evidenzia lasimmetria dei ventricoli laterali . 
 discussion the prognosis of vm in a foetus is mostly affected by the extent of dilatation ( mild , moderate , severe ) , the presence of associated anomalies ( structural , chromosomal ) and the nel 76% dei casi mentre la vm lieve associata nel 41% dei casi ; la prognosi inuenzata dalle anomalie pre senti [ 1 , 6 , 914 ]  . 
severe vm ( ad > 15 mm ) has an unfavourable prognosis , with a survival rate at 2 years that does not exceed 16% in the associated form and 33% in the isolated for in this case , normal neurological and physical development is reported in 1062.5% depending on the study [ 3 , 68 ]  . 
in isolated forms , a delay in neurological development can be found in 25% of cases of moderate vm and in up to 7% of cases of mild vm [ 1 , 6 , 915 ]  . 
progression is associated with a 22% rate of chromosomal anomalies and with a negative prognosis in 44% of cases , in comparison with 1% and 7% , respectively , of the forms that do not progress ( stabilisation or regression ) [ 9 ]  . 
 [ 18 ] of 101 cases of mild and moderate isolated vm , no difference was found between prognosis of regressed , stabilised or progressed vm , as all three kinds of evolution were observed in the group of newborns , with poor neurological outcome . 
 [ 6 ] analysed vm evolution in 106 living newborns out of a sample of 176 vm cases ( divided into three groups based on extent of dilatation : mild , moderate and severe )  . 
they reported improvement / disappearance of vm in 50 cases ( 47% ) , stabilisation in 37 ( 35% ) and worsening in 19 ( 18% ) , correlating such results with prognostic data . 
what emerged from their study was that vm evolution in utero is linked to a better prognosis when vm regresses or disappears , regardless of the extent of dilatation at rst presentation . 
according to the literature , diagnosis and evolution of vm in utero are potentially able to modify the prognosis , and knowledge of how often vm can improve , stabilise or worsen can inuence counselling to parents and the follow - up of pregnancy . 
 moreover , conditions predisposing to vm were present in two foetuses in whom foetal mri did not detected associated anomalies : one case of cytomegalovirus infection during pregnancy and one case of down syndrome . 
in our study , 07% dei casi di vm lieve [ 1 , 6 , 915 ]  . per quello che riguarda levoluzione della dilatazione nelle vm lievi e moderate isolate , la revisione effettuata da melchiorre et al . 
 [ 9 ] riporta che la progressione della vm avviene nel 16% dei casi , mentre una stabilizzazione riportata nel 43% e una normalizzazione in utero avviene nel 41% dei casi . 
la progressione associata a un tasso di anomalie cromosomiche del 22% , a un ritardo dello sviluppo neurologico nel 17% dei casi e a una prognosi negativa nel 44% dei casi , in confronto con l1% ed il 7% rispettivamente delle forme che non progrediscono ( stabilizzazione o regressione ) [ 9 ]  . 
 [ 18 ] su 101 casi di vm lievi e moderate isolate non sono invece emerse differenze nella prognosi tra vm regredite , stabilizzate o progredite , in quanto tutti e tre i tipi di evoluzione si sono osservati nel gruppo dei neonati con uno scarso esito neurologico . 
 [ 6 ] , invece , su un campione di 176 casi di vm ( suddivisi in 3 gruppi , considerando lentit della dilatazione : lieve , moderata , severa ) hanno analizzato levoluzione della vm nei 106 nati vivi , riportando un miglioramento / scomparsa in 50 casi ( 47% ) , una stabilizzazione in 37 casi ( 35% ) e un peggioramento in 19 casi ( 18% ) , correlando tali risultati con il dato prognostico . 
dal loro studio risultato che levoluzione della vm in utero collegata a una prognosi migliore quando la vm regredisce o scompare , indipendentemente dal grado di dilatazione alla prima presentazione . 
in accordo con la letteratura , la diagnosi e levoluzione della vm in utero sono fattori potenzialmente in grado di modicare la prognosi del feto e lessere a conoscenza di quanto spesso una vm pu migliorare , stabilizzarsi o peggiorare inuenza il consulto familiare medico e la gestione della gravidanza . nella nostra casistica , in 16 / 34 ( 47% ) neonati c stata una normalizzazione delle dimensioni dei ventricoli laterali alla nascita . 
inoltre , in 2 feti , in cui la rm fetale non aveva riscontrato anomalie associate , erano presenti condizioni predisponenti la vm : 1 caso di infezione da cmv in corso di gravidanza e 1 caso di sindrome di down . 
nel nostro studio , 10 / 11 ( 91% ) feti con diagnosi di vm associata ad anomalie strutturali intra - assiali hanno mostrato stabilit o progressione di malattia , mentre 12 / 21 ( 57% ) neonati che presentavano diagnosi di vm lieve isolata alla rm fetale si sono normalizzati alla nascita . 
 [ 9 ] , per quello che riguarda le vm lievi e moderate , ab1210 radiol med ( 2013 ) 118 : 11991211 ten of 11 ( 91% ) foetuses with a diagnosis of vm associated with intra - axial structural anomalies showed disease stability or progression , whereas 12 of 21 ( 57% ) with isolated mild vm at foetal mri had normalised at birth . 
 [ 9 ] , we noted progression in one of 29 ( 4% ) cases ( associated vm ) and stabilisation in 12 ( 41% ) : eight of those 12 ( 67% ) were isolated and four were ( 33% ) associated . 
on the other hand , when we compared our data with those of gaglioti et al . , considering mild , moderate and severe vm , there was normalisation in 16 of 34 ( 47% ) of our cases , stabilisation in 16 ( 47% ) and progression in two ( 5% )  . in comparison with literature data , our study evaluated the evolution of vm in a systematic manner , with patients subdivided into groups according to the prenatal extent of ventricular dilatation and to the presence / absence of associated anomalies . 
in addition , it exclusively analysed radiological ndings without correlating them to clinical data regarding patients neurological outcome . consistent with the literature , we found that in the presence of mild isolated vm , an in utero normalisation of the dilatation can be expected with high probability , whereas moderate , severe and associated vm are more likely to remain stable or worsen over time , requiring close postnatal follow - up with both encephalic us and mri . the limitations of our study were a relatively small patient population ( 34 ) , a majority of mild vm ( 25 / 34 ) and the possibility of comparing prenatal and postnatal mri in only a limited number of cases . biamo riportato una progressione in 1 / 29 ( 4% ) caso ( vm associata ) , una stabilizzazione in 12 / 29 ( 41% ) casi : 8 / 12 ( 67% ) vm isolate , 4 / 12 ( 33% ) vm associate . 
confrontando invece i nostri dati con quelli di gaglioti et al . , considerando in toto sia le vm lievi , che moderate e severe , c stata una normalizzazione in 16 / 34 ( 47% ) casi , una stabilizzazione in 16 / 34 ( 47% ) casi e una progressione in 2 / 34 ( 5% ) casi . in confronto con i dati della letteratura , il nostro studio ha valutato levoluzione della vm in modo sistematico , suddividendo i pazienti in gruppi a seconda del grado pre - natale della dilatazione ventricolare e alla presenza o meno di anomalie associate , e ha analizzato esclusivamente il dato radiologico , senza correlarlo con i dati clinici riguardanti la prognosi neurologica dei soggetti . in accordo con i dati della letteratura ne emerso che , in presenza di una vm di basso grado senza anomalie associate , ci si pu aspettare con unalta probabilit una normalizzazione in utero della dilatazione , mentre una vm di grado moderato , severo o con anomalie associate pi probabilmente tenderanno a rimanere stabili o a peggiorare nel tempo , necessitando di uno stretto follow - up post - natale , che includa sia lecograa transfontanellare che la rm . 
 i limiti del nostro studio sono stati quelli di avere avuto a disposizione un campione non molto grande ( 34 pazienti ) , di cui la maggioranza ( 25 / 34 ) con vm lieve , e la possibilit di fare un confronto tra rm fetale e rm post - natale solo in un numero limitato di casi . conclusioni conclusions the higher the vm grade , the higher the probability of associated anomalies identied by foetal mri . 
on the other hand , foetal - associated vm has a high probability of remaining stable at birth . trans - cranial us is a noninvasive technique that does not need sedation of the newborn and is easily repeatable . 
for these reasons it has acquired an important role in managing cases of regression / stability of the condition , allowing monitoring of ventricular dimensions and conrmation of normal cases . postnatal encephalic mri has an important role in cases of vm stability / progression by detecting the cause and directing the patient to neurosurgical intervention when needed . 
per tali motivi ha avuto un ruolo importante nella gestione dei casi di regressione / stabilit di malattia , permettendo di tenere sotto controllo le dimensioni dei ventricoli e confermando eventuali quadri di normalit . la rm encefalo post - natale ha avuto un ruolo importante sia nei casi di stabilit / progressione di malattia , riconoscendo la causa della vm , sia nellindirizzare il paziente allintervento neurochirurgico quando indicato . radiol med ( 2013 ) 118 : 11991211 1211 conict of interest the authors declare that thay have no conict of interest related to the publication of this article 1 . 
imbriaco , via posillipo 196 , 80123 napoli , italy , e - mail : mimbriaco@hotmail.com received : 26 february 2012 / accepted : 16 april 2012 / published online : 27 may 2013 springer - verlag 2013 abstract purpose . 
we retrospectively reviewed the data sets of 828 consecutive patients ( f / m ; 821 / 7 ; mean age , 5011 years ) who underwent breast mr imaging . 
 nellinterpretazione di un esame rm della mammella , 1110 radiol med ( 2013 ) 118 : 11091118 inappropriate management and possible legal issues . keywords breast neoplasm magnetic resonance imaging risulta indispensabile anche la valutazione delle strutture extra - ghiandolari , per evitare terapie inadeguate e possibili problematiche medico - legali . parole chiave mammella neoplasia risonanza magnetica introduction introduzione contrast - enhanced magnetic resonance ( mr ) imaging is an established diagnostic tool for evaluating disease extent in patients with known breast cancer , in monitoring the response to neoadjuvant therapy and in screening patients at high risk for breast carcinoma [ 15 ]  . 
the high sensitivity of this technique results in the discovery of breast lesions that frequently are occult to mammography and ultrasound ( us ) [ 6 , 7 ]  . 
although breast mr imaging is primarily geared towards visualisation of both breasts , incidental extramammary ndings may be detected [ 8 , 9 ]  . the incidence and importance of incidental extramammary ndings on breast mr imaging is not generally known , and the purpose of our large retrospective singlecentre study was to determine the frequency of these ndings , categorise their importance and assess their impact on patient treatment . 
 materials and methods patients we retrospectively reviewed the data sets of 828 consecutive patients ( f / m , 821 / 7 ; mean age , 5011years ; age range , 2383 ) who underwent breast mr imaging at our institution between january 2003 and march 2011 . 
the most common clinical indication for breast mr imaging was to assess lesion extent in patients with known breast tumour ( 380 patients , 46% ) , followed by characterisation of equivocal ndings at conventional mammography and or us ( 331 patients , 40% )  . 
the remaining indications included mr imaging in high - risk women ( 43 cases , 5% ) and examination of patients after breast augmentation therapy ( 74 cases , 9% )  . in the case of suspicious extramammary ndings , further dedicated imaging procedures were performed to conrm breast mr imaging observations . 
 la risonanza magnetica ( rm ) della mammella rappresenta una metodica estremamente accurata nella valutazione dellestensione di malattia nelle pazienti con neoplasia mammaria nota , nel monitoraggio della risposta alla terapia neo - adiuvante e nello screening delle pazienti ad alto rischio per eteroplasia mammaria [ 15 ]  . 
sebbene un esame rm della mammella abbia come scopo principale la valutazione delle ghiandole mammarie , reperti incidentali extra - mammari sono spesso identicati al di fuori del campo di vista delle ghiandole mammarie ; questo stato dimostrato in alcuni recenti lavori [ 8 , 9 ]  . lincidenza e limportanza dei reperti incidentali extramammari riscontrati allesame rm della mammella non generalmente conosciuta e , pertanto , lo scopo di questo ampio studio retrospettivo stato di determinare la frequenza di tali reperti , di categorizzarne limportanza e di valutarne limpatto clinico sulla terapia delle pazienti . 
 materiali e metodi pazienti lo studio stato eseguito in un singolo centro e retrospettivamente sono stati rivalutati gli esami rm della mammella di 828 pazienti ( f / m 821 / 7 , et media 5011 anni , range 23 / 83 ) , che sono state sottoposte allesame rm presso il nostro istituto da gennaio 2003 a marzo 2011 . 
la pi comune indicazione clinica allesame rm della mammella stata la valutazione dellestensione di malattia nelle pazienti con neoplasia mammaria nota ( 380 pazienti , 46% ) , seguita dalla caratterizzazione di risultati equivo ci o non conclusivi allimaging mammograco ed ecograco convenzionale ( 331 pazienti , 40% )  . 
le restanti indicazioni includevano pazienti ad alto rischio per eteropla sia mammaria ( 43 casi , 5% ) e la valutazione di pazienti sottoposte a intervento di mastoplastica additiva ( 74 casi , 9% )  . nei casi di riscontro di lesioni sospette extra - mammarie , radiol med ( 2013 ) 118 : 11091118 breast mr imaging technique for all mr examinations , we used a 1.5 - tesla system ( gyroscan , intera , philips , the netherlands ) with a dedicated surface breast coil . 
the total duration of the dynamic study was approximately 6 mafter the examination , subtraction images were obtained by subtraction of the unenhanced images from the rst contrast - enhanced image on a pixel by pixel basis . breast mr image interpretation breast mr image interpretation was performed at the time of image acquisition , separately and in a random order . 
all mr images were retrospectively reviewed , and the presence of an extramammary incidental nding was determined in consensus by two experienced breast radiologists with 12 ( mi ) and 8 ( di ) years of experience , respectively , in breast mr imaging . results collateral ndings were detected in 282 / 828 ( 34% ) patients , with a prevalence of extramammary ndings in examinations obtained for assessing lesion extent in patients with known breast tumour ( 52% )  . 
in the 282 patients with collateral ndings , 480 incidental lesions were found ; of these , 230 ( 48% ) were intrathoracic and the remaining 250 ( 52% ) were extrathoracic . the most common site of localisation was the liver , with 231 / 480 cases ( 48% )  . 
the second most relevant group of collateral ndings consisted of bony lesions ( 99 / 480 ; 21% ) , followed by mediastinal and axillary lymph nodes ( 70 / 480 ; 14% ) , lung parenchyma ( 36 / 480 ; 8% ) and other sites ( 44 / 480 ; 9% )  . 
in particolare , sono stati eseguiti esami di tomograa computerizzata ( tc ) del torace e delladdome , esami ecograci ed esami dedicati rm del rachide dorsale o del fegato e scintigraa ossea con tc99m - mdp . 
le pazienti sono state studiate in posizione prona con entrambe le mammelle alloggiate allinterno di unantenna dedicata per limaging della mammella , cercando di evitare la compressione delle ghiandole mammarie durante lesecuzione dellesame . 
dopo avere acquisito una sequenza t2 - pesata secondo un piano sagittale [ tempo di ripetizione ( tr ) / tempo di eco ( te ) : 8 , 990 / 107 ] , stata ottenuta una sequenza t1 con soppressione del grasso 2d fast spoiled recalled echo ( 8 , 89 / 1 , 7 ; ip angle 12 ; matrice 256256 ; campo di vista 1618 cm2 ) secondo un piano assiale , che stata eseguita prima e 5 volte dopo la somministrazione rapida a bolo di 0 , 1 mmol / l di gadopentetato dimeglumina ( magnevist , bayer schering pharma ) per kilogrammo di peso corporeo , a una velocit di iniezione di 2 , 0 ml / s . 
 interpretazione della rm della mammella linterpretazione della rm mammaria stata effettuata al momento delle acquisizioni , separatamente e in ordine randomizzato da due radiologi con esperienza nellimaging della mammella ( mi e di )  . 
tutte le immagini di risonanza sono state successivamente rianalizzate e la presenza di reperti extra - mammari stata effettuata in modo congiunto da due esperti radiologici dellimaging senologico , rispettivamente con 12 anni ( mi ) e 8 anni ( di ) di esperienza nellimaging rm della mammella . 
 risultati nel gruppo totale di pazienti sono stati riscontrati reperti 1112 radiol med ( 2013 ) 118 : 11091118 table 1 nonsignicant extramammary ndings ( n = 414 ) incidentally detected on breast magnetic resonance imaging in 244 patients findings liver cysts bone haemangioma axillary / mediastinal lymph nodes lung parenchyma nodules liver haemangioma radicular cyst gallbladder lithiasis splenic cyst hiatus hernia poland syndrome focal hepatic steatosis hepatic adenoma mild pleural effusion bronchiectasis thyroid goitre reperti cisti epatica emangioma osseo linfonodo ascellare / mediastinico noduli parenchimali polmonari emangioma epatico cisti radicolare litiasi vescicale cisti splenica ernia iatale sindrome di poland steatosi epatica focale adenoma epatico moderata diffusione pleurica bronchiectasia gozzo tiroideo n ( % ) 210 ( 51 ) 72 ( 17 ) 55 ( 13.3 ) 26 ( 6.3 ) 14 ( 3.4 ) 12 ( 2.9 ) 9 ( 2.2 ) 8 ( 1.9 ) 2 ( 0.5 ) 1 ( 0.25 ) 1 ( 0.25 ) 1 ( 0.25 ) 1 ( 0.25 ) 1 ( 0.25 ) 1 ( 0.25 ) n ( % ) 210 ( 51 ) 72 ( 17 ) 55 ( 13 , 3 ) 26 ( 6 , 3 ) 14 ( 3 , 4 ) 12 ( 2 , 9 ) 9 ( 2 , 2 ) 8 ( 1 , 9 ) 2 ( 0 , 5 ) 1 ( 0 , 25 ) 1 ( 0 , 25 ) 1 ( 0 , 25 ) 1 ( 0 , 25 ) 1 ( 0 , 25 ) 1 ( 0 , 25 ) tabella 1 reperti incidentali extra - mammari non signicativi ( n = 414 ) riscontrati alla rm della mammella , in 244 pazienti sions , 15 mediastinal / auxiliary lymph nodes , six metastatic lung lesions , ve metastatic liver lesions , four pneumonitis , two aneurysms of the ascending aorta , two adrenal adenomas , one neurobroma of the back , one multiple myeloma , one mediastinal lymphoma , one sternal amyloidosis , one left ventricular dilatation and one trapezium lipoma . 
 tables 1 and 2 summarise the extramammary ndings , and figures 13 show examples of those ndings . discussion the results of this study demonstrate that a signicant number of patients who underwent breast mr imaging had incidental extramammary ndings ; of these collateral ndings , collaterali in 282 / 828 ( 34% ) casi , con una prevalenza di reperti extra - mammari nei casi di pazienti studiate per valutare lestensione di malattia con eteroplasia mammaria nota ( 52% )  . 
nelle 282 pazienti con reperti collaterali , stato riscontrato un totale di 480 reperti incidentali ; di questi , 230 ( 48% ) erano intra - toracici , mentre i restanti 250 ( 52% ) erano extra - toracici . 
il secondo gruppo pi rilevante di reperti collaterali sono state le lesioni ossee ( 99 / 480 ; 21% ) , seguite dai linfonodi mediastinici e ascellari ( 70 / 480 ; 14% ) , dal parenchima polmonare ( 36 / 480 ; 8% ) e da altre localizzazioni ( 44 / 480 ; 9% )  . 
di questi , 26 risultavano lesioni ossee metastatiche , 15 linfonodi mediastinici e / o ascellari , 6 metastasi polmonari , 5 metastasi epatiche , 4 polmoniti , 2 aneurismi dellaorta ascendente , 2 adenomi surrenalici , 1 neurobroma del dorso , 1 mieloma multiplo , 1 linfoma mediastinico , 1 amiloidosi sternale , 1 cardiomiopatia dilatatativa del ventricolo sinistro , 1 lipoma del trapezio . le tabelle 1 e 2 riportano i reperti extra - mammari non signicativi e signicativi , riscontrati incidentalmente in 282 pazienti . 
 discussione i risultati di questo ampio studio retrospettivo dimostrano che un numero signicativo di pazienti che si sottopongono a esame rm della mammella , presentano reperti incidentali extra - mammari ; di questi , il 14% ha una rilevanza clinica , necessitando ulteriori approfondimenti diagnostici . 
pertanto , linterpretazione della rm mammaria dovrebbe incorporare unattenta analisi delle strutture adiacenti extra - mammarie , allo scopo di riconoscere quelle lesioni signicative che possono modicare la prognosi e il trattamento delle pazienti che si sottopongono a esame rm della mammella . 
 la rm stata utilizzata con successo nellimaging della mammella , essendo in grado di fornire eccellenti dettagli del parenchima mammario con un alta qualit e unelevata risoluzione di contrasto [ 14 ]  . 
in particolare , sempre pi crescente lutilizzo della rm mammaria per valutare lestensione di malattia nelle pazienti con eteroplasia mammaria nota , nel monitoraggio della risposta alla terapia neoadiuvante e nello screening delle pazienti ad alto rischio per eteroplasia mammaria ; grazie anche allelevata sensibilit della rm nellidenticazione delle lesioni mammarie , che spesso sono occulte allimaging convenzionale mammograradiol med ( 2013 ) 118 : 11091118 1113 table 2 signicant extramammary ndings ( n = 66 ) incidentally found on breast magnetic resonance ( mr ) imaging in 38 patients tabella 2 reperti incidentali extra - mammari signicativi ( n = 66 ) riscontrati alla risonanza magnetica ( rm ) della mammella , in 38 pazienti findings bone metastases mediastinal / axillary lymph nodes lung metastases liver metastases pneumonitis ascending aorta aneurysm adrenal adenoma dorsal neurobroma multiple myeloma mediastinal lymphoma sternal amyloidosis left ventricular dilatation trapezium lipoma ct , computed tomography ; pet , positron - emission tomography ; us , ultrasound n ( % ) 26 ( 39 ) 15 ( 23 ) 6 ( 9 ) 5 ( 8 ) 4 ( 6 ) 2 ( 3 ) 2 ( 3 ) 1 ( 1.5 ) 1 ( 1.5 ) 1 ( 1.5 ) 1 ( 1.5 ) 1 ( 1.5 ) 1 ( 1.5 ) reperti metastasi osee linfonodo ascellare / mediastinico metastasi polmonari metastasi epatiche polmonite abneurisma dellaorta ascendente adenoma adrenale neurobroma dorsale mieloma multiplo lymphoma mediastinico amiloidosi sternale dilatazione ventricolare sinistra lipoma del trapezio tc , tomograa computerizzata ; pet , tomograa ad emissione di positroni n ( % ) 26 ( 39 ) 15 ( 23 ) 6 ( 9 ) 5 ( 8 ) 4 ( 6 ) 2 ( 3 ) 2 ( 3 ) 1 ( 1 , 5 ) 1 ( 1 , 5 ) 1 ( 1 , 5 ) 1 ( 1 , 5 ) 1 ( 1 , 5 ) 1 ( 1 , 5 ) 14% had clinical relevance and deserved further diagnostic investigation . 
therefore , the interpretation of breast mr imaging should incorporate a careful analysis of the adjacent extramammary structures in order to recognise signicant lesions that may modify the patients prognosis and treatment . mr imaging has been successfully used in breast imaging because it provides excellent depiction of the details of breast parenchyma with high - quality contrast resolution [ 1 4 ]  . 
in particular , the use of breast mr imaging to evaluate disease extent in patients with known breast cancer , monitor response to neoadjuvant therapy and screen patients at high risk for breast cancer is signicantly increasing , and the high sensitivity of mr imaging has resulted in the discovery of breast lesions that are frequently occult to conventional diagnostic procedures , such as mammography and us [ 10 , 11 ]  . 
 [ 12 ] hanno prospettivamente analizzato la prevalenza e la rilevanza di reperti incidentali in 1013 pazienti sottoposte a rm della mammella nel follow up post - terapia per neoplasia mammaria , nella stadiazione preoperatoria e nello screening di pazienti ad alto rischio per eteroplasia mammaria , cos come per la valutazione di casi equivoci o non diagnostici allimaging senologico convenzionale , con mammograa ed ecograa . in questo lavoro , i reperti incidentali extra - mammari sono stati riscontrati in 92 ( 9% ) dei 1013 pazienti . 
1a , b a 50 - year - old woman with a solitary lung lesion identied in the posterior segment of the right lower lobe on t2 - weighted breast mr imaging ( a , arrow )  . 
1a , b donna di 50 anni , con rilievo allesame rm della mammella , sulla sequenza t2 - pesata , in corrispondenza del segmento posteriore del lobo polmonare inferiore di destra , di un nodulo singolo polmonare ( a , freccia ) ; la paziente stata sottoposta successivamente a esame tc del polmone ( b , freccia ) e ad agobiopsia e la diagnosi nale stata di amartoma polmonare . 
2a , b a 67 - year - old woman with a solitary lung lesion identied in the lingular segment of the left lung on t2 - weighted breast mr imaging ( a , arrow )  . 
2a , b donna di 67 anni , con rilievo allesame rm della mammella , sulla sequenza t2 - pesata , in corrispondenza del segmento lingulare del polmone di sinistra , di un nodulo singolo polmonare ( a , freccia ) ; la paziente stata sottoposta successivamente a esame tc del polmone ( b , freccia ) e ad agobiopsia e la diagnosi nale stata di metastasi polmonare , da carcinoma primitivo della mammella . 
3a , b donna di 48 anni , con rilievo allesame rm della mammella , di unarea focale di basso segnale in t2 ( a , freccia ) in corrispondenza di un metamero del rachide dorsale , a livello di t9 ; questa lesione mostrava intensa captazione di fdg allesame pet ( b , freccia ) e la diagnosi nale stata di metastasi vertebrale , da carcinoma primitivo della mammella . 
 [ 12 ] prospectively analysed the prevalence and relevance of incidental ndings in 1 , 013 patients undergoing breast mr imaging as follow - up after breast cancer therapy , for preoperative staging and for screening of high - risk patients as well as for clarication of unclear clinical examinations or inconclusive conventional mammograms . 
furthermore , mr imaging had markedly more incidental extramammary ndings in staging ( 39.5% ) and follow - up ( 11.6% ) examinations , with a prevalence of incidental malignant ndings of 81% in patients examined for preoperative staging . 
however , in our series , of the 231 incidentally discovered liver lesions , only ve were metastatic hepatic lesions ; in all other cases , lesion morphology , homogeneous signal intensity and specic diagnostic examinations , including us and ct , allowed us to exclude the malignant nature of these lesions . 
 our ndings are also consistent with previous data by khalil negli studi di stadiazione ( 39 , 5% ) e di follow - up ( 11 , 6% ) , con una prevalenza di reperti incidentali maligni dell81% nelle pazienti studiate per la stadiazione preoperatoria [ 12 ]  . 
in accordo con questo studio , nel nostro lavoro la maggiore prevalenza di reperti incidentali extra - mammari stata a livello del fegato ; tuttavia , nel nostro studio , delle 231 lesioni incidentali epatiche , solo in 5 casi abbiamo riscontrato lesioni metastatiche ; in tutti gli altri casi , la morfologia delle lesioni , lomogenea intensit di segnale allesame rm e lintegrazione con esami specici mirati come la tc e lecograa hanno permesso di escludere la natura maligna di queste lesioni . 
 [ 15 ] , che hanno mostrato che la probabilit di una lesione epatica di essere maligna inferiore al 20% , anche in pazienti con neoplasia mammaria primitiva nota . nei casi di lesioni parenchimali polmonari incidentali , la tc e lesame pet - tc con fdg sono state le prime scelte diagnostiche per caratterizzare e discriminare la natura delle lesioni sospette e , inne , in tutti i casi di lesioni incidentali ossee , la rm con sequenze dedicate o la scintigraa ossea ci hanno aiutato per caratterizzare meglio le lesioni ossee incidentali riscontrate allesame rm della mammel1116 radiol med ( 2013 ) 118 : 11091118 et al . 
 [ 14 , 15 ] , who showed that the probability of a hepatic lesion being malignant is < 20% , even in patients with known primary breast cancer . in cases of incidental lung parenchymal lesions , ct and uorodeoxyglucose positron - emission tomography / ct ( fdg - pet / ct ) scan were the rst choices by which to characterise and discriminate the nature of these suspicious lesions . 
the typical features of these metastases were low signal intensity on t1 - weighted images and high signal intensity on t2 - weighted images , without evidence of enhancement on postcontrast images . 
it is well known that normal bone marrow gives high signal intensity on mr imaging due to its fat content , but when normal fatty marrow is inltrated by tumour , there is a focal decrease in signal intensity [ 1418 ]  . 
in particular , in our study , 39% ( 26 / 66 ) of signicant extramammary ndings , in nine patients , were occult bony metastases conrmed either by bone scintigraphy or mr performed with dedicated sequences ; all these patients were therefore eligible for adjuvant therapy ( either chemotherapy or hormonal therapy ) rather than surgical therapy , as has been initially planned before the mr examination . 
 regarding lymph node involvement , we adopted a lymph node size of 1.5 cm combined with a long - to - short - axis ratio of < 1.6 as the most accurate criterion to dene the presence of a pathological lymph node [ 19 ]  . 
this is probably due to the lower contrast resolution of the axial enhanced t1 - weighted 2d fast spoiled recalled echo sequence that we used compared with the most recent and innovative t1 - weighted 3d techniques . 
finally , our success in characterising incidentally detected lesions la ; in particolare , nel nostro studio la maggioranza delle metastasi ossee scoperte come reperto incidentale erano localizzate a livello del rachide dorsale ; le caratteristiche tipiche di tali metastasi erano un basso segnale nelle sequenze dipendenti dal t1 e un elevato segnale in t2 , senza segni di impregnazione sulle sequenze post - contrastograche ; ben noto che il midollo osseo normale presenta un elevato segnale in rm a causa del suo contenuto adiposo ; tuttavia , quando il normale segnale del grasso midollare risulta inltrato da tessuto eteroplasico , vi una riduzione focale della normale intensit di segnale [ 1418 ]  . 
questi risultati sono particolarmente importanti , dal momento che lidenticazione di metastasi ossee occulte pu inuire sulla terapia di queste pazienti , che richiederanno una terapia sistemica al posto di una terapia locale . 
in particolare , nel nostro studio il 39% ( 26 / 66 ) dei reperti incidentali extra - mammari , in 9 pazienti , sono risultate metastasi ossee occulte confermate sia dalla scintigraa ossea che dalla rm eseguita con sequenze dedicate ; tutte queste pazienti sono state pertanto indirizzate a una terapia adiuvante ( con chemioterapia o ormonoterapia ) invece che a una terapia chirurgica , cos come era stato programmato , prima di eseguire la rm della mammella . 
riguardo al coinvolgimento linfonodale , abbiamo adottato una dimensione massima di 1 , 5 cm o pi grande di tale valore , assieme al rapporto tra lasse lungo e lasse corto < 1 , 6 , come il parametro pi accurato per denire la presenza di un linfonodo patologico [ 19 ]  . 
 lo studio era retrospettivo e la popolazione dei pazienti stata ristretta a una sola istituzione ed molto verosimile che lincidenza e limportanza dei reperti incidentali possa variare in base alle caratteristiche delle pazienti che si sottopongono allesame rm della mammella . 
unaltra limitazione del nostro studio stata che la maggior parte dei reperti extra - mammari stata scoperta sulle sequenze t2 - pesate morfologiche ; ci probabilmente dovuto alla pi bassa risoluzione di contrasto delle immagini assiali t1 - pesate 2d fast spoiled recalled echo che abbiamo utilizzato , in confronto alle pi recenti e innovative tecniche di studio t1 - 3d . 
inne , il nostro successo nel caratterizzare le lesioni incidentali ha verosimilmente beneciato della revisione di tutti gli studi prima della dimissione delle pazienti e nellesecuzione di ulteriori sequenze dedicate , laddove fosse necessario . con lavvento delle apparecchiature di rm a 3 tesla , radiol med ( 2013 ) 118 : 11091118 1117 probably benets from reviewing all studies before the patient is dismissed and by performing additional sequences as necessary . 
 with the advent of 3 - tesla mr scanners , it is reasonable to hypothesise an increasing use of higher eld - strength mr scanners in clinical settings and breast imaging in the near future . 
benign lesions , most notably hepatic cysts , are by far the most frequent ndings ; however , a small but not negligible percentage of patients have signicant ndings that deserve further diagnostic investigation . 
 therefore , this relatively high incidence of extramammary incidental ndings emphasises the importance of breast mr examinations being performed and interpreted by radiologists with a high level of expertise and training in breast mr imaging so as to avoid diagnostic errors and possible legal issues . acknowledgements the authors sincerely thank graciana diezroux for critically reviewing this paper , and guglielmo caprio , gennaro fraia and fabio garbino for their valuable technical assistance in making this study possible . ipotizzabile che , in un prossimo futuro , venga incrementato lutilizzo di macchine ad alto campo magnetico nella pratica clinica e , in particolare , nellimaging della mammella ; il migliore rapporto segnale / rumore dei sistemi a 3 tesla pu tradursi in una migliore risoluzione spaziale e di contrasto e nella diagnosi di un pi ampio numero di piccole lesioni extra - mammarie , in confronto alle apparecchiature da 1 , 5 tesla ; pertanto , i radiologi dovrebbero essere attenti alla possibilit di riscontro di lesioni incidentali extra - mammarie , in particolare quando lavorano con sistemi rm ad alto campo . 
le lesioni benigne epatiche e , in particolare , le cisti sono di gran lunga le pi frequenti ; tuttavia , una piccola e signicativa percentuale di pazienti presentano reperti signicativi che necessitano di ulteriori approfondimenti diagnostici . 
pertanto , questa relativa alta incidenza di reperti incidentali extra - mammari , accentua limportanza di una corretta esecuzione e interpretazione della rm della mammella , da parte di radiologi con elevata esperienza e preparazione nellimaging rm mammario , allo scopo di eliminare possibili errori dignostici ed eventuali problematiche medico - legali . 
 ringraziamenti gli autori ringraziano la dottoressa graciana diez - roux , phd per la revisione del manoscritto e i tecnici guglielmo caprio , gennaro fraia e fabio garbino per il loro aiuto tecnico , che ha reso possibile lesecuzione degli esami rm della mammella . 
nieder springer - verlag berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 642 - 19924 - 0 e - isbn : 978 - 3 - 642 - 19925 - 7 published online : 25 july 2013 springer - verlag 2013 keeping in mind that lung cancer is the leading tumourous killer with more than 1.6 million new cases diagnosed yearly world - wide with a dismal 5 year survival rate , one will open this hefty book with great curiosity and expectations ; including expectations on tumour biology , clinical , instrumental and imaging diagnosis , therapy and end - results . 
tutte le differenti sfaccettature di questi argomenti sono presentate e discusse ampiamente , avendo sempre presenti le ben note differenze esistenti tra i tumori del polmone non a piccole ed a piccole cellule . in questo volume di 836 pagine , il lettore trover 58 capitoli suddivisi in dodici parti dedicate alla presentazione e discussione dei seguenti argomenti : basi scientiche del tumore del polmone ; indagini cliniche ; considerazioni di base sul trattamento ; strategie attuali nel trattamento del tumore del polmone non a piccole cellule in fase iniziale ; strategie attuali nel trattamento del tumore polmone non a piccole cellule in fase localmente avanzata ; strategie attuali nel trattamento del tumore del polmone a piccole cellule ; trattamento in gruppi particolari di pazienti ed in altri scenari ; tossicit associata al trattamento ; studi sulla qualit della vita e sui fattori prognostici ; progressi tecnici nella terapia del tumore del polmone ; progressi biologici nel tumore del polmone per terminare con ricerca clinica nel tumore del polmone . 
 for those who are not familiar with or used to reading the results of different clinical trials it will not be easy to unravel with the different data gathered and presented even when these trials are sponsored and performed under the aegis of very serious international scientic societies . 
to resolve these conundrum , hints are given on how well - designed and prospective large and randomized clinical trials and proper meta - analyses are needed and ongoing in order to provide radiotherapists , clinicians and surgeons with sound results to be used in what translational medicine refers to as bench to bedside to benet the patient . 
these trials should offer up - to - date and continuously enforced evidence to guide professionals in the optimal planning of radiotherapy alone or combined with chemotherapy and surgery , in order to reduce possible associated toxicities . 
 once again , in this review i have to complain about the acronyms : in this book only 6 out of the 58 chapters list the acronyms to be found in the text . 
for the remaining 52 chapters as i am not familiar with the acronyms , i had to ll in 6 pages with abbreviations just to keep abreast with what i was reading and trying to understand and learn ( the index too is of little help in this matter , being also quite sparse in citations in comparison with the extensive text )  . this important and pace - keeping text book comes to life under the wise editorial guidance of jeremic who ( apart from writing some chapters himself ) coordinates a large cohort of well - known international experts in the eld ; it is intended to offer the reader and most of all , those directly involved in ghting lung cancer with the above reported weapons , important theoretical , diagnostic , efcient discussion tools with the hope that it might set the stage for further improvements , and help consolidate researchers efforts . 
 che ( iper od ipofrazionamento ; frazionamento accelerato ; intensicazione di dose nella pianicazione dei trattamenti adattativi ) e nei nuovi agenti antitumorali chemioterapici che , malgrado tutto , hanno come conclusione degli scarsi risultati nali per il paziente . per coloro che non hanno familiarit o che non sono abituati a leggere i risultati di diverse sperimentazioni cliniche , non sar facile districarsi con i molteplici dati raccolti e presentati , anche quando queste sperimentazioni sono sponsorizzate e condotte sotto legida di assai serie societ scientiche internazionali . per risolvere questo difcile ostacolo vengono avanzati suggerimenti sul come sperimentazioni cliniche randomizzate , ben preparate e prospettiche nonch delle meta - analisi appropriate siano necessarie ed in corso di svolgimento per offrire a radioterapisti , clinici e chirurghi risultati certi da utilizzare in quello che la medicina translazionale chiama dal banco di laboratorio al letto del paziente per il benecio del malato . 
 ancora una volta , anche in questa recensione devo fare un appunto sulluso degli acronimi : in questo volume solo 6 dei 58 capitoli riportano un elenco degli acronimi utilizzati . 
per i rimanenti 52 capitoli , dal momento che non sono familiare con gli acronimi , ho dovuto riempire 6 pagine di abbreviazioni nel tentativo di restare edotto su quanto stavo leggendo e tentando di capire ed imparare ( da questo punto di vista anche lindice di poco aiuto , indice discretamente povero di citazioni rispetto alle dimensioni del testo )  . 
 questo volume , importante e aggiornato , stato redatto sotto la saggia guida editoriale del jeremic che ( oltre ad aver scritto alcuni dei capitoli ) coordina numerosi esperti internazionali ben riconosciuti nel campo . 
esso ha lo scopo di offrire al lettore ( ed in particolare a coloro quotidianamente impegnati nella lotta contro il cancro del polmone con tutte le armi sopra ricordate ) strumenti teorici e diagnostici importanti ed efcaci per la discussione , nella speranza che possa offrire il punto di partenza per ulteriori progressi , come aiuto anche nel consolidare gli sforzi dei ricercatori . 
 + 39 - 045 - 6013629 , e - mail : gfoti81@yahoo.it received : 12 january 2012 / accepted : 23 february 2012 / published online : 25 july 2013 springer - verlag 2013 abstract purpose . 
fifty - one patients ( 25 men , 26 women ; mean age , 52 years ) , preoperatively investigated by both mdct and mri and subsequently operated on with a histological diagnosis of nfpet , were included in this study . 
mdct and mri accuracy in evaluating location , size , margins , baseline density / signal intensity , structure , pattern of enhancement , peak enhancement phase , involvement of main pancreatic duct , involvement of adjacent organs , inltration of peritumoural vessels , involvement of locoregional lymph nodes , and liver metastases was compared using pearson correlation , mannwhitney and chi - square tests . 
scopo del presente lavoro stato confrontare laccuratezza diagnostica della tomograa computerizzata multidetettore ( tcmd ) e della risonanza magnetica ( rm ) nella valutazione preoperatoria dei tumori endocrini non funzionanti ( tenf ) del pancreas . 
sono stati inclusi nello studio 51 pazienti ( 25 uomini , 26 donne , et media 52 anni ) studiati nel preoperatorio mediante tcmd e rm e sottoposti a chirurgia con diagnosi istologica di tenf . 
 laccuratezza diagnostica di tcmd e rm nel valutare sede della lesione , dimensioni , margini , densit / intensit di segnale pre - contrastograca , struttura della lesione , pattern di enhancement , fase di massima impregnazione , coinvolgimento del dotto pancreatico principale , inltrazione di organi viciniori , inltrazione delle strutture vascolari peritumorali , coinvolgimento dei linfonodi locoregionali , metastasi epatiche , stata comparata mediante test di pearson , mann - whitney e chi - square test . 
tcmd e rm hanno mostrato simile accuratezza nel valutare dimensioni tumorali , margini lesionali , densit / intensit di segnale pre - contrastograca , struttura lesionale , pattern di impregnazione , coinvolgimento del dotto pancreatico principale , inltrazione degli organi contigui , linfonodi peripancreatici , metastasi epatiche ( p > 0 , 05 )  . 
la tcmd stata superiore alla rm nel valutare linltrazione vascolare ( p = 0 , 025 )  . radiol med ( 2013 ) 118 : 10821101 1083 the best imaging tool for preoperative evaluation of nfpet . keywords multidetector computed tomography ( mdct ) magnetic resonance imaging ( mri ) pancreas nonfunctioning pancreatic endocrine tumours ( nfpet ) conclusioni . 
la tcmd stata superiore alla rm nel valutare il coinvolgimento vascolare e dovrebbe essere considerata lindagine di prima scelta per la valutazione preoperatoria dei tenf pancreatici . parole chiave tomograa computerizzata ( tc ) risonanza magnetica ( rm ) pancreas tumori endocrini non funzionanti ( tenf ) introduction introduzione pancreatic endocrine tumours ( pet ) represent approximately 12% of all pancreatic tumours [ 1 , 2 ] and have an incidence of approximately one case per 100 , 000 population per year . 
as these tumours are not syndromic , they tend to be discovered either incidentally at an initial stage when they are still clinically silent or at a late stage due to the appearance of symptoms related to the mass effect [ 2 , 4 ]  . 
however , despite being frequently diagnosed at a late stage of disease , nfpet have a relatively good prognosis , with 5 - year survival rates up to 80% [ 2 , 3 ]  . surgical resection is the best therapeutic option : unlike other , more aggressive , pancreatic tumours such as adenocarcinoma , nfpet is eligible for either cytoreductive or merely palliative surgery , even in the presence of locally inltrating lesions with or without nodal or distant metastases [ 2 , 5 ]  . 
several diagnostic techniques have been used to evaluate nfpet , including computed tomography ( ct ) , magnetic resonance imaging ( mri ) , contrast - enhanced ultrasound ( ceus ) , octreoscan and positron emission tomography ( pet ) ct [ 923 ]  . 
only ct and mri , by virtue of their panoramic capabilities and high spatial resolution , can provide a precise assessment of disease extent through evaluation of the primary tumour , locoregional invasion and nodal and distant metastases , which predominantly involve the liver [ 2326 ]  . 
the literature , however , contains no recent studies evaluating the diagnostic accuracy of modern mdct and mri systems in the preoperative assessment of nfpet , particularly in comparing the results of the two modalities in the same case series . 
essendo non sindromiche , queste neoplasie vengono scoperte incidentalmente , quando ancora clinicamente silenti , o tardivamente per la comparsa di sintomi correlati alleffetto massa [ 2 , 4 ]  . 
sebbene frequentemente diagnosticati in uno stadio avanzato di malattia , i tenf risultano caratterizzati da una prognosi relativamente buona , con una sopravvivenza a 5 anni no all80% [ 2 , 3 ]  . la resezione chirurgica rappresenta la migliore opzione terapeutica : a differenza di tumori pancreatici pi aggressivi , come ladenocarcinoma , nel caso dei tenf lapproccio chirurgico pu essere preso in considerazione anche in caso di lesioni localmente inltranti , con o senza metastasi linfonodali o a distanza , con intento cito - riduttivo o meramente palliativo [ 2 , 5 ]  . 
esistono inoltre approcci terapeutici alternativi capaci di garantire un miglioramento della prognosi , fra i quali la terapia medica e quella medico - nucleare [ 6 , 7 ]  . 
stata pertanto recentemente proposta una stadiazione tnm allo scopo di promuovere ununiforme straticazione del rischio , aiutando nella scelta dellapproccio terapeutico di prima linea [ 8 ]  . la diagnostica per immagini svolge pertanto un ruolo cruciale nella pianicazione terapeutica . 
diverse tecniche diagnostiche sono state utilizzate per valutare i tenf , tra cui tomograa computerizzata ( tc ) , risonanza magnetica ( rm ) , ecograa con mezzo di contrasto ( ceus ) , octreoscan e pet - tc [ 923 ]  . 
tuttavia , solo tc e rm , in virt della loro panoramicit e dellelevata risoluzione spaziale , offrono la possibilit di effettuare un preciso bilancio di malattia , valutando il tumore primitivo , linltrazione locoregionale e le metastasi linfonodali e a distanza , localizzate prevalentemente in sede epatica [ 2326 ]  . 
in letteratura , tuttavia , non sono disponibili studi recenti che valutino laccuratezza diagnostica delle moderne apparecchiature di tomograa computerizzata multidetettore ( tcmd ) e di rm nella valutazione preoperatoria dei tenf , in particolare confrontando i risultati nella medesima casistica . 
lo scopo di questo studio pertanto quello di confrontare laccuratezza diagnostica della tcmd e della rm nella valutazione preoperatoria dei 1084 radiol med ( 2013 ) 118 : 10821101 tenf , utilizzando come standard di riferimento la chirurgia e i dati anatomopatologici . materiali e metodi popolazione dello studio nel periodo compreso fra gennaio 2005 e dicembre 2010 , lanalisi dei registri dellunit operativa di chirurgia b e di anatomia patologica del nostro ospedale ha individuato 187 pazienti consecutivi con diagnosi istologica di tenf considerabili per linclusione . 
sono stati inclusi nello studio tutti i pazienti con diagnosi istologica di tenf , studiati mediante tcmd e rm nellimmediato preoperatorio ( entro 14 giorni dalla chirurgia , range 114 giorni ) e , successivamente , sottoposti a intervento chirurgico . 
sono stati esclusi 89 pazienti per mancanza di indagini preoperatorie che rispondessero ai criteri di inclusione ( inclusi gli studi effettuati mediante protocolli diversi o con eccessivo gap temporale dallintervento ) , e 47 pazienti non sottoposti a intervento di resezione ( malattia avanzata documentata alle indagini preoperatorie , presenza di comorbidit gravi )  . 
la popolazione di studio era quindi composta da 51 pazienti ( 25 uomini , 26 donne , et media 52 anni , range da 26 a 78 anni )  . 
 durante lintervento sono stati valutati i seguenti rilievi in accordo ai criteri di stadiazione tnm [ 8 ] : dimensioni del tumore primitivo , inltrazione dei grossi vasi peripancreatici , del tessuto adiposo peripancreatico e di eventuali organi viciniori , coinvolgimento dei linfonodi locoregionali , presenza di metastasi a distanza localizzate in sede epatica . 
linltrazione delle strutture vascolari peritumorali ( tripode celiaco , vena porta , arteria e vena mesenterica superiore , arteria e vena splenica , in base alla sede della lesione primitiva ) stata valutata durante lintervento nei 51 pazienti arruolati , e per un sottogruppo addizionale di 10 pazienti sottoposti a intervento chirurgico senza resezione del tumore primitivo . 
1 criteri di inclusione ed esclusione applicati e relativa popolazione nale dello studio . chirurgia materials and methods study population an analysis of the records of the divisions of surgery ( surgery b ) and pathologic anatomy of our hospital identied 187 consecutive patients who received a histological diagnosis of nfpet between january 2005 and december 2010 and who were eligible for inclusion in the study . 
we included all patients with a histological diagnosis of nfpet who were studied by mdct and mri in the immediate preoperative period ( within 14 days before surgery ; range , 114 days ) and who subsequently underwent surgery . 
we excluded 89 patients due to lack of preoperative investigations fullling the inclusion criteria ( studies performed with different protocols or excessive time interval between imradiol med ( 2013 ) 118 : 10821101 1085 aging and surgery ) , and 47 patients who did not undergo surgical resection ( demonstration of advanced - stage disease on preoperative imaging , presence of severe comorbidities )  . 
the following surgical ndings were assessed in accordance with the tnm staging criteria [ 8 ] : size of the primary tumour ; invasion of large peripancreatic vessels , peripancreatic fat and adjacent organs ; involvement of locoregional lymph nodes ; presence of distant metastases involving the liver . 
invasion of the peritumoural vessels ( coeliac trunk , portal vein , superior mesenteric artery and vein , splenic artery and vein , depending on the site of the primary tumour ) was evaluated at surgery in all 51 patients , as well as in a subgroup of ten patients who underwent surgery without primary tumour resection . 
the extent of vascular involvement was classied according to a similar scale to that employed for pancreatic adenocarcinomas [ 27 ] : grade 1 = no signs of invasion ( no contact between vessel and primary tumour ) ; grade 2 = partial invasion ( contact between vessel and primary tumour for a length > 1 mm and < 2 cm in the longitudinal axis and / or > 10 and < 180 in the transverse axis ) ; grade = diffuse invasion ( contact between vessel and tumour for a length > 2 cm in the longitudinal axis and / or > 180 in the transverse axis of the vessel )  . 
all tumours were assessed for the following parameters : size of the primary tumour ( in millimetres ) ; involvement of the main pancreatic duct ( positive if diameter > 3mm ) ; invasion of adjacent vessels and / or organs ; involvement of locoregional lymph nodes . 
 per tutti i tumori sono stati valutati i seguenti rilievi : dimensioni del tumore primitivo ( in mm ) ; coinvolgimento del dotto pancreatico principale ( presente in caso di calibro > 3mm ) ; inltrazione delle strutture vascolari e / o degli organi viciniori ; coinvolgimento dei linfonodi locoregionali . 
dei tumori inclusi nello studio stato inoltre determinato il grading secondo la classicazione clinico - patologica who ( world health organization ) [ 28 ] , e il valore del ki - 67 [ 29 ]  . 
 tecniche di studio protocollo tcmd tutte le indagini tc sono state effettuate con uno scanner multi - detettore ( brilliant 64 , philips , olanda ) , utilizzando i seguenti parametri di scansione : spessore fetta dello strato 1 mm , 120 kv , mas variabili in base alla massa del paziente ( normalmente compresi fra 200 e 300 ) , pitch = 1 . 
in seguito a una scansione pre - contrastograca , sono state ottenute tre scansioni contrastograche dopo infusione endovenosa di mezzo di contrasto , utilizzando la tecnica del bolus tracking : fase arteriosa pancreatica ( in media 35 secondi di ritardo ) , fase venosa portale ( in media 70 secondi di ritardo ) e fase venosa tardiva ( in media 120 secondi di ritardo )  . 
liniezione del mezzo di contrasto organo iodato ( ultravist 370 , bayerschering , germania , 370 mg di iodio / ml ) , stata effettuata tramite unagocannula posizionata in una vena antecubitale del braccio , mediante iniettore automatico con usso di 3 ml / secondo , seguita da un bolo di 40 ml di soluzione siologica . 
 protocollo rm tutte le indagini rm sono state eseguite con uno scanner da 1 , 5 tesla ( magnetom symphony , siemens , enlargen , germania ) , utilizzando bobine phased - array per ottenere il miglior rapporto segnale rumore . 
stato somministrato a tutti i pazienti un mezzo di contrasto orale negativo ( lumirem , guerbet , roissy , francia ) per ridurre lintensit di segnale del tratto gastroenterico , riducendone gli artefatti . 
in fase pre - contrastograca sono state utilizzate sequenze gradient echo ( gre ) t1 - dipendenti in apnea respiratoria [ tempo di ripetizione ( tr ) / tempo di eco ( te ) , 107 / 4 , 8 ms ] , con e senza soppressione selettiva del segnale del grasso ; sequenze fast spin echo ( fse ) t2 sincronizzate con il respiro ( tr / te , 4950 / 102 ms ) , senza e con saturazione del grasso ; se1086 radiol med ( 2013 ) 118 : 10821101 scanner ( brilliance 64 , philips medical system , best , the netherlands ) using the following scan parameters : slice thickness 1 mm , 120 kv , varying milliampere depending on patient size ( normally 200300 ) and pitch 1 . 
infusion of contrast material using the bolus - tracking technique : an arterial pancreatic phase ( mean delay , 35 s ) , a portal venous phase ( mean delay , 70 s ) and a late venous phase ( mean delay , 120 s )  . 
iodinated contrast material ( ultravist 370 , bayer - schering , germany , 370 mg iodine / ml ) was administered at a ow rate of 3 ml / s via a needle cannula placed in an antecubital vein with an automatic injector , followed by a 40 - ml bolus of saline solution . 
 quenze t2 - dipendenti haste multiplanari ( tr / te , 1900 / 76 ms ) ; sequenze colangio - pancreatograche rare ( tr / te , 1900 / 984 ms )  . 
successivamente alliniezione endovenosa di mezzo di contrasto paramagnetico ( gadobenato dimeglumina , multihance , bracco , milano , italia ) con usso di 2 ml / s sono state acquisite in fase dinamica sequenze gre t1 con soppressione del grasso ( tr / te , 3 / 2 ms ; ip angle 10 ) nelle fasi arteriosa pancreatica ( 35 secondi ) , venosa portale ( 70 secondi ) e venosa tardiva ( 120 secondi ) , calcolate mediante la tecnica del bolus test . 
una fase tardiva di escrezione epato - biliare ( circa 1 ora di ritardo dalla somministrazione del mezzo di contrasto ) stata ottenuta in tutti i pazienti per migliorare le possibilit di identicazione e caratterizzazione delle lesioni focali epatiche . mri protocol analisi delle immagini all mri studies were obtained with a 1.5 - tesla scanner ( magnetom symphony , siemens , erlangen , germany ) , using phased - array coils to achieve the best signal - to - noise ratio ( snr )  . 
the precontrast study consisted of the following sequences : t1 - weighted breath - hold gradient echo ( gre ) [ time to repetition ( tr ) / time to echo ( te ) , 107 / 4.8 ms ] with and without fat suppression ; respiratory - gated t2 - weighted fast spin echo ( fse ) ( tr / te , 4 , 950 / 102 ms ) without and with fat saturation ; t2 - weighted multiplanar half - fourier acquisition with single - shot turbo spin echo ( haste ) ( tr / te , 1 , 900 / 76 ms ) ; cholangiopancreatographic rapid acquisition with relaxation ( rare ) ( tr / te , 1 , 900 / 984 ms )  . 
administration of paramagnetic contrast material ( gadobenate dimeglumine , multihance , bracco , milan , italy ) at a rate of 2 ml / s , the following dynamic sequences were acquired : t1 - weighted gre with fat suppression ( tr / te , 3 / 2 ms ; ip angle 10 ) in the arterial pancreatic ( 35 s ) , portal venous ( 70 s ) and late venous phase ( 120 s ) determined with the bolus test technique . 
a late excretory hepatobiliary phase ( ~1 h after contrast administration ) was obtained in all patients to increase the chance of identifying and characterising any focal hepatic lesions . image analysis mdct and mr images were retrospectively and independently assessed by two radiologists experienced in pancreatic diseases . 
the examinations were reviewed in random order , with a time interval of at least 2 months between reviews so as to reduce the risk of bias due to latent memory . 
i radiologi coinvolti nel processo di lettura non erano a conoscenza dei dati clinici , chirurgici e anatomo - patologici , ma erano consapevoli che le indagini preoperatorie fossero state effettuate per la valutazione preoperatoria di pazienti affetti da tenf pancreatico . 
gli studi sono stati valutati in ordine randomizzato , con un gap temporale di almeno 2 mesi fra la lettura delle due indagini , allo scopo di ridurre il rischio di bias da memoria latente . 
 nel sottogruppo di lesioni ipervascolarizzate , stata inoltre determinata la fase di massima impregnazione , separando le lesioni con picco in fase arteriosa pancreatica ( pattern tipico ) , da quelle con picco in fase venosa portale o tardiva ( pattern atipico )  . analisi statistica lanalisi statistica stata effettuata mediante software spss ( versione 19.0 ; spss , an ibm company , chicago , il )  . 
 sensibilit ( se ) , specicit ( sp ) , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) e accuratezza ( acc ) di tcmd e rm sono stati calcolati per i parametri relativi alla classicazione tnm , utilizzando come standard di riferimento la diagnosi anatomo - patologica su pezzo operatorio ; allo scopo di rendere la valutazione del coinvolgimento vascolare pi aderente alla pratica clinica , lanalisi di questo parametro stata effettuata su una coorte allargata di pazienti ( n = 61 ) , includendo anche quelli sottoposti a intervento chirurgico senza resezione e utilizzando , pertanto , i rilievi chirurgici come standard di riferimento . lindice di correlazione di pearson stato utilizzato per correlare il diametro delle lesioni misurato allimaging e quello rilevato allindagine patologica . 
sensitivity , specicity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy of mdct and mri were calculated for each tnm parameter using the histopathological diagnosis on the surgical specimen as the reference standard . 
in order to make assess vascular involvement more closely reective of clinical practice , this parameter was analysed on an extended cohort of patients ( n = 61 ) , which included patients who underwent surgery without resection , with the surgical ndings used as the reference standard . pearsons correlation coefcient was used to correlate lesion diameter as measured at imaging with that measured at pathology . 
 results surgery and histopathology seventeen tumours were located in the pancreatic head and / or uncinate process , 32 in the body - tail region and two showed diffuse involvement of the entire gland ( both in patients affected by von hippel lindau syndrome )  . 
 these include pancreaticoduodenectomy in 15 cases ( two with classic technique , 13 with pylorus - preserving technique ) ; splenopancreatectomy in 24 cases ; total pancreatectomy in three cases ; atypical resection in nine cases ( six enucleations , three intermediate resections )  . 
resection of adjacent organs and / or vessels was carried out in six patients : two underwent gastric resection ( one associated with partial resection and reconstruction of the common trunk of the portal vein ) ; in two patients , the left adrenal gland in one the right adrenal gland was removed ; one patient underwent resection of the stomach , left kidney and adrenal gland , part of the transverse colon , left colic exure and mesocolon ; four patients underwent hepatic metastases resection . at pathology , mean lesion diameter was 4.2 ( range , 0.8 12 ) cm ; the pancreatic duct was normal in 42 / 51 ( 82.3% ) cases and involved ( calibre > 3 mm ) in 9 / 51 cases ( 17.7% ) ; radiol med ( 2013 ) 118 : 10821101 utilizzando il chi - square test . 
 risultati chirurgia e anatomia patologica diciassette tumori erano localizzati in corrispondenza della testa e / o del processo uncinato del pancreas , 32 nella regione del corpo - coda pancreatici , 2 inne presentavano una localizzazione diffusa , coinvolgendo lintera ghiandola ( entrambi in pazienti affetti da sindrome di von hippel - lindau )  . 
 i tipi di interventi chirurgici effettuati sono schematizzati nella tabella 1 : lintervento stato di duoedeno - cefalopancreasectomia in 15 casi ( 2 con tecnica classica , 13 con tecnica piloro - preserving ) , di splenopancreasectomia in 24 casi , di pancreasectomia totale in 3 casi , di resezione atipica in 9 casi ( 6 enucleazioni , 3 resezioni intermedie )  . 
la resezione di organi viciniori e / o strutture vascolari stata effettuata in 6 pazienti : in 2 pazienti stata effettuata una resezione dello stomaco ( in un caso in associazione a resezione parziale e ricostruzione del tronco comune della vena porta ) ; in 2 pazienti stato asportato il surrene sinistro e in 1 paziente quello destro ; in 1 paziente , inne , sono stati resecati stomaco , surrene e rene sinistro , parte del colon trasverso e della essura colica sinistra e del mesocolon ; in 4 pazienti stata effettuata una metastasectomia epatica . allesame anatomo - patologico , il diametro medio dei tumori era di 4 , 2 cm ( range 0 , 812 cm ) ; il dotto pancreatico era normale in 42 / 51 ( 82 , 3% ) casi , mentre risultava coinvolto ( calibro > 3 mm ) in 9 / 51 casi ( 17 , 7% ) ; linltrazione di uno o pi organi viciniori stata confermata in 6 / 51 ( 11 , 7% ) pazienti . 
lanalisi del coinvolgimento delle strutture vascolari peritumorali , eseguita in corso di intervento su di un totale di 61 pazienti ( incluso un sottogruppo di 10 pazienti sottoposti a intervento chirurgico senza resezione del tumore primitivo ) , ha rilevato la presenza di inltrazione vascolare diffusa in 11 / 61 casi ( 18% ) , parziale in 12 / 61 casi ( 19 , 7% ) , mentre il coinvolgimento vascolare stato escluso in 38 / 61 casi ( 62 , 3% )  . 
 la presenza di metastasi ai linfonodi loco - regionali stata documentata in 18 / 51 ( 35 , 3% ) casi ; la presenza di metastasi epatiche inne stata confermata ( mediante octreoscan , pet - ct , biopsia o intra - operatoriamente ) in 11 / 51 pazienti ( 21 , 5% )  . 
alla tcmd il diametro medio delle lesioni stato di 4 , 4 cm ( range 112 cm ) , con ottima correlazione con i dati anatomo - patologici ( r = 0 , 94 )  . 
nella scansione basale 45 / 51 ( 88 , 3% ) lesioni erano prevalentemente isodense rispetto al pancreas , 4 / 51 ( 7 , 8% ) apparivano prevalentemente iperdense ( presenza di calcicazioni intralesionali ) , mentre 2 / 51 ( 3 , 9% ) erano prevalentemente ipodense ( per aspetto cistico o necrosi estesa )  . 
la struttura tumorale risultata omogenea in 22 / 51 ( 43 , 1% ) lesioni , disomogenea nelle rimanenti 29 / 51 ( 56 , 9% ) lesioni ( calcicazioni intralesionali n = 4 ; aspetto cistico n = 2 ; necrosi intralesionale evidente solo dopo contrasto n = 23 )  . 
in fase contrastograca , 39 / 51 ( 76 , 4% ) lesioni sono risultate ipervascolarizzate rispetto al pancreas sano , 10 / 51 ( 19 , 7% ) ipovascolarizzate , 2 / 51 ( 3 , 9% ) isovascolarizzate in tutte le fasi contrastograche ( identicate in base alleffetto massa o alla disomogeneit in fase pre - contrastograca )  . 
nel sottogruppo di 39 lesioni ipervascolarizzate , la fase di massima impregnazione rispetto al parenchima ghiandolare stata raggiunta nella fase arteriosa pancreatica per 29 / 39 ( 74 , 3% ) lesioni , in fase venosa portale per 8 / 39 ( 20 , 5% ) lesioni e in fase venosa tardiva per 2 / 39 ( 5 , 2% ) lesioni . 
tumour structure was homogeneous in 22 / 51 ( 43.1% ) lesions and inhomogeneous in the remaining 29 / 51 ( 56.9% ) ( intralesional calcications , n = 4 ; cystic appearance , n = 2 ; intralesional necrosis visible only after contrast administration , n = 23 )  . 
 on contrast - enhanced scans , 39 / 51 ( 76.4% ) lesions were hypervascular compared with the healthy pancreas , 10 / 51 ( 19.7% ) were hypovascular and 2 / 51 ( 3.9% ) were isovascular in all contrast phases ( identied based on mass effect or heterogeneity on unenhanced scans )  . 
involvement of the peritumoural nodes was excluded in 37 / 51 cases ( 72.5% ) and suggested in the remaining 14 / 51 ( 27.5% ) , riferica della lesione , in relazione alla sua natura cistica o allabbondante necrosi . la tcmd si rivelata unindagine accurata nella valutazione del coinvolgimento del dotto pancreatico principale con valori di se , sp , vpp , vpn e acc rispettivamente di 88 , 8% , 92 , 8% , 72 , 7% , 97 , 5% e 92 , 1% . 
linltrazione di organi viciniori stata giudicata assente mediante tcmd in 44 / 51 casi ( 86 , 2% ) , mentre stata suggerita dai rilievi radiologici in 7 / 51 casi ( 13 , 8% ) , con valori di se , sp , vpp , vpn e acc rispettivamente di 83 , 3% , 95 , 5% , 71 , 4% , 97 , 7% e 94 , 1% . 
il coinvolgimento dei linfonodi peritumorali non era apprezzabile in 37 / 51 casi ( 72 , 5% ) , mentre era suggerito allimaging nei rimanenti 14 / 51 casi ( 27 , 5% ) , con valori di se , sp , vpp , vpn e acc rispettivamente di 61 , 1% , 87 , 8% , 73 , 3% , 80 , 5% e 78 , 4% . 
il coinvolgimento delle strutture vascolari , valutato su un totale di 61 pazienti ( incluso un sottogruppo di 10 pazienti sottoposti a intervento chirurgico senza resezione del tumore primitivo ) stato valutato come assente in 34 / 61 casi ( 55 , 7% ) , come parziale in 14 / 61 casi ( 22 , 9% ) e come diffuso in 13 / 61 casi ( 21 , 4% ) , con valori di se , sp , vpp , vpn e acc rispettivamente di 86 , 9% , 86 , 8% , 80 , 0% , 91 , 6% e 86 , 9% . 
 in accordance with tnm classication [ 8 ] , mdct allowed correct staging of 40 / 51 ( 78.4% ) patients , with six cases of overstaging ( two from stage i to ii ; two from stage ii to iii ; two from stage iii to iv ) and ve of understaging ( two from stage iv to iii ; two from stage iii to ii ; one from stage ii to stage i )  . 
tumour structure was homogeneous in 20 / 51 ( 39.2% ) lesions and inhomogeneous in the remaining 31 / 51 ( 60.8% ) ( frankly cystic appearance , n = 3 ; evident intralesional necrosis on postcontrast scans , n = 28 )  . 
 in the contrast - enhanced phase , 41 / 51 ( 80.4% ) were hypervascular relative to the healthy pancreas , 8 / 51 ( 15.7% ) were hypovascular and 2 / 51 ( 3.9% ) were isovascular in all phases and identied due to mass effect , t2 hyperintensity or t1 hypointensity . 
in fase pre - contrastograca , nelle sequenze t1 - dipendenti , 15 / 51 ( 29 , 4% ) lesioni erano prevalentemente isointense rispetto al pancreas sano , mentre 36 / 51 ( 70 , 6% ) risultavano prevalentemente ipointense ; nelle sequenze t2dipendenti , 10 / 51 ( 19 , 6% ) lesioni erano prevalentemente isointense , 40 / 51 ( 78 , 4% ) lesioni erano prevalentemente iperintense ( delle quali 4 a contenuto uido ) , con 1 / 51 ( 2 , 0% ) lesioni ipointensa . 
la struttura tumorale risultata omogenea in 20 / 51 ( 39 , 2% ) lesioni , disomogenea nelle rimanenti 31 / 51 ( 60 , 8% ) lesioni ( aspetto francamente cistico n = 3 ; necrosi intralesionale evidente dopo contrasto n = 28 )  . 
 in fase contrastograca 41 / 51 ( 80 , 4% ) lesioni sono risultate ipervascolarizzate rispetto al pancreas sano , 8 / 51 ( 15 , 7% ) ipovascolarizzate , 2 / 51 ( 3 , 9% ) isovascolarizzate in tutte le fasi contrastograche e identicate in base alleffetto massa , alliperintensit nelle sequenze t2 - dipendenti o alliponitensit in quelle t1 - dipendenti . 
nel sottogruppo di 41 lesioni ipervascolarizzate , la massima impregnazione rispetto al parenchima ghiandolare stata raggiunta nella fase arteriosa pancreatica per 25 / 41 ( 60 , 9% ) lesioni , in fase venosa portale per 12 / 41 ( 29 , 2% ) lesioni e in fase venosa tardiva per 4 / 41 ( 9 , 7% ) lesioni . 
in 5 casi , limpregnazione tumorale era apprezzabile solo nella porzione periferica della lesione , in relazione alla sua natura cistica o allabbondante necrosi . nella valutazione del coinvolgimento del dotto pancreatico principale la rm ha presentato valori di se , sp , vpp , vpn e acc rispettivamente di 100% , 95 , 2% , 81 , 8% , 100% e 96 , 0% . 
linltrazione delle strutture vascolari , valutata su un totale di 61 pazienti ( incluso un sottogruppo di 10 pazienti sottoposti a intervento senza resezione del tumore primitivo ) , stata considerata assente in 36 / 61 casi ( 59 , 0% ) , parziale in 13 / 61 casi ( 21 , 3% ) e diffusa in 12 / 61 casi ( 19 , 7% ) , con valori di se , sp , vpp , vpn e acc rispettivamente di 78 , 2% , 81 , 5% , 72 , 0% , 86 , 1% e 80 , 3% . 
 in accordance with the tnm classication [ 8 ] , mri allowed correct staging of 39 / 51 ( 76.4% ) patients , with six cases of overstaging ( two from stage i to stage ii ; one from stage ii to iii ; three from stage iii to stage iv ) and six cases of understaging ( one from stage iv to iii ; three from stage iii to ii ; two from stage ii to stage i )  . 
lanalisi comparativa ha messo in evidenza unottima concordanza fra tcmd e rm per quanto riguarda le dimensioni tumorali stimate allimaging , i margini lesionali , la densit / intensit di segnale in fase pre - contrastograca , la struttura della lesione , il pattern di impregnazione lesionale in fase post - contrastograca ( p > 0 , 05 )  . 
a large cystic nfpet of the pancreatic tail can be recognised in axial images acquired during the portal venous phase both at mdct ( a , b ) and mri ( c , d )  . 
un grosso tenf di natura cistica , localizzato in corrispondenza della coda pancreatica , apprezzabile nelle immagini assiali ottenute durante la fase venosa portale sia alla tcmd ( a , b ) che alla rm ( c , d )  . 
nel complesso , la tcmd si dimostrata solo lievemente superiore alla rm nel determinare lo stadio tnm , senza differenze statisticamente signicative ( 40 versus 39 lesioni correttamente stadiate , p > 0 , 05 )  . 
nessuno dei parametri intrinseci del tumore primitivo ( pattern di impregnazione , struttura tumorale , margini della lesione , dilatazione del dotto pancreatico principale ) valutati mediante tcmd e rm , ha mostrato una correlazione signicativa con il grading who n con i valori del ki - 67 . discussione sebbene rappresentino unentit rara , i tenf pancreatici 1094 radiol med ( 2013 ) 118 : 10821101 fig . 
these ndings are well depicted on contrast - enhanced mdct axial images ( a ) and paracoronal maximum intensity projection ( mip ) reconstructed images ( b ) and on contrast - enhanced axial mri ( c ) and heavily t2 - weighted thick - slab mr cholangiopancreatographic images in the coronal plane ( d )  . 
i rilievi sono ben dimostrati alla tcmd mediante scansioni post - contrastograche sul piano assiale ( a ) e ricostruzioni mip paracoronali ( b ) , e alla rm mediante scansioni assiali post - contrastograche ( c ) o nelle immagini colangio - wirsung - rm fortemente t2 - dipendenti a grande spessore di fetta acquisite sul piano coronale ( d )  . 
none of the intrinsic parameters of the primary tumour ( enhancement pattern , tumour structure , lesion margins , dilatation of the main pancreatic duct ) evaluated with mdct and mri showed a signicant correlation with the who grades or the ki - 67 values . discussion although rare , nfpet appear to be rising in incidence , in part as a result of the increased rate of incidental diagnoses in asymptomatic patients [ 26 ]  . 
lo sviluppo di nuove e pi aggressive tecniche chirurgiche , unitamente alla possibilit di effettuare valide terapie alternative , ha reso sempre pi frequenti gli interventi di tipo palliativo [ 24 , 30 , 31 ]  . 
lapproccio terapeutico e la prognosi di questi tumori dipendono , infatti , non solo dalla possibilit di ottenere una diagnosi precoce , ma anche dai risultati di uneventuale resezione chirurgica [ 30 , 3134 ]  . 
a tumour of the pancreatic tail is well depicted on axial contrast - enhanced mdct ( a , b ) and contrast - enhanced mri ( c , d )  . 
alcune aree di ispessimento nodulare sono apprezzabili in prossimit dellilo splenico , espressione di sconnamento del tumore nel tessuto adiposo peri - pancreatico ( freccia in a e in c )  . 
sia alla tcmd che alla rm possibile dimostrare laspetto normale della ghiandola surrenalica sinistra . more aggressive surgical techniques , combined with the possibility of undertaking effective alternative treatments , has increased the frequency of palliative interventions [ 24 , 30 , 31 ]  . 
treatment and prognosis of these tumours depend not only on the possibility of establishing an early diagnosis but also on the outcomes of possible surgical resection [ 30 , 3134 ]  . 
 among imaging modalities , mdct and mri have the highest diagnostic potential for evaluating pancreatic tumours on account of their spatial and contrast resolution and their panoramic capabilities : in our study , we therefore valutazione dei tumori pancreatici , in virt della loro elevata risoluzione spaziale e di contrasto e della loro grande panoramicit : nel nostro studio abbiamo confrontato pertanto laccuratezza di queste due tecniche dimmagine nella valutazione preoperatoria dei tenf , utilizzando come standard di riferimento i rilievi chirurgici e anatomo - patologici . 
sebbene la tcmd sia stata lievemente pi precisa della rm grazie alla possibilit di ottenere immagini di alta qualit in tutti i piani dello spazio , stata registrata una differenza non signicativa ( p > 0 , 05 )  . 
anche le caratteristiche intrinseche dei tumori , valutate mediante tcmd e rm , sono risultate molto simili : non vi stata infat1096 radiol med ( 2013 ) 118 : 10821101 fig . 
a large inhomogeneous hypervascular tumour of the pancreatic head ( star ) is clearly depicted on mdct ( a , b ) and mri ( c , d )  . 
sia alla tcmd ( a , b ) che alla rm ( c , d ) si apprezza un grosso tumore discretamente vascolarizzato in sede cefalo - pancreatica ( asterisco )  . 
as expected , mdct and mri had very similar results in identifying and assessing the size of the primary tumour , with a good correlation with the diameter measured on the surgical specimen . 
in some cases , mdct revealed intralesional calcications undetected by mri , ti alcuna differenza sostanziale per quanto concerne i margini lesionali , la struttura tumorale e la densit / intensit di segnale in fase pre - contrastograca ( p > 0 , 05 )  . 
in alcuni casi , la tcmd ha messo in evidenza calcicazioni intralesionali non evidenziabili alla rm , mentre la rm ha identicato focolai di necrosi intratumorali non evidenti alla tcmd . 
 come attendibile in relazione alla simile farmacocinetica dei mezzi di contrasto utilizzati , tcmd e rm non hanno presentato alcuna differenza signicativa concernente i pattern di impregnazione dei tenf ( p > 0 , 05 )  . 
bisogna tuttavia sottolineare che piccole differenze esistono , potendo in parte essere giusticate dalla migliore risoluzione temporale della tcmd , ma anche dalla maggiore risoluzione di contrasto e cospicuit del potenziamento contrastograco della rm : nella nostra esperienza , sebbene la rm abbia messo in evidenza lipervascolarizzazione tumorale in un numero radiol med ( 2013 ) 118 : 10821101 1097 fig . 
at mdct , primary tumour of the pancreatic head and the liver metastasis of the right hepatic lobe appear inhomogeneously hypervascular during the arterial pancreatic phase ( a ) , showing washout during the late venous phase ( b )  . 
alla tcmd , sia il tumore primitivo localizzato in sede cefalo - pancreatica che la metastasi epatica del lobo destro appaiono disomogeneamente ipervascolarizzati in fase arteriosa pancreatica ( a ) , mostrando un discreto wash - out in fase venosa tardiva ( b ) ; tali rilievi vengono dimostrati anche alla rm con mezzo di contrasto , che conferma il pattern di ipervascolarizzazione nella immagine assiale acquisita in fase arteriosa pancreatica ( c ) e il wash - out nellimmagine coronale acquisita in fase venosa tardiva ( d ) , sia per il tumore primitivo che per la lesione ripetitiva localizzata nel lobo destro del fegato . 
however , it should be noted that small differences do exist , in part accounted for by the better temporal resolution of mdct but also by the greater contrast resolution and conspicuity of mri enhancement . 
the scan phase most frequently revealing maximum tumour enhancement was the arterial pancreatic maggiore di casi rispetto alla tcmd ( 41 versus 39 ) , la differenza stata troppo esigua per incidere sulla valutazione dei rimanenti parametri . 
la fase di maggior potenziamento tumorale stata rappresentata pi frequentemente dalla fase arteriosa pancreatica ; tuttavia , sia alla tcmd che alla rm , buona parte delle lesioni analizzate ha raggiunto il picco di enhancement in fase venosa portale ( 20 , 5 e 29 , 2% , rispettivamente ) o tardiva ( 5 , 2 e 9 , 7% , rispettivamente ) : ne deriva la necessit di ottenere uno studio contrastograco multifasico allo scopo di aumentare le possibilit di meglio delimitare il tumore rispetto al parenchima risparmiato . 
 sia la tcmd che la rm hanno dimostrato elevati valori di accuratezza nel valutare il coinvolgimento del dotto pancreatico principale ( p > 0 , 05 ) ; questo parametro stato 1098 radiol med ( 2013 ) 118 : 10821101 fig . 
both at mdct ( a ) and mri ( b ) , the axial contrast - enhanced scan obtained during the portal venous phase shows a nfpet of the pancreatic head located close to superior mesenteric vein ( arrow in a and b )  . 
le immagini assiali acquisite in fase venosa portale sia alla rm ( a ) che alla tc ( b ) , mostrano un tenf della testa pancreatica localizzato in adiacenza alla vena mesenterica superiore ( freccia in a e b )  . 
le immagini rm ottenute sul piano coronale ( c ) non permettono di escludere linltrazione della struttura vascolare ( frecce in c ) ; la ricostruzione coronale ottenuta mediante tcmd ( d ) dimostra che esiste un piano di clivaggio adiposo fra il tumore e il vaso ( frecce in d )  . 
 both mdct and mri demonstrated high levels of accuracy in evaluating involvement of the main pancreatic duct ( p > 0.05 ) ; this parameter was inuenced by tumour size and site , being more frequent in the case of large lesions located in the pancreatic head . 
a differenza , tuttavia , del diametro tumorale , per il quale stata recentemente dimostrata una relazione con la malignit lesionale [ 35 ] , il coinvolgimento duttale considerato singolarmente non correla con il grading tumorale . 
these results might , however , depend on the relatively low incidence of these ndings ( identied at pathology in six and 18 patients , respectively ) and on their uneven distribution within the study population . 
the problem is further compounded by the fact that these ndings are relatively less common in patients undergoing surgical resection ( with available pathological tnm results ) compared with those with advanced disease at diagnosis , often excluded from such study . 
a possible explanation lies in the tendency these tumour types have to present with large hepatic metastases , with similar imaging features to the primary tumour ( hypervascular in the arterial phase , washout in venous and late phases ) that can be well identied with both imaging techniques thanks to dynamic postcontrast imaging . 
the reason lies in the tnm staging system itself [ 8 ] , as tumours are upstaged from stage ii to iii not only in the case of large - vessel involvement but also if adjacent organs are invaded ( expression of the passage of the t parameter from t3 to t4 ) and in the case of nodal metastases ( expression of the passage of the n parameter from n0 to n1 )  . 
it should also be noted that vascular invasion , considered alone , is a relatively minor parameter in nfpet preoperative evaluation compared with nodal or distant metastases , and one that does not constitute an absolute contraindication to surgery [ 30 , 31 ]  . 
our data demonstrate that no radiological parameter assessed on mdct and mri ( tumour margins , tumour structure , enhancement pattern , dilatation of the main pancreatic duct ) has a signicant correlation with loro non uniforme distribuzione allinterno della popolazione di studio . 
il problema ulteriormente amplicato dal fatto che tali rilievi sono relativamente pi rari nei pazienti sottoposti a intervento di resezione ( con disponibilit di un tnm patologico ) rispetto a quelli con malattia avanzata alla diagnosi , spesso scartati dallo studio ; tali fattori potrebbero quindi aver generato un bias da selezione , con conseguente sottostima della reale incidenza dei rilievi stessi . 
 anche se stato dimostrato che la rm superiore alla tcmd nellidenticazione di lesioni ripetitive epatiche , soprattutto anche grazie al valore aggiunto della fase di escrezione epatobiliare [ 36 ] , i nostri dati hanno evidenziato simili valori di accuratezza per le due metodiche ( 92 , 1 versus 94 , 1% , p > 0 , 05 ) : la possibile spiegazione risiede nella tendenza di questi tumori a presentare metastasi epatiche di grosse dimensioni , con caratteristiche imaging simili al tumore primitivo ( ipervascolarizzazione in fase arteriosa , wash - out in fase venosa e tardiva ) ben identicabili grazie a entrambe le metodiche mediante uno studio contrastograco dinamico . 
 la tcmd ha presentano maggiore accuratezza rispetto alla rm nella valutazione del coinvolgimento vascolare ( 86 , 9% versus 80 , 3% ) , con una differenza statisticamente signicativa fra le due metodiche ( p = 0 , 025 )  . 
inoltre , grazie ai moderni software di ricostruzione delle immagini possibile ottenere dalle immagini tcmd ricostruzioni multiplanari in qualsiasi piano dello spazio , di qualit solitamente superiore rispetto a quelle ottenibili mediante imaging rm . 
le migliori prestazioni della tcmd nel valutare il coinvolgimento vascolare non si sono per tradotte in un vantaggio concreto nel processo di stadiazione preoperatoria dei tenf : il motivo da ricercare nella stadiazione tnm stessa [ 8 ] , che prevede un passaggio dallo stadio ii al iii non solo in caso di coinvolgimento dei grossi vasi , ma anche in caso di inltrazione di organi viciniori ( espressione del passaggio del parametro t da t3 a t4 ) e in caso di presenza di metastasi linfonodali ( espressione del passaggio del parametro n da n0 a n1 )  . 
bisogna inoltre sottolineare che linltrazione vascolare , considerata singolarmente , rappresenta un parametro relativamente poco importante nella valutazione preoperatoria dei tenf rispetto alla presenza di metastasi linfonodali e a distanza , non rappresentando una controindicazione assoluta allintervento [ 30 , 31 ]  . 
 nel complesso , la tcmd si dimostrata solo lievemente superiore alla rm nel determinare lo stadio tnm , anche se la differenza non statisticamente signicativa ( 40 versus 39 lesioni correttamente valutate , p > 0 , 05 )  . 
i nostri dati dimostrano che nessun parametro radiologico valutato alla tcmd e alla rm ( margini tumorali , struttura tumorale , pattern di impregnazione , dilatazione del dotto pancreatico principale ) presenta una correlazione signicativa con la 1100 radiol med ( 2013 ) 118 : 10821101 who classication and ki - 67 values . 
we did not investigate the possible correlation between these parameters and the presence of nodal and hepatic metastases because of the relatively small size of the subgroup of patients exhibiting these ndings . 
finally , we performed no detailed analysis of the relationship between tnm stage and who classication and ki - 67 values , despite the fact that this correlation has already been reported by other studies [ 32 , 33 ]  . our study has some limitations : ( 1 ) we performed a retrospective review of only one histological type of tumour with a known diagnosis , even though this condition is fairly typical of routine practice where we often need to stage a lesion that has already been characterised ; ( 2 ) we enrolled a relatively small number of patients , but this was to be expected given the stringent inclusion criteria and the relative rarity of the disease ; ( 3 ) the majority of imaging ndings were evaluated on the basis of quantitative or semiquantitative analysis , which is , however , probably the approach that can best be reproduced in clinical practice . classicazione who e con i valori del ki - 67 . 
however , results suggest that in view of the slightly better accuracy and greater availability and accessibility of mdct , this should be considered the examination of choice for preoperative evaluation of nfpet . 
mri represents an alternative technique to be taken into consideration when mdct is contraindicated . tcmd e rm hanno presentato simili valori di accuratezza diagnostica per quanto concerne la valutazione di pressoch tutti i parametri esaminati . 
i risultati ottenuti suggeriscono tuttavia che , in virt dellaccuratezza lievemente superiore e della maggiore diffusione e accessibilit , la tcmd debba essere considerata come lindagine di prima scelta per la valutazione preoperatoria dei tenf pancreatici . 
la rm rappresenta tuttavia una tecnica di studio alternativa , da considerare quando la tcmd sia controindicata . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
gallini 2 , 33081 aviano ( pn ) , italy 2department of epidemiology and biostatistics , centro di riferimento oncologico , cro , aviano ( pn ) , italy 3department of medical physics , centro di riferimento oncologico , cro , aviano ( pn ) , italy correspondence to : m . 
daily orthogonal anterior / posterior and lateral kv - images were taken before each fraction and compared with the digitally - reconstructed radiographs , both using bony landmarks and ducial markers as reference . 
l utilizzo di marcatori duciali nella ig - pbi permette di migliorare laccuratezza del set - up rispetto allallineamento basato sui reperi ossei , in particolare nella direzione superiore / inferiore . radiol med ( 2013 ) 118 : 12121219 1213 parole chiave radioterapia guidata dalle immagini irradiazione parziale della mammella marcatori duciali introduction introduzione partial breast irradiation ( pbi ) has been emerging in the multidisciplinary management of early stage breast cancer after conservative surgery . 
treatment of only part of the breast has been justied by the observation that after lumpectomy most recurrences seem to occur in proximity to the primary tumour [ 1 , 2 ]  . 
the most often used modality is the three - dimensional conformal external beam radiotherapy ( 3d - crt ) technique , as described by the researchers of the william beaumont hospital [ 3 , 4 ]  . 
igrt can be dened as the use of frequent imaging during the course of radiotherapy treatment to track the target volume , and to ensure that highprecision dose distribution is delivered as planned . 
igrt with radio - opaque ducial markers has been established as a robust method to improve accuracy in patient set - up in a variety of pathologies , including prostate and lung cancer [ 5 ]  . although external beam pbi has been widely used in clinical practice , only few studies have investigated the role of igrt applied to this technique [ 6 ] , and it is not possible to draw denitive conclusions in this setting . 
in this study we investigated the role of igrt with ducial markers for pbi by comparing the table shifts for set - up correction based on bony anatomy and ducial markers . 
all the patients underwent a complete freebreathing computed tomography ( ct ) simulation to include all the organs at risk ( oar ) , according to the radiation therapy oncology group ( rtog ) 0413 protocol [ 7 ]  . 
the clinical target volume ( ctv ) consisted of the lumpectomy cavity , identied by the surgical clips , uniformly expanded by 1015 mm , limited to 5 mm from the skin surface and 5 mm from the lungchest wall interface . 
 il trattamento mirato ad una sola parte della mammella giusticato dal fatto che dopo quadrantectomia la maggior parte delle recidive si osservavano in prossimit del tumore primitivo [ 1 , 2 ]  . 
la tecnica pi comunemente utilizzata la radioterapia 3d conformazionale a fasci esterni , come descritto dai ricercatori del william beaumont hospital [ 3 , 4 ]  . la radioterapia guidata dalle immagini ( igrt ) rappresenta un fondamentale successo raggiunto negli ultimi anni nel campo della radioterapia oncologica . 
 ligrt con marcatori duciali radiopachi rappresenta una tecnica riproducibile per migliorare laccuratezza del setup del paziente in diverse patologie , tra cui il carcinoma della prostata e del polmone [ 5 ]  . nonostante la pbi a fasci esterni sia comunemente utilizzata nella pratica clinica , solo pochi studi hanno indagato il ruolo delligrt applicata a questa tecnica [ 6 ] , e quindi non possibile trarre conclusioni denitive in questo ambito . 
nel periodo di studio sono state sottoposte a pbi guidata dalle immagini ( ig - pbi ) 15 pazienti , con uno schema di 35 gy in 7 frazioni giornaliere ( 5 gy / frazione )  . 
le caratteristiche delle pazienti e dei tumori sono elencate in tabella 1 . al momento della chirurgia sono stati collocati nel letto tumorale almeno 3 marcatori duciali radiopachi ( clips chirurgiche )  . 
tutte le pazienti sono state sottoposte a simulazione in tomograa computerizzata ( tc ) in respiro libero , includendo tutti gli organi a rischio ( oar ) , in ac1214 table 1 patient and tumour characteristics radiol med ( 2013 ) 118 : 12121219 age , years median range ecog performance status 0 1 2 3 affected breast right left tumour location upper outer upper inner lower outer lower inner histology invasive ductal carcinoma invasive lobular carcinoma tumour dimension , cm median range t stage t1 t2 n stage n0 n1a ( mic ) nx grading g1 g2 g3 tabella 1 caratteristiche dei pazienti e del tumore et , anni mediana range performance status secondo ecog 0 1 2 3 mammella affetta destra sinistra posizione del tumore supero - esterno supero - interno infero - esterno infero - interno istologia carcinoma duttale invasivo carcinoma lobulare invasivo dimensioni del tumore , cm mediana range stadio t t1 t2 stadio n n0 n1a ( mic ) nx grado g1 g2 g3 6169 0 , 42 , 5 6169 0.42.5 the planning target volume ( ptv ) was calculated from the ctv using uniform three - dimensional expansion of 5 m ptv for evaluation ( ptv - eval ) is the structure used for dose - volume histogram ( dvh ) constraints and analysis ; it is limited to exclude the part outside the ipsilateral breast and the rst 5 mm of tissue under the skin and excluding the ptv expansion beyond the posterior extent of breast tissue . 
 radiation therapy was delivered to the ptv using threedimensional conformal elds , adopting the eld within a eld technique to improve dose homogeneity within the ptv and dosimetric coverage , as previously described [ 8 ]  . 
all treatments were developed using the eclipse treatment planning system ( varian medical systems , palo alto , ca , usa ) , using multiple planar and non - coplanar 6 - mv photon beams . 
the treatment was delivered by a trilogy linear accelerator equipped with a kv on - board imager system and a 120 - leaves millennium mlc ( varian medical systems )  . cordo con il protocollo radiation therapy oncology group ( rtog ) 0413 [ 7 ]  . 
il clinical target volume ( ctv ) consisteva nella cavit chirurgica , identicata dalle clips chirurgiche , uniformemente espansa di 1015 mm , limitata a 5 mm dalla supercie cutanea e 5 mm dall interfaccia polmone - parete toracica . 
il planning target volume ( ptv ) stato calcolato partendo dal ctv utilizzando una espansione tridimensionale di 5 mil ptv per la valutazione ( ptv - eval ) la struttura usata per lanalisi degli istogrammi dose volume ( dvh ) ; esso veniva limitato per escludere le strutture al di fuori della mammella ispilaterale e i 5 mm sottostanti la cute ed escludendo lespansione posteriormente oltre il tessuto mammario . 
il trattamento radioterapico veniva erogato al ptv utilizzando fasci di fotoni conformati , adottando la tecnica eld within a eld con lo scopo di minimizzare la dose agli organi adiacenti e ottenere una copertura efcace dl target [ 8 ]  . 
 right / left shifts were represented by x coordinate with + sign representing right shift and sign representing left shift ; superior / inferior shifts were represented by y coordinate with + sign representing superior shift and sign representing inferior shift ; anterior / posterior shifts were represented by z coordinate with + sign representing anterior shift and sign representing posterior shipatients were treated on ducial markers based shifts . the mean and standard deviation ( sd ) of displacements using both methods were calculated . 
students t test was used to detect a meaningful difference of 3 mm in absolute value between the shifts obtained with the bony landmarks method and ducial markers method ; statistical signicance was claimed for p < 0.05. results a total of 105 igrt sessions were obtained . 
the mean superior / inferior , right / left , and anterior / posterior shifts registered using the bony landmarks method were 2 mm ( sd 10 mm ) , 0 mm ( sd 7 mm ) , and 1 mm ( sd 7 mm ) , respecleclipse tratment planning system ( varian medical system , palo alto , ca , usa ) , utilizzando fasci multipli planari e non coplanari di fotoni da 6 mv . 
il trattamento radiante veniva erogato 34 settimane dalla simulazione con acceleratore lineare trilogy ( varian medical system )  . il set - up iniziale veniva eseguito grazie allallineamento dei tatuaggi cutanei con i laser di centramento . 
per il trattamento radiante il set - up delle pazienti si basava sulle clips chirurgiche . la media e la deviazione standard ( sd ) degli spostamenti sono stati calcolati con entrambi i metodi . 
il test t di student stato utilizzato per valutare se la differenza assoluta media tra gli spostamenti ottenuti con i due metodi fosse 1216 radiol med ( 2013 ) 118 : 12121219 fig . 
2 set - up del paziente utilizzando i marcatori duciali come riferimento . table 2 mean shifts and standard deviation derived from the bony landmark method and the ducial marker method bony landmark method fiducial markers method mean shift ( mm ) sd ( mm ) mean shift ( mm ) sd ( mm ) rl , right / left ; ap , anterior / posterior ; si , superior / inferior ; sd , standard deviation tabella 2 shift medi e deviazioni standard derivati dal metodo dei reperi ossei e dei marcatori duciali metodo dei reperi ossei metodo dei marcatori duciali shift medio ( mm ) ds ( mm ) shift medio ( mm ) ds ( mm ) ds , destra / sinistra ; ap , anteriore / posteriore ; si , superiore / inferiore ; ds , deviazione standard tively . 
the distribution of the mean differences in absolute value along the cardinal directions is reported in figure 3 . discussion in the present study we investigated the role of ducial markers for image - guided partial breast irradiation ( igpbi ) , by comparing the shifts based on bony anatomy and superiore a 3 mm ; stata attribuita signicativit statistica per p < 0 , 05 . risultati sono state eseguite 105 sessioni totali di igrt . 
gli spostamenti medi per il controllo del set - up basato sui reperi ossei nelle direzioni superiore / anteriore , destra / sinistra e anteriore / posteriore risultato essere di 2 mm ( sd 10 mm ) , 0 mm ( sd 7 mm ) , e 1 mm ( sd 7 mm ) , rispettivamente . 
gli spostamenti medi per il controllo del set - up basato sui marcatori duciali nelle direzioni superiore / anteriore , destra / sinistra e anteriore / posteriore risultato essere di 0 mm ( sd 7 mm ) , 1 mm ( sd 4 mm ) , e 0 mm ( sd 5 mm ) , rispettivamente ( tabella 2 )  . 
nevertheless , the ducial - markers method proved to be more accurate ( p = 0.001 ) along the superior / inferior direction ( table 3 )  . the superiority of the ducial marker method in the sole longitudinal direction might be explained by the different arm position kept by patients during the radiotherapy course , which can lead to a consensual shift of the breast and therefore of the target volume . the shifts for set - up correction reported in our study are rather wide , with a range of 10 , 7 and 7 mm along the sue anteriore / posteriore risulta essere di 5 mm ( range , 26 mm ) ( p = 0 , 001 ) , 3 mm ( range , 24 mm ) [ p = non signicativo ( ns ) ] , e 3 mm ( range , 14 mm ) ( p = ns ) ( tabella 3 )  . 
la distribuzione delle frequenze assolute riportata in figura 3 . discussione questo studio ha voluto denire il ruolo dei marcatori duciali nellig - pbi , confrontando gli spostamenti per la correzione del set - up relativi al posizionamento delle pazienti 1218 table 3 mean shift differences in absolute value ( mm ) between the bony landmark method and the ducial marker method mean shift difference ( mm ) range ( mm ) 24 14 26 0.001 rl , right / left ; ap , anterior / posterior ; si , superior / inferior ; ns , not signicant tabella 3 differenze medie degli shift in valore assoluto ( mm ) tra il metodo basato sui reperi ossei e i marcatori duciali differenze medie degli shift ( mm ) range ( mm ) 24 14 26 0 , 001 ds , destra / sinistra ; ap , anteriore / posteriore ; si , superiore / inferiore ; ns , non signicativo perior / inferior , lateral , and anterior / posterior direction , respectively , conrming the need of image - guidance for pbi . 
 with external - beam pbi techniques , the target volume being smaller than conventional whole - breast radiation therapy , the probability of a geographical miss becomes higher , and the need for image - guidance has been advocated to eliminate large random set - up errors . 
the average superior / inferior , lateral and anterior / posterior shifts registered were 2 mm ( range , 05 mm ) , 2 mm ( range , 14 mm ) , and 3 mm ( range , 15 mm ) , respectively . 
first , the advanced age of our patients ( median age , 69 years ) may cause difculties in patients positioning and set - up accuracy , leading to wide set - up errors . 
 in conclusion , we have shown that the use of ducial markers for ig - pbi increases the set - up accuracy compared to the bony landmarks , in particular along the superior / inferior direction . 
the role igrt is crucial to reduce the ctvptv margin , leading to a substantial reduction of the irradiation of the surrounding organs at risk including hearth , lung and residual breast . 
invece risultato pi accurato ( p = 0 , 001 ) lallineamento sui marcatori duciali nella direzione superiore / inferiore ( tabella 3 )  . la superiorit del metodo basato sui marcatori duciali nella sola direzione longitudinale pu essere spiegato dal diverso posizionamento del braccio mantenuto dalla paziente durante i trattamenti radioterapici , che pu provocare un normale spostamento della mammella e quindi del volume target . gli spostamenti della correzione del set - up riportati in questo studio sono piuttosto ampi , con un range di 10 , 7 e 7 mm lungo le direzioni superiore / inferiore , laterale e anteriore / posteriore , rispettivamente , confermando la necessit dellimage - guidance per la pbi . 
la tecnica pbi a fasci esterni prevede una notevole riduzione del volume target rispetto alla radioterapia convenzionale ( irradiazione dellintera ghiandola mammaria ) , per cui la probabilit di un errore del posizionamento diventa consistente e quindi si rende necessario lutilizzo dellimage - guidance per eliminare errori random del set - up . 
gli autori del princess margaret hospital hanno riportato che gli errori random sono ridotti da 2 , 4 , 2 , 2 e 2 , 9 mm dai tatuaggi a 1 , 5 , 1 , 5 e 1 , 6 mm grazie allutilizzo di cone - beam tc nelle direzioni destra / sinistra , anteriore / posteriore , e superiore / inferiore , rispettivamente [ 9 ]  . 
gli spostamenti medi registrati per la correzione del set - up nelle direzioni superiore / inferiore , laterale e anteriore / posteriore sono stati di 2 mm ( range , 05 mm ) , 2 mm ( range , 14 mm ) , e 3 mm ( range , 15 mm ) , rispettivamente . il nostro studio presenta alcuni limiti . 
primo , let avanzata delle pazienti ( et media = 69 anni ) pu aver causato difcolt nel posizionamento delle pazienti e nellaccuratezza del set - up , condizionando ampi errori di set - up . 
secondo , la piccola dimensione del campione potrebbe aver sottostimato altre differenze tra i due metodi di correzione del set up . in conclusione , abbiamo dimostrato che luso dei marcatori duciali per lig - pbi migliora laccuratezza del set - up rispetto ai reperi ossei , in particolare lungo la direzione superiore / inferiore . 
il ruolo delligrt cruciale per ridurre il margine ctv - ptv , portando ad una riduzione sostanziale dellirradiazione agli organi a rischio circostanti , tra cui cuore , polmone e mammella residua . 
la riduzione del margine ctv - ptv ci ha permesso di utilizzare un regime di radioterapia ipofrazionato , consistente in 35 gy erogati in 7 frazioni giornaliere ( 5 gy / frazione )  . 
i risultati cosmetici e la tossicit di questo schema di ipofrazionamento verranno riportati successivamente . radiol med ( 2013 ) 118 : 12121219 1219 conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
malag , e - mail : rmalag@sirm.org received : 2 january 2012 / accepted : 26 january 2012 / published online : 27 may 2013 springer - verlag 2013 abstract three separate venous systems drain the blood returning from the heart walls . 
coronary angiography ( ca ) with multidetector computed tomography ( mdct - ca ) and multiplanar reformations ( mpr ) , maximum intensity projection ( mip ) and 3d reconstructions provides noninvasive visualisation of normal cardiac veins and anatomical variants . 
the purpose of this pictorial review is to describe by mdct - ca the anatomy and main variants of the cardiac venous system . keywords mdct - ca venography cardiac veins anatomic variations riassunto il sangue reuo dal cuore raccolto da tre sistemi di vene caratterizzate da una notevole variabilit in termini di frequenza , calibro e decorso . 
conoscere lanatomia venosa cardiaca importante in relazione a manovre di cardiologia interventistica che richiedono la cateterizzazione delle vene cardiache , dal momento che alcune varianti anatomiche possono ostacolare o controindicare laccesso alle vene target . 
langiograa coronarica mediante tomograa computerizzata multistrato ( tcms ) permette , tramite ricostruzioni 3d , ricostruzioni multiplanari ( mpr ) , mpr curve e proiezioni di massima intensit ( mip ) , la visualizzazione dellanatomia venosa cardiaca normale e delle sue varianti in modo non invasivo , fornendo una valida alternativa alla venograa retrograda . 
lo scopo di questo pictorial consiste nella descrizione mediante immagini tcms con ricostruzioni 3d dellanatomia e delle principali varianti delle vene cardiache . parole chiave angiograa coronarica - tcms vene cardiache varianti anatomiche introduction introduzione blood returning from heart walls is collected by three different venous systems . 
the il sangue reuo dal cuore raccolto da tre sistemi di vene tra loro ampiamente connesse e caratterizzate da una notevole variabilit in termini di frequenza , calibro e decorso [ 1 , 2 ]  . 
placing implantable cardioverter debrillators ( icd ) and biventricular pacemakers in patients with heart failure and impaired ventricular synchronisation requires access to the venous tree through the cs to place an electrode at the posterior or posterolateral wall of the left ventricle . 
the anatomical variations involve presence , size and vessel course and venous conuence angle . to date , the method used to investigate the venous tree has been retrograde venography [ 311 ]  . 
coronary angiography ( ca ) with multidetector computed tomography ( mdct - ca ) allows noninvasive investigation through 3d , multiplanar reformation ( mpr ) and maximum intensity projection ( mip ) reconstructions normal cardiac venous anatomy and anatomical variations , thus providing an adequate and accurate alternative to retrograde venography [ 1215 ]  . 
the purpose of this pictorial is to describe , using mdct - ca imaging , the main variants of cardiac veins . normal anatomy blood returning from the heart walls is collected by three venous systems that are widely interconnected [ 1 ]  . 
the three systems are : ( 1 ) the anterior vein , ( 2 ) the coronary siradiol med ( 2013 ) 118 : 11491156 sistema delle vene di tebesio e il sistema del seno coronarico ( cs )  . 
il posizionamento di debrillatori e di pacemaker bi - ventricolari , utilizzati nella terapia di resincronizzazione cardiaca ( crt ) nei pazienti affetti da scompenso cardiaco con alterata sincronizzazione ventricolare , rende necessario laccesso al sistema venoso del seno coronarico per collocare un elettrodo stimolatore in corrispondenza della parete posteriore o postero - laterale del ventricolo di sinistra . 
le variazioni anatomiche interessano il calibro , il decorso , langolo di conuenza venosa e la presenza stessa di tali vasi . ad oggi la metodica pi utilizzata per lo studio delle vene cardiache e quindi per la visualizzazione delle eventuali varianti la venograa retrograda [ 311 ]  . 
langiograa coronarica mediante tomograa computerizzata multistrato ( tcms ) permette tramite ricostruzioni 3d , ricostruzioni multiplanari ( mpr ) , mpr curve e proiezioni di massima intensit ( mip ) la visualizzazione dellanatomia venosa cardiaca normale e delle sue varianti in modo non invasivo , fornendo una valida ed accurata alternativa alla venograa retrograda [ 1215 ]  . 
lo scopo di questo pictorial consiste nella descrizione , mediante immagini tcms con ricostruzioni 3d , dei principali aspetti anatomici e delle varianti anatomiche delle vene cardiache . anatomia venosa il sangue reuo dal cuore raccolto da tre sistemi di vene tra loro ampiamente connesse [ 1 ] : il sistema delle vene anteriori , il sistema delle vene di tebesio e il sistema del cs . 
1a - c three - dimensional normal venous anatomy : normal anatomy of the cardiac venous system with maximum intensity projection mip images ( a ) and volume rendering ( b , c )  . 
it runs along the posterior coronary groove , crosses the crux of the heart and ends in the right atrium , below the ostium of the inferior vena cava and above the atrioventricular plane . 
as it courses in the atrioventricular groove forming a u - shaped path , the gcv receives lmv at the obtuse margwhen it reaches the crux of the heart , the gcv ends in the cs at the orice of the mv , which is a remnant of the embryonic left upper cardinal vein [ 1 ]  . 
mentre procede nella met sinistra del solco coronario , formando un tragitto a u , la gcv riceve , in corrispondenza del margine ottuso , un afuente non costante : la vena marginale sinistra ( lmv )  . 
portandosi in direzione della croce del cuore , la gcv si continua nel cs in corrispondenza dellostio della vena obliqua dellatrio sinistro o vena di marshall ( mv ) , residuo della vena cardinale embrionale superiore sinistra [ 1 ]  . 
 importante notare che nei pazienti in cui la lpv singola , essa molto posteriore ed parallela e vicina alla vena cardiaca media ( mcv ) , risultando probabilmente sfavorevole 1152 radiol med ( 2013 ) 118 : 11491156 the interventional cardiologist . 
as the vieussens valve and the mv are not always represented , it might be difcult to establish the boundary between the cs and the gcv [ 21 ]  . 
this vein is a variable vessel [ 1 ] : sometimes it is not represented ; in other cases , several vessels running parallel to one other have been described . 
it moves along the posterior interventricular groove and ends in the cs at the crux of the heart [ 1 ] , forming a 6090 angle [ 21 ]  . 
the diameter of its orice is approximately 2.61.3 mm [ 21 ]  . the scv ( fig 1a , b ) runs along the right diaphragmatic part of the coronary groove and ends in the cs . 
the scv receives the right cardiac vein , a slender vessel belonging to the anterior cardiac venous systethis vein runs along the acute margin and ends in the scv or directly in the atrial lumen . the anterior venous system drains blood from the sternocostal surface of the right ventricle . 
the anterior veins run along the anterior ventricular surface , in subepicardial position , cross the cs and the right coronary artery deeply or supercially and end in the right atrium separately or creating one or more common trunks . 
 the right marginal vein is the main vessel of the anterior venous system , ending in the anterior or , rarely , posterior wall of the right atrium independently or after receiving one or more small anterior veins . 
the anterior and coronary venous systems are widely interconnected at the apex and close to the atrioventricular groove [ 1 ]  . the thebesian venous system consists of many minute veins called the thebesian veins . 
questultima un esile vaso , appartenente al sistema delle vene cardiache anteriori , che sale lungo il margine acuto del cuore e che pu terminare nella scv oppure direttamente nellatrio destro . il secondo sistema venoso , rappresentato dalle vene cardiache anteriori , drena parte del sangue proveniente dalla faccia sterno - costale del ventricolo destro . 
il numero delle vene cardiache anteriori piuttosto variabile : di norma non sono pi di due o tre , ma in alcuni casi ne sono state descritte no a cinque . 
esse risalgono la parete anteriore del ventricolo in posizione subepicardica , incrociano il seno coronario , passando profondamente o supercialmente allarteria coronaria destra , e terminano nellatrio destro separatamente o dopo aver dato origine ad uno o pi tronchi comuni . 
il sistema del cs e il sistema delle vene anteriori sono ampiamente anastomizzati a livello dellapice cardiaco e in prossimit dal solco interventricolare anteriore [ 1 ]  . il terzo sistema venoso costituito da minute e numerose vene : le vene di tebesio . 
le ricostruzioni mip ( a , b ) e tridimensionali mostrano ( c ) una scv che termina nella vena cardiaca media ( mcv ) invece che nel seno coronario . 
 le immagini mip ( a ) e 3d ( b ) mostrano lorigine anomala della vena cardiaca posteriore dalla vena cardiaca media . radiol med ( 2013 ) 118 : 11491156 1155 discussion discussione anatomical variations of the cardiac venous circulation are so frequent that it is difcult , at least for some elements , to dene normal anatomy [ 1 ]  . 
studied the coronary venous system by mdctca in 89 patients and obtained adequate image quality in 84 examinations [ 24 ]  . the authors noted above demonstrated the presence of the lmv in 67% of cases and the lpv in 75% of patients . 
all patients had at least one of these two vessels : in 52% there was only one vessel ; in 25% both veins were represented ; in 22% there were three or more vessels . 
the angles of conuence between these vessels and the cs are also variable : < 90 for 93% of the lpv and for 94% of the lmv [ 24 ]  . le varianti anatomiche del circolo venoso cardiaco sono tanto frequenti da rendere difcile , almeno per quanto riguarda alcuni elementi , la denizione dellassetto anatomico normale [ 1 ]  . 
sono molto pi eterogenee in termini di presenza , numero , dimensioni e decorso la scv , la mcv , la vena di marshall , lpv e lmv [ 1 ]  . 
questi autori hanno dimostrato la presenza della lmv nel 67% dei casi e della lpv in 75% dei pazienti ; tutti i pazienti presentavano almeno uno dei due vasi : nel 52% dei casi vi era un solo vaso , nel 25% dei casi erano rappresentate entrambe le vene e nel 22% dei casi vi erano tre o pi vasi . 
stata inoltre descritta la variabilit della distanza tra lostio del cs e le vene che percorrono la parete posterolaterale del ventricolo di sinistra : 62 , 5 mm32 , 5 mm per la lmv e 58 , 6 mm32 mm per la lpv . 
 anche langolo di ingresso nel cs variabile : inferiore ai 90 per il 93% delle lpv e per il 94% delle lmv [ 24 ]  . 1156 conclusions radiol med ( 2013 ) 118 : 11491156 conclusioni mdct - ca is able to provide highly accurate anatomical imaging of the cardiac venous system , allowing a preliminary assessment of the coronary venous anatomy , particularly regarding cs calibre ; size , course and extent of target veins for catheterisation and lead placement ; and it allows exclusion of conditions and anatomical variations that might hinder correct lead placement . 
mdct - ca venous mapping may represent an alternative to retrograde venography , as it provides a noninvasive evaluation of cardiac veins . attualmente la ac - tcms in grado di fornire un imaging anatomico delle vene cardiache con elevata accuratezza permettendo una preliminare valutazione dellanatomia del sistema venoso coronarico , del calibro del seno coronario , del calibro e dellestensione delle vene coronariche ai ni del cateterismo e dellimpianto di elettrodo stimolatore e consentendo di escludere la presenza di condizioni e di varianti anatomiche possibile causa di ostacolo al corretto posizionamento degli elettrocateteri . 
 lesame si propone quindi come alternativa alla venograa retrograda in quanto fornisce una visualizzazione con modalit non invasiva . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
alberti , spedali civili , piazzale spedali civili 1 , 25123 brescia , italy 2radiotherapy and radiosurgery department , istituto clinico humanitas , humanitas cancer center , rozzano - milano , italy 3radiation oncology department , tomotherapy unit , ospedale regionale u . 
maria nuova , reggio emilia , italy 5service doncologie radiothrapie , chu ibn rochd , casablanca , morocco 6department of radiation oncology , university of florence , florence , italy 7division of radiotherapy , european institute of oncology and university of milan , milan , italy 8department of medical and surgical sciences , radiation oncology unit , university of turin , turin , italy correspondence to : b . 
de bari , e - mail : bdebari@yahoo.it received : 27 february 2012 / accepted : 27 april 2012 / published online : 27 may 2013 springer - verlag 2013 abstract purpose . 
despite the large number of patients treated with rt , some issues about optimal techniques , doses , volumes , timing , and association with androgen deprivation are still subject of debate . 
two of them were prostate cancer cases that could be treated by rt + / hormonal therapy ( ht ) , different for t stage of primary tumour according to tnm , preoperative diagnostic procedures for staging , initial prostate specic antigen ( ipsa ) , and gleason score sum of biopsy . 
for each clinical case , radiation oncologists were asked to : ( a ) give indication to pretreatment procedures for staging ; ( b ) give indication to treatment ; ( c ) dene specically , where indicated , total dose , type of fractionation , volumes of treatment , type of technique , riassunto obiettivo . 
nonostante il grande numero di pazienti trattati con rt , alcune controversie circa la tecnica ottimale di trattamento , le dosi , i volumi , il timing rispetto alla chirurgia e lassociazione con la terapia ormonale sono ancora oggetto di dibattito . 
due di questi casi clinici si presentavano adeguati alla rt a scopo radicale + / ormonoterapia ( ot ) , ed erano diversi per stadio clinico , procedure diagnostiche di staging pre - trattamento , antigene specico della prostata ( psa ) iniziale , gleason score bioptico . 
per ogni caso clinico si chiedeva di ( a ) dare indicazione a nuove procedure di staging pre - trattamento ; ( b ) dare indicazione al trattamento ; radiol med ( 2013 ) 118 : 12201239 1221 type of image - guided setup control ; ( d ) indicate if ht should be prescribed ; ( e ) dene criteria that particularly inuenced prescription . 
these patients probably deserve a more uniform approach , based on upto - date , detailed , and evidence - based recommendations . keywords procaina survey radical radiotherapy prostate cancer hormonal therapy ( c ) denire in particolare , se indicato , la dose totale , il tipo di frazionamento , i volumi di trattamento , il tipo di tecnica , il tipo di controllo del set - up guidato dalle immagini ; ( d ) dare indicazione a un trattamento ormonale eventuale ; ( e ) denire i criteri maggiormente inuenzanti la prescrizione . 
questi pazienti meriterebbero un approccio pi uniforme basato su raccomandazioni aggiornate , dettagliate e condivise sulla base delle evidenze disponibili . parole chiave procaina survey radioterapia radicale cancro prostatico ormonoterapia introduction introduzione prostate cancer is the second cause of cancer incidence and the third cause of cancer - related death in males [ 1 ]  . 
 radiotherapy ( rt ) , with or without hormonal therapies ( ht ) , offers a potentially curative treatment , in both lowintermediate and high - risk prostate cancer patients [ 24 ]  . 
moreover , in recent years , new modalities in treatment planning , delivery , and setup verication have been introduced in the clinical setting of prostate cancer patients [ 58 ]  . 
in 2002 , a national italian survey assessed the pattern of care in the treatment of 1759 prostate cancer patients concluding that the full spectrum of treatment options could be offered to prostate cancer patients [ 9 ]  . 
la radioterapia ( rt ) , con o senza ormonoterapia ( ot ) offre un trattamento potenzialmente curativo , sia per pazienti con cancro prostatico a rischio basso - intermedio che per pazienti ad rischio alto [ 24 ]  . 
inoltre , recentemente sono state introdotte nel trattamento dei pazienti con cancro prostatico nuove modalit nella pianicazione ed erogazione del trattamento , oltre che nella verica del set - up [ 58 ]  . 
nel 2002 , una survey nazionale italiana ha valutato il pattern of practice nel trattamento di 1759 pazienti affetti da cancro alla prostata concludendo che gi allora lintero spettro di opzioni di trattamento poteva essere offerto a tali pazienti [ 9 ]  . 
inoltre , i progressi nel campo delle scienze radiologiche e della medicina nucleare hanno sicuramente inuenzato la pratica clinica degli oncologi radioterapisti in questo scenario clinico [ 1012 ]  . il progetto procaina ( prostate cancer indications attitudes ) unindagine nazionale promossa da airo giovani ( la sezione giovani dellassociazione italiana di 1222 radiol med ( 2013 ) 118 : 12201239 oncology ) on behalf of the airo prostate cancer working group in order to assess patterns of care in prostate rt among italian radiation oncologists and to analyse criteria that inuence the choices of physicians . in the survey , a questionnaire with four cases of prostate cancer was submitted to radiation oncologists attending the airo 2010 national congress . 
every questionnaire consisted of two parts . the rst part contained personal and professional details ( italian working region , public / private hospital , academic / non - academic title , on - going prostate cancer trials in respondents department )  . the second part presented four clinical cases of prostate cancer patients , two candidates for exclusive radical rt ( table 1 ) and two candidates for post - operative rt [ 13 ]  . 
for each of the two clinical cases of exclusive rt , the radiation oncologists were asked to : establish the indication for complementary pre - treatment staging imaging ; establish the indication for treatment ; dene specically , where indicated , total dose , type of fractionation , volumes of treatment , type of technique , type of image - guided approach ; enced the prescription . every clinical case presented the same scheme . 
i 2 casi clinici di radioterapia post - operatoria sono stati oggetto di un report a parte [ 13 ]  . materiali e metodi popolazione e contesto di studio trecento questionari anonimi sono stati consegnati ai partecipanti al congresso nazionale airo 2010 . 
ogni questionario era composto da 2 parti . la prima parte conteneva informazioni personali e professionali ( regione di lavoro , ospedale pubblico / privato , titolo accademico , presenza nel proprio centro di un protocollo attivo sul tumore della prostata )  . lultima parte presentava 4 casi clinici di tumore della prostata , 2 candidabili a rt esclusiva ( tabella 1 ) e 2 candidabili a rt post - operatoria [ 13 ]  . 
per ognuno dei 2 casi concernenti la radioterapia esclusiva , stato chiesto ai radio - oncologi di : indicare eventuali esami radiologici di stadiazione pretrattamento ; dare indicazione eventuale a trattamento radiante ; denire nello specico dose totale , tipo di frazionamento , volumi di trattamento , tipo di tecnica di rt , tipo di approccio igrt ; caratterizzare i fattori inuenzanti la scelta terapeutica . ogni caso clinico presentava il medesimo schema . 
il presente studio riguarda solamente i 2 casi clinici riguardanti lo scenario della rt radicale . in totale , 128 / 300 questionari sono stati considerati per la presente analisi . only questionnaires that were completely lled , at least in the part of the clinical cases , were considered for the nal analysis . 
the present report presents only the data and results about the two cases regarding radical rt . risultati give information about the reasons that particularly inucriteri di inclusione e raccolta dati 1223 radiol med ( 2013 ) 118 : 12201239 table 1 description of the two proposed clinical cases clinical case #1 ( high - risk patient ) clinical case #2 ( low - risk patient ) 72 years , ps : 0 ( ecog )  . 
no psa decrease after antibiotics and antiinammatory therapies biopsies : prostate adenocarcinoma , gleason score 5 + 4 ( 7 / 12 positive biopsy cores ) dre : increased dimensions of the prostate ( > 5 cm in cranio - caudal direction ) , hard nodule at the left lobe . 
 no signs of extra - capsular invasion trus : volume : 55 cc , signs of extra - capsular extension , hypoechogenic nodule of 3 cm in diameter in the left lobe . 
no comorbidities signs and symptoms : moderate nocturia + increased psa , without remission after antibiotics ( 6 ng / ml and 9 ng / ml before and after antibiotics , respectively )  . biopsies : prostate adenocarcinoma , gleason score 3 + 3 ( 2 / 12 positive biopsy cores ) dre : no pathological signs at prostate examination , without nodules . 
nessuna riduzione del psa dopo terapia antibiotica e anti - inammatoria biopsie : adenocarcinoma prostatico , gleason score 5 + 4 ( 7 / 12 biopsie positive ) dre : prostata di dimensioni aumentate ( > 5 cm nella direzione cranio - caudale ) , nodulo duro nel lobo sinistro . 
non segni di effrazione extracapsulare trus : volume : 55 cc , segni di effrazione extracapsulare , nodulo ipoecogeno di 3 cm di diametro nel lobo sinistro non segni di invasione delle vescicole seminali scintigraa ossea e tc addominale : negative 60 anni , ps : 0 ( ecog )  . 
nessuna riduzione del psa dopo terapia antibiotica ( 6 ng / ml e 9 ng / ml rispettivamente prima e dopo terapia antibiotica ) biopsie : adenocarcinoma della prostata , gleason score 3 + 3 ( 2 / 12 biopsie positive ) dre : non segni patologici allesame prostatico , non noduli sospetti . 
 most of them ( 9.5% of total ) declared a clinical trial on image - guided rt ( igrt ) with the use of cone - beam computed tomography ( cb - ct ) during rt for prostate cancer treatment , while the others declared at least one trial for metastatic patients . analisi descrittiva la tabella 3 riassume i principali risultati dello studio , mostrando le principali differenze tra i 2 casi . 
come possibile osservare nella tabella 4 , sono evidenziabili importanti differenze . radiol med ( 2013 ) 118 : 12201239 1227 descriptive analysis caso clinico #1 table 3 summarizes the principal results of the survey , showing the main differences between the two proposed clinical cases . 
as can be seen in table 4 , important differences can be underlined . clinical case #1 the rst clinical case was a high - risk prostate cancer patient ( following the damico classication , [ 14 ] )  . 
the descriptive analysis showed : staging : 58.6% of the radiation oncologists considered appropriate to prescribe other radiological procedures , with 43.7% of them stating they would prescribe pretreatment magnetic resonance imaging ( mri ) , 4.7% 11 - choline positron - emission tomography / ct ( pet / ct ) and 10.2% both the proposed procedures ; treatment indication : in 99.2% of questionnaires rt was indicated ; association with ht : even though 6.1% would prescribe only rt , the majority of respondents considered appropriate a treatment with rt - ht , with an optimal ht duration ranging between 12 ( 17.2% ) and 36 months ( 65.6% ) ; doses and volumes : 72.7% would deliver a radiation dose between 70 and 80 gy . 
intraprostatic markers were chosen by 3.2% of respondents ; patient condition : full bladder and empty rectum in the supine position were preferred in 85.2% of the cases ; il primo caso clinico riguardava un paziente affetto da carcinoma prostatico ad alto rischio ( secondo la classicazione di damico [ 14 ] )  . 
lanalisi descrittiva ha mostrato : stadiazione : il 58 , 6% dei radio - oncologi ritiene appropriato prescrivere altre indagini radiologiche , in particolare una risonanza magnetica nucleare ( rmn ) nel 43 , 7% dei casi , una tc - pet colina ( tc - pet ) nel 4 , 7% dei casi ed entrambe nel 10 , 2% delle risposte ; indicazione al trattamento : la rt stata indicata del 99 , 2% dei questionari ; associazione con deprivazione androgenica ( ht ) : il 6 , 1% dei partecipanti prescriverebbe sola rt ; tuttavia , la maggior parte dei radio - oncologi considera appropriata la combinazione terapeutica tra rt e ht della durata ottimale di 12 mesi ( 17 , 2% ) o 36 mesi ( 65 , 6% ) ; dosi e volumi : il 72 , 7% dei radio - oncologi prescriverebbe una dose compresa tra 70 gy e 80 gy . 
un ipofrazionamento moderato stato scelto nel 29 , 1% dei questionari ( 2530 frazioni di 2 , 13 gy ) , mentre solo 2 colleghi erogherebbero dosi per frazione > 3 gy . 
la prostata e le vescichette seminali ( con margini adeguati ) sono stati giudicati essere il volume bersaglio nel 50 , 8% dei casi , mentre la pelvi stata scelta nel 39 , 8% dei questionari ; tecniche : la radioterapia conformazionale 3d ( 3dcrt ) o a intensit modulata ( imrt ) stata scelta rispettivamente dal 41 , 4% e dal 45 , 3% dei partecipanti . 
interessante notare che il 10 , 2% dei radio - oncologi utilizzerebbe la imrt per il volume pelvico e la 3dcrt per la prostata ; controllo del posizionamento del paziente : le immagini portali settimanali sono state scelte dal 46 , 8% , la cbct dal 16 , 1% giornalmente e dal 16 , 1% settimanalmente . 
i reperi duciali intra - prostatici sono stati scelti nel 3 , 2% dei questionari ; preparazione del paziente : vescica piena e retto vuoto , in posizione supina , lo scenario preferito nell85 , 2% dei casi ; lo stadio di malattia da solo ( 13 , 2% ) o associato ai dati di letteratura ( 10 , 2% ) o allet e alla letteratura ( 11% ) sono stati i criteri di scelta pi rappresentati per decidere la necessit e le modalit della rt . caso clinico #2 il secondo caso clinico riguardava un paziente affetto da tumore della prostata a basso rischio ( secondo la classicazione di damico [ 14 ] )  . 
in 15% of answers radical prostatectomy was considered the best option for the patient ; association with ht : even though 10.7% would prescribe ht , the majority of radiation oncologists considered appropriate a treatment with exclusive rt ; doses and volumes : 68.5% would deliver a dose of radiotherapy between 70 and 80 gy . 
the prostate alone ( with adequate margins ) was the target volume in 76% of indications , while irradiation of seminal vesicles was considered desirable in 23.1% of cases ; techniques : a total of 97.2% of respondents would deliver rt by 3d - crt ( 45.1% ) or imrt ( 52.1% ) ; control of patient setup : weekly portal imaging was the method proposed by 56.7% of radiation oncologists for controlling patient setup , while 29.8% of them would perform igrt by cb - ct , on a daily ( 14.9% ) or a weekly basis ( 14.9% ) ; patient condition : full bladder and empty rectum in the supine position was preferred by 81.1% ; none of the proposed criteria reached at least 10% of the preferences . 
the literature data together with the patients age ( 9.1% ) or disease stage ( 8.3% ) were the most represented criteria for the choice of treatment prescription and modalities . indicata dall82 , 6% dei questionari . 
la radioterapia a fasci esterni ( ebrt ) stata scelta dal 54 , 3% del radiooncologi , la brachiterapia ( brt ) dal 28 , 3% ( 20 / 128 a basso rateo di dose , 8 / 128 ad alto rateo di dose )  . 
il 15% dei questionari consigliava la prostatectomia radicale ; associazione con deprivazione androgenica ( ht ) : anche se il 10 , 7% dei radio - oncologi prescriverebbe ht , la maggioranza considera appropriato un trattamento con rt esclusiva ; dosi e volumi : il 68 , 5% dei radio - oncologi prescriverebbe una dose compresa tra 70 gy e 80 gy . 
un ipofrazionamento moderato stato scelto nel 32 , 4% dei questionari ( 2530 frazioni di 2 , 13 gy ) , mentre solo 1 collega erogherebbe dosi per frazione > 3 gy . 
la prostata sola ( con margini adeguati ) stata giudicata essere il volume bersaglio nel 76% dei casi , mentre laggiunta delle vescichette seminali stata scelta nel 23 , 1% dei questionari ; tecniche : la radioterapia conformazionale 3d ( 3dcrt ) o ad intensit modulata ( imrt ) stata scelta dal 45 , 1% e dal 52 , 1% dei partecipanti ( totale di 97 , 2% )  . controllo del posizionamento del paziente : le immagini portali settimanali sono state scelte dal 56 , 7% , la cbct dal 14 , 9% giornalmente e dal 14 , 9% settimanalmente ; preparazione del paziente : vescica piena e retto vuoto , in posizione supina , lo scenario preferito nell81 , 1% dei casi ; nessuno dei criteri di scelta proposti ha raggiunto la soglia del 10% . 
i dati di letteratura insieme allet del paziente ( 9 , 1% ) o insieme allo stadio di malattia ( 8 , 3% ) sono stati i pi considerati nel decidere la necessit e le modalit della rt . discussione in questo studio presentiamo il primo sondaggio , basato su questionari , sulle scelte dei radio - oncologi italiani nellaffrontare il trattamento rt radicale nei pazienti affetti da neoplasia prostatica . 
quindi , questa stata la principale motivazione nel condurre il sondaggio . sebbene limpatto dellesperienza o del volume di pazienti nellospedale non sia oggetto di questo lavoro , i risultati del sondaggio potrebbero probabilmente riettere non solo le varie strategie applicate nei diversi centri di radioterapia italiani , ma anche le differenti esperienze dei clinici intervistati ( numero di pazienti con cancro della prostata trattati annualmente , livello di training , ad esempio specialisti rispetto a specializzandi )  . 1230 discussion we present the rst italian questionnaire - based survey of italian radiation oncologists on radical rt in prostate cancer patients . 
although this clinical subset is rather frequent in daily clinical practice , the pattern of care could vary considerably between different countries and , within the same country , between different physicians . 
 moreover , a possible bias of the survey could be the fact that some radiation oncologists would answer following evidence largely available in the literature ( i.e. , by saying what seems the best thing to do ) rather than following their real clinical practice ( i.e. , by saying what seems the best i can do )  . 
 one of the major issues in this sense would be the correct therapeutic approach , particularly in the choice between radical prostatectomy ( rp ) and radical irradiation ( ri )  . 
although no clinical randomised trial has been performed to directly compare rp and ri , available data seem to conrm that in clinically localised prostate cancer the two approaches are equally effective [ 15 ]  . 
on the contrary , in locally advanced prostate cancer patients , different surgical reports have shown the high risk of extracapsular extension and / or microscopic residual disease , and rt + / ht is the standard of care with the highest level of evidence [ 15 ]  . a possible solution could be a real multidisciplinary approach in a context of close cooperation between surgeons and radiation oncologists in order to deliver more evidencebased treatments , to avoid overtreatment and soaring costs [ 16 ]  . 
the introduction and spread of the concept of prostate units in hospitals would be a possible solution [ 17 ]  . to treat or not to treat : a real dilemma ? active surveillance ( as ) is an acceptable therapeutic option for clinically localised prostate cancer patients [ 18 , 19 ]  . 
 available data show that the 5to 10 - year cancer - specic mortality is very low for most prostate cancers , except for those that are poorly differentiated [ 20 , 21 ]  . 
the aim of this attitude is to reduce the number of overtreatments , reserving therapies only to the 30% of men that would require delayed radical intervention [ 22 ]  . 
different series have identied several eligibility criteria for potential as patients [ 15 ]  . radiol med ( 2013 ) 118 : 12201239 inoltre , un possibile bias dello studio potrebbe risiedere nel fatto che alcuni radio - oncologi possono rispondere seguendo maggiormente le evidenze disponibili in letteratura ( ad esempio , indicando ci che sembra il meglio da fare ) senza realmente effettuare nella pratica clinica ci che si affermato ( ad esempio , il meglio che si pu fare )  . 
 nonostante ci , riteniamo che i nostri risultati forniscano un interessante spaccato riguardante le controversie nella gestione del tumore della prostata . uno dei principali problemi in questo senso sarebbe il corretto approccio terapeutico , in particolare nella scelta tra prostatectomia radicale ( rp ) e irradiazione radicale ( ri )  . 
al contrario , nei pazienti affetti da tumore localmente avanzato , diversi report chirurgici hanno dimostrato lalto rischio di estensione extracapsulare e / o malattia microscopica residua , e la rt + / ot lo standard di cura con il pi alto livello di evidenza [ 15 ]  . una possibile soluzione potrebbe essere un vero approccio multidisciplinare in un contesto di stretta collaborazione tra chirurghi e radio - oncologi , al ne di fornire pi trattamenti evidence - based , per evitare over - treatment con conseguente aumento dei costi [ 16 ]  . 
lintroduzione e la diffusione del concetto di gruppo multidisciplinare uro - oncologico negli ospedali sarebbe una possibile soluzione [ 17 ]  . trattare o non trattare : un vero dilemma ? la sorveglianza attiva ( as ) unopzione terapeutica accettabile per i pazienti affetti da cancro della prostata clinicamente localizzato [ 18 , 19 ]  . 
i dati disponibili mostrano che a 510 anni la mortalit cancro - specica molto bassa per la maggior parte dei tumori della prostata , a eccezione di quelli scarsamente differenziati [ 20 , 21 ]  . 
lo scopo di questo atteggiamento di ridurre il numero di overtreatment , riservando terapie soltanto al 30% degli uomini che richiederebbe un intervento terapeutico radicale ritardato nel tempo [ 22 ]  . 
diverse serie hanno individuato vari criteri di ammissibilit per i pazienti potenzialmente candidati a as [ 15 ]  . nella nostra indagine , il secondo caso clinico potrebbe avere caratteristiche tali da proporre una as . 
tuttavia , let e / o lo stadio clinico non sono stati il criterio di scelta pi importante per gli oncologi , con solo il 2 , 5% e 4 , 1% delle preferenze , rispettivamente ( tabella 4 )  . quali esami di staging prima del trattamento ? le linee guida della associazione europea di urologia ritengono che la stadiazione di un paziente affetto da cancro alla prostata debba essere effettuata con la dre , la concenradiol med ( 2013 ) 118 : 12201239 1231 in our survey , the second clinical case would have characteristics that could potentially justify proposing as . 
in addition to morphological t2 - weighted sequences , the main functional techniques employed for prostate evaluation are diffusion - weighted mri [ 23 ] , dynamic contrast - enhanced mri [ 24 ] , and proton mr spectroscopic imaging [ 25 ]  . 
it was shown that 11c - choline petct is able to detect foci of prostate cancer , but with a high false - negative rate on a sextant basis ; the sensitivity of the method became signicant ( 83% ) only for nodules greater trazione sierica di psa e le biopsie ecoguidate [ 15 ]  . recentemente , le moderne tecniche di scienze radiologiche e di medicina nucleare stanno giocando un ruolo crescente nella stadiazione di pazienti con cancro alla prostata . 
la possibilit di incorporare i dettagli funzionali nella risonanza magnetica ad alta risoluzione spaziale aumenta lutilit di questa procedura diagnostica , che potenzialmente pu essere una guida per la gestione terapeutica in pazienti con cancro prostatico . 
oltre alle sequenze morfologiche t2 - pesate , le principali tecniche impiegate per la valutazione funzionale della prostata sono la diffusion - weighted mri [ 23 ] , la dinamic contrast enhanced mri [ 24 ] e la mri spettroscopica [ 25 ]  . 
questo potrebbe essere probabilmente correlato a un accesso limitato alla mri . il ruolo della pettc nella stadiazione di pazienti affetti da cancro della prostata ancora in fase di valutazione e i risultati preliminari sono in conitto . 
stato dimostrato che la pet / ct con 11c - colina in grado di rilevare foci di cancro alla prostata , ma con un alto tasso di falsi negativi ; la sensibilit del metodo diventa signicativa ( 83% ) solo per noduli superiori a 5 m husarik et al . 
 [ 29 ] hanno pubblicato risultati scoraggianti sulla stadiazione del tumore della prostata con pet / ct - 11ccolina : la reale utilit nella stadiazione di pazienti dopo prostatectomia radicale stata valutata per i livelli di psa > 2 ng / ml . 
infatti , se alcuni autori ritengono che una soglia di suv di 2 , 65 sia in grado di rilevare e individuare correttamente le principali aree di cancro alla prostata [ 30 , 31 ] , altri supportano lutilizzo di altri parametri , come la delayed - early suvmax [ 32 ] o il rapporto tra suvmax del 1232 radiol med ( 2013 ) 118 : 12201239 than 5 mhusarik et al . 
 [ 29 ] published discouraging ndings in staging prostate cancer with 11c - choline pet - ct : the real usefulness in the staging of patients with radical prostatectomy was assessed for psa levels > 2 ng / ml . 
in fact , while some authors consider that a suv threshold of 2.65 can detect and correctly locate major areas of prostate cancer [ 30 , 31 ] , others support the use of different techniques , such as the ( delayed - early ) suvmax [ 32 ] or the ratio between the suvmax of prostate cancer and that of pelvic muscle [ 33 ]  . 
 in conclusion , based on the spatial resolution of pet systems ( about 5 mm ) , 11c - choline pet / ct could be useful to detect lesions greater than 5 mm within the prostate gland , especially when the acquisition is dynamic , or when early and delayed images are both acquired ( dual phase ) [ 34 ]  . correctly , the radiation oncologists participating in this survey did not consider 11c - choline pet / ct an essential diagnostic tool in staging the proposed clinical cases : it was prescribed by only 5.5% of respondents ( alone or with mri ) in the low - risk clinical case , and by 14.9% of them ( alone or with mri ) in the high - risk case , with only 4.7% of respondents prescribing only 11 - choline pet / ct in this setting . volume to treat , doses and techniques volumes volumes to be treated in prostate cancer radiotherapy still remain debated . 
particularly , it is still not universally dened whether the seminal vesicles ( sv ) and pelvic lymph nodes should be encompassed in the clinical target volume ( ctv ) in the irradiation of low - intermediate and high - risk prostate cancers , respectively . 
these controversies are becoming increasingly important in this era of high conformal and intensity - modulated radiotherapy techniques . sv invasion is clearly a negative prognostic factor and sv should be encompassed in the ctv when other negative prognostic factors exist , such as higher clinical stage , high psa values , multiple positive biopsies and in the case of invasion of the base of the prostate [ 35 ]  . 
pathology investigators showed that only the rst centimetre of sv ( starting from the base of the prostate ) seems to be essential , because only 6% of patients showed an invasion greater than 2 cm [ 37 ]  . 
it should be noted that the internal target volume ( itv ) of sv is more important than the prostate volume , with at least 810 mm of margins to be added in order to take into account sv movements , in the era of igrt [ 38 , 39 ]  . 
even though some retrospective studies [ 4042 ] cancro e quella della muscolatura pelvica [ 33 ]  . in conclusione , in base alla risoluzione spaziale dei sistemi pet ( circa 5 mm ) , la pet / ct con 11c - colina potrebbe essere utile per rilevare lesioni superiori a 5 millimetri allinterno della ghiandola prostatica , specialmente quando lacquisizione dinamica o quando le immagini sono acquisite sia in fase precoci che ritardata ( a doppia fase ) [ 34 ]  . correttamente , gli oncologi partecipanti a questa indagine non la ritengono uno strumento diagnostico indispensabile nella stadiazione dei casi clinici proposti : stata prescritta solo dal 5 , 5% di essi ( da sola o con mri ) nel caso di basso rischio clinico , e nel 14 , 9% di essi ( da sola o con mri ) nel caso ad alto rischio clinico , con solo il 4 , 7% dei radio - oncologi che la indicavano come unico esame da consigliare . volume da trattare , dosi e tecniche volumi i volumi da trattare in radioterapia nel cancro della prostata sono ancora dibattuti . 
in particolare , non ancora universalmente denito se le vescicole seminali ( sv ) e i linfonodi pelvici debbano essere compresi nel volume bersaglio clinico ( ctv ) dellirradiazione rispettivamente di tumori a basso rischio e a rischio intermedio - alto . 
tali controversie sono diventate sempre pi importanti in questa epoca di rt altamente conformazionale e di tecniche di radioterapia a intensit modulata . linltrazione delle sv chiaramente un fattore prognostico negativo e le sv dovrebbero essere comprese nel ctv quando emergono altri fattori prognostici negativi come uno stadio clinico avanzato , elevati valori di psa , molteplici biopsie positive e in caso di invasione della base della prostata [ 35 ]  . 
 in anatomia patologica , ricercatori hanno dimostrato che soltanto il primo centimetro di sv ( partendo dalla base della prostata ) sembra essere essenziale , perch solo il 6% dei pazienti ha mostrato uninvasione superiore a 2 cm [ 37 ]  . 
va notato che il volume bersaglio interno ( itv ) delle sv pi importante rispetto al volume della prostata , con almeno 810 mm di margini da aggiungere per tenere conto dei movimenti delle sv nellera della radioterapia guidata dalle immagini ( igrt ) [ 38 , 39 ]  . lirradiazione dei linfonodi pelvici rimane un elemento controverso in radioterapia in pazienti con rischio intermedio - alto di cancro alla prostata . 
anche se alcuni studi retrospettivi [ 4042 ] hanno dimostrato un vantaggio signicativo in termini di controllo biochimico per i pazienti che hanno un ct3 o un rischio > 15% ( stimato con la formula di roach [ 43 ] ) , altri studi retrospettivi e tutti e 3 gli studi prospettici randomizzati , in particolare , non hanno mostrato un signicativo vantaggio a favore della irradiazione pelvica [ 4446 ]  . 
deve essere notato che tutti e tre gli studi randomizzati presentano alcuni limiti che rendono questi studi radiol med ( 2013 ) 118 : 12201239 1233 showed a signicant advantage in terms of biochemical control for patients having a ct3 or a risk > 15% ( estimated with the roach formula [ 43 ] ) , other retrospective studies and all the three randomised studies specically aiming to establish the role of pelvic irradiation [ 4446 ] failed to show any signicant advantage in favour of pelvic irradiation . 
the trial 7706 of the radiation therapy oncology group ( rtog ) evaluated the interest of pelvic irradiation in low - risk prostate cancer patients ( stage a2 and b ) , having a low risk of pelvic micrometastases . 
the rtog 9413 study investigated in four arms patients with a pre - treatment psa < 100 ng / ml and a risk of pelvic nodal metastases > 15% ( estimated with the roach formula [ 39 ] )  . 
this study had quite a complicated 2x2 factorial design because it aimed to evaluate , on the same population , the value of neoadjuvant ht ( vs adjuvant ht ) and of pelvic irradiation . 
because of an unexpected positive interaction between neoadjuvant ht and pelvic irradiation , nally , the total number of patients is not statistically sufcient to correctly compare the four arms of the study and to draw denitive conclusions . 
finally , the french study group for urologic tumors ( groupe detude des tumeurs uro - gnitales , getug ) published the getug01 trial where the upper border of the pelvic irradiation elds was at s1 - s2 level , probably being too small , and only almost 50% of the patients presented a risk of pelvic micrometastases > 15% . 
at the same time , in this study , multifactiorial analysis showed that ht and nodal risk ( estimated with the roach formula [ 39 ] ) were the only prognostic factors . 
in consideration of these results , two approaches can be debated : only prostate irradiation , based on the negative results of randomised trials , vs prostate + nodal irradiation , based on the bias of these same studies and on the lack of evidence supporting irradiation of the prostate alone , as all the studies of concomitant rt - ht have been conducted by irradiating also nodal areas . it should be noted that the guidelines of the national comprehensive cancer network ( nccn ) conclude that ...patients with high - risk cancers are candidates for pelvic lymph node irradiation ( 7880 + gy ) and the addition of neoadjuvant / concomitant / adjuvant ht for a total of 23 years or 46 months in case of a single high risk adverse factor . 
patients with low - risk cancers should not receive either pelvic lymph node radiation or ht [ 47 ]  . in our survey , the radiation oncologists clearly showed that they shared these difculties in deciding for clinical case #1 ( high - risk patient ) : 60.2% stated they would treat prostate + / seminal vesicles , while 39.8% of them would also treat the nodal pelvic areas . 
il trial 77 - 06 del radiation therapy oncology group ( rtog ) ha valutato linteresse di unirradiazione pelvica in pazienti a basso rischio di cancro alla prostata ( stadio aua a2 e b ) , aventi un basso rischio di micrometastasi pelviche . 
lo studio rtog 9413 ha randomizzato in 4 bracci pazienti con un psa < 100 ng / ml pre - trattamento e il rischio di metastasi linfonodali pelviche > 15% ( stimato con la formula di roach [ 39 ] )  . 
questo studio era caratterizzato da un complicato disegno fattoriale 2x2 , perch valutava , sulla stessa popolazione , il ruolo della ht neoadiuvante ( vs ht adiuvante ) e dellirradiazione pelvica . 
a causa di uninterazione inaspettatamente positiva tra ht neoadiuvante e irradiazione pelvica , il numero totale di pazienti non stato statisticamente sufciente per confrontare correttamente i 4 bracci dello studio e quindi di trarre conclusioni denitive . 
inne , il gruppo francese per i tumori urologici ( groupe detude des tumeurs uro - gnitales , getug ) ha pubblicato lo studio getug01 , dove il margine superiore dei campi di irradiazione pelvica era posto al livello s1 - s2 , probabilmente troppo limitato , e solo circa il 50% dei pazienti presentava un rischio di micrometastasi pelviche > 15% . 
allo stesso tempo , in questo studio , lanalisi multifattoriale ha mostrato che lht e il rischio di invasione linfonodale ( stimato con la formula di roach [ 39 ] ) erano gli unici fattori prognostici . 
guardando a questi risultati , possono essere proposte due losoe : lirradiazione della sola prostata , sulla base dei risultati negativi di studi clinici randomizzati contro lirradiazione della prostata + pelvi , sulla base dei bias di questi stessi studi e sulla mancanza di prove che sostengono lirradiazione della sola prostata , poich tutti gli studi di rt - ht concomitante che sono stati condotti includevano lirradiazione delle aree linfonodali pelviche . va notato che le linee guida del national comprehensive cancer network ( nccn ) concludono che ... 
i pazienti con tumori ad alto rischio sono candidati allirradiazione dei linfonodi pelvici ( + 7880 gy ) e allaggiunta di ht neoadiuvante / concomitante / adiuvante per un totale di 23 anni o 6 mesi in caso di un unico fattore negativo di rischio elevato . 
i pazienti con tumori a basso rischio non dovrebbero ricevere lirradiazione pelvica linfonodale o lht [ 47 ]  . nella nostra indagine , i radio - oncologi hanno mostrato chiaramente di condividere queste difcolt nel prendere una decisione per il caso clinico #1 ( paziente ad alto rischio ) : il 60 , 2% ha dichiarato di essere in favore del trattamento della sola prostata + / vescicole seminali , mentre il 39 , 8% avrebbe irradiato anche le aree linfonodali pelviche . 
al contrario , solo l1% avrebbe trattato anche le aree linfonodali pelviche nel caso clinico #2 ( paziente a basso rischio )  . daltra parte , guardando la concomitanza con lht , i nostri risultati mostrano una buona aderenza degli oncologi radioterapisti italiani alle linee guida internazionali in merito alla prescrizione dellht : il 90 , 3% di loro non avrebbe 1234 radiol med ( 2013 ) 118 : 12201239 them would also treat the nodal pelvic areas in clinical case #2 ( low - risk patient )  . 
 on the other hand , looking at concurrent ht , our results show a good adherence of italian radiation oncologists to the international guidelines in prescribing ht : 90.3% of them would not deliver ht to the low - risk patient , while rt - ht would be the best treatment for the high - risk patient for 93.7% of them , with 82.8% prescribing long - term ht ( at least 12 months )  . 
 dose escalation has been allowed after the introduction of modern rt techniques , such as 3d - crt , imrt and , recently , volumetric modulated arc therapy ( vmat , rapidarc )  . 
results of randomised trials showed that increasing total dose is associated with improved biochemical outcomes , often in patients presenting higher initial psa levels ( > 1015 ng / ml ) [ 4852 ]  . 
recent analyses and reviews of tumour control in prostate cancer [ 5355 ] have suggested an alpha / beta value in the order of 1 to 3 gy for prostate cancer , which is somewhat lower than the value typically ascribed to the adjacent organs at risk ( oars ) , such as the urinary bladder and rectuif this is true , rt would offer a unique opportunity to improve the therapeutic ratio by adopting hypofractionated approach . the modern techniques of modulated and focused irradiation allow for a reduction of doses delivered to oars . 
 therefore it has been possible to study the efcacy and the toxicities of hypofractionated schedules : published studies show that hypofractionation is at least as effective as standard fractionation , without increasing the rate of acute and late toxicities [ 55 , 56 ]  . prescritto lht per il paziente a basso rischio , mentre la rt - ht sarebbe stata selezionata dal 93 , 7% come miglior trattamento per il paziente ad alto rischio , con l82 , 8% degli oncologi radioterapisti che avrebbe prescritto una ht a lungo termine ( almeno 12 mesi )  . limpatto della dose totale stato ampiamente dimostrato . 
 la dose escalation stata studiata dopo lintroduzione di moderne tecniche di rt , come la 3d - crt , limrt e , recentemente , la volumetric modulated arc therapy ( vmat , rapidarc , tomotherapy )  . 
i risultati di studi clinici randomizzati hanno mostrato che laumento della dose totale associato a migliori risultati biochimici , spesso in pazienti che presentano elevati livelli iniziali di psa ( > 1015 ng / ml ) [ 4852 ]  . 
una dose di 75 , 679 , 2 gy in frazioni da 1 , 8 gy alla prostata ( con o senza vescicole seminali ) appropriata per i pazienti con tumori a basso rischio . 
i pazienti a rischio intermedio e alto devono ricevere dosi comprese tra 75 , 6 e 81 , 0 gy [ 43 ]  . nella nostra indagine , gli oncologi radioterapisti hanno correttamente dichiarato di erogare almeno 70 gy : solo il 2 , 3% e il 5 , 5% di loro eroga dosi inferiori a 70 gy , rispettivamente , nel caso clinico 1 e 2 . dose / frazione diversi studi radiobiologici e clinici sembrano indicare che il cancro alla prostata abbia una particolare sensibilit alla dose / frazione . 
recenti analisi e recensioni sul controllo tumorale nel carcinoma della prostata [ 5355 ] hanno suggerito un alfa / beta da 1 a 3 gy per il cancro alla prostata , che moderatamente inferiore al valore in genere attribuito , per le tossicit tardive , agli organi a rischio adiacenti ( oar ) , come la vescica e il retto . 
se questo vero , la rt offrirebbe unopportunit unica per migliorare il rapporto terapeutico adottando lapproccio ipofrazionato . le moderne tecniche di imrt permettono una riduzione della dose somministrata agli organi a rischio . 
pertanto stato possibile studiare lefcacia e la tossicit degli schemi ipofrazionati : studi pubblicati dimostrano che lipofrazionamento almeno altrettanto efcace quanto il frazionamento standard , senza aumentare il tasso di tossicit acuta e tardiva [ 55 , 56 ]  . queste evidenze radiobiologiche e cliniche , assieme ad alcuni problemi organizzativi ( ad esempio liste dattesa e riduzione del numero di frazioni per paziente ) hanno favorito negli ultimi anni la diffusione degli schemi ipofrazionati nei radiol med ( 2013 ) 118 : 12201239 1235 this radiobiological and clinical evidence , together with some organisational issues ( i.e. , waiting lists , reduction of the number of fractions for the patients... ) has promoted the diffusion of hypofractionated schedules among italian radiotherapy departments . 
in our survey , hypofractionation was chosen by 29.132.4% of radiation oncologists , showing quite an important diffusion of this irradiation technique among italian radiation oncologists . irradiation technique : imrtigrt , brachytherapy imrt is now considered the standard of care in the treatment of prostate cancer [ 56 ]  . 
this highly conformal technique showed in different studies the possibility of reducing the rate of acute and late side effects , without affecting the efcacy of the treatment [ 50 ]  . 
it should be noted that imrt is not available in all italian radiotherapy departments , a fact that surely affected choices and the results of our survey . igrt is becoming more and more important in the treatment of cancer patients [ 57 ]  . 
the impact of these techniques in terms of tumour control and toxicities should be prospectively evaluated . in our survey , even if 46.856.7% of radiation oncologists controlled the setup of the patient by weekly electronic portal imaging ( epi ) , igrt by cb - ct was the standard of care for almost one third of radiotherapy departments . 
as for imrt , igrt is not available in all italian radiotherapy centres already , which may no doubt have affect choices and the results of our survey . interstitial brt delivers a localised , high dose ( 125145 gy ) of radiation to the prostate , with minimal exposure of the bladder , rectum , or other adjacent organs and tissues . 
indeed , brt is done as a single outpatient procedure and it seems to be associated with a lower rate of post - treatment incontinence than radical prostatectomy , and it has a lower cost . 
nella nostra indagine , lipofrazionamento stato scelto da 29 , 132 , 4% degli oncologi radioterapisti , mostrando una diffusione importante di queste tecniche di irradiazione tra i radio - oncologi italiani . tecnica di irradiazione : imrtigrt , brachiterapia limrt ormai considerata lo standard di cura nel trattamento del tumore alla prostata [ 56 ]  . 
questa tecnica altamente conformata ha mostrato in diversi studi la possibilit di ridurre il tasso di effetti collaterali acuti e tardivi , senza compromettere lefcacia del trattamento [ 50 ]  . 
nel nostro studio , stata la tecnica di scelta per il 52 , 1% e il 55 , 4% degli oncologi , rispettivamente per il caso clinico #1 e #2 . 
 va notato che limrt non disponibile in tutti i reparti di radioterapia italiani : ci potrebbe sicuramente aver inuenzato la scelta e i risultati del nostro studio . ligrt sta diventando sempre pi importante nel trattamento di pazienti affetti da cancro [ 57 ]  . 
limpatto di queste tecniche in termini di controllo tumorale e tossicit deve essere valutato prospetticamente . nella nostra indagine , anche se il 46 , 856 , 7% dei radiooncologi controllerebbe la congurazione del paziente con veriche portali settimanali ( epi ) , ligrt con cone beam ct lo standard di cura per quasi 1 / 3 dei dipartimenti di rt . 
come limrt , ligrt non ancora disponibile in tutti i centri di radioterapia italiani e ci potrebbe , ancora una volta , aver inuenzato la scelta e i risultati del nostro studio . la brt interstiziale eroga una dose elevata ( 125145 gy ) di radiazioni estremamente localizzata alla prostata , con esposizione minima della vescica , del retto o di altri organi e tessuti adiacenti . 
infatti , viene eseguita come procedura ambulatoriale unica e sembra essere associata a un tasso pi basso di incontinenza post - trattamento rispet to alla prostatectomia radicale , rispetto alla quale ha , inoltre , un costo inferiore . 
altri rari effetti collaterali possibili comprendono stenosi uretrale , incontinenza urinaria , ematuria ricorrente , sanguinamento rettale , procti te , e lo sviluppo di cancro alla vescica e di altri tumori secondari . uno dei possibili vantaggi principali della brt la possibilit di ridurre il rischio di disfunzione erettile , che stata riportata dal 30 al 35% degli uomini , 5 anni dopo la 1236 radiol med ( 2013 ) 118 : 12201239 cancer and other secondary cancers . 
one of the possible major advantages of brt is the possibility of reducing the risk of erectile dysfunction , which has been reported in 30 to 35% of men at 5 years after the procedure ( compared to more than 50% of surgical or ebrt treatments ) [ 60 ]  . 
one large long - term study reported an 8 - year biochemical recurrence rate of 18% in patients with low - risk cancer and 30% in patients with intermediate - risk cancer [ 61 ]  . 
the american brachytherapy society recently published its guidelines for hdr - brt for prostate cancer patients [ 62 ]  . procedura ( rispetto a oltre il 50% di trattamenti chirurgici o ebrt ) [ 60 ]  . nessuno studio clinico randomizzato controllato ha confrontato la brachiterapia con la prostatectomia radicale o la radioterapia a fasci esterni . 
un ampio studio a lungo termine ha riportato un tasso di recidiva biochimica del 18% a 8 anni nei pazienti con cancro a basso rischio e del 30% in pazienti con cancro a rischio intermedio [ 61 ]  . 
la qualit dellimpianto , cio lerogazione di oltre il 90% della dose di radiazione al volume target , un importante predittore di successo e pu dipendere sia dalla strumentazione disponibile che dallabilit delloperatore . 
la societ americana di brachiterapia ha recentemente pubblicato le sue linee guida per la hdr - brt per i pazienti affetti da tumore alla prostata [ 62 ]  . factors driving treatment choices fattori inuenzanti le scelte terapeutiche in our study , the factors inuencing treatment choices in the questionnaires were various and a clear absence of uniformity emerged from the data analysis : disease stage , alone ( 13.2% ) or associated with the literature data ( 10.2% ) or with age , and the published literature ( 11% ) were the most represented criteria in choosing treatment prescription and modalities for clinical case #1 , while none of the proposed criteria reached at least 10% of the preferences in the clinical case #2 . 
our data could therefore constitute an important base to consider the need for a multidisciplinary national consensus conference which summarizes the evidence and solving , if possible , controversies in the treatment of prostate cancer patients . globalmente , lindagine ha mostrato un elevato livello di consenso tra i radio - oncologi italiani nella prescrizione esclusiva di rt + / ht per i pazienti con cancro alla prostata . 
i nostri dati potrebbero essere probabilmente una base importante per considerare lopportunit di una consensus conference nazionale multidisciplinare per sottolineare e risolvere , se possibile , le controversie nel trattamento di pazienti affetti da cancro alla prostata . conict of interest all the authors declare that they have no conict of interest related to the publication of this article . 
all of the above is summarised in a concise key point box at the end of each section , enriched by a suggested reading list and pertinent , well reproduced images . due to the fact that this volume derives from daily practice , one will nd hospital jargon and acronyms that are sometimes impossible for outsiders to understand . 
apart from this , it will be appreciated and frequently used by all those working in this difcult and fascinating eld of radiology to obtain the best results for the patient . questo volume , in formato tascabile , con le sue 194 pagine rappresenta il quarto testo nella collana interventional radiology series , i cui altri titoli sono rappresentati da : handbook of angioplasty and stenting procedures ; transcatheter embolization and therapy ; interventional radiology techniques in ablation ( in via di pubblicazione )  . la collana ir ha come scopo di fornire ai radiologi interventisti ( sia esperti che tirocinanti ) informazioni sintetiche , veloci , immediate su ogni tipo di procedura con cui possano confrontarsi nella pratica quotidiana . come precisato nellintroduzione e nelle due prefazioni , il testo strutturato secondo quello che riconosciuto come formato a punta di proiettile con lo scopo di consentire un facile accesso allinformazione richiesta ( soprattutto gli editori si aspettano che il volume possa essere disponibile nelle sale di radiologia interventistica in modo di fornire risposte immediate alle domande e dubbi delloperatore )  . il volume in oggetto si occupa delle procedure bioptiche e di drenaggio , descrivendone caratteristiche ed indicazioni cliniche , valutazione diagnostica , anatomia , attrezzatura , medicinali , preparazione del paziente , modalit della procedura , assitenza post - procedurale e controllo delle complicanze . 
gli argomenti di cui sopra sono raccolti in una concisa tabella alla ne di ogni sezione , arricchita da un elenco di letture suggerite e da immagini pertinenti e ben riprodotte . dal momento che questo volume derivato dalla pratica quotidiana , costringer il lettore a confrontarsi con termini di gergo ospedaliero ed acronimi che sono spesso impossibili da interpretare per chi non vi avvezzo . 
malan 2 , 20097 san donato milanese , milan , italy 5radiology unit , university hospital , varese hospital , viale borri 57 , 21100 varese , italy 6medicine and health sciences unit , molise university , campobasso , italy 7medical sciences unit , cagliari university hospital , cagliari , italy 8thoracic surgery unit , university of parma , parma hospital , via gramsci 14 , 43100 parma , italy 9radiology unit , s . 
de filippo , unit operativa di scienze radiologiche , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 334 - 6896363 , fax : + 39 - 0521 - 703774 , e - mail : massimo.delippo@unipr.it received : 23 april 2012 / accepted : 6 august 2012 / published online : 25 july 2013 springer - verlag 2013 abstract purpose . 
from january 2007 to march 2010 , we retrospectively reviewed the ct images of 198 patients of both sexes ( 124 males and 74 females ; mean age , 70 years ; range age , 4490 ) used for the guidance of ttfna of pulmonary nodules . 
the most common negative predictive factor of ct - guided ttfna is the wrong position of the needle tip , as observed in the sagittal and axial oblique sections of the mpr reconstructions . 
per i noduli dei lobi superiori stata 84 , 2% , per quelli dei lobi inferiori 85 , 3% , per quelli della lingula e del lobo medio 90 , 9% . 
il ricorso alle immagini mpr sagittali e assiali oblique durante lagoaspirazione utile per il corretto planning della traiettoria dellago , questultimo aspetto cruciale che inuenza laccuratezza diagnostica della procedura . parole chiave nodulo polmonare ricostruzione multiplanare ago - biopsia trans - toracica biopsia tcguidata fattori diagnostici predittivi introduction introduzione computed tomography ( ct ) - guided trans - thoracic neneedle aspiration ( ttfna ) biopsy is currently considered a reliable diagnostic technique for the diagnosis of pulmonary nodules and masses , especially for malignant pulmonary lesions [ 14 ]  . 
several studies emphasise the overall accuracy of ct - guided ttfna in the characterisation of pulmonary lesions , which ranges from 74% to 95% , depending on nodule size , operator experience , and the type of statistical analysis used [ 1 , 513 ]  . 
in agreement with other authors , we believe that the diagnostic accuracy of ct - guided ttfna is comparable to that of histology in cases of malignancy , but lower in cases of benignity ( granuloma , parenchymal lymph node , hamartoma ) [ 14 , 15 ]  . 
the most frequent complications are pneumothorax and haemorrhagic suffusion ; the mortality rate is < 0.1% [ 2 , 5 , 1926 ]  . different types of needles with different calibre and lagobiopsia transtoracica con ago sottile ( ttfna ) guidata da tomograa computerizzata ( tc ) considerata una procedura afdabile per la diagnosi di natura dei noduli e delle masse polmonari , in particolare per le lesioni maligne [ 14 ]  . 
however , the smaller the needle , the lower the rate of complications and amount of blood contamination , and the greater the likelihood of obtaining a highly cellular sample . our primary objective was to evaluate factors predicting the diagnostic accuracy of ct - guided ttfna of solid noncalcied , subsolid and mixed pulmonary nodules and to analyse which factors are mainly responsible for false negative results , with a view to suggesting a method for their correction . 
 scopo dello studio stato individuare i fattori che predicono laccuratezza diagnostica dellagobiopsia transtoracica tc - guidata dei noduli polmonari solidi non calcici , subsolidi e misti ; identicare eventuali fattori responsabili di falsi negativi proponendo un metodo per la loro correzione . materials and methods study population we conducted a retrospective review of the noncontrastenhanced chest ct images of 198 patients ( 124 men and 74 women ; mean age , 70 years ; age range , 4490 ) who underwent ct - guided ttfna between january 2007 and june 2010 for pulmonary lesions suspicious for primary or secondary neoplasall patients underwent only one biopsy , regardless of the presence of more than one suspicious nodule . 
patients with lesions larger than 3 cm , or with mediastinal or chest wall lesions were excluded . biopsy procedure a multidetector ct helical scanner ( somatom emotion 6 , siemens , erlangen , germany ) was used , with the simultaneous acquisition of six slices per full rotation . 
patient position ( supine , prone , or lateral ) was decided on the basis of the location of the target lesion relative to the pleural ssures , large bronchi , vascular structures , and bones and distance from the chest wall , as shown on the previous ct scan . 
il decubito sul lettino ( supino , prono o laterale ) stato deciso sulla base della precedente indagine tc in funzione della posizione della lesione target rispetto a scissure pleuriche , grossi bronchi , strutture vascolari , ossa e distanza dalla parete toracica . 
in alcuni casi stata praticata anestesia locale con soluzione di lidocaina 1% . dopo aver introdotto un ago chiba point centimetrato da 22 g della lunghezza adeguata , stata effettuata una successiva scansione tc per vericare leffettiva localizzazione intralesionale della punta dellago , possibilmente nel contesto di tessuto solido non calcico . 
per aspirare il materiale biologico abbiamo collegato una siringa da 20 ml inserita su manico franzen . 1074 radiol med ( 2013 ) 118 : 10711081 appropriate length was introduced and a ct scan obtained to check the correct localisation of the needle tip within the lesion , possibly in the context of noncalcied solid tissue . 
 in 78 patients , open biopsy or surgical excision of the lung lesion was performed within 4 months of ct - guided ttfna , and so in these selected cases we were able to compare the results of histology and cytology . 
 image analysis all images of the procedures were saved in the hospitals picture archiving and communication system ( pacs ) and were reviewed separately by two radiologists ( mdf and mz ) with 11 years of experience each in thoracic radiology and ct - guided pulmonary biopsies . 
 statistical analysis the variables considered for statistical analysis were : the age and sex of the patient ; size ( 0.7 < x < 3 cm ) and density lidoneit o meno del materiale prelevato stata validata immediatamente al microscopio ottico dal citopatologo previo striscio su vetrino , immersione in alcol al 95% e colorazione con giemsa . 
 the overall diagnostic accuracy of the procedure for the nodules studied with ct - guided ttfna followed by surgical biopsy was expressed with the formula : true positive ( tp ) + true negative ( tn ) / tp + tn + false positive ( fp ) + false negative ( fn ) ; sensitivity as : tp / tp + fn ; specicity as : tn / tn + fp ; positive predictive value ( ppv ) as : tp / tp + fp ; and negative predictive value ( npv ) as : tn / tn + fn [ 28 ]  . 
among the remaining 42 cases ( 31.3% ) , in which no cancer cells were found , 21 samples contained red blood cells , 17 samples had inammatory cells ( mainly histiocytes ) , two samples contained cells and material compatible with tuberculosis , one sample was consistent with sarcoidosis and one with parietal cells of bronchogenic cysts . 
 open biopsy or tumour resection was performed in 78 cases ( 57.3% ) , and in particular in : 60 / 136 cases with neoplastic cytology ; 12 / 42 with non - neoplastic cytology ; 6 / 20 inadequate or insufcient samples . 
 among these 78 cases , we found 60 tp cases , two tn cases , 10 fn cases , no fp case , and six cases of inadequate or insufcient samples . 
 out of 42 nodules in patients who did not undergo surgery , 30 were retrospectively regarded as tn on the basis of the ct follow - up and clinical evolution . 
 of the 76 cases with neoplastic cellularity which did not undergo open biopsy , six were regarded as fp ( well - differentiated adenocarcinoma at cytology ) , since a reduction in nodule volume was observed on follow - up ct at 3 , 6 , 12 months so that no open biopsy was performed ; these patients were very elderly and had cardiopulmonary comorbidities . 
in 31 of these 76 cases , staging with positron emissione tomography ( pet ) and total - body ct showed nodal metastatic involvement which precluded surgery ; 13 died due to other causes , 16 refused open biopsy , 10 received treatment at other hospitals . veri positivi ( vp ) + veri negativi ( vn ) / vp + vn + falsi positivi ( fp ) + falsi negativi ( fn )  . 
abbiamo usato test statistici descrittivi per i dati nominali , come il chi - quadro di pearson . risultati sono risultate diagnostiche 178 su 198 ( 89 , 9% ) ago - biopsie di noduli polmonari di dimensioni comprese tra 7 e 30 m dei restanti 20 prelievi bioptici ( 10 , 1% ) , 8 erano inadeguati e 12 insufcienti . cellule neoplastiche sono state riscontrate in 136 dei 178 casi ( 76 , 4% del totale dei prelievi idonei ; 68 , 7% del totale dei noduli )  . 
dei restanti 42 casi ( 31 , 3% ) di prelievi ricchi di cellularit senza cellule neoplastiche : 21 contenevano globuli rossi , 17 cellule inammatorie ( prevalentemente istiociti ) , 2 cellule e materiale compatibili con infezione tubercolare , 1 era riconducibile a sarcoidosi e 1 a cellule parietali di cisti broncogena . 
 dei 136 casi in cui sono risultate al prelievo citologico cellule neoplastiche , la resezione o la biopsia chirurgica del nodulo stata eseguita in 78 casi ( 57 , 3% ) , in particolare : 60 pazienti operati su 136 con citologia neoplastica ; 12 pazienti operati su 42 con citologia non - neoplastica ; 6 pazienti operati su 20 campioni inadeguati o insufcienti . tra questi 78 casi abbiamo riscontrato 60 casi veri positivi ( pazienti risultati positivi per neoplasia alla ttfna e alla biopsia chirurgica ) , 2 casi veri negativi ( pazienti risultatti negativi alla ttfna , ma che nel dubbio clinico hanno eseguito la biopsia chirurgica , anchessa negativa ) , 10 casi falsi negativi ( pazienti risultati negativi alla ttfna , ma positivi alla biopsia chirurgica ) , nessun caso di falso positivo e 6 casi di campioni inadeguati o insufcienti . su 42 noduli non sottoposti ad intervento chirurgico : 30 sono stati retrospettivamente considerati come veri negativi ( sulla base del follow - up con tc e sullevoluzione clinica )  . dei 76 casi con cellularit neoplastica non sottoposti a biopsia chirurgica , 6 sono stati considerati falsi positivi ( adenocarcinoma ben differenziato alla citologia mediante prelievo tc ) in quanto era stata osservata una riduzione del volume del nodulo nel follow - up tc a 3 , 6 e12 mesi , per cui non stata eseguita la biopsia chirurgica ; tali pazienti erano molto anziani e presentavano gravi comorbilit cardiopneumologiche . 
 for nodules not in contact with the pleural plane , diagnostic accuracy was : 84.2% for a distance from 0 to 1 cm ; 86.6% for a distance from 1 to 2 cm ; 85.7% for a distance from 2 to 3 cm ; 77.7% for a distance over 3 c nel determinare il successo della procedure , calcolandone laccuaratezza diagnostica . 
per i noduli non in contatto con il piano pleurico , laccuratezza diagnostica stata : distanza da 0 a 10 mm : 84 , 2% ; distanza da 11 a 20 mm : 86 , 6% ; distanza da 21 a 30 mm : 85 , 7% ; distanza di oltre 30 mm : 77 , 7% . il valore dellanalisi statistica ( in relazione alla distanza del nodulo dal piano pleurico ) utilizzando il test chi quadrato di pearson stato p = 0 , 54 . in relazione alla sede anatomica del nodulo polmonare the result of the statistical analysis ( with respect to the distance between the nodule and the pleural surface ) using pearsons chi square test was p = 0.54. with regard to nodule location within the lung , diagnoslaccuratezza diagnostica stata : lobi polmonari superiori : 84 , 2% ; lobi polmonari inferiori : 85 , 3% ; lingula e lobo polmonare medio : 90 , 9% . tic accuracy was : 84.2% pulmonary upper lobes ; 85.3% pulmonary lower lobes ; 90.9% pulmonary lingula and middle lobes . 
altre complicanze son state la soffusione emorragica in 53 casi ( 26 , 8% ) e 2 casi di emottisi ; non si vericata alcuna complicanza maggiore . 1078 radiol med ( 2013 ) 118 : 10711081 ( 28.3% ) , none of whom required pleural drainage , haemorrhagic effusion in 53 cases ( 26.8% ) , and haemoptysis in two cases ; there were no major complications . 
 discussione discussion our retrospective analysis demonstrated that the overall diagnostic accuracy of ct - guided ttfna for pulmonary solid , mixed and subsolid nodules between 0.7 and 3 cm was 86% . 
where only small malignant lesions ( < 2 cm ) are considered , the accuracy of ct - guided ttfna has been reported to range from 51% to 84% [ 1 , 22 , 29 ]  . 
 the large variations in accuracy reported in the literature for pulmonary ct - guided ttfna is not only due to different sampling modalities , operator experience , nodule size , or presence of cytological assistance during the procedure , but also dependent on nodule density . 
in our experience , the accuracy of ct - guided ttfna for solid nodules from 0.7 to 3 cm was 95% , and 85% for solid nodules smaller than 2 c shimizu et al . 
the poor accuracy of ctguided ttfna for this type of lesion can be explained by low lesion cellularity which markedly impairs the sampling capacity of a ne needle [ 27 ]  . 
therefore it is reasonable to choose cutting needles rather than non - cutting ones when performing ct - guided biopsies to characterise the nature of ggo nodules [ 5 , 30 ]  . 
 [ 22 ] ( 96% ) ; in questi studi furono tuttavia incluse numerose lesioni polmonari di diametri maggiori di 3 cm che verosimilmente hanno contribuito ad incrementare laccuratezza diagnostica della procedura . 
laccuratezza insoddisfacente della ttfna tcguidata , per i noduli di ggo , potrebbe essere dovuta alla scarsa cellularit di tali lesioni , questultima ridurrebbe notevolmente la capacit di un ago sottile di prelevare il campione adeguato [ 27 ]  . 
sulla scorta di tali dati ragionevole preferire lutilizzo di aghi trancianti , nel corso dei prelievi bioptici tc - guidati per la diagnosi di natura dei noduli di ggo [ 5 , 30 ]  . 
abbiamo riscontrato tuttavia unaccuratezza leggermente inferiore per i noduli localizzati nei lobi superiori rispetto a quelli presenti nei lobi inferiori ( 83 , 3% vs 85 , 1% )  . 
si noti come le immagini mpr parasagittali e paracoronali ( b , c ) , eseguite retrospettivamente , dimostrino la punta dellago allesterno del nodulo ( frecce )  . ule distance from the pleura . 
this is somewhat counterintuitive , as upper lobe nodules move minimally during breathing compared to lower lobe ones . the presence of the shoulder blades and collar bones , overlapping the upper pulmonary lobe , may have a negative impact on the accuracy of ct - guided ttfna . 
multiple factors may be responsible for false negative results in ct - guided ttfna : extensive tumour necrosis , insufcient material ( inadequate sampling ) , operator inexperience , poor patient compliance , etc [ 3134 ]  . 
alla valutazione retrospettiva , limmagine mpr parasagittale ( b ) dimostra come la punta dellago sia allesterno del nodulo ( freccia )  . negatively affected the adequacy of the sample . 
in these cases the use of mpr reformats during the procedure could be useful to plan and verify in real time the best trajectory and inclination of the needle in the three spatial planes in order to improve the techniques ppv . in conclusion , the positive predictive factors of ct - guided ttfna of pulmonary nodules are correlated to nodule size ( the larger the diameter , the better the accuracy ) , noncalcic nodule density ( the higher the density , the better the accuracy ) , and distance between the nodule and the pleural plane ( the shorter the distance , the better the accuracy )  . the most common negative predictive factor of ctguided ttfna is the wrong placement of the needle tip , not appreciated in the native axial images but retrospectively observed on the sagittal and axial oblique mpr images . 
major complications , requiring additional corrective surgical procedure , occurred in three ( 7% ) patients ( one patient with prosthesis , one patient with tissue expander and one patient with deep inferior epigastric perforator ap )  . 
tra ottobre 2007 e novembre 2010 , presso il nostro dipartimento , 46 pazienti affette da neoplasia della mammella sono state sottoposte a trattamento radioterapico dopo intervento di mastectomia radicale e ricostruzione mammaria . 
a un follow - up mediano di 19 mesi , si osservata la comparsa di eritema cutaneo di grado 1 e 2 rispettivamente in 44 ( 96% ) e in 2 ( 4% ) pazienti . 
allanalisi univariata il fumo , la chemioterapia , il tamoxifene e la ricostruzione con protesi risultano associate a un maggior rischio di complicanze generali ( contrattura capsulare e fallimento della ricostruzione )  . 
sono necessari ulteriori studi per denire meglio la sequenza ottimale di trattamento tra ricostruzione mammaria e radioterapia . radiol med ( 2013 ) 118 : 12401250 1241 keywords breast cancer breast reconstruction postmastectomy radiation therapy parole chiave tumore della mammella ricostruzione mammaria radioterapia post - mastectomia . introduction introduzione post - mastectomy radiation therapy ( pmrt ) can improve survival and loco - regional control in patients with locally advanced breast cancer [ 13 ]  . 
in the past , postoperative radiotherapy ( rt ) was generally recommended only for selected patients with tumour - positive margins , locally advanced disease , or at least four positive lymph nodes [ 4 ]  . 
 more recently , several trials have shown the advantage of using post - mastectomy radiotherapy also in patients with stage ii tumours and less than four positive lymph nodes , thus increasing the number of patients receiving this treatment [ 5 ]  . 
many women wish to pursue immediate breast reconstruction ( ibr ) , whether or not they undergo postmastectomy radiotherapy , because it reduces the psychological and cosmetic impact of mastectomy [ 6 ]  . 
on the other hand , a recent meta - analysis showed that patients undergoing br and pmrt are more likely to suffer morbidity when compared to patients not receiving radiotherapy [ 8 ]  . 
several studies have evaluated the effect of pmrt on patients with breast reconstruction , and most of them report that postoperative radiotherapy can unfavourably affect the cosmetic outcome of breast reconstruction [ 11 , 12 ]  . 
the la radioterapia post - mastectomia ( pmrt ) consente un aumento della sopravvivenza e del controllo loco - regionale in pazienti con tumore della mammella localmente avanzato [ 13 ]  . 
negli anni passati , la radioterapia ( rt ) post - operatoria stata generalmente raccomandata solo in pazienti selezionate con presenza di margini chirurgici positivi , malattia localmente avanzata , o almeno 4 linfonodi positivi [ 4 ]  . 
pi recentemente , numerosi studi hanno mostrato un vantaggio nellutilizzo della radioterapia post - mastectomia anche in pazienti con tumori allo stadio ii e meno di 4 linfonodi positivi , portando cos a un aumento del numero di pazienti che ricevono questo trattamento [ 5 ]  . 
 molte donne desiderano sottoporsi a ricostruzione mammaria immediata ( ibr ) , indipendentemente dal fatto che effettueranno o meno trattamento radioterapico post - mastectomia , perch libr riduce limpatto psicologico e cosmetico della mastectomia [ 6 ]  . 
daltra parte , una meta - analisi recente ha mostrato che le pazienti che vengono sottoposte a ricostruzione mammaria ( br ) e pmrt andranno incontro con maggior probabilit a complicanze , in confronto a quelle che non ricevono radioterapia [ 8 ]  . 
di conseguenza , il ruolo della pmrt nella gestione generale delle pazienti che effettuano la ricostruzione immediata rappresenta una sda per i medici . due sono le tecniche di ricostruzione utilizzate di frequente . 
nella seconda tecnica si posiziona , a livello retro pettorale , un espansore temporaneo che successivamente viene sostituito da un impianto permanente dopo il trattamento [ 9 , 10 ]  . 
 numerosi studi hanno valutato leffetto della pmrt sulle pazienti con ricostruzione mammaria : secondo la maggior parte di essi , la radioterapia post - operatoria pu inuenzare in maniera negativa il risultato cosmetico della ricostruzione stessa [ 11 , 12 ]  . 
di conseguenza , il timing ottimale della ricostruzione mammaria dopo mastectomia in pazienti che necessitano di trattamento radioterapico rimane ancora una questione controversa . nel presente studio abbiamo valutato la nostra esperienza in pazienti che hanno ricevuto radioterapia post - mastectomia dopo ricostruzione mammaria . 
a total of 43 patients with locally advanced disease were treated : four patients ( 9% ) with stage iia , 19 patients ( 41% ) with stage iiia , two patients ( 4% ) with stage iiib , 18 patients ( 39% ) with stage iiic and three patients with recurrent disease . surgeons of the plastic surgery and breast surgery units of our institution or other institutions performed the mastectomy and breast reconstruction . 
 the latissimus dorsi ap is made up of skin , fat , muscle , and blood vessels from the upper back and is placed under the skin of the chest . 
an implant was placed beneath the ap in some cases to provide adequate bulk for the breast recontra ottobre 2007 e novembre 2010 , presso il nostro dipartimento , 46 pazienti affette da neoplasia della mammella sono state sottoposte a trattamento radioterapico , dopo intervento di mastectomia radicale e ricostruzione mammaria . 
 su un totale di 46 pazienti , 4 pazienti ( 9% ) presentavano malattia allo stadio iia , 19 pazienti ( 41% ) stadio iiia , 2 pazienti ( 4% ) stadio iiib , 18 pazienti ( 39% ) stadio iiic e 3 pazienti malattia recidivante . la mastectomia e la ricostruzione mammaria sono state eseguite da chirurghi dellunit di chirurgia plastica e di chirurgia senologica presso il nostro o altri istituti . 
the skin , fat , blood vessels , and at least one abdominal muscle were cut from the abdomen and connected to the blood vessels in the chest through microsurgery techniques . 
the expander is a saline - lled envelope to which saline can be added through a valve at regular intervals to ll it over time ( about 4 to 6 months )  . 
some expanders are left in place as the nal implant . the types of reconstruction used in our patients were as follows : diep ap in 13 patients ( 28% ) ; latissimus dorsi muscle ap without prosthesis in four patients ( 9% ) ; latissimus dorsi muscle ap plus prosthesis in 10 patients ( 22% ) ; permanent prosthesis in eight patients ( 17% ) ; tissue expander in 11 patients ( 24% )  . after the breast reconstruction , all patients were treated with external beam radiotherapy to the chest wall using tangential elds . 
the dose was delivered in accordance with recommendations of the icru report 62 of target coverage of at least 95% and not more than 107% of the prescription dose in order to minimise the dose to the organs at risk ( oars ) ( table 2 )  . the median time from br to radiotherapy was 6 months 1243 diata stata eseguita allo stesso tempo della mastectomia . 
 dopo la rimozione del tessuto mammario , il chirurgo ha posizionato un impianto costituito da una protesi riempita di soluzione siologica o gel di silicone o da un tessuto autologo . 
la cute , il grasso , i vasi sanguigni e almeno uno dei muscoli addominali sono stati tagliati dalladdome e collegati ai vasi sanguigni nel torace attraverso tecniche di microchirurgia . 
alcuni espansori vengono lasciati in sede come impianto denitivo . per le nostre pazienti sono state utilizzate diverse tecniche di ricostruzione mammaria come segue : lembo diep in 13 pazienti ( 28% ) ; lembo gran dorsale senza protesi in 4 pazienti ( 9% ) ; lembo gran dorsale con protesi in 10 pazienti ( 22% ) ; protesi permanente in 8 pazienti ( 17% ) ; espansore tissutale in 11 pazienti ( 24% )  . dopo la ricostruzione mammaria tutte le pazienti sono state trattate con radioterapia a fasci esterni sulla parete toracica , utilizzando campi tangenziali . 
 la dose stata somministrata in accordo con le raccomandazioni del report 62 icru , che prevedono una copertura del target di almeno il 95% e di non pi del 107% della prescrizione di dose in modo da ridurre la dose agli organi a rischio ( tabella 2 )  . lintervallo di tempo mediano tra la ricostruzione e la rt stato di 6 mesi ( range 29 ) per le pazienti che hanno ricevuto chemioterapia adiuvante e 4 mesi ( range 17 ) per quelle che non sono state sottoposte a chemioterapia . 
tre pazienti sono state trattate a causa di recidiva rispettivamente a 7 , 22 mesi e 9 anni dopo la ricostruzione mammaria . tra le 46 pazienti , 3 ( 6% ) sono state sottoposte a chemioterapia neo - adiuvante , 24 ( 53% ) a chemioterapia neoiii iii 1244 table 3 bakers classication grade baker score implant shell not palpable and not visible implant shell slightly rm but not visible implant shell clearly rm and visible implant shell very rm , implant dislocation and deformation , pain tabella 3 classicazione di baker grado classicazione di baker impianto protesico non palpabile e non visibile impianto protesico lievemente indurito , palpabile ma non visibile impianto protesico indurito con iniziale alterazione della forma , poco mobile , palpabile e visibile impianto protesico di consistenza dura con distorsione marcata della morfologia , dolente e dolorabile ( range , 29 ) for patients who received adjuvant chemotherapy and 4 months ( range , 17 ) for the ones who did not receive chemotherapy . 
three patients were treated due to recurrence 7 , 22 months and 9 years after breast reconstruction , respectively . among the 46 patients , three patients ( 6% ) were treated with neo - adjuvant chemotherapy , 24 ( 53% ) with neo - adjuvant and adjuvant chemotherapy , 16 ( 35% ) with adjuvant chemotherapy and three ( 6% ) did not receive chemotherapy . 
twenty - seven patients ( 59% ) were treated with adjuvant hormonal therapy . the objective of this analysis was to evaluate the outcomes , complications and patients satisfaction after pmrt . 
complications associated with implants included capsular contracture , rupture , extrusion , malposition , and removal because of pa capsular contracture was graded according to bakers classication ( table 3 ) [ 14 ]  . 
adverse side effects related to radiotherapy were scored according to the classication of the radiation therapy oncology group / european organisation for research and treatment of cancer ( rtog / eortc ) [ 15 ]  . 
ventisette pazienti ( 59% ) sono state trattate con terapia ormonale adiuvante . lobiettivo di questa analisi stato quello di valutare i risultati , le complicanze e il grado di soddisfazione delle pazienti dopo il trattamento radioterapico . 
gli eventi avversi correlati al trattamento radioterapico sono stati classicati in accordo con la classicazione del radiation therapy oncology group / european organisation for research and treatment of cancer ( rtog / eortc ) [ 15 ]  . 
 stata eseguita unanalisi univariata per vericare linuenza dei fattori contrattura capsulare e fallimento della ricostruzione sulle complicanze generali : stadio t ( t1 - t2 vs t3 - t4 ) , stato n ( n - positivo vs n - negativo ) , terapia ormonale adiuvante con tamoxifene ( si / no ) , chemioterapia ( si / no ) , tipo di ricostruzione ( lembo / impianto ) e fumo ( si / no )  . 
un p value inferiore a 0 , 05 stato considerato come statisticamente signicativo . risultati tra ottobre 2007 e novembre 2010 , 46 pazienti con ricostruzione mammaria post - mastectomia sono state sottoposte a trattamento radioterapico . 
le visite di follow - up sono state eseguite ogni 3 mesi durante il primo anno e poi ogni 6 mesi , e comprendevano un esame sico della parete toracica e dei linfonodi regionali . 
follow - up examinations were performed every 3 months during the rst year and then every 6 months , and included physical examination of the chest wall and regional lymph nodes . 
at the time of this analysis , two patients ( 4% ) had died due to metastatic disease ( table 4 )  . immediately after the end of radiotherapy , a skin erythema grade 1 and 2 was seen in 44 ( 96% ) and two ( 4% ) patients , respectively . 
additional corrective surgical procedure was performed in these three patients 12 months after radiotherapy . among the 29 patients with prosthesis or tissue expander , ve ( 17% ) had no signs of capsular contracture , 19 ( 65% ) had a baker type ii contracture , three ( 11% ) a baker type iii contracture and two ( 7% ) a baker type iv contracture . on univariate analysis , smoking ( p = 0.001 ) , chemotherapy ( p = 0.001 ) , tamoxifen ( p = 0.001 ) and reconstruction with immediatamente dopo il termine della radioterapia , stata osservata la comparsa di eritema cutaneo di grado 1 e 2 rispettivamente in 44 ( 96% ) e 2 pazienti ( 4% )  . 
due pazienti hanno riferito comparsa di dolore loco - regionale . le complicanze maggiori sono state riscontrate solo in 3 pazienti ( 7% ) ( 1 paziente con protesi , 1 con espansore tissutale e 1 con lembo diep )  . 
in queste 3 pazienti stata necessaria unulteriore procedura chirurgica correttiva 12 mesi dopo la radioterapia . tra le 29 pazienti con protesi o espansore tissutale , 5 ( 17% ) non presentavano segni di contrattura capsulare , 19 ( 65% ) manifestavano contrattura di tipo baker ii , 3 ( 11% ) contrattura di tipo baker iii e 2 ( 7% ) presentavano contrattura di tipo baker iv . allanalisi univariata il fumo ( p = 0 , 001 ) , la chemioterapia ( p = 0 , 001 ) , la terapia ormonale con tamoxifene ( p = 0 , 001 ) e la ricostruzione con impianto protesico ( p = 0 , 001 ) sono stati identicati come fattori prognostici signicativi per la comparsa di complicanze . 
tutti i valori di p dellanalisi univariata sono riportati in tabella 5 . tra le 46 pazienti irradiate , 40 ( 86% ) sono state molto soddisfatte o soddisfatte del risultato cosmetico della ricostruzione e hanno valutato il risultato estetico complessivo come buono / eccellente . 
le restanti 6 pazienti hanno denito il risultato estetico come scarso / insufciente . discussione attualmente presso la nostra istituzione l85% delle pazienti viene sottoposto a ricostruzione al tempo stesso della mastectomia . 
all p values from univariate analysis are reported in table 5 . among the 46 irradiated patients , 40 ( 86% ) were very satised or satised with the cosmetic outcome of the reconstruction and evaluated the cosmetic results as good / excellent . 
il tasso di complicanze maggiori stato basso : solo 3 pazienti hanno richiesto unulteriore procedura chirurgica correttiva a causa di contrattura capsulare ( baker iii - iv ) e fallimento della ricostruzione . 
 [ 16 ] che hanno riportato complicanze maggiori , che hanno richiesto radiol med ( 2013 ) 118 : 12401250 discussion at our institution , 85% of patients currently undergo reconstruction at the time of mastectomy . 
the rate of major complications was low , with only three patients requiring an additional corrective surgical procedure because of capsular contracture ( baker type iii - iv )  . 
 [ 16 ] who reported major complications , requiring implant removal , in only 3 / 74 patients who underwent breast reconstruction with a tissue expander / implant or permanent implant followed by pmrt . 
 [ 17 ] reported that 68% of the irradiated patients with tissue expander / implant breast reconstruction developed capsular contracture , compared with 40% of the non - irradiated group . 
in our study , 40 patients ( 86% ) were satised with cosmetic outcome and six ( 14% ) were not , with three of these patients requiring an additional corrective surgical procedure . the question is not only that radiation therapy can affect the cosmetic outcome and increase postoperative complications , but also that immediate breast reconstruction itself 1247 rimozione dellimpianto , solo in 3 su 74 pazienti sottoposte a ricostruzione mammaria con un espansore tissutale / impianto o impianto permanente seguito da pmrt . 
 [ 17 ] hanno rilevato che il 68% delle pazienti irradiate con ricostruzione mammaria con espansore tissutale / impianto hanno sviluppato contrattura capsulare in confronto al 40% del gruppo non irradiato . 
 [ 20 ] hanno riportato simili livelli di soddisfazione generale in donne sottoposte a ricostruzione mammaria immediata o ritardata seguita da radioterapia , nonostante la maggior parte delle pazienti avrebbe preferito la ricostruzione immediata . 
nel nostro studio , 40 pazienti ( 86% ) sono state soddisfatte del risultato cosmetico e 6 ( 14% ) sono risultate insoddisfatte ; 3 di queste hanno dovuto sottoporsi a unulteriore procedura chirurgica correttiva . la questione non solo il fatto che la radioterapia pu inuenzare il risultato cosmetico e aumentare le complicanze post - operatorie , ma anche che la ricostruzione mammaria immediata stessa pu alterare la somministrazione e lefcacia della radioterapia . 
 [ 21 ] hanno valutato in maniera retrospettiva limpatto della ibr sulla pianicazione del trattamento radioterapico e hanno trovato che il piano di trattamento radioterapico dopo ricostruzione mammaria immediata era compromesso in pi della met delle pazienti ( 52% ) , se confrontato col 7% delle pazienti che erano state sottoposte a mastectomia senza ricostruzione . 
una soluzione potenziale , anche in termini di riduzione del tasso di incidenza di complicanze generali , potrebbe essere la ricostruzione mammaria immediata / ritardata [ 22 ] con lutilizzo di un espansore tissutale posizionato dopo la mastectomia skin - sparing e sostituito da protesi permanente quando i risultati istologici sono dis1248 radiol med ( 2013 ) 118 : 12401250 can impair the delivery and efcacy of radiotherapy . 
 [ 21 ] evaluated retrospectively the impact of ibr on the technical delivery of pmrt and found that radiationtreatment planning after ibr was compromised in more than half of the patients ( 52% ) , compared with 7% of patients who had undergone mastectomy without reconstruction . 
a potential solution , also in terms of rate of overall complications , could be provided by delayed - immediate breast reconstruction [ 22 ] with the use of a tissue expander placed after skin - sparing mastectomy and replaced by permanent implant when the denitive pathological results are available and a decision on the need for radiotherapy is taken . 
 [ 16 ] , no signicant difference in the overall rate of major or minor complications was found between patients who underwent breast reconstruction with a tissue expander / implant or permanent implant followed by pmrt . 
the capsular contracture rate was similar in the two groups and signicantly higher compared to non - irradiated patients . another issue still a matter of debate is the timing of ibr and administration of chemotherapy . 
 [ 24 ] performed a retrospective analysis of 595 patients with breast cancer treated with or without ibr and adjuvant chemotherapy and found that ibr delayed the initiation of adjuvant chemotherapy but did not lead to omission or signicant clinical delay ( more than 12 weeks ) in chemotherapy . 
 in our study , ibr did not lead to signicant clinical delay in adjuvant chemotherapy in any of our patients . the association between complication rates and risk factors was examined by several studies . 
 [ 25 ] , in a retrospective review of 1037 patients who underwent mastectomy plus autologous tissue or expander / implant reconstruction , found that radiation therapy was the greatest risk factor for major complications in tissue expander / implant reconstruction . 
in addition , a body mass index ( bmi ) > 30 was found to be a signicant risk factor for total complications , while no association was found with smoking , age , chemotherapy , diabetes or hypertension . 
our results further support performing immediate autologous reconstruction followed by pmrt , as the rate of complications is acceptably low and a secondary ap reponibili e sia stata presa una decisione sulla necessit del trattamento radioterapico . 
 [ 16 ] non stata trovata alcuna differenza signicativa nel tasso complessivo di complicanze maggiori o minori tra le pazienti sottoposte a ricostruzione con espansore o protesi permanente dopo pmrt . 
 [ 23 ] hanno riferito che il tasso di fallimento della ricostruzione era signicativamente pi alto ( 40% ) nelle pazienti con espansore rispetto alle pazienti con protesi permanente ( 6 , 4% )  . 
il tasso di contrattura capsulare era simile nei 2 gruppi e signicativamente pi alto se confrontato con le pazienti non irradiate . unaltra questione che ancora materia di dibattito il timing della ibr e della somministrazione della chemioterapia . 
hanno effettuato unanalisi retrospettiva su 595 pazienti con tumore della mammella trattate con o senza ibr e chemioterapia adiuvante e hanno trovato che libr ha ritardato linizio della chemioterapia adiuvante ma non ha portato alla sua omissione o a un ritardo clinico signicativo ( pi di 12 settimane )  . 
 nel nostro studio , libr non ha portato in alcun caso a un ritardo clinico signicativo nellinizio della chemioterapia adiuvante . lassociazione tra tasso di complicanze e fattori di rischio stata esaminata da numerosi studi . 
 [ 25 ] in unanalisi retrospettiva di 1037 pazienti sottoposte a mastectomia e ricostruzione con tessuto autologo o espansore / impianto hanno dimostrato che la radioterapia era il principale fattore di rischio per complicanze maggiori nel caso della ricostruzione con espansore / impianto . 
con il trattamento radiante , il 58 , 8% delle pazienti ha presentato complicanze maggiori e minori , mentre solo il 27 , 6% di quelle non irradiate ha presentato complicanze . 
inoltre , un indice di massa corporea ( bmi ) > 30 risultato essere un fattore di rischio signicativo per complicanze generali , mentre non stata trovata alcuna associazione col fumo , let , la chemioterapia , il diabete e lipertensione . 
i nostri risultati supportano ulteriormente lesecuzione della ricostruzione autologa immediata seguita dalla pmrt , in quanto il tasso di complicanze risultato accettabile e nel nostro caso stato necessario un intervento correttivo solo in una paziente con lembo autologo . 
 [ 26 ] hanno valutato i fattori associati al fallimento della ricostruzione e alla contrattura capsulare in 141 pazienradiol med ( 2013 ) 118 : 12401250 1249 construction was necessary in only one patient with autologous ap . 
 [ 26 ] evaluated the factors associated with reconstruction failure and capsular contracture in 141 patients who underwent mastectomy and ibr with a tissue expander and implant followed by rt . 
univariate analysis showed that tumour size t3 or t4 , smoking and positive axillary nodes were the main factors associated with reconstruction failure , whereas the surgeon , hormonal therapy and smoking were associated with baker iii and iv capsular contracture . 
in our study , univariate analysis showed smoking , chemotherapy , tamoxifen and reconstruction with implant to be signicantly associated with overall complications ( capsular contracture and reconstruction failure )  . 
no other factors , including tumour size and node status , had any impact on the complication rate . in conclusion , within the limitation of a retrospective review with a small number of patients , our study demonstrates that pmrt can be delivered safely to patients after breast reconstruction , with very low rates of complications . 
more prospective studies with longer follow - up periods are needed to denitively establish the optimum sequencing of breast reconstruction and pmrt . ti sottoposte a mastectomia e ibr con un espansore tissutale e impianto seguiti da rt . 
le pazienti che avevano ricevuto il tamoxifene entro 28 giorni prima della ricostruzione mammaria presentavano un aumentato rischio di complicanze vascolari del lembo in confronto alle pazienti che non avevano ricevuto il trattamento . nel nostro studio , allanalisi univariata il fumo , la chemioterapia , il tamoxifene e la ricostruzione con protesi risultano associate in maniera signicativa a un maggior rischio di complicanze ( contrattura capsulare e fallimento della ricostruzione )  . in conclusione , pur con i limiti propri di uno studio retrospettivo e con un esiguo numero di pazienti , il nostro lavoro dimostra che la radioterapia post - mastectomia pu essere somministrata alle pazienti dopo ricostruzione mammaria in maniera sicura con un tasso di complicanze molto basso . 
 sono necessari ulteriori studi prospettici con follow - up di durata maggiore per stabilire denitivamente la sequenza ottimale della ricostruzione mammaria e della pmrt . acknowledgments the authors thank stefano bracci for his assistance with statistics ringraziamenti gli autori ringraziano stefano bracci per lassistenza nellanalisi statistica . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
of the 41 nonmalignant lesions , 35 underwent follow - up breast mr imaging ( mean , 2619 months ) , which demonstrated no lesions changes ; six lesions underwent surgery because of poor radiologicalpathological correlation ; of these 6 lesions , 3 were nonmalignant , one was borderline ( lobular carcinoma in situ ) and two were malignant ( well - differentiated tubular carcinoma and inltrating ductal carcinoma )  . 
delle 41 lesioni non maligne , 35 sono state sottoposte a mri mammaria di follow - up ( media 2619 mesi ) , che non ha dimostrato modicazioni delle lesioni stesse ; 6 lesioni sono andate incontro a intervento chirurgico a causa della insufciente correlazione radiologica - patologica e sono risultate essere non maligne in 3 casi , bordeline in 1 caso ( carcinoma lobulare in situ ) e maligne in 2 casi ( carcinoma tubulare ben differenziato e carcinoma duttale inltrante )  . 
sensibilit , specicit , valori predittivi positive e negativo , accuratezza diagnostica sono risultati essere , rispettivamente , 93 , 5% , 100% , 100% , 95 , 1% e 97 , 1% considerando il carcinoma lobulare in situ un risultato 1138 radiol med ( 2013 ) 118 : 11371148 conclusions . 
la mrbb con un sistema coassiale ferromagnetico - amagnetico ha rappresentato un modo semplice per eseguire una procedura bioptica ed stata facilmente applicabile nella routine clinica . parole chiave risonanza magnetica mammaria lesione mammaria biopsia mammaria ago coassiale follow - up introduction introduzione breast magnetic resonance ( mr ) imaging can detect lesions that are not identied with other techniques , such as mammography or second - look ultrasonography ( us ) [ 13 ]  . 
some authors reported their experience with fully mr - compatible [ 4 ] and vacuum - assisted breast biopsy ( vabb ) systems [ 511 ] , which have unquestionable advantages but bear some problems , such as high costs and low availability . 
 [ 12 ] presented their clinical experience with 14 - gauge stainless steel core biopsy needles and concluded that their technique was safe and effective for mrbb , with limited costs . 
however , the authors stated that the main limitation of the study was the insufcient followup of nonmalignant biopsies . the aim of this paper is to describe our clinical experience with a widely available and easy to use mrbb system consisting of a nonmagnetic coaxial needle and a ferromagnetic 14 - , 16or 18 - gauge core biopsy needle for suspicious mr - only lesions . 
in the same period , 333 suspicious mr - detected lesions underwent second - look us , which was positive in 263 cases ( 79% ) ; 70 of 333 ( 21% ) were mr - only lesions , which underwent mrbb . 
in 4 / 66 patients , mrbb was performed on limaging di risonanza magnetica ( mri ) mammaria pu evidenziare lesioni non identicate con altre metodiche , come la mammograa o lecograa second look [ 13 ]  . 
alcuni autori hanno riportato la loro esperienza con sistemi di biopsia mammaria completamente mri - compatibili [ 4 ] e vacuum - assisted ( vabb ) [ 511 ] , i quali hanno indiscutibili vantaggi ma recano alcuni problemi , come gli alti costi e la scarsa disponibilit . 
tuttavia , gli autori hanno dichiarato che la maggiore limitazione del loro studio era linsufciente follow - up sulle biopsie non maligne . lo scopo del lavoro stato quello di descrivere la nostra esperienza clinica con un sistema di mrbb largamente disponibile e di facile utilizzo , consistente in un ago coassiale amagnetico e un ago ferromagnetico per core biopsy da 14 , 16 or 18 g da utilizzare su lesioni sospette mri - only . 
nel medesimo periodo , 333 lesioni identicate dalla mri sono state sottoposte a ecograa second look , la quale risultata positiva in 263 casi ( 79% ) ; 70 su 333 radiol med ( 2013 ) 118 : 11371148 1139 two lesions , in three cases during the same session and in one case 61 months after the rst procedure ( in 2002 and in 2007 )  . 
twenty - four of the 66 women ( 36.4% ) underwent mr imaging because of equivocal or discordant ndings at mammography and / or us , 17 ( 25.7% ) for follow - up after personal history of breast cancer , 15 ( 22.7% ) for familial / genetic risk of breast cancer , six ( 9.1% ) because they were diagnosed with carcinoma of unknown primary ( cup ) syndrome and the remaining four ( 6.1% ) for evaluation of disease extent in recently diagnosed breast cancer . 
 equipment and procedures the mrbb procedure was performed as described in previous papers [ 13 , 14 ] using a 1.5 - t magnet ( gyroscan intera master , philips medical systems , best , the netherlands ) with a dedicated localization device ( stereotactic localization device for gyroscan systems , philips medical systems , best , the netherlands )  . 
briey , the equipment consisted of a support allowing patient positioning in a semiprone position ( 20 tilt ) and a breast compression device consisting of two plates ( medial and lateral )  . 
 after patient positioning , a coronal dynamic t1 - weighted study was performed , with intravenous injection of 0.1 mmol / kg gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa ) ( magnevist , bayer schering pharma ag , berlin , germany )  . 
after identifying the enhancing lesion , the marker tubes made it possible to obtain its spatial coordinates and to select the best hole in the compression plate through which the needles would be inserted later . 
after another t1 - weighted sequence with a needle phantom in the selected hole to check the lesion coordinates ( the phantom should point exactly to the lesion ) , local anaesthesia with lidocaine was performed ( lidocaina cloridrato 2% , salf spa , italy ) , and the coaxial needle was inserted in the breast . 
the coaxial needles used in this study were lowartefact 12 - , 14or 16 - gauge devices ( sterylab , italy ; vigeo , italy ; daum , germany ; invivo , usa )  . 
due to the nonmagnetic nature of the devices , only a small susceptibility artefact was visible on the t1 - weighted sequence implemented to verify that the coaxial needle was in the correct position ( beside the lesion with the tip directed towards the lesion but not entering the lesion itself )  . 
finally , the biopsy procedure was performed outside the magnet bore with stainless steel 14 - , 16or 18 - gauge semiautomatic or automatic core bi ( 21% ) erano lesioni mri - only che sono state sottoposte a mrbb . sessantasei pazienti di sesso femminile ( et 49 , 58 , 8 anni , range 3173 anni ) sono state sottoposte a mrbb dopo aver rmato un consenso informato . 
in 4 delle 66 pazienti , la mrbb stata eseguita su 2 lesioni , in 3 casi nella stessa sessione , in 1 caso 61 mesi dopo la prima procedura ( nel 2002 e nel 2007 )  . 
ventiquattro dei 66 soggetti ( 36 , 4% ) sono stati sottoposti a mri per reperti equivoci o discordanti alla mammograa e / o ecograa , 17 ( 25 , 7% ) per follow - up dopo storia personale di carcinoma mammario , 15 ( 22 , 7% ) per rischio genetico / familiare di carcinoma mammario , 6 ( 9 , 1% ) poich avevano ricevuto la diagnosi di carcinoma of unknown primary ( cup ) syndrome , e i rimanenti 4 ( 6 , 1% ) soggetti per valutazione dellestensione di malattia in carcinoma mammario di recente diagnosi . attrezzatura e procedure la procedura di mrbb stata eseguita come precedentemente descritto in altri articoli [ 13 , 14 ] su un magnete a 1 , 5 t ( gyroscan intera master , philips medical systems , best , olanda ) con un device dedicato per la localizzazione ( stereotactic localization device for gyroscan systems , philips medical systems , best , olanda )  . 
brevemente , lattrezzatura consistita in un supporto che ha permesso di posizionare la paziente in posizione semiprona ( 20 gradi di inclinazione ) , e di un device per la compressione della mammella , consistente in due piastre ( mediale e laterale )  . 
 dopo il posizionamento della paziente , stato eseguito uno studio dinamico t1 - pesato coronale , con infusione endovenosa di 0 , 1 mmol / kg di gd - dtpa ( magnevist , bayer schering pharma ag , berlino , germania )  . 
dopo lidenticazione della lesione , i tubi marcatori hanno permesso di ottenere le sue coordinate nello spazio e di scegliere il miglior foro della piastra di compressione attraverso la quale sarebbero poi stati inseriti gli aghi . 
d aspetto dellago fantoccio ( iperintenso in questa immagine coronale t1 pesata ) dopo il suo posizionamento in un foro della piastra di compressione . opsy needles ( sterylab , italy ; vigeo , italy ; daum , germany ; invivo , usa ) passing through the coaxial needle . 
in ve cases ( 7.1% ) , a marker clip was positioned in the biopsy site ( gelmark , senorx , inc . , irvine , ca , usa )  . 
the entire mrbb procedure , from patient positioning to the last t1 - weighted sequence , took approximately 45 min ; we did not perform a thorough evaluation of times . 
 gli aghi coassiali usati nel presente studio sono stati device caratterizzati da bassi artefatti da 12 , 14 o 16 g ( sterylab , italia ; vigeo , italia ; daum , germania ; invivo , usa )  . 
 grazie alla natura amagnetica dei device , nella sequenza t1 - pesata eseguita per vericare che lago coassiale fosse nella corretta posizione ( adiacente alla lesione con la punta diretta verso la stessa , senza entrare nella lesione ) , solo lievi artefatti da suscettibilit erano visibili . 
inne , la procedura bioptica stata eseguita al di fuori del magnete , con aghi da core biopsy semiautomatici o automatici di acciaio inossidabile ( sterylab , italia ; vigeo , italia ; daum , germania ; invivo , usa ) , passando attraverso lago coassiale . 
 nel caso di una lesione vicina alla piastra di compressione perforata ( 5 su 70 lesioni , 7 , 1% ) , la mrbb stata eseguita radiol med ( 2013 ) 118 : 11371148 1141 fig . 
2a - e a 49 - year - old patient with a suspicious 9 - mm enhancing lesion in the left breast ( histology at biopsy : ductal carcinoma in situ ; nal histology : inltrating ductal carcinoma )  . 
2a - e paziente di 49 anni con una lesione sospetta dotata di enhancement di 9 mm alla mammella sinistra ( istologia alla biopsia : dcis ; istologia denitiva : carcinoma duttale inltrante )  . 
a immagine coronale t1 - pesata pre - contrasto che mostra la mammella affetta posizionata nel device di compressione perforata con i due tubi marcatori riempiti con glicerina che appaiono come spot iperintensi . 
larea iperintensa del sanguinamento minore nel sito della lesione ancora visibile . standards of reference if the biopsy result indicated malignancy , the standard of reference was histology on the surgical specimen . 
lintera procedura di mrbb , dal posizionamento della 1142 table 1 lesion size lesions size n ( % ) < 6 mm 610 mm 1120 mm > 20 mm total < 6 mm 610 mm 1120 mm > 20 mm totale 8 ( 11.4 ) 45 ( 64.3 ) 14 ( 20 ) 3 ( 4.3 ) 70 ( 100 ) 8 ( 11 , 4 ) 45 ( 64 , 3 ) 14 ( 20 ) 3 ( 4 , 3 ) 70 ( 100 ) tabella 1 dimensione delle lesioni dimensione delle lesioni n ( % ) statistical analysis for quantitative parameters , statistical analyses were performed by mean values , standard deviations ( sd ) and ranges . 
the study used the most common indexes of diagnostic performance : sensitivity , specicity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy . 
diagnostic accuracy was calculated with the formula : ( true positives + true negatives ) / ( true positives + true negatives + false positives + false negatives )  . 
 true positives , true negatives , false positives and false negatives are intended as the biopsy results compared with reference standards results . results mean lesion diameter was 10.26 ( range , 340 ) meight lesions ( 11.4% ) were enhancing foci < 6 mm in diameter , 45 ( 64.3% ) were masses between 6 and 10 mm , 14 ( 20% ) were masses between 11 and 20 mm and the remaining 3 ( 4.3% ) were masses > 20 mm in diameter ( table 1 )  . 
the results of histology on biopsy specimens are radiol med ( 2013 ) 118 : 11371148 paziente allultima sequenza t1 - pesata , durata circa 45 minuti ; non abbiamo implementato una precisa valutazione dei tempi . 
alcuni componenti del device di localizzazione mammaria che abbiamo utilizzato sono mostrate in figura 1 ; le immagini ottenute durante una procedura di mrbb sono mostrate in figura 2 . standard di riferimento se il risultato della biopsia stato maligno , lo standard di riferimento stato listologia sul pezzo operatorio . 
 se il risultato della biopsia stato non maligno , gli standard di riferimento sono stati la mri mammaria di follow - up o listologia sul pezzo operatorio . analisi statistica per i parametri quantitativi , le analisi statistiche sono state effettuate mediante valori medi , deviazioni standard e intervalli . 
in questo studio , sono stati utilizzati i pi comuni indici di performance diagnostica : sensibilit , specicit , valore predittivo positivo ( ppv ) , valore predittivo negativo ( npv ) , accuratezza diagnostica . 
laccuratezza diagnostica stata calcolata con la formula : ( veri positivi + veri negativi ) / ( veri positivi + veri negativi + falsi positivi + falsi negativi )  . 
i veri positivi , i veri negativi , i falsi positivi e i falsi negativi sono intesi come i risultati delle biopsie rapportati ai risultati degli standard di riferimento . risultati il diametro medio delle lesioni stato di 10 , 26 mm ( range 340 mm )  . 
 of the 41 nonmalignant lesions ( 58.6% of the total ) , 35 ( 85.4% ) underwent follow - up mr imaging for a mean period of 2619 ( range , 1168 ) months . 
of the 35 nonmalignant ndings that underwent follow - up mr imaging , 14 were normal breast tissue , 6 were normal breast tissue mixed with areas of brosis , 4 were normal breast tissue mixed with areas of adenosis and the remaining 11 included ndings of brocystic disease , brous - connectiveadipose tissue , ductal hyperplasia without atypias , sclerosis and sclerosing adenosis . 
two lesions had the marker clip positioned at the lesion site and underwent subsequent mammography - guided positiva ( maligna ) stata registrata in 29 casi ( 41 , 4% )  . 
in 10 dei 29 casi maligni ( 34 , 5% ) , la lesione era in situ ( 9 carcinomi duttali in situ , dcis , e 1 carcinoma papillare in situ )  . 
la concordanza fra la biopsia e listologia denitiva stata molto alta , poich solamente 1 lesione , che alla biopsia era un dcis , stato upgradato a carcinoma duttale invasivo dopo la chirurgia . 
 delle 41 lesioni non maligne ( 58 , 6% del totale ) , 35 ( 85 , 4% ) sono state sottoposte a mri di follow - up per un periodo medio di 2619 mesi ( range 1168 mesi )  . 
dei 35 reperti non maligni che sono stati sottoposti a follow - up con mri , 14 erano tessuto mammario normale , 6 erano tessuto mammario normale frammisto ad aree di brosi , 4 erano tessuto mammario normale frammisto ad aree di adenosi , e i rimanenti 11 risultati bioptici comprendevano reperti di malattia brocistica , tessuto bro - connettivo - adiposo , iperplasia duttale senza atipie , sclerosi , adenosi sclerosante . 
due lesioni avevano una marker clip posizionata nella sede della lesione e sono state sottoposte a successiva localizzazione con lo posizionato sotto guida mammograca ; le altre 4 sono state localizzate prima dellintervento chirurgico con lo posizionato sotto guida mri . 
listologia denitiva ha mostrato lesioni non maligne in 3 ( brosi e tessuto mammario normale , malattia brocistica , e tessuto mammario normale , rispettivamente ) , lesione borderline in 1 ( carcinoma lobulare in situ , lcis ; listologia su biopsia aveva dimostrato unicamente malattia brocistica ) e lesioni maligne in 2 casi ( carcinoma duttale invasivo e carcinoma tubulare ; listologia sulle biopsie aveva dimostrato unicamente tessuto mammario normale e tessuto bro - adiposo , rispettivamente ) ( tabella 3 )  . sensibilit , specicit , ppv , npv e accuratezza diagnostica della procedura di mrbb sono stati , rispettivamente , 93 , 5% , 100% , 100% , 95 , 1% e 97 , 1% se la lesione borderline ( lcis ) fosse considerata un risultato istologico non maligno ; 90 , 6% , 100% , 100% , 92 , 7% e 95 , 7% se il lcis fosse considerato un risultato maligno . 
i dati per le analisi statistiche sopra menzionate si trovano nella tabella 4 . fa , tessuto bro - adiposo ; tc , carcinoma tubulare ; nbt , tessuto mammario normale ; idc , carcinoma duttale invasivo ; fcd , malattia brocistica ; lcis , carcinoma lobulare in situ ; s , sclerosi ; f , brosi ; a , adenosi ; pep , proliferazione papillare epiteliale ; am , metaplasia apocrina ; idp , papilloma intraduttale discussione wire localization ; the other 4 were localized preoperatively by a wire positioned under mr guidance . 
abbiamo utilizzato un sistema consistente in un ago coassiale amagnetico e un ago ferromagnetico per core biopsy da 14 , 16 o 18 g core biopsy needle , i quali erano gli unici materiali ampiamente disponibili quando abbiamo iniziato la nostra esperienza nel 2002 . 
 le lesioni sottoposte a mrbb nel nostro studio avevano diametro medio di 10 , 26 mm ( range 340 mm ) , e 53 di esse ( 75 , 7% del totale ) erano entro i 10 mi nostri dati sono comparabili a quelli dei pi importanti articoli apparsi in letteratura . 
in questi studi , il diametro medio delle lesioni era fra 8 , 5 [ 12 ] e 17 mm [ 8 ] , e il range era fra 2 , 5 [ 6 ] e 100 mm [ 8 ]  . come mostrato nella sezione dei risultati , la procedura ha mostrato specicit e ppv ottimali ( non abbiamo avuto nessun risultato falso positivo )  . 
 lesions that underwent mrbb in our study had a mean diameter of 10.26 ( range , 340 ) mm , and 53 ( 75.7% of the total ) were within 10 m our data are comparable with those reported by the most important studies published in the literature . 
in those studies , lesions had a mean diameter between 8.5 [ 12 ] and 17 mm [ 8 ] , and a range between 2.5 [ 6 ] and 100 mm [ 8 ]  . in our experience , the procedure had optimal specicity and ppv ( there were no false positive results )  . 
 [ 9 ] , reported no false negative results . the 2 false negative cases were discovered at surgery performed shortly after mrbb because the radiologist was not satised with the clinical , radiological and pathological correlation between the patients medical history , mr appearance of the lesions and the result of histology on the biopsy specimens . 
la piccola dimensione rappresenta una limitazione nota nel campionamento delle lesioni mri - only , anche se recenti articoli sembrano suggerire che questa non una limitazione per i sistemi vabb . 
al contrario , la prossimit alla parete toracica ancora considerata una sda per tutti i sistemi di biopsia [ 16 ]  . nelle 2 pazienti con risultati falsi negativi , sono stati utilizzati aghi core da 16 g . 
siamo consapevoli che lutilizzo di aghi di dimensioni variabili ( aghi per core biopsy da 14 , 16 e 18 g ) rappresenta una signicativa limitazione del nostro studio , poich un fattore confondente . 
tuttavia , questo uno studio retrospettivo basato sulla nostra attivit clinica di routine , quando ciascun radiologo ha scelto gli aghi con cui si sentiva maggiormente a proprio agio in considerazione della specica paziente con cui si stava rapportando . 
 on the contrary , closeness to the chest wall is still considered a challenge for all biopsy systems [ 16 ]  . in the 2 patients with false negative results , 16 - gauge core needles were used . 
we are aware that the use of variable needle sizes ( 14 - , 16and 18 - gauge core biopsy needles ) is a signicant limitation of our study , as it is a confounding factor . 
however , this is a retrospective study based on our routine clinical activity , when every radiologist chose the needles he / she felt more comfortable with for the particular patient he / she was dealing with . 
moreover , at certain time points in our study , the only coaxial needle size available on the market was 16 gauge , which meant we could only use 18 - gauge biopsy needles . 
ve out of 29 ( 17.2% ) [ 17 ]  . among the 6 nonmalignant lesions that underwent surgical intervention , 1 turned out to be lcis , which is considered a high - risk lesion . 
in our study , the radiologicalpathological correlation of this 15 - mm - thick , 30 - mm - long lesion was again not considered satisfactory , and surgery was performed . 
the most common approach is to implement a close imaging follow - up , also with mr imaging , because there is the risk of developing multicentric and / or bilateral invasive breast cancer after a diagnosis of lobular neoplasia . 
we could speculate that this reects the relatively small sample size of our study . six of 70 ( 8.6% ) lesions had to undergo additional surgery after the mrbb procedure . 
 all 35 nonmalignant lesions followed - up with mr imaging were characterised by a concordant radiologicalpathological correlation ; they were stable for many months , and no further diagnostic procedures were needed . 
the followup was quite long in the majority of cases ( up to 68 months ) ; in our opinion , out of a study setting , a 2or 3 - year folinoltre , in alcuni momenti del nostro studio , la sola dimensione di ago coassiale disponibile sul mercato era quella di 16 g , pertanto potevamo utilizzare unicamente aghi da biopsia da 18 g . 
5 dcis upgradati su 29 ( 17 , 2% ) [ 17 ]  . fra le 6 lesioni non maligne che sono state sottoposte a intervento chirurgico , 1 risultata essere un lcis , che considerato una lesione ad alto rischio . 
nel nostro studio , ancora una volta la correlazione radiologica - patologica di questa lesione con spessore di 15 mm ed estensione di 30 mm non stata soddisfacente ed stato eseguito lintervento chirurgico . 
lapproccio pi comune quello di eseguire uno stretto follow - up con limaging , anche con mri , poich esiste il rischio di sviluppare un carcinoma invasivo multicentrico e / o bilaterale dopo la diagnosi di neoplasia lobulare . 
 curiosamente , non abbiamo avuto alcun caso di iperplasia duttale atipica , che lanormalit ad alto rischio pi comune allistologia , come valutato anche da un recente studio di strigel et al . 
potremmo supporre che questo sia il risultato della dimensione relativamente ridotta del campione del nostro studio . sei su 70 lesioni sono state sottoposte a ulteriore chirurgia dopo la procedura di mrbb . 
 tutte le 35 lesioni che sono state sottoposte a follow - up con mri erano caratterizzate da correlazione radiologicapatologica concordante , sono rimaste stabili per molti mesi , e non sono state necessarie ulteriori procedure diagnostiche . 
il follow - up stato piuttosto lungo nella maggioranza dei casi ( no a 68 mesi ) ; nella nostra opinione , al di fuori delle condizioni dello studio , un follow - up di 2 o 3 anni con mri mammaria ogni 612 mesi dopo la mrbb potrebbe essere considerato esteso in modo sufciente per essere condenti circa il fatto che lesioni mammarie dotate di enhancement siano dei veri negativi . le tempistiche della procedura di mrbb non sono state precisamente valutate nello studio , sebbene la nostra anaradiol med ( 2013 ) 118 : 11371148 1147 low - up with breast mr evaluation every 612 months after mrbb should be considered long enough to be condent that enhancing breast lesions are true negatives . lisi approssimativa ( 45minuti ) in accordo con i dati nella letteratura riguardanti sistemi di biopsia non vacuum - assisted [ 4 , 13 ]  . mrbb procedure times were not thoroughly evaluated in our study , even though our rough evaluation ( 45 min ) is consistent with literature data regarding non - vabb systems [ 4 , 13 ]  . conclusioni conclusions the mrbb system used in this study , consisting of a nonmagnetic coaxial needle and a ferromagnetic 14 - , 16or 18 - gauge core biopsy needle , represented an easy way of performing a biopsy procedure and was well applicable in the routine clinical setting . 
we also performed a critical revision of each case that , despite being benign , remained suspicious for the radiologist ; this avoided any diagnostic delays on malignancies . we are aware that current european consensus guidelines advocate that vabb should be used in preference to core needle biopsy [ 20 ]  . 
we continued to perform mrbb with core needles until 2008 , when we switched to a vabb syste il sistema di mrbb che abbiamo utilizzato , consistente in un ago coassiale amagnetico e un ago ferromagnetico per core biopsy da 14 , 16 o 18 g core biopsy needle , ha rappresentato una facile modalit per eseguire una procedura bioptica , ed stato facilmente applicabile nella routine clinica . 
questo ha permesso di evitare ritardi diagnostici su lesioni maligne . siamo a conoscenza del fatto che le attuali linee - guida europee in consenso sostengano che la vabb dovrebbe essere preferita alla biopsia core needle [ 20 ]  . 
senologia clinica e screening mammograco , dipartimento di radiodiagnostica , apss , trento italy 3servizio di diagnostica clinica senologica , ospedale koelliker , c.so galileo ferraris 256 , torino , italy 4dipartimento di scienze biomediche ed oncologia umana , universit di torino , a.o.u. 
the median pathological tumour size was 22.3 mmri and dbt had a level of concordance with pathology of 70% and 66% , respectively , which was higher than that of dm ( 54% )  . 
per ogni metodica , stata valutata lestensione massima tumorale ; le misurazioni sono state considerate concordanti con listologia se comprese nei 5 m stato calcolato il coefciente di correlazione di pearson rispetto allestensione istologica per ciascuna metodica . 
il diametro medio delle lesioni stato 22 , 3 m rm e dbt hanno avuto rispettivamente una concordanza del 70% e 66% con listologia , superiore alla dm ( 54% )  . 
limpiego della dbt sembra implementare i risultati della dm , sebbene lrm rimanga la metodica di riferimento . parole chiave carcinoma mammario staging preoperatorio tomosintesi rm estensione tumorale introduction introduzione breast cancer size is one of the main prognostic indicators and a determining factor for surgical treatment planning . 
 therefore , accurate prediction of tumour size at diagnosis , assessed by imaging , is essential for planning appropriate management . many published studies have evaluated and compared the accuracy of digital mammography ( dm ) , ultrasonography ( us ) and magnetic resonance imaging ( mri ) in the preoperative staging of breast cancer [ 111 ]  . 
however , there are currently few studies which consider also digital breast tomosynthesis ( dbt ) [ 1214 ] and no studies comparing dbt to mri . preoperative tumour size is commonly measured with dm and / or us and , in accordance with the european guidelines , only in selected cases with mri [ 111 , 15 , 16 ]  . the recent clinical application of dbt as a complementary or adjunctive technique to dm seems able to overcome one of the major problems of the two - dimensional technique , by reducing the obscuring effect of overlying tissues and allowing a better view of lesion margins [ 12 ]  . 
 our hypothesis was that , considering these peculiarities , the measurement of lesion size using dbt could be more accurate than using dm and us , and approach mri accuracy . 
the purpose of our study was therefore to compare the accuracy of dm , dbt , us and mri in the preoperative assessment of tumour size , using pathological size as the gold standard , in 110 patients with newly diagnosed breast cancer . materials and methods we retrospectively reviewed 149 breast cancers in 110 patients who underwent dm , dbt , us and mri at our institula dimensione del tumore mammario rappresenta uno dei fattori prognostici principali , nonch il parametro determinante nella scelta del trattamento chirurgico - terapeutico . 
 laccuratezza della valutazione delle dimensioni della neoplasia alla diagnosi , mediante le metodiche di imaging , dunque indispensabile per una corretta pianicazione terapeutica . in letteratura vi sono numerosi studi che valutano e confrontano laccuratezza della mammograa ( dm ) , dellecograa ( us ) e della risonanza magnetica ( rm ) nello staging pre - operatorio del carcinoma mammario [ 111 ] ; al momento attuale , invece , vi sono pochi studi che considerino anche la tomosintesi ( dbt ) [ 1214 ] e non esistono studi che comparino questultima alla rm nella valutazione dellestensione delle lesioni mammarie . normalmente , le misurazioni pre - operatorie delle lesioni sono effettuate con la dm e / o con us e in casi selezionati , secondo le indicazioni delle linee guida europee , con la rm [ 111 , 15 , 16 ]  . recentemente introdotta nella pratica clinica come tecnica complementare e / o aggiuntiva alla dm , la dbt sembra attualmente in grado di superare uno dei maggiori limiti della tecnica 2d , riducendo il mascheramento delle lesioni e permettendo una migliore visualizzazione dei loro margini , superando i problemi derivanti dalla sovrapposizione dei tessuti [ 12 ]  . la nostra ipotesi che , grazie a questa peculiarit della metodica , la misurazione delle lesioni con la dbt possa essere pi precisa rispetto alla dm e allus , avvicinandosi allaccuratezza della rm . 
scopo dello studio stato dunque confrontare laccuratezza della dm , dbt , us e rm nella valutazione pre - operatoria dellestensione tumorale rispetto allesame istologico denitivo ( utilizzato come gold standard ) in 110 pazienti affette da neoplasia mammaria . radiol med ( 2013 ) 118 : 11191136 1121 tion between january 2010 and december 2011 , before denitive surgery . 
patients who underwent neoadjuvant chemotherapy were excluded from the study . all patients meeting the following inclusion criteria ( approved by the local ethics committee ) underwent combined dm and dbt ( combo mode ) : ( 1 ) women with suspicious ndings requiring needle biopsy ; ( 2 ) women with a history of breast cancer ; ( 3 ) women with previous mammograms classied as breast imaging - reporting and data system ( bi - rads ) 3 , 4 or 5 ; ( 4 ) symptomatic women [ palpable lump , changes in breast shape or volume , skin retraction , areola and / or nipple changes , unilateral mono - oricial nipple discharge , palpable lymph node with carcinoma of unknown primary ( cup ) syndrome , unilateral not premenstrual breast pain ] ; ( 5 ) asymptomatic women aged 50 years , with known dense breasts from previous examination ; ( 6 ) asymptomatic women between 40 and 49 years . before undergoing the mammographic examination , all patients were informed about the technical aspects , benets and risks of dbt , and they subsequently gave their informed consent . combined dbt and dm involves the acquisition of standard bilateral two - view mammograms ( cranio - caudal and medio - lateral oblique ) within a single compression for each projection . 
overall scanning time is about 5 seconds and reconstruction time is about 10 seconds . us examination was performed in all patients on a dedicated unit ( hitachi logos hi vision or esaote my lab twice ) using a 1018 mhz probe . all patients subsequently underwent preoperative mri ( achieva 1.5 t , philips ) using a dedicated 7 - channel phased - array coil . 
in accordance with the literature and the european society of breast cancer specialists ( eusoma ) guidelines [ 1517 ] , the 110 patients included in our study underwent preoperative mri staging because they : ( 1 ) had a newly diagnosed invasive lobular carcinoma ; ( 2 ) had a high risk of breast cancer ; ( 3 ) were aged < 60 years and had a > 1 cm discrepancy between the dm and us measurements , with expected impact on treatment decisions ; ( 4 ) were eligible candidates for partial breast irradiation ( pbi ) on the basis on conventional imaging . 
we also included , as per further eusoma recommendations [ 16 ] , patients : ( 1 ) with dense breasts [ women < 40 years with dense breasts or women with dense breasts associated with an intermediate lifetime risk ( 15%20% ) due to other factors ] ; ( 2 ) with multifocal , multicentric or bilateral cancer ( invasive and / or ductal carcinoma in situ , dcis ) demonstrated on conventional imaging and conrmed by pathology ; ( 3 ) with materiali e metodi sono state valutate retrospettivamente 149 neoplasie mammarie in 110 pazienti che tra gennaio 2010 e dicembre 2011 sono state sottoposte a dm , dbt , us e rm , presso il nostro servizio , prima di effettuare lintervento chirurgico . 
in tutti i casi stato utilizzato il mammografo selenia dimensions prodotto da hologic inc ( bedford , ma , usa )  . per la modalit dbt , la scansione viene eseguita utilizzando unangolazione complessiva di 15 ( 7 , 5 ) con 15 esposizioni a bassa dose . 
il tempo totale di scansione di circa 5 secondi e il tempo di ricostruzione di circa 10 secondi . lesame ultrasonograco stato eseguito in tutte le pazienti con apparecchiatura dedicata ( hitachi logos hi vision oppure esaote my lab twice ) con sonda da 1018 mhz . 
 tutte le 110 pazienti sono state successivamente sottoposte a rm di staging pre - operatorio utilizzando unapparecchiatura achieva da 1 , 5 t ( philips ) con bobina dedicata phased - array a 7 canali . 
 secondo le indicazioni della letteratura ed in particolare le linee guida delleuropean society of breast cancer specialists ( eusoma ) [ 1517 ] , le 110 pazienti incluse nello studio hanno eseguito la stadiazione pre - operatoria con rm in quanto pazienti : ( 1 ) con nuova diagnosi di carcinoma lobulare inltrante ; ( 2 ) ad alto rischio per tumore della mam1122 radiol med ( 2013 ) 118 : 11191136 mella ; ( 3 ) con et < 60 anni e con discrepanza > 1 cm nella misurazione tra dm e us per valutare un possibile cambiamento del tipo di approccio chirurgico ; ( 4 ) candidabili a partial breast irradiation ( pbi ) sulla base dellimaging convenzionale ; sono state inoltre incluse , come ulteriormente proposto dalleusoma [ 16 ] , pazienti : ( 1 ) con mammelle dense [ mammelle dense in donne < 40 anni di et o mammelle dense associate ad un lifetime risk intermedio ( 15% 20% ) dovuto ad altri fattori ] ; ( 2 ) con diagnosi di tumore multifocale , multicentrico o bilaterale ( invasivo o carcinoma duttale in situ cdis ) gi accertata con le metodiche convenzionali e confermata dallistologia ; ( 3 ) pazienti con diagnosi di cdis unilaterale / unifocale allimaging convenzionale ( per escludere la presenza di un carcinoma invasivo sincrono omolaterale o controlaterale ) ; ( 4 ) pazienti con tumore di paget ; ( 5 ) pazienti candidate a mastectomia skin sparing , per la valutazione del complesso areola - capezzolo . le immagini mammograche ( dm e dbt sia valutate singolarmente , che in associazione ) , ecograche ed di rm sono state rivalutate retrospettivamente in modo indipendente da due radiologi esperti in senologia ( e con esperienza in dbt di almeno 2 anni ) , a conoscenza dello scopo studio , ma non a conoscenza dellestensione istologica delle lesioni , le cui misurazioni sono state utilizzate come gold standard . 
 per la classicazione dei reperti mammograci ( in dm e in dbt ) sono stati valutati la densit del parenchima mammario utilizzando il sistema bi - rads di densit ( broadiposa , bi - rads 1 : 0%25% di tessuto ghiandolare ; broghiandolare , bi - rads 2 : 26%50% ; moderatamente densa , bi - rads 3 : 51%75% ; estremamente densa , bi - rads 4 : > 75% ) e la presenza di segni mammograci sospetti ( microcalcicazioni , opacit focali o distorsioni parenchimali ) [ 18 , 19 ]  . per ogni lesione visibile in dm , dbt e rm stato misurato lasse maggiore al monitor della workstation mediante software dedicato . 
per quanto riguarda lus invece , sono state rivalutate le immagini statiche ecograche delle lesioni ( acquisite durante lindagine diagnostica ed archiviate nel database pazienti dellapparecchiatura ) , effettuando la misurazione della dimensione massima . tutte le pazienti sono state sottoposte ad intervento chirurgico di exeresi della neoplasia primitiva e a chirurgia del cavo ascellare ( biopsia del linfonodo sentinella e / o a dissezione ascellare )  . i campioni sono stati inviati ai laboratori del dipartimento di anatomia patologica della nostra azienda sanitaria - ospedaliera , previa valutazione radiograca nel pezzo operatorio delleffettiva presenza della lesione . 
1a , b coefciente di correlazione lineare di pearson : confronto tra dbt e rm ( a ) e tra dbt e dm ( b ) rispetto allistologia [ differenze risultate statisticamente signicative ( p < 0 , 01 ) ]  . unilateral unifocal pure dcis at conventional imaging ( to exclude synchronous ipsilateral or contralateral invasive carcinoma ) ; ( 4 ) with pagets disease ; ( 5 ) candidate for total skin - sparing mastectomy ( evaluation of nipple - areola complex )  . the dbt , dm ( evaluated individually or in combination ) , us and mr images were retrieved for retrospective independent interpretation by two radiologists experienced in breast imaging ( with more than 2 years experience in dbt ) ; the radiologists were aware of the study purpose , but were blinded to the histological lesion size , considered the gold standard . 
images of each modality were presented randomly to each reader in separate sessions and any discrepancy in opinion was resolved by consensus . for the mammographic classication ( on dm and dbt ) , we evaluated breast density using bi - rads categories ( fatty , bi - rads 1 : 0%25% of glandular tissue ; scattered broglandular , bi - rads 2 : 26%50% ; heterogeneously dense , bi - rads 3 : 51%75% ; extremely dense , bi - rads 4 : > 75% ) and the presence of suspicious mammographic radiol med ( 2013 ) 118 : 11191136 1123 fig . 
in the lower - outer quadrant of the right breast a spiculated mass ( red arrow ) is seen on both the cranio - caudal ( cc ) ( b ) and medio - lateral oblique ( mlo ) ( c ) views on the 3d images . 
nelle immagini 3d si osserva nel quadrante infero - esterno di destra unopacit a margini spiculati ( freccia rossa ) sia nella proiezione cranio - caudale ( cc ) ( b ) , che nella medio - laterale obliqua ( mlo ) ( c )  . 
e rm : limmagine dinamica acquisita sul piano assiale ha confermato la presenza di una lesione di tipo mass nel quadrante inferoesterno di destra , dotata di disomogeneo contrast enhancement e margini irregolari . 
misurazione della lesione : 11 mf preparato istologico della lesione : carcinoma lobulare inltrante ( dimensioni 12 mm ) ( pt1c g2 )  . 1124 radiol med ( 2013 ) 118 : 11191136 ndings ( microcalcications , masses or focal parenchymal distortion ) [ 18 , 19 ]  . 4 mm , dal margine profondo al margine superciale verso la cute . for each lesion visible on dm , dbt and mri the maximum tumour size was measured to the nearest millimetre using dedicated software on the workstation . 
as for the us examinations , we reviewed the static us images of the lesions ( acquired during the diagnostic examination and stored in the systems patient database ) and performed the measurements of the maximum tumour size . 
 all patients underwent surgical excision of the primary tumour and sentinel lymph node biopsy and / or axillary dissection . the breast specimens were sent to the laboratories of the pathology department of our hospital , after verifying the actual presence of the lesion in the surgical specimen by radiographic evaluation . 
each sample , after being macroscopically measured , was cut into multiple 4 - mm - thick sections from the deep margin to the supercial edge towards the sk each slice of breast tissue was stretched over a sheet of blotting paper , taking care to maintain the orientation established by the surgeons . 
when the tumour was not macroscopically identied , sampling was performed by following the radiologists directions and by viewing the exact location of the lesion on postoperative specimen radiography , received at the pathology department . 
in addition , the need to perform macrosections was evaluated in each case ; macrosections were prepared especially in cases where the tumour was ( i ) very large , ( ii ) not denable with certainty due to the presence of spicules or peritumoural thickening , ( iii ) not macroscopically visible , as in tumours in situ with intra - adipose growth and spread and detectable only for the presence of microcalcications . sampling was performed using a photographic device installed under the fume hood , which makes it possible to acquire images of each level , and to mark on each image the exact position of the single sample . 
the samples , whether traditional or in macrosections , were placed into special plastic cassettes and loaded into the automatic processor , where they were immersed in alcohol , xylene and parafn . after processing , the tissue in the cassettes was embedded in parafn , and sections of 4 micron in thickness were cut , placed on slides and stained with haematoxylin and eos microscopic histological measurements were made on the slides using a metric eyepiece . 
in fact , if the tumour was visualised on sections at different levels , with knowledge of the thickness of the single layer , it was possible to obtain a three - dimensional measurement of the lesion . ogni sezione stata posta su fogli di carta bibula , mantenendo lorientamento stabilito dai chirurghi . 
nel caso in cui il tumore non era stato macroscopicamente identicato veniva invece eseguito il campionamento seguendo le indicazioni del radiologo e visualizzando sulla radiograa del pezzo , pervenuta in anatomia patologica , lesatta localizzazione della lesione . 
inoltre , in ogni singolo caso stata valutata lopportunit di eseguire delle macrosezioni , che sono state allestite soprattutto nei casi in cui il tumore risultava ( i ) particolarmente esteso , ( ii ) non delimitabile con certezza per la presenza di spicule o addensamenti peri - neoplastici , ( iii ) non visibile macroscopicamente , come nel caso di tumori in situ a crescita e diffusione intra - adiposa ed identicabili solo per la presenza di microcalcicazioni . 
 la fase di campionamento stata effettuata utilizzando unapparecchiatura fotograca , installata sotto la cappa aspiratrice , che permette di acquisire immagini di ogni livello , nonch di contrassegnare su di esse lesatta localizzazione del singolo campionamento . 
i prelievi effettuati tradizionalmente o mediante macrosezioni sono stati posti in apposite biocassette in plastica , sono stati inseriti nel processatore automatico dove hanno subito passaggi in alcoli , xilolo e parafna . 
 dopo la processazione , il tessuto nelle biocassette stato incluso in parafna e da questo sono state tagliate sezioni di 4 micron di spessore , che sono state poste su vetrini e colorate con ematossilina ed eosina . 
 infatti , se la visualizzazione della neoplasia avveniva su sezioni a livelli diversi , essendo a conoscenza dello spessore del singolo livello , si potuto ottenere una misurazione tridimensionale della lesione . 
 analisi statistica per analizzare la correlazione fra le misurazioni delle lesioni effettuate mediante dm , dbt , us e rm e le dimensioni dellistologico denitivo , stato calcolato il coefciente di correlazione lineare di pearson ( r )  . 
 stato anche valutato il coefciente di correlazione delle varie metodiche di imaging , rispetto allesame istologico denitivo , in base alla densit mammaria , al tipo di segno mammograco e allistotipo delle lesioni . per ogni lesione stata calcolata la differenza in milliradiol med ( 2013 ) 118 : 11191136 statistical analysis pearsons linear correlation coefcient ( r ) was calculated for each modality in order to analyse the correlation between the lesion measurements performed by dm , dbt , us and mri compared to the pathological size . 
we also assessed the correlation coefcient compared to nal histology of each imaging modality , in relation to breast density , mammographic features and histological tumour type . for each lesion , the difference in size in millimetres was calculated between the imaging and pathology measurements , in order to assess correlations and to generate scatter plots . 
the measurements were considered concordant with histology if they were within 5 mm , and underand overestimated , respectively , if they were < 5 mm and > 5 mm compared to pathological size . 
 nella valutazione della concordanza , le lesioni sono state inoltre straticate in base alle dimensioni 2 cm e > 2 cm . stata inoltre calcolata la detection rate ( dr ) delle varie metodiche di imaging . le differenze statisticamente signicative tra i valori osservati nello studio sono state calcolate mediante il test chi - quadrato e il test t di student , usando come soglia di signicativit un valore di p < 0 , 01 . 
in this subgroup , no r value was statistically signicant ( table 1 )  . as for mammographic density , patients were divided into two groups : fatty breasts ( bi - rads 1 + bi - rads 2 ) and dense breasts ( bi - rads 3 + bi - rads 4 )  . 
 per i carcinomi duttali in situ si osservato un coefciente di correlazione di 0 , 93 per la dm e la dbt e di 0 , 88 per lrm ( valori non statisticamente signicativi , p > 0 , 01 )  . 
per lus non risultato valutabile . per le lesioni classicate come opacit alla dm e alla dbt si osservata una correlazione di 0 , 86 alla dm , 0 , 9 alla dbt , 0 , 82 allus e 0 , 92 alla rm . 
per valutare lestensione di ogni lesione , in dbt abbiamo effettuato le misurazioni in due modi : sia considerando solo il core lesionale sia includendo la massima estensione delle spicule , ottenendo rispettivamente una correlazione di 0 , 88 e di 0 , 81 . 
la differenza tra i due coefcienti della dbt considerando il solo core lesionale o anche le spicule non risultata statisticamente signicativa . per le distorsioni risultata una correlazione di 0 , 85 alla dm , 0 , 93 alla dbt , 0 , 75 allus e 0 , 94 alla rm . 
per le microcalcicazioni inne abbiamo osservato un coefciente di pearson di 0 , 72 per la dm , 0 , 75 per la dbt e 0 , 85 per lrm . 
 mammograa la dm risultata la metodica meno concordante con lesame istologico denitivo : 81 casi ( 54 , 4% ) sono risultati concordanti , 21 sottostimati ( 14 , 1% ) e 21 sovrastimati ( 14 , 1% ) ; 26 lesioni non sono risultate visibili alla dm ( 17 , 4% )  . 
 per le lesioni t1 la concordanza tra dm e listologico denitivo stata del 65 , 9% , per tumori > 2 cm stata invece del 39 , 1% . tomosintesi la dbt ha una concordanza con lesame istologico denitivo del 66 , 4% ( 99 casi ) ; 17 casi sono risultati sottostimati ( 11 , 4% ) e 17 sovrastimati ( 11 , 4% ) ; 16 lesioni non sono risultate visibili ( 10 , 7% )  . 
 in us la concordanza per neoplasie 2 cm stata del 74 , 1% , per lesioni > 2 cm stata del 32 , 8% . risonanza magnetica lrm risultata in assoluto la metodica con la maggior concordanza rispetto allistologia : infatti , 105 lesioni , pari al 70 , 5% , sono risultate concordanti , 13 ( 8 , 7% ) sottostimate e 27 ( 18 , 1% ) sovrastimate . 
 per i casi t1 abbiamo avuto una concordanza dell83 , 5% con listologia ; nei t2 o superiori invece stata del 53 , 1% . complessivamente tra le quattro modalit di imaging le differenze tra le concordanze risultate statisticamente signicative ( p < 0 , 01 ) sono state tra lrm e la dm , tra lrm e la dbt e tra lrm e lus . 
 lanalisi congiunta di dm e dbt non ha determinato un incremento del numero di lesioni visibili rispetto alla sola dbt ; invece lassociazione tra dm e us e tra dbt e us ha incrementato la dr rispettivamente al 94 , 6% e al 96% ( valori statisticamente signicativi , p < 0 , 01 )  . per il calcolo della dr abbiamo anche suddiviso le 110 pazienti in due sottogruppi : neoplasia unifocale o multifocale . nei casi di lesioni unifocali la dr stata del 91 , 9% per la dm , del 97 , 7% per la dbt , dell84 , 9% per lus e del 100% per lrm . 
le differenze di dr tra le metodiche sono risultate tutte statisticamente signicative ( p < 0 , 01 )  . nelle pazienti affette da patologia multifocale invece la dr stata del 69 , 8% per la dm , del 77 , 8% per la dbt , del 74 , 6% per lus e del 93 , 6% per lrm . 
le differenze di dr tra rm e dbt , tra rm e dm e tra rm e us sono risultate statisticamente signicative ( p < 0 , 01 ) , invece tra dbt e dm , tra dbt e us e tra dm e us il valore di p risultato maggiore di 0 , 01 . lrm ha individuato la patologia tumorale in tutte le 110 pazienti ; le 4 lesioni non visualizzate allrm sono state riscontrate in pazienti affette da patologia multifocale e avevano dimensione media allistologico denitivo di 4 , 25 mm . discussione unaccurata misurazione dellestensione tumorale fondamentale per lo staging pre - operatorio del carcinoma del la mammella , al ne di stabilire il corretto trattamento chirurgico terapeutico , soprattutto se di tipo conservativo [ 12 ]  . bench lesame istologico denitivo rimanga il gold standard , le decisioni terapeutiche e chirurgiche devono essere intraprese sulla base dellimaging , principalmente sulle metodiche convenzionali ( dm ed us ) ed implementato in casi selezionati dallimpiego della rm . lus spesso sottostima la reale estensione tumorale , bench risulti particolarmente utile in pazienti con seni densi , soprattutto quando la lesione mammograca difcilmente valutabile per la sovrapposizione dei tessuti o per la sommazione di strutture differenti [ 11 , 12 ]  . 
queste lesioni sono caratterizzate dalla presenza di un cono dombra posteriore che ne oscura il margine profondo , rendendo pertanto la misurazione sullasse maggiore pi difcolto sa [ 11 ]  . 
 lrm , secondo la letteratura [ 14 , 6 , 8 ] , risulta lindagine pi accurata e sensibile tra tutte le modalit di imaging pre - operatorie per la valutazione della reale estensione tumorale ( sebbene tenda a sovrastimarla ) e per la diagnosi di multifocalit e multicentricit [ 1517 ]  . 
 inoltre , la rm attualmente considerata la metodica pi afdabile per lo staging dei carcinomi lobulari inltranti ; infatti , in una recente revisione della letteratura [ 20 ] , la rm ha dimostrato una sensibilit del 93% per questo particolare istotipo ed unalta correlazione con listologia ; permette inoltre il riscontro di lesioni occulte controlaterali nel 7% dei casi , cambiando lapproccio chirurgico in circa il 25% dei casi [ 16 ]  . come gi precedentemente sottolineato , la misurazione delle lesioni con la dm risulta spesso difcoltosa a causa delleffetto di mascheramento dovuto alla sovrapposizione dei tessuti . inoltre in dm la misurazione dellestensione tumorale pu essere inuenzata dalle variazioni della distanza tra il tumore e il detettore , dai margini della lesione mal delimitabili e dallentit della compressione della mammella durante lindagine . inne , con le proiezioni mammograche standard non sempre possibile ottenere leffettiva massima estensione tumorale . 
un aiuto pu essere fornito dallutilizzo di proiezioni mammograche aggiuntive ( ingrandimenti o compressioni ) che possono facilitare la visualizzazione dei margini delle lesioni [ 11 ]  . al momento attuale , esiste un solo studio pubblicato in letteratura [ 12 ] che analizzi laccuratezza della dbt nella valutazione dellestensione tumorale ; non esistono invece studi che correlino la dbt alla rm nella diagnosi pre - operatoria . 1130 radiol med ( 2013 ) 118 : 11191136 lying tissues or the summation of different structures [ 11 , 12 ]  . 
however , while us is capable of measuring in multiple planes , it should be noted that often the largest dimension of the lesion cannot be measured , especially if we consider that many cancers are vertical ( taller - than - wide ) lesions . 
these lesions are characterised by posterior acoustic shadowing which obscures the posterior border of the lesion , often making measurement of the longest axis difcult [ 11 ]  . according to the literature data [ 14 , 6 , 8 ] , mri is the most accurate and sensitive preoperative imaging modality for the evaluation of tumour extent ( although it has a substantial risk of overestimation ) and for the detection of multifocal , multicentric breast cancer [ 1517 ]  . 
in addition , mri is currently considered the most reliable method for preoperative staging of invasive lobular carcinomas ; in fact , as reported in a recent literature review [ 20 ] , mri has a sensitivity of 93% in detecting this special type of tumour and a high level of agreement with histology ; mri also allows the detection of contralateral occult lesions in 7% of cases , changing the surgical approach in about 25% of patients [ 16 ]  . as outlined above , dm lesion measurements are often difcult due to the effect of masking and to the tissues superposition . 
moreover , dm tumour measurement can be inuenced by variations in the distance between the tumour and the detector , by poorly delineated tumour outlines and by compression of the breast during examination . 
the use of additional mammographic views ( magnication or compression ) can improve visualisation of lesion margins [ 11 ]  . at present , there is only one published study [ 12 ] that analysed the accuracy of dbt in the evaluation of tumour size , and no studies comparing dbt and mri in the preoperative assessment of breast cancer size . in our study , mri and dbt measurements had the highest correlation with pathological tumour size and thus provided better results than dm and us . 
 [ 12 ] , we found dm to have a higher pearsons correlation coefcient than us ( r : 0.83 versus r : 0.77 ) , probably as a result of the greater proportion in our series of bi - rads 1 and bi - rads 2 breast density , which facilitates the correct measurement of the lesions . 
 [ 11 ] , who found the linear regression coefcient of mammography to be higher than ultrasound ( r2 : 0.74 versus r2 : 0.60 ) compared to the nal nel nostro studio lrm e la dbt si sono rivelate le due metodiche con la pi alta correlazione con le dimensioni indicate allistologico denitivo , ottenendo quindi risultati migliori rispetto alla mammograa e allecograa . 
 [ 12 ] , risulta pi alta la correlazione di pearson della dm ( r : 0 , 83 versus r : 0 , 77 ) a causa della maggior presenza , nella nostra casistica , di densit mammarie birads 1 e bi - rads 2 , che rendono pi agevole la corretta misurazione delle lesioni . 
questo risultato pu essere spiegabile per la particolare presentazione di questo istotipo tumorale , spesso associato alla presenza di una distorsione parenchimale allesame mammograco , pi difcilmente visualizzabile alla sola dm e meno facilmente misurabile per la difcolt nel valutare i reali margini di estensione della neoplasia . 
 inoltre alcuni tumori lobulari inltranti crescono in multipli piccoli foci oppure in singole le di cellule , inltrando diffusamente le normali strutture della mammella senza formare unevidente massa alla mammograa [ 12 ]  . 
 per i carcinomi in situ la dbt e la dm sono risultate le due metodiche con la pi alta correlazione di pearson rispetto allistologico denitivo ; hanno avuto infatti un valore r di 0 , 93 , pi alto rispetto allrm ( r : 0 , 88 )  . 
lrm ha comunque dimostrato una buona correlazione in analogia a quanto riportato in letteratura ove stato dimostrato che alcune forme in situ possono essere visualizzabili solo con la dm , altre con rm e dm e altre ancora con la sola rm [ 6 , 16 , 21 , 22 ]  . nella nostra serie valutando i segni mammograci abbiamo ottenuto correlazioni similari tra dbt e rm per le distorsioni parenchimali ( r : 0 , 93 e r : 0 , 94 rispettivamente ) superiori alla mammograa bidimensionale ( r : 0 , 85 )  . 
 questo valore potrebbe essere ascrivibile alla maggior accuratezza dimostrata dalla dbt nel valutare le distorsioni architetturali rispetto alla dm , la cui possibile spiegazione potrebbe dipendere dalla disposizione su singoli piani dello spazio di questo tipo di lesioni , quindi meglio visualizzabili 1132 radiol med ( 2013 ) 118 : 11191136 often associated with the presence of parenchymal distortion at mammography ; for this reason , it is more difcult to see and less easy to measure on dm , because of the difculty assessing the real extent of the tumour margins . 
 in relation to this mammographic feature , the difference between dbt and dm can be related to the previously reported better visualisation of lesion margins obtained with dbt , which can help to better interpret the mammographic feature and better outline the lesion . 
 [ 23 ] for two - dimensional mammography measurements , the dbt evaluation of spiculated masses is more accurate if we include only the core lesion , without considering the extension of spicules [ 23 ]  . there was no signicant difference between dm and dbt , in relation to the size of microcalcications , in agreement with the study of meacock et al . 
 [ 13 ] presented at european congress of radiology ( ecr ) 2010 . nelle immagini ricostruite a 1 mm in dbt . per le opacit non vi una sostanziale differenza tra dbt e rm ( r : 0 , 9 e 0 , 92 , rispettivamente )  . 
la differenza tra dbt e dm potrebbe essere riferibile in questo tipo di alterazione mammograca alla gi segnalata possibile miglior visualizzazione dei margini delle lesioni ottenuta con la dbt , utile sia per una pi corretta interpretazione del segno mammograco , che per una pi precisa delimitazione della lesione . 
analizzando in particolare le opacit che presentavano margini spiculati alle indagini mammograche ( dm + dbt ) , abbiamo ottenuto una correlazione pi elevata con la dbt rispetto allistologico denivo quando abbiamo misurato il solo core lesionale rispetto alla massima estensione delle spicule ( r : 0 , 88 versus 0 , 81 )  . 
 [ 23 ] , anche per la dbt risulta pi accurato , in caso di opacit a margini spiculati , effettuare la misurazione pre - operatoria includendo il solo core lesionale , senza considerare lestensione delle spicule . per quanto riguarda le microcalcicazioni come segno mammograco , non vi stata una rilevante differenza nella misura dellestensione tra 2d e 3d , risultato in accordo con il lavoro di meacock et al . 
 [ 13 ] presentato alleuropean congress of radiology ( ecr ) 2010 . osservando la correlazione di pearson rispetto alle diverse densit possiamo rilevare che per le mammelle non dense non vi una signicativa differenza nella correlazione tra mammograa 2d e 3d ( r : 0 , 87 e 0 , 9 , rispettivamente )  . nel sottogruppo delle mammelle dense invece si osserva una correlazione della dbt ( r : 0 , 88 ) nettamente pi alta rispetto alla mammograa 2d ( r : 0 , 78 ) e pressoch analoga allrm ( r : 0 , 89 ) , rispetto allistologico denivo . 
lelevata differenza tra dm e dbt nel sottogruppo con densit birads 3 e bi - rads 4 da attribuire alla capacit della dbt di superare il problema della sovrapposizione dei tessuti e di riuscire pertanto ad evidenziare meglio i margini delle lesioni nelle mammelle dense . 
in this subgroup ( bi - rads 3 and bi - rads 4 ) , the large difference between dm and dbt is due to the dbt capability of overcoming the problems of overlapping tissue and therefore better highlighting lesion margins in dense breasts . 
most literature reports , however , state that dm underestimates the true size of lesions , especially spiculated lesions , due to difculties in assessing their margins [ 12 ]  . us seems to underestimate the true size of lesions , with 16.8% of underestimated cases , as reported by dummin et al . 
in fact , on us very often only the hypoechoic part of the lesion is included in the measurement and not the hyperechoic zone representing the spiculated periphery [ 12 ]  . mri , consistent with other studies [ 1 , 4 , 6 ] tends to overestimate true tumour size ( in 18.1% of cases in our series ) , but it proved to be the most accurate modality , as it had the least standard deviation from the size at pathology and therefore showed the least dispersion in the sample [ 4 ]  . for both t1 and t2 or higher tumours , mri was the modality with the highest agreement with pathology , which was 83.5% for tumours 2 cm and 53.1% for tumours > 2 cm , respectively , as already reported by onesti et al . 
 [ 12 ] ; these authors found that , for lesions greater than 20 mm , there was an increased difference of correlation between imaging and nal histological examination , with a consequent reduction of agreement , considering also the chosen cut - off of 5 mm . ( 66 , 4% )  . 
 sia la dbt che la dm , risultata tra le quattro metodiche quella con la minor concordanza rispetto allanatomia patologica , hanno avuto un egual numero di casi sovra e sottostimati . 
nella maggior parte dei lavori presenti in letteratura invece stata descritta una sottostima delle reali dimensioni delle lesioni in dm , specie per le opacit a margini spiculati , a causa delle difcolt nel valutarne i margini [ 12 ]  . 
infatti spesso in ecograa viene inclusa nella misurazione solo la parte ipoecogena della lesione mentre non viene considerata la zona iperecogena che rappresenta la periferia e che corrisponde alla componente spiculata [ 12 ]  . lrm , in accordo con altri lavori presenti in letteratura [ 1 , 4 , 6 ] , tende invece a sovrastimare la reale estensione tumorale ( nella nostra serie nel 18 , 1% dei casi ) ma la metodica che risultata pi precisa avendo la minor deviazione standard dal valore dellistologico denitivo e quindi la minor dispersione del campione [ 4 ]  . sia per i tumori t1 che per le neoplasie t2 o superiori , la metodica con la maggiore concordanza risultata lrm con valori rispettivamente del 83 , 5% se 2 cm e del 53 , 1% se > 2 cm , come gi descritto in letteratura da onesti et al . 
 la dbt si rivelata la metodica che pi si avvicina allrm sia per neoplasie 2 cm che > 2 cm , con una concordanza rispettivamente del 77 , 6% e 51 , 6% . la dm e lus hanno avuto buoni valori di concordanza per lesioni t1 ( 65 , 9% e 74 , 1% ) ottenendo invece valori inferiori per lesioni > 2 cquesti risultati sono analoghi a quelli ottenuti nel lavoro di frnvik et al . 
 [ 12 ] , nel quale viene rilevato che per lesioni di dimensioni superiori ai 20 mm si ha un aumento della differenza di correlazione tra le metodiche di imaging e lesame istologico , con conseguente riduzione della concordanza , anche a causa del cut - off scelto di 5 mm . analizzando in dettaglio la dr delle varie metodiche di imaging si deve evidenziare che grazie alla dbt abbiamo potuto diagnosticare e misurare un numero maggiore di lesioni rispetto alla dm e allus . 
la dbt ha infatti portato ad un incremento della dr del 6 , 7% rispetto alla dm , e dell8 , 8% rispetto allus , risultando la metodica che si avvicina di pi al valore della rm . 
il nostro dato parrebbe in accordo con quanto gi emerso da un altro studio , in cui veniva riportato che la dbt determinava un incremento della dr della dm dell8% [ 14 ]  . nelle pazienti affette da patologia unifocale la dbt ha avuto un alto tasso di dr , pari al 97 , 7% , avvicinandosi al 100% dellrm . 
 per i casi multifocali invece , la dbt ha ottenuto una dr 1134 radiol med ( 2013 ) 118 : 11191136 if we analyse the detection rate of the different imaging modalities , it should be noted that thanks to dbt we were able to diagnose and measure a larger number of lesions compared to dm and us . 
our data agree with those reported in a previous study , in which dbt caused an 8% increase in detection rate compared to dm [ 14 ]  . in patients with unifocal disease , dbt had a high detection rate , 97.7% , approaching the 100% rate of mri . 
for multifocal cases , by contrast , dbt obtained a detection rate of 77.8% , moderately lower than mri ( 93.6% ) , but higher than the other two conventional methods . 
this is due to the fact that some lesions not visible at dbt were visible at us examination , while in multifocal - multicentric cases dbt allowed the detection of more lesions compared to us . mri and dbt can provide different types of information about suspicious breast lesions , thanks to the use of contrast medium , mri is able to provide information about lesion vascularisation which dbt cannot provide . 
therefore , dbt seems to be able to play a major role in breast imaging and , according to our data , even in the preoperative staging of breast cancer [ 24 , 25 ]  . despite the good results in terms of dimensional accuracy and breast lesion detection demonstrated by dbt , compared to dm and us , we have to consider some limitations of our study . 
the retrospective review of the dm , dbt , us and mri images and the lesion measurements were performed by the same two radiologists who , although unaware of pathological size , were not blinded to the individual methods , so it cannot be excluded that one type of imaging may have partly inuenced the other ones . 
besides , the retrospective review of us images ( given the retrospective nature of the study , it was impossible to repeat the us measurements in real - time to verify that they were actually taken along the lesion long axis ) may have produced a not completely correct approximation of the measurements obtained with this modality . in our study , we did not establish the possible contribution of a computer - aided diagnosis ( cad ) system for mri in the evaluation of breast lesion size , as suggested by del 77 , 8% , modicamente pi bassa rispetto allrm ( 93 , 6% ) ma pi alta rispetto alle altre due metodiche convenzionali . 
 la differenza di dr tra dbt e rm per i casi multifocali risultata statisticamente signicativa ( p < 0 , 01 )  . lassociazione di dbt e us ha permesso di incrementare signicativamente la dr delle singole metodiche ( portandola al 96% ) permettendo quindi di recuperare un consistente numero di lesioni , avvicinandosi ai valori dellrm . 
 ci da imputarsi al fatto che una quota di lesioni non visibili alla dbt sono risultate visibili alla successiva indagine us , mentre in caso di multifocalit multicentricit la dbt ha permesso di rilevare pi lesioni rispetto allus . di fatto , la rm e la dbt possono fornire differenti tipi di informazioni riguardo le alterazioni mammarie , prima di tutto poich lrm , grazie allutilizzo del mezzo di contrasto , in grado di fornire informazioni sulla vascolarizzazione delle lesioni che la dbt non in grado di fornire . 
pertanto la dbt sembra in grado di inserirsi a pieno titolo nel novero delle tecniche idonee allo studio della mammella e per quanto valutato nel nostro studio anche nello staging pre - operatorio delle lesioni [ 24 , 25 ]  . nonostante i buoni risultati in termini di accuratezza nella valutazione dimensionale e nellindividuazione delle lesioni mammarie dimostrata dalla dbt , rispetto alla dm e allus , si deve tuttavia tener conto di alcuni limiti del nostro studio . 
infatti , la rivalutazione a posteriori delle immagini e la misurazione delle lesioni in dm , dbt , us e rm stata effettuata dagli stessi due radiologi che , bench non fossero a conoscenza dellestensione istologica delle neoplasie , non erano di fatto ciechi alle singole metodiche e pertanto non si pu escludere che un tipo di imaging possa aver in parte inuenzato laltro . 
anche il tipo di rivalutazione delle immagini ecograche ( per la natura stessa dello studio retrospettivo , non stato infatti possibile ripetere una misurazione ecograca in real - time , al ne di vericare che fosse stata eseguita lungo leffettivo asse maggiore della lesione ) pu aver determinato unapprossimazione non del tutto corretta delle misurazioni effettuate con questa metodica . nel nostro studio , non abbiamo considerato il possibile contributo di un sistema computer - aided diagnosis ( cad ) per rm nella valutazione delle dimensioni delle lesioni mammarie , come proposto nel lavoro di levrini et al . 
 further studies with larger patient populations are required to establish whether cad systems should be used extensively with mri , including for the estimation of lesion size . in conclusion , although dbt is superior to dm in the evaluation of tumour size , our results conrm that mri still remains the most accurate imaging technique in preoperative staging of breast cancer . 
gallbladder wall oedema was related to moderatesevere inammatory activity ( p < 0.05 ) , alanine transaminase ( alt ) ( p = 0.012 ) and aspartate aminotransferase ( ast ) ( p = 0.027 ) levels but not to brosis or other laboratory data , including serum quantitative dna for hepatitis b virus ( hbv ) , with the p = 0.1050.846. 
sessantasette pazienti in cui era stata fatta diagnosi clinica e istologica di chb e 18 soggetti sani senza alcuna storia di malattie epatiche sono stati sottoposti ad imaging rm addominale . 
si evidenziata una differenza statisticamente signicativa per la presenza di edema della parete colecisti tra i gruppi di grado 04 ( p = 0 , 000 ) , ma non tra i gruppi di grado 3 e 4 ( p = 0 , 729 )  . 
ledema della parete colecistica era correlato ad attivit inammatoria moderata - severa ( p < 0 , 05 ) , alanina transaminasi ( alt ) ( p = 0 , 012 ) e aspartato aminotransferasi ( ast ) ( p = 0 , 027 ) , ma non era correlato alla brosi o ad altri dati di laboratorio inclusi il dosaggio sierico del dna per il virus dellepatite b con valore di p compreso tra 0 , 105 e 0 , 846 . 
ledema della parete colecistica per i pazienti con chb pu essere dimostrato specicatamente tramite imaging con rm ed correlato con attivit radiol med ( 2013 ) 118 : 11021108 1103 keywords chronic hepatitis b magnetic resonance imaging gallbladder wall oedema inammation inammatoria epatica moderata - severa , alt e ast elevate , ma non con brosi parole chiave epatite b cronica imaging con risonanza magnetica edema della parete colecistica inammazione introduction materials and methods oedema of the gallbladder wall is often discovered in patients with various diseases , such as acute or chronic cholecystitis [ 13 ] , viral hepatitis [ 4 , 5 ] , hepatic failure [ 6 ] and acute poststreptococcal glomerulonephritis [ 7 ]  . 
because ndings of gallbladder wall oedema , as one pattern of gallbladder wall thickening on us , are nonspecic , the differential diagnosis of gallbladder disease in patients with thickened gallbladder wall can be difcult [ 810 ]  . 
computed tomography ( ct ) and magnetic resonance imaging ( mri ) , especially mri , have been used to evaluate gallbladder diseases [ 3 , 11 , 12 ]  . 
 the correlation of mri ndings and histologic specimens of gallbladder wall oedema on t2 - weighted imaging can suggest that the inner layer , with low signal intensity , represents intact mucosal and muscular layers , and the outer layer with high signal intensity represents oedematous subserosal layers [ 3 ]  . 
 chronic hepatitis b ( chb ) is one of the most common liver diseases , and infected individuals are at an increased risk of developing cirrhosis , liver failure and hepatocellular carcinoma ( hcc ) [ 1416 ]  . 
one study of acute hepatitis reveals that the necrosis and inammation of the liver parenchyma can lead to thickening of the gallbladder wall , representing an inammatory , reaction with hyperaemia in the serosal and muscular layers adjacent to the liver [ 10 ]  . 
 during our clinical practice , gallbladder wall oedema was also often found in patients with chb . a few studies describe image characteristics for gallbladder wall oedema on ct or mri [ 3 , 17 , 18 ]  . 
the purposes of our study were to characterise gallbladder wall oedema on mri and correlate these ndings with histopathology and laboratory data in patients with chb . patients this study was conducted in accordance with the guidelines of the institutional review board of our institution . 
between january 2005 and july 2010 , all consecutive inpatients with chronic hepatitis b virus ( hbv ) infection who underwent abdominal mri examination before antiviral treatment were selected retrospectively . 
selection criteria was a diagnosis of chb , with available pathology reports from the biopsy and clinical evaluation , including positive serum hepatitis b surface antigen for at least 6 months . 
patients with hepatic malignant diseases such as hcc or with other hepatobiliary diseases such as cholecystitis , hepatic abscess or cholangitis , or with other forms of hepatitis such as alcoholic hepatitis , viral hepatitis except hepatitis b and autoimmune hepatitis , or with systemic or abdominal diseases resulting in pathological gallbladder changes such as hepatic failure and acute glomerulonephritis , were excluded by appropriate clinical , laboratory and radiological investigations . 
all patients and controls were negative for anti - human immunodeciency virus antibody . all intact laboratory data of 67 inpatients had been collected within 3 days prior to or after the mri examination . 
 among data , total protein , albumin , albumin / globulin ratio , alanine aminotransferase ( alt ) , aspartate aminotransferase ( ast ) , alt / ast ratio , total bilirubin , cholinesterase , prothrombin time activity percentage ( pta ) , platelet and quantitative deoxyribonucleic acid ( dna ) for hbv in blood were noted . liver pathology experienced hepatologists performed the percutaneous liver biopsies in the right lobe of the liver using sonographic 1104 radiol med ( 2013 ) 118 : 11021108 guidance and an 18 - gauge spring - loaded biopsy device . 
all core biopsy samples , 1.5 cm in length , were obtained within 3 days after the mri examination and examined by the same pathologist , who was unaware of clinical , biochemical and instrumental data . 
histological diagnosis and hepatic inammation ( grade 04 , g0 - 4 ) and brosis ( stage 04 , s0 - 4 ) were assessed by a simplied system for scoring in chronic viral hepatitis according to scheuer and hbscher [ 19 , 20 ]  . mri technique fat - suppressed , all mri examinations were performed on a 1.5 - t scanner ( signa , ge healthcare , usa ) with 38 mt / m gradient subsystems and 120 - t m - 1 s - 1 gradient switch rates using a phasedarray torso coil . 
gadolinium diethylenetriaminepentaacetic acid ( gd - dtpa , magnevist ; schering , berlin , germany ; 0.1mmol / kg of body weight ) was administered intravenously at a rate of 3.0 ml / s with a power injector ( spectris mr injector system ; medrad , pittsburgh , pa , usa ) , followed by a 20 - ml saline solution ush . imaging analysis original data were transferred to the workstation ( advanced workstation 4.3 , sun microsystems )  . 
oedematous wall thickness for each patient was dened as a mean of the maximal and minimum distance from the exterior margin of the inner layer with low signal intensity , to the exterior margin of the outer layer with high signal intensity for the gallbladder body . statistical analysis quantitative data are presented as meanstandard deviation ( sd )  . 
all statistical analyses were performed with spss 13.0 for windows ( spss inc . , chicago , il , usa )  . results sample characteristics sixty - seven patients with chb , 52 men and 15 women ( age range , 1863 years ; mean age , 40.88.3 years ) and 18 healthy volunteers , 13 men and 5 women ( age range , 2463 years ; mean age , 42.411.4 years ) met inclusion criteria . 
the outer layer , which corresponded pathologically to oedematous subserosal layers , did not enhance on contrast - enhanced mri , but the inner radiol med ( 2013 ) 118 : 11021108 1105 fig . 
there was no discernible layering in the gallbladder wall without oedema on t2weighted or enhanced images , and no high signal intensity for the outer layer on t2 - weighted images . correlations with histopathology the average thickness of the oedematous wall for all 12 patients was 5.683.78 ( range , 2.213.6 ) mm ; in particular , 4.351.98 ( range , 2.57.8 ) mm for six patients with g3 and 7.024.81 ( range , 2.213.6 ) mm for six patients with g4 . 
there was a statistically signicant difference for the presence of gallbladder wall oedema among groups with g0g4 ( p = 0.000 , fishers exact test for rc table ) but not between groups with g3 and g4 ( p = 0.729 , fishers exact test )  . 
all patients were grouped into two new groups : a mild - disease group comprising g1 and g2 , and a moderateto - severe - disease group comprising g3 and g4 ( frequency of wall oedema in the moderatesevere group was 33.33% , 12 / 36 )  . 
there was a statistically signicant difference for the presence of gallbladder wall oedema between controls , mild and moderatesevere groups ( p = 0.000 , fishers exact test for rc table ) , between mild and moderatesevere groups ( p = 0.000 , fishers exact test ) and between controls and moderatesevere group ( p = 0.005 , fishers exact test )  . 
between the two groups , there were statistically signicant differences for alt ( t = 2.669 , p = 0.012 ) and ast ( t = 2.310 , p = 0.027 ) but not for total protein , albumin , albumin / globulin ratio , alt / ast ratio , total bilirubin , cholinesterase , pta , platelets or quantitative dna for hbv , with p values of 0.1050.846. 
there was no statistically signicant difference for the presence of gallbladder radiol med ( 2013 ) 118 : 11021108 1107 wall oedema between the two groups with g3 and g4 . 
thickness of gallbladder wall oedema was not correlated with hepatic inammation or brosis . the normal gallbladder wall is composed of four layers : mucosa , lamina propria , an irregular muscle layer and an adventitial coat of loose connective tissue covered partly with serosa . 
in the oedematous gallbladder wall , there was an intact mucosa and muscular layer corresponding to the thin inner layer of dark signal intensity , and oedematous subserosa corresponding to the thicker outer layer of high signal intensity on mr t2 - weighted images [ 3 ]  . 
the serosa was often shown as a thin striation of enhancement on the exterior margin of the outer layer . gallbladder wall oedema is often observed in patients with viral hepatitis [ 4 , 5 , 10 , 18 ] or other nonbiliary diseases [ 7 ]  . 
another is that necrosis and inammation of liver parenchyma causes oedema of the gallbladder wall , representing an inammatory reaction , with hyperaemia in the serosal and muscular layers adjacent to the liver . 
the possible pathophysiologic mechanism leading to oedema of the gallbladder wall in these diseases is due to elevated portal venous pressure , elevated systemic venous pressure , decreased intravascular osmotic pressure or a combination of these factors [ 22 ]  . 
our results support the hypothesis that gallbladder wall oedema is correlated with necrosis and inammation of liver parenchyma . we correlated gallbladder wall oedema with histopathology and laboratory data in patients with chb by using mri . 
 we found that gallbladder wall oedema discovered only in g3 or g4 patients was correlated with moderatesevere inammatory activity , elevated alt and ast , but not with brosis or other laboratory data , including serum hepatitis b viremia . 
there was a high specicity ( 100% ) but a low sensitivity ( 33.33% ) for diagnosing moderatesevere inammatory activity using gallbladder wall oedema in patients with chb on mri  . 
the thickness of gallbladder wall oedema was not correlated with hepatic inammation or brosis . one limitation of our study is the relatively small sample size of patients with gallbladder wall oedema . 
 in summary , gallbladder wall oedema for patients with chb can be specically demonstrated by mri and in our study was correlated with moderatesevere hepatic inammatory activity , elevated alt and ast , but not with brosis or other laboratory data , including serum hepatitis b viremia . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
this study was done to evaluate by direct comparison the image quality of magnetic resonance urography ( mru ) and computed tomography urography ( ctu ) and to assess the diagnostic condence of the two techniques in detecting urothelial malignancy in patients with haematuria materials and methods . 
there is a potential role for mru in urinary tract imaging , but as diagnostic condence in detecting urothelial malignancy is poorer than in ctu , it might be riassunto obiettivo . 
nella nostra serie luro - tc ha dimostrato una migliore visibilit delle strutture uroteliali ( p < 0 , 01 ) , con una condenza diagnostica maggiore rispetto alluro - rm ( area sotto la curva roc 0 , 994 versus 0 , 938 )  . 
vi un ruolo potenziale per luro - rm nellimaging del tratto urinario , ma dal momento che radiol med ( 2013 ) 118 : 11841198 1185 reserved for patients at low risk for malignancy and for evaluating obstructed patients . keywords ct urography mr urography haematuria urinary tract hydronephrosis la condenza diagnostica nella diagnosi di patologia neoplastica uroteliale inferiore a quella delluro - tc , potrebbe essere riservata ai pazienti con basso rischio neoplastico e per la valutazione dei paziente ostruiti . parole chiave uro - tc uro - rm ematuria via escretrice urinaria idronefrosi introduction introduzione haematuria is a common urological problem , accounting for a great number of urology referrals , and its prevalence ranges from 5% to 20% [ 1 ]  . 
although a precise consensus on managing haematuria has not yet been reached [ 2 ] , its evaluation constitutes an increasing workload for radiologists involved in urinary tract imaging [ 1 , 3 ]  . 
most guidelines still recommend intravenous urography ( ivu ) as a second - line test [ 4 ] , but its use has decreased in recent decades , and now it has been completely replaced by computed tomography urography ( ctu ) [ 57 ]  . 
it has been dened by the members of the ct urography working group of the european society of urogenital radiology ( esur ) as a diagnostic examination optimized for imaging the kidneys , ureters and bladder , that involves the use of multidetector ct ( mdct ) with thin - slice imaging , intravenous administration of a contrast medium , and imaging in the excretory phase [ 8 ]  . 
however ctu , especially when performed with a multiphase technique , is associated with high radiation doses according to the published data as high as 1035 msv , depending on the number of phases , indication and technical parameters used [ 9 , 10 ]  . 
for this reason , it is still important to investigate further techniques that can provide diagnostic effectiveness with no or less radiation exposure . magnetic resonance urography ( mru ) is a promising technique for studying the urinary tract , and it serves as an alternative imaging technique for children , pregnant women and patients with a contraindication to iodinated contrast media administration . 
nevertheless , it has not been widely adopted in clinical practice [ 6 ]  . mru can be performed by using heavily t2 - weighted sequences without contrast material to image the urinary tract as a static collection of uid ( static - uid mru ) or by using 3d t1 spoiled gradient - echo ( ge ) sequences performed during the excretory phase after administration of gadolinium - based contrast material ( excretory mru )  . several studies have shown the potential of mru in evaluating urinary tract diseases , but its sensitivity in detecting lematuria un sintomo urologico molto comune , responsabile di un elevato numero di consulti urologici , con una prevalenza che varia dal 5% al 20% [ 1 ]  . 
sebbene non esista ancora un preciso consenso sulla gestione del paziente con ematuria [ 2 ] , la sua valutazione costituisce un carico di lavoro in continuo aumento per i radiologi a cui viene richiesto di indagare il tratto urinario [ 1 , 3 ]  . 
vi sono linee guida che ancora raccomandano lurograa come esame di secondo livello [ 4 ] , ma il suo uso diminuito negli ultimi decenni e attualmente essa stata completamente sostituita dallurograa con tomograa computerizzata ( uro - tc ) [ 57 ]  . 
denita dai membri del gruppo di lavoro sulluro - tc della societ europea di radiologia urogenitale ( esur ) come un esame diagnostico ottimizzato per la visualizzazione di reni , ureteri e vescica , che richiede lutilizzo di unapparecchiatura multidetettore per lacquisizione di immagini a strato sottile e la somministrazione endovenosa di mezzo di contrasto , con acquisizione delle immagini in fase escretoria [ 8 ] , luro - tc rappresenta la modalit di imaging di scelta per il riconoscimento della patologia neoplastica maligna uroteliale . 
tuttavia essa espone il paziente ad unelevata dose di radiazione , in particolare se eseguita con tecnica multifasica , che pu raggiungere , in base ai dati di letteratura , i 1035 msv , con variazioni che dipendono dai parametri tecnici prescelti , dal numero di fasi e dal quesito clinico [ 9 , 10 ]  . 
 lurograa con risonanza magnetica ( uro - rm ) rappresenta una promettente tecnica per lo studio dellapparato urinario , ma attualmente riservata come alternativa per lo studio dei bambini , delle donne in gravidanza e dei pazienti con controindicazioni alla somministrazione di mezzo di contrasto iodato e non ancora stata introdotta abitualmente nella pratica clinica [ 6 ]  . 
 luro - rm pu essere eseguita con sequenze fortemente pesate in t2 , senza la somministrazione del mezzo di contrasto , per visualizzare la via escretrice come liquido sta1186 radiol med ( 2013 ) 118 : 11841198 urothelial malignancy has to be further investigated [ 6 , 11 , 12 ]  . 
two radiologists with experience in genitourinary imaging analysed image quality and blindly evaluated type , dimension and location of lesions recognisable in these patients and reported the condence level of the diagnosis for both examinations . 
a rst contrast medium bolus of 400 mgi / kg was injected at 2 ml / s , followed by a delay of 7 min before the second bolus of 200 mgi / kg injected at 2 ml / s . 
the nephrographicexcretory phase scan was acquired 100 s after beginning injection of the second bolus , with the following parameters : collimation 640.5 mm , pitch 0.828 , 120 kv , automatic current modulation based on the scout image with sure exposure software . mr urography mru studies were performed with a 1.5 - t system ( intera achieva , philips medical systems , best , the netherlands )  . 
 first , a t2 turbo spin - echo ( tse ) sequence and a 3d static - uid mru sequence were performed in the coronal uro - rm tico ( pielo - rm ) o mediante sequenze gradient echo ( ge ) tridimensionali pesate in t1 acquisite durante la fase escretoria dopo somministrazione di mezzo di contrasto a base di gadolinio ( uro - rm escretoria )  . molteplici lavori hanno dimostrato il potenziale dellurorm nella valutazione della patologia urologica , ma la sua sensibilit nel riconoscimento della patologia neoplastica uroteliale necessita di ulteriori studi [ 6 , 11 , 12 ]  . 
per quanto a nostra conoscenza , attualmente non esiste alcuno studio sistematico che abbia testato la condenza diagnostica delluro - rm nella valutazione dellematuria , pertanto scopo del nostro lavoro stato valutare la condenza diagnostica delluro - rm nel riconoscimento della patologia neoplastica uroteliale , mediante un confronto diretto con luro - tc . 
 materiali e metodi sono stati retrospettivamente identicati 35 pazienti con ematuria microo macroscopica sottoposti sia ad uro - tc che ad uro - rm , fra gennaio 2009 e ottobre 2010 . 
due radiologi con esperienza nellimaging genitourinario hanno analizzato la qualit dimmagine e valutato in cieco il tipo , le dimensioni e la localizzazione delle lesioni riconoscibili in questi pazienti , riportando quindi il livello di condenza diagnostica di entrambe le tecniche . 
dopo aver spiegato ai pazienti la natura dellesame , stato ottenuto un consenso informato . uro - tc tutti gli esami uro - tc sono stato condotti utilizzando unapparecchiatura tc a 64 strati ( aquilion 64 , toshiba medical systems , tokyo , giappone )  . 
in tutti i pazienti stata eseguita una preliminare scansione diretta a bassa dose , a 120 kv e con modulazione automatica della corrente , estesa dal polo superiore dei reni alla base vescicale . 
per la scansione contrastograca stato utilizzato il metodo split - bolus con una prima iniezione di mezzo di contrasto di 400 mgi / kg , a 2 ml / s ( iomeron 350 , bracco , milano , italia ) , seguita da una pausa di 7 minuti , e quindi da un secondo bolo di 200 mgi / kg a 2 ml / s . 
a t1 - weighted 3d ge excretory mru sequence in the coronal plane was performed with a delay of 10 m sequence parameters are summarised in table 1 . image analysis two radiologists analysed the upper , middle and lower calyces , pelvis and ureter on each side as well as the bladder , assessing overall quality of visualisation of each portion on a six - point scale ( 0 = absence of visualisation ; 1 = poor visualisation ; 2 = fair visualisation ; 3 = moderate visualisation ; 4 = good visualisation ; 5 = excellent visualisation ) using a modied version of the classication proposed by fry et al . 
radiologists were then asked to evaluate the images focusing on the calyces of the upper , middle and lower group , renal pelvis , lumbar , sacral and pelvic ureter on each side as well as the bladder , assigning independently a condence level in the diagnosis of urothelial malignancy according to a ve - grade scale ( 1 = denitely absent ; 2 = probably absent ; 3 = indeterminate ; 4 = probably present ; 5 = denitely present )  . 
ct and mr window settings were optimised according to reader experience and practice . statistical analysis comparison of ctu and mru image quality in the different portions of the excretory system was performed using chiatura a 1 , 5 t ( intera achieva , philips medical systems , best , olanda ) , utilizzando una bobina di supercie phased array ( sense - body )  . 
ai pazienti stato richiesto di vuotare la vescica immediatamente prima dellesame e di assumere 150 ml di mezzo di contrasto negativo per os per eliminare il segnale t2 dei uidi nel contesto delle anse intestinali . 
 luro - rm stata eseguita con sequenze pielo - rm ed escretorie . sono state acquisite preliminarmente una sequenza turbo spin - echo ( tse ) t2 pesata e una sequenza pielo - rm 3d sul piano coronale . 
quindi sono stati iniettati furosemide 0 , 1 mg / kg , somministrata per aumentare la distensione della via escretrice , e mezzo di contrasto a base di gadolinio 0 , 05 mmol / kg ( prohance , bracco , milano , italia )  . 
i parametri delle sequenze utilizzate sono riassunti nella tabella 1 . analisi delle immagini due radiologi hanno analizzato i calici superiori , medi ed inferiori , la pelvi renale e luretere di ciascun lato e la vescica , considerando la qualit complessiva di visualizzazione di ciascuna porzione mediante una scala a sei punti ( 0 = visualizzazione assente ; 1 = scarsa visualizzazione ; 2 = mediocre visualizzazione ; 3 = discreta visualizzazione ; 4 = buona visualizzazione ; 5 = eccellente visualizzazione ) , utilizzando una versione modicata della classicazione proposta da fry et al . 
i due radiologi hanno quindi valutato le immagini , focalizzando lattenzione sui calici del gruppo superiore , medio ed inferiore , la pelvi renale , luretere lombare , sacrale e pelvico di ciascun lato e la vescica ed hanno assegnato indipendentemente un livello di condenza per la diagnosi di patologia neoplastica uroteliale secondo 1188 radiol med ( 2013 ) 118 : 11841198 fig . 
 sia luro - tc che luro - rm illustrano la normale anatomia del tratto urinario , con buona rappresentazione anche delle strutture pi minute , quali i calici . the wilcoxon matched - pairs test . 
receiver - operator characteristic ( roc ) curve analysis was employed to assess overall condence of diagnosis of urothelial malignancy using the response from the ve - grade scale [ 14 ]  . 
the areas under the curve ( auc ) were calculated using dedicated software ( jrocfit , johns hopkins university , baltimore , md , usa ) and compared with the method described by delong et al . 
one patient had been previously treated with surgical removal of the left kidney and ureter ; two patients had had a cystectomy with removal of the pelvic ureter on one side . 
i valori di nestra e livello per la tc e la rm sono stati ottimizzati dal singolo lettore , in accordo con la propria pratica ed esperienza . analisi statistica il confronto fra la qualit dimmagine in uro - tc ed in urorm nei diversi tratti del sistema escretore stato eseguito mediante il test di wilcoxon per dati appaiati . 
lanalisi delle curve receiver operator characteristic ( roc ) stata impiegata per valutare la condenza diagnostica generale nella diagnosi di patologia neoplastica uroteliale utilizzando i risultati della valutazione secondo la scala a cinque punti [ 14 ]  . 
larea sotto le curve stata calcolata utilizzando un software dedicato ( jrocfit , johns hopkins university , baltimore , md . , usa ) e comparata mediante il metodo descritto da delong et al . 
ricostruzione mip a strato spesso , con rimozione elettronica dellosso , delluro - tc ( a ) e delluro - rm ( b )  . table 2 average subjective image quality at computed tomography urography ( ctu ) and magnetic resonance urography ( mru ) for two radiologists . 
in fact , the highest score was assigned in 263 / 378 portions of the urinary tract in ctu but in only 155 / 378 portions in mru by reader 1 , and in 246 and 145 / 378 , respectively , by reader 2 . 
considrisultati qualit dimmagine per la valutazione della qualit sono state considerati 378 segmenti del tratto urinario ( calici del gruppo superiore , medio ed inferiore , pelvi ed uretere di ciascun lato e vescica ) in 35 pazienti . 
a uro - rm in fase escretoria : gli artefatti da respiro ostacolano il riconoscimento di un difetto di riempimento in un calice del gruppo superiore ( freccia )  . 
b luro - tc eseguita nello stesso paziente permette , invece , di individuare agevolmente un calcolo misto ( freccia )  . ering the different excretory portions , mru image quality was signicantly lower than that of ctu at the level of calyces ( 151 / 207 segments scored as 5 in ctu and 84 / 207 in mru by reader 1 , and 154 in ctu and 80 / 207 in mru by reader 2 ) ; in the other tracts , the difference was not statistically signicant . 
in these series , 21 neoplastic lesions were present , as conrmed by subsequent pathological examinations , in some cases extending over more than one region ( table 3 ) ; 29 / 514 regions were positive for malignancy and 485 / 514 were negative . 
considering all kinds of urinary tract disease ( two chronic inammations , one ureteropelvic junction syndrome , one ureterocele , four stones , two brotic stenosis ) , 38 / 514 were positive ( table 4 )  . 
considerando i diversi tratti del sistema escretore urinario la qualit dimmagine in uro - tc stata signicativamente migliore a livello dei calici ( 151 / 207 segmenti con punteggio 5 in uro - tc e 84 / 207 in uro - rm per il lettore 1 , 154 in uro - tc e 80 in uro - rm per il lettore 2 ) , mentre negli altri tratti la differenza non stata statisticamente signicativa . 
as to false negatives , two small lesions and two cases of wall thickening were not visible at mru , and reader 1 also overlooked a tumour recognisable only as an alteration of bladder shape . 
the two reviewers considered uninterpretable a large number of segments at sono stata riscontrate 21 lesioni neoplastiche uroteliali , in alcuni casi con estensione a pi tratti ( tabella 3 ) ; 29 / 514 tratti erano positivi per neoplasia e 485 / 514 erano negativi . 
 considerando tutti i tipi di patologia uroteliale ( 2 casi di inammazione cronica , una sindrome del giunto , un ureterocele , 4 casi di litiasi , 2 casi di stenosi cicatriziale ) 38 / 514 tratti sono risultati positivi ( tabella 4 )  . i risultati delle curve roc sono riassunti nella figura 4 e nella tabella 5 . 
la concordanza inter - osservatore stata buona per entrambe le modalit di imaging ( valore di k = 0 , 62 ) , mentre la differenza fra le aree sotto le curve dei due lettori non si dimostrata statisticamente signicativa . 
 per entrambi i radiologi la capacit diagnostica dellurorm stata inferiore a quella delluro - tc e la differenza 1192 radiol med ( 2013 ) 118 : 11841198 1 - specicity 1 - specicity fig . 
the area under the roc curve is 0.994 for ctu ( continuous line ) and 0.938 for mru ( dashed line ) for reader 1 and 0.976 for ctu and 0.907 for mru for reader 2 . 
 mru , 83 and 75 , respectively , due to poor image quality ; ctu showed fewer noninterpretable segments ( 41 and 62 , respectively ) , most due to incomplete distention or opacication of the urinary tract . evaluation of the ten patients with obstructed and nonexcreting kidney showed a statistically signicant shift of better overall image quality from ctu to mru ( p < 0.01 ) for both readers . 
considering the different excretory portions , subjective image quality of mru was signicantly better than image quality of ctu at the level of the calyces and ureters for reader 2 ; difference was not signicant at these levels for reader 1 . 
lassenza di patologia neoplastica stata correttamente identicata in 403 / 485 e 404 / 485 tratti rispettivamente sulla base delle immagini di uro - rm e in 444 / 485 e 422 / 485 tratti in uro - tc . 
per quanto riguarda i falsi negativi , 2 piccole lesioni e 2 ispessimenti di parete non sono stati dimostrati dalle immagini di uro - rm e al lettore 1 sfuggito anche una neoplasia riconoscibile solo come alterazione della morfologia vescicale . 
i due lettori hanno considerato non interpretabili un gran numero di tratti in uro - rm , 83 e 75 rispettivamente , a causa della scarsa qualit dimmagine , mentre in uro - tc il numero di tratti dubbi stato inferiore ( 41 e 62 rispettivamente ) , per lo pi dovuti ad unincompleta distensione od opacizzazione del sistema escretore . la valutazione dei 10 pazienti che si presentavano con sistema escretore ostruito o non funzionante ha dimostrato uno spostamento della migliore qualit dimmagine dalla tc verso la rm , in modo statisticamente signicativo ( p < 0 , 01 ) per entrambi i radiologi . 
la concordanza inter - osservatore si dimostrata buona per luro - rm e discreta per luro - tc ( valore di k = 0 , 69 e 0 , 43 rispettivamente )  . 
nella valutazione dei singoli tratti del sistema escretore , la qualit dimmagine soggettiva stata signicativamente migliore in uro - rm a livello dei calici e degli ureteri per il lettore 2 , mentre la differenza non si dimostrata statisticamente signicativa a questi livelli per laltro radiologo . 
tuttavia la dimensione del campione troppo piccola per eseguire un confronto fra la condenza diagnostica delluro - tc e delluro - rm . discussione numerosi studi hanno illustrato il grande potenziale delluro - rm per lo studio del apparato urinario [ 6 , 11 , 12 , 16 ]  . 
a la ricostruzione coronale delluro - tc dimostra chiaramente la presenza di un ispessimento di parete del calice inferiore , associato a multipli minuti difetti di opacizzazione ( freccia )  . 
a un difetto di riempimento chiaramente visibile nel contesto di un calice del gruppo superiore ( freccia ) nellimmagine di uro - rm escretoria , ma la relativa insensibilit alle calcicazioni non permette una diagnosi di natura . 
however , the size of this sample is too small for an effective comparison between the diagnostic condence of ctu and mru . discussion several studies show a large potential of mru for urinary tract imaging [ 6 , 11 , 12 , 16 ]  . 
it represents an appealing alternative to ctu in haematuria evaluation thanks to the absence of radiation exposure and the possibility of urinary tract depiction without the use of contrast material in staticuid sequences . 
patients with microscopic haematuria have a relatively low risk of malignancy if young ( < 50 years for men and < 60 years for women ) [ 1 ]  . previous studies demonstrate that mru can recognise 74% of small nonobstructing carcinomas [ 12 ] and can detect neoplastic causes of urinary tract obstruction with an accuracy of 88% [ 1719 ]  . 
in our study , these data are conrmed , as mru detected malignancy of the urinary tract with a high diagnostic condence ( roc area 0.93 ) , recognising 82.7% of the tumours , with an accuracy of 83.5%. 
i pazienti pi giovani ( < 50 anni per gli uomini e < 60 anni per le donne ) con microematuria presentano invece un rischio neoplastico relativamente basso [ 1 ]  . studi precedenti hanno dimostrato che luro - rm in grado di riconoscere il 74% dei piccoli tumori uroteliali non ostruenti [ 12 ] e pu dimostrare la causa neoplastica di ostruzione con unaccuratezza pari all88% [ 1719 ]  . 
il nostro studio conferma questi dati , infatti luro - rm ha riconosciuto la patologia neoplastica con unelevata condenza diagnostica ( area sotto la curva roc pari 0 , 93 ) , individuando l82 , 7% dei tumori , con unaccuratezza dell83 , 5% . 
 tuttavia studiando i pazienti con luro - tc la condenza diagnostica risultata maggiore , con un riconoscimento dell89 , 6% delle stesse lesioni , con unaccuratezza del 91 , 8% ( area sotto la curva roc 0 , 99 )  . questa differenza dovuta ad alcuni limiti intrinseci della risonanza magnetica . 
innanzitutto la risoluzione spaziale minore rispetto alla tc e perci i tumori a cellule transizionali , di dimensioni anche millimetriche , possono essere misconosciuti , come accaduto in due pazienti della nostra casistica . 
inoltre luro - rm relativamente insensibile alle calcicazioni , con una conseguente scarsa condenza diagnostica nella differenziazione fra calcoli e difetti di riempimento di natura neoplastica , a meno che non si riesca a dimostrare lenhancement delle lesioni o lassenza di contatto con la parete . 
in pi le capacit panoramiche della tc radiol med ( 2013 ) 118 : 11841198 1195 table 6 average subjective image quality at computed tomography urography ( ctu ) and magnetic resonance urography ( mru ) in hydronephrotic patients . 
first , spatial resolution is lower than that of ct , and millimetric localisation of transitional cell carcinoma could thus be missed , as happened for two patients in our series . 
moreover , mru is relatively insensitive to calcications , with consequent poor diagnostic condence in differentiating a stone from a neoplastic lling defect , unless contrast enhancement is demonstrated with other focused sequences or the lling defect is not contiguous to the urinary wall . 
moreover , the panoramic capabilities of ct allow diagnosis of malignancies presenting with either wall thickening and or a lling defect , whereas both staticuid and excretory sequences offer only lumen depiction . 
 last , it is more difcult to obtain diagnostic - quality images with mru compared with ctu , and in fact , the diagnostic condence of mru is especially affected by the presence of noninterpretable segments , particularly at the calyceal level . 
nevertheless , ctu , depending on contrast medium excretion , cannot depict the urinary tract of obstructed patients , whereas dilated calyces and ureters are well delineated by static - uid mru , allowing not only recognition of the site of obstruction , where dynamic sequence could be focused , but also exclusion of synchronous lesions . consentono di riconoscere sia le neoplasie che determinano un difetto di riempimento sia quelle che si presentano con un ispessimento di parete , mentre sia la pielo - rm che luro - rm escretoria offrono solo una visualizzazione del lume urinario . inne , pi difcile ottenere immagini di qualit diagnostica in uro - rm che in uro - tc ed infatti la condenza diagnostica in uro - rm ridotta soprattutto dalla presenza di un elevato numero di tratti indeterminati , in particolare a livello caliceale . 
gli artefatti da movimento e da respiro ostacolano la visualizzazione della via escretrice , mentre anche nei pazienti poco collaboranti limaging in tc risulta di qualit diagnostica . daltro canto luro - tc , dipendendo dallescrezione del mezzo di contrasto , non in grado di visualizzare in modo ottimale la via escretrice dei pazienti ostruiti , mentre i calici e gli ureteri dilatati vengono ben delineati dalla pielorm , permettendo non solo di riconoscere la sede dellostruzione , dove si pu focalizzare una sequenza dinamica , ma anche di escludere la presenza di lesioni sincrone a monte . 
 questo studio presenta un limite importante : abbiamo considerato solamente la pielo - rm e la sequenza di uro - rm escretoria , mentre anche altre sequenze avrebbero potuto essere utili per indagare la causa di ematuria , come sottolineato da altri lavori [ 12 , 20 ]  . 
a static - uid mru allows good visualisation of the site of obstruction ( arrow ) and of the left dilated ureter , with a lling defect not in contact with the ureter wall above the obstruction . 
in urotc la lesione ostruente ben riconoscibile nellimmagine assiale ( freccia in d ) e nella ricostruzione mpr sul piano coronale ( freccia in e ) , mentre non escludibile con certezza la presenza di lesioni sincrone a monte . 
 this study has a major limitation : we considered only static - uid and excretory mru sequences , whereas other sequences could also have been useful in studying haematuria , as depicted by other studies [ 12 , 20 ]  . 
in our study , ctu was performed with a split - bolus technique , which granted both nephrographic and excretory information in a single scan , whereas both static - uid and excretory mru show only the urinary tract lumen . 
additional sequences could be performed to improve sensitivity in recognising wall thickening and pathological enhancement ; however , these would still be unable to afford the same spatial resolution as ctu . stata eseguita con una tecnica split - bolus , che garantisce in una singola scansione sia informazioni nefrograche che escretorie , mentre sia la pielo - rm che luro - rm escretoria dimostrano solo il lume della via escretrice . 
per migliorare la sensibilit nel riconoscimento degli ispessimenti di parete e degli enhancement patologici , potrebbero essere eseguite ulteriori sequenze , ma che comunque non potrebbero garantire la stessa risoluzione spaziale delluro - tc . nel passato la risonanza magnetica rappresentava unalternativa per lo studio dei pazienti con insufcienza renale che necessitavano di uno studio contrastograco , ma radiol med ( 2013 ) 118 : 11841198 1197 mr imaging once represented an alternative modality when a contrast - enhanced study was needed in patients with renal impairment , but the association between gadoliniumbased contrast material administration and nephrogenic systemic brosis reduced this indication , and so the risks and benets of mru examination should be carefully assessed for each patient [ 2022 ]  . 
 in conclusion , although further investigation is needed in larger populations , our study suggests that ctu has a higher detection rate for urothelial malignancy than does mru and therefore should be preferred for aged patients presenting with gross haematuria , who are at high risk for malignancy , as its higher diagnostic performance certainly balances the risk of radiation exposure . 
on the other hand , mru is a useful imaging modality in evaluating patients with obstructed or poorly functioning kidney regardless of the malignancy risk and potentially might have a role when investigating young patients with microhaematuria , who are at low risk for malignancy [ 1 ] and in whom radiation exposure is an important limiting factor . lassociazione riscontrata fra la brosi nefrogenica sistemica e il mezzo di contrasto a base di gadolinio ha ridotto questa indicazione e perci il bilancio fra rischio e benecio dellesame uro - rm deve essere attentamente analizzato per ciascun paziente [ 2022 ]  . in conclusione , sebbene siano necessari ulteriori studi su popolazioni pi ampie , il nostro lavoro indica una maggiore capacit di riconoscimento della patologia neoplastica uroteliale delluro - tc rispetto alluro - rm e perci la prima deve essere preferita nei pazienti anziani con ematuria macroscopica , ad elevato rischio neoplastico , dal momento che la sua capacit diagnostica pi elevata certamente bilancia il rischio derivante dallesposizione a radiazioni ionizzanti . 
daltra parte luro - rm unutile modalit di imaging per la valutazione dei pazienti ostruiti o con scarsa funzionalit escretoria , indipendentemente dal rischio neoplastico , e potrebbe rivestire un ruolo nello studio dei pazienti giovani con microematuria , a basso rischio neoplastico [ 1 ] , nei quali lesposizione a radiazioni ionizzanti rappresenta un importante fattore limitante . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
twelve patients ( 13 wrists ) underwent surgery for scapholunate dissociation and were followed up with clinical ( visual analogue scale , mayo wrist score , patient - rated wrist evaluation , and disabilities of the arm , shoulder , and hand ) and radiological assessment ( conventional radiography and ct arthrography )  . 
our results show that mdct arthrography has the same value as conventional radiography in the evaluation of standard parameters ( scapholunate gap , scapholunate angle , radiolunate angle , capitolunate angle , carpal height index ) , but in addition provides an accurate delineation of the fcr tendon graft , allowing riassunto obiettivo . 
dodici pazienti ( 13 polsi ) operati per stabilizzazione in dsl ; follow - up a 47 , 2 mesi mediante valutazione clinica ( visual analogue scale vas , mayo wrist score , patient - rated wrist evaluation prwe e disabilities of the arm , shoulder and hand scale dash ) e radiologica ( rx e artro - tc )  . 
i criteri radiograci analizzati sono stati : lintervallo scafo - lunato , langolo scafo - lunato , langolo radio - lunato , langolo capitolunato e lindice di altezza del carpo . 
i nostri risultati mostrano che lartro - tc ha lo stesso valore della radiograa nella valutazione dei parametri standard ( intervallo scafo - lunato , angolo scafolunato , angolo capitato lunato , angolo radio - lunato , indice di altezza carpale ) e consente inoltre lidenticazione del neolegamento permettendo la differenziazione di spessore , direzione e grado di tensione . 1158 radiol med ( 2013 ) 118 : 11571170 differentiation of its thickness , direction and degree of tension . parole chiave polso artro - tc instabilit carpale stabilizzazione scafo - lunata chirurgia del polso keywords wrist mdct arthrography carpal instability scapholunate stabilization wrist surgery introduction introduzione the wrist is a complex anatomical structure made up of several intercarpal joints allowing articular motion in the different spatial planes [ 1 ]  . 
carpal instability results from a disturbance of the static and dynamic balance of forces at the wrist under conditions of normal daily living , and is caused by alterations in the ligament structures or lesions to the carpal bones [ 2 , 3 ]  . 
the term dynamic instability refers to a deformity which normally arises during motion only , whereas static instability refers to a condition which is also present with the wrist at rest [ 3 , 4 ]  . the scapholunate ( sl ) and lunotriquetral ( lt ) interosseous ligaments are the main causes of carpal instability , and scapholunate dissociation ( sld ) , which may present as an isolated condition or associated with radial or scaphoid fractures , is the most important pattern of carpal instability [ 57 ]  . 
if complete tear of the scapholunate ligament is associated with injury to the extrinsic ligaments , both the scaphoid and lunate are malaligned even at rest , giving rise to a static pattern of sld , whereas the dynamic pattern can only be detected under stress conditions [ 710 ]  . the treatment of sld remains controversial , with several surgical solutions being proposed , including scaphotrapezial or capitate - scaphoid arthrodesis , capsulodesis , tenodesis and ligament repair [ 1114 ]  . 
in 1995 , brunelli described a surgical procedure for the treatment of sld associated with scaphoid subluxation and rotation , which consisted of tenodesis using the exor carpi radialis ( fcr ) tendon [ 15 ]  . 
in the original report , a strip of fcr was passed dorsally through the scaphoid and secured to the radius ; in 1998 wrightington modied brunellis procedure by xing the tendon strip on the dorsal aspect of the lunate ( modied brunelli - stanley procedure ) [ 1618 ]  . 
multidetector computed tomography ( mdct ) following joint distension with contrast material ( ct arthrography ) , with its high spatial resolution , is a valuable tool for the diagnosis and assessment of a wide range of joint disorders [ 22 ]  . 
the aim of this study was to evaluate the outcome of patients with sld treated with brunelli - stanley tenodesis and assess the role of ct arthrography for the follow - up by comparing the results with those of conventional radiography , considil polso una struttura anatomica complessa , costituita da diverse articolazioni intercarpali che consentono movimenti articolari nei diversi piani dello spazio [ 1 ]  . 
linstabilit carpale secondaria a un disturbo nel bilancio delle forze in fase statica e dinamica del polso in condizioni di normale attivit ed determinata da alterazioni delle strutture legamentose o da lesioni delle ossa carpali [ 2 , 3 ]  . 
si utilizza la denizione instabilit dinamica in presenza di una deformit che insorge solamente durante il movimento , mentre si denomina instabilit statica la presenza del disturbo anche in condizioni di riposo funzionale [ 3 , 4 ]  . i legamenti scafo - lunato ( sl ) e luno - piramidale ( lt ) sono i legamenti interossei maggiormente responsabili della stabilit : il pi importante pattern di instabilit carpale rappresentato dalla dissociazione scafo - lunata ( dsl ) , che pu presentarsi come patologia isolata o in associazione a fratture radiali o scafoidee [ 57 ]  . 
se la rottura completa del legamento scafolunato associata a lesione dei legamenti estrinseci , sia lo scafoide che il semilunare sono disallineati gi a riposo ( fase statica del dsl ) , mentre la fase dinamica della dsl rilevabile solo in condizioni di stress [ 710 ]  . il trattamento della dsl ancora controverso : in letteratura sono state proposte diverse soluzioni chirurgiche tra cui lartrodesi scafo - trapezoidale o scafo - capitata , la capsulodesi , la tenodesi e la legamentoplastica [ 1114 ]  . 
nel 1995 brunelli ha descritto una procedura chirurgica per il trattamento della dsl associata a sublussazione e rotazione dello scafoide che prevedeva una tenodesi con il tendine essore radiale del carpo ( frc ) [ 15 ]  . 
nella descrizione originale , un lembo di frc veniva portato dorsalmente attraverso lo scafoide e ssato al radio ; nel 1998 wrightington ha importato una modica allintervento di brunelli ssando il lembo di tendine dorsalmente nel semilunare ( intervento di brunelli - stanley modicato ) [ 1618 ]  . il follow - up post chirurgico nei vari lavori riportati in letteratura menziona unicamente lutilizzo della radiograa convenzionale [ 1921 ]  . 
la tomograa computerizzata multidetettore ( tcmd ) dopo distensione articolare con mdc ( artro - tc ) , grazie alla sua elevata risoluzione spaziale , uno strumento prezioso per la diagnosi e la valutazione di un ampio spettro di disturbi articolari [ 22 ]  . 
lo scopo del nostro lavoro la valutazione delloutcome in pazienti con dsl trattata con tenodesi ( brunelli - stanley ) e la descrizione del ruolo dellartro - tc nel follow - up , confrontando i radiol med ( 2013 ) 118 : 11571170 1159 ered the gold standard for the evaluation of the postoperative wrist [ 23 ]  . suoi risultati con quelli dellesame radiograco , considerato gold standard per la valutazione del polso operato [ 23 ]  . materials and methods materiale e metodi brunelli - stanley tenodesis was performed on 13 wrists ( nine dominant , four nondominant ) in 12 consecutive patients ( 11 male , one female ; mean age , 37 years ; range , 2352 ) affected by sld . 
 patients were excluded from the study if they had a history of previous wrist surgery . the preoperative diagnostic work - up consisted of a complete radiographic study in all cases , with standard views and three dynamic views . 
patients were followed up for 47.2 months ( range , 1675 months ) by means of clinical and radiological assessment of the wrist . clinical assessment the presence of wrist pain was assessed by using a visual analogue scale ( vas ) before and after surgery . 
wrist function was assessed with the mayo wrist score [ 25 ] , the prwe ( patient - rated wrist evaluation ) [ 26 ] and dash ( disability of the arm , shoulder and hand ) questionnaires [ 27 ]  . 
 radiological assessment preoperative imaging preoperative conventional radiography of the affected wrist was obtained in the two standard views ( anterior - posterior and latero - lateral in neutral position ) and two stress views ( anterior - posterior and latero - lateral with clenched st and supinated forearm )  . postperative imaging sono stati trattati consecutivamente 13 polsi ( 9 polsi dominanti , 4 polsi non dominanti ) in 12 pazienti ( 11 maschi , 1 femmina ) con et media di 37 anni ( range 2352 anni ) con dsl , mediante tenodesi secondo brunelli modicata stanley . 
allesame clinico il test di watson [ 24 ] era positivo in tutti i polsi ; il tempo medio intercorso tra il trauma e lintervento chirurgico stato di 10 , 5 mesi ( range 126 mesi )  . 
il follow - up stato di 47 , 2 mesi ( range 1675 mesi ) e ha previsto la valutazione clinica e radiologica del polso . valutazione clinica la presenza di dolore al polso stata valutata utilizzando una scala analogica visiva ( vas ) prima e dopo lintervento chirurgico . 
la funzionalit del polso stata valutata mediante il mayo wrist score [ 25 ] e completata utilizzando il questionario prwe ( patient - rated wrist evaluation ) [ 26 ] e il questionario dash ( disability of the arm , shoulder and hand ) [ 27 ]  . 
following disinfection of the skin , 34 ml of appropriately diluted iodinated contrast material ( iomeron 250 mg / ml , bracco , italy ) was injected into the radiocarpal joint under sterile conditions , using a 24 g needle . 
 a small eld of view ( fov100 mm ) was selected to achieve a voxel size of approximately 0.2 mthe ct arthrography images were assessed for the same parameters considered on conventional radiography ( scapholunate gap , scapholunate angle , radiolunate angle , capitolunate angle , carpal height index )  . 
i criteri radiograci valutati sia ai radiogrammi pre - intervento che post - intervento sono stati : lintervallo scafo - lunato , misurato sul radiogramma antero - posteriore in posizione neutrale e sul radiogramma antero - posteriore in posizione di stress tra il punto medio della faccetta mediale dello scafoide e il punto medio della faccetta laterale del semilunare , espresso in millimetri [ 28 , 29 ] ; langolo scafo - lunato per valutare linstabilit tra scafoide e semilunare , misurato sul radiogramma laterolaterale in posizione neutrale e considerato patologico se > 80 [ 30 ] ; langolo radio - lunato per valutare la presenza di uninstabilit dorsale del segmento intermedio ( disi ) misurato sul radiogramma latero - laterale in posizione neutrale e considerato patologico se > 15 [ 31 , 32 ] ; langolo capito - lunato per valutare la presenza di uninstabilit dorsale del segmento intermedio ( disi ) , misurato sul radiogramma in posizione neutrale valori normali 015 [ 29 ] ; lindice di altezza del carpo , calcolato come coefciente di nattras ( rapporto tra laltezza del carpo e laltezza del capitato ) , come misura di un eventuale collasso carpale ( range : 0 , 540 , 03 mm ) [ 33 ]  . le misurazioni sui radiogrammi pre - trattamento sono state eseguite da un singolo medico chirurgo specialista in radiodiagnostica ( eg ) , mentre quelle sui radiogrammi post - trattamento sono state valutate da un secondo medico chirurgo specialista in radiodiagnostica ( dm )  . liter diagnostico post - intervento stato completato in 9 pazienti su 12 con lesecuzione di artro - tc di polso . 
sono stati iniettati in condizioni sterili , con ago 24 g , 34 ml di mezzo di contrasto iodato opportunamente diluito ( iomeron 250 mg / ml , bracco , italia ) nellarticolazione radio - carpica . 
 un piccolo campo di vista ( fov~100 mm ) stato selezionato per raggiungere una dimensione dei voxel di circa 0 , 2 m nelle immagini di artro - tc sono stati valutati i medesimi parametri considerati ai radiogrammi convenzionali ( intervallo scafo - lunato , angolo scafo - lunato , angolo radiolunato , angolo capito - lunato , indice di altezza del carpo )  . 
statistical signicance was set at a value of p < 0.05. il polo prossimale dello scafoide , misurato in millimetri nelle ricostruzioni coronali ; spessore dellemitendine di frc ( flexor carpi radialis ) a livello del foro di uscita dorsale del tunnel osseo e a livello dellancoraggio allancoretta o al semilunare , misurati in millimetri nelle ricostruzioni sagittali ; integrit e grado di tensione dellemitendine di frc ; segni di degenerazione articolare . le misurazioni sulle immagini artro - tc sono state eseguite da un singolo medico chirurgo specialista in radiodiagnostica , il medesimo che ha eseguito le misurazioni sui radiogrammi pre - trattamento ( eg )  . 
sono stati impiegati specici test statistici per il calcolo di medie , frequenze , percentuali e analisi comparativa dei dati ottenuti , tra cui lutilizzo del t - test di student . 
 2 , 5 10 , 5 6 , 5 3 , 5 21 , 6 7 , 5 3 , 3 8 , 3 6 , 6 1 , 6 vas , visual analogue scale ; prwe , patient - rated wrist evaluation ; dash , disabilities of the arm , shoulder , and hand ; mayo , mayo wrist score ; pre , before treatment ; post , after treatment vas , visual analogue scale ; prwe , patient - rated wrist evaluation ; dash , disabilities of the arm , shoulder , and hand ; mayo , mayo wrist score ; prima , prima del trattamento ; dopo , dopo trattamento 1162 radiol med ( 2013 ) 118 : 11571170 radiol med ( 2013 ) 118 : 11571170 1163 fig . 
lesame comparativo mostra lassenza di una signicativa differenza tra il valore dello spazio scafo - lunato misurato sui radiogrammi convenzionali e quello misurato sulle ricostruzioni mpr dellartro - tc prima dellintervento e al follow - up . 
the mean scores at clinical assessment were 7 ( range , 025 ) on the prwe questionnaire , 5.9 ( 021 ) on the dash questionnaire , and 80 ( range , 6095 ) on the mayo wrist score . comparative analysis : conventional radiology vs . 
si osservata una riduzione statisticamente signicativa del dolore post - intervento ( p < 0 , 0001 , deviazione standard tra le due medie di 0 , 5 )  . 
al follow - up lintervallo scafo - lunato ( sl ) medio risultato di 2 , 21 mm ( range : 1 , 54 ) nelle proiezioni in rest e 2 , 85 mm ( range 1 , 55 ) nelle proiezioni in stress . 
la valutazione statistica ha dimostrato una signicativit nella riduzione dellampiezza dellintervallo scafolunato ai radiogrammi in rest ( p < 0 , 0001 , deviazione standard = 0 , 3 ) e ai radiogrammi in stress ( p = 0 , 015 , deviazione standard = 0 , 5 )  . 
lanalisi dei dati misurati ai radiogrammi in rest e i valori misurati alle immagini artro - tc in posizione neutra non hanno evidenziato una differenza statisticamente signicativa tra la radiograa convenzionale e lartro - tc ( p = 0 , 4 , deviazione standard = 0 , 2 )  . 1164 radiol med ( 2013 ) 118 : 11571170 fig . 
lesame comparativo mostra lassenza di una signicativa differenza tra il valore dellangolo scafo - lunato misurato sui radiogrammi convenzionali e quello misurato sulle ricostruzioni mpr dellartro - tc prima dellintervento e al follow - up . 
the difference between the preand postoperative values of the sl angle was not statistically signicant ( p = 0.58 , standard deviation = 6.5 ) , nor was the difference ( p = 0.22 , standard deviation = 5.14 ) between the values measured at conventional radiography and ct arthrography . radiolunate angle the preoperative radiolunate ( rl ) angle was 12.3 ( range , 627 ) ; at follow - up it was 8.6 ( range , 220 ) on radiography and 6.02 ( range , 018 ) on the multiplanar ct reconstructions . 
la differenza tra i valori angolari sl pre - operatori e post - operatori non risultata statisticamente signicativa ( p = 0 , 58 , deviazione standard = 6 , 5 ) , cos come non si osservata una differenza statisticamente signicativa ( p = 0 , 22 , deviazione standard = 5 , 14 ) tra i valori ottenuti in radiologia tradizionale e quelli calcolati allartro - tc . angolo radio - lunato prima della chirurgia langolo radio - lunato ( rl ) era di 12 , 3 ( range 627 ) ; al follow - up di 8 , 6 ( range 220 ) e di 6 , 02 ( range 018 ) nelle ricostruzioni mpr . 
la differenza tra i gradi radio - lunato ( rl ) pre - operatori e i gradi rl post - operatori non risultata statisticamente signicativa ( p = 0 , 25 , deviazione standard = 3 , 03 )  . 
analysis of the data prima del trattamento allesame radiograco langolo cl era di 15 , 2 ( range 336 ) ; al follow - up radiograco era di 11 , 6 ( range 220 ) e nelle ricostruzioni mpr di 11 angolo capitato - lunato radiol med ( 2013 ) 118 : 11571170 1165 fig . 
lesame comparativo mostra lassenza di una signicativa differenza tra il valore dellangolo capitato - lunato misurato sui radiogrammi convenzionali e quello misurato sulle ricostruzioni mpr dellartro - tc prima dellintervento e al follow - up ( p - value = 0 , 004 ) e lartro - tc ( p - value = 0 , 003 )  . 
la valutazione dei dati ha evidenziato una riduzione dellangolo capitato - lunato ( cl ) blandamente statisticamente signicativa tra le misurazioni pree post - trattamento , sia tra le misure ottenute in radiologia convenzionale ( p = 0 , 06 , deviazione standard = 2 , 31 ) sia per il confronto tra misure ottenute sui radiogrammi pretrattamento e quelle ottenute in artro - tc post - trattamento ( p = 0 , 07 , deviazione standard = 2 , 09 )  . non si osservata una differenza signicativa ( p = 0 , 26 , deviazione standard = 0 , 5 ) tra le misurazioni effettuate sui radiogrammi e le immagini artro - tc al follow - up . indice di altezza carpale ( coefciente di nattras ) prima della chirurgia era di 1 , 46 ( range 1 , 201 , 60 ) alla ra1166 radiol med ( 2013 ) 118 : 11571170 diography and 1.45 ( range , 1.251.56 ) on multiplanar ct reconstructions . 
 reduction of articular range of motion , especially during exion , and grip strength are the main clinical complaints leading to surgical repair of scapholunate dissociation [ 1721 ]  . 
 imaging , which is very useful in the preoperative diagnosis , can also play an important role in the postoperative follow - up , as it provides a concrete assessment of the effects of the procedure on wrist joint mechanics . 
a variety of dynamic views ( radial and ulnar deviation ) can be used to improve diagnostic sensitivity in identifying initial forms of instability not yet visible on standard static radiograms , and stress views of both wrists with clenched st can help to establish the diagnosis of scapholunate dissociation [ 28 , 33 , 34 ]  . 
 if the diagnosis remains uncertain with conventional radiography , multiplanar techniques such as ct or magnetic resonance ( mr ) imaging should be used which have a high level of sensitivity in assessing occult fractures [ 3537 ]  . 
 mr imaging is recommended for the study of the triangular brocartilage and ligaments but , as is known , it cannot be used in postoperative patients because of magnetic susceptibility artefacts due to metallic implants degrading image quality . 
intra - articular injection of contrast medium increases the diagnostic accuracy of both ct or mr imaging [ 35 ]  . spiral ct , thanks to multidetector technology , offers diograa ; nel follow - up era di 1 , 5 ( range 1 , 201 , 60 ) alla radiograa e 1 , 45 ( range 1 , 251 , 56 ) nelle ricostruzioni mpr . 
lanalisi dei dati non ha rilevato una differenza statisticamente signicativa tra lesame radiograco convenzionale e lartro - tc nella valutazione dei parametri considerati nel follow - up . riportiamo di seguito gli ulteriori risultati valutati alle immagini tomograche : la distanza media tra il foro duscita dorsale del tunnel osseo e il polo prossimale dello scafoide nelle ricostruzioni coronali risultata 1 , 2 cm ( range 0 , 61 , 8 ) e nel 67% dei casi era maggiore di 1 clo spessore medio dellemitendine frc era 2 , 3 mm ( range 1 , 3 3 , 5 ) alluscita dal tunnel osseo e 1 , 8 mm ( range 1 , 22 , 7 ) a livello del sito di ancoraggio . 
nei restanti casi non stato rilevato nessun segno di compromissione articolare . discussione la rottura del legamento scafo - lunato la lesione pi frequente del polso : linterruzione del collegamento tra lo scafoide e il semilunare porta a una sublussazione rotatoria dello scafoide e al collasso del carpo noto come disi ( dorsiexed intercalated segmental instability ) [ 2 ]  . 
la riduzione dellescursione articolare , soprattutto in essione , e della forza di presa , rappresenta la principale problematica clinica correlata agli interventi per la dissociazione scafo - lunata [ 1721 ]  . limaging , molto utile nella diagnosi pre - operatoria della dissociazione scafo - lunata , pu ricoprire un ruolo importante anche nel follow - up del paziente operato , al ne di valutare concretamente i risultati dellintervento sulla meccanica articolare del polso . 
una variet di proiezioni dinamiche ( deviazione radiale e ulnare ) pu essere effettuata per migliorare la sensibilit della metodica nella identicazione di forme dinstabilit iniziali non visibili nei radiogrammi standard statici ; inoltre la proiezione a pugno chiuso in stress di entrambi i polsi pu essere daiuto nella diagnosi di dissociazione scafo - lunata [ 28 , 33 , 34 ]  . se la diagnosi rimane dubbia con lindagine radiograca convenzionale utile ricorrere a metodiche multiplanari come la tc e la rm , che hanno unelevata sensibilit nella valutazione di fratture occulte [ 3537 ]  . 
la rm raccomandabile per lo studio della brocartilagine triangolare e delle strutture legamentose ma , come ben noto , sconsigliata nella valutazione dei pazienti operati a causa della presenza di artefatti da suscettivit magnetica dovuti agli impianti metallici , che possono disturbare la qualit dellimmagine . 
 liniezione intra - articolare di mezzo di contrasto aumenta laccuratezza della diagnosi sia della tc che della rm [ 35 ]  . radiol med ( 2013 ) 118 : 11571170 1167 high spatial resolution and allows the acquisition of isotropic voxels which permit retrospective reconstruction of high - quality images in the three spatial planes ; in addition , intra - articular injection of iodinated contrast material can overcome the typical limitations of low contrast resolution [ 37 , 38 ]  . 
we therefore opted for ct arthrography rather than mr imaging and used it as a gold standard to depict the alignment of the carpal bones and evaluate the state of the ligaments . 
technological development has made it possible to acquire isotropic voxels allowing image reformation in the three spatial planes and generation of high - quality three - dimensional images ; moreover , the introduction of tube current modulation can help reduce radiation doses by 3050% [ 38 , 39 ]  . analysis of our data indicates that there is no statistically signicant difference between the measurements obtained on conventional radiography and the multiplanar ct reconstructions , suggesting concordance of results . 
however , further studies with larger series are required to conrm the preliminary ndings obtained in this study . the results of the radiological measurements suggest progressive stretching of the tendon graft , especially in the sagittal plane , which is probably related to the histological and mechanical features of the tendon , which differ from those of a ligament . 
moreover , in one third of subjects it appeared loose or frankly lax . one aspect of the brunelli - stanley procedure , which is still controversial , is the exact position of the exit hole of the bone tunnel . 
 [ 30 ] state that the tunnel exit hole should be placed at the point of insertion of the scapholunate ligament and suggests avoiding the vicinity of the scapholunate joint , where the bone is poorly vascularised , so as to prevent complications such as necrosis and fractures . 
the correlation was la tc spirale , grazie alla tecnologia multidetettore , offre unalta risoluzione spaziale e permette lacquisizione di voxel isotropici che garantiscono la possibilit di ricostruire retrospettivamente immagini di alta qualit in tutti i piani spaziali ; inoltre liniezione intra - articolare di mezzo di contrasto iodato pu superare il limite della ridotta risoluzione di contrasto tipica della tc [ 37 , 38 ]  . 
abbiamo dunque scelto lartro - tc al posto della rm e utilizzandola come goldstandard per descrivere lallineamento delle ossa carpali e per valutare lo stato dei legamenti . con lartro - tc i legamenti articolari e i vari compartimenti articolari sono ben delineati e le sezioni trasversali forniscono unesatta localizzazione della lesione [ 37 , 39 ]  . 
grazie allo sviluppo della tecnologia , oggi possibile acquisire voxel isotropici che consentono la riformattazione delle immagini nei tre piani dello spazio e la creazione di immagini 3d di alta qualit ; inoltre lintroduzione della modulazione di tensione del tubo radiologico permette una riduzione della dose al paziente stimata attorno al 3050% [ 38 , 39 ]  . nel nostro studio lanalisi dei dati indica che non vi una differenza statisticamente signicativa tra le misurazioni radiologiche eseguite sulla radiograa convenzionale e sulle ricostruzioni mpr dellartro - tc , suggerendo una concordanza dei risultati . 
tuttavia , sono necessari ulteriori studi con casistiche numericamente pi ampie al ne di poter confermare i dati preliminari ottenuti in questo studio . i risultati delle misurazioni radiologiche suggeriscono un progressivo stiramento dellemitendine , soprattutto nel piano sagittale , probabilmente correlato alle caratteristiche istologiche e meccaniche del tendine , diverse da quelle di un legamento . 
inoltre , in un terzo dei casi , esso appariva deteso o francamente lasso . nellesecuzione dellintervento di brunelli - stanley , una problematica ancora aperta e per cui non c accordo in letteratura , lesatta posizione del foro di uscita del tunnel osseo . 
 [ 30 ] precisano che luscita del tunnel deve trovarsi a livello dellinserzione della porzione dorsale del legamento scafolunato e suggerisce di evitare le vicinanze dellarticolazione scafo - lunata , dove losso scarsamente vascolarizzato , al ne di evitare complicanze quali necrosi e fratture . 
nel nostro studio abbiamo osservato una correlazione statisticamente signicativa tra il posizio1168 radiol med ( 2013 ) 118 : 11571170 detected only in the measurements made on the radiographs and not in those made on the ct arthrograms . 
on the other hand , this modality allowed us to assess the quality and size of the tendon strip and to detect the progressive thinning along its course ; statistical analysis did not reveal any relationship between the features of the tendon strip and maintenance of the correct alignment of the carpal bones . our analysis also revealed a correlation between the position of the tunnel exit hole and the radiolunate angle . 
 however , we believe this result to be of minor importance as it is not supported by a similar correlation between the exit hole and the capitolunate angle . the ct arthrography images showed the presence of chondral erosions of the radiocarpal articular surfaces as an early sign of osteoarthritis , a nding that could not be evaluated with radiography alone . 
this is very important information for the correct assessment of a postoperative wrist in that persisting malalignment of the carpal segments leads to degenerative arthritis , the so - called scapholunate advanced collapse ( slac )  . 
 [ 30 ] , in a series of 38 wrists , reported the presence of minimal signs of degenerative osteoarthritis at the radial styloid process in seven cases ; the author also reported two cases of recurrence of carpal collapse with disi of the lunate and two other cases of wrist with slac , all of which asymptomatic . 
 conclusions in the literature , patients treated with brunelli - stanley stabilisation surgery undergo clinical and radiological follow - up using conventional radiography alone [ 1921 , 29 , 33 , 34 ]  . 
 our results show that while ct arthrography is just as valuable as conventional radiography in evaluating the standard parameters ( scapholunate gap , scapholunate angle , capitolunate angle , radiolunate angle , carpal height index ) , it has the advantage of depicting the fcr stabiliser tendon graft , with the possibility of determining its thickness , direction , degree of tension and possible lesions . 
it also provides an accurate and direct detection of any associated lesions affecting the triangular brocartilage , chondral surface and intra - articular ligaments in postoperative patients , lesions which conventional radiography alone is unable to depict [ 5 , 35 ]  . 
questa metodica ci ha permesso tuttavia di valutare la qualit e le dimensioni dellemitendine e di rilevare un progressivo assottigliamento lungo il suo decorso ; lanalisi statistica non ha evidenziato alcun rapporto tra le caratteristiche dellemitendine e il mantenimento di un corretto allineamento delle ossa carpali . dalla nostra analisi emersa anche una correlazione tra il posizionamento del foro di uscita del tunnel osseo e langolo radio - lunato . 
 tuttavia riteniamo questo risultato di scarsa importanza , in quanto non supportato da una simile correlazione tra il foro di uscita e langolo capito - lunato . le immagini artro - tc hanno mostrato la presenza di erosioni condrali delle superci radio - carpiche , quale segno precoce di osteoartrosi : tale rilievo non sarebbe valutabile al solo esame radiograco . 
questa unaltra informazione estremamente importante per una corretta valutazione del polso operato , in quanto la persistenza del disallineamento dei segmenti del carpo determina la comparsa di unartrosi degenerativa del polso , il cosiddetto slac ( scapholunate advanced collapse )  . 
 [ 30 ] , in una serie di 38 polsi , riportano la presenza di minimi segni di artrosi scafo - stiloidea in 7 casi ; lautore riferisce anche 2 casi di recidiva del collasso carpale con disi del semilunare e 2 di polso slac , tutti asintomatici . conclusioni in letteratura i pazienti sottoposti a intervento chirurgico di stabilizzazione di brunelli - stanley eseguivano un follow - up solo da un punto di vista clinico e radiologico utilizzando come gold standard lesame radiograco convenzionale [ 1921 , 29 , 33 , 34 ]  . 
 i nostri risultati mostrano che lartro - tc ha lo stesso valore della radiograa convenzionale nella valutazione dei parametri standard ( intervallo scafo - lunato , angolo scafolunato , angolo capitato lunato , angolo radio - lunato , indice di altezza carpale ) , ma consente inoltre lidenticazione del neo - legamento stabilizzatore fcr permettendo la differenziazione di spessore , direzione , il grado di tensione ed eventuali lesioni del neo - legamento ; fornisce inoltre unaccurata e diretta identicazione di eventuali lesioni associate della brocartilagine triangolare , della supercie condrale e dei legamenti intra - articolari nei pazienti operati non valutabili al solo esame radiograco [ 5 , 35 ]  . radiol med ( 2013 ) 118 : 11571170 1169 conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
 of these patients , 477 ( 89% ) had active bleeding and underwent bae and / or nbae ( 295 males and 182 females , aged between 12 and 71 years )  . 
the aetiology of haemoptysis was as follows : cystic brosis ( 23% ) , bronchiectasis ( 13% ) , tuberculosis sequelae ( 8% ) , chronic obstructive pulmonary disease ( copd ) ( 6% ) and no apparent cause ( 21% )  . 
major complications were recorded in 3 / 477 ( 0.6% ) : stroke ( n = 1 ) , transient ischaemic attack ( tia ) ( n = 1 ) and transient quadriplegia ( n = 1 )  . 
dal 1979 al 2010 , 534 pazienti sottoposti ad angiograa delle arterie bronchiali per emottisi sono stati retrospettivamente valutati ; 477 ( 89% ) avevano sanguinamento attivo e hanno eseguito bae e / o nbae ( 295 maschi e 182 femmine , et compresa tra 12 e 71 anni )  . 
leziologia dellemottisi stata brosi cistica ( 23% ) , bronchiectasie ( 13% ) , esiti tubercolari ( 8% ) , broncopneumopatia cronica ostruttiva ( bpco ) ( 6% ) e sine materia ( 21% )  . 
tre / 477 ( 0 , 6% ) pazienti presentarono complicanze maggiori : ictus cerebrale ( 1 ) , attacco ischemico transiente ( tia ) ( 1 ) e tetraparesi transitoria ( 1 ) ; 143 / 477 ( 30% ) presentarono complicanze minori : dolore toracico 86 / 143 ( 60% ) e disfagia 29 / 143 ( 20% )  . 
 1172 radiol med ( 2013 ) 118 : 11711183 keywords embolization bronchial arteries nonbronchial systemic arteries haemoptysis parole chiave embolizzazione arterie bronchiali arterie sistemiche non bronchiali emottisi introduction introduzione massive haemoptysis is a medical emergency requiring prompt diagnosis and treatment . 
haemoptysis is a symptom of a wide range of lung conditions that lead to the development and hypertrophy of the bronchial circulation , such as cystic brosis , bronchiectasis , active or previous tuberculosis , lung cancer , aspergilloma , lung abscesses , berchets or wegeners vasculitis , and sarcoidosis [ 2 , 57 ]  . 
in some cases , haemoptysis has no apparent cause and is known as idiopathic haemoptysis and have no identiable cause that triggers the pathophysiological mechanism and are classied by exclusion . 
in the literature , they account for 342% of cases [ 5 , 9 , 10 ]  . embolisation of the bronchial arteries is a valuable therapeutic option in patients with no indication for surgery , who are not candidates for surgery or who do not respond to conservative treatments [ 11 , 12 ]  . 
the pulmonary region was not among the rst applications , owing to the complexity of its double vascularisation : a functional low - pressure system for alveolar gas exchanges composed of pulmonary arteries and veins , and a second high - pressure system supplying the bronchopulmonary parenchyma and consisting of bronchial arteries and veins . 
the thin anastomoses between the pulmonary and bronchial arterial systems are only virtual under normal circumstances , but in acute or chronic conditions , they can produce compensatory hypertrophy of the bronchial arteries [ 12 , 13 ]  . since the rst cases of endovascular bronchial embolisation described by remy et al . 
today , embolisation occupies a central role among the most successful techniques as a result of its excellent long - term results compared with medical therapy , timely bleeding management [ 16 ] and minimal invasiveness as compared with surgery [ 17 ]  . this paper reviews 30 years of diagnostic and interventional experience with patients with haemoptysis at our centre and provides an analysis of the aetiology , diagnosis and efcacy of embolisation and its possible complications . lemottisi massiva unemergenza medica che necessita di pronta diagnosi e altrettanto immediata gestione terapeutica . 
lemottisi un sintomo che sottende una vasta serie di patologie polmonari che portano allo sviluppo e allipertroa del circolo bronchiale , quali la brosi cistica , le bronchiectasie , la tubercolosi attiva o in esiti , il cancro del polmone , gli aspergillomi , gli ascessi polmonari , le vasculiti del tipo berchet o wegener e la sarcoidosi [ 2 , 57 ]  . 
esistono inoltre emottisi sine materia dette idiopatiche ; esse non riconoscono una causa documentabile che innesca il meccanismo siopatologico e vengono classicate per esclusione ; in letteratura sono comprese fra il 3% e il 42% [ 5 , 9 , 10 ]  . lembolizzazione delle arterie bronchiali ( bae ) rappresenta una valida opzione terapeutica nei pazienti che non hanno indicazioni o non possono essere sottoposti ad intervento chirurgico o che non rispondono ai trattamenti conservativi [ 11 , 12 ]  . 
il distretto polmonare non fu certo fra i primi ad essere percorso , per la complessit del duplice sistema di vascolarizzazione , uno a bassa pressione , funzionale , deputato agli scambi gassosi alveolari composto da arterie e vene polmonari , e laltro ad alta pressione , sostenuto da arterie e vene bronchiali deputato ad alimentare il parenchima bronco - polmonare . 
le sottili anastomosi tra i sistemi arterioso polmonare e bronchiale sono , in condizioni di assoluta normalit , virtuali , ma in condizioni patologiche , acute o croniche , si assiste a unipertroa compensatoria delle arterie bronchiali [ 12 , 13 ]  . sin dai primi casi di embolizzazione bronchiale endovascolare descritti da remy et al . 
i motivi risiedono negli ottimi risultati a distanza rispetto alle terapie mediche , nella tempestivit del controllo del sanguinamento [ 16 ] e nella minima invasivit rispetto alla terapia chirurgiradiol med ( 2013 ) 118 : 11711183 1173 table 1 causes of haemoptysis tabella 1 cause di emottisi aetiology embolization , n ( % ) eziologia embolizzazione , n ( % ) 112 ( 23.5 ) 62 ( 13 ) 36 ( 7.5 ) 30 ( 6.3 ) 28 ( 5.9 ) 21 ( 4.4 ) 13 ( 2.7 ) 12 ( 2.5 ) 15 ( 3.1 ) 14 ( 2.9 ) 9 ( 1.9 ) 7 ( 1.5 ) 6 ( 1.3 ) 4 ( 0.8 ) 7 ( 1.5 ) 1 ( 0.2 ) 100 ( 21 ) 477 cystic brosis bronchiectasis tuberculosis sequelae copd pneumoconiosis sarcoidosis hypervascularity hstiocytosis previouis lobectomy lung carcinoma pneumonia aneurysm of bronchial artery oral antithrombotic therapy tetralogy of fallot aspergilloma berchets vasculitis sine materia total chronic obstructive pulmonary disease materials and methods fibrosi cistica bronchiectasie esiti tubercolari bpco pneumoconiosi sarcoidosi lesione ipervascolare istiocitosi pregressa lobectomia carcinoma polmonare polmonite aneurisma a . 
bronchiale terapia orale anticoagulante tetralogia di fallot aspergilloma vasculite di berchet sine materia totale broncopneumopatia cronica ostruttiva 112 ( 23.5 ) 62 ( 13 ) 36 ( 7.5 ) 30 ( 6.3 ) 28 ( 5.9 ) 21 ( 4.4 ) 13 ( 2.7 ) 12 ( 2.5 ) 15 ( 3.1 ) 14 ( 2.9 ) 9 ( 1.9 ) 7 ( 1.5 ) 6 ( 1.3 ) 4 ( 0.8 ) 7 ( 1.5 ) 1 ( 0.2 ) 100 ( 21 ) a total of 534 patients who had undergone angiography for haemoptysis between 1979 and 2010 were retrospectively reviewed . 
of these , 477 ( 295 males and 182 females , age 1271 years ) underwent embolisation of the bronchial arteries and / or nonbronchial systemic arteries with a mean follow - up period of 14 ( 836 ) months . 
to identify causes and sites of bleeding , chest radiography and bronchoscopy were employed in the early period , whereas multidetector computed tomography ( mdct ) was preferred in the more recent period . 
the most frequent were cystic brosis ( 23% ) , bronchiectasis ( 13% ) , tuberculosis sequelae ( 8% ) and chronic obstructive pulmonary disease ( copd ) ( 6% )  . 
in 21% of cases , haemoptysis was classied as idiopathic , as no abnormalities were observed in either the parenchyma or the bronchial arteries . a variety of embolisation materials have been used over the years . 
the most frequently used in the early years of our experience was spongostan ( brin gel ) , followed by polyvinyl alcohol particles ( pva ) with a diameter of 150300 m if there were no bronchopulmonary anastomoses , > 300 m if they were present , and 500700 m when several distal branches had already been embolised with smaller particles . 
questo lavoro rappresenta una review della nostra esperienza diagnostica ed interventistica di oltre 30 anni sui pazienti con emottisi , analizzando leziologia , la diagnosi e lefcacia della terapia embolizzante e le eventuali complicanze . materiali e metodi sono stati valutati retrospettivamente 534 pazienti sottoposti ad angiograa per emottisi dal 1979 al 2010 ; di questi , 477 pazienti ( 295 maschi e 182 femmine , di et compresa fra 12 e 71 anni ) , hanno eseguito bae e / o delle arterie sistemiche non bronchiali ( nbae ) con un follow - up medio di 14 mesi ( 836 mesi )  . 
per lindividuazione delle cause e della sede del sanguinamento si ricorso inizialmente , alla radiograa del torace e alla broncoscopia e pi recentemente sempre alla tomograa computerizzata multidetettore ( tcmd )  . 
le cause individuate pi frequentemente sono state la brosi cistica ( 23% ) , le bronchiectasie ( 13% ) , gli esiti tubercolari ( 8% ) e la broncopneumopatia cronica ostruttiva ( bpco ) ( 6% )  . 
il materiale pi frequentemente utilizzato , allinizio della nostra esperienza , stato lo spongostan ( gelatina di brina ) , successivamente , sono state sempre pi utilizzate le particelle di polivinil - alcool ( pva ) , con diame1174 radiol med ( 2013 ) 118 : 11711183 yond the common origin of intercostobronchial trunks and of arteries supplying the spinal cord . 
automatic injectors have been increasingly used in the more recent period . the study was approved by our local ethics committee according to the standards of the declaration of helsinki and to the current ethical guidelines . statistical analysis all variables were examined with descriptive methods ; cross - tabulations were checked with chi - squared test , or by fishers exact test . 
 results diagnostic angiography was performed on 534 patients with haemoptysis , 477 / 534 ( 89% ) of whom had active bleeding and subsequently underwent embolisation of the bronchial and / or nonbronchial systemic arteries . 
the major complications , affecting only 3 / 477 patients ( 0.6% ) , included one case of stroke and one case of transient ischaemic attack ( tia ) after the embolisation procedure and one of immediate transient tetraplegia due to spasm of the medullary artery . 
on the other hand , in moderate recurrent haemoptysis , the most critical aspect is the difculty maintaining an acceptable level of interpersonal relationships , and the psychological implications of this call for an effective therapeutic solution . 
more rarely , the tro di 150300 micron in assenza di anastomosi broncopolmonari , > 300 micron quando presenti e di 500700 micron in presenza di rami pi distali gi embolizzati da particelle pi piccole . 
per la cateterizzazione selettiva delle arterie bronchiali sono stati impiegati cateteri diversamente congurati , tra cui i pi frequenti sono del tipo vertebral , cobra , simmons1 , head hunter ; lutilizzo di cateteri coassiali ha permesso la cateterizzazione delle arterie pi distali , superando lorigine comune di tronchi intercostobronchiali e di arterie dirette ad alimentare il midollo spinale . 
da qualche anno si ricorre sempre pi spesso alluso di iniettori automatici . lo studio ha ricevuto lapprovazione del comitato etico locale , conforme agli standard della dichiarazione di helsinki e alle attuali linee guide etiche . analisi statistica tutte le variabili sono state esaminate con le metodiche descrittive , le tabelle crociate sono state valutate con il test del chi - quadro o con il test esatto di fischer . 
le curve di sopravivenze sono state analizzate dalla regressione semiparametrica di cox . risultati langiograa diagnostica stata eseguita in 534 pazienti con emottisi , 477 / 534 ( 89% ) dei quali hanno avuto sanguinamento attivo e successivamente sono stati sottoposti ad embolizzazione delle arterie bronchiali e / o sistemiche non bronchiali . 
in 458 su 477 pazienti ( 96% ) si prodotta completa risoluzione dellemottisi nelle 24 ore successive alla procedura ; nel 2% dei pazienti il sanguinamento si risolto entro 48 ore . 
tra le complicanze maggiori , che riguardano solo 3 su 477 pazienti ( 0 , 6% ) , si sono vericati un caso di ictus cerebrale e un caso di attacco ischemico transiente ( tia ) dopo la procedura di embolizzazione e uno di tetraparesi transitoria immediato da spasmo dellarteria midollare . 
tra le complicanze minori osservate in 143 su 477 pazienti ( 30% ) , il dolore toracico e la disfagia si sono vericati rispettivamente nel 60% e nel 20% dei casi . 
la recidiva di emottisi nei pazienti con brosi cistica stata del 38% , mentre nelle altre patologie stata osservata nel 21% dei casi ( p = 0 , 08 )  . 
 radiol med ( 2013 ) 118 : 11711183 1175 bleeding involves nonbronchial systemic vessels not originating from the thoracic aorta . imaging , which relies on chest radiography and mdct , is always supplemented by bronchoscopy to evaluate correlated diseases and identify bleeding site . 
although chest radiography has long been considered useful for identifying the underlying disease and bleeding site , it succeeds in indicating lesion site and nature no more than 50% of cases , as reported in a retrospective review [ 5 ]  . 
mdct has high sensitivity and specicity and is adequate for documenting the origin of the bronchial arteries and / or nonbronchial systemic arteries and their morphological and topographical characteristics [ 19 25 ]  . 
side and specic site of bleeding are identied on ct in 63% of patients [ 26 , 27 ] , a percentage that reaches 100% if ct is combined with bronchoscopy [ 5 ]  . 
the disease most frequently associated with diagnostic failure is cystic brosis [ 7 ] , in which the presence of multiple signs including central and peripheral interstitial thickening , bronchiectasis often lled with mucus , occupation of the terminal bronchioles and intralobular airspace , consolidations and groundglass opacities forms such a complex pattern that in most cases it is impossible to identify any discrete sites . 
however , a bilateral origin of bleeding cannot be ruled out in these patients . ct angiography allows recognition of bronchial arteries , their calibre and their mediastinal course with greater accuracy than aortography and more completeness than conventional selective angiography [ 1921 ]  . 
today , in the approach to the patient with haemoptysis , we therefore consider mdct essential , as it identies bleeding causes and sites ( ground - glass areas or consolidation ) and allows subsequent embolisation to be planned by depicting the bronchial and nonbronchial branches , their course and their calibre , which , when > 2 mm , is considered responsible for the bleeding . 
 chronic inammation with pleural involvement radically disrupts the normal anatomy , and the circulation develops new vessels , which emerge from the mammary , subclavian , intercostal and thoracic arteries , from the pericardial and discussione lemottisi , quando acuta e massiva , rappresenta una situazione clinica in grado di mettere a rischio la vita di un paziente . 
daltro canto , nelle emottisi di modesta entit ricorrenti , laspetto pi delicato rappresentato dalla difcolt per il paziente a mantenere una vita di relazione accettabile ed il risvolto psicologico richiede una soluzione terapeutica efcace . 
le arterie bronchiali sono la principale fonte di emottisi e pertanto negli anni sono andati perfezionandosi e incrementandosi gli studi relativi alla identicazione e alla diagnosi delle alterazioni di questi vasi . 
pi raramente il sanguinamento sostenuto da vasi sistemici non bronchiali , ad origine non dallaorta toracica . limaging , rappresentato dalla radiograa tradizionale ( rx ) e dalla tcmd , si sempre afancato alla broncoscopia , nella valutazione della patologia correlata e nellindividuazione della sede del sanguinamento . 
nella nostra esperienza , la broncoscopia viene usata sempre di meno , nonostante sia una metodica in grado di fornire un sospetto sulla provenienza dellemottisi [ 6 , 18 ]  . 
nelle forme massive , non fornisce chiare indicazioni sulle cause e neanche sulla sede del sanguinamento , a causa dellinvasione di entrambi gli alberi bronchiali [ 3 , 6 ]  . 
lrx torace ha rappresentato , per molto tempo , un utile aiuto nella denizione della malattia responsabile del sintomo e del lato del sanguinamento ma , come riportato in unanalisi retrospettiva [ 5 ] , permette la diagnosi sia di sede che di natura soltanto nel 50% dei casi . 
 la tcmd presenta alta sensibilit e specicit ed un adeguato strumento per documentare lorigine delle arterie bronchiali e / o delle arterie sistemiche non bronchiali e la loro caratterizzazione morfologica e topograca [ 1925 ]  . 
 il lato del sanguinamento e la sede specica vengono individuate dalla tc nel 63% dei pazienti [ 26 , 27 ] ; inoltre possibile raggiungere il 100% quando alla tc si associa la broncoscopia [ 5 ]  . 
la patologia pi esposta a questi insuccessi rappresentata dalla brosi cistica [ 7 ] , in cui lassociazione di elementi semiologici multipli , tra cui lispessimento dellinterstizio centrale e periferico , le bronchiectasie spesso ripiene di muco , loccupazione dei bronchioli terminali e dello spazio aereo intralobulare , gli addensamenti e le aree a vetro smerigliato rappresentano un quadro cos complesso che , nella maggioranza dei casi , impedisce la specicit di attribuzione della loro sede . 
in our experience , the incidence of bleeding from these arteries was 3% . among the complications of bronchial artery embolisation ( bae ) and nonbronchial artery embolisation ( nbae ) , spinal cord infarction due to the close relations between the bronchial and spinal circulations is the most worrying . 
the largest branch , the artery of adamkieradiol med ( 2013 ) 118 : 11711183 si pu escludere , peraltro , in questi pazienti la provenienza bilaterale del sanguinamento . langio - tc permette , per di pi , lidenticazione delle arterie bronchiali , il loro calibro e decorso nel mediastino con unaccuratezza superiore allaortograa e in maniera pi completa rispetto allo studio angiograco selettivo tradizionale [ 1921 ] ; la panoramicit delle immagini ha permesso anche lindividuazione delle arterie bronchiali sistemiche non bronchiali . 
pertanto , oggi , nellapproccio al paziente con emottisi , riteniamo indispensabile lo studio tcmd che porta a conoscenza della causa della patologia , qualora sconosciuta , della sede del sanguinamento ( aree a vetro smerigliato o addensamento ) e della pianicazione del successivo trattamento embolizzante , grazie alla documentazione dei rami bronchiali e non bronchiali , del loro decorso e del calibro che , quando > 2 mm , viene considerato responsabile di sanguinamento . 
 nella nostra esperienza lincidenza del sanguinamento da queste arterie risultato del 3% . tra le complicanze delle embolizzazione delle bae e nbae , linfarto del midollo spinale dovuto alle stretti rapporti tra il circolo bronchiale e quello spinale , la complicanza pi preoccupante . 
questarteria ha un caratteristico andamento rettilineo , proiettantesi sui processi spinosi vertebrali , per cui dobbligo , in fase angiograca , approfondire con proiezioni oblique il decorso e la morfologia di tutte le arterie che si proiettano sul rachide . 
 la mielite trasversa unaltra complicanza riportata in letteratura in meno dell1% dei casi dopo angiograa delle arterie bronchiali , seguita o meno dallembolizzazione , associata pi spesso allutilizzo di mezzo di contrasto non radiol med ( 2013 ) 118 : 11711183 1177 fig . 
this artery follows a characteristic linear course projecting over the vertebral spinous processes ; consequently , the course and morphology of all arteries projecting over the spine should be further investigated using oblique projections at angiography . 
 transverse myelitis is another complication , which is reported in < 1% of cases after angiography of bronchial arteries followed or not by embolisation and is more often associated with the use of nonionic contrast material [ 24 , 30 ]  . 
no case of transverse myelitis was observed in our experience . the literature contains rare reports of inadvertent occlusion of the intracerebral arteries , especially when systemic branches collateral to the bronchial tree originate directly from the subclavian artery or its branches . 
nessun caso di mielite trasversa stato osservato nella nostra esperienza . in letteratura sono riportati rari casi di inavvertita occlusione delle arterie intracerebrali , soprattutto quando rami collaterali sistemici allalbero bronchiale originano direttamente dallarteria succlavia o dai rami dellarteria succlavia . 
nella nostra esperienza si vericato un caso di ictus cerebrale dopo circa 23 ore dallembolizzazione e un caso di tia in presenza di un circolo collaterale con usso verso lasse carotideo , manifestatosi nella fase nale della procedura . 
complicanze pi comuni , solitamente transitorie , sono il dolore toracico e la disfagia , che possono vericarsi per 27 giorni dopo la procedura di embolizzazione , dovuti probabilmente al coinvolgimento di piccoli rami delle arterie che irrorano lesofago [ 31 ]  . 
selective catheterisation of a right intercostalbronchial branch , with extensive areas of hypervascularisation of the upper lobe ; hypertrophy and tortuosity of the second right intercostal artery ( a )  . 
b embolizzazione selettiva con conservazione del ii ramo intercostale destro . embolisation , and one case of tia in the presence of a collateral circulation with blood ow towards the carotid axis , developing in the nal stage of the procedure . 
more common and usually transient complications are chest pain and dysphagia , which may occur 27 days after embolisation and are probably due to the involvement of small arterial branches supplying the oesophagus [ 31 ]  . 
 it was clear from the start that the pathology behind haemoptysis was an arterial hypervascularisation based on parenchymal inammation or bronchial vascular hypertrophy due to inadequate blood ow in the pulmonary systethe currently most accredited pathophysiological interpretation was conrmed in our experience by two cases of haemoptysis associated with right pulmonary artery occlusion due to brosis from tuberculous adenitis . 
in these cases , chest radiography evidenced right hilar enlargement , pulmonary angiography showed obstruction of the right branch in one case and of the branch to the upper lobe in the other , whereas bronchial arteriography demonstrated hypertrophy of the meticolosa rimane uno dei principali fattori in grado di ridurre il rischio di complicanze [ 31 ]  . 
fin dallinizio si evidenzi che alla base dellemottisi risiedeva un fenomeno di ipervascolarizzazione arteriosa sostenuta da alterazioni ogistiche parenchimali o da ipertroa vascolare bronchiale conseguente a ipoafusso nel sistema polmonare . 
 more recently , improvements in embolisation materials and , in particular , in coaxial catheters , have helped to achieve excellent results , even though they have not signicantly impacted success rates . 
excessively rapid exclusion of the bronchial circulation and incomplete occlusion of the branches supplying the hypervascular lesion , whether bronchial or nonbronchial systemic , are conditions predisposing to the relapse of bleeding . 
pi recentemente , il miglioramento dei materiali utilizzati nella procedura e in particolare di cateteri coassiali ha contribuito al raggiungimento di ottimi risultati , pur non avendo signicativamente modicato la percentuale di successi . 
lesclusione troppo rapida del circolo bronchiale e locclusione non completa dei rami afferenti alla sede ipervascolarizzata , bronchiali o sistemici non bronchiali , rappresentano condizioni predisponenti la ricomparsa del sanguinamento . 
durante la procedura di embolizzazione obbligatoria lesclusione di tutti i rami ipertroci sviluppati allinterno del polmone ; lembolizzazione deve essere quanto pi periferica possibile coinvolgendo tutti i rami di suddivisione in modo da impedire che rami profondi ancora pervi richiamino sangue da arterie sistemiche non bronchiali . 
occorre , inoltre , scegliere accuratamente la misura degli agenti embolizzanti per evitarne il passaggio attraverso le anastomosi bronco - polmonari sia fra arterie bronchiali e vene polmonari che fra arterie bronchiali e arterie polmonari , frequenti nei pazienti con emottisi ; pertanto il diametro dei materiali dovrebbe essere pi grande di 325 radiol med ( 2013 ) 118 : 11711183 1181 ary branches so as to prevent deep , still patent , branches from receiving blood from nonbronchial systemic arteries . 
 the size of the embolic agents should also be carefully selected in order to prevent them passing through the bronchopulmonary anastomoses between the bronchial arteries and pulmonary veins and between the bronchial arteries and pulmonary arteries , which are frequent in patients with haemoptysis . 
therefore , the diameter of materials should be > 325 m , which is the size of the largest bronchopulmonary anastomosis found in the human lung [ 32 ]  . 
we observed that in the presence of large shunts within the pulmonary artery , the extent of haemoptysis tends to be massive and , conversely , that shunting was present in all patients , with a history of daily blood loss exceeding 600 ml . 
 spongostan represented the best embolising , despite the fact that it was prepared manually by cutting to the desired size and shape to produce tiny and , above all , heterogeneous elements able to induce a transient vascular occlusion . 
it has also been demonstrated that , in cases of recurrent haemoptysis , the use of periodically repeated embolisation procedures ( no more than four in our experience ) , even in the absence of bleeding , improves symptoms and reduces relapse . 
the extent and chronic nature of the pathological processes in these patients , as well as involvement of bronchial and nonbronchial systemic branches , are no doubt responsible for m , che la misura pi grande di anastomosi broncopolmonare individuata nel polmone umano [ 32 ]  . 
abbiamo osservato che in presenza di voluminosi shunt con larteria polmonare , lentit dellemottisi era notevole e viceversa che in tutti i casi in cui in anamnesi risultava una perdita di sangue giornaliera di oltre 600 ml , gli shunt erano presenti . 
 lo spongostan ha rappresentato per lungo tempo il migliore materiale embolizzante , nonostante fosse realizzato manualmente attraverso una tta operazione di sminuzzamento e di parcellizzazione , tale da realizzare elementi molto piccoli e soprattutto disomogenei , in grado di provocare unocclusione temporanea del vaso . 
il materiale riassorbibile viene considerato teoricamente meno efcace rispetto al pva ; tuttavia non esistono evidenze che dimostrino un risultato a lungo termine signicativamente inferiore rispetto a quello ottenuto con il materiale non riassorbibile ; i risultati immediati , dimostratisi peraltro ottimi , sia nella nostra esperienza che nella letteratura pi recente , non sono , infatti , inuenzati dalla differenza di assorbibilit dei materiali . 
 limpiego della tcmd e il miglioramento dei materiali ha reso questa procedura pi sicura e di maggiore duttilit , nonostante statisticamente i risultati di successo non sono signicativamente migliorati nel corso degli anni . 
si dimostrato inoltre che , in caso di emoftoe ricorrente , luso di procedure di embolizzazione ripetute periodicamente ( nella nostra esperienza non superiori a 4 ) , anche in assenza di sanguinamento , consente un miglioramento della sintomatologia con riduzione delle recidive . 
il maggior numero di recidive stato osservato nei pazienti con brosi cistica ( 38% ) rispetto alle altre cause di emottisi 21% ( p = 0 , 06 )  . 
the high rates of recurrence and postprocedure mortality in lung cancer patients have often advised against the use of this procedure , except in severe emergency situations . nella nostra casistica sono stati limitati i casi di aspergilloma e di carcinomi polmonari trattati con bae . 
lelevata percentuale di recidiva e lalta mortalit dopo la procedura , nel caso di tumore polmonare , hanno spesso sconsigliato luso della procedura , se non in situazioni di grave emergenza . conclusions conclusioni temporary and long - term control of haemoptysis through embolisation of the bronchial and nonbronchial systemic arteries may reduce the risk of death and improve the quality of life of patients with chronic pulmonary disease . 
the interventional radiologists experience is crucial to successfully controlling haemoptysis and preventing its complications . il controllo temporaneo e a lungo tempo dellemottisi con lembolizzazione delle arterie bronchiali e sistemiche non bronchiali pu diminuire il rischio di morte e migliorare la qualit di vita dei pazienti con patologia polmonare cronica . la bae e nbae un metodo efcace e sicuro nel trattamento acuto dellemottisi , con bassa percentuale di recidive e complicanze maggiori e minori . 
avogadro , novara , italy 3sdo fisica sanitaria , aou maggiore della carit , novara , italy 4 scdu oncologia , aou maggiore della carit , universit del piemonte orientale a . 
a nuclear medicine specialist interpreted wb - bs images and two blinded radiologists , rst independently and then jointly , interpreted the wb - dwibs images by completing a reading grid categorising the skeletal segments . 
we found a good level of interobserver agreement for the wb - dwibs images and an excellent level of agreement in the subjective judgement of presence or absence of disease between wb - bs and wb - dwibs after consensual double reading . 
un medico nucleare ha interpretato le immagini della sotb e due medici radiologi prima individualmente rispettivamente in cieco e poi esprimendo un parere congiunto hanno letto e interpretato le immagini di wb - dwibs , compilando una scheda di lettura predenita con una categorizzazione dei segmenti scheletrici . 
stata calcolata la concordanza interosservatore per la lettura delle immagini wb - dwibs e anche la concordanza tra le due tecniche ( wb - dwibs e sotb ) con il test k di cohen . 
lanalisi dellaccordo tra la lettura del medico nucleare e del radiologo , calcolata mediante il k statistico di cohen , ha fornito un valore di k = 0 , 87 [ 95% intervallo di condenza ( ci ) = 0 , 760 , 98 ]  . 
dallanalisi dei risultati si osservano una buona corrispondenza delle letture radiologiche della wb - dwibs e un ottimo accordo nel giudizio soggettivo di presenza o assenza di lesioni tra la sotb e la wb - dwibs effettuata in doppia lettura in consensus . 
le sedi anatomiche di maggiore discordanza tra dwibs e sotb sono rappresentate dal bacino , coccige e sterno , sedi nelle quali la sotb trova i suoi principali limiti di detezione parole chiave risonanza magnetica - dwibs metastasi ossee scintigraa introduction introduzione detecting bone metastases relies on x - ray screening and the use of bone scintigraphy ( bs )  . 
secondary bone lesions can also be documented with computed tomography ( ct ) and ct - positron emission tomography ( ct - pet ) in the course of tnm staging . 
bone scintigraphy is one of the most frequently ordered investigations for suspected bone metastases , particularly during oncological follow - up , and it remains a reference modality for oncologists [ 1 ]  . 
 false negative ndings and low sensitivity , on the other hand , may be caused by fast - growing lytic lesions , lesions with low metabolism or avascular anatomical sites . 
the role of conventional magnetic resonance ( mr ) imaging detecting bone metastases has long been established , and research is focusing on validating whole - body mr imaging for the staging of bone metastases [ 46 ]  . 
this has prompted increasing interest in determining the real diagnostic impact of whole - body diffusion - weighted imaging ( wb - dwi ) , compared with bs , in detecting bone metastases . 
 la scintigraa ossea rappresenta , allo stato attuale , una delle indagini maggiormente richieste nel sospetto di metastasi ossee e soprattutto nella fase di follow - up , e mantiene un ruolo di metodica di riferimento per gli oncologi [ 1 ] , ma ha dei limiti noti che ne riducono la specicit e la sensibilit [ 2 , 3 ]  . 
le fratture e le alterazioni degenerative sono , causando turn - over metabolico dellosso , le cause pi frequenti di falsi positivi , comportando una riduzione della specicit della metodica ; le lesioni litiche a rapido accrescimento , le lesioni a basso metabolismo , oppure quando la sede anatomica avascolare , possono causare falsi negativi e quindi una riduzione di sensibilit . 
il ruolo della risonanza magnetica ( rm ) convenzionale nei confronti della ricerca di metastasi ossee consolidato da tempo e attualmente , linteresse della letteratura si sta orientando verso la validazione della rm whole body nella stadiazione delle metastasi scheletriche [ 46 ]  . 
 sorto , quindi , linteresse nel capire quale possa essere il reale impatto diagnostico dellimaging di diffusione whole - body rispetto alla scintigraa ossea , nel riconoscere la presenza delle metastasi ossee . 
scopo del presente studio determinare quale sia laccuratezza diagnostica e la concordanza della rm whole - body con tecnica diffusion weighted imaging with background body signal suppression ( wb - dwibs ) , nei confronti della sotb , nella identicazione delle metastasi ossee . radiol med ( 2013 ) 118 : 465475 solid tumours ( breast , colon , lung , bladder , kidney , prostate ) and suspected bone metastases underwent wb - bs and whole - body mr imaging using diffusion - weighted imaging with background suppression ( wb - dwibs )  . 
at the time of the study , all 23 patients had a histological or imaging diagnosis of primary tumour and had undergone wb - bs that either conrmed or excluded the presence of bone metastases . 
 after providing informed consent , all patients underwent a wb - mri with conventional [ t1 - weighted spin - echo ( se ) and short tau inversion recovery ( stir ) ] and dw sequences . 
al momento dellosservazione tutti i 23 pazienti erano gi in possesso di una diagnosi istologica o strumentale di tumore primitivo e di una scintigraa ossea che attestava o escludeva la presenza di metastasi ossee . previo consenso informato , tutti i pazienti sono stati sottoposti a unindagine rm whole - body , che includeva sequenze convenzionali [ spin echo t1 pesate e short tau inversion recovery ( stir ) ] e sequenze pesate in diffusione . 
we used a qbody coil , with the patient positioned feet rst on an extended anatomical coverage table based on rolling - table technology ( mobitrack , philips , best , the netherlands )  . 
after an initial scout sequence , a dw sequence was obtained using echo - planar imaging with fat suppression through a stir sequence ( diffusion - weighted imaging with background suppression ) ( table 1 ) , repeated on multiple axial slabs from the epicranial aponeurosis to the proximal femoral diaphysis . image assessment for each patients in this observational study , images from the two procedures were read by a nuclear physician with > 10 years experience with bs and by two radiologists with > 15 years experience in mr imaging who were unaware of the clinical ndings . 
a database was then created that contained the following tutti i pazienti sono stati sottoposti a scintigraa ossea total body mediante gamma camera a doppia testa ( ecam 2t siemens , varicam ge ) mediante iniezione per via endovenosa di 550740 mbq ( 1520 mci ) di 99 mtc - difo sfonato . imaging di diffusione tutti i pazienti sono stati studiati con magnete rm operante a 1 , 5 t ( achieva , philips , best , olanda ) , release 2.1. 
abbiamo utilizzato la bobina q - body , posizionando il paziente ( in modo che entrasse nel gantry caudo - cranialmente , feet rst ) , su un tavolo porta - paziente a copertura anatomica estesa , con tecnologia basata sul tavolo mobile ( mobitrak , philips , best , olanda )  . 
the analysis assigns a default rating of 0 to all unreported targets . statistical analysis analysis was conducted on all patients ( n = 23 , for a total of 529 sites assessed )  . 
agreement between the two radiologists individual readings and between their joint reading of the wb - dwibs images and the results of wb - bs , with regard to the absence or presence of metastasis in the 529 sites analysed , was expressed using cohens kappa statistic [ 8 ] with a 95% condence interval ( ci )  . for per - patient analysis , 22 contingency tables were constructed based on evaluation of the presence or absence lettura delle immagini per ognuno dei 23 pazienti inclusi in questo studio osservazionale sono stati visionati in cieco , senza precedente conoscenza del quadro clinico , le immagini delle due indagi ni cui sono stati sottoposti , rispettivamente da un me dico specialista in medicina nucleare , con pi di dieci anni di esperienza nella lettura delle immagini scintigrache e da due medici specialisti in radiologia , con pi di quin dici anni di esperienza nel campo della risonanza magnetica . 
uno specializzando di radiologia del iv anno di radiologia ha quindi assegnato a ogni paziente un numero progressivo da 1 a 23 , rendendo anonima lanagraca , in rigoroso ordine alfabetico ed stato poi creato un database che indicasse per ogni paziente , let , la sede del tumore primitivo , la localizzazione delle metastasi ossee riconosciute dalla sotb e di quelle riconosciute dalla risonanza magnetica dwibs . 
analysis of agreement between the nuclear physicians and the radiologists readings , based on the reading grid , provided a value of = 0.87 ( 95% ci = 0.760.98 ) , indicating excellent agreement in the subjective judgement of the presence or absence of metastases in the analysis of wb - bs and wbdwibs by independent and blinded readers . per - patient analysis the 23 patients were all undergoing follow - up for solid tumours : breast ( n = 6 ) , colon ( n = 5 ) , lung ( n = 5 ) , bladder ( n = 2 ) , kidney ( n = 1 ) and prostate ( n = 4 )  . 
after classifying wb - bsnegative patients with either no bone localisation ( n = 7 ) or with grade 1 localisations ( n = 5 ) corresponding to the answer noprobably not to the question of disease presence , 12 patients were negative to wb - bs and 11 positive to it . 
the fact that patients obtain the same positive assessment for the presence of metastasis on wb - dwibs and wb - bs does not in itself indicate agreement between the two modalities . 
lesion location also needs to be taken into account : for example , if one technique considers a patient positive for disease in a cervical vertebra and the other for disease in the lumbar spine , this does not indicate agreement . 
the observers judgements , on a per - lesion basis , are shown in table 4 , and the corresponding analysis , expressed with a 22 contingency table , is given in table 5 . 
laccordo sia tra le due letture radiologiche che tra la lettura in consensus successiva da parte dei due radiologi della wb - dwibs con quella della sotb , per la sola assenza o presenza di metastasi in ciascuno dei 529 siti analizzati stato espresso mediante la statistica k di cohen [ 8 ] riportata insieme allintervallo di condenza al 95% . per unanalisi basata sui singoli pazienti , sono state create tabelle di contingenza 22 basate sul giudizio di mera presenza o assenza di metastasi , dalle quali sono stati calcolati i valori di sensibilit e specicit . 
in seguito , si effettuata unanalisi basata sulle singole lesioni , quindi solo nei pazienti positivi alla sotb , metodica con la quale ci si pregge il confronto della rm ( dwibs )  . risultati accordo interosservatore lanalisi dellaccordo tra le due letture radiologiche ha fornito una buona concordanza con k = 0 , 68 [ 95% intervallo di condenza ( ci ) = 0 , 590 , 74 ] , quindi sostanziale ; lanalisi dellaccordo tra la lettura del medico nucleare e del radiologo , basata sulla scheda di lettura e la categorizzazione proposta ha fornito un valore di k = 0 , 87 ( 95% ci = 0 , 760 , 98 ) cio un ottimo accordo nel giudizio soggettivo di presenza o assenza di metastasi nellanalisi di sotb e wb - dwibs effettuata da osservatori indipendenti e in cieco . analisi per paziente i 23 pazienti studiati erano tutti in follow - up da tumori solidi , con la seguente ripartizione : 6 per neoplasia mammaria , 5 per neoplasia del colon , 5 per neoplasia polmonare , 2 per neoplasia vescicale , 1 per neoplasia renale , 4 per neoplasia prostatica . 
avendo classicato come pazienti negativi alla sotb quelli con nessuna localizzazione ( n = 7 ) o quelli con localizzazioni di grado 1 ( n = 5 ) corrispondente a giudizio probabilmente no alla domanda sulla presenza di localizzazione di malattia , risultano complessivamente 12 pazienti negativi e 11 positivi alla sotb . 
these can be summarised in cervicaldorsallumbar segments of the spine and in long di contingenza 22 , basata su un mero giudizio di presenza di metastasi per paziente , pu essere riassunta come in tabella 3 . 
il fatto che i pazienti ricevano lo stesso giudizio dalla dwibs e dalla sotb come positivi per presenza di metastasi non di per s indice di accordo fra le due metodiche . 
per questo , in seconda istanza , abbiamo considerato il sottogruppo dei pazienti positivi per localizzazioni di malattia alla sotb ( 11 pazienti ) per un totale di 20 lesioni complessive . 
il giudizio degli osservatori , lesione per lesione , riportato nella tabella 4 e la corrispondente analisi , espressa in tabella di contingenza 22 , riportata in tabella 5 nella quale il totale di n = 253 sedi anatomiche stato ottenuto moltiplicando il numero di sedi anatomiche per il numero totale dei pazienti ( n = 23 )  . 
nellanalisi per lesione si ottiene un valore di sensibilit pari all80% ( 95% ci = 75%85% ) e un valore di specicit pari al 98 , 2 % ( 95% ci = 96 , 5%99 , 8% )  . 
con un diverso raggruppamento anche il valore di specicit ne risulterebbe modicato , mentre il valore di sensibilit rimarrebbe inalterato . valutando le singole localizzazioni per singole sedi , 4 lesioni ( pazienti 2 , 8 e 21 ) positive alla sotb , non sono state riconosciute come tali alla dwibs . 
questo determina il ridotto valore di sensibilit rispetto alla corrispondente table 4 distribution of cases based on the number of lesions detected patient number lesions on wb - bs ( n ) lesions on wb - dwibs ( n ) lesions on wb - bs and wb - dwibs ( n ) wb - bs total sotb totale total totale total totale wb - bs , whole - body bone scintigraphy ; wb - dwibs , whole - body diffusion - weighted imaging with background suppression tabella 4 distribuzione della casistica in base al numero delle lesioni riscontrate paziente no . 
 lesioni sotb ( n ) lesioni dwibs ( n ) lesioni sotb e dwibs ( n ) sotb , scintigraa ossea ; dwibs , diffusion weighted imaging with background body signal suppression ; pz , paziente 472 wb - bs table 5 lesion - based contingency table tabella 5 tabella di contingenza lesione per lesione radiol med ( 2013 ) 118 : 465475 wb - dwibs total 229 233 total sotb totale dwibs 229 233 totale 253 wb - dwibs , whole - body diffusion - weighted imaging with background suppression ; wb - bs , whole - body bone scintigraphy sotb , scintigraa ossea ; dwibs , diffusion weighted imaging with background body signal suppression femur bones . 
sites of disagreement were the coccyx , the sternum and the pelvis ( positive on wb - bs and negative on wbdwibs ) and the long bones of the lower limbs ( negative on wb - bs but positive on wb - dwibs )  . 
 sedi di non concordanza della lettura sono state , da quanto denito positivo in scintigraa ossea : il coccige , lo sterno , e il bacino , e per quanto riguarda quanto denito positivo alla rm e non alla scintigraa , le ossa lunghe degli arti inferiori . 
per validare una nuova meto dica nellambito della diagnostica per immagini , com la diffusione a rm applicata in campo whole body , neces sario un confronto con la metodica standard pi consolidata nelliter diagnostico e clinico dei pazienti . 
la scinti graa ossea con tecnezio - 99 rappresenta attualmente sempre la metodica di prima istanza per la ricerca di me tastasi ossee grazie al suo approccio metabolico - funzio nale al riconoscimento della localizzazione scheletrica di malattia , pur con i limiti noti che la contraddistinguono [ 2 , 3 ]  . i primi studi [ 9 ] sulle applicazioni cliniche della rmradiol med ( 2013 ) 118 : 465475 fig . 
1a - d wb - bs of a patient being followed up for renal cell carcinoma ( a ) shows tracer uptake in the right iliac wing that was not appreciated on magnetic resonance wb - dwibs ( b = 1 , 000 ) in coronal multiplanar reconstruction ( mpr ) ( b ) , and corresponding to a bone broma . 
1a - d in paziente in follow - up per carcinoma renale la sotb ( a ) documenta presenza di accumulo di tracciante in corrispondenza dellala iliaca destra non apprezzabile alla rm - wb - dwibs ( b = 1000 ) nella ricostruzione multiplanare ( mpr ) coronale ( b ) e corrispondente a broma osseo . 
la tc in mpr coronali ( d ) eseguita in approfondimento di tale reperto , documenta la presenza di una lesione polipoide ( freccia ) , caratterizzata da intenso enhancement di mezzo di contrasto in corrispondenza porzione della essura epatica del colon . 
in studi successivi [ 1012 ] si dimostrato che il valore aggiunto alla rm convenzionale , delle sequenze in diffusione , in letteratura , si inscrive in incremento di sensibilit e valore predittivo positivo nella detezione di metastasi scheletriche rispetto alla rm convenzionale whole body e alla scintigraa ossea , con incremento di sensibilit e valore predittivo positivo ( ppv ) rispettivamente dell8% e del 3% . per una corretta valutazione del contributo della diffusione allimaging diagnostico , inteso come protocollo stand - alone , cio un esame esclusivamente composto da sequenze in diffusione con relative ricostruzioni multiplanari , abbiamo condotto sia in precedenza [ 13 ] che nel presente studio , un confronto tra questa tecnica e la sotb . 
c sagittal short tau inversion recovery ( stir ) image showing high signal intensity in the trabecular bone of the sternal manubrium ( not visible in this image ) related to the presence of septic emboli from the area of lumbar spondylodiscitis . 
c stir in sagittale mostra iperintensit di segnale a della spongiosa ossea a livello del manubrio sternale ( non visibile in questa immagine ) da riferire alla presenza di emboli settici a partenza dal focolaio spondilodiscitico lombare . 
la sotb ( d ) in proiezione anteriore mostra accumulo focale del tracciante a livello lombare . to correctly evaluate the impact of dwi as a stand - alone protocol that is , an examination consisting only of dw sequences with multiplanar reconstruction , this and previous study of ours [ 13 ] compared dwi with wb - bs . 
despite the small number of patients studied ( reected in the large cis for sensitivity ) , wb - dwibs proved to have similar efcacy to wb - bs for detecting bone metastases . 
 given that no other studies have compared stand - alone wb - dwibs and wb - bs for detecting metastases , we are dwibs come metodica a se stante nella pratica clinica , ma solo per portare un contributo nel percorso di analisi scientica che ne evidenzi privilegi e difetti . 
pur nei limiti della bassa numero sit del campione ( testimoniata dai grandi intervalli di condenza per la sensibilit ) la tecnica wb - dwibs si dimo stra essere in grado di identicare le lesioni metastatiche ossee in maniera sostanzialmente sovrapponibile alla sotb . 
 non vi sono studi di confronto tra la wb - dwibs a se stante e la scintigraa ossea per la ricerca di secondarismi e pertanto non possiamo paragonare i nostri risultati con radiol med ( 2013 ) 118 : 465475 unable to compare our results with those of previous reports . 
giovanni battista di torino , via genova 3 , 10126 torino , italy 2istituto di radiologia , 2a facolt , universit degli studi di torino , ospedale san luigi gonzaga , orbassano ( to ) , italy correspondence to : c . 
this retrospective analysis was carried out to assess the feasibility and results of transjugular intrahepatic portal systemic shunt ( tips ) performed with ultrasound ( us ) - guided percutaneous puncture of the hepatic veins . 
in eight cases , a percutaneous puncture of the middle ( n = 7 ) or right ( n = 1 ) hepatic vein was required because the hepatic vein ostium was not accessible . 
three patients were eligible for liver transplantation , whereas the others were excluded due to shunt thrombosis ( n = 1 ) and previous nonhepatic neoplasms ( n = 3 )  . 
in 8 casi si resa necessaria la puntura percutanea delle vene epatiche mediana ( n = 7 ) o destra ( n = 1 ) , dopo tentativi fallimentari di cateterismo retrogrado ostiale . 
un paziente deceduto per edema polmonare ; 3 pazienti sono eleggibili per il trapianto epatico , mentre gli altri sono stati esclusi per occlusione dello shunt ( n = 1 ) o pregresse neoplasie extraepatiche ( n = 3 )  . 
lapproccio percutaneo alle vene epatiche rapido , sicuro ed utile nellevitare lesioni epatiche traumatiche . keywords interventional radiology transjugular parole chiave radiologia inteventistica transjugular 380 radiol med ( 2013 ) 118 : 379385 intrahepatic portosystemic shunt interventional ultrasonography hepatic veins intrahepatic portosystemic shunt ecograa interventistica vene epatiche introduction introduzione transjugular intrahepatic portal systemic shunt ( tips ) has become a standard procedure for treating complications of portal hypertension refractory to medical and endoscopic therapy . 
progressive advances in angiographic materials , increased operator experience and the use of ultrasound ( us ) to guide the portal puncture ensure high rates of technical success [ 13 ]  . 
the hepatic veins amenable to tips are the right and the middle hepatic ve these veins are usually catheterised via a retrograde transjugular approach from the inferior vena cava ( ivc ) to approach , by appropriately rotating the curved needle , the main intrahepatic portal branches 23 cm from the conuence . 
however , in the rare cases in which the hepatic veins cannot be catheterised via a retrograde approach ( because of recent and incomplete hepatic vein thrombosis , unilateral intrahepatic portal thrombosis , medial dislocation of the right main portal branch due to severe parenchymal atrophy , extrinsic compression of the ivc by the caudate lobe , expansile lesions at the hepatic vein conuence , etc . ) , ancillary techniques may be needed to successfully complete the procedure [ 46 ]  . 
i progressivi afnamenti dei materiali angiograci , lesperienza degli operatori e limpiego della guida ecograca ( us ) durante la puntura portale garantiscono un elevato successo tecnico [ 13 ]  . 
le vene epatiche proponibili per la tips sono la destra e la mediana : solitamente esse vengono cateterizzate per via retrograda transgiugulare dalla vena cava inferiore ( vci ) , al ne di poter approcciare , con opportuna rotazione dellago curvo , i rami portali intraepatici principali a 23 centimetri dalla conuenza . 
tuttavia , in rari casi in cui le vene epatiche non sono cateterizzabili per via retrograda ( trombosi recente ed incompleta delle vene epatiche , trombosi portale intraepatica monolaterale , dislocazione mediale del ramo portale principale di destra determinata da marcata atroa parenchimale , compressione estrinseca sullvci da parte del lobo caudato , lesioni espansive poste alla conuenza delle vene epatiche ecc . ) , per condurre a termine con successo la procedura pu essere necessario ricorrere a tecniche accessorie [ 46 ]  . 
in 8 / 153 ( 5.2% ) , seven men and one woman aged 4375 years ( mean 57.1 ) , treated for budd - chiari syndrome ( n = 1 ) , recurrent refractory variceal bleeding ( n = 1 ) , refractory ascites ( n = 2 ) and maintenance of portal vein patency prior to orthotopic liver transplantation ( olt ) in the presence of partial intrahepatic portal thrombosis ( n = 3 ) or markedly reduced portal ow due to spontaneous splenorenal shunt ( n = 1 ) , it was necessary to perform a us - guided percutaneous puncture of the middle or right hepatic vein , as the veins were inaccessible via the transcaval route . 
 prior to angiographic manoeuvres , the patients were clinically classied [ three in childpugh class a 56 , ve in nel periodo compreso tra novembre 2007 e febbraio 2011 , 153 pazienti sono stati sottoposti a tips presso il nostro istituto . 
in 8 / 153 ( 5 , 2% ) , 7 maschi e 1 femmina , di et compresa tra 43 e 75 anni ( media 57 , 1 ) , trattati per sindrome di budd - chiari ( 1 caso ) , emorragia varicosa recidivante refrattaria ( 1 caso ) , ascite refrattaria ( 2 casi ) e tutela della perviet portale in previsione di trapianto epatico ( olt ) in presenza di trombosi portale intraepatica parziale ( 3 casi ) o marcato ipoafusso portale determinato da uno shunt spontaneo spleno - renale ( 1 caso ) , si resa necessaria la puntura percutanea us - guidata della vena epatica mediana o destra , in quanto inaccessibili per via transcavale . 
1a - c si esegue la puntura percutanea eco - guidata della vena epatica mediana ( testa di freccia ) utilizzando un ago di chiba di 21 g e 15 cm di lunghezza ( freccie piene ) ( a ) , il cui apice ben apprezzabile nel lume della vena ( freccia vuota ) ( b )  . 
 class b 78 and overall model for end - stage liver disease ( meld ) score between 6 and 16 ] and assessed with imaging studies [ colour - doppler us in all cases and further diagnostic investigation with four - phase computed tomography ( ct ) in 3 / 8 cases ]  . 
all procedures were performed in the angiography room ( allura xperct fd20 - philips ) by three interventional radiologists with > 10 years experience , two of whom were involved in the angiographic examination and one in us imaging ( my lab 70 xvg , esaote biomedical , genoa , italy )  . 
using an intercostal access , a 15 - cm - long , 21 - gauge chiba needle ( pbn medicals , stenlose , denmark ) was used to puncture the middle vein in 7 / 8 cases and the right vein in 1 / 8 cases . 
after obturator removal , the correct position of the needle was checked rst by aspirating blood and then by injecting a few millilitres of contrast material ( ultravist 370 mg / ml , bayer schering pharma ag , berlin , germany )  . 
 le procedure sono sempre state eseguite in sala angiograca ( allura xperct fd20 , philips ) da 3 radiologi interventisti con esperienza ultra decennale , di cui 2 impegnati nelle manovre angiograche ed 1 nellesecuzione dellecograa ( my lab 70 xvg , esaote biomedical , genova , italia ) ; completavano lequipe 1 anestesista rianimatore , 1 infermiere professionale ed 1 tecnico di radiologia . 
 con accesso intercostale , utilizzando un ago chiba di 21 g e 15 cm di lunghezza ( pbn medicals , stenlose , danimarca ) , stata punta la vena mediana in 7 / 8 casi e la vena destra in 1 / 8 casi . 
estratto il mandrino , stato vericato il corretto posizionamento dellago dapprima mediante aspirazione di sangue e , successivamente , iniettando pochi ml di mezzo di contrasto ( ultravist 370 mg / ml , bayer schering pharma ag , berlino , germania )  . 
2a - c il lo guida introdotto in vena epatica viene sospinto in vci ( freccia piena ) ( a ) , dove catturato con un laccio ( freccia vuota ) cos da ottenere un accesso transepatico - giugulare ( b )  . 
attraverso il catetere dallaccesso giugulare si introduce successivamente una guida rigida teonata di 0 , 035 pollici e 180 cm di lunghezza ; su questultima inne , rimosso il catetere , si raggiunge per via retrograda la vena epatica con il set di rsch - uchida ( freccia )  . ( 4 f ) of the skater coaxial set ( pbn medicals , stenlose , denmark ) was inserted into the hepatic vein using the percutaneous access . 
a 180 - cm - long , 0.035in. , superstiff , teon - coated guidewire ( boston scientic , natick , ma , usa ) was then inserted , which was advanced deep into the hepatic vein parallel to the guidewire previously left in place . 
slato lago , la cannula di calibro minore ( 4 f ) del set coassiale skater ( pbn medicals , stenlose , danimarca ) stata inserita in vena epatica dallapproccio percutaneo . 
nel catetere stata poi introdotta una guida teonata superstiff di 0 , 035 pollici e 180 cm di lunghezza ( boston scientic corporation , natick , ma , usa ) , che stata sospinta profondamente in vena epatica , parallelamente alla guida gi in sede . 
dopo aver rimosso la guida di 0 , 020 pollici , lasciando in sede lesile cannula angiograca , la tips stata condotta con tecnica classica , radiol med ( 2013 ) 118 : 379385 continuous infusion of remifentanil ( mean dosage 0.05 g / kg / min ) and low doses of benzodiazepine ( midazolam and / or propofol )  . 
 portography and venous pressure measurements with a 5 - f , 90 - cm - long , calibrated pigtail catheter ( optimed , ettlingen , germany ) were carried out before and after shunt placement . 
in 6 / 8 cases ( 75% ) , a dedicated viatorr stent ( wl gore , dundee , scotland ) measuring 10 mm in diameter and 57 cm in length , dilated to a calibre of 8 mm , was deployed ; in 2 / 8 cases ( 25% ) , during the rst year of our study , we used two wallstents ( boston scientic ) , one 14 mm and one 16 mm in diameter and and 6 cm in length , dilated to 10 mm and 12 mm , respectively . utilizzando la guida us per la puntura portale , eseguita in sedo - analgesia con infusione continua di remifentanil ( dosaggio medio 0 , 05 g / kg / min ) e benzodiazepine a basse dosi ( midazolam e / o propofol )  . 
 prima e dopo il confezionamento dello shunt sono state eseguite la portograa e la misurazione delle pressioni venose con catetere pig - tail centimetrato di 5 f di calibro e 90 cm di lunghezza ( optimed , ettlingen , germania )  . 
haemodynamic and clinical success was achieved in 7 / 8 patients ( 87.5% ) , as one case of thrombosis of the nondedicated stent ( wallstent ) occurred 30 days after the procedure . 
in ve patients , the childpugh and meld class was not changed by tips placement , whereas the last two could not be assessed as they were undergoing anticoagulation therapy with dicumarol . 
although temporarily off the active waiting list , 3 / 7 patients are eligible for olt , whereas 4 / 7 patients were excluded : one due to shunt occlusion ( see above ) with development of a portal cavernoma , and three because of a history of extrahepatic neoplas there were no procedure - related complications . risultati il successo della tips e le relative complicanze sono stati valutati secondo le linee guida della society of interventional radiology ( sir ) [ 1 ]  . 
il gradiente porto - sistemico medio pre - tips stato di 25 mmhg ( range 1438 mmhg ) ; le 4 trombosi presentavano valori particolarmente elevati ( range 2238 mmhg )  . 
il successo emodinamico e clinico stato ottenuto in 7 / 8 pazienti ( 87 , 5% ) : si vericata una trombosi dello stent non dedicato ( wallstent ) a 30 giorni dal suo impianto . 
sette pazienti sono vivi ed in buona salute ; in cinque pazienti le classi child e meld non sono state inuenzate dalla tips , mentre gli ultimi due non sono valutabili perch in terapia con dicumarolici ( tao )  . 
sono eleggibili per lolt , seppur momentaneamente al di fuori della lista attiva , 3 / 7 pazienti mentre 4 / 7 pazienti sono stati esclusi : uno per locclusione gi descritta dello shunt , con formazione di cavernomatosi portale , e tre per una pregressa neoplasia extraepatica . 
non si sono vericate complicanze legate alla procedura . discussion discussione the conventional tips procedure , especially when carried out by expert operators and under us guidance [ 2 , 3 ] , is successfully completed in almost all cases [ 7 ] , and the shunt can be placed in either the right hepatic vein ( more easy to catheterise via retrograde approach under uoroscopic guidance ) or the middle hepatic vehowever , in certain conditions ( 5% of cases ) such as complete thrombosis of a portal hemisystem , severe hypotrophy of liver segments la tips con tecnica classica , soprattutto se eseguita da operatori esperti e con lausilio della guida us [ 2 , 3 ] , pu essere confezionata con successo nella quasi totalit dei casi [ 7 ] ; per lo shunt possono essere utilizzate sia la vena epatica destra , pi facilmente cateterizzabile per via retrograda con guida uoroscopica , sia la vena mediana . 
tuttavia , in particolari condizioni ( 5% dei casi ) , quali la trombosi completa di un emisistema portale , la marcata ipotroa dei segmenti 384 radiol med ( 2013 ) 118 : 379385 v and viii ( which alters anatomical relationships between the right portal branches and the ipsilateral hepatic vein ) [ 810 ] and incomplete budd - chiari syndromes [ 1114 ] only one hepatic vein will be suitable for shunting , but its transostial catheterisation may prove impossible [ 1 ]  . 
in these cases , us - guided percutaneous puncture of the target hepatic vein allows resolution of one of the earliest technical problems that may arise during tips placement , in only a few minutes and with a minimal amount of additional angiographic material . 
however , compared with the technique proposed by us , their approach is more invasive , exclusively practicable between the right hepatic vein and the ipsilateral portal branches , and entails the use of uncoated stents , which have lower patency than do dedicated stents [ 7 ]  . 
the only contraindication for percutaneous puncture of a hepatic vein is complete budd - chiari syndrome , in which case tips can only be performed through direct portal puncture from the ivc [ 5 , 15 ] or through direct intrahepatic portosystemic shunt ( dips ) , a technique that involves the simultaneous percutaneous puncture of the intrahepatic portal vein and retrohepatic ivc under us guidance [ 6 , 1618 ]  . 
 in conclusion , our experience demonstrates that in a small but nonnegligible proportion of patients with complicated portal hypertension , tips placement can be performed exclusively through us - guided percutaneous puncture of a hepatic vein , as this technique proved to be safe , feasible and effective , as well as providing a portosystemic shunt resulting in clinical improvement and the possibility of deferring olt in the majority of cases [ 19 ]  . 
 epatici v ed viii ( che altera i rapporti anatomici tra i rami portali di destra e la vena epatica omolaterale ) [ 810 ] e le sindromi di budd - chiari incomplete [ 1114 ] , risulta idonea per lo shunt ununica vena epatica , il cui cateterismo transostiale pu rivelarsi impossibile [ 1 ]  . 
in questi casi la puntura percutanea us - guidata della vena epatica target consente di risolvere , in pochi minuti e con limpiego di una minima quantit di materiale angiograco aggiuntivo , uno dei pi precoci problemi tecnici che si possono riscontrare in corso di tips . 
tuttavia tale procedura , rispetto alla tecnica da noi proposta , risulta pi invasiva , attuabile esclusivamente tra la vena epatica destra ed i rami portali omolaterali e prevede limpiego di stent non ricoperti , la cui perviet non ottimale , risultando inferiore a quella degli stent dedicati [ 7 ]  . 
unica controindicazione alla puntura percutanea di una vena epatica la sindrome di budd - chiari completa , nel qual caso la tips pu essere eseguita esclusivamente con puntura portale diretta dalla vci [ 5 , 15 ] o in alternativa tramite direct intrahepatic portocaval shunt ( dips ) , tecnica descritta da numerosi autori , che prevede la puntura percutanea simultanea us - guidata della vena porta intraepatica e della vci retroepatica [ 6 , 1618 ]  . 
 in conclusione , la nostra esperienza dimostra che in una piccola , ma non trascurabile , percentuale di pazienti con ipertensione portale complicata , la tips pu essere confezionata esclusivamente con lausilio della puntura percutanea us - guidata di una vena epatica , che si rivelata una tecnica sicura , fattibile ed efcace , in grado di garantire la creazione di uno shunt porto - sistemico che , nella gran parte dei casi , signica miglioramento clinico e possibilit di procrastinare nel tempo lolt [ 19 ]  . 
 in fact , while the initial problem was just to describe and interpret the new imaging , the additional tasks for the radiologist are to complement and complete the interview with a too often barely known patient . according to the medical radiological act and the law 187 / 2000 , radiologists should provide clinical history and explanations before and after the patients examination , but frequently they are not properly trained ( as is well explained by pasquale marano in the chapter training and communication )  . in addition , the radiologist is often invisible , since he is too busy in serially writing reports , expression of forensic medicine paperwork rather than art of the medical care . all these aspects are analysed in the book which , in order to be more incisive and convincing , describes in an agile but complete way the story of communication in radiology with the contribution of many specialists and experts , not only radiologists . 
we realise that communication has improved hand in hand with imaging renement ( from the analogical era of shadows radiologist , in which little value was given to report , to toti - potent and pan - exploring modern imaging , in which reports and communication are decisive )  . 
because of its complexity , communication has to be addressed in a multi - specialised way and in many areas of expertise ( humanistic and technical )  . thus , the book consists of an introduction , which deals with current health scenarios , the history of communication , the role and commitment of the teaching ; a general part , which deals with the new patient , prevention programs , the new radiologist - patient relationship , the medico - legal asquello della comunicazione in radiologia un argomento relativamente nuovo , nato alla ne degli anni novanta quando ci si cominci a occupare delle regole per redigere un buon referto e da allora proseguito e adattato alle crescenti esigenze sanitarie della societ . 
infatti , se il problema iniziale era quello di descrivere e interpretare il nuovo imaging , i compiti aggiuntivi del medico radiologo sono quelli di integrare e completare con il colloquio il rapporto con un paziente troppo spesso poco conosciuto . latto medico radiologico e la dlgs 187 / 2000 prevedono anamnesi e spiegazioni prima e dopo lesame , ma frequentemente i radiologi non sono adeguatamente preparati ( come fa ben intendere pasquale marano nel capitolo formazione e comunicazione )  . a ci si aggiunga una mentalit manageriale ( o dovremmo dire mercantile ? ) , che rende invisibile il radiologo occupato a redigere referti in serie , espressione pi di suggello medico - legale che di arte medica . di tutto ci si occupa il libro che , per essere pi incisivo e convincente , traccia in modo agile ma compiuto la storia della comunicazione radiologica e si avvale dellapporto di tanti specialisti ed esperti della materia , non solo radiologi . 
 cos , ci rendiamo conto che la comunicazione si afnata col miglioramento dellimaging ( dallepoca analogica del radiologo delle ombre , in cui il referto aveva ben poco valore , allimaging odierno toti - potente e pan - esplorante , in cui il referto e , pi in generale , la comunicazione sono decisivi )  . 
 perci , il libro si compone di una parte introduttiva , che tratta degli scenari sanitari attuali , della storia della comunicazione , del ruolo e dellimpegno formativo della didattica ; una parte generale , che analizza il nuovo paziente , i radiol med ( 2013 ) 118 : 520521 pects , pitfalls and tips for the radiologist ; a special part , where pacs - related ( picture archiving and communication system - related ) problems are analysed ( from economic and management aspects to the electronic database and the structured report )  . 
cardinale , deals with issues related to current exams ( e.g. , the value of incidental ndings , the appropriateness of examination referrals , the relationship with the prescribing physician , the management of breast screening ) and underlines the lack of a specic radiological culture . this book is addressed to all radiologists , from experts ( that nd professional conrmations ) to the youngest ( who , caught in the enthusiasm of imaging procedures and technology , can neglect communication , considered less rewarding )  . 
 while waiting for a full integration of the educational curricula , in which communication - related problems should be considered mandatory , it is appropriate for them to get equipped to defend the medical content of the radiological act . georgio cosmacini , radiologist and a notable italian historian of medicine , said : the image extracted from each person has not only a biological but also a biographical content , to which each doctor should turn his attention and competence . 
and here , the knowledge of problems and the ability to communicate makes the professional difference . programmi di prevenzione , il nuovo rapporto radiologo - paziente , gli aspetti medico - legali , le insidie e i consigli per il radiologo ; di una parte speciale , ove vengono trattate le problematiche legate al pacs ( picture archiving and communication system ) : dagli aspetti economico - gestionali allarchivio informatico , al referto strutturato . 
cardinale , tratta di problematiche connesse agli esami odierni ( ad esempio , il valore dei reperti incidentali , lappropriatezza delle richieste desame , il rapporto col medico prescrivente , la gestione dello screening senologico ) e sottolinea la carenza di una cultura radiologica specica . il testo si rivolge a tutti i radiologi , dai pi esperti ( che vi trovano conferme professionali ) ai pi giovani ( che , presi dallentusiasmo per le procedure di imaging e per tecnologia , possono trascurare gli aspetti comunicativi perch ritenuti meno appaganti )  . 
nellattesa di unintegrazione dei programmi didattici che renda obbligatorio lo studio delle problematiche della comunicazione , sar opportuno che si attrezzino a difendere il contenuto medico dellatto radiologico . come dice il grande storico italiano della medicina , giorgio cosmacini , radiologo : limmagine estratta da ogni persona ha s un contenuto biologico , ma anche un contenuto biograco cui il medico deve rivolgere la propria attenzione e la propria capacit . 
ferro dipartimento di radiologia e radiologia interventistica , irccs azienda ospedaliera ed universitaria san martino , ist istituto nazionale per la ricerca sul cancro , largo rosanna benzi 10 , 16132 genova , italy correspondence to : u.g. 
 le complicanze minori sono avvenute in dieci pazienti : malfunzionamento / rottura del catetere ( n = 9 ) , fuoriuscita di materiale gastrico dal tramite cutaneo ( n = 1 )  . 
la prg con tecnica di singola puntura e posizionamento di due ancore una procedura rapida , sicura ed efcace . parole chiave gastropessi gastrostomia radiologica percutanea fissaggio a t o ancora radiol med ( 2013 ) 118 : 356365 introduction introduzione percutaneous radiological gastrostomy ( prg ) consists of creating an articial gastrocutaneous stula between the anterior wall of the stomach and the anterior abdomen . 
gastropexy is the xation of the anterior gastric wall to the anterior abdominal wall by using a t - shaped fastener , known as an anchor [ 10 ]  . 
there is no consensus as to the minimum number of anchors to be used , which may range from one , placed through the gastrostomy tract , to four , arranged to form a rectangle around the tract [ 1 , 711 ]  . 
the purpose of this study was to assess the technical success and complications of prg performed with a single puncture and placement of two anchors through the gastrostomy tract . materials and methods patients between january 2008 and june 2011 , 163 consecutive patients ( 56 women and 107 men ) , aged 4193 ( mean 76 ) years , underwent prg with a modied technique consisting of a single puncture and the placement of two anchors through the gastrostomy tract . 
indications for prg placement for enteral feeding were as follows : neurological disorder in 133 patients , head and neck tumour in 23 patients and other conditions in the remaining six patients . 
the study was approved by the local ethics committee , and written informed consent was obtained from all patients or their legal guardians . materials in all 163 patients , the willsoglesby percutaneous gastrostomy set ( cook , bloomington , in , usa ) was used , which consists of a 0.035distally tapered metal guidewire , a 0.035 - stiff metal guidewire , a 12 - f willsoglesby gastrostomy catheter , a 10 - f dilator and a 17 - gauge introducer needle loaded with a suture anchor . 
 a tuttoggi ci sono controversie sul numero sufciente di ancore da usare , che pu variare da una , posizionata attraverso il tragitto della gastrostomia , no a quattro , posizionate a rettangolo attorno al tragitto della gastrostomia stessa [ 1 , 711 ]  . 
scopo del presente studio valutare il successo tecnico e le complicanze della prg con tecnica di singola puntura e posizionamento di due ancore attraverso il tragitto della gastrostomia . materiali e metodi pazienti da gennaio 2008 a giugno 2011 , 163 pazienti consecutivi ( 56 femmine , 107 maschi ) , det compresa tra 41 e 93 anni ( media 76 anni ) , sono stati sottoposti a prg con tecnica modicata mediante singola puntura e posizionamento di due ancore attraverso il tragitto della gastrostomia . 
le indicazioni al posizionamento di prg per nutrizione enterale sono risultate essere : patologia neurologica in 133 pazienti , tumore testa - collo in 23 pazienti ed altre patologie nei restanti 6 pazienti . 
lo studio stato approvato dal comitato etico locale e tutti i pazienti o loro tutori legali hanno fornito per iscritto il loro consenso informato . materiale in tutti i 163 pazienti stato utilizzato il set per gastrostomia percutanea wills - oglesby ( cook , bloomington , indiana , usa ) , composto da : guida metallica da 0 , 035 inch rastremata distalmente , guida rigida metallica da 0 , 035 inch , catetere gastrostomico wills - oglesby da 12 fr , dilatatore da 10 fr , ago - introduttore da 17 gauge caricato con unancora sutura . 
1a la sutura seta da 0 viene fatta passare a 1 , 5 cm dallapice del dilatatore da 10 fr ( subito sotto la parte rastremata del dilatatore )  . 
antibiotic prophylaxis with amoxicillin 1 , 000 mg / clavulanic acid 200 mg . the inferior margin of the liver was identied on ultrasound ( us ) and its position marked on the skin with a surgical pen . 
in all patients , 5 mg of hyoscine - n - butylbromide ( buscopan , boehringer - ingelheim , florence , italy ) was injected intravenously to relax the muscles and obtain adequate gastric distension . 
the stomach was then distended with 5001 , 000 ml of air insufated under uoroscopic guidance using a 100 - ml syringe in order to appose the anterior gastric wall to the anterior abdominal wall , under the costal margin , and to displace the transverse colon caudally . 
conrmation that the tip of the introducer needle had been inserted into the gastric lumen was obtained by aspirating air into the syringe and then injecting contrast material to visualise the gastric folds . 
circa trenta minuti prima della procedura stata somministrata , in tutti i pazienti , una prolassi antibiotica endovena ( ev ) di amoxicillina 1000 mg / acido clavulanico 200 mg . il margine inferiore epatico stato valutato tramite ecotomograa in tutti i pazienti e successivamente segnato , nella sua proiezione sulla cute , tramite pennarello dermograco . 
in tutti i pazienti stata eseguita iniezione ev di 5 mg di joshine - n - butyl - bromide ( buscopan , boehring ingelheim , firenze , italia ) allo scopo di garantire unadeguata distensione gastrica dovuta al rilassamento delle cellule muscolari lisce . 
lo stomaco stato quindi disteso con una quantit di aria variabile tra i 500 ed i 1000 ml , insufata , sotto guida uoroscopica , tramite una siringa da 100 ml , per portare la parete gastrica anteriore a contatto con la parete addominale anteriore , al di sotto del margine costale e per dislocare caudalmente il colon trasverso . 
 stato quindi inserito , attraverso lincisione cutanea , lago - introduttore da 17 gauge , contenente la sutura con ancora gastrointestinale cope ( cook , bloomington , indiana , usa )  . 
la conferma che lapice dellago introduttore fosse stato posizionato nel lume gastrico stata ottenuta mediante laspirazione di aria allinterno della siringa e successiva iniezione di mezzo di contrasto , al ne di rilevare le pliche gastriche . 
 follow - up tutti i pazienti sono stati sottoposti a follow - up clinico e , se necessario , mediante imaging ( radiograa delladdome e tomograa computerizzata ) a 30 giorni . 
sono state classicate come complicanze maggiori tutte quelle che hanno prolungato lospedalizzazione o richiesto una procedura chirurgica ; tutte le altre sono state classicate come complicanze minori [ 12 ]  . 
le ancore sono state liberate allinterno del lume gastrico a 710 giorni dalla procedura . risultati il successo tecnico della prg , con tecnica di singola puntura e posizionamento di due ancore attraverso il tragitto della gastrostomia , stato del 100% ( 163 / 163 pazienti )  . 
in 158 pazienti ( 97% ) stato eseguito laccesso percutaneo lungo la linea alba , nei restanti 5 pazienti ( 3% ) stato eseguito laccesso percutaneo lungo laponeurosi tra muscolo retto e muscoli obliqui delladdome . 
il tempo medio della procedura di gastropessi e di posizionamento del catetere gastrostomico stato di 9 minuti ( con un range tra i 4 e i 12 minuti )  . 
durante la procedura la uoroscopia stata pulsata ( 4 pulsazioni / s ) , con un tempo medio di scopia di 1 minuto e 12 secondi ( con un range di tempo tra i 33 secondi e i 4 minuti e 52 secondi )  . la mortalit a 30 giorni dalla procedura stata dell1 , 2% ( 2 / 163 pazienti )  . 
2a topography of the anterior abdominal wall where the linea alba is depicted in yellow ( arrows ) and the aponeurosis between the rectus abdominis and oblique muscles in blue ( arrowheads )  . 
b topography of the anterior gastric wall where the two gastric puncture sites are shown ( stars ) between the gastric antrum and body and the middle portion of the gastric body . 
2a disegno anatomico della parete addominale anteriore ove viene rappresentata la linea alba in giallo ( frecce ) e laponeurosi tra muscolo retto e muscoli obliqui in blu ( testa di frecce )  . 
b disegno anatomico della parete gastrica anteriore ove vengono rappresentati i due siti di puntura gastrica ( stelle ) : tra antro e corpo gastrico , e porzione media del corpo gastrico . 
3a release of the rst anchor ( arrow ) by pushing the distally tapered , 0.035 - metal guidewire , b introduction of the dilator and second 10 - f anchor , c release of the second anchor ( dashed arrow ) by withdrawing the distally tapered , 0.035 - metal guidewire , d retraction of the second anchor ( dashed arrow ) at the gastric entrance site where the rst anchor is already placed ( arrow ) , e introduction of the 12 - f gastrostomy catheter into the gastric cavity . 
3a rilascio della prima ancora ( freccia ) mediante la spinta della guida metallica da 0 , 035 inch rastremata distalmente , b introduzione del dilatatoreseconda ancora da 10 fr , c rilascio della seconda ancora ( freccia tratteggiata ) mediante retrazione della guida metallica da 0 , 035 inch rastremata distalmente , d retrazione della seconda ancora ( freccia tratteggiata ) a livello del sito dentrata gastrico ove gi presente la prima ancora ( freccia ) , e inserzione del catetere gastrostomico da 12 fr in cavit gastrica , notare le due ancore ( freccia , freccia tratteggiata ) , f controllo nale con mezzo di contrasto . 362 radiol med ( 2013 ) 118 : 356365 talisation or required surgery were classied as major ; all others were classied as minor [ 12 ]  . 
the anchors were released within the gastric lumen 710 days after the procedure . results the technical success rate of single - puncture prg with two anchors placed through the gastrostomy tract was 100% ( 163 / 163 patients )  . 
in 158 patients ( 97% ) percutaneous access was achieved along the linea alba and in the remaining ve ( 3% ) along the aponeurosis between the rectus and oblique abdominal muscles . 
the average time required by gastropexy and placement of the gastrostomy catheter was 9 ( range 412 ) mduring the procedure , uoroscopy was pulsed ( four pulses / s ) , with a mean overall uoroscopy time of 1 m12 s ( range 33 s to 4 min and 52 s )  . mortality at 30 days from the procedure was 1.2% ( 2 / 163 patients )  . 
major complications at 30 days occurred in three patients ( 1.8% ) : two gastric haemorrhages and one pneumoperitoneuthe two gastric haemorrhages were related to the probable bleeding of a collateral branch of the gastroepiploic artery caused by an erroneous too caudal gastric puncture . 
minor complications at 30 days occurred in ten patients ( 6.1% ) : eight malfunctions of the gastrostomy catheter , one leakage of gastric contents through the insertion site and one breakage of the gastrostomy catheter . 
 no patient developed either skin infection or pain related to the presence of the gastropexy anchors . discussion both radiological and endoscopic percutaneous gastrostomy techniques have replaced surgical gastrostomy , as they do not require general anaesthesia and are less invasive , with lower guinamento di un ramo collaterale dellarteria gastroepiploica , per lerronea puntura gastrica troppo caudale . 
le complicanze minori a 30 giorni si sono vericate in 10 pazienti ( 6 , 1% ) : 8 malfunzionamenti del catetere gastrostomico , 1 fuoriuscita di materiale gastrico attraverso il tramite cutaneo e 1 rottura del catetere gastrostomico . 
inne , il caso di rottura del catetere gastrostomico stato trattato con successo mediante rimozione e sostituzione di questultimo con uno analogo di medesimo diametro ( 12 fr )  . 
nessun paziente ha sviluppato infezione cutanea n dolore dovuto alla presenza delle ancore da gastropessi . discussione le tecniche di gastrostomia percutanea , sia quella radiologica che quella endoscopica , hanno rimpiazzato la gastrostomia chirurgica , sia per lassenza di anestesia generale sia per la ridotta invasivit e morbilit [ 13 ]  . 
il notevole vantaggio della tecnica radiologica , rispetto a quella endoscopica , il possibile superamento di quasi tutte le stenoostruzioni dellipofaringe o esofagee mediante il catetere angiograco , il quale permette lindispensabile insufazione di aria allinterno della cavit gastrica [ 14 ]  . la gastropessi mediante ancore a t un ulteriore strumento nellarmamentario del radiologo interventista . 
essa ha due funzioni principali : la prima di stabilizzare la parete anteriore dello stomaco durante la procedura di prg evitando il possibile dislocamento del catetere gastrostomico a livello intraperitoneale con conseguente peritonite ; la seconda di garantire una pi rapida maturazione della stomia gastrocutanea , riducendo la probabilit di fuoriuscita di materiale gastrico attraverso il tramite cutaneo , di rottura del tramite stesso e di emorragia nei giorni successivi alla procedura [ 1 , 9 , 15 ]  . 
the signicant benet of the radiological approach compared with endoscopy is its ability to cross all stenoses / obstructions of the hypopharynx or oesophagus with the angiography catheter , which allows the necessary step of insufating air inside the gastric cavity [ 14 ]  . gastropexy with t - fasteners is an additional tool in the interventional radiologists armamentariuit serves two main functions : the rst is to stabilise the anterior stomach wall during the prg procedure , thus avoiding any intraperitoneal displacement of the gastrostomy catheter , which may result in peritonitis ; the second is to ensure faster maturation of the stoma , reducing the likelihood of gastric content leaking though the stoma tract , of catheter breakage and of bleeding in the days following the procedure [ 1 , 9 , 15 ]  . 
with the single - anchor technique , which requires a single puncture only [ 11 ] , the anchor is placed through the preloaded 17 - gauge introducer needle by pushing a metal guidewire within the introducer needle itself . 
indeed , while placing the dilators on the guide , the anchor is pulled to prevent the anterior wall from being pushed back by the abdominal wall , which may occasionally cause damage to the gastrostomy tract or rupture of the anchor itself , with consequent migration into the peritoneal cavity through the gastrostomy tract [ 11 ]  . 
additionally , the use of a single anchor can produce considerable tension in a single site , causing gastric wall ischaemia , with possible necrosis and nally widening of the gastrocutaneous stoma [ 11 , 16 ]  . 
therefore , the use of a single anchor through the same tract as used by the gastrostomy catheter might not be adequate for gastropexy for the following reasons : possible rupture of the anchor during the prg manoeuvre , possible damage to the gastric wall ( ischaemia / haemorrhage ) , possible migration of the anchor and gastrostomy catheter into the peritoneal cavity [ 11 ]  . the technique with two or more anchors ( generally up to four ) requires that they be inserted through the introducer needle either laterally ( two - anchor technique ) or so as to form a triangle ( three - anchor technique ) or a square ( fouranchor technique ) with reference to the future route of the gastrostomy catheter . 
after placing the gastropexy anchors , gastrostomy is performed according to the following steps : puncture of the anterior stomach wall at the centre of the gastropexy anchors , placement of a stiff metal guidewire through the needle , progressive widening of the gastrostomy tract and , nally , placement of the gastrostomy tube . 
the risk of bleeding therefore theoretisola ancora , che prevede una sola puntura [ 11 ] , lancora viene posizionata attraverso il pre - caricato ago - introduttore da 17 gauge mediante la spinta di una guida metallica allinterno dellago - introduttore stesso . 
tuttavia , la tecnica con singola puntura e posizionamento di una sola ancora , pur essendo una procedura semplice e rapida , non risulta essere priva di rischi e di complicanze . 
infatti , durante il posizionamento dei dilatatori sulla guida , lancora viene tirata per impedire che la parete anteriore venga spinta in profondit dalla parete addominale , creando occasionalmente un danno a livello del tramite gastro - cutaneo o la rottura dellancora stessa con conseguente migrazione di questultima nella cavit peritoneale attraverso il tramite [ 11 ]  . 
in aggiunta luso di una singola ancora pu creare una considerevole tensione in un singolo punto , creando quindi danni ischemici alla parete gastrica , con possibile necrosi ed in ultimo allargamento della stomia gastro - cutanea [ 11 , 16 ]  . 
pertanto , luso di una singola ancora attraverso lo stesso tragitto del catetere gastrostomico potrebbe risultare essere non adeguato per la gastropessi per i seguenti motivi : possibile rottura dellancora durante la manovra di prg , possibile danno alla parete gastrica ( ischemia / emorragia ) , possibile migrazione in cavit peritoneale dellancora e del catetere gastrostomico [ 11 ]  . la tecnica mediante il posizionamento di due o pi ancore ( in genere no ad un massimo di quattro ) , prevede il posizionamento delle ancore stesse , attraverso lago - introduttore , lateralmente ( tecnica a due ancore ) , a triangolo ( tecnica a tre ancore ) o a quadrato ( tecnica a quattro ancore ) rispetto al futuro tragitto del catetere gastrostomico . 
posizionate le ancore da gastropessi , viene eseguita la gastrostomia secondo i seguenti passaggi : puntura della parete anteriore dello stomaco al centro delle ancore da gastropessi , posizionamento di guida metallica rigida attraverso lago , dilatazione progressiva del tramite ed , inne , posizionamento del catetere gastrostomico . 
di conseguenza , il rischio di emorragia teoricamente aumentato proporzionalmente allaumentare del numero di punture , e quindi , del numero di ancore [ 11 ]  . la nostra tecnica prevede la singola puntura e il posizionamento di due ancore attraverso lo stesso tragitto del catetere gastrostomico . 
furthermore , it makes it easier to enter the gastric cavity in the middle portion between the gastric antrum and body or gastric body itself ( preventing puncturing major branches of the gastric or gastroepiploic arteries ) , thus minimising the risk of bleeding . 
as reported in the literature , and in our opinion , placement of at least two anchors ensures good stability of the anterior stomach wall during prg and faster maturation of the stoma [ 11 , 17 ]  . 
in our experience , compared with the two techniques we performed in the past that is , multiple anchors around the gastrostomy catheter or a single anchor placed in the same tract as the catheter itself we believe that a single puncture combined with gastropexy with two anchors placed in the same tract as the gastrostomy catheter is the best solution to ensure a fast prg procedure , with less trauma and greater safety . our data regarding major ( 1.8% ) and minor ( 6.1% ) complications are encouraging , compared with our previous experience with conventional techniques and with the literature , which reports 8% for major [ 1315 , 18 ] and 12% for minor [ 9 , 13 , 14 , 18 ] complications . 
 two other technical details , which should not be underestimated in our opinion , are the placement of a gauze pad on the anchor threads at skin level and antibiotic prophylaxis . 
 placing a gauze pad on the anchor threads allows lowering of the excessive pressure exerted by the anchors on the gastric mucosa and skthe reduced tension ensures lack of pain in the days following the procedure . 
we agree with other authors [ 1 , 14 ] that the anchors should be removed after 710 days , as it ensures a good and stable adhesion between the gastric and abdominal wall , allowing the gastrostomy to mature , while preventing any possible foreign - body reaction and / or inammation . 
although there is no agreement regarding the need for antibiotic prophylaxis in prg procedures , we believe it to be necessary , as most patients are prone to infection in view of advanced age , impaired nutritional state , underlying disease and possible immunosuppression [ 21 ]  . 
come riportato in letteratura e anche a nostro giudizio , il posizionamento di almeno due ancore garantisce una buona stabilit della parete anteriore dello stomaco durante la prg e una pi rapida maturazione della stomia gastrocutanea [ 11 , 17 ]  . 
dalla nostra esperienza , confrontata con le altre due tecniche da noi eseguite in passato , ovvero tramite plurime ancore collocate attorno al catetere gastrostomico o mediante singola ancora posizionata nel medesimo tragitto del catetere stesso , riteniamo che la singola puntura abbinata alla gastropessi con due ancore collocate nello stesso tragitto del catetere gastrostomico sia la soluzione migliore per eseguire la procedura di prg in maniera rapida , meno traumatica possibile e maggiormente sicura . i dati della nostra casistica , riguardo alle complicanze maggiori ( 1 , 8% ) e minori ( 6 , 1% ) sono incoraggianti , comparati sia alla nostra precedente esperienza con tecniche tradizionali sia ai dati della letteratura , che arrivano sino all8% per le maggiori [ 1315 , 18 ] e sino al 12% per le minori [ 9 , 13 , 14 , 18 ]  . 
 altri due particolari tecnici , che a nostro parere non sono da sottovalutare , sono il posizionamento del tamponcino di garza sui li delle ancore a livello cutaneo e la prolassi antibiotica . 
il posizionamento del tamponcino di garza sui li delle ancore a livello cutaneo permette di ridurre leccessiva pressione esercitata dalle ancore a livello della mucosa gastrica e a livello cutaneo . 
noi siamo daccordo , come altri autori [ 1 , 14 ] , nel rimuovere le ancore a 710 giorni per garantire una stabile e buona adesione tra la parete gastrica e la parete addominale afnch maturi la gastrostomia , senza superare tale limite per evitare possibili reazioni da corpi estranei e / o inammazioni . 
per evitare o ridurre al minimo la possibile infezione , che una delle pi frequenti complicanze minori [ 14 ] , abbiamo eseguito una prolassi antibiotica in tutti i pazienti . 
non vi ancora un consenso in letteratura sulla necessit di eseguire o meno la prolassi antibiotica nella manovra di prg , ma noi riteniamo che essa sia necessaria considerato che la maggior parte dei pazienti sottoposti a tale procedura vulnerabile alle infezioni per let avanzata , lo stato nutrizionale compromesso , la patologia di base ed eventuali stati immunosoppressivi [ 21 ]  . 
questa nostra convinzione supportata da due meta - analisi che dimostrano lefcacia della terapia antibiotica nel ridurre le infezioni peristomali nella gastrostomia percutanea endoscopica [ 22 , 23 ]  . the use of smallto medium - sized catheters ( 1214 f ) might be considered a limitation of the percutaneous approach ; however , in our series , the eight cases ( 5% ) of cathlutilizzo di cateteri di piccolo - medio calibro ( 1214 fr ) potrebbe sembrare un limite della metodica percutanea , tuttavia nella nostra casistica i soli 8 casi ( 5% ) di malradiol med ( 2013 ) 118 : 356365 eter malfunction due to partial or total occlusion were all solved by advancing a metal guidewire through the catheter to revise it . 
the limitations of this study lie in the relatively small number of patients and its prospective observational nature . funzionamento del catetere gastrostomico per occlusione parziale o totale sono tutti risolti con revisione tramite passaggio al suo interno di guida metallica . 
i limiti di questo studio sono rappresentati dal numero relativamente basso di pazienti e dal suo carattere prospettico osservazionale . conclusions conclusioni prg with a single - puncture technique and placement of two anchors is a minimally invasive , fast , effective , welltolerated and safe procedure ensuring stable maturation of the gastrostomy . 
further prospective and randomised studies are required to conrm the superiority of this technique compared with the others described in the literature . la prg con tecnica di singola puntura e posizionamento di due ancore una procedura mini - invasiva rapida , efcace , ben tollerabile e sicura che garantisce una stabile maturazione della gastrostomia . 
biti1 1radiotherapy unit , department of medical and surgical critical care , university of florence , florence , italy 2molecular and nutritional epidemiology unit , ispo ( cancer research and prevention institute ) , university of florence , florence , italy 3department of surgery , department of medical and surgical critical care , university of florence , florence , italy 4diagnostic senology unit , department of medical and surgical critical care , university of florence , florence , italy 5division of pathological anatomy , department of medical and surgical critical care , university of florence , florence , italy correspondence to : icro meattini , radiotherapy unit , university of florence , largo g.a. 
brambilla 3 , 50134 florence , italy tel . : + 39 - 055 - 7947719 , fax : + 39 - 055 - 4379930 , e - mail : icro.meattini@uni.it received : 9 october 2011 / accepted : 4 december 2011 / published online : 9 august 2012 springer - verlag 2012 abstract purpose . 
at a median follow - up of 8.9 [ range , 0.620 ; standard deviation ( sd ) , 4.98 ] years , 32 patients ( 53.3% ) were alive and 16 patients died ( 26.7% ) due to disease progression and 12 ( 20% ) due to other causes . 
at univariate analysis for overall survival , pathological tumour size ( p = 0.031 ) , histological subtype ( p = 0.013 ) and nodal status ( p = 0.006 ) emerged as signicant predictors of death . 
abbiamo analizzato le caratteristiche clinico - patologiche di 60 pazienti affetti da carcinoma mammario maschile trattati presso la nostra unit di radioterapia in un periodo compreso tra il 1971 ed il 2011 . 
allanalisi univariata per sopravvivenza assoluta , le dimensioni patologiche del tumore ( p = 0 , 031 ) , listologia ( p = 0 , 013 ) e lo stato linfonodale ( p = 0 , 006 ) sono emersi quali signicativi predittori di morte . 
in considerazione della rarit della patologia , molti sono i temi ancora dibattuti e necessitano radiol med ( 2013 ) 118 : 476486 pathological tumour size and positive nodal status as unfavourable features for survival in male breast cancer . keywords male breast cancer prognostic factors surgery mastectomy breast - conserving surgery radiotherapy futuri studi collaborativi . 
 parole chiave carcinoma mammario maschile fattori prognostici chirurgia mastectomia chirurgia conservative della mammella radioterapia introduction introduzione male breast cancer ( mbc ) is a rare disease , accounting for < 1% of all malignancies in men and for only 1% of all incidents of breast carcinoma ( bc ) [ 1 ]  . 
 the annual prevalence of mbc in europe is 1 : 100 , 000 patients ; 900 new cases are diagnosed each year in the united states [ 3 ]  . mbc causes are incompletely characterised and understood . 
the rarity of the disease has precluded randomised clinical trials and made prospective studies difcult to conduct ; much of our knowledge regarding biology , natural history and treatment strategies for bc in men have been extrapolated from women [ 4 ]  . 
we conducted a retrospective analysis to evaluate the prognostic factors and management options of mbc treated in a single institution over a period of 40 years . il carcinoma mammario maschile ( mbc ) rappresenta una malattia rara , costituendo meno dell1% di tutte le neoplasie nelluomo e solo l1% di tutte le diagnosi di carcinoma mammario ( bc ) [ 1 ]  . 
la prevalenza annuale di mbc in europa di 1 ogni 100000 uomini ; negli stati uniti ogni anno vengono diagnosticati 900 nuovi casi [ 3 ]  . le cause del mbc non sono completamente caratterizzate e comprese ; inoltre la rarit della malattia ha precluso studi clinici randomizzati e ha reso difcoltosa la conduzione di studi prospettici ; la maggior parte delle conoscenze riguardo la biologia , la storia naturale e le strategie di trattamento del bc nei pazienti di sesso maschile sono state estrapolate da quelli di sesso femminile [ 4 ]  . 
abbiamo condotto unanalisi retrospettiva mono - istituzionale su di una popolazione di pazienti trattati presso il nostro istituto in un periodo di circa 40 anni , al ne di individuarne i maggiori fattori prognostici e lideale gestione del trattamento . materials and methods patients materiali e metodi pazienti from 1971 to 2011 , 60 patients affected by mbc were treated at our radiotherapy unit . 
patients were followed up at our centre every 6 months for 5 years after adjuvant treatment for mb , then annually until 10 years and then every 2 years . sessanta pazienti affetti da mbc sono stati trattati tra il 1971 e il 2011 presso la nostra unit di radioterapia . 
i pazienti sono stati successivamente controllati clinicamente presso il nostro centro ogni sei mesi per i primi cinque anni dal termine del trattamento adiuvante , poi annualmente no a dieci anni e successivamente ogni due anni . pathology methods metodi anatomo - patologici oestrogen receptor ( er ) and progesterone receptor ( pgr ) status were reviewed when available ; expression scores were based on percentages of positive nuclei over the total number of cancer cell nuclei counted . 
for er and pgr status , two categories ( negative / positive ) were considered lo stato recettoriale estrogenico ( er ) e progestinico ( pgr ) stato valutato quando disponibile ; il valore dellespressione espressione della percentuale di nuclei postivi sul totale di nuclei cellulari contati . 
per quanto riguarda lo stato di er e pgr sono state considerate due catego rie ( negativo / positivo ) in accordo con il ben noto valore 478 radiol med ( 2013 ) 118 : 476486 according to well - established cutoff values ( 10% for both er and pgr ) [ 5 ]  . 
 her - 2 immunohistochemistry ( ihc ) expression ( when available ) was scored , as follows : 0 , no or only faint membrane staining ; 1 + , faint membrane staining in > 10% of tumour cells or incomplete membrane staining ; 2 + , weak to moderate membrane staining in > 10% of tumour cells ; 3 + , intense circumferential membrane staining in > 10% of tumour cells . 
histological tumour grading was assessed according to elston and ellis [ 7 ]  . statistical analysis survival time was calculated from the date of surgery to the date of death , or for events or date of last follow - up for the patients who were still alive . 
local recurrence - free survival ( lrfs ) and distant - metastasis - free survival ( dmfs ) were calculated from the date of surgery to the date of lr and dm occurrence , respectively . 
the crude probability of death or lr / dm occurrence was estimated using the kaplanmeier method , and differences between patient groups were assessed by the log - rank test . 
estimated relative risks ( rr ) of dying or lr / dm occurrence were expressed as hazard ratios ( hr ) and their corresponding 95% condence intervals ( 95% ci )  . 
 lespressione immuno - istochimica ( ihc ) del gene her2 stata valutata come segue ( dove disponibile ) : 0 , non colorazione o minima colorazione di membrana ; 1 + , minima colorazione di membrana in > 10% delle cellule tumorali , colorazione di membrana incompleta ; 2 + , colorazione di membrana da debole a moderata in > 10% delle cellule tumorali ; 3 + , intensa colorazione di membrana circonferenziale in > 10% delle cellule tumorali . 
 il grado istologico del tumore stato valutato in accordo a elston e ellis [ 7 ]  . analisi statistica la sopravvivenza stata calcolata dalla data della chirurgia a quella della morte , per quanto riguarda gli eventi , o a quella dellultimo follow - up per i pazienti risultati viventi . 
la sopravvivenza libera da recidiva locale ( lrfs ) e da metastasi a distanza ( dmfs ) stata calcolata dalla data della chirurgia a quella di diagnosi di lr e / o dm , rispettivamente . 
la probabilit di decesso o lr / dm stata stimata usando il metodo di kaplan - meier e le differenze tra vari gruppi di pazienti sono state valutate attraverso log - rank test . 
il rischio relativo di morte o lr / dm stato espresso con hazard - ratio ( hr ) e il corrispondente intervallo di condenza del 95% ( 95%ci )  . 
stato utilizzato il software sas 9.1 ( sas institute , cary , ny )  . risultati caratteristiche dei pazienti let mediana della casistica alla diagnosi di carcinoma mammario stata di 62 anni ( range 2784 )  . 
la maggior parte erano casi di bc iniziale ( stadio i - ii : 41 pazienti , 68 , 3% ; stadio iii : 19 pazienti , 31 , 7% ) , con istotipo duttale invasivo ( 83 , 3% ) e stato linfonodale negativo ( 51 , 7% )  . 
 twenty - six patients received adjuvant radiotherapy ( rt ) ; treatment volumes were chest wall and regional nodes in six patients and exclusively chest wall in 18 cases ; two patients received rt after bcs . 
er and / or pgr tey ( 33 , 3% ) ; due pazienti ( 3 , 3% ) sono stati sottoposti a chirurgia conservativa della mammella ( bcs )  . 
 nella nostra casistica , 26 pazienti hanno ricevuto radioterapia ( rt ) adiuvante ; i volumi di trattamento sono consistiti nella parete toracica e drenaggi linfonodali regionali in 6 pazienti , nella parete toracica esclusiva in 18 casi ; due pazienti hanno ricevuto rt dopo bcs . 
at univariate regression analysis for os ( table 2 ) , pathological tumour size ( p = 0.031 ) , histological subtype ( p = 0.013 ) and nodal status ( p = 0.006 ) emerged as signicant death predictors . ( range 0 , 64 , 8 ; sd 1 , 6 )  . 
allanalisi univariata ( tabella 1 ) , nessun parametro emerso come predittore signicativo di lr ; le dimensioni patologiche della neoplasia ( p = 0 , 015 ) e lo stato linfonodale ( p = 0 , 009 ) sono invece emersi come predittori signicativi di dm ; un effetto borderline stato evidenziato per la variante istologica ( p = 0 , 056 ) e let alla diagnosi ( p = 0 , 076 )  . per quanto riguarda la sopravvivenza assoluta ( os ) , ad un follow - up mediano per lintera serie di 8 , 9 anni ( range 0 , 620 ; sd 4 , 98 ) , 32 pazienti ( 53 , 3% ) risultano attualmente viventi , mentre 16 ( 26 , 7% ) sono deceduti a causa della malattia e 12 ( 20% ) per altre cause . 
advanced tumour size ( p = 0.0021 ) , positive nodal status ( p = 0.0008 ) and mbc diagnosis before the year 2000 ( p = 0.0049 ) emerged as independent signicant dm predictors ; no features were found to be independent predictors of lr . discussion epidemiology and genetic factors the incidence of mbc in western countries is about 0.5 : 100 , 000 men per year , with a median age at presentae la variante istologica cribriforme invasiva ( p = 0 , 0003 )  . 
 una maggiore dimensione del tumore ( p = 0 , 002 ) , lo stato linfonodale positivo ( p = 0 , 0008 ) e la diagnosi di mbc avvenuta prima dellanno 2000 ( p = 0 , 0049 ) , sono emersi come predittori indipendenti di dm ; nessun parametro risultato predittore indipendente di lr . discussione epidemiologia e fattori genetici lincidenza di mbc nei paesi occidentali di 0 , 5 per 100000 uomini per anno , con un et alla presentazione mediana di 68 anni [ 2 ]  . 
la maggioranza degli uomini con bc non hanno fattori di rischio identicabili , anche se negli anni vi sono susseguite numerose teorie riguardo la genesi della malattia [ 813 ]  . 
il carcinoma duttale invasivo rappresenta il sottotipo predominante , rappresentando approssimativamente il radiol med ( 2013 ) 118 : 476486 table 3 multivariate analysis ( cox regression models ) with selection of parameters to identify the most signicant predictors of death and disease relapse variable parameter hr ( 95% ci ) death predictors pt 34 vs . 
medullary , tubular , papillary , small - cell and mucinous carcinoma constitute < 15% of cases [ 14 ] ; lobular carcinoma is a rare occurrence [ 15 ]  . 
 in our series , the most represented histology was invasive ductal carcinoma , which resulted in a protective role in terms of os ( p < 0.003 ) when compared with other histological subtypes . 
this represents an unexpected nding ; invasive cribriform carcinoma is known as a rare subtype of invasive bc usually associated with an excellent prognosis [ 16 ]  . pathological features pathological tumour size and nodal status are the main prognostic factors in mbc . 
 [ 17 ] found a 40% higher risk of death in men with a tumour > 2 csimilarly , men with nodal involvement have a 50% higher risk of death than node - negative patients [ 18 ]  . 
le varianti midollare , tubulare , papillare , a piccole cellule e mucinoso costituiscono meno del 15% dei casi [ 14 ] ; il carcinoma lobulare rappresenta unevenienza rara [ 15 ]  . 
nella nostra esperienza listologia pi rappresentata stata il carcinoma duttale invasivo , che risultata essere protettiva in termini di os ( p < 0 , 003 ) , se confrontata con le altre istologie . 
questo dato rappresenta un risultato inatteso ; il carcinoma cribriforme invasivo noto per essere un raro , unico sottotipo di bc invasivo caratterizzato da una prognosi eccellente [ 16 ]  . caratteristiche patologiche la dimensione patologica della neoplasia e lo stato linfonodale rappresentano i fattori prognostici principali nel mbc . 
 [ 19 ] , in uno studio retrospettivo di coorte su 246059 pazienti di sesso maschile e femminile registrati nel national cancer institutes surveillance , epidemiology , and end results ( seer ) , hanno riscontrato una mortalit da bc signicativamente maggio484 radiol med ( 2013 ) 118 : 476486 erlich et al . 
 [ 19 ] , in a retrospective , population - based cohort study of 246 , 059 men and women with bc recorded in the national cancer institutes surveillance , epidemiology , and end results ( seer ) , found a signicantly greater bc - specic mortality rate in stage i disease for men than for women . 
in line with the major published studies , we found a signicant impact of pathological tumour stage and nodal involvement on dm and os rate ; in 2011 , these features still represent the principal predictors of outcome of mbc patients . surgery and adjuvant treatment local treatment for bc is usually the same in men and women . 
from data found in the literature , modied radical mastectomy is used in approximately 70% of patients , followed by radical mastectomy ( 830% ) , total mastectomy ( 514% ) , and bcs with or without rt ( 113% ) [ 19 ]  . 
 historically , radical mastectomy was often performed , probably due to practice patterns and later stage at diagnosis in older series , but retrospective studies indicate that the outcome for men is equally good when treated with less invasive surgery [ 20 , 21 ]  . 
in recent years , according to clinical practice in women , sentinel node biopsy has been evaluated in men [ 2224 ] , but due to the rarity of this disease , large studies establishing the sensitivity and specicity of sentinel node biopsy are not possible . 
many series showed a better lrfs without a survival benet [ 22 , 2529 ]  . the majority of our cases received radical surgery with lla ; 43.3% of patients underwent adjuvant rt . 
due to the small size of the study sample and the long observation period , our analysis evidenced no predictor of lr occurrence ; however , a borderline effect on dm occurrence was found for year of diagnosis ( p = 0.076 ) , probably due to improved diagnostic tools , surgical procedures and rt techniques . 
we do think that the real benet of adjuvant rt should be addressed in future collaborative studies . data supporting a signicant benet of ct in women with bc are well established , whereas little information is re nel sesso maschile nello stadio i di malattia . 
in accordo con i maggiori studi offerti dalla letteratura internazionale , abbiamo evidenziato un signicativo impatto della dimensione patologica della neoplasia e dellinteressamento linfonodale nel tasso di incidenza di dm e os ; nel 2011 questi elementi sembrano ancora rappresentare i pi importanti fattori prognostici nel mbc . chirurgia e trattamento adiuvante il trattamento locale del bc solitamente il medesimo nelluomo e nella donna . 
dati di letteratura dimostrano come neluomo la mastectomia radicale modicata rappresenti approssimativamente il 70% delle procedure , seguita dalla mastectomia radicale ( 8%30% ) , dalla mastectomia totale ( 5%14% ) , e dalla chirurgia conservativa della mammella seguita o meno dalla rt ( 1%13% ) [ 19 ]  . 
 storicamente la mastectomia radicale stato lintervento maggiormente effettuato , probabilmente a causa dellesperienza routinaria e della stadiazione solitamente avanzata al momento della diagnosi in questi pazienti ; tuttavia , studi retrospettivi hanno indicato come la prognosi nei pazienti di sesso maschile sia comparabile quando trattati con chirurgia meno invasiva [ 20 , 21 ]  . 
in anni recenti , in accordo con la pratica clinica nelle donne , stato valutato anche negli uomini la possibilit di eseguire lanalisi del linfonodo sentinella [ 2224 ] , ma a causa della rarit della malattia , non sono possibili ampi studi che chiariscano la reale sensibilit e specicit di tale procedura . pochi dati sono disponibili in letteratura riguardo lutilizzo di rt adiuvante nel mbc . 
numerose casistiche hanno evidenziato una miglior lrfs senza un vantaggio in termini di sopravvivenza assoluta [ 22 , 2529 ]  . la maggior parte dei nostri casi stata sottoposta a chirurgia radicale seguita da lla ; il 43 , 3% dei pazienti ha effettuato rt adiuvante . 
in considerazione della limitazione numerica del campione e del lungo periodo di osservazione , la nostra analisi non ha evidenziato alcun predittore signicativo di lr ; tuttavia un effetto border - line in termini di rischio di dm stato riscontrato per lanno di diagnosi di malattia ( p = 0 , 076 ) , probabilmente a causa del miglioramento degli strumenti diagnostici e delle procedure chirurgiche e allo sviluppo di pi rafnate tecniche radioterapiche . 
in particolare non abbiamo trovato differenze statisticamente signicative in termini di os nei pazienti che hanno effettuato rt dopo la chirurgia , anche se i pazienti radiotrattati hanno una miglior lrfs ( 95 , 8% versus 85 , 3% )  . 
noi siamo fermamente convinti che il reale benecio della rt adiuvante andrebbe valutato in futuri studi collaborativi . dati a supporto di un signicativo benecio nei confronti della ct in donne affette da bc sono ben consolidati , mentre poche sono le evidenze disponibili per quanto riguarradiol med ( 2013 ) 118 : 476486 available with regard to male patients . 
there are no denitive data about use of trastuzumab in mbc [ 33 ] , but it should be considered also in men with her - 2 - positive status because of the signicant benet observed in women . the mainstay of systemic therapy for hormone - receptor positive mbc is ht . 
in our experience , ct and ht did not inuence outcome in mbc patients . da i pazienti di sesso maschile ; i lavori pubblicati tuttavia sembrano supportare un benecio analogo per le donne e per gli uomini [ 3032 ]  . 
non esistono dati denitivi riguardo luso di trastuzumab nel mbc [ 33 ] , ma considerando il signicativo benecio dimostrato nelle donne , bisognerebbe valutarne luso anche nei pazienti di sesso maschile con stato her - 2 positivo . il caposaldo della terapia sistemica nei pazienti affetti da mbc con stato recettoriale positivo rappresentato dalla terapia ormonale ( ht )  . 
tamoxifene il farmaco che stato maggiormente investigato [ 34 ] ; per quanto riguarda il ruolo degli inibitori dellaromatasi , non vi sono ancora evidenze sufcienti a supportare un loro utilizzo routinario nei pazienti mbc [ 35 ]  . 
 conclusions conclusioni despite the modern multimodality approach and improvement in diagnostic tools , surgical procedures , rt and systemic treatments , mbc remains a rare and complex disease , and future collaborative studies are required . 
our experience conrmed the prognostic role of greater pathological tumour size and positive nodal status as unfavourable features for survival in mbc . nonostante il moderno approccio multidisciplinare , il miglioramento degli strumenti diagnostici , lo sviluppo delle procedure chirurgiche , radioterapiche e delle terapie sistemiche , mbc rimane ancora una malattia rara e complessa , che necessita di futuri studi collaborativi . 
three - dimensional ra provides a virtual view of the surgical eld with the same orientation required for the surgical approach and , compared with surgical ndings , reliably dened location , orientation , morphology and relationship with parent vessels of the aneurysm in all cases . 
lo studio rotazionale stato sempre eseguito con singola iniezione di 20 cc di mezzo di contrasto ( mdc ) del vaso afferente alla lesione dopo panangiograa cerebrale diagnostica nelle due proiezioni ortogonali . 
la 3dra ha permesso la visualizzazione virtuale del campo operatorio con lorientamento necessario per lapproccio chirurgico e , confrontata con i reperti chirurgici , in tutti i casi ha denito con estrema afdabilit la sede , lorientamento , la morfologia e il rapporto con i vasi parenti dellaneurisma . 
la 3dra una metodica afdabile per la valutazione preliminare degli aneurismi cerebrali candidati ad intervento chirurgico in termini di previsualizzazione del campo operatorio e studio delle caratteristiche della lesione , utili per interventi pi rapidi e sicuri . 
la metodica inoltre consente di ridurre signicativamente il numero di proiezioni angiograche e quindi la dose di esposizione e mdc al paziente . keywords cerebral angiography intracranial aneurysm neurosurgery imaging three - dimensional imaging aneurysm clipping parole chiave angiograa cerebrale aneurisma intracranico neurochirurgia imaging 3d clipping introduction introduzione cerebral aneurysms are potentially at risk of subarachnoid haemorrhage ( sah ) , which is associated with high morbidity , and a mortality rate of approximately 26% [ 1 ]  . 
in recent decades , the development and improvement of equipment and materials in the eld of interventional neuroradiology have made it possible to promote percutaneous treatment , which is associated with fewer risks and complications compared with conventional surgery [ 2 , 3 ]  . 
digital angiography is still considered the gold standard for assessing cerebral aneurysms compared with noninvasive imaging modalities [ 5 , 6 ]  . after having evaluated the advantages of three - dimensional rotational angiography ( 3dra ) in the endovascular treatment of intracranial aneurysms in a previous paper [ 7 ] , we analysed its usefulness as a systematic preliminary examination in a population of patients undergoing conventional craniotomy and evaluated its potential in the postoperative follow - up . materials and methods we retrospectively evaluated 100 patients treated with craniotomy and aneurysm clipping over a 3 - year period between november 2007 and november 2010 after obtaining approval of the study by the local ethics committee . 
vascular lesions in the remaining 68 cases were incidental ndings in patients undergoing brain magnetic resonance ( mr ) imaging for a variety of clinical questions , and 18 / 68 had multiple aneurysms . 
sites of the 111 aneurysms treated are summarised in table 1 . gli aneurismi cerebrali rappresentano una patologia potenzialmente a rischio di emorragia subaracnoidea ( esa ) alla quale associata unelevata morbilit e una mortalit di circa il 26% [ 1 ]  . 
negli ultimi decenni , lo sviluppo e il miglioramento delle apparecchiature di imaging diagnostico e dei materiali nellambito della neuroradiologia interventistica , ha permesso di favorire il trattamento percutaneo , gravato da minori rischi e complicanze , rispetto alla chirurgia tradizionale [ 2 , 3 ]  . 
tuttavia , in alcune situazioni cliniche e anatomiche sfavorevoli la chirurgia subentra ancora quale trattamento di prima istanza [ 4 ] e , come per la terapia endovascolare , pu avvantaggiarsi del work - up di imaging preliminare che , utilizzato ai ni della strategia dapproccio , ne pu condizionare lesito e i rischi correlati . 
 attualmente langiograa digitale da considerarsi ancora esame gold - standard per la valutazione degli aneurismi cerebrali rispetto alle metodiche di imaging non invasivo [ 5 , 6 ]  . dopo aver valutato i vantaggi dellimpiego dellangiograa rotazionale 3d ( 3dra ) ai ni del trattamento endovascolare in un precedente lavoro [ 7 ] , in questo studio analizziamo lutilit di tale strumento diagnostico quale sistematico esame preliminare in una popolazione di pazienti sottoposti ad intervento chirurgico craniotomico tradizionale e ne valutiamo le potenzialit nel controllo postoperatorio . materiali e metodi sono stati valutati retrospettivamente 100 pazienti trattati con intervento di craniotomia e apposizione di clip metalliche per aneurisma cerebrale in 3 anni dal novembre del 2007 al novembre del 2010 , dopo approvazione del lavoro da parte del comitato etico interno . 
le lesioni vascolari nei restanti 68 casi costituivano reperto occasionale in pazienti radiol med ( 2013 ) 118 : 415430 table 1 distribution of treated 111 intracranial aneurysms in 100 patients treated by surgery showing number , percentage and anatomical site mca bifurc , middle cerebral artery bifurcation ; acoma , anterior communicating artery ; ic bifurc , internal carotid bifurcation ; pcoma , posterior communicating artery ; ophthalm ic , ophthalmic internal carotid ; terminal ic , terminal internal carotid tabella 1 distribuzione degli aneurismi cerebrali operati . 
sono elencati il numero , la percentuale e la sede anatomica di 111 aneurismi trattati chirurgicamente in 100 pazienti n ( % ) 28 ( 25 ) 25 ( 23 ) 21 ( 19 ) 15 ( 13 ) 12 ( 11 ) 10 ( 9 ) n ( % ) 28 ( 25 ) 25 ( 23 ) 21 ( 19 ) 15 ( 13 ) 12 ( 11 ) 10 ( 9 ) site mca bifurc . acoma ( a1 - a2 ) ic bifurc . pcoma ophthalic terminal ic sede biforcazione acm acoma ( a1 - a2 ) biforcazione ci acomp ci tratto oftalmico ci terminale acm , arteria cerebrale media ; acoma , arteria comunicante anteriore ; ci , carotide interna ; acomp , arteria comunicante posteriore angiography all patients underwent conventional 2d angiography supplemented with a 3dra acquisition ( philips allura xper fd 20 monoplane system with at - panel detector ) prior to surgery and a similar angiographic examination within days or weeks after the surgical procedure . 
in all cases , two 2d orthogonal projections [ anteroposterior ( ap ) and laterolateral ( ll ) , supplemented by an oblique projection in some cases ] were obtained for each selectively opacied brain - supplying vessel . 
during the examination , the subsequent rotational acquisition was always obtained with selective catheterisation of the vessel supplying the aneurysm ( s ) ( internal carotid or vertebral artery ) with a single injection of 1520 cc of nonionic iodinated contrast material at a ow rate of 34 ml / s and 240 rotation of the c - arm in propeller mode . 
immediately after rotational acquisition and within seconds of receiving the nonsubtracted angiographic series via a network connection , the systems software ( workstation integris 3dra ) automatically generated the 3d model with a 5123 matrix . 
from this , volume rendering ( vr ) and sottoposti a risonanza magnetica ( rm ) cerebrale per diversi quesiti clinici e 18 / 68 erano affetti da aneurismi multipli . 
la sede di complessivi 111 aneurismi operati riassunta nella tabella 1 . angiograa tutti i pazienti sono stati sottoposti ad un esame angiograco tradizionale 2d integrato da acquisizione 3dcon angiografo rotazionale ( 3dra ; angiografo rotazionale monoplano philips allura xper fd 20 con detettore at - panel ) preliminarmente allintervento chirurgico e ulteriore esame angiograco con le stesse modalit nei giorni o settimane successivi allintervento . 
lo studio angiograco cerebrale stato eseguito tramite accesso femorale in 98 casi ( 2 restanti casi con puntura diretta della carotide comune ) e sono sempre state acquisite 2 proiezioni ortogonali 2d [ antero - posteriore ( ap ) e latero - laterale ( ll ) , integrate in alcuni casi da 1 proiezione obliqua ] per singolo vaso cerebro - afferente opacizzato selettivamente . 
durante lesame , la successiva acquisizione rotazionale stata sempre effettuata mediante cateterizzazione selettiva del vaso afferente alla / e lesione / i aneurismatica / e ( carotide interna o arteria vertebrale ) con singola iniezione di 1520 cc di mezzo di contrasto ( mdc ) iodato non - ionico , usso a 34 ml / s e rotazione dellarco di 240 in modalit propeller . 
immediatamente al termine dellacquisizione rotazionale , dopo ricezione automatica della serie angiograca non sottratta attraverso una connessione di rete , il software dellapparecchiatura ( workstation integris 3d - ra ) in pochi secondi ha prodotto automaticamente il modello volumetrico in 3d con matrice di 5123 sul quale sono state poi scelte ricostruzioni in volume rendering ( vr ) e gradient rendering ( gr ) , valutabili in modalit multiproiettiva a 360 . 
sono stati preliminarmente esclusi 6 pazienti nei quali lesame angiograco con tecnica 3d non stato ritenuto valutabile a causa di eccessivi artefatti da movimento . tecnica chirurgica gli aneurismi sono stati trattati tramite craniotomia classica mediante approccio pterionale , frontale o fronto - pterionale con intervento mininvasivo e posizionamento di clip metalliche sul colletto aneurismatico . 
i reperti intraoperatori sono stati registrati su video - recorder . analisi dei dati la prima valutazione retrospettiva degli esami angiograci preoperatori stata effettuata per confrontare lafdabili418 radiol med ( 2013 ) 118 : 415430 gradient rendering ( gr ) reconstructions were chosen that could be evaluated in multiple projections over 360 . 
six patients were excluded from the analysis owing to excessive motion artefacts preventing evaluation of the 3d angiographic examination . surgical technique aneurysms were treated with conventional craniotomy with pterional , frontal or frontalpterional approach with a minimally invasive procedure and placement of metal clips on the aneurysm neck . 
the intraoperative ndings were recorded with a videocamera . data analysis a rst review of the preoperative angiograms was done to compare the reliability of the 3d model ( obtained with rotational acquisition with the possibility of multiple - projection analysis ) and the standard 2d images in identifying the aneurysm , after having dened intraand interobserver agreement of the two independent interventional neuroradiologists ( ap and mr , with 13 and 25 years of experience , respectively ) , who analysed the images in a blinded fashion . 
 aneurysm visualisation was graded on a 5 - point scale ( 1 , aneurysm not detected ; 2 , probably absent ; 3 , uncertain ; 4 , probably present ; 5 , denitely present )  . the readers then determined the reliability of 3dra in assessing : ( 1 ) morphology , ( 2 ) aneurysm site and orientation , ( 3 ) visualisation of the aneurysm neck and its relationship with the parent vessels on a 4 - point scale ( 1 , poor ; 2 , sufcient ; 3 , good ; 4 , excellent ) on each angiographic study . 
 after dening the interreader agreement , comparison of results was made directly with the intraoperative ndings analysed by two independent neurosurgeons ( ge and aa , with 7 and 16 years of experience , respectively ) who evaluated the ndings using the same numerical score . 
evaluation of lesion morphology took into account the visualisation of possible lobulations or accessory pouches . as concerns postoperative assessment , the 3d model and the 2d images in the standard conventional angiographic projections were analysed in a blinded fashion by the two neuroradiologists who assessed : ( 1 ) visualisation of the relationship between surgical clips and intracranial vessels , ( 2 ) possible vascular stenoses or occlusions caused by the clips , and ( 3 ) possible residual aneurysmal dilatations . 
la valutazione della visualizzazione dellaneurisma stata espressa con una scala di 5 punti ( 1 aneurisma non rilevato , 2 probabilmente assente , 3 incerto , 4 probabilmente presente , 5 certamente presente )  . successivamente stata determinata lafdabilit della tecnica 3dra nel valutare : ( 1 ) la morfologia , ( 2 ) la sede e lorientamento dellaneurisma e ( 3 ) la visualizzazione del colletto aneurismatico e il suo rapporto con i vasi parenti , utilizzando una scala di 4 punti ( 1 visualizzazione insufciente , 2 sufciente , 3 buona , 4 eccellente ) per ogni singola valutazione . 
per quanto riguarda la morfologia della lesione stata considerata la visualizzazione di eventuali lobulazioni o tasche accessorie . per quel che concerne il post - operatorio , il modello 3d e le immagini 2d nelle proiezioni angiograche tradizionali standard sono state analizzate in cieco dai due neuroradiologi che hanno valutato : ( 1 ) la visualizzazione del rapporto delle clip chirurgiche con i vasi intracranici , ( 2 ) eventuali stenosi o occlusioni vasali causati dalle clip e ( 3 ) eventuali residui delle lesioni aneurismatiche trattate . 
il confronto tra le due tecniche , anche in questo caso , stato effettuato su una scala espressa in 4 punti ( 1 visualizzazione insufciente , 2 sufciente , 3 buona , 4 eccellente ) e dopo valutazione dellagreement tra gli osservatori . analisi statistica lagreement tra gli osservatori stato determinato utilizzando lindice kappa di cohen , con intervallo di condenza del 95% . 
il confronto tra i valori di score medio ottenuti dalle singole valutazioni stato effettuato utilizzando il test dellanalisi della varianza ( anova ) con il post - test di tukey - kramer per identicare differenze signicative tra le singole medie dei vari gruppi . 
un valore di p < 0 , 05 stato considerato statisticamente signicativo . statistical analysis risultati interobserver agreement was determined using cohens il modello 3d ha richiesto un breve lavoro di post - procesradiol med ( 2013 ) 118 : 415430 kappa statistic with 95% condence interval ( ci )  . 
comparison between mean scores obtained from individual evaluations was made using the analysis of variance ( anova ) test with the tukeykramer post - test to identify any signicant differences between the single means of the various groups . 
 a value of p < 0.05 was considered to be statistically signicant . results the 3d model required some postprocessing to eliminate overlapping skeletal structures in a minority of cases ( 10 / 100 patients ) , in which less - than - optimal immobility produced moderate ghost artefacts . 
additional artefacts ( ve cases ) inherent to the technique and mainly consisting of incomplete distinction of contiguous vessels also required postprocessing with a second high - resolution reconstruction ; however , according to the observers , these artefacts did not hinder the interpretation of images to any signicant extent . 
in all other cases , selective opacication of the vessel being studied , without superimposition of venous vessels , allowed accurate volumetric imaging without the need for postprocessing . there were no signicant intraor interobserver differences between the two neuroradiologists independent evaluations after analysis of the preand postoperative 2d and 3d angiograms , nor were there any signicant differences between independent evaluations of intraoperative ndings by the two neurosurgeons . 
comparison of 2d and 3d angiographic technique reliability in preoperative aneurysm detection revealed a statistically signicant difference ( p < 0.001 ) in favour of the 3d technique ( table 2 )  . 
in 3 / 102 remaining cases , lobulations were either not conrmed at surgery or were considered to have insufcient visibility due to unfavourable location within the small surgical eld . visualisation of the aneurysm neck and its relationship with the parent vessels proved to be signicantly better on 3d angiograms compared with intraoperative ndings sing per eliminare dalle immagini le sovrastrutture scheletriche in pochi casi ( 10 / 100 pazienti ) nei quali la non perfetta immobilit del paziente ha prodotto moderati artefatti fantasma . 
pochi ulteriori artefatti ( 5 casi ) intrinseci alla metodica , e consistenti principalmente nellincompleta dissociabilit di vasi contigui , hanno richiesto il post - processing con una seconda ricostruzione ad alta risoluzione , ma tuttavia , a detta degli osservatori , non hanno limitato signicativamente linterpretazione diagnostica delle immagini . 
negli altri casi , la selettiva opacizzazione del vaso indagato , senza sovrapposizione di vasi venosi , ha permesso sempre di ottenere un accurato imaging volumetrico senza necessit di post - processing . non si sono registrate differenze signicative intrao interosservazionali tra le valutazioni indipendenti dei due neuroradiologi dopo analisi delle immagini angiograche 2d e del modello 3d pree post - operatori , n differenze signicative tra le valutazioni indipendenti dei due neurochirurghi nella descrizione dei reperti intraoperatori . 
la comparazione dellafdabilit delle due tecniche angiograche 2d e 3d nellidenticazione pre - operatoria degli aneurismi ha rilevato una differenza statisticamente signicativa ( p < 0 , 001 ) a favore della metodica tridimensionale rispetto allangiograa 2d standard ( tabella 2 )  . 
il modello 3d vr , grazie alla multiproiettivit , mostra un piccolo bleb aneurismatico ( c , freccia ) sulla carotide interna terminale , confermato chirurgicamente . radiol med ( 2013 ) 118 : 415430 fig . 
the 3d angiography well depicts site , orientation , morphology and relationship with the parent arteries of an aneurysm of the middle cerebral artery , allowing a virtual view of the surgical eld ( a )  . 
la tecnica angiograca 3d mostra in modo ottimale sede , orientamento , morfologia e rapporti con i vasi parenti di un aneurisma della biforcazione di arteria cerebrale media ( acm ) , permettendone la visualizzazione secondo linclinazione del campo operatorio ( a )  . 
 doppler ultrasound and / or intraoperative videoangiography ( 20 cases ) were necessary to achieve correct clip placement without inadvertently occluding one or more parent vessels . in addition , beyond statistical analysis , the virtually innite multiple projections that can be acquired with the tre le immagini angiograche tridimensionali hanno ottenuto un valore di score medio corrispondente ad un giudizio tra il buono e leccellente ( tabella 2 )  . 
tale potenzialit ha permesso in tutti i casi una pi accurata scelta dellapproccio chirurgico e del materiale da utilizzare preliminarmente alla craniotomia , come riferito dai neurochirurghi non coinvolti nellanalisi retrospettiva e che hanno operato con conoscenza dei reperti angiograci 3d . 
 nel post - operatorio per quel che concerne la visualizzazione del rapporto delle clip chirurgiche con i vasi parenti sono risultate migliori le immagini angiograche tridimensionali rispetto a quelle 2d standard con una differenza statisticamente signicativa ( p < 0 , 001 ) ( tabella 2 )  . 
le immagini 2d sono sempre state valutate dai neuroradiologi sia con modalit di sottrazione digitale , al ne di visualizzare in modo selettivo i vasi , sia con modalit senza sottrazione per visualizzare direttamente le clip . 
this allowed for a more accurate choice of surgical approach and material to be used , as reported by the neurosurgeons , who performed the surgical procedures on the basis of the 3d angiography images and were not involved in the retrospective analysis . 
 with regard to visualisation of the relationship between surgical clips and parent vessels in the postoperative period , 3d angiograms were signicantly better than standard 2d images ( p < 0.001 ; table 2 )  . 
the 2d images were always evaluated with and without digital subtraction in order to selectively visualise the vessels in the rst case and to directly visualise the clips in the second . 
sul modello 3d le immagini sono state giudicate insufcienti in 3 / 18 casi di vasospasmo / stenosi a causa di alcuni artefatti legati ad immagini di trasporto delle clip metalliche o a incompleta dissociabilit delle clip rispetto ai vasi dovuta al grado di opacit poco dissimile . discussione nonostante il trattamento endovascolare sia diventato di prima scelta dopo risultati e report ormai condivisi [ 3 ] e per ovvi motivi di mininvasivit e ridotti rischi legati alla procedura percutanea rispetto alla chirurgia open tradizionale , questultima ha ancora un ruolo determinante nel trattamento degli aneurismi cerebrali particolarmente complessi o in sedi spesso difcilmente controllabili per via endovascolare ( ad esempio , la biforcazione dellarteria cerebrale media ) , in caso di aneurismi giganti e / o con trombosi intra - aneurismatica o inne in urgenza nelle situazioni associate ad ematoma cerebrale [ 4 ]  . 
oggi la chirurgia per craniotomia dellaneurisma , grazie ai progressi tecnologici riguardanti i materiali , lutilizzo del microscopio e della navigazione guidata dai dati dellimaging , meno invasiva e pu essere molto efcace con ridotte sequele neurologiche rispetto al passato . 
langiograa digitale rappresenta ancora oggi lesame diagnostico fondamentale per la corretta valutazione degli aneurismi cerebrali , per consentire la scelta terapeutica pi appropriata tra il trattamento endovascolare e chirurgico e per fornire la guida essenziale nella strategia dapproccio in entrambi i tipi di intervento , permettendo di ridurne linvasivit e incrementarne lefcacia . 
the 3d image , oriented according to the surgical approach , shows a huge aneurysm of the middle cerebral artery bifurcation , with evidence of a small accessory pouch at the base near the neck ( a , arrow ) , the probable site of rupture . 
compared with surgery , the multiple - projection 3d images allow better distinction between aneurysmal neck and parent arteries ( d , arrow again shows the accessory aneurysmal pouch )  . 
postoperative 2d angiography adequately depicts an extensive aneurysmal remnant on the digitally subtracted anteroposterior view ( f , arrow ) but does not permit complete distinction of the parent arteries or visualisation of clips . 
limmagine angiograca 3d , orientata secondo lapproccio chirurgico , mostra un voluminoso aneurisma della biforcazione di acm con evidenza di una piccola tasca accessoria alla base vicino al colletto ( a , freccia ) , verosimile sede della rottura della sacca . 
il reperto confermato in sede intraoperatoria ( b , freccia ) ed apprezzabile un coagulo ematico sulla tasca ( c , freccia ) che ne conferma altrettanto la sede di rottura . 
rispetto alla chirurgia , le immagini 3d , con una diversa proiezione , permettono una migliore dissociazione di colletto aneurismatico e vasi parenti ( d , la freccia indica ancora la tasca accessoria dellaneurisma )  . 
 langiograa 2d post - operatoria mostra adeguatamente un ampio residuo aneurismatico sullimmagine a sottrazione digitale in proiezione ap ( f , freccia ) , ma non permette la completa dissociazione dei vasi parenti n la visualizzazione delle clip . 
il modello 3d ( h ) permette invece la visualizzazione selettiva e contemporanea delle clip ( freccia ) e dei vasi arteriosi secondo il piano operatorio ( confronta con e ) ; grazie alla multiproiettivit , mostra inoltre chiaramente i rapporti del residuo aneurismatico ( asterisco ) con le clip e permette unadeguata dissociazione dei vasi parenti ( i )  . 424 radiol med ( 2013 ) 118 : 415430 fig . 
the 3d angiography ( a ) at the level of the right internal carotid artery depicts three aneurysms affecting , respectively , the bifurcation ( solid arrow ) , the anterior choroidal artery infundibulum ( open arrow ) and the posterior communicating artery ( pcoma ) infundibulum ( dotted arrow )  . 
a surgical eld of view orientation ( b , solid arrow : pcoma aneurysm and dotted arrow : choroidal aneurysm ) allows optimal preview of surgical ndings ( c , arrow : pcoma aneurysm ; d , white arrow : clip on the pcoma aneurysm neck ; black arrow : anterior choroidal aneurysm )  . 
postoperative digitally subtracted 2d angiogram with standard projections shows stenosis at the origin of the a1 tract of the right anterior cerebral artery ( e , small arrow ) ; clips are roughly visible thanks to ghost artefacts ( e , f , large arrows )  . 
langiograa 3d ( a ) identica sulla stessa carotide interna destra 3 aneurismi rispettivamente della biforcazione del vaso ( freccia piena ) , dellinfundibolo di corioidea anteriore ( freccia vuota ) e dellinfundibolo di arteria comunicante posteriore ( acomp ; freccia tratteggiata )  . 
la proiezione orientata secondo il piano operatorio ( b , freccia piena : aneurisma di acomp e freccia tratteggiata : aneurisma di corioidea ) consente la ottimale previsualizzazione dei reperti chirurgici ( c , freccia : aneurisma di acomp ; d , freccia bianca : clip posizionata sullaneurisma di acomp e freccia nera : aneurisma di corioidea anteriore )  . 
langiograa 2d post - operatoria secondo le due proiezioni standard con tecnica sottratta mostra una stenosi allorigine del tratto a1 dellarteria cerebrale anteriore ( aca ) destra ( e , freccia piccola ) e in modo appena percettibile le clip grazie a tenui artefatti fantasma ( e , f , frecce grandi )  . 
il modello 3d , orientato secondo diverse proiezioni , chiarisce i rapporti delle clip con i vasi arteriosi ( g , confronta con f ; h , frecce : le clip posizionate sulle lesioni di corioidea e acomp ) , lassenza di residui aneurismatici , e conferma la stenosi del tratto a1 causato da una clip metallica ( i , freccia )  . radiol med ( 2013 ) 118 : 415430 fig . 
the 2d digitally subtracted angiography with standard views ( a , b ) shows postoperative ndings : clips are visible because of ghost artefacts ( arrows ) , and there is no evidence of any aneurysm sac remnant . 
langiograa 2d secondo le proiezioni standard ( a , b ) con tecnica di sottrazione mostra gli esiti dellintervento , con visibilit delle clip per artefatti fantasma ( frecce ) e senza apparenti residui di sacca aneurismatica . 
today , technological advances in materials , the use of the microscope and image - guided navigation have made aneurysm repair through craniotomy less invasive and highly effective , with fewer neurological sequelae than in the past . 
digital angiography is still the fundamental diagnostic examination for correct evaluation of cerebral aneurysms , tomograa computerizzata ( tc ) e langio - rm ] , rispetto a un decennio fa , divenuto molto competitivo e , ai ni diagnostici della individuazione e rappresentazione degli aneurismi , si avvia senzaltro a sostituire la metodica invasiva in breve tempo , pi che altro nei centri ove non esista una pronta disponibilit neurointerventistica per procedure endovascolari . 
in particolare langio - tc , mediante le apparecchiature multi - slice di ultima generazione ( 64 e 320 row ) e grazie ad accorgimenti quali la tecnica di sottrazione digitale , attualmente in grado di fornire quasi tutti gli elementi diagnostici necessari per la pianicazione dellatto chirurgico [ 8 ] , con alcuni limiti per le lesioni di piccole dimensioni e vicine alle strutture ossee . 
ma se pure i progressi della tecnologia hanno reso le indagini non invasive molto afdabili , tuttavia la maggiore risoluzione spaziale , la selettivit dello studio contrastograco dei singoli vasi , nonch la possibilit di procedere direttamente allatto terapeutico endovascolare durante la stessa seduta diagnostica , re426 radiol med ( 2013 ) 118 : 415430 as it helps the surgeon choose between endovascular and surgical treatment , provides a roadmap for either approach , reduces invasiveness and increases efcacy . 
in particular , cta , with latest - generation multislice scanners ( 64 and 320 detector rows ) and techniques such as digital subtraction , is able to provide almost all the diagnostic information required for planning the surgical procedure [ 8 ] , albeit with some limitations in small lesions close to bony structures . 
however , although technological progress has made noninvasive imaging highly reliable , the greater spatial resolution , selective opacication of individual vessels and the possibility of directly treating the lesion during the same imaging session , have all contributed to the superiority of angiography compared with noninvasive modalities [ 57 , 911 ]  . 
in addition , studies focusing on the potential of noninvasive imaging as a stereotactic guide for surgery have had very little inuence on microsurgical clipping of aneurysms [ 12 ]  . 
additionally , the recent advent of rotational acquisition with volumetric reconstructions has increasingly gained acceptance and produced convincing results for studying other areas also , such as spine , biliary tract and visceral and peripheral vessels and to guide therapeutic procedures in those areas [ 13 ]  . 
our results on a large patient population conrm those reported by several smaller case series or preliminary studies [ 7 , 912 , 1417 ] , as well as the large studies of van rooij et al . , which compared the techniques ability with standard angiography to detect aneurysms [ 18 , 19 ] and fenestration of intracranial arteries [ 20 ]  . 
firstly , thanks to multiple projections and volumetric surface evaluation , the technique can detect a larger number of aneurysms than can 2d angiography , particularly in lesions 2mm or obscured by overlapping cerebral vessels at sites such as bifurcation of the middle cerebral artery , as reported by other authors [ 7 , 10 , 1719 ]  . 
in the neurosurgical literature , this observation is reected in the nding of small additional lesions missed by standard angiography and discovered during procedures on symptomatic lesions [ 18 , 21 ]  . 
 direct comparison between 3d imaging and surgery yielded similar results in the denition of site , orientation stano tuttora le caratteristiche che fanno dellangiograa una tecnica superiore rispetto alle metodiche non invasive [ 57 , 911 ]  . 
inoltre , i lavori incentrati sulle potenzialit dellimaging non invasivo quale guida anche stereotassica alla chirurgia , hanno inuenzato molto poco il clipping microchirurgico degli aneurismi [ 12 ]  . 
la stessa angiograa tradizionale tuttavia ora mostra i suoi limiti di fronte alle maggiori necessit richieste sia dalla terapia endovascolare che dalla chirurgia , e nellultimo decennio lavvento della tecnica rotazionale con ricostruzione volumetrica delle immagini sta trovando sempre maggiori consensi e risultati convincenti , anche per lo studio e come guida a procedure terapeutiche in altri distretti , quali il rachide , le vie biliari o i vasi viscerali e periferici [ 13 ]  . 
i nostri risultati su unampia popolazione confermano i dati emersi da diversi studi su casistiche minori o con esperienze preliminari [ 7 , 912 , 1417 ] e dagli studi di van rooij et al . 
 [ 18 , 19 ] su ampie casistiche ma focalizzati rispettivamente sulla sola capacit della tecnica nellidenticazione degli aneurismi a confronto con langiograa standard o nellindividuazione di fenestrazioni dei vasi intracranici [ 20 ]  . 
in primo luogo , grazie alla multiproiettivit e valutazione volumetrica di supercie , questa tecnica in grado di individuare un maggior numero di aneurismi rispetto allangiograa 2d , prevalentemente in caso di lesioni di dimensioni 2 mm o nascoste dalla sovrapposizione dei vasi cerebrali in particolari sedi quale la biforcazione dellarteria cerebrale media , come riportato anche da diversi autori [ 7 , 10 , 1719 ]  . 
nella letteratura neurochirurgica tale dato ha un riscontro nel fenomeno del rilievo di piccole lesioni addizionali rimaste occulte allangiograa standard e scoperte durante interventi su lesioni sintomatiche [ 18 , 21 ]  . 
la dimostrazione dettagliata di lobulazioni della sacca aneurismatica fornisce indicazioni sulla probabile sede di avvenuta rottura delle lesioni in trattamento durgenza dopo esa , soprattutto in caso di aneurismi multipli ove pu essere difcile comprendere quale abbia provocato lemorragia . 
nella patologia trattata in elezione pu rappresentare invece un indice predittivo della sede pi fragile sulla sacca e / o dellaneurisma a maggior rischio di rottura [ 16 , 22 , 23 ]  . 
 unitamente alla possibilit di orientare il modello 3d per ottenere la visualizzazione virtuale del campo operatorio , lafdabilit della tecnica assume un ruolo decisivo ai ni della pianicazione dellintervento chirurgico per conosceradiol med ( 2013 ) 118 : 415430 and morphology of aneurysms . 
detailed depiction of aneurysm sac lobulations provides indications on the probable rupture site of aneurysms undergoing emergency treatment following sah , especially in the case of multiple aneurysms , where it may be difcult to understand which one was responsible for the haemorrhage . 
in lesions undergoing elective treatment , it may instead represent a predictor of the most fragile portion of the sac and / or of the aneurysm most susceptible to rupture [ 16 , 22 , 23 ]  . 
together with the possibility of orientating the 3d model to obtain a virtual view of the surgical eld , the reliability of the technique has a decisive role in mapping the vascular anatomy and relationships between the aneurysm neck and parent vessels when planning surgery . 
in particular , the superiority of 3dra over surgery in differentiating the neck from vascular structures may provide crucial information to reduce the risk of incorrect clipping ; to choose the most appropriate treatment , such as sac coating ; and to provide strategic indications for intraoperative aneurysm handling to reduce the risk of premature rupture , cerebral infarction and neurological sequelae [ 12 , 1517 ]  . 
in fact , the neurosurgeon may nd it difcult to completely visualise the lesion and expose the neck owing to superimposition of cerebral structures or blood clots and necrotic tissue ( in emergency procedures following sah and in 20 cases in our study ) [ 12 , 15 ]  . 
the absence of such information is also associated with a greater use of additional support instrumentation , such as doppler and intraoperative indocyanine green videoangiography [ 24 ] , which are not always appropriate . 
 [ 12 ] have gone as far as proposing the integration of 3dra in surgical navigation systems . adverse outcomes of surgery , in addition to acute complications , include incomplete exclusion of the aneurysm after clipping . 
the incidence of residual aneurysms after minimally invasive surgery is reported to range from 3.8% and 18% , and the risk of bleeding due to residual aneurysm is between 3.5% and 28% in the various series [ 26 , 27 ]  . 
regrowth of a residual aneurysm and recurrence after correct clipping are reported to range from 1.5% to 15% in the different series and are related to dysplasia of the parent vessels [ 27 ]  . 
however , on the basis of our experience and reports in the literature , a small residual aneurysm ( 12 mm ) may be difcult to detect on standard 2d projections owing to superimposition of cerre in anticipo lanatomia vascolare e i rapporti topograci tra colletto aneurismatico e i vasi parenti . 
in particolare , la superiorit della 3dra rispetto alla stessa chirurgia nel dissociare il colletto dalle strutture vasali pu rappresentare un riferimento fondamentale per ridurre il rischio di mal posizionamento della clip metallica , scegliere il miglior tipo di terapia , quale il coating della sacca , e fornire indicazioni strategiche per la manipolazione dellaneurisma durante lintervento , che riducono il rischio di rottura prematura della lesione , di infarto cerebrale e le relative variabili sequele neurologiche [ 12 , 1517 ]  . 
il neurochirurgo infatti pu avere difcolt nella completa visualizzazione della lesione e nellesposizione del colletto a causa della sovrapposizione di strutture cerebrali o coaguli ematici e tessuto necrotico ( in urgenza dopo esa e in 20 casi nel nostro studio ) [ 12 , 15 ]  . 
in mancanza di tali dati oltretutto necessario anche un maggior ricorso a strumentazioni aggiuntive di supporto non sempre adeguate , quali il doppler e la video - angiograa intra - operatoria al verde di indocianina [ 24 ] , per cui alcuni autori , come raabe et al . 
 [ 12 ] , si spingono a proporre lintegrazione della 3dra nei sistemi di navigazione chirurgica . oltre alle complicanze acute , tra gli esiti sfavorevoli della chirurgia inclusa la non completa esclusione dellaneurisma dopo il clipping per varie cause : difcoltosa visualizzazione del colletto o colletto molto ampio , protezione di vasi parenti o perforanti , problemi nel design della clip [ 25 ]  . 
lincidenza di aneurismi residui dopo chirurgia mininvasiva presente nella letteratura con una frequenza tra il 3 , 8% e il 18% ed il rischio di sanguinamento da aneurisma residuo compreso tra il 3 , 5% e il 28% secondo le diverse casistiche [ 26 , 27 ]  . 
la ricrescita di un residuo o lo sviluppo di recidiva dopo il corretto posizionamento delle clip invece stimato in diversi studi tra l1 , 5% e il 15% e legato alla displasia dei vasi parenti [ 27 ]  . 
in base alla nostra esperienza e alla letteratura , tuttavia , un piccolo residuo aneurismatico ( tra 1 e 2 mm ) pu essere di difcile individuazione nelle proiezioni 2d standard a causa della sovrapposizione delle arterie cerebrali o delle stesse clip , specialmente quando multiple . 
nel nostro studio la tecnica 3d ci ha aiutato a comprendere meglio lanatomia vascolare post - operatoria talora complessa , fornendo un imaging multiproiettivo risultato generalmente superiore alle proiezioni 2d convenzionali , con inclinazioni sovrapponibili alla vista del campo operatorio , con la visualizzazione contemporanea delle clip e dei vasi parenti e la possibilit di misurare le reali dimensioni del residuo , un dato 428 radiol med ( 2013 ) 118 : 415430 ebral arteries or the clips themselves , especially when multiple clips are used . 
in our study , the 3d technique helped us better understand the sometimes complex postoperative vascular anatomy by providing multiple - projection images with the same inclination as the surgical eld , simultaneous visualisation of the clips and parent vessels and the possibility of measuring the size of the residual lesion information that cannot be directly obtained from 2d projections . 
our data , in fact , conrmed the usefulness of 3dra in the postoperative follow - up on a large patient population and demonstrated , consistent with other reports , a higher incidence of residual aneurysms ( 19 cases , 17% ) compared with data reported for conventional angiography [ 27 ]  . finally , the advantages of the 3d technique also include shorter examination times and reduced dose of ionising radiation and iodinated contrast material , given that a single injection of 1520 cc of contrast medium provides a 3d multiple projection model , the assessment potential of which would require multiple , repeated , and in any case not always exhaustive conventional angiographic projections conned within the limited excursion of the c - arm [ 1618 , 28 ]  . 
another advantage is less subjectivity and operator dependence required in 3dra , which is a standard procedure compared with 2dra , where the neuroradiologist has to select tube inclinations for different projections according to personal preference and experience . in some of our cases ( 15 / 100 ) , 3d reconstruction produced some transport artefacts , with poor subtraction of skeletal structures or apparent fusion and inability to separate contiguous vessels or the aneurysm sac and parent vessels . 
these artefacts are well known and mainly related to spatial resolution of single angiography devices , to the degree of geometric distortion inherent in the acquisition mode or to the less - than - optimal immobility of patients during the examination [ 16 , 18 ]  . 
in our experience , artefacts were infrequent and not very conspicuous , thanks to at - panel detector technology , and propeller rotation that reduces acquisition time [ 29 ]  . 
also , artefacts never precluded image interpretation or were resolved with no need for further angiographic acquisitions , thanks to a second high - resolution detail reconstruction with the postprocessing software . che non pu essere ottenuto in modo diretto sulle proiezioni 2d . 
i nostri dati infatti confermano lutilit della 3dra nel follow - up postoperatorio su unampia popolazione e hanno dimostrato , in modo similare ad altri report , una percentuale di residui aneurismatici maggiore ( 19 casi , 17% ) rispetto ai dati della letteratura basata sulle valutazioni con angiograa convenzionale [ 27 ]  . i vantaggi della tecnica 3d , inne , risiedono anche nella riduzione dei tempi desame , ma soprattutto nella riduzione della dose di radiazioni ionizzanti e della somministrazione di mezzo di contrasto iodato al paziente in quanto con una sola iniezione di 1520 cc di mdc si ottiene un modello 3d multiproiettivo le cui potenzialit valutative esaminate no a questo punto richiederebbero multiple , ripetute e comunque non sempre esaustive proiezioni angiograche convenzionali , connate nei limiti di escursione del tubo a c [ 1618 , 28 ]  . 
di pari passo va la minor soggettivit e operatore - dipendenza dellesame angiograco con tecnica tridimensionale , che standard , rispetto allesame convenzionale ove il neuroradiologo sceglie in modo individuale e in base alla sua esperienza le diverse inclinazioni del tubo per le diverse proiezioni . in alcuni nostri casi ( 15 / 100 ) la ricostruzione 3d ha prodotto alcuni artefatti di trasporto dellimmagine , con scarsa sottrazione delle strutture scheletriche o apparente fusione e indissociabilit di vasi contigui come tra sacca aneurismatica e vasi parenti . 
tali artefatti sono descritti e legati principalmente alla risoluzione spaziale delle singole apparecchiature , al grado di distorsione geometrica intrinseca alla modalit di acquisizione o alla non perfetta immobilit del paziente nel corso dellesame [ 16 , 18 ]  . 
nella nostra esperienza tuttavia gli artefatti sono risultati poco frequenti e grazie alla tecnologia del detettore at - panel e alla modalit propeller di rotazione del tubo , che riduce il tempo di acquisizione [ 29 ] , sono apparsi poco evidenti , non costituendo mai un reale limite allinterpretazione delle immagini o comunque risolti senza alcun ricorso ad ulteriori acquisizioni angiograche , grazie ad una seconda ricostruzione di dettaglio ad alta risoluzione tramite il software per il post - processing . conclusioni conclusions three - dimensional ra is a reliable method for the overall evaluation of cerebral aneurysms undergoing surgery . 
the technique identies a greater number of aneurysms compared with conventional angiography and allows a virtual la 3dra una metodica afdabile per la valutazione generale degli aneurismi cerebrali sottoposti ad intervento chirurgico . 
la tecnica individua un maggior numero di aneurismi rispetto allangiograa standard e permette la visualizzazione virtuale del campo operatorio e lo studio radiol med ( 2013 ) 118 : 415430 view of the surgical eld and an accurate study of lesion characteristics , thereby helping the surgeon plan treatment in order to improve efcacy and reduce invasiveness . 
ettorre1 1sezione di scienze radiologiche del dipartimento materno infantile e scienze radiologiche , universit degli studi di catania , catania , italy 2dipartimento materno infantile e scienze radiologiche , sezione di ostetricia , universit degli studi di catania , catania , italy 3dipartimento g.f. 
 + 39 - 095 - 3782360 , e - mail : pietrofoti@hotmail.com received : 20 july 2011 / accepted : 30 september 2011 / published online : 9 august 2012 springer - verlag 2012 abstract purpose . 
in assessing myometrial invasion , mr imaging showed 70% accuracy , 80% sensitivity , 40% specicity , 80% positive predictive value ( ppv ) , and 40% negative predictive value ( npv )  . 
nel valutare linvasione del miometrio la rm ha mostrato accuratezza del 70% , sensibilit dell80% , specicit del 40% , valore predittivo positivo ( vpp ) dell80% , valore predittivo negativo ( vpn ) del 40% . 
 nellidenticare linltrazione della cervice la rm ha mostrato accuratezza del 95% , sensibilit del 100% , specicit del 94 , 4% , vpp del 66 , 7% , vpn del 100% . 
la rm una tecnica afdabile nella valutazione preoperatoria del carcinoma dellendometrio ; il suo limite principale rappresentato dalla distinzione fra stadio ia e ib , poco inuente sulla strategia chirurgica . 
 la collaborazione fra clinico e radiologo fondamentale per evitare errori di stadiazione . 488 radiol med ( 2013 ) 118 : 487503 keywords magnetic resonance imaging endometrial cancer staging parole chiave risonanza magnetica carcinoma dellendometrio stadiazione introduction introduzione endometrial carcinoma is the most frequent gynaecological malignancy , with 95% of endometrial cancers being diagnosed in women > 40 years of age [ 1 ]  . 
in particular , invasion of the outer half of the myometrium and tumour grade are associated with an increased risk of metastases to the pelvic and para - aortic lymph nodes [ 1 , 2 ]  . the main symptom of endometrial carcinoma is represented by metrorrhagia . 
disease staging , which is based on the international federation of gynecology and obstetrics ( figo ) classication ( table 1 ) , is essentially surgical , even though accurate preoperative assessment of disease extent with diagnostic imaging may optimise the surgical choice and treatment strategy . 
several imaging techniques have been used for preoperative staging : us , computed tomography ( ct ) and magnetic resonance ( mr ) imaging [ 3 ] ; of these , contrast - enhanced mr imaging proved to be the most effective [ 4 ]  . 
in particular , the main role of mr imaging is to assess the depth of myometrial invasion , cervical invasion and the presence of lymph node metastases . the purpose of our study was to evaluate the role of mr imaging in the staging of endometrial carcinoma . 
to this end , we prospectively determined the diagnostic capabilities of mr imaging in assessing myometrial and cervical invasion , as well as lymph node involvement , by comparing mr with surgical staging and histological ndings ( standard of reference )  . 
we also analysed the main causes of error in mr staging . materials and methods patients this prospective study was approved by the local ethics committee , and each patient provided informed consent . 
in particolare linvasione della met esterna del miometrio ed il grado della neoplasia sono associati ad un incremento del rischio di sviluppare metastasi ai linfonodi pelvici e para - aortici [ 1 , 2 ]  . il sintomo principale delle pazienti con carcinoma dellendometrio rappresentato dalla metrorragia . 
la stadiazione , basata sulla classicazione fdration internationale de gyncologie et dobsttrique ( figo ) ( tabella 1 ) , sostanzialmente chirurgica , tuttavia unaccurata valutazione preoperatoria dellestensione della neoplasia , effettuata con metodiche di imaging , pu consentire di ottimizzare la scelta chirurgica e la strategia terapeutica . 
 nella stadiazione preoperatoria sono state impiegate diverse tecniche : ecograa , tomograa computerizzata ( tc ) e risonanza magnetica ( rm ) [ 3 ] ; fra queste la rm con mezzo di contrasto ha mostrato la maggiore efcacia [ 4 ]  . 
 in particolare il ruolo principale della rm consiste nella valutazione della profondit di invasione del miometrio , dellinvasione della cervice e nella ricerca di eventuali metastasi linfonodali . lo scopo del nostro studio quello di valutare il ruolo della rm nella stadiazione del carcinoma dellendometrio . 
inclusion criteria were : ( 1 ) endometrial carcinoma conrmed histologically after hysteroscopy ; ( 2 ) mr staging carried out at our institute ; ( 3 ) surgery performed at our university hospital . 
three patients were excluded from the study : two on account of the nding of endometrial stromal sarcoma and one with inoperable stage - iva clear - cell carcinoma . the remaining 20 patients ( mean age , 62 years ; age range , 3785 years ) were included in the study . 
surgery , performed in all patients , included type 1 radical ( n = 4 ) , type 2 ( n = 15 ) and type 3 ( n = 1 ) hysterectomy according to pivers classication [ 5 ]  . 
nel periodo compreso fra settembre 2008 e marzo 2010 , 23 pazienti consecutive con neoplasia maligna dellendometrio , provenienti dal reparto di ostetricia e ginecologia del nostro nosocomio , sono state prese in esame per essere arruolate nello studio . 
i criteri di inclusione nello studio sono stati i seguenti : ( 1 ) carcinoma dellendometrio accertato istologicamente dopo esame isteroscopio ; ( 2 ) esame rm eseguito presso il nostro istituto per stadiazione della neoplasia ; ( 3 ) intervento chirurgico eseguito presso la nostra azienda ospedaliero - universitaria . 
tre pazienti sono state escluse dallo studio : due per il riscontro di sarcoma 490 radiol med ( 2013 ) 118 : 487503 patients underwent lymphadenectomy : pelvic lymph node sampling ( n = 3 ) , pelvic lymphadenectomy ( n = 8 ) , pelvic and lumboaortic lymphadenectomy ( n = 4 )  . 
tutte le pazienti sono state sottoposte ad intervento chirurgico : in 4 pazienti stata eseguita unisterectomia radicale tipo 1 , in 15 pazienti unisterectomia tipo 2 ed in 1 paziente unisterectomia tipo 3 secondo la classicazione di piver et al . 
quindici / 20 pazienti ( 75% ) sono state sottoposte a linfoadenectomia : in 3 casi stato eseguito un sampling dei linfonodi pelvici , in 8 casi stata eseguita una linfoadenectomia pelvica , in 4 casi una linfoadenectomia pelvica e lombo - aortica . 
in all patients , staging was completed by a ct scan of the chest , abdomen and pelvis , performed before surgery . image analysis mr examination was performed by a radiologist with 6 years experience in gynaecological imaging . 
mr images were visualised on a picture archiving and communication system ( pacs ) workstation , and the radiologist was aware of the ndings of the gynaecological and hysteroscopic examinations . 
preoperative mr staging was based on the figo classication ( table 1 ) and took into consideration the following parameters : myometrial invasion ; cervical invasion ; pelvic and lumboaortic lymph node involvement . figo classication in force at the time of designing this prospective study ( 2008 ) was used , which allowed comparison with the results published in the literature . 
in tutte le pazienti la stadiazione stata completata con un esame tc condotto a livello del torace , delladdome e della pelvi , eseguito prima dellintervento chirurgico . analisi delle immagini lesame rm stato eseguito da un radiologo con 6 anni di esperienza nel settore oggetto dello studio . 
il radiologo disponeva delle informazioni relati492 radiol med ( 2013 ) 118 : 487503 myometrial invasion was identied by the loss of physiological signal hypointensity of the junctional zone on t2 - weighted images ; depth of myometrial invasion was determined on the basis of measurements of the remaining healthy myometrium , and if the residual healthy myometrium was thick ( > 50% of overall myometrial thickness ) , the tumour was classied as stage ib ; if the residual healthy myometrium was thin ( < 50% of overall myometrial thickness ) , the lesion was classied as stage ic . cervical invasion was classied as positive or negative and was identied as cervical dilatation produced by tissue having the same signal intensity as the endometrial lesion and / or as destruction of cervical stroma , which is physiologically hypointense on t2 - weighted images . lymph node assessment was based on size , with any lymph nodes with a short axis longer than 1 cm being considered pathological . statistical analysis diagnostic capabilities of mr compared with the reference standard were evaluated with standard statistical analyses . 
 in the assessment of myometrial invasion , cervical invasion and presence of lymph node metastases , we calculated accuracy , sensitivity , specicity , positive predictive value ( ppv ) and negative predictive value ( npv )  . 
in the assessment of myometrial invasion ( classied as absent , < 50% or > 50% ) , all cases in which mr understaged the disease were considered false negative results , whereas all cases in which mr overstaged the disease were considered false positives . 
la stadiazione preoperatoria effettuata con la rm , basata sulla classicazione figo ( tabella 1 ) , ha valutato i seguenti parametri : invasione del miometrio ; invasione della cervice ; interessamento dei linfonodi pelvici e lombo - aortici . stata utilizzata la classicazione figo in vigore al momento della progettazione dello studio prospettico ( 2008 ) ; questo ci ha permesso di effettuare un confronto con i risultati dei reports presenti in letteratura . 
linvasione del miometrio stata classicata come : assente , < 50% o > 50% ( stadio ia , ib e ic rispettivamente ) ed stata valutata nel seguente modo : ispessimento / eterogeneit di segnale dellendometrio e della cavit endometriale con conservazione della zona giunzionale che appare siologicamente ipointensa nelle immagini t2 - ponderate e mostra impregnazione precoce nelle immagini t1 - ponderate acquisite dopo somministrazione ev di mdc : stadio ia ; linvasione del miometrio stata identicata con la perdita della siologica ipointensit di segnale della zona giunzionale nelle immagini t2 ponderate . 
se il miometrio sano residuo spesso ( oltre il 50% dello spessore complessivo del miometrio ) il tumore assegnato allo stadio ib ; se il miometrio sano residuo sottile ( meno del 50% dello spessore complessivo del miometrio ) la lesione assegnata allo stadio ic . linvasione della cervice stata valutata come positiva o negativa ed stata identicata come dilatazione del canale cervicale da parte di tessuto con la stessa intensit di segnale della lesione endometriale e / o come distruzione dello stroma cervicale siologicamente ipointenso nelle immagini t2 - ponderate . nella valutazione dei linfonodi si tenuto un criterio dimensionale , considerando patologici i linfonodi con asse corto superiore ad 1 cm . analisi statistica le capacit diagnostiche della rm nei confronti dello standard di riferimento sono state valutate utilizzando calcoli statistici standard . 
per la valutazione dellinltrazione del miometrio , dellinvasione della cervice e della presenza di metastasi linfonodali sono stati calcolati : accuratezza , sensibilit , specicit , valore predittivo positivo e negativo . 
nella valutazione dellinvasione del miometrio ( distinta secondo tre classi : assente , < 50% , > 50% ) i casi dove la rm ha sottostadiato la patologia sono stati considerati radiol med ( 2013 ) 118 : 487503 table 2 surgical staging . 
le immagini sagittale ( a ) e coronale obliqua ( b ) fse t2 - ponderate mostrano il carcinoma endometriale come massa ipointensa sul lato sinistro della cavit endometriale ( freccia ) con integrit della zona giunzionale ; questultima presenta bassa intensit di segnale ( testa di freccia )  . 
 caratterizzato da ghiandole ben riconoscibili rivestite da cellule epiteliali colonnari straticate citologicamente maligne ( colorazione con ematossilina e eosina , ingrandimento 200 )  . 494 radiol med ( 2013 ) 118 : 487503 fig . 
sagittal t2 - weighted fse ( a ) and coronal oblique t2 - weighted fse ( b ) images depict endometrial cancer inltrating the junctional zone ( arrow ) , indicating myometrial invasion < 50% of its thickness . 
le immagini sagittale fse t2 - ponderata ( a ) e coronale obliqua fse t2 - ponderata ( b ) mostrano il carcinoma dellendometrio che inltra la zona giunzionale ( freccia ) , espressione di invasione del miometrio inferiore al 50% del suo spessore . 
caratterizzato da ghiandole ben riconoscibili frammiste a foglietti solidi di cellule maligne ( colorazione con ematossilina e eosina , ingrandimento 200 )  . results of mr staging were as follows ( table 3 ) : stage ia , four cases ; stage ib , seven cases ; stage ic , four cases ; stage ic ( n1 ) , one case ; stage iia , one case ; stage iib two cases ; stage iiia ( n1 ) , one case . compared with surgical staging , mr correctly staged 13 / 20 ( 65% ) , understaged 3 / 20 ( 15% ) , and overstaged 4 / 20 come falsi negativi mentre i casi in cui la rm ha sovrastadiato la patologia sono stati considerati come falsi positivi . 
tale valutazione ha riguardato linvasione del miometrio ( distinta secondo tre classi : assente , < 50% , > 50% ) , linvasione della cervice e la presenza di metastasi linfonodali . 
nei casi in cui si riscontrata una discrepanza fra la stadiazione rm e quella chirurgica sono state ricercate ed elencate le possibili cause di errore . radiol med ( 2013 ) 118 : 487503 fig . 
sagittal ( a ) and axial oblique ( b ) t2 - weighted fse images depict endometrial cancer inltrating the myometrium by > 50% of its thickness ( arrow ) ; the junctional zone of low signal intensity is entirely inltrated . 
le immagini sagittale ( a ) e assiale obliqua ( b ) fse t2 - ponderate mostrano un carcinoma dellendometrio che inltra il miometrio per pi della met del suo spessore ( freccia ) ; la zona giunzionale ipointensa completamente inltrata . 
 caratterizzato da foglietti solidi di cellule con ghiandole appena riconoscibili ( colorazione con ematossilina e eosina , ingrandimento 200 )  . ( 20% ) cases ( table 4 )  . 
sagittal t2 - weighted fse images ( a , b ) , axial oblique t2 - weighted fse image ( c ) , axial oblique gadolinium - enhanced t1 - weighted lava image ( d )  . 
a , b immagini sagittali fse t2 - ponderate , c immagine assiale obliqua fse t2 - ponderata , d immagine assiale obliqua t1 - ponderata lava dopo somministrazione ev di gadolinio . 
nella valutazione dellinltrazione del miometrio la rm ha mostrato i seguenti risultati ( tabella 5 ) : accuratezza 70% ; sensibilit 80% [ 95% intervallo di condenza ( ci ) limit 59 , 8%100 , 2% ] ; specicit 40% ( 95% ci limit 2 , 9%82 , 9% ) ; valore predittivo positivo 80% ; valore predittivo negativo 40% . nellidenticazione della mancanza di inltrazione dellendometrio ( stadio ia ) emersa una scarsa correlazione fra la stadiazione rm e quella chirurgica ( r di pearson = 0 , 37 )  . 
nellidenticazione dellinvasione del miometrio < 50% ( stadio ib ) e dellinvasione del miometrio > 50% ( stadio ic ) emersa unelevata correlazione fra la stadiazione rm e quella chirurgica ( r di pearson = 0 , 49 e 0 , 68 rispettivamente )  . in 2 / 20 casi ( 10% ) la stadiazione chirurgica ha evidenziato invasione della cervice , reperto valutato correttamente dallesame rm . 
nella valutazione dellinvasione della cervice la rm ha mostrato i seguenti risultati ( tabella 5 ) : accuratezza 95% ; sensibilit 100% ( 95% ci limit 100%100% ) ; specicit 94 , 4% ( 95% ci limit 83 , 9%105% ) ; table 4 comparison between magnetic resonance ( mr ) imaging and surgical staging tabella 4 confronto tra stadiazione in risonanza magnetica ( rm ) e stadiazione chirurgica case n . 
sagittal ( a ) , coronal oblique ( b ) and axial oblique ( c ) t2 - weighted fse images show endometrial cancer ( arrow ) that seems to inltrate the junctional zone , indicating myometrial invasion < 50 % of its thickness ( stage ib )  . 
le immagini sagittale ( a ) , coronale obliqua ( b ) e assiale obliqua ( c ) fse t2 - ponderate mostrano il carcinoma dellendometrio ( freccia ) che sembra inltrare la zona giunzionale , espressione di invasione del miometrio inferiore al 50% del suo spessore ( stadio ib )  . 
e si osserva un focolaio di adenomiosi ( testa di freccia ) , causa di errore ( colorazione con ematossilina e eosina , ingrandimento 200 )  . mr ( true positives ) , which also correctly staged the remaining 13 cases ( true negatives )  . 
in the assessment of lymph node metastases , a high correlation was found between mr and surgical staging ( pearson r = 1 )  . table 6 shows the factors associated with the presence of false negative and false positive results in the assessment of myometrial invasion and the factors associated with the presence of false positive results in the assessment of cervical invasion . 
the possivalore predittivo positivo 66 , 7% ; valore predittivo negativo 100% . nella valutazione dellinvasione della cervice emersa una marcata correlazione fra la stadiazione rm e quella chirurgica ( r di pearson = 0 , 79 )  . 
valutazione con rm dellinltrazione del miometrio , dellinvasione della cervice e delle metastasi linfonodali inltrazione miometrio invasione cervice metastasi linfonodali vpp , valore predittivo positivo ; vpn , valore predittivo negativo ble cause of error in the assessment of cervical invasion was dilatation and curettage performed during hysteroscopy . 
ct examination performed on all patients before surgery did not change the results of mr staging . discussion the main role of mr in staging of endometrial carcinoma consists in depicting the depth of myometrial invasion , cervical invasion and lymph node metastases . 
this could be explained by the fact that we assessed stages ia , ib and ic separately , whereas other authors [ 6 ] assessed myometrial invasion as > 50% or < 50% ( stages ib and ic )  . 
in order to avoid lymphadenectomy and its related morbidity in patients with a reduced likelihood of lymph node metastases , the procedure should be performed when myometrial correlazione fra la stadiazione rm e quella chirurgica ( r di pearson = 1 )  . la tabella 6 mostra i fattori legati alla presenza di falsi negativi e falsi positivi nella valutazione dellinltrazione del miometrio e i fattori associati alla presenza di falsi positivi nella valutazione dellinvasione della cervice . 
lesame tc eseguito in tutte le pazienti prima dellintervento chirurgico non ha modicato la stadiazione effettuata con rm . discussione il ruolo principale della rm nella stadiazione del carcinoma dellendometrio consiste nella valutazione della profondit di invasione del miometrio , dellinltrazione della cervice e nella ricerca di eventuali metastasi linfonodali . 
 laccuratezza complessiva della rm nella valutazione di tali parametri compresa fra il 71% ed il 97% nelle varie casistiche presenti in letteratura [ 1 , 2 , 6 , 7 ]  . 
nel nostro studio , nella valutazione dellinltrazione del miometrio , la rm ha mostrato accuratezza del 70% , sensibilit dell80% , specicit del 40% , valore predittivo positivo del 75% e valore predittivo negativo del 40% . 
ci potrebbe essere dovuto 500 radiol med ( 2013 ) 118 : 487503 table 6 causes of error in evaluating myometrial and cervical invasion cause of error myometrial invasion false negative case 8 case 13 case 19 false positive case 2 case 10 case 11 cervical invasion false positive case 18 polypoid tumour , leiomyomas polypoid tumour , adenomyosis , leiomyomas leiomyomas polypoid tumour , adenomyosis , leiomyomas polypoid tumour , leiomyomas polypoid tumour , adenomyosis tabella 6 cause di errore nella valutazione dellinltrazione del miometrio e della cervice curettage cause di errore invasione del miometrio falsi negativi caso 8 caso 13 caso 19 falsi positivi caso 2 caso 10 caso 11 invasione della cervice falsi positivi caso 18 tumore polipoide , leiomiomi tumore polipoide , adenomiosi , leiomiomi leiomiomi tumore polipoide , adenomiosi , leiomiomi tumore polipoide , leiomiomi tumore polipoide , adenomiosi raschiamento invasion is deeper than 50% or at advanced stages of the disease [ 6 ]  . 
therefore , from this point of view , the most important aspect in preoperative mr assessment is the distinction between stages ib and ic ( myometrial invasion > 50% or < 50% , respectively )  . 
this is probably the reason the new figo staging system includes stages ia and ib into a single new stage ia [ 8 ]  . a new perspective in assessing myometrial invasion is represented by the use of mr diffusion - weighted imaging ( dwi )  . 
recently applied to abdominal imaging , this method is based on the diffusion of water molecules , which provides information on the extracellular compartment , tissue cellularity and integrity of cell membranes . 
dwi , with its high - contrast resolution , is a complement to conventional morphological mr imaging : endometrial carcinoma appears markedly hyperintense and the normal myometrium hypointense , which facilitates identication of the margin al fatto che nella nostra casistica abbiamo valutato separatamente gli stadi ia , ib e ic . 
al ne di evitare la linfoadenectomia e la sua morbidit nei pazienti con ridotta probabilit di sviluppare metastasi linfonodali , la linfoadenectomia andrebbe eseguita quando linvasione miometriale superiore al 50% o nei casi avanzati [ 6 ]  . 
da questo punto di vista laspetto pi importante nella valutazione preoperatoria con esame rm riguarda pertanto la distinzione fra stadio ib e ic ( invasione miometriale rispettivamente minore o maggiore del 50% )  . 
probabilmente per questo motivo che nella nuova stadiazione figo gli stadi ia ed ib sono stati inglobati in un unico nuovo stadio ia [ 8 ]  . una nuova prospettiva nella valutazione dellinltrazione del miometrio rappresentata dallutilizzo delle sequenze rm pesate in diffusione ( dwi )  . 
si tratta di una tecnica di recente applicazione in ambito addominale , basata sui moti di diffusione delle molecole dacqua , che fornisce informazioni sul compartimento extracellulare , sulla cellularit tissutale e sullintegrit delle membrane cellulari . 
le immagini pesate in diffusione , per la loro elevata risoluzione di contrasto , rappresentano unintegrazione dellimaging morfologico convenzionale con rm : il carcinoma dellendometrio appare fortemente iperintenso , mentre il miometrio normale presenta bassa intensit di segnale , cosicch risulta particolarmente facile identicare il conne fra il tessuto neoplastico e quello sano . 
secondo alcuni autori [ 911 ] le sequenze dwi possono fornire informazioni utili nella valutazione preoperatoria dellinvasione miometriale e possono rappresentare una valida alternativa alle sequenze t1 dinamiche , nei pazienti che presentano controindicazioni al mezzo di contrasto paramagnetico a causa di allergia al gadolinio oppure a causa di una condizione di insufcienza renale con rischio di sviluppare una brosi nefrogenica sistemica . nei casi in cui la stadiazione rm non coincideva con quella chirurgica abbiamo analizzato le possibili cause di errore nella valutazione dellinvasione miometriale associate alla presenza di falsi positivi e falsi negativi . 
le principali cause di pitfalls da noi riscontrate sono state : tumore polipoide ( 5 / 6 casi ) , adenomiosi diffusa ( 3 / 6 casi ) , leiomiomi intramurali ( 5 / 6 casi )  . 
according to some authors [ 911 ] , dwi sequences can provide useful information in preoperative assessment of myometrial invasion and may represent a valuable alternative to t1 dynamic sequences in patients with contraindications to the use of paramagnetic contrast agents due to allergy or renal failure , with an increased risk of nephrogenic systemic brosis . when mr staging did not coincide with surgical staging , we analysed the possible causes of error in assessing myometrial invasion associated with the presence of false positive and false negative results . 
the main causes of error were polypoid tumour ( 5 / 6 cases ) , diffuse adenomyosis ( 3 / 6 cases ) and intramural leiomyomas ( 5 / 6 cases )  . 
in this case , at nal examination of the surgical specimen , the cervix appeared dilated , with an irregular surface ; at histological examination , the endocervical epithelium was no longer recognisable , having been replaced by abundant granulation tissue . 
this emphasises the need for close cooperation between gynaecologists and radiologists and , in particular , for the latter to be aware of any extraradiological diagnostic procedures performed so as to avoid errors in imaging ndings interpretation . 
in the literature , one of the main limitations of mr imaging is the presence of tumours with supercial involvement of the endocervix , which is often not identiable on mr imaging . in 6 / 20 cases ( 30% ) , there was high - grade disease ( g3 ) ; these cases were associated with the most advanced stages in our series : ic ( n = 3 ) , ic n1 ( n = 1 ) , iia ( n = 1 ) and iiia n1 ( n = 1 )  . 
this nding is consistent with the literature , where invasion of the outer half of the myometrium and tumour grade are associated with a higher risk of lymph node metastases . 
these high values portati da altri autori [ 1 , 2 , 6 ] in studi precedenti . nel nostro studio , nella valutazione dellinvasione della cervice la rm ha mostrato accuratezza del 95% , sensibilit del 100% , specicit del 94 , 4% , valore predittivo positivo del 66 , 7% e valore predittivo negativo del 100% . 
in questo caso allesame nale sul pezzo operatorio la cervice appariva dilatata con supercie irregolare e allesame istologico lepitelio dellendocervice non era pi riconoscibile ed al suo posto era apprezzabile abbondante tessuto di granulazione . 
ci pone laccento sulla necessit di una stretta collaborazione fra clinico e radiologo ed in particolare sulla necessit da parte di questultimo di conoscere la modalit di esecuzione delle procedure diagnostiche extraradiologiche al ne di evitare errori nellinterpretazione dei reperti di imaging . 
in letteratura uno dei limiti della metodica rappresentato dalla presenza di tumori con coinvolgimento superciale dellendocervice , spesso non identicabile allesame rm . in 6 / 20 casi ( 30% ) la neoplasia presentava grado elevato ( g3 ) ; questi casi sono associati agli stadi pi avanzati della nostra casistica : stadio ic ( 3 casi ) , stadio ic n1 ( 1 caso ) , stadio iia ( 1 caso ) e stadio iiia n1 ( 1 caso )  . 
questo dato correla con quelli esistenti in letteratura secondo cui linvasione della met esterna del miometrio ed il grado della neoplasia sono associati ad un aumentato rischio di sviluppare metastasi linfonodali . 
la nostra valutazione dei linfonodi con risonanza magnetica , basata su un criterio dimensionale , ha mostrato valori di accuratezza , sensibilit , specicit , valore predittivo positivo e negativo del 100% . 
valori cos elevati sono dovuti alle dimensioni dei linfonodi metastatici che , nella nostra casistica , erano comprese tra 2 e 5 c sappiamo per che anche linfonodi con asse corto inferiore al centimetro possono essere sede di micro metastasi , cos come linfonodi con asse corto superiore al centimetro possono essere reattivi . 
questo il limite principale della rm 502 radiol med ( 2013 ) 118 : 487503 are related to the size of the metastatic lymph nodes , which ranged from 2 to 5 chowever , we know that lymph nodes with short axis < 1 cm may also be the site of micrometastases , just like lymph nodes with short axis > 1 cm may be reactive . 
a new perspective in this eld is represented by the use of new negative superparamagnetic contrast agents , the so - called ultrasmall superparamagnetic particulate iron oxide ( uspio ) agents , which is specic for reticuloendothelial cells and which are currently at an advanced stage of experimentation [ 1214 ]  . 
 however , even without the use of specic contrast agents , mr imaging still has a slight advantage over other methods ( ct ) in the study of lymph nodes . 
in fact , accurate assessment of the t parameter ( myometrial invasion ) , which is made possible by the excellent contrast resolution of mr imaging , provides indirect information on the likelihood of lymph node metastases , which is greater when myometrial invasion exceeds 50% [ 15 ]  . in assessing lymph node involvement , the entire abdomen must be carefully studied in that endometrial carcinoma may produce paraaortic lymph node metastases , even in the absence of pelvic lymph node metastases . 
in our study , staging was completed by a ct scan which , performed in all patients before surgery , did not modify the results of mr staging . our study suffers several limitations . 
a second is that only 15 ( 75% ) of the 20 patients underwent lymphadenectomy with histological examination ; in the remaining ve , lymph node assessment was done by surgical inspection and palpation , which are less reliable than histology [ 7 ]  . 
una nuova prospettiva in questo campo rappresentata dallutilizzo di nuovi mezzi di contrasto superparamagnetici negativi ( ultrasmall superparamagnetic particulate iron oxide , uspio ) specici per le cellule reticolo - endoteliali , attualmente in avanzata fase di sperimentazione [ 1214 ]  . 
laccurata valutazione del parametro t ( inltrazione del miometrio ) , possibile con rm grazie alla sua eccellente risoluzione di contrasto , consente infatti di trarre indirettamente delle conclusioni sulla probabilit della presenza di metastasi linfonodali , che risulta pi elevata quando linvasione miometriale supera il 50% [ 15 ]  . nella valutazione del coinvolgimento linfonodale deve essere attentamente studiato lintero addome in quanto il carcinoma dellendometrio pu metastatizzare direttamente ai linfonodi para aortici anche in assenza di metastasi ai linfonodi pelvici . 
nel nostro studio la stadiazione stata completata con un esame tc che , eseguito in tutte le pazienti prima dellintervento chirurgico , non ha tuttavia modicato la stadiazione rm . il nostro studio presenta alcuni limiti . 
un limite legato al fatto che solo 15 ( 75% ) delle 20 pazienti sono state sottoposte a linfoadenectomia con successivo esame istologico dei linfonodi ; nelle restanti 5 pazienti la valutazione dei linfonodi avvenuta attraverso osservazione chirurgica e palpazione che presentano attendibilit inferiore rispetto allesame istologico [ 7 ]  . 
altri limiti sono legati alla presenza di un solo osservatore nellanalisi delle immagini rm , che non ha permesso di valutare la variabilit interosservatore , e alla mancata valutazione dellinuenza della stadiazione rm sulla strategia terapeutica . 
despite the above limitations , the results of our study are consistent with those reported in the literature and conrm the importance of preoperative mr imaging for studying endometrial cancer . 
in fact , although multiplanar capabilities and excellent contrast resolution make mr the most accurate imaging technique in this eld , it is still far from being the ideal method for staging endometrial carcinoma . 
al di l dei limiti sopraelencati , i risultati del nostro studio appaiono in linea con quelli esistenti in letteratura e confermano limportanza della rm preoperatoria nello studio delle neoplasie dellendometrio . 
la rm , infatti , grazie alle sue caratteristiche multiplanari e ad uneccellente risoluzione di contrasto , attualmente considerata la tecnica di imaging pi accurata in questo campo ; tuttavia ancora lontana dal rappresentare la metodica ideale nella stadiazione del carcinoma dellendometrio . 
the most important causes of error in mr staging are tumour with polypoid macroscopic structure , the presence of diffuse adenomyosis and intramural leiomyomas , and invasive diagnostic procedures ( curettage ) performed before mr examination . 
therefore , cooperation between gynaecologists and radiologists is essential to enable correct interpretation of imaging ndings and avoid staging errors . principale della metodica nella valutazione dellinltrazione del miometrio rappresentato dalla distinzione fra stadio ia e ib che appare comunque poco inuente sulla strategia chirurgica . 
le principali cause di errore nella stadiazione rm sono rappresentate dalla struttura macroscopica polipoide della neoplasia , dalla presenza di adenomiosi diffusa e di leiomiomi intramurali e dallesecuzione di procedure diagnostiche invasive ( raschiamento ) prima dellesame rm . 
knauth springer - verlag berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 540 - 85087 - 8 e - isbn : 978 - 3 - 540 - 85 - 090 - 8 published online : 22 october 2012 springer - verlag 2012 ultra high eld mri ( uhf - mr ) is a very fast growing and developing mri technology . 
this is evolving so rapidly that the editors in their preface , write that trying to catch the essence of ongoing research in all relevant aspects technologies , methods , research and applications seemed like trying to nail a pudding to a wall . on the contrary , when one gets to the end of the book , he / she realizes that the pudding has been successfully nailed . 
it must be stated that due to the novelty and to problems related to the topic that the unaware reader will sometime get lost in the physics and technical explanations and discussions needed to properly present and clarify the topic . once the technologies and methods and contrasts chapters are digested , a thorough presentation and discussion about the safety ( a very important issue in uhf - mr ) is submitted before full immersion in the practical applications chapters . 
in this fascinating section of the book beautiful high resolution images of the brain are presented , demonstrating incredibly subtle microstructural changes which might be found in some neurological disorders , discussed in the neuroscientic applications and clinical neuro chapters . 
 the use of uhf - mr in oncology as well as in musculoskeletal disorders is presented ( emphasis is put on the very early , preclinical detection of cartilage changes , so important in degenerative diseases )  . 
the last two chapters are devoted to high - eld spectroscopy and to molecular and translational research , both fascinating and important research elds with future applications in the clinical setting . 
 if a criticism can be raised about the gures it is the fact la risonanza magnetica a campo elevato ( uhf - mr ) una tecnologia rm in assai rapida crescita e sviluppo , unevoluzione tale che i curatori del volume , nella loro prefazione , scrivono che tentare di afferrare lessenza della ricerca corrente in tutti i suoi aspetti pi rilevanti tecnologie , metodi , ricerca ed applicazioni sembrava quasi di voler intraprendere unimpresa disperata . 
 invece , quando il lettore arriva alla ne del volume si rende conto che limpresa disperata stata portata a termine con successo . il testo diviso in quattro parti ( tecnologie ; sicurezza ; metodi e mezzi di contrasto ; applicazioni ) che fanno seguito ad una stringata introduzione . 
occorre considerare che , a causa della novit e dei problemi inerenti alla materia , lignaro lettore si trover talvolta sperso nelle spiegazioni e discussioni siche e tecniche necessarie per presentarla e chiarirla in modo adeguato . 
dopo avere digerito i capitoli dedicati alle tecnologie , ai metodi ed ai mezzi di contrasto , viene presentata una discussione accurata e precisa circa la sicurezza ( un argomento molto importante nella uhf - mr ) , prima dellimmersione completa nei capitoli sulle applicazioni pratiche . 
in questa affascinante sezione del volume sono presentate magniche immagini ad alta risoluzione del cervello , che dimostrano alterazioni incredibilmente ni , di possibile riscontro in alcune malattie neurologiche , discusse poi nelle applicazioni neuroscientiche e nei capitoli dedicati alla neurologia clinica . 
viene presentato anche limpiego della uhf - mr in oncologia e nelle malattie muscolo - scheletriche ( con unenfasi particolare sulle alterazioni molto precoci , precliniche della cartilagine , cos importanti nelle malattie degenerative )  . 
gli ultimi due capitoli sono dedicati alla spettroscopia ad alto campo ed alla ricerca molecolare e translazionale , entrambi campi di ricerca affascinante ed importante per le future applicazioni in campo clinico . 
 se una critica pu essere avanzata riguardo alle immagini consiste nel fatto che talvolta ne vengono presentate radiol med ( 2013 ) 118 : 518519 that sometimes every possible study image is presented , so they are sometimes smaller than a stamp , making impossible ( or at least for me ) to properly appreciate what they want to document . 
acronyms , as usual are a problem ( apart from the musculoskeletal chapter where they are listed at its beginning in order of citation ) , even if they are not used at large . 
each chapter is enriched by an ample updated reference list . molteplici riferite ad una stessa indagine , cos che risultano spesso pi piccole di un francobollo , rendendo impossibile ( almeno per me ) ladeguato apprezzamento di ci che vogliono documentare . 
 gli acronimi , anche se non usati in gran quantit , rappresentano al solito un problema ( ad esclusione del capitolo dedicato allapparato musculoscheletrico , dove sono elencati , in ordine di citazione , allinizio dello stesso )  . 
su un sistema ad 1 , 5 t , due radiologi hanno retrospettivamente caratterizzato come benigne o maligne 50 lfe solide : ( a ) attraverso la av dellintensit di segnale nelle immagini dwi acquisite a b = 800 s / mm2 e nella mappa adc ; ( b ) quanticando ladc delle lesioni . 
complessivamente , laccuratezza di entrambi i metodi risultata limitata a causa della sovrapposizione 344 radiol med ( 2013 ) 118 : 343355 delle caratteristiche di segnale e di adc fra lesioni solide benigne e maligne . 
 parole chiave imaging pesato in diffusione analisi visiva coefciente di diffusione apparente lesioni focali epatiche accuratezza introduction introduzione diffusion - weighted imaging ( dwi ) provides functional information about brownian motion of water molecules within tissues , expressed as the apparent diffusion coefcient ( adc ) [ 1 ]  . 
based on microstructural tissue changes , malignant focal livers lesions ( flls ) are supposed to have restricted water diffusion , whereas benign ones are not [ 2 ]  . 
 however , quantication of adc in flls has some limits : rst , there is a large overlap between adcs of solid benign flls [ such as focal nodular hyperplasia ( fnh ) or hepatocellular adenoma ( ha ) ] and malignant lesions [ such as hepatocellular carcinoma ( hcc ) and metastases ] [ 6 ] ; second , adc values are largely dependent on dwi sequence parameters , such as the set of b values , or the use of the parallel imaging technique [ 7 ]  . 
however , only a few studies have investigated the role of visual analysis ( va ) of dwi images and adc maps for characterising flls [ 12 , 13 ]  . 
we hypothesise that va has the potential to complement or replace adc - q in this setting , as it allows an easier approach for radiologists to estimate the diffusion pattern of flls . 
adc - q in discriminating between malignant and solid benign flls . materials and methods institutional review board approval was obtained for this retrospective study . patient population limaging pesato in diffusione ( dwi ) fornisce informazioni funzionali sul moto browniano delle molecole dacqua nel contesto dei tessuti , esprimendole come coefciente di diffusione apparente ( adc ) [ 1 ]  . 
si suppone che , a causa di modicazioni tissutali microstrutturali , le lesioni focali epatiche ( lfe ) maligne presentino una restrizione della diffusione molecolare dellacqua , al contrario di quanto avviene per le lesioni benigne [ 2 ]  . 
questo assunto stato oggetto di diversi studi , i quali hanno dimostrato che la quanticazione delladc ( q - adc ) ha le potenzialit per differenziare le lfe benigne da quelle maligne [ 35 ]  . 
 la q - adc nelle lfe , tuttavia , affetta da alcuni limiti : primo , vi una ampia sovrapposizione fra gli adc delle lfe solide benigne [ ad esempio liperplasia nodulare focale ( inf ) o ladenoma epatocellulare ( ae ) ] e maligne [ ad esempio lepatocarcinoma ( hcc ) e le metastasi ] [ 6 ] ; in secondo luogo , i valori di adc variano signicativamente a seconda dei parametri di acquisizione delle sequenze di dwi , quali il set di b - values impiegato o luso delle tecniche di parallel imaging [ 7 ]  . 
solo un numero ridotto di studi , tuttavia , ha investigato il ruolo dellanalisi visiva ( av ) delle immagini dwi e della mappe adc ai ni della caratterizzazione delle lfe [ 12 , 13 ]  . 
 abbiamo ipotizzato che , in questo scenario , la av abbia un ruolo potenzialmente complementare o sostitutivo della q - adc , poich essa consente un approccio pi semplice allinterpretazione dei pattern di diffusione delle lfe . 
 we performed a computerised search for all patients who underwent liver magnetic resonance ( mr ) imaging at our institution for rst assessment of sonographically detected flls between february 2009 and may 2010 . 
our standmateriali e metodi questo studio retrospettivo ha ottenuto lapprovazione istituzionale per il suo svolgimento . radiol med ( 2013 ) 118 : 343355 table 1 characteristics of focal liver lesions in the study . 
la diagnosi in consensus stata formulata da due radiologi esperti che hanno revisionato i dati clinici dei pazienti ed esami di imaging di follow - up nellarco di 1 anno ( vedi testo ) lesioni ( n ) diametro medio / diametro massimo ( cm ) standard di riferimento istologia diagnosi in consensus hcc , epatocarcinoma ; inf , iperplasia nodulare focale ; ae , adenoma epatocellulare ard mr imaging protocol for this indication includes dwi ; 130 patients were identied . 
we excluded : ( a ) patients with flls showing typical mr appearance of cysts and / or haemangiomas [ 14 ] ( n = 65 ) ; ( b ) patients with poor dwi image quality due to distortion or ghosting artefacts ( n = 3 ) ; ( c ) lack of standard of reference for lesion conrmation ( n = 30 )  . 
 thirty - two patients were enrolled ( 13 men , 19 women ; age range , 2179 years ; mean age , 57.0 years ) , 14 with a cirrhotic liver and 18 with a noncirrhotic liver . 
 for 38 lesions , the standard of reference was represented by a consensus panel diagnosis provided by two readers with > 10 years of experience in abdominal radiology ( cz , mb )  . 
 they reviewed : ( a ) the patients history before and after baseline mr imaging ; ( b ) baseline computed tomography ( ct ) ( when available ) and mr examinations ; ( c ) ct or mr images performed during a follow - up period of at least 1 popolazione di studio stata effettuata una ricerca computerizzata per identicare tutti i pazienti che fossero stati sottoposti nel nostro istituto , tra febbraio 2009 e maggio 2010 , ad una risonanza magnetica ( rm ) di caratterizzazione di lfe identicate in un precedente esame ecograco . 
nel complesso , quindi , sono stati arruolati 32 soggetti ( 13 maschi , 19 femmine ; range di et 2179 anni , et media 57 , 0 anni ) , nei quali le lfe erano su fegato cirrotico in 14 casi e su fegato non cirrotico in 18 casi . 
di queste , sono state incluse nellanalisi quelle con diametro massimo 1 , 0 cm , per un totale di 50 lesioni , allo scopo di assicurare una cospicuit visiva adeguata durante la av delle mappe adc . 
 346 radiol med ( 2013 ) 118 : 343355 year ( mean of 2.8 examinations per patient ) , including ct examinations obtained after transarterial chemoembolisation ( tace ) in nine lesions assessed as hcc ( see below )  . 
 lesions that remained stable in number and dimensions despite the absence of therapy were assumed to be benign ( n = 11 ) , including three lesions in cirrhotic livers nally assessed as dysplastic nodules . 
lesions were assumed to be malignant when presenting : ( a ) suspicious appearance at baseline mr imaging , followed by increase in number and dimensions and / or response to medical therapy or interventional procedures ( n = 8 ) ; ( b ) typical pattern for hcc according to the recently validated criteria of the american association for the study of liver diseases [ 15 ] ( n = 19 )  . 
regardless of specic appearance , fnhs and has were included in one single group of benign solid flls due to potential difculties in differential diagnosis by imaging alone [ 17 ]  . 
 mr imaging protocol all mr imaging studies were performed on a 1.5 - t system ( magnetom avanto , siemens medical systems , erlangen , germany ) equipped with a surface phased - array body coil . 
volumetric , fatsaturated , t1 - weighted , volume interpolated , breath - hold examination ( vibe ) sequence was used for the dynamic study before and 30 , 70 and 300 s after i.v. 
images were acquired also in the hepatospecic phase at about 1 h after contrast administration . dwi was performed before the dynamic study , with a respiratory - triggered , single - shot echo - planar sequence implementing motion - probing gradients . 
fat saturation with spectral adiabatic inversion recovery ( spair ) was applied to reduce artefacts , together with parallel imaging ( generalised autocalibrating partially parallel acquisition ; grappa ) with an acceleration factor of 2 . 
 image analysis image analysis was performed by two radiologists in consensus ( mdp , sp , with 5 and 2 years of experience in abdominal imaging , respectively ) , blinded to the nal lesion diagnosis and to the t1and t2 - weighted and postcontrast images . 
dwi images were analysed with dedicated software ( leonardo syngo , siemens medical systems , erlangen , germany ) , which automatically generated corresponding adc maps with a 3point regression analysis . standard di riferimento lo standard di riferimento consistito nella analisi istologica dopo biopsia o chirurgia per , rispettivamente , 8 e 4 lesioni ( tabella 1 )  . 
le immagini di esami tc o rm effettuati durante un periodo di follow - up di almeno 1 anno a partire dalla rm iniziale ( media di 2 , 8 esami per paziente )  . 
tra gli esami di followup erano incluse tc post - chemio - embolizzazione trans - arteriosa ( tace ) per 9 lesioni diagnosticate come hcc ( vedi oltre )  . 
le lesioni rimaste stabili in numero e dimensioni nonostante lassenza di terapia sono state considerate come benigne ( n = 11 ) , comprese 3 lesioni su fegati cirrotici diagnosticate come noduli displasici . 
una semeiotica sospetta alla rm iniziale , con successivo incremento in numero e / o dimensioni e / o risposta a terapia medica o a procedure interventive ( n = 8 ) ; b . 
un pattern tipico per hcc secondo i criteri della american association for the study of liver diseases ( aasld ) recentemente validati ( n = 19 ) [ 15 ]  . 
indipendentemente dalla semeiotica specica , le ifn e gli ae sono stati inclusi in un singolo gruppo di lfe solide benigne , considerata la difcolt potenziale di diagnosi differenziale attraverso il solo imaging [ 17 ]  . 
 protocollo rm tutti gli studi rm sono stati effettuati su un magnete da 1 , 5 t ( magnetom avanto , siemens medical systems , erlangen , germania ) , utilizzando una bobina phased - array di supercie . 
 la sequenza pesata in t1 volume interpolated breath hold examination ( vibe ) , volumetrica ed a saturazione del grasso , stata usata per lo studio dinamico prima e dopo 30 , 70 e 300 s dalla iniezione endovena ( ev ) di 0 , 1 mmol / kg di gadobenato dimeglumina ( multihance , bracco , milano , italia )  . 
 lo studio dwi stato acquisito prima dello studio dinamico mediante una sequenza triggerata con il respiro di tipo single - shot echo - planare con gradienti sensibili alla diffuradiol med ( 2013 ) 118 : 343355 table 2 acquisition parameters of the magnetic resonance ( mr ) imaging protocol . 
for heterogeneous lesions , one to three rois as large as possible up to 1 , 256 mm2 ( depending on lesion dimensions ) were positioned , avoiding areas of necrosis and / or haemorrhage and / or including solid areas with different signal intensity . 
le immagini dwi sono state analizzate mediante software dedicato ( leonardo syngo , siemens medical systems , erlangen , germania ) , grazie al quale sono state elaborate e presentate automaticamente anche le mappe adc calcolate con una regressione lineare su 3 punti . i radiologi hanno provveduto alla q - adc delle lfe po348 radiol med ( 2013 ) 118 : 343355 isointense to hyperintense on b = 800 s / mm2 images and hypointense on adc maps , whereas they were assessed as benign if isointense to hyperintense on adc maps , regardless of their appearance on dwi images . 
those of cirrhotic or noncirrhotic liver parenchyma . receiving operating characteristics ( roc ) analysis was performed : ( a ) to determine the adc threshold corresponding to best sensitivity and specicity of adc - q in diagnosing malignancy ; ( b ) to compare areas under the curve ( aucs ) of va vs . 
data cross - tabulation after comparison with standards of reference led to the calculation of sensitivity , specicity , positive ( ppv ) and negative ( npv ) predictive values and accuracy for malignancy of both methods . 
an alfa value < 0.05 was considered statistically signicant by adjusting it with the bonferroni correction in case of multiple pairwise comparisons [ 19 ]  . finally , agreement between va and adc - q in diagnosing malignancy of flls was estimated with the statistic . 
in caso di lesioni eterogenee , sono state posizionate da 1 a 3 roi , le pi ampie possibili ( no a 1256 mm2 ) in relazione alle dimensioni delle lesioni , evitando aree di necrosi e / o di emorragia ed eventualmente effettuando il posizionamento su aree solide con diversa intensit di segnale . 
 dopo un intervallo di quattro settimane , lanalisi visiva stata effettuata valutando , per ogni lesione , sia lintensit di segnale nelle immagini dwi acquisite a b = 800 s / mm2 , sia il loro aspetto nella mappa adc . 
abbiamo analizzato anche la mappa adc per tenere in conto leffetto del fenomeno di t2 shine - trough nel determinare liperintensit delle lesioni nelle immagini dwi [ 18 ]  . 
ricorrendo a criteri adottati in precedenza [ 13 ] , le lesioni sono state caratterizzate come maligne se isointense od iperintense nelle immagini a b = 800 s / mm2 ed ipointense in mappa adc ; sono state caratterizzate come benigne quando isointense od iperintense in mappa adc , indipendentemente dal segnale nelle immagini dwi . 
 ci si serviti , inoltre , di una analisi receiving operating characteristics ( roc ) allo scopo di : ( a ) determinare la soglia di adc corrispondente alle migliori sensibilit e specicit della q - adc nella diagnosi di malignit ; ( b ) confrontare le aree sotto la curva ( auc ) di av e q - adc , come misura globale di efcacia diagnostica . 
1 mean apparent diffusion coefcient ( adc ) values measured for focal nodular hyperplasia / hepatocellular adenoma ( fnh / ha ) , hepatocellular carcinoma ( hcc ) and metastases . 
by taking into account the bonferroni correction for pairwise comparisons ( alfa level = 0.017 ) , metastases were shown to have signicantly lower adc compared with fnh / ha and hcc . 
1 diagramma box and whisker per i valori medi di coefciente di diffusione apparente ( adc ) di iperplasia nodulare focale / adenoma epatocellulare ( inf / ae ) , epatocarcinoma ( hcc ) e metastasi . 
tenendo conto della correzione di bonferroni per i confronti appaiati ( alfa pari a 0 , 017 ) , le metastasi hanno mostrato un adc signicativamente minore rispetto al gruppo inf / ae ed allhcc . 
 metastases and fnhs / has showed signicantly lower ( p = 0.0156 ) and higher ( p = 0.0204 ) mean adcs , respectively , compared with those of the noncirrhotic liver parenchyma ( 1.080.6610 - 3 mm2 / s )  . 
la signicativit statistica stata assunta per unalfa inferiore a 0 , 05 , ricorrendo alla correzione di bonferroni in caso di comparazioni appaiate multiple [ 19 ]  . inne , stato stimato lagreement tra av e q - adc nella diagnosi di malignit usando la statistica k di cohen . 
tre lesioni caratterizzate come noduli displasici ed 1 angioma atipico mostravano adc medi di , rispettivamente , 1 , 160 , 08 ( range 1 , 111 , 26 ) ed 1 , 80 10 - 3 mm2 / s . 
 le metastasi e le lesioni del gruppo inf / ae hanno dimostrato valori di adc medio rispettivamente minori ( p = 0 , 0156 ) e maggiori ( p = 0 , 0204 ) nei confronti del parenchima epatico non cirrotico ( 1 , 080 , 6610 - 3 mm2 / s )  . 
 al contrario , non stata osservata differenza signicativa ( p = 0 , 0652 ) fra ladc medio degli hcc e quello dei fegati cirrotici ( 0 , 970 , 1910 - 3 mm2 / s )  . 
 accuracy for malignancy accuratezza nella diagnosi di malignit accuracy of the adc - q for malignancy ( 68.0% ; 95% ci 37.666.1 ) was higher than that of va ( 52.0% ; 95% ci 53.280.1 ) ( table 4 )  . 
 350 radiol med ( 2013 ) 118 : 343355 table 3 distribution of 50 focal liver lesions according to the pattern of signal intensity at dwi at b = 800 s / mm2 / adc map ( visual analysis )  . 
data show that the majority of malignant lesions , particularly hepatocellular carcinoma ( hcc ) , were assessed as false - negative cases , whereas only one benign lesion was assessed as a false - positive case final diagnosis at the standard of reference pattern of signal intensity for benignancy pattern of signal intensity for malignancy isointense / isointense hyperintense / isointense hyperintense / hyperintense hypointense / hypointense hyperintense / hypointense metastases hcc dysplastic nodules fnh / ha atypical haemangioma 8 ( 36.4% ) 1 ( 33.3% ) 6 ( 50.0% ) 4 ( 18.1% ) 2 ( 66.7% ) 3 ( 25.0% ) 3 ( 25.0% ) 8 ( 36.4% ) 2 ( 16.7% ) 1 ( 8.3% ) 9 ( 75.0% ) 2 ( 9.1% ) fnh , focal nodular hyperplasia ; ha , hepatocellular adenoma tabella 3 distribuzione , alla analisi visiva , delle 50 lesioni focali epatiche oggetto di studio in relazione al pattern di segnale nelle immagini pesate in diffusione / mappa adc . 
la maggior parte delle lesioni maligne , specialmente gli epatocarcinomi ( hcc ) , sono stati diagnosticate come falso - negative , mentre 1 sola lesione benigna stata diagnosticata come falso - positiva diagnosi nale allo standard di riferimento metastasi hcc noduli displasici inf / ae angioma atipico pattern di intensit di segnale per benignit pattern di intensit di segnale per malignit isointensit / isointensit 8 ( 36 , 4% ) 1 ( 33 , 3% ) 6 ( 50 , 0% ) iperintensit / isointensit 4 ( 18 , 1% ) 2 ( 66 , 7% ) 3 ( 25 , 0% ) iperintensit / iperintensit 3 ( 25 , 0% ) 8 ( 36 , 4% ) 2 ( 16 , 7% ) ipointensit / ipointensit 1 ( 8 , 3% ) iperintensit / ipointensit 9 ( 75 , 0% ) 2 ( 9 , 1% ) inf , iperplasia nodulare focale ; ae , adenoma epatocellulare the most relevant factor causing the difference in accuracy was the number of false - negative cases . 
adc threshold for malignancy was 1.0910 - 3 mm2 / s according to roc analysis , leading to 13 false - negative cases ( three metastases and ten hccs ) using adc - q . 
remaining metastases and hccs showed a visual pattern suggesting diffusion similar to or greater than the surrounding parenchyma on the adc map , corresponding to three and 20 false - negative cases , respectively . 
concerning benign lesions , all were correctly characterised by both methods , except for one and three false - positive cases with va ( one ha ) and adc - q ( one fnh and two has below the threshold for malignancy ) , respectively . 
la soglia di malignit per ladc risultata 1 , 0910 - 3 mm2 / s allanalisi roc , determinando 13 casi falsi negativi ( 3 metastasi e 10 hcc ) usando q - adc . 
i rimanenti casi di metastasi ed hcc mostravano , nella mappa adc , un pattern di segnale suggestivo per una diffusione uguale o superiore a quella del parenchima epatico circostante , determinando rispettivamente 3 e 20 falsi negativi . 
per quanto riguarda le lesioni benigne , esse sono state correttamente caratterizzate da entrambi i metodi , fatta eccezione per i seguenti falsi positivi : nel caso della av 1 ae ; nel caso della q - adc 1 inf e 2 ae con adc al di sotto della soglia di malignit . 
nel complesso , quindi , la av ha dimostrato una specicit ed un vpp superiori rispetto alla q - adc ( tabella 4 )  . i risultati della straticazione sono mostrati in tabella 5 . 
 agreement tra q - adc e av sebbene i criteri di sospetto siano stati riscontrati solo in 11 / 34 lesioni ( 32 , 3% ) alla av e 21 / 34 lesioni ( 61 , 7% ) alla q - adc , la loro presenza stata altamente predittiva per malignit , come attestato da un vpp alto per entrambi i metodi ( tabella 4 )  . 
daltra parte , la diagnosi corretta di malignit stata effettuata con la sola q - adc in 10 casi di hcc , ed in nessun caso con la sola av . 
 discussione abbiamo ipotizzato che la av potesse sostituire la stima delladc sulla base dei seguenti assunti : ( a ) la av consente una approccio pi immediate alle lfe , poich essa ricalca lo standard di interpretazione visiva delle immagini radiotable 4 diagnostic performance of visual analysis ( va ) and apparent diffusion coefcient quantication ( adc - q ) in differentiating malignant vs . 
 agreement between adc - q and va although va and / or adc - q criteria for suspicion were found only in 11 / 34 ( 32.3% ) and 21 / 34 ( 61.7% ) lesions , respectively , their presence was highly predictive for malignancy , corresponding to a high ppv for both methods ( table 4 )  . 
 discussion we hypothesised that va might replace adc estimates based on the following statements : ( a ) va permits an easier approach to flls , as it parallels the standard of interpretation approach to radiological images ; ( b ) va does not need workstation and time - consuming measurements [ 13 ] ; ( c ) 100 - specicity fig . 
2 aree sotto la curva ( auc ) dellanalisi visiva ( av ) e della quanticazione del coefciente di diffusione apparente ( q - adc ) determinate dallanalisi receiving operating characteristic ( roc )  . 
le soglie della quanticazione del coefciente di diffusione apparente ( q - adc ) di malignit sono risultate , rispettivamente , 0 , 91 e 1 , 0910 - 3 mm2 / s q - adc accuratezza per metastasi ( % ) accuratezza per hcc ( % ) 9 , 1 ( 1 , 429 , 2 ) 75 , 0 ( 54 , 888 , 6 ) 66 , 7 ( 46 , 482 , 5 ) 54 , 4 ( 32 , 275 , 5 ) av , analisi visiva radiol med ( 2013 ) 118 : 343355 logiche ; ( b ) la av non richiede misurazioni time - consuming e lutilizzo di workstation dedicate [ 13 ] ; ( c ) la av non dipende da una soglia di interpretazione dei dati a forte variabilit . 
innanzitutto , abbiamo escluso dallanalisi cisti ed angiomi poich tali lesioni mostrano , rispetto alle lfe benigne solide , sia adc caratteristicamente alti sia una semeiotica del segnale tipica [ 21 ] , determinando il rischio di sovrastimare laccuratezza della dwi per lesioni di maggior rilievo clinico . 
la dwi , infatti , sarebbe pi utile nella caratterizzazione di lesioni solide benigne o maligne , poich difcile , spesso , operare questa distinzione in rm , specie se non si ricorre alla somministrazione di mezzo di contrasto [ 2 ]  . 
3a - c false - negative case of a 63 - year - old male patient with hepatic cirrhosis , - fetoprotein elevation and multifocal hepatocellular carcinoma ( hcc )  . 
larger lesion showed slightly inhomogeneous hyperintensity on the image at higher b value ( 800 s / mm2 ) ( a ) and hyperintensity on the apparent diffusion coefcient ( adc ) map ( b ) , suggesting preserved diffusion with t2 shine - through affecting the diffusion - weighted image ( dwi )  . 
la lesione di maggiori dimensioni mostrava segnale iperintenso , lievemente disomogeneo nelle immagini a massimo b value ( 800 s / mm2 ) ( a ) ed iperintensit in mappa adc ( b ) , a suggerire una diffusivit conservata e la presenza delleffetto t2 shinethrough contaminante le immagini pesate in diffusione . 
first , we excluded cysts and haemangiomas from the analysis because of the signicantly higher adc and more typical signal intensity features they show compared with solid flls [ 21 ] , leading to the risk of overestimating dwi accuracy for clinically relevant lesions . 
indeed , dwi would be more helpful for characterising solid lesions as benign or malignant , as it is often difcult to make this distinction on mri , especially without contrast medium administration [ 2 ]  . 
on the contrary , hccs were the most prevalent malignant flls in our series ( n = 22 ) , with an average adc of 1.1910 - 3 mm2 / s . 
 conversely , when stratifying for metastases ( n = 12 ) , we showed that : ( a ) adc ( 0.8710 - 3 mm2 / s ) was signicantly lower than that of hcc and the group of fnh / ha ( 1.23103 mm2 / s ) ; ( b ) three false - negative cases only were found with va . 
to detect restricted diffusivity , we analysed adc maps to correct for the t2 - shine - through effect , thus determining hyperintensity at a higher b value [ 18 ]  . 
first , hyperintensity on images with stronger diffusion weighting might be related mainly to the increase in tumour t2 relaxation time rather than to restriction of water diffusion within hcc [ 22 ]  . 
al contrario , gli hcc sono state le lesioni maligne predominanti nel nostro studio ( n = 22 ) , con un adc medio di 1 , 1910 - 3 mm2 / s . 
gli hcc hanno rappresentato la sorgente principale di casi falsi negativi ( 10 per la q - adc e 20 per la av ) , rendendo ragione di una sensibilit straticata davvero deludente sia per la av ( 9 , 1% ) , sia per la q - adc ( 54 , 4% )  . 
gli hcc falsi negativi hanno rappresentato anche la causa del poco soddisfacente valore di agreement fra i due metodi ( k = 0 , 51 ) nella diagnosi di malignit . 
al contrario , straticando lanalisi per le metastasi ( n = 12 ) , abbiamo evidenziato che : ( a ) ladc ( 0 , 8710 - 3 mm2 / s ) era signicativamente minore rispetto a quello dellhcc e del gruppo inf / ae ( 1 , 2310 - 3 mm2 / s ) ; ( b ) i casi falsi negativi usando la av sono risultati solamente 3 . 
in sostanza , la av ha dimostrato una performance diagnostica migliore per le metastasi rispetto alla q - adc , sebbene laccuratezza sia comunque inferiore rispetto a quella riportata da battal et al . 
al ne di identicare con sicurezza una ridotta diffusivit , abbiamo analizzato le mappe adc , le quali consentono di correggere leffetto di t2 - shine - through ( trascinamento del t2 ) che causa iperintensit ( ai b values pi alti ) non legata alla restrizione della diffusione [ 18 ]  . 
primo , liperintensit nelle immagini a pi forte pesatura in diffusione potrebbe essere legata pi allincremento del tempo di rilassamento t2 dellhcc che alla restrizione della diffusione intralesionale [ 22 ]  . 
secondo , il fenomeno di t2 shine - through potrebbe inuenzare , in realt , anche il segnale delle mappe adc , come dimostrato per alcune lesioni cerebrali [ 23 , 24 ]  . 
al contrario dellhcc , le metastasi presentavano il segnale atteso in caso di restrizione della diffusivit [ 25 ] nella maggior parte dei casi ( 75 , 0% )  . 
 i nostri risultati suggeriscono che i pattern di segnale dellhcc e delle metastasi potrebbero essere sostanzialmente differenti in relazione a determinanti istologici , ma questo assunto dovrebbe essere vericato da studi ulteriori di correlazione radio - patologica . abbiamo osservato che la av aggiunge specicit rispetto alla q - adc ( incremento dall81 , 3% al 93 , 8% ) , in accordo con battal et al . 
nonetheless , it remains a suboptimal tool because , in accordance with well - established results [ 21 ] , we found that adc values of hcc signicantly overlap with those of the group of fnh / ha . 
as known , larger b value leads to lower adc by reducing the inuence of t2 - weighting and perfusion on dwi images and adc maps [ 1 ]  . 
first , sample size is relatively small because , unlike most authors [ 3 , 5 , 14 , 26 ] , we excluded from the analysis cysts and haemangiomas with typical appearance , as explained above . 
this limitation reects clinical practice , in which dwi is used to characterise lesions that often do not need histological demonstration to be treated , as occurs for typical hccs and metastases . 
third , no denite adc threshold for malignancy was used to perform adc - q analysis , as occurs in clinical practice , because of adc variability ( see above )  . 
overall , the accuracy for malignancy was disappointing with both methods because of the overlap in visual appearance and adc values of benign and malignant flls . acknowledgements acknowledgments to alessandro furlan , from the department of radiology , university of pittsburgh medical center , for the thoughtful revision of this manuscript . conict of interest none come abbiamo osservato in accordo con risultati consolidati [ 21 ] , i valori di adc dellhcc si sovrappongono signicativamente a quelli del gruppo inf / ae . 
va sottolineato che i valori di adc e le soglie di malignit che abbiamo osservato ( rispettivamente 1 , 09 e 0 , 9110 - 3 mm2 / s per hcc e metastasi ) sono risultati pi bassi rispetto a quelli riportati in precedenti esperienze ( con massimo b value no a 600 s / mm2 ) [ 21 ]  . 
come noto , infatti , b values maggiori determinano adc minori riducendo linuenza della pesatura in t2 e della componente di perfusione microcapillare sulle immagini dwi e sulla mappa adc [ 1 ]  . 
primo , la dimensione campionaria relativamente piccola perch , a differenza della maggior parte di altri autori [ 3 , 5 , 14 , 26 ] , abbiamo escluso dallanalisi cisti ed angiomi sulla base del razionale descritto sopra . 
secondo , non stata disponibile la conferma istologica per la maggior parte delle lfe ( specialmente nel caso degli hcc ) , con la conseguente impossibilit di stabilire una relazione fra caratteristiche istologiche ed i pattern di intensit di segnale o gli adc . 
tale limite rispecchia quanto accade nella pratica clinica , nella quale la dwi potrebbe essere demandata a caratterizzare lesioni che spesso non richiedono conferma istologica per essere trattate , come accade per gli hcc tipici e per le metastasi . 
terzo , non stata usata una soglia denita di adc nello stabilire la malignit mediante q - adc , come del resto accade nella pratica clinica in relazione alla notevole variabilit delladc stesso ( vedi sopra )  . 
poich abbiamo osservato che esattamente come accade per la av esiste un signicativo overlap di adc per lhcc , ragionevole concludere che il nostro modello abbia fornito dei risultati consistenti . in conclusione , nel differenziare lfe come maligne o benigne la av si dimostrata , rispetto alla q - adc , meno accurata per lhcc e pi accurata per le metastasi . 
cuore , largo gemelli 8 , 00168 roma , italy 2istituto nazionale di riposo e cura dellanziano ( inrca ) , roma , italy 3istituto di bioimmagini e scienze radiologiche delluniversit cattolica del s . 
cuore , roma , italy 4consiglio nazionale delle ricerche presso ministero dellambiente , roma , italy 5istituto nazionale di riposo e cura dellanziano ( inrca ) , ancona , italy 6istituto di radiologia , universit g . 
the authors examined all insurance claims relating to presumed errors in interventional radiology led by radiologists over a period of 14 years after isolating them from the insurance database of all radiologists registered with the italian society of medical radiology ( sirm ) between 1 january1993 and 31 december 2006 . 
sono state esaminate tutte le denunce assicurative causate da presunti errori in radiologia interventistica in un periodo di 14 anni , enuncleandole dal data - base assicurativo dei radiologi iscritti alla societ italiana di radiologia medica ( sirm ) dal 01 / 01 / 1993 al 31 / 12 / 2006 . 
la radiologia interventistica , attivit sovrapponibile per prolo di rischio biologico alle procedure chirurgiche , espone gli operatori ad un elevato rischio di contenzioso medico - legale sia per problemi intrinseci alle tecniche usate , sia per la necessit di radiol med ( 2013 ) 118 : 504517 conclusions . 
adopting good radiological practices , scrupulous review of procedures and efciency of the instruments used and audit of organisational and management processes are all factors that can help reduce the likelihood of error . 
ladozione di buone pratiche radiologiche , la scrupolosa revisione delle procedure e dellefcienza tecnica degli strumenti usati , la verica delle procedure organizzative e gestionali sono i fattori che riducono la probabilit dellerrore . 
the risk of italian radiologists facing a lawsuit for presumed malpractice is progressively increasing and is estimated to be in the order of 44 per 1 , 000 , corresponding to a probability > 1 of being sued in the course of their working life [ 1 ]  . 
this risk is comparable with that reported for other european countries [ 2 , 3 ] and the united states [ 46 ] , which have seen a tendency of radiologists to abandon disciplines considered to be at higher risk of litigation [ 79 ]  . radiologists incurring a malpractice claim tend at times to adopt a defensive approach in their professional practice [ 10 ]  . 
in a pilot study conducted on a group of italian radiologists and radiotherapists [ 11 ] , we observed that one third ( 33.4% ) had faced a civil or criminal proceeding for presumed malpractice , and 9.5% had faced more than one . 
among those who had incurred a claim , there was a higher incidence ( > 60% ) of anxiety , anger and , in one third of cases , helplessness , disappointment , anguish and humiliation ; one in 20 reported the appearance of physical symptoms following the claim , and almost 40% admitted having modied their professional practice by adopting a defensive medicine approach . interventional radiology , dened as any minimally invasive endoor extravascular therapeutic procedure performed under the guidance of uoroscopy , sonography or computed tomography , is closer in terms of occupational risk prole to the surgical disciplines [ 12 ]  . 
il rischio di ricevere una denuncia per presunta malpractice nei radiologi italiani in progressivo aumento ed attualmente stimato nellordine del 44 per mille , il che corrisponde ad una probabilit maggiore di uno di essere citato nel corso della propria vita professionale [ 1 ]  . 
tale rischio risulta oggi paragonabile a quello rilevato in altri paesi europei [ 2 , 3 ] e negli stati uniti [ 46 ] , dove stata osservata la tendenza dei radiologi ad abbandonare la pratica nei settori ritenuti pi a rischio di denunce [ 79 ]  . i radiologi che ricevono una denuncia tendono talora a modicare in senso difensivo la propria condotta professionale [ 10 ]  . 
in uno studio - pilota condotto su un gruppo di radiologi e radioterapisti italiani [ 11 ] abbiamo osservato che un terzo di essi ( 33 , 4% ) aveva subito denunce civili o penali per supposta malapratica , e che il 9 , 5% era stato denunciato pi di una volta . 
 materials and methods data were derived from the cohort of italian radiologists who took out a professional civil liability insurance with sirm between 1 january 1993 and 31 december 2006 . 
the mean observed cohort was 2 , 871 per year , and the total number of the cohort ( group of individuals at risk of litigation ) was to 40 , 201 persons per year ( with as many 1 - year - long observations )  . 
the group of interventional radiologists are estimated to account for a maximum of 7% of the total population , that is , 2 , 814 persons per year . each radiologists claims were examined in anonymous forin addition , to safeguard condentiality , we were not allowed access to all documentation but only to the reported motivation of the claithe analysis took into account setting ( public or private facility ) , date of the event , date of ling the claim and outcome ( death or injury ) of the event . for the purposes of the study , we included among the interventional techniques all those listed by the society of interventional radiology ( sir ) [ 16 ] : angiography , angioplasty , biliary stenting , central venous access , embolisation and chemoembolisation , gastrostomy , maintenance of haemodynamic accesses , needle biopsies , procedures on telangiectasias , radiofrequency ablation , stenting , stentgrafting , thrombolysis , transjugular intrahepatic shunt , vertebroplasty , aneurysm repair , arteriovenous malformations , bleeding , thrombosis , application of caval lters , drainage procedures and catheterisation . avvicina , per ci che riguarda il rischio professionale , alle discipline chirurgiche pi che a quelle mediche [ 12 ]  . 
anche sotto il prolo medico - legale la radiologia interventistica pi simile alla chirurgia che alla medicina ; difatti , mentre in questultima , come nella radiodiagnostica , il contenzioso origina prevalentemente da comportamenti di tipo omissivo , nella radiologia interventistica come in chirurgia esso prevalentemente di tipo commissivo . negli stati uniti circa un terzo di tutte le denunce contro i radiologi conseguono a procedure interventistiche [ 13 ] e questa quota sembra in aumento , anche se potrebbe darsi che laumento delle denunce sia solo conseguenza dellaumento delle procedure eseguite [ 14 ]  . 
 nel 2006 , su 8145 radiologi iscritti alla societ italiana di radiologia medica ( sirm ) , 574 ( 7 , 0% ) hanno aderito alla sezione di radiologia vascolare ed interventistica . 
questo numero in costante aumento dal 1995 , quando erano 351 ( su 5757 iscritti , 6 , 1% )  . scopo di questo lavoro di valutare la frequenza ed il tipo di denunce che riguardano gli operatori di radiologia interventistica , al ne di individuare le pi corrette procedure per prevenire tale fenomeno . 
 materiali e metodi la base - dati ricavata dalla coorte dei radiologi italiani che hanno sottoscritto lassicurazione di responsabilit civile professionale con la sirm dal 01 / 01 / 1993 al 31 / 12 / 2006 . 
il numero medio di persone osservate in ciascun anno 2871 ed il totale della coorte ( gruppo di individui che hanno in comune il rischio di denuncia per responsabilit civile ) conta 40201 persone / anno ( cio comprende altrettante osservazioni della durata di un anno )  . 
la coorte di radiologi interventisti si pu stimare pari al massimo al 7% della popolazione totale , cio 2814 persone / anno . le segnalazioni effettuate da ciascun radiologo , sono state esaminate in forma anonima e , per ragioni di riservatezza , non stato consentito laccesso allintera documentazione bens alla sola motivazione della denuncia . 
si tenuto conto della sede ( struttura pubblica o privata ) , della data di occorrenza , della data di presentazione della denuncia e dellesito ( decesso o lesioni ) dellevento lesivo denunciato . ai ni del presente lavoro , abbiamo incluso tra le tecniche interventistiche quelle elencate dalla society of interventional radiology ( sir ) [ 16 ] : angiograa , angioplastica , radiol med ( 2013 ) 118 : 504517 as observed in our previous studies conducted on the same cohort of radiologists , only part of the claims were led the same year of the event ; the majority were led up to 10 years later [ 1723 ]  . 
the considerable time lag between the event and the claim complicated the analysis in that the number of claims related to procedures performed during the study period is still incomplete . 
following a method adopted in previous studies [ 1 ] , in order to obtain an estimate of claims relating to all events occurring in the study period , we calculated the latency period of the older claims for which the right to civil compensation can be considered extinct and then applied the same latency period to extrapolate the number of claims still to be led after the end of the study period , based on the formula : xi = ni / pk where x , the number of claims still to be led relating to each year of activity , will equal the number n of claims already led , divided by the cumulative percentage p of claims led during the rst years of the study period at a distance k from the harmful event . 
this method assumes that the tendency to sue radiologists is constant over time , and therefore represents an underestimation of the phenomenon , considering that the tendency of italian patients to sue physicians is currently greater than observed years ago [ 24 , 25 ]  . to calculate the risk of an interventional radiologist facing a malpractice claim , we divided the number of claims estimated as reported above by the number of radiologists practising interventional radiology in our cohort ( 2 , 814 persons per year ) , assuming that an interventional radiologist has an equal tendency to take out insurance as do other sirm members , and therefore that 7% of the study population practised interventional radiology . 
in 12 cases ( 12% ) , the description available did not allow us to identify with any stenting biliare , accesso venoso centrale , embolizzazione e chemoembolizzazione , gastrostomia , mantenimento di accessi emodinamici , agobiopsia , interventi su teleangectasie , ablazione a radiofrequenze , stent , stent - graft , trombolisi , shunt intraepatico transgiugulare , vertebroplastica , trattamento di aneurismi , malformazioni arterovenose , sanguinamenti , trombosi , applicazione di ltri cavali , drenaggi , cateterizzazioni . come gi osservato in altri studi da noi condotti sulla stessa coorte di radiologi , solo una parte delle denunce stata sporta nello stesso anno dellevento lesivo , mentre la maggior parte viene avanzata dopo uno , due o pi anni , no a un massimo di dieci anni dallevento [ 1723 ]  . 
la notevole latenza tra evento lesivo e denuncia complica la valutazione del fenomeno , in quanto il numero di denunce relative alle attivit radiologiche svolte nel periodo in esame deve ritenersi ancora incompleto . 
seguendo un metodo gi impiegato in precedenti lavori [ 1 ] per ottenere una stima del numero di denunce che si riferiranno a tutti gli eventi occorsi nel periodo di osservazione , abbiamo calcolato la latenza delle denunce relative agli anni pi lontani , per i quali si pu ormai ritenere estinto il diritto al risarcimento civile , e abbiamo quindi estrapolato il numero di denunce che perverranno , osservando la stessa latenza , dopo la conclusione del periodo di osservazione , in base alla formula : xi = ni / pk secondo cui il numero x di denunce che perverranno , riferite ad ogni singolo anno lavorativo , sar uguale al numero attuale n di denunce , diviso per la percentuale cumulativa p di denunce stabilizzate che si sono registrate nei primi anni di osservazione alla distanza k dellevento lesivo . 
tale metodo si basa sullipotesi che la propensione a denunciare i radiologi sia costante nel tempo , e rappresenta quindi una sottostima del fenomeno , in considerazione del fatto che la propensione ad avviare procedimenti per malapratica contro i medici da parte dei pazienti italiani attualmente risulta maggiore di quella che si osservava anni fa [ 24 , 25 ]  . per calcolare il rischio di ricevere una denuncia da parte di un radiologo che si occupa di radiologia interventistica abbiamo diviso il numero di denunce cos stimato per il numero di radiologi che si occupano di radiologia interventistica nella nostra coorte ( 2814 persone / anno ) , ipotizzando che la propensione ad assicurarsi per un radiologo interventista sia uguale a quella degli altri radiologi che si iscrivono alla sirm , e quindi che il 7% della popolazione da noi osservata si occupi di radiologia interventistica . 
 risultati nel periodo di osservazione sono state inoltrate 98 denunce table 1 number of claims per year of ling and per year of occurrence , and estimate of the number of claims expected 7 years after the end of the study period claims led , n ( % ) occurrence of harmful event , n ( % ) correction factora expected cases radiol med ( 2013 ) 118 : 504517 508 year 1993 1994 1995 1996 1997 1998 1999 2000 2001 2002 2003 2004 2005 2006 tot . 
the mean amount of compensation claimed for each event was 838 , 633 , considerably more than that claimed over the same period for events caused by radiological procedures , which was equal to 524 , 126 [ 25 ]  . 
 these proportions reect the relative distribution of public and private interventional radiology centres [ 15 ]  . at the end of the study period , fewer than half of litigations had been settled ( judicially or extrajudicially ) , so it ( tabella 1 )  . 
una valutazione dettagliata ( tabella 2 ) indica come causa pi frequente il manifestarsi di complicanze dopo procedure interventistiche del distretto vascolare ( 43 casi , pari al 43 , 9% )  . 
con frequenza inferiore si sono registrate denunce per complicanze dopo ago - biopsia ( 14 casi , 14 , 3% ) o dopo sclero - embolizzazione o termo ablazione ( 12 casi , 12 , 2% )  . 
un altro evento segnalato come causa della denuncia la rottura accidentale di cateteri o protesi con migrazione di parti meccaniche nel distretto vascolare , sia arterioso che venoso ( 6 casi , 6 , 1% )  . 
meno frequenti sono le denunce derivanti da lesioni sul rachide ( 4 casi , 4% ) , da omessa o ritardata esecuzione dellesame ( 3 casi , 3% ) o da omesso o inadeguato consenso informato ( 4 casi , 4 , 1% )  . 
it should be remembered that the distribution of claims per year of occurrence is incomplete in that the last year of the study ( 2006 ) only includes claims led within the same year of the event , in 2005 only those led up to 1 year after the event and in 2004 up to 2 years after , etc . 
only 29 claims ( 30% ) were led during the same year of the event ; all the others were led up to a maximum of 7 years after the event . 
 assuming the hypothesis that the tendency to sue is constant , the latency of claims during the rst 7 years of observation ( table 3 ) will be equal to that observed for the following years of the cohort . 
 12 casi ( 12% ) la descrizione in nostro possesso non ha consentito di identicare con certezza il tipo di problema che stato allorigine della denuncia . le conseguenze presunte per i pazienti sono state il decesso in 21 casi ( 21 , 4% ) , le lesioni nei rimanenti 77 ( 78 , 6% )  . 
 lindennizzo medio richiesto per ciascun sinistro stato di 838633 euro , largamente superiore allimporto medio richiesto in italia nello stesso periodo per ciascun sinistro in ambito radiologico , che pari a 524126 euro [ 25 ]  . 
gli incidenti si sono vericati per lo pi in strutture pubbliche ( 81 casi , 82 , 7% ) , mentre nelle strutture private accreditate si sono avuti 17 casi ( 17 , 3% )  . 
tali proporzioni ricalcano la distribuzione dei centri di radiologia interventistica tra strutture pubbliche e private [ 15 ]  . alla conclusione del periodo di osservazione , meno di met delle controversie risulta chiusa ( in sede giudiziaria o extragiudiziaria ) ; non possibile quindi sapere quante delle denunce si siano effettivamente risolte in danno dello specialista radiologo . 
solo 29 denunce ( 30% ) risultano presentate nello stesso anno dellevento lesivo ; tutte le altre denunce sono state presentate dopo uno o pi anni dallevento lesivo , no a un massimo di 7 anni . 
 accettando lipotesi che la tendenza a denunciare sia costante , la latenza delle denunce nei primi sette anni di osservazione ( tabella 3 ) sar uguale a quella che si potr osservare per i successivi anni della coorte . 
ci equivale a dire che i radiologi interventisti hanno la certezza statistica ( probabilit pari a uno ) di ricevere mediamente una denuncia ogni 21 , 1 anni di attivit . 
tale tasso di rischio non risulta signicativamente diverso da quello cui si trova esposto qualunque radiologo italiano , che stimato nel periodo in esame pari a 44 per mille [ 1 , 25 ]  . discussione il nostro studio evidenzia che , al contrario di quel che ci si sarebbe potuto attendere considerando lelevato rischio intrinseco alle procedure interventistiche , la probabilit di essere denunciati per i radiologi che effettuano attivit interventistiche non sostanzialmente diversa da quello che corrono tutti i radiologi . 
ben noto che la radiologia interventistica trova applicazione elettiva in pazienti con gravi patologie e che spesso lintervento del radiologo interventista richiesto in urgenza / emergenza , in situazioni ad elevato rischio clinico . 
il fatto che la frequenza delle denunce per i radiologi interventisti sia invece simile a quella generale della disciplina quindi da attribuire in primo luogo alle doti professionali dei radiologi interventisti italiani che operano in qualicati centri pubblici o privati . 
 discussion our study showed that , in contrast to expectations considering the high intrinsic risk of interventional procedures , the likelihood of operators being sued does not differ substantially from that of all radiologists . 
it is well known that interventional radiology has an elective application in severely ill patients and that often the procedure is requested in emergenda richieste di risarcimento , che sono sensibilmente pi elevate di quelle medie della disciplina , o da processi penali per omicidio o lesioni personali gravi . 
 al di l dei risvolti giudiziari , la denuncia da parte di un paziente pu indurre nel radiologo denunciato la comparsa di una sindrome da stress professionale , con disturbi obiettivabili sul piano psicosico che spesso sono presenti a distanza notevole dallevento . 
the fact that the frequency of claims against interventional radiologists is instead similar to that seen among radiologists in general is therefore to be ascribed rstly to the professional skills of the interventional radiologists operating in qualied public or private centres . 
however , even the best operators can incur litigation and be called upon to defend themselves from claims for damages ( for amounts that are , on average , substantially higher than those received by diagnostic radiologists ) or in trials for homicide or severe bodily injury . 
 beyond the legal consequences , a claim led by a patient may cause the radiologist to develop professional stress syndrome , with objective psychological and physical disorders persisting even a long time after the event . 
the professional may be induced to change clinical practice and adopt a so - called defensive approach , which is considered the rst cause of increased healthcare expenditure , or may even abandon the practice that generated the litigation . 
data are based on a sufciently large study population ( around 50% of practising italian radiologists registered with sirm ) , which was followed over a long period of time . 
on the other hand , whereas a period of 14 years is longer than considered in similar investigations conducted abroad , it may be insufcient to describe the phenomenon of medicolegal litigation in italy , as claims can be led even many years after the presumed harmful event and civil lawsuits are abnormally long ( reason we are unable to determine the outcome of most claims led )  . 
as the rst type of systematic error would lead to underestimating the expected number of claims and the second to overestimate it , it can be assumed that the nal effect on the claim rate would be irrelevant and thus conrm our estimate . 
a further limitation concerns the fact that insurance claims were examined in anonymous form , and condentiality concerns allowed access to the main cause for the claim as communicated by the radiologist but not to the entire documentation . 
where this description was excessively reticent , we were unable to track down the cause of the malpractice claiseveral questions our study has left unanswered could be only addressed by studying the legal proceedings for which a verdict has been reached . 
we hope that in italy it will be soon possible to access medical malpractice databases , such as the one recently created for research purposes by the catholic university of sacred heart and the court of rome . re indotto a modicare la propria pratica clinica nel senso della cosiddetta medicina difensiva , che ritenuta la prima causa dellaumento della spesa sanitaria , o addirittura ad astenersi dallattivit che ha generato il contenzioso . 
i dati presentati sono tratti da una popolazione sufcientemente numerosa ( circa il 50% dei radiologi italiani in attivit e iscritti alla societ scientica ) , seguita per un lungo arco temporale . 
daltra parte una limitazione del nostro studio che un intervallo di 14 anni , seppure molto pi protratto di quello degli studi condotti oltre frontiera , potrebbe essere comunque insufciente a descrivere il contenzioso medico - legale italiano , a causa della possibilit di rivendicare il risarcimento molti anni do po levento che lo avrebbe causato , e della abnorme durata dei processi civili ( per cui non ancora possibile conoscere il risultato della maggior parte delle azioni intentate )  . 
 anche la stima da noi operata sul numero totale di denunce attese potrebbe discostarsi dalla realt sia se , nel corso degli anni , dovesse aumentare la propensione a denunciare i medici , sia se dovesse aumentare la percentuale dei radiologi che effettuano tecniche interventistiche . 
poich il primo tipo di errore sistematico porterebbe a sottostima re il numero atteso di denunce , e il secondo a sovrastimarlo , presumibile comunque che il risultato nale sul tasso di denunce sia irrilevante , confermando quindi la nostra stima . 
una ulteriore limitazione riguarda il fatto che le segnalazioni sono state esaminate in forma anonima e , per ragioni di riservatezza , non stato possibile laccesso allintera documentazione , ma solo alla causa principa le segnalata dal radiologo . 
ci si augura che sia presto possibile nel nostro paese laccesso a banche - dati sulla malapratica medica , quale quella recentemente progettata a questo scopo dalluniversit cattolica del sacro cuore e dal tribunale di roma . in generale , le denunce assicurative di responsabilit civile verso i radiologi riguardano soprattutto la mancata o omessa diagnosi nella interpretazione dei reperti iconograci [ 2628 ]  . 
negli stati uniti la maggior parte delle denunce civili contro i radiologi interventisti sostenuta per battery , cio per avere effettuato una attivit invasiva senza avere priradiol med ( 2013 ) 118 : 504517 in general , insurance claims for civil liability of radiologists mainly concern misdiagnosis or nondiagnosis in interpreting imaging ndings [ 2628 ]  . 
in the united states , most civil litigations against interventional radiologists refer to cases of medical battery ; that is , having performed an invasive procedure without having rst sought the patients consent . 
 american law in fact affords absolute protection of an individuals integrity : whereas the courts sometimes accept that the most basic medical procedures physical examination or venous blood sampling may be performed on the basis of the implicit consent of the patient who went to the medical ofce , explicit consent is required for all other procedures ( generally only verbal , but must still be requested and expressed )  . 
without consent , the physician can be charged with intentional injuries and be condemned , in addition to paying damages , to administrative nes that are not covered by insurance policies . 
a smaller proportion of claims against interventional radiologists in the united stated is due to negligence concerning the way the procedure was performed , incompleteness of the consent obtained , early or late complications and communication of results to the patient and referring physician [ 29 ]  . 
in these cases of malpractice , the burden of proof of the injury lies with the plaintiff . despite the considerable differences between legal systems in italy and the united states , our cohort showed the same causes of claims as those reported for north american radiologists . 
we therefore believe that to reduce the probability of litigation or to improve the possibility of defence , it is necessary to make use of all measures that experience and good clinical practice suggest . preventive measures prior to examination , maximum attention should be paid to the principle of justication of medical acts when selecting the patient . 
the indication for an interventional procedure is proposed by the referring physician but should be shared by the radiologist after careful analysis of the possibilities , risks , alternatives and benets : the diagnostic or therapeutic goals must justify the risk inherent in the procedure weighed against the expected benets . 
nella dottrina americana infatti lintegrit della persona tutelata in modo assoluto : le corti accettano talora che lo svolgimento delle procedure mediche pi elementari , come la visita medica o il prelievo venoso , possa avvenire sulla base di un consenso implicito da parte del paziente che si recato presso lo studio medico , mentre per tutte le altre operazioni richiesto un consenso esplicito ( generalmente solo verbale , ma che deve essere formalmente richiesto ed espresso )  . 
in difetto , il medico pu essere incriminato per lesioni intenzionali ed essere condannato , oltre al risarcimento , anche a sanzioni amministrative che non sono coperte dalle polizze assicurative . 
una quota proporzionalmente minore delle denunce contro i radiologi interventisti statunitensi dovuta a negligenza , riguardante le modalit di svolgimento della procedura , lincompletezza del consenso ottenuto , le eventuali complicazioni anche tardive e la comunicazione dei risultati al paziente e al medico curante [ 29 ]  . 
in questi casi di malpractice lonere della prova del danno grava sul richiedente . nonostante le profonde differenze del nostro sistema giuridico con quello americano , nella nostra coorte ricorrono gli stessi motivi di denuncia evidenziati a carico dei radiologi doltreoceano . 
riteniamo quindi che per ridurre le probabilit di incorrere in contenzioso o per migliorare le possibilit di difesa , sia opportuno ricorrere a tutte le misure che lesperienza e la buona pratica clinica consigliano . le misure di prevenzione nella fase che precede lesame , la massima attenzione va posta al principio di giusticazione dellatto medico nella selezione del paziente . 
lindicazione alla procedura interventistica proposta dal medico curante , ma deve essere condivisa dal radiologo esecutore sulla base di una attenta analisi di possibilit , rischi , alternative e beneci : le nalit diagnostiche o terapeutiche devono giusticare il rischio insito nella procedura a fronte dei beneci attesi . 
con la rma del modulo di consenso informato il paziente dimostra di essere stato completamente informato su tutti gli aspetti dalla prestazione , di averne compreso le nalit , le alternative , e di accettarne i rischi . 
i conrm that i have been informed of the benets i can expect from the treatment of my condition , of the possible complications ( including invalidating and / or life - threatening complications ) due to known and unknown causes , which are possible but not preventable , related to my state of ill health and to the materials used , of the predictable discomfort and the risks that may originate from the performance of the examination , and of the possible alternative treatments available either within or outside of the facility . aware of the general and specic risks inherent to the technique and the methods used , which have been clearly and understandably explained to me , and of the possible complications deriving from the adopted treatments and aware that during the course of the therapeutic procedure unforeseen situations may arise which require different procedures from those contemplated , i accept as of now any change to the agreed treatment or method of delivering the treatment , should the need arise and should my psychologicalphysical condition prevent me from expressing additional consent . finally , i am well aware that no assurance or absolute guarantee has been given to me regarding the desired results of the diagnostic / therapeutic interventional procedure . i have been given the opportunity to ask questions which have been answered in a complete and satisfactory manner . the following person / s were present at the interview i conrm that i have read and fully understood the above . date the radiologist patients signature ( or legal guardian ) for women of child - bearing age : i hereby state that i am not pregnant ( signature ) fig . 
on this subject , much still needs to be done if in europe > 50% of patients state that they are dissatised with the way consent was obtained [ 33 ] and if patients undergoing interventional procedures tend to underestimate the risks and overestimate the benets , with their knowledge of risks improving only after having received appropriate information [ 34 ]  . 
even though the information should be provided by both the referring physician and the radiologist , it is the duty of the radiologist performing the procedure to provide specic information and obtain the patients signed consent to be attached to the medical record . 
anche se linformazione dovrebbe essere data sia dal medico proponente lesame che dal radiologo , spetta a questultimo , esecutore della procedura , la specica informazione e la raccolta del consenso con rma del paziente , da allegare alla cartella clinica . 
 where the radiologist foresees a possibility of having to change the initial aims during the examination , it would be best to inform the patient of this possibility beforehand and obtain his / her consent before the examination . 
if the procedure has only recently been adopted in clinical practice , the procedure should be conducted under the supervision of an adequately experienced colleague or , alternatively , the consent form should indicate that experience with the new technique is still limited [ 29 ]  . with regard to technical aspects of the procedure , it is the radiologists duty to ensure the availability of all equipment necessary for performing the procedure ( instruments , material , medications ) and to check , before starting the procedure , the availability of specialists able to deal with possible complications beyond the radiologists specic scope of practice . as in us law , italian law does not require the clinical success of every procedure but is does require that the radiologists conduct is reasonable and in compliance with the guidelines . 
it is best to document each step of the procedure with images and include in the medical record or radiology report a detailed description of the technique , an indication of the material and medications used and an assessment of the patients clinical status . 
any technical problem due to instrumentation or difculties due to poor patient cooperation should be noted . the postprocedural phase is particularly delicate : even after the patient has been transferred to the ward , the interventional radiologist cannot ignore the subsequent clinical course as regards aspects pertaining to the procedure ; this includes checking the site of access of needles or instruments and verifying the patients clinical stability , especially as regards renal function and possible late reactions to the contrast medium . effetti iatrogeni anche letali ( seppure eccezionali ) e della possibilit di eventuali azioni di correzione . 
nel caso che il radiologo preveda la possibilit di cambiare , nel corso dellesame , gli obiettivi iniziali , sarebbe bene provvedere ad informare preventivamente su questa possibilit il paziente , ottenendone il consenso prima dellesame . 
nel caso di una procedura da poco entrata nella pratica clinica , opportuno ricorrere alla supervisione di un collega con adeguata pratica o , in alternativa , indicare nel consenso informato che lesperienza con la nuova metodica ancora limitata [ 29 ]  . per quanto riguarda gli aspetti tecnici della procedura compito del radiologo accertarsi della presenza e disponibilit di tutto quanto e necessario alla esecuzione della prestazione ( strumentazioni , materiale , farmaci ) cos come egli deve vericare prima di iniziare lintervento la disponibilit degli specialisti per eventuali complicazioni che eccedano la propria competenza specica . nella giurisprudenza italiana , come in quella anglosassone , non richiesto il successo clinico di ogni procedura , ma si valuta se la condotta del radiologo stata ragionevole e conforme alle linee - guida . 
buona regola documentare iconogracamente ogni fase della procedura e riportare sulla cartella clinica o sul referto radiologico la puntuale descrizione della manovra , lindicazione dei materiali e dei farmaci utilizzati e la valutazione dello stato clinico del paziente . 
bene annotare sempre eventuali problemi tecnici o dello strumentario o difcolt derivanti dalla scarsa collaborazione del paziente . una fase particolarmente delicata quella post - intervento : anche dopo il trasferimento del paziente al reparto di degenza , il radiologo interventista non pu ignorare la successiva evoluzione clinica del paziente per gli aspetti inerenti la sua prestazione : tra laltro , il controllo della sede di introduzione degli aghi o degli strumenti e la verica della stabilit clinica del paziente , con particolare riferimento alla funzionalit renale per le possibili reazioni tardive al mezzo di contrasto . conclusioni conclusions the radiologists role has dramatically changed in recent years . 
radiologists no longer only perform diagnostic tests but often carry out therapeutic procedures either alone or as part of a teainterventional radiology is similar to surgical specialties in which the need to guarantee accountability has led to the introduction , in the more advanced countries , of recertication schemes to validate the physicians tness il ruolo del radiologo profondamente cambiato negli ultimi anni . 
la radiologia interventistica afne alle specialit chirurgiche nelle quali lesigenza di garantire la responsabilit professionale ( accountability ) ha portato nei paesi pi progrediti allintroduzione di procedure di certicazione , attraverso le quali viene vericata la capacit del medico di svolgere la sua specica attivit ad un livello compatibile con gli sviluppi 516 radiol med ( 2013 ) 118 : 504517 to practice at a level compatible with recent developments in the discipline . 
 this process is underway in all english - speaking countries , although with different characteristics from country to country [ 39 , 40 ] , and it is likely that similar schemes will be introduced in italy as well [ 12 ]  . 
nonetheless , interventional radiologists must , as of now , start to guarantee maximum professionalism and compliance with good practices if they want to limit their risk of incurring litigation . 
nei paesi anglosassoni tale processo ormai in atto un po ovunque , anche se con caratteristiche diverse da paese a paese [ 39 , 40 ] ed probabile che procedure analoghe siano introdotte prima o poi anche nel nostro paese [ 12 ]  . 
in ogni caso , il radiologo interventista deve , n da ora , garantire il massimo livello di professionalit e di adesione alle buone pratiche , se vuole limitare il rischio di andare incontro a contenzioso . 
gandini1 1istituto di radiologia diagnostica ed interventistica , universit di torino , aou san giovanni battista di torino , sede molinette , via genova 3 , 10126 torino , italy 2divisione universitaria di ematologia , aou san giovanni battista , torino , italy 3s.s.c.v.d. 
women aged 30 years were screened with clinical breast examination , ultrasound ( us ) and , if necessary , mammography ; women > 30 years had clinical breast examination , us and mammography . 
il presente uno studio retrospettivo condotto su 54 donne che tra il 1980 e il 2010 sono state sottoposte a radioterapia per lh ( et media 36 , 6 anni )  . 
 le pazienti con meno di 30 anni hanno effettuato visita clinica , ecograa e mammograa quando indicata , quelle con pi di 30 anni visita clinica , ecograa e mammograa . 
considerando giovane et e densit mammaria , le pazienti con meno di 30 anni dovrebbero essere sottoposte ad ecograa e rm , mentre quelle con pi 402 radiol med ( 2013 ) 118 : 401414 keywords hodgkins lymphoma radiotherapy breast cancer di 30 anni a mammograa ed ecograa , con eventuale rm , quando necessaria . parole chiave linfoma di hodgkin radioterapia carcinoma mammario introduction introduzione several studies have reported that the development of secondary malignancies is the main cause of morbidity and mortality in survivors of hodgkins lymphoma ( hl )  . 
the most frequent secondary malignancy among women is breast cancer ( bc ) , and the risk of developing this neoplasm is closely related to the irradiation of supradiaphragmatic lymph nodes [ 15 ]  . 
compared with the general population , the relative risk ( rr ) at 30 years 6to 17 - fold greater , reaching 75to 136 - fold in women treated at 16 years [ 1 , 68 ]  . 
 the reported variability in the rr of developing breast cancer depends on the heterogeneity of study populations in terms of proportion of irradiated women , age at the time of radiotherapy , radiation volume and dose , adopted chemotherapy protocols , and duration and completeness of clinical follow - up [ 916 ]  . 
the extent of risk appears to decrease with increasing age at the time of radiotherapy and remains statistically signicant up to the age of 30 years , thereby suggesting that the age group between puberty and 30 years is the most vulnerable to radiation - induced carcinogenesis [ 1720 ]  . 
the introduction of chemotherapeutic agents in treatment protocols has made it possible to decrease radiation volumes and doses , thus reducing the risk of radiation - induced breast cancer [ 1215 , 17 , 2326 ]  . 
 the purposes of our study were to : ( 1 ) estimate the rr of breast cancer in women who underwent radiotherapy for hl , and ( 2 ) study the features of the diagnosed breast cancers on conventional imaging [ mammography and ultrasound ( us ) ]  . 
 materials and methods population numerosi studi hanno evidenziato come nei pazienti sopravvissuti al linfoma di hodgkin ( lh ) lo sviluppo di neoplasie secondarie maligne rappresenti la principale causa di morbilit e mortalit . 
tra le donne , la neoplasia secondaria in assoluto pi frequente il carcinoma della mammella e il rischio di sviluppare tale neoplasia strettamente correlato allirradiazione delle stazioni linfonodali sovradiaframmatiche [ 15 ]  . 
rispetto alla popolazione generale , il rischio relativo di sviluppare una neoplasia mammaria in donne radiotrattate per lh prima dei 30 anni 617 volte superiore , no ad arrivare a 75136 volte superiore in donne trattate prima dei 16 anni [ 1 , 68 ]  . 
 la variabilit del rischio relativo di sviluppare una neoplasia mammaria riportata in letteratura dipende dalleterogeneit presente nei campioni di studio in termini di percentuali di donne irradiate , et in corrispondenza del trattamento radioterapico , volumi e dosaggi di irradiazione , protocolli chemioterapici adottati , durata e completezza del follow - up clinico applicato [ 916 ]  . 
lentit del rischio pare diminuire con laumento dellet al momento dellirradiazione , rimanendo statisticamente signicativo no ai 30 anni , delineando dunque la fascia di et compresa tra la pubert e i 30 anni come quella in assoluto pi suscettibile alla cancerogenesi radioindotta [ 1720 ]  . 
 lintroduzione dei farmaci chemioterapici nei protocolli di trattamento ha consentito la riduzione dei volumi da irradiare e la somministrazione di minori dosi di radiazioni , determinando una riduzione del rischio [ 1215 , 17 , 2326 ]  . 
 gli obiettivi del nostro lavoro sono stati : ( 1 ) valutare il rischio relativo di sviluppare neoplasie mammarie nelle donne radiotrattate per lh ; ( 2 ) valutare la presentazione allimaging convenzionale ( mammograa ed ecograa ) dei tumori mammari diagnosticati . 
of these , 11 patients had not undergone radiotherapy , whereas six had completed radiotherapy < 3 years before this study was materiali e metodi popolazione abbiamo condotto uno studio retrospettivo su 107 donne che tra gennaio 1980 e giugno 2010 hanno ricevuto una radiol med ( 2013 ) 118 : 401414 initiated . 
of the 90 remaining women , 54 had undergone radiotherapy and were referred to our radiology department for early follow - up breast imaging after being adequately informed by the haemato - oncologist of the increased risk of breast cancer . the 54 women comprising the study group ( mean age , 36.6 years ; range , 1980 years ) had a mean age of 26.1 years ( range , 871 years ) at the time of hl diagnosis . 
in 85% of patients ( 46 / 54 ) , hl had been diagnosed at an initial stage ( iii ) , and in the remaining 15% ( 8 / 54 ) at an advanced stage ( iiiiv ) ; eight patients has a mediastinal mass at presentation . 
 mean interval between radiation therapy and rst follow - up imaging was 5.5 ( range , 118 ) years . radiotherapy consisted of involved - eld radiation therapy ( 72% , 39 / 54 ) , mantle irradiation ( 18% , 10 / 54 ) and subtotal nodal irradiation % ( stni , used from 1982 to 1993 only ) ( 10% , 5 / 54 )  . 
in 53 / 54 patients , radiotherapy ( mean dose , 31.8 gy ; range , 2044 gy ) was combined with chemotherapy ; one patient only was treated with radiation therapy alone . 
 chemotherapy regimens followed the abvd ( adriamycin , bleomycin , vinblastine and dacarbazine ) protocol in 43 / 53 cases , mopp ( mechlorethamine , vincristine , procarbazine and prednisone ) in 5 / 53 cases , abvd + mopp in 1 / 53 cases , beacopp ( bleomycin , etoposide , adriamycin , cyclophosphamide , vincristine , procarbazine and prednisone ) in 1 / 53 cases , abv + copp in 2 / 53 cases , and eve ( epirubicin , vinblastine and etoposide ) in 1 / 53 cases ( table 1 )  . surveillance protocol based on age , the 54 patients underwent individualised breast follow - up : patients 30 years of age underwent clinical and us examination , supplemented with mammography in the case of diagnostic suspicion ; patients > 30 years of age underwent clinical and us examination and bilateral mammography in the two standard projections ( craniocaudal and mediolateral oblique ) supplemented , whenever needed , by magnication views . as suggested [ 2731 ] , from september 2009 patients < 30 years of age underwent clinical examination , magnetic resonance ( mr ) imaging and us . 
during the study period , 35 women underwent yearly mammography and us examinations ; 11 underwent 6 - monthly us and yearly mammographic examinations , whereas eight underwent yearly us , supplemented in three cases with contrast - enhanced breast mr imaging . diagnosi di lh e relativo follow - up clinico e terapeutico . 
 tra queste , 11 pazienti non sono state sottoposte a trattamento radioterapico mentre 6 , al momento della realizzazione del nostro studio , avevano concluso il trattamento radiante da meno di 3 anni . 
tra le 90 donne rimanenti , 54 dopo essere state sottoposte a trattamento radioterapico e adeguatamente informate dagli specialisti oncoematologi riguardo allaumentato rischio di sviluppare una neoplasia mammaria , sono state inviate presso il nostro servizio di radiologia per intraprendere precocemente un follow - up senologico . le 54 donne inserite nello studio con unet media di 36 , 6 anni ( range : 1980 anni ) presentavano unet media alla diagnosi di lh di 26 , 1 anni ( range : 871 anni )  . 
nell85% delle pazienti ( 46 / 54 ) il lh era stato diagnosticato in stadio iniziale ( iii ) , nel rimanente 15% ( 8 / 54 ) in stadio avanzato ( iii - iv ) ; 8 casi presentavano allesordio bulky mediastinico . 
lintervallo medio intercorso tra la terapia radiante e lesecuzione del primo controllo senologico mediante tecniche di imaging stato di 5 , 5 anni ( range : 118 anni )  . il trattamento radioterapico stato nella maggior parte dei casi involved elds ( 72% , 39 / 54 ) e in una minor parte dei casi mantellina ( 18% , 10 / 54 ) e sub - total nodal irradiation ( 10% , 5 / 54 ) ( stni , utilizzata negli anni compresi tra il 1982 e il 1993 , successivamente non pi utilizzata )  . 
in 53 / 54 pazienti , il trattamento radioterapico ( dose media 31 , 8 gy , range : 2044 gy ) stato combinato con chemioterapia , mentre un caso stato trattato esclusivamente con radioterapia . 
mammographic , us and mr images were read by two breast radiologists in consensus . for patients undergoing ne - needle aspiration cytology ( fnac ) , ndings were classied into ve categories in agreement with the fourth edition of the european guidelines : c1 = inadequate for diagnosis , c2 = benign epithelial cells , c3 = atypia ( probably benign ) , c4 = suspicious of malignancy , c5 = malignant . 
in the case of core biopsy / histology , ndings were classied into ve categories : b1 = normal breast tissue , b2 = benign , b3 = benign but of uncertain malignant potential , b4 = suspicious of malignancy , b5 = malignant [ 33 ]  . 
all patients provided their informed consent before undergoing needle biopsy . data analysis we calculated the number of neoplasms developed in our patient population series and measured the incidence rate based on the number of cases per person - year of risk . 
rr of breast cancer in women treated with radiotherapy for hl was indicated as the ratio between observed incidence rate and the rate of invasive breast carcinoma in the general population of the city of turin , recorded for the years 2004 2006 by the referral centre for cancer epidemiology and prevention in the piedmont region ( 171.3 / 100 , 000 ) [ 34 ]  . 
 mammographic and us features of the neoplasms detected were also analysed . results neoplasms come suggerito da recenti studi [ 2731 ] , da settembre 2009 le pazienti di et inferiore a 30 anni sono state sottoposte a visita clinica , risonanza magnetica ed esame ecograco . 
durante il periodo di studio , 35 donne sono state sottoposte a mammograa ed ecograa annuali ; 11 donne hanno effettuato ecograa semestrale e mammograa annuale , mentre 8 donne hanno eseguito ecograa annuale , in 3 casi completata con risonanza magnetica mammaria con mezzo di contrasto . interpretazione dei reperti stata valutata la densit mammaria allindagine mammograca in accordo con la classicazione breast imaging reporting and data system ( bi - rads ) dellamerican college of radiology che suddivide le mammelle in quattro categorie : d1 = adiposa , d2 = broghiandolare , d3 = moderatamente densa , d4 = prevalentemente densa [ 32 ]  . 
la metodologia di codica dei reperti mammograci utilizzata stata conforme alla classicazione proposta dallamerican college of radiology , sistema bi - rads [ 32 ]  . analogamente , anche i reperti ecograci e di risonanza magnetica sono stati classicati facendo riferimento alle categorie suggerite dal bi - rads atlas [ 32 ]  . 
nelle pazienti sottoposte ad esame citologico su agoaspirato i reperti sono stati suddivisi in 5 categorie in accordo alla quarta edizione delle linee guida europee : c1 = inadeguato , c2 = negativo , c3 = dubbio ( lesione probabilmente benigna ) , c4 = sospetto di malignit , c5 = positivo [ 33 ]  . in caso di esame microistologico , i reperti sono stati classicati in 5 categorie : b1 = normale , b2 = benigno , b3 = lesione di incerto signicato , b4 = sospetto di malignit , b5 = positivo [ 33 ]  . 
tutte le pazienti , prima di essere sottoposte a prelievo agobioptico , hanno rmato un consenso informato . analisi dei dati during the observation period , seven invasive breast cancers were detected ( 6 / 54 , 11.1% ) , ve of which were unilateral and one bilateral metachronous ( rst onset at 14 years and second at 25 years after radiotherapy , cases 1 and 2 in tables 24 )  . 
of the six women who developed a secondary malignancy , two had a family history of breast carcinoma ( cases 1 , 2 and 5 in tables 24 )  . 
considering the ration of 171.3 / 100 , 000 cases per person - year as a reference incidence rate for invasive breast carcinoma in the general population of turin , our experience shows that women who received radiotherapy for hl had a 6.2 - fold higher risk stato calcolato il numero di neoplasie insorte nella popolazione in esame ed stata effettuata la valutazione del tasso di incidenza osservato , tenendo conto del numero di casi / annipersona di rischio . 
il rischio relativo di sviluppare una neoplasia mammaria nelle donne radiotrattate per lh stato espresso come rapporto tra il tasso di incidenza osservato e tasso di incidenza di carcinoma invasivo della mammella nella popolazione generale residente a torino , registrato negli anni 20042006 dal centro di riferimento per lepidemiologia e la prevenzione oncologica in piemonte ( 171 , 3 / 100000 ) [ 34 ]  . 
 age at hl diagnosis stage at hl diagnosis age at bc diagnosis rt dose ( gy ) latency from rt to bc radiol med ( 2013 ) 118 : 401414 * bilateral metachronous cancer abvd , adriamycin , bleomycin , vinblastine , dacarbazine ; bc , breast cancer ; eve , epirubicin , vinblastine , etoposide ; hl , hodgkins lymphoma ; if , involved elds ; mopp , mechlorethamine vincristine procarbazine prednisone ; rt , radiotherapy ; stni , subtotal nodal irradiation tabella 2 caratteristiche cliniche dei 7 casi di neoplasia mammaria caso no . 
 risultati the mean age at diagnosis of breast cancer was 42.4 ( range , 2855 ) years , and mean interval between completion of radiation therapy and disease onset was 15.1 ( range , 326 ) years . 
mean radiation dose to the six women who developed breast cancer was 37.6 ( range , 36 - 40 ) gy ( table 2 ) ; the other women had a mean dose of 31.3 ( range , 2044 ) surgery was performed on ve cases of breast cancer ( quadrantectomy in four , mastectomy in one ) , complemented by hormone therapy in three cases and by radiotherapy in one case . 
one neoplasm was treated with excisional biopsy followed by hormone therapy , and one case was treated with chemotherapy alone ( table 4 )  . histologically , there were ve ductal inltrating carcinomas , one inltrating lobular carcinoma , and one invasive mucinous carcinoma ; six cases were classied as stage t1 and one as stage t4 ( carcinomatous mastitis )  . 
histological nuclear grade of the inltrating tumours according to the elstonellis system was intermediate in four cases ( g2 ) , and high in three ( g3 ) [ 35 ]  . 
analysis of hormone receptor status indicated sensitivity to estrogens and progesterone in neoplasie durante il periodo di osservazione , sono stati rilevati 7 carcinomi invasivi della mammella ( 6 / 54 , 11 , 1% ) di cui 5 monolaterali e 1 bilaterale metacrono ( prima insorgenza dopo 14 anni e seconda insorgenza dopo 25 anni dal radiotrattamento , casi 1 e 2 nelle tabelle 24 )  . 
considerando come riferimento un tasso di incidenza di carcinoma invasivo della mammella pari a 171 , 3 / 100000 persone / anno registrato nella popolazione generale residente a torino , la nostra esperienza dimostra come le donne radiotrattate per lh presentino un rischio 6 , 2 volte superiore rispetto alla popolazione generale di sviluppare una neoplasia mammaria . 
 breast density pathology ptnm grade * bilateral metachronous cancer idc , invasive ductal carcinoma ; ilc , invasive lobular carcinoma tabella 3 densit mammograca e analisi istopatologica dei 7 casi di neoplasia mammaria caso no . 
in the course of the study , breast imaging was complemented by us - guided cytology and / or microhistology in three women , and the results were negative for malignancy . in addition , eight patients developed iatrogenic hypothyroidism during the observation period , which was related to radiation exposure in the mediastinal region ; one patient underwent subtotal thyroidectomy owing to the presence of struma , and two patients underwent total thyroidectomy ( as a prophylactic measure in one case with trabecular adenoma and due to papillary carcinoma in the other )  . 
 radiological features of neoplasms mammographic breast density was d3 in 23 / 46 cases , d2 in 13 / 46 cases and d1 in 10 / 46 cases ; in the eight cases studied by us only , breast structure was hyperechoic with predominant glandular component , as conrmed in the three studied with mr imaging also . 
la dose media di radiazioni somministrata alle 6 donne che hanno sviluppato la neoplasia stata di 37 , 6 gy ( range : 3640 gy ) ( tabella 2 ) , mentre nelle altre donne la media stata di 31 , 3 gy ( range : 2044 gy )  . il trattamento chirurgico stato riservato a 5 neoplasie mammarie ( quadrantectomia in 4 casi , mastectomia in un caso ) , integrato in 3 casi da ormonoterapia e in un solo caso da radioterapia . 
una neoplasia stata sottoposta a biopsia chirurgica escissionale seguita da ormonoterapia e in un caso si optato per il solo trattamento chemioterapico ( tabella 4 )  . dal punto di vista istologico , le 7 neoplasie riscontrate corrispondevano in 5 casi a carcinomi duttali inltranti , in un caso a carcinoma lobulare inltrante e in un caso a carcinoma mucinoso invasivo ; 6 neoplasie erano in stadio t1 e una allo stadio t4 ( mastite carcinomatosa )  . 
lanalisi dello status recettoriale ha evidenziato in tutti i casi sensibilit a estrogeni e progesterone e in un solo caso la positivit a c - erbb2 ( tabelle 3 e 4 )  . 
 nel corso del nostro studio , a completamento dellindagine senologica eseguita mediante tecniche di imaging , altre 3 donne sono state sottoposte ad esame citologico e / o microistologico ecoguidato con esito negativo per patologia table 4 prognostic factors and treatment of seven breast cancer cases case receptor status bc treatment 408 er + pr + er + pr + er + pr + ki67 18% c - erbb2 + er + pr + c - erbb2 er + ki67 23% c - erbb2 er + ki67 16% c - erbb2 er + pr + ki67 25% c - erbb2 chemotherapy quadrantectomy hormone therapy quadrantectomy radiotherapy hormone therapy quadrantectomy chemotherapy hormone therapy quadrantectomy hormone therapy chemotherapy mastectomy * bilateral metachronous cancer er + , oestrogen receptor positive ; pr + , progesterone receptor positive tabella 4 fattori prognostici e protocollo terapeutico dei 7 casi di neoplasia mammaria caso status recettoriale terapia tumore mammario chemioterapia quadrantectomia chemioterapia ormonoterapia quadrantectomia quadrantectomia ormonoterapia quadrantectomia radioterapia ormonoterapia er + pr + er + pr + er + pr + ki67 18% c - erbb2 + er + pr + c - erbb2 er + pr + ki67 23% c - erbb2 er + pr + ki67 16% c - erbb2 er + pr + ki67 25% c - erbb2 * tumore bilaterale metacrono er + , positivit per i recettori per gli estrogeni ; pr + , positivit per i recettori per i progestinici chemioterapia mastectomia ormonoterapia radiol med ( 2013 ) 118 : 401414 neoplastica . 
collateralmente , durante il periodo di osservazione della popolazione in esame , 8 pazienti hanno sviluppato ipotiroidismo iatrogeno riconducibile allesposizione al trattamento radioterapico ricevuto in sede mediastinica ; una paziente stata sottoposta a tiroidectomia subtotale per la presenza di struma e 2 pazienti sono state sottoposte a tiroidectomia totale ( in un caso prolattica per la presenza di adenoma trabecolare e in un caso per un carcinoma papillare )  . 
 caratteristiche radiologiche delle neoplasie la densit mammaria rilevata allindagine mammograca risultata d3 in 23 / 46 casi , d2 in 13 / 46 casi e d1 in 10 / 46 casi ; negli 8 casi controllati esclusivamente con esame ecograco la struttura ghiandolare era di tipo iperecogeno con componente ghiandolare largamente prevalente sul tessuto adiposo , come confermato nei 3 casi sottoposti anche a risonanza magnetica . 
al controllo ecograco , le 6 opacit corrispondevano a formazioni nodulari ipoecogene disomogenee a margini irregolari con cono dombra posteriore , mentre il cluster di microcalcicazioni non era visibile ecogracamente . discussione analogamente agli studi riportati in letteratura [ 3943 ] , anche la nostra esperienza ha dimostrato come le donne radiotrattate per lh presentino un aumentato rischio di sviluppare il carcinoma della mammella rispetto alla popolazione generale ( rischio relativo 6 , 2 ) , sebbene tale dato debba essere valutato tenendo conto delle rilevanti limitazioni in termini statistici che contraddistinguono il nostro campione di studio . let al momento del trattamento radioterapico pare costituisca la variabile pi importante nella determinazione del rischio [ 117 ]  . 
a spiculated mass in the upper outer quadrant of the right breast was found at screening mammogram ( a , craniocaudal view ; b mediolateral oblique view ; c magnication view )  . 
allesame mammograco , stata rilevata unopacit a margini spiculati in corrispondenza del quadrante supero - esterno destro ( a proiezione cranio - caudale ; b proiezione obliqua medio - laterale ; c ingrandimento mirato )  . 
however , this nding should be interpreted taking into account the major statistical limitations that characterise our series . age at the time of radiotherapy seems to represent the most signicant variable in risk determination [ 117 ]  . 
the six patients who developed breast cancer had all undergone radiotherapy before the age of 40 years and four of them before the age of 30 . diotrattata per lh in sede mediastinica e in giovane et , sufciente ricordare che , in base agli studi presenti in letteratura , una percentuale compresa tra il 12% e il 20% di queste pazienti svilupper un tumore mammario entro i 45 anni , percentuale correlabile allincidenza cumulativa di neoplasia mammaria compresa tra l1% e il 5% a 30 anni e tra il 10% e il 19% a 40 anni delle donne portatrici della mutazione del gene brca [ 1 , 3638 ]  . 
 sia let media alla diagnosi di neoplasia mammaria che lintervallo medio intercorso tra il completamento del trattamento radioterapico e lo sviluppo del carcinoma della mammella individuati nel nostro studio sono in accordo con quanto riportato in letteratura [ 9 , 10 , 19 ] , quindi signicativamente pi bassa rispetto allet media di insorgenza di 57 anni riportata per la popolazione generale [ 10 ]  . 
 nel nostro campione di studio , le donne che hanno sviluppato una neoplasia mammaria avevano ricevuto una dose media di radiazioni pi elevata rispetto alle altre pazienti ( 37 , 6 contro 31 , 3 gy ) e due di esse avevano ricevuto radiol med ( 2013 ) 118 : 401414 410 fig . 
 ( a proiezione obliqua medio - laterale ; b proiezione cranio - caudale ; c ingrandimento mirato )  . eleven per cent of women undergoing breast surveillance at our centre developed breast cancer . 
to appreciate the extent of breast cancer risk among women receiving mediastinal radiation for hl at a young age , it is sufcient to remember that , according to published studies , 12%20% of these patients will develop breast cancer before the age of 45 years , as against a cumulative incidence of breast cancer of 1%5% at 30 years of age and of 10%19% at 40 years among women with the brca mutation [ 1 , 3638 ]  . 
 both mean age at diagnosis and mean interval between completion of radiotherapy and onset of breast cancer in our study are in line with data reported in the literature [ 9 , 10 , 19 ] , with mean age at onset ( 57 years ) being signicantly lower than that reported for the general population [ 10 ]  . 
anche questo aspetto correlabile alle evidenze presenti in letteratura che suggeriscono un aumento lineare del rischio di sviluppare la neoplasia mammaria in rapporto allaumento della dose di radiazioni somministrata alla paziente [ 6 , 22 , 41 ]  . 
this nding is also in line with evidence reported in the literature , suggesting a linear increase in breast cancer risk with increasing radiation dose [ 6 , 22 , 41 ]  . 
according to numerous studies , 87%100% of cases of breast cancer in hl survivors are detectable on mammography , thanks to the high prevalence of microcalcications ( 62%72% ) [ 6 , 27 , 44 ] ; however , in our experience , neoplastic lesions appeared as opacities in 6 / 7 cases and as a microcalcication cluster in one . considering that young age and high breast density are common features among women undergoing breast surveillance after radiotherapy for hl , the role of mr imaging will become increasingly crucial [ 2831 , 38 , 4551 ]  . 
it has high sensitivity ( 80%100% ) for detecting inltrating tumours , but its specicity is lower ( 87%95% ) and , compared with mammography , has lower sensitivity for detecting ductal carcinoma in situ [ 27 , 45 , 46 , 49 , 50 ]  . 
 to date , however , no denite conclusion has been reached regarding the most effective modality for breast surveillance in hl survivors or the impact that an aggressive screening strategy might have in terms of decreasing mortality due to secondary breast cancer . 
recommended that breast surveillance in women irradiated for hl before the age of 30 should be initiated 8 years after completion of treatment regardless of patient age , in that 8 years was the shortest reported interval between irradiation and development of secondary malignancy [ 19 ]  . 
suggested performing a rst mammogram 5 years after radiotherapy , followed by mammogram every 2 years , with annual mammography starting 10 years after completion of radiotherapy [ 52 ]  . 
from the royal college of radiologists reported that women who had received supradiaphragmatic irradiation for hl before 17 years of age should initiate breast surveillance at age 25 [ 27 ]  . 
women treated between 17 and 35 years of age were to begin screening 8 years after completion of radiotherapy , and women between 25 and 29 years of age were to undergo annual mr imaging or , if contraindicated , us ; in this age bracket , mammography was not recommended [ 27 ]  . 
 in 2008 , the childrens oncology group ( cog ) updated criteria introduced in 2003 for the long - term follow - up for survivors of childhood , adolescent , and young adult cancer , which recommended that for women who had received medium to high radiation doses to the chest ( > 20 gy ) , surveillance with annual mammograms should start at 25 years of age or , regardless of age , 8 years after completion of radiotherapy [ 53 ] ; screening included , as suggested by the american cancer society ( acs ) and by the united senologica , il ruolo della risonanza magnetica nei prossimi anni tuttavia destinato a diventare sempre pi importante [ 2831 , 38 , 4551 ]  . 
la risonanza magnetica , ormai universalmente accettata come principale tecnica di screening nelle giovani donne geneticamente predisposte al rischio di sviluppare neoplasie mammarie ( pazienti portatrici della mutazione del gene brca ) , una metodica molto sensibile ( 80%100% ) nel rilevare tumori inltranti , accompagnata per da una minor specicit ( 87%95% ) , e rispetto alla mammograa presenta minor sensibilit nellindividuare carcinomi duttali in situ [ 27 , 45 , 46 , 49 , 50 ]  . 
 ad oggi , tuttavia , non esistono dati certi su quale possa essere la migliore strategia di sorveglianza senologica da applicare a donne radiotrattate per lh e soprattutto sullimpatto che unaggressiva strategia di screening possa avere in termini di riduzione della mortalit da neoplasia mammaria secondaria . 
 [ 19 ] raccomandavano che la sorveglianza senologica in donne radiotrattate per lh prima dei 30 anni iniziasse a partire da 8 anni dalla ne del trattamento , indipendentemente dallet della paziente , in quanto 8 anni rappresentavano lintervallo osservato pi breve tra lirradiazione e lo sviluppo del tumore secondario [ 19 ]  . 
 [ 52 ] consigliavano una prima mammograa 5 anni dopo il radiotrattamento , quindi una mammograa ogni 2 anni e dopo 10 anni lesecuzione annuale dellesame [ 52 ]  . 
 [ 27 ] del royal college of radiologists ritenevano appropriato iniziare la sorveglianza , in donne che avessero ricevuto una radioterapia sovradiaframmatica per lh prima dei 17 anni , a partire dai 25 anni [ 27 ]  . 
tra i 25 e i 29 anni di et le donne dovevano essere sottoposte a risonanza magnetica annuale , o nel caso di controindicazioni allesecuzione della risonanza magnetica , a esame ecograco ; in questa fascia di et la mammograa non era raccomandata . 
 nel 2008 il childrens oncology group ( cog ) ha aggiornato i criteri introdotti nel 2003 per il long - term followup for survivors of childhood , adolescent , and young adult cancer che prevedevano per le donne esposte a dosi medioalte di radiazioni in sede toracica ( dosi > 20 gy ) linizio della sorveglianza a 25 anni di et , o indipendentemente dallet , a partire da 8 anni dal completamento del trattamento radioterapico tramite screening mammograco annuale [ 53 ] , includendo , analogamente a quanto suggerito anche dallamerican cancer society e dallo united kingdom department of health [ 29 , 30 ] , lutilizzo della risonanza magnetica in associazione allesecuzione della mammograa annuale [ 28 ]  . 
nel nostro studio lintervallo medio intercorso tra il completamento delle cure radioterapiche per il lh e lesecuzione del primo controllo senologico mediante tecniche di imaging stato di 5 , 5 anni , inferiore dunque anche ai tempi indicati nelle principali linee guida internazionali . 
 412 radiol med ( 2013 ) 118 : 401414 kingdom department of health [ 29 , 30 ] , the use of mr imaging combined with yearly mammograms [ 28 ]  . 
in our study , the mean interval between completion of radiotherapy for hl and the rst breast imaging study was 5.5 years , shorter than the intervals recommended in the leading international guidelines . 
 furthermore , an interesting nding from the literature [ 44 , 54 ] is that women who have undergone radiotherapy for hl apparently tend to underestimate the risk of developing a secondary breast cancer , which may lead to reduced compliance with screening recommendations . 
therefore , we believe it is extremely important that the haemato - oncologists and radiologists cooperate , as they do at our institution , in order to provide all patients undergoing radiotherapy for hl and especially younger women with all the information they need to understand their increased risk of developing breast cancer . the main limitations of our study are its retrospective nature and the small and heterogeneous patient population ( only 18 / 54 patients were < 20 years of age at the time of hl diagnosis , and over the 30 - year - long observation period , patients underwent different chemoand radiotherapy protocols ) ; in addition , mr imaging was introduced at the end of 2009 and used in three cases only to complement conventional breast imaging . conclusions treatment protocols for hl that include irradiation of supradiaphragmatic lymph nodes have helped to achieve high rates of disease - free survival , although the radiation exposure of breast tissue , in particular in young women , has signicantly increased the risk of developing breast cancer compared with the general population . 
our study conrms that patients treated with radiotherapy for hl have a higher rr of developing breast carcinoma and that they need , as a consequence , to undergo adequate breast surveillance protocols . 
therefore , although all breast cancers in our series were detected at mammography , in agreement with the acs and with other recent important studies , we suggest the use of mr imaging in patients 30 years of age and who have undergone radiation therapy for hl and as a complementary method to us / mammography in patients > 30 , as suggested for women with brca mutations . un dato interessante che emerge inoltre dalla letteratura [ 44 , 54 ] , riguarda lapparente tendenza da parte delle donne radiotrattate per lh a sottovalutare il rischio di sviluppare una neoplasia mammaria secondaria , atteggiamento che pu determinare una ridotta aderenza a programmi di screening . 
in tal senso , riteniamo dunque molto importante la collaborazione sviluppatasi nella nostra esperienza tra specialisti oncoematologi e radiologi il cui obiettivo quello di fornire a tutte le pazienti radiotrattate per lh , e in modo particolare alle donne pi giovani , le informazioni necessarie a comprendere lelevato rischio di sviluppare una neoplasia mammaria che le contraddistingue . la natura retrospettiva , nonch una casistica ridotta in termini numerici ed eterogenea riguardo ad alcuni aspetti ( in soli 18 / 54 casi let alla diagnosi di lh risultata essere inferiore a 20 anni e nellampio arco di tempo considerato , 30 anni , le pazienti sono state sottoposte a diversi protocolli di trattamento chemio - radioterapico ) rappresentano i principali limiti del nostro studio , unitamente al fatto che solo a partire dalla ne del 2009 e in soli 3 casi , stato introdotto lutilizzo della risonanza magnetica a completamento dellindagine senologica eseguita mediante limaging convenzionale . conclusioni i protocolli di trattamento per il lh comprendenti lirradiazione delle stazioni linfonodali sovradiaframmatiche hanno contribuito a determinare elevati tassi di sopravvivenza liberi da malattia , ma lesposizione del tessuto mammario alle radiazioni , soprattutto in giovani donne , ha signicativamente aumentato il rischio , rispetto alla popolazione generale , di sviluppare una neoplasia mammaria . 
il nostro studio conferma un aumento del rischio relativo di sviluppare il carcinoma mammario nelle pazienti radiotrattate per lh e dunque la necessit di sottoporre tale popolazione ad unadeguata sorveglianza senologica . 
interventional radiology achieved complete clinical success in 74 cases ( 85.9% ) and in particular in 95.2% of stulas , 76.5% of stenoses and 33.3% of complete bile duct transections . 
abbiamo registrato un successo clinico complessivo ( guarigione della complicanza ottenuta con le procedure interventistiche ) in 74 / 85 casi ( 85 , 9% ) : 95 , 2% nelle stole , 76 , 5% nelle stenosi e 33 , 3% nei distacchi completi . 
le procedure percutanee sono fattibili , radiol med ( 2013 ) 118 : 386400 endoscopy , which is precluded in many of these patients , and to surgery , which has higher morbidity and mortality rates . keywords interventional radiology biliary tract diseases postoperative complications efcaci e sicure nel trattamento delle complicanze precoci post - operatorie delle vie biliari ; rappresentano una valida alternativa al trattamento endoscopico , non eseguibile in molti di questi pazienti , ed alla chirurgia , gravata da tassi di morbilit e mortalit pi elevati . parole chiave radiologia interventistica patologie delle vie biliari complicanze post operatorie introduction introduzione postoperative biliary complications remain a signicant problem in the eld of hepatobiliary surgery and , more generally , in clinical practice . 
in recent years , the incidence of these lesions has steadily increased as a result of the more extensive use of laparoscopic cholecystectomy ( lc ) [ 18 ] and of complex surgical techniques such as cephalic duodenopancreatectomy ( cdp ) or extended hepatic resections ( hr ) [ 913 ]  . 
the type of biliary injury resulting from surgical procedures varies but can be classied into two main types : stenoses obstructing bile ow , and stulas with extraluminal bile leakage ( including complete transection of the bile duct )  . 
clinically , these complications manifest with pain , fever and worsening jaundice due to cholangitis or infected bilomas , to more severe conditions such as biliary peritonitis ( with possible life - threatening sepsis ) or , in the long term , secondary biliary cirrhosis . 
in addition to repeated conventional surgery , which remains , however , burdened by signicant morbidity rates , time off work and long hospital stays despite technological progress , endoscopic and / or percutaneous approaches are gaining ground , which in part overcome the problems of surgery while providing the same level of efcacy [ 1418 ]  . 
our primary goals were to evaluate technical and clinical success , complications and perioperative mortality ; our secondary goals were to analyse treatment duration and recurrence rates . materials and methods le complicanze post - operatorie degli interventi alle vie biliari rappresentano un problema molto attuale in ambito chirurgico epato - biliare e , pi in generale , in ambito clinico ; negli ultimi anni lincidenza di queste lesioni ha dimostrato , infatti , un costante incremento , da mettere in relazione sia al crescente utilizzo della colecistectomia laparoscopica ( cl ) [ 18 ] sia alla maggior diffusione di interventi chirurgici ad alto coefciente di difcolt come la duodeno - cefalo - pancreasectomia ( dcp ) o le resezioni epatiche ( re ) allargate [ 913 ]  . 
la tipologia del danno delle vie biliari conseguente a procedure chirurgiche eterogenea , ma sostanzialmente riconducibile a due lesioni fondamentali : le stenosi con ostacolo al deusso biliare e le stole con spandimento extraluminale di bile ( inclusi i distacchi completi della via biliare )  . 
 clinicamente si manifestano con dolore , febbre e ittero ingravescente secondari a colangite o a formazione di raccolte infette , no a quadri pi severi come la peritonite biliare ( che pu esitare in quadri settici , anche mortali ) oppure , nel lungo termine , la cirrosi biliare secondaria ; il loro precoce riconoscimento pertanto cruciale al ne sia di attuare tempestivamente il trattamento pi idoneo , sia di prevenirne le complicanze [ 12 ]  . 
le opzioni terapeutiche sono diverse e tuttora dibattute : accanto al tradizionale reintervento chirurgico , gravato nonostante il progresso della tecnica da unincidenza non trascurabile di morbilit e prolungata ospedalizzazione , si stanno infatti affermando i trattamenti endoscopici e / o percutanei in grado di offrire , a parit di efcacia , una riduzione di tale incidenza [ 1418 ]  . 
 lobiettivo primario stato valutare il successo tecnico e clinico , le complicanze e la mortalit perioperatoria , quello secondario la durata del trattamento e lincidenza di recidive a distanza . between march 2007 and march 2010 , we carried out a total of 85 percutaneous procedures on 75 patients ( 42 men and 33 women ; age range , 1788 years ; mean age , 60.8 years ) with biliary lesions . 
ten patients underwent a double treatment : ve due to new lesion onset following surgical reopmateriali e metodi nel periodo compreso tra marzo 2007 e marzo 2010 pres388 radiol med ( 2013 ) 118 : 386400 eration , one for the appearance of a second lesion following hepatic thermoablation and four due to recurrence of the original stenosis , which had already treated percutaneously . 
as for stenoses , we only considered iatrogenic lesions arising immediately after operation , thereby excluding any cicatricial brotic stenoses , which are mainly anastomotic and tend to represent a later complication of surgery . 
the majority of lesions were stulas ( 62 , 73% ) , followed by stenoses ( 17 , 20% ) and complete bile duct transections ( 6 , 7% )  . 
in 32 cases ( 37.7% ) , lesions ( 26 stulas , ve stenoses , one transection ) were secondary to biliary surgery for gallstones ( 12 cases ) or to pancreaticduodenal surgery for neoplasms of the pancreatic head ( 20 cases ) , with creation of a biliodigestive anastomosis ( bda )  . 
in 26 cases ( 30.6% ) , the lesions ( 16 stulas , seven stenoses , three transections ) were a complication of lc ; in 18 ( 21.1% ) , they were secondary to hr , which included ten typical partial hepatectomies ( ve right - sided , ve left - sided ) , four extended resections ( two right - sided , two left - sided ) and four segmental hepatectomies ( 11 stulas , ve stenoses , two transections )  . 
fistulas and complete biliary transections were characterised by the appearance of biliary material in the surgical drains without any signicant symptoms or by manifestations of intraperitoneal biliary collections : onset of acute pain in the right hypochondriac region , state of sepsis with elevated inammatory indices and , more rarely , biliary peritonitis . 
 classicazione le complicanze precoci post - operatorie delle vie biliari sono state classicate in tre gruppi , in base alla tipologia delle lesioni : stole ( comprese le deiscenze anastomotiche ) , stenosi e distacchi completi . 
riguardo alle stenosi abbiamo preso in considerazione unicamente quelle iatrogene , insorte nellimmediato post - operatorio escludendo le stenosi di natura brotico - cicatriziale , in prevalenza anastomotiche , che complicano gli interventi chirurgici pi tardivamente . 
 la maggior parte delle lesioni era rappresentata da stole ( 62 / 85 , 73% ) , le stenosi sono state 17 / 85 ( 20% ) e i distacchi completi delle vie biliari 6 / 85 ( 7% )  . 
in 32 / 85 casi ( 37 , 7% ) le lesioni ( 26 stole , 5 stenosi , 1 distacco ) erano secondarie ad interventi di chirurgia biliare per calcolosi ( 12 casi ) e pancreatico - duodenale per neoplasie cefalo - pancreatiche ( 20 casi ) con il confezionamento di unanastomosi biliodigestiva ( abd )  . 
in 26 / 85 casi ( 30 , 6% ) le lesioni ( 16 stole , 7 stenosi , 3 distacchi ) hanno complicato interventi di colecistectomia laparoscopica , mentre in 18 / 85 ( 21 , 1% ) sono state la conseguenza di interventi di resezione epatica , di cui 10 epatectomie parziali tipiche ( 5 destra e 5 sinistra ) , 4 resezioni allargate ( 2 destra e 2 sinistra ) e 4 epatectomie segmentarie ( 11 stole , 5 stenosi , 2 distacchi )  . 
la sede delle lesioni riassunta nella tabella 2 . presentazione clinica in tutti i pazienti lesordio clinico stato precoce : nelle stole e nei distacchi completi delle vie biliari stato caratterizzato dalla comparsa di materiale biliare nei drenaggi chirurgici in assenza di una sintomatologia signicativa o da manifestazioni secondarie alla presenza di raccolte biliari intraperitonali ( insorgenza di dolore acuto a partenza dallipocondrio destro , stato settico con rialzo degli indici di ogosi e , pi raramente , peritonite biliare )  . 
collections located at different sites ( interhepatophrenic , infrahepatic , cholecystectomy bed , morrisons recess ) were drained under us guidance in 4 / 23 cases , ct guidance in 3 / 23 cases and uoroscopic guidance in the interventional room in 16 / 23 cases . 
in the remaining 67 cases ( 78.9% ) , no noninvasive level - two investigation was performed as the patients were referred for ir on the basis of clinical symptoms ( most often biliary material in surgical drains or elevated cholestasis indices ) and us ndings to conrm clinical suspicion and perform the most appropriate percutaneous treatment in the same session . technical approach preliminary diagnostic cholangiography was performed using previously placed catheters : surgical drains in 16 cases ( 19% ) , nasobiliary tubes in 4 cases ( 5% ) and percutaneous transhepatic biliary drains ( ptbd ) in 17 cases ( 20% ) of which only seven were used for the subsequent percutaneous manoeuvres . 
overall , at the rst approach , 64 ptcs were performed with single access ( intercostal for right - sided ducts , or where not feasible , transepigastric for left - sided ducts ) , 13 with double access , right and left , and one with a third percutaneous right - sided access . 
puncture radiol med ( 2013 ) 118 : 386400 variabile ( range 533 gg , media 18 gg ) : nei casi di postcolecistectomia laparoscopica non convertita ( 7 pazienti ) il rialzo degli enzimi di colestasi si vericato pi precocemente ( range 522 gg , media 14 gg ) rispetto ai 10 pazienti trattati con abd o resezione epatica ( range 1233 gg , media 22 , 8 gg )  . diagnosi strumentale tutti i pazienti sono stati preliminarmente valutati con lecograa ( us ) : soltanto 18 / 85 casi ( 21 , 1% ) sono stati sottoposti ad unindagine di secondo livello [ tomograa computerizzata ( tc ) o risonanza magnetica / colangiopancreatograa con risonanza magnetica ( rm / cprm ) ]  . 
le raccolte localizzate in diverse sedi ( interepato - diaframmatica , sottoepatica , letto di colecistectomia , recesso di morrison ) sono state drenate con guida us in 4 / 23 casi , tc in 3 / 23 casi e radioscopica , in sala interventistica , in 16 / 23 casi . 
nei restanti 67 / 85 casi ( 78 , 9% ) lindagine non invasiva di secondo livello non stata eseguita , in quanto il paziente stato inviato alla ri sulla base della sintomatologia clinica ( pi frequentemente la comparsa di materiale biliare nei drenaggi chirurgici o il rialzo degli indici di colestasi ) e del quadro us , per confermare il sospetto clinico ed effettuare contestualmente il trattamento percutaneo pi appropriato . approccio tecnico le colangiograe diagnostiche preliminari sono state eseguite attraverso cateteri precedentemente posizionati : drenaggi chirurgici in 16 / 85 casi ( 19% ) , sondini naso - biliari in 4 / 85 casi ( 5% ) e cateteri percutanei transepatici di drenaggio biliare ( dtb ) in 17 / 85 pazienti ( 20% ) , dei quali soltanto 7 sono stati utilizzati per le successive manovre percutanee . 
complessivamente al primo approccio sono state effettuate 64 cpt con accesso singolo ( intercostale sui dotti di destra o laddove non eseguibile , trans - epigastrico sui dotti di sinistra ) , 13 con doppio accesso , destro e sinistro e 1 con terzo accesso percutaneo destro . 
la puntura e il cateterismo delle vie biliari sono stati effettuati con ago di chiba e set coassiali ( skater introducer set biliary access - angiotech , pbn medicals , danimarca ) e sotto controllo anestesiologico in sedo - analgesia con monitoraggio continuo del paziente . 
 il tentativo di valicare il segmento biliare interessato dalla lesione ( stola o stenosi biliare ) per raggiungere il lume intestinale e ricostituire la continuit bilio - digestiva sempre stato effettuato al primo approccio . 
d controllo colangiograco a 7 giorni con iniezione dallintroduttore ( freccia ) : completa risoluzione della stenosi . and catheterisation of the bile ducts were achieved with chiba needles and coaxial sets ( skater introducer set for biliary access , angiotech , pbn medicals , denmark )  . 
the attempt to cross the segment affected by the biliary stula or stenosis to reach the intestinal lumen and re - establish biliodigestive continuity was made at the rst approach in all cases . 
in 16 / 62 stole ( 25 , 8% ) stata inserita una protesi : in 11 / 16 casi con abd stato utilizzato uno stent metallico coperto di 1012 mm di calibro ( jostent , abbott enterprises , beringer , ch ) , a distanza media dalla prima procedura di 9 , 2 gg [ deviazione standard ( ds ) 5 , 9 gg ] , mentre nei restanti 5 / 16 casi con vie biliari integre una protesi plastica di 12 14 f di calibro ( carey - coons , boston scientic )  . 
cholangiography performed at 7 days through the externalinternal biliary drain shows persistence of a small stula ( open arrowhead ) after replacement of the surgical drain with a percutaneous multihole drainage catheter ( black arrowhead ) ( c )  . 
c controllo colangiograco a 7 giorni : liniezione di mezzo di contrasto attraverso il dtbei dimostra la persistenza di una esile stola ( testa di freccia vuota ) dopo sostituzione del tubo chirurgico con catetere di drenaggio pluriforato ( testa di freccia piena )  . 
e risultato nale : abd di ampio calibro e completa risoluzione della stola . after the rst procedure , where in the remaining 5 / 16 cases with intact bile ducts , we used a 12to 14 - f plastic endoprosthesis ( carey - coons , boston scientic , boston , ma , usa )  . 
in 4 casi di stenosi complesse causate da clips chirurgiche ( 3 cl ed 1 re ) , sono stati utilizzati cateteri a palloncino dotati di 4 aterotomi , di 8 mm di calibro ( cutting balloon , boston scientic , boston )  . 
in una stenosi di abd , causa linefcacia di tre bpt , stato posizionato uno stent metallico coperto di 10 mm di calibro ( jostent , abbott enterprises , beringer , ch )  . 
nei distacchi completi attraverso il dtbe posizionato in precedenza stato eseguito , quando possibile , un approccio percutaneoendoscopico con tecnica del rendez - vous . radiol med ( 2013 ) 118 : 386400 catheters with four atherotomes were used ( cutting balloon , boston scientic )  . 
 follow - up involved 59 patients discharged with clinical recovery , as 11 / 75 patients ( three stulas , four stenoses , four transections ) were reoperated and excluded from the followup and ve patients died due to progression of the underlying tumour . 
in the majority of patients , clinical and haematological monitoring was sufcient ; any even minimal change in the ndings was investigated with us , which was complemented by ct ( n = 3 ) and / or mr imaging ( n = 5 ) in eight equivocal cases . 
the former was dened as the feasibility of the ir procedures aimed at re - establishing continuity of the injured or stenotic bile duct and the latter as symptom regression with resolution of the complication and / or of the iatrogenic injury as a result of the ir procedure . technical success if we exclude the seven patients with previously placed ptbd , percutaneous transhepatic catheterisation and biliary drainage was completed in all cases ( 100% )  . 
in 73 cases ( 85.9% ) , the manoeuvre succeeded at the rst attempt and in only four cases ( 4.7% ) at the second attempt , after placement of an external biliary drain the remaining eight cases ( 9.4% ) , the attempt failed because of : ( a ) failure to cross a stenosis in four patients ( two lc and two hr ) and inability to restore the transected common bile duct in four ( two lc , one hr , one cdp ) owing to the presence of a bda ; ( b ) failure of the endoscopic approach . 
in all these cases an external biliary drain was left in place while the next treatment strategies were planned . clinical success il monitoraggio , che ha avuto una durata media di 16 , 7 mesi ( ds 10 , 5 ) , stato effettuato in 59 pazienti dimessi con guarigione clinica , poich 11 / 75 pazienti ( 3 stole , 4 stenosi e 4 distacchi ) sono stati sottoposti a reintervento chirurgico e quindi esclusi dal follow - up e 5 pazienti sono deceduti durante il follow - up per evoluzione della malattia neoplastica di base . 
nella maggior parte dei pazienti stato sufciente un monitoraggio clinico e siero - ematologico ; in caso di modicazioni seppur minime di questi quadri stata sempre eseguita lecograa , completata in 8 casi dubbi con tc e / o rm ( 5 rm e 3 tc )  . risultati nella valutazione dei risultati abbiamo considerato separatamente il successo tecnico e clinico , intendendo nel primo caso la fattibilit delle procedure di radiologia interventistica nalizzata al ripristino della continuit della via biliare lesionata o stenotica e nel secondo la regressione della sintomatologia con guarigione della complicanza e / o della lesione iatrogena mediata dal trattamento percutaneo . successo tecnico escludendo i 7 pazienti portatori di un dtb precedentemente posizionato , il cateterismo percutaneo transepatico e il drenaggio delle vie biliari sono stati possibili in 78 / 78 casi ( 100% )  . 
in 73 / 85 casi ( 85 , 9% ) la manovra riuscita al primo tentativo e in soli 4 / 85 casi ( 4 , 7% ) al secondo , previo posizionamento di un dtbe . 
nei restanti 8 / 85 casi ( 9 , 4% ) il tentativo fallito a causa di : ( a ) impossibilit di valicare una stenosi in 4 pazienti ( 2 cl e 2 re ) e ( b ) impossibilit di riguadagnare la via biliare principale a valle di un distacco in altrettanti ( 2 cl , 1 re , 1 dcp ) per la presenza di una abd o per linsuccesso dellapproccio endoscopico . 
 successo clinico abbiamo riportato un successo clinico complessivo in 74 / 85 casi ( 85 , 9% ) , con un tempo medio di trattamento di 34 , 9 giorni ( ds 23 , 7 gg ; mediana di 26 giorni ) ed una media di 4 , 1 procedure eseguite ( ds 1 , 4 ; media di 3 procedure )  . 
3a - c major stula originating from the cystic duct stump ( open arrow ) and right hepatic duct ( arrowhead ) , with interhepatophrenic bile collection drained by a 10 - f multihole catheter ( black arrow ) ( a , b )  . 
3a - c ampia stola ad origine dal moncone del cistico ( freccia vuota ) e dal dotto epatico destro ( testa di freccia ) , con raccolta inter - epatodiaframmatica drenata con catetere pluriforato di 10 f di calibro ( freccia piena ) ( a , b )  . 
 fistulas a total of 43 / 62 cases of biliary leakage ( 69.3% ) resolved with drainage alone , in most cases at the third cholangiographic examination ( mean total procedures , 3.8 ; sd , 1.1 ) ; mean catheter indwelling time was 29 ( sd , 15.8 ) days in 20 / 43 cases , the stula involved the bda , in 14 the common hepatic duct and in nine the cystic duct . 
in the ve patients with intact bile ducts who received plastic endoprostheses ( carey coons ) , stulas resolved completely in < 50 ( mean , 49.5 , sd , 31.3 ) days , and the endoprostheses were removed endoscopically . 
in the remaining three ( 4.8% ) cases ( one bda and two hr ) in which the stula was located in the intrahepatic bile ducts , percutaneous treatment did not produce the expected outcome . 
 gione con il solo drenaggio , nella maggior parte dei casi al terzo controllo colangiograco ( media procedure 3 , 8 totali , ds 1 , 1 ) ; il tempo medio di dimora del catetere stato di 29 gg ( ds 15 , 8 )  . 
in 20 / 43 casi la stola era situata a livello dellabd , in 14 / 43 casi interessava il dotto epatico comune , in 9 / 43 casi il dotto cistico . 
nei 5 casi con vie biliari integre in cui stata utilizzata la protesi plastica ( carey - coons ) , la completa risoluzione della stola si realizzata in un periodo inferiore ai 50 giorni ( media 49 , 5 gg , ds 31 , 3 gg ) con successiva rimozione della protesi per via endoscopica . 
nei restanti 3 / 62 ( 4 , 8% ) casi ( 1 abd e 2 re ) nei quali la stola era localizzata a livello delle vbi , il trattamento percutaneo non ha ottenuto il risultato atteso ; non sussistendo pertanto le condizioni tecniche idonee al posizionamento di una protesi , il paziente stato sottoposto ad un reintervento chirurgico . 
 stenosi in 13 / 17 casi ( 76 , 5% ) si ottenuto un completo successo radiol med ( 2013 ) 118 : 386400 stenosis complete clinical success was achieved in 13 / 17 cases ( 76.5% ) , on average after 20.7 ( sd , 16.9 ) days and after performing two procedures per patient ( sd , 1.1 ) ; in 11 / 13 patients , stenosis affected the bda and in two the biliary conuence . 
in the only case treated with a jostent , satisfactory bda calibre restoration after 7 days of placement of the stent ( subsequently pushed into the intestinal loop ) was conrmed on successive cholangiographic examinations performed until hospital discharge . 
 clinical failure coincided with technical failure in 4 / 17 cases ( 23.5% ) due to the onset of severe haemobilia requiring arterial embolisation in one case ( 5.5% ) of complex stenosis of the biliary conuence and due to the inability to crossclip - related stenoses associated with large stulas in three cases ( 18% )  . 
the remaining four patients ( 66.7% ) were referred for surgery , as they were not eligible for the percutaneousendoscopic rendezvous approach owing to the presence of a bda or endoscopic approach failure . 
treatment duration number of procedures according to intervention type , lesion and percutaneous procedure are given in table 4 . recurrence rate in the 10 / 75 patients who underwent two treatments , four showed recurrence at follow - up of a lesion judged as resolved at hospital discharge , corresponding to 6.7% of cases undergoing follow - up ( 4 / 59 )  . 
in two cases , bda stenosis recurred at 17 and 18 months after treatment , respectively ; in one case , a stula recurred 1 month after treatment ; in the other case , a stenosis developed at the site of a previous stula 7 months after treatment . 
in all four patients ( 100% ) , repeat treatment was technically and clinically successful , resulting in leion resolution . complications clinico , in media dopo 20 , 7 gg ( ds 16 , 9 gg ) e lattuazione di 2 procedure per ciascun paziente ( ds 1 , 1 ) ; in 11 / 13 pazienti la stenosi era situata a livello dellabd ed in 2 / 13 pazienti a livello della conuenza biliare . 
nei 4 casi trattati con cutting ballon si ottenuto un successo completo ; nellunico caso trattato con jostent il soddisfacente ripristino del calibro dellabd dopo 7 gg di permanenza dello stent ( poi sospinto nellansa intestinale ) stato confermato ai successivi controlli colangiograci no alla dimissione . 
 linsuccesso clinico ha coinciso con linsuccesso tecnico in 4 / 17 ( 23 , 5% ) casi : in un caso ( 5 , 5% ) di stenosi complessa della conuenza biliare , per linsorgenza di una grave emobilia che ha richiesto unembolizzazione arteriosa e in 3 / 17 casi ( 18% ) per limpossibilit di valicare stenosi serrate da clips chirurgiche , associate a stole ad ampia portata ; dopo 3 tentativi infruttuosi i pazienti sono stati sottoposti a reintervento chirurgico con vie biliari comunque drenate . distacchi in 2 / 6 casi ( 33 , 3% ) stato possibile lapproccio percutaneo - endoscopico con tecnica del rendez - vous con successo clinico completo dopo una media di 58 , 9 gg ( ds 28 , 9 ) e 5 , 5 procedure ( ds 2 , 1 )  . 
i restanti 4 / 6 pazienti ( 66 , 7% ) sono stati indirizzati alla chirurgia per limpossibilit di un rendez - vous percutaneo - endoscopico , a causa della presenza di unabd o per il fallimento dellapproccio endoscopico . 
la durata del trattamento ed il numero delle procedure in funzione del tipo di intervento , di lesione e di procedura percutanea sono riportati nella tabella 4 . incidenza di recidive a distanza dei 10 / 75 pazienti sottoposti a due trattamenti , 4 / 10 hanno presentato durante il follow - up una recidiva di una lesione dichiarata guarita alla dimissione che corrisponde al 6 , 7% dei casi monitorati ( 4 / 59 )  . 
in 2 casi si vericata la recidiva di una stenosi a livello dellabd rispettivamente a 17 e 18 mesi dal trattamento , in 1 caso la riapertura del tramite stoloso ad 1 mese dal trattamento e nellultimo caso comparsa una stenosi nella sede di una precedente stola a distanza di 7 mesi dal trattamento . 
in tutti e quattro i pazienti ( 100% ) il ri - trattamento ha avuto successo tecnico e clinico , con risoluzione delle lesioni . complicanze during treatments , we had 2 / 85 ( 2.3% ) severe complications , in both cases , severe haemobilia requiring emergency angiography . 
in both patients , arteriography showed iatrogenic injury to a branch of the right hepatic artery , which nel corso dei trattamenti abbiamo riportato 2 / 85 ( 2 , 3% ) complicanze gravi , in entrambi i casi rappresentate da emobilia importante che ha richiesto uno studio angiograco durgenza . 
in entrambi i pazienti larteriograa ha evidenziato una lesione iatrogena di un ramo dellarteria epatiradiol med ( 2013 ) 118 : 386400 ca destra , embolizzata con successo con spirali metalliche . 
 uno dei due pazienti ( 88 anni ) , clinicamente molto compromesso , deceduto per multiple organ failure ( mof ) a distanza di 48 h dal trattamento endovascolare con drenaggi funzionanti e bile pulita , rappresentando lunico caso di mortalit perioperatoria . 
one of the two patients ( 88 years ) was in critical clinical condition and died of multiple organ failure 48 h after endovascular treatment , with well - functioning drains and clear bile . 
minor complications occurred in six cases ( 7% ) : two of mild haemobilia that resolved with repeated lavage and closure outside the draining catheter , two partial dislocations of the catheter , one haematoma at the site of the right transhepatic access that resolved spontaneously and one of catheter cracking that was remedied by replacement . discussion the incidence of early postoperative biliary complications is reported to be slowly but steadily increasing [ 14 ] , even though some published studies state that the rate is substantially stable , with statistically random uctuations from year to year [ 58 ]  . 
in contrast to the literature , which reports lc to account for at least 2 / 3 cases of postoperative biliary complications [ 812 ] , in our study , we found a more homogeneous distribution ( 38.8% lesions caused by cdp , 21.2% by hr , and only 30.6% to lc ) , probably because we are sent patients from multiple hepatobiliary surgery referral centres that perform highly complex surgical operations . 
although various pathological classications of postoperative biliary complications have been proposed [ 1417 ] , we believe that classication into stulas , stenoses and complete transection is the most suited to dening a correct therapeutic strategy . 
in stulas in which biliary catheterisation is difcult due to the absence of dilatation , our treatment approach is in line with reported experiences [ 1824 ] , even though the lincidenza di complicanze precoci post - operatorie delle vie biliari riferita in lieve , ma costante crescita negli ultimi anni [ 14 ] , anche se in letteratura alcuni studi ne riportano una sostanziale stabilit , con oscillazioni statisticamente casuali da anno ad anno [ 58 ]  . 
contrariamente a quanto riferito in letteratura dove la cl rappresenta la causa pi frequente , almeno 2 / 3 dei casi , di complicanza post - operaroria delle vie biliari [ 812 ] , noi abbiamo riscontrato una distribuzione pi omogenea ( 38 , 8% lesioni conseguenti a dcp , 21 , 2% a re e solo 30 , 6% ad interventi di cl ) pi probabilmente correlabile allafferenza esclusiva al nostro istituto di plurimi centri di riferimento per la chirurgia epato - biliare che attuano interventi ad elevato coefciente di difcolt . 
sebbene siano state proposte diverse classicazioni anatomo - patologiche delle complicanze post - operatorie delle vie biliari [ 1417 ] riteniamo che la suddivisione in stole , stenosi e distacchi completi sia quella pi funzionale allimpostazione di una corretta strategia terapeutica . 
nelle stole , in cui il cateterismo delle vie biliari , come noto difcoltoso , per lassenza di dilatazione , il nostro approccio terapeutico si allinea con le esperienze della letteratura [ 1824 ] , pur avvalendosi la nostra casistica di un maggior numero di trattamenti rispetto alle serie considerate . 
in caso di fallimento clinico delle procedure di ri , il dtbe ha consentito di risolvere il problema dello stravaso extraluminale di bile nel 100% dei pazienti e di eseguire leventuale reintervento chirurgico ( 9 , 4% ) in condizioni di elezione , mentre il posizionamento di un dtbei ( 98 , 5% dei casi nel corso della prima procedura ) risultato efcace ai ni della guarigione in oltre i 2 / 3 dei pazienti con una sola recidiva al follow - up . riguardo alla scelta del calibro del drenaggio biliare , problema dibattuto in letteratura [ 18 , 21 ] , riteniamo che il calibro da noi utilizzato ( 78 f ) rappresenti un buon compromesso in grado da un lato di limitare il traumatismo della manovra e dallaltro di garantire un drenaggio efcace per la risoluzione della stola . 
lesecuzione di controlli colangiograci a breve - medio termine ( 57 gg ) consentoradiol med ( 2013 ) 118 : 386400 table 4 overall treatment duration ( in days and procedures ) and recurrence rate during the follow - up in relation to intervention and lesion type and interventional radiology procedure treatment duration ( days ) treatment procedures recurrence rate total operation lc conver . 
lc , conversion into laparotomy of a laparoscopic cholecystectomy ; cdp , cephalic duodenopancreatectomy ; hr , hepatic resection ; sd , standard deviation tabella 4 durata del trattamento ( in giorni e sedute ) e tasso di recidive nel follow - up in relazione a tipo di intervento , lesione e procedura di radiologia interventistica durata trattamento ( giorni ) sedute trattamento recidiva media media cl , colecistectomia laparoscopica ; conver . 
cl , conversione in laparotomia da colecistectomia laparoscopica ; dcp , duodeno - cefalo - ancreasectomia ; re , resezione epatica ; ds , deviazione standard number of treatments was higher . 
in the case of clinical failure of ir procedures , external biliary drains resolved the extraluminal biliary leakage in 100% of patients , allowing elective surgical reoperation ( 9.4% ) , whereas the placement of an externalinternal transhepatic biliary drain ( 98.5% of cases during the rst procedure ) was effective in > 2 / 3 patients , with only one recurrence at follow - up . the choice of biliary drainage catheter calibre is a muchno di valutarne lefcacia e la loro eventuale sostituzione con altri di maggior calibro ( da 10 f in soli 6 casi della nostra esperienza )  . 
sebbene in letteratura non siano riferite esperienze riguardo allimpiego di stent coperti o di protesi plastiche nel trattamento delle stole biliari , i nostri risultati sono stati soddisfacenti senza complicanze o recidive e sovrapponibili a quelli gi riferiti in due analoghi studi condotti nel nostro istituto nel 2002 e nel 2008 [ 23 , 24 ]  . 
shortto midterm cholangiographic examinations ( 57 days ) allow evaluation of effective drainage and replacement with larger catheters , if necessary ( 10 f in only six cases in our series )  . 
although the literature does not report any experience with the use of covered stents or plastic endoprostheses in treating biliary stulas , our results have been satisfactory , with no complications or recurrence , and are comparable with those of two similar studies conducted at our centre in 2002 and in 2008 [ 23 , 24 ]  . 
however , as stent or endoprosthesis placement prolongs treatment ( 59 days for stents and 50 days for plastic endoprostheses ) compared with externalinternal biliary drainage alone ( 29 days ) , patients need to be accurately selected to justify the longer hospital stay , cost and risk of nosocomial infections . 
in light of our experience ( 95.2% clinical efcacy , < 3% immediate complication rate , 1.2% perioperative mortality and a 4.6% recurrence rate at follow - up ) , we believe that ir can provide a valuable alternative to surgery ( long - term efcacy < 80% , 20 30% morbidity and 3 7% mortality , increasing to 20% in patients with associated conditions ) for treating stulas [ 14 , 2527 ]  . 
it has almost identical efcacy to treatment with endoscopic retrograde cholangiopancreatography ( ercp ) , with sphincterectomy and placement of biliary endoprosthesis ( even though there is wide variation , from 80% to 100% , in the different series ) [ 2830 ]  . 
in addition , there is the added benet of being feasible in patients with bda , who accounted for more than 50% of cases in our study . cases of complete bile duct transection are more complex , as the clinical picture is more severe and treatment options fewer . 
in our view , the percutaneous approach , which is difcult owing to failure of the biliary tree to dilate and the need for forced access in segmental transections , is fundamental ; in addition to providing an accurate anatomical marker of the site of transection , placement of a percutaneous transhepatic biliary drain allows the urgent clinical problem to be solved such that , if needed , the patient can then face surgery more safely . 
despite obtaining full recovery with the endoscopic percutaneous approach in only 2 / 6 cases ( 3% ) in our series , we believe it is worth attempting this procedure at least once , as long as that no technical obstacle exists . 
as is known , percutaneous treatment of postoperative biliary stenoses is an alternative both to the endoscopic approach , if it fails , and to surgery , which is hampered by unfavourable rates of efcacy , morbidity and mortality [ 25 , 31 , 32 ]  . 
in agreement with some studies [ 33 ] and in disagreement with others [ 34 ] , our theratuttavia poich il loro posizionamento allunga i tempi di trattamento ( 59 gg per gli stent e 50 gg per le protesi plastiche ) rispetto al solo dtbei ( 29 gg ) riteniamo che sia indispensabile unaccurata selezione dei pazienti che giustichi sia lincremento dei tempi di ospedalizzazione , dei costi e del rischio di insorgenza di complicanze infettive nosocomiali . 
alla luce della nostra esperienza ( efcacia clinica pari al 95 , 2% , tasso di complicanze immediate inferiore al 3% , mortalit pressoch nulla ed incidenza di recidive al follow - up del 4 , 6% ) riteniamo che nel trattamento delle stole la ri possa rappresentare una valida opzione alla chirurgia ( efcacia a distanza inferiore all80% , morbilit del 20%30% e mortalit dal 3%7% no al 20% in caso di patologie associate ) [ 14 , 2527 ]  . 
nei confronti del trattamento endoscopico mediante ercp , con snterotomia e posizionamento di protesi endobiliare , ha unefcacia pressoch sovrapponibile ( anche se la variabilit da studio a studio molto alta , con valori compresi tra l80% e il 100% ) [ 2830 ] , con il vantaggio di poter essere eseguita anche in presenza di pazienti con abd , che nella nostra casistica rappresentavano oltre la met dei casi . i casi di distacco completo delle vie biliari costituiscono un problema assai pi complesso per il quadro clinico pi grave e le pi limitate possibilit terapeutiche . 
lapproccio percutaneo , difcoltoso non solo per lassenza di dilatazione dellalbero biliare ma anche , nei casi di distacchi segmentari , per la necessit di un accesso obbligato , , a nostro avviso , fondamentale ; infatti , mediante il posizionamento di un dtb oltre a fornire un preciso repere anatomico della sede del distacco , consente di risolvere il problema clinico urgente permettendo al paziente di affrontare un eventuale intervento chirurgico in maggior sicurezza . 
sebbene nella nostra esperienza con lapproccio endoscopico / percutaneo abbiamo ottenuto la guarigione soltanto in 2 / 6 casi ( 33% ) riteniamo che tale procedura possa essere meritevole di almeno un tentativo , quando non esistano impedimenti di natura tecnica . 
il trattamento percutaneo delle stenosi biliari post - operatorie rappresenta , com noto , unalternativa sia al fallimento dellapproccio endoscopico sia allintervento chirurgico gravato da unincidenza sfavorevole di efcacia , morbilit e mortalit [ 25 , 31 , 32 ]  . 
in accordo con alcuni dati della letteratura [ 33 ] e in disaccordo con altri [ 34 ] la nostra strategia terapeutica stata quella di valicare al primo tentativo la stenosi per eseguire contestualmente la bpt . 
la percentuale del nostro insuccesso tecnico ( 23 , 5% ) , superiore a quello riferito in esperienze recenti della letteratura [ 33 , 34 ] , dipeso dallimpossibilit di trattare stenosi precoci rappresentate dai 3 casi con radiol med ( 2013 ) 118 : 386400 peutic strategy is to cross the stenosis at the rst attempt in order to carry out percutaneous transhepatic bilioplasty in the same session . 
our technical failure rate ( 23.5% ) , higher than that reported in recent studies [ 33 , 34 ] , was related to our inability to treat early stenoses in the three cases of cliprelated stenoses associated with extensive stulas , and by the case of complex stenosis of the biliary conuence resulting in severe perioperative haemobilia . 
the use of accessory devices ( cutting balloon , covered or removable stents ) , as suggested in the literature [ 24 , 3437 ] , proved effective for treating late stenoses and may be valuable for early stenoses , as well . the incidence and type of severe complications observed in our study are similar to those reported in the literature [ 18 , 21 ] : haemorrhagic complications are the most dangerous , and operators should have access to an angiography room and suitable material for arterial embolisation , which is the treatment of choice [ 38 ]  . 
by contrast , mild venous haemobilia requires no particular intervention apart from increasing the frequency of cholangiographic examinations to ascertain that bleeding has truly stopped . stenosi da clips chirurgiche associate a stole ad ampia portata ed al caso di stenosi complessa della conuenza biliare esitata in grave emobilia periprocedurale . 
 per lo stesso motivo la percentuale di recidiva a distanza che abbiamo riportato ( 18 , 2% , con insorgenza media a 16 , 5 mesi dalla dimissione ) stata inferiore rispetto a quella riferita in letteratura [ 33 , 34 ]  . 
limpiego di device accessori ( cutting - balloon , stent coperti o rimovibili ) utilizzati , come suggerisce la letteratura [ 24 , 3437 ] , nel trattamento della stenosi a distanza nella nostra esperienza si rivelato efcace e potrebbe rappresentare una valida opzione anche per le stenosi precoci . 
lincidenza e il tipo di complicanze gravi che abbiamo riportato sono sovrapponibili a quelle riferite in letteratura [ 18 , 21 ] : le complicanze emorragiche sono le pi temibili e gli operatori dovrebbero avere la disponibilit di un sala angiograca e del materiale idoneo per poterle trattare con lembolizzazione arteriosa che rappresenta la terapia di scelta [ 38 ]  . 
al contrario nei casi di emobilie lievi , di pertinenza venosa , non necessario ricorrere ad alcun comportamento particolare , se non quello di aumentare la frequenza dei controlli colangiograci per vericare leffettivo esaurimento del sanguinamento . conclusions conclusioni percutaneous treatment of early postoperative biliary complications is feasible , safe and effective and can therefore be proposed as a valuable alternative to endoscopic and surgical techniques . 
fava1 1department of radiology , san luigi gonzaga hospital , university of turin , orbassano ( turin ) , italy 2department of thoracic surgery , san luigi gonzaga hospital , university of turin , orbassano ( turin ) , italy 3pet center , irmet spa , turin , italy correspondence to : l . 
luigi gonzaga university hospital , regione gonzole 10 , 10043 orbassano ( turin ) , italy , tel . : + 39 - 011 - 9026406 , e - mail : luciano.cardinale@gmail.com received : 6 july 2011 / accepted : 5 october 2011 / published online : 17 september 2012 springer - verlag 2012 abstract this study describes the diffuse neoplastic conditions that may affect pleural membranes . 
 finally , we discuss the best diagnostic approach in the case of suspected primary or secondary neoplastic involvement of pleural membranes . keywords malignant pleural mesothelioma ct pleural metastases mr imaging pleural neoplasms riassunto questa trattazione illustra le patologie neoplastiche diffuse che coinvolgono a vario titolo i foglietti pleurici . 
 il mesotelioma la prima neoplasia di origine pleurica per frequenza ed importanza , di seguito analizzeremo gli aspetti peculiari anche dellinteressamento metastatico della pleura da parte di carcinomi , linfomi e timomi . 
inne analizzeremo quale pu essere il corretto iter diagnostico nel sospetto di interessamento neoplastico , primitivo o secondario , dei foglietti pleurici . parole chiave mesotelioma pleurico maligno tc metastasi pleuriche rm tumori pleurici introduction introduzione pleural neoplasms may be classied as benign or malignant and primary or secondary . 
malignant pleural mesothelioma is the most frequent primary pleural neoplas its onset is closely linked to a history of occupational or environmental exposure to asbestos , and it is characterised by extremely aggressive behaviour and a dismal prognosis . 
 although any malignancy is capable of giving rise to pleural metastases , cancers of the lung and breast , lymphomas , le neoplasie che insorgono a carico della pleura possono essere benigne o maligne , primitive o secondarie . 
il mesotelioma pleurico maligno la pi frequente neoplasia pleurica primitiva , la cui insorgenza strettamente correlata a una pregressa esposizione , lavorativa o ambientale , allasbesto ed caratterizzato da un comportamento biologico assai aggressivo e prognosi infausta . 
pur essendo qualsiasi neoplasia maligna in grado radiol med ( 2013 ) 118 : 366378 and gastrointestinal and genitourinary cancers are those that most frequently metastasise to the pleura [ 2 ]  . the diagnostic contribution of imaging , in particular of radiology [ conventional radiography and computed tomography ( ct ) ] , is universally acknowledged and well documented . 
magnetic resonance ( mr ) imaging and , more recently , positron emission tomography ( pet ) have increasingly gained ground as level - two techniques capable of contributing additional useful information to the diagnosis and staging of disease . 
chest ultrasound ( us ) may also play an important role in the diagnosis of diffuse neoplastic conditions of the pleura as it relies on the same semiological criteria as ct or magnetic resonance ( mr ) imaging : its use in chest imaging has recently gained increasing acceptance , overcoming the extreme suspicion with which it was viewed in the past . 
a nding often associated with , and in some cases predominates , the clinical picture in both inammatory and neoplastic lesions is pleural effusion : in the differential diagnosis , identifying serosal thickening , especially if nodular , may prove highly useful . in consideration of the frequency with which radiologists are called upon to differentiate among diffuse neoplastic conditions of the pleural serosa and the clinical importance of a prompt diagnosis , this paper illustrates imaging features typical of primary and secondary diffuse pleural neoplasms and briey discusses the use of thoracoscopy and cytologic examination . primary neoplastic disease : malignant pleural mesothelioma malignant pleural mesothelioma is the most frequent primary neoplasm of the pleura . 
 di dare origine a metastasi pleuriche , le neoplasie polmonari e mammarie , i linfomi , le neoplasie del tratto gastro - intestinale e genito - urinario sono , in ordine di frequenza , quelle che pi spesso coinvolgono secondariamente la pleura [ 2 ]  . 
la risonanza magnetica ( rm ) e pi recentemente la tomograa ad emissione di positroni ( pet ) si stanno sempre pi affermando come metodiche di secondo livello in grado di aggiungere ulteriori informazioni , utili ai ni della diagnosi e della stadiazione della malattia . 
anche lecograa toracica ( us ) pu rivestire un ruolo importante nella diagnosi delle malattie neoplastiche diffuse della pleura avvalendosi degli stessi criteri di semeiotica di cui si avvalgono tc o rm : il suo utilizzo in ambito toracico ha suscitato ultimamente sempre maggiori consensi , al contrario di quanto accadeva in passato ove il rapporto con il distretto toracico era vissuto con estrema difdenza . 
un elemento che spesso concomitante e talvolta si sovrappone in maniera preponderante ai processi patologici sopra riportati il versamento liquido , che pu dominare la scena sia nelle lesioni ogistiche che in quelle neoplastiche : utile ai ni della diagnosi differenziale pu risultare lidenticazione di un ispessimento della sierosa , specie se di carattere nodulare . in questo articolo , in considerazione della frequenza con cui il radiologo coinvolto nella diagnosi differenziale delle malattie neoplastiche diffuse della sierosa pleurica e dellimportanza clinica che assume in queste circostanze un sollecito inquadramento diagnostico , verranno discussi e illustrati gli aspetti dellimaging riconducibili alle neoplasie primitive o secondarie che coinvolgono diffusamente la sierosa pleurica ed un accenno allutilizzo della toracoscopia e dellesame citologico . patologia neoplastica primitiva : mesotelioma pleurico maligno il mesotelioma pleurico maligno la pi frequente neoplasia pleurica primitiva , la cui incidenza andata progressivamente aumentando negli ultimi decenni in rapporto alla accresciuta esposizione , professionale e ambientale , alle bre di asbesto . 
poich il periodo di latenza intercorrente fra esposizione allasbesto e comparsa della neoplasia di almeno 20 anni , la massima incidenza viene osservata negli individui della 6a8a decade di et e , poich la maggior parte dei casi si sviluppa a seguito di una esposizione lavorativa allasbesto , il sesso maschile risulta interessato assai pi spesso di quello femminile , con un rapporto di 15 e 3 casi per milione , rispettivamente [ 3 , 4 ]  . allesordio il quadro radiologico contraddistinto dal368 radiol med ( 2013 ) 118 : 366378 fig . 
 the neoplastic nature of the thickening may therefore be hypothesised in the presence of circumferential involvement ( 100% specicity ) , nodularity ( 94% specicity ) , thickness > 10 mm ( 94% specicity ) and involvement of the mediastinal border ( 88% specicity ) [ 6 , 7 ]  . 
however , the sensitivity of these signs is low , ranging from 30% to 60% depending on the series [ 7 ] , and the nding of a normal pleural surface at ct does not rule out the neoplastic nature of the effusion [ 6 ]  . 
the posterior and inferior portions of the hemithoraces are most frequently involved , probably owing to gravitational factors , leading to hypomobility and retraction of the basal regions with effects on respiratory function [ 8 ]  . 
 la natura neoplastica di un ispessimento dunque ipotizzabile in presenza di estensione circonferenziale ( specicit 100% ) , nodularit ( specicit 94% ) , spessore maggiore di 10 mm ( specicit 94% ) e coinvolgimento della limitante mediastinica ( specicit 88% ) [ 6 , 7 ]  . 
la sensibilit dei segni citati , tuttavia , bassa potendo variare dal 30% al 60% a seconda delle casistiche [ 7 ] e , infatti , il riscontro di una supercie pleurica di normale morfologia alla tc non esclude la natura neoplastica del versamento [ 6 ]  . 
sono interessate pi spesso le porzioni posteriori e inferiori degli emitoraci probabilmente per cause gravitazionali ; ne conseguono ipomobilit e retrazione radiol med ( 2013 ) 118 : 366378 370 fig . 
pleural mesothelioma is characterised by intermediate or slightly hyperintense signal on t1 - weighted sequences compared to the surrounding healthy tissue and by a more intense signal on t2 - weighted sequences . 
the signal of pleural mesothelioma may be further enhanced by using gadolinium - based paramagnetic contrast material . the combination of morphological data and information on signal intensity has been found to increase signicantly the sensitivity and specicity of mr imaging [ 11 ]  . 
le metastasi a distanza sono relativamente poco comuni , soprattutto nelle prime fasi della malattia , cos come linteressamento linfonodale . il radiogramma del torace costituisce lesame di primo livello , evidenziando spesso versamento pleurico di carattere aspecico , ed pi raramente evocativo in presenza di opacit margino - costali mammellonate [ 5 ] .la tc senza dubbio pi accurata rispetto alla radiologia tradizionale sia nellidenticazione sia nella caratterizzazione della patologia pleurica . 
4a , b malignant pleural mesothelioma in a 74 - year - old man with a large mass at the right lower third of the hemithorax and diaphragmatic inltration : comparison between ct and mr imaging . 
even though no comparative studies of the potential of multislice ct ( msct ) and mr imaging have been conducted , the development and quality of ct and the use of highquality multiplanar reconstructions have decreased the gap with mr imaging , particularly for assessing the diaphragm and chest wall . 
this , combined with the greater availability of ct equipment and the faster acquisition speed , suggest limiting the use of mr imaging to equivocal cases requiring higher contrast resolution . recent research on the biological characteristics of malignant mesothelioma has shown that prognosis is directly linked to the angiogenic index and that the tumour can be treated with the new - generation antiangiogenic drugs [ 12 ]  . 
il mesotelioma pleurico si caratterizza , rispetto al tessuto sano circostante , per un segnale intermedio o lievemente iperintenso nelle sequenze t1 pesate , e un segnale pi intenso nelle sequenze pesate in t2 . 
il segnale del mesotelioma pleurico pu essere ulteriormente evidenziato mediante uso di mezzo di contrasto paramagnetico ( a base di gadolinio )  . combinando i dati morfologici con le informazioni relative allintensit di segnale , la sensibilit e la specicit della rm aumentano notevolmente [ 11 ]  . 
inoltre , le sequenze pesate in t1 , con soppressione del grasso , hanno dimostrato la maggior sensibilit nel rilevare enhancement delle scissure interlobari e per valutare linvasione delle strutture adiacenti . 
tuttavia non esistono , allo stato attuale , studi comparativi che confrontino le potenzialit della tc multistrato ( tcms ) rispetto alla rm , ciononostante levoluzione e la qualit della tecnologia tc e lutilizzo di ricostruzioni multiplanari di alta qualit hanno consentito una riduzione del gap con la rm in particolare per quanto concerne lo studio del diaframma e della parete toracica . 
questi progressi , uniti alla maggior disponibilit delle macchine e a una maggior velocit di acquisizione , suggeriscono di connare lapprofondimento mediante rm solo in casi controversi , in virt della maggior risoluzione di contrasto di questultima . recenti ricerche sulle caratteristiche biologiche del mesotelioma maligno , hanno mostrato come la prognosi del paziente sia direttamente legata allindice angiogenetico proprio della malattia e quindi aggredibile con farmaci antiangiogenetici di nuova concezione [ 12 ]  . 
dopo iniezione di mezzo di contrasto paramagnetico , vengono acquisite immagini sequenziali ad intervallo di tempo sso sul tessuto tumorale e lanalisi farmacocinetica su queste sequenze fornisce accurate informazioni sulla microvascolarizzazione della massa . 
 la pet presenta una limitata resa diagnostica nella valutazione dellinteressamento linfonodale loco - regionale per il frequente riscontro sia di falsi positivi che di falsi ne372 radiol med ( 2013 ) 118 : 366378 fig . 
b scansione coronale di indagine rm fast spin echo ( fse ) t2 pesata : le componenti solide e liquide presentano segnale differente e possono essere differenziate con facilit per leccellente risoluzione di contrasto , con versamento iperintenso e masse pleuriche ipointense . 
 enhanced mr imaging is , in fact , an essential tool for assessing tumour perfusion , and mr is currently the modality used to assess response to these experimental therapies in clinical trials [ 13 ]  . 
 pet has limited diagnostic yield in detecting locoregional lymph node involvement , as it often produces both false positive and false negative results , whereas it plays an important role in detecting distant metastases during staging [ 9 , 14 , 15 ]  . us can readily depict secondary invasion of the chest wall and pleura in mesothelioma and lung and breast cancer . 
 pathological conditions involving pleura or chest wall soft tissues often have similar characteristics and common criteria for malignancy : they have blurred and poorly dened margins and they are hypoechoic , heterogeneous vascularised [ 1620 ]  . 
us may occasionally provide additional staging information when diaphragm involvement is suspected , thus proving to be superior to ct ( see below ) [ 21 ]  . a detailed comparison of conventional radiology , us and ct demonstrated that none of the three modalities alone is able to provide a comprehensive diagnosis , as each has different specicity and sensitivity for detecting pathognogativi , mentre svolge un ruolo importante nella stadiazione per la ricerca di metastasi a distanza [ 9 , 14 , 15 ]  . lecograa pu facilmente dimostrare una invasione secondaria della parete toracica e della pleura in presenza di un mesotelioma cos come di un tumore polmonare , e di un tumore mammario . 
le patologie che coinvolgono la pleura o i tessuti molli della parete toracica hanno spesso caratteristiche simili e con criteri di malignit comuni : hanno bordi sfumati e poco deniti , sono ipoecogene e disomogenee , e vascolarizzate [ 1620 ]  . 
inoltre , per la possibilit di controllo real - time e per la duttilit della metodica , la guida ecograca sempre pi diffusamente utilizzata durante le procedure bioptiche sulle lesioni della parete toracica e della pleura . 
lecograa pu occasionalmente aggiungere informazioni ulteriori ai ni stadiativi della malattia nel sospetto di interessamento diaframmatico risultando superiore alla tc ( vedi anche paragrafo successivo ) [ 21 ]  . in realt , unanalisi dettagliata di confronto tra radiologia tradizionale , ecograa e tc , dimostrava come nessuna delle tre metodiche fosse in grado di essere esaustiva nella diagnosi essendo dotata di specicit e sensibilit assai differenti nellidenticazione delle lesioni patognomoniche di mesotelioma e concludeva sulla effettiva necessit di ricorrere alle tre metodiche in maniera complementare [ 22 ]  . anche nel mesotelioma la recente introduzione di nuove radiol med ( 2013 ) 118 : 366378 possibilit terapeutiche con farmaci antiangiogenetici ha fatto sorgere la necessit di una corretta valutazione della risposta al trattamento instaurato facendo riferimento a criteri non solo dimensionali , ma anche di tipo funzionale e valutando nel tempo la progressione o meno della vascolarizzazione neoplastica mediante studi perfusionali [ 15 ]  . 
analogamente agli studi funzionali tc e rm , anche la pet parrebbe in grado di monitorare la risposta al trattamento e di valutare la successiva prognosi a distanza dei pazienti trattati [ 9 ]  . patologia neoplastica secondaria : carcinomi nei pazienti di et superiore ai 50 anni le metastasi pleuriche rappresentano la seconda causa di versamento dopo lo scompenso cardiaco . 
in una rassegna comprendente 1783 pazienti portatori di versamento pleurico maligno , i tumori extrapleurici iniziali pi frequentemente in causa risultarono il carcinoma broncogeno ( 36% del totale dei casi ) e quello della mammella ( 25% ) , seguiti , in ordine di frequenza dalle lesioni a carico del sistema gastro - intestinale e genito - urinario [ 23 ]  . 
 il riconoscimento diretto delle localizzazioni secondarie a livello dei foglietti pleurici da parte delle metodiche di imaging nella maggior parte dei casi infruttuosa in quanto le metastasi pleuriche molto spesso hanno dimensioni ridotte ( < 5 mm ) , di difcile riconoscimento [ 24 ]  . 
i segni diretti dellinteressamento neoplastico delle superci pleuriche si caratterizzano allimaging radiologico per la presenza di un ispessimento liscio e diffuso oppure grossolanamente nodulare ; le dimensioni delle lesioni non sono uniformi e la densit pu essere disomogenea . 
plurime lesioni focali pleuriche con enhancement di aspetto disomogeneo associate a versamento a livello dellemitorace destro in uomo di 57 anni affetto da carcinoma squamoso scarsamente differenziato del faringe . monic lesions , which led us to conclude that the three modalities should be used in a complementary manner [ 22 ]  . in mesothelioma , as in other tumours , the recent introduction of new antiangiogenic treatments call for accurate assessment of treatment response by analysing both dimensional and functional criteria and assessing the progression of tumour vascularisation by means of perfusion studies [ 15 ]  . 
as with functional ct and mr imaging , pet seems capable of monitoring treatment response and predicting prognosis after treatment [ 9 ]  . secondary neoplastic disease : carcinomas in patients older than 50 years , pleural metastases are the second - most frequent cause of effusion after heart failure . 
in a survey conducted on 1 , 783 patients with malignant pleural effusion , the most frequent primary extrapleural tumours were bronchogenic carcinoma ( 36% ) and breast carcinoma ( 25% ) , followed by gastrointestinal and genitourinary lesions [ 23 ]  . 
 direct visualisation of pleural metastases by diagnostic imaging is often unsuccessful because the metastases tend to be very small ( < 5 mm ) and difcult to recognise [ 24 ]  . 
the direct imaging signs of neoplastic pleural involvement are the presence of smooth and diffuse or grossly nodular thickening ; lesion size is not uniform and density may be inhomogeneous . 
lesions are often multiple and usually unilateral [ 6 ]  . although mr imaging does not show signicantly different morphological results compared with ct , it does provide useful information on signal intensity , which is high on t2 - weighted sequences in the case of malignancy , with 100% sensitivity and 87% specicity [ 25 ]  . 
in a study conducted on 35 patients with bronchogenic carcinoma and suspected pleural metastases , pet was able to diagnose secondary pleural involvement in 16 of 18 patients , with overall sensitivity , specicity and accuracy values of 88% , 94% and 91% , respectively [ 26 ]  . us has always had a well - dened role in the study of pleural effusion , in view of its ability to depict even small effusions . 
in addition , the possibility of identifying septations inside the effusion ( loculated effusion ) gives it an advantage over ct , thanks to the possibility of changing patient position and real - time imaging , which help to clarify equivocal or manifestly pathological ndings . a recent study [ 21 ] compared the diagnostic potential of chest us and ct for detecting signs suggestive of malignant disease in patients with pleural effusion . 
in systemic lymphatic disease , pleural effusion typically develops as a result of mediastinal lymph node involvement and obstruction to lymphatic drainage of la rm non presenta reperti signicativamente diversi in confronto alla tc per quanto concerne il dato morfologico , ma fornisce interessanti risultati relativamente allintensit del segnale , che elevata nelle sequenze t2 pesate in presenza di malignit con una sensibilit del 100% e una specicit dell87% [ 25 ]  . 
in uno studio condotto su 35 pazienti affetti da carcinoma broncogeno con sospette metastasi pleuriche , la pet stata in grado di diagnosticare un coinvolgimento secondario della pleura in 16 su 18 pazienti con valori complessivi di sensibilit , specicit e accuratezza rispettivamente del 88% , 94% e 91% [ 26 ]  . tradizionalmente lecograa ha da sempre mantenuto un ruolo ben codicato nello studio dei versamenti pleurici grazie alla sua efcacia nel riconoscimento dei versamenti anche di modesta entit . 
inoltre , la possibilit di individuare la presenza di sepimenti allinterno del versamento ( versamento pluriconcamerato ) la pone in posizione di vantaggio anche nei confronti della tc per la possibilit di variare i decubiti e per la conduzione in real - time dellesame , potendo approfondire e documentare meglio i reperti dubbi o i riscontri francamente patologici . in una recente indagine [ 21 ] sono state confrontate le potenzialit diagnostiche dellecograa toracica e della tc nella ricerca di segni suggestivi di malignit in presenza di versamento . 
in presenza di una linfopatia sistemica , la comparsa di un versamento pleurico per lo pi secondaria al coinvolgimento dei linfonodi mediastinici e al conseguente ostacolo al drenaggio linfatico della sierosa pleurica . 
 di solito limaging sia tc sia rm si caratterizza per la presenza di noduli multipli ( o solitari ) oppure di ispessimenti a placca con larga base dimpianto , spesso accompagnati da un versamento liquido . 
inoltre esistono tre piccole interruzioni di continuo allorigine anteromediale del diaframma : uno mediale e due parasagittali ( forami del morgagni ) che permettono la comunicazione tra comparto toracico e addominale . 
inne un timoma che invade la pleura , pu valicare il diaframma per inltrazione diretta , superando la fascia endotoracica e la fascia trasversale , mettendo in comunicazione diretta la parete toracica con quella addominale . approccio clinico conclusivo alla diagnosi denitiva nelle malattie neoplastiche diffuse della sierosa pleurica : esame citologico e toracoscopia come stato diffusamente riportato in precedenza , il riscontro clinico - radiograco di un versamento pleurico pu essere espressione di una patologia di origine pleurica , polmonare o extrapolmonare [ 33 ]  . 
nei pazienti di et superiore a 60 anni , la maggior parte dei versamenti pleurici causata da una lesione neoplastica maligna , primitiva o secondaria , che si trova pi spesso in stadio evolutivo avanzato ed caratterizzata da una rapida compromissione della qualit di vita e da una prognosi severa , con sopravvivenza mediana inferiore a 12 mesi . 
 qualora raccolta anamnestica , esame clinico e indagini radiograche non consentano di avanzare con elevata probabilit lipotesi di versamento pleurico di tipo trasudatizio ( pi spesso secondario a insufcienza ventricolare sinistra , cirrosi epatica , ipoalbuminemia e dialisi peritoneale ) , il passo diagnostico successivo costituito dallesame chimifig . 
7 contrast - enhanced ct at the level of the lung bases shows diffuse nonnodular pleural thickenings ( arrow ) and effusion in the left hemithorax and ipsilateral paravertebral mass ( asterisk ) in a 27 - year - old woman with non - hodgkins lymphoma . 
7 la scansione tc , eseguita a livello delle basi polmonari , dopo somministrazione di mezzo di contrasto mostra diffuso ispessimento pleurico non nodulare ( freccia ) con versamento in corrispondenza dellemitorace sinistro e massa paravertebrale omolaterale ( asterisco ) in donna di anni 27 affetta da linfoma non hodgk the pleural serosa . 
both ct and mr imaging normally show the presence of multiple ( or solitary ) nodules , or of broad - based plaque - like thickening , often accompanied by effusion . 
contrast - enhanced ct at the level of the aortic arch showing extensive pleural localisations in the right hemithorax and chest wall inltration in a 49 - year - old woman . 
the authors described three potential routes through which neoplastic cells may pass from the chest to the abdomen : the rst is dissemination into the retroperitoneum through the retrocrural space . 
nei casi rimasti privi di diagnosi o quando non sia stato possibile distinguere fra mesotelioma radiol med ( 2013 ) 118 : 366378 secondly , there are three small openings on the anteromedial portion of the diaphragm one medial and two parasagittal ( foramina of morgagni ) which connect the thoracic and the abdominal compartments . 
lastly , pleural thymomas may cross the diaphragm through direct inltration by penetrating the endothoracic and transverse fascia and creating a direct communication between the chest and abdominal walls . conclusive clinical approach to the nal diagnosis in diffuse neoplastic pleural diseases : cytology and thoracoscopy as widely reported by other authors , clinical and radiographic nding of pleural effusion may reect pleural , pulmonary or extrapulmonary disease [ 33 ]  . 
in patients older than 60 years , most pleural effusions are caused by a primary or secondary malignancy , which is often at an advanced stage and characterised by rapid decline in quality of life and a poor prognosis , with a median survival < 12 months . 
 when patient history , clinical examination and radiographic ndings do not support a likely hypothesis of transudative pleural effusion ( often secondary to left ventricular dysfunction , liver cirrhosis , hypoalbuminaemia and peritoneal dialysis ) , the next diagnostic step is thoracentesis with chemical , bacteriological and cytological analysis of the uid . 
when no diagnosis is reached or when it is not possible to differentiate between malignant pleural mesothelioma and metastatic involvement , transparietal ctor us - guided core needle biopsy signicantly increases the diagnostic yield of cytological analysis of the thoracentesis uid [ 34 , 35 ]  . recently , in consideration of the medicolegal and insurance implications of a diagnosis of malignant pleural mesothelioma , early thoracoscopy or videothoracoscopy has increasingly been used for the diagnosis . 
thoracoscopy is a minimally invasive technique with a diagnostic yield of almost 100% in that it allows exploration of the entire pleural surface and enables targeted biopsies , providing sufcient material for histological examination and immunohistochemical analysis , if needed . 
11 immagine ottenuta con toracoscopia video - assistita che dimostra multiple ed eterogenee mammellonature pleuriche in quadro di mesotelioma maligno . pleurico maligno e coinvolgimento metastatico della pleura , lagobiopsia transparietale , eseguita con ago tranciante sotto controllo tc o ecograco consente di incrementare signicativamente la resa diagnostica dellesame citologico del liquido di toracentesi [ 34 , 35 ]  . in tempi recenti , anche in considerazione delle conseguenze medico - legali e assicurative derivanti dalla diagnosi di mesotelioma pleurico maligno , si fatto sempre pi frequente limpiego precoce della toracoscopia ( o videotoracoscopia ) diagnostica . 
la toracoscopia una manovra scarsamente invasiva , caratterizzata da una resa diagnostica prossima al 100% in quanto consente di esplorare lintera supercie pleurica e di eseguire biopsie mirate sotto il controllo della vista , e fornisce materiale adeguato per lesame istologico e per eventuali indagini immunoistochimiche . 
in assenza di versamento , quando il cavo pleurico risulta obliterato dalla crescita neoplastica , non possibile eseguire la toracoscopia e si fa quindi ricorso alla biopsia pleurica a cielo aperto , utilizzando una piccola toracotomia . 
197 , ruijin 2nd road , shanghai 200025 , china correspondence to : xiao - yi ding , tel . : + 86 - 18918967155 , fax : + 86 - 21 - 64150737 , e - mail : dxyrj@hotmail.com received : 29 october 2011 / accepted : 15 december 2011 / published online : 9 august 2012 springer - verlag 2012 abstract purpose . 
this study was done to investigate x - ray , computed tomography ( ct ) and magnetic resonance ( mr ) imaging features of recurrence in giant cell tumour of bone ( gctb ) and to evaluate risk factors . 
the common radiological ndings ; factors related to tumour recurrence such as gender , age , location ; pathological fracture , campanacci grading and surgical procedure were analysed by nonparametric test ( mannwhitney u test for two independent samples test and kruskalwallis h test for multiple independent samples test )  . 
the imaging features of recurrent gctb were as follows : osteolytic destruction or bone resorption of graft bone or around the polymethylmethacrylate ( pmma ) , soft tissue mass formation and expansile change . 
 i rilievi radiologici ed i fattori correlati alla recidiva tumorale come sesso , et , sede , presenza di frattura patologica , classicazione di campanacci e procedura chirurgica sono stato analizzate mediante test non parametrici ( test u di mann - whitney u e test h di kruskal - wallis )  . 
le principali caratteristiche radiologiche del gctb recidivante sono risultate essere : distruzione osteolitica , riassorbimento dellinnesto osseo o in adiacenza al polimetilmetacrilato ( pmma ) , insorgenza di massa nei tessuti molli e comparsa di formazione espansiva . 
 riassorbimento osseo , insorgenza di massa nei tessuti molli e comparsa di formazioni espansive sono segni radiologici afdabili di recidiva . parole chiave neoplasie ossee tumore a cellule giganti recidiva tomograa computerizzata radiograa risonanza magnetica introduction giant cell tumour of bone ( gctb ) is a benign but locally aggressive neoplasm accounting for approximately 5% of all primary bone tumours [ 1 , 2 ]  . 
many studies show that tumour size , location , x - ray grading , pathological fracture and histological grading have no impact on tumour recurrence , invasiveness and distant metastases [ 9 ]  . 
the recurrence rate after wide resection is 312% , and intralesional curettage shows an overall recurrence rate of 1618% [ 8 , 10 ]  . radiological monitoring can be used for early detection of recurrence [ 35 , 11 ]  . 
recommend that mr imaging be performed if the patient presents with newly occurring pain or swelling or the standard x - rays shows any suspicious ndings [ 7 ]  . 
the purpose was to investigate x - ray , ct and mr imaging features of recurrence in gctb and evaluate the risk factors . materials and methods patients between june 1990 and september 2011 , 316 patients with a histologically proven diagnosis of gctb were treated surgically at our institution . 
sixty - eight primary gctb were located in the distal femur , followed by proximal tibia ( n = 57 ) , mobile spine ( n = 24 ) , sacrum ( n = 23 ) , distal radius ( n = 21 ) and other locations ( n = 123 ) ( table 1 )  . routine postoperative follow - up examinations were performed at 1 , 3 and / or 6 months and thereafter every 6 months for 3 years . 
ct and mr imaging were used for further investigation when radiography demonstrated a suspected relapse ( such as graft or bone resorption , expansile change and local soft tissue swelling / mass formation , etc . ) or when clinical symptoms and signs suggested recurrence despite negative radiography . 
the main symptoms of recurrence were local mass and mild pain and / or limitation of activity , of which 24 cases had localised swelling and pain as the initial symptoms . 
the lesions were graded according to the campanacci staging system [ 12 ] : 11 cases were classied as grade 1 , 39 as grade 2 and ve as grade 3 . in 55 recurrent cases , four showed malignant transforma458 radiol med ( 2013 ) 118 : 456464 table 1 treatment data and factors related to recurrence in giant cell tumour of bone ( gctb )  . 
age , location , campanacci grading and adjuvants were analysed with the kruskalwallis h test tabella 1 dati relativi al trattamento e fattori correlati alla recidiva del tumore osseo a cellule giganti ( gctb )  . 
in two patients , a recurrent lesion in the proximal tibia crossed over the knee joint to involve the distal femur ; in one case , the proximal tibia lesion involved the bular head and destroyed the knee joint . 
of the eight cases of pathological fracture at preliminary diagnosis , ve fractures were located in the lower limb and three in the upper limb . all 55 recurrent patients underwent plain x - ray , 39 ct , and 29 mr imaging . 
patient records were screened for clinical data , operative notes and follow - up records . imaging procedures all patients underwent anteriorposterior and lateral plain radiographs routinely , and exposure factors varied depending on diseased region . 
ct examination was performed in 39 cases with a 4or 16 - slice multidetector spiral ct scanner ( lightspeed , general electric medical systems , milwaukee , wi , usa ) , according to an established protocol . 
a combination of axial , sagittal and coronal images was obtained using a t1 - weighted spin - echo ( se ) sequence and a t2 - weighted fast se ( fse ) sequence with and without fat suppression . 
 statistical analysis the common radiological ndings ; factors related to tumour recurrence such as gender , age and location ; pathologic fracture , campanacci grading and surgical procedure were analysed by nonparametric test ( mannwhitney u test for two independent samples test and kruskalwallis h test for multiple independent samples test ) using spss version 13.0 ( spss inc , chicago , il , usa )  . 
two cases with recurrence in the proximal tibia manifested graft resorption , and the lesion crossed over the knee joint and resulted in expansile osteolytic bone destruction in the distal femur . 
one case with recurrence in the proximal tibia demonstrated bone absorption around pmma and involved expansile destruction in the bular head , also leading to knee swelling and destruction of articular surface . 
2a - e recurrent gctb in the proximal tibia after bone - cement lling : a osteolytic destruction , > 5 - mm irregular lucent area ( black arrows ) and soft tissue mass ( white arrow ) in the front of cement were manifested on radiography . 
2a - e recidiva di gctb nella porzione prossimale della tibia dopo riempimento dellosso con cemento : a alla radiograa si sono evidenziate osteolisi , presenza di area radiotrasparente > 5 mm ( frecce nere ) e di massa nei tessuti molli ( freccia bianca ) in adiacenza al cemento . 
3a , b recurrent gctb in the 9th to 11th thoracic vertebrae : a the lesion was not detected , other than the condition of internal xation , on account of excessive overlapping on radiographic images . 
la massa nei tessuti molli ed il coinvolgimento del canale vertebrale sono evidenziabili nonostante gli artefatti da indurimento del fascio secondari alla presenza di dispositivo di ssazione interna metallico . table 2 common radiographic ndings in recurrent giant cell tumour of bone ( gctb )  . 
in the curettage group , 23 cases had postoperative relapse after curettage and autologous or allogenic bone grafting , 17 cases after curettage and bone cement lling ( pmma ) , ve cases after vertebral lesion curettage and internal xation and four cases after simple curettage . 
in the group treated with wide resection , three cases were relapses after resection of the distal radius and autologous bula transplantation , and three occurred after resection and articial prosthetic replacement . 
among patients undergoing intralesional adjuvants , those treated with pmma plus phenol had a lower ( p = 0.029 ) risk of having local recurrence than did patients treated with bone grafting plus phenol and no adjuvants ( bone grafting )  . 
there was no statistical signicance in other factors , including gender , age , location , pathological fracture and campanacci staging ( table 1 )  . discussion the biological behaviour of gctb is aggressive . 
in this study , the recurrence rate was 17.4% , the median relapse time was 22 months and 65.5% of recurrences occurred 462 radiol med ( 2013 ) 118 : 456464 fig . 
5ad recurrent gctb in the sacrum : lesion and surrounding soft tissue mass and their relationships with vertebral canal and pelvic cavity : a sagittal t1 - weighted image , b axial t2 - weighted image , c coronal t2 - weighted image , d sagittal fat - suppressed t2 - weighted image . 
5a - d recidiva di gctb nel sacro : lesione e massa nei tessuti molli circostanti e loro relazione con il canale vertebrale e lo scavo pelvico : a immagine sagittale t1 - dipendente , b immagine assiale t2 - dipendente , c immagine coronale t2 - dipendente , d magine sagittale t2 - dipendente con soppressione del segnale del tessuto adiposo . 
la recidiva tumorale presenta intensit di segnale bassa - intermedia nelle immagini t1 - dipendenti e segnale eterogeneamente elevato nelle immagini t2 - dipendenti . radiol med ( 2013 ) 118 : 456464 within 24 months after surgery , consistent with the literature [ 7 ]  . 
therefore , short - term re - examinations and manipulations should be performed within this period , although recurrence in gctb is usually nonfatal [ 35 , 13 ]  . 
imaging abnormalities can appear earlier than clinical pain or dysfunction , which may allow further attempts to preserve joint function rather than proceeding to en bloc resection and massive prosthetic replacement [ 11 ]  . 
on radiography , local bone absorption or sclerotic rim after implantation of autologous bone or bone allograft and a 2to 4 - mm translucent zone between pmma and normal bone after pmma implantation did not represent recurrence at follow - up . 
new graft or bone resorption , soft tissue mass formation and aggravated expansile change were signicant ndings for recurrence , although some of these patients had no obvious clinical symptoms . 
ct and mr imaging had higher costs than x - ray and were used for further examination when radiography suggested a relapse or when clinical symptoms and signs suggested recurrence despite negative radiography . 
ct has a higher density resolution , and cross - sectional scanning can avoid overlapping interference due to pmma or metal xation , which can clearly display the structure within scraped lesions , cortical disruption , surrounding soft tissue mass , bone resorption and destruction . 
mr imaging has good soft tissue resolution , which can help assess joint involvement [ 11 ] and better display the soft tissue masses of recurrent lesions , a particularly obvious advantage after bone - cement lling . 
pmma appeared as a signal vacuity on all sequences and did not interfere with mr images as much as it did on ct , where there was substantial beam - hardening artefact . 
 contrast - enhanced examination helps distinguish tumour recurrence from scar and guide needle biopsy and operative procedure . surgical treatment options include intralesional curettage or segmental resection [ 10 ]  . 
in recent years , many authors have employed intralesional curettage plus adjuvant therapy ( high - speed burr , bone - cement lling ) to treat campanacci grade 3 gctb , and the relapse rate was no different from that of campanacci grade 2 [ 13 ]  . 
in the cases of curettage , the recurrence rate was higher after implantation of autogenous or allogenic bone rather than pmma [ 3 , 9 , 13 , 15 ]  . 
it is possible that pmma can make the local temperature rise beyond 60 to ablate tumour cells in the process of polymerisation , and the released monomer also has toxicity , which can effectively kill residual tumour cells of the inner wall of the cavity [ 13 , 19 ]  . 
it is conducive to early detection of recurrent lesions , but it is sometimes difcult to identify nonfusion of transplanted bone and tumour recurrence on radiographs [ 13 ]  . since 1969 , pmma has markedly reduced the recurrence rate of gctb [ 19 ]  . 
local curettage plus adjuvant therapy ( bone - cement lling after high - speed burr , chemical cautery , argon knife , laser carbonization , etc . ) can effectively reduce recurrence [ 3 , 4 , 13 , 19 ] , but validation of the efcacy of adjuvant therapy still lacks well - controlled , comparative studies . 
an important cause of recurrent soft tissue mass formation may be regional perforation of cortical bone into soft tissue or soft tissue contamination during operation [ 3 , 13 ]  . 
this study was undertaken to identify tumoural inltration of peri - enhancing brain tissue in patients with glioblastoma by means of perfusion computed tomography ( pct ) parameters , cerebral blood volume ( cbv ) and permeability surface ( ps )  . 
eight patients with surgically treated glioblastoma who were eligible for radiotherapy and nine patients with brain metastases from lung and breast cancer underwent ct before and after injection of contrast mediucbv and ps were calculated in the contrast - enhancing lesion area , in the area of perilesional oedema and in the normal - appearing white matter ( nawm ) , normalised to contralateral symmetrical areas . 
signicant differences in nps ( p < 0.005 ) were found between the typically vasogenic oedema surrounding the metastases and signal alteration surrounding the glial neoplason the contrary , no signicant differences were detected in the same areas for ncbv . 
scopo del presente studio stato identicare linltrazione tumorale del tessuto cerebrale circostante larea lesionale dimpregnazione in pazienti con glioblastoma tramite tomograa computerizzata perfusionale ( tcp ) , valutando i parametri volume ematico cerebrale ( cbv ) e supercie di permeabilit ( ps )  . 
otto pazienti affetti da glioblastoma trattato chirurgicamente , candidati alla radioterapia , e nove pazienti con metastasi cerebrali da tumore polmonare e mammario hanno effettuato una tc prima e dopo somministrazione di mezzo di contrasto . 
queste 432 radiol med ( 2013 ) 118 : 431443 keywords glioblastoma perfusion computed tomography cerebral blood volume permeability surface informazioni possono essere utilizzate per integrare il piano di trattamento radioterapico e / o chirurgico . parole chiave glioblastoma tomograa computerizzata perfusionale volume ematico cerebrale supercie di permeabilit introduction introduzione glioma malignancy is related to their ability to inltrate the brain tissue and recruit or synthesise vascular networks for further growth [ 1 ]  . 
within the tumour mass , cell hypoglycaemia and hypoxia lead to the production of angiogenic cytokines , with subsequent neoangiogenesis and increased volume and ow of blood in the tumour bed [ 1 ]  . 
it is known that angiogenesis is inuenced by broblast growth factor ( fgf ) , transforming growth factor beta ( tgf - ) , vascular endothelial growth factor ( vegf ) and platelet - derived growth factor ( pdgf ) , although it is assumed that these are not the only factors involved [ 1 ]  . 
it is also known that angiogenesis and neoangiogenesis are controlled by different mechanisms : vegf and fgf act directly on endothelial cells , whereas tgfand pdgf interact with inammatory and connective tissue cells . the pathological grading of gliomas is based on cytological and histological parameters , such as cytological atypia , mitosis , necrosis , cellularity , vascularity and endothelial cell proliferation . 
as the overall grade is assigned by using the highest - grade region , it is possible that a highgrade tumour may be misclassied as a result of sampling error . 
as malignant tumours are accompanied by angiogenic growth factor expression [ 3 ] , surrogate markers of tumour angiogenesis , microvascular density and increased vascular permeability have been associated with neoangiogenesis and tumour grading . 
vascular permeability has been non - invasively measured using various magnetic resonance ( mr ) perfusion techniques , which show that regional blood volume and microvascular permeability correlate with tumour grade [ 68 ]  . 
advanced mr techniques , such as spectroscopy , diffusion - tensor imaging ( dti ) and perfusion - weighted imaging ( pwi ) all of which provide more substructural information [ 9 ] are now widely used to characterise brain tumours [ 10 ] and predict the transformation and recurrence of gliomas and patient survival [ 11 ]  . perfusion ct ( pct ) is an alternative means of assessing cerebral haemodynamics in patients with stroke or brain tumours [ 12 , 13 ] and has some advantages over mr imaging la malignit dei gliomi legata alla loro capacit di inltrare il tessuto cerebrale e generare delle nuove reti vascolari per sostenere la propria crescita [ 1 ]  . 
allinterno della massa tumorale in rapida crescita , il decit ossigenativo e glicemico portano alla produzione di citochine angiogenetiche , stimolo per la neoangiogenesi tumorale che aumenta il volume ed il usso sanguigno allinterno del tumore [ 1 ]  . 
 risaputo che la neoangiogenesi dipende dal broblast growth factor ( fgf ) , dal trasforming growth factor - beta ( tgf - beta ) , dal vascular endotelial growth factor ( vegf ) e dal platelet derived growth factor ( pdgf ) , sebbene questi non siano gli unici fattori coinvolti [ 1 ]  . 
peraltro langiogenesi e la neoangiogenesi sono controllate da diversi meccanismi : vegf e fgf agiscono direttamente sulle cellule endoteliali , mentre tgf - beta e pdgf interagiscono con cellule inammatorie e del tessuto connettivale . 
 il grading dei gliomi si basa su diversi parametri citologici ed istologici quali atipie citologiche , numero di mitosi , presenza di necrosi , cellularit , neovascolarizzazione e proliferazione di cellule endoteliali . 
i tumori gliali di grado iv possono essere inoltre caratterizzati da una certa eterogeneit con presenza nella stessa massa tumorale di aree di alto e basso grado [ 2 ]  . 
il grading tumorale complessivo assegnato utilizzando la regione a pi alto grado contenuta nella massa tumorale , ed quindi possibile che venga sottoposta a biopsia unarea a basso grado allinterno del tumore e che quindi il grading venga sottostimato . 
siccome i tumori maligni sono accompagnati dallespressione di fattori di crescita angiogenetici [ 3 ] , che sono considerati markers dellangiogenesi tumorale , la densit microvascolare e laumento della permeabilit vascolare sono stati ricondotti alla neoangiogenesi tumorale e alla presenza di una rete microvascolare tumorale e , per questo motivo , sono correlati con il grading del tumore . 
una pi alta permeabilit si associa ad un pi alto grading patologico [ 4 ] e a una riduzione della risposta alla terapia anti - angiogenetica [ 5 ]  . 
 la misurazione non invasiva della permeabilit vascolare stata eseguita usando varie tecniche perfusionali , tra le quali la risonanza magnetica ( rm ) - perfusion , che hanno mostrato come il volume di sangue regionale e le misurazioni della permeabilit microvascolare siano correlate con il grado del tumore [ 68 ]  . 
le tecniche di rm avanzate , quali la spettroscopia , la diffusion - tensor imaging ( dti ) e la perfusion - weighted imaging ( pwi ) , ognuna delle quali forradiol med ( 2013 ) 118 : 431443 [ 14 ]  . 
it requires a multislice ct scanner equipped with an automatic injector and produces a cine scan that provides information based on the analysis of the rst pass of an intravenously administered contrast bolus into cerebral vessels . 
 postprocessing must be carried out on a separate workstation to generate colour perfusion maps and calculate regions of interest ( rois ) [ 1517 ]  . the primary application of pct in ischaemic disease is to calculate brain perfusion and cerebral haemodynamic reserve by mapping cerebral blood ow ( cbf ) , cerebral blood volume ( cbv ) and mean transit time ( mtt ) , which unlike with mr imaging may be done with a single acquisition . 
conventional imaging is less effective in differentiating gliomas because although contrast - enhanced images reveal a disrupted or absent bbb , it does not necessarily reveal tumour microvascularity or neovascularity . malignant brain gliomas are characterised by neovascularity and increased angiogenic activity and have a higher proportion of immature and hyperpermeable vessels [ 18 ]  . 
 recent studies [ 12 , 1921 ] show that pct imaging is helpful in assessing preoperative histological grade , differentiating tumour enhancement and radiation necrosis , evaluating response to antiangiogenic agents and guiding biopsy procedures when the biopsy target is chosen on the basis of the identication of hypervascularity inside heterogeneous tumours . 
in the case of contrast - enhanced ct , the hypodense halo surrounding a metastatic lesion [ 24 ] represents pure vasogenic oedema not containing any tumour cells , whereas the hypodense halo next to a glioma may consist of oedema and tumour tissue without any signicant bbb loss . 
the aim of this study was to investigate whether there is any statistically signicant difference in cbv and ps values in the hypodense area surrounding highgrade gliomas and that surrounding metastases in a control group with metastatic brain lesions . 
 recentemente stata introdotta la tomograa computerizzata perfusionale ( tcp ) come metodo alternativo per la valutazione dellaemodinamica cerebrale in corso di ictus ed in presenza di tumori cerebrali [ 12 , 13 ] , con alcuni vantaggi rispetto allimaging di rm [ 14 ]  . 
essa richiede un tomografo multistrato , con un iniettore automatico , che sia in grado di effettuare scansioni in modalit cine per fornire informazioni basate sullanalisi del primo passaggio del bolo di contrasto intravenoso nei vasi cerebrali . 
il post - processing si effettua su apposita workstation che genera mappe di perfusione a colori e permette il calcolo della perfusione allinterno di speciche regioni di interesse ( rois ) [ 1517 ]  . 
 come prima applicazione nella patologia ischemica la tcp permette di valutare la perfusione e la riserva emodinamica cerebrale attraverso la generazione delle mappe di usso ematico cerebrale ( cbf ) , volume ematico cerebrale ( cbv ) e tempo di transito medio ( mtt ) che , diversamente dalle tecniche di rm , pu avvenire mediante una singola acquisizione ; ma inoltre in grado di valutare lintegrit della barriera emato - encefalica ( bee ) attraverso un altro parametro : la supercie di permeabilit ( ps )  . 
le tecniche di imaging convenzionali sono meno efcaci nel differenziare i gliomi perch , sebbene le immagini dinamiche rivelino distruzione o assenza della bee , ci non sufciente per caratterizzare lassetto di microvascolarizzazione e di neovascolarizzazione tumorale . i gliomi cerebrali maligni sono caratterizzati da una neovascolarizzazione , da un aumento dellattivit angiogenetica , ed hanno una quota maggiore di vasi immaturi ed iper - permeabili [ 18 ]  . 
studi recenti [ 12 , 1921 ] hanno dimostrato che la tcp utile nel determinare il grado istologico pre - operatorio , nel differenziare tra impregnazione tumorale e necrosi post - radioterapica , nel valutare la risposta alla terapia anti - angiogenetica e nel guidare le procedure bioptiche quando viene scelto il bersaglio bioptico sulla base dellidenticazione dellipervascolarizzazione allinterno di masse tumorali eterogenee . 
 nel nostro studio abbiamo ipotizzato che la tcp , attraverso il calcolo delle mappe cbv e ps , possa essere utile per valutare larea parenchimale perilesionale subito adiacente alla regione di enhancement tumorale . 
nellesame tc convenzionale con contrasto , lalone ipodenso che circonda la lesione metastatica , caratterizzata da enhancement [ 24 ] , sicuramente espressione di un edema puro vasogenico senza la presenza di cellule tumorali allinterno . 
they underwent brain pct 1 month after surgery ( t0 , baseline ) and every 3 months after radiotherapy until tumour progression ( t1 ) , dened as an increase in the area of residual enhancement or as the appearance of nodular or diffuse enhancement . 
 the control group consisted of nine patients with brain metastases from lung ( four cases ) or breast ( ve cases ) cancer , who also underwent pct during the ct examination scheduled for radiotherapy planning . 
 this prospective study was approved by our institutional review board , and all patients gave informed consent . perfusion computed tomography pct was performed using a 64 - slice multidetector row ct ( mdct ) scanner ( general electric , milwaukee , wi , usa )  . 
 a noncontrast enhanced ct head scan ( gantry tilt 0 ) was used to localise the roi before obtaining a perfusion scan , for which 50 ml of nonionic contrast ( 370 mgi / ml ) was injected at a rate of 4 ml / s through a 20 - gauge intravenous line . 
five seconds after the injection , a continuous cine scan was started using the following parameters : 90 kvp , 100 ma , 85 - mm sections and 1 s / rotation , for a duration of 45 s . 
 using the artery with the greatest peak and slope on time attenuation curves as the arterial input function and the superior sagittal sinus as the output venous function , colourcoded maps were generated on the basis of the cbv and ps data , with the latter exploiting capillary permeability [ 25 ]  . 
 no patient experienced an adverse reaction to the contrast medium . ps nella regione di ipodensit circostante i gliomi ad alto grado in confronto alla regione di ipodensit attorno a metastasi in un gruppo di controllo di pazienti con lesioni metastatiche cerebrali . 
abbiamo inoltre confrontato i valori di cbv e ps nel gruppo di pazienti affetti da glioma prima della terapia chirurgica o radiante , ed alla comparsa di recidiva di malattia a tre mesi dalla terapia radiante o chirurgica . 
 materiali e metodi selezione dei pazienti da giugno 2009 a dicembre 2010 , abbiamo arruolato un gruppo di studio costituito da 8 pazienti , 6 uomini e 2 donne , di et compresa tra i 58 ed i 69 anni ( et media 60 anni ) affetti da glioma cerebrale di alto grado [ grado iv secondo la classicazione world health organization ( who ) , glioblastoma multiforme ] , trattati chirurgicamente e con radioe chemioterapia adiuvante . 
essi hanno effettuato una tcp dellencefalo ad 1 mese dallintervento chirurgico ( tempo t0 ) ed ogni 3 mesi , dopo la radioterapia , no alla progressione di malattia ( comparsa di recidiva / residuo ) che stata denita come un aumento dellenhancement sui margini di resezione o come comparsa di un avanzamento nodulare , sempre sui margini di resezione , caratterizzato da evidente contrast - enhancement allesame contrastograco standard ( tempo t1 )  . 
 stato poi utilizzato un gruppo di controllo costituito da 9 pazienti con metastasi cerebrali ( 5 metastasi da tumore polmonare e 4 da tumore mammario ) , anchessi sottoposti a tcp durante lesame tc , ed inseriti in un piano di trattamento radioterapico . 
ogni paziente stato valutato al ne di escludere la presenza di insufcienza renale ed allergia . il nostro studio prospettico stato approvato dal comitato etico e ad ogni paziente stato fornito un modulo per la compilazione del consenso informato . image analysis tomograa computerizzata perfusionale we performed a retrospective roi - based analysis using a dedicated workstation ( advantage windows 4.4 , ge ) equipped with specic perfusion analysis software ( perfusion 3 , ge )  . 
the same rois were mirrored to the unaffected contralateral side as controls unless they proved to be affected ( which occurred when they were near the midline ) , in which case the rois lo studio perfusionale dellencefalo stato eseguito mediante un tomografo multidetettore a 64 le di detettori ( general electric , milwakee , usa )  . 
al ne di localizzare la regione da studiare , si proceduto ad eseguire una scansione basale [ senza somministrazione di mezzo di contrasto ( mdc ) ] con inclinazione del gantry di 0 . 
 a 5 secondi dal tempo di iniezione stata acquisita una scansione in modalit cine ( continua ) con la seguente tecnica : 90 kvp , 100 mas ed 1 secondo di rotazione per una durata di 45 secondi . radiol med ( 2013 ) 118 : 431443 fig . 
1 roi al tempo t1 tracciate manualmente nellarea di impregnazione tumorale , nellarea ipodensa perilesionale ( edema 1 pi prossimale ed edema 2 pi periferico ) e nella sostanza bianca contigua apparentemente sana ( nawm )  . were positioned in the most homogeneous - looking normal part of the parenchyma . 
to avoid any partial volume effect due to other anatomical structures , rois were positioned in the most solid portion of the tumour area ( the most homogeneous contrast - enhancing area ) and the most uniform hypodense area of peritumoural oedema , avoiding any necrotic or haemorrhagic foci . four separate roi measurements were obtained , and the maximum value was recorded [ 26 ]  . 
to minimise variability , each parameter was normalised to the mirrored roi measurements of the unaffected contralateral side and called normalised cbv ( ncbv ) and normalised ps ( nps )  . statistical analysis rois were positioned by the same observer at different times ( 1 month apart ) to evaluate testretest reproducibility ( r ) , which was determined by using repeated analysis of variance ( anova ) measurement methods . 
successivamente , attraverso un software dedicato , abbiamo elaborato delle mappe a colori per lidenticazione del cbv e della ps [ 25 ]  . non si sono vericate reazioni avverse al mdc in tutti i pazienti dei gruppi in studio . analisi delle immagini stata condotta unanalisi retrospettiva su una workstation dedicata ( advantage windows 4.4 , ge ) utilizzando un software di analisi perfusionale ( perfusion 3 ge )  . 
attraverso uno strumento di mirroring , le roi precedentemente tracciate sono state riportate su punti esattamente corrispondenti dellencefalo del lato controlaterale sano , al ne di ottenere un gruppo di controllo . 
2 t0 : manually drawn rois on the enhancing tumour area , the perilesional hypodense area ( the nearest oedema 1 and the more peripheral oedema 2 ) and on the contiguous normal - appearing white matter ( nawm )  . 
4a ncbv values in oedema 1 , oedema 2 , enh and normal - appearing white matter ( nawm ) in patients affected by glioma at t0 and t1 , compared with patients affected by metastases . 
4a box e whiskers plots dei valori di ncbv calcolati nelledema 1 , nelledema 2 , nellenh e nella nawm in pazienti affetti da glioma al tempo t0 e t1 , confrontati con i pazienti affetti da metastasi . 
signicant differences of the chosen metrics ( ncbv and nps ) in the selected rois ( nawm , oedema 1 , oedema 2 and enh ) between glioma patients and controls were evaluated using the mannwhitney u test . 
 results an average r of 0.77 was obtained from the analysis of test retest reproducibility among the chosen metrics , indicating an acceptable variability of the roi positioning process as performed by the same observer at different times . 
 per ridurre al minimo la variabilit , ogni parametro stato normalizzato rispetto alle misure delle roi nel lato controlaterale sano e nominati come ncbv ed nps . analisi statistica le roi sono state posizionate dallo stesso osservatore in tempi diversi per valutare la riproducibilit test - retest ( r ) , determinata usando misurazioni ripetute con il metodo dellanalisi della varianza ( anova )  . 
per la riproducibilit del test - retest si stabilito che r fosse espresso con un numero tra 0 e 1 , dove 0 indica assenza di riproducibilit ed 1 indica perfetta riproducibilit . 
le differenze nei valori medi misurati per ncbv e nps nelle roi selezionate ( nawm , edema 1 , edema 2 ed enh ) nei pazienti con glioma sono stati valutati attraverso il metodo anova friedman , test nonparametrico che valuta tre o pi campioni appaiati . 
 le differenze statisticamente signicative dei parametri scelti ( ncbv ed nps ) nelle roi selezionate ( nawm , edema 1 , edema 2 ed enh ) ai diversi tempi t0 e t1 nella popolazione di studio sono state valutate retrospettivamente tramite il test di wilcoxon . 
le differenze statisticamente signicative dei parametri scelti ( ncbv ed nps ) nelle roi selezionate ( nawm , edema 1 , edema 2 ed enh ) tra i 438 ncbv nps ncbv nps ncbv nps ncbv nps table 1 values of ncbv and nps in glioma patients and in patients with brain metastases at time t0 and t1 . 
 risultati abbiamo ottenuto un valore medio di r pari a 0 , 77 studiando la riproducibilit tra i parametri scelti che indica una variabilit accettabile nel processo di posizionamento delle roi da parte dello stesso osservatore in tempi diversi . 
5a box e whiskers plots dei valori di ncbv calcolati nella nawm in pazienti affetti da glioma al tempo t0 e t1 , confrontati con i pazienti affetti da metastasi . 
6a box e whiskers plots dei valori di ncbv calcolati nelledema 2 in pazienti affetti da glioma al tempo t0 e t1 , confrontati con i pazienti affetti da metastasi . 
b box e whiskers plots dei valori di nps nelledema 2 in pazienti affetti da glioma al tempo t0 e t1 , confrontati con i pazienti affetti da metastasi . discussion the role of pct in grading gliomas has been widely discussed [ 3 , 12 , 13 , 19 , 23 , 27 ] , but its potential as a means of functional imaging capable of revealing subtle ultrastructural changes inside brain peritumoural tissue has not yet been fully evaluated . 
al ne di valutare se tali cambiamenti fossero dovuti alla presenza 440 radiol med ( 2013 ) 118 : 431443 sia deledema vasogenico che del tessuto tumorale nellarea edematosa , abbiamo confrontato interindividualmente i valori relativi a ncbv e nps con i corrispettivi ottenuti nei pazienti con metastasi ( tabella 1 )  . 
nella letteratura che tratta di tc perfusionale , il cbv considerato un accurato biomarker della malignit del tessuto neoplastico , in quanto i valori di cbv possono essere correlati al grading tumorale [ 7 , 12 , 19 , 2835 ] e alla progressione maligna ad un grado peggiore [ 22 ] , ma meno si conosce invece delleffettivo ruolo del parametro ps . esiste una base teorica [ 36 ] che mostra una relazione tra la permeabilit endoteliale ed il grading tumorale , in quanto i tumori ad alto grado come noto esprimono un aumentato livello di citochine vasoattive e fattori di crescita endoteliali ( vegf ) che promuovono la proliferazione endoteliale ed un incremento della permeabilit vascolare . 
al ne di valutare questa tendenza dei gliomi esiste un parametro chiamato microvascularity endothelial permeability surface area product ( ps ) che caratterizza la diffusione di alcuni mezzi di contrasto dai vasi sanguigni allo spazio interstiziale , in relazione al danno e allaumentata permeabilit della bee . 
il usso della diffusione del mezzo di contrasto attraverso lendotelio capillare dipende sia dal coefciente di diffusione proprio del mezzo di contrasto che dal coefciente di diffusione di tutta la supercie di estensione fig . 
7a box e whiskers plots dei valori di ncbv calcolati nelledema 1 in pazienti affetti da glioma al tempo t0 e t1 , confrontati con i pazienti affetti da metastasi . 
b box e whiskers plots dei valori di nps nelledema 1 in pazienti affetti da glioma al tempo t0 e t1 , confrontati con i pazienti affetti da metastasi . mour or its progression [ 6 , 2830 ]  . 
in the pct literature , cbv is considered an accurate biomarker of the aggressiveness of neoplastic tissue , as it correlates with tumour grade [ 7 , 12 , 19 , 2835 ] and its progression to a worse grade [ 22 ] , but less is known about the real role of the ps coefcient . 
 there is a theoretical rationale [ 36 ] for a relationship between endothelial permeability and tumour grade , because high - grade tumours typically express increased levels of vascular endothelial growth factor ( vegf ) , which promotes endothelial proliferation and directly increases endothelial permeability . 
this can be evaluated by using a parameter radiol med ( 2013 ) 118 : 431443 called microvascular endothelial permeability surface area product ( ps ) , which characterises the spread of contrast from blood vessels into the interstitial space due to a decient or leaky bbb . 
the diffusion ux of contrast agent across the capillary endothelium depends on both the diffusion coefcient of the contrast agent and the total surface area of the water - lled pores of the capillary endotheliu ps is computed using the impulse residue function ( irf )  . 
the irf is used to estimate the rst - pass fraction of contrast agent that remains in the tissue the extraction fraction [ 21 ] which is related to the rate at which the contrast leaks out of the vasculature . 
in physiological terms , ps is the rate at which contrast agent ows into extravascular tissues and is related to the transfer constant ( another parameter of vascular leakage ) by : k - trans = ef where k - trans is the transfer ( which also has the same dimensions as ow ) constant . 
in normal cerebral vasculature , ps is negligible for all of the currently used contrast agents . we found that the perilesional density alteration revealed by ct , which corresponds to the perilesional hyperintensity in t2 - weighted and uid attenuated inversion recovery ( flair ) mr images , has different nps values from those of the vasogenic oedema surrounding a solid nodular metastasis . the role of cbv has been previously evaluated for the characterisation of neoplastic tissue , whereas our study focused on perilesional brain tissue . 
our ndings indicate that ncbv does not predict ultrastructural changes underlying the hypodense area , whereas nps ( that could be assumed nk - trans ) reveals differences between both the proximal and distal areas ( oedema 1 and oedema 2 ) and the vasogenic oedema surrounding a metastasis . 
these differences seem to be similar when analysed in the peri - enhancing tissue at t1 ( when tumour progression occurred ) and at t0 . another interesting result of our study is the decreasing values of nps in the perilesional tissue between oedema 1 and oedema 2 in glioma patients ( table 1 ) , which suggests the presence of a gradient of ultrastructural changes that diminish with their distance from the main lesion . 
on the other hand , the control group of patients with metastases showed a slightly increasing gradient from the nearest perilesional tissue to the distal nawm , which can be explained as a reduction in the physiological leakage of contrast in dei pori permeabili alle molecole dacqua dellendotelio capillare . 
lirf viene utilizzato per stimare la frazione di primo passaggio del mezzo di contrasto che rimane nel tessuto o frazione di estrazione [ 21 ] , correlata alla velocit con cui il mezzo di contrasto fuoriesce dal sistema vascolare attraverso la seguente relazione : e = 1 - e - ps / f dove ps la supercie di permeabilit ed f il usso . siccome il ps ha la stessa dimensione del usso , il rapporto ps / f adimensionale . 
in termini siologici il ps la velocit con cui il mezzo di contrasto uisce nellinterstizio extravascolare ed correlato al k - trans , altro parametro comunemente legato alla permeabilit vascolare , attraverso la seguente relazione : k - trans = ef da cui il k - trans presenta le stesse dimensioni del usso . 
in un tessuto cerebrale caratterizzato da normale vascolarizzazione il valore di ps sar quindi trascurabile . nel nostro studio abbiamo rilevato che lalterazione della densit perilesionale visibile in tc , che corrisponde alliperintensit nelle immagini uid attenuated inversion recovery ( flair ) e t2 pesate della rm , ha diverse caratteristiche in termini di nps rispetto alledema vasogenico circostante una metastasi solida nodulare . il ruolo del cbv stato gi valutato precedentemente per la caratterizzazione della lesione neoplastica , mentre il nostro studio focalizzato alla valutazione del tessuto cerebrale perilesionale . 
in particolare il calcolo dei dati ha rilevato che il ncbv non permette di rilevare le eventuali alterazioni ultrastrutturali allinterno dellipodensit peritumorale , mentre il nps ( considerato equivalente al k - trans ) in grado di fornire differenze statisticamente signicative sia nelle aree ipodense pi prossimali ( edema 1 ) che in quelle pi distali ( edema 2 ) in comparazione con i valori trovati nelle aree di ipodensit vasogenica perimetastatica . inoltre la differenza tra i valori di ps misurati nellarea di ipodensit peritumorale e nellarea di edema vasogenico perimetastatico appare maggiore quando viene calcolata nel tessuto circostante la porzione solida di enhancement al tempo t1 ( progressione di malattia ) rispetto al t0 , in accordo con una progressione a distanza della malattia nel tessuto nervoso perilesionale . 
daltra parte , nel gruppo di controllo dei pazienti affetti da metastasi , troviamo un gradiente lievemente crescente di nps andando dal tessuto perilesionale pi limitrofo verso quello pi distale sino alla nawm . 
questo pu essere spiegato come una riduzione della siologica permeabilit al mezzo di contrasto del tessuto cerebrale non neoplastico , dovuto alleffetto compressivo o effetto - massa indotto dalledema interstiziale sottostante ledema vasogenico . 442 radiol med ( 2013 ) 118 : 431443 nonneoplastic brain tissue due to the compressive or mass effect induced by the underlying interstitial oedema . conclusioni conclusions our results reect neuropathology ndings [ 37 , 38 ] , indicating that recurrence of a high - grade glioma often starts from neoplastic tissue not included in the surgical excision volume or radiation beam because it is not seen as enhancing tissue but it is hidden inside the perilesional oedema - like alteration . the main limitation of our study is the small number of patients ; this is because it was structured as a pilot study due to the slightly invasive technique involving the use of iodinated contrast media . pct can detect ultrastructural changes that could be included inside a treatment volume . 
the main drawback of this diagnostic technique is that it is not possible to cover the entire volume of the brain , even with 64 - row ct scanners , and so it is limited in evaluating bigger tumours or larger areas . 
on the other hand , ct scanners are widely available , and pct is faster than mr pwi . i nostri risultati riettono ci che conosciamo dalla neuropatologia [ 37 , 38 ] , cio che la recidiva dei gliomi ad alto grado spesso inizia da un tessuto neoplastico non incluso nel volume di escissione chirurgica o di radioterapia perch non caratterizzato da enhancement e nascosto nellipodensit perilesionale comunemente riferita ad edema . il limite del nostro studio lesiguo numero di pazienti principalmente perch stato strutturato come uno studio pilota in quanto la tecnica leggermente invasiva e necessita lutilizzo del mezzo di contrasto iodato . la tc perfusionale in grado di evidenziare le alterazioni ultrastrutturali che dovrebbero essere comprese in un volume di trattamento . 
il suo svantaggio principale che attualmente , anche con unapparecchiatura tc a 64 le di detettori , non possibile coprire lintero volume cerebrale ; lo studio quindi limitato alla valutazione di neoplasie e aree cerebrali di dimensioni limitate . 
catalano1 1department of radiological sciences , university of rome sapienza , viale regina elena 324 , 00161 rome , italy 2department of pediatrics , university of rome sapienza , viale regina elena 324 , 00161 rome , italy correspondence to : f . 
seventeen patients with middle lobe syndrome ( mean age 6.2 years ) underwent chest ct at the time of diagnosis ( 100 kv , care dose with quality reference of 70 mas ; collimation 241.2 mm ; rotation time 0.33 s ; scan time 5 s ) ; at follow - up after a mean of 15.3 months , all patients were evaluated with chest mr imaging with a respiratory - triggered t2 - weighted blade sequence ( tr 2 , 000 ; te 27 ms ; fov 400 mm ; ip angle 150 ; slice thickness 5 mm ) and chest x - ray . 
mr imaging and chest x - ray identied consolidations in 65% and 35% , bronchiectases in 35% and 29% , bronchial wall thickening in 59% and 6% and mucous plugging in 25% and 0% , respectively . 
 rm / rx hanno riportato , rispettivamente , consolidazioni : 65% / 35% ; bronchiectasie : 35% / 29% ; ispessimento delle radiol med ( 2013 ) 118 : 444455 conclusions . 
chest mr imaging might represent a feasible and radiation - free option for an overall assessment of the lung in the follow - up of patients with middle lobe syndrome . keywords middle lobe syndrome chest magnetic resonance imaging follow - up atelectasis pareti bronchiali : 59% / 6% ; mucous - plugging : 25% / 0% . 
lesame rx sembra sottostimare , in confronto alla rm , la frequenza di tali alterazioni nel corso del follow - up ; la rm polmonare pu rappresentare una metodica promettente e priva di radiazioni ionizzanti nel follow - up di questi pazienti . parole chiave sindrome del lobo medio risonanza magnetica polmonare follow - up atelettasia introduction introduzione middle lobe syndrome ( mls ) is a clinical condition typically seen in paediatric patients and characterised by chronic inammation of the middle lobe of the right lung ( as well as the lingula in some cases ) with recurrent bouts of pneumonia refractory to conventional treatment , leading to partial or complete atelectasis and changes to the affected airways [ 1 ]  . 
although no recognised guidelines exist for the assessment and follow - up of mls , the rst - line diagnostic tool is usually chest x - ray ( cxr ) , which is able to depict atelectasis or ill - dened consolidation in the middle lobe [ 6 ]  . 
la diagnosi di slm resa difcoltosa dalla aspecicit dei sintomi e dalla loro grande variabilit inter - individuale [ 24 ] ; per tali ragioni i casi di slm sono pi frequenti di quanto normalmente venga stimato ed attualmente non sono noti i precisi valori di incidenza e prevalenza della malattia . 
pur non esistendo attualmente delle linee guida riconosciute nella valutazione e nel follow - up della slm , lesame eseguito in prima istanza solitamente rappresentato dal radiogramma ( rx ) del torace , che pu dimostrare un quadro di atelettasia o di sfumato consolidamento a livello del lobo medio [ 6 ]  . 
 visti i complessi e variabili processi patogenetici alla base dellinstaurarsi della sindrome [ 7 , 8 ] ( anomalie anatomico - conformazionali delle vie aeree , stenosi estrinseche o intrinseche , presenza di corpi estranei , possibile presenza di altri reperti patologici localizzati in altre sedi ) lesame in tomograa computerizzata ( tc ) del torace normalmente richiesto per confermare la diagnosi e studiare lesatto grado di severit ed estensione delle alterazioni parenchimali e a carico delle vie aeree , informazioni che non possono essere adeguatamente fornite dallesame rx standard [ 1 , 9 ]  . 
 owing to the chronic course and insidiousness of the clinical and pathological features of mls , patients are subjected to a large number of examinations ( ct and cxr ) both for diagnosis and follow - up during treatment . 
the risks due to radiation exposure , especially as regards ct examination , have been signicantly limited in both adults and children by the application of new low - dose chest ct protocols [ 13 ]  . 
however , considering the chronic course of the disease and the long life expectancy of the patient , exposure to radiological examinations should be limited as far as possible , with careful evaluation of risks and benets for each patient . 
the largest study reported in the literature on the application of chest mr imaging in children was conducted on patients affected by cystic brosis ( cf ) [ 14 , 15 ]  . 
as is known , mr imaging has advantages and disadvantages : the former include the possibility of modulating the intrinsic contrast of organs to obtain accurate characterisation of diseased tissues ; on the other hand , chest mr imaging has limited spatial resolution in comparison with ct . the purpose of our study was to evaluate the most common lung changes and their location reported on ct at the time of mls diagnosis and to assess the possible role of chest mr imaging in the long - term follow - up of these changes compared with cxr . materials and methods patient population and informed consent the study was conducted after receiving the approval of the local ethics committee . 
 proprio per il decorso cronico ed il carattere subdolo che la sindrome presenta nella sua espressione clinico - patologica , i pazienti affetti vengono sottoposti ad un alto numero di esami radiologici ( tc ed rx ) , necessari sia per la diagnosi , che per il follow - up in corso di terapia . 
il rischio legato allesposizione alle radiazioni ionizzanti , specialmente in tc , si notevolmente ridotto negli ultimi anni , sia per la popolazione adulta che per quella pediatrica , con lapplicazione di nuovi protocolli tc del torace a basso dosaggio [ 13 ]  . 
in virt del decorso cronico e dellalta aspettativa di vita di questi pazienti , tuttavia auspicabile ridurre il pi possibile lesposizione ad esami radiologici , effettuando una attenta valutazione rischio / benecio per ogni paziente . 
la pi vasta esperienza riportata in letteratura sullapplicazione della rm polmonare in et pediatrica riguarda la valutazione di pazienti affetti da brosi cistica ( fc ) [ 14 , 15 ]  . 
la rm presenta , come noto , dei vantaggi e degli svantaggi : tra i primi la possibilit di modulare il contrasto intrinseco degli organi , permettendo unaccurata caratterizzazione tissutale in quadri patologici ; di contro , la rm polmonare , rispetto alla tc , presenta il principale limite di una limitata risoluzione spaziale . lo scopo di questo studio stato quello di valutare quali sono le alterazioni polmonari pi frequenti nella slm e la loro localizzazione al momento della diagnosi con esame tc e valutare il possibile ruolo della rm polmonare nel follow - up a distanza di tali alterazioni in confronto con lrx . materiali e metodi popolazione dei pazienti e consenso informato lo studio stato condotto dopo lapprovazione del comitato etico locale . 
tutti i pazienti , o i loro tutori legali , hanno sottoscritto un consenso informato prima dellinclusione nello studio e sono stati informati sulle modalit di esecuradiol med ( 2013 ) 118 : 444455 ct protocol before ct acquisition , each patient was instructed to take a deep breath and hold it for an adequate length of time ; ct was performed at the end of a deep inspiration . 
highresolution ct images were acquired from the lung apices to the upper abdomen during a single breath - hold using a spiral 64 - detector - row ct scanner ( volume sensation cardiac , siemens , erlangen , germany )  . 
parameters were 100 kv , care dose with quality reference at 70 mas ; collimation 241.2 mm ; rotation time 0.33 s ; scanning time 5 s ; reconstruction kernels b30 ( mediastinum ) and b60 ( lung parenchyma )  . 
let media dei pazienti al momento della diagnosi e dellesecuzione dellesame tc era di 6 , 2 anni ( 2 , 1 )  . nellarco temporale compreso tra settembre 2008 e febbraio 2011 , secondo indicazione del clinico , tutti i pazienti sono stati richiamati per una valutazione di follow - up con esecuzione di un esame rx e di un esame di rm del polmone , effettuati con una distanza temporale massima di 3 giorni ( 1 )  . 
il tempo medio intercorso tra lesame tc e gli esami rx ed rm , variabile da paziente a paziente , era di 15 , 3 mesi ( 5 , 1 )  . 
dopo il primo controllo rm , due pazienti hanno eseguito ulteriori controlli di follow - up con rm . mr imaging protocol protocollo tc all mr examinations were performed with a 1.5 - t device ( magnetom avanto , siemens , erlangen , germany ) using t2 - weighted blade ( motion correction with radial blades ) sequences with navigator - based respiratory gating ( tr 2 , 000 ; te 27 ms ; fov 400 mm ; ip angle 150 ; slice 5 mm ) acquired in axial and coronal planes . 
a combination of two surface coils was used to cover the entire chest and the spine . cxr protocol image evaluation cxr examination was performed in two projections [ posteroanterior ( pa ) and laterolateral ( ll ) ] , in agreement with the european community commission guidelines [ 19 ]  . all studies were anonymised and sent to a picture archiving and communication system ( pacs ) workstation for image evaluation . 
the observers were blinded to patients clinical information and results of the other studies . each study ( ct , mri , cxr ) was assessed for the presence of pathological changes : consolidations , bronchiectases , bronchial wall thickening , mucous plugging . 
le immagini tc ad alta risoluzione sono state acquisite con uno scanner tc spirale a 64 detettori ( volume sensation cardiac , siemens , erlangen , germania ) , senza iniezione di mezzo di contrasto , in una singola apnea dagli apici polmonari no alladdome superiore . i parametri utilizzati per la scansione sono stati : 100 kv , care dose con riferimento di qualit a 70 mas ; collimazione : 241 , 2 mm ; tempo di rotazione : 0 , 33 s ; tempo di scansione : 5 s ; ricostruzioni kernel : b30 ( valutazione del mediastino ) e b60 ( valutazione del parenchima polmonare )  . 
il dose length product ( dlp , calcolato in mgy / cm2 ) e dose efcace ( calcolati in msv ) sono stati registrati per ogni esame . protocollo rm ogni studio rm stato effettuato con unapparecchiatura 1 , 5 t ( magnetom avanto , siemens , enlargen , germania ) con sequenze t2 pesate blade ( motion correction with radial blades ) sincronizzate con gli atti del respiro tramite navigatore [ tempo di ripetizione ( tr ) : 2000 ; tempo di eco ( te ) : 27 ms ; campo di vista ( fov ) : 400 mm ; ip angle : 150 ; strato : 5 mm ] acquisite sul piano assiale e coronale . 
 stata utilizzata una combinazione di due bobine di supercie al ne di coprire tutto il torace e la spina dorsale . protocollo rx lo studio rx stato eseguito in due proiezioni [ postero - an448 radiol med ( 2013 ) 118 : 444455 teriore ( pa ) e latero - laterale ( ll ) ] , secondo le linee guida della european community commission [ 19 ]  . valutazione degli studi tutti gli studi sono stati resi anonimi ed inviati ad una workstation con picture archiving and communication system ( pacs ) per la valutazione delle immagini . 
gli osservatori al momento della valutazione non erano a conoscenza delle informazioni cliniche dei pazienti e dei risultati delle altre metodiche . ogni studio ( tc , rm , rx ) stato valutato per la presenza di alcune alterazioni patologiche : consolidazioni , bronchiectasie , ispessimento delle pareti bronchiali e mucous plugging . 
ciascuna categoria patologica stata valutata secondo le denizioni precedentemente riportate in un sistema di scoring internazionalmente convalidato per le alterazioni polmonari nei pazienti affetti da fc [ 20 ]  . 
tutte le alterazioni sono state valutate secondo un criterio topograco di suddivisione per lobi ; nel caso della valutazione di aree di consolidazione , per il lobo medio stata effettuata una differenziazione tra interessamento lobare completo o parziale ( segmento mediale o laterale )  . 
1 il graco mostra la distribuzione lobare delle alterazioni polmonari riscontrate allesame tc di base per tutte le categorie considerate ( i valori numerici sono espressi in percentuale )  . 
changes identied and their location on each modality were entered into an electronic database ( microsoft excel 2008 for macintosh , microsoft , redmond , wa , usa ) for statistical analysis . results image acquisition risultati acquisizione degli studi mean scanning time for mr imaging was 6 ( range 48 ) min in the axial plane and 4 ( range 37 ) min in the coronal plane ; overall scanning time , including the time for patient preparation , was 14 ( range 1017 ) min on average , depending on patient size and level of cooperation in breath - holding . 
la mediadeviazione standard del dlp stata 10621mgy / cm2 , la dose efcace stata di 1 , 50 , 5 msv . location and frequency of lung abnormalities identied at baseline ct examination are reported in figs . 
overall , the middle lobe was most frequently involved , followed valutazione dei casi alla diagnosi : esame tc le localizzazioni e la frequenza delle alterazioni polmonaradiol med ( 2013 ) 118 : 444455 mucous plugging consolidation bronchial wall thickening bronchiectasis fig . 
lalterazione pi frequente al momento della diagnosi la consolidazione presente nella totalit dei pazienti seguita dallispessimento delle pareti bronchiali , dal mucous plugging e dalle bronchiectasie . by the lingula and the left lower lobe to the same extent , by the right lower and upper lobes and by the left upper lobe . 
bronchial wall thickening was reported in nine patients ( 53% ) , with most frequent location at the middle lobe ( 47% )  . consolidations were detected in all patients ( 100% ) , with location at the middle lobe in 14 ( 84% of cases ) , of whom nine ( 64% ) had widespread consolidation , two ( 14% ) only at the level of the lateral segment and three ( 21% ) only at the level of the medial segment . 
ct studies identied lymphadenopathy in 11 patients ( 64% ) , 58% with right hilar location . follow - up assessment : cxr and mr imaging results of ct examinations , as compared with follow - up mr imaging and cxr , are reported in figure 3 . 
detection of bronchiectasis on mr imaging remained unchanged compared with baseline ct , with six patients ( 35% ) showing bronchiectasis ( most frequently located at the level of the middle lobe )  . 
on cxr , bronchiectasis was reported in ve patients ( 29% )  . bronchial wall thickening was seen in ten patients ( 59% ) on mr imaging ( mostly at the middle lobe ) , thus showing a ri riscontrate allesame tc di diagnosi sono riportate nei graci nelle figure 1 e 2 . 
nel complesso , il lobo interessato pi frequentemente stato il lobo medio , seguito dalla lingula e dal lobo inferiore sinistro in egual misura , dal lobo inferiore e superiore di destra e dal lobo superiore sinistro . 
 lo studio tc ha riportato la presenza di bronchiectasie in un totale di 6 pazienti ( 35% ) ; la sede principale di localizzazione risultata il lobo medio ( 24% dei casi )  . 
stato riportato ispessimento delle pareti bronchiali in un totale di 9 pazienti ( 53% ) , con sede principale di localizzazione a livello del lobo medio ( 47% )  . consolidazioni sono state riscontrate in tutti i pazienti ( 100% ) , con localizzazione a livello del lobo medio in 14 pazienti ( 84% dei casi ) , di cui in 9 pazienti ( 64% ) completa , in 2 ( 14% ) solo a livello del segmento laterale ed in 3 ( 21% ) solo a livello del segmento mediale . 
il riscontro delle bronchiectasie in rm rimasto invariato rispetto alla tc di base , con un totale di 6 pazienti ( 35% ) interessati ( con localizzazione principale a livello del lobo medio )  . 
in rx sono state riportate bronchiectasie in 5 pazienti ( 29% )  . ispessimento delle pareti bronchiali stato riscontrato in 10 pazienti ( 59% ) in rm ( localizzazione principale nel lobo medio ) , dimostrando una progressione rispetto alla tc di base ; in rx stato individuato un solo paziente ( 6% ) con ispessimento delle pareti bronchiali . 
in rx stata evidenziata atelettasia in 6 pazienti ( 35% ) , di cui completa in 4 ( 66% ) , del segmento mediale in 1 ( 9% ) e del segmento laterale in 1 ( 9% )  . 
mucous plugging stato riscontrato in 4 pazienti ( 25% ) in rm ( riduzione rispetto al precedente esame tc ) con localizzazione principale a livello del lobo medio , ed in nessun paziente in rx . 
nei due pazienti che hanno eseguito ulteriori follow - up con rm , gli studi hanno evidenziato una progressiva riduzione delle450 radiol med ( 2013 ) 118 : 444455 bronchiectasis consolidations x - ray x - ray bronchial wall thickening mucous plugging x - ray x - ray fig . 
3 i graci mostrano , per ogni singola alterazione valutata , la frequenza di riscontro allesame tc di base ed agli esami rm ed rx di follow - up ; i dati sono espressi in percentuale . 
cxr identied atelectasis in six patients ( 35% ) ; this was complete in four ( 66% ) and involved the medial segment alone in one ( 9% ) and the lateral segment in one ( 9% )  . 
mucous plugging was identied in four patients ( 25% ) on mr imaging ( fewer than on previous ct ) , mostly located at the middle lobe level , and in none of the patients on cxr . 
the two patients who underwent additional follow - up mr imaging showed a progressive dediscussione la slm un quadro clinico dellet pediatrica caratterizzato da decorso subdolo e da una grande variabilit ed aspecicit del corteo sintomatologico . 
le alterazioni patologiche riscontrate con le metodiche di imaging sono espressione di un insulto inammatorio cronico a carico delle vie aeree , che si estrinseca con quadri di diversa gravit . lalterazione pi caratteristica rappresentata dalla presenza di consolidazioni a carattere atelettasico ( con estensione lobare completa o incompleta ) del lobo medio ( meno frequentemente della lingula ) ; linsulto inammatorio cronico generato da episodi bronco - pneumonici recidiradiol med ( 2013 ) 118 : 444455 fig . 
5a - c la tc di base ( a ) mostra la presenza di una circoscritta area di atelettasia localizzata a livello del lobo medio , in sede para - cardiaca . 
le esperienze riportate su questa categoria di pazienti dimostrano una grande variabilit nellapproccio diagnostico con metodiche radiologiche , indicando alcuni il solo esame radiol med ( 2013 ) 118 : 444455 452 fig . 
6a - c studi di follow - up in uno dei due pazienti sottoposti ad ulteriori controlli con esame rm : gli studi dimostrano una progressiva riduzione , no alla pressoch completa risoluzione ( b , c ) , nellarco di 12 mesi , dellarea di atelettasia in sede lobare media ( a )  . widely variable and nonspecic symptoms . 
the pathological abnormalities identied on diagnostic imaging reect chronic airway inammation of varying severity . the most typical abnormality is atelectatic consolidations ( with complete or incomplete lobar involvement ) at the middle lobe ( less frequently at the lingula ) ; chronic inammation produced by recurrent bouts of bronchopneumonia may lead to irreversible airway damage , with the onset of bronchiectasis . 
the workup of these patients varies widely in the modalities used for the diagnostic approach , with some indicating that cxr alone is adequate for both diagnosis and follow - up and others highlighting the importance of ct at diagnosis [ 1 , 2 , 21 , 22 ]  . 
 results of our study , based on ct examination obtained at diagnosis , as well as those from previous international studies demonstrate that a signicant number of patients have lung parenchymal and airway abnormalities ( bronchial wall thickening , bronchiectasis , mucous plugging ) that form a more diversied and complex pathological pattern compared with middle lobe atelectasis alone [ 23 ]  . 
in the light of these considerations and on account of the tendency of mls symptoms to become chronic and cyclic , patients with this syndrome need to be followed rx come sufciente sia al momento della diagnosi che nel follow - up , altri , enfatizzando limportanza della tc al momento della diagnosi [ 1 , 2 , 21 , 22 ]  . 
 i nostri risultati derivati dallo studio tc eseguito alla diagnosi , insieme a quelli derivati da studi internazionali precedentemente riportati , hanno dimostrato , in una signicativa quota di pazienti , la presenza di alterazioni polmonari parenchimali ed a carico delle vie aeree ( ispessimento delle pareti bronchiali , bronchiectasie , mucous plugging ) che vanno a comporre un quadro patologico pi variegato e complesso rispetto alla presenza isolata dellatelettasia lobare media [ 23 ]  . 
alla luce di queste considerazioni e per la tendenza intrinseca alla cronicizzazione e ciclicit del quadro sintomatologico che caratterizzano la slm , i pazienti affetti da tale sindrome necessitano di un adeguato followup per lunghi periodi di tempo con metodiche di imaging che permettano una accurata valutazione di tutte le alterazioni polmonari potenzialmente presenti . 
 [ 1 ] mette in luce limportanza della tc nel follow - up dei pazienti affetti da slm e lafdabilit di questa metodica nellindividuazione di aree atelettasiche a livello lobare medio . 
 il follow - up con esame tc del torace condurrebbe tuttavia alla somministrazione di una dose di radiazioni ionizzanti nel tempo non trascurabile , considerata la lunga aspettativa di vita di questi pazienti ( pressoch sovrapponibile alla popolazione sana di pari et ) [ 24 ]  . 
 [ 1 ] emphasised the importance of ct in the follow - up of patients with mls and the reliability of this method in identifying areas of atelectasis at the level of the middle lobe . 
however , follow - up with chest ct would involve exposure to signicant doses of ionising radiation over time , in consideration of the long life expectancy of these patients ( almost equivalent to that of the healthy population of the same age ) [ 24 ]  . in 1995 , de boeck et al . 
despite the signicantly lower level of accuracy compared with ct , conventional cxr has been traditionally used in the follow - up of patients with mls on account of the good compromise between low radiation dose delivered and diagnostic information obtained , in particular in cases of acute exacerbation of disease ( short - term follow - up of foci of bronchopneumonia )  . 
 in our study , mr imaging was performed in addition to cxr to evaluate the diagnostic potential of the two modalities for the follow - up of patients with mls , compared with ct examination performed at diagnosis . 
most investigations into using chest mr imaging have been conducted on patients with cf [ 14 , 15 ] , and no published study has looked into its possible role for evaluating patients with mls . 
at that time , however , mr imaging of the lung had many limitations , in particular as a result of : ( 1 ) signal loss caused by physiological motion ( cardiac and respiratory motion of the diaphragm and chest wall ) ; ( 2 ) low proton density and low signal - to - noise ratio ( snr ) caused by the small amount of lung tissue . 
firstly , the signal loss caused by cardiac and respiratory motion may be compensated for by using fast sequences acquired during breath - holding or with cardiac and respiratory gating . 
in addition , the lack of information due to early signal loss may be overcome by using sequences with short tr and te , which help to maintain a higher signal before its decay [ 14 ]  . 
the reason underlying the use of different sequences was to nd a compromise between the rapid signal loss in the lung parenchyma and susceptibility effects ; this has led to improvements in gradient echo ( gre ) and turbo spin - echo ( tse ) sequences [ 27 , 28 ]  . 
nonostante il grado di accuratezza signicativamente inferiore rispetto alla tc , lo studio con rx del torace standard stato quindi tradizionalmente adottato nel follow - up dei pazienti affetti da slm a fronte del buon compromesso tra le basse dosi di radiazioni somministrate e le informazioni diagnostiche derivate , soprattutto in caso di acutizzazioni ( follow - up a breve termine di focolai bronco - pneumonici )  . 
 nel nostro studio abbiamo afancato allesame rx anche un esame rm del torace , confrontandone le potenzialit diagnostiche nel follow - up di un gruppo di pazienti con slm al confronto con un precedente esame tc effettuato al momento della diagnosi . 
in quel periodo la rm nello studio del parenchima polmonare riportava per molti limiti , principalmente legati a : ( 1 ) perdita di segnale dovuta al movimento siologico ( battito cardiaco e movimento respiratorio del diaframma e della parete toracica ) ; ( 2 ) bassa densit protonica e basso rapporto segnale - rumore ( snr ) a causa della scarsa quantit di tessuto polmonare . 
in primo luogo , la perdita del segnale causata dal movimento cardiaco e respiratorio pu essere compensata mediante lutilizzo di sequenze rapide acquisite in apnea o con sincronizzazione cardiaca e con gli atti respiratori . 
in secondo luogo , la carenza di informazioni derivata dal precoce decadimento del segnale del parenchima polmonare pu essere superata usando sequenze con tr e te brevi , che possono mantenere pi alto il segnale prima del suo decadimento [ 14 ]  . 
la ragione alla base dellutilizzo di diverse sequenze stata quella di trovare un compromesso tra il rapido decadimento dellintensit di segnale del parenchima polmonare e gli effetti di suscettibilit ; cos nel corso del tempo sono stati proposti diversi miglioramenti nelle sequenze gradient - echo e turbo spin echo ( tse ) [ 27 , 28 ]  . 
pi di recente , sequenze half - fourier acquisition single - shot turbo spin - echo ( haste ) sono state applicate in diversi centri ottenendo alta qualit diagnostica e riduzione degli artefatti [ 25 , 29 ] , con tempi di acquisizione sempre pi rapidi , che hanno reso questa sequenza meno sensibile anche ai movimenti respiratori e cardiaci . nel nostro studio , stata scelta solo la sequenza blade per limaging polmonare , in quanto : ( 1 ) una sequenza che 454 radiol med ( 2013 ) 118 : 444455 high diagnostic quality and fewer artefacts [ 25 , 29 ] with increasingly faster acquisition times , which have made this sequence less susceptible to respiratory and cardiac motion . in our study , lung imaging was performed with blade sequences alone because : ( 1 ) they are characterised by few respiratory motion artefacts , and ( 2 ) their radial sampling of the k - space leads to signicantly sharper images , even in poorly cooperative patients [ 16 , 17 ]  . 
 a recent study addressed the value of chest mr imaging with blade sequences in comparison with ct in adult patients affected by primary immune deciencies with lung parenchymal involvement ; the study reported almost identical results between the two modalities in moderate to advanced disease and slightly inferior results for mr imaging in mild disease [ 30 ]  . 
the most signicant results were achieved in bronchial wall thickening ( an indicator of airway inammation ) , residual areas of atelectasis and mucous plugging , which cxr failed to detect in all patients . 
in the two patients who underwent additional mr imaging during the follow - up , a progressive decrease in the extent of middle lobar atelectasis was demonstrated . in conclusion , on the basis of our preliminary experience , chest mr imaging appears to be a valuable and promising method for the follow - up of patients with mls . 
the main limitation of our study , however , is the long time interval between baseline ct and follow - up mr imaging , which prevented a reliable assessment of diagnostic accuracy of chest mr imaging compared with ct in patients with mls . 
 further studies on larger patient populations are needed to obtain a direct comparison between ct and mr performed at the same time in order to establish the exact sensitivity and specicity of mr imaging in studying patients with mls . mostra pochi artefatti causati da movimenti respiratori ; ( 2 ) ha una lettura radiale dello spazio k che si traduce in immagini molto pi nitide , anche in pazienti scarsamente collaboranti [ 16 , 17 ]  . 
uno studio recentemente riportato in letteratura ha valutato la validit della rm polmonare con sequenze blade in un confronto diretto con lesame tc ; lo studio , effettuato su pazienti adulti affetti da immunodecienze primitive con coinvolgimento patologico del parenchima polmonare , ha riportato risultati pressoch sovrapponibili tra le due metodiche in quadri di malattia moderata / avanzata e performance lievemente inferiori per la rm in quadri di coinvolgimento patologico lieve [ 30 ]  . 
 i nostri risultati hanno dimostrato la validit della rm polmonare nella ricerca di quattro principali alterazioni patologiche ( consolidazioni , ispessimento delle pareti bronchiali , bronchiectasie e mucous plugging )  . 
i risultati pi signicativi si sono avuti nella ricerca dellispessimento delle pareti bronchiali ( indice di attivit di ogosi delle vie aeree ) , di aree atelettasiche residue e nella visualizzazione del mucous plugging , riportato dallrx in nessun paziente . 
 la rm ha inoltre permesso la valutazione della presenza di linfoadenopatie in sede ilare e mediastinica , riportando una riduzione della loro frequenza nellesame di follow - up rispetto alla tc desordio . 
nei due pazienti che hanno effettuato ulteriori controlli con rm nel tempo , stata riscontrata una progressiva riduzione dellestensione dellarea di atelettasia riscontrata in sede lobare media . in conclusione , sulla base della nostra esperienza preliminare , la rm polmonare sembra rappresentare una metodica valida e molto promettente nella valutazione di followup dei pazienti affetti da slm . 
il limite principale di questo studio rappresentato , tuttavia , dal signicativo lasso di tempo intercorso tra lesecuzione dellesame tc di diagnosi e lesame rm di follow - up : questo non ha permesso di eseguire una effettiva valutazione del grado di accuratezza diagnostica della rm polmonare rispetto allesame tc nei pazienti affetti da slm . 
knauth springer - verlag berlin heidelberg , 2012 issn : 0942 - 5373 isbn : 0978 - 3 - 642 - 12455 - 6 e - isbn : 978 - 3 - 642 - 12456 - 3 published online : 16 march 2013 springer - verlag 2013 the aim of this 352 page book was to review , study and present in their variety all disease types and pathologic conditions affecting the scrotuaccordingly , this is a truly comprehensive book , presenting the results of long - standing cooperation between radiologists , urologists and paediatric surgeons working in the eld from italy and around the world . 
 the patients clinical history is emphasized and physical examination of the scrotum is the rst diagnostic step , followed by ultrasound ( us ) and sometimes magnetic resonance imaging ( mri ) , rarely by nuclear medicine and contrast - enhanced us studies . 
clinical presentation followed by imaging , management and end - results is quite useful and gives the reader a comprehensive , exhaustive and precise spectrum of the presented and discussed topic , illustrated by very beautiful images . the editors of this book should be praised not only for the book as a whole but for the very precise and useful abbreviation list to be found at the beginning of the book and the comprehensive index at its end . scopo di questo volume di 352 pagine stato quello di rivedere , studiare e presentare in tutte le sue variet ogni possibile tipo di malattia ed affezione patologica dello scroto . 
 ne deriva , come conseguenza , un testo veramente completo che presenta i risultati di lungo e fruttuoso lavoro di cooperazione tra radiologi , urologi e chirurghi pediatri che si occupano del problema in italia e nel mondo . grande enfasi posta sulla storia clinica del paziente e sullesame sico dello scroto , quali primi passi nelliter diagnostico , seguiti dallecograa , talvolta dalla risonanza magnetica ( rm ) e raramente dalla medicina nucleare e dallecograa con contrasto . 
 dopo i capitoli di apertura in cui sono trattate la strumentazione ecograca e di rm e lanatomia dello scroto , il lettore ne trover altri 29 dedicati sia alla precisa valutazione clinica delle malattie dello scroto delladulto e del bambino , quali trauma , dolore scrotale acuto , tumefazioni scrotali tumori , cisti , infertilit maschile in tutte le sue possibili varianti ( presentazione molto precisa ed approfondita , interessante pi landrologo che il radiologo ) , testicolo ritenuto , reperti occasionali calcicazioni e quadri miscellanei , che al loro quadro per immagini ed al trattamento e conseguente risultato , tutti descritti in grande dettaglio . i capitoli sono impostati in modo tale che la presentazione clinica ( seguita da immagini , trattamento e risultato nale ) risulta assai utile , dando al lettore un quadro esauriente , completo e preciso dellargomento trattato , illustrato anche da immagini molto belle . i curatori del volume devono essere lodati non solo per il volume nel suo complesso , ma anche per lassai preciso ed utile iniziale elenco delle abbreviazioni e per laccurato indice nale . radiol med ( 2013 ) 118 : 14241425 1425 due to its content , this book should be considered a pace - setter in the eld , giving radiologists , urologists , andrologists , paediatric surgeons and paediatricians a very handy instrument ( a compliment to italian radiology ) in their daily practice in this difcult and consequential eld . dato il suo contenuto , questo volume pu essere considerato di primo piano e fondamentale in questo campo , offrendo a radiologi , urologi , andrologi , chirurghi pediatri e pediatri uno strumento assai utile ( un omaggio alla radiologia italiana ! ) nella loro pratica quotiana in questo campo difcile ed importante . 
nel 42% dei pazienti reclutati non si potuta utilizzare labi ( nel 9 , 34% non era rilevabile un polso arterioso e nel 14 , 02% larteria non era comprimibile ) oppure si rivelato inesatto ( nel 18 , 7% prima e nel 15 , 9% dopo la realizzazione della pta )  . 
labi mostra limiti significativi nella diagnosi e nel trattamento dei pazienti con cli rispetto alla tcpo2 . 1374 radiol med ( 2013 ) 118 : 13731378 keywords peripheral transluminal angioplasty peripheral arterial occlusive disease transcutaneous oxygen pressure revascularization reperfusion parole chiave angioplastica translumninale periferica malattia occlusiva eriferica arteriosa tensione transcutanea di ossigeno rivascolarizzazione riperfusione introduction critical limb ischaemia ( cli ) is commonly defined as the presence of chronic ischaemic pain at rest , ulcer or gangrene in the foot that is attributable to objectively proven peripheral arterial occlusive disease ( paod ) [ 1 , 2 ]  . 
however , this index can only be determined in large arteries and not in nonpalpable lowflow arteries ; it is also unsuitable for patients with calcified ( noncompressible ) arteries . 
these handicaps frequently occur in diabetic patients and prevent reliable ankle - pressure measurements [ 47 ]  . studies on microcirculation continue to increase as attempts are made to obtain an imaging diagnosis together with a functional assessment of tissue . 
an increase in tcpo2 in patients following peripheral transluminal angioplasty ( pta ) reflects the physiological significance of microvascular revascularisation achieved in the treated limb and serves to assess functional improvement in tissue oxygenation obtained with pta . 
 the objective of this study was to evaluate the limitations of abi in revascularisation of diabetic patients with cli undergoing pta treatment compared with the degree of arterial stenosis and tcpo2 . materials and methods from 1 july 2008 to 30 november 2011 , 250 consecutive patients with limb ischaemia who were sent to the vascular radiology service for clinical evaluation and diagnostic tests [ arteriography and / or computed tomography angiography ( cta ) and abi ] were examined for suitability for pta . 
all were evaluated for signs of posterior tibial and dorsalis pedis signals ; abi was measured by the doppler continuous - wave technique , and tcpo2 was measured on the dorsum of the foot . 
duplex scanning was performed in cases with reduced or absent foot signal , abi < 0.90 ( in the absence of arterial calcification ) or tcpo2 < 50 mmhg ( in the absence of oedema )  . 
 abi was measured using a 12 - cm sphygmomanometer cuff placed just above the ankle , and a doppler instrument with an 8 mhz frequency ( multi - dopplex ii huntleigh healthcare limited , cardiff , uk ) was used to measure systolic pressure of the posterior tibial and dorsal pedal arteries of each leg . 
these pressures were then normalised with the higher brachial pressure of either arm to determine abi . tcpo2 measurements in the diabetic limb were taken upon hospital admission and reassessed 1 day after pta . 
 tcpo2 measurements were taken on the dorsum of the foot with the patient resting in the supine position in an air - conditioned room maintained at 22c and with the electrode at 44c . 
 statistical analysis statistical analysis compared preand post - treatment results by the equality of means for paired data using paired radiol med ( 2013 ) 118 : 13731378 1375 table 1 demographic and clinical characteristics of study population ( n = 104 )  . 
data are percent or mean1 standard deviation tasc , inter - society consensus for the management of peripheral artery disease ; tcpo2 , transcutaneous oxygen tension tabella 1 caratteristiche demografiche e cliniche della popolazione studiata ( n = 104 )  . 
results were considered significant with a p value < 0.01. results in 181 ( 72.4% ) of the 250 consecutive patients with limb ischaemia admitted to our vascular radiology service , at least one pedal pulse was absent , abi was < 0.90 ( in the absence of arterial calcification ) , tcpo2 was < 50 mmhg and / or duplex scanning showed evidence of significant stenosis . 
these 114 patients were referred for an angiographic or cta study , and in 136 limbs , the presence of a stenotic narrowing > 50% of the vessel lumen in at least one artery of the ischaemic limb was observed . 
abi was not measurable in 25 limbs ( 23.36% , 25 / 107 ) because of the absence of both tibial signals in ten patients ( 9.34% , 10 / 107 ) or the presence of arterial calcifications in 15 ( 14.02% , 15 / 107 )  . 
 after pta , abi was not measurable in 17 patients ( 15.90% , 17 / 107 ) because of the absence of an arterial signal in three ( 2.80% , 3 / 107 ) or the presence of arterial calcifications in 14 ( 13.08% , 14 / 107 )  . 1376 radiol med ( 2013 ) 118 : 13731378 fig . 
2 stenosi nei pazienti con abi > 0 , 91 ( prima e dopo pta ; il numero identifica ciascun paziente , permettendo di monitorare il cambiamento )  . abi could be determined in 82 cases ( 76.63% ) : 20 cases ( 18.7% , 20 / 107 ) displayed a normal abi with serious arterial stenosis or a very low tcpo2 , which justified carrying out pta , the results of which are shown in figures 1 and 2 ( initially , each case was assigned a number to facilitate follow - up on the charts before and after treatment )  . 
 in 42% of patients , abi was erroneous or could not be used : in 23.36% because it was impossible to determine abi ( no signal or the artery could not be compressed ) ; in 18.7% , a false negative was obtained ( a normal abi but with high levels of arterial stenosis and / or a low tcpo2 )  . statistical analysis revealed minimal correlation between techniques ( tcpo2 and abi ) ( r = 0.14 ; p < 0.199 ) , which means that both indices show a relationship conditioned by the patients improvement rather than by any true correspondence between parameters . discussion radiologists use abi to evaluate pta . 
however , even if arterial stenosis is considerably reduced and abi is normal , it is not possible to know whether the blood flow in the treated limb has increased . 
 radiol med ( 2013 ) 118 : 13731378 1377 however , abi can only be determined in large - artery trunks and not in nonpalpable , low - flow arteries ; it is also unsuitable for patients with calcified ( noncompressible ) arteries . 
as shown in our study results , it was impossible to determine abi before pta in 23.36% of patients ( in 9.34% because of the lack of a signal , and in 14.02% because of an arterial calcification )  . 
however , in all these patients , it was possible to measure tcpo2 without difficulty before and after pta . our results show that an abi > 0.9 does not rule out cli , stenosis > 50 % or tcpo2 > 30 mmhg . 
this may be the key reason abi does not always reliably predict the magnitude of the cli [ 10 , 16 , 17 ]  . for this reason , the inter - society consensus for the management of peripheral artery disease ( tasc ) 2000 proposed a range of 3050 mmhg as a level of moderate ischaemia . 
these findings confirm that abi is not related to microcirculation of the treated limb . the study presented here shows that an increase in tcpo2 over pretreatment values in the same patient demonstrates the effectiveness of pta in revascularisation . 
for this reason , we propose the use of tcpo2 as an indicator of reperfusion achieved through pta . a limitation of this study is that none of the three parameters analysed ( abi , tcpo2 or arteriography ) provides a clinical prediction of limb salvage . 
 we are carrying out clinical monitoring to assess which of diagnostic method correlates best with limb salvage . conclusions abi shows significant limitations in diagnosing and treating cli patients compared with tcpo2 . 
orsola - malpighi , via massarenti 9 , 40128 bologna , italy 2department of clinical sciences , section of radiological sciences , university of parma , via gramsci 14 , 43100 parma , italy corrispondence to : d . 
ninety - seven patients with a total of 146 subsolid nodules [ 140 pure ground - glass opacities ( pggos ) and six mixed ground - glass opacities ( mggos ) ] were retrospectively recruited . 
two chest radiologists independently reviewed the hrct features of the nodules ( location , shape , size , density ) and the patients clinical characteristics ( sex , age , smoking and cancer history )  . 
an increase in size and / or density was seen in 32% of ssn , and in particular in partly solid ( mggos ) , large ( 10 mm ) and irregular nodules . 
ssn growth was more frequent in patients with advanced age and a history of smoking , and occurred even after a long period of stability ( 39% of pggos changed over 3 years )  . 
the observation of a sample of cancer patients has shown that ssn may frequently grow in size and / or density in these patients , especially if associated riassunto obiettivo . 
sono stati reclutati in maniera retrospettiva 97 pazienti , per un totale di 146 nss ( 140 ground glass puri pggo , e 6 ground glass misti mggo )  . 
le caratteristiche hrct dei noduli ( localizzazione , forma , dimensioni , densit ) e quelle cliniche dei pazienti ( sesso , et , abitudine al fumo e anamnesi oncologica ) sono state valutate indipendentemente da due radiologi toracici . 
durante il follow - up il 58% dei nss rimasto invariato , il 10% scomparso , mentre in circa un terzo dei casi ( 32% ) si vericato un aumento di dimensioni e / o densit , specialmente in caso di noduli parzialmente solidi ( mggo ) , di grandi dimensioni ( 10 mm ) e irregolari . 
la crescita stata pi frequente in soggetti di et avanzata e con storia di fumo e si vericata anche dopo un lungo periodo di stabilit ( 39% di pggo modicati oltre i 3 anni )  . 
 le patologie oncologiche pi frequentemente associate a crescita dei nss sono risultate i tumori del polmone 1270 radiol med ( 2013 ) 118 : 12691280 with cancers of lung , breast , colon and bladder . 
losservazione di un campione di pazienti oncologici ha dimostrato come i nss frequentemente possono crescere di dimensioni e / o densit in questi pazienti , soprattutto se associati a tumori del polmone , della mammella , del colon e della vescica . 
la maggioranza di essi ha mostrato un tempo di sviluppo estremamente lento , perci , un follow - up superiore ai 3 anni appare giusticato anche nei pazienti oncologici . parole chiave nodulo polmonare subsolido ground glass hrct follow - up paziente oncologico introduction introduzione the widespread use of whole - body computed tomography ( ct ) for diagnosing and monitoring malignant disease has led to a signicant increase in the detection of subsolid pulmonary nodules ( ssn ) , whose clinical signicance remains unclear . the category of ssn includes those consisting exclusively of ground - glass opacity ( pure ground - glass opacity pggo ) and mixed or partially solid nodules , consisting of a solid component and a ground - glass opacity ( mixed groundglass opacity mggo ) [ 1 , 2 ]  . ssn can be the expression of benign conditions ( organising pneumonia , focal brosis , areas of inammation or bleeding ) , but may also represent preneoplastic lesions , such as atypical adenomatous hyperplasia ( aah ) [ 3 ] , or adenocarcinoma in situ ( formerly bronchiolo - alveoar carcinoma bac [ 4 , 5 ] ) and , less frequently , pulmonary metastasis [ 6 , 7 ]  . ssn generally display slower growth rates as compared to solid lesions . 
focal interstitial brosis also persists over a prolonged follow - up period and its growth pattern over time it still unknown [ 9 ]  . these data highlight the need for longer follow - up periods , as two years are not sufcient for determining the benign or malignant nature of ssn . 
 however , it is conceivable that subsolid nodules detected in routine settings may show different ct features and growth patterns . our study retrospectively analysed a population consisting of cancer patients in a non - screening clinical context . 
stato riportato un tempo di raddoppio di 988470 giorni per laah , 567168 giorni per il bac e 384212 giorni per ladenocarcinoma misto con componente bac [ 8 ]  . 
anche la brosi interstiziale focale persiste nellarco di un follow - up prolungato ed ancora sconosciuto il suo pattern di crescita nel tempo [ 9 ]  . questi dati mettono in luce limportanza di un follow - up prolungato , in quanto il tradizionale follow - up a 2 anni insufciente per determinare la natura benigna o maligna di un nss . 
tuttavia , ipotizzabile che noduli rilevati in un contesto di routine possano mostrare caratteristiche tc e comportamento differenti . il nostro studio ha analizzato retrospettivamente una poradiol med ( 2013 ) 118 : 12691280 1271 table 1 details of the patients cancer types . 
twenty patients were affected by a primary lung cancer , 77 by an extrathoracic malignancy lung cancer : 20 adenocarcinoma 8 adenocarcinoma in situ ( bac ) 2 extrapulmonary cancer : 77 breast 15 prostate 4 kidney 3 colon 11 ovary 4 skin carcinoma 2 squamous cell carcinoma 4 histology not available 6 lnh 6 skin melanoma 3 endometrium 1 liver 6 bile ducts 3 retroperitoneal liposarcoma 1 bladder 6 pancreas 3 ureter 1 stomach 4 gist 3 larynx 1 bac , bronchioloalveolar carcinoma ; lnh , non - hodgkin lymphoma ; gist , gastrointestinal stromal tumour tabella 1 speciche relative al tipo di tumore dei pazienti . 
venti pazienti avevano un tumore polmonare primitivo , 77 invece erano affetti da un tumore extratoracico tumori polmonari : 20 adenocarcinoma 8 adenocarcinoma in situ ( bac ) 2 carcinoma a cellule squamose 4 istologia non disponibile 6 tumori extrapolmonari : 77 mammella 15 prostata 4 reni 3 colon 11 ovaio 4 carcinoma cutaneo 2 lnh 6 melanoma cutaneo 3 endometrio 1 fegato 6 dotti biliari 3 liposarcoma retroperitoneale 1 vescica 6 pancreas 3 uretere 1 stomaco 4 gist 3 laringe 1 bac , carcinoma bronchiolo - alveolare ; lnh , linfoma non hodgkin ; gist , tumore stromale gastro - intestinale evaluated the ct features that can best differentiate between benign and malignant ssn , their evolution during follow - up and which neoplastic diseases are most frequently associated with ssn growth in size and / or in density . polazione composta da pazienti oncologici , fuori da ogni contesto di screening tumorale . 
sono state valutate le caratteristiche tc in grado di distinguere tra nss benigni e maligni , la loro evoluzione durante il follow - up e le patologie neoplastiche pi frequentemente associate a crescita dimensionale e / o densitometrica delle lesioni . materials and methods patients ninety - seven cancer patients ( 48 women and 49 men ; age range , 1988 years ; mean age , 65 years ) with evidence of ssn on high - resolution ct ( hrct ) were retrospectively identied from among all whole - body ct studies completed with thin reconstructions on the lung parenchyma ( hrct ) , performed at our institution between june 2006 and june 2010 . 
at least two hrct examinations were available for all patients in order to evaluate the evolution of ndings ; follow - up varied from 3 to 56 months ( mean , 27 months ) with an average of six hrct scans per patient . materiali e metodi pazienti novantasette pazienti oncologici ( 48 donne e 49 uomini , di et compresa tra 19 e 88 anni , et media 65 anni ) con evidenza di nss alla hrct , sono stati identicati retrospettivamente , sul totale delle tc total body completate con ricostruzioni sottili sul parenchima polmonare ( hrct ) effettuate nel nostro istituto tra giugno 2006 e giugno 2010 . 
la ricerca stata eseguita mediante un sistema di ricerca computerizzato per parola - chiave ( nodulo , ground - glass ) sullarchivio dei referti radiologici ( e - ris pacs , biotron )  . venti pazienti erano affetti da un tumore polmonare primitivo ( 20 , 6% ) e 77 da una neoplasia extratoracica , in assenza di tumori polmonari primitivi ( 79 , 4% )  . 
per tutti i pazienti erano disponibili almeno due controlli hrct per la valutazione evolutiva dei reperti ; la durata del follow1272 radiol med ( 2013 ) 118 : 12691280 since the study aim was to evaluate indeterminate small subsolid nodules , patients with lesions 3 cm in size and those with more than four nodules were excluded from the analysis . hrct protocol ct scans were performed using three different ct systems : 70 patients ( 72.2% ) were examined with a 16 - detector - row scanner ( siemens sensation cardiac , forchheim , germany ) , 21 patients ( 21.6% ) with a different 16 - detector - row scanner ( ge medical systems lightspeed , milwaukee , wi ) and six patients ( 6.2% ) with a 64 - detector - row scanner ( ge medical systems lightspeed , milwaukee , wi )  . the lung parenchyma was evaluated with hrct volumetric reconstructions . 
reconstruction parameters were : 2 mm slice thickness , 1 mm reconstruction interval , 120 kvp , 180 ma ( with automatic tube current modulation ) and 1.15 mm pitch for the 16 - detector - row ct scanners ; 1.25 mm slice thickness , 1 mm reconstruction interval , 120 kvp , 180 ma ( with automatic tube current modulation ) , and 0.5 mm pitch for the 64 - dectector - row scanners . 
the follow - up of each patient was performed with the same equipment and reconstruction parameters . interpretation of hrct scans all hrct scans were reviewed separately by two chest radiologists with different levels of experience in chest ct . 
dimensional variations > 1 mm , observed by both operators , were considered signicant . according to the densitometric characteristics , ssn were classied as pggo when the broncho - vascular structures could be identied within an area of increased parenchymal density , and mggos when , by switching window widths and levels , also a solid component could be appreciated . 
 densitometric changes were classied as : ( 1 ) stable , ( 2 ) increased density , ( 3 ) development of a solid component or ( 4 ) evolution into a completely solid nodule . finally , the assessments of the densitometric and size up stata variabile dai 3 ai 56 mesi ( media di 27 mesi ) con una media di circa 6 controlli hrct per paziente . dal momento che lo scopo dello studio era di valutare piccoli noduli subsolidi a signicato incerto , sono stati esclusi dallanalisi sia i pazienti con lesioni di dimensioni 3 cm sia quelli con pi di 4 noduli . protocollo hrct gli studi tc sono stati ottenuti utilizzando tre differenti apparecchiature : 70 pazienti ( 72 , 2% ) sono stati esaminati mediante una tc a 16 strati ( siemens sensation cardiac , forchheim , germany ) , 21 pazienti ( 21 , 6% ) mediante una differente tc a 16 strati ( ge medical systems lightspeed , milwaukee , wi ) e 6 pazienti ( 6 , 2% ) mediante una tc a 64 strati ( ge medical systems lightspeed , milwaukee , wi )  . la valutazione del parenchima polmonare stata eseguita con metodica hrct volumetrica . 
per le tc a 16 strati sono stati utilizzati i seguenti parametri di ricostruzione : spessore di strato 2 mm , intervallo di ricostruzione 1 mm , 120 kvp , 180 ma ( modulazione di corrente automatica ) , pitch 1 , 15 mm ; per le immagini ottenute con la tc a 64 strati , invece , sono stati usati i seguenti parametri : spessore di strato 1 , 25 mm , intervallo di ricostruzione 1 mm , 120 kvp , 180 ma ( modulazione di corrente automatica ) , pitch 0 , 5 mil follow - up di ciascun paziente stato eseguito con la medesima apparecchiatura e con gli stessi parametri di ricostruzione . interpretazione delle immagini hrct tutte le immagini hrct sono state visionate separatamente da due radiologi toracici con differente esperienza nellinterpretazione della tc del torace , non a conoscenza della storia clinica dei pazienti . 
per ogni nss sono state analizzate le seguenti caratteristiche hrct : ( 1 ) localizzazione , ( 2 ) numero ( lesioni singole o multiple ) , ( 3 ) forma ( rotondeggiante o irregolare ) , ( 4 ) dimensioni e caratteristiche densitometriche ( presenza / assenza di una componente solida ) alla prima hrct , ( 5 ) dimensioni e variazioni delle caratteristiche densitometriche alle hrct di controllo . per denire la dimensione dei nss stato ottenuto il diametro massimo assiale ( in mm ) allequatore di ogni nodulo , attraverso una nestra polmonare ( - 600 ( cid : 31 ) 1500 ) e ingrandimento ( cid : 31 ) 2 , dai due radiologi indipendentemente . 
confrontando le misure effettuate sullhrct iniziale con quelle effettuate nei successivi controlli stato possibile dimostrarne : ( 1 ) un aumento , ( 2 ) una riduzione , ( 3 ) la stabilit o ( 4 ) la scomparsa . 
stata considerata signicativa una variazione dimensionale > 1 mm , osservata da entrambi gli operatori . in base alle caratteristiche densitometriche , i nss sono stati classicati come pggo quando allinterno di una zona a incrementata densit era possibile individuare le strutture bronco - vasali , e mggo quando , modicando ampiezza radiol med ( 2013 ) 118 : 12691280 1273 changes were incorporated so that a ssn could be dened as changed ( if size and / or density changed ) , stable or disappeared . 
there was no disagreement about the presence or absence of lesions , while the few cases of disagreement regarding variations in shape or densitometry were subsequently resolved by consensus . statistical analysis the bland - altman test was used to evaluate inter - observer variability : for each ssn , the difference between the measurements performed by the rst and the second observer was calculated for both the baseline and the followup hrct . 
all statistical analysis was performed using spss ( statistical package for the social sciences , chicago , il )  . results a total of 146 ssn were analysed ( an average of 1.5 nodules per patient ; range , 14 )  . 
the mean size at baseline hrct was 9 mm ( range , 3 to 28 mm ) ; 70% of ssn were located in the upper lobes ; 119 were morphologically classied as rounded ( r ) and 27 as irregular ( ir )  . 
according to the baseline densitometric characteristics , six nodules ( 4.1% ) were classied as mggo ( 5 r , 1 ir ) and 140 nodules ( 95.9% ) as pggo ( 114 r , 26 ir )  . e livello della nestra , era possibile identicare anche una componente solida . 
le variazioni densitometiche sono state classicate come : ( 1 ) stabilit , ( 2 ) incremento di densit , ( 3 ) sviluppo di componente solida , ( 4 ) evoluzione in nodulo completamente solido . inne , i dati delle variazoni densitometiche e dimensionali sono stati integrati , in modo che ogni nss potesse essere denito modicato ( ove vi fossero variazioni dimensionali e / o densitometriche ) , invariato o scomparso . 
poich nessun nodulo nella nostra casistica diminuito di dimensioni ( un solo nodulo prima diminuito e successivamente scomparso ) , di seguito ci riferiremo a noduli modicati intendendo quelli aumentati di dimensioni e / o densit . variabilit inter - observer i limiti di concordanza delle misurazioni effettuate dai due operatori sono risultati : - 0 , 852 e 0 , 844 m poich la variabilit inter - observer risultata molto bassa , si deciso di considerare valide le misurazioni effettuate dal primo operatore . 
non si vericato alcun disaccordo circa la presenza / assenza delle lesioni , mentre i pochi casi di disaccordo vericatisi riguardo la forma o la variazione densitometrica e dimensionale sono stati successivamente risolti tramite consenso . analisi statistica per valutare la variabilit inter - observer stato utilizzato il test di bland - altman : per ciascun nss stata calcolata la differenza tra le misure effettuate dal primo osservatore e quelle del secondo osservatore , sia per la prima hrct sia per lultima hrct di controllo . 
la dimensione media alla hrct iniziale era 9 mm ( range da 3 a 28 mm ) ; morfologicamente 119 nss sono stati classicati come rotondeggianti ( r ) e 27 irregolari ( ir )  . 
al controllo dopo 36 mesi ( e ) si apprezza un ulteriore incremento dimensionale ( 13 mm ) cui si associa anche un incremento di densit , senza tuttavia la presenza di componente solida gos changed on a average of 15 months after rst detection ( range , 824 months )  . 
smoking was also found to be a factor of increased risk : 2.4% in current smokers and 1.7% in former smokers , compared to never - smokers . discussion the management of the ssn presents several as yet unresolved problems . 
considering that transient nodules may disappear within 36 months , the importance of short - term mente come lesioni maligne ( 7 metastasi e 5 tumori primitivi ) ( tabella 2 )  . 
i noduli modicati avevano una dimensione media superiore rispetto a quella dei noduli stabili ( 11 mm vs 7 , 8 mm ) ; ponendo un cut - off 10 mm , la signicativit risultata < 0 , 001 . 
i pggo rotondeggianti di piccole dimensioni ( < 5 mm ) sono tendenzialmente rimasti invariati nel tempo ( p = 0 , 007 ) , mentre stata riscontrata una tendenza dei pggo irregolari a modicarsi maggiormente ( p = 0 , 055 )  . 
al controllo dopo 45 mesi ( f ) il nodulo appare incrementato di dimensioni ( 26 mm ) , con caratteristiche densitometriche invariate hrct follow - up to document the persistence of lesions [ 11 ] is known . 
nella nostra casistica anche il fumo rappresenta un fattore di aumentato rischio : 2 , 4% nei current smokers , mentre negli ex - fumatori il rischio incrementato di 1 , 7% rispetto ai non fumatori . radiol med ( 2013 ) 118 : 12691280 1277 fig . 
il nodulo appare invariato al controllo a 4 mesi ( b ) , ridotto di dimensioni a 10 mesi ( c ) , mentre non pi apprezzabile a 20 mesi ( d )  . 
this means that pggo stability , even over a prolonged period of time , should not necessarily be considered evidence of benignity . in their interim guidelines [ 14 ] , godoy and naidich suggested a follow - up of at least three - years for lesions between 5 and 10 mm in size , while all mggo , regardless of size , should be removed because they are very likely to be cancerous . only a few studies have addressed the clinical signicance of ssn in patients with cancer . 
 [ 15 ] , in a study of 34 patients with a history of extrapulmonary cancer , reported that ssn tend to have a high rate of malignancy , but none of the 59 ggos analysed were found to be a metastasis from extrapulmonary cancer : the majority were primary lung cancers ( 24 adenocarcinomas , 16 bac , 14 aah , 4 focal brosis , 1 granuloma )  . 
in our study , we found 5 primary lung cancers and 7 metastatic lesions out of 12 removed ssn , 3 of which discussione il management dei nss presenta diverse problematiche a oggi ancora irrisolte . 
 nota limportanza di un follow - up hrct a breve termine per documentare la persistenza delle lesioni [ 11 ] , in quanto noduli transitori possono sparire entro 36 mesi , ma non ancora chiaro per quanto tempo debba essere prolungato il follow - up in caso di lesioni persistenti che non si modicano ( stabili morfo - dimensionalmente dopo i primi controlli )  . 
ci dimostra come la stabilit di una lesione pggo , anche per un periodo di tempo prolungato , non deponga necessariamente per la sua benignit . nelle loro linee guida provvisorie [ 14 ] , godoy e naidich suggeriscono un follow - up di almeno 3 anni per le lesioni 1278 radiol med ( 2013 ) 118 : 12691280 table 2 histological characteristics of 12 subsolid nodules excised during follow - up . 
five nodules were found to be primary lung cancer and seven were metastatic lesions primary lung cancer metastasis 3 adenocarcinoma 2 adenocarcinoma in situ ( bac ) 2 pulmonary adenocarcinoma 1 pulmonary squamous cell carcinoma 4 bladder carcinoma bac , bronchioloalveolar carcinoma tabella 2 caratteristiche istologiche dei 12 noduli subsolidi asportati durante il follow - up . 
cinque noduli sono risultati tumori polmonari primitivi e 7 lesioni metastatiche tumore polmonare primitivo metastasi 3 adenocarcinoma 2 adenocarcinoma in situ ( bac ) 2 adenocarcinoma polmonare 1 carcinoma a cellule squamose 4 carcinoma vescicale bac , carcinoma bronchiolo - alveolare related to a primary lung cancer , and 4 metastasis from bladder cancer ( in two different patients )  . the oncological diseases , most commonly associated with ssn growth in size and / or in density were lung cancer ( 34% ) and , among the extrathoracic diseases , breast ( 15% ) , colon ( 15% ) and bladder cancer ( 10% )  . the observation of a sample of cancer patients has shown how the characteristics that guide toward malignancy of a lesion are similar to those observed in non - cancer patients [ 14 , 16 , 17 ]  . 
the tendency of irregular pggos to change during the follow - up did not reach statistical signicance ( p = 0.055 ) , probably because of the low number of this type of nodules in our series . the disappearance of two nodules after more than 6 months of stability allows for important considerations , because no similar case has been reported in literature to our knowledge . 
this nding suggests that , although the persistence of a pggo may raise a suspicion of malignancy , this is not always the case , and also some benign lesions may persist for a long time and then disappear . older patients and those with a smoking history have an increased risk of pggo growth ( increased risk : 1.04% for each year ; 2.4% in current smokers and 1.7% in former smokers )  . we also observed that the majority of pggo changed after 2 years of stability ( 41.5% ) , but in a high percentage of pggo tra i 5 e i 10 mm di diametro , mentre le mggo , a prescindere dalle dimensioni , dovrebbero essere asportate poich altamente probabile la loro natura maligna . solo pochi studi si sono occupati del signicato clinico dei nss nei pazienti oncologici . 
 [ 15 ] in uno studio su 34 pazienti con tumori extrapolmonari , riportano che i nss tendono ad avere un alto tasso di malignit , ma nessuna delle 59 lesioni analizzate risultata essere una metastasi da tumore extrapolmonare : nella maggior parte dei casi si trattava di nuovi primitivi polmonari ( 24 adenocarcinomi , 16 bac , 14 aah , 4 brosi focale , 1 granuloma )  . 
nel nostro studio , su 12 nss asportati abbiamo riscontrato 5 tumori polmonari primitivi e 7 lesioni metastatiche , delle quali 3 riferibili a un primitivo polmonare e 4 metastasi da tumore vescicale ( in 2 distinti pazienti )  . le patologie oncologiche pi frequentemente associate a crescita dimensionale e / o densitometica dei nss sono risultate i tumori del polmone ( 34% ) e , tra le patologie extratoraciche , i tumori della mammella ( 15% ) , del colon ( 15% ) e della vescica ( 10% )  . losservazione di un campione di pazienti oncologici ha dimostrato come le caratteristiche che orientano verso la malignit di una lesione siano simili a quelle riscontrate nei pazienti non oncologici [ 14 , 16 , 17 ]  . 
in particolare abbiamo osservato che : la presenza di una componente solida depone per la malignit della lesione , i noduli pggo rotondeggianti e di piccole dimensioni ( < 5 mm ) sono tendenzialmente stabili ( p = 0 , 007 ) e i pggo di dimensioni 10 mm hanno unalta probabilit di modicarsi nel tempo ( p < 0 , 001 )  . 
la tendenza dei pggo irregolari a modicarsi durante il follow - up non risultata statisticamente signicativa ( p = 0 , 055 ) , probabilmente a causa del basso numero di noduli con tali caratteristiche . la scomparsa di due noduli dopo pi di 6 mesi di documentata stabilit consente di fare importanti considerazioni , poich non stato descritto in letteratura nessun altro caso a nostra conoscenza . 
questo riscontro suggerisce che , nonostante la persistenza di un nodulo pggo ponga il sospetto di malignit della lesione , ci non sia sempre vero e che anche alcune lesioni benigne possano persistere a lungo nel tempo per poi scomparire . nei pazienti pi anziani e con storia di fumo , il rischio di crescita dei noduli pggo risultato pi elevato ( rischio aggiuntivo : 1 , 04% per anno di et ; 2 , 4% nei fumatori e 1 , 7% negli ex fumatori )  . 
 abbiamo osservato inoltre come la maggioranza dei pggo si sia modicata dopo 2 anni di stabilit ( 41 , 5% ) , ma in unalta percentuale di casi ( 39% ) la crescita delle lesioni stata osservata anche oltre i 3 anni . 
confermiamo pertanto limportanza di un follow - up prolungato oltre i 3 anni anradiol med ( 2013 ) 118 : 12691280 1279 cases ( 39% ) lesion growth was observed even after 3 years . 
 mggos , by contrast , showed a signicantly faster ( mean , 15 months ) growth in size and / or in density . therefore , we conrm the importance of a prolonged follow - up over 3 years in patients with cancer and suggest the comparison , where possible , with the oldest available hrct images , in order to early detect even most subtle changes in ssn size and densitometry . the limits of our study are evident : the retrospective design implies that follow - up duration is highly variable from patient to patient ; in addition , it cannot be excluded that the treatments carried out might have led to an alteration of the natural history of some nodules . 
despite the availability of histological reports for the majority of mggos , none of the persisting pggos were removed , so we were only able to evaluate the hrct changes , without knowing the real histology . 
finally , since patients were identied retrospectively through a keyword search of our hospitals electronic archive of radiological reports , there is a possibility that some unreported ssn were excluded from the study . che nei pazienti oncologici e consigliamo il confronto , ove possibile , con le pi vecchie immagini hrct disponibili , in modo da poter riconoscere precocemente anche le variazioni dimensionali e / o densitometriche meno evidenti . i limiti di questo studio sono evidenti : lanalisi retrospettiva comporta una durata di follow - up molto variabile da paziente a paziente ; inoltre non possibile escludere che terapie effettuate possano aver determinato unalterazione della storia naturale di alcuni noduli . nonostante siano disponibili i referti istologici della maggior parte dei noduli mggo , nessuna delle lesioni pggo stata asportata e quindi stato possibile valutarne solamente le modiche hrct , senza conoscerne la reale istologia . inne , la ricerca dei pazienti stata effettuata in maniera retrospettiva sullarchivio dei referti radiologici del nostro istituto , utilizzando un sistema di ricerca computerizzato per parola - chiave , perci vi la possibilit che alcuni nss non segnalati siano stati esclusi dallo studio . conclusioni conclusions this study analysed a group of cancer patients with ssn in a non - screening clinical context . 
during follow - up , the majority of ssn remained stable ( 58% ) ; a small percentage disappeared ( 10% ) , while one third ( 32% ) increased in size and / or density , especially those that were partly solid ( mggo ) , large , and irregular . 
growth was more frequent in the elderly and smokers , and may occur even after a long period of stability ( 39% of pggos changed over 3 years )  . 
as a consequence , a follow - up period longer than 3 years is warranted even in cancer patients . questo studio ha analizzato un gruppo di pazienti oncologici con nss non sottoposti a screening tumorale . 
durante il follow - up la maggioranza dei nss rimasta stabile ( 58% ) ; una piccola percentuale scomparsa ( 10% ) , mentre in circa un terzo dei casi ( 32% ) si vericato un aumento di dimensioni e / o densit , specialmente in caso di noduli parzialmente solidi ( mggo ) , di grandi dimensioni e irregolari . 
la crescita stata pi frequente in soggetti di et avanzata e con storia di fumo e si vericata anche dopo un lungo periodo di stabilit ( 39% di pggo modicati oltre i 3 anni )  . 
tra i 12 nss asportati , abbiamo riscontrato 5 tumori polmonari primitivi e 7 lesioni metastatiche ; le patologie oncologiche pi frequentemente associate a crescita dei nss sono risultate in primis i tumori del polmone e , tra le patologie extratoraciche , i tumori della mammella , del colon e della vescica . 
avogadro , scuola di specializzazione in radiodiagnostica , novara , italy 3scdu ortopedia e traumatologia , aou maggiore della carit di novara , italy 4ortopedia , casa di cura frate sole , figline valdarno ( fi ) , italy 5sc fisica medica , aou maggiore della carit , novara , italy correspondence to : a . 
stecco , tel : + 39 - 0321 - 3732004 , fax : + 39 - 0321 - 3733425 , e - mail : a.stecco@libero.it received : 7 march 2012 / accepted : 21 june 2012 / published online : 27 may 2013 springer - verlag 2013 abstract objective . 
sono state acquisite le ricostruzioni mpr in tc e le immagini rm sul piano sagittale : la misura dellarea della glena e la misura del danno osseo sono state effettuate utilizzando il metodo pico . 
la misura dellarea glenoidea risulta di 575 , 29 mm2 con rm e di 573 , 76 mm2 con tc e le rispettive misure del deficit glenoideo sono di 4 , 38% e 4 , 34% . 
la concordanza inter - osservatore in tc e rm risultata buona con k > 0 , 81 , il coefficiente di varianza < 5% del valor medio sia in tc che rm . 
dislocation can be caused by an indirect , lowor high - energy mechanism and , although it may be an isolated event , it often tends to recur and creates a clinical picture of shoulder instability . evaluating glenoid bone loss has become fundamentally important for the therapeutic choice [ 1 ] , and a number of studies have shown that a high percentage of patients with shoulder instability present glenoid bone loss [ 17 ]  . 
it is therefore essential to have a preoperative diagnostic instrument that is predictive , simple and easy to use insofar as the choice of therapy is based on the guidelines proposed by provencher et al . 
la spalla larticolazione in cui la perdita dei rapporti articolari si verifica pi spesso ; la lussazione , causata da un meccanismo indiretto a bassa o ad alta energia , pu rappresentare un evento isolato , ma pi spesso tende a riprodursi nel tempo configurando il quadro di instabilit . la valutazione delle lesioni ossee della rima glenoidea , come difetto osseo ( bone loss ) , ha assunto negli ultimi anni unimportanza fondamentale nella scelta terapeutica [ 1 ]  . 
il principale obiettivo nello studio delle lesioni ossee della rima glenoidea valutare il grado di difetto osseo e definirne la severit oltre una certa percentuale di perdita della superficie globale della glena . 
 quindi fondamentale disporre di uno strumento diagnostico pre - operatorio dotato di una buona predittivit , facile e semplice , in quanto la scelta del trattamento terapeutico deve seguire le linee guida proposte da provencher et al . 
mri was carried out using a 1.5 tesla philips achieva ( philips medical systems , best , the netherlands ) with a surface coil [ voxel size 0.7 mm , flip angle 50 , thickness 0.7 mm , time to repetition ( tr ) 23 , time to echo ( te ) 5.1 ] and a 3d - t1w fast field echo ( ffe ) sequence . 
i pazienti , previo consenso informato , sono stati sottoposti a tc e rm della spalla sana e di quella patologica nella stessa giornata . metodo di quantificazione del danno glenoideo per le scansioni tomografiche stato usato uno strumento light speed vct a 64 file di detettori ( ge , milwaukee , wisconsin , usa )  . 
the pico method involves drawing a circular area ( x ) on an oblique sagittal en face image of the healthy shoulder using the lower glenoid margin as a base . 
 this circle is then transposed to the image of the pathological shoulder and the area of the sector with missing bone is drawn and calculated ( bone loss , yi )  . 
bone loss was measured three times by two operators in consensus ( in order to reduce measurement error ) , and the mean value of the three measurements was recorded ( y ) , whereas x was only calculated once by the two operators in consensus . % bone loss = area y area x * 100 the effective ct doses were estimated starting from the individual dose ratios archived in the picture archiving and communication system ( pacs ) and using version 1.02 of the impact ct patient dose calculator software ( impact , london , uk ) , which is based on montecarlo simulations and uses the international commission on radiological protection ( icrp ) 103 weighting factors for tissue . 
 statistical analysis the statistical analyses were made using the medcalc 12.2.0.1 statistical package ( medcalc software mariakerke , belgium )  . the repeated measures of mean glenoid bone loss made by more than one operator using the ct and mr images were analysed by calculating their coefficient of variance ( cv ) and standard deviation using the test for repeated measures [ 11 ]  . 
 the variability of the independent manual measurements , evaluated in terms of standard deviation and variance , was very good as the cv was less than 5% of the mean value of algoritmo per losso , spessore di strato 0 , 6 mm , tempo di rotazione 0 , 6 s , voltaggio 140 kv e intensit 180 ma . 
lesame rm stato eseguito mediante apparecchiatura philips serie achieva ( philips medical systems , best , olanda ) a 1 , 5 tesla , con una bobina di superficie ( voxel size 0 , 7 mm , flip angle 50 , thickness 0 , 7 mm , tempo di ripetizione ( tr ) 23 , tempo di eco ( te ) 5 , 1 ) utilizzando la sequenza t1 - 3d fast field echo ( ffe )  . 
il metodo pico prevede che sullimmagine sagittale obliqua della glena sana ( immagine en face della glena ) si disegni unarea circolare ( x ) utilizzando come base il margine inferiore della glena . 
la misurazione del difetto osseo stata ripetuta tre volte da due operatori in consensus ( per ridurre lerrore della misura , utilizzando la media delle tre , y ) , mentre larea circolare x stata calcolata una sola volta sempre dai due operatori in consensus . % difetto osseo = area y area x * 100 le dosi efficaci in tc sono state stimate a partire dai rapporti di dose individuale archiviati sul picture archiving and communication system ( pacs ) e utilizzando il software impact ct patient dose calculator v1.02 ( impact , london , uk ) , che basato su simulazioni montecarlo e utilizza i fattori di peso per il tessuto dell international commission on radiological protection ( ircp ) 103 . 
 analisi statistiche tutte le analisi statistiche sono state eseguite mediante il pacchetto applicativo statistico medcalc 12.2.0.1 ( medcalc software mariakerke , belgium )  . le misure ripetute da pi operatori effettuate sulle immagini tc e rm del danno medio del deficit osseo glenoideo sono state analizzate valutando il coefficiente di varianza e la deviazione standard con il test per misure ripetute [ 11 ]  . 
 successivamente , stata valutata la concordanza inter - osservatore tra i due osservatori rm e tc , mediante il test di concordanza k di cohen [ 12 ] , classificando in classi di concordanza comprese tra poor e very good , rispettivamente se k < 0 , 20 o k > 0 , 81 [ 13 ]  . stato applicato il test di bland - altman per la correlazione delle differenze tra le due tecniche di misurazione , plottando le misure delle due metodiche contro la media delle stesse , sia per le misure ottenute sulla glena normale con entrambe le metodiche , che per le misure di danno glenoideo . 1338 radiol med ( 2013 ) 118 : 13351343 fig . 
larea della glena della spalla sana misurata varia tra 481 , 44 e 694 , 34 mm2 in tc , tra 482 , 69 e 694 , 41 mm2 in rm , con un valore medio rispettivamente di 573 , 76 mm2 e 575 , 29 mm2 . 
il valore medio del difetto glenoideo , misurato manualmente dai due operatori , variava tra 0 e 92 , 78 mm2 in rm e tra 0 e 94 , 79 mm2 in tc . 
 la variabilit delle misurazioni manuali indipendenti , valutata in termini di deviazione standard che di varianza , stata molto buona , risultando il coefficiente di varianza ( cv ) inferiore al 5% del valore medio sia nella tc ( 4 , 88% ) che nella rm ( 4 , 08% )  . 
nel 2003 [ 9 ] hanno calcolato la percentuale del deficit osseo glenoideo mediante un metodo tc con ricostruzi oni 3d , dimostrando come la met inferiore della glena possa essere considerata con buona approssimazione una circonferenza passante da ore tre a ore nove . 
poich in uno stesso individuo la superficie delle due glene identica , calcolando prima larea circonferenziale della met inferiore della glena sana , possibile valutare la morfologia della glena patologica e calcolare il deficit osseo in termini di area ( espressa in mm2 ) o in percentuale di superficie , semplicemente disegnando larea deficitaria o il contorno del frammento . 
 [ 19 ] , in uno studio del 2007 , hanno confrontato laccuratezza della tc rispetto allartroscopia nella valutazione del difetto osseo della glena ; cinquanta pazienti sono stati sottoposti allesame tc e successivamente allartroscopia . 
 [ 20 ] hanno confrontato la tc 2d e 3d nella quantificazione del danno osseo nellinstabilit anteriore di spalla , riscontrando lequivalenza tra le due tecniche . sebbene la tc rappresenti la metodica delezione per valutare lentit del danno glenoideo ( presenta , infatti , unalta sensibilit : 93% e specificit : 78% ) , la risonanza magnetica largamente utilizzata nella diagnosi preoperatoria delle lesioni a carico dei tessuti molli articolari ( cercine glenoideo , apparato capsulo - legamentoso ) [ 2125 ]  . 
 [ 18 ] , effettuato su 14 glene di cadaveri , ha validato il meto do proposto da sugaya applicato alla rm come metodica sovrapponibile alla tc per quantificare il danno glenoideo . 
 [ 26 ] , utilizzando unapparecchia tura ad alto campo ( 3t ) , ne hanno dimostrato sia lapplicabilit per una migliore visualizzazione delle strutture ossee , tendinee , cartilaginee e legamentose , sia una maggiore risoluzione spaziale , particolarmente utile nello stu dio delle articolazioni o di alcune loro componenti fino a oggi valutabili in maniera sub - ottimale con esami non artrografici . nel nostro studio , per la prima volta , il metodo pico stato applicato in vivo , sia in tc che rm , per confrontare fig . 
ct - mr : tc - rm ; average of ct and mr : media di tc e rm . recurrent dislocations or luxations and , more importantly , it influences the type of surgery . 
many methods of ascertaining the presence and extent of bone loss have been described in the literature , and some authors have tried to quantify it radiologically or arthroscopically [ 2 , 1518 ]  . 
 [ 9 ] calculated the percentage of glenoid bone loss using ct - based 3d reconstructions , and showed that the lower half of the glenoid cavity can with good approximation be considered a circumference passing from three oclock to nine oclock . 
as the surfaces of the two glenoid cavities in the same subject are identical , by first calculating the circumferential area of the lower half of the healthy shoulder , the bone loss can be calculated in terms of area ( expressed in mm2 ) or percentage simply by drawing the area of the deficiency or the outline of the fragment . 
 [ 19 ] compared the accuracy of ct and arthroscopy in assessing glenoid bone loss in 50 patients , and found that ct was highly sensitive and specific , and that the findings correlated closely with the arthroscopic findings . 
 [ 20 ] compared 2d and 3d ct for the quantification of bone loss in anterior shoulder instability , and discovered that the two techniques were equivalent . although the 93% sensitivity and 78% specificity of ct make it the method of choice for assessing glenoid bone loss , mri is widely used in the preoperative diagnosis of lesions affecting articular soft tissue ( the glenoid rim , the capsular - ligament complex ) [ 2125 ]  . 
 [ 18 ] have evaluated the use of sugayas method on mr images of 14 cadaveric shoulders , and found that the results were the same as those obtained using ct . 
 [ 26 ] , using high - resolution equipment ( 3t ) , showed both its ap1342 radiol med ( 2013 ) 118 : 13351343 plicability for better visualisation of bone , cartilage and ligament structures , and better spatial resolution ; the latter is particularly useful in the study of the joints or other components so far only sub - optimally evaluated with nonarthrographic examinations . our study is the first to use the pico method in vivo to compare the diagnostic accuracy of ct and mr imaging . 
 the two series of measurements can be considered substantially equivalent , as shown by the cohen kappa value of > 0.81 , and so this pilot study has established that the results are sufficiently promising to allow the planning of a study of a larger group of patients . albeit with the limitation of the small number of patients due to the preliminary nature of this study , it can be concluded that either ct or mri can be used as a preoperative diagnostic technique for measuring bone loss using the pico method . 
it has also been demonstrated that mri can be used as a reference method not only for studying the rotator cuffs and the glenoid rim , but also for quantifying bone loss ; this makes it possible to limit the patients exposure to ionising radiation when diagnosing the bone loss associated with shoulder instability . laccuratezza diagnostica delle due metodiche . 
le due serie di misurazioni ottenute con tc e rm possono ritener si sostanzialmente equivalenti come dimostrato dal valore k di cohen ottenuto ( k > 0 , 81 ) ; pertanto questo studio pilo ta ha permesso di stabilire che i risultati ottenuti applicando il metodo pico a spalle studiate in vivo sia con la tc che con la rm sono sufficientemente promettenti per pianificare uno studio allargato su una popolazione pi estesa . si pu concludere che , pur con la limitazione del numero ridotto di pazienti data la natura preliminare di que sto studio , possibile applicare indifferentemente i metodi tc e rm per misurare il difetto osseo della spalla con il metodo pico come tecnica diagnostica pre - operatoria . 
si inoltre dimostrato che la risonanza magnetica pu esse re utilizzata come metodica di riferimento non solo nello studio della cuffia dei rotatori e del cercine , ma anche per la quantificazione del danno osseo ; ci permette di limitare lesposizione dei pazienti a radiazioni ionizzanti nella diagnosi della perdita ossea associata allinstabilit di spalla . conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . 
pulmonary artery sarcomas ( pas ) are rare malignant tumours that originate from the intimal layer of the pulmonary artery , occur in middle age and have a poor prognosis . 
between 2008 and 2012 , we managed four adult patients with a nonspecific clinical presentation who , at the conclusion of the diagnostic process , were found to be affected by pas . 
because of the initial suspicion of pulmonary embolism , all patients underwent chest radiograph , lung perfusion scintigraphy , trans - oesophageal echocardiography , and computed tomography ( ct ) angiography of the chest . 
then , because of the peculiar ct findings and lack of response to anticoagulation therapy , a clinical suspicion of pas was considered and all patients underwent positron - emission tomography ( pet ) - ct , and one patient also magnetic resonance imaging ( mri ) of the chest . 
tra il 2008 ed il 2012 sono giunti alla nostra osservazione 4 pazienti adulti , con quadro clinico non specifico che al termine delliter diagnostico sono risultati affetti da sap . 
tutti i pazienti , per il sospetto iniziale di embolia polmonare , hanno eseguito una radiografia del torace , una scintigrafia polmonare perfusionale , unecocardiografia trans - esofagea , e una angio - tomografia computerizzata ( tc ) torace . 
in seguito alle peculiari caratteristiche tc associate alla mancata risposta alla terapia anticoagulante , nel sospetto clinico di sap , stata effettuata una tomografia ad emissione di positroni ( pet ) - tc ed in un caso anche una risonanza magnetica ( rm ) toracica . 
ct is the technique that enabled the first step in the differential diagnosis between pas and pulmonary embolisthe ct characteristics suggestive of pas included the particular filling defect occupying the entire lumen of the pulmonary trunk with increase in diameter of the involved vessel and patchy and delayed contrast enhancement at ct angiography , more evident in the venous phase . 
le caratteristiche suggestive per sap includevano il particolare difetto di riempimento occupante lintero lume del tronco polmonare con aumento di diametro del vaso coinvolto e il contrast enhancement disomogeneo e ritardato alla angio - tc , ancora pi evidente in fase venosa . 
la diagnosi precoce mediante imaging integrato rimane ancora al giorno doggi la via principale da perseguire per ottenere miglioramenti in termini prognostici . parole chiave sarcoma arteria polmonare diagnosi differenziale tomografia computerizzata risonanza magnetica tomografia ad emissione positroni introduction introduzione primary heart tumours are rare , and malignant ones are only a small subtype of these . 
therefore , cardiac sarcomas are generally classified into right heart sarcomas , left heart sarcomas and pulmonary artery sarcomas ( pas ) [ 1 ]  . pas is a rare , poorly differentiated , malignant tumour which originates in most cases from the totipotent intimal stem cells , and for this reason is referred to as intimal sarcoma ; in the literature about 250 cases have been described [ 2 , 3 ]  . intimal pas are usually malignant mesenchymal tumours which are poorly differentiated with fibroblastic or miofibroblastic differentiation . 
in some cases they may present specific histological patterns and be classified into osteosarcomas , rhabdomyosarcomas and angiosarcomas i tumori primitivi cardiaci sono rari e quelli maligni ne rappresentano solo un piccolo sottotipo . 
 il sap un tumore maligno raro , poco differenziato , che origina per la maggiore parte dalle cellule intimali totipotenti , e per questo viene denominato sarcoma intimale ; in letteratura ne sono stati descritti circa 250 casi [ 2 , 3 ]  . i sarcomi intimali sono in genere dei tumori maligni mesenchimali poco differenziati con differenziazione fibroblastica o miofibroblastica . 
pas occur in middle age , with nonspecific clinical features which may mimic other diseases such as lung cancer , mediastinal masses , and especially acute or chronic pulmonary embolism [ 4 , 5 ]  . 
they have a poor prognosis , so early and proper diagnosis is necessary to establish the appropriate therapy . the purpose of this paper is to provide recommendations for the diagnostic imaging classification of this rare and still poorly understood disease , on the basis of our experience with four patients , who accounted for 0.3% of patients with pulmonary hypertension who were managed at our institute over the past 5 years . leiomiosarcomi dellarteria polmonare invece sono sarcomi che originano dalla tonaca media del vaso e sono denominati sarcomi murali [ 3 ]  . 
hanno una prognosi sfavorevole , quindi necessaria una diagnosi precoce e corretta per impostare lopportuna terapia . lo scopo del nostro lavoro di dare suggerimenti sullinquadramento diagnostico dal punto di vista dellimaging di questa patologia a bassissima incidenza ed ancora poco conosciuta , sulla base della nostra esperienza su 4 casi di sap , che rappresentano lo 0 , 3% dei pazienti con ipertensione polmonare giunti alla nostra osservazione negli ultimi 5 anni . materials and methods between 2008 and 2012 , we managed four adult patients ( two women and two men ; mean age , 5013.4 years ) who , at the conclusion of the diagnostic pathway , were found to be affected by pas . 
all patients had a nonspecific clinical presentation , simulating the far more common condition of pulmonary embolissymptoms and signs included : chest pain , cough , dyspnoea , haemoptysis , pulmonary hypertension , and right heart failure . 
in two cases there were also systemic manifestations such as fever , anaemia , night sweats and weight loss ( indicators of malignancy )  . because of the initial suspicion of pulmonary embolism , all patients underwent chest radiograph , lung perfusion scintigraphy , trans - oesophageal echocardiography , and computed tomography ( ct ) angiography of the chest . 
thereafter , because of the peculiar ct findings and lack of response to anticoagulation therapy , a clinical suspicion of pas was considered and all patients were investigated with positron emission tomography ( pet ) - ct and one patient also with chest magnetic resonance imaging ( mri )  . all patients subsequently underwent thromboendoarterectomy with histological investigation of the surgical specimen , which confirmed the clinical and radiological suspicion of pas . 
the remaining two patients are currently alive at 14 and 6 months after diagnosis . materiali e metodi tra il 2008 ed il 2012 sono giunti alla nostra osservazione 4 pazienti adulti , di cui 2 donne e 2 uomini , con et media 5013 , 4 anni , i quali , a conclusione delliter diagnostico , sono risultati affetti da sap . 
 tutti i pazienti , per il sospetto iniziale di embolia polmonare , hanno eseguito una radiografia del torace , una scintigrafia polmonare perfusionale , unecocardiografia trans - esofagea , e una angio - tomografia computerizzata ( tc ) torace . 
in seguito alle peculiari caratteristiche tc associate alla mancata risposta alla terapia anticoagulante , nel sospetto clinico di sap , in tutti i pazienti stato effettuato un approfondimento diagnostico mediante tomografia ad emissione di positroni ( pet ) - tc ed in un caso anche una risonanza magnetica ( rm ) toracica . in seguito tutti i pazienti sono stati sottoposti a tromboendoarteriectomia con indagine istologica del pezzo operatorio che ha confermato il sospetto clinico - radiologico di sap . 
i restanti due pazienti sono attualmente in vita a 14 e 6 mesi dalla diagnosi . il follow - up stato effettuato mediante radiografia del torace ( valutazione dello stato emodinamico ) , angio - tc e pet - tc ( valutazione residuo e attivit della malattia )  . follow - up was carried out with chest radiograph ( evaluation of haemodynamic status ) , ct angiography and petct ( evaluation of residual disease activity )  . risultati 1262 results integration of different imaging modalities was of fundamental importance for substantiating the clinical suspicion of pas , in consideration of the difficulties surrounding the differential diagnosis and the need for an early diagnosis of this rare disease . chest radiography was performed as the first - level investigation , but the result was always nonspecific . 
however , it proved to be of limited value in the differential diagnosis because , by not depicting the filling defects directly , it does not allow one to evaluate their nature , the precise location and extent . trans - oesophageal echocardiography was also used in the diagnostic work - up of pas and provided useful information about valvular and ventricular function , the physiological significance of the lesions and their effect on the other cardiac structures . pulmonary angiography was not used in the initial diagnostic phase , because of the better results of ct , pet - ct and mri . 
subsequent pulmonary angiography performed under fluoroscopic guidance at the same time as the assessment of pulmonary pressures by right heart catheterisation revealed the presence of intraluminal opacification defects , the abrupt termination of some arterial branches and parenchymal perfusion defects . 
in addition , in one case pas appeared as a polypoid filling defect that moved during the cardiac cycle . ct is the technique that allowed the first step in the differential diagnosis between pas and pulmonary embolis the ct signs lending support to a diagnosis of pas rather than chronic pulmonary embolism included both morphological and densitometric aspects . 
risultata di scarsa utilit nella diagnosi differenziale poich , non permettendo la visualizzazione diretta del difetto di riempimento , non ha consentito di valutarne la natura , la precisa localizzazione e lestensione . lecocardiografia trans - esofagea stata anchessa impiegata nelliter diagnostico del sap e ha fornito utili informazioni sulla funzionalit ventricolare e valvolare , sul significato fisiologico delle lesioni ed il loro effetto sulle altre strutture cardiache . langiopneumografia nella nostra esperienza non stata utilizzata in fase diagnostica iniziale , per i migliori risultati di tc , pet - tc e rm . 
in una fase successiva , contestualmente alla valutazione delle pressioni polmonari mediante cateterismo cardiaco destro , lintroduzione di mezzo di contrasto nelle arterie polmonari sotto guida fluoroscopia ha evidenziato la presenza di difetti di opacizzazione intraluminali , linterruzione brusca di alcuni rami arteriosi e difetti di perfusione parenchimale . 
in un caso inoltre il sap si presentava come difetto di riempimento polipoide , mobile durante il ciclo cardiaco . la tc la metodica che ha permesso di effettuare il primo step nella diagnosi differenziale tra sap ed embolia polmonare . 
reconstructed coronal ct angiography image ( b ) shows multiple filling defects of the pulmonary trunk and its main , lobar and segmental branches , with extraluminal extension in some areas ( arrows )  . 
b langio - tc in ricostruzione coronale mostra multipli difetti di riempimento a carico del tronco polmonare e delle sue diramazioni principali , lobari e segmentarie , con estensione extraluminale in alcune aree ( frecce )  . 
2a - d the axial ct scans before ( a ) and after contrast administration during the arterial ( b ) and venous phase ( c ) show filling defects of the common trunk , left and right pulmonary arteries , with significant contrast enhancement in venous phase ( 80 hu versus 50 hu at baseline )  . 
2a - d le scansioni assiali tc prima ( a ) e dopo mezzo di contrasto in fase arteriosa ( b ) e venosa ( c ) mostrano difetti di riempimento di tronco comune , arteria polmonare sinistra e destra , con evidente captazione di mezzo di contrasto in fase venosa ( basale 50 hu , fase venosa 80 hu )  . 
the filling defect due to the angiosarcoma ( x ) is isodense in the unenhanced ct scan ( a ) and shows contrast enhancement on the contrast - enhanced scan ( b ) ; the superimposed acute thrombotic material ( y ) is poorly discernible on the unenhanced scan ( a ) and does not enhance after contrast administration ( b )  . 
il difetto di riempimento dovuto allangiosarcoma ( x ) appare isodenso nella scansione tc senza mdc ( a ) e mostra successivamente impregnazione contrastografica ( b ) , mentre il materiale trombotico in fase acuta sovrapposto ( y ) appare scarsamente differenziabile senza mdc ( a ) e non mostra impregnazione contrastografica ( b )  . 
anche limmagine assiale di fusione pet - tc ( c ) e limmagine pet con correzione dellattenuazione ( d ) mostrano incremento delluptake di fdg a livello del tessuto tumorale nellarteria polmonare di destra , ma non del materiale trombotico sovrapposto . discussion discussione from the viewpoint of imaging , the differential diagnosis between pas and thrombo - embolic disease is difficult , even though the ct features may be specific in patients with advanced malignant disease . 
 the absence of predisposing factors for pulmonary embolism ( no venous thrombosis of the lower limbs on colour doppler ultrasound , no finding suggestive of hypercoagulable state ) and the progressive worsening of dyspnoea in patients with an intraluminal filling defect despite anticoagulation therapy are factors suggestive of pas . 
the lack of response to anticoagulation therapy correlated with the imaging findings may be decisive for the diagnosis . nelliter diagnostico , dal punto di vista della diagnostica per immagini , la diagnosi differenziale fra sap e malattia trombo - embolica risulta difficile , nonostante le caratteristiche tc possano essere specifiche in pazienti con patologia maligna avanzata . lassenza di fattori predisponenti per embolia ( assenza di trombosi venosa degli arti inferiori alleco doppler ) ed il progressivo peggioramento della dispnea in paziente con difetto di riempimento delle arterie polmonari nonostante la terapia anticoagulante sono fattori suggestivi per sap . 
black - blood t1 - weighted coronal images without contrast medium ( a ) and after paramagnetic contrast medium ( b , c ) show a mass occupying the pulmonary trunk and right pulmonary artery , and extends into the left pulmonary artery . 
immagini coronali t1 pesate senza mdc ( a ) e dopo mdc paramagnetico ( b , c ) mostrano una massa che occupa il tronco polmonare e larteria polmonare di destra e si estende anche nellarteria polmonare sinistra . 
 the main role of chest x - ray is to exclude other diseases that may present with similar symptoms and to provide elements to guide subsequent diagnostic investigations [ 6 ]  . the ct features suggestive of pas rather than thromboembolic disease included : large low - density filling defect occupying the entire lumen of the pulmonary trunk or main branches of the pulmonary artery , with increase in diameter of the involved vessel and extraluminal extension of the tumour . 
on the noncontrast ct scan , the filling defect was generally isodense compared to the lumen of the pulmonary trunk with areas of hypodensity due to acute apposition of il ruolo principale della radiografia del torace di escludere altre patologie che possono presentarsi con la stessa sintomatologia e dare utili suggerimenti per il successivo work - up [ 6 ]  . in tc le caratteristiche suggestive per sap rispetto alla malattia trombo - embolica polmonare includono : voluminoso difetto di riempimento occupante lintero lume del tronco polmonare o dei rami principali dellarteria polmonare , con aumento di diametro del vaso coinvolto ed estensione extraluminale del tumore . 
 however , foci of calcification can also be detected in cases of chronic embolism or thrombosis in situ [ 8 ] , although they tend to occur on the artery wall and peripherally in these cases . pet - ct was used to confirm the suspicion of pas and to distinguish between pas and pulmonary embolism on the basis of the increased radiopharmaceutical uptake of tumours [ 9 , 10 ]  . 
combining ct and pet - ct therefore proved to be extremely useful in assessing patients with suspected pas . mri , despite a greater capacity for tissue characterisation , has some disadvantages compared to ct : these include a lower spatial resolution and a need for a longer breathhold time , which is a problem if we consider that the majority of the patients examined for this condition are heavily dyspnoeic . 
the intensity of contrast enhancement after contrast injection is correlated with the degree of tumour differentiation [ 11 , 12 ] and can be also used in post - intervention follow - up and monitoring to evaluate residual or recurrent tumour [ 13 ]  . pas have a poor prognosis . 
in the case of tumours causing occlusion of the main arterial branches with significant haemodynamic changes , procedures with palliative intent are often carried out which generally consist of endoarterectomy . 
the role of chemotherapy and radiotherapy has yet to be defined , but a specific adjuvant therapy may be administered in specific subtypes of sarcoma for a more effective treatment [ 3 , 4 ]  . 
focolai di calcificazione si possono rilevare tuttavia anche in casi di embolia cronica o di trombosi in situ [ 8 ] , anche se in tali casi si presentano solitamente in sede periferica e parietale . la pet - tc stata impiegata per confermare il sospetto di sap e distinguere tra sap ed embolia polmonare sulla base dellipercaptazione del radiofarmaco della componente neoplastica [ 9 , 10 ]  . 
la combinazione tc e pet - tc si rivelata pertanto di estrema utilit nella valutazione dei pazienti con sospetto sap . la rm , nonostante una maggiore capacit di caratterizzazione tissutale , presenta alcuni svantaggi rispetto alla tc , in particolare la risoluzione spaziale comunque inferiore e la necessit di una durata dellapnea maggiore , tenendo presente che la maggior parte dei pazienti esaminati per questa patologia sono fortemente dispnoici . 
il ruolo della chemioe della radioterapia deve ancora essere definito , ma una terapia adiuvante specifica potrebbe essere somministrata in particolari sottotipi di sarcoma per un trattamento pi efficace [ 3 , 4 ]  . 
 per queste ragioni , una diagnosi precoce corretta di fondamentale importanza ed il radiologo in genere il primo a potere porre sospetto di sap in pazienti con grave dispnea e difetto di riempimento nellarteria polmonare . pas is a highly aggressive and rapidly evolving disease , which is underdiagnosed and misunderstood . 
la diagnosi precoce mediante imaging integrato rimane ancora al giorno doggi la via principale da perseguire per ottenere miglioramenti in termini prognostici . nelle immagini angio - tc la presenza di un difetto di riempimento con contrast enhancement nellarteria polmonare deve porre il sospetto di lesione maligna e lipotesi 1268 radiol med ( 2013 ) 118 : 12591268 intensity on contrast - enhanced mri . 
the presence of extraluminal tumour extension as well as distant metastases are reliable signs in the differential diagnosis between pas and pulmonary embolism , but these are manifestations of advanced cancer . for these reasons , the radiologist must be aware of the imaging characteristics of this rare disease to be able to raise the suspicion of pas in patients with severe dyspnoea and filling defect of the pulmonary artery unresponsive to anticoagulation therapy . deve essere confermata da un elevato uptake alla pet - tc con fdg o da iperintensit in rm con mezzo di contrasto . 
patients with atypical chest pain and suspected obstructive cad were directed to one of two diagnostic pathways : the traditional protocol ( examination , stress test , ca ) and the current protocol ( examination , stress test , mdct - ca , and ca , if necessary )  . 
mdct - ca had an accuracy of 66% , a sensitivity and specicity of 21% and 87% , respectively , and a positive ( ppv ) and negative ( npv ) predictive value of 40% and 70% , respectively . 
comparison between conventional ca ( cca ) and mdct - ca showed a sensitivity and specicity of 92% and 89% , respectively , a ppv and npv of 89% , and an accuracy of 92% . 
sono stati considerati due percorsi diagnostici per pazienti con dolore toracico atipico e sospetta coronaropatia ostruttiva : il protocollo tradizionale ( visita , stress test , coronarograa ) e il protocollo attuale , ( visita , stress test , ac - tcms ed eventuale coronarograa )  . 
lo stress test nei confronti dellac - tcms ha attenuto valori di accuratezza del 66% con sensibilit e specicit del 21% e 87% e valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) di 40% e 70% . 
il confronto tra acc e ac - tcms ha rilevato una sensibilit e specicit pari a 92% e 89% , un vpp e vpn pari a 89% per unaccuratezza complessiva del 92% . 
il protocollo radiol med ( 2013 ) 118 : 12941308 1295 protocol : 1 , 645 euro against 322 euro ( mean ) , but it shows a better cost - effectiveness ratio . 
 keywords mdct coronary angiography stress test coronary angiography cost analysis atypical chest pain tradizionale risultato avere costi pi elevati rispetto a quello modicato dalla ac - tcms , 1645 euro contro 322 euro ( media ) , ma dimostra un miglior rapporto costo / efcacia . 
dai nostri dati , lutilizzazione di un protocollo che prevede lac - tcms come spartiacque principale per i pazienti da inviare alla coronarograa , risulta vantaggioso in termini di costo e di efcacia diagnostica . 
 parole chiave angiograa coronarica mediante tcms stress test coronarograa analisi dei costi dolore toracico atipico introduction introduzione coronary angiography ( ca ) with multidetector computed tomography ( mdct - ca ) represents an accurate diagnostic test to rule out obstructive coronary artery disease ( cad ) [ 18 ]  . 
the stress test is widely used as a rst - level cardiological screening test in patients with low to intermediate cardiovascular risk ; however , its diagnostic performance is lower than that of mdct - ca [ 10 ] , with a high number of false positive tests and an even higher number of false negative tests . 
in patients with prolonged chest pain , cca is frequently the only examination able to denitively exclude obstructive cad , as it represents the gold standard technique for detecting coronary stenosis . 
the aim of our study was to evaluate , the cost - effectiveness and incremental diagnostic value of mdct - ca in clinical practice in patients with suspected obstructive cad compared with the traditional diagnostic pathway . 
attualmente le linee guida indicano nel caso di pazienti con angina stabile , dolore toracico tipico o atipico ed in presenza di fattori di rischio cardiovascolare , lesecuzione di un elettrocardiogramma ( ecg ) e di una prova da sforzo [ 911 ]  . 
nonostante lutilizzo del test da sforzo sia ampiamente usato come screening cardiologico di primo livello nella categoria di pazienti a basso - medio rischio cardiovascolare , la sua performance diagnostica decisamente minore rispetto a quella fornita dalla ac - tcms [ 10 ] , con un elevato numero di falsi positivi , ma soprattutto di falsi negativi . 
i pazienti con dolore toracico tipico e atipico , ma con test da sforzo negativo sono indirizzati ad ulteriori test diagnostici non invasivi , ma spesso lacc si rivela lunico esame in grado di escludere denitivamente la coronaropatia ostruttiva se la sintomatologia dolorosa perdura , ed essa rappresenta oggi il gold standard per lidenticazione delle stenosi coronariche . 
scopo del presente 1296 materials and methods study population between january 2009 and june 2011 , 720 consecutive patients ( mean age , 6511.5 years ; 344 men ) undergoing 64 - slice mdct - ca ( brilliance 64 , philips , the netherlands ) were considered . 
 all patients underwent mdct - ca if spontaneous or - blocker - induced heart rate was 65 bpm and if they were able to hold their breath for the time required to acquire the volume data ( 1012 s )  . 
the following patients were excluded from the mdct - ca study : symptomatic patients with acute chest pain and an ecg positive for ischaemia , those with a heart rate 65 bpm , those with a known allergy to iodinated contrast material , pregnant women , patients with respiratory failure , with unstable clinical condition and severe heart failure . 
cca on the basis of analysis of specicity , sensitivity , ppv and npv of the individual techniques ( especially in view of the well - known low accuracy of the cycle test ) and the costeffectiveness ratio of the rst two pathways , we considered a third diagnostic pathway in which mdct - ca was the rst - line modality : 3 . 
mdct - ca positive for stenosis > 50% radiol med ( 2013 ) 118 : 12941308 lavoro valutare il valore diagnostico incrementale dellintroduzione della ac - tcms nella gestione clinica del paziente con sospetta coronaropatia ostruttiva ( cad ) rispetto al tradizionale percorso diagnostico in termini di rapporto costo / efcacia . materiali e metodi popolazione campione nel periodo compreso tra gennaio 2009 e giugno 2011 sono stati considerati 720 pazienti consecutivi ( et media 6511 , 51 anni , 344 maschi ) sottoposti ad ac - tcms mediante apparecchio tcms a 64 detettori ( brilliance 64 , philips , paesi bassi ) disponibile presso il nostro istituto . tutti i pazienti dello studio sono stati sottoposti allindagine ac - tcms se la frequenza cardiaca era 65 battiti per minuto ( bpm ) spontanea o indotta dalla somministrazione endovenosa di - bloccante , e se la capacit di mantenere unapnea era sufciente per il periodo di acquisizione del volume toracico ( 1012 s )  . 
un altro criterio di inclusione stata la presenza di ritmo cardiaco sinusale ; sono stati accettati nello studio , tuttavia , anche i pazienti con brillazione atriale cronica con risposta ventricolare medio bassa , inducibile < 65 bp sono stati esclusi dal presente studio tutti i pazienti con cad nota trattati con stent o by - pass . 
sono stati esclusi i pazienti sintomatici con dolore toracico acuto e ecg positivo per ischemia , con frequenza cardiaca > 65 bpm , allergia nota al mezzo di contrasto iodato , gravidanza , insufcienza respiratoria , stato clinico instabile e scompenso cardiaco di grado severo . 
caa pretest evaluation for each patient , we recorded indication for the test and calculated the pretest risk ( mdct - ca ) of cad in relation to : smoking hypertension positive family history of cad diabetes mellitus and hypercholesterolaemia using the morise score 2 . 
acc. sulla base dellanalisi dei dati in termini specicit , sensibilit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) delle metodiche ( in particolare della scarsa accuratezza del cicloergometro gi nota in letteratura ) , e del rapporto costo / efcacia dei primi due percorsi , stato inoltre ipotizzato il seguente percorso diagnostico in cui 1298 radiol med ( 2013 ) 118 : 12941308 fig . 
3 percorso diagnostico modicato dallutilizzo della ac - tcms prima del cicloergometro nei pazienti con dolore toracico atipico . mdct - ca scan scan protocol the contrast - enhanced study was obtained using 80100 ml of iodinated contrast medium ( iomeprol 400 mgi / ml , iomeron , bracco , milan , italy ) injected intravenously at 5 ml / s ow rate , followed by 40 ml of saline . 
the contrast medium was injected with an automatic dual - head injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an antecubital vein with a 16 - g needle cannula . 
the optimal acquisition protocol was chosen based on the patients heart rate and anthropometric characteristics [ body mass index ( bmi ) ] in order to balance dose sparing with optimal image quality . 
 image analysis images were evaluated by a radiologist with 6 years of continuing training in mdct - ca and , in the event of disagreement between clinicalanamnestic data and mdct - ca ndings , the case was reviewed with a cardiologist . 
for each lesion , a visual assessment of the stenosis was performed using current international criteria [ 7 , 8 ] : 020% , no stenosis or wall irregularities 2050% , nonsignicant stenosis lac - tcms risulta essere metodica di prima linea : 3 . 
acc. valutazione pre - test per ciascun paziente stata registrata lindicazione allesame ed stato tracciato un prolo di rischio pre - test ( preac - tcms ) di cardiopatia aterosclerotica in rapporto a : anamnesi positiva per fumo ; ipertensione ; familiarit per eventi cardiaci acuti ; diabete e ipercolesterolemia utilizzando il morise score . esecuzione dellesame ac - tcms protocollo di scansione sono stati somministrati per via endovenosa 80100 ml di mezzo di contrasto non ionico iodato ( iomeprol 400 mgl / ml , iomeron , bracco , milano , italia ) con un usso di 5 ml / s , seguito da 40 ml di soluzione salina allo stesso usso . 
il mezzo di contrasto stato introdotto tramite un iniettore automatico a doppia pompa ( stellant , medrad , pittsburgh , pa , usa ) connesso a una vena antecubitale con un agocannula da 16 g . 
the ecg trace was recorded in all stages of the test , starting from rest phase through incremental negative energy of 25 w every 2 min to achieve the expected maximal threshold . 
la valutazione delle arterie coronarie ha previsto uno studio dei singoli segmenti effettuato seguendo una classicazione dellalbero coronarico a 17 segmenti secondo lamerican heart association ( aha ) [ 15 ]  . 
per ogni lesione stata effettuata una stima di stenosi visuale distinta secondo i criteri internazionali [ 7 , 8 ] : 0%20% , assenza di stenosi o irregolarit parietali ; 20%50% , stenosi non signicativa ; 50%70% , stenosi signicativa ; 70%100% , stenosi severa occludente o sub occludente . test da sforzo mediante cicloergometro ciascun paziente stato posizionato su un cicloergometro in posizione seduta . 
il tracciato elettrocardiograco stato registrato in tutte le fasi dellindagine , partendo da una fase di riposo no ad arrivare a energie negative incrementali di 25 w ogni 2 minuti , no al raggiungimento della soglia massima teorica . 
il test risultato dubbio per patologia signicativa in caso vi fosse un sotto - slivellamento st minore dei parametri indicati con persistenza del pattern al recupero , in presenza di sintomatologia tipica , o se presente angina tipica anche in assenza di alterazioni elettrocardiograche . 
in tutti gli altri casi lesame risultato essere negativo . analisi statistica sono stati calcolati la specicit , la sensibilit , il vpp , il vpn rispettivamente di : ac - tcms vs . 
equipment costs were calculated on the basis of mean time of use for each examination and taking into consideration purchase cost ( obtained from ofcial data of the hospital directorate ) and amortisement ( calculated on a temporal basis , at constant annual value , assuming a mean lifespan of 8 years for radiological and cardiological equipment )  . we did not calculate the common costs of the production factors of the radiology and cardiology departments , i.e. 
 factors that support the diagnostic activity , as they do not change with the total yearly number of examinations and are an independent variable , being specic for each department . 
in the evaluation of differential costs , we considered the technical act , ignoring all other costs related to patient management , as done in other published studies [ 16 , 17 ]  . considering that the cycle test , ecg and mdct - ca were performed on an outpatient basis , the cost of the single examinations was calculated on the basis on the italian national health service tariffs . 
in evaluating the cost - effectiveness ratio , we used patterson et al.s il costo differenziale stato calcolato per ogni percorso diagnostico come somma dei costi delle apparecchiature , dei costi dei materiali e dei costi del personale , con le modalit in uso presso il nostro istituto e presso il dipartimento di cardiologia . 
il costo delle apparecchiature stato calcolato in base al tempo medio di utilizzo per esame delle stesse , valutando il costo dacquisto ( ricavato dalla documentazione ufciale della direzione sanitaria ) ed il calcolo dellammortamento ( effettuato su base temporale , a valore annuo costante , assumendo una durata media della vita delle apparecchiature radiologiche e cardiologiche di otto anni )  . non sono stati calcolati i costi comuni dei fattori produttivi interni allistituto di radiologia e del dipartimento di cardiologia , cio quei fattori che garantiscono unattivit di supporto a tutti gli atti diagnostici svolti nel reparto , poich si tratta di costi che non si modicano al variare del numero totale di esami svolti nel periodo annuo e che , essendo specici per ogni struttura , rappresentano una variabile indipendente . 
nella valutazione del costo differenziale ci siamo limitati a considerare latto tecnico , ignorando tutti gli altri costi legati alla gestione del paziente , cos come in altri lavori della letteratura [ 16 , 17 ]  . considerando il fatto che il cicloergometro , lecg e la ac - tcms sono stati eseguiti in regime ambulatoriale senza necessit di ricovero il costo delle singole procedure stato calcolato in base al tariffario del servizio sanitario nazionale applicato anche per esami eseguiti in regime ambulatoriale espletati nella nostra unit operativa . 
 analisi costo / efcacia stata calcolata per ogni percorso lanalisi di costo - efcacia , una forma di piena valutazione economica dove sia i costi che le conseguenze di un programma diagnostico o terapeutico vengono contemporaneamente esaminati . 
usando i dati di sensibilit e specicit , e quindi di accuratezza diagnostica delle singole metodiche stata effettuata lanalisi costo - efcacia dei tre protocolli diagnostici assumendo che il ruolo di esame dirimente era : per il primo protocollo la acc ; per il secondo protocollo il cicloergometro ; per il terzo protocollo la ac - tcms . lefcacia di tali percorsi quindi stata considerata pari a quella dellesame dirimente di quel dato protocollo . 
inne i costi delle diverse metodiche sono stati messi in relazione con laccuratezza diagnostica delle stesse , ottenendo valori di costo / accuratezza per ogni percorso diagnostico . radiol med ( 2013 ) 118 : 12941308 table 2 costs of the different procedures 1301 cost analysis procedure / admission description tariff ( euro ) cycle test mdct - ca cardiological examination ecg diagnostic angiography preprocedure examinations place where procedure is done laboratory tests chest x - ray echocardiogram total pre - procedure examinations haemodynamic room operators involved in the operating room / dedicated clinic qualication execution time personnel costs + regional tax materials , reagents , devices , etc . 
finally , the costs of each method were correlated with its diagnostic accuracy in order to calculate the cost - accuracy values of each diagnostic pathway . results all patients who underwent mdct - ca were at low to intermediate risk of cad , with a discrepancy between symptoms and the clinicallaboratory data . 
it was dened as optimal in 360 / 550 ( 85% ) cases , moderate in 62 / 550 ( 13% ) and poor in 8 / 550 ( 2% ) due to breathing motion artefacts during the scan . 
scans were performed without any dose - saving protocol ( 16.05 msv ) in 41% cases , with retrospective gating and dose modulation ( 8.2 msv ) in 45% and with prospective gating ( 1.2 msv ) in 14% cases . according to image evaluation , 393 / 550 ( 71% ) patients had nonsignicant lesions , 122 / 393 ( 31% ) of whom had no coronary lesions , whereas 157 / 393 ( 29% ) patients had at least one signicant lesion . 
this test conrmed signicant stenosis ( > 50% of coronary lumen narrowing ) in 166 / 128 ( 91% ) patients , and 59 / 128 ( 46% ) patients were revascularised . 
when comparing cca to mdct - ca , the detection of signicant stenosis in a per - patient analysis showed 92% sensitivity , 89% specicity , and 89% and 92% ppv and npv , respectively . 
the overall diagnostic accuracy was 91% . based on risk prole and clinical data , 214 / 550 ( 39% ) patients underwent the cycle test , 15% with positive results and 85% with uncertain or nonsignicant results . 
when considering mdct - ca as the gold standard , the diagnostic performance of the stress test in discriminating patients with signicant stenosis showed a sensitivity and specicity risultati i pazienti sottoposti ad indagine ac - tcms erano soggetti con basso - medio rischio di cad con discrepanza tra sintomatologia e dati clinico - laboratoristici . 
i rilievi anamnestici hanno permesso di distinguere un prolo di rischio basso per la presenza di uno o due fattori di rischio e intermedio per la presenza di due o pi fattori di rischio . 
la qualit delle indagini actcms valutata dal radiologo e basata su un criterio qualitativo stata denita in 360 / 550 ( 85% ) casi buona in 62 / 550 ( 13% ) casi discreta , in 8 / 550 ( 2% ) casi scarsa per artefatti da movimento respiratorio del paziente durante la scansione . 
lacquisizione delle immagini stata effettuata nel 41% dei casi senza alcun tipo di protocollo a risparmio di dose ( 16 , 05 msv ) , nel 45% dei casi con gating retrospettivo e modulazione della dose ( 8 , 2 msv ) e nel 14% dei casi con gating prospettico ( 1 , 2 msv )  . nellambito della valutazione delle immagini in 393 / 550 ( 71% ) casi non vi erano lesioni signicative , dei quali 122 / 393 ( 31% ) erano cad free , cio totalmente privi di lesioni coronariche ; nei rimanenti 157 / 393 ( 29% ) pazienti sono state riconosciute lesioni signicative ad almeno un segmento coronarico . 
dei 157 pazienti risultati positivi allac - tcms , 128 / 157 ( 82% ) sono stati sottoposti ad acc , che ha confermato la stenosi > 50% del lume coronarico in 116 / 128 ( 91% ) pazienti . 
il confronto diretto tra acc e ac - tcms nella valutazione di stenosi signicative mediante analisi per paziente ha rilevato una sensibilit pari a 92% , una specicit pari a 89% , un vpp e vpn pari a 89 % e 92% rispettivamente . 
laccuratezza diagnostica globale della ac - ctms risultata essere pari a 91% . sulla base dei proli di rischio e dei dati clinico anamnestici precedentemente allac - tcms sono stati sottoposti a cicloergometro 214 / 550 ( 39% ) pazienti di cui solo il 15% risultato positivo mentre l85% dubbio o non signicativo . 
 considerando come riferimento la ac - tcms , la capacit diagnostica della prova da sforzo nella identicazione di pazienti con lesioni signicative ha dimostrato una sensibilit e specicit pari a 21% e 87% , con un vpp e vpn di 42% e 70% rispettivamente ( tabella 3 )  . il costo di ogni percorso diagnostico stato calcolato sulla base della somma dei costi delle differenti procedure e riportato in tabella 4 . 
i protocolli 2 e 3 evitando di sottoporre i pazienti negativi a procedure angiograche , consentono un risparmio medio per ogni paziente negativo di 1323 euro e 1384 euro rispettivamente . 
cca when evaluating patients with signicant coronary artery stenosis tabella 3 performance diagnostica espressa dalla prova da sforzo nella determinazione di pazienti con lesioni signicative vs angiograa coronarica mediante tomograa computerizzata multistrato ( ac - tcms ) cycle test vs . 
 by avoiding the need for cca , the second and third pathways allow average savings of 1 , 323 euro and 1 , 384 euro , respectively , in the case of negative patients . regarding the cost - effectiveness analysis , for each diagnostic pathway , we obtained a curve representing the trend of improvement in relation to the pretest percentage of cardiovascular risk ; the curves of three pathways are compared in figure 4 . discussion few studies have reported on the real diagnostic accuracy of mdct - ca obtained in a clinical setting , which reects the effective performance of the technique in routine practice [ 4 , 19 , 20 ]  . 
in clinical practice , the cardiologist and the clinician can use the information provided by the method to send the patient to an appropriate diagnostic pathway with optimal accuracy [ 20 ]  . consistent with the literature , the high positive and negative predictive values found in our series gives mdct - ca a gatekeeping role in relation to cca . 
despite this , our data conrm a valid diagnostic performance of mdct - ca also in a real clinical setting [ 4 , 9 , 19 , 20 ]  . the suboptimal diagnostic performance of the stress test in stata ottenuta una curva che rappresenta il trend di miglioramento in rapporto alla percentuale pre - test del rischio cardiovascolare ; le curve dei tre percorsi sono messe a confronto nella figura 4 . discussione attualmente pochi studi riportano la reale accuratezza diagnostica estrapolata da un contesto clinico , che consiste nella effettiva performance della metodica sul campo [ 4 , 19 , 20 ]  . 
nella pratica clinica , il cardiologo ed il clinico possono utilizzare le informazioni ottenute da questa metodica per indirizzare con maggior accuratezza il paziente al percorso diagnostico terapeutico ottimale [ 20 ]  . 
 in linea con i dati della letteratura anche nella nostra casistica lelevato valore predittivo positivo e negativo della ac - tcms gli conferisce un ruolo di spartiacque nei confronti della coronarograa . 
nonostante ci i nostri dati confermano unottima performance diagnostica dellac - tcms anche in un contesto clinico reale [ 4 , 9 , 19 , 20 ]  . la scarsa performance diagnostica espressa dalla prova da sforzo nella determinazione di pazienti con lesioni signicative ottenuta nel nostro lavoro aderente ai risultati espressi in precedenti lavori pubblicati su questo argomento [ 10 , 11 ]  . 
because the diagnostic performance of this test is inadequate for this patient population , the purpose of our study was to modify the diagnostic algorithm by incorporating the use of mdct - ca . 
questi daranno informazioni utili sulla riduzione di riserva coronarica causata dalle lesioni evidenziate anatomicamente dalla tc , cos da indirizzare a procedure invasive di rivascolarizzazione solo i pazienti con lesioni ateromasiche funfig . 
 these tests could give additional useful information about the reduction of coronary reserve resulting from the lesions depicted by mdct , so as to send only those patients with functionally signicant cad to invasive revascularisation procedures . 
this modied algorithm changes the approach to diagnostic cca and our study , as many others before , shows how this can lead to several disadvantages compared with a multi - step approach [ 16 ]  . 
cost - effectiveness analysis correlates the percentage of correct diagnoses to the cost necessary to reach them ; this aspect provides an additional indicator to mere diagnostic accuracy . on the basis of our results and the recent literature [ 11 , 16 ] it is clear that the introduction of mdct - ca improves diagnostic performance ; at the same time , it is important to emphasise when to use it in the clinical workup . 
the modied diagnostic pathway with mdct - ca provides a greater overall diagnostic accuracy , but it takes on a high value of cost - effectiveness if mdct - ca is considered the rst - level examination in place of the cycle test . 
this leads to higher cost - effectiveness values compared with the standard pathway , which , even though burdened by the high cost of cca , obtained fairly good cost - effectiveness values as a result of its high sensitivity . 
the use of mdct - ca as a screening test is an early , effective and relatively inexpensive diagnostic tool in a population in which the stress test has limited sensitivity . 
consequently , it is preferable to send to cca only patients with positive ndings at mdct - ca and at low to intermediate risk , and to use cca only for revascularisation procedures . 
our data indicate that the low diagnostic accuracy of the stress test ( 66% ) , especially in low - risk patients ( in whom accuracy falls to about 50% ) , makes the second diagnostic protocol the least economically viable . according to the cost - effectiveness analysis based on our data , a single mdct - ca costs about 230.03 euro , whereas cca costs about 1 , 551 euro . 
mdct - ca has a better cost - effectiveness ratio compared with cca as long as the pretest probability is < 86% , which corresponds to low to intermediate risk patients . the results of our study demonstrate how , based on clinical and anamnestic data , no signicant lesions were detected zionalmente signicative . 
tale algoritmo modicato cambia dunque lapproccio mirato verso lacc diagnostica , e il nostro studio , come altri precedenti , mostra come ci comporti diversi svantaggi , confrontato con un approccio a stadi [ 16 ]  . 
 lanalisi costo / efcacia mette in relazione la percentuale di diagnosi corrette con il costo necessario a raggiungerle ; questo aspetto fornisce quindi un indicatore aggiuntivo alla semplice accuratezza diagnostica . 
 dai risultati ottenuti e dalla recente letteratura [ 11 , 16 ] si pu evincere come lintroduzione della ac - tcms migliori la performance diagnostica ; al tempo stesso importante sottolineare il punto in cui essa viene inserita nel workup clinico . 
il protocollo diagnostico modicato con lac - tcms fornisce una maggiore accuratezza diagnostica globale , ma acquisisce un alto valore di costo / efcacia se la ac - tcms viene posta come esame di primo livello , al posto del cicloergometro . 
in tal modo si ottengono valori di costo / efcacia maggiori del protocollo standard , che pur gravato dagli alti costi dellacc , otteneva dei valori di costo / efcacia discreti dovuti allalta sensibilit della stessa . 
 vista la popolazione presa in considerazione , di individui con rischio medio - basso , la metodica che fornisce il migliore rapporto costo / efcacia risulta essere lac - tcms . 
 lutilizzo dellacc con il solo scopo diagnostico , pur garantendo una sensibilit del 100% , gravato da costi elevati , di conseguenza preferibile inviare allacc solo i casi positivi selezionati tramite lac - tcms ed utilizzare lacc solo per procedure interventistiche di rivascolarizzazione nei pazienti a basso - medio rischio . 
dai nostri dati si pu evincere che la scarsa accuratezza del cicloergometro ( 66% ) , specie nei pazienti a basso rischio ( dove la sua accuratezza scende a circa il 50% ) , rende il secondo protocollo diagnostico , addirittura il meno conveniente in termini economici . 
secondo una analisi di costo - efcacia basata sui nostri dati la actcms fa registrare un costo totale di 230 , 03 euro mentre la coronarograa fa registrare un costo totale 1551 euro . 
la ac - tcms presenta un rapporto costo - efcacia pi favorevole rispetto alla coronarograa no all86% di probabilit pre - test , ossia in condizioni di rischio cardiovascolare basso ed intermedio . i risultati del nostro studio mostrano come sulla base della clinica e dei dati anamnestici nei 2 / 3 circa dei pazienti non siano state riscontrate lesioni signicative , abbreviando quindi gli iter terapeutici e migliorando la performance diaradiol med ( 2013 ) 118 : 12941308 1307 in two of three patients examined , thus shortening their therapeutic pathway and improving diagnostic performance in assessing low to intermediate risk patients . 
there were , however , many lesions with stenosis 50% , which necessitated a comparison with cca , stress ecg or scintigraphy , conrming the presence of borderline lesions but excluding indications for treatment with angioplasty or stenting . 
 our evaluation was carried out on a patient - based analysis instead of a per - segment or a per - vessel analysis , so as not to exclude from further investigation patients potentially affected by signicant cad . gnostica nella valutazione del paziente a rischio . 
molte sono per le lesioni con stenosi 50% che hanno necessitato di un confronto mediante coronarograa o eco - stress o scintigraa , confermando la presenza di lesione borderline , ma escludendone lindicazione al trattamento mediante angioplastica o stent . 
la nostra valutazione stata effettuata su unanalisi per paziente e non per segmento o vaso , in modo da cercare di non escludere da eventuali ulteriori indagini soggetti potenzialmente affetti da malattia coronarica signicativa . conclusioni conclusions our study , in agreement with the literature , conrms the better diagnostic performance of mdct - ca compared with the stress test and its similar accuracy to cca . 
in addition , the use of a pathway that considers mdct - ca as a gatekeeper to identify patients to send to cca is advantageous in terms of cost and diagnostic effectiveness . il nostro studio , in linea con i dati della letteratura , conferma una miglior performance diagnostica dellac - tcms nei confronti del test da sforzo ed unaccuratezza simile a quella dellacc . 
inoltre , lutilizzazione di un protocollo che prevede lac - tcms come spartiacque principale per identicare i pazienti da inviare allacc , risulta vantaggioso in termini di costo e di efcacia diagnostica . 
29 , xinquan road , fuzhou 350001 , china 3department of pathology , ruijin hospital , shanghai jiao tong university school of medicine , shanghai , china correspondence to : xiao - yi ding , tel . : + 86 - 18 - 918967155 , fax : + 86 - 21 - 64150737 , e - mail : dxyrj@hotmail.com received : 17 february 2012 / accepted : 26 march 2012 / published online : 27 may 2013 springer - verlag 2013 abstract purpose . 
radiography ( n = 9 ) , magnetic resonance imaging ( mri ) ( n = 6 ) , computed tomography ( ct ) ( n = 3 ) and clinical course of nine patients ( five males and four females ; mean age , 26 years ) with pathologically confirmed gcro were retrospectively reviewed . 
an ill - defined margin surrounding a predominantly osteolytic lesion was detected at the proximal tibia ( n = 7 ) or femur ( n = 2 ) on imaging studies . 
lo scopo di questo studio stato di rivedere la presentazione clinica , le caratteristiche allimaging , la patologia e gli esiti di pazienti con osteosarcoma ricco in cellule giganti delle ossa lunghe materiali e metodi . 
radiografia ( n = 9 ) , imaging con risonanza magnetica ( mri ) ( n = 6 ) , tomografia computerizzata ( ct ) ( n = 3 ) e decorso clinico di nove pazienti ( cinque maschi e quattro femmine ; et media 26 anni ) con gcro confermato anatomo - patologicamente sono stati esaminati retrospettivamente . 
allimaging stato riscontrato un margine indefinito che circonda una lesione prevalentemente osteolitica a livello della tibia prossimale ( n = 7 ) o del femore ( n = 2 )  . 
la massima dimensione tumorale stata in media di 4 , 7 cm5 , 2 cm7 , 8 c microscopicamente , i tumori erano composti di cellule tumorali atipiche con scarsa formazione di osteoide e cellule giganti multinucleate . 
tre pazienti erano morti e 6 erano in vita allultimo follow - up . radiol med ( 2013 ) 118 : 13241334 1325 shows an osteolytic lesion with locally spared new bone formation in the metaphysis and / or metaepiphysis on imaging . 
histologically , the atypical tumour cells with osteoid formation and multinucleated giant cells are the key factor in the diagnosis and differential diagnosis . keywords bone neoplasms giant cell tumour of bone osteosarcoma tomography x - ray computed tomography magnetic resonance imaging conclusioni . 
istologicamente , le cellule tumorali atipiche con formazione di osteoide e le cellule giganti multinucleate sono i fattori chiave nella diagnosi e nella diagnosi differenziale . parole chiave neoplasia ossea tumore osseo a cellule giganti osteosarcoma tomografia computerizzata risonanza magnetica introduction osteosarcoma is the most common nonhaemopoietic primary malignant tumour of bone and in which neoplastic cells produce osteoid [ 1 ]  . 
for giant cell - rich osteosarcoma ( gcro ) , the multinucleated giant cells are so obvious that these cells cover up the heteromorphic tumour cells of osteosarcoma , and histological images of many uniformly distributed multinucleated osteoclast - like giant cells are similar to giant cell tumour of bone [ 2 ]  . 
gcro is usually misdiagnosed as giant cell tumour of bone , as they have similar radiological and pathological features , which have seldom been reported in the literature [ 3 , 59 ]  . 
owing to the different prognoses and treatment strategies for these tumours , it is important to make the right diagnosis [ 8 ]  . to the best of our knowledge , there is a paucity of literature regarding patients with gcro . 
the purpose of this study was to review clinical , radiological and pathological features of gcro of long bones . materials and methods nine consecutive patients admitted to the authors institution between february 1997 and december 2011 were reviewed . 
histological criteria to define gcro were as follows : on lowpower view , these lesions show multinucleated giant cells simulating a giant cell tumour ; on high power , cytological anaplasia of stromal cells and malignant osteoid production can be identified [ 5 , 11 , 12 ]  . in the initial radiological diagnosis , six patients were diagnosed as having giant cell tumour ; one patient each was diagnosed with malignant tumour , possible osteosarcoma and osteosarcoma . 
detailed diagnostic results are shown in table 3 . results clinical findings presenting symptoms were pain duration for < 3 months in three patients and between 3 and 6 months in three . 
average symptom duration was 7 ( range 224 ) months ( table 4 )  . 1326 radiol med ( 2013 ) 118 : 13241334 radiol med ( 2013 ) 118 : 13241334 1327 imaging findings seven osteosarcomas were in the proximal tibia , one in the proximal femur and one in the distal femur . 
in brief , radiographic findings of lysis were seen in nine patients ; eccentric growth in six ; ossification in four ; expansile growth , cortical destruction and soft tissue extension in three ; periosteal reaction and joint involvement in two . three patients underwent ct scanning that clearly showed a large area of low - attenuated mass with focal bone formation . 
summarising , ct features of eccentricity , ossification , lysis , cortical destruction and soft tissue extension were showed in three patients , expansile growth and joint involvement in two and periosteal reaction in one . mr scanning was performed in six cases , of which five lesions were eccentric and one was centric . 
there were different degrees of long t1 and long t2 concentrated or scattered areas of necrosis , and no evidence 1328 table 3 initial radiological and pathological diagnosis of giant cell - rich osteosarcoma tabella 3 diagnosi iniziale radiologica e patologica dellosteosarcoma ricco in cellule giganti patient no . 
 initial radiological diagnosis initial pathological diagnosis radiol med ( 2013 ) 118 : 13241334 giant cell tumour malignant tumour giant cell tumour giant cell tumour possible osteosarcoma giant cell tumour osteosarcoma giant cell tumour giant cell tumour giant cell - rich osteosarcoma giant cell - rich osteosarcoma giant cell tumour giant cell tumour giant cell - rich osteosarcoma giant cell tumour giant cell - rich osteosarcoma giant cell - rich osteosarcoma giant cell - rich osteosarcoma fig . 
on the whole , mri features , regarding lysis , were displayed in six patients : eccentricity , ossification and cystic change in five , cortical destruction and soft tissue extension in four , joint involvement in three and expansile growth in one . pathological features osteoid formation in the final multispot sampling . 
heteromorphism of giant cells was not obvious with pallid - stained cytoplasm . discussion all tumours were composed of atypical tumour cells and as subtypes of conventional osteosarcoma , gcro and other subtypes are listed separately as unusual histological radiol med ( 2013 ) 118 : 13241334 1329 forms [ 1 ]  . 
about 1325% of cases of osteosarcoma , accompanied by a few osteoclast - like giant cells , can be seen in haemorrhagic and perivascular areas [ 13 , 14 ] , but the histology of gcro with a large number of osteoclast - like giant cells similar to giant cell tumour is rare . 
in our collection of 305 cases of osteosarcoma , only nine cases presented the giant cell - tumour - like structure , accounting for 2.9%. mean age of all patients at diagnosis , including those in this study , was 24.7 ( range 667 ) years . 
in all reported cases , including the cases in this study , 12 affected the femur , 11 the tibia and one each the radius , rib , mandible and maxilla , respectively . 
gcro was distinguished from conventional osteosarcoma on the basis of the predominantly osteolytic lesion without notable ossification or periosteal reaction on imaging findings , and on histological findings of numerous giant cells with scanty osteoid . 
the basic proliferating component of giant cell - rich malignant fibrous histiocytoma is a fibrohistiocytic cell exhibiting a storiform or pinwheel pattern and never forming bone or osteoid directly [ 15 , 16 ]  . 
except for osteoclast - like giant cells , heteromorphism and mitoschisis of tumour cells with more or less osteoid in gcro can be seen , whereas many uniformly distributed osteoclast - like giant cells , interstitial oval or short spindle - shaped mononucleated cells without osteoid of tumour can be seen in giant cell tumour . 
gcro should be differentiated from malignant giant cell tumour . the radiographic appearances of malignant giant cell tumours are similar to those of benign giant cell tumours [ 19 ]  . 
visibile enhancement diffuso e marcato , eccetto che per larea necrotica dopo la somministrazione endovenosa di mdc ( frecce nere spesse )  . radiol med ( 2013 ) 118 : 13241334 1331 fig . 
diffuse or lacelike strong enhancement was seen in the mass , except for the area of necrosis ( thin black arrows ) or bone formation ( thick black arrows )  . 
4a - f ragazzo di 18 anni con gcro nella tibia prossimale ( paziente n 2 ) : a , b rm ( immagine t1 - pesata ) : la lesione ha prevalentemente segnale isointenso ( freccia bianca ) con focale ipointensit ( freccia nera ) rispetto al muscolo . 
c , d rm ( immagine t2 - pesata e immagine stir ) : il tumore mostra segnale eterogeneo iperintenso ( freccia bianca ) contenente area di focale ipointensit ( freccia nera )  . 
e , f rm ( acquisizione con soppressione del grasso dopo mdc ) : intenso enhancement diffuso o cordoniforme nella massa tranne che nellarea di necrosi ( frecce nere sottili ) o di neoproduzione ossea ( frecce nere spesse )  . 
 la lesione eccentrica ha distrutto la corticale focale e la superficie articolare ed ha coinvolto le articolazioni del ginocchio ( freccia bianca )  . of osteoid by the malignant spindle cells is not seen in malignant giant cell tumours , and an area of giant cell tumour is present in addition to verified areas of sarcomatous stroma [ 20 ]  . 
in our study , five of the nine patients showed a soft tissue mass with different degrees of cortical destruction , which may be related with tumour size and eccentric growth . 
we also found that tumours in the epiphyses of proximal tibias were more likely to cause soft tissue extensions and destroy the knee joints , which may be related to 1332 radiol med ( 2013 ) 118 : 13241334 fig . 
5a - f ragazza di 19 anni con gcro nel femore distale ( paziente n 5 ) : a , b rm ( immagine t1 - pesata ) : la lesione mostra segnale isointenso ( frecce nere ) con aree con intensit di segnale leggermente inferiore ( frecce bianche )  . 
c rm ( immagine t2 - pesata ) : il tumore mostra un segnale ad alta intensit diffuso ed eterogeneo ( freccia nera ) con aree focali di segnale ipointenso ( freccia bianca )  . 
d - f rm con mdc : enhancement diffuso e marcato nella maggior parte della massa tumorale tranne che per le aree di necrosi ( frecce nere ) e di neoproduzione di tessuto osseo ( freccia bianca )  . the predominantly cancellous bone of the epiphyses . 
in our study , due to lack of knowledge regarding the spectrum of gcros and nonspecific osteolytic destruction with limited ossification on imaging , six patients were misdiagnosed as having giant cell tumour at initial radiological diagnosis . the histopathologic characteristics that identify gcro include the presence of numerous osteoclast - like giant cells , with scanty osteoid formation by the tumour cells [ 4 , 10 , 11 ] : but osteoid formation in some gcros was very limited , and heteromorphism of mononuclear tumour cells was not obvious . 
6a - c gcro : a lesion showed multinucleated giant cells ( arrows ) simulating a giant cell tumour [ hematoxylin and eosin ( h&e ) , 40 ]  . 
6a - c microfotografie di gcro : a la lesione mostra cellule giganti multinucleate ( frecce ) che simulano un tumore a cellule giganti ( ematossilinaeosina , 40 )  . 
c numerose cellule giganti multinucleate osteoclasto - simili ( frecce spesse ) possono essere viste tra le cellule tumorali atipiche , rotonde , ovali , fusiformi , fusiformi brevi e poligonali ( frecce sottili ) ( ematossilina - eosina , 360 )  . diagnosed as a giant cell tumour in interoperatively surgical frozen section , and paraffin - section review established a diagnosis of gcro . 
histological examination could only depict a small area , which may have complicated the diagnosis , especially as the tissue was drawn from the site of converted osteoclast - like giant cells with inconspicuous osteoid . 
pathological tissues should be drawn from multiple sites , so heteromorphism and pathological mitosis of tumour cells should be observed carefully . poor prognostic indicators include the presence of metastasis and local recurrence . 
these observations reflect the similar prognosis of gcro , compared with conventional osteosarcoma . conclusions gcro is a rarer variant of , and has very close resemblance to , giant cell tumour . 
prognosis is similar to that of conventional osteosarcoma . acknowledgements this study was supported by the national natural science foundation of china ( project number : 81072188 )  . conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . 
this study assessed the diagnostic accuracy of coronary artery stenosis evaluation obtained by three readers at different levels of training or at different points of the learning curve proposed by the international guidelines . 
three radiologists in training with different levels of experience in mdct - ca scored 50 cases at various time points of the learning curve : baseline , 4 weeks , 8 weeks and 6 months . 
the trainee radiologists evaluated the degree of stenosis on each coronary segment , and overall accuracy was calculated on a per - segment , pervessel and per - patient basis . 
all readers improved analysis accuracy per segment ( range , 7390% ) ; sensitivity reached 45% per segment , 84% per vessel and 93% per patient ; specicity was 99% per segment and vessel and 98% per patient . 
valutare laccuratezza diagnostica nella stima di stenosi coronarica con langiograa coronarica mediante tcms ( ac - tcms ) ottenuta da tre lettori nei vari livelli di training proposti dalle linee guida internazionali come curva di apprendimento . 
tre lettori medici in formazione con esperienza in ac - tcms differente hanno eseguito lanalisi sistematica delle ac - tcms di 50 pazienti in diversi step della curva di apprendimento : iniziale , a 4 settimane , 8 settimane , 6 mesi . 
tutti i lettori hanno incrementato la loro accuratezza ( range 7390% ) nellanalisi per segmento ; la sensibilit con valori massimi per segmento pari a 45% , per vaso a 84% e per paziente a 93% ; la specicit con valori massimi per lanalisi per segmento e vaso pari a 99% e per paziente pari a 98% . 
sebbene tutti i lettori abbiano migliorato la loro performance diagnostica aumentando la loro esperienza in ac - tcms , pu essere necessario un tempo pi lungo per raggiungere unesperienza adeguata in actcms tale da consentire una valutazione indipendente . keywords mdct - ca learning curve diagnostic accuracy training coronary artery stenosis parole chiave ac - tcms curva di apprendimento accuratezza diagnostica training stenosi coronarica 1282 introduction radiol med ( 2013 ) 118 : 12811293 introduzione coronary angiography using multidetector computed tomography ( mdct - ca ) is a recent technique for nonivasive study of coronary arteries . 
additionally , the evaluation of coronary stenoses was done in a qualitative manner , so that diagnostic accuracy might vary as a function of the operators level of expertise [ 4 , 5 ]  . to guarantee a high level of overall accuracy , the european society of cardiology and the american college of cardiology ( esc , acc ) have established minimum requirements in terms of number of cases interpreted and learning hours to identify three training steps , dening three levels of prociency [ 1 , 6 ]  . 
 the aim of this study was to assess diagnostic accuracy coronary stenosis evaluation by three readers with different levels of prociency in mdct - ca , that is , at one of the three different points of the learning curve proposed by the international guidelines . 
 inoltre , la valutazione delle stenosi coronariche effettuata in modo qualitativo , per cui laccuratezza diagnostica pu variare a seconda dellesperienza delloperatore [ 4 , 5 ]  . al ne di garantire unaccuratezza globale elevata le societ europee e americane di radiologia e cardiologia ( esc e acc ) hanno denito dei requisiti minimi di casi letti e ore di formazione distinti in step di formazione per denire tre livelli di esperienza minima garantita [ 1 , 6 ]  . 
 scopo del nostro lavoro , pertanto , valutare laccuratezza diagnostica nella stima di stenosi coronarica ottenuta da tre lettori con differente esperienza in ac - tcms nei vari livelli di training proposti dalle linee guida come curva di apprendimento . 
 materials and methods sample population materiali e metodi popolazione campione we evaluated 50 patients ( 32 men and 18 women ; mean age , 63.2 years ) who underwent 64 - slice mdct - ca examinations . 
all patients provided their written informed consent to undergo the examination . sono stati valutati 50 pazienti ( 32 maschi e 18 femmine , et media 63 , 2 anni ) sottoposti ad ac - tcms a 64 strati . 
tutti i pazienti sottoposti allo studio hanno fornito consenso informato scritto allesame . indications indicazioni all patients enrolled for the mdct - ca study had clinical indications for the examination : atypical chest pain of uncertain origin discrepancy between clinical data and challenge tests exclusion of occlusive coronary disease in patients tutti i pazienti arruolati allesecuzione di ac - tcms avevano indicazioni cliniche allesecuzione dellesame per : dolore toracico atipico di dubbia origine ; discordanza tra clinica e test provocativi ; esclusione di coronaropatia occlusiva in pazienti da sotschedules for major surgery all patients underwent conventional coronary angiography ( cca ) within 2 weeks of the ct examination . toporre a interventi di chirurgia maggiore . tutti i pazienti considerati sono stati sottoposti ad angiograa coronarica convenzionale ( acc ) entro due settimane dallesecuzione dellesame tc . 
in order to calculate each patients risk prole , we considered the main risk factors for tutti i pazienti arruolati per lo studio presentavano un prolo di rischio per coronaropatia medio / basso . 
al ne di prolo di rischio radiol med ( 2013 ) 118 : 12811293 1283 atherosclerosis and coronary artery disease : overweight status , with body mass index ( bmi ) > 25 , history of smoking , hypertension , dyslipidaemia or diabetes and family history of acute cardiac events . 
the prevalence of disease was 42% ( table 1 )  . exclusion criteria calcolare il prolo di rischio per ogni paziente sono stati valutati i fattori principali responsabili di aterosclerosi e quindi di coronaropatia , vale a dire il sovrappeso con indice di massa corporea ( body mass index , bmi ) > 25 , lanamnesi positiva per fumo , ipertensione , dislipidemia , diabete e familiarit positiva per eventi cardiaci acuti . 
 metodi di valutazione arruolamento lettori prereading training before analysing the sample images , all readers received tuition from a radiologist ( gold standard , gs ) with 6 years experience in cardiac ct . 
at the end of the tuition period , the gs radiologist provided practical training at a dedicated mdct - ca workstation by analysing ten cases not included in the study . 
randomisation using the function randbetween in ofce excel 2007 was done to eliminate the repetition bias associated with reading the same case over time and to maintain blinded reading at each phase of the learning curve . 
agreement between the gs reading and cca data was considered the standard reference . temporal criteria the phases of the learning curve were established followtre lettori ( r1 , r2 e r3 ) , medici in formazione in diagnostica per immagini hanno eseguito lanalisi sistematica delle ac - tcms . 
ciascun lettore aveva una differente esperienza in angiograa coronarica tcms : il primo ( r1 ) nulla , il secondo ( r2 ) di 6 mesi e il terzo ( r3 ) di 1 anno . 
 training pre - lettura a tutti i lettori , prima dellinizio dellanalisi delle immagini campione , sono state impartite lezioni da parte di un radiologo ( gold standard , gs ) esperto in cardio - tc ( 6 anni ) in tecnica di esecuzione dellesame cardio - tc , tecnica di analisi delle immagini , semeiotica radiologica dellanatomia delle arterie coronarie , delle varianti , della placca coronarica . 
in aggiunta , sono stati consegnati due testi specici in ac - tcms per fornire basi di tecnica cardio - tc e semeiotica cardiologica applicata . al termine delle lezioni , stato effettuato da parte del radiologo gs un tutoraggio pratico alla workstation dedicata alla lettura degli esami ac - tcms mediante la analisi di dieci casi esclusi dallo studio che sono stati ricostruiti e analizzati mediante analisi per segmento , vaso principale ( arteria coronaria destra , tronco comune , arteria discendente anteriore e arteria circonessa ) e paziente , commentati sulla base delle notizie clinico - anamnestiche e , inne , refertati . randomizzazione dei pazienti i lettori ( r1 , r2 e r3 ) non erano in nessuna fase della curva di apprendimento a conoscenza dei dati anagraci dei pazienti , delle indicazioni cliniche allesame , della presenza o meno di stent o bypass . 
la randomizzazione stata eseguita al ne di annullare il bias di ripetizione dellerrore associato alla lettura dello stesso caso nel tempo e al ne di mantenere la lettura in cieco da parte dei lettori in ogni fase della curva . 
different reading phases were dened : phase 0 : reading of the data set after initial training phase 1 : reading at 4 weeks , corresponding to training phase 2 : reading at 8 weeks , corresponding to training phase 3 : reading at 6 months , corresponding to training level 1 level 2 level 3 training between readings during the interval between readings , readers were given tools to enable them to acquire the necessary competence to proceed to the next training level . 
all cases were commented on with the gs , and the results obtained were compared with those of the cca examination , if performed , or with the results of the challenge tests . 
 mdct - ca parameters analysed all three readers and the gs carried out data - set analysis using detres 1975 classication of the coronary arteries into 16 segments [ 8 ]  . 
for each patient , a form was lled in summarising per - segment analyses . coronary circulation dominance coronary circulation was distinguished into right dominant , left dominant or balanced depending on whether the posterolateral branch ( segment 4b ) and the posterior interventricular artery ( segment 4a ) originated from the rca , the lcx or both [ 9 , 10 ]  . segment classication segments were classied according to the 16 - segment classication of the american heart association ( aha ) [ 8 ]  . 
 the rca was classied as segments 14 , the lm as segment 5 , the lad and its diagonal branches as segments 610 and the lcx and its obtuse marginal branches as segments 1115 . 
the intermediate branch , if present , was classied as segment 16 . segment patency each segment was initially classied as patent or occluded depending on whether contrast material could be identied within its lumen . la randomizzazione dei dataset stata effettuata da parte del radiologo tutor ( gs )  . lo stesso radiologo gs che ha selezionato la popolazione campione ha effettuato la lettura mediante analisi dei dataset per segmento , per vaso e per paziente . 
lagreement tra la lettura del gs con i dati della acc stato considerato quale lettura standard di riferimento . criteri temporali le fasi della curva di apprendimento hanno seguito le linee guida indicate dalla societ americana di cardiologia [ 7 ]  . 
 sono state denite differenti fasi di lettura : fase 0 : lettura dei dataset alla ne del training iniziale ; fase 1 : lettura a 4 settimane con livello di training 1 ; fase 2 : lettura a 8 settimane con livello di training 2 ; fase 3 : lettura a 6 mesi con livello di training 3 . training inter - lettura nellintervallo tra una lettura e la successiva sono stati forniti ai vari lettori gli strumenti per acquisire la competenza sufciente a passare al livello di training successivo . 
tutti i lettori hanno partecipato attivamente alla preparazione dei pazienti da sottoporre a ac - tcms , allesecuzione tecnica dellesame , alla ricostruzione dei dataset , alla valutazione prima in cieco e poi mediante supervisione del radiologo tutor degli esami acquisiti . 
tutti i casi sono stati commentati con il tutor ( gs ) e i risultati ottenuti sono stati confrontati con lacc se effettuata o con i risultati dei test provocativi . 
 parametri ac - tcms in analisi tutti i lettori r1 , r2 e r3 e il tutor gs hanno effettuato lanalisi dei dataset utilizzando lo schema di segmentazione coronarica a 16 segmenti di detre [ 8 ]  . 
per ogni paziente stato compilato un modulo che riassumeva schematizzando lanalisi per segmento . dominanza circolo coronarico la dominanza del circolo coronarico stata distinta in destra , sinistra o bilanciata a seconda che il ramo postero - laterale ( segmento 4b ) e larteria interventricolare posteriore ( segmento 4a ) originassero , rispettivamente , dallarteria coronaria destra , dallarteria circonessa o da entrambe [ 9 , 10 ]  . 1286 degree of stenosis the degree of stenosis resulting from brofatty , mixed or calcied plaques was rated according to criteria reported in recent guidelines [ 11 ] , namely : 020% = wall irregularities ; 2050% = nonsignicant stenosis ; 5070% = signicant stenosis ; 70100% = subocclusive stenosis . condence in evaluation condence was dened as the subjective degree of condence in determining patency or nonpatency of a segment and its degree of stenosis . 
the qualitative scale of condence was : 1 = poor condence ; 2 = air condence ; 3 = good condence . image quality data - set quality in general and image quality for segment analyses were subjectively rated as : 1 = poor ; 2 = fair ; 3 = excellent . presence of stents / bypass grafts the possible presence of a stent and its patency were recorded for each segment . 
for each patient , the readers recorded the possible presence of an aortocoronary bypass graft , its course and its patency . calcium burden per segment for each segment , readers subjectively rated the calcium burden as : 0 = absent ; 1 = moderate ; 2 = high . radiol med ( 2013 ) 118 : 12811293 classicazione segmenti la classicazione per segmenti utilizzata segue lo schema a 16 segmenti dellaha [ 8 ]  . 
larteria coronaria destra stata classicata nei segmenti da 1 a 4 , il tronco comune in segmento 5 , larteria discendente anteriore e i suoi rami collaterali diagonali dal segmento 6 al segmento 10 , larteria circonessa e i suoi rami collaterali marginali ottusi dal segmento 11 al segmento 15 . 
leventuale presenza di un ramo intermedio stata classicata come segmento 16 . perviet del segmento ogni segmento stato inizialmente classicato come pervio o occluso a seconda che nel lume del segmento fosse identicato mezzo di contrasto . grado di stenosi il grado di stenosi sostenuto da placche brolipidiche , mi ste o calciche stato distinto secondo i criteri delle recenti linee guida [ 11 ] : stenosi 020% irregolarit parietali ; stenosi 2050% stenosi non signicativa ; stenosi 5070% stenosi signicativa ; stenosi 70100% stenosi sub - occlu siva . condenza nella valutazione la condenza nella valutazione stata denita come il grado soggettivo di sicurezza nel determinare la perviet o meno del segmento e il grado di stenosi . 
il criterio qualitativo di condenza stato distinto in : 1 = scarsa condenza ; 2 = discreta condenza ; 3 = buona condenza . data set evaluation times qualit dellimmagine for each patient , the time taken to read the examination was recorded in min from data - set opening to completing the analysis . la qualit del dataset in generale e delle immagini per lanalisi del segmento stata valutata in modo soggettivo e distinta in : 1 = scarsa ; 2 = discreta ; 3 = ottima . statistical analysis intraobserver diagnostic accuracy diagnostic accuracy in evaluating the coronary tree and identifying the degree of coronary stenoses ( 50% and > 50% ) at the segment ( segments 116 ) , vessel ( rca , lm , lad , lcx ) and patient level allowed us to obtain values of sensitivity , specicity and positive and negative predictive values ( ppv and npv ) for each reader at each phase of the learning curve . presenza di stent / by - pass leventuale presenza di stent e la sua perviet stata registrata per ogni segmento . 
per ogni paziente stata registrata leventuale presenza di bypass aorto - coronarico , il suo decorso e la sua perviet . carico di calcio per segmento per ogni segmento , il lettore ha giudicato il carico di calcio ateromasico e distinto soggettivamente in : 0 = assente ; 1 = discreto carico di calcio ; 2 = elevato carico di calcio . radiol med ( 2013 ) 118 : 12811293 results mdct - ca parameters coronary circulation dominance 1287 tempo di lettura del dataste per ogni paziente stato registrato il tempo di lettura dellesame espresso in minuti dallapertura del dataset alla ne dellanalisi . coronary circulation dominance was correctly identied by r1 in 44 / 50 cases ( 88% ) at time 0 and in 50 / 50 ( 100% ) at time 3 ; by r2 in 45 / 50 cases ( 90% ) at time 0 and in 50 / 50 at time 3 ( 100% ) ; and by r3 in 46 / 50 cases ( 92% ) at time 0 and in 50 / 50 ( 100% ) at time 3 ( table 2 )  . 
 analisi statistica accuratezza diagnostica intra - osservatore segment classication segments were correctly classied in the initial phase in 740 / 800 cases ( 92.5% ) by r1 , in 704 / 800 cases ( 88% ) by r2 and in 750 / 800 cases ( 93.7% ) by r3 ; in the last phase all readers correctly classied all segments [ 800 / 800 cases ( 100% ) ]  . 
 classicazione segmenti i segmenti sono stati classicati correttamente dal lettore 1 nella prima fase in 740 / 800 casi ( 92 , 5% ) , per il secondo in 704 / 800 casi ( 88% ) , per il terzo in 750 / 800 casi ( 93 , 7% ) , nellultima lettura in 800 / 8000 casi ( 100% ) in tutti i lettori . 
il ramo intermedio ( segmento 16 ) stato correttamente identicato in 42 / 50 casi ( 84% ) per il primo lettore , in 39 / 50 ( 78% ) per il secondo lettore , in 40 / 50 ( 80% ) casi per il terzo lettore . perviet del segmento i segmenti occlusi ( stenosi 100% ) sono stati correttamente identicati in 0 / 17 casi per ciascun lettore , sia allinizio che al termine della curva . 
i 17 segmenti sono in tutti i casi stati descritti da tutti i lettori come sub - occlusi ( 70 100% )  . 1288 radiol med ( 2013 ) 118 : 12811293 segments 10 , 14 and 15 . 
the intermediate branch ( segment 16 ) was correctly identied in 42 / 50 cases ( 84% ) by r1 , in 39 / 50 cases ( 78% ) by r2 and in 40 / 50 cases ( 80% ) by r3 . grado di stenosi segment patency the occluded segments ( stenosis 100% ) were correctly identied in 0 / 17 cases by each reader , both at baseline and at the end of the learning curve . 
all 17 occluded segments were reported as subocclusive ( 70100% ) by all readers . degree of stenosis all readers increased their diagnostic accuracy in the persegment analysis : the range was 7589% for r1 , 7382% for r2 and 8190% for r3 . 
figure 1ac reports the increase tutti i lettori hanno incrementato la loro accuratezza diagnostica , con un range per r1 da 75 a 89% , per r2 da 73 a 82% e per r3 da 81 a 90% nellanalisi per segmento . 
1a - o graci riassuntivi delle curve di performance dei tre lettori . radiol med ( 2013 ) 118 : 12811293 1289 in diagnostic accuracy per segment , per vessel and per patient . 
r2 demonstrated a mean condence level of 3 ( good ) in 272 / 800 segments ( 34% ) at initial reading and in 780 / 800 segments ( 97.5% ) at the last reading . 
r1 rated them poor in 112 / 800 segments ( 14% ) at initial reading , 97 / 800 ( 12.1% ) at the second reading and 74 / 800 ( 9.2% ) at the third and fourth readings . 
il secondo lettore ha dimostrato una condenza media pari a 3 ( buona ) in 272 / 800 segmenti ( 34% ) nella prima lettura , in 780 / 800 segmenti ( 97 , 5% ) per lultima lettura . 
il terzo lettore ha dimostrato una condenza media pari a 3 ( buona ) in 336 / 800 segmenti ( 42% ) nella prima lettura , in 762 / 800 segmenti ( 95% ) per lultima lettura . qualit dellimmagine lo standard di riferimento ( gs ) ha descritto i dataset come poveri in 49 / 800 segmenti ( 6 , 1% ) , mentre il primo lettore ( r1 ) ha descritto i dataset come poveri in 112 / 800 segmenti ( 14% ) per la prima lettura , 97 / 800 ( 12 , 1% ) per la seconda lettura , in 74 / 800 ( 9 , 2% ) per la terza e la quarta lettura . 
 il secondo lettore r2 ha descritto i dataset come poveri in 38 / 800 segmenti ( 4 , 7% ) per la prima lettura , 35 / 800 ( 5% ) per la seconda lettura , in 40 / 800 per la terza lettura , 37 / 800 ( 4 , 7% ) per lultima lettura . 
il terzo lettore r3 ha descritto i dataset come poveri in 76 / 800 segmenti ( 9 , 5% ) per la prima lettura , 11 / 800 ( 11 , 6% ) per la seconda lettura , in 40 / 800 ( 5% ) per la terza lettura , 74 / 800 ( 9 , 2% ) per lultima lettura . presenza di stent la presenza di stent stata identicata dal gs in 4 / 50 casi , dal primo lettore r1 in 4 / 50 casi , dal secondo lettore r2 in 0 / 50 casi , dal terzo lettore in 0 / 50 casi . stents were identied by the gs in 4 / 50 cases . 
there were no discrepancies in the identication of calcium burden per segment between the different readings . data - set evaluation times the gs evaluated the 50 cases in a mean time of 16.5 m evaluation times for r1 were 40 min on average at initial il carico di calcio stato identicato correttamente come assente in 339 / 800 segmenti ( 42 , 4% ) per il gs , in 272 / 800 segmenti ( 34% ) per il primo lettore r1 , in 293 / 800 segmenti ( 36 , 6% ) per il secondo lettore , in 288 / 800 segmenti ( 36% ) per il terzo lettore . 
tra le varie letture non vi sono state discrepanze nellidenticazione del carico di calcio per segmento . tempo di lettura del dataset considerando che il gs ha impiegato un tempo medio di 16 , 5 minuti per la valutazione dei 50 casi , il primo lettore per la prima lettura ha impiegato mediamente 40 minuti , per la seconda lettura 22 minuti , per la terza lettura 12 minuti . 
il secondo lettore per la prima lettura ha impiegato mediamente 26 minuti , per la seconda lettura 16 minuti , per 1290 radiol med ( 2013 ) 118 : 12811293 reading , 22 min at the second reading , and 12 min at the third reading . 
for r3 , they were 21 min at initial reading , 17 min at the second reading and 11 min at the third reading . discussion patient selection , scan performance and mdct - ca image reconstruction and interpretation all require various levels of experience . 
patient selection depends on specic cardiological expertise , with knowledge of mdct - ca integration with coronary angiography and stress testing ; scan performance requires expertise in drug administration in order to attain an adequate heart rate to perform the examination ; technical radiological expertise is also necessary to implement a correct acquisition protocol to ensure that the patient is exposed to a minimal radiation dose . 
data analysis requires knowledge of coronary anatomy as well as of the most common ct artefacts . mdct - ca has only recently been added to the diagnostic imaging studies available for coronary arteries in the clinical settings , having been previously only used in validation studies carried out in research settings . 
as a result , very few centres perform mdct - ca according to clinical criteria , and most of them are related to research centres or universities where specialty courses include specic training in cardiac imaging . 
the increasing availability of 64 - slice ct systems has led to mdct - ca also being offered in centres without cardiological expertise or where radiologists lack specic competency in cardiac ct . 
 in 2006 , the european and american cardiological and radiological associations jointly proposed guidelines specifying the minimum prociency levels for correct use of mdct - ca [ 1 , 7 ]  . 
although the guidelines refer to criteria of time , number of cases to be analysed and supervision by an expert cardiac radiologist , the literature contains only few reports describing the effectiveness of these guidelines in terms of diagnostic accuracy at the different levels of training . 
our results also indicated that each reader improved in diagnostic accuracy per patient from a minimum of 67% to a maximum of 87% at the end of the learning curve , a value still much lower than those reported in the literature ( 97100% )  . 
il terzo lettore per la prima lettura ha impiegato mediamente 21 minuti , per la seconda lettura 17 minuti , per la terza lettura 11 minuti . discussione larruolamento dei pazienti , lesecuzione tecnica , la ricostruzione e linterpretazione dellac - tcms richiedono esperienza a vari livelli . 
larruolamento dei pazienti richiede conoscenze cardiologiche speciche , con conoscenza dellintegrazione della metodica con la coronarograa e il test da sforzo ; lesecuzione dellesame richiede competenza nella somministrazione dei farmaci al ne di ottenere una frequenza cardiaca adeguata allacquisizione dellesame ; inoltre , richiede competenze tecniche radiologiche al ne di esporre il paziente alla minima dose radiogena mediante protocollo di acquisizione corretto . 
solo recentemente lac - tcms entrata a far parte delle metodiche imaging per lo studio delle arterie coronarie in ambito clinico , essendo precedentemente utilizzata solo in centri di ricerca ove stata validata . 
ne consegue che i centri che attualmente eseguono lac - tcms secondo criteri clinici sono molto limitati e per lo pi legati a centri di ricerca o universit ove i corsi di specializzazione prevedono una formazione specica anche in cardioradiologia . 
la disponibilit sempre maggiore di apparecchiature tc a 64 strati ha portato recentemente allesecuzione di esami ac - tcms anche in centri in cui la cardiologia non presente o in cui il radiologo non ha una competenza specica in cardio - tc . 
 dal 2006 , le societ europee e americane congiunte hanno proposto linee guida con livelli di training minimi necessari per un corretto utilizzo dellac - tcms [ 1 , 7 ]  . 
sebbene le linee guida facciano riferimento a criteri temporali , a numero di esami da analizzare e alla supervisione di un esperto in cardioradiologia , in letteratura esistono solo pochi lavori che descrivono lefcacia di tali linee guida in termini di accuratezza diagnostica nei vari livelli di training . 
in particolare , anche dai nostri risultati emerge come la sensibilit e la specicit siano molto basse alla prima lettura ( sensibilit 0 , 330 , 40 ; specicit 0 , 890 , 95 ) nellanalisi per segmento ma aumentino nellultima lettura ( sensibilit 0 , 870 , 96 ; specicit 0 , 99 )  . 
dai risultati emerge per ogni singolo lettore un incremento nella performance diagnostica che va da unaccuratezza nellanalisi per paziente minima del 67% a un valore massimo ottenuto al termine della curva dell87% , valore piuttosto lontano dai valori di accuratezza della metodica riproposti in letteratura che variano tra il 97 e il 100% . 
il valore predittivo negativo , punto cardine della metodica cardio - tc di esclusione di patologia coronarica radiol med ( 2013 ) 118 : 12811293 1291 parameter for excluding occlusive disease in cardiac ct , was varied between 56% and 78% at the end of the learning curve , values that are also much lower than reported by other authors ( 100% )  . 
 all readers , who started from different levels of experience with mdct - ca ( 01 year of experience with cardiac ct ) showed improvement in diagnostic performance , achieving very similar results at the end of the learning curve . 
when approaching a new diagnostic task , beginners lack knowledge and experience , intermediates have adequate knowledge but limited experience and experts have both knowledge and experience [ 14 ]  . 
readers at the intermediate level might also have an overcondent approach to the task , whereas those at initial and advanced stages may be more motivated to perform well . our results indicate that 6 months of extensive training in cardiac ct are not enough to achieve a sufcient level of accuracy for reliable management of patients undergoing mdct - ca . 
had 3 years experience with cardiac ct , and the expert ( gs ) reader in our study had 6 years ; it is therefore likely that > 1 year of experience is needed to attain levels of diagnostic performance close to those reported in the literature . 
in routine clinical practice , double reading of a cardiac ct scan is rarely possible , and diagnostic performance is likely to be slightly lower than 100% . it should be noted that in our study , readers remained blinded to patients clinical data and history until the end of the learning curve , so that their tendency to underestimate lesions was not corrected unless it involved the clinical cases reviewed during the intervals between reading sessions . 
 it could therefore be argued that one of the limitations of the training requirements proposed by the guidelines is the number of cases to be assessed in the interval between readings , so that readers can be made aware of the possible consequences of the overor underestimation of the degree of stenosis . 
firstly , the number of occlusiva , assume valori variabili al termine della curva dal 56 al 78% , anchessi molto discordanti da quanto riportato in letteratura , ove vengono descritti risultati di predittivit negativa vicini al 100% . tutti i lettori , partendo da unesperienza in ac - tcms molto differente variabile da zero a un anno di attivit in sezione di cardio - tc , hanno dimostrato un incremento nella performance diagnostica con risultati al termine della curva molto vicini tra loro . 
nellapproccio a un nuovo compito diagnostico , i principianti mancano di conoscenze ed esperienza , gli intermedi hanno adeguate conoscenze ma unesperienza limitata , i medici esperti hanno sia le conoscenze che lesperienza adeguate [ 14 ]  . 
 i lettori a uno stadio intermedio potrebbero inoltre avere un approccio al compito condizionato dalla sovrastima delle loro stesse capacit , mentre negli stadi iniziali e avanzati potrebbero essere pi motivati . dai risultati emerge come 6 mesi di training estensivo in cardio - tc non siano affatto sufcienti per ottenere livelli di accuratezza adeguati per unafdabile gestione dei pazienti sottoposti a cardio - tc . 
secondo la ten - year rule [ 18 ] , sono necessari circa 10 anni di anzianit per raggiungere unesperienza ottimale , indipendentemente dal campo di applicazione medica ; i lettori standard di riferimento nel lavoro di pugliese avevano unesperienza di 3 anni dedicata alla cardio - tc , nel nostro studio il lettore standard di riferimento aveva 6 anni di esperienza . 
 inoltre , i lavori pubblicati in cui la performance diagnostica si avvicina al 100% descrivono la lettura dei casi da due esperti , nella quale il dubbio diagnostico risolto in consenso . 
nella pratica clinica quotidiana non quasi mai possibile la doppia lettura di un esame cardio - tc ed verosimile che la performance diagnostica sia lievemente inferiore al 100% . va sottolineato , inoltre , il fatto che i lettori sono rimasti in cieco dei dati clinico - anamnestici dei pazienti no al termine della curva ; pertanto , la loro tendenza alla sottostima delle lesioni non stata corretta se non nei casi clinici osservati e discussi negli intervalli tra una lettura e la successiva . 
si potrebbe ipotizzare , pertanto , che uno dei limiti dei requisiti di training proposti dalle linee guida sia il numero di esami da affrontare nellintervallo interlettura , in modo da permettere ai lettori di venire a conoscenza prima delle potenziali conseguenze di una sovrao sottostima del grado di stenosi . 
innanzitutto , il numero 1292 radiol med ( 2013 ) 118 : 12811293 participants was small ( three readers ) , and all were trainee radiologists , whereas in clinical practice , cardiac ct examinations are also read by cardiologists . 
second , the inclusion of participants considered very similar levels of experience at baseline ( zero , 6 months and 1 year ) , so the results were only slightly different ; however , our main objective was to evaluate the improvement in the diagnostic performance of inexperienced physicians reading mdctca examinations . in contrast to pugliese et al.s study [ 12 ] , our analysis was carried out at the segment , main vessel and patient levels ; we believe per - patient analysis to be more representative of true diagnostic performance because the clinical implications of an error in a per - patient analysis are no doubt greater than in a per - segment analysis . 
 dei partecipanti era piccolo ( tre lettori ) e tutti appartenenti alla disciplina radiologica , mentre nella realt clinica sovente gli esami di cardio - tc sono valutati anche da cardiologi . 
inoltre , linclusione di partecipanti ha considerato intervalli di esperienza base molto vicini tra loro ( esperienza zero , sei mesi e un anno ) e quindi i risultati ottenuti sono solo leggermente differenti ; tuttavia , il nostro scopo principale era quello di valutare il miglioramento della performance diagnostica in ac - tcms dei medici ancora inesperti . a differenza di come valutato da pugliese et al . 
 [ 12 ] , la nostra analisi stata effettuata per segmento , vaso maggiore e paziente ; riteniamo che lanalisi per paziente sia la pi esplicativa della vera performance diagnostica , in quanto nella pratica clinica le implicazioni di un errore effettuato su un paziente piuttosto che su un segmento sono senzaltro maggiori . 
 conclusions conclusioni in conclusion , although all readers improved their diagnostic performance as they gained increasing experience with mdct - ca , a longer training period may be required to attain an adequate level of competence to be able to read mdct angiograms as independent practitioners . in conclusione , sebbene tutti i lettori abbiano migliorato la loro performance diagnostica aumentando la loro esperienza in ac - tcms , pu essere necessario un tempo pi lungo per raggiungere unesperienza adeguata in ac - tcms come professionista indipendente . conict of interest the authors declare that they have no conict of interest related to the publication of the article . 
the main hallmark of takotsubo cardiomyopathy ( tt - cmp ) is transient ischaemia , with completely reversible regional contractile dysfunction , which involves the mid - apical segments and shows no angiographic signs of coronary artery disease ( cad )  . 
seventeen patients with a clinical and angiographic diagnosis of tt - cmp underwent cardiovascular magnetic resonance ( cmr ) imaging in the acute phase and at follow - up after 4 months . 
a standard acquisition protocol including turbo spin echo ( tse ) t2 - weighted short - tau inversion - recovery ( t2 stir ) , steady - state free - precession cine ( ssfp cine ) and lateenhancement ( le ) imaging after gadolinium benzyloxypropionic tetraacetic acid ( gd - bopta ) administration was performed . 
in all patients , t2 stir images showed a diffuse homogeneous hyperintensity that extended to all mid - apical segments and perfectly matched the area of regional dysfunction , reflecting tissue oedema . 
la cardiomiopatia di takotsubo ( tt - cmp ) una sindrome caratterizzata da unischemia transitoria , con disfunzione contrattile completamente reversibile , che coinvolge i segmenti medio - apicali , con coronarie angiograficamente indenni . 
questo studio si propone di valutare , attraverso risonanza magnetica cardiaca ( cmr ) , i segni morfologici di infiammazione in pazienti con ttcmp , correlando i risultati con i dati laboratoristici . 
diciassette pazienti con diagnosi clinica e angiografica di tt - cmp sono stati sottoposti a cmr in fase acuta e dopo 4 mesi , con protocollo standard comprendente cine steady - state free - precession ( cinessfp ) , t2 - short tau inversion recovery ( t2 - stir ) e late enhancement ( le ) imaging . 
in tutti i pazienti , le sequenze t2 - stir hanno evidenziato una diffusa imbibizione edematosa dei segmenti medio - apicali a distribuzione non - coronarica e correlata con la sede della disfunzione contrattile ; in 5 pazienti sottoposti a emb , listologia ha confermato ledema interstiziale massivo associato al caratteristico quadro di necrosi a bande di contrazione . 
al controllo , tutti i pazienti hanno mostrato completa regressione delledema con significativo recupero funzionale del ventricolo sinistro ( frazione di eiezione da 48 , 7% a 59 , 8% )  . 
tt - cmp appears to be triggered by neurohormonal factors often resulting from strong emotional stress preceding the acute event and reported by the patient ( hence the name of broken heart syndrome ) [ 4 ]  . the diagnosis is thus based on a combination of coronary angiography ( which demonstrates the absence of epicardial coronary lesions and the typical ballooning appearance of the lv on ventriculography , shown in figure 2 ) , ecg and laboratory tests , as well as on reversibility of the changes [ 5 , 6 ]  . 
these diagnostic criteria , however , are inadequate for differentiating acute - phase tt - cmp from other possible diagnoses caused by infarction with normal coronaries , such as acute myocarditis or subendocardial necrosis due to microvascular disease [ 7 , 8 ]  . 
in this perspective , cardiovascular magnetic resonance ( cmr ) imaging has an emerging role in diagnosing tt - cmp owing to the possibility of combining functional data and tissue characterisation , thereby allowing detection of possible irreversible tissue injury and interstitial oedema [ 912 ]  . 
dal punto di vista eziopatogenetico , il quadro sembra scatenato da fattori neuro - ormonali spesso scatenati da forti stress psico - emotivi che prece dono lepisodio acuto e riferiti anamnesticamente dal paziente ( da cui il nome anche di broken heart syndrome ) [ 4 ]  . la diagnosi si basa quindi sulla combinazione di esame coronarografico ( che dimostra lassenza di lesioni a carico dei vasi coronarici epicardici e laspetto tipico del ventricolo sinistro durante ventricolo grafia , come mostrato in figura 2 ) , clinico - laboratoristico ed elettrocardiografico e sul concetto di reversibilit della alterazioni [ 5 , 6 ]  . 
sulla base di tali criteri diagnostici , tuttavia , non possibile differenziare in fase acuta la sindrome da altre possibili diagnosi differenziali da infarto a coronarie indenne quali la miocardite acuta o la necrosi subendocardica da malattia del microcircolo [ 7 , 8 ] ; in tal senso , lesame di risonanza magnetica cardiaca ( cmr ) trova impiego sempre maggiore nellinquadramento di tale condizione , per la possibilit di combinare i reperti funzionali con la capacit di caratterizzazione tissutale della metodica , che consente di identificare leventuale presenza di danno tissutale irreversibile e di edema interstiziale [ 912 ]  . 
2a - c a 55 - year - old patient presenting to the emergency department with chest pain , elevated serum troponin and c - reactive protein ( crp ) levels . 
 ventriculography ( a , b ) shows hypoakinesia of the middle segments and akinesia of the apical segments and apex , with typical left ventricular ballooning in the end - systolic phase ( b , arrowheads )  . 
2a - c paziente di 55 anni , giunta in pronto soccorso ( ps ) per dolore toracico , con rialzo dei marker sierici di troponina e proteina c - reattiva ( crp )  . 
patient histories in 8 / 17 ( 47% ) cases revealed the presence of trigger events preceding the acute episode , predominantly consisting of emotional stress of varying nature ( recent death or severe illness of a relative , stressful events at work , endoscopic procedures )  . 
 all patients underwent a cmr study in the acute phase ( on average within 2.4 days of admission ) and at follow - up 34 months after symptom onset ; five patients also underwent emb in the acute phase . 
 mr protocol cmr study was carried out with a new - generation system ( siemens magnetom avanto , erlangen , germany ) operating at 1.5 t with high - performing gradients ( rise time , 44 mt / m ; slew rate , 600 ms ) and using 16 - element phasedarray surface coils . 
in all patients , vector - cardiogram gating ( vcg ) was applied by placing three electrodes on the chest segni morfologici di infiammazione in pazienti con sospetta ttcmp , correlando il quadro rm con i dati clinico - laboratoristici e , ove disponibile , con i dati forniti dalla biopsia endomiocardica ( emb )  . materiali e metodi popolazione di studio nel periodo compreso tra gennaio 2008 e febbraio 2010 , 17 pazienti di sesso femminile ( et media 629 , 8 anni ; range 5472 anni ) , sono state sottoposte a esame di cmr , nel sospetto clinico di ttcmp . 
in tutte le pazienti era stato infatti riscontrato dolore toracico e / o dispnea , movimento troponinico con modificazioni elettrocardiografiche del tratto st e aspetto balloniforme dellapice ventricolare in assenza di lesioni coronariche epicardiche allesame angiografico selettivo effettuato allingresso . 
in tutti i casi , inoltre , allammissione era stato riscontrato un movimen to aspecifico degli indici di flogosi ( in particolare dei valori di proteina c reattiva )  . 
anam nesticamente stato possibile identificare eventi trigger prima dellepisodio acuto in 8 / 17 pazienti ( 47% ) con sistenti prevalentemente in stress emozionali di varia natura ( lutto recente o severa malattia di un familiare , eventi stressanti in ambito lavorativo , procedure endoscopiche )  . 
 tutte le pazienti sono quindi state sottoposte a esame di cmr in fase acuta ( media 2 , 4 giorni ) e nel follow - up 34 mesi dallinsorgenza della sintomatologia ; in 5 pazienti stata anche effettuata la biopsia endomiocardica ( emb ) in fase acuta . 
 radiol med ( 2013 ) 118 : 13091323 1313 wall at the level of the second intercostal space along the left lateral sternal line , at the level of the fourth intercostal space along the left lateral sternal line and at the level of the fifth intercostal space along the left hemiclavicular line so as to obtain an ecg trace providing good visualisation of the qrs complex . images were acquired in the standard cmr scan planes , in the short axis , vertical long axis ( two - chamber view ) and horizontal long axis ( four - chamber view ) using a combined protocol consisting of morphological t2 - weighted shorttau inversion recovery ( stir ) black - blood sequences [ t2 stir : time to repetition ( tr ) 2rr ; time to echo ( te ) 64 ; thickness 8 mm ; matrix 138256 ] in the short axis , vertical long axis and horizontal long axis to evaluate myocardial oedema . 
functional steady - state free - precession gradientecho sequences ( ssfp : tr 3.5 ms , te 2 ms , flip angle 500 , matrix 272272 , thickness 8 mm , gap 10 mm ) covered the entire lv to quantify ventricular volumes and evaluate cardiac motion . moreover , all patients were imaged with inversion - recovery late - enhancement sequences ( ir - le : tr 5 ms ; te 2.3 ms ; flip angle 150 ; thickness 8 mm ; matrix 128256 ; ti optimised to null the signal of the myocardium ) 1520 min after i.v. 
administration of contrast material [ gadolinium benzyloxy - propionic tetraacetic acid ( gd - bopta ) , multihance bracco ; 0.1 mmol / kg , dose 12 ml ; flow rate 3 ml / s ] to evaluate possible late enhancement ( le )  . 
contrast material was administered with a dual - head automatic injector ( medrad stellant dual ; medrad , palo alto pa , usa )  . image analysis after reconstruction of raw data sets , images were evaluated on a dedicated workstation ( leonardo vd10a siemens medical solutions , forchheim , germany ) during consensus reading by two radiologists experienced in cardiovascular imaging . 
specific software ( syngo argus , siemens ) was used , allowing ventricular volumes and myocardial mass to be determined by tracing the endocardial and epicardial contours in a semiautomatic manner . 
for the purposes of image analysis , the lv was divided into 17 segments based on the classification of the american heart association ( aha ) [ 13 ]  . for all patients , both qualitative and quantitative assessments were obtained . 
qualitative analysis permitted identification of the presence , site ( aha segments ) and extent of myocardial oedema ( t2 stir sequences ) and ir - le sequences , where present . 
then , the ssfp cine sequences were used to quantify ventricular volumes [ end - systolic volume ( esv ) ; end - diastolic volume ( edv ) ; ejection fraction ( ef ) ] , regional and global lv function , and lv mass by semiautomatically tracing the endocardial and epicardial contours on images acquired at end - systole and end - diastole . 
any le protocollo rm lindagine rm stata eseguita utilizzando un magnete di ultima generazione ( siemens magnetom avanto , erlangen , germania ) operante a 1 , 5 t con gradienti altamente performanti ( velocit di risalita dei gradienti : 44 mt / m ; slew - rate 600 v / ms ) e impiegando bobine di superficie ( tipo phased array ) a 16 canali . 
in tutte le pazienti stato utilizzato un gating cardiaco di tipo vector - cardiogram ( vcg ) posizionando 3 elettrodi sulla parete toracica a livello del secondo spazio intercostale sulla marginosternale di sinistra , sul quarto spazio intercostale sulla marginosternale di sinistra e sul quinto spazio intercostale sullemiclaveare di sinistra , in modo da ottenere un tracciato ecg in cui il complesso qrs fosse ben visualizzabile . le immagini sono state acquisite secondo piani di scansione standard di cardio - rm in asse corto , 2 camere ( o asse lungo verticale ) e 4 camere ( o asse lungo orizzontale ) , utilizzando un protocollo combinato che comprendeva sequenze morfologiche a sangue nero tipo short - tau inversion recovery t2 pesate [ stir t2w : tempo di ripetizione ( tr ) 2rr ; tempo di eco ( te ) 64 ; spessore 8 mm ; matrice 138256 ] in asse corto , asse lungo verticale e 4 camere per valutare i fenomeni di edema miocardico , sequenze funzionali gradient - echo steady - state free - precession ( ssfp : tr 3 , 5 ms , te 2 ms , fa 500 , matrice 272272 , spessore 8 mm , gap 10 mm ) coprendo lintero volume ventricolare sinistro per la quantificazione dei volumi ventricolari e la valutazione della cinesi cardiaca . in tutte le pazienti , inoltre , sono state effettuate sequenze inversion - recovery ( ir - le : tr 5 ms ; te 2 , 3 ms ; flip angle 150 ; spessore 8 mm ; matrice 128256 ; ti ottimizzato per abbattere il segnale miocardico ) 1520 minuti dopo somministrazione endovenosa di mezzo di contrasto ( mdc ) ( gd - bopta , multihance , bracco , italia ; 0 , 1 mmol / kg , dose somministrata 12 ml ; flusso 3 ml / s ) , per la valutazione di eventuali fenomeni di late - enhancement ( le )  . 
il mdc stato somministrato utilizzando un iniettore automatico a doppia testata ( medrad stellant dual ; medrad , palo alto pa , usa )  . analisi delle immagini dopo ricostruzione dei dati grezzi , le immagini sono state valutate in consenso da due esperti radiologi cardiovascolari , su una stazione di lavoro dedicata ( leonardo vd10a siemens medical solutions , forchheim , germania ) , utilizzando software dedicato ( syngo argus , siemens medical solutions ) che consente di effettuare una valutazione di volumi ventricolari e massa miocardica tracciando i bordi endocardici ed epicardici in modo semiautomatico . 
per lanalisi delle immagini , il miocardio ventricolare sinistro stato diviso in 17 segmenti in base alla classificazione aha [ 13 ]  . in tutti i pazienti stata effettuata una valutazione qualitativa e quantitativa . 
in the same segments , t2 short - tau inversion - recovery ( stir ) ( c ) sequences show a noncoronary distribution of high signal intensity related to myocardial oedema ( arrows )  . 
le sequenze cine ssfp ( a , b ) confermano lipo - acinesia dei segmenti medi e lacinesia dei segmenti apicali e dellapice ( punte di freccia ) , con apicalbalooning del ventricolo sinistro . 
nelle stesse sedi , le sequenze t2 stir ( c ) mostrano la presenza di unestesa area di iperintensit del segnale con distribuzione non coronarica , da riferire a edema miocardico ( frecce )  . 
 nelle sequenze t1 de - ir ( d ) non si documenta tuttavia la presenza di accumuli patologici di mdc . was quantified in grams by manually drawing a region of interest ( roi ) over the myocardial segments showing normal signal intensity ( si ) and applying a cutoff value of 5 standard deviations ( sd ) above the mean si of apparently normal heart to identify any segments with le [ 14 , 15 ]  . 
analysis of the t2 stir images obtained to assess myocardial oedema involved measuring the increase in si by placing an roi over the entire lv ; the value obtained was then related to the si recorded in skeletal muscle ( extensor spinae or longissimus dorsi , depending on muscle homogeneity ) to obtain a ratio expressed as t2 si ratio [ 16 ]  . 
successivamente , utilizzando le sequenze cine - ssfp sono stati quantificati i volumi ventricolari ( volume telesistolico , edv ; volume telediastolico , esv ; frazione di eiezione , fe ) , la funzione ventricolare sinistra regionale e globale e la massa ventricolare sinistra , tracciando in modo semiautomatico i bordi endocardici ed epicardici dalle immagini acquisite in fase telesistolica e telediastolica . 
leventuale le stato inoltre quantificato in grammi tracciando manualmente una regione di interesse ( roi ) nei segmenti miocardici che apparivano di normale intensit e utilizzando un valore soglia 5 deviazioni standard , superiore alla media dellintensit di segnale del miocardio apparentemente normale per identificare i segmenti con le [ 14 , 15 ]  . 
lanalisi delle immagini stir t2 pesate per la valutazione delledema miocardico prevedeva la misura dellincremento dellintensit del segnale attraverso il posizionamento di una roi nellintero miocardio ventricolare sinistro ; il valore ottenuto veniva quindi rapportato con il valore dellintensit del segnale riscontrato in un muscolo scheletrico ( estensore della colonna o lunghissimo del dorso , a seconda dellomogeneit del muscolo ) , ottenendo in tal modo un rapporto espresso come t2 ratio [ 16 ]  . 
4a - d a 57 - year - old patient presenting to the emergency department with chest pain and dyspnoea ( arising after an argument with colleagues at work ) , with elevated serum troponin - 1 and st elevation at electrocardiography ( ecg )  . 
cardiovascular magnetic resonance ( cmr ) was performed 18 h after admission : steady - state free - precession ( ssfp ) cine sequences ( a , b ) show segmental left ventricular wall - motion dysfunction , with dyskinesia and akinesia of the midapical segments and apex ( arrowheads )  . 
t2 short - tau inversion - recovery ( stir ) sequences ( c ) show a bright area in the same location , related to myocardial oedema ( arrowheads ) and pericardial effusion along the inferior wall of the left ventricle ( arrowheads )  . 
4a - d paziente di 57 anni giunta in pronto soccorso per dolore toracico e dispnea ( insorti a seguito di un litigio sul posto di lavoro ) , con aumento dei valori sierici di tni e sovraslivellamento del tratto st allesame elettrocardiografico . 
lesame di rm cardiaca veniva eseguito durante il ricovero ( 18 ore dopo laccesso in ps ) : le sequenze cine ssfp ( a , b ) mostrano alterazione della contrattilit segmentaria del ventricolo sinistro , con discinesia e acinesia dei segmenti medio - apicali e dellapice ( punte di freccia )  . 
nelle stesse sedi le sequenze stir t2 pesate ( c ) evidenziano unarea a elevata intensit di segnale , da riferire a edema miocardico ( punte di freccia ) e falda di versamento pericardico lungo la parete inferiore del ventricolo sinistro ( punte di freccia )  . 
nelle sequenze de - ir , eseguite dopo somministrazione di mdc ( d ) non si apprezzano aree di potenziamento nel contesto del miocardio ventricolare . pazienti veniva inoltre valutata la presenza di versamento pleurico e pericardico . 
le was detected on contrast - enhanced imaging in 2 / 17 patients , with a noncoronary distribution of enhancement ( patchy enhancement ) , predominantly seen at the lateral segments . 
lalterazione cinetica regionale ( ipocinesia , acinesia e discinesia ) si concentra a livello dei segmenti medi e soprattutto apicali e dellapice . biopsy findings emb was obtained in five patients ( but in neither of the two patients with le )  . 
results in the acute phase and follow - up are summarised in tables 2 and 3 and in figures 8 and 9 . discussion findings of this study , in five cases with histological correlation , confirm two fundamental aspects of tt - cmp . 
dopo mdc , stata rilevata la presenza di le in 2 / 17 pazienti , con pattern di potenziamento a distribuzione non coronarica ( enhancement a chiazze ) , prevalentemente localizzato nei segmenti laterali . 
il calcolo dei volumi ventricolari ha inoltre mostrato un netto incremento della frazione di eiezione ( fe da 47 , 28 , 4% a 64 , 36 , 2% ) e riduzione del volume tele diaradiol med ( 2013 ) 118 : 13091323 1317 stolico ( edv da 135 , 28 , 83 ml a 108 , 616 , 6 ml )  . 
i risultati in fase acuta e nel follow - up sono riassunti nelle tabelle 2 e 3 e nelle figure 8 e 9 . discussione il presente studio , correlato in cinque casi dai reperti istologici , conferma due aspetti fondamentali della tt - cmp . 
non sono stati riportati casi di coinvolgimento del ventricolo destro , diversamente da quanto descritto in studi con casistica pi ampia in cui una disfunzione ventricolare destra presente nel 30% dei casi , non sono stati inoltre riscontrati casi di ipo - acinesia esclusivamente a livello basale ( inverted takotsubo )  . 
questa maggiore uniformit dei pattern di ballooning nella nostra popolazione di studio potrebbe essere dovuta al pi esiguo numero di casi analizzati rispetto agli studi multicentrici precedentemente pubblicati . il secondo dato riguarda la costante presenza di edema tissutale in fase acuta nella popolazione di studio in esame , che si rivelata poi reversibile al follow - up . 
6 il preparato di colorazione con ematossilina - eosina evidenzia massivo edema interstiziale ( asterisco ) associato alla necrosi a bande di contrazione ( freccia ) , che caratterizza la patologia . 
in keeping with the literature , all patients in our study showed full functional recovery at follow - up , confirming the transient nature of the ventricular dysfunction seen in tt - cmp . 
there were no cases of rv involvement , in contrast to reports from larger studies that detected rv dysfunction in 30% of cases ; there were no cases of hypoakinesia affecting exclusively the basal segments ( inverted takotsubo )  . 
si osserva inoltre , nelle sequenze stir t2 pesate , completo riassorbimento dei fenomeni edemi geni intramiocardici . table 2 results of morphological and functional evaluation in the acute phase and at follow - up . 
in the acute phase , reduction in ejection fraction and an increase in end - diastolic volume was seen , with a statistically significant increase of the t2 si ratio , reflecting tissue oedema . 
at follow - up after 4 months , there was functional recovery of the left ventricle and complete resolution of the myocardial oedema ( significantly decreased mean t2 si ratio ) tabella 2 risultati della valutazione morfologica e funzionale in fase acuta e follow - up . 
in fase acuta sono stati osservati riduzione dei valori di frazione di eiezione e aumento del volume tele - diastolico , con incremento statisticamente significativo del t2 - ratio compatibile con la presenza di edema tissutale . 
determination of ventricular volumes shows increased ejection fraction in all patients at follow - up tabella 3 analisi per paziente delle modificazioni dei valori di frazione di eiezione in fase acuta e al follow - up . 
the pathophysiological substrate justifying the myocardial oedema in these patients has not been elucidated , even though the presence of inflammatory phenomena and transient ischaemia would appear to play a central role . 
moreover , in our series , myocardial segments exhibiting the most severe oedema corresponded to the armiocardico infatti una caratteristica fondamentale della tt - cmp , essendo generalmente presente nella maggior parte dei pazienti affetti da questa sindrome [ 17 , 18 ]  . 
il substrato patofisiologico che giustifichi la presenza di edema miocardico in questi pazienti non appare ancora ben definito ; tuttavia , la presenza di fenomeni infiammatori e di ischemia transitoria sembrerebbero comunque giocare un ruolo fondamentale . 
inoltre , le pazienti che presentavano una maggiore quantit di edema a livello globale avevano valori di frazione di eiezione pi bassi . radiol med ( 2013 ) 118 : 13091323 1319 fig . 
8a , b rappresentazione grafica per paziente delle modificazioni dei valori di frazione di eiezione ( ef ) ( a ) e di volume telediastolico ( edv ) ( b ) in fase acuta e al follow - up . acute phase follow - up fig . 
additionally , patients presenting with the greatest extent of overall oedema had lower ef values . these findings emphasise the importance of quantifying and mapping oedema in patients with tt - cmp , as these data reflect the extent of myocardial injury sustained during the acute phase and coincide with the areas of greater questi dati sottolineano limportanza della quantificazione e dellidentificazione dei fenomeni di edema nei pazienti con tt - cmp , poich questi riflettono lentit del danno che il miocardio subisce in fase acuta e coincidono con le zone maggiormente disfunzionanti a livello cinetico . 
altro dato fondamentale per un corretto inquadramento della tt - cmp , la distribuzione tipicamente non - coronarica 1320 radiol med ( 2013 ) 118 : 13091323 wall - motion dysfunction . 
another crucial feature for correct diagnosis of tt - cmp is the typically noncoronary distribution of tissue oedema , an element that can help differentiate the syndrome from , for example , aborted infarction , characterised by oedema without le but with segmental coronary distribution of tissue injury and positive coronary angiography [ 19 , 20 ]  . 
 the absence of le is another feature observed in the majority of our study population and which was found to be associated with global and regional wall - motion recovery in all patients . 
this result is also confirmed by other studies conducted on larger population samples [ 21 , 22 ]  . an absence of functional recovery at follow - up was observed only in the two patients , who showed le persistence at follow - up , which in these cases may have reflected tissue injury due to ischaemia or inflammation . 
this hypothesis is supported by a previous report that defined a subgroup of tt - cmp patients with positive le in the absence of functional recovery and histological findings of increased collagen 1 and fibronectin due to expansion of the extracellular matrix [ 23 ]  . 
therefore , persistence of tissue injury on follow - up cmr and lack of an emotional trigger preceding the acute event in two patients in our series strongly suggest acute myocarditis , even though we were unable to obtain histological confirmation of this diagnosis . 
nonetheless , it is thought that the pathological accumulation of gadolinium in these patients may reflect interstitial fibrosis or subendocardial necrosis , which are present in acute myocarditis or non - stemi infarction [ 24 ]  . in general , cmr may play a fundamental role in differentiating this clinical setting , which is definable as a takotsubo phenotype ( absence of coronary lesions , stemi - type changes and lv apical ballooning ) , from the other forms of acute ventricular dysfunction associated with healthy coronary arteries ( infarction with normal coronary arteries and acute myocarditis ) , where it may have a major impact on the clinical and therapeutic management of patients . tt - cmp has an incidence of 0.72.5% among patients presenting with suspected acute coronary syndrome ( acs ) [ 25 ]  . 
moreover , it is enough to consider the negative prognostic significance of acute myocarditis , which carries the risk of evolving into dilated cardiomyopathy and decompensated heart failure , with a need for immunosuppressive treatment in many cases [ 26 , 27 ]  . another interesting aspect of our study was the possibility of correlating cmr and emb data , which confirmed the delledema tissutale , elemento utile per differenziare la sindrome , ad esempio , dal cosiddetto infarto abortito , in cui presente edema senza le , ma con distribuzione segmentaria - coronarica del danno tissutale e reperti coronarografici positivi [ 19 , 20 ]  . 
 lassenza di le un altro dato emerso nella gran parte della nostra popolazione di studio ed risultato associato in tutti i casi a recupero cinetico globale e regionale a distanza . 
il dato confermato anche in altri lavori con pi ampia popolazione di studio [ 21 , 22 ]  . lassenza di recupero funzionale a distanza stata osservata unicamente nelle due pazienti con le positivo ; la persistenza del le nel follow - up in questi due casi potrebbe suggerire la possibilit di un danno tissutale dovuto a fenomeni di ischemia o infiammazione . 
questo troverebbe conferma in alcuni dati presenti in letteratura che definiscono un sottogruppo di pazienti con tt - cmp con le positivo in assenza di recupero funzionale e reperti istologici di aumento di collagene di tipo i e fibronectina per espansione della matrice extracellulare [ 23 ]  . 
nella nostra popolazione di studio , quindi , la persistenza del danno tissutale in rm a distanza e lassenza di un trigger psico - emotivo precedente il quadro acuto riscontrate in 2 pazienti , sono elementi fortemente suggestivi per miocardite acuta che , per , non stato possibile confermare dal punto di vista istologico . 
 ulteriori studi dovranno tuttavia essere condotti per correlare anche dal punto di vista istologico la presenza di le con le altre possibili diagnosi differenziali di malattia a coronarie sane , anche se lidea che laccumulo patologico di gadolinio in questi pazienti sia lespressione dei fenomeni di fibrosi interstiziale o di necrosi subendocardica che sono , ad esempio , presenti nelle miocarditi acute o nellinfarto tipo non - stemi [ 24 ]  . in generale , comunque , la cmr pu avere un ruolo fondamentale nella diagnostica differenziale tra questo setting clinico , definibile come fenotipo takotsubo ( assenza di lesioni coronarografiche , modificazioni tipo stemi e apical ballooning del ventricolo sinistro ) , e le altre forme di disfunzione ventricolare acuta a coronarie sane ( infarto a coronarie sane e miocardite acuta ) , con potenziale rilevante impatto sulla gestione clinica e terapeutica del paziente . la tt - cmp annovera , infatti , unincidenza dello 0 , 7 2 , 5% dei pazienti che si presentano in ospedale con sospetto di sindrome coronarica acuta [ 25 ]  . 
il riconoscimento della tt - cmp nellambito delle diagnosi differenziali , soprattutto in donne in post - menopausa che si presentano con sintomi da sindrome coronarica acuta ( sca ) , potrebbe dunque evitare trattamenti potenzialmente dannosi con agenti trombolitici . 
 basti inoltre pensare al significato prognostico sfavo revole di una miocardite acuta con rischio di evolutivit verso cardiomiopatia dilatativa e scompenso e necessit di trattare con farmaci immunosopressori in molti casi [ 26 , 27 ]  . altro elemento di interesse nel nostro studio riguarda la possibilit di correlazione dei dati rm con lemb , che ha confermato in tutte le 7 pazienti biopticate la presenza di radiol med ( 2013 ) 118 : 13091323 1321 presence of massive oedema in the absence of interstitial fibrosis in all five patients who underwent biopsy . 
 although little is still known regarding the mechanisms underlying the association between tt - cmp and myocardial injury , the pathophysiological explanation seems to be an insult due to catecholamine hypersecretion , which leads to microvascular dysfunction or coronary spasm , in the absence of obstructive disease . 
the activity of plasma mediators is heightened by the increased responsiveness of adrenergic cardiac and receptors , which are especially represented at the level of the middle and apical segments , where the main biostructural and functional changes take place . the evidence provided by the histological sections shows inflammation to be a peculiar aspect of acute ttcmp . 
this inflammation is characterised by an increase in intramyocardial water and extravasation of inflammatory cells , with cellular damage within the sarcomeres , due to disassembly of the actinmyosin bridges within contractile fibres and resulting in loss of contractile function . 
in our study , biopsy findings confirmed the presence of inflammation ( lymphocytes , leukocytes , macrophage infiltrates ) and abnormalities in the contraction bands , elements that , instead , are absent in ischaemic heart disease , which is typically characterised by coagulation necrosis . in conclusion , in patients with tt - cmp , cmr allows not only precise evaluation of segmental contractility but also , thanks to the t2 - weighted stir sequences , noninvasive detection of myocardial oedema , which is a reflection of tissue damage and inflammation and thus potentially a specific marker for this disease . 
 study limitations limitations of our study include the lack of systematic histological correlation in all patients and the acquisition of t2 stir sequences with phased - array coils alone , with the risk of overestimating tissue oedema as a result of hyperintense signal on the anterior aspect of the lv , which is closer to the surface coil . 
however , to minimise this risk , we used a quantification method based on the t2 si ratio , as suggested in the literature [ 28 ] , which involved normalising the myocardial signal with that of a skeletal muscle . 
as an alternative approach , abdel - aty suggested using body coils that , despite their lower signal - to - noise ratio , allow for better estimation of myocardial oedema [ 29 ]  . 
our cmr protocol did not provide for systemic use of the early enhancement technique , which appears to have provided interesting results in the setting of tt - cmp , reflecting myocardial hyperaemia and capillary leakage [ 22 ]  . sebbene il meccanismo sottinteso allassociazione tra tt - cmp e danno miocardico sia poco conosciuto , il meccanismo fisiopatologico sembra consistere in un insulto da iperincrezione catecolaminica , che determina una disfunzione del microcircolo o uno spasmo coronarico , in assenza di persistente ostruzione microvascolare . 
lattivit dei mediatori plasmatici viene potenziata dallaumentata responsivit dei recettori e - adrenergici cardiaci , particolarmente rappresentati a livello dei segmenti medio - apicali , che sono appunto quelli sede delle principali alterazioni bio - strutturali e funzionali . le evidenze fornite dai preparati istologici dimostrano come laspetto peculiare della tt - cmp in fase acuta sia lo stato infiammatorio locale , caratterizzato dallaumento del contenuto idrico intramiocardico e stravaso di cellule infiammatorie , con danno cellulare allinterno dei sarcomeri , per disgregazione dei ponti actina - miosina allinterno delle fibre contrattili del miocardio e conseguente perdita della funzione contrattile . 
nel nostro studio , i reperti bioptici hanno confermato la presenza di segni di infiammazione ( infiltrati di linfociti , leucociti e macrofagi ) e alterazione delle bande di contrazione , elementi invece assenti nella cardiopatia ischemica caratterizzata tipicamente da necrosi coagulativa . lesame rm nei pazienti con tt - cmp , in conclusione , oltre alla precisa valutazione della contrattilit segmentaria , consente , grazie allutilizzo delle sequenze stir t2 - pesate , di individuare in modo non invasivo ledema miocardico che , riflettendo il danno tissutale e lo stato infiammatorio , pu essere considerato un marker specifico di patologia . 
 limiti dello studio tra i limiti dello studio sono da menzionare lassenza di correlazione istologica sistematica in tutti i pazienti esaminati e lacquisizione di sequenze t2 stir con le sole bobine phased array , con rischio di sovrastima delledema tissutale dovuta al presenza di segnale iperintenso sulla parete anteriore del ventricolo sinistro , pi contigua alla bobina di superficie . 
tuttavia , per minimizzare tale pitfall stato utilizzato un approccio di quantificazione basato sul parametro del t2 ratio , come suggerito in letteratura [ 28 ] , normalizzando il segnale del miocardio con quello di un muscolo scheletrico per minimizzare questo problema . 
come approccio alternativo , abdel - aty suggerisce lutilizzo di bobine body che , seppur gravate da rapporto segnale - rumore ridotto , consentono una stima reale maggiore delledema miocardico [ 29 ]  . 
nel nostro protocollo rm non stato effettuato in modo sistematico la tecnica di early enhancement che , comunque , sembra aver dato risultati interessanti in pazienti con tt - cmp , riflettendo la presenza di iperemia e stravaso di sangue dai capillari miocardici [ 22 ]  . 1322 conclusions radiol med ( 2013 ) 118 : 13091323 conclusioni this study shows that tissue oedema on cmr is a highly sensitive marker for acute tt - cmp when combined with location in the midapical segments affected by regional dysfunction , relative sparing of the basal segments and almost complete reversal at follow - up . 
oedema , which was confirmed in all patients who underwent emb , is a nonspecific marker that is constantly present in the acute phase and can thus be used to noninvasively monitor disease severity . 
 il presente studio , condotto con cmr , evidenzia come ledema tissutale rappresenti un marker altamente sensibile di ttcm in fase acuta , con localizzazione nei segmenti medio - apicali interessati dalla disfunzione regionale , relativo risparmio della base e regressione pressoch completa nel follow - up . 
ledema , confermato anche in tutti i pazienti sottoposti a emb , rappresenta un marker aspecifico costantemente presente in fase acuta e pu essere utilizzato per monitorare la severit di malattia . 
 the rst issue was published in january 1914 and for a hundred years the journal has continuously represented the most important tool for the scientic and educational updating of italian radiologists . 
 after a century of history , at a time of great vitality of italian radiology la radiologia medica , while continuing in its role as the ofcial organ of sirm , captures the new and advanced needs of members and prepares for a new challenge . as recently reported [ 1 ] , it is my great pleasure to conrm that the rst 2014 issue of la radiologia medica , now a monthly journal , will be published only in the english language and online : sirm has decided to increase its scientic contribution to radiology through an ofcial englishlanguage journal . 
 at the same time , sirm has created a new italian - language journal , il giornale italiano di radiologia medica , which will be published bimonthly and distributed in paper format , to complement the online la radiologia medica in the task of providing professional updating and education to members . electronic publishing compared with print - only articles has many advantages : rapid turnover time from submission to publication , lower costs related to printing , ease of archiving and retrieval , instantaneous retrieval of references , and the possibility to publish larger documents with colour and movies economically [ 2 ]  . 
la radiologia medica has always published high - quality radiological research papers , maintaining its positioning as a multidisciplinary journal covering all clinical and technical aspects of diagnostic imaging , radiotherapy , medical physics and radiobiology . 
at least two special issues with guest editors will be considered each year in order to make the journal an effective tool for scientic and professional updates on elds of particular relevance . our in each table of contents will include high - quality original research and focused review articles ( generally commissioned ) issue . 
 la radiologia medica , as many other radiological journals , uses a workow solution called editorial manager ( em ) to manage all the peer review process : the em software contains a number of handy tools for streamlining the editorial and review workow , including a feature that automatically suggests appropriate reviewers on the basis of their eld of interest . 
the hard work of reviewing is performed by numerous referees including the members of the full scientic editorial board : the journal will be attractive to authors if the review turnaround time is short , and electronic publication is rapid . 
a peer - reviewed journal cannot function without reviewers : skilled manuscript reviewers from many countries outside of italy will be added to our tea of course , high - level peer review performance should be considered crucial to maintain high - quality standards and avoid publishing manuscripts of low quality . 
authorship credit should be based on : ( 1 ) substantial contributions to conception and design , or acquisition of data , or analysis and interpretation 1258 radiol med ( 2013 ) 118 : 12571258 of data ; ( 2 ) drafting the article or revising it critically for important intellectual content ; and ( 3 ) nal approval of the version to be published . 
measures of success include the international ranking of the journal , the productivity of scientists who publish in the journal , the frequency of article downloads , the number of manuscripts submitted to the journal , and the rate at which articles are accepted or rejected [ 6 ]  . 
the impact factor is most often used to measure the scientic quality of biomedical the 2 - year if of la radiologia medica is now 1.461 , as reported by the journal citation report 2012 published by the institute for scientic information ( isi )  . 
 based upon the 2 - year if , the journal is ranked 67 of 120 imaging we intend to continue to provide our readers with essential , up - to - date material ; our journal must enhance current and future radiology practice and serve as a constant reminder that the health of the patient comes rst . 
the hope is that manuscript submissions to la radiologia medica from outside of italy will continue to increase , facilitated by the online process and by the english - only publication . 
the treatment algorithm was neo - adjuvant chemotherapy ( ct ) administered for four cycles , followed by preoperative sc - rt administered 1 week after chemotherapy completion , delivering 20 gy in ve fractions over 1 week . 
lapproccio terapeutico prevedeva un trattamento sistemico neoadiuvante ( 4 cicli ) seguito da radioterapia ipofrazionata short - course per una dose totale di 20 gy in 5 sedute consecutive erogate in una settimana . 
this treatment resulted in favourable lc , os , low rates of toxicity and satisfying qol . keywords rectal cancer preoperative short - course radiation therapy combined chemo - radiation therapy allesame istologico denitivo , una stabilit di malattia stata ottenuta in 24 pazienti ( 36% ) , una riduzione di malattia in 34 pazienti ( 50 , 7% ) e una progressione in solo 9 casi ( 13 , 3% )  . 
nel corso del follow - up sono state evidenziate due recidive loco - regionali ( entrambe in campo di trattamento radioterapico ) con un controllo locale a 5 anni del 97% . 
il trattamento radioterapico ipofrazionato neoadiuvante associato a chemioterapia nei tumori del retto localmente avanzati risulta essere ben tollerato , con ottimi risultati in termini di controllo locale , sopravvivenza globale e qualit di vita dei pazienti . parole chiave tumore del retto radioterapia pre - operatoria ipofrazionata radio - chemioterapia introduction introduzione rectal cancer is the fourth most frequent tumour worldwide , representing about one - third of large bowel malignancies and the third cause of death among men and women [ 1 ]  . 
 management of locally advanced resectable rectal cancer requires a multidisciplinary approach , because , although surgery still plays a fundamental role , the addition of radiation therapy and chemotherapy in a preoperative or adjuvant setting results in signicantly improved local control ( lc ) and overall survival ( os ) compared to surgery alone [ 24 ]  . numerous trials have shown that preoperative radiation therapy ( rt ) can decrease the risk of local relapse up to 5070% . 
 ideally , preoperative rt could also reduce treatment - related toxicity in comparison to adjuvant rt , as reported by several randomised trials that demonstrated lower toxicity and better compliance of rt when administered before rather than after surgery [ 5 , 6 ]  . the most frequent regimens in the preoperative setting of patients with resectable rectal cancer are conventionally fractionated concomitant chemo - radiation therapy ( 4550 gy in 1.82 gy per fraction ) with delayed surgery or shortil tumore del retto la quarta neoplasia per frequenza , rappresentando un terzo circa delle neoplasie del grosso intestino e la terza causa di morte negli uomini e nelle donne . 
il trattamento di queste neoplasie richiede un approccio multidisciplinare : nonostante infatti la chirurgia giochi un ruolo fondamentale , laggiunta di radioterapia e chemioterapia allatto chirurgico migliora signicativamente il controllo locale e la sopravvivenza globale [ 24 ]  . 
 molti studi hanno dimostrato che la radioterapia neoadiuvante pu ridurre il rischio di recidiva locale di malat tia del 5070% , mentre lapproccio adiuvante riduce questo rischio di solo il 3040% . 
alcuni importanti studi randomizzati hanno dimostrato inoltre una riduzione della tossicit correlata al trattamento con la radioterapia neoadiuvante , quando confrontato allapproccio post - operatorio [ 5 , 6 ]  . i pi frequenti approcci neoadiuvanti seguono essenzialmente due schemi : il primo prevede radio - chemioterapia concomitante , in cui la radioterapia eseguita con frazionamento convenzionale a un dose totale di 4550 gy erogata in 2528 frazioni , seguita a distanza di 48 settimane da intervento chirurgico ; il secondo prevede radioterapia iporadiol med ( 2013 ) 118 : 13971411 1399 course irradiation ( 25 gy in ve fractions ) with immediate surgery [ 511 ] , with similar results in terms of long - term survival , local control and late morbidity [ 6 , 912 ]  . the radiation oncology unit conducted a prospective observational trial of neo - adjuvant chemotherapy and shortcourse radiation therapy , followed by immediate surgery for resectable rectal cancer . 
questi due approcci hanno dimostrato risultati sovrapponibili in termini di sopravvivenza , controllo locale e tossicit tardiva [ 6 , 912 ]  . presso la sc di radioterapia oncologica dellazienda ospedaliera di reggio emilia abbiamo condotto uno studio prospettico osservazionale di chemioterapia e radioterapia ipofrazionata neoadiuvante , seguita da chirurgia immediata . 
 questo protocollo differisce dagli altri studi pubblicati in letteratura fondamentalmente per due aspetti : la radioterapia neoadiuvante ipofrazionata short - course combinata con la terapia sistemica e la dose totale di radioterapia modicata rispetto allo standard ( 25 gy in 5 sedute ) , al ne di ridurre potenzialmente la tossicit correlata al trattamento . materials and methods sixty - seven patients were treated with a neo - adjuvant chemotherapy / short - course radiation scheme at the oncological radiotherapy division of the reggio emilia hospital in italy . materiali e metodi study design this is a report of a common practice - derived , protocol driven , prospective treatment schedule of a preoperative shortcourse radiation treatment with the introduction of neoadjuvant chemotherapy . 
the protocol had been approved by the local ethics committee . patient selection eligibility criteria were : histologically proven diagnosis of primary rectal cancer , maximum 10 cm above the dentate line ( upper limit ) , clinical stage t3 or t4 , n0 or n + according to the uicc ( international union against cancer ) classication system , resectable rectal cancer , no evidence of sphincter involvement , no evidence of metastatic disease , no medical contraindications to radiation therapy , chemotherapy or surgery after multidisciplinary evaluation , ecog ( eastern cooperative oncology group ) performance status 2 , age > 18 years and < 80 years , no prior pelvic radiation therapy and written informed consent . exclusion criteria were : previous or concurrent malignancies , locally advanced inoperable disease , presence of metastatic disease or recurrent rectal cancer , concurrent severe medical conditions , stenotic tumour , medical or psychiatric conditions that could interfere with the patients informed consent . sono stati arruolati nel protocollo di studio 67 pazienti affetti da neoplasia del retto localmente avanzata trattati presso la radioterapia oncologia dellospedale di reggio emilia . disegno di studio questo studio un report di un protocollo interno di radioterapia ipofrazionata short - course a intento neoadiuvante associato a terapia sistemica nei tumori del retto . 
il protocollo di trattamento stato approvato dal comitato etico locale . selezione dei pazienti i criteri di eleggibilit del protocollo erano i seguenti : diagnosi istologicamente confermata di neoplasia del retto , sita a una distanza massima di 10 cm dalla linea dentata , in stadio clinico localmente avanzato ( t3 - t4 , n0 - n1 secondo la classicazione uicc international union against cancer ) , operabile , senza interessamento dello sntere e senza evidenza di diffusione sistemica . 
tutti i pazienti dovevano rmare il consenso informato preparato ad hoc . criteri di esclusione : precedente diagnosi di neoplasie maligne in altre sedi , malattia rettale inoperabile , presenza 1400 pretreatment stage evaluation pretreatment staging of the patients required digital rectal examination , laboratory studies , colonoscopy and computed tomography ( ct ) of the pelvis - abdomen - chest and endorectal ultrasound . valutazione pre - trattamento radiol med ( 2013 ) 118 : 13971411 di diffusione sistemica di malattia , gravi comorbilit , tumori stenosanti il lume rettale , altre condizioni mediche o clinico - psichiatriche che avrebbero potuto interferire con il consenso informato dei pazienti . preoperative therapy preoperative therapy was planned as follows : neo - adjuvant chemotherapy according to the de gramont scheme until 2003 and subsequently folfox 6 scheme ( oxaliplatin 100 mg / m2 and folinic acid 400 mg / m2 on day 1 followed by a 5 - fu bolus 400 mg / m2 and a 46 - hour infusion of 3000 mg / m2 every 2 weeks ) ; subsequent short - course rt consisting of 20 gy delivered in ve fractions , over 1 week , prescribed at the isocenter of the plan according to the international commission on radiation units and measurements ( icru ) report . 
the planning target volume ( ptv ) was dened as the ctv with a margin of 2 corgans at risk routinely considered in these patients were the bladder , femoral heads and bowels ( large and small bowel excluding ptv )  . three - dimensional rt was performed in all patients , according to the institutional practice , with each patient in the prone position with full bladder in order to displace the small bowel anteriorly and superiorly . la valutazione pre - trattamento dei pazienti comprendeva lesplorazione rettale digitoguidata , gli esami laboratoristici , la colonscopia , la tomograa assiale computerizzata del torace - addome - pelvi e leco - endoscopia . terapia neoadiuvante lapproccio neoadiuvante era cos pianicato : chemioterapia neoadiuvante secondo schema de gramont no 2003 ; successivamente folfox 6 ; successiva radioterapia ipofrazionata short - course ( dose totale 20 gy in 5 sedute giornaliere )  . 
la vescica , le teste femorali e lintestino venivano considerati organi a rischio . tutti i pazienti venivano sottoposti a radioterapia 3d conformazionale , in accordo con la nostra pratica clinica , in posizione prona e riempimento vescicale in modo da dislocare le anse intestinali anteriormente e superiormente al campo di irradiazione . surgery and pathological evaluation chirurgia according to the protocol , surgery was performed within seven days after rt completion ; although total mesorectal excision ( tme ) was the preferred surgical technique , it was not mandatory . 
the decision to perform a low anterior resection ( ar ) vs an abdomino - perineal resection ( apr ) depended on the distance of the lesion ( measured before preoperative chemo - radiation ) from the anal verge . 
 la valutazione isto - patologica seguiva le procedure standard , includendo la classicazione uicc e tnm , il numero di linfonodi reperiti ed il numero di linfonodi patologici , cos come lo stato dei margini . adjuvant chemotherapy follow - up chemioterapia adiuvante adjuvant chemotherapy consisting of six cycles of folfox was recommended after surgery for 6 months for patients with pathological stage t4 or n + disease . il trattamento sistemico adiuvante veniva indicato nei pazienti in stadio patologico t4 o n + e consisteva in 6 cicli di folfox ( de gramont prima del 2003 )  . radiol med ( 2013 ) 118 : 13971411 1401 follow - up follow - up all patients were followed - up at 6 - month intervals for 3 years and then once yearly . 
colonoscopy was performed every 6 months for the rst 2 years after surgery . outcome measures and denition of study end - points tutti i pazienti , dopo il trattamento combinato , venivano seguiti a intervalli semestrali per i primi 3 anni e successivamente annualmente . 
the secondary outcome measures were overall survival ( os ) , disease - free survival ( dfs ) , acute and late toxicity , and quality of life . early skin , small / large bowel and bladder toxicity was recorded according to the radiation therapy oncology group ( rtog ) common toxicity criteria . 
toxicity was dened as late if it occurred more than 3 months after radiation therapy , and was recorded according to the rtog scale . the assessment of complications was detailed and included intraoperative complications , general postoperative complications , specic postoperative complications ( bleeding requiring intervention , anastomotic leakage , ileus , abdominal and pelvic abscesses , peritonitis , stula , colostomy complications )  . 
the remaining six items are intended to be mono - item scales describing relevant canceroriented symptoms ( dyspnoea , insomnia , appetite , constipation , diarrhoea , nancial difculties )  . 
it is composed of four functional scales ( body image , sexual functioning , sexual enjoyment , and future perspective ) and various symptom scales ( urinary problems , chemotherapy side effects , gastrointestinal symptoms , sexual problems , defecation problems and weight loss )  . 
 gli endpoint secondari erano rappresentati dalla sopravvivenza globale , dalla sopravvivenza libera da malattia , dalla tossicit acuta e tardiva e dalla qualit di vita dei pazienti . la tossicit acuta e tardiva cutanea , intestinale e urinaria veniva registrata utilizzando le scale di tossicit dellrtog ( radiation therapy oncology group )  . 
la tossicit era denita tardiva se compariva pi di 3 mesi dopo la terapia radiante ed era registrata secondo la scala rtog . tutte le complicazioni intrae peri - operatorie sono state registrate , cos come le complicanze post - operatorie . 
un alto valore del punteggio delle diverse scale rappresenta un buono stato di salute , mentre un alto valore nel punteggio delle scale dei sintomi rappresenta un cattivo stato di salute . 
 questo strumento composto da 4 scale funzionali ( immagine corporea , funzionalit e soddisfazione sessuale , aspettative future ) e varie scale di sintomi ( problemi urinari , effetti collaterali della chemioterapia , sintomi gastroenterici , disturbi della sfera sessuale , alterazione dellalvo e perdita di peso )  . la scala fiql composta da 29 domande che costituiscono 4 scale diverse ; stile di vita ( 10 domande ) , comportamento ( 9 domande ) , depressione e percezione di se stesso ( 7 domande ) e imbarazzo ( 3 domande )  . 1402 radiol med ( 2013 ) 118 : 13971411 items form four scales : lifestyle ( 10 items ) , coping / behavior ( 9 items ) , depression / self - perception ( 7 items ) , and embarrassment ( 3 items )  . iief was a self - administered questionnaire assessing erectile function ( ef ) , orgasmic function ( of ) , sexual desire ( sd ) , intercourse satisfaction ( is ) and overall satisfaction ( os )  . statistical analysis all survival analyses were calculated according to the kaplan - meier method . 
the main patients and tumour characteristics are summarised in table 1 . all patients underwent chemo - radiation therapy ( the rst 28 with de gramont chemotherapy schema and the subsequent 39 patients with folfox ) and subsequent surgery without any major protocol violation . 
grade i and ii gastrointestinal ( diarrhoea ) acute toxicity was shown in one and six patients , respectively . all patients underwent surgery performed within seven days after rt completion according to our protocol . 
no pathological complete response was detected . complete local resection of the rectal cancer was achieved in 100% of cases , with mean distance of the tumour from the surgical margins of 44 mm ( range 7120 mm ) ( table 2 )  . 
 in ultimo , liief un questionario auto - somministrato che esplora diverse aree della sfera sessuale ( funzionalit erettile , funzionalit orgasmica , soddisfazione intercorrente e generale )  . analisi statistica tutte le analisi di sopravvivenza sono state calcolate utilizzando il metodo kaplan - meier . 
le variabili analizzate sono : sesso , et , stadio clinico e patologico , tipo di chirurgia , presenza di stenosi alla diagnosi e la distanza tra la malattia e sntere anale . 
le caratteristiche cliniche e patologiche dei pazienti sono riassunte in tabella 1 . tutti i pazienti sono stati sottoposti a trattamento combinato radio - chemioterapico ( i primi 28 pazienti con schema de gramont e i successivi 39 con folfox 6 ) e successiva chirurgia . 
una tossicit acuta genitourinaria stata riportata di grado 1 in due pazienti e di grado 2 da 4 pazienti , mentre tossicit acuta gastroenterica di grado 1 e 2 si manifestata , in forma di diarrea , in sette pazienti . tutti i pazienti sono stati sottoposti a intervento chirurgico entro sette giorni dalla ne della radioterapia . 
lanalisi isto - patologica del pezzo operatorio ha dimostrato che il 28 , 4% dei pazienti era in stadio i , il 35 , 7% in stadio ii e il 35 , 9% in stadio iii . 
una netta riduzione della malattia si evidenziata in 34 pazienti ( 50 , 7% ) , una stabilit in 24 pazienti ( 36% ) e una progressione di malattia in 9 casi ( 13 , 3% )  . 
la resezione della neoplasia stata completa in tutti i pazienti , con una distanza media del tumore dai margini chirurgici di 44 mm ( range 7120 mm ) ( tabella 2 )  . non stata osservata mortalit peri - operatoria . 
re - operation due to postoperative complications was required in only one patient for anastomotic stenosis 15 months after surgery . adjuvant chemotherapy was administered in 21 patients following the protocol design . 
 at the last follow - up a total of two locoregional recurrences , both within the rt volume , were observed , resulting in a 5 - year lc of 97% . 
 the rst patient , with presacral recurrence , was treated with multi - agent chemotherapy and was alive at last follow - up . a total of 11 systemic relapses were observed resulting in a 5 - year actuarial dfs rate of 84% , with mean time to systemic progression of 24 months . 
twenty - two patients died during the follow - up because of rectal cancer progression ( n = 8 ) , intercurrent disease ( n = 9 ) and unknown causes ( n = 5 )  . the 5 - year os rate was 67% . 
no death because of late toxicity was observed . at the time the qol questionnaires were sent out , 18 patients had died and two were still alive with local recurrences . 
gastrointestinal symptoms including nausea / vomiting , constipation and / or appetite loss were reported to be very rare , while diarrhoea was frequently reported in the plicazioni post - operatorie precoci di grado lieve - moderato sono state riportate nel 24% dei casi . 
complicazioni tardive sono state riportate invece in 5 pazienti ( 7% ) , ma solo un paziente ha richiesto un successivo intervento chirurgico per stenosi dellanastomosi 15 mesi dopo il primo intervento chirurgico . il trattamento sistemico adiuvante stato eseguito in soli 21 pazienti . il follow - up mediano dei pazienti viventi di 114 mesi con un range di 40178 mesi . 
il primo paziente che ha evidenziato recidiva di malattia , ha manifestato dopo circa 14 mesi dallintervento chirurgico una recidiva in regione pre - sacrale , e sottoposto a chemioterapia di i linea risulta ancora vivo allultimo follow - up . 
un secondo paziente invece ha sviluppato una ripresa linfonodale di malattia circa 48 mesi dopo il trattamento ed deceduto dopo 18 mesi per progressione sistemica di malattia . allultimo follow - up sono state riportate 11 recidive sistemiche con una sopravvivenza libera da malattia dell84% e un tempo medio alla progressione sistemica di 24 mesi . 
 solo 48 pazienti , di cui 39 operati conservativamente e 12 con amputazione addomino - perineale , hanno compilato i questionari relativi alla qualit di vita , con un tempo medio trascorso dalla ne della radioterapia e la compilazione dei questionari di 84 mesi ( range 48156 )  . 
i pazienti sottoposti a chirurgia conservativa hanno riportato risultati migliori in termini di qualit di vita globale ( 75 vs 60 ) , cos come gli aspetti pi prettamente funzionali . 
sintomi gastroenterici ( nausea , vomito , costipazione , inappetenza ) sono risultati essere eventi rari in entrambi i gruppi di pazienti , mentre la diarrea stata riportata pi frequentemente nei pazienti sottoposti a chirurgia conservativa . 
 treatment of locally advanced resectable rectal cancer has slowly changed over the last few years , with increased localregional tumour control during the past 1015 years , mainly due to the introduction of total mesorectal excision ( tme )  . 
 unfortunately , local relapse after this surgical procedure alone for locally advanced resectable rectal cancer still ranges between 15% and 21% in randomised trials [ 15 , 16 ]  . 
it is differenza tra i due gruppi di pazienti in termini di qualit di vita esplorata con gli specici questionari risultata statisticamente signicativa ( p < 0 , 001 )  . il questionario specico per lincontinenza fecale ( fecal incontinence quality of life scale fiql ) stato somministrato solo ai pazienti sottoposti a chirurgia con preservazione dello sntere anale . 
 in ultimo , il tasso di disfunzione erettile risultata maggiore nei pazienti sottoposti ad amputazione addominoperineale rispetto a quelli trattati con chirurgia conservati ( 47% vs 75% )  . discussione questo studio prospettico osservazionale riporta i risultati di un approccio neoadiuvante combinato chemioterapico e radioterapico ( schema ipofrazionato short - course ) seguito da chirurgia immediata nelle neoplasie localmente avanzate del retto . il trattamento di tali neoplasie ha subito notevoli cambiamenti negli ultimi anni , con un netto incremento del controllo loco - regionale evidenziato negli ultimi 1015 anni , principalmente dovuto allintroduzione della tme . 
risulta chiaro , quindi , che le neoplasie localmente avanzate del retto necessitano di un approccio multimodale , con un trattamento radioterapico 1406 radiol med ( 2013 ) 118 : 13971411 clear , therefore , that patients with locally advanced resectable rectal cancer need a combined treatment , with radiation therapy associated with surgical procedure in a preoperative or postoperative setting . 
the positive impact of preoperative rt in terms of local control and overall survival was demonstrated by seven european phase iii trials [ 6 , 1520 ] and by a metanalysis [ 21 ]  . when rt is considered an option in a setting of preoperative rectal cancer treatment , two major approaches exist : either a short course approach or long term radiation therapy , the latter sometimes combined with chemotherapy [ 17 , 18 ] ; today the question which preoperative treatment is best is still open . 
data supporting short - course preoperative rt were shown in the swedish rectal cancer trial and in the dutch colorectal cancer group trial ( ckvo 9504 ) , both showing lower rates of local recurrence after preoperative radiotherapy compared with surgery alone ( 11% vs 27% and 6% vs 12% , respectively )  . 
the swedish trial showed also a signicant improvement of 5 - year survival rates with preoperative short - course rt . although no trial has yet provided the nal answer , several studies have highlighted some of the advantages and disadvantages of long - term preoperative ct - rt and short course rt . 
 [ 19 , 22 ] showed no difference in terms of sphincter preservation rate and no major clinically relevant difference between short - course preoperative rt and long - course concomitant radio - chemotherapy followed by delayed surgery . 
 the only difference showed in this trial , as in several other studies , was in the rate of tumour downsizing , which was found to be higher with long - course chemo - radiation [ 6 ]  . 
 the recent review [ 23 ] of major published studies of shortcourse preoperative radiation and the more conventional approach of long - course neo - adjuvant chemo - radiation showed that although long - course preoperative chemo - radiation is associated with higher rates of reversible acute toxicity , it appears to be more a signicant and higher rate of late gastrointestinal toxicity observed in short - course preoperative radiation studies . a recent metanalysis [ 24 ] compared preoperative shortcourse radiotherapy with neo - adjuvant conventional chemoradiotherapy . 
no differences between chemo - radiotherapy and short - course rt were found in terms of survival , local recurrence , mortality , resectability , and rate of sphincter preservation . 
this may be related to the interval between radiotherapy and surgery that is too short in preoperative short - course rt protocols , preventing the regression detectable after a longer interval time [ 25 ]  . 
in fact , when delaying surgery to 68 weeks after shortcourse rt , the pathologic complete response and r0 resection rate were similar to those observed after preoperative associato alla chirurgia sia in setting neoadiuvante che post - operatorio . 
alcuni studi hanno evidenziato un vantaggio dellapproccio neoadiuvante rispetto alla radioterapia post - operatoria [ 6 , 13 ] soprattutto in termini di controllo locale e sopravvivenza globale , come dimostrato da sette studi di fase iii europei [ 6 , 1520 ] e da una recente metanalisi [ 21 ]  . quando parliamo di radioterapia neoadiuvante , si aprono fondamentalmente due scenari : il primo consiste in un trattamento radio - chemioterapico concomitante [ 17 , 18 ] in cui la radioterapia viene erogata con frazionamento convenzionale a una dose totale di 45 - 50 gy ; il secondo invece in una radioterapia esclusiva con schema ipofrazionato . 
la sola differenza evidenziata in questo e in altri studi , la percentuale di downsizing del tumore , che risulta nettamente maggiore nei pazienti sottoposti a radio - chemioterapia concomitante long - course [ 6 ]  . 
 una recente revisione [ 23 ] evidenzia che nonostante lapproccio concomitante sia associato a un tasso maggiore di tossicit acuta , sembra che la radioterapia ipofrazionata sia associata a un rischio maggiore di tossicit tardiva . 
 una metanalisi [ 24 ] pubblicata recentemente ha confrontato i due approcci neoadiuvanti e non ha evidenziato differenze in termini di controllo locale di malattia , sopravvivenza globale , mortalit , tasso di resecabilit e tasso di preservazione snteriale . 
di contro , questa metanalisi ha confermato il pi alto tasso di downsizing nei pazienti sottoposti a radio - chemioterapia long - course rispetto alla sola radioterapia short - course . 
questo dato potrebbe essere attribuito allintervallo temporale intercorrente tra la radioterapia e la chirurgia che risulta molto breve nei protocolli di radioterapia short - course , tanto da non rendere evidente la regressione tumorale evidenziabile con un pi lungo intervallo temporale [ 25 ]  . 
infatti , quando la chirurgia viene posticipata a 68 settimane dal termine della radioterapia short - course , il tasso di risposte patologiche complete e di resezione chirurgica completa sembra essere sovrapponibile a quelle osservate dopo trattamento radio - chemioterapico concomitante long - course , come dimostrato recentemente da radu et al . 
alla luce di questi dati , resta il dilemma , sottolineato dalleditoriale di pahlmanns [ 27 ] , di come interpretare leffetto di downsizing in vivo se la chirurgia pianicata corrisponde a quella eseguita . 
 [ 28 ] , in una recente revisione della letteratura , concludono che la scelta tra tipo di frazionamento ottimale di radioterapia , il timing della chirurgia e luso radiol med ( 2013 ) 118 : 13971411 1407 chemo - radiotherapy , as shown by radu et al . 
however , the dilemma is , as underlined by pahlmanns editorial [ 27 ] , how to interpret the downsizing effect in vivo , if the planned surgery corresponds to the performed one . 
 [ 28 ] in a recent review conrm that the optimal fractionation of rt , timing of surgery , and the best use of concomitant ct remain controversial . building on the success of chemotherapy in colorectal cancer , a potentially complementary approach to primary rt involves the use of chemotherapy and surgery to avoid rt . 
 [ 29 ] analysed 26 patients with t3 or t4 and n0 - 2 nonmetastatic resectable rectal cancer , treated with neo - adjuvant chemotherapy ( two cycles of irinotecan , 5 - fu and lv ) showing a 5 - year relapse - free and overall survival rates of 74% and 84% , respectively . 
 [ 30 ] used preoperative uorouracil , leucovorin , and oxaliplatin plus bevacizumab with no rt in carefully selected patients , with a surprising 23% pcr rate achieved with the chemotherapy regimen and excellent local control ( again with relatively short follow - up in selected group of patients )  . 
the new us alliance cooperative group ( previously cancer and leukemia group b , american college of surgeons oncology group , and north central cancer treatment group ) plans to study this approach further ( without use of bevacizumab ) in a multicentre randomised trial . 
the recent review [ 31 ] concluded that there is now enough preliminary evidence to support the view that in less locally advanced patients selected by initial mri , the role of neo - adjuvant chemotherapy alone , without radiation , but the utility of this approach should be explored compared with scprt or crt in selected patients with rectal cancer where the impact of radiotherapy on dfs and os is marginal . 
 in this scenario we undertook a prospective observational study to determine the feasibility and the impact on local control and quality of life of the combination of shortcourse preoperative rt and neo - adjuvant chemotherapy in patients affected by locally advanced resectable rectal cancer . 
the addition of chemotherapy to the hypofractionated radiation treatment , suggested by the hypothesis that induction chemotherapy would reduce gross tumour burden and improve oxygenation and hence sensitise to rt , has led us to reduce the total dose of radiotherapy by 20% compared to the standard scheme proposed by the swedish study ( 20 gy in ve consecutive fractions vs 25 gy in ve fractions ) with a biologically effective radiation therapy dose ( bed ) of 28 gy , despite the fact that the colorectal cancer collaborative group had recommended a bed > 30 gy on the basis of a metanalysis . 
 we hypothesised that the moderate reduction of bed della chemioterapia concomitante alla radioterapia rimangono , ancora oggi , controversi . sulla scorta del successo ottenuto dalla terapia sistemica nelle neoplasie del colon , alcuni studi hanno valutato un approccio neoadiuvante esclusivamente chemioterapico nel trattamento delle neoplasie localmente avanzate del retto . 
 [ 29 ] , ad esempio , hanno analizza to 26 pazienti affetti da neoplasia del retto in stadio t3 or t4 , n02 , m0 sottoposti a chemioterapia neoadiuvante ( 2 cicli di irinotecan , 5 - fu and lv ) e hanno riportato un tasso di sopravvivenza globale e libera da malattia a 5 an ni dell84% e 74% rispettivamente . 
 [ 30 ] ha evidenziato un tasso di risposte patologiche complete dopo sola chemioterapia neoadiuvante ( uorouracil , leucovorin , oxaliplatin e bevacizumab ) , senza radioterapia , del 23% . 
il nuovo us alliance cooperative group ( in origine cancer and leukemia group b , american college of surgeons oncology group , and north central cancer treatment group ) ha pianicato un studio multicentrico randomizzato che investighi questo approccio terapeutico ( senza bevacizumab )  . 
una recente revisione della letteratura [ 31 ] ha concluso che vi unevidenza molto preliminare che i pazienti affetti da neoplasia del retto localmente avanzata , la cui malattia venga stadiata con risonanza magnetica , possano beneciare di un trattamento neoadiuvante di sola chemioterapia omettendo il tempo radioterapico , bench siano necessari studi futuri di confronto tra i vari approcci terapeutici in pazienti altamente selezionati in cui limpatto della radioterapia sul controllo di malattia possa essere giudicato marginale . in questo scenario , abbiamo intrapreso uno studio prospettico osservazionale che si poneva lobiettivo di valutare la fattibilit e i risultati in termini di controllo di malattia , tossicit e qualit di vita , di un approccio neoadiuvante di chemioterapia seguita da radioterapia ipofrazionata e chirurgia immediata in pazienti affetti da neoplasia localmente avanzata del retto . 
laggiunta della chemioterapia a un trattamento radioterapico ipofrazionato , con lipotesi che la chemioterapia di induzione riduca il carico tumorale e aumenti lossigenazione del tumore aumentandone quindi la radiosensibilit , ha comportato una riduzione della dose totale di radioterapia del 20% rispetto alla dose standard utilizzata nello studio svedese , con una diminuzione della dose biologica equivalente ( bed ) da > 30 gy a 28 gy . 
per , tali interazioni generalmente sono note nei trattamenti radio - chemioterapici concomitanti piuttosto che sequenziali , anche se possibile 1408 radiol med ( 2013 ) 118 : 13971411 would be compensated by the antitumour activity of chemotherapy , without increasing treatment - related toxicity . 
it is possible that the additive effects of chemotherapy followed by radiation may compensate for the lower dose of radiation used in this study . to our knowledge , our study is the rst one that analysed the combination of neo - adjuvant chemotherapy and shortcourse rt in a preoperative setting in patients affected by locally advanced resectable rectal cancer . according to the protocol , only patients with ct3 / t4 or n + disease were eligible . 
 [ 32 ] showed that not only radio - chemotherapy but also short - term radiotherapy can lead to a signicant reduction in tumour size as early as 1.3 days after the end of treatment . in terms of results , the local recurrence rate in this trial was lower than in other studies , although tme was not performed in all patients . 
this may be related to the fact that it was a single - centre study with standardised quality - controlled surgery and a high rate of optimally performed surgical procedures , also documented by the nding of no case of r + disease . 
 this study did not investigate the role of the preoperative short course ct - rt in terms of sphincter preservation , because the decision to perform ar vs apr depended on the distance of the lesion from the anal verge , as evaluated before preoperative chemo - radiation . 
 [ 33 ] found patients with postoperative complication rates of 27% in the preoperative short - course radiotherapy group , compared with 21% in the neo - adjuvant radio - chemotherapy group . one of the main potential problems of hypo - fractionated radiotherapy is late toxicity , especially in terms of risk of incontinence and sexual dysfunction [ 3438 ]  . 
the relative low rate of long term complications , observed in our study group , may be due to the relatively low total dose of radiotherapy ( 20 gy in ve fractions compared with standard 25 gy in ve fractions ) and to the small volume of treatment che siano presenti anche in regimi di trattamenti sequenziali , come il nostro studio , e in grado quindi di compensare una riduzione moderata della dose di radioterapia . 
il nostro studio appare essere lunico presente in letteratura che abbia associato un trattamento neoadiuvante radioterapico short - course a una terapia sistemica nei tumori del retto in stadio ct3 / t4 e / o n +  . 
 [ 32 ] mostrarono che non solo la radio chemioterapia long - course ma anche la radioterapia shortcourse pu comportare una riduzione della massa tu morale . analizzando i risultati del nostro studio , il tasso di recidiva locale sembra essere pi basso rispetto a quanto riportato in letteratura , anche a fronte di una tme non sempre eseguita . 
questo studio non ha valutato limpatto della radioterapia pre - operatoria short - course sulla preservazione snteriale , in quanto il tipo di intervento chirurgico veniva deciso sulla base della distanza della malattia iniziale dallo sntere anale , come valutato agli esami di stadiazione pre - operatoria . 
nel nostro studio , anche se il 20% dei pazienti si presentava con malattia del retto basso , il tasso di preservazione snteriale risultato molto alto , in quanto pianicato e ottenuto in tutti i pazienti con neoplasia localizzata almeno a 5 cm dalla rima anale . 
 [ 33 ] hanno riportato un tasso di complicanze post - operatorie del 27% nel gruppo di pazienti sottoposti a radioterapia short - course rispetto al 21% nei pazienti trattati con chemio - radio concomitante long - course . uno dei maggiori potenziali problemi dellipofrazionamento la tossicit tardiva , soprattutto in termini di rischio di incontinenza e disfunzione sessuale [ 3438 ]  . 
 [ 33 ] ha evidenziato un tasso globale di tossicit del 28 , 3% e una percentuale di tossicit tardiva denita severa del 10 , 1% dopo un follow - up mediano di 48 mesi . 
 gli ottimi risultati ottenuti dal nostro approccio in termini di tossicit tardiva potrebbero essere giusticati dalla pi bassa dose totale di radioterapia . alcuni importanti limiti di questo studio necessitano di approfondimento . 
in prima istanza , questo uno sturadiol med ( 2013 ) 118 : 13971411 1409 only involving the rectum and the perirectal nodes . the limitations of this trial , however , should be acknowledged . 
the rst point is that our study is a prospective observational study , born by a common practice - derived prospective treatment schedule of a hypofractionated neo - adjuvant radiation treatment with the introduction of the systemic therapy according to the de gramont scheme before and folffox 6 scheme subsequently . 
the principles of total mesorectal excision ( tme ) were not mandatory ( even though it was performed in many patients ) and there was no histopathological examination of the circumferential resection margin ( pcrm ) , the most important predictor for local recurrence / prognosis after preoperative rt or chemo - radiation therapy . 
 on the other hand , two novel aspects of this study are the combination of chemotherapy with short course preoperative radiation , and the extensive use of qol questionnaires with long follow - up . 
the strength of this study was the homogeneity of the cohort of patients treated with the same chemotherapeutic agents , the same rt technique in terms of doses and volumes and with a surgical approach performed in the same centre with well established quality control . 
this study was a pilot trial that could serve as the basis for a larger , possibly multicentre , prospective study to determine the difference in terms of disease control and quality of life between long - course and short - course preoperative rt in combination with chemotherapy . dio prospettico osservazionale , nato da un protocollo interno di pratica clinica , in cui il trattamento standard di radioterapia neoadiuvante short - course stato modicato dallaggiunta della chemioterapia neoadiuvante e dalla riduzione della dose totale . 
inoltre , diversi regimi chemioterapici si sono alternati nel corso dello studio ( dal 2003 stato aggiunto loxaliplatino ) , lutilizzo della tecnica chirurgica di tme non era mandatoria e , come tale , non eseguita in tutti i pazienti e , in ultimo , non vi una valutazione isto - patologica del margine di resezione circonferenziale ( a oggi riconosciuto come uno dei maggiori fattori predittivi di recidiva locale )  . 
 a fronte di queste limitazioni , il nostro studio ha due nuovi importanti aspetti a suo favore : la proposta di nuovo approccio radio - chemioterapico neoadiuvante e lutilizzo di questionari sulla qualit di vita analizzati a un lungo follow - up . 
indubbiamente un punto di forza lomogeneit del campione e del tipo di trattamento , chemioterapico , radioterapico , cos come chirurgico . questo studio pilota potrebbe essere utile per disegnare futuri studi prospettici randomizzati multicentrici di confronto tra un approccio neoadiuvante di radio - chemioterapia concomitante long - course e radioterapia short - course , in termini di controllo di malattia e qualit di vita . conclusioni conclusions in our study neo - adjuvant chemotherapy and short - course radiation treatment followed by immediate surgery generated relatively high local control rates . 
 acknowledgements the authors are greateful to doctor luciano armaroli , former director of radiation oncology unit at arci spedale santa maria nuova , reggio emilia , until 2008 , who has been the author and promoter of this study . nel nostro studio la chemioterapia neoadiuvante e la radioterapia pre - operatoria short - course , seguite da chirurgia immediata , hanno dimostrato un alto tasso di controllo locale di malattia . sono necessari futuri studi multicentrici per identicare il corretto approccio neoadiuvante atto a ottenere i migliori risultati in termini di controllo di malattia e tossicit tardiva . ringraziamenti gli autori ringraziano il dott . 
luciano armaroli , direttore della struttura complessa di radioterapia oncologica no al 2008 , ideatore e promotore di questo studio . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
 incidence and anatomical location of lesions le denunce per la diagnostica dellapparato muscoloscheletrico : frequenza e sedi anatomiche coinvolte adriano fileni1 gaia fileni2 paoletta mirk3 giulia magnavita4 marzia nicoli5 nicola magnavita5 1istituto nazionale malattie infettive l . 
tel. : + 39 - 347 - 3300367 , fax : + 39 - 06 - 61909399 , e - mail : nicolamagnavita@gmail.com received : 6 march 2012 / accepted : 4 april 2012 / published online : 25 june 2013 springer - verlag 2013 abstract purpose . 
during the period considered , a total of 416 claims for alleged diagnostic errors relating to the musculoskeletal system were led against radiologists ; of these , 389 ( 93.5% ) concerned failure to report fractures , and 15 ( 3.6% ) failure to diagnose a tumour . 
incorrect interpretation of bone pathology is among the most common causes of litigation against radiologists ; alone , it accounts for 36.4% of all malpractice claims led during the observation period . 
lerrata interpretazione della patologia ossea tra le pi frequenti cause di contenzioso verso i radiologi ; da sola essa rappresenta il 36 , 4% di tutte le denunce per presunto errore diagnostico pervenute nel periodo di osservazione . 
la consapevolezza del rischio dovrebbe indurre alla massima prudenza e diligenza . parole chiave malpratica radiologia scheletrica ossa e articolazioni fratture cancro denunce radiologi stress responsabilit diagnosi introduction introduzione medico - legal litigation against radiologists appears to be constantly rising [ 1 , 2 ] as a result of the growing number il contenzioso medico - legale contro i radiologi appare in continuo aumento [ 1 , 2 ] , sia per il crescente numero di esaradiol med ( 2013 ) 118 : 13881396 1389 of procedures performed and reported , which increases the chances of error , and because the retention of radiological images allows critical reviews even at a much later date , when the clinical evolution leads greater attention being paid a posteriori to ndings which had initially not been recognised as pathological . the risk of an italian radiologist being sued for alleged malpractice is currently estimated to be in the order of 44 per thousand , which corresponds to a likelihood greater than one of being sued during ones working life [ 3 ]  . 
 physical and psychological effects have also been described , which make up the so - called malpractice stress syndrome [ 8 , 9 ]  . missed fractures are the most frequent cause of malpractice claims against emergency department physicians [ 1012 ] and the most common cause of litigation against radiologists for failure of diagnosis [ 13 ]  . 
the last of these categories also includes all of those cases in which the radiologist did not specify the motivation of the claim , deciding to do so at a later date . claims were also classied according to the organ or body system affected by the alleged diagnostic error . 
in this study we focused our attention on the musculoskeletal system . mi eseguiti e refertati , che aumenta la probabilit di errore , sia perch la conservazione degli esami radiologici consente una rivalutazione critica anche a notevole distanza di tempo dallaccertamento diagnostico e non raro che levoluzione clinica consenta di prestare maggiore attenzione a posteriori a immagini che in un primo momento non erano state riconosciute come patologiche . il rischio di ricevere una denuncia per presunta malpractice fra radiologi italiani attualmente stimato nellordine del 44 per mille , il che corrisponde a una probabilit maggiore di uno di essere citato nel corso della propria vita professionale [ 3 ]  . 
sono descritte anche possibili conseguenze sul piano sico e psicologico , che si inquadrano nel cosiddetto stress da malpractice [ 8 , 9 ]  . le fratture non diagnosticate rappresentano la causa pi frequente di denuncia contro i medici nei servizi di emergenza e urgenza [ 1012 ] e rappresentano la pi frequente causa di citazione per omessa diagnosi contro i radiologi [ 13 ]  . 
we were unable to identify the technique used ( conventional radiology , computed tomography or magnetic resonance imaging ) or obtain additional details about the individual cases . the data were analysed with descriptive statistics , by using the statistical package for the social sciences ( spss / pc 15.0 , ibm , new york )  . 
however , the proportion of claims pertaining to the musculoskeletal system relative to the total number of claims led each year remained almost constant ( table 2 )  . a more detailed analysis of the causes of claims regarding skeletal pathology revealed that 390 cases related to fractures and 26 cases to primary or secondary skeletal neoplasms . 
the presumed diagnostic error was chiey of omission ( 400 cases , 96.2% ) , but there were also a few cases of radiol med ( 2013 ) 118 : 13881396 dellorgano o apparato corporeo sede del presunto errore diagnostico . 
in questo lavoro abbiamo preso in considerazione lapparato muscolo - scheletrico . altre informazioni delle quali stato possibile tenere conto riguardano la provenienza della denuncia ( struttura sanitaria pubblica o privata ) e limporto della richiesta di risarcimento , nei casi in cui questa era specicata . 
non stato possibile risalire al tipo di tecnica usata ( radiologia tradizionale , tc o rm ) n avere particolari sui singoli casi . i dati sono stati analizzati mediante statistiche descrittive , utilizzando lo statistical package for social sciences ( spss / pc 15.0 , ibm , new york )  . 
tuttavia , la percentuale delle denunce relative allapparato muscolo - scheletrico rispetto al totale delle denunce pervenute in ciascun anno quasi costante ( tabella 2 )  . analizzando pi in dettaglio lorigine delle 416 denunce riguardanti la patologia scheletrica , si osserva che esse sono riferite in 390 casi a fratture e in 26 casi a neopla sie primitive o secondarie dello scheletro . 
il presunto erro re diagnostico prevalentemente di tipo omissivo ( 400 casi , 96 , 2% ) , ma non mancano i falsi positivi ( 16 casi , 3 , 8% ) , anche questi riguardanti quasi esclusivamente le fratture . nella tabella 3 specicata la sede anatomica delle lesioni ossee causa di denuncia . 
limitando lanalisi alle 360 denunce per le quali la sede anatomica era specicata nella richiesta di assistenza allassicurazione , si evidenzia come esse riguardino segmenti scheletrici diversi , con prevalenza per lo scheletro superiore ( 179 casi , 49 , 7% ) rispetto a quello inferiore ( 136 denunce , 37 , 8% ) e al rachide ( 45 , 12 , 5% )  . 
vi unelevata frequenza di fratture ai polsi e , in particolare , allo scafoide ( 19 casi ) , alle ossa delle mani , braccia , gomiti , spalle e clavicole . 
le denunce per lo scheletro inferiore vedono al primo posto le fratture ai piedi , con prevalenza del calcagno ( 18 casi ) , seguite da femori , gambe e caviglie , bacino . 
2 numero delle denunce riferite allapparato muscolo - scheletrico pervenute nel corso del periodo di osservazione . false positive diagnosis ( 16 cases , 3.8% ) , most of which also relating to fractures . 
in particular , there was a high incidence of fractures of the wrist , especially of the scaphoid ( n = 19 ) , and of the bones of the hands , arms , elbows , shoulders and clavicles . 
claims regarding the lower skeleton included fractures of the foot , with a predominance of the calcaneus ( n = 18 ) , followed by the femur , leg and ankle , and pelvis . 
le denunce per erronea descrizione di lesioni non riscontrate a un successivo intervento chirurgico ( falsi positivi ) hanno riguardato in oltre met dei casi ( 9 su 16 ) articolazioni , cartilagini , menischi , tendini . le denunce riguardanti le lesioni dellapparato scheletrico sono presentate mediamente dopo 1 , 6 anni dallevento stesso . 
ricordiamo che nellintera coorte esaminata , tra i rimanenti 1003 casi , ve ne sono stati 403 mortali ( 40% ) [ 3 ]  . claims for skeletal system lesions tend to be led on average 1.6 years after the alleged error . 
in detail , 20% of skeletal system claims are led during the same year of occurrence of the harmful event , 62% within one year , and approximately 80% within two years ( table 4 )  . as for the type of facility ( public or private ) in which the harmful events occurred , most claims referred to events occurring in public facilities ( 313 / 407 cases with specied setting , 76.9% ) , and only 94 ( 23.1% ) in private facilities . death is seldom the cause of claims for compensation in litigations regarding the musculoskeletal system : 12 deaths ( 2.9% ) as against 403 ( 40% ) out of a total of 1003 claims for the entire cohort [ 3 ]  . the amount of compensation claimed for failure to detect a fracture amounted to 100 , 000 euro on average , and is therefore substantially less than requested for other types of radiological error , which may be over 1 , 000 , 000 euro [ 3 ]  . discussion our study shows that litigations arising out of musculoskeletal investigations are the most frequent cause of malpractice claims against radiologists . 
however , even though this statement holds true for a reasonably long period of time ( 14 years ) , the length of the prescriptive period in italy , and the growing tendency to sue radiologists for failure to detect cancer , which only becomes clinically manifest years after the radiological procedure , make it likely that claims due to si riferisce ad altri tipi di sinistri radiologici , per i quali la richiesta pu in alcuni casi superare il milione di euro [ 3 ]  . discussione il nostro studio evidenzia come le controversie che originano da esami dellapparato muscolo - scheletrico siano la pi frequente causa delle denunce contro i radiologi . 
tale affermazione risulta vera in un periodo di tempo ragionevolmente lungo ( 14 anni ) , anche se la lunghezza dei tempi di prescrizione consentiti dal nostro ordinamento e la crescente tendenza a denunciare i radiologi per omessa identicazione di lesioni neoplastiche , che sono clinicamente evidenti solo a distanza dallesecuzione dellesame radiologico , rendono probabile che le denunce originate dalle neoplasie della mammella , del torace e delladdome siano ancora pi rilevanti di quelle che si riferiscono al sistema scheletrico , come da noi stimato in precedenti lavori [ 2 , 3 ]  . 
gli esami di radiologia convenzionale sono tuttora ritenuti indispensabili nello studio della patologia traumatica e nel nostro paese sembra che il ricorso ai servizi di pronto soccorso sia molto rilevante e in continuo aumento . 
the italian ministry of health estimated a total of 22.5 million accesses to the emergency departments of public and private accredited facilities in 2004 [ 14 ] , but ofcial documents also incorporate data from the italian society of emergency medicine which estimated 50 million access for the same period [ 15 ]  . 
 despite the lack of reliable gures , it is easy to agree that a large number of emergency department accesses require radiological investigations , and that many of these regard the skeletal systeinvestigations made in emergency situations are often carried out in suboptimal condition , with unscheduled workloads and short examination and reporting times . 
it is also worth noting that , even in the case of minor lesions , such as the majority of skeletal lesions , the compensation demanded is higher than the annual income of any radiologist working in a public or private facility , and that on average each radiologist can expect one malpractice claim every 20 years of working life [ 2 ]  . 
the nancial commitment devenzionati [ 14 ] , ma accolgono in documenti ufciali an che le stime della societ italiana di medicina di emergenza / urgenza che si attestano nello stesso periodo sui 50 milioni di accessi lanno [ 15 ]  . 
pur in mancanza di un dato certo , facile convenire che gran parte degli accessi in pronto soccorso richiede lesecuzione di accertamenti radiograci e che molti di questi si riferiscono al sistema scheletrico . 
 appena il caso di ricordare che , anche per le lesioni meno gravi quali , mediamente , quelle a carico dellapparato scheletrico , gli importi richiesti sono superiori al reddito annuale di un radiologo dipendente , sia nella sanit pubblica che in quella privata , e che leventodenuncia sia atteso statisticamente una volta circa ogni 20 anni di carriera [ 2 ]  . 
limpegno economico richiesto a ciascun radiologo per assicurarsi contro il rischio quindi molto rilevante , soprattutto se si tiene conto del fatto che le denunce possono essere presentate a notevole distanza di tempo dallevento lesivo ed perci necessario assicurarsi per un tempo molto lungo e idealmente oltre la ne della vita professionale . lanalisi della distribuzione delle sedi anatomiche che hanno dato origine alle denunce indica che tutte le parti radiol med ( 2013 ) 118 : 13881396 1395 manded of each radiologist to maintain liability insurance is quite heavy , especially is we consider that claims can be led even years after the presumed harmful event , such that the insurance must be maintained for a very long period of time and ideally beyond the end of ones working life . the analysis of the distribution of the anatomical locations giving rise to the claims indicates that while any site may be involved , there is a greater frequency of claims originating from lesions affecting the upper skeleton , in particular hands and wrists . 
the scaphoid bone is associated with the highest number of claims , which attests to the difculty in diagnosing scaphoid fractures . in our series , there was a small number of claims due to missed sternal or costal fractures , which other studies reported to be the most frequent sites of missed diagnosis [ 16 ]  . 
the most likely explanation is that the study of major head trauma in the emergency department and outpatients clinic is usually done directly with computed tomography , which is able to depict even minimal bone abnormalities . 
as a result , the possibility of fractures being missed in these locations tends to be very small . by contrast , the failure to diagnose spinal fractures , and in particular fractures of the cervical spine , should raise concern if we consider how much a missed diagnosis of fracture at this site can signify in terms of injury and compensation . 
the high number of claims highlights the difculties and limitations of conventional radiology in the cervical spine , above all in polytrauma patients , and suggests in the presence of even minimal radiological evidence or technically limited radiological investigation prompt use of computed tomography . 
 it is enough to consider that even just moving a patient with an undiagnosed odontoid fracture may lead to extremely serious neurological damage with quadriplegia or death due to bulbar compression . 
 similar interpretation difculties are encountered in femur fractures when the fracture , in particular of the femoral neck , is impacted or without fragment displacement . later years of observation of our cohort revealed the emergence of claims due to the false positive diagnosis of possono essere coinvolte , ma con maggiore frequenza le denunce originano da lesioni del distretto superiore , in particolare mani e polsi . 
lo scafoide losso con maggio ri segnalazioni e ci testimonia della sua criticit diagnostica . nella nostra casistica si osserva un basso numero di denunce per mancata segnalazione di fratture a sterno e coste che viceversa , sulla base di studi precedenti [ 16 ] , risultano essere le sedi nelle quali pi frequente il misconosci mento radiologico . 
in questo caso la spiegazione pi verosimile che lo studio dei traumi cranici maggiori in pronto soccorso ( ps ) e dipertimento di emergenza e accettazione ( dea ) generalmente effettuato direttamente con la tc , che in grado di evidenziare anche minime alterazioni ossee . 
levenienza di fratture non evidenziate in queste sedi dunque modesta . al contrario , la mancata diagnosi di fratture del rachide , specie cervicale , deve essere fonte di preoccupazione se si considera quanto una mancata diagnosi di frattura in tale sede possa rappresentare in termini di danno e risarcimento . 
soprattutto le 22 denunce relative al rachide cervicale , di cui 11 riferibili a lesioni non evidenziate a carico del dente dellepistrofeo , individuano unarea estremamente critica per la radiologia tradizionale . 
lalto numero di denunce in questa sede evidenzia la difcolt e i limiti dello studio radiologico convenzionale del rachide cervicale , specie nei pazienti politraumatizzati , e deve consigliare in presenza di segni radiologici anche minimi o in caso di indagine radiologica tecnicamente limitata di ricorrere senza indugi allesame tc . 
basti pensare che la movimentazione di un paziente , al quale non stata evidenziata una frattura al dente dellepistrofeo , pu comportare un danno neurologico gravissimo con tetraparesi o morte da compressione dei centri bulbari . 
 negli ultimi anni di osservazione nella nostra casistica emerge il fenomeno delle denunce per errata diagnosi di patologie legamentose o meniscali , che hanno determinato lesecuzione di un intervento chirurgico risultato poi inuti1396 radiol med ( 2013 ) 118 : 13881396 ligament or meniscal pathology leading to unnecessary surgical procedures . 
i casi di false positivit nella diagnostica per immagini sono allorigine di una quota minore , ma signicativa , di denunce contro i radiologi anche nelle casistiche britanniche [ 4 ] o americane [ 6 , 13 ] e si teme che il ricorso a tecniche di assistenza alla diagnosi , come la computed - aided diagnosis ( cad ) [ 17 ] o un orientamento verso la medicina difensiva [ 18 ] , possano aumentare la frequenza di questa categoria di errori . conclusions conclusioni in conclusion , radiologists should be aware that skeletal radiology has the highest frequency of malpractice claims against radiologists . 
patients with atypical chest pain and suspected obstructive cad were directed to one of two diagnostic pathways : the traditional protocol ( examination , stress test , ca ) and the current protocol ( examination , stress test , mdct - ca , and ca , if necessary )  . 
mdct - ca had an accuracy of 66% , a sensitivity and specicity of 21% and 87% , respectively , and a positive ( ppv ) and negative ( npv ) predictive value of 40% and 70% , respectively . 
comparison between conventional ca ( cca ) and mdct - ca showed a sensitivity and specicity of 92% and 89% , respectively , a ppv and npv of 89% , and an accuracy of 92% . 
sono stati considerati due percorsi diagnostici per pazienti con dolore toracico atipico e sospetta coronaropatia ostruttiva : il protocollo tradizionale ( visita , stress test , coronarograa ) e il protocollo attuale , ( visita , stress test , ac - tcms ed eventuale coronarograa )  . 
lo stress test nei confronti dellac - tcms ha attenuto valori di accuratezza del 66% con sensibilit e specicit del 21% e 87% e valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) di 40% e 70% . 
il confronto tra acc e ac - tcms ha rilevato una sensibilit e specicit pari a 92% e 89% , un vpp e vpn pari a 89% per unaccuratezza complessiva del 92% . 
il protocollo radiol med ( 2013 ) 118 : 12941308 1295 protocol : 1 , 645 euro against 322 euro ( mean ) , but it shows a better cost - effectiveness ratio . 
 keywords mdct coronary angiography stress test coronary angiography cost analysis atypical chest pain tradizionale risultato avere costi pi elevati rispetto a quello modicato dalla ac - tcms , 1645 euro contro 322 euro ( media ) , ma dimostra un miglior rapporto costo / efcacia . 
dai nostri dati , lutilizzazione di un protocollo che prevede lac - tcms come spartiacque principale per i pazienti da inviare alla coronarograa , risulta vantaggioso in termini di costo e di efcacia diagnostica . 
 parole chiave angiograa coronarica mediante tcms stress test coronarograa analisi dei costi dolore toracico atipico introduction introduzione coronary angiography ( ca ) with multidetector computed tomography ( mdct - ca ) represents an accurate diagnostic test to rule out obstructive coronary artery disease ( cad ) [ 18 ]  . 
the stress test is widely used as a rst - level cardiological screening test in patients with low to intermediate cardiovascular risk ; however , its diagnostic performance is lower than that of mdct - ca [ 10 ] , with a high number of false positive tests and an even higher number of false negative tests . 
in patients with prolonged chest pain , cca is frequently the only examination able to denitively exclude obstructive cad , as it represents the gold standard technique for detecting coronary stenosis . 
the aim of our study was to evaluate , the cost - effectiveness and incremental diagnostic value of mdct - ca in clinical practice in patients with suspected obstructive cad compared with the traditional diagnostic pathway . 
attualmente le linee guida indicano nel caso di pazienti con angina stabile , dolore toracico tipico o atipico ed in presenza di fattori di rischio cardiovascolare , lesecuzione di un elettrocardiogramma ( ecg ) e di una prova da sforzo [ 911 ]  . 
nonostante lutilizzo del test da sforzo sia ampiamente usato come screening cardiologico di primo livello nella categoria di pazienti a basso - medio rischio cardiovascolare , la sua performance diagnostica decisamente minore rispetto a quella fornita dalla ac - tcms [ 10 ] , con un elevato numero di falsi positivi , ma soprattutto di falsi negativi . 
i pazienti con dolore toracico tipico e atipico , ma con test da sforzo negativo sono indirizzati ad ulteriori test diagnostici non invasivi , ma spesso lacc si rivela lunico esame in grado di escludere denitivamente la coronaropatia ostruttiva se la sintomatologia dolorosa perdura , ed essa rappresenta oggi il gold standard per lidenticazione delle stenosi coronariche . 
scopo del presente 1296 materials and methods study population between january 2009 and june 2011 , 720 consecutive patients ( mean age , 6511.5 years ; 344 men ) undergoing 64 - slice mdct - ca ( brilliance 64 , philips , the netherlands ) were considered . 
 all patients underwent mdct - ca if spontaneous or - blocker - induced heart rate was 65 bpm and if they were able to hold their breath for the time required to acquire the volume data ( 1012 s )  . 
the following patients were excluded from the mdct - ca study : symptomatic patients with acute chest pain and an ecg positive for ischaemia , those with a heart rate 65 bpm , those with a known allergy to iodinated contrast material , pregnant women , patients with respiratory failure , with unstable clinical condition and severe heart failure . 
cca on the basis of analysis of specicity , sensitivity , ppv and npv of the individual techniques ( especially in view of the well - known low accuracy of the cycle test ) and the costeffectiveness ratio of the rst two pathways , we considered a third diagnostic pathway in which mdct - ca was the rst - line modality : 3 . 
mdct - ca positive for stenosis > 50% radiol med ( 2013 ) 118 : 12941308 lavoro valutare il valore diagnostico incrementale dellintroduzione della ac - tcms nella gestione clinica del paziente con sospetta coronaropatia ostruttiva ( cad ) rispetto al tradizionale percorso diagnostico in termini di rapporto costo / efcacia . materiali e metodi popolazione campione nel periodo compreso tra gennaio 2009 e giugno 2011 sono stati considerati 720 pazienti consecutivi ( et media 6511 , 51 anni , 344 maschi ) sottoposti ad ac - tcms mediante apparecchio tcms a 64 detettori ( brilliance 64 , philips , paesi bassi ) disponibile presso il nostro istituto . tutti i pazienti dello studio sono stati sottoposti allindagine ac - tcms se la frequenza cardiaca era 65 battiti per minuto ( bpm ) spontanea o indotta dalla somministrazione endovenosa di - bloccante , e se la capacit di mantenere unapnea era sufciente per il periodo di acquisizione del volume toracico ( 1012 s )  . 
un altro criterio di inclusione stata la presenza di ritmo cardiaco sinusale ; sono stati accettati nello studio , tuttavia , anche i pazienti con brillazione atriale cronica con risposta ventricolare medio bassa , inducibile < 65 bp sono stati esclusi dal presente studio tutti i pazienti con cad nota trattati con stent o by - pass . 
sono stati esclusi i pazienti sintomatici con dolore toracico acuto e ecg positivo per ischemia , con frequenza cardiaca > 65 bpm , allergia nota al mezzo di contrasto iodato , gravidanza , insufcienza respiratoria , stato clinico instabile e scompenso cardiaco di grado severo . 
caa pretest evaluation for each patient , we recorded indication for the test and calculated the pretest risk ( mdct - ca ) of cad in relation to : smoking hypertension positive family history of cad diabetes mellitus and hypercholesterolaemia using the morise score 2 . 
acc. sulla base dellanalisi dei dati in termini specicit , sensibilit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) delle metodiche ( in particolare della scarsa accuratezza del cicloergometro gi nota in letteratura ) , e del rapporto costo / efcacia dei primi due percorsi , stato inoltre ipotizzato il seguente percorso diagnostico in cui 1298 radiol med ( 2013 ) 118 : 12941308 fig . 
3 percorso diagnostico modicato dallutilizzo della ac - tcms prima del cicloergometro nei pazienti con dolore toracico atipico . mdct - ca scan scan protocol the contrast - enhanced study was obtained using 80100 ml of iodinated contrast medium ( iomeprol 400 mgi / ml , iomeron , bracco , milan , italy ) injected intravenously at 5 ml / s ow rate , followed by 40 ml of saline . 
the contrast medium was injected with an automatic dual - head injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an antecubital vein with a 16 - g needle cannula . 
the optimal acquisition protocol was chosen based on the patients heart rate and anthropometric characteristics [ body mass index ( bmi ) ] in order to balance dose sparing with optimal image quality . 
 image analysis images were evaluated by a radiologist with 6 years of continuing training in mdct - ca and , in the event of disagreement between clinicalanamnestic data and mdct - ca ndings , the case was reviewed with a cardiologist . 
for each lesion , a visual assessment of the stenosis was performed using current international criteria [ 7 , 8 ] : 020% , no stenosis or wall irregularities 2050% , nonsignicant stenosis lac - tcms risulta essere metodica di prima linea : 3 . 
acc. valutazione pre - test per ciascun paziente stata registrata lindicazione allesame ed stato tracciato un prolo di rischio pre - test ( preac - tcms ) di cardiopatia aterosclerotica in rapporto a : anamnesi positiva per fumo ; ipertensione ; familiarit per eventi cardiaci acuti ; diabete e ipercolesterolemia utilizzando il morise score . esecuzione dellesame ac - tcms protocollo di scansione sono stati somministrati per via endovenosa 80100 ml di mezzo di contrasto non ionico iodato ( iomeprol 400 mgl / ml , iomeron , bracco , milano , italia ) con un usso di 5 ml / s , seguito da 40 ml di soluzione salina allo stesso usso . 
il mezzo di contrasto stato introdotto tramite un iniettore automatico a doppia pompa ( stellant , medrad , pittsburgh , pa , usa ) connesso a una vena antecubitale con un agocannula da 16 g . 
the ecg trace was recorded in all stages of the test , starting from rest phase through incremental negative energy of 25 w every 2 min to achieve the expected maximal threshold . 
la valutazione delle arterie coronarie ha previsto uno studio dei singoli segmenti effettuato seguendo una classicazione dellalbero coronarico a 17 segmenti secondo lamerican heart association ( aha ) [ 15 ]  . 
per ogni lesione stata effettuata una stima di stenosi visuale distinta secondo i criteri internazionali [ 7 , 8 ] : 0%20% , assenza di stenosi o irregolarit parietali ; 20%50% , stenosi non signicativa ; 50%70% , stenosi signicativa ; 70%100% , stenosi severa occludente o sub occludente . test da sforzo mediante cicloergometro ciascun paziente stato posizionato su un cicloergometro in posizione seduta . 
il tracciato elettrocardiograco stato registrato in tutte le fasi dellindagine , partendo da una fase di riposo no ad arrivare a energie negative incrementali di 25 w ogni 2 minuti , no al raggiungimento della soglia massima teorica . 
il test risultato dubbio per patologia signicativa in caso vi fosse un sotto - slivellamento st minore dei parametri indicati con persistenza del pattern al recupero , in presenza di sintomatologia tipica , o se presente angina tipica anche in assenza di alterazioni elettrocardiograche . 
in tutti gli altri casi lesame risultato essere negativo . analisi statistica sono stati calcolati la specicit , la sensibilit , il vpp , il vpn rispettivamente di : ac - tcms vs . 
equipment costs were calculated on the basis of mean time of use for each examination and taking into consideration purchase cost ( obtained from ofcial data of the hospital directorate ) and amortisement ( calculated on a temporal basis , at constant annual value , assuming a mean lifespan of 8 years for radiological and cardiological equipment )  . we did not calculate the common costs of the production factors of the radiology and cardiology departments , i.e. 
 factors that support the diagnostic activity , as they do not change with the total yearly number of examinations and are an independent variable , being specic for each department . 
in the evaluation of differential costs , we considered the technical act , ignoring all other costs related to patient management , as done in other published studies [ 16 , 17 ]  . considering that the cycle test , ecg and mdct - ca were performed on an outpatient basis , the cost of the single examinations was calculated on the basis on the italian national health service tariffs . 
in evaluating the cost - effectiveness ratio , we used patterson et al.s il costo differenziale stato calcolato per ogni percorso diagnostico come somma dei costi delle apparecchiature , dei costi dei materiali e dei costi del personale , con le modalit in uso presso il nostro istituto e presso il dipartimento di cardiologia . 
il costo delle apparecchiature stato calcolato in base al tempo medio di utilizzo per esame delle stesse , valutando il costo dacquisto ( ricavato dalla documentazione ufciale della direzione sanitaria ) ed il calcolo dellammortamento ( effettuato su base temporale , a valore annuo costante , assumendo una durata media della vita delle apparecchiature radiologiche e cardiologiche di otto anni )  . non sono stati calcolati i costi comuni dei fattori produttivi interni allistituto di radiologia e del dipartimento di cardiologia , cio quei fattori che garantiscono unattivit di supporto a tutti gli atti diagnostici svolti nel reparto , poich si tratta di costi che non si modicano al variare del numero totale di esami svolti nel periodo annuo e che , essendo specici per ogni struttura , rappresentano una variabile indipendente . 
nella valutazione del costo differenziale ci siamo limitati a considerare latto tecnico , ignorando tutti gli altri costi legati alla gestione del paziente , cos come in altri lavori della letteratura [ 16 , 17 ]  . considerando il fatto che il cicloergometro , lecg e la ac - tcms sono stati eseguiti in regime ambulatoriale senza necessit di ricovero il costo delle singole procedure stato calcolato in base al tariffario del servizio sanitario nazionale applicato anche per esami eseguiti in regime ambulatoriale espletati nella nostra unit operativa . 
 analisi costo / efcacia stata calcolata per ogni percorso lanalisi di costo - efcacia , una forma di piena valutazione economica dove sia i costi che le conseguenze di un programma diagnostico o terapeutico vengono contemporaneamente esaminati . 
usando i dati di sensibilit e specicit , e quindi di accuratezza diagnostica delle singole metodiche stata effettuata lanalisi costo - efcacia dei tre protocolli diagnostici assumendo che il ruolo di esame dirimente era : per il primo protocollo la acc ; per il secondo protocollo il cicloergometro ; per il terzo protocollo la ac - tcms . lefcacia di tali percorsi quindi stata considerata pari a quella dellesame dirimente di quel dato protocollo . 
inne i costi delle diverse metodiche sono stati messi in relazione con laccuratezza diagnostica delle stesse , ottenendo valori di costo / accuratezza per ogni percorso diagnostico . radiol med ( 2013 ) 118 : 12941308 table 2 costs of the different procedures 1301 cost analysis procedure / admission description tariff ( euro ) cycle test mdct - ca cardiological examination ecg diagnostic angiography preprocedure examinations place where procedure is done laboratory tests chest x - ray echocardiogram total pre - procedure examinations haemodynamic room operators involved in the operating room / dedicated clinic qualication execution time personnel costs + regional tax materials , reagents , devices , etc . 
finally , the costs of each method were correlated with its diagnostic accuracy in order to calculate the cost - accuracy values of each diagnostic pathway . results all patients who underwent mdct - ca were at low to intermediate risk of cad , with a discrepancy between symptoms and the clinicallaboratory data . 
it was dened as optimal in 360 / 550 ( 85% ) cases , moderate in 62 / 550 ( 13% ) and poor in 8 / 550 ( 2% ) due to breathing motion artefacts during the scan . 
scans were performed without any dose - saving protocol ( 16.05 msv ) in 41% cases , with retrospective gating and dose modulation ( 8.2 msv ) in 45% and with prospective gating ( 1.2 msv ) in 14% cases . according to image evaluation , 393 / 550 ( 71% ) patients had nonsignicant lesions , 122 / 393 ( 31% ) of whom had no coronary lesions , whereas 157 / 393 ( 29% ) patients had at least one signicant lesion . 
this test conrmed signicant stenosis ( > 50% of coronary lumen narrowing ) in 166 / 128 ( 91% ) patients , and 59 / 128 ( 46% ) patients were revascularised . 
when comparing cca to mdct - ca , the detection of signicant stenosis in a per - patient analysis showed 92% sensitivity , 89% specicity , and 89% and 92% ppv and npv , respectively . 
the overall diagnostic accuracy was 91% . based on risk prole and clinical data , 214 / 550 ( 39% ) patients underwent the cycle test , 15% with positive results and 85% with uncertain or nonsignicant results . 
when considering mdct - ca as the gold standard , the diagnostic performance of the stress test in discriminating patients with signicant stenosis showed a sensitivity and specicity risultati i pazienti sottoposti ad indagine ac - tcms erano soggetti con basso - medio rischio di cad con discrepanza tra sintomatologia e dati clinico - laboratoristici . 
i rilievi anamnestici hanno permesso di distinguere un prolo di rischio basso per la presenza di uno o due fattori di rischio e intermedio per la presenza di due o pi fattori di rischio . 
la qualit delle indagini actcms valutata dal radiologo e basata su un criterio qualitativo stata denita in 360 / 550 ( 85% ) casi buona in 62 / 550 ( 13% ) casi discreta , in 8 / 550 ( 2% ) casi scarsa per artefatti da movimento respiratorio del paziente durante la scansione . 
lacquisizione delle immagini stata effettuata nel 41% dei casi senza alcun tipo di protocollo a risparmio di dose ( 16 , 05 msv ) , nel 45% dei casi con gating retrospettivo e modulazione della dose ( 8 , 2 msv ) e nel 14% dei casi con gating prospettico ( 1 , 2 msv )  . nellambito della valutazione delle immagini in 393 / 550 ( 71% ) casi non vi erano lesioni signicative , dei quali 122 / 393 ( 31% ) erano cad free , cio totalmente privi di lesioni coronariche ; nei rimanenti 157 / 393 ( 29% ) pazienti sono state riconosciute lesioni signicative ad almeno un segmento coronarico . 
dei 157 pazienti risultati positivi allac - tcms , 128 / 157 ( 82% ) sono stati sottoposti ad acc , che ha confermato la stenosi > 50% del lume coronarico in 116 / 128 ( 91% ) pazienti . 
il confronto diretto tra acc e ac - tcms nella valutazione di stenosi signicative mediante analisi per paziente ha rilevato una sensibilit pari a 92% , una specicit pari a 89% , un vpp e vpn pari a 89 % e 92% rispettivamente . 
laccuratezza diagnostica globale della ac - ctms risultata essere pari a 91% . sulla base dei proli di rischio e dei dati clinico anamnestici precedentemente allac - tcms sono stati sottoposti a cicloergometro 214 / 550 ( 39% ) pazienti di cui solo il 15% risultato positivo mentre l85% dubbio o non signicativo . 
 considerando come riferimento la ac - tcms , la capacit diagnostica della prova da sforzo nella identicazione di pazienti con lesioni signicative ha dimostrato una sensibilit e specicit pari a 21% e 87% , con un vpp e vpn di 42% e 70% rispettivamente ( tabella 3 )  . il costo di ogni percorso diagnostico stato calcolato sulla base della somma dei costi delle differenti procedure e riportato in tabella 4 . 
i protocolli 2 e 3 evitando di sottoporre i pazienti negativi a procedure angiograche , consentono un risparmio medio per ogni paziente negativo di 1323 euro e 1384 euro rispettivamente . 
cca when evaluating patients with signicant coronary artery stenosis tabella 3 performance diagnostica espressa dalla prova da sforzo nella determinazione di pazienti con lesioni signicative vs angiograa coronarica mediante tomograa computerizzata multistrato ( ac - tcms ) cycle test vs . 
 by avoiding the need for cca , the second and third pathways allow average savings of 1 , 323 euro and 1 , 384 euro , respectively , in the case of negative patients . regarding the cost - effectiveness analysis , for each diagnostic pathway , we obtained a curve representing the trend of improvement in relation to the pretest percentage of cardiovascular risk ; the curves of three pathways are compared in figure 4 . discussion few studies have reported on the real diagnostic accuracy of mdct - ca obtained in a clinical setting , which reects the effective performance of the technique in routine practice [ 4 , 19 , 20 ]  . 
in clinical practice , the cardiologist and the clinician can use the information provided by the method to send the patient to an appropriate diagnostic pathway with optimal accuracy [ 20 ]  . consistent with the literature , the high positive and negative predictive values found in our series gives mdct - ca a gatekeeping role in relation to cca . 
despite this , our data conrm a valid diagnostic performance of mdct - ca also in a real clinical setting [ 4 , 9 , 19 , 20 ]  . the suboptimal diagnostic performance of the stress test in stata ottenuta una curva che rappresenta il trend di miglioramento in rapporto alla percentuale pre - test del rischio cardiovascolare ; le curve dei tre percorsi sono messe a confronto nella figura 4 . discussione attualmente pochi studi riportano la reale accuratezza diagnostica estrapolata da un contesto clinico , che consiste nella effettiva performance della metodica sul campo [ 4 , 19 , 20 ]  . 
nella pratica clinica , il cardiologo ed il clinico possono utilizzare le informazioni ottenute da questa metodica per indirizzare con maggior accuratezza il paziente al percorso diagnostico terapeutico ottimale [ 20 ]  . 
 in linea con i dati della letteratura anche nella nostra casistica lelevato valore predittivo positivo e negativo della ac - tcms gli conferisce un ruolo di spartiacque nei confronti della coronarograa . 
nonostante ci i nostri dati confermano unottima performance diagnostica dellac - tcms anche in un contesto clinico reale [ 4 , 9 , 19 , 20 ]  . la scarsa performance diagnostica espressa dalla prova da sforzo nella determinazione di pazienti con lesioni signicative ottenuta nel nostro lavoro aderente ai risultati espressi in precedenti lavori pubblicati su questo argomento [ 10 , 11 ]  . 
because the diagnostic performance of this test is inadequate for this patient population , the purpose of our study was to modify the diagnostic algorithm by incorporating the use of mdct - ca . 
questi daranno informazioni utili sulla riduzione di riserva coronarica causata dalle lesioni evidenziate anatomicamente dalla tc , cos da indirizzare a procedure invasive di rivascolarizzazione solo i pazienti con lesioni ateromasiche funfig . 
 these tests could give additional useful information about the reduction of coronary reserve resulting from the lesions depicted by mdct , so as to send only those patients with functionally signicant cad to invasive revascularisation procedures . 
this modied algorithm changes the approach to diagnostic cca and our study , as many others before , shows how this can lead to several disadvantages compared with a multi - step approach [ 16 ]  . 
cost - effectiveness analysis correlates the percentage of correct diagnoses to the cost necessary to reach them ; this aspect provides an additional indicator to mere diagnostic accuracy . on the basis of our results and the recent literature [ 11 , 16 ] it is clear that the introduction of mdct - ca improves diagnostic performance ; at the same time , it is important to emphasise when to use it in the clinical workup . 
the modied diagnostic pathway with mdct - ca provides a greater overall diagnostic accuracy , but it takes on a high value of cost - effectiveness if mdct - ca is considered the rst - level examination in place of the cycle test . 
this leads to higher cost - effectiveness values compared with the standard pathway , which , even though burdened by the high cost of cca , obtained fairly good cost - effectiveness values as a result of its high sensitivity . 
the use of mdct - ca as a screening test is an early , effective and relatively inexpensive diagnostic tool in a population in which the stress test has limited sensitivity . 
consequently , it is preferable to send to cca only patients with positive ndings at mdct - ca and at low to intermediate risk , and to use cca only for revascularisation procedures . 
our data indicate that the low diagnostic accuracy of the stress test ( 66% ) , especially in low - risk patients ( in whom accuracy falls to about 50% ) , makes the second diagnostic protocol the least economically viable . according to the cost - effectiveness analysis based on our data , a single mdct - ca costs about 230.03 euro , whereas cca costs about 1 , 551 euro . 
mdct - ca has a better cost - effectiveness ratio compared with cca as long as the pretest probability is < 86% , which corresponds to low to intermediate risk patients . the results of our study demonstrate how , based on clinical and anamnestic data , no signicant lesions were detected zionalmente signicative . 
tale algoritmo modicato cambia dunque lapproccio mirato verso lacc diagnostica , e il nostro studio , come altri precedenti , mostra come ci comporti diversi svantaggi , confrontato con un approccio a stadi [ 16 ]  . 
 lanalisi costo / efcacia mette in relazione la percentuale di diagnosi corrette con il costo necessario a raggiungerle ; questo aspetto fornisce quindi un indicatore aggiuntivo alla semplice accuratezza diagnostica . 
 dai risultati ottenuti e dalla recente letteratura [ 11 , 16 ] si pu evincere come lintroduzione della ac - tcms migliori la performance diagnostica ; al tempo stesso importante sottolineare il punto in cui essa viene inserita nel workup clinico . 
il protocollo diagnostico modicato con lac - tcms fornisce una maggiore accuratezza diagnostica globale , ma acquisisce un alto valore di costo / efcacia se la ac - tcms viene posta come esame di primo livello , al posto del cicloergometro . 
in tal modo si ottengono valori di costo / efcacia maggiori del protocollo standard , che pur gravato dagli alti costi dellacc , otteneva dei valori di costo / efcacia discreti dovuti allalta sensibilit della stessa . 
 vista la popolazione presa in considerazione , di individui con rischio medio - basso , la metodica che fornisce il migliore rapporto costo / efcacia risulta essere lac - tcms . 
 lutilizzo dellacc con il solo scopo diagnostico , pur garantendo una sensibilit del 100% , gravato da costi elevati , di conseguenza preferibile inviare allacc solo i casi positivi selezionati tramite lac - tcms ed utilizzare lacc solo per procedure interventistiche di rivascolarizzazione nei pazienti a basso - medio rischio . 
dai nostri dati si pu evincere che la scarsa accuratezza del cicloergometro ( 66% ) , specie nei pazienti a basso rischio ( dove la sua accuratezza scende a circa il 50% ) , rende il secondo protocollo diagnostico , addirittura il meno conveniente in termini economici . 
secondo una analisi di costo - efcacia basata sui nostri dati la actcms fa registrare un costo totale di 230 , 03 euro mentre la coronarograa fa registrare un costo totale 1551 euro . 
la ac - tcms presenta un rapporto costo - efcacia pi favorevole rispetto alla coronarograa no all86% di probabilit pre - test , ossia in condizioni di rischio cardiovascolare basso ed intermedio . i risultati del nostro studio mostrano come sulla base della clinica e dei dati anamnestici nei 2 / 3 circa dei pazienti non siano state riscontrate lesioni signicative , abbreviando quindi gli iter terapeutici e migliorando la performance diaradiol med ( 2013 ) 118 : 12941308 1307 in two of three patients examined , thus shortening their therapeutic pathway and improving diagnostic performance in assessing low to intermediate risk patients . 
there were , however , many lesions with stenosis 50% , which necessitated a comparison with cca , stress ecg or scintigraphy , conrming the presence of borderline lesions but excluding indications for treatment with angioplasty or stenting . 
 our evaluation was carried out on a patient - based analysis instead of a per - segment or a per - vessel analysis , so as not to exclude from further investigation patients potentially affected by signicant cad . gnostica nella valutazione del paziente a rischio . 
molte sono per le lesioni con stenosi 50% che hanno necessitato di un confronto mediante coronarograa o eco - stress o scintigraa , confermando la presenza di lesione borderline , ma escludendone lindicazione al trattamento mediante angioplastica o stent . 
la nostra valutazione stata effettuata su unanalisi per paziente e non per segmento o vaso , in modo da cercare di non escludere da eventuali ulteriori indagini soggetti potenzialmente affetti da malattia coronarica signicativa . conclusioni conclusions our study , in agreement with the literature , conrms the better diagnostic performance of mdct - ca compared with the stress test and its similar accuracy to cca . 
in addition , the use of a pathway that considers mdct - ca as a gatekeeper to identify patients to send to cca is advantageous in terms of cost and diagnostic effectiveness . il nostro studio , in linea con i dati della letteratura , conferma una miglior performance diagnostica dellac - tcms nei confronti del test da sforzo ed unaccuratezza simile a quella dellacc . 
inoltre , lutilizzazione di un protocollo che prevede lac - tcms come spartiacque principale per identicare i pazienti da inviare allacc , risulta vantaggioso in termini di costo e di efcacia diagnostica . 
orsola - malpighi , via massarenti 9 , 40128 bologna , italy 2department of clinical sciences , section of radiological sciences , university of parma , via gramsci 14 , 43100 parma , italy corrispondence to : d . 
ninety - seven patients with a total of 146 subsolid nodules [ 140 pure ground - glass opacities ( pggos ) and six mixed ground - glass opacities ( mggos ) ] were retrospectively recruited . 
two chest radiologists independently reviewed the hrct features of the nodules ( location , shape , size , density ) and the patients clinical characteristics ( sex , age , smoking and cancer history )  . 
an increase in size and / or density was seen in 32% of ssn , and in particular in partly solid ( mggos ) , large ( 10 mm ) and irregular nodules . 
ssn growth was more frequent in patients with advanced age and a history of smoking , and occurred even after a long period of stability ( 39% of pggos changed over 3 years )  . 
the observation of a sample of cancer patients has shown that ssn may frequently grow in size and / or density in these patients , especially if associated riassunto obiettivo . 
sono stati reclutati in maniera retrospettiva 97 pazienti , per un totale di 146 nss ( 140 ground glass puri pggo , e 6 ground glass misti mggo )  . 
le caratteristiche hrct dei noduli ( localizzazione , forma , dimensioni , densit ) e quelle cliniche dei pazienti ( sesso , et , abitudine al fumo e anamnesi oncologica ) sono state valutate indipendentemente da due radiologi toracici . 
durante il follow - up il 58% dei nss rimasto invariato , il 10% scomparso , mentre in circa un terzo dei casi ( 32% ) si vericato un aumento di dimensioni e / o densit , specialmente in caso di noduli parzialmente solidi ( mggo ) , di grandi dimensioni ( 10 mm ) e irregolari . 
la crescita stata pi frequente in soggetti di et avanzata e con storia di fumo e si vericata anche dopo un lungo periodo di stabilit ( 39% di pggo modicati oltre i 3 anni )  . 
 le patologie oncologiche pi frequentemente associate a crescita dei nss sono risultate i tumori del polmone 1270 radiol med ( 2013 ) 118 : 12691280 with cancers of lung , breast , colon and bladder . 
losservazione di un campione di pazienti oncologici ha dimostrato come i nss frequentemente possono crescere di dimensioni e / o densit in questi pazienti , soprattutto se associati a tumori del polmone , della mammella , del colon e della vescica . 
la maggioranza di essi ha mostrato un tempo di sviluppo estremamente lento , perci , un follow - up superiore ai 3 anni appare giusticato anche nei pazienti oncologici . parole chiave nodulo polmonare subsolido ground glass hrct follow - up paziente oncologico introduction introduzione the widespread use of whole - body computed tomography ( ct ) for diagnosing and monitoring malignant disease has led to a signicant increase in the detection of subsolid pulmonary nodules ( ssn ) , whose clinical signicance remains unclear . the category of ssn includes those consisting exclusively of ground - glass opacity ( pure ground - glass opacity pggo ) and mixed or partially solid nodules , consisting of a solid component and a ground - glass opacity ( mixed groundglass opacity mggo ) [ 1 , 2 ]  . ssn can be the expression of benign conditions ( organising pneumonia , focal brosis , areas of inammation or bleeding ) , but may also represent preneoplastic lesions , such as atypical adenomatous hyperplasia ( aah ) [ 3 ] , or adenocarcinoma in situ ( formerly bronchiolo - alveoar carcinoma bac [ 4 , 5 ] ) and , less frequently , pulmonary metastasis [ 6 , 7 ]  . ssn generally display slower growth rates as compared to solid lesions . 
focal interstitial brosis also persists over a prolonged follow - up period and its growth pattern over time it still unknown [ 9 ]  . these data highlight the need for longer follow - up periods , as two years are not sufcient for determining the benign or malignant nature of ssn . 
 however , it is conceivable that subsolid nodules detected in routine settings may show different ct features and growth patterns . our study retrospectively analysed a population consisting of cancer patients in a non - screening clinical context . 
stato riportato un tempo di raddoppio di 988470 giorni per laah , 567168 giorni per il bac e 384212 giorni per ladenocarcinoma misto con componente bac [ 8 ]  . 
anche la brosi interstiziale focale persiste nellarco di un follow - up prolungato ed ancora sconosciuto il suo pattern di crescita nel tempo [ 9 ]  . questi dati mettono in luce limportanza di un follow - up prolungato , in quanto il tradizionale follow - up a 2 anni insufciente per determinare la natura benigna o maligna di un nss . 
tuttavia , ipotizzabile che noduli rilevati in un contesto di routine possano mostrare caratteristiche tc e comportamento differenti . il nostro studio ha analizzato retrospettivamente una poradiol med ( 2013 ) 118 : 12691280 1271 table 1 details of the patients cancer types . 
twenty patients were affected by a primary lung cancer , 77 by an extrathoracic malignancy lung cancer : 20 adenocarcinoma 8 adenocarcinoma in situ ( bac ) 2 extrapulmonary cancer : 77 breast 15 prostate 4 kidney 3 colon 11 ovary 4 skin carcinoma 2 squamous cell carcinoma 4 histology not available 6 lnh 6 skin melanoma 3 endometrium 1 liver 6 bile ducts 3 retroperitoneal liposarcoma 1 bladder 6 pancreas 3 ureter 1 stomach 4 gist 3 larynx 1 bac , bronchioloalveolar carcinoma ; lnh , non - hodgkin lymphoma ; gist , gastrointestinal stromal tumour tabella 1 speciche relative al tipo di tumore dei pazienti . 
venti pazienti avevano un tumore polmonare primitivo , 77 invece erano affetti da un tumore extratoracico tumori polmonari : 20 adenocarcinoma 8 adenocarcinoma in situ ( bac ) 2 carcinoma a cellule squamose 4 istologia non disponibile 6 tumori extrapolmonari : 77 mammella 15 prostata 4 reni 3 colon 11 ovaio 4 carcinoma cutaneo 2 lnh 6 melanoma cutaneo 3 endometrio 1 fegato 6 dotti biliari 3 liposarcoma retroperitoneale 1 vescica 6 pancreas 3 uretere 1 stomaco 4 gist 3 laringe 1 bac , carcinoma bronchiolo - alveolare ; lnh , linfoma non hodgkin ; gist , tumore stromale gastro - intestinale evaluated the ct features that can best differentiate between benign and malignant ssn , their evolution during follow - up and which neoplastic diseases are most frequently associated with ssn growth in size and / or in density . polazione composta da pazienti oncologici , fuori da ogni contesto di screening tumorale . 
sono state valutate le caratteristiche tc in grado di distinguere tra nss benigni e maligni , la loro evoluzione durante il follow - up e le patologie neoplastiche pi frequentemente associate a crescita dimensionale e / o densitometrica delle lesioni . materials and methods patients ninety - seven cancer patients ( 48 women and 49 men ; age range , 1988 years ; mean age , 65 years ) with evidence of ssn on high - resolution ct ( hrct ) were retrospectively identied from among all whole - body ct studies completed with thin reconstructions on the lung parenchyma ( hrct ) , performed at our institution between june 2006 and june 2010 . 
at least two hrct examinations were available for all patients in order to evaluate the evolution of ndings ; follow - up varied from 3 to 56 months ( mean , 27 months ) with an average of six hrct scans per patient . materiali e metodi pazienti novantasette pazienti oncologici ( 48 donne e 49 uomini , di et compresa tra 19 e 88 anni , et media 65 anni ) con evidenza di nss alla hrct , sono stati identicati retrospettivamente , sul totale delle tc total body completate con ricostruzioni sottili sul parenchima polmonare ( hrct ) effettuate nel nostro istituto tra giugno 2006 e giugno 2010 . 
la ricerca stata eseguita mediante un sistema di ricerca computerizzato per parola - chiave ( nodulo , ground - glass ) sullarchivio dei referti radiologici ( e - ris pacs , biotron )  . venti pazienti erano affetti da un tumore polmonare primitivo ( 20 , 6% ) e 77 da una neoplasia extratoracica , in assenza di tumori polmonari primitivi ( 79 , 4% )  . 
per tutti i pazienti erano disponibili almeno due controlli hrct per la valutazione evolutiva dei reperti ; la durata del follow1272 radiol med ( 2013 ) 118 : 12691280 since the study aim was to evaluate indeterminate small subsolid nodules , patients with lesions 3 cm in size and those with more than four nodules were excluded from the analysis . hrct protocol ct scans were performed using three different ct systems : 70 patients ( 72.2% ) were examined with a 16 - detector - row scanner ( siemens sensation cardiac , forchheim , germany ) , 21 patients ( 21.6% ) with a different 16 - detector - row scanner ( ge medical systems lightspeed , milwaukee , wi ) and six patients ( 6.2% ) with a 64 - detector - row scanner ( ge medical systems lightspeed , milwaukee , wi )  . the lung parenchyma was evaluated with hrct volumetric reconstructions . 
reconstruction parameters were : 2 mm slice thickness , 1 mm reconstruction interval , 120 kvp , 180 ma ( with automatic tube current modulation ) and 1.15 mm pitch for the 16 - detector - row ct scanners ; 1.25 mm slice thickness , 1 mm reconstruction interval , 120 kvp , 180 ma ( with automatic tube current modulation ) , and 0.5 mm pitch for the 64 - dectector - row scanners . 
the follow - up of each patient was performed with the same equipment and reconstruction parameters . interpretation of hrct scans all hrct scans were reviewed separately by two chest radiologists with different levels of experience in chest ct . 
dimensional variations > 1 mm , observed by both operators , were considered signicant . according to the densitometric characteristics , ssn were classied as pggo when the broncho - vascular structures could be identied within an area of increased parenchymal density , and mggos when , by switching window widths and levels , also a solid component could be appreciated . 
 densitometric changes were classied as : ( 1 ) stable , ( 2 ) increased density , ( 3 ) development of a solid component or ( 4 ) evolution into a completely solid nodule . finally , the assessments of the densitometric and size up stata variabile dai 3 ai 56 mesi ( media di 27 mesi ) con una media di circa 6 controlli hrct per paziente . dal momento che lo scopo dello studio era di valutare piccoli noduli subsolidi a signicato incerto , sono stati esclusi dallanalisi sia i pazienti con lesioni di dimensioni 3 cm sia quelli con pi di 4 noduli . protocollo hrct gli studi tc sono stati ottenuti utilizzando tre differenti apparecchiature : 70 pazienti ( 72 , 2% ) sono stati esaminati mediante una tc a 16 strati ( siemens sensation cardiac , forchheim , germany ) , 21 pazienti ( 21 , 6% ) mediante una differente tc a 16 strati ( ge medical systems lightspeed , milwaukee , wi ) e 6 pazienti ( 6 , 2% ) mediante una tc a 64 strati ( ge medical systems lightspeed , milwaukee , wi )  . la valutazione del parenchima polmonare stata eseguita con metodica hrct volumetrica . 
per le tc a 16 strati sono stati utilizzati i seguenti parametri di ricostruzione : spessore di strato 2 mm , intervallo di ricostruzione 1 mm , 120 kvp , 180 ma ( modulazione di corrente automatica ) , pitch 1 , 15 mm ; per le immagini ottenute con la tc a 64 strati , invece , sono stati usati i seguenti parametri : spessore di strato 1 , 25 mm , intervallo di ricostruzione 1 mm , 120 kvp , 180 ma ( modulazione di corrente automatica ) , pitch 0 , 5 mil follow - up di ciascun paziente stato eseguito con la medesima apparecchiatura e con gli stessi parametri di ricostruzione . interpretazione delle immagini hrct tutte le immagini hrct sono state visionate separatamente da due radiologi toracici con differente esperienza nellinterpretazione della tc del torace , non a conoscenza della storia clinica dei pazienti . 
per ogni nss sono state analizzate le seguenti caratteristiche hrct : ( 1 ) localizzazione , ( 2 ) numero ( lesioni singole o multiple ) , ( 3 ) forma ( rotondeggiante o irregolare ) , ( 4 ) dimensioni e caratteristiche densitometriche ( presenza / assenza di una componente solida ) alla prima hrct , ( 5 ) dimensioni e variazioni delle caratteristiche densitometriche alle hrct di controllo . per denire la dimensione dei nss stato ottenuto il diametro massimo assiale ( in mm ) allequatore di ogni nodulo , attraverso una nestra polmonare ( - 600 ( cid : 31 ) 1500 ) e ingrandimento ( cid : 31 ) 2 , dai due radiologi indipendentemente . 
confrontando le misure effettuate sullhrct iniziale con quelle effettuate nei successivi controlli stato possibile dimostrarne : ( 1 ) un aumento , ( 2 ) una riduzione , ( 3 ) la stabilit o ( 4 ) la scomparsa . 
stata considerata signicativa una variazione dimensionale > 1 mm , osservata da entrambi gli operatori . in base alle caratteristiche densitometriche , i nss sono stati classicati come pggo quando allinterno di una zona a incrementata densit era possibile individuare le strutture bronco - vasali , e mggo quando , modicando ampiezza radiol med ( 2013 ) 118 : 12691280 1273 changes were incorporated so that a ssn could be dened as changed ( if size and / or density changed ) , stable or disappeared . 
there was no disagreement about the presence or absence of lesions , while the few cases of disagreement regarding variations in shape or densitometry were subsequently resolved by consensus . statistical analysis the bland - altman test was used to evaluate inter - observer variability : for each ssn , the difference between the measurements performed by the rst and the second observer was calculated for both the baseline and the followup hrct . 
all statistical analysis was performed using spss ( statistical package for the social sciences , chicago , il )  . results a total of 146 ssn were analysed ( an average of 1.5 nodules per patient ; range , 14 )  . 
the mean size at baseline hrct was 9 mm ( range , 3 to 28 mm ) ; 70% of ssn were located in the upper lobes ; 119 were morphologically classied as rounded ( r ) and 27 as irregular ( ir )  . 
according to the baseline densitometric characteristics , six nodules ( 4.1% ) were classied as mggo ( 5 r , 1 ir ) and 140 nodules ( 95.9% ) as pggo ( 114 r , 26 ir )  . e livello della nestra , era possibile identicare anche una componente solida . 
le variazioni densitometiche sono state classicate come : ( 1 ) stabilit , ( 2 ) incremento di densit , ( 3 ) sviluppo di componente solida , ( 4 ) evoluzione in nodulo completamente solido . inne , i dati delle variazoni densitometiche e dimensionali sono stati integrati , in modo che ogni nss potesse essere denito modicato ( ove vi fossero variazioni dimensionali e / o densitometriche ) , invariato o scomparso . 
poich nessun nodulo nella nostra casistica diminuito di dimensioni ( un solo nodulo prima diminuito e successivamente scomparso ) , di seguito ci riferiremo a noduli modicati intendendo quelli aumentati di dimensioni e / o densit . variabilit inter - observer i limiti di concordanza delle misurazioni effettuate dai due operatori sono risultati : - 0 , 852 e 0 , 844 m poich la variabilit inter - observer risultata molto bassa , si deciso di considerare valide le misurazioni effettuate dal primo operatore . 
non si vericato alcun disaccordo circa la presenza / assenza delle lesioni , mentre i pochi casi di disaccordo vericatisi riguardo la forma o la variazione densitometrica e dimensionale sono stati successivamente risolti tramite consenso . analisi statistica per valutare la variabilit inter - observer stato utilizzato il test di bland - altman : per ciascun nss stata calcolata la differenza tra le misure effettuate dal primo osservatore e quelle del secondo osservatore , sia per la prima hrct sia per lultima hrct di controllo . 
la dimensione media alla hrct iniziale era 9 mm ( range da 3 a 28 mm ) ; morfologicamente 119 nss sono stati classicati come rotondeggianti ( r ) e 27 irregolari ( ir )  . 
al controllo dopo 36 mesi ( e ) si apprezza un ulteriore incremento dimensionale ( 13 mm ) cui si associa anche un incremento di densit , senza tuttavia la presenza di componente solida gos changed on a average of 15 months after rst detection ( range , 824 months )  . 
smoking was also found to be a factor of increased risk : 2.4% in current smokers and 1.7% in former smokers , compared to never - smokers . discussion the management of the ssn presents several as yet unresolved problems . 
considering that transient nodules may disappear within 36 months , the importance of short - term mente come lesioni maligne ( 7 metastasi e 5 tumori primitivi ) ( tabella 2 )  . 
i noduli modicati avevano una dimensione media superiore rispetto a quella dei noduli stabili ( 11 mm vs 7 , 8 mm ) ; ponendo un cut - off 10 mm , la signicativit risultata < 0 , 001 . 
i pggo rotondeggianti di piccole dimensioni ( < 5 mm ) sono tendenzialmente rimasti invariati nel tempo ( p = 0 , 007 ) , mentre stata riscontrata una tendenza dei pggo irregolari a modicarsi maggiormente ( p = 0 , 055 )  . 
al controllo dopo 45 mesi ( f ) il nodulo appare incrementato di dimensioni ( 26 mm ) , con caratteristiche densitometriche invariate hrct follow - up to document the persistence of lesions [ 11 ] is known . 
nella nostra casistica anche il fumo rappresenta un fattore di aumentato rischio : 2 , 4% nei current smokers , mentre negli ex - fumatori il rischio incrementato di 1 , 7% rispetto ai non fumatori . radiol med ( 2013 ) 118 : 12691280 1277 fig . 
il nodulo appare invariato al controllo a 4 mesi ( b ) , ridotto di dimensioni a 10 mesi ( c ) , mentre non pi apprezzabile a 20 mesi ( d )  . 
this means that pggo stability , even over a prolonged period of time , should not necessarily be considered evidence of benignity . in their interim guidelines [ 14 ] , godoy and naidich suggested a follow - up of at least three - years for lesions between 5 and 10 mm in size , while all mggo , regardless of size , should be removed because they are very likely to be cancerous . only a few studies have addressed the clinical signicance of ssn in patients with cancer . 
 [ 15 ] , in a study of 34 patients with a history of extrapulmonary cancer , reported that ssn tend to have a high rate of malignancy , but none of the 59 ggos analysed were found to be a metastasis from extrapulmonary cancer : the majority were primary lung cancers ( 24 adenocarcinomas , 16 bac , 14 aah , 4 focal brosis , 1 granuloma )  . 
in our study , we found 5 primary lung cancers and 7 metastatic lesions out of 12 removed ssn , 3 of which discussione il management dei nss presenta diverse problematiche a oggi ancora irrisolte . 
 nota limportanza di un follow - up hrct a breve termine per documentare la persistenza delle lesioni [ 11 ] , in quanto noduli transitori possono sparire entro 36 mesi , ma non ancora chiaro per quanto tempo debba essere prolungato il follow - up in caso di lesioni persistenti che non si modicano ( stabili morfo - dimensionalmente dopo i primi controlli )  . 
ci dimostra come la stabilit di una lesione pggo , anche per un periodo di tempo prolungato , non deponga necessariamente per la sua benignit . nelle loro linee guida provvisorie [ 14 ] , godoy e naidich suggeriscono un follow - up di almeno 3 anni per le lesioni 1278 radiol med ( 2013 ) 118 : 12691280 table 2 histological characteristics of 12 subsolid nodules excised during follow - up . 
five nodules were found to be primary lung cancer and seven were metastatic lesions primary lung cancer metastasis 3 adenocarcinoma 2 adenocarcinoma in situ ( bac ) 2 pulmonary adenocarcinoma 1 pulmonary squamous cell carcinoma 4 bladder carcinoma bac , bronchioloalveolar carcinoma tabella 2 caratteristiche istologiche dei 12 noduli subsolidi asportati durante il follow - up . 
cinque noduli sono risultati tumori polmonari primitivi e 7 lesioni metastatiche tumore polmonare primitivo metastasi 3 adenocarcinoma 2 adenocarcinoma in situ ( bac ) 2 adenocarcinoma polmonare 1 carcinoma a cellule squamose 4 carcinoma vescicale bac , carcinoma bronchiolo - alveolare related to a primary lung cancer , and 4 metastasis from bladder cancer ( in two different patients )  . the oncological diseases , most commonly associated with ssn growth in size and / or in density were lung cancer ( 34% ) and , among the extrathoracic diseases , breast ( 15% ) , colon ( 15% ) and bladder cancer ( 10% )  . the observation of a sample of cancer patients has shown how the characteristics that guide toward malignancy of a lesion are similar to those observed in non - cancer patients [ 14 , 16 , 17 ]  . 
the tendency of irregular pggos to change during the follow - up did not reach statistical signicance ( p = 0.055 ) , probably because of the low number of this type of nodules in our series . the disappearance of two nodules after more than 6 months of stability allows for important considerations , because no similar case has been reported in literature to our knowledge . 
this nding suggests that , although the persistence of a pggo may raise a suspicion of malignancy , this is not always the case , and also some benign lesions may persist for a long time and then disappear . older patients and those with a smoking history have an increased risk of pggo growth ( increased risk : 1.04% for each year ; 2.4% in current smokers and 1.7% in former smokers )  . we also observed that the majority of pggo changed after 2 years of stability ( 41.5% ) , but in a high percentage of pggo tra i 5 e i 10 mm di diametro , mentre le mggo , a prescindere dalle dimensioni , dovrebbero essere asportate poich altamente probabile la loro natura maligna . solo pochi studi si sono occupati del signicato clinico dei nss nei pazienti oncologici . 
 [ 15 ] in uno studio su 34 pazienti con tumori extrapolmonari , riportano che i nss tendono ad avere un alto tasso di malignit , ma nessuna delle 59 lesioni analizzate risultata essere una metastasi da tumore extrapolmonare : nella maggior parte dei casi si trattava di nuovi primitivi polmonari ( 24 adenocarcinomi , 16 bac , 14 aah , 4 brosi focale , 1 granuloma )  . 
nel nostro studio , su 12 nss asportati abbiamo riscontrato 5 tumori polmonari primitivi e 7 lesioni metastatiche , delle quali 3 riferibili a un primitivo polmonare e 4 metastasi da tumore vescicale ( in 2 distinti pazienti )  . le patologie oncologiche pi frequentemente associate a crescita dimensionale e / o densitometica dei nss sono risultate i tumori del polmone ( 34% ) e , tra le patologie extratoraciche , i tumori della mammella ( 15% ) , del colon ( 15% ) e della vescica ( 10% )  . losservazione di un campione di pazienti oncologici ha dimostrato come le caratteristiche che orientano verso la malignit di una lesione siano simili a quelle riscontrate nei pazienti non oncologici [ 14 , 16 , 17 ]  . 
in particolare abbiamo osservato che : la presenza di una componente solida depone per la malignit della lesione , i noduli pggo rotondeggianti e di piccole dimensioni ( < 5 mm ) sono tendenzialmente stabili ( p = 0 , 007 ) e i pggo di dimensioni 10 mm hanno unalta probabilit di modicarsi nel tempo ( p < 0 , 001 )  . 
la tendenza dei pggo irregolari a modicarsi durante il follow - up non risultata statisticamente signicativa ( p = 0 , 055 ) , probabilmente a causa del basso numero di noduli con tali caratteristiche . la scomparsa di due noduli dopo pi di 6 mesi di documentata stabilit consente di fare importanti considerazioni , poich non stato descritto in letteratura nessun altro caso a nostra conoscenza . 
questo riscontro suggerisce che , nonostante la persistenza di un nodulo pggo ponga il sospetto di malignit della lesione , ci non sia sempre vero e che anche alcune lesioni benigne possano persistere a lungo nel tempo per poi scomparire . nei pazienti pi anziani e con storia di fumo , il rischio di crescita dei noduli pggo risultato pi elevato ( rischio aggiuntivo : 1 , 04% per anno di et ; 2 , 4% nei fumatori e 1 , 7% negli ex fumatori )  . 
 abbiamo osservato inoltre come la maggioranza dei pggo si sia modicata dopo 2 anni di stabilit ( 41 , 5% ) , ma in unalta percentuale di casi ( 39% ) la crescita delle lesioni stata osservata anche oltre i 3 anni . 
confermiamo pertanto limportanza di un follow - up prolungato oltre i 3 anni anradiol med ( 2013 ) 118 : 12691280 1279 cases ( 39% ) lesion growth was observed even after 3 years . 
 mggos , by contrast , showed a signicantly faster ( mean , 15 months ) growth in size and / or in density . therefore , we conrm the importance of a prolonged follow - up over 3 years in patients with cancer and suggest the comparison , where possible , with the oldest available hrct images , in order to early detect even most subtle changes in ssn size and densitometry . the limits of our study are evident : the retrospective design implies that follow - up duration is highly variable from patient to patient ; in addition , it cannot be excluded that the treatments carried out might have led to an alteration of the natural history of some nodules . 
despite the availability of histological reports for the majority of mggos , none of the persisting pggos were removed , so we were only able to evaluate the hrct changes , without knowing the real histology . 
finally , since patients were identied retrospectively through a keyword search of our hospitals electronic archive of radiological reports , there is a possibility that some unreported ssn were excluded from the study . che nei pazienti oncologici e consigliamo il confronto , ove possibile , con le pi vecchie immagini hrct disponibili , in modo da poter riconoscere precocemente anche le variazioni dimensionali e / o densitometriche meno evidenti . i limiti di questo studio sono evidenti : lanalisi retrospettiva comporta una durata di follow - up molto variabile da paziente a paziente ; inoltre non possibile escludere che terapie effettuate possano aver determinato unalterazione della storia naturale di alcuni noduli . nonostante siano disponibili i referti istologici della maggior parte dei noduli mggo , nessuna delle lesioni pggo stata asportata e quindi stato possibile valutarne solamente le modiche hrct , senza conoscerne la reale istologia . inne , la ricerca dei pazienti stata effettuata in maniera retrospettiva sullarchivio dei referti radiologici del nostro istituto , utilizzando un sistema di ricerca computerizzato per parola - chiave , perci vi la possibilit che alcuni nss non segnalati siano stati esclusi dallo studio . conclusioni conclusions this study analysed a group of cancer patients with ssn in a non - screening clinical context . 
during follow - up , the majority of ssn remained stable ( 58% ) ; a small percentage disappeared ( 10% ) , while one third ( 32% ) increased in size and / or density , especially those that were partly solid ( mggo ) , large , and irregular . 
growth was more frequent in the elderly and smokers , and may occur even after a long period of stability ( 39% of pggos changed over 3 years )  . 
as a consequence , a follow - up period longer than 3 years is warranted even in cancer patients . questo studio ha analizzato un gruppo di pazienti oncologici con nss non sottoposti a screening tumorale . 
durante il follow - up la maggioranza dei nss rimasta stabile ( 58% ) ; una piccola percentuale scomparsa ( 10% ) , mentre in circa un terzo dei casi ( 32% ) si vericato un aumento di dimensioni e / o densit , specialmente in caso di noduli parzialmente solidi ( mggo ) , di grandi dimensioni e irregolari . 
la crescita stata pi frequente in soggetti di et avanzata e con storia di fumo e si vericata anche dopo un lungo periodo di stabilit ( 39% di pggo modicati oltre i 3 anni )  . 
tra i 12 nss asportati , abbiamo riscontrato 5 tumori polmonari primitivi e 7 lesioni metastatiche ; le patologie oncologiche pi frequentemente associate a crescita dei nss sono risultate in primis i tumori del polmone e , tra le patologie extratoraciche , i tumori della mammella , del colon e della vescica . 
knauth springer heidelberg , dordrecht , london , new york , 2012 issn : 0942 - 5373 isbn : 978 - 3 - 642 - 02483 - 2 e - isbn : 978 - 3 - 642 - 02484 - 9 published online : 16 march 2013 springer - verlag 2013 reading the introduction of this 491 - page book one will nd the following lemma : systemic vasculitis encompasses a wide spectrum of inammatory disorders involving blood vessels of varying size . the aim of the editors and their large cohort of contributors from africa ( many from tunisia ) , asia , europe and north america was to fully unravel and highlight the clinical and imaging ndings of these world - wide spread diseases affecting arteries and veins , large or small vessels and capillaries . in recent years , research has been more and more focused on the study of the biological , anatomo - pathological causes of these mysterious diseases : their origin , what primary trigger is involved with the possible , different and uncertain causes ( smoking ? drugs ? infection ? environmental or individual habits ? )  . progress in research has run along with advances in imaging modalities such as us , mdct , mri , dwi and pet ( which is able to detect early inammation and monitor and follow - up disease activity in treatment )  . 
all of the above coupled with possible and various therapeutic options are well described in the layout of the various chapters . the book is divided into seven parts plus one section of auto evaluation . 
part i is devoted to chapters introducing vasculitis historical medical background , classications , anatomy and histopathology , immunology , medical imaging and evaluation of carotid atherosclerosis and inammation by enhanced ultrasound . 
part iii deals with vasculitis involving predominantly medium size vessels : polyarteritis nel leggere lintroduzione a questo volume di 491 pagine , si trover il seguente lemma : .le vasculiti sistemiche comprendono un vasto spettro di processi inammatori che interessano vasi del sangue dalle differenti dimensioni . 
 scopo dei curatori del volume e del loro esteso gruppo di collaboratori , provenienti da africa ( molti dalla tunisia ) , asia , europa e nord - america , stato quello di analizzare nel dettaglio e mettere in evidenza i quadri clinici e per immagini di queste malattie a diffusione mondiale e che interessano arterie e vene , vasi di grandi e piccole dimensioni ed i capillari . nel corso degli ultimi anni le ricerche si sono sempre pi focalizzate sullo studio delle cause biologiche ed anatomopatologiche di queste malattie misteriose : sulla loro origine , su quale ne sia il meccanismo primitivo scatenante con possibili , differenti ed incerte cause ( il fumo ? droghe ? infezioni ? cause ambientali od abitudini individuali ? )  . 
 i progressi della ricerca sono proceduti in parallelo con quelli delle metodiche dindagine , ultrasuoni ( us ) , mdct , mri , dwi e pet ( questultima in grado di rilevare i primi segni dellinammazione e poi monitorare nel tempo lo stato di attivit della malattia in corso di terapia )  . 
la parte i dedicata a capitoli che introducono i dati storici medici sulla vasculite ( classicazioni , anatomia ed istopatologia , immunologia , studio per immagini ) e sulla valutazione dellaterosclerosi ed inammazione dellaorta mediante ecograa con mezzo di contrasto . 
la parte ii tratta le vasculiti che interessano principalmente i grandi vasi : arterite a cellule giganti , malattia di takayasu , sindrome di cogan , malattia di behet e periaortite cronica . 
la parte iii tratta le vasculiti che interesradiol med ( 2013 ) 118 : 14261427 1427 nodosa , thromboangiitis obliterans or buergers disease , kawasaki disease , central nervous system angiitis , inammatory veno - occlusive disease . 
part iv deals with vasculitis involving predominantly small vessels : granulomatosis with polyangiitis ( wegeners ) , henoch - schnlein purpura , churg - strauss syndrome , goodpastures disease , microscopic polyangiitis . 
part vii deals with vasculitis by organ system : nervous system , cardiovascular , respiratory tract , digestive system , renal vasculitis , oto - rhino - laryngologic system , ophthalmic , musculoskeletal vasculitis . 
 this is a book which is to be recommended to clinicians , surgeons ( general and vascular ) , paediatricians and neurologists who will benet from the endless source of information and discussions found in the text . 
 sano principalmente i vasi di medie dimensioni : poliarterite nodosa , tromboangioite obliterante o malattia di buerger , malattia di kawasaki , angiite del sistema nervoso centrale e la malattia inammatoria veno - occlusiva . 
la parte iv tratta le vasculiti che interessano principalmente i vasi di piccole dimensioni : granulomatosi associata a poliangiite ( wegener ) , purpura di henoch - schnlein , sindrome di churgstrauss , malattia di goodpasture , poliangiite microscopica . 
 la parte vii tratta le vasculiti per sistema di organo : del sistema nervoso , cardiovascolare , respiratorio , digerente , vasculiti renali , del sistema oto - rino - laringologico , oftalmico e muscolo - scheletrico . le malattie di takayasu e kawasaki , come la purpura di henoch - schnlein , sono trattate in extenso sia nella parte dedicata agli adulti che in quella pediatrica del volume . 
ogni capitolo corredato da una bibliograa molto corposa . le caratteristiche delle singole malattie sono illustrate da immagini molto precise e ben riprodotte ( mancanti talora di quelle frecce , che dovrebbero invece essere riprodotte secondo quanto scritto nelle didascalie delle immagini )  . 
we are thus indebted to the following experts who reviewed papers which completed the peer - reviewing process within 2013 . la qualit scientica della rivista la radiologia medica dipende dalla collaborazione qualicata e puntuale di esperti riconosciuti che hanno dedicato il loro tempo alla revisione scientica degli articoli inviati per la pubblicazione . 
knauth springer - verlag berlin heidelberg , 2012 issn : 0942 - 5373 isbn : 0978 - 3 - 642 - 12455 - 6 e - isbn : 978 - 3 - 642 - 12456 - 3 published online : 16 march 2013 springer - verlag 2013 the aim of this 352 page book was to review , study and present in their variety all disease types and pathologic conditions affecting the scrotuaccordingly , this is a truly comprehensive book , presenting the results of long - standing cooperation between radiologists , urologists and paediatric surgeons working in the eld from italy and around the world . 
 the patients clinical history is emphasized and physical examination of the scrotum is the rst diagnostic step , followed by ultrasound ( us ) and sometimes magnetic resonance imaging ( mri ) , rarely by nuclear medicine and contrast - enhanced us studies . 
clinical presentation followed by imaging , management and end - results is quite useful and gives the reader a comprehensive , exhaustive and precise spectrum of the presented and discussed topic , illustrated by very beautiful images . the editors of this book should be praised not only for the book as a whole but for the very precise and useful abbreviation list to be found at the beginning of the book and the comprehensive index at its end . scopo di questo volume di 352 pagine stato quello di rivedere , studiare e presentare in tutte le sue variet ogni possibile tipo di malattia ed affezione patologica dello scroto . 
 ne deriva , come conseguenza , un testo veramente completo che presenta i risultati di lungo e fruttuoso lavoro di cooperazione tra radiologi , urologi e chirurghi pediatri che si occupano del problema in italia e nel mondo . grande enfasi posta sulla storia clinica del paziente e sullesame sico dello scroto , quali primi passi nelliter diagnostico , seguiti dallecograa , talvolta dalla risonanza magnetica ( rm ) e raramente dalla medicina nucleare e dallecograa con contrasto . 
 dopo i capitoli di apertura in cui sono trattate la strumentazione ecograca e di rm e lanatomia dello scroto , il lettore ne trover altri 29 dedicati sia alla precisa valutazione clinica delle malattie dello scroto delladulto e del bambino , quali trauma , dolore scrotale acuto , tumefazioni scrotali tumori , cisti , infertilit maschile in tutte le sue possibili varianti ( presentazione molto precisa ed approfondita , interessante pi landrologo che il radiologo ) , testicolo ritenuto , reperti occasionali calcicazioni e quadri miscellanei , che al loro quadro per immagini ed al trattamento e conseguente risultato , tutti descritti in grande dettaglio . i capitoli sono impostati in modo tale che la presentazione clinica ( seguita da immagini , trattamento e risultato nale ) risulta assai utile , dando al lettore un quadro esauriente , completo e preciso dellargomento trattato , illustrato anche da immagini molto belle . i curatori del volume devono essere lodati non solo per il volume nel suo complesso , ma anche per lassai preciso ed utile iniziale elenco delle abbreviazioni e per laccurato indice nale . radiol med ( 2013 ) 118 : 14241425 1425 due to its content , this book should be considered a pace - setter in the eld , giving radiologists , urologists , andrologists , paediatric surgeons and paediatricians a very handy instrument ( a compliment to italian radiology ) in their daily practice in this difcult and consequential eld . dato il suo contenuto , questo volume pu essere considerato di primo piano e fondamentale in questo campo , offrendo a radiologi , urologi , andrologi , chirurghi pediatri e pediatri uno strumento assai utile ( un omaggio alla radiologia italiana ! ) nella loro pratica quotiana in questo campo difcile ed importante . 
nel 42% dei pazienti reclutati non si potuta utilizzare labi ( nel 9 , 34% non era rilevabile un polso arterioso e nel 14 , 02% larteria non era comprimibile ) oppure si rivelato inesatto ( nel 18 , 7% prima e nel 15 , 9% dopo la realizzazione della pta )  . 
labi mostra limiti significativi nella diagnosi e nel trattamento dei pazienti con cli rispetto alla tcpo2 . 1374 radiol med ( 2013 ) 118 : 13731378 keywords peripheral transluminal angioplasty peripheral arterial occlusive disease transcutaneous oxygen pressure revascularization reperfusion parole chiave angioplastica translumninale periferica malattia occlusiva eriferica arteriosa tensione transcutanea di ossigeno rivascolarizzazione riperfusione introduction critical limb ischaemia ( cli ) is commonly defined as the presence of chronic ischaemic pain at rest , ulcer or gangrene in the foot that is attributable to objectively proven peripheral arterial occlusive disease ( paod ) [ 1 , 2 ]  . 
however , this index can only be determined in large arteries and not in nonpalpable lowflow arteries ; it is also unsuitable for patients with calcified ( noncompressible ) arteries . 
these handicaps frequently occur in diabetic patients and prevent reliable ankle - pressure measurements [ 47 ]  . studies on microcirculation continue to increase as attempts are made to obtain an imaging diagnosis together with a functional assessment of tissue . 
an increase in tcpo2 in patients following peripheral transluminal angioplasty ( pta ) reflects the physiological significance of microvascular revascularisation achieved in the treated limb and serves to assess functional improvement in tissue oxygenation obtained with pta . 
 the objective of this study was to evaluate the limitations of abi in revascularisation of diabetic patients with cli undergoing pta treatment compared with the degree of arterial stenosis and tcpo2 . materials and methods from 1 july 2008 to 30 november 2011 , 250 consecutive patients with limb ischaemia who were sent to the vascular radiology service for clinical evaluation and diagnostic tests [ arteriography and / or computed tomography angiography ( cta ) and abi ] were examined for suitability for pta . 
all were evaluated for signs of posterior tibial and dorsalis pedis signals ; abi was measured by the doppler continuous - wave technique , and tcpo2 was measured on the dorsum of the foot . 
duplex scanning was performed in cases with reduced or absent foot signal , abi < 0.90 ( in the absence of arterial calcification ) or tcpo2 < 50 mmhg ( in the absence of oedema )  . 
 abi was measured using a 12 - cm sphygmomanometer cuff placed just above the ankle , and a doppler instrument with an 8 mhz frequency ( multi - dopplex ii huntleigh healthcare limited , cardiff , uk ) was used to measure systolic pressure of the posterior tibial and dorsal pedal arteries of each leg . 
these pressures were then normalised with the higher brachial pressure of either arm to determine abi . tcpo2 measurements in the diabetic limb were taken upon hospital admission and reassessed 1 day after pta . 
 tcpo2 measurements were taken on the dorsum of the foot with the patient resting in the supine position in an air - conditioned room maintained at 22c and with the electrode at 44c . 
 statistical analysis statistical analysis compared preand post - treatment results by the equality of means for paired data using paired radiol med ( 2013 ) 118 : 13731378 1375 table 1 demographic and clinical characteristics of study population ( n = 104 )  . 
data are percent or mean1 standard deviation tasc , inter - society consensus for the management of peripheral artery disease ; tcpo2 , transcutaneous oxygen tension tabella 1 caratteristiche demografiche e cliniche della popolazione studiata ( n = 104 )  . 
results were considered significant with a p value < 0.01. results in 181 ( 72.4% ) of the 250 consecutive patients with limb ischaemia admitted to our vascular radiology service , at least one pedal pulse was absent , abi was < 0.90 ( in the absence of arterial calcification ) , tcpo2 was < 50 mmhg and / or duplex scanning showed evidence of significant stenosis . 
these 114 patients were referred for an angiographic or cta study , and in 136 limbs , the presence of a stenotic narrowing > 50% of the vessel lumen in at least one artery of the ischaemic limb was observed . 
abi was not measurable in 25 limbs ( 23.36% , 25 / 107 ) because of the absence of both tibial signals in ten patients ( 9.34% , 10 / 107 ) or the presence of arterial calcifications in 15 ( 14.02% , 15 / 107 )  . 
 after pta , abi was not measurable in 17 patients ( 15.90% , 17 / 107 ) because of the absence of an arterial signal in three ( 2.80% , 3 / 107 ) or the presence of arterial calcifications in 14 ( 13.08% , 14 / 107 )  . 1376 radiol med ( 2013 ) 118 : 13731378 fig . 
2 stenosi nei pazienti con abi > 0 , 91 ( prima e dopo pta ; il numero identifica ciascun paziente , permettendo di monitorare il cambiamento )  . abi could be determined in 82 cases ( 76.63% ) : 20 cases ( 18.7% , 20 / 107 ) displayed a normal abi with serious arterial stenosis or a very low tcpo2 , which justified carrying out pta , the results of which are shown in figures 1 and 2 ( initially , each case was assigned a number to facilitate follow - up on the charts before and after treatment )  . 
 in 42% of patients , abi was erroneous or could not be used : in 23.36% because it was impossible to determine abi ( no signal or the artery could not be compressed ) ; in 18.7% , a false negative was obtained ( a normal abi but with high levels of arterial stenosis and / or a low tcpo2 )  . statistical analysis revealed minimal correlation between techniques ( tcpo2 and abi ) ( r = 0.14 ; p < 0.199 ) , which means that both indices show a relationship conditioned by the patients improvement rather than by any true correspondence between parameters . discussion radiologists use abi to evaluate pta . 
however , even if arterial stenosis is considerably reduced and abi is normal , it is not possible to know whether the blood flow in the treated limb has increased . 
 radiol med ( 2013 ) 118 : 13731378 1377 however , abi can only be determined in large - artery trunks and not in nonpalpable , low - flow arteries ; it is also unsuitable for patients with calcified ( noncompressible ) arteries . 
as shown in our study results , it was impossible to determine abi before pta in 23.36% of patients ( in 9.34% because of the lack of a signal , and in 14.02% because of an arterial calcification )  . 
however , in all these patients , it was possible to measure tcpo2 without difficulty before and after pta . our results show that an abi > 0.9 does not rule out cli , stenosis > 50 % or tcpo2 > 30 mmhg . 
this may be the key reason abi does not always reliably predict the magnitude of the cli [ 10 , 16 , 17 ]  . for this reason , the inter - society consensus for the management of peripheral artery disease ( tasc ) 2000 proposed a range of 3050 mmhg as a level of moderate ischaemia . 
these findings confirm that abi is not related to microcirculation of the treated limb . the study presented here shows that an increase in tcpo2 over pretreatment values in the same patient demonstrates the effectiveness of pta in revascularisation . 
for this reason , we propose the use of tcpo2 as an indicator of reperfusion achieved through pta . a limitation of this study is that none of the three parameters analysed ( abi , tcpo2 or arteriography ) provides a clinical prediction of limb salvage . 
 we are carrying out clinical monitoring to assess which of diagnostic method correlates best with limb salvage . conclusions abi shows significant limitations in diagnosing and treating cli patients compared with tcpo2 . 
the treatment algorithm was neo - adjuvant chemotherapy ( ct ) administered for four cycles , followed by preoperative sc - rt administered 1 week after chemotherapy completion , delivering 20 gy in ve fractions over 1 week . 
lapproccio terapeutico prevedeva un trattamento sistemico neoadiuvante ( 4 cicli ) seguito da radioterapia ipofrazionata short - course per una dose totale di 20 gy in 5 sedute consecutive erogate in una settimana . 
this treatment resulted in favourable lc , os , low rates of toxicity and satisfying qol . keywords rectal cancer preoperative short - course radiation therapy combined chemo - radiation therapy allesame istologico denitivo , una stabilit di malattia stata ottenuta in 24 pazienti ( 36% ) , una riduzione di malattia in 34 pazienti ( 50 , 7% ) e una progressione in solo 9 casi ( 13 , 3% )  . 
nel corso del follow - up sono state evidenziate due recidive loco - regionali ( entrambe in campo di trattamento radioterapico ) con un controllo locale a 5 anni del 97% . 
il trattamento radioterapico ipofrazionato neoadiuvante associato a chemioterapia nei tumori del retto localmente avanzati risulta essere ben tollerato , con ottimi risultati in termini di controllo locale , sopravvivenza globale e qualit di vita dei pazienti . parole chiave tumore del retto radioterapia pre - operatoria ipofrazionata radio - chemioterapia introduction introduzione rectal cancer is the fourth most frequent tumour worldwide , representing about one - third of large bowel malignancies and the third cause of death among men and women [ 1 ]  . 
 management of locally advanced resectable rectal cancer requires a multidisciplinary approach , because , although surgery still plays a fundamental role , the addition of radiation therapy and chemotherapy in a preoperative or adjuvant setting results in signicantly improved local control ( lc ) and overall survival ( os ) compared to surgery alone [ 24 ]  . numerous trials have shown that preoperative radiation therapy ( rt ) can decrease the risk of local relapse up to 5070% . 
 ideally , preoperative rt could also reduce treatment - related toxicity in comparison to adjuvant rt , as reported by several randomised trials that demonstrated lower toxicity and better compliance of rt when administered before rather than after surgery [ 5 , 6 ]  . the most frequent regimens in the preoperative setting of patients with resectable rectal cancer are conventionally fractionated concomitant chemo - radiation therapy ( 4550 gy in 1.82 gy per fraction ) with delayed surgery or shortil tumore del retto la quarta neoplasia per frequenza , rappresentando un terzo circa delle neoplasie del grosso intestino e la terza causa di morte negli uomini e nelle donne . 
il trattamento di queste neoplasie richiede un approccio multidisciplinare : nonostante infatti la chirurgia giochi un ruolo fondamentale , laggiunta di radioterapia e chemioterapia allatto chirurgico migliora signicativamente il controllo locale e la sopravvivenza globale [ 24 ]  . 
 molti studi hanno dimostrato che la radioterapia neoadiuvante pu ridurre il rischio di recidiva locale di malat tia del 5070% , mentre lapproccio adiuvante riduce questo rischio di solo il 3040% . 
alcuni importanti studi randomizzati hanno dimostrato inoltre una riduzione della tossicit correlata al trattamento con la radioterapia neoadiuvante , quando confrontato allapproccio post - operatorio [ 5 , 6 ]  . i pi frequenti approcci neoadiuvanti seguono essenzialmente due schemi : il primo prevede radio - chemioterapia concomitante , in cui la radioterapia eseguita con frazionamento convenzionale a un dose totale di 4550 gy erogata in 2528 frazioni , seguita a distanza di 48 settimane da intervento chirurgico ; il secondo prevede radioterapia iporadiol med ( 2013 ) 118 : 13971411 1399 course irradiation ( 25 gy in ve fractions ) with immediate surgery [ 511 ] , with similar results in terms of long - term survival , local control and late morbidity [ 6 , 912 ]  . the radiation oncology unit conducted a prospective observational trial of neo - adjuvant chemotherapy and shortcourse radiation therapy , followed by immediate surgery for resectable rectal cancer . 
questi due approcci hanno dimostrato risultati sovrapponibili in termini di sopravvivenza , controllo locale e tossicit tardiva [ 6 , 912 ]  . presso la sc di radioterapia oncologica dellazienda ospedaliera di reggio emilia abbiamo condotto uno studio prospettico osservazionale di chemioterapia e radioterapia ipofrazionata neoadiuvante , seguita da chirurgia immediata . 
 questo protocollo differisce dagli altri studi pubblicati in letteratura fondamentalmente per due aspetti : la radioterapia neoadiuvante ipofrazionata short - course combinata con la terapia sistemica e la dose totale di radioterapia modicata rispetto allo standard ( 25 gy in 5 sedute ) , al ne di ridurre potenzialmente la tossicit correlata al trattamento . materials and methods sixty - seven patients were treated with a neo - adjuvant chemotherapy / short - course radiation scheme at the oncological radiotherapy division of the reggio emilia hospital in italy . materiali e metodi study design this is a report of a common practice - derived , protocol driven , prospective treatment schedule of a preoperative shortcourse radiation treatment with the introduction of neoadjuvant chemotherapy . 
the protocol had been approved by the local ethics committee . patient selection eligibility criteria were : histologically proven diagnosis of primary rectal cancer , maximum 10 cm above the dentate line ( upper limit ) , clinical stage t3 or t4 , n0 or n + according to the uicc ( international union against cancer ) classication system , resectable rectal cancer , no evidence of sphincter involvement , no evidence of metastatic disease , no medical contraindications to radiation therapy , chemotherapy or surgery after multidisciplinary evaluation , ecog ( eastern cooperative oncology group ) performance status 2 , age > 18 years and < 80 years , no prior pelvic radiation therapy and written informed consent . exclusion criteria were : previous or concurrent malignancies , locally advanced inoperable disease , presence of metastatic disease or recurrent rectal cancer , concurrent severe medical conditions , stenotic tumour , medical or psychiatric conditions that could interfere with the patients informed consent . sono stati arruolati nel protocollo di studio 67 pazienti affetti da neoplasia del retto localmente avanzata trattati presso la radioterapia oncologia dellospedale di reggio emilia . disegno di studio questo studio un report di un protocollo interno di radioterapia ipofrazionata short - course a intento neoadiuvante associato a terapia sistemica nei tumori del retto . 
il protocollo di trattamento stato approvato dal comitato etico locale . selezione dei pazienti i criteri di eleggibilit del protocollo erano i seguenti : diagnosi istologicamente confermata di neoplasia del retto , sita a una distanza massima di 10 cm dalla linea dentata , in stadio clinico localmente avanzato ( t3 - t4 , n0 - n1 secondo la classicazione uicc international union against cancer ) , operabile , senza interessamento dello sntere e senza evidenza di diffusione sistemica . 
tutti i pazienti dovevano rmare il consenso informato preparato ad hoc . criteri di esclusione : precedente diagnosi di neoplasie maligne in altre sedi , malattia rettale inoperabile , presenza 1400 pretreatment stage evaluation pretreatment staging of the patients required digital rectal examination , laboratory studies , colonoscopy and computed tomography ( ct ) of the pelvis - abdomen - chest and endorectal ultrasound . valutazione pre - trattamento radiol med ( 2013 ) 118 : 13971411 di diffusione sistemica di malattia , gravi comorbilit , tumori stenosanti il lume rettale , altre condizioni mediche o clinico - psichiatriche che avrebbero potuto interferire con il consenso informato dei pazienti . preoperative therapy preoperative therapy was planned as follows : neo - adjuvant chemotherapy according to the de gramont scheme until 2003 and subsequently folfox 6 scheme ( oxaliplatin 100 mg / m2 and folinic acid 400 mg / m2 on day 1 followed by a 5 - fu bolus 400 mg / m2 and a 46 - hour infusion of 3000 mg / m2 every 2 weeks ) ; subsequent short - course rt consisting of 20 gy delivered in ve fractions , over 1 week , prescribed at the isocenter of the plan according to the international commission on radiation units and measurements ( icru ) report . 
the planning target volume ( ptv ) was dened as the ctv with a margin of 2 corgans at risk routinely considered in these patients were the bladder , femoral heads and bowels ( large and small bowel excluding ptv )  . three - dimensional rt was performed in all patients , according to the institutional practice , with each patient in the prone position with full bladder in order to displace the small bowel anteriorly and superiorly . la valutazione pre - trattamento dei pazienti comprendeva lesplorazione rettale digitoguidata , gli esami laboratoristici , la colonscopia , la tomograa assiale computerizzata del torace - addome - pelvi e leco - endoscopia . terapia neoadiuvante lapproccio neoadiuvante era cos pianicato : chemioterapia neoadiuvante secondo schema de gramont no 2003 ; successivamente folfox 6 ; successiva radioterapia ipofrazionata short - course ( dose totale 20 gy in 5 sedute giornaliere )  . 
la vescica , le teste femorali e lintestino venivano considerati organi a rischio . tutti i pazienti venivano sottoposti a radioterapia 3d conformazionale , in accordo con la nostra pratica clinica , in posizione prona e riempimento vescicale in modo da dislocare le anse intestinali anteriormente e superiormente al campo di irradiazione . surgery and pathological evaluation chirurgia according to the protocol , surgery was performed within seven days after rt completion ; although total mesorectal excision ( tme ) was the preferred surgical technique , it was not mandatory . 
the decision to perform a low anterior resection ( ar ) vs an abdomino - perineal resection ( apr ) depended on the distance of the lesion ( measured before preoperative chemo - radiation ) from the anal verge . 
 la valutazione isto - patologica seguiva le procedure standard , includendo la classicazione uicc e tnm , il numero di linfonodi reperiti ed il numero di linfonodi patologici , cos come lo stato dei margini . adjuvant chemotherapy follow - up chemioterapia adiuvante adjuvant chemotherapy consisting of six cycles of folfox was recommended after surgery for 6 months for patients with pathological stage t4 or n + disease . il trattamento sistemico adiuvante veniva indicato nei pazienti in stadio patologico t4 o n + e consisteva in 6 cicli di folfox ( de gramont prima del 2003 )  . radiol med ( 2013 ) 118 : 13971411 1401 follow - up follow - up all patients were followed - up at 6 - month intervals for 3 years and then once yearly . 
colonoscopy was performed every 6 months for the rst 2 years after surgery . outcome measures and denition of study end - points tutti i pazienti , dopo il trattamento combinato , venivano seguiti a intervalli semestrali per i primi 3 anni e successivamente annualmente . 
the secondary outcome measures were overall survival ( os ) , disease - free survival ( dfs ) , acute and late toxicity , and quality of life . early skin , small / large bowel and bladder toxicity was recorded according to the radiation therapy oncology group ( rtog ) common toxicity criteria . 
toxicity was dened as late if it occurred more than 3 months after radiation therapy , and was recorded according to the rtog scale . the assessment of complications was detailed and included intraoperative complications , general postoperative complications , specic postoperative complications ( bleeding requiring intervention , anastomotic leakage , ileus , abdominal and pelvic abscesses , peritonitis , stula , colostomy complications )  . 
the remaining six items are intended to be mono - item scales describing relevant canceroriented symptoms ( dyspnoea , insomnia , appetite , constipation , diarrhoea , nancial difculties )  . 
it is composed of four functional scales ( body image , sexual functioning , sexual enjoyment , and future perspective ) and various symptom scales ( urinary problems , chemotherapy side effects , gastrointestinal symptoms , sexual problems , defecation problems and weight loss )  . 
 gli endpoint secondari erano rappresentati dalla sopravvivenza globale , dalla sopravvivenza libera da malattia , dalla tossicit acuta e tardiva e dalla qualit di vita dei pazienti . la tossicit acuta e tardiva cutanea , intestinale e urinaria veniva registrata utilizzando le scale di tossicit dellrtog ( radiation therapy oncology group )  . 
la tossicit era denita tardiva se compariva pi di 3 mesi dopo la terapia radiante ed era registrata secondo la scala rtog . tutte le complicazioni intrae peri - operatorie sono state registrate , cos come le complicanze post - operatorie . 
un alto valore del punteggio delle diverse scale rappresenta un buono stato di salute , mentre un alto valore nel punteggio delle scale dei sintomi rappresenta un cattivo stato di salute . 
 questo strumento composto da 4 scale funzionali ( immagine corporea , funzionalit e soddisfazione sessuale , aspettative future ) e varie scale di sintomi ( problemi urinari , effetti collaterali della chemioterapia , sintomi gastroenterici , disturbi della sfera sessuale , alterazione dellalvo e perdita di peso )  . la scala fiql composta da 29 domande che costituiscono 4 scale diverse ; stile di vita ( 10 domande ) , comportamento ( 9 domande ) , depressione e percezione di se stesso ( 7 domande ) e imbarazzo ( 3 domande )  . 1402 radiol med ( 2013 ) 118 : 13971411 items form four scales : lifestyle ( 10 items ) , coping / behavior ( 9 items ) , depression / self - perception ( 7 items ) , and embarrassment ( 3 items )  . iief was a self - administered questionnaire assessing erectile function ( ef ) , orgasmic function ( of ) , sexual desire ( sd ) , intercourse satisfaction ( is ) and overall satisfaction ( os )  . statistical analysis all survival analyses were calculated according to the kaplan - meier method . 
the main patients and tumour characteristics are summarised in table 1 . all patients underwent chemo - radiation therapy ( the rst 28 with de gramont chemotherapy schema and the subsequent 39 patients with folfox ) and subsequent surgery without any major protocol violation . 
grade i and ii gastrointestinal ( diarrhoea ) acute toxicity was shown in one and six patients , respectively . all patients underwent surgery performed within seven days after rt completion according to our protocol . 
no pathological complete response was detected . complete local resection of the rectal cancer was achieved in 100% of cases , with mean distance of the tumour from the surgical margins of 44 mm ( range 7120 mm ) ( table 2 )  . 
 in ultimo , liief un questionario auto - somministrato che esplora diverse aree della sfera sessuale ( funzionalit erettile , funzionalit orgasmica , soddisfazione intercorrente e generale )  . analisi statistica tutte le analisi di sopravvivenza sono state calcolate utilizzando il metodo kaplan - meier . 
le variabili analizzate sono : sesso , et , stadio clinico e patologico , tipo di chirurgia , presenza di stenosi alla diagnosi e la distanza tra la malattia e sntere anale . 
le caratteristiche cliniche e patologiche dei pazienti sono riassunte in tabella 1 . tutti i pazienti sono stati sottoposti a trattamento combinato radio - chemioterapico ( i primi 28 pazienti con schema de gramont e i successivi 39 con folfox 6 ) e successiva chirurgia . 
una tossicit acuta genitourinaria stata riportata di grado 1 in due pazienti e di grado 2 da 4 pazienti , mentre tossicit acuta gastroenterica di grado 1 e 2 si manifestata , in forma di diarrea , in sette pazienti . tutti i pazienti sono stati sottoposti a intervento chirurgico entro sette giorni dalla ne della radioterapia . 
lanalisi isto - patologica del pezzo operatorio ha dimostrato che il 28 , 4% dei pazienti era in stadio i , il 35 , 7% in stadio ii e il 35 , 9% in stadio iii . 
una netta riduzione della malattia si evidenziata in 34 pazienti ( 50 , 7% ) , una stabilit in 24 pazienti ( 36% ) e una progressione di malattia in 9 casi ( 13 , 3% )  . 
la resezione della neoplasia stata completa in tutti i pazienti , con una distanza media del tumore dai margini chirurgici di 44 mm ( range 7120 mm ) ( tabella 2 )  . non stata osservata mortalit peri - operatoria . 
re - operation due to postoperative complications was required in only one patient for anastomotic stenosis 15 months after surgery . adjuvant chemotherapy was administered in 21 patients following the protocol design . 
 at the last follow - up a total of two locoregional recurrences , both within the rt volume , were observed , resulting in a 5 - year lc of 97% . 
 the rst patient , with presacral recurrence , was treated with multi - agent chemotherapy and was alive at last follow - up . a total of 11 systemic relapses were observed resulting in a 5 - year actuarial dfs rate of 84% , with mean time to systemic progression of 24 months . 
twenty - two patients died during the follow - up because of rectal cancer progression ( n = 8 ) , intercurrent disease ( n = 9 ) and unknown causes ( n = 5 )  . the 5 - year os rate was 67% . 
no death because of late toxicity was observed . at the time the qol questionnaires were sent out , 18 patients had died and two were still alive with local recurrences . 
gastrointestinal symptoms including nausea / vomiting , constipation and / or appetite loss were reported to be very rare , while diarrhoea was frequently reported in the plicazioni post - operatorie precoci di grado lieve - moderato sono state riportate nel 24% dei casi . 
complicazioni tardive sono state riportate invece in 5 pazienti ( 7% ) , ma solo un paziente ha richiesto un successivo intervento chirurgico per stenosi dellanastomosi 15 mesi dopo il primo intervento chirurgico . il trattamento sistemico adiuvante stato eseguito in soli 21 pazienti . il follow - up mediano dei pazienti viventi di 114 mesi con un range di 40178 mesi . 
il primo paziente che ha evidenziato recidiva di malattia , ha manifestato dopo circa 14 mesi dallintervento chirurgico una recidiva in regione pre - sacrale , e sottoposto a chemioterapia di i linea risulta ancora vivo allultimo follow - up . 
un secondo paziente invece ha sviluppato una ripresa linfonodale di malattia circa 48 mesi dopo il trattamento ed deceduto dopo 18 mesi per progressione sistemica di malattia . allultimo follow - up sono state riportate 11 recidive sistemiche con una sopravvivenza libera da malattia dell84% e un tempo medio alla progressione sistemica di 24 mesi . 
 solo 48 pazienti , di cui 39 operati conservativamente e 12 con amputazione addomino - perineale , hanno compilato i questionari relativi alla qualit di vita , con un tempo medio trascorso dalla ne della radioterapia e la compilazione dei questionari di 84 mesi ( range 48156 )  . 
i pazienti sottoposti a chirurgia conservativa hanno riportato risultati migliori in termini di qualit di vita globale ( 75 vs 60 ) , cos come gli aspetti pi prettamente funzionali . 
sintomi gastroenterici ( nausea , vomito , costipazione , inappetenza ) sono risultati essere eventi rari in entrambi i gruppi di pazienti , mentre la diarrea stata riportata pi frequentemente nei pazienti sottoposti a chirurgia conservativa . 
 treatment of locally advanced resectable rectal cancer has slowly changed over the last few years , with increased localregional tumour control during the past 1015 years , mainly due to the introduction of total mesorectal excision ( tme )  . 
 unfortunately , local relapse after this surgical procedure alone for locally advanced resectable rectal cancer still ranges between 15% and 21% in randomised trials [ 15 , 16 ]  . 
it is differenza tra i due gruppi di pazienti in termini di qualit di vita esplorata con gli specici questionari risultata statisticamente signicativa ( p < 0 , 001 )  . il questionario specico per lincontinenza fecale ( fecal incontinence quality of life scale fiql ) stato somministrato solo ai pazienti sottoposti a chirurgia con preservazione dello sntere anale . 
 in ultimo , il tasso di disfunzione erettile risultata maggiore nei pazienti sottoposti ad amputazione addominoperineale rispetto a quelli trattati con chirurgia conservati ( 47% vs 75% )  . discussione questo studio prospettico osservazionale riporta i risultati di un approccio neoadiuvante combinato chemioterapico e radioterapico ( schema ipofrazionato short - course ) seguito da chirurgia immediata nelle neoplasie localmente avanzate del retto . il trattamento di tali neoplasie ha subito notevoli cambiamenti negli ultimi anni , con un netto incremento del controllo loco - regionale evidenziato negli ultimi 1015 anni , principalmente dovuto allintroduzione della tme . 
risulta chiaro , quindi , che le neoplasie localmente avanzate del retto necessitano di un approccio multimodale , con un trattamento radioterapico 1406 radiol med ( 2013 ) 118 : 13971411 clear , therefore , that patients with locally advanced resectable rectal cancer need a combined treatment , with radiation therapy associated with surgical procedure in a preoperative or postoperative setting . 
the positive impact of preoperative rt in terms of local control and overall survival was demonstrated by seven european phase iii trials [ 6 , 1520 ] and by a metanalysis [ 21 ]  . when rt is considered an option in a setting of preoperative rectal cancer treatment , two major approaches exist : either a short course approach or long term radiation therapy , the latter sometimes combined with chemotherapy [ 17 , 18 ] ; today the question which preoperative treatment is best is still open . 
data supporting short - course preoperative rt were shown in the swedish rectal cancer trial and in the dutch colorectal cancer group trial ( ckvo 9504 ) , both showing lower rates of local recurrence after preoperative radiotherapy compared with surgery alone ( 11% vs 27% and 6% vs 12% , respectively )  . 
the swedish trial showed also a signicant improvement of 5 - year survival rates with preoperative short - course rt . although no trial has yet provided the nal answer , several studies have highlighted some of the advantages and disadvantages of long - term preoperative ct - rt and short course rt . 
 [ 19 , 22 ] showed no difference in terms of sphincter preservation rate and no major clinically relevant difference between short - course preoperative rt and long - course concomitant radio - chemotherapy followed by delayed surgery . 
 the only difference showed in this trial , as in several other studies , was in the rate of tumour downsizing , which was found to be higher with long - course chemo - radiation [ 6 ]  . 
 the recent review [ 23 ] of major published studies of shortcourse preoperative radiation and the more conventional approach of long - course neo - adjuvant chemo - radiation showed that although long - course preoperative chemo - radiation is associated with higher rates of reversible acute toxicity , it appears to be more a signicant and higher rate of late gastrointestinal toxicity observed in short - course preoperative radiation studies . a recent metanalysis [ 24 ] compared preoperative shortcourse radiotherapy with neo - adjuvant conventional chemoradiotherapy . 
no differences between chemo - radiotherapy and short - course rt were found in terms of survival , local recurrence , mortality , resectability , and rate of sphincter preservation . 
this may be related to the interval between radiotherapy and surgery that is too short in preoperative short - course rt protocols , preventing the regression detectable after a longer interval time [ 25 ]  . 
in fact , when delaying surgery to 68 weeks after shortcourse rt , the pathologic complete response and r0 resection rate were similar to those observed after preoperative associato alla chirurgia sia in setting neoadiuvante che post - operatorio . 
alcuni studi hanno evidenziato un vantaggio dellapproccio neoadiuvante rispetto alla radioterapia post - operatoria [ 6 , 13 ] soprattutto in termini di controllo locale e sopravvivenza globale , come dimostrato da sette studi di fase iii europei [ 6 , 1520 ] e da una recente metanalisi [ 21 ]  . quando parliamo di radioterapia neoadiuvante , si aprono fondamentalmente due scenari : il primo consiste in un trattamento radio - chemioterapico concomitante [ 17 , 18 ] in cui la radioterapia viene erogata con frazionamento convenzionale a una dose totale di 45 - 50 gy ; il secondo invece in una radioterapia esclusiva con schema ipofrazionato . 
la sola differenza evidenziata in questo e in altri studi , la percentuale di downsizing del tumore , che risulta nettamente maggiore nei pazienti sottoposti a radio - chemioterapia concomitante long - course [ 6 ]  . 
 una recente revisione [ 23 ] evidenzia che nonostante lapproccio concomitante sia associato a un tasso maggiore di tossicit acuta , sembra che la radioterapia ipofrazionata sia associata a un rischio maggiore di tossicit tardiva . 
 una metanalisi [ 24 ] pubblicata recentemente ha confrontato i due approcci neoadiuvanti e non ha evidenziato differenze in termini di controllo locale di malattia , sopravvivenza globale , mortalit , tasso di resecabilit e tasso di preservazione snteriale . 
di contro , questa metanalisi ha confermato il pi alto tasso di downsizing nei pazienti sottoposti a radio - chemioterapia long - course rispetto alla sola radioterapia short - course . 
questo dato potrebbe essere attribuito allintervallo temporale intercorrente tra la radioterapia e la chirurgia che risulta molto breve nei protocolli di radioterapia short - course , tanto da non rendere evidente la regressione tumorale evidenziabile con un pi lungo intervallo temporale [ 25 ]  . 
infatti , quando la chirurgia viene posticipata a 68 settimane dal termine della radioterapia short - course , il tasso di risposte patologiche complete e di resezione chirurgica completa sembra essere sovrapponibile a quelle osservate dopo trattamento radio - chemioterapico concomitante long - course , come dimostrato recentemente da radu et al . 
alla luce di questi dati , resta il dilemma , sottolineato dalleditoriale di pahlmanns [ 27 ] , di come interpretare leffetto di downsizing in vivo se la chirurgia pianicata corrisponde a quella eseguita . 
 [ 28 ] , in una recente revisione della letteratura , concludono che la scelta tra tipo di frazionamento ottimale di radioterapia , il timing della chirurgia e luso radiol med ( 2013 ) 118 : 13971411 1407 chemo - radiotherapy , as shown by radu et al . 
however , the dilemma is , as underlined by pahlmanns editorial [ 27 ] , how to interpret the downsizing effect in vivo , if the planned surgery corresponds to the performed one . 
 [ 28 ] in a recent review conrm that the optimal fractionation of rt , timing of surgery , and the best use of concomitant ct remain controversial . building on the success of chemotherapy in colorectal cancer , a potentially complementary approach to primary rt involves the use of chemotherapy and surgery to avoid rt . 
 [ 29 ] analysed 26 patients with t3 or t4 and n0 - 2 nonmetastatic resectable rectal cancer , treated with neo - adjuvant chemotherapy ( two cycles of irinotecan , 5 - fu and lv ) showing a 5 - year relapse - free and overall survival rates of 74% and 84% , respectively . 
 [ 30 ] used preoperative uorouracil , leucovorin , and oxaliplatin plus bevacizumab with no rt in carefully selected patients , with a surprising 23% pcr rate achieved with the chemotherapy regimen and excellent local control ( again with relatively short follow - up in selected group of patients )  . 
the new us alliance cooperative group ( previously cancer and leukemia group b , american college of surgeons oncology group , and north central cancer treatment group ) plans to study this approach further ( without use of bevacizumab ) in a multicentre randomised trial . 
the recent review [ 31 ] concluded that there is now enough preliminary evidence to support the view that in less locally advanced patients selected by initial mri , the role of neo - adjuvant chemotherapy alone , without radiation , but the utility of this approach should be explored compared with scprt or crt in selected patients with rectal cancer where the impact of radiotherapy on dfs and os is marginal . 
 in this scenario we undertook a prospective observational study to determine the feasibility and the impact on local control and quality of life of the combination of shortcourse preoperative rt and neo - adjuvant chemotherapy in patients affected by locally advanced resectable rectal cancer . 
the addition of chemotherapy to the hypofractionated radiation treatment , suggested by the hypothesis that induction chemotherapy would reduce gross tumour burden and improve oxygenation and hence sensitise to rt , has led us to reduce the total dose of radiotherapy by 20% compared to the standard scheme proposed by the swedish study ( 20 gy in ve consecutive fractions vs 25 gy in ve fractions ) with a biologically effective radiation therapy dose ( bed ) of 28 gy , despite the fact that the colorectal cancer collaborative group had recommended a bed > 30 gy on the basis of a metanalysis . 
 we hypothesised that the moderate reduction of bed della chemioterapia concomitante alla radioterapia rimangono , ancora oggi , controversi . sulla scorta del successo ottenuto dalla terapia sistemica nelle neoplasie del colon , alcuni studi hanno valutato un approccio neoadiuvante esclusivamente chemioterapico nel trattamento delle neoplasie localmente avanzate del retto . 
 [ 29 ] , ad esempio , hanno analizza to 26 pazienti affetti da neoplasia del retto in stadio t3 or t4 , n02 , m0 sottoposti a chemioterapia neoadiuvante ( 2 cicli di irinotecan , 5 - fu and lv ) e hanno riportato un tasso di sopravvivenza globale e libera da malattia a 5 an ni dell84% e 74% rispettivamente . 
 [ 30 ] ha evidenziato un tasso di risposte patologiche complete dopo sola chemioterapia neoadiuvante ( uorouracil , leucovorin , oxaliplatin e bevacizumab ) , senza radioterapia , del 23% . 
il nuovo us alliance cooperative group ( in origine cancer and leukemia group b , american college of surgeons oncology group , and north central cancer treatment group ) ha pianicato un studio multicentrico randomizzato che investighi questo approccio terapeutico ( senza bevacizumab )  . 
una recente revisione della letteratura [ 31 ] ha concluso che vi unevidenza molto preliminare che i pazienti affetti da neoplasia del retto localmente avanzata , la cui malattia venga stadiata con risonanza magnetica , possano beneciare di un trattamento neoadiuvante di sola chemioterapia omettendo il tempo radioterapico , bench siano necessari studi futuri di confronto tra i vari approcci terapeutici in pazienti altamente selezionati in cui limpatto della radioterapia sul controllo di malattia possa essere giudicato marginale . in questo scenario , abbiamo intrapreso uno studio prospettico osservazionale che si poneva lobiettivo di valutare la fattibilit e i risultati in termini di controllo di malattia , tossicit e qualit di vita , di un approccio neoadiuvante di chemioterapia seguita da radioterapia ipofrazionata e chirurgia immediata in pazienti affetti da neoplasia localmente avanzata del retto . 
laggiunta della chemioterapia a un trattamento radioterapico ipofrazionato , con lipotesi che la chemioterapia di induzione riduca il carico tumorale e aumenti lossigenazione del tumore aumentandone quindi la radiosensibilit , ha comportato una riduzione della dose totale di radioterapia del 20% rispetto alla dose standard utilizzata nello studio svedese , con una diminuzione della dose biologica equivalente ( bed ) da > 30 gy a 28 gy . 
per , tali interazioni generalmente sono note nei trattamenti radio - chemioterapici concomitanti piuttosto che sequenziali , anche se possibile 1408 radiol med ( 2013 ) 118 : 13971411 would be compensated by the antitumour activity of chemotherapy , without increasing treatment - related toxicity . 
it is possible that the additive effects of chemotherapy followed by radiation may compensate for the lower dose of radiation used in this study . to our knowledge , our study is the rst one that analysed the combination of neo - adjuvant chemotherapy and shortcourse rt in a preoperative setting in patients affected by locally advanced resectable rectal cancer . according to the protocol , only patients with ct3 / t4 or n + disease were eligible . 
 [ 32 ] showed that not only radio - chemotherapy but also short - term radiotherapy can lead to a signicant reduction in tumour size as early as 1.3 days after the end of treatment . in terms of results , the local recurrence rate in this trial was lower than in other studies , although tme was not performed in all patients . 
this may be related to the fact that it was a single - centre study with standardised quality - controlled surgery and a high rate of optimally performed surgical procedures , also documented by the nding of no case of r + disease . 
 this study did not investigate the role of the preoperative short course ct - rt in terms of sphincter preservation , because the decision to perform ar vs apr depended on the distance of the lesion from the anal verge , as evaluated before preoperative chemo - radiation . 
 [ 33 ] found patients with postoperative complication rates of 27% in the preoperative short - course radiotherapy group , compared with 21% in the neo - adjuvant radio - chemotherapy group . one of the main potential problems of hypo - fractionated radiotherapy is late toxicity , especially in terms of risk of incontinence and sexual dysfunction [ 3438 ]  . 
the relative low rate of long term complications , observed in our study group , may be due to the relatively low total dose of radiotherapy ( 20 gy in ve fractions compared with standard 25 gy in ve fractions ) and to the small volume of treatment che siano presenti anche in regimi di trattamenti sequenziali , come il nostro studio , e in grado quindi di compensare una riduzione moderata della dose di radioterapia . 
il nostro studio appare essere lunico presente in letteratura che abbia associato un trattamento neoadiuvante radioterapico short - course a una terapia sistemica nei tumori del retto in stadio ct3 / t4 e / o n +  . 
 [ 32 ] mostrarono che non solo la radio chemioterapia long - course ma anche la radioterapia shortcourse pu comportare una riduzione della massa tu morale . analizzando i risultati del nostro studio , il tasso di recidiva locale sembra essere pi basso rispetto a quanto riportato in letteratura , anche a fronte di una tme non sempre eseguita . 
questo studio non ha valutato limpatto della radioterapia pre - operatoria short - course sulla preservazione snteriale , in quanto il tipo di intervento chirurgico veniva deciso sulla base della distanza della malattia iniziale dallo sntere anale , come valutato agli esami di stadiazione pre - operatoria . 
nel nostro studio , anche se il 20% dei pazienti si presentava con malattia del retto basso , il tasso di preservazione snteriale risultato molto alto , in quanto pianicato e ottenuto in tutti i pazienti con neoplasia localizzata almeno a 5 cm dalla rima anale . 
 [ 33 ] hanno riportato un tasso di complicanze post - operatorie del 27% nel gruppo di pazienti sottoposti a radioterapia short - course rispetto al 21% nei pazienti trattati con chemio - radio concomitante long - course . uno dei maggiori potenziali problemi dellipofrazionamento la tossicit tardiva , soprattutto in termini di rischio di incontinenza e disfunzione sessuale [ 3438 ]  . 
 [ 33 ] ha evidenziato un tasso globale di tossicit del 28 , 3% e una percentuale di tossicit tardiva denita severa del 10 , 1% dopo un follow - up mediano di 48 mesi . 
 gli ottimi risultati ottenuti dal nostro approccio in termini di tossicit tardiva potrebbero essere giusticati dalla pi bassa dose totale di radioterapia . alcuni importanti limiti di questo studio necessitano di approfondimento . 
in prima istanza , questo uno sturadiol med ( 2013 ) 118 : 13971411 1409 only involving the rectum and the perirectal nodes . the limitations of this trial , however , should be acknowledged . 
the rst point is that our study is a prospective observational study , born by a common practice - derived prospective treatment schedule of a hypofractionated neo - adjuvant radiation treatment with the introduction of the systemic therapy according to the de gramont scheme before and folffox 6 scheme subsequently . 
the principles of total mesorectal excision ( tme ) were not mandatory ( even though it was performed in many patients ) and there was no histopathological examination of the circumferential resection margin ( pcrm ) , the most important predictor for local recurrence / prognosis after preoperative rt or chemo - radiation therapy . 
 on the other hand , two novel aspects of this study are the combination of chemotherapy with short course preoperative radiation , and the extensive use of qol questionnaires with long follow - up . 
the strength of this study was the homogeneity of the cohort of patients treated with the same chemotherapeutic agents , the same rt technique in terms of doses and volumes and with a surgical approach performed in the same centre with well established quality control . 
this study was a pilot trial that could serve as the basis for a larger , possibly multicentre , prospective study to determine the difference in terms of disease control and quality of life between long - course and short - course preoperative rt in combination with chemotherapy . dio prospettico osservazionale , nato da un protocollo interno di pratica clinica , in cui il trattamento standard di radioterapia neoadiuvante short - course stato modicato dallaggiunta della chemioterapia neoadiuvante e dalla riduzione della dose totale . 
inoltre , diversi regimi chemioterapici si sono alternati nel corso dello studio ( dal 2003 stato aggiunto loxaliplatino ) , lutilizzo della tecnica chirurgica di tme non era mandatoria e , come tale , non eseguita in tutti i pazienti e , in ultimo , non vi una valutazione isto - patologica del margine di resezione circonferenziale ( a oggi riconosciuto come uno dei maggiori fattori predittivi di recidiva locale )  . 
 a fronte di queste limitazioni , il nostro studio ha due nuovi importanti aspetti a suo favore : la proposta di nuovo approccio radio - chemioterapico neoadiuvante e lutilizzo di questionari sulla qualit di vita analizzati a un lungo follow - up . 
indubbiamente un punto di forza lomogeneit del campione e del tipo di trattamento , chemioterapico , radioterapico , cos come chirurgico . questo studio pilota potrebbe essere utile per disegnare futuri studi prospettici randomizzati multicentrici di confronto tra un approccio neoadiuvante di radio - chemioterapia concomitante long - course e radioterapia short - course , in termini di controllo di malattia e qualit di vita . conclusioni conclusions in our study neo - adjuvant chemotherapy and short - course radiation treatment followed by immediate surgery generated relatively high local control rates . 
 acknowledgements the authors are greateful to doctor luciano armaroli , former director of radiation oncology unit at arci spedale santa maria nuova , reggio emilia , until 2008 , who has been the author and promoter of this study . nel nostro studio la chemioterapia neoadiuvante e la radioterapia pre - operatoria short - course , seguite da chirurgia immediata , hanno dimostrato un alto tasso di controllo locale di malattia . sono necessari futuri studi multicentrici per identicare il corretto approccio neoadiuvante atto a ottenere i migliori risultati in termini di controllo di malattia e tossicit tardiva . ringraziamenti gli autori ringraziano il dott . 
luciano armaroli , direttore della struttura complessa di radioterapia oncologica no al 2008 , ideatore e promotore di questo studio . conict of interest the authors declare that they have no conict of interest related to the publication of this article . 
avogadro , scuola di specializzazione in radiodiagnostica , novara , italy 3scdu ortopedia e traumatologia , aou maggiore della carit di novara , italy 4ortopedia , casa di cura frate sole , figline valdarno ( fi ) , italy 5sc fisica medica , aou maggiore della carit , novara , italy correspondence to : a . 
stecco , tel : + 39 - 0321 - 3732004 , fax : + 39 - 0321 - 3733425 , e - mail : a.stecco@libero.it received : 7 march 2012 / accepted : 21 june 2012 / published online : 27 may 2013 springer - verlag 2013 abstract objective . 
sono state acquisite le ricostruzioni mpr in tc e le immagini rm sul piano sagittale : la misura dellarea della glena e la misura del danno osseo sono state effettuate utilizzando il metodo pico . 
la misura dellarea glenoidea risulta di 575 , 29 mm2 con rm e di 573 , 76 mm2 con tc e le rispettive misure del deficit glenoideo sono di 4 , 38% e 4 , 34% . 
la concordanza inter - osservatore in tc e rm risultata buona con k > 0 , 81 , il coefficiente di varianza < 5% del valor medio sia in tc che rm . 
dislocation can be caused by an indirect , lowor high - energy mechanism and , although it may be an isolated event , it often tends to recur and creates a clinical picture of shoulder instability . evaluating glenoid bone loss has become fundamentally important for the therapeutic choice [ 1 ] , and a number of studies have shown that a high percentage of patients with shoulder instability present glenoid bone loss [ 17 ]  . 
it is therefore essential to have a preoperative diagnostic instrument that is predictive , simple and easy to use insofar as the choice of therapy is based on the guidelines proposed by provencher et al . 
la spalla larticolazione in cui la perdita dei rapporti articolari si verifica pi spesso ; la lussazione , causata da un meccanismo indiretto a bassa o ad alta energia , pu rappresentare un evento isolato , ma pi spesso tende a riprodursi nel tempo configurando il quadro di instabilit . la valutazione delle lesioni ossee della rima glenoidea , come difetto osseo ( bone loss ) , ha assunto negli ultimi anni unimportanza fondamentale nella scelta terapeutica [ 1 ]  . 
il principale obiettivo nello studio delle lesioni ossee della rima glenoidea valutare il grado di difetto osseo e definirne la severit oltre una certa percentuale di perdita della superficie globale della glena . 
 quindi fondamentale disporre di uno strumento diagnostico pre - operatorio dotato di una buona predittivit , facile e semplice , in quanto la scelta del trattamento terapeutico deve seguire le linee guida proposte da provencher et al . 
mri was carried out using a 1.5 tesla philips achieva ( philips medical systems , best , the netherlands ) with a surface coil [ voxel size 0.7 mm , flip angle 50 , thickness 0.7 mm , time to repetition ( tr ) 23 , time to echo ( te ) 5.1 ] and a 3d - t1w fast field echo ( ffe ) sequence . 
i pazienti , previo consenso informato , sono stati sottoposti a tc e rm della spalla sana e di quella patologica nella stessa giornata . metodo di quantificazione del danno glenoideo per le scansioni tomografiche stato usato uno strumento light speed vct a 64 file di detettori ( ge , milwaukee , wisconsin , usa )  . 
the pico method involves drawing a circular area ( x ) on an oblique sagittal en face image of the healthy shoulder using the lower glenoid margin as a base . 
 this circle is then transposed to the image of the pathological shoulder and the area of the sector with missing bone is drawn and calculated ( bone loss , yi )  . 
bone loss was measured three times by two operators in consensus ( in order to reduce measurement error ) , and the mean value of the three measurements was recorded ( y ) , whereas x was only calculated once by the two operators in consensus . % bone loss = area y area x * 100 the effective ct doses were estimated starting from the individual dose ratios archived in the picture archiving and communication system ( pacs ) and using version 1.02 of the impact ct patient dose calculator software ( impact , london , uk ) , which is based on montecarlo simulations and uses the international commission on radiological protection ( icrp ) 103 weighting factors for tissue . 
 statistical analysis the statistical analyses were made using the medcalc 12.2.0.1 statistical package ( medcalc software mariakerke , belgium )  . the repeated measures of mean glenoid bone loss made by more than one operator using the ct and mr images were analysed by calculating their coefficient of variance ( cv ) and standard deviation using the test for repeated measures [ 11 ]  . 
 the variability of the independent manual measurements , evaluated in terms of standard deviation and variance , was very good as the cv was less than 5% of the mean value of algoritmo per losso , spessore di strato 0 , 6 mm , tempo di rotazione 0 , 6 s , voltaggio 140 kv e intensit 180 ma . 
lesame rm stato eseguito mediante apparecchiatura philips serie achieva ( philips medical systems , best , olanda ) a 1 , 5 tesla , con una bobina di superficie ( voxel size 0 , 7 mm , flip angle 50 , thickness 0 , 7 mm , tempo di ripetizione ( tr ) 23 , tempo di eco ( te ) 5 , 1 ) utilizzando la sequenza t1 - 3d fast field echo ( ffe )  . 
il metodo pico prevede che sullimmagine sagittale obliqua della glena sana ( immagine en face della glena ) si disegni unarea circolare ( x ) utilizzando come base il margine inferiore della glena . 
la misurazione del difetto osseo stata ripetuta tre volte da due operatori in consensus ( per ridurre lerrore della misura , utilizzando la media delle tre , y ) , mentre larea circolare x stata calcolata una sola volta sempre dai due operatori in consensus . % difetto osseo = area y area x * 100 le dosi efficaci in tc sono state stimate a partire dai rapporti di dose individuale archiviati sul picture archiving and communication system ( pacs ) e utilizzando il software impact ct patient dose calculator v1.02 ( impact , london , uk ) , che basato su simulazioni montecarlo e utilizza i fattori di peso per il tessuto dell international commission on radiological protection ( ircp ) 103 . 
 analisi statistiche tutte le analisi statistiche sono state eseguite mediante il pacchetto applicativo statistico medcalc 12.2.0.1 ( medcalc software mariakerke , belgium )  . le misure ripetute da pi operatori effettuate sulle immagini tc e rm del danno medio del deficit osseo glenoideo sono state analizzate valutando il coefficiente di varianza e la deviazione standard con il test per misure ripetute [ 11 ]  . 
 successivamente , stata valutata la concordanza inter - osservatore tra i due osservatori rm e tc , mediante il test di concordanza k di cohen [ 12 ] , classificando in classi di concordanza comprese tra poor e very good , rispettivamente se k < 0 , 20 o k > 0 , 81 [ 13 ]  . stato applicato il test di bland - altman per la correlazione delle differenze tra le due tecniche di misurazione , plottando le misure delle due metodiche contro la media delle stesse , sia per le misure ottenute sulla glena normale con entrambe le metodiche , che per le misure di danno glenoideo . 1338 radiol med ( 2013 ) 118 : 13351343 fig . 
larea della glena della spalla sana misurata varia tra 481 , 44 e 694 , 34 mm2 in tc , tra 482 , 69 e 694 , 41 mm2 in rm , con un valore medio rispettivamente di 573 , 76 mm2 e 575 , 29 mm2 . 
il valore medio del difetto glenoideo , misurato manualmente dai due operatori , variava tra 0 e 92 , 78 mm2 in rm e tra 0 e 94 , 79 mm2 in tc . 
 la variabilit delle misurazioni manuali indipendenti , valutata in termini di deviazione standard che di varianza , stata molto buona , risultando il coefficiente di varianza ( cv ) inferiore al 5% del valore medio sia nella tc ( 4 , 88% ) che nella rm ( 4 , 08% )  . 
nel 2003 [ 9 ] hanno calcolato la percentuale del deficit osseo glenoideo mediante un metodo tc con ricostruzi oni 3d , dimostrando come la met inferiore della glena possa essere considerata con buona approssimazione una circonferenza passante da ore tre a ore nove . 
poich in uno stesso individuo la superficie delle due glene identica , calcolando prima larea circonferenziale della met inferiore della glena sana , possibile valutare la morfologia della glena patologica e calcolare il deficit osseo in termini di area ( espressa in mm2 ) o in percentuale di superficie , semplicemente disegnando larea deficitaria o il contorno del frammento . 
 [ 19 ] , in uno studio del 2007 , hanno confrontato laccuratezza della tc rispetto allartroscopia nella valutazione del difetto osseo della glena ; cinquanta pazienti sono stati sottoposti allesame tc e successivamente allartroscopia . 
 [ 20 ] hanno confrontato la tc 2d e 3d nella quantificazione del danno osseo nellinstabilit anteriore di spalla , riscontrando lequivalenza tra le due tecniche . sebbene la tc rappresenti la metodica delezione per valutare lentit del danno glenoideo ( presenta , infatti , unalta sensibilit : 93% e specificit : 78% ) , la risonanza magnetica largamente utilizzata nella diagnosi preoperatoria delle lesioni a carico dei tessuti molli articolari ( cercine glenoideo , apparato capsulo - legamentoso ) [ 2125 ]  . 
 [ 18 ] , effettuato su 14 glene di cadaveri , ha validato il meto do proposto da sugaya applicato alla rm come metodica sovrapponibile alla tc per quantificare il danno glenoideo . 
 [ 26 ] , utilizzando unapparecchia tura ad alto campo ( 3t ) , ne hanno dimostrato sia lapplicabilit per una migliore visualizzazione delle strutture ossee , tendinee , cartilaginee e legamentose , sia una maggiore risoluzione spaziale , particolarmente utile nello stu dio delle articolazioni o di alcune loro componenti fino a oggi valutabili in maniera sub - ottimale con esami non artrografici . nel nostro studio , per la prima volta , il metodo pico stato applicato in vivo , sia in tc che rm , per confrontare fig . 
ct - mr : tc - rm ; average of ct and mr : media di tc e rm . recurrent dislocations or luxations and , more importantly , it influences the type of surgery . 
many methods of ascertaining the presence and extent of bone loss have been described in the literature , and some authors have tried to quantify it radiologically or arthroscopically [ 2 , 1518 ]  . 
 [ 9 ] calculated the percentage of glenoid bone loss using ct - based 3d reconstructions , and showed that the lower half of the glenoid cavity can with good approximation be considered a circumference passing from three oclock to nine oclock . 
as the surfaces of the two glenoid cavities in the same subject are identical , by first calculating the circumferential area of the lower half of the healthy shoulder , the bone loss can be calculated in terms of area ( expressed in mm2 ) or percentage simply by drawing the area of the deficiency or the outline of the fragment . 
 [ 19 ] compared the accuracy of ct and arthroscopy in assessing glenoid bone loss in 50 patients , and found that ct was highly sensitive and specific , and that the findings correlated closely with the arthroscopic findings . 
 [ 20 ] compared 2d and 3d ct for the quantification of bone loss in anterior shoulder instability , and discovered that the two techniques were equivalent . although the 93% sensitivity and 78% specificity of ct make it the method of choice for assessing glenoid bone loss , mri is widely used in the preoperative diagnosis of lesions affecting articular soft tissue ( the glenoid rim , the capsular - ligament complex ) [ 2125 ]  . 
 [ 18 ] have evaluated the use of sugayas method on mr images of 14 cadaveric shoulders , and found that the results were the same as those obtained using ct . 
 [ 26 ] , using high - resolution equipment ( 3t ) , showed both its ap1342 radiol med ( 2013 ) 118 : 13351343 plicability for better visualisation of bone , cartilage and ligament structures , and better spatial resolution ; the latter is particularly useful in the study of the joints or other components so far only sub - optimally evaluated with nonarthrographic examinations . our study is the first to use the pico method in vivo to compare the diagnostic accuracy of ct and mr imaging . 
 the two series of measurements can be considered substantially equivalent , as shown by the cohen kappa value of > 0.81 , and so this pilot study has established that the results are sufficiently promising to allow the planning of a study of a larger group of patients . albeit with the limitation of the small number of patients due to the preliminary nature of this study , it can be concluded that either ct or mri can be used as a preoperative diagnostic technique for measuring bone loss using the pico method . 
it has also been demonstrated that mri can be used as a reference method not only for studying the rotator cuffs and the glenoid rim , but also for quantifying bone loss ; this makes it possible to limit the patients exposure to ionising radiation when diagnosing the bone loss associated with shoulder instability . laccuratezza diagnostica delle due metodiche . 
le due serie di misurazioni ottenute con tc e rm possono ritener si sostanzialmente equivalenti come dimostrato dal valore k di cohen ottenuto ( k > 0 , 81 ) ; pertanto questo studio pilo ta ha permesso di stabilire che i risultati ottenuti applicando il metodo pico a spalle studiate in vivo sia con la tc che con la rm sono sufficientemente promettenti per pianificare uno studio allargato su una popolazione pi estesa . si pu concludere che , pur con la limitazione del numero ridotto di pazienti data la natura preliminare di que sto studio , possibile applicare indifferentemente i metodi tc e rm per misurare il difetto osseo della spalla con il metodo pico come tecnica diagnostica pre - operatoria . 
si inoltre dimostrato che la risonanza magnetica pu esse re utilizzata come metodica di riferimento non solo nello studio della cuffia dei rotatori e del cercine , ma anche per la quantificazione del danno osseo ; ci permette di limitare lesposizione dei pazienti a radiazioni ionizzanti nella diagnosi della perdita ossea associata allinstabilit di spalla . conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . 
ruggieri1 1department of orthopaedics , istituto ortopedico rizzoli , bologna , italy 2department of interventional angiographic radiology , istituto ortopedico rizzoli , bologna , italy 3department of radiology , istituto ortopedico rizzoli , bologna , italy 4department of anesthesiology , s . 
rossi , department of orthopaedics , orthopaedic oncology service , istituto ortopedico rizzoli , university of bologna , via di barbiano 1 / 10 , 40136 , bologna , italy , tel . : + 39 - 051 - 6366460 , fax : + 39 - 051 - 6366540 , e - mail : giuseppe.rossi@ior.it received : 6 october 2011 / accepted : 4 december 2011 / published online : 9 august 2012 springer - verlag 2012 abstract purpose . 
all patients had primary treatments including chemotherapy , radiation therapy , radiofrequency thermal ablation , and / or surgery for their advanced sarcomas and were referred for embolisation as end - stage treatment for continuous severe local pathe effect of embolisation was evaluated with a pain score scale and analgesic use . 
tutti i pazienti sono stati sottoposti ad un trattamento di prima linea che includeva chemioterapia , radioterapia , termoablazione con radiofrequenza e / o chirurgia per sarcomi in fase avanzata , e sono stati successivamente trattati con lembolizzazione come trattamento nale per il dolore locale severo e continuo . 
trentasei pazienti con sarcomi altamente ipervascolarizzati , sarcomi della pelvi e del cingolo scapolare sono andati incontro ad una quasi completa risoluzione del dolore e ad una riduzione delluso di analgesici maggiore del 50% . 
embolisation is a safe and effective local palliative treatment for patients with advanced sarcomas , providing optimum pain relief with the least discomfort and the possibility of minor complications only . keywords selective embolization nbca advanced bone sarcomas follow - up nessun paziente ha lamentato la ricomparsa del dolore con intensit pari a quella presente prima dellembolizzazione . 
lembolizzazione un trattamento palliativo locale sicuro ed efcace per i pazienti con sarcomi ossei in fase avanzata , garantendo unottimale risoluzione del dolore , un minimo disagio ed una minor incidenza di complicanze . parole chiave embolizzazione selettiva nbca sarcomi dellosso in fase avanzata introduction introduzione advanced bone sarcomas have two distinct clinical forms : ( 1 ) metastatic advanced in various organs , and ( 2 ) locally advanced , either primary or recurrent , and unresectable . 
 metastatic advanced sarcomas are usually regarded as an incurable , fatal condition that requires only palliation ; the tumours tend to be chemoresistant and prognosis is poor [ 14 ]  . 
locally advanced sarcomas namely , primary or recurrent and unresectable usually involve all compartments of the limb or a major adjacent structure , such as the neurovascular bundle , pelvic organs , chest wall or vertebra [ 1 ]  . 
unresectable tumours may be large masses involving challenging , sites such as the pelvis , the sacrum and spine ; or occur in patients who are poor surgical candidates or refuse denitive surgery [ 4 , 5 ]  . 
locally advanced bone sarcomas tend to be very symptomatic , leading to severe pain , sepsis , tumour fungation , haemorrhage , thrombosis , pathological fractures , severe functional impairment and poor quality of life . 
these tumours are not amenable to limited locoregional intervention , such as standard limb salvage or amputation , but necessitate a major amputative surgical procedure to effect a potential cure ; yet , even then , the prognosis is poor [ 1 , 7 ]  . over the past 40 years , advances in diagnostic imaging , interventional radiology , chemotherapy and surgery have greatly improved the outcome of patients with bone sarcoma and made limb salvage possible without compromising survival [ 5 , 8 , 9 ]  . 
agi sarcomi dellosso in fase avanzata si presentano in due forme cliniche distinte : ( 1 ) avanzati con metastasi in diversi organi ; ( 2 ) localmente in fase avanzata , sia primari che ricorrenti , e non resecabili . 
i sarcomi metastatici in fase avanzata sono di solito visti come una condizione incurabile e letale che richiede solo una palliazione ; questi tumori hanno la tendenza ad essere chemioresistenti e con prognosi scarsa [ 14 ]  . 
i sarcomi localmente in fase avanzata , primari o ricorrenti , e non resecabili , di solito coinvolgono tutti i compartimenti di un arto o le strutture nobili adiacenti come i fasci vasculonervosi , gli organi pelvici , la parete toracica o le vertebre [ 1 ]  . 
i tumori non resecabili possono essere grandi masse coinvolgenti siti critici come la pelvi , il sacro e il rachide , oppure tumori in pazienti con scarsa indicazione chirurgica o che riutino la chirurgia radicale [ 4 , 5 ]  . 
i sarcomi dellosso localmente in fase avanzata tendono ad essere molto sintomatici , dando dolore severo , sepsi , vegetazione tumorale , emorragia , trombosi , fratture patologiche , severa limitazione funzionale e scarsa qualit di vita . 
questi tumori non sono trattabili con interventi locoregionali limitati come il salvataggio standard dellarto o lamputazione , ma necessitano di procedure chirurgiche pi radicali per un intento potenzialmente curativo ; tuttavia , nonostante questo , la prognosi scarsa [ 1 , 7 ]  . negli ultimi 40 anni i progressi della diagnostica per immagini , della radiologia interventiva , della chemioterapia e della chirurgia hanno migliorato notevolmente loutcome dei pazienti con sarcoma , ed hanno reso possibile la preservazione dellarto senza compromettere la sopravvivenza [ 5 , 8 , 9 ]  . 
sono attualmente disponibili trattamenti medici e 1346 radiol med ( 2013 ) 118 : 13441359 gressive local and medical treatments are available [ 10 ] , but in consideration of the poor prognosis , most treatments are aimed at palliation [ 1 ]  . 
the indications for palliative major amputation , including forequarter amputation and standard or extended hemipelvectomy in patients with locally advanced sarcomas include : ( 1 ) involvement of a proximal limb or a major joint accompanied by intractable pain , sepsis , tumour fungation , haemorrhage , vascular thrombosis , pathologic fractures and radiation - induced necrosis ; and / or ( 2 ) a limb with severe functional impairment [ 12 , 13 ]  . 
moreover , palliative major amputation is not feasible for patients with locally advanced , unresectable sarcomas . in this setting , the role of conservative local treatments , such as medical treatments and analgesics , isolated limb perfusion , radiation therapy , embolisation , chemoembolisation , thermal ablation and cryotherapy , is important for palliation . 
the aim of palliative treatments is to achieve a mild response by offering the least discomfort possible with the minimum possible medical risks for optimum pain relief and quality of the remaining life . 
in this article , we present a series of patients with advanced bone sarcomas treated with transcatheter selective and superselective arterial embolisation with n - 2 - butyl cyanoacrylate ( nbca ) , emphasising the palliative role of embolisation for pain relief in end - stage sarcoma patients . materials and methods we retrospectively studied the medical les of 43 patients with locally advanced bone sarcomas treated with palliative selective or superselective transcatheter embolisation from 2004 to 2011 . 
all patients had primary treatments , including chemotherapy , radiation therapy , radiofrequency thermal ablation and / or surgery for their advanced sarcomas and were referred for embolisation because of continuous severe local pain ( 710 points in visual pain scale pre - embolisation )  . 
after receiving explanations regarding the possible risks and complications of embolisalocali aggressivi [ 10 ] , tuttavia in previsione di una prognosi scarsa la maggior parte dei trattamenti sono rivolti alla palliazione [ 1 ]  . 
le indicazioni per unamputazione palliativa maggiore , compresa lamputazione radicale dellarto e lemipelvectomia standard o estesa , in pazienti con sarcomi in fase avanzata localmente , includono il coinvolgimento della radice dellarto o di unarticolazione maggiore accompagnati da dolore intrattabile , sepsi , vegetazione tumorale , emorragia , trombosi , fratture patologiche necrosi post - attinica e / o un arto con severa limitazione funzionale [ 12 , 13 ]  . 
per di pi lamputazione palliativa maggiore non eseguibile su pazienti con sarcomi in fase avanzata non resecabili . alla luce di ci , il ruolo dei trattamenti conservativi , che include la terapia medica e analgesica , la perfusione isolata dellarto , la radioterapia , embolizzazione e chemioembolizzazione , la termoablazione e la crioterapia hanno un ruolo importante nella palliazione . 
lo scopo dei trattamenti palliativi il raggiungimento di una buona risposta arrecando al paziente la minor sofferenza con il minor rischio possibile , per ottenere la miglior analgesia e una qualit di vita adeguata . 
in questo articolo presentiamo una serie di pazienti affetti da sarcoma osseo in fase avanzata trattati mediante embolizzazione arteriosa selettiva e superselettiva con n - 2 - butil - ciano - acrilato ( nbca ) allo scopo di enfatizzare il ruolo palliativo dellembolizzazione nel trattamento della sintomatologia dolorosa in pazienti con sarcoma in stadio terminale . materiali e metodi abbiamo studiato retrospettivamente le cartelle cliniche di 43 pazienti con sarcomi dellosso localmente in fase avanzata trattati con embolizzazione selettiva o superselettiva dal 2004 al 2011 . 
tutti i pazienti erano stati sottoposti a trattamenti di prima linea che includevano chemioterapia , radioterapia , termoablazione con radiofrequenze e / o intervento chirurgico per sarcoma in fase avanzata e sono stati successivamente indirizzati allembolizzazione per dolore locale severo e continuo ( punteggio da 7 a 10 in una scala del dolore visiva , prima dellembolizzazione )  . 
il follow - up medio stato di 7 mesi ( range 119 mesi ) ; tutti i pazienti sono deceduti allultimo follow - up ( tabella 1 )  . radiol med ( 2013 ) 118 : 13441359 1347 1348 radiol med ( 2013 ) 118 : 13441359 radiol med ( 2013 ) 118 : 13441359 1349 tion , all patients gave their informed consent for the procedure . 
the mean follow - up was 7 ( range , 119 ) months ; all patients were dead at the last follow - up ( table 1 )  . indication for angiography and embolisation was continuous severe pain refractory to analgesics ; at the time of embolisation , all patients were administered continuous transdermal or repeated bolus injections of morphine . 
diagnostic digital subtraction angiography ( dsa ) was performed to identify the pathological tumour vasculature ( contrast media : iomeprol 300 mg / ml , iomeron , bracco , milan , italy , and iohexol 350 mg / ml , omnipaque , ge healthcare , milan , italy ; angiographic apparatus : philips integris v3000 cesar - scp - visub , philips medical systems , eindhoven , the netherlands , and siemens angiostar plus / plus o.r. , siemens ag , medicals engineering , forchheim , germany )  . 
 the femoral artery was catheterised with a 4 - f ( cordis corporation , miami , fl , usa ) or 5 - f ( terumo corporation , tokyo , japan ) introducer . 
the embolic agent used was the nbca ( glubran 2 , gem , viareggio , italy ) in 33% lipiodol [ 1 acon ( 10 ml ) , lipiodol ultrauido , guerber s.p.a. 
 from the mixture , 1 ml was aspirated in an insulin ( 1 ml ) syringe ; depending on the vascular injury , 0.10.2 ml of the aspirate mixture was injected , sandwiched with 2 + 2 ml of 5% glucosate solution under uoroscopic control . 
 a total of 53 embolisation procedures were performed ; one patient had four , one had three and ve had two . patients were admitted on the day of the procedure and discharged the day after . 
complications and local pain were lindicazione allangiograa e allembolizzazione un dolore continuo e severo , refrattario agli analgesici ; al momento dellembolizzazione a tutti i pazienti stata somministrata morna sotto forma di cerotto transdermico o ripetuti boli endovenosi . 
langiograa diagnostica con sottrazione digitale ( mezzo di contrasto : iomeprol 300 mg / ml , iomeron , bracco , milano , italia ; e iohexol 350 mg / ml , omnipaque , ge healthcare , milano , italia ; apparato angiograco : philips integris v3000 cesar - scp - visub , philips medical systems , eindhoven , paesi bassi : siemens angiostar plus / plus o.r. , siemens ag , medicals engineering , forchheim , germania ) stata eseguita per identicare la vascolarizzazione patologica del tumore . 
larteria femorale stata cateterizzata con un introduttore da 4 french ( cordis corporation , miami , fl , usa ) o da 5 french ( terumo corporation , tokyo , giappone )  . 
nei pazienti con sarcomi del rachide e della pelvi stata eseguita unaortograa panoramica usando cateteri pigtail da 4 french ( cordis corporation ) , seguita da unarteriograa selettiva e superselettiva mediante cateteri cobra , simmons e vertebrali ( terumo corporation ) o microcateteri di 130 cm da 2 , 72 , 9 french pre - sagomati mc - pp27131 ( coaxial catheters system , terumo corporation )  . 
 lagente embolizzante utilizzato stato lnbca ( glubran 2 , gem , viareggio , italia ) in 33% di lipiodol ( 1 acone 10 ml , lipiodol ultrauido , guerber s.p.a. , francia ) , prima e dopo la somministrazione di soluzione glucosata al 5% , allo scopo di prevenire la polimerizzazione con il sangue durante la somministrazione dellagente embolizzante attraverso il catetere . 
un acone ( 1 ml ) di nbca viene miscelato con 2 ml di lipiodol al 33% e da questa miscela viene aspirato 1 ml in una siringa da insulina ( 1 ml ) ; a seconda del danno vascolare 0 , 10 , 2 ml della miscela aspirata vengono iniettati sotto controllo uoroscopico , inframezzati a 2 + 2 ml di soluzione glucosata al 5% . 
sono state eseguite un totale di 53 embolizzazioni ; un paziente stato sottoposto a 4 procedure , un altro a 3 procedure e cinque pazienti a 2 procedure . i pazienti sono stati ricoverati dal giorno della procedura no al giorno successivo . 
lintensit del dolore stata valutata con un punteggio da 0 a 10 su una scala visiva , da 0 ( assenza di dolore ) a 10 ( dolore severo e costante ) e con luso di analgesici . 
la risoluzione del dolore stata denita come la riduzione maggiore o uguale al 50% della dose di analgesici utilizzati e riduzione maggiore o uguale al 50% 1350 radiol med ( 2013 ) 118 : 13441359 fig . 
1a axial ( left ) and sagittal ( right ) mr images of the lumbar spine of a 45 - year - old man with a locally advanced recurrent brosarcoma of the l4 vertebra ( patient 33 )  . 
1a immagini di rm assiali ( sinistra ) e sagittali ( destra ) del rachide lombare in un uomo di 45 anni con brosarcoma recidivante localmente in fase avanzata di l4 ( paziente 33 )  . 
pain relief was dened as 50% reduction in pain score and 50% reduction in analgesic doses ; no relief as < 50% decrease . risultati del punteggio iniziale della scala del dolore , mentre la mancata risoluzione stata denita come una riduzione inferiore al 50% . results in all patients , angiography showed increased pathological vascularisation of the advanced sarcomas . 
lower pathological vascularisation compared with the other advanced sarcomas , but increased vascularisation was observed in in tutti i pazienti langiograa ha mostrato un incremento della vascolarizzazione patologica nei sarcomi in fase avanzata . 
2a coronal mr images of the pelvis of a 19 - year - old woman with a locally advanced , unresectable osteosarcoma of the pelvis and sacrum , extending to the lower lumbar spine ( patient 34 )  . 
b digital subtraction angiography shows the pathological tumour vessels originating from the left l3 and l4 arteries ( arrows ) and the superior gluteal artery ( not shown )  . 
2a immagini rm coronali del bacino in una donna di 19 anni con osteosarcoma non resecabile localmente in fase avanzata della pelvi e del sacro , che si estende al rachide lombare inferiore ( paziente 34 )  . 
b langiograa con sottrazione digitale mostra la vascolarizzazione patologica del tumore originata dalle arterie per l3 ed l4 di sinistra ( frecce ) e dallarteria glutea superiore ( non mostrata )  . 
b digital subtraction angiography shows the pathological tumour vessels originating from the right l3 , l4 and l5 arteries , and a hypertrophic branch of the middle sacral artery ( msa , arrows )  . 
b langiograa con sottrazione digitale mostra la vascolarizzazione patologica del tumore originante dalle arterie di destra per l3 , l4 ed l5 , e un ramo ipertroco dellarteria sacrale media ( msa , frecce )  . 
in patients with repeat embolisation ( patients 9 , 15 , 17 , 19 , 21 , 22 and 26 ) , angiography showed no signicant pathological revascularisation or recanalisation of the previously occluded tumour vessels . all patients had variable pain relief . 
moderate pain relief ( 46 points in visual pain scale postembolisation ) was experienced by seven patients with spinal and sacral lesions ; these patients had 50% reduction of daily analgesic doses ( patients 5 , 15 , 29 , 33 , 38 , 40 and 43 )  . 
however , within the available follow - up , no patient had recurrent pain with the intensity of that before embolisation . all patients experienced ischaemic pain ( 810 points in visual pain scale ) at the site of embolisation , which was treated with analgesics and resolved completely the day after embolisation . 
six patients with advanced pelvic sarcomas experienced paraesthesias at the distribution of the sciatic nerve ; these patients were treated with methylprednisolone 1 g per day for 1 week , with complete symptom resolution within the week . discussion managing patients with advanced sarcomas is aimed at palliation . 
although we did not measure quality of life , we believe that pain relief is directly associated with improved quality of the remaining life of patients with advanced bone cancer . primary and metastatic bone cancers elicit osteolytic and osteoblastic reactions associated with incapacitating bone pain and pathological fractures [ 15 , 16 ]  . 
nei pazienti con embolizzazioni ripetute ( pazienti 9 , 15 , 17 , 19 , 21 , 22 e 26 ) langiograa non ha evidenziato rivascolarizzazione patologica o ricanalizzazione dei vasi tumorali precedentemente embolizzati . tutti i pazienti hanno avuto un sollievo dal dolore di grado variabile . 
moderata risoluzione del dolore ( 46 punti nella scala visiva post - embolizzazione ) stata ottenuta in 7 pazienti con lesioni del sacro e del rachide ; questi pazienti hanno ottenuto una riduzione maggiore del 50% della dose quotidiana di analgesici ( pazienti 5 , 15 , 29 , 33 , 38 , 40 e 43 )  . 
non siamo in grado di documentare la durata della risoluzione della sintomatologia dolorosa poich tutti i pazienti erano affetti da neoplasia in stadio terminale e sono deceduti a breve distanza dallembolizzazione . 
in ogni caso , nonostante i limiti del follow - up disponibile , nessun paziente ha avuto una recidiva del dolore di intensit pari a quella precedente lembolizzazione . tutti i pazienti hanno manifestato un dolore di natura ischemica ( 810 punti nella scala visiva del dolore ) nella sede dellembolizzazione che stato trattato con analgesici e si risolto completamente il giorno successivo alla procedura . 
sei pazienti con sarcoma pelvico in fase avanzata hanno riferito parestesie nel territorio di distribuzione del nervo sciatico ; questi pazienti sono stati trattati con 1 g di metilprednisolone al giorno per una settimana , con completa risoluzione dei sintomi entro una settimana . discussione la gestione dei pazienti con sarcoma in fase avanzata volta alla palliazione . 
nonostante non abbiamo rilevato la qualit di vita , crediamo che il sollievo dal dolore sia direttamente associato ad un miglioramento della qualit del resto della vita nei pazienti con tumori in fase avanzata . i tumori maligni dellosso , primitivi e metastatici , provocano reazioni osteolitiche ed osteoblastiche associate a dolori ossei invalidanti e fratture patologiche [ 15 , 16 ]  . 
il dolore dei tumori in fase avanzata descritto da moderato a severo in circa il 40%50% dei pazienti e da molto severo a straziante nel 25%30% dei pazienti [ 17 ]  . 
moreover , many cancer patients require opioid dose escalation to maintain adequate pain relief due to diminished analgesic effect with repeated opioid administration ( analgesic tolerance ) and / or advancement of the disease resulting in greater pain and therefore requiring more opioid [ 2123 ]  . 
additionally , prolonged opioid administration might exacerbate bone - cancer - induced pain in some patients and thus require supplemental pain medication to overcome both opioid and cancer - induced hyperalgesia and pain [ 2326 ]  . 
clinical studies have reported that opioids administered through different routes can unexpectedly produce hyperalgesia and allodynia , particularly during rapid opioid dose escalation , a phenomenon described as an emerging iatrogenic syndrome [ 27 . 
an experimental study in mice in which osteolytic sarcoma cells were injected and sealed into bone showed that sustained morphine administration through osmotic mini pumps ( 1 ) enhanced rather than alleviated sarcoma - induced spontaneous and evoked pain in a dose - dependent and naloxone - sensitive manner ; ( 2 ) increased expression of pronociceptive neural markers in the dorsal root ganglia ; ( 3 ) increased neural markers of cell damage in sarcoma , but not control , mice ; ( 4 ) increased osteoclastogenesis and incidence of spontaneous fracture in a dose - dependent and naloxone - sensitive manner . 
these data raise the possibility that maintaining cancer patients on sustained morphine might worsen rather than alleviate cancer - induced pain and accelerate cancer - induced bone loss in osteolytic cancers [ 23 ]  . 
isolated limb perfusion with tumour necrosis factor - alpha ( tnf - ) plus melphalan has also been used as a local conservative treatment for patients with advanced primary or recurrent soft tissue sarcomas [ 34 , 35 ]  . 
inoltre molti pazienti richiedono un progressivo aumento della dose per mantenere un adeguato controllo del dolore a causa della ridotta analgesia che si verica con la somministrazione ripetuta di oppioidi ( tolleranza analgesica ) e / o della progressione di malattia che provoca un aumento del dolore e , di conseguenza , unaumentata richiesta di oppioidi [ 2123 ]  . 
in pi la somministrazione prolungata di oppioidi in qualche paziente potrebbe esacerbare il dolore tumore - correlato e quindi richiedere farmaci supplementari per un miglior controllo del dolore e delliperalgesia cancro ed oppioidi - indotti [ 2326 ]  . 
studi clinici hanno riportato che la somministrazione di oppiodi attraverso differenti vie pu inaspettatamente provocare iperalgesia ed allodinia soprattutto durante la rapida riduzione della dose , fenomeno descritto come sindrome iatrogena emergente [ 27 ]  . 
agonisti non peptidici , come morna , ossimorna e fentanile , e peptidi che agiscono sui recettori per gli oppioidi , hanno dimostrato provocare iperalgesia [ 24 , 2931 ]  . 
questi dati svelano la possibilit che nei pazienti neoplastici il trattamento cronico con morna potrebbe peggiorare piuttosto che alleviare il dolore cancro - indotto e accelerare la perdita di osso nei tumori osteolitici [ 23 ]  . 
alla luce di ci dovrebbero essere incoraggiati trattamenti alternativi per lalleviamento del dolore . la radioterapia , la perfusione isolata dellarto , termoe crioablazione sono oggi impiegate nel trattamento dei sarcomi in fase avanzata . 
la radioterapia stata usata come trattamento palliativo combinato con la chemioterapia per gli osteosarcomi non resecabili e per le metastasi ossee multiple o dolorose non resecabili [ 32 , 33 ]  . 
la perfusione isolata dellarto con tumor necrosis factor - alfa ( tnf ) pi melfalan stata anche usata come trattamento conservativo locale nei pazienti con sarcomi in fase avanzata dei tessuti molli , primitivi o recidivanti [ 34 , 35 ]  . 
potrebbe anche indurre una signicativa risposta tumorale e permettere il salvataggio dellarto in alternativa allamputazione maggiore palliativa per i sarcomi ossei localmente in fase radiol med ( 2013 ) 118 : 13441359 1355 and allow limb salvage as an alternative to palliative major amputation for locally recurrent and advanced bone sarcomas without systemic spread [ 1 , 35 ]  . 
thermal ablation using ethanol , radiofrequency , laser , microwave , ultrasound or cryoablation is a palliative treatment to control tumours locally in patients who cannot tolerate a major surgical procedure because of multiple comorbidities or multiple metastatic lesions [ 36 ]  . 
the indications for thermal and cryoablation include painful lesions < 3 cm in diameter limited to one or two sites , slow - growing metastases and moderate or severe pa patients with lower pain scores or numerous painful lesions are not treated with ablation because this type of pain is better treated with a systemic rather than a local approach . 
moreover , tumours close to neurovascular bundles or the skin cannot be adequately ablated due to the risk of nerve and vascular injury or wound breakdown [ 37 ]  . 
 in contrast to cryoablation , radiofrequency energy poorly penetrates sclerotic bone ; therefore , radiofrequency ablation can be used for lung metastases but not for osteoblastic bone metastases [ 3741 ]  . 
 in surgically complex cases , angiography may accurately determine tumour vascular mapping and haemodynamic status and assist in surgical planning by showing vascular displacement that occurs in the anatomic region with a large soft tissue component [ 8 , 42 ]  . 
angiography can also assist in estimating tumour response to induction chemotherapy [ 43 ] ; complete disappearance of tumour vascularity after preoperative chemotherapy correlates with a good treatment response [ 43 , 44 ]  . 
subsequently , primary or serial embolisation has been used for to control tumour growth most commonly for bone metastases from various carcinomas , benign bone tumours such as giant cell tumours and aneurysmal bone cysts and , rarely , for palliative treatment of bone sarcomas [ 4548 ]  . 
a therapeutic alternative or complementary treatment for local control of locally advanced sarcomas , sarcomas with too many bone metastases to easily resect and pelvic or axial sarcomas with lung metastases [ 5 , 46 ]  . chemoembolisation consisting of direct chemotherapeutic agent administration into the tumour through selective avanzata senza diffusione sistemica [ 1 , 35 ]  . 
la termoablazione con etanolo , radiofrequenze , laser , microonde , ultrasuoni o la crioablazione sono un trattamento palliativo per il controllo locale del tumore in pazienti che non potrebbero tollerare un intervento chirurgico maggiore a causa di comorbilit o lesioni metastatiche multiple [ 36 ]  . 
 le indicazioni alla termoe crioablazione includono lesioni dolorose inferiori ai 3 cm di diametro , limitate ad uno o due siti , metastasi a lenta crescita e dolore da moderato a severo . 
i pazienti con dolore di grado inferiore o con numerose lesioni dolorose non vengono trattati con lablazione poich questo tipo di dolore risponde meglio ad un approccio sistemico pi che locale . 
inoltre , le lesioni in prossimit dei fasci neurovascolari o della cute non possono essere adeguatamente ablate a causa del rischio di lesioni nervose e vascolari o di deiscenza della ferita [ 37 ]  . 
al contrario della crioablazione , lenergia delle radiofrequenze penetra poco nellosso sclerotico ; pertanto questo tipo di ablazione pu essere utilizzata nelle metastasi polmonari ma non nelle lesioni ossee osteblastiche [ 3741 ]  . nei casi chirurgici complessi langiograa potrebe essere in grado di determinare accuratamente la mappa vascolare e lo stato emodinamico del tumore , ed aiutare cos la pianicazione chirurgica mostrando il decorso vascolare in regioni anatomiche ricche di componenti tissutali molli [ 8 , 42 ]  . 
langiograa pu inoltre essere daiuto nella valutazione della risposta tumorale alla chemioterapia dinduzione [ 43 ] ; la completa scomparsa della vascolarizzazione tumorale dopo la chemioterapia preoperatoria correlata ad una buona risposta al trattamento [ 43 , 44 ]  . 
in oncologia , lembolizzazione adiuvante stata utilizzata per la riduzione delle dimensione dei tumori in vista dellintervento chirurgico , per facilitare il controllo del sanguinamento intraoperatorio , per il trattamento delle complicanze emorragiche e per la riduzione del dolore . 
successivamente , una o ripetute embolizzazioni sono state utilizzate per il controllo della crescita tumorale soprattutto nelle metastasi ossee di vari carcinomi , nei tumori ossei benigni come i tumori a cellule giganti e le cisti aneurismatiche dellosso , e , raramente , nel trattamento palliativo dei sarcomi ossei [ 4548 ]  . 
come alternativa terapeutica o trattamento complementare nel controllo locale di sarcomi localmente in fase avanzata , sarcomi con troppe metastasi ossee per poter essere facilmente resecati e sarcomi pelvici o assiali con metastasi polmonari [ 5 , 46 ]  . 
 anche la chemioembolizzazione consistente nella somministrazione di agenti chemioterapici allinterno della neoplasia attraverso la cateterizzazione selettiva dei vasi afferenti , seguita dallembolizzazione convenzionale con 1356 radiol med ( 2013 ) 118 : 13441359 catheterisation of feeding vessels , followed by conventional embolisation with an embolic agent , has also been reported for neoadjuvant chemotherapy , inducing tumour necrosis without major complications [ 44 , 46 , 4951 ]  . 
tumour devascularisation was accomplished with embolisation , as evidenced by postembolisation angiography and postoperative histology showing large areas of necrosis in 70.2%94.2% of tumour specimens [ 44 , 51 ]  . 
 complications included some exacerbation of local pain during and immediately after embolisation that was treated with opioids and resolved completely , local skin redness , swelling , burning sensation and a blister - like change in the skin that was relieved after symptomatic treatment , and mild postembolisation syndrome [ 44 ]  . 
 by selective and superselective occlusion of the pathological tumour vessels , arterial ow is obstructed , resulting in pain reduction , tumour necrosis and tumour size reduction [ 47 , 49 ]  . 
pain reduction is considered to be related to periosteum decompression , with or without tumour volume reduction , and suppressed nociceptor activation by reducing algesic chemical production [ 52 , 53 ]  . pain relief occurs at 12 h to several days after embolisation , usually within 1 week [ 53 ]  . 
 although we acknowledge that embolisation cannot be considered as rst - line treatment for cancer patients with un agente embolico , stata riportata come chemioterapia neoadiuvante poich induce la necrosi tumorale in assenza di complicanze maggiori [ 44 , 46 , 4951 ]  . 
la devascolarizzazione tumorale stata realizzata mediante embolizzazione , come dimostrato dallangiograa post - procedurale e dallistologia post - operatoria che ha evidenziato la presenza di estese aree necrotiche nel 70 , 2%94 , 2% dei campioni tumorali [ 44 , 51 ]  . 
 le complicanze includono lesacerbazione di dolore locale durante e subito dopo lembolizzazione che , trattato con oppioidi , si completamente risolto , arrossamento cutaneo locale , tumefazione , sensazione di bruciore , comparsa di vescicole cutanee risoltesi dopo trattamento sintomatico e sindrome postembolizzazione di media intensit [ 44 ]  . 
 come la nostra serie di pazienti ha dimostrato , i sarcomi dellosso sono tumori ipervascolari con estesa neovascolarizzazione e quindi si impregnano durante langiograa con mezzo di contrasto [ 44 , 51 ]  . 
con locclusione selettiva e superselettiva dei vasi tumorali patologici , il usso arterioso al tumore interrotto con riduzione del dolore , necrosi tumorale e riduzione delle dimensioni della neoplasia [ 47 , 49 ]  . 
la riduzione del dolore ritenuta essere correlata alla decompressione del periostio con o senza diminuzione del volume tumorale , e la soppressione dellattivazione dei nocicettori che risulta in una ridotta produzione di mediatori chimici dellalgesia [ 52 , 53 ]  . il sollievo dal dolore si verica da 12 ore a qualche giorno dopo lembolizzazione , di solito entro una settimana [ 53 ]  . 
 anche se sappiamo che lembolizzazione non pu essere considerata il trattamento di prima linea nei pazienti con radiol med ( 2013 ) 118 : 13441359 1357 bone sarcomas because of the available documented treatment options , it would be interesting to evaluate the role of embolisation for pain relief and tumour necrosis in a series of bone sarcoma patients with longer expected survival . considerations for choosing an embolic agent are delivery speed and reliability , occlusive effect duration , normal tissue preservation and operator experience . 
currently available embolic agents include gelfoam , polyvinyl alcohol ( pva ) particles , liquid ( absolute alcohol ) , coils , tissue adhesives , ethanol , microbrillar collagen and autologous blood clot [ 47 , 52 , 54 ]  . 
their advantages include compressibility , allowing easy passage through a microcatheter with a luminal diameter smaller than that of the spheres and more uniform in size than pva , and the particle size does not changed in liquids [ 52 ]  . 
gelatine sponge is dissolvable material that comes in small , at , rectangular blocks that can be cut with scissors into elongated rectangles and rolled into pledgets , which can then be injected by catheters or microcatheters . 
liquid embolic agents , including absolute alcohol , nbca , ethibloc ( ethicon , norderstedt , germany ) , sodium tetradecyl sulphate and onyx ( microtherapeutics , irvine , ca , usa ) offer advantages of low viscosity for easy injection through small catheters or catheters with many bends through tortuous blood vessels [ 47 , 54 ]  . 
although nbca can pass through bent catheters navigating tortuous blood vessels , it does not permeate all the way to the capillary level and therefore does not cause tissue death . 
in our practice and in this study , nbca was the preferred embolic agent because we consider it the most appropriate embolic agent for controlled and permanent occlusion of the tumour vessels and tumour devascularisation , without any complications . sarcomi dellosso a causa delle valide alternative disponibili documentate , potrebbe essere interessante valutare il ruolo dellembolizzazione nella gestione del dolore e della necrosi tumorale in una serie di pazienti affetti da sarcomi dellosso con unaspettativa di vita maggiore . le considerazioni da fare per la scelta dellagente embolizzante sono la velocit e lafdabilit nel raggiungimento del sito da trattare , la durata delleffetto occludente , la preservazione del tessuto sano e lesperienza delloperatore . 
 attualmente gli agenti embolici disponibili includono gelfoam , particelle di alcool polivinilico ( pva ) , liquidi ( alcool puro ) , bobine , sostanze adesive tissutali , etanolo , collagene microbrillare e coaguli di sangue autologo [ 47 , 52 , 54 ]  . 
i vantaggi del loro uso includono il fatto che sono compressibili permettendone il passagio attraverso un microcatetere con lume di diametro pi piccolo rispetto a quello delle sfere , di dimensioni pi uniformi che il pva , e le dimensioni delle particelle non cambiano a contatto con i liquidi [ 52 ]  . 
la spugna di gelatina un materiale degradabile simile alla spugna che si presenta sotto forma di piccoli blocchi piatti rettangolari che possono essere tagliati con le forbici in rettangoli allungati e arrotolati in tamponi che vengono successivamente iniettati attraverso cateteri o microcateteri . 
una volta che la stasi del usso arterioso , completa o parziale , stata ottenuta con la spugna di gelatina , alcuni radiologi interventivi utilizzano le spirali per la completa occlusione del vaso [ 52 ]  . 
agenti embolizzanti liquidi , inclusi alcool puro , nbca , ethibloc ( ethicon , norderstedt , germania ) , sodio tetradecil solfato e onyx ( microtherapeutics , irvine , california ) , offrono il vantaggio di una viscosit inferiore per uniniezione pi facile attraverso cateteri piccoli o con diverse curve per vasi toruosi [ 47 , 54 ]  . 
anche se lnbca passa attraverso le curvature dei cateteri in vasi tortuosi , non in grado di permeare attraverso lalbero capillare , motivo per cui non in grado di provocare la morte tissutale . 
nella nostra esperienza , e in questo studio , lnbca stato preferito come agente embolizzante poich da noi considerato il pi appropriato per locclusione embolica controllata e permanente dei vasi tumorali e per la devascolarizzazione neoplastica , in assenza di complicanze . 1358 conclusions radiol med ( 2013 ) 118 : 13441359 conclusioni selective embolisation is a safe and effective local palliative treatment for patients with locally advanced sarcomas . 
 although current experience is limited , embolisation can provide optimum pain relief and improve the quality of the remaining life of these patients by offering the least discomfort with the minimum possible complications . lembolizzazione selettiva una metodica sicura ed efcace nel trattamento palliativo locale dei pazienti affetti da sarcoma in fase avanzata . 
anche se lesperienza attuale limitata , lembolizzazione pu garantire unottima risoluzione della sintomatologia dolorosa ed un miglioramento della qualit di vita rimanente offrendo ai pazienti il minor disagio e le minori complicanze possibili . 
ruggieri2 1department of interventional angiographic radiology , istituto ortopedico rizzoli , bologna , italy 2department of orthopedics , istituto ortopedico rizzoli , university of bologna , bologna , italy 3department of radiology , istituto ortopedico rizzoli , bologna , italy correspondence to : p . 
ruggieri , orthopaedic oncology service , department of orthopaedics , istituto ortopedico rizzoli , university of bologna , via di barbiano 1 / 10 , 40136 bologna , italy , tel . : + 39 - 051 - 6366460 , fax : + 39 - 051 - 6366540 , e - mail : pietro.ruggieri@ior.it received : 11 may 2011 / accepted : 3 august 2011 / published online : 19 march 2012 springer - verlag 2012 abstract purpose . 
we retrospectively studied 107 patients with bone metastases from renal cell carcinoma treated from december 2002 to january 2011 with 163 embolisations using n - 2 - butyl cyanoacrylate ( nbca )  . 
mean maximal tumour diameter after embolisation was 4.0 cone patient had intraprocedural tear of the left l3 artery and iliopsoas haemorrhage and was treated with occlusion of the bleeding vessel with nbca . 
abbiamo studiato retrospettivamente 107 pazienti con metastasi da carcinoma renale trattati con 163 embolizzazioni con n - 2 - butil ciano - acrilato ( nbca ) da dicembre 2002 a gennaio 2011 . 
la media dei diametri tumorali dopo lembolizzazione stata di 4 , 0 cun paziente ha riportato , durante la procedura , una lesione dellarteria sinistra di l3 ed emorragia nellileo - psoas , stato trattato con occlusione del vaso sanguinante con nbca . 
dopo la procedura sono stati diagnosticati 15 casi ( 9 , 2% ) di sindrome post292 radiol med ( 2013 ) 118 : 291302 as primary or palliative treatment of bone metastases from renal cell carcinoma . 
una rigorosa aderenza ai principi di embolizzazione attraverso catetere importante per evitare complicazioni . parole chiave embolizzazione selettiva nbca metastasi ossee carcinoma a cellule renali introduction introduzione bone metastases are estimated to occur in 3045% of patients with renal cell or thyroid carcinoma , which are by far the most often embolised bone metastases reported in the interventional literature [ 111 ]  . 
this may cause technical difculties with respect to the extent of surgery and primary stability for pain relief [ 1 , 17 , 18 ] , as adequate surgical procedures are associated with substantial blood loss [ 24 , 17 ]  . embolisation has an important role in treating hypervascular bone metastases [ 4 ]  . 
embolisation with the most appropriate embolic agent can provide pain relief and tumour size reduction in up to 90% of cases ; multiple procedures are frequently necessary [ 1 , 19 , 20 ]  . 
it is typically performed in 4to 6 - week intervals until symptomatic improvement occurs or tumour vascularity disappears , as judged by angiography , magnetic resonance imaging ( mri ) , or computed tomography ( ct ) scan . 
however , if wide resection is planned , there is no indication for preoperative embolisation because it would lead to marked hypervascularity in the area surrounding the tumour , which would result in heavy bleeding during surgery [ 4 , 5 ]  . nei pazienti con carcinoma renale o della tiroide lincidenza delle metastasi ossee stimata attorno al 30%40% , tali metastasi sono riportate essere quelle pi frequentemente sottoposte ad embolizzazione nella letteratura interventistica [ 111 ]  . 
 ci pu essere causa di difcolt tecniche rispetto allestensione della resezione e allottenimento di stabilizzazione primaria per la riduzione del dolore [ 1 , 17 , 18 ] , inoltre unadeguata procedura chirurgica associata ad unimportante perdita ematica [ 24 , 17 ]  . lembolizzazione ha unimportante ruolo nel trattamento di metastasi ipervascolarizzate [ 4 ]  . 
lembolizzazione , eseguita con il pi appropriato agente embolizzante , pu determinare una riduzione del dolore e la riduzione della dimensione tumorale in pi del 90% dei casi ; procedure multiple sono spesso necessarie [ 1 , 19 , 20 ]  . 
questo tipicamente raggiunto in un periodo di 46 settimane prima che i miglioramenti sintomatici si verichino o la riduzione della vascolarizzazione del tumore diventi manifesta allangiograa , alla risonanza magnetica ( rm ) ed alla tomograa computerizzata ( tc )  . 
lembolizzazione preoperatoria determina devascolarizzazione del tumore , controllo dellemorragia e riduzione delle perdite ematiche intraoperatorie facilitando il curettage della lesione [ 9 ] ; tiradiol med ( 2013 ) 118 : 291302 compared with the amount of information on the effects of surgical and medical treatments , few data exist concerning embolisation of bone metastases [ 1 , 2 , 4 , 9 , 10 , 17 ]  . 
the aim of this study was to report on selective embolisation for palliative and / or adjuvant treatment of bone metastases from renal cell carcinoma and discuss clinical and imaging results . patients and methods we retrospectively studied the les of 107 patients with bone metastases from renal cell carcinoma treated by selective transfemoral embolisation using n - 2 - butyl cyanoacrylate ( nbca ) during an 8 - year period , from december 2002 to january 2011 . 
this study was approved by the institutional review board / ethics committee of the authors institution . under local anaesthesia using the seldinger technique through femoral artery catheterisation , diagnostic digital subtraction angiography ( dsa ) ( contrast medium iomeprol 300 mg / ml , iomeron , bracco , milan , italy and iohexol 350 mg / ml , omnipaque , ge healthcare , mississauga , on , canada ) was performed before the embolisation to identify feeding vessels . 
 the femoral artery was catheterised with a 4 ( cordis corporation , miami , fl , usa ) or 5 - french ( terumo corporation , tokyo , japan ) introducer . 
flexible and stiff guidewires were picamente la chirurgia dovrebbe essere effettuata fra le 24 e le 48 ore dopo lembolizzazione allo scopo di prevenire la ricanalizzazione [ 3 , 4 ]  . 
se invece stata programmata una resezione ampia , non c indicazione allembolizzazione preoperatoria perch potrebbe determinare marcata ipervascolarizzazione dellarea attorno al tumore che potrebbe determinare pesanti perdite ematiche durante lintervento chirurgico [ 4 , 5 ]  . 
 a confronto con tutte le informazioni sugli effetti dei trattamenti chirurgici e medici esistono pochi dati riguardo lembolizzazione delle metastasi [ 1 , 2 , 4 , 9 , 10 , 17 ] e addirittura molti meno riguardo lembolizzazione delle metastasi ossee da carcinoma renale [ 111 , 2024 ]  . 
 materiali e metodi abbiamo studiato retrospettivamente i dati relativi a 107 pazienti con metastasi ossee da carcinoma renale trattati con embolizzazione selettiva transfemorale con lutilizzo di n - 2 - butil ciano - acrilato ( nbca ) in un periodo di 8 anni , da dicembre 2002 a gennaio 2011 . 
questo studio stato approvato dallinstitutional review board / comitato etico dellistituto di appartenenza degli autori . preliminarmente allembolizzazione con tecnica seldinger , sotto anestesia locale e attraverso la cateterizzazione dellarteria femorale , stata eseguita langiograa diagnostica digitale di sottrazione ( mezzo di contrasto : iomeprol 300 mg / ml , iomeron , bracco , milano , italia ; iohexol 350 mg / ml , omnipaque , ge healthcare , mississauga , on , canada ) per identicare i vasi nutritizi . 
from the mixture , 1 ml was aspirated in an insulin ( 1 - ml ) syringe ; depending on the pathological vasculature , 0.10.2 ml of the aspirate mixture was injected , sandwiched with 2 + 2 ml of 5% glucosate solution under uoroscopic control . 
if more than 1 acon ( 1 ml ) of nbca was necessary because of high vascularisation of the lesions , a new mixture was prepared in a similar manner , overall , 0.52 ml of nbca was used for each embolisation . 
 clinical and imaging effects of treatment were evaluated every 2 months for the rst 6 months , every 3 months for the next 6 months , every 6 months thereafter for 3 years and then annually . 
the clinical effect was determined by pain evaluation using a 0 to 10 - point visual pain scale from 0 ( no pain ) to 10 ( severe and constant pain ) [ 25 ] and the use of analgesics , including acetaminophen , nonsteroidal anti - inammatory drugs and narcotics . 
a clinical response was achieved in 157 of the 163 embolisations ( 96% ) ; no response was achieved in six embolisations of pelvic and sacral bone metastases ( sacroiliac lesions )  . 
mean duration of pain restata cateterizzata con lausilio di un 4 french introducer ( cordis corporation , miami , fl , usa ) o di un 5 french introducer ( terumo corporation , tokyo , giappone )  . 
inoltre , nei pazienti con metastasi vertebrali e pelviche , stata eseguita unaortograa panoramica con lausilio di un 4 french pigtail catheters ( cordis corporation ) , seguita da unarteriograa superselettiva con lausilio di cateteri cobra , simmons e vertebral ( terumo corporation , tokyo , giappone ) o 2 , 72 , 9 french progreat pre - shaped , 130 cm microcateteri ( coaxial catheters system , terumo corporation , tokyo , giappone )  . 
sono state utilizzate tipologie di guide sia essibile che rigide , con un diametro di 0 , 035 ( 0 , 89 mm ) , una lunghezza di 150 cm e 180 cm con un tip essibile di 3 cm ( radifocus guide wire m , terumo corporation , tokyo , gaippone )  . 
in tutti i pazienti , lagente embolizzante utilizzato stato il nbca ( glubran 2 , gem , viareggio , italia ) in 33% lipiodol ( lipiodol ultrauido , guerber s.p.a. , francia ) sandwiched con glucosata al 5% . 
per la miscela , 1 ml stato aspirato in una siringa da insulina ( 1 ml ) ; a seconda della vascolarizzazione patologica , 0 , 10 , 2 ml della miscela aspirata stata iniettata sandwiched con 2 + 2 ml di soluzione glucosata al 5% sotto controllo uoroscopico . 
nel caso in cui pi di 1 acone ( 1 ml ) di nbca fosse stato necessario a causa della ricca vascolarizzazione della metastasi stata preparata una nuova miscela in modo simile . 
 gli effetti clinico - radiologici del trattamento sono stati valutati ogni 2 mesi per i primi 6 mesi , ogni 3 per i successivi 6 mesi , ogni 6 mesi per i successivi 3 anni e poi annualmente . 
gli effetti clinici sono stati determinati dalla valutazione del dolore con lausilio di un indicatore visivo di dolore ( 010 ) con scala da 0 ( nessun dolore ) a 10 ( dolore intenso e costante ) [ 25 ] e dalleventuale uso di analgesici , incluso lacetaminofene , anti - inammatori non steroidei ( fans ) e narcotici . 
una risposta clinica stata denita da una riduzione di almeno il 50% del dolore e la riduzione di almeno il 50% delle dosi di analgesici mentre la non risposta stata denita come una riduzione minore del 50% . 
una risposta clinica stata ottenuta in 157 delle 163 embolizzazioni ( 96% ) ; nessuna risposta stata ottenuta in 6 embolizzazioni di metastasi delle pelvi e del sacro ( metastasi della sacro - iliaca )  . 
un sollievo quasi completo dal dolore stato ( punteggio di 03 nella scala di indicatore visivo dopo lembolizzazione ) e riduzione della dose giornaliera di analgesici maggiore del 50% si sono vericati nei pazienti con dolore pi severo prima della procedura ( punteggio di 710 nella scala di indicatori visivi prima dellembolizzazione ) , come nei pazienti con metastasi alle estremit o al cingolo scapolare . 
una riduzione moderata del dolore ( punteggio di 46 nella scala di indicatore visivo dopo lembolizzazione ) e riduzione della dose giornaliera di analgesico del 50% si sono vericati nei pazienti con metastasi vertebrali ( punteggio di 58 nella scala di indicatore visivo prima dellembolizzazione )  . 
la recidiva di dolore stata sempre di 34 punti inferiore nella scala di indicatore visivo rispetto al punteggio precedentemente allembolizzazione . aree di ipoattenuazione , quale indice di necrosi , sono state osservate in tutti i pazienti . 
i migliori risultati radiologici in termini di ipoattenuazione e riduzione della massa tumorale sono stati ottenuti nelle metastasi che apparivano altamente vascolarizzate e destruenti rispettivamente allangiograa ed alla tc preliminari e nelle metastasi del cingolo scapolare . 
ossicazioni abbondanti si sono vericate in 6 pazienti ; in questi pazienti non stata osservata una progressione locale della metastasi nelle valutazioni radiologiche durante il follow - up . una complicanza intraprocedurale maggiore si vericata in un paziente con metastasi vertebrale al rachide lombare . 
almost complete pain relief ( 03 points on visual pain scale postembolisation ) and > 50% reduction of analgesic daily doses occurred in all patients with severe pain prior to the procedure ( 710 points on visual pain scale pre - embolisation ) , such as patients with extremity and shoulder - girdle lesions . 
moderate pain relief ( 46 points on visual pain scale postembolisation ) and 50% reduction of analgesics daily doses was observed in patients with spinal lesions ( 58 points on visual pain scale pre - embolisation )  . 
mean maximal tumour diameter after embolisation was 4.0 ( range 210 ) cthe best imaging response in terms of hypoattenuation and tumour size reduction were observed in highly destructive and hypervascular metastatic lesions as observed in preprocedural ct scan and angiography respectively , and lesions of the shoulder girdle . 
2a anteroposterior radiograph of the pelvis of a 72 - year - old man with a painful supra - acetabular bone metastasis from renal cell carcinoma ( arrows )  . 
b dsa shows pathological vascularisation originating from branches of the right superior gluteal artery ( arrow 1 ) and the obturator artery ( arrow 2 ) , and a hypertrophied branch originating from the deep femoral artery ( arrow 3 )  . 
b larteriograa digitale di sottrazione mostra la vascolarizzazione patologica che origina dai rami dellarteria glutea superiore destra ( freccia 1 ) e dellarteria otturatoria ( freccia 2 ) , ed un ramo ipertroco originato dallarteria femorale profonda ( freccia 3 )  . 
3a digital subtraction arteriography of the left lower extremity of a 72 - year - old man with a painful bone metastasis of the left femur from renal cell carcinoma shows intramedullary pathological vascularisation suggestive of intramedullary metastasis ( arrows )  . 
b selective catheterisation through a perforating nutrient artery ( arrow 1 ) shows the intramedullary metastasis ( arrows 2 ) and increased pathological vascularisation at the site of the osteolysis ( arrow 3 )  . 
3a arteriograa digitale di sottrazione dellarto inferiore sinistro di un paziente di 72 anni con una dolorosa metastasi al femore sinistro mostra vascolarizzazione patologica endomidollare , suggestiva di metastasi endomidollare ( frecce )  . 
b la cateterizzazione selettiva attraverso arteria nutritizia perforante ( freccia 1 ) mostra la metastasi endomidollare ( freccia 2 ) e laumentata vascolarizzazione patologica nella sede dellosteolisi ( freccia 3 )  . 
4a anteroposterior radiograph of the left hip of a 60 - year - old man with a painful bone metastasis from renal cell carcinoma at the lesser trochanter ( arrows )  . 
b early ( left ) and late ( right ) phase dsa after selective catheterisation through the deep femoral artery shows the pathological vascularisation originating from the lateral femoral circumex artery ( arrow 1 ) and a segmental branch of the deep femoral artery ( arrow 2 )  . 
b le fasi precoce ( sinistra ) e tardiva ( destra ) dellarteriograa digitale di sottrazione dopo cateterizzazione selettiva attraverso la larteria femorale profonda mostrano la vascolarizzazione patologica originata dallarteria circonessa femorale laterale ( freccia 1 ) ed un ramo segmentario dellarteria femorale profonda ( freccia 2 )  . 
d la radiograa antero - posteriore dellanca sinistra 12 mesi dopo lembolizazione mostra una lesione metastatica stabile con alcune ossicazioni ( frecce )  . table 1 number and site of repeat embolisations performed in the 23 patients with recurrent pain and tumour progression patients with repeat embolisations ( n ) 2 embolizations 3 embolizations 4 embolizations 5 embolizations site of repeat embolisations pelvis spine femur thoracic cage humerus pelvi vertebre femore gabbia toracica omero tabella 1 numero e sede delle embolizzazioni ripetute realizzate in 23 pazienti con dolore recidivato e progressione del tumore sede delle embolizzazioni ripetute pazienti con embolizzazioni ripetute ( n ) 2 embolizzazioni 3 embolizzazioni 4 embolizzazioni 5 embolizzazioni 298 radiol med ( 2013 ) 118 : 291302 fig . 
5a dsa shows intraprocedural tear of the left l3 artery ( arrow 1 ) and extravasation of contrast medium into the iliopsoas muscle ( arrows 2 ) in a 48 - year - old man with sacral bone metastasis from renal cell carcinoma ( arrow 3 )  . 
5a laortograa digitale di sottrazione mostra la lesione intraprocedurale dellarteria sinistra di l3 ( freccia 1 ) e stravaso del mezzo di contrasto nel muscolo ileo - psoas ( freccia 2 ) in un uomo di 48 anni con metastasi sacrale da carcinoma renale ( freccia 3 )  . 
abundant ossication was seen in six patients ; in these patients , metastatic lesion progression was not observed at follow - up imaging evaluation . one intraprocedural major complication occurred in one patient with lumbar spine metastasis . 
paraesthesias in the lower extremities were observed after 25 embolisations ( 25% ) of pelvis and sacrum metastatic lesions ; these patients were treated with methylprednisolone administration 1 g / day for 1 week , and all recovered completely within a week . discussion renal cell carcinoma is typically a hypervascular tumour [ 3 ]  . 
selective transcatheter embolisation offers a rational therapeutic approach for pain relief as an important and efcacious adjunct in managing patients with hypervascular renal cell bone metastases [ 3 ]  . 
la sindrome da post - embolizzazione , che si manifesta con febbre o brividi , nausea , vomito , ed un aumento del dolore ischemico nel sito di embolizzazione stata diagnosticata dopo 15 procedure ( 9 , 2% )  . 
parestesie alle estremit inferiori si sono vericate dopo 25 embolizzazioni ( 25% ) di metastasi delle pelvi e del sacro ; questi pazienti sono stati trattati con successo con 1 g di metilprednisone al giorno per una settimana . 
lembolizzazione selettiva trans - catetere offre un razionale approccio terapeutico per la riduzione del dolore , intesa come importante ed efcace parte della gestione del paziente con metastasi ossee ipervascolarizzate da carcinoma renale [ 3 ]  . 
lembolizzazione preoperatoria stata applicata sia al tumore primitivo preliminarmente alla nefrectomia [ 21 , 23 ] sia alle metastasi per limitare le perdite ematiche intraoperatorie [ 1 , 2 , 4 , 22 ] , combinata con chemioterapia e radioterapia [ 3 , 26 , 27 ]  . 
lembolizzazione stata efcacie nel ridurre il dolore nel 96% delle proradiol med ( 2013 ) 118 : 291302 [ 21 , 23 ] and to metastatic bone lesions to limit intraoperative blood loss [ 1 , 2 , 4 , 22 ] and combined with radiation and chemotherapy [ 3 , 26 , 27 ]  . 
therefore , it can be questioned whether the additional treatments contributed to the success of embolisation or even that the success of embolisation may be entirely attributable to these treatments . 
third , we did not evaluate the effect of embolisation on survival ; however , in line with the literature [ 17 ] , life expectancy is not inuenced by embolisation therapy , and embolisation does not appear to improve survival . 
this is not surprising , because embolisation only targets a portion of the tumour burden . case reports and small series have previously documented the role of embolisation for bone metastases from renal cell carcinoma [ 111 , 2024 ] using mostly a combination of gelfoam and metallic coils [ 9 , 20 ]  . 
lesions that did not respond to embolisation were in varied anatomical distributions , including the chest wall , pelvis and lower extremity , and were not clustered in any single region . 
complications included lowerextremity paralysis after embolisation at the l1 vertebral body , pulmonary embolism after embolisation at the t1 vertebral body and transient paralysis of the sciatic nerve after embolisation of a right ilium metastasis . 
per primo , il presente studio ha carattere retrospettivo , per quanto nei pazienti oncologici uno studio prospettico risulta essere di difcile esecuzione , studi istituzionali ben controllati risultano molto utili per valutare lefcacia dei trattamenti . 
terzo , non stato valutato leffetto dellembolizzazione sulla sopravvivenza ; comunque , in linea con la letteratura [ 17 ] , laspettativa di vita non sembra essere inuenzata dallembolizzazione e questultima non sembra migliorare la sopravvivenza . 
 case report e piccoli studi hanno precedentemente documentato il ruolo dellembolizzazione nel trattamento delle metastasi da carcinoma renale [ 111 , 2024 ] , prevalentemente usando una combinazione di gelfoam e spirali metalliche [ 9 , 20 ]  . 
questi studi hanno denito alcuni principi dellembolizzazione nellapplicazione ai carcinomi renali , riguardo al successo tecnico , alla sicurezza , agli effetti clinici ed avversi ed alla ripetibilit [ 6 ]  . 
uno studio ha riportato una casistica di 21 pazienti in cui sono state eseguite 30 embolizzazioni per 39 metastasi , usando come agente embolizzante lalcol polivinilico [ 3 ]  . 
le complicazioni includevano la paralisi degli arti inferiori dopo embolizzazione di una metastasi al soma di l1 , embolia polmonare a seguito dellembolizzazione del soma di t1 e una paralisi transitoria del nervo sciatico dopo embolizzazione di metastasi allileo . 
dal confronto fra i risultati del precedente studio e quelli ottenuti nel presente possiamo concludere che le metastasi da carcinoma renale sono associate ad una migliore e pi duratura riduzione del 300 radiol med ( 2013 ) 118 : 291302 carcinoma metastases are associated with better and longer duration of pain relief and higher reduction of tumour size and ossication compared with bone metastases from other cancers . 
based on these results , we believe that the most important factor for embolisation of bone metastases is lesion vascularity rather than tumour size , and we recommend embolisation for bone metastases from renal cell carcinoma . the result of an embolisation procedure partly depends on the specic characteristics of the embolic agent : composition , size , interaction between with the vessel wall , speed and reliability of delivery , duration of occlusive effect and preservation of normal tissue all help to determine the level of vascular occlusion [ 1 , 3 , 26 , 27 , 30 ]  . 
 in our practice and in this study , nbca was the preferred embolic agent because we consider it the most appropriate agent for control and permanent occlusion of the target vessels and for tumour devascularisation . 
technical complications such as embolisation material choking the catheter , the catheter becoming stuck to the wall of the vessel , unintentional reux of embolisation material , and coils perforating the vessel wall have been reported in up to 25% of patients undergoing embolisation of bone metastases [ 4 , 11 ]  . 
embolisation of adjacent or distant nontargeted vessels can result in normal tissue loss and may be associated with nerve palsy , skin breakdown and subcutaneous or muscle necrosis and infection [ 1 , 3 , 26 , 31 ]  . 
during pelvic embolisations , ischaemic neuropathies of the sciatic and femoral nerves may occur dolore , ad una pi alta riduzione del volume tumorale ed ad un maggior numero di ossicazioni rispetto a metastasi da altri istotipi . 
basandoci su questi risultati , crediamo che il miglior parametro per predire il risultato clinico - radiologico dellembolizzazione sia la vascolarizzazione della lesione piuttosto che le dimensioni , si raccomanda quindi lembolizzazione nel trattamento delle metastasi da carcinoma renale . il risultato dellembolizzazione dipende parzialmente dal tipo di agente embolizzante . 
la composizione e le dimensioni , la velocit e lafdabilit , linterazione con i vasi , la durata dellocclusione , la preservazione del tessuto normale sono tutti fattori che determinano il livello di occlusione vascolare [ 1 , 3 , 26 , 27 , 30 ]  . 
gelfoam , alcol polivinilico ( pva ) , particelle , liquidi , spirali metalliche , adesivi tissutali , collagene microbrillare e coauguli di sangue autologo sono stati usati come agenti embolizzanti [ 30 ]  . 
la somministrazione in bolo di piccole dosi di nbca ( 0 , 10 , 2 ml ) sandwiched sotto controllo uoroscopico , guidato dallarteriograa , permette una procedura sicura ed afdabile . 
nella nostra pratica e nel presente studio , lnbca lagente embolizzante preferito perch lo consideriamo dotato di maggior appropriatezza per locclusione permanente e controllata dei vasi bersaglio e dunque per la devascolarizzazione tumorale . 
le complicazioni tecniche come lostruzione del catetere da parte delle sostanze embolizzanti , il blocco del catetere nel vaso , il reusso involontario dellagente embolizzante , la perforazione della parete vasale dalle spirali metalliche sono stati riportati come superiori al 25% nei pazienti sottoposti a tale procedura [ 4 , 11 ]  . 
lembolizzazione di vasi non bersaglio adiacenti o a distanza pu risultare in paralisi nervosa , necrosi cutanea , sottocutanea , dei muscoli o infezione [ 1 , 3 , 26 , 31 ]  . 
in the future , specic systemic treatment modalities for cancer patients with bone metastases may be safer and more effective for palliation , and possibly improve survival . ischemiche dei nervi femorale e sciatico se vengono occlusi vasi nervosi [ 31 ]  . 
salvatore2 1institute of biostructure and bioimage , national council of research ( cnr ) , federico ii university school of medicine , via pansini 5 , edicio 10 , 80131 naples , italy 2department of biomorphological and functional science . 
the study population comprised ten smoker ( 7 / 3 m / w , age 4276 years ) and 16 nonsmoker ( 8 / 8 men / women , age 4780 years ) diabetic patients . 
 the anklebrachial index ( abi ) was determined , and colour doppler ultrasound ( cdus ) of the lower legs was performed to determine the presence of peripheral arteriopathy disease ( pad )  . 
sono entrati a far parte dello studio 10 pazienti diabetici fumatori ( 7 / 3 maschi / femmine , et 4276 anni ) e 16 diabetici non fumatori ( 8 / 8 maschi / femmine ; et 4780 anni )  . 
la presenza e la gravit della arteriopatia obliterante degli arti inferiori ( pad ) stata valutata con misurazione delle pressioni distali e del rapporto caviglia / braccio ( abi ) e con eco - color doppler ( ecd )  . 
lesposizione cronica al fumo di sigaretta inuenza signicativamente il circolo arterioso periferico radiol med ( 2013 ) 118 : 206214 e la ceus con analisi del wash - in delle curve intensit / tempo una metodica utile nella valutazione delle alterazioni microcircolatorie . parole chiave ecograa con mezzo di contrasto vasculopatia periferica diabete fumo microcircolo introduction introduzione cigarette smoking constitutes a well - established risk factor for occlusive peripheral vascular disease and , subsequently , amputation . 
current methods routinely used to diagnose peripheral arterial disease ( pad ) measure the degree of large - vessel stenosis [ 1 ] but do not measure tissue blood ow , and they are unable to assess small - vessel disease and collateral perfusion . 
the aim of this study was to evaluate the effects of tobacco smoke on the microcirculation using ceus in diabetic patients with and without pad . materials and methods we studied 26 diabetic patients comprising ten current smokers and 16 nonsmokers . 
a score was assigned according to the presence and grade of stenosis at cdus examination ( 1 = normal artery , 2 = stenosis > 50% , 3 = total occlusion ) in seven arterial districts for each leg ( common , profunda and supercial femoral arteries ; popliteal artery , anterior and posterior tibial arteries ; peroneal artery )  . 
le metodiche attualmente utilizzate per la diagnosi dellarteriopatia obliterante periferica valutano principalmente il grado di stenosi dei grandi vasi arteriosi [ 1 ] senza fornire informazioni sulla perfusione tissutale , sul microcircolo e sul circolo collaterale . 
 materiali e metodi sono entrati a far parte dello studio 26 pazienti diabetici di cui 10 fumatori abituali ( fumatori da non meno di 5 anni ) e 16 non fumatori . 
i pazienti sono stati sottoposti ad un prelievo ematico a digiuno , a misurazione dellindice caviglia / braccio ( abi ) e ad esame eco - color doppler ( ecd ) degli arti inferiori . 
 ad ogni paziente stato assegnato un punteggio sulla base dei risultati dellesame ecd ( 1 = arteria normale , 2 = stenosi > 50% , 3 = occlusione totale ) considerando sette segmenti arteriosi per ogni arto ( arterie femorali comune , profonda e superciale ; arteria poplitea ; arterie tibiali anteriore e posteriore ; arteria peroniera )  . in ogni paziente larto con lesioni troche o con labi pi basso stato sottoposto ad ecograa con mezzo di contrasto per la valutazione della perfusione ematica muscolare . 
 per limaging contrastograco stato utilizzato un ecografo philips iu22 con trasduttore lineare 93 mhz con il seguente settaggio : mechanical index 0 , 06 , acoustic output 90% , gray map 1 , frame rate 13 hz . 
dopo 10 minuti di riposo in posizione supina stato iniettato un bolo di 2 , 4 ml di sonovue ( bracco , milano , italia ) in una vena antecubitale , seguito immediatamente da una soluzione salina di 5 ml , ed stato acquisito un 208 radiol med ( 2013 ) 118 : 206214 fig . 
the wash - in curve was analysed using the systems time - intensity curve analysis software ( qlab ) , which displays the acoustic intensity ( in decibels ) during acquisition time in a manually dened region of interest ( roi )  . 
four different rois were dened and placed over the following areas : ( a ) the entire gastrocnemius muscle region , ( b ) a small muscular artery , ( c ) a small muscular vein ( d ) gastrocnemius muscle tissue without artery / vein at a depth of 1 cm from the skin plane . 
la fase di washin delle curve intensit / tempo stata analizzata utilizzando il software qlab ( philips ) che mostra laumento dellintensit acustica ( in db ) nel tempo in una denita regione dinteresse . 
sono state delimitate manualmente le seguenti quattro regioni dinteresse ( roi ) : ( a ) una sezione di tutto il muscolo gastrocnemio ; ( b ) una piccola arteria muscolare ; ( c ) una piccola vena muscolare ; ( d ) una porzione del muscolo gastrocnemio senza arterie e vene , ad 1 cm di profondit dal piano cutaneo . 
le roib , c , d sono state utilizzate per la misurazione dei at in arteria , in vena e nel tessuto ( ata , atv , att )  . 
il tempo di transito arteria / vena ( a / vtt ) stato misurato considerando la differenza tra ata e atv ed il tempo di transito arteria / tessuto ( a / ttt ) stato misurato dalla differenza tra ata e att . lanalisi statistica stata eseguita utilizzando il software spss versione 16.0 ( spss , chicago , il , usa )  . 
il tempo di picco ( ttp ) il tempo dalliniezione del mezzo di contrasto no al picco massimo dintensit , e corrisponde alla durata del wash - lintensit assoluta del picco ( aip ) corrisponde al picco massimo di intensit della curva di wash - il tempo di incremento ( it ) il tempo dallinizio dellaumento di intensit del mezzo di contrasto no al suo picco massimo . 
the difference between ata and atv was considered as the artery / vein transit time ( a / vtt ) and the difference between ata and att as the artery / tissue transit time ( a / ttt )  . 
a p value < 0.05 was considered statistically signicant ( two - tailed test )  . results the clinical characteristics for smoker and nonsmoker diabetic patients are provided in table 1 . 
twenty patients ( eight smokers / 12 nonsmokers ) showed pad ( fontaine iiv ) and 6 / 26 patients had no pad ( two smokers / four nonsmokers )  . during ceus examination none of the study participants reported any side effects ; mean examination time was strate nella tabella 1 . 
stata osservata una considerevole variabilit dei parametri delle curve di wash - in ( ttp range 21 , 2757 , 43 s , aip range 4 , 5419 , 68 db ) ed i fumatori presentavano unintensit dellenhancement contrastograco ( aip ) lievemente pi bassa ma statisticamente non signicativa ( tabella 2 )  . discussione la misura dellabi un metodo economico e ben standardizzato per ottenere informazioni sul macrocircolo , ma 210 radiol med ( 2013 ) 118 : 206214 table 1 patients descriptive characteristics . 
il valore diagnostico delle tecniche convenzionali di studio come labi e lecd molto ridotto nei pazienti diabetici per la scarsa compliance vascolare , causata dalle calcicazioni della media , dalla diffusa malattia distale e dalle anomalie funzionali del microcircolo [ 3 , 4 ]  . 
lecograa con mezzo di contrasto utilizza microbolle di gas inerti che rimangono interamente connate nel distretto vascolare e posseggono caratteristiche reologiche simili a quelle dei globuli rossi e pertanto forniscono informazioni sul microcircolo [ 5 , 6 ]  . 
 nel gruppo di pazienti che abbiamo studiato lecd e labi non hanno evidenziato differenze signicative tra radiol med ( 2013 ) 118 : 206214 table 2 parameters of time - intensity curves evaluated in smoker and nonsmoker diabetic patients . 
 per il confronto tra i parametri stato utilizzato il test non parametrico di mann - withney non fumatori ( n = 16 ) fumatori ( n = 10 ) smokers , smokers had lower aip , but the difference was not signicant . 
the diagnostic performance of conventional techniques such as abi and cdus is reduced in diabetic patients because of vascular noncompliance caused by medial calcication , diffuse distal disease and functional microcirculation abnormalities [ 3 , 4 ]  . 
in this study we focused on functional aspects of the peripheral microcirculation studying , with us , the time between injection and detection of contrast medium and bolus distribution after it had entered the roi . 
it uses gas - lled microbubbles that are inert , remain entirely within the vascular space and possess intravascular rheology similar to that of red blood cells [ 5 , 6 ]  . in our patients no signicant difference was found in the fumatori e non fumatori , mentre lo studio della perfusione con mezzo di contrasto ha evidenziato un signicativa alterazione della perfusione muscolare nei pazienti fumatori . 
 questo potrebbe essere dovuto al fatto che le modicazioni dellabi riettono esclusivamente la compromissione dei macrovasi e lecd riesce ad evidenziare solo le stenosi ed i vasi collaterali di grosso calibro , ma entrambe le metodiche non sono in grado di valutare leffetto dellarteriopatia sulla perfusione muscolare . 
la ceus , con lanalisi delle curve intensit / tempo , fornisce informazioni riguardanti la rilevanza emodinamica delle stenosi e potrebbe riettere gli effetti del fumo sul livello di collateralizzazione e sul meccanismo di adattamento del microcircolo . 
esso determina complesse alterazioni delle funzioni microcircolatorie periferiche : inappropriata vasodilatazione a riposo , alterata vasodilatazione endotelio - dipendente e indipendente [ 10 ] , ridotto recupero della vasodilatazione endotelio - dipendente in risposta agli effetti acuti del fumo [ 11 ] , riduzione generale del 212 radiol med ( 2013 ) 118 : 206214 cdus score and abi between smokers and nonsmokers , whereas ceus revealed signicant impairment of muscle perfusion in smokers . 
this could be due to the fact that changes in abi exclusively reect impaired macrocirculation and cdus is able to visualise only large stenosis and collaterals , but neither method can evaluate the impact on muscle perfusion . 
ceus with time - intensity curve analysis integrates information about the haemodynamic relevance of a stenotic lesion and could reect the effects of smoking on the level of collateralisation and on adaptive mechanisms in microcirculation . 
smokers are characterised by a complex alteration in the regulation of peripheral microcirculation : inappropriate resting vasodilatation , impaired endotheliumdependent and - independent vasodilatation [ 10 ] , paradoxical recovery of endothelium - dependent vasodilatation in response to acute smoking [ 11 ] , reduction in general smooth muscle relaxation [ 12 ] and arterial elasticity [ 13 ]  . 
however , whether this nding can be extrapolated to microvascular function remains to be establish . arrival time in the artery and tissue measure the initial phase of enhancement and may depend on patient - related factors , such as heart - time volume , whereas a / t transit time depends on the degree of arterialisation of the tissue examfig . 
time - to - peak ( ttp ) , arrival time to tissue ( att ) , arterial / tissue transit time ( a / ttt ) in smokers and nonsmokers . 
4 effetto del fumo di sigaretta sui parametri della curva di wash - i fumatori ( a destra ) presentano un signicativo aumento del tempo di picco ( ttp , box blu ) , del tempo di arrivo al tessuto ( att , box verde ) , e del tempo di transito arteria / tessuto ( a / ttt , box giallo )  . 
sono mostrati la mediana ( barra orizzontale ) e il range interquartile ( box )  . rilassamento della muscolatura liscia [ 12 ] e dellelasticit arteriosa [ 13 ]  . 
queste alterazioni osservate nei fumatori potrebbero riettere un deterioramento del microcircolo come suggerito in altri studi [ 14 , 15 ] , tuttavia resta da stabilire se questi risultati possano o meno essere correlati alla funzione microvascolare . i tempi di arrivo in arteria e nel tessuto misurano liniziale fig . 
the contrast agent penetrates slowly into the muscle area examined ; the delay in the att and ttp of the contrast medium might be due to the patterns of histopathological changes in microcirculation . 
in smoking patients tissue arterialisation could be reduced , and in ischaemic tissue with brotic reorganisation and irregular vascular system ( many occluded and / or stenosed vessels ; shunts ) , the contrast medium requires more time to reach peak enhancement . however , the absolute intensity peak and a / v transit time did not differ signicantly . 
however , we must take into account the fact that ata is inuenced only by the rst pass of the contrast agent , whereas atv may also be partly affected by recirculation , i.e. 
therefore , arterial parameters and a / ttt may represent the most reliable indicators of the real state of the microcirculation . quantitative analysis of contrast enhancement is frequently used to differentiate between malignant and benign lesions , but it is rarely used to analyse tissue perfusion without comparison with a normal reference tissue . 
the average signal from one or more rois is plotted as a function of time and represented in logarithmic scale ; the relationship between video level on b - scan and received echo intensity is complicated by dynamic compression and physical factors , such as attenuation of the us beam by the contrast agent itself , so that quantitative interpretation may be unreliable or misleading . 
however , transcutaneous oximetry could be used [ 16 ]  . in conclusion , contrast imaging of muscle perfusion is an easily applicable and safe approach and a very promising method for studying skeletal muscle perfusion in diseases such as diabetic microangiopathy . 
smoking results in reduced peripheral microcirculation in diabetic patients , effects that could affect the risk of foot ulceration independently of the severity of macrovascular disease . fase di enhancement e possono dipendere da fattori correlati al paziente , come la frequenza e la gittata cardiaca , mentre il tempo di transito arteria / tessuto dipende dal grado di arterializzazione del tessuto esaminato . 
nei pazienti fumatori larterializzazione tissutale ridotta ed in un tessuto ischemico e / o brotico con un sistema vascolare mal funzionante ( occlusioni , stenosi e shunt ) il mezzo di contrasto potrebbe richiedere molto pi tempo per raggiungere il picco di enhancement . contrariamente non sono state rilevate modicazioni signicative dellintensit massima e dei tempi di transito artero - venoso tra i due gruppi e da questo si potrebbe desumere che la quantit totale di contrasto che passa attraverso il tessuto muscolare possa essere la stessa . 
inoltre , mentre lat in arteria inuenzato solo dal primo passaggio del mezzo di contrasto , lat in vena potrebbe essere parzialmente modicato dal ricircolo , cio dal secondo passaggio del contrasto ultrasonograco . 
pertanto verosimile che solo i parametri arteriosi e la / ttt rappresentino il reale stato del microcircolo . lanalisi quantitativa dellenhancement contrastograco viene frequentemente utilizzata per differenziare lesioni benigne da maligne , ma raramente per analizzare la perfusione tissutale senza la comparazione con un normale tessuto di riferimento . 
fonti di errore potrebbero essere dovute al fatto che il segnale medio da una o pi roi un graco in funzione del tempo rappresentato in scala logaritmica , la relazione tra lecogenicit video in scala di grigi e lintensit ecograca ricevuta pu essere alterata dalla compressione dinamica e da fattori sici come lattenuazione del fascio ultrasonoro dovuta alla presenza del contrasto stesso . un limite del nostro studio la mancanza di una tecnica gold - standard di riferimento per la valutazione della funzione microvascolare che attualmente , a nostra conoscenza , non disponibile ad esclusione dellossimetria transcutanea , di difcile applicazione su larga scala [ 16 ]  . in conclusione , indipendentemente dallentit delle lesioni ostruttive presenti nellarteriopatia periferica , il fumo determina una compromissione della microcircolazione periferica nel diabetico ; questo potrebbe aumentare il rischio di sviluppare lesioni troche e condizionarne levoluzione clinica . 
lutilizzo dellecograa con mezzo di contrasto nella valutazione della perfusione muscolare una tecnica sicura e di facile applicazione ed inoltre un promettente metodo di studio di patologie come la microangiopatia diabetica che pu fornire informazioni utili , integrative di quelle ottenute con altre metodiche di imaging . 
this is not always possible due to the small size of the remnant liver : in this scenario , portal venous embolization of the affected parenchyma plays a major role , allowing on one hand , precise resection of the affected parenchyma , on the other increased size of the remnant liver , thus increasing the number of patients to whom this procedure can be offered . in the book one will nd a detailed discussion on how and when portal vein embolization alone ( as pioneered by makuuchi ) , or coupled with hepatic vein embolization or following transcatheter arterial embolization can be used and provide good results in terms of patient post - surgical survival . 
 throughout the 31 chapters , which are divided into six parts ( history and anatomy ; preoperative assessment ; embolization techniques ; clinical outcomes ; additional strategies for resection and embolization ; evidence and the future ) , one easily learns which imaging techniques are useful for ( most of all ultrasound and multidetector computer tomography ) , in the rst instance diagnosing the tumour , measurement of total liver and future remnant size , discovquesto volume dedicato ad un argomento molto importante , pratico ed affascinante : come trattare , mediante lembolizzazione venosa del parenchima interessato , i pazienti portatori di tumori primitivi del fegato o di lesioni secondarie ad un tumore primitivo del colon - retto . la resezione chirurgica del parenchima epatico interessato lunica opzione terapeutica offerta a tali pazienti , con un buon tasso di successo e di sopravvivenza a lungo termine . la resezione , dopo la riduzione delle dimensioni del tumore mediante chemo - embolizzazione nei pazienti con carcinoma epatocellulare o dopo chemioterapia neodadiuvante in quelli con metastasi da tumore colo - rettale , ora possibile , se lorgano residuo ha dimensioni sufcienti da permettere adeguate e sufcienti funzioni post - chirurgiche ed una buona qualit di vita . 
ci per non sempre possibile date le dimensioni ridotte del residuo epatico : in questo scenario lembolizzazione venosa portale del parenchima interessato riveste un ruolo di primo piano , permettendo da un lato la resezione precisa del parenchima malato , dallaltro un aumento nelle dimensioni del residuo epatico , incrementando cos il numero dei pazienti cui tale metodica pu essere offerta . nel volume il lettore trover una discussione dettagliata sul come e quando lembolizzazione della vena porta da sola ( come presentata dal pioniere makuuchi ) , in associazione con lembolizzazione delle vene epatiche o al seguito di embolizzazione arteriosa trans - catetere pu essere utilizzata , offrendo buoni risultati in termine di sopravvivenza post - chirurgica . 
 nei 31 capitoli , divisi in sei parti ( storia ed anatomia ; valutazione preoperatoria ; tecniche di embolizzazione ; risultati clinici ; strategie addizionali per la resezione e lembolizzazione ; evidenze ed il futuro ) , il lettore impara con facilit quali tecniche di immagine ( in particolare lecograa e la tc multidetettore ) sono utili per diagnosticare in prima istanza il tumore , misurare poi il volume totale radiol med ( 2013 ) 118 : 340341 ering further localizations ; when and how it is possible to perform procedures in order to obtain the best results and which are the future perspectives ( in view of the results on stem cells enhancing hepatic regeneration )  . all the information found in the text derives from experience gathered over the years in third reference centres in japan ( where portal embolization was developed ) , europe and around the world . this is a book that will be appreciated not only by interventional radiologists and hepatobiliary surgeons , but also by the broad audience of those dedicated to the treatment of liver diseases and to research in this eld . 
 del fegato e quello del futuro residuo epatico , diagnosticare eventuali altre localizzazioni ; quando e come sia possibile eseguire le procedure per ottenere i migliori risultati e quali sono le prospettive future ( in vista anche dei risultati delle cellule staminali favorenti la rigenerazione epatica )  . 
vinci1 1department of diagnostic imaging , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 2department of medical science section of hygiene , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 3department of diagnostic imaging , university of palermo , via del vespro 127 , 91027 palermo , italy 4department of gastroenterology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy correspondence to : l.p. 
we evaluated the diagnostic accuracy of magnetic resonance enterography ( mr - e ) in assessing crohns disease ( cd ) activity by differentiating acute , chronic and remission stages of disease through a quantitative mr - e assessment . 
in all cases , the ileum and large bowel were imaged with morphological sequences ( heavily t2 - weighted single - shot , dual fast - eld echo , balanced fast - eld echo ) and a postcontrast dynamic sequence ( t1 - weighted high - resolution isotropic volume excitation )  . 
mr - e ndings were compared with clinicallaboratory data and disease activity indices [ crohns disease activity index ( cdai ) ; inammatory bowel disease questionnaire ( ibdq ) ]  . 
scopo del nostro lavoro stato valutare laccuratezza diagnostica dellenterograa con risonanza magnetica ( e - rm ) nella determinazione dellattivit del morbo di crohn ( mc ) differenziando gli stati di malattia acuta , cronica e di remissione attraverso un indice quantitativo ( e - rm score )  . 
in tutti i casi lileo e lintestino crasso sono stati studiati utilizzando sequenze morfologiche ( t2w single shotheavy weight , dual fast eld echo , balanced fast eld echo ) ed una sequenza dinamica post - contrastograca ( t1w high resolution isotropic volume excitation )  . 
i dati della e - rm sono stati confrontati con quelli clinico - laboratoristici e con gli indici di attivit di malattia ( crohn disease activity index , cdai ; inammatory bowel disease questionnaire , ibdq )  . 
the mr - e score proposed in this study proved to be useful in assessing disease severity and monitoring response to treatment . keyword crohns disease mr enterography disease activity mr enterography score nel restante 34% una fase di malattia attiva . 
lo score e - rm da noi proposto si rivelato utile nella valutazione della severit di malattia e nel monitoraggio della risposta al trattamento . parole chiave morbo di crohn enterograa - rm attivit di malattia score e - rm introduction introduzione crohns disease ( cd ) is a chronic inammatory disease of the gastrointestinal tract characterised by a granulomatous , noncaseous , transmural and segmental inammation . 
the crohns disease activity index ( cdai ) , the most widely used clinical score , and the inammatory bowel disease questionnaire ( ibdq ) , commonly used to evaluate the patients quality of life [ health - related quality of life ( hr - qol ) ] , are not universally accepted , as they are heavily based on the patients subjective assessment of symptoms [ 24 ]  . magnetic resonance ( mr ) imaging has been proposed as a diagnostic tool for studying cd since numerous scientic studies demonstrated its high sensitivity in assessing both disease activity [ 59 ] and severity [ 1013 ] at the level of the terminal ileu the aims of this study were : ( a ) to examine the diagnostic performance of mr enterography ( mr - e ) of the ileum and colon in assessing typical ndings of the acute , chronic and remission stages of cd ; ( b ) to establish the techniques reliability in determining disease activity based on a radiological score ( mr - e score ) by correlating the results with the clinical scores ( cdai and ibdq )  . il morbo di crohn ( mc ) una patologia inammatoria cronica del tratto gastrointestinale caratterizzata da una reazione granulomatosa , non caseosa , transmurale e segmentaria . 
il crohn disease activity index ( cdai ) , lo score clinico pi ampiamente utilizzato , e linammatory bowel disease questionnaire ( ibdq ) , di comune impiego per valutare la qualit di vita del paziente ( health - related quality of life , hrqol ) , non sono universalmente accettati in quanto basati prevalentemente su una valutazione soggettiva della sintomatologia [ 24 ]  . la risonanza magnetica ( rm ) stata recentemente proposta come strumento diagnostico per lo studio del mc , poich numerosi lavori scientici hanno dimostrato alta sensibilit nella valutazione tanto dellattivit [ 59 ] quanto della severit di malattia a livello dellileo terminale [ 1013 ]  . 
 scopo del nostro lavoro stato quello di esaminare le performance diagnostiche dellenterograa con risonanza magnetica ( e - rm ) di ileo e colon nella valutazione dei reperti tipici delle fasi acuta , cronica e di remissione del mc e di stabilirne lafdabilit nella determinazione dellattivit radiol med ( 2013 ) 118 : 181195 materials and methods study population di malattia attraverso limpiego di uno score basato sulle caratteristiche radiologiche ( e - rm score ) confrontandolo con gli score clinici ( cdai e ibdq )  . between 2008 and 2010 , we prospectively recruited 100 patients ( 51 men , 49 women ; mean age 37.4414.91 , range 1879 )  . 
the study population , recruited for mr - e during follow - up at the gastroenterology division of our hospital , was receiving oral treatment with corticosteroids or other agents such as azathioprine , iniximab , mesalazine or antibiotics . 
informed consent was obtained from each patient prior to the mr examination . disease assessment presence , extent and severity of the pathological segments were rst evaluated with an endoscopic examination exploring the last 2025 cm of ileum ; lesion distribution was dened by endoscopically dividing the gastrointestinal tract into ve segments : duodenum and jejunum ; ileum , terminal ileum ( including the ileocaecal valve ) ; caecum and ascending colon ; transverse and descending colon ; rectumsigmoid colon . 
the disease was considered inactive with a cdai score < 150 ( score = 0 ) , mildly to moderately active with a score 150 and 450 ( score = 1 ) , and severely active with a score > 450 ( score = 2 )  . 
the disease was assessed as inactive with an ibdq score 170 ( score = 0 ) , mildly or moderately active with a score > 135 and < 169 ( score = 1 ) and severely active with a score 134 ( score = 2 )  . imaging technique all patients underwent mr - e on a 1.5 - tesla mr unit ( achieva , philips medical system , eindhoven , the netherlands ) with a maximum gradient strength of 30 mt / patients were all studied in the supine position using a phased - array body coil . 
after an overnight fast and 45 min before the mr examination , each patient received orally a solution of biphasic contrast medium [ polyethylene glycol ( peg ) ]  . 
the solution had been previously prepared by dissolving a granular powder containing 34.8 g of peg 4 , 000 ( selg , promefarm , italy ) , 1.42 g sodium sulphate , 0.42 g sodium bicarbonate , 0.36 g sodium chloride materiali e metodi popolazione di studio tra il 2008 e il 2010 , sono stati reclutati in maniera prospettica 100 pazienti ( 51 maschi e 49 femmine ; et media 37 , 4414 , 91 ; range det 1879 )  . 
la popolazione di studio , reclutata per effettuare una valutazione rm durante un periodo di follow - up , effettuato regolarmente presso lunit operativa di gastroenterologia del nostro nosocomio , era in trattamento farmacologico con corticosteroidi orali , o altri farmaci quali : azatioprina , iniximab , mesalazina o antibiotici . 
prima delleffettuazione dellesame rm da ogni paziente stato ottenuto il consenso informato . valutazione di malattia la presenza , lestensione e la severit dei segmenti patologici stata identicata in prima istanza mediante esame endoscopico con esplorazione degli ultimi 2025 cm dellileo ; la distribuzione delle lesioni era stata denita dividendo endoscopicamente il tratto gastroenterico in 5 segmenti : duodeno e digiuno ; ileo , ileo terminale ( comprendente la valvola ileo - ciecale ) ; cieco e colon ascendente ; trasverso e colon discendente ; retto - sigma . 
 la malattia veniva considerata inattiva con uno score cdai < 150 ( punteggio = 0 ) , da lievemente a moderatamente attiva ( punteggio = 1 ) con uno score150 e 450 e severa ( punteggio = 2 ) con uno score > 450 . 
la malattia stata valutata inattiva con uno score ibdq170 ( punteggio = 0 ) , lievemente o moderatamente attiva con uno score > 135 e < 169 ( punteggio = 1 ) , e severa con uno score134 ( punteggio = 2 )  . tecnica dimaging in tutti i pazienti stato effettuato un esame di e - rm con una apparecchiatura da 1 , 5 tesla ( achieva , philips medical system , eindhoven , olanda ) con un gradiente massimo pari a 30 mt / tutti i pazienti sono stati studiati in decubito su184 radiol med ( 2013 ) 118 : 181195 and 0.18 g potassium chloride in 2 , 000 ml water . 
inhibition of bowel peristalsis , crucial for reducing motion artefacts , was achieved by injecting 10 ml / mg n - butyl scopolamine ( buscopan , boringher ingelheim , florence , italy ) intravenously before starting the mr examination . 
administration of gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa ) ( magnevist , schering ag , germany ) , the protocol required the following breathhold sequences : axial single - shot heavily t2 - weighted ; axial t1 - weighted dual fast eld echo ( ffe ) ; coronal balanced fast eld echo ( ffe )  . 
acquisition parameters are shown in table 1 . image analysis images were evaluated by a radiologist experienced in abdominal mr imaging ( lm with 20 years experience ) who was unaware of clinicallaboratory ndings and results pino utilizzando una bobina phased - array body . 
dopo una notte di digiuno e 45 minuti prima dellindagine rm , ad ogni paziente stata somministrata per os una soluzione di mezzo di contrasto ( mdc ) bifasico di glicole polietilenico ( peg )  . 
 tale soluzione era stata preparata prima della somministrazione dissolvendo una polvere granulare contenente 34 , 8 g di peg 4000 ( selg , promefarm , italia ) , 1 , 42 g di solfato di sodio anidrato , 0 , 42 g di bicarbonato di sodio , 0 , 36 g di clorito di sodio , 0 , 18 g di clorito di potassio disciolti in 2000 ml di acqua . 
linibizione della peristalsi intestinale , essenziale per ridurre gli artefatti da movimento , stata ottenuta con iniezione endovena ( ev ) di 10 ml / mg di n - butilscopolamina ( buscopan , boringher ingelheim , firenze , italia ) somministrata al paziente prima di iniziare lesame e - rm . 
 prima della somministrazione ev di gadopentate dimeglumine ( gd - dtpa ) ( magnevist , schering ag , germania ) , il protocollo includeva le seguenti sequenze breath - hold : assiale t2 - pesata single shot - heavy weight ( ssh - hvw ) ; assiale t1 - pesata dual fast eld echo ( ffe ) ; coronale balanced fast eld echo ( bffe )  . 
evaluation of disease activity was based on analysis of ve parameters : bowelwall thickening ; presence of bowel - wall enhancement ; distribution of bowel - wall enhancement ; mesenteric brofatty proliferation ; presence of local complications ( localised free uid , phlegmon , mesenteric lymphadenopathy , abscess or stula )  . 
 more specically , in agreement with previous studies [ 4 , 5 ] , the increase was considered mild to moderate if wall contrast enhancement was greater than that of the spleen and less than that of the renal cortex and marked if it was equal to that of the renal cortex . 
the disease phase was considered to be in remission with a score = 0 , chronic with a score 1 and 4 , and active with a score 5 and 8 . 
 a remission phase was dened as segments showing inactive disease with endoluminalmucosal lesions not detectable at imaging and minimal wall thickening ( 3 mm ) that was therefore not relevant to our assessment or showing complete healing after pharmacological therapy . 
i parametri di acquisizione sono mostrati nella tabella 1 . analisi delle immagini le immagini sono state valutate da un radiologo esperto in rm addominale ( l.m. , 20 anni di esperienza ) non a conoscenza dei reperti clinico - laboratoristici e dei risultati del preliminare esame endoscopico . 
la valutazione dellattivit di malattia si basata sullanalisi di 5 parametri : ispessimento della parete intestinale ; presenza di contrast enhancement ( ce ) parietale ; pattern di distribuzione del ce parietale ; proliferazione broadiposa del mesentere ; presenza di complicanze locali ( uido libero localizzato , emmoni , linfoadeopatie mesenteriche , ascessi o stole )  . 
 un segmento intestinale stato considerato patologico se ispessito ( spessore di parete > 3 mm ) o con aumentato enhancement dopo somministrazione ev di gadolinio ; in particolare , in accordo a precedenti studi [ 4 , 5 ] , lincremento era considerato lieve - moderato se il ce parietale era maggiore a quello della milza e inferiore a quello della corticale renale , marcato se il ce parietale era uguale a quello della corticale renale . 
in particolare ( tabella 2 ) uno score tra 0 e 2 stato assegnato allo spessore di parete , alla presenza di ce parietale e al pattern di distribuzione del ce parietale . 
per fase di remissione abbiamo considerato quei segmenti in fase di malattia non attiva con lesioni endoluminali - mucosali non identicabili radiolotable 2 summary of magnetic resonance enterography ( mr - e ) score ( 02 ) mr ndings wall thickness ( mm ) wall contrast enhancement enhancement pattern fibrofatty proliferation local complications acompared with enhancement of spleen and cortical kidney tabella 2 score ( 02 ) dellenterograa con risonanza magnetica ( e - rm ) schematizzato reperti rm spessore di parete ( mm ) contrast enhancement parietale pattern di contrast enhancement proliferazione broadiposa complicanze locali arispetto al ce della corticale renale e della milza absent absent assente assente assente 3.16.0 milda transmural present present 3 , 16 , 0 lievea transmurale presente presente markeda layered marcatoa straticato 186 radiol med ( 2013 ) 118 : 181195 segments with signs of acute disease such as wall thickening > 6 mm with homogeneous , moderate to marked , layered contrast enhancement , presence of target sign , mesenteric brofatty proliferation and local complications . statistical analysis statistical analysis was conducted with commercially available software ( statamp 10.0 , statacorp lp , college station , tx , usa )  . 
bowel - wall enhancement was absent in 17 / 100 patients ( 17% ) , mild to moderate in 60 / 100 ( 60% ) and marked in 23 / 100 ( 23% ) , with a transmural enhancement pattern in 58 / 100 ( 58% ) and a layered pattern in 28 / 100 ( 28% )  . 
 correlations a statistically signicant difference was found in the degree of wall enhancement between clinically remitting gicamente , minimo ispessimento di parete di poco 3 mm , pertanto non signicativo alla nostra valutazione , o con restituito ad integrum dopo trattamento farmacologico . 
abbiamo denito in fase cronica i segmenti che presentavano , a seguito dei fenomeni ripartivo - cicatriziali , ispessimento parietale compreso tra 3 , 1 e 6 , 0 mm con restringimento luminale e con lieve - moderato , disomogeneo e transmurale ce , ed eventuale presenza di alterazioni mesenteriali e linfoadenopatie loco - regionali . 
in fase attiva abbiamo incluso segmenti con segni di malattia acuta quali ispessimento parietale > 6 mm con ce moderato - marcato di tipo omogeneo e straticato presenza del segno del bersaglio , di iperplasia bro - adiposa mesenteriale e complicanze locali . analisi statistica lanalisi statistica stata condotta con un software disponibile in commercio ( statamp 10.0 , statacorp lp , college station , texas , usa )  . 
 risultati valutazione dellattivit di malattia e reperti e - rm la e - rm stata ben tollerata in quasi tutti i pazienti , solo 7 pazienti hanno mostrato scarsa compliance alla somministrazione di peg per os , per linsorgenza di dolori crampiformi addominali e urgenza defecatoria . 
tra i pazienti esaminati , lo spessore medio della parete intestinale risultato pari a 4 , 162 , 25 mm ( range 1 , 910 , 7 mm )  . 
 il ce parietale risultato assente in 17 / 100 pazienti ( 17% ) , lieve - moderato in 60 / 100 pazienti ( 60% ) e marcato in 23 / 100 pazienti ( 23% ) , con pattern contrastograco di tipo transmurale in 58 / 100 pazienti ( 58% ) e straticato in 28 / 100 pazienti ( 28% )  . 
le lesioni sono state riscontrate sia a livello dellintestino tenue che dei segmenti colici con maggiore frequenza di localizzazione in corrispondenza di ileo ed ileo terminale ( tabella 5 )  . 
 abbiamo riscontrato una differenza statisticamente signicativa nel grado di ce parietale tra pazienti con malattia clinicamente in fase di remissione o cronica ( cdai < 150 ) e pazienti con malattia clinicamente attiva ( cdai150 ; 2 = 31 , 80 ; p < 0 , 001 )  . 
inoltre , abbiamo rilevato una differenza statisticamente signicativa nel pattern di ce parietale tra pazienti con cdai < 150 e pazienti con cdai150 ( 2 = 21 , 12 ; p < 0 , 0001 )  . 
a , b axial heavily t2 - weighted single - shot and coronal balanced fast - eld echo images showed no signicant wall thickening ( 0 points ) ( arrowhead )  . 
c , d absence of wall enhancement ( 0 points ) ( arrowhead ) on postcontrast coronal t1 - weighted high - resolution isotropic volume excitation sequence and resulting axial multiplanar reconstruction . 
a , b le immagini assiale t2 - pesata ssh - hvw e coronale bffe non mostrano signicativo ispessimento parietale ( 0 punti ) ( punta di freccia )  . 
c , d non evidente presa di contrasto parietale ( 0 punti ) ( punta di freccia ) nella sequenza post - contrastograca coronale t1 - pesata thrive ed assiale con ricostruzione multplanare ( mpr ) risultante . 
a , b mild wall thickening ( 1 point ) ( arrowheads ) of hypogastric ileal loop appreciable on axial heavily t2 - weighted single - shot and coronal balanced fast - eld echo images . 
c , d postcontrast coronal t1 - weighted weighted high - resolution isotropic volume excitation sequence and resulting axial multiplanar reconstruction demonstrate mild contrast enhancement ( 1 point ) with transmural pattern ( 1 point ) ( arrowheads )  . 
a , b lieve ispessimento parietale ( 1 punto ) ( punte di freccia ) di unansa ileale in sede ipogastrica apprezzabile nelle immagini assiale t2 - pesata ssh - hvw e coronale bffe . 
c , d dopo somministrazione di mdc ev nella sequenza coronale t1pesata thrive ed assiale mpr risultante si apprezza moderato ce ( 1 punto ) con pattern transmurale ( punte di freccia ) ( 1 punto )  . 
 a , b the descending colon shows marked wall thickening ( 2 points ) and luminal narrowing on coronal balanced fast - eld echo ( arrowheads ) and axial heavily t2 - weighted single - shot images ( arrow )  . 
 a , b il colon discendente presenta marcato ispessimento parietale ( 2 punti ) con restringimento luminale evidente nelle immagini coronale bffe ( punte di freccia ) e assiale t2 - pesata ssh - hvw ( freccia )  . 
c , d moderato ce ( 1 punto ) con pattern transmurale ( 1 punto ) nella sequenza coronale t1 - pesata thrive ( punte di freccia ) ed assiale mpr risultante ( freccia ) dopo somministrazione di mdc ev . 190 radiol med ( 2013 ) 118 : 181195 fig . 
ac axial heavily t2 - weighted single - shot and coronal balanced fast - eld echo images clearly show extensive marked wall thickening ( 2 points ) of the hypogastric ileal loop . 
a - c diffuso e marcato ispessimento parietale ( 2 punti ) di unansa ileale a livello ipogastrico , ben evidente nelle immagini assiali t2 - pesate ssh - hvw e coronale bffe . 
sono presenti , inoltre , marcata proliferazione broadiposa del mesentere periviscerale ( 1 punto ) ( punte di freccia ) e lindoadenopatie mesenteriche ( 1 punto ) ( freccia )  . 
d - f marcato ce ( 2 punti ) di tipo straticato ( 2 punti ) della stessa ansa dopo somministrazione di mdc ben evidente nelle immagini in coronale e assiale mpr risultante t1 - pesata thrive . 
the group of patients with cdai150 included a to ( fase acuta o non cicatriziale ) risultava maggiore rispetto a quella di pazienti con pattern di ce parietale transmurale ( fase cronica o cicatriziale )  . 
una differenza statisticamente signicativa stata rilevata nel pattern di ce parietale tra radiol med ( 2013 ) 118 : 181195 table 6 percentages of magnetic resonance enterography ( mr - e ) score values and corresponding phase of disease activity in our sample mr - e score disease activity 9% inactive 57% chronic 34% active 9% , malattia in fase di remissione 57% , malattia cronica 34% , malattia attiva tabella 6 percentuali di valori di score dellenterograa con risonanza magnetica ( e - rm ) e corrispondenti stadi dellattivit di malattia riscontrati nel nostro campione score e - rm percentualetotale e attivit di malattia higher percentage of cases with a layered enhancement pattern ( acute or noncicatricial phase ) compared with cases with a transmural pattern ( chronic or cicatricial phase )  . 
multivariate analysis demonstrated that among the various mr - e ndings , the parameter most closely correlated with disease activity was the pattern of contrast enhancement , followed by wall thickness and local complications . discussion no absolute clinical criteria yet exist to dene and quantify inammatory activity in cd [ 15 ]  . 
it has been demonstrated that a less - than - accurate diagnosis of cd increases the morbidity and mortality rates related to direct complications of pazienti con e pazienti senza complicanze locali ( 2 = 7 , 13 ; p < 0 , 01 )  . 
lanalisi multivariata ha dimostrato che nellambito dei reperti rm , il parametro che si associa maggiormente allattivit di malattia il pattern di ce parietale , seguito dallo spessore di parete e dalle complicanze locali . discussione a tuttoggi , non sono disponibili criteri clinici assoluti per denire e quanticare lattivit inammatoria del mc [ 15 ]  . 
 stato dimostrato che una diagnosi poco accurata di mc aumenta la morbilit e la mortalit a causa sia delle complicanze , direttamente legate alla malattia [ 18 , 19 ] sia della prolungata terapia medica con immunosoppressori [ 1820 ]  . il ruolo degli indici clinici di attivit di malattia tra cui il 192 radiol med ( 2013 ) 118 : 181195 fig . 
5 correlazione tra score e - rm e cdai e tra score e - rm ed ibdq . the disease [ 18 , 19 ] as well as to prolonged treatment with immunosuppressants [ 1820 ]  . the role of the clinical indices of disease activity , such as cdai and ibdq , remains highly controversial . 
cdai provides an overall assessment of the clinical situation , which is more based on the patients subjective symptoms than on anatomical parameters , so that no locoregional analysis can be carried out for multifocal lesions , which are common in cd . 
despite its known limitations , however , cdai remains the reference standard for the clinical assessment of disease activity [ 2123 ] , as biochemical parameters such as c - reactive protein and erythrocyte sedimentation rate have high sensitivity but poor specicity [ 2224 ]  . the imaging reference standard for cd diagnosis and staging is endoscopy ( associated with histology )  . 
other imaging procedures such as ultrasound , scintigraphy , computed tomography ( ct ) and mr imaging used as an adjunct to the endoscopic gold standard can assist in the diagnosis . 
numerous studies in the literature evaluated the diagnostic accuracy of ct enterography and mr - e in comparison with endoscopy ( ileocolonoscopy and capsule endoscopy ) [ 2527 ]  . 
 in addition , despite the limitations of poor mucosal detail [ 29 , 30 ] , its high denition and contrast resolution of soft tissue provides it with signicant diagnostic accuracy and an ability to differentiate active inammation from remission and chronic disease [ 30 ]  . 
in particolare , il cdai fornisce una valutazione globale della situazione clinica del paziente , risentendo pi della sintomatologia soggettiva che dei parametri anatomici e pertanto non rendendo possibile unanalisi loco - regionale per lesioni intestinali multifocali , comuni nel mc . 
nonostante i limiti riconosciuti , tuttavia , il cdai resta lo standard di riferimento per la valutazione clinica dellattivit di malattia [ 2123 ] , poich i parametri biochimici , quali proteina c - reattiva ( pcr ) e velocit di eritrosedimentazione ( ves ) , sono molto sensibili ma scarsamente specici [ 2224 ]  . lo standard strumentale di riferimento per la diagnosi e per la determinazione dello stadio della patologia lendoscopia ( associata allistologia ) , la quale , tuttavia , consente di visualizzare solo il colon e lultimo tratto dellintestino tenue ed scarsamente tollerato dal paziente . 
in associazione al gold standard endoscopico , altre procedure di imaging quali ultrasonograa , esami scintigraci , tomograa computerizzata ( tc ) e rm sono di valido supporto nella diagnosi . 
in particolare la e - rm , tecnica non invasiva e che non impiega radiazioni ionizzanti , ha mostrato alti valori di sensibilit e specicit nella valutazione del mc [ 28 ] , e nonostante i limiti relativi al dettaglio mucosale [ 29 , 30 ] grazie alla sua alta denizione e risoluzione di contrasto dei tessuti molli dotata di signicativa accuratezza diagnostica ed in grado di discriminare linammazione attiva dalle fasi di remissione e cronica [ 30 ]  . 
i protocolli di imaging e - rm , attualmente , sono stati ampiamente standardizzati , sia nelle tecniche di distensione del piccolo intestino che nelle sequenze utilizzate [ 13 , 3133 ]  . radiol med ( 2013 ) 118 : 181195 sequences used and techniques to achieve small - bowel distension [ 13 , 3133 ]  . a good depiction of the intestinal wall is highly important in evaluating cd , as collapsed bowel loops can conceal lesions or mimic disease by suggesting pathologically thickened loops in healthy segments [ 34 ]  . 
therefore , good intestinal preparation and correct timing between preparation and examination are indispensable for an optimal mr - e study , as also demonstrated in our series ( 94% of patients )  . 
 in agreement with the literature [ 4 , 35 ] , we dened as pathological a wall thickness > 3 mm and found a mean overall thickness of 4.162.25 min line with other authors [ 27 ] , we did not assess the correlation between cdai and wall thickening because increased wall thickness may also be related to wall brosissubstenosis ( chronic or cicatricial phase )  . 
also consistent with the literature [ 22 , 36 , 37 ] , the degree and pattern of wall enhancement were examined in the enterographic phase 7090 s after the beginning of contrast administration . 
we found a statistically signicant difference in the degree of wall enhancement in patients with a remission or chronic phase of disease ( cdai < 150 ) compared with those with clinically active disease ( cdai150 )  . 
 [ 39 ] , the condition of hypoxia in chronic disease could trigger the process of angiogenesis , which would justify the increased microvessel permeability and the increased wall enhancement typical of active disease . 
 other predictors of disease activity were the presence of mesenteric brofatty proliferation and local complications , as previously reported [ 29 ] ; this nding was also validated by the clinical results , as local complications were more frequently seen in the group of patients with cdai > 150 . 
 we proposed a new multiparameter mr - e score ( based on the ve above - mentioned parameters ) that provides a standardised analysis of the small bowel and colon for assessing disease activity in cd . 
there was a strong correlation between mr - e and cdai scores ( r = 0.86 ; p < 0.001 ) , la buona delineazione della parete intestinale molto importante nella valutazione del mc , in quanto anse collassate possono nascondere lesioni o mimare la malattia suggerendo anse patologicamente ispessite in segmenti non affetti [ 34 ]  . 
 pertanto , una buona preparazione intestinale ed un corretto timing tra essa e lesecuzione dellesame sono indispensabili per una ottimale e - rm , come dimostrato anche nel nostro studio ( 94% dei pazienti )  . 
in accordo con i dati riportati in letteratura [ 4 , 35 ] , nella nostra esperienza abbiamo denito patologico uno spessore di parete > 3 mm , con uno spessore medio globale di 4 , 162 , 25 mnon abbiamo valutato , come riportato da altri autori [ 27 ] , la correlazione tra cdai ed ispessimento parietale in quanto laumento di spessore parietale pu essere determinato anche ad una condizione di substenosi - brosi parietale ( cronica o in fase cicatriziale )  . 
in accordo con altri studi riportati in letteratura [ 22 , 36 , 37 ] , il grado e il pattern di ce parietale sono stati esaminati nella fase enterograca , a 7090 s dallinizio della somministrazione di mdc . 
abbiamo riscontrato una differenza statisticamente signicativa nel grado di ce parietale in pazienti con malattia in fase di remissione o cronica ( cdai < 150 ) rispetto a pazienti con malattia clinicamente attiva ( cdai150 )  . 
 [ 39 ] la condizione di ipossia della malattia cronica potrebbe innescare il processo di angiogenesi che giusticherebbe unaumentata permeabilit della parete vasale e laumento del ce parietale tipico della malattia attiva . 
in accordo con altri studi [ 4 , 36 , 40 ] , stato evidenziato che il pattern di ce parietale straticato pu essere associato ad una maggiore attivit di malattia . 
la signicativa diminuzione dello spessore e del ce parietale il reperto pi afdabile nel predire la remissione clinica di malattia in quei pazienti con precedente fase attiva sottoposti a terapia [ 37 ]  . 
 altri fattori predittivi di attivit di malattia sono stati la presenza di proliferazione broadiposa mesenteriale e complicanze locali , come anche riportato da altri autori [ 29 ] ; dato confortato anche clinicamente , poich nel nostro campione le complicanze locali sono state riscontrate con maggiore frequenza nel gruppo di soggetti con cdai > 150 . 
 abbiamo proposto un nuovo score e - rm multiparametrico ( dato dai sopracitati 5 parametri ) al ne di unanalisi standardizzata del piccolo intestino e del colon e per la valutazione dellattivit di malattia . 
 [ 40 ] proposed a multiparameter mr score ( score7 ) , even though limited to the terminal ileuconsistent with the literature [ 21 ] , our results suggest that the overall evaluation of disease activity must necessarily be based on the integration of several parameters ; in our mr - e score , the most signicant parameter for disease activity was the layered enhancement pattern . our study has some limitations related to the recruitment of patients during the follow - up : we were unable to correlate mr - e ndings with an objective reference standard such as biopsy , as no further histopathological examination was called for during follow - up . 
local complications detected with mr imaging , including the two enteroenteric stulas , were not conrmed at surgery owing to resolution of the clinical picture following pharmacological treatment . una forte correlazione tra score e - rm e cdai ( r = 0 , 86 ; p < 0 , 001 ) , come anche riportato da laghi et al . 
in accordo con altri studi [ 21 ] , i nostri risultati suggeriscono che la valutazione complessiva dellattivit di malattia deve necessariamente basarsi sullintegrazione di pi parametri ; del nostro score e - rm il pi indicativo di malattia attiva stato il pattern di ce parietale di tipo straticato . il nostro studio presenta alcuni limiti legati al reclutamento dei pazienti nel follow - up . 
guglielmi2 , 6 1 department of radiology , faculty of medicine , chiang mai university , thailand 2 department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 3 department of anatomy , faculty of medicine , chiang mai university , thailand 4 department of pathology , faculty of medicine , chiang mai university , thailand 5 department of orthopaedics , faculty of medicine , chiang mai university , thailand 6 department of radiology , scientic institute hospital casa sollievo della sofferenza , viale cappuccini 1 , 71013 san giovanni rotondo ( fg ) , italy correspondence to : g . 
guglielmi , department of radiology , university of foggia , viale luigi pinto 1 , foggia 71100 , italy , tel . : + 39 - 0881 - 733866 , fax : + 39 - 0881 - 350368 , e - mail : g.guglielmi@unifg.it received : 26 october 2011 / accepted : 18 november 2011 / published online : 28 june 2012 springer - verlag 2012 abstract purpose . 
one hundred and sixty foreign bodies consisting of 52 - mm fresh wood , dry wood , glass , porcelain and plastic fragments were randomly placed in the plantar soft tissue of the forefoot and sole . 
to identify riassunto obiettivo lo scopo di questo studio determinare laccuratezza della radiograa tradizionale , della tomograa computerizzata ( tc ) e della risonanza magnetica nucleare ( rmn ) nellidenticazione dei corpi estranei inseriti nei piedi di cadaveri . materiali e metodi nei tessuti molli plantari dellavampiede e del meso - retropiede sono stati posizionati , in maniera casuale , centosessanta corpi estranei di legno fresco , legno secco , vetro , porcellana e plastica dalle dimensioni di 52 msono state inoltre praticate centosessanta incisioni senza inserire alcun corpo estraneo . 
le radiograe , tc e rmn alla ricerca dei corpi estranei sono state interpretate in cieco . risultati la sensibilit e la specicit complessive sono risultate rispettivamente del 29% e 100% usando le radiograe , del 63% e 98% usando la tc e del 58% e 100% usando la rmn . 
la tc si rivelata migliore rispetto alla rmn nellindividuazione del legno fresco , ricco di acqua . conclusioni radiologia tradizionale , tc e rmn sono 304 radiol med ( 2013 ) 118 : 303310 foreign bodies with mri , pulse sequences should be used to enhance the susceptibility artefact . 
in water - rich wood , as in chronically retained wood , ct is more accurate than mri . keywords foreign body foot injuries soft tissue infection computed tomography magnetic resonance imaging altamente speciche nella rilevazione dei corpi estranei ma presentano una bassa sensibilit . 
 parole chiave corpo estraneo ferite al piede infezione dei tessuti molli tomograa computerizzata risonanza magnetica introduction materials and methods retained foreign bodies ( fb ) are a common problem occurring after penetrating injuries . 
the diagnostic assessment of retained fb is challenging : the majority of patients do not report penetrating injuries because symptoms can occur several months or even years after the event [ 35 ]  . 
moreover , penetrating injuries may not be noticed in patients with neuropathic arthropathy of the foot . in clinical practice , when a retained fb is strongly suspected , ultrasonography ( us ) is a good modality for detection and can be used as a guide for extraction [ 6 , 7 ]  . 
on the other hand , with a low index of suspicion , patients presenting with masses and infection of the foot are generally evaluated with radiography , computed tomography ( ct ) or magnetic resonance imaging ( mri )  . 
although several papers report incidental ndings of fb on ct and mri [ 4 , 5 , 810 ] , the accuracy of these imaging tools in fb detection remains unknown . 
several in vitro studies in animal tissue have been performed [ 1113 ] ; however , these tissue types were unable to adequately simulate the complex tissue structures of the human foot . 
a study using cadaveric hands showed a high efcacy of ct and mri in fb detection , but fb sizes were larger than clinically applicable [ 14 ]  . the purpose of this controlled study was to determine the accuracy of radiography , ct and mri in detecting fb in cadaver feet . 
to determine the size to be used in this study , fb 23 mm , 25 mm and 210 mm were inserted in porcine muscle and scanned with ct and mri . 
multiplanar reconstructions ( mpr ) were obtained in the axial , coronal and sagittal views using 3 - mm slice thickness without gaps . radiographs , ct and mri were interpreted ( by consensus ) by two musculoskeletal radiologists ( np and cs ) who were free to modify the window level setting and use the magnication and zoom tools available on the workstation . 
although glass and porcelain are radiopaque , radiographs failed to reveal 15 pieces of glass ( 47 % ) and three of 32 pieces of porcelain ( 9 % )  . 
on ct , plastic density was approximately 1020 hounseld units ( hu ) , dry wood 90130 hu , fresh wood 150200 hu , glass 450 500 hu and porcelain 1 , 5002 , 000 hu . 
the background density of tissue of the foot was approximately 90 to 100 hu for subcutaneous tissue , 50 - 60 for muscle , 100 - 110 for tendon and 1 , 300 - 1 , 500 for cortical bone . 
although radiography has been reported to reveal radiolucent fb in 15% of cases [ 18 ] , the lucency of small retained fb is not sufcient to make it visible . 
although radiography cannot exclude the presence of an fb , it remains the rst step used in evaluating the foot because it is widely available , easy to perform and inex308 radiol med ( 2013 ) 118 : 303310 fig . 
4a , b ct of the foot showing wooden foreign bodies ( fb ) : coronal image of the forefoot shows a fresh wood fb ( arrow ) , which is hyperdense to the adjacent tendon ( a )  . 
in chronically retained fb , radiographs can reveal bone changes ( related to fb ) , such as erosions , osteoblastic lesions and periosteal reaction [ 19 , 20 ]  . unlike radiographs , ct detection rate is not affected by fb location . 
although ct is an excellent technique for identifying radiopaque fb , its capability of measuring soft tissue density makes ct particularly useful for detecting some radiolucent fb , such as wood . 
on ct , soft tissue calcication , which is common in patients with arteriosclerosis , neuropathy , venous stasis , trauma and renal insufciency , can mimic fb [ 21 ]  . 
in living patients , the use of contrast material intravenously may reduce this false positive nding because it helps delineate vascular structures and fb inammation . on mri , most fb show a variable degree of hypointense signal in all pulse sequences . 
the hypointense signal intensity of the fb , accompanied by inammation of the surrounding soft tissue , appears as a target lesion in cross - sectional images [ 2 ]  . 
when reviewing the images , we found that detecting high - density wood compared with low - density soft tissue on ct is easier than searching for hypointense wood in the higher signal intensity background on mri . 
 in general , dry wooden fb are porous , gaseous materials radiol med ( 2013 ) 118 : 303310 fig 5a , b axial t1 - weighted mri of porcine muscle shows appearance of each foreign body ( fb ) type . 
however , dry wood in our study was hyperdense to muscle , probably due to its structure containing less gas ( insufcient to produce a low density on ct ) or to the fact that the embedded wood absorbed uid in the specimens and became hyperdense . 
as ct density of muscle in our specimens ( 5060 hu ) was close to that of living individuals ( 5169 hu ) [ 25 ] , the postmortem effect is unlikely to have profoundly altered the tissue . 
susceptibility artefact helps fb detection on mri ; therefore , pulse sequences that enhance the susceptibility artefact , such as frequency - specic fat suppression and long te pulse sequences , can improve fb detection . 
malan 2 , 20097 san donato milanese , italy 2scuola di specializzazione in radiodiagnostica , universit degli studi di milano , via festa del perdono 7 , 20122 milan , italy 3dipartimento di scienze biomediche per la salute , universit degli studi di milano , piazza e . 
malan 2 , 20097 san donato milanese , italy , tel . : + 39 - 02 - 52774468 , fax : + 39 - 02 - 52774925 , e - mail : f.sardanelli@grupposandonato.it received : 20 october 2011 / accepted : 2 january 2012 / published online : 9 august 2012 springer - verlag 2012 abstract purpose . 
pathology revealed 82 malignancies and 20 benign lesions : 70 invasive carcinomas ( 57 ductal , nine lobular , three mucinous , one papillary ) and 12 dcis : 10 broadenomas , two papillomas , two atypical ductal hyperplasias and six other benign lesions . 
sensitivity of aibv was 74% ( 61 / 82 ) , specicity 94% ( 108 / 115 ) , accuracy 86% ( 169 / 197 ) , positive predictive value 90% ( 61 / 68 ) and negative predictive value 84% ( 108 / 129 )  . 
una serie consecutiva di 197 pazienti senza precedenti interventi mammari stata sottoposta a risonanza magnetica ( rm ) bilaterale con mezzo di contrasto ( gadoterato meglumina , 0 , 1 mmol / kg )  . 
i vasi con diametro 2 mm e lunghezza 3 cm sono stati contati sulle proiezioni di massima intensit : una differenza 2 nel numero di questi vasi tra le due mammelle stata considerata iavm . 
la differenza tra sensibilit delliavm per i carcinoma invasivi e quella per i carcinomi duttali in situ ( dcis ) e lassociazione tra liavm e il diametro delle lesioni invasive o il grado ( g ) istologico stata valutata mediante test 2 . 
listopatologia ha rivelato 82 lesioni maligne e 20 benigne : 70 carcinomi invasivi ( 57 duttali , 9 lobulari , 3 mucinosi , 1 papillare ) e 12 dcis ; 10 broadenomi , 2 papillomi , 2 iperplasie duttali atipiche e 6 altre lesioni benigne . 
an association between aibv and ipsilateral cancer exists , particularly for invasive cancers 20 mm or with high pathologic grade . keywords breast cancer magnetic resonance imaging breast vascular map asymmetry diagnostic performance ( 169 / 197 ) , il valore predittivo positivo 90% ( 61 / 68 ) , il valore predittivo negativo 84% ( 108 / 129 )  . 
 parole chiave tumore mammario risonanza magnetica vascolarizzazione mammaria , asimmetria performance diagnostica introduction introduzione magnetic resonance ( mr ) imaging is increasingly used as a diagnostic tool for breast diseases , as demonstrated by a recent national survey in the united states [ 1 ]  . 
accepted indications for breast mr imaging include screening of high - risk women , occult primary breast cancer research , evaluation of response to neoadjuvant chemotherapy , suspected breast cancer recurrence ( when mammography and ultrasonography are not conclusive ) and evaluation of breast implant integrity [ 2 ]  . 
for all of these indications except for evaluation of breast implant integrity , a protocol including a dynamic contrast - enhanced study is required [ 4 ]  . a formalised approach to evaluate and characterise breast lesions using mr imaging came with the breast imaging reporting and data system ( bi - rads ) classication , which introduced the basic differentiation among focus enhancement , masslike enhancement and nonmasslike enhancement . 
breast mr interpretation is now , at best , based on the integration of morphologic and dynamic information [ 4 , 5 ]  . in recent years , several studies have focused on the analysis of whole - breast vascularity on the maximum intensity projections ( mips ) obtained from the subtracted ( enhanced minus unenhanced ) images as additional information available for both breasts , thus allowing comparative evaluation . 
 in this regard , several authors demonstrated an association between the asymmetric increase of breast vascularity and cancers ipsilateral to the breast with the larger vascularity luso della risonanza magnetica ( rm ) nella diagnostica senologica in continuo incremento , come dimostrato recentemente da uno studio condotto negli stati uniti [ 1 ]  . 
 le indicazioni riconosciute alluso della rm mammaria comprendono lo screening delle donne ad alto rischio , la ricerca di un carcinoma mammario occulto , la valutazione della risposta alla chemioterapia neoadiuvante , il sospetto di recidiva di malattia ( nei casi in cui la mammograa e lecograa risultino non conclusive ) e la valutazione degli impianti protesici [ 2 ]  . 
luso della rm per la stadiazione loco - regionale prechirurgica e per la caratterizzazione di reperti dubbi allimaging tradizionale , invece , ancora oggetto di dibattito [ 2 ]  . 
per tutte queste indicazioni , eccezion fatta per la valutazione degli impianti protesici , necessario un protocollo dindagine che includa uno studio dinamico con mezzo di contrasto [ 4 ]  . un approccio standardizzato per valutare e caratterizzare le lesioni mammarie alla rm la classicazione breast imaging report and data system ( bi - rads ) , che ha introdotto la fondamentale distinzione morfologica tra foci di enhancement , enhancement masslike e non - masslike . 
di fatto , linterpretazione della rm mammaria ad oggi basato sullintegrazione di informazioni morfologiche e dinamiche [ 4 , 5 ]  . negli ultimi anni , diversi studi hanno analizzato la vascolarizzazione mammaria sulle ricostruzioni maximum intensity projection ( mip ) ricavate dalle immagini sottratte ( post - contrasto meno pre - contrasto ) come informazione aggiuntiva basata sul confronto tra le due mammelle . 
however , the sample sizes of these studies was relatively small ( ranging from 22 to 106 patients ) , the percentage of ductal carcinoma in situ ( dcis ) on the total number of cancers was highly variable ( ranging from 0% to 21% ) , and one of the studies included only patients with cancer [ 9 ]  . the aim of our study was to estimate , in a large consecutive series of patients , the diagnostic value of breast vascular map asymmetry as a marker of malignancy ipsilateral to the breast with larger vascularity . materials and methods study population and design tra lincremento asimmetrico della vascolarizzazione mammaria e la presenza di un carcinoma ipsilateralmente alla mammella con la vascolarizzazione maggiore [ 611 ]  . 
ad ogni modo , la dimensione del campione di questi studi era relativamente basso ( numero di pazienti compreso tra 22 e 106 ) , la percentuale di carcinomi duttali in situ ( dcis ) sul numero totale di carcinomi era molto variabile ( compreso tra 0% e 21% )  . 
inoltre , uno degli studi comprendeva solo pazienti con lesioni maligne [ 9 ]  . lo scopo del nostro studio stato valutare su unampia serie consecutiva di pazienti la performance diagnostica dellasimmetria della mappa vascolare mammaria come marker di malignit ipsilaterale alla mammella con maggiore vascolarizzazione . this retrospective study was approved by the local ethics committee , and informed consent was waived . 
of 476 studies , 279 were excluded due to conditions that could have inuenced asymmetry of breast vascularity , such as previous breast surgery ( n = 165 ) , breast implants ( n = 29 ) , neoadjuvant chemotherapy ( n = 24 ) , inappropriate menstrual cycle phase ( n = 13 ) and bilateral cancer ( n = 2 )  . 
moreover , we excluded cases of unilateral acquisition ( n = 17 ) , studies with motion artefacts ( n = 14 ) , repeated examinations ( n = 12 ) and examinations interrupted for claustrophobia ( n = 3 )  . 
the remaining 197 patients four men and 193 women with a mean agestandard deviation of 5313 years entered the analysis . mr imaging all breast mr examinations were performed using a 1.5 - t unit ( magnetom sonata maestro class , siemens medical solutions , erlangen , germany ) equipped with a 40 mt / m gradient power and a dedicated four - element , two - channel phased - array coil . 
the dynamic study was performed using a coronal t1 - weighted 3d spoiled fast low - angle shot sequence before and after intravenous injection of 0.1 mmol / kg gadoterate meglumine ( gd - dota , dotarem ; guerbet , paris , france )  . 
technical parameters were : tr = 11 ms , te = 4.8 ms , ip angle = 25 , fov = 384192 mm2 , matrix = 384192 , slice thickness = 1 mm , giving an isotropic voxel size of 111 mm3 . 
the contrast material injection started together with the rst enhanced acquisition , and no time delay was interposed between subsequent contrastenhanced phases . materiali e metodi popolazione e disegno dello studio questo studio retrospettivo stato approvato dal comitato etico locale . 
di queste 476 indagini , 279 sono state escluse per condizioni che avrebbero potuto inuenzare la vascolarizzazione mammaria , tra cui pregressi interventi chirurgici ( n = 165 ) , presenza di impianti protesici ( n = 29 ) , chemioterapia neoadiuvante ( n = 24 ) , fase inappropriata del ciclo mestruale ( n = 13 ) e carcinoma bilaterale ( n = 2 )  . 
inoltre , abbiamo escluso casi di acquisizione unilaterale ( n = 17 ) , studi con artefatti da movimento ( n = 14 ) , indagini ripetute ( n = 12 ) ed esami interrotti per claustrofobia ( n = 3 )  . 
sono stati analizzati ai ni del presente studio i restanti 197 pazienti ( 4 uomini e 193 donne con unet mediadeviazione standard di 5313 anni )  . protocollo rm tutte le indagini sono state eseguite con apparecchiatura da 1 , 5 t ( magnetom sonata maestro class , siemens medical solutions , erlangen , germania ) , attrezzata con gradienti da 40 mt / m e una bobina dedicata phased - array a 4 elementi e 2 canali . 
lo studio dinamico stato eseguito mediante sequenze coronali t1 - pesate 3d spoiled fast low - angle shot prima e dopo iniezione intravenosa di 0 , 1 mmol / kg di gadoterato meglumina ( gd - dota , dotarem ; guerbet , parigi , francia )  . 
i parametri tecnici erano i seguenti : tr = 11 ms , te = 4 , 8 ms , ip angle = 25 , campo di vista = 384192 mm2 , matrice = 384192 , spessore di strato = 1 mm , corrispondente a voxel isotropici di 111 mm3 . 
in b mostrato il metodo di conteggio dei vasi , con un righello applicato al ne di misurare lunghezza e calibro dei vasi . postprocessing and image analysis five postcontrast image series were acquired , and the unenhanced images were used as a mask and subtracted . 
a radiology resident with 3 years of experience in breast mr imaging , blinded to the results of the reference standard , obtained mip reconstructions using the rst dynamic phase in order to have the highest angiographic effect as possible for both arteries and veins [ 8 ]  . 
liniezione del mezzo di contrasto iniziata insieme alla prima acquisizione dinamica e nessun ritardo stato interposto tra le successive sequenze dinamiche . post - processing e analisi delle immagini sono state acquisite cinque serie dinamiche post - contrasto e le immagini pre - contrasto sono state usate come maschera di sottrazione . 
uno specializzando in radiologia con 3 anni di esperienza in rm mammaria , in cieco rispetto ai risultati dello standard di riferimento , ha utilizzato le ricostruzioni mip della prima sequenza dinamica al ne di ottenere il maggior effetto angiograco sia per le arterie che per le radiol med ( 2013 ) 118 : 239250 maximal diameter of enhancing lesions was measured ( in cases of multifocal or multicentric lesions , the largest lesion was considered )  . reference standard of the 197 examinations , 102 showed at least one lesion ascertained with histopathology after surgical excision ( n = 87 ) or core - needle biopsy ( n = 15 )  . 
the remaining 95 examinations were negative ( n = 72 ) or showed benign lesions ( n = 23 ) : they were ascertained with at least 1 year of follow - up with mammography , ultrasonography , and / or mr imaging . statistical analysis the presence of vascular asymmetry was considered a marker of malignancy . 
in particular , the following criteria were adopted : asymmetrically increased vascularity associated with ipsilateral cancer ( invasive carcinomas or dcis ) was considered a true positive , independently from the presence of synchronous contrast - enhancing benign lesion in both breasts ; symmetric breast vascularity associated with unilateral cancer was considered a false negative , independently from the presence of synchronous contrast - enhancing benign lesion in both breasts ; asymmetrically increased vascularity associated with contralateral cancer ( paradoxical asymmetry ) was considered a false negative , independently from the presence of synchronous contrast - enhancing benign lesion in both breasts ; asymmetrically increased vascularity associated with one or more ipsilateral or contralateral benign lesion was considered false positive ; asymmetrically increased vascularity associated with the absence of lesions in both breasts was considered false positive ; symmetrical breast vascularity associated with one or more ipsilateral or contralateral benign lesion was considered true negative ; symmetrical breast vascularity associated with absence of lesions in both breasts was considered true negative . sensitivity , specicity , accuracy and positive ( ppv ) and negative ( npv ) predictive values of vascular asymmetry as a marker of ipsilateral breast cancer were calculated . 
the effect of invasive lesion size on sensitivity was estimated considering the following categories of diameter : < 9 mm , 1014 mm , 1519 mm and 20 m vene [ 8 ]  . 
sulle stesse immagini , il medesimo osservatore ha misurato il diametro massimo delle lesioni con enhancement ( in casi di carcinomi multifocali o multicentrici ha considerato la lesione di maggiori dimensioni )  . standard di riferimento su 197 indagini , 102 hanno mostrato almeno una lesione , successivamente sottoposte a indagine istologica dopo escissione chirurgica ( n = 87 ) o a biopsia core - needle ( n = 15 )  . 
le restanti 95 indagini sono risultate negative ( n = 72 ) o mostravano lesioni benigne ( n = 23 ) : queste indagini sono state rivalutate con mammograa , ecograa e / o rm almeno 1 anno dopo la rm considerata nel presente studio . analisi statistica la presenza di asimmetria vascolare stata considerata come marker di malignit . 
in particolare , abbiamo adottato i seguenti criteri : un incremento asimmetrico della vascolarizzazione associato a un carcinoma omolaterale ( invasivo o dcis ) stato considerato come vero positivo , indipendentemente dalla presenza di lesioni benigne sincrone in entrambe le mammelle ; una vascolarizzazione mammaria simmetrica associata a un carcinoma monolaterale stata considerata come falso negativo , indipendentemente dalla presenza di lesioni benigne sincrone in entrambe le mammelle ; un incremento asimmetrico della vascolarizzazione associato a un carcinoma controlaterale ( asimmetria paradossa ) stato considerato come falso negativo , indipendentemente dalla presenza di lesioni benigne sincrone in entrambe le mammelle ; un incremento asimmetrico della vascolarizzazione associato a una o pi lesioni benigne omolaterali o controlaterali stato considerato come falso positivo ; un incremento asimmetrico della vascolarizzazione in assenza di lesioni mammarie stato considerato come falso positivo ; la simmetria della vascolarizzazione mammaria associata a una o pi lesioni benigne stata considerata come vero negativo ; una simmetria della vascolarizzazione mammaria in assenza di lesioni mammarie stata considerata come vero negativo . abbiamo calcolato sensibilit , specicit , accuratezza , 244 radiol med ( 2013 ) 118 : 239250 moreover , median malignant lesion diameter of false negatives was compared with that of true positives using the mannwhitney u test . 
the 20 benign lesions were identied , as follows : 10 broadenomas , two papillomas , two atypical ductal hyperplasias , one brosclerosis , one adenosis , one phylloid tumour and three other benign lesions . 
sensitivity for invasive cancers ( 80% ; 56 / 70 ; 95%ci , 6989% ) was signicantly ( p < 0.001 ) higher than that for dcis ( 42% ; 5 / 12 ; 95%ci , 1572% )  . 
 moreover , the rate of g12 malignant lesions among false negatives ( 13 / 14 ) was signicantly larger ( p = 0.009 ) than that among true positives ( 28 / 55 )  . 
considering specicity , the median benign lesion diameter of false positives ( 24 mm ) was signicantly larger ( p = 0.011 ) than that of true negatives ( 14 mm )  . examples of true positives , true negatives , false negatives , and false positives are shown in figures 13 . valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) dellasimmetria vascolare come marker di malignit di un carcinoma ipsilaterale . 
 stata valutata linuenza della dimensione delle lesioni invasive sulla sensibilit denendo le seguenti categorie : < 9 mm , 1014 mm , 1519 mm e 20 mlassociazione tra tasso di presenza di incremento asimmetrico della vascolarizzazione mammaria e classi dimensionali delle lesioni invasive stata valutata con test 2 . 
abbiamo trovato in totale 20 lesioni benigne , tra cui 10 broadenomi , 2 papillomi , 2 iperplasie duttali con atipie , 1 brosclerosi , 1 adenosi , 1 tumore lloide e 3 lesioni benigne di altro tipo . 
la prevalenza di cancro risultata del 42% ( 82 / 197 ) , con un rapporto carcinomi invasivi / dcis pari a 70 / 12 ( 5 , 8 )  . performance diagnostica e correlazioni una sintesi della performance diagnostica globale dellincremento asimmetrico della vascolarizzazione ipsilateralmente a una lesione maligna mostrata in tabella 1 . 
la sensibilit per i carcinomi invasivi ( 80% ; 56 / 70 ; 95%ic 6989% ) risultata signicativamente ( p < 0 , 001 ) maggiore di quella per i dcis ( 42% ; 5 / 12 ; 95%ic 1572% )  . 
inoltre , abbiamo osservato una correlazione positiva tra sensibilit e diametro dei carcinomi invasivi ( tabella 2 )  . radiol med ( 2013 ) 118 : 239250 table 1 diagnostic performance of breast vascular asymmetry as a marker of ipsilateral malignancy item point estimation ( % ) tabella 1 performance diagnostica dellasimmetria vascolare mammaria come marker di malignit indicatore stima puntuale ( % ) rapporto 95%ic ( % ) ratio 61 / 82 108 / 115 169 / 197 61 / 68 108 / 129 61 / 82 108 / 115 169 / 197 61 / 68 108 / 129 ratio 2 / 5 9 / 13 15 / 19 30 / 33 56 / 70 2 / 5 9 / 13 15 / 19 30 / 33 56 / 70 95%ci ( % ) 6483 8898 8090 8096 7690 6483 8898 8090 8096 7690 95%ci ( % ) 5 - 85 3991 5694 7698 6989 585 3991 5694 7698 6989 table 2 inuence of lesion diameter on the sensitivity of breast vascular asymmetry for invasive cancers lesion diameter ( mm ) point estimation ( % ) 95%ci , 95% condence interval tabella 2 inuenza del diametro lesionale dei carcinomi invasivi sulla sensibilit dellasimmetria vascolare mammaria diametro lesionale ( mm ) stima puntuale ( % ) rapporto 95%ic ( % ) sensitivity specicity accuracy positive predictive value negative predictive value cancer prevalence 42% 95%ci , 95% condence interval sensibilit specicit accuratezza valore predittivo positivo valore predittivo negativo prevalenza di malattia 42% 95%ic , intervallo di condenza al 95% 1014 1519 20 overall 1014 1519 20 totale 95%ic , intervallo di condenza al 95% discussion mr angiography of the breast is integrated into the standard breast examination when a dynamic 3d contrast - enhanced imaging technique is used . 
as the acquisition time of each postcontrast sequence of the dynamic study is usually between 60 and 120 s , the rst or the second postinjection phase is generally the most suitable for angiographic evaluation [ 8 , 12 ]  . 
in fact , subsequent acquisitions are more dependent on whole - body interstitial diffusion followed by renal excretion of the contrast agent [ 8 , 12 ]  . in the last ten years , several studies evaluated the association between asymmetric increased vascularity and ipsilateral cancer [ 611 ] by using different technical approaches . 
inoltre , il tasso delle lesioni maligne g1 - 2 tra i falsi negativi ( 13 / 14 ) risultato signicativamente maggiore ( p = 0 , 009 ) di quello tra i veri positivi ( 28 / 55 )  . 
considerando la specicit , il diametro mediano delle lesioni benigne falsamente positive ( 24 mm ) risultato signicativamente maggiore ( p = 0 , 011 ) di quello delle lesioni benigne vere negative ( 14 mm )  . esempi di veri positivi , veri negativi , falsi negativi e falsi positivi sono mostrati nelle figure 13 . discussione lo studio vascolare alla rm mammaria integrato nello studio dinamico standard tridimensionale basato sulla somministrazione di mezzo di contrasto . 
in tutti questi casi , le mappe vascolari sono simmetriche ( falsi negativi )  . and a specicity of 57% ; the latter , performed with the same technique and contrast agent but with a dose of 0.2 mmol / kg on 101 patients ( cancer prevalence of 77% and a percentage of dcis on the total number of malignancies equal to 21% ) showed a sensitivity of 72% and a specicity of 100% . in 2008 , using the same semiquantitative method developed in 2005 by our group [ 8 ] schmitz et al . 
 [ 10 ] evaluated 44 patients with 45% cancer prevalence ( percentage of dcis on the total number of malignancies equal to 12% ) with 0.1 mmol / kg of gadobutrol and 3d sequences at 3.0 tena mammaria interna , in termini di quantit e simmetria . 
 dal momento che il tempo di acquisizione di ogni sequenza dinamica post - contrasto solitamente compreso tra 60 e 120 s , la prima o la seconda sequenza post - contrasto sono generalmente le pi adatte per la valutazione angiograca [ 8 , 12 ]  . 
infatti , le sequenze successive sono maggiormente inuenzate dalla diffusione del contrasto nellinterstizio di tutto il corpo e dalleliminazione renale dello stesso [ 8 , 12 ]  . nellultimo decennio , alcuni studi hanno valutato , con differenti approcci tecnici , lassociazione tra lincremento 248 radiol med ( 2013 ) 118 : 239250 fig . 
a , b a 42 - year - old woman presenting with a retroareolar papilloma and a deep retroglandular brosclerosis in the left breast : the vascular map is symmetric , giving a true negative result . 
based on morphological and kinetic analysis , sensitivity was 100% and specicity 74% ; after adjustment for the breast vascularity score , specicity signicantly increased to 87% , without affecting sensitivity . in this study , we adopted the same vessel - counting method to dene vascular asymmetry . 
however , we analysed a larger series of breast mr examinations ( n = 197 ) , including not only malignant lesions but also benign lesions and negative examinations , for an overall cancer prevalence of 42% , which is close to the 50% ideal cancer prevalence for estimating the performance of a diagnostic test . 
 similarly , among benign lesions , false positives resulted in a median lesion diameter ( 24 mm ) larger ( p = 0.011 ) than that asimmetrico della vascolarizzazione e la presenza di un carcinoma ipsilaterale [ 611 ]  . 
il primo studio , eseguito con 0 , 1 mmol / kg di gadopentato dimeglumina e sequenze tridimensionali su una serie di 106 pazienti ( prevalenza di malattia dell80% e percentuale di dcis sul numero totale dei carcinomi del 7% ) , ha mostrato una sensibilit del 77% e una specicit del 57% ; il secondo , eseguito con la stessa tecnica e lo stesso mezzo di contrasto ma con una dose di 0 , 2 mmol / kg su 101 pazienti ( prevalenza di malattia del 77% e una percentuale di dcis sul totale dei carcinomi del 21% ) ha mostrato una sensibilit del 72% e una specicit del 100% . nel 2008 , utilizzando lo stesso metodo semiquantitativo sviluppato nel 2005 dal nostro gruppo [ 8 ] , schmitz et al . 
 [ 10 ] hanno valutato 44 pazienti con una prevalenza di malattia di 45% ( percentuale di dcis sul totale dei carcinomi uguale a 12% ) studiati con 0 , 1 mmol / kg di gadobutrolo e sequenze tridimensionali a 3 , 0 t . 
basandosi sui dati morfologici e cinetici , la sensibilit risultata del 100% e la specicit del 74% ; integrando i dati sulla vascolarizzione mammaria , la specicit aumentata signicativamente al 87% , senza riduzione della sensibilit . in questo studio abbiamo utilizzato il metodo di conteggio dei vasi per denire lasimmetria vascolare , proposto radiol med ( 2013 ) 118 : 239250 fig . 
4a , b axial ( a ) and coronal ( b ) 3d maximum intensity projection images of a 61 - year - old woman presenting with a large multifocal g3 invasive ductal carcinoma in the left breast . 
4a , b maximum intrensity projection tridimensionale in assiale ( a ) e in coronale ( b ) di una donna di 61 anni con un grosso carcinoma duttale inltrante g3 multifocale alla mammella sinistra , con coinvolgimento ipsilaterale dei linfonodi ascellari . 
tuttavia , la presenza di un grosso vaso allinterno della mammella sinistra suggerisce unasimmetria vascolare ipsilaterale . of true negatives ( 14 mm )  . combining these results , we may argue that , regardless of histology ( malignant or benign ) , the larger the lesion , the higher the probability of developing an ipsilateral vascular asymmetry . 
in particular , of seven benign lesions > 23 mm , only three were true negatives ( specicity 43% ) due to the presence of large hypervascularised broadenomas ; similarly , of 27 malignant lesions > 23 mm , 25 were true positives ( sensitivity 93% )  . 
tuttavia , noi abbiamo analizzato una serie pi ampia di pazienti ( n = 197 ) comprendendo non solo lesioni maligne , ma anche lesioni benigne e indagini negative , per una prevalenza di malattia del 42% , vicina alla prevalenza ideale del 50% per la valutazione della performance diagnostica di un test . 
la sensibilit relativamente bassa che abbiamo ottenuto dovuta al numero relativamente alto di falsi negativi che , a loro volta , hanno mostrato un diametro mediano di lesione signicativamente minore di quello dei veri positivi , per i carcinomi invasivi ( 15 mm versus 20 mm ; p = 0 , 016 ) , per i dcis ( 15 mm versus 28 mm ; p = 0 , 030 ) , e per tutte le lesioni maligne ( 15 mm versus 20 mm ; p = 0 , 001 )  . 
 considerando i soli veri positivi , il confronto tra i carcinomi invasivi e i dcis in termini di diametro lesionale ( 20 mm versus 28 mm ) non risultato signicativo ( p = 0 , 188 )  . 
ne deriva lipotesi di un diverso fenomeno biologico nello sviluppo dellasimmetria della mappa vascolare , ovvero che i carcinomi invasivi inducono ( o comunque si associano a ) questa asimmetria con una probabilit maggiore rispetto ai dcis . 
allo stesso modo , relativamente alle lesioni benigne , i falsi positivi hanno mostrato un diametro lesionale mediano ( 24 mm ) maggiore ( p = 0 , 011 ) di quello dei veri negativi ( 14 mm )  . combinando questi risultati , possiamo sostenere che , a prescindere dallistologia ( maligno o benigno ) , la probabilit di osservare una asimmetria vascolare ipsilaterale maggiore allaumentare del diametro della lesione . 
in particolare , su 7 lesioni benigne con diametro maggiore di 23 mm , solo 3 sono risultate veri negativi ( specicit 43% ) a causa della presenza di grossi broadenomi ipervascolarizzati ; analogamente , su 27 lesioni maligne maggiori di 23 mm , 25 sono risultate veri positivi ( sensibilit 93% )  . 
ovviamente , le nostre osservazioni non consentono di trarre conclusioni su un diretto rapporto causa - effetto . riguardo alla correlazione tra il grado patologico dei carcinomi invasivi e lasimmetria vascolare , abbiamo evidenziato che il tasso di lesioni g3 era 49% ( 27 / 55 ) tra i veri positivi e solo 7% ( 1 / 14 ) tra i falsi negativi ( p = 0 , 009 )  . 
first , in the denition of breast vascular map asymmetry , branching vessels may cause problems in counting : in this study , we decided to consider a y - shaped vessel as a twofold vessel ( of course , if satisfying the counting criteria )  . 
this may represent a bias resulting in reduced true positives and consequently underestimated sensitivity . in conclusion , our study conrms the association between the presence of a malignant breast lesion and an ipsilateral vascular asymmetry , in particular for invasive cancers with a diameter > 20 mm or for malignant g3 lesions . 
per prima cosa , i vasi ramicati possono causare problemi nel conteggio : in questo studio abbiamo deciso di considerare un vaso con morfologia a y come due vasi distinti ( ovviamente qualora i criteri di conteggio fossero rispettati )  . 
questo potrebbe rappresentare un bias con conseguente riduzione dei veri positivi e , pertanto , della sensibilit . in conclusione , il nostro studio conferma lassociazione tra la presenza di una lesione maligna e asimmetria vascolare ipsilaterale alla rm mammaria . 
andrea , via di grottarossa 1035 - 1039 , 00189 rome , italy 2division of medical physics , university la sapienza , rome , italy 3department of health science , university of laquila , italy 4department of women health and medicine of the territory , university la sapienza , rome , italy correspondence to : l . 
 312 radiol med ( 2013 ) 118 : 311322 keywords endometrial cancer radiotherapy brachytherapy parole chiave cancro dellendometrio radioterapia brachiterapia introduction introduzione endometrial carcinoma ( ec ) is the most common gynaecological cancer in the western world [ 1 ]  . 
the standard surgical approach consists of laparotomy , peritoneal washing , total hysterectomy and bilateral salpingo - oophorectomy ( th / bso ) with or without lymph node dissection [ 3 ]  . 
 randomised trials have shown that adjuvant pelvic irradiation can decrease the risk of local recurrence but has not been shown to improve overall survival ( os ) [ 4 ]  . 
pathologic risk factors for recurrence include increasing age ( > 6065 years ) , high tumour grade , deep myometrial invasion ( mi ) ( > 50% ) , lymphovascular space invasion ( lvsi ) , and lymph node involvement . 
vaginal cuff brachytherapy ( vbt ) alone may be used as adjuvant treatment for early - stage endometrial cancer , principally for low - risk disease ( stage iab grade 12 ) [ 5 ] or intermediate - risk disease ( stage iab grade 3 , stage ic grade 12 or stage iia grade 1 with < 50% of mi ) [ 6 ] , with satisfactory rates of local control and low rates of acute toxicity [ 7 ]  . 
the postoperative radiation therapy in endometrial carcinoma ( portec ) - 2 trial is the most important study to report results regarding os and disease - free survival ( dfs ) of patients with endometrial carcinoma treated with ebrt and / or vbt ; the enrolled women presented highintermediate risk at diagnosis [ 9 , 10 ]  . 
in addition , we aimed to assess toxicity rates and prognostic factors . materials and methods patient characteristics between september 2007 and february 2011 , 40 patients il carcinoma dellendometrio ( ce ) il tumore ginecologico pi comune nel mondo occidentale [ 1 ]  . 
 la prognosi eccellente nello stadio iniziale , anche se , ci sono sottogruppi ad alto rischio per malattia metastatica , ad esempio , pazienti con classicazione della federazione internazionale di ginecologia e ostetricia ( figo ) stadio ic grado 3 con sopravvivenza globale a 5 anni del 79% [ 2 ]  . 
studi randomizzati hanno dimostrato che lirradiazione pelvica post - operatoria pu diminuire il rischio di recidiva locale , ma non hanno mostrato un miglioramento della sopravvivenza globale [ 4 ]  . 
i fattori di rischio per la recidiva includono let avanzata ( > 6065 anni ) , il basso grado di differenziazione , linvasione profonda del miometrio ( > 50% ) , linvasione dello spazio linfovascolare e il coinvolgimento linfonodale . 
la brachiterapia vaginale ( vbt , vaginal brachytherapy ) pu essere usata da sola come un trattamento adiuvante per i primi stadi del ce , soprattutto per la malattia a basso rischio ( stadio ia - ib g1 - 2 ) [ 5 ] o rischio intermedio ( stadio ia - b g3 , stadio ic g1 - 2 o stadio iia g1 con < 50% di invasione dellmiometrio ) [ 6 ] , ottenendo un controllo locale soddisfacente e con meno tossicit acute [ 7 ]  . 
il post - operative radiation therapy for endometrial carcinoma ( portec ) - 2 lo studio pi importante che riporta risultati attinenti alla sopravvivenza globale e sopravvivenza libera da malattia delle pazienti con carcinoma dellendometrio trattate con radioterapia e / o vbt , le donne arruolate presentavano rischio altointermedio al momento della diagnosi [ 9 , 10 ]  . 
 nel nostro istituto di radioterapia oncologica , quaranta pazienti con tumore dellendometrio sono state trattate con radioterapia a fasci esterni 3d ( ebrt 3d ) e / o con brachiterapia vaginale ad alto dose - rate ( hdr , high doserate vbt )  . 
gli obiettivi dello studio erano di valutare il controllo locale della malattia in termini di sopravvivenza globale ( os , overall survival ) , sopravvivenza libera da malattia ( dfs , disease - free survival ) e sopravvivenza libera da recidiva locale ( lrfs , local relapse free survival )  . 
pretreatment evaluation included patient history , physical examination , complete blood count , platelet count , chest x - ray , endometrial biopsy , endovaginal ultrasound and / or total - body computed tomography ( ct ) scan . 
the pathological stage was dened according to figo 1988 surgical staging syste overall stage distribution was as follows : ia in 2 / 40 ( 5% ) patients ; ib in 9 / 40 ( 22.5% ) patients ; ic in 12 / 40 ( 30% ) patients ; iia in 5 / 40 ( 12.5% ) patients ; iib in 8 / 40 ( 20% ) patients ; iiia in 2 / 40 ( 5% ) patients ; iiic in 2 / 40 ( 5% ) patients . 
grade 2 was the most frequent histological grade , seen in 24 patients ( 60% ) , whereas 12 patients had ( 30% ) grade 3 and four had grade 1 ( 10% )  . 
 patients were dened as low , intermediate or high risk according to the following criteria : pt1 stage with mi 50% and grade 12 for low risk ; pt1 stage with mi 50% and grade 3 ; pt1 stage with mi > 50% and grade 12 for intermediate risk ; pt1 stage with mi > 50% and grade 3 or greater advanced stage for high risk disease . 
 treatment surgery consisted of th / bso without node dissection in 16 patients ( 40% ) or th / bso with bilateral pelvic lymph node dissection in 24 ( 60% )  . 
 the superior border was dened as a line drawn through the l4l5 space , whereas the inferior border was below the obturator canal , including the proximal one half to two thirds of the vagina . 
ebrt was performed to a dose of 45 gy in 25 fractions ve times a week ( 15 patients ) or to 50.4 gy in 28 fractions ve times a week ( 19 patients )  . 
 brachytherapy was administered in all patients 23 materiali e metodi caratteristiche dei pazienti tra settembre 2007 e febbraio 2011 , quaranta pazienti con tumore dellendometrio sono state trattate con radioterapia adiuvante presso il nostro istituto di radioterapia oncologica . 
la valutazione pre - trattamento comprendeva lanamnesi , lesame obiettivo , lemocromo completo con conta delle piastrine , una radiograa del torace , la biopsia dellendometrio , lecograa endovaginale e / o tomograa computerizzata ( tc ) total body . 
il grado istologico di differenziazione pi frequente stato il g2 , osservato in 24 pazienti ( 60% ) , mentre 12 pazienti presentavano g3 ( 30% ) e 4 pazienti presentavano g1 ( 10% )  . 
linvasione del miometrio ( im ) > 50% era presente in 23 pazienti ( 57 , 5% ) , linvasione dello spazio linfovascolare ( islv ) era presente in 4 pazienti ( 10% )  . le pazienti sono state classicate come basso , intermedio o alto rischio secondo i seguenti criteri : pt1 con invasione del miometrio 50% e g1 - 2 come basso rischio ; pt1 con invasione del miometrio 50% e g3 , pt1 con invasione del miometrio > 50% e g1 - 2 come rischio intermedio ; pt1 con invasione del miometrio > 50% e g3 o stadio pi avanzato come alto rischio . 
diciannove pazienti ( 47 , 5% ) presentavano alto rischio , 14 pazienti ( 35% ) presentavano un rischio intermedio e 7 pazienti ( 17 , 5% ) presentavano basso rischio per malattia metastatica . 
le caratteristiche dei pazienti sono riassunte nella tabella 1 . trattamento lintervento chirurgico consisteva nellisterectomia totale e annessiectomia bilaterale senza linfadenectomia ( lad ) in 16 pazienti ( 40% ) , o con dissezione dei linfonodi pelvici bilaterali in 24 pazienti ( 60% )  . 
bladder and rectum were considered organs at risk , with dose constraints as follows : for the bladder , a dose < 80% was delivered to a volume of 5 cc ; for the rectum , a dose < 75% was delivered to a volume of 5 cc and for each fraction . 
vbt regimens were 15 gy in three fractions of 5 gy each for patients receiving previous ebrt ( 34 patients , 85% ) or 21 gy in three fractions of 7 gy each for patients receiving vbt alone ( six patients , 15% )  . 
il bordo superiore stato denito come una linea tracciata attraverso lo spazio l4 - l5 , mentre il bordo inferiore era al di sotto il canale otturatore comprendendo dalla met no ai due terzi prossimali della vagina . 
una dose di 45 gy in 25 frazioni 5 volte a settimana ( 15 pazienti ) o ad una dose di 50 , 4 gy in 28 frazioni 5 volte a settimana ( 19 pazienti ) stata erogata con la radioterapia a fasci esterni . la brachiterapia stata somministrata in tutti le pazienti a 23 settimane dalla ne della radioterapia dopo una visita ginecologica . 
 dfs was calculated from the date of the end of rt course to the date of either distant metastases or locoregional recurrence or date of the last follow - up . 
a p value < 0.05 was considered statistically signicant . results recurrence and survival mean and median follow - ups were 23.22 and 26 ( range 641 ) months , respectively . 
vescica e retto sono stati considerati come organi a rischio con vincoli di dose come segue : per la vescica una dose inferiore a 80% somministrata ad un volume di 5 cc , e per il retto una dose inferiore al 75% somministrata ad un volume di 5 cc per ogni frazione . trentaquattro pazienti ( 85% ) sono state sottoposte a radioterapia pelvica ed hanno ricevuto in seguito un boost brachiterapico al terzo superiore della vagina . 
gli schemi di vbt erano 15 gy in 3 frazioni da 5 gy ciascuna per le pazienti trattate precedentemen te con ebrt ( 34 pazienti , 85% ) , o 21 gy in 3 frazioni da 7 gy per le pazienti trattate solo con vbt ( 6 pazienti , 15% )  . 
quattro pazienti avevano ricevuto carboplatino e paclitaxel : 3 pazienti con alto rischio ( stadio iia , iib e iiia , rispettivamente ) e una paziente con rischio intermedio ( stadio ic g2 )  . 
tutti que ste pazienti avevano ricevuto in seguito ebrt + vbt adiuvante . follow - up e statistica il primo follow - up di valutazione stato eseguito 6 settimane dopo la ne della radioterapia . 
nel follow - up la sorveglianza consisteva nella visita clinica con esame obiettivo , citologia vaginale ogni sei mesi , ecograa endovaginale ed esami radiologici . le tossicit acute gastrointestinali e genitourinarie sono state registrate ogni settimana durante il trattamento e no a 90 giorni dopo . 
le tossicit tardive erano basate sulla scala subjective , objective , management and analytic / late effects on normal tissues ( soma - lent ) [ 12 ]  . la sopravvivenza globale stata calcolata dalla data della diagnosi alla data del decesso per qualsiasi causa o data dellultimo follow - up . 
la sopravvivenza libera da malattia stata calcolata dalla data del termine della radioterapia alla data di comparsa di metastasi a distanza o di recidiva locoregionale o data dellultimo follow - up . 
 la sopravvivenza libera da recidiva locale stata calcolata dalla data della ne della radioterapia alla prima comparsa di recidiva locale o data dellultimo follow - up . lanalisi statistica stata effettuata utilizzando il softwaradiol med ( 2013 ) 118 : 311322 re statistico spss versione 13.0. 
il valore di p < 0 , 05 stato considerato statisticamente signicativo . risultati ricadute e sopravvivenza il follow - up medio e mediano stato di 23 , 22 mesi e 26 mesi , rispettivamente ( range 641 mesi )  . 
 le metastasi linfonodali epatiche si sono vericate in una paziente di 78 anni sottoposta ad istero - annessiectomia bilaterale con linfoadenectomia ( adenocarcinoma dellendometrio con rischio intermedio , stadio ib , g3 ) seguita da radioterapia + brachiterapia hdr adiuvante . 
una paziente di 65 anni presentava tumore dellendometrio ad alto rischio di stadio iib g2 , stata sottoposta ad intervento chirurgico per due delle lesioni polmonari e successivamente a chemioterapia . 
la metastasi polmonari si sono vericate anche in una donna di 58 anni che era stata sottoposta a chemioterapia adiuvante e radioterapia per un adenocarcinoma dellendometrio a rischio intermedio , stadio ic g2 ; lei stata sottoposta a chemioterapia . 
i dettagli su ogni paziente con ricaduta a distanza sono elencati nella tabella 2 . in particolare , nessuna delle pazienti sottoposta alla sola vbt presentava ricaduta di malattia locale o a distanza . 
one 65 - year - old patient with stage iib , grade 2 , high - risk endometrial cancer underwent surgery for two of the lung lesions and subsequent chemotherapy . 
 the other lung recurrence occurred in a 58 - year - old woman who had undergone adjuvant chemotherapy and rt for a ic stage , grade 2 , intermediate - risk endometrial adenocarcinoma . 
la tossicit acuta dovuta allebrt stata osservata in 15 ( 37 , 5% ) pazienti : 11 pazienti ( 27 , 5% ) hanno sviluppato tossicit gastrointestinale di grado 1 - 2 e 9 pazienti ( 22 , 5% ) hanno sviluppato tossicit genitourinaria di grado 1 - 2 . 
non stata osservata nessuna tossicit acuta dopo la sola brachiterapia . le tossicit tardive sono state registrate in 14 pazienti ( 35% ) : latroa vaginale stata osservata in 5 pazienti ( 3 pazienti con grado 1 , 7 , 5% , e 2 pazienti con grado 2 , 5% ) ; le teleangiectasie di grado1 sono state osservate in 7 pazienti ( 17 , 5% ) , lincontinenza urinaria stata osservata in una paziente ( 2 , 5% ) e la diarrea stata osservata in una paziente ( 2 , 5% )  . 
per gli altri fattori analizzati ( et , grado istologico , chemioterapia adiuvante , invasione del miometrio , linfadenectomia , alto rischio ) non stato osservato nessun impatto sulla sopravvivenza libera da malattia . 
allanalisi multivariata , linvasione dello spazio linfovascolare stata identicata come un importante fattore prognostico per la dfs ( p = 0 , 01 )  . discussione il trattamento adiuvante per ridurre il rischio di recidive stato tradizionalmente la ebrt , che attualmente offerta ad un terzo delle donne con cancro dellendometrio , associata o meno alla brachiterapia della cupola vaginale ( vbt ) [ 13 ]  . 
stato trovato un tasso di fallimento pelvico del 6 , 9% con la sola brachiterapia vaginale rispetto al 1 , 9% ( p < 0 , 001 ) con laggiunta della radioterapia a fasci esterni in pazienti con carcinoma dellendometrio di stadio i . 
nello studio del gynecologic oncology group ( gog ) 99 [ 17 , 18 ] sono state arruolate pazienti con stadio ib - iib ( g1 - 3 ) e randomizzate allosservazione o allebrt pelvica ( 50 , 4 gy )  . 
lo studio ha dimostrato che lincidenza delle recidive era pi alta per le pazienti sottoposte ad osservazione ( 12% ) rispetto a quelle sottoposte alla radioterapia ( 4% ) ; non stata segnalata alcuna differenza riguardo la sopravvivenza . 
tuttavia , i sottogruppi di pazienti con grado 3 e con invasione profonda del miometrio ( stadio ic g3 ) sono stati segnalati come a rischio elevato di recidiva sia locoregionale che a distanza . 
 [ 19 ] hanno riportato i tassi di recidiva e di sopravvivenza in 106 pazienti con carcinoma dellendometrio in stadio i ; i risultati clinici mostravano che il carcinoma dellendometrio in stadio ic g2 , 3 e ib g3 era associato con un signicativo aumento del rischio di ricaduta a distanza . 320 radiol med ( 2013 ) 118 : 311322 1.9% ( p < 0.001 ) with the addition of pelvic external rt for stage i endometrial carcinoma patients . 
the incidence of recurrence was higher for patients in the observation arm ( 12% ) compared with the external pelvic rt arm ( 4% ) ; no difference in survival was reported . 
however , subgroups of patients with grade 3 tumours with deep mi ( stage ic grade 3 ) was reported to have a considerably higher risk of both locoregional and distant relapse . 
 [ 19 ] reported relapse and survival rates of 106 patients with stage i endometrial cancer ; outcomes showed that stage ic grade 23 and ib grade 3 endometrial carcinoma was associated with signicantly increased risk of distant relapse . 
 the prospective a study in the treatment of endometrial cancer ( astec ) study [ 20 , 21 ] randomised 1 , 048 women with stage i endometrial cancer to undergo lymph node dissection or standard surgery . 
 the portec - 2 [ 9 , 10 ] randomised trial allocated 427 patients with highintermediate risk endometrial cancer to receive pelvic external irradiation ( 46 gy ) versus vbt ( 21 gy with hdr or 30 gy with ldr )  . 
le ricadu te a distanza si sono vericate in 4 delle nostre pazienti , due di loro avevano stadio iib g2 alla diagnosi , una paziente presentava stadio ic g2 , una paziente presentava stadio ib g3 . 
lo studio prospettico a study in the treatment of endometrial cancer ( astec ) [ 20 , 21 ] ha randomizzato 1048 donne con ce stadio i sottoponendole a linfadenectomia o chirurgia standard . 
lo studio ha dimostrato che la radioterapia adiuvante migliora la sopravvivenza globale rispetto alle pazienti non sottoposte ad rt . il trial randomizzato portec - 2 [ 9 , 10 ] arruol 427 pazienti con cancro dellendometrio a rischio alto - intermedio di ricevere irradiazione pelvica ( 46 gy ) o la brachiterapia vaginale [ 21 gy con hdr o 30 gy con low dose - rate ( ldr ) ]  . 
anche se , un aumento modesto ma statisticamente signicativo delle recidive pelviche si vericato con la sola vbt ( 3 , 6% vs 0 , 7% , p = 0 , 03 )  . 
abbiamo avuto tassi di sopravvivenza simili a quelli riportati in letteratura [ 16 , 2729 ] : sopravvivenza globale del 96 , 4% e sopravvivenza libera da malattia dell86 , 9% , rispettivamente . 
altri hanno identicato tassi simili di effetti avversi acuti e tardivi dopo radioterapia pelvica e / o brachiterapia vaginale [ 30 , 31 ]  . allanalisi univariata e multivariata , abbiamo trovato che il marcatore silver homologue ( silv ) era un fattore prognostico signicativo per la dfs ( p = 0 , 001 e p = 0 , 01 , rispettivamente )  . 
altri non hanno identicato il silv come fattore prognostico signicativo per la sopravvivenza [ 32 ]  . conclusioni la probabilit di recidive locali nei carcinomi dellendometrio bassa dopo chirurgia e radioterapia adiuvante . 
tuttavia la sopravvivenza globale e la sopravvivenza libera da malattia sono simili al trattamento con radioterapia a fasci esterni , mentre nella brachiterapia vaginale la qualit della vita signicativamente migliore con meno effetti tossici soprattutto gastrointestinali . 
rossi pj , jani ab , horowitz ir , johnstone pa ( 2008 ) adjuvant brachytherapy removes survival disadvantage of local disease extension in stage iiic endometrial cancer : a seer registry analysis . 
bolukbasi y , demirci s , ozsaran z et al ( 2008 ) postoperative radiotherapy in intermediate and high - risk stage i endometrial cancer : analysis of prognostic factors and survival . 
rovirosa a , ascaso c , sanchez - reyes a et al ( 2010 ) three or four fractions of 4 - 5 gy per week in postoperative high - dose - rate brachytherapy for endometrial carcinoma . 
jacquier springer , heidelberg dordrecht london new york , 2011 isbn : 978 - 3 - 642 - 18456 - 7 e - isbn : 978 - 3 - 642 - 18456 - 4 published online : 9 august 2012 springer - verlag 2012 the purpose of this 142 page book is to offer the specialist as well as the specialist - in - training and students a large amount of clinical cases describing different sorts of cardiac masses , to be used in their daily practice in cardiac diagnostic work - ow . 
 one will nd a few introductory text pages describing cardiac magnetic resonance imaging techniques and sequences and multi - detector computed tomography image acquisition followed by a few pages dedicated to anatomic pitfall cases ( always to be kept in mind in order to avoid making a wrong diagnosis )  . 
the following pages focus on describing cases of cardiac thrombus , benign tumours , infectious lesions , malignant tumours , and the text closes with synoptic tables and reference lists . the presented cases have been collected by members of the french society of cardiovascular imaging . 
each case is presented with a pertinent short clinical history , very well chosen and reproduced images , nal diagnosis and comments on the presented images , plus tables summarizing pertinent data . this book will surely become a useful companion to cardiologists and radiologists helping them in resolving doubts and difcult diagnostic problems . scopo di questo volumetto di 142 pagine di offrire allo specialista , allo specializzando ed agli studenti una notevole quantit di casi clinici aventi come oggetto differenti tipi di masse cardiache , da utilizzare nella pratica quotidiana nel usso della diagnostica cardiaca . il lettore trover poche pagine di introduzione con la descrizione delle tecniche e sequenze di risonanza magnetica e della acquisizione delle immagini mediante la tomograa computerizzata multi - detettore , seguite da altre poche dedicate a casi di trabocchetti anatomici ( da tenere sempre in mente per evitare diagnosi errate )  . 
le pagine seguenti sono dedicate alla descrizione di casi di trombi cardiaci , tumori benigni , lesioni infettive , tumori maligni , con il testo che si chiude con delle tabelle sinottiche ed un elenco di voci bibliograche . i casi presentati sono stati raccolti da componenti della societ francese di imaging cardiovascolare . 
scuro 10 , 37134 verona , italy 2department of surgery , university of verona , verona , italy 3department of medicine and public health , university of verona , verona , italy correspondence to : m . 
inclusion criteria were incidentally discovered cystic neoplasm of the pancreas with nonmeasurable walls , no mural nodules and no communication with the pancreatic ductal system and who underwent 1 mr / mrcp examination . 
criteri di inclusione sono stati neoplasia cistica pancreatica scoperta incidentalmente con setti sottili , priva di nodulazioni parietali , non comunicante con il sistema duttale pancreatico , sottoposta ad 1 esame di rm / cprm . 
lanalisi delle immagini , alla diagnosi e durante il follow - up , ha incluso : aspetto macroscopico ( micro - , macro - cistico , misto ) , numero di cisti ( uni - , oligo - , multi - cistico ) , diametro massimo della neoplasia . 
il tasso di 164 radiol med ( 2013 ) 118 : 163180 most common , accounting for 48% and 44% of cases , respectively , and showed no change over time . 
 pseudocysts represent 40% of cystic pancreatic lesions and develop as a complication of acute pancreatitis , whereas congenital cysts are rare , representing < 1% of cystic pancreatic lesions [ 8 ]  . cystic pancreatic neoplasms have a different biological behaviour ranging from benign to borderline and malignant lesions . 
intraductal papillary mucinous neoplasms ( ipmns ) , mucinous cystic neoplasms ( mcns ) and pancreatic intraepithelial neoplasms are well - established precursors of invasive carcinoma and warrant surgery [ 3 , 9 , 10 ]  . 
serous cystadenomas ( scas ) show a benign biological and clinical course , with no indication for surgery but for clinicalradiological follow - up only [ 1 , 1014 ]  . 
benign cystic pancreatic neoplasms are characterised by thin walls , sharp margins , lack of mural nodules , homogeneously thin septae , no signs of communication with the pancreatic duct system and are detected in patients without any history of acute or chronic pancreatitis . 
 the medical need for clinicalradiological follow - up of incidentally detected benign noncommunicating cystic neoplasms ( bncns ) is due to their potential growth over time , especially lesions > 4 cm [ 18 ]  . 
 because of its high tissue contrast and multiplanar capacity , magnetic resonance ( mr ) imaging is accurate in diagle lesioni cistiche pancreatiche vengono diagnosticate con una frequenza in costante aumento nella popolazione generale , con una prevalenza che varia tra il 2 , 6% ed il 19 , 6% ed aumenta con laumentare dellet dei pazienti ; ci giusticato dai progressi tecnologici nelle tecniche di diagnostica per immagini e dal loro crescente utilizzo [ 17 ]  . 
le pseudocisti , che rappresentano una complicanza della pancreatite acuta , costituiscono il 40% delle lesioni cistiche pancreatiche , mentre le cisti congenite sono aneddotiche e costituiscono meno dell1% dei casi [ 8 ]  . le neoplasie cistiche pancreatiche presentano un comportamento biologico che pu variare dal benigno , al borderline no al francamente maligno . 
le neoplasie intraduttali papillari mucinose ( ipmns ) , le neoplasie cistiche mucinose ( cmns ) e le neoplasie pancreatiche intraepiteliali , ad esempio , sono noti precursori dei rispettivi carcinomi invasivi e , per questo , sono candidate a resezione chirurgica [ 3 , 9 , 10 ] ; il cistoadenoma sieroso ( cas ) , invece , presenta un comportamento biologico tipicamente benigno e , quindi , non necessita di resezione chirurgica , bens di un follow - up clinico - radiologico [ 1 , 1014 ]  . la corretta caratterizzazione delle neoplasie cistiche pancreatiche scoperte incidentalmente di fondamentale importanza al ne di valutare correttamente i potenziali rischi ad esse correlati e di evitare procedure chirurgiche non necessarie [ 1 , 1517 ]  . 
si possono denire benigne quelle neoplasie cistiche pancreatiche con pareti e setti omogeneamente sottili , margini netti , assenza di nodulazioni parietali e assenza di comunicazione con il sistema duttale , scoperte incidentalmente in un paziente senza reperti anamnestici di pancreatite acuta o cronica . la necessit di un follow - up clinico - radiologico per le neoplasie cistiche benigne non comunicanti con il sistema duttale pancreatico ( bncns ) scoperte incidentalmente correlata al loro potenziale incremento volumetrico radiol med ( 2013 ) 118 : 163180 nosing and characterising incidentally discovered bncns by means of t2 - weighted images and in depicting the relationship between the lesion and pancreatic ductal system by means of mr cholangiopancreatography ( mrcp ) images [ 4 , 1924 ]  . 
 the objective of our study was to determine mr / mrcp imaging features of incidentally discovered pancreatic bncns to assess their evolution over time and identify mr / mrcp imaging features predictive of tumour growth . materials and methods patient population our retrospective study was approved by the investigational review board and the requirement for informed consent was waived . 
from our institutions medical records , pathology and radiology database , we retrieved all patients with diagnosis of cystic pancreatic neoplasm treated between january 2003 and may 2010 for inclusion in our study . 
inclusion criteria were incidentally discovered cystic pancreatic neoplasm with nonmeasurable wall and lack of mural nodules , absence of communication with the pancreatic ductal system and availability of one or more mr / mrcp examinations . 
the absence of communication between the neoplasm and the pancreatic ductal system was evaluated preliminarily by two observers independently , both on thick - slab mrcp images and on the coronal and axial t2 - weighted images included in our protocol ( table 1 )  . 
exclusion criteria were history of acute pancreatitis , more than two cystic neoplasms / patient , cystic lesions communicating with the pancreatic ductal system , cystic lesions with thick walls and / or mural nodules , cystic lesions with peripheral eggshell calcications at computed tomography ( ct ) , presence of symptoms referable to the lesion at diagnosis , patients who underwent mr / mrcp examinations at other centres , poor mr image quality and presence of von hippel - lindau disease . 
the study population comprised 62 patients with a median age of 58.6 ( range , 22.284.0 ) years consisting of 41 women ( median age , 54.8 years ; range , 22.284.0 years ) and 21 men ( median age , 62.9 years ; range , 36.977.5 years ) , with a male / female ratio of 1 / 1.95. 
conversely , 47 / 62 ( 76% ) patients underwent clinicalradiological follow - up with a median 19.5 ( range , 761 ) months and a median nel tempo , fatto questo pi evidente per quelle lesioni con diametro maggiore di 4 cm [ 18 ] ; tale crescita pu rendere sintomatiche tali neoplasie come conseguenza delleffettomassa esercitato nei confronti delle strutture adiacenti . grazie alla sua elevata risoluzione di contrasto ed alla sua multiplanariet , la risonanza magnetica ( rm ) una metodica accurata per la diagnosi e la caratterizzazione delle neoplasie cistiche pancreatiche , in particolare mediante lutilizzo di immagini t2 - dipendenti e di immagini di colangio - pancreatograa con rm ( cprm ) , queste ultime particolarmente utili per chiarire i rapporti tra la neoplasia ed il sistema duttale [ 4 , 1924 ]  . lobiettivo del nostro studio stato quello di descrivere gli aspetti rm / cprm delle neoplasie cistiche benigne non comunicanti con il sistema duttale pancreatico ( bncns ) scoperte incidentalmente e di valutare la loro evoluzione nel tempo , ricercando eventuali aspetti rm / cprm predittivi di una loro crescita . materiali e metodi popolazione di pazienti il nostro studio retrospettivo stato approvato dal comitato etico del nostro istituto ; non stata necessaria lacquisizione di un consenso informato . 
sono stati considerati per linclusione tutti i pazienti affetti da neoplasia cistica pancreatica evidenziati mediante una ricerca tra i referti radiologici , anatomo - patologici e clinici del nostro policlinico , tra gennaio 2003 e maggio 2010 . 
i criteri di inclusione sono stati : neoplasie cistiche pancreatiche , scoperte incidentalmente , con pareti e setti uniformemente sottili , prive di nodulazioni parietali e di comunicazione con il sistema duttale pancreatico , sottoposte ad almeno un esame di rm / cprm . 
lassenza di comunicazione tra la neoplasia ed il sistema duttale pancreatico stata valutata , preliminarmente , da due osservatori , in modo indipendente , sulle immagini di cprm a strato spesso e sulle immagini t2 - dipendenti , coronali ed assiali , incluse nel nostro protocollo di esame ( tabella 1 ) ; sono state escluse dallo studio tutte quelle neoplasie in cui una comunicazione con il sistema duttale fosse sospettata da parte di uno o di entrambi i radiologi . 
i criteri di esclusione sono stati : presenza di comunicazione , sospetta o accertata , con il sistema duttale pancreatico , reperto anamnestico di pancreatite acuta o cronica , pi di due neoplasie cistiche nello stesso paziente , presenza di ispessimenti o nodulazioni parietali , presenza di calcicazioni periferiche in precedenti esami tc , presenza di sintomi correlabili con la neoplasia al momento della diagnosi , esami di rm / cprm eseguiti solo presso altre sedi , malattia di von hippel - lindau . 
la popolazione in studio ha compreso quindi 62 pazienti con unet mediana di 58 , 6 anni ( range 22 , 284 , 0 anni ) , di cui 166 radiol med ( 2013 ) 118 : 163180 number of mr / mrcp examinations of three ( range , two to seven ) examinations . 
 magnetic resonance imaging mr imaging was performed on a 1.5 - t scanner ( magnetom symphony , siemens , erlangen , germany ) using a 4 - channel phased - array coil . 
to eliminate overlapping uid - containing organs on t2 - weighted images , 50150 ml of superparamagnetic iron oxide particles ( ferumoxsil , lumirem , guerbet , aulnay - sous - bois , france ) were administered 10 - 20 min imaging . 
a quadriphasic dynamic study was performed during injection of 0.1 mmol / kg body weight of gadolinium chelates at a ow rate of 22.5 ml / s 41 femmine ( et mediana 54 , 8 anni ; range 22 , 284 , 0 anni ) e 21 maschi ( et mediana 62 , 9 anni ; range 36 , 977 , 5 anni ) , con un rapporto maschi / femmine di 1 / 1 , 95 . 
quindici / 62 ( 24% ) pazienti sono stati sottoposti a resezione chirurgica della neoplasia dopo il primo esame rm / cprm , per dubbi diagnostici con neoplasie cistiche mucino - secernenti in 11 / 15 ( 73 , 3% ) casi e per volere personale del paziente nei rimanenti 4 / 15 ( 26 , 7% )  . 
quarantasette / 62 ( 76% ) pazienti , invece , sono stati sottoposti ad un follow - up clinico - radiologico , con una mediana di followup di 19 , 5 mesi ( range 761 mesi ) e con un numero mediano di 3 esami rm / cprm ( range 27 esami )  . 
per 24 / 62 pazienti stato possibile ottenere una conferma istologica riguardo la natura della neoplasia : in 15 / 24 casi dopo resezione chirurgica ed in 9 / 24 per mezzo di una biopsia percutanea . 
 allesame isto - patologico tutte le 24 lesioni analizzate sono risultate essere cistoadenomi sierosi . imaging di risonanza magnetica tutti gli esami di rm sono stati eseguiti con un apparecchio con magnete da 1 , 5 t ( magnetom symphony , siemens , erlangen , germania ) , utilizzando una bobina a quattro canali phased array . 
the dynamic study included a pre - contrast - phase , late - arterial / pancreatic phase ( 3545 s ) , portal venous phase ( 7580 s ) and delayed phase ( > 180 s )  . 
quantitative image analysis was performed by a third radiologist ( mdo with 10 years of experience ) on axial and coronal t2 - weighted [ half - fourier - acquisition single shot turbo spin echo ( haste ) ] images using an electronic calliper on magnied images , when necessary . 
 qualitative analysis comprised the following parameters : bncn site ( head or body / tail ) ; macroscopic pattern ( microcystic , diameter of all cysts < 2 cm ; macrocystic , diameter of all cysts 2 cm ; mixed ) ; number of cysts ( unicystic ; oligocystic , < 6 cysts ; multicystic , 6 cysts ) ; signal intensity of cystic content on t1and t2 - weighted images compared with adjacent pancreatic parenchyma ; presence / absence of central scar , presence / absence of septa and / or cystic - wall contrast enhancement , main pancreatic duct ( mpd ) pattern ( linear / tortuous ) ; upstream mpd endoluminal - lling defects ( present / absent ) ; dilated side branches in upstream ductal system ( present / absent ) ; signal intensity of upstream pancreatic parenchyma on t1 - weighted images ( hypo - / isointense )  . 
we evaluated maximum lesion diameter ( by measuring the maximum diameter in both the axial and coronal planes and noting the largest one ) ; 3d volume of the bncn calculated using a formula assuming an ellipsoid conguration ( v = 4 / 3 pa / 2b / 2c / 2 = p / 6 abc ) where a , b and c are the orthogonal maximum diameters of the bncn ; maximum diameter of the upstream and downstream main pancreatic duct ; ratio between upstream and downstream main pancreatic duct diameter . 
 in patients undergoing clinicalradiological follow - up , results of qualitative and quantitative image analysis performed on follow - up mr / mrcp images were compared with those recorded at diagnosis . 
quantitative changes over time were assessed : annual variations were calculated according to the following formula : [ ( last observation value rst observation value ) / observation period ] 12 and expressed as mean values and ranges . 
 eliminare la sovrapposizione del segnale proveniente dai uidi intestinali nelle acquisizioni t2 - dipendenti , sono stati somministrati , 1020 minuti prima dellesame , 50150 ml di particelle di ossido di ferro con effetto superparamagnetico ( ferumoxsil , lumirem , guerbet , alunay - sous - bois , francia )  . 
lo studio dinamico , durante somministrazione endovena ( ev ) di chelati del gadolinio , stato eseguito mediante sequenze gradient echo 3d volumetriche ( volumetric interpolated breath - hold examination , vibe , dimensione del voxel 1 , 30 , 83 , 0 mm , matrice 235256512 ) utilizzando una tecnica di imaging parallelo ( fattore di accelerazione grappa 2 )  . 
stato eseguito uno studio quadrifasico durante la somministrazione ev di 0 , 1 mmol / kg di peso corporeo di chelati del gadolinio ( multihance , bracco , milano , italia ; magnevist , schering , berlino , germania ) attraverso un iniettore automatico ( spectris , medrad , pittsburgh , pennsylvania , usa ) con un usso di 22 , 5 ml / s . 
sono state acquisite immagini in fase pre - contrastograca , in fase arteriosa pancreatica ( 3545 s ) , in fase venosa portale ( 75 80 s ) ed in fase tardiva ( > 180 s )  . analisi delle immagini lanalisi qualitativa delle immagini rm / cprm stata eseguita su di una workstation da due radiologi , rm e mb , con 15 e 3 anni di esperienza in radiologia gastrointestinale , rispettivamente , che erano a conoscenza della diagnosi di neoplasia cistica benigna del pancreas . 
lanalisi quantitativa delle immagini stata eseguita da un terzo radiologo , mdo , 10 anni di esperienza in radiologia gastrointestinale , su immagini t2 - dipendenti half - fourier single - shot turbo spin - echo ( haste ) assiali e coronali , ingrandite laddove necessario . 
le analisi qualitativa e quantitativa sono state eseguite sia sulle immagini ottenute alla diagnosi che su quelle ottenute durante leventuale follow - up utilizzando i medesimi criteri . lanalisi qualitativa ha incluso : localizzazione della bncn ( testa o corpo / coda ) ; pattern macroscopico ( microcistico : tutte cisti con diametro massimo < 2 cm , macrocistico : tutte cisti con diametro 2 cm , o misto : coesistenza dei precedenti aspetti ) ; numero di cisti ( unicistico , oligocistico : < 6 cisti , multicistico : 6 cisti ) ; intensit di segnale del contenuto cistico nelle immagini t1e t2 - dipendenti rispetto al parenchima pancreatico adiacente ( ipo - , isoo iper - intenso ) ; presenza o assenza di una cicatrice centrale ; presenza o assenza di impregnazione di contrasto da parte delle pareti delle cisti ; aspetto del dotto pancreatico principale ( dpp ) ( lineare o tortuoso ) ; presenza o assenza di difetti di riempimento nel dpp e di dilatazione di dotti pancreatici di secondo ordine a 168 statistical analysis interobserver variability was assessed for qualitative image analysis parameters . 
measurements obtained on mr / mrcp images at diagnosis and at last follow - up examination were compared with the paired - samples t test ( conrmed with the wilcoxon signed ranks test )  . 
for this purpose , in all bncns that underwent follow - up , we calculated the percentage of annual variation of tumour volume compared with baseline , as follows : { [ ( last observation value rst observation value ) 100 / rst observation value ] / observation period } 12 . subsequently , we subdivided our patient population into two groups according to the median percentage annual variation of tumour volume : bncns that showed an annual increase in volume 10% ( 25 lesions ) and those with an increase in volume > 10% ( 24 lesions )  . 
comparison between these two groups was conducted with fishers exact test for categorical variables and with the mannwhitney test for continuous variables . furthermore , a multivariate analysis was performed with the binary logistic regression model to evaluate the relative role of the mr / mrcp imaging parameters in predicting lesion enlargement considering age , sex , site , number of cysts ( oligocystic , multicystic ) , central scar , septa / wall enhancement and mpd morphology as potential confounders . 
 lesion site : 37 / 64 ( 58% ) bncns were located in the pancreatic head and 27 / 64 ( 42% ) in the body / tail of the gland . 
 macroscopic pattern : 31 / 64 ( 48% ) bncns showed a mixed pattern ; 28 / 64 ( 44% ) a microcystic pattern ; and 5 / 64 radiol med ( 2013 ) 118 : 163180 monte della bncn ; intensit di segnale del parenchima pancreatico a monte della bncn nelle immagini t1 - dipendenti , rispetto a quello a valle ( ipo - , isoo iper - intenso )  . lanalisi quantitativa stata eseguita su immagini t2dipendenti secondo i piani assiale e coronale . 
sono stati valutati : il diametro massimo della lesione ( misurando il diametro massimo sia sul piano assiale che su quello coronale ed annotando il maggiore ) , volume tridimensionale ( calcolato utilizzando la formula dellellissoide : v = 4 / 3a / 2b / 2c / 2 = / 6 abc , dove a , b e c sono i diametri massimi ortogonali della lesione ) , diametro massimo del dpp a monte ed a valle della lesione , rapporto tra diametro del dpp a monte ed a valle . nei pazienti sottoposti a follow - up clinico - radiologico i risultati delle analisi qualitativa e quantitativa eseguite durante il follow - up sono stati valutati a confronto con quelli eseguiti alla diagnosi . 
le variazioni quantitative nel tempo secondo state calcolate con la formula [ ( valore allultima osservazionevalore alla prima osservazione ) / periodo di osservazione ] 12 , e sono state espresse come valori medi e range . analisi statistica stata calcolata la variabilit inter - osservatore nella valutazione dei parametri qualitativi ; la forza della concordanza stata classicata nel modo seguente : < 0 , 20 scarsa , 0 , 210 , 40 intermedia , 0 , 410 , 60 moderata , 0 , 610 , 80 buona , 0 , 811 , 0 ottima . 
le misurazioni eseguite sulle immagini rm / cprm alla diagnosi ed allultimo follow - up sono state confrontate mediante il test t di student per campioni appaiati ( confermato mediante il test di wilcoxon per ranghi )  . al ne di identicare gli aspetti rm / cprm predittivi di una crescita delle lesioni abbiamo eseguito sia una analisi univariata che una analisi multivariata . 
per tale scopo , per tutte le lesioni sottoposte a follow - up abbiamo calcolato lincremento volumetrico annuo percentuale rispetto al valore di base come segue : { [ ( valore allultima osservazionevalore alla diagnosi ) 100 / valore alla prima osservazione ] / periodo intercorso } 12 . 
 in seguito abbiamo suddiviso i pazienti in 2 gruppi basandoci sul valore mediano di crescita volumetrica percentuale annua calcolata , che risultato essere 10% : abbia mo cos ottenuto un gruppo di 25 bncns con aumento volumetrico percentuale annuo 10% ed un altro di 24 bncns con aumento volumetrico percentuale annuo > 10% . 
il confronto tra questi due gruppi stato eseguito mediante il fischer exact test , per le variabili categoriali , e mediante il radiol med ( 2013 ) 118 : 163180 fig . 
 axial t2 - weighted haste ( tr / te ( cid : 31 ) / 102 ) magnetic resonance ( mr ) image clearly shows the presence of a central scar ( arrow ) , pathognomonic for serous cystadenoma , in the lesion located in the body / tail ; upstream to this lesion , a dilation of the main pancreatic duct with a tortuous pattern is appreciable ( a )  . 
1a , b due neoplasie cistiche pancreatiche benigne non comunicanti con il dotto pancreatico principale con aspetto microcistico , localizzate nella testa e nel corpo - coda della ghiandola , scoperte incidentalmente nel medesimo paziente . 
a limmagine haste [ tempo di ripetizione ( tr ) / tempo di eco ( te ) ( cid : 31 ) / 102 ] t2 - dipendente orientata secondo il piano assiale mostra la presenza di una cicatrice centrale ( freccia ) , patognomonica per cistoadenoma sieroso , nel contesto della neoplasia localizzata al corpo - coda ; apprezzabile una dilatazione del dotto pancreatico principale a monte di tale lesione . 
 qualitative image analysis at follow - up inoltre stata eseguita una analisi multivariata mediante il modello di regressione logistica lineare per valutare il ruolo relativo dei parametri rm / cprm nella predizione dellingrandimento della lesione , considerando let , il sesso , il numero di cisti , la presenza di cicatrice centrale , limpregnazione di contrasto dei setti e delle pareti e la morfologia del dpp quali potenziali fattori confondenti . 
in particular , the bncn macroscopic pattern ( microcystic ; macrocystic ; mixed ) did not change during follow - up in any lesion . i risultati dellanalisi qualitativa alla diagnosi sono riportati in tabella 2 . le lesioni avevano le seguenti localizzazioni : 37 / 64 ( 58% ) neoplasie cistiche benigne non comunicanti con il si170 radiol med ( 2013 ) 118 : 163180 fig . 
 axial t2 - weighted haste ( tr / te ( cid : 31 ) / 102 ) mr image shows the lobulated margins of the lesion and the presence of a central scar ( arrow ) , which is pathognomonic for serous cystadenoma , in the rst patient . 
a limmagine assiale haste ( tr / te ( cid : 31 ) / 102 ) t2 - dipendente si apprezza la lobulatura dei margini lesionali e la presenza di una cicatrice centrale ( freccia ) , patognomonica per cistoadenoma sieroso . 
b limmagine assiale gradient echo ( tr / te 4 , 5 / 1 , 7 ms ) t1 - dipendente con saturazione selettiva del segnale del tessuto adiposo ottenuta durante la fase venosa portale dello studio dinamico nel medesimo paziente dimostra la presa di contrasto da parte della cicatrice centrale e dei setti intralesionali ( freccia ) ; non si apprezza presa di contrasto da parte del contenuto delle cisti . 
nessuno dei parametri qualitativi osservati alla diagnosi si modicato durante il follow - up nel gruppo di 49 neoplasie seguite nel tempo parametri prevalenza ( % ) 172 radiol med ( 2013 ) 118 : 163180 fig . 
3a , b unicystic , benign , noncommunicating , cystic neoplasm of the pancreatic head with macrocystic pattern , incidentally discovered in a patient without any history of acute or chronic pancreatitis . 
3a , b neoplasia cistica benigna del pancreas non comunicante con il dotto pancreatico principale con aspetto unicistico macrocistico scoperta incidentalmente in un paziente senza storia di pancreatite acuta o cronica . 
b limmagine gradient echo ( tr / te 4 , 5 / 1 , 7 ms ) t1 - dipendente ottenuta durante la fase arteriosa dello studio dinamico la lesione mostra margini netti , assenza di setti o nodulazioni parietali e pareti uniformemente sottili . 
mean maximum downstream mpd diameter and upstream / downstream mpd diameter ratio showed no signicant difference during the follow - up period ( p = 0.33 and p = 0.14 , respectively ) ( table 3 )  . analisi qualitativa al follow - up nessuno dei parametri inclusi nellanalisi qualitativa ha mostrato variazioni tra la diagnosi ed il follow - up . 
in particolare , laspetto macroscopico ( microcistico , macrocistico o misto ) delle bncns non ha in alcun caso mostrato cambiamenti nel tempo . analisi quantitativa alla diagnosi il diametro massimo mediano di tutte le bncns alla diagnosi risultato essere di 35 , 5 mm ( range 15136 mm ) , con un volume 3d stimato mediano di 15 , 3 cm3 ( range 0 , 6 1075 cm3 )  . 
 considerando solamente le 49 / 64 ( 77% ) bncns sottoposte a follow - up , esse presentavano un diametro massimo mediano alla diagnosi di 35 , 0 mm ( range 15136 mm ) ed un volume 3d stimato mediano di 14 , 9 cm3 ( range 0 , 61075 cm3 ) ; il gruppo di 15 / 64 ( 23% ) lesioni sottoposto a resezione chirurgica dopo il primo esame rm / cprm presentava invece un diametro massimo mediano alla diagnosi di 37 , 0 mm ( range 1785 mm ) ed un volume 3d stimato mediano di radiol med ( 2013 ) 118 : 163180 table 3 benign noncommunicating cystic pancreatic neoplasms that underwent clinicalradiological follow - up ( n = 49 ) ; median follow - up time 19 months ( range , 761 months )  . 
4a , b mixed - type , benign , noncommunicating , cystic neoplasm of the pancreatic head that increased in size over time ( follow - up 31 months )  . 
axial t2 - weighted haste ( tr / te ( cid : 31 ) / 102 ) ( a ) at diagnosis compared with axial t2 - weighted rapid acquisition with relaxation enhancement ( rare ) follow - up mr image ( tr / te 4 , 500 / 102 ) obtained 31 months later ( b )  . 
 immagine assiale haste ( tr / te ( cid : 31 ) / 102 ) t2 - dipendente alla diagnosi ( a ) valutata a confronto con immagine assiale rapid acquisition with relaxation enhancement ( rare ) ( tr / te 4500 / 102 ) t2 - dipendente di follow - up eseguita 31 mesi pi tardi ( b )  . 
il diametro massimo della neoplasia passato da 46 a 61 mm in 31 mesi , con una crescita di 5 , 9 mm / anno . 174 radiol med ( 2013 ) 118 : 163180 results of univariate analysis for mr / mrcp imaging features that may predict lesion enlargement during followup are reported in table 4 . 
in particular , features that showed a signicant correlation with a > 10% annual increase in bncn volume were macroscopic pattern namely , macrocystic or mixed ( p < 0.001 ) and tumour size ( p < 0.001 ) ( table 4 )  . 
 as for tumour size , the multivariate analysis conrmed the direct relationship between lesion diameter at diagnosis and risk of tumour enlargement : in particular , each 5 mm more in lesion diameter at diagnosis corresponded to a 1.89 - fold increased risk of tumour growth ( tables 4 and 5 )  . 
 discussion medical diagnostic requirements in incidentally discovered pancreatic bncns are twofold : to differentiate these lesions from potentially or frankly malignant cystic pancreatic neoplasms ; to perform a follow - up , as their evolution over time is variable , with some lesions remaining stable and some tending to grow [ 18 ]  . 
in these cases , wall thickness may be a useful sign for the differential diagnosis [ 17 ]  . all incidentally discovered bncns were hyperintense on t2 - weighted images , with high contrast - to - noise ratio with the adjacent pancreatic parenchyma , which appears hypointense on t2 - weighted images . 
considerando solo le 15 / 64 ( 23% ) bncns resecate , esso presentava un valore mediano di 3 , 5 mm ( range 25 mm ) , mentre considerando solamente le 49 / 64 ( 77% ) lesioni sottoposte a follow - up tale valore era di 2 , 0 mm ( range 110 mm )  . 
la mediana tra i rapporti tra diametro del dpp a monte ed a valle delle bncns presentava un valore di 1 , 0 ( range 0 , 55 )  . 
considerando solo le 15 / 64 ( 23% ) bncns resecate tale valore era uguale a 1 , 8 ( range 0 , 75 ) , mentre considerando solamente le 49 / 64 ( 77% ) sottoposte a follow - up tale valore era uguale a 1 , 0 ( range 0 , 52 , 5 )  . analisi quantitativa al follow - up il diametro massimo mediano delle bncns allultimo follow - up ( per le 49 bncns sottoposte a follow - up ) risultato 38 , 0 mm ( range 15139 mm ) , con un volume 3d stimato mediano di 17 , 4 cm3 ( range 0 , 71169 , 7 cm3 ) ( tabella 3 )  . 
la mediana dei rapporti tra dotto pancreatico medio ( mpd ) a monte ed a valle delle bncns risultata 1 , 0 ( range 0 , 52 , 5 )  . 
il valore medio del diametro massimo del dpp a monte delle lesioni ha presentato un incremento di 0 , 1 mm / anno ( range 0 , 01 , 5 mm / anno ) ( p = 0 , 025 ) , mentre il diametro massimo del dpp a valle delle bncns ed il rapporto tra dpp a monte ed a valle non hanno mostrato signicative variazioni ( p = 0 , 33 e p = 0 , 14 , rispettivamente ) ( tabella 3 )  . i risultati dellanalisi univariata riguardante i parametri rm / cprm potenzialmente predittivi di un incremento volumetrico delle bncns sono riportati in tabella 4 . 
nella nostra casistica , gli aspetti rm / cprm che hanno mostrato una correlazione signicativa con un signicativo aumento volumetrico della bncns ( > 10% annuo ) sono stati laspetto macroscopico , in particolare il pattern macrocistico o misto ( p < 0 , 001 ) , ed il diametro massimo della lesione ( p < 0 , 001 )  . 
the same slice on axial t2 - weighted haste ( tr / te ( cid : 31 ) / 102 ) mr image demonstrates that all cysts appear hyperintense , with the same signal intensity ( b )  . 
la paziente stata sottoposta a duodenocefalopancreasectomia ; lanalisi istologica ha rivelato la presenza di un cistoadenoma sieroso con aspetto misto e con segni di sanguinamento nel contesto della cisti di maggiori dimensioni . 
a limmagine gradient echo ( tr / te 4 , 5 / 1 , 7 ms ) t1 - dipendente con saturazione selettiva del segnale del tessuto adiposo mostra un contenuto isointenso nel contesto della cisti di maggiori dimensioni ( iperintenso rispetto alla altre cisti ) come risultato di un effetto paramagnetico . 
b limmagine haste ( tr / te ( cid : 31 ) / 102 ) dimostra come tutte le cisti presentino la medesima iperintensit di segnale nelle immagini t2 - dipendenti . 
 during follow - up , qualitative image parameters showed no variation ; in particular , lesion morphology did not change over time , suggesting that microcystic , mixed and macrocystic neoplasms are not different evolutive steps of the same i risultati dellanalisi multivariata sono riportati in tabella 5 . 
le neoplasie cistiche benigne non comunicanti con il sistema duttale pancreatico con aspetto macroscopico macrocistico o misto hanno presentato un aumento volumetrico 4 , 78 volte maggiore rispetto a quelle con aspetto microcistico . 
laspetto macrocistico nel caso di neoplasie cistiche pancreatiche asintomatiche rappresenta tuttora una sda per il radiologo , poich esso pu essere apprezzabile sia per neoplasie benigne che per neoplasie pre - maligne o francamente maligne ; in questi casi la valutazione dello spessore delle pareti pu essere un parametro utile per una corretta differenziazione [ 17 ]  . tutte le bncns scoperte incidentalmente hanno presentato un contenuto cistico iperintenso nelle immagini t2 - dipendenti , con un elevato rapporto segnale - rumore nei confronti del parenchima pancreatico adiacente , che appariva ipointenso . 
in tutti i 6 casi tale effetto era dovuto alla pre176 radiol med ( 2013 ) 118 : 163180 table 4 univariate analysis of benign noncommunicating cystic pancreatic neoplasms that underwent clinicalradiological follow - up ( n = 49 )  . 
this suggests that small bncns ( < 3cm ) can be safely referred for a longinterval clinicalradiological follow - up because of the low risk of tumour growth [ 27 , 28 ]  . 
 senza di segni di sanguinamento intralesionale , fatto questo confermato allanalisi istologica . durante il periodo di follow - up tutti i parametri qualitativi analizzati non hanno mostrato alcuna variazione ; in particolare , laspetto morfologico delle lesioni non si mai modicato , fatto questo che suggerisce come le neoplasie microcistiche , miste e macrocistiche non siano differenti passaggi evolutivi di una stessa lesione , ma bens entit completamente differenti tra loro . 
in particolare , il diametro massimo mediano delle bncns che sono state sottoposte a follow - up passato dai 35 mm della diagnosi ai 38 mm dellultimo follow - up ( p < 0 , 001 )  . 
il valore mediano di crescita annua nella nostra casistica ( 2 , 0 mm ) risultato tuttavia signicativamente inferiore rispetto a quello riportato nel lavoro citato ( 6 , 4 mm )  . 
questo suggerisce come le neoplasie cistiche non comunicanti con il sistema duttale pancreatico scoperte incidentalmente possano essere sottoposte ad un follow - up con intervalli di sorveglianza lunghi se di dimensioni piccole alla diagnosi [ 27 , 28 ]  . un altro parametro che ha dimostrato un signicativo incremento durante il follow - up stato il diametro del dotto pancreatico principale a monte delle lesioni ( 0 , 1 mm / anno , p = 0 , 025 ) , a differenza del diametro del dpp a valle delle lesioni che invece non ha mostrato differenze signicative tra diagnosi e follow - up ( p = 0 , 33 )  . 
6 scatter plot indicante la correlazione tra la variazione percentuale annua del volume lesionale , a partire dal valore di base , ed il diametro massimo della lesione al momento della diagnosi . 
gli istogrammi a barre sovrapposti rappresentano la percentuale di lesioni con un incremento volumetrico annuo > 10% allinterno dei gruppi divisi in base alla dimensione delle lesioni alla diagnosi : 03 cm ( blu ) , 34 cm ( giallo ) e > 4 cm ( grigio )  . 
this most likely represents the result of the mass effect exerted by the enlarging neoplas long - standing mpd compression may lead to chronic inammation and brosis of the upstream pancreas , therefore changing the consistency of the pancreatic parenchyma from a friable , soft pancreas to a brotic hard one . as yet , there is no denite consensus about the appropriate radiological follow - up strategy for incidentally discovered bncns . 
based on general knowledge of the biological behaviour of asymptomatic pancreatic bncns and the results of our work , these lesions can safely undergo a long - interval follow - up . 
we suggest one mr / mrcp examination every 2 years for bncns with a low growth potential and one examination per year for those with a high growth potential namely , macrocystic or mixed and / or > 3 cm in maximum diameter . our study has two main limitations , primarily related to its retrospective design . 
the rst is the variability and relatively short follow - up period ( median , 19.5 months ; range , 761 months ) compared with the natural history of the lesions , which may not be conclusive regarding the natural conseguente brosi del parenchima pancreatico a monte , che modicher di conseguenza la sua consistenza da sofce e friabile a dura e brotica . non vi ad oggi un consenso denitivo riguardo la strategia di follow - up pi corretta per le bncns scoperte incidentalmente ; in particolare , gli intervalli di follow - up consigliati per tali lesioni variano ampiamente in letteratura da 6 a 24 mesi [ 13 , 2931 ]  . 
data la ormai assoda ta conoscenza riguardo il comportamento biologico indolente delle neoplasie cistiche benigne non comunicanti con il sistema duttale pancreatico e visti i risultati del nostro studio , si pu concludere che per tali lesioni siano indicati intervalli di follow - up tendenzialmente lunghi . 
noi suggeriamo un esame di rm / cprm ogni 2 anni per le bncns a basso potenziale di crescita ed invece un esame di rm / cprm annuale per le bncns ad elevato potenziale di crescita , e cio per quelle con aspetto macroscopico macrocistico o misto e / o per quelle con diametro massimo > 3 cm . il nostro studio presenta due principali limitazioni , sostanzialmente dovute al suo disegno retrospettivo . 
la prima costituita dallampia variabilit e dalla relativa brevit della durata del follow - up ( mediana 19 , 5 mesi con un range compreso tra 7 e 61 mesi ) rispetto alla storia naturale della malattia ; ci potrebbe rendere i risultati esposti non completamente conclusivi . 
 conclusioni conclusions the mixed pattern in incidentally discovered pancreatic bncns is very frequent ( 48% ) and is followed by the microcystic and then the macrocystic patterns ( 44% and 8% , respectively )  . 
mr / mrcp parameters predictive of higher tumour growth are macrocystic or mixed pattern and lesion size > 3 cm ; therefore for lesions presenting these characteristics , a yearly mr / mrcp follow - up examination is recommended , whereas we suggest a 2 - year - interval mr / mrcp follow - up for lesions with a low growth potential . 
 laspetto macroscopico misto molto frequente ( 48% ) nelle neoplasie cistiche benigne non comunicanti con il dotto pancreatico principale , seguito da quello microcistico e dal macrocistico ( 44% e 8% , rispettivamente )  . 
laspetto macroscopico delle lesioni ( microcistico , macrocistico o misto ) non varia nel tempo ; tali aspetti sembrano rappresentare diverse entit , non diversi stadi evolutivi della medesima lesione . 
centro interdipartimentale per lo studio dellhht , azienda universitario ospedaliera consorziale policlinico , universit degli studi di bari , bari , italy 2sezione di ginicologia ed ostertricia , dipartimento di scienze chirurgiche generali e specialistiche , azienda universitario ospedaliera consorziale policlinico , universit degli studi di bari , bari , italy correspondence to : a.scardapane , istituto di radiologia , universit degli studi di bari , azienda universitario ospedaliera consorziale policlinico , piazza giulio cesare 11 , 70124 bari , italy , tel . : + 39 - 080 - 5478840 , e - mail : a.scardapane@radiologia.uniba.it received : 26 may 2011 / accepted : 7 september 2011 / published online : 28 june 2012 springer - verlag 2012 abstract purpose . 
laparoscopy conrmed the presence of endometriosis in 119 / 143 patients ( 83% ) ; in 76 / 119 ( 64% ) deep pelvic endometriosis was diagnosed , whereas in the remaining 43 / 119 ( 36% ) , supercial peritoneal implants and endometriomas were found . 
centoquarantatre pazienti ( et media 34 , 35 , 1 anni ) con sospetto clinico di endometriosi pelvica profonda sono state valutate mediante rm pelvica completata con colonograa - rm . 
la laparoscopia ha confermato la presenza di endometriosi in 119 / 143 pazienti ( 83% ) ; in 76 / 119 ( 64% ) era evidente endometriosi pelvica profonda , mentre nelle rimanenti 43 / 119 ( 36% ) erano presenti endometriomi e impianti peritoneali superciali . 
la rm ha presentato valori di sensibilit , specicit , vpp , vpn e accuratezza diagnostica rispettivamente compresi tra 67%100% , 85%100% , 83%100% , 84%100% , 84%100% nel riconoscimento delle diverse sedi di impianto della patologia . 324 radiol med ( 2013 ) 118 : 323338 conclusions . 
la rm associata a colonograa rappresenta una metodica accurata per lo studio delle pazienti con endometriosi pelvica profonda da sottoporre ad intervento chirurgico laparoscopico e per la caratterizzazione delle lesioni endometriosiche . 
in particolare la colonograa - rm consente elevati valori di accuratezza nellidenticazione delle lesioni intestinali . parole chiave endometriosi pelvica profonda endometriosi intestinale risonanza magnetica colonograa - rm introduction introduzione endometriosis is a benign , oestrogen - dependent gynaecological disease that affects 1015 % of women of childbearing age and represents one of the main causes of infertility [ 13 ]  . 
the most common sites of involvement are ovaries , fallopian tubes , uterosacral ligaments ( usl ) and pelvic peritoneum ; less frequent locations are all those seen in deep pelvic endometriosis ( dpe ) , which is dened by the presence of lesions penetrating the retroperitoneal space or pelvic - organ walls to a depth of at least 5 mm and resulting in brosis and muscular hyperplasia [ 5 ]  . 
 dpe is known as posterior when lesions are located posterior to the uterus , and in particular , they involve the pouch of douglas , the retrocervical space or torus uterinus , the usl , the rectovaginal septum ( rvs ) and the bowel wall . 
from a clinical point of view , in contrast to the often asymptomatic peritoneal implants , dpe causes chronic pelvic pain , dysmenorrhoea , dyspareunia , dyschezia , urinary symptoms and infertility . 
 laparoscopy plays a crucial role in diagnosing and treating endometriosis , as it provides direct visualisation of the presence and extent of endometriotic lesions while allowing for mostly conservative surgical procedures , which preserve pelvic anatomy and function [ 6 , 7 ]  . 
however , the laparoscopic approach is limited by the impossibility of reaching the subperitoneal planes , especially in the presence of deep pelvic lesions with extensive adhesions and cul - de - sac obliteration [ 8 ]  . 
to ensure an adequate surgical approach in these cases , it is necessary to carry out preoperative assessment with panoramic imaging techniques that provide complete depiction of all pelvic planes . 
several such techniques have been suggested over the past decade , including transvaginal and transrectal ultrasonography ( us ) , double - contrast barium enema , computed tomography ( ct ) and magnetic resonance ( mr ) imaging , each of lendometriosi una malattia ginecologica benigna , estrogeno - dipendente , che interessa circa il 10%15% della popolazione femminile in et fertile e rientra tra le principali cause dinfertilit [ 13 ]  . 
le sedi maggiormente interessate dalla malattia sono le ovaie , le tube , i ligamenti utero - sacrali e il peritoneo pelvico ; seguono con frequenza minore tutte quelle localizzazioni che vanno sotto il nome di endometriosi pelvica profonda ( dpe ) , denita dalla presenza di lesioni che si estendono per almeno 5 mm di profondit nello spazio retroperitoneale o nella parete degli organi pelvici , con conseguente brosi e iperplasia muscolare [ 5 ]  . 
la dpe viene denita posteriore quando le lesioni sono localizzate posteriormente allutero in particolare a livello dello scavo del douglas , dello spazio retro cervicale o torus uterino , dei ligamenti utero - sacrali , del setto retto - vaginale e della parete intestinale . 
da un punto di vista clinico , rispetto agli impianti peritoneali a decorso spesso asintomatico , la dpe causa di dolore pelvico cronico , dismenorrea , dispareunia , dischezia , sintomi urinari e infertilit . 
la laparoscopia riveste un ruolo cruciale nella diagnosi e nella terapia dellendometriosi : essa consente di visualizzare direttamente i focolai endometriosici , di valutarne lestensione e , allo stesso tempo , rende possibile lesecuzione di procedure chirurgiche per lo pi conservative , nel rispetto dellintegrit anatomo - funzionale della pelvi [ 6 , 7 ]  . 
lapproccio laparoscopico ha tuttavia dei limiti rappresentati dallimpossibilit di raggiungere i piani sottoperitoneali specie in presenza di lesioni pelviche profonde caratterizzate da estese aderenze ed obliterazione dello spazio del douglas [ 8 ]  . 
in tali casi , per un adeguato approccio chirurgico , indispensabile una valutazione preoperatoria con tecniche di diagnostica per immagini panoramiche che permettano una rappresentazione completa di tutti i piani pelvici . 
 however , according to recent reports , mr imaging is the most accurate modality for studying dpe , as it provides a comprehensive map of endometriotic localisations [ 14 , 15 ]  . 
 in addition , when combined with colonography , mr imaging achieves a high level of diagnostic accuracy in detecting bowel lesions , often considered to be difcult to assess with this technique [ 16 ]  . the purpose of this study was to determine the diagnostic accuracy of mr imaging combined with colonography in the preoperative assessment of dpe in a group of consecutively enrolled patients undergoing laparoscopic surgery . materials and methods between march 2008 and january 2011 , 143 patients ( mean age 34.35.1 years ) with a clinical suspicion of dpe underwent mr completed by mr colonography . 
all patients had previously undergone gynaecological assessment for endometriosis , infertility or chronic pelvic pa the patients were enrolled in the study on the basis of the following inclusion criteria : ( 1 ) clinical symptoms suggestive of endometriosis , including chronic pelvic pain , dysmenorrhoea , dyspareunia and infertility ( n = 76 ) ; ( 2 ) us evidence of endometriotic cysts or peritoneal implants ( n = 81 ) ; ( 3 ) detection on gynaecological examination of endometriotic nodules at the vaginal fornix , rectum or usl ( n = 69 ) ; ( 4 ) symptoms suggestive of bladder endometriosis , such as tenesmus and dysuria ( n = 16 ) , and of colorectal endometriosis , such as abdominal pain before and during defaecation , rectal pain during menstruation , irritable bowel syndrome , rectal tenesmus ( n = 73 )  . 
during surgery , presence , site , number and extent of endometriotic lesions were carefully assessed ; all surgical specimens were sent for histological examination to conrm the presence of endometriotic tissue , paying particular attention to the intestinal and vesical specimens . 
the study was conducted in agreement with the principles of the declaration of helsinki , and approved by the local ethics committee ; all patients provided their informed consent for the mr examination . mr imaging protocol mr examination was performed with a 1.5 - t scanner transrettale , il clisma opaco a doppio contrasto , la tomograa computerizzata ( tc ) e la risonanza magnetica nucleare ( rm ) , ciascuna delle quali in grado di fornire utili informazioni preoperatorie [ 913 ]  . 
tuttavia secondo recenti dati della letteratura , la rm rappresenta lindagine pi accurata per lo studio della dpe , poich fornisce una mappa esaustiva delle localizzazioni endometriosiche [ 14 , 15 ]  . 
la rm , inoltre , quando associata a colonograa permette di raggiungere unelevata accuratezza diagnostica anche nel riconoscimento di lesioni intestinali spesso considerate di difcile valutazione con tale metodica [ 16 ]  . obiettivo del presente studio , pertanto , valutare laccuratezza diagnostica della rm associata a colonograa , nella valutazione pre - operatoria della dpe in un gruppo di pazienti arruolate consecutivamente e sottoposte ad intervento per via laparoscopica . materiali e metodi nel periodo compreso tra marzo 2008 e gennaio 2011 , 143 pazienti ( et media 34 , 35 , 1 anni ) con sospetto clinico di endometriosi pelvica profonda sono state sottoposte a rm completata con colonograa - rm . 
 le pazienti sono state incluse nello studio in base ai seguenti criteri : ( 1 ) sintomatologia clinica riconducibile ad endometriosi , ovvero dolore pelvico cronico , dismenorrea , dispareunia e infertilit ( n = 76 ) ; ( 2 ) evidenza ecograca di cisti endometriosiche o impianti peritoneali ( n = 81 ) ; ( 3 ) palpazione alla visita ginecologica di noduli endometriosici del fornice vaginale , del retto o dei ligamenti utero - sacrali ( n = 69 ) ; ( 4 ) disturbi suggestivi di endometriosi vescicale , quali tenesmo e bruciore alla minzione ( n = 16 ) e di endometriosi del colon - retto , quali dolore addominale prima e durante la defecazione , algie al retto durante il usso mestruale , sindrome del colon irritabile , tenesmo rettale ( n = 73 )  . 
nel corso dellintervento sono stati accuratamente valutati la presenza , la sede , il numero e lestensione delle lesioni endometriosiche ; tutti i reperti operatori sono stati avviati ad esame istologico per accertare la presenza di tessuto endometriosico , ponendo particolare attenzione ai reperti intestinali e vescicali . 
lo studio stato condotto in accordo con i principi della dichiarazione di helsinki e ha ricevuto lapprovazione del comitato etico locale ; tutte le pazienti hanno fornito il proprio consenso informato allesecuzione della rm . 
 326 radiol med ( 2013 ) 118 : 323338 ( philips , achieva 1.5 ) using a 4 - channel surface coil [ sensitivity - encoding ( sense ) body coil ] , regardless of the phase of the menstrual cycle . 
all patients underwent bowel preparation consisting of 4 l of polyethylene glycol solution ( selg - esse 1000 , promefarm , italy ) on the day before examination , associated with a low - residue diet for 3 days . 
 the study protocol consisted of two phases : ( 1 ) a high - resolution mr examination of the pelvis ( hr - mr ) with overall duration of 15 min ; and ( 2 ) mr colonography with overall duration from 10 to 13 mhr - mr included the following sequences : t2 - weighted turbo spin - echo ( tse ) in the axial , coronal and sagittal planes [ matrix 512512 ; eld of view ( fov ) 260 ; number of signal averages ( nsa ) 3 ; te 110 ms ; shortest tr ; number of sections 24 ; thickness 45 mm ; acquisition time 3 min and 30 s ] ; t1 - weighted tse sequences in the axial plane ( matrix 512512 ; fov 260 ; nsa 2 ; te 11 ms ; shortest tr ; number of sections 24 ; thickness 5 mm ; acquisition time 3 min and 5 s ) ; t1 - weighted high - resolution isotropic volume ( thrive ) sequences in the axial plane ( matrix 256256 ; number of sections 100 ; thickness 2 mm ; sense factor 4 ; shortest te / tr ; ip angle 10 ; fov 350 )  . prior to mr colonography , patients received 20 mg of butyl scopolamine bromide ( buscopan , boehringer ingelheim , florence , italy ) intravenously . 
colonic distension , performed on patients in the supine position by administering 1.52 l of water via a rectal tube , was monitored with a thick - slab uoroscopic rapid acquisition with relaxation enhancement ( rare ) sequence ( one 120 - mm - thick image every 10 s )  . 
thrive sequences in the axial , coronal and sagittal planes [ matrix 256 256 ; number of sections 100 ; thickness 2 mm ; sense factor 4 ; shortest te / tr ; ip angle 10 ; fov 350 ( axial ) and 450 ( coronal and axial ) ; acquisition time 19 s / sequence ] ; b . 
balanced turbo eld echo ( btfe ) sequences in the axial , coronal and sagittal planes ( matrix 256 256 ; number of sections 40 ; thickness 8 mm with 4 mm overlap ; shortest te / tr ; ip angle 90 ; fov 350450 ; acquisition time 21 s / sequence )  . image interpretation the diagnosis of dpe was established according to the criprotocollo rm gli esami rm sono stati eseguiti con magnete da 1 , 5 tesla ( philips , achieva 1.5 , paesi bassi ) utilizzando una bobina di supercie a 4 canali ( sense - body coil ) , indipendentemente dalla fase del ciclo mestruale . 
tutte le pazienti sono state sottoposte a preparazione intestinale mediante somministrazione di 4 l di una soluzione di polietilenglicole ( selgesse 1000 , promefarm , italia ) il giorno prima dellesame associata ad una dieta a basso contenuto di scorie nei 3 giorni precedenti . 
lrm - hr prevedeva le seguenti sequenze : sequenze turbo spin - echo ( tse ) t2 pesate nei piani assiale , coronale e sagittale [ matrice 512512 , campo di vista ( fov ) 260 , number of signals averaged ( nsa ) 3 , tempo di eco ( te ) 110 ms , tempo di ripetizione ( tr ) shortest , numero di sezioni 24 , spessore 45 mm , tempo di acquisizione 3 minuti e 30 secondi ] ; sequenze tse spin - echo t1 pesate sul piano assiale con ( matrice 512512 , fov 260 , nsa 2 , te 11 ms , tr shortest , numero di sezioni 24 , spessore 5 mm , tempo di acquisizione 3 minuti e 5 secondi ) ; sequenza t1 high resolution isotropic volume examination ( thrive ) sul piano assiale ( matrice 256256 , numero di sezioni 100 , spessore 2 mm , sense factor 4 , te / tr shortest , ip angle 10 , fov 350 )  . prima di eseguire la colonograa - rm , sono stati somministrati per via endovenosa 20 mg di butilbromuro di scopolamina ( buscopan , boehringer ingelheim , firenze , italia )  . 
la distensione del colon , eseguita a paziente supina previa somministrazione di 1 , 52 litri di acqua mediante sonda rettale , stata monitorata con sequenza uoroscopica rapid acquisition with relaxation enhancement ( rare ) a strato spesso ( una immagine con spessore di 120 mm ogni 10 secondi )  . 
sequenze thrive nei piani assiale , coronale e sagittale ( matrice 256256 , numero di sezioni 100 , spessore 2 mm , sense factor 4 , te / tr shortest , ip angle 10 , fov 350 , assiale , e 450 , coronale e assiale , tempo di acquisizione 19 s / sequenza ) ; b . 
sequenze turbo - eld echo balanced ( btfe ) nei piani assiale , coronale e sagittale ( matrice 256256 , numero di sezioni 40 , spessore 8 mm con overlap di 4 mm , te / tr shortest , ip angle 90 , fov 350450 , tempo di acquisizione 21 s / sequenza )  . radiol med ( 2013 ) 118 : 323338 fig . 
1 immagini sequenziali di uoroscopia - rm che permettono di controllare il riempimento colico e vericare ladeguata distensione del viscere sino al cieco ( punta di freccia ) con visualizzazione dellultima ansa ileale ( freccia )  . teria suggested by bazot et al . 
 [ 14 ] , on the basis of the presence of morphological abnormalities ( low - signal - intensity nodules or spiculated masses on t2 - weighted sequences ) associated with high - signal - intensity foci corresponding to haemorrhagic foci on t1 - weighted and / or fat - suppressed sequences . 
these are classied into direct signs ( presence of parietal nodules or plaques with low signal intensity on t2 - weighted sequences and high - signal - intensity foci on t1 - weighted sequences ) and indirect signs ( adhesions between bowel loops , uterus and / or adjacent organs , abnormal angulation of bowel loops and retroverted uterus )  . 
in addition , lesions located at the level of the bladder and ureters were reported , with a diagnosis of ureteral inltration being established in the presence of ureteral dilatation due to inltration by a endometriotic nodule . 
 sensitivity , specicity , negative ( npv ) and positive ( ppv ) predictive values and diagnostic accuracy were calculated for each site examined , with laparoscopy being considered the gold standard for diagnosis . interpretazione delle immagini la diagnosi di endometriosi pelvica profonda stata formulata secondo i criteri proposti da bazot et al . 
 [ 14 ] , in base alla presenza di anomalie morfologiche ( noduli o aree di brosi di aspetto spiculato con segnale ipointenso nelle sequenze t2 pesate ) associate ad alterazioni di segnale rappresentate da foci iperintensi corrispondenti a foci emorragici nelle sequenze t1 pesate e / o nelle sequenze con soppressione del grasso . 
tali lesioni sono state ricercate a livello del compartimento posteriore , a livello dello scavo del douglas , del torus uterinus , dei ligamenti utero - sacrali ( lus ) , del setto retto - vaginale ( srv )  . 
 [ 15 ] distinti in segni diretti ( presenza di nodulo o placca parietale con segnale ipointenso nelle sequenze t2 dipendenti e foci iperitensi in quelle t1 dipendenti ) ed indiretti ( perdita del piano di clivaggio tra anse intestinali , utero e / o organi adiacenti , anomala angolazione delle anse intestinali e retroversione uterina )  . 
nella colonograa - rm invece , sono stati ricercati noduli sottomucosi , con impregnazione contrastograca dopo iniezione endovena ( ev ) di gadolinio [ 16 ]  . la presenza di convergenza tra strutture pelviche e la perdita dei corrispondenti piani di clivaggio , senza delimitabili lesioni nodulari , ha consentito la diagnosi di obliterazione degli spazi pelvici su base aderenziale . 
in questultimo caso la diagnosi dinltrazione ureterale stata formulata quando fosse riconoscibi328 results surgical ndings laparoscopy conrmed the presence of endometriosis in 119 / 143 patients ( 83% ) ; in particular , dpe was diagnosed in 76 / 119 ( 64% ) women , whereas the remaining 43 / 119 ( 36% ) were found to be affected by endometriomas and supercial peritoneal implants . 
intestinal lesions ( size range 1545 mm ; mean 27 mm ) were identied in 32 / 119 ( 27% ) patients ; of these 17 / 119 ( 14% ) were located at the rectum , 10 / 119 ( 8% ) at the sigmoid ( at the rectosigmoid junction in ve cases and the distal sigmoid in ve cases ) , 4 / 119 ( 3% ) at the caecum , and 1 / 119 ( 0.8% ) at the ileal level . 
these lesions required bowel resection in 28 cases , whereas nodulectomy was performed in four cases ( one rectal lesion , two sigmoid lesions and one ileal lesion )  . 
of patients with anterior compartment lesions 3 / 119 ( 2.5 % ) had bladder lesions with involvement of the uterovesical fold , whereas 4 / 119 ( 3% ) had ureteral lesions . 
in the remaining 24 patients in whom endometriosis was not detected , surgery revealed the following results : functional ovarian cysts ( n = 9 ) , haemorrhagic corpus luteum ( n = 7 ) , sactosalpinx ( n = 4 ) , dermoid cysts ( n = 3 ) and ovarian broma ( n = 1 )  . mr ndings mr imaging was well tolerated by all patients . 
sensibilit , specicit , valore predittivo negativo ( vpn ) e positivo ( vpp ) e accuratezza diagnostica sono stati calcolati per ciascuna delle sedi esaminate , considerando i reperti laparoscopici quali gold standard per la diagnosi . 
 risultati reperti operatori la laparoscopia ha confermato la presenza di endometriosi in 119 / 143 pazienti ( 83% ) ; in particolare in 76 / 119 ( 64% ) donne era evidente dpe , mentre nelle rimanenti 43 / 119 ( 36% ) erano presenti endometriomi e impianti peritoneali superciali . 
tra le pazienti con dpe , il coinvolgimento dei lus , del torus uterinus , del srv e della vagina stato riscontrato rispettivamente in 57 / 119 ( 48% ) , 60 / 119 ( 50% ) , 45 / 119 ( 38% ) e 1 / 119 ( 1% ) casi , mentre lobliterazione su base aderenziale dello scavo del douglas stata osservata in 24 / 119 ( 20% ) donne . 
tali lesioni hanno richiesto una resezione intestinale in 28 casi , mentre in 4 ( 1 lesione rettale , 2 lesioni del sigma e 1 lesione ileale ) , stata eseguita una nodulectomia . 
per quanto riguarda le lesioni del compartimento anteriore , 3 / 119 ( 3% ) pazienti mostravano lesioni vescicali con interessamento della plica vescico - uterina , mentre in 4 / 119 ( 3% ) casi vi erano lesioni delluretere . 
 nelle restanti 24 pazienti ove non stata riscontrata endometriosi , la chirurgia ha rilevato i seguenti reperti : cisti ovarica funzionale ( n = 9 ) , corpo luteo emorragico ( n = 7 ) , sactosalpinge ( n = 4 ) , cisti dermoide ( n = 3 ) e broma ovarico ( n = 1 )  . 
linltrazione vaginale radiol med ( 2013 ) 118 : 323338 table 1 comparison between mr and laparoscopic ndings in 119 women with proven endometriosis site sensitivity ( % ) specicity ( % ) ppv ( % ) npv ( % ) accuracy ( % ) 100 100 100 100 100 100 100 100 usl torus rvs vagina douglas bowel bladder ureters sede lus torus srv vagina douglas intestino vescica ureteri 118 116 115 118 116 115 usl , uterosacral ligaments ; rvs , rectovaginal septum ; tp , true positive ; fp , false positive ; fn , false negative ; tn , true negative ; ppv , positive predictive value ; npv , negative predictive value tabella 1 confronto tra reperti rm e laparoscopici nelle 119 pazienti con endometriosi accertata . 
 accuratezza ( % ) sensibilit ( % ) 100 specicit ( % ) 100 100 100 vpp ( % ) 100 100 100 vpn ( % ) 100 lus , ligamenti utero - sacrali ; srv , setto retto - vaginale ; vp , veri positivi ; fp , falsi positivi ; fn , falsi negativi ; vn , veri negativi ; vpp , valore predittivo positivo ; vpn , valore predittivo negativo stata evidenziata in 1 / 119 pazienti ( 0 , 8% ) , mentre lobliterazione del douglas in 23 / 119 casi ( 19% ) con unaccuratezza diagnostica pari al 100% e al 94% , rispettivamente . i falsi negativi evidenziati alla rm si sono vericati per lesioni con morfologia lineare o a placca ( 5 casi per i lus , 3 per il torus e 4 per il srv ) , per marcata retroversione uterina ( 3 casi per i lus , 5 per il torus , 1 per il srv e 3 per il douglas ) o per la presenza di voluminosi endometriomi che non consentivano la corretta valutazione dello spazio retrouterino ( 2 casi per i lus , 2 per il srv e 1 per il douglas )  . 
i falsi positivi sono stati determinati a livello di torus uterino e srv , dalla presenza di fenomeni aderenziali retro - uterini erroneamente interpretati come lesioni nodulari , a livello dei lus da un apparente ispessimento lineare non evidenziato alla laparoscopia . la presenza di endometriosi intestinale stata evidenziata in 33 / 119 casi ( 28% ) con unaccuratezza diagnostica del 96% . 
in 9 / 33 casi ( 27% ; 2 lesioni rettali , 3 del sigma distale , 3 del cieco e 1 ileale ) , il riconoscimento del nodulo parietale stato possibile esclusivamente con la colonograa - rm , che grazie alla distensione del colon , ha permesso di evidenziare anche la presenza di stenosi luminale . 
 false positive results at the level of the torus uterinus and rvs were related to the presence of retrouterine adhesions incorrectly interpreted as nodular lesions and those at the 330 radiol med ( 2013 ) 118 : 323338 fig . 
 le immagini tse t2 dipendenti sul piano assiale ( a ) e sagittale ( b ) dimostrano la presenza di un nodulo ipointenso del srv ( punte di freccia )  . level of the usl to an apparent linear thickening not conrmed at laparoscopy . the presence of bowel endometriosis was detected in 33 / 119 cases ( 28% ) , with 96% diagnostic accuracy . 
in 9 / 33 cases ( 27% ; two lesions of the rectum , three of the distal sigmoid , three of the caecum and one of the ileum ) , recognition of the parietal nodule was only possible with mr colonography which , thanks to colonic distension , also identied the presence of luminal stenosis . 
in three patients , the mr nding of rectal endometriosis was not conrmed by laparoscopy , which showed rectal adhesions ; in another two cases , surgery demonstrated two small nonstenotic nodular lesions of the distal sigmoid not identied on mr examination . 
in fact , us has extremely non stato confermato alla laparoscopia che invece ha evidenziato un coinvolgimento di tipo aderenziale dello stesso , mentre in altri due casi in sede operatoria , sono state evidenziate due piccole lesioni nodulari del sigma distale , non stenosanti , misconosciute allesame rm . 
 discussione il ruolo della risonanza magnetica nella conferma dellipotesi clinica di endometriosi pelvica profonda stato gi sottolineato in letteratura e ha lindubbio vantaggio di consentire , senza lutilizzo di radiazioni ionizzanti , una completa valutazione dellestensione di malattia , soprattutto in presenza di localizzazioni pelviche subperitoneali , spesso non riconoscibili mediante esame ginecologico e chirurgia laparoscopica [ 14 , 2022 ]  . 
la metodica infatti ha elevatissima accuratezza nello studio delle lesioni ovariche e nella visualizzazione degli spazi pelvici interessati dalla malattia [ 13 , 20 , 23 , 24 ]  . 
la necessit di unesperienza specica nella valutazione della dpe caratterizzata da lesioni di difcile identicazione rappresenta tuttavia un limite delletg il cui risultato diviene attendibile solo in centri con elevato numero di pazienti con endometriosi ; inoltre il campo di vista limitato delletg non consente lo studio di spazi anatomici lontani dal trasduttore come il sigma ed il cieco che , possono essere interessati dalla malattia . 
al momento tra le tecniche dimaging , la rm rappresenta lindagine complessivamente pi accurata per lo staging preoperatorio della dpe con unaccuratezza diagnostica media a seconda delle diverse radiol med ( 2013 ) 118 : 323338 fig . 
4a - d deep pelvic endometriosis : axial ( a , b ) and sagittal ( c ) t2 - weighted images show a hypointense nodule inltrating the anterior wall of the sigmoid colon ( arrowhead ) ; endometriotic nodule of the torus uterinus ( arrow in b )  . 
le immagini t2 dipendenti sul piano assiale ( a , b ) e sagittale ( c ) mettono in evidenza un nodulo ipointenso che inltra la parete anteriore del sigma ( punte di freccia )  . 
colonograa - rm : limmagine thrive sul piano assiale dopo iniezione di mezzo di contrasto ev ( d ) facilita il riconoscimento della lesione intestinale inltrante ( punte di freccia )  . high accuracy when studying ovarian lesions and identifying pelvic locations of disease [ 13 , 20 , 23 , 24 ]  . 
however , the need for specic experience in assessing dpe , characterised by poorly identiable lesions , is a limitation of us , the results of which are only reliable when obtained in centres with large numbers of patients with endometriosis ; furthermore , the small fov typical of us precludes the study of anatomical regions distant from the transducer , such as the sigmoid colon and caecum , which may be affected by the disease . 
mr imaging is currently the most accurate modality for preoperative staging of dpe , with a mean diagnostic accuracy of > 90 % in the different case series [ 1416 , 25 ]  . in our experience , the most commonly affected sites were the usl ( 75% ) and the torus uterinus ( 79% ) , which conrms previous reports [ 7 , 14 ]  . 
correlation with laparoscopic ndings showed that mr imaging detects usl lesions with sensitivity , specicity , ppv , npv and diagnostic accuracy of 82% , 85% , 84% , 84% and 84% , respectively ; its sensitivity , specicity , ppv , npv and diagnostic accuracy in detecting lesions of the torus uterinus were 87% , casistiche in letteratura , superiore al 90% [ 1416 , 25 ]  . nella nostra esperienza , le sedi pi frequentemente colpite dalla patologia sono stati i ligamenti utero - sacrali ( 75% ) e il torus uterinus ( 79% ) , confermando cos dati gi presenti in letteratura [ 7 , 14 ]  . 
dal confronto col reperto laparoscopico emerso che la rm in grado di riconoscere lesioni a carico dei ligamenti utero - sacrali con sensibilit , specicit , vpp , vpn e accuratezza diagnostica pari all82% , 85% , 84% , 84% e 84% , rispettivamente ; mentre sensibilit , specicit , vpp , vpn e accuratezza diagnostica nellidenticazione di lesioni del torus uterinus sono dell87% , 90% , 90% , 87% e 88% . 
tali valori non si discostano in maniera signicativa da altri studi condotti precedentemente [ 14 , 26 , 27 ] , pertanto la rm risulta indagine estremamente sensibile nel riconoscimento di localizzazioni dello spazio retro - cervicale , consentendo la visualizzazione di lesioni difcilmente identicabili data la loro localizzazione profonda . 
 lobliterazione dello scavo del douglas stata riscontrata allesame laparoscopico nel 20% dei casi e a tal proposito la rm ha mostrato una sensibilit e unaccuratezza diagnostica pari all83% e al 94% , rispettivamente . 
5a - f deep pelvic endometriosis : axial t2 - weighted image ( a ) , axial t1 - weighted image ( b ) and sagittal t2 - weighted images ( c , d ) ; adhesions between the ovaries and the anterior wall of the rectum , where an endometriotic nodule is visible ( arrowhead ) ; submucosal myoma ( * )  . 
 magnetic resonance ( mr ) colonography : contrast - enhanced sagittal t1 - weighted high - resolution isotropic volume examination ( thrive ) images ( e , f ) conrm the submucosal rectal nodule and show a second endometriotic lesion of the sigmoid ( arrow )  . 
immagine tse t2 dipendente sul piano assiale ( a ) , tse t1 dipendente sul piano assiale ( b ) e immagini tse t2 dipendenti sul piano sagittale ( c , d )  . 
presenza di un importante complesso aderenziale tra le due ovaie e la parete anteriore del retto che mostra una lesione nodulare di tipo endometriosico ( punta di freccia )  . 
mr imaging is therefore extremely sensitive in identifying retrocervical localisations , as it is able to depict lesions that are otherwise poorly detectable because of their deep location . cul - de - sac obliteration was found on laparoscopy in 20% of cases , in which mr showed 83% and 94% sensitivity and diagnostic accuracy , respectively . 
tali immagini infatti hanno consentito la visualizzazione contestuale del douglas , del retto e del setto retto - vaginale , evidenziando che in tutti i casi in cui vi era unobliterazione del douglas erano associate lesioni del srv e in un caso anche linltrazione della vagina . 
6a - f deep pelvic endometriosis : axial t1 - weighted high - resolution isotropic volume examination ( thrive ) image ( a ) , t2 - weighted sagittal image ( b ) and t2 - weighted coronal image ; large endometrioma ( * ) ; ileal loops are contiguous to the uterus , but no nodule is visible ( arrowhead )  . 
immagine thrive sul piano assiale ( a ) , immagine tse t2 dipendente sul piano sagittale ( b ) e immagine tse t2 dipendente sul piano coronale ( c )  . 
in fact , these images allowed simultaneous visualisation of the pouch of douglas , the rectum and the rvs , indicating that all cases of cul - desac obliteration were associated with rvs lesions and , in one case , with inltration of the vagina . 
this nding is not surprising , as the rvs originates embryologically from the fusion of the two layers of the peritoneal cul - de - sac and extends downwards between the rectum and the posterior wall of the vagina to the levator ani muscle . 
 in our experience , and in agreement with published data , misdiagnoses at the level of the posterior compartment were related to linear or plaque - like lesions without real endometriotic nodules , to an unfavourable anatomical situation caused by marked uterine retroversion or to posterior endometriomas preventing adequate visualisation of the pouch of douglas . 
with regard to identifying bowel endometriosis , there is no agreement in the literature as to the best noninvasive diagnostic fusione dei 2 piani del cul - de - sac peritoneale e si estende verso il basso tra retto e parete posteriore della vagina no al muscolo elevatore dellano . 
 nella nostra esperienza , gli errori diagnostici a livello del comparto posteriore sono derivati in accordo con la letteratura , da lesioni a morfologia lineare o a placca in assenza di veri e propri noduli endometriosici , da una condizione anatomica sfavorevole determinata da marcata retroversione uterina o da endometriomi posteriori , che impedivano unadeguata visualizzazione dello scavo del douglas . 
recenti studi suggeriscono unelevata accuratezza diagnostica delletg transvaginale e transrettale nel riconoscimento dellinltrazione parietale con il limite di poter esplorare esclusivamente il retto [ 13 , 20 , 23 , 29 , 30 ]  . 
anche la tc con distensione acquosa del colon stata proposta con ottimi risultati nella valutazione dellendometriosi intestinale , tuttavia luso di tale tecnica non giusticato 334 radiol med ( 2013 ) 118 : 323338 fig . 
8a - f deep pelvic endometriosis : axial ( ac ) and sagittal ( d , e ) t2 - weighted images ; large endometrioma ( * ) ; left ureteral dilatation due to hypointense endometriotic nodule in the left pelvis ( arrowhead )  . 
recent studies suggest that transvaginal and transrectal us have a high diagnostic accuracy in detecting wall inltration , albeit with the limitation of depicting the rectum only [ 13 , 20 , 23 , 29 , 30 ]  . 
inoltre , la ridotta risoluzione di contrasto della tecnica genera una scarsa accuratezza diagnostica per le localizzazioni pelradiol med ( 2013 ) 118 : 323338 sion by water enteroclysis has also been used with excellent results in assessing bowel endometriosis ; however , the routine use of this technique cannot be recommended , thus avoiding radiation exposure in young patients with endometriosis [ 10 , 11 ]  . 
furthermore , the limited contrast resolution of ct results in poor diagnostic accuracy in pelvic localisations of the disease . the reported results of mr imaging differ according to the protocol and scanners used ; namely bazot et al . 
conversely , other studies report a lower accuracy of mr imaging compared with panoramic studies of the colon , such as double - contrast enema , which is capable of depicting lesions in more distal segments , such as the sigmoid and caecum [ 9 , 32 ]  . 
 the use of mr colonography was recently described as a complement to pelvic hr - mr imaging and represents a signicant improvement in the diagnostic capabilities of pelvic hr - mr , as it allows detection of a signicantly higher number of lesions and better diagnostic agreement among radiologists with different levels of experience [ 16 ]  . 
injection of contrast material allowed identication of 9 / 33 ( 27% ) bowel lesions missed at baseline mr imaging ( one nodule in the rectum , three in the sigmoid and caecum , one in the ileum ; table 2 ) ; in addition , it improved the study of the bowel wall and enabled assessment of the degree of luminal stenosis , thus helping to select the most appropriate surgical treatment . 
therefore , we believe this technique should be proposed in all patients presenting with severe dpe and signs of bowel involvement on hr - mr , with the aim of avoiding the use of radiographic bowel - imaging techniques that are still included in the preoperative workup of endometriosis [ 3234 ]  . bladder endometriosis was recognised in 2 / 3 cases conrmed at laparoscopy and was localised at the uterovesical fold in all cases , with 67% sensitivity and 99% diagnostic accuracy . 
the limited presence of bladder and ureteral lesions in our series and in published reports makes it difcult to reach any conclusions as to the accuracy of mr imaging in these sites , even though our results do not differ signicantly from previously published ndings [ 14 , 27 , 3537 ]  . 
in our experience , the diagnosis of bladder involvement was straightforward when the lesion was nodular , whereas it was missed in the case of plaque - like lesions producing adhesions between the uterus and bladder dome . 
 [ 31 ] , hanno recentemente dimostrato unelevata accuratezza della sola rm pelvica nel riconoscimento di lesioni rettali senza particolari vantaggi diagnostici delle sequenze con distensione luminale o con iniezione endovenosa di gadolinio . 
altri studi invece riportano una minore accuratezza della metodica rispetto a tecniche di studio panoramiche del colon quali il clisma a doppio contrasto , per la capacit di queste ultime di evidenziare lesioni in segmenti pi distali come sigma e cieco [ 9 , 32 ]  . 
 luso della colonograa - rm stato recentemente descritto come completamento della rm - hr della pelvi e ha permesso un signicativo miglioramento delle possibilit diagnostiche rispetto alla rm - hr pelvica , consentendo il riconoscimento di un numero di lesioni signicativamente superiore e un maggiore accordo diagnostico tra radiologi con diversa esperienza [ 16 ]  . 
 nella nostra casistica , la distensione dellintero colon e liniezione ev di mezzo di contrasto hanno permesso lidenticazione di 9 / 33 ( 27% ) lesioni intestinali non riconoscibili allrm di base ( 1 nodulo del retto , 3 del sigma e del cieco ed 1 dellileo ) ( tabella 2 ) e , una pi accurata valutazione della parete intestinale e del grado di stenosi luminale , ai ni della scelta del miglior trattamento chirurgico . 
luso di tale tecnica , a nostro avviso , pertanto proponibile in tutte le pazienti che alla rm - hr presentino dpe severa e segni di coinvolgimento intestinale , allo scopo di evitare il ricorso alle tecniche radiologiche di studio del colon che tuttora rientrano nel work - up preoperatorio [ 3234 ]  . lendometriosi vescicale stata riconosciuta in 2 dei 3 casi laparoscopicamente accertati , e in tutte le pazienti era localizzata a livello della plica vescico - uterina con una sensibilit ed accuratezza diagnostica della metodica del 67% e 99% rispettivamente . 
la scarsa prevalenza di queste ultime lesioni nella nostra serie e in quelle precedentemente pubblicate in letteratura rende difcile esprimere considerazioni conclusive circa laccuratezza dellrm in tali sedi , anche se questi risultati non si discostano signicativamente da quelli precedentemente pubblicati [ 14 , 27 , 3537 ]  . 
nella nostra esperienza la diagnosi di coinvolgimento vescicale stata agevole quando si presentava sotto forma di lesione nodulare , mentre stata misconosciuta nelle lesioni a placca che determinavano aderenze tra utero e cupola vescicale ; tali lesioni , probabilmente , sono pi facilmente diagnosticabili con lecograa sfruttando la visualizzazione dinamica e documentando il mancato scorrimento della supercie uterina rispetto a quella vescicale [ 38 ]  . 
 20 / 20 8 / 8 4 / 4 1 / 1 20 / 20 8 / 8 4 / 4 1 / 1 15 / 20 n.a. , non applicabile ; mdc , mezzo di contrasto nary tract dilatation and the presence of endometriotic tissue inltrating the transition point between the dilated and nondilated portions of the ureter . 
therefore , future research should aim to assess the accuracy of mr colonography in relation to its ability to predict the degree of wall inltration , crucial preoperative information that is difcult to assess with conventional imaging . 
second is the low prevalence of caecal or ileal lesions , for which mr colonography might prove essential for the diagnosis , does not help us to understand the impact of their detection on subsequent patient management . 
a multidisciplinary evaluation , providing thorough information about the mr imaging procedure and the advantages of the approach prior to obtaining patient consent , as well as a comfortable clinical setting , are all at the basis of the patients full cooperation . 
nella nostra serie , lunico falso negativo stato determinato da un caso in cui la laparoscopia aveva individuato un parziale coinvolgimento ureterale in assenza di dilatazione a monte . il nostro studio presenta tuttavia alcuni limiti : in primo luogo lassenza di correlazione tra i reperti rm e quelli istologici . 
ricerche future pertanto , dovrebbero essere nalizzate a valutare laccuratezza della colonograa - rm rispetto alla capacit di predire il grado di inltrazione parietale , dato preoperatorio di sicuro interesse ma difcilmente valutabile con le tecniche dimaging . 
in secondo luogo , la bassa prevalenza nella nostra casistica di lesioni cecali o ileali nelle quali luso della colonograa - rm potrebbe essere realmente indispensabile per la diagnosi , non permette ancora di comprendere il reale impatto del loro riconoscimento sulla successiva gestione del paziente . 
la valutazione multidisciplinare , un completo consenso informato riguardante le modalit desecuzione dellindagine rm ed i vantaggi diagnostici di tale approccio , ed un ambiente clinico confortevole , sono alla base della piena collaborazione da parte delle pazienti . 
 radiol med ( 2013 ) 118 : 323338 conclusions conclusioni our study conrms the role of mr imaging as the method of choice for studying patients with dpe scheduled for laparoscopy . 
 furthermore , complementation with mr colonography allows for high diagnostic accuracy , even in the case of colorectal localisations of disease . il nostro lavoro conferma il ruolo della rm come metodica di elezione per lo studio delle pazienti con dpe da sottoporre a laparoscopia . 
lesame infatti , in maniera non invasiva e senza limpiego di radiazioni ionizzanti , fornisce una valutazione panoramica della pelvi e , grazie alla elevata risoluzione di contrasto , consente di caratterizzare quelle lesioni pelviche profonde ad elevata componente brotica e quindi difcilmente riconoscibili con altre metodiche di imaging . 
in keeping with the literature , our study demonstrates the effectiveness of endovascular repair of paa , with shortand mid - term patency rates comparable to those of open surgery . 
da gennaio 2009 a luglio 2010 , 10 pazienti ( 9 maschi e 1 femmina ; et media 6912 anni ) affetti da paa sono stati sottoposti a trattamento endovascolare mediante posizionamento di stent ricoperto eparinato . 
sono necessari studi con maggiore casistica e pi lungo follow - up per confermare questi risultati . parole chiave aneurisma popliteo trattamento endovascolare stent ricoperto 230 introduction popliteal artery aneurysms ( paa ) are a rare condition , with an overall incidence < 0.1% , which increases to 1% in the 6580 age range [ 1 , 2 ]  . 
they are , however , the most frequent peripheral aneurysms , accounting for 7080% of all cases [ 3 , 4 ] ; they are bilateral in around 60% of cases and associated with abdominal aortic aneurysms in 4049% of cases [ 5 ]  . 
other less common causes , especially in young patients , are iatrogenic or posttraumatic pseudoaneurysms , mycotic aneurysms , collagen disorders ( ehlersdanlos syndrome ) and rheumatic disease ( behets disease ) [ 6 , 7 ]  . 
 [ 8 ] , sinister harbingers of sudden catastrophe , as the distal embolisation of thrombotic fragments and / or acute thrombosis of the aneurysm sac can lead to severe acute limb ischaemia . 
it is estimated that 1424% of asymptomatic paas become symptomatic each year [ 9 ] : the most frequent clinical manifestations are acute or chronic ischaemia with intermittent claudication ; pain at rest or trophic lesions ; compression of the popliteal vein with deep vein thrombosis or lower - limb oedema ; compression of the ischiatic nerve or its branches with burning pain ; aneurysm rupture , a rare complication associated with a high risk of limb loss [ 10 ]  . 
the main factors affecting treatment are aneurysm size , morphology , poor distal runoff and the presence of an intramural thrombus at risk of embolic complications [ 12 ]  . 
 [ 13 ] suggested a threshold value of 2 cm , whereas galland and magee [ 14 ] suggested 3 ctreatment is currently indicated for symptomatic paas of any size or for asymptomatic paas > 2 cm [ 15 , 16 ] , whereas medical antiplatelet therapy and close follow - up are indicated for asymptomatic paas < 2 cm [ 12 ]  . 
the standard treatment is surgery with ligation of the aneurysm and autologous ( saphenous vein ) , or heterologous [ expanded polytetrauoroethylene ( eptfe ) ] by - pass grafting with medial or posterior approach , which has a high rate of technical success and 7080% patency at 5 years [ 9 , 11 , 14 , 17 ]  . 
by transferring to paa the experience and technology used to treat aortic and thoracic aneurysms , we can reduce operative complications and achieve similar rates of technical success and shortand midterm patency to those of open surgery . 
the purpose of our study was to evaluate radiol med ( 2013 ) 118 : 229238 introduzione gli aneurismi dellarteria poplitea ( paa ) sono una patologia rara , con una incidenza globale < 0 , 1% che sale all1% nella fascia di et 6580 anni [ 1 , 2 ] ; sono tuttavia gli aneurismi periferici pi frequenti , rappresentandone il 70%80% della totalit [ 3 , 4 ] , in circa il 60% dei casi sono bilaterali e nel 40%49% dei casi sono associati alla presenza di aneurisma dellaorta addominale [ 5 ]  . 
la causa pi frequente di paa laterosclerosi ; cause rare , soprattutto in pazienti giovani , possono essere rappresentate da pseudoaneurismi iatrogeni o post - traumatici , aneurismi micotici , collagenopatie ( sindrome di ehlers - danlos ) o malattie reumatiche ( malattia di behet ) [ 6 , 7 ]  . 
 [ 8 ] , sono sinistri messaggeri di imminente catastrofe in quanto lembolizzazione distale di frammenti trombotici e / o la trombosi acuta della sacca aneurismatica possono causare importanti ischemie acute darto . 
si stima che il 14%24% allanno di paa asintomatici diventino sintomatici [ 9 ] : le manifestazioni cliniche pi frequenti sono rappresentate da ischemia acuta o cronica con claudicatio intermittens , dolore a riposo o lesioni troche ; compressione della vena poplitea con trombosi venosa profonda o edema dellarto inferiore ; compressione del nervo ischiatico o delle sue branche con dolore urente ; rottura dellaneurisma , complicanza rara ma ad alto rischio di perdita darto [ 10 ]  . 
i principali fattori che inuenzano il trattamento sono le dimensioni dellaneurisma , la morfologia dello stesso , uno scarso runoff distale e la presenza di trombo intramurale emboligeno [ 12 ]  . 
 [ 14 ] i 3 cm : attualmente indicato il trattamento in pazienti con paa sintomatici , indipendentemente dalle dimensioni , o paa asintomatici > 2 cm [ 15 , 16 ] , mentre indicata terapia medica antiaggregante e stretto follow - up per quelli asintomatici < 2 cm [ 12 ]  . 
il trattamento standard rappresentato dallintervento chirurgico con legatura dellaneurisma e by - pass autologo ( vena safena ) o eterologo con politetrauoroetilene ( eptfe ) con approccio mediale o posteriore , con alto successo tecnico e tasso di perviet a 5 anni del 70%80% [ 9 , 11 , 14 , 17 ]  . 
lo sviluppo delle tecniche endovascolari ha reso questo approccio particolarmente interessante nella gestione dei paa , per la possibilit , mutuando lesperienza e la tecnologia endovascolare accumulata nel trattamento degli aneurismi aortici e toracici , di ridurre le complicanze operatorie con analogo risultato in termini di successo tecnico e di perviet a breve e medio termine rispetto allintervento chirurgico radiol med ( 2013 ) 118 : 229238 the effectiveness of endovascular treatment of paas [ endovascular popliteal artery aneurysm repair ( evpar ) ] with a heparin - coated stent - graft and compare preliminary data with those available in the literature . materials and methods between january 2009 and july 2010 , ten patients with paa underwent evpar with placement of a heparin - coated stent - graindications for the procedure were aneurysm dilatation > 20 mm in diameter or symptomatic paa , with a proximal and distal landing zone measuring at least 15 mm in length . 
all patients underwent prior colour doppler ultrasound ( cdus ) to dene paa diameter and length , the presence of mural thrombus , vessel tortuosity , length and diameter of the proximal and distal landing zones and to assess leg vessels . 
obiettivo del nostro studio valutare lefcacia del trattamento endovascolare degli paa ( endovascular popliteal artery aneurysm repair , evpar ) mediante stent ricoperto eparinato , confrontando i nostri dati preliminari con quelli presenti in letteratura . materiali e metodi da gennaio 2009 a luglio 2010 10 pazienti affetti da paa sono stati sottoposti a trattamento endovascolare mediante posizionamento di stent ricoperto eparinato . 
le indicazioni al trattamento erano la presenza di dilatazione aneurismatica di diametro > 20 mm o la presenza di paa sintomatico , con landing zone prossimale e distale di almeno 15 mm di lunghezza . 
in tutti i casi stato eseguito esame eco - color doppler ( ecd ) pre - procedurale , per denire il diametro e la lunghezza del paa , la presenza di trombo parietale , la fig . 
langio - tc pre - trattamento con ricostruzioni multiplanari ( mpr ) documenta la presenza di aneurisma del tratto sovra / retro - genicolato ( a ) parzialmente trombizzato , del diametro assiale massimo di 2 , 3 clangiograa diagnostica preliminare conferma tale reperto ( b ) : laneurisma stato trattato con successo mediante posizionamento di stent viabahn ( c , d )  . 232 radiol med ( 2013 ) 118 : 229238 aneurism site and size and healthy segments upstream and downstream and the state of the distal vessels using dynamic projections with the knee exed . 
to ensure adequate coverage of the aneurysm , stentgraft size was always overestimated by 15 mm proximally and distally to the aneurys especially large aneurysms and those with a difference in diameter of the upstream and downstream vessel were treated with multiple stents , with at least a 20 mm overlap . 
after stent - graft deployment , lowpressure in - stent angioplasty was performed to ensure optimal stent adhesion to the vessel walls , and in the case of multiple stents , to ensure adequate overlap . 
 the technical success of the procedure was dened as complete exclusion of the aneurysm , as evaluated on the nal postprocedural angiograpatency was dened as the presence of stenoses < 50% at the site of the stent , as assessed on follow - up cdus scans at 1 , 6 and 12 months . 
 using a term borrowed from aortic pathology , we dened an endoleak as the presence of blood ow outside the stentgraft lumen but within the aneurysm sac and adopted the conventional classication into four types . the endpoint of the study was to assess the effectiveness of evpar with heparin - bonded stent - graft by analysing technical success and length of the procedure , primary and secondary patency rates at 1 , 6 and 12 months and complication rate . results a total of ten paas in ten patients ( nine men and one woman ) with a mean age of 6912 years underwent evpar . 
a total of 13 stents were deployed , in two cases owing to the different diameter of the proximal and distal landing zones and in one case because the aneurysm involved a long segment of the popliteal artery . 
il follow - up postprocedurale stato effettuato in tutti i pazienti mediante esame ecd a 1 , 6 e 12 mesi dalla procedura . tutte le procedure sono state eseguite in sala angiograca , in anestesia locale . 
mediante puntura anterograda trans - femorale comune omolaterale e accesso vascolare 812 f , stato eseguito angiogramma diagnostico preliminare che ha confermato la sede e le dimensioni dellaneurisma e dei tratti sani a monte e a valle e lo stato dei vasi distali anche con lausilio di proiezioni dinamiche in essione dellarto . 
nei casi di lesione particolarmente estesa o di differente diametro del vaso a monte e a valle , si proceduto al posizionamento di multipli stent , embricati tra loro per almeno 20 mdopo il rilascio dellendograft , stata eseguita angioplastica intrastent a bassa pressione per assicurare una ottimale adesione dello stesso alle pareti del vaso di origine e , nel caso di stent multipli , unadeguata embricatura degli stessi , ed stata quindi eseguita angiograa nale di controllo anche con arto in essione . 
dopo la procedura stata impostata terapia medica con acido acetilsalicilico ( asa ) 100 mg / die e clopidogrel 75 mg / die . il successo tecnico della procedura stato denito come completa esclusione dellaneurisma dopo il rilascio dello stent ed stato valutato allangiogramma nale di controllo . 
la perviet stata denita come presenza di stenosi < 50% del diametro del vaso nella sede dello stent ed stata valutata allecd di follow - up a 1 , 6 e 12 mesi . 
mutuando il termine della patologia aortica , stato denito endoleak la presenza di usso ematico al di fuori dello stent ed allinterno della sacca aneurismatica ed stata adottata la comune classicazione in quattro tipi . lendpoint dello studio stata la valutazione dellef cacia del trattamento endovascolare dellaneurisma popliteo mediante stent ricoperto eparinato , analizzando il successo tecnico e la durata della procedura , la perviet primaria e secondaria ad 1 , 6 e 12 mesi e lincidenza di complicanze . risultati un totale di dieci paa in dieci pazienti ( 9 maschi e 1 donna ) con et media di 6912 anni sono stati sottoposti a evpar . 
in tutti i casi stato impiegato stent ricoperto eparinato tipo viabahn ; in 3 casi sono stati utilizzati n = 2 stent per paziente per un totale di 13 stent , in due casi per differente calibro della landing zone prossimale e distale ed in un caso per presenza di aneurisma coinvolgente larteria poplitea per un lungo tratto . 
in un paziente , a 3 mesi dal posizionamento dello stent si vericata occlusione trombotica dello stesso : giunto al pronto soccorso del nostro ospedale con un quadro di ischemia acuta dellarto inferiore , trattata con successo mediante terapia trombolitica intra - arteriosa e secondaria pta intra - stent . 
al follow - up a 6 mesi abbiamo riscontrato perviet primaria del 90% e perviet secondaria del 100% ; al follow - up a 12 mesi abbiamo ulteriormente osservato analoghi valori di perviet primaria e secondaria ( rispettivamente 90% e 100% ) con riscontro tuttavia di un caso di endoleak di ii tipo ( 10% ) , non associato ad incremento volumetrico della sacca aneurismatica e pertanto non meritevole di alcun tipo di trattamento , ma solo di stretto follow - up . 
 non abbiamo avuto nessun caso di migrazione o frattura dello stent o di dissezioni dei vasi di ancoraggio dello stesso ; in nessun caso stata richiesta amputazione maggiore o minore a causa di embolizzazione distale di trombi parietali . discussione bench il trattamento chirurgico sia ancora lopzione di scelta nel trattamento degli paa [ 1719 ] , il passaggio allera endovascolare sta rapidamente modicando la gestione di tale patologia , rappresentando unopzione sempre pi sicura ed efcace . 
langiograa preliminare documenta la presenza di aneurisma della poplitea nel tratto retro - genicolato ( a ) , trattato mediante posizionamento di stent viabahn ( b , c )  . was lost to follow - up or died during the observation period . 
the patient presented to the hospitals emergency department with acute lowerlimb ischaemia , which was successfully treated with intraarterial thrombolysis and secondary in - stent percutaneous transluminal angioplasty ( pta )  . 
at 12 months , the primary and secondary patency rates remained unchanged ( 90% and 100% , respectively ) , with only one case of type - ii endoleak ( 10% ) that required close surveillance only and no treatment , as it was not associated with enlargement of the aneurysm sac . 
there were no cases of stent migration or fracture or of vessel dissection ; no patient required either major or minor amputation due to distal embolisation of a mural thrombus . discussion although surgery remains the treatment of choice for paa repair [ 1719 ] , transition to the endovascular age is rapidly changing the management of paas , with evpar becomti sforzi sono stati fatti nella ricerca di stent sempre pi adatti al trattamento di tale patologia , spesso con scarsi risultati [ 21 ]  . 
lo stent ricoperto da noi utilizzato costituito da una maglia metallica in nitinolo rivestito internamen te in ptfe , dotato di estrema essibilit , capacit di torsione , compressione longitudinale e forza radiale e riesce pertanto ad adattarsi alla tortuosit dei vasi del distret to femoro - popliteo , contrastando il continuo stress meccanico a cui sottoposto . 
lintervento chirurgico open richiede infatti la dissezione dei tessuti e la modicazione dellanatomia della fossa poplitea con rischio di complicanze locali , con incidenza di infezioni a livello delle ferite chirurgiche del 10%20% [ 23 ]  . 
in uno studio nazionale svedese [ 19 ] sul trattamento chirurgico di paa , si riscontrata unincidenza del 2% di perdita darto post - procedurale , con un tasso signicativo di complicanze post - operatorie neurologiche , infettive , e vascolari ( ematoma )  . 
lintervento chirurgico inoltre gravato da una mortalit dell1 , 6% , da un tasso di crescita post - esclusione della sacca aneurismatica no al 30% , con conseguente possibile rottura della stessa , ed al rischio di sindrome compartimentale [ 2426 ]  . levpar unopzione particolarmente attraente perch radiol med ( 2013 ) 118 : 229238 ing an increasingly safe and effective option . 
characterised by extreme exibility , tolerance to torsion , longitudinal compression and radial force , this stent can adapt to the tortuous femoropopliteal vessels and resists the continuous mechanical stresses observed in this region . 
although offering the best results in the treatment of paas , as demonstrated by a recent meta - analysis [ 22 ] , open surgery is often replaced by evpar owing to the advantages of minimal invasiveness . 
open surgery , in fact , requires tissue dissection and modication of popliteal fossa anatomy , with a risk of local complications and a 10 20% incidence of surgical wound infection [ 23 ]  . 
a national swedish study [ 19 ] on the surgical treatment of paas found a 2% incidence of postoperative limb loss , with a high rate of postoperative neurological , infectious and vascular complications ( haematomas )  . 
surgery is also accompanied by a 1.6% mortality rate , by a 30% rate of aneurysm sac enlargement after exclusion with possible rupture and by a risk of compartment syndrome [ 2426 ]  . evpar is a particularly attractive option because it reduces local complications as well as the duration and technical difculty of the procedure and length of hospital stay . 
it is also particularly suited to patients with severe cardiorespiratory comorbidities for whom surgery is not indicated or for those who refuse open surgery . in a large prospective study of 73 paas treated with evpar , tielliu et al . 
 [ 27 ] reported a primary and secondary patency rate of 77% and 86% at 3 years and of 70% and 76% at 5 years , respectively a result comparable with that of conventional surgery . 
in a previous study [ 28 ] , the same group showed that the most important prognostic factor for long - term patency was administration of clopidogrel , for which there is therefore an absolute indication in patients with popliteal stent - grain our experience , postprocedural medical therapy with clopidogrel ( 75 mg / day ) and asa ( 100 mg / day ) gave good results , so we believe this pharmacological approach should be indicated in the management of these patients . 
 [ 39 ] found primary patency rates of 100 % and 81 % , respectively , at 1 year and of 88% and 71% at 72 months , respectively , with satisfactory results for the use of stents in the popliteal region . 
 [ 30 ] , who reported primary and secondary patency rates of 83% and 100% , respectively , in 15 evpar procedures followed up for an average of 52 months . 
further conrmation of the long - term safety and efcacy of evpar was provided by a recent meta - analysis comparing surgery and evpar [ 31 ] , which found no statistically signicant difference between consente di ridurre le complicanze locali , la durata e la difcolt tecnica della procedura ed il tempo di degenza ospedaliera ; rappresenta inoltre un intervento particolarmente adatto per pazienti con gravi comorbilit cardio - respiratorie per i quali la chirurgia non indicata o per pazienti che riutano lintervento open . in un largo studio prospettico di 73 paa trattati per via endovascolare , tielliu et al . 
 [ 27 ] hanno riportato un tasso di perviet primaria e secondaria a 3 anni rispettivamente del 77% e 86% ed a 5 anni del 70% e 76% , sovrapponibile a quello ottenuto con chirurgia tradizionale . 
in un precedente studio [ 28 ] , lo stesso gruppo ha dimostrato che il pi importante fattore prognostico nel determinare la perviet a distanza la somministrazione di clopidogrel , che rappresenta pertanto una terapia medica post - procedurale assolutamente indicata in pazienti con stent ricoperto popliteo . 
nella nostra esperienza abbiamo impostato una terapia medica post - procedurale con clopidogrel ( 75 mg / die ) ed asa ( 100 mg / die ) , ottenendo buoni risultati ; riteniamo pertanto tale approccio farmacologico indicato nella gestione di questi pazienti . 
 [ 29 ] , in uno studio prospettico di confronto tra 27 aneurismi trattati chirurgicamente e 21 per via endovascolare , hanno riscontrato una perviet primaria ad 1 anno rispettivamente del 100% ( open ) e dell81% ( evpar ) ed a 72 mesi rispettivamente dell88% ( open ) e del 71% ( evpar ) , ottenendo pertanto risultati soddisfacenti con limpiego di stent a livello popliteo . 
 [ 30 ] che , in 15 aneurismi trattati per via endovascolare , hanno riscontrato , ad un lungo follow - up medio di 52 mesi , una perviet primaria e secondaria rispettivamente dell83% e del 100% . 
a sottolineare ulteriormente la sicurezza ed efcacia a distanza del trattamento endovascolare cina [ 31 ] , in una recente metanalisi di confronto tra il trattamento chirurgico e quello endovascolare , ha dimostrato che non si riscontra differenza statisticamente signicativa di perviet primaria ad 1 anno e di perviet primaria e secondaria a 3 anni tra le due opzioni terapeutiche , con perviet primaria e secondaria del gruppo evpar a 1 anno dell83% e 86% ed a 3 anni del 74% e 85% . nella nostra esperienza , abbiamo riscontrato un successo tecnico del 100% , con completa esclusione dellaneurisma in tutti i casi in assenza di complicanze peri e post - procedurali signicative ; la perviet primaria ad un mese dalla procedura stata del 100% . 
 [ 32 ] hanno riscontrato una perviet primaria a 6 mesi dell86% , con due occlusioni trombotiche vericatesi nello stesso periodo 236 radiol med ( 2013 ) 118 : 229238 primary patency at 1 year and primary and secondary patency at 3 years ( primary and secondary patency rates of 83% and 86% at 1 year and of 74% and 85% at 3 years )  . 
 in our limited experience , there was only one case of endoleak ( 10% ) , in line with the literature [ 2935 ] : it was a low - ow type ii endoleak detected at 12 months and not associated with enlargement of the aneurysm sac and thus requiring no treatment . 
there were no cases of stent fracture or migration , demonstrating that the stent - graft was well suited to this region , for years considered a hostile environment due to the knee joint . 
for experienced operators , stent deployment is technically straightforward , ensuring shorter hospital stays and lower costs than surgery , with a lower incidence of local and systemic complications ( none in our series )  . our ndings are therefore in agreement with previous reports and demonstrate that evpar is effective and provides long - lasting results comparable with open surgery [ 36 ]  . 
in our series , all paas were treated with new - generation heparin - coated stents using propaten bioactive surface technology in which the heparin molecules are covalently bonded to the ptfe inner surface through an end - point attachment , ensuring high stability , sustained thromboresistance and no leaching of heparin molecules into the blood ow : these newgeneration stents may therefore ensure a satisfactory level of long - term patency that is comparable with that provided by open surgery . 
our series seems to conrm this potential : at a mean follow - up of 1 year , primary patency was high ( 90% ) , slightly higher than previously reported [ 3235 ] , with only one case of thrombotic occlusion . 
 [ 33 ] , in 57 paa trattati mediante evpar , hanno ottenuto una perviet primaria e secondaria ad 1 anno dell85 , 8% e 87 , 5% , che si assesta su questi valori anche a 3 anni di distanza , come anche documentato da mohan et al . 
 [ 34 ] in una valutazione retrospettiva di 30 paa trattati mediante stent endovascolare , in cui i valori di perviet primaria e secondaria erano rispettivamente a 6 mesi 84 , 7% e 88 , 7% , a 12 mesi 80% e 88 , 7% , a 24 e 36 mesi 74 , 5% e 83 , 2% . 
 nella nostra limitata esperienza abbiamo riscontrato un solo caso di endoleak ( 10% ) , in linea con i dati della letteratura [ 2935 ] : si trattava di un endoleak di ii tipo a basso usso riscontrato a 12 mesi , non associato ad incremento volumetrico della sacca aneurismatica e pertanto non meritevole di alcun trattamento . 
in operatori esperti il posizionamento di stent risulta pertanto tecnicamente semplice , garantendo una ridotta degenza e quindi ridotti costi rispetto al trattamento chirurgico , con una minore incidenza di complicanze locali e sistemiche ( nessuna nella nostra casistica )  . i dati da noi ottenuti pertanto sono in linea con quelli presenti in letteratura e documentano lefcacia del trattamento endovascolare degli paa con risultati duraturi nel tempo , sovrapponibili a quelli ottenuti con il trattamento chirurgico tradizionale [ 36 ]  . 
nella nostra esperienza tutti i paa sono stati trattati mediante stent eparinati di nuova generazione , con tecnologia propaten bioactive surface , in cui il legame delle molecole di eparina alla supercie interna in ptfe del graft di tipo covalente ter mino - terminale , che assicura unalta stabilit di legame , con tromboresistenza duratura nel tempo e mancato ri lascio delle molecole di eparina nel usso ematico : tali stent di ultima generazione potrebbero pertanto garantire un soddisfacente grado di perviet a distanza di tem po , sovrapponibile a quello ottenuto con la chirurgia tradizionale . 
nella nostra casistica tale potenzialit sembra essere confermata : ad 1 anno di follow - up abbia mo riscontrato un alto valore di perviet primaria ( 90% ) , leggermente superiore agli studi sino ad ora pubblicati [ 3235 ] , con un solo caso di occlusione trombotica ; tuttavia necessario un pi lungo follow - up con un numero maggiore di pazienti trattati per poter esprimere dei giudizi denitivi . 
 i limiti del nostro studio sono rappresentati dal ridotto numero di pazienti e dal breve follow - up : si tratta tuttavia di una patologia rara per cui difcile disporre , in un singolo radiol med ( 2013 ) 118 : 229238 tients and the short follow - up period : however , paa is a rare condition , and it is difcult for a single centre to bring together a large patient cohort . consistent with the literature , evpar with new - generation covered stent - grafts is a safe and effective option ensuring good patency rates over time . 
scuro 10 , 37134 verona , italy , tel . : + 39 - 045 - 8124301 , fax : + 39 - 045 - 8027490 , e - mail : albertocontro@gmail.com received : 8 june 2011 / accepted : 12 september 2011 / published online : 14 may 2012 springer - verlag 2012 abstract purpose . 
 this treatment , when performed in the angiography room , is safe and effective and is probably relatively uncommon and underused . keywords postpartum haemorrhage arterial embolization bleeding hysterectomy riassunto obiettivo . 
nel periodo compreso tra gennaio 2004 e dicembre 2010 stato condotto uno studio prospettico non randomizzato in cui 10 donne con diagnosi di ep severa sono state sottoposte a trattamento endovascolare in emergenza . 
 il trattamento in sala angiograca sicuro , efcace e probabilmente poco diffuso e sotto - utilizzato . parole chiave emorragia post - partum embolizzazione arteriosa sanguinamento isterectomia 216 introduction postpartum haemorrhage ( pph ) is one of the most frequent causes of maternal mortality . 
pph affects 5% of all deliveries and is the direct cause of about 140 , 000 maternal deaths each year : it is responsible for the one maternal death every 4 min , with half of these deaths occurring within 24 h of delivery . 
 when not fatal , pph causes severe morbidity : sequelae include adult respiratory distress syndrome , coagulopathy , shock and pituitary necrosis ( sheehans syndrome ) [ 1 ]  . 
the 2004 report of the condential enquiry into maternal and child health ( cem - ach ) , published in the uk every 3 years by the royal college of obstetricians and gynaecologists , describes 17 deaths directly attributable to bleeding ( three from placental abruption , four from placenta praevia , and ten from pph without abnormal placental implantation ) , for a total of 8.5 deaths per 1 , 000 , 000 pregnancies [ 2 ]  . 
for each patient dying from bleeding , more than 60 women undergo peripartum hysterectomy . the purpose of this study was to assess the indications for and technique and results of endovascular treatment for pph . 
endovascular treatment for severe pph was performed in an emergency setting for women experiencing an estimated blood loss > 2 , 500 ml and / or > 5 u of blood transfused and / or haemorrhage with superimposed coagulopathy [ 4 ]  . 
haemoglobin ( hb ) values ranged from a minimum of 4.9 g / dl to a maximum of 10.6 g / dl ( mean 6.8 g / dl ) , whereas haematocrit ( ht ) varied between 14% and 30.3% ( mean , 20% )  . 
lep ha incidenza del 5% nella totalit dei parti ed causa diretta di circa 140.000 morti materne / anno : responsabile di 1 morte di donna gravida ogni 4 minuti , la met dei decessi avviene entro 24 ore dal parto . 
 quando non letale , alla ep consegue grave morbilit : le sequele includono la sindrome da stress respiratorio delladulto , coagulopatia , shock e necrosi delliposi ( sindrome di sheehan ) [ 1 ]  . 
listerectomia peri - partum frequentemente eseguita per trattare lemorragia ostetrica che minaccia la sopravvivenza della donna e pu quindi essere considerata un near miss event per la mortalit materna da emorragia . 
 il rapporto del 2004 del condential enquiry nel maternal and child health ( cem - ach ) , pubblicato in gran bretagna ogni tre anni dal royal college of obstetrician and gyneacologists , riporta 17 decessi direttamente imputabili ad emorragia ( 3 per distacco di placenta , 4 per placenta previa e 10 per ep senza anomalie di impianto placentare ) , per un totale di 8 , 5 morti per 1000000 gravidanze [ 2 ]  . 
 lunited kingdom obstetric surveillance system ( ukoss ) [ 3 ] ha riportato uno studio osservazionale della durata di 13 mesi in cui 315 donne sono state sottoposte ad isterectomia peri - partum per controllare lemorragia con tasso del 41 , 0 per 100.000 gravidanze : lintervallo di condenza stato del 95% , compreso fra 36 , 6 e 45 , 8 su 100.000 gravidanze ; per ogni paziente deceduta per emorragia , pi di 60 donne sono sottoposte ad isterectomia peri - partum . obiettivo di questo lavoro valutare indicazioni , tecnica e risultati del trattamento endovascolare della ep . 
 il trattamento endovascolare stato espletato in emergenza per ep severa : perdita di sangue stimata maggiore di 2500 ml e / o pi di 5 unit di sangue trasfuse e / o quadro emorragico con sovrapposta coagulopatia [ 4 ]  . 
the procedure began with aortography by means of a 5 - f pigtail catheter ( cordis , miami , fl , usa ) with tip placed above the renal arteries . 
images were obtained using digital subtraction angiography ( dsa ) after injection of 20 ml of high iodine concentration nonionic contrast material ( 370 mg / ml ) at a ow rate of 10 ml / s through an automatic injector . 
selective acquisitions of the hypogastric artery were then obtained following catheterisation of the vessel with a 5 - f cobra 2 catheter ( terumo , tokyo , japan )  . 
la procedura iniziata con aortograa mediante caterere pigtail ( cordis , miami , florida , usa ) del calibro di 5 french con estremo posizionato al di sopra delle arterie renali . 
le acquisizioni sono state ottenute in sottrazione digitale ( dsa ) con iniezioni di 20 ml di mezzo di contrasto iodato non ionico ad elevata concentrazione ( 370 mg / ml ) mediante iniettore automatico ad una velocit di 10 ml al secondo . 
 il cateterismo selettivo dellarteria ipogastrica omolaterale allaccesso percutaneo stato eseguito ansando il catetere in aorta addominale con tecnica waltman loop . 218 radiol med ( 2013 ) 118 : 215228 percutaneous access was achieved by looping the catheter in the abdominal aorta following the waltman loop technique . 
in cases in which dsa diagnosed bleeding resulting from focal arterial laceration , selective embolisation of the lacerated vessel was achieved with a 5 - f diagnostic catheter and a coaxial microcatheter . 
when the segment of artery downstream from the laceration could not be reached , glubran 2 glue ( 1 ml diluted 1 : 1 with the oil - based contrast agent lipiodol ) was used alone or in combination with microcoils . 
in cases in which dsa diagnosed diffuse bleeding from uterine atony or posthysterectomy bleeding , bilateral embolisation of the hypogastric artery branches downstream from the superior gluteal artery was performed using reabsorbable material ( spongostan ) and a diagnostic catheter . the nal check was conducted by repositioning the pigtail catheter in the suprarenal abdominal aorta to conrm bilateral occlusion of the hypogastric arteries and reperfusion of the site of the haemorrhage through the ovarian arteries or the external pudendal arteries . 
nei casi in cui la dsa ha diagnosticato sanguinamento conseguente a lacerazione arteriosa focale stata effettuata una embolizzazione selettiva del vaso lacerato utilizzando catetere diagnostico del calibro di 5 french e microcatetere coassiale . 
quando non stato possibile raggiungere il tratto di arteria a valle della lacerazione , stata utilizzata colla glubran 2 ( 1 ml diluito in rapporto 1 : 1 con mezzo di contrasto oleoso lipiodol ) , da sola o in associazione alle microspirali . 
nei casi in cui la dsa ha diagnosticato sanguinamento diffuso da atonia uterina o post - isterectomia stata espletata lembolizzazione bilaterale dei rami arteriosi dellarteria ipogastrica a valle dellarteria glutea superiore con materiale riassorbibile ( spongostan ) attraverso catetere diagnostico . il controllo nale stato effettuato riposizionando il catetere pig - tail in aorta addominale sovra - renale per confermare locclusione bilaterale delle arterie ipogastriche e leventuale riperfusione del sito emorragico da parte delle arterie ovariche o delle arterie pudende esterne . 
b il radiogramma diretto dopo embolizzazione trans - catetere delle arterie uterine con spongostan dimostra larresto bilaterale del usso arterioso con ristagno prolungato di mezzo di contrasto nel tratto prossimale di entrambe le arterie uterine ( frecce )  . 220 radiol med ( 2013 ) 118 : 215228 fig . 
a dsa with injection through a coaxial catheter , with tip placed inside the right internal pudendal artery , shows an arterial laceration near the trifurcation of the internal pudendal artery and vaginal bleeding ( arrowheads )  . 
a la dsa con iniezione da catetere coassiale il cui estremo posizionato in arteria pudenda interna di destra evidenzia la lacerazione arteriosa in corrispondenza della triforcazione della arteria pudenda interna ed il sanguinamento vaginale ( testa di freccia )  . 
nei rimanenti 2 , le pazienti dopo lembolizzazione sono state sottoposte a nuova laparotomia con rimozione dei coaguli , emostasi chirurgica e zaffatura con garze che ha determinato larresto completo del sanguinamento . 
a 72 ore , i valori dellhb variavano da un minimo di 8 , 2 g / dl ad un massimo di 13 , 4 g / dl con valore medio di 10 , 65 g / dl , mentre lht variava da un minimo di 24% ad un massimo di 40 , 9% con un valore medio di 31 , 5% . discussion transcatheter embolisation has been used successfully for many years to treat severe , spontaneous , iatrogenic and traumatic arterial haemorrhage . 
a dsa with injection through a coaxial catheter , with its end placed in the left inferior haemorrhoidal artery , shows the site of bleeding ( arrowheads ) and indicates that a distal endovascular ligation with microcoils cannot be performed . 
b after the injection of acrylic glue diluted 1 : 1 with lipiodol , shows radiography residual radiopaque glue in the collection and cast of distal branches of the inferior haemorrhoidal artery ( arrows )  . 
a la dsa con iniezione da catetere coassiale il cui estremo posizionato in arteria emorroidaria inferiore di sinistra evidenzia la sede del sanguinamento ( teste di freccia ) e la impossibilit di procedere alla legatura endovascolare distale con microspirale . 
b dopo la iniezione di colla acrilica con diluizione 1 / 1 con lipiodol , il radiogramma diretto dimostra i residui di colla x - opaca nella raccolta ed il calco dei rami distali dellarteria emorroidaria inferiore ( frecce )  . 
c , d la dsa selettiva con iniezione in arteria ipogastrica omolaterale ( c ) e controlaterale ( d ) conferma larresto del sanguinamento . posed for treating pph by brown et al . 
pph after spontaneous delivery with vaginal bleeding and / or an important vaginal haematoma : in this case , dellarteria media circonessa in una paziente gi sottoposta ad intervento di legatura delle arterie ipogastriche ed isterectomia per emorragia severa . 
in questa evenienza lesame clinico permette di sospettare la sede del sanguinamento , ma il trattamento chirurgico ha grandi difcolt tecniche nellisolamento e nella 222 radiol med ( 2013 ) 118 : 215228 fig . 
evidence of outcomes of hysterectomy with corpuscular uid collection and gas bubbles in the lesser pelvis ; thin contrast - medium collection on the left side of the midline , consistent with arterial bleeding ( arrowheads in c )  . 
e arterial - phase 3d reconstruction clearly shows temporary clamping of the aorta just above the carrefour ( arrows ) and active bleeding of the anterior branches of the left hypogastric artery ( arrowhead )  . 
in piccolo bacino si evidenziano gli esiti di isterectomia con raccolta corpuscolata e bolle gassose ; a sinistra della linea mediana si evidenzia sottile raccolta di mezzo di contrasto compatibile con sanguinamento arterioso ( teste di freccia in c )  . 
e la ricostruzione tridimensionale in fase arteriosa bene dimostra il clampaggio provvisorio dellaorta in sede immediatamente craniale alla biforcazione ( frecce ) ed il sanguinamento attivo dai rami anteriori dellarteria ipogastrica sinistra ( testa di freccia )  . 
f la ricostruzione tridimensionale in fase venosa evidenzia il progressivo accumularsi del sangue opaco in piccolo bacino ( testa di freccia )  . radiol med ( 2013 ) 118 : 215228 fig . 
a dsa with aortic injection shows a signicant peripheral vasoconstriction near the external iliac arteries in contrast with the diameter of common iliac arteries and particularly with that of hypogastric arteries , which show an increased diameter and more apparent bleeding on the left side ( arrowhead )  . 
a la dsa con iniezione in aorta evidenzia importante vasocostrizione periferica in corrispondenza delle arterie iliache esterne che contrasta con il calibro delle arterie iliache comuni e soprattutto con quello delle arterie ipogastriche che hanno calibro aumentato e sanguinamento pi evidente a sinistra ( testa di freccia )  . 
c , d dopo embolizzazione trans - catetere bilaterale dei rami anteriori dellarteria ipogastrica con spongostan e legatura endovascolare dellarteria ipogastrica di sinistra con spirale posizionata a valle dellorigine della arteria glutea superiore ( freccia in c ) , la dsa selettiva con iniezione in arteria ipogastrica sinistra e destra conferma la occlusione bilaterale dei rami anteriori ( frecce )  . 224 radiol med ( 2013 ) 118 : 215228 fig . 
7a , b severe pph in a puerpera treated with hysterectomy and surgical ligation of the hypogastric arteries : multiple radiopaque gauzes can be observed in the small pelvis ( asterisks ) after hysterectomy . 
7a , b ep severa in puerpera sottoposta ad isterectomia e legatura chirurgica delle arterie ipogastriche : in piccolo bacino sono riconoscibili multiple garze radiopache ( asterischi ) in esiti di intervento chirurgico di isterectomia . 
the glue correctly diluted with lipiodol and injected through a microcatheter immediately upstream from the arterial laceration and carried by the arterial blood ow can achieve rapid and denitive occlusion of the vessel upstream and downstream from the rupture . 
once the bleeding artery has been denitively occluded , it is always advisable to perform selective diagnostic angiography of the contralateral hypogastric artery to exclude persisting supply to the lacerated artery from the collateral circulation . 
la colla , diluita correttamente con lipiodol , iniettata attraverso microcatetere immediatamente a monte della lacerazione arteriosa e trasportata dal usso arterioso , in grado di occludere rapidamente ed in maniera denitiva il vaso a monte ed a valle della rottura . 
dopo aver occluso in modo denitivo il vaso arterioso sede del sanguinamento buona norma espletare sempre angiograa diagnostica selettiva in arteria ipogastrica controlaterale per escludere che la collateralit rifornisca ancora larteria lacerata . 
d dopo la rimozione della compressione del tamponamento vaginale e lo svuotamento della vescica , la dsa selettiva con iniezione in arteria ipogastrica dimostra la lesione arteriosa ed il sanguinamento attivo ( teste di freccia )  . experience , embolisation successfully arrested pph in all patients affected by vaginal bleeding . 
the value of this treatment has been conrmed in large series of patients with posttraumatic arterial bleeding of the lesser numericamente importanti nei sanguinamenti arteriosi post - traumatici del piccolo bacino . 
in the case of pph secondary to uterine atony and unresponsive to medical therapy , the interventional procedure was performed under emergency conditions before hysterectomy via laparotomy : in our experience , dsa readily diagnosed diffuse uterine bleeding consequent to uterine hypotony . 
selective angiography of the hypogastric arteries showed pooling of contrast material in the area of the gravid uterus and hypertrophy of the uterine vessels , and embolisation of the uterine arteries with absorbable material ( spongostan ) proved effective . 
embolisation of the hypogastric arteries with absorbable material even when failing to achieve complete clinical success , greatly reduces arterial blood ow to the uterus and does not interfere with subsequent surgical measures or with hysterectomy , if needed . 
according to the american college of obstetricians and gynaecologists ( acog ) , hysterectomy for uterine atony should only be considered after having attempted all possible approaches , including endovascular therapy [ 9 ] and uterine tamponade ( with gauzes , foley catheter , sengstakenblakemore tube , bakri balloon )  . 
in our experience surgical ligation of the hypogastric arteries associated with hysterectomy proved ineffective and complicated the subsequent embolisation . in post - hysterectomy pph , the procedure was successful in two of four patients , but the following surgery was decisive in the two cases of failure . 
 in the second case , in a patient who had already undergone hysterectomy and surgical and endovascular ligation of the hypogastric arteries , surgical exploration showed persistent bleeding from the afferent ovarian arteries . 
nella nostra esperienza la dsa ha agevolmente diagnosticato il sanguinamento uterino diffuso conseguente allipotonia uterina : langiograa selettiva delle arterie ipogastriche evidenzia ristagno di mezzo di contrasto nellarea dellutero gravidico ed ipertroa dei vasi uterini e lembolizzazione delle arterie uterine con materiale riassorbibile ( spongostan ) sino allarresto del usso si dimostrata efcace . 
lembolizzazione con materiale riassorbibile delle arterie ipogastriche , anche quando non abbia completo successo clinico , riduce sensibilmente lafferenza arteriosa allutero e non interferisce con eventuali successivi provvedimenti chirurgici o con listerectomia , se necessaria . 
lamerican college of obstetrician and gynaecologists ( acog ) indica che listerectomia per atonia uterina dovrebbe essere presa in considerazione solo dopo aver messo in atto tutte le possibilit terapeutiche tra cui il trattamento endovascolare [ 9 ] ed il tamponamento dellutero ( con garze , catetere di foley , tubo di sengstaken - blakemore , pallone di bakri ) che dovrebbe esser preso nuovamente in considerazione qualora la procedura intervenzionale fosse risultata poco efcace [ 1013 ]  . 
punto determinante di questo approccio sta nel fatto che il successo del trattamento endovascolare da solo o in associazione al tamponamento uterino evita listerectomia e conserva la fertilit della donna . 
nella nostra esperienza la legatura chirurgica delle arterie ipogastriche associata ad isterectomia si dimostrata inefcace ed ha complicato la successiva embolizzazione . nella ep post - isterectomia la procedura ha avuto successo in 2 / 4 pazienti , ma il seguente intervento chirurgico stato risolutivo nei due insuccessi . 
nel secondo , in una paziente gi sottoposta ad isterectomia e legatura chirurgica ed endovascolare delle arterie ipogastriche , lesplorazione chirurgica ha evidenziato il persistere del sanguinamento da afferenze arteriose ovariche . 
anche in questi due casi lembolizzazione preliminare stata a nostro avviso importante in quanto ha permesso di ristabilire le condizioni coagulative ed emodinamiche adiuvanti lintervento chirurgico . radiol med ( 2013 ) 118 : 215228 cases , we found preliminary embolisation important , as it allowed us to restore coagulation and haemodynamic conditions , thus facilitating surgery . in our experience , endovascular treatment of pph was free from complications . 
 reported an incidence < 1.6% in a series of 14 patients [ 14 ] ; badawy et al . , in a review of 138 cases of arterial embolisation for pph covering 20 years , reported a complication rate of 8.7% , with the most frequent events being fever , lowerlimb ischaemia , necrosis of the bladder or rectal wall , injuries to nerve structures and late rebleeding [ 15 ]  . 
 [ 17 ] conducted a systematic review of all studies that evaluated success rates of treatment of severe pph with uterine balloon tamponade , uterine compression sutures , pelvic devascularisation and arterial embolisation . 
 they concluded that although there is no evidence of an optimal method for managing severe pph ( table 2 ) , arterial embolisation does ensure a high rate of clinical success with the lowest degree of invasiveness and without precluding further intervention [ 17 ]  . in the uk , recent reports recommend that gynaecologists should consider all possible measures to stop the bleeding , including transcatheter pelvic embolisation , before contemglobalmente nella nostra esperienza il trattamento endovascolare della ep non stato gravato da complicanze . 
 [ 15 ] in una review su 138 casi di embolizzazione arteriosa per ep occorsi in 20 anni descrivono un tasso di complicanze dell8 , 7% che vede come pi frequenti febbre , ischemia degli arti inferiori , necrosi della parete vescicale o rettale , lesioni di strutture nervose e risanguinamento tardivo . 
 [ 17 ] hanno condotto una revisione sistematica per identicare tutti gli studi che valutano i tassi di successo nel trattamento della ep severa mediante limpiego di tamponamento uterino con palloncino , suture compressive uterine , devascolarizzazione pelvica ed embolizzazione arteriosa . 
dal momento che dalla ricerca non emerso alcun trial randomizzato controllato , gli autori hanno spostato la loro attenzione sugli studi osservazionali ( 396 pubblicazioni ) selezionandone 46 che sono stati inclusi nella revisione sistematica . 
inoltre raccomandato a tutti gli ospedali dotati di unit parto di istituire un servizio di radiologia interventistica di emergenza dal momento che questo ha la potenzialit di salvare la vita delle pazienti con ep severa [ 2 , 18 ]  . conclusions conclusioni careful clinical assessment of pph , immediate correction of coagulation abnormalities and immediate access to angiography and endovascular treatment can , in our opinion , have a signicant impact on reducing hysterectomy and mortality rates due to pph . 
our experience and review of the literature indicate that treating pph in the angiography room with endovascular ligation and / or transcatheter embolisation is safe and effective , although it is probably relatively uncommon and underused . lattenta valutazione clinica delle perdite ematiche nel post - partum , la correzione immediata delle alterazioni della coagulazione ed il ricorso immediato alla angiograa ed al trattamento endovascolare possono , a nostro avviso , avere impatto signicativo nella riduzione delle isterectomie e della mortalit per ep . 
frascisco1 1department of emergency medicine , san luigi gonzaga university hospital , torino , italy 2department of emergency medicine , new york methodist hospital , ny , usa 3institute of radiology , san luigi gonzaga university hospital , torino , italy correspondence to : l . 
radiologia , ospedale san luigi gonzaga , regione gonzole 10 , orbassano , 10040 torino , italy , e - mail : luciano.cardinale@gmail.com received : 7 july 2011 / accepted : 26 october 2011 / published online : 28 june 2012 springer - verlag 2012 abstract chronic heart failure is a complex clinical syndrome often characterised by recurrent episodes of acute decompensation . 
the latest developments in lung us are not because of technological advance but are based on new applications and discovering the meanings of specic sonographic artefacts designated as b - lines . 
real - time sonography of the lung targeted to detection of b - lines allows bedside diagnosis of respiratory failure due to impairment of cardiac function , as well as quantication and monitoring of pulmonary interstitial uid . 
lung us saves time and cost , provides immediate information to the clinician and relies on very easy - toacquire and highly reproducible data . keyword heart failure pulmonary congestion pulmonary interstitial uid lung ultrasound respiratory failure riassunto linsufcienza cardiaca cronica una complessa sindrome clinica caratterizzata spesso da episodi ricorrenti di scompenso acuto . 
lecograa polmonare mirata alla identicazione delle linee b permette la diagnosi al letto del paziente in tempo reale dellinsufcienza respiratoria dovuta a scompenso cardiaco , cos come la quanticazione ed il monitoraggio della congestione polmonare . 
la tecnica ecograca polmonare riduce i tempi ed i costi diagnostici , e si basa su segni semplici da identicare ed altamente riproducibili che forniscono immediate informazioni nella gestione del paziente . radiol med ( 2013 ) 118 : 196205 parole chiave insufcienza cardiac congestione polmonare fluidi interstiziali polmonari ecograa polmonare insufcienza respiratoria congestion in heart failure ods , usually performed exclusively in the intensive care and cardiology settings . exacerbation of heart failure is a complex condition , the main feature of which is haemodynamic pressure overload . 
 when excess uid is redistributed within the lungs , congestion results in interstitial and alveolar oedema , causing what is commonly named pulmonary congestion [ 1 , 2 ]  . 
invasive measurement of pressure across pulmonary capillaries by a pulmonary artery catheter , the pulmonary capillary wedge pressure ( pcwp ) , represents a good estimate of pressure overload due to congestive heart failure [ 3 , 4 ]  . 
another important sign of decompensation is high values of cardiac left ventricular lling pressure ( lvfp ) , which usually indicates lung redistribution of uids , which can be the rst step towards the development of pulmonary oedema . 
for instances , it has been shown that measuring pressure overload by pulmonary artery catheter in patients hospitalised for acute decompensated heart failure is a useful tool for correct management of the disease [ 3 ]  . however , measuring pcwp and lvfp is not essential in the challenging process of clinical management of heart failure for at least two main reasons . 
first , pulmonary interstitial uid and alveolar oedema are not always the direct consequence of uid accumulation but very often are the result of redistribution induced by vascular mechanisms [ 5 ]  . 
the evaluation study of congestive heart failure and pulmonary artery catheterization effectiveness ( escape ) trial showed no impact on overall mortality and hospitalisation rates of pulmonary artery catheter - guided therapy over therapy guided by clinical evaluation and judgement alone in heart failure patients [ 4 ]  . 
for this reason , clinicians should be aware of the clear difference existing between peripheral and pulmonary uid , which are two different aspects of the phenomenon of pressure overload in congestive heart failure that can coexist and be symptomatic ( clinical congestion ) or be separate and even silent [ 5 ]  . 
the second factor that limits the routine use of pcwp and lvfp in managing heart failure is that these data are not easy to acquire because they are measured by invasive and sophisticated methevaluating congestion and pulmonary interstitial uid in daily practice , peripheral congestion and pulmonary interstitial uid are assessed by clinical evaluation and some simple instrumental tests . 
often , symptoms of pressure overload , such as dyspnoea , pulmonary rales , weight gain with oedema and jugular venous distension may develop several days after the increase of the values of pcwp and lvfp [ 68 ]  . 
on the other hand , it is also known that clearance of symptoms during hospital stay of patients admitted for acute decompensated heart failure is not always linked to a stable real improvement of uid accumulation . 
finally , it has been shown that physical ndings of uid accumulation are neither sensitive nor specic for congestive heart failure , even if examination is performed by an expert physician [ 9 , 10 ]  . guidelines of the european society of cardiology recognise chest radiography , cardiac natriuretic peptides and echocardiography ( ecg ) as essential tools for evaluating patients with known or suspected heart failure [ 11 ]  . 
other radiological signs of pulmonary interstitial uid , such as peribronchial cufng and septal lines , are highly dependent on image quality and reader experience ( clinician vs radiologist reading ) [ 13 , 14 ]  . 
radiological signs of vascular overload , such as vascular pedicle and azygos vein enlargement , have different values of accuracy depending on patient position during imaging ( erect vs supine )  . 
in general , each individual sign of heart failure at chest radiography is inadequate , with only moderate accura198 radiol med ( 2013 ) 118 : 196205 cy and particularly limited sensitivity , and the overall radiological impression reaches good accuracy in the emergency diagnosis of congestive heart failure only when a rigorous grading technique is applied [ 15 ]  . 
recognising congestive heart failure with the patient in the semierect or supine position using portable radiography depends to a greater extent on the presence of pulmonary oedema , a condition detected as central alveolar oedema only in more severe cases [ 16 , 17 ]  . 
lastly , the absence of chest radiographic ndings of pulmonary interstitial uid does not exclude the presence of a high pcwp , even when > 30 mmhg [ 18 ]  . natriuretic hormones are useful in the follow - up of patients with heart failure , but some doubts remain about their utility in the initial diagnosis and the real cutoff values between normal and pathologic [ 1923 ]  . ecocardiography still remains the standard criterion for diagnostic evaluation of patients with heart failure , especially for assessing systolic and diastolic cardiac function . 
the ratio of peak early mitral ow velocity ( e ) divided by mitral annular early diastolic velocity ( e0 ) by tissue doppler imaging ( e / e0 ) , that strictly correlate with lvfp and allow indirect estimate of pcwp [ 24 , 25 ]  . 
 moreover , it does not allow direct evaluation and follow - up of pulmonary interstitial uid during acute decompensation . recognising , quantifying and monitoring pulmonary interstitial uid is essential when evaluating patients with established or suspected heart failure . 
assessing pulmonary interstitial uid allows clinicians to recognise a cardiogenic cause of respiratory failure upon arrival in the emergency department or to evaluate appropriateness of discharge in hospitalised patients admitted for decompensated heart failure . 
lung uid accumulation can develop well before the appearance of clinical signs during the slow process of decompensation of established heart failure , and its early detection and treatment could prevent hospitalisation [ 7 , 8 ]  . 
thus , in acutely dyspnoeic patients in the emergency department and in established heart failure outpatients and inpatients , pulmonary interstitial uid should be routinely investigated to recognise heart failure , to treat impending worsening and to avoid inappropriately early discharge [ 5 ]  . 
this method should be sensitive enough to distinguish pulmonary interstitial uid from peripheral congestion , which , as said , can be dissociated . utility of lung ultrasound in the past , respected sources considered sonography as having inherent limitations in lung evaluation . 
this consideration , together with the widespread use of conventional chest radiographic examination and the development of new thoracic imaging technologies , prevented for many years progress in lung us procedures . 
over the last two decades , the concept of using sonography as a real - time bedside clinical tool ( point of care ) in the hands of the same physician who is treating the patient is obtaining a growing consensus , which has led to a number of new applications . 
 quite recently , lung us opened new perspectives in the bedside evaluation of lung water , and many authors produced a growing number of papers showing its accuracy in diagnosing pulmonary diseases [ 2729 ]  . 
particularly , some vertical echogenic linear artefacts , designated as b - lines , are simple , noninvasive and semiquantitative signs of pulmonary interstitial uid that can be evaluated at bedside . 
 interstitial syndrome the relationship between diffuse lung interstitial involvement in diseases and the generation of multiple and bilateral sonographic b - lines was shown by a rst study published in 1997 [ 32 ]  . 
the authors examined a critically ill population ( n = 250 ) undergoing invasive ventilation in the intensive care unit and compared lung us for b - lines with the radiological diagnoses ( chest radiography and ct scan )  . 
questo avviene tipicamente nelledema polmonare , dove alveoli normalmente aerati coesistono con strutture ricche di uidi ( i setti interlobulari ispessiti e / o gli alveoli con contenuto uido )  . pulmonary brosis , with similar frequency and only slight difference in distribution between these diagnostic categories . 
the fundamental technique for diagnosing interstitial syndrome consisted of examining the anterior and lateral chest using four intercostal scans per side , corresponding to the upper and inferior areas anteriorly and the upper and basal areas laterally . 
a positive scan was characterised by a minimum of three b - lines , whereas a positive examination was dened by at least two positive areas per side [ 33 ]  . 
simple detection of b - lines does not allow differentiation of the disease involving the lung interstitium , but other us signs can be used to conrm the diagnosis of congestive heart failure . 
focused cardiac sonography can be performed using the same probe as that for lung examination , looking for global left ventricular function impairment , which will be detected in about 50% of cases of acute decompensated heart failure [ 34 ]  . 
the same probe can also be used to detect an even smaller amount of anechoic pleural effusion , which is a frequent condition in heart failure , with a diagnostic accuracy higher than chest radiography and very close to ct scan [ 35 , 36 ]  . 
finally , assessment of the proximal inferior vena cava can be also performed during the same us examination , and a pattern of dilation with limited or absent respiratory excursion of its diameter can conrm heart failure . measuring lung water since the publication of the rst articles showing the usefulness of lung us in the diagnosis of interstitial syndrome in critically ill and emergency medicine patients , others have followed . 
in caso di polmone normalmente aerato con interstizio regolare , lunica immagine che pu essere visualizzata la riessione sotto la linea pleurica della immagine della parete toracica dalla sonda alla pleura parietale , mentre non sono visualizzabili artefatti verticali ( o eventualmente solo pochi di essi )  . then admitted to beds in emergency medicine . 
the population examined was different from that of the previous study performed in the intensive care unit , because patients were spontaneously breathing , not critically ill , and were affected by more varied and multiple diseases . 
b - lines were detected mainly in patients with cardiogenic pulmonary oedema , interstitial pneumonia , multiple - foci bacterial pneumonia and 200 radiol med ( 2013 ) 118 : 196205 acute decompensated heart failure [ 41 ]  . 
the study authors concluded that blines could be easily used as a bedside method to assess the efcacy of treatment and clearing of pulmonary interstitial uid in these hospitalised patients . another important contribution to demonstrating the usefulness of b - lines in the follow - up of pulmonary interstitial uid comes from studies of lung us in evaluating patients undergoing haemodialysis [ 42 , 43 ]  . 
once more , data from these studies support lung us as a useful method for evaluating real - time changes in evlw and assessing pulmonary response to removal of uid overload . differential diagnosis of cardiogenic pulmonary interstitial uid the primary diagnosis of pulmonary interstitial uid in the emergency setting is crucial for the differential diagnosis between a cardiogenic and noncardiogenic respiratory failure . 
in a study performed in dyspnoeic patients in the emergency department , diffuse b - lines were detected in 100% of patients with cardiogenic pulmonary oedema but was absent in 92% of cases with exacerbation of copd and 98.75% of those with normal lungs [ 44 ]  . 
the conclusion of the study was that sonographic detection of b - lines might help distinguish pulmonary oedema from exacerbation of copd . other studies show the correlation between b - lines and natriuretic peptides in the primary evaluation of acute decompensated heart failure in the emergency department [ 45 , 46 ]  . 
conclusions from these studies is that lung us can be used alone or can provide additional predictive power to natriuretic peptides in the immediate evaluation of dyspnoeic patients and detection of the cardiac origin of the symptom . scoring pulmonary interstitial uid the importance of lung us for b - lines is that it can also be fig . 
quando un pattern simile viene visualizzato in multiple aree del torace anteriore e laterale , si fa diagnosi di sindrome interstiziale ecograca . amount of extravascular lung water ( evlw )  . 
the number of b - lines detected by lung us in patients undergoing cardiac surgery was directly related to the amount of evlw assessed by a semiquantitative chest radiography and the invasive thermodilution method [ 37 , 38 ]  . 
these papers paved the way for the use of lung us in the follow - up of pulmonary interstitial uid in the cardiology setting in selected patients with known heart failure and without pulmonary diseases . 
the same authors also showed the importance of b - lines as a prognostic indicator , showing that mortality is related to the amount of lung water during acute decompensation [ 39 ]  . 
the sonographic method used to measure extravascular lung water is based on semiquantication of b - lines , which is more time consuming than the eight - area technique explained earlier . monitoring pulmonary interstitial uid the strict correlation between b - lines and evlw allows us to speculate about the usefulness of lung us in the followup of pulmonary interstitial uid . 
a recent study showed that b - lines signicantly cleared after adequate treatment during the hospital stay in patients admitted for radiol med ( 2013 ) 118 : 196205 fig . 
si trattava di un caso di grave insufcienza cardiaca inizialmente refrattaria alla terapia , nel quale la risoluzione delledema polmonare si ottenuta solo dopo 4 settimane dal ricovero . 202 radiol med ( 2013 ) 118 : 196205 fig . 
in questo caso meno grave del precedente in gura 4 , il miglioramento clinico stato ottenuto dopo soli 3 giorni di terapia medica intensiva e ventilazione in c - pap . considered a semiquantitative method for assessing evlw . 
 this is extremely important in the face of the possibility of monitoring heart - failure - related pulmonary interstitial uid during the hospital stay and in the follow - up of outpatients . 
apart from the relative complexity of each method , b - lines can be objectively measured , thus allowing accurate quantication or semiquantication of evlw , monitoring of pulmonary interstitial uid and even indicating prognosis [ 3743 ]  . 
rather , these artefacts are signs of interstitial uid with thickened interlobular septa , which are not only linked to a cardiac disease but also to the pulmonary condition in cases of lesion oedema and inammatory processes due to acute and chronic diseases , as happens in acute respiratory distress syndrome ( ards ) , infections and brosis . 
even if some authors have demonstrated signicant differences in distribution and features of watery cardiogenic b - lines radiol med ( 2013 ) 118 : 196205 from lesion b - lines , i.e. 
rather , b - lines identify a syndrome , namely , the sonographic interstitial syndrome , which can be caused by different pathogenic mechanisms , not only hydrostatic , but also due to inammation and altered vascular permeability . 
however , despite this lack of specicity , the value of lung us for b - lines in the emergency setting or in selected cardiac patients has been well proven . 
the possibility of ruling out or ruling in some diseases by simply detecting or excluding a sonographic interstitial pattern , thus greatly reducing the diagnostic alternatives , has many useful consequences in the emergency setting . 
moreover , the value of lung us can be dramatically improved when it is combined with other diagnostic tools , both clinical and instrumental . another limitation of lung us could be interreader variability in assessing sonographic images , especially when they refer to artefact analysis . 
application of standardised diagnostic rules dening features of the b - line , a positive scan and a positive examination will help the process and make the technique highly reproducible . 
accurate diagnosis and follow - up of pulmonary interstitial uid in heart failure is important in many scenarios : ( 1 ) in the emergency setting , for the differential diagnosis of acute dyspnoea ; ( 2 ) in inpatient management , to titrate therapy and decide timing of discharge ; ( 3 ) in outpatients , to prevent the impending decompensation and avoid hospitalisation . 
lanzara , second university of naples , piazza miraglia 5 , 80131 naples , italy 2department of orthodontics , faculty of medicine and surgery , second university of naples , via de crecchio 6 , 80131 naples , italy 3human anatomy unit , department of public , clinical and preventive medicine , second university of naples , via armanni 5 , 80138 naples , italy correspondence to : f . 
iaselli , corso trieste 273 , 81100 caserta , italy , tel . : + 39 - 333 - 8411634 , e - mail : francescoiaselli@hotmail.it received : 29 july 2011 / accepted : 12 september 2011 / published online : 14 may 2012 springer - verlag 2012 abstract the aim of our study was to dene the changes in morphovolumetric features of neurocranium , basicranium and splanchnocranium in the population of campania , southern italy , over the last 2 , 700 years . 
this was a very intense period for this region from both historical and evolutionary perspectives and was marked by the succession of colonisations , dominations and invasions by several european and non - european peoples , events that profoundly inuenced the original genetic heritage , which subsequently became more complex . 
unlike most previous authors , we based our craniometric comparative analysis on multidetector computed tomography ( mdct ) studies of contemporary and ancient series dating to between the seventh and fth centuries b.c. 
while highlighting a remarkable stability of 22 / 32 of the indices considered , as an effect of the role of the genetic heritage in preserving morphovolumetric features in a given population , statistical analysis showed some interesting results : the main changes concerned the splanchnocranium and the occlusion , indicating a higher sensitivity of these districts to environmental factors , mainly related to diet . 
in particular , the riassunto scopo del nostro studio stato quello di denire le variazioni occorse a carico delle caratteristiche morfovolumetriche del neurocranio , del basicranio e dello splancnocranio nella popolazione della campania , italia meridionale , negli ultimi 2700 anni , periodo straordinariamente intenso dal punto di vista storico ed evolutivo per questa regione , caratterizzato dalla successione di colonizzazioni , dominazioni ed invasioni da parte di diverse popolazioni europee e non - europee , eventi che hanno profondamente inuenzato e condizionato loriginale patrimonio genetico , divenuto pi complesso . 
 a differenza della maggior parte degli autori che ci hanno preceduto , abbiamo basato la nostra analisi craniometrica che vede il confronto tra una serie contemporanea ed una antica , risalente al vii - v secolo prima di cristo e composta di crani ritrovati nelle antiche necropoli etrusche di pompei e pontecagnano sulla tomograa computerizzata multidetettore , estremamente afdabile nellidenticazione di punti craniometrici e nella misurazione di indici lineari ed angolari grazie allimpiego delle ricostruzioni multiplanari e tridimensionali . 
i risultati statistici del nostro lavoro , pur evidenziando una sostanziale stabilit di ben ventidue dei trentadue indici considerati , effetto del ruolo delleredit genetica nella conservazione di determinate caratteristiche morfo - volumetriche , hanno mostrato alcuni risultati interessanti : le principali modicazioni hanno interessato radiol med ( 2013 ) 118 : 276290 neurocranium increased in overall capacity in response to the growing brain and changed shape with a progressive shift to a dolichocranic , attened frontal pattern ; the basicranium shape was preserved , as indicated by the stability of the cranial base ( nsba ) angle over time . 
the splanchnocranium , on the contrary , has undergone a dramatic involution , even conditioning gnathic structures with changes in palatal shape ( more acute ) and in the relationship between the jaws on the sagittal plane , resulting in increased prevalence of angles class i and iii malocclusions . 
 keywords human evolution craniometry neurocranium splanchnocranium occlusion computed tomography lo splancnocranio e lassetto gnatico , indicando una maggiore sensibilit di questi distretti allinuenza di fattori ambientali , in primo luogo correlati alla dieta ; il complesso neurobasicranico , invece , ha mantenuto le sue caratteristiche morfo - volumetriche straordinariamente intatte . 
il neurocranio , in particolare , ha aumentato la sua capacit complessiva in risposta alla crescita del cervello e ha modicato la sua forma con un progressivo spostamento al pattern dolicocranico , con riduzione della convessit esterna dellosso frontale ; il basicranio ha mantenuto la sua forma nel tempo , come indicato dalla stabilit dellangolo nasion ( n ) - sella turcica ( s ) - basion ( ba )  . 
lo splancnocranio , al contrario , ha subito una drammatica involuzione , che ha coinvolto pure le strutture coinvolte nella masticazione , con variazioni della forma del palato , diventata pi acuta , e del rapporto delle due ossa mascellari sul piano sagittale , con conseguente incremento del rischio di sviluppare malocclusioni di classe iii secondo angle . 
 parole chiave evoluzione umana craniometria neurocranio splancnocranio assetto gnatico tomograa computerizzata introduction introduzione the museum of human anatomy at the second university of naples , one of the worlds oldest medical schools , houses unique collections of anatomical specimens that in terms of number , variety of preparation techniques and storage conditions represent a heritage of incomparable historical , scientic and teaching value . 
these collections include a series of ancient skulls found in the ancient necropoles of pompeii and pontecagnano ( campania , southern italy ) dating back to the etruscan civilisation , between the seventh and fth centuries b.c. 
our aims were to evaluate changes in craniofacial features over 2 , 700 years and to determine the accuracy and the potential of multidetector computed tomography ( mdct ) compared with those of conventional cephalometry for craniometric studies . 
 il museo di anatomia umana della seconda universit degli studi di napoli , una delle pi antiche scuole di medicina nel mondo , ospita collezioni uniche di pezzi anatomici che , per quantit , variet di tecniche di preparazione e condizioni di conservazione , rappresentano un patrimonio di valore storico , scientico e didattico senza pari . 
abbiamo effettuato unanalisi craniometrica comparativa mediante tomograa computerizzata ( tc ) tra questa serie antica ed una serie moderna di crani appartenenti agli attuali abitanti della campania ; nostri scopi sono stati la valutazione delle variazioni avvenute nelle caratteristiche craniofacciali negli ultimo 2700 anni e la denizione dellaccuratezza e delle potenzialit della tc multidetettore ( tcmd ) in confronto a quelle della cefalometrica convenzionale impiegata nei precedenti studi . 
1 la collezione di crani antichi del museo di anatomia umana della seconda universit degli studi di napoli . the biorbital distance and the bizygomatic breadth ; in three skulls it was not possible to evaluate the prosthion ( pr ) , the posterior nasal spine ( pns ) and the upper intermolar distance ( uid ) because of the extensively damaged upper dental arch ; in one skull the less - than - ideal state of preservation of the parietal and temporal bones prevented measurement of the biasterionic distance ; all skulls lacked the jaw . 
it was therefore necessary to choose completely original craniometric references ( landmarks and , above all , linear and angular indices ) , to dene splanchnocrania morphovolumetric features , unlike the case with the choice of references for the neurobasicranial complex . to limit the bias common to all comparative anthropometric studies related to a degree of genetic contamination that inevitably occurs over time in relation to biological , historical and social phenomena , the modern skulls were from the same geographic area as the ancient ones . 
in fact , 40 adults ( 20 men , 20 women , aged between 19 and 52 years , mean 39 years ) were randomly selected from 300 patients who underwent head ct examination from november 2009 to december 2010 at the department of diagnostic imaging of the second university of naples and born between the provinces of naples and salerno from families rooted in this territory for at least three generations . 
patients with bony or dental diseases , craniofacial bone deformities , severe dentoskeletal malocclusions and / or previously treated with orthodontic and / or maxillofacial surgery were excluded from our study . 
ci nonostante , in sette crani non stato possibile misurare n la distanza biorbitaria n lampiezza bizigomatica , in tre crani non stato possibile valutare lindice prosthion ( pr ) , la spina nasale posteriore ( snp ) e la distanza intermolare superiore a causa dellesteso danno dellarcata dentaria superiore , in un cranio il cattivo grado di conservazione delle ossa parietali e temporali non ha consentito la misurazione della distanza biasterionica . 
inne , in tutti i crani antichi mancava la mandibola : la conseguenza per noi stata , al momento di denire le caratteristiche morfo - volumetriche dello splancnocranio , la necessit di scegliere riferimenti craniometrici del tutto originali ( punti e , soprattutto , indici lineari ed angolari ) , a differenza di quanto accaduto nella scelta dei riferimenti per il complesso neurobasicranio . al ne di limitare il bias comune a tutti gli studi antropometrici comparativi correlato ad un certo grado di contaminazione genetica che inevitabilmente si verica nel tempo in relazione al vericarsi di fenomeni biologici , sociali e storici , i crani moderni sono stati selezionati dalla stessa area geograca degli antichi : infatti , a partire dal totale di trecento pazienti che si sono sottoposti a esame tcmd da novembre del 2009 a dicembre del 2010 presso il dipartimento di diagnostica per immagini della seconda universit degli studi di napoli , sono stati selezionati radiol med ( 2013 ) 118 : 276290 fig . 
image acquisition was performed with a volumetric technique ( slice thickness , 1 mm ; reconstruction interval , 0.5 mm ; pitch , 1 ; kvp , 120 ; mas , 100 ; scan time , 0.5 s ; matrix , 512512 )  . 
 ( for further information on craniometric points refer to the common texts of human anatomy . ) ] ; 28 linear indices and four angular indices ( table 1 )  . for both the ancient and the modern series , the location of craniometric landmarks and the measurement of linear casualmente solo quaranta soggetti adulti ( 20 maschi , 20 femmine , con et compresa tra 19 e 52 anni , con et media di 39 anni ) nati tra le province di napoli e salerno e appartenenti a famiglie stabili sul territorio almeno nelle ultime tre generazioni . 
i pazienti con patologie ossee o dentarie , con deformit dello scheletro craniofacciale , severe malocclusioni e / o precedentemente sottoposti ad interventi di chirurgia ortodontica e / o maxillo - facciale , sono stati esclusi dal nostro studio . 
ognuno di essi veniva posizionato su di un piano rigido allinterno di un apparecchio tc a 4 detettori ( aquilion , toshiba , tokyo , giappone ) e centrato con il fascio di luce verticale corrispondente alla linea mediana e con il fascio di luce orizzontale corrispondente ad una linea immaginaria che univa i due porion ( linea biporionica )  . 
lacquisizione dellimmagine era acquisita con tecnica volumetrica ( spessore di strato : 1 mm ; intervallo di ricostruzione : 0 , 5 mm ; pitch : 1 ; kvp : 120 ; mas : 100 ; tempo di scansione : 0 , 5 secondi ; matrice : 512512 )  . 
 280 radiol med ( 2013 ) 118 : 276290 and angular indices were independently performed by two pairs of observers , each including a radiologist and an odontologist with experience in the use of the postprocessing software . 
 using the dedicated software ( pasw statistics 18 , chicago , il , usa , available online at the website com / statistics / ) , a comparative statistical analysis was performed between values obtained in the two series . 
for each index we calculated mean , standard deviation ( sd ) , standard error ( se ) and t value ( data from the latter two measures are not shown )  . 
there was also an increase in the sella turcica nasion frontal ( s - n - f ) angle , reecting the degree of prominence and development of the logo e da un odontostomatologo esperti nellutilizzo del software di post - processing vital , vitrea . 
per ciascun indice abbiamo calcolato la media , la deviazione standard , lerrore standard ed il valore del test t di student ( questi ultimi due indici non compaiono nella tabella dei risultati )  . 
solo i risultati probabilmente signicativi sono stati discussi e vericati con una valutazione combinata del parametro o dei parametri incerti con indici correlati allo stesso distretto anatomico e caratterizzati da un valore biologico simile . 282 radiol med ( 2013 ) 118 : 276290 frontal bone , in the transition from the ancient to the contemporary series . 
sempre nel passaggio dalla serie antica alla contemporanea , si anche vericato un aumento dellangolo s - n - f , espressione del grado di prominentable 2 results of the craniometric comparative study . 
given , therefore , the prevalence of reduced transverse vs anteroposterior diameter in the time interval analysed , we can assume a change in the shape of the palate and thus of the upper dental arch , which , besides the reduced size , has taken on a more acute shape . discussion most craniometric comparative analyses to date are from conventional cephalometry , a two - dimensional representation of a three - dimensional object , in which accuracy is limited by the so - called projection error and identication error [ 3 , 4 ]  . 
these limits , along with growing evidence regarding the accuracy of volumetric ct in the craniometric eld , led us to employ this latter approach to our study [ 5 za e di sviluppo dellosso frontale . 
la variazione pi signicativa a carico nellambito dello splancnocranio stata la riduzione dellangolo s - n - sna ( p < 0 , 001 , nel passaggio dalla serie antica m : 84 , 9 , s : 2 , 5 alla contemporanea m : 81 , 2 , s : 2 , 9 )  . 
la valutazione comparativa dei diametri trasverso e longitudinale del palato ( agevolmente eseguibile mediante limpiego di ricostruzioni tridimensionali , figura 4 , e multiplanari tra le due serie ha messo in evidenza una signicativa , p < 0 , 05 , con m1 : 52 , 7 mm e m2 : 49 , 5 mm , riduzione dellindice pr - snp , espressione della lunghezza del palato , ed una signicativa , p < 0 , 01 , con m1 : 45 , 9 mm e m2 : 43 , 2 mm , con bassi valori di deviazione standard ) riduzione della distanza intermolare superiore : considerata , inoltre , la pi importante involuzione volumetrica del diametro trasverso rispetto allantero - posteriore nellinter284 radiol med ( 2013 ) 118 : 276290 fig . 
for the same reason , there was an increase in the degree of external convexity of the occipital bone , a phenomenon widely described in the literature as occipital bunning . 
 vallo di tempo considerato , possiamo assumere che si sia vericata una variazione nella forma del palato , e quindi dellarcata dentaria superiore , che , oltre ad essersi ridotti di dimensioni , hanno assunto una forma pi acuta . discussione la maggior parte delle analisi craniometriche comparative ad oggi pubblicate si basano sulla cefalometria tradizionale , rappresentazione bidimensionale di un oggetto tridimensionale , la cui accuratezza limitata dai cosiddetti errore di proiezione ed errore di identicazione [ 3 , 4 ]  . 
questi limiti , unitamente alle crescenti evidenze riguardo laccuratezza della tcmd negli studi craniometrici , ci ha spinto ad utilizzare questo ultimo approccio nel nostro studio [ 514 ]  . 
the sella turcicanasionfrontal angle , reecting the degree of external convexity of the frontal bone ; its increase from a value of 83.8 in the old series to 88.4 in the modern series is one of the most signicant results of our work and falls within the age - old evolutionary process indicated by the term frontal attening , which started at an early stage of human evolution in response to the increase in volume of the frontal lobe . 
langolo s - n - f , espressione del grado di convessit esterna dellosso frontale : laumento del suo valore da 83 , 8 nella serie antica a 88 , 4 nella moderna , uno dei risultati pi signicativi nel nostro lavoro e rientra nel lungo e antico processo evolutivo indicato con il termine di frontal attening dagli autori anglosassoni , iniziato in uno stadio iniziale dellevoluzione umana in risposta alla crescita volumetrica del lobo frontale . 
the close dimensional relationship between the anterior arm of the basicranium dabilit di houston hanno indicato unelevata correlazione tra le variabili misurate , con valori compresi tra 0 , 98 e 0 , 83 . nel nostro studio abbiamo riscontrato un incremento dei tre diametri massimi del cranio , espressione di un aumento della capacit cranica in toto nella serie contemporanea rispetto allantica . 
il braccio anteriore , n - s , corrisponde al planum sphenoideum , il posteriore , s - ba , alla supercie intracranica del clivus . ( n - s , decreased in the transition from the ancient to the contemporary series ) and the maxilla , already described in previous studies , was an additional factor responsible for the back displacement of the maxilla in the sagittal plane , demonstrating the interrelationships between the different subunits of the skull . due to the lack of the jaw in all ancient skulls , however , we could not conrm the widely described correlation between the size of the s - ba and the mandible and the consequent substantial stability of the position of the latter in the sagittal plane [ 27 ]  . 
however , on the basis of previous reports ( correlation in the sense of stability ) and the lack of change in the position of the articular point ( corresponding to the glenoid cavity of the temporal bone , which accommodates the mandibular condyles , thus closely anatomically related to the basion ) in our study , as documented by the substantial stability of its distance from the frontomaxillonasal suture [ 2830 ] , we can assume that no signicant mandibular morphovolumetric changes occurred and that this bone maintained its sagittal position almost unchanged . 
 with these assumptions , we can assume the following variations to occlusion in our population : the declining incidence of molar ratio of angles class i ( which continues today to be the dominant class in europe ) , and a signicant increase in the incidence of the angles class iii . 
7 the s - n - ans angle : this angular index reects the degree of maxillary prognathism : its decrease from a value of 84.9 in the old series to 88.4 in the modern series is one of the most signicant results of our work . 
7 langolo s - n - sna.questindice angolare espressione del grado di prognatismo del mascellare superiore : il suo decremento dal valore di 84 , 9 nella serie antica a quello di 88 , 4 nella moderna uno dei pi signicativi risultati nel nostro studio . 
la stretta correlazione dimensionale tra il braccio anteriore della base cranica ( n - s , ridottosi nel passaggio dalla serie antica alla contemporanea ) ed il mascellare superiore , gi descritta in precedenti lavori [ 10 , 19 , 20 ] , stato un ulteriore fattore coinvolto nellarretramento del mascellare superiore sul piano sagittale , a dimostrazione delle relazioni radiol med ( 2013 ) 118 : 276290 in response to ever - increasing allergens and environmental pollutants , are associated with a greater risk in the contemporary population of developing malocclusion of angles class i [ 3133 ]  . 
 in the modern series we also found an increase in facial height ( which must be seen in the millennial transition from the brachyfacial to the dolichofacial pattern , already evidenced in other european populations [ 34 , 35 ] ) and in interorbital distance ( which , although not signicant , is part of the long evolutionary pathway from primates to humans , characterised by the progressive increase in the distance between two maxillofrontal structures )  . 
afk is formed between the palatal plane and the posterior arm of the skull base and reects anatomically the degree of inclination of the oor of the nose and of the hard palate , so therefore of the upper airways and digestive tract [ 3638 ]  . 
moreover , the afk being an index of the relationship between the heights of the anterior and posterior half of the face , we can assume , even not having mandibles in the ancient series , that the ratio between the heights of the two halves of the face ( anterior and posterior ) is kept constant , although probably with varied distances , mainly because of the involution of the lower third of the face ( decreased height of the alveolar ridges consequent to the decreased masticatory load )  . conclusions twenty - two of thirty - two linear and angular indices considered in this study showed no signicant changes . 
this result assumes even more importance when one considers the role of the cranial base in the harmonious growth of the neurocranium , basicranium and splanchnocraniuin addition to this nding , our study also revealed the stability of facial morphovolumetric features , with the physiognomic characteristics of the population remaining remarkably similar over the considered time , despite the intense phenomena of genetic contamination . 
despite this , it is important to note the increase in prevalence of the dolichofacial pattern , as seen by the gradual decrease of facial depth and , above all , by the increase in facial height . 
a causa della mancanza della mandibola in tutti i crani appartenenti alla serie antica , tuttavia , non abbiamo potuto confermare la correlazione ampiamente descritta tra le dimensioni del braccio posteriore della base cranica ( s - ba ) e la mandibola e la conseguente sostanziale stabilit della posizione di questultima nel piano sagittale [ 27 ]  . 
tuttavia , sulla scorta dei risultati ottenuti da diversi autori nel passato [ 2830 ] ( correlazione nel senso della stabilit ) e dellassenza di variazioni nella posizione del punto craniometrico articolare ( corrispondente alla cavit glenoidea dellosso temporale che accoglie il condilo mandibolare e strettamente correlato dal punto di vista anatomico al basion ) nel nostro studio , come dimostrato dalla sostanziale stabilit della sua distanza dalla sutura fronto - maxillo - nasale [ 2830 ] , possiamo ipotizzare che non si siano vericate signicative variazioni a carico delle caratteristiche morfo - volumetriche della mandibola e che essa abbia mantenuto pressoch invariata la propria posizione nel piano sagittale nella nestra di tempo considerata . 
 con questi presupposti , possiamo assumere che si siano vericate le seguenti variazioni dellassetto gnatico nella popolazione da noi considerata : una ridotta prevalenza del rapporto molare di classe i secondo angle ( che continua tuttavia a rappresentare il rapporto dominante in europa ) ed un incremento signicativo nellincidenza del rapporto molare di classe iii secondo angle . 
queste variazioni , causate dalla riduzione dei carichi masticatori sul mascellare superiore e sullaumentata incidenza di respirazione orale in risposta allincremento degli allergeni e degli agenti inquinanti nellambiente , sono associate con un rischio maggiore nella popolazione contemporanea di sviluppare malocclusioni di i classe secondo angle [ 3133 ]  . 
 nella serie moderna abbiamo anche riscontrato un incremento in altezza del volto ( inquadrabile nella millenaria transizione dal pattern brachifacciale al dolicofacciale , gi intrapresa da altre popolazioni europee ) [ 34 , 35 ] e della distanza interorbitaria ( che , sebbene non signicativa , parte del lungo percorso evolutivo dai primati agli uomini , caratterizzato dal progressivo aumento della distanza tra i due maxillo - frontali )  . 
lacf formato dal piano palatale e dal braccio posteriore della base cranica , riettendo il grado di inclinazione del pavimento della cavit nasale e del palato duro , quindi delle alte vie respiratorie e digestive [ 3638 ]  . 
 inoltre , essendo lacf un indice del rapporto esistente tra laltezza della met anteriore e posteriore del volto , possia288 radiol med ( 2013 ) 118 : 276290 mo ipotizzate , anche senza avere a disposizione le mandibole nella serie antica , che il rapporto tra queste due met del volto ( anteriore e posteriore ) si sia mantenuto costante , sebbene probabilmente con distanze variate , principalmente a causa dellinvoluzione del terzo inferiore del volto ( riduzione in altezza delle creste alveolari conseguenti alla riduzione del carico masticatorio )  . conclusioni ventidue dei trentadue indici lineari ed angolari considerati nel nostro studio non hanno mostrato signicative variazioni . 
le principali variazioni nel nostro studio hanno interessato gli indici riferiti alle strutture gnatiche ed allo splancnocranio pi in generale , pi suscettibili alle inuenza ambientali rispetto al complesso neurobasicranico . 
il risultato pi signicativo stata la stabilit del valore dellangolo della base cranica , gi evidenziata da autori precedenti [ 19 , 20 ] ; questo risultato assume ancor pi importanza se si considera il ruolo della base cranica nella crescita proporzionata del neurocranio , del basicranio e dello splancnocranio . 
oltre a questo reperto , il nostro studio ha anche rivelato la stabilit delle caratteristiche morfovolumetriche dello scheletro facciale : la sionomia della popolazione , quindi , rimasta incredibilmente costante nel periodo considerato a dispetto degli intensi fenomeni di contaminazione genetica ; in ogni caso , un riscontro che deve essere sottolineato lincremento della prevalenza del pattern dolicofacciale , come dimostrato dalla graduale riduzione della profondit del volto e , soprattutto , dallincremento della sua altezza . 
 nellacquisizione di tutti questi dati , la tcmd ha giocato un ruolo chiave , consentendoci di identicare con alto grado di dettaglio i riferimenti anatomici predeniti in tutti i crani , con un tasso di variabilit interosservatore sostanzialmente trascurabile se confrontato con quello riscontrato in precedenti lavori basati sulla tecnica convenzionale . 
la tcmd ci ha anche consentito di effettuare accurate , agevoli e , soprattutto , riproducibili misurazioni lineari ed angolari , eliminando cos i ben noti limiti della cefalometria convenzionale , correlati agli errori di proiezione e di identicazione . 
 non abbiamo riscontrato sue signicative variazioni nellintervallo di tempo considerato , a conferma del mantenimento di una relazione costante tra le regioni anteriore ( verde ) e posteriore del volto ( blu )  . in the acquisition of all of these data , mdct played a key role , allowing us to identify with a high degree of detail the default craniometric references in all samples , with a substantially negligible rate of interobserver variability compared to that found in previous studies based on the conventional technique . 
ct also allowed us to perform accurate , reliable and , above all , reproducible linear and angular measurements , so eliminating the well - known limits of conventional cephalometry , which are related to projection and identication errors . 
filippi1 , 2 1neuroimaging research unit , institute of experimental neurology , division of neuroscience , san raffaele scientic institute , vita - salute san raffaele university , via olgettina 60 , 20132 milan , italy 2department of neurology , san raffaele scientic institute , vita - salute san raffaele university , via olgettina 60 , 20132 milan , italy 3neuroradiology unit , san raffaele scientic institute , vita - salute san raffaele university , via olgettina 60 , 20132 milan , italy correspondence to : m . 
for this reason , it has become an integral part of the diagnostic workup of patients with clinically isolated syndromes who are at risk of developing denite ms , and it is always recommended in patients with denite ms to conrm the diagnosis and monitor the disease course . 
crucial to the use of mr imaging for diagnostic purposes is the identication of lesion features in terms of site , shape and size that may be considered suggestive or typical for ms , and thus help in the differential diagnosis with other neurological diseases with similar clinical presentation to ms . 
this need has led to the publication of several guidelines for characterising ms lesions on both dualecho ( t2 and proton density ) and t1 - weighted sequences after administration of contrast material . 
currently , when making a clinical diagnosis and monitoring patients with suspected ms , neurologists and neuroradiologists make use of specic diagnostic criteria that have changed over the years and will probably continue to be updated . 
in patients with a denite diagnosis of ms , on the other hand , the main problem is to dene standard procedures for monitoring the course of riassunto la risonanza magnetica ( rm ) una metodica estremamente sensibile nel rilevare le alterazioni focali della sostanza bianca ( sb ) dei pazienti con sclerosi multipla ( sm )  . 
per questo motivo , parte integrante del processo diagnostico in pazienti con sindromi clinicamente isolate ( cis ) a rischio di evoluzione verso una forma denita di sm , ed sempre consigliata nei pazienti con sm conclamata per confermare la diagnosi e per monitorarne levoluzione . 
uno dei punti fondamentali per lutilizzo della rm a scopo diagnostico lidenticazione di caratteristiche di imaging delle lesioni , in termini di sede , forma , e dimensioni , che possano essere considerate suggestive o tipiche di sm , e contribuire cos al processo di diagnosi differenziale verso altre patologie neurologiche , che possono avere un esordio clinico simile a quello della sm . 
ci ha condotto alla pubblicazione di diverse linee - guida per la caratterizzazione delle lesioni della sm sia sulle sequenze pesate in doppio - eco ( t2 e densit protonica ) che su quelle pesate in t1 dopo somministrazione di mezzo di contrasto . 
attualmente , neurologi e neuroradiologi basano linquadramento clinico e il monitoraggio dei pazienti con un sospetto di sm su specici criteri diagnostici che si sono andati modicando nel tempo e che molto probabilmente continueranno ad essere aggiornati . 
quindi fondamentale che il radiologo acquisisca familiarit con tali criteri al ne di migliorare 252 radiol med ( 2013 ) 118 : 251264 the disease and response to pharmacological treatments . 
 even though no guidelines currently exist , it is possible to suggest some strategies to improve the assessment in this setting . keywords magnetic resonance imaging multiple sclerosis diagnosis monitoring la qualit della sua valutazione diagnostica . 
nei pazienti con una diagnosi certa di sm , il problema fondamentale invece quello di denire delle procedure standard per il monitoraggio del decorso della malattia e della risposta a trattamenti farmacologici . 
anche se in questo caso mancano linee - guida denite , possibile suggerire alcune strategie per migliorare le modalit di valutazione in questo ambito . parole chiave risonanza magnetica sclerosi multipla diagnosi monitoraggio introduction introduzione magnetic resonance imaging ( mri ) is a highly sensitive modality for detecting focal abnormalities of the white matter in patients with multiple sclerosis ( ms )  . 
for this reason , it has been incorporated into the diagnostic workup of patients with clinically isolated syndromes ( cis ) who are at risk of developing a denite form of ms , and it is always recommended in patients with denite ms to conrm the diagnosis and monitor the course of the disease . one of the main goals of diagnostic mri is to identify the imaging features in terms of lesion location , morphology and size that may be considered suggestive or typical of ms , thus contributing to the differential diagnosis with other neurological diseases with similar clinical presentation . 
this has led to the publication of several guidelines for characterising ms lesions on both dual - echo ( t2and proton densityweighted ) and contrast - enhanced t1 - weighted imaging . 
currently , when making a clinical diagnosis and monitoring patients with suspected ms , neurologists and neuroradiologists make use of specic diagnostic criteria that have changed over the years and will probably continue to be updated . 
 in patients with a denite diagnosis of ms , on the other hand , the main problem is to dene standard procedures for monitoring disease course and response to pharmacological treatments . 
even though no guidelines currently exist , it is possible to suggest some strategies to improve the assessment in this setting . la risonanza magnetica ( rm ) una metodica estremamente sensibile nel rilevare le alterazioni focali della sostanza bianca ( sb ) dei pazienti con sclerosi multipla ( sm )  . 
per questo motivo , parte integrante del processo diagnostico in pazienti con sindromi clinicamente isolate ( cis ) a rischio di evoluzione verso una forma denita di sm , ed sempre consigliata nei pazienti con sm conclamata per confermare la diagnosi e per monitorarne levoluzione . uno dei punti fondamentali per lutilizzo della rm a scopo diagnostico lidenticazione di caratteristiche di imaging delle lesioni , in termini di sede , forma , e dimensioni , che possano essere considerate suggestive o tipiche di sm , e contribuire cos al processo di diagnosi differenziale verso altre patologie neurologiche , che possono avere un esordio clinico simile a quello della sm . 
ci ha condotto alla pubblicazione di diverse linee - guida per la caratterizzazione delle lesioni della sm sia sulle sequenze pesate in doppioeco ( t2 e densit protonica ) che su quelle pesate in t1 dopo somministrazione di mezzo di contrasto . 
attualmente , neurologi e neuroradiologi basano linquadramento clinico e il monitoraggio dei pazienti con un sospetto di sm su specici criteri diagnostici che si sono andati modicando nel tempo e che molto probabilmente continueranno ad essere aggiornati . 
 nei pazienti con una diagnosi certa di sm , il problema fondamentale invece quello di denire delle procedure standard per il monitoraggio del decorso della malattia e della risposta a trattamenti farmacologici . 
ms typically starts with an acute attack , which is followed by a relapsingremitting phase ( rrms ) and subsequently by a progressive accumulation of disabilities [ secondary progressive ms ( spms ) ]  . 
a diagnosis of ms presupposes fullment of three requirements : demonstration of dis and dit of the pathological process , and ruling out of other conditions that may mimic ms . historically , the most important criteria accepted by the international scientic community were those developed by schumacher et al . 
 although they were developed before the spread of mri techniques , these criteria still constitute a reference tool for some basic denitions , such as the concepts of dis and dit of the pathological process and the characteristics of a relapse . 
 [ 4 ] performed a retrospective study in which the mri ndings of patients with denite ms were compared with those of control individuals with nonspecic white - matter lesions in order to identify the features that best discriminated between the two groups . 
fullment of patys criteria [ 3 ] requires the presence of at least four lesions at any location in the brain or three lesions of which one must be in a periventricular location . 
fazekass criteria require the presence of at least three lesions in the brain , two of which must have the following characteristics : one infratentorial lesion , and one periventricular lesion or one lesion with diameter > 6 m in 1997 , barkhof et al . 
 [ 5 ] conducted a prospective study on patients with cis in order to dene the mri features of initial disease that were capable of identifying patients centrale ( snc ) , caratterizzata dalla disseminazione spaziale e temporale del processo patologico , ossia dalla formazione di lesioni in sedi e in tempi diversi a livello dellencefalo , del nervo ottico e del midollo spinale . 
la diagnosi di sm prevede tre presupposti imprescindibili : la dimostrazione della disseminazione spaziale ( dis ) del processo patologico , la disseminazione temporale ( dit ) dello stesso e lesclusione di altre patologie eventualmente responsabili del quadro clinico . storicamente , i criteri pi importanti e accettati dalla comunit scientica internazionale sono stati quelli elaborati da schumacher et al . 
pur essendo stati elaborati in unepoca precedente allutilizzo su vasta scala delle tecniche di rm , sono tuttora un punto di riferimento per alcune denizioni fondamentali , quali il concetto di disseminazione spazio - temporale del processo patologico e la denizione delle caratteristiche di una ricaduta di malattia . 
 [ 3 ] , formulati in uno studio prospettico , allo scopo di individuare il valore predittivo dei reperti di rm per lo sviluppo di sm denita in pazienti con cis allesordio , e quelli di fazekas et al . 
 [ 4 ] , formulati sulla base di uno studio retrospettivo in pazienti con sm denita , i cui reperti rm vennero confrontati con quelli di controlli con lesioni aspeciche della sb , allo scopo di identicare le caratteristiche che meglio distinguevano i due gruppi . 
 [ 3 ] richiede la presenza di almeno 4 lesioni encefaliche ( in qualunque sede ) o , in alternativa , di 3 lesioni di cui almeno una abbia una localizzazione periventricolare . 
 [ 4 ] richiedono la presenza di 3 o pi lesioni encefaliche , con almeno due delle seguenti caratteristiche : una lesione sottotentoriale , una lesione periventricolare o una lesione con diametro maggiore di 6 m nel 1997 , barkhof et al . 
 [ 5 ] hanno condotto uno studio prospettico in pazienti con cis con lo scopo di denire le ca ratteristiche di rm dellencefalo allesordio che identicassero i pazienti a maggior rischio di sviluppare sm in un perio254 radiol med ( 2013 ) 118 : 251264 at increased risk of developing ms over a 3 - year period . 
 by using logistic regression analysis , the study devised a multiparameter model that included the following mri features : presence of at least one gadolinium - enhancing lesion , at least one subcortical lesion , at least one infratentorial lesion and three or more periventricular lesions . 
if postcontrast images are not available , the presence of one or more enhancing lesions may be replaced by the presence of one or more hyperintense lesions on t2 - weighted images . the introduction of immunomodulating drugs that are effective in the early stages of ms has emphasised the need for early diagnosis also in patients without a second clinical attack . 
given the availability , objectivity and sensitivity of mri in detecting spatial and temporal changes relating to the pathological process , this imaging modality has emerged as one of the main instruments for supporting and accelerating the diagnostic workup of patients with cis . 
insidious onset and progression of neurological disturbances without relapses or remissions , suggestive of ppms . the interpretation of mri ndings in terms of dis is based on the barkhof criteria [ 5 ]  . 
grazie ad unanalisi di regressione logistica , questo studio ha elaborato un modello multiparametrico che prevede le seguenti caratteristiche di rm : presenza di almeno una lesione captante il gadolinio ( gd ) , presenza di almeno una lesione sottocorticale , presenza di almeno una lesione sottotentoriale e presenza di 3 o pi lesioni periventricolari . 
 in assenza di immagini ottenute dopo somministrazione di gd , la presenza di una o pi lesioni captanti pu essere sostituita dalla presenza di 9 o pi lesioni iperintense in t2 . lintroduzione di farmaci immunomodulanti dotati di provata efcacia anche nelle fasi iniziali della sm ha aumentato la necessit di una diagnosi precoce di malattia anche nei pazienti senza un secondo episodio clinico conclamato . 
date le sue caratteristiche di diffusione , obiettivit e sensibilit nel rilevare le alterazioni nello spazio e nel tempo correlate al processo patologico , la rm emersa come uno degli strumenti principali per coadiuvare ed accelerare il processo diagnostico nei pazienti con cis . 
esordio subacuto e progressivo di disturbi neurologici , senza riacutizzazioni e remissioni , suggestivo di sm - pp . linterpretazione dei dati rm in termini di dis fondata sullapplicazione dei criteri di barkhof et al . 
linquadramento dei dati clinici , di laboratorio ( analisi del liquor con ricerca di bande oligoclonali ) e strumentali ( rm e potenziali evocati ) nalizzato alla dimostrazione della disseminazione spaziale e temporale delle lesioni . 
dis clinica : evidenza clinica obiettiva della presenza di due o pi lesioni del snc , sia nel contesto di uno stesso attacco sia in due attacchi tra loro distinti ; 2 . 
3 o pi lesioni periventricolari ; qualora siano disponibili reperti rm del midollo , una lesione midollare pu sostituire una lesione encefalica nel contesto della conta globale o in quella delle lesioni sottotentoriali ; radiol med ( 2013 ) 118 : 251264 c . 
combined dis : presence of at least two mri lesions plus cerebrospinal uid ( csf ) abnormalities consistent with demyelinating disease . dit may be demonstrated both clinically and through imaging in the following ways : 1 . 
one or more gadolinium - enhancing lesions at locations not compatible with the neurological disturbances of the original clinical event ( in the case of mri performed 3 months after the clinical event ) ; b . 
if criteria described in ( a ) are not satised , then one or more new t2 lesions or one or more gadoliniumenhancing lesion on a second mri scan obtained at least 3 months after the rst follow - up examination described in point ( a ) ; as mentioned , ppms differs strongly in clinical presentation from the cis forms . 
application of the mcdonald criteria to patients with progressive neurological syndromes addresses the need to establish an early and accurate diagnosis of ppms , in which the mri pattern is often characterised by few lesions and rare signs of disease activity over time . 
 in patients with insidious progression of neurological disturbances suggestive of ms , the diagnosis of ms according to the mcdonald criteria may be made in the presence of : 1 . 
demonstration of dit , as dened with mri criteria ( see above ) , or with clinical evidence of continued progression for at least 1 year . although the mcdonald criteria have the merit of having formally introduced mri into the diagnostic workup of patients with cis , these criteria are clearly not without limitations , one of which is the lack of a systematic consideration of mri ndings at the spinal cord level . 
dis combinata : presenza di almeno 2 lesioni rm e di alterazioni del liquor cefalorachidiano compatibili con malattia demielinizzante . la dit pu essere dimostrata sia sul piano clinico che su quello strumentale ( rm ) nei seguenti modi : 1 . 
presenza di una o pi lesioni captanti il gd in sede non congrua con i disturbi neurologici dellattacco desordio ( in caso di esame eseguito almeno 3 mesi dopo lepisodio di disfunzione neurologica ) ; b . 
in caso di assenza dei reperti descritti al punto 2a , presenza di una o pi lesioni nuove in t2 o una o pi lesioni captanti il gd su un ulteriore esame rm eseguito ad almeno 3 mesi di distanza dal primo esame di follow - up di cui al punto 2a . come accennato precedentemente , la sm - pp si differenzia nettamente rispetto alle forme cis per caratteristiche cliniche di esordio . 
lapplicazione dei criteri di mcdonald in pazienti con sindromi neurologiche progressive viene incontro alla necessit di giungere ad una diagnosi precoce ed accurata di sm - pp , che spesso presenta reperti di rm caratterizzati da poche lesioni e rara comparsa di segni di attivit nel tempo . 
in pazienti con esordio subdolo e progressivo di disturbi neurologici suggestivi di sm , la diagnosi di sm secondo i criteri di mcdonald pu essere fatta in presenza di : 1 . 
positivit dei potenziali evocati visivi ( pev ) associata alla presenza di 48 lesioni encefaliche alla rm o alla presenza di meno di 4 lesioni encefaliche e di una lesione midollare ; 3 . 
dimostrazione della dit , denita con i criteri di rm ( vedi sopra ) , oppure con levidenza clinica di progressione continua dei disturbi neurologici per almeno 1 anno . nonostante i criteri di mcdonald abbiano il merito principale di avere incluso formalmente la rm nel processo diagnostico dei pazienti con cis , tali criteri non sono , chiaramente , privi di limiti , tra cui la mancanza di una considerazione sistematica dei reperti rm del midollo . 
noto che la presenza di lesioni midollari , in generale , un reperto dotato di maggiore specicit patologica rispetto al riscontro di lesioni encefaliche , in quanto , a differenza di queste ultime , molto raro in corso di invecchiamento siologico . 
 256 radiol med ( 2013 ) 118 : 251264 that a nding of spinal cord lesions has higher pathological specicity compared with a nding of brain lesions , given that , unlike the latter , spinal cord lesions are very rarely seen in healthy ageing . 
at least three periventricular lesions . spinal cord lesions should have the typical features of those seen in ms ( little or no swelling of the cord , unequivocally hyperintense on t2 , at least 3 mm in size , less than two vertebral segments in length and occupying only part of the cord cross - section )  . 
a gadolinium - enhancing spinal cord lesion is considered equivalent to both an enhancing lesion and an infratentorial lesion ( thus satisfying two of the above - mentioned conditions )  . dit may be demonstrated both clinically and through imaging ( mri ) in the following manner : 1 . 
one gadolinium - enhancing lesion on mri performed at least 3 months after onset of the rst clinical attack , provided that the lesion is located at a site not involved in the rst attack ; b . 
one new t2 lesion on mri performed at least 30 days after onset of the clinical attack ( this criterion is valid for all mr examinations performed after the baseline reference scan )  . in patients with insidious progression of neurological disorders suggestive of ms , the diagnosis of ppms according to the 2005 criteria may be established in the presence 1 . 
positive csf test ( evidence of oligoclonal bands or increased immunoglobulin g ( igg ) index , or both )  . in base alla precedenti osservazioni , nel 2005 il processo diagnostico proposto dai criteri di mcdonald stato rivalutato . 
3 o pi lesioni periventricolari . le lesioni midollari devono avere le caratteristiche tipiche di quelle riscontrate usualmente nella sm ( modesto o assente rigonamento del midollo , inequivocabilmente iperintense in t2 , dimensione di almeno 3 mm , estensione per non pi di 2 mielomeri in lunghezza e interessamento di solo parte della sezione traversa del midollo )  . 
viene inoltre ribadito che una lesione midollare captante il gd pu contare sia come lesione captante che come lesione infratentoriale ( soddisfacendo pertanto 2 delle condizioni sopra menzionate )  . la dit pu essere dimostrata sia sul piano clinico che su quello strumentale ( rm ) nei seguenti modi : 1 . 
presenza di una nuova lesione in t2 rispetto ad un esame eseguito almeno 30 giorni dopo linsorgenza dellattacco clinico ( criterio valido per ogni esame successivo a quello basale di riferimento )  . in pazienti con esordio subdolo e progressivo di disturbi neurologici suggestivi di sm , la diagnosi di sm - pp secondo i criteri 2005 pu essere fatta in presenza di : 1 . 
esame liquor positivo ( evidenza di bande oligoclonali o aumento dellimmunoglobuline g ( igg ) index o entrambi )  . nel corso degli ultimi anni , diverse proposte sono state avanzate nel tentativo di semplicare i criteri diagnostici indicati e per renderli pi facilmente integrabili nellambito clinico . 
in caso di sindromi del tronco encefalo e midollari , vanno escluse dalla quanticazione le lesioni presenti in queste strutture ; radiol med ( 2013 ) 118 : 251264 in recent years , several proposals have been put forward in an attempt to simplify diagnostic criteria and make them easier to apply in a clinical setting . 
 it should be noted that , compared with previous criteria , swanton et al.s are easier to remember and apply in clinical practice , and they do not require the administration of contrast material . 
 [ 9 ] suggest that a single mri scan performed early ( within 3 months ) after onset of cis is highly specic in predicting the development of denite ms whenever both gadolinium - enhancing and - nonenhancing lesions are present , a circumstance that by itself appears to indicate dit without any need to seek conrmation by performing follow - up mri to demonstrate the development of new lesions . more recently , swantons and roviras criteria were incorporated into the magnims criteria ( european network for magnetic resonance research in ms ) with the aim of further simplifying the diagnostic criteria while maintaining the high level of specicity required for minimising false positive results [ 10 ]  . 
an mri scan performed at any time after symptom onset demonstrating dis and showing at least one asymptomatic gadolinium - enhancing and - nonenhancing lesion ( to be used as evidence of dit ) is sufcient to diagnose 2 . 
an abnormal mri scan at any time after clinical onset but not fullling the criteria for dis and dit requires follow - up mri . in detail , the following simplied criteria for mri demonstration of dis and dit are proposed : 2 . 
si deve tuttavia considerare che la somministrazione del mezzo di contrasto fornisce informazioni di fondamentale importanza per una corretta diagnosi differenziale nei pazienti che si presentano con una cis . i criteri proposti da rovira et al . 
 [ 9 ] hanno suggerito che una singola rm effettuata precocemente ( entro 3 mesi ) dallesordio di una cis altamente specica nel predire lo sviluppo di sm denita qualora siano presenti contemporaneamente sia lesioni captanti che non captanti il gd , circostanza che suggerirebbe gi una dit , senza la necessit di dover effettuare successive rm per la dimostrazione di nuove lesioni per confermarla . recentemente , i criteri di swanton e di rovira sono stati inclusi nei nuovi criteri elaborati dal gruppo delleuropean network for magnetic resonance research in multiple sclerosis ( magnims ) , con lobiettivo di semplicare ulteriormente i criteri diagnostici , mantenendo unalta specicit , essenziale per minimizzare i falsi positivi [ 10 ]  . 
una rm eseguita in qualsiasi momento rispetto allesordio della sintomatologia clinica che mostri dis e la coesistenza di almeno una lesione captante il mezzo di contrasto asintomatica , in aggiunta a lesioni non captanti ( da utilizzare come evidenza di dit ) sufciente per porre diagnosi di sm ; 2 . 
una rm eseguita in qualsiasi momento rispetto allesordio della sintomatologia clinica che mostri dis , ma in assenza di lesioni captanti il mezzo di contrasto , oppure con tutte le lesioni captanti il mezzo di contrasto contemporaneamente ( senza quindi evidenza di dit ) , richiede lesecuzione di una nuova rm per dimostrare la presenza di nuove lesioni in t2 o nuove lesioni captanti il mezzo di contrasto ; 3 . 
una rm alterata eseguita in qualsiasi momento rispetto allesordio della sintomatologia clinica ma che non soddis i requisiti di dis e dit richiede lesecuzione di un follow - up di rm . nel dettaglio , vengono proposti i seguenti criteri semplicati per la dimostrazione di dis e dit tramite la rm : 1 . 
pi di 1 lesione asintomatica sulle sequenze pesate in t2 in pi di 2 delle 4 localizzazioni considerate caratteristiche per sm : periventricolare , sottocorticale , infratentoriale e midollo spinale ; 258 radiol med ( 2013 ) 118 : 251264 1 . 
 the recent introduction of double inversion recovery sequences ( dir ) [ 11 ] has allowed in vivo visualisation of some of the cortical lesions ( cl ) seen in ms patients . 
 [ 12 ] evaluated the role of cl in patients with cis and led to the denition of the following criterion for demonstrating dis : presence of at least one cl , at least one infratentorial lesion , at least one spinal cord lesion or gadolinium - enhancing lesion . 
positivity of at least two of these three criteria had high specicity ( 93% ) while maintaining high sensitivity ( 77% ) and accuracy ( 86% ) in identifying patients at risk of developing clinically denite ms . 
 recently , the group of international experts who participated in drafting the rst diagnostic criteria carried out a further revision of mri criteria to address the critical aspects emerging from their application and to extend applicability to non - caucasian and paediatric populations . 
presenza di una nuova lesione su sequenze pesate in t2 e / o di una lesione captante rispetto ad un esame eseguito in precedenza , indipendentemente dal tempo di esecuzione di questo esame . 
 la recente introduzione delle sequenze double inversion recovery ( dir ) [ 11 ] ha permesso la visualizzazione , in vivo , di una parte delle lesioni corticali ( cl ) presenti nei pazienti con sm . 
 [ 12 ] ha valutato il ruolo delle cl nei pazienti con cis e ha portato alla denizione del seguente criterio per la dimostrazione di dis : presenza di almeno una cl , presenza di almeno una lesione infratentoriale , presenza di almeno una lesione midollare o una lesione captante il gd . 
la positivit di almeno due dei precedenti tre criteri ha mostrato unelevata specicit ( 93% ) , mantenendo una elevata sensibilit ( 77% ) e accuratezza ( 86% ) nellidenticare i soggetti a rischio di evoluzione a sm denita . 
 recentemente , il gruppo di esperti internazionali che aveva partecipato alla stesura dei primi criteri diagnostici della malattia ha formulato unulteriore revisione dei criteri di rm , tenendo in considerazione le criticit emerse dalla loro applicazione e cercando di estenderne lapplicabilit anche a popolazioni adulte di origine non - caucasica e in ambito pediatrico . 
i criteri proposti da questa nuova revisione per la dimostrazione di dis e dit nei pazienti con cis [ 13 ] sono sovrapponibili a quelli recentemente suggeriti dal gruppo magnims [ 10 ]  . 
vengono inoltre descritte le caratteristiche di imaging che dovrebbero essere riscontrate nei pazienti con sm pediatrica . questa revisione prende anche in considerazione la necessit di unattenta diagnosi differenziale con la neuromielite ottica ( nmo ) e lo spettro di disordini associati . 
performance of the mri criteria in patients with cis and clinical features considered atypical for ms and in patients with other multifocal white - matter lesions was not evaluated systematically . 
la performance dei criteri di rm nei pazienti con cis e caratteristiche cliniche considerate atipiche per sm e nei pazienti con altre patologie multifocali della sb del snc non stata valutata in maniera sistematica . 
studi futuri dovranno considerare se lutilizzo di magneti ad alto campo ( 3 , 0 tesla o maggiori ) e lacquisizione di sequenze di rm di introduzione pi recente ( ad esempio , dir ) inuenzino la diagnosi di sm . 
 practical recommendations for using mri for diagnosing ms in patients with cis raccomandazioni pratiche per lutilizzo della rm per la diagnosi di sm in pazienti cis on the basis of our previous discussion , the report of an mri examination of a patient with cis suggestive of ms in base a quanto precedentemente discusso , la refertazione di un esame di rm in un paziente che si presenta con una 260 radiol med ( 2013 ) 118 : 251264 fig . 
1a - c axial uid - attenuated inversion recovery images of the brain ( a , b ) and t2 - weighted images of the cervical spinal cord ( c ) of a patient with a clinically isolated syndrome of the central nervous system at onset . 
lesions can be seen in at least two of four locations typical for multiple sclerosis : ( 1 ) periventricular ( circles ) , ( 2 ) subcortical ( asterisks ) , ( 3 ) infratentorial ( arrowheads ) , ( 4 ) spinal cord ( arrows )  . 
1a - c immagini assiali flair dellencefalo ( a , b ) e pesate in t2 del midollo cervicale ( c ) di un paziente con una sindrome clinicamente isolata del sistema nervoso centrale allesordio . 
sono visibili pi lesioni in almeno 2 delle 4 aree tipicamente interessate dalla sclerosi multipla : ( 1 ) periventricolare ( cerchi ) ; ( 2 ) sottocorticale ( asterischi ) ; ( 3 ) infratentoriale ( punte di freccia ) ; ( 4 ) midollo spinale ( frecce )  . 
2a - c axial t2 - weighted ( a ) , uid - attenuated inversion recovery ( b ) and contrast - enhanced t1 - weighted images ( c ) of the brain in a patient with a clinically isolated syndrome of central nervous system at onset . 
lesions can be seen in at least two of four locations typical for multiple sclerosis : ( 1 ) periventricular ( circles ) , ( 2 ) subcortical ( asterisks )  . 
2a - c immagini assiali pesate in t2 ( a ) , flair ( b ) e t1 dopo somministrazione di mezzo di contrasto ( c ) dellencefalo di un paziente con una sindrome clinicamente isolata del sistema nervoso centrale allesordio . 
sulla immagine pesata in t1 dopo la somministrazione di mezzo di contrasto si pu inoltre osservare la contemporanea presenza di lesioni captanti ( freccia ) e non ( punta di freccia ) il mezzo di contrasto . 
in base alla revisione del 2010 dei criteri di mcdonald , soddisfatto il criterio anche per la disseminazione temporale della malattia . radiol med ( 2013 ) 118 : 251264 should contemplate the following information : 1 . 
denition of dis through detection of hyperintense lesions on axial t2 - weighted [ or uid - attenuated inversion recovery ( flair ) ] sequences with reference to each of the typical locations of disease ( periventricular , subcortical , infratentorial , spinal cord )  . 
in addition , although not absolutely necessary , it would be useful to indicate possible fullment of the dis and dit criteria according to the guidelines presented [ 13 ] and the need to perform a follow - up examination in the event that a single mri scan shows insufcient evidence for a diagnosis of ms . cis suggestiva di sm dovrebbe contemplare le seguenti informazioni : 1 . 
denizione della presenza di dis tramite la dimostrazione di lesioni iperintense su un esame assiale pesato in t2 ( o uid - attenuated inversion recovery , flair ) con riferimento a ciascuna delle aree privilegiate dalla malattia ( periventricolari , sottocorticali , infratentoriali e midollari )  . 
come dato aggiuntivo , ma non assolutamente necessario , utile indicare leventuale soddisfazione dei criteri di dis e dit secondo i criteri presentati [ 13 ] e la necessit di eseguire un esame di controllo in caso un singolo esame di rm non mostri evidenze sufcienti per porre diagnosi di sm . recommendation for using mri in patients with denite ms raccomandazioni per lutilizzo della rm in pazienti con sm denita mri has become an extremely useful instrument for monitoring patients with a denite diagnosis of ms . 
this aspect is becoming increasingly important , as more and more treatments are being approved for ms . mri for monitoring disease course in patients with denite ms la rm diventata uno strumento estremamente utile per il monitoraggio dei pazienti con una diagnosi denita di sm . 
 nei pazienti con sm - rr o secondariamente progressiva , infatti , lattivit di malattia rilevata con la rm 510 volte superiore a quella evidenziabile clinicamente in termini di ricadute . 
 questo aspetto sta diventando sempre pi rilevante visto che i trattamenti autorizzati per la sm sono sempre pi numerosi e che lo saranno ancora di pi nei prossimi anni . rm per il monitoraggio del decorso della malattia nei pazienti con sm denita even though no standardised guidelines exist , the recommended approach is as follows : 1 . 
 262 radiol med ( 2013 ) 118 : 251264 mri for monitoring response to treatment rm per il monitoraggio della risposta terapeutica even in this setting , no internationally accepted guidelines exist . 
however , patients about to start a new treatment or to change treatment should undergo a brain mri scan ( t2 / flair sequences and contrast - enhanced t1 sequences )  . 
 this mri scan should then be repeated after 6 months and 1 year to assess the effectiveness of the new treatment regimen . clearly , one of the critical aspects in this context is the denition of cutoff points for assessing the patients response to a given drug ( responder / nonresponder )  . 
 [ 14 ] studied 222 patients affected by rrms after the rst year of treatment with interferon ( ifn ) - 1b and assessed the risk of new clinical relapses and increase in disability over the following 1236 months . 
presence of two or more active lesions ( dened as new or enlarging t2 lesions or contrast - enhancing lesions ) at mr performed at 12 months ( mri + )  . 
tuttavia , in pazienti che stiano per iniziare un nuovo trattamento o nei quali prevista una modica del trattamento in corso dovrebbe essere eseguita una rm dellencefalo ( sequenze t2 / flair e sequenze pesate in t1 dopo la somministrazione di mezzo di contrasto )  . 
tale rm dovrebbe essere poi ripetuta a distanza di 6 mesi ed 1 anno per valutare lefcacia del nuovo regime terapeutico . chiaramente , in questo ambito , uno degli aspetti critici denire dei cut - off rispetto ai quali stimare la risposta di un dato paziente ad un determinato farmaco ( responder / nonresponder )  . 
 [ 14 ] hanno studiato 222 pazienti affetti da sm - rr dopo il primo anno di terapia con interferone ( ifn ) - 1b e hanno valutato il rischio di nuove ricadute cliniche di malattia e di aumento della disabilit nellarco dei 1236 mesi successivi . 
la presenza di pi di 2 lesioni attive ( denite come lesioni nuove o aumentate di volume in t2 oppure captanti il mezzo di contrasto ) alla rm eseguita dopo un anno ( mri + ) : in presenza di positivit di tutte e tre le variabili ( r + / p + / mri + ) , il rischio di ricadute di 9 , 8 volte superiore e il rischio di progressione di 6 , 5 volte superiore nei successivi 1236 mesi rispetto ai pazienti che non presentano questi indici ; in presenza di due variabili positive ( r + / p - / mri + ) , il rischio di ricadute di 8 , 3 volte superiore e il rischio di progressione di 4 , 4 volte superiore nei successivi 1236 mesi ; in presenza di due variabili positive ( r - / p + / mri + ) , il rischio di ricadute di 3 , 3 volte superiore e il rischio di progressione di 7 , 1 volte superiore nei successivi 1236 mesi ; in presenza di una sola tra queste variabili ( r - / p - / mri + ) , il rischio di ricadute compreso tra 1 , 8 e 1 , 1 e il rischio di progressione compreso tra 0 , 3 e 3 , 9 nei successivi 1236 mesi ; in assenza di mri + : nessun rischio signicativo di ricadute o progressione . 
 in base ai risultati sopra descritti , stato recentemente proposto [ 15 ] un algoritmo decisionale per la valutazione della risposta alla terapia immunomodulante in pazienti affetti da sm - rr . 
patients without active disease on mri ( two or fewer active lesions over 612 months ) should undergo clinical and imaging assessment after 6 months / 1 year , the results of which will guide management decisions . 
 when monitoring a patient with a denite diagnosis of ms and who is undergoing treatment , the report of an mri examination should therefore incorporate a comparison with a previous examination and include the following information : 1 . 
nei pazienti senza attivit rm ( due o meno lesioni attive in 612 mesi ) , ci si dovrebbe limitare ad una valutazione clinica e radiologica effettuata a 6 mesi / 1 anno di distanza , sulla base della quale decidere come procedere . 
 nel monitoraggio di un paziente con diagnosi denita di sm e in trattamento , la refertazione di un esame di rm dovrebbe , quindi , prevedere un confronto rispetto ad un esame precedente e contemplare le seguenti informazioni : 1 . 
indicazione se il numero totale di lesioni attive uguale indicazioni generali un aspetto critico per la valutazione longitudinale delle alterazioni di rm correlate alla sm lutilizzo di protocolli standardizzati di acquisizione , che contemplino luso di sequenze sse per lacquisizione degli esami e di procedure standardizzate per il posizionamento ed il riposizionamento dei pazienti . 
and genmab a / s ; has received funding for travel from bayer schering pharma , biogen - domp , genmab a / s , merck serono , and teva pharmaceutical industries ltd . ; serves as a consultant to bayer schering pharma , biogen - domp , genmab a / s , merck serono , pepgen corporation , and teva pharmaceutical industries ltd . ; serves on speakers bureaus for bayer schering pharma , biogen - domp , genmab a / s , merck serono , and teva pharmaceutical industries ltd . ; receives research support from bayer schering pharma , biogen - domp , genmab a / s , merck serono , teva pharmaceutical industries ltd . , and fondazione italiana sclerosi multipla . 
the purpose of this study was to determine computed tomography ( ct ) and magnetic resonance ( mr ) ndings of silent sinus syndrome ( sss ) a rare clinical entity with the constellation of progressive enophthalmos and hypoglobus , facial asymmetry and possible diplopia due to otherwise asymptomatic maxillary sinus disease . 
we reviewed the preand postoperative ct and mr images of six patients with a denitive diagnosis of sss and compared the radiological and clinical ndings with those reported in the literature . 
lo scopo di questo lavoro la presentazione dei reperti caratteristici di tomograa computerizzata ( tc ) e risonanza magnetica ( rm ) su cui si basa la diagnosi della sindrome del seno silenzioso ( sss ) , una rara condizione clinica caratterizzata da enoftalmo ed ipoglobo monolaterali , asimmetria facciale e possibile diplopia , nel contesto di una sinusopatia pauci - / asintomatica . 
entrambe le metodiche ( tc e rm ) consentono la diagnosi di sss , ma la tc dimostra pi facilmente gli elementi essenziali per la diagnosi e la diagnosi differenziale rispetto alle altre patologie sinusali , anche in pazienti senza un corretto inquadramento clinico . 
 [ 1 ] per descrivere una condizione clinica caratterizzata da enoftalmo ed ipoglobo monolaterali e spontanei associati a sinusite mascellare asintomatica , da cui la denominazione di seno 266 radiol med ( 2013 ) 118 : 265275 the term imploding antrum syndrome to better emphasise the relatively acute onset of maxillary and orbital changes . 
 in fact , enophthalmos and hypoglobus are a consequence of orbital oor collapse and of retraction / atelectasis of the underlying maxillary sinus , the aetiopathogenesis of which is still unclear but nds its cornerstone in maxillary ostium obstruction and in the ensuing hypoventilation , with negative pressure , of the maxillary sinus [ 38 ]  . 
sss has been extensively described in the literature of the past 20 years , both from a clinical and a diagnostic imaging viewpoint , with a marked increase in the frequency of cases reported in the past 5 years . 
despite an established description of its clinical and diagnostic features , sss remains known almost exclusively to ear , nose and throat specialists and ophthalmologists and is often not considered as a possible cause of diplopia , enophthalmos and facial asymmetry . 
lenoftalmo e lipoglobo sono infatti una conseguenza dellabbassamento del pavimento orbitario e della retrazione / atelettasia del sottostante seno mascellare , la cui eziopatogenesi , non ancora del tutto chiara , trova i suoi punti cardine nellostruzione dellostio mascellare e nella conseguente ipoventilazione , a pressione negativa , del seno mascellare [ 38 ]  . 
la sss stata ben denita dalla letteratura scientica degli ultimi 20 anni , sia sotto il prolo clinico che sotto il prolo di diagnostica per immagini , con un netto incremento della frequenza dei casi riportati negli ultimi 5 anni . 
a fronte di una chiara codica delle caratteristiche cliniche e di diagnostica per immagini , la sss rimane una condizione nota quasi esclusivamente ad otorinolaringoiatri ed oculisti , e frequentemente non viene considerata come possibile causa di diplopia , enoftalmo ed asimmetria facciale . 
nella pratica quotidiana il radiologo pu trovarsi nella condizione di valutare pazienti con sss senza un corretto inquadramento clinico , mediante tomograa computerizzata ( tc ) e risonanza magnetica ( rm ) eseguite con tecniche variabili a secondo dellorientamento clinico e della specialit del medico richiedente . lo scopo di questo lavoro di ribadire i reperti tc e rm della sss attraverso unanalisi rigorosa dei segni nei diversi piani dello spazio e con le diverse metodiche , al ne di rendere agevole una diagnosi che spesso radiologica prima che clinica . materials and methods materiali e metodi in our study we retrospectively reviewed ct and mr imaging examinations of six patients who were referred to our general hospital between january 2003 and january 2010 with a denite clinical and radiological diagnosis of sss ( four men and two women ; mean age , 44 years ; range , 22 67 years )  . 
we reviewed all ct and mr scans of the skull and head - and - neck region performed on the patients , including those performed at other institutions ( all in digital format )  . 
four patients underwent followup imaging within 1 month from the rst examination ( mr imaging in one case and ct in three other cases ) ; only two patients were imaged with a single modality ( ct in one , mr in one )  . 
postoperative assessment was carried out using mr imaging in two cases , ct in one and combined mr and ct in one . all mr scans were performed using a 1.5 - t device with a dedicated eight - channel birdcage coil and always included axial t1and t2 - weighted fast spin echo ( fse ) sequences nel nostro studio sono stati retrospettivamente inclusi gli esami tc e rm di sei pazienti afferiti al nostro policlinico nel periodo compreso tra gennaio 2003 e gennaio 2010 , con diagnosi clinica e radiologica denitiva di sindrome del seno silenzioso ( 4 maschi e 2 femmine ; et media : 44 anni ; range : 2267 anni )  . 
abbiamo rivalutato tutti gli esami tc ed rm del cranio e del distretto del capo - collo a cui il nostro campione stato sottoposto , anche quelli eseguiti presso altri presidi ( tutti su supporto digitale )  . 
quattro pazienti sono stati sottoposti entro un mese ad un secondo esame di diagnostica per immagini ( rm in un caso e tc negli altri tre casi ) ; solo per due pazienti stata impiegata ununica metodica ( tc in un paziente , rm in un paziente )  . 
due pazienti sono stati sottoposti ad antrostomia mascellare per via endoscopica ( ess ) , ed uno di loro ad un secondo intervento di riparazione del pavimento orbitario ( ofr )  . 
i controlli postoperatori sono stati effettuati con rm in due casi , con tc in un caso , e con rm e tc in un caso . tutti gli esami rm sono stati eseguiti su apparecchiatura da 1 , 5 t , con bobina birdcage dedicata a 8 canali , e comradiol med ( 2013 ) 118 : 265275 with 4 - mm thickness and coronal t1and t2 - weighted fse sequences with 3to 4 - mm thickness . 
fat suppression was applied to at least one contrast - enhanced t2 and t1 sequence . the ct studies were performed on 16and 64 - slice multidetector scanners using axial acquisitions with thickness ranging from 0.6 to 1 mm , followed by 2d image reconstruction in the coronal and sagittal planes ( 1 - mm thickness ) and in one case by 3d volume surface reconstructions . 
 the ct scans were analysed using both a bone and a softtissue reconstruction algorithall images were reviewed by two neuroradiologists in consensus to identify for each study ( preand postoperative ct and / or mr ) the ndings characteristics of sss on the basis of a review of studies published since 1964 . 
diplopia was slowly progressive in three patients ( cases 1 , 4 and 5 ) , had a relatively acute onset in three patients ( cases 2 , 3 and 6 ) and was associated with orbital muscle paralysis / impairment in two patients ( cases 3 and 4 )  . 
in the four patients undergoing surgery , endoscopy documented occlusion of the affected maxillary sinus infundibulum and changes in the ipsilateral orbital oor ( extremely reduced and dehiscent in cases 3 and 4 )  . 
 in the two patients undergoing maxillary antrostomy , postoperative radiological follow - up depicted restored sinus ventilation , although with no signicant clinical improvement , which was conversely obtained in the two patients who also underwent orbital oor reconstruction ( in one case following antrostomy , in one simultaneous to it )  . 
as a consequence of orbital oor dehiscence into the maxillary sinus , the coronal t2 / t1 - weighted mr images and ct reconstructions reformatted in the coronal plane depicted an increase in orbital volume , with downward attraction of the extraand intraconical fat . 
in all patients , ct showed maxillary infundibulum obstruction with lateral dislocation of the uncinate process , prendevano sempre sequenze assiali fast spin echo ( fse ) t1e t2 - dipendenti dello spessore di 4 mm e sequenze coronali fse t1e t2 - dipendenti dello spessore di 34 m in 3 studi rm sono state impiegate sequenze t1 - dipendenti dopo somministrazione di mezzo di contrasto . 
 gli studi tc sono stati eseguiti su apparecchi multidetettore ( da 16 a 64 strati ) mediante acquisizione assiale di spessore compreso tra 0 , 6 e 1 mm , con produzione di immagini 2d ricostruite sui piani coronale e sagittale ( spessore 1 mm ) ed in un caso di ricostruzioni 3d volume surface . 
tutte le immagini sono state rivalutate da due neuroradiologi in consenso , per rilevare in ogni studio ( tc e / o rm pree post - chirurgico ) i reperti che , ad una revisione della letteratura a partire dal 1964 ad oggi , risultano come caratteristici della sss . 
tutti i dati sono stati resi anonimi per lo studio e per la pubblicazione . risultati i dati clinici e radiologici dei nostri sei pazienti sono caratteristici della sindrome del seno silenzioso . 
la diplopia stata lentamente progressiva in tre pazienti ( casi 1 , 4 e 5 ) , ha mostrato uninsorgenza relativamente acuta in tre pazienti ( casi 2 , 3 e 6 ) e si associata alla paralisi / ipofunzione del muscolo orbitale in due pazienti ( casi 3 e 4 )  . 
allesame obiettivo stata sempre rilevata unasimmetria facciale con depressione malare , enoftalmo ( compreso tra 2 e 4 mm ) ed ipoglobo ( marcato nel caso 3 e 5 )  . 
nei quattro pazienti sottoposti a procedure chirurgiche , lesame endoscopico ha direttamente documentato locclusione dellinfundibolo del seno mascellare patologico e le modicazioni del pavimento dellorbita omolaterale ( estremamente assottigliato e deiscente nel caso 3 e 4 )  . 
nei due pazienti sottoposti ad antrostomia mascellare il follow - up radiologico post - operatorio ha documentato la re - areazione del seno , senza per signicativo miglioramento clinico , ottenuto invece nei due pazienti sottoposti anche a ricostruzione del pavimento orbitario ( in un caso successiva allantrostomia , in uno contemporanea )  . 
come conseguenza della deiscenza del pavimento orbitario nel seno mascellare , le immagini coronali rm t2 / t1 - dipendenti e le ricostruzioni tc riformate sul piano coronale hanno documentato aumento del volume dellorbitario , con attrazione verso il basso del tessuto adiposo extraed intraconico . 
in patients with visual disturbances ( cases 2 , 3 and 4 ) , ct images reconstructed in the coronal plane and coronal t1or t2 - weighted fat - saturated mr images showed alterations in the normal position of the orbital muscles . discussion the rst case of enophthalmos caused by paucior asymptomatic sinus disease was reported by montgomery in 1964 [ 9 ] , but it was only 30 years later that soparkar et al . 
 [ 1 ] coined the term silent sinus syndrome to indicate a condition characterised by spontaneous and unilateral enophthalmos and hypoglobus associated with volume reduction and ipsilateral maxillary sinus retraction , without any symptoms of sinusitis or any history of trauma or surgical procedure on the nasal and paranasal cavities [ 1 , 3 ]  . 
enophthalmos and hypoglobus are almost constantly associated with malar depression and facial asymmetry , whereas visual disturbances such as vertical diplopia ( frequently transient ) , lid retraction / pseudoptosis , lagophthalmos and blurred vision are less frequent [ 10 ]  . 
however , several cases have been reported in which the rapid collapse of the orbital oor , thin and dehiscent , produced an almost acute onset [ 11 ]  . 
 the evolution is variable , ranging from a relative stability of symptoms and ct / mr ndings over several years to a rapid evolution in < 1 year , towards diplopia and an increase in hypoglobus , enophthalmos and facial asymmetry [ 1 , 2 , 4 , 10 ]  . 
initially , the hypothesis that chronic obstructive sinusitis coexisted with a primary condition of sinus hypoplasia was formulated ; however , several authors demonstrated the absolute normality of the maxillary sinus walls before clinical and radiological manifestations of sss [ 6 , 7 , 1214 ] , which conrms that it is an acquired condition . 
studies identied infundibular obstruction as a probable pathogenetic event , which leads to sinus hypoventilation and development of negative pressure , with a mechanism that resembles that of middle ear atelectasis ne dellinfundibolo mascellare con dislocazione laterale del processo uncinato , mentre la rm evidenziava questo stato solo in quattro casi . 
in tutti i pazienti la tc ha meglio rilevato lassottigliamento delle pareti del seno ( pavimento orbitario in 6 pazienti , parete anteriore in quattro pazienti e parete posteriore in due pazienti )  . 
altre reperti radiologici riscontrati sono stati lipoplasia del turbinato medio ( caso 2 , 3 e 4 ) e la deviazione del setto nasale ( caso 1 e 4 )  . 
nei pazienti con disturbi oculari ( casi 2 , 3 e 4 ) con le immagini tc ricostruite sul piano coronale e rm coronali t1 - pesate o t2 fat - sat , si sono evidenziate le modicazioni della normale posizione dei muscoli orbitari . discussione il primo caso di enoftalmo causato da sinusopatia pauci - / asintomatica stato riportato in letteratura nel 1964 da montgomery [ 9 ] , ma solo 30 anni dopo soparkar et al . 
 [ 1 ] hanno coniato il termine di sindrome del seno silenzioso per indicare una condizione caratterizzata da enoftalmo e ipoglobo spontanei e monolaterali , associati a riduzione di volume / retrazione del seno mascellare omolaterale , in assenza di sintomatologia sinusitica e di storia di traumi e pregressi interventi chirurgici sulle cavit nasali e paranasali [ 1 , 3 ]  . 
allenoftalmo ed allipoglobo si associano quasi costantemente la depressione malare e lasimmetria facciale , mentre risultano meno frequenti disturbi visivi quali la diplopia verticale ( frequentemente transitoria ) , il sollevamento palpebrale / pseudo - ptosi , il lagoftalmo e la visione offuscata [ 10 ]  . 
levoluzione variabile , da una relativa stabilit dei sintomi e dei reperti tc / rm per anni , alla rapida evoluzione , in meno di un anno , verso la diplopia e lincremento di ipoglobo , enoftalmo ed asimmetria facciale [ 1 , 2 , 4 , 10 ]  . 
inizialmente era stata avanzata lipotesi che la sinusite cronica ostruttiva si sovrapponesse ad una condizione primaria di ipoplasia sinusale , ma numerosi autori hanno dimostrato lassoluta normalit delle pareti del seno mascellare prima dellevidenza dei reperti clinici e radiologici della sss [ 6 , 7 , 1214 ] , rendendo ormai denito che si tratta di una condizione acquisita . 
 recenti lavori identicano come probabili eventi patogenetici lostruzione dellinfundibolo , la conseguente ipoventilazione sinusale e linstaurarsi di una pressione negativa , con un meccanismo simile a quello dellatelettasia dellorecchio medio da mal funzionamento della tuba di eustachio [ 37 , radiol med ( 2013 ) 118 : 265275 from eustachian tube dysfunction [ 37 , 1518 ]  . 
furthermore , progressive osteomalacia [ 7 ] or probably reduced osteoblastic activity [ 19 ] is thought to contribute to inward bowing of the sinus bone and to orbital oor osteomalacia . 
regardless of the speed of symptom onset , the mechanism that lies at the basis of infundibular obstruction has not yet been denitely claried : some peculiar anatomical congurations of the ostiomeatal complex , in association with mucosal thickness , might lead to complete obstruction of sinus drainage [ 1921 ]  . 
 surgical intervention is useful to stop progression of maxillary and orbital alterations and to correct enophthalmos or facial deformity , although it does not seem to produce a signicant restoration of orbital muscle function and , consequently , of diplopia [ 11 , 21 ]  . 
biopsy of the maxillary sinus mucosa , which has no diagnostic or therapeutic indication , has been performed in the event of misdiagnosis or diagnostic uncertainty [ 3 ]  . 
the typical ndings of sss are represented by maxillary sinus volume reduction with inward bowing of the walls , orbital oor depression and compensatory increase in orbital volume and retroantral space . 
the sinus is completely , or almost completely , occluded by secretions and by thickening of mucosa that line the sinuses , the adjacent uncinate process looks lateralised and the middle meatus is expanded . 
la persistenza della pressione negativa causerebbe una lenta atelettasia del seno mascellare ; inoltre un progressivo processo osteomalacico [ 7 ] o probabilmente una ridotta attivit osteoblastica [ 19 ] concorrerebbero allintroessione delle pareti ossee del seno e allosteomalacia del pavimento orbitario . 
a prescindere dalla rapidit di insorgenza della sintomatologia , il meccanismo primario alla base dellostruzione dellinfundibolo non denitivamente chiarito : particolari congurazioni anatomiche del complesso ostio - meatale , in associazione allo spessore della mucosa , potrebbero favorire unostruzione completa del drenaggio sinusale [ 1921 ]  . 
lintervento chirurgico risulta utile nellarrestare la progressione delle alterazioni mascellari ed orbitarie , nel correggere lenoftalmo o la deformit facciale , ma non sembra determinare un signicativo recupero della funzionalit dei muscoli orbitari e quindi della diplopia [ 11 , 21 ]  . 
la biopsia della mucosa del seno mascellare , che non trova alcuna indicazione diagnostica o terapeutica , stata eseguita in passato nei casi di errata diagnosi o dubbio diagnostico [ 3 ]  . 
i reperti caratteristici della sss sono rappresentati dalla riduzione di volume del seno mascellare con aspetto retratto delle pareti , dalla depressione del pavimento orbitario e dal compensatorio incremento del volume dellorbita e dello spazio adiposo retroantrale . 
2a - c in a patient with right vertical diplopia , coronal mr images ( a , b ) better demonstrate collapse of extraand intraconical fat pad ( arrow ) and downwards bowing of the right orbital inferior rectus muscle ( arrowhead ) compared with the contralateral one ( double arrowheads ) than does the sagittal view ( c )  . 
2a - c le immagini rm in coronale ( a , b ) offrono una migliore visualizzazione rispetto al piano sagittale ( c ) della dislocazione verso il basso del tessuto adiposo extraed intraconico ( freccia ) e del muscolo retto inferiore di destra ( punta di freccia ) rispetto al controlato ( doppia punta di freccia ) , in paziente con diplopia verticale destra . 
 fundibulum occlusion and lateral retraction of the uncinate process are also best evaluated in the coronal plane , as is the width of the middle meatus ( which appears expanded ) , possible hypoplasia of the middle turbinate [ 3 , 10 , 24 ] and septal deviation . 
 owing to the moderate thickness of these structures , their nature ( osteocartilaginous ) and their environment ( airways ) , the modality of choice for studying the uncinate process and its branches is thin - slice ct imaging with coronal reformations [ 25 ]  . 
 ricerca dellocclusione dellinfundibolo mascellare e la retrazione laterale del processo uncinato sono meglio evidenti sul piano coronale , cos come la valutazione dellampiezza del meato medio ( che risulta espanso ) , la possibile ipoplasia del turbinato medio [ 3 , 10 , 24 ] e la deviazione del setto nasale . 
a causa del modesto spessore di queste strutture , della loro natura ( osteo - cartilaginea ) e dellambiente in cui si trovano ( cavit aeree ) , la metodica di elezione per valutare il processo uncinato ed i suoi rapporti , la tc con immagini a spessore sottile riformate sul piano coronale [ 25 ]  . 
le immagini tc permettono di apprezzare lassottigliamento della parete posteriore del seno mascellare alterato ( freccia punteggiata in a )  . sinus walls collapse , to a variable extent , and the anterior and posterior walls are the most frequently involved [ 2 , 4 ]  . 
radiologically , chronic sinusitis and maxillary sinus hypoplasia are the conditions that most frequently enter the differential diagnosis with sss , whereas trauma and cancer are rarely considered [ 26 ]  . 
however , it should be noted that even in sss the coexistence of chronic inammation can make the maxillary sinus walls look sclerotic [ 2 , 12 ] , which can complicate the differential diagnosis . 
maxillary sinus hypoplasia is characterised by sinus il collabimento delle pareti del seno di grado variabile , ed interessa prevalentemente le pareti anteriore e posteriore [ 2 , 4 ]  . 
dal punto di vista radiologico , la sinusite cronica e lipoplasia del seno mascellare sono le condizioni che pi frequentemente entrano in diagnosi differenziale con la sss , molto raramente i traumi ed i tumori [ 26 ]  . 
va per considerato che anche nella sss il coesistente stato di inammazione cronica pu far s che le pareti del seno mascellare appaiono sclerotiche [ 2 , 12 ] , e questo pu rendere pi difcoltosa la diagnosi differenziale . 
4a - f coronal reformatted ct images ( a ) better demonstrate lateral retraction of the uncinate process in the affected sinus ( dotted arrow ) and maxillary infundibulum obliteration ( double arrows ) compared with the axial view ( b )  . 
coronal and sagittal ct images show thinning of the orbital oor ( a , d ) ; axial ct image ( c ) shows focal demineralisation of the anterior sinus wall ( double arrowheads ) , which is emphasised on the 3d volume - rendered image ( * )  . 
4a - f le immagini tc riformate sul piano coronale ( a ) permettono di identicare con maggiore facilit rispetto alle immagini assiali ( b ) la posizione laterale del processo uncinato dal lato del seno affetto ( freccia continua ) e locclusione dellinfundibolo mascellare ( doppie frecce continue )  . 
le immagini coronali e sagittali evidenziano lassottigliamento del pavimento dellorbita ( a , d ) , quelle assiali ( c ) la focale osteomalacia della parete anteriore ( doppie punte di freccia ) , enfatizzata dalle immagini 3d volume rendering ( vr ) ( * )  . 
it has been described since 1964 [ 9 ] in international scientic papers , mostly originating from otorhinolaryngological and ophthalmological clinical settings [ 13 , 5 , 6 , 813 , 1524 , 2731 ] and , to a lesser extent , in diagnostic imaging studies [ 4 , 7 , 14 , 25 , 26 ]  . 
radiologists should be able to recognise ct and mr signs typical of this condition , as they may be required to formulate a diagnosis of sss on the sole basis of these ndings and without a clear conclusioni la sindrome del seno silenzioso una condizione relativamente rara , la cui frequenza probabilmente sottostimata in quanto largamente ignorata come possibile causa di diplopia , enoftalmo ed asimmetria facciale [ 30 , 31 ]  . 
stata descritta a partire dal 1964 [ 9 ] con contribuiti scientici internazionali provenienti principalmente da ambienti clinici specialistici ( otorinolaringoiatrici ed oculistici ) [ 13 , 5 , 6 , 813 , 1524 , 2731 ] , ed in minor misura da lavori di diagnostica per immagini [ 4 , 7 , 14 , 25 , 26 ]  . 
il radiologo tenuto a conoscere i segni tc ed rm di questa condizione , in quanto nella pratica quotidiana pu essere chiamato in causa per porre diagnosi di sss solo sulla base dei suoi reperti , anche senza un preciso sospetto clinico . 
5a - d axial ( a ) and coronal ( b ) ct images show right sinus opacication ( asterisk ) and decrease in volume , the inward trend of anterior , medial and lateral sinus walls ( arrows ) and the ipsilateral anterior wall bone malacia ( arrowhead )  . 
5a - d le immagini tc assiale ( a ) e coronale riformata ( b ) mostrano un seno mascellare destro opacato ( * ) , di dimensioni inferiori al controlaterale , con pareti retratte internamente ( frecce ) e parete anteriore di aspetto malacico ( punta di freccia )  . 
6a , b le immagini assiale ( a ) e quella ricostruita sul piano coronale ( b ) dimostrano lobliterazione del seno mascellare di destra , senza deiscenza del pavimento dellorbita ( freccia tratteggiata ) , e lispessimento / sclerosi delle pareti anteriore ( freccia ) e posteriore ( punta di freccia ) del seno in un paziente con sinusite cronica ( pattern infundibolare )  . 
ct is the method of choice in the study of the nasal and paranasal cavities ; integration of axial images and coronal reconstructions enables detection of all those ndings necessary to formulate to a diagnosis of sss and rule out the most common differential diagnoses ( chronic sinusitis , maxillary sinus hypoplasia )  . 
therefore , the correct diagnosis of sss can be obtained by using a single method , and the combination of mr and ct should be restricted to cases in which following a diagnosis based on mr a ct study is needed for surgical planning . 
a thorough knowledge of sss che la rm permettono il riconoscimento dei reperti caratteristici della sss , a condizione che includano nel loro campo di vista le orbite ed i seni mascellari . 
la tc la metodica di elezione per lo studio delle cavit nasali e paranasali , lintegrazione tra immagini acquisite sul piano assiale e quelle ricostruite sul piano coronale , permette di identicare tutti i reperti necessari alla diagnosi di sss e di escludere le pi comuni patologie che entrano in diagnosi differenziale ( sinusite cronica , ipoplasia del seno mascellare )  . 
la corretta diagnosi della sss pu essere ottenuta , quindi , con una singola metodica , e lintegrazione tra rm e tc deve essere riservata ai casi in cui a seguito di una diagnosi basata sulla rm sia necessario uno studio tc per la pianicazione chirurgica . 
note the slight inwards trend of the anterior sinus wall ( arrow in a ) and the downwards trend of the orbital oor ( dotted arrow in b )  . 
la tc dimostra laspetto caratteristico delle pareti del seno ipoplasico , che appaiono pi spesse ( linea tratteggiata ) rispetto al controlato ( doppia linea ) , e di aspetto spongioso . among radiologists may help to reduce the number of imaging procedures that sss patients need to undergo , thus leading to faster and more efcient diagnostic and therapeutic management , averting the need for unnecessary and costly procedures . sss tra i radiologi potr portare alla riduzione del numero delle procedure di diagnostica per immagini a cui vengono sottoposti questi pazienti ed a una pi rapida ed efcace gestione diagnostico - terapeutica , senza il ricorso a procedure inutili e costose . 
mazziotti , via consolare pompea 1871 , 98165 messina , italy , tel . : + 39 - 090 - 3973213 , fax : + 39 - 090 - 2937427 , e - mail : smazziotti@unime.it received : 5 april 2011 / accepted : 26 june 2011 / published online : 19 march 2012 springer - verlag 2012 abstract the oral cavity is a complex anatomical region consisting of different anatomical sites and subsites . 
cross - sectional computed tomography ( ct ) and magnetic resonance imaging ( mri ) play a key role in staging locoregional disease by demonstrating submucosal spread and involvement of deep layers ; evaluation of specific pathways of spread to peculiar anatomical subsites is also fundamental information that can be obtained with these techniques . 
 the purpose of this paper is to illustrate ct and mri findings of anatomical subsites involved by tumours of the oral cavity . keywords oral cavity neoplasm computed tomography magnetic resonance imaging riassunto il cavo orale rappresenta una regione anatomica complessa , nella cui costituzione rientrano differenti aree e logge . 
limaging panesplorante ottenuto con tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) assume un ruolo fondamentale nella stadiazione locoregionale di malattia , dimostrando la possibile estensione sottomucosa e il coinvolgimento dei piani profondi ; fondamentale inoltre linformazione ottenibile con tali indagini relativamente alla identificazione di peculiari vie di diffusione in alcune particolari sub - sedi anatomiche . 
 scopo del lavoro illustrare i rilievi di semeiotica tc e rm nelle neoplasie del cavo orale relativamente al coinvolgimento delle diverse sub - sedi anatomiche . parole chiave cavo orale neoplasia tomografia computerizzata risonanza magnetica introduction introduzione the oral cavity is a complex anatomical region made up of various sites and subsites , and oral cancer is undoubtedly the most frequent and significant pathological condition affecting the region . 
nellambito di tale distretto la patologia neoplastica rappresenta certamente levento pi frequente e di maggiore rilevanza clini124 radiol med ( 2013 ) 118 : 123139 around 7% [ 1 ]  . 
the most frequent histological type ( 90% ) is squamous cell carcinoma ( scc ) , followed by tumours of the minor salivary glands ( adenoid cystic carcinoma , adenocarcinoma , mucoepidermoid carcinoma ) , lymphoma and the rarer sarcomas ( liposarcoma and rhabdomyosarcoma ) [ 1 , 2 ]  . 
in europe , and specifically in italy , the most frequently affected subsites are the lower lip ( 38% ) , the tongue ( 22% ) , the floor of the mouth ( 17% ) and the gingiva ( 6% ) [ 14 ]  . the most important risk factors influencing development of the disease include smoking and alcohol abuse , particularly when the two are associated . 
in most cases , oral cancers can be identified at clinical examination , which is often the first diagnostic step and which also allows assessment of mucosal involvement [ 1 , 3 , 4 ]  . 
computed tomography ( ct ) and magnetic resonance ( mr ) imaging of the oral cavity play a fundamental role in locoregional staging thanks to their ability to demonstrate the possible extension to the submucosa and the involvement of the deeper planes . 
the techniques also provide fundamental information regarding identification of peculiar patterns of spread to some anatomical subsites [ 14 ] the aim of this paper is to illustrate the ct and mr findings in oral cancers with particular attention to the various anatomical subsites . 
listotipo pi frequente ( 90% ) rappresentato dal carcinoma squamoso ( cs ) , seguito dai tumori delle ghiandole salivari minori ( carcinoma adenoido - cistico , adenocarcinoma , carcinoma mucoepidermoide ) , dal linfoma e dai pi rari sarcomi ( liposarcoma e rabdomiosarcoma ) [ 1 , 2 ]  . 
in europa e , specificatamente in italia , le sottosedi pi colpite sono il labbro inferiore ( 38% ) , la lingua ( 22% ) , il pavimento orale ( 17% ) , la gengiva ( 6% ) [ 14 ]  . 
 tra i pi significativi fattori di rischio condizionanti lo sviluppo di tale neoplasia , si annoverano il fumo e labuso di alcool , con particolare rilievo assunto dalla loro associazione ; meno rilevanti appaiono il ridotto apporto vitaminico e lesposizione ai raggi ultravioletti [ 14 ]  . 
nella maggioranza dei casi le neoplasie del cavo orale sono apprezzabili allesame clinico che costituisce spesso il primo momento diagnostico , consentendo inoltre di verificare in modo immediato il coinvolgimento mucoso [ 1 , 3 , 4 ]  . 
limaging panesplorante [ tomografia computerizzata ( tc ) e / o risonanza magnetica ( rm ) ] , assume un ruolo fondamentale nella stadiazione loco - regionale di malattia , dimostrando la possibile estensione sottomucosa e il coinvolgimento dei piani profondi ; fondamentale infine linformazione ottenibile con tali indagini e relativa alla identificazione di peculiari vie di diffusione in alcune sub - sedi anatomiche [ 14 ]  . 
 study technique computed tomography tecnica di studio according to the clinical indication , acquisition volume can be restricted to the oral cavity or extended to the neck and maxillofacial region . 
in addition to problems relating to multiplanar reconstructions , and in particular those affecting data management during postprocessing , there is also the important issue of the methodological stratagems to be adopted during volume acquisition , such as the puffed - cheek technique , open - mouth acquisition or protruded - tongue acquisition [ 57 ]  . 
lastly , contrast - enhanced study of the oral cavity is a crucial and compulsory phase that should be performed with dynamic acquisition techniques capable of differentiating the purely arterial phase ( to visualise the lingual artery , a fundamental anatomical landmark ) from the venous and interstitial phases [ 8 , 9 ]  . tomografia computerizzata il volume di acquisizione , secondo le indicazioni cliniche , pu essere limitato al cavo orale o esteso al collo e al distretto maxillo - facciale . 
in fase di post - processing convenzionalmente si ottengono immagini parallele o perpendicolari al palato duro ; bisogna tuttavia considerare la possibilit di ottenere ricostruzioni lungo traiettorie spezzate o curve che ben rappresentano le diverse sub sedi anatomiche . 
oltre alle problematiche legate alla ricostruzione multiplanare , che investono la gestione dei dati nel corso del post - processing , vi da aggiungere limportanza , talvolta decisiva , del ricorso ad alcuni accorgimenti metodologici da porsi in essere , preliminarmente , durante lacquisizione volumetrica , quali per esempio lacquisizione con distensione gassosa delle guance , lacquisizione a bocca aperta o lacquisizione a lingua estrusa [ 57 ]  . 
infine , lo studio contrastografico del cavo orale rappresenta un momento ineludibile e di fondamentale importanza radiol med ( 2013 ) 118 : 123139 magnetic resonance imaging anatomical evaluation of the various subsites of the oral cavity using mr imaging consists of t1and t2 - weighted sequences acquired in axial ( parallel to the hard palate ) and coronal ( perpendicular to the hard palate ) planes . 
in addition , images obtained in the sagittal or oblique planes can in certain circumstances better visualise certain structures . multiplanar radiological anatomy of the oral cavity from the point of view of radiological anatomy , several subsites can be identified in the oral cavity . 
these include tongue , floor of the mouth , lip , cheek , alveolar - gingival arches , retromolar trigone , vestibule and hard palate [ 14 , 10 , 11 ]  . 
evaluation should be extended to some of the suprahyoid spaces adjacent to the oral cavity , including the sublingual space , the submandibular space , the buccal space and the masticator space [ 14 , 1012 ]  . 
these spaces are bounded by the deep cervical fascia , which inserts on the hyoid bone and divides this region into compartments . tongue a key element in the anatomical evaluation of the tongue is the lingual septum , which in normal conditions runs sagittally along the midline and divides the tongue into two symmetrical halves [ 24 , 10 , 13 ]  . 
its fibrofatty nature makes it immediately identifiable at ct as a hypodense strip ( midline low - density plane ) running from the base of the hyoid bone and the hyoglossal membrane to the apex of the tongue [ 24 , 10 ]  . 
acquiring images with the tongue protruded enables better evaluation of the tongue freed from the surrounding soft parts , which have the same density and can thus hamper evaluation of the tongue [ 5 , 7 ]  . floor of the mouth the reference structure in this anatomical site is the mylohyoid muscle , a flat and triangular muscle with fibres on two sides that insert medially into the median raphe . 
the coronal plane provides the best visualisation of the mylohyoid muscle , which separates the sublingual space , situated superomedie va realizzato con tecniche di acquisizione dinamiche , in grado di differenziare la fase arteriosa pura ( indispensabile per visualizzare larteria linguale , repere anatomico fondamentale dal punto di vista anatomo - chirurgico ) , dai successivi momenti dimpregnazione venosa ed interstiziale [ 8 , 9 ]  . risonanza magnetica la valutazione anatomica con rm delle diverse sub - sedi del cavo orale si estrinseca di base attraverso lacquisizione di scansioni t1 e t2 dipendenti , orientate lungo i piani assiale ( parallelo al palato duro ) e coronale ( perpendicolare al palato duro )  . 
lintegrazione con immagini ottenute lungo il piano sagittale o piani obliqui variamente orientati consente , in particolari circostanze , di meglio identificare alcune strutture . anatomia radiologica multiplanare del cavo orale nel cavo orale , da un punto di vista anatomo - radiologico , sono identificabili alcune sub - sedi rappresentate da lingua , pavimento orale , labbra , guance , arcate alveolo - gengivali , trigono retromolare , vestibolo e palato duro [ 14 , 10 , 11 ]  . 
 la valutazione deve necessariamente essere estesa ad alcuni tra gli spazi cervicali sopraioidei attigui al cavo orale , quali lo spazio sublinguale , il sottomandibolare , il buccale e il masticatorio [ 14 , 1012 ]  . 
 lingua elemento chiave nella valutazione anatomica della lingua rappresentato dal setto linguale che , in condizioni normali , decorre sagittalmente sul piano mediano e divide la lingua in due met simmetriche [ 24 , 10 , 13 ]  . 
la sua costituzione fibroadiposa lo rende facilmente apprezzabile in tc come stria ipodensa ( midline - low density - plane ) , con decorso dalla base dellosso ioide e della membrana ioglossa allapice linguale [ 24 , 10 ]  . 
la rm , caratterizzata da elevata risoluzione di contrasto , consente lottimale valutazione della muscolatura intrinseca della lingua , agevolmente differenziabile dalle strutture fibroadipose di supporto , iperintense nelle immagini t1 dipendenti [ 24 , 10 , 13 ]  . 
lacquisizione a lingua estrusa permette di meglio valutare la lingua liberata dalle adiacenze con le parti molli attigue che , a causa della uguale densit , costituiscono un ostacolo rilevante alla valutazione della stessa [ 5 , 7 ]  . 126 radiol med ( 2013 ) 118 : 123139 pavimento orale struttura di riferimento in tale sede anatomica il muscolo miloioideo , diaframma muscolare le cui fibre dei due lati si inseriscono medialmente sul rafe mediano , decorrendo dallosso ioide alla branca orizzontale della mandibola , inserendosi sulla linea miloioidea [ 2 , 3 , 10 ]  . 
m , muscolo miloioideo ; gi , muscolo genioioideo ; di , ventre anteriore del muscolo digastrico ; freccia , linea miloioidea ; teste di freccia , muscolo platisma ; ssl , spazio sublinguale ; ssm , spazio sottomandibolare . 
this muscular diaphragm is incomplete posteriorly , which favours the transcompartmental spread of pathological processes at that level [ 5 , 10 , 13 , 14 ]  . il costituente anatomico principale del labbro rappresentato dal muscolo orbicolare della bocca , composto solo in parte da fibre proprie e , prevalentemente , da fibre afferenti da altri muscoli facciali quali il muscolo elevatore del labbro superiore , il muscolo risorio , lelevatore dellangolo della bocca e il depressore dellangolo della bocca ; entrano nella compagine muscolare anche il muscolo depressore del labbro inferiore , il mentale le fibre del muscolo buccinatore [ 2 , 3 , 10 , 13 ]  . 
the musculature also includes the depressor muscle of the lower lip , the levator menti and fibres of the buccinator muscle [ 2 , 3 , 10 , 13 ]  . 
questultima , corrispondente al corpo adiposo del bichat , maggiormente sviluppata nel neonato con la funzione di favorire lo scorrimento dei piani muscolari durante i processi di suzione e masticazione [ 10 , 11 , 13 , 15 ]  . 
 the latter , known as the buccal fat pad , is more developed spazio masticatorio lo strato superficiale della fascia cervicale profonda a livello del bordo inferiore della mandibola si sdoppia , avvolgendo i muscoli della masticazione , cos delimitando lo spazio masticatorio [ 10 , 12 , 16 ]  . 
dal punto di vista anatomo - radiologico , quindi , bisogna tenere in considerazione le potenzialit della tc nella valutazione della corticale ossea sul versante vestibolare , linguale e , soprattutto , nelle sedi di edentulia , rappresentando queste ultime una barriera meno resistente allinfiltrazione neoplastica dellosso [ 1012 , 16 ]  . 
la sua mucosa si continua con quella che riveste le attigue sub - sedi del cavo orale e , postero - medialmente , con quella del pilastro anteriore della loggia tonsillare [ 2 , 3 , 10 ]  . 
il trigono retromolare costituisce pertanto un vero e proprio crocevia nel quale convergomasticator space the superficial layer of the deep cervical fascia splits at the level of the lower border of the mandible , surrounding the muscles of mastication and thus defining the masticator space [ 10 , 12 , 16 ]  . 
from the point of view of radiological anatomy , therefore , ct can be useful in evaluating the cortical bone on the vestibular side , the lingual side and particularly at sites of edentulism , the latter being a less resistant barrier to neoplastic infiltration of the bone [ 1012 , 16 ]  . 
arrowhead , parotid duct , which divides the fat content of the buccal space into an anterior portion ( star ) and posterior portion , corresponding to the buccinator fat pad ( asterisk )  . 
testa di freccia : dotto parotideo di stenone che suddivide il contenuto adiposo dello spazio bucale in una porzione anteriore ( stella ) ed una porzione posteriore corrispondente alla bolla del bichat ( asterisco )  . 
 nellacquisizione tc con distensione gassosa delle guance , le superfici mucose si separano e la cavit vestibola re apprezzabile insufflata daria con morfologia a ferro di cavallo a concavit posteriore . 
 una completa valutazione anatomica non pu prescindere dalla identificazione dei forami palatini ed incisivo con i rispettivi canali , potenziali vie di diffusione neoplastica perineurale del carcinoma adenoideo - cistico delle ghiandole salivari minori [ 24 , 10 , 14 , 1618 ]  . neoplasie del cavo orale lingua le sedi di pi frequente insorgenza delle neoplasie linguali sono le porzioni laterali e la faccia inferiore [ 10 , 19 ]  . 
 gli aspetti anatomo - patologici macroscopici insieme alla ricca vascolarizzazione del tessuto eteroformativo tipici del cs della lingua danno contezza dei principali aspetti di semeiotica allimaging panesplorante [ 10 , 19 ]  . 
m , muscolo massetere ; t , muscolo temporale ; ptl , muscolo pterigoideo laterale ; asterisco , muscolo pterigoideo mediale . ing the adjacent subsites of the oral cavity and posteromedially with that of the anterior pillar of the tonsillar fossa [ 2 , 3 , 10 ]  . 
the retromolar trigone therefore is a crossroad where numerous muscular and nervous structures converge , as well as adipose spaces , which are potential pathways of lesser resistance to neoplastic spread [ 2 , 3 , 10 ]  . 
in ct acquisitions with the puffed - cheek technique , the mucosal surfaces are separated and the vestibular cavity can be appreciated as an air - filled horseshoe - shaped space . 
these are , in fact , potential pathways of perineural neoplastic spread of adenoid - cystic carcinoma of the minor salivary glands [ 24 , 10 , 14 , 1618 ]  . radiol med ( 2013 ) 118 : 123139 iii posteriore del corpo linguale pi facilmente presentano una tendenza a diffondere in profondit con coinvolgimento delle componenti del pavimento orale . 
la peculiarit di tale neoplasia , infine , a diffondere attraverso vie anatomiche preformate rappresentate dai fasci della muscolatura estrinseca , giustifica il coinvolgimento , sovente tardivo , di strutture ossee limitrofe , ma non adiacenti , quali losso ioide e la mandibola [ 10 , 19 , 20 ]  . pavimento orale il 90% delle neoplasie del pavimento orale originano a circa 2 cm dalla linea mediana anteriore [ 9 , 10 , 19 , 20 ]  . 
lestensione sottomucosa comporta usualmente il coinvolgimento dello spazio sublinguale a prevalente contenuto adiposo ( lateral - low density - plane ) , sede del dotto di wharton , del nervo linguale , della ghiandola sublinguale e del lobo profondo della ghiandola sottomandibolare . 
il diaframma , posteriormente incompleto , rappresentato dal muscolo miloioideo che separa lo spazio sub - linguale da quello sottomandibolare , facilita la diffusione neoplastica trans - compartimentale [ 9 , 10 , 21 , 22 ]  . 
tm , muscolo temporale ; b , spazio buccale ; tr , trigono retromolare ; freccia , canale mandibolare . oral cancer tongue the most frequent sites for the development of tongue cancer are the lateral portions and the inferior face [ 10 , 19 ]  . 
the gross pathology features together with the rich vasculature of the heterogeneous tissue typical of scc of the tongue give rise to the main imaging appearances of the tumours [ 10 , 19 ]  . 
the forms that involve the inferior face of the posterior third of the tongue body more frequently tend to spread deeply , thus involving components of the floor of the mouth . 
this justifies the often late involvement of nearby but not adjacent skeletal structures , such as the hyoid bone and mandible [ 10 , 19 , 20 ]  . 130 radiol med ( 2013 ) 118 : 123139 fig . 
7a , b axial contrast - enhanced computed tomography image obtained with protruded tongue technique ( a ) and sagittal multiplanar reconstruction ( mpr ) image ( b )  . 
7a , b scansioni tc assiale dopo somministrazione endovena di mezzo di contrasto eseguita a lingua estrusa ( a ) e ricostruzione multiplanare ( mpr ) sagittale ( b )  . 
neoformazione del corpo linguale circoscritta allemilingua sinistra , nelle mpr il processo patologico ad elevata impregnazione contrastografica ( asterisco ) ben dissociabile dallarteria linguale ( teste di freccia )  . radiol med ( 2013 ) 118 : 123139 fig . 
 la lesione mostra un preponderante sviluppo in profondit con infiltrazione a tutto spessore del corpo linguale , del pavimento del cavo orale sino a giungere nel grasso della loggia sottomandibolare a ridosso della ghiandola ( s )  . 132 radiol med ( 2013 ) 118 : 123139 fig . 
in una ricostruzione in proiezione di massima intesit ( mip ) assiale condotta a livello dellosso ioide ( b ) apprezzabile coinvolgimento strutturale osteolitico del corpo dello ioide ( freccia ) e voluminosa adenopatia metastatica giugulo - digastrica destra ( asterisco )  . floor of the mouth as many as 90% of cancers of the floor of the mouth originate at around 2 cm from the anterior midline [ 9 , 10 , 19 , 20 ]  . 
extension to the submucosa usually means involvement of the sublingual space , with its prevalently adipose content ( lateral low - density plane ) , which contains the submandibular duct , the lingual nerve , the sublingual gland and the deep lobe of the submandibular gland . 
squamous cell carcinoma of the lip ( asterisk ) involving the buccal space and infiltrating the buccinator muscle up to its insertion in the pterygomandibular raphe ( arrow )  . 
carcinoma squamoso del labbro ( asterisco ) che invade il grasso dello spazio buccale e infiltra il muscolo buccinatore sino alla sua inserzione in corrispondenza del rafe pterigo - mandibolare ( freccia )  . 
tale rilievo appare ben evidente nel confronto con il lato sano controlaterale . radiol med ( 2013 ) 118 : 123139 the most common site for the onset of scc of the lip is the vermilion border [ 9 , 10 , 21 , 22 ]  . 
 cheek ( buccal space ) although they may be easily examined clinically , carcinomas situated in the buccal space and vestibule are often associated with an unpredictable locoregional pattern of spread , with an unfavourable prognosis [ 1 , 9 , 10 , 20 , 2328 ]  . 
 bolo , seppur di facile ispezione clinica , possono dar luogo a quadri di diffusone loco - regionale sovente imprevedibili e prognosticamente sfavorevoli [ 1 , 9 , 10 , 20 , 2328 ]  . 
12a - c axial computed tomography ( a ) and coronal multiplanar reconstruction ( b ) images obtained with puffed - cheek technique showing pathological tissue infiltrating the buccinator muscle and extending to the retromolar trigone ( arrow in a )  . 
la ricostruzione volume rendering technique ( vrt ) ( c ) dimostra la ridotta distensibilit della guancia sinistra . 134 radiol med ( 2013 ) 118 : 123139 therefore , imaging can play a decisive role in most cases . 
 alternatively , it may spread posteriorly towards the masseter muscle and the adipose layer that connects the buccal fat pad to the buccal space located more deeply [ 1 , 9 , 10 , 20 , 2328 ]  . 
the most frequent findings are mandibular bone erosion and invasion of the muscles ( medial and lateral pterygoid , masseter and temporal ) and fascia [ 1 , 9 , 10 , 20 , 2328 ]  . gingiva gingival cancers make up a rather unique group due to the close adherence between the mucosa , the periosteum and the skeletal tissue of the maxilla and mandible . 
as a result , at imaging , gingival cancers can appear similar to tumours arising from the skeletal components of this region [ 1 , 9 , 10 , 20 , 2328 ]  . 
in the event the mandible is involved , establishing the degree of involvement of the cortical and spongy bone and the possible spread to the mandibular canal is crucial for surgical purposes [ 1 , 9 , 10 , 20 , 23 , 24 , 2628 ]  . 
 retromolar trigone due to the particular characteristics of the retromolar trigone , carcinomas that arise in this subsite make up a unique pathological entity , which is hampered by a variety of prognostic and therapeutic problems [ 2934 ]  . 
ne deriva che le neoplasie gengivali , possono assumere comportamenti allimaging analoghi a quelli di neoplasie a origine dalle componenti scheletriche di tale regione [ 1 , 9 , 10 , 20 , 2328 ]  . 
nel caso sia coinvolto il mascellare inferiore , fondamentale ai fini chirurgici stabilire il grado di interessamento della corticale e della spongiosa e leventuale estensione al canale mandibolare [ 1 , 9 , 10 , 20 , 23 , 24 , 2628 ]  . 
 trigono retromolare i carcinomi che insorgono nella regione del trigono retromolare , in virt delle caratteristiche topografiche di tale sub - sede , rappresentano unentit patologica del tutto peculiare , gravata da problematiche prognostiche e terapeutiche differenti [ 2934 ]  . 
la diffusione mediale prevede linfiltrazione dello spazio adiposo pterigomandibolare , dei muscoli masticatori ( pterigoideo esterno , interno e temporale ) e , nei casi pi avanzati , del margine laterale della lingua . 
la diffusione allo spazio pterigomandibolare rappresenta un evento particolarmente critico , in quanto da essa pu derivare la diffusione della neoplasia al grasso contenuto nel forame mandibolare , con conseguente infiltrazione del nervo alveolare inferiore . 
le scansioni rm assiali t1 pesate acquisite prima ( b ) e dopo ( c , d ) somministrazione endovenosa di gadolinio dimostrano la presenza di tessuto patologico ad elevata impregnazione contrastografica che si sviluppa a ridosso del mascellare posteriore , sia sul versante linguale che su quello vestibolare . 
spread to the pterygomandibular space is a particularly critical event , in that from there the tumour may spread to the fat contained in the mandibular foramen , with consequent infiltration of the inferior alveolar nerve . 
cos come nei tumori della mucosa gengivale , anche nelle neoplasie del trigono retromolare linteressamento dellosso mandibolare un evento non raro , pi frequente nelle mandibole edentule , poich losso alveolare non costituisce una valida barriera alla progressione della neoplasia . 
involvement of the insertion of the temporal muscle ( tm ) is also well depicted , as well as focal bone erosion of the ascending ramus of the mandible ( short arrow ) ; healthy mandibular foramen ( long arrow )  . 
on an oblique sagittal reconstruction obtained on a more external plane ( b ) , the neoplasm obliterates the fat plane ( black arrow ) between the masseter ( m ) and buccinator muscles ( white arrow ) ; the latter appears thickened . 
evidente il coinvolgimento dellinserzione del muscolo temporale ( tm ) e la focale erosione della branca montante della mandibola ( freccia corta ) ; freccia lunga : forame mandibolare normale . 
in una ricostruzione sagittale obliqua ottenuta su un piano pi esterno ( b ) , la neoplasia determina la cancellazione del piano adiposo ( freccia nera ) tra muscolo massetere ( m ) e muscolo buccinatore ( freccia bianca ) che si presenta ispessito . 
la ricostruzione sagittale obliqua con finestra delle parti molli ( a ) dimostra la neoplasia ( c ) che oblitera il grasso contenuto nel forame mandibolare ( freccia )  . 
 radiol med ( 2013 ) 118 : 123139 with tumours of the gingival mucosa , involvement of the mandibular bone in carcinomas of the retromolar trigone is a rare event that occurs more commonly in the edentulous mandible , as the alveolar bone is not a valid barrier to disease progression . 
as the hard palate is lined by mucosa that is closely related to the periosteum and is continuous on both sides with infine una caratteristica via di diffusione delle neoplasie in questa sede rappresentata dalla diffusione perineurale lungo il nervo alveolare inferiore , il nervo linguale e il nervo miloioideo . 
essendo il palato duro rivestito da mucosa strettamente aderente al periostio e in continui t nei due lati con la mucosa gengivale , esse rappresen tano , usualmente , lestensione di carcinomi primitivi della gengiva . 
ct image obtained through the level of the hard palate ( a ) shows a large osteolytic lesion in the right side causing enlargement of greater palatine foramen ( asterisk )  . 
much rarer is the primary tumour of the mucosa lining the hard palate or arising from the minor salivary glands located in the mucosa [ 9 , 10 , 20 , 23 , 24 ]  . 
the most common histological types include adenoid - cystic carcinoma with its typical spread pattern along the perineural pathways of the palatine nerves , with secondary involvement of the pterygopalatine fossa and further retrograde spread along the mandibular nerve [ 9 , 10 , 20 , 23 , 24 , 35 ]  . 
tra gli istotipi pi frequenti , va ricordato il carcinoma ade noideo - cistico con la sua tipica modalit di diffusione perineurale lungo i nervi palatini , con secondario coinvolgimento della fossa pterigo - palatina ed ulteriore diffu sione retrograda lungo il nervo mandibolare [ 9 , 10 , 20 , 23 , 24 , 35 ]  . 
all patients showed disease progression ( with a concurrent reduction in lung volume in two , 40% ) and a progression of honeycombing , with increased number and size of cysts in four ( 80% )  . 
sette pazienti sottoposti a trapianto mono - polmonare sono stati studiati evolutivamente ; di questi 2 ( 28 , 6% ) sono stati esclusi dalla nostra analisi perch deceduti nel post - trapianto , mentre i restanti 5 ( 71 , 4% ) sono stati valutati mediante tomografia computerizzata ( tc ) per 67 , 638 , 56 mesi . 
tutti i pazienti ( 5 / 5 , 100% ) hanno evidenziato un progressione della malattia ( con riduzione consensuale dei volumi polmonari in 2 / 5 , 40% ) e una evoluzione dellhoneycombing ( con incremento numerico e dimensionale delle cisti in 4 / 5 , 80% )  . 
tutte le cisti target sono andate incontro a modificazioni dimensionali ( ingrandimento o riduzione ) con evidenza di complicanze in 3 / 5 pazienti ( 60% ) , quali rottura spontanea con pneumotorace e sviluppo di inclusi ( micetomi )  . 
this behaviour could be explained by the variety of the pathogenetic processes underlying honeycombing , with cysts that may present abnormal communication with the airway , including the development of a check - valve mechanism . keywords follow - up pulmonary fibrosis / pathophysiology cysts uip la tendenza globale del pattern cistico quella dellincremento dimensionale ; le singole cisti , possono per subire un diverso destino , potendo andare incontro ad ingrandimento , riduzione o complicanze . 
ci si spiega in considerazione delleterogeneit dei processi patogenetici alla base dellhoneycombing , con cisti che possono presentare anomale comunicazioni con le vie aeree come lo sviluppo di un meccanismo a valvola . parole chiave follow - up fibrosi polmonare / fisiopatologia cisti uip introduction introduzione idiopathic pulmonary fibrosis ( ipf ) , the pathological and radiological correlate of which is usual interstitial pneumonia ( uip ) , is a progressive pulmonary disease characterised by a diffuse , bilateral , predominantly basal fibrosing pattern . 
 the most common among the idiopathic ips , the disease is refractory to immunosuppressive therapy and is associated with a poor outcome , having a median survival between 2 and 4 years after diagnosis [ 13 ]  . 
in particular , patients with single - lung transplantation offer a unique setting in which to study the evolution of uip in the native lung over a longer period than do nontransplanted patients [ 4 ]  . the purpose of our study was to retrospectively review the natural history of patients treated with single - lung transplantation , with special focus on the morphological and dimensional changes in honeycomb cysts as well as on disease progression . 
in fact , although cysts are a crucial albeit nonspecific finding for the diagnosis of uip , the pathogenesis and evolution of honeycombing remain poorly understood [ 5 ]  . materials and methods study population and image acquisition technique from 2003 to 2006 , single - lung transplantation was performed on seven men , with a mean age at diagnosis of 53.863.93 years , 5 / 7 ( 71.4% ) of whom were smokers and 1 / 7 ( 14.3% ) who had a history of occupational exposure to airborne particulates . 
two of the la fibrosi polmonare idiopatica ( ipf ) , il cui corrispettivo anatomo - patologico e radiologico rappresentato dalla polmonite interstiziale usuale ( uip ) , una patologia polmonare progressiva caratterizzata da un pattern fibrosante diffuso , bilaterale , a prevalente sede basale . 
tale patologia la pi diffusa tra le polmoniti interstiziali idiopatiche , refrattaria alle terapie immunosoppressive e si associa ad una prognosi severa , con una mediana di sopravvivenza compresa tra i 2 e i 4 anni dopo la diagnosi [ 13 ]  . 
 reading and interpretation of images radiological images were independently reviewed with window settings for pulmonary parenchyma and mediastinum by two radiologists with extensive experience in chest radiology and by two radiology residents , who provided a final diagnostic interpretation . 
ct images acquired before 2006 were only available as hard copies , whereas those acquired after 2006 were available on the picture archiving and communication system ( pacs ) workstation . 
to analyse the radiological evolution of the disease , all hard copies of the ct studies obtained before 2006 were digitised with a dedicated scanner equipped with film acquisition software . 
the following parameters were considered : uip severity score : this scoring system , based on akira et al.s method , involves subdividing the two lungs into six zones ( upper , middle and lower , right and left lung ) and assigning to each a score of 0 - 4 depending on the extent of involvement : 0 = none , 1 = < 25% , 2 = 2550% , 3 = 50 - 75% , 4 = > 75% [ 6 ]  . 
at presentation , four out of five patients ( 80% ) had a predominantly microcystic pattern ( cysts < 5 mm )  . cyst size : this was assessed qualitatively and quantitatively by defining a visual score and identifying target cysts . 
 [ 7 ] : 1 = < 2 mm , 2 = 25 mm , 3 = 510 mm , 4 = 1020 mm , 5 = > 20 mthis score was calculated in three different axial planes for each ct examination using the aortic arch , carina and lung bases 2 cm above the right diaphragmatic dome as reference points . 
conversely , target cysts , at least two per patient , were defined as the largest cysts , the measurement of which was most reproducible ; these cysts were assessed for dimensional changes , with measurements taken along the largest axial diameter of the cyst . presso il nostro policlinico nel periodo compreso tra il 2003 e il 2006 . 
la totalit dei pazienti presentava , in linea con la letteratura [ 3 ] , sintomi quali : dispnea ingravescente dopo sforzo minimo , riferita come mancanza di respiro , tosse ed astenia . 
tutti i pazienti allo studio di tomografia computerizzata ( tc ) polmonare mostravano segni radiologici riferibili ad un pattern uip , successivamente confermato dallesame istologico condotto sul pezzo chirurgico del polmone nativo asportato . 
di questi , 2 / 7 ( 28 , 6% ) sono stati esclusi dalla nostra analisi in quanto deceduti un mese circa dopo il trapianto per complicanze infettive ; i restanti 5 / 7 ( 71 , 4% ) sono stati valutati evolutivamente mediante tc per una media di 67 , 638 , 56 mesi . 
 le indagini tc sono state eseguite su tc siemens 6 strati , tc siemens 16 strati ( somatom sensation cardiac 16 , forchheim , germania ) e tc general electric 16 strati ( ge healthcare , fairfield , usa ) senza somministrazione di mezzo di contrasto ( mdc ) , a decubito supino con ricostruzioni a strato sottile , senza sincronizzazione spirometrica e con scansioni cranio - caudali . 
 interpretazione e lettura delle immagini le immagini radiologiche ottenute sono state indipendentemente esaminate , con specifiche finestre per il parenchima polmonare e per il mediastino , da due medici specialisti in radiodiagnostica e nello specifico da un massimo esperto in radiologia toracica con pluriennale esperienza in tale settore e da due medici in formazione in radiodiagnostica , ottenendo una interpretazione diagnostica finale . 
le immagini tc precedenti allanno 2006 erano disponibili esclusivamente su pellicola , mentre per le indagini acquisite a partire dallanno 2006 , la lettura stata condotta sulle workstation picture archiving and communication system ( pacs )  . 
per analizzare levolutivit radiologica della patologia stato necessario scansionare tutti i radiogrammi degli studi tc eseguiti prima del 2006 mediante scanner dedicato con software per pellicole ; attraverso le opportune calibrazioni stato possibile eseguire misurazioni comparative ed ottenere informazioni di tipo quantitativo che hanno permesso il confronto con gli studi successivi disponibili a pacs . 
 [ 6 ] , consiste nella suddivisione dei due polmoni in 6 zone ( superiore , media ed inferiore sia per il polmone destro che per il polmone sinistro ) , assegnando per ciascuno un punteggio da 0 a 4 in base al grado di estensione parenchimale : score 0 ( assente ) , score 1 ( < 25% ) , score 2 ( 25%50% ) , score 3 ( 50%75% ) , score 4 ( > 75% )  . 
quattro pazienti su 5 ( 80% ) presentavano al momento della nostra prima osservazione un patradiol med ( 2013 ) 118 : 4050 measurement of lung volumes and length from apex to base : this measurement was only performed on ct scans acquired after 2006 using dedicated software for quantifying lung capacity of the native lung , with the following parameters : low value - 1 , 024 hu ; high value - 200 hu , mediastinal window without contrast medium and 5 - mm thickness . 
lung volumes were also measured from apex to base of the native lung in a single coronal image using the trachea and bifurcation as reference points , so as to obtain an additional parameter for comparison and confirmation of volume determinations . results four of five patients ( 80% ) died during the study period ; of these , two ( 40% ) died of infectious complications , one ( 20% ) due to onset of carcinoma in the native lung and left maxillary sinus and one ( 20% ) due to kaposis sarcoma . 
 these data were not surprising , as they could be interpreted as complications in patients undergoing aggressive antirejection therapy ; in particular , an increased risk of developing cancer of the native lung has already been reported as a possible effect of immunosuppressive therapy and a history of smoking [ 8 , 9 ]  . 
tale score stato valutato per ogni tc su tre diversi piani in assiale , utilizzando come riferimento larco aortico , la carena e le basi polmonari 2 cm sopra la cupola diaframmatica destra . 
le cisti target , in numero di almeno due per paziente , sono invece state definite dalle cisti di maggiori dimensioni , le cui misurazioni presentavano i caratteri della maggior riproducibilit ; di queste sono state valutate le modificazioni dimensionali , tramite misurazione condotta lungo il diametro massimo della cisti stessa sul piano assiale . misurazione dei volumi polmonari e dellaltezza apicebasi . 
tale calcolo stato eseguito solamente sulle tc acquisite dopo lanno 2006 utilizzando software dedicato per la quantificazione della capacit polmonare del polmone nativo con parametri : low value - 1024 hu ; high value - 200 hu , finestra per il mediastino senza mdc e spessore di 5 minoltre i volumi polmonari sono stati valutati eseguendo una misurazione apice - base del polmone nativo , su una singola immagine coronale orientata , utilizzando come riferimento la trachea e la biforcazione dei bronchi principali , disponendo cos di un ulteriore criterio di comparazione a conferma della quantificazione volumetrica . risultati quattro pazienti su 5 ( 80% ) sono deceduti durante il periodo della nostra osservazione ; in particolare , 2 / 5 ( 40% ) sono deceduti per complicanze infettive , 1 / 5 ( 20% ) per sviluppo di carcinoma sul polmone nativo e a livello del seno mascellare sinistro e 1 / 5 ( 20% ) per sarcoma di kaposi . 
questi dati non ci hanno sorpreso in quanto interpretabili come complicanze in pazienti sottoposti ad un forte regime anti - rigetto ; in particolare , anche un aumentato rischio di sviluppo di tumore polmonare sul polmone nativo era gi stato registrato in letteratura , come possibile conseguenza della terapia immunosoppressiva e dellanamnesi positiva per fumo [ 8 , 9 ]  . 
di questi , in 2 / 5 ( 40% ) si registrata una riduzione dei volumi polmonare , in 3 / 5 ( 40% ) il volume polmonare rimasto invariato ( tabella 1 )  . 
1a , b a 63 - year - old man who underwent single left - lung transplantation ; the right native lung shows a radiological pattern typical of usual interstitial pneumonia . 
a la tc ad alta risoluzione ( hrct ) del polmone destro evidenzia la presenza di honeycombing prevalentemente di tipo micro - cistico ( score visivo ground - glass = 3 ) , a disposizione basale sub - pleurica con diametro massimo delle cisti target ( asterisco ) rispettivamente di 7 , 5 e 6 , 2 mm cui si associano aspetti di fibrosi polmonare . 
b il controllo hrct a 5 anni evidenzia incremento numerico e dimensionale delle cisti ed evoluzione da pattern micro - cistico a macro - cistico ( score visivo ground - glass = 4 ) con dimensioni delle cisti target ( asterisco ) rispettivamente di 16 , 3 e 15 , 3 malcune cisti appaiono complicate dalla presenza di inclusi fungini ( freccia )  . finding of basal - subpleural honeycombing , frequently concentric , with a propensity for progressive involvement of the central and upper parenchymal regions . 
in addition , areas of honeycombing are typically interposed with areas of normal lung and may alternate with small areas of ground - glass attenuation ; to some extent , these findings reflect the spatial and temporal heterogeneity of the histopathological pattern [ 13 , 1013 ]  . the term honeycomb lung ( wabenlunge ) originated in germany in the nineteenth century to indicate congenital abnormalities in bronchial development , associated with the presence of bronchiectasis ; in fact , in the first half of the twentieth century , ipf was not yet established as a welldefined pathological entity , and only occasional reports appeared in which the authors used different terms to describe the cases . 
the third hypothesis centres on bronchiolar stenoses and obliteration : bronchiolar obstruction is correlated with deviation of the air flow through the pores of kohn and the channels of lambert , the outflow of which is limited during expiration by the distorted bronchiolar architecture ( possible check - valve mechanism ) [ 15 ]  . a radiological - pathological analysis by mino et al . 
this study emphasised that in most patients with ipf / uip , ct revealed a dimensional increase of the honeycomb cysts over time and that nei pazienti con pattern radiologico tipico ( circa 50% 70% dei casi ) , il reperto chiave per la diagnosi rappresentato dalla presenza di honeycombing a disposizione basalesubpleurica , frequentemente disposto a strati concentrici , con tendenza al progressivo coinvolgimento delle regioni parenchimali centrali e superiori ; si associano aspetti di fibrosi polmonare , ovvero bronchiectasie da trazione , distorsione dellarchitettura , riduzione dei volumi polmonari e reticoli irregolari . 
 tipicamente , inoltre , le aree di honeycombing si interpongono ad aree di parenchima normale e si possono alternare ad opacit a vetro smerigliato poco estese ; questi reperti riflettono , entro certi limiti , leterogeneit spaziale e temporale del quadro istopatologico [ 13 , 1013 ]  . il termine honeycombing ( wabenlunge ) nacque in germania nel xix secolo per indicare anomalie congenite dello sviluppo bronchiale , associate alla presenza di bronchiecradiol med ( 2013 ) 118 : 4050 fig . 
2a , b a 62 - year old man who underwent single left - lung transplantation ; the right native lung shows a radiological pattern typical of unusual interstitial pneumonia . 
a the native lung shows honeycombing with subpleural and basal distribution , with loss of normal lung architecture ; the larger cyst has a maximum diameter of 16.99 mm ( arrow )  . 
a al polmone destro presenza di honeycombing a disposizione basale sub - pleurica ed aspetti di distorsione del parenchima polmonare con formazione cistica di maggiori dimensioni di 16 , 9 mm ( freccia )  . 
these findings support the view that at the basis of some honeycomb cysts are processes involving bronchiolar stenosis and obliteration that may trigger a check - valve mechanism [ 16 ]  . 
therefore , these results are in line with hepplestons report from 1956 , which identified two types of cysts : small cysts , in free communication with the airways , and larger cysts , for which he hypothesised a check - valve mechanism [ 17 ]  . 
the fact that different pathogenetic factors may be implicated in the formation of honeycomb cysts accounts for the partially conflicting results reported in the literature , with most cysts showing a tendency to decrease in size during expiration ( however , the limited patient population must always be kept in mind ) [ 1820 ]  . considering the limited data available on this subject , our study although retrospective in nature and involving a small number of patients aimed to shed light on honeycombing by analysing both the global tendency of the phenomenon and the evolution of the single cyst . 
this was made possible by the follow - up of patients who underwent single - lung transplantation , a condition that allowed for a considerably longer follow - up period than would have been possible in nontransplanted patients treated with cortisone and immunosuppressive therapy alone . 
 until recently , single - lung transplantation was considered the surgical option of choice , being associated with a tasie ; infatti , fino alla met del xx secolo , la fibrosi polmonare idiopatica non costituiva ancora unentit patologica ben definita e nota , con sporadici case report in cui i singoli autori presentavano , con differente modalit e terminologia , i reperti osservati . 
oggi lhoneycombing viene definito dalla presenza di areole di iperdiafania assoluta ( cisti ) di dimensioni variabili tra i 2 e i 20 mm ( occasionalmente anche superiori ) , con parete fibrosa e chiaramente identificabile e che si associano a completa perdita della architettura normale lobulare - acinare [ 14 ]  . 
la seconda si focalizza sulle bronchiolectasie : i bronchioli non coinvolti nel processo fibrotico , ma adiacenti ad esso , andrebbero incontro ad una dilatazione compensatoria come effetto della trazione inspiratoria cui essi sarebbero sottoposti a livello locale . 
 infine la terza ipotesi si incentra sulle stenosi ed obliterazioni bronchiolari : lostruzione bronchiolare sarebbe infatti correlata ad una deviazione del flusso aereo attraverso i pori di kohn e i canali di lambert , il cui deflusso sarebbe per limitato in espirazione proprio dalla distorta architettura bronchiolare ( possibile meccanismo a valvola ) [ 15 ]  . 
a al polmone destro moderata presenza di honeycombing a disposizione sub - pleurica , aree di ground - glass ed aspetti di fibrosi del parenchima polmonare con presenza voluminosa formazione cistica con diametro maggiore di 6 , 1 cm ( freccia )  . 
b il controllo hrtc a 6 anni evidenzia la scomparsa della formazione cistica in seguito a rottura spontanea ed evidente progressione dellestensione della uip . shorter surgical procedure , less trauma and less risk of ischaemic injury . 
in addition , the restrictive pattern of the native lung seems to promote selective ventilation and perfuradiol med ( 2013 ) 118 : 4050 una valutazione comparativa anatomo - radiologica , come in realt tutti questi meccanismi siano coinvolti nella patogenesi dellhoneycombing . 
tale studio ha evidenziato che nella maggior parte dei pazienti con ipf / uip , le indagini tc mostravano nel tempo un incremento dimensionale delle cisti di honeycombing e che , dal punto di vista istologico , le cisti di maggiori dimensioni si caratterizzavano per anomale comunicazioni con le strutture bronchiolari [ 7 ]  . 
 [ 16 ] , attraverso indagine tc spirale acquisita in inspirium ed espirium , hanno dimostrato che esistono due tipi di cisti : cisti che si riducono in fase di espirazione e cisti , di maggiori dimensioni , che invece non si modificano in espiriuquesti dati sostengono lipotesi che , alla base di alcune cisti di honeycombing , vi siano dei processi di stenosi e obliterazione bronchiolare con linnesco di un meccanismo a valvola [ 16 ]  . 
peraltro tali risultati concordano con quanto riportato da heppleston [ 17 ] gi nel 1956 ; anchegli identificava due tipi di cisti : cisti di piccole dimensioni , in libera comunicazione con le vie aeree e cisti di maggiori dimensioni , per le quali ipotizzava un meccanismo a valvola [ 17 ]  . 
il fatto che nella patogenesi delle cisti di honeycombing possano essere implicati differenti fattori patogenetici , rende ragione del fatto che alcuni autori siano giunti a risultati parzialmente discordanti , registrando come la maggior parte delle cisti abbia una tendenza alla riduzione dimensionale durante la fase di espirazione ( si tenga presente che si tratta comunque di casistiche limitate ) [ 1820 ]  . in considerazione degli esigui e limitati dati disponibili in letteratura al riguardo , il nostro studio sia pure con i limiti di una indagine retrospettiva e della piccola casistica ha lintento di far chiarezza sulla complessit del fenomeno honeycombing , analizzando sia la tendenza globale del fenomeno , che il comportamento evolutivo delle singole cisti . 
questo stato possibile grazie al follow - up dei pazienti sottoposti a trapianto mono - polmonare , condizione che ci ha permesso una osservazione per tempi molto pi lunghi rispetto a quanto non consentirebbe la storia naturale della malattia , in pazienti non trapiantati e trattati esclusivamente con terapia cortisonica e immunosoppressiva . 
 tradizionalmente , il trapianto mono - polmonare era fino a pochi anni fa considerato lopzione chirurgica di scelta , in quanto correlato ad una procedura chirurgica pi breve con minor trauma operatorio e minor rischio di danno ischemico ; peraltro il pattern restrittivo del polmone nativo favorirebbe la ventilazione e perfusione selettiva a carico del polmone trapiantato . 
diversi studi tuttavia hanno suggerito che il trapianto bi - polmonare possa contribuire a ridurre il danno funzionale in caso di complicanze precoci quali danno da riperfusione o rigetto acuto , inoltre questa tecnica sembra essere correlata ad una migliore sopravvivenza a lungo termine [ 21 , 22 ]  . 
however , several studies have suggested that double - lung transplantation may help to reduce functional damage in the case of early complications , such as reperfusion damage or acute rejection ; in addition , it appears to be correlated with better long - term survival rates [ 21 , 22 ]  . 
as a consequence , even though this issue is still under debate also in consideration of the ethical problems concerning the shortage of donors the international society for heart and lung transplantation ( ishlt ) noted a recent increasing use of double - lung transplantation [ 23 ]  . 
in line with this trend , at our hospital , single - lung transplantation has progressively been replaced by double - lung transplantation , in part as a result of the changing profile of patients receiving the transplantation ( more patients with pulmonary hypertension versus patients with ipf )  . 
the follow - up of a group of patients with single - lung transplantation provides a unique and probably unrepeatable opportunity to study the evolution of honeycombing . in conclusion , our results not only confirm that uip progresses despite immunosuppressive treatment and that it is associated with a progressive reduction in lung volumes [ 4 , 2426 ] , but also provide important insights into the natural history of honeycombing . 
honeycombing is therefore a dynamic process , the progression of which is dependent on a number of complex pathogenetic mechanisms . the limitations of our study include the small number of patients , due to the highly selective population considered ; the retrospective design , which entailed comparing ct scans acquired with different technical parameters ; the availability of only hard copies for the earlier ( pre - 2006 ) ct scans ; and the possibility of using dedicated software to calculate lung volumes only on the scans acquired after 2006 . despite these limitations , some considerations can be made regarding the natural history of honeycomb cysts . 
compared with these authors experience , our follow - up period was significantly longer because we monitored the evolution of the radiological features of uip in the native lung of patients who underwent single - lung transplantation and documented the possible complications of the cysts . 
 although the pathogenesis of honeycombing remains unclear , on the basis of our results , we can speculate that numerous mechanisms are implicated , including a checkvalve mechanisour data demonstrate that honeycombing is a dynamic process in which the cystic pattern has an overetici legati alla carenza di donatori , linternational society for heart and lung transplantation ( ishlt ) ha registrato negli ultimi anni sempre un maggiore utilizzo della tecnica del trapianto bi - polmonare [ 23 ]  . 
in accordo con questa tendenza , presso il nostro policlinico stato progressivamente abbandonato il trapianto mono - polmonare a favore del trapianto bi - polmonare , anche in considerazione di un progressivo cambiamento della tipologia di pazienti cui tale trapianto rivolto ( incremento dei trapianti nei pazienti con ipertensione polmonare versus pazienti con fibrosi polmonare idiopatica )  . 
pertanto , il follow - up del gruppo di pazienti sottoposti a trapianto mono - polmonare costituisce una possibilit unica e probabilmente irripetibile per valutare evolutivamente la storia naturale dellhoneycombing . in conclusione , i nostri risultati confermano che la uip progredisce nel tempo nonostante la terapia immunosoppressiva e si associa ad una progressiva riduzione dei volumi polmonari [ 4 , 2426 ] ed offrono importanti spunti di riflessione per quanto concerne levolutivit dellhoneycombing . 
le singole cisti hanno per evidenziato comportamenti molto variabili , potendo andare incontro ad incrementi o riduzioni dimensionali e a complicanze ( rottura con pneumotorace o sviluppo di inclusi fungini )  . 
lhoneycombing costituisce pertanto un processo dinamico , in cui svariati e complessi meccanismi patogenetici sembrerebbero essere coinvolti , con una evoluzione in senso peggiorativo . i limiti del nostro studio riguardano lesigua casistica , dovuta alla selettivit della popolazione in esame , la valutazione retrospettiva dei pazienti stessi con relativo confronto di indagini tc acquisite in parte con parametri tecnici differenti ; lassenza su pacs delle immagini tc precedenti il 2006 , disponibili solo su pellicola ed infine la possibilit di calcolare i volumi polmonari con software dedicato esclusivamente per gli esami eseguito dal 2006 in poi . pur con tali limiti , stato possibile fornire delle considerazioni sulla tendenza evolutiva delle cisti di honeycombing . 
 [ 6 ] rispetto al quale stato da noi eseguito un follow - up nettamente pi lungo , perch abbiamo monitorato levolutivit dei segni radiologici della uip nel polmone nativo in pazienti sottoposti a trapianto mono - polmonare ed inoltre abbiamo documentato possibili complicanze a cui le cisti sono andate incontro . 
 non possiamo esprimerci circa la patogenesi del processo di honeycombing ; in base alle nostre osservazioni , comunque , possiamo ipotizzare che esistano molteplici meccanismi coinvolti , tra cui un meccanismo a valvola . 
i nostri dati dimostrano che lhoneycombing un processo dinamico , in cui la tendenza globale del pattern cistico 50 radiol med ( 2013 ) 118 : 4050 all tendency to increase in size from microto macrocystic ; however , the larger cysts may have a variable progression , with the possible development of complications . 
these results can be explained by considering the different pathogenetic processes responsible for honeycombing , with cysts exhibiting abnormal and variable communications with the airways . verso lincremento dimensionale da microa macrocistico ; le cisti di maggiori dimensioni possono per subire un destino variabile , potendo andare incontro anche a complicanze . 
damasio , via montallegro 4 , 16145 genova , italy , tel . : + 39 - 010 - 5636572 , fax : 39 - 010 - 385599 , e - mail : beatrice.damasio@libero.it received : 31 may 2011 / accepted : 14 july 2011 / published online : 10 february 2012 springer - verlag 2012 abstract purpose . 
we reviewed the clinical and imaging findings [ 30 cdus , five magnetic resonance ( mr ) and one computed tomography ( ct ) examination ] in 30 patients with dkt ( 23 men and seven women ; median age 65 years ; range 55 - 82 )  . 
three patients had graft dysfunction : one had chronic rejection and two had pathologies involving one kidney only ( one encrusted pyeloureteritis of a left graft and one occluded main artery of a left graft )  . 
tre pazienti avevano disfunzione del trapianto : uno con rigetto cronico e due con patologie coinvolgenti un solo rene ( 1 pielonefrite incrostata rene sinistro e 1 occlusione dellarteria renale sinistra )  . 
lusd fornisce utili informazioni nei pazienti con dkt , permettendo il riscontro di anomalie asintomatiche unilaterali non clinicamente sospette ; a livelli comparabili di funzione renale , i pazienti con dkt hanno valori di ri pi alti e volume renale inferiore rispetto ai pazienti con skt . parole chiave trapianto renale donatori marginali reperti allimaging radiol med ( 2013 ) 118 : 1422 introduction although renal transplantation is the treatment of choice for chronic uraemia [ 1 ] , many patients with end - stage renal disease do not receive transplants due to the limited organ supply and increasing demand [ 2 ]  . 
engrafting both kidneys from the same donor to a single recipient is a strategy to provide enough nephron mass to ensure survival , comparable to that of single kidney transplant ( skt ) from ideal donors [ 3 ]  . 
even though ultrasonography ( us ) and colour doppler ( cdus ) are extensively used to assess the structure and function of transplanted kidneys , few data are available on their use in dkt [ 6 ]  . 
we therefore planned this study with the aim of analysing differences , if any , between us imaging and doppler features obtained in dkts compared with those of single ideal grafts . 
us and cdus imaging data [ mean values of left and right lengths , volume and resistive index ( ri ) ] from asymptomatic dkts were compared with data available for 14 patients ( 13 men , one woman ) with skt having similar graft function as estimated by glomerular filtration rate ( gfr ) calculated according to the cockroftgault formula . 
clinical data [ age , months from transplantation , pretransplant dialysis age , donor age , occurrence of delayed graft function ( dgf ) , serum creatinine , and urinary protein excretion rate ] were collected at the time of us evaluation . 
graft survival of all patients was checked at the 2 - year follow - up . kidneys were evaluated by us for dilatation of the pyelocalyceal system and thickening of the urothelial surface . 
renal ri was introduzione sebbene il trapianto di rene costituisca il trattamento di elezione nelluremia [ 1 ] , molti pazienti con insufficienza renale non possono essere sottoposti a trapianto a causa della disparit tra domanda e disponibilit di organi [ 2 ]  . 
il trapianto renale da donatore marginale ( dm ) , includendo anche donatori cadaveri pi anziani , si propone come possibile soluzione a questo problema fornendo un maggiore numero di reni trapiantabili . 
tuttavia i reni dei dm hanno una massa nefronica inferiore , come conseguenza dellinvecchiamento , e / o dellinteressamento dorgano secondario a diabete , ipertensione o a patologia renale intrinseca subclinica . 
il trapianto di entrambi i reni dello stesso donatore a un ricevente unico permette di fornire una massa nefronica adeguata ad assicurare una sopravvivenza dorgano paragonabile a quella del trapianto di rene singolo da donatore ideale [ 3 ]  . 
il trapianto di doppio rene ( dkt ) generalmente riservato a riceventi pi anziani , in accordo con la politica di assegnazione dorgano old - for - old [ 4 ]  . 
nonostante lestensivo utilizzo dellecografia ( us ) e del color doppler nel monitoraggio della morfostruttura e della funzione del rene trapiantato , pochi dati sono al momento disponibili sugli aspetti us e color doppler nel dkt [ 6 ]  . 
scopo di questo lavoro di analizzare leventuale differenza tra aspetti us e color doppler ( usd ) nel dkt a confronto con il trapianto di rene singolo da donatore ideale . materiali e metodi sono stati valutati i reperti usd di 30 pazienti con dkt ( 23 maschi ; 7 femmine ) seguiti presso il nostro centro : 2 pazienti presentavano , al momento dellesame , rialzo dei valori di creatinina e uno recente insorgenza di macroematuria ; i restanti 27 pazienti con dkt erano asintomatici . 
i reperti usd [ valori medi del diametro longitudinale ( dl ) del rene destro e sinistro , volume renale ( vr ) e indice di resistenza ( ri ) ] dei pazienti asintomatici con dkt sono stati confrontati con quelli di 14 pazienti ( 13 maschi , 1 femmina ) con trapianto di rene singolo da donatore ideale ( skt ) con funzione renale [ valore di glomerular filtration rate ( gfr ) , calcolato con formula di cockroft - gault ] comparabile . 
i dati clinici [ et , mesi dal trapianto , et dialitica pre - trapianto , et del donatore , ritardata ripresa funzionale ( dgf ) , creatininemia e proteinuria ] sono stati raccolti al momento della valutazione ecografica . 
la sopravvivenza dorgano di tutti i pazienti stata valutata a 2 anni di follow - up . allesame usd sono stati valutati : la presenza di even16 radiol med ( 2013 ) 118 : 1422 calculated as the mean value of three consecutive samplings at the interlobar level at the upper pole , lower pole and middle third of the kidney . 
a contrast - enhanced magnetic resonance ( mr ) imaging study was requested after us in five cases , and a spiral computed tomography ( ct ) scan without contrast medium was performed in one patient . 
 statistics descriptive statistics are reported in terms of absolute frequencies and percentages for categorical variables and in terms of medians and quartiles ( 1st through 3rd ) for continuous variables , as they were not normally distributed . 
the statistical package statistica ( statsoft corp . , tulsa , ok , usa ) was used for all analyses . results among dkts with worsening graft function , one patient had chronic rejection and one thrombosis of the left renal artery ; the patient with gross haematuria had unilateral encrusted pyeloureteritis . 
in the second patient , who had thrombosis of the left renal artery , us demonstrated asymmetric kidneys with markedly decreased left renal volume and very few intrarenal cdus signals from the affected side . 
us examination of the patient with unilateral encrusted pyeloureteritis showed mild dilatation of the renal pelvis and marked hyperechogenicity of the urothelial surface in the calyces , pelvis and ureter of the left kidney . 
according to clinical transplant data , no patient suffered from dgf , two developed graft failure and one had a functioning graft at follow - up . demographic , clinical and us parameters of asymptomatic dkt patients are reported in table 1 . 
no significant tuale dilatazione pielocaliciale e di ispessimento della parete uroteliale ; lecogenicit parenchimale , che stata considerata normale ( in caso di buona differenziazione corticomidollare , con piramidi relativamente ipoecogene ben identificabili ) o aumentata ( in caso di perdita della normale differenziazione corticomidollare ) ; i diametri renali ed il volume renale ( lunghezzalarghezza spessore0 , 49 )  . 
gli esami usd sono stati condotti come parte del normale monitoraggio periodico post - trapianto . analisi statistica la statistica descrittiva delle variabili categoriche riportata come frequenze assolute e percentuali per le variabili di tipo continuo , che presentavano distribuzione non gaussiana , come mediana e quartile ( 1 e 3 quartile )  . 
la comparazione tra gruppi dei parametri qualitativi stata eseguita con il test esatto di fisher ; mentre la valutazione comparative dei parametri quantitativi con test non parametrico : test - u di mann - whitney . 
per lanalisi statistica stato utilizzato il programma di statistica ( statsoft corp . , tulsa , ok )  . risultati tra i pazienti con dkt con peggioramento della funzione renale uno aveva rigetto cronico e il secondo trombosi della arteria renale di sinistra ; il paziente con macroematuria aveva una pieloureterite incrostata unilaterale . 
 la valutazione us del paziente con pielo - ureterite incrostata unilaterale mostrava lieve dilatazione della pelvi renale con marcata iperecogenicit della superificie uroteliale di calici , radiol med ( 2013 ) 118 : 1422 fig . 
1a - c patient with double kidney transplantation and renal failure due to unilateral thrombosis of the left renal artery : ultrasound ( a , b ) shows asymmetric kidneys , decreased left renal volume ( b ) and very few left intrarenal colour doppler signals ( b )  . 
1a - c paziente con trapianto di doppio rene e insufficienza renale dovuta a trombosi unilaterale della arteria del rene sinistro ; lecografia ( a , b ) mostra reni asimmetrici con ridotto volume del rene sinistro ( b ) e rari segnali vascolari intrarenali ( b ) alla valutazione color doppler . 
1 : at 4 months follow - up the patient developed stenosis of the main artery of the remaining kidney , as confirmed by aliasing at colour doppler ( a ) and high velocity with high resistive index on spectral wave analysis ( b )  . 
2a , b stesso paziente presentato in figura 1 : a 4 mesi di follow - up il paziente svilupp una stenosi dellarteria del rene controlaterale confermata dallaliasing al color doppler ( a ) e dallo spettro ad alta velocit con alto ri ( b )  . 
il rene controlaterale risultava normale , con la sola eccezione di una cisti semplice corticale di 3 cnessuno di questi pazienti aveva presentato dgf , due 18 radiol med ( 2013 ) 118 : 1422 fig . 
3a , b patient with double kidney transplant , gross haematuria and unilateral left encrusted pyeloureteritis : ultrasound examination shows mild dilatation of the renal pelvis and marked hyperechogenicity of the urothelial surface of the left kidney due to calcifications ( a , black arrow )  . 
3a , b paziente con trapianto di doppio rene , macroematuria e pielonefrite incrostata monolaterale sinistra : lesame ecografico mostra una lieve dilatazione della pelvi renale con marcata iperecogenicit della superficie uroteliale del rene sinistro dovuta a calcificazioni ( a , freccia nera )  . 
la tc conferma la presenza di diffuse calcificazioni della superficie uroteliale ( b , freccia bianca )  . table 1 demographic , clinical and ultrasound characteristics of patients with double kidney transplantation ( dkt ) mean median min max lower quartile upper quartile p value sd , standard deviation ; tx , transplantation ; gfr , glomerular filtration rate ; vol . , volume ; ri , resistive index , ns , not significant tabella 1 caratteristiche clinico - demografiche e aspetti eco - color doppler nei pazienti con trapianto di doppio rene ( dkt ) media mediana minimo massimo ds quartile inferiore quartile superiore p age ( years ) months from tx months of dialysis pre tx donor age ( years ) serum creatinine ( mg / dl ) estimated gfr ( ml / min ) proteinuria ( g / l ) vol . 
anomalie unilaterali sono state identificate in 6 casi ( in 3 pazienti ectasia pelvica con modico ispessimento uroteliale , in uno ureterite del tratto terminale delluretere e in due presenza di linfocele )  . 
nessuno dei 27 pazienti asintomatici con dkt ha presentato insufficienza dorgano al follow - up . nei 14 pazienti con skt i reni provenivano da donatori pi giovani in confronto con i dkt , tuttavia let dei riceventi non era significativamente differente tra i due gruppi ( tabella 2 )  . la tabella 3 valuta comparativamente i pazienti asintomatici con dkt verso quelli con skt . 
nei pazienti con dkt , non essendoci differenze significative tra i due reni , stato considerato , nel confronto con i pazienti con skt , il valore medio dei due reni . 
 la valutazione doppler ha mostrato valori di ri > 0 , 8 in 8 / 27 pazienti con dkt asintomatici ; tutti avevano funzione renale stabile al follow - up ; dgf risultava in 1 solo di questi . 
solo 1 / 14 pazienti con skt aveva ri > 0 , 8 al momento dello studio , in assenza di pregressa dgf . discussione lecografia probabilmente la modalit di imaging pi adatta nel monitoraggio del rene trapiantato essendo una tecnica non invasiva , utile nellidentificazione di eventuali complicazioni chirurgiche urologiche e vascolari di frequente riscontro nellimmediato post - trapianto . 
urographic sequence ( 10 min post gadolinium injection ) in the coronal plane : a large lymphocele ( white arrow ) is in close contact with the urinary tract and causes unilateral left hydronephrosis ; the right kidney presents normal urographic phase without hydronephrosis ; the bladder is compressed and dislocated to the right ( black arrow )  . 
4 uro - rm : sequenza urografica dopo somministrazione di mezzo di contrasto ( 10 min dopo somministrazione di gadolinio ) in un piano coronale : un grosso linfocele ( freccia bianca ) appare in contatto con la via urinaria e causa idronefrosi unilaterale sinistra ; il rene destro presenta una normale fase urografica senza idronefrosi . 
none of the 27 asymptomatic patients with dkt had graft failure within the follow - up period . the 14 skt patients received the graft from younger donors than donors for dkt recipients , but recipient age was not significantly different between groups ( table 2 )  . 
only 1 / 14 patients in the skt group had an ri > 0.8 at study entry , without a positive history for dgf . inoltre un eccellente strumento per lidentificazione di eventuali complicanze anche in una fase pi tardiva del posttrapianto [ 7 ]  . 
anche se ben noto lo scarso valore diagnostico dellusd nelle cause mediche di disfunzione precoce dorgano come la necrosi tubulare acuta , il rigetto e la neradiol med ( 2013 ) 118 : 1422 discussion us is probably the most effective imaging technique for evaluating patients with renal transplantation , as it is noninvasive , can detect urological and vascular surgical complications that occur in the early postoperative period and is an excellent tool for identifying complications in the more prolonged follow - up [ 7 ]  . 
although us is not diagnostic for the medical causes of early graft dysfunction , such as acute tubular necrosis , rejection and drug nephrotoxicity all of which require renal biopsy for detection [ 8 , 9 ] serial cdus vascular impedance measurements are the most common method for noninvasive monitoring of kidney grafts . 
however , several important data were obtained with the us study in asymptomatic patients also . in dkt patients , diseases causing severe impairment or even loss of only one of the two grafts are not always followed by return of the patient to dialysis , consistent with report by andres et al . 
 in fact , clinical or laboratory signs of renal impairment were not present in our asymptomatic group of dkts , even in the case in which a unilateral lymphocele caused obstruction of the excretory syste finally , our study showed different us and cdus findings in dkt patients from those in patients receiving kidneys from ideal donors . 
 it is known that ri directly relates to age [ 12 ] and is also correlated with arteriolosclerosis of intrarenal vessels [ 13 ] , but no data exist on volume and ri of dkt kidneys before transplantation . 
other factors , such as recipients age and increased vascular stiffness [ 14 , 15 ] , may explain the increased ri , even though the patients with dkts were not significantly older than those with skts . 
some authors , indeed , suggest that marginal kidneys have greater susceptibility to nephrotoxic effects of cni and that it is necessary to tailor specifically immunosuppressive therapy in dkts [ 16 ]  . frotossicit da farmaci , la cui diagnosi richiede la biopsia renale [ 8 , 9 ] , misurazioni seriali color doppler dellimpedenza vascolare costituiscono la metodica pi comune , non invasiva , per il monitoraggio del rene trapiantato . 
 lusd si dimostrato uno strumento clinicamente utile anche nel nostro gruppo di pazienti con dkt , dal momento che ha permesso di identificare le cause di disfunzione renale in tre pazienti sintomatici ; ha inoltre fornito importanti informazioni anche nei pazienti asintomatici . 
 nei pazienti con dkt infatti una disfunzione anche severa di un solo rene , pur con completa assenza funzionale monolaterale , non sempre accompagnata da perdita funzionale con ripresa della dialisi perch , come riportato da andres et al . 
infatti nel gruppo dei pazienti asintomatici con dkt , non erano presenti segni clinico - laboratoristici di disfunzione dorgano anche nel caso in cui un linfocele unilaterale causava ostruzione monolaterale della trafila urinaria . 
infatti nota la relazione diretta tra ri ed et [ 12 ] e con il grado di arteriolosclerosi dei vasi intrarenali [ 13 ] ; tuttavia non ci sono dati sul volume e sullri dei dkt prima del trapianto . 
altri fattori come let del ricevente e laumentata rigidit delle pareti arteriolari [ 14 , 15 ] potrebbero spiegare lincremento dei valori di ri , anche se , nel nostro studio , i pazienti valutati con dkt non erano significativamente pi anziani dei pazienti con skt . 
alcuni autori suggeriscono che i reni marginali siano maggiormente suscettibili agli effetti nefrotossici dei cni e che pertanto questi pazienti richiedano un adattamento mirato della terapia immunosoppressiva [ 16 ]  . 
 [ 10 ] hanno infatti mostrato come un valore di ri > 0 , 8 sia un fattore prognostico negativo per la sopravvi22 radiol med ( 2013 ) 118 : 1422 knowledge that dkts have ris higher than skts may have clinical implications . 
in our series , we found that 8 / 27 cases of asymptomatic dkt exceeded this ri value , and this was not correlated with graft loss at 2 years . 
then , elevated ri cannot be considered a poor prognostic indicator , at least in dkts , and care should be taken to translate data from skt to dkt patients . venza dorgano e del paziente , anche se tale osservazione non consistente con le osservazioni di altri autori [ 17 ]  . 
 nel nostro studio abbiamo riscontrato valori di ri > 0 , 8 in 8 / 27 pazienti asintomatici con dkt senza evidenza di perdita dorgano a 2 anni di follow - up . 
rummo , via dellangelo 1 , 82100 benevento , italy 2dipartimento di statistica , universit degli studi del sannio , benevento , italy 3radiology department , medical university south carolina ( musc ) , charleston , sc , usa correspondence to : m . 
 lo studio dsc - mr stato ottenuto con uno scanner da 1 , 5 t , monitorando il primo passaggio del mezzo di contrasto con una sequenza t2 - pesata . 
il miglior modello lineare tc = slopemr + errore e fornisce una stima molto significativa dello slope = 1 , 08 ; ci significa che i risultati della tc possono essere previsti dai valori dello studio rm . 
nella nostra popolazione di pazienti la p - tc e la dsc - mr forniscono valori proporzionali di rcbv nella valutazione dei hhg , e possono conseguentemente essere usati in maniera intercambiabile nei gliomi di alto grado cerebrali . parole chiave dynamic susceptibility contrast enhanced mr imaging tc perfusione gliomi di alto grado effetto t1 introduction introduzione a noninvasive evaluation of brain perfusion is possible by dynamic imaging of the transit of an exogenous iodinated or gadolinium - based contrast agent through the brain , i.e. 
notably , previous studies clearly suggest that measurement of relative cerebral blood volume ( cbv ) improves the prediction of glioma grading when compared with conventional mri [ 47 ]  . 
furthermore , the development of advanced antiangiogenic therapies for patients with gliomas requires that neuroimaging provide information on tumour physiology in addition to anatomy [ 8 - 10 ]  . p - ct and dsc - mri have specific and respective differences , advantages and drawbacks . 
 furthermore , in some cases , p - ct has advantages over perfusion mr because of the rapidity , the measure of absolute perfusion values and the wider accessibility compared with perfusion mr , which may not be readily available in some centres . the purpose of this study was to compare cbv measurements in high - grade gliomas ( hgg ) obtained with dscmri and p - ct in the same patient population . la valutazione non invasiva della perfusione cerebrale attualmente possibile attraverso limaging dinamico del transito cerebrale di un mezzo di contrasto esogeno , sia esso iodato o a base di gadolinio , cio con la perfusione in tomografia computerizzata ( p - tc ) o con dynamic susceptibility contrast - enhanced in risonanza magnetica ( dsc - mr )  . 
in tempi pi recenti , invece , c un crescente interesse sulle possibili applicazioni di queste metodiche allimaging dei tumori [ 2 , 3 , 5 , 6 ]  . 
infatti , interessante notare come alcuni studi sottolineino che le misure del volume emati co cerebrale relativo ( rcbv ) migliorino la predizione del grading dei gliomi rispetto allo studio in risonanza ma gnetica ( rm ) convenzionale [ 47 ]  . 
inoltre lo sviluppo di nuove ed avanzate terapie anti - angiogenetiche nei pazienti affetti da glioma richiede al neuroimaging delle informazioni sulla fisiologia tumorale oltre che sullanatomia [ 810 ]  . la p - tc e la dsc - mr presentano delle specifiche differenze , ognuna con i suoi vantaggi e limiti , ma si rileva una carenza di analisi comparative su dati acquisiti con le due metodiche , negli stessi pazienti . 
inoltre , in alcuni casi , la tc potrebbe presentare dei vantaggi rispetto alla rm per la rapidit , la misura assoluta dei valori di perfusione , la pi ampia accessibilit sul territorio rispetto alle tecniche rm in perfusione che possono non essere disponibili i tutti i centri . 
 lobiettivo di questo studio di comparare le misure del rcbv nei gliomi di alto grado ( hgg ) ottenuta con tecnica dsc - mr e p - tc nello stesso gruppo di pazienti . materials and methods materiali e metodi 142 patients at our institution , all patients presenting with a neuroradiological suspicion of brain tumour are studied with conventional mri and dsc - mri . 
by the end of june 2008 , 17 patients ( eight men and nine women , age range 4080 years ) were enrolled underwent brain p - ct and mri . 
fifteen patients were diagnosed with who grade iv glioma and two with grade iii . imaging protocols mri was performed using a 1.5 - t magnet ( signa excite , general electric medical systems , usa )  . 
a localising sagittal t1 - weighted image was obtained , which was followed by nonenhanced axial t1 - weighted fast spin echo ( fse ) , axial and coronal fluid - attenuated inversion recovery ( flair ) and axial t2 - weighted images . 
dsc - mri was performed with a t2 - weighted spin echo ( se ) echo - planar ( ep ) sequence with 13 adjacent 7 - mm - thick sections , 0 gap , 192128 matrix , time to repetition ( tr ) 1900 , time to echo ( te ) 80 . 
the sequence was obtained during infusion of a 0.1 - mmol / kg bolus of gadobutrol ( gadovist , bayer schering , usa ) at a 5 ml / s rate , with 7 s delay , through an 18to 20 - gauge needle cannula , followed by 20 ml saline at the same rate , using a power injector ( medrad spectris mr injector )  . 
after unenhanced ct of the entire brain to localise the region of interest ( roi ) , two adjacent 10 - mmthick sections at the level of the largest tumour diameter were identified . 
p - ct source data were derived from sequential scans obtained in cine mode ( 80 kv , 100 ma , thickness 10 mm , gap 0 ) acquired with a 5 - s delay after i.v. 
administration of 40 ml nonionic contrast medium ( iomeron 350 mg / ml bracco italy ) at 5 ml / s through an 18to 20 - gauge needle cannula , followed by 20 ml saline at the same rate using a radiol med ( 2013 ) 118 : 140151 pazienti nella nostra unit di neuroradiologia tutti i pazienti che si presentano con il sospetto di tumore cerebrale , sono sottoposti di routine a studio rm e dsc - mr . 
da marzo 2006 , stato proposto a tutti i pazienti che presentavano un esame rm e dsc - mr fortemente suggestivo di neoplasia gliale di alto grado , di partecipare allo studio . 
alla fine di giugno 2008 , 17 pazienti ( 8 uomini e 9 donne , con intervallo di et 4080 anni ) hanno accettato di partecipare allo studio e di conseguenza sono stati arruolati , eseguendo la p - tc oltre alla rm . 
 quindici pazienti sono stati diagnosticati stadio iv e due stadio iii . protocolli di imaging lesame rm stato eseguito usando uno scanner da 1 , 5 t ( signa excite , general electric medical systems , usa )  . 
 stata ottenuta per prima unimmagine di localizzazione pesata in t1 , seguita da unassiale t1 fast spin echo senza contrasto , assiale e coronale fluid - attenuated inversion recovery ( flair ) e immagini assiali t2 pesate . 
lo studio dsc - mr stato eseguito usando una sequenza t2 spinecho ( se ) eco - planare , con 13 sezioni adiacenti di 7 mm di spessore , gap = 0 , matrice di 192128 , tempo di ripetizione ( tr ) 1900 , tempo di eco ( te ) 80 , durante linfusione di 0 , 1 mmol / kg in bolo di gadobutrolo ( gadovist , bayer schering , usa ) a 5 ml / s di velocit di iniezione , con 7 secondi di ritardo , attraverso unagocannula di 1820 gauge , seguito da 20 ml di soluzione salina alla stessa velocit , usando un iniettore automatico ( medrad spectris mr injector )  . 
dopo la scansione tc senza contrasto dellintero volume cerebrale per localizzare la regione dinteresse , sono state identificate due sezioni adiacenti di 10 mm di spessore a livello della porzione pi grande del tumore . 
images were acquired at a temporal sampling rate of one image per second , resulting in a series of 45 images for each assessed slice , for a total of 90 images . postprocessing of perfusion data and image analysis acquired p - ct source images were transferred to a workstation ( advantage windows , ge healthcare ) equipped with a commercially available perfusion software package ( ct perfusion version 3 ) for postprocessing of parametric cbv gaps . 
one neuroradiologist ( mds ) then postprocessed data , choosing the arterial input function ( aif ) from the anterior cerebral artery ( aca ) and venous function ( vf ) from the superior sagittal sinus . 
using a deconvolution model , the software then generated colour - coded cbv maps . the acquired dsc - mri source images were evaluated by a dedicated software package ( functool 2 - ge )  . 
a dynamic signal - intensity time curve was generated by placing a single roi over the unaffected contralateral braafter obtaining the signal - intensity time curve , the observer manually selected the pre - enhancement image , i.e. 
 perfusion maps generated from both p - ct and dsc - mri were overlaid on the respective contrast - enhanced source images using an intermediate grade of transparency . from the mr examination , the observer selected the two slices that corresponded with ct study slices . 
on both mri and ct slices , four rois in the area considered to have the maximum cbv value , on the base of the colour scale , were selected . 
we planned to record the maximal abnormality because this method has been demonstrated to provide the highest intraobserver and interobserver reproducibility in perfusion measurements [ 11 ]  . for each patient , three rois were placed in the contralateral normal - appearing white matter , and the mean value was recorded to obtain the normalised cbv values . 
le immagini sono acquisite con un rate di 1 al secondo , con il risultato di 45 immagini per ogni sezione selezionata , per un totale di 90 immagini . post - processing dei dati di perfusione ed analisi delle immagini le immagini acquisite dallo studio p - tc sono state trasferite su una workstation ( advantage windows , ge healthcare ) dotata di un software commerciale ( ct perfusion 3 ) per il post - processing dei dati parametrici delle mappe del volume ematico cerebrale ( cbv )  . 
un neuroradiologo ( mds ) ha processato i dati scegliendo la arterial imput function ( aif ) dallarteria cerebrale anteriore ( aca ) e la funzione venosa ( vf ) dal seno sagittale superiore . 
sono poi state generate delle mappe colorimetriche del cbv usando un modello di deconvoluzione . le immagini sorgente dello studio dsc - mr sono state valutate attraverso un software dedicato ( functool 2 - ge )  . 
 una volta ottenute le curve segnale - tempo losservatore ha scelto manualmente limmagine pre - enhancement , cio lultima immagine prima dellarrivo del bolo di contrasto e limmagine post - enhancement che definisce la fine del passaggio del bolo di contrasto . 
le mappe di perfusione generate dai dati ottenuti con lo studio p - tc e dsc - mr sono state sovrapposte alle rispettive immagini sorgente , usando un grado intermedio di trasparenza . losservatore ha selezionato , a questo punto , due immagini dellesame rm corrispondenti con le due sezioni dellesame tc . 
per minimizzare lerrore , la dimensione delle roi stata mantenuta costante ( 45 mm2 ) ; abbiamo utilizzato delle roi piccole per minimizzare i fenomeni di volume parziale dovuti alleterogeneit del campione . 
tre roi sono state posizionate nella porzione periferica e con impregnazione del tumore , evitando vasi ematici e la corteccia . statistical analysis statistical analysis was performed on the rcbv obtained by p - ct and dsc - mri . 
in the analyses , such an observation was removed from the data sets because : ( a ) it is does not affect the existence of the linear trend between the two measures , ( b ) its presence in the computation can inflate il metodo che ha mostrato la massima riproducibilit sia intrache interosservatore secondo quanto riportato dalla letteratura [ 11 ]  . per ogni paziente 3 roi sono state messe nella sostanza bianca sana controlaterale e il valore medio stato registrato per ottenere dei valori normalizzati di cbv . 
per rendere possibile il confronto abbiamo applicato la medesima procedura sia ai dati ottenuti con dsc - mr che a quelli ottenuti con p - tc . radiol med ( 2013 ) 118 : 140151 analisi statistica lanalisi statistica stata eseguita sui dati di rcbv ottenuti sia dagli studi p - tc che dsc - mr . 
i due gruppi di dati analizzati esprimono i rapporti tra il massimo valore di cbv rapportato a quello della sostanza bianca sana , ottenuti con le metodologie precedentemente descritte , sia nel caso dello studio tc che di quello rm . 
 nellanalisi che presentiamo questo tipo di osservazione stata rimossa per due ordini di motivi , perch non influisce sullesistenza di un trend lineare tra i due gruppi di misure e perch la sua presenza nel computo pu inficiare la variabilit , ridurre lefficienza della stima e la potenza del test . 
il metodo ordinary least squares ( ols ) stato usato per stimare il modello lineare ct = intercetta + slopemr + error ed il modello ct = slopemr + error , che appare il migliore per i dati in studio . 
 nella successiva analisi statistica stata rimossa losservazione n14 dal gruppo di dati perch considerato outlier . il valore medio del rcbv risultato 5 , 561 , 55 per la p - tc e 4 , 921 , 52 per la dsc - mr . 
il test di shapiro - wilks ha dimostrato che entrambi i campioni sono ben approssimati da una distribuzione gaussiana con un valore di p = 0 , 204 per la tc e p = 0 , 389 per la rm . 
nello scatter ( mostrato nella figura 3 dove viene anche mostrata la linea di regressione stimata con il secondo modello descritto di seguito ) , evidente la relazione lineare esistente tra i due gruppi di dati , perci stato testato un modello preliminare di regressione lineare . 
the method of the ordinary least squares ( ols ) was used first to estimate the linear model ct = intercept + slopemr + error , and then the model ct = slopemr + error , which appear to be best for data under study . 
the shapiro - wilks test demonstrated that both samples are well approximated by a gaussian distribution , providing p values of 0.204 for ct and 0.389 for the mri data set . 
given these results , the t 146 radiol med ( 2013 ) 118 : 140151 test for paired data was performed to test the null hypothesis that the two populations had the same mean value . 
 hence , we consider the linear model ct = slopemr + error , in which the estimate of slope is 1.08096 with an associated p value of zero , beyond any reasonable approximation . 
in this case , linear dependence is estimated as mr = 0.91ct , which is also highly statistically significant . discussion neuroimaging plays an integral role in the workup of intracranial tumours , including tumour diagnosis and evaluation of tumour physiology . 
compared perfusion measurements derived using p - ct and dsc - mri in extracranial head and neck tumours and determined that the two modalities may be used interchangeably [ 15 ]  . 
the purpose of our study was to compare rcbv values obtained with p - ct with those from dsc - mri in patients with hgg . p - ct imaging was obtained by monitoring the first pass of iodinated contrast agent bolus through the cerebral vasculature . 
the technique is based on the central volume principle , which relates cerebral blood flow ( cbf ) , cbv and mean transit time ( mtt ) in the following equation : cbf = cbv / mtt [ 3 , 10 , 13 ]  . 
the commercial algorithm we employed uses a deconvolution - based analysis , which requires the operator to place small roi over one artery and one vein to provide input functions [ 1620 ]  . 
di conseguenza consideriamo il modello lineare ct = slopemr + error dove la stima dello slope 1 , 08096 con un valore associato di p = 0 , al di l di ogni ragionevole approssimazione . 
la stima dei residui del modello appare normale , infatti il test di shapiro - wilks per la normalit non rifiuta lipotesi nulla ( p = 0 , 7168 )  . 
in questo secondo caso la stima della dipendenza lineare rm = 0 , 91tc che analogamente altamente statisticamente significativa . discussione limaging neuro - radiologico riveste un ruolo cruciale nella diagnosi di tumore cerebrale e nella valutazione della fisiologia tumorale . 
lobiettivo del nostro studio stato di comparare i valori di rcbv ottenuti con la p - tc con quelli ottenuti con dsc - mr in pazienti affetti da hgg . lo studio p - tc stato ottenuto attraverso il monitoraggio del primo passaggio di mezzo di contrasto attraverso i vasi cerebrali . 
la tecnica si basa sul principio del volume centrale che mette in relazione il flusso ematico cerebrale ( cbf ) , il cbv e il tempo di transito medio ( mtt ) nella seguente equazione : cbf = cbv / mtt [ 3 , 10 , 13 ]  . 
lalgoritmo commerciale di cui ci siamo serviti , si basa sul modello della deconvoluzione , che richiede alloperatore di posizionare una piccola roi su unarteria e una su una vena per dare le funzioni di input [ 1620 ]  . 
 questo metodo ha il vantaggio di dare delle misure quantitative dei parametri di emodinamica . lapproccio rm usa principalmente 3 tipi di tecniche per misurare la perfusione [ 21 ] tra cui limpiego di traccianti esogeni come mezzi di contrasto paramagnetici o traccianti endogeni , come il sangue marcato magneticamente [ 22 ]  . 
la seconda opzione prevede limaging rapido del primo passaggio di mezzi di contrasto a base di gadolinio eseguito mediante sequenze pesate in t1 e in t2 o t2 *  . 
in questo studio abbiamo scelto un approccio basato sugli effetti della suscettibilit magnetica radiol med ( 2013 ) 118 : 140151 the mri approach uses mainly three different techniques to measure tissue perfusion [ 21 ] , including exogenous tracer agents , such as paramagnetic contrast material ; and endogenous tracer agents , such as magnetically labelled blood [ 22 ]  . 
the latter are based on rapid imaging of the first pass of gadolinium - based contrast material and can be performed using either t1 - weighted and t2 or t2 * - weighted technique . 
as p - ct gives a quantitative estimation of cbv but dsc - mri does not , we chose a white matter roi as an internal standard to by which to normalise cbv values and make comparison possible . 
hence , cbv values were obtained from the ratio between the maximum cbv value measured within the tumour ( avoiding the cortical portion of the tumour and the vessels ) compared with the cbv of the contralateral normal - appearing white matter . 
it is generally not possible to place the roi exactly in the same tumour region , because slice thickness , matrix and slice angulation of mri and ct studies are different . 
however , the purpose of this study was to demonstrate that , given the correct application of the protocols for analysing ct and mr images , numerical results obtained with the two methods are linearly dependent for the same patient . 
dal momento che la p - tc fornisce una stima quantitativa del cbv mentre la dsc - mr no , abbiamo scelto una roi nella sostanza bianca come standard interno per normalizzare il cbv e rendere possibile il confronto . 
di conseguenza i valori di cbv sono stati ottenuti come rapporti tra il massimo cbv misurato nel tumore ( evitando la porzione corticale e i vasi ) comparato con il cbv della sostanza bianca sana controlaterale . 
evidente che non possibile posizionare le roi esattamente nello stesso punto del tumore , a causa del diverso spessore di strato , della matrice e dellangolazione diversa tra tc e rm . 
comunque lobiettivo di questo studio dimostrare che , data la corretta esecuzione dei protocolli di analisi delle immagini tc e rm , i risultati ottenuti con le due metodiche sono linearmente dipendenti nello stesso paziente . 
nel nostro campione tale differenza appariva essere inferiore nei tumori che presentavano poco e nessun enhancement dopo somministrazione di mezzo di contrasto [ cio con poca o nulla rottura della barriera emato - encefalica ( bee ) ]  . 
una possibile spiegazione di tale fenomeno che nelle regioni di severa rottura della bee , lo stravaso interstiziale di mezzo di contrasto causa un accorciamento del t1 con una conseguente riduzione della perdita di segnale misurata in t2 . 
infatti lalterata permeabilit delle aree con danno di barriera comporta uno stravaso di contrasto nellinterstizio che porta il segnale sopra la linea di base per un effetto di accorciamento del t1 dovuto al contrasto paramagnetico . 
ci interpretato dallalgoritmo come un volume ematico negativo e viene 148 radiol med ( 2013 ) 118 : 140151 tion of this phenomenon is that in regions of severe bbb breakdown , the interstitial extravasation of contrast medium causes a t1 shortening , leading to a decrease in measured t2 signal loss induced by intravascular contrast agent . 
in fact , the high permeability of the impaired areas leads to extravasation of contrast material into the interstitium , which increases the signal above the baseline due to the t1 shortening effect of paramagnetic contrast mediuthis is interpreted by the algorithm as negative blood volume and is subtracted from the positive blood volume , which is represented by the t2 signal drop . 
in addition , the decreased concentration gradient between intraand extravascular compartments caused by contrast leakage in situations of severe disruption or absence of bbb might contribute to inaccurate estimation of rcbv measurements . 
another possible approach is to use a gradient - echo ( ge ) echo - planar ( ep ) sequence with small flip angle and long tr to reduce sensitivity to t1 contamination ; it is also possible to use non - gadolinium - based contrast material , which is characterised by stronger t2 / t2 * effects and negligible t1 effects compared with gadoliniu however , spampinato et al . 
compared rcbv values derived from two consecutive dsc - mri studies and demonstrated that predose gadolinium administration was not efficient for compensating for the underestimation of intratumoural rcbv due to the t1 shortening effect [ 28 ]  . 
in our study we did not administer a gadolinium predose before measuring the first pass of contrast medium , and this is probably why rcbv values measured with mri were lower , on average , compared with ct . 
this seems consistent with results obtained with p - ct and dsc - mri in the evaluation of squamous cell carcinoma of the upper aerodigestive tract [ 15 ]  . sottratto al volume positivo rappresentato dalla perdita di segnale t2 . 
in aggiunta il ridotto gradiente di concentrazione tra compartimento intraed extra - vascolare , causato della perdita di contrasto che si verifica in situazioni di rottura della bee , pu contribuire ad una stima inaccurata della misura del rcbv . 
 [ 28 ] , recentemente , hanno comparato i valori di rcbv derivati da due studi consecutivi dsc - mr , dimostrando che la somministrazione di una predose di gadolinio non un modo efficace di compensare la sottostima del rcbv intra - tumorale dovuta allaccorciamento del t1 [ 28 ]  . 
nel nostro studio abbiamo scelto di non somministrare una predose di gadolinio prima dello studio di perfusione e questa probabilmente la ragione per cui i valori di rcbv misurati con la dscmr sono in media pi bassi di quelli misurati con le p - tc . 
i coefficienti 1 , 08 e 0 , 91 sono approssimativamente luno il reciproco dellaltro ( la differenza dovuta ad un errore di arrotondamento durante il calcolo della stima )  . 
ci sembra in linea con i risultati ottenuti nei carcinomi squamocellulari dellalto tratto digestivo con p - tc e dsc - mr [ 15 ]  . la rm resta la modalit di scelta nella valutazione dei tumori cerebrali per la sua elevata sensibilit e capacit di delineare il dettaglio anatomico . 
 limaging dsc - mr pu essere realizzato sia sfruttando radiol med ( 2013 ) 118 : 140151 mri is the imaging modality of choice for assessing brain tumour because of its high sensitivity and exquisite delineation of anatomical relationships . 
a potential limitation of dsc - mri occurs in the case of bbb damage . dsc - mr perfusion imaging can be performed using either a ge or se - ep sequence [ 29 ]  . 
however , although se sequences are less sensitive than ge to susceptibility artefacts , perfusion imaging is based on a very fast mri technique , epi , which allows imaging of rapidly changing physiological processes , such as blood flow . 
due to the lack of radio frequency refocusing pulses , epi sequences are extremely sensitive to off - resonance effects and to structures or lesions that induce strong magnetic field inhomogeneity , such as blood products , calcium , melanin , metals or lesions near brain - bone - air interface , as in the middle and anterior cranial fossa . 
moreover , patients with hgg may have a very poor performance status and consequently poor compliance , and therefore require a more rapid examination , such as p - ct , to establish the diagnosis and possibly guide the biopsy . 
obviously , p - ct plays an important role in all patients with implanted electronic devices , metallic prostheses , drug - infusion pumps and all the other conditions that contraindicate mr examination . p - ct is characterised by high spatial resolution and the absence of susceptibility artefacts . 
furthermore , p - ct is relatively inexpensive and widely accessible and might allow evaluation of multiple perfusion parameters , such as permeability and mean transit time , with a single acquisition . 
on the other hand , exposure to ionising radiation , use of iodinated contrast media which are potentially nephrotoxic and allergenic and limited anatomical coverage , are important limitations of this technique . 
however , strong correlation found in this population of hgg patients studied in a single institution , which allows us to state that there is no difference , on average , when the perfusion study is performed using dscmri or p - ct . 
invece , le sequenze se sono meno influenzate da artefatti di suscettivit e sono pi sensibili ai cambiamenti che genera il mezzo di contrasto paramagnetico passando attraverso piccoli vasi e capillari . 
 in realt anche se le sequenze se sono meno sensibili agli artefatti da suscettivit rispetto alle ge , limaging di perfusione si basa su tecniche di risonanza magnetica molto veloci , le epi , che consentono limaging di processi fisiologici molto veloci , come il flusso ematico . 
a causa dellassenza di un impulso di rifocalizzazione , le epi sono molto sensibili agli effetti off - resonance e a quelle strutture o lesioni che inducono forte inomogeneit del campo magnetico , come i prodotti di degradazione dellemoglobina , calcio , melanina , metalli o lesioni prossime allinterfaccia aria - ossoencefalo , come accade in fossa cranica media ed anteriore . 
ci significa che quando c una grossa quantit di questi artefatti , la dsc - mr non riesce a fornire informazioni significative e la p - tc potrebbe essere pi indicata . 
 inoltre i pazienti affetti da hhg possono essere in cattive condizioni cliniche e per questo motivo avere poca compliance e richiedere un esame pi rapido come la p - tc che guidi la diagnosi ed eventualmente la biopsia . 
ovviamente la p - tc trova spazio importante anche in quei pazienti con device elettronici , protesi metalliche , pompe di infusione di farmaci e tutte le altre condizioni che controindicato la rm . 
comunque la forte correlazione trovata in questa popolazione di pazienti affetti da hgg , studiati in un unico centro , consente di affermare che non vi differenza in media , quando la perfusione viene eseguita usando la dsc - mr e la p - tc . 
le due tecniche pertanto possono essere ritenute equivalenti nella valutazione del rcbv nei gliomi di alto grado . conclusioni in conclusione , per quanto noto , questo il primo studio 150 conclusions to the best our knowledge , this is the first study to compare perfusion measurements using p - ct and dsc - mri in patients affected by hgg . 
 the larger anatomical coverage of mri , together with the possibility of combining information obtained from other advanced techniques , clearly makes mri the first choice in the workup of intracranial brain tumours . 
however , when dsc - mri fails to provide meaningful information due to the large amount of susceptibility artefacts , when poor patient compliance requires a more rapid examination , in all cases of absolute contraindications to mri or in centres in which perfusion mri is not available , p - ct might be used as well . 
data reported in this study require validation in a larger sample of patients . radiol med ( 2013 ) 118 : 140151 che confronta i valori di cbv ottenuti con tecnica p - tc e dsc - mr , negli stessi pazienti affetti da hgg . 
indubbiamente , la maggiore copertura anatomica della rm , insieme alla possibilit di ottenere ulteriori informazioni diagnostiche dalla integrazione con altre tecniche di imaging avanzato ( diffusione , spettroscopia , ecc . ) , rendono la rm e la dsc - mr le tecniche di scelta nello studio standard dei tumori cerebrali . 
tuttavia , nei casi in cui la dsc - mr non fornisca informazioni soddisfacenti , a causa degli artefatti da suscettibilit magnetica o nei casi in cui la scarsa compliance del paziente richieda un esame pi rapido , nonch in tutti i casi di controindicazione assoluta alla rm o quando il centro diagnostico non disponga della dsc - mr , la p - tc pu essere usata in sostituzione . 
du pr leclerq , 59037 lille , france 2uc cardiologia interventistica , ospedale san salvatore , pesaro , italy 3dpartement de radiologie , chu caremeau , 30029 nmes cedex 9 , france 4department of cardiothoracic surgery , falk cardiovascular research center , 300 pasteur drive , stanford , ca 94305 - 5407 , usa 5service de radiologie , hopital rangueil , 1 av jean - poulhes , 31059 toulouse , france correspondence to : m . 
endovascular therapy has taken a predominant role in the therapeutic management of malperfusion syndrome with aortic fenestration , peripheral stenting and stent - grafting , all of which are procedures within the domain of expertise of current interventional radiologists . 
the purpose of this editorial is to present a when , what and how - to guide for all radiologists who encounter complicated aortic dissection . keywords aortic dissection malperfusion stent - graft fenestration riassunto la sindrome da malperfusione una complicanza della dissezione aortica ( dao ) caratterizzata da un insufficiente apporto ematico a uno o pi territori e risultante in una disfunzione dellorgano irrorato . 
lanalisi del radiologo mirata a riconoscere pi elementi : la presenza di complicanze identificabili allimaging ( segni imminenti di rottura aortica ) , lanatomia della dissezione ( presenza e localizzazione dei fori o porte dingresso e di rientro , estensione , diametri aortici ) , il meccanismo specifico di malperfusione . 
la terapia endovascolare , in cui il radiologo diviene attore , ha assunto oggi un ruolo predominante , al pari e forse pi della chirurgia , nei pazienti con dissezione aortica complicata da sindrome di malperfusione , sia in caso di dissezione di tipo a che di tipo b . 
la fenestrazione , lo stenting periferico e limpianto di endoprotesi rappresentano il culmine di un ragionamento clinico e radiologico specifico per ogni singolo paziente e contesto , acuto e cronico . 
 questo articolo si propone di presentare un quadro della problematica data dalla sindrome da malperfusione , radiol med ( 2013 ) 118 : 7488 introduction introduzione cercando di fornire una guida alluso per il radiologo che si trovi di fronte a questo tipo di situazione . parole chiave dissezione aortica malperfusione stentgraft fenestrazione la tavola rotonda sullaorta toracica tenutasi a verona lo scorso giugno durante il congresso della societ italiana di radiologia medica ( sirm ) stata unoccasione decisamente proficua da una parte per lattualit dei temi proposti , dallaltra , e forse di pi , per la partecipazione attiva dei radiologi presenti alla discussione finale . 
cosa fare ? il collega , con questo caso clinico , proponeva la discussione su un argomento difficile ma ben preciso , che sfortunatamente non ha potuto essere esaurito per il termine della sessione . 
la sindrome da malperfusione una complicanza della dissezione aortica e si riscontra in una percentuale dei pazienti compresa fra il 25% e il 50% ( nelle dissezioni di tipo a circa 1 / 3 dei soggetti ) [ 1 , 2 ]  . 
questo articolo si propone di affrontare dunque il tema , cercando di presentare un quadro riassuntivo , ma completo , che possa servire come when , what and how to do per il radiologo che si trovi di fronte a questo tipo di situazione . 
un aspetto fondamentale verr sottolineato : la sindrome da malperfusione un problema clinico , nella cui gestione entrano mezzi diagnostici e terapeutici anche , e oggi sempre pi , radiologici . definizione la sindrome da malperfusione , in pubmed nota come malperfusion syndrome , una complicanza della dissezione aortica caratterizzata da un insufficiente apporto ematico ( ischemia ) a uno o pi territori definiti end - organs e risultante in una disfunzione dellorgano irrorato . quali sono questi territori e come orientarsi verso la presenza di una malperfusione ? ripercorrendo tutta laorta , dalla valvola alla biforcazione iliaca : miocardio , per il coinvolgimento delle coronarie : si configura un quadro di ischemia miocardica , dal dolore anginoso , alle alterazioni dellelettro - cardiogramma ( ecg ) , allinfarto ; encefalo , per il coinvolgimento di uno o pi tronchi sopraaortici : la sintomatologia neurologica varia dallalterazione dello stato mentale allattacco ischemico transitorio ( tia ) / ictus ; midollo spinale : paraplegia ; intestino , per il coinvolgimento di una o pi arterie diat the last congress of the italian society of radiology ( sirm ) , rossella fattori chaired a session focused on thoracic aortic diseases . 
 malperfusion syndrome is a complication of aortic dissection encountered in 2550% of patients ( and in around one third of patients with type a dissection ) [ 1 , 2 ]  . 
the purpose of this article is to present a practical how - to guide for all radiologists who may be faced with malperfusion syndrome in the course of clinically managing patients with complicated aortic dissection . 
special attention is directed to the definition of particular clinical scenarios that represent the more common manifestations of branch - vessel involvement . definition malperfusion syndrome is a complication of aortic dissection defined as end - organ ischaemia caused by branchvessel involvement and resulting in clinical symptoms and functional impairment in a wide range of arterial beds that spans a spectrum between mild dysfunction to tissue necrosis , resulting in organ damage as specified below : heart , for involvement of coronary arteries , with consequent electrocardiogram ( ecg ) alterations , myocardial necrosis ; brain , for implication of supra - aortic vessels , with various clinical presentations reproducing ischaemic patterns ; spine , with consequent paraplegia ; bowel , for digestive - trunk implication , causing mesenteric ischaemia scenarios and relative symptomatology and biological patterns ( lactate dehydrogenase elevation ) ; kidneys , with settings of renal insufficiency and severe refractory hypertension ; in chronic cases , renal atrophy ; lower limbs , with absence of peripheral pulses and findings of lower - limb acute ischaemia ; in chronic cases , claudication . early clinical recognition is critical , and radiological findings are key for establishing diagnostic confirmation and treatment planning . 
patients with uncomplicated aortic dissections confined to the descending thoracic aorta ( stanford type b or debakey type iii ) are currently treated with medical therapy but recently have been considered candidates for endovascular therapy [ 7 ]  . radiological anatomy of malperfusion syndrome williams et al . 
un parametro ematochimico importante lelevazione della lattico deidrogenasi ( ldh ) ; reni : insorgenza di insufficienza renale acuta o ipertensione severa resistente a terapia ; nei casi cronici , peggioramento della funzionalit renale , atrofia parenchimale ; arti inferiori : perdita dei polsi , segni di ischemia periferica ; nei casi cronici , claudicatio . la diagnosi necessariamente clinica e i rilievi radiologici assumono un ruolo di conferma ed entrano nella pianificazione della terapia . 
la presenza di una malperfusione rientra in una serie di parametri che definisce la dissezione complicata versus non complicata , un concetto che sta superando , o quantomeno affiancandosi , alle pi conosciute classificazioni di de bakey prima e di stanford successivamente . 
a prescindere dal tipo anatomico di dissezione , infatti , una dissezione complicata caratterizzata dalla presenza di una o pi delle seguenti evenienze : instabilit emodinamica ( ipotensione / shock , ipertensione resistente alla terapia medica ) ; segni radiologici / clinici di imminente rottura aortica ; sindrome da malperfusione . la presenza di uno di questi elementi richiede il trattamento in urgenza ed evolve il concetto derivato dalla classificazione di stanford secondo cui : dissezione di tipo a ( coinvolgimento dellaorta ascendente ) = chirurgia ; dissezione di tipo b ( a valle dellarteria succlavia sinistra ) = terapia medica . 
la mortalit in - hospital secondo i dati irad del 9 , 6% , 32 , 1% e 6 , 5% per i pazienti trattati rispettivamante con terapia medica , chirurgia e tecniche endovascolari [ 5 ]  . 
un dato interessante che un terzo dei pazienti presentava complicanze ( malperfusione , instabilit emodinamica ) , e che il trattamento chirurgico comportava una mortalit sensibilmente maggiore rispetto alla terapia endovascolare in questo gruppo radiol med ( 2013 ) 118 : 7488 fig . 
2a - c static obstruction of the left renal artery : a ct axial image showing extension of the flap into the renal artery with stenosis ( arrow ) of the true lumen . 
2a - c occlusione statica di arteria renale sinistra , immagine angio - tc assiale ( a ) : la stenosi ( freccia ) determinata dallestensione del flap di dissezione attraverso lostio con conseguente propagazione del falso lume nellarteria viscerale ( tl , vero lume ; fl , falso lume )  . 
in b ricostruzione al disegno del trattamento tramite stenting dopo cateterismo selettivo dellarteria renale , e in c controllo angio - tc , immagine coronale ( multi - planar reconstruction , mpr )  . 
this mechanism , called tirement ostiale in the french literature , corresponding to compression of the true lumen caused by false lumen overpressure associated with extension of the flap into the visceral artery . 
questo tipo di meccanismo , conosciuto nella letteratura specialistica francese con il nome di etirement ostiale , generato da una componente dinamica di iperpressione nel falso lume ed allo stesso tempo dallocclusione statica dovuta allestensione del flap nellarteria collaterale ( t , vero lume ; f , falso lume )  . 
a paper in radiographics based on 64 - detector - row computed tomography ( ct ) recommends ecg - gated acquisition as the standard technique for suspected aortic dissection [ 13 ]  . 
in our experience with a 64row scanner and according to further evidence [ 1416 ] , a ct angiography study of the entire aorta , from the lung apices to the groin , is recommended . 
i pazienti con dissezione di tipo b confinata allaorta discendente ( stanford b ) non complicata sono attualmente trattati con terapia medica , anche se alcuni studi sono in corso per valutare lopportunit di proporre un trattamento endovascolare in questi casi [ 7 ]  . 
il radiologo devessere in grado di definire lanatomia della dissezione identificandone lestensione ( classificazioni anatomiche di stanford , pi attuale , o di de bakey ) , la localizzazione dei fori dingresso ( o porta dentrata , in letteratura anglosassone entry tear ) e di rientro ( re - entry tears ) , e lesistenza di complicanze ( segni di rottura , malperfusione )  . 
allelegante lavoro di williams e lee pubblicato su radiology ormai pi di dieci anni fa [ 8 ] si deve la sistematizzazione dellanatomia radiologica della sindrome da malperfusione ed in particolare dei meccanismi di occlusione delle arterie viscerali ( branch - vessels )  . 
tuttavia , a causa dellequilibrio emodinamico che si stabilisce fra il vero e il falso lume , lo stesso flap spinto durante i movimenti sisto - diastolici contro gli osti viscerali provocandone locclusione ; radiol med ( 2013 ) 118 : 7488 fig . 
la discontinuit fra il lume aortico e quello della collaterale dovuto a un vero e proprio strappamento dellintima con flap residuo nellarteria che crea la stenosi , come si vede nellimmagine angiografica b centrata sullarteria renale sinistra . 
anche in questo caso il trattamento risiede nel cateterismo selettivo dal vero lume aortico al vero lume della branca viscerale per poi procedere ad uno stenting a ponte fra i due per ristabilire la continuit ( schematizzato nel disegno , c )  . dilatation in patients with type b dissection [ 17 ]  . 
in that 2007 report , published in new england journal of medicine , some conceptual models of risk according to the status of false lumen were hypothesised : patients with patent proximal and patent distal re - entry tears have an absence of thrombus in the false lumen , with systolic , diastolic and mean arterial pressures similar to true lumen valves . 
in cases with a patent proximal entry tear and occluded reentry tears , the diastolic and mean pressures in the blind sac exceed the same recordings in the true lumen . 
il ruolo predominante nello studio della dissezione aortica , se non altro in fase acuta , svolto dalla tc , per le note ragioni di disponibilit dellapparecchiatura , di tempi di acquisizione dellesame e ancora oggi di risoluzione spaziale delle immagini . 
una recente pubblicazione sullargomento [ 13 ] concentra lattenzione sulle apparecchiature multistrato a 64 detettori e raccomanda di eseguire uno studio con gating cardiaco in caso di sospetto diagnostico di dissezione , ma non approfondisce come completare il protocollo per lesplorazione dellaorta addominale e della perfusione dorgano . 
nella nostra esperienza , sulla base anche di evidenze gi apparse in letteratura [ 1416 ] importante eseguire un esame angio - tc ( fase quindi arteriosa ) dalla base del collo alle teste femorali e completare lesame con una fase pi tardiva . 
lesame viene completato con una fase pi tardiva , acquisita con un ritardo di 90120 secondi dalliniezione , sempre su tutta laorta , mirata al riconoscimento di una perfusione a flusso lento del falso lume . 
in effetti , lo stato di perfusione del falso lume stato recentemente proposto come fattore prognostico negativo nel follow - up dei pazienti che divengono portatori di dissezione cronica [ 17 ]  . 
in questo lavoro apparso su new england journal of medicine nel 2007 [ 17 ] , di impronta osservazionale , gli autori propongono anche due ipotesi patogenetiche : la prima sarebbe basata essenzialmente su fattori emodinamici , per cui nei pazienti con trombosi parziale del falso lume a causa della presenfig . 
5 dissezione aortica di tipo a con malperfusione viscerale , renale e digestiva , da meccanismo dinamico : immagine angio - tc , assiale , a livello dellemergenza dellarteria renale destra ( freccia ) , che appare non opacizzata . 
le punte di freccia indicano la differenza di enhancement corticale renale con rene destro chiaramente ipoperfuso . the liver and spleen : in the case of coeliac trunk involvement ; the bowel : in the case of superior mesenteric artery involvement . the vascular and organ - specific radiological findings suggesting malperfusion should be interpreted in the light of the clinical context that guides the diagnosis and patient management . acute aortic dissection complicated noncomplicated malperfusion rupture cardiac complications preventive therapy dynamic obstruction static obstruction type a dissection type b dissection fenestration stenting stentgraft whether type a : preventive therapy surgery + medical therapy medical therapy stentgraft fig . 
 acute aortic dissection ( diagnosis within 15 days from symptom onset ) the first - line approach is a complete clinical evaluation that must focus on identifying evidence of a complicated dissection ; all treatments will be directed at managing complications . 
ct study is crucial for treatment planning , as detailed below : a dynamic obstruction can be managed by two distinct endovascular solutions : coverage of the entry tear by thoracic endovascular aortic repair ( tevar ) , especially if malperfusion is associated with findings of rupture , runoff , impending rupture and / or creation of a greater false lumen outflow by fenestrating the intimal flap [ 18 ] ; a static obstruction or ostial disconnection is more amenable to focal treatment of the malperfused branch by peripheral stenting ( ostial or as bridge to the true lumen ) ; a mixed mechanism of obstruction is usually managed by coverage of the entry tear , followed by stenting of the affected branch . an important issue is the timing of interventions for treating dissection complicated by visceral malperfusion . 
 several therapeutic options exist for this condition , and the radiologist can become the main player . za di un foro dingresso ma non di uscita si osserverebbero dei valori medi e diastolici di pressione pi elevati rispetto ai pazienti con falso lume completamente permeabile ( presenza di una porta dentrata e di uscita ) e a quelli con falso lume interamente trombizzato ( onda pressoria pressocch inesistente )  . 
la seconda ipotesi propone invece la trombosi come fattore di indebolimento della parete a causa dellinfiammazione locale e della neovascolarizzazione , come gi avanzato negli aneurismi addominali . parallelamente allo studio dellanatomia vascolare , condotto secondo questi criteri , devono essere ricercati i segni radiologici di uneventuale ipoperfusione dorgano con unattenta analisi di entrambe le fasi acquisite . 
nello specifico : la presenza di un meccanismo dinamico orienta a due soluzioni : la chiusura del foro dingresso tramite endoprotesi ( stent - graft ) ; la creazione di un foro di rientro . 
 con la prima soluzione , indicata in particolare quando sia presente il rischio di rottura aortica , il trattamento si propone di ridirigere il flusso nel vero lume per favorirne la riespansione e allo stesso tempo indurre una trombosi del falso ; la seconda soluzione , come vedremo in seguito realizzabile con una procedura di fenestrazione del flap intimale , mira a riequlibrare il gradiente emodinamico fra i due lumi favorendo il flusso ematico di uscita dal falso per detenderlo e ristabilire una buona perfusione del vero [ 18 ] ; la presenza di un meccanismo di tipo statico o di una disconnessione ostiale indica piuttosto un trattamento isolato della malperfusione tramite stenting della branca viscerale allostio o a ponte fra il vero lume aortico e il vero lume della collaterale ; in caso di meccanismo misto , statico e dinamico insieme , di solito conveniente cominciare con la copertura del foro dingresso e completare con uno stenting della branca coinvolta . argomento importante la tempistica degli interventi rientranti nelliter terapeutico di una dissezione complicata da malperfusione viscerale . 
 alcuni gruppi hanno avanzato la possibilit di un cam biamento di questo atteggiamento a favore di una filosofia che privilegi le tecniche endovascolari di risoluzione della malperfusione posticipando la riparazione chirurgica dellaorta ascendente [ 19 , 20 ]  . 
questo tipo di strategia terapeutica implica la presenza di un team di radiologi vascolari interventisti che possano svolgere tali procedure in tempi ragionevoli per poi poter indirizzare il paziente al blocco operatorio ed effettuare la sostituzione dellaorta fig . 
classical management of this situation recommends immediate surgery to replace the ascending aorta ; some reports support a delayed surgical repair in favour of early treatment of malperfusion by endovascular fenestration . 
8 ricostruzione al disegno di dissezione aortica di tipo a con foro dingresso sullaorta ascendente ( asterisco ) e foro di rientro ( uscita , outgate ) sulla biforcazione iliaca . 
this type of strategy implies the presence of a team of interventional vascular radiologists able to perform the procedure in a reasonable timeframe before sending the patient to the operating room for replacement of the ascending aorta . 
a type b dissection associated with malperfusion syndrome caused by a dynamic mechanism is typically managed by one of two interventional procedures : radiol med ( 2013 ) 118 : 7488 fig . 
9a type b aortic dissection with entry tear just below the origin of the left subclavian artery orig coverage of the tear by thoracic endovascular aortic repair ( tevar ) is now a widespread treatment . 
however , in cases in which a mixed type of obstruction is present , both tevar and branch peripheral stenting may be necessary to achieve the optimal outcome . tevar for aortic dissection was first reported in the medical literature in 1999 for lesions involving the descending aorta [ 21 ] ; since then , it has gained widespread acceptance for treating different types of aortic pathologies , including those involving more proximal segments . 
anche questa evenienza , tuttavia , non esime da casi particolari in cui lassociazione dei due meccanismi , statico e dinamico , rende insufficiente la sola chiusura della porta dentrata tramite endoprotesi e necessita il completamento del trattamento con uno stenting del ramo arterioso viscerale . limpianto di unendoprotesi toracica ( thoracic endovascular aortic repair , tevar ) , introdotto nel 1999 nella pratica clinica [ 21 ] , ha avuto nellultima decade un ampio sviluppo di applicazioni e indicazioni . 
inizialmente utilizzato per lesioni localizzate sullaorta discendente a valle 84 radiol med ( 2013 ) 118 : 7488 dellarteria succlavia sinistra , oggi viene proposto anche per il trattamento di lesioni pi a monte come alternativa alla chirurgia . 
il contesto pi comune sicuramente la dissezione di tipo a , ma una fenestrazione pu essere proposta anche nei casi di tipo b in cui il trattamento tramite endoprotesi non sia proponibile o efficace [ 22 ]  . 
 le prime tecniche chirurgiche , sviluppate attorno al 1930 , sono ormai usate raramente ; a partire dalla prima fenestrazione percutanea descritta nel 1990 , sembra che circa 120 procedure siano state descritte [ 23 ]  . 
la procedura pu essere completata attraverso linserimento di un pallone di gran diametro e ad alta compliance ( lo stesso usato per la dilatazione delle endoprotesi ) che viene ritirato dallalto verso il basso attraverso laorta addominale allo scopo di dispiegare il flap intimale [ 24 ]  . dissezione aortica cronica ( diagnosi dopo 15 giorni dallinsorgenza ) questa evenienza sicuramente meno articolata della dissezione acuta e la condotta terapeutica pu beneficiare ovviamente di una riflessione pi a freddo . 
una dissezione cronica , da un punto di vista anatomico , si pu presentare come una dissezione di tipo a gi sottoposta a chirurgia ( chirurgia che , come visto , viene effettuata in acuto ) o come levoluzione di una dissezione di tipo b . 
11 branching dellarco aortico per trattamento di una lesione coinvolgente lorigine dei tronchi sopra aortici in paziente inoperabile : endoprotesi toracica fenestrata , dopo il posizionamento , con inserimento di un modulo endoprotesico nel tronco brachiocefalico ( freccia ) e stent coperto nella carotide sinistra ( punta di freccia )  . 
12a endovascular aortic fenestration using the scissor technique : two rigid guidewires are placed in the true and false lumens , and an 8 - f , 45 - cm - long sheath is advanced from the distal re - entry tear to the abdominal aorta to destroy the intimal flap . 
b preand c postfenestration angiograms showing , respectively , dynamic occlusion of the true lumen and resolution of the malperfusion following fenestration that created a large communication between the two lumens . 
12a ricostruzione al disegno di fenestrazione con la tecnica delle forbici ( scissor technique ) : lintroduttore 8 f viene avanzato lungo due guide rigide posizionate rispettivamente nel vero e nel falso lume in modo da ottenere una distruzione del flap intimale ( vedi testo )  . 
le immagini arteriografiche intraprocedurali pre ( b ) e post - fenestrazione ( c ) mostrano rispettivamente locclusione dinamica del vero lume con ipoperfusione delle arterie digestive ( freccia , ams ) e il ripristino del flusso seguente alla fenestrazione , che ha creato unampia comunicazione fra i due lumi . 
in fact , a range of different individual manoeuvres have been proposed in a variety of small case series with use of a wide range of endovascular devices ( intravascular ultrasound , angioplasty balloons , stents , snares , occlusion balloons , transeptal needles )  . 
commonly encountered complications and possible endovascular treatments have already been described for acute cases , as follows : aortic rupture , tevar ; rottura dellaorta ; sindrome da malperfusione . in questo caso , come in acuto , si pone lindicazione a intervenire . 
come ? nel caso della rottura aortica con il tevar ; nel caso di una sindrome da malperfusione tenendo presenti le regole dettate dallanatomia della malperfusione , basate come visto sul riconoscimento del meccanismo di occlusione delle arterie viscerali . la presenza di un meccanismo dinamico orienta verso un in particolare : tevar ; la presenza di un meccanismo di tipo statico o di una disconnessione ostiale fa porre indicazione per uno stenting della branca viscerale allostio o , eventualmente , a ponte fra il vero lume aortico e il vero lume della collaterale . 
in una dissezione cronica , infatti , il flap intimale caratterizzato da una maggiore consistenza ( sullimaging testimoniata da una membrana spessa , talvolta con calcificazioni ) , difficilmente distruttibile da una fenestrazione endovascolare . 
in caso di meccanismo misto , statico e dinamico , come visto nella fase acuta ci si pu porre la do86 radiol med ( 2013 ) 118 : 7488 malperfusion syndrome , dependent on treatment planning based upon imaging , clinical symptoms and examinations . as discussed above for acute cases , dynamic obstruction predictably responds to closure of the entry tear with tevar , whereas static obstruction and ostial disconnection are treated by peripheral stenting . 
 percutaneous fenestration does not play a role in a chronic process , as balloon dilation of a thick , calcified , intimal flap , which is typical of chronic cases , is rarely effective . 
in cases with a mixed type of occlusion , the combination of dynamic and static mechanisms of branch - vessel involvement may raise uncertainty regarding the relative roles of local treatment of the effected branch and remote treatment of the aortic entry tear as the most effective method of addressing malperfusion [ 2 ]  . 
ultimately , most of these complex cases are approached in a step - by - step process , with an individual management strategy predicated on the specific anatomical characteristics , including the number and mechanisms of branch involvement , and any residual ischaemia not addressed by the initial procedural technique . 
stenosis due to a dissection flap is very different from an atheroma , and it is likely that stenting will induce a haemodynamic effect on the false lumen , such that a risk of iliac or aortic rupture exists . 
limpianto dellendoprotesi , volto come gi detto alla riperfusione privilegiata del vero lume , richiede una stretta sorveglianza dellevoluzione , soprattutto clinica , per verificare se la chiusura della porta dentrata sufficiente a svolgere questa funzione . 
la stenosi dovuta al flap di dissezione ben diversa da una lesione ateromasica ed verosimile che limpianto di uno stent determini un effetto emodinamico sul falso lume per il quale il rischio di rottura iliaca o aortica va considerato . 
come comportarsi una volta che il paziente sia stato classificato come non complicato ? come schematizzato nelle figure 6 e 7 : in caso di dissezione acuta tipo a viene sempre dettata lindicazione alla chirurgia in considerazione della mortalit elevata riscontrata nei pazienti trattati con terapia conservativa ( 56% ) [ 3 ] ; la dissezione acuta di tipo b ancora consensualmente lasciata su terapia medica ( antipertensiva ) , seppure diversi studi hanno recentemente proposto il tevar anche nei casi non complicati [ 7 ] ; in caso di dissezione cronica , alcuni studi hanno dimostrato lutilit dei farmaci - bloccanti e degli antagonisti del recettore dellangiotensina 2 ( ara 2 ) nel diminuire levoluzione estasiante del falso lume [ 25 ] ; il follow - up obbligatorio per i pazienti cronici , dove le indicazioni al tevar , oggetto di continuo dibattito in letteratura , sono legate ad alcuni parametri : il diametro aortico , lo stato di perfusione del falso lume , la presenza di sintomi . conclusioni al termine di un articolo editoriale sempre interessante ricevere dei messaggi chiave . 
le immagini angio tc , tutte assiali , mostrano : in alto la stenosi del vero lume allorigine dellarteria iliaca sinistra con estensione del flap di dissezione ( frecce ) sullasse a valle ; in basso il controllo dopo trattamento , che comprendeva copertura con endoprotesi del foro dingresso a livello toracico e stenting dellasse iliaco . 
 in caso di malperfusione a livello iliaco , probabilmente consigliabile trattare prima la causa della malperfusione ( porta dentrata ) e poi la stenosi , onde evitare la compressione dello stent e soprattutto un possibile sovraccarico di pressione nel falso lume con rischio di rottura . conclusions this editorial focuses on some key points : pure anatomical classification in type a and b is evolving in a more clinical concept , which differentiates complicated and noncomplicated cases ; ct imaging of the entire aorta and iliac axes should always be planned and takes a role in diagnosis and treatment planning ; a patient - specific multidisciplinary discussion led by an interventional radiologist is crucial for proposing endovascular options ; therapeutic strategy is targeted to treat the complication first and then the pathology ( life - threatening conditions )  . finally , the answer to the opening question : what to do for a patient with chronic aortic dissection who presents with recent renal impairment ? the authors await the thoughts of readers to promote further discussion . la classificazione puramente morfologica della dissezione sta evolvendo verso una visione pi completa che distingue i casi complicati da quelli non complicati ; limaging , in particolare la tc , deve prevedere lo studio dal torace alla pelvi e assume un ruolo nella conferma diagnostica della sindrome da malperfusione e nella pianificazione terapeutica ; il radiologo interventista occupa , con le tecniche endovascolari , un ruolo chiave nella discussione multidisciplinare che resta obbligatoria per ogni paziente ; il trattamento della sindrome da malperfusione deve essere mirato in prima istanza alla complicanza e poi alla patologia di base ( trattamento di salvataggio )  . si ritorna dunque alla domanda proposta al congresso : come comportarsi nel caso di un paziente con dissezione aortica cronica che abbia sviluppato una malperfusione renale ? gli autori aspettano le risposte dei colleghi lettori per sollevare la discussione . 
follow - up examinations showed that the stent - graft remained patent in patients 1 , 2 and 4 , whereas stent occlusion occurred after 15 months in patient 3 ; in this case , a pseudoaneurysm proximal to the stent was identified , and although repeat stent - grafting successfully stopped the bleeding , the patient died of multiple organ failure 1 week later . 
il posizionamento in emergenza di radiol med ( 2013 ) 118 : 152157 endoprotesi una modalit tecnicamente realizzabile e terapeuticamente efficace nel trattamento di pazienti ad alto rischio che hanno subito la rottura iatrogena di unarteria periferica . 
the blood pressures of four patients ranged from 70 / 30 to 110 / 80 mmhg and heart rates from 108 to 132 bp percutaneous endovascular stent - grafting was performed with patients informed consent . 
digital subtraction angiography ( dsa ) was performed over the ruptured artery with a siemens multistar t.o.p or siemens artis dta carm imagery system ( siemens , germany )  . 
under fluoroscopy , a 5 - f catheter along with a 0.035hydrophilic guide wire ( terumo , tokyo , japan ) was inserted into the distal segment of the ruptured arteries [ profunda femoris artery ( pfa ) in cases 1 and 3 ; sfa in case 2 ; internal carotid artery ( ica ) in case 4 ]  . 
after replacement of the 0.035stiff guidewire ( terumo , tokyo , japan ) , a polytetrafluoroethylene ( ptfe ) - covered nitinol stent ( fluency , bard , usa ) was transported through the ruptured section . 
the size of stent - grafts used in cases 2 and 3 was 8 mm60 mm and in cases 1 and 4 was 8 mm80 mintraoperatively , 3 , 000 u of heparin was administered through the sheath . 
although it is a conventional therapeutic option for managing arterial injuries , vascular surgery is not appropriate in patients who are in poor physical condition and cannot tolerate the stress of surgery . 
in this article , we describe the clinical experience and median - term follow - up outcomes of four cases complicated by iatrogenic peripheral arterial ruptures . materials and methods between october 2005 and october 2009 , four patients with iatrogenic peripheral arterial ruptures were treated by stentgrafting in our hospital . 
the patient was transferred to our emergency service with continuous gauze compression applied to the left gro in cases 2 and 3 , both patients complained of sudden were evaluated at 6 - month intervals by ultrasonography of the lower - limb arteries . 154 results technical success was achieved in all four patients . 
patients were discharged within 57 days after stent - grafting . during follow - up ( 1336 months ) , ultrasonography showed that the stent - graft remained patent and the blood supply to the distal extremity was sufficient in cases 1 , 2 and 4 ; femoral stent - graft occlusion occurred after 15 months in case 3 . 
in case 3 , dsa identified an obliteration of the stent - graft in the right common femoral artery ( cfa ) , downstream displacement of the proximal end of the stentgraft and extravasation of contrast media from the proxiradiol med ( 2013 ) 118 : 152157 mal end of the graan 8 mm60 mm stent - graft ( fluency , bard ) was implanted . 
however , the patient died of multiple organ failure 1 week later due to intractable hypotension . discussion postcatheterisation pseudoaneurysms are the most common iatrogenic arterial injury , whereas arterial rupture is one of the most severe and emergent complications . 
1a - d necrosis and ulcerations occurred in the subcutaneous tissue of the groin following subcutaneous injection of a pseudomonas aeruginosa preparation and resulted in rupture of the femoral artery . 
a left common femoral artery ( cfa ) was compressed and obliterated , whereas the profunda femoris artery ( pfa ) and the superficial femoral artery ( sfa ) were not visualised . 
a larteria femorale comune di sinistra ( afc ) stata compressa ed obliterata e quindi larteria femorale profonda ( afp ) e larteria femorale superficiale ( afs ) non sono visualizzate . 
d dopo posizionamento dellendoprotesi permane il flusso ematico nella afc di sinistra e non si visualizza spandimento di mezzo di contrasto . radiol med ( 2013 ) 118 : 152157 fig . 
 the surgical approach is mainly used in young patients who are expected to have a long survival and in cases complicated by regional infections ; seriously compressed vessels , nerves , or skin ; or previous failure of minimally invasive treatment [ 2 ]  . 
 [ 6 ] reported that technical success was achieved in both patients who underwent endovascular balloon - expandable stent - grafting for injuries of the external iliac artery during hip surgery . 
the major reason for occlusion , in our opinion , may be thrombosis induced by twisting of the stent - grafts during adjacent joint motion and the slow blood flow in the stent - graft due to occlusive lesions in distal arterial branches . 
in addition to covering the arterial defect , the stent - graft also ensures blood supply to the distal artery , which is equivalent to the surgical ligation and bypass procedures for ruptured arteries . 
according to the authors analysis , the unfavourable clinical result was a direct result of not replacing the hip prosthesis or implanting an extraanatomical femorofemoral graft to bypass the infected area [ 6 ]  . 
we believe the complication may be a result of excessive vascular tension during hip - joint motion . balloon - expanding stent - grafts are superior because they enable more accurate localisation and result in better matching of the calibre of the injured blood vessels . 
due to their superior flexibility and radial expansion force against the extrinsic forces , self - expanding stent - grafts are more suitable for treating superficial sites , such as the carotid artery and groin [ 10 ]  . 
b following stent - grafting , normal blood flow in the right cfa was maintained , with no contrast media extravasation ; right profunda femoris artery ( pfa ) branches were clearly visible . 
a stravaso di mezzo di contrasto dalla lesione del muro anteriore dellarteria femorale comune di destra ( afc ) con obliterazione dellarteria femorale superficiale di destra ( afs )  . 
b dopo posizionamento di endoprotesi si preservato un normale flusso ematico nella afc di destra , senza stravaso di mezzo di contrasto ; i rami dellarteria femorale profonda ( afp ) sono chiaramente visibili . 
d dopo la ripetizione della procedura di posizionamento di endoprotesi , la afc di destra non mostra stravaso di mezzo di contrasto ma n flusso ematico oltre lestremit distale dellendoprotesi . 
e dopo lintroduzione della guida nei rami della afp , sono visibili minimo flusso ematico e difetti di riempimento nella afc e afp di destra . a higher risk of thrombosis and immunogenicity than are ptfe - covered stents [ 11 ]  . 
due to the absence of longterm follow - up study on stent - grafting , the procedure may be associated with unfavourable outcomes in young patients who are expected to have a long survival . 
therefore , stentgrafting is not recommended in young patients except in emergent cases . the 38 - year - old patient in case 1 in this report underwent emergency stent - grafting due to hypotension , extensive metastases of the malignant tumour and shorter survival expectancy . 
additionally , the left groin tissue defect did not allow for surgical incision healing , and the simple ligation of the artery for haemostasis would have impaired the blood supply to the lower limbs . 
an adjuvant bypass procedure was likely to incur regional infections due to the exposed autologous or artificial vessels at the site of the defect . we used ptfe - covered self - expanding stent - grafts with a calibre of 8 mm and a length of 68 cm in all four patients . 
stent - grafting was performed within 6 h of arterial rupture in all cases , except for the secondary stent - grafting in case 3 , which was performed 22 h after arterial rupture ; that patient finally died of multiple organ failure due to intractable hypotension , although the stentgraft successfully controlled the haemorrhage . in summary , we propose some critical measures in stentgrafting procedures used to treat iatrogenic peripheral arterial ruptures . 
second , self - expanding stent - grafts should be used in superficial and circuitous arterial ruptures that are in close proximity to joints ; the stent should have a calibre 1to 2 - mm larger than the diameter of the ruptured artery and a length 3to 4 - cm longer than that of the arterial rupture . 
such procedures radiol med ( 2013 ) 118 : 152157 are particularly useful for the rescue of high - risk patients and are considered a favourable alternative to surgical treatment . 
knauth springer - verlag , berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 540 - 89231 - 1 e - isbn : 978 - 3 - 540 - 89232 - 8 published online : 9 august 2012 springer - verlag 2012 computer tomography ( ct ) due to its continuous , revolutionary technical improvements ( helical ct , multislice - row offering multiplanar reconstructions ) has become an important and ever - increasing adjuvant instrument in acute abdomen imaging in association with ultrasound ( us ) and , less frequently magnetic resonance imaging ( mri )  . while us with its focused abdominal sonogram for trauma ( fast ) modality can be used as the rst , immediately available tool in the screening of possible lesions in acute abdomen in a trauma setting , ct is able to further implement these us suspected ndings and offer the emergency staff and abdominal surgeons a precise picture of the abdominal situation and so set the direction for patient care . 
 mri on the contrary , while more precise in terms of tissue and vascular characterization , due to its long performance time is out of scope in the majority of acute abdomen cases , most of all in trauma . it should be stressed that plain lm radiographs do still play a role as a rst screening modality in non - trauma and even in the trauma setting . the book is divided into ve parts : epidemiology data and clinical ndings ; elementary ct ndings ; ct techniques ; ct diagnosis in non traumatic abdomen ; ct diagnosis in traumatic abdomen . 
 the bulk of the book is devoted to ct diagnosis in the non traumatic abdomen : each possible cause of acute abdomen affecting abdominal organs is presented , dealt with and discussed in its 18 parts , from acute liver disease , to acute pancreatitis , acute appendicitis , bowel obstruction and perforation , urologic and gynecologic emergencies and complications of abdominal surgery . the text provides an introduction ( epidemiology and physiopathology ) to each condition , followed by a discusla tomograa computerizzata ( tc ) grazie ai continui e rivoluzionari progressi tecnici ( tc spirale , multi - strato con possibilit di ricostruzione multiplanari ) diventata uno strumento importante e di sempre maggior aiuto nello studio per immagini delladdome acuto , in associazione con lecograa ( us ) e , con minor frequenza , la risonanza magnetica ( rm )  . 
 mentre gli us con la tecnica focused abdominal sonogram for trauma ( fast , ecograa mirata delladdome nel trauma ) pu essere utilizzata come il primo ed immediatamente disponibile strumento di valutazione di possibili lesioni addominali acute in caso di trauma , la tc in grado di perfezionarne i reperti sospetti e cos offrire al personale del reparto di emergenza ed al chirurgo addominale un quadro preciso della situazione , indirizzandoli nella cura del paziente . 
invece la rm , pur essendo pi precisa in termini di caratterizzazione tissutale e vascolare , a causa del suo lungo tempo di ripresa , da considerarsi fuori gioco nella maggior parte dei casi di addome acuto , in particolare traumatico . da non dimenticare che i radiogrammi diretti delladdome rivestono ancora un ruolo importante come primo approccio diagnostico in caso di addome acuto sia traumatico che non traumatico . 
 il volume diviso in cinque parti : dati epidemiologici e reperti clinici ; quadri tc elementari ; tecniche tc ; diagnosi tc delladdome non traumatico ; diagnosi tc delladdome traumatico . 
 la maggior parte del volume dedicato alla diagnosi tc delladdome non traumatico : viene presentata , trattata e discussa nelle sue 18 parti ogni possible causa di addome acuto interessante gli organi addominali , dallinteressamento epatico alla pancreatite acuta , allappendicite , allostruzione e perforazione intestinale , alle emergenze urologiche e ginecologiche , nonch alle complicanze chirurgiche . il testo presenta una introduzione sulla epidemiologia e siopatologia di ciascuna condizione , seguita da una diradiol med ( 2013 ) 118 : 160161 sion of clinical presentation , laboratory , radiographic , ultrasound and ct ndings and possible pitfalls ( presented and discussed in extenso ) , differential diagnosis , enriched by tables summarizing the most important data and proper and well reproduced images . 
all of the above is aimed to offer the reader state of the art and up - dated knowledge on the management of patients with acute abdomen . the last and longest part of the book is devoted to the in - depth presentation and discussion of the use of ct in the diagnosis of traumatic abdomen in all its possible variations : here much stress is put on the impact on patient management following ct diagnosis under such conditions . the book lay - out is unusual : the abstract is very often identical to the chapter introduction . this book will be a user - friendly companion to general radiologists and most of all to emergency department radiologists , clinicians , and abdominal surgeons who will nd a source of knowledge deriving from the large experience of the books editor and his co - authors . 
 scussione sulla presentazione clinica , sui dati di laboratorio , radiograci , ecograci e tc e sui possibili trabocchetti diagnostici ( presentati e discussi in extenso ) e sulla diagnosi differenziale ; il tutto arricchito da tabelle riassumenti i dati pi importanti e da immagini adeguate e ben riprodotte . 
il volume vuole essere uno strumento per offrire al lettore una conoscenza davanguardia ed aggiornata sul trattamento dei pazienti affetti da un addome acuto . lultima ed in s la pi lunga parte del volume dedicata ad una profonda presentazione e discussione dellimpiego della tc nella diagnosi delladdome acuto in tutte le sue possibili varianti : qui , enfasi particolare viene rivolta al trattamento del paziente affetto da tale condizione a seguito della diagnosi tc . colpisce un aspetto inusuale della impostazione del volume : il sommario di apertura assai spesso identico allintroduzione del capitolo . il volume sar un compagno di facile uso per i radiologi generali ed in particolare per quelli dei reparti di emergenza , per il clinici e per i chirurghi addominale che vi troveranno una notevole fonte di informazioni derivata dalla larga esperienza delleditore del volume e dei suoi co - autori . 
stabile ianora1 1sezione di diagnostica per immagini , centro interdipartimentale per lo studio dellhht , universit degli studi di bari , azienda universitario - ospedaliera consorziale policlinico , bari , italy 2sezione di medicina interna augusto murri , di.m.i.m.p. 
scardapane , istituto di radiologia , universit degli studi di bari , azienda universitario - ospedaliera consorziale policlinico , piazza giulio cesare 11 , 70124 bari , italy , tel . : + 39 - 080 - 5478840 , fax : + 39 - 080 - 5592911 , e - mail : a.scardapane@radiologia.uniba.it received : 29 march 2011 / accepted : 25 may 2011 / published online : 10 february 2012 springer - verlag 2012 abstract purpose . 
between february 2001 and december 2010 , 171 consecutive hht patients ( 95 men and 76 women ) were studied with triphasic multidetector computed tomography ( mdct ) in 91 cases , magnetic resonance imaging ( mri ) in 34 cases and both in the remaining 46 cases . 
arteriovenous shunts were found in 24 / 171 ( 14% ) cases , arterioportal shunts in 52 / 171 ( 30% ) , mixed shunts in 26 / 171 ( 15% ) , telangiectases in 84 / 171 ( 49% ) and transient hepatic attenuation differences ( thads ) in 70 / 171 ( 41% )  . 
la presenza di alterazioni epatiche stata ricercata in 91 casi con tcmd trifasica ( fase arteriosa precoce , tardiva e fase venosa ) e in 34 con angio - risonanza magnetica ( rm ) dinamica , i rimanenti 46 pazienti sono stati sottoposti ad entrambi gli esami . 
in 126 / 171 ( 74% ) pazienti sono state diagnosticate alterazioni vascolari epatiche costituite da fistole artero - venose ( 24 / 171 , 14% ) , fistole artero - portali ( 52 / 171 , 30% ) , fistole miste ( 26 / 171 , 15% ) , telangiectasie ( 84 / 171 , 49% ) e disordini di perfuzione ( thads ) ( 70 / 171 , 41% )  . 
in 6 / 171 casi ( 3 donne e 3 uomini , 3 , 5% ) sono state descritte lesioni nodulari epatiche ipervascolarizzate associate in 5 pazienti ad altre lesioni vascolari . 
it is characterised by vascular abnormalities such as telangiectases and arteriovenous malformations that may affect any bodily region and result in recurrent bleeding and anaemia [ 1 , 2 ]  . 
although the skin and mucosal tissues are most frequently involved , a substantial number of patients have concurrent involvement of the lung , brain or liver or other abdominal viscera , such as the gastrointestinal canal and the pancreas . 
hht diagnosis is generally established on the basis of the clinical curaao criteria ( table 1 ) , although genetic testing is now available in referral centres to identify mutations in the alk1 and eng genes , which are responsible for mutation of genes involved in the regulation of endothelial growth factors [ 35 ]  . hepatic involvement in hht is characterised by vascular malformations , which are classified as telangiectases , arteriovenous , arterioportal and portovenous shunts , large confluent vascular masses ( lcvm ) ; and perfusion disorders , such as transient hepatic attenuation differences ( thad ) distributed throughout the parenchyma . 
thanks to the increasing use of diagnostic imaging techniques , such as multidetector computed tomography ( mdct ) and magnetic resonance ( mr ) imaging , the prevalence of these malformations , previously thought to be low , is today considered to be around 70% [ 68 ]  . 
among the hepatic manifestations of hht , a nodular transformation of the parenchyma has also been reported , which translates into a high frequency of focal nodular hyperplasia ( fnh ) and regenerative nodules of varying size , which may extensively involve the liver parenchyma and lead to nodular regenerative hyperplasia ( nrh ) [ 9 , 10 ]  . 
 in particular , the high frequency of fnh compared with the la telangiectasia emorragica ereditaria ( hht ) o malattia di rendu - osler - weber un disordine genetico ereditario a trasmissione autosomica dominante e penetranza incompleta , con una frequenza stimata intorno a 1 / 6000 soggetti . 
essa caratterizzata da lesioni angiodisplastiche quali telangiectasie e malformazioni artero - venose che possono interessare qualunque distretto corporeo con conseguenti frequenti sanguinamenti ed anemizzazione [ 1 , 2 ]  . 
la cute e le mucose sono le sedi pi frequentemente colpite dalle lesioni , tuttavia un numero rilevante di pazienti mostra anche un contemporaneo interessamento polmonare , epatico , cerebrale o di altri visceri addominali quali il tubo gastroenterico e il pancreas . 
la diagnosi di hht formulata sulla base dei criteri clinici di curaao ( tabella 1 ) anche se nei centri di riferimento per lo studio della malattia ormai disponibile il test genetico per la ricerca delle mutazioni dei geni alk1 ed eng responsabili di mutazioni di geni implicati nella regolazione dei fattori di crescita endoteliale [ 35 ]  . linteressamento epatico in corso di hht caratterizzato da alterazioni vascolari , distinte in telangiectasie , fistole artero - venose , artero - portali e porto - venose , grandi masse vascolari ( lcvms ) e disordini di perfusione ( thads ) ubiquitariamente distribuiti nel parenchima . 
grazie al sempre pi frequente impiego di tecniche di diagnostica per immagini quali la tc multidetettore ( tcmd ) e la risonanza magnetica ( rm ) , la prevalenza di queste alterazioni , in passato considerata piuttosto rara , oggi stimata intorno al 70% [ 68 ]  . 
tra le manifestazioni dellhht a livello epatico stata descritta anche una trasformazione nodulare del parenchima che si traduce in unelevata frequenza di iperplasia nodulare focale ( fnh ) e di noduli rigenerativi di diverse dimensioni che possono anche interessare estesamente il parenchima epatico e determinare un quadro di iperplasia nodulare rigenerativa ( nrh ) [ 9 , 10 ]  . 
 sebbene in letteratura lattivit rigenerativa del parenchima epatico in corso di hht sia spesso menzionata , radiol med ( 2013 ) 118 : 113 table 1 hereditary haemorrhagic telangiectasia ( hht ) diagnosis according to the clinical curaao diagnostic criteria criteria epistaxis ( spontaneous , recurrent nosebleeds ) telangiectases ( multiple at characteristic sites such as lips , nose , fingers and oral cavity ) visceral lesions cerebral and spinal arteriovenous malformations pulmonary arteriovenous malformations gastrointestinal telangiectases family history ( first - degree relatives affected by hht according to these criteria ) diagnosis definite : presence of 3 criteria possible : presence of 2 criteria unlikely : presence of fewer than 2 criteria tabella 1 criteri diagnostici clinici di curaao per la diagnosi di hht criteri epistassi ( spontanea , ricorrente ) telangiectasie ( multiple in sedi tipiche come labbra , naso , dita e cavit orale ) lesioni viscerali malformazioni artero - venose cerebrali e spinali malformazioni artero - venose polmonari telangiectasie gastroenteriche storia familiare ( parente di primo grado affetto da hht secondo questi criteri ) diagnosi certa : presenza di 3 criteri possibile : presenza di 2 criteri improbabile : presenza di meno di 2 criteri general population was well documented in a multicentric study by buscarini et al . 
 [ 15 ] , whereas a high rate of nodular regenerative lesions was reported in a prospective series studied with mr imaging [ 16 ]  . the purpose of this retrospective study was to evaluate the frequency of nodular regenerative lesions in a large cohort of patients with hht who were enrolled consecutively at the interdisciplinary centre for the study of hht of our university . materials and methods patients we retrospectively studied 171 patients ( 95 men ; 76 women ) who came to the interdepartmental centre for the study of hht of the university of bari between february 2001 and december 2010 . 
 [ 15 ] , mentre unelevata percentuale di lesioni nodulari rigenerative stata recentemente riportata in una casistica prospettica valutata con rm [ 16 ]  . obiettivo di questo studio retrospettivo pertanto valutare la frequenza di lesioni nodulari rigenerative in unampia coorte di pazienti affetti da hht arruolati consecutivamente presso il centro interdisciplinare per lo studio della suddetta malattia della nostra universit . 
 materiali e metodi pazienti sono stati studiati retrospettivamente 171 pazienti ( 95 maschi e 76 femmine ) afferiti , tra febbraio 2001 e dicembre 2010 , presso il centro interdipartimentale per la studio dellhht delluniversit degli studi di bari . 
una sintomatologia clinica riconducibile al coinvolgimento epatico era evidente in 14 / 171 ( 8% ) pazienti che riferivano in 3 / 171 casi ( 2% ) un episodio di ematemesi sostenuto da varici esofagee , in 9 / 171 ( 5% ) una condizione di insufficienza cardiaca ad alta portata sostenuta da fistole artero - venose epatiche e in 2 / 171 ( 1% ) casi una colangite su base ischemica . 
dopo aver ottenuto consenso informato scritto , 91 / 171 ( 53% ) pazienti sono stati sottoposti a tcms , 46 / 171 ( 27% ) sia a tcms sia a rm e 34 / 171 ( 20% ) unicamente a rm . 
 protocollo dellesame tcmd lo studio tc stato eseguito impiegando una tcmd a 4 detettori ( philips mx8000 , philips medical systems , royal philips electronic , best , paesi bassi ) in 85 / 171 casi ( 50% ) e a 16 detettori ( tsx - 101a - aquilion , toshiba medical system , tochigi , giappone ) in 52 / 171 casi ( 30% )  . 
dopo iniezione endovena ( e.v. ) di 1 , 5 ml / kg di mezzo di contrasto ( mdc ) organo - iodato non ionico ad alta concentrazione ( 370400 mgi / ml ) con flusso di 4 ml / s , stato eseguito un protocollo di studio trifasico ( fase arteriosa precoce , fase arteriosa tardiva e fase venosa ) secondo le modalit gi descritte in letteratura [ 6 ] , con spessore di strato di 2 , 5 e 1 mm , pitch di 1 , 25 e 1 , 75 , incremento di ricostruzione di 1 e 0 , 8 mm , rotazione del tubo di 0 , 5 , kv / mas di 120 / 250 , rispettivamente per la tc a 4 detettori e 16 detettori . il ritardo di scansione per la fase arteriosa precoce radiol med ( 2013 ) 118 : 113 symptoms of hepatic involvement were evident in 14 / 171 ( 8% ) patients ; more specifically , 3 / 171 reported ( 2% ) an episode of haematemesis due to oesophageal varices , 9 / 171 ( 5% ) had high - output heart failure due to arteriovenous shunts ( avs ) , and 2 / 171 ( 1% ) had ischaemic cholangitis . 
 after providing written informed consent , 91 / 171 ( 53% ) patients underwent mdct , 46 / 171 ( 27% ) both mdct and mr imaging , and 34 / 171 ( 20% ) mr imaging alone . 
 mdct protocol the mdct study was performed using a 4 - detector scanner ( philips mx8000 , philips medical systems , royal philips electronic , best , the netherlands ) in 85 / 171 cases ( 50% ) and a 16 - detector scanner ( tsx - 101a - aquilion , toshiba medical system , tochigi , japan ) in 52 / 171 cases ( 30% )  . 
all images were transferred to a workstation ( vitrea 4.1 , vital images , minneapolis , mn , usa ) in order to obtain multiplanar reformations ( mpr ) and maximum intensity projection ( mip ) reconstructions . mr imaging protocol mr scans were acquired using a 1.5 - t superconductive magnet ( philips achieva v1.54 ) with a 4 - channel surface coil ( sense body coil ) placed on the upper abdomen , according to a previously described technique [ 7 ]  . 
la fase arteriosa tardiva e la fase venosa sono state acquisite con un ritardo di scansione rispettivamente di 1520 s e 45 s dalla prima acquisizione ; tutte le immagini sono state in seguito trasferite ad una workstation ( vitrea 4.1 , vital images , minneapolis , minnesota , usa ) al fine di ottenere ricostruzioni in multiplanar reformation ( mpr ) e maximum intensity projection ( mip )  . protocollo dellesame rm la rm stata condotta mediante un magnete superconduttivo da 1 , 5 tesla ( philips achieva v1.54 ) , con posizionamento di una bobina di superficie a 4 canali ( sense body coil ) sulladdome superiore secondo le modalit riportate in letteratura [ 7 ]  . 
larrivo del mezzo di contrasto in aorta stato valutato mediante una sequenza di bolus tracking in tempo reale e la prima sequenza dinamica stata lanciata appena laorta addominale diveniva visibile . 
 lacquisizione angiografica era seguita da una sequenza radiol med ( 2013 ) 118 : 113 balanced turbo field echo ( b - tfe ) sequences in the coronal plane ( thickness 8 mm with 4 mm overlap ; shortest te / tr ; flip angle 90 ; fov 350400 ; respiratory breathhold )  . subsequently , after injection of 0.2 mmol / kg of paramagnetic contrast agent ( gadobenate dimeglumine multihance , bracco , milan , italy in 65 cases , or gadopentetate dimeglumine magnevist , bayer schering , berlin , germany in 15 patients ) at a rate of 2.5 ml / s followed by a 25 - ml bolus of saline solution , eight consecutive dynamic sequences were acquired in the coronal plane during a single breath - hold using t1w 3d fast - field echo ( t1 ffe ) sequences with the following parameters : 4050 scans in the coronal plane with 2.5 mm thickness , 450 fov ( rectangular 90% ) , 0.80.82.5 voxel , short tr / te , 25 flip angle , sense factor 3 , 256 matrix ( 512 reconstruction matrix ) , with an overall acquisition time of 24 s ( 3 s for each dynamic phase )  . arrival of the contrast agent into the aorta was detected using a real - time bolus tracking sequence , and the first dynamic sequence was acquired as soon as the abdominal aorta became visible . 
 angiographic acquisition was followed by an axial t1w high - resolution isotropic volume examination ( thrive ) sequence during the venous phase for complete assessment of the hepatic parenchyma [ 100 slices with 2 - mm thickness , sense factor 4 , 350380 fov ( rfov 6570% ) , 1921 s acquisition time ]  . 
 in one case , a second mr examination was performed using a superparamagnetic hepatospecific contrast agent ( ferumoxide , endorem , guerbet ) about 1 week after the first examination . parameters assessed on both modalities , the typical vascular malformations of hht were searched for , namely : telangiectases ( small , rounded lesions with a maximum diameter < 10 mm , with enhancement in the early arterial phase after contrast injection and poorly defined on the remaining scans ) ; assiale t1w high - resolution isotropic volume examination ( thrive ) in fase venosa , per una completa valutazione del parenchima epatico ( 100 slice con spessore 2 mm , sense factor 4 , fov 350380 , rfov 65%70% , tempo di acquisizione 1921 secondi )  . 
in un caso , stata eseguita una seconda risonanza magnetica con mezzo di contrasto epato - specifico superparamagnetico ( ferumoxide , endorem , guerbet ) dopo circa una settimana dal primo esame . parametri valutati per entrambe le metodiche sono state ricercate le alterazioni vascolari tipiche dellhht distinte in : telangiectasie ( piccole lesioni rotondeggianti del diametro massimo inferiore a 10 mm con enhancement dopo iniezione di mdc in fase arteriosa precoce e mal delimitabili nelle restanti scansioni ) ; grandi masse vascolari confluenti ( lcvms ) ( lesioni con le medesime caratteristiche rispetto alle telangiectasie , ma di dimensioni > 10 mm ) ; disordini di perfusione ( thads ) ; malformazioni artero - venose ( havms ) , classificate come fistole arterovenose ( fav ) , fistole arteroportali ( fap ) e fistole porto - sistemiche ( fps )  . per quanto riguarda il tipo di havms , stata fatta diagnosi di fav quando si osservava lopacizzazione delle vene epatiche in fase arteriosa precoce , le fap , invece , sono state diagnosticate se i rami intraepatici portali o la vena porta erano chiaramente visibili in fase arteriosa precoce con densit o segnale significativamente superiori rispetto alla vena splenica . 
telangiectases were observed in 84 / 171 ( 49% ) cases , whereas lcvm and thad were seen in 20 / 171 ( 12% ) and in 70 / 171 ( 41% ) , respectively . 
in no patient was pss seen . in 6 / 171 ( 3.5% ) patients ( three women and three men , two of whom were siblings ) , single ( n = 2 ) or multiple ( n = 4 ) focal lesions were seen , with size ranging from 15 to 55 mtwo patients had undergone mdct , three mr imaging and one both examinations ( table 2 )  . 
le telangectasie sono state osservate in 84 / 171 ( 49% ) casi mentre la presenza di lcvms e thads stata dimostrata rispettivamente in 20 / 171 ( 12% ) e in 70 / 171 ( 41% ) pazienti . 
havms sono state diagnosticate in 92 / 171 ( 54% ) casi , con entrambe le metodiche ; di queste , 24 / 171 ( 14% ) erano fav , 52 / 171 ( 30% ) fap e infine in 26 / 171 ( 15% ) pazienti , erano evidenti sia fav che fap . 
in nessun paziente sono state riconosciute fps . in 6 / 171 ( 3 , 5% ) pazienti ( tre femmine e tre maschi di cui due fratelli ) sono state riscontrate lesioni focali uniche ( n = 2 ) o multiple ( n = 4 ) di dimensioni comprese tra 15 mm e 55 mdue pazienti erano stati sottoposti a tcmd , tre a rm e un paziente ad entrambi gli esami ( tabella 2 )  . 
tre pazienti sono stati sottoposti a follow - up ecografici annuali ( rispettivamente da 8 , 3 ed 1 anni ) che non hanno messo in evidenza alcuna modificazione del quadro epatico . 
 discussione il coinvolgimento epatico nei pazienti hht asintomatico in circa il 95% dei casi ; nel restante 5% dei pazienti la malattia epatica sintomatica e si manifesta con tre possibili quadri clinici : ( 1 ) insufficienza cardiaca ad alto flusso secondaria a importanti fistole artero - venose ; ( 2 ) ipertensione portale in pazienti che sviluppano una cirrosi radiol med ( 2013 ) 118 : 113 radiol med ( 2013 ) 118 : 113 fig . 
b mra in the portal phase : early opacification of the hepatic veins due to arteriovenous shunt ( arrowheads ) ; hypervascular hepatic lesion depicted in segment vi ( arrow )  . 
three patients underwent yearly follow - up with ultrasound ( us ) ( for 8 , 3 and 1 year , respectively ) , with no evidence of any change of the hepatic abnormalities . 
 discussion liver involvement in hht patients is asymptomatic in around 95% of cases ; the remaining 5% of patients showed the following possible clinical manifestations : ( 1 ) highoutput heart failure secondary to major avs ; ( 2 ) portal hysu base vascolare ; ( 3 ) patologia biliare da ischemia delle vie biliari intraepatiche [ 17 , 18 ]  . 
la trasformazione nodulare del parenchima epatico nei pazienti con hht , nota sin dalla fine degli anni settanta come pseudo - cirrosi o cirrosi atipica poich non associata ad insufficienza epatica e a fibrosi parenchimale attualmente considerata una risposta iperplastica del fegato allipoperfusione dovuta alle fistole artero - venose [ 9 , 19 ]  . 
tcmd in fase arteriosa precoce ( a , b ) , tcmd in fase venosa ( c ) , scansione ssh t2 pesata ( d ) , scansione thrive in fase epatospecifica ( e )  . 
presenza di piccole telangiectasie ( frecce sottili in a ) e di lesione ipervascolarizzata del vi segmento ( freccia in b ) che mostra una pseudo - capsula ( punte di freccia in c )  . 
la lesione , sostanzialmente isointensa rispetto al fegato nelle sequenze t2 pesate ( freccia in d ) mostra omogeneo uptake di mdc in fase epatospecifica ( freccia in e )  . 
nodular transformation of the hepatic parenchyma in hht patients , known since the late 1970s as pseudocirrhosis or atypical cirrhosis as not associated with liver failure and parenchymal fibrosis , is currently thought to be a hyperplastic response of the liver to the hypoperfusion produced by avs [ 9 , 19 ]  . 
in these cases , the liver has a finely granular appearance owing to the presence of nodules only few millimetres in size that may merge to form lesions approximately 1 cm in size . 
these nodules range from 5 to 20 mm in size and may occasionally reach 5 cm ; when surrounded by fibrous septa , they are indistinguishable from cirrhotic nodules [ 20 ]  . 
in questi casi il fegato ha aspetto finemente granulare per la presenza di noduli di pochi millimetri che possono confluire in lesioni di circa 1 ci noduli rigenerativi contenenti pi di un tratto portale vengono definiti noduli iperplastici multiacinari . 
 tali noduli hanno dimensioni comprese tra 5 e 20 mm e occasionalmente possono raggiungere i 5 cm ; quando circondati da setti fibrosi sono indistinguibili dai noduli cirrotici [ 20 ]  . 
tutte le alterazioni citate sono state associate da diversi autori allhht e recentemente , in uno studio condotto su fegati espiantati da pazienti con hht , stato dimostrato come possano coesistere nello stesso organo in risposta alle alterazioni della vascolarizzazione [ 9 , 13 , 19 ]  . 
 lutilizzo sempre maggiore , nella valutazione diagnostica di questi pazienti , di metodiche di imaging come lecotomografia , la tomografia computerizzata e la risonanza radiol med ( 2013 ) 118 : 113 fig . 
a study conducted on livers explanted from patients with hht demonstrated that the abnormalities may coexist in the same patient in response to vessel abnormalities [ 9 , 13 , 19 ]  . 
 the increasing use of us , ct and mr imaging in the diagnostic assessment of these patients has provided further magnetica ha permesso di conoscere molto pi dettagliatamente le caratteristiche delle lesioni epatiche dei pazienti con hht [ 7 , 22 ]  . 
 [ 16 ] in 23 pazienti arruolati consecutivamente e sottoposti a rm.nel primo studio rilevata una prevalenza di fnh circa cento volte superiore rispetto alla popolazione normale ( 5 / 274 ; 1 , 8% )  . 
le lesioni sono state riscontrate in 4 femmine ed 1 maschio e la loro diagnosi stata posta in 4 / 5 pazienti sulla base di reperti radiol med ( 2013 ) 118 : 113 insight into the features of hepatic lesions in patients with hht [ 7 , 22 ]  . 
the lesions were detected in four women and one man , and their diagnoses were established in 4 / 5 patients on the basis of findings typical of fnh on at least two of the modalities used ( us , ct and mr imaging ) , whereas in 1 / 5 cases it was confirmed by percutaneous biopsy . 
the diagnostic criteria for nrh are the presence of multiple nodules of varying size , isointense on baseline t1w and t2w sequences , hypervascular during the arterial phase and isointense during the venous phase after contrast administration . 
 at our centre , liver assessment by ct and / or mr imaging is included in the screening of all adult patients regardless of the presence of specific clinical signs . 
the review of our series allowed us to recognise in 6 / 171 ( 3.5% ) cases multiple ( n = 4 ) or single ( n = 2 ) nodular lesions in three men and three women , respectively . 
in the cases studied by mr imaging , the nodules were predominantly isointense relative to the parenchyma both at baseline and on the sequences acquired during the hepatospecific phase , which suggests their benign nature [ 23 ]  . in contrast to the experience by buscarini et al . 
 [ 15 ] , no typical fnh was identified , and we found a high prevalence of lesions among men ; however , most lesions we identified had some signs in common with fnh , such as a baseline signal similar to that of the healthy parenchyma , hypervascularity during the arterial phase , venous isoattenuation / isointensity and hepatospecific contrast agent uptake , which might justify terms such as atypical fnh or fnh - like lesions . 
patient selection may account for this difference , as the 23 patients recruited in milot et al.s study were most likely affected by advanced - stage liver disease given the percentage of symptomatic patients ( 13 / 23 , 56.5% ) , which is significantly higher than reported in the literature and seen in our series based on systematic screening [ 7 , 18 , 24 ]  . the cases of nrh we identified in hht patients were characterised by large lesions with features similar to fnh , which may also manifest as multiple lesions as confirmed by the histological findings by brenard et al . 
i criteri diagnostici per la rnh consistono nella presenza di noduli multipli di diverso diametro , isointensi nelle sequenze t1 e t2 di base e , dopo iniezione di mdc , ipervascolarizzati in fase arteriosa e isointensi in fase venosa . 
 nel nostro centro interdipartimentale per lo studio dellhht la valutazione del fegato con tc e / o rm inserita nello screening di tutti i pazienti adulti indipendentemente dalla presenza di segni clinici specifici . 
la revisione di questa casistica ha permesso di riconoscere in 6 / 171 ( 3 , 5% ) casi , lesioni nodulari multiple ( n = 4 ) o uniche ( n = 2 ) rispettivamente in tre maschi e tre femmine . 
nei casi studiati con rm i noduli erano sostanzialmente isointensi rispetto al parenchima sia nelle sequenze di base sia in quelle in fase epatospecifica suggerendone la natura epatocitaria benigna [ 23 ]  . rispetto allesperienza di buscarini et al . 
 [ 15 ] , nella nostra serie di pazienti non abbiamo mai osservato fnh tipiche , con una elevata prevalenza di lesioni nel sesso maschile ; tuttavia la maggior parte delle formazioni da noi descritte mostrano alcuni segni in comune con lfnh quali il segnale di base simile a quello del fegato sano , lipervascolarizzazione in fase arteriosa , lisodensit / isointensit venosa e la captazione di mdc epatospecifico che potrebbero giustificare lutilizzo del termine fnh atipiche o lesioni fnh - like . 
la spiegazione di questa differenza da ricercare nella selezione dei pazienti poich i 23 soggetti reclutati nel lavoro di scuola francese sembrano essere affetti da forme molto avanzate di malattia epatica in considerazione della percentuale di pazienti sintomatici 13 / 23 ( 56 , 5% ) significativamente superiore rispetto a quella riportata in letteratura e nella nostra casistica basata su uno screening sistematico [ 7 , 18 , 24 ]  . lrnh da noi osservata nei pazienti con hht contraddistinta da lesioni di grosse dimensioni con caratteristiche simili allfnh che possono manifestasi anche in forma multipla in accordo con i rilievi istologici di brenard et al . 
diversamente dalla nrh precedentemente definita in letteratura come iperplasia monoacinare da occlusione venosa , nellhht un ruolo determinante svolto dalliperafflusso arterioso distrettuale responsabile di una risposta iperplastica del parenchima in analogia al meccanismo 12 radiol med ( 2013 ) 118 : 113 nrh , previously defined as monoacinar hyperplasia secondary to venous occlusion , in hht a decisive role is played by the arterial hyperperfusion responsible for a hyperplastic parenchymal response , as occurs with fnh [ 20 ]  . 
in fact , in 5 / 6 ( 83% ) patients in our series , nodular regeneration was associated with important vascular abnormalities , such as telangiectases and avs , and with dilated hepatic artery ; in one case only was ct unable to depict any clear vascular lesion . 
these shunts , most of which are portovenous , have been described in the literature and are probably responsible for metabolic alterations that can only be identified with laboratory tests such as the breath tests [ 12 , 25 ]  . the main limitation of our study was the absence of histological confirmation for these lesions , even though guidelines for studying hht advise against the use of invasive procedures such as biopsy [ 10 ]  . 
the differential diagnosis between the different hypervascular focal hepatic lesions ( adenoma ; fnh ; hepatocellular carcinoma ) is essential and carried out with diagnostic imaging techniques ; among them , mr imaging with hepatospecific contrast agents is the most helpful for characterising the different diseases [ 23 ]  . 
 the former are true focal hepatic lesions that are recognised for their mass effect and , in some cases , deformation of the liver contour ; the latter are probably confluent telangiectases or part of a large avm nidus , usually recognisable during the arterial phase and no longer definable during the venous phase , as happens with perfusion disorders [ 6 ]  . evocato per lfnh [ 20 ]  . 
nella nostra esperienza , in 5 / 6 ( 83% ) pazienti , la rigenerazione nodulare era infatti associata ad importanti alterazioni vascolari come telangiectasie e fistole artero - venose e alla dilatazione dellarteria epatica ; in un solo paziente la tc non metteva in evidenza chiare lesioni vascolari . 
tali anastomosi , prevalentemente di tipo porto - venoso , sono state descritte in letteratura e sono probabilmente responsabili di alterazioni metaboliche rilevabili esclusivamente con test di laboratorio come i breath test [ 12 , 25 ]  . il limite principale del nostro studio lassenza di conferma istologica per queste lesioni anche se le linee guida per lo studio dellhht sconsigliano qualsiasi procedura invasiva come la biopsia [ 10 ]  . 
la diagnosi differenziale tra le diverse lesioni epatiche focali ipervascolarizzate ( adenoma , fnh , hcc ) indispensabile ed pertanto affidata alle tecniche di diagnostica per immagini ; tra queste la rm con mdc epatospecifici lindagine che offre le maggiori possibilit di caratterizzare le diverse patologie [ 23 ]  . 
nel primo caso si tratta di vere lesioni focali epatiche riconoscibili per il loro effetto massa e per leventuale deformazione dei contorni epatici , nel secondo caso si tratta probabilmente di telangiectasie confluenti o di voluminosi nidus fistolosi , in genere riconoscibili in fase arteriosa e non pi delimitabili , in maniera analoga a disturbi di perfusione , in fase venosa [ 6 ]  . conclusioni conclusions the presence of hyperplastic hepatic regenerative nodules is frequent in patients with hht , mostly in association with large havm . 
in our experience , these nodules have a similar appearance to fnh without the pathognomonic features of the latter , such as a central scar or higher prevalence among women . 
knowledge of these aspects of liver involvement by hht is essential for distinguishing regenerative from malignant lesions and avoiding invasive procedures , which are known to be particularly dangerous for these patients . 
 la presenza di noduli rigenerativi iperplastici epatici frequente nei pazienti con hht , soprattutto in associazione ad estese havtali noduli nella nostra esperienza , presentano aspetti simili allfnh senza mostrarne le caratteristiche patognomoniche , come la cicatrice centrale o la prevalenza nel sesso femminile . 
 tutti i problemi sopra esposti ( tolleranza del tessuto normale alla re - irradiazione , passando attraverso concetti di frazionamento , ipertermia e re - irradiazione , rapporto terapetico tra re - irradiazione e farmaci citotossici ed altri agenti che ne modificano la risposta , nonch riduzione delle dosi ai tessuti sani mediante tecnologia avanzata ) sono radiol med ( 2013 ) 118 : 158159 gan or region of interest ( brain and eye tumours ; head and neck , lung , breast , prostate , rectal cancer ; gynaecological malignancies , soft tissue sarcomas , bone and brain metastases ) in the books sixteen chapters . this very detailed and in - depth book , will be appreciated by those working in the field , oncology radiotherapists as well as clinicians and surgeons who have to deal with this difficult medical problem . trattati e discussi in dettaglio sulla base dellorgano o della regione di interesse ( tumori cerebrali e dellocchio , del capo e collo , polmone , mammella , prostata , retto , tumori ginecologici , sarcomi delle parti molli , metastasi ossee e cerebrali ) nei sedici capitoli del volume . 
the aim of this study was to evaluate the efficacy of endovascular treatment of isolated iliac artery aneurysms ( iiaa ) and compare our data with those reported in the literature . 
from may 2005 to december 2010 , 32 patients ( 31 men and one woman ; mean age 7312 years ) with a total of 40 iiaas underwent endovascular treatment at our institute . 
da maggio 2005 a dicembre 2010 , 32 pazienti ( 31 maschi ed 1 femmina ; et media 7312 anni ) con un totale di 40 iiaa sono stati sottoposti a trattamento endovascolare . 
ad un follow - up medio di 36 mesi , abbiamo ottenuto successo tecnico del 100% ; perviet primaria del 95% e perviet secondaria del 100% ; esclusione dal circolo dellaneurisma dell84 , 6% . 
tale riscontro in linea con i pi recenti dati della letteratura e conferma la sicurezza e la validit a lungo termine del posizionamento di endoprotesi . keywords isolated iliac artery aneurysms endovascular treatment stent - graft interventional radiology parole chiave aneurismi isolati dellarteria iliaca trattamento endovascolare endoprotesi radiologia interventistica radiol med ( 2013 ) 118 : 6273 introduction although relatively infrequent , isolated iliac artery aneurysms ( iiaas ) are associated with a high risk of rupture and patient death . 
an iliac aneurysm is defined as a focal increase in vessel diameter of at least 50% : for example , the common iliac artery ( cia ) is considered aneurysmal when it has a diameter > 1.85 cm in men and > 1.5 cm in women , on account of the difference in size of the healthy vessels in the two sexes [ 1 ]  . 
iiaas are located in the cia in 70% of cases , in the internal iliac artery ( iia ) in 20% of cases , and in the external iliac artery ( eia ) in only 10% of cases [ 2 ]  . 
iliac aneurysms are rarely isolated : 84% of patients , with or without concomitant aneurysm of the abdominal aorta , present with more than one aneurysm of the iliac arteries [ 3 ]  . 
the most common cause of iiaa is atherosclerosis ; less frequent causes are para - anastomotic pseudoaneurysms , penetrating pelvic traumas , iatrogenic lesions , bacterial infections , kawasakis syndrome [ 7 ] , behets disease [ 8 ] , fibromuscular dysplasia [ 9 ] , takayasus arteritis and connective tissue diseases such as cystic medial necrosis [ 10 ] , marfans syndrome and ehlers - danlos syndrome . 
iiaa treatment is indicated if the aneurysm is > 3 cm , if it has a growth rate > 7 mm in 6 months or > 1 cm in a year or if the patient is symptomatic [ 3 , 12 ]  . surgery has been the standard treatment for years and involves either placing an aortobiiliac or aortobifemoral bypass , or endoaneurysmorrhaphy in the case of common iliac artery aneurysms . 
internal iliac aneurysms are instead treated by proximal ligation of the artery , possibly associated with distal ligation , aneurysmectomy combined with graft interposition or aneurysmorrhaphy [ 13 , 14 ]  . 
although surgery generally enjoys high levels of technical success , it is accompanied by several complications such as bleeding , surgical infections , ureteral injury and distal embolisation with lower - limb ischaemia . 
the mortality rate of elective aneurysm surgery is relatively low ( 06.2% ) , whereas that of emergency surgery is significant and ranges from 0% to 55.5% [ 2 , 11 , 12 , 1517 ]  . 
the 5 - year survival rate after elecintroduzione bench relativamente infrequenti , gli aneurismi isolati dellasse arterioso iliaco ( iiaa ) sono associati ad alto rischio di rottura e di morte . 
si definisce aneurisma iliaco un aumento focale del calibro vasale superiore al 50% : ad esempio liliaca comune si definisce aneurismatica quando presenta calibro vasale > 1 , 85 cm nelluomo e > 1 , 5 cm nella donna , in virt del differente diametro del vaso sano nei due sessi [ 1 ]  . 
la maggior parte degli aneurismi iliaci sono associati ad aneurismi dellaorta addominale sottorenale ; gli iiaa sono localizzati nel 70% dei casi a livello delliliaca comune ( cia ) , nel 20% dei casi a livello delliliaca interna ( iia ) e solo nel 10% dei casi a livello delliliaca esterna ( eia ) [ 2 ]  . 
raramente gli aneurismi iliaci sono singoli : l84% dei pazienti , in presenza o meno di contemporaneo aneurisma dellaorta addominale , presenta pi di un aneurisma a livello delle arterie iliache [ 3 ]  . 
la causa pi frequente di iiaa la patologia aterosclerotica ; cause pi rare sono pseudoaneurismi para - anastomotici , traumi pelvici penetranti , lesioni iatrogene , infezioni batteriche , malattia di kawasaki [ 7 ] , malattia di behcet [ 8 ] , displasia fibromuscolare [ 9 ] , arterite di takayasu e patologie del connettivo come la necrosi cistica della media [ 10 ] , la sindrome di marfan e la sindrome di ehlers - danlos . 
gli iiaa sono generalmente asintomatici e la diagnosi posta occasionalmente in corso di esami strumentali eseguiti per altri motivi ; le manifestazioni cliniche pi frequenti sono legate a sintomatologia compressiva a livello delle strutture adiacenti quali il plesso sacrale , il colon , la vena iliaca o luretere ; nel caso di rottura , il paziente generalmente lamenta intenso dolore addominale a rapida insorgenza associato a bradicardia , ipotensione e sudorazio ne [ 5 , 11 ]  . 
la storia naturale degli iiaa la loro progressiva dilatazione sino alla rottura , che dipende dalle dimensioni degli stessi : aneurismi di diametro < 3 cm hanno un tasso di crescita di 0 , 050 , 15 cm / anno mentre aneurismi di diametro > 3 cm di 0 , 28 cm / anno [ 3 ]  . 
il trattamento degli iiaa indicato se le dimensioni dellaneurisma sono di > 3 cm , se laneurisma presenta un tasso di crescita > 7 mm in 6 mesi o > 1 cm allanno o se i pazienti sono sintomatici [ 3 , 12 ]  . lintervento chirurgico ha rappresentato per anni il trattamento standard per tale patologia : esso consiste nel posizionamento di by - pass aorto - bisiliaco o aortobifemorale o nellendoaneurismorrafia per gli aneurismi delliliaca comune ; nella legatura prossimale della stessa , eventualmente associata a legatura distale , nellaneurismectomia associata ad interposizione protesica o nellaneurismorrafia per quelli delliliaca interna [ 13 , 14 ]  . 
lintervento chirurgico generalmente associato ad un alto grado di 64 radiol med ( 2013 ) 118 : 6273 tive surgery is 70% , whereas that of emergency procedures is 55% [ 5 ]  . 
over the last decade , the development of endovascular techniques has made this option extremely interesting for treating iiaas because it combines shorter operative times , a lower incidence of complications and perioperative mortality and excellent long - term results [ 18 , 19 ]  . 
the purpose of our study was to assess the shortand long - term efficacy of the endovascular treatment of iiaas in patients referred to our institute and to compare our results with those reported in the literature . materials and methods between may 2005 and december 2010 , 32 patients ( 31 men and one woman ; mean age , 7312 years ) with a total of 40 iiaas ( mean diameter 4.4 cm ) underwent endovascular treatment at our centre . 
 finally , patients who had undergone surgical exclusion of an abdominal aortic aneurysm with a subsequent de novo diagnosis of iliac aneurysm were included . in seven patients , with a total of nine aneurysms ( mean diameter 5.9 cm ) , the procedure was performed in an emergency setting because of aneurysm rupture ; in the remaining 25 patients , with a total of 31 aneurysms ( mean diameter 4 cm ) , surgery was elective . 
table 1 shows the characteristics of the patients and aneurysms . in all cases , preliminary computed tomography angiography ( cta ) was performed to adequately assess aneurysm characteristics ( site , size , proximal and distal neck , involvement of the aortic and iliac bifurcations ) , take measurements to plan treatment and to select the most suitable stent - gra prior to the procedure , all patients were informed about benefits and risks and provided their informed consent . 
in 14 cases , the procedure was performed under local anaesthesia and with anaesthesiological assistance ( lidocaine 2% ) , in 13 cases under intraspinal anaesthesia and in successo tecnico , ma gravato da una serie di complicanze quali emorragia , infezioni della ferita chirurgica , danno ureterale , embolizzazione distale con ischemia degli arti inferiori . 
la mortalit per gli aneurismi trattati chirurgicamente in elezione relativamente bassa ( 0%6 , 2% ) mentre per quelli in urgenza consistente ed oscilla tra lo 0% ed il 55 , 5% [ 2 , 11 , 12 , 1517 ]  . 
 nellultimo decennio , lo sviluppo delle tecniche endovascolari ha reso questo approccio particolarmente interessante nel trattamento degli iiaa , poich combina una riduzione dei tempi operatori , una minor incidenza di complicanze e di mortalit peri - procedurali , con ottimi risultati a distanza [ 18 , 19 ] , assurgendo , in molti centri , a trattamento di prima istanza , sia in elezione che in urgenza . 
obiettivo del nostro studio valutare lefficacia a breve e lungo termine del trattamento endovascolare degli iiaa sui pazienti pervenuti al nostro istituto e raffrontare i nostri dati con quelli della letteratura . materiali e metodi da maggio 2005 a dicembre 2010 , 32 pazienti ( 31 maschi ed 1 femmina ; et media 7312 anni ) con un totale di 40 iiaa ( diametro medio complessivo 4 , 4 cm ) sono stati sottoposti a trattamento endovascolare . 
di questi , 9 erano localizzati esclusivamente alla cia , 16 alla cia con estensione al carrefour aortico e / o alla biforcazione iliaca , 6 presentavano concomitante localizzazione aneurismatica a livello della cia e delliia , 3 presentavano esclusivo coinvolgimento delliia ( tabella 1 )  . 
sono stati inclusi nello studio pazienti con presenza di malformazione aneurismatica , singola o multipla , localizzata a livello dellasse arterioso iliaco in assenza di concomitante aneurisma a livello dellaorta addominale . 
sono stati esclusi dallo studio pazienti con concomitante presenza di aneurisma dellaorta addominale e sottoposti a trattamento endovascolare ; sono stati invece considerati i pazienti sottoposti precedentemente ad intervento di esclusione di aneurisma dellaorta addominale con successiva diagnosi de novo di aneurisma iliaco . in 7 pazienti , per un totale di 9 aneurismi ( diametro medio 5 , 9 cm ) , la procedura stata eseguita in regime di urgenza a causa di rottura degli stessi ; nei restanti 25 pazienti , per un totale di 31 aneurismi ( diametro medio 4 cm ) lintervento stato eseguito in elezione . 
in 21 cases , bilateral percutaneous access was achieved by inserting a 1218 - fr introducer sheath ipsilateral to the site to be treated and a 5 - fr introducer sheath on the contralateral side in order to obtain a preliminary angiographic evaluation using a calibrated pigtail catheter ( optimed , ettinger , germany )  . 
in 11 cases , unfavourable anatomy necessitated a combined approach , with surgical exposure of the femoral artery ipsilateral to the site to be treated and a contralateral percutaneous puncture . in agreement with published data [ 20 ] , patients with cia aneurysms were treated by stent - graft placement . 
those with aneurysms of the cia and aortic bifurcation were treated with a bifurcated aortic stent - graft and coil embolisation of the iia origin if the iliac bifurcation was involved . 
 patients with concomitant aneurysm of the cia and the iia were treated with stent - graft placement and coil embolisation of the origin and the two distal branches of the hypogastric artery , as were those with isolated aneurysms of the iia . stent - graft size ( mean diameter 16.23.2mm ; mean gimento del carrefour aortico e della biforcazione iliaca ) e per pianificare il trattamento mediante le opportune misurazioni , al fine di scegliere lendoprotesi pi adatta . 
 lintervento stato eseguito in 18 casi in sala angiografica con angiografo integris v5000 ( philips medical system , best , olanda ) ; nei restanti 14 casi in sala operatoria ibrida con angiografo portatile bv300 ( philips medical system , best , olanda )  . 
in 14 casi la procedura stata eseguita in anestesia locale ed assistenza anestesiologica ( lidocaina 2% ) , in 13 casi in anestesia spinale e in 5 casi in anestesia generale . 
if the stent - graft was incompletely sealed or if there was evidence of type ii endoleaks after placement , in - stent angioplasty was performed . before releasing the stent - graft , the hypogastric artery was embolised during the procedure by means of contralateral femoral access , selective catheterisation of the iia with a hooked catheter and delivery of platinum coils . 
during the procedure , patients were administered an intra - arterial bolus of 5 , 000 iu heparin , and in the postoperative period , they received subcutaneous low - molecular - weight heparin ( lovenox 40 mg , bracco , milan , italy ) every 12 h for 3 days , clopidogrel 75 mg / day for 6 weeks and ticlopidine 120 mg / day or acetyl salicylic acid ( asa ) 100 mg / day lifelong . 
the follow - up was done with cta or contrast - enhanced ultrasound ( ceus ) at 1 , 6 and 12 months and yearly thereafter . results the nine patients with isolated cia aneurysm were treated with tubular uni - iliac stent - grafts of the following types : zenith ( cook , bloomington , in , usa ) ( four cases ) , fluency ( bard , murray hill , nj , usa ) ( two cases ) , excluder ( wl gore , flagstaff , az , usa ) ( three cases )  . 
the nine patients with cia aneurysm involving the aortic bifurcation were treated with the following aortobiiliac stent - grafts : excluder ( wl gore ) ( seven cases ) and zenith ( cook ) ( two cases )  . 
 the three patients with cia aneurysm extending proximally to the aortic bifurcation and distally to the iliac bifurcation were treated with aortobiiliac stent - grafts , such as excluder ( wl gore ) ( one case ) , zenith ( cook ) ( one case ) and valiant ( medtronic , sunnyvale , ca , usa ) ( one case ) , as well as embolisation of the iia origin using balt platinum coils ( ab medica , milan , italy )  . 
the four patients with cia aneurysm extending to the iliac bifurcation were treated with the following uni - iliac stent - grafts : fluency ( bard ) ( two cases ) , zenith ( cook ) ( one case ) and excluder ( wl gore ) ( one case ) and with iia embolization of the origin using balt ( ab medica ) and vortex ( boston scientific , natek , na , usa ) platinum coils . 
in caso di incompleto sealing dellendoprotesi o di evidenza di endoleak di ii tipo dopo il rilascio della stessa stata eseguita angioplastica allinterno della protesi . lembolizzazione dellipogastrica stata effettuata durante lintervento , prima del rilascio dellendoprotesi , mediante accesso femorale controlaterale , cateterismo selettivo delliliaca interna con catetere uncinato e rilascio di spirali in platino . 
only one perioperative complication occurred , which was during treatment of a cia aneurysm extending to the aortic bifurcation with a zenith ( cook ) aortouniiliac stent - graft : during withdrawal of the device , the iliac extension migrated caudally up to the vicinity of the inguinal ligament , resulting in incorrect seal between the body and the extension . 
because the patient also presented with occlusion of the contralateral iliac axis , at the end of the endovascular time , a femorofemoral bypass was constructed , which allowed preservation of pelvic and lower - limb flow . 
in due casi di aneurisma della cia coinvolgente la biforcazione iliaca ( uno esteso sino al carrefour aortico ) trattati rispettivamente in urgenza ed in elezione , non stata effettua ta lembolizzazione dellipogastrica , nel primo caso per ridurre i tempi procedurali a causa della condizione di shock emodinamico del paziente e nellaltro per la presenza di steno - occlusione allorigine delliia . 
si avuta solo una complicanza peri - procedurale realizzatasi durante il trattamento di aneurisma della cia esteso al carrefour aortico mediante endoprotesi aorto - monoiliaca zenith ( cook , bloomington , in , usa ) : si verificata la migrazione caudale , sino in prossimit del legamento inguinale , dellestensione iliaca durante la fase di ritiro del device con conseguente mancato seeling tra il corpo e lestensione . 
durante il follow - up sono deceduti 4 pazienti ( 12 , 5% ) : uno al secondo giorno post - operatorio per arresto cardiocircolatorio ( numero totale di pazienti sottoposti a follow - up : 31 ) , due a circa 24 mesi dallintervento , rispettivamente per progressione di malattia neoplastica e per infarto miocardico ed il 4 paziente a 32 mesi per insufficienza renale cronica ( irc ) terminale . 
in 5 / 39 aneurismi trattati ( 12 , 8% ) abbiamo riscontrato la presenza di endoleak di ii tipo : di questi , 2 erano in pazienti con aneurisma della cia esteso al carrefour aortico , 1 in paziente con aneurisma isolato della cia e due nei casi descritti di copertura dellipogastrica con endoprotesi senza embolizzazione della stessa . 
2 cta performed 24 months after the procedure documents the outcome of the placement of an aortouniiliac stent - graft landing in the external iliac artery due to caudal migration of the external iliac leg during delivery , with complete exclusion of the cia aneurysm extending to the aortic bifurcation . 
si documentano gli esiti del posizionamento di endoprotesi aorto - monoiliaca ad atterraggio in iliaca esterna per migrazione caudale della gamba iliaca durante il rilascio , con completa esclusione dal circolo dellaneurisma delliliaca comune esteso al carrefour aortico . 
il by - pass crociato femoro - femorale destro - sinistro ha consentito di preservare il flusso pelvico e dellarto inferiore controlaterale , con risultati duraturi nel tempo . one at 32 months due to end - stage chronic kidney disease . 
in 5 / 39 aneurysms ( 12.8% ) , we found type ii endoleaks : two were in patients with cia aneurysm extending to the aortic bifurcation , one in a patient with an isolated cia aneurysm and two in the cases of coverage of the hypogastric artery with stent - graft without embolisation . 
one patient with iia aneurysm treated on an emergency basis with placement of an iliac stent - graft without preventive coil embolisation of the hypogastric artery presented at the 3 - year follow - up with complete exclusion and thrombosis of the aneurysm radiol med ( 2013 ) 118 : 6273 fig . 
there were two cases ( 5% ) of thrombotic occlusion of the stent - graft at 1 and 6 months , respectively , resulting from a residual stenosis affecting the branch facing towards the new bifurcation in patients with tight bifurcation ; both were treated successfully with an intra - arterial fibrinolysis and angioplasty . 
in three cases ( 60% ) , this was transient and resolved within months , in two cases ( 40% ) it was persistent , and in one case ( 3.2% of the total ) it was associated with sexual dysfunction . 
compared with surgery , the endovascular approach allows the aneurysm to be treated without the need for deep pelvic dissecdeciso di soprassedere da ogni tentativo di trattamento e di osservarli soltanto nel tempo . 
abbiamo avuto due casi ( 5% ) di occlusione trombotica della protesi , rispettivamente a 1 e 6 mesi dal posizionamento della stessa in rapporto a residuo di stenosi a carico della branca protesa al neocarrefour in pazienti con carrefour stretto , trattati entrambi con successo mediante terapia fibrinolitica intra - arteriosa ed angioplastica ; i controlli a distanza hanno documentato perviet del graft in assenza di iperplasia intimale e / o restenosi intra - stent . 
otto pazienti ( 25 , 8% ) ( 5 con aneurisma della cia esteso alla biforcazione iliaca , 2 con aneurismi della cia e della iia , 1 con aneurisma della iia ; tutti trattati con spirali ) hanno lamentato claudicatio glutea , in tre casi ( 60% ) transitoria e risoltasi dopo pochi mesi ed in due casi ( 40% ) persistente , associata , in un caso ( 3 , 2% del totale ) , a deficit sessuali . 
la sopravvivenza complessiva ad 1 , 2 , 3 , e 6 anni stata del 96 , 8% , 84 , 2% , 66 , 6% , 64% rispettivamente . 70 radiol med ( 2013 ) 118 : 6273 discussione il trattamento degli iiaa mediante approccio endovascolare ( eviar , endovascular iliac artery aneurysm repair ) diventato , negli ultimi anni , una opzione interessante ed efficace . 
rispetto alla chirurgia , lapproccio endovascolare consente il trattamento dellaneurisma senza necessit di dissezione pelvica profonda , rischiosa in pazienti con concomitanti problematiche cardio - respiratorie , obesi o gi trattati chirurgicamente in sede pelvica o addominale [ 7 ]  . 
la ridotta invasivit del trattamento endovascolare consente la riduzione della degenza post - operatoria , delle complicanze post - procedurali e fornisce unopzione di cura a pazienti con gravi comorbilit cardio - respiratorie , che non potrebbero essere trattati chirurgicamente . 
a fronte degli alti rischi procedurali correlati allintervento chirurgico [ 12 ] , lapproccio endovascolare nonostante le potenziali complicanze rappresentate da ischemia colica , embolizzazione distale , trombosi della protesi , infezioni ed endoleak con possibile incremento volumetrico della sacca aneurismatica fino alla sua rottura [ 18 ] , rappresenta una opzione pi sicura rispetto ai rischi procedurali correlati allintervento chirurgico [ 12 ] , con efficacia duratura a lungo termine [ 1830 ]  . nel recente confronto tra 24 pazienti trattati chirurgicamente e 32 trattati per via endovascolare , patel et al . 
 [ 22 ] , nel confronto tra trattamento chirurgico ( 394 pazienti ) ed endovascolare ( 44 pazienti ) , riportano simili perviet primaria e secondaria ( 99 , 6% ) a 5 anni dallintervento , sopravvivenza libera da ulteriori interventi e sopravvivenza complessiva ma a fronte di una riduzione della mortalit , delle complicanze post - operatorie e del tempo di degenza nel gruppo eviar . 
 [ 24 ] , riscontrano una riduzione del tempo operatorio , delle perdite ematiche , della degenza e delle complicanze post - operatorie nei pazienti trattati mediante eviar , con una perviet primaria nel primo studio del 97% a tre anni dallintervento e nel secondo studio del 100% a due anni . 
nella nostra esperienza , ( 32 pazienti con 40 iiaa ) con follow - up medio di 36 mesi , abbiamo ottenuto successo tecnico in tutti i pazienti in assenza di complicanze maggiori peri - procedurali ; in un caso si verificata la migrazione caudale della protesi , trattata prontamente mediante interposizione di estensioni iliache . 
in special situations , such as emergencies or tight stenosis of the origin , iia aneurysms can be treated with stent - graft placement , with good results over time . 
gli altri due casi trattati in questo modo hanno sviluppato endoleak di ii tipo , senza tuttavia incremento volumetrico della sacca aneurismatica . tion , which is dangerous in patients with concomitant cardiorespiratory problems , obese patients or those with previous pelvic or abdominal surgery [ 7 ]  . 
the low invasiveness of the endovascular treatment allows for shorter postoperative hospital stay and reduced postprocedural complications and offers a treatment option to patients with serious cardiorespiratory comorbidities who are not eligible for surgery . 
 despite the potential complications of bowel ischaemia , distal embolisation , stent - graft thrombosis , infections and endoleaks with possible enlargement and rupture of the aneurysm sac [ 18 ] , the endovascular approach offers not only a safer option than surgery with all its procedural risks [ 12 ] , but also long - term efficacy [ 1830 ]  . in the recent comparison of open surgery ( 24 patients ) and eviar ( 32 patients ) , patel et al . 
 [ 22 ] , in their comparison of surgery ( 394 patients ) and endovascular treatment ( 44 patients ) , reported similar primary and secondary patency rates ( 99.6% ) at 5 years , similar survival free from radiol med ( 2013 ) 118 : 6273 reintervention and overall survival , but with a reduction in mortality rate , postoperative complications , and hospitalisation for the eviar group . 
 [ 24 ] noted a reduction in operative time , blood loss , hospital stay and postoperative complications in patients treated with eviar , with a primary patency rate of 97% at 3 years in the former study and of 100% at 2 years in the latter one . 
in our experience with 32 patients and 40 iiaas , with a mean follow - up of 36 months , technical success was achieved in all patients without any major perioperative complications . 
in our experience , the endoleak rate was 12.8% , which is in line with the literature : in all cases , they were low - flow type ii leaks from the hypogastric artery , for which no treatment was given and which caused no enlargement and / or rupture of the aneurysm sac . 
 in two cases , they were cia aneurysms extending to the iliac bifurcation , which were treated with stent - grafts but without iia coil embolisation one because the procedure was performed under emergency conditions and the other because of severe stenosis of the origin of the hypogastric artery . 
this stresses the importance of iia embolisation in preventing endoleaks , as recommended in all studies , even though the development of lowflow endoleaks without any enlargement of the aneurysm leads us to believe that , under emergency conditions or / and in patients with unfavourable anatomy , embolisation can be omitted without affecting the long - term efficacy of the procedure . 
in our experience , the endovascular treatment of iiaas is a safe and effective option with long - lasting results , and as such , it is the first - choice treatment at our centre . 
in maniera analoga ai dati della letteratura [ 1829 ] , non abbiamo riscontrato alcun decesso correlato alla procedura , con un tasso complessivo di sopravvivenza ad 1 , 2 , 3 , e 6 anni del 96 , 8% , 84 , 2% , 66 , 6% , 64% rispettivamente . 
i nostri tassi di perviet primaria ( 95% ) e secondaria ( 100% ) sono analoghi a quelli ottenuti nelle pi ampie casistiche internazionali , come quella recentemente presentata da boules et al . 
nella nostra esperienza abbiamo riscontrato una percentuale di endoleak del 12 , 8% , in linea con i dati della letteratura : si trattava in tutti i casi di leak di ii tipo a basso flusso a , partenza dallipogastrica , per i quali non stato effettuato alcun trattamento e che non hanno comportato incremento e / o rottura della sacca aneurismatica . 
in due casi si trattava di aneurismi delliliaca comune estesi alla biforcazione iliaca trattati mediante endoprotesi ma senza embolizzazione con spirali delliia , perch eseguito luno in regime durgenza e laltro per presenza di stenosi severa allorigine dellipogastrica ; in un paziente portatore di aneurisma isolato delliia stato utilizzato un endograft senza embolizzazione dellaneurisma , al fine di ridurre i tempi procedurali perch eseguito in urgenza . 
ci ribadisce limportanza dellembolizzazione delliia nella prevenzio ne dellendoleak , raccomandata in tutti gli studi , ma lo sviluppo di endoleak a basso flusso in assenza di aumento volumetrico dellaneurisma ci fa ritenere che in situazioni di emergenza o / e in presenza di anatomia sfavorevole si possa soprassedere alla embolizzazione , senza inficiare lefficacia a lungo termine della procedura . 
la bas sa percentuale di riduzione volumetrica della sacca aneurismatica ( 12 , 8% ) da noi osservata in linea con dati della letteratura [ 2129 ] , cos come lincidenza di claudicatio glutea ( 25 , 8% ) , nella maggior parte dei casi transitoria . 
 il trattamento degli iiaa per via endovascolare rappresenta , nella nostra esperienza , una opzione sicura , efficace e con risultati duraturi nel tempo ed nel nostro istituto il trattamento di prima scelta nella gestione di tale patolo gia . 
sono stati ottenuti , nella maggior parte dei casi lesclusione dal circolo degli aneurismi e la perviet del graft con riduzione del tempo operatorio , delle complicanze peri e post - procedurali e della mortalit , sia in elezio72 radiol med ( 2013 ) 118 : 6273 in a shorter operative time , with fewer periand postprocedure complications and lower mortality rates under both elective and emergency conditions compared with surgery . 
 the limitations of our study are its retrospective design and the limited number of patients enrolled ; iiaa is , however , a rare condition for which no prospective studies have been published to date . 
we therefore believe , based on our experience , that endovascular treatment is the first choice in the management of isolated aneurysms of the iliac arterial axis . ne che in urgenza , rispetto allintervento chirurgico . 
 i limiti del nostro studio sono la natura retrospettiva dello stesso e il numero non elevato di pazienti inclusi ; trattasi comunque di patologia rara per la quale non disponiamo attualmente di studi prospettici . 
pastorino4 1sezione di radiologia , dipartimento di scienze radiologiche e istocitopatologiche , universit di bologna , bologna , italy 2sezione di radiodiagnostica , dipartimento di fisiopatologia clinica , universit di firenze , firenze , italy 3sezione di radiodiagnostica , dipartimento di scienze cliniche , universit di parma , parma , italy 4chirurgia toracica , istituto nazionale tumori , milano , italy correspondence to : m . 
the aim is to present the main theoretical and practical problems related to lung cancer screening , the historical background and results of observational studies and the main ongoing randomised controlled trials . 
 the opinion of the authors is that too many questions are still awaiting an answer . keywords lung cancer cancer screening ct scan riassunto a dieci anni dai primi lavori sullargomento , questo editoriale fa il punto della situazione sullo screening del tumore polmonare mediante tomografia computerizzata ( tc ) a bassa dose . 
vengono esposti i principali problemi teorici e pratici connessi alla screening oncologico per il tumore polmonare , le premesse storiche , i risultati degli studi osservazionali ed i principali trial randomizzati e controllati in corso . 
vengono esposti i risultati , insieme alle molte questioni ancora irrisolte e alle domande che attendono una risposta . parole chiave carcinoma polmonare screening tc introduction introduzione ten years ago , in the pages of this journal , one of the authors published a paper on screening for lung cancer using lowdose spiral ct [ 1 ]  . 
the aim of that publication was to present the main problems associated with screening , but the final , takehome message was rather simple : it was too early to think about activating mass screening ; we needed to learn more in order to avoid being misled by common sense . 
 dieci anni fa , sulle pagine di questa rivista , uno di noi pubblic un articolo riguardante lo screening del tumore polmonare mediante tomografia computerizzata ( tc ) spirale a bassa dose [ 1 ]  . 
quella pubblicazione aveva lo scopo di esporre i principali problemi connessi con questo tipo di screening , ma il messaggio di fondo era semplice : troppo presto per pensare di attivare uno screening di massa ; inoltre , in questo campo , il senso comune pu essere ingannevole . 
lung cancer is the leading cause of cancer mortality and is responsible for 30% of cancer deaths , killing more individuals than cancers of the breast , prostate , colon , liver and kidney combined . 
the main reason for treatment failure is that first diagnosis occurs when the disease has already reached an advanced stage in 70% of cases ; only 20% of patients can undergo surgery ; for patients with an advanced stage , the 5 - year survival is around 15% , as against > 50% in tumours resected at stage 1 . 
the large randomised controlled trials ( rct ) of the 1970s based on chest radiography ( cxr ) with or without sputum cytology gave unsatisfactory results , mainly because of the low sensitivity of cxr . 
on the other hand , we have learnt a great deal from these results , which revealed , for example , an apparent paradox : in the screened group ( the intervention arm ) , the overall 5 - year survival increases , but specific mortality due to lung cancer is not reduced . 
moreover , the 20 - year follow - up of this trial , performed by the mayo clinic [ 6 ] , showed an increase in mortality of 11% in the intervention arm compared with the usual - care arthis paradox could be explained as a consequence of the socalled lead - time bias ( diagnostic anticipation ) , added to the effects of the inappropriate medical and surgery treatments . 
 [ 7 , 8 ] ; the positive results are less frequent in the case of incidence screening ( subsequent annual examinations ) ; ct scans had an accuracy rate twoto four - times higher than cxr in identifying low - stage peripheral lung tumours . 
since those first experiences , several observational studies have been performed internationally and in italy [ 911 ] , although some of them are based on a very small number of participants and therefore are of limited significance . 
 radiol med ( 2013 ) 118 : 5161 uno screening di questo tipo poteva legittimamente essere avviato solo per motivi di studio . il problema riassumiamo di seguito i termini della questione , come si sono andati precisando negli anni trascorsi [ 35 ] : 1 . 
i grandi studi randomizzati e controllati ( rct ) degli anni 70 del secolo scorso , basati sul radiogramma del torace ( rx ) , con o senza citologia dellescreato , hanno dato risultati negativi , soprattutto a causa della scarsa sensibilit del rx , ma ci hanno insegnato molto . 
tra laltro , da essi emerso un apparente paradosso : nel gruppo sottoposto a screening ( il braccio attivo ) la sopravvivenza a 5 anni aumenta , mentre nello stesso gruppo la mortalit specifica , cio dovuta al tumore polmonare , non si riduce . 
anzi , la prosecuzione per oltre 20 anni dello studio principale , quello della mayo clinic [ 6 ] ha evidenziato un aumento della mortalit dell11% nel braccio attivo , rispetto a quello di controllo . 
il paradosso una conseguenza del cosiddetto lead time bias ( anticipazione diagnostica ) , sommato agli effetti dellincontro ( diciamo cos ) intempestivo con la medicina e soprattutto con la chirurgia . 
lintroduzione della tc spirale ha dimostrato che lindagine a bassa dose in grado di mostrare la presenza di noduli polmonari con frequenza almeno 3 volte superiore al rx , noduli neoplastici con frequenza circa 4 volte superiore e tumori in basso stadio con frequenza 24 volte maggiore . 
la detection rate della tc per piccoli tumori periferici nei soggetti sottoposti allo screening di prevalenza ( la prima tc ) negli studi osservazionali ( non randomizzati ) va da 0 , 5% a 2 , 7% . 
a seguito delle prime esperienze , sono stati avviati vari studi osservazionali , anche in italia [ 911 ] , alcuni dei quali per basati su un numero molto piccolo di partecipanti e quindi poco significativi . 
 radiol med ( 2013 ) 118 : 5161 observational studies with low - dose ct studi osservazionali con tc a bassa dose as we were accumulating experience , some of the many problems anticipated in 2001 emerged with evidence [ 1 ] : 1 . 
of course , the diagnostic assessment of a nodule requires adjunctive investigations , such as follow - up ct studies , contrast - enhanced ct and nuclear medicine examinations , with an increase of radiation dose and cost as well as invasive and risky procedures and anxiety for the patients and their relatives . 
meanwhile , many inconsistencies and contradictions of the elcap studies have been noted [ 19 ] , and doubts have been cast about the reliability of ct screening in determining the so - called stage shift [ 20 ] ( reduction of advanced malignancies , with a simultaneous increasing in the identification of low - stage tumours ) , which is an indispensable prerequisite for considering the usefulness of screening . 
above all , it became clear that the possible benefit of screening should only be assessed on the basis of mortality , considered as the primary endpoint of rct studies . 
survival should not be conmano a mano che le esperienze degli studi osservazionali si andavano accumulando , emergevano con evidenza alcuni dei tanti problemi anticipati nel 2001 [ 1 ] : 1 . 
naturalmente , il riscontro di un nodulo indeterminato richiede di adottare controlli pi ravvicinati con tc a bassa dose , eventuali studi tc diagnostici a dose piena e con iniezione di contrasto , esami medico - nucleari ( fluordeossiglucosio - tomografia ad emissione di positroni , fdg - pet ) , procedure di biopsia sotto guida tc e dunque comportano aumento della dose radiante e dei costi , nonch procedure invasive e rischiose , comprensibile ansiet del soggetto e dei suoi familiari . 
un aspetto particolare poi rappresentato dalla incapacit dello screening con tc a bassa dose annuale di identificare in fase precoce il microcitoma , in rapporto alla velocissima crescita di questa neoplasia che , sebbene in diminuzione , rappresenta tuttora il 15%18% dei tumori polmonari maligni e che fortemente associata al fumo [ 17 ]  . 
inoltre persistevano molti dubbi sul fatto che lo screening tc fosse in grado di determinare lo stage shift [ 20 ] , cio la riduzione delle neoplasie in stadio avanzato con contemporaneo aumento dei tumori in basso stadio ; premessa questa indispensabile per poter considerare la 54 radiol med ( 2013 ) 118 : 5161 sidered a good parameter , because it is influenced by the type of diagnostic approach and by various biases ( including lead time )  . 
due to lack of space , technical and organisational problems that would be connected to a hypothetical mass screening [ 2124 ] , economic evaluation of cost - effectiveness [ 25 ] and ethical , social and political open questions will not be discussed here . 
the incidental finding or the screen - detection of a small - sized tumour anticipates the diagnosis and is therefore always associated with an apparent increase in survival , even without any therapy . 
if you consider mortality instead of survival as an endpoint , you avoid falling into this trap , but this can be achieved only in rct studies and not observational trials due to the lack of a usual - care ara second bias ( length time ) is related to the fact that slow - growing tumours present an asymptomatic phase ( preclinical ) longer than fast - growing tumours . 
as in breast cancer , the missed tumours are the more aggressive ( interval cancers ) , which are diagnosed when clinical signs and symptoms develop in the interval between a screening test and the following one . 
the time when metastatic dissemination starts , which can occur when the tumour is very small ( 1to 2 - mm ) in many cases , because of early angiogenesis . 
however , perhaps the most insidious bias is the third one , the so - called overdiagnosis , which can be of two types [ 1 ] and can lead to contaminated results in rct studies . 
 tumours with a volume - doubling time ( vdt ) > 400 days represent up to 1 / 3 of screen - detected cancers , and possibile utilit dello screening . 
anche cos , peraltro ( lo anticipiamo perch si possa capire quanto segue ) , un beneficio inferiore al 20% di fatto non individuabile , perch per dimostrarlo sarebbero necessari trial giganteschi , con costi proibitivi . 
per motivi di spazio , non affronteremo qui i problemi tecnici ed organizzativi che sarebbero collegati ad un ipotetico screening di massa [ 2124 ] , le compatibilit economiche e la valutazione del rapporto costo / beneficio [ 25 ] , le questioni aperte sul piano etico , sociale e politico . 
 lindividuazione casuale o allo screening di un tumore di piccole dimensioni anticipa la diagnosi e quindi sempre associata ad un apparente aumento della sopravvivenza , anche in assenza di qualunque terapia . 
usare la mortalit come end - point , piuttosto che la sopravvivenza , evita di cadere in questa trappola , ma ci pu essere realizzato solo in rct e non in studi osservazionali , senza braccio di controllo . 
un secondo bias ( length time ) legato al fatto che i tumori a lenta crescita hanno una fase asintomatica ( pre - clinica ) molto pi lunga di quelli a crescita rapida . 
nel caso del cancro polmonare ( come in quello mammario ) a sfuggire sono proprio i tumori pi aggressivi ( interval cancers ) , tipicamente il microcitoma , che vengono diagnosticati sulla base di segni e sintomi , nellintervallo fra un esame di screening e laltro . 
purtroppo ancora impossibile , nel singolo caso , individuare il punto critico nella storia naturale della malattia , cio il momento in cui inizia la disseminazione metastatica , che in molti casi avviene quando il tumore piccolissimo ( 12 mm ) , in rapporto ai fenomeni di angiogenesi neoplastica . 
esso pu inquinare anche gli studi rct e consiste nella individuazione di un nodulo che davvero un tumore maligno ma che non destinato ad radiol med ( 2013 ) 118 : 5161 they are reported to be more frequent in women [ 29 ]  . 
 thus , in an elderly patient with major comorbidities , the screening report of a cancer of this kind in fact determines a shortening and worsening in quality of life ( another apparent paradox )  . 
starting from the historical studies about epidemiological autopsy [ 31 ] , several authors state that probably only a minority of all lung cancers become symptomatic intravitam before death occurs for other reasons . 
this conclusion is not surprising when considering the long vdt of the former bronchioloalveolar carcinoma ( today called adenocarcinoma in situ or minimally invasive ) or of premalignant lesions , such as atypical adenomatous hyperplasia ( a frequent cause of overdiagnosis accounting for > 20 % of small peripheral screen - detected nodules ) [ 32 ]  . 
on the other hand , the life expectancy of a heavy smoker > 70 years of age is < 5 years ; moreover , in patients with lung cancer , the relative risk of death of other causes is three times higher than in controls and even higher than in patients with other solid tumours . 
some of them are so aggressive and metastasise so early that they cannot be detected in any way ; others present such a slow growth that an overdiagnosis bias occurs . there is still much to learn about lung cancer and about the integration of different techniques that allow its early detection and characterisation [ 33 ]  . 
in addition , it would be certainly highly useful to develop a better classification of the highest - risk groups ( pretest stratification ) by identifying functional , clinical and radiological markers , genetic and proteomic biomarkers or applying the electronic nose to detect other significant risk factors independent of smoking history , as functional airflow obstruction appears to be [ 3436 ]  . 
 as a consequence of the above , it is evident that nonrandomised , single - arm , observational studies can only point out the possible usefulness of screening but cannot provide any decisive results in this regard . 
 in italy , the screening programme involves three studies : italung , detection and screening of early lung cancer ( dante ) , multicentric italian lung detection ( mild ) [ 33 , 37 , 38 ]  . 
 in that trial , a 3 - year interim analysis of results showed no significant difference in either all - cause or lung - cancer - specific mortality rates between the two cohorts . 
i tumori con tempo di raddoppio volumetrico ( vdt ) superiore a 400 giorni rappresentano circa 1 / 3 delle neoplasie individuate allo screening e si osservano soprattutto nel sesso femminile [ 29 ]  . 
trovare allo screening un tumore di questo tipo in un anziano con importanti comorbilit significa in pratica accorciare e peggiorare la vita che gli resta ( un altro apparente paradosso )  . 
vari studi , a partire da quelli ormai storici di autopsia epidemiologica [ 31 ] indicano che , probabilmente , solo una minoranza di tutti i tumori polmonari producono sintomi intra - vitam , prima cio che avvenga il decesso per altre ragioni . 
pensiamo ai lunghi tempi di raddoppio del carcinoma bronchiolo - alveolare ( oggi adenocarcinoma in situ o minimamente invasivo ) oppure di forme preneoplastiche come la iperplasia adenomatosa atipica , causa frequente di sovradiagnosi . 
daltro canto , laspettativa di vita di un forte fumatore ultrasettantenne inferiore a 5 anni ed il rischio relativo di decesso per altre cause nei pazienti con tumore polmonare tre volte superiore a quello dei controlli e molto pi elevato rispetto a quello di pazienti con altre neoplasie solide . 
inoltre , sarebbe certo molto utile definire meglio ( stratificare pre - test ) i gruppi a maggior rischio , individuando marcatori funzionali , clinici , radiologici , biomarkers genetici , proteomici o utilizzando il naso elettronico per selezionare fattori di rischio indipendenti e significativi da integrare con la storia di fumo , come sembrerebbe essere la compromissione di tipo ostruttivo alle prove di funzionalit respiratoria [ 3436 ]  . da quanto abbiamo detto , risulta fra laltro con evidenza che gli studi osservazionali non randomizzati , a braccio singolo , non possono fornire risultati decisivi , ma possono soltanto indicare la possibilit che lo screening sia utile . 
tra essi , il dante trial ha caratteristiche del tutto peculiari e difficilmente 56 radiol med ( 2013 ) 118 : 5161 initiated british screening programme has some interesting features ( single - screen design ) and may demonstrate in the future a reduction in specific mortality of at least 30 % [ 39 ]  . 
in europe , the main study is the ongoing dutchbelgian randomised lung cancer multi - slice ct screening trial ( nelson ) launched in 2003 , results of which are expected between 2012 and 2016 [ 41 ]  . 
it involves nearly 15 , 000 participants and provides only clinical observation for the usual - care arm ( as , in general , in all european studies )  . 
one important result that has already emerged from this trial is that even benign lesions may show a significant growth , given that 85 % of nodules with a vdt < 400 days after a 3 month - observation are , in fact , benign [ 41 ]  . 
that trial , unlike european ones , offered cxr for the usual - care arm , enrolled about 54 , 000 people , provided three rounds of annual screening and a follow - up for a maximum period of 8 years after randomisation , with a cost of us $250 million ( cost of each ct $300500 )  . 
age of the enrolled participants ranged from 55 to 74 years and smoking history was of at least 30 packyears ( one pack / day for 30 years )  . 
participants were inhabitants of large us cities , were on average younger and with a higher educational level than the general population of smokers ( the typical participation bias already mentioned in the literature ) [ 42 ]  . 
the nlst study was interrupted a couple of years earlier than expected because the authors claimed to have achieved a demonstrable benefit and that therefore it would not have been ethical to continue . 
unexpectedly , the announcement of trial discontinuation due to excess benefit was made in the media ( new york times , 4 november 2010 ) , more than 6 months before the publication of part of the results in a scientific journal [ 43 ]  . 
this inversion of the physiological flow of health information from the scientific community to the media is likely related to the risk of medicolegal implications of keeping participants at high risk in the usual - care arm , where they were paragonabili a quelle degli altri studi . 
 anche lo screening britannico , appena avviato , ha alcune peculiarit interessanti ( single screen design ) e potr , a termine , evidenziare una riduzione della mortalit specifica non inferiore al 30% [ 39 ]  . 
in europa , oltre allo studi danese ( dlcst ) , lo studio principale , tuttora in corso , quello belga - olandese ( nelson trial ) , partito nel 2003 , i cui risultati sono attesi nel 2015 [ 41 ]  . 
l85% dei noduli con vdt inferiore a 400 giorni dopo 3 mesi di osservazione , risultano infatti benigni [ 41 ]  . lo studio di gran lunga pi importante per quello americano ( national lung screening trial , nlst ) , avviato nel 2002 in 33 centri , da parte del national cancer institute e dellamerican college of radiology imaging network [ 42 ]  . 
questo trial , che , a differenza di quelli europei , offriva per il braccio di controllo lrx del torace , ha arruolato circa 54000 volontari , per tre anni consecutivi di screening seguiti da un follow - up massimo di otto anni dalla randomizzazione , con un costo di 250 milioni di dollari . 
let dei soggetti arruolati variava da 55 a 74 anni ; la storia di fumo era di almeno 30 pacchi / anno , quindi particolarmente importante ( equivalente ad un pacchetto al giorno per 30 anni )  . 
lo studio nlst stato interrotto con un paio di anni di anticipo rispetto al previsto , perch gli autori hanno dichiarato di aver raggiunto un beneficio dimostrabile e che quindi non sarebbe stato etico proseguire . 
inopinatamente lannuncio dellinterruzione per eccesso di beneficio stato fatto sui media ( new york times del 4 novembre 2010 ) , pi di 6 mesi prima della pubblicazione di una parte dei risultati su una rivista scientifica [ 43 ]  . 
tale inversione del fisiologico flusso di informazioni concernenti la salute fra comunit scientifica e media verosimilmente legato ai rischi di implicazioni radiol med ( 2013 ) 118 : 5161 offered the apparently less useful examination ( cxr ) for reducing mortality . 
the prevalence of nodules , relatively low compared with other studies , is due to the choice of considering only those with a diameter > 4 m the incidence of lung cancer was of 2.4% in the intervention arm and 2.1% in the usual - care ar more than 60% of detected cancers were stage 1 . 
a total of 796 deaths from lung cancer were documented : 356 in the intervention arm ( corresponding to a cumulative mortality rate for cancer of 247 per 100 , 000 per year ) versus 443 in the usual - care arm ( corresponding to 309 per 100 , 000 per year )  . 
 moreover , 20% is the minimal potentially detectable benefit in such a study and , according to the mathematical models used in such cases , a reduction in specific mortality rates > 40% would probably be cost effective , whereas a 20% reduction would not [ 25 ]  . 
it is easy to conclude that it is very unlikely that studies with lower statistical power , such as the european ones still in progress , will be able to confirm or refute the minimum useful result emerging from the american trial , even without considering the difficult comparison between studies with such different designs . 
finishing the trial might have possibly shown a more significant benefit , but it could also have resulted in a risk of increasing overdiagnosis bias , with contamination of the results . 
in fact , it is known from the literature that the early closure of an rct study can overestimate usefulness ( too good to be true ) , and various authors suggest that the results of rcts stopped early should be considered with some scepticism [ 4446 ]  . 
it showed a statistically significant reduction in general mortality of 6.7% in the intervention arm compared with the usual - care arm , with only one fourth due to lung cancer and the remaining three fourths to cardiovascular causes . 
if we exclude the proportion linked to cancer , the difference is no medico - legali , particolarmente elevati nella societ statunitense , nel mantenere nel braccio di controllo soggetti ad alto rischio cui era stata prospettata lindagine apparentemente meno utile per ridurre la mortalit ( cio lrx )  . proviamo insieme ad analizzare i risultati pubblicati [ 43 ]  . 
gli esami positivi per noduli indeterminati sono stati tre volte pi frequenti fra i primi ( 24 , 2% versus 6 , 9% ) , ma moltissimi noduli sono infine risultati benigni , cio falsi positivi ( 96 , 4% versus 94 , 5% )  . 
 nel braccio attivo , 16 pazienti sono deceduti entro due mesi da una biopsia eseguita per valutare un nodulo scoperto alla tc ; 6 di questi non avevano un cancro . 
si sono registrati 796 decessi da tumore polmonare in totale , di cui 356 nel braccio attivo ( corrispondenti ad una mortalit cumulativa per cancro di 247 / 100000 / anno ) versus 443 nei controlli ( corrispondenti a 309 / 100000 / anno )  . 
questa cifra corrisponde alla dichiarata riduzione di mortalit specifica nel braccio attivo del 20 , 3% [ p = 0 , 004 ; intervallo di confidenza ( ci ) 95% ]  . 
facciamo inoltre notare che il 20% il beneficio minimo potenzialmente rilevabile in uno studio con simili caratteristiche e che , secondo i modelli matematici utilizzati in questi casi , una riduzione della mortalit specifica superiore al 40% sarebbe probabilmente cost - effective , una inferiore al 20% no [ 25 ]  . 
si pu facilmente dedurre che molto improbabile che rct di potenza statistica inferiore , come quelli europei tuttora in corso , possano confermare e tantomeno smentire il risultato minimo utile che emerge dal trial americano , anche senza considerare le difficolt derivanti dal paragone fra studi dal disegno cos diverso . 
portarlo a termine avrebbe forse consentito di dimostrare un beneficio pi significativo , ma avrebbe anche comportato il rischio di evidenziare sempre pi un bias di sovradiagnosi che , con molta probabilit , ne inquina i risultati . 
in effetti , noto dalla letteratura che la chiusura prematura di un rct pu notevolmente sovrastimarne lutilit ( too good to be true ) e vari autori suggeriscono che i risultati di un rct interrotto precocemente dovrebbero essere considerati con scetticismo [ 4446 ]  . 
 esso ha evidenziato una riduzione statisticamente significativa della mortalit da tutte le cause pari al 6 , 7% nel braccio attivo rispetto ai controlli , di cui per solo dovuto al 58 radiol med ( 2013 ) 118 : 5161 longer significant , but it is still embarrassing and difficult to expla could a chest ct per year protect against stroke and heart attack while a simple cxr does not have this power ? we already know the so - called healthy volunteer effect , reported , for example , in the prostate , lung , colon , ovary ( plco ) trial [ 47 ]  . 
however , how can we explain the difference between the two arms of the nlst study ? as we previously mentioned , the nlst findings are probably affected by a strong element of overdiagnosis [ 48 ]  . 
in fact , in a trial with these characteristics , after 67 years of observation , the proportion of participants with tumour development should be the same in both arms . 
if a difference persists ( in the nlst trial , 119 surplus cancers in the intervention arm after nearly 7 years ) , this means that ct detects tumours that would not grow enough to be identified with the second test ( cxr ) ; thus , there is a bias of overdiagnosis ( pseudodisease )  . 
 the experience of mayo screening [ 6 ] has clearly demonstrated the a follow - up of at least 1015 years is required to fully explore this important aspect ; thus the early interruption of a trial for ethical reasons cannot be considered acceptable . 
 it should also be noted that the nlst trial , contrary to the smaller european trials , does not have a real control arm , because smokers not undergoing ct study were offered cxr , which as demonstrated by the extension of the mayo clinic trial of the 1970s has a paradoxical negative effect of increasing mortality [ 6 ]  . 
for example , recent conference communications [ 4951 ] of provisional results of the ongoing european trials indicate an absence of stage shift and a definite increase in all - cause and specific mortality rates among smokers enrolled in the active arm , which , though not statistically significant , is consistent with the results of marcus et al . 
 forse fare una tc toracica allanno protegge da infarto miocardico ed ictus cerebri mentre un semplice rx non ha questo potere ? conoscevamo gi il cosiddetto healthy volunteer effect , segnalato per esempio nel trial prostata , polmone , colon , ovaio ( plco ) [ 47 ]  . 
la spiegazione di questo ennesimo apparente paradosso semplice : le persone con malattie croniche e , generalmente , in cattive condizioni di salute non si arruolano come volontari in rct . 
ma come spiegare la differenza fra i due bracci dello studio nlst ? come abbiamo gi anticipato , lo studio nlst probabilmente gravato da un forte elemento di sovradiagnosi [ 48 ]  . 
infatti , dopo 67 anni di osservazione , in un trial con queste caratteristiche , la proporzione di soggetti in cui alla fine si sviluppa un tumore dovrebbe essere la stessa nei due bracci . 
se la differenza persiste ( nel trial nlst , 119 tumori in eccesso nel braccio attivo , dopo quasi 7 anni ) , ci sta ad indicare che la tc individua tumori che non sarebbero comunque destinati a crescere abbastanza da essere individuati con il secondo test ( lrx ) ed quindi presente sovradiagnosi ( pseudodisease )  . 
 lesperienza estesa dello screening con rx effettuato presso la mayo clinic [ 6 ] ha dimostrato con evidenza che necessario un follow - up di almeno 1015 anni per esplorare compiutamente questo importante aspetto , con buona pace per linterruzione precoce per motivi etici . facciamo ancora notare che lo studio nlst , a differenza dei trial europei , non ha un vero gruppo di controllo , in quanto , ai soggetti cui non era stato offerto lesame tc , veniva invece somministrato periodicamente lrx del torace che , come ha ben dimostrato lestensione del mayo trial degli anni 70 , ha un paradossale effetto dannoso , di incremento della mortalit [ 6 ]  . 
per esempio , recenti comunicazioni congressuali [ 4951 ] riguardanti i risultati provvisori dei trial europei ancora in corso , indicano assenza di stage shift , decisa sovradiagnosi e mortalit generica e specifica simili o addirittura pi elevate nel braccio attivo rispetto ai controlli , sia pure senza che venga raggiunta una significativit statistica ma in analogia con i gi citati risultati di marcus et al . 
and beyond even allowing that other rcts will provide more definite confirmation of the effectiveness of low - dose ct in reducing lung cancer mortality rates , there are many other issues that need to be clarified : 1 . 
can the number of false positives be reduced ? in particular , is it possible to reduce either the number of individuals who , following a positive low - dose screening ct study , undergo further investigation with tests exposing ..e oltre anche ammesso che altri rct confermino in maniera pi sicura lefficacia della tc a bassa dose nel ridurre la mortalit da tumore polmonare , esistono molte altre questioni che attendono una risposta : 1 . 
 possibile ridurre i falsi positivi ? in particolare ci si chiede se sia possibile ridurre vuoi il numero di soggetti che a seguito di una positivit al test di screening con radiol med ( 2013 ) 118 : 5161 them to ionising radiation ( in the italung study , the dose from these further investigations accounted for 23% of the total dose ) [ 52 ] or the number of patients undergoing surgery for benign disease on average , 18% but as high as 33% [ 3 ] 2 . 
could the american trial results be also applied to younger patients with a less heavy smoking history or belonging to other ethnic groups with different lung cancer epidemiology , such as the japanese population ? 3 . 
whereas validated guidelines for solid nodules are available and well known [ 53 ] , for nonsolid nodules , there are only interim and partly questionable guidelines [ 5456 ]  . 
beyond screening itself , how should we behave in the case of an incidental finding of an indeterminate , nonsolid , nodule detected in a ct study performed for other reasons in a smoker ? tc a bassa dose vanno incontro ad ulteriori accertamenti con indagini che espongono a radiazioni ionizzanti ( nello studio italung la dose legata a questi ulteriori accertamenti stata il 23% della dose totale ) [ 52 ] vuoi il numero di soggetti operati per neoplasia benigna sul totale degli operati , in media il 18% ma fino al 33% [ 3 ]  . 
i risultati del trial statunitense sono applicabili anche a soggetti pi giovani o con una storia di fumo meno importante oppure appartenenti ad altri gruppi etnici , con differente epidemiologia dei tumori polmonari , come i giapponesi ? 3 . 
chi esattamente dovrebbe essere studiato e per quanti anni ? lo screening dovrebbe essere protratto per tutta la vita ? necessario fare una tc allanno o pi di rado ? 4 . 
mentre per i noduli solidi esistono linee guida validate e ben conosciute [ 53 ] , per i noduli non solidi esistono solo linee guida provvisorie e abbastanza discutibili [ 5456 ]  . 
infine , al di l dello screening vero e proprio , come ci dovremmo comportare di fronte al singolo caso del fumatore in cui la tc , eseguita per altre ragioni , evidenzia un nodulo indeterminato e , soprattutto , non solido ? conclusions conclusioni ten years after our first analysis of this difficult and exciting topic , it is inevitable to repeat that , despite the dramatic increase in knowledge , we do not yet know enough , and the early interruption of the nlst trial did not help . 
it will not be easy to compare and integrate results of the nlst study with those of the plco ( cxr versus no screening for four solid tumours ) and of european trials , when they are concluded . 
more modestly , we believe that with the conclusion of the nlst study , we have probably reached the end of one phase of research to open a new phase , because of the many unresolved issues . 
in the meantime , if possible , we will attempt to resist the impending tsunami of requests for lowdose ct screening examinations , whether selfor physician referred , but in any case outside any protocol . 
this scenario , fuelled by the media and by radiological marketing , is unfortunately the most likely one and the most dangerous for the radiologist . dopo 10 anni dalla nostra prima riflessione sullo screening della neoplasia polmonare con tc , tema difficile e appassionante , inevitabile ripetere che , nonostante lenorme aumento delle conoscenze , non ne sappiamo ancora abbastanza . 
non sar facile paragonare ed integrare i risultati dello studio nlst con quelli dello studio plco ( rx versus no screening per quattro tumori solidi ) e dei trial europei , quando essi saranno conclusi . 
 intanto crediamo doveroso continuare ad arginare il possibile tsunami legato ad una enorme richiesta di esami di screening con tc a bassa dose su base volontaristica individuale oppure dietro richiesta medica , ma comunque al di fuori di qualunque protocollo . 
the mr imaging protocol included static t2 - weighted fast spin - echo ( fse ) images in the sagittal , axial and coronal planes ; dynamic midsagittal t2 - weighted single - shot ( ss ) - fse and fast imaging employing steady - state acquisition ( fiesta ) cine images during contraction , rest , straining and defecation . 
comparison between cd and mr with evacuation phase ( mrwep ) showed no significant differences in sphincter hypotonia , dyssynergia , rectocele or rectal prolapse and significant differences in descending perineucomparison between cd and mr without evacuation phase ( mrwoep ) showed no significant differences in sphincter hypotonia , dyssynergia or enterocele but significant differences in rectocele , rectal prolapse and descending perineucomparison between mrwep and mrwoep showed no significant differences in sphincter hypotonia , dyssynergia , enterocele or descending perineum but significant differences in rectocele , rectal prolapse , peritoneocele , cervical riassunto obiettivo . 
sono state acquisite sequenze statiche fast spin echo ( fse ) - t2 - pesate sui piani sagittale , assiale e coronale e sequenze dinamiche single shot fast spin echo ( ssfse ) e fast imaging employing steady - state acquisition ( fiesta ) sul piano sagittale mediano durante contrazione dello sfintere anale , riposo , ponzamento , defecazione . 
il confronto dt vs rm con fase di evacuazione ( rmce ) ha evidenziato differenze statisticamente non significative nellipotonia sfinteriale , dissinergia , rettocele , prolasso rettale , enterocele e differenze significative nel perineo discendente . 
il confronto dt vs rm senza fase di evacuazione ( rmse ) ha evidenziato differenze non significative nellipotonia sfinteriale , dissinergia , enterocele e differenze significative nel rettocele , prolasso rettale , perineo discendente . 
la fase di evacuazione fondamentale . parole chiave risonanza magnetica pavimento pelvico rm dinamica prolasso defecografia introduction introduzione outlet obstruction refers to all pelvic floor disorders causing incomplete evacuation of faecal content from the rectu outlet obstruction syndrome is a common clinical problem that heavily affects patients quality of life ( qol )  . 
its excellent contrast resolution for soft tissue means it is capable of depicting anatomical abnormalities affecting pelvic structures , whereas the high temporal resolution recently achieved with fast imaging techniques allows dynamic assessment of function . 
 however , there is no uniformity of mr imaging protocols in international studies published to date . diagnostic assessment of the pelvic floor is currently based on the examination and imaging modalities using ionising radiation , such as conventional defecography ( cd )  . 
mr imaging is increasingly used to study these disorders and seems to meet the requirements of a modality able to provide a multicompartment evaluation . the purposes of our study were to develop an mr protocol allowing morphological and functional study of the pelvic floor during the same imaging session ; to prospectively compare the capabilities of mr with those of cd , which is considered the reference standard , when studying outlet obstruction syndromes ; and to assess the impact of the evacuation phase of mr imaging on the final diagnosis . materials and methods study population our study was approved by the local ethics committee , and il termine defecazione ostruita comprende tutte le disfunzioni del pavimento pelvico responsabili di una incompleta evacuazione del contenuto fecale dal retto . 
la eccellente risoluzione di contrasto per i tessuti molli le conferisce la capacit di identificare le alterazioni anatomiche delle strutture pelviche , la elevata risoluzione temporale , risultato del recente sviluppo dellimaging veloce , consente di effettuare uno studio dinamico con finalit anche funzionali . 
fino ad oggi , tuttavia , nella letteratura mondiale non vi uniformit nel protocollo desame rm . la valutazione diagnostica del pavimento pelvico attualmente affidata allesame clinico e a metodiche di imaging che utilizzano radiazioni ionizzanti come la defecografia tradizionale ( dt )  . 
la rm , sempre pi utilizzata nello studio di tali patologie , sembra aver soddisfatto il requisito di metodica in grado di effettuare una valutazione multicompartimentale . gli obiettivi del nostro studio sono : sviluppare un protocollo rm che consenta di effettuare , nella stessa seduta , uno studio morfologico e funzionale del pavimento pelvico ; confrontare , in maniera prospettica , le capacit diagnostiche della rm con quelle della dt , considerata come standard di riferimento , nello studio della sindrome da defecazione ostruita ; valutare il contributo della fase di evacuazione dellesame rm sulla diagnosi finale . radiol med ( 2013 ) 118 : 2339 all patients provided informed consent . 
between july 2007 and january 2009 , 19 consecutive patients ( two men and 17 women ; mean age 54 years ; range 3677 years ) were included in the study . 
in all 19 patients ( 100% ) , the indication for mr examination was outlet obstruction syndrome associated with urinary and faecal incontinence in 3 / 19 patients ( 15% ) and with urinary difficulty in 1 / 19 patients ( 5% )  . 
of the 19 patients , nine ( 47% ) had a history of pelvic surgery , which included anal fissure , staple transanal rectal resection ( starr ) , rectopexy , endometriosis , reconstructive pelvic floor surgery , cystopexy , anterior rectocele and haemorrhoidectomy . 
all patients were studied with pelvic cd ( entero - defecography ) and mr imaging , with an interval between the two examinations not exceeding 1 month ( mean 124 days ; range 426 days )  . 
cd was performed before mr imaging in all cases . mr imaging protocol mr examinations were performed with a closed - configuration superconducting unit with a 1.5 - t field strength ( gesigna hdx 1.5 t , ge medical systems , milwaukee , wi , usa ) using an 8 - channel torso coil . materiali e metodi popolazione di studio lo studio stato approvato dal comitato etico ed ogni paziente ha firmato un consenso informato . 
da luglio 2007 a gennaio 2009 , 19 pazienti consecutivi ( 2 uomini e 17 donne ; et media 54 anni ; range di et 3677 anni ) sono stati inclusi nel nostro studio . 
in tutti i 19 pazienti ( 100% ) lindicazione dellesame rm era rappresentata da defecazione ostruita cui si associava in 3 / 19 pazienti ( 15% ) incontinenza urinaria e fecale ed in 1 / 19 paziente ( 5% ) difficolt minzionale . 
dei 19 pazienti 9 ( 47% ) avevano una storia di interventi chirurgici in sede pelvica che comprendevano : ragade anale , stapled trans anal rectal resection ( starr ) , rettopessi , endometriosi , plastica del pavimento pelvico con protesi , cistopessi , rettocele anteriore , emorroidectomia . 
delle 17 donne 5 erano nullipare , le altre 12 riferivano un numero di parti compreso fra 1 e 6 . tutti i pazienti sono stati sottoposti a dt ( entero - defecografia ) e ad rm della pelvi con un intervallo temporale fra i due esami non superiore ad 1 mese ( media 124 giorni , range 426 giorni )  . 
patients are invited to wear a large pad , a stratagem that has the dual purpose of preventing soiling of the mr bed and reducing psychological discomfort [ 3 ]  . 
inside the gantry , the rectum is distended with approximately 150 ml of ultrasound gel ( hyperintense on t2 and fiesta sequences ) introduced through a nelaton catheter ( 20 ch , 6.67 mm360 mm ) ( bicakcilar , istanbul , turkey ) and a 50ml catheter - tip syringe . 
inside the gantry , the patient lies supine ( feet first ) , with knees slightly flexed , as this position facilitates evacuation of rectal contrast agent during defecation . sequences our protocol includes the acquisition of : high - spatial - resolution static sequences to study the morphology of the levator ani ; dynamic sequences to study abnormalities of the pelvic organs during contraction , rest , straining and defecation . 
 static sequences included t2 - weighted fast spin - echo gli esami rm sono stati eseguiti con un magnete superconduttivo a geometria chiusa ( ge - signa hdx 1 , 5 t , ge medical systems , milwaukee , wi , usa ) con intensit di campo magnetico di 1 , 5 tesla , utilizzando una bobina 8 canali torso . preparazione la preparazione e la collaborazione del paziente sono fondamentali per la buona riuscita dellesame . 
 il paziente viene invitato ad indossare un pannolone ; questo accorgimento ha un duplice scopo : evitare la contaminazione del lettino della rm e ridurre il disagio psicologico [ 3 ]  . 
 allinterno del gantry si procede alla distensione del retto con circa 150 ml di gel ecografico [ iperintenso nelle sequenze t2 e fast imaging employing steady - state acquisition ( fiesta ) ] , introdotto mediante un catetere di nelaton ( 20 ch , 6 , 67 mm360 mm ) ( bicakcilar , istanbul , turchia ) ed una siringa da 50 ml con punta larga . 
allinterno del gantry il paziente viene posizionato in decubito supino 26 radiol med ( 2013 ) 118 : 2339 ( fse ) sequences in the sagittal , axial and coronal planes . 
 the technical parameters for this sequence were time to repetition ( tr ) / time to echo ( te ) , 4 , 675 / 100 ; flip angle , 90 ; section thickness , 4 mm ; interslice gap , 1 mm ; bandwidth , 41.67 khz ; field of view ( fov ) , 32 cm ; matrix , 320224 ; number of averages , 4 ; number of images , 26 ; acquisition time , 3 min 49 s . dynamic sequences were performed in the midsagittal plane identified on the t2 - weighted fse static images , with the pubic symphysis , urethra , vagina , rectum and coccyx included in the fov . 
overall examination time , including patient preparation , was approximately 40 min . image analysis cd was performed by a radiologist with 10 years experience and mr imaging by a radiologist with 6 years specific experience . 
 mr results were compared with those of cd , which was considered the reference standard . degree of prolapse and measurements dynamic sequences were assessed by analysing the position of the pelvic organs with respect to the landmarks during rest , contraction , straining and defecation . 
fixed landmarks are the ( feet first ) con le ginocchia lievemente flesse ; tale posizione serve ad agevolare levacuazione del mezzo di contrasto ( mdc ) endorettale durante la fase di defecazione . sequenze il nostro protocollo prevede lesecuzione di : sequenze statiche ad elevata risoluzione spaziale per valutare la morfologia del muscolo elevatore dellano ; sequenze dinamiche per valutare le modificazioni degli organi pelvici durante contrazione , rilassamento , ponzamento e defecazione . le sequenze statiche comprendevano sequenze t2 - pesate fast spin - echo ( fse ) eseguite sui piani sagittale , assiale e coronale . 
i parametri tecnici di questa sequenza sono i seguenti : tempo di ripetizione ( tr ) / tempo di eco ( te ) 4675 / 100 ; flip angle 90 ; section thickness 4 mm ; interslice gap 1 mm ; bandwidth 41 , 67 khz ; campo di vista ( fov ) 32 cm ; matrice 320224 ; numero medie 4 ; numero immagini 26 ; tempo di acquisizione 3 min e 49 s . sulle immagini statiche fse t2 - pesate stato individuato il piano sagittale mediano sul quale eseguire le sequenze dinamiche in modo da comprendere nel campo di vista la sinfisi pubica , luretra , la vagina , il retto ed il coccige . 
nella fase dinamica abbiamo utilizzato due tipi di sequenze : single - shot fast spin echo ( ssfse ) t2 - pesate e fiesta eseguite con le seguenti modalit : ssfse ( tr / te 708 / 90 ; flip angle 90 ; section thickness 8 mm ; bandwidth 83 , 3 khz ; fov 34 cm ; matrice 384224 ; numero medie 0 , 5 ; tempo di acquisizione di ciascuna immagine 0 , 3 s ) sul piano sagittale mediano eseguita con modalit sequenziale durante : contrazione , rilassamento , ponzamento ; fiesta ( tr / te 3 , 3 / 1 , 4 ; flip angle 45 ; section thickness 8 mm ; bandwidth 125 khz ; fov 35 cm ; matrice 224224 ; numero medie 1 ; numero immagini 20 ; tempo di acquisizione 20 s ) sul piano sagittale mediano eseguita con modalit multifase in acquisizione continua durante : contrazione , rilassamento , ponzamento e defecazione . quando lesame clinico suggeriva la presenza di un rettocele laterale o di un prolasso laterale le sequenze dinamiche sono state eseguite anche sui piani assiale e coronale . 
 la durata totale dellesame , compresa la preparazione del paziente , di circa 40 min . analisi delle immagini la dt stata eseguita da un radiologo con 10 anni di esperienza ; la rm stata eseguita da un radiologo con 6 anni di esperienza nel settore oggetto dello studio . 
la visualizzazione delradiol med ( 2013 ) 118 : 2339 pubococcygeal line ( pcl ) , extending from the lower border of the pubic symphysis to the last coccygeal joint . 
mobile landmarks are : bladder neck for the anterior compartment ; uterine cervix , or vaginal vault in the case of hysterectomy , for the middle compartment ; anterior rectal wall and anorectal junction for the posterior compartment ; pouch of douglas for the peritoneal compartment [ 4 , 5 ]  . on dynamic sequences , descent of one or more of the mobile landmarks below the pcl is considered pathological . 
prolapse is measured by drawing a line perpendicular to the pcl , passing through the mobile landmarks . the mr classification of pelvic prolapse derives from clinical classifications and is summarised in table 1 . 
the other pathological conditions assessed are listed below [ 1 , 610 ] : descending perineum : the anorectal junction , point of intersection between the lines drawn along the posterior profile of the rectum and the central axis of the anal canal , descends > 5 cm below the pcl during straining or defecation ; rectal prolapse : rectoanal invagination , which may be defined as internal or external ; internal rectal prolapse , also called intussusception , may be classified as internal intrarectal prolapse if the invagination is limited to the rectum or as internal intra - anal prolapse if the apex enters the anal canal and remains inside it during straining ; external rectal prolapse is invagination of the rectal wall through the anal canal , and the diagnosis is clinical . physiologically , the anorectal angle ( ara ) , formed by the two lines that identify the anorectal junction , ranges between 90 and 110 . 
i risultati della rm sono stati confrontati con quelli della dt , considerata come standard di riferimento . grado dei prolassi e misurazioni la valutazione delle sequenze dinamiche stata condotta sullanalisi della posizione degli organi pelvici rispetto a dei punti di repere a riposo , durante contrazione , ponzamento e defecazione . 
i punti di repere mobili sono rappresentati da : collo vescicale per il compartimento anteriore ; cervice uterina , o cupola vaginale in caso di isterectomia , per il compartimento intermedio ; parete rettale anteriore e giunzione ano - rettale per il compartimento posteriore ; cavo del douglas per il compartimento peritoneale [ 4 , nelle sequenze dinamiche la discesa di uno o pi punti di repere mobili al di sotto della linea pubo - coccigea considerata patologica . 
la misurazione dei prolassi si effettua tracciando una linea perpendicolare alla linea pubo - coccigea , passante per i punti di repere mobili . la classificazione rm dei prolassi pelvici deriva da quelle cliniche ed riassunta nella tabella 1 . 
le altre condizioni patologiche prese in esame sono elencate di seguito [ 1 , 610 ] : perineo discendente : la giunzione ano - rettale , punto di intersezione fra le linee tracciate lungo il profilo posteriore del retto e lungo lasse centrale del canale anale , discende di oltre 5 cm al di sotto della linea pubo - coccigea sotto ponzamento o durante la defecazione ; prolasso rettale : invaginazione della parete rettale . 
il prolasso rettale interno , chiamato anche intussuscezione , pu essere classificato come prolasso interno intra - rettale se linvaginazione confinata al retto , o come prolasso interno intra - anale se il suo apice penetra nel canale anale e rimane al suo interno sotto ponzamento . 
il prolasso rettale esterno uninvaginazione della parete rettale attraverso il canale anale e rappresenta una diagnosi clinica . in condizioni fisiologiche langolo ano - rettale ( ara , compreso fra le due linee che identificano la giunzione anorettale ) si mantiene fra 90 e 110 . 
 during straining and defecation , the ara widens on account of the reflex inhibition of the puborectal muscle , with a 1520 increase compared with the angle measured at rest [ 11 ]  . 
in the case of spastic pelvic floor syndrome ( anismus , pelvic floor dyssynergia ) , during evacuation , the ara tends to become more acute rather than obtuse , which indicates a failed release of the puborectal muscle [ 12 ]  . statistical analysis data from static sequences used for morphological assessment of the levator ani muscle were analysed first . 
 to assess the impact of the evacuation phase on the final diagnosis , we initially considered all phases ( contraction , rest , straining on ssfse ; and contraction , rest , straining and evacuation on fiesta ) , which were indicated as mr with evacuation phase ( mrwep )  . 
later , the evacuation phase was excluded from the analysis ( contraction , rest and straining phases on ssfse and fiesta sequences ) , indicated as mr without evacuation phase ( mrwoep )  . 
the comparison took into account the following clinicalpathological conditions : sphincter hypotonia , pelvic floor dyssynergia , rectocele , rectal prolapse ( including intussusception ) , enterocele and descending perineufor each patient , the presence and extent of the disorder were assessed . diagnostic capabilities of mr with and without evacuation phase compared with the reference standard were assessed by measuring accuracy , sensitivity , specificity and positive ( ppv ) and negative ( npv ) predictive values . 
statistical differences among the three methods were assessed using one - way analysis of variance ( anova ) , followed by post hoc tests ( duncans test ) as needed . 
in view of the frequent involvement of multiple compartments in pelvic floor disorders , for each patient , we assessed the number and type of compartments involved on the basis of findings of mrwep and mrwoep . results in all 19 patients , pelvic mr imaging was completed sucni pelvici rispetto alla linea pubo - coccigea e la riduzione dellara di 1520 ( dovuta alla contrazione del muscolo pubo - rettale )  . 
nella sindrome da spasticit del pavimento pelvico ( anismus , dissinergia del pavimento pelvico ) durante levacuazione lara tende a diventare pi acuto anzich ottuso , espressione del mancato rilasciamento del muscolo puborettale [ 12 ]  . analisi statistica una prima analisi dei dati ha riguardato le sequenze statiche sulle quali stata effettuata una valutazione morfologica del muscolo elevatore dellano . 
al fine di valutare la rilevanza della fase di evacuazione sulla diagnosi finale , sono state inizialmente prese in esame tutte le fasi eseguite ( contrazione , riposo , ponzamento per le ssfse e contrazione , riposo , ponzamento ed evacuazione per le fiesta ) indicandole con il termine : rm con fase di evacuazione ; successivamente la fase di evacuazione stata esclusa dalla valutazione ( fasi di contrazione , riposo e ponzamento per le ssfse e per le fiesta ) : rm senza fase di evacuazione . 
il confronto tra le metodiche ha riguardato le seguenti condizioni clinico - patologiche : ipotonia sfinteriale , dissinergia del pavimento pelvico , rettocele , prolasso rettale ( comprendente anche lintussuscezione ) , enterocele , perineo discendente . 
 per ogni paziente stata valutata la presenza della patologia ed il suo grado . le capacit diagnostiche della rm con e senza fase di evacuazione nei confronti dello standard di riferimento sono state valutate calcolando accuratezza , sensibilit , specificit , valore predittivo positivo e negativo . 
la presenza di eventuali differenze statistiche tra le tre metodiche prese in esame stata analizzata attraverso lutilizzo dellanalisi della varianza ( anova ) a una via seguita da confronti post - hoc ( test di duncan ) quando necessari . 
per le altre condizioni clinico - patologiche rilevabili solo con esame rm : peritoneocele , cervicocistoptosi ed isteroptosi stato effettuato un confronto tra rm con fase di evacuazione ed rm senza fase di evacuazione . 
 no claustrophobic reaction was reported by any of the patients . mento multicompartimentale delle alterazioni del pavimento pelvico , per ogni paziente stato valutato il numero e il tipo di compartimenti interessati sulla base dei reperti rm sia con fase di evacuazione che senza fase di evacuazione . static sequences : morphological findings static sequences were used to assess the morphology of the levator ani muscle . 
nessuna reazione claustrofobica stata riscontrata nei pazienti sottoposti ad esame rm . sequenze statiche : reperti morfologici dynamic sequences : comparison between conventional and mr defecography cd revealed four cases of sphincter hypotonia , all of which were identified on mr both with and without the evacuation phase . 
la dt ha evidenziato 2 enteroceli : 1 di i grado ed 1 di ii grado , entrambi sono stati evidenziati dalla rm con fase di evacuazione che ha stadiato correttamente lenterocele di i grado e ha sottostadiato lenterocele di ii grado della dt come i grado . 
lanalisi statistica dei dati appena esposti ha portato ai risultati riassunti nelle tabelle 2 e 3 . per i casi di peritoneocele e per lo studio dei compartimenti anteriore e medio , non valutabili con la entero - defecografia , i dati riguardano solo lesame rm . 
la rm con fase di evacuazione ha evidenziato 3 casi di peritoneocele , 2 di i grado ed 1 di ii grado , nessuno dei quali stato identificato nella rm senza fase di evacuazione . 
la valutazione mediante rm con fase di evacuazione ed rm senza fase di evacuazione del numero e del tipo di compartimenti interessati da alterazioni per numero di pazienti ha portato ai risultati esposti nella tabella 5 . nella patologia del pavimento pelvico lesame clinico accompagnato da unaccurata anamnesi rappresenta tuttoggi lelemento fondamentale della diagnosi [ 1 ] ; a questo si associano diversi test fisiologici e metodiche di imaging come la defecografia tradizionale e la rm . 
da notare la concomitante presenza di un cistocele ( testa di freccia )  . of the statistical analysis of these data are summarised in tables 2 and 3 . the cases of peritoneocele and the study of the anterior and middle compartments could not be assessed on enterodefecography , so data regard mr imaging only . 
mrwep identified three cases of peritoneocele : two grade i and one radiol med ( 2013 ) 118 : 2339 radiol med ( 2013 ) 118 : 2339 table 3 statistical analysis . 
analysis of the number and type of compartments showing abnormalities on mrwep and mrwoep and the number of patients affected is reported in table 5 . discussion in pelvic floor disorders , clinical examination coupled with careful patient history remains the mainstay of the diagnosis [ 1 ] ; these are combined with physiological tests and imaging techniques , such as conventional defecography and mr imaging . 
tali sequenze sono dotate di uneccellente risoluzione di contrasto : la parete degli organi cavi ( vescica , retto ) ipointensa e contrasta nettamente con i fluidi contenuti allinterno dei visceri e con il tessuto adiposo periviscerale , entrambi iperintensi ; ci consente unottimale distinzione dei compartimenti pelvici sul piano sagittale . 
le sequenze ssfse presentano tempi di acquisizione rapidi ( 0 , 52 , 5 secondi per immagine ) , ma il loro utilizzo richiede un intervallo di circa 12 secondi fra unacquisizione e laltra per consentire il recupero t1 ed evitare la saturazione dei fluidi ; ci ne limita la risoluzione temporale e rende impossibile effettuare un imaging in real - time . 
le sequenze fiesta sono caratterizzate da una pesatura ibrida t2 / t1 e presentano un contrasto t2 lievemente inferiore alle ssfse a causa della parziale pesatura t1 ; i tempi di acquisizione sono pi rapidi ( minori di 1 s ) e , a differenza delle ssfse , non necessitano di una pausa fra le acquisizioni per il recupero t1 . 
per tale motivo abbiamo utilizzato una sequenza fiesta ( 1 immagine / s ) nella fase di evacuazione in modo da consentire al paziente di raggiungere il massimo grado di sforzo durante il ponzamento . 
la cervice uterina ( freccia ) discende al di sotto della linea pubo - coccigea ( linea )  . quences provide excellent contrast resolution : the wall of the hollow organs ( bladder , rectum ) appears hypointense , contrasting markedly with the hyperintensity of the fluid in the bowel and with the perivisceral fat ; this allows excellent depiction of pelvic compartments in the sagittal plane . 
 ssfse sequences have fast acquisition times ( 0.52.5 s per image ) , but their use requires 1to 2 - s intervals between acquisitions to permit t1 recovery and prevent fluid saturation ; this reduces the temporal resolution and precludes real - time imaging . 
fiesta sequences are characterised by hybrid t2 - t1 weighting and have a slightly lower t2 contrast compared with ssfse as a result of partial t1 weighting ; acquisition times are faster ( shorter than 1 s ) and , unlike ssfse , do not require any interval between acquisitions for t1 recovery . 
we therefore used a fiesta sequence ( one image ) during the evacuation phase to allow the patient to achieve the maximal degree of effort during straining . the choice of sequences and intracavitary contrast material are closely connected . 
the use of water - sensitive sequences led us to use a water - like contrast agent ( ultrasound gel ) , which has a signal intensity equivalent to that of fluid ; this allowed us to opacify the rectum only , taking advantage of the natural contrast provided by urine . in our protocol , the dynamic phase was preceded by a static phase . 
this phase was obtained with a t2 - weighted fse sequence in the three spatial planes , in which high spatial resolution provided accurate morphological assessment of the levator ani . 
comparison [ one - way analysis of variance ( anova ) ] of magnetic resonance ( mr ) imaging with and without evacuation phase in the diagnostic evaluation of the different clinical and pathological conditions condition mrwep vs . 
confronto statistico [ analisi della varianza ( anova ) a una via ] dei risultati della risonanza magnetica con fase di evacuazione ( rmce ) e della risonanza magnetica senza fase di evacuazione ( rmse ) nella valutazione diagnostica di diverse condizioni clinico - patologiche patologia rmce vs . 
rmse peritoneocele cervicocistoptosi isteroptosi p = 0 , 074 p = 0 , 006 p = 0 , 016 la scelta delle sequenze e del mezzo di contrasto endocavitario sono strettamente legate . 
lutilizzo di sequenze water sensitive ci ha indotto ad utilizzare un mezzo di contrasto water like ( gel ecografico ) con intensit di segnale uguale a quella dei fluidi ; questo ci ha consentito di opacizzare soltanto il retto , sfruttando peraltro il contrasto naturale dellurina . nel nostro protocollo la fase dinamica preceduta da una fase statica . 
per tale fase abbiamo utilizzato una sequenza fse t2 - pesata eseguita sui tre piani dello spazio , la cui elevata risoluzione spaziale ha consentito unaccurata valutazione morfologica del muscolo elevatore dellano . 
 [ 16 ] reported that mr imaging was superior to dynamic fluoroscopy and suggested its use as an alternative , as it was able to provide simultaneous depiction of all pelvic compartments in a noninvasive manner . 
lassociazione delle fasi statica e dinamica ci ha permesso di identificare la presenza di alterazioni morfologiche e funzionali che spesso concorrono nella patogenesi delle disfunzioni del pavimento pelvico [ 3 ] e della sindrome da defecazione ostruita . i primi studi sul pavimento pelvico con rm risalgono al 1991 [ 10 , 14 ]  . 
 [ 16 ] hanno riscontrato una superiorit della rm nei confronti della fluoroscopia dinamica e hanno proposto la rm come alternativa alla fluoroscopia per la sua capacit di visualizzare simultaneamente tutti i compartimenti pelvici in maniera non invasiva . 
 [ 17 ] , la rm risultata meno accurata della cistocolpodefecografia presentando un alto numero di falsi negativi , probabilmente in relazione al decubito supino ed alla mancata esecuzione della fase di evacuazione . 
 [ 19 ] hanno confrontato lefficacia diagnostica della defecografia - rm con la entero - colpo - cisto - defecografia ( eccd ) nella valutazione delle ernie del pavimento pelvico riscontrando una maggiore sensibilit della eccd nellevidenziare il contenuto delle ernie , probabilmente in relazione al decubito supino dei pazienti nel magnete . non tutti i protocolli esistenti in letteratura , prevedono lesecuzione di sequenze statiche sui tre piani dello spazio . 
 nel nostro studio abbiamo confrontato le capacit diagnostiche della rm con quelle della dt nella sindrome da defecazione ostruita adottando un protocollo rm che consentisse un accurato studio morfologico con sequenze statiche ed uno studio funzionale con sequenze dinamiche . 
dal momento che non tutti gli autori eseguono la fase di evacuazione abbiamo cercato di valutare il contributo della fase evacuativa dellesame rm sulla diagnosi finale . in alcune condizioni clinico - patologiche di carattere prevalentemente funzionale come lipotonia sfinteriale e la dissinergia del pavimento pelvico non abbiamo riscontrato differenze fra le metodiche ; la dt e la rm con e senza fase 36 radiol med ( 2013 ) 118 : 2339 conducted on 1 , 142 patients , cappabianca et al . 
 [ 19 ] compared the diagnostic effectiveness of mr defecography with that of entero - colpo - cysto - defecography ( eccd ) to assess pelvic floor hernias and found that eccd had higher sensitivity in depicting the content of hernias , probably as a result of the supine position of patients inside the magnet . not all published protocols require the acquisition of static sequences in the three spatial planes . 
in our study , we compared the diagnostic capabilities of mr and cd in outlet obstruction syndrome by following an mr protocol that includes an accurate morphological study based on static sequences and a functional study based on dynamic sequences . 
in consideration of the fact that not all authors include the evacuation phase , we attempted to verify the contribution of this mr imaging phase on the final diagnosis . in several , especially functional , pathological conditions , such as sphincter hypotonia and pelvic floor dyssynergia , we found no significant differences between the two techniques ; cd and mrwep and mrwoep detected the same number of cases . 
in pelvic floor dyssynergia , persistent contraction of the puborectalis is easily identified during the straining phase , even though it becomes stronger during the subsequent evacuation phase . in anterior rectocele studies , mrwep identified the same number of cases as cd , even though some were understaged . 
therefore , in descending perineum studies , in addition to the evacuation phase , other fundamental factors may be patient position or contrast medium composition , which allow a greater degree of straining on cd . 
in multicompartment assessment of findings observed in our series , the posterior compartment proved to be the most frequently involved , which correlates with the clinical findings of patients referred for outlet obstruction . 
nella dissinergia la persistente contrazione del muscolo puborettale facilmente identificabile gi nella fase di ponzamento , sebbene si accentui nella successiva fase di evacuazione . nello studio del rettocele anteriore la rm con fase di evacuazione ha identificato lo stesso numero di casi della dt , sebbene ne abbia sottostadiati alcuni . 
nello studio dei prolassi rettali i risultati della dt e della rm con fase di evacuazione sono pressoch sovrapponibili , mentre decisamente inferiore risulta la capacit diagnostica della rm senza fase di evacuazione con 1 solo caso identificato . 
nello studio di tale condizione risulta pertanto determinate , oltre alla fase di evacuazione , probabilmente anche il decubito del paziente o la composizione del mezzo di contrasto che nellesame tradizionale consentono di raggiungere un maggior grado di ponzamento . 
nello studio dei compartimenti anteriore e medio e del peritoneocele , dove la valutazione ha riguardato solo la rm , lesame condotto con fase di evacuazione si dimostrato decisamente superiore a quello senza fase di evacuazione . 
questultimo non ha identificato nessun caso di peritoneocele e di isteroptosi ed ha evidenziato soltanto il 27% ( 3 / 11 ) dei casi di cervicocistoptosi evidenziati dalla rm con fase di evacuazione . 
nella valutazione multicompartimentale dei reperti osservati nella nostra casistica , il compartimento maggiormente coinvolto stato quello posteriore e ci correla con il dato clinico dei pazienti giunti alla nostra osservazione per defecazione ostruita . 
anche sotto questo aspetto la rm con fase di evacuazione si dimostrata superiore alla rm senza fase di evacuazione : la prima ha evidenziato un coinvolgimento di pi compartimenti nel 63% ( 12 / 19 ) dei pazienti , la seconda solo nel 5% ( 1 / 19 )  . 
complessivamente la rm con fase di evacuazione e la dt si sono dimostrate sostanzialmente equivalenti nellaipotonia sfinteriale , dissinergia , rettocele , prolasso rettale ed enterocele mentre la dt radiol med ( 2013 ) 118 : 2339 perior to mrwoep : the former identified involvement of several compartments in 63% ( 12 / 19 ) and the latter only in 5% of patients ( 1 / 19 )  . 
overall , mrwep and cd proved to be equivalent in detecting sphincter hypotonia , dyssynergia , rectocele , rectal prolapse and enterocele , whereas cd was superior in detecting descending perineu mrwoep , except in the case of sphincter hypotonia and dyssynergia , performed substantially worse that the two other methods in the study of all compartments . 
cd plays a key role in studying patients with pelvic floor dysfunction , even though it has several limitations : complexity of the examination and procedural invasiveness , projective imaging , failure to depict soft tissues , limited ability to detect abnormalities in the anterior and middle compartments [ 20 , 21 ] , exposure to ionising radiation ( mean effective radiation dose > 4.9 msv ) [ 22 , 23 ]  . mr imaging has several advantages : noninvasiveness , cross - sectional and multiplanar imaging , possibility of performing a multicompartmental study , excellent contrast resolution for soft tissues , direct depiction of muscular structures ( levator ani ) , good temporal resolution with possibility of performing a dynamic study and absence of ionising radiation . 
consistent with previous authors [ 19 , 24 ] , we found the evacuation phase to be fundamental , as it ensures high intra - abdominal pressure with complete dynamic assessment of pelvic floor disorders ; conclusive findings might be missed or underestimated if the evacuation phase is omitted [ 17 ]  . our study has several some limitations . 
 [ 24 ] studied the capabilities of an open - configuration , low - field , titling mr system for assessing pelvic floor disorders , with patients in the supine and orthostatic positions . 
la rm senza fase di evacuazione , fatta eccezione per lipotonia sfinteriale e la dissinergia , si dimostrata decisamente inferiore alle altre due metodiche nello studio di tutti i compartimenti . 
la dt gioca un ruolo importante nella valutazione dei pazienti con disfunzione del pavimento pelvico , ma gravata da alcuni limiti : complessit dellesame ed invasivit della preparazione , imaging proiettivo , mancata visualizzazione dei tessuti molli , ridotta capacit nellidentificare le anomalie dei compartimenti anteriore e medio [ 20 , 21 ] , esposizione alle radiazioni ionizzanti ( dose di radiazione effettiva media di oltre 4 , 9 msv ) [ 22 , 23 ]  . nonostante i limiti evidenziati dal nostro studio , la rm presenta numerosi vantaggi : non invasivit , imaging tomografico e multiplanare , possibilit di effettuare uno studio multicompartimentale , eccellente risoluzione di contrasto nello studio dei tessuti molli , visualizzazione diretta delle strutture muscolari ( elevatore dellano ) , buona risoluzione temporale con possibilit di eseguire uno studio dinamico , assenza di radiazioni ionizzanti . 
come sostenuto da altri autori [ 19 , 24 ] , anche nel nostro studio risultata di importanza fondamentale la fase di evacuazione che assicurando unelevata pressione intra - addominale , consente una completa valutazione dinamica delle patologie del pavimento pelvico ; reperti decisivi possono essere persi o sottostimati se viene omessa la fase di defecazione [ 17 ]  . il nostro studio ha alcuni limiti . 
 [ 24 ] hanno valutato le capacit di un sistema rm aperto a basso campo a decubito variabile nellesaminare i disordini del pavimento pelvico con paziente in posizione supina e in ortostatismo . 
as a result , comparison between cd and mr imaging involved disorders affecting the posterior compartment only , to the exclusion of those of the anterior and middle compartments . guardato solo le patologie del compartimento posteriore e non stato possibile paragonare le due metodiche nei compartimenti anteriore e medio . conclusions mr imaging allows both a morphological and a functional assessment of outlet obstruction syndrome . 
mr imaging is noninvasive and easy to perforin our opinion , it should supplement cd to provide a global , noninvasive assessment of pelvic anatomy and the interaction of pelvic organs , especially in patients with multicompartment disorder , with a view to selecting the most appropriate treatment [ 19 ] and reduce the rate of postoperative recurrence . 
 mr examination should always incorporate all static and dynamic phases in the protocol ; the diagnostic effectiveness of the modality is , above all , related to the evacuation phase , which is essential for visualising all pathological conditions and must always be included in the study protocol . conclusioni attualmente la rm consente di effettuare un inquadramento diagnostico sia di tipo morfologico che funzionale della sindrome da defecazione ostruita . 
a nostro giudizio , il suo ruolo , ad integrazione della dt , pu essere quello di una migliore valutazione globale non invasiva dellanatomia pelvica e dellinterazione degli organi pelvici , soprattutto in pazienti con patologia multicompartimentale , al fine di scegliere la strategia terapeutica pi corretta [ 19 ] e ridurre le recidive post - chirurgiche . 
salvatore di coppito , 67100 laquila , italy 2cattedra di ortopedia , universit di laquila , laquila , italy 3chirurgia della spalla , istituto humanitas , milano , italy correspondence to : a . 
this study aimed to evaluate the diagnostic possibilities of mr arthrography in the correct identification of complex tears of the biceps pulley and their possible correlation with anterosuperior impingement ( asi ) development . 
mr arthrography images showed a spectrum of tears that , according to the habermeyer classification , were subdivided into four groups : type 1 in three patients ; type 2 in five ; type 3 in seven ; type 4 in eight . 
 allesame artro - rm sono state riscontrate 3 lesioni di tipo 1 , 5 lesioni di tipo 2 , 7 lesioni di tipo 3 e 8 lesioni di tipo 4 . 
lartro - rm risultata essere una metodica estremamente valida per la diagnosi delle lesioni dellintervallo dei rotatori ; sulla base della nostra esperienza , soltanto le lesioni complesse della puleggia bicipitale , sono correlate allo sviluppo di ias . radiol med ( 2013 ) 118 : 112122 keywords mri arthro - mri shoulder internal impingement anterosuperior impingement shoulder parole chiave risonanza magnetica artro - rm impingement interno di spalla impingement anterosuperiore spalla introduction introduzione anterosuperior impingement ( asi ) of the shoulder is described as a form of internal conflict [ 13 ] among the tendinous components of the anterior part of the rotator cuff and the humeral head , and the superoanterior labrum and the glenoid cilium [ 4 ]  . 
first described by gerber and sebesta [ 5 ] , asi is responsible for chronic anterior pain , which is exacerbated by the so - called follow - through movements , common in some sports activities such as tennis and baseball [ 4 ]  . 
although contact between the mentioned anatomical structures is physiological , in the athlete , the repetition of flexion and internal rotation movements of the arm can cause an anatomical lesion at the site of impingement , leading to clinical dysfunction and reduced sporting performance . 
although asi may involve many structures simultaneously [ 47 ] , the most frequently involved is the space within the rotator interval called the biceps pulley [ 811 ]  . 
several scientific studies have demonstrated the diagnostic usefulness of ultrasound ( us ) , magnetic resonance ( mr ) imaging and , in particular , mr arthrography for evaluating disorders affecting this complex anatomical area [ 10 , 12 , 13 ]  . the purpose of our study was to evaluate the diagnostic possibilities of mr arthrography for correctly identifying complex tears of the biceps pulley and their possible correlation with asi development . 
 materials and methods after providing informed consent , 23 patients ( 20 men and three women ; age range , 1835 ) who underwent mr arthrography of the shoulder between february 2008 and february 2011 were recruited in this retrospective study . 
 of these , 12 were professional athletes ( 2 baseball and 7 tennis players , 2 track and field athletes , 1 swimmer ) , and 11 were amateurs ( 9 tennis players , 2 swimmers )  . 
all patients with a clinical suspicion of defect in the intra - articular complex of stabilisation of the long head of the biceps tendon ( lhbt ) underwent mr arthrography . 
the shoulders were studied with a dedicated limpingement antero - superiore ( ias ) di spalla una forma di conflitto interno [ 13 ] che si instaura fra le componenti tendinee della porzione anteriore della cuffia dei rotatori , la testa omerale , il labbro sopraequatoriale anteriore ed il ciglio glenoideo [ 4 ]  . 
lias , descritto per la prima volta da gerber e sebesta [ 5 ] , d vita ad un vero e proprio quadro sindromico caratterizzato da una sintomatologia dolorosa cronica anteriore esacerbata dai cosiddetti movimenti di follow - through , tipici di alcuni sport tra cui il tennis ed il baseball [ 4 ]  . 
sebbene il contatto tra le strutture anatomiche sopramenzionate sia fisiologico , nello sportivo , lesecuzione reiterata dei movimenti di flessione ed intrarotazione del braccio pu determinare un danno anatomico nel sito di impingement ed una conseguente sindrome clinico - disfunzionale con riduzione della performance sportiva . 
sebbene le lesioni osservate in caso di ias possano coinvolgere simultaneamente varie strutture [ 47 ] , il reperto patologico pi frequente costituito da un danno di unarea precisa dellintervallo dei rotatori definita puleggia bicipitale [ 811 ]  . 
numerosi studi scientifici hanno dimostrato la valenza diagnostica dellecografia e soprattutto della risonanza magnetica ( rm ) e dellartro - rm nella valutazione delle patologie di questa complessa area anatomica [ 10 , 12 , 13 ]  . lo scopo del nostro lavoro stato quello di valutare le potenzialit diagnostiche dellartro - rm nella corretta identificazione di lesioni complesse della puleggia bicipitale e la loro eventuale correlazione con lo sviluppo di ias . materiali e metodi previo consenso informato , sono stati inclusi nello studio retrospettivo 23 pazienti dediti ad attivit sportiva , di et compresa tra 18 e 35 anni ( 20 maschi e 3 femmine ) che nel periodo compreso tra febbraio 2008 e febbraio 2011 sono stati sottoposti ad esame artro - rm di spalla ; di questi 12 praticavano attivit sportiva di tipo professionistico ( 2 baseball , 7 tennis , 2 atletica , 1 nuoto ) ed 11 praticavano attivit sportiva dilettantistica ( 9 tennis , 2 nuoto )  . 
tutti i pazienti sono stati sottoposti ad esame artro - rm con sospetto clinico di patologia del sistema di 114 radiol med ( 2013 ) 118 : 112122 surface coil , with the arm in neutral position and in internal and external rotation . acquisitions in internal and external rotation , aimed at evaluating the lhbt , were obtained in the axial planes . 
patients underwent mr arthrography after intra - articular injection of 1318 cc of 0.0025 m gadoliniuthe protocol was based on proton - density ( pd ) - weighted sequences , with or without fat suppression [ time to echo ( te ) , 13.5 ms ; time to repetition ( tr ) , 1 , 800 ms ] and t1 - weighted ( te = 25 ms ; tr = 350 ms ) spin - echo ( se ) sequences obtained in the three planes ( axial , oblique sagittal and oblique coronal )  . 
the axial plane was obtained with acquisitions orientated perpendicularly to the glenohumeral joint ; the oblique sagittal plane was obtained parallel to the contour of the humeral glena and the oblique coronal plane was obtained parallel to the scapular spine . 
problematic cases ( n = 3 ) were discussed . from 7 to 45 days after mr arthrography examinations , all patients underwent arthroscopic surgery , during which the surgeon evaluated the possible presence of a conflict between the subscapularis tendon and the humeral greater tubercle against the superoanterior glenoid labrum during flexion , horizontal abduction and internal rotation movements . 
il protocollo artro - rm prevedeva lutilizzo di sequenze pesate in densit protonica ( dp ) senza e con soppressione del segnale del tessuto adiposo [ tempo di eco ( te ) = 13 , 5 ms ; tempo di ripetizione ( tr ) = 1800 ms ] e sequenze spinecho ( se ) t1 - pesate ( te = 20 ms ; tr = 400 ms ) , eseguite sui tre piani di scansione ( assiale , sagittale obliquo e coronale obliquo )  . 
il piano assiale stato ottenuto con pacchetto di acquisizione orientato perpendicolarmente allarticolazione gleno - omerale , il piano sagittale obliquo stato ottenuto con pacchetto di acquisizione orientato parallelamente al profilo della glena omerale ed il piano coronale obliquo stato ottenuto con pacchetto di acquisizione orientato parallelamente alla spina scapolare . 
i casi dubbi ( in numero di 3 ) sono stati quindi rivalutati congiuntamente per ottenere un consenso . tutti i pazienti in un periodo compreso tra i 7 ed i 45 giorni successivi allesame artro - rm sono stati sottoposti ad intervento chirurgico per via artroscopica . 
in tale sede stata valutata leventuale presenza di un conflitto tra il sottoscapolare ed il trochine omerale contro il ciglio glenoideo sopraequatoriale anteriore nei movimenti di flessione , adduzione orizzontale ed intrarotazione . 
 risultati nella valutazione diagnostica artro - rm si ottenuta una elevata concordanza interoperatore [ kappa pesato = 0 , 883 ; 95% intervallo di confidenza ( ci ) da 0 , 758 a 1000 ]  . 
schematic representation ( adapted from [ 7 ] ) ( a ) ; mr arthrography , oblique sagittal se t1 - weighted image ( b ) ; mr arthrography axial se t1 - weighted image ( c )  . 
a schema ( adattato da [ 7 ] ) ; b immagine artro - rm sagittale obliqua se t1pesata ; c immagine artro - rm assiale se t1 - pesata . 
 at arthroscopic evaluation , one patient had type 1 lesion , five type 2 , five type 3 and ten type 4 ; absence of tendon ligament defects was observed in two patients . 
non sono stati osservati aspetti riferibili a lesione del legamento coraco - omerale ( lco ) e della cuffia posteriore n condizioni di normalit anatomica . alla valutazione artroscopica 1 paziente presentava lesione di tipo 1 , 5 pazienti presentavano lesione di tipo 2 , 5 pazienti lesione di tipo 3 e 10 pazienti lesione di tipo 4 ; 2 pazienti non mostravano alterazioni tendo - legamentose di rilievo . 
alle manovre dinamiche eseguite durante lartroscopia , segni di ias sono stati riscontrati in 3 pazienti con lesione di tipo 3 ed in 10 pazienti con lesione di tipo 4 . 
2a - d type 1 lesion ( adapted from [ 7 ] ) ( a ) ; mr arthrography oblique sagittal ( b ) and axial ( c ) pd - weighted images show an inhomogeneous and unstretched superior glenohumeral ligament ( sghl ) ( arrows )  . 
limmagine artroscopica ( d ) conferma la lesione isolata del lgos ( * ) che appare iperemico e sfrangiato . patients with type 4 lesion and in 4 / 5 patients with type 3 lesion . 
these results are summarised in table 2 . discussione discussion asi is a recently described and identified nonoutlet impingement [ 13 ] and a possible cause of a chronic anterior shoulder pain [ 1 , 46 ]  . 
the conflicting anatomical structures are many , including the humeral labrum and humeral greater tubercle , but there is constant involvement of the external components of the rotator interval , which form the biceps pulley . 
the rotator interval is an anatomical space traversed by the lhbt from its origin in the humeral groove up to its insertion on the superior tubercle of the scapula [ 8 , lias una forma di non - outlet impingement [ 13 ] di relativamente recente descrizione ed identificazione , possibile causa di una sintomatologia dolorosa anteriore cronica di spalla [ 1 , 46 ]  . 
le strutture anatomiche che entrano in conflitto possono essere diverse , ivi comprese labbro e trochine omerale , ma con un interessamento pressoch costante delle componenti esterne dellintervallo dei rotatori che costituiscono la puleggia bicipitale . 
lintervallo dei rotatori uno spazio anatomico attraversato dal clb dalla sua emergenza a livello della doccia omerale fino alla sua inserzione sul tubercolo sovraglenoideo della scapola [ 8 , 1014 ]  . 
pertanto il clb , nel suo tratto orizzontale , attraversa un tunnel le cui pareti sono costituite dal tendine sottoscapolare anteriormente e dal tendine sopraspinoso posteriormente mentre il suo pavimento ed il suo tetto sono costituiti rispettivamente dal lgos e dal lco [ 8 , 1517 ]  . 
mr arthrography oblique sagittal pd - weighted image ( b ) shows an inhomogeneous superior glenohumeral ligament ( sghl ) ( white arrow ) and a tear of the anterior articular side of the supraspinatus tendon ( black arrow )  . 
mr arthrography fat - suppressed pdweighted image in aber ( c ) well depicts supraspinatus tendon tear with penetration of contrast agent within tendinous fibres ( white arrow )  . 
in its horizontal course , the lhbt runs through a tunnel - shaped space , the walls of which are constituted by the subscapularis tendon anteriorly and by the supraspinatus tendon posteriorly ; its floor and roof are constituted by the sghl and chl , respectively [ 8 , 1517 ]  . at the entrance into the bicipital groove , the sghl , chl and upper insertions of the subscapularis blend to form a tendonligamentous complex with annular morphology called anterior pulley of reflection or biceps pulley a contained system of fundamental physiological , biomechanical and pathological importance [ 911 , 1630 ]  . 
 minimum conflict among the different anterosuperior anatomical structures of the shoulder is physiological [ 4 , 6 ] , but the repetition of particular movements leads to the development of pathology at the conflict site . 
in allingresso della doccia bicipitale , il lgos e il lco e le inserzioni alte del sottoscapolare si uniscono formando un complesso tendo - legamentoso a morfologia anulare chiamato puleggia anteriore di riflessione o puleggia bicipitale [ 911 , 1630 ]  . 
 si ritiene che un minimo conflitto tra le varie strutture anatomiche antero - superiori della spalla , sia in un certo qual modo fisiologico [ 4 , 6 ]  . 
 il reiterarsi di particolari movimenti che predispone allo sviluppo della patologia nella sede del conflitto , e per questo motivo che i conflitti interni della spalla ( antero - superiore e postero - superiore ) [ 17 ] si verificano spesso nello sportivo . 
nella nostra esperienza , in accordo ai dati gi presenti in letteratura [ 7 ] , abbiamo notato che lias si associa a lesioni pi o meno estese della puleggia bicipitale , con interessamento costante del lgos . 
 lartro - rm consente , con una minima invasivit , di esaminare in maniera completa lintervallo dei rotatori , la puleg118 radiol med ( 2013 ) 118 : 112122 fig . 
mr arthrography oblique sagittal pd - weighted image ( b ) shows a superior glenohumeral ligament ( sghl ) tear ( black arrow ) and a partial subscapularis tendon tear ( white arrow ) ; long head of the biceps tendon ( lhbt ) ( thin white arrow ) appears inhomogeneous and reduced in volume . 
mr arthrography axial pd - weighted fat - suppressed image ( c ) confirms an inhomogeneous sghl ( large white arrow ) and a partial tear of subscapularis tendon ( white arrow )  . 
lesame artroscopico ( d ) conferma la lesione del lgos ( * ) e del sottoscapolare ( freccia bianca ) ; notare il clb iperemico e ridotto di volume . our experience , in agreement with the literature [ 7 ] , asi was associated with more or less extensive tears of the biceps pulley , with constant involvement of the sghl . 
 minimally invasive mr arthrography can provide complete depiction of the rotator cuff , the biceps pulley and the anterior tendinous components of the rotator cuff , resulting in a valuable technique for guidance towards the most appropriate treatment , which is almost exclusively surgical in athletes [ 4 ]  . at mr arthrography , the diagnosis of type 1 lesion was accomplished when the sghl appeared not to be stretched or frayed , in both the oblique sagittal and axial planes . 
conversely , in type 2 lesions , the inhomogeneous aspect of the sghl was gia bicipitale e le componenti tendinee anteriori della cuffia dei rotatori in maniera di indirizzare in maniera precisa il paziente al trattamento pi idoneo che , nel caso dello sportivo , quasi esclusivamente chirurgico [ 4 ]  . 
 allesame artro - rm la diagnosi di lesione di tipo 1 stata posta nel caso in cui il lgos appariva deteso e sfrangiato sia sui piani di scansione sagittali - obliqui che assiali . 
questi tipi di lesione , a prevalente estrinsecazione sul versante articolare , erano caratterizzati da una insinuazione di mezzo di contrasto tra le radiol med ( 2013 ) 118 : 112122 fig . 
mr arthrography oblique sagittal fat - suppressed pd - weighted image ( b ) shows a complex lesional involvement of biceps pulley characterised by a superior glenohumeral ligament ( sghl ) tear , subscapularis tendon tear ( large black arrow ) and anterior - side supraspinatus tendon tear ( black arrow )  . 
mr arthrography axial fat - suppressed pd - weighted image ( c ) well depicts subscapularis tendon tear ( long arrows ) and anteromedial subluxation of lhbt ( large arrow )  . 
lesame artroscopico ( d ) documenta una lesione associata della porzione anteriore del sopraspinoso ( freccia ) e del sottoscapolare ( * ) con un clb che appare iperemico , sfrangiato e sublussato antero - medialmente . associated with a supraspinatus tendon tear involving its anterior insertional area . 
this type of lesion , with a prevalent manifestation on the articular portion , was characterised by the presence of contrast agent collection in the tendon fibres that , in the case of involvement / extension of or to the bursal side , leaked into the subacromiondeltoid bursa . 
type 3 lesions showed the same mr arthrography appearance as type 2 lesions , with the presence of contrast agent collection in the subscapularis fibres ; tendon interruption , in this case , showed a prevalent transverse component , better depicted on all axial images . 
at arthroscopy , only 5 / 7 cases , recognised as type 3 lesions at mr arthrography , were confirmed ; the other two cases were refibre tendinee che , nel caso di coinvolgimento / estensione del / al versante bursale stravasava nella borsa sottoacromiondeltoidea . 
le lesioni di tipo 3 mostravano le stesse caratteristiche semeiologiche delle lesioni di tipo 2 , ma con insinuazione di mezzo di contrasto tra le fibre del sottoscapolare ; le soluzioni di continuo tendinee in questo caso , presentavano una prevalente componente trasversale , ben documentabile sopratutto nelle immagini ottenute secondo piani assiali . 
allartroscopia solo 5 su 7 casi diagnosticati allartro - rm come lesione di tipo 3 sono stati confermati ; gli altri 2 pazienti sono stati classificati artroscopicamente come lesione di tipo 4 in quanto stato riscontrato un cointable 2 correlation of magnetic resonance ( mr ) arthrography results with arthroscopy lesion pattern according to habermeyer asi arthroscopy ( n ) mr arthrography ( n ) arthroscopy ( n ) radiol med ( 2013 ) 118 : 112122 120 type normal type 1 type 2 type 3 type 4 asi , anterosuperior impingement tipo normalit tipo 1 tipo 2 tipo 3 tipo 4 ias , impingement antero - superiore artro - rm ( n ) tabella 2 correlazione dei risultati artro - risonanza magnetica ( rm ) con lartroscopia pattern lesionale secondo habermeyer ias artroscopia ( n ) artroscopia ( n ) classified as type 4 due to involvement of the articular side of the supraspinatus anteriorly . volgimento lesionale della porzione anteriore del versante articolare del sopraspinoso . in type 4 lesions , the large breach of both the subscapular and supraspinatus tendons associated with sghl tear was well documented by the presence of contrast agent leakage into the periarticular recess ; in these cases , the lhbt in its angular aspect appeared thick and inhomogeneous , as from overload . 
at mr arthrography , this involvement was not always seen , as it was more evident in type 4 lesions ( seen in six cases ) and not always diagnosed in type 3 lesions ( seen in two cases )  . 
conversely , mr arthrography was accurate in diagnosing irregularity of the tubercular contour of the humeral nelle lesioni di tipo 4 , in associazione alla lesione del lgos , la breccia di lesione sia del sottoscapolare che del sopraspinoso era ben documentabile allartro - rm con marcato stravaso di mezzo di contrasto nei recessi periarticolari ; in questi casi il clb , a livello del suo tratto angolare , mostrava aspetti da sovraccarico , apparendo ispessito e disomogeneo . 
tutte le alterazioni evidenziate allartro - rm negli 8 casi classificati come lesione di tipo 4 sono state confermate allartroscopia . nella valutazione diagnostica artro - rm , oltre alle immagini ottenute secondo un piano di scansione sagittale - obliquo , quelle che hanno contribuito ad un corretto bilancio lesionale sono state le dp e se t1 - pesate con soppressione del segnale del tessuto adiposo , ottenute secondo un piano coronale nelle lesioni di tipo 2 e tipo 4 e quelle ottenute secondo un piano assiale nelle lesioni di tipo 3 e tipo 4 . 
 dalla valutazione dei nostri risultati si pu notare uneccellente correlazione artroscopia - artro - rm nelle lesioni di tipo 2 ( 5 / 5 = 100% ) e 4 ( 8 / 8 = 100% ) ed una buona correlazione nelle lesioni di tipo 3 ( 5 / 7 = 71 , 4% )  . 
nelle lesioni di tipo 1 , invece , anche in considerazione dellesiguo numero di pazienti , la correlazione artroscopia - artro - rm non stata soddisfacente ( 1 / 3 = 33 , 3% )  . 
a nostro avviso la problematica diagnostica principale delle lesioni isolate radiol med ( 2013 ) 118 : 112122 head , as confirmed by correlation with arthroscopic findings . analysis of these data showed the usefulness of mr arthrography for evaluating tendon pathology and show some limits in the case of isolated glenohumeral ligament pathology . 
the main diagnostic problem in lesions affecting the rotator interval components lies more in the presence of several anatomical variants rather than residing in the complexity of the area under examination . 
the incomplete distension of the area after contrast medium injection poses another problefor the same reasons , in our opinion , there is a general trend to underestimate type 4 lesions . 
in fact , two cases documented as type 3 at mr arthrography were considered type 4 at arthroscopy owing to the evidence of an irregular appearance of the articular aspect of the supraspinatus anteriorly . 
these lesions are not always easy to identify with mr arthrography , especially when appropriate distension of the anterosuperior capsular region is not obtained . complex lesions of the biceps pulley can be associated with lhbt instability . 
if compared with standard mr arthrography , it allows a dynamic evaluation that , besides showing certain types of anatomical injuries and related structural alterations , is also able to reveal lhbt ( micro ) instability , which usually requires other techniques for detection . patients with complex lesions with a suffering lhbt are those who show the most significant signs of asi , as shown by dynamic tests during arthroscopy . 
our experience , supported also by the literature , therefore supports the hypothesis that asi is constantly associated with an overload of the pulley - cuff system that , over time , leads to microor macroinstability of lhbt . 
 conflict of interest none delle componenti dellintervallo dei rotatori risiede , oltre che nelle complessit della regione in esame , anche nellampio spettro delle varianti anatomiche presenti a questo livello e nella non sempre adeguata distensione contrastografica dellarea in esame . 
infatti , come gi detto precedentemente , 2 casi di lesione di tipo 3 allartro - rm sono state considerate di tipo 4 allartroscopia poich era presente una irregolarit lesionale della porzione anteriore articolare del sopraspinoso , lesione questa di non sempre facile individuazione in artrorm soprattutto in presenza di una scarsa distensione della regione capsulare antero - superiore . le lesioni complesse della puleggia anteriore di riflessione possono essere associate ad una patologia da instabilit del clb ; in questi casi pu essere utile ricorrere a scansioni aggiuntive in intraed extra - rotazione o in aber . 
questo tipo di approccio allo studio del clb , a nostro giudizio appare particolarmente valido , poich aggiunge allesame artro - rm standard una valutazione dinamica che , se da una parte evidenzia un determinato tipo di danno anatomico e le modificazioni strutturali da esso derivate , da unaltra potrebbe slatentizzare o rendere meglio evidente una ( micro ) instabilit del clb non altrimenti documentabile , se non eventualmente con altra metodica . 
 proprio nei pazienti con lesioni complesse in cui si ha un clb sofferente che si apprezzano i segni pi significativi di ias come provato dai test dinamici eseguiti in corso di artroscopia . 
la nostra esperienza , confortata anche dai dati della letteratura , sostiene quindi lipotesi che lias sia associato costantemente ad un sovraccarico del sistema puleggia - cuffia che con il tempo porta ad una micro o macroinstabilit del clb . 
 in conclusione , alla luce di quanto descritto appare quanto mai importante un corretto inquadramento clinico - radiologico dei soggetti con lesioni del sistema puleggia - cuffia ed in questo lartro - rm risulta sicuramente il gold standard diagnostico . 
il mancato riconoscimento ed il conseguente mancato o inadeguato trattamento di queste alterazioni pu concorrere allo svilupparsi ed al progredire di un meccanismo a cascata in cui verosimilmente la sublussazione anteromediale e la tendinopatia del clb sono gli eventi terminali . 
longo , department of physics , university of trieste & infn , via valerio 2 , 34100 trieste , italy , tel . : + 39 - 040 - 5583383 , fax : + 39 - 040 - 558 3350 , e - mail : renata.longo@ts.infn.it received : 26 july 2011 / accepted : 23 august 2011 / published online : 28 june 2012 springer - verlag 2012 abstract objective . 
the study was performed at the synchrotron radiation for medical physics ( syrmep ) beamline of the elettra synchrotron radiation ( sr ) facility in trieste ( italy ) ; x - ray beams were in the range 1622 kev with a high degree of monochromaticity and spatial coherence . 
lo studio stato condotto presso le linea synchrotron radiation for medical physics ( syrmep ; elettra , trieste ) utilizzando fasci di raggi x monocromatici , ad alta coerenza spaziale , con energia compresa tra 16 e 22 kev . 
fantocci e campioni chirurgici sono stati impiegati per le prove iniziali ; immagini ottenute a syrmep su pellicola e su cr sono state confrontate con immagini ottenute presso un mammografo digitale . 
le immagini acquisite a syrmep su pellicola e su cr sono state ottenute a parit di dose ; la qualit delle immagini cr risultata confrontabile o superiore a quella con pellicola . 
il sistema cr analizzato risulta adeguato per eseguire mammografie in contrasto di fase . 90 radiol med ( 2013 ) 118 : 89100 keywords mammography phase - contrast imaging synchrotron radiation parole chiave mammografia phase contrast imaging luce di sincrotrone introduction introduzione the past decade saw the development of techniques exploiting the undulatory properties of the incident x - ray beam to improve the quality of radiographic images . 
this geometry allows transformation of the phase modulation caused by the beam passing through elements with different optical properties into an amplitude modulation , which creates additional contrast to the absorption contrast thereby enhancing the visibility of the edges of structures ( edge enhancement ) [ 1 ]  . 
this effect can only be visualised if high - resolution detectors are used and if the imaging system has a high degree of spatial coherence ; the degree of spatial coherence of a system is inversely proportional to its distance from the object to be imaged [ 2 ]  . 
 in consideration of the low contrast of breast tissue due to absorption , these techniques are particularly indicated , and are thus being investigated , in the field of breast imaging [ 27 ]  . 
the first clinical trial of phase - contrast mammography with synchrotron radiation ( sr ) is underway at the synchrotron radiation for medical physics ( syrmep ) beamline of the elettra synchrotron in trieste , italy [ 8 , 9 ]  . 
 the phase contrast that characterises mammography with sr provides better depiction of tissue edges and therefore increases the visibility of breast structure and possible lesions compared with images obtained with a direct radiography ( dr ) digital mammography unit [ 10 ]  . 
the trial was started with screen - film systems used as detectors because a very high spatial resolution is needed to visualise the edge enhancement effects typical of the technique [ 11 ]  . 
the introduction into the italian market of computed radiography ( cr ) mammography systems with adequate spatial resolution [ 12 ] prompted our group to verify the feasibility of using such systems in phase - contrast mammography . 
to this end , collaboration was started with fuji italia , which led to the use of the fuji fcr profectcs ( pixel size 50 m ) system on test objects and surgical specimens . 
the adequacy of the systems spatial resolution for visualising lultima decade ha visto lo sviluppo di tecniche volte a sfruttare le propriet ondulatorie del fascio incidente di raggi x per incrementare la qualit delle immagini radiografiche . 
questa geometria consente di trasformare la modulazione di fase che si produce quando il fascio attraversa elementi con propriet ottiche diverse , in una modulazione in ampiezza che crea un contrasto aggiuntivo rispetto al contrasto dassorbimento migliorando la visibilit dei bordi delle strutture ( edge enhacement ) [ 1 ]  . 
il grado di coerenza spaziale di un sistema tanto maggiore quanto pi piccola la dimensione della sorgente e quanto pi grande la sua distanza dalloggetto da radiografare [ 2 ]  . 
presso la linea synchrotron radiation for medical physics ( syrmep ) della macchina di luce elettra di trieste in corso la prima sperimentazione clinica di mammografia in contrasto di fase con luce di sincrotrone [ 8 , 9 ]  . 
il contrasto di fase che caratterizza le mammografie con luce di sincrotrone consente una migliore visualizzazione dei contorni dei tessuti aumentando la visibilit , sia della struttura mammaria , che delle lesioni , rispetto alle immagini ottenute con un mammografo digitale direct radiology ( dr ) [ 10 ]  . 
la sperimentazione stata avviata utilizzando come rivelatori dimmagine sistemi schermo - pellicola poich , per poter visualizzare gli effetti di edge enhancement tipici di tale tecnica , richiesta al rivelatore una risoluzione spaziale molto spinta [ 11 ]  . 
lintroduzione sul mercato italiano di sistemi di computed radiology ( cr ) per mammografia con risoluzione spaziale adeguata [ 12 ] , ha indotto radiol med ( 2013 ) 118 : 89100 phase effects was verified by using a specially designed object . 
the good quality of the results achieved then prompted the decision to use the cr system to examine two patients participating in the clinical trial of mammography with sr . materials and methods the syrmep beamline allows mammography to be carried out using a laminar beam with a cross - section of 220.3 cm2 at the compression unit and tuneable monochromatic energy between 17 and 22 kev . 
the size of the beam requires a vertical scan to produce a two - dimensional image and , because the beam is fixed in space , it is the breast and the detector that must be moved synchronously during the acquisition . 
the bed can be rotated 360 around the vertical axis to obtain craniocaudal ( cc ) and mediolateral oblique ( mlo ) views ; this feature will also allow future tomographic imaging techniques to be developed . 
1 posizionamento della paziente sul lettino dedicato alla mammografia nella sala radiologica allestita presso la linea di luce syrmep del sincrotrone elettra di trieste . il nostro gruppo a verificare la possibilit di utilizzare tali sistemi anche nella mammografia in contrasto di fase . 
in questottica nata una collaborazione con fuji italia che ci ha portato a utilizzare il sistema fuji fcr profectcs ( pixel size 50m ) su oggetti test e reperti operatori . 
i buoni risultati conseguiti hanno determinato la scelta di utilizzare il sistema cr nellesame di due pazienti arruolate nellambito dello studio clinico di mammografia con luce di sincrotrone . materiali e metodi la linea di luce syrmep consente di utilizzare per la mammografia un fascio laminare di sezione 220 , 3 cm2 alla posizione del compressore ed energia monocromatica selezionabile tra 17 kev e 22 kev . 
date le dimensioni del fascio necessaria una scansione verticale per produrre unimmagine bidimensionale ed , essendo il fascio fisso nello spazio , durante lacquisizione sono la mammella ed il rivelatore a venir traslati in modo sincrono . 
il lettino pu essere ruotato di 360 attorno allasse verticale per ottenere le proiezioni cranio - caudale ( cc ) e media - laterale obliqua ( mlo ) e consentendo futuri sviluppi di tecniche tomografiche . 
sul fascio di radiazione x , a monte della paziente , posta una coppia di camere a ionizzazione calibrate per interconfronto rispetto al campione primario di riferimento per le basse energie del laboratorio metrologico dellenea [ 1315 ]  . 
le letture delle camere sono acquisite durante tutto lesame per misurare on - line il valore del kerma in ingresso allorgano al fine di garantire la sicurezza dellesposizione e consentendo , peraltro , la dosimetria in vivo nel corso dellesame . 
la visualizzazione degli effetti di fase ottenuta allontanando il rivelatore dallorgano da radiografare ; per questo motivo il rivelatore stato posto ad una distanza di 2 m dalluscita 92 radiol med ( 2013 ) 118 : 89100 ment ( enea ) metrological laboratory [ 1315 ]  . 
the readings of the ionising chambers are acquired throughout the examination to measure online the entrance air - kerma value and ensure safety of the exposure , as well as allowing in vivo dosimetry during the examination . 
 visualisation of the phase effects is obtained by moving the detector away from the organ being imaged ; for this reason the detector was placed 2 m away from the compression unit , behind an antiscattering screen that has a slit opening in correspondence with the direct x - ray beam ; this way , the contribution of scattered radiation to image formation is minimised without reducing the efficiency of the detector , unlike the case with antiscattering grids . 
 in this study , we compared images obtained with sr , under the same exposure conditions with a screen - film system ( kodak min - r 2000 ) and a computed radiography ( cr ) system ( fuji fcr profectcs ) and those acquired with a direct radiography ( dr ) mammography unit senographe2000d ( general electric , milwaukee , wi , usa )  . at first we studied a test object consisting of six nylon threads attached to a 3 - cm - thick plexiglas slab ; the diameter of the threads was 100 m , 200 m , 350 m , 480 m , 550 m and 700 this simple test object provides a good demonstration of the efficacy of the phase - contrast technique compared with the absorption technique . 
the finer threads are , in fact , virtually invisible in the absorption images owing to their low intrinsic contrast ; phase - contrast imaging , specifically devised for use with low - contrast objects , makes such objects discernible thanks to the edge - enhancement effect . 
the images of the test object demonstrated that the cr system had sufficient spatial resolution for this application . next , we acquired images of surgical specimens : three total mastectomies and five quadrantectomies . 
all tissues were studied fresh ( without fixative ) , so the number of images acquired for each specimen was determined by the need not to compromise the subsequent histological and biomolecular examination . 
after the patients informed consent had been obtained by the surgeon , the pathologist personally collected the specimen from the operating theatre and inserted it into the plastic bag , which he immediately sealed with a vacuum packing device . 
 dal compressore , dietro ad uno schermo antiscattering su cui aperta una fenditura in corrispondenza del fascio diretto di radiazione x ; in tal modo si minimizza il contributo della radiazione diffusa alla formazione dellimmagine senza ridurre lefficienza del sistema di rivelazione , a differenza di quanto avviene con la griglia antiscattering . 
 in questo studio sono state confrontate le immagini ottenute con luce di sincrotrone , nelle medesime condizioni di esposizione , con un sistema schermo pellicola ( kodak minr 2000 ) e un sistema di cr ( fuji fcr profectcs ) e quelle acquisite mediante mammografo dr senographe2000d ( general electric , milwaukee , wisconsin , usa )  . inizialmente stato studiato un oggetto test costituito da 6 fili di nylon applicati su uno spessore omogeneo di 3 cm di plexiglass il cui diametro rispettivamente 100 m , 200 m , 350 m , 480 m , 550 m e 700 questo semplice oggetto test consente di illustrare lefficacia della tecnica in contrasto di fase rispetto a quella in assorbimento . 
i fili pi sottili sono , infatti , praticamente invisibili nelle immagini in assorbimento a causa del loro basso contrasto intrinseco , mentre il contrasto di fase , presente proprio per oggetti di queste caratteristiche , li rende riconoscibili grazie alleffetto che ne evidenzia i contorni . 
le immagini delloggetto test con i fili di nylon hanno consentito di dimostrare ladeguatezza della risoluzione spaziale del sistema cr per questa applicazione . in seguito sono state acquisite immagini di alcuni tessuti operatori : tre mastectomie totali e cinque quadrantectomie . 
tutti i tessuti sono stati studiati a fresco ( senza laggiunta del fissativo ) , e quindi la quantit di immagini acquisite per ciascun campione stata condizionata dalla necessit di non compromettere il successivo studio istologico e biomolecolare dei tessuti . 
previa acquisizione da parte del chirurgo del consenso informato della paziente , lanatomopatologo ha provveduto personalmente a ritirare il campione dalla sala operatoria e ad inserirlo nella busta di plastica ed immediatamente a sigillarla con strumento in grado di creare il vuoto . 
al termine di questa procedura la busta con il campione stata inserita in una borsa refrigerata con ghiaccio per consentire la conservazione ottimale del materiale durante il trasporto al laboratorio elettra . 
 lanatomopatologo stato sempre presente a tutte le fasi di acquisizione delle immagini a garanzia del rispetto dei tempi e per una corretta manipolazione del campione necessaria allacquisizione delle diverse scansioni . 
al termine delle acquisizioni delle immagini lo stesso anatomopatologo ha provveduto a portare il campione al laboratorio di istopatologia dove stato estratto dalla busta sigillata ed immerso nel fissativo ( formalina neutra tamponata al 10% )  . 
 a ci hanno fatto seguito le normali tappe istopatologiche radiol med ( 2013 ) 118 : 89100 at the end of the examination , the pathologist personally took the samples to the histopathology laboratory where they were removed from the sealed plastic bag and immersed in fixative ( 10% buffered neutral formalin )  . 
this was followed by the usual histopathological steps of sampling and processing following the standard protocol of the laboratory . tissues from quadrantectomies were relatively small and presented no anatomical landmarks that might help to define the projection used . 
 mammography with sr was then performed with the cr system on two patients selected on the basis of the enrolment criteria for the research project approved by the local ethics committee [ 10 ]  . 
for each image obtained at the syrmep beamline , the mean glandular dose was derived from the incident airkerma , the x - ray - beam energy being known [ 16 ]  . 
for images obtained with the dr mammography system , known variables are the anode - filter combination , applied voltage , current delivered and air - kerma estimate provided by the mammography system on the basis of which we evaluated glandular dose [ 17 ]  . 
 di campionamento e processamento , come previsto dal protocollo standard del laboratorio . i tessuti da quadrantectomie erano piuttosto piccoli e privi di reperi anatomici per consentire la definizione della proiezione utilizzata . 
 successivamente sono state sottoposte ad indagine mammografica con luce di sincrotrone , col sistema cr in studio , due pazienti selezionate secondo i criteri di arruolamento previsti nel progetto di ricerca approvato dal comitato etico competente [ 10 ]  . 
per ciascuna delle immagini ottenute presso la linea syrmep la dose ghiandolare media stata calcolata a partire dalla misura del kerma in aria incidente , nota lenergia del fascio di raggi x [ 16 ]  . 
per le immagini ottenute col mammografo digitale sono note la combinazione anodo filtro , la tensione applicata , la corrente erogata e la stima del kerma in aria fornita dal mammografo stesso in base alla quale stata valutata la dose ghiandolare [ 17 ]  . 
nelle immagini acquisite con mammografo in modalit standard solo i 4 fili di diametro maggiore ( 350 , 480 , 550 e 700 m ) sono visibili , mentre nelle immagini ottenute in modalit mirata anche il filo di diametro pari a 200 m , per un totale di 5 / 6 , visibile , ma con un aumento della dose in ingresso di un fattore circa tre rispetto allimmagine standard , ottenuta a dosi simili a quelle impiegate per le immagini con luce di sincrotrone . 
d immagine acquisita con mammografo dr in modalit mirata mo / mo , 27 kvp , 40 , 6 mas , ese = 5 , 95 mgy . a factor of three compared to the standard image , obtained at similar doses to those used for the images with sr . 
 campioni chirurgici surgical specimens for all images of surgical specimens , we studied the dependence of image quality on variations of beam energy , with both cr and screen - film systems . 
moreover , for each tissue , we produced a reference image with the dr mammography syste the sample on which we were able to perform the most complete study while adhering to acquisition time and transport constraints was one of the quadrantectomy specimens . 
 thickness of the compressed tissue was approximately 2 cin the case of mammography with sr within the clinical protocol adopted at the syrmep beamline , an x - ray beam energy of 17.5 kev would be used for a compressed breast thickness of 2 cthe image of the same specimen imaged with the dr mammography system is shown in figure 3 . 
 two complete sets of images of this specimen were acper tutti i campioni chirurgici acquisiti stata studiata la dipendenza della qualit delle immagini al variare dellenergia del fascio , sia con il sistema cr sia con il sistema schermo pellicola . 
evaluation of sr images obtained on film showed that the loss of contrast with increasing beam energy is such that images obtained at energies > 19.5 kev are diagnostically unacceptable . subsequently , mammograms obtained at each monochromatic energy at the synchrotron and the reference mammogram obtained with the dr system were ordered according to image quality by assigning a score of 1 to the best image and 3 to the worst ( table 1 )  . 
above this level , cr image obtained with monochromatic beam continued to be preferable to that produced with the conventional spectrum , which in turn was better than the film image produced with sr . 
alla valutazione comparativa delle immagini con luce di sincrotrone ottenute su pellicola risultato che la perdita di contrasto al crescere dellenergia del fascio tale da rendere non accettabili , dal punto di vista diagnostico , le immagini ottenute a energie superiori a 19 , 5 kev . successivamente sono state messe in ordine decrescente , in termini di qualit dellimmagine , le mammografie ottenute al sincrotrone a ciascuna energia monocromatica e la mammografia di riferimento ottenuta con il sistema dr assegnando un punteggio pari a 1 allimmagine migliore e 3 alla peggiore ( tabella 1 )  . 
il confronto qualitativo indi ca che le immagini ottenute con luce di sincrotrone riportano sempre una valutazione migliore rispetto alle imma gini del mammografo fino ad unenergia di 19 kev . 
al di sopra di questa energia limmagine cr ottenuta con fa scio monocromatico continua ad essere preferibile rispetto a quella prodotta con spettro convenzionale men96 radiol med ( 2013 ) 118 : 89100 fig . 
il film , invece , risulta pre feribile al sistema cr per le energie molto basse ( 16 , 5 17 , 5 ) seppure con una differenza minima nel giudizio di qualit , e pari ad esso a 18 e 18 , 5 kev . 
si noti come per le energie al di sotto dei 17 kev i valori di kerma siano eccessivamente alti per un possi bile utilizzo clinico di tali energie nella attuale configu razione . 
 mammografie cliniche nelle mammografie eseguite su due pazienti selezionate secondo i criteri usati per lo studio clinico in corso [ 10 ] , la mammografia con luce di sincrotrone ha consentito di ottenere un dettaglio di immagine superiore rispetto a quanto ottenibile con il mammografo dr . 
 con la mammografia digitale in questa paziente era stata riscontrata una minima distorsione parenchimale con due calcificazioni sovrapposte in sede paraareolare a destra ( r4a bi - rads )  . 
b dettaglio di a : minima distorsione parenchimale in sede para - areolare superiore destra con calcificazione tondeggiante ( r4a ) ; c immagine digitale in contrasto di fase acquisita con luce di sincrotrone in proiezione mlo : spessore 4 , 8 cm , energia del fascio di raggi x 19 , 5 kev , ese 2 , 15 mgy , dgm 0 , 72 mgy ; d dettaglio di c : si evidenzia opacit con distorsione a margini sfumati e calcificazioni ( r4c )  . mography detected minimal architectural distortion with two overlying calcifications in the right para - areolar region ( bi - rads r4a )  . 
the distortion was not confirmed by mammography with sr , which better depicted the microfibronodular structure of the breast parenchyma and showed features consistent with benign disease ( r3 )  . 
the patient was also negative at follow - up mammography and us at 2 years . discussion and conclusions images of the test object made with nylon threads show that the cr system is adequate for use in phase - contrast mammography , as it allows visualisation of the same number of threads identified on the screen - film system with sr . 
con la mammografia con luce di sincrotrone la distorsione non stata confermata perch stato possibile valutare meglio il parenchima ghiandolare nella sua struttura microfibronodulare e tale area presentava caratteristiche compatibili con un quadro di benignit ( r3 )  . 
la paziente risultata negativa al follow - up mammografico ed ecografico a due anni . discussione e conclusioni le immagini delloggetto test realizzato con fili di nylon mostrano che il sistema cr studiato adeguato per essere utilizzato per la mammografia in contrasto di fase , in quanto permette la visualizzazione dello stesso numero di fili visibili con sistema schermo - pellicola , sempre con luce di sincrotrone . 
in particolare il sistema cr studiato presenta una risoluzione spaziale sufficiente alla visualizzazione degli effetti di fase che contribuiscono in modo decisivo nellaggiungere qualit diagnostica alle immagini radiologiche con luce di sincrotrone rispetto a quelle ottenute con mammografo convenzionale . 
 nello studio della dipendenza dallenergia della qualit delle immagini di campioni chirurgici non stupisce il fatto che alle energie pi elevate , dove il contrasto intrinseco dellimmagine risulta pi basso , le immagini su pellicola radiol med ( 2013 ) 118 : 89100 fig . 
7a immagine ottenuta con mammografo digitale in proiezione mlo ; spessore 4 , 4 cm , rh / rh , 29 kvp , 57 , 9 mas , ese 5 , 65 mgy , dgm 1 , 19 mgy ; b dettaglio di a : distorsione parenchimale ai quadranti superiori in mammografia digitale ( r4a ) ; c immagine digitale in contrasto di fase acquisita con luce di sincrotrone in proiezione mlo : spessore di 4 , 5 cm , energia del fascio di raggi x 19 kev , ese 3 , 06 mgy , dgm 0 , 88 mgy ; d dettaglio di c : parenchima a struttura in parte microfibronodulare senza evidenza di lesioni sospette ( r3 )  . sr compared with those obtained with conventional mammography . 
 in the study of energy dependence of image quality of surgical specimens , it is not surprising that at higher energies , where intrinsic image contrast is lower , film images show lower quality than do cr images . 
in this case , the intrinsic contrast of the object at the polychromatic spectrum used by the dr mammography unit is higher ( mo / mo , 26 kvp ) and , being digital , both systems allow contrast to be maximised . 
therefore , the better image quality obtained at the syrmep beamline can be ascribed to phase contrast . results obtained on test objects and tissue specimens allowed the cr system to be used within the clinical trial according to the examination protocol already in use and optimised for film exposures . 
 in conclusion , mammography with sr and cr detectors provided better diagnostic confidence compared with conventional mammography in the two patients studied : it provided a diagnosis of malignancy in the first patient and risultino di qualit inferiore a quelle acquisite con cr . 
 invece interessante notare che col sistema cr anche le immagini ottenute alle energie pi alte , dove lenergia del fascio monocromatico risulta superiore allenergia media dello spettro policromatico , risultano migliori di quelle ottenute col mammografo digitale , pur essendo associate a dosi in ingresso fino 10 volte inferiori a quella rilasciata nellacquisizione standard al mammografo ( ese = 1 , 7 mgy al mammografo mentre con luce di sincrotrone a 22 kev ese = 0 , 14 mgy )  . 
in questo caso il contrasto intrinseco delloggetto allo spettro policromatico utilizzato dal mammografo dr pi elevato ( mo / mo , 26 kvp ) ed entrambi i sistemi , in quanto digitali , consentono una massimizzazione del contrasto . 
pertanto la miglior qualit dellimmagine ottenuta alla linea syrmep attribuibile al contrasto di fase . questi risultati ottenuti su oggetti test e tessuti hanno consentito lutilizzo del sistema cr in esame nellambi to dello studio clinico in corso secondo il protocollo desame gi utilizzato e ottimizzato per lesposizione delle pellicole . 
 in conclusione la mammografia con luce di sincrotrone e rivelatore cr ha permesso di ottenere una maggior confidenza diagnostica nelle due pazienti studiate rispetto allindagine mammografica tradizionale , ponendo diagnosi di malignit nella prima paziente e di benignit nella seconda , laddove la mammografia digitale individuava una lesione di dubbia natura . 
questo studio , pertanto , apre la 100 radiol med ( 2013 ) 118 : 89100 of benign disease in the second , where digital mammography had identified an equivocal lesion . 
la qualit delle immagini digitali con luce di sincrotrone ottenute ad alta energia e bassa dose indica la possibilit di una ulteriore ottimizzazione nellutilizzo clinico della radiazione di sincrotrone con rivelatori digitali che lascia spazio allintroduzione di tecniche pi complesse ( ad esempio tomografiche )  . 
simonetti dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , fondazione policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy correspondence to : g . 
twelve nhl patients who were candidates for bmt underwent three mr examinations of the lumbosacral spine : before ablative therapy for bmt , 154 days and 5424 days after bmt . 
 we observed a statistically significant difference between ff values calculated at the various mr studies ( p = 0.02 ) and between red blood cell count ( p = 0.017 ) , platelet count ( p = 0.003 ) and haematocrit ( p < 0.001 ) at the three mr studies . 
mr spectroscopy of the bone marrow of nhl patients undergoing bmt is noninvasive and highly sensitive for characterising and monitoring bone marrow after bmt . keywords bone marrow transplantation 3 - tesla magnetic resonance spectroscopy riassunto obiettivo . 
scopo del presente lavoro stato valutare lutilit della spettroscopia mediante risonanza magnetica ( rm ) a 3 tesla nei pazienti affetti da linfoma non - hodgkin ( lnh ) sottoposti a trapianto di midollo osseo ( tmo )  . 
dodici pazienti affetti da lnh candidati al tmo sono stati sottoposti a 3 esami rm del rachide lombo - sacrale : prima della terapia ablativa per il tmo , dopo 154 giorni dal tmo e dopo 5424 giorni . 
abbiamo osservato una differenza statisticamente significativa tra i valori di ff calcolati ai vari controlli rm ( p = 0 , 02 ) , tra il numero dei globuli rossi ( p = 0 , 017 ) , delle piastrine ( p = 0 , 003 ) e tra i valori dellematocrito ( p < 0 , 001 ) tra i tre controlli rm . 
la rm con studio spettroscopico del midollo osseo su pazienti con lnh sottoposti a tmo rappresenta una metodica non invasiva e molto sensibile nella caratterizzazione e monitoraggio del midollo osseo dopo tmo . 
 parole chiave trapianto di midollo osseo risonanza magnetica ( rm ) a 3 tesla spettroscopia 102 introduction transplantation of haematopoietic stem cells , or bone marrow transplantation ( bmt ) , is considered a powerful therapeutic aid for treating many haematological and lymphatic diseases , as it enables the use of higher doses of cytotoxic chemotherapy agents in combination with radiotherapy [ 15 ]  . 
regardless of the type of transplant , the posttransplant course may often be affected by a series of complications , such as opportunistic infections , slow marrow repopulation and recurrence or graft - versus - host disease ( gvhd )  . 
 monitoring marrow recovery following bmt is therefore an essential step in managing these patients [ 6 , 7 ] and is usually done with a full blood count on peripheral blood , iliac crest biopsy and bone marrow aspiration . 
however , in addition to being invasive and painful , the latter procedures are carried out on a single location and therefore often fail to provide information regarding the entire haematopoietic system and cellularity and composition of the bone marrow . 
magnetic resonance ( mr ) spectroscopy of the bone marrow , correlated with the preand posttransplant blood parameters , can provide information on the composition and possible physiological and pathological changes in vertebrae bone marrow before , during and after treatment . 
 the main aim of our study was to analyse changes in certain specific mr spectroscopy parameters in patients affected non - hodgkins lymphoma ( nhl ) subjected to autologous bmt by means of follow - up examinations and to correlate such changes with blood parameters and specific characteristics of the transplant in order to assess the usefulness of follow - up with 3 - tesla mr imaging . 
 radiol med ( 2013 ) 118 : 101111 introduzione il trapianto di cellule staminali emopoietiche ( tmo ) ora considerato un importante ausilio terapeutico per il trattamento di molte emolinfopatie , permettendo lutilizzo di pi alte dosi di farmaci chemioterapici citotossici in combinazione con la radioterapia [ 15 ]  . 
indipendentemente dalla tipologia di trapianto , il decorso post - trapianto pu essere spesso influenzato da una serie di complicanze quali infezioni opportunistiche , una lenta ripopolazione midollare , comparsa di recidive e la reazione contro lospite ( graftversus - host disease , gvhd ) ; il trapianto autologo di cellule staminali e di cellule staminali periferiche pu notevolmente ridurre lincidenza di tali eventi . 
questultime oltre ad essere procedure invasive e dolorose , essendo ottenute da una singola localizzazione , spesso non forniscono dati rappresentativi dellintero sistema ematopoietico , della cellularit e della composizione del midollo osseo . 
la risonanza magnetica ( rm ) con indagine spettroscopica ( mrs ) del midollo osseo , correlata con i parametri ematologici pree post - trapianto di cellule staminali emopoietiche consente di ottenere , in maniera non invasiva , informazioni sulla composizione e sulle eventuali alterazioni fisiologiche e patologiche del midollo osseo presenti nelle vertebre prima , durante e dopo il trattamento . 
 lobiettivo principale del nostro studio stato quello di analizzare le variazioni espresse da determinati e specifici parametri di mrs nei pazienti affetti da linfoma nonhodgkin ( lnh ) sottoposti a trapianto autologo di cellule staminali emopoietiche effettuando controlli a distanza e correlandoli con i parametri e le caratteristiche specifiche del trapianto al fine di poter stabilire lutilit del follow - up mediante esame rm a 3 tesla . 
sono stati studiati un totale di 12 pazienti maschi , con et media di 357 , 2 anni , affetti da lnh candidati al tmo autologo , confrontati con 12 soggetti di controllo concordi per et e sesso . 
ogni paziente ha eseguito 3 radiol med ( 2013 ) 118 : 101111 examinations : the first immediately prior to ablative therapy , the second approximately 15 days after bmt and the third approximately 3 months after bmt . 
 controlli di rm del rachide lombo - sacrale : il primo controllo subito prima dellinizio della terapia ablativa per il tmo , il secondo a distanza di circa quindici giorni dallesecuzione del tmo e il terzo dopo circa tre mesi . 
 image acquisition acquisizione delle immagini morphological and metabolic spectroscopy images were acquired with a 3 - tesla unit ( philips intera achieva , best , the netherlands ) equipped with maximum gradient amplitude and slew rate of 80 mt / m and 200 mt / m / ms , respectively ; we used body coils for signal transmission and synergy spine phased - array coils for signal reception . 
the lumbar spine was studied using the following sequences : t2 turbo spin echo ( tse ) , including the entire lumbar - sacral segment in the acquisition volume [ time to repetition ( tr ) 5 , 086 ms , time to echo ( te ) 120 ms ] ; t1 - weighted tse ( tr 265 ms , te 7.2 ms ) ; t2 - weighted tse with selective fat signal suppression [ short - tau inversion recovery ( stir ) ] to assess the presence of spongy bone oedema , which is an indication of recent fracture for collapsed vertebral bodies or of neoplastic replacement as regards the vertebral bodies involved by disease . 
all sequences were acquired in the sagittal plane with a slice thickness of 4 mm and interslice gap of 0.4 mm ; field of view was 300 mm , with a matrix of 352280 . 
on the basis of the t2 - weighted , especially stir , images , two independent observers identified the midlumbar vertebrae with normal signal intensity , which were selected for spectroscopic acquisition volume placement . 
acquisition was performed with a 2d double spin - echo point - resolved spatially localised spectroscopic sequence ( press ) , with single voxel analysis ( tr 2 , 000 ms , te 40 ms , spectral amplitude 2 , 000 hz , matrix 512512 , nominal voxel resolution 151515 mm )  . 
 the volume of interest ( voi ) was selected on the basis of sagittal t2 - weighted and t2 - stir images taking care to select a homogeneous volume of vertebral body . 
 le immagini morfologiche , cos come quelle metaboliche di spettroscopia , sono state acquisite con unapparecchiatura ad alto campo da 3 t ( philips intera achieva , best , paesi bassi ) equipaggiata con gradienti di ampiezza massima e tempo di salita di 80 mt / m e 200 mt / m / ms rispettivamente , utilizzando la bobina del corpo per la trasmissione degli impulsi di eccitazione e delle bobine sinergy spine phasedarray per la ricezione del segnale . 
lo studio del rachide lombare stato eseguito mediante le seguenti sequenze : t2 - turbo spin echo ( tse ) , includendo nel volume dacquisizione lintero tratto lombo - sacrale [ tempo di ripetizione ( tr ) 5086 ms , tempo di eco ( te ) 120 ms ] ; tse t1 pesata ( tr 265 ms , te 7 , 2 ms ) ; tse t2 pesata con soppressione selettiva del segnale del tessuto adiposo ( short - tau inversion recovery , stir ) al fine di valutare leventuale presenza di edema intraspongioso , indice di frattura recente per i somi vertebrali crollati o di sostituzione neoplastica per quanto riguarda i somi vertebrali sede di localizzazione di malattia . 
tutte le sequenze sono state acquisite sul piano sagittale con spessore di strato di 4 mm ed intervallo tra le sezioni di 0 , 4 mm ; il campo di vista ( fov ) era di 300 mm con una matrice di 352280 . 
 sulla base delle immagini t2 pesate , soprattutto stir , sono state individuate da due osservatori indipendenti le vertebre a livello medio - lombare con normale intensit di segnale , selezionate per il successivo posizionamento del volume di acquisizione spettroscopica . 
lacquisizione stata eseguita con sequenza double spin - echo point - resolved spatially localized spectroscopic sequence ( press ) con tecnica bidimensionale , con analisi single voxel ( tr 2000 ms , te 40 ms , ampiezza spettrale 2000 hz , matrice di 512512 , risoluzione nominale del voxel di 15 mm15 mm15 mm )  . 
 il volume dinteresse sottoposto ad analisi spettroscopica ( voi ) stato selezionato sulla base delle immagini t2pesate e t2 - stir sul piano sagittale , cercando di scegliere un volume di corpo vertebrale il pi possibile omogeneo . 
al fine di valutare la variabilit intra - osservatore e inter - osservatore , ciascun operatore , indipendentemente dallaltro , ha selezionato per ogni esame 2 voi sulla medesima vertebra e registrato i risultati dellanalisi spettroscopica . 
1 esempio di posizionamento del voxel per la spettroscopia allinterno del soma vertebrale di l3 in un paziente di controllo . statistical analysis each observer analysed 72 spectroscopies for a total of 144 observations . 
ff values recorded by the two observers for each patient at the same time points ( t0 , t1 , t2 ) were matched to create a bland - altman plot [ 8 ] , and lins method [ 9 , 10 ] was used to calculate the interobserver coefficient of concordance ( rho - c ) and the limits of agreement . 
 similarly , ff pair values recorded by each observer for the same patient at the same time ( t0 , t1 , t2 ) were used to create a bland - altman plot was for each observer , and limits of agreement and repeatability coefficient were calculated . 
a value of p < 0.05 was considered to indicate statistical significance . results data obtained were assessed by two radiologists and one haematologist working in consensus ( gs , am , lc )  . 
appaiando i valori di ff rilevati dai due osservatori per ciascun paziente nel medesimo tempo t ( t0 , t1 , t2 ) stato realizzato un grafico di bland - altman [ 8 ] e , mediante il medoto di lin [ 9 , 10 ] , stato calcolato il coefficiente di concordanza inter - osservatore ( rho_c ) ed i limiti di accordo . 
analogamente , appaiando le coppie di valori di ff rilevati da ciascuno dei due osservatori per lo stesso paziente , nel medesimo tempo t ( t0 , t1 , t2 ) , stato costruito un grafico di bland - altman per ciascun osservatore e sono stati calcolati i limiti di accordo ed il coefficiente di ripetibilit . 
lemocromo ha mostrato un numero di globuli rossi alla prima rm di 4 , 290 , 3106 / mm3 , di piastrine di radiol med ( 2013 ) 118 : 101111 fig . 
spectroscopy before ( a ) and 11 ( b ) and 84 ( c ) days after bmt shows net increase of ff% associated with decrease in water peak at the second and third follow - up examination , indicating a failed bone marrow recovery ( platelet count at the third follow - up was 30103 / mm3 )  . 
at the second mr examination , the rbc count was 3.50.5 million / mm3 , platelet count 104132 thousand / mm3 and wbc count was 7.25.2 thousand / mm3 , with 6.324.7 thousand / mm3 neutrophils and 0.220.12 thousand / mm3 lymphocytes . 
 at the third mr examination , rbc count was 3.40.9 million / mm3 , platelets 3720 thousand / mm3 and wbc 6.28 thousand / mm3 , with 57.5 thousand / mm3 neutrophils and 0.620.4 thousand / mm3 lymphocytes . 
 these was a statistically significant difference between ff calculated at the various time points ( p = 0.02 ) between rbc ( p = 0.017 ) , platelet ( p = 0.003 ) and haematocrit ( p < 0.001 ) values , whereas no significant differences were found in the overall number of wbc ( p = 0.63 ) , neutrophils ( p = 0.22 ) and platelets ( p = 0.22 ) between the three time points ( table 1 )  . 
the mean of the differences between ff record19434103 / mm3 e di globuli bianchi di 6 , 44 , 7103 / mm3 , con un numero medio di neutrofili di 54 , 9103 / mm3 e di linfociti di 0 , 710 , 31103 / mm3 . 
alla seconda rm abbiamo osservato un numero di globuli rossi di 3 , 50 , 5106 / mm3 , un numero di piastrine di 104132103 / mm3 e un numero di leucociti di 7 , 25 , 2103 / mm3 , con 6 , 324 , 7103 / mm3 neutrofili e 0 , 220 , 12103 / mm3 linfociti . 
il terzo controllo rm ha mostrato 3 , 40 , 9106 / mm3 di globuli rossi , 3720103 / mm3 di piastrine e 6.28103 / mm3 di leucociti , con 57 , 5103 / mm3 neutrofili e 0 , 620 , 4103 / mm3 linfociti . 
 vi una differenza statisticamente significativa tra i valori percentuali di ff calcolati ai vari controlli rm ( p = 0 , 02 ) , tra il numero dei globuli rossi ( p = 0 , 017 ) , delle piastrine ( p = 0 , 003 ) e tra i valori dellematocrito ( p < 0 , 001 ) ; mentre non si sono osservate differenze statisticamente significative nel numero dei globuli bianchi in toto ( p = 0 , 63 ) , dei neutrofili ( p = 0 , 22 ) e delle piastrine ( p = 0 , 22 ) tra i tre controlli rm ( tabella 1 )  . 
la percentuale ff presenta una correlazione statisticamente significativa con il numero delle piastrine ( r = 0 , 72 ; p = 0 , 01 ) , mentre non stata osservata nessuna correlazione statisticamente significativa tra la ff e il numero dei globuli rossi , dei globuli bianchi , dei neutrofili , dei linradiol med ( 2013 ) 118 : 101111 fig . 
il coefficiente di ripetibilit del primo osservatore 7 , 5% ( p < 0 , 05 ) , mentre per il secondo osservatore 6 , 98% ( p < 0 , 05 )  . the literature contains many studies on the application of mr imaging to patients with blood and lymph node diseases [ 1115 ]  . 
 [ 6 ] states that mr imaging of the lumbosacral spine , in contrast to biopsy techniques that demonstrate only the local composition of the bone marrow , provides both a characterisation of the composition of the haematopoietic bone marrow and an estimation of the spatial distribution of water and fat , thereby enabling a global and noninvasive evaluation of the bone marrow and providing important additional discussione in letteratura vi sono diversi studi riguardanti lapplicazione dellesame rm su pazienti con emolinfopatie [ 1115 ]  . 
 [ 6 ] asserisce che lo studio con rm del rachide lombo - sacrale , in contrasto con le tecniche bioptiche che dimostrano solo la composizione locale del midollo osseo , permette sia una caratterizzazione della composizione del midollo osseo emopoietico che una stima della distribuzione spaziale di acqua e lipidi , consentendo quindi una valutazione globale non invasiva del midollo osseo e for108 radiol med ( 2013 ) 118 : 101111 fig . 
in fact , clinical and laboratory data despite being abnormal in the event of blood and lymph node diseases always need to be complemented with bone marrow aspiration or core biopsy in order to reach a definite diagnosis . 
considering variability in disease site and extension , investigations performed at one site only may often lead to sampling errors in that they fail to provide diagnostic results representative of the entire haematopoietic system [ 16 ]  . 
in addition to establishing the presence of disease , mr imaging can guide a biopsy towards a specific disease site and monitor , in a noninvasive manner , response to treatment through serial examinations . mr imaging and mr spectroscopy of the bone marrow at sites with a greater amount of haematopoietic marrow ( vertebrae and pelvis ) provide fast and noninvasive estimations of the composition of bone marrow and the ratio between red and yellow marrow . 
in effetti , i dati clinici e di laboratorio pur essendo anormali in presenza di emolinfopatia , necessitano sempre dintegrazione mediante ago aspirato o biopsia midollare per giungere a una diagnosi di certezza ; considerando la variabilit in sede ed estensione di malattia , spesso tali indagini condotte effettuate in un solo punto , possono portare ad un errore di campionamento in quanto non consentono di ottenere risultati diagnostici rappresentativi di tutto il sistema ematopoietico [ 16 ]  . 
la rm oltre a stabilire la presenza della patologia , pu condurre in modo appropriato una biopsia verso una specifica localizzazione di malattia midollare e monitorizzare , in maniera non invasiva , la risposta della malattia al trattamento mediante controlli seriati nel tempo . 
 la rm e la spettroscopia con rm del midollo osseo nelle sedi in cui pi abbondante nelladulto il contenuto di midollo osseo emopoietico ( vertebre e bacino ) permette di ottenere in maniera assolutamente non invasiva e in breve tempo una stima della composizione del midollo osseo stesso ed il rapporto midollo rosso / midollo giallo . 
ci reso possibile grazie alle caratteristiche intrinseche della rm ( cio allintensit del segnale rispettivamente in t1 e in t2 ) e soradiol med ( 2013 ) 118 : 101111 frequency of hydrogen ( h ) atoms according to the chemical bonds in which they participate . 
in fact , hypocellular bone marrow ( yellow marrow ) is histologically rich in lipids and low in haematopoietic cells , so that the spectrum will show a high ff due to limited water content . 
conversely , a marrow rich in haematopoietic cells therefore with a high density of stem cells ( red marrow ) will exhibit a spectrum with a low lipid content and a high water peak and therefore with a low ff . 
in haematological cancers ( leukaemias , lymphomas , myelomas ) , the bone marrow is completely replaced by water - rich tumour cells , so the spectrum produced usually has a very low ff . 
after ablative therapy , the cellular component decreases , leaving virtually only a lipid peak , often associated with haemosiderin deposition due to cell death , with resulting magnetic field heterogeneity and major artefacts detrimental to spectral quality [ 18 ]  . 
 in the remaining four patients ( 33% ) , there was a significant increase ( p < 0.05 ) in ff values only at the second mr examination , suggesting a lower immediate efficacy of ablative therapy or incorrect timing of the examination . 
considering all ff recordings also in light of intra and interobserver variability in spectroscopic determinations we saw a significant increase ( p < 0.05 ) in ff values at the second mr examination in 100% of patients studied . on the subject of interand intraobserver variability , some points need to be made . 
in particular , the value of interobserver concordance ( rho - c = 0.950.1 ) is very high , indicating a very high level of agreement between the two observers . 
however , the repeatability coefficient equal prattutto al fenomeno del chemical shift , cio alla diversa frequenza cui risuonano gli atomi didrogeno ( h ) secondo i legami chimici in cui sono incorporati . 
 nello specifico , lo spettro ottenuto in una vertebra composto prevalentemente da una serie di picchi : il primo , situato tra 0 , 8 e 2 , 2 parti per milione ( ppm ) appartiene al segnale dei legami chimici dei gruppi metilene ( - ch2 - ) , a 1 , 2 ppm e metile ( - ch3 ) a 0 , 8 ppm , contenuti nelle catene alifatiche degli acidi grassi saturi ; il secondo situato a 5 , 6 ppm ed generato dai gruppi vinilici ( - ch = ch ) contenuti negli acidi grassi insaturi , infine il segnale dellacqua ( h2o ) situato a 4 , 8 ppil rapporto percentuale tra il segnale totale fornito dai lipidi e quello fornito dallacqua definito ff% e fornisce una stima della composizione del midollo osseo e del rapporto midollo rosso / midollo giallo [ 17 ]  . 
 infatti , un midollo osseo ipocellulare ( midollo giallo ) dal punto di vista istologico ricco in lipidi e povero di elementi cellulari emopoietici , per cui lo spettro mostrer una ff% elevata , per il basso contenuto idrico ; di contro in un midollo ricco in elementi ematopoietici , quindi con unalta densit di cellule staminali ( midollo rosso ) , osserveremo uno spettro con un basso contenuto in lipidi a fronte di un picco dellacqua elevato , quindi con una ff% bassa . 
nelle patologie oncoematologiche ( leucemie , linfomi e mielomi ) il midollo osseo completamente sostituito da elementi neoplastici , ricchi in acqua , pertanto lo spettro ottenuto in questi casi mostra in genere una ff% bassissima ; dopo terapia ablativa diminuisce la componente cellulare per cui abbiamo quasi solo il picco dei lipidi , cui spesso si associa la deposizione di emosiderina , dovuta alla morte degli elementi cellulari , con conseguente disomogeneit del campo magnetico , che pu provocare notevoli artefatti alla qualit dello spettro ottenuto [ 18 ]  . 
nei rimanenti 4 pazienti ( 33% ) , si osservato un incremento statisticamente significativo ( p < 0 , 05 ) dei valori di ff% solo nel secondo follow - up , suggestivo per una minore efficacia immediata della terapia ablativa o per un timing non corretto nellesecuzione dellesame . 
considerando le rilevazioni di ff% nel complesso , anche alla luce della variabilit intra ed inter osservatore nelle misure spettroscopiche , si rilevato un incremento significativo ( p < 0 , 05 ) di ff% nel secondo follow - up nel 100% dei pazienti studiati . per quanto concerne la variabilit intered intra - operatore , sono dobbligo alcune precisazioni . 
in particolare il valore di concordanza inter - osservatore rilevato ( rho - c = 0 , 950 , 1 ) molto elevato , indicando che mediamente i due osservatori esiste un elevato di grado di concordanza nelle rilevazioni . 
this value should not be confused with the repeatability rate , as it indicates the values beyond which the differences between the two observers determinations cannot be attributed to chance . 
instead , it might be interesting to investigate the repeatability of the determinations of the system for mr spectroscopic analysis in order to quantify the absolute errors on the single determinations provided by the machine . correlating ff values with cell types normally present in the full blood count , we found a significant correlation between ff and platelet count . 
this finding suggests that the number of circulating platelets after bmt provides the most accurate estimation of recovery of haematopoietic activity within the marrow or , in other words , of the efficacy of the bmt . 
on patients affected by beta - thalassaemia treated with stem cell transplantation , which demonstrated that assessing the percentage of the area of red marrow in the proximal femur may be useful to predict the outcome of treatment and may be used as an additional predictive factor [ 19 ]  . 
 in conclusion , although our study lacked adequate statistical power due to the small population , it indicated that mr spectroscopy of the bone marrow in nhl patients treated with autologous stem cell transplantation is a noninvasive modality that is highly sensitive for characterising and monitoring bone marrow following transplantation . 
 pari al doppio della deviazione standard delle medie delle differenze tra le rilevazioni dei due osservatori , assume un valore quasi critico ( 24 , 2% = 8 , 4% )  . 
questo valore non va confuso con la percentuale di ripetibilit , in quanto indica il valore oltre il quale le differenze tra le rilevazioni dei due osservatori non possono essere attribuite al caso ed espresso in percentuale poich in questo studio stata quantificata la percentuale di grassi liberi . 
relativamente alla variabilit intra - osservatore , dallanalisi dei grafici e dai valori estrapolati , possiamo osservare che il secondo osservatore pur fornendo risultati pi consistenti , ovvero con una media delle differenze tra le rilevazioni appaiate , minore rispetto al primo osservatore , nel complesso ha limiti di accordo sovrapponibili e si pu per tanto escludere la presenza di un bias dovuto alla differente esperienza tra gli osservatori . 
invece potrebbe essere interessante indagare la ripetibilit delle rilevazioni del sistema di analisi spettroscopica rm in modo da poter quantificare in maniera precisa gli errori assoluti sulle singole rilevazioni della macchina . correlando i valori di ff% con gli elementi cellulari presenti normalmente nellemocromo abbiamo ottenuto una correlazione statisticamente significativa tra i valori di ff% e il numero delle piastrine in circolo . 
tale rilievo ci permette di ipotizzare che il numero delle piastrine in circolo dopo tmo il parametro che ci d una migliore stima della reale ripresa di attivit ematopoietica midollare , cio dellefficacia del tmo . 
 poich nella routine clinica i parametri utili a stabilire i tempi di attecchimento emopoietico dopo tmo , sono il numero dei globuli bianchi e delle piastrine in circolo , tale correlazione pu permetterci di ipotizzare per la spettroscopia con rm un ruolo sia di monitoraggio dellefficacia del tmo , sia di conferma della scarsa o nulla attivit midollare residua . 
 [ 19 ] su pazienti affetti da beta - talassemia trattati con trapianto di cellule staminali , che ha dimostrato come la valutazione della percentuale della quantit di midollo rosso della porzione prossimale del femore pu essere un utile parametro per prevedere la riuscita del trapianto e pu essere utilizzato come un fattore predittivo addizionale [ 19 ]  . 
 [ 7 ] avevano fallito nel dimostrare che lespansione dei progenitori ematopoietici nel midollo osseo monitorizzata mediante rm spettroscopica correlava con i livelli di progenitori mobilizzati in circolo [ 16 ]  . 
 in conclusione , il nostro studio , pur richiedendo conferme pi ampie poich realizzato su una coorte relativamente piccola per fornire unadeguata importanza statistica , ha indicato la rm con studio spettroscopico del midollo osseo in pazienti con lnh sottoposti a trapianto autologo di cellule staminali , come una metodica non invasiva e molto sensibile nella caratterizzazione e monitoraggio del midollo osseo dopo trapianto . 
knauth springer - verlag berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 642 - 17871 - 9 eisbn : 978 - 3 - 642 - 17872 - 6 published online : 16 march 2013 springer - verlag 2013 acute appendicitis , according to statistics , represents a lifetime risk estimated at about 7% in females and 9% in males . 
 according to clinical and historical data , diagnosis should be easy and straightforward ( crampy abdominal pain at the umbilicus , vomiting and migration of pain to the right iliac fossa ) indicating surgical removal ( appendectomy is the most frequently performed emergency surgical procedure )  . 
this dichotomy between clinical signs and negative / positive end results has prompted wide and spread discussion among clinicians and surgeons about the proper and definitive signs leading to correct diagnosis . 
on the one side ( the dangerous side ) misdiagnoses are followed by perforation , abscess , phlegmon , peritonitis and possible demise ; on the other ( the quiet ) to unnecessary appendectomies , skipping the proper diagnosis of right lower quadrant ( rlq ) pain very often due to gynaecological problems or lower intestinal diseases . the aim of this very beautiful book is to present all possible information about appendicitis in all its facets , both in adults and children , describing in depth : clinical , laboratory , pathology and imaging data in order to offer clinicians , surgeons and emergency departments staff members a proper and updated guide to rlq problems . 
 there is a much ado about which is the best imaging modality to be employed in order to reach proper diagnosis : ultrasound ( us , number one modality in children ) ? , computed tomography ( ct ) when us is doubtful ? , ct alone or lappendicite acuta , secondo le statistiche , rappresenta una fonte di rischio durante la vita per circa il 7% delle femmine ed il 9% nei maschi , presentando un picco nei bambini e nei giovani adulti che poi si riduce con let . secondo i dati clinici e storici , la diagnosi di appendicite dovrebbe essere facile e senza problemi ( dolori addominali crampiformi allombelico , vomito e migrazione del dolore alla fossa iliaca destra ) , avendo come conseguenza la rimozione chirurgica ( lappendicectomia rappresenta lintervento chirurgico durgenza pi frequente )  . 
questa dicotomia tra i segni clinici ed i risultati finali positivi o negativi stata fonte di discussioni ampie e diffuse tra i clinici ed i chirurghi su quali siano i segni certi e definitivi che indirizzano alla diagnosi corretta . 
da un lato infatti ( quello pericoloso ) , le diagnosi non corrette hanno come conseguenza perforazioni , ascessi , peritoniti ed anche morte ; dallaltro ( il tranquillo ) , appendicectomie inutili , che non tengono conto di quella che dovrebbe essere la diagnosi corretta dei dolori al basso fianco destro , assai spesso aventi invece come causa problemi ginecologici o malattie dellintestino tenue distale . scopo fondamentale di questo libro molto bello di fornire al lettore ogni possibile informazione sullappendicite in tutte le sue possibili sfaccettature , sia nelladulto che nel bambino , descrivendo in dettaglio i dati clinici , di laboratorio , anatomopatologici e per immagini , in modo tale da offrire a clinici , chirurghi e personale dei reparti di emergenza una guida adeguata e ben aggiornata circa i problemi del quadrante inferiore addominale destro . 
 grande enfasi e discussione posta su quale sia la miglior modalit di immagine da utilizzare per giungere alla diagnosi corretta : ecografia ( modalit diagnostica numero uno nei bambini ) ; tomografia computerizzata ( tc ) , quando radiol med ( 2013 ) 118 : 704705 coupled with contrast media ? , magnetic resonance imaging ( mri ) ( this is a luxury even if its multiplanar evaluation of the abdomen , without radiation is a bonus most of all in children and pregnant women ) ?  . 
rotondo2 1dipartimento di odontoiatria , facolt di medicina e chirurgia , seconda universit di napoli , via de crecchio 6 , 80131 napoli , italy 2 sezione scientifica di radiologia , unit di radiologia , radioterapia , dipartimento di internistica clinica e sperimentale f . 
iaselli , corso trieste 273 , 81100 caserta , italy , tel . : + 39 - 333 - 8411634 , fax : + 39 - 0823443679 , e - mail : francescoiaselli@hotmail.it received : 26 october 2011 / accepted : 20 february 2012 / published online : 29 november 2012 springer - verlag 2012 abstract purpose . 
by comparing the values obtained in the two series , we calculated the degree of significance of each difference between children with osahs and controls using the student t test . 
differences of only 5 / 27 linear and angular indices considered were not statistically significant between groups , thus confirming susceptibility to the disorder in relation to certain splanchnocranic morphovolumetric features . 
dal confronto dei valori ottenuti nelle due serie abbiamo infine calcolato attraverso il test t di student il grado di significativit della differenza tra i bambini affetti da osahs ed i controlli . 
le differenze di solo cinque dei ventisette indici lineari ed angolari valutati non sono risultate statisticamente significative tra i due gruppi , confermando la predisposizione al disturbo determinata da un particolare assetto dello splancnocranio . 
despite the limitations associated with the 2d nature of conventional cephalometry , mainly related to projection and identification errors , and despite the upright position during examination , we consider the diagnostic value and information content of this technique high , thus reaffirming its role as a first - line imaging investigation in children with sleep - related breathing disorders . keywords osahs craniofacial skull cephalometry mandibolare e la distanza tra la sella e losso ioide , indice affidabile della posizione verticale di questultimo . 
nonostante i limiti legati alla natura bidimensionale dellindagine cefalometrica convenzionale , principalmente correlati agli errori di proiezione e di identificazione , e nonostante lesecuzione dellesame in posizione eretta , consideriamo elevato il valore diagnostico dellindagine ed il suo contenuto informativo , riaffermando cos il suo ruolo di indagine di imaging prima istanza nei bambini con disturbi del respiro legati al sonno . parole chiave osahs scheletro craniofacciale cefalometria introduction introduzione obstructive sleep apnoeahypopnoea syndrome ( osahs ) is a common disorder of childhood characterised by repeated episodes of upper airway obstruction during sleep , resulting in sleep fragmentation and daytime sleepiness . 
if not promptly and adequately treated , the syndrome can lead to neurodevelopmental disorders , learning defects , growth retardation , pulmonary hypertension and other severe cardiorespiratory sequelae [ 13 ]  . 
soft tissue changes leading to a reduction in the calibre of the upper airway ( mainly related lymphatic adenotonsillar tissue hyperplasia ) and hypotonia of muscles that normally maintain patency of that tissue are the main factors implicated in the onset of the disorder in childhood [ 4 ]  . 
in recent decades , however , several authors have suggested that the cause of osahs in children , as in adults , may be due to changes in morphovolumetric features of the craniofacial skull . 
therefore , shape , size , or simply position of a craniofacial bone structure can lead to a narrower airway either indirectly by modifying the normal insertion points of upper respiratory muscles and impairing muscle function , or directly by bone structures constituting incompressible limits of both nasal fossae and pharynx [ 3 , 59 ]  . 
in order to evaluate morphovolumetric features of the craniofacial skeleton in children with osahs , cephalometric teleradiography was introduced to this field and is no preferred as the initial approach in paediatric patients because of its low cost , wide availability and speed over computed tomography ( ct ) and magnetic resonance imaging ( mri ) , even though the latter are more exhaustive due to higher spatial ( multiplanar and 3d rendering ) and contrast resolution ( excellent visualisation of soft tissue ) [ 10 ]  . 
we compared teleradiography studies obtained in a series of osahs children with those of healthy la sindrome delle apnee - ipopnee ostruttive nel sonno ( osahs ) un frequente disturbo dellet pediatrica caratterizzato da ripetuti episodi di chiusura delle vie aeree superiori durante il sonno , con conseguente sua frammentazione e sonnolenza diurna . 
se non tempestivamente ed adeguatamente trattata , la sindrome pu portare a disturbi neurocomportamentali , difetti di apprendimento , ritardo della crescita , ipertensione polmonare e altre sequele cardiorespiratorie severe [ 13 ]  . 
alterazioni dei tessuti molli determinanti riduzione del calibro delle vie aeree superiori ( principalmente iperplasia del tessuto linfatico adenotonsillare ) e perdita del tono dei muscoli che mantengono normalmente beante il lume di queste ultime sono i fattori maggiormente indicati in letteratura nella comparsa del disturbo in et pediatrica [ 4 ]  . 
nelle ultime decadi , poi , diversi autori hanno ipotizzato che alla base della osahs nel bambino come nelladulto possano esserci alterazioni morfovolumetriche dello scheletro craniofacciale che costituirebbero di fatto la causa iniziale del ridotto calibro delle vie aeree su cui solo in un secondo momento verrebbero ad inserirsi alterazioni a carico dei tessuti molli e , quindi , linsufficienza neuromuscolare . 
in particolare , la conformazione , le dimensioni o semplicemente la posizione di una struttura ossea possono determinare un restringimento del lume aereo indirettamente , attraverso la modificazione dei normali punti di inserzione dei muscoli delle prime vie e la conseguente compromissione della loro funzione , o direttamente , costituendo le stesse strutture ossee limiti anatomici non compressibili della cavit nasale e del faringe [ 3 , 59 ]  . 
proprio per valutare le caratteristiche morfovolumetriche dello scheletro craniofacciale nei pazienti affetti da osahs , anche in tale ambito impiegata la teleradiografia cefalometrica , indagine che per le sue caratteristiche di basso costo , ampia disponibilit sul territorio e rapidit di 650 radiol med ( 2013 ) 118 : 648659 children to evaluate differences between morphovolumetric features and identify changes in shape and , in particular , size and position of the craniofacial bones potentially associated with the disorder . 
we also obtained prognostic and therapeutic indications on the basis of data in the literature . materials and methods forty children with osahs ( 20 boys , 20 girls ; age range , 414 years ; mean age , 8.95 years ) underwent cephalometric evaluation from june 2009 to september 2011 . 
diagnosis was made at the sleep centre of the infantile neuropsychiatry department of our university hospital on the basis of accurate clinical assessment and medical history , sleep questionnaire compiled by parents and polysomnography . 
 the 40 patients not affected by osahs or any other type of breathing disorder ( mouth breathing , snoring , etc . ) ( 20 boys , 20 girls ; age range , 515 years ; mean age , 9.4 years ) were selected from a sample of 300 patients who underwent teleradiography at our department of diagnostic imaging between 2008 and 2011 for clinical problems not related to osahs . 
in selecting controls , we only considered the need to create a series as similar as possible in terms of male : female ratio and age to that of the osahs group ; otherwise , the choice was made quite randomly . 
cephalometric examinations were acquired with a sirona ortophos xg 5 ( sirona dental system gmbh , bensheim , germany ) system with study participants holding their breath after a slight forced expiration , 10 s after a voluntary swallow requested by the technician ( this is aimed at enabling the return of the tongue and jaw to a neutral position at the time of image acquisition )  . 
all examinations were performed in the upright position ( on the basis of previous evidence of there being no difference between results of examinations performed in the supine and upright positions ) [ 10 ] , with the frankfurt plane parallel to the floor and the lips relaxed . 
 all cephalograms were obtained with constant physical and technical parameters ( 71 kvp ; 10 mas ; te 0.8 s ; focal length , 165 cm ; distance from the midline of the head to the cassette , 14 cm ) and were imported into a software programme for image postprocessing ( vital , vitrea , mn , united states )  . 
nel nostro studio gli esami di teleradiografia di una serie di bambini affetti da osahs sono stati confrontati con quelli di bambini sani al fine di valutare le differenze tra le caratteristiche morfovolumetriche tra le due serie e di identificare alterazioni di conformazione e , soprattutto , di dimensione e posizione delle ossa dello splancnocranio associate al disturbo con conseguente possibilit di trarre indicazioni prognostiche e terapeutiche sulla scorta delle evidenze presenti in letteratura . materiali e metodi nel gruppo dei 40 pazienti affetti da osahs ( 20 maschi , 20 femmine , et compresa tra 4 e 14 anni , et media di 8 , 95 anni ) ammessi alla valutazione cefalometrica da giugno 2009 a settembre 2011 la diagnosi era stata posta median te valutazione clinico - anamnestica approfondita , questionario sul sonno compilato dai genitori ed esame polison nografico presso il centro del sonno dellambulatorio di neuropsichiatria infantile della nostra universit . 
 i 40 pazienti non affetti n da osahs n da qualsiasi altro tipo di disturbo del respiro ( respirazione orale , abitudine al russare , ecc . ; 20 maschi , 20 femmine , et compresa tra 5 e 15 anni , et media 9 , 4 anni ) sono stati selezionati a partire da un campione di circa 300 pazienti valutati mediante teleradiografia per problematiche cliniche diverse dalla osahs dal 2008 al 2012 presso il nostro dipartimento di diagnostica per immagini . 
nella scelta dei pazienti abbiamo tenuto conto esclusivamente della necessit di creare un campione quanto pi simile possibile a quello dei soggetti affetti da osahs in termini di rapporto maschio : femmina e di et ; per il resto la scelta stata del tutto casuale . 
gli esami cefalometrici sono stati acquisiti a respiro bloccato dopo una leggera espirazione forzata dieci secondi dopo una deglutizione volontaria richiesta dal tecnico ( questultima manovra ha il fine di consentire il ritorno della lingua e della mandibola in posizione neutra al momento dellacquisizione ) con apparecchio sirona ortophos xg 5 ( sirona dental systeme gmbh , bensheim , germania )  . 
gli esami ar cond pog c3ai ans pns cond pog radiol med ( 2013 ) 118 : 648659 table 1 craniometric landmarks considered in our study : from the following 16 landmarks 27 linear and angular indices were derived abbreviation definition craniometric landmark articulare basion condylar gnathion gonion hyoid iodide menton nasion pogonion subspinale supramental sella turcica antero - inferior edge of c3 anterior nasal spine posterior nasal spine the intersection of the posterior border of the condylar process and the inferior border of the basilar part of the occipital bone the median point of the anterior margin of the foramen magnum the most anterior point of the mandibular condyle the most anteroinferior point on the symphysis of the chin the point at the intersection of the mandibular ramus and the mandibular plane the most cranially located point on the hyoid bone the most anterior point of the body of the hyoid bone the most posterior point of the mandibular symphysis the most anterior point of the frontonasal suture on the midline the most anteriorly located point on the symphysis of the chin the deepest midline concavity on the anterior maxilla the deepest midline concavity on the mandibular symphysis the midpoint of the pituitary fossa the most inferoanterior point of the body of the third cervical vertebra the tip of the bony anterior nasal spine the tip of the bony posterior nasal spine tabella 1 punti craniometrici considerati nel nostro studio . 
the distance from the hyoid bone to the mandibular plane is expressed as the ratio of the distance between the mandibular plane and hy , with the measurement taken perpendicular to the mandibular plane , and the length of the mandibular plane itself fig . 
for each index , we calculated mean , standard deviation ( sd ) , standard error ( se ) and t value ( the latter two are not shown in the results table )  . 
 we excluded overweight or obese children to minimise bias related to the negative effect of excess weight on respiratory performance described by several authors in both paediatric and adult patients [ 13 ]  . 
per ciascun indice abbiamo calcolato la media , la deviazione standard , lerrore standard ed il valore del t ( questi ultimi due indici non compaiono nella tabella dei risultati )  . 
il grado di significativit delle differenze ottenute per ciascun risultato stato definito attraverso il test t di student : valori di p > 0 , 05 , < 0 , 05 , < 0 , 01 e < 0 , 001 sono stati considerate rispettivamente indicative di differenze non significative , scarsamente significative , probabilmente significative ed altamente significative . 
 dallo studio sono stati esclusi bambini in sovrappeso o obesi , al fine di ridurre quanto pi possibile il bias legato alleffetto negativo delleccedenza ponderale sulla performance respiratoria anche di soggetti pediatrici descritto da diversi autori [ 13 ]  . 
abbiamo inoltre escluso bambini affetti da sindromi di cui nota lassociazione con alterazioni dello scheletro craniofacciale e da malattie sistemiche o portatori di deformit delle ossa dello splancnocranio su base congenita e / o traumatica immediatamente apprezzabili allesame obiettivo . 
whole anterior facial height and height of the lower half of the anterior face were greater in the osahs group than in controls ( both results were statistically significant )  . 
lerrore interosservatore calcolato nel nostro studio risultato accettabile e i valori del coefficiente di affidabilit di houston hanno indicato unelevata correlazione tra le variabili misurate dai due team , con valori compresi tra 0 , 96 e 0 , 85 . 
laltezza totale anteriore del volto e laltezza della met inferiore del volto sono maggiori nei soggetti affetti da osahs che nei controlli ( entrambi i dati sono significativi dal punto di vista statistico )  . 
despite the low standard deviation values , we found no significant differences in the inclination of the palatal plane , thus of the upper jaw , in the sagittal plane . 
the hyoid bone was displaced inferiorly and anteriorly in children with osahs : this is shown by the highly significant difference of the index hy s , the significant differences of the indices h palatal plane , h c3ai and relative distance of the hyoid bone and the only probably significant differences of indices h posterior pharyngeal wall and gn go h . 
however , regarding the position of each maxillary bone in the sagittal plane , in the osahs group , we found only a probably significant difference ( due to high sd values ) in maxilla position and a significant difference in mandible position in both cases in the sense of retroposition . 
 comparative evaluation of indices related to nasopharyngeal depth ( ar go gn , ba s pns , mpas ) showed a moderate - to - high difference between groups , with lower values in children with osahs , indicating compression of the airways in the anteroposterior direction . 
finally , there was a significant difference between groups in the cranial base angle and a probably significant difference in the length of the whole basicranium and its anterior and posterior arms , with lower values in the osahs group in all cases . 
the statistical value of differences in index n s , anterior arm of the cranial base , in particular , was limited by the high sd value . discussion the association of nocturnal enuresis in children with sleeprelated breathing disorders with a dolichocephalic pattern identified by the cephalic index was demonstrated by carotenuto et al . 
in the study reported here , measurement of several indices referring to anterior and posterior height and depth of the face also show that children with osahs have , compared with controls , a longer face , with a tendency to dolichocephaly and a prevalent increase in lower anterior facial height . 
both jaws were smaller in the osahs group , particularly the mandible , which , moreover , had a significantly modified degree of inclination in the sagittal plane , allo sviluppo in profondit della mandibola sono differenti tra le due serie , con valori numerici maggiori nei controlli e con grado di significativit intermedio , nonostante gli alti valori di deviazione standard . 
losso ioide dislocato inferiormente ed anteriormente nei bambini affetti da osahs : lo testimoniano la differenza altamente significativa dellindice hy - s , le differenze significative degli indici h - piano palatale e h - c3ai e della distanza relativa dellosso ioide e le differenze solo probabilmente significative degli indici h - parete posteriore del faringe e gn - go - h . 
 per quanto riguarda , invece , la posizione assoluta di entrambe le ossa nel piano sagittale , nel gruppo con osahs abbiamo registrato una differenza solo probabilmente significativa ( a causa degli alti valori di deviazione standard ) della posizione del mascellare superiore e significativa della mandibola , in tutti e due i casi nel senso della retroposizione . 
la valutazione comparativa degli indici riferiti allestensione in profondit del complesso rinofaringeo ( ar - go - gn , ba - s - snp , sapm ) ha evidenziato una differenza di grado medio - alto tra i due gruppi , con valori numerici inferiori nei bambini affetti da osahs , ad indicare compressione delle vie aeree lungo un vettore antero - posteriore . 
infine , tra i due gruppi emersa una differenza significativa riguardo lampiezza dellangolo della base cranica e differenze solo probabilmente significative riguardo la lunghezza complessiva del basicranio e quelle del suo braccio anteriore e posteriore , con valori numerici in tutti i casi inferiori nel gruppo osahs . 
la significativit della differenza a carico dellindice n - s , braccio anteriore della base cranica , in particolare , stata limitata dallelevato valore di devizione standard . discussione lassociazione dellenuresi notturna con un pattern dolicocefalico identificato attraverso il calcolo dellindice cefalico nei bambini con disturbi del respiro correlati al sonno stata dimostrata da carotenuto et al . 
anche in questo lavoro , dal calcolo di diversi indici riferiti alle altezze anteriore e posteriore del volto ed alla sua profondit , emerso che i bambini affetti da osahs presentano , rispetto ai controlli , un volto allungato , con tendenza alla dolicocefalia , con prevalente incremento dello sviluppo in altezza della met inferiore del volto anteriormente , reperto questultimo da inquadrare nelle modificazioni dello scheletro craniofacciale secondarie allostacolato flusso 656 radiol med ( 2013 ) 118 : 648659 aereo attraverso il naso ed alla necessit di ottimizzare la respirazione orale ( ad esempio ogivalizzazione del palato duro , spostamento in senso dorso - caudale della mandibola con conseguente caudalizzazione del me ) [ 6 , 7 , 1521 ]  . 
 la riduzione del piano mandibolare registrata nel gruppo osahs , inoltre , si associa generalmente alla retrusione della lingua ed allarretramento del punto dinserzione del muscolo genioglosso ( che si inserisce in corrispondenza del go ) con conseguente riduzione dellazione protrusiva di questultimo e riduzione dello sapm [ 2 , 8 ]  . 
 oltre al sicuo ruolo di fattori genetici , nella definizione del pattern micrognatico nei bambini affetti da osahs ha senza dubbio avuto un peso fondamentale la componente ambientale , in particolare legata alla variazione delle abitudini alimentari verificatasi a seguito della rivoluzione industriale , con prevalenza del consumo di alimenti a bassa consistenza ( macinati , tritati , cotti , ecc . ) e conseguente ridotto carico sulle strutture ossee , dentarie e muscoli dellapparato masticatorio , avviatosi cos ad un percorso di progressiva involuzione [ 22 ]  . 
nel gruppo osahs da noi considerato variata anche la posizione delle ossa mascellari sul piano sagittale : entrambe sono arretrate ( come testimoniato dal valore inferiore degli angoli s - n - a e s - n - b , con valore medio diagnostico per retrognatia ) , senza dubbio anche per la loro riduzione dimensionale , ma soprattutto per la necessit di restringere le vie aeree superiori di fronte allaumento della concentrazione degli allergeni e degli inquinanti ambientali verificatosi con andamento esponenziale negli ultimi trecento - quattrocento anni nei paesi occidentali [ 23 ]  . 
lo spostamento combinato in senso posteriore di entrambe le ossa mascellari nel gruppo osahs da noi valutato , inoltre , non ha determinato variazioni significative dellindice anb rispetto ai controlli , dunque a significative variazioni del rapporto molare . 
la gi menzionata minore estensione in profondit dellosso mascellare superiore nel gruppo osahs ( variazione solo probabilmente significativa , principalmente a causa degli elevati valori di deviazione standard in entrambi i gruppi ) rientra nellambito della compressione in senso antero - posteriore del volto , strettamente correlata alla riduzione del braccio anteriore del basicranio , segmento anatomicamente e funzionalmente intimamente correlato al mascellare superiore ; non abbiafig . 
this cephalogram well depicts the steep appearance of the mandibular plane widely described in connection with osahs and with the high - angle facial pattern and the low position of the hyoid bone ( arrow ) fig . 
the lower value of mandibular plane length found in the osahs group , moreover , is associated with tongue retrusion and back displacement of the insertion point of the genioglossus ( which inserts near to the go ) with consequent reduced protrusive action of the latter and reduced mpas [ 2 , 8 ]  . 
 this is particularly related to dietary changes since the industrial revolution , with prevalent consumption of lowconsistency foods ( minced , chopped , cooked , etc . ) and consequent decreased load over the bony , dental and muscular structures of the masticatory apparatus , thus encouraging a tendency to its progressive involution [ 22 ]  . 
jaw position in the sagittal plane in the osahs group in our study had changed , being back displaced ( as displayed by the lower values of angles s n a and s n b , with mean value diagnostic for retrognathia ) , in part due to a reduction in size but also due to the necessity for upper airway narrowing because of increased allergen concentrations and environmental pollutants , which occurred at an exponential rate over the last 300 to 400 years in western countries [ 23 ]  . several literature reports address the beneficial effects radiol med ( 2013 ) 118 : 648659 of maxillomandibular advancement in cases of severe retrognathia previously unsuccessfully treated by adenotonsillectomy . 
the combined back displacement of both maxillary bones in the osahs group did not result in significant changes in the anb index , and therefore in molar ratio , compared with controls . 
the abovementioned lower maxillary depth in the osahs group ( only probably significant difference , mainly due to the high sd values in both groups ) is part of the anteroposterior compression of the face and is related to the decrease in the front arm of the skull base , anatomically and functionally bound to the maxilla . 
 in addition to these differences in linear indices of the cranial base between groups , a very interesting result in our study was the significant difference in the value of the cranial base angle , with a lower value in the osahs group . 
 most craniometric studies in the literature describe the cranial base angle as a remarkably stable index from individual to individual , such that it is frequently used as a marker of genetic or racial affinity . 
greater flexion of the cranial base angle ( statistically significant , especially for the low sd values in both groups ) is further evidence of anteroposterior compression of the face and airways . 
this was also demonstrated by the lower value of angle ba s snp in the osahs group , an index related to the minimum retropalatal area measured with ct and mri , representing the bony boundaries of the nasopharynx ( statistically significant )  . 
reduced angular indices n s ba and ba s snp found in our study is described in several previous studies as a cause of obstruction due to alteration of the normal insertion points of the pharynx dilator muscles . 
 furthermore , this finding is associated by several authors with a poor response to adenotonsillectomy [ 7 , 2931 ]  . a direct indicator of obstruction , well assessed with teleradiography , is the mpas : a favourable contrast situation allows identification and measurement of the air column between the base of the tongue and the back wall of the pharynx . 
results provide an indication of the depth of the minimum retroglossal space ( the definition of which using teleradiography is no doubt limited by the upright position and wakefulness , thus being significantly less accurate than results obtained with axial ct or mri ) and allow implementation of the information content of the technique . 
 finally , a considerable difference was found in the position of the hyoid bone between groups : comparison of indices evidenced a ventrocaudal displacement of the bone , an alteration reported in the majority of previous studies of similar design , with the hyoid bone at the level of the c4c6 vertebrae rather than c3c4 , as normal [ 10 , 2224 ]  . 
 oltre alle differenze appena menzionate degli indici lineari riferiti alla base cranica tra i due gruppi , un risultato davvero interessante nel nostro studio si rivelato la differenza significativa del valore dellangolo della base cranica , con valore significativamente pi basso nel gruppo osahs . 
la maggior parte degli studi craniometrici in letteratura descrivono langolo della base cranica come un indice straordinariamente stabile da soggetto a soggetto , tanto da essere frequentemente impiegato come marcatore di affinit genetica o razziale tra diversi individui . 
il risultato ottenuto nel gruppo osahs , una maggiore flessione dellangolo della base cranica significativa dal punto di vista statistico , soprattutto in virt di bassi valori di deviazione standard in entrambi i gruppi in esame , unulteriore dimostrazione di una compressione in senso antero - posteriore del volto e delle vie aeree , anche testimoniata dal valore significativamente inferiore dellangolo ba - s - snp , indice questultimo correlato allarea minima retropalatale misurata in tc e rm ed espressione dei limiti ossei del rinofaringe . 
la riduzione degli indici angolari n - s - ba e ba - s - snp da noi registrata stata descritta in diversi studi in letteratura come causa di ostruzione per alterazione dei normali punti di inserzione dei muscoli dilatatori del faringe ; inoltre anche tale riscontro stato posto da diversi autori in relazione con il fallimento dellapproccio chirurgico mediante adenotonsillectomia [ 7 , 2931 ]  . 
 indice diretto di ostruzione ben valutabile alla teleradiografia lo sapm : una situazione favorevole di contrasto permette di identificare e misurare la colonna aerea compresa tra la base della lingua e la parete posteriore del faringe , ottenendo cos un indicazione sullarea retroglossa minima ( la cui definizione indubbiamente limitata dalla posizione eretta e dallo stato di sveglia e sensibilmente meno accurata rispetto a quella ottenuta con limaging assiale mediante tc ed rm ) ed implementando il contenuto informativo dellesame . 
 considerevole , in ultimo , si rivelata la differenza nella posizione dellosso ioide tra i due gruppi : il confronto degli indici ad essa riferiti ha evidenziato uno spostamento in senso ventro - caudale dellosso stesso , alterazione riscontrata nella maggior parte degli studi in letteratura con un disegno simile al nostro , con osso ioide a livello delle vertebre c4 - c6 piuttosto che c3 - c4 come normale [ 10 , 22 24 ]  . 
 [ 5 ] , riscontrando un analogo spostamento in senso ventrocaudale dellosso in soggetti pediatrici affetti da disturbi del respiro durante il sonno , hanno attribuito la componente di spostamento anteriore alle ripetute iperestensioni del capo mirate ad ottimizzare la respirazione orale , quella caudale ad unalterata funzione del muscolo genioglosso , probabilmente da correlare allo spostamento posteriore del suo punto di inserzione 658 radiol med ( 2013 ) 118 : 648659 nent of the displacement to the repeated head extensions of children aimed at optimising oral breathing and the caudal component to impaired genioglossus muscle function , correlated with posterior displacement of its insertion on the mandible caused by the abovementioned micrognathia and retrognathia [ 4 , 5 , 22 , 24 , 32 , 33 ]  . 
 as did several previous authors , we overcame the limitation of older cephalometry for measuring the vertical position of the hyoid bone in relation to the mandibular plane only ( no significant variation in our study )  . 
we decided to use two linear indices derived from connection of the hyoid bone with more stable , and therefore more reliable , craniometric landmarks ( sella turcica and palatal plane , with the distance between the hyoid bone and the palatal plane being a reliable index of the length of the upper airway , linearly related to the risk ; and the frequency and severity of the obstruction , which was significantly greater in the osahs group ) [ 9 , 28 , 32 ]  . 
the value of the distance between hyoid bone and mandibular plane in our study , however , actually turned out to be significant only in relation to the distance to go gn , with a significant difference between groups . 
 the position of the hyoid bone is in close relationship with airways calibre in children and adults with osahs , particularly with the retroglossal area ( several muscles of the tongue and the floor of the mouth inserting on the hyoid bone are affected by this positional change ) [ 14 , 29 ]  . 
an excessively ventrocaudal position of the hyoid bone in children with osahs , moreover , was described in association with therapeutic failure of adenotonsillectomy , just as in adults with osahs it is associated with failure of uvulopharyngoplasty [ 2 , 12 , 30 , 33 ]  . conclusions only five of 27 linear and angular indices were not statistically significantly different between children with osahs and controls , confirming a predisposition to the disorder created by the presence of specific craniofacial features . 
 the most statistically significant differences were mandibular plane inclination , typically steep in the osahs group ; the ar go - gn , consequently increased in the same group ; and the distance between sella and hyoid bone , which is a reliable index of the vertical location of the latter . 
despite the limitations related to the 2d nature of the conventional cephalometric investigation , mainly consisting of projection and identification errors and upright imaging , we consider the diagnostic value of the examination and its information content to be high , thus reaffirming its role as the firstchoice radiological investigation in children with sleep - related breathing disorders . mandibolare causato dalla micrognatia e dalla retrognatia sopra menzionate [ 4 , 5 , 22 , 24 , 32 , 33 ]  . 
 come diversi autori in passato , abbiamo superato il limite della vecchia cefalometria di considerare la posizione verticale dellosso ioide esclusivamente rispetto al piano mandibolare ( variazione non significativa nel nostro studio ) ; abbiamo piuttosto scelto di impiegare altri due indici lineari ricavati dallunione dellosso ioide stesso con riferimenti craniometrici pi fissi , quindi pi affidabili ( sella turcica e piano palatale , con la distanza osso ioide - piano palatale affidabile indice della lunghezza della via aerea , parametro correlato in maniera lineare al rischio , alla frequenza ed alla severit delle ostruzioni , significativamente maggiore nel gruppo osahs ) [ 9 , 28 , 32 ]  . 
il valore della distanza dellosso ioide dal piano mandibolare nel nostro studio , invece , si rivelata effettivamente significativa solo in rapporto con la distanza go - gn , con differenza significativa tra i due gruppi . 
la posizione dellosso ioide stata posta in stretta relazione con il calibro delle vie aeree nei soggetti pediatrici ed adulti affetti da osahs , in particolare con larea retroglossa ( diversi muscoli della lingua e del pavimento della bocca inserendosi sullosso ioide risentono di variazioni della sua posizione ) [ 14 , 29 ] ; inoltre nelle diverse fasce di et si confermata lassociazione di tale reperto con la frequenza e la severit delle ostruzioni [ 25 , 28 ]  . 
una posizione eccessivamente bassa e ventrale dellosso ioide in bambini affetti da osahs , inoltre , stata descritta in associazione con il fallimento terapeutico delladenotonsillectomia cosiccome nelladulto con osahs tale reperto associato ad un fallimento delluvulofaringoplastica [ 2 , 12 , 30 , 33 ]  . conclusioni le differenze di solo cinque sul totale dei ventisette indici lineari ed angolari sono risultate non significative tra il gruppo dei bambini affetti da osahs ed i controlli , ad indicare la certa predisposizione alla comparsa del disturbo creata dalla presenza di specifiche caratteristiche craniofacciali . 
 le differenze pi significative dal punto di vista statistico hanno riguardato linclinazione del piano mandibolare , caratteristicamente ripido nel gruppo osahs , langolo argo - gn , di conseguenza maggiore nello stesso gruppo , e la distanza dalla sella allosso ioide , indice affidabile della localizzazione caudale di questultimo . 
this study was undertaken to evaluate the feasibility , safety and efficacy of a new combined singlestep therapy in patients with unresectable multinodular unilobar hepatocellular carcinoma ( hcc ) , with at least one lesion > 3 cm , with balloon - occluded radiofrequency ablation ( bo - rfa ) plus transcatheter arterial chemoembolization ( tace ) of the main lesion and tace of the other lesions . 
ten consecutive patients with multinodular ( two to six nodules ) unilobar unresectable hcc and with a main target lesion > 3 cm ( range , 3.56 cm ) not suitable for curative therapy were enrolled in our single - centre multidisciplinary pilot study . 
valutare nei pazienti affetti da epatocarcinoma multinodulare unilobare non resecabile , con almeno una lesione con diametro > 3 cm , la fattibilit , la sicurezza e lefficacia di una nuova terapia combinata con rfa durante occlusione arteriosa con catetere per pta ( borfa ) seguita da tace della lesione principale e tace delle restanti lesioni , in ununica seduta . 
 early local efficacy was evaluated on 1 - month follow - up multiphasic computed tomography ( ct ) on the basis of the modified response evaluation criteria in solid tumors ( m - recist )  . 
overall technical success , defined as complete devascularisation of all nodules during the arterial phase , was achieved in seven of 10 patients , with three cases of partial response ( persistence of small hypervascular nodules )  . 
tace and bo - rfa , plus tace in a singlestep approach seems to be a safe and effective combined therapy for treating advanced , unresectable hcc lesions , allowing a high rate of complete local response to be achieved in large lesions also . keywords hepatocellular carcinoma radiofrequency ablation chemoembolization combined therapy treatment algorithm multidisciplinare . 
il piano di trattamento stato : rfa ( ago con punta esposta da 3 cm ) della lesione target durante occlusione endovascolare dellarteria epatica afferente al tumore con catetere per pta seguita da una tace selettiva della stessa , pi una tace lobare per il trattamento delle altre lesioni ( 450 mg di carboplatino pi lipiodol associato a embolizzazione temporanea con spongostan )  . 
 lefficacia locale in fase precoce stata valutata mediante tc multifasica eseguita a un mese dalla procedura , sulla base dei criteri m - recist ; separatamente stata , inoltre , effettuata una valutazione delle lesioni target in termini di enhancement , diametro dellarea necrotica e presenza e distribuzione di lipiodol . 
il successo tecnico complessivo , definito come la completa devascolarizzazione di tutti i noduli in fase arteriosa , stato ottenuto in 7 / 10 pazienti con 3 risposte parziali ( persistenza di piccoli noduli ipervascolarizzati )  . 
 considerando solo le lesioni target , il successo tecnico stato raggiunto in tutti i pazienti , con la presenza di unarea priva di enhancement nella zona corrispondente al precedente nodulo di hcc ( diametro necrotico 3 , 55 cm ) , con un accumulo periferico di lipiodol circonferenziale ( margine di sicurezza ) , di almeno 0 , 5 cm ( 0 , 51 , 3 cm )  . 
il trattamento combinato con bo - rfa seguita da tace , in un approccio single - step , sembra essere una terapia sicura ed efficace per il trattamento dellhcc avanzato non resecabile , permettendo di ottenere un alto tasso di risposta locale completa anche in lesioni di grandi dimensioni . parole chiave epatocarcinoma termoablazione a radiofrequenza chemioembolizzazione terapia combinata algoritmo di trattamento introduction introduzione hepatocellular carcinoma ( hcc ) is the fourth most common cancer in the world , responsible for an estimated 1 million deaths annually due to its poor prognosis due to rapid infiltrating growth and its frequent onset as a complication of liver cirrhosis [ 1 ]  . 
tumour diameter is an important prognostic factor in patients with hcc ; prognosis worsens markedly when the maximum diameter is > 5 cm [ 28 ]  . consensus about a common treatment strategy for patients with hcc has not been reached worldwide , even though several proposals have been published . 
surgical approaches , including liver resection and liver transplantalepatocarcinoma ( hcc ) il quarto tumore per frequenza nel mondo , responsabile di circa 1 milione di decessi / anno , essendo caratterizzato da una prognosi sfavorevole a causa della sua rapida crescita a carattere infiltrativo e della sua insorgenza , nella maggior parte dei casi , su un fegato cirrotico [ 1 ]  . 
la prognosi , infatti , peggiora nettamente quando il diametro massimo della lesione supera i 5 cm [ 28 ]  . a tuttoggi non stata ancora raggiunta una strategia terapeutica universalmente condivisa per i pazienti affetti da hcc , anche se sono state avanzate numerose proposte . 
 la pi recente tra queste la classificazione barcelona - cliradiol med ( 2013 ) 118 : 555569 tion , are regarded as curative treatments for hcc [ 10 , 11 ]  . 
 however , only 929% of patients are suitable for surgical therapy due to poor hepatic reserve resulting from underlying chronic liver disease , multifocal distribution of tumour nodules , extrahepatic metastases , early vascular invasion , shortage of donor organs , high complication rates and comorbidities [ 1214 ]  . 
 local ablation [ alcohol injection or radiofrequency ablation ( rfa ) ] is a safe and effective therapy for patients with small lesions who cannot undergo resection [ 1517 ]  . 
transcatheter arterial chemoembolization ( tace ) is recommended as a first - line , noncurative therapy for nonsurgical patients with large / multifocal hcc who do not have vascular invasion or extrahepatic spread [ 18 , 19 ]  . 
for patients who have either failed tace or who present with more advanced hcc , new data indicate the efficacy of sorafenib in prolonging life [ 9 , 20 ]  . 
 available data suggest that combined therapy with rfa and chemoembolization is superior to either one alone in improving patient survival , but it is not clear which is the best combination of these two procedures [ 2125 ]  . the purpose of our study was to evaluate feasibility , safety and efficacy of a new combined single - step therapy in patients with unresectable multinodular unilobar hcc , with at least one lesion > 3 cm , with balloon - occluded rfa ( bo - rfa ) plus tace of the main lesion and tace of the other lesions . materials and methods study design and population the ethical conduct of the study was approved by our departmental review board in agreement with the 1990 declaration of helsinki and subsequent amendments . 
a prospective single - centre multidisciplinary pilot study was carried out to test a new single - step combined therapy with rfa of the main target lesion during balloon - occlusion of the hepatic artery supplying the tumour , followed by selective chemoembolisation ; the procedure was completed by a lobar chemoembolization focused on the treatment of the other small nodules . requirements for inclusion were : ( a ) multinodular hcc with a main lesion 3 cm in diameter and not suitable for surgery ; ( b ) unilobar nodules ; ( c ) liver cirrhosis classified as childpugh class a or b ; ( d ) no vascular invasion or extrahepatic metastases ; ( e ) no previous treatment . 
 exclusion criteria were : ( a ) childpugh class c ; ( b ) platelet count < 40 , 000 / l and international normalized nic liver cancer ( bclc ) per la stadiazione e il trattamento dellhcc [ 9 ]  . 
tuttavia , solo il 929% dei pazienti con hcc alla diagnosi sono suscettibili di terapia chirurgica a causa di diversi fattori quali la compromissione della funzionalit epatica dovuta allepatopatia cronica sottostante , la distribuzione multifocale del tumore , la presenza di metastasi extra - epatiche , la precoce invasione vascolare , la carenza di donatori di organi , lalto tasso di complicanze e comorbidit [ 1214 ]  . lablazione locoregionale ( attraverso liniezione di alcool o mediante radiofrequenza ) una terapia sicura ed efficace per i pazienti con lesioni di piccole dimensioni che non possono essere sottoposti a resezione chirurgica [ 1517 ]  . 
la chemioembolizzazione transarteriosa ( transarterial chemoembolization , tace ) invece raccomandata come terapia di scelta non curativa per i pazienti non suscettibili di approccio chirurgico che presentano un hcc di grandi dimensioni e / o multifocale senza invasione vascolare o diffusione extraepatica [ 18 , 19 ]  . 
infine , per i pazienti in cui il trattamento con tace abbia fallito , o che presentino un hcc molto avanzato , nuovi dati indicano lefficacia del sorafenib nel prolungare la sopravvivenza [ 9 , 20 ]  . recentemente sono stati pubblicati numerosi studi che hanno valutato un approccio multimodale nella terapia dellhcc avanzato allo scopo di aumentare lefficacia dei singoli trattamenti . 
i dati finora disponibili suggeriscono che la terapia combinata con ablazione a radiofrequenza ( radiofrequency ablation , rfa ) e chemioembolizzazione superiore in termini di sopravvivenza alla chemioembolizzazione o alla rfa da sola , ma non chiaro quale sia la migliore combinazione di queste due procedure [ 2125 ]  . sulla base di questo background , lobiettivo del nostro studio quello di valutare la fattibilit , la sicurezza e lefficacia di una nuova terapia combinata in approccio singlestep in pazienti affetti da hcc multinodulare , unilobare , non resecabile con almeno una lesione di diametro superiore ai 3 cm , con rfa durante occlusione arteriosa ( balloon occlusion , bo ) temporanea endovascolare seguita da tace della lesione principale e tace delle altre lesioni . materiali e metodi disegno dello studio / popolazione di studio la condotta etica dello studio stata approvata dal comitato etico e dallautorit competente del nostro dipartimento , in accordo con la dichiarazione di helsinki del 1990 e i successivi emendamenti . 
stato condotto uno studio pilota multidisciplinare monocentrico prospettico per testare una nuova terapia combinata in approccio single - step con rfa della lesione target di maggiori dimensioni durante locclusione endovascolare con catetere per angioplastica transluminale percutanea ( percutaneous transluminal angioplasty , pta ) dellarteria epatica afferente al tumore , seguita da una tace selettiva ; la procedura stata quindi completata da una chemioembolizzazione lobare focalizzata al trattamento 558 radiol med ( 2013 ) 118 : 555569 ratio ( inr ) of > 1.5 ; ( c ) severe renal impairment or serum creatinine levels > 2 mg / dl . pretreatment workup a routine physical examination , laboratory tests and imaging studies , including ultrasonography ( us ) , unenhanced and contrast - mediumenhanced computed tomography ( ct ) performed with a multiphasic protocol ( contrast flow rate 4 ml / s ; unenhanced , arterial , portal and late phases ; slice thickness , 0.625 mm ) using a 64 - multidetector - row ct scanner ( lightspeed vct , ge medical systems ) , were performed within 2 weeks before treatment in all patients . 
 the diagnosis of hcc was made on the basis of a positive serum - fetoprotein level ( > 20 ng / ml ) with positive imaging findings or at least two imaging techniques showing characteristic findings of arterial hypervascularisation in high - risk patients [ 26 ]  . treatment antibiotics were administered prophylactically before and 12 days after the procedures ( ciprofloxacin 500 mg )  . 
 diagnostic angiography was always performed under local anaesthesia ( 10 ml of 1% lidocaine ) using the seldinger technique through a right common femoral approach by placing a 6 - f angiographic introducer . 
an internally cooled electrode with a 3 - cm exposed tip ( cool - tip rf ablation system , valleylab , covidien ) was then introduced into the target nodule , and the occlusion balloon in the hepatic artery was filled with a mixture of saline solution and contrast material . 
the rf generator was activated , and a power needed to maintain a temperature of 90115c at the hook tips was delivered for 12 mat the end of the procedure , the electrode was withdrawn , the occlusion balloon deflated and immediate results evaluated with angiography . 
 i requisiti per linclusione nel nostro studio sono stati : ( a ) hcc multinodulare con una lesione principale con un diametro 3 cm , non suscettibile di trattamento chirurgico ; ( b ) distribuzione unilobare dei noduli ; ( c ) cirrosi epatica in classe a o b della classificazione di child - pugh ; ( d ) assenza di invasione vascolare e di metastasi extraepatiche ; ( e ) nessun precedente trattamento dellhcc . 
i criteri di esclusione sono stati : ( a ) classe c di child - pugh ; ( b ) una conta piastrinica inferiore a 40.000 / l e un valore di inr maggiore di 1 , 5 ; ( c ) insufficienza renale severa o valori di creatinina sierica superiori a 2 mg / dl . procedure pre - trattamento entro due settimane dal trattamento sono stati eseguiti in tutti i pazienti un esame obiettivo completo , esami laboratoristici ed esami radiologici , quali unecografia ( us ) e una tomografia computerizzata ( tc ) spirale multifasica eseguita senza e con infusione di mezzo di contrasto ( mdc ) ( velocit di infusione del contrasto 4 ml / s ; acquisizione senza mdc e in fase arteriosa , portale e tardiva ; collimazione : 0 , 625 mm ) utilizzando uno scanner multidetettore a 64 strati ( lightspeed vct , ge medical systems )  . 
la diagnosi di hcc stata effettuata sulla base dellaumento dei valori di - fetoproteina ( > 20 ng / ml ) associato a reperti radiologici suggestivi per hcc o almeno due tecniche di imaging con reperti caratteristici di ipervascolarizzazione in pazienti ad alto rischio [ 26 ]  . trattamento prima della procedura e fino a 12 giorni dopo stata somministrata una terapia antibiotica a scopo profilattico ( ciprofloxacina 500 mg )  . 
la fase angiografica diagnostica stata eseguita previo approccio transfemorale comune destro , in anestesia locale ( 10 ml di lidocaina 1% ) , utilizzando la tecnica di seldinger , posizionando un introduttore angiografico di 6 fr . 
 una guida angiografica 0 , 014 - inch ( choice , boston scientific ) stata introdotta nellarteria epatica afferente alla lesione , consentendo un adeguato e sicuro posizionamento di un catetere per pta monorail , a basso profilo ( 4520 mm , muso , terumo , tokyo , giappone )  . 
come analgesico per la sedazione stato usato fentanyl citrato ( 0 , 10 , 2 mg , phentanest , daiichi sankyo , tokyo , giappone ) , mentre la lidocaina ( xylocaine , astrazeneca international , osaka , giappone ) come anestetico locale . 
in particolare , un ago da termoablazione con una punta esposta di 3 cm ( cool - tip rf ablation system , valleylab , covidien ) stato introdotto nel contesto del nodulo target ; contemporaneamente stato gonfiato il radiol med ( 2013 ) 118 : 555569 embolisation of the main lesion was performed using a coaxial technique and placing a 2.7 - f microcatheter ( progreat ; terumo , tokyo , japan ) in the distal segmental hepatic artery that was feeding the hcc . 
in all cases , an emulsion of carboplatin and iodised oil ( lipiodol ultra fluid , mitsui , tokyo , japan ) was infused , followed by embolisation performed with gelatine sponge particles ( gelfoam , pfizer , tokyo , japan )  . 
a major complication was defined as an event that engenders substantial morbidity and disability or an increased level of care or that requires hospital admission or substantially lengthened hospital stay . 
 to evaluate complications after the procedure , all patients underwent haemoglobin , serum aminotransferase , meld and childpugh - related liver tests within 24 h , 7 days and 30 days after the procedure , and us within 4872 h after the procedure . 
alfa - fetoprotein and multiphasic spiral ct studies ( 64 - row ct lightspeed vct scanner , ge medical systems ; contrast flow rate 4 ml / s ; unenhanced , arterial , portal and late phases ; slice thickness , 0.625 mm ) were performed 1 month after the procedure to evaluate response to combined therapy ( bo - rfa + tace )  . 
complete and partial response , stable and progressive disease were determined as follows : complete response was defined as complete lesion devascularisation during the arterial phase ; necrosis was defined as no enhancing tissue ; complete necrosis of a lesion with a safety margin 5 mm in both arterial and portal venous phase images was considered to be indicative of complete response . 
 al termine della radiofrequenza , stata effettuata una tace ; in particolare , stata eseguita una chemioembolizzazione superselettiva della lesione principale usando una tecnica coassiale e introducendo un microcatetere di 2 , 7 fr ( progreat , terumo , tokyo , giappone ) nel segmento distale dellarteria epatica afferente al nodulo di hcc . 
in tutti i casi , si proceduto allinfusione di una emulsione di carboplatino ( carboplatin ) e lipiodol ( lipiodol ultra fluid , mitsui , tokyo , giappone ) , seguita da embolizzazione mediante particelle riassorbibili di spongostan ( gelfoam , pfizer , tokyo , giappone )  . 
in particolare , una complicanza maggiore stata definita come un evento che determina unimportante morbilit e invalidit o che richiede un intervento terapeutico maggiore o unospedalizzazione o un prolungamento della degenza . 
tutte le altre complicanze sono state considerate minori [ 27 ]  . per la valutazione delle complicanze post - procedurali , tutti i pazienti sono stati sottoposti a dosaggio dellemoglobina , degli indici di epatocitonecrosi e dei parametri epatici correlati agli scores di meld e child - pugh entro 24 ore , e dopo 7 e 30 giorni dalla procedura . 
un mese dopo la procedura sono stati eseguiti dosaggio dellalfafetoproteina e una tc spirale multifasica ( scanner multidetettore a 64 strati , ct lightspeed vct scanner , ge medical systems ; acquisizione senza mdc e in fase arteriosa , portale e tardiva ; 120 ml di mdc con flusso 4 ml / s ; collimazione 0 , 625 mm ) per valutare la risposta alla terapia combinata ( bo - rfa + tace )  . dopo il trattamento , le lesioni possono o meno subire delle modifiche nelle dimensioni . 
risposta completa , risposta parziale , stabilit e progressione di malattia sono state con560 radiol med ( 2013 ) 118 : 555569 radiol med ( 2013 ) 118 : 555569 fig . 
magnetic resonance ( mr ) images demonstrate a large target hypovascular nodule in hepatic segment vi ( 5 cm in diameter ) ( ac ) , with concomitant associated unilobar lesions ( d ) , as confirmed by digital subtraction angiography ( dsa ) ( e )  . 
the radiofrequency ablation ( rfa ) electrode is placed into the main target lesion under ultrasound ( us ) guidance , and the rf generator was activated during balloon occlusion ( arrow in f ) of the tumour arterial supply . 
after rfa , a superselective chemoembolization of the main lesion is performed by placing a microcatheter in the distal segmental hepatic artery feeding the hepatocellular carcinoma ( hcc ) ( i )  . 
le immagini mri mostrano un nodulo target di grandi dimensioni ipovascolare nel vi segmento epatico ( diametro 5 cm ) ( a - c ) con associate altre lesioni concomitanti a distribuzione unilobare ( d ) , come confermato dalla dsa ( e )  . 
lelettrodo per rfa viene posizionato a livello della lesione target sotto guida ecografica e il generatore di radiofrequenze viene attivato durante occlusione con palloncino ( freccia in f ) dellarteria afferente al tumore . 
progressive disease is at least a 20% increase or appearance of new lesions . according to our ethical committee , all patients with relapsing or progressive tumours were treated with the best possible options ( other percutaneous therapies such as repeated tace , supportive care )  . 
 tace group all patients were individually matched with a balanced group of patients ( ratio 1 : 2 ) who underwent tace alone in single - step treatment in our centre during the previous year to compare initial technical effects in terms of tumour necrosis . 
the tace group was considered the control group in order to perform a formal comparison of efficacy between standard treatment and investigational treatment groups . results study population between april and september 2010 , ten consecutive pasiderate come segue : una risposta completa stata definita come completa devascolarizzazione della lesione durante la fase arteriosa ; la necrosi stata definita come assenza di enhancement ; la necrosi completa di una lesione con la presenza di un margine di sicurezza maggiore o uguale di 5 mm in fase arteriosa e venosa portale stata considerata indicativa di risposta completa . 
the underlying biopsy - proven cirrhosis was related to hepatitis c in five patients ( 50% ) , hepatitis b in two patients ( 20% ) , alcohol use in one patient ( 10% ) and cryptogenic in two patients ( 20% )  . 
il gruppo tace stato considerato alla stregua di un gruppo di controllo in modo da effettuare una comparazione formale di efficacia tra il trattamento standard e il trattamento sperimentale . risultati popolazione dello studio tra aprile e settembre 2010 , dieci pazienti consecutivi ( 10 uomini ; et media 68 , 78 , 6 anni ; range 5679 anni ) con hcc multinodulare ( 26 noduli ) , unilobare , non resecabile ( diagnosticato secondo linee guida aasld per la gestione dellhcc , 2010 ) e con una lesione target > 3 cm , non suscettibile di terapie curative , sono stati arruolati nel nostro centro per questo studio pilota multidisciplinare . 
laltezza e il peso medio dei pazienti risultato pari a 169 , 66 , 8 cm ( range 160184 cm ) e di 70 , 47 , 3 kg ( range 6293 kg ) , rispettivamente ; il bmi risultato pari a 29 , 24 , 8 kg / m2 ( range 23 , 535 kg / m2 )  . linsufficienza epatica stata valutata con punteggio child - pugh : cirrosi in classe a in 7 pazienti ( 70% ) , classe b in 3 pazienti ( 30% )  . 
la cirrosi sottostante , diagnosticata istologicamente , risultata correlata a infezione da epatite c in 5 pazienti ( 50% ) , epatite b in 2 pazienti ( 20% ) , abuso di alcool in 1 paziente ( 10% ) , e criptogenetica in 2 pazienti ( 20% )  . 
nessun danno si verificato a livello dellarteria epatica ; in particolare , non stata registrata alcuna trombosi o dissezione arteriosa , lacerazione o rottura . i pazienti sono stati dimessi tra le 7296 h . 
digital subtraction angiography ( dsa ) image demonstrates a main hepatocellular carcinoma ( hcc ) nodule in segment viii ( arrow in a ) abutting the diaphragthis was treated with balloon - occluded radiofrequency ablation ( bo - rfa ) ( b ) followed by selective chemoembolization ( c ) ; the other small adjacent nodule ( arrowhead in a ) was treated with chemoembolization only . 
le immagini dsa mostrano un nodulo target di hcc nellviii segmento ( freccia in a ) strettamente adiacente al diaframma , trattato con bo - rfa ( b ) , e successiva chemioembolizzazione ( c ) ; un altro piccolo nodulo adiacente ( freccia sopra in a ) stato trattato esclusivamente con chemioembolizzazione . 
conversely , when we considered concomitant nodules , complete lipiodol uptake without conosservato un ematoma sottocapsulare autolimitantesi e in 7 pazienti ipertransaminasemia , per i quali non stato comunque richiesto alcun trattamento . 
i livelli di alfafetoproteina hanno subito un decremento in tutti i pazienti che presentavano valori pre - trattamento elevati , riportandosi allinterno del range di normalit in 7 pazienti , tra 20100 g / l in 2 , e da 1 , 528 a 975 g / l in 1 paziente , con un decremento statisticamente significativo rispetto ai valori al baseline ( p < 0 , 05 )  . risultati a breve termine allesame tc eseguito a 1 mese dal trattamento , se si considera la lesione target , stata sempre ottenuta unarea priva di enhancement nella zona corrispondente al precedente nodulo di hcc ( diametro medio dellarea necrotica 3 , 420 , 41 cm , range 34 , 5 cm ) , con un accumulo periferico circonferenziale di lipiodol , quale margine di sicurezza , di almeno 1 , 020 , 71 cm ( 0 , 32 , 8 cm ) , con un diametro finale medio 564 radiol med ( 2013 ) 118 : 555569 fig . 
post - rfa transarterial chemoembolization ( tace ) ( d ) allowed us to treat active arterial bleeding without any other adjunctive treatment , with complete resolution of the complication , as demonstrated by ultrasound performed 48 h after the procedure ( e ) and 1 - month computed tomography ( ct ) follow - up ( f )  . 
la tace post - rfa ( d ) ha permesso di trattare il sanguinamento arterioso attivo senza necessit di trattamenti aggiuntivi , con completa risoluzione della complicanza , come evidenziato da unecografia eseguita 48 ore dopo la procedura ( e ) , e dalla tc a un mese ( f ) ; nel dettaglio , le immagini tc dimostrano la necrosi completa della lesione senza alcuna complicanza . 
 trast enhancement was obtained in 13 / 27 lesions ( 48.2% ) , whereas a partial response was obtained in the remaining 14 lesions : residual tumour < 30% in nine ( 33.3% ) ; 3050% in four lesions ( 14.8% ) ; > 50% in one lesion ( 3.7% ) , without progressive disease or new lesions observed ( 0% )  . 
among 87 patients with multinodular della lesione trattata ( area necrotica e margine di sicurezza ) di 4 , 530 , 53 cm ( range 3 , 65 , 5 cm )  . se si considera solo la lesione target , stata ottenuta una risposta completa in 7 / 10 ( 70% ) pazienti , una risposta parziale in 3 / 10 pazienti ( tumore vitale residuo < 30% : 1 paziente ; 3050% : 2 pazienti ; > 50% : 0 pazienti ) , in assenza di progressione di malattia . 
se si considerano i noduli concomitanti , stata osservata una captazione completa di lipiodol senza contrast - enhancement in 13 / 27 lesioni ( 48 , 2% ) , mentre stata ottenuta una risposta parziale nelle altre 14 lesioni ( tumore residuo < 30% : 9 lesioni , 33 , 3% ; 3050% : 4 lesioni , 14 , 8% ; > 50% : 1 lesione , 3 , 7% ) , senza progressione di malattia o comparsa di nuove lesioni ( 0% )  . 
riassumendo , una necrosi completa o un tumore residuo < 30% stato ottenuto in 22 / 27 lesioni ( 81 , 5% )  . radiol med ( 2013 ) 118 : 555569 unilobar hcc treated with selective / lobar chemoembolization ( tace ) alone [ emulsion of 450 mg of carboplatin and iodised oil followed by embolisation performed with gelatine sponge particles ( gelfoam ; pfizer , tokyo , japan ) ] , we selected 20 patients who were individually matched with the study population to create a balanced control group to formally compare efficacy between standard and investigational treatment in a single - step approach . the tace group comprised 20 patients with similar epidemiological ( 18 men , two women ; mean age , 66.46.3 years ; range , 5483 years ) and lesion ( multinodular unilobar unresectable hcc with a target main lesion > 3 cm ) characteristics . 
when considering concomitant nodules , complete lipiodol uptake without contrast enhancement was obtained in 10 / 51 lesions ( 19.6% ) , whereas a partial response was obtained in the remaining 40 lesions : residual tumour < 30% in 12 lesions ( 23.5% ) ; 3050% in 19 lesions ( 37.2% ) ; > 50% in ten lesions ( 19.6% ) , without progressive disease or new lesions observed ( 0% )  . 
its major weakness is related to the limited size of coagulation necrosis that can be obtained ; in fact , a complete short - term necrosis can be achieved in < 5070% of lesions > 3 cm in diameter , even if the procedure is repeated [ 17 ]  . 
central lesions should be avoided because of the risk of injury to the central gruppo tace stata eseguita una ricerca nel sistema di archivio elettronico per identificare tutti i pazienti sottoposti a tace nel nostro dipartimento tra gennaio e dicembre 2009 . 
su un totale di 87 pazienti con hcc multinodulare unilobare trattati con singola chemioembolizzazione ( tace ) selettiva / lobare ( emulsione di 450 mg di carboplatino [ carboplatin ] e lipiodol [ lipiodol ultra fluid ] seguita da embolizzazione effettuata con particelle riassorbibili di spongostan [ gelfoam ] ) , sono stati selezionati 20 pazienti da confrontare con la popolazione di studio , al fine di creare un gruppo equilibrato di controllo per eseguire un confronto formale tra lefficacia del trattamento standard e il gruppo di trattamento sperimentale con approccio combinato in single - step . il gruppo tace risultato composto da 20 pazienti con caratteristiche simili epidemiologiche ( 18 uomini , 2 donne ; et media : 66 , 46 , 3 anni ; range 5483 anni ) e simile tipologia di lesioni ( hcc multinodulare unilobare non resecabile con una lesione target maggiore di 3 cm )  . 
il diametro medio della lesione target risultato pari a 4 , 30 , 4 cm ( 3 , 36 , 2 cm ) con un totale di 51 lesioni associate ( 8 pazienti avevano un altro nodulo di hcc inferiore a 3 cm , 8 meno di 5 lesioni unilobari concomitanti e 4 pi di 5 lesioni unilobari concomitanti )  . al controllo tc eseguito a 1 mese dal trattamento , se si considera la lesione target , una risposta completa stata ottenuta in 2 / 20 ( 10% ) pazienti , una risposta parziale , con tumore vitale residuo < 30% , in 4 / 20 ( 20% ) pazienti , con tumore vitale residuo > 30% in 8 / 20 ( 40% ) pazienti , e con tumore vitale residuo > 50% nei restanti 6 / 20 pazienti ( 30% )  . 
 se si considerano i noduli concomitanti , stata osservata una captazione completa di lipiodol senza contrast - enhancement in 10 / 51 lesioni ( 19.6% ) , mentre una risposta parziale stata osservata nelle restanti 40 lesioni ( residuo tumorale < 30% : 12 lesioni , 23 , 5% ; 3050% : 19 lesioni , 37 , 2% ; > 50% : 10 lesioni , 19 , 6% ) , in assenza di progressione di malattia o comparsa di nuove lesioni ( 0% )  . 
riassumendo , una necrosi completa o con residuo tumorale < 30% stata osservata in 22 / 51 lesioni ( 43 , 1% )  . discussione sebbene i programmi di screening per pazienti ad alto rischio siano attualmente molto diffusi , rendendo possibile la diagnosi di hcc in fasi iniziali , alcuni pazienti si presentano ancora alla diagnosi con hcc di grandi dimensioni e con una prognosi sfavorevole perch suscettibili solo di trattamenti palliativi . 
noto che i pazienti in cui viene effettuata diagnosi in fase precoce di early - hcc rappresentano i candidati ottimali per la resezione , trapianto di fegato o ablazione percutanea . 
il suo limite principale legato alla possibilit di ottenere solo unestensione modesta della necrosi coagulativa ; come dato di fatto , una necrosi 566 radiol med ( 2013 ) 118 : 555569 bile duct and vessels , whereas lesions bordering a large ( > 3 mm ) vessel may not respond because of thermal protection provided by the adjacent blood flow , a phenomenon termed heat sink . 
to increase the area of coagulation necrosis ( ablation zone size ) , arterial occlusion such as balloon occlusion , embolisation and chemoembolization are combined with rfa [ 28 , 29 ]  . however , if these options are not feasible , patients must be considered for palliation . 
finally , patients at a terminal stage with deeply impaired physical condition ( performance status > 2 ) and / or massive tumour burden with heavily impaired liver function should receive symptomatic treatment to avoid unnecessary suffering . the main aims of research in this field should be to increase the rate of patients suitable for curative treatment and , consequently , reduce indications for palliation only . 
 recent data suggest that combined therapy with rfa and chemoembolization is superior to chemoembolization or rfa alone in improving patient survival and more effective for treating large tumours [ 2125 ]  . 
 according to our approach , balloon occlusion of tumour arterial supply seems to increase the area of coagulation necrosis ( ablation zone size ) obtained with rfa , reducing arterial blood flow and minimising heat loss ( heat sink ) , as also reported by rossi et al . 
on the other hand , tace seems to increase the local effect of rfa by acting on the large zones of sublethal heating created during rfa application in tissues surrounding the electrode . 
 in detail , the chemotherapy drug should be concentrated in a relatively small volume of residual viable neoplastic tissue characterised by reduced cell resistance to the drug due to previous exposure to sublethal heating . 
the rationale for performing tace after rfa was based on the hypothesis that there could be a loss of efficacy of the drugs used during tace when they completa di breve durata pu essere realizzata in meno del 5070% delle lesioni di diametro maggiore di 3 cm , anche se la procedura viene ripetuta [ 17 ]  . 
il trattamento delle lesioni centrali dovrebbe essere evitato per il rischio elevato di danno a strutture centrali dellalbero biliare e vascolare , mentre quello di lesioni adiacenti ai grandi vasi ( > 3 mm ) potrebbe non presentare unadeguata risposta a causa della dispersione termica legata al flusso sanguigno , fenomeno chiamato heat sink . 
 il flusso sanguigno favorisce la dispersione di calore , per cui la riduzione o linterruzione dello stesso durante la procedura di rf permette di aumentare il volume della zona ablata . 
locclusione arteriosa , come ad esempio locclusione con palloncino , lembolizzazione e la chemioembolizzazione , viene combinata con la rfa per aumentare larea di necrosi coagulativa ( dimensione dellarea di ablazione ) [ 28 , 29 ]  . se tali opzioni terapeutiche non sono eseguibili , i pazienti devono essere considerati per un trattamento palliativo . 
i pazienti che si presentano con una malattia in stadio pi avanzato o che falliscono un trattamento con tace sono candidati al sorafenib a condizione che rimangano in classe child - pugh a e con un buon performance status . 
infine , i pazienti con malattia in stadio terminale in condizioni generali scadute ( performance status > 2 ) e / o con estensione tumorale massiva con funzionalit epatica residua pesantemente compromessa , potrebbero ricevere un trattamento sintomatico per evitare sofferenze non necessarie . 
 lo scopo principale dei ricercatori in questo campo di interesse dovrebbe essere aumentare il tasso di pazienti candidabili a trattamenti curativi e conseguentemente ridurre le indicazioni per la sola palliazione . 
recenti dati suggeriscono che la terapia combinata con rfa e chemioembolizzazione superiore ai singoli trattamenti in termini di aumento della sopravvivenza , ed pi efficace nel trattamento di tumori di grandi dimensioni [ 2125 ]  . 
 secondo il nostro approccio , locclusione con palloncino dellarteria afferente alla lesione tumorale sembra aumentare larea di necrosi coagulativa ( dimensioni dellarea di ablazione ) ottenuta con la rfa , riducendo il flusso arterioso e minimizzando la dispersione di calore ( heat sink ) , come stato riportato da rossi et al . 
in particolare , il chemioterapico potrebbe concentrarsi in un volume relativamente piccolo di tessuto neoplastico residuo vitale caratterizzato da una ridotta resistenza cellulare al farmaco per la precedente esposizione alla dose subletale di calore . 
 our approach allowed us to obtain a high rate of complete local response in large lesions as well ( mean diameter of the target lesion , 4.10.5 cm ) , with a complete necrosis or residual tumour < 30% obtained in 80% of patients . 
 these results are interesting if compared to the rate of complete necrosis or residual tumour < 30% obtained in the tace control group ( 30% for the target lesion and ~ 43% for associated nodules )  . 
it is well known that tace alone needs to be repeated either at regular intervals or on demand and that repeating tace may damage noncancerous hepatocyte functions and affect clinical course . 
moreover , our approach allowed us to expand the indication for rfa to previously contraindicated cases with difficulty in the application or the high - risk nature of rfa [ 17 ]  . 
hepatic tumours adjacent to the diaphragm with a consequent high risk of thermal injury , or tumours located on the intra - abdominal free surface or proximal to the hepatic portal region . 
in fact , the aim of ensuring a safety margin should be related to the high risk of damage to the hepatic artery or portal vein , which would lead to hepatic infarction , or bile - duct injury - associated complications , such as biloma or abscess . 
il razionale nelleseguire la tace dopo la rfa basato sullipotesi che i farmaci usati durante la tace potrebbero essere meno efficaci se esposti ad alte temperature [ 30 ]  . 
 nel dettaglio , il nostro approccio ha permesso di ottenere un alto tasso di risposta locale completa in lesioni di grandi dimensioni ( diametro medio della lesione target 4 , 10 , 5 cm ) con una necrosi completa o la persistenza di un residuo tumorale < 30% , ottenuto nell80% dei pazienti . 
relativamente ai noduli associati , il nostro approccio ha permesso di trattare lesioni multiple in ununica seduta , ottenendo una necrosi completa o un residuo tumorale < 30% in 22 / 27 lesioni ( 81 , 5% )  . questi risultati sono molto interessanti se comparati anche con la percentuale di necrosi completa o di residuo tumorale inferiore al 30% ottenuta nel gruppo tace di controllo ( 30% per le lesioni target e circa il 43% per i noduli associati )  . 
 noto che la sola tace richiede la ripetizione del trattamento a intervalli regolari o al bisogno e le ripetute sedute di tace potrebbero danneggiare gli epatociti sani e condizionare perci il decorso clinico . 
durante il follow - up , inoltre , la lesione residua pu riacquisire la propria vascolarizzazione permettendo al tumore di continuare a crescere e influenzando , cos , la risposta finale al trattamento . 
peraltro , il nostro approccio ha permesso di espandere le indicazioni alla rfa anche ai casi precedentemente controindicati per difficolt nellesecuzione o per lalto rischio insito nella procedura [ 17 ]  . 
in dettaglio , stato possibile trattare efficacemente con rfa anche lesioni complesse ( 4 / 10 , 40% ) , ad esempio noduli epatici adiacenti al diaframma con un conseguente alto rischio di danno termico , oppure tumori localizzati a livello della superficie libera intra - addominale o prossimali alla regione portale epatica . 
come dato di fatto , lobiettivo di assicurare un margine di sicurezza dovrebbe contrastare lalto rischio di danno allarteria epatica o alla vena porta , che causerebbe uneventuale area infartuale , oppure le complicanze associate al danno dei dotti biliari , quale un biloma o un ascesso . 
 further studies with long - term follow - up are also needed to determine the survival rate at 1 , 3 , and 5 years in these patients . in conclusion , our pilot study demonstrated that in patients with multinodular , unilobar , unresectable hcc with at least one lesion > 3 cm , bo - rfa plus tace in the main lesion associated with tace in the other lesions in a single - step approach seems to be a safe and feasible combined therapy for treating advanced hcc . 
this proof - of - concept study shows that our multimodal , single - step approach could represent a curative treatment for patients with advanced hcc previously suitable for a palliative approach only ( tace or sorafenib ) and a possible effective downstaging procedure in patients initially not candidates to liver transplantation . necessit di trasfusioni di sangue o di ulteriori trattamenti . 
 in conclusione , lo studio pilota ha dimostrato che nei pazienti affetti da epatocarcinoma multinodulare , unilobare , non resecabile , con almeno una lesione target con diametro superiore ai 3 cm , il trattamento combinato con rfa durante occlusione arteriosa temporanea endovascolare con catetere da pta seguita da tace della lesione principale associata a tace delle altre lesioni in un approccio single - step , sembra essere una terapia fattibile e sicura per il trattamento dellhcc avanzato . 
 lymphoscintigraphy , as stated by the editors in their preface to the book is a nuclear medicine imaging procedure that provides information about the functional status of the lymphatic system . born as a procedure aimed to study peripheral oedema and lymph effusion , lymphoscintigraphy is nowadays particularly employed in the detection of sentinel nodes . 
sentinel nodes are those representing the first station encountered by cancerous lymph on its way to systemic diffusion . evaluation of these nodes by means of radio - guided biopsy helps to affirm or rule out that cancer lymph spread is under way locally or further along at other echelon nodes . 
 in order to fully appreciate the importance of this assertion the reader needs to deeply understand basic concepts on lymphatic system anatomy , function , pathophysiology and lymphoscintigraphy procedures ( radiopharmaceutical use and technical instrumentation ) all described in the first three chapters of the book . the opening chapters are followed by two chapters on the clinical evaluation of patients affected by oedema of the extremities and by diseases causing lymphoedema or intracavitary lymph effusion . 
the following 8 chore chapters are designed to describe and make clear to the reader the sentinel node biopsy use of in surgical oncology by means of planar static and dynamic lymphoscintigraphy coupled with spect / ct fusion imaging modalities . 
these chapters deal with different sorts of malignancies ; the most interesting are those on breast cancer and coetaneous melanoma . pubblicato sotto legida del gruppo di studio di chirurgia radioguidata dellassociazione italiana di medicina nucleare ( aimn ) , questo atlante si prefigge lo scopo di diffondere la conoscenza delle metodiche della linfoscintigrafia in medicina nucleare nello studio del sistema linfatico e nella valutazione delle sue affezioni , soprattutto nel cancro . 
 la valutazione di questi linfonodi , mediante una biopsia radio - guidata , risulta utile nel confermare od escludere che una diffusione cancerogena linfatica sia in atto localmente o pi oltre in linfonodi di stazioni successive . 
per apprezzare in pieno limportanza di questa affermazione il lettore deve comprendere a fondo dei concetti di base sullanatomia , funzione , patofisiologia del sistema linfatico , nonch sulle procedure operative linfoscintigrafiche ( uso dei radiofarmaci e strumentazione tecnica ) , tutte descritte nei primi tre capitoli del volume . ai capitoli di apertura , ne fanno seguito due sulla valutazione clinica dei pazienti affetti da edema delle estremit e da malattie che provocano linfedema o versamenti linfatici endocavitari . 
i successivi ed impegnativi 8 capitoli hanno lo scopo di descrivere e chiarire al lettore luso della biopsia del linfonodo sentinella nella chirugia oncologica mediante luso della linfoscintigrafia planare statica e dinamica associata alle modalit di fusione per immagini spect / ct . 
 questi capitoli trattano diversi tipi di lesioni maligne : i pi interessanti sono quelli sul carcinoma mammario e sul melanoma cutaneo . radiol med ( 2013 ) 118 : 702703 each of these chapters is enriched by teaching cases which ( by the use of very nice images coupled with a short clinical background and technical imaging data ) show how useful and important lymphoscintigraphy can be in the patients diagnostic evaluation and treatment : a procedure which very often offers to the surgeon hints on how to avoid unnecessary or extensive node dissection , avoiding related possible morbidity and late effects . 
noteworthy is the absence of a list of used abbreviations and an index . ciascuno di questi capitoli arricchito da casi educazionali che ( mediante limpiego di immagini molto belle , associate ad una breve disanima clinica e relativi dati tecnici ) , dimostrano quanto sia utile ed importante la linfoscintigrafia nella valutazione diagnostica e nel trattamento del paziente : procedura che assai spesso offre al chirurgo indicazioni su come evitare dissezioni nodali inutili od estese , evitando cos la possibile , associata morbilit nonch conseguenze tardive . questo volume sar di sicuro apprezzato dai medici di medicina nucleare , dai chirurghi oncologici , dai radiologi e dagli specializzandi in questo difficile campo . 
i valori di adc dei tumori ben differenziati e moderatamente differenziati sono stati significativamente diversi ( p = 0 , 005 ) rispetto ai valori degli npc scarsamente differenziati o indifferenziati . 
il valore di adc pu essere considerato un parametro prognostico non invasivo che correla con i parametri prognostici per lnpc . parole chiave diffusione nasofaringe carcinoma rm radiol med ( 2013 ) 118 : 534539 introduction nasopharyngeal carcinoma ( npc ) is one of the most common malignancies in chinese and southeast asians . 
established prognostic factors , such as histopathological type , tumour grade , primary tumour volume and nodal status , correlate significantly with overall survival and recurrence [ 14 ]  . diffusion - weighted magnetic resonance ( mr ) imaging has a growing role in managing patients with npc [ 5 ]  . 
it is used to differentiate npc from lymphoma [ 68 ] , characterise metastatic cervical lymph nodes [ 9 , 10 ] and differentiate recurrent tumour from postradiation changes [ 11 ]  . 
the apparent diffusion coefficient ( adc ) value has been correlated with some of the prognostic parameters of breast cancer [ 12 , 13 ] , lung cancer [ 14 ] and retinoblastoma [ 15 ]  . 
to our knowledge , no study in the english - language literature has investigated the correlation of adc with the prognostic parameters of npc , which was therefore the aim of this study . materials and method this prospective study was conducted on 33 consecutive patients with npc who underwent preand postcontrast and diffusion - weighted mr imaging ( dw - mri ) of the head and neck . 
the study finally comprised 30 patients ( 19 men , 11 women ; age range , 3872 ; mean age , 61 years ) with untreated , pathologically proven npc . 
 the study was approved by the institutional review board , and all patients provided informed consent . all mr imaging studies were performed with a 1.5 - tesla unit ( symphony ; siemens medical system , erlangen , germany ) equipped with a self - shielded gradient set ( 30 mt / m maximum gradient strength and 120 t / m / s slew rate ) for echo - planar imaging . 
all patients underwent axial t1and t2 - weighted imaging ( tr / te 9 , 000 / 70 ms ) with section thickness 4 mm , interslice 1 mm , field of view ( fov ) 2030 cm and an acquisition matrix 256224 . diffusion - weighted images were obtained using multislice , spin - echo , echo - planar sequences . 
imaging parameters were tr , 10 , 000 ms ; te , 108 ms ; number of excitations ( nex ) , 12 ; bandwidth , 300 khz ; matrix , 256128 ; fov , 2030 cm ; section thickness , 5 mm ; interslice gap , 1 mdiffusion gradients were applied in the three orthogonal directions ( x , y and z )  . 
after intravenous injection of 0.1 mmol / kg gadopentetate dimeglumine ( magnevist ; schering , berlin , germany ) , fat - suppressed t1 - weighted mr images ( tr / te , 400575 / 1315 ms ) were acquired in the axial , coronal and sagittal planes . 
fat suppression was accomplished with a frequency - selective presaturation pulse . image analysis was done by a radiologist ( aa ) with 20 years of experience with mr imaging who was blinded to clinical data and histopathological results . 
enlarged cervical lymph nodes were diagnosed on t2 and postcontrast t1 - weighted images if the shortest axial diameter was 5 mm in the lateral retropharyngeal region , 11 mm in the jugulodigastric region or 10 mm in other nonretropharyngeal neck nodes [ 1 ]  . the final diagnosis for npc was made by fibre - optic endoscopy with biopsy and histopathological examination . 
the pathological type of npc was classified according to world health organization ( who ) classification into squamous cell carcinoma ( type 1 ) , nonkeratinising carcinoma ( type 2 ) and undifferentiated carcinoma ( type 3 ) [ 16 ]  . 
the final diagnosis of nodal metastasis was determined following fine - needle aspiration biopsy ( fnab ) of the largest node . statistical analysis was performed using spss ( statistical package for the social sciences , version 10 )  . 
a grafico a barra che mostra il valore di adc nelle diverse tipologie di npc : non si evidenzia una differenza significativa nel valore di adc tra i diversi tipi patologici ( p = 0 , 300 )  . 
b grafico a barra che mostra il valore di adc nei differenti gradi tumorali : il valore di adc dei npc scarsamente differenziati o indifferenziati significativamente minore ( p = 0 , 005 ) rispetto a quello dei tumori moderatamente o ben differenziati . 
c grafico a barra che mostra il valore di adc dei npc in relazione al volume del tumore : il valore di adc minore nei pazienti con tumori di volume maggiore ( p = 0 , 030 )  . 
dwmr imaging can differentiate npc from nasopharyngeal lymphoma on the basis of adc values , as the latter has a lower adc value [ 68 ]  . in our study , adc value varied according to histopathological types : type 2 had a lower value than types 1 and 3 , but the difference was not significant . 
the adc value of retinoblastoma correlated well with the degree of tumour differentiation [ 15 ]  . primary ncp tumour volume is reported to have a close relationship with prognosis in head and neck cancer . 
 there is a negative correlation between adc value and the size of breast cancer ( r = 0.504 , p = 0.001 ) and retinoblastoma ( r = 0.680 , p = 0.015 ) [ 12 , 15 ]  . 
this may be attributed to the increasing bulk of the tumour , which entails an increased number of tumour clonogen areas , with subsequent restricted diffusion of large tumours . the presence of metastatic cervical lymph nodes is the most important single predictor of long - term survival in patients with npc . 
also , dw - mr imaging has been used to differentiate metastatic from reactive lymph nodes in patients with squamous - cell carcinoma of the head and neck [ 10 ]  . 
filippi8 on behalf of airo young and airo prostate cancer working group 1radiotherapy and radiosurgery department , istituto clinico humanitas , humanitas cancer center , rozzano ( mi ) , italy 2radiotherapy department , istituto del radio o . 
maria nuova , reggio emilia , italy 5service doncologie radiothrapie , chu ibn rochd , casablanca , morocco 6department of radiation oncology , university of florence , florence , italy 7division of radiotherapy , european institute of oncology , university of milan , milan , italy 8department of medical and surgical sciences , radiation oncology unit , university of torino , torino , italy correspondence to : b . 
de bari , e - mail : bdebari@yahoo.it received : 20 december 2011 / accepted : 20 february 2012 / published online : 28 january 2013 springer - verlag 2013 abstract purpose . 
radiotherapy ( rt ) has an established role in the postoperative treatment of prostate cancer patients with extracapsular extension , positive surgical margins or a detectable post - operative prostate - specific antigen ( psa )  . 
despite the large number of patients treated with postoperative rt , some issues about optimal technique , doses , volumes , timing and association with androgen deprivation are still subject of debate . 
two of them were cases of postoperative prostate cancer , differing in t stage of the primary tumour according to the tnm classification , preoperative staging procedures , preoperative psa ( ipsa ) , gleason score of biopsies and definitive pathological specimen after surgery and postoperative psa . 
la radioterapia ( rt ) ha un ruolo ben stabilito nel trattamento postoperatorio dei pazienti con tumore della prostata in caso di diffusione extracapsulare , margini chirurgici positivi o di antigene prostatico specifico postoperatorio ( psa ) dosabile dopo la chirurgia . 
nonostante il grande numero di pazienti trattati , alcuni problemi circa la tecnica ottimale di trattamento , le dosi , i volumi , il timing rispetto alla chirurgia e lassociazione con la terapia ormonale sono ancora oggetto di dibattito . 
questi pazienti meriterebbero un approccio pi uniforme basato su raccomandazioni aggiornate , dettagliate e condivise sulla base delle evidenze disponibili . parole chiave procaina survey radioterapia postoperatoria tumore prostatico introduction introduzione postoperative radiotherapy ( rt ) in prostate cancer patients offers a potentially curative treatment method for selected high risk patients and / or with biochemical relapse after radical prostatectomy and may also reduce the risk of recurrence [ 17 ]  . 
the benefit of postoperative rt in terms of biochemical control , metastasis - free ( mfs ) and overall ( os ) survival was demonstrated in three large randomised studies [ 2 , 3 , 6 ]  . 
the presence of a biochemical relapse and / or of elevated levels of prostatespecific antigen ( psa ) after surgery , as well as results of analysis of surgical specimens , can direct radiation oncologists towards prescribing immediate adjuvant rather than salvage rt . 
indeed , two attitudes exist ( immediate vs salvage ) , and both may be justified . in favour of immediate adjuvant rt is the evidence that recurrence is often local , that immediate rt is likely to be more effective than salvage rt in n0 patients and that it could potentially avoid spread outside the pelvis of an inila radioterapia ( rt ) post - operatoria offre ai pazienti con tumore della prostata un trattamento potenzialmente curativo , in casi selezionati ad alto rischio e / o con recidiva biochimica dopo una prostatectomia radicale , e potrebbe essere in grado di ridurre il rischio di recidiva [ 17 ]  . 
il beneficio della rt post - operatoria in termini di controllo biochimico , sopravvivenza libera da malattia e sopravvivenza globale stata di recente dimostrata in 3 grandi trials clinici randomizzati [ 2 , 3 , 6 ]  . 
la presenza di una recidiva biochimica e / o di livelli elevati di antigene prostatico specifico ( psa ) dopo la chirurgia , cos come i risultati dellanalisi del pezzo operatorio possono indirizzare la scelta delloncologo radioterapista verso una rt adiuvante immediata o verso una rt di salvataggio . 
indeed , it can be argued that amongst patients in observational arms of the published randomised trials [ 2 , 3 , 6 ] , there is an important number of patients who did not develop biochemical failure ; therefore , salvage rt would irradiate ( and expose patients to potential treatment - related complications ) only patients presenting real biochemical evidence of failure . 
 in recent years , several rt modalities have been introduced for treating prostate cancer patients [ 815 ] : the full spectrum of treatment options is currently offered in italy , and their clinical impact should be prospectively evaluated . 
 moreover , advances in radiological sciences and nuclear medicine have had an impact on the daily clinical practice of radiation oncologists treating postoperative prostate cancer patients [ 16 ]  . 
finally , despite the wide scientific evidences base for treating these patients , several aspects are still open to discussion . the procaina ( prostate cancer indications attitudes ) project is a national italian survey conducted by the young group of italian association of radiation oncology ( young airo ) on behalf of the airo prostate cancer working group that assesses patterns of care among italian radiation oncologists and analyses criteria that influence their choices . 
the questionnaire consisted of two parts : the first section was to be completed using professional details ( italian region , public / private hospital , academic / not - academic position , ongoing prostate cancer trials at associated department of affiliation )  . 
for each case , radiache la recidiva spesso locale , che ha pi probabilit di essere efficace rispetto alla rt di salvataggio nei pazienti n0 e che pu potenzialmente evitare la diffusione di malattia al di fuori della pelvi . 
infatti , si pu notare che tra i pazienti nei bracci di osservazione degli studi clinici randomizzati [ 2 , 3 , 6 ] c una buona porzione di pazienti che non sviluppavano recidiva biochimica , bench non trattati : una radioterapia di salvataggio riserverebbe lirradiazione ( e le tossicit potenziali correlate al trattamento ) a quei pazienti che presentano una vera recidiva biochimica . 
 inoltre , i tassi di cura potrebbero non essere compromessi se lirradiazione fosse effettuata precocemente al momento dellevidenza di recidiva biochimica . negli ultimi anni , numerose modalit di rt sono state introdotte nel trattamento dei pazienti con cancro prostatico [ 815 ] : lo spettro completo delle opzioni di trattamento attualmente disponibile in italia e il loro impatto clinico deve essere valutato prospetticamente . 
inoltre , gli avanzamenti nel campo delle scienze radiologiche e della medicina nucleare hanno avuto un impatto nella pratica clinica quotidiana degli oncologi radioterapisti nel trattamento postoperatorio dei pazienti con tumore della prostata [ 16 ]  . 
infine , nonostante esistano numerose evidenze per questo tipo di pazienti , diversi aspetti restano delle questioni aperte . il progetto procaina ( prostate cancer indications attitudes ) unindagine nazionale promossa dallassociazione italiana di radioterapia oncologica ( airo ) giovani , con il patrocinio del gruppo di lavoro airo prostata , allo scopo di definire le scelte terapeutiche degli oncologi radioterapisti italiani ed analizzare i criteri che influenzano tali scelte . 
il presente report si sofferma sui risultati dellindagine riguardanti i pazienti candidati a rt post - operatoria , mentre i 2 casi clinici di radioterapia radicale saranno aggetto di un report a parte . 
 le evidenze e le controversie presenti in letteratura circa la rt nel setting post - operatorio sono state anche sottolineate e discusse . materiali e metodi popolazione e contesto durante il congresso nazionale airo 2010 , tenutosi a napoli ( italia ) 300 questionari anonimi sono stati distribuiti agli oncologi radioterapisti partecipanti al congresso . 
the questions are summarised in table 2 . inclusion criteria and data analysis a total of 300 questionnaires were distributed to radiation oncologists before the beginning of the airo national congress . 
sottoposto successivamente a prostatectomia retropubica radicale senza linfoadenectomia esame istologico : pt2cpn0pmx , gs 4 + 4 , r0 ; psa < 0 , 01 ng / ml in fase post - operatoria . 
 a clinical trial for prostate cancer patients was in progress at the departments of 20.6% of radiation oncologists ; the majority ( 9.5% ) stated a clinical trial involved image - guided rt ( igrt ) using cone - beam computed tomography ct ( cbct ) during rt for prostate cancer treatment , whereas the remainder reported at least one trial for metastatic patients . clinical cases table 3 summarises the most important results of the survey showing the main differences between the two clinical cases of postoperative prostate cancer . 
 casi clinici al termine del congresso , 128 / 300 ( 41% ) questionari sono stati correttamente compilati e considerati nella presente analisi . caratteristiche degli oncologi radioterapisti le informazioni professionali erano disponibili per 113 / 128 ( 91 , 8% ) dei partecipanti . 
 discussion this is the first survey among italian radiation oncologists stiche , mentre il 9 , 4% ritiene appropriata una risonanza magnetica ( rm ) pre - trattamento ed il 5 , 5% una tc - tomografia ad emissione di positroni ( pet ) con colina ; indicazione al trattamento : nell89 , 8% dei questionari , vi indicazione a rt entro i 6 mesi dalla prostatectomia radicale retro - pubica , mentre nel 9 , 4% di essi , la rt riservata al trattamento della recidiva biochimica ; dosi e volumi : nel 61 , 4% dei casi , una dose compresa tra 60 gy e 70 gy ritenuta appropriata , mentre nel 23 , 6% dei casi preferita una dose inferiore a 60 gy e nel 15% una dose superiore o uguale a 70 gy ; il frazionamento convenzionale la schedula di trattamento preferita ( 84 , 3% ) , mentre lipofrazionamento scelto nel 15 , 7% dei casi . 
la sola loggia prostatica preferita come volume di trattamento nel 92 , 1% dei questionari , mentre la pelvi aggiunta nei campi di rt nel 7 , 9% ; tecniche : la radioterapia conformazionale 3d ( 3d - crt ) la tecnica di scelta nel 79 , 5% dei casi , mentre la radioterapia ad intensit modulata ( imrt ) stata scelta nel 20 , 5% ; verifica del posizionamento : una valutazione settimanale mediante immagini portali ritenuta indicata nel 64 , 5% dei questionari , una cb - tc settimanale nel 13 , 2% ed una cb - tc quotidiana nel 12 , 4% ; preparazione del paziente : vescica piena e retto vuoto la condizione di preparazione preferita dall82 , 5% degli oncologi radioterapisti . lo stadio di malattia , la prognosi del paziente ed i dati di letteratura ( 12 , 6% ) sono stati i fattori maggiormente condizionanti la prescrizione e le modalit del trattamento . caso clinico numero 2 nel secondo caso clinico , denominato caso salvataggio , sono stati analizzati i seguenti aspetti : indicazione al trattamento : il 94 , 4% degli oncologi radioterapisti considera indicata una rt di salvataggio ; dosi e volumi : dosi maggiori di 70 gy ( 50 , 8% ) e dosi comprese tra 60 gy e 70 gy ( 41 , 3% ) sono considerate appropriate dai partecipanti ; il frazionamento convenzionale scelto dal 79 , 4% dei medici , mentre lipofrazionamento dal 20 , 6% . 
la sola loggia prostatica il volume di trattamento preferito dal 77% dei partecipanti , mentre la pelvi aggiunta al volume di trattamento dal 23% ; tecniche : la 3d - crt scelta dal 66 , 7% dei oncologi radioterapisti , mentre il resto ha scelto la imrt ; verifica del posizionamento : una valutazione settimanale mediante immagini portali ritenuta indicata nel 58 , 8% dei questionari , mentre una cb - ct settimanale o quotidiana rispettivamente nel 15 , 1% ; preparazione del paziente : vescica piena e retto vuoto la condizione di preparazione preferita dall82 , 5% degli oncologi radioterapisti . la prognosi del paziente ed i dati di letteratura sono i fattori maggiormente condizionanti la prescrizione e le modalit del trattamento ( 8 , 7% )  . 670 radiol med ( 2013 ) 118 : 660678 concerning postoperative rt in prostate cancer patients . 
one major issue in this sense is the appropriate therapeutic approach , particularly as regards the choice between radical prostatectomy ( rp ) and radical irradiation ( ri )  . 
even if a direct comparison between rp and ri in the context of a randomised trial has never been conducted , available data seem to confirm that in clinically localised prostate cancer , the two approaches are equally effective [ 17 ]  . conversely , in locally advanced prostate cancer patients , different surgical reports show the high risk of extracapsular extension and / or microscopic residual disease , and rtot is the standard of care with the highest level of evidence [ 17 ]  . a discussion regarding the crucial question about correct staging and candidate selection for ri or rp is beyond the scope of this paper . 
however , it should be stressed that the choice to irradiate a patient in a postoperative and / or salvage setting is not always an evidence - based process but a pragdiscussione questa la prima indagine condotta tra gli oncologi radioterapisti italiani riguardante la rt post - operatoria in pazienti affetti da cancro alla prostata . 
questo sottogruppo clinico piuttosto frequente nella pratica clinica quotidiana , tuttavia le modalit di trattamento variano ampiamente tra i diversi paesi e , allinterno dello stesso paese , tra medici diversi . 
la tabella 6 riassume gli argomenti a sostegno dei 2 diversi atteggiamenti . diverse ragioni cliniche , tecniche e organizzative locali potrebbero influenzare non solo la prescrizione di rt , ma anche la decisione di porre o meno indicazione alla radioterapia in ambito post - operatorio . 
una delle principali problematiche in questo senso sarebbe il corretto approccio terapeutico , in particolare nella scelta tra prostatectomia radicale ( rp ) e lirradiazione radicale ( ri )  . 
anche se un confronto diretto tra rp e ri nel contesto di uno studio randomizzato non mai stato condotto , i dati disponibili sembrano confermare che nel cancro della prostata clinicamente localizzato i due tipi di approcci mostrano di essere ugualmente efficaci [ 17 ]  . al contrario , nei pazienti affetti da tumore localmente avanzato della prostata , diversi studi chirurgici hanno dimostrato lalto rischio di estensione extracapsulare e / o di malattia microscopica residua , e la rtterapia ormonale ( ot ) lo standard di cura con il pi alto livello di evidenza [ 17 ]  . una discussione sulla questione cruciale per la corretta stadiazione e la selezione dei pazienti candidati al ri o rp table 5 pros and cons of adjuvant and salvage radiation therapy ( rt ) immediate rt pros recurrence is often local in n0 patients . 
a possible solution could be a real multidisciplinary approach in a context of close cooperation between surgeons and radiation oncologists in order to deliver more evidence - based treatments , thus overtreatment and rising costs [ 18 ]  . 
the introduction and spread of prostate units in hospitals would be a possible solution [ 19 ]  . to treat or not to treat : a dilemma in the adjuvant case , the presence of a microscopic positive margin ( r1 ) after surgery ( tnm stage pt2br1 , pn0 ) , although postoperative psa is undetectable , suggests the utility of immediate rt , i.e. , within 6 months after surgery . 
indeed , three recent randomised trials show a benefit of postoperative rt compared with the wait - and - see approach ( table 6 ) [ 2 , 3 , 6 ]  . 
in fact , the wait - and - see strategy with salvage rt when psa is rising is a common approach of many urologists and radiation oncologists faced with patients with evidence of extraprostatic disease and undetectable postoperative psa . 
in ogni caso , va sottolineato che la scelta di irradiare un paziente in fase postoperatoria e / o in un setting di salvataggio non sempre un processo evidence based , ma una conseguenza pragmatica di unindicazione alla chirurgia data in pazienti che non sono correttamente e / o completamente stadiati . 
una possibile soluzione potrebbe essere un vero approccio multidisciplinare in un contesto di stretta collaborazione tra chirurghi e oncologi radioterapisti , al fine di indicare pi trattamenti basati sullevidenza , per evitare trattamenti superflui ed un aumento dei costi [ 18 ]  . 
lintroduzione e la diffusione del concetto di prostate unit negli ospedali potrebbe essere una possibile soluzione [ 19 ]  . trattare o non trattare : un dilemma nel caso adiuvante , la presenza di un margine microscopico positivo ( r1 ) dopo lintervento chirurgico ( stadio tnm pt2br1 , pn0 ) , anche se il psa post - operatorio indosabile , suggerisce lutilit di immediata dellrt entro 6 mesi dopo la chirurgia . 
infatti , 3 studi randomizzati pubblicati di recente hanno mostrato un beneficio della rt post - operatoria rispetto allatteggiamento wait - and - see ( tabella 5 ) [ 2 , 3 , 6 ]  . 
in effetti , la strategia di aspettare per la rt di salvataggio quando il psa sta aumentando , un approccio comune di molti urologi ed oncologi radio672 radiol med ( 2013 ) 118 : 660678 radiol med ( 2013 ) 118 : 660678 summarises the principal results of published randomised trials . 
 updates of the southwest oncology group ( swog ) 8794 and european organization for research and treatment of cancer ( eortc ) 2291 trials evaluate other endpoints as well as biochemical improvements [ 2 , 4 ]  . 
after a re - evaluation of the pathology results obtained on the specimens , the authors stated that margin status in the rt arm was the strongest predictor of prolonged biochemical disease - free survival ( dfs )  . 
 [ 4 ] of swog 8794 , patient follow - up continued after the first report , and authors showed a significant advantage for metastasis - free survival in the rt arm ( p = 0.016 ; 93 / 214 events in the rt arm vs 114 / 211 events in observation only arm )  . 
moreover , survival was significantly higher in the experimental arm ( p = 0.023 ; 88 / 214 deaths in the rt arm versus 110 / 211 deaths in observation only arm )  . 
 this was the first report showing that postoperative rt , despite the relatively modest dose used in the late 1980s , can significantly reduce the risk of metastasis in the presence of extracapsular extension after radical retropubic prostatectomy . 
however , for patients with recurrent prostate cancer after radical prostatectomy , salvage rt remains the only potentially curative therapy , with exclusive hormonal therapies having only a limited role in tumour control and definitive cure in these patients . 
 [ 22 ] , evaluating the risk of biochemical relapse at 1 and 3 years , stated that a psa value > 0.2 ng / ml is an appropriate cutoff point to define psa recurrence after radical prostatectomy [ 22 ]  . 
that definition of recurrence was also adopted by the european association of urology ( eau ) [ 22 ]  . which staging procedure before treating ? despite several papers reporting criteria based on grading , terapisti che affrontano il paziente con evidenza di malattia extraprostatica ed psa post - operatorio non dosabile . 
la tabella 5 riassume i principali risultati degli studi randomizzati pubblicati . aggiornamenti dello studio southwest oncology group ( swog ) 8794 e dello studio european organization for the research and . 
treatment of cancer ( eortc ) 2291 sono stati recentemente pubblicati per valutare altri obiettivi , nonch per stimare i risultati biochimici a lungo termine [ 2 , 4 ]  . 
dopo una nuova valutazione dei risultati relativi ai campioni istopatologici , gli autori hanno sostenuto che lo stato dei margini chirurgici , nel braccio sottoposto a rt , era il pi forte fattore predittivo di prolungata sopravvivenza libera da malattia . 
 [ 4 ] hanno rivisto i dati dello studio swog 8794 : il follow - up continuato dopo la prima pubblicazione , e gli autori hanno mostrato un vantaggio significativo per la sopravvivenza libera da metastasi nel gruppo sottoposto alla radioterapia ( p = 0 , 016 ; 93 / 214 eventi nel braccio radioterapia contro 114 / 211 eventi nel braccio con sola osservazione )  . 
inoltre , la sopravvivenza era significativamente migliore nel braccio sperimentale ( p = 0 , 023 ; 88 / 214 morti nel braccio radioterapia contro 110 / 211 morti nel braccio della sola osservazione )  . 
questo stato il primo studio che ha dimostrato che la rt post - operatoria , nonostante la dose relativamente modesta utilizzata alla fine degli anni 80 , pu ridurre significativamente il rischio di metastasi in presenza di estensione extracapsulare dopo prostatectomia radicale retropubica . nel caso adiuvante e nel caso di salvataggio , lindicazione allirradiazione stata votata dall84 , 4% e dal 94 , 8% dei medici , rispettivamente , mostrando un alto tasso di uniformit nella scelta del trattamento tra gli oncologi radioterapisti italiani . 
per quanto riguarda la rt di salvataggio , stato pubblicato un tasso di limitata efficacia , se prescritta dopo la ricaduta del psa o per recidiva locale [ 20 , 21 ]  . 
tuttavia , nei pazienti con cancro alla prostata recidivante dopo la prostatectomia radicale , la rt di salvataggio rimane lunica terapia potenzialmente curativa , con le terapie ormonali che hanno un ruolo limitato nel controllo del tumore e nella cura definitiva di questi pazienti . 
 [ 22 ] , valutando il rischio di recidiva biochimica ad 1 anno ed a 3 anni , hanno recentemente affermato che un valore di psa superiore a 0 , 2 ng / ml un valore limite opportuno per definire la recidiva di psa dopo prostatectomia radicale [ 22 ]  . 
tale definizione di recidiva stata di recente adottata anche dalla european association of urology ( eau ) [ 22 ]  . 674 radiol med ( 2013 ) 118 : 660678 t stage , psa doubling time and disease - free period after surgery to distinguish between local and distant failure [ 23 25 ] , it remains difficult to distinguish patients with isolated local recurrence from those with occult distant metastases who are unlikely to benefit from local rt [ 23 ]  . 
 one of the principal limits of this technique is its low sensitivity when psa is < 1 ng / ml , i.e. , when the cancer burden is low but more amenable to local therapies , reducing dramatically the usefulness of this technique in studying these patients [ 24 , 25 ]  . 
endorectal mr imaging may also have a role in defining target volumes for salvage rt after prostatectomy , also because of the possibility of identifying the presence of a macroscopic local relapse and / or remnant prostatic tissue after surgery [ 27 ]  . 
thus , postoperative remnants of prostate tissue in the surgical bed could ( and should ) be included in the clinical target volume ( ctv ) [ 29 ]  . 
 what is the adequate dose and fractionation ? one of the more interesting issues in rt is the optimal dose level , which remains to be clarified in these patients . 
some reports assume that the residual tumour burden after retropubic prostatectomy would be many logarithms smaller than in the case of radical irradiation , in which a clear doseresponse effect was demonstrated [ 3032 ]  . 
even though quali procedure di staging prima di prescrivere il trattamento ? nonostante diversi studi abbiano riportato criteri basati su stadio del t , tempo di raddoppiamento del psa , e periodo libero da malattia dopo un intervento chirurgico [ 2325 ] , resta complicato distinguere tra i pazienti con recidiva locale isolata e quelli con metastasi occulte a distanza , che difficilmente potranno beneficiare di una rt locale sulla loggia prostatica [ 23 ]  . 
luso della pet - tc con 11ccolina sembra essere promettente come procedura singola di ristadiazione per i pazienti sottoposti a intervento chirurgico con un aumento del psa ; tale esame sembra superiore alla tc / pet con fluordeossiglucosio ( fdg ) ed complementare allimaging convenzionale [ 24 ]  . 
uno dei limiti principali di questa tecnica la bassa sensibilit quando il psa inferiore a 1 ng / ml , cio quando il carico di malattia basso ma pi suscettibile di terapie locali , riducendo drasticamente lutilit di questa tecnica per lo studio di questi pazienti [ 24 , 25 ]  . nel caso di salvataggio proposto ai medici nellindagine in corso , la decisione di dare una indicazione nel 94 , 8% dei casi era probabilmente pi influenzata dalla positivit dellesame pet con 11ccolina sul letto prostatico che dal solo valore di psa dopo lintervento chirurgico , anche se superiore a 0 , 2 ng / ml . la rmbobina endorettale sta guadagnando un crescente favore nella valutazione dei pazienti con recidiva biochimica dopo intervento chirurgico [ 26 ]  . 
la rm con bobina endorettale pu anche avere un ruolo nella definizione dei volumi bersaglio per la rt di salvataggio dopo prostatectomia , anche grazie alla possibilit di identificare la presenza di una recidiva locale macroscopica e / o di tessuto prostatico residuo dopo lintervento chirurgico [ 27 ]  . 
cos , i residui post - operatori di tessuto prostatico sul letto chirurgico potrebbero ( e dovrebbero ) essere inseriti nel volume bersaglio clinico ( ctv ) [ 29 ]  . 
comunque , va notato che laumento psa spesso lunico segno di recidiva , rendendo meno utili tutti questi strumenti diagnostici [ 30 ]  . quali sono le dosi e gli schemi di frazionamento adeguati ? una delle questioni pi interessanti sulla rt il livello di dose ottimale , questione che rimane da chiarire in questo tipo di pazienti . 
da alcuni studi si presume che il carico tumorale residuo dopo prostatectomia retropubica sarebbe molti logaritmi inferiore rispetto al caso di irradiazione radicale , in cui stata dimostrato una chiaro effetto doserisposta [ 3032 ]  . 
solo poche serie retrospettive , di radiol med ( 2013 ) 118 : 660678 they present some important biases ( short follow - up , limited sample size , retrospective study design ) , all studies support the idea that dose escalation could be interesting in this clinical setting . 
indeed , according to their data , it could be assumed that higher doses could potentially achieve significantly better rates of disease - free control , but there are no studies with a high level of evidence to support these conclusions . 
in our survey , the most represented prescribed doses were between 60 gy and 70 gy in 61.4% in the adjuvant case and > 70 gy in 50.8% of choices in the salvage case , showing a quite low uniformity among italian radiation oncologists . 
considering fractionation , although some evidence suggests an interesting role for hypofractionation [ 37 ] in prostate cancer in the context of exclusive radical treatment , available data for the postoperative setting are poor and less clear . 
tolerability data for pelvic rt with new rt techniques such as imrt , which reduce bowel involvement , are promising [ 4143 ] , suggesting its potential feasibility in selected cases , such as patients at high risk for regional microscopic disease . 
in this survey , radiation oncologists preferred to prescribe rt only to the prostatic bed in both cases proposed in the questionnaire , with high values of uniformity : 92.1% in the adjuvant case and 77% in the salvage case . choices about irradiation technique and control setup control are probably more related to technological possibilities available in radiation departments than to evidence from the literature . 
whereas imrt seems to determine a reduction of acute toxicity in some series of patients , especially piccole dimensioni , hanno affrontato il tema del ruolo della dose escalation nella rt adiuvante o di salvataggio [ 3335 ]  . 
 anche se presentano alcuni bias importanti ( follow - up breve , limitata dimensione del campione , disegno retrospettivo dello studio ) , tutti questi studi hanno sostenuto lipotesi che laumento della dose potrebbe essere interessante in questo contesto clinico . 
infatti , in base ai questi dati , si potrebbe presumere che dosi pi elevate potrebbero ottenere maggiori percentuali di controllo libero da malattia , ma non ci sono studi con un alto livello di evidenza che potrebbero dare un sostegno a tali conclusioni . 
 [ 36 ] che ha mostrato un guadagno proporzionale atteso di quasi il 3% per ogni incremento di un singolo gray , nella sopravvivenza libera da recidiva biochimica [ 36 ]  . 
 nella nostra indagine , i dosaggi prescritti pi rappresentati sono nel range tra i 60 gy e 70 gy nel 61 , 4% per il caso adiuvante e superiori a 70 gy nel 50 , 8% per il caso di salvataggio , delineando una uniformit ridotta tra oncologi radioterapisti in italia . 
guardando il frazionamento , bench alcune evidenze abbiano suggerito un ruolo interessante per lipofrazionamento nel cancro della prostata nel contesto del trattamento esclusivo radicale [ 37 ] , i dati disponibili per lambito post - operatorio sono scarsi e meno chiari . 
questi dati mostrano un buon tasso di consenso tra gli oncologi radiologi italiani . volumi e tecniche di trattamento per definizione , il volume bersaglio clinico per il trattamento post - operatorio di rt il letto prostatico . 
inoltre , in alcune istituzioni , linclusione dellintera pelvi potrebbe essere considerata clinicamente utile in casi selezionati ( cio dopo un linfoadenectomia limitata e / o in presenza di rischio elevato di metastatizzazione linfonodale ) , anche se non vi alcuna evidenza nella letteratura di un vantaggio clinico dellirradiazione delle regioni linfonodali pelviche in fase di rt post - operatoria . 
i dati di tollerabilit di rt pelvica con nuove tecniche di radioterapia , quali limrt , riducendo il coinvolgimento intestinale , sono promettenti [ 4143 ] , suggerendo la sua potenziale fattibilit in casi selezionati , come ad esempio nei pazienti ad alto rischio di diffusione di malattia microscopica loco - regionale . 
 in questa indagine , gli oncologi radioterapisti hanno preferito prescrivere la rt sul solo letto prostatico in entrambi i casi proposti nel questionario , con alti valori di uniformit nelle risposte : 92 , 1% nel caso in cui adiuvante e del 77% nel caso in cui salvataggio . le scelte sulla tecnica di irradiazione e del posizionamento sono probabilmente pi legati alle possibilit tecnologiche disponibili nei reparti di radioterapia oncologica rispetto alle evidenze in letteratura . 
these results confirm that the newest igrt modalities , such as cbct or other systems [ 42 ] , are still not so commonly used in clinical practice for postoperative cancer treatments . 
another possible explanation for this choice may be that these new igrt techniques are still not available in several italian radiation oncology departments . factors driving treatment choice radicale [ 43 , 44 ]  . 
sebbene la imrt sembri determinare una riduzione delle tossicit acuta in alcune serie di pazienti , soprattutto quando lintera pelvi viene trattata [ 42 , 43 ] , limpatto clinico di queste nuove tecniche di rt nel setting postoperatorio rimane comunque da definire prospetticamente . 
i nostri risultati hanno mostrato che il 69 , 5% e il 66 , 7% degli oncologi radioterapisti ha rispettivamente preferito la 3dcrt per il caso adiuvante e di salvataggio . 
posizione supina / vescica piena / retto vuoto stata la scelta preferita per il posizionamento e la preparazione dei pazienti : 82 , 5% stato il tasso di consenso in entrambi i casi clinici . 
il controllo del posizionamento stato effettuato principalmente con immagini portali settimanali ( pi ) che sono preferite rispetto ad altre tecniche di igrt , con il 64 , 5% ed il 55 , 8% delle preferenze rispettivamente nel caso adiuvante e di salvataggio . 
questi risultati hanno confermato che le modalit pi recenti di igrt , come la cb - tc o altri sistemi [ 42 ] , non sono ancora cos comunemente utilizzati nella pratica clinica per la rt post - operatoria . 
unaltra possibile spiegazione di questa scelta pu essere il fatto che queste nuove tecniche di igrt non sono ancora molto diffuse nei diversi reparti di radioterapia oncologica italiani . in our study , factors influencing treatment choices in the questionnaires were various , and a clear lack of uniformity emerged . 
none of the proposed criteria , either alone or in combination , achieved the minimum cutoff of 10% in the salvage case , whereas only disease stage , prognosis and published evidence were the most indicated criteria ( 12.5% ) in the adjuvant case . 
for these reasons , we retrospectively decided to compare four blocks of items : ( 1 ) scientific evidence ; ( 2 ) factors pertaining to disease and treatment ( risk category , prognosis , treatment toxicity ) ; fattori condizionanti le scelte terapeutiche nel nostro studio , i fattori che influenzano le scelte di trattamento nei questionari sono stati vari e una palese assenza di uniformit emersa dallanalisi dei dati . 
nessuno dei criteri proposti , da solo o associato ad un altro , ha raggiunto un di cut - off minimo del 10% in caso di salvataggio , mentre solo lo stadio della malattia assieme alla prognosi ed i dati pubblicati in letteratura sono stati i criteri pi indicati ( 12 , 5% ) nel caso adiuvante . 
per queste ragioni , abbiamo retrospettivamente deciso di fare un confronto tra 4 blocchi : radiol med ( 2013 ) 118 : 660678 ( 3 ) factors pertaining to the patient ( ps , comorbidities , age , patient comfort ) ; ( 4 ) factors pertaining to management ( waiting list , economic reasons )  . 
in both proposed cases , it is difficult to understand the reasons for this heterogeneity : considering that these patients are commonly treated in italy and that a wide evidence base is available , it would be desirable to approach these clinical situations with a more evidence - based radiotherapy . ( 1 ) evidenze scientifiche ; ( 2 ) fattori relativi alla malattia e al trattamento : categoria di rischio , prognosi , tossicit del trattamento ; ( 3 ) fattori relativi al paziente : psa , comorbilit , et , comfort del paziente ; ( 4 ) fattori relativi alla gestione : lista dattesa , motivi economici . 
in conclusione , i criteri principali che sono stati presi in considerazione sono stati i fattori relativi alla malattia ed al trattamento + i fattori relativi al pazientele evidenze scientifiche . 
in entrambi i casi proposti , difficile capire le ragioni di questa eterogeneit : considerando che questi pazienti sono ampiamente trattati in italia e che sono disponibili molti dati in letteratura , sarebbe auspicabile affrontare queste situazioni cliniche con una rt maggiormente basata sulle evidenze . conclusions conclusioni overall , this survey shows a high level of agreement amongst italian radiation oncologists in treating prostate cancer patients in an adjuvant or salvage setting . 
therefore , our data could provide the opportunity for considering the need to set up a multidisciplinary national consensus conference to summarise the evidence and solve , if possible , controversies around treating these patients both in the adjuvant and salvage settings . questindagine ha mostrato globalmente un alto livello di consenso tra gli oncologi radioterapisti italiani nel trattamento adiuvante o di salvataggio dei pazienti con tumore della prostata operato . 
cademartiri1 , 2 , 14 1dipartimento di radiologia , azienda ospedaliero - universitaria , parma , italy 2radiologia , clinica giovanni xxiii , monastier , treviso , italy 3dipartimento di radiologia , universit di palermo , palermo , italy 4dipartimento di radiologia , policlinico santorsola , universit di bologna , bologna , italy 5dipartimento di radiologia , universit di roma la sapienza polo pontino , latina , italy 6dipartimento di cardiologia e radiologia , ospedale san gennaro asl1 , napoli , italy 7cpc , ospedale san raffaele , milano , italy 8dipartimento di radiologia , azienda ospedaliero - universitaria , genova , italy 9dipartimento di cardiologia e radiologia , azienda ospedaliero - universitaria , foggia , italy 10dipartimento di cardiologia e radiologia , azienda ospedaliero - universitaria , firenze , italy 11dipartimento di radiologia , universit di verona , verona , italy 12dipartimento di radiologia , universit federico ii , napoli , italy 13dipartimento di radiologia , fondazione sdn - irccs , napoli , italy 14dipartimento di radiologia , erasmus medical center , rotterdam , olanda correspondence to : f . 
cademartiri , area cardio - vascolare , casa di cura giovanni xxiii , via giovanni xxiii 7 , 31050 monastier di treviso , italy , e - mail : filippocademartiri@gmail.com studio finanziato / sponsorizzato con fondi istituzionali di sirm , bando sirm per la ricerca per il biennio 2009 - 2010 . 
this is a retrospective observational study that began in january 2003 conducted on patients with suspected cad assessed with ctca on the basis of symptoms ( chest pain , dyspnoea ) and / riassunto obiettivo . 
scopo del presente lavoro stato valutare il valore prognostico della angiografia coronarica mediante tomografia computerizzata ( ctca ) in una ampia popolazione multicentrica di pazienti con sospetta malattia coronarica ( cad ) ed in particolare il valore incrementale rispetto ai tradizionali sistemi di stratificazione del rischio . 
questo uno studio osservazionale retrospettivo con inizio da gennaio 2003 su pazienti con sospetta cad valutati mediante ctca sulla base di sintomi ( dolore toracico , dispnea ) e / o per stress test 592 radiol med ( 2013 ) 118 : 591607 or abnormal or equivocal stress test and / or a high cardiovascular risk profile . 
exclusion criteria are renal insufficiency , allergy to iodinated contrast material , pregnancy and previous myocardial infarction or revascularisation ( percutaneous coronary intervention and / or coronary artery bypass graft )  . 
primary endpoints are death , major adverse cardiovascular events ( cardiac death , unstable angina requiring hospitalisation , acute myocardial infarction ) and shifting of cardiovascular risk category on the basis of coronary plaque burden . 
the information collected from the prognostic registry for coronary artery disease ( prorecad ) will provide insight into the prognostic value of ctca in addition to demographic and clinical features . 
the results will allow for better use and interpretation of ctca for prognostic purposes . keywords computed tomography coronary angiography coronary artery disease prevalence of disease prognosis risk stratification registry alterato o dubbio e / o per un elevato profilo di rischio cardiovascolare . 
criteri di esclusione sono : insufficienza renale , allergia al mezzo di contrasto iodato , gravidanza , pregresso infarto miocardico e rivascolarizzazione [ rivascolarizzazione coronaria percutanea ( pci ) e / o rivascolarizzazione chirurgica miocardica mediante confezionamento di bypass coronarici ( cabg ) ]  . 
gli obiettivi primari dello studio sono : morte ; eventi cardiaci avversi maggiori ( mace ) ( vale a dire , morte cardiaca , ricovero per angina instabile , infarto miocardico acuto ) ; variazione della categoria di prevalenza del rischio cardiovascolare sulla base del carico di placca coronarica . 
le informazioni raccolte dal registro di prognosi per la malattia delle arterie coronarie ( prorecad ) aggiungeranno importanti informazioni sul valore prognostico della ctca oltre alle caratteristiche demografiche e cliniche . 
i risultati consentiranno un utilizzo ed una interpretazione ottimale della ctca ai fini prognostici . parole chiave angiografia coronarica a tomografia computerizzata malattia delle arterie coronarie prevalenza di malattia prognosi stratificazione del rischio registro introduction introduzione cardiovascular disease and coronary artery disease ( cad ) are the leading causes of morbidity and mortality in industrialised countries [ 14 ]  . 
these tests [ stress electrocardiography ( ecg ) , stress single - photon emission computed tomography ( spect ) , stress echocardiography , stress magnetic resonance imaging ( mri ) ] offer many advantages but also pose numerous risks . 
moreover , these methods are unle malattie cardiovascolari e delle arterie coronarie ( cad ) sono la principale causa di morbilit e mortalit nei paesi industrializzati [ 14 ]  . 
queste modalit dindagine [ stress elettrocardiografico ( ecg ) , stress tomografia computerizzata ad emissione di singoli fotoni ( spect ) , stress ecocardiografico , stress risonanza magnetica ( rm ) ] hanno molti vantaggi ma anche molti rischi . 
in alcuni casi queste non sono fattibili , in altri possono generare falsi positivi o negativi , oppure alcune indagini non sono eseguibili radiol med ( 2013 ) 118 : 591607 able to detect subclinical atherosclerosis and only provide information when cad causes significant obstruction and / or ischaemia [ 4 ]  . 
 the introduction of the coronary artery calcium score ( cacs ) in the 1990s led to a relative simplification in the assessment of risk based on coronary calcium [ 5 ]  . 
therefore , in order to carry out adequate evaluation and correct statistical analysis of the impact of each variable , a large population of referral patients is required . rationale the project is aimed at collecting ( retrospectively ) a large population of patients with suspected cad who underwent ctca and who are adequately stratified . 
under these conditions , we can assess the absolute and incremental value of ctca in stratifying disease prevalence ( nonobstructive / obstructive ) and predict outcome in patients with suspected cad . 
 negli anni 90 , lintroduzione del coronary artery calcium score ( cacs ) ha permesso una relativa semplificazione nella valutazione del rischio del paziente basata sulla quantit di calcio coronario [ 5 ]  . 
con lintroduzione dellangiografia coronarica a tomografia computerizzata ( ctca ) stato possibile valutare lintero albero coronarico in termini di presenza di cad ( presente / assente ) , estensione ( prossimale e / o distale ) , distribuzione ( per - vaso e per - segmento ) , grado di stenosi del vaso ( < o 50% ) , composizione della cad ( calcifica , mista , non calcifica ) [ 616 ]  . 
le prime esperienze hanno dimostrato che la ctca ha un valore incrementale in termini di stratificazione del rischio , di malattia e di prognosi superiore alle altre tecniche convenzionali ( cacs , framingham , euroscore , duke , morise , diamond e forrester ) [ 1725 ]  . 
il principale ostacolo che si presenta quando tentiamo di valutare e stratificare una popolazione dipende dal fatto che il numero di pazienti e le rispettive variabili sono molteplici se confrontati con gli endpoint [ eventi cardiovascolari maggiori avversi ( mace ) ]  . 
quindi al fine di effettuare unadeguata valutazione ed una corretta analisi statistica dellimpatto di ogni variabile individuale diventa necessario disporre di unampia popolazione di pazienti di riferimento . razionale il progetto ha lo scopo di raggruppare ( con modalit retrospettiva ) unampia popolazione di pazienti con sospetta cad che siano stati sottoposti a ctca ed adeguatamente stratificati . 
poste tali condizioni , noi saremo in grado di valutare il valore assoluto ed incrementale della ctca nella stratificazione della prevalenza di malattia ( non ostruttiva / ostruttiva ) e nella prognosi del paziente con sospetta cad . 
follow - up 3 years for ct scanners 16 slices i dati sono stati raccolti dal rispettivo database istituzionale relativo ai pazienti sottoposti a ctca per sospetta cad . 594 radiol med ( 2013 ) 118 : 591607 study design and patient population criteri di inclusione generali this is a retrospective observational study ( registry of consecutive patients meeting the inclusion criteria ) of patients with suspected obstructive cad who underwent ctca . 
each centre will contribute at least 200 patients ( with complete clinical history and data sets for evaluation )  . in clinical practice , patients are referred for ctca on the basis of symptoms ( chest pain , dyspnoea on exertion ) and / or equivocal / discordant stress test results and / or high cardiovascular risk profile . 
exclusion criteria are renal failure ( creatinine clearance < 60ml / min ) , known allergy to iodinated contrast agents , unstable clinical condition , pregnancy and known cad [ previous myocardial infarction , previous revascularisation with percutaneous coronary intervention ( pci ) and / or coronary artery bypass graft ( cabg ) ]  . all patients are assessed for cardiovascular risk factors and symptoms . 
family history of heart disease symptoms are classified as absent , typical chest pain , atypical chest pain , dyspnoea and nonanginal pa the pretest cardiovascular risk is assessed using the main stratification methods ( framingham , euroscore , duke , morise , diamond and forrester )  . follow - up follow - up data are collected through outpatient visits and / or telephone interviews and / or from clinical databases of patients referral hospitals . 
follow - up3 anni per apparecchiature tc16 - strati . disegno dello studio e popolazione dei pazienti lo studio di tipo osservazionale retrospettivo ( pazienti consecutivi che rispettino i criteri di inclusione ; registro ) , in pazienti con sospetta malattia ostruttiva delle arterie coronarie e sottoposti a ctca . 
i centri partecipanti ( tabella 1 ) forniranno i dati ottenuti mediante ctca con appa recchiatura a 16 strati ( follow - up3 anni ) o superiore ( ctca con apparecchiatura a 64 slice ; follow - up12 mesi )  . 
ogni centro fornir almeno 200 pazienti ( con informazioni clinico - anamnestiche e data set completi per la valutazione )  . nella pratica clinica , i pazienti vengono inviati a ctca sulla base di sintomi ( dolore toracico , dispnea da sforzo ) e / o test stress dubbio - discordante e / o elevato profilo di rischio cardiovascolare . 
 follow - up i dati del follow - up di tutti i pazienti saranno ottenuti meradiol med ( 2013 ) 118 : 591607 table 1 participating centres number centre location role expected patients administrative and scientific coordination ; enrolment ; data analysis enrolment enrolment parma and treviso latina coordinating centers dibimel , radiology department , university of palermo palermo radiology department , sant orsola teaching hospital , bologna university radiology department , la sapienza university , polo pontino radiology and cardiology department , san gennaro hospital , asl 1 cpc cardiovascular prevention centre , irccs san raffaele hospital radiology and cardiology department , hospital of carrara carrara radiology department , la sapienza university rome radiology department , san martino university hospital genoa foggia university hospital of foggia florence university hospital careggi of florence verona university hospital of verona naples university hospital of naples total expected patients naples milan enrolment enrolment enrolment enrolment enrolment data analysis enrolment enrolment enrolment enrolment tabella 1 elenco centri partecipanti sede parma e treviso palermo pazienti attesi ruolo coordinamento amministrativo 500 e scientifico ; arruolamento ; analisi dati arruolamento 200 centro centro coordinatore dibimel , dipartimento di radiologia , universit universit degli studi dipartimento di radiologia , policlinico santorsola , universit degli studi dipartimento di radiologia , universit degli studi la sapienza , polo pontino dipartimento di radiologia e cardiologia , ospedale san gennaro , asl 1 cpc , centro prevenzione cardiovascolare , irccs ospedale san raffaele dipartimento di radiologia e cardiologia , ospedale di carrara dipartimento di radiologia , universit degli studi la sapienza dipartimento di radiologia , azienda ospedaliero universitaria san martino azienda ospedaliero - universitaria di foggia azienda ospedaliero - universitaria careggi di firenze azienda ospedaliero - universitaria di verona azienda ospedaliero - universitaria di napoli totale pazienti attesi bologna arruolamento latina arruolamento napoli arruolamento milano arruolamento carrara arruolamento roma arruolamento genova analisi dati foggia firenze verona napoli arruolamento arruolamento arruolamento arruolamento 500 200 200 200 200 2 , 700 200 200 200 200 200 200 2700 no . 
subanalyses consider the endpoints separately : mortality from all causes , hard events ( cardiac death , nonfatal myocardial infarction , unstable angina ) , revascularisations beyond 6090 days and total events . diante visita ambulatoriale e / o intervista telefonica e / o raccolta dal database clinico dellistituto di riferimento . 
morte cardiaca , 596 patient preparation prior to the examination , all patients with heart rate > 65 beats per minute ( bpm ) and no contraindications ( asthma or bronchospasm , systolic pressure < 100 mmhg , severe aortic stenosis or severely depressed ejection fraction ) [ 29 ] receive beta - blockers orally and or intravenously . 
 data acquisition with multislice computed tomography scans are performed using 16 - slice or higher ct scanners ( somatom sensation 16 - 64 cardiac , definition ds , and definition flash , siemens , forchheim , germany ; vct and ct - 750hd , gehc , paris , france ; brilliance 64 , philips , best , the netherlands ; aquilion 16 - 64 , toshiba , japan ) ( table 2 )  . 
patients first undergo a prospectively triggered coronary calcium scan with standard parameters [ 5 ]  . ctca scans are then acquired after administering 60 120 ml of nonionic contrast material at a 46 ml / s flow rate , depending on the patients characteristics ( table 3 )  . 
ctca is done with the best available parameters for each scanner ( table 2 )  . with appropriate software / hardware and whenever technically feasible ( heart rate < 60 bpm and stable sinus rhythm ) , the step - and - shoot scan protocol with prospective ecg triggering is used [ 1 ]  . 
as most data were acquired before 2009 , there is a relatively low prevalence of studies using prospective scanning in this first phase . in order to optimise image quality , data are reconstructed in the end - diastolic phase ( 450 / 300 ms before the following r wave and / or at 6080% of the r - r interval )  . 
when deemed appropriate , a reconstruction is also obtained in the end - systolic phase ( + 225 / + 325 ms after the previous r wave and / or at 2540% of the r - r interval )  . 
data sets reconstructed along the short axis are sent to a dedicated workstation to be subsequently evaluated and postprocessed . data analysis coronary artery calcium score intracoronary calcium scores are assessed using the dedicatradiol med ( 2013 ) 118 : 591607 2 . 
nelle sub - analisi verranno considerati separatamente gli endpoint : mortalit per tutte le cause , eventi hard ( morte cardiaca , infarto miocardico non fatale , angina instabile ) , rivascolarizzazioni oltre i 6090 giorni , ed eventi totali . preparazione dei pazienti prima dellesame stata effettuata la somministrazione di beta - bloccante per via orale e / o endovenosa a tutti i pazienti con frequenza cardiaca > 65 battiti per minuto ( bpm ) e in assenza di controindicazioni ( asma o broncospasmo , pressione sistolica < 100 mmhg , stenosi aortica severa o severa compromissione della frazione di eiezione ) [ 29 ]  . 
inoltre , in assenza di controindicazioni ( allergia nota , pressione sistolica < 100 mmhg ) , stata eseguita una somministrazione sublinguale di 0 , 3 mg di nitro - derivati [ 29 , 30 ]  . 
 acquisizione dei dati mediante tomografia computerizzata multislice le scansioni sono state effettuate con sistemi tc a 16 strati o superiori ( somatom sensation 16 - 64 cardiac , definition ds , e definition flash , siemens , forchheim , germania ; vct e ct - 750hd , gehc , paris , francia ; brilliance 64 , philips , best , paesi bassi ; aquilion 16 - 64 , toshiba , giappone ) ( tabella 2 )  . 
 quindi , la scansione ctca stata effettuata dopo somministrazione di 60120 ml di agente di contrasto non ionico ad una velocit di flusso di 46 ml / s sulla base delle caratteristiche del paziente ( tabella 3 )  . 
coronary plaques are defined as structures > 1 mm2 within or adjacent to the vessel lumen and clearly discernible from it , surrounded by fat and / or pericardium [ 1 , 5 ]  . 
patients are classified as belonging to one of three groups based on ctca results : ( 1 ) patients with normal coronary arteries , ( 2 ) patients with nonobstructive cad , and ( 3 ) patients with obstructive cad ( presence of at least one plaque causing stenosis 50% ) [ 21 ]  . in presenza di software / hardware adeguato e quando possibile dal punto di vista tecnico ( frequenza cardiaca < 60 bpm e ritmo stabile sinusale ) stato effettuato il protocollo di scansione step - and - shoot con triggering ecg prospettico [ 1 ]  . 
essendo i dati per lo pi risalenti al periodo antecedente al 2009 la prevalenza di studi effettuati con modalit di scansione prospettica sar relativamente bassa in questa prima fase . per ottimizzare la qualit di immagine , i dati sono stati ricostruiti in fase tele - diastolica ( - 450 / - 300 ms prima dellonda r successiva e / o al 60%80% dellintervallo rr )  . 
quando ritenuto opportuno stata effettuata anche una ricostruzione in fase tele - sistolica ( + 225 / + 325 ms dopo londa r precedente e / o al 25%40% dellinterval lo rr )  . 
i data set ricostruiti in asse corto sono stati trasferiti su una workstation dedicata per la successive valutazione ed esecuzione del post - processing . analisi dei dati coronary artery calcium score il valore di calcio intra - coronarico valutato mediante applicazione di un software dedicato associato alle rispettive radiol med ( 2013 ) 118 : 591607 atherosclerotic coronary plaques are then classified by type ( mixed , calcified , noncalcified ) , by vessel remodelling ( absent ; positive / negative ) and by axial distribution of atherosclerosis ( eccentric / concentric ) [ 1 , 26 ]  . 
values and differences are compared using students t test for paired data and analysis of variance ( anova ) if normally distributed or with the kruskalwallis method if the distribution is not normal . 
le placche coronariche sono state definite come strutture > 1 mm2 situate allinterno / o adiacenti al lu me del vaso e chiaramente distinguibili da esso , circonda te da tessuto adiposo e / o pericardio [ 1 , 5 ]  . 
le placche coronariche sono state definite come ostruttive se deter minano una riduzione di calibro del vaso 50% e non ostruttive se determinano una riduzione di calibro del vaso < 50% [ 1 ]  . 
i pazienti sono stati classificati ed inseriti allinterno di uno dei tre gruppi sulla base dei risultati della ctca : ( 1 ) pazienti con arterie coronariche normali , ( 2 ) pazienti con malattia non ostruttiva delle arterie coronarie , e ( 3 ) pazienti con malattia ostruttiva delle arterie coronarie ( presenza di una o pi placche che determinano stenosi 50% ) [ 21 ]  . le placche aterosclerotiche coronariche sono quindi state classificate per tipo ( mista , calcifica , non calcifica ) , per il rimodellamento vasale ( assente ; presente positivo / negativo ) e per distribuzione assiale dellaterosclerosi ( eccentrica / concentrica ) [ 1 , 26 ]  . 
 primary endpoints analisi statistica primary endpoints comprise : ( 1 ) death from all causes ; ( 2 ) hard events ( cardiac death , hospitalisation for unstable angina , acute myocardial infarction ) and ( 3 ) shifting of cardiovascular risk category based on coronary plaque burden . secondary endpoints secondary endpoints are : ( 1 ) mace + coronary revascularisation following ctca ( pci and cabg ) beyond 90 days ; le caratteristiche di base della popolazione , espresse come numeri e percentuali , saranno confrontate mediante il test del chi - quadrato . 
verranno messi a confronto i valori e le differenze mediante test t di student per dati appaiati , e mediante analisi della varianza se normalmente distribuiti oppure con il metodo kruskal - wallis . 
the study was approved by the ethics committee of the coordinating centre and registered at clinicaltrials . gov with the id number nct01384721 . discussion in this preliminary paper , we describe the rationale and methods of the prognostic registry for coronary artery disease ( prorecad )  . 
la sotto - analisi per la stratificazione pre - test del rischio cardiovascolare sar calcolata , in prima battuta , con lo score di morise [ 33 , 34 ]  . 
 obiettivi primari gli obiettivi secondari comprendono : ( 1 ) morte per tutte le cause ; ( 2 ) eventi hard ( morte cardiaca , ospedalizza zione per angina instabile , infarto miocardico acuto ) ; ( 3 ) variazione della categoria di prevalenza del rischio cardiovascolare sulla base del carico di placca corona rica . obiettivi secondari gli obiettivi secondari comprendono : ( 1 ) mace + rivasco larizzazione coronarica in seguito a ctca ( pci e / o cabg ) oltre i 90 giorni ; ( 2 ) prevalenza e prognosi di pazienti in base al numero di fattori di rischio ed allestensione della malattia coronarica . il database ambulatoriale / ospedaliero [ radiology information system ( ris ) - picture archiving and communications system ( pacs ) radiologico / cardiologico , cartelle cliniche , ecc . ] verr utilizzato come sorgente dei dati che verranno sempre utilizzati anonimi ed in modo aggregato ( non sar possibile risalire allidentit ed alla provenienza dei pazienti )  . 
the prorecad intends to further verify this value with an italian multicentre study and with continuing follow - up . to date , ctca has shown excellent performance in the diagnosis of inclusion and exclusion of obstructive coronary disease in patients with suspected cad [ 1 , 4 , 35 ]  . 
in recent decades , functional modalities have been extensively investigated with regard to their diagnostic and , above all , prognostic values . guidelines , diagnostic criteria and algorithms consider inducible ischaemia to be the main diagnostic and prognostic criterion that should guide subsequent treatment decisions [ 1 , 4 , 35 ]  . 
for years , validation studies were performed using electron - beam ct and mri , with suboptimal results [ 1 , 4 , 35 ] , especially in terms of clinical implementation . 
il registro prorecad intende ampliare questo concetto con uno studi multicentrico italiano e con un follow - up continuativo nel tempo . la ctca ha dimostrato fino ad ora una ottima performance diagnostica per la diagnosi di inclusione ed esclusione della coronaropatia ostruttiva nei pazienti con sospetta cad [ 1 , 4 , 35 ]  . 
inoltre , nei decenni scorsi le metodiche funzionali sono state valutate approfonditamente per quanto concerne il loro valore diagnostico ma soprattutto quello prognostico . parte delle linee guida e dei criteri e degli algoritmi diagnostici il fatto che la dimostrazione di ischemia inducibile sia il principale criterio diagnostico e prognostico che deve guidare le successive decisioni terapeutiche [ 1 , 4 , 35 ]  . 
per anni con lelectron - beam ct e con la risonanza magnetica sono stati effettuati studi di validazione con risultati sub - ottimali [ 1 , 4 , 35 ] , soprattutto nellottica di una implementazione clini ca . 
dal 2000 in avanti stata introdotta la ctca che , grazie ad una evoluzione tecnologica molto rapida , stata in grado di porsi come valida alternativa diagnosti ca per lesclusione di coronaropatia ostruttiva . 
questo dato confermato dallintroduzione di raccomandazioni di utilizzo e criteri di appropriatezza dedicati per lutilizzo della metodica . attualmente accettato che un paziente con sospetta cad e test provocativo dubbio o inconclusivo o non eseguibile possa essere sottoposto a ctca [ 1 , 4 , 35 ]  . 
questo algoritmo diagnostico anche supportato dalle raccomandazioni della societ italiana di radiologia medica [ 36 ]  . linformazione mancante fino ad ora stata quella riguardante la prognosi dei pazienti sottoposti a ctca stratificata in base alle caratteristiche dellalbero coronarico rilevate con la metodica . 
tale informazione appare promet602 radiol med ( 2013 ) 118 : 591607 2000 , ctca has undergone very rapid technological developments , establishing itself as a valuable diagnostic alternative for determining the exclusion of obstructive cad . 
this is confirmed by the introduction of recommendations for use and appropriateness criteria for this examination . today , it is widely accepted that a patient with suspected cad and equivocal , inconclusive or unfeasible provocative test should undergo ctca [ 1 , 4 , 35 ]  . 
this diagnostic algorithm is also recommended by the italian society of medical radiology [ 36 ]  . the missing information has been the prognosis of patients undergoing ctca stratified on the basis on features of the coronary trees identified . 
this information appears promising in terms of restratification compared with conventional methods for cardiovascular risk stratification and ischaemia tests . transferability to clinical practice in studies characterised by epidemiological and / or outcome assessments , analysis of a large sample of patients is required , especially if the events / endpoints are infrequent and if multivariate analyses evaluating event predictors are to be performed [ 26 , 37 ]  . 
the information gained from these studies is therefore strengthened and closer to what can really be expected from the method or test used . currently , patients who have undergone ctca are routinely referred for cardiological assessment regardless of ctca findings . 
 on the basis of the results of our study , operators will be able to better interpret ctca images and , in particular , each patients cardiovascular risk category according to the presence , extent , severity and type of atherosclerotic plaque ( noncalcified , mixed , calcified )  . 
this will improve stratification of the single patient into cardiovascular risk categories and enable referring physicians to use this information to end the diagnostic workup , initiate specific treatment or proceed with further investigations . potential impact the potential impact of our study on the management of patients with suspected cad is both simple and revolutionary . 
la multicentricit favorisce anche la trasferibilit dei risultati nella pratica clinica in quanto le differenze di expertise , tecnologia , logistica dei vari centri si focalizzano su end - point comuni . 
linformazione ricavata da questi studi ne risulta rafforzata e pi vicina a quello che realmente ci pu aspettare dalla metodica o dal test utilizzato . attualmente , i pazienti sottoposti a ctca vengono inviati di routine a valutazione cardiologica indipendentemente dal risultato della stessa ; valutazione che potrebbe essere non necessaria qualora lo studio dimostrasse lassenza di cad e quindi una marcata riduzione del rischio di eventi cardiovascolari futuri ( pari a circa lo 0% )  . 
 gli operatori , sulla base dei risultati del nostro studio , saranno in grado di fornire una miglior interpretazione delle immagini ed in particolare della categoria di rischio cardiovascolare di ogni paziente sulla base della valutazione di presenza , estensione , grado di severit , e tipo di placca aterosclerotica ( non calcifica , mista , calcifica )  . 
 sar possibile effettuare una pi corretta stratificazio ne del singolo paziente allinterno della categoria di rischio cardiovascolare e di conseguenza i medici di riferimento potranno utilizzare tale informazione per considerare concluso il percorso diagnostico , promuovere un determinato trattamento medico o proseguire con unulteriore indagine . impatto potenziale il potenziale impatto del nostro studio sulla gestione del paziente con sospetta cad semplice ed allo stesso tempo rivoluzionario . 
i pazienti precedentemente dimessi con valutazione di rischio cardiovascolare intermedio / eleva to e riscontro alla ctca di coronarie indenni da malattia aterosclerotica ( bassa / molto bassa probabilit di even ti cardiovascolari futuri ) non verranno sottoposti ad ulteriori indagini o trattamenti , se non in caso di sintomi specifici di nuova insorgenza . 
mentre , i pazienti dimessi con valutazione di rischio cardiovascolare intermedio / basso ed elevata / molto elevata probabilit di eventi cardiovascolari futuri alla ctca ( pazienti con cad estesa , ostruttiva e / o predominanza di placche non calcifiche ) verranno sotradiol med ( 2013 ) 118 : 591607 fig . 
in the preliminary population of the prorecad registry , the prevalence of patients with healthy coronary arteries is 36% , that of patients with nonobstructive atherosclerosis is 43% and that of patients with obstructive cad is 22% . 
cad , coronary artery disease ; ctca , computed tomography coronary angiography ; omt , optimal medical therapy ; rf , risk factors ; 3vd , 3 - vessel obstructive disease ; lm , obstructive disease of the left main trunk ; cag , conventional coronary angiography ; prev . , prevalence of patients fig . 
nella popolazione preliminare del registro prorecad la prevalenza di pazienti con coronarie indenni del 36% , quella di pazienti con aterosclerosi non ostruttiva del 43% e quella di pazienti con cad ostruttiva del 22% . 
 considerazioni specifiche sulla popolazione italiana lo studio prorecad , sar in grado di fornire informazioni specifiche sulla popolazione italiana in merito alla distribuzione di malattia ed al rischio di eventi . 
questa valutazione sar inoltre completata dalla possibilit di studiare i differenti profili di rischio in relazione alla provenienza geografica dei pazienti . vantaggi e limitazioni intrinseche dello studio lo studio prorecad uno studio finanziato dalla socieradiol med ( 2013 ) 118 : 591607 limitations susceptibility to ( inclusion ) bias nonrandomised participation nonconsecutive enrolment unmeasurable confounders incomplete follow - up lower data quality ( heterogeneity and completeness ) incomplete data unreliable conclusions about treatment effects unbalanced comparisons unreliable risk adjustment suscettibilit ai bias ( di inclusione ) partecipazione non randomizzata arruolamento non consecutivo fattori di confondimento non misurabili follow - up incompleto ridotta qualit dei dati ( eterogeneit e completezza ) dati incompleti conclusioni non affidabili su effetto terapie confronti non bilanciati aggiustamento del rischio non affidabile table 5 characteristics of cardiovascular imaging registries 604 advantages inclusion of a wide spectrum of patients inclusion of a large number of patients over short periods of time multivendor ( with regard to technology and therapies ) multicentric , with greater number of participating centres generalisability of results higher statistical power in subgroups long enrolment periods long - term follow - up possible safety studies possible lower cost than rcts shorter duration than rct suitable for data mining linkage with other data sources possible evaluation of new treatments possible comparative evaluation of effectiveness postmarketing surveillance evaluation of treatment compliance evaluation of good clinical practices evaluation of adherence to guidelines evaluation of quality of care monitoring of changes in practice and outcomes over time tracking effects on surrogate endpoints over time and their clinical consequences rct , randomised controlled trial . 
modificato da [ 37 ] vantaggi limitazioni inclusione di un ampio spettro di pazienti inclusione di un numero elevato di pazienti in tempi brevi multi - vendor ( per quanto attiene alla tecnologia ed alle terapie ) multi - centrici con maggior numero di centri arruolabili generalizzabilit dei risultati maggiore potenza statistica nei sotto - gruppi lunghi periodi di reclutamento possibilit di follow - up a lungo termine possibilit di studi di sicurezza costi inferiori ai rct tempi inferiori ai rct adatti al data mining collegabili ad altre fonti di dati possibilit di valutare nuove terapie valutazioni comparativa di effectiveness sorveglianza post - marketing valutazione della compliance terapeutica valutazione della buona pratica clinica valutazione aderenza alle linee guida valutazione qualit dellassistenza valutazione dei cambiamenti della pratica e degli outcomes nel tempo valutazione degli effetti su endpoint surrogati nel tempo e sulle loro conseguenze cliniche rct , trial controllati randomizzati . 
 [ 37 ] advantages and inherent limitations the prorecad study is funded by the italian society of medical radiology and uses technologies from all major t italiana di radiologia medica che utilizza tecnologie di tutti i maggiori produttori industriali di apparecchiature e mezzi di contrasto . 
other advantages intrinsic to the operating mode of this registry include greater ease of implementation , shorter duration and larger number of recruitable patients with relatively long follow - up compared with a randomised controlled trial ( rct )  . 
all objectives being equal , a registry study costs at least ten times less than an rct . a tutte le macchine presenti sul territorio ( table 5 ) [ 26 ]  . 
 tra gli altri vantaggi intrinseci in relazione alla modalit operativa del registro vi sono : la maggiore agilit dello studio , i tempi contenuti ed il numero elevato di pazienti arruolabili con follow - up relativamente lunghi se paragonati al potenziale di un trial randomizzato controllato ( rct )  . 
 a parit di obiettivi un registro costa almeno dieci volte meno di un analogo rct . conclusions the prorecad will provide information on the absolute and incremental prognostic value of ctca in the italian population . acknowledgements we thank the following people for their help with data collection : erica maffei and radiographer chiara martini , radiology department , university hospital of parma ; ludovico la grutta and giovanni gentile , dibimel , radiology department , university of palermo ; luigi lovato and giovanni rinaldi , radiology department , santorsola teaching hospital , university of bologna ; caruso and bellini , radiology department , la sapienza university , rome , polo pontino , latina ; roberto de rosa and gennaro ratti , radiology and cardiology department , san gennaro hospital , naples ; manuela giglio , cpc san raffaele hospital , milan ; alessandra zuccarelli , tito torri , and piercarlo rossi , radiology and cardiology department , hospital of carrara ; bettina conti and ilaria iampieri , radiology department , la sapienza university , rome ; margherita castiglione morelli , university hospital san martino , genoa ; david antoniucci and manlio acquafresca , university hospital careggi , florence ; stefania daniele , istituto di biostrutture e bioimagini , consiglio nazionale delle ricerche , naples . conclusioni il registro prorecad fornir informazioni sul valore prognostico assoluto ed incrementale della ctca nella popolazione italiana . ringraziamenti si ringraziano le persone seguenti per collaborazione nella raccolta dati : dr.ssa erica maffei e tsrm chiara martini , dipartimento di radiologia , azienda ospedaliero - universitaria di parma ; dr . 
gennaro ratti , dipartimento di radiologia e cardiologia , ospeda le san gennaro , napoli ; dr.ssa manuela giglio , cpc ospedale san raffaele , milano ; dr.ssa alessandra zuccarelli , dr . 
piercarlo rossi , dipartimento di radiologia e cardiolo gia , ospedale di carrara ; dr.ssa bettina conti e dr.ssa ilaria iampieri , dipartimento di radiologia , universit la sapienza di roma ; dr.ssa margherita castiglione morelli , azienda ospedaliero - universitaria san martino , genova ; dr . 
twenty - two corpses including six cases of fresh - water drowning ( group a ) and 16 deaths by other causes ( group b ) , among which were also different forms of mechanical asphyxia other than drowning , underwent mdct and conventional autopsy . 
mdct , together with conventional autopsy , may contribute to the diagnosis of drowning , by measuring blood density in the heart chambers . keywords multi detector row computed tomography virtual autopsy drowning riassunto obiettivo . 
sono stati sottoposti a tcms ed esame autoptico convenzionale 22 cadaveri , di cui 6 morti per annegamento in acqua dolce ( gruppo a ) e 16 per altre cause ( gruppo b ) , tra le quali erano presenti anche asfissie meccaniche diverse dallannegamento . 
la tcms pu essere impiegata per la misura della densit ematica nelle camere cardiache per la diagnosi di morte da annegamento in acqua dolce in ausilio allesame autoptico convenzionale . parole chiave tomografia computerizzata multistrato autopsia virtuale annegamento 680 introduction in recent years , the usefulness of virtual autopsy , together with conventional autopsy , has become clear [ 16 ]  . 
conventional macroscopic autopsy criteria used are multiorgan hyperaemia , increased blood flow , abundant hypostases , detection of fluid in the airways or lungs , lung hyperinflation , fluid in paranasal sinuses , water in the gastric cavity , dilation of cardiac chambers and great vessels and haemodilution [ 711 ] , together with pulmonary hyperaeria and hyperhydria and emphysema at histological examination . 
haemodilution in the case of fresh - water drowning , as in the cases in this study , is due to water absorption through the airways inside the alveolar cavities and then inside the pulmonary venules , causing reduced blood density first of the small and then of the large circulation [ 12 ]  . 
 because of the direct communication between the left chambers of the heart and the alveoli , this phenomenon will be more evident in the left than in the right chambers . 
 when a death by drowning is suspected , during conventional autopsy , the difference of blood density between heart chambers is usually determined by using the blotting - paper test or the freezing - point test after taking a small amount of blood from the heart chambers . 
the purpose of our study was to verify the role of multidetector computed tomography ( mdct ) performed before conventional autopsy in measuring the difference in blood density inside the right and left heart chambers . 
if confirmed , this would be further proof of the cause of death and may become an alternative diagnostic procedure to classic cadaver dissection . materials and methods from january to september 2011 , 22 corpses ( 4 females , 18 males ) transported for forensic investigation to the institute of legal medicine of our university hospital and then autopsied on behalf of the judicial authority underwent mdct imaging . 
during autopsy , in the case of a body found in water , the blottingpaper test was used . radiol med ( 2013 ) 118 : 679687 introduzione limpiego dellautopsia virtuale , accanto allautopsia convenzionale , negli ultimi anni ha confermato sempre di pi la propria utilit [ 16 ]  . 
i criteri autoptici macroscopici tradizionalmente impiegati a tale scopo sono : iperemia poliviscerale , aumentata fluidit del sangue , ipostasi abbondanti , riscontro di fluido nelle vie aeree o nei polmoni , iperinflazione polmonare , fluido nei seni paranasali , acqua nel la cavit gastrica , dilatazione delle camere cardiache e dei grossi vasi ed emodiluizione [ 711 ] ; ad essi si aggiunge il quadro istologico di iperaeria e iperidria polmonare associata a enfisema . 
il fenomeno dellemodiluizione nei ca si di annegamento in acqua dolce , ossia quelli qui esami nati e ai quali si far sempre riferimento , avviene per riassorbimento del liquido che entra nelle vie aeree , e quindi nelle cavit alveolari , dai capillari polmonari , provocan do una riduzione della concentrazione del sangue allinterno del piccolo circolo e successivamente del grande circo lo [ 12 ]  . 
 tale fenomeno risulter maggiore nelle camere cardiache di sinistra che direttamente comunicano con le cavit alveolari , rispetto alle camere cardiache di destra con conseguente differenza di densit del sangue al loro interno . 
 nel sospetto di morte per annegamento , durante lesame autoptico viene convenzionalmente verificata la differenza di concentrazione tra sangue del piccolo e del grande circolo mediante prova emocartometrica o verifica del punto di congelamento dopo il prelievo di una piccola quantit di sangue dalle cavit cardiache . 
questa prova , sebbene sia considerata criterio utile alla diagnosi finale , non risulta sempre fattibile a causa della difficolt del prelievo del sangue dalle cavit cardiache e dei fenomeni putrefattivi che possono occorrere . 
obiettivo del nostro studio quello di verificare se la tomografia computerizzata multistrato ( tcms ) effettuata prima dellautopsia convenzionale possa dimostrare la differenza di concentrazione tra sangue delle cavit di destra e di sinistra , tramite misurazione della densit ematica al loro interno . 
ci , se confermato , risulterebbe ulteriore elemento probatorio della causa di morte e potrebbe proporsi quale procedura diagnostica , se del caso , alternativa alla classica sezione cadaverica . materiali e metodi da gennaio a settembre 2011 sono stati sottoposti a esame tcms 22 corpi ( 4 femmine , 18 maschi ) trasportati per accertamenti forensi allistituto di medicina legale della noradiol med ( 2013 ) 118 : 679687 study group a the study group ( group a ) comprised six drowned corpses ( 2 females , 4 males )  . 
all the bodies were found in fresh water , and the diagnosis of death by drowning was made after conventional autopsy together with the search for diatoms ( unicellular organisms provided with a silica skeleton , ubiquitously distributed in water ) in lung tissue and sternal bone marrow . 
at the unit of legal medicine of verona , this investigation is considered crucial for the differential diagnosis , even in corpses discovered in water [ 13 , 14 ]  . 
 control group b the control group ( group b ) comprised the remaining corpses ( 2 females , 14 males ) of people who died due to causes other than drowning ( table 1 )  . 
images were obtained from the skull to the pelvis with the following scanning parameters : 120 kvp , 200 ma , collimation 61.5 m reconstruction slice thickness was 2 mm , with a 1 - mm interval . 
examination time was < 5 min in all cases . image analysis blood density was measured three times within the right ventriculum and atrium , left ventriculum and atrium , thoracic aorta and pulmonary trunk by positioning a region of interest ( roi ) , taking care to cover the maximum area and avoid cardiac or vascular walls . 
the time taken for this task was approximately 10 min 2 / 6 drowned corpses and in 4 / 16 corpses dead from other causes , measurement was not possible because of the absence of a sufficient amount of blood within the cavity . 
we also compared blood density values of the different cardiac chambers within groups a and b . statistical analysis statistical analysis was performed using a statistical software package ( graphpad prism 5 for windows )  . 
nel corso di autopsia , in caso di corpo rinvenuto in acqua , stato eseguito il test emocartometrico . gruppo di studio a il gruppo di studio ( gruppo a ) costituito da 6 morti per annegamento ( 2 femmine , 4 maschi )  . 
tutti i corpi sono stati rinvenuti in acqua dolce e la diagnosi di morte per annegamento stata fatta dopo esame autoptico convenzionale unitamente a ricerca delle diatomee nel tessuto polmonare e nel midollo osseo sternale ; tale indagine , presso lunit operativa complessa di medicina legale di verona considerata dirimente nella diagnosi differenziale nei casi di rinvenimento di cadavere in acqua [ 13 , 14 ]  . 
 gruppo di controllo b il gruppo di controllo ( gruppo b ) formato dai rimanenti 16 cadaveri ( 2 femmine , 14 maschi ) , morti certamente per cause diverse dallannegamento ( tabella 1 )  . 
let media era di 52 anni ( range 178 anni )  . imaging tutti i corpi inclusi nello studio sono stati sottoposti a indagine tcms a 64 strati ( brillance ct , philips , best , olanda ) con tempo di rotazione di 0 , 75 secondi . 
lo studio stato esteso dalla teca cranica alla pelvi con scansione a 120 kvp , 200 ma , e collimazione di 61 , 5 m stato utilizzato uno spessore di ricostruzione di 2 mm , con un intervallo di ricostruzione di 1 mnei casi in cui venissero sospettate fratture degli arti inferiori o la morte fosse avvenuta in seguito a un evento traumatico , sono stati inclusi nella scansione anche gli arti inferiori . 
il tempo impiegato per lesecuzione della scansione stato in tutti i casi inferiore a 5 minuti . analisi delle immagini per ogni corpo sono state effettuate tre misurazioni della densit del sangue , rispettivamente allinterno di : atrio e ventricolo di destra , atrio e ventricolo di sinistra , aorta 682 radiol med ( 2013 ) 118 : 679687 table 1 causes of death of corpses who underwent multidetector computed tomography ( mdct ) and conventional autopsy cause of death drowning asphyxia aortic dissection ab ingestis asphyxia polytrauma polytrauma splenic injury abdominal trauma alcohol intoxication myocardial infarction acute respiratory failure in silicosis charred body cocaine overdose drowning asphyxia hanging asphyxia strangulation asphyxia cerebellar hemorrhage drowning asphyxia myocardial infarction traumatic head injury by gunshot traumatic head injury by gunshot drowning asphyxia drowning asphyxia drowning asphyxia tabella 1 cause di morte dei cadaveri sottoposti a esame tcms ed esame autoptico causa di morte asfissia da annegamento morte naturale dissezione aortica asfissia neonatale ab ingestis politrauma con lesioni viscerali politrauma con lesioni viscerali trauma addominale lacerazione splenica intossicazione da alcol morte naturale infarto miocardico acuto insufficienza respiratoria acuta in antraco - silicosi cadavere carbonizzato overdose da cocaina asfissia da annegamento asfissia da impiccamento asfissia da strangolamento morte naturale emorragia cerebellare asfissia da annegamento morte naturale infarto miocardico acuto trauma cranico da colpo di arma da fuoco trauma cranico da colpi di arma da fuoco asfissia da annegamento asfissia da annegamento asfissia da annegamento results comparison of blood density values between groups a and b mean blood density measured within right atrium and ventriculum , left atrium and ventriculum and aorta was lower in toracica e tronco polmonare . 
le misurazioni sono state effettuate posizionando una region of interest ( roi ) allinterno di tali strutture , coprendo la maggior area possibile , e prestando attenzione a non includere pareti cardiache o vasali . 
in 2 cadaveri , su 6 morti per annegamento , e in 4 cadaveri , su 16 morti per altre cause , non stato possibile effettuare le misure a causa dellassenza di una quantit sufficiente di sangue allinterno delle cavit . 
sono stati inoltre paragonati tutti i valori di densit ematica tra le camere cardiache di destra e sinistra allinterno dei gruppi a e b . analisi statistica lanalisi statistica stata effettuata con software dedicato ( graphpad prism 5 per windows )  . 
il livello di significativit statistica scelto stato del 5% . risultati confronto valori di densit ematica tra gruppo a e gruppo la densit media del sangue misurata rispettivamente allinterno di atrio e ventricolo di destra , di atrio e ventricolo di sinistra , e dellaorta risultata inferiore nel gruppo a rispetto al gruppo b ( tabella 2 )  . 
 confronto valori di densit ematica allinterno dei gruppi a e b sono stati confrontati i valori di densit ematica allinterno delle camere cardiache di destra e sinistra allinterno dei due gruppi ( tabella 3 )  . 
1a - c densit ematiche misurate allinterno di atrio di destra e di sinistra in un morto per annegamento in sezione assiale ( a ) e sagittale ( b )  . 
c prova emocartometrica eseguita sullo stesso cadavere che conferma la densit ematica superiore nelle camere di destra rispetto a quelli di sinistra . group a than in group b ( table 2 )  . 
 discussione comparison of blood density values within groups a and b blood density values measured inside the right and left cardiac chambers were compared within each group ( table 3 )  . 
2a , b blood - density values measured inside right and left atrium of a corpse dead by causes other than drowning : axial ( a ) and coronal ( b ) images . 
2a , b densit ematiche misurate allinterno di atrio di destra e di sinistra in un morto non per annegamento in sezione assiale ( a ) e coronale ( b )  . 
for this reason , conventional autopsy findings ( such as the blotting - paper test ) must be complemented with laboratory tests , such as the search for diatoms , which can confirm or refute the diagnosis of drowning [ 12 , 13 ]  . the scientific role of imaging techniques in forensic pathology has been widely demonstrated [ 17 ] , and the use of imaging techniques such as mdct and magnetic resonance imaging ( mri ) is now available in most institutions . 
these imaging findings are fluid level in the paranasal and nasal sinuses , fluid in the subglottic trachea and main bronchi , ground - glass lung opacity , gastric distension with copious amounts of liquid and haemodilution . 
the underlying pathophysiological mechanism of death by fresh - water drowning is the entrance of water into the alveolar cavity , the following dilution of the surfactant and the passage of water from the alveoli to the pulmonary capillaries , causing haemodilution , hypervolaemia , hyponatraemia , hyperkalaemia , and haemolysis [ 17 ]  . 
in the case of saltwater drowning , because of the hypertonicity of the water compared with pulmonary circulation blood , the phenomenon will be the opposite , with consequent haemoconcentration , hypovolaemia and hypernatraemia . 
a lower blood density in corpses dead from fresh - water drowning compared with those dead from other causes has already been demonstrated by christe [ 16 ] , and this phenomenon would reflect general haemodilution due to the passage of water from alveoli to the small and then large circulation . 
 ra sono : livello fluido nei seni nasali e paranasali , fluido nella trachea sottoglottica e nei bronchi principali , opacit polmonari a ground glass , distensione gastrica con abbondante quantit di liquido ed emodiluizione . 
il meccani smo fisiopatologico alla base della morte per annegamento in acqua dolce consiste nellingresso di acqua allinterno delle cavit alveolari , successiva diluizione del surfattante per il passaggio di acqua dolce dagli alveoli ai capilla ri polmonari causando emodiluizione , ipervolemia , iponatremia , iperkaliemia ed emolisi [ 17 ]  . 
nel caso di annegamento in acqua salata , a causa dellipertonicit della stessa rispetto al sangue sito allinterno del circolo polmonare , il fenomeno sar lopposto con conseguente emoconcentrazione , ipovolemia e ipernatremia . 
una minore densit ematica nei morti per annegamento in acqua dolce rispetto ai morti per altre cause stata gi dimo strata da christe [ 16 ] e questo fenomeno rispecchiereb be lemodiluizione generalizzata che si ha per il passag gio dagli alveoli al piccolo circolo e quindi al grande circolo . i nostri risultati ( tabelle 2 , 3 ) confermano tale fenomeno poich nel gruppo a ( morti per annegamento in acqua dolce ) tutti i valori di densit misurati , eccetto quelli ricavati nel tronco polmonare , sono inferiori rispetto agli stessi valori misurati nel gruppo b . 
su questo fenomeno si basa limpiego del test emocartometrico 686 radiol med ( 2013 ) 118 : 679687 our results ( tables 2 and 3 ) are consistent with the literature , as all density values measured in group a ( corpses dead from drowning ) , except those measured in the pulmonary trunk , were lower than those in group b . 
furthermore , in the case of drowning in fresh water , haemodilution will be greater in the left cardiac chambers , which are in direct communication with the alveolar cavities , than in the right cardiac chambers . 
this phenomenon is exploited by the blotting - paper test and the freezing - point test carried out after removal of a small amount of blood from the cardiac chambers during conventional autopsy . 
in the case of freshwater drowning , the blood contained inside the right cardiac chambers will expand less on blotting paper or will freeze earlier , whereas in the case of saltwater drowning , the blood will expand more and freeze later . 
the performance and reliability of these tests are influenced primarily by the possibility of finding blood in the cardiac chambers , aorta and pulmonary trunk , and secondarily by postmortem putrefaction . 
therefore , with this study we proposed to determine the role of mdct in the analysis of blood density within the four cardiac chambers , the aorta and the pulmonary trunk in corpses dead from drowning , comparing values with those of corpses dead from other causes . 
this phenomenon was more evident when considering blood density within the atrial chambers than within the ventricular chambers , which may be due to putrefactive phenomena that , as already reported , occur earlier within the ventricle [ 1113 ]  . 
 the results of our study suggest that the detection of lower blood density in the left atrium compared with the right atrium could be considered a significant additional finding for the diagnosis of death by drowning , as obtained from macroscopic evidence and the blotting - paper test during autopsy , as well as from the search for diatoms . 
the main limitation of this study is the small sample of deaths by drowning . e della verifica del punto di congelamento dopo prelievo di una piccola quantit di sangue dalle cavit cardiache allesame autoptico convenzionale . 
in caso di annegamento in acqua dolce , il sangue contenuto allinterno delle cavit di destra si espander meno su carta assorbente o congeler prima ; in caso invece di annegamento in acqua di mare , il sangue destro si espander di pi e congeler successivamente . 
esecuzione e affidabilit di tali test sono condizionati in primis dalla possibilit di reperire sangue nelle cavit cardiache e nei tronchi principali , in secondo luogo dai fenomeni putrefattivi postmortali . 
con questo studio , abbiamo quindi voluto verificare il contributo della tcms nellanalisi della densit del sangue allinterno delle quattro camere cardiache e di aorta e tronco polmonare in un gruppo di morti per annegamento in acqua dolce confrontando i valori con un gruppo di morti per altra causa . 
la densit ematica misurata risultata effettivamente inferiore nel gruppo dei morti annegati rispetto al gruppo dei morti per altra causa e tale differenza risultata statisticamente significativa in atrio e ventricolo di sinistra . 
tale fenomeno risultato pi evidente andando a considerare le misure di densit allinterno delle camere atriali rispetto a quelli delle camere ventricolari e ci pu essere dovuto a fenomeni putrefattivi che , come gi dimostrato , risultano pi precoci allinterno del ventricolo che nellatrio [ 1113 ]  . 
secondo quanto ricavato da questo studio potrebbe essere possibile affermare che il riscontro di densit inferiori nellatrio di sinistra rispetto a quello di destra pu essere considerato un rilievo aggiuntivo alla conclusione della diagnosi di morte , cos come ricavato dalle evidenze macroscopiche e dalla prova emocartometrica in sede autoptica , nonch dalla conferma della ricerca di diatomee . 
limite di questo studio lesiguit del campione della popolazione dei morti per annegamento . conclusioni conclusions the use of mdct in association with conventional autopsy may be helpful in diagnosing death by drowning . 
although we cannot state with certainty that the virtual autopsy can replace conventional postmortem examination , it is possible to hypothesise that it could be a reliable complement to enhance diagnostic sensitivity . 
it is more than a concise , updated text about the fascinating world of radiology ; as stated in di guglielmos introduction and cardinales preface , radiology is not a static branch of medicine , but an ever changing , magmatic matter flowing like the ticino river ( sometimes at an easy pace , sometimes very rough ) in pavia . 
 the subject requires a very precise and thorough presentation in order to offer the user the correct diagnostic tools and the ensuing correct diagnostic results , stressing that , what is up to date today may be downgraded out of date tomorrow . 
in each chapter , page sides are highlighted with a different colour to facilitate identification when one peruses the book . chapters are organised in such a way as to follow a balanced lay - out : technology and diagnostic procedures , radiological anatomy and basic knowledge of radiological semeiotics . the reader is then led by hand through the possible and most suitable procedure / s in order to work out a diagnostic problem avoiding unnecessary , more expensive and dangerous solutions in terms of radiation or contrast media exposure . questo volume stato pensato , non solo per gli studenti di medicina , ma anche per gli specializzandi in radiologia ed in extenso per i medici generici . 
pu essere considerato qualcosa di pi di un testo conciso e ben aggiornato sullaffascinante mondo della radiologia : come affermato dal di guglielmo nella sua introduzione e dal cardinale nella prefazione , la radiologia non una branca statica della medicina , ma una materia in continuo , magmatico cambiamento che scorre , con flusso talora tranquillo , talora molto impetuoso come il fiume ticino attraverso pavia . largomento richiede una disanima molto precisa e puntuale , tale da presentare al lettore gli strumenti diagnostici corretti ed i conseguenti risultati diagnostici corretti , mettendo ben in evidenza come ci che oggi sembra moderno ed aggiornato pu essere del tutto desueto ed inutile domani . 
 dopo questa precisazione , ben comprensibile come il volume sia stato pianificato e preparato . facendo seguito alle precise generalit ( descrizione di tutte le modalit radiologiche , dalla radiologia tradizionale alla protezionistica , passando attraverso i mezzi di contrasto , la tomografia e la tac , gli ultrasuoni , la risonanza magnetica , la medicina nucleare ecc . , discutendone i loro principi generali ) ed alla sistematica ( con la spiegazione di come un approccio diagnostico debba essere pianificato attraverso la conoscenza dellanatomia e della semeiotica radiologica ) il lettore trover i successivi 10 capitoli . 
 questi capitoli trattano gli apparati locomotore , respiratorio , cardio - vascolare , digerente ed urinario , la senologia , la radiologia interventistica , gli organi delladdome superiore , lodontostomatologia e la neuroradiologia . 
i bordi delle pagine di ciascun capitolo sono caratterizzati da un colore diverso , cos da facilitarne lidentificazione da parte del lettore del volume . i capitoli sono organizzati in modo tale da seguire unimpostazione ben bilanciata : tecnologia e procedure diagnostiche , anatomia radiologica e conoscenze di base della semeiotica radiologica . 
 il lettore poi accompagnato per mano attraverso la / e procedura / e possibile / i e pi indicata / e allo scopo di risolvere uno specifico problema diagnostico , evitando soluzioni radiol med ( 2013 ) 118 : 700701 as stated above , this 363 - page book has been designed for medical students : in view of this , only the essentials of radiology are presented in a very clear and precise way by di guglielmo and his large group of co - authors most of whom are from the university of pavia institute of radiology . 
the text is thus easy and pleasant to read and enriched by a very large number of beautiful , well reproduced images ( i only have doubts about some of these in the odontostomatology chapter ) , made even more clear by very useful , broad arrows and by precise figure cap tions . i am sure that not only students ( who are invited to study with the last words buon studio of the preface ) but also trainees in radiology , general practitioners and even clinicians from different branches of medicine , who might not have a clear idea about which imaging modality / ies may better clarify their patients problem , will derive great advantage by expanding their knowledge on the topic , most of all in these days of expenditure cuts . the few misprints encountered in the text will surely be corrected in a future , well deserved second new edition of the book . 
 inutili , pi costose e pericolose in termini di esposizione alle radiazioni o ai mezzi di contrasto . come riportato sopra , questo volume di 363 pagine stato progettato per gli studenti di medicina : proprio per questo gli elementi essenziali della radiologia sono presentati in modo molto chiaro e preciso dal di guglielmo e dal suo ampio gruppo di collaboratori , per la maggior parte dallistituto di radiologia delluniversit di pavia . 
il testo dunque facile e piacevole da leggere , arricchito da un gran numero di immagini molto belle e ben riprodotte ( anche se ho alcune riserve per alcune immagini del capitolo sullodontostomatologia ) , figure rese ancora pi chiare dalluso di utili ed evidenti frecce e da precise didascalie delle figure . 
valore medio di volume , distanza mesiodistale ed apico - coronale sono nel gruppo controllo rispettivamente 703 , 2185 , 3 mm3 , 28 , 69 , 4 mm e 252 , 84 mm ; nel gruppo test , invece , sono 738 , 2189 , 2 mm3 , 27 , 53 , 6 mm e 25 , 32 , 97 mriguardo a tali misure , non si osserva differenza significativa tra i gruppi . 
i valori di intensit significativamente 524 radiol med ( 2013 ) 118 : 523533 value of treatment with biomaterials to obtain earlier bone regeneration . pi elevati nel gruppo test , documentano la validit del trattamento con biomateriali per una rigenerazione ossea pi precoce . keywords multidetector computed tomography jaw osteointegration biocompatible materials cysts jaw parole chiave tomografia computerizzata multidetettore mandibola osteointegrazione materiali biocompatibili cisti mandibolari introduction introduzione bone physiologically undergoes a constant and balanced process of resorption and neoformation of organic and inorganic matrix [ 1 ]  . 
numerous studies have investigated bone regeneration at sites of pathological bone defects in the jaw , contributing to the development of new surgical procedures involving the use of bone grafts and to changes in treatment planning [ 2 ]  . autologous bone is the best grafting material on account of its high osteogenic , osteoconductive and osteoinductive properties [ 2 , 3 ] ; however , bone harvesting requires an invasive procedure , and often a second surgical access at the donor site may be necessary [ 4 ]  . 
the use of heterologous material and , in particular , bovine bone , for filling the different types of jaw bone defects , such as cysts [ 5 , 6 ] , defects following second and third molar extraction and periodontal and iatrogenic bone defects , is a valuable therapeutic approach that provides excellent bone regeneration , as documented by densitometric assessment of the cavity with computed tomography ( ct ) [ 68 ]  . 
in this regard , ct dentascan is capable of documenting the quality and density of available bone [ 9 ]  . in this study , we selected acquired jaw bone defects developing on the vestibular and lingual walls , which remained intact though thinned due to the synthesis of osteolytic cytokines by the cyst [ 10 ]  . 
the purpose of the study was to perform a clinical and radiological evaluation of the regenerative effects of deproteinised bovine bone following excision of jaw cysts by comparing patients treated with deproteinised bovine bone ( test group ) and patients allocated to spontaneous healing ( control group )  . materials and methods study population il tessuto osseo fisiologicamente soggetto a costanti ed equilibrati processi di riassorbimento e neoapposizione di matrice organica ed inorganica [ 1 ]  . 
negli ultimi anni , la rigenerazione ossea nel sito di difetti ossei patologici acquisiti in sede mandibolare , stata oggetto di numerosi studi che hanno contribuito allo sviluppo di procedure chirurgiche innovative con innesti ossei ed hanno cambiato le modalit di pianificazione del trattamento [ 2 ]  . il miglior materiale da innesto rappresentato dallosso autologo , in considerazione del suo elevatissimo potenziale osteogenetico , osteoconduttivo ed osteoinduttivo [ 2 , 3 ] ; tuttavia il suo prelievo richiede una procedura invasiva e spesso si rende necessario un secondo accesso chirurgico a livello del sito donatore [ 4 ]  . 
lutilizzo di materiali eterologhi e , nello specifico , dellosso bovino a riempimento di vari tipi di difetti ossei dei mascellari , quali cisti [ 5 , 6 ] , esiti post - estrattivi di secondi e terzi molari , lacune ossee parodontali e di natura iatrogena , si dimostrato un valido approccio terapeutico con notevoli risultati in termini di rigenerazione del tessuto osseo , ben documentabili attraverso valutazione densitometrica della cavit su immagini ottenute con tomografia computerizzata ( tc ) [ 68 ]  . 
a tale proposito , la tc - dentascan consente di documentare la qualit dellosso disponibile e la sua densit [ 9 ]  . in questo studio sono stati selezionati difetti ossei mandibolari acquisiti che si sviluppano nellambito delle pareti vestibolari e linguali e che lasciano queste ultime integre , sebbene assottigliate a causa della sintesi da parte della formazione cistica , di citochine stimolanti i processi osteolitici [ 10 ]  . 
scopo del presente lavoro stato quello di valutare , dal punto di vista clinico e radiologico , gli effetti rigenerativi dellosso bovino deproteinizzato , dopo lexeresi di lesioni mandibolari , con uno studio comparativo che pone a confronto pazienti ( test ) trattati con osso bovino deproteinizzato e pazienti ( controllo ) lasciati guarire spontaneamente . this prospective , single - centre study was developed through the cooperation of the department of medical and surgical specialties , oral surgery and the division of radiological sciences . 
the study comprised 80 patients ( mean age , 42.98 ; range , 2556 years ) with a radiological diagnosis of jaw cyst who were examined between january 2007 and materiali e metodi popolazione di studio lo studio stato svolto in modalit prospettica , con caradiol med ( 2013 ) 118 : 523533 august 2011 and treated with surgical excision of the cyst . 
the study population was randomised to one of two groups : the control group ( spontaneous healing , 40 patients ) , and the test group ( treatment with deproteinised bovine bone grafting , 40 patients )  . 
the dental arch was placed at the isocentre to take advantage of the greater homogeneity of the radiation beathe fov was the same for all examinations . images were processed on a dedicated workstation ( advantage workstation ) with the dentascan v7.0.2 reconstruction protocol ; image interpretation was performed by two radiologists . 
for each lesion , we determined : ( 1 ) apicalcoronal distance , measured on the multiplanar reconstructions ; ( 2 ) mesialdistal distance , measured on native axial images ; ( 3 ) volume and average pixel intensity ( api ) , measured by applying a volume - rendering ( vr ) segmentation technique ; api was measured on the follow - up scans . 
the volumes of each lesion were obtained by manually tracing the outlines of the lesion on each axial scan ; the volume , standard deviation ( sd ) and api values of the pixels included were automatically calculated by the segmentation software . 
the maximum lesion height and width values are reported in table 1 . rattere monocentrico , ed nato dalla collaborazione tra il dipartimento di specialit medico chirurgiche , chirurgia orale , e la sezione di scienze radiologiche . 
sono stati inclusi nello studio 80 pazienti ( et media 42 , 98 , range 2556 ) con diagnosi radiologica di cisti ossea mandibolare , esaminati nel periodo compreso tra gennaio 2007 ed agosto 2011 e trattati chirurgicamente con intervento di exeresi di formazione cistica . 
tutti i pazienti sono stati esaminati mediante studio tc - dentascan , con valutazione pre - operatoria e post - operatoria ; questultima stata eseguita ad un follow - up di 12 mesi dopo lintervento di enucleazione . 
la popolazione di studio stata suddivisa mediante criterio randomizzato in due gruppi : gruppo controllo , 40 pazienti soggetti a guarigione spontanea ; gruppo test , 40 soggetti trattati con osso bovino deproteinizzato . 
il gruppo controllo e il gruppo test presentano et media rispettivamente di 42 , 9 e 43 , 1 anni ; la loro distribuzione pertanto indipendente rispetto a tale parametro . sono stati adottati i seguenti criteri di inclusione : ( 1 ) pazienti con parete vestibolare intatta , ma assottigliata ; ( 2 ) pazienti con lesioni ossee mandibolari uniloculari , con dimensione verticale ( in senso apico - coronale ) compresa nel range tra 1530 mm e con dimensione orizzontale ( in senso mesio - distale ) compresa nel range tra 1540 mi criteri di esclusione adottati sono stati i seguenti : ( 1 ) pazienti fumatori ; ( 2 ) soggetti con bruxismo ; ( 3 ) trattamento con bifosfonati ; ( 4 ) presenza di patologie sistemiche del metabolismo osseo ( iperparatiroidismo , insufficienza renale cronica , ecc . ) ; ( 5 ) turbe della coagulazione . tecnica desame tc lesame tc - dentascan mandibolare stato eseguito mediante apparecchio spirale multidetettore , adoperando il seguente protocollo di studio : kv = 120 , ma = 140 , collimazione = 0 , 625 , intervallo = 0 , 6 , campo di vista ( fov ) = 12 , 717 , 2 cm , matrice 512512 , tilt gantry = 0 ; la durata di ciascuno studio stata di circa 1015 minuti . 
il fov di acquisizione stato mantenuto invariato in tutti gli esami effettuati . le immagini acquisite sono state elaborate su consolle dedicata ( advantage workstation ) , con protocollo di ricostruzione dentascan v7.0.2 ; la lettura delle immagini stata compiuta da due radiologi . 
le immagini diagnostitable 1 values of axial and volume measurements of bone defects observed in control group and test groups radiol med ( 2013 ) 118 : 523533 526 no . 
 ( test ) l a - c ( test ) l m - d ( test ) volume ( test ) 458 pt , patient ; ctr , control group ; test , test group ; l a - c , apical - coronal distance ; l m - d , mesial - distal distance surgical management all patients were premedicated with antibiotics and anti - inflammatory agents , and treatment was continued for 6 days after surgery . 
in all cases , when the dental elements were present , a linear paramarginal incision was performed 23 mm apical to the mucogingival line periodontium sparing and more coronally when dental elements were absent . 
per ciascuna lesione sono stati calcolati : ( 1 ) dimensione apicocoronale , rilevata nelle immagini ricostruite in modalit multiplanare ; ( 2 ) dimensione mesio - distale , calcolata nelle immagini assiali native ; ( 3 ) volume ed average pixel intensity ( api ) , calcolati mediante procedura di segmentazione in applicazione di volume rendering ; lapi stato misurato nellesame di follow - up . 
i volumi di ciascuna lesione sono stati ottenuti tracciando manualmente dei contorni nelle radiol med ( 2013 ) 118 : 523533 tabella 1 valori delle misure assiali e volumetriche dei difetti ossei osservati nel gruppo controllo e nel gruppo test no . 
 statistical analysis was carried out with dedicated software singole scansioni assiali ; volume , deviazione standard e valore medio dellintensit dei pixel inclusi ( api ) sono stati elaborati automaticamente dalla console , mediante software di segmentazione dedicato . 
i valori di altezza massima e larghezza massima rilevati nella popolazione di studio sono proposti nella tabella 1 . management chirurgico tutti i pazienti sono stati premedicati con terapia antibiotica e terapia anti - infiammatoria , proseguita per i 6 giorni successivi allintervento chirurgico . 
nella tabella 1 riportiamo i valori dei volumi dei difetti ossei osservati nel gruppo controllo e nel gruppo test ; il valore medio osservato nel gruppo test di 703 , 2185 , 3 mm3 ; nel gruppo controllo la media dei volumi riscontrata di 738 , 2189 , 2 mm3 . 
nel gruppo controllo il valore medio della dimensione mesio - distale ed apico - coronale stato , rispettivamente , di 28 , 69 , 4 mm e di 252 , 84 mm ; nel gruppo test tali valori sono di 27 , 53 , 6 mm e di 25 , 32 , 97 mnon si osserva differenza statisticamente significativa tra i due gruppi , considerando le misure riportate nel grafico . 
mean values in the test group were 703.2185.3 mm3 ; in the control group , mean volumes were 738.2189.2 mm3 ; volumes in the two groups show no statistical difference , with p = 0.4. 
il valore medio osservato nel gruppo test di 703 , 2185 , 3 mm3 ; nel gruppo controllo , la media dei volumi riscontrata di 738 , 2189 , 2 mm3 ; dal confronto tra i valori dei volume dei due gruppi non si osserva differenza statisticamente significativa , con valore di p = 0 , 4 . 
la volumetria osservata tra i due gruppi ( test e controllo ) non differisce in maniera statisticamente significativa ; anche tale fattore avrebbe potuto rappresentare un parametro in grado di influenzare la percentuale di rigenerazione ossea . 
il valore medio di intensit di pixel osservato nel gruppo test 1102 , 8124 , 3 , significativamente pi alto rispetto a quello ricavato nel gruppo controllo , dove invece stato osservato un valore medio di 624 , 9133 , 3 . 
immagini assiali , ricostruzioni panorex e sezioni parasagittali contigue relative al sito di innesto , documentano lavvenuta rigenerazione ossea , con completo riempimento della cavit residua da parte di tessuto ad elevata densit ( freccia bianca ) , dal versante vestibolare a quello linguale ; possibile inoltre valutare lo stato delle corticali ossee ed i rapporti con le radici degli elementi dentari adiacenti . discussion in our study population , patient age and bone defect volume appear to be independent with respect to patient group allocation . 
in this setting , biomaterials may accelerate bone regeneration by acting as a scaffold [ 2 , 6 ] and promoting early filling of the defect , as indicated by api values in our study ; with faster regeneration ( 6 months to 1 year )  . 
 alcuni studi hanno enfatizzato il ruolo della tc nella valutazione della densit ossea dellosso mascellare ; il pattern di distribuzione tridimensionale di densit , permetterebbe una valutazione pi accurata di propriet e comportamento bio - meccanico dello scheletro mandibolare [ 11 ] ; mediante limpiego del dentascan si ottengono diversi indici di qualit ossea , come ad esempio il cawoodhowell o il norton - gramble [ 9 , 12 , 13 ]  . 
the possibility of obtaining these assessments is very important in daily clinical practice , as it enables adequate planning of maxillofacial surgery and assessment of bone response after implant or bone graft insertion [ 11 ]  . 
in particular , one of the main limitations is the inability to obtain a separate evaluation of trabecular and cortical bone , with the risk of insufficient quantification of bone structure [ 16 ]  . 
limpiego della tc - dentascan sarebbe pertanto indispensabile non solo in fase pre - operatoria in quanto unica metodica in grado di fornire dettagliate informazioni sui rapporti della lesione con le importanti strutture anatomiche adiacenti ( canale mandibolare , nervo 532 radiol med ( 2013 ) 118 : 523533 alveolare inferiore , corticale vestibolare e linguale ) ma anche in fase post - operatoria , specie quando , in previsione di un trattamento implantare , diviene presidio insostituibile , per valutare fattori critici dai quali dipende il successo implanto - protesico : la quantit e la qualit dellosso , rappresentati rispettivamente dalla dimensione verticale / orizzontale / trasversale e dalla mineralizzazione [ 17 ]  . 
limpiego di tomografi computerizzati a fascio conico potrebbe consentire di valutare la qualit e la quantit della struttura ossea con impiego di dosi di radiazioni relativamente basse ; alcuni studi hanno infatti recentemente dimostrato che la tc a fascio conico ottiene informazioni riguardo la struttura ossea sovrapponibili alla tomografia computerizzata multidetettore [ 15 ]  . 
 [ 18 ] , alla diagnostica dellimplantologia di base e dei traumi , in quanto processi neoformati o trattamenti implantari estesi devono essere studiati con apparecchi di tomografia computerizzata con fascio radiante a lama [ 18 ] ; al fine di ridurre la dose , tali autori suggeriscono di ottenere immagini da apparecchi tc multidetettore impiegando basso voltaggio [ 18 ]  . nellampio gruppo dei materiali di rigenerazione ossea , numerosi studi in vitro , in vivo , studi preclinici e clinici randomizzati su esseri umani , hanno dimostrato come losso bovino deproteinizzato , trattato con determinati procedimenti chimico - fisici , sia efficace per riparare i difetti ossei , a seguito di varie condizioni patologiche , in quanto tale sostituto manterrebbe la sua naturale architettura [ 6 ] e verrebbe privato delle componenti antigeniche innescanti immunoreazioni nel soggetto [ 2 ]  . 
secondo studi di ingegneria biomolecolare , si sono osservati gli effetti di tale materiale nei confronti dellattivit degli osteoblasti , intesa come regolazione dellespressione genica di queste importanti componenti cellulari [ 1921 ]  . le valutazioni istomorfometriche hanno dimostrato poi ladeguata propriet di riassorbimento e sostituzione del materiale analizzato con tessuto osseo neoformato [ 21 ]  . 
 the use of cone - beam ct scanners could provide an assessment of the quality and quantity of bone structure with relatively low radiation doses ; cone - beam ct provides information on bone structure similar to that obtained with multidetector ct [ 15 ]  . 
to reduce radiation dose , these authors suggest acquiring multidetector ct images with low tube voltage [ 18 ]  . among the many materials used for bone regeneration , several in vitro , in vivo , preclinical studies and randomised clinical trials demonstrate that deproteinised bovine bone , treated with specific chemicalphysical methods , is effective for repairing bone defects in a number of pathological conditions , as this substitute material seems to preserve its natural architecture [ 6 ] and does not contain antigenic components triggering immune reactions [ 2 ]  . 
according to some biomolecular engineering studies , this material has positive effects on osteoblast activity in that it regulates the genetic expression of these important cellular components [ 1921 ]  . histomorphometric studies demonstrate adequate resorption of the material and its substitution with newly formed bone [ 21 ]  . 
in addition to the previously mentioned osteoconductive properties and lack of inflammatory reaction , deproteinised bovine bone also exhibits good resorption rates , which could facilitate bone defect healing over an adequate period of time ; these data have been further validated by targeted midand long - term radiographic examinations [ 22 , 23 ]  . 
we analysed all radiological teleconsultations / telediagnoses requested by theatres of operations : kosovo , iraq , chad , warships etna ( indian ocean ) and cavour ( earthquake in haiti ) , for a total of 1 , 132 cases . 
the use of teleradiology by the military medical corps helped attain an accurate diagnosis in almost all cases , significantly reducing diagnostic errors and limiting transfers from theatres of operation to cases genuinely necessitating transfer . keywords teleradiology telemedicine riassunto obiettivo . 
sono stati analizzati tutti i teleconsulti / telediagnosi di radiologia richiesti dai diversi teatri operativi , rappresentati da kosovo , iraq , ciad , nave etna ( oceano indiano ) e nave cavour ( terremoto di haiti ) , per un totale di 1132 casi . 
nellambito della casistica acquisita dal kosovo ( 827 ) , stato valutato lintero campione dei pazienti trasferiti presso il policlinico militare di roma celio in seguito alla diagnosi teleradiologica ( 27 esami analizzati )  . 
limpiego della teleradiologia da parte della sanit militare ha consentito di favorire la diagnosi nella quasi totalit dei casi e di ridurre in modo considerevole gli errori diagnostici , limitando i trasferimenti dai teatri operativi ai casi realmente necessari . parole chiave teleradiologia telemedicina introduction teleradiology is defined as the transmission of radiological images and , where applicable , medical reports from one location to another for the purposes of remote consultation , introduzione la teleradiologia definita come la trasmissione a distanza di immagini radiologiche ed eventuali referti , finalizzata al teleconsulto , alla telediagnosi o alla teledidattica.lenorme radiol med ( 2013 ) 118 : 688699 diagnosis or teaching . 
the relentless technological progress that has revolutionised diagnostic imaging , particularly regarding image handling and processing , has made teleradiology the cornerstone of telemedicine [ 1 ]  . the fields of application of telemedicine , intended as the electronic exchange of healthcare data , are many and include virtually every medical speciality . 
telemedicine is increasingly considered an essential aid in making appropriate and effective clinical decisions , establishing close operational links among hospitals and / or physicians , even when separated by great distances [ 14 ]  . 
major geopolitical changes of the last 1520 years led to the deployment of a large number of men , women and equipment to the most remote places of the planet to guarantee peace and security in areas of conflict and offer humanitarian aid to populations in troubled regions . 
the need to ensure fundamental support to the limited medical personnel in theatres of operation and the need to reach accurate diagnoses without delay often under critical environmental and territorial conditions have found in telemedicine a key resource for ensuring adequate support both to military personnel and civilians . 
for these reasons , since deployment of the italian military forces to bosnia in 1996 following the dayton peace accords , telemedicine has become a unique instrument of the military healthcare system that , thanks to experience acquired and consolidated over the years and to continuous technological advancements , has reached extremely high levels of quality and efficiency [ 5 , 10 ]  . one of the most developed areas of telemedicine is teleradiology , which in a military setting is understood as the transmission of a diagnostic imaging examination , performed and processed in a theatre of military operation , to a higher - level healthcare facility via a telemedicine syste it includes teleconsultation , requested by the radiologist in the area of operation ; telemanagement , if the radiologist is not present at the scene of operation but receives images acquired by the radiology technician via the internet ; and teleconsultation , concerning the request for a remote second opinion on a radiological examination [ 14 , 6 , 7 ]  . the purpose of this paper is to describe recent advances and technical evolution of teleradiology in the military setting by evaluating a series of cases ( 1 , 132 radiological examinations ) collected between january 2006 and december 2010 . 
analysis of data allows us to outline the benefits of teleradiology , the peculiarities of its use in out - of - area missions and likely future scenarios . ed inarrestabile progresso tecnologico che ha rivoluzionato le metodiche di radiodiagnostica nel corso degli ultimi anni , ed in particolare la possibilit di gestire ed elaborare in modo ottimale le immagini , pongono oggi la teleradiologia quale elemento cardine nellambito di tutta la branca della telemedicina [ 1 ]  . i campi di applicazione della telemedicina , intesa come scambio di dati sanitari per via telematica , sono numerosi e comprendono praticamente ogni specializzazione medica . 
a tuttoggi rappresenta un servizio con finalit plurime , mirato ad elevare la qualit in sanit , a migliorare le prestazioni sanitarie , a favorire laggiornamento dei professionisti e ad ottimizzare il trasferimento di esperienze e di informazioni . 
la telemedicina viene sempre pi considerata come elemento di supporto indispensabile per decisioni cliniche appropriate ed efficaci , consentendo di realizzare uno stretto legame operativo tra pi ospedali e / o pi medici , anche se molto distanti [ 14 ]  . 
i grossi mutamenti degli ultimi 1520 anni dello scenario geopolitico internazionale hanno comportato un ingente impiego di uomini e mezzi nei luoghi pi disparati del pianeta , con il fine di garantire la pace e la sicurezza nelle zone di conflitto e laiuto umanitario alle popolazioni in difficolt . 
 la necessit di garantire un sostegno fondamentale alle limitate risorse di personale medico nei teatri operativi e lesigenza di intervenire con diagnosi efficaci in tempi rapidi , spesso peraltro ulteriormente condizionate dalle gravi situazioni ambientali del territorio , hanno trovato nella telemedicina una risorsa fondamentale e determinante per assicurare un supporto sanitario adeguato sia al personale militare che alla popolazione civile . 
per tali ragioni , fin dallimpiego del contingente militare italiano in bosnia nel 1996 in seguito agli accordi di pace di dayton , il servizio di telemedicina ha costituito uno strumento peculiare della sanit militare che , grazie alle esperienze acquisite e consolidate nel corso degli anni ed al costante progresso tecnologico , ha raggiunto oggi livelli di elevatissima qualit ed efficienza [ 5 , 10 ]  . uno dei settori di maggiore sviluppo della telemedicina rappresentato dalla teleradiologia , la quale , in ambito militare , intesa come la trasmissione di un esame di diagnostica per immagini , acquisito ed elaborato in un teatro di operazioni , ad una struttura sanitaria di livello superiore mediante un sistema di telemedicina . 
comprende sia il teleconsulto , richiesto dal radiologo presente nella zona di operazione , sia la telegestione , nel caso in cui lo specialista radiologo non sia presente direttamente sullo scenario operativo , ma riceva la documentazione iconografica acquisita dal tecnico sanitario di radiologia medica presente in loco attraverso la rete , sia la teleconsulenza , riguardante la ri690 materials and methods patient population the study considered a large case series ( 1 , 132 radiological examinations ) collected between january 2006 and december 2010 by the military healthcare systeall examinations requested from the various theatres of operation kosovo , iraq , chad , etna warship ( indian ocean ) and cavour warship ( earthquake in haiti ) were analysed , for a total of 1 , 132 cases . 
within the series of teleradiology requests sent from kosovo ( 827 examinations ) , we retrospectively evaluated the entire sample of patients transferred following teleradiology diagnosis ( 27 cases )  . 
during operations in iraq and chad in 2008 , data were transmitted using indirect digital technology ; that is , analogue images digitised with computed radiography ( cr )  . 
transmission of radiology and computed tomography ( ct ) examinations from the warships cavour and etna ( 2010 ) was performed using direct digital systems . the celio military hospital in rome , which is equipped with radiology information system ( ris ) and picture archiving and communication system ( pacs ) patient data and image management and with a 24 - h radiology unit , served as the network control station , which was intended as the central station for image reception in italy . 
data were mostly transmitted via the sicral military satellite operating on the x - band , the reference band for radar and satellite communications used by the military and space agencies . 
if the area from which the images were sent was not covered by the military satellite , ku - band civilian satellites were used : this band is generally used by the us national aeronautics and space administration ( nasa ) and television satellites . 
data were transmitted by store and forward , a method in which images remain stored on the server of the remote station and are then viewed at the military hospital in rome , where the resolution of regions of interest ( rois ) can radiol med ( 2013 ) 118 : 688699 chiesta di una second opinion a distanza sullatto medicoradiologico compiuto [ 14 , 6 , 7 ]  . lo scopo di questo lavoro di evidenziare i progressi e levoluzione tecnica della teleradiologia in ambito militare nel corso degli ultimi anni , valutando lintera casistica ( 1132 esami radiologici ) ottenuta nel periodo compreso tra gennaio 2006 e dicembre 2010 . 
lanalisi dei dati ricavati consente di delineare i vantaggi nellutilizzo dello strumento teleradiologico , le peculiarit del suo impiego nelle missioni fuori aerea ed i probabili scenari futuri . materiali e metodi popolazione di pazienti lo studio stato condotto sulla base dellimportante casistica ( 1132 esami radiologici ) ottenuta nel periodo compreso tra gennaio 2006 e dicembre 2010 attraverso limpiego di tale strumento da parte della sanit militare . 
sono stati complessivamente analizzati tutti gli esami radiologici richiesti dai diversi teatri operativi , rappresentati da kosovo , iraq , ciad , nave etna ( oceano indiano ) e nave cavour ( terremoto di haiti ) , per un totale di 1132 casi . 
nellambito della casistica delle richieste di teleradiologia pervenute dal teatro operativo del kosovo ( 827 esami ) , stato valutato retrospettivamente lintero campione ( 27 casi ) dei pazienti trasferiti in seguito alla diagnosi teleradiologica . 
durante le operazioni in iraq ed in ciad , nel 2008 , la trasmissione di dati stata acquisita con tecnologia digitale indiretta , ossia attraverso immagini analogiche digitalizzate mediante computer radiography ( cr ) .la trasmissione di esami di radiologia e tomografia computerizzata dalle navi cavour ed etna ( 2010 ) stata realizzata con sistemi di tecnologia digitale diretta . radiol med ( 2013 ) 118 : 688699 be magnified using the pixel - on - demand technique . 
 within the series acquired from the kosovo theatre of operations ( 827 radiological examinations ) , we analysed the entire sample of patients transferred following teleradiological diagnosis ( 27 cases ) by comparing radiological examinations performed in the theatre of operation and reported via teleradiology and those performed on the same patients after transfer to the celio military hospital . for the most severe cases , mainly consisting of major trauma in the case of soldiers and cancer in the case of civilians , we were unable to make a retrospective comparative analysis between examinations . 
military patients with major trauma were initially treated at the healthcare facilities in the theatres of operation and were only transferred to the celio military hospital after having been stabilised . 
similarly , civilians with severe trauma or cancer were treated at the civilian hospitals available in the areas of operation , after diagnostic assessment and , in some cases , immediate treatment . 
 data were analysed by calculating sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy of all examinations performed and for each type of examination and request . 
 concordance between diagnoses was analysed using cohens kappa ( ) test . results between january 2006 and december 2010 , the total number of teleconsultations / radiological telediagnoses requested from the various theatres of operation was 1 , 132 : military 704 and civilians 428 ( table 1 )  . all radiological examinations received from kosovo , the theatre of operation originating the largest number of requests ( 827 teleconsultations : 432 military and 395 civilians ) were assessed retrospectively ( table 2 )  . 
an additional 14 teleconsultations on scanned ct images obtained at civilian hospitals were added to the series of civilian patients : three for hepatocellular carcinoma , one for a retroperitoneal mass , one for haemothorax , two for brain tumour , two for ct angiography in major trauma , two for suspected aortic dissection , one for acute pancreatitis , one for multiple pelvic fractures and one for a vertebral fracture . following teleradiological diagnosis , of 432 cases from armed forces at the kosovo theatre , 27 were transferred to the celio military hospital in rome . 
comparison could therefore be made between diagnoses by the same il policlinico militare di roma celio , dotato di un sistema radiology information system ( ris ) e picture archiving and communication system ( pacs ) per la gestione di dati ed immagini dei pazienti e di una unit operativa radiologica in servizio attivo 24 ore su 24 , ha costituito la stazione capo maglia , intesa come il punto di ricevimento centrale delle immagini sul territorio nazionale . 
la trasmissione dei dati stata affidata prevalentemente al satellite militare sicral a banda x , che rappresenta la banda di riferimento per le comunicazioni radar e satellitari da parte dei militari e delle agenzie spaziali . 
nel caso di impossibilit del satellite militare a coprire larea di invio delle immagini , sono stati utilizzati satelliti civili a banda ku , questultima generalmente impiegata dai satelliti della nasa e dai satelliti televisivi . 
la trasmissione dei dati avvenuta in store and forward , modalit per cui le immagini restano archiviate nel server della stazione remota , per essere quindi visualizzate presso il policlinico militare di roma , con la possibilit di magnificare la risoluzione delle regioni di interesse tramite la tecnica pixel on demand . 
 nellambito della casistica acquisita dal teatro operativo del kosovo ( 827 esami radiologici ) , stato analizzato lintero campione ( 27 casi ) dei pazienti trasferiti in seguito alla diagnosi teleradiologica , operando un confronto tra gli esami radiologici eseguiti in zona di operazione e refertati in teleradiologia e quelli effettuati sugli stessi pazienti sgomberati presso il policlinico militare di roma celio , struttura sanitaria militare di riferimento sul territorio nazionale . per i casi di maggiore gravit , rappresentati prevalentemente da traumatismi maggiori per i pazienti militari e da patologie oncologiche per i pazienti civili , non stato possibile operare unanalisi retrospettiva di confronto tra gli esami eseguiti in teatro di operazione e quelli effettuati allarrivo in ospedale . 
nel caso dei traumatismi maggiori , infatti , i pazienti militari sono stati gestiti preliminarmente presso le strutture sanitarie predisposte in zona di operazione e solo successivamente trasferiti , una volta stabilizzati , presso il policlinico militare celio . 
analogamente , i pazienti civili con traumatismi gravi o affetti da patologie oncologiche , dopo linquadramento diagnostico e leventuale trattamento immediato , sono stati gestiti presso le strutture ospedaliere civili presenti nellarea di operazione . 
 in questi casi la teleradiologia stata impiegata prevalentemente come teleconsulto radiologico , in particolare su esami di tomografia computerizzata ( tc ) effettuati presso strutture civili del territorio o su esami tc inviati dalla nave cavour durante loperazione per il terremoto di haiti nel 2010 . 
 lanalisi statistica dei dati raccolti stata realizzata calcolando sensibilit , specificit , valore predittivo positivo ( ppv ) , valore predittivo negativo ( npv ) ed accuratezza diagnostica per il totale degli esami effettuati e per ogni singola tipologia di esami e di richiesta pervenute . 
 all teleradiological diagnoses were confirmed at the hospital , with the exception of two chest x - ray examinations : in these cases , the remote report mentioned an inflammatory consolidation that was not confirmed by the military hospital , which included ct . 
table 3 summarises all cases in which a comparison could be made between examinations at both locations . statistical analysis of all results yielded 92.59% overall sensitivity , 0% specificity , 100% positive predictive value ( ppv ) , 0% negative predictive value ( npv ) and a 92.59% diagnostic accuracy for teleradiology . 
statistical analysis of results according to examination type and indications provided 100% sensitivity , 0% specificity , 100% ppv , 0% npv and 100% diagnostic accuracy for the following categories : chest x - ray for suspected pneumothorax , ankle x - ray , mandible x - ray , leg and ankle x - ray and hand x - ray . 
 statistical analysis of results provided by teleradiology showed test specificity and npv of 0% in both the evaluation of all cases examined and results by type of examination and indications , as there were no cases of healthy patients [ true negative ( tn ) ]  . 
alla casistica dei pazienti civili vanno aggiunti 14 teleconsulenze su immagini scansionate di esami tc eseguiti presso strutture ospedaliere civili cos suddivise : 3 consulenze su epatocarcinoma , 1 consulenza su massa retroperitoneale , 1 consulenza su emotorace , 2 consulenze su neoplasia cerebrale , 2 consulenze su angio - tc in traumatismi maggiori , 2 consulenze su sospetta dissezione aortica , 1 consulenza su pancreatite acuta , 1 consulenza su fratture multiple del bacino , 1 consulenza su frattura vertebrale . a seguito della diagnosi teleradiologica , su un totale 694 radiol med ( 2013 ) 118 : 688699 di 432 casi analizzati dallo scenario operativo del kosovo appartenenti alle forze armate , sono stati trasferiti 27 pazienti presso il policlinico militare di roma . 
loperazione di trasferimento stata eseguita in tempi estremamente rapidi , per cui lintervallo temporale tra gli esami refertati per via telematica e quelli eseguiti e refertati contestualmente al ricovero dei pazienti presso il policlinico di roma stato compreso entro un tempo non superiore ai 5 giorni dal primo esame . 
 tutte le diagnosi effettuate in teleradiologia sono state confermate in ospedale , ad eccezione di due rx torace : in tali casi la refertazione a distanza si esprimeva su un addensamento di significato flogistico non confermato dalla diagnosi eseguita presso il policlinico militare , anche mediante metodica tc . 
la tabella 3 riassume tutti i casi per cui stato possibile eseguire un confronto tra esami radiografici effettuati in telemedicina ed esami radiografici eseguiti presso il policlinico militare . lanalisi statistica del totale dei risultati analizzati ha riportato per lo strumento teleradiologico una sensibilit globale del 92 , 59% , una specificit dello 0% , un ppv del 100% , un npv dello 0% ed unaccuratezza diagnostica del 92 , 59% . la valutazione statistica dei risultati ottenuti per le diverse tipologie di esami ed indicazioni ha riportato sensibilit del 100% , specificit dello 0% , ppv del 100% , npv dello 0% ed accuratezza diagnostica del 100% per le seguenti categorie : rx torace per sospetto pneumotorace , rx caviglia , rx mandibola , rx gamba e caviglia ed rx mano . 
 lo studio del sottogruppo rx torace per sospetto addensamento flogistico ha riportato una sensibilit del 60% , specificit dello 0% , ppv del 100% , npv dello 0% e accuratezza diagnostica del 60% . 
 lanalisi statistica dei risultati ottenuti attraverso la metodica teleradiologica ha dimostrato una specificit ed un vpn del test pari a 0% sia nella valutazione di tutti i casi esaminati sia nello studio dei risultati ottenuti per le diverse tipologie di esami ed indicazioni poich in nessun caso sono stati osservati pazienti sani ( veri negativi , vn )  . 
per questultimo risultato statistico ( vn = 0 ) sia la specificit , che indica la capacit del test di identificare correttamente i pazienti sani e che si ottiene dalla divisione dei vn per il totale dei malati , sia il vpn , che esprime la probabilit che un soggetto con risultato negativo al test sia realmente sano e che si ottiene dalla divisione dei vn per il totale dei risultati negativi al test , sono entrambe pari a 0 . lo studio della concordanza tra le diagnosi effettuate a distanza in teleradiologia e quelle effettuate presso il polifig . 
in those cases , teleradiology was used as a radiological teleconsultation tool mainly to seek a second opinion , as both ships had a radiologist and a radiology technician on board . 
extensive lesion of the left side of the cheek with loss of bone continuity in the frontal and temporal processes of the zygomatic bone , maxillary bone zygomatic process and mandibular ramus and condyle . 
voluminosa lesione in corrispondenza dellemilato sinistro della guancia , con interruzione della continuit ossea a carico del processo frontale e del processo temporale dellosso zigomatico e del processo zigomatico dellosso mascellare , nonch del ramo e del condilo mandibolare . 
la valutazione specifica della concordanza per le diverse categorie di indicazioni e di esami eseguiti , ha mostrato una concordanza perfetta per tutte le categorie suddette ( = 1 ) ad eccezione del sottogruppo di casi rx torace per sospetto addensamento flogistico , per il quale la concordanza risultata essere di grado moderato ( = 0 , 6 )  . 
 durante le operazioni del 2010 dalle navi cavour ( terremoto di haiti ) ed etna ( oceano indiano ) stata utilizzata per la prima volta la tecnologia digitale diretta per la trasmissione di esami di radiologia e tomografia computerizzata . 
in questo caso la teleradiologia stata impiegata sotto forma di teleconsulto radiologico , prevalentemente come second opinion , essendo entrambe le navi provviste di medico radiologo e tecnico di radiologia . 
il servizio stato approntato e consolidato nella sua massima efficienza dopo anni di sperimentazione e di implementazione dello strumento della telemedicina , iniziato fin dal 1996 in seguito al dispiego del personale militare italiano nelloperazione di pace in bosnia . gli operatori tecnici , altamente specializzati , sono in grado di eseguire in tempi brevissimi i collegamenti dai vari teatri operativi alla cosiddetta stazione capo maglia , intesa come il punto di ricevimento centrale delle immagini sul territorio nazionale , che per litalia si identifica con il policlinico militare di roma celio . 
la trasmissione dei dati avviene con modalit store and forward . la dottrina north atlantic treaty organization ( nato ) prevede 4 tipi di strutture sanitarie con relativa dotazione di sistemi di diagnostica per immagini : il role 1 , in cui non sono previsti sistemi diagnostici ; il role 2 , che prevede radiologia ed ecografia ; il role 3 , comprendente radiologia convenzionale , ecografia e tc . 
le prime tre strutture sanitarie sono collocate generalmente al di fuori del territorio nazionale , in particolare nello specifico contesto dei territori di operazione , con diversa dislocazione a seconda dello scenario geografico e delle modalit di impiego del personale militare [ 5 , 10 ]  . 696 discussion teleradiological activities rely on a service that has been fully operative since january 2003 , set up under the athena [ ce3 ] project participated in by the chiefs of defence , tel bios and the san raffaele institute in milan . 
 the service was launched in 1996 following the deployment of italian military personnel in peacekeeping operations in bosnia and was prepared and brought to its maximal efficiency after years of telemedicine testing and implementation . the highly specialised technical operators are able to rapidly establish connections from the various theatres of operations to the network control station i.e. 
data are transmitted by a storeand - forward mechanism . the north atlantic treaty organisation ( nato ) doctrine envisages four levels of medical treatment facilities , each with their respective diagnostic imaging systems : role 1 , without diagnostic imaging facilities ; role 2 , with radiology and ultrasonography ; role 3 , with conventional radiology , ultrasonography , and ct . 
the first three facilities are generally located abroad in the context of theatres of operation and are variously deployed according to the geographical setting and types of engagement of military personnel [ 5 , 10 ]  . the highest level of medical treatment facility , role 4 , coincides with the referral hospital in the country of origin , which is equipped with all diagnostic imaging modalities ( conventional radiology , ultrasound , ct , magnetic resonance imaging , digital subtraction angiography )  . 
the referral hospital for italy , celio military hospital in rome , is equipped with ris and pacs systems for patient data and image management and a radiology unit operating around the clock dedicated to reporting remote images . 
devices all comply with the digital imaging and communications in medicine ( dicom ) standard and are tightly interoperable and interdependent , so the remote interlocutors can be absolutely certain that data transmitted and images received are of high quality and complete . 
telecommunication systems used for this purpose are chosen to ensure fast and reliable transmission , taking into account traffic volumes for the different radiological images ( table 4 )  . 
in theatres of operation , prompt diagnoses are fundamental for patient management and choosing subsequent diagnostic and / or therapeutic workup ( immediate treatment , transfer or management )  . 
large traffic volumes are transmitted using broadband frequencies ( bandwidth > 1 , 000 mb / s ) with data compression . the application of teleradiology in the military setting is probably the most significant example of the dramatic techradiol med ( 2013 ) 118 : 688699 lultimo livello di struttura sanitaria militare , il role 4 , coincide con lospedale di riferimento sul territorio nazionale provvisto di tutte le metodiche di diagnostica per immagini [ radiologia , ecografia , tc , risonanza magnetica ( rm ) , angiografia digitale sottrattiva ( dsa ) ]  . 
le apparecchiature utilizzate , tutte conformi allo standard digital imaging and communications in medicine ( dicom ) , sono strettamente interoperabili ed interdipendenti tra loro , in modo da fornire allinterlocutore remoto la garanzia assoluta che i dati trasmessi e le immagini ricevute siano completi e di elevata qualit . 
la scelta dei sistemi di telecomunicazione viene effettuata con la finalit di assicurare tempi di trasmissione rapidi ed affidabili , tenendo conto dei volumi di traffico per le diverse immagini radiologiche ( tabella 4 )  . 
la tempestivit della diagnosi in teatro di operazione , infatti , un elemento fondamentale per la gestione del paziente e per la scelta del successivo iter diagnostico e / o terapeutico ( trattamento immediato , sgombero o gestione )  . 
la trasmissione di grandi volumi di traffico ottenuta attraverso limpiego di frequenze a banda larga ( ampiezza di banda > 1000 mbit / s ) e con la compressione dei dati . lapplicazione della teleradiologia in ambito militare costituisce lesempio probabilmente pi significativo dellenorme evoluzione tecnologica che tale strumento ha subito negli ultimi anni , di pari passo con i profondi cambiamenti che hanno rivoluzionato tutta la branca radiologica . 
basti pensare che , nei primi impieghi della teleradiologia durante i conflitti in bosnia nel 1996 ed in albania nel 1999 , le immagini radiologiche erano inviate a distanza attraverso la ripresa della pellicola radiografica con una videocamera o la fotografia della pellicola stessa . 
 durante le operazioni in iraq ed in ciad , nel 2008 , stata utilizzata per la prima volta in teleradiologia militare la trasmissione di dati con tecnologia digitale indiretta , ossia attraverso immagini analogiche digitalizzate mediante cr , fino a giungere allutilizzo della tecnologia digitale diretta per la trasmissione di esami di radiologia e tomografia computerizzata dalle navi cavour ed etna ( 2010 )  . 
to appreciate this development , it is enough to consider that when teleradiology was first used during the conflicts in bosnia ( 1996 ) and albania ( 1999 ) , radiological images were sent to remote locations by filming the radiographic image with a video camera or by taking photographs of it . 
analogue images digitised with computed radiography ( cr ) , was first used in military teleradiology during operations in iraq and chad in 2008 ; direct digital technology was used to transmit x - ray and ct examinations from the warships cavour and etna in 2010 . 
in fact , use of the digital cr system makes it possible to harness all the benefits of digital technology , especially the ability to further process images acquired in analogue format at remote stations , because an imaging plate ( ip ) is used instead of the screen - film syste an ip consists of a highly sensitive detector that records diagnostic images as electrical signals and uses the same equipment as that used in analogue imaging . 
data are transmitted via the x - band sicral military satellite , but civilian satellites working on the ku band may also be used if the military satellite cannot cover the transmission area . in this study , radiological examinations repeated on patient admission to the military hospital confirmed the telediagnosis in almost all cases , proving the quality and reliability of this diagnostic tool . 
la trasmissione dei dati avviene tramite il satellite militare sicral a banda x con la possibilit di usufruire di satelliti civili con banda ku nel caso in cui il satellite militare non possa coprire larea di invio delle immagini . 
 gli esami radiografici ripetuti allarrivo presso il policlinico militare dei pazienti trasferiti hanno confermato , in quasi la totalit dei casi , la diagnosi eseguita per via telematica , dimostrando la qualit e laffidabilit di tale strumento diagnostico . 
le differenze interpretative riscontrate possono essere imputabili alla diversa qualit tecnica degli esami radiografici effettuati , in quanto acquisiti con tecnica analogica per il kosovo e con tecnica digitale presso il policlinico militare di roma . 
 inoltre importante considerare anche lintervallo temporale trascorso tra la diagnosi teleradiologica di addensamento su base flogistica e lo studio eseguito al rientro in italia ( compreso entro un massimo di 5 giorni ) , entro il quale verosimile presupporre una riduzione del processo eventualmente in atto . 698 radiol med ( 2013 ) 118 : 688699 raphy was the diagnosis of inflammatory consolidation not confirmed . 
 the time elapsed between the teleradiology diagnosis of inflammatory consolidation and the examination performed in italy should also be considered ( maximum 5 days ) , as the inflammatory process may have partially resolved during this time . the possibility of performing radiological examinations without the presence of a radiologist improved patient comfort by avoiding transfer to other healthcare facilities , a particularly critical process in a theatre of operation given the risks inherent in land movements . 
 the large proportion of teleconsultations / telediagnoses requested for civilian patients demonstrates that teleradiology has become a prerequisite for humanitarian activities , allowing appropriate diagnosis to be made in poorly accessible areas that often a healthcare facility or diagnostic equipment . 
in this regard , our results show that the use of direct digital technology on the cavour and etna during operations in haiti and the indian ocean were particularly important . 
use of direct digital technology allowed images to be transferred in real time and without the technical limitations of scanning , thus enabling the military hospital radiologists to provide immediate , high - quality consultation on x - ray and ct examinations , even in severe cases . 
 the future of military teleradiology includes some key technical developments : acquisition of all images with the direct digital technique ; building shelters equipped with suspended digital x - ray systems ; equipping role 1 facilities ; and ambulances with latest - generation , digital ultrasound systems , both portable and stationary . 
with regard to image handling , attention is placed on the possibility of transferring large volumes of raw data for postprocessing . a direct connection between the teleradiology image acquisition system and the ris - pacs system and the military hospital in rome is being devised so that radiological examination can be directly sent to pacs via a control workstation . 
as a result , the patients examination data can be directly linked to the images and , after the report , the examination will be automatically signed and archived in the syste conclusions analysis of radiological teleconsultation shows that telerala possibilit di eseguire esami radiologici senza la presenza fisica del medico radiologo ha garantito di migliorare il comfort dei pazienti e di evitarne lo spostamento verso altre strutture sanitarie , attivit particolarmente delicata in teatro di operazione per i rischi intrinseci connessi ai movimenti sul territorio . 
 lelevato numero di teleconsulti / telediagnosi concernenti pazienti civili ha inoltre dimostrato che la teleradiologia rappresenta un sistema ormai imprescindibile anche per le attivit di carattere umanitario , consentendo di effettuare diagnosi appropriate in zone impervie , quasi sempre prive di strutture sanitarie e di attrezzature diagnostiche . 
 a tale riguardo , come evidenziato dai risultati , particolare rilevanza ha costituito limpiego della tecnologia digitale diretta sulle navi cavour ed etna durante le operazioni per il terremoto di haiti e per loceano indiano nel 2010 . 
 limpiego della tecnologia digitale diretta ha , infatti , consentito di poter trasferire immagini in tempo reale e senza i limiti tecnici della scannerizzazione , permettendo ai medici radiologici del policlinico militare di roma di fornire una consulenza immediata , adeguata e di elevata qualit su esami rx e tc riguardanti anche casi di particolare gravit . 
 lo scenario del prossimo futuro in ambito militare prevede alcune evoluzioni tecniche fondamentali : lacquisizione di tutte le immagini con tecnica digitale diretta ; la realizzazione di shelter dotati di pensile rx digitalizzato ; la dotazione di sistemi ad ultrasuoni ( ecografi ) di nuova generazione digitali , anche portatili , su ambulanza o allinterno del role 1.per quanto riguarda la gestione delle immagini , lattenzione focalizzata sulla possibilit di implementare il sistema attraverso la trasmissione di grandi volumi di dati grezzi , cos da poter elaborare ricostruzioni in post - processing . inoltre in fase di definizione il collegamento diretto tra il sistema di acquisizione delle immagini in teleradiologia ed il sistema ris - pacs del policlinico militare di roma , in modo che lesame radiologico , una volta eseguito , venga inviato direttamente al pacs attraverso una postazione di controllo . 
 conclusioni lanalisi dei teleconsulti radiologici effettuati ha evidenziato come lutilizzo della teleradiologia abbia consentito di favorire la diagnosi nella maggioranza dei casi , di ridurre in modo considerevole gli errori diagnostici e di indirizzare adeguatamente il successivo percorso terapeutico e gestionale del paziente . 
grazie allausilio di tale strumento stato radiol med ( 2013 ) 118 : 688699 diology helped establish diagnoses in the majority of cases considered , with dramatically reduced diagnostic errors and accurately guided subsequent patient treatment and management . 
this tool enabled medical evacuations , that is , transfers by helicopter from theatres of operation which were restricted to urgent cases only reduced costs and use of personnel . on the basis of the results of this study , we conclude that teleradiology has become a highly useful tool for co - operation between the different healthcare facilities . 
in particular , we found that using this technique was crucial for both radiologists in ( out - of - area ) field hospitals and specialists of other disciplines ( clinical and surgical )  . 
our study confirms the role of teleradiology as a key telemedicine tool for managing healthcare in out - ofarea operations , ensuring extremely high levels of reliability and efficiency . possibile limitare i medevac ( medical evacuation ) , ossia i trasferimenti elitrasportati dal teatro operativo , solo ai casi realmente necessari , con conseguente riduzione dei costi e dellimpiego del personale . sulla base dei dati emersi da questo studio , si pu affermare che la teleradiologia rappresenta ormai uno strumento di assoluta utilit per la cooperazione tra le diverse strutture sanitarie presenti sul territorio . 
in particolare , limpiego della teleradiologia risultato un ausilio fondamentale sia per il medico radiologo operante nellospedale da campo ( fuori area ) sia per lo specialista di altra branca ( clinica o chirurgica )  . 
conventional ultrasound ( us ) and quantitative elastography were performed in 108 women with 114 breast lesions by two experienced radiologists , and pathological results were available in all cases . 
108 donne con lesioni alla mammella sono state sottoposte ad ecografia convenzionale ed a studio elastografico quantitativo mediante supersonic shear imaging da due radiologi esperti ; in ogni caso era disponibile il riscontro anatomopatologico delle lesioni . 
le lesioni maligne manifestavano elasticit massima e media significativamente maggiore ( 111 , 5769 , 29 kpa e 54 , 49 33 , 70 kpa ) rispetto alle lesioni benigne ( 59 , 0045 , 35 kpa e 36 , 6426 , 18 kpa ) ( p < 0 , 01 )  . 
lelasticit media e massima del carcinoma duttale invasivo ( cdi ) risultata significativamente maggiore rispetto al fibroadenoma ( p < 0 , 01 ) , mentre non sono emerse differenze statisticamente significative con la fibroadenosi , il papilloma e linfiammazione ( p > 0 , 01 )  . 
 le lesioni con bi - rads 5 presentavano tutte unelasticit media e massima significativamente maggiore rispetto alle lesioni con bi - rads 3 ( p < 0 , 01 )  . 
shear - wave elastography gives quantitative elasticity information that could potentially help in breast - lesion characterisation , although it cannot replace conventional bi - rads in the differentiation of breast lesions . keywords breast neoplasms ultrasonography shearwave elastography diagnosis quantitative analysis introduction elastography is an emerging imaging technique that quantifies the stiffness of a breast lesion in relation to the background adipose and fibroglandular tissues [ 1 , 2 ]  . 
this property can be described by youngs modulus which is defined as e = / where is the applied stress and is the resultant deformation of the tissue . in the last few years , sonoelastography has been applied to the diagnosis of breast , thyroid , muscle , liver , prostate disease [ 38 ]  . 
reported a sensitivity of 0.76 for es and 0.79 for sr , and a specificity of 0.81 for es and 0.76 for sr [ 11 ]  . shear - wave elastography ( swe ) is a new method for obtaining elastography images . 
within a given region of interest ( roi ) , defined by an electronic cursor , values for stiffness maximum , mean and standard deviation ( sd ) are produced . 
another paper demonstrated that shear - wave elastography was helpful in differentiating benign from malignant breast masses and may increase the ability of breast us to differentiate between benign and malignant masses [ 13 ]  . 
 [ 14 ] demonstrated that swe could provide quantitative and reproducible information on solid breast lesions with diagnostic dellelasticit massima e media risultata essere pressoch perfetta [ coefficiente di correlazione intraclasse ( cci ) = 0 , 87 e 0 , 79 ]  . 
lelastografia quantitativa mediante supersonic shear imaging fornisce informazioni che potrebbero essere potenzialmente utili nella caratterizzazione delle lesioni alla mammella , sebbene non possa sostituire il sistema bi - rads convenzionale nella loro differenziazione . parole chiave tumore della mammella ecografia shear - wave elastografia diagnosi analisi quantitativa accuracy at least as good as conventional us with breast imaging reporting and data system ( bi - rads ) classification . 
however , these studies have only limited elasticity parameters and did not assess the correlation of elasticity and bi - rads . the study reported here evaluated the role and accuracy of swe in characterising breast nodules and differentiating between malignant and benign lesions by using multiple elasticity values . 
 patients and methods patients from march 2010 to june 2010 , a prospective study was conducted at our institute to evaluate the utility and diagnostic performance of quantitative elastography using the aixplorer us system ( supersonic imagine , aix en provence , france )  . 
we excluded pregnant and lactating women , those with breast implants , women receiving chemotherapy or radiotherapy for any cancer , those with biopsied skin masses and those with a history of ipsilateral breast surgery . 
written informed consent was obtained from every patient at enrolment . radiol med ( 2013 ) 118 : 583590 table 1 correlation between pathological diagnosis and breast imaging reporting and data system ( bi - rads ) category tabella 1 correlazione tra diagnosi patologica e categorie bi - rads pathology bi - rads category idc ( n = 44 ) dcis ( n = 2 ) fibroadenoma ( n = 43 ) fibroadenosis ( n = 15 ) papilloma ( n = 4 ) inflammation ( n = 6 ) idc , invasive ductal carcinoma ; dcis , ductal carcinoma in situ us and swe examinations us and swe examinations were performed with an aixplorer us system ( supersonic imagine , aix en provence , france ) with a probe frequency of 15 - 4 mhz . 
us images were classified according to the american college of radiology ( acr ) bi - rads [ 15 ] by two breast radiologists ( yan huang and wen bo wan ) with 10 and 12 years of experience , respectively , in breast us . 
bi - rads categories 13 were taken as benign , whereas scores of 4 or 5 were taken as malignant . after us examination , the radiologist switched to elastography mode . 
the probe must be kept still for 1020 s during image acquisition ( due to a slow frame rate ) , and this was often best done during a breathhold . 
after recording a stable image , a region of interest ( roi ) as large as possible was chosen to cover the entire lesion , including lesion borders and any calcification , to calculate elasticity value . 
two independent expert observers performed a blinded review of static images of all lesions . statistical analysis all analyses were performed using spss 11.0 , standard version ( spss inc , chicago , il , usa )  . 
students t test and receiver operating characteristic ( roc ) analyses ( with associated measures , including sensitivity , specificity and accuracy ) were used to assess the diagnostic value of maximum , mean and minimum elasticity ratio and to choose diagnostic cutoff values . 
benign lesions consisted of fibroadenoma ( n = 43 ) , fibroadenosis ( n = 15 ) , papilloma ( n = 4 ) and inflammation ( n = 6 )  . 
the correlation between pathological diagnosis and bi - rads category is presented in table 1 . benign / malignant differentiation by elasticity maximum , mean and minimum elasticity and elasticity ratio between both malignant and benign lesions and surrounding parenchyma are presented in table 2 . 
sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy for maximum elasticity , mean elasticity and bi - rads are shown in table 3 . 
when combining bi - rads and maximum elasticity , diagnostic sensitivity increased significantly ( p = 0.000 ) , whereas diagnostic specificity , ppv and accuracy all decreased , although the difference was not statistically significant ( p > 0.01 ) ( table 3 )  . 
they all increased with increasing bi - rads category : bi - rads 5 were all significantly higher than bi - rads 3 . maximum , mean and minimum elasticity and elasticity ratio between lesions and surrounding parenchyma with different pathology can be seen in table 4 . 
maximum and mean elasticity of idc was significantly higher than in fibroadenoma reproducibility reliability of quantitative elasticity measurements on swe 588 radiol med ( 2013 ) 118 : 583590 fig . 
 discussion in prior studies , elastography imaging has shown potential for differentiating benign from malignant breast disease and could possibly reduce the overall number of breast biopsies [ 9 , 16 , 17 ]  . 
these are both semiquantitative parameters , which are highly dependent on the organs compressibility limits under stress and on the skill of the operator to correctly compress the tissue [ 18 ]  . 
 radiol med ( 2013 ) 118 : 583590 swe is a new method for obtaining elastography images in which an acoustic pressure wave induces slow - moving lateral waves within the tissue , and the speed shear - wave propagation is proportional to the tissues elastic modulus . 
 the velocity information can be mapped to create an image of the stiffness , with the option of measuring swe features , such as minimum , mean and maximum elasticity in an roi . 
thus , further studies should be carried out to identify the best cutoff point to optimise the differentiation of benign and malignant lesions . our study showed that maximum and mean idc elasticity was higher than those of papilloma and inflammation but without statistical significance . 
 in this study , with the increase in bi - rads , maximum and mean elasticity increased , and there was a significant difference between bi - rads 3 and 5 in maximum and mean elasticity . 
consistent image generation is critical for the serial study of masses for example , to follow - up probably benign masses or to monitor response of breast carcinomas to neoadjuvant chemotherapy and the reliability of swe could be helpful in these clinical situations . 
our study demonstrates that swe is a reliable method and that maximum and mean elasticity are reliable values , which helps the further application of this method . there are some limitations to our study . 
an additional study is necessary to confirm the correlation of elasticity values with each variable and to identify variables that can affect the false - positive or false - negative results . in conclusion , swe provides quantitative elasticity information that can potentially help characterise breast lesions . 
biti1 1radiotherapy unit , 2department of surgery , and 3department of pathology , university of florence , viale morgagni 85 , 50134 florence , italy 4molecular and nutritional epidemiology unit , cancer research and prevention center , scientific institute of tuscany , florence , italy 5radiotherapy unit , ifca , university of florence , italy correspondence to : d . 
all patients underwent preoperative radiotherapy ( 45 gy in 1.8 - gy fractions ) with concurrent ox ( 80 mg / m2 i.v. , day 1 ) and a 120h continuous infusion of 5 - fu ( 1 , 000 mg / m2 per day )  . 
lo scopo di questo studio quello di valutare la risposta patologica ( pr ) , il controllo di malattia e la sicurezza del trattamento chemioterapico basato sulluso di oxaliplatino e 5 - fluorouracile in associazione alla radioterapia nel trattamento del tumore del retto localmente avanzato . 
sono stati analizzati retrospettivamente , nel periodo compreso tra novembre 2002 e dicembre 2010 , 90 pazienti affetti da tumore del retto localmente avanzato sottoposti a radio - chemioterapia ( crt ) pre - operatoria . 
tutti i pazienti hanno ricevuto una radioterapia pre - operatoria ( 45 gy in 1 , 8 gy per frazione ) associata ad oxaliplatino ( 80 mg / m2 endovena , giorno 1 ) ed uninfusione continua di 120 ore di 5 - fluorouracile ( 1000 mg / m2 al giorno )  . 
in 6 pazienti stata ottenuta una risposta patologica completa ( 6 , 7% ) , in 39 pazienti ( 43 , 3% ) stata evidenziata una riduzione dello stadio iniziale di malattia . 
neoadjuvant systemic chemotherapy based on ox and 5 - uc associated with radiotherapy is well tolerated , with good results in terms of pathological response , disease control and survival , in rectal cancer patients . keywords locally advanced rectal cancer chemoradiotherapy oxaliplatin 5 - fluorouracil globale ( os ) e la sopravvivenza libera da malattia ( dfs ) sono state rispettivamente del 62 , 9% e 52 , 8% . 
nei pazienti affetti da tumore del retto , la chemioterapia pre - operatoria , basata sulluso delloxaliplatino ed il 5 - fluoruracile ed associata alla radioterapia , ben tollerata con buoni risultati in termini di risposta patologica , controllo di malattia e sopravvivenza . parole chiave tumore del retto localmente avanzato radio - chemioterapia oxaliplatino 5 - fluorouracile introduction introduzione in europe , colorectal rectal cancer ( crc ) is the second most common neoplasm in the population [ 1 ] , with approximately 138 , 000 new cases diagnostic every year . 
the most important surgical breakthrough in recent years was the advent of total mesorectal excision ( tme ) , an approach that has dramatically reduced the rates of local recurrence of advanced rectal tumours [ 3 ]  . 
 recent studies demonstrate that neoadjuvant treatment can lead to reduced local recurrence and significant tumour downstaging in advanced disease [ 4 ] ; in addiction , it ensures a greater chance of preserving the sphincter . 
two european trials , the european organisation for research and treatment of cancer ( eortc ) trial 22921 [ 8 ] and the fdration francophone de la cancrologie digestive ( ffcd ) trial 9203 [ 9 ] showed a significantly increased rate of complete pathological response and local control with the addition of chemotherapy [ 5 - fluorouracil ( 5 - fu ) ] to radiotherapy . 
even if pyrimidine - based schedules are often used , there is no consensus in europa il tumore colorettale ( crc ) la seconda neoplasia pi comune nella popolazione [ 1 ] ed ogni anno vengono diagnosticati circa 138000 nuovi casi . 
negli ultimi anni il cambiamento pi significativo nellambito chirurgico dovuto allavvento dellescissione mesorettale ( tme ) , con questo approccio chirurgico si ridotta drasticamente lincidenza di recidiva locale nei pazienti affetti da tumore rettale [ 3 ]  . 
 la letteratura dimostra che il trattamento pre - operatorio pu determinare una riduzione della recidiva locale ed una significativa riduzione delle dimensioni della malattia in caso di malattia avanzata [ 4 ] , inoltre pu garantire unalta possibilit di preservazione dello sfintere . 
 [ 5 ] hanno dimostrato che nei pazienti sottoposti a radio - chemioterapia ( crt ) pre - operatoria la percentuale di preservazione dello sfintere durante la chirurgia pi che raddoppiata rispetto ai pazienti sottoposti a trattamento post - operatorio . 
due studi europei , lo studio european organisation for the research and treatment of cancer 22921 [ 8 ] e lo studio federation francophone de cancrologie digestive ( ffcd ) 9203 [ 9 ] hanno dimostrato che aggiungendo alla radioterapia il trattamento chemioterapico ( 5 - fluorouracile ) si ottiene un significativo incremento della percentuale di risposta patologica completa e controllo lo572 radiol med ( 2013 ) 118 : 570582 about the gold standard chemotherapy regimen . 
our study retrospectively analysed toxicity , pathological response , local control and survival rates of crc patients treated with neoadjuvant crt . materials and methods patient selection between november 2002 and december 2010 , 94 patients with locally advanced rectal cancer were treated with neoadjuvant crt at the radiotherapy unit of the university of florence . 
before treatment , every patient underwent staging with digital rectal examination ( dre ) and chest and abdomen computed tomography ( ct ) to determine t stage and exclude liver and lung metastases . 
due to the use of oxaliplatin ( ox ) and its association with renal toxicity , kidney function was evaluated through creatinine ( cr ) and creatinine clearance ( crcl )  . 
conformal radiotherapy was delivered by a four - field box or three - field technique using high - energy x - photons ( 25 mv ) by a linear accelerator to a total dose of 45 gy over 5 weeks ( 1.8 gy in five fractions / week ) to the reference point according to the international commission on radiation units ( icru ) 5062 . 
clinical target volume ( ctv ) encompassed the tumour , defined by mr imaging and clinical evaluation , as well as total mesorectum , common and internal iliac and obturator lymph nodes . 
the lower limit of the ctv was , for both t3 and t4 disease , a minimum of 2 cm caudal to gross disease , and the upper margin was the rectosigmoid junction . 
il nostro studio ha analizzato retrospettivamente tossicit , risposta patologica , controllo locale e sopravvivenza nei pazienti affetti da tumore localmente avanzato del retto e sottoposti a radio chemioterapia pre - operatoria . 
 materiali e metodi selezione dei pazienti nel periodo compreso tra novembre 2002 e dicembre 2010 , 94 pazienti affetti da tumore del retto localmente avanzato sono stati trattati con crt neoadiuvante presso lunit di radioterapia delluniversit di firenze . 
tutti i pazienti sono stati sottoposti prima del trattamento a valutazione clinica ed esplorazione digitorettale ( dre ) , una tomografia computerizzata ( tc ) del torace e addome con mezzo di contrasto ( mdc ) per determinare lo stadio t e per escludere metastasi epatiche e polmonari . 
a causa della possibile nefrotossicit legata allimpiego delloxaliplatino , la funzionalit renale era testata con la creatininemia e clearance della creatinina . trattamento tutti i pazienti sono stati sottoposti ad un trattamento associato crt . 
la radioterapia ( rt ) conformazionale stata erogata con la tecnica a quattro campi ( four - field box ) o a tre campi , utilizzando fotoni ad alta energia ( 25 mv ) con un acceleratore lineare , per una dose totale di 45 gy per 5 settimane ( 1 , 8 gy in 5 frazioni settimanali ) prescritta al punto di riferimento in accordo con linternational commission on radiation units ( icru ) 5062 . 
la tc di simulazione stata eseguita in posizione prona , il belly board stato utilizzato per ridurre il volume di intestino compreso radiol med ( 2013 ) 118 : 570582 side - wall musculature or the bone . 
electronic portal images or cone - beam ct were used to verify positioning on the first day of treatment and weekly thereafter . chemotherapy was administered during the first and fifth weeks of radiotherapy ; the first day of treatment , patients received a bolus of ox ( 80 mg / m2 ) , and 5 - fu was given as a 120 - h continuous infusion at a dose of 1 , 000 mg / m2 per day . 
complete pathological response was defined as the absence of residual tumour at the time of histological examination ; tumour downstaging refers to a change in stage between pretreatment clinical and posttreatment clinical or pathological evaluation . 
 follow - up and evaluation postoperative follow - up was performed every 3 months for 2 years with clinical evaluation and cea , then every 6 months for a total of 5 years . 
le sezioni tc sono state acquisite con uno spessore di 5 mle immagini della rm sono state utilizzate per meglio definire il volume tumorale ma non stata eseguita per nessun paziente la fusione delle immagini rm - tc . 
il clinical target volume ( ctv ) comprendeva il tumore , definito dalle immagini della rm e dalla valutazione clinica , ed il mesoretto , i linfonodi iliaci comuni , interni ed otturatori . 
il limite inferiore del ctv era esteso , sia per lo stadio t3 che t4 , almeno 2 cm caudalmente alla malattia visibile , il margine superiore si trovava alla giunzione rettosigmoidea . 
lintestino , la vescica e le teste femorali erano disegnate come organi a rischio in tutte le sezioni tc , per ogni paziente veniva valutato un istogramma dose - volume . 
immagini portali elettroniche o la cone - beam tc erano utilizzate per verificare il posizionamento il primo giorno di trattamento e successivamente settimanalmente . la chemioterapia ( ct ) era somministrata durante la prima e quinta settimana di radioterapia ; il primo giorno di trattamento i pazienti ricevevano un bolo di oxaliplatino ( 80 mg / m2 ) , il fluorouracile era somministrato come uninfusione continua di 120 ore ad una dose di 1000 mg / m2 al giorno . 
la risposta patologica completa era definita come assenza di residuo tumorale al momento dellanalisi , la riduzione dello stadio tumorale ( downstaging ) si riferiva al cambio di stadio tra la valutazione clinica pretrattamento e la valutazione clinica o patologica posttrattamento . 
 follow - up e valutazione il follow - up post - operatorio stato eseguito ogni tre mesi per i primi due anni con la valutazione clinica ed il dosaggio dellantigene carcino - embrionario ( cea ) , poi ogni sei mesi per un totale di 5 anni . 
la recidiva locale era definita come evidenza di tumore entro la regione pelvica o perineale , la malattia metastatica era definita come evidenza di malattia al di fuori dellarea pelvica 574 radiol med ( 2013 ) 118 : 570582 gression models with stepwise selection were performed to identify the major predictors of death or lr . 
la probabilit cruda di morte o la lr era stimata utilizzando il metodo di kaplan - meier e le differenze tra i gruppi di pazienti erano stabilite con il test log - rank . 
la os e la dfs erano rispettivamente 62 , 9% e 52 , 8% . in 31 pazienti ( 34 , 4% ) la chirurgia stata eseguita entro 6 settimane dal termine del trattamento neoadiuvante , nel 65 , 6% dei pazienti la chirurgia stata eseguita successivamente per decisione del chirurgo . 
pathological tumour staging after surgery showed primary tumour downstaging ( ypt < 2 ) in 39 patients ( 43.3% ) , six of whom ( 6.7% ) had complete pathological response ( ypt0 )  . 
la stadiazione patologica del tumore dopo la chirurgia ha mostrato un downstaging ( ypt2 ) in 39 pazienti ( 43 , 3% ) , 6 dei quali ( 6 , 7% ) hanno presentato una risposta patologica completa ( ypt0 )  . 
dei 39 pazienti con risposta patologica completa dopo il trattamento neoadiuvante , 4 pazienti con stadio ct4 ( 10 , 3% ) e 10 con stadio ct3 ( 25 , 6% ) hanno presentato una riduzione dello stadio pt di pi di due punti ( rispettivamente : ct4 = pt2 o pt1 o pt0 e ct3 = pt1 o pt0 )  . 
degli 87 pazienti con linfonodi inizialmente stadiati come cn0 , 21 avevano linfonodi patologicamente positivi ( tutti pn1 )  . quando abbiamo analizzato i fattori che influivano sulla risposta patologica parziale ( pr ) e completa ( cr ) ( tabella 2 ) solo lo stadio ct risultato statisticamente significativo ; la malattia ct4 aveva una risposta migliore al trattamento neoadiuvante rispetto alla malattia in stadio ct3 ( p = 0 , 008 )  . 
 allanalisi univariata linterruzione della chemioterapia stato lunico fattore che influenzava in maniera statisticamente significativa la dfs e los ( tabelle 3 e 4 ) ; confrontando i pazienti che avevano ricevuto un solo ciclo di chemioterapia ( n = 12 ) ed i pazienti che non avevano avuto alcuna interruzione del trattamento sistemico ( n = 78 ) , la dfs a 5 anni era rispettivamente del 21 , 4% e 56 , 5% ( p = 0 , 001 ) e los era rispettivamente del 38 , 6% e 66 , 4% ( p = 0 , 028 )  . 
allanalisi multivariata , linterruzione della chemioterapia era lunico fattore prognostico per la dfs ( p = 0 , 0027 ) ed os ( p = 0 , 05 )  . 
solo 9 ( 10% ) pazienti avevano interrotto il trattamento radioterapico per pi di una settimana a causa della tossicit intestinale , tutti i 90 pazienti avevano raggiunto la dose programmata di radioterapia . 
la chemioterapia stata somministrata a tutti i pazienti , quando si sono verificate tossicit ematologiche ed intestinali , la dose di farmaco stata ridotta ( 11 , 1% dei pazienti ) e nei 12 ( 13 , 3% ) pazienti nei quali non si verificata la risoluzione dei sintomi , il trattamento stato interrotto . 
when haematological and gastrointestinal toxicity was recorded , chemotherapy dose was reduced ( 11.1% of patients ) ; in 12 ( 13.3% ) patients in whom the symptoms did not resolve , the treatment was stopped . 
our results are consistent with those of the german rectal cancer study [ 5 ] in which 421 ti trattati tumori del retto in stadio clinico t3 - t4 con radioterapia pre - operatoria e chemioterapia con sali di platino e 5 - fluorouracile . 
nel nostro studio la risposta patologica completa non ha determinato un miglior controllo locale , infatti la sopravvivenza libera da malattia non stata significativamente influenzata dalla risposta patologica ( p = 0 , 52 )  . 
 [ 12 ] hanno riportato i risultati del trattamento crt associato in 578 radiol med ( 2013 ) 118 : 570582 tabella 3 analisi della sopravvivenza libera da malattia ( dfs ) in 90 pazienti affetti da tumore del retto in accordo a caratteristiche individuali selezionate variabile pazienti , n eventi , n dfs , % hr ( 95%ci ) * hr ( 95%ci ) * * sesso maschio femmina et anni < 60 60 3 4 n0 n + distanza dallorifizio anale ( cm ) 5 > 5 interruzione rt no s interruzione cht no s risposta alla crt no s ( pr / cr ) 02 34 53 , 4 51 , 5 58 , 6 49 , 5 54 , 8 32 , 1 52 , 0 100 , 0 55 , 0 55 , 8 54 , 6 37 , 0 56 , 5 21 , 4 46 , 4 67 , 6 71 , 9 44 , 6 0 , 29 0 , 59 0 , 37 0 , 40 0 , 46 0 , 30 0 , 52 0 , 22 tutti i pazienti rt , radioterapia ; cht , chemioterapia ; crt , radio - chemioterapia ; pr , risposta patologica ; cr , risposta completa ; hr , hazard ratio * modello di regressione univariata di cox ; * * modello di regressione multivariata di cox con stepwise selection 52 , 8 0 , 001 3 , 8 ( 1 , 599 , 15 ) 4 , 67 ( 1 , 7112 , 76 ) patients with rectal cancer were randomly assigned to receive neoadjuvant crt and 402 patients to receive postoperative treatment . 
 [ 13 ] avevano analizzato 295 pazienti con un tumore rettale cii e ciii e sottoposti a radioterapia e chemioterapia basata sulluso di 5 - fluorouracile e poi a chirurgia . 
il downstaging non influenzava la prognosi oncologica dei pazienti con tumore rettale in cii , invece nei pazienti con malattia in stadio ciii lottenimento di un downstaging incrementava significativamente la sopravvivenza globale , ma non il controllo locale . 
we believe that other factors related more closely to sensitivity to preoperative crt for example , disease biology could probably better define patient prognosis . consistent with the literature , the 5 - year dfs in our study was 52.8%. 
eortc 22921 trial [ 8 ] randomised 1 , 011 patients with t3 or t4 resectable rectal cancer into four arms : preoperative chemoradiation , preoperative radiotherapy , preoperative radiotherapy with adjuvant chemotherapy and preoperative chemoradiation with adjuvant chemotherapy . 
the only factor that at univariate and multivariate analyses significantly influenced dfs in accordo ai dati della letteratura , nel nostro studio la dfs a 5 anni era del 52 , 8% . 
lo studio european organization for research and treatment of cancer ( eortc ) 22921 trial [ 8 ] aveva randomizzato 1011 pazienti con tumore del retto t3 o t4 in quattro bracci : crt pre - operatoria , radioterapia pre - operatoria , radioterapia pre - operatoria con chemioterapia adiuvante , e crt pre - operatoria con chemioterapia adiuvante . 
 ormai ben conosciuto leffetto radio - sensibilizzante della chemioterapia ed il fatto che laggiunta della chemioterapia alla radioterapia neoadiuvante nel tumore del retto determina un incremento del controllo locale [ 5 , 9 ]  . 
 it is well known that chemotherapy has a radiosensitiser effect and that the addition of chemotherapy to neoadjuvant radiotherapy for rectal cancer gives improved local control [ 5 , 9 ]  . 
 ox and 5 - fu chemotherapy in the preoperative setting showed an efficacy similar to other regimens , such as irinotecan , capecitabine , fluorouracil and leucovorin [ 10 , 14 , 15 ]  . in recent years , the role of ox in neoadjuvant treatment of rectal cancer has been debated after the results observed in the studio terapia adiuvante retto ( star ) and action clinique coordonnes en cancrologie digestive accord 12 / 0405 prodige 2 trials [ 16 , 17 ]  . 
 results showed that the addition of ox to fluorouracilchiaro come linterruzione del trattamento sistemico pu determinare un peggioramento della prognosi , come stato dimostrato nel nostro studio linterruzione della ct era il solo fattore prognostico che influenzava significativamente los ( p = 0 , 02 )  . 
la chemioterapia con oxaliplatino ed il 5 - fluorouracile ha dimostrato nel regime pre - operatorio efficacia simile ad altri schemi terapeutici quali quelli contenenti irinotecano , capecitabina , fluorouracile e leucovorin [ 10 , 14 , 15 ]  . 
 negli ultimi anni il ruolo delloxaliplatino nel trattamento pre - operatorio dei pazienti affetti da tumore del retto dibattuto dopo la pubblicazione dei risultati osservati negli studi star ed accord 12 / 0405 prodige 2 [ 16 , 17 ]  . 
nella nostra analisi sono stati evidenziati solo un grado1 e 2 di tossicit gastrointestinale , la ragione del differente profilo radiol med ( 2013 ) 118 : 570582 table 5 adverse events during chemoradiotherapy tabella 5 eventi avversi durante il trattamento radio chemioterapico event toxicity grade anaemia neutropaenia thrombocytopaenia anorexia nausea / vomiting diarrhoea evento grado di tossicit anemia neutropenia trombocitopenia anoressia nausea / vomito diarrea based chemotherapy with concurrent radiotherapy significantly increases toxicity without any gain in tumour response . 
the reason for the different toxicity profile of ox in our protocol and in the star and accord 12 / 0405 prodige 2 trials could be that our patients received only two infusions of ox on the first day of the first and fifth week of radiotherapy and not a weekly infusion , and also that chemotherapy was administered as inpatient treatment with the administration of supportive care if necessary . 
 di tossicit delloxaliplatino nel nostro studio e negli studi star e accord 12 / 0405 prodige 2 trials potrebbe essere dovuto alla differente modalit di somministrazione , infatti i nostri pazienti ricevevano solo due infusioni di oxaliplatino , il primo giorno della prima e della quinta settimana di radioterapia e non una somministrazione settimanale , inoltre tutti i pazienti eseguivano il trattamento chemioterapico in regime di ricovero con la possibilit di essere supportati con terapia qualora fosse stato necessario . 
nel nostro studio loxaliplatino ed il 5 - fluorouracile con radioterapia concomitante ha determinato un accettabile controllo locale e a distanza ( rispettivamente 2 , 2% e 25 , 6% ) , al contrario gli studi star e accord 12 / 0405 prodige 2 non hanno analizzato il controllo locale e a distanza del regime radio chemioterapico ma solo la risposta patologica . 
 a causa dellimportante ruolo della chemioterapia nel controllo locale e nella sopravvivenza , futuri studi clinici dovrebbero coinvolgere un numero maggiore di pazienti ed avere follow - up pi lunghi per investigare il vantaggio dellimpiego di nuovi farmaci , come i farmaci biologici , che hanno gi un ruolo di primaria importanza nel trattamento adiuvante e nella malattia metastatica . 
luso di una chemioterapia basata sulloxaliplatino ed il 5 - fluorouracile associata alla radioterapia ben tollerata , con un buon controllo locale di malattia ( dfs = 52 , 8% ) e prognosi ( os = 62 , 9% )  . 
orsola malpighi , azienda ospedaliero universitaria di bologna , via massarenti 9 , 40138 bologna , italy 3servizio aziendale di fisica sanitaria , azienda sanitaria dellalto adige , via l . 
 despite the different characteristics of new detector materials , frequently , the same radiological protocols previously optimised for screen film are still used with digital equipment without any critical review . 
images acquired with direct digital radiography equipment and a computed radiography system were analysed with specially developed commercial software with a four - alternative forced - choice method : the most promising protocols were then scored by two senior radiologists . 
the computed radiography system showed both better image quality and lower dose at lower energies ( 85 kvp and 95 kvp ) than those currently used ( 125 kvp )  . 
la radiologia digitale ha ormai sostituito quella analogica in molti ospedali : nonostante le caratteristiche fisiche e tecnologiche dei materiali che compongono i nuovi rivelatori siano completamente diverse rispetto agli accoppiamenti schermo - pellicola , spesso i protocolli radiologici ottimizzati per questi ultimi vengono usati anche con le apparecchiature digitali senza alcuna revisione critica . 
stata effettuata unanalisi su immagini radiografiche digitali acquisite con due sistemi , uno di direct radiography ed uno di computed radiography , mediante la statistica della scelta forzata a quattro alternative implementata su un software dedicato : i protocolli radiologici pi promettenti sono stati poi valutati quantitativamente da due esperti radiologi . 
il sistema di computed radiography ha mostrato sia una migliore qualit delle immagini sia una minore dose ad energie pi basse ( 85 kvp e 95 kvp ) di quella attualmente utilizzata ( 125 kvp )  . 
lapparecchiatura di direct radiography ha confermato prestazioni superiori in termini di dose e di qualit delle immagini rispetto al sistema di computed radiography . radiol med ( 2013 ) 118 : 540554 keywords thoracic radiography digital radiography image processing conclusioni . 
in generale , nellesame del torace eseguito con sistemi digitali si pu ottenere un miglior rapporto qualit dellimmagine / dose efficace abbassando la tensione del tubo radiogeno . parole chiave radiologia toracica radiografia digitale elaborazione dellimmagine introduction introduzione in recent years , storage phosphor - based computed radiography ( cr ) and flat - panel direct digital radiography ( ddr ) have been replacing the conventional screen - film ( sf ) technology in many radiological departments due to the numerous advantages of digital imaging [ 15 ]  . 
 the chest is an important example of this kind of examination because it is the most commonly performed diagnostic radiography procedure in radiology departments [ 1014 ]  . various contrast - detail phantoms are widely used to compare performances of systems for projective radiology in visualising low - contrast details [ 1523 ]  . 
in light of the findings of a previous report [ 24 ] , this study used the contrast - detail radiology ( cdrad ) phantom to acquire images with several posteroanterior ( pa ) chest radiological protocols in order to analyse the quality of each image vs . 
the imparted dose and propose protocols with the best compromise between image quality and patient dose . materials and methods imaging systems the ddr equipment investigated in this study was a csi : tl / asi : h - based flat - panel system axiom aristos ( siemens , germany )  . 
the system employs a 0.5 - mm - thick thalliumdoped caesium iodide phosphor layer directly deposited over an amorphous silicon plate containing an array of photodiodes and thin - film transistor switches for light detection and signal readout , respectively . 
the active area of the detector is 4343 cm2 , corresponding to a 3 , 0013 , 001 matrix with a pixel size of 143 the equipment enables virtually the entire range of radiographic applications to be performed in a room allowing movements around all three axes negli ultimi anni , grazie ai molti vantaggi che presenta limaging digitale , i sistemi di computed radiography ( cr ) basati sullimpiego di fosfori a memoria e quelli di direct radiography ( dr ) con pannello piatto stanno sostituendo la tecnologia schermo - pellicola ( sp ) tradizionalmente utilizzata allinterno delle unit operative di radiologia [ 15 ]  . 
 spesso con le apparecchiature cr o dr vengono ancora usati gli stessi protocolli che erano stati ottimizzati per i sistemi sp [ 6 ] , ma il k - edge ( cio lenergia per la quale si ha la maggior efficienza di assorbimento dei raggi x ) dei materiali con cui sono realizzati i rivelatori digitali non lo stesso che si aveva nei sistemi sp [ 79 ]  . 
per questo motivo , sarebbe necessaria unattenta ottimizzazione dei protocolli di esposizione , soprattutto quando limmagine comprende regioni anatomiche nelle quali sono presenti zone sia ad alta sia a bassa attenuazione . 
in particolare , il torace un esempio importante di questo tipo di procedure anche perch rappresenta lesame radiodiagnostico pi diffuso nei dipartimenti di radiologia [ 1014 ]  . per confrontare le prestazioni di diverse apparecchiature per radiologia proiettiva , quando si vogliono visualizzare dettagli a basso contrasto , sono stati ampiamente utilizzati diversi tipi di fantocci contrasto - dettaglio [ 1523 ]  . 
 alla luce dei risultati ottenuti in un precedente lavoro [ 24 ] , in questo studio stato utilizzato il fantoccio cdrad per acquisire delle immagini con diversi protocolli che possono essere associati alla radiografia del torace nella proiezione postero - anteriore ( pa ) , analizzando poi la qualit di ogni immagine rispetto alla dose erogata e valutando infine quali protocolli presentino il miglior compromesso fra la qualit dellimmagine ottenuta e la dose al paziente . materiali e metodi apparecchiature utilizzate lapparecchiatura dr analizzata in questo studio un sistema axiom aristos ( siemens , germania ) dotato di un pannello piatto csi : tl / asi : h . 
il sistema utilizza uno strato spesso 0 , 5 mm di fosfori di ioduro di cesio drogato al tallio , 542 radiol med ( 2013 ) 118 : 540554 direttamente depositati sopra un pannello di silicio amorfo contenente uno strato di rivelazione di fotodiodi e transistor a film sottile che permettono rispettivamente di rilevare la luce e leggere il segnale . 
inoltre , al detettore possono essere associate due griglie antidiffusione statiche , scelte in base allesame da eseguire : per le radiografie al torace si utilizza una griglia con 40 lamelle / cm , rapporto di griglia pari a 12 : 1 e distanza di focalizzazione ( fd ) pari a 180 cm . il sistema di cr analizzato in questo studio costituito da un lettore cr - 850 ( carestream health , usa ) , utilizzato insieme con degli schermi ( imaging plates , ip ) modello general purpose della dimensione di 3543 cm2 , come mostrato in figura 2 . 
ogni ip , che corrisponde ad una matrice di 20482500 pixel di 172 mm ognuno , costituito da fosfori a memoria composti da fluoro - alogenuri di bario attivati alleuropio . 
limmagine cr viene prodotta utilizzando un sistema radiografico composto da tubo radiogeno e teleradiografo , contenente una griglia con 36 lamelle / cm , rapporto di griglia pari a 12 : 1 e fd = 180 centrambi i sistemi sono installati presso lunit operativa di radiologia durgenza dellazienda ospedaliero - universitaria di bologna . aquisizione delle immagini la qualit delle immagini stata valutata attraverso le curve contrasto - dettaglio ottenute con il fatoccio cdrad modello 2.0 ( artinis medical systems , paesi bassi )  . 
nella figura 3 si mostra schematicamente il fantoccio : un parallelepipedo di plexiglas ( 26 , 526 , 51 cm3 ) contenente dei fori cilindrici di diametro e profondit crescente ( entrambe le dimensioni aumentano da 0 , 3 a 0 , 8 mm )  . 
i fori sono inseriti in una griglia di 225 celle : in ogni riga il diametro dei fori costante e la profondit aumenta in maniera esponenziale , mentre in ogni colonna la profondit costante e il diametro aumenta in maniera esponenziale . 
le prime tre righe contengono un unico foro per cella , mentre in ogni cella delle altre 12 righe sono presenti due fori identici ( il primo al centro e laltro in uno dei quattro angoli , scelto in maniera casuale )  . 
necessario identificare correttamente il foro nellangolo , secondo il metodo della scelta forzata con quattro alternative . durante le esposizioni il fantoccio cdrad stato inserito fra due strati aggiuntivi ( 55 mm anteriormente e 64 mm posteriormente ) di polimetilmetacrilato ( pmma ) , in modo da ottenere una radiazione diffusa ed unattenuazione simili a quelle che si hanno per la proiezione pa del torace di un paziente adulto : il tutto stato posizionato davanti al rivefig . 
two stationary antiscatter grids integrate the detector depending on which examination is carried out : for chest examinations , a 12 : 1 grid ratio with 40 strips / cm , 180 - cm focus - to - detector distance ( fdd ) grid was used . the computed radiography system studied was a cr - 850 image reader ( carestream health , usa ) used in conjunction with 3543 cm2 general - purpose imaging plates ( ip ) , as shown in figure 2 . 
cr imaging was produced using overcouch x - ray equipment and a wall bucky radiographic system ( for chest examinations : 36 strips / cm , 12 : 1 grid ratio , fdd = 180 cm )  . 
3a , b fantoccio cdrad ( a ) e sua immagine radiografica ( b )  . dent and emergency department ( a & e ) of our university hospital . image acquisition image quality was assessed by contrast - detail curve evaluation with the cdrad type 2.0 phantom ( artinis medical systems , the netherlands )  . 
in the first three rows , there is only one hole per square ; in the remaining 12 , there are two identical holes per square ( the first in the centre and the second in a randomly selected corner )  . 
correct identification of the corner detail represents a four - alternative forced - choice method . during exposure , the cdrad phantom was embedded between additional polymethylmethacrylate ( pmma ) layers ( 55 mm front and 64 mm behind ) , to provide scatter and to give attenuation similar to a pa adult chest projection , and placed against the detector - grid assembly of each equipment . 
le immagini sono state acquisite nella disposizione clinica ( griglia e camera a ionizzazione per il prodotto dosearea dap in posizione , fuoco da 0 , 6 mm , distanza fuoco rivelatore = 180 cm ) con diversi protocolli di esposizione , su entrambi i sistemi digitali . 
il potenziale del tubo stato diminuito da 125 kvp ( lenergia utilizzata nella nostra radiologia durgenza per effettuare la radiografia al torace pa sia con il sistema cr sia con quello dr ) fino a 70 kvp , ad intervalli di 5 kvp : per ogni valore di kvp il carico del tubo ( mas ) stato progressivamente aumentato in maniera manuale , secondo quanto permesso dal generatore , finch la dose efficace ( e ) risultava pari a circa 1 , 5 volte il valore attuale . per ogni protocollo sono state prodotte da tre a otto immagini in modo da ridurre la variabilit [ 9 ] ed il fantoccio cdrad stato leggermente spostato fra due esposizioni successive . 
per ogni immagine stata misurata la dose superficiale in ingresso ( entrance surface dose , esd ) , utilizzando un dosimetro a stato solido ( mult - o - meter 510 , unfors instruments , svezia ) regolarmente calibrato . 
tube potentials varied from 125 kvp ( that is , energy in use in the a & e for both cr and ddr ) down to 70 kvp at 5 - kvp intervals : for each kvp setting , the tube load ( mas ) was manually raised step by step , as allowed by the equipment generator until effective dose ( e ) was at least approximately 1.5 times the current standard value . three to eight replicated images were produced for all protocols to reduce variability [ 9 ] ; the cdrad plate was slightly moved between subsequent exposures . 
for each image , the entrance surface dose ( esd ) was measured with a regularly calibrated solid - state dosimeter ( mult - o - meter 510 , unfors instruments , sweden )  . 
effective dose was calculated from esd values using the national radiological protection board ( nrpb ) conversion coefficients [ 25 ]  . image quality evaluation to assess picture quality , digital imaging and communications in medicine ( dicom ) images for presentation , processed with the algorithm routinely applied to chest examinations , were considered . 
image evaluation was carried out with two methodologies : first , image groups were analysed communications in medicine ( dicom ) , sono state elaborate con lalgoritmo comunemente applicato agli esami del torace e la valutazione della qualit avvenuta secondo due metodologie . 
1.1 ( artinis medical systems , paesi bassi ) che permette di rilevare in maniera automatica le curve contrasto - dettaglio , applicando un filtro welch satterthwaite ( in pratica un test t di student modificato ) allimmagine dei fori per determinare la posizione del secondo foro fra i quattro possibili angoli . i risultati sono indicati sotto forma di un indice di qualit globale , il fattore di merito della qualit dellimmagine ( inverse image quality figure , iqfinv ) , definito come : iqfinv = ^ i = l , diametroi * profondit ( 1 ) in cui diametroi e profonditi indicano le dimensioni dellultimo foro visibile nella i - esima colonna [ 26 ]  . 
maggiore il fattore di merito e migliore la qualit dellimradiol med ( 2013 ) 118 : 540554 magine [ 27 ] : in letteratura stato dimostrato come questo valore sia una quantit affidabile per confrontare le prestazioni di diversi sistemi [ 24 ]  . successivamente , un sottoinsieme delle immagini stato analizzato con la stessa metodologia da due radiologi esperti , a cui sono state mostrate soltanto le immagini acquisite con i protocolli che erano risultati i pi promettenti ( cio quei protocolli per i quali sia la dose efficace era inferiore almeno del 3% a quella del protocollo attuale sia il valore di iqfinv era maggiore almeno del 3% rispetto al valore delliqfinv del protocollo attuale , in base a quanto calcolato dal software )  . 
i due radiologi potevano variare a piacimento la luminosit , il contrasto e lingrandimento delle immagini per poter meglio identificare la posizione del secondo foro , nel caso lo considerassero visibile . 
infine , come esempio , sono state acquisite con diversi protocolli alcune radiografie digitali del torace utilizzando il fantoccio antropomorfo del torace rsd - 77spl ( radiology support device , long beach , usa )  . risultati in figura 4 si mostra un esempio di grafico a punti che rappresenta i punteggi , corretti seguendo i criteri proposti dai costruttori del cdrad [ 26 ] , e la curva contrasto - dettaglio nonch il valore di iqfinv corrispondenti . 
in tabella 2 sono riportati i protocolli clinici analizzati per il sistema cr , con le relative esd e dose efficace , insieme con il valore di iqfinv calcolato dal programma software . 
rispetto al protocollo clinico attualmente utilizzato ( 125 kvp / 4 mas ) , la maggior riduzione di dose efficace ( 17% ) stata ottenuta con il protocollo 100 kvp / 6 mas , che presenta anche un aumento di iqfinv pari al 3 , 5% . 
altri protocolli da tenere in considerazione sono 95 kvp / 8 mas e 85 kvp / 10 mas , per i quali il valore di iqfinv aumenta ancora di pi ( rispettivamente del 5 , 8% e del 8 , 4% ) e la dose rimane comunque al di sotto di quella del protocollo attuale ( rispettivamente diminuisce del 4% e del 13% )  . come esempio del processo di ottimizzazione bisognerebbe anche considerare il protocollo 85 kvp / 12 mas : in questo caso si ha una qualit dellimmagine leggermente superiore rispetto alla tecnica con 85 kvp / 10 mas ( iqfinv = 2 , 46 vs iqfinv = 2 , 45 ) , per la dose aumenta del 12% rispetto al protocollo eseguito con 10 mas , che quindi da preferire . 
nellultima colonna della tabella 2 viene riportato il valore di iqfinv , ave ( cio il valore iqfinv calco lato dal software per questi protocolli , mediato con il punteggio ottenuto dai radiologi ) : tenendo in considerazione anche la valutazione degli osservatori umani , i fig . 
4 esempio di grafico in cui vengono riportati : i punti che rappresentano i punteggi , corretti secondo i criteri indicati dal produttore del fantoccio cdrad , la curva contrasto - dettaglio risultante ed il valore delliqfinv . with the cdrad analyser ver . 
1.1 software ( artinis ) for automated contrast detail evaluation , which applies a welch satterthwaite filter ( basically a modified student t test ) to the image of the holes in order to decide the location of the second hole among the four possible corners . 
results are expressed in terms of an overall image - quality index , the inverse image quality figure ( iqfinv ) being defined as iqfinv = ^ i = l diameteri * depthi , ( 1 ) where diameteri and depthi refer to the just visible hole of column i [ 26 ] ; the higher the score , the better the image quality [ 27 ]  . 
this figure of merit is a reliable quantity for performance comparison of different systems [ 24 ]  . subsequently , a restricted set of images was analysed with the same method by two senior radiologists : they scored only the images acquired with the most promising protocols ( defined as those having both an effective dose at least 3% lower than the e of the present protocol and an iqfinv value at least 3% higher than the iqfinv value of the present protocol , as calculated by the software )  . 
human observers were allowed to adjust image brightness / contrast and to magnify images to full resolution and were then requested to identify locations of the second holes if they were considered visible . 
finally , a few examples of digital chest x - ray images were taken with the different protocols using 546 results the anthropomorphic chest phantom rsd - 77spl ( radiology support device , long beach , ca , usa )  . protocolli migliori sembrano essere quelli a 95 kvp ed a 85 kvp . radiol med ( 2013 ) 118 : 540554 figure 4 shows an example of a diagram with dots representing scores , corrected by following criteria proposed by the in tabella 3 si riportano i protocolli clinici analizzati per il sistema dr , con le relative esd e dose efficace , insieme con il valore di iqfinv calcolato dal programma software . 
in questo caso il protocollo attuale ( 125 kvp / 1 mas ) sembra essere gi ottimizzato , anche se il protocollo a 75 kvp / 2 , 8 mas potrebbe costituire una valida alternativa : intable 2 computed radiography system : clinical protocols and corresponding entrance surface dose ( esd ) , effective dose ( e ) , inverse image quality figure ( iqfinv ) ( software programme ) and average iqfinv , ave ( software programme values averaged with scores obtained by two radiologists )  . 
in table 2 , clinical protocols for the cr system , the corresponding esd and effective dose are shown together with the resulting iqfinv values obtained with the software programme . 
when the human observers scores are taken into account , the best two protocols seem to be those at 95 kvp and at 85 kvp . table 3 shows clinical protocols for the dr system , and the corresponding esd and effective dose are shown together with the resulting iqfinv values obtained with the software prograin this case , protocol now used ( 125 kvp / 2 ) do la relazione che intercorre tra la qualit dellimmagine e la dose . 
in questo studio , la qualit dellimmagine , intesa come la capacit di distinguere il contrasto ed i dettagli da parte di una apparecchiatura radiologica , stata valutata utilizzando liqfinv e la dose stata misurata sfruttando la grandezza dose efficace . 
le pi recenti raccomandazioni della commissione internazionale per la protezione radiologica ( international commission on radiological protection , icrp ) sottolineano come la dose efficace sia un parametro critico se viene utilizzata indiscrimina tamente per quantificare il rischio radiologico di un paziente sottoposto ad esposizione medica , perch e stata definita sulla base della distribuzione in et ed in condizioni di salute della popolazione in genere e dei lavoratori e queste possono essere anche molto differenti dalla di stribuzione che si riscontra tra i pazienti [ 28 ]  . 
nel presente lavoro la grandezza e stata invece utilizzata per confrontare le dosi erogate dalle diverse modalit di imaging quando viene applicata una stessa procedura clinica , quindi ladozione di tale grandezza perfettamente aptable 3 direct digital radiography equipment : clinical protocols and corresponding entrance surface dose ( esd ) , effective dose ( e ) , inverse image quality figure iqfinv ( software program ) and iqfinv , ave ( software program values averaged with scores obtained by two radiologists )  . 
in this study , image quality intended as the overall contrast - detail performance of radiological equipment was scored by the iqfinv , and the dose was measured by the quantity effective dose . 
recent recommendations of the international commission on radiological protection ( icrp ) [ 28 ] state that effective dose is a critical parameter when it is used in an nondiscriminating way for quantifying radiological risk of patients undergoing medical exposures , because e has been defined on the basis of age distribution and health of workpropriata secondo quanto indicato nelle ultime raccoman dazioni . per confrontare i diversi protocolli , lutilizzo di un fantoccio a basso contrasto pu essere molto utile , ma lanalisi dovrebbe essere eseguita sia da osservatori umani sia da un programma software : il primo tipo di analisi importante perch la percezione delluomo ed i criteri decisionali sono elementi fondamentali nel processo di dia gnosi medica , mentre lutilizzo del software permette di avere un analisi intrinsecamente obiettiva . 
sebbene loggetto di test non sia un fantoccio antropomorfo , la di sposizione sperimentale dovrebbe permettere di ottenere in maniera clinicamente realistica una radiazione diffusa che simuli i livelli di rumore che si hanno per i diversi valori di potenziale del tubo e di dose , consentendo di trasporre i risultati ottenuti alla realt clinica . 
inoltre , il metodo statistico della scelta forzata con quattro alter native ha dei vantaggi rispetto allanalisi receiver operating characteristic ( roc ) [ 29 ] : una metodologia facilmente implementabile in un ambiente ospedaliero , nessun 550 radiol med ( 2013 ) 118 : 540554 ers / population in general , and those distributions could be very different among patients . 
in this study , e was used to compare doses delivered by various imaging modalities applied to the same clinical procedure , and therefore , the adoption of this quantity should be perfectly appropriate according to the most recent recommendations . to compare different protocols , a low - contrast phantom can be very useful , but the analysis should be performed by both a human observer and a software programme : the former is important because human perception and decision - making criteria are fundamental elements in the medical diagnostic process ; the latter is useful because of its intrinsic objective nature . 
although the test object is not an anthropomorphic phantom , the experimental setup should provide a clinically realistic localised scatter to mimic levels of quantum noise at the various tube potentials and dose values , allowing transfer of result to the clinical environment . 
moreover , advantages of using a four - alternative forced - choice compared with receiver operating characteristic ( roc ) analysis [ 29 ] are that the method is easy to implement in a hospital environment , no patients or volunteers are exposed to radiation , radiological protocol settings can be clearly controlled and phantom studies have a good correlation with studies based on the assessment of clinical images [ 30 ]  . digital systems have wide dynamic ranges and allow high variation in doses ; therefore , radiological protocols must be optimised to obtain good image quality at the lowest possible patient exposure according to the as low as reasonably achievable ( alara ) principle [ 28 ]  . 
images produced with the cr system at 95 kvp and 85 kvp have a slightly better quality than images produced at higher energies , and the effective doses are 4% and 13% lower , respectively , than e at 125 kvp . 
in figure 5 , cr images of a chest anthropomorphic phantom taken at 125 kvp , 95 kvp and 85 kvp are shown as an example . a similar , although less marked , trend was observed with the ddr equipment : the best image quality was obtained at 125 kvp , but at 75 kvp , the quality is still good and the dose is 18% lower . 
tube potentials lower than 70 kvp were not investigated because , as a general statement , they should produce an excessively low x - ray beam energy to allow photons to penetrate the patient without setting either very high milliampere to obtain acceptable contrast - to - noise ratio ( cnr ) and exposure times that are too long ( due to lower radiation yield ) for chest radiography compared with those required in the european quality criteria [ 31 , 32 ]  . the rationale behind the use of high energies for sf systems was more to keep a suitable range of optical densipaziente o volontario viene esposto alla radiazione , i protocolli radiologici possono essere facilmente controllati e gli studi effettuati su fantoccio hanno una buona correlazione con gli studi basati sulla valutazione di immagini cliniche [ 30 ]  . i sistemi digitali hanno un range dinamico ampio e permettono di avere grandi variazioni di dose , quindi importante che i protocolli radiologici siano ottimizzati per garantire una buona qualit dellimmagine con la minor esposizione possibile per il paziente secondo il principio as low as reasonably achievable ( alara ) [ 28 ]  . 
le immagini prodotte con il sistema cr a 95 kvp e 85 kvp hanno una qualit leggermente migliore delle immagini prodotte ad energie pi alte ed una dose efficace inferiore del 4% e del 13% rispetto a quella ottenuta a 125kvp . 
questo pu dipendere sia da un cambiamento nella risposta del rivelatore con lenergia dei fotoni sia da un maggior contrasto del segnale quando il potenziale del tubo radiogeno pi basso . 
in figura 5 si riportano , a titolo di esempio , le immagini di un fantoccio antropomorfo del torace acquisite con il sistema cr impostando 125 , 95 e 85 kvp . un andamento simile , sia pure meno marcato , stato osservato con lapparecchiatura dr : limmagine di miglior qualit stata ottenuta a 125 kvp , ma a 75 kvp la qualit ancora buona con un risparmio di dose del 18% . 
 i potenziali del tubo inferiori a 70 kvp non sono stati considerati perch produrrebbero unenergia del fascio troppo bassa affinch i fotoni possano penetrare il paziente : a ci si dovrebbe ovviare regolando i mas a valori molto alti in modo da produrre unimmagine con un rapporto contrasto - rumore ( contrast - to - noise ratio , cnr ) accettabile , ma il tempo di esposizione risulterebbe troppo lungo ( a causa della minore radiazione prodotta ) per la radiografia del torace rispetto a quanto richiesto dai criteri europei di qualit delle immagini radiologiche [ 31 , 32 ]  . con i sistemi sp era necessario lutilizzo delle alte energie pi per ottenere un range di densit ottiche adatto a visualizzare linterno del polmone ed il mediastino che per massimizzare la visibilit dei dettagli in queste regioni anatomiche [ 33 ]  . 
nelle apparecchiature digitali il range dinamico pi ampio e la possibilit di post - elaborare limmagine permettono il superamento di queste li mitazioni : pertanto lutilizzo di valori di kvp pi bassi di quelli attualmente usati per la radiografia del torace sembrerebbe essere fortemente raccomandato con i sistemi digitali . questa conclusione giustificata anche dallanalisi dei principali fattori fisici che influenzano la qualit dellimmagine : infatti nei sistemi digitali possibile regolare faradiol med ( 2013 ) 118 : 540554 fig . 
5a - c immagini di un fantoccio torace antropomorfico ottenute con il sistema di computed radiography e diversi protocolli radiologici : a 125 kvp , 4 mas ( a ) ; 95 kvp , 8 mas ( b ) ; 85 kvp , 10 mas ( c )  . ties across both mediastinum and the lung than to maximise detail conspicuity in these anatomical regions [ 33 ]  . 
with digital equipment , the wide dynamic range and the ability to postprocess images can overcome these limitations : therefore , lower kilovolt peak than those used at the present time cilmente anche in fase di visualizzazione il contrasto , che il pi importante parametro da considerare nella scelta del potenziale quando si vuole acquisire unimmagine di tessuti con diversi valori di attenuazione . 
inoltre , importante considerare anche il rumore allinterno dellimmagine 552 radiol med ( 2013 ) 118 : 540554 in chest examinations seem to be strongly recommended with digital systems . this conclusion is justified also from an analysis of the basic physical factors influencing image quality : indeed , in digital systems , contrast which is the most important parameter to consider when choosing tube potential for imaging tissues with different attenuations can be easily adjusted at acquisition and display . 
therefore , noise should also be considered , as detail detectability is not a function of contrast alone , and cnr provides a very useful indicator of the imaging performance of a radiological system [ 34 ]  . 
when the image is degraded by noise , the conspicuity of details is better as the cnr is higher , and the choice of kilovoltage with digital detectors could be based on the value of this parameter : a cnr increase as kilovolt peak decreased was described in a previous paper with a setup similar to that used in our study [ 24 ]  . ddr systems are reported by many to have a better image quality for a given radiation dose compared with cr systems [ 1719 , 35 , 36 ]  . 
indeed , ddr systems reach approximately a 30% higher value of the image quality figure of merit at < 60% of the effective dose compared with cr equipment . conclusions the limited dynamic range of screen - film technology definitely required the use of high energies for chest examinations : conversely , lower tube potentials could be used with digital systems ; therefore , technical parameters that are most appropriate need to be re - evaluated . 
this study shows that radiological protocols in use at the present time for chest examinations with digital systems can be improved by lowering the kilovolt peak and slightly increasing the milliampere values : in this way , less radiation dose is needed to produce images of the same quality , or even of better quality . 
the next step should be to implement the promising results of this phantom study in clinical images in order to achieve a considerable dose reduction in a large proportion of radiological examinations . conflict of interest none dato che la capacit di rilevare i dettagli non funzione del solo contrasto : il cnr costituisce un indicatore davvero utile delle prestazioni di un sistema radiologico [ 34 ]  . 
in altre parole , la visibilit dei dettagli dipende dal contrasto in relazione al livello di rumore di fondo ( cos come avviene nel cielo notturno : le stelle sembrano tanto pi luminose quanto pi la notte fonda )  . 
quando limmagine degradata dal rumore la visibilit dei dettagli anatomici aumenta allaumentare del cnr e la scelta del potenziale in un rivelatore digitale dovrebbe essere basata sul valore di questo parametro : il modo in cui il cnr aumenta al diminuire dei kvp descritto in un precedente lavoro , in cui veniva utilizzata una disposizione sperimentale simile a quella del presente studio [ 24 ]  . diversi autori hanno dimostrato come i sistemi dr abbiano una miglior qualit dellimmagine , a parit di dose di radiazione erogata , rispetto ai sistemi cr [ 1719 , 35 , 36 ]  . 
in questo lavoro , si mostra come i protocolli radio logici per gli esami al torace eseguiti con rivelatori a pannello piatto producano sia una migliore qualit dellimmagine sia un minor livello di dose se confrontati con gli schermi di fosfori a memoria . 
infatti , i sistemi dr per mettono di ottenere un valore del fattore di merito della qualit dellimmagine maggiore di circa il 30% e una dose efficace inferiore al 60% se confrontati con lapparecchiatura cr . conclusioni il range dinamico limitato della tecnologia schermo - pellicola richiedeva assolutamente luso di alte energie nellesecuzione degli esami al torace ; con i sistemi digitali , al contrario , possibile utilizzare dei potenziali pi bassi e quindi diventa necessario rivalutare quali parametri tecnici siano i pi appropriati per eseguire lesame . 
questo studio mostra che i protocolli attualmente utilizzati per effettuare le radiografie al torace con i sistemi digitali possono essere migliorati abbassando il valore dei kvp e aumentando leggermente i mas : in questo modo necessaria meno dose per ottenere immagini della stessa qualit , o persino di qualit superiore . 
donner2 1dipartimento di radiodiagnostica , apss di trento , trento , italy 2medicina nucleare , ospedale santa chiara , largo medaglie doro 9 , 38122 trento , italy correspondence to : u . 
to evaluate vascular uptake , the nuclear medicine physician employed both a semiquantitative method based on standardised uptake value ( suv ) determination and a qualitative method based on a visual score from 0 to 3 on the maximum intensity projection ( mip ) reformats . 
finally , a joint assessment was carried out between the nuclear medicine physician and the reporting radiologist , in which pet metabolic data were re - evaluated taking into account clinical data and baseline ct scans . 
mcnemars test was used to compare four types of analysis : semiquantitative ( cutoff 2.4 ) , qualitative with standard cutoff ( grade 2 ) , qualitative with reduced cutoff ( grade 1 ) and joint . 
per valutare la captazione vascolare il medico nucleare ha utilizzato sia il metodo semi - quantitativo , basato sulla misurazione del suv , che il metodo qualitativo , assegnando un punteggio visuale da 0 a 3 sulle ricostruzioni mip . 
lanalisi semiquantitativa ( sens 74 , 19% , spec 78 , 78% , acc 76 , 56% ) e quella qualitativa con soglia standard ( sens 64 , 51% , spec 84 , 84% , acc 75 , 00% ) non hanno presentato differenze statisticamente significative nella diagnosi di vgv , mentre il metodo qualitativo con soglia inferiore ( sens 93 , 54% , spec 75 , 75% , acc 84 , 37% ) risultato superiore a entrambe . 
one of the emerging applications of this form of metabolic imaging is assessing patients with nonspecific symptoms such as fever , joint pain and weight loss , in order to guide the complex process of differential diagnosis in case of inconclusive level - one laboratory and imaging investigations [ 1 ]  . 
lvv is responsible for up to 17% of cases of fever of unknown origin in elderly patients [ 2 ]  . lvv diagnosis traditionally relied upon clinical , laboratory , histopathological and imaging criteria defined by the american college of rheumatology ( acr ) in 1990 [ 3 ]  . 
biopsy , when obtained from the temporal artery for suspected horton arteritis , is often falsely negative ( 40% of cases ) as a result of segmental distribution of lesions with sparing of some vessel segments [ 5 ]  . 
in the event of diagnostic delays , the natural course of lvv leads to fibrotic stenosis of the vessel lumen , with possible thrombosis and limaging ibrido realizzato mediante fusione tra le acquisizioni della tomografia a emissione di positroni ( pet ) con 18f - fluoro - desossi - glucosio ( 18f - fdg ) e le immagini di tomografia computerizzata ( tc ) rappresenta uno strumento diagnostico con cui il radiologo , spesso coinvolto in sedute di refertazione congiunta con il medico nucleare o in consulti multidisciplinari , si deve confrontare quotidianamente , non solo per la patologia oncologica , ma anche per lo studio delle malattie infiammatorie e infettive . 
una delle applicazioni emergenti di tale imaging metabolico rappresentata dalla valutazione di pazienti con sintomi aspecifici quali febbre , artromialgia e calo ponderale , al fine di orientare la complessa diagnosi differenziale in caso di insuccesso delle indagini laboratoristiche e strumentali di primo livello [ 1 ]  . 
listopatologia , che rappresenta il gold standard nella diagnosi di infiammazione vascolare attiva , non pu essere impiegata di routine per il rischio legato al prelievo di tessuto , specie dellaorta : la biopsia , quando eseguita a livello dellarteria temporale nel sospetto di arterite di horton , spesso falsamente negativa ( 40% circa dei casi ) a causa della distribuzione segmentaria delle lesioni , con risparmio di alcuni tratti vasali [ 5 ]  . 
in caso di ritardo diagnostico , levoluzione naturale della vgv conduce alla stenosi fibrotica del lume , radiol med ( 2013 ) 118 : 633647 downstream infarction or to aneurysmal dilatation with dissection or rupture . 
moreover , pet - ct is used to evaluate the distribution of vascular lesions for selecting the biopsy site and to assess response to therapy during follow - up [ 8 ]  . 
a growing , though still not well - established , application is the study of forms of vasculitis previously considered typical of small and middle - size vessels , as a finding of involvement of large vessels is a negative prognostic factor that warrants a more aggressive immunosuppressive therapy . 
nowadays , in fact , the inflammatory involvement of large vessels is no longer considered exclusive to giant - cell arteritis , takayasu arteritis and isolated aortitis [ 911 ]  . 
il limite noto di tale esame rappresentato dalla risoluzione spaziale , in quanto non possibile rilevare lipercaptazione vascolare delle arterie di calibro inferiore a 45 m unapplicazione crescente , ma non ancora ben codificata , rappresentata dallo studio di vasculiti un tempo considerate tipiche dei vasi piccoli e medi , in quanto il riscontro di coinvolgimento dei grandi vasi rappresenta un criterio prognostico negativo , che rende necessaria una terapia immunosoppressiva pi aggressiva . 
exclusion criteria were absence of changes in inflammatory markers [ erythrocyte sedimentation rate ( esr ) , c - reactive protein ( crp ) and white blood cell count ( wbc ) ] in the 3 months prior to the examination , a finding of oncohaematological disease and lack of diagnosis at discharge . 
i criteri di esclusione sono stati : lassenza di alterazione degli indici di flogosi ( ves , pcr e conta dei leucociti ) nei 3 mesi prima dellesame , il riscontro di patologia onco - ematologica e la mancanza di diagnosi alla dimissione . 
 in 31 patients , the final diagnosis of lvv was formulated by the rheumatologist at discharge on the basis of clinical , laboratory and histological criteria defined by the acr [ 3 ] , morphological vascular examinations ( cdus , cta , mra , dsa ) and metabolic pet - ct imaging with [ 18f ] - fdg . 
of the 31 patients with lvv , 14 were found to be affected by hortons giant - cell arteritis ( only eight of them with a histological diagnosis on a temporal artery biopsy ) , five by takayasu arteritis , five by systemic antineutrophil cytoplasmic antibody ( anca ) vasculitis not otherwise specified , two by isolated aortitis , one by churg - strauss syndrome , one by wegener granulomatosis , one by behet vasculitis and one by vasculitis with coexisting seronegative human leukocyte antigen ( hla ) - b27positive spondyloarthritis . 
the remaining 33 patients found to be free of lvv were discharged with the following diagnoses : connective tissue disorder ( 13 ) , eight of which were of infectious origin ( three bacterial sepsis , three viral fever , one periaortic infection after aorto - bi - iliac bypass , one pelvic abscess ) ; small - vessel vasculitis ( 5 ) ( two behet disease , two cutaneous leukocytoclastic vasculitis , one systemic anca - positive vasculitis ) ; atherosclerotic vasculopathy ( 3 ) ; acute vascular dissection ( 2 ) ; ( one dissection of the superior mesenteric artery , one dissecting aortic aneurysm ) ; sarcoidosis ( 1 ) ; antiphospholipid syndrome ( 1 )  . 
acquisition parameters for the pet scan were 3 min per bed position and six bed positions on average ; ct scan parameters were 120 mas ( quality reference ma with care dose system for beam - intensity modulation ) and 120 kv . 
 reconstructions were obtained with a 168168 matrix , with field of view ( fov ) 50 c postprocessing with iterative algorithms ( flash 3d ) and / or ordered subset expectation gie . 
in met dei pazienti ( 32 su 64 ) al momento dellesame pet - tc era in corso la terapia corticosteroidea e / o immunosoppressiva , poich la diagnosi era gi stata formulata sulla base dei criteri clinico - laboratoristici oppure perch la gravit del quadro clinico aveva imposto di non ritardare la terapia . 
 la diagnosi finale di vgv stata formulata in 31 su 64 pazienti dal reumatologo alla dimissione sulla base dei criteri clinici , laboratoristici e istologici definiti dallamerican college of rheumatology [ 3 ] , degli esami vascolari morfologici ( eco - color - doppler , angio - tc , angio - rm , dsa ) e dellimaging metabolico pet - tc con 18f - fdg . 
dei 31 pazienti con vgv 14 sono risultati affetti da arterite gigantocellulare di horton ( solo 8 con diagnosi istologica su biopsia positiva dellarteria temporale ) , 5 da arterite di takayasu , 5 da vasculite sistemica ancanon meglio specificata , 2 da aortite isolata , 1 da sindrome di churg - strauss , 1 da granulomatosi di wegener , 1 da vasculite di behet , 1 da vasculite in corso di spondiloartrite sieronegativa hla - b27 +  . 
i rimanenti 33 pazienti su 64 in cui stato escluso limpegno vasculitico dei grandi vasi sono stati dimessi con diagnosi di connettivopatia in 13 casi , di eziologia infettiva in 8 casi ( 3 di sepsi batteriche , 3 di febbre virale , 1 di infezione periaortica in esiti di bypass aortobisiliaco , 1 di ascesso pelvico ) , di vasculite dei piccoli vasi in 5 casi ( 2 vasculite di behet , 2 vasculite cutanea leucocitoclasica , 1 vasculite sistemica anca + ) , di vasculopatia aterosclerotica in 3 casi , di dissecazione vascolare acuta in 2 casi ( 1 dissecazione della mesenterica superiore , 1 aneurisma aortico dissecante ) , di sarcoidosi in 1 caso , di sindrome da anticorpi antifosfolipidi in 1 caso . 
 pet - tc con 18f - fdg la scansione pet - tc stata effettuata con tomografo ibrido siemens biograph sensation , somatom 64 - slice ( siemens medical solutions ) dalla base cranica al tratto prossimale degli arti inferiori a 1 h 10 dalla somministrazione endovenosa di 18f - fdg ( 3 , 7 mbq / kg ) , dopo adeguata idratazione , digiuno di almeno 6 ore e verifica della glicemia ( inferiore a 130140 mg / dl )  . 
i parametri di acquisizione utilizzati sono stati per la pet di 3 minuti per lettino in media 6 lettini ( bed position ) e per la tc di 120 ma / sec ( quality reference ma con sistema care dose per la modulazione dellintensit del fascio ) e di 120 kv . 
la ricostruzione stata eseguita in matrice 168168 con campo di vista ( field of view , fov ) di 50 c la ricostruzione in post - processing tramite algoritmi iterativi ( flash 3d ) e / o ordered subset expectation maximization ( osem ) stata effettuata tramite workstation ( e.soft - leonardo workstation sms - siemens medical solutions ) dedicata sia allelaborazione delle immagini pet corrette per lattenuazione tramite i dati delle scansioni tc , sia alla loro fusione con queste ultime ai fini della localizzazione anatomo - strutturale dei foci di aumentato metabolismo . radiol med ( 2013 ) 118 : 633647 fig . 
1a - d pattern of vascular distribution of fluorine - 18 fluorodeoxyglucose ( [ 18f ] - fdg ) on coronal maximum intensity projection ( mip ) images of different patients . 
 maximization ( osem ) was carried out at a workstation ( e.soft - leonardo , siemens medical solutions ) dedicated to processing both ct - based attenuation - corrected pet images and pet - ct image fusion for anatomicalstructural localisation of foci of increased metabolism . distribution of [ 18f ] - fdg assessment of the areas of increased uptake of the labelled glucose analogue at vessel wall level , performed on mip images , led to the identification of four patterns unrelated to the degree of uptake : 1 . 
 distribuzione del 18f - fdg la valutazione su ricostruzioni mip dellaumentato metabolismo dellanalogo glucidico marcato a livello della parete vascolare , indipendentemente dal grado di captazione , ha portato allindividuazione di quattro pattern : 1 . 
data regarding sensitivity , specificity and accuracy of the different types of semiquantitative and qualitative analyses were calculated on the basis of the rheumatologists final diagnosis at discharge , which was taken as the reference standard . 
because all pet - ct examinations done at our centre are reported jointly by the nuclear medicine physician and the radiologist , we introduced a third analysis , called joint analysis , which took into account not only metabolic imaging but also clinical and baseline ct data to establish a personalised diagnosis , as recommended by previous authors [ 18 ]  . 
the different methods of analysis were finally compared using the mcnemar test , with significance set at p < 0.05. semiquantitative analysis semiquantitative analysis was performed after evaluating the vascular distribution of [ 18f ] - fdg uptake at five sites ( ascending aorta , epiaortic vessels , pulmonary arteries , descending aorta , iliac - femoral axes )  . 
 with such a method , we measured for each patient the maximum standardised uptake value ( suvmax ( bw ) ) , representing the highest activity of radiotracer in vascular wall tissue . 
 this nondimensional measure is calculated on the basis of the following parameters : body weight in kilograms , height in centimetres , administered activity in mbq , injection time , start time of acquisition , radiotracer half - life ( 109.8 min for [ 18f ] - fdg )  . 
 qualitative analysis qualitative analysis was based on visual comparison between vascular and hepatic uptake on the 5 - mm coronal mip reconstructions , with hepatic uptake taken as a reference . 
in the literature , score 1 is usually considered negative to avoid false positive errors , as can be found in elderly or diabetic patients with diffuse arteriosclerosis [ 4 , 12 , 17 ]  . 
we also evaluated the alternative hypothesis of considering score 1 to be positive , as even mild glucose uptake in patients receiving immunosuppressive therapy is known to indicate possible residual radiol med ( 2013 ) 118 : 633647 dificate in letteratura : lanalisi semi - quantitativa [ 14 , 15 ] e lanalisi qualitativa [ 16 , 17 ]  . 
i dati di sensibilit , specificit e accuratezza per i diversi tipi di analisi semi - qualitativa e quantitativa sono stati calcolati prendendo come standard di riferimento la diagnosi finale formulata dal reumatologo alla dimissione . 
dato che nel nostro centro la refertazione della pet - tc viene effettuata congiuntamente dal medico nucleare e dal radiologo , abbiamo introdotto una terza analisi , definita collegiale , che tiene conto non solo dellimaging metabolico , ma anche delle informazioni cliniche e delle immagini tc basali , per una diagnosi individualizzata come auspicato da alcuni autori [ 18 ]  . 
le diverse metodiche di analisi sono state infine confrontate utilizzando il test di mcnemar , con soglia di significativit p < 0 , 05 . analisi semi - quantitativa lanalisi semi - quantitativa stata condotta dopo aver valutato la distribuzione vascolare delluptake di 18f - fdg in 5 sedi ( aorta ascendente , tronchi epiaortici , arterie polmonari , aorta discendente , assi iliaco - femorali ) ; in particolare , stata disposta una region of interest tridimensionale ( roi 3d ) nella sede di massimo accumulo dellanalogo glucidico marcato . 
con tale metodo , per ogni paziente stato misurato il valore massimo di captazione standardizzata ( suvmax ) , indice dellattivit pi elevata del radiofarmaco nel tessu to delle pareti vascolari . 
tale misura adimensionale vie ne calcolata utilizzando i seguenti parametri : peso del paziente espresso in kg , altezza del paziente in centimetri , attivit al tempo della somministrazione espressa in mbq , tempo delliniezione , tempo dellinizio dacquisizione , tempo di dimezzamento del radioisotopo ( 109 , 8 minuti per il 18f - fdg )  . 
 analisi qualitativa lanalisi qualitativa stata effettuata mediante il confronto visuale su ricostruzioni di tipo maximum intensity projection ( mip ) coronali con spessore di 5 mm tra la captazione vascolare e quella del fegato , preso come riferimento . 
il grado 1 di solito in letteratura viene considerato negativo per evitare errori di falsa positivit , in quanto pu essere riscontrato nei soggetti anziani o diabetici con diffusa arteriosclerosi [ 4 , 12 , 17 ]  . 
stata valutata anche lipotesi alternativa , in cui il grado 1 ritenuto positivo , in quanto noto che nei pazienti gi sottoposti a trattamento immunosoppressivo anche una scarsa captazione dellanalogo glucidico marcato pu essere indice di attivit residua di malattia a livello dei grandi vasi [ 8 , 19 ]  . 
abdominal computed tomography ( ct ) scan with contrast medium ( a ) , obtained in an emergency setting for pain , clearly depicts enhancing concentric aortic wall thickening related to active large - vessel vasculitis ( lvv )  . 
after 1 week of high - dose corticosteroid therapy , positron emission tomography ( pet ) - ct ( b ) shows only mild fluorine - 18 fluorodeoxyglucose ( [ 18f ] - fdg ) uptake ( grade 1 ) at the level of abdominal aorta , with maximum standardised uptake value ( suvmax ) value of 2.1. 
mr angiography with gadolinium ( c ) demonstrates stenosis of the subclavian artery , of the abdominal aorta , of the superior mesenteric artery and of the right renal artery , associated with a triangular area of kidney infarction . 
la tc addome con mezzo di contrasto ( a ) , eseguita per dolore in urgenza , rileva un chiaro ispessimento concentrico di parete dellaorta con enhancement in rapporto a vgv in fase attiva . 
dopo una settimana di terapia corticosteroidea ad alte dosi , la pet - tc ( b ) rileva solo lieve captazione del 18f - fdg ( grado 1 ) a livello dellaorta addominale con valore massimo del suv di 2 , 1 . 
langio - rm con gadolinio ( c ) dimostra stenosi dellarteria succlavia sinistra , dellaorta addominale , della mesenterica superiore e dellarteria renale destra , associata a unarea triangolare di infarto del rene destro . 
radiological findings of pathological changes , such as lanalisi collegiale stata basata sul metodo qualitativo con soglia 1 , con lintroduzione di alcuni elementi correttivi di tipo clinico e radiologico segnalati in letteratura e considerati di aiuto per aumentare la specificit dellesame [ 1 , 7 , 20 ]  . 
le immagini pet - tc di fusione sui piani sagittale ( a ) , coronale ( b ) e assiale ( c ) fanno rilevare ipermetabolismo focale di grado 3 in corrispondenza della parete aortica ( suv = 4 , 5 )  . 
focal ( considered more compatible with atherosclerotic plaques than with lvv ) rather than linear uptake of [ 18f ] fdg at the level of the large vessels on mip reconstructions assessed by the nuclear medicine specialist ; 3 . 
degree of uptake in relation to clinical data , considering all elderly ( age > 70 years ) or diabetic patients with mild uptake ( = 1 ) at qualitative analysis not justified by immunosuppressive therapy to be negative . results distribution of [ 18f ] - fdg in the 31 patients with lvv ( lvv + ) , as assessed on mip reconstructions and considering that many patients exhibited more than one of the four distribution patterns , was as follows : 19 tram track ( 61% ) , 13 crossbow ( 42% ) , 12 lambda ( 38% ) , two focal ( 6% ) and two absent . 
in the remaining 33 patients without lvv ( lvv ) vascular distribution of [ 18f ] - fdg on mip reconstructions was : four tram track ( 12% ) , one crossbow ( 3% ) , three lambda ( 9% ) , three focal ( 9% ) and 25 absent . 
il grado di captazione in relazione ai dati clinici , considerando negativi i pazienti anziani ( et > 70 anni ) o diabetici con captazione di basso grado ( = 1 ) allanalisi qualitativa , non giustificabile dalla contemporanea somministrazione di terapia immunosoppressiva . risultati la distribuzione del 18f - fdg valutata sulle ricostruzioni mip , considerando che molti pazienti presentavano pi di uno dei quattro pattern descritti , stata la seguente nei 31 pazienti con vgv ( vgv + ) : 19 a binario ( 61% ) , 13 a balestra ( 42% ) , 12 a lambda ( 38% ) , 2 focale ( 6% ) , 2 assente . 
nei restanti 33 pazienti senza vgv ( vgv - ) , la distribuzione vascolare del 18f - fdg sulle ricostruzioni mip stata la seguente : 4 a binario ( 12% ) , 1 a balestra ( 3% ) , 3 a lambda ( 9% ) , 3 focale ( 9% ) , 25 assente . 
using 2 as a pathological cutoff value , qualitative analysis had 64.51 % senda vgv e 11 affetti da altre patologie . nellanalisi semi - quantitativa , il suvmax risultato in tutti i casi superiore a 1 , 2 , compresi i 33 pazienti senza vgv : tale valore di captazione vascolare era stato fissato come cut - off nello studio di kobayashi [ 15 ] , in cui si utilizzavano pazienti oncologici come controllo e non pazienti con elevazione degli indici di flogosi , ma sarebbe risultato non idoneo nel nostro campione di pazienti . 
nella nostra casistica , luptake vascolare stato considerato patologico quando 2 , 4 : con questa soglia , la sensibilit dellesame pet - tc stata del 74 , 19% , la specificit del 78 , 78% , laccuratezza del 76 , 56% ( tabella 1 )  . 
nei 33 pazienti vgv - , la media stata di 2 , 10 ( ds1 , 13 ) , nei 31 pazienti vgv + la media stata di 3 , 09 ( ds0 , 56 ) , una differenza statisticamente non significativa ( p = 2 , 76 ) utilizzando il test t per campioni indipendenti . 
invece , la differenza risultata significativa ( p < 0 , 001 ) , analogamente a quanto riportato da altri autori [ 12 ] , dividendo i pazienti con vgv in due sottogruppi sulla base della somministrazione di terapia immunosoppressiva : nei 20 pazienti in terapia , il suv medio stato di 2 , 61 ( ds0 , 35 ) , mentre negli 11 pazienti non in terapia la media stata di 3 , 92 ( ds0 , 70 )  . 
 nellanalisi qualitativa , il punteggio medio stato di 0 , 42 ( ds1 , 41 ) nei 33 pazienti vgvcontro una media di 1 , 93 ( ds 0 , 96 ) , nei 31 pazienti vgv + , differenza statisticamente non significativa ( p = 6 , 22 ) utilizzando il test t per campioni indipendenti . 
nei 20 pazienti vgv + in terapia immunosoppressiva , il punteggio medio stato di 1 , 5 ( ds2 , 12 ) , mentre negli 11 pazienti vgv + non in terapia il punteggio medio stato di 2 , 72 ( ds0 , 70 ) ; la differenza statistica tra i due sottogruppi stata significativa ( p < 0 , 001 )  . 
quando vengono inclusi come patologici anche i pazienti con captazione vascolare di grado 1 , la sensibilit aumenta notevolmente , risultando del 93 , 54% , ma la speci642 radiol med ( 2013 ) 118 : 633647 sitivity , 84.84% specificity and 75% accuracy . 
considering pathological also , patients with grade 1 uptake have sensitivity increases up to 93.54% but specificity falls to 75.75% , with an overall accuracy of 84.37% ( table 1 )  . 
in two cases , on the other hand , the false positive results could not be corrected : one diabetic patient with septic fever and diffuse grade 2 vascular uptake ; the other with dissection and linear uptake along the superior mesenteric artery owing to the presence of intramural haematoma mistaken for wall thickening due to vasculitis ( follow - up ct helped establish the correct diagnosis )  . 
finally , qualitative analysis with pathological cutoff 1 was compared with the nuclear physicians and radiologists joint analysis , which took into account three corrective factors as well as the visual comparison between vascular and hepatic uptake . 
complessivamente , con lanalisi collegiale la sensibilit della pet - tc stata del 93 , 54% , la specificit del 93 , 93% , laccuratezza del 93 , 75% ( tabella 1 )  . 
in due casi , invece , non stato possibile correggere lerrore di falsa positivit : un paziente diabetico con febbre settica e diffusa captazione vascolare di grado 2 , laltro con dissecazione e accumulo lineare del radiofarmaco lungo larteria mesenterica superiore , per la presenza di ematoma intramurale che stato scambiato per ispessimento parietale da vasculite ( gli esami tc di follow - up hanno consentito di giungere alla diagnosi corretta )  . 
 confronto statistico dal confronto statistico con il test di mcnemar , la differenza risultata non significativa tra il metodo semi - quantitativo con cut - off del suv > 2 , 4 e il metodo qualitativo con punteggio patologico 2 sulle ricostruzioni mip ( p = 0 , 1824 )  . 
invece , lanalisi qualitativa con soglia patologica 1 ha ottenuto una performance diagnostica statisticamente superiore sia al metodo semi - quantitativo ( p = 0 , 0455 ) che al metodo qualitativo con punteggio patologico di 2 e 3 ( p = 0 , 0015 )  . 
diagnosing lvv is complicated by three factors : the lack of validated criteria for a pathological cutoff , the greater frequency of this disease in elderly patients with arteriosclerotic abnormalities and , above all , the concurrent administration of immunosuppressive agents , especially high - dose corticosteroids [ 8 , 12 , 17 ]  . 
we therefore attempted to compare some methods for analysing pet - ct study to identify the most reliable for diagnosing lvv , emphasising the advantages produced by cooperation between radiologist and nuclear medicine specialist . study limitations are the influence that pet - ct examination had on the rheumatologists final diagnosis ; the inability to obtain a histological diagnosis in the majority of patients with lvv , which implies a lack of a real gold standard ; and the lack of correlation between inflammatory markers and vascular uptake , even though this aspect is still debated , as some studies have revealed a poor correlation both at diagnosis [ 4 ] and during the follow - up [ 19 ] between pet - ct findings and inflammatory indices . the reported sensitivity of pet - ct in individuals with elevated inflammatory markers not undergoing corticosteroid therapy varies between 77% and 92% and specificity between 89% and 100% [ 2 ]  . 
however , on the one hand , these studies do not evaluate the influence of immunosuppressive therapy on pet - ct results and , on the other hand , oncological patients or healthy individuals are used as comparison group for the vascular uptake [ 1417 ]  . 
these two factors immunosuppressive therapy and systemic inflammatory condition make our sample more closely reflective of the daily reality of those involved in reading pet - ct examinations performed for suspected lvv compared with other studies . 
 [ 12 ] , questo studio retrospettivo prende in considerazione un campione di pazienti a elevato sospetto reumatologico , rappresentativo delle problematiche incontrate nella pratica quotidiana da chi affronta la refertazione degli esami pettc . 
la diagnosi di vgv , infatti , resa complessa da tre fattori : la mancanza di criteri validati di soglia patologica , la maggiore frequenza di questa malattia nei pazienti anziani che presentano alterazioni vascolari arteriosclerotiche e , soprattutto , la concomitante somministrazione di farmaci immunosoppressivi , specie i corticosteroidi ad alte dosi [ 8 , 12 , 17 ]  . 
perci si cercato di confrontare alcuni metodi di analisi dellesame pet - tc per individuare il pi affidabile nella diagnosi di vgv , sottolineando i punti di forza che possono scaturire dalla collaborazione tra radiologo e medico nucleare . i limiti di questo studio sono rappresentati in primo luogo dallinfluenza che lesame pet - tc ha esercitato sulla diagnosi finale del reumatologo , in secondo luogo dallimpossibilit di ottenere la diagnosi istologica nella maggioranza dei casi di vgv che comporta la mancanza di un reale goldstandard e , infine , dalla mancata associazione tra i markers sierologici dellinfiammazione con il livello di captazione vascolare dellanalogo glucidico radiomarcato , anche se tale aspetto ancora dibattuto perch alcuni studi hanno rilevato scarsa correlazione sia nella fase diagnostica [ 4 ] che di follow - up [ 19 ] tra il quadro pet - tc e gli indici di flogosi . in letteratura , la sensibilit dellesame pet - tc varia dal 77 al 92% e la specificit dall89 al 100% in individui con elevazione degli indici di flogosi non sottoposti a trattamento corticosteroideo [ 2 ]  . 
tuttavia , in tali studi da un lato non viene valutata linfluenza della terapia immunosoppressiva sui risultati dellesame pet - tc , dallaltro la captazione vascolare viene in genere confrontata con quella di pazienti oncologici o sani [ 1417 ] utilizzati come gruppo di controllo . 
 inoltre , tutti i pazienti , essendo di provenienza reumatologica , presentavano uno stato infiammatorio generalizzato con elevazione degli indici di flogosi , come testimoniato dallalto numero di casi con attivazione midollare anche tra i pazienti vgve dalla maggiore captazione vascolare , con suv superiore a 1 , 2 in tutti i casi . 
questi due fattori , terapia immunosoppressiva e stato infiammatorio sistemico , rendono il campione da noi esaminato pi vicino alla realt quotidiana di chi si confronta con la lettura degli esami pet - tc nel sospetto di vgv rispetto ad altri studi . 
in our series , in contrast , the difference between the two groups was not significant , so we did not consider it useful to propose a lower cutoff value to distinguish lvv + patients undergoing immunosuppressive therapy from patients lvv patients . the presence of inflammatory changes at the level of atherosclerotic plaques in elderly patients or those with cardiovascular risk factors is the greatest cause of false positive results on pet - ct [ 18 ]  . 
an evaluation of a group of patients with carotid stenosis revealed that around one third of plaques had an suv > 1.6 at fdg - pet : such increased metabolism is related to the presence of macrophage - rich lipidic areas and to plaque instability [ 21 ]  . 
we therefore thought it would be justified to adopt a suv cutoff value of > 2.4 , as also used in a study of patients with acute aortic syndrome [ 23 ] , in order to avoid false positive errors . other known pet - ct criteria for distinguishing lvv from inflammatory atherosclerotic changes are the typical crossbow pattern at the level of the epiaortic vessels , linear uptake along the vessels ( atheromatous plaques have focal uptake corresponding to wall calcifications ) and response to corticosteroid treatment [ 7 ]  . 
as regards the pattern of vascular uptake , our study confirms that tram - track and , especially , crossbow patterns are the most characteristic if not pathognomonic of a diagnosis of lvv , whereas the focal pattern is the least specific . 
the lambda appearance should not be underestimated and should be considered typical of arteriosclerosis [ 24 ] : in our experience it was found with non - negligible frequency ( 38% ) in the group of patients with lvv . 
clearly , to improve pet - ct diagnostic reliability in the presence of a lambda pattern , one should consider the extent of vascular uptake , association with other patterns in cases of diffuse vascular involvement and absence of aorto - iliac - femoral calcifications on ct scans . the masking effect produced by immunosuppressive therapy is a known cause of false negative results on pet - ct [ 4 , 17 , 19 ] , such that to increase its sensitivity in diagnosing lvv , it is recommended that corticosteroid therapy be suspended before the examination , even though the severity of the patients condition and clinical requirements often do not allow this . 
nella nostra casistica , invece , la differenza tra i due gruppi risultata statisticamente non significativa e pertanto non abbiamo ritenuto utile proporre un valore di cut - off pi basso per distinguere i pazienti con vgv + in terapia immunosoppressiva da quelli vgv -  . la presenza di alterazioni infiammatorie a livello delle placche aterosclerotiche in pazienti anziani o con fattori di rischio cardiovascolare la causa pi frequente di falsi positivi allesame pet - tc [ 18 ]  . 
la valutazione di un gruppo di pazienti con stenosi carotidea ha rivelato che in circa 1 / 3 delle placche presente captazione con suv > 1 , 6 alla fdg - pet : tale aumentato metabolismo correlato alla presenza di aree lipidiche ricche di macrofagi e a instabilit della placca [ 21 ]  . 
da uno studio prospettico su ampia casistica emerso che luptake vascolare aumenta con let e , dopo i 60 anni , il suv pu presentare valori in media di 2 , 010 , 5 [ 22 ]  . 
quindi , ci sembrato giustificato adottare un valore di cut - off del suv > 2 , 4 , utilizzato anche in uno studio su pazienti con sindrome aortica acuta [ 23 ] , al fine di evitare errori di falsa positivit . altri criteri pet - tc noti per distinguere la vgv dalle alterazioni infiammatorie aterosclerotiche sono la distribuzione tipica ai tronchi epiaortici con aspetto a balestra , la captazione lineare lungo i vasi , mentre le placche ateromasiche hanno captazione focale spesso in corrispondenza di calcificazioni parietali e , infine , la risposta al trattamento corticosteroideo [ 7 ]  . 
per quanto riguarda il pattern di distribuzione della captazione vascolare , il nostro studio conferma che laspetto a binario e soprattutto quello a balestra sono i pi caratteristici , se non patognomonici , per la diagnosi di vgv , mentre laspetto focale il meno specifico . 
laspetto a lambda non va sottovalutato , considerandolo tipico dellarteriosclerosi [ 24 ] : nella nostra esperienza stata riscontrata con frequenza non trascurabile ( 38% ) nel gruppo di pazienti vgv +  . 
di certo , al fine di aumentare laffidabilit diagnostica della pet - tc in presenza di un pattern a lambda vanno considerati il grado di captazione vascolare , lassociazione con altri pattern in caso di interessamento vascolare diffuso e lassenza di calcificazioni aorto - iliaco - femorali nelle scansioni tc . leffetto mascheramento indotto dalla terapia immunosoppressiva una causa nota di errore di falsa negativit dellesame pet - tc [ 4 , 17 , 19 ] tanto che , per aumentare la sensibilit nella diagnosi di vgv , si raccomanda di sospendere la terapia corticosteroidea in anticipo ; tuttavia , la severit delle condizioni dei pazienti e le esigenze cliniche spesso non lo consentono . 
nella nostra casistica , la sensibilit dellanalisi qualitativa migliorata in maniera statisticamente significativa ( dal 64 , 5 al 93 , 5% ) , includendo i gradi 1 di captazione vascolare , anche se la specificit si abbassata dall84 , 8 al 75 , 7% . 
di certo , nei pazienti in terapia immunosoppressiva la sola misurazione semiquantitativa del suv non un criterio sufficiente per la diagnosi di vgv , ma pu essere di aiuto nel follow - up per valutare la risposta al trattamento [ 4 , 15 , 25 ]  . 
clearly , in patients undergoing immunosuppressive therapy , semiquantitative measurement of suv alone is not a sufficient criterion for a diagnosis of lvv , although it may be helpful in assessing response to treatment during the follow - up [ 4 , 15 , 25 ]  . 
the debate on this topic is still open , as persisting uptake over time may depend not only on the reactivation of arteritis but also on vascular remodelling with neoangiogenesis and wall fibrosis [ 8 ]  . statistical comparisons demonstrated that the qualitative analysis with a pathological cutoff 2 had a similar diagnostic performance to the semiquantitative method with cutoff 2.4 ; on the other hand , qualitative analysis proved to be superior to the semiquantitative method when we included patients with grade 1 vascular uptake , who are normally not considered pathological in other studies , due to the risk of exchanging inflammatory atherosclerotic changes for vasculitis [ 20 ]  . 
the reason is no doubt the high rate ( 50% ) of patients receiving immunosuppressive therapy before undergoing pet - ct , which reflects the real situation of the rheumatology referrals in our series . 
actually , in lvv + patients receiving immunosuppressive therapy , both mean vascular uptake measured with suv and mean visual score obtained on mip reconstructions proved to be substantially lower than those of lvv + patients not receiving therapy , and the difference was statistically significant . finally , joint analysis demonstrated that correlation with ct images and clinical data can increase pet - ct specificity in diagnosing lvv if elderly patients not undergoing immunosuppressive therapy with grade 1 uptake and those with focal uptake in correspondence with wall calcifications seen on baseline ct are considered negative . 
qualitative analysis of uptake on mip reconstructions aperto , poich luptake persistente a distanza di tempo potrebbe dipendere non solo dalla riattivazione di arterite , ma anche dal rimodellamento vascolare con neoangiogenesi e fibrosi di parete [ 8 ]  . dal confronto statistico , lanalisi qualitativa con soglia patologica 2 ha dimostrato una performance diagnostica analoga al metodo semi - quantitativo con cut - off del suv 2 , 4 , mentre lanalisi qualitativa risultata superiore al metodo semi - quantitativo quando si includono i pazienti con captazione vascolare lieve di grado 1 , che normalmente vengono considerati non patologici negli altri studi per il rischio di scambiare per vasculite le alterazioni infiammatorie aterosclerotiche [ 20 ]  . 
il motivo sicuramente attribuibile allalto tasso ( 50% ) di pazienti gi in terapia immunosoppressiva al momento dellesame pet - tc , che rispecchia la situazione reale dei pazienti di provenienza reumatologica nella nostra casistica . 
in effetti , nei pazienti vgv + in terapia immunosoppressiva , sia la captazione vascolare media misurata tramite suv che il punteggio medio ottenuto dal confronto visuale sulle ricostruzioni mip sono risultati nettamente inferiori a quelli dei pazienti vgv + senza terapia , con differenza statisticamente significativa . infine , lanalisi collegiale ha dimostrato che , grazie alla correlazione con le immagini tc e ai dati clinici , si pu aumentare la specificit dellesame pet - tc nella diagnosi di vgv , se vengono giudicati negativi i pazienti anziani non sottoposti a terapia immunosoppressiva con captazione di grado 1 o quelli con captazione focale in corrispondenza di calcificazioni parietali evidenziate nella tc basale . 
nella nostra casistica , i falsi positivi sono stati causati anche dalla presenza di dissecazione arteriosa o di infezioni perivascolari : in entrambe le situazioni , la rivalutazione attenta delle immagini tc basali nellanalisi collegiale ha consentito di ridurre il numero di tali errori . 
nellanalisi semi - quantitativa il cut - off 2 , 4 del suv valido per ridurre i falsi positivi da alterazioni aterosclerotiche , ma non assolutamente applicabile nei pazienti gi in terapia immunosoppressiva a causa della bassa sensibilit ; 2 . 
review of baseline ct images can help exclude a diagnosis of vasculitis in the case of increased vascular uptake at the level of wall calcifications , inflammatory collections with gas bubbles and aortic dissection . in our experience , cooperation between radiologist and nuclear medicine physician creates an added value in interpreting pet - ct examinations , which must be personalised for the individual patient . 
to this end , it is important to take into account not only the degree of vascular uptake but also ct images and clinical - laboratory data . grado 1 di captazione nei pazienti in terapia immunosoppressiva ; 3 . 
this study was undertaken to demonstrate the effectiveness of ultrasound ( us ) - guided placement of porta - cath ( pc ) through the right internal jugular vein ( rijv ) by evaluating the onset of early and late complications . 
in order to evaluate pneumothorax ( pnx ) , all patients underwent chest x - ray a few hours after the end of the procedure unless there were clinical indications . 
this procedure incurs very small number of complications compared with other positioning techniques using accesses such as the subclavian vecomplications recorded in our study are comparable , in type and riassunto obiettivo . 
le complicanze che abbiamo osservato sono paragonabili sia in termini di incidenza che di tipologia a radiol med ( 2013 ) 118 : 608615 incidence , to those found by other authors , with the most frequent being device infection . quelle riscontrate da altri autori ; infatti anche dal nostro studio emerge che linfezione del dispositivo risulta essere la complicanza pi frequente . keywords port - a - cath ultrasound guidance rijv complications parole chiave port - a - cath guida ecografica vgid complicanze introduction introduzione in recent years we have witnessed a considerable increase in the number of port - a - cath ( pc ) placements due to the continually growing number of applications for this device . 
 prescription of this system is mainly oncological [ 1 ] , but the pc can also be used for blood sampling or blood transfusion to avoid repeated searches for peripheral veins . 
until a few years ago , injection flow was a limit ; at present , thanks to the infusion set compatible with some devices , contrast media can be injected with flows up to 5 ml / s . 
very often , placement of venous pc was , and is still , carried out by puncturing the subclavian vein using anatomical landmarks [ 2 ] , but placement of these devices can also be performed through puncture of the subclavian vein under ultrasound ( us ) guidance [ 3 ]  . 
however , in our experience , puncture of the right internal jugular vein ( rijv ) under us guidance proves to be easier for the operator and considerably reduces the risk of complications , particularly pneumothorax [ 4 ]  . 
us guidance also provides crucial information with regard to venous access patency or the presence of intraluminal thrombosis . the aim of our study was to demonstrate the effectiveness of pc placement through the rijv by evaluating the type and frequency of procedural complications . materials and methods this was a retrospective study that evaluated early and late complications and efficacy of us - guided puncture of the rijv for pc placement of pc . 
inoltre con alcuni pc possibile eseguire anche esami contrastografici , e , se fino a qualche tempo fa il flusso di iniezione ne rappresentava un limite , oggi grazie ai set di infusione compatibili con alcuni dispositivi , si pu effettuare liniezione di mezzo di contrasto con flussi fino a 5 ml / s . 
molto spesso , in particolare in passato , il posizionamento di pc venosi veniva e viene a tuttoggi effettuato attraverso la puntura della vena succlavia mediante reperi anatomici [ 2 ] , ma pu essere eseguito anche attraverso il reperimento del vaso sotto guida ecografica [ 3 ]  . 
con lincedere del tempo , lutilizzo , sempre pi diffuso , della puntura eco - guidata ( us ) , specie per la radiologia interventistica , ha sensibilmente ridotto il numero di complicanze [ 1 ]  . la vena succlavia destra il vaso che pi frequentemente viene utilizzato , ad oggi , come accesso , tuttavia nella nostra esperienza , grazie allausilio della guida us , la puntura della vena giugulare interna di destra ( vgid ) risulta essere pi agevole per loperatore e permette di ridurre notevolmente il rischio di complicanze , in particolare lo pneumotorace ( pnx ) [ 4 ]  . 
tra laltro con questo accesso la gestione di un possibile ematoma risulta essere pi facile rispetto ad un eventuale emotorace causato da una puntura accidentale dellarteria succlavia [ 4 ]  . 
lausilio della guida us inoltre fornisce indiscutibilmente delle informazioni di estrema importanza riguardo la perviet dellaccesso venoso e / o la presenza di eventuali trombosi intraluminali . questo lavoro nato con lo scopo di dimostrare lefficacia del posizionamento di pc venosi , attraverso la vgid sotto guida ecografica , valutando il tipo e la frequenza delle complicanze procedurali . 610 radiol med ( 2013 ) 118 : 608615 fig . 
exclusion criteria were active infection , coagulopathy ( defined as platelet count < 50 , 000 l and / or prothrombin time ( pt ) > 18 s ) and life expectancy < 6 months . 
after double sterilisation ( alcohol and betadine ) of the right thorax and neck , local anaesthesia ( 20 ml mepivacaine ) was applied and a skin incision made parallel to langers lines . 
the catheter materiali e metodi il nostro uno studio retrospettivo che volge lattenzione alla valutazione delle complicanze precoci e tardive e allefficacia della tecnica di puntura us guidata della vgid per il posizionamento di pc . 
dal 30 giugno 2008 al 30 giugno 11 sono stati posizionati presso lunit operativa di radiologia del nostro ospedale 695 pc in 694 pazienti ( 387 femmine , 307 maschi ) con et compresa tra 27 e 89 anni ( et media 58 ) candidati alla chemioterapia infusionale . 
i criteri di esclusione dei pazienti dallo studio sono : infezione in atto , coagulopatie [ definita come conta piastrinica < 50000 l e / o tempo di protrombina ( pt ) > 18 secondi ] , aspettativa di vita inferiore ai 6 mesi . 
caudalmente alla clavicola facciamo partire il tunnel fino al sito di venopunradiol med ( 2013 ) 118 : 608615 tura , a tal fine utilizziamo un tunnelizzatore , che verr poi piegato a 90 per facilitarne luscita a livello del sito di venopuntura . 
 per effettuare la connessione del pc , eseguiamo una sutura di fissazione tra langolo della tasca e la base del pc , effettuiamo la connessione tra catetere e reservoir e dopo aver testato il funzionamento del dispositivo con liniezione allinterno del catetere 0 , 5 ml di eparina diluiti in circa 2 ml di soluzione fisiologica , lo adagiamo e lo fissiamo nella tasca . 
 per effettuare la chiusura della tasca e del sito di venopuntura , suturiamo la breccia chirurgica con fili riassorbibili sottocutanei ed intradermici ed il sito della venopuntura con steri - strip . 
3 creazione della tasca sottocutanea . was advanced to the junction of the superior vena cava and right atrium , and the introducer was clamped with fingers . to estabilish pc connection a fixation suture was performed between the corner of the pocket and the base of the pc and a connection made between the catheter and reservoir . 
then , after assuring proper device functioning with an injection of 0.5 ml heparin diluted in about 2 ml saline , the device was fixed inside the pocket . the surgical wound was closed with absorbable subcutaneous and intradermal threads , and the venipuncture site was closed with steri - strip . per la visualizzazione della vgid abbiamo usato ecografo esaote preirus , sonda ecografica lineare 513 mhz , e copri - sonda sterile . us guidance was provided by an esaote preius system , with a 513 mhz linear - array probe and a sterile probe cover . 
implanted devices were bard slimport rosenblatt 7 - f dual lumen , braun celsite 6.5 - f single lumen , baxter healthport focus 8 - f single lumen and healthport focus dc 10.5 - f dual lumen , with introducer respective introducer sets . 
we evaluated success and complication rate , defining complications as periprocedural if occurring during the first 24 h of the procedure , early if occurring between 24 h and the next 30 days and late if occurring after 30 days . 
we also evaluated procedure duration and compared results with those published in literature . i dispositivi che abbiamo utilizzato sono : bard slim port rosenblatt a doppia camera da 7 fr , braun celsite monocamera da 6 , 5 fr , baxter healt port focus monocamera da 8 fr e healt port focus dc a doppia camera da 10 , 5 fr con i loro rispettivi set introduttori . tutti i pazienti sono stati sottoposti ad rx del torace di controllo a distanza di qualche ora dal termine della procedura salvo diversa indicazione clinica per la valutazione di eventuali falde di pnx . 
abbiamo valutato la riuscita , il tasso di complicanze definendole come peri - procedurali se insorte nelle prime 24 ore dal termine della procedura , precoci se insorte tra le 24 ore e i 30 giorni successivi e tardive se insorte dopo i 30 giorni , comparando poi i risultati ottenuti nel nostro studio con quelli pubblicati in letteratura . 
using the existing pocket , a new dual - lumen pc was placed through the right subclavian vein one case of breast cancer , the tumour mass had incorporated the device completely , so it was necessary to place a second one with the right subclavian access . giorno fino ad un massimo di 470 giorni con una media di 168 giorni / paziente . 
in un caso di neoplasia della mammella la massa neoplastica ha inglobato completamente il dispositivo , per cui si reso necessario posizionarne un secondo con accesso trans - succlavio sinistro . discussion in recent years , we have witnessed a considerable increase in the number of pc placements due to the continually grownegli ultimi anni i posizionamenti di pc sono notevolmendiscussione radiol med ( 2013 ) 118 : 608615 table 1 type of complications complication pneumothorax intracatheter thrombosis port - a - cath infection disconnection total tabella 1 natura delle complicanze complicanza pneumotorace trombosi intracatetere infezione port - a - cath deconnessione totale n ( % ) 1 ( 0.14 ) 1 ( 0.14 ) 2 ( 0.28 ) 2 ( 0.28 ) 7 ( 0.84 ) n ( % ) 1 ( 0 , 14 ) 1 ( 0 , 14 ) 2 ( 0 , 28 ) 2 ( 0 , 28 ) 7 ( 0 , 84 ) ing number of applications . 
some drugs used in chemotherapy might prove harmful to the endothelium of peripheral veins in the long term [ 5 ] , without considering further possibilities of extravasation and toxicity in peripheral tissues . 
described the placement of these devices as a matter of surgical relevance , performed by a section of the cephalic vein or by direct puncture of the subclavian vein or rijv [ 2 ]  . 
described the pc implantation procedure under radiological guidance ( us and fluoroscopy ) , demonstrating safety and success of the technique , with rates comparable with those achieved with surgery [ 6 ]  . 
the most commonly used technique involves puncture of a central vein with the seldinger technique : first the vein is punctured with a large - calibre needle , through which a wire is passed ( j - shaped guidewire )  . 
la prescrizione dellimpianto prevalentemente di tipo oncologico [ 1 ] , viene effettuata al fine di garantire un accesso venoso centrale sempre disponibile per chemioterapie infusionali : alcuni farmaci utilizzati infatti risulterebbero a lungo termine lesivi per lendotelio delle vene periferiche [ 5 ] , senza contare lulteriore possibilit di stravaso e di tossicit a livello dei tessuti periferici . 
fino a qualche anno fa un limite a questo utilizzo era rappresentato dallimpossibilit di effettuare iniezioni ad alto flusso , ma oggi grazie ai set di infusione compatibili con alcuni dispositivi , possibile iniettare il mezzo di contrasto con flussi fino a 5 ml / s . 
 [ 2 ] descrissero il posizionamento di questi dispositivi come procedura di pertinenza chirurgica , effettuata mediante sezione della vena cefalica o mediante puntura diretta delle vene succlavia o giugulare destra . 
 [ 6 ] hanno descritto la procedura di impianto di pc , eseguita mediante guida radiologica ( ecografica e fluoroscopica ) dimostrandone la sicurezza e la riuscita , con tassi comparabili a quelli chirurgici [ 6 ]  . 
la tecnica attualmente pi diffusa prevede la puntura di una vena centrale con tecnica di seldinger : dapprima si punge la vena con un ago di grosso calibro e quindi , su questo , si fa passare un filo metallico ( guida a j , per la sua forma )  . 
 se si incannula una vena distante dal posizionamento del pc ( ad esempio , la giugulare ) , il catetere deve essere tunnelizzato , ovvero lo si deve fare passare sotto la pelle , creando un vero e proprio tunnel sottocutaneo [ 4 ]  . 
lutilizzo di dispositivi tunnelizzati , ha il vantaggio di ridurre il rischio di infezioni [ 7 ]  . tuttavia in letteratura esistono diverse varianti relative alla tecnica di esecuzione dellimpianto : hearns et al . 
 [ 8 ] , ad esempio , in un recente lavoro hanno proposto una procedura che prevedeva lutilizzo di una singola incisione , eliminando la necessit di un secondo accesso e le complicanze ad esso associate . 
attualmente tuttavia non vi accordo unanime su quale sia il miglior accesso per limpianto di pc : comunemente viene scelta la vena succlavia destra , co614 radiol med ( 2013 ) 118 : 608615 real subcutaneous tunnel [ 4 ]  . 
although the right subclavian vein is commonly chosen , the decision often depends on the experience of the individual operator , as does the shortand long - term complication rate [ 913 ]  . 
in addition , to avoid the risk of embolism , we clamp the proximal end of the pc with a tourniquet while it is being advanced through the peel - away sheath and then clamp the introducer sheath with our fingers while the catheter is being advanced . several other approaches have also been reported : biffi et al . 
in 2008 [ 14 ] compared access via the jugular , subclavian and cephalic veins , demonstrating that the lowest rate of procedural complications was achieved with the us - guided subclavian vein approach . 
other authors ( plumhans et al . ) show the lowest rate of procedural complications to be achieved with jugular vein access [ 4 ] ; yet again , some ( hong et al . , in 2009 ) compared access via the high and low jugulars [ 15 ]  . 
 among those reported in literature with highly variable rates in the different studies are haemorrhage of varying severity caused by laceration of the vessel to be canalised or of a nearby artery ( 03% ) , injury to neural structures or lymphatic duct ( if the vessels of the left hemithorax are involved ) ( 00.1% ) , infection ( 0.84% ) , venous thrombosis ( 012.8% ) , cardiac abnormalities such as an arrhythmia due to the guidewire or catheter being pushed up to the heart , malpositioning of the catheter or its migration ( 01% ) , haemothorax ( 01.3% ) and pneumothorax ( 01.5% ) [ 6 , 14 , 16 ]  . we evaluated complication rates , defining them as periprocedural if occurring in the first 24 h after the procedure , early if occurring 24 h to 30 days after the procedure and late if occurring later than 30 days . 
inoltre per evitare il rischio di embolia clampiamo lestremit prossimale del pc con la pinza emostatica durante lavanzamento attraverso il peel - away sheath e poi pinziamo con le dita lintroduttore mentre si avanza con il catetere . in letteratura esistono diversi studi che utilizzano approcci diversi : biffi et al . 
nel 2008 [ 14 ] hanno comparato laccesso per via giugulare , succlavia e cefalica , valutandone il tasso di complicanze procedurali dimostrandone il minor numero nellapproccio eco - guidato per via succlavia ; altri autori [ 4 ] hanno invece dimostrato un minor numero di complicanze nellaccesso per via giugulare ; altri ancora [ 15 ] hanno confrontato lapproccio per via giugulare alta con quello per via giugulare bassa . le complicanze procedurali , indipendentemente dal punto di accesso utilizzato , possono essere immediate o comparire tardivamente . 
tra quelle segnalate in letteratura , con percentuali molto variabili nei diversi studi , vi sono : emorragie pi o meno importanti per lacerazione del vaso da incannulare o dellarteria vicina ( 0%3% ) , le lesioni di strutture nervose o del dotto linfatico ( se si opera sui vasi dellemitorace sinistro ) ( 0%0 , 1% ) , infezione ( 0 , 8%4% ) , trombosi della vena ( 0%12 , 8% ) , alterazioni cardiache come una aritmia dovuta alla guida metallica o al catetere che vengono spinti fino al cuore , malposizionamento del catetere o sua migrazione in altra sede ( 0%1% ) , emotorace ( 0%1 , 3% ) e pneumotorace ( 0%1 , 5% ) [ 6 , 14 , 15 ]  . 
 nella nostra casistica abbiamo valutato il tasso di complicanze definendole come peri - procedurali se insorte nelle prime 24 ore dal termine della procedura , precoci se insorte tra le 24 ore e i 30 giorni successivi e tardive se insorte dopo i 30 giorni . 
 conclusioni conclusions results of our study enable us to state that pc placement through the rijv under us guidance appears to be a valid procedure in terms of technical success and one that is associated with fewer complications compared with other placement techniques , particularly compared with subclavian access . 
furthermore , despite being more uncomfortable for the patient , because tunnelling prolongs the procedure , access via the rijv allows for safer management of any possible bleeding as makes it is easier to manually compress the injured vessel . i risultati ottenuti dalla nostra esperienza ci permettono di affermare che il posizionamento di pc venosi con accesso per vgid sotto guida us risulta essere una procedura valida in termini di successo tecnico e gravata da un ridottissimo numero di complicanze , rispetto alle altre tecniche di posizionamento ed in particolare rispetto allaccesso per via succlavia . 
infatti le complicanze che abbiamo osservato sono paragonabili sia in termini di incidenza che di tipologia a quelle riscontrate da altri autori : anche nel nostro studio abbiamo infatti osservato che linfezione del dispositivo risulta essere la pi frequente . 
inoltre laccesso per vgid , seppur possa esser pi disagevole per il paziente a causa dei tempi procedurali pi lunghi , legati alla tunnelizzazione , tuttavia permette una gestione pi sicura nei casi di eventuale emorragia grazie ad una pi facile compressione manuale del vaso lesionato . 
during a mean follow - up period of 29.6 months , no cases of stent - graft migration were observed ; the overall incidence of endoleaks was 27% ( 60 / 222 ) and comprised four type i ( 1.8% ) and one type iii ( 0.45% ) , all treated by stent - graft extension , and 55 type 2 ( 24.8% ) , eight of which ( 14.5% ) were treated by percutaneous injection of thrombin 10 / 222 cases ( 4.5% ) , thrombotic occlusion of the iliac extension was detected , which was successfully treated by transcatheter intra - arterial thrombolysis . 
a un follow - up medio di 29 , 6 mesi , lincidenza complessiva di endoleak stata del 27% ( 60 / 222 ) : quattro endoleak di tipo i ( 1 , 8% ) e uno di tipo iii ( 0 , 45% ) , trattati mediante stent - graft , e 55 endoleak di tipo ii ( 24 , 8% ) , di cui 8 trattati mediante iniezione translombare di trombina . 
il nostro studio , in linea con i dati di letteratura , documenta la sicurezza e lefficacia a lungo termine dellevar . parole chiave evar aorta endoleak aneurisma introduction introduzione abdominal aortic aneurysm ( aaa ) is defined as the presence of an aortic dilatation > 3cm [ 1 ]  . 
the natural course of aaa is one of progressive enlargement leading to rupture , with a growth rate of 0.20.3 cm / year for aneurysms with a diameter of 3055 mm and a faster growth for larger aneurysms [ 2 , 3 ]  . 
aneurysm size is an independent risk factor for rupture : aaa < 5 cm have a 1% risk of rupture at 12 months , which increases to approximately 30% if the aaa is > 7 cm [ 4 ]  . 
in addition , it often represents the first clinical manifestation of the disease : indeed , in most cases , the aaa is incidentally discovered during imaging investigations performed for other reasons [ 6 ]  . 
in order to minimise the risk of aaa rupture , treatment is indicated when the size of the aneurysm reaches a threshold level above which the risk becomes significant : this cutoff level has been set at a diameter of 5.5 cm because the risk of rupture for aaa < 5.5 cm is lower than the mortality rate associated with an elective procedure in the majority of centres [ 7 ]  . aaa treatment is indicated in the case of : ( 1 ) maximum axial diameter > 5.5 cm ; ( 2 ) rapid growth ( > 1 cm / year ) ; ( 3 ) rupture ; ( 4 ) presence of associated symptoms ( pain ) [ 8 ]  . 
for many years , the standard treatment was open surgery , which was associated with a perioperative ( < 30 days ) mortality rate of 815% [ 9 ] and a rate of periprocedural complications of approximately 10% [ 10 ]  . 
since parodis first report in 1991 [ 11 ] , endovascular repair of aaa ( evar ) has increasingly gained ground as a safe and effective option enabling a three - fold reduction in perioperative mortality ( 12% ) rate compared with open surgery [ 1215 ]  . 
the main advantages over open surgical repair include shorter procedure time , possibility of local anaesthesia , less surgical trauma , less postoperative pain , shorter stay in hospital and intensive care unit , less blood loss and lower postoperative mortality and morbidity [ 16 ]  . the aim of this study was to assess the effectiveness of evar by means of a retrospective review of our 6 - year experience at a single centre . si definisce aneurisma dellaorta addominale ( aaa ) la presenza di dilatazione del vaso > 3cm [ 1 ]  . 
la storia naturale degli aaa il loro progressivo accrescimento sino alla rottura , con un tasso di crescita di 0 , 20 , 3 cm / anno per aneurismi di diametro compreso tra 30 e 55 mm mentre aneurismi di calibro maggiore sono associati a una pi rapida evoluzione [ 2 , 3 ]  . 
 le dimensioni dellaneurisma sono un fattore di rischio indipendente di rottura : aaa di calibro inferiore a 5 cm presentano un rischio di rottura a 12 mesi dell1% , che aumenta allaumentare delle dimensioni della sacca nativa , fino a un rischio del 30% circa per aaa > 7 cm [ 4 ]  . 
la rottura di un aaa un evento gravissimo , associato a un tasso complessivo di mortalit dell8090% [ 5 ] e rappresenta spesso la prima manifestazione clinica della patologia stessa : nella maggior parte dei casi la diagnosi un riscontro casuale in corso di esami strumentali eseguiti per altri motivi [ 6 ]  . 
al fine di ridurre il pi possibile il rischio di rottura dellaaa , il trattamento indicato quando le dimensioni raggiungono un livello soglia al di sopra del quale tale rischio significativo : stato pertanto posto come cut - off un diametro di 5 , 5 cm , in quanto il rischio di rottura di aaa < 5 , 5 cm inferiore alla mortalit dellintervento elettivo nella maggior parte dei centri [ 7 ]  . si pone indicazione al trattamento degli aaa in caso di : ( 1 ) calibro assiale massimo > 5 , 5 cm ; ( 2 ) rapido accrescimento dellaneurisma ( > 1 cm / anno ) ; ( 3 ) rottura dellaneurisma ; ( 4 ) presenza di sintomatologia associata ( dolore ) [ 8 ]  . 
il trattamento standard stato per anni rappresentato dallintervento chirurgico open , associato a un tasso di mortalit perioperatoria ( < 30 giorni ) compreso tra l8 e il 15% [ 9 ] e a un tasso di complicanze periprocedurali del 10% circa [ 10 ]  . 
nel 1991 [ 11 ] , il trattamento endovascolare degli aaa ( evar ) si sempre pi affermato come opzione sicura ed efficace , associata a una riduzione della mortalit perioperatoria di circa un terzo ( 12% ) rispetto allintervento chirurgico open [ 1215 ]  . 
i principali vantaggi rispetto alla riparazione chirurgica a cielo aperto comprendono : riduzione della durata dellintervento ; possibilit dimpiego dellanestesia 618 radiol med ( 2013 ) 118 : 616632 table 1 characteristics of patients and abdominal aortic aneurysms ( aaa ) treated characteristics n ( % ) treated patients sex ( m / f ) mean age ( years ) coronary artery disease smoking chronic obstructive pulmonary disease arterial hypertension diabetes dislipidemia 213 / 9 ( 96 / 4 ) 76 ( 5497 ) 84 ( 38 ) 145 ( 65.3 ) 75 ( 33.8 ) 164 ( 73.8 ) 68 ( 30.3 ) 93 ( 42 ) treated aneurysms number mean diameter ( mm ) elective procedure urgent procedure ruptured aaa symptomatic aaa 59 ( 40100 ) 168 ( 75.7 ) 54 ( 24.3 ) 34 ( 63 ) 20 ( 37 ) tabella 1 caratteristica dei pazienti e degli aneurismi addominali aortici ( aaa ) trattati caratteristiche n ( % ) pazienti trattati sesso ( m / f ) et media patologia coronaria fumo di sigaretta bpco ipertensione arteriosa diabete dislipidemia aneurismi trattati numero diametro medio ( mm ) elezione urgenza aaa rotto aaa sintomatico 213 / 9 ( 96 / 4 ) 76 ( 9754 ) 84 ( 38 ) 145 ( 65 , 3 ) 75 ( 33 , 8 ) 164 ( 73 , 8 ) 68 ( 30 , 3 ) 93 ( 42 ) 59 ( 40100 ) 168 ( 75 , 7 ) 54 ( 24 , 3 ) 34 ( 63 ) 20 ( 37 ) bpco , broncopneumopatia cronica ostruttiva materials and methods between april 2005 and august 2011 , 222 patients ( 213 men , nine women ; mean age , 76 years ; range , 5497 ) with aaa underwent evar with placement of a stent - grathe aneurysms had a mean diameter of 59 mm and length of 60 mtable 1 summarises the characteristics of patients and aneurysms . 
 consistent with the literature , the following inclusion criteria were adopted : presence of an infrarenal abdominal aneurysm with diameter > 5.5 cm , aortic neck > 1.5 cm in length , < 3.2 cm in calibre and with < 60 angle between the locale , minori traumi chirurgici , minor dolore postoperatorio , riduzione della degenza ospedaliera e in unit di terapia intensiva , riduzione della perdita ematica e quindi riduzione della mortalit e della morbilit postoperatoria [ 16 ]  . obiettivo del nostro studio valutare lefficacia del trattamento endovascolare degli aneurismi dellaorta addominale , analizzando la nostra esperienza di 6 anni . materiali e metodi da aprile 2005 ad agosto 2011 , 222 pazienti ( 213 maschi , 9 femmine ) di et media di 76 anni ( range : 5497 ) affetti da aneurisma dellaorta addominale sono stati sottoposti a trattamento endovascolare mediante posizionamento di endoprotesi . 
per la natura retrospettiva dello studio , non stato necessario richiedere il parere del comitato etico del nostro istituto . i criteri di inclusione , in accordo con i dati di letteratura , erano la presenza di aneurisma addominale sottorenale di diametro > 5 , 5 cm , con un colletto aortico > 1 , 5 cm di lunghezza , < 3 , 2 cm di calibro e con angolo compreso tra aorta sovra renale e juxtarenale < 60 e alto rischio per procedure di chirurgia tradizionale in rapporto a comorbidit importanti quali insufficienza respiratoria , insufficienza cardiaca , addome ostile per precedenti interventi chirurgici , o la presenza di sintomatologia / rottura [ 17 ]  . 
in 220 / 222 pazienti trattati stato effettuato preliminarmente uno studio angio - tc , al fine di confermare la diagnosi , valutare le dimensioni ( calibro ed estensione cranio - caudale ) dellaneurisma , il colletto prossimale e distale , il coinvolgimento delle arterie iliache e femorali . 
il protocollo di acquisizione ha previsto lo studio senza mezzo di contrasto ( mdc ) con spessori di 5 mm e lo studio con mdc a strato sottile ( 0 , 625 mm )  . 
i parametri di scansione sono stati : kv 100120 , ma 250500 mas , tempo di rotazione 0 , 5 s , pitch 0 , 0984 , scansione cranio - caudale con field of view ( fov ) ampio , da sopra il diaframma sino alle arterie femorali . 
il mdc iodato non ionico ( iomeron 400 mg / ml ) stato somministrato per via endovenosa a volume di 100 radiol med ( 2013 ) 118 : 616632 fig . 
1a - d endovascular treatment of ruptured abdominal aortic aneurys emergency contrast - enhanced computed tomography ( ct ) scan shows the presence of a ruptured abdominal aortic aneurysm with retroperitoneal leakage of contrast medium ( a ) , as confirmed by intraoperative angiography ( b ) , treated by endovascular repair ( evar ) ( c )  . 
langio - tc eseguita in urgenza documenta la presenza di aneurisma dellaorta addominale con spandimento retroperitoneale di mdc ( a ) , come confermato allaortografia intraoperatoria ( b ) , trattata mediante endoprotesi aortobisiliaca ( c )  . 
il controllo angio - tc a 1 mese conferma lefficacia del trattamento , con regolare perviet dellendoprotesi , in assenza di endoleak evidenti ( d )  . suprarenal and juxtarenal aorta and at high risk for open surgery because of major comorbidities , such as respiratory failure , heart failure , hostile abdomen due to previous surgery or presence of symptoms / rupture [ 17 ]  . 
la lunghezza e il diametro del colletto del vaso nativo sono state calcolate sulle immagini assiali , perpendicolari allasse di ricostruzione , con limiti avventizia - avventizia [ 19 ]  . 
abdominal ultrasound imaging showed a 7.0 - cm infrarenal saccular aortic aneuryscontrast - enhanced computed tomography ( ct ) imaging of the aneurysm showed compression of the inferior vena cava with an aortocaval fistula ( a , b )  . 
to prevent pulmonary embolism caused by the presence of sac thrombosis near the vena cava lumen , a temporary vena cava filter was deployed before the procedure and a bifurcated stent - graft placed ( c )  . 
lecografia addominale mostrava aneurisma dellaorta addominale di 7 cm ; langio - tc preliminare documentava compressione della vena cava con presenza di fistola aorto - cavale ( a , b )  . 
il paziente stato trattato mediante posizionamento di filtro cavale , per prevenire lembolia polmonare a partenza dalla sacca aneurismatica trombotica , ed endoprotesi aorto - bisiliaca ( c )  . 
in 220 of all cases , patients underwent preliminary computed tomography ( ct ) angiography to confirm the diagnosis , evaluate size ( diameter and craniocaudal extension ) of the aneurysm , the proximal and distal neck and involvement of the iliac and femoral arteries . 
the acquisition protocol included a non - contrast - enhanced study with 5 - mm slice accordo con la letteratura [ 17 ] , pari al 1020% rispetto alle dimensioni del vaso nativo per assicurare un buon sealing ; la lunghezza stata calcolata partendo dallarteria renale pi bassa fino al previsto punto di atterraggio su vaso sano per assicurare la completa esclusione dellaneurisma [ 17 ]  . 
 in 2 / 222 pazienti giunti alla nostra osservazione con quadro di shock emodinamico , trasferiti in sala direttamente dal pronto soccorso , stata posizionata endoprotesi solo sulla base dellangiogramma preoperatorio . radiol med ( 2013 ) 118 : 616632 thickness and a thin - section ( 0.625 mm ) contrast - enhanced study . 
scan parameters were 100120 kv , 250500 mas , 0.5 s rotation time , 0.0984 pitch , and craniocaudal scan with wide field of view ( fov ) from above the diaphragm to the femoral arteries . 
a dose of 100 ml of nonionic iodinated contrast material ( iomeron 400 mg / ml ) was administered intravenously at a flow rate of 3 ml / s ; the best scan delay to ensure adequate arterial - phase images was obtained with the bolus - tracking technique ( smart - prep ) with a region of interest ( roi ) at the level of the emergence of the coeliac trunk . 
image assessment included single axial images , multiplanar reconstructions ( mpr ) , maximum intensity projection ( mip ) and volume rendering technique ( vrt ) ; all measurements were obtained with vessel analysis software . 
length and diameter of the native vessel neck was calculated on axial images perpendicular to the reconstruction axis , with measurements taken from adventitia to adventitia [ 19 ]  . 
in agreement with the literature [ 17 ] , stentgrafts were always oversized with respect to the diameter of the proximal and distal neck , in particular , by 1020% relative to the native vessel , to ensure optimal sealing . 
the length was calculated from the lowest renal artery up to the planned landing site on a healthy portion of vessel to ensure complete exclusion of the aneurysm [ 17 ]  . 
in two patients who were transferred directly from the emergency department owing to haemodynamic shock , the stent - graft was deployed on the basis of the preoperative angiogram alone . all procedures performed until december 2009 ( 97 patients ) were carried out in an angiography suite using an integris v5000 system ( philips medical system , best , the netherlands ) ; subsequently , after the operating theatre had been equipped with a shielded room for radiological surgical procedures , all evar procedures ( 125 ) were carried out there using a bv300 portable angiography system ( philips medical system )  . 
our hospitals decision was based on recent guidelines of the main endovascular surgery societies [ 8 ] , which while stressing their preference for a fixed angiography system require that these procedures be undertaken in the operating theatre so that possible complications necessitating an open approach can be dealt with ( rupture / dissection of the artery at the access site , of the iliac axis , of the aorta , technical failure during stent - graft deployment with surgical conversion )  . 
in gli interventi sono stati eseguiti fino a dicembre 2009 ( 97 / 222 pazienti ) in sala angiografica mediante limpiego di angiografo integris v5000 ( philips medical system , best , olanda ) ; successivamente ( 125 / 222 pazienti ) in sala operatoria dopo la realizzazione di sala schermata per procedure radiologico - chirurgiche , mediante angiografo portatile bv300 ( philips medical system , best , olanda )  . 
la scelta della nostra azienda ospedaliera stata effettuata in accordo con le recenti linee guida delle maggiori societ di chirurgia endovascolare [ 8 ] che , pur sottolineando la preferenza per la presenza di un angiografo fisso , richiedono tuttavia di effettuare tali interventi in una sala operatoria per far fronte a eventuali complicanze che richiedono un approccio open ( per esempio : rottura / dissezione dellarteria nella sede di accesso , dellasse iliaco , dellaorta , insuccesso tecnico durante il rilascio dellendograft con conversione chirurgica )  . 
tutti gli interventi sono stati eseguiti grazie alla collaborazione di un team multidisciplinare costituito da radiologi interventisti , chirurghi vascolari , anestesisti , tecnici e infermieri dedicati.durante la procedura stata somministrata eparina a bolo ( 50 ui / kg ) e antibioticoterapia . 
la tabella 2 riassume le caratteristiche procedurali . il trattamento stato eseguito in 77 casi ( 34 , 7% ) in anestesia generale , in 107 casi ( 48 , 2% ) in anestesia spinale , in 23 casi ( 10 , 3% ) in anestesia locale , in 15 casi ( 6 , 7% ) in anestesia epidurale . 
nel 48 , 6% ( 108 pazienti ) lintervento stato effettuato mediante esposizione chirurgica femorale bilaterale ; nel 30% dei casi ( 62 pazienti ) per via percutanea e nel restante 23 , 4% ( 52 pazienti ) mediante esposizione chirurgica e puntura percutanea controlaterale . 
nel nostro istituto viene adottata come prima scelta lesposizione chirurgica delle arterie femorali in quanto ritenuta opzione pi sicura in presenza di arterie femorali marcatamente calcifiche con le quali non si otterrebbe unadeguata emostasi con sistemi di chiusura percutanei . 
il sistema di chiusura percutaneo utilizzato in tutti i casi stato il perclose proglide ( abbott vascular inc , redwood city , ca , usa )  . in tutti i casi , il posizionamento di endoprotesi stato preceduto dallesecuzione di aortografia discendente con catetere centimetrato tipo pig - tail ( optimed , ettinger , germania ) , collegato a iniettore automatico ( mark v plus , medrad , warrendale , pa , usa ) che ha consentito la visualizzazione delle arterie renali , punto di ancoraggio prossimale , e della biforcazione iliaca , punto di ancoraggio distale . 
surgical exposure of the femoral arteries is the preferred approach at our centre , as we believe it to be the safest option in the presence of markedly calcified femoral arteries that would not achieve adequate haemostasis with percutaneous closure systems . 
the percutaneous closure system used in all cases was perclose proglide ( abbott vascular inc , redwood city , ca , usa )  . in all cases , stent - graft deployment was preceded by descending aortography , with a graduated pigtail catheter ( optimed , ettinger , germany ) connected to an automatic injector ( mark v plus , medrad , warrendale , pa , usa ) , which allowed visualisation of renal arteries , proximal attachment site and iliac bifurcation and distal attachment site . 
the angiogram was performed with 25 ml nonionic contrast medium ( iomeron 400 bracco imaging , milan , italy ) administered at a flow rate of 16 ml / s . with the use of large - bore introducer sheaths ( 18to 24 - f , cook , bloomington , in , usa ) and stiff guidewires ( backup , boston scientific , natick , ma , usa ) , aorto - uni - iliac and aorto - bi - iliac stents were deployed , followed by placement of overlapping iliac extensions of a sufficient length to ensure complete closure of the aneuryspostprocedure aortography was then performed to check adequate sealing of the stent - graft or the presence of an endoleak . 
whenever it was necessary , in - stent angioplasty was done using reliant ab46 ( medtronic , sunnyvale , ca , usa ) or equalizer ( boston scientific ) balloons . cate , di lunghezza tale da assicurare la completa esclusione dellaneurisma . 
si quindi proceduto a esecuzione di aortografia di controllo per evidenziare ladeguato sealing della protesi o la presenza di endoleak : qualora necessario si proceduto ad angioplastica intraprotesica con palloni reliant ab46 ( medtronic , sunnyvale , ca , usa ) o equalizer ( boston scientific , natick , ma )  . nei 222 pazienti trattati , sono state impiantate 74 protesi zenith ( cook , bloomington , in , usa ) ( 33 , 3% ) , 85 excluder ( wl gore , flagstaff , az , usa ) ( 38 , 2% ) , 1 le maitre endofit ( 0 , 4% ) , 2 talent ( medtronic , sunnyvale , ca , usa ) ( 0 , 9% ) , 1 aorfix ( lombard medical ) ( 0 , 4% ) , 35 endurant ( medtronic , sunnyvale , ca , usa ) ( 15 , 7% ) e 24 evita ( jotec , milano , italia ) ( 10 , 8% )  . 
abbiamo avuto cinque casi di endoleak di i tipo precoce , trattati intraproceduralmente mediante posizionamento di tre cuffie protesiche prossimali ( due jotec , una gore excluder ) e due estensioni iliache distali ( una jotec e una gore )  . 
riteniamo infatti , in accordo con i dati della letteratura [ 20 , 21 ] , che il bypass femoro - femorale rappresenti uno svantaggio per i rischi correlati di occlusione tardiva o infezione , preferendo pertanto come prima opzione il device biforcato , in grado di assicurare una maggior conformabilit al trattamento . 
there were five cases of early type i endoleak , which were treated intraprocedurally by placing three proximal extender cuffs ( two jotec , one gore excluder ) and two distal iliac extensions ( one jotec and one gore )  . 
 indeed , we agree with the literature [ 20 , 21 ] that femorofemoral bypass carries associated risks of late occlusion or infection and thus prefer the bifurcated device as a first option , as it ensures greater conformability . 
 [ 22 ] , we employed aortouni - iliac stent - grafts in the case of unfavourable anatomy ( chronic occlusion of an iliac axis or unfavourable bifurcation , n = 7 ) , or urgent procedures due to aneurysm rupture and haemorrhagic shock ( n = 10 ) and type iii endoleak ( n = 1 )  . follow - up included ct angiography at 1 month , contrast - enhanced ultrasound ( ceus ) with i.v. 
the ct angiography protocol involved baseline acquisitions and a contrast - enhanced study with thin - slice arterial phase with 60 - s scan delay after contrast injection and fov centred on the stentgra ct parameters used at follow - up were the same as those used for preliminary imaging . we carried out a single - centre retrospective review of the efficacy of aaa treatment by stent - graft deployment , of the incidence of perioperative complications and of procedurerelated mortality rate ( < 30 days ) and analysed long - term follow - up . results in our experience , we had 98.6% technical success , with the stent - graft being deployed correctly and without intraprocedural complications in 219 cases . 
in three cases ( 1.4% ) , surgical conversion became necessary : in one due to caudal migration of the main body of the stent - graft , in one case because of device fracture at the time of deployment and in the remaining case due to inability to retrieve the device from the contralateral iliac extension due to the presence of a previously placed self - expanding stent in the external iliac artery . 
this was a patient with a ruptured aneurysm and haemodynamic instability who arrived directly to the operating theatre without undergoing a preliminary ct angiogram ; the patients large build caused degradation of angiographic image quality ( table 3 )  . grafia con mdc ( sonovue , bracco imaging , milano italia ; 2 , 5 ml ev a bolo , seguito da bolo di 10 ml di soluzione fisiologica ) ( contrast - enhanced ultrasound , ceus ) a 6 mesi quindi controllo annuale alternativamente con angio - tc e ceus . 
il protocollo angio - tc prevede acquisizioni basali e studio con mdc in fase arteriosa a strato sottile e acquisizione tardiva , a 60 secondi dallinfusione del contrasto , con fov mirato sulla protesi . 
i parametri tc impiegati sono analoghi a quelli dello studio pre - trattamento precedentemente esposti . stata effettuata una valutazione retrospettiva monocentrica dellefficacia del trattamento mediante endoprotesi negli aaa , dellincidenza delle complicanze peri - operatorie , della mortalit correlata allintervento ( < 30 giorni ) ed stato analizzato il follow - up a lungo termine . risultati nella nostra esperienza abbiamo ottenuto successo tecnico nel 98 , 6% dei casi : in 219 casi , infatti , il posizionamento della protesi avvenuto in maniera adeguata , in assenza di complicanze intraprocedurali . 
in tre casi ( 1 , 4% ) stata necessaria la conversione chirurgica , in un caso per migrazione caudale del corpo principale della protesi , in un caso per documentata rottura al momento del rilascio della protesi stessa , e nel restante caso per impossibilit di recupero del device dallestensione iliaca controlaterale a causa della presenza di un pregresso stent autoespandibile in iliaca esterna . 
si trattava di un paziente con aneurisma rotto , in condizioni di instabilit emodinamica , giunto in sala operatoria senza angio - tc preliminare e di costituzione robusta , il che degradava la qualit delle immagini angiografiche ( tabella 3 )  . la mortalit post - operatoria ( < 30 gg ) stata del 7 , 6% ( 17 / 222 pazienti )  . 
in 13 casi ( 76 , 5% ) si trattava di pazienti sottoposti a evar in regime durgenza : la mortalit postoperatoria per interventi effettuati in regime durgenza risultata del 24% ( 13 / 54 pazienti ) mentre per gli interventi effettuati in regime delezione risultata del 2 , 3% ( 4 / 168 pazienti )  . 
of these , 13 ( 76.5% ) were patients who underwent evar as an urgent procedure : postoperative mortality for urgent procedures was 24% ( 13 / 54 patients ) and 2.3% ( 4 / 168 patients ) for elective procedures . 
this combined approach , performed under ct guidance , was done in accordance with data reported in the literature [ 2325 ] , which suggest the use of coils and thrombin to ensure longer - lasting thrombosis of the reperfused aneurysm sac . 
tale approccio terapeutico combinato , effettuato sotto guida tc , stato adottato in linea con i dati della letteratura [ 2325 ] , che suggeriscono luso delle spirali associato alla trombina per ottenere una pi duratura trombosi della sacca riperfusa . 
i restanti 47 casi di endoleak di ii tipo non erano associati a incremento dimensionale della sacca aneurismatica nativa e pertanto sono stati gestiti in maniera conservativa mediante follow - up semestrale con metodica ceus . si osservata unincidenza di endoleak di i tipo dell1 , 8% ( 4 / 222 casi ) , due casi di endoleak di tipo ia riscontrati rispettivamente a 6 e 12 mesi di follow - up , trattati mediante posizionamento di cuffia protesica prossimale e due casi di endoleak di tipo ib , riscontrati rispettivamente a 6 e 24 mesi di follow - up , trattati mediante estensioni iliache . 
sono stati impiegati materiali dello stesso produttore dellendoprotesi impiantata . in 10 casi ( 4 , 5% ) si riscontrata unocclusione trombotica dellestensione iliaca , in sette casi al follow - up a 1 mese e in tre casi al follow - up a 6 mesi . 
in sei casi tale complicanza si verificata con protesi evita jotec ( 25% del totale impiantate ) , in 2 casi con protesi zenith cook ( 2 , 7% del totale impiantate ) , in 1 caso con protesi excluder gore ( 1 , 1% del totale impiantate ) e in 1 caso con protesi endurant medtronic ( 2 , 8% del totale impiantate )  . 
patient previously treated by endovascular abdominal aorta repair ( evar ) presented to the emergency department with acute abdominal pacontrast - enhanced computed tomography ( ct ) scan shows active bleeding from the stent - graft ( a , b )  . 
alla valutazione angiografica si documenta la presenza di endoleak di iii tipo ( c , d ) , trattato mediante posizionamento di protesi aorto - monoiliaca ( e )  . radiol med ( 2013 ) 118 : 616632 626 fig . 
la ceus di controllo 2 anni dopo evar ( a ) documenta voluminoso endoleak di ii tipo ad alto flusso , associato a incremento volumetrico della sacca nativa , trattato mediante iniezione trans - lombare di trombina bovina ( b ) , con completa risoluzione dellendoleak ( c )  . cuff ; two type ib , seen at 6 and 24 months , were treated by iliac extensions . 
in six cases , this complication occurred with an evita jotec stent - graft ( 25% of the total ) , in two cases with a zenith cook ( 2.7% of the total ) , in one case with an excluder gore ( 1.1% of the total ) and in one case with an endurant medtronic ( 2.8% of the total )  . 
in one case ( 0.45% ) , an infection developed that required stent - graft explantation . it is important to consider the incidence of complications in patients treated in urgent settings : in 12 cases ( 22.2% of urgent cases ) , we observed the development of type ii endoleaks , in two cases ( 3.7% ) type i and in one case ( 1.8% ) stent - graft infection . overall reintervention rate was 10.8% ( 24 / 222 patients ) : ten cases of fibrinolysis for thrombosis of the iliac branch , two cases of placement of stent extensions for type ib endoleaks , three cases of placement of stent cuffs for type ia trarteriosa . 
in un caso ( 0 , 45% ) si verificata infezione della protesi che ha richiesto lespianto della stessa . importante considerare lincidenza di complicanze nei pazienti trattati in regime durgenza : in 12 casi ( 22 , 2% delle urgenze ) si osservata la comparsa di endoleak di tipo ii , in 2 ( 3 , 7% ) di endoleak di tipo i , in 1 ( 1 , 8% ) infezione della protesi . il tasso complessivo di reintervento stato del 10 , 8% ( 24 / 222 pazienti ) : 10 trattamenti di fibrinolisi per trombosi della branca iliaca , 2 posizionamenti di estensioni protesiche per endoleak di tipo ib , 3 posizionamenti di cuffie protesiche per endoleak di tipo ia e iii , 8 iniezioni trans - lombari di trombina intrasacca per leak di ii tipo , 1 espianto di protesi per infezione della stessa . 
la degenza ospedaliera media stata di 4 giorni e il tempo di ricovero medio in unit di terapia intensiva stato di 2 giorni . discussione dalla sua introduzione nella pratica clinica nei primi anni 90 [ 11 ] , il trattamento endovascolare degli aneurismi radiol med ( 2013 ) 118 : 616632 and type iii endoleaks , eight translumbar injections of intrasac thrombin for type ii leaks , one stent - graft explantation due to infection . 
mean hospital stay was 4 days , and mean stay in the intensive care unit was 2 days . discussion since its introduction into clinical practice in the early 1990s [ 11 ] , endovascular repair of aaa has increasingly gained ground as a safe and effective surgical method , ensuring lower postoperative mortality and morbidity rates compared with open surgery [ 8 ]  . 
this result is among the best levels of technical success reported in the literature : in 1.4% of our cases ( 3 / 222 patients ) , primary surgical conversion was necessary . a strongly debated subject is what is the advantage offered by evar over open surgery in terms of early mortality rates ( < 30 days )  . 
the dutch randomised endovascular aneurysm management ( dream ) trial [ 28 ] shows a rate of postoperative death of 2.6% in the evar group compared with 5.7% in the open surgery group . 
 even the overall mortality rate in our study 8.9% of patients who underwent elective procedures ( 15 of 168 ) is similar to that reported in published studies [ 1730 ]  . 
 [ 28 ] , in 351 pazienti trattati mediante evar , hanno documentato unincidenza di complicanze correlate al dispositivo o alla procedura , come occlusione trombotica di una branca protesica , mancata apertura del free - flow , mancato recupero del sistema di rilascio del corpo principale , scivolamento caudale del corpo principale , migrazione di una branca protesica e rottura intraprocedurale dellendoprotesi compresa tra il 9 e il 16% . 
 tale risultato si attesta sui migliori livelli di successo tecnico riportati in letteratura : nell1 , 4% dei casi ( 3 pazienti su 222 ) stata necessaria la conversione chirurgica primaria . argomento di grande dibattito il vantaggio fornito dallevar rispetto allor in termini di mortalit precoce ( < 30 giorni )  . 
il dream trial [ 28 ] mostra una percentuale di decessi postoperatori del 2 , 6% nel gruppo evar rispetto al 5 , 7% del gruppo open ; negli ultimi anni la mortalit postoperatoria ulteriormente diminuita , come confermato da lederle et al . 
anche la mortalit complessiva da noi rilevata , 8 , 9% dei pazienti operati in elezione ( 15 su 168 ) , risulta sovrapponibile alle stime degli studi pubblicati [ 1730 ]  . 
per quanto concerne gli interventi eseguiti in regime durgenza , in letteratura riportato un tasso di mortalit post - procedurale compreso tra il 18 e il 53% [ 22 , 3133 ]  . 
 [ 31 ] in uno studio di confronto tra 1037 pazienti trattati con evar e 763 con or , riporta una mortalit < 30 giorni dopo evar demergenza del 21 , 2% , ridotta rispetto a quella dellintervento chirurgico ( 36 , 3% )  . 
hanno osservato una mortalit postoperatoria del 28 , 5% , riscontrando come pi importante fattore prognostico negativo la presenza di shock allingresso , a cui stata posizionata una endoprotesi aorto - monoiliaca [ 22 ]  . 
recorded a postoperative mortality rate of 28.5% and reported the most important negative prognostic factor was haemodynamic shock on admission , with lit postoperatoria sia in elezione che in urgenza , con dati sovrapponibili a quelli presenti in letteratura . il protocollo di follow - up da noi impiegato , rappresentato alternativamente da angio - tc e ceus , quello indicato radiol med ( 2013 ) 118 : 616632 placement of an aorto - uni - iliac stent - graft [ 22 ]  . 
our study therefore demonstrates the effectiveness of evar in terms of postoperative mortality rates in both elective and urgent settings , with data very similar to those reported in the literature . 
 [ 34 ] demonstrated that sensitivity and specificity of non - contrast - enhanced us in the diagnosis of endoleaks were 77% and 94% , respectively , whereas those of ceus were 88% and 98% . 
 [ 35 ] , however , suggested using ct angiography with delayed - phase imaging and 33 - mm sections as the gold standard for measuring aaa diameter , visualising collateral reperfusion and endoleak diagnosis on account of its higher sensitivity . 
on the basis of the literature [ 36 , 37 ] and our personal experience , we recommend performing the follow - up by alternating triphasic ct angiography and ceus . 
they concluded that despite having the highest absolute sensitivity and specificity , ct cannot be used alone in follow - up protocols but needs to be associated with ceus . among the complications seen at follow - up , the most common and worthy of note are endoleaks ( table 4 ) [ 39 ]  . 
in addition , their results indicate that most type ii endoleaks ( 30100% ) resolve spontaneously within 6 months , without any damage to the stent - graft and without requiring any intervention . 
 [ 41 ] in a study of 486 patients treated with evar noting the incidence of type ii endoleak was 18.5% ( 90 patients ) , of whom 7.2% ( 35 patients ) required treatment because of growth of the aneurysm sac . 
 of the 55 type ii endoleaks , 47 ( 85.5% ) were low - flow and eight ( 14.5% ) were high flow associated with enlargement of the aneurysm sac and therefore treated with translumbar thrombin injection . 
 [ 34 ] hanno dimostrato che la sensibilit e la specificit nella diagnosi di endoleak dellecografia senza mdc sono rispettivamente del 77 e 94% , mentre quelle dellecografia con contrasto ( ceus ) dell88 e 98% ; buth et al . , tuttavia [ 35 ] , suggeriscono langio - tc con fase ritardata e sezioni di 3 mm come gold - standard per la misurazione del diametro dellaaa , per levidenziazione della riperfusione collaterale e anche per la diagnosi di endoleak , in quanto dotata di maggior sensibilit . 
in base ai dati di letteratura [ 36 , 37 ] , surrogati dalla nostra esperienza , suggeriamo di eseguire il follow - up alternativamente mediante angio - tc trifasica e ceus : tale approccio consente di ridurre lesposizione a radiazioni ionizzanti e al mdc della tc con adeguata accuratezza diagnostica . 
 [ 38 ] hanno infatti recentemente dimostrato che i principali svantaggi dellangio - tc sono la nefrotossicit indotta dal mezzo di contrasto , lesposizione a radiazioni ionizzanti a potenziale effetto cancerogeno e i costi , concludendo che la tc , nonostante sia la metodica con migliori sensibilit e specificit assolute , non pu essere utilizzata isolatamente nei protocolli di follow - up ma deve essere associata alla ceus . nellambito delle complicanze riscontrate al follow - up , la pi comune e meritevole di discussione rappresentata dagli endoleak ( tabella 4 ) [ 39 ]  . 
dai loro risultati si evince , inoltre , che la maggior parte degli endoleak di tipo ii ( dal 30 al 100% ) va incontro a risoluzione spontanea nei primi 6 mesi , senza danneggiare in alcun modo la protesi e senza richiedere interventi terapeutici . 
 [ 41 ] che in 486 pazienti sottoposti a evar hanno ottenuto unincidenza di endoleak di tipo ii del 18 , 5% ( 90 pazienti ) , di cui il 7 , 2% ( 35 pazienti ) necessita di intervento terapeutico a causa dellincremento volumetrico della sacca . 
nella nostra esperienza , in linea con i dati della letteratura , abbiamo riscontrato unincidenza complessiva di endoleak del 27% ( 60 / 222 pazienti ) : in 4 casi si trattava di endoleak di tipo i ( 1 , 8% del totale ) , in 55 casi di endoleak di tipo ii ( 24 , 8% ) e in 1 caso di endoleak di tipo iii ( 0 , 45% )  . 
gli endoleak di i e iii tipo sono stati prontamente trattati mediante posizionamento di stent - graft addizionali , in accordo con i dati di letteratura [ 4244 ] ; dei 55 casi di endoleak di ii tipo , 47 ( 85 , 5% ) erano a basso flusso , mentre 8 casi ( 14 , 5% ) erano ad alto flusso , associati a incremento dimensionale della sacca aneurismatica e trattati mediante iniezione translombare di trombina . 
il nostro studio conferma che la maggior parte degli endoleak di ii tipo sono a basso flusso , non determinanti incremento volumetrico della sacca nativa e pertanto non richiedenti 630 radiol med ( 2013 ) 118 : 616632 al . 
our study indicates that the majority of type ii endoleaks are low flow and do not cause sac enlargement , thus requiring no treatment but only close follow - up . 
in such cases , we recommend surveillance with ceus at 6 - month intervals , as ceus has high sensitivity and specificity for detecting endoleaks . as observed in the evar 1 trial , stent - grafts are prone to a greater risk of thrombosis of the iliac extensions than are he endografts implanted during open surgery [ 17 ]  . 
in a review of the european collaborators on stent / graft techniques for aortic aneurysm repair ( eurostar ) registry covering a postoperative period longer than 8 years , kinking of a stent - graft limb was observed in 3.7% of cases and was significantly associated with type i and iii endoleaks , graft migration and graft thrombosis [ 45 ]  . 
in our series , we had a 4.5% incidence ( 10 / 222 patients ) of thrombotic occlusion of the iliac extension limb , in all cases successfully treated with intra - arterial fibrinolysis . 
 the risk of stent - graft infection after evar is very low , as demonstrated by the eurostar registry , with only three cases among 2 , 846 patients ( 0.1% ) after a follow - up period of 5 years [ 45 ]  . 
only one patient in our series ( 0.45% ) developed graft infection requiring explantation of the graft itself . our 6 - year experience on a large series of patients leads us to believe that evar is a safe and effective method associated with low postoperative mortality and morbidity rates . 
 after a mean follow - up of 29.6 months , we found an incidence of complications similar to that reported in the literature , which demonstrated the effectiveness of this approach when carried out at a dedicated centre . conclusions evar represents a safe and effective procedure capable of ensuring adequate exclusion of the aneurysm , with lower mortality than that of standard open surgery . 
we had a postoperative mortality rate of 2.3% for elective procedures and of 24.1% for urgent procedures , in either case lower than reported for open surgery [ 3133 ] , which demonstrates the value of this treatment in all clinical settings . technical and clinical success of evar is , in our opinion , largely dependent on adequate treatment planning and materials selection , which should be done by the interventional radiologist according to the anatomical characteristics of the individual patient . 
thus , it is crucial to perform preliminary ct angiography to estimate , on the basis of mpr reconstructions along the axis perpendicular to the vessel , craniocaudal extension of the aneurysm and diameter of the trattamento correttivo ma stretto follow - up : in tali casi , consigliamo di eseguire ceus con frequenza semestrale . 
tale metodica di imaging , infatti , gode di alta sensibilit e specificit nellidentificazione degli endoleak . come osservato nellevar 1 trial , gli stent - graft sono soggetti a un maggior rischio di trombosi delle estensioni iliache rispetto alle protesi impiantate durante la riparazione open [ 17 ]  . 
in una review di eurostar registry di un periodo postoperatorio superiore a 8 anni , locclusione di una branca dello stent - graft si osservata nel 3 , 7% dei casi , significativamente associata a endoleak di tipo i e iii , alla migrazione e alla trombosi del graft [ 45 ]  . 
nella nostra casistica abbiamo riscontrato nel 4 , 5% dei casi ( 10 / 222 pazienti ) occlusione trombotica dellestensione protesica iliaca , in tutti i casi trattata con successo mediante terapia fibrinolitica intrarteriosa . 
 il rischio dinfezione del graft dopo evar molto basso , come testimoniato da eurostar registry , con solo 3 casi su 2.846 pazienti ( 0 , 1% ) a un follow - up di 5 anni [ 45 ]  . 
levar 1 trial ha mostrato unincidenza paragonabile nella riparazione endovascolare e nella chirurgia classica ( 0 , 4 e 0 , 2% , rispettivamente ) in un periodo superiore a 4 anni di followup [ 17 ]  . 
solo uno dei pazienti da noi trattati ( 0 , 45% ) andato incontro a infezione del graft , che ha richiesto lespianto dello stesso . nella nostra esperienza di 6 anni su un ampio numero di pazienti trattati , riteniamo levar una metodica sicura ed efficace , associata a un basso tasso di mortalit e morbilit postoperatoria . 
a un follow - up medio di 29 , 6 mesi , abbiamo riscontrato unincidenza di complicanze in linea con i dati della letteratura , a documentare lefficacia di tale approccio in un centro dedicato . conclusioni levar rappresenta , nella nostra esperienza , una procedura sicura ed efficace , in grado di assicurare unadeguata esclusione dellaneurisma , con un tasso di mortalit inferiore rispetto alla chirurgia standard . 
abbiamo riscontrato un tasso di mortalit postoperatoria in elezione del 2 , 3% e in urgenza del 24 , 1% , in entrambi i casi inferiore a quella dellintervento chirurgico open riportata in letteratura [ 3133 ] , documentando la validit di tale trattamento in tutte le condizioni cliniche . il successo tecnico - clinico dellevar passa , a nostro avviso , attraverso unadeguata pianificazione del trattamento e unadeguata scelta dei materiali , che deve essere fatta dal radiologo interventista in base alle caratteristiche anatomiche del singolo paziente : fondamentale risulta , pertanto , lesecuzione di un corretto studio angio - tc preliminare che consente , mediante ricostruzioni elettroniche mpr sullasse perpendicolare del vaso , di stimare correttamente le dimensioni dellaneurisma in termini di estensione cranio - caudale radiol med ( 2013 ) 118 : 616632 proximal and distal neck . 
in case of type ii endoleak with enlargement of the aneurysm sac , translumbar injection of thrombin and coil placement is an adequate therapeutic option capable of ensuring thrombosis of the reperfused area . finally , we believe the operators experience to be the main determinant of procedural success , so that evar should be offered in centres of excellence in which a large number of procedures are performed and where both elective and urgent cases can be managed . 
it is fundamental that there should be a dedicated multidisciplinary team composed of interventional radiologists , vascular surgeons , anaesthetists , radiology technicians and nurses on call 24 h / day 7 days / week and capable of managing with high levels of competence , safety and effectiveness both elective and urgent situations . 
in particular , the concomitant presence in the operating theatre of a vascular surgeon and an interventional radiologist ensures prompt management of potential intraprocedural complications that , although uncommon in our experience , may nonetheless prove to be extremely serious . e di diametro del colletto prossimale e distale . 
la stretta osservanza di tale approccio metodologico ci ha permesso di osservare una bassa incidenza di endoleak di i tipo ( 1 , 8% )  . nel follow - up riteniamo utile eseguire alternativamente studio angio - tc trifasico e ceus a 1 , 6 , 12 mesi e poi annualmente , riservando uno stretto monitoraggio mediante ceus semestrale ai pazienti con endoleak di ii tipo . 
in caso di endoleak di ii tipo con aumento dimensionale della sacca nativa , liniezione trans - lombare di trombina e spirali rappresenta unadeguata opzione terapeutica in grado di assicurare la trombosi della zona riperfusa . riteniamo , infine , che il principale fattore determinante il buon esito dellintervento lesperienza delloperatore , per cui levar deve essere eseguito in centri deccellenza che eseguano un ampio numero di interventi e sappiano gestire tanto lelezione quanto lurgenza . 
fondamentale pertanto la presenza di un team dedicato composto da varie figure professionali quali radiologi interventisti , chirurghi vascolari , anestesisti , tecnici di radiologia e infermieri professionali , reperibili 24h al giorno per 7 giorni alla settimana , in grado di gestire con estrema competenza , sicurezza ed efficacia tanto le situazioni in elezione che in urgenza . 
at present , chest - computed tomography imaging is considered the most effective method for the detection of lung abnormalities in early - stage disease and quantitative assessment of severity and progression of covid - 19 pneumonia . 
although chest x - ray ( cxr ) is considered not sensitive for the detection of pulmonary involvement in the early stage of the disease , we believe that , in the current emergency setting , cxr can be a useful diagnostic tool for monitoring the rapid progression of lung abnormalities in infected patients , particularly in intensive care units . 
in this short communication , we present our experimental cxr scoring system that we are applying to hospitalized patients with covid - 19 pneumonia to quantify and monitor the severity and progression of this new infectious disease . 
 we also present the results of our preliminary validation study on a sample of 100 hospitalized patients with sars - cov - 2 infection for whom the final outcome ( recovery or death ) was available . keywords sars - cov - 2 covid - 19 chest x - ray computed tomography scoring system introduction severe acute respiratory syndrome coronavirus 2 ( sarscov - 2 ) is a new virus recently isolated from humans . 
 sars - cov - 2 was discovered to be the pathogen responsible for a cluster of pneumonia cases associated with severe respiratory disease that occurred in december 2019 in wuhan , china [ 1 ]  . 
this novel pulmonary infection , formally called coronavirus disease 2019 ( covid - 19 ) [ 3 ] , has spread rapidly throughout china and beyond [ 2 , 4 ]  . on 21 february 2020 , sars - cov - 2 infection was also detected in northern italy . 
since then , the number of * andrea borghesi andrea.borghesi@unibs.it 1 department ofmedical andsurgical specialties , radiological sciences andpublic health , university ofbrescia , asst spedali civili ofbrescia , piazzale spedali civili , 1 , 25123brescia , italy sars - cov - 2 infection cases has grown exponentially . 
on 8 march 2020 , the number of italians with sars - cov - 2 infection was 7375 with a 48% hospitalization rate ( 18% in intensive care units ) and a 5% mortality rate . at present , the reference standard to make a definitive diagnosis of sars - cov - 2 infection is the reverse - transcription - polymerase - chain - reaction assay ( rt - pcr ) [ 5 ]  . radiological imaging plays a crucial role in the detection and management of covid - 19 patients . 
computed tomography ( ct ) imaging is considered the most effective method for the detection of lung abnormalities , particularly in the early stage of the disease [ 4 , 612 ]  . 
moreover , serial chest ct imaging with different time intervals ( from three to seven days ) is also effective in assessing the disease progression ( from the time of initial diagnosis of covid - 19 until patient discharge ) [ 6 , 7 , 13 ]  . however , the increasing number of hospitalized patients and the consequent increase in radiological examinations would make the constant use of chest ct scan ( from diagnosis to discharge ) difficult to sustain over time . 
therefore , in our radiology department , we are trying to limit the vol . : ( 0123456789 ) 1 3 510 la radiologia medica ( 2020 ) 125 : 509513 use of ct imaging for monitoring patients with confirmed infection . although chest x - ray ( cxr ) is considered not sensitive for the detection of pulmonary involvement in early - stage disease [ 4 , 14 ] , we believe that , in the current emergency setting , cxr ( standard or bedside ) can be a useful diagnostic tool for monitoring ( day after day ) the rapid progression of lung abnormalities in covid - 19 , particularly in critical patients admitted to intensive care units . the radiological quantification of the severity and progression of lung abnormalities is of great importance in determining the appropriate clinical management and respiratory support for infected patients . 
at the present time , different ct scoring systems and only one cxr scoring system were applied to quantify the pulmonary involvement in covid - 19 [ 6 , 7 , 11 ]  . 
this cxr scoring system is a simple five - point grading tool that was proposed in 2015 , and it was designed for non - radiologist clinicians [ 15 ]  . 
the goal of this scoring system was to facilitate the clinical grading of cxr reports into five different severity categories in hospitalized patients with acute respiratory infection . to the best of our knowledge , there are no published papers in which a dedicated cxr grading system for covid - 19 pneumonia has been designed for radiologists . the aim of this short communication is to present our experimental cxr scoring system that we are applying to hospitalized patients with covid - 19 pneumonia . 
we also assessed the validity of this cxr scoring system on a sample of 100 hospitalized patients with sars - cov - 2 infection for whom the final outcome ( recovery or death ) was available . materials andmethods cxr scoring system based on the current knowledge of common chest ct findings in covid - 19 pneumonia ( ground - glass opacity with or without patchy consolidation ) [ 4 , 68 , 1012 ] , we designed a dedicated cxr scoring system for hospitalized patients with sars - cov - 2 infection ( confirmed by rt - pcr )  . our cxr scoring system for covid - 19 pneumonia ( which we named brixia score ) includes two steps of image analysis . in the first step , the lungs are divided into six zones on frontal chest projection ( posteroanterior or anteroposterior projection according to the patient position ) ( fig.1 ) : upper zones ( a and d ) : above the inferior wall of the aortic arch middle zones ( b and e ) : below the inferior wall of the aortic arch and above the inferior wall of the right inferior pulmonary vein ( i.e. , the hilar structures ) fig . 
 line b is drawn at the level of the inferior wall of the right inferior pulmonary vea and d upper zones ; b and e middle zones ; c and f lower zones lower zones ( c and f ) : below the inferior wall of the right inferior pulmonary vein ( i.e. , the lung bases ) for technical reasons ( for example bedside cxr in critical patients ) , it could be difficult to identify some anatomical landmarks . 
near to the overall score , the partial score of each zone ( from a to f ) is also entered between square brackets . other cxr findings ( such as pleural effusion , pulmonary vessel enlargement ) , not included in the scoring system , are recorded in the descriptive part of the cxr report . an example of our cxr report is shown below : chest x - ray symmetrical lung expansion . 1 3 la radiologia medica ( 2020 ) 125 : 509513 to these 100 cxr reports was independently assessed by an experienced thoracic radiologist who reassigned the score for each cxr examination . to determine the agreement between radiologists in the application of the new cxr scoring system , the first score of each cxr examination was compared with the second score reassigned by the experienced thoracic radiologist . 
we use the kw ( specifically the linear kw ) because the cxr scoring system was designed on an 18 - point continuous - ordinal scale and the degree of disagreement between the scores had a different weight . 
p - values of less than 0.05 were considered statistically significant . results the score entered in the cxr reports ranged from 0 to 16 ( median 6.5 ; interquartile range 211 )  . 
it is quite simple and can be easily replicated in other clinical settings . we obviously realize that this method required further studies to confirm its validity because the score depends mainly on the quality of the cxr images and the experience of the observers . 
the purpose of this study was to retrospectively evaluate correlations between the cxr score and the age or sex of italian patients infected with sars - cov - 2 . materials and methods between march 4 , 2020 , and march 18 , 2020 , all cxr reports containing the new scoring system were retrieved . 
nonparametric statistical tests were used to examine the relationship between the severity of lung disease and the age or sex . results 783 italian patients ( 532 males and 251 females ) with sars - cov - 2 infection were enrolled . 
males aged 50years or older and females aged 80years or older with coronavirus disease 2019 showed the highest cxr score ( median 8 )  . conclusions males aged 50years or older and females aged 80years or older showed the highest risk of developing severe lung disease . 
our results may help to identify the highest - risk patients and those who require specific treatment strategies . keywords sars - cov - 2 covid - 19 chest x - ray scoring system introduction severe acute respiratory syndrome coronavirus 2 ( sarscov - 2 ) is a betacoronavirus that was discovered to be responsible for an acute respiratory syndrome called coronavirus disease 2019 ( covid - 19 ) [ 13 ]  . 
to improve the risk stratification and aid clinicians in defining a tailored level of care for highrisk patients , an experimental chest x - ray ( cxr ) scoring system for quantifying the severity and progression of lung abnormalities in covid - 19 pneumonia was introduced in our diagnostic imaging department [ 10 ]  . 
the selected patients were divided into seven groups according to age : 2029 years ( group a ) , 3039years ( group b ) , 4049years ( group c ) , 5059years ( group d ) , 6069years ( group e ) , 7079years ( group f ) , and 80years ( group g )  . statistical analysis the data are presented as the number ( % ) or the median and the interquartile range because the age of the patients and the cxr score were not normally distributed . 
p values of < 0.05 were considered statistically significant . results the search identified 783 italian patients ( 532 males and 251 females ) with confirmed sars - cov - 2 infection ( table1 )  . 
the cxr score of group f was significantly higher than that of group c . discussion the literature reports that older age and underlying comorbidities ( such as hypertension , diabetes , cardiovascular disease , and oncologic history ) are risk factors of fatal outcome in adult patients with confirmed sars - cov - 2 infection [ 69 ]  . 
however , the currently available data on covid - 19 were obtained exclusively from asian patients . to the best of our knowledge , this study is the first to examine the relationship between the severity of lung disease and the age or sex in european ( italians ) patients . 
in addition , no published study used a radiographic severity index to analyze these correlations . in our large sample , 67.9% of hospitalized patients were males and only 15.2% were younger than 50years . 
obviously , we realize that further studies , particularly enrolling european patients , are needed to confirm the effectiveness of this new cxr scoring system in predicting the risk of worst outcome . the main limitations of this study include the retrospective nature of our analysis and lack of comparison between cxr score and patient comorbidities ( such as hypertension , diabetes , cardiovascular disease , and oncologic history ) or final outcome ( recovery versus death ) because these clinical data were only available in a small percentage of patients due to the short time for case collection and the large sample size . in conclusion , we found that males aged 50 years or older and females aged 80years or older showed the highest risk of developing severe lung disease . 
3 box - and - whisker plots showing the distribution of chest x - ray ( cxr ) scores by age group in males ( m ) and females ( f ) acknowledgements the authors thank their colleagues in the diagnostic imaging department , asst spedali civili of brescia . 
 ( savona , italy ) for the outstanding technical support . funding the author states that this work has not received any funding . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures followed were in accordance with the ethical standards of the responsible committee on human experimentation ( institutional and national ) and with the helsinki declaration of 1975 , as revised in 2008 . 
currently , it is unknown how well cmr - ft - based strain values agree with manually obtained strain values . methods in 45 subjects ( 15 controls , 15 acute myocardial infarction , 15 non - ischemic dilated cardiomyopathy ) , end - systolic manually derived strains were compared to four cmr - ft software packages . 
statistical analysis included blandaltman plots , intra - class correlation coefficient ( icc ) and coefficient of variation ( cv )  . results manual contouring yielded excellent intra - observer ( icc 0.903 ( grs ) to 0.995 ( gcs ) ) and inter - observer agreement ( icc 0.915 ( grs ) to 0.966 ( gcs ) ) with cv ranging 4.7% ( gcs ) to 20.7% ( grs ) and 12.7% ( gcs ) to 20.0% ( grs ) , for intra - observer and inter - observer agreement , respectively . 
although echocardiographic speckle tracking is clinically the most used approach , feature - tracking software applied to cine cardiovascular magnetic resonance ( cmr ) images provides strain images as well , and it has the advantage that it is part of a comprehensive examination , providing in - depth evaluation of the myocardium using a combination of myocardial mapping vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 444450 and contrast - enhanced images . 
besides the image or feature - tracking algorithms , based on optical flow technology , using the differences in signal intensity between myocardium and surrounding structures , to propagate endoand epicardial contours over the cardiac cycle , also elastic , non - rigid deformation algorithms are available to estimate myocardial strain in shortand long - axis direction [ 2 , 5 , 6 ]  . 
moreover , excellent intraand inter - observer reproducibility as well as good inter - study agreement has been reported [ 1118 ]  . in a recent publication , comparing three software packages using optical flow technology and one software using a non - rigid deformation algorithm in a cohort of 45 patients , we reported the best intraand inter - observer reproducibility for the elastic deformation algorithm but found significantly lower values for global radial and longitudinal strain compared to the other software packages [ 19 ]  . 
to clarify this discrepancy and to better understand its value in the clinical setting , we decided to compare the above cmr - ft data to a manually derived strain value obtained by two observers not involved in the contouring of the cmr - ft study . methods for the current study , we re - used the same patient dataset as we used before to study the reproducibility of global myocardial strain comparing 4 different software packages [ 19 ]  . 
 the cohort included 45 patients , with a first group ( n = 15 ) presenting normal cmr findings , i.e. , lv ejection fraction 50% , end - diastolic lv wall thickness 12mm and no myocardial enhancement at late gadolinium enhancement imaging ( control group )  . 
for assessment of lv dimensions and function , steady - state free - precession breath - hold cine images were acquired in the following orientations : vertical and horizontal long - axis , short - axis and left ventricular ( lv ) outflow tract view . 
for the late gadolinium enhancement studies , a dose of 0.15ml of gadobutrol ( gadovist , bayer ) per kilogram of body weight was administered , and we used a breath - hold t1 - weighted three - dimensional contrast - enhanced phase - sensitive inversion - recovery ( psir ) gradient - echo sequence in cardiac short - axis , vertical long - axis and horizontal long - axis view ; psir images were acquired 10to 15 - min post - contrast administration . 
manual contouring was performed on the vertical and horizontal long - axis , as well as on the same three ( i.e. , basal / mid / apical ) short - axis cine images as used in reference [ 19 ]  . 
as we reported myocardial strain at end systole , manual contouring was performed at both end diastole and end systole by two experienced cmr readers ( i.e. , at least two years of cmr experience ( pp , jb ) )  . 
global circumferential and longitudinal strains are expressed as the mean of the endo and epicardial strato calculate radial strain , a centerline technique was applied defining the center between the endo and epicardial contours in short - axis direction on which 100 chords were defined . 
the average change in chord length between end diastole and end systole expresses the global radial strain . statistics all cmr studies were performed on a 1.5 t unit ( ingenia ; philips healthcare ) by using commercially available cmr imaging software , electrocardiographic triggering and summary statistics for continuous variables are presented as mean standard deviation ( sd ) or medians with interquartile ranges ( iqr ) , as appropriate . 
differences between manual contouring and the four cmr - ft software packages were tested with one - way analysis of variance ( anova ) with post hoc unpaired t tests with tukey hsd correction for multiple comparisons . 
inter - observer ( two readers ) and intra - observer ( two readings ) reproducibility was assessed by using the absolute mean error , intra - class correlation coefficients ( iccs ) and the coefficient of variation ( cv ) and compared to the data obtained by cmr - ft software . 
in table1 are shown the relevant clinical and cmr data . manual intra andinterobserver agreement as shown in table2 , manual contouring yielded an excellent intraand inter - observer agreement with icc values ranging 0.903 ( grs ) to 0.995 ( gcs ) for intra - observer and 0.915 ( grs ) to 0.966 ( gcs ) for inter - observer variability . 
dcm , dilated cardiomyopathy ; gcs , global circumferential strain ; gls , global longitudinal strain ; grs , global radial strain ; sd , standard deviation ( grs ) and 12.7% ( gcs ) to 20.0% ( grs ) for intraand inter - observer reproducibility , respectively . 
 in contrast , medviso and circle yielded significantly different values at anova in one or more strain directions , i.e. , grs for circle and grs and gcs for medviso . 
gcs , global circumferential strain ; gls , global longitudinal strain ; grs , global radial stra * significantly different from manual contours in anova with post hoc tukey hsd correction for multiple comparisons la radiologia medica ( 2020 ) 125 : 444450 fig . 
as myocardial strain yields independent prognostic value over well - accepted functional parameters , such as ejection fraction , there is increasing interest to measure and report global myocardial strain values in addition to ejection fraction [ 1 , 3 ]  . 
typically , myocardial contours are drawn on shortand / or long - axis cine cmr images at one time frame of the cardiac cycle and then propagated over the rest of the cine images , providing timestrain curves [ 2 ]  . 
in this study , we reported end - systolic strain , as it is most frequently used . the current study not only complements , but also sheds light on the reasons for the rather poor inter - vendor agreement between cmr - ft vendors in particular for gls and grs as reported before [ 19 ]  . 
firstly , cmr - ft is equal or even superior to ( expert ) manual contouring regarding intra - observer and inter - observer reproducibility ( see supplementary table )  . 
as shown in panel a , b , i and j of fig.3 , there is a clear inverse relation between magnitude of grs and gls and strain underestimation with a strong trend toward systematic bias . these observations emphasize the need to assess reproducibility together with accuracy . 
while reproducibility assessment is quite straightforward , validation of new approaches is often more challenging , in particular when the reference technique ( i.e. , gold standard ) faces similar challenges as the technique under study . 
cmr - ft software has been compared to spatial modulation of magnetization ( spamm ) myocardial tagging , harmonic phase imaging ( harp ) and invasive strain measures such against sonomicrometry , showing moderate to good correlation [ 5 , 810 , 14 , 24 ]  . 
when comparing intraand interobserver agreement , cmr - ft software performs similar ( or even superior ) to manual contouring , which is definitely encouraging as computer - aided support not only shortens analysis time , but on top provides strain values over the entire cardiac cycle , something which is too time - consuming to be done manually . 
 however , this setup reflects clinical routine as the time between contrast administration and acquisition of the lateenhancement images is used for cine imaging , and thus to shorten total cmr time . 
extrapolating our findings , we think to the observed differences between some cmr - ft and manual approach will only get larger . 1 3 450 la radiologia medica ( 2020 ) 125 : 444450 in conclusion , this study emphasizes to be cautious to clinically use some cmr - ft algorithms to assess global myocardial strains . 
thus , according to our initial evidence , we recommend to perform seriate chest x - rays in the days following the onset of mechanical ventilation even if the immediate monitoring suggests an improvement . 
studies on a larger scale are necessary to fully assess the findings at chest radiographs of critical , mechanically ventilated patients and their correlation with the long - term outcome . keywords covid - 19 radiology chest x - ray outbreak introduction the current global outbreak of covid - 19 represents a major challenge in terms of epidemiology , contagiousness , treatment , as well as clinical and radiological behavior of this disease [ 1 ]  . 
radiological imaging plays a key role in the diagnostic process and during the monitoring of the clinical conditions especially of patients in the intensive care unit ( icu ) [ 2 ]  . 
in particular , using computed tomography ( ct ) not only the extension and the severity of the disease can be precisely characterized , but according to the recent study of bai etal . 
nevertheless , in the following days , over an interval of 6days from intubation , four patients previously stable or with a former improvement ( overall 33.3% ) had a rapid worsening of the vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 514516 fig . 
due to a worsening of the clinical conditions , during the second day after admission , he underwent endotracheal intubation ( b ) with a significant improvement of the radiological findings within 24 h ( c )  . 
within 6days , 89% of the patients ( n = 16 ) showed a wide patch of parenchymal consolidations at imaging , a finding which is consistent with the literature [ 3 , 4 ]  . 
thus , according to our preliminary evidence , we recommend to perform seriate chest x - rays in the days following the onset of mechanical ventilation even if the immediate monitoring suggests a radiological amelioration of the pattern . several studies already demonstrated the chameleonic and heterogeneous behavior of covid - 19 infections [ 6 ]  . 
thus , ct also taking advantage of low - dose protocols certainly plays a pivotal role not only in detecting subtle initial findings , but it also accurately characterizes severe cases [ 9 ]  . chest x - ray , on the contrary , surely has a limited role in diagnosing the most common initial pattern of covid - 19 typically defined by ground glass . 
nevertheless , we should not overlook the importance of this tool in clinical practice , especially when dealing with hospitalized patients in icu affected by severe infections with pulmonary consolidations . in fact , traditional imaging can guarantee a reliable continuous monitoring of icu patients and guide therapeutic decisions . in the province of hubei , the introduction of ct changes among the diagnostic criteria for covid - 19 led to an improvement in the diagnostic performance [ 5 ]  . 
a data analysis was performed at the end of the literature search . results eight original articles with prospective design and one with retrospective design were included in this review : 4 studies focused on rheumatoid arthritis , 2 on rheumatoid and other arthritides , 1 on lateral epicondylosis and 2 on carpal tunnel syndrome . 
despite some methodological differences , all studies compared the performance of smi with that of a conventional doppler technique such as power and color doppler and found an improvement in vascularity detection with smi . 
future investigations should include larger samples of patients with long - term follow - up . keywords doppler microflow imaging musculoskeletal imaging superb microvascular imaging ultrasound introduction in the recent years , ultrasound ( us ) has progressively gained a central role in the evaluation of the musculoskeletal system [ 13 ]  . 
us is a cost - effective , time - saving and noninvasive modality which enables a thorough evaluation of most superficial structures in the musculoskeletal system [ 48 ] * carmelo messina carmelo.messina@unimi.it 1 dipartimento di scienze biomediche perla salute , universit degli studi di milano , via luigi mangiagalli 31 , 20133milano , italy irccs istituto ortopedico galeazzi , milano , italy 3 asst grande ospedale metropolitano niguarda , milano , italy 4 dipartimento di radiologia e neuroradiologia pediatrica , ospedale dei bambini v . 
buzzi , milano , italy 5 sezione di scienze radiologiche , dipartimento di biomedicina , neuroscienze e diagnostica avanzata , universit degli studi di palermo , palermo , italy and has the unique capability to visualize the vascularity of soft - tissue structures thanks to the integration with doppler techniques , such as power doppler ( pd ) and color doppler ( cd ) imaging [ 9 ]  . 
among them , superb microvascular imaging ( smi ; canon medical systems , otawara , japan ) is a relatively new technique that can differentiate flow signals from overlaying tissue motion artifacts , thus preserving small slow - flow vessels with high detail and definition . 
the color mode depicts the same vessels as a color overlay image , namely giving b - mode and color information simultaneously [ 11 ]  . the first studies on smi investigated its role in breast [ 1214 ] , testes [ 15 ] and thyroid [ 16 ]  . 
our purpose is to systematically review the current literature concerning the role of smi in the evaluation of musculoskeletal disorders . materials andmethods a systematic review was conducted for the period 2013 to april 2019 , starting from the first applications of smi , using the pubmed and medline databases . 
inclusion criteria were : ( 1 ) studies dealing with musculoskeletal applications of smi ; ( 2 ) involvement of human participants ; ( 3 ) english language ; ( 4 ) statement that approval from the local ethics committee and informed consent from each patient or a waiver for it were obtained . 
a data analysis was conducted at the end of the literature search . results the database search process retrieved 134 articles published between 2013 and april 2019 ; of these , 10 articles dealt with musculoskeletal applications of smi [ 1827 ]  . 
a case series illustrating the use of smi for evaluating rheumatoid arthritis [ 18 ] and a narrative review dealing with clinical applications of smi in the skeletal muscle as well as other organs [ 19 ] were excluded from our analysis . 
specifically , four studies focusing on rheumatoid arthritis only , two on rheumatoid and other arthritides , one on lateral epicondylosis and two on carpal tunnel syndrome are included [ 2028 ]  . 
figure2 shows a case of patellar insertional tendinopathy ( jumpers knee ) depicted using pd and smi from our experience . meta - analysis of data was not possible due to the low number of papers for each condition and the different parameters evaluated in each study . discussion our main finding is that clinical application of smi in the musculoskeletal system has commenced in patients with rheumatoid arthritis , other inflammatory arthritides and osteoarthritis , lateral epicondylosis and carpal tunnel syndrome . 
apart from some methodological differences , all 1 3 la radiologia medica ( 2020 ) 125 : 481490 1 3 484 la radiologia medica ( 2020 ) 125 : 481490 1 3 la radiologia medica ( 2020 ) 125 : 481490 table 2 scoring systems adopted for vascularity assessment using smi and conventional doppler imaging in different musculoskeletal disorders , according to the current literature authors disease scoring system rheumatoid arthritis li etal . 
 [ 23 ] 0 : no vascular signal in the synovium 1 : single vascular signal in the synovium 2 : vascular signals in less than half of the area of the synovium 3 : more than half of the area of the synovium covered by vascular signals lim etal . 
 [ 26 ] rheumatoid arthritis and other arthritides 0 : no vascular signal in the synovium 1 : smi detected up to 25% more vessels than pd or vice versa 2 : smi detected 2550% more vessels than pd or vice versa 3 : smi detected more than 50% of vessels than pd or vice versa 1 : up to 3 vascular signals in the synovium 2 : more than 3 vascular signals in less than half of the area of the synovium 3 : more than half of the area of the synovium covered by vascular signals 0 : no vascular signal in the synovium 1 : 12 vascular signals in the synovium 2 : 34 short linear vascular signals in less than half of the area of the synovium 3 : more than half of the area of the synovium covered by vascular signals 0 : no vascular signal 1 : 1 or 2 focal color - encoded spots 2 : 1 linear or more than 2 focal color - encoded spots 3 : more than 1 color - encoded linear spots 0 : no blood flow 1 : 1 to 2 spot blood flow 2 : more than 2 spot blood flow or 1 to 2 strip blood flow ( longer than 1 mm ) 3 : more than 2 strip blood flow yu etal . 
 [ 21 ] carpal tunnel syndrome nine studies share the common purpose of comparing the diagnostic performance of smi with that of a conventional doppler technique , such as pd and / or cd . 
additionally , inter - observer agreement for smi was moderate - to - excellent in the evaluated papers and these data support the fact that it is a reliable and reproducible technique . 
the following paragraphs address the role of smi in several musculoskeletal disorders , as emerged from our analysis of the current literature . rheumatoid arthritis rheumatoid arthritis is a chronic systemic inflammatory disease that primarily affects the synovial membrane [ 29 ]  . 
 doppler us techniques have been largely demonstrated to be excellent in evaluating changes in synovial vascularity resulting from either natural history of the disease or response to therapy [ 3133 ]  . 
specifically , pd has been reported to improve the accuracy of the 2010 american college of rheumatology / european league against rheumatism classification criteria for rheumatoid arthritis [ 34 ]  . 
 owing to its capability of depicting low - velocity flow and minute blood vessels , smi has the potential to become of major importance in the evaluation and treatment planning of patients with rheumatoid arthritis . to date , rheumatoid arthritis has received most of the attention regarding smi , and several studies focused on the assessment of rheumatoid synovitis using smi ( table1 )  . 
examined wrist and hand joints in 30 patients with early rheumatoid arthritis or rheumatoid arthritis under treatment with rituximab and demonstrated that smi detected a higher degree of synovial vascularity compared to pd [ 25 ]  . 
 found smi to be more sensitive than pd for detecting hand and wrist synovitis in a series of 26 patients with rheumatoid 1 3 486 la radiologia medica ( 2020 ) 125 : 481490 need for a different scoring system taking into account the different features of smi compared to conventional doppler techniques [ 25 , 26 ]  . 
did not use an absolute scoring system for vascularity assessment but evaluated pd and smi signals relative to each other , scanning primarily hand and wrist joints in 19 patients with rheumatoid arthritis [ 24 ]  . 
specifically , when vascular signal was detected on both pd and smi , its conspicuity was graded with a visual analogue scale comparing these two techniques based on sensitivity and resolution . 
this study also included patients with other forms of arthritis , and no separate data analysis was provided for thehowever , these authors reported that smi increased overall conspicuity of vascular signal in symptomatic joints in comparison with pd . 
hence , future prospective investigations with long - term follow - up are required to validate the role of smi and properly define its clinical applicability in patients with rheumatoid arthritis . other arthritides the presence of vascularity plays a key role in the evaluation of patients with joint pain and swelling , in particular those patients with some form of arthritis , as increased vascularity indicates active disease [ 37 ]  . 
previous studies showed that , although pd signal is related to active inflammation , the lack of vascular flow on pd cannot reliably exclude disease activity [ 3840 ]  . 
thus , smi appears of great value where pd is currently the reference standard for the assessment of active joint inflammation , including inflammatory arthritides and osteoarthritis [ 41 , 42 ]  . according to our review , only a few studies investigated the role of smi in the assessment of non - rheumatoid synovitis and their findings disagree . 
comprised , further than those with rheumatoid arthritis , 2 patients with osteoarthritis , 2 with seronegative spondyloarthropathy , 2 with polymyalgia rheumatica , 1 with unclassified arthritis , 1 with systemic lupus erythematosus , 1 with mixed connective tissue disease , 1 with adult - onset stills disease , 1 with granulomatosis with polyangiitis and finally 1 with sarcoidosis [ 26 ]  . 
a pd shows hypervascularity of the patellar tendon ( arrowheads ) at its proximal insertion into the patella ( p ) , b in the same patient , color mode smi and c monochrome mode smi show tendon hyperemia , which consists of two linear vascular signals and is more conspicuous than vascularity detected using conventional doppler imaging . 
evaluated hand and wrist joints in 56 patients and reported that smi correlated with pd and was more sensitive for detection of rheumatoid synovitis , even in the subsets of 28 patients with clinical remission and 17 patients with available followup information [ 23 ]  . 
of note , however , these five studies [ 23 , 2528 ] used semiquantitative scoring systems based on the absolute quantity of synovial vascular signals that were originally suited for pd ( table2 ) [ 35 , 36 ]  . 
hence , some authors underlined the 1 3 la radiologia medica ( 2020 ) 125 : 481490 included , in addition to those with rheumatoid arthritis , 27 patients with osteoarthritis , 16 with inflammatory arthritis , 9 with psoriatic arthritis and 12 with no definitive diagnosis at the time of study [ 24 ]  . 
further investigations may be aimed to analyze different forms of arthritides separately to understand whether smi has a major role and clarify its applicability in clinical practice . insertional tendinopathy insertional tendinopathies are painful overuse - related disorders , in which the capability of the tendons to repair is compromised [ 4347 ]  . 
this increased vascularity can be detected using conventional doppler techniques , although some studies suggested that doppler imaging has yet to reach the desired accuracy rates in visualizing neovessels in tendons [ 50 , 51 ]  . 
smi can depict slow - flow fine vessels and then has the potential to improve the results of conventional doppler modalities in this setting . according to our review , arslan et al . 
compared the diagnostic performance of smi and other us modalities for diagnosing lateral epicondylosis in 44 patients , using a four - point grading system for smi [ 20 ]  . 
such preliminary findings suggest that smi may improve diagnostic accuracy for detecting tendon neovascularization ; thus , other insertional tendinopathies deserve further investigation . entrapment neuropathy peripheral nerves are provided by a rich anastomotic system of blood vessels extending from epineuria to fascicles [ 52 , 53 ]  . 
this hypervascularity can be assessed using pd and cd , and doppler signal has been shown to increase in patients with nerve entrapment in comparison with healthy individuals [ 5558 ]  . 
the main reason behind may be that intraneural vessels are fine and blood flow is slow ; thus , conventional doppler techniques may fail to detect true vascularity within the nerve . 
thus , smi may be of great value in the assessment of increased intraneural blood flow resulting from nerve entrapment . according to our results , only two studies investigated the use of smi in entrapment neuropathies , focusing on carpal tunnel syndrome . 
compared the value of smi with pd and cd in 50 patients with carpal tunnel syndrome , using a semiquantitative scoring system based on richness of vascular signal within the median nerve [ 21 ]  . 
the blood flow display ratio ( i.e. , number of patients with some vascular signal / total number of patients ) for smi was significantly higher than that of pd and cd ; then , smi was more sensitive in demonstrating intraneural vascularity when compared with conventional doppler imaging . 
additionally , b - mode us evaluation of nerve cross - sectional area was combined with smi , pd and cd , and the highest diagnostic accuracy resulted from combination with smi [ 21 ]  . 
blood flow images were interpreted using a four - point grading systethis study was in accordance with chen etal . , as smi was more sensitive for quantifying intraneural vascularity in comparison with pd . 
further studies using smi to evaluate the relationship between increased intraneural blood flow and other entrapment syndromes are necessary . conclusion this study is limited to a systematic review of the literature , and no meta - analysis was performed because of the lack of homogeneity between studies in terms of evaluated diseases and parameters . 
despite this limitation , in the light of the current literature , smi may have a great potential for the diagnosis and grading of different musculoskeletal disorders , as well as treatment planning and therapeutic response monitoring . 
preliminary studies have shown promising results in patients with rheumatoid arthritis , lateral epicondylosis and carpal tunnel syndrome , where the combined use of smi and b - mode us achieved the highest diagnostic performance in certain conditions . 
potential risk - related factors of as events were determined via univariate and multivariate logistic regression analyses . results the rate of as events after uae for adenomyosis was 12.82% ( 25 / 195 )  . 
and adenomyosis patients with low vascularity should be carefully selected to undergo uae treatment . keywords adenomyosis asherman syndrome angiography uae introduction recent studies suggest that uterine artery embolization ( uae ) is an effective treatment for adenomyosis [ 14 ]  . 
several studies * yongqiang yu csirwyg85@yeah.net 1 department ofradiology , the first affiliated hospital , anhui medical university , 218 jixi street , hefei230022 , pa , peoplesrepublicofchina 2 department ofradiology , the first affiliated hospital , university ofscience andtechnology ofchina , 17 lujiang street , hefei230022 , pa , peoplesrepublicofchina 3 department ofradiology , women andchildren health care hospital affiliated hospital , anhui medical university , 15 yimin street , hefei230022 , pa , peoplesrepublicofchina show that uae has little effect on ovarian function [ 1316 ]  . 
 it has been reported that the incidence of asherman syndrome ( as ) in uterine myoma uae is about 10.2%13.7% and as arises from partial or complete endometrial damage or adhesions caused by uterine invasive diagnosis and treatment . 
 the inclusion criteria included patients with adenomyosis diagnosed by either magnetic resonance imaging ( mri ) or ultrasonography ( us ) and clinical symptoms of menorrhagia and dysmenorrhea , and those who expressed the desire to preserve the uterus . 
a nonionic contrast medium ( 300mg iodine / ml ; omnipaque ; ge , shanghai , china ) was used as the injection mediu angiography was performed using high - pressure injector at 68kpa of pressure ( abdominal aortography : 10ml / s , 2025ml ; uterine arterial angiography : 12ml / s , 68ml ) , during which the vascular characteristics of adenomyosis were observed . 
angiographic images were assessed using a digital post - processing workstation . the primary endpoints of embolization treatments included lesion occlusion , stasis of the distal end of the uterine artery , and decrease in flow to the proximal end of the uterine artery , at constant patency of the uterine artery . classification ofvascular types the vascular characteristics of adenomyosis were categorized by interventional radiologists as detailed by tang , zhou , and chen [ 1921 ]  . 
a hypervascular , which shows abundant peripheral blood flow and central blood flow of the lesions ; b an isovascular lesion with less blood flow on the center ; c a hypovascular lesion lack of vessels at either the periphery or the center 1 3 la radiologia medica ( 2020 ) 125 : 437443 fig . 
all intrauterine adhesions ( iua ) were evaluated based on the american fertility society ( afs ) scoring system and divided into three levels ( table2 ) [ 22 ]  . statistical analysis in both univariate and multivariate analyses , age , uterine size , type , secondary anemia , previous medical therapy , previous gynecological invasive therapy vascularity grade , vascular supply , ovarian branch development , uterine size , and pva vial dose were included to assess the factors affecting as . 
all vascular subtraction maps were distinguished by vascularity density , blood supply , and ovarian branch artery development , as shown in table3 . the 15 - month follow - up indicated that a total of 113 of the 147 patients ( 76.87% ) with dysmenorrhea and 136 of 159 patients ( 85.53% ) with menorrhagia experienced improvement after uae . 
three patients had severe uterus infection , and two of these three patients underwent a hysterectomy . a total of 27 patients had either oligomenorrhea or amenorrhea , two of which were an ovarian failure . 
 of seven patients ( two cases were moderate and five cases were severe ) who have fertility requirements undergoing 1 3 440 la radiologia medica ( 2020 ) 125 : 437443 table 3 intraoperative potential factor for asherman syndrome ( n = 195 ) category value vascularity grades hypervascular isovascular hypovascular vascular supply equal unequal number of pva vials 2 > 2 ovarian branch development unilateral bilateral none pva polyvinyl alcohol 85 ( 43.58% ) 53 ( 27.18% ) 57 ( 29.23% ) 149 ( 76.41% ) 46 ( 23.59% ) 126 ( 64.62% ) 69 ( 35.38% ) 83 ( 42.56% ) 43 ( 22.05% ) 69 ( 35.38% ) hysteroscopic adhesiolysis , only three cases showed improvement in afs scores and there is no case of a successful pregnancy . univariate logistic regression analyses showed that vascularity grades and uterine size were significantly associated with as after uae . 
the risk of as progression was increased ( table4 ) in patients with hypovascular lesions and uterine size 314.90cm3. following univariate analysis , the factors found to be significantly associated with disease progression were included in the multivariate analysis . 
after adjusting for all other factors , the multivariate analysis showed that the as in patients with hypovascular lesions was significantly higher than that in other patients ( table5 )  . discussion in the case of poor drug treatment of adenomyosis , including hormonal [ 23 ] , uae as a conservative treatment can effectively improve the symptoms of adenomyosis [ 24 , 25 ]  . 
however , the effect of adenomyosis on the fertility outcome after uae treatment remains to be further explored ; compared to myoma embolization , literature data as well as guidelines concerning the role of embolization in adenomyosis are still scarce , and whether it can replace hysterectomy depends on this [ 26 ]  . this study retrospectively analyzed as in 195 patients with adenomyosis after uae treatment . 
previous studies have shown that vascularity grades in uterine myoma are related to the clinical efficacy and complications of uae and consider that the same procedures are applied to study adenomyosis [ 20 , 27 , 28 ]  . 
however , dsa is the current gold standard for evaluating the distribution of blood flow to the lesion [ 33 ] , and it can accurately identify the abundance of vessels in adenomyosis lesions . 
the cause is speculated to be as follows : ( 1 ) compared with the adenomyosis , lesions of myoma usually have a more abundant blood supply ; ( 2 ) adenomyosis lesions often show an ill - defined margin and no regular pattern , and endometrial cells and focal angiogenesis undergo a progressive process similar to that of tumor metastasis . 
however , most uterine myoma has a pseudo - envelope [ 19 , 30 , 35 ]  . the above speculations lead to reduced efficiency of embolic agents into the lesions and increase the likelihood of reflux , despite super - selective catheterization . 
however , in order to achieve an endpoint of embolization , a small amount of embolic agent reflux is inevitable , resulting in ectopic embolization including normal myometrium , especially at the end of the embolization in the area with low vascularity , the injection of a higher - density contrast agent may displace the lower - density particles , causing embolic agent reflux [ 36 ]  . 
 by contrast , there are well - developed vessels in hypervascular areas , and the embolic agent reaches farther than the hypovascular regions , which results in the avoidance of the embolization of nontarget vessels . as events were significantly higher in the low vascular adenomyosis compared with the high vascular adenomyosis , which is like the above view , because the flow made it difficult for the embolic agent to reach the target vessel and reflux deposited more embolic agents into the surrounding myometriuand there will be a series of ischemic , incomplete , or complete necrosis and inflammatory reactions after embolization [ 37 , 38 ]  . 
treatment of adenomyosis by uae can lead to the destruction of parts of the uterine myometrium and the endometrial basal layer , secondary iua , and endometrial atrophy resulting in as . 
therefore , further research should consider these aspects . 1 3 442 la radiologia medica ( 2020 ) 125 : 437443 in conclusion , the grades of vascularity were found to be an independent prognostic factor affecting as after uae for adenomyosis . 
the imaging was obtained before and immediately exercise ; additionally , imaging was performed at 3h , 6h , and 24h after exercise , and an ivim index was calculated . 
a correlation was found between the ivim index at 24h after exercise and the degree of the muscle ache ( r = 0.80 ) conclusions the capillary blood volume significantly increased after exercise when compared to before exercise . 
there was a correlation between the degree of muscle ache and the amount of capillary blood volume measured from the femoral muscle at 24h after exercise . keywords intravoxel incoherent motion capillary blood flow dwi muscle muscle ache introduction diffusion - weighted imaging ( dwi ) of the human body is based on restricted diffusion , which depends on the size of the cellular constituents [ 15 ] and on perfusion information by incoherent motion , such as in capillaries . 
there are many studies , which have reported using ivim to evaluate the differentiation and malignancy grade of tumor lesions in the prostate , liver , brain , breast , and pancreas [ 817 ]  . 
the evaluation of capillary blood volume is a very important tool , clinically ; however , these measurements are difficult to obtathe capillary blood volume of the superficial tissue is evaluated using an optical technique [ 18 , 19 ] , but it does not report on measurements found in the deep tissue . although it is known that intramuscular capillary blood volume increases with exercise , there is little known about the time course of these patterns following exercise . 
furthermore , the relationship between intramuscular capillary blood volume and muscle ache is still unclear [ 2022 ]  . the evaluation index of ivim is known as the pseudodiffusion coefficient [ d * ] and perfusion fraction [ f ] , although precision is low due to the influence of the t2 shine - through effect and measurement error [ 11 , 23 ]  . 
the v value is measured by fourier vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 474480 analysis for the diffusion signal decay curves with b values less than 50s / mm2 . the objective of this study was to evaluate the intramuscular capillary blood volume , before and after exercise , using specific indexes of ivim . 
in addition , we examined the association between muscle ache and capillary blood volume after the exercise . materials andmethods subjects andscanning parameters our institutions ethical review board approved this prospective study , and written informed consent was obtained from all volunteers recruited . 
the subjects were scanned by t1 - weighted imaging and echo planar diffusionweighted imaging of the limb with multi - b values on axial slices using a 32 - channel body array coil with a 1.5 - t clinical mri system ( ingenia ; philips medical systems , best , the netherlands )  . 
it was imaged five times over the following time course : before exercise ; just after exercise ; and at 3h , 6h , and 24h following the completion of exercise . 
all subjects were instructed to rest as much as possible during the first 24h after the exercise . the imaging parameters were tr = 3000 ms , te = 117ms , fov = 300mm , slice thickness = 5mm , phase encoding matrix = 120 , sense factor = 2 , and average = 2 . 
each subject was positioned feet first . interview andanalysis in addition , we measured the degree of muscle ache in the thigh and leg by interviewing the subjects during the 24 - h imaging session . 
participants were asked to rate the degree of their muscle ache using a 10 - point rating scale , with 10 representing maximal muscle ache and 0 representing no muscle ache . three radiologists ( with 8 , 12 , and 31years of experience , respectively ) set circular regions of interest ( rois ) to the diffusion - weighted images of the thigh muscle and the leg muscle of each b value , and each signal intensity was measured . 
d is calculated by the following equation : d = ln ( s1000s100 ) ( 1000 100 ) here , s1000 and s100 are signal intensities of b = 1000 and 100s / mm2 . 
f is calculated by the following equation : f = ( s0 sinter ) s0 here , sinter is the intersection point of the y - axis and line through ln s1000 and s100 . 
the size of the roi was 10 mm in diameter , and the settings were set so as not to include the great vessels ( by the consultation of three radiologists ) 1 3 476 la radiologia medica ( 2020 ) 125 : 474480 fig . 
2 association with the pseudo - diffusion coefficient [ d * ] , perfusion fraction [ f ] , vascularity value [ v ] , and apparent diffusion coefficient [ adc ] for the diffusion decay curve fig . 
3 signal intensity of dwi of the multi - b values of the thigh muscle during each time interval ( before exercise , just after exercise , and at 3h , 6h , and 24h after exercise )  . 
finally , the apparent diffusion coefficient [ adc ] was calculated using the signals of dwi with b = 0 and 1000s / mm2 . the correlation between the degree of muscle ache and each ivim index was analyzed for the thigh and leg of eleven subjects . 
the coefficient of correlation with the v value was 0.8051 , and with the f value , it was 0.6529. results the signal intensities of the dwi using multiple b values at each time interval ( before and after exercise , and at 3h , 6h , and 24h after exercise ) are shown in fig.3. 
however , changes in the discussion it is known that the number of capillaries and capillary blood volume decrease with aging and increase by performing exercise [ 21 , 22 , 2426 ]  . 
therefore , in this study , to evaluate whether such an approach is possible , we examined capillary blood volume measurement by using the ivim of dwi . according to the results of this study , the v , d * , and f values ( used as the ivim index ) increased after exercise when compared with before exercise ; additionally , these values decreased at 3h after exercise when compared with the values measured immediately after exercise . 
the cause of the muscle ache remains unknown ; in the past , it was suggested that dull pain resulted from the inhibition of muscle oxygenation due lactic 1 3 la radiologia medica ( 2020 ) 125 : 474480 fig . 
however , this theory is no longer accepted , as it has been shown that there is little association between muscle pain and lactic acid levels [ 28 ]  . 
 based on these results , it can be suggested that increased capillary blood volume and muscle ache may be associated with muscle inflammation . moreover , with respect to the index of ivim , the v value was more effective in reflecting capillary blood volume than the f and d * values . 
this result is consistent with those of other studies [ 26 ] , suggesting that the v value can be used to analyze the diffusion decay curve more precisely . one limitation of this study was the small number of patients included in the evaluation . 
 further studies are required to investigate the potential association between muscle ache and capillary blood volume . conclusions changes in the capillary blood volume of the muscle of the lower limb due to exercise were successfully measured by ivim . 
there was a positive correlation between the level of capillary blood volume of the thigh muscle at 24h after exercise and degree of the muscle ache . 1 3 478 la radiologia medica ( 2020 ) 125 : 474480 fig . 
 the purpose of our study is to develop and validate ct - based radiomics models for gist risk stratification . methods three hundred and sixty - six patients clinically suspected of primary gists from january 2013 to february 2018 were retrospectively enrolled , among which data from 140 patients were eventually analyzed after exclusion . 
the radiomics signature demonstrated favorable performance for the risk stratification of gists with an auc of 0.809 ( 95% ci 0.7770.841 ) and an accuracy of 67.5% for the validation cohort . 
meanwhile , this ct - based radiomics signature showed good diagnostic accuracy to distinguish between nonadvanced and advanced gists , as well as the four risk stratifications of gists . conclusion our findings highlight the potential of a quantitative radiomics analysis as a complementary tool to achieve an accurate diagnosis for gists . keywords computed tomography gastrointestinal stromal tumors radiomics diagnosis introduction gastrointestinal stromal tumors ( gists ) , which often occur in the stomach or small intestine , are the most common primary mesenchymal tumor of the gastrointestinal tract [ 13 ]  . 
cajal cells in the gastrointestinal tract wall are the origin of gists [ 4 , 5 ] , which have malignant potential as a result of activating mutations in the kit proto - oncogene or platelet - derived growth factor receptor alpha gene [ 6 , 7 ]  . 
 16 xinhua west road , cangzhou061000 , china 2 department ofpathology , cangzhou central hospital , cangzhou061000 , china 3 ge healthcare , shanghai210000 , china 4 department ofradiology , cangzhou renmin hospital , cangzhou061000 , china vol . : ( 0123456789 ) 1 3 466 la radiologia medica ( 2020 ) 125 : 465473 stratify gists into four risk categories : very low risk , low risk , intermediate risk and high risk [ 8 ]  . 
as the risk and malignant potential increase , gist patients prognosis decreases . until approximately the early 2000s , gists generally had a poor prognosis due to the lack of effective treatments . 
the discovery of imatinib mesylate , a small molecular inhibitor of receptor tyrosine kinases , has dramatically changed the outcome of patients with high - risk gists [ 9 ]  . 
in recent years , the pathological risk degree of gists has become an issue of great concern [ 10 ]  . computed tomography ( ct ) , a common pretreatment examination , is beneficial for showing tissues adjacent to the primary tumor in detail and determining metastasis or recurrence of gists [ 11 ]  . 
therefore , there is an increasing need for accurate and objective stratification of the gist risks using quantitative techniques . radiomics , which transforms medical images into mineable high - dimensional data , has recently shown a great potential in aiding clinical decision - making [ 18 ]  . 
 therefore , the purpose of our study was to develop and validate ct - based radiomics models for gist risk stratification . materials andmethods characteristics ofpatients this retrospective research was approved by our institutional review board in cangzhou central hospital , which waived the requirement for informed consent . 
the inclusion criteria were as follows : ( 1 ) surgical resection of the tumor and complete clinic - pathological data ; ( 2 ) no treatment prior to surgery ; ( 3 ) preoperative contrastenhanced ct examination with good image quality . 
the exclusion criteria were as follows : ( 1 ) unresectable tumor or endoscopic resection ; ( 2 ) with treatment before surgery ; ( 3 ) no preoperative contrast - enhanced ct or poorquality ct images . 
the study population characteristics are summarized in table1 . ct image acquisition all 140 patients underwent abdominal and / or pelvic contrast - enhanced ct examination covering the whole tumor using a 320 - detector row scanner ( toshiba medical systems , otawara , japan ) in our hospital . 
the ct imaging parameters were as follows : tube voltage 120kv ; tube current 100450ma ; rotation time 0.5s ; detector collimation 64 0.625mm ; matrix 512 512 ; pitch 0.61.2 : 1 ; thickness 5mfor dynamic contrast - enhanced ct imaging , an iodinated contrast agent ( 1ml / kg ) was intravenously injected at a rate of 3.5ml / s with an automatic power injector . 
all three phases of ct images were reconstructed using a thickness of 2mm . reference standard this study was divided into two parts , based on the nih 2008 consensus classification system [ 8 ] , which includes tumor size , mitotic count and tumor site ( table2 )  . 
the very - low - risk and low - risk categories were considered nonadvanced gists , while the intermediate - risk and high - risk categories were considered advanced gists . 
there were ultimately 100 patients in the training cohort and 40 patients in the validation cohort . tumor segmentation lesions were delineated on the ct arterial phase images using the itk - snap software ( available at org ) , because the arterial phase is better for distinguishing a tumor mass from adjoining normal tissue . 
the whole - tumor volume was determined by manually drawing a region of interest along the border of the tumor on each consecutive slice covering the whole lesion while excluding intra - luminal air and calcification . 
a for the delineation of an intestinal stromal tumor ; b for the one slice area of the same intestinal stromal tumor ; c for the whole volume extracted from the same intestinal stromal tumor 1 3 468 la radiologia medica ( 2020 ) 125 : 465473 radiomics feature extraction andfeature selection quantitative radiomics feature extraction was conducted , as previously described [ 23 ]  . 
the radiomics features in this study contained 396 features , which included ( 1 ) 42 first - order statistics features , ( 2 ) nine shape and size features and ( 3 ) 345 texture features including 144 gray level cooccurence matrix ( glcm ) , 180 gray level run length matrix ( glrlm ) , 11 gray level size zone matrix ( glszm ) and ten haralick features . 
the features were extracted automatically using the ak radiomics analysis software ( a.k. ; ge healthcare , shanghai , china ) , similar as previous reports [ 24 , 25 ]  . after being centered and scaled , highly redundant and correlated features underwent a two - step feature selection procedure . 
each node in the decision trees is a condition on a single feature that is designed to split the dataset into two sets , to ensure similar response values are in the same set . 
 [ 26 ] proposed that at least 1015 times of events per predictor variable are required to generate reasonably stable estimates of the impact of the dependent variables for multivariate analysis . 
thus , in our study , the top five most important features , using gini impurity as the criterion , were selected as the final radiomics features . radiomics model building andvalidation the five selected radiomics features and corresponding labels ( e.g. , a binary label for predicting nonadvanced / advanced gists and encoded labels for predicting four types of risk ) were fed into two rf classifiers to build the prediction model . 
the final results , which included accuracy , sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) , were the average results across the three calculations used to quantify the performance of two models . 
the same indexes as in the primary cohorts were calculated for independent model evaluation . statistical method statistical analysis was performed using spss 22.0 software ( spss inc . , chicago , il , usa )  . 
t test was used to analyze continuous variables ( age ) and risk degree , while x2 test or fisher test was used to analyze the relational categorical variables ( site , sex ) and risk degree , where available . 
the first five important features calculated by rf ranking were runlenthnonuiformity_angle0_offset4 , runlenthnonuiformity_alldirection_offset1_sd , longrunlowgreylevelemphasis_angle0_offset1 , surface volume ratio and greylevelnouniformity_alldirection_offset4_sd . the importance of the remaining features calculated by rf ranking is presented in table5 . radiomics model performance p < 0.05 indicates that difference is statistically significant when determining whether the radiomics model could distinguish nonadvanced from advanced gists , as well as fig . 
the radiomics signature demonstrated favorable performance for the risk stratification of gists with an auc of 0.809 ( 95% ci 0.7770.841 ) and an accuracy of 67.5% for the validation cohort . 
the introduction of imatinib as an effective targeted therapy and the development of risk stratification for gists have changed the paradigm of gist treatments [ 9 , 29 ]  . 
however , variability in expertise in subjective assessments of mitotic count and ct findings , as well as the possibility of non - representative biopsy samples due to tumor heterogeneity , can be challenging and difficult to overcome [ 31 ]  . 
a possible remedy for this limitation is to identify tumors as vois and extract radiomics features from them for a more comprehensive analysis [ 24 , 32 , 33 ]  . 
 compared with local biopsy samples and two - dimensional features , the 3d volume ct - based radiomics signature contains more detailed information to avoid the influence of tumor heterogeneity [ 18 , 34 ]  . the stratification of patients based on the gist risk of recurrence is a key issue in managing primary gists [ 35 ]  . 
 the national comprehensive cancer network guidelines recommend adjuvant imatinib treatment of 3years for patients with a significant risk of recurrence ( i.e. , high - risk and intermediate - risk levels ) [ 36 ]  . 
however , patients , who have favorable outcomes after undergoing resection of verylow - risk or low - risk tumors , are likely to be cured by surgery alone and should not receive adjuvant imatinib [ 37 , 38 ]  . 
 thus , in the first portion of our study , we classified patients in the very - low - risk and low - risk stratifications of gists as having nonadvanced gists , and patients in the moderaterisk and high - risk stratifications as having advanced gists . 
because ct is usually used to examine gists preoperatively [ 29 ] , ctbased radiomics signature in distinguishing nonadvanced from advanced gists could have better popularization and application in clinical practice . 
wang [ 11 ] found that diagnostic accuracy of support vector machine diagnostic model , established with ten imaging features as indexes , was 70.0% , and it was especially reliable when diagnosing gists of high or low risk . 
tao chen reported that the generated radiomics model had an auc value of 0.867 [ 95% confidence interval ( ci ) 0.8030.932 ] in the primary cohort and 0.847 ( 95% ci 0.7650.930 ) in the external cohort for differentiating lowand high - malignant - potential gists [ 39 ]  . 
our results for the binary classification had an auc value of 0.935 ( 95% ci 0.8701.000 ) in the validated cohort , showing a good consistency with previous research , which strongly supports the potential of radiomics analysis in terms of diagnostic accuracy . 
 [ 40 ] reported that very - low - risk , low - risk and intermediate - risk gists generally had favorable and similar outcomes , whereas the high - risk category would be considered for adjuvant treatment . 
based on the perspective of clinical treatment and prognosis , clinicians are more concerned for patients with high - risk gists , because these patients require postoperative targeted drugs to prevent recurrences . 
ct - based radiomics analysis is important and necessary as a noninvasive complementary approach to provide a complete characterization of the tumor , especially in cases with incomplete tumor samples . 
radiomics analysis could also be conducted on existing images without additional cost , thus having the potential for a wider range of clinical applications . nevertheless , the current study had some limitations . 
 ( 1 ) we did not conduct a direct comparison between subjective ct features and pathological results , because it is possible for radiomics features of the whole volume tumor to represent the macroand micro - pathology . 
 ( 2 ) it was not determined whether the venous phase could be used to distinguish the four risk degrees of gists , and further studies are necessary to address this point . 
 ( 3 ) although the arterial phase provided a good visibility of the tumor , this phase may be more commonly influenced by the type , amount and flow injection of contrast agent during radiomics , which may limit the reproducibility of the results . 
 ( 4 ) there were only eight cases of tumors with very - low - risk degree , which might have produced bias in the assessment of the risk stratification of gists between the pathological diagnosis and the radiomics analysis . 
 ( 5 ) gene expression profiles are promising new methods for assessing the risk of gist recurrence and / or metastasis [ 42 ] , and further investigation is needed to better understand the potential mechanism . conclusion we hereby conclude that radiomics analysis can capture features of the four risk categories of gists . 
we therefore provide a ct - based radiomics signature to distinguish between nonadvanced and advanced gists , as well as the four risk stratifications of gists , with good diagnostic accuracy . 
the two ct protocols were applied using iterative reconstruction ( asir ) 40% but different noise indexes , recording dose - length product ( dlp ) and volume computed tomography dose index ( ctdivol )  . 
for each patient , two single cts , at enrollment ( group 1 ) and at follow - up after lowering the dose ( group 2 ) , were evaluated by two radiologists evaluating , for each examination , five different lung regions ( central zonecz ; peripheral zonepz ; sub - pleural regionspr ; centrilobular regionclr ; and apical zoneaz )  . 
however , disagreement was limited to a score 4 ( excellent ) - to - score 3 ( good ) iq transition ; apart from a single case in pz , both the observers scored the iq at follow - up as 2 ( sufficient ) starting from a score 4 ( excellent )  . conclusion dose reduction achieved in the follow - up ct scans , although a lower iq still allows a good diagnostic confidence . keywords chest computerized tomography iterative reconstruction image quality radiation dose introduction in the past decades , the average annual per capita effective dose from medicine has approximately doubled worldwide [ 14 ]  . computed tomography ( ct ) examinations are associated with absorbed doses much higher than conventional * pierluca piselli pierluca.piselli@inmi.it 1 radiology unit , national institute forinfectious diseases l . 
spallanzani irccs , via portuense 292 , 00149rome , italy radiology , and although they account approximately for 17% of the total number of medical radiation - based procedures , they contribute to 50% of the overall dose delivered to the population [ 57 ]  . although , in the past , the literature estimates that between 0.7 and 2% of new cancer cases in the usa each year can be attributed exclusively to ct scanning [ 8 , 9 ] , nowadays several studies stated that the risk is definitely lower and is needed to provide more robust analysis in defining the cancer risks potentially induced by ct scans [ 1013 ]  . therefore , it is understood that first of all ct studies must be performed tailoring examinations in an appropriate clinical setting , there is a remarkable technologic effort to decrease the radiation dose during justified ct scanning as low as reasonably achievable [ 1417 ] , and furthermore , we must keep in mind that some subjects often required vol . : ( 0123456789 ) 1 3 452 la radiologia medica ( 2020 ) 125 : 451460 short - term repeated ct examinations , increasing the total dose of radiation they are exposed to [ 18 , 19 ]  . centering the patient in the middle of the scanning area . 
no intravenous contrast was administered in both ct series . several controllable factors influence the radiation dose , and various dose - reduction strategies have been explored , but all these techniques are associated with degraded image quality due to the increased image noise . nowadays , iterative reconstruction ( ir ) represents a well - established tool , which allows an excellent level of dose reduction , preserving an image quality and decreasing the image noise [ 2022 ]  . 
accepting a higher ni of the reconstructed image results in lowering ma , therefore lowering the radiation dose . however , some authors warned against the risk that the ir techniques reliability in resolving the spatial resolution of low - contrast objects could be lost for radiation dose reduction in 25% or more [ 2325 ]  . many papers on ir of thoracic ct have been published ; however , to our knowledge , no studies have investigated the utility to increase the ni with further dose reduction , keeping the same ir percentage . in our study , we compared intra - individual subjective image quality and radiation dose used for two consecutive thoracic cts , performed in patients with lung infection diseases using the same ir percentage , and higher ni at the follow - up examinations . materials andmethods participant recruitment andsampling from june 2015 to february 2018 , 59 consecutive adult patients underwent clinically indicated non - enhanced chest ct because of pulmonary infection , and they repeated a second clinically justified chest ct performed either for evaluating the lung involvement after the therapy or for further evaluations of the previous disease or for other complications . 
patients were excluded if they met any one of the following conditions : age below 20years , pregnant , inability to suspend respiration during ct , previous thoracic surgery , and a metal device in the thorax . 
ctdivol is an estimate of average x - ray tube output , and dlp is the total x - ray output integrated throughout the entire scan , obtained by multiplying ctdivol by the scanned length in centimeters of the patient . 
the estimated ct dose was expressed in milligrays ( mgy ) and dlp expressed in milligrays - centimeters ( mgy / cm )  . ctdivol and dlp were recorded for all the patients following the completion of the examination according to the dose report , automatically generated by ct . 
reviewers were unaware of 1 3 la radiologia medica ( 2020 ) 125 : 451460 any medical notices of the patients and image acquisition technique . all data sets were reviewed with lung window settings ( window width = 1800 hu , window center = 450hu )  . 
 according to other authors [ 2125 ] , lung was divided into five regions : central zone ( cz ) , including the main and segment bronchi within 20 mm of hila ; peripheral lung zone ( pz ) , within 2040 mm of hila including small bronchi and bronchioles ; sub - pleural region ( spr ) , within 10 mm of the chest wall ; centrilobular region ( clr ) ; and apical zone ( az )  . the subjective image quality ( iq ) was individually assessed in all patients on the basis of the distinction of anatomic details such as sub - segmental bronchi wall thickness and vessel margins , peripheral bronchi wall thickness and vessel margins , image noise , artifacts , and diagnostic quality using a 4 - point likert scale , based on the european guidelines on quality criteria for ct defined for assessing iq as follows [ 27 ] : 1 . 
excellent : excellent image quality , distinct anatomic details , no / minimal image noise or artifacts , full diagnostic confidence . statistical analysis the goal of our analysis was to provide estimates of the change in reviewer scores for the follow - up ct dose . 
this method called visual grading characteristic ( vgc ) analysis simply allows to assess the difference in image quality between two modalities [ 30 ] and was extensively used in the radiology field to compare iq obtained using different protocols of ir [ 31 , 32 ]  . 
for the two methods , the image criteria score ( ics ) was calculated , corresponding to the proportion of images from a specific method for which the criterion is fulfilled . a continuous vgc curve based on the binormal assumption of the image quality distributions can be obtained , by plotting the cumulative distributions of the rating data for two compared systems against each other . 
in our case , we compared ics corresponding to the follow - up low - dose scan ( low dose ) system versus the ics corresponding to the baseline higher - dose scan ( high dose )  . the vgc curve can be analyzed in a manner similar to that used in receiver operating characteristic ( roc ) analysis [ 33 ]  . 
a p value less than 0.05 was considered statistically significant . results among the fifty - nine patients , thirty - three subjects were men ; median age was 46years ( interquartile range , iqr 28 56years )  . 
1 distribution of volume ct dose index ( ctdivol ) ( upper panel ) and dose - length product ( dlp ) ( lower panel ) recorded in the baseline enrollment ct scans using high - dosage protocol ( ctdivol high and dlp high , respectively ) and in the follow - up ct scans using low - dosage protocol ( ctdivol low and dlp low , respectively )  . 
this can be achieved using patients weight , diameter measurements , body mass index , or just as a qualitative visual classification . because these methods provide very approximate x - ray attenuation estimates and do not take into account for attenuation changes within the patient region being scanned , the technologist must use a margin of technique high enough to avoid the possibility of compromising the diagnostic quality of images with too much noise . this effect is partly due to limitations in the current standard reconstruction method of fbp . 
fbp is an algorithm based on simpler mathematical assumptions of the tomographic imaging system and reconstructs images data at a slice thickness of 0.625mm , with a lung convolution kernel . 
2 examples of chest ct with images of normal pulmonary structures and scoring of image quality graded on 4 - point scale , comparing those obtained using a standard high - dose protocol with low noise index ( ni ) ( left ) and low - dose protocol with high ni ( right )  . 
cd ( central , peripheral , sub - pleural zones ) : c image quality score of 4 ( excellent image quality without any artifact ) , d image quality score of 4 1 3 456 la radiologia medica ( 2020 ) 125 : 451460 fig . 
3 examples of chest ct with images of normal pulmonary structures of the apical zone and scoring of image quality graded on 4 - point scale , comparing those obtained using a standard high - dose protocol with low noise index ( ni ) ( left ) and low - dose protocol with high ni ( right )  . 
however , due to the approximate nature of fbp reconstruction , there is a deviation between measured and calculated projections that directly correlates increased spatial resolution with increased image noise , even partially amended by the application of different reconstruction kernels [ 7 , 1416 ]  . for chest ct , a mild increase in noise may not limit diagnostic accuracy , because the air in the lung generates more contrast than it is associated with solid organs , and therefore , the detection of pathological changes in the lung is less dependent on image noise caused by a low radiation dose than in solid organs . nowadays , an alternative mathematic algorithm , ir , was introduced to ct , and many studies have confirmed the capability of ir to obtain an optimal image quality in lowdose ct examinations , above all in chest ct [ 17 , 2022 ]  . unlike traditional filtered back projection ( fbp ) technique , ir is based on a correction loop within the image generation process , which leads to significant reduction in noise with the maintenance of image resolution . 
there are different algorithms for ir . asir is a hybrid algorithm , blending with fbp images , that generates a set of synthesized projections by modeling the data collection process , such as the statistical system information ( including photon statistics and electronic acquisition noise ) , without modeling of the system optics . the ni is a parameter that corresponds to the relative noise in the reconstructed images , and the amount of this noise is selected . 
the ni value will be approximately equal to the standard deviation in the central region of the image when a 1 3 la radiologia medica ( 2020 ) 125 : 451460 uniform phantom ( with the patients attenuation characteristics ) is scanned and reconstructed . a higher ni means the images contain more noise but had been achieved with lower ma ( kv is not altered ) and therefore with lower dose . 
a lower ni means the images contain less noise , but had be obtained with higher ma and therefore with higher dose . however , many artifacts could be significantly associated with a coarse image appearance with disadvantages in the depiction of the most subtle anatomical details and pathologies [ 2325 ]  . in our study , we compared subjective iq and radiation dose used for two consecutive thoracic cts in the same patient considering two different radiation doses . 
an agreement between the two observers evaluating group 1 ( high dose ) cts was perfect ; however , the agreement ranged from moderate to good in group 2 ( low dose ) examinations . 
however , in our study , even for the zones which resulted to be categorized with a lower score , the artifacts have not determined the images with reduced ( score , 2 ) or poor ( score , 1 ) quality neither in the group 2 scans ( apart from a single case ) , resulting in an overall comparable iq between the baseline and the follow - up chest cts . 
considering the comparison among same patient group 1 and group 2 cts , for both observers the disagreement was limited to a score 4 ( excellent ) to score 3 ( good )  . however , it is mandatory that the detection and characterization of normal and pathological features should not be compromised in the pursuit of reduced radiation dose levels and the diagnostic performances maintained . in our study , according to the alara principle , the increased ni produced a significant radiation dose reduction for chest cts performing with asir . 
no statistically significant differences in terms of finding a detection and distribution were evident among the two ct protocols for any category of anatomical details . moreover , the reduction in dose increasing ni in chest cts is not necessary to have a new performant ct with new - generation adaptive statistical iterative reconstruction ( asir - v ) [ 35 ] , but also older scanner equipped with asir can reach easily this important objective [ 36 ]  . this is a very important result for reducing the irradiation of the population that more and more frequently is subjected to cts and in particular for a large number of patients that undergo chest cts for infectious diseases . this study was limited in several in some aspects . 
considering pneumonia patterns in follow - up evolution and presuming that if the ct performed with reduced dose is able to identify normal anatomical signs , even small and subtle , it will be able to evaluate the pathological ones too ; we preferred to avoid losing any difference in comparison of the two chest ct groups . 
second , we used subjective criteria as measure of acceptable iq . conclusions in conclusion , all the cts with asir increasing ni can perform unenhanced chest ct using a very low radiation dose , still maintaining a good iq and not influencing a good diagnostic accuracy . transferring our results to the clinical routine , it would produce a significant radiation dose reduction and might be used routinely for the early monitoring of pneumonias . 
this is extremely important in some patients cohort , such as young women or patients who need repetitive ct examinations , where the advantage of lowering radiation dose does not impair diagnostic performance . 1 3 458 la radiologia medica ( 2020 ) 125 : 451460 1 3 la radiologia medica ( 2020 ) 125 : 451460 fig . 
4 visual grading characteristic ( vgc ) analysis curves ( black curves ) in which the image criteria score ( ics ) data of the highdose baseline scan ( icshigh ) are plotted against those of the low - dose follow - up scan ( icslow )  . 
vgc curves are shown for all five regions of the lung considered : a central zone ( cz ) , including the main and segment bronchi within 20mm of hila ; b peripheral lung zone ( pz ) , within 2040 mm of hila including small bronchi and bronchioles ; c sub - pleural region ( spr ) , within 10 mm of the chest wall ; d centrilobular region ( clr ) ; and e apical zone ( az )  . 
italian radiology departments found themselves at the forefront in the management of suspected and positive covid cases , both in diagnosis , in estimating the severity of the disease and in follow - up . 
in this context sirm recommends chest x - ray as first - line imaging tool , ct as additional tool that shows typical features of covid pneumonia , and ultrasound of the lungs as monitoring tool . 
in this emergency situation , several expectations have been raised by the scientific community about the role that artificial intelligence can have in improving the diagnosis and treatment of coronavirus infection , and sirm wishes to deliver clear statements to the radiological community , on the usefulness of artificial intelligence as a radiological decision support system in covid - 19 positive patients . 
 ( 1 ) sirm supports the research on the use of artificial intelligence as a predictive and prognostic decision support system , especially in hospitalized patients and those admitted to intensive care , and welcomes single center of multicenter studies for a clinical validation of the test . 
 ( 3 ) chest ct with artificial intelligence cannot replace molecular diagnosis tests with nose - pharyngeal swab ( rrt - pcr ) in suspected for covid - 19 patients . keywords artificial intellingence ethics covid - 19 imaging computed tomography introduction the novel coronavirus ( sars - cov - 2 ) infection outbreak , rapidly spreading from wuhan city ( hubei province , china ) to extra continental countries since december 2019 , has * emanuele neri emanuele.neri@med.unipi.it 1 department oftranslational research , diagnostic radiology 3 , university ofpisa , pisa , italy 2 department ofradiology , careggi university hospital , florence , italy 3 malpighi radiology unit , department ofdiagnostic andpreventive medicine , santorsola malpighi university hospital , bologna , italy 4 department ofclinical andexperimental medicine , f . 
lanzara , university ofcampania luigi vanvitelli , naples , italy been declared pandemic by the world health organization ( who ) on march 2020 [ 1 ]  . to date , the number of covid - 19 ( coronavirus disease 2019 ) confirmed cases is constantly growing , with a death rate of 7% . 
they conclude that chest ct has a high sensitivity for diagnosis ofcovid - 19 and may be considered as a primary tool for the currentcovid - 19 detection in epidemic areas [ 4 ]  . 
using ct in screening and / or asymptomatic patients , the probability to find radiological signs of covid - 19 infection is low and therefore the use of ct would lead to many negative tests ( even in patients with rrt - pcr positive tests ) , thus increasing the workload of the radiology departments and the risk of transmission of the infection . in a study of bai etal . , in which of 213 ct examinations of positive covid patients have been retrospectively reviewed by 3 chinese and 4 us radiologists , they distinguishedcovid - 19 from viral pneumonia onchestctwith high specificity but moderate sensitivity . 
another study by li y and xia l , on 53 cases , concluded that chestcthad a low rate of missed diagnosis ofcovid - 19 ( 3.9% , 2 / 51 ) and may be useful as a standard method for the rapid diagnosis ofcovid - 19 to optimize the management of patients . 
 however , ctis still limited for identifying specific viruses and distinguishing between viruses [ 5 ]  . while ct has low specificity for identifying covid - 19 lung infection , a recent study by yuan etal . 
in agreement with the italian association of ultrasonography in medicine and biology , and the italian association of scientific medical societies , sirm recommends : chest x - ray as first - line imaging tool that allows a first assessment of patients , especially in the emergency room , and can direct the differential diagnosis toward other possible causes of pulmonary parenchymal involvement , other than covid - 19 infection [ 8 ]  . ct as additional tool that shows typical features of covid pneumonia , as the most common bilateral ground - glass opacities involving mainly the lower lobes [ 9 ]  . ultrasound of the lungs as monitoring tool also to evaluate the effectiveness of prone - supination maneuvers [ 10 , 11 ]  . sirm recommends , as high priority , to ensure appropriatesanitation procedures on the scan equipmentafter detecting any suspected or positive covid - 19 patients , since the risk of spreading the infection into the ct suite . sirm recommendations ontheuse ofartificial intelligence incovid19 as diagnostic imaging is an ecosystem of digital data , which is collected for each patient who undergoes any radiographic , computed tomography , magnetic resonance , ultrasound , and all nuclear medicine investigation , so much data , or big data , need an accurate interpretation related to the clinical problem for which the patient undergoes the investigation ; this is the task of the radiologist , through the radiological medical act , that is summarized in the radiological report . 
in this context , artificial intelligence is a promising technology that allows to process so big data and extract meaningful information [ 1214 ]  . in a paper about the role of artificial intelligence in covid pandemic , santosh kc etal . 
chest ct with artificial intelligence cannot replace molecular diagnosis tests with nose - pharyngeal swab ( rt - pcr ) or in suspected for covid - 19 patients ; conclusions few data are available about the role of artificial intelligence as a radiological decision support system in covid19 patients ; it is too early to apply this technology in clinical practice as first - line modality . 
there are in fact many ethical and medico - legal implications in the use of this technology that , even in this emergency situation , do not allow its routine use [ 2325 ]  . 
the multivariate of the technological solutions available both in the research centers and on the market poses serious questions on the variability of the results that can be generated by the software . 
salvage ebrt to the residual prostate was performed with moderate hypofractionation schedule ( mhrt ) in 28 fractions ( n = 16 ) or with extreme hypofractionation schedule ( sbrt ) in 5 fractions ( n = 8 ) by means of image - guided volumetric modulation arc therapy . 
complete local control of disease was achieved in 23 / 24 patients ( 96% )  . conclusions our data confirm the feasibility and the low toxicity of salvage ebrt with both schedules of treatment after hifu failure . 
hifu has the capability to create a tissue ablation * michele rigo michele.rigo@sacrocuore.it 1 advanced radiation oncology department , cancer care center , irccs sacro cuore don calabria hospital , via don sempreboni 5 , 37034verona , negrar , italy 2 radiation oncology department , university ofbrescia , brescia , italy 3 columbus clinic center , milan , italy by means of intense ultrasound waves with focused heating of the targeted tissues . 
hifu has been originally proposed for prostate gland benign diseases ; subsequently , it was rapidly introduced as a noninvasive option for pc with definitive or salvage intent [ 2 ]  . 
according to available clinical data , hifu is associated with a low incidence of urinary incontinence and allows the preservation of sexual activity when proposed as primary treatment option [ 37 ]  . 
nevertheless , hifu indication as definitive primary treatment for prostate cancer remains object of debate and several guidelines consider this approach experimental and recommend to propose hifu only inside study protocols [ 8 ]  . 
although hifu could be considered a promising approach for prostate cancer , in strictly selected cases , the biochemical failure rates and disease - free survival are lower when compared to radical radiotherapy [ 9 ]  . 
moreover , substantial uncertainties remain concerning the monitoring post - hifu and the vol . : ( 0123456789 ) 1 3 492 la radiologia medica ( 2020 ) 125 : 491499 re - treatment criteria or therapeutic options . 
of these , twenty - one patients underwent a single session of hifu , whereas three patients were treated by means of two hifu courses to both prostatic lobes . radiotherapy procedures a contrast - free computed tomography ( ct ) scan with 3mm slice thickness from l2 to 10cm below the level of ischiatic lower bone margin was acquired for the simulation of all patients . 
daily specific preparation was requested : comfortably full bladder ( drinking 500ml of water 30min before every treatment session ) and empty rectupatients were submitted to planning ct in the treatment position : supine , arms on chest , with combifix frame ( civco , orange city , ia , usa )  . 
three permanent tattoos were marked on the skin at the time of planning ct scan . the gross tumor volume ( gtv ) encompassed the prostate or the prostate plus seminal vesicles for patients with one or more risk factor ( initial psa > 10 , gleason 7 , > t2a )  . 
oars planning objectives were as follows : ( 1 ) in case of mhrt for rectum v50 gy < 45% , v60gy < 30% , v65gy < 20% ; for bladder v60gy < 35% ; for femoral heads d1cm3 < 45gy ; for intestinal cavity v20gy < 40% , dmean < 20gy and dmax < 48gy ; ( 2 ) in case of sbrt for rectum v18gy < 50% , v28gy < 20% , v32gy < 10% , v35gy < 5% , dmax < 36gy ; for bladder v37 gy < 10% , v35 gy < 50% ; for femoral heads v25gy < 25% . treatments were performed with volumetric modulated arc therapy ( vmat ) and were delivered using truebeam linac ( varian medical system , palo alto , ca , usa )  . 
follow - up visits were scheduled at regular intervals every 3months after the end of the treatment in order to evaluate the psa trend and acute and late symptoms . clinical endpoints primary endpoint of the present study was treatment - related toxicity . 
secondary endpoints were biochemical disease - free survival ( according to astro phoenix definition ) and local control . results hifu patient characteristics at initial diagnosis by biopsy , the gleason score was 3 + 3 in 16 patients , 3 + 4 in 6 patients , 4 + 3 in one patient and 4 + 5 in another one . 
prior to hifu , all patients were staged with bone scintigraphy and ct scan and no distant metastases were detected . all patients completed hifu without adverse events but experienced biochemical failure based on stuttgard definition . 
so they were referred in our institute at advanced radiation oncology department and discussed in our multidisciplinary genitourinary tumor board ( mtb ) for choosing the most appropriate diagnostic restaging examination in order to assess the recurrence sites : 19 patients were submitted to 11c choline pet / ct , 4 patients to gallium68psma - 11 ( hbed - cc ) - pet / ct and one to pelvic mri and bone scintigraphy . 
the median psa value before salvage ebrt was 4.6ng / ml ( range 1.1227.86ng / ml ) , and the median interval between hifu and ebrt was 39months ( range 3136months )  . salvage ebrt was performed with moderate hypofractionation schedule ( mhrt ) in 28 fractions ( n = 16 ) or with extreme hypofractionation schedule ( sbrt ) in 5 fractions ( n = 8 )  . 
due to the absence of evidence on the most appropriate radiation dose fractionation in case of local relapse after hifu , the two different treatment schedules were both illustrated and proposed and the decision was made based on patients preference . 
only five patients ( 21% ) had additional androgen deprivation therapy ( adt ) during ebrt treatment ( four in mhrt cohort and one in sbrt cohort )  . no major radiation - related gi and gu toxicity was recorded for both schedules of hypofractionated ebrt , and no differences were observed between the two groups in terms of acute toxicity . 
all patients experienced a psa value drop after ebrt : the median psa nadir was 0.26ng / ml ( range 0.0112.05ng / ml ) , and it was reached in a median time of 17months . 
after salvage ebrt , all patients were submitted to restaging pet - ct that showed metabolic response on residual prostatic gland in 23 / 24 patients ( 96% overall local control )  . 
the median psa value before mhrt was 4.29ng / ml ( range 227.86ng / ml ) , and the median interval between hifu and mhrt was 39months ( range 3120months )  . 
at the time of follow - up , a complete local control of disease was achieved in 15 / 16 patients ( 94% ) : during follow - up , only one patient experienced a local failure after 2years from ebrt documented by psa rising and 11c choline pet - ct . 
1 kaplanmeier curve showing biochemical relapsefree survival after ebrt biochemical non - evidence of disease biochemical non - evidence of disease biochemical non - evidence of disease biochemical non - evidence of disease biochemical non - evidence of disease biochemical non - evidence of disease follow - up . 
eight ( 50% ) of patients experienced acute grade 1 gu toxicities such as mild dysuria , urinary frequency or urgency . all patients recovered from this acute toxicity in the weeks following the treatment , and no late toxicities were recorded . 
no one suffered erectile or voiding dysfunction ( i.e. , urinary obstruction or incontinence , stricture )  . sbrt patient characteristics the median age of this cohort of patients was 68years old ( range 6481 )  . 
the median psa value before sbrt was 5.16 ng / ml ( range 1.9714.36 ng / ml ) , and the median interval between hifu and sbrt was 54months ( range 8136months )  . 
the median psa nadir 1 3 496 la radiologia medica ( 2020 ) 125 : 491499 was 0.64ng / ml ( range 0.1212.05ng / ml ) and occurred within a median time of 8months ( range 327months )  . 
at the time of follow - up , a complete local control of disease was achieved in all patients ( 100% )  . two patients ( 25% ) experienced biochemical failure three and six months after treatment , respectively . 
in both of cases , a restaging with 11c choline pet - ct was performed and the examinations showed a pathologic lymph node not previously treated and sbrt on pet - positive node and adt was performed . 
four ( 50% ) of patients experienced acute grade 1 gu toxicities , all the previous patients recovered from this acute toxicity in the weeks following the treatment , and no late toxicities were assessed . 
toxicities are reported in table2 . discussion although hifu is still considered experimental in several guidelines [ 8 ] , in strictly selected patients affected by localized prostate cancer , this local approach could represent a potential alternative to the well - recognized standard treatment options . 
however , post - interventional changes of the tissue , such as edema or hemorrhage , can affect tumor detection on mpmri [ 26 ]  . during these last years , the role of molecular imaging has become outstanding in the management of prostate cancer by means of new tracers introduced in clinical practice , including choline and psma . 
these novel positron emission tomography ( pet ) tracers allow to detect post - hifu local recurrences with high rates of sensitivity and specificity , as reported in some series [ 27 ]  . in this context , local recurrences can be treated by a second course of hifu ablation or by radiation therapy [ 28 ]  . in the present article , we report our experience concerning salvage high - dose ebrt guided by molecular imaging . 
the great improvement of radiotherapy techniques with daily image guidance such as cone beam ct allows to deliver radiation with very high accuracy reducing margins and allowing the reduction in irradiated healthy tissue , while reducing toxicity risk . 
better understanding of radiobiology and in particular of the biology of radiation high doses allowed to assess that prostate cancer is particularly sensitive to high radiation doses ( low alpha / beta ratio ) , which are even lower than surrounding late responding healthy organs [ 1019 ]  . 
more specifically , in radical setting , various randomized studies have reported robust data of tolerability and effectiveness , in regard to the adoption of moderate hypofractionated schedule of fractionation when compared to conventional approach [ 1019 ]  . 
although derived from non - randomized trials , comparable data emerged in the last 10years about the clinical application of extreme hypofractionation for lowand intermediate - risk prostate cancer , demonstrating optimal results concerning biochemical control and tolerability [ 1619 , 29 , 30 ] , frequently similar to conventional and moderate hypofractionation schedules [ 14 ]  . moderate hypofractionation and extreme hypofractionation , already successfully applied in our department [ 1519 ] , were both considered for the present post - hifu patients series . 
due to the absence of evidence on the most appropriate radiation dose fractionation in case of local relapse after hifu , the two different treatment schedules were both illustrated and proposed . 
thus , the decision was made based on patient preference . although the present series is relatively small and heterogeneous , to the best of our knowledge , this is the first study , in the literature , reporting clinical outcomes by two different ebrt regimens with salvage intent : moderate and extreme hypofractionation post - hifu failure . 
four ( 50% ) of patients experienced acute grade 1 gu toxicities , all the previous patients recovered from this acute toxicity in the weeks following the treatment , and no late toxicities were assessed . 
 [ 28 ] , the patients underwent standard fractionation conformal radiotherapy with a median dose of 72gy with salvage intent post - hifu local relapse detected by positive biopsy and the absence of extraprostatic disease on magnetic resonance imaging ( mri ) , thoracic - abdominal computed tomography ( ct ) and ct bone scan . 
about one half of the patients had minor side effects and the rates observed were equivalent to those observed in many series of radiotherapy alone , with a rate of grade 1 and 2 urinary complications of 230% , a rate of grade 3 complications of less than 5% and very rare grade 4 complications . 
gastrointestinal grade 4 complications might be slightly more frequent than grade 4 urinary complications at 0.11%. a retrospective study by alongi and colleagues [ 2 ] analyzing 15 patients with salvage ebrt confirmed the feasibility and very low acute morbidity of pet - choline - guided moderate hypofractionated ebrt . 
more deeply , in this last experience , acute gu grade 1 and grade 2 toxicities were recorded in 7 / 15 and 4 / 15 patients , respectively , and rectal acute grade 1 and grade 2 toxicities in 3 / 15 and 2 / 15 , respectively . 
summary of the studies available in the literature is shown in table3 . conclusion our data confirm feasibility and low toxicity of salvage ebrt with both schedules of treatment after hifu failure . 
ai software must be useful categorizing the disease into different severities , integrating the structured report , prepared according to subjective considerations , with quantitative , objective assessments of the extent of the lesions . 
in the post - processing phase , software , thanks to the help of a colorimetric map , recognizes the ground glass and differentiates it from consolidation and quantifies them as a percentage with respect to the healthy parenchyma . 
therefore , keeping in mind that ct has high diagnostic sensitivity in identifying lesions , but not specific for covid - 19 and similar to other infectious viral diseases , it is mandatory to have an ai software that expresses objective evaluations of the percentage of ventilated lung parenchyma compared to the affected one . keywords sars - cov - 2 artificial intelligence structured report introduction the world health organization ( who ) on march 11 , 2020 , has communicated the novel coronavirus ( covid - 19 ) outbreak a global pandemic . 
although * alfonso reginelli alfonso.reginelli@hotmail.com 1 department ofprecision medicine , university ofcampania luigi vanvitelli , 80138naples , italy 2 radiology department , asst bolognini hospital , bergamoest , italy containment measures in china have reduced all new cases , this reduction has not occurred elsewhere and italy has been particularly hard hit . 
there is now serious concern regarding the ability of the italian national health system to respond effectively to the needs of infected patients requiring intensive care for covid - 19 pneumonia . 
the percentage of intensive care unit ( icu ) patients reported daily in italy between march 1 and march 11 , 2020 , was constantly between 9 and 11% of the patients infected . 
since february 21 , in italy the number of patients infected closely follows an exponential trend [ 3 , 4 ] and covid - 19 diagnosis is performed by detecting pathogenic samples and traces of the specific immune response by means of a saliva sample in symptomatic patients . 
currently , the screening work is passive and is mainly based on symptoms , but unfortunately as the number of asymptomatic patients increases , prevention and control of the epidemic become vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 500504 even more difficult . 
hrct is the most accurate technique in identifying pathognomic findings of interstitial pneumonia as ground glass areas , crazy paving , nodules and consolidations , monoor bilateral , patchy or multifocal , central and / or peripheral distribution , declivous or nondeclivous [ 711 ]  . 
ct is widely used , has rapid acquisition speed and high sensitivity , which has led to a large number of patients referred to imaging and the number of confirmed patients whose evolution must be followed . 
 however , after examination , disinfection of ct room is mandatory and wait on average 20min , time necessary for the exchange of air to secure the equipment and the environments . 
unfortunately , covid - 19 patients have similar imaging characteristics as interstitial pneumonia caused by other viruses and ai software programs are not able to differentiate covid - 19 from other viral pneumonias . 
furthermore , common to all big data - based applications , all deep learning methods have lack of transparency and interpretability and it is impossible to determine what imaging features are being used to determine the output . however , advantages of software are automated measurements of wall thickness for intuitive airway analysis , lobe segmentation and visualization . 
beside clinical procedures and treatments , ai promises a new paradigm for health care , with different tools that are built upon machine learning ( ml ) algorithms and support the decision - making processes . 
ai software must be useful categorizing the disease into different severities , integrating the structured report [ 14 ] , prepared according to subjective considerations , with quantitative , objective assessments of the extent of the lesions . in this communication , we present an example of a good tool for the radiologist ( thoracic vcar software , ge healthcare , italy ) in covid - 19 diagnosis [ 1 ]  . 
in the post - processing phase , software , thanks to the help of a colorimetric map , recognizes the ground glass and differentiates it from consolidation and quantifies them as a percentage with respect to the healthy parenchyma . 
this objective information is useful for evaluating regression or progression disease in response to drug therapy as well as evaluating the effectiveness of pronation maneuvers for alveolar recruitment in icu patients . 
on the basis of the scientific evidence acquired so far , it is also intended to underline that , considering the nonspecificity of hrct patterns of covid - 19 pneumonia that do not allow to express a diagnostic judgment of certainty , the chest hrct examination cannot be considered a substitute for the rtpcr test in the diagnosis of covid - 19 nor used as a means of clinical screening , but it represents a good support [ 15 ]  . conclusion therefore , keeping in mind that ct has high diagnostic sensitivity in identifying lesions , but not specific for covid - 19 and similar to other infectious viral diseases , it is mandatory to have an ai software that expresses objective evaluations of the percentage of ventilated lung parenchyma compared to the affected one . 1 3 502 la radiologia medica ( 2020 ) 125 : 500504 fig . 
1 example of lung analysis in a patient covid - 19 with the thoracic vcar software in axial ( a ) and sagittal ( b ) planes 1 3 la radiologia medica ( 2020 ) 125 : 500504 fig . 
therefore , in order to reduce inappropriate investigations , the findings of the present study suggest that the reduction in overprescription could be reached through the improvement of training of health personnel and the propagation of a no - blame culture aimed at minimizing defensive medicine . keywords clinical risk management inappropriate investigations ct overprescription defensive medicine guidelines indication introduction in recent years , an exponential growth of health services request was assessed , due to programs that aim to empower the utilization of quality health services [ 1 ]  . 
on the one hand , such growth if it is due to advances in imaging technology , on the * davide ferorelli davideferorelli@gmail.com interdisciplinary department ofmedicine , section oflegal medicine , university ofbari , general hospital , bari , italy 2 department ofbasic medical science , neuroscience andsensory organs , orthopaedics unit , university ofbari , general hospital , bari , italy 3 neuroradiology unit , bari general hospital , bari , italy 4 emergency room unit , bari general hospital , bari , italy 5 policlinico di bari hospital , university ofbari , piazza g . 
cesare 11 , 70124bari , italy other it is influenced by the development of defensive medicine , in which the practice is motivated by legal rather than medical reasons [ 3 ]  . 
overuse of diagnostic imaging can also represent a potential risk to patient health because of long - term morbidity in terms of radiation hazards [ 5 ]  . so , the quest of a balance between the provision of performance and patient health should be an important aim of healthcare policy and management based as much as possible on the prescription appropriateness . the aim of this study was to quantify overprescription and its causes through evaluation of computer tomography ( ct ) scan prescriptions in patients with head injuries referred to an emergency department . 
hospital episode statistics data indicate that there are more than 110 , 000 admissions to hospitals in england with a primary vol . : ( 0123456789 ) 1 3 596 la radiologia medica ( 2020 ) 125 : 595599 diagnosis of head injury every year . 
there are no reliable up - to - date figures for the total denominator of attenders with a head injury at emergency departments , but a figure of one million emergency department attenders for the united kingdom as a whole is often quoted , but this is based on figures from not very recent [ 7 ]  . 
 recent recommendations of the scottish intercollegiate guidelines network centre define the identification of patients with a high risk of intracranial complications using the gcs ( glasgow coma scale ) , the presence of a skull fracture and various other clinical variables . 
these high - risk patients are recommended for ct scanning , while the admission for observation was considered a tool for patients with a medium risk of intracranial complications [ 9 ]  . neurosurgeons supported an enhanced role for ct imaging after head injury since 1990 and 1998 [ 10 ]  . 
different statements recommended a more liberal ct scanning policy , while they still adhering to the skull x - ray as the first - line investigation in the majority of minor / mild head injuries [ 11 ]  . this change in emphasis is reflected in an observed increase in ct scanning . 
this move to ct reflects a general consensus that earlier definitive imaging is associated with improved outcomes [ 13 ]  . about the prescription appropriateness , the italian society of medical radiology ( sirm ) joined the choosing wisely italy project ( brought into the choosing wisely international campaign during the amsterdam meeting , june 2014 ) [ 14 ] and listed five processes with high risk of inappropriateness based on the italys slow medicine indications [ 15 ]  . 
the fifth point recommends no routine skull x - ray in minor head injury , whereas the ct is recommended for lesions detection even if immediate the ct is not indicated in patients with gcs of 15 , no risk factors , and no other symptoms except pain at the point of impact . cultural education and operational planning play a central role : it is essential to bring a no - blame culture and develop a structured clinical governance by directly involving health professionals and empowering them in awareness that the most common reason for an inappropriate ct investigation was the inability to affect patient management [ 16 ]  . so , the purpose of our study was not to limit free medical choice , but to support it through an update of knowledge in diagnostic imaging as it has been done in other clinical fields also through internet - based survey [ 17 ]  . the aim of this study is to quantify the rate and investigate the causes of head ct scan over prescription in an emergency department , trying to reduce inappropriate prescriptions . 
these criteria were based on a virtuous management of resources , a better quality of patient care , and in accordance with the principle of equity . the study was divided into two phases , and it involved patients that accessed to the emergency department . 
in italy , patients that accessed to medical care at emergency rooms are treated based on their triage level : non - urgent , moderately critical code , and very critical code [ 18 ]  . phase 1 measurement of the prescription appropriateness . thanks to the cooperation between the clinical risk management unit and the neuroradiology unit , a set of 100 requests of ct scans was collected on a random basis through the access to the emergency department database over a period of 5months , from february to june 2017 . 
 for each request , the following parameter was considered : age ( excluding paediatric patients because of different clinical indications ) , sex ( both male and female ) , hospital priority code , reason of access to emergency care ( head trauma , polytrauma ; neurological disorders , headache , syncope , coma , other ) , risk factors , the time spent in the emergency department , discharge procedure ( home / hospitalization ) , and prognosis . 
then , a cd copy was made for each ct scan . the head ct requests were analysed by three experts in guidelines and scientific evidences on head ct prescription in an emergency department . 
expertsa neurologist , a radiologist , and an anaesthesiologistevaluated the prescription appropriateness of head ct scan in head injury without environmental pressures and without the risk of an overprescription due to defensive medicine . 
the nice guidelines of 2017 published by the national institute for health and care excellence were selected , as the more recent and reliable in immediate head ct prescription . this first phase aimed to analyse prescription appropriateness of this exam and the impact of the overprescription on resource use . phase 2 evaluation of the impact on patients . the three experts assessed the incidence and the number of lesions in the analysed exams , quantifying false negatives and false positives and evaluating the presence of lesions in exams supposed as inappropriate and vice versa . all the evaluations were reported on the office excel form for data collection . 
causes of access to the emergency department were head trauma ( 39% ) , neurological disorders ( 26% ) , other ( 10% ) , headache ( 8% ) , polytrauma ( 7% ) , coma ( 6% ) , and syncope ( 4% )  . 
the majority was accepted by the emergency department with a moderately critical code ( 68% ) , followed by a very critical code ( 20% ) , and a not critical / not very critical code ( 12% )  . 
the indication for ct was demanded in the guidelines in 68.0% of the cases ( n = 68 ) , and the indication was confirmed by the experts in guidelines in 94.0% of the cases ( n = 94 )  . 
some medical specialities are at high - risk for legal argument , but no reliable data are actually available for quantification of ct scan over prescription in italy . the sample was composed of 100 subjects with an average age of 61.3 : this is important for the patient management in the emergency department as the age - related risk factors . 68% of patients were accepted by the emergency department with a moderately critical code and 20% with a very critical code . 
in fact , results demonstrated that 32% of ct scans were not appropriate according to the guidelines and 1 in 32 represented a false negative ( a ct scan not appropriate , but with the evidence of an encephalic lesion )  . 
 1 3 598 la radiologia medica ( 2020 ) 125 : 595599 it is relevant not only for radiological protection but also for ethical issue and professional responsibility [ 21 , 22 ]  . our study demonstrated that this phenomenon is due not only to defensive medicine , as after experts re - evaluation in 94% nevertheless ct scans were indicated . the findings of the present study suggest that overprescription is determined by two main factors : defensive medicine in 6% of cases ( 94% of prescription was confirmed by the experts control ) and failure of guideline adherence in 32% ( 68% of prescription was confirmed by the most up - todate guidelines ) furthermore , it was found that ct scans indications for head trauma ( 39% of our sample ) are more adherent to the 2006 italian guidelines than to the most recent nice 2014 . so , an appropriate training of health personnel is necessary both to prevent patient exposure to unnecessary ionizing radiations and for an optimal allocation of public resources , as to limit wastefulness in health system as much as possible . conclusion appropriateness , quality , safety , fairness , user participation through interpersonal communication [ 23 ] , and efficiency represent the main quality indicators of italian national health service . 
clinical governance aims to achieve the best possible result in health care , through the research of a balance among usefulness of health services , patient safety , and proper allocation of resources . 
 in this study , we evaluate the relationship between visceral adipose tissue ( vat ) and non - clear cell renal cell carcinoma ( nccrcc ) in male patients . methods in this retrospective study , two groups were included : nccrcc group and control group . 
vat / sat ratio was subsequently calculated . results statistically significant differences between the two groups were found in tat area ( p = 0.05 ) , vat area ( p < 0.01 ) and vat / sat ratio ( p < 0.05 ) , while no significant difference was found in sat area . conclusions this study demonstrates an increased visceral adipose tissue in male patients with nccrcc . keywords adiposopathy carcinogenesis computed tomography non - clear cell renal cell carcinoma visceral adipose tissue introduction epidemiological studies have shown a direct correlation between obesity and carcinogenesis in various sites , in particular esophagus , pancreas , colorectum , breast ( postmenopausal ) , endometrium and kidney [ 1 , 2 ]  . 
obesity is defined as a body mass index ( bmi ) greater than 30kg / m2 , while overweight is defined as bmi greater than 25kg / m2 [ 3 ]  . 
diagnostica perimmagini territoriale aziendale , cittadella della salute azienda sanitaria locale di lecce , piazza filippo bottazzi , 73100lecce , italy 2 unit ofdiagnostic imaging , universit campus bio - medico di roma , via alvaro del portillo , 21 , 00128rome , italy 3 pathology unit , universit campus bio - medico di roma , via alvaro del portillo , 21 , 00128rome , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 538543 distribution of adipose tissue between individuals , nor it can give information on the quantity of the two compartments separately : visceral adipose tissue ( vat ) and subcutaneous adipose tissue ( sat ) [ 4 ]  . 
 the importance of the evaluation of the different compartments of adipose tissue derives from the concept that central obesity is more indicative of increased risk of insulin resistance , metabolic syndrome and cardiovascular diseases as compared to bmi alone [ 9 ]  . 
subjects with increased amount of vat , compared to sat , are exposed to a greater risk of development of insulin resistance [ 10 ] and metabolic syndrome [ 11 ]  . vat secretes growth factors , proinflammatory cytokines and adipokines , which are considered mediating factors associated with the oncogenesis of obesity - related tumors [ 8 ]  . computed tomography ( ct ) and magnetic resonance imaging ( mri ) are essential imaging techniques for noninvasive tissue evaluation and characterization [ 1216 ]  . it is known that men and women have different distributions of adipose tissue : women have more subcutaneous adipose tissue , while men have more visceral adipose tissue [ 9 ]  . 
premenopausal women have higher levels of sat ; after menopause , the estrogen levels fall , and the distribution of adipose tissue changes with an increased quantity of vat and a greater risk of obesity - related metabolic disorders [ 9 ]  . to date , the contribution of abdominal adipose tissue distribution to the development of non - clear cell renal cell carcinoma ( nccrcc ) has not been investigated . in this study , we use a ct imaging - based approach to test the hypothesis that male patients with nccrcc might have an increased amount of vat . methods patients in this retrospective study , we included two groups : the nccrcc group and the control group ; nccrcc group was composed of 13 papillary renal cell carcinoma ( prcc ) and 13 chromophobe renal cell carcinoma ( chrcc ) ( mean age 63.2 , range 4685 )  . 
nccrcc group data are listed in table1 . as the abdominal ct is regularly not performed in healthy subjects , as a control group we included 35 table 1 table of the data of nccrcc group mean age ethnicity histology laterality nccrcc history of other malignancy history of neoadjuvant treatment staging male ( 26 ) 63.2 ; 4685 ( 10 ) caucasian ( 26 ) prcc ( 13 ) chrcc ( 13 ) right ( 10 ) left ( 16 ) no ( 24 ) yes ( 2 ) no ( 25 ) yes ( 1 ) t1an0m0 ( 16 ) t1an0mx ( 1 ) t1bn0m0 ( 4 ) t2an0m0 ( 2 ) t2bn0m0 ( 2 ) t3an1mx ( 1 ) caucasian male patients who have performed a chestabdomen ct for preoperative cardiovascular surgery planning ( mean age 61.1 , range 4082 )  . patients included in the control groups underwent the following cardiac surgery : 18 mitral valve replacement , 8 aortic valve replacement , 1 mitral and tricuspid valve replacement , 2 left atrial myxoma resection , 3 combined coronary artery bypass and mitral valve replacement , 1 combined coronary artery bypass and aortic valve replacement , 1 combined coronary artery bypass with mitral and tricuspid valve replacement , and 1 aortic valve and ascending aorta replacement . 
finally , values of vat area were calculated by subtracting values of sat area from those of tat area . statistical analysis the tat , vat and sat areas and the vat / sat ratio were compared between the two groups using the students t test . 
showed that low levels of adiponectin are related to rcc , supporting the hypothesis that low levels of adiponectin may mediate the effect of visceral adipose tissue on the pathogenesis of rcc . 
in this study , 70 rcc patients were enrolled : 52 clear cell renal cell carcinoma ( ccrcc ) , 8 prcc , 6 chrcc , 1 collecting duct carcinoma and 3 unclassified [ 22 ]  . adiponectin is an adipokine produced by visceral adipocytes and its levels are reduced in obese subjects [ 23 , 24 ]  . 
a previous study from our group compared the amount of tat , vat , sat areas and vat / sat ratio of 10 ccrcc male patients and control patients , showing significant differences of the amount of vat and the vat / sat ratio [ 28 ]  . another study compared 63 caucasian prostate cancer patients with 63 age - matched healthy control patients ; the distribution of body adipose tissue was measured by ct with a 10 - mm - thick slice at the level of l4 . 
1 axial ct images show the rois of the vat areas in control patient ( a ) and nccrcc patient ( b ) 1 3 la radiologia medica ( 2020 ) 125 : 538543 fig . 
2 mean value of tat , vat , sat areas and vat / sat ratio in control and nccrcc groups were found in vat , tat and vat / sat ratio among the two groups , with a greater amount of vat in patients with prostate cancer , suggesting a role of visceral adipose tissue as a risk factor for prostate cancer [ 29 ]  . 
moreover , we have recently explored patients with non - small cell lung cancer and we found no significant differences between vat and sat compared to the control group [ 30 ]  . the present study was the first investigating abdominal adipose tissue distribution in a group of patients with nccrcc . 
our results showed significant differences in the mean tat area , vat area and vat / sat ratio between nccrcc patients and control patients . vat area could be considered as a quantitative imaging biomarker that might be linked to oncological risk of developing nccrcc . 
according to our results , this feature is of particular importance in patients with undetermined / unclear renal lesions . as a limitation , the retrospective nature of our study did not allow us to obtain more clinical information of the enrolled patients , such as hormonal status , in order to expand our analysis . 
future studies , with a greater number of patients and including female subjects , would be helpful in order to confirm the association between vat area and nccrcc risk . conclusions the results of this study suggest a link between abdominal , especially visceral , adipose tissue accumulation and nccrcc . 1 3 542 la radiologia medica ( 2020 ) 125 : 538543 author contributions all authors contributed to the study conception and design . 
all authors read and approved the final manuscript . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval approval from the institutional review board was not required because this is an observational retrospective study ; only existing information collected from human participants is used ; and there are not any identifiers linking individual to the data . ethical standards this article does not contain any studies with animals performed by any of the authors . 
the results were pooled by experience , analyzing sensitivity , specificity , accuracy ( area under roc curve ) , likelihood ratios , predictive values and overstaging / understaging . results addition of dwi improved diagnostic performance by specialists radiologists , particularly post - chemoradiotherapy ( accuracy 0.740.84 ; positive likelihood ratio 3.99.1 ; overstaging 168% ) , less so at primary staging ( specificity 7687.2% ; overstaging 2111% )  . 
residents showed small changes , except for notably increased sensitivity in both primary staging ( 35.743% ) and post - chemoradiotherapy ( 41.758.3% ) staging , at the expense of increased overstaging . conclusions the addition of dwi improved the diagnostic performance of emvi by experienced radiologists , downgrading overstaging , especially in post - chemoradiotherapy follow - up . 
 although staging is usually performed according to the american joint committee on cancer ( ajcc ) guidelines , some other features , such as circumferential resection margin or extramural venous infiltration ( emvi ) , should also be reflected in reports [ 35 ]  . emvi is defined histologically as the presence of tumor cells beyond the muscularis propria in an endothelium - lined vessel ; it is considered as a t3 stage , but not specifically assessed in the staging [ 2 , 6 ]  . 
this is despite the fact that different studies have demonstrated the role emvi plays as an independent predictor of lymph node metastasis , disease - free / overall survival , local recurrence and synchronous / metachronous distant metastases [ 714 ]  . 
previous studies have reported a moderate to high accuracy in the detection of emvi using high - resolution t2w ( hrt2w ) mri sequences , but with a wide range of documented sensitivities and initial staging results showing better results than the post - crt results [ 8 , 9 , 11 , 15 ]  . there are few references to the performance of diffusion - weighted imaging ( dwi ) concerning emvi , most likely due to the possible reduction in usefulness resulting from its lower resolution , even though larger vessels could be assessed [ 16 ]  . 
furthermore , dwi could allow a more accurate evaluation of the tumor contour , thanks to better distinction of reactive tissue or microvessels adjacent to the tumor with comparable signal intensity , and differentiation of fibrosis and viable tumoral remnants [ 16 , 19 ]  . on the other hand , dwi has demonstrated to improve rectal cancer detection and delimitation added to t2w sequences ; radiologists without the previous experience could benefit to a larger extent from that . 
in that case , using dwi might be helpful during the early stages of the learning curve or in less - specialized radiologists or centers . hence , the aim of the study was to assess the potential changes in mri detection of emvi in rectal cancer , both in primary staging and post - crt follow - up , produced by the use of dwi added to hrt2w , compared to the use of hrt2w alone . 
as a secondary objective , while these potential improvements were analyzed in experienced radiologists , the performance of radiologists without prior experience in rectal cancer staging and radiology residents was also considered . methods patient population this cross - sectional study was approved by the research ethics committee of our center . 
all patients satisfied the following inclusion criteria : ( 1 ) rectal cancer diagnosis , proven by colonoscopy and biopsy ; ( 2 ) correctly performed rectal mri , using an identical technique to that of all the other mris , with no significant artifacts and fully available for review ; ( 3 ) post - crt follow - up mri when neoadjuvant treatment was necessary ; and ( 4 ) surgery after mri with complete surgical specimen ( total mesorectal excision / abdominoperineal resection )  . 
the neoadjuvant therapy schedule consisted in 825mg / m2 of capecitabine ( oral , twice daily ) on an outpatient basis , concurrently with radiotherapy ( long cycle , normofractionated pelvic radiation at a total dose of 50.4gy over 25 sessions )  . 
in general , the indication for crt did not include iia stages with at most millimetric infiltration , with no factors of poor prognosis . pathological analysis the standard of reference was pathological staging . 
all histopathologic slides were reviewed by two experienced pathologist ( 7 and 10years experience in interpretation of colorectal cancer specimens ) to give the histological stage , following the guidelines of the ajcc [ 3 ]  . 
1 workflow chart of the study la radiologia medica ( 2020 ) 125 : 522530 table 1 mri acquisition protocol hrt2w plane axial , coronal , sagittal axial axial , coronal , sagittal reference tr / te ( ms ) slide thickness matrix f.o.v. duration pelvis 4700 / 95 6mm 256 230 150s tumor axis 4000 / 95 3mm 256 230 135s pelvis 5000 / 70 5mm 192 115 200s endothelium - lined space that is either surrounded by a rim of smooth muscle or contains red blood cells [ 22 ]  . mri protocol all patients underwent 1.5 - t rectal mri in the same center ( magnetom avanto ; siemens healthcare , berlin , germany ) , using a 16 - channel phased - array body surface coil . 
contrast materials were not used . image assessment the images of every case were reviewed by ten radiologists with different degrees of experience in staging rectal cancer using mri , independently and blinded to any information except for the presence of biopsy - proven malignancy . 
the ner and rr received a baseline training ( 2h ) before the start of the study , consisting of review and discussion of several cases from our center and imaging examples . radiologists were asked to assess the presence or absence of emvi in each patient , twice every single case . 
the proposed scale was adapted to a three - point one ( 1negative , 2doubtful , 3positive )  . after a minimum 1 - month washout period , with the aim of preventing memory bias , radiologists analyzed all mris a second time , and this time using both hrt2w and dwi images presented side by side . 
the suspicion criterion for 1 3 la radiologia medica ( 2020 ) 125 : 522530 emvi in dwi was pre - defined as the presence of high signal intensity on a high b - value sequence and moderate to high hypointensity on the adc ( restricted diffusion ) , neighboring the main tumor and coincident with the location of the vessel in the hrt2w sequence ( figs.3 , 4 ) [ 16 ]  . 
2 primary staging mri from a 73 - year - old man with rectal adenocarcinoma : axial ( a ) and sagittal - to - tumor and ( b ) high - resolution t2w sequences . 
3 primary staging mri from a 77 - year - old man with rectal adenocarcinoma : sagittal - to - tumor high - resolution t2w sequence ( a ) and axial diffusion - weighted imaging ( b ) and adc map ( c )  . 
an expanded tubular structure adjacent to the posterior wall of the rectum ( arrowheads ) presented similar intensity in t2w sequence , suggestive of extramural venous infiltration that was histologically confirmed . 
tubular ( white arrow ) and nodular ( arrowhead ) expansion of vessels with moderate intensity was visible ( arrows ) in the axial high - resolution t2w sequence ( a )  . 
the histological results confirmed the persistence of extramural venous infiltration 1 3 526 la radiologia medica ( 2020 ) 125 : 522530 diagnostic accuracy ( by means of the area under the roc curveauc ) , sensitivity and specificity , positive and negative predictive values ( ppv / npv ) and likelihood ratios were all calculated for each group in every reading , group and category ( primary staging or post - crt followup )  . 
subsequently , over staging and understaging rates and intragroup agreement ( fleisss kappa ) were obtained for every reading . table 2 demographic and histological staging data of the sample demographic data mean age male ( 75 ) female ( 25 ) mri study and corresponding histology primary staging adenocarcinoma no malignancy analyzed lymph nodes ( average ) post - chemoradiotherapy follow - up adenocarcinoma no malignancy analyzed lymph nodes ( average ) surgery approach ( total mesorectal excision ) anterior approach abdominoperineal resection histological staging ( surgical specimen ) 63 y . 
 at primary staging , out of the 19 cases with positive nodes , four were related to histologically positive emvi ( 21% of cases ) , while post - crt group revealed malignant nodes in 18 cases , two of them emvi positive ( 11% )  . the results for accuracy are presented in table3 , while table4 shows sensitivity , specificity , likelihood ratios , predictive values and intragroup agreement results . 
all the results for the er group showed statistical significance by themselves ( p < 0.05 ) , as were those of the dwi reading by the other groups , except for the post - crt follow - up by the ner and the accuracy results . 
the distribution of the groups and pooling by experience is the same as that in table3 la radiologia medica ( 2020 ) 125 : 522530 global emvi primary staging post - crt overst . 
our results show a significant improvement in the performance of the er group with the additional use of dwi , especially in the post - crt follow - up and associated with the accuracy and positive predictive parameters . 
benefits in the detection and delimitation of viable tumors , secondary to the use of dwi , have been reported in previous studies [ 21 , 24 , 25 ]  . 
furthermore , it has been suggested that using dwi could allow a more accurate evaluation of the tumor contour , with better distinction of reactive tissue or microvessels adjacent to the tumor that has a comparable signal intensity to it [ 19 ]  . 
 meanwhile , our mri detection prevalence was within the documented ranges of 23.747.6% , with a sample range of 22%28% ( 16.638.8% at primary staging ; 15.228.2% at post - crt follow - up ) [ 31 ]  . 
 our results were mostly within the documented ranges , but the comparison with the previous work is hindered by some methodological differences : consensus readings between two radiologists , added contrast - enhanced sequences or samples including specific tumoral stages , were sometimes present [ 2729 ]  . we could only find two studies of emvi including dwi . 
in the second study , the use of gadolinium - enhanced t1w sequences along with dwi and the absence of histological correlation of primary staging mri both limit in comparison with our results [ 34 ]  . 
those authors reported a moderate increase of sensitivity with the addition of dwi and contrast - enhanced t1w , both at primary and post - crt staging ( 4350% to 57% ; and 29% to 4357% , respectively )  . 
despite the coincident greater improvement in the post - crt follow - up , unlike us they reported almost no changes in accuracy and specificity . to the best of our knowledge , no previous study included inexperienced radiologists in the mri assessment of emvi ; their results might represent the early stages of the learning curve . 
we hypothesize that the previously reported increase in viable tumor detection and delimitation with the use of dwi could be related to this finding [ 21 , 24 , 25 ]  . 
however , 1 3 la radiologia medica ( 2020 ) 125 : 522530 the interpretation of post - crt follow - up mri may sometimes be challenging , hindering the identification of vessels within the fibrotic or inflammatory aftermath , or overstaging peritumoral high signal intensity in dwi [ 16 , 18 , 26 ]  . 
since they had less experience in the use of dwi , misinterpretations were more likely ; factors such as edema , desmoplastic reaction or inflammation may have led to overstaging , which obviously lowers the accuracy rate [ 16 , 35 ]  . 
nonetheless , the results of the inexperienced radiologists must be interpreted cautiously : the small amount of positive emvi cases in the sample ( particularly post - crt ) may have yielded aberrant changes between readings . our study had some limitations to consider . 
third , the different angulation and slide thickness of hrt2w and dwi hindered comparison ; in order to increase the accuracy of the study , the same characteristics for both sequences would have been preferable . 
furthermore , the dwi slide thickness also hindered proper assessment of small vessels ( < 3mm ) ; but anyway , their identification and characterization may be challenging due to insufficient spatial resolution or partial volume artifacts [ 11 , 18 ]  . 
finally , the statistical analysis was restricted by the small number of positive results ; a problem present in most studies of this topic , due to the limited number of cases . 
this should be borne in mind during interpretation , especially in terms of sensitivity and ppv values , as it limits the clinical significance of the findings . conclusions according to the results of the study , adding dwi to hrt2w sequences improved the diagnostic performance of experienced radiologists and downgraded overstaging , especially in the post - crt follow - up mri . 
for the inexperienced radiologists and residents this addition brought about fewer changes , with some improvements in the primary staging and increased sensitivity in both primary staging and postcrt staging , respectively . acknowledgements we would like to thank christopher evans for his kind support in the translation of this work . funding this study was funded by the medical college of las palmas foundation [ research grant , year 2018 ]  . 
how tocreate ano fly zone : anorthern italy experience giampaolomontesi1 saidedibiase1 sarachierchini1 giovannipavanato1 graziellaeliavirdis1 edgardocontato2 giovannimandoliti1 received : 8 april 2020 / accepted : 27 april 2020 / published online : 15 may 2020 italian society of medical radiology 2020 abstract background sars - cov - 2 pandemic represents a troubling health emergency but also a main challenge for the clinical governance of the systediscontinuation of radiation treatments is not desirable and potentially life - threatening . 
we report our extended protocol , draft to manage clinical activities in our radiotherapy department , by minimizing contagion risks . methods we used telephonic screening to assess the need for patient admission . 
the activities were distributed during the whole workday , avoiding overlap to reduce aggregation . results from 1st february 2020 to 31 march 2020 , we reported an increase in the number of first medical examinations and treatments , compared to the same period of the previous year . 
no covid - 19 cases were detected . conclusion during covid - 19 pandemic , we introduced procedures that allowed us to ensure the continuity in oncological cares , with limited risks of infection for patients and staff . keywords covid - 19 pandemic sars - cov - 2 coronavirus radiotherapy radiation oncology introduction since sars - cov - 2 spread throughout the world , clinicians operating out of urgency area , faced out an overwhelming issue concerning the clinical governance of the system . in high - risk areas , directions of hospitals , closed outpatient treatments and follow - up , except for oncological ones . 
the interview is aimed to assess general health condition , the presence of neoplasm - related symptoms , the results of prescribed tests and / or reports of diagnostic radiology exams . in case of stable or not evident disease , the appointment is cancelled and rescheduled as soon as possible . 
the patients are asked about the presence of fever , cough , flu - like symptoms ( arthralgia , myalgia , cold , diarrhoea ) , about the contact with positive or suspect case of covid - 19 and finally about the geographical provenience . 
in case that the triage is suspect for symptoms or risk of contagion , the referring physician activates the procedure by contacting the patient general practitioner ( gp ) or a national dedicate emergence telephone number ( etn )  . patients who need access toradiotherapy department : reserved entrance in order to reduce contacts and infections , radiotherapy staff and patients are invited to access to the department using this gateway rather than the main entrance of the hospital . 
spinal cord compression , superior vena cava syndrome , life - threatening lower airway obstruction , digestive or respiratory haemorrhage and life - threatening brain lesion , radiation therapy might be delivered within 2448h . 
therefore , we considered crucial to pre - identify risk classes of potential to contagion by telephonic triage : not - suspicious asymptomatic ( low risk ) who can be admitted and treated without restrictions and suspicious asymptomatic or suspicious symptomatic ( high risk ) , which should be referred to gp or to etn , and even sent to diagnostic swab , when recommended [ 3 , 4 ]  . for other palliative non - urgent treatments , i.e. 
painful metastatic bone lesions , lung cancer causing chest pain or pancoast syndrome , tumours causing nerve root and soft tissue infiltration , relief of impending airways or bowel obstruction , it is generally indicated that radiotherapy should be started within 7days . 
in high - risk contact , adequate personal protective equipment ( ppe ) was required to safely undergo treatments [ 5 , 6 ] , while in low - risk class , no specific restriction has been indicated . nonurgent treatments in non - urgent cases : prostate cancer patients , breast cancer patients , benign cns tumour or even non - oncologic patients , treatment could be postponed following priority codes that mainly indicates up to 3months interval from diagnosis to treatment . 
 head and neck cancers , rectal and anal cancer , gastroesophageal junction , we select patients to avoid delays in consultation and treatment which may adversely affect potentially curable cancer patients [ 7 ]  . covid19 positive patients finally , in covid - 19 positive patients , it is nowadays very difficult to give an indication to settle the risk of cancer complications / risk of infection ratio . 
moreover , a potential spread of contagion through health care operators may awfully affect the ability to provide care , also leading to service closure . documents and position paper globally tend to advise against the beginning of a radiation treatment in covid - 19 positive patients [ 8 ]  . modulation oftheactivities with the aim of reducing the number of people in the waiting - room , all the activities ( first medical examination , simulation ct , day hospital access and follow - up visits ) are distributed during the whole workday , avoiding overlap . 
the patients in treatment are located in a second distinct waiting roochairs of the two waiting room are spaced with the aim to maintain a minimum distance of 1all patients are recommended to strictly observe the assigned schedule to avoid extra waiting time . 1 3 602 results from 1st february 2020 to 31 march 2020 , we reported an increase in the number of first medical examinations , from 114 to 124 compared to the same period of the previous year . 
the aim of this work was to study invitro the effects of direct exposure of the jarvik 2000 lvad to 10 - mv photon beams . methods jarvik 2000 pump was immersed in a siliconized box filled with deionized water . 
during irradiation , the external flow maker controller and the lithium battery were positioned away from the beapump parameter data ( included voltage , current and frequency ) were measured , recorded and analyzed for changes in pump function among baseline , pre - irradiation , during irradiation , post - irradiation and after 6months . 
the measured x - ray attenuation differed from the calculated one by tps by 34% . conclusion the jarvik 2000 resulted stable under direct x - ray beam of 10 - mv energy . 
its strong attenuation , however , can affect dose deposition in the pump in tps , and it must be taken into account . keywords jarvik 2000 system radiotherapy vad in vitro evaluation introduction currently , left ventricular assist devices ( lvad ) is considered a standard care for patients with advanced heart failure . 
the treatment of these patients that require surgery , radiation or chemotherapy in lvad recipients is complex due to the potential interaction of therapies with the function of the pump . 
as reported in the literature [ 2 , 3 ] , the concomitant presence of a lvad system can be associated with severe complications , including bleeding , infection and lvad malfunction . among the concomitant diseases that occur in lvad patients , cancer that requires radiation therapy has specific aspects that may raise specific concerns . 
in the literature , the effects of radiation exposure during oncologic radiotherapy vol . : ( 0123456789 ) 1 3 562 la radiologia medica ( 2020 ) 125 : 561568 ( rt ) have long been studied for the most common cardiovascular implantable electronic cardiac devices ( cieds ) , such as implantable cardioverter defibrillators ( icds ) and pacemakers ( pms )  . 
for these devices , rt has to be administrated using specific guidelines in order to avoid possible malfunction or failure [ 46 ] due to electromagnetic interference ( emi ) and direct damage via ionizing radiation [ 7 ]  . 
ionizing radiation can also create induce interactions with the electronic circuits mainly associated with the currentvoltage characteristics of the transistors that are easily degradable in proximity to an ionizing radiation field . 
another issue is the interaction between the controller and the battery due to the presence of neutrons in the treatment rooneutrons are produced by interaction of photon beams 10mv with the inner parts of the linear accelerator ( linac ) [ 12 , 13 ]  . 
they can damage both the complementary metal - oxide semiconductor ( cmos ) present in the external system controller and the battery [ 14 ] , even if they are not in the direct path of the rt field . guidelines and the literature provide numerous indications to preserve the functionality of cieds in patients undergoing rt [ 4 , 1528 ]  . 
although some malfunctions due to radiations can cause deleterious complications up to the death of the patient , the effects of high - energy photon beam interaction ( 6mv ) with lvad systems have not been extensively studied [ 1 , 2935 ]  . 
in particular , malfunctions due to the presence of neutrons that might remotely interact with components of the system , such as controllers and batteries , have not been studied . 
this study aimed to evaluate invitro effects of direct exposure of jarvik 2000 lvad system to 10 - mv photon beams . materials andmethods the device the jarvik 2000 ( jarvik heart , inc , new york , ny ) lvad system is an electric axial flow pump generating a nonpulsatile flow . 
it is supported by ceramic bearings and spins blood to generate an average flow rate of 5 l / min ( up to 7 l / min ) with a rotation speed of 800012000rpm [ 32 ]  . 
the intermitted low - speed phase permits an adequate filling of left ventricular cavity and anterograde flow through the aortic valve reducing the risk of aortic root thrombosis . the device is connected to an external flow maker controller delivering power via a tunneled driveline from a lithium ion battery . 
the display shows the instant pump consumption . the flow maker controller is continuously powered by the lithium battery and drives the jarvik 2000 pump with a thrice - redundant three - phase power supply . 
a thrice - redundant supply ensures continuous functioning of the pump in case of eventual damage to the electrical connection . experimental setup andtreatment planning the jarvik 2000 lvad system was tested under exposure to 10 - mv photon beams produced by the synergy agility ( elekta ltd . , crawley , uk ) linac . 
in this slowing status ( ils ) , the contraction of the left ventricle caused the anterograde outflow through the aortic valve and achieved the complete wash - out of the aortic root . voltage , current and frequency parameters were initially measured to establish a reference baseline ( bl )  . 
during the irradiation , parameters were monitored to verify that the external controller was functioning correctly . during the irradiation , parameters were monitored to verify that the external flow maker controller and the lithium ion battery were functioning correctly . 
the entire measurement session lasted 6months . the mannwhitney u statistics implementation in r [ 36 ] was used on median of time points per measure per nominal power in order to test the stability of the parameters in time fig . 
a metex m3850 - d multimeter was used for 1 3 564 la radiologia medica ( 2020 ) 125 : 561568 at different operating assistance level speeds chosen by the operator . in the case of pump attenuation and ic , the linac accelerator was programmed to deliver 2gy at a dose rate of 6gy / min at the isocenter , both with and without the pump ( with the center of the pump coinciding with the isocenter ) placed in the siliconized box filled with deionized water . 
 the box was moved in 2mm increments on the central axes of the phantom along the entire length of the pump so as to record the maximum value of the pump attenuation . 
 results for each operating status ( s1 or s2 ) , the investigated parameters included current ( ma ) , voltage ( mv ) and frequency ( hz ) as a function of nominal power ( w )  . 
table1 and table2 report w , ma , mv and hz values , measured for bl , pre , treat , post and final for s1 and s2 , respectively . 
these results seem to indicate that the dose algorithm in the tps did not adequately model the energy distribution when the field passed through the titanium components . discussion the management of patients with aicds or pmks undergoing radiation therapy is well supported by the literature [ 4 , 1528 ]  . 
even though the jarvik 2000 lvad is commonly employed as a bridge to heart transplantation or as destination therapy in case of end - stage heart failure , the interaction of radiation therapy with this specific lvad has not been investigated as well [ 1 , 2935 ]  . 
the main issue is related to the table ct to electron density ( ed ) in the tps oncentra masterplan that cannot be modified and therefore does not compensate for elements with electronic densities greater than those normally encountered in the body . 
the p value of the mannwhitney u test is reported too table 3 jarvik 2000 lvad system maximum attenuation ic measurements 2d array measurements tps estimation %difference ictps = 34 ; %difference 2d arraytps = 27% maximum attenuation by the algorithm as a very dense bone , resulting in underestimation of attenuation . 
in cases when it is unavoidable , a different beam angle that does not go through the device should be selected in order to accurately administer the desired dose to the target . the results of the effects of radiation with lvad system showed the differences between ma , mv and hz values collected for each nominal power in the bl and those values registered immediately before , during and immediately after radiation delivery and 6months later the last reading were not statistically significant . 
these results were consistent with the fact that the controller , the most sensitive component of the jarvik 2000 to radiation damage , was placed outside the direct beam , at the opposite end of the treatment couch , during therapeutic delivery of radiation . 
the pump , instead , as it did not contain implanted circuitry , was not affected by radiation and continued to operate normally . even if the battery and the controller were placed outside the direct photon , they could interact with neutrons , generated as secondary radiation types in linac with photons energy 10mv . 
the dose by neutron was estimated to be roughly 0.5% of the x - ray dose at isocenter , which means about 3.3cgy in our case [ 37 ]  . 
moreover , the neutron dose scales with the inverse of the square distance , so that at the distance where we placed the controller ( 1.5m away from the isocenter ) , the neutron dose was less than 2cgy . the fact that the battery worked until it was exhausted and the parameter values measured in the controller remained stable over the time means that interactions with neutrons did not produce effects jeopardizing the function of this component . another potential issue was the interference with static magnetic fields created by linac . 
therapeutic radiation , in fact , was associated with various sources of emi including couch drive motors , shutters , x - ray tube rotors , cooling pumps , x - ray transformers , power supplies , magnetrons , klystrons , waveguide assemblies and beam pulse forming circuits . 
reported the case of a patient with cardiac ventricular assist device ( vad ) undergoing rt to the rectum 1 3 la radiologia medica ( 2020 ) 125 : 561568 [ 34 ]  . 
in any case , these effects are usually transient and are only observed when the machine is turned on [ 9 ]  . for the jarvik 2000 , however , this issue is a serious matter as the pump contains a neodymium - iron - boron magnet housed inside the titanium - welded shell . 
in any case , more invitro and invivo studies on a large scale are required to confirm the absence of emi effects on the pump . the results of this study are in accordance with those reported by gossman etal . 
had already conducted previous testing with the heartware hvad pump and found no electronic instability in the application of radiation therapeutic x - rays and protons [ 29 ]  . 
due to the lack of reported studies , we decided to use both energy and not too high doses in order to be conservative . subsequent studies should expand this experimental design to evaluate more than one jarvik 2000 system to confirm these results and investigate long - term effects using doses higher than those employed in this preliminary study and 1518 - mv photon beams in order to take into account eventual malfunctions due to neutrons component conclusion the jarvik 2000 lvad functionality was investigated under direct x - ray beam of 10mv energy delivered from a linac . 
the results obtained indicated that both direct irradiation and indirect irradiation , through x - ray on the pump and scattered neutrons on the controller and battery , respectively , do not affect the normal function of the lvad . 
in any case , particular attention must be paid to the tps dose calculation in the presence of such a systewe found that the tps underestimated the absorbed dose from the pump due to a bad modeling of the titanium components of the pump itself . 
the authors describe how to achieve the intra - articular fragment line in order to address the surgical management . the authors evaluated retrospectively 40 patients with distal radius fractures , after tc scan pre - operative examination . 
they identified five types of common fractures pattern . figure3 shows , with a very impressive manner , the frequency of fracture occurrence . in the description of materials and methods , the authors do not describe the type of trauma . 
this detail could be really important , especially if one of the aims was to choose the surgical approach for each types of fractures [ 1 ]  . in a recent paper , biondi etal . 
they analysis deepen the wrist position at the time of injuries . so , the data reported in both articles could be analysed together , in fact the reported t line could be easily explained with a throttle position . 
in fact the carpal bones are slightly flex and the firs carpal row could impact on the dorsal portion of the radius . i encourage the authors to consider the different line fracture as the consequent of different carpus position . 
you have an effect on others , and therefore , you are responsible for what you do and what you decide to do.but if you do not do this yourself , but an artificial intelligence system , it becomes difficult and important to be able to ascribe responsibility when something goes wrong . 
the manuscript addresses the following statements : ( 1 ) using ai , the radiologist is responsible for the diagnosis ; ( 2 ) radiologists must be trained on the use of ai since they are responsible for the actions of machines ; ( 3 ) radiologists involved in r&d have the responsibility to guide the respect of rules for a trustworthy ai ; ( 4 ) radiologist responsibility is at risk of validating the unknown ( black box ) ; ( 5 ) radiologist decision may be biased by the ai automation ; ( 6 ) risk of a paradox : increasing ai tools to compensate the lack of radiologists ; ( 7 ) need of informed consent and quality measures . 
future legislation must outline the contours of the professionals responsibility , with respect to the provision of the service performed autonomously by ai , balancing the professionals ability to influence and therefore correct the machine , limiting the sphere of autonomy that instead technological evolution would like to recognize to robots . keywords artificial intelligence robotics ethics radiology introduction we are living in the automation society that automates more tasks and automates to a larger extent than before [ 1 ]  . the boost to automation originates from the introduction of artificial intelligence in many human tasks . 
such systems allow to automate and * emanuele neri emanuele.neri@med.unipi.it 1 diagnostic radiology 3 , department oftranslational research , university ofpisa , pisa , italy 2 radiology unit , department ofdiagnostic andpreventive medicine , sant orsola malpighi university hospital , bologna , italy 3 department ofemergency radiology , university hospital careggi , florence , italy 4 snr foundation , rome , italy 5 department ofradiology , university ofcampania luigi vanvitelli , naples , italy repeat human tasks as switching on and off the house light , scheduling a music playlist , switching on and off the heating in our house , etc . : all processes that can be programmed and that intelligent systems can learn to perform independently after performing them during a learning phase , which could be defined the ground truth . 
at the base of these automatic actions , there are machine / deep learning algorithms that enter into our daily life and , from our actions , learn to suggest common and new behaviors in our living . automation is a benefit until these automated actions are carried out in harmony with what we want , but when the automated actions go further , suggesting or carrying out unwanted actions or causing damage to things and people , questions of responsibility arise which have been unexplored up until now . the aim of this editorial is to find an answer to the question who or what is responsible for the benefits and harms of using this technology ? vol . : ( 0123456789 ) 1 3 518 la radiologia medica ( 2020 ) 125 : 517521 who orwhat istheagent ofresponsibility ? when human beings make decisions , the action itself is normally connected with a direct responsibility by the agent who generated the action . 
you have an effect on others , and therefore , you are responsible for what you do and what you decide to do . but if you do not do this yourself , but an artificial intelligence system , it becomes difficult and important to be able to ascribe responsibility when something goes wrong . a typical example is the case of a self - driving car or an airplane using ai [ 3 ] ; it should be asked : if the automation system of the car or the airplane autopilot causes an accident , who is responsible ? the greek philosopher and polymath aristotle gives an answer to this problem [ 4 ]  . 
so , in the control condition , you are responsible if you do it ( or have done it ) , if you are the agent of the action , if you have caused the action , if you have a sufficient degree of control over the action , but to attribute a full responsibility , an epistemic condition , as you know what you are doing or you are aware what you are doing ( or knew what you were doing ) , is required . aristotle argued in the nicomachean ethics that the action must have its origin in the agent and that one must not be ignorant of what one is doing [ 5 ]  . ai technologies do not meet traditional criteria for full moral action ( and hence preconditions for responsibility ) such as freedom and consciousness , and therefore , they also cannot be ( held ) responsible [ 6 ]  . with regard to the two aristotelian conditions , it is thus assumed that it does not make sense to demand that the ai agent act voluntarily or without ignorance , since an ai agent lacks the preconditions for this : an ai cannot really act freely ( as in having free will ) or know ( as in being aware of ) what it is doing . if this assumption holds , then our only option is to make humans responsible for what the ai technology does . key point 1 using ai the radiologist is responsible for the diagnosis . a help fromthelaws on february 16th , 2017 , the european parliament approved a resolution with recommendations to the commission on civil law rules on robotics [ 7 , 8 ]  . 
in fact , the resolution refers to the role of robotics in surgery , but the similarities of the relationship between robots and the surgeon with the relationship between artificial intelligence and radiologist are so strong that they are superimposable . the resolution was based on a study requested by the european parliaments committee on legal affairs and commissioned , supervised and published by the policy department for citizens rights and constitutional affairs . 
the study highlights the importance of a resolution for the immediate creation of a legislative instrument governing robotics and artificial intelligence , to anticipate any scientific developments foreseeable over the medium term and which could be adapted to track progress . 
we can therefore state that the resolution correctly predicted the current situation . the study furthermore explored the liability for damages caused by an autonomous robot and stated that the expression robots liability should be banned , since it implies that the robot might itself incur civil liability for any damage caused . 
instead the concept of vicarious liability for the robot ( s ) was proposed . in the paragraph dedicated to medical robots , the resolution of the european parliament underlines : the importance of appropriate education , training and preparation for health professionals , such as doctors and care assistants ; the need to define the minimum professional requirements to use a robot ; the respect of the principle of the supervised autonomy of robots ; the need for training for users to allow them to familiarize themselves with the technological requirements in this field ; the risk of self - diagnosis of patients using mobile robot ; and , consequently , the need for doctors to be trained in dealing with self - diagnosed cases . 
important key factors of a trustworthy ai for radiology are also the data governance , the privacy and the transparency , for which an ai system should guarantee at the same time quality , integrity and confidentiality of the data processed and be explicable about the processes / algorithms used to process patients data . the theme of explicability is very important as an ai system is considered a kind of black box , of which perhaps mathematical and logical processes are understood , but not clearly the transformations of the data contained in it after various passages within the neural network ( i.e. , the convolutional networks )  . radiologists are familiar with digital imaging and informatics , and those with an imaging informatics special interest are frequently involved in ai algorithms development and clinical validation . 
therefore , they have the potential to look into the black box and guide the research and development process , ensuring the respect of rules . key point 3 radiologists involved in r&d have the responsibility to guide the respect of rules for a trustworthy ai . professional risks fortheradiologist use oftheblack box inclinical practice in a cad paradigm , as first reader , second reader , or in concurrent reading [ 1215 ]  . 
in all cases , the final responsibility is in the hands of the radiologist , and a debate is still open about including cad results into the radiology report and informing patients that the diagnosis is supported by automated software . however , a clear distinction between cad and ai must be traced , since cad is designed to perform specific tasks on the basis of a training set and ai power and promise is that useful features can exist that are not currently known or are beyond the limit of human detection . 
a typical example is radiomics , where a texture analysis can generate hundreds of features that a human being cannot generate and interpret [ 16 ]  . in clinical practice , radiologists will be asked to monitor ai system outputs and validate ai interpretations ; so they risk to carry the ultimate responsibility of validating what they cannot understand . key point 4 radiologist responsibility is at risk of validating the unknown ( black box )  . automation bias the recent north america and european multi - society paper about ethics of artificial intelligence in radiology reports the risk of the automation bias [ 17 ]  . automation bias is the tendency for humans to favor machine - generated decisions , ignoring contrary data or conflicting human decisions . 
automation bias leads to errors of omission and commission , where omission errors occur when a human fails to notice , or disregards , the failure of the ai tool . 
this is compounded by ai decisions made based on features that are too subtle for humans to detect . commission errors occur when the radiologist erroneously accepts or implements a machines decision in spite of other evidence to the contrary . the typical feature of the act performed by the radiologist , as a professional , is the autonomy of decisions on the provision of service and the technical tools to be used , and the personality of the service [ 18 ]  . 
it is clear that these peculiarities must be harmonized with the automation of in radiology , the clinical use of computer - aided diagnosis ( cad ) is well known ; multiple studies have shown advantages , limitations and risks of image interpretation key point 5 radiologist decision may be biased by the ai automation . 1 3 520 la radiologia medica ( 2020 ) 125 : 517521 shortage ofradiologists andinappropriate training much discussion has been raised in the media about the introduction of artificial intelligence in radiological practice , suggesting that radiologists could become useless or even disappear as a specialty [ 1921 ]  . 
this could lead to a lack of motivation for young doctors to pursue a career in radiology , with a real imminent risk of not having enough radiologist specialists . an additional risk for young doctors in training is the reduction in training opportunities . 
in fact , if the use of artificial intelligence systems in clinical practice can accelerate interpretation times , it can also reduce the number of examinations / images that a radiologist in training will be able to interpret . 
in other words , the greater the automatic tasks performed by artificial intelligence , the less those performed by the radiologist . the paradox of this situation would be the need to implement ever greater ai tasks to compensate for the progressive lack of radiologists . key point 6 risk of a paradox : increasing ai tools to compensate the lack of radiologists . radiologistpatient relationship anddata integrity a contingent problem with the introduction of ai and of no less importance is transparency toward patients . 
they must be informed that the diagnosis was obtained with the help of the ai . all this poses problems to the patients informed consent and the adoption of quality measures of the patients care providers ( public or private institutions ) on ai systems . quality measures should relate to software robustness and data security , as well as constant updating of software and hardware , avoiding equipment obsolescence . 
particular attention should also be paid to image processing , guaranteeing its integrity during the analysis process with neural networks , thus avoiding a modification of the raw data . key point 7 need for informed consent and quality measures . conclusions artificial intelligence is entering the radiological discipline very quickly and will soon be in clinical use . 
the european society of radiology stated that the most likely and immediate impact of ai will be on the management of radiology workflows , improving and automating acquisition protocols , appropriateness ( with clinical decision support systems ) , structured reporting , up to the ability to interpret the big data of image biobanks connected to tissue biobanks , with the development of radiogenomics [ 22 ]  . but the fundamental problem of an ethical and not harmful ai still remains . are there solutions ? in a recent article published by thomas ps etal . , the application of a defined seldon algorithm is described . 
this paper aims at developing a system for computer - aided diagnosis to help in the detection , labeling and segmentation of lumbar vertebral body ( vb ) and to further classify each vb into normal , malignant and benign vcfs . 
the dice similarity coefficient ( dsc ) for segmentation reached up to 94.27% , and the classification results show that shape and texture features together are able to correctly classify with an accuracy rate of 95.34%. 
the final outcomes are expected to be useful in the analysis of vertebral compression fractures . keywords vertebral compression fractures vertebral body segmentation vertebral body classification mri statistical texture features shape features distances slopes introduction medical imaging continues to have a substantial role in the diagnosis and follow - up of vertebral fractures . 
this is especially common in the elderly population due to the higher incidence of vcfs secondary to bone failure , whereas a radiologist will have no doubt about the etiology of a traumatic vcf . 
clinically , bone failure related to osteoporosis is diagnosed as benign , whereas metastatic * adela arpitha adelaarpitha23@gmail.com 1 department ofstudies incomputer science , university ofmysore , manasagangotri , mysore , karnataka570006 , india cancer affecting bone is diagnosed as malignant . 
although complaints associated with each vcf types , benign and malignant , may be similar , the differentiation between these two types of vertebral fracture is fundamental for the diagnosis and treatment of the patient [ 2 ]  . 
mri is the mainstay imaging modality for spinal abnormalities and is the most accurate technique to evaluate non - traumatic vcfs [ 3 ]  . the anatomy of the spine is built up of 33 vertebrae ( 7 cervical , 12 thoracic , 5 lumbar , 5 fused sacrum and 4 fused coccyx vertebrae ) with soft intervertebral disks in between each vertebra aiding and supporting in the flexible movements of the spine . 
the vertebra is comprised of two sections : anterior section consisting of the vertebral body ( vb ) and posterior section having the vertebral arch , as well as seven processes . 
1 a labeled sagittal view of spine ; b basic labeled instance of a lumbar vertebra the distribution of the signal intensity abnormality throughout the vb is an important criterion to help in the differentiation between a benign and a malignant vcf in mri . 
the study of the segmentation of mri spine image and its classification into different etiologies such as fractures and deformations is of crucial importance for computeraided medical image identification and clinical studies . 
in this scenario , the accurate observation of the appearance of vcfs in mris and the appropriate assessment by the radiologist become fundamental to establish the appropriate treatment for the patient . in current clinical practice , most of the procedures for quantitative morphometric analysis of vbs are performed manually by a radiologist or a clinician , in a manner that is labor - intensive and subject to significant inter - observer and intra - observer variability . 
also , due to the expensive work involved with quantitative evaluation performed manually , the usability of such methods is not practical on a large scale [ 1 ]  . 
the different appearances of the vbs in relation to the etiology and severity of the fractures cause variations in signal intensity profiles and in shape of the vertebral bodies [ 6 ]  . 
different instances of normal , benign and malignant vbs are shown in fig.2. malignant vcfs are known to cause posterior vb cortex convex bulging more frequently , while benign vcf may cause a posterior wall fragment retropulsion with angulated or irregular contours . 
malignant vcfs could result in a posterior bulge or convexity of the posterior vb wall though it may occur together with a concave deformation in the region of the vertebral plateaus . 
however , vertebrae without any fracture may present small bone outgrowths and some marginal bone proliferation known as bone spurs or osteophytes , which may cause shape abnormalities [ 3 ]  . 
with more complex spinal curves such as cases with scoliosis , kyphosis and lordosis , there is more variation in disk and vertebra size , and also with more complicated background the whole spine situation remains a much bigger challenge [ 7 ]  . 
therefore , a reliable and reproducible automated or semiautomated computerized method would be welcome to assist or augment the radiologists performance and reproducibility . literature review onsegmentation andclassification ofvcfs genant etal.s [ 8 ] proposal of a semiquantitative method for the evaluation of vertebral fractures related to osteoporosis , till date , is considered a gold standard for fracture classification which combines numerical classification with a visual inspection . 
authors of [ 9 ] concluded that a vertebral 1 3 la radiologia medica ( 2020 ) 125 : 551560 deformity does not always indicate a vertebral fracture , but that a vertebral fracture is always accompanied by the vertebral deformity . the segmentation of grayscale medical images has been extensively researched in the past decades . 
the random forest - based approach is proposed in [ 12 ] to segment vbs followed by a biomarker evaluation framework that extracts vertebral heights and widths from the segmentations obtained . 
in [ 13 ] , an automatic method is proposed based on iterative convolutional neural networks which utilized the inherent order of the vertebral column to train the network with as little as ten manual reference segmentations . 
a localization fcn found the bounding box of the lumbar region , and a segmentation fcn performed pixel - wise multi - class segmentation to map cropped lumber region volumetric data onto their volume - wise labels . 
furthermore , repeated heavy training processes may be required for the segmentation of different types of images ( e.g. , use of different contrasts , sequences or different mr scanners )  . 
of the 13 , 400 images generated , 12 , 700 are used for training and the remaining for testing with 100 images for each of the seven vertebra fracture classifications . 
an automated method is presented in [ 17 ] to detect spine compression fractures by first segmenting the spinal column and extracting the sagittal patches which are subsequently classified as binary using a convolutional neural network ( cnn )  . 
 using the median sagittal planes of lumbar spine mris in [ 18 ] , statistical features of gray levels , texture and shape are extracted to analyze the contours of the vbs from the manually segmented vbs . 
the k - nearest neighbor method , a neural network with radial basis functions and a nave bayes classifier are used with feature selection that resulted in an area under the receiver operating characteristic ( roc ) curve of 97% in distinguishing between normal and fractured vertebral bodies and 92% in discriminating between benign and malignant fractures . in the work of [ 3 ] using manually segmented vbs , the principal axis of each vb is identified using moments and then statistical features of height and width measured perpendicular and parallel to the principal axis are computed . 
the same set of classifiers as in [ 18 ] are used , which obtained roc accuracy of 96% in the recognition of vcfs as compared with normal vertebral bodies and 73% for the classification of benign versus malignant vcfs . 
a total of 17 contrast and texture features are extracted from manually segmented vbs in [ 19 ] , and the classification of malignant versus benign vcfs is performed using the k - nearest 1 3 554 la radiologia medica ( 2020 ) 125 : 551560 neighbor ( knn ) classifier ( k = 3 ) with the euclidean distance and tenfold cross - validation . 
this backdrop shows that there is still a need and scope for the development of automatic segmentation and classification methods , and we are proposing one in this paper . purpose ofthepresent study many of the reviewed studies have developed computeraided design ( cad ) systems to segment and classify vertebral fractures using imaging modalities based on ionizing radiations such as x - ray , dxa and more using ct . 
thus , the objective of this work is to develop digital image processing and pattern recognition techniques for the detection , labeling , segmentation and classification of vertebral bodies in lateral mri images of the lumbar spine . 
 the motivation for this work to use a mixture of texture and shape features to fulfill the objective is based on the typical and atypical nature of the appearance of benign and malignant fractures ( fig.2 ) and also inspired by the works in [ 3 , 5 , 18 , 19 ]  . 
the techniques used for detection , segmentation and labeling are based on morphological and shape features , whereas a blend of both shape and texture features is used for the classification of vcfs . 
the paper winds up with a conclusion along with proposals for probable extensions . methodology it is priorly known that images of malignant vertebral collapse typically exhibit low signal intensity throughout the entire vb involved in t1 - weighted mri . 
figure3 displays the workflow of the proposed method , and the subsequent subsections describe in detail detection , segmentation , labeling and classification procedures . detection the preprocessed image is applied with morphological operations with different structural elements . 
3 work flow of the proposed method 1 3 la radiologia medica ( 2020 ) 125 : 551560 this process , the detected objects are labeled in descending order of visual appearance , which results in the fifth lumbar vb being labeled as one and so on . 
from the illustration in fig.4b , it is evident that the line joining the successive centroids in the thoracic region is almost vertical , whereas the same in the lumbar region deviates significantly . 
to assist 1 3 556 la radiologia medica ( 2020 ) 125 : 551560 once all the conditions are examined , the labels are rechecked to see if they are consecutive . 
the objects from the resulting image are re - labeled once again in ascending order of appearance which fetches the final segmented output . classification each lumbar vb from the segmented output is considered for classification . 
the feature selection for this work is motivated by the works in [ 2 , 18 , 19 ] who have shown that a good mixture of shape and texture features produces better classification . 
the following are the shape features used in the current work . compactness ( cp ) is given in eq . ( 6 ) , with vb perimeter as p and area within perimeter as a . 
the subsequent subsections will describe the texture features used in this work . in statistical texture analysis , texture features are computed from the statistical distribution of observed combinations of intensities at specified positions relative to each other in the image . histogram of an image is the count of how many pixels in the image possess a given gray - level value . 
from the graylevel histogram of each vb , many statistical measurements of the first order and higher order are derived that well capture the differing properties of normal and fractured vbs . 
 statistical features used in this work are mean , variance , standard deviation , coefficient of variation , skewness and kurtosis . gray - level co - occurrence matrix ( glcm ) , also known as the gray - level spatial dependence matrix , is another statistical method suggested by haralick [ 21 ] to extract second - order statistics from an image by examining texture that considers the spatial relationship of pixels . 
contrast , correlation , energy , entropy and homogeneity are the statistics derived from glcm and are used here for classification . tamura features [ 22 ] are an approach that explores texture representation from a different angle since it is motivated by the psychological studies on human visual perception of textures and have huge potential in image representation . 
on a whole , 310 lumbar vertebral bodies are analyzed of which there are 102 vertebral bodies with vcfs , out of which 54 are benign ( osteoporosis ) and 48 are malignant ( bone metastasis ) vcfs , and the remaining are normal vertebral bodies . 
the rois ( lumbar vertebral bodies ) used in the present study represent the results of consensus between two observers . the segmentation performance is evaluated using leaveten - out cross - validation , where each time ten out of the 62 cases are sequentially taken out for testing and the remaining are taken in for training . 
for each case in test data , quantitative metrics such as accuracy , sensitivity , specificity and dsc are analyzed using eqs . ( 15 ) , ( 16 ) , ( 17 ) and ( 18 )  . 
it is a common phenomenon where the ( 15 ) ( 16 ) ( 17 ) ( 18 ) 1 3 558 la radiologia medica ( 2020 ) 125 : 551560 fractured or abnormal classes are fewer in number in contrast to the normal class . 
smote is an instance - based augmentation where the number of samples identified as belonging to minority class is sampled and doubled the previous count [ 25 ]  . after augmentation , the dataset now consists of 108 normal vbs and 204 fractured vbs of which 108 are benign fracture vbs and 96 are malignant fracture vbs . 
the augmented data were classified using support vector machine ( svm ) , and the performance of classification is evaluated using precision , recall and f - score using eqs . ( 19 ) , ( 20 ) and ( 21 )  . 
the shape features used in the present , i.e. , measures of width , length , area , axis lengths , perimeter , and distances from the centroid to boundary points of vb , relate well to the approach used by genant etal . 
the slightly higher percentage of dsc in [ 14 ] and [ 15 ] are due to factors like larger dataset , deep learning approaches and user - initialized points for a better start of segmentation . 
moreover , segmentation of the vb in this dataset has not been reported by any of the earlier works . as mentioned earlier , the distribution of the t1signal intensity over a vb is an important criterion to discriminate between normal and fractured vcfs in mri . 
5 classification evaluation measures using precision , recall and f - score using a only shape features ; b only texture features ; c both shape and texture features 1 3 la radiologia medica ( 2020 ) 125 : 551560 features , and the spatial distribution of low - intensity signals is characterized by the texture features . 
from the results shown in fig.5 , for combined features , it can be seen that the precision for normal vbs slightly increases , whereas there is a higher increase in accuracy and even greater increase in the recall rate . 
the mean classification accuracy of our work compared to the works of [ 3 , 5 , 18 , 19 ] using the same dataset can be rated the second highest . 
the overall results obtained indicate better performance for cad of compression fractures of vb . the limitations in our study are the usage of only the lumbar spine and the analysis being restricted only to the central sagittal plane which may cause some loss of information . conclusion the proposed segmentation and classification methods based on shape , texture and combined shape and texture features have honed the entire process providing high dsc and accuracy that may assist in the diagnosis of compression fractures of vb . 
complete remission ( n = 1 ) and partial remission ( n = 13 ) of local tumor were obtained in 14 patients , and the local tumor control rate was 87.5% ( 14 / 16 )  . 
the radiological - radiotherapeutic procedure could be an alternative tool in the case of refusing other treatments by the patients . keywords dysphagia esophageal stricture intraluminal radioactive treatment esophageal carcinoma introduction esophageal cancer often shows high rates of morbidity and mortality , and poor prognosis , because half of patients are unable to be resected at the time of diagnosis [ 1 , 2 ]  . 
these patients include those with a kamofsky score less than 60 , patients who are prone to stent migration due to severe cardiac curvature , patients with severe dyspnea due to airway compression after placement of esophageal stents , and cervical esophageal cancer with fear of foreign yonghua bi and xiaoyan zhu have contributed equally to this work and share co - first authors dreamweaver08@126.com * xinwei han * jianzhuang ren rrjjzzjrk@126.com 1 department ofinterventional radiology , the first affiliated hospital ofzhengzhou university , no . 
1 , east jian she road , zhengzhou450052 , china 2 department ofhistology andembryology , college ofbasic medicine , zhengzhou university , zhengzhou , china vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 544550 somatosensory sensation after stent placement , and so on . 
 in this study , a radioactive feeding tube was placed under fluoroscopic guidance , and a radioactive seed chain was placed across the occlusive segment of the esophagus for brachytherapy for the treatment for malignant obstruction caused by the esophageal cancer . 
we aimed to report the safety and effectiveness of the radioactive feeding tube in the palliation of esophageal malignant obstruction . materials andmethods patient selection this study was approved by the institutional ethics committee of our hospital . 
then , both ends of catheter were sealed off to form the 125i seed chaaccording to the length of the esophageal lesion , the two 125i seed chains were placed parallel to the gastrointestinal feeding tube . 
according to the length of esophageal lesions , two seed chains were placed parallel to the gastrointestinal feeding tube , fixed with tape , and then fixed on the feeding tube with surgical suture . 
 the seeds were fixed on both sides of the nasal feeding tube with a distance of 4mm and an angle of 180 . feeding tube insertion all procedures were performed under local anesthesia and fluoroscopic guidance with a floor - based flat panel angio system ( artis zeego , siemens healthineers , erlangen , germany )  . 
fluoroscopy 1 3 la radiologia medica ( 2020 ) 125 : 544550 confirmed that the proximal end of the nasogastric feeding tube was located in the jejunuat 35days after seed chain implantation , the patients received nasal feeding . observations anddefinitions baseline demographics such as age , gender , procedure time , comorbidities and tumor site were collected . 
procedure time was defined as the time required for the preoperative radioactive feeding tube to complete the placement of the seed chalocal tumor control was evaluated by the response evaluation criteria in solid tumors ( recist )  . 
neuhaus dysphagia grade , contrast medium patency and tumor local condition were evaluated during follow - up . statistical analysis continuous variables were shown as means standard deviation or median with interquartile ranges ( iqr )  . 
the median postoperative karnofsky score was 65.0 points ( iqr 60.070.0 ) , and neuhaus dysphagia score analysis showed grade 0 in six patients , grade i in eight patients , and grade ii in two patients . 
by the end of the follow - up period , six patients were taking food by mouth after pulling out the nasogastric feeding tube due to the improvement of symptoms . 
during the follow - up period , four patients have survived , one patient died of heart failure at 9.6months after the procedure , and 10 patients died of tumor progression at 1.147.8months , including the aforementioned two deaths . 
although the brachytherapy stent can achieve both symptom relief and a therapeutic effect [ 14 ] , it is not suitable for some special patients , such as those who tend to stent migration due to the curvature of the cardiac structure or who have severe dyspnea due to tracheal pressure after stent placement [ 10 ]  . 
we propose that it is possible to combine nasal feeding with brachytherapy to play a role of double carving with one stone . some researchers have begun to try to bind radioactive seeds to plastic tubes or drainage tubes to make seed chains and use them in the human cavity for short - range radiotherapy . 
insertion of seed chains has been successfully applied to bile duct obstruction [ 15 , 16 ] ; portal vein cancer thrombus [ 17 ] , and vena cava obstruction caused by tumor invasion [ 18 ] , and has achieved a good clinical effect . 
therefore , we speculated that the seed chain could be bound a nasal feeding tube for patients with advanced esophageal cancer who could not or refused to receive esophageal stents in order to achieve the dual objective of intraluminal brachytherapy for esophageal cancer and enteral nutrition . 
in addition , there is little space - occupying effect on the nasal feeding tube , and there is no need to worry about the occurrence of dyspnea caused by airway compression after esophageal stent placement , the massive bleeding caused by friction between the stent and the esophageal wall , or stent migration . 
the radioactive feeding tube can be adjusted or replaced easily if migration happens . postoperative ct showed that the local wall was reduced in varying degrees , but the local wall was still thickened . 
 gastroscopic biopsy showed that the tumor remained , and the following reasons were considered : in the early stage of implantation , the effect of brachytherapy was good because the seeds were close to the lesion , but with tumor shrinkage , the lumen enlarged and the tumor and the seeds were not close to each other , which might affect the curative effect . 
a threerow seed chain with an angle of 120 or a four - row seed chain with an angle of 90 may show a better therapeutic effect , but these seed chains require further clinical research . owing to the extra complexity of delivery compared with esophageal stents , brachytherapy may be insufficient to increase patient acceptance [ 19 ]  . 
 [ 14 ] found that patients who received esophageal stents loaded with radioactive iodine ( 125i ) seeds had prolonged overall survival compared to those who received conventional covered stents . 
it is a retrospective analysis of treatment for esophageal tumors with radioactive feeding tube in a single center and in a small series of patients ; the study is lacking comparison with other palliative treatments . 
whether long - term patients really benefit from survival , how many rows of seeds should be used for better efficacy , how to choose seed activity , and when to stop intracavitary radiotherapy remain to be solved , which requires more comparative randomized studies . in conclusion , the preparation of a radioactive feeding tube is simple and easy . 
data from a cohort of 40 patients with a reported clinical history suggestive for either disease , who had undergone at least their first imaging test related to their condition at the same institution , were entered into esr iguide . 
the appropriateness level of the diagnostic tests suggested by esr iguide was compared with that of the tests actually performed . results all patients underwent several imaging examinations , ranging from a minimum of 1 to a maximum of 4 , for a total of 98 diagnostic procedures . 
 although the benefits gained from the ongoing improvement of imaging techniques are undeniable , it remains unclear whether all the required tests may be justified for medical reasons or whether diagnostic imaging is being overused . 
 inappropriate imaging requests lead to several issues including longer waiting lists , inflated healthcare costs , and potentially worse patient outcome due to delayed diagnosis and / or improper treatment . 
 the cds system for european imaging referral guidelines , which derive from an adaptation of the american college of radiologists ( acr ) appropriateness criteria to european standards of practice [ 47 ]  . 
esr iguide is an online web portal that requires patient data as user input and accordingly displays which imaging tests are suggested together with their appropriateness level , estimated cost , and expected radiation exposure . 
two consultation options are available : indication - driven ( starting with clinical scenarios ) or procedure - driven ( starting with the diagnostic test that one may want to request ) [ 5 ]  . some studies have evaluated the effectiveness of cds systems in improving the diagnostic management of patients with various clinical conditions , showing that compared to cds - unassisted practice , their usage can result in an increased rate of appropriate examinations and a decreased rate of inappropriate examinations [ 810 ]  . 
however , to the best of our knowledge , there are no published works so far in the literature that have tested the performance of esr iguide in assisting diagnostic decision - making and potentially optimising healthcare resources . 
this would be especially important in an attempt to harmonise and improve disease management with a heavy individual and social impact that require a complex diagnostic and therapeutic approach , such as liver cancer [ 11 , 12 ]  . our aim was to evaluate how esr iguide could impact the diagnostic pathway of patients with hepatocellular carcinoma ( hcc ) and cholangiocarcinoma ( cc )  . specifically related to their disease condition at the same institution ( table1 )  . for each patient , all relevant data ( including patient age , gender , and clinical indication ) were entered into the esr iguide tool without selecting any imaging test ( indicationdriven mode )  . 
a p value less than 0.05 was set as threshold for statistical significance . results all patients underwent several imaging examinations , ranging from a minimum of 1 to a maximum of 4 , for a total of 98 diagnostic procedures ( table2 )  . 
on the other hand , of the 9 examinations performed and not suggested by esr iguide , 7 ( 77.8% ) were biopsies , 1 ( 11.1% ) colonoscopy , and 1 ( 11.1% ) gastroscopy , respectively . ultrasound ( us ) and ct had been performed in 33 and 31 patients , respectively , and were the most frequently table 1 distribution of patients clinical signs and symptoms clinical signs and symptoms # of patients ( % ) methods we retrospectively reviewed the medical records of 113 patients with a final diagnosis of hcc or cc ( either radiologically or pathologically proven ) , who had been referred to the oncology department of blinded from january 2013 to may 2017 at the beginning of their diagnostic pathway . 
among them , we analysed a cohort of 40 patients ( 35.4% ) with a reported clinical history of signs , symptoms and laboratory values suggestive for hcc or cc , who had undergone at least their first diagnostic imaging examination abdominal pain liver lesions on us hepatitis asthenia weight loss cirrhosis jaundice diarrhoea abnormal liver function tests nausea and / or vomiting 13 ( 32.5% ) 7 ( 17.5% ) 6 ( 15.0% ) 6 ( 15.0% ) 5 ( 12.5% ) 4 ( 10.0% ) 4 ( 10.0% ) 2 ( 5.0% ) 1 ( 2.5% ) 1 ( 2.5% ) 1 3 la radiologia medica ( 2020 ) 125 : 531537 performed diagnostic tests , making up together more than 65% of all imaging examinations . 
17 and 13 patients underwent biopsy and mri , respectively , and only one had abdominal x - ray , contrast enema , gastroscopy or colonoscopy . us was suggested as usually appropriate by esr iguide for all patients , but only 33 ( 82.5% ) went ahead with it . 
 conversely , abdominal ct was recommended as appropriate for 38 patients and correctly performed in 30 of them , with only one patient receiving abdominal ct although this latter had been classified as inappropriate by esr iguide . mri was suggested as usually appropriate in 37 patients and performed in 13 of them , whereas 3 other patients underwent mri although this latter received an appropriateness score lower than 7 . 
as to radiographic tests , one patient underwent abdominal x - ray ( which was suggested as appropriate in 15 cases ) , and one patient underwent barium contrast enema , a test that would have been considered as usually not appropriate by esr iguide . 
inappropriate testing leads to longer waiting lists , potential risks for patient health and medico - legal issues due to wrong or delayed diagnosis , and potential unnecessary exposure to ionising radiation . 
according to some studies , the reason for the increased demand for non - clinically justified tests could be identified in defensive medicine or in the use of medical imaging to reassure patients , despite there being no real suspicion of a disease [ 1315 ]  . the high costs and limited resources of healthcare systems justify the need for control tools aimed at an appropriate use of imaging . 
in the following years , many alternatives were developed in europe , such as the royal college of radiologists ( rcr ) irefer and the french guidelines [ 16 , 17 ]  . 
 moreover , the italian national agency for regional health services produced a text titled guidelines for diagnostic imaging in 2004 , which has not been updated since and among other issues , states that the radiologist can choose the best possible procedure for a given case [ 18 ]  . 
in this context , the european society of radiology introduced esr iguide in 2015 ( then updated in 2016 ) and started with pilot implementations in europe [ 4 , 7 ]  . in this study , we retrospectively evaluated the appropriateness level of imaging examinations performed in the diagnostic workup of 40 patients with hcc or cc , using the esr iguide appropriateness criteria as a reference . 
this is in line with current guidelines , for which the diagnostic algorithm for hcc and cc is mainly based on radiological imaging , whereas pathological confirmation is relegated to cases in which imaging alone cannot establish a diagnosis [ 19 , 20 ]  . mri was suggested as usually appropriate in a higher number of cases than it had actually been performed . 
however , mri has higher costs than ct or us , is more time - consuming , and is usually less readily available than ct or us ( resulting in longer waiting lists )  . 
 this could explain the lower number of mri examinations requested by referring physicians compared to those deemed as appropriate . us was performed in 33 patients only , but suggested for all patients by esr iguide . 
this was because the patients clinical conditions were suggestive of a neoplastic disease , and / or because patients had reached the emergency room in acute conditions and ct had eventually been considered more appropriate than us . 
on the other hand , ct was indicated by the esr iguide in 38 patients but performed in only 30 of them , since in the remaining 8 cases diagnosis had been reached using mri before ct . the examinations that were found to be inappropriate in our study were performed not as first test , but as further steps of the diagnostic pathway . 
as a matter of fact , currently esr iguide does not allow entering data collected after the patients diagnostic workup has begun , and in our opinion , this circumstance might deserve further investigation . 
it could also be hypothesised that the examinations 1 3 534 la radiologia medica ( 2020 ) 125 : 531537 1 3 la radiologia medica ( 2020 ) 125 : 531537 fig . 
b upon selection of jaundice as clinical indication , a list of candidate diagnostic tests is displayed , each with its appropriateness ranking , estimated cost , and expected radiation exposure ( relative radiation level , rrl )  . 
by clicking on display evidence , the user is directed to a portable document format ( pdf ) file containing the acr appropriateness criteria for the diagnostic management of jaundice and a summary of literature review ( supplementary material )  . 
c by clicking on the select this service tab ( related to us , abdomen in this example ) , a brief report with the appropriateness score of the selected test is generated that can be emailed or converted into a pdf file performed as third and fourth diagnostic tests did not play a decisive role for diagnosis , although they were useful for refining it . 
firstly , we based our analysis on the available data , but there may have been some relevant information missing in the medical history that could have better outlined patients clinical pathways , partly due to the current absence of a centralised electronic patient record system at our institution . 
this study aimed to quantify skull base morphometry and intracranial volume to investigate their relationships with the severity of scaphocephaly . methods we studied 66 infants with iss identifying three groups according to the morphological severity of cranial deformity ( group i : mild deformity ; group ii : moderate deformity ; group iii : severe deformity ) , by combining two scaphocephaly severity indices as descriptors of the relation of three morphological measurements ( length , width and height ) we perform a quantitative analysis using high - resolution ct images calculating following parameters : cranial fossae dimensions , supratentorial ( icv ) and infratentorial ( pcfv ) cranial volume , supratentorial ( wbv ) and infratentorial ( pcfbv ) brain volume , icv / wbv , pcfv / pcfbv , supratentorial and infratentorial cerebrospinal fluid ( csf )  . results in all subgroups , anterior and middle skull base lengths were increased , while posterior hemifossae lengths were unchanged . 
in particular , our study suggests that patients with severe deformity might have an earlier depletion of reserve mechanisms with a reduced compliance of the overall skull during encephalic growth and these patients might require early surgical cranial expansion . keywords high - resolution ct sagittal craniosynostosis scaphocephaly craniocephalic index vertico - longitudinal index * rosalinda calandrelli rosalinda.calandrelli@policlinicogemelli.it 1 polo scienze delle immagini , di laboratorio ed infettivologiche , area diagnostica perimmagini , universit cattolica del sacro cuore , fondazione policlinico universitario agostino gemelli , largo francesco vito 1 , 00168rome , italy 2 polo scienze dellinvecchiamento , neurologiche , ortopediche e della testa - collo , area neuroscienze , universit cattolica del sacro cuore , fondazione policlinico universitario agostino gemelli , rome , italy introduction sagittal synostosis is the most common form of isolated suture synostosis with an incidence of approximately 1 in 5000 and a 4 : 1 male - to - female ratio , accounting for 40 to 60% of single suture synostoses [ 14 ]  . the fusion of the sagittal suture can be located in the anterior or posterior region of the sagittal suture or can affect the entire cranial suture [ 5 ]  . 
moreover , the sagittal synostosis may progress along the sagittal arch involving the metopic suture ( major suture ) and / or the minor sutures of the skull base ( ethmoido - frontal sutures ) [ 6 , 7 ]  . the diagnostic phenotype in isolated sagittal synostosis ( iss ) is characterized by a dysmorphic craniofacial complex . 
 the cranial dysmorphism exhibits antero - posteriorly expanded vol . : ( 0123456789 ) 1 3 586 la radiologia medica ( 2020 ) 125 : 585594 neurocranium ( dolichocephaly ) with increased prominence of the forehead and occiput , variable bony ridging over the sagittal suture ( scaphocephaly ) , biparietal and bitemporal narrowing and increased head circumference [ 8 ]  . 
these skull changes reflect the compensatory growth perpendicular to the fused sagittal synostosis [ 3 , 9 ]  . in particular , the skull changes mainly occur at the sutures lying in close proximity to the synostosed sagittal suture ( coronal and lambdoidal sutures ) even if minor sutures at the skull base , such as the sphenopetrosal , sphenosquamosal and sphenofrontal sutures may be subjected to compensatory changes [ 10 ]  . the degree of suture fusion , severity of head shape deformity and additional changes such as frontal and occipital bossing and biparietal narrowing can vary significantly among affected individuals [ 2 ]  . some reports described that the distinct morphologies of the neurocranium reflect the site of initial synostosis , whether anterior or posterior or central , the timing of premature synostosis and the synostotic involvement of other sutures of the sagittal arch [ 9 , 11 ]  . 
other reports , based on clinical and preoperative computed tomography ( ct ) scan assessment , related the different abnormal head shapes to typical closure pattern of sagittal suture and correlated the length of synostosis with the severity of skull deformity [ 12 ]  . 
moreover , other studies quantified the degree of severity of scaphocephalic skull form measuring a set of cranial indices by using different plane and internal landmarks [ 2 ]  . 
these cephalic indices described the relation of two morphological measurements ( length and width ) , but they do not fully account for the overall abnormal head shape because skulls height is not considered . on the other hand , a few studies have previously considered intracranial volume as a measure of iss severity , but the comparisons between intracranial volumes ( icvs ) in patients with sagittal synostosis and healthy patients have given variable results , leading to questions regarding the validity of the normal reference material and the comparability of the measurement techniques [ 1317 ]  . the aims of our study were : ( 1 ) identifying the degree of premature synostosis of sagittal suture and its extension to the other sutures of the sagittal arch ; ( 2 ) developing a novel approach to accurately classify the severity of iss by combining two indices as descriptors of the relationship of three morphological measurements ( length , width and height ) ; ( 3 ) relating the severity of iss with skull volume and morphometry . materials andmethods study population we retrospectively reviewed multiplanar high - resolution 3d - ct images of 66 infants with iss consecutively admitted to our hospital between 2015 and 2017 ( 13 females and 53 males ; mean age 124.86 days , range 76194 days )  . 
all patients underwent a phosphor - calcic biology test to rule out metabolic disorders and bone deformities ( none of them showed alterations )  . three groups of infants were identified by combining the scaphocephalic ( ssi - a ) and vertico - longitudinal ( vli ) indices as descriptors of the relation between length , width and height ( group i : infants with mild deformity ; group ii : infants with moderate deformity ; group iii : infants with severe deformity )  . sixty - four age - matched healthy subjects ( mean age 125.22days , range 94180days ) who underwent ct examinations for minor craniofacial trauma were enrolled as controls . 
the study was approved by the local institutional review board . ct scan ct scans were performed using a ge light speed pro 64 system ( ge medical system , milwaukee , wi , usa ) equipped with an automatic tube current modulation technique called the automa technique for low - dose scanning . 
scanning was performed under spontaneous sleeping after feeding in all infants . the levels of radiation exposure ( dlp ) were between 420 and 550mgy * cm ; these levels are a good balance to visualize the skull base minor sutures and brain . analysis ofthesutural pattern axial and coronal high - resolution slices implemented with 3d - ct reconstructions were used to determine the status of each suture along the sagittal arch and to exclude the involvement of sutures of the other sutural arches . 
sagittal suture was divided into three sections based on anatomical location ( anteriorcentralposterior ) , and each section was scored as fused ( f ) or patent ( p )  . 
infants with a completely fused sagittal suture were coded as fff ( anterior , central and posterior sections fused ) ; infants whose suture was partially fused were coded as fpp , pfp , pff , ffp , ppf , fpf , according to the synostotic status of each section of the suture . 
if the metopic suture was fused , the presence of synostosis was determined by the presence of a metopic notch which is an omega - shaped or w - shaped 1 3 la radiologia medica ( 2020 ) 125 : 585594 notching of the endocranial ridge ; otherwise , in the presence of metopic spur , the metopic suture was considered physiologically closed [ 18 ]  . 
infants with metopic suture synostosis were not included in the study ( table1 )  . quantitative analysis skull shape quantification ct images implemented by three conventional orthogonal reformatted viewports of the skull were used to compute the scaphocephaly severity index ( ssi ) in the a plane and the respective vertico - longitudinal index . 
we used this plane because of the greater accuracy for quantifying the severity of sagittal synostosis [ 2 ]  . ssi in the a plane with a lateral view of a 3d reformation of the skull , a skull base plane was determined by using the frontal nasal suture anteriorly and the opisthion ( the middle point on the posterior margin of the foramen magnum of the occipital bone of the skull ) posteriorly . 
the ratio cranial width to the cranial lengthx100 was performed to define the scaphocephaly severity index ( ssi ) in the a plane . vertical - longitudinal index ( vli ) represents the ratio of cranial height and cranial lengthx100 . 
 it is composed of the sagittal suture ( white arrow in c : patent suture ; black arrow in h : synostotic suture ) metopic suture ( white arrow in d : patent suture ; black arrow in i : metopic spur in physiologically close suture ) , and the ethmoido - frontal * sutures ( white and black arrows in e , l patent sutures )  . 
n 2 completely fused incompletely fused patent metopic notch metopic spur < 33% from 33 to 66% > 66% percentages of sagittal synostosis fn : frontonasal ; fm : frontomaxillar fig . 
ssi in the a plane : ( b ) with a lateral view of a 3d reformation of the skull , a skull base plane was determined by using the frontal nasal suture anteriorly and the opisthion posteriorly ( red dot line in a )  . 
the cranial height represents the distance between the basion ( ba ) and the bregma ( br ) morphology in hyperdolichocephalic ( < 66% ) and dolichocephalic ( 6677% ) , while concerning the vertico - longitudinal index , we divided skull morphology considering percentage of vertical growth either below < 78% or between 78 and 85% [ 2 , 10 , 19 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 585594 a score system was developed assigning 1 point or 2 points as following : 2 points for values < 66% and < 78% and 1 point for values between 6677 and 7885% in ssi - a and vli , respectively . 
the overall score was calculated by the sum , and it was used to classify our patients according to the severity of head shape on a 4 - point ordinal scale ( 2 = mild , 3 = moderate , 4 = severe )  . morphometric and volumetric data were assessed and related to skull deformity severity . skull base morphometry on 3d - ct images , an endocranial view was used to place several landmarks to measure the skull base and hemifossae . 
the skull base was divided into two hemibases using an anatomic median line traced from the anterior edge of the crista galli for the acf ( c ) to the center of the sella turcica for the mcf ( s ) and to the opisthion for the pcf ( o )  . 
the symmetry of the hemibases and the lengths of the acf ( cx ) , mcf ( xm ) and pcf ( mo ) on each side were measured and expressed in centimeters . 
the landmarks for lengths were the anterior edge of the crista galli ( c ) , the xiphoid of the lesser wing of the sphenoid ( x ) , the internal acoustic meatus ( m ) and the opisthion ( o ) [ 20 ]  . 
the measurements were performed twice by the same examiner in two different sittings . supratentorial intracranial volume ( icv ) included the entire supratentorial intracranial cavity calculated after defining the start slice just above the plane extending from the tentorium to the posterior petroclinoid ligaments and the end slice just beneath the vertex of the skull . 
the interface between the inner table of the skull and the surface of the brain was outlined in every slice . supratentorial whole brain volume ( wbv ) was defined as the brain tissue volume contained within the icv . 
landmarks : c = anterior edge of the crista galli ; s = centre of the sella turcica ; o = opisthion ; x = xiphoid of the lesser wing ; and m = internal acoustic meatus . 
cx , xm and mo lengths are measured on each side and represent the size of the anterior cranial fossa ( cx ) , the middle cranial fossa ( xm ) and the posterior cranial fossa ( mo )  . 
the cso^ angle is measured on each side and corresponds to the total of the csx^ angle ( anterior cranial fossa ) , xsm^ angle ( middle cranial fossa ) and mso^ angle ( posterior cranial fossa )  . 
cs and so lengths are measured on the middle plane 1 3 590 la radiologia medica ( 2020 ) 125 : 585594 pcf brain volume ( pcfbv ) was defined as the volume of the neural structures contained within the pcf . 
because of the skewed data distribution , kruskalwallis test followed by post hoc mannwhitney u test was performed to compare data from different groups . spearmans correlation was used to analyze the correlation between synostosis extension and ssi and between synostosis extension and vli . statistical significance was set at p < 0.05. 
supratentorial intracranial volume ( icv ) is shown in red shaded areas ( a and b ) ; it includes the entire supratentorial intracranial cavity from the plane extending from the tentorium to the posterior petroclinoid ligaments to the vertex of the skull . 
pcf volume ( pcfv ) is represented in blue shared areas ( d and e ) ; it was defined as the anatomical area from the plane extending from the tentorium to the posterior petroclinoid ligaments to the foramen magnu pcf brain volume ( pcfbv ) is represented in purple shared area ( f ) ; it was defined as the volume of the neural structures contained within the pcf . 
in particular , middle hemifossae lengths ( xm ) were increased in all groups , anterior hemifossae lengths ( cx ) were increased in mild and moderate groups ( p < 0.05 ) , while posterior hemifossae lengths ( mo ) were unchanged . in the mild group , icv / wbv was significantly different and icv , wbv and csf supratentorial volume increased . 
in moderate and severe groups , fcpv / fcpbv was found significantly different and csf infratentorial volume reduced ; fcpbv was found increased only in the severe group ( table3 )  . discussion the premature fusion of sagittal suture is accompanied by compensatory growth of the skull parallel to the fused suture rendering the skull long and narrow in shape [ 21 ] , and the assessment of head shape deformity severity is useful in understanding the pathogenesis and clinical course of these patients . previous clinical studies usually evaluated the cephalic index at the skull vault ( ci ) and scaphocephaly severity indices ( ssis ) computed ( 1 ) just above the top of the lateral ventricles ( a plane ) , ( 2 ) at the foramina of monroe ( f - plane ) and ( 3 ) at the level of the maximal dimension of the fourth ventricle ( m - plane ) to describe the shape variation in the head [ 2 , 10 ]  . 
these indices described the two - dimensional ratio of maximum breadth and maximum length , only addressing the dolichocephalic component of the skull , but the three - dimensional head shape was not taken into account [ 22 ]  . 
in particular , the reduction in posterior skull height accompanying several presentations of scaphocephaly has been seldom described in this condition [ 23 ] and this may explain the lack of correlation between the above scaphocephaly severity indices and the measurements of intracranial volume previously reported [ 24 ]  . the first step of the present study was to analyze the early synostotic involvement along the four sutural arches in order to correctly identify infants with isolated sagittal craniosynostosis ( iss )  . 
moreover , a correlation between sagittal synostosis extension and two cephalic indices ( vli and ssi ) was performed . in case of metopic suture fusion , the presence of a metopic spur contributed to identification of infant with iss . 
we encountered a wide range of variability in terms of extension ( sagittal synostosis ratio ) and location of the synostosis ( anterior , central , posterior ) , but the central section involvement was always present . 
these data were in accordance with previous studies reporting that the central part of the sagittal suture fuses first , followed by fusion of either the anterior or the posterior section [ 25 ]  . we did not find a correlation between synostosis extension and our cephalic indices ( vli and ssi )  . 
cx = crista gallixiphoid of the lesser wing of the sphenoid length ; xm = xiphoid of the lesser wing of the sphenoidinternal acoustic meatus length ; mo = internal acoustic meatusopisthion length effect on skull shape [ 27 , 28 ]  . 
we did not perform a longitudinal study about the time course of sagittal progressive synostosis ; consequently , we are not able to know whether the deformity gets worse over time or it may remain stable as previously suggested [ 29 ]  . the second step of our study was to develop a novel approach to accurately assess the severity of the overall skull deformity in iss patients . 
our method combines two indices ( ssi and vli in the a plane ) as descriptors of the relation of three morphological measurements ( length , width and height )  . 
according to these two indices , three groups of infants were detected ( mild , moderate and severe ) considering to the degree of skull shape deformity . the third step was to perform a morphometric analysis of the skull base and a volumetric analysis of the skull in these groups of infants in order to investigate the relationship between the morpho - volumetric skull changes and the severity of the head shape deformity . 
 these studies are barely comparable for several methods differences such as the age and the sample size of the studied patients , methods of evaluation , characteristics of control groups but , above all , the lack of the threedimensional assessment of the head deformity [ 22 , 30 ]  . the age range for our infants was from 2 to 6months ; they were classified in three groups considering the three morphological measurements ( length , width and height ) , and they were compared with an age - matched control group . in all groups , we found symmetry of the anterior , middle and posterior cranial fossae along with the increase in the anterior and middle length of the skull base ( cs ) ; in particular , middle fossae were increased in all subgroups , while anterior fossae were increased only in mild and moderate groups . 
it suggests an impact of calvarial remodeling on the anterior and middle skull base , probably because the central section of the sagittal suture seems to be the first to fuse ; moreover , in the severe group , the minor elongation of the skull base might be related to the earlier timing of sutural synostosis with consequent early depletion of compensatory mechanisms . 1 3 la radiologia medica ( 2020 ) 125 : 585594 in all groups , we analyzed the supratentorial and infratentorial intracranial volumes . 
concerning the supratentorial volume , our analysis showed that , in mild group , icv / wbv ratio was different and the volumes of intracranial compartments ( icv , wbv and cerebrospinal fluid space volume ) were increased compared with controls ; on the other hand , in the moderate and severe groups , supratentorial cranial volumes were not significantly different from those of normal children . 
probably , it is due to the effects of the compensatory changes accompanying the sagittal suture synostosis with consequent different compliances of the supratentorial volume ; timing of the sagittal suture prenatal synostosis might play a key role in this phenomenon . 
in particular , an earlier closure of sagittal suture may cause a ceiling effect of compensatory mechanism over the time , while this compensatory process may be still active when a later closure of sagittal suture happens ; consequently , infants with mild shape deformity have larger volumes . concerning the infratentorial volume , in all groups , we found a normal fcpv , but in moderate and severe groups , fcpv / fcpbv and csf infratentorial volume were significantly reduced ; fcpbv was found significantly increased only in the severe group . 
because in moderate and severe groups , fcpv was normal , but fcpv / fcpbv was reduced , this suggests an increase in the brain tissue volume contained in the bony pcf and the reduction in infratentorial csf supports this hypothesis . 
previous studies reported postero - inferior shift of the brainstem associated with a vertical orientation of the tentorium cerebelli suggesting a reduction in the pcf volume [ 31 ]  . 
in particular , in moderate and severe groups , we suppose a reduced compliance of the skull during encephalic growth and supratentorial cranial volume does not allow to contain the cerebral growth with secondary downward of brainstem ; the significant increase in fcpbv in severe group compared with moderate group confirms that this mechanism is more pronounced in severe group . conclusion this study provides new insights in understanding the compensatory changes that occur in patients with different degrees of iss severity . 
classifying patients according to the three morphological measurements ( length , width and height ) enhances our understandings of the pathophysiological mechanisms determining skull growth and may provide useful information in the setting of the preoperative evaluation . 
in particular , our study suggests that patients belonging to the severe group have an earlier depletion of reserve mechanisms with a reduced compliance of the overall skull during the encephalic growth and this might require early surgical cranial expansion procedure . authors contribution rc is responsible for project development , data collection and manuscript writing . 
cc contributed to project development and manuscript writing . funding no funding was received for this study . compliance with ethical standards conflict of interest rosalinda calandrelli , fabio pilato , luca massimi and marco panfili declare that they have no conflict of interest . 
all patients complained of radicular pain with or without neck pain ; diagnosis of contained cervical disc herniation was obtained by mri ; all patients had received conservative therapy which did not result in symptom improvement . 
exclusion from our series consisted of patients who had undergone previous surgery at the indicated level , or those with myelopathy , or those in whom more than a sole herniation was treated in the same session . 
indeed , pain originating from intervertebral disc pathology is difficult to manage and is costly to healthcare organizations in western countries [ 1 ]  . in these patients , pain syndromes and deficits may arise as a combination of both ischaemia and inflammation and may be related to the mechanical compression of the nerve root * anna maria ierardi amierardi@yahoo.it 1 diagnostic andinterventional radiology department , asst santi paolo e carlo , san paolo hospital , university ofmilan , via a di rudin 8 , 20142milan , italy 2 radiology department , santanna university hospital , via aldo moro 8 , 44124ferrara , italy 3 department ofmorphology , surgery andexperimental medicine , university offerrara , via l . 
ariosto 35 , 44121ferrara , italy 4 radiology department , asst sette laghi , university ofinsubria , varse , italy 5 department ofbiomedical anddental sciences andmorphofunctional imaging , university ofmessina , messina , italy 6 department ofneuroradiology ( f.t. ) , fondazione irccs ca granda , ospedale maggiore policlinico , milan , italy 7 unit operativa di radiologia , fondazione irccs ca granda , ospedale maggiore policlinico , milan , italy vol . : ( 0123456789 ) 1 3 570 la radiologia medica ( 2020 ) 125 : 569577 by the portion of the extruded disc , accompanying inflammatory response and released chemical mediators [ 2 , 3 ]  . when conservative treatment fails and symptoms persist or worsen , surgical treatment is considered . 
in recent years , the trend towards minimally invasive spine surgery is the result of a diverse combination of factors including the aim to reduce perioperative complications and post - operative recovery time , the development and refinement of new technologies and patient awareness of emerging therapeutic approaches [ 4 ]  . a discrete number of minimally invasive methods for treating cervical hernias through devices inserted percutaneously into the intervertebral space and subsequent disc decompression has been developed , most commonly involving mechanical or energy - based removal of some portion of the nucleus pulposus , used in the therapy of small - tomedium - sized hernias of intervertebral discs [ 5 ]  . 
in each case , indications and contraindications to the procedure were evaluated on the basis of the cirse guidelines [ 9 ]  . before the intervention , all patients received conservative therapy ( including physical therapy combined with anti - inflammatory drugs and muscle relaxants at the manufacturers recommended therapeutic dose for no less than 68weeks ) , which did not result in symptom improvement . absolute contraindications were : sequestered disc fragment ; spondylolisthesis ; stenosis of the spinal canal ; asymptomatic intervertebral disc bulging incidentally discovered at computed tomography or mr imaging ; untreated , ongoing active infection and / or discitis ; and pregnancy . relative contraindications were as follows : coagulopathy ( to be corrected before the procedure ) ; anticoagulant therapy ( to be interrupted before the operation ) ; and severe degenerative disc pathology ( more than two - thirds in disc height decrease )  . table 1 details of the patient characteristics of each treatment group percutaneous discectomy ( group a ) percutaneous nucleoplasty ( group b ) total of patients males females level of disc herniation c3c4 c4c5 c5c6 c6c7 1 3 la radiologia medica ( 2020 ) 125 : 569577 patients who had undergone previous surgery at the indicated level , or those with myelopathy , or those in whom more than a sole herniation was treated in the same session were excluded from our series . procedure andpostoperative evaluation all the procedures were performed in our angiographic suite ( ge - innova 2100 - iq , ge healthcare , usa ) by two interventional radiologists with more than 10years of experience in percutaneous techniques . 
in each case , the operator has chosen the technique employed on the basis of his confidence with the procedure . the patient was placed in a supine position with the neck slightly extended ; the shoulders were gently held in a downward position with tape or a soft strap . 
local anaesthesia at the needle entrance site was achieved with subcutaneous injection of a 10 - ml solution of lidocaine , to monitor any changes in symptoms . firm pressure was digitally applied to the space between the right sternocleidomastoid muscle and the trachea and directed towards the targeted intervertebral disc space . 
void number , duration and ablation intensity were all adjusted according to the size and hardness of the herniated disc . conversely , in the pcd group , a manual discectomy was carried out introducing a probe ( diskom percutaneous discectomy probe , biopsybell , mirandola , italy ) into the cannula of the needle . 
after switching off , the device could be removed . in both the treatment groups , the estimated removed disc material was approximately 1ml . all patients were monitored during the operation , and ecg , blood pressure and oxygen saturation were measured . overall procedure time , fluoroscopy time and radiation dose administered were recorded . the overall procedure time was registered as the time from the patient positioning on the angiographic bed and the end of the procedure itself ( output of the patient from the angiographic suite )  . 
the radiation dose was expressed in terms of dose area product ( dap , gy * cm2 )  . complications were classified into major and minor according to the cirse classification system [ 9 ]  . pre - operative antibiotic prophylaxis with a cephalosporin was administered . 
1 a , b lateral c - arm fluoroscopic image obtained to deploy the needle into the disc to be treated ( a ) ; anteroposterior view is used only to check the correct position of the tip of the needle ( b ) 1 3 la radiologia medica ( 2020 ) 125 : 569577 572 fig . 
2 a , b pcn ( percutaneous nucleoplasty ) : fluoroscopic lateral view after the removal of the stylet ( a ) and the insertion of the coblation catheter into the introducer needle ( b ) fig . 
the correlation of mri findings with patient satisfaction is shown in table3 . students t - test in comparison with fisher exact test was used to evaluate the correlation between overall clinical outcomes at 2 and 6months ( graded by modified macnab criteria ) and treatment choice ( pcn or pcd )  . a p value < 0.05 was considered statistically significant . 
in neurologically stable patients , conservative treatment is widely accepted as the first - line therapeutic option , with pain relief and substantial reduction in disability reported in about 40% of cases [ 12 ]  . 
early surgical treatment is nowadays mostly fostered in patients presenting with progressive neurological symptoms or clinical signs of myelopathy [ 13 ]  . when conservative management fails , with symptom persistence or worsening , surgery may be considered . 
 [ 14 ] have successfully demonstrated that symptom duration is a key determinant of surgical outcome , and patients treated within the first 6months from clinical onset have a more satisfactory improvement in symptoms . nevertheless , there is no clear established consensus , either on general management or on the most appropriate timing to resort to elective surgery [ 13 ] , and decision - making is often based on the experience of the individual physician and local production volume . table 2 clinical outcome in terms of patient satisfaction at 2 and 6months in the two treatment groups percutaneous discectomy percutaneous nucleoplasty ( group a ) ( group b ) excellent good fair / poor excellent good fair / poor macnab at 2months macnab at 6months excellent good fair / poor 1 3 la radiologia medica ( 2020 ) 125 : 569577 574 fig . 
5 boxplot graph showing clinical outcomes in terms of patient satisfaction evaluated by the macnab score at 6months after the minimally invasive procedures table 3 correlation of clinical success with mri findings in patients who had received imaging follow - up percutaneous discectomy ( group a ) percutaneous nucleoplasty ( group b ) macnab at 46months macnab at 46months excellent good fair / poor excellent good fair / poor post - operative mri findings disc herniation regression ( complete or partial ) persistent disc herniation open surgical treatments range from conventional anterior discectomy and fusion to artificial disc replacement , with the former remaining the most commonly performed procedure in single - level cervical disc herniations [ 15 ]  . 
 because of poor general performance status or comorbidities , not all patients are considered eligible for an open approach , and , even if good candidates , they may refuse the intervention . 
moreover , surgery invariably entails the risk of peri - operative complications , which must always be considered in the assessment of the riskbenefit ratio . given the need to bridge the gap between non - operative treatments and open invasive procedures , the current trend 1 3 la radiologia medica ( 2020 ) 125 : 569577 of evolution in spinal surgery has been towards patient - tailored techniques and reduction in surgical - related trauma ; in recent years , a variety of imaging - guided percutaneous minimally invasive approaches have been proposed for the treatment of discogenic pain and radiculopathy - related disability , with the aim to obtain disc decompression . 
 [ 16 ] have verified the biomechanical changes behind the clinical success of percutaneous discectomy : the authors found that the removal of a certain amount of nucleus pulposus material , though increasing radial bulge , unequally results in the reduction in disc height and internal pressure , thereby postulating the pivotal role of tension decline in symptom improvement . the ideal selection criteria for percutaneous approach include small - to - medium - sized hernias and symptomatic single - level contained cervical disc herniation with negligible disc degeneration [ 17 ]  . 
contraindications are represented by segmental instability , sequestered or calcified disc , prominent osteophytes , severe degenerative disc disease , discitis , neural foramen or spinal canal stenosis , malignancy , previous disc surgery at the same level , impaired coagulation and pregnancy [ 17 ]  . mechanical , thermal and chemical decompression , together with biomaterial implantation techniques , is currently employed . 
in the last decade , a discrete number of validation studies have been published on individual techniques [ 17 ]  . our results showed no significant statistical difference in mean modified macnab score at 2 and 6months among patients grouped by treatment choice . 
average success rates , visual analog scale ( vas ) evaluation of pain relief , neck disability index values and overall patient satisfaction are indeed mostly solid and concordant for all percutaneous approaches [ 18 ]  . 
in 2010 , a randomized controlled trial ( rct ) by cesaroni and nardi [ 19 ] demonstrated that percutaneously treated patients exhibited better outcomes at 1 - year follow - up compared to the conservative control arin 2011 , the rct by erginousakis etal . 
conversely , in 2017 , a review of the literature and meta - analysis by epstein [ 21 ] found no significant difference in the reported outcome after laser discectomy and thermo - annulo - nucleoplasty techniques compared with non - surgical treatment . 
 other than that , percutaneous techniques are safe and costeffective , allowing outpatient surgery under local anaesthesia [ 22 ]  . in our series , we retrospectively compared two different percutaneous techniques : percutaneous cervical nucleoplasty ( pcn ) and percutaneous cervical discectomy ( pcd )  . 
pcn is a percutaneous disc decompression technique based on coblation technology : a bipolar probe delivers radiofrequency energy , generating a plasma field of ionized particles inside the disc nucleus . 
furthermore , coagulation and contraction of the collagen reticulum occurs . instead , pcd relies on opening a window through the outer fibrous ring of the herniated disc and removing nucleus fragments by suction . 
different systems for mechanical removal of disc material have been employed in some series , mainly in the lumbar spine , including the use of spiral tips [ 23 ]  . pcd and pcn have been extensively employed and evaluated both in lumbar and cervical radiculopathy treatment . 
moreover , among patients who received an mri reassessment , imaging features were concordant with patient perception of outcome . we have demonstrated that both pcn and pcd are safe approaches . 
in the literature , percutaneous decompression is associated with infrequent and mild complications ; nonetheless , even minimally invasive procedures , like pcd and pcn , entail the potential risk of complications [ 9 ]  . 
in our series , until the last follow - up check , there has been no concerning event or undesired periprocedural symptoms . 1 3 576 la radiologia medica ( 2020 ) 125 : 569577 in addition to the retrospective single - centre nature of our study , some limitations merit consideration . 
larger patient cohorts and randomized clinical studies are required to define the clinical benefits of one technology over the other , and with open surgical treatment in terms of safety and patient outcomes . conclusion pcd and pcn are both minimally invasive procedures , which have proven to be safe and effective in terms of pain relief in contained cervical herniation treatment . 
in our cohort , no differences were observed between the techniques regarding clinical outcome and complications at 2and 6 - month clinical follow - up . funding the authors received no specific funding for this work . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
in particular , four findings were considered : ( 1 ) bone marrow oedema ; ( 2 ) reactive phenomena ( perilesional inflammatory reaction for extra - articular lesions or synovial reaction for intra - articular lesions ) ; ( 3 ) bone remodelling ( disappearance of the nidus and bone healing ) ; ( 4 ) ring sign ( considered as the granulation tissue around the nidus treated )  . 
these findings were evaluated using mri and ct with a follow - up study that lasted up to 24months . keywords osteoid osteoma mrgfus rfa bone ablation ablation follow - up interventional radiology introduction osteoid osteoma ( oo ) is a benign bone tumour that account for about 1012% of all benign bone lesions and 23% of all primary bone tumours [ 1 ]  . 
typically it occurs in the first two decades of life ( 75% of cases between 5 and 25years old ) and it affects mainly men ( male female ratio 3 : 1 )  . 
 osteoid osteomas are usually extra - articularly ; intra - articular lesions are less common ( 1012% ) [ 3 , 4 ]  . imaging is usually typical : a radiolucent central nidus , which may display a variable amount of mineralization , * francesco arrigoni arrigoni.francesco@gmail.com 1 department ofemergency andinterventional radiology , san salvatore hospital , laquila , italy 2 department ofbiotechnological andapplied clinical sciences , university oflaquila , laquila , italy 3 department ofoncological orthopaedics , ifo - regina elena national cancer institute , rome , italy surrounded by cortical thickening and / or reactive sclerosis [ 5 , 6 ]  . clinically it is painful : the pain , caused by prostaglandins released by the nidus [ 7 ] , increases intensity during the night and relieved by non - steroidal anti - inflammatory drugs ( nsaids ) particularly salicylates [ 1 ]  . 
 mini invasive treatments ( in particular , percutaneous computed tomography ( ct ) - guided radio frequency ablation ( rfa ) [ 11 ] ) , and magnetic resonance - guided focused ultrasound ablation ( mrgfus ) [ 12 , 13 ] have become the gold standard techniques for management of this lesion . 
multiple studies [ 14 , 15 ] have investigated and confirmed effectiveness , safety and low invasiveness of these treatments ; anyway , the results are based mainly on clinical data [ 16 , 17 ]  . 
on the other hand , only few studies describe the evolution of the imaging features of the treated lesions along the follow - up [ 18 , 19 ] , generally using contrast - enhanced mri sequences and usually with an observational aithe aim of our study is instead to looking for some characteristic vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 578584 diagnostic findings that characterize the imaging at the diagnosis and that change along the follow - up ( up to 24months ) after radiofrequency ablation ( rfa ) or magnetic resonance - guided focused ultrasound ( mrgfus ) treatment . 
 the knowledge of these features and their evolution over time in fact could be of particular interest in order to confirm the minimally invasive nature of the procedures and in order to detect the best time of follow - up in case of suspicion of a treatment failure . materials andmethods we have retrospectively analysed , through a second reading , the imaging outcome of the follow - up of successfully minimally invasive treatments ( rfa and mrgfus ) of osteoid osteoma . of all the patients treated and followed in our hospital , we selected only case that followed these inclusion criteria : 1 . 
treatment , for whom there was not a complete report of any clinical and imaging data before and after . for each treatment we review any clinical and imaging data acquired before and after treatment . about clinical data a 010 visual analogue scale ( vas ) was used to assess pain symptomatology . instrumental evaluations were based on mri and ct scans . 
the preprocedural imaging was not - standardized because patients have come from different diagnostic centres with their imaging ; however , each patient had an mri and ct examination of the pathological bone segment . 
ct scans ( aquilion one , toshiba , tokyo , japan ) were performed on the area of interest to limit radiation exposure , considering the young ages of patients . baseline imaging was considered the scans acquired before the procedure ( using both mri and ct scans )  . 
the follow - up were performed from 4 to 6months after treatment ( follow - up 1 , fu1 ) , from 9 to 12months ( follow - up 2 fu2 ) and from 18 to 24months ( follow - up 3 , fu3 ) after treatment . 
the fu1 consisted in mri examination only ; fu2 and fu3 consisted in mri and ct scans . prior of the examinations second lecture , two senior authors ( cm and ab ) with more than 25years of experience in musculoskeletal radiology , selected the four most representative imaging findings that , according to their experience but also to the literature [ 15 , 18 ] , usually characterize the preand post - procedural imaging of an osteoid osteoma correctly and successfully treated . 
1 reactive phenomena in intra - articular lesion : ct ( a ) and mri t2w image with fat saturation ( b ) : osteoid osteoma of the talus ( white arrow ) with synovial reaction ( arrowheads ) and bone oedema ( @ ) ; significant reduction of the bone oedema and synovitis ( arrowheads and @ , respectively ) 6months after treatment ( c ) ; they have a complete resolution at the 12months follow - up ( d ) fig . 
2 reactive phenomena in extra - articular lesion : ct ( a ) and mri t2w image with fat saturation ( b ) : osteoid osteoma of the lateral profile of the tibia ( white arrows ) with perilesional reaction ( arrowheads ) and bone oedema ( @ ) ; c 6months follow - up : they still remain a slight bone oedema and reactive phenomena ( arrowhead and @ , respectively ) results demographic data based on inclusion / exclusion criteria , we evaluated 34 patients affected by osteoid osteoma ( 23 male and 11 female ; mean ages 23years ) treated with radiofrequency ablation ( rfa ) or mrgfus ( respectively , 13 and 21 cases )  . the intra - articular lesions ( ia ) were 13 ; 21 were extraarticular ( ea ) lesions . 1 3 la radiologia medica ( 2020 ) 125 : 578584 fig . 
3 bone remodelling : ct osteoid osteoma of the anterior profile of the proximal femur ( white arrows ) ( a ) ; there are an initial sclerosis of the nidus at 12months follow - up and a complete re structuring and sclerosis of the bone at 24months follow - up , respectively , ( b ) and ( c ) fig . 
4 ring sign : ct ( a ) and mri t2w image with fat saturation ( b ) : osteoid osteoma of the anterior profile of the femoral neck ( white arrows ) ; 6 months follow - up ( b ) shows granulation tissue , identified as a central hypointense area surrounded by a peripheral hyperintense rim ( arrowheads )  . 
at fu1 , the vas score was 0 for all patients , and this value was confirmed in all the following checks ( fu2 and fu3 )  . imaging data all the results are summarized in table1 . at fu1 we noticed a remarkable reduction of all inflammatory phenomena ; the bone marrow oedema had been significantly reduced , both in the ia and ea lesions : in fact 9 patients ( 69% ) with an ia osteoma had a reduction of 6070% of the oedema , while 4 patients ( 31% ) had a complete resolution of this sign ; 18 patients ( 86% ) with an ea lesions had a reduction of 6070% of the oedema , while 3 patients ( 14% ) had a complete resolution of the oedema . 
 we also found that the synovitis disappeared in 7 patients ( 53% ) and was notably reduced in 6 patients ( 46% ) , while perilesional flogistics reaction was considerably reduced in 16 patients ( 76% ) and disappeared in 5 patients ( 24% )  . 
at the fu2 , we recorded a complete resolution of the bone marrow oedema and of the reactive phenomena in 95% of cases ; only 2 patients ( 15% ) with an ia osteoid osteoma still had signs of synovial inflammatory reaction . the bone remodelling , better assessable with ct , started to be clearly evident only at 12months : 4 patients ( 31% ) of the ia group and 5 patients ( 24% ) of the ea group showed a clear evidence of bone restructuring towards a bone healing . 
only the 15% of patients still showed an incomplete restructuring of the bone after two years of follow - up . the ring sign was the more difficult sign to assess because sometimes it was very slightly visible . 
a curative aim is required in order to kill the painful symptoms that compromise the daily activities of young patients . since we did not want to demonstrate the efficacy of the procedures , we have included only patients successfully treated in our unit , regardless of the type of treatment performed , both rfa and mrgfus : in fact both the treatments are heat - based procedure of thermal ablation and as previously demonstrated the choice of the most appropriate procedure to treat each lesion is based on the accessibility of the nidus [ 10 ]  . 
all the studies carried out so far have focused mainly on the evaluation of the effectiveness of the procedures , considering first of all the clinical outcome [ 21 , 22 ]  . 
clinical results in fact are the first data that correlate with the outcome of the treatment , since as shown in the literature [ 15 ] already the disappearance of pain some days after treatment can be indicative of therapeutic success . to our knowledge , however , imaging features of the post - procedural evolution of these procedures have not yet been systematically codified [ 15 , 23 ]  . 
moreover , we have looked for signs that are clearly 1 3 la radiologia medica ( 2020 ) 125 : 578584 visible on a basic imaging ( non - contrast - enhanced t1w and t2w mri sequences , also with fat saturation and ct ) because as in the daily practice , patients suffering for oo reach the reference hospital for treatment coming from different diagnostic centres with an imaging , already performed , that usually is enough for diagnosis and for planning treatment . so , in order to avoid repeating imaging ( as also contrast administration ) , in our study we have identified and reported four easy - to - find signs that prove the success of the procedure and we have schematically summarized : ( i ) disappearance of bone marrow oedema around the lesion , ( ii ) the reduction of perilesional flogistic / synovial reaction , ( iii ) the restructuring of the bone and ( iv ) the ring sign . the first two , in particular , suggest the absence of biological activity within the treated lesion : in fact bone oedema and perilesional flogistic / synovial reaction stand for the presence of flogistic environment that typically comes with an active osteoid osteoma . 
 on the other hand , because in no one patient these features were found as pre - treatment , the persistence of a comparable entity of bone oedema / flogistic reaction is strongly suggestive for an uncomplete treatment . 
one year after treatment , only in case of ia lesions is still possible to find flogistic reaction , however slight , also in patient successfully treated . the restructuring the bone defines the effectiveness of the procedures as also their mini - invasiveness that does not alter the structure of the bone allowing bone healing . 
 our experience , however , showed that it is needed to wait 12months after treatment to observe a clear evidence of in a statistically significant percentage of patients ( from 43% of ia lesions to 82% ea lesions )  . 
the central necrotic area of the ring is the result of the ablation , and the surrounding zone is the result of a sub - lethal thermal injury . therefore , identifying the ring sign around the lesion at the first follow - up means that there was a thermal insult within the pathological tissue . 
so , in our experience , the ring sign is present 6months after treatment and 1year after the procedures there is only a low evidence . about the type of instrumental method to be used , we assessed that mri is useful from the beginning because of its ability to identify all the reactive phenomena ( bone marrow oedema , synovitis and perilesional reaction ) , while the use of ct scan can be postponed to 1years control avoiding exposing young patients to excessive radiations . 
ct scan is useful to identify the bone remodelling up to the bone healing of the skeletal segment that we can found in the long - term follow - up . this study has some limitations . 
first the arbitrary choice of the four findings to investigate : we chose the reactive phenomena ( i and ii ) because they are usually present in an active and painful lesion . 
 however , the evaluation of the follow - up using these signs has a practical advantage in the clinical practice : only not contrast - enhanced sequences were used ( t2w with fat saturation sequences and t1w sequences are enough to evaluate the outcome of a treatment )  . 
another limit is represented by the date of follow - up that is not fixed but is intended as a period ( from 4 to 6 , from 9 to 12 and from 18 to 24months ) : this limitation is , however , difficult to overcome because patients successfully treated and so without pain , have usually a poor compliance to undergone to diagnostic examinations for follow - up . 
finally it lacks a differentiation between patient treated with rfa and those treated with mrgfus : this choice was made to avoid dispersing the data ; as the sample of patients followed will increase , a dedicated study will be performed . in conclusion , even if the follow - up of the minimally invasive treatment of osteoid osteoma is mainly clinical , the imaging follow - up can be useful in case of persistence of pain or clinical suspicion of recurrence . 
the best protocol to assess the effectiveness of the procedure should include an mri within the first 12months to assess the reduction and / or the disappearance of the flogistic reaction the always comes with the lesion ; after 12months a ct scan of the skeletal segment could be very useful to assess the bone remodelling and the bone healing with the disappearance of the lesion treated . acknowledgments authors wish to thank angela martella for translating the manuscript . funding this work has not been supported by any funding . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical standards all the clinical procedures described in the study were performed in accordance with the helsinki declaration and patients signed an informed consent . 1 3 584 la radiologia medica ( 2020 ) 125 : 578584 informed consent this article is a retrospective study . 
hospital administrations had to provide a prompt response to a rapidly evolving emergency characterized by the necessity of giving access to an enormous number of infected patients , guaranteeing appropriate care to patients in need of other types of treatment , and simultaneously preserving the well - being of healthcare providers . 
to optimize the diagnostic pathway during the current covid - 19 outbreak , the hospital administration of our tertiary center applied a highly structured framework assigning specific tasks to the different units composing the department of imaging . 
in particular , since the beginning of the pandemic , a mobile ct scanner in a truck was rented and became operative for all patients with a confirmed diagnosis of covid - 19 and another ct was assigned for all suspected cases . 
thus , according to the experience gained in our center , we recommend to all hospital administrations facing the covid - 19 outbreak to promptly adapt their resources , creating precise and safe pathways for their diagnostic units . keywords management covid - 19 radiology safety emergency the current covid - 19 outbreak represents a major challenge for all healthcare systems not only regarding the diagnostic and therapeutic processes but also in terms of global management of the delivered care [ 1 , 2 ]  . 
as shown for previous epidemics like sars , a structured approach to the radiological departments including the implementation of specific devices has a positive impact on the overall management of patients [ 4 ]  . in particular , during the current pandemic , attention had to be devoted in separating suspected from confirmed covid - 19 patients in need of urgent radiological imaging avoiding any possible contamination or delay in the provided care . 
especially regarding the last aspect , molecular tests which are , up to now , the main applied diagnostic vol . : ( 0123456789 ) 1 3 692 la radiologia medica ( 2020 ) 125 : 691694 tool , require some hours to be processed . 
in this interval of time , the clinical pathway of critical patients should not be interrupted and emergency rooms ( er ) should not be overcrowded . establishing proper pathways can be particularly challenging in large hospitals , as ours , acting usually as referring centers for numerous and various diseases . 
moreover , the ct of the academic radiological unit ( orange in the graph ) has been assigned for examining all suspected cases of covid - 19 ( i.e. , symptomatic or asymptomatic subjects at high risk of infection , waiting for the results of the molecular test and requiring urgent scans )  . in case of patients in critical conditions who cannot be transported to the truck , the ct of the academic unit is used and then properly disinfected and locked following the guidelines [ 5 ]  . 
all other cts of the hospital ( i.e. , green in the graph ) are used for non - covid - 19 patients , aiming to avoid any interruption of the routine clinical activity especially regarding surgical , oncological , and pediatric patients who require care that cannot be postponed . obviously , all patients who require an urgent ct scan but cannot be transported to any of the two assigned cts ( i.e. , mobile ct for confirmed cases , ct of the academic unit for suspected patients ) are examined in the nearest radiological unit and afterwards the ct room is carefully cleaned and disinfected [ 5 ]  . the success and efficacy of the management applied by our administration is demonstrated by the fact that during the outbreak , the radiological workflow was never interrupted . 
in fact , during the first month of the pandemic in the regione veneto , in our hospital , 1946 ct scans were performed , 69 of which using the mobile device ( i.e. , for covid - 19 - positive patients ) , and 539 with the academic scanner ( i.e. , for suspected covid - 19 , covid19 patients who could have not been transported to the truck , and non - covid - 19 patients referring to the academic unit )  . 
considering that the national lockdown led to a reduction of the deferrable surgical procedures and clinical assessments , and in turn of the prescribed radiological examinations , in our center , in comparison to the same interval of time of the previous year , only a 29.3% decrease of ct scans occurred . it certainly has to be noted that all covid - 19 patients are mainly monitored by chest x - rays and our hospital has 11 mobile x - ray devices which can be assigned for infected patients . 
nevertheless , in case of clinical conditions requiring ct scans , it is mandatory to assure that these examinations are safely performed [ 6 ]  . a further sign of the success of the applied method is represented by the evidence that according to the surveillance of healthcare providers belonging to the department of diagnostic imaging , up to now , none contracted the disease . 
he went immediately to quarantine and none else in his unit was affected . all healthcare providers of the department worked in safety , using the recommended protective equipment ( i.e. , surgical mask and gloves dealing with non - covid - 19 patients ; filtering masks , gloves , long sleeved gown , protective shoe covers , and eye protection dealing with suspected or positive covid - 19 patients ) [ 7 ]  . 
patients had to wear a mask , the safety distance of at least 2m was applied in all waiting rooms , caregivers had limited access , and everyone accessing the department was screened ( e.g. , temperature check , anamnesis focused on the main covid - 19 symptoms )  . as suggested in the recent article of mossa - basha etal . , the preparedness of hospitals is essential to face this dramatic situation [ 8 ]  . 
according to the experience gained in our center , we recommend to all hospital administrations facing the covid - 19 outbreak to promptly adapt their resources , creating precise and safe pathways for their diagnostic units . we strongly believe that only a precise organization of the workload , figuring out the designation of devices dedicated not only to confirmed covid - 19 cases but also to suspected patients , will provide a fully beneficial service for the entire healthcare system , assuring the best delivered care to all patients , guaranteeing the safety of the healthcare providers , and optimizing the economic resources . 1 3 la radiologia medica ( 2020 ) 125 : 691694 fig . 
all patients with a confirmed diagnosis of covid - 19 are scanned in a mobile ct scanner ( i.e. , represented in red ) , which is available since the early phase of the outbreak in our region . 
other units such as the women care center with patients in need of radiological examinations will follow the same pathway for suspected and confirmed covid - 19 patients and use the nearest ct room for covid19 - negative patients . 
clinicopathological ( cp ) data and preoperative ct scans , preand post - contrast medium ( cm ) administration , of 57 surgically treated nsclc patients , were retrospectively collected . 
after ct volumetric density measurement of primary gross tumour volume ( gtv ) , aorta and tracheal air , density correction was conducted on gtv ( reference values : aortic blood and tracheal air )  . 
cp and imaging data were correlated with patients 1 - , 3and 5 - year os , alone and combined ( uni - / multivariate logistic regression and akaike information criterion )  . 
after normalization resulted an improvement in predicting 1 - year os for some of the grey level size zonebased features ( large zone low grey level emphasis ) and for the combined cp - imaging model , a worse performance for grey level co - occurrence matrix ( cluster prominence and shade ) and first - order statistical ( range ) parameters for 1and 5 - year os , respectively . 
density corrections of volumetric ct data showed an opposite influence on the performance of imaging quantitative features in predicting os of surgically treated nsclc patients , even if no statistically significant for almost all predictors . keywords nsclc personalized medicine textural analysis radiomics correction methods biotechnology innovation * alessandra farchione alessandra.farchione@policlinicogemelli.it 1 dipartimento diagnostica perimmagini , radioterapia oncologica ed ematologia , fondazione policlinico universitario agostino gemelli irccs , largo agostino gemelli 8 , largo francesco vito 1 , 00168rome , italy 2 dipartimento universitario scienze radiologiche ed ematologiche , universit cattolica del sacro cuore , largo francesco vito 1 , 00168rome , italy 3 fondazione policlinico universitario agostino gemelli irccs , largo agostino gemelli 8 , largo francesco vito 1 , 00168rome , italy 4 dipartimento scienze cardiovascolari e toraciche , fondazione policlinico universitario agostino gemelli irccs , largo agostino gemelli 8 , largo francesco vito 1 , 00168rome , italy 5 uoc radiologia , ospedale g . 
mazzini , asl teramo , piazza italia , 64100teramo , italy 6 dipartimento di scienze cliniche e sperimentali , universit degli studi di brescia , c / o piazzale spedali civili 1 , 25123brescia , italy vol . : ( 0123456789 ) 1 3 626 introduction when dealing with cancer the evaluation of the patients prognosis is crucial in order to determine the most suitable therapeutic management [ 1 ]  . 
features derived from multiple disciplines are thus needed to characterize the single patient , as they differ among individuals with similar disease , in order to obtain a tailored treatment or the so - called personalized medicine [ 4 ]  . in the clinical setting of predicting lung cancer survival , during the last few years , multiple authors have demonstrated the usefulness of technological innovations represented by quantitative imaging tools as texture and radiomics analysis [ 5 , 6 ]  . 
in the context of texture analysis , medical images are described as a function of the pixel / voxel values and of their spatial distribution and relationships : multiple quantitative imaging features can be therefore mathematically extracted from clinical images [ 5 ]  . 
intuitively , those data are related to tumour structure and potentially contain prognostic information that can be integrated in multimodality models of treatments , as in the so - called radiomics process [ 4 ]  . many sources of variability can affect computed tomography ( ct ) lung density measurements in daily practice , related to both patients characteristics and image acquisition parameters , which can represent data noise and introduce discrepancies among measurements [ 7 , 8 ]  . 
 an attempt has been applied in the thoracic site with the quantitative assessment of emphysema , using a modified corrected threshold according to blood and air density [ 9 , 10 ]  . the aim of this study was to apply the above - described density correction method to the quantitative analysis of ct images of nsclc in patients candidate to surgery , with the purpose of determining its influence on the overall survival ( os ) prediction after resection . la radiologia medica ( 2020 ) 125 : 625635 materials andmethods patients andtumours patients affected by nsclc and surgically treated with curative intent at our hospital from january 2008 to august 2018 were retrospectively enrolled . inclusion criteria were : ( 1 ) pathological confirmation of nsclc ; ( 2 ) thoracic ct study before surgery and prior to any other treatment ; ( 2 ) same ct scan technical parameters ; ( 3 ) images of satisfactory quality and without significant artefacts . 
the pathological stage of nsclcs was defined according to the tumour , node and metastasis ( tnm ) staging classification system / american joint committee on cancer at the time of diagnosis ( 6th , 7th and 8th edition ) [ 1113 ]  . 
for post - contrast acquisitions , non - ionic contrast medium ( cm ) with a concentration of 370 mgi / ml ( ultravist , iopromide , bayer , milan , italy ) or 350 mgi / ml ( iomeron , iomeprol , bracco imaging , italy ) was administered intravenously with a dose of 90ml in the case of chest ct scans , 1.52ml / kg in the case of a total body acquisition . 
 cm was administered with a power injector ( medrad stellant dual head injector ; medrad , warrendale , pa , usa ) at an injection rate of 3ml / s , followed by saline flush injected at the same rate . 
the primary tumour segmentation , displayed both on axial and coronal planes , is represented in non - contrastenhanced ( a , b ) and contrast - enhanced images ( c , d )  . 
the corresponding three - dimensional roi , with and without the lung volume , is represented in ( e ) and ( f ) , respectively segmentation images were loaded on a radiotherapy delineation console ( eclipse , varian medical system ) for volume definition . 
in order to select and better define tumours margins , the lesions were at first evaluated and segmented on thinner section images ( 1.25mm ) , with bone reconstruction algorithm on both lung and mediastinum window settings ( width 1600 hu , level 600 hu and width 360 hu , level 60 hu , respectively )  . 
the defined region of interest ( roi ) was then applied and eventually adjusted on the corresponding thicker ( 2.5mm ) images with kernel standard to obtain the final area for analysis . 
for each examination , on both without and with contrast - enhanced images , three - dimensional ( 3d ) rois were segmented to define the following volumes : ( 1 ) gross tumour volume ( gtv ) , corresponding to the primary tumour ( figs.1 and 2 ) ; ( 2 ) trachea , including the tracheal lumen from a subglottic plane to the carina , since tracheal air correction method has shown better prognostic correlation in the literature ( fig.3 ) [ 9 ] ; ( 3 ) aorta , including the aorta lumen from a plane passing through higher medial diaphragm insertion to a plane through lower adrenal glands margin , since blood density value is more stable in the aorta below the diaphragm ( fig.4 ) [ 10 ]  . 
a further inner margin of 2mm to the tracheal and aortic wall was applied to avoid partial volume artefacts . density correction andfeatures extraction dicom files containing the images used for delineation and the voxel structures sets with contours coordinates were analysed using moddicom , a software developed in - house by a multidisciplinary group devoted to biotechnology innovation for cancer aid [ 14 ]  . normalized gtv density ( y ) was achieved from the original ct pixel density ( x ) using the following formula [ 9 ] : 1 3 628 la radiologia medica ( 2020 ) 125 : 625635 fig . 
the primary tumour segmentation , displayed both on axial and coronal planes , is represented in non - contrastenhanced ( a , b ) and contrast - enhanced images ( c , d )  . 
the figure shows the segmentation of the aorta on coronal reconstructions , in both non - contrast - enhanced ( a ) and contrast - enhanced images ( b ) , and the corresponding three - dimensional roi ( c )  . 
we therefore obtained four imaging sets : ( 1 ) without cm / non - normalized , ( 2 ) without cm / normalized , ( 3 ) with cm / non - normalized and ( 4 ) with cm / normalized . from each imaging set , first - order statistical ( intensitybased statistical and intensity histogram ) and textural ( grey level co - occurrence , grey level run length and grey level size zone ) features were extracted as previously described [ 15 , 16 ]  . 
the pearsons test was used to quantify the linear correlations between features , with a cut - off value of 0.3 , in order to eliminate redundancies and identify features independence . 
in order to make the most convenient choice , we considered the features capable to give a different ( nonrelated ) informative contribution in predicting clinical outcomes . receiving operator characteristic curve ( roc ) and area under the curve ( auc ) were used to evaluate models performance . 
 ( % ) 29 ( 51 ) 18 ( 32 ) 1 3 la radiologia medica ( 2020 ) 125 : 625635 table 2 univariate and multivariate analysis results with cm with cm without cm without cm features non - norm norm features non - norm norm p value p value auc value auc value p value p value auc value auc value delong test p value 1 year os delong test p value univariate analysis gender f_cm.clust. 
no statistically significant difference , however , has been demonstrated for any of the analysis when applying density correction . discussion in this study we applied a density correction method of lung ct scans based on air and blood densities , in order to reduce the variability affecting ct images acquisition and 1 3 la radiologia medica ( 2020 ) 125 : 625635 the derived imaging quantitative parameters when using texture analysis of nsclc . 
we observed an opposite influence of the normalization on the predictive performance of the imaging features alone or combined in multivariate models when used to predict os of surgically treated nsclc patients , even if no statistically significant for almost all quantifiers . in our study , among first - order statistical features 90th percentile and range were correlated with 3and 5 - year os , respectively . 
it could be supposed that a higher scale of density values inside a tumour is related to the presence of different tissue components and , therefore , to higher heterogeneity . 
the identified parameters were in the class of grey level co - occurrence matrix ( cluster shade and cluster prominence ) that describes how pixel / voxel grey levels are distributed along an image direction and of grey level size zonebased features ( large zone low grey level emphasisand zone size entropy ) that counts the number of groups of neighbouring pixel / voxel with the same grey level [ 15 ]  . 
intratumour heterogeneity is a known factor of poor prognosis , related to the cancer aggressive biology and to the existence of therapy - resistant subpopulations [ 3 , 18 , 19 ]  . 
moreover , textural parameters have been associated with angiogenesis and hypoxia in nsclc and further types of hallmarks of tumour heterogeneity related to irregularity in distribution of tumour vessels [ 20 ]  . 
an improvement in predicting 1 - year os has been observed after normalization for large zone low grey level emphasis , in the class grey level size zonebased features , and for the combined cp quantitative imaging features model . 
by the contrary , after density correction a worse performance was observed for grey level co - occurrence matrix and first - order statistical parameters in predicting 1and 5 - year os , respectively . 
heterogeneous density of neoplastic images is generally due to the co - existence of areas of viable and hypoxic / necrotic tissue , but in contrast - enhanced images the irregularity in the distribution of blood vessels can be better represented [ 20 ]  . in the last few years , texture analysis and radiomics research in ct have significantly increased , especially in the field of lung cancer in order to aid clinical care in numerous areas [ 46 ]  . 
one of the main advantages of these approaches is the availability of large amounts of retrospective data derived from medical images acquired for standard clinical diagnostic [ 8 ]  . 
in order to overcome the variation in density depending on the level of the thorax and related to the beam - hardening effect , we calculated both air and blood attenuation values on a 3d volume and segmented the aorta below the diaphragm as previous authors [ 10 , 27 ]  . in order to minimize the variability in texture analysis relative to technical issues , in this study we used the machines from the same ct vendors , similar ct versions and the same imaging parameters both for acquisition and reconstruction . 
 specifically thin slice thickness and a smooth reconstruction algorithm were considered for this analysis , as they were demonstrated to be the most favourable parameters to ensure the reproducibility of extracted quantitative features [ 31 , 34 ]  . 
 thicker slices have reduced noise levels , but at the same time the reduced spatial resolution and the larger partial volume effect can blur the images and reduce texture details [ 31 , 34 ]  . 
segmentation was conducted by using a semi - automatic system ( computer - aided edge detection followed by manual curation ) , as it resulted to be the more reproducible one according to the literature data [ 7 , 38 ]  . 
however , the 1 3 634 la radiologia medica ( 2020 ) 125 : 625635 primary aim of our study was not to create a predictive model for survival , already existing in the literature , but to test the effect of density correction on the performance of quantitative radiological features . 
we did not take into account the effects of haemoglobin or haematocrit levels on blood density correction : as blood is one of the main constituents in the lung , such variations could affect the lung density measurements [ 10 ]  . 
moreover , we did not test the influence of the inspiration level that , even with breathing instructions during ct scanning , may variably influence quantitative assessment [ 8 ]  . 
however , when conducting multi - centre studies with high amount of data or when comparing results from different authors , technical parameter is variable ; therefore , it will be interesting to test this correction method against ct data from different machines , imaging parameters and software system analysis . in the era of personalized medicine , many studies demonstrated the potential of radiomics analysis in clinical application . 
however , the lack of standardization , or at least the correlation among imaging features acquired in different settings , reduces their clinical strength and applicability , as well as the comparability among different experiences . 
the applied system in our study , nevertheless , showed an opposite influence on the performance of imaging quantitative features in predicting os of surgically treated nsclc patients and , moreover , with no statistical significance for almost all predictors . 
an alternative useful tool could be the application of filtration methods to the ct textural analysis of lung cancer , in order to decrease high - frequency noise and enhance features at different spatial scales [ 8 , 20 , 39 ] , or the use of standardized technical protocols in case of prospective studies . acknowledgements the authors thank luca boldrini for his advice on revision of the manuscript . funding the research did not receive any specific grant from funding agencies in the public , commercial or not - for - profit sectors . compliance with ethical standards conflict of interest the authors declare that they have no funding or conflict of interest regarding this study . ethical approval the study is part of an institutional review boardapproved protocol . 
all the procedures performed in this study involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
radiation exposure ( dose area product [ dap ] , air kerma ( ak ) and fluoroscopy time [ ft ] ) , technical success , clinical success , complications and survival were analyzed . results in total , 29 patients had cpvt and 20 patients had pc . 
tips was successfully placed in 94% ( 46 / 49 ) of patients via a transjugular approach alone ( n = 40 ) , a transjugular / transhepatic approach ( n = 5 ) and a transjugular / transsplenic approach ( n = 1 )  . 
overall survival rate was 75% . conclusion in our experience , the use of real - time ultrasound guidance allowed the majority of the tips to be performed via a transjugular approach alone with a reasonably low radiation exposure considering the high technical difficulties of the selected cohort of patients with cvpt or pc . keywords ascites bleeding liver cirrhosis * roberto miraglia rmiraglia@ismett.edu 1 radiology service , department ofdiagnostic andtherapeutic services , mediterranean institute fortransplantation andadvanced specialized therapies ( irccs - ismett ) , via ernesto tricomi , 5 , 90127palermo , pa , italy 2 medical imaging department , mater dei hospital , msida , 3 department ofmedicine dimed , radiology institute , malta padua , italy 4 hepatology unit , mediterranean institute fortransplantation andadvanced specialized therapies ( irccs - ismett ) , palermo , italy introduction transjugular intrahepatic portosystemic shunt ( tips ) is a well - established procedure for the treatment of cirrhotic and non - cirrhotic patients with complications of portal hypertension such as variceal bleeding and refractory ascites [ 1 ] and is considered to be one of the most complex and radiation intensive procedures in abdominal interventional radiology [ 2 ]  . 
the presence of complete portal vein thrombosis ( cpvt ) or portal cavernoma ( pc ) , previously considered as relative or absolute contraindications to tips creation , increases technical difficulties of tips creation . 
as familiarity with this procedure grows , an increasing number of these patients have undergone successful shunt placement , with technical success reported between 75% and 98% vol . : ( 0123456789 ) 1 3 610 la radiologia medica ( 2020 ) 125 : 609617 of cases in centers with high experience [ 37 ]  . 
the data available regarding patient radiation exposure during tips creation are sparse , and a few series with a large number of procedures are available [ 2 , 810 ]  . 
data reported in those series are based , however , on all tips creation , including a majority of patients with a patent portal system , and are not focused on patients with cpvt and / or pc . 
our aim was to quantify tips - related patient radiation exposure in our center in patients with cpvt or pc using real - time ultrasound guidance for portal vein targeting ; technical success , clinical success and complication rates were also evaluated . materials andmethods this single center retrospective study was reviewed and approved by the institutional research review board , and informed consent form was waived . 
 no financial support has been provided for this study . from july 1999 to september 2018 , 787 tips creations were performed in the radiology unit of a single transplant center . 
 between august 2009 and september 2018 , at our institution a total of 459 patients underwent tips creation and insertion of an e - ptfe - covered endoprosthesis ( viatorr ; w.l.gore & associates , inc . , flagstaff , az , usa ) for complications of portal hypertension using real - time ultrasound guidance for portal vein targeting . 
cpvt was defined as complete occlusion of the main portal vein , with or without involvement of intrahepatic portal branches on contrastenhanced computed tomography and / or magnetic resonance imaging performed within 1month before tips creation ; pc was defined as the presence of tortuous hepatopetal collateral veins that bypassed the occluded portal vein for the patent intrahepatic segmental vessels with the replacement of the original main portal vein with a fibrotic cord on contrastenhanced computed tomography and / or magnetic resonance imaging performed within 1month before tips creation . 
in cases of failure of portal system catheterization using real - time ultrasound guidance , a combined ultrasound - guided transhepatictransjugular [ 1315 ] or transsplenictransjugular [ 16 , 17 ] approach was used as previously described . 
following portal system catheterization , direct portography was performed , followed by portosystemic pressure gradient ( psg ) measurement , defined as the difference between the portal pressure and inferior vena caval pressure [ 18 ]  . 
dilatation of the intrahepatic tract and portal vein was performed with a 10 - mm non - compliant balloon catheter ( mustang ; boston scientific , galway , ireland ) ; subsequently , a viatorr endoprosthesis ( viatorr ; w.l.gore & associates , inc . , flagstaff , az , usa ) was deployed , followed by 10 - mm - diameter balloon dilatation . 
 all patients were followed up in the outpatient clinic with clinical , biochemical and doppler ultrasound evaluation , initially at 1month after tips , then at 3months , and every 6months thereafter . 
tips was revised in case of recurrent variceal bleeding , continued need for paracentesis without the evidence of he for more than 3months post - tips creation , and in cases of doppler findings of tips dysfunction . 
 doppler us criteria for tips dysfunction included portal flow velocity lower than 30cm / s , change in the direction of flow in the intrahepatic portal branches from hepatofugal to hepatopetal , intra - stent flow velocity lower than 60 or higher than 190cm / s or intra - stent flow velocity gradient greater than 50% [ 19 ]  . dosimetric data for every tips procedure were systematically archived into our radiology information system ( ris ) and picture archiving and communication system ( pacs ) ( centricity ris 4.2i , general electric medical systems , usa )  . 
for every procedure , the dose area product ( dap ) given in gy * cm2 , air kerma ( ak ) given in gy and fluoroscopy time ( ft ) given in minutes were retrospectively documented . 
dap ( or kerma area product ) was considered as a surrogate measurement of the entire amount of energy delivered to the patient by the radiation beam during the procedure and is the quantity recommended by the international commission on radiation units to measure patient doses in interventional radiology [ 20 ]  . 
it is measured at the interventional reference point ( irp ) defined as a point that is 15cm closer to the focal spot than the system isocenter around which the gantry rotates . 
the society of interventional radiologycardiovascular and interventional radiology society of europe ( sircirse ) international guideline on patient radiation management states that fluoroscopy time should not be used to monitor patient irradiation during interventional procedures ; however , fluoroscopy time might provide an indication of procedure complexity , even though it does not always correlate with other dose metrics [ 22 , 23 ]  . procedures were performed in an angiographic suite with an image intensifier - based digital system ( advantax , general electric medical systems , usa ) during the period before july 2010 . 
procedures performed after july 1 3 612 la radiologia medica ( 2020 ) 125 : 609617 2010 were performed in a flat - panel - based detector angiographic suite ( innova 4100 , general electric medical systems , usa )  . 
this equipment allows operators to choose from five different trajectories , each one using a different nominal dose ( 100 , 90 , 70 , 50 and 35% , respectively ) , three different frame rates ( 30 , 15 and 7.5frame / s ) and two different image detail levels ( normal and low )  . 
most tips procedures were performed with the detector in the posteroanterior projection with no cranio - caudal or oblique tilting ; however , these maneuvers were at times required in a few of the more complex procedures . 
this , coupled with the enhanced detective quantum efficiency of the detector , lowers the receptor entrance dose levels and produces enhanced image contrast at the expense of increased noise . 
it has been previously reported that this technique results in a mean reduction of 75% in dap per image when compared to a default reference standard dose acquisition protocol used during tips creation [ 24 ]  . 
fluoroscopy protocols were optimized in each systethe automatic exposure control system , designed to automatically determine the optimal technique parameters such as kv , mas , focal spot size and spectral filtration , was used in both systems . 
the last image hold feature , which displays the last active fluoroscopic image , was always used since this enables image capture without additional fluoroscopic exposure . results our study cohort consisted of 49 patients . 
forty - one out of 49 patients were cirrhotic . twenty - nine patients ( 60% ) had radiological evidence of cpvt ; of these patients , 5 had concomitant complete intrahepatic portal vein thrombosis , 18 had concomitant partial intrahepatic portal vein thrombosis , and 6 had patent intrahepatic portal branches . twenty patients ( 40% ) had pc ; of these patients , 10 had concomitant intrahepatic cavernoma . primary indications for tips insertion were prevention of recurrent episodes of gastroesophageal variceal bleeding in patients who had failed endoscopic and / or medical therapy ( n = 14 ) , uncontrollable variceal bleeding ( n = 2 ) and refractory ascites or refractory hydrothorax ( n = 25 )  . 
 eight patients underwent tips on the basis of portal system thrombosis alone , unresponsive to anticoagulant therapy , in order to recanalize the portal vein and maintain transplant waiting list status . 
five patients had previous liver transplantation , 3 of whom received whole liver transplantation , while the remaining 2 patients underwent partial liver transplant ( right lobe graft )  . tips was successfully created in 46 out of 49 patients ( 94% ) with a transjugular approach alone ( n = 40 ) , a transjugular / transhepatic approach ( n = 5 ) and a transjugular / transsplenic approach ( n = 1 )  . 
no deterministic or stochastic radiation - related complications were observed in our study group . in 3 patients , we were not able to successfully create a tips : 2 patients had cpvt and 1 patient had pc . 
a single stent was deployed in 29 out of 46 patients ( 63% ) , and two coaxial stents were deployed in the remaining 17 patients ( 37% )  . 
clinical results are summarized in table3 . discussion as expected , radiation exposure in our cohort of patients varied according to the complexity of the procedure , with a wide range in dap , ak and ft . 
 [ 9 ] reported 211 tips performed using real - time ultrasound guidance for portal vein targeting a 75th percentile dap of 150gy * cm2 and a 75th percentile ft of 25.7min ; more recently , bundy etal . 
 [ 10 ] reported la radiologia medica ( 2020 ) 125 : 609617 in 120 tips a 75th percentile dap of 609gy * cm2 and a 75th percentile ft of 63.7mdata reported in those series are based , however , on all tips creation , including a majority of patients with a patent portal system , and are not focused on patients with cpvt and / or pc . 
to the best of our knowledge , our study is the first single - center survey reporting data on patient radiation exposure during tips creation in patients with cpvt and / or pc . 
 [ 10 ] in their general population of patients undergoing tips creation ; this result could be due to the systematic use of real - time ultrasound guidance used for portal vein targeting . 
of note , in this case series of tips creation in patients with cpvt or pc , a transjugular approach , with real - time ultrasound guidance for portal vein targeting , was used in the majority of cases , reserving the more complex transhepatic or transsplenic approaches for only a few cases , thus further decreasing patient radiation dose . the ak median and 75th percentile levels recorded in this study are relatively low when given the complexity of the procedures being performed . 
in fact , none of the patients suffered any deterministic or stochastic radiation - related complications during the follow - up period . these data are particularly relevant since tips is being increasingly performed in patients with cpvt and / or pc . 
 complete and extensive thrombosis may exclude patients from transplantation or require complex surgical techniques associated with a high risk of morbidity and mortality [ 26 , 27 ] ; for this reason , recently , tips creation has been recommended in liver transplant candidates who have progressive portal vein thrombosis refractory to anticoagulation therapy [ 6 ]  . 
report a systematic use of the transsplenic approach with 5 cases of hemoperitoneum ( 8% ) , 3 of which were secondary to the splenic access , and one case ( 2% ) of radiation skin burn . 
notably , the clinical results obtained in our cohort showed tips creation to be effective not only in patients with previous bleeding but also in patients with refractory ascites with results similar 1 3 la radiologia medica ( 2020 ) 125 : 609617 fig . 
ac mdct , portal venous phase , showing mild ascites , splenomegaly , large gastroesophageal varices , complete thrombosis of intrahepatic portal branches ( ) and main portal vein up till the spleno - mesenteric confluence ( not shown )  . 
f portography performed after portal system catheterization shows complete thrombosis of the intrahepatic portal branches and main portal ve of note , there is reverse flow in the splenic vein and a large patent coronary vein filling gastroesophageal varices . 
g portography after 10 - mm - diameter e - ptfe - covered stent placement shows good flow in the stent , reduced filling of the coronary vein , no reverse flow in the splenic vein and mild residual filling defect in the main portal vein in keeping with partial residual thrombosis ( )  . 
 this can be easily demonstrated by reviewing the methodology described in recent tips - related publications , with many centers still advocating the use of other techniques [ 3038 ]  . the limitations of our study include the lack of accurate risk estimation for stochastic effects , since these should be quantified using the patient - specific monte carlo simulation . 
another limitation is that the number of procedures analyzed is relatively low ; however , the majority of the tips - related dosimetric studies available were performed with different cohorts of patients with a patent portal systeall procedures were performed by 3 faculty level radiologists with several years of experience in tips creation , with a potential impact on fluoroscopy time . conclusion tips creation in patients with cpvt and / or pc is technically challenging and radiation intensive ; however , high technical and clinical success can be achieved in procedures performed by experienced operators . 
real - time sonographic guidance to target the portal venous system can be helpful to obtain technical success via a transjugular approach alone in majority of cases with a reasonably low radiation exposure considering the high technical difficulties of the selected cohort of patients , reserving the more complex transhepatic or transsplenic approaches only for few cases . 1 3 616 la radiologia medica ( 2020 ) 125 : 609617 fig . 
a combined percutaneous transhepatic / transjugular approach was performed to recanalize the portal vein remnant ( cf ) and successfully deploy an e - ptfe - covered stent ( g , h )  . 
radiol med 2020 ; 125 : 155156 antoniobrillantino1 francescaiacobellis2 alfonsoreginelli3 adolforenzi4 robertograssi3 received : 12 february 2020 / accepted : 19 february 2020 / published online : 5 march 2020 italian society of medical radiology 2020 abstract in the preoperative work - up of patients with anorectal fistulas , 3d - eaus may represent the first - line diagnostic tool , showing high diagnostic accuracy in the evaluation of internal openings , primary tracks and secondary extension . 
in the cases of fistulas classified as complex by 3d - eaus , mri may be indicated as adjunctive diagnostic imaging examination , to more accurately detect the fistulas secondary extensions , and so , to more carefully describe the fistulas complete anatomy . keywords 3d - eaus endoanal ultrasound magnetic resonance imaging anal fistula perianal sepsis to the editor , we read with interest the comments of mathew etal . 
to our study [ 1 ] , and we would like to clarify some points . endoanal ultrasound ( eaus ) , which we employed since the 1990s , represents a consolidated diagnostic tool in the study of perianal sepsis [ 2 ] , with equipment , technique , indications and tolerability very different from trans - rectal ultrasound for the study of the prostate . if compared with trans - rectal one , eaus represents a less invasive examination , due to the inferior size of the * francesca iacobellis iacobellisf@gmail.com 1 department ofsurgery , a . 
vanvitelli , piazza miraglia 2 , 80138naples , italy 4 department ofsurgery , buon consiglio fatebenefratelli hospital , via manzoni 220 , 80123naples , italy dedicated probe and the maximum depth reached that slightly exceeds the puborectal sling . furthermore , three - dimensional ( 3d ) eaus , when employed for the study of anal incontinence and perianal sepsis , requires a lower execution time than trans - rectal ultrasound for urologic purpose , allowing an automatic 3d anorectal scan in about 60s , without any biopsy . patients with perianal sepsis commonly report perianal and not endoanal pain , so they well tolerate a simple digital rectal exploration as well as eaus , differently from patients with prostatitis which often report intense pain at the introduction of the explorer finger only . 
in the rarer cases of patients with endoanal pain from intersphincteric abscesses , the execution celerity and the routine use of the anesthetic gel make the eaus examination always feasible . 
in our experience , the only limit to the employment of eaus is represented by anal canal stenosis that is a very rare condition in patients with perianal sepsis . three - dimensional endoanal ultrasound has high diagnostic power in the evaluation of perianal sepsis . in our previous study [ 3 ] , the sensitivity , specificity and limits of 3d - eaus were already investigated and reported , as well as the concordance between 3d - eaus and surgery in recognizing the intersphincteric or transsphincteric tracts vol . : ( 0123456789 ) 1 3 696 la radiologia medica ( 2020 ) 125 : 695696 with favorable results for 3d - eaus . 
particularly , 3d - eaus showed high sensitivity and specificity in the diagnosis of sepsis of anorectal source and good diagnostic accuracy in the detection of internal openings , primary and secondary tracts , with the main limitations in the identification of pelvirectal abscesses and supraelevator tracts . magnetic resonance imaging ( mri ) has undoubted advantages as soft tissue contrast , operator independence , multiplanar capabilities and excellent field of view , but it is burdened by higher costs , longer execution time and lower availability [ 1 , 4 , 5 ]  . in the more recent study [ 1 ] , we compared the diagnostic performance of 3d - eaus with mri in the study of perianal sepsis , showing comparable sensitivity and specificity in the evaluation of fistulas internal openings and primary tracks , and significantly higher accuracy of mri in the evaluation of secondary extensions in cases of complex fistulas . 
this pictorial review attempts to provide insights to interpret the radiological appearances of the craniocervical junction on conventional radiography , computed tomography and magnetic resonance imaging in relation to various musculoskeletal disease processes . keywords cervical spine atlantoaxial joint odontoid process magnetic resonance imaging computed tomography introduction the craniovertebral junction is an extremely complex joint composed of occiput , atlas , odontoid process and ligamentous support structures . 
it includes nerve structures , including the medulla , spinal cord and lower cranial nerves , whose proper protection is essential for survival . the joint is involved in several musculoskeletal diseases ( msds ) , whose symptomatic interpretation is a challenge for rheumatologists , while imaging this small structure continues to be a challenge for radiologists . magnetic resonance imaging ( mri ) is the technique of choice for assessing changes in the craniovertebral junction . 
computerized tomography ( ct ) ( with multislice , spiral or helical and 3d reconstructions ) on the other hand is an excellent and sometimes better technique than mri in characterizing the presence of bone alterations . 
orsola - malpighi , bologna , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 654667 allows craniometric measurements to be made that are not possible with radiography . knowledge of the complex anatomy , of morphological changes due to pathological processes , of the relationships of the odontoid process with other structures , integrated with the clinical background , can provide significant diagnoses since complications ( e.g. , subluxations or dislocations , fractures of the odontoid process ) at this level can be lethal [ 13 ]  . the involvement ofcraniocervical junction inrheumatoid arthritis rheumatoid arthritis ( ra ) is the most common chronic inflammatory disease , affecting 0.5% of the population [ 4 ] ( table1 )  . 
according to some case studies , cervical spine involvement is second in frequency , varying between 25 and 88% in patients with long - term ra [ 3 , 58 ]  . 
the inflammatory process of synovial tissue leads to progressive ligamentous laxity and progressive damage to cartilage and bone structures , resulting in instability and possible subluxation of the odontoid process . 
ra concerns both the upper cervical structures ( c1 and c2 , with the atlantoaxial , atlantoodontoid and atlantooccipital joints ) and the subaxial cervical spine [ 7 ]  . 
 atlantoaxial instability defines different types of morphological alterations , where anterior atlantoaxial subluxation ( aas ) is the most common presentation , followed by lateral aas ( about 20% of cases ) , and posterior aas ( about 7% of cases ) [ 8 ]  . 
anterior aas is diagnosed when the anterior atlantoodontoid interval ( aadi ) , measured from the posterior face of the anterior arc of c1 to the anterior face of the odontoid process , is greater than 3m posterior aas occurs when the anterior arc of the atlas has shifted to the odontoid process . 
atlantoaxial canal stenosis is recognized when the posterior dental interval ( padi ) , measured from the posterior face of the odontoid process to the anterior face of the c1 lamina , is less than 14mhow reliable these craniometric measurements are in fact remains a controversial and debated issue [ 11 , 12 ]  . 
in some cases , atlantoaxial instability may progress in the vertical migration of the odontoid process into the cranial cavity ( also known as vertical subluxation or basic invagination ) [ 7 , 13 ]  . 
in very table 1 comparative features of rheumatoid arthritis , ankylosing spondylitis and psoriatic arthritis rheumatoid arthritis ankylosing spondylitis psoriatic arthritis male / female ratio onset ( age , years ) prevalence general population ( % ) 0.46 peripheral involvement 2550 symmetrical , polyarthritis typical joints involved wrists , metacarpophalangeal hip , knee joints , proximal interphalangeal joints 1535 0.37 uncommon , asymmetrical oligoarthritis 3335 0.42 asymmetrical / symmetrical oligoarthritis / polyarthritis distal interphalangeal joints enthesitis dactylitis axial involvement not a feature not a feature atlantoaxial joint involvement , no typical feature uncommon sacroiliitis and spondylitis pretypical feature typical feature of active disease sacroiliitis and spondylitis present dominant features in 40% of patients dermatologic manifestations rheumatoid nodules , vasculitis not typical spondylitis ( uncommon ) radiography ( peripheral joints ) erosion ( distal interphalangeal erosion , periarticular osteoporosis coxitis , bone formation ( shaft various features of psoriasis ( plague , guttate , pustular , erythroderma , nail disease ) periostitis ) joints , pencil - in - cup lesions ) , new bone formation ( shaft periostitis , ankylosis ) radiography ( axis ) atlantoaxial subluxation bilateral sacroiliitis , vertebral bodies squaring , symmetrical and marginal syndesmophytes , cervical ankylosis in the late stage unilateral ( or bilateral ) sacroiliitis , asymmetrical and non - marginal syndesmophytes , atlantoaxial subluxation 1 3 la radiologia medica ( 2020 ) 125 : 654667 656 fig . 
the fractured odontoid process ascended beyond the foramen magnum and moved posteriorly into the vertebral canal compressing the bulb - medullary junction ( arrowhead ) rare cases , vertical migration of the odontoid process may lead to sudden death [ 5 , 17 ]  . 
a limitation of conventional radiography is the evaluation of bone structures only and without describing the characteristics of the retro - odontoid synovial tissues and their impact on neural structures . 
bundschuh and colleagues described the cervicalmedullary angle as the angle between a line drawn along the anterior aspects of the cervicalmedullary cord and another line along the medulla [ 3 ]  . 
patients with a cervicalmedullary angle < 135 may suffer from cranial settling and clinical signs of c2 root pain , neural compression or myelopathy . ct scan can provide detailed bone information and has been shown to have a greater correlation with neurological deficits than aadi assessment . 
the latter include male sex , the presence of rheumatoid factor ( rf ) and of anti - citrullinated protein antibodies ( acpa ) , rheumatoid nodules , severe peripheral disease with early and extensive development of erosive damage , intense systemic inflammatory response at onset ( measured by the reactive c protein ) , long - term disease and prolonged use of corticosteroids [ 1 , 2 , 1822 ]  . 
b sagittal , c coronal images t1 spir images with contrast show a high signal of the synovial pannus , of the articular masses of c1 , and in particular of c2 on the right , in relation to active inflammatory phenomena ( arrow )  . 
the odontoid process appears lateralized with marked reduction in the space between the right lateral mass of c1 and the odontoid process ( arrowhead ) 1 3 la radiologia medica ( 2020 ) 125 : 654667 association between cervical arthritis and peripheral erosive disease [ 18 , 23 ]  . 
this relationship reinforces the theory of the influence of synovitis in bone destruction , as already demonstrated during the initial phases of phlogistic process in hand and feet [ 24 , 25 ]  . 
according to this finding , many authors suggest to submit every patient with active , erosive and acpa positive early ra ( era ) , to the baseline cervicale spine mri [ 26 , 27 ]  . the involvement ofcraniocervical junction inspondyloarthritis the term spondyloarthritis is identifies a group of diseases that share inflammation of the joints and entheses . 
the most common conditions for this group of diseases are ankylosing spondylitis ( as ) and psoriatic arthritis ( psa ) , while reactive arthritis and entoropatic spondyloarthritis have a lower prevalence ( table1 )  . 
as an involvement of the craniocervical junction , anterior aas is the most frequent finding ( 6.821% ) , usually observed in patients with severe and long - lasting disease [ 28 ]  . ankylosing spondylitis typically , inflammatory changes and ankylosis begin in the lower portions of the spine with a tendency toward upward progression in the more advanced stages of the disease , when cervical spine involvement becomes relatively common in the as [ 29 ]  . 
 the most commonly observed lesion is vertebral squaring , followed by syndesmophytes , erosion of the vertebral body , discites and involvement of the joint facets [ 31 ]  . 
the most advanced pictures are described as the appearance of a bamboo spine , while calcification of the interspinous ligament can give the appearance of a dagger spine . a synovial component at the level of the transverse ligament can also be demonstrated in patients with as , but to a lesser extent than in ra [ 32 , 33 ]  . advanced lesions such as dislocation , zygapophyseal joint fusion , secondary atlantooccipital ossification and spinal canal stenosis can also be seen as a final part of an advanced pathological process . 
atlantodental ossification or ankylosis increases with age and duration of disease in the as and is more frequent in severe symptomatic and structural forms of disease [ 31 ]  . psoriatic arthritis the involvement of the cervical spine can be documented in 3575% of cases of psa . 
the abnormalities of the cervical spine during psa are generally milder and less common than in ra , with the possible exclusion of apophyseal joint ankylosis [ 18 ]  . 
other conventional radiology works describe a higher prevalence , documenting frequent anomalies of the joint facets ( osteophytes , loss of joint space and sclerosis ) in psa , particularly at levels c3c4 and c4c5 [ 37 ]  . 
bobek and colleagues reported a prevalence of 68% cervical spine involvement in patients with suggestive symptoms , and in 29% of cases these inflammatory lesions were detectable in conventional fig . 
sagittal images , a t1 weighted , b t2 weighted , c t2 stir show thickening of the atlanto - epistrophic soft tissues due to synovitis associated with some areas of subchondral erosion of the odontoid process ( arrow ) 1 3 658 la radiologia medica ( 2020 ) 125 : 654667 fig . 
4 psoriatic arthritis , a axial , b coronal , c sagittal ct images demonstrate marked reduction of thickness of the articular rhymes c1c2 with areas of sclerosis and subchondral erosions more evident on the left in the periodontoid medial portion ( arrow )  . 
during psa the predictive factors of cervical spine involvement are a long duration of the disease , an active disease in the first 5years and the presence of peripheral involvement [ 40 ]  . 
cervical joint disease is not related to the severity of the skin or nail disease [ 38 ]  . the involvement ofcraniocervical junction indiffuse idiopathic skeletal hyperostosis diffused idiopathic skeletal hyperostosis ( dish ) is a systemic disease , not linked to inflammatory processes , which is quite frequent ( 10% prevalence in subjects over 50years of age ) [ 4143 ]  . 
the diagnosis of dish requires the presence in conventional radiology of a continuous flow ossification ( fluid wax ) of the anterior longitudinal ligament of at least four contiguous thoracic vertebral bodies , the maintenance of intervertebral spaces , the absence of degeneration of the apophyseal joint or inflammatory lesions of the sacroiliac joints [ 45 ]  . 
5 diffuse idiopathic skeletal hyperostosis , a fse t1 weighted , b gre t1 weighted , c stir sagittal images show widespread ossification and irregular thickening of the anterior longitudinal ligament from c3 to d1 with minimal anterior disk degeneration , typical of dish . 
the anterior longitudinal ligament appears iso - hyperintense to the bone marrow both in t1 and in t2 due to the presence of yellow marrow in the ossified and thickened ligament ( arrow ) 1 3 la radiologia medica ( 2020 ) 125 : 654667 bone changes . 
compared to conventional radiology , ct scans are more sensitive in detecting structural changes in the dish [ 48 ]  . the differential diagnosis of dish includes other conditions that have exuberant proliferation of new bone in common and enthesopathies such as as . 
the main distinguishing features of dish compared to as are an older age at the onset of symptoms , often mild or even absent ( frequently the disease is an occasional finding ) , no association with hla b27 , no involvement of the sacroiliac joints or erosive lesions of the peripheral entheses , no obliteration of the apophyseal joint and gross ossification of the anterior longitudinal ligament . 
like the as , the dish also tends to ossify the ligaments and entheses , however , in the absence of inflammatory phenomena [ 49 , 50 ] ( table2 )  . 
dish may also predispose to odynophagia , gastroesophageal reflux disease , aphonia , dysphonia and aspiration pneumonia [ 56 ]  . a myelopathy condition may also be associated with ossification of the posterior longitudinal ligament ( opll ) and ossification of the flavum ligament ( olf ) , two other possible complications of dish ( up to 50% of cases ) [ 57 ]  . 
 opll is most frequently located in the cervical spine ( 70% ) , followed by the thoracic spine ( 15% ) and the upper lumbar spine ( l1l3 ) ( 15% )  . 
opll is divided into four subtypes according to position : ( 1 ) continuous ossification ( fluent ossification at different levels and related disks ) , ( 2 ) segmental ( posterior to each vertebral body and not beyond the level of the adjacent disk ) , ( 3 ) mixed ( combination of segmental and continuous types ) and ( 4 ) focal ( which occurs only at the level of the disk )  . 
ct and mri detect in more detail certain peculiarities ( e.g. , opll , olf ) and complications ( e.g. , spinal canal stenosis and compressive myelomalacia , fracture dislocation involving anterior and posterior elements ) [ 59 ]  . table 2 distinguishing features of diffuse idiopathic skeletal hyperostosis ( dish ) and ankylosing spondylitis . 
 [ 49 ] etiology prevalence usual age of onset ( years ) sex ratio ( m / f ) dorsal kyphosis limitation of spinal mobility pain limitation of chest expansion laboratory investigations associated diseases radiological features dish ankylosing spondylitis idiopathic 3.825.0% > 50 frequent frequent unusual frequent non - specific and inconclusive high esr and crp diabetes mellitus , obesity autoimmune 0.051.4% < 40 very frequent very frequent very frequent very frequent uveitis , ulcerative colitis hyperostosis si joint erosion si joint ( synovial ) obliteration si joint ( ligamentous ) obliteration apophyseal joint obliteration all ossification pll ossification syndesmophytes enthesopathies ( whiskering ) with erosions enthesopathies ( whiskering ) without erosions very frequent hla - b27 ( european whites ) hla - b27 ( african americans ) very frequent absent unusual frequent absent very frequent very frequent absent absent about 8% about 2% frequent very frequent very frequent very frequent very frequent unusual frequent unusual very frequent frequent about 90% about 50% dish diffuse idiopathic skeletal hyperostosis , all anterior longitudinal ligament , pll posterior longitudinal ligament , si sacroiliac 1 3 660 la radiologia medica ( 2020 ) 125 : 654667 the involvement ofcraniocervical junction incrystalassociated arthropathies the cervical spine may also be affected in arthropathies associated with crystals , with some specific semiological characteristics . 
in this review the focus is mainly on the three most common conditions , in particular calcium pyrophosphate dihydrate deposition disease ( cppd ) , the hydroxyapatite crystal deposition disease ( hadd ) , and the monosodium urate crystals disease ( gout )  . 
the majority of crystal diseases are related to cppd or hadd ; gout is much less common . calcium pyrophosphate dihydrate crystal deposition disease cppd is a very common crystal deposition disease , especially in the elderly population . 
most cases are sporadic ; however , there are rare familiar forms , in which the cppd present with metabolic disorders ( e.g. , abnormalities of magnesium and potassium ions such as in gitelmans syndrome )  . 
it rarely affects the structures of the dorsal or lumbar spine , including the intervertebral disks , the posterior longitudinal ligament , the facet joints , the flavum ligament or the sacroiliac joints [ 62 ]  . 
this clinical entity , called crowned dens syndrome ( cds ) , may mimic several conditions and may be among the causes of a fever of unknown origin [ 64 , 65 ]  . 
the tla is a strong band of fibers designed to maintain contact between the odontoid process and the anterior arc of c1 , if damaged , may occur atlantoaxial subluxation . 
 being mainly composed of fibrocartilage , tla , such as the knee meniscus , triangular wrist fibrocartilage and pubic symphysis , is a preferred site for cppd [ 67 ]  . conventional radiography is very useful for the diagnosis of cppd in peripheral joints . 
6 crowned dens syndrome , a sagittal t1 weighted , b t2 weighted images of cervical spine show abundant tissue around the odontoid process with fine calcifications in the context ( arrow )  . 
the intervertebral disk remained at low signal intensity , unlike the infectious inflammatory forms , c sagittal t1 spir after contrast medium shows inhomogeneous contrastographic uptake of tissue around the odontoid process ( dotted arrow ) 1 3 la radiologia medica ( 2020 ) 125 : 654667 fig . 
7 crowned dens syndrome , a the axial ct image shows calcification of the transverse ligament of the atlas that appears thickened ( arrow ) , b coronal , c sagittal images show abundant periodontoid calcifications ( arrowhead ) and erosions of the odontoid process in the same patient ( dotted arrow ) hydroxyapatite crystal deposition disease hadd is a systemic disease of unknown etiology determined by para - articular and / or intra - articular deposition of ha crystals [ 69 ]  . 
even for this condition , the actual incidence is unknown as it is believed to be widely underdiagnosed and is often an occasional finding [ 70 , 71 ]  . 
hadd is more common in middle age , equally distributed between the sexes , and is rarer than cppd [ 72 ]  . imaging allows accurate diagnosis in cases with typical calcific deposits and destructive lesions ( table3 )  . 
there are three different clinical and radiological entities at the cervical level of hadd , including ( 1 ) calcific tendonitis of the longus colli , ( 2 ) cds and ( 3 ) calcinous discal [ 69 ]  . calcific tendinitis ofthelongus colli this disease generally affects adults between the ages of 30 and 60 . 
mri may also show inflammatory vertebral lesions characterized by the presence of bone marrow edema and erosive - like alterations table 3 radiographic manifestations of hydroxyapatite crystal deposition disease of the cervical spine . 
 [ 60 ] crystal deposition in the longus colli tendon calcific ( nonosseous ) density in the prevertebral ( or retropharyngeal ) soft tissues , typically at the c1c2 level regression of the calcification ( spontaneous or after nonsteroidal antiinflammatory drug treatment ) crystal deposition elsewhere in the spine paraspinal longitudinal ligaments intervertebral disk ( discal calcinosis ) apophyseal joints calcifications surrounding the odontoid process hydroxyapatite crystal - induced arthritis in chronic long - standing disease any spinal joint may be involved ( rare ) cervical myelopathy and cervical cord compression ( elderly women ) 1 3 662 fig . 
8 hydroxyapatite crystal deposition disease , a lateral cervical spine radiography , b sagittal bone ct show calcification in the retropharyngeal prevertebral space at c2 , below the anterior arch of c1 , due to calcific tendinitis of the longus colli muscle ( arrow ) la radiologia medica ( 2020 ) 125 : 654667 [ 77 ]  . 
knowledge of this entity is important to prevent unnecessary invasive surgical treatments or prolonged antibiotic therapies [ 82 ]  . calcifications surrounding theodontoid process like cppd , hadd can also cause deposits that cause a cds [ 60 , 63 ]  . 
from the imaging point of view , it can be seen that calcifications of articular cartilage are a pathognomonic sign of cppd , and therefore , radiological examinations performed on the appendicular skeleton can be helpful . 
however , the diagnosis of certainty can only be made by analysis of synovial fluid . discal calcinosis it is more common in the cervical spine , where it causes symptoms such as pain , stiffness and reduced range of movement [ 84 , 85 ]  . 
ct and mri are generally not necessary , but they may be able to better differentiate the lesions . gout gout is a common form of crystal disease characterized by the deposition of monosodium urate crystals ( msu )  . 
konatalapalli and colleagues showed that 35% of patients with poorly controlled gout had evidence of ct scans of spinal gout with erosion and / or tophi [ 90 ]  . 
although it may be completely asymptomatic , axial gout is also a definite cause of acute back pain and may also manifest with signs of radiculopathy and spinal cord compression [ 92 ]  . 
in mri tophaceous deposits appear as a homogeneous images with a signal ranging from intermediate to low on t1 ( signal intensity similar to that of the muscle ) , in t2 the image appears homogeneous and may show low or high intensity . 
 ct typically shows the presence of intra - articular and juxta - articular erosions with sclerotic margins and a higher attenuation density than the surrounding muscle [ 94 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 654667 in 2015 , the american college of rheumatology / european league against rheumatism drew up new criteria for the classification of gout . 
dect is increasingly regarded as a very sensitive technique for the identification of msu deposits , even in preclinical phases [ 95 , 96 ] , as it can differentiate substances within tissues according to their relative absorption of x - rays [ 97 ]  . the involvement ofcraniocervical junction ininfectious diseases the infectious processes are mainly carried out through either local extension or hematological seeding , causing abscesses in the prevertebral , intraspinal or epidural region . 
tuberculosis of the cervical spine is also a rare but very dangerous occurrence . septic arthritis oftheatlantoaxial joint the atlantoaxial joint represents the site of septic arthritis in 34% of all spinal infections . 
more often , spinal abscess is associated with predisposing conditions such as intravenous drug use , diabetes mellitus , human immunodeficiency virus ( hiv ) infection , pathological obesity , terminal renal failure , or previous trauma , surgery or locoregional anesthesia procedures . 
 septic arthritis of the atlantoaxial joint may be accompanied by simultaneous osteomyelitis of the odontoid process [ 99 ]  . a defined clinical picture , called grisel syndrome , is the atlantoaxial subluxation associated with infection of the pharynx and surrounding tissues [ 100 ]  . 
the first radiographic signs that appear are anterior radiolucency at the level of the subchondral region , followed by loss of definition of the vertebral plate and narrowing of the intervertebral disk . 
in the acute phase of the infective process , the vertebral plates of adjacent vertebral bodies are poorly defined , with diffusely hypointense images in spin - echo sequence t1 weighted without contrast , and hyperintensive on t2 - weighted images . 
in the case of infective processes , an atlantoaxial effusion lateral to the atlantoaxial joint , which is not present in the case of crystal arthropathy , can often be documented [ 103 ]  . 
post - contrast gd - dtpa t1 weighted images reveal an enhancement of the vertebral bodies , peripheral soft tissue to the intervertebral disks and may also document areas of necrosis . 
the symptoms can be initially variable and not well defined ( patients can be apyretic , and with normal acute phase reactants ) , while x - rays , as for infectious processes supported by bacteria , are often negative in the early stages [ 106 , 107 ]  . 
ct and mri can diagnose these entities early and accurately , but cultural examinations performed on surgical samples may be necessary . table 4 comparison of crystalinduced arthritis and septic arthritis of the atlantoaxial joint . 
 [ 103 ] crystal - induced arthritis septic arthritis neck pain symptom duration from onset severe resolves within 9days severe persists for several months without appropriate treatment computed tomography calcification around the odonbone destruction of c1 and / or c2 magnetic resonance imaging prognosis toid process no marked changes good joint effusion poor without appropriate treatment 1 3 la radiologia medica ( 2020 ) 125 : 654667 664 fig . 
9 staphylococcus infection of the atlantoaxial joint , a axial stir image shows edema and infiltration of the lateral and posterior paravertebral soft tissues at c2 level bilaterally with involvement of the epidural space ( arrow ) , b t1 axial fs image with mdc shows intense contrastographic uptake of paravertebral and epidural soft tissue with thickening of the meninges ( arrowhead ) , c stir , d t1 - w sagittal images with contrast medium confirm the edema and the infiltration of the posterolateral paravertebral soft tissues between c1 and c2 ( dotted arrow ) tubercular spondylitis conclusions atlantoaxial involvement is extremely rare in the course of tuberculosis , estimated to represent 0.31% of cases of tubercular spondylitis [ 108 112 ]  . 
in grade 2 there are minimal bone changes with ligamentous lesions and anterior subluxation of c1 on c2 , there may or may not be a cranial migration of the odontoid process . 
 in grade 3 there is a marked alteration of the bone structures , with a complete elimination of the anterior arch of the first cervical vertebra [ 109 ]  . 
very rare is a disease with advanced destructive processes also affecting the atlas , in which case there is an emergency that requires prompt immobilization to avoid catastrophic neurological complications [ 112 ]  . cervical pain is a high prevalence condition in the general population ( 1020% ) , similar to that of low back pa the involvement of the craniocervical junction should always be suspected in patients with msd , representing a frequent involvement of ra . 
in case of suspected inflammatory involvement of the atlantoaxial joint , crystal arthropathies must always be kept in mind ( in particular cppd because of its high prevalence in the elderly population ) , and in these circumstances ct is useful . 
in this article , we discuss the current practice in uk and the reason for the change over the last few years . keywords arthrogram shoulder uk direct mr arthrograms ( mra ) utilise distension of the joint capsule to separate intra - capsular structures and hence improve visualisation , when compared to conventional non - arthrographic mri . 
 although mra of the shoulder is performed in many centres across the uk , there is variation in the way this study is performed , including whether gadolinium - based contrast agents ( gdcas ) , saline or other agents are used to distend the joint space . an online survey was conducted of musculoskeletal radiologists in the uk to ascertain current practise in mra of the shoulder , changes in practice in the last 5years , and reasons for such changes . 
totally , 94% of respondents used gdcas in the injectate used to distend the glenohumeral joint space . historically , direct mr arthrography of the shoulder utilising either gadolinium and saline mixture , or saline alone was both initially described in the 1990s [ 1 , 2 ]  . 
a further technique known as indirect mr arthrography which relies on diffusion of gdcas from synovium into the joint fluid following intravascular injection was also developed , but this does not provide the joint distension which is helpful for visualisation of intra - capsular structures [ 3 ]  . 
since then , direct mra shoulder arthrography utilising gdcas has become an established practice . medicines and healthcare regulatory authority ( mhra ) advice to health professionals in the uk states that gdcas should be used only when diagnostic information is essential and not available with unenhanced magnetic resonance imaging [ 4 ]  . 
however , this study utilised different sequences between the mras with gdcas and saline , and used imaging parameters that may not be comparable with current practice such as relatively low field strength ( 1.0t ) and no fat suppression . more recent studies have questioned the benefit of using gdcas in mr arthrograms [ 68 ]  . 
 [ 6 ] compared mras with gdcas against saline mras , and found no significant difference in diagnostic accuracy for labral and rotator cuff pathology with arthroscopy as the gold standard . even without gdcas , there is intrinsic contrast between fluid injected into the glenohumeral joint during direct mr arthrograms and lower - signal intra - capsular structures on t2 and other fluid - sensitive sequences . 
 [ 7 ] reported comparable diagnostic accuracy for rotator cuff and labral pathology on mras of the shoulder using t1 and t2 - weighted sequences , and when using t2 - weighted sequences alone . 
 [ 8 ] reported comparable diagnostic accuracy for labral and cartilage pathology on t1and t2 - weighted sequences . safety concerns ofgadoliniumcontaining contrast agent use only two respondents cite concerns regarding gdca safety as their reason for omitting gdcas in mr shoulder arthrograms . 
this is not due to lack of awareness , as 77% were aware of the recent developments on gadolinium retention . there is increasing evidence of the long - term deposition of gadolinium in the brain and other tissues following intravascular use of gdcas , particularly linear agents [ 9 , 10 ]  . 
the precise nature of the gadolinium that is deposited within tissues ( dechelated or bound gadolinium , or intact gdca ) has not been established , and therefore the toxicity and clinical consequences are unknown [ 13 ]  . 
a research roadmap by nih / acr / rsna workgroup was published in 2018 identifying important knowledge gaps about gadolinium chelates that need to be addressed to better understand the safety implications of gadolinium deposition [ 13 ]  . 
the evidence for gadolinium deposition within the brain and body has resulted in withdrawal of licences of linear agents from intravascular use in the uk by the mhra , which has been in effect since 1 february 2018 [ 4 ]  . importantly , the developing body of evidence for brain and other tissue gadolinium deposition relates to intravascular use , not when used intra - articularly as for mras . 
safety concerns regarding gdcas are less of a concern in mras as the doses of gdca used in direct shoulder mras are a tiny fraction of those used intravenously for contrast - enhanced studies . 
however , there was a supply shortage of pre - filled magnevist syringes in early 2019 , prompting consideration of alternatives . magnevist was also previously available as an intravascular preparation at a concentration of 0.5 mmol / ml ( 500 mmol / l )  . 
this is technically feasible , but would be outside their uk licence of these gadolinium compounds , and thus be subject to local pharmacy policies on off - label use . 
adherence to gmc guidance on unlicensed medications would be recommended in these instances [ 15 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 605608 there are currently no gadolinium - based agents that are licensed for intra - articular use in children in the uk . funding no funding to declare.ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . impact ofincreased magnet field strength onmri two respondents cited the presence of 3 tesla ( 3t ) imaging as a reason to change their current practice with shoulder mra . 
magee [ 19 ] reported that the likelihood of finding an additional finding on mra is small ( 6% ) if an initial non - arthrographic conventional mri was abnormal . varying experience withmr shoulder arthrograms performed withandwithoutgadolinium at the authors institution , all mr shoulder arthrograms have been performed without gadolinium in the past 2years with satisfactory visualisation of the cartilage and labru in contrast , 4 survey respondents reported previously performing arthrograms without gdcas due to supply issues , but have a preference for mr arthrograms with gdcas due to concerns on imaging quality . 
the quality of the imaging achieved with and without the use of gdcas may vary from centre to centre depending on the field strength , mr sequences and radiographer expertise . conclusion the use of gadolinium - based agents for shoulder mra is prevalent in the uk . 
conventional mri is the preferred imaging modality for diagnosis and treatment monitoring vol . : ( 0123456789 ) 1 3 648 la radiologia medica ( 2020 ) 125 : 647653 in head and neck tumors owing to its superior soft tissue resolution ; however , it has poor diagnostic accuracy in differentiating between the two tumors because of the overlapping morphology - based imaging features [ 4 ]  . diffusion - weighted imaging ( dwi ) develops an image contrast based on the difference in diffusivity of water molecules in distinct tissues . 
 in recent years , the utility of dwi for differentiating between benign and malignant diseases and identifying pathological differences of certain malignancies in the head and neck region has been well established [ 57 ]  . 
nevertheless , most previous studies usually performed quantitative analysis based on one single region of interest ( roi ) on the largest tumor section , which might have underestimated whole - tumor characteristics . 
thus far , to our best knowledge , there has been no reported study that has applied adc histogram analysis to quantify the difference between primary npc and npl . the purpose of this study was to investigate the value of the whole - tumor histogram analysis of adc maps in the differentiation of npc and npc . materials andmethods patients selection this study was approved by the institutional ethics review board of our hospital , and the requirement for informed consent was waived given the studys retrospective nature . 
for both groups of patients , the following inclusion criteria were applied : ( 1 ) pathologically proven npc or npl , ( 2 ) without any anti - tumor treatment before mr examination , and ( 3 ) complete imaging data with dw sequences . 
the final study population comprised 127 patients : 89 patients with npc and 38 with npl . mri protocols all mri procedures were performed using a 3.0 t system ( trio tim ; siemens , erlangen germany ) with a head and neck combined coil from the suprasellar cistern to the collarbone . 
the protocol was as follows : ( 1 ) t1 - weighted sequences in axial , sagittal , and coronal planes , ( 2 ) axial t2 - weighted sequences , ( 3 ) axial dw - weighted sequences with diffusion sensitivity values of 0 and 1000s / mm2 , ( 4 ) enhanced t1 - weighted sequences in axial , sagittal and coronal planes . 
all parameters were described in detail ( table1 )  . analysis ofdw images all the adc maps were automatically created by using the software ( siemens medical system )  . 
to access interobserver reproducibility , the measurement obtained by radiologist 1 was compared with the measurement by radiologist 2 . image segmentation was performed by using itk - snap open - source software to assess the volume of the whole tumor . 
 at the same time , to minimize the influence of the partial table 1 mr imaging parameters sequence echo time ( ms ) matrix field of view ( mm2 ) repetition time ( ms ) section thickness ( mm ) t1 - weighted imaging t2 - weighted imaging 6000 5600 384 307 384 307 192 192 240 ( 220260 ) 240 ( 220260 ) 240 ( 220260 ) 1 3 la radiologia medica ( 2020 ) 125 : 647653 volume effect , rois were drawn slightly smaller than the real lesion . 
receiver operating characteristic ( roc ) curves and the area under the curve ( auc ) were used to evaluate the ability of each parameter to distinguish between the two groups . 
an icc value close to 1 represented almost perfect agreement and reliability , and if the 95% confidence interval of the difference includes 0 , the difference between the two raters was considered insignificant . results patients characteristics one hundred twenty - seven patients were enrolled in our study , including 80 male patients ( mean age , 39years ; range , 3069years ) and 47 female patients ( mean age , 45years ; age range , 2880years )  . 
in case of npl , the histopathological types were diffuse large b cell lymphoma ( n = 24 ) , natural killer / t - cell lymphoma ( n = 7 ) , malt ( n = 4 ) , and mantle cell lymphoma ( n = 3 )  . comparison ofadcrelated parameters betweennpc andnpl the results for the comparison of adc histogram - derived parameters and roi - based adc values ( adcmean ) between npc and npl are presented in table1 . 
c whole - tumor histogram of adc values demonstrates a narrow range and a negative skewness curve , indicating high uniformity and low skewness 1 3 650 la radiologia medica ( 2020 ) 125 : 647653 fig . 
moreover , roc curve analysis showed that uniformity was the optimal parameter with the highest accuracy ( auc = 0.758 ) , followed by the 10th percentile adc ( auc = 0.758 ) to differentiate between the two tumor types . 
particularly , in some atypical cases , differential diagnosis is still quite challenging . diffusion - weighted imaging is a functional imaging technique with noninvasive quantification and has proven valuable in differentiating benign from malignant disease , especially in different types of head and neck malignancies . 
 in this study , we analyzed the adcmean with conventional the roi - based method , and the results showed that the adc value of npc was significantly higher than nhl . 
thus , this method may be prone to information loss , thereby failing to reflect the nature of the whole tumor . histogram analysis of adc can evaluate the distribution of adc values to reflect the biological heterogeneity of a tumor by classifying domains of different diffusivity [ 20 ]  . 
 heterogeneity is an important feature of a tumor and could be visualized graphically and quantified by means of the parameters acquired from the histogramoreover , wholetumor analysis of adc can provide a more comprehensive evaluation of the entire tumor heterogeneity [ 21 ]  . 
recently , this approach has shown promise for differentiating between different tumor types , tumor grades , and monitoring therapeutic response in head and neck cancers [ 1316 ]  . 
however , to our knowledge , the utility of this approach for differentiating npc from npl has not yet been evaluated . uniformity and skewness are two important parameters calculated by histogram analysis to present microstructural and functional heterogeneity of a tumor [ 22 , 23 ]  . 
positive skewness indicates that the distribution peak of the histogram has a longer or flatter tail on the right with most voxels containing an adc less than the mean , suggesting that there is a large portion of highly cellular composition within the tumor . 
our results showed that npl had significantly higher skewness than npc , which exhibited a positive distribution of adc values that might be explained by the high cellularity and high nucleus - to - cytoplasm ratio in npl that fig . 
our finding suggests that wholetumor analysis of adc could be a new noninvasive quantitative method to distinguish between and detect the tissue characteristics of the two nasopharyngeal tumors in clinical practice . npc and npl are the two most common nasopharyngeal malignancies in the southern provinces of china [ 1 ]  . 
as imaging features of the two diseases usually overlap , namely homogenous , non - necrotic density / intensity , intermediate intensity on t1wi and slight hyper - intensity on t2wi , and mild enhancement after contrast - medium injection , it is difficult to distinguish them based only on the morphological characteristics on routine mri . 
although some previous studies have described differences in mri features , regional 1 3 652 la radiologia medica ( 2020 ) 125 : 647653 remarkably restricts the mobility of water . 
it can be established as a significant , clinically relevant imaging biomarker in nasopharyngeal tumors to aid in clinical diagnosis . in addition to skewness and uniformity , the percentile adc was also a useful predictor for differentiating npc from npl . 
in our study , histogram - derived adc metrics ( mean adc , median adc , 10th percentile adc , and 25th percentile adc ) for npc were significantly higher than those for npl . 
the diagnostic superiority of the 10th percentile adc may be attributed to the fact that the lower percentile adc values are more representative of heterogeneity in a tumor than the higher percentile adc values . 
moreover , compared with conventional roi - based adcmean , the 10th percentile adc might be a more promising imaging biomarker to differentiate npc from npl in clinical practice . our study has some limitations . 
further detailed studies combining conventional mri and adc histogram analysis should be conducted to address these issues . in conclusion , whole - tumor histogram analysis of adc maps could improve the diagnostic performance for differentiating npc from npl . 
real - time reverse - transcription polymerase chain reaction ( rt - pcr ) demonstrated a low sensibility , therefore chest computed tomography ( ct ) plays a pivotal role not only in the early detection and diagnosis , especially for false negative rt - pcr tests , but also in monitoring the clinical course and in evaluating the disease severity . 
this paper reports the ct findings with some hints on the temporal changes over the course of the disease : the ct hallmarks of covid - 19 are bilateral distribution of ground glass opacities with or without consolidation in the posterior and peripheral lung , but the predominant findings in later phases include consolidations , linear opacities , crazy - paving pattern , reversed halo sign and vascular enlargement . 
 the ct findings of covid - 19 overlap with the ct findings of other diseases , in particular the viral pneumonia including influenza viruses , parainfluenza virus , adenovirus , respiratory syncytial virus , rhinovirus , human metapneumovirus , etc . 
 salesi , via conca 71 , 60030ancona , an , italy 2 dipartimento di scienze cliniche specialistiche e odontostomatologiche , university politecnica delle marche , ancona , an , italy 3 clinica reumatologica , ospedale carlo urbani , jesi , an , italy 4 dipartimento di scienze cliniche e molecolari , university politecnica delle marche , ancona , an , italy 5 divisione di reumatologia , dipartimento di medicina interna , asst fatebenefratelli - sacco , milan university school ofmedicine , milan , italy 6 dipartimento di radiologia . 
asst fatebenefratelli - sacco , milan university school ofmedicine , milan , italy 7 divisione di malattie infettive , department di scienze cliniche e biomolecolari , asst fatebenefratelli - sacco , milan university school ofmedicine , milan , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 636646 introduction the virus now known as sars - cov - 2 , showed up in wuhan market in december 2019 and , starting from there , it rapidly spread throughout the world [ 1 , 2 ] , faster than other coronaviruses such as sars - cov - 1 previously did . 
 the global economic , social , historical , institutional and scientific impact of covid - 19 is and will remain substantial ; the scientific community is still working to identify the disease in its earlier stages , when it is asymptomatic and the nasopharyngeal swab may still be negative . the clinical expressions of covid - 19 range from asymptomatic course to mild ( low - level fever , fatigue , and a dry cough together with symptoms such as nasal congestion , a runny nose , diarrhea and slight weakness with or without pneumonia ) to severe form , characterized by dyspnea and / or hypoxemia that can quickly progress to septic shock , uncorrectable metabolic acidosis , coagulation disorders , hospital admission , need for intensive care , and death in 4.315% of patients [ 3 ]  . early disease progression can be rapid [ 4 ]  . 
several evidences suggest that the virus may induce a pro - inflammatory state related to the over - activation of effector t cells with associated massive production of pro - inflammatory cytokines that may play a key role in the development of the lung disease and damage , which in turn lead to acute lung injury ( ali ) [ 911 ]  . 
positive and negative predictive values are highly dependent on prevalence . moreover , rt - pcr is time - consuming [ 17 ] and a rapid decision - making is necessary in the early stages of an epidemic disease . 
consequently , some covid - 19 patients may not be promptly identified and , therefore , not treated and isolated , with contribution to the disease spread ; it is highly suggested to discharge the patient after obtaining two consecutive negative rt - pcr test results [ 15 , 17 , 18 ]  . 
 chest ct is a widely accessible , fast and non - invasive diagnostic tool for pneumonia . although rt - pcr remains the reference for the diagnosis of covid - 19 , ct may at least partially overcome the limitations of rt - pcr [ 13 ]  . 
 [ 17 ] confirmed the high sensitivity of ct ( 97% ) , but a poor specificity was recorded ( 25% ) , with an accuracy of 68% for the diagnosis of covid19 ; therefore , typical findings on ct may rule out false negative rt - pcr tests , however there is a considerable overlap between covid - 19 and other viral pneumonia ct features [ 19 , 20 ]  . 
the same authors also highlight the fact that follow - up chest ct scans were capable of detecting an improvement in the condition of 42% of patients before their rt - pcr findings were negative [ 17 ]  . 
they also analyzed the positive predictive value ( ppv ) , negative predictive value ( npv ) , accuracy , sensitivity and specificity of chest ct in different age groups of both genders , and found that it was more accurate and had higher ppvs in patients aged 60years than in younger patients and that , although there were no gender - based differences in its sensitivity , accuracy and ppv , it was more specific and had higher npvs in women [ 17 ]  . 
the sixth edition of the official diagnosis and treatment protocol of the national health commission of china states that chest ct is one of the diagnostic criteria for covid - 19 [ 21 ]  . 
even if some studies report protocols with high slice thickness ( up to 8mm ) [ 26 ] , a slice thickness < 3mm is preferred , being the optimal 0.61.5mm with no reconstruction gap [ 27 ]  . 
 optimal scan parameters for a non - contrast chest ct are 100120kv with modulated ma for dose - saving and optimal pitch values of 11.5 [ 27 , 28 ]  . 
however , the management of motion artifacts relies on low rotation times and high pitch values ; in this case the high - pitch , dual source acquisition may be helpful though not fully validated for pulmonary imaging [ 29 ]  . 
the post - contrast acquisition is optimized with bolus - tracking techniques [ 30 ]  . considering the need for seral examinations during the disease course , some authors raised concerns about radiation dose suggesting the implementation of low - dose ct protocols [ 31 ]  . 
the available strategies involve both the lowering of tube voltage and / or tube current with implementation of iterative reconstructions : it has to be pointed that most of these protocols were developed in a screeningsetting for detection of lung nodules [ 32 ]  . 
preliminary results in covid19 demonstrated encouraging results of spectral shaping coupled with dual - source acquisition [ 33 , 34 ]  . ct imaging features ofcovid19 covid - 19 demonstrated characteristic ct features during its course , so serial ct examinations may be helpful for monitoring disease course and to ensure a timely treatment . 
the hallmark of covid - 19 is the bilateral presence of patchy ground glass opacities ( ggos ) that may coalesce into dense , consolidative lesions , with a predominantly peripheral distribution under the pleura and along the bronchovascular bundles [ 3 , 35 ]  . 
as the disease progresses , the number of lesions may rapidly increase and extend to central areas with the left lower lobe being more often involved than the upper / middle and right lobes [ 36 ]  . 
during the disease recovery , the lesions are gradually absorbed over a period of two weeks , leading to the formation of fibrotic stripes [ 25 ]  . in addition to ggos and consolidations , covid - 19 pneumonia may show other ct findings or patterns such as interstitial thickening , crazy - paving pattern , reversed halo sign , halo sign , and airway and vascular changes . 
 consolidations are reported in 263% of cases , they may be multifocal , patchy or segmental , with sub - pleural or peri - bronchovascular distribution [ 28 , 41 ]  . 
the development of consolidations may be related to disease progression within two weeks after disease onset [ 25 ] , this is in accordance with the fact that within 13weeks , ggos are preceding or co - existing with consolidations [ 42 ]  . 
moreover , as consolidations have been found to be more common in middle - late disease or in patients aged > 50years [ 39 ] , they may be a warning sign of a severe course . reticular opacities a reticular pattern consists in a complex network of linear opacities related to interlobular and intralobular septal thickening [ 37 , 43 ] ( fig.4 ) due to lymphocyte infiltration [ 38 ]  . 
less extensive consolidations can be seen in the left upper and middle lobe ( white arrowheads ) , as well as a solid nodule surrounded by a ground glass halo in the middle lobe ( white arrow ) fig . 
 chest ct scan showing bilateral ggos in the apical segments of both lower lobes ( white arrows ) may help to differentiate covid - 19 pneumonia from other forms of pneumonia . 
figure1 shows the ct manifestations of covid - 19 described in published articles . ground glass opacities ( ggos ) ggos are unspecific findings defined as hazy lung opacities that do not obscure the underlying vascular or bronchial margins ( fig.2 ) , are supposed to be related to a partial airspace filling or to interstitial thickening [ 37 ]  . 
the predominant ct pattern in covid - 19 is bilateral ggos associated with consolidations , but the findings may differ from patient to patient or the stage of the disease [ 3 , 35 ]  . 
 [ 36 ] described the imaging findings of 121 symptomatic patients in relation to the time between symptom onset and the time of the patient underwent to a ct scan . 
who observed a vast predominance of small sub - pleural ggos during early disease , with the subsequent development of crazy - paving and of consolidation up to two weeks ( peaking after 10days ) [ 25 ]  . 
confirmed the predominance of ggos after symptom onset , with the percentage decreasing during the course of the disease ; they also described the co - presence of consolidation as the second most prevalent finding with the percentage increasing to 24% at 611days after disease onset [ 24 ]  . 
described the first post - mortem biopsy study in which they found pulmonary edema and a hyaline membrane , which suggests the underlying pathological mechanism of ggos [ 38 ]  . 
chest ct scan showing ggos and thickened pulmonary interstitial structures ( black circles ) , with a reticular pattern and fibrous stripes in both lower lobes ( black arrows ) and consolidations [ 25 ]  . 
 [ 45 ] reported that actually the bronchi are filled by gelatinous mucus plugs , therefore the term air bronchogram may be considered inaccurate as the bronchi are not filled with air and were found in association with a slight bronchial dilatation . 
the assumed pathological mechanism is bronchial obstruction and bronchial wall inflammatory damage , both leading to the destruction of bronchial wall structures , to the development of fibrosis , and to consequent bronchiectasis [ 37 ]  . 
intriguingly , as in the case of middle east respiratory syndrome coronavirus ( mers - cov ) infection , the presence of pleural effusion has been suggested as a prognostic factor of a worse outcome [ 41 , 42 ]  . 
the pathological mechanism underlying this sign is unclear ; it has been associated with angio - invasive fungal infections or hypervascular metastases , as a possible sign of peri - lesion hemorrhage [ 48 ] , viral infections , and organizing pneumonia [ 49 ]  . 
these signs have been reported in association to covid - 19 and is thought to be related to a healing lesion with a lower density core or an evolving lesion around a pre - existing ggo [ 50 , 51 ]  . 
this finding has been reported in 48% of patients with covid19 [ 28 , 42 ] , and it has been suggested as a likely significant risk factor for covid - 19 - patients with severe / critical pneumonia [ 41 ]  . 
ct scan showing the presence of right pleural effusion ( white full arrow ) , and consolidation and pleural thickening in the left lower lobe ( white empty arrow ) [ 46 ]  . 
ct scan showing a reversed halo sign ( focal rounded ggos surrounded by ring - like consolidation ) in the anterior segment of the right upper lobe ( white circle )  . 
it also shows ggos bilaterally in the upper lobes and in the apical segment of the left lower lobe , with superimposed interlobular septal thickening and intralobular lines ( crazy - paving ) in the left lung ( white full arrowheads ) , and focal consolidation with an air bronchogram in the right upper lobe ( white empty arrowhead ) fig . 
this hypothesis that may have been confirmed by a recent study that showed a higher incidence of pericardial effusion in association with severe / critical patients [ 41 ]  . covid19 andpulmonary embolism ( pe ) recently , some papers reported presence of coagulation disorders in patients affected by covid - 19 and suggested that microvascular thrombotic events may be involved in respiratory failure in covid - 19 [ 5456 ] rising the hypothesis that subsegmental vascular enlargement close to ggos could be a sing related to thrombosis [ 27 , 35 , 57 ] , however this sign may be also related to loco - regional hyperemia . 
broadly speaking , infection of the respiratory tract is a known risk factor of inpatient pe [ 59 ] , current literature reports pe in 2230% of patients affected by covid - 19 [ 30 , 56 , 60 , 61 ] ( fig.10 ) and ct angiography is indicated when pe is clinically suspected . differential diagnosis being rt - pcr the reference for covid - 19 diagnosis , ct demonstrated high sensitivity ( 97% ) but poor specificity ( 25% ) [ 17 ]  . 
this is mostly due to the fact that the ct appearance of covid - 19 overlap with other viral pneumonia , including influenza viruses , parainfluenza virus , adenovirus , respiratory syncytial virus , rhinovirus , human metapneumovirus , etc . 
image shows a pulmonary embolus in a segmental branch of the right pulmonary artery for the middle lobe ( white arrow ) in a patient with bilateral consolidations and pleural effusion ( empty arrows ) most of the viral pneumonia involve both lungs and multiple lung lobes with predominant distribution in posterior and peripheral part of the lungs ; however , there are some findings that could be useful in the differential diagnosis . 
chest ct in patients with influenza pneumonia shows bilateral patchy areas of ggos with or without focal areas of consolidation , usually in the lower lobes . radiological presentation of covid - 19 is not much different from pneumonia associated with the other two coronaviruses , sars and mers , probably the reason of that should be related to the fact that since they belong to the same coronaviridae family , they present the same underlying pathological mechanisthe pulmonary lesions in sarscov - 1 included bilateral extensive consolidation ; localized hemorrhage and necrosis ; desquamative pulmonary alveolitis and bronchitis ; proliferation and desquamation of alveolar epithelial cells ; exudation of proteins , monocytes , lymphocytes , and plasma cells in alveoli ; and hyaline membrane formation [ 5 , 16 , 35 , 63 , 64 ]  . 
however , differently from the reported sars cases , the covid - 19 pneumonia showed a tendency of multifocal distribution and a periphery distribution of ggo at the upper lobes and a basilar or subpleural preference in the lower lobes [ 65 ]  . 
moreover , the frequency of consolidation and severity score were also much lower 1 3 la radiologia medica ( 2020 ) 125 : 636646 than in sars , which might explain the lower death rates of covid - 19 pneumonia than sars . 
similarly to mers , covid - 19 pneumonia also presents a distribution at the right and left lower lobes but a more peripheral distribution could be recognized in the right and left upper lobes [ 65 ]  . 
 the archetypal responses associated with covid - 19 pneumonia are acute ggos that may later fuse together into consolidations that gradually develop and organize themselves in a linear pattern with a prevalent peripheral distribution , and eventually show a crazy - paving pattern or a reversed halo sign [ 66 ]  . 
 furthermore , unlike covid - 19 , neither sars nor mers were significant associated with lymphadenopathy , pleural effusion , nodules , or cavitations [ 65 ]  . moreover , covid - 19 ct features demonstrated some overlap with other pulmonary conditions such as pulmonary edema , pulmonary hemorrhage [ 67 ] , bronchiolitis obliterans , chronic obstructive pulmonary disease and druginduced lung disease [ 62 ]  . 
in pulmonary edema , chest ct demonstrates ggos with central distribution , often associated with smooth interlobular septal thickening , pleural effusion , and cardiomegaly , indicating congestive heart failure . 
for example , the most common chest ct features in methotrexate - induced lung disease diffuse parenchymal opacification , reticular opacities , and centrilobular nodules with a non - specific interstitial pneumonia pattern [ 62 ]  . therefore , it is necessary that the radiologists are confident with the different imaging patterns of covid - 19 and their changes during the course of the disease [ 24 , 35 ] in order to guarantee the prompt detection of disease progression and potential complications . conclusions in conclusion , our comprehensive review of published studies and front - line experience of interpreting ct images of covid - 19 pneumonia confirm the importance of ct in the diagnosis and management of covid - 19 infection . 
unlike other forms of pneumonia , covid - 19 pneumonia shows a high prevalence of bilateral ggos with a predominantly 1 3 644 la radiologia medica ( 2020 ) 125 : 636646 peripheral distribution on ct scans that are often paired with consolidations and interstitial thickening , and is less frequently associated with widespread distribution , pleural effusion or lymphadenopathy [ 19 , 62 ]  . clinicians and radiologists should familiarize themselves with ct findings in covid - 19 patients for various reasons [ 68 , 69 ] : chest ct images can arise an early suspicion of covid - 19 pneumonia and , in the correct clinical setting , bilateral ggos or consolidation should prompt radiologists to suggest it as a possible diagnosis ; ct can , therefore , complement rt - pcr in covid - 19 diagnosis [ 22 ]  . 
we recorded the coordinate of measurement points on the arterial vessels ( x , y , and z ) in each portal phase , original image of the arterial phase , and arterial phase with nrr . 
hence , it can visualize correctly the anatomy of the vessel . keywords non - rigid registration three - dimensional ct angiography multiphase fusion imaging misregistration surgical vascular anatomy preoperative simulation introduction recently , laparoscopic gastrectomy has been widely used in the field of gastroenterological surgery . 
 meanwhile , in terms of disadvantages , the entire view of the operative field is difficult to view , and the lesions , organs , and vessels cannot be directly manipulated by the surgeon during treatment . 
furthermore , previous studies have reported that the incidence of injury * hiroyuki takashima takashima@sapmed.ac.jp 1 division ofradiology andnuclear medicine , sapporo medical university hospital , south - 1 , west - 16 , chuo - ku , sapporo , hokkaido060 - 8543 , japan in the vessels during surgery significantly decreased with preoperative simulation using ct scan [ 3 ]  . the use of ct scan during preoperative simulation generally facilitates visualization of the artery and vein with threedimensional ct angiography ( 3d - cta ) [ 4 ] , which is helpful for a safe ligation of the vessels and dissection of the lymph nodes [ 5 ]  . 
to solve such problem , various applications have been developed , which include rigid registration by moving and rotating the distortion of x , y , and z directions [ 8 ]  . 
however , deviations can occur due to the effect of diaphragm movements during breathing ; as such , it is difficult to correct breathing - induced deviations using rigid registration [ 9 , 10 ]  . 
these phase scannings were performed during expiration . materials andmethods image analyses subjects andscanning technique the institutional review board of our institution approved this retrospective analysis and waived the need for informed consent . we retrospectively and consecutively selected 55 patients who underwent preoperative 3d - cta prior to gastroenterological surgery between january 2015 and february 2017 at our institution . 
finally , 54 patients ( 22 female and 32 male ; mean age of 65.9 [ range 2585 ] years ) were enrolled , excluding those with a history of gastroenterological surgery . ct images were obtained using a 320 - row ct scanner ( aquilion one , canon medical , tokyo , japan )  . 
the arterial phase images were scanned using a bolus - triggered technique by placing the cursor in the aorta at the level of the diaphragm and setting the threshold to 200 hu . 
the vessels were measured at three points , which included bifurcation of the anterior and lateral segment branch in the right hepatic artery ( rha ) , bifurcation of the splenic and common hepatic artery in the celiac artery ( cea ) , and proximal portion of the ileocolic artery ( ica ) on the superior mesenteric artery . 
we recorded the coordinate of these measurement points ( x , y , and z ) in each portal phase , original image of the arterial phase , and arterial phase with nrr . 
the distance of misregistration between the two points was calculated with the coordinate of the original image with nrr and that of the portal phase as true value using the following formula [ 11 ] : dwithout nrr = xa xb ya yb za zb fov ( mm ) dwith nrr = xa xc ya yc za zc fov ( mm ) ( xa , ya , za ) : spatial coordinate on portal phase fig . 
b misregistration of the arterial phase image corrected with non - rigid registration and portal phase image 1 3 620 la radiologia medica ( 2020 ) 125 : 618624 fig . 
c arterial phase with nrr ( xc : 10 , yc : 41 , zc : 44 ) ( xb , yb , zb ) : spatial coordinate on arterial phase without ( xc , yc , zc ) : spatial coordinate on arterial phase with nrr dwithout nrr : distance of misregistration between portal and original arterial phases dwith nrr : distance of misregistration between portal and arterial phases with nrr . the regression was significant ( p < 0.05 ) , proportional bias was present . 
the mannwhitney u test was used to test the statistical significance of the distance of misregistration between 2 points on the original and nrr image , which was set at a p value < 0.05. 
moreover , a mean difference 1.96 sd based on the brandaltman statistics was observed on all points and images , and significant systematic bias between measurements not identified as zero was included in the 95% ci . 
furthermore , misregistration of the z direction was more likely to increase than that of the x and y directions . discussion laparoscopic surgery has gained wide acceptance in surgical practice as it has numerous advantages , including minimal surgical incision , low intraoperative blood loss , shorter hospital stay , and faster return to normal bowel function compared with conventional open surgery [ 13 , 14 ]  . 
however , it is difficult to obtain an image of the entire operative field under a laparoscope , and the lesions , organs , and vessels cannot be manipulated directly . 
3d - cta fusion imaging facilitates the identification of the direction and position of the vessel because of fused images with appropriate scan timing for arterial and portal phases [ 15 ]  . 
moreover , the areas near the left gastric vein ( lgv ) and hepatic artery ( ha ) , which have anatomical variations , are challenging to view during lymph node dissection [ 19 , 20 ]  . 
hence , preoperative assessment of the precise arrangement of the perigastric vascular supply , including the lgv and ha , is important in preventing unnecessary bleeding and in facilitating a safe surgery . 
furthermore , previous studies have reported the importance of confirming the relative position of the ica and ileocolic vein ( icv ) preoperatively due to the ligation of the origin of the ica and icv and dissection of lymph node [ 17 , 21 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 618624 fig . 
5 volume rendering ( vr ) images of the relation to the celiac artery and left gastric vein obtained using preoperative multi - phased fused computed tomography scan in a patient with pancreatic cancer . 
the red and blue vessels were the celiac artery ( cea ) and left gastric vein ( lgv ) , respectively , and the green was the lymph nodes ( ln ) ( #7 )  . 
c vr images corrected with a non - rigid registration misregistration of the vessel and organization adjacent to the diaphragm has been observed in the z axis ( cranialcaudal ) [ 7 , 11 ]  . 
 however , in terms of disadvantages , the visualization of the vessel can be reduced by motion artifact in case a patient experiences difficulty in breath holding over 30s on scan time . meanwhile , liver analysis is equipped with nrr that performs registration by deforming the liver region of each phase . 
nrr algorithms based on elastic deformations , such as abdominal organs or vessels , were calculated using information about organ surface and grayscale data between images during the process [ 23 ]  . 
seventy - three patients with a ce - mri with phased array coil of the pelvis before the start of srt were included in the present study . results at imaging review , recurrence local recurrent disease was diagnosed in 48 of 73 patients . 
by considering as reference standard the decrease in prostate - specific antigen ( psa ) value after radiotherapy , we defined : 41 true positive ( patients with mri evidence of local recurrence and psa value decreasing after srt ) , 7 false positive ( patients with mri evidence of local recurrence without biochemical response after srt ) , 3 true negative ( patients without mri evidence of local recurrence and stable or increased psa value after srt ) and 22 false negative ( patients without mri evidence of local recurrence and psa value decreasing after srt ) cases . 
generally , rp is the first choice treatment modality for younger patients with localized tumors , while rt is preferred for elderly patients or for patients who are not fit for surgery [ 2 ]  . the recurrence rates after rp or after rt are similar and range from 10 to 30% within 5years , depending on the gleason score and other risk factors ( i.e. , involvement of seminal vesicles or lymph nodes , margin status at surgery , etc . ) , and the main pattern of treatment failure is predominantly local [ 36 ]  . the diagnosis of local recurrence of prostate cancer after rp or ebrt is today a real challenge . due to the long natural history of the disease , in the evaluation of the patterns of recurrence a surrogate of actual clinical recurrence is usually investigated , defined as biochemical recurrence and based on temporal trends of prostate - specific antigen ( psa ) serum values . variations of psa values after local treatment are different to each treatment option [ 79 ]  . according to national cancer center network ( nccn ) criteria , biochemical recurrence after rp is defined as a psa value that fails to decrease to undetectable levels after surgery or undetectable psa after surgery with a subsequent detectable psa level that increases on two or more sequential laboratory determinations [ 10 ]  . in most patients with biochemical recurrence , the site of failure is predominantly local [ 6 ]  . the expected psa nadir ( i.e. , the lowest recorded value after treatment ) is also different according to each treatment option . 
after rt , prostate parenchyma producing psa is not completely eliminated , and a psa value greater than zero may be detected even weeks or months after the end of therapy . 
on the contrary , after rp , the serum psa level should decrease to an undetectable level ( < 0.1ng / ml ) within 2130days and should keep this level . 
any detectable level and / or increase in serum psa level after rp should be considered as a marker of persistent disease or disease recurrence . salvage radiotherapy ( srt ) is considered the treatment of choice in case of local disease recurrence after surgery , offering a potential chance of cure , especially when patients are referred early and high radiation doses are delivered [ 1113 ]  . imaging before the start of rt is primarily used to identify patients with metastatic disease , that is , patients who would not benefit from local treatment . 
in 2010 showed that commonly used imaging techniques ( magnetic resonance imaging [ mri ] , positron emission tomography [ pet ] , trans - rectal ultrasonography [ trus ] , computed tomography [ ct ] , scintigraphy , etc . ) were not sensitive enough to detect small volumes of local disease recurrence , thus recommending the use of clinicalpathological variables to guide the treatment [ 14 ]  . however , in recent years , further refinement of imaging techniques such as pet and mri has proved useful to improve the possibility of identifying the site and extent of local recurrence , leading to better tailoring of srt [ 15 ]  . 
in particular , thanks to its high spatial resolution , mri appears as the most promising technique for an accurate evaluation of the prostatic fossa after prostatectomy [ 16 ]  . several studies in the literature have already evaluated the accuracy of mri with the use of an endorectal coil for the detection of local recurrence after radical prostatectomy [ 1719 ]  . to the best of our knowledge , only a few studies have examined the accuracy of mri ( 3t and 1.5t ) using a phased array coil . 
the aim of this retrospective study is to evaluate the sensitivity of contrast - enhanced magnetic resonance ( ce - mri ) using a phased array coil in detecting local disease recurrence after radical prostatectomy in patients referred for salvage radiotherapy , and to correlate its findings with psa values before the start of srt . materials andmethods inclusion criteria two hundred and thirteen patients treated at our institute the asst grande ospedale metropolitano niguarda in the period between september 2006 and november 2017 with srt after radical prostatectomy were reviewed . 
all patients with biochemical recurrence who were evaluated at our institution with a ce - mri with phased array coil of the pelvis before the start of srt were included in the present study . 
the time interval between ce - mri and the start of srt is presented as median [ i quartile , iii quartile ] , range . to estimate the sensitivity of ce - mri , patients were ordered according to increasing psa pre - rt values and grouped in bins with step of 0.1. 
in case of systemic disease , however , rt on prostatic bed would be useless , and the best therapeutic option would be antiandrogenic therapy ( androgen deprivation therapy adt ) [ 20 , 21 ]  . it is clear that salvage rt results are better for lower psa level at the time of recurrence : recent studies have shown favorable response rates when salvage radiotherapy was administered at serum psa levels of < 0.5ng / ml [ 20 , 22 ]  . in this clinical context , diagnostic imaging techniques are useful to differentiate local and systemic recurrence and to direct patients to the best therapeutic approach , i.e. , radiotherapy for local recurrence and hormone therapy for systemic disease [ 20 , 21 ]  . in detecting early recurrence , trus ( trans - rectal ultrasonography ) has neither high sensitivity nor specificity [ 23 , 24 ]  . 
choline / pet - ct is instead recommended when the value of the psa is greater than 1.4ng / ml because of its sensitivity and specificity for distant metastases , involved lymph nodes , and local recurrence detecting only in patients with high psa values [ 25 , 26 ]  . 
furthermore , choline / petct ability to detect local recurrence depends on the size of the lesion , being higher for lesions with a diameter 1cm [ 27 ]  . another emerging technique to identify local or systemic disease recurrence is the gallium - prostate - specific - membrane antigen pet - ct ( gapsma / pet - ct )  . 
gapsma / petct results can lead to a remarkable change in treatment , e.g. , the modification of radiation fields , dose escalation to macroscopic tumor lesions , and initiation of androgen deprivation therapy ( adt )  . 
currently , despite the higher sensitivity compared to choline / pet - ct , no general recommendation for a psa cutoff prior to postoperative staging with gapsma / pet - ct exists because only preliminary results have been reported [ 28 ]  . 1 3 688 la radiologia medica ( 2020 ) 125 : 683690 several studies have shown the usefulness of mri in detecting local recurrence of prostate cancer until now . 
 mri , in fact , combines anatomical and biological information thanks to the combination of morphological images as t2 - weighted ( t2w ) images and functional techniques as contrast - enhanced images ( ce ) , diffusion - weighted imaging ( dwi ) , and mr spectroscopic imaging ( mrsi )  . 
in our study , only morphological images and contrast - enhanced images were considered in the evaluation of the prostatic fossa after radical prostatectomy . anatomy of the pelvis is drastically modified by the surgical procedure : imaging should show the bladder neck descending into the prostatic fossa with a more conical shape and the vesicourethral anastomosis inferior to the bladder neck on the sagittal view [ 29 ]  . the individual sequences have a different usefulness in post - rp imaging , in particular , for the detection of recurrence . 
dwi can be useful for distinguishing tumor from mimicking etiologies , but the utility of this sequence depends largely on the use of metallic surgical clips : if clips were used , because of the introduction of susceptibility artifacts , the value is reduced [ 30 ]  . contrast - enhanced images certainly represent the most reliable parameter in the detection of local recurrence . 
in normal postoperative ce - mr imaging sequences , there should be no enhancement in the arterial phase , but only a low - level enhancement of vesicourethral anastomosis ( vua ) during the venous phase . 
 [ 17 ] reviewed unenhanced mri images of 48 patients with biochemical recurrence after rp ( psa ranging from undetectable to 10ng / ml ) identifying sensitivity and specificity values of 95% and 100% , respectively . 
 [ 19 ] reported similar results , with a sensitivity of 84.1% ( compared to 61.4% ) and a specificity of 89.3% ( compared to 82.1% ) when contrast - enhanced images were evaluated in addition to t2w images compared to t2w images only . the choice by our group to review morphological ( e.g. , t2w ) and enhanced images , comes from these scientific evidence . in our study , ce - mri studies of 73 patients submitted to radical prostatectomy and showing a biochemical recurrence were reviewed , representing a larger study population than in the majority of similar reports in the literature . in particular , rishke etal . 
there are several reasons to justify the missed detection of a local recurrence at mri , 1 3 la radiologia medica ( 2020 ) 125 : 683690 as radiologists may have experienced in the daily practice of prostatic imaging , or common mimics and pitfalls . 
 this observation reinforces the hypothesis of a correlation between increasing psa levels and lesion detectability . limitation ofthestudy first of all , this is a retrospective study and the results need to be confirmed in future prospective clinical trials . 
modern imaging , as dynamic - 18f - choline pet / ct may identify site of recurrence , allowing dose escalation to a biological target volume . methods hundred and fifty patients showed a local relapse at dynamic - 18f - choline pet / ct at time of biochemical recurrence . 
salvage radiotherapy ( srt ) is generally considered as the standard of care for patients with an increasing psa after rp [ 4 ] , by its ability to achieve a 63.5% freedom from biochemical failure at 5years [ 5 ]  . two major factors are crucial in srt : psa at time of treatment and total dose . 
in a recent review and meta - analysis , king [ 6 ] recorded a 2.4% decline in psa relapse - free * luca eolo trodella luca.trodella@unicampus.it 1 radiation oncology , campus bio - medico university , via a . 
currently , eau , estro and siog underline the importance of starting srt with a psa 0.5ng / ml , while no information is provided with regard to total dose [ 4 ]  . it if it can be argued that a doseresponse relationship for srt is a radical setting [ 7 , 8 ] , the issue of toxicity has , however , been raised with increasing srt dose [ 9 ]  . 
as toxicity in modern radiotherapy is , related to the issue of dosevolume issue [ 10 ] , increasing total dose to small volume should not therefore be detrimental . several authors have investigated the diagnostic accuracy of choline petct with an overall sensitivity from 38 to 98% . 
all patients underwent dynamic 18f - choline pet / ct at time of biochemical recurrence , while multiparametric magnetic resonance imaging ( mri ) was not routinely performed . in particular , btv was defined numerically by means of focal 18f - fch kinetics uptake using a computer - based roi ( region of interest ) with a tumor / background cut - off of 50% ; a nuclear physician and a radiation oncologist with at least 10years experience in petct images / analysis manually contoured this volume . 
 total dose to btv was 80gy with conventional fractionation of 2gy / die . lymph - node areas were delineated according to radiation therapy oncology group ( rtog ) guidelines [ 14 ] , and received 46gy with standard fractionation . 
prostatic fossa was also defined according to rtog criteria [ 15 ]  . the simulation protocol required a moderately full bladder and an empty rectuthis condition was verified for all patients at the time of the simulation . all patients received intensity modulated radiotherapy ( imrt ) or volumetric modulated arc therapy ( vmat ) delivered by a linear accelerator . 
normal tissue constraints used in the imrt or vmat planning were generally vdose ( i.e. , the percentage of normal tissue exceeding a defined dose ) : rectum v40 < 60% , v50 < 50% , v60 < 25% , v72 < 15% , v76 < 5% ; bladder : v50 < 50% , v60 < 25% , v70 < 5% ; femoral heads : dmax < 50gy ; penile bulb : dmean < 52gy . 
 geometrical verification was applied by a cone beam ct ( at least on a weekly basis ) , while a 2d verification ( kv or mv match ) was applied daily . toxicity was recorded prospectively and redefined according to ctcae ( common toxicity criteria for adverse events ) scale vers . 
 follow - up procedures included psa value and clinical evaluation 2months after the end of srt , followed by a psa and clinical evaluation every 3months for 2years , and every 6months thereafter . psa response was defined as any post - srt value less than 0.1ng / ml , while biochemical progression was defined as any psa increase after the psa nadir . 
patients who underwent neo - adjuvant and concurrent adt were evaluated for biochemical progression only . any biochemical progression after srt was analyzed by pet / ct scan , whole - bone radionuclide scan or pelvic mri ; disease progression was classified as biochemical ( psa increase only ) and clinical ( positive imaging or clinical exam )  . the study was developed according to the principles outlined in the declaration of helsinki . 
all patients agreed to the treatment and gave their written informed consent prior to radiation therapy . here , we review , retrospectively , data of a cohort , treated according to a uniform institutional treatment policy in order to assess toxicity and feasibility of such an approach and , secondly , to evaluate its activity . the ethical committee campus bio - medico university reviewed and approved this retrospective study . statistical analysis descriptive statistics assumed study sample characteristics . 
 relapse - free survival ( rfs ) was evaluated from the end of srt to the observation of progression or recurrence , either biochemical , clinical or radiological , or to the last followup if no event was observed . 
psa value less than 0.5ng / ml at time of srt was recorded in 83 patients ( 55% )  . 1 3 670 la radiologia medica ( 2020 ) 125 : 668673 table 1 patients characteristics ( n = 150 patients ) age at salvage radiation therapy ( years ) pathological gleason score table 2 radiation - related toxicity according to the ctc vers . 
two patients experienced a grade 3 urethral stenosis . with a median follow - up of 63.5months , 105 patients were free of recurrence without any adt , while 45 patients ( 30% ) experienced a biochemical or clinical progression . 
for exploratory purposes only , univariate analysis was performed investigating the impact of age , time from radical prostatectomy to srt , psa level at srt , nodal irradiation , gleason score , seminal vesicles involvement ( svi ) and extracapsular extension ( ece ) at time of surgery . an improvement in rfs was recorded for those patients with psa < 0.5ng / ml at time of srt or age > 70years , or gleason score 6 , or absence of ece at time of surgery . 
moreover , in 8 patients ( 5% ) , a nodal metastasis was also detected . whole pelvis radiotherapy was delivered to 82 patients ( 55% ) ; in those patients with a single positive lymph node , a boost dose was delivered up to 7680gy . treatment was well tolerated : all but 11 patients ( 7.3% ) completed the srt without any interruption ( table2 )  . the causes of treatment interruptions in those patients were all due to proctitis : seven patients experienced a grade 2 proctitis , recovered in all but one within 4days . 
three patients experienced a grade 3 proctitis with rectal bleeding ( recovered in 7 , 8 , 14days ) ; in one case the patient was on anti - coagulant therapy , while the other two cases were complicated by acute inflammation of hemorrhoids ( one patient ) and anal fissures . 
two factors , psa at time of treatment and total dose , have been recorded as crucial . king [ 6 ] , analyzing data of 71 series , including 10 , 034 patients treated between 1996 and 2015 , recorded a 2% gain in rfs for each additional gy in total dose between 60 and 70gy . in the same way , bernard et al . 
 [ 8 ] observed better results in terms of biochemical and local failure in patients who underwent high - dose srt ( 70gy ) with a 5 - year biochemical failure of 39% , near to the 63.5 of 5 - years freedom from biochemical failure in the multi - institutional series of pisansky etal . 
 [ 17 ] , instead , reported a 7 - year biochemical progression - free survival of 37% with 70gy . in the present analysis , we have updated data on 150 patients treated with high - dose srt with a median followup of 5years . 
our data irradiating to high dose very small volumes with modern techniques , supports the potential role of increasing total dose with no increased toxicity , such as in a radical setting [ 7 , 10 ]  . 1 3 672 la radiologia medica ( 2020 ) 125 : 668673 moreover , the ability to detecting the site of recurrence by petct remains a concern . 
in fact , the recommended psa level to prescribe choline pet should be at least 11.5ng / ml because its detection rate with psa < 1ng / ml is only 36% [ 20 ]  . 
 as recorded by degrado [ 21 ] , prostate cancer cells have a rapid uptake , within 26min , while the presence of the tracer in the bladder begins approximately 68min after injection . 
rtog 9601 explored the addition of 24months - bicalutamide to srt ( 64.8gy in 36 daily fractions , 5days a week ) in a population with a psa value at srt ranging from 0.2 to 4ng / ml , recording a benefit in both overall survival and metastasisfree survival . 
 moreover , patients were re - staged after a subsequent clinical or biochemical progression with conventional imaging only ( ct and bone scan )  . currently , the inclusion of petct is recommended also in recent asco guidelines [ 26 ] , with different patient populations among the present population ( all patients received petct before srt ) and rtog 9601 and getug - 16 trials . the activity and level of toxicity analyzed in the present paper underlines the ability to deliver high - dose srt in addition to standard treatment to prostatic fossa , without adding relevant toxicity . therefore , these results deserve to be explored in a prospective randomized trial , while awaiting data from the sakk 09 / 10 trial . compliance with ethical standards conflict of interest the authors declare that they have no competing interests . ethical approval all procedures performed in this study involving human participants were carried out in accordance with the ethical standards of the institutional research committee and in line with the 1964 helsinki declaration . 
future national clinical collaborative studies are advocated in order to investigate these controversial topics about breast cancer radiotherapy . keywords survey breast cancer airo hypofractionated radiotherapy partial - breast irradiation re - irradiation radiotherapy and neoadjuvant therapy introduction radiation therapy ( rt ) is an important part of breast cancer ( bc ) treatment . 
after conservative surgery for early - stage disease and after mastectomy for node - positive patients , rt halves the overall recurrence rate and reduces bc mortality by about one - sixth , with excellent cosmetic results [ 1 , 2 ]  . 
radiation therapy deeply changed in the last 2 decades , because modern technologies permit more precise treatments , achieving a better distribution of dose , volume * fabiana gregucci fabianagregucci@gmail.com extended author information available on the last page of the article de - escalation approach and less toxicity . 
furthermore , a better knowledge of tumor biology [ 3 ] and the availability of more effective systemic therapies [ 4 ] allow the adoption of alternative and personalized risk - adapted radiotherapy schemes . 
the standard of care for loco - regional recurrence is a salvage mastectomy , although recently published data suggest that a second breast - conserving surgery ( bcs ) followed by rrt can be a possible option [ 10 ]  . 
today , a large variety of treatment options and many different dosefractionation schedules exist , including brachytherapy ( bt ) [ 1214 ] , external beam radiation ( ebrt ) [ 15 , 16 ] and intraoperative radiotherapy ( iort ) [ 1719 ]  . in the context of integration between systemic therapies and radiation treatment , a topic that generates uncertainty in the clinical practice , is the management of the patient affected by breast cancer and treated with nac . 
this therapeutic uncertainty arises from the heterogeneity of the published data , relating to the predictive factors of loco - regional relapse [ 2028 ] and to the lack of adequate follow - up in patients treated with or without post - nac rt . 
nac is currently used for patients with large tumors or aggressive histology , not only to reduce tumor size to facilitate breast conservation , but also to assess invivo tumor response to the chemotherapy . 
the preoperative classification of breast cancer by molecular subtypes has influenced not only the response to chemotherapy , but also the choice of systemic agents , and it helps to predict the risk of recurrence [ 29 , 30 ]  . 
 a 2012 study that used national surgical adjuvant breast and bowel project ( nsabp ) b - 18 and b - 27 trial data identifies the clinical status of the lymph node , the size of the primary neoplasm and the response to the nac treatment as the main risk factors [ 31 ]  . guided by this changing wind , surveys get a snapshot of the current medical practice about gray questions and stimulate a discussion leading to the development of tailored trials . 
the aim of this survey is to report italian radiation oncologists practice in the management of bc on these controversial issues . materials andmethods in october 2017 , a nationwide 21 - point questionnaire was distributed online via surveymonkey to the italian radiation oncologists using the mailing list of airo . 
each individual radiotherapy cancer care center indicated , within its team , the radiation oncologist with the most expertise in the treatment of breast cancer , identifying him / her as the only respondent to the survey . 
in almost all cases ( 91% ) , an expert multidisciplinary discussion was performed to choose the best treatment for each patient . hypofractionated radiotherapy regarding the first topic , the 49% of participating centers answered to treat their patients with a hrt . 
the 95% of centers used this treatment approach as clinical practice after bcs for early - stage bc , mostly in women older than 50years ( 40% ) affected by invasive ductal carcinoma ( idc ) ( 89% )  . 
indeed , chest wall and lymph node area were irradiated with hypofractionated regimes in 13% and 15% of cases , respectively . partialbreast irradiation andreirradiation the second topic investigated the use of pbi and rrt . 
the age factor was not related to the rrt chosen ( 68% of answers were all age ) , and the most frequent histological type was idc ( 82% ) alone or associated with other histology subtypes . 
the answers concerning the irradiation volumes were so represented below : 54% total rrt ( wbi / chest wall irradiation ) and 94% pbi ( including 42% of tumor bed rt )  . 
the percentages of prescription dose for rrt were the following : 40gy / 15fr in 50% , 42gy / 16fr in 39% , 50gy / 25fr in 34% , 34gy / 10fr in 14% and 45gy / 18fr in 9% of cases , considering that more than one answer was allowed . radiotherapy afterneoadjuvant chemotherapy the last topic of this survey was rt after nac , to which 11% of the participating rt centers had replied . 
in the 55% of cases , a clinical patient evaluation was performed by the radiation oncologist at the end of systemic therapy , in 40% before the start of nac and 5% during it . 
the chest wall and the ipsilateral lymph nodes irradiation ( lni ) was a shared choice by most of the italian radiation oncologists ( 94% and 73% , respectively ) in the case of locally advanced bc at the disease diagnosis ( ct3 - t4 and / or cn2 - n3 ) , regardless of the kind of response obtained after nac ( complete response vs partial response ) and also independently of the axillary surgical approach ( sentinel lymph node biopsyslbvs axillary lymph node dissectionalnd )  . 
in the case of disease diagnosis with limited lymph node involvement ( cn1 ) , the same therapeutic option was chosen based on the response obtained after nac but not based on the axillary surgical approach : in the case of residual disease after nac ( ypn + ) , post - mastectomy rt was performed in the 79% and 76% of cases after slb and alnd , respectively . 
regarding the volumes of lni , in 39% of cases only the third nodal level was irradiated after alnd with 10 removed lymph nodes ( rlns ) ; in 39% of cases , the second and third nodal levels were irradiated after alnd with < 10 rlns ; and in 44% of cases , the firstthird nodal levels were irradiated after slb without alnd . 
only 11% of the centers had responded to use hrt on chest wall or lymph node area after nac , while 40% of them did not choose hrt after nac . discussion the management of bc is a very complex matter . 
considering that in 2017 the incidence of bc in italy has been estimated to be around 50 , 500 new cases with a 5 - year survival and 10 - year survival of 87% and 80% , respectively [ 32 ] , it is clear that the bc care represents an important part of the day - to - day clinical practice and significant commitment to resources for the health care system [ 33 , 34 ]  . 
according to the highest quality of care [ 35 ] , in 91% of the italian cancer care centers an experts multidisciplinary discussion was performed to choose the best treatment for each patient . the first topic of the italian survey regarded hrt . 
compared to a conventional regimen of 50gy in 25 fr , with a similar efficacy and toxicity profile , hrt is more suitable for patients and more cost - effective for health care system [ 33 , 34 ]  . 
the use of hrt - wbi has been gradually increasing in the most of italian rt centers in recent years , where it represents in the 95% of cases the standard of care with a prescription dose ranging between 39gy and 45gy with high use of moderately hrt ( 40gy / 15fr or 42.4gy / 16fr in 62% of cases )  . 
these results are in line with the recommendations of the main scientific societies [ 69 ] and reflect the effect of 1 3 la radiologia medica ( 2020 ) 125 : 674682 the long - term data derived by clinical randomized trials [ 5 ]  . 
 on the other hand , the characteristics of the population on which these trials focused ( middle age women , prevalence of idc , early - stage disease ) make difficult to transpose the same evidence in different population groups or in different treatment options , such as young and elderly patients , pure dcis , post - mastectomy and / or lni . 
as a matter of fact , the choice to use a hypofractionated scheme in our national experience seems to be influenced by patients age and the histotype , remaining in patients age > 70years [ 37 ] or in the case of dcis [ 38 , 39 ] a therapeutic choice not shared by the majority of italian cancer care centers , 4% and 48% , respectively . 
regarding the irradiation volumes , if the hrtwbi is performed by all interviewed centers , the hrt at the chest wall and / or lymph nodes areas is a reality limited to 13% and 15% of centers , respectively . 
although data derived from both national [ 40 , 41 ] and international [ 42 , 43 ] studies encourage the use of hrt on the chest wall and lymph nodes , a prospective safety and efficacy trial is probably needed to allow a customs clearance of this therapeutic option . a second topic of our survey regards pbi and re - treatment . 
the requirement of pbi is to achieve a high rate of local control , ensuring a low profile of loco - regional toxicity , through the irradiation of a smaller volume compared to wbi . 
the results obtained from the main randomized trials [ 4447 ] that were focused on this therapeutic option , showed us that the correct selection of the patient is the key to success for pbi , regardless of the used technique . 
 in the recent years , the growing experience in pbi associated with the evidence of a low - toxicity profile has increased its use for a salvage breast conservation for ipsilateral recurrence after bcs followed by rt . 
considerations regarding rrt include the initial treatment delivered , the time interval to relapse , the number of tumor foci within the breast , the ability to obtain negative margins , the ability to achieve a reasonable cosmetic outcome , the presence or absence of distant metastases , previous treatment modalities used and patient preference [ 10 , 11 ]  . 
despite the promising results achieved so far with second bcs and rrt [ 1219 ] , there is no robust evidence for considering such an approach as the standard management . 
the most important issue regarding bc ipsilateral local recurrence is the risk of patients developing metastatic disease , considering that often a recurrence of disease is marked by more aggressive biological behavior [ 48 ]  . 
the risk of metastatic disease is related to pathological features of the bc recurrence and the time interval between the relapse of cancer and the primary diagnosis ( 48months ) [ 49 ]  . 
in this framework , in which the local control affects less the overall survival of the patients with bc recurrence , an invasive surgical treatment such as mastectomy could lose meaning in favor of more conservative and safe treatment . in line with these important criticisms , the rrt does not represent a current practice in the italian scenario ( 0.6% of cases ) where , to date , it remains a no - fly zone and needs a much more long - term effectiveness confirmation . 
a common point of agreement is the time interval to relapse , and the 80% of the interviewed centers states that rrt is performed in the case of time interval between primary diagnosis and recurrence > 5years . our last topic of great interest is regarding the management of rt after nac . 
nac is the standard treatment for locally advanced breast cancer at the disease diagnosis and an option for operable disease to allow a conservative surgery ( downstaging and downsizing ) [ 20 ]  . 
several randomized trials have not documented significant differences in disease - free survival and overall survival between primary and adjuvant chemotherapy , identifying the advantage of nac in the best loco - regional treatment of the disease [ 20 ]  . 
data on the predictive factors of loco - regional relapse after nac are rather heterogeneous , but the clinical status of the lymph nodes , the size of the primary breast tumor and the nac response represent the main risk factors [ 50 ]  . 
after primary systemic treatment , the indications to the adjuvant rt and the treatment volumes , even today , are not always well defined because they derive from the results of retrospective studies and from the results of the prospective studies that have not been designed to evaluate the role of postoperative rt after nac . 
although recent studies show that the complete pathological response to nac is a predictive prognostic factor and the results of a combined analysis of nsabp studies 18 and 27 suggest evaluating the indications to rt based on the response to nac [ 51 ] , in our study the factor that mostly seems to influence the indication to the chest wall and the ipsilateral lymph nodes irradiation after nac is the extension of the disease at diagnosis ( ct3 - t4 and / or cn2 - n3 )  . 
 waiting to have conclusive evidence regarding this issue , 1 3 680 la radiologia medica ( 2020 ) 125 : 674682 the multidisciplinary discussion that allows agreeing on the best therapeutic choice for the individual patient remains a milestone . conclusions surveys allow to obtain a real picture of current clinical practice . 
although the percentage of responding centers is relatively low , it is important to highlight that they are highvolume treatment institutes for breast disease and the radiation oncologists who participated in this survey are clinicians actively engaged within airo breast cancer working group . 
regarding the radiation treatment in the management of breast cancer , these data are important considering the incidence , prevalence and complexity of this pathology , in addition to the heterogeneity of the possible clinical contexts and the treatment options that may be pursued . 
future investigations are advocated to establish well - tailored future studies . acknowledgements this study was promoted and supported by the italian society of radiotherapy and clinical oncology ( airo ) breast group . 
also , diseases that mimic the symptoms , signs or imaging characteristics of gca may only be revealed on pathology . bardi and diamantopoulos [ 1 ] conclude that imaging modalities are more sensitive than temporal artery biopsy ( tab ) in the diagnosis of giant cell arteritis ( gca )  . however , the literature on the relative sensitivity of tab versus imaging is conflicting . 
comprehensive reviews suggest that properly performed tab have a sensitivity between 77% [ 2 ] and 87% , [ 3 ] but there may be false positives when the vasculitis is segmental and the specimen does not sample an affected area . 
many of the tab in the tabul study [ 5 ] were substandard ; 7% of the attempted tab did not retrieve a temporal artery , and 43% of the tab specimens were less than 1cm in length . patients with the clinical symptoms and signs of gca can have a myriad of mimicking diseases including syphilis , sarcoidosis , metastases , amyloidosis , zoster , and granulomatosis with polyangiitis , which may not be diagnosed in an expedient fashion without pathology . 
the psa value , tumor adcmin value , tumor diameter , and pi - rads score were compared between the clinically significant and nonsignificant pca groups using students t - test . 
the correlations between the serum psa level , gs , pi - rads v2 score , tumor adcmin value , and tumor diameter were evaluated separately ( pearsons correlation analysis was used for peripheral gland tumors , and spearmans correlation analysis for central gland tumors )  . 
the cut - off values for the peripheral and central gland tumors are as follows : lesion diameter , 13.5mm and 19mm ; tumor adcmin , 0.709 103mm2 / s and 0.874 103mm2 / s ; and psa level , 8.47ng / ml and 11.10ng / ml , respectively . conclusion the current pi - rads v2 scoring system can be inadequate in distinguishing clinically significant and insignificant groups in central gland tumors . 
in low - risk patients with a gleason score ( gs ) of 6 , prostate - specific antigen ( psa ) of < 10ng / ml , and clinical stage of t2a , the prognosis is better , whereas for the high - risk group , the disease has an aggressive progression and causes high rates of metastatic disease and mortality vol . : ( 0123456789 ) 1 3 828 la radiologia medica ( 2020 ) 125 : 827837 [ 2 ]  . 
the aim of pca treatment is to prevent over - treatment by avoiding the unnecessary side effects of radiotherapy , surgery , or hormone treatment in patients with slow progressive disease , as well as preventing under - treatment of those that require an aggressive approach [ 28 ]  . digital rectal examination and psa , a serum tumor marker , are used in the diagnosis and screening of pca [ 711 ]  . 
transrectal ultrasonography ( trus ) - guided 12 - core biopsy is accepted as a standard , but its effectiveness may be limited [ 4 , 5 , 9 , 12 , 13 ]  . 
in particular , anterior tumors may not be detected , or some of the clinically significant cancers can be identified as presenting low risk [ 4 , 5 , 8 , 9 , 1218 ]  . 
therefore , for the evaluation of patients suspected of having pca , multiparametric magnetic resonance imaging ( mpmri ) is recommended , and in cases where necessary , an mri - us fusion biopsy can be undertaken to better determine the characteristics of the tumor [ 46 , 8 , 9 , 12 , 13 , 1921 ]  . 
 a prostate imaging reporting and data system ( pi - rads ) was published in 2012 and revised in 2015 ( pi - rads v2 ) to ensure standardization in obtaining , interpreting and reporting mpmri images [ 22 ]  . the most important prognostic factor in pca is gs and its clinical stage [ 3 , 7 , 23 , 24 ]  . 
the aim of this study was to determine the relationship between the serum psa level , gs , pi - rads v2 score , minimum apparent diffusion coefficient ( adc ) of the tumor , and the largest tumor diameter in patients with pca that underwent rp and to comparatively evaluate these parameters in clinically significant and insignificant groups classified according to gs . materials andmethods the study was performed retrospectively with the reevaluation of prostate mpmri scans performed from january 2015 to february 2019 and obtained from the hospital image archive . 
ten cases for whom there were technical insufficiencies in imaging ( motion artifact , poor quality examination , inappropriate b - value ) or the pathology reports were not available , as well as 13 patients with a pi - rads v2 score of lower than 4 ( pi - rads 1 - 3 ) were excluded from the study . 
 the routine prostate mpmri protocol included triplanar t2 - weighted imaging without fat suppression , diffusionweighted imaging ( dwi ) in the axial plane , fat - suppressed t2 - weighted and pre / post - contrast t1 - weighted imaging in the axial plane , and dynamic contrast - enhanced ( dce ) imaging . 
measurements were performed twice , and the lower mean adc was 1 3 la radiologia medica ( 2020 ) 125 : 827837 table 1 imaging parameters of mri parameters axial t2w sagittal t2w coronal t2w axial t2w fat sat axial t1w sequence tr ( ms ) te ( ms ) slice thickness ( mm ) fov ( cm ) matrix b values ( s / mm2 ) 8300 288 288 10 , 000 288 288 9100 320 320 8500 288 288 352 224 4000 90.4 80 80 0 , 500 , 2000 lava 160 128 t2w t2 - weighted , dwe diffusion - weighted imaging , dce dynamic contrast - enhanced , epi echo planar imaging , fov field of view , fse fast spin echo , nex number of excitations , te echo time , tr repetition time used for evaluation . 
the mri findings were correlated with the pathology results . study design the final gs of the rp specimen of the lesion with the same localization in mri and pathological reports was noted . 
the relationships between the pi - rads score , adcmin value of the tumor , largest diameter of the tumor , serum psa level , and gs were investigated . statistical analysis spss software v.22.0 ( chicago , il ) was used for statistical analysis . 
 students t - test was used to investigate whether the psa value , tumor adcmin value , tumor diameter , and pi - rads score differed between the groups with clinically significant and nonsignificant pca . 
a receiver operating characteristic ( roc ) analysis was performed to evaluate the efficacy of the tumor adcmin , the largest tumor diameter and psa values in differentiating clinically significant and insignificant tumors . 
for the cut - off value of each criterion , the sensitivity and specificity values were calculated at the 95% confidence interval . results a total of 84 lesions were detected in the mpmri of 76 patients ( two lesions in eight patients )  . 
clinically significant pca ( gs 7 ) was present in nine of the central gland lesions ( 60% ) , and clinically insignificant pca ( gs 6 ) in six central gland lesions ( 40% )  . 
at a cut - off value of 0.874 103mm2 / s , we were able to distinguish between clinically significant and insignificant tumors with a sensitivity of 66.7% and specificity of 100% . 
the auc of psa was measured as 0.833 , and at the cut - off value of 11.10ng / ml , this parameter had 77.8% sensitivity and 100% specificity in the differentiation of the two tumor groups . according to the pathology results , 54 of the peripheral gland tumors ( 78.3% ) were clinically significant ( gs 7 ) and 15 ( 21.7% ) were clinically insignificant ( gs 6 )  . 
the psa values significantly differed between the two groups ( p = 0.003 ) , with the patients in the clinically 1 3 832 la radiologia medica ( 2020 ) 125 : 827837 fig . 
the tumor adcmin had an auc of 0.841 , and at the cut - off value of 0.709 10 3mm2 / s , this parameter had a sensitivity of 93.3% and a specificity of 53.7% in the differentiation of clinically significant and insignificant tumors . 
4 receiver operating characteristic ( roc ) analysis for the efficacy of the a tumor adcmin ( auc = 0.841 ) , b tumor diameter ( auc = 0.898 ) , c psa values ( auc = 0.833 ) in differentiating clinically significant and insignificant tumors in peripheral gland tumors discussion psa and gs are traditionally used for risk classification in the diagnosis , treatment and follow - up of pca [ 28 ]  . 
in recent decades , with the increasing use of mpmri , it has been reported that some findings and parameters obtained from mpmri can also contribute to risk classification [ 2933 ]  . 
 in the current study , we evaluated the correlations between the traditional risk factors of psa and gs and parameters obtained from mpmri findings , namely the pi - rads score , lesion size , and calculated adc values . 
we found correlations between psa , gs , pi - rads score , lesion size , and adc values at different levels ( weak , moderate , and high ) in both central and peripheral gland tumors . 
the clinically significant and nonsignificant groups formed according to the final gs were found to significantly differ in terms of the psa value , tumor adc value , tumor diameter , and pi - rads score in all parameters for the peripheral gland 1 3 834 la radiologia medica ( 2020 ) 125 : 827837 tumors , and tumor diameter and tumor adc for the central gland tumors . 
the tumor adc value , lesion diameter , and efficacy of psa in differentiating clinically significant and nonsignificant tumors also differed between the central and peripheral gland tumors . according to the recommendations of pi - rads v2 , determination of the lesion score is based on a subjective evaluation . 
in the literature , many studies used adc values for quantitative assessment of peripheral zone lesions , and an inverse correlation was found between gs and adc values [ 3 , 7 , 23 , 24 , 3340 ]  . 
in some of these studies , the gs data were obtained from a trus - guided biopsy , but it is known that these results are not always consistent with the final gs . 
the final gs is very important in the management of patients , especially in making an active surveillance decision ; therefore , in the current study , the gs obtained from rp was used as reference . 
except for a few studies [ 7 , 24 , 39 ] , a differentiation of clinically significant ( gs 7 ) and insignificant ( gs 6 ) pca was not made . 
in contrast , in the current study , clinical significance was considered when investigating the correlation between gs and various parameters , and the patients were evaluated in two pca groups ( significantinsignificant ) according to gs . 
there was a moderate inverse correlation between the tumor adcmin value and gs in both central zone and peripheral zone tumors , which is consistent with the studies in the literature . 
according to the results of this study , revealing that a low tumor adc value presents a higher possibility of clinically significant tumor , it can be considered to include the adc value , a quantitative mri parameter , in the pirads scoring system or use it as a predictive parameter . 
 although t2 - weighted images are the basic sequence used in the evaluation of central gland tumors , the presence of an inverse correlation between the adc values and gs suggests that diffusion examination has a diagnostic contribution for central gland tumors . 
the tumor adcmin values and the cutoff values determined for adcmin in the current study can be used to differentiate between clinically significant and insignificant disease groups and predict disease progression . the literature contains studies evaluating the diagnostic accuracy of mpmri and pi - rads in the diagnosis of pca [ 20 , 27 , 29 , 34 , 41 ]  . 
no difference was found in the pi - rads ( 4 or 5 ) score between the clinically significant and insignificant groups for the central gland tumors , but these scores significantly differed for the peripheral zone tumors . 
another reason for this result may be that the measurement of lesion size in the central gland is more subjective compared to the measurement undertaken in the peripheral gland due to the faint appearance of the lesion borders in the former . 
based on the results of the current study , it is considered that the pi - rads v2 score can be used to predict the aggressiveness of the disease in peripheral gland tumors . 
for the central gland tumors , however , the validity of the scoring system should be further investigated . in the current study , the psa values were correlated with tumor diameter and gs in both central and peripheral gland tumors . 
 although 10ng / ml is used as a common threshold value , patients with psa values between 2 and 10 are included in the gray zone [ 28 , 42 ]  . 
considering that psa is not an ideal marker and it has low specificity , the prostate health index ( phi ) has recently been developed based on propsa , the isoform of psa , to prevent unnecessary biopsies [ 43 ]  . 
in pca , the determination of a serum psa value higher than normal is not due to the increased production of psa but rather as a result of the deterioration of the prostate structure , leading to elevated psa in circulation . 
our study indicated that more psa was released into the circulation in peripheral gland tumors , which may be due to the different histopathological features of the central and peripheral glands . 
the central 1 3 la radiologia medica ( 2020 ) 125 : 827837 gland being richer than stroma may serve a barrier function in the passage of psa into circulation . in this study , for the differentiation of clinically significant and insignificant lesions , the optimal cut - off value of tumor diameter was determined as 19mm in central gland tumors and 13.5mm in peripheral gland tumors . 
another limitation may be considered as the absence of whole - mount sectioning of specimens with special equipment for the pathological examination ; however , localization was determined according to pi - rads v2 when evaluating the results ; thus , a radio - pathological localization agreement was achieved . 
despite these limitations , the study provided significant data . conclusions in conclusion , in the current treatment approach to pca , it is very important to distinguish clinically significant and insignificant tumors . 
the currently used pi - rads v2 scoring system satisfies this need to a large extent , but it may be inadequate in distinguishing cases with clinically significant and insignificant pca in central gland tumors . 
it should also be noted that when deciding on active surveillance in patients with peripheral gland tumors , it may be necessary to use a lower psa cut - off value than reported in the literature . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical statement all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments os comparable ethical standards . informed consent for this type of study , formal consent is not required . 
the aim of this review is to discuss , in the light of our single - center experience , the technique , current applications , results , and future perspectives of this novel technology . keywords tremor parkinsons disease vim thalamotomy mrgfus functional neurosurgery interventional neuroradiology introduction tremor is the dominant symptom of essential tremor ( et ) and one of the most common motor symptoms of parkinsons disease ( pd )  . 
it has a prevalence of about 6.5% in the population over 65years of age , causing significant disability and limitation in patients daily activities , and resulting in social distress and isolation [ 1 , 2 ]  . 
 tremor can be treated pharmacologically when symptoms * federico bruno federico.bruno.1988@gmail.com 1 department ofbiotechnological andapplied clinical sciences , university oflaquila , via vetoio 1 , 67100laquila , italy 2 radiology department , san salvatore hospital , laquila , italy 3 neurology unit , san salvatore hospital , laquila , italy 4 department ofneurosurgery , san salvatore hospital , laquila , italy 5 neurology unit , department ofmedicine , health andenvironment sciences , laquila , italy become interfering with the patients daily activities , but many of the drugs used have variable effects and carry an increased risk of side effects . 
in fact , while et and pd tremor have different etiology and pathophysiology , several functional neurosurgical treatment showed efficacy in the treatment of the symptoms in both et an pd tremor ; currently available surgical options for the treatment of tremor include deep brain stimulation ( dbs ) , radiofrequency thalamotomy ( rf ) , and radiation therapy ( gamma - knife ) [ 3 ]  . 
these treatments are directed to specific anatomical areas involved in the neurofunctional circuits of movement control , mainly at the level of the thalamus , where the ways of movement control are most represented . 
in particular , the thalamus regulates the motor component through the pallidus - thalamus - cortical ( extrapyramidal system ) and the cerebellum - thalamus - cortical circuits ( regulation of muscle tone ) ; the ventral intermediate nucleus ( vim ) of the thalamus is the target of choice for patients with essential tremor and for some patients with tremorigenic parkinsons disease . 
recently , transcranial thalamotomy using magnetic resonance guided high - intensity focused ultrasounds ( tc - mrgfus ) has emerged as a novel vol . : ( 0123456789 ) 1 3 878 la radiologia medica ( 2020 ) 125 : 877886 minimally invasive ablation method and as an innovative and promising treatment for ablation of deep brain structures . 
ablation by focused ultrasounds , a method already used for the treatment of several pathologies , including uterine fibroids and bone tumors [ 513 ] , does not require open surgical access and determines very precise lesions that can be monitored in real - time using thermometric mr imaging [ 14 , 15 ]  . 
the very recent clinical approval of mrgfus thalamotomy for the treatment of unilateral tremor has led to a rapid expansion of preclinical and clinical research for numerous therapeutic indications in the neurological and neurosurgical fields [ 16 ]  . the system the focused ultrasound system ( neuroablate 4000 , insightec ltd , carmel - tirat , israel ) is integrated into an mr scanner for clinical applications ( 3t mr750w , ge healthcare at our institution )  . 
main contraindications to treatment are represented by the presence of other brain pathologies ( brain tumors , intracranial aneurysms ) , brain or cranial implants ( shunts , electrodes , patches ) that cannot be avoided during treatment , cerebral hemorrhages or seizures in the last year , and non - correctable hemorrhagic risk factors [ 18 ]  . patient preparation the procedure is performed in a hospitalization setting . 
the day of the procedure , the stereotaxic frame is fixed to the skull by screws positioned anteriorly at supraorbital level and posteriorly at the level of the occipital protuberance , after subcutaneous and periosteal injection of a mixture of local anesthetics ( 5ml mepivacaine 2% , 5ml ropivacaine 2% ) [ 19 ]  . 
after stereotaxic frame fixation ( b ) , the patient is positioned with the head into the helmet ( c ) 1 3 la radiologia medica ( 2020 ) 125 : 877886 a fundamental parameter during treatment , given that a low sdr causes less ultrasound transmission and focalization through the skull . 
the fusion of the images allows identifying intracranial calcifications ( choroid plexuses , basal nuclei ) and the areas containing air ( frontal sinuses , folds between the membrane and the skin ) that can block the transmission of ultrasounds and are marked as " no - pass zones " for ultrasound beams . 
 fiducial markers on the three spatial planes are placed to identify any movement of the head during treatment [ 21 ]  . subsequently , the anterior and posterior commissure ( ac , pc ) and the plane passing through them are identified . 
the first ( alignment ) includes short sonications with very low energy ( 15003000j ) , so that the temperature increase is visible in the thermometric maps without creating biological effects ; in this way it is possible to confirm that the sonication point fig . 
in the lower panel , skull score parameters ( sdr , skull area , active elements ) are displayed 1 3 880 la radiologia medica ( 2020 ) 125 : 877886 coincides with the target coordinates , and eventually correct the focus . 
 the second step ( verification ) includes sonications with increasing energy and power parameters to reach higher temperatures ( 4652c ) to obtain a neuromodulation effect , confirming the efficacy of the treatment in the target and the possible presence of adverse effects . 
the clinical response is controlled both during sonication to assess the reduction / disappearance of the tremor , and at the end of each sonication to assess the appearance of adverse effects . 
in the last step ( treatment ) the actual ablationthe energy , the sonication time , and the number of sonications are increased and modulated to reach maximum temperatures of 60c at the level of target . 
 generally , the lesion ( necrosis ) is effective with at least two sonications that have reached temperatures > 56c [ 23 ]  . at the end of the treatment , after draining the water from the helmet and removing the stereotaxic frame , the patient can stand up and undergo a final complete neurological examination before being transferred back to the ward , under observation until the following day . 
the average duration of the treatment , from the positioning to the end of the treatment , is about 3h . target the ventrolateral area of the thalamus has been the main target of stereotactic surgery for the treatment of tremor since the early 1950s . 
the target of choice was shown to be the area of the relay nuclei of the vestibular and proprioceptive afferents fibers , i.e. , the ventral intermediate nucleus ( vim ) according to hassler [ 31 ] , or the ventral and posterior part of the ventral posterior nucleus ( vlp ) , receiving cerebellar afferents , according to hirai and jones [ 28 ]  . 
3 screenshot of the console showing sonication monitoring thanks to thermometric maps ( ac ) and graphs showing energy delivery ( d , e ) and average and maximum temperature reached ( f , g ) 1 3 la radiologia medica ( 2020 ) 125 : 877886 sequences . 
the small vim is still considered " invisible " with the commonly used mr imaging techniques and can be defined more from a functional point of view than from a purely anatomical one . 
for this reason , indirect targeting based on data from stereotactic atlases and data previously obtained from the authors with substantial experience in the field of thalamotomy and deep brain stimulation ( dbs ) still represents the " gold standard " method for target localization [ 32 , 33 ]  . 
i the authors experience , in the case of an important mismatch between the distance from the midline and the wall of the fourth ventricle , we usually set the target by averaging the coordinates of the two landmarks . 
in most of the treatments we performed movement of the target to find the optimal sonication point where to obtain the maximum clinical response without side effects ; the number of shifts with respect to the initial coordinates was very variable from patient to patient , from a minimum of no displacement up to a maximum of 9 movements during a single treatment . 
have used wair ( white matter attenuated inversion recovery ) sequences and found a similar display in terms of shape , spatial orientation and signal contrast of the vim with respect to what is described in some stereotaxic atlases , and have successfully applied the mr findings for targeting direct vim in dbs in patients with essential tremor and parkinsons [ 33 ]  . 
in mrgfus thalamotomy , this limit is overcome mainly since there are no intraparenchymal electrodes , and focused ultrasound beams do not cause tissue damage trough the path , but only at the level of the focal point [ 36 ]  . 
however , precise localization of the target is also fundamental with the use of focused ultrasounds , since repeated sonications outside the target area can still lead to edema and cavitation , with consequent problems in the assessment of the response , in reaching therapeutic temperatures , or in an enlargement of the area of necrosis . 
technological advances in the future will undoubtedly be able to obtain a better visualization of the target structures , with the implementation of mr sequences such as tractography , to obtain a reduction in the duration of the procedure and the incidence of adverse effects [ 34 , 37 ]  . results the first study to report its experience in the use of mrgfus for thalamotomy described an immediate and persistent improvement in tremor in 4 treated patients , with a 90 - day follow - up [ 24 ]  . 
adverse effects reported were paresthesia of the tongue and lips ( in 9 patients , persistent at follow - up in 2 ) , balance disorders ( 5 patients ) , and gait ( 4 patients , with complete resolution at 1 - month follow - up )  . 
the safety and efficacy of the vim thalamotomy with ultrasounds have been validated by three clinical studies that have shown significant improvement in the tremor of the contralateral hand and reduction in the related disability [ 15 , 24 , 25 ]  . 
presented long - term results at 5years in a cohort of 44 et patients [ 27 ] ; their results showed a reduction in crst scores in the treated hand from the baseline ( median 19 ; range 732 , 44 patients ) to a median of 17 at 6months ( 31 patients ; p < 0.0001 ) , 15 at 1year ( 24 patients ; p < 0.0001 ) , 18 at 2years ( 15 patients ; p < 0.0001 ) , 19 at 3years , ( 10 patients ; p < 0.0001 ) , 21 at 4years ( 6 patients ; p < 0.01 ) , and 23 at 5years ( 2 patients )  . 
clinical evaluation in pd patients included also the updrs ( unified parkinsons disease rating scale ) score , with particular reference for its part iii ( motor examination )  . 
the clinical scores were recorded before treatment , immediately after treatment and with follow - up at 1 , 6 , and 12months . treatment was effective ( substantial and immediate reduction in the tremor ) in 49 patients out of 50 ( 98% )  . 
in the patient where treatment was not effective , the procedure was suspended early due to the onset of unsustainable side effects ( nausea , headache ) and the impossibility to reach ablative temperature with increasing sonication parameters . 
at the clinical follow - up , they found a progressive improvement in the updrs score by 34.1 at 1 month , 1 month , and by 46.2% at 6 months ( p = 0.009 ) , and with a parallel improvement in the quality of life scores . 
thalamotomyrelated complications from our experience occurred in 8 patients ( 16% ) , reported in table2 . imaging followup adverse events the most frequent adverse events related to sonications reported in the literature are represented by vertigo , lipotimia , headache , nausea , and scalp burning [ 29 ]  . 
the first area is represented by a central hypointense spot ( not always appreciable ) surrounded by a hyperintense zone demarcated by peripheral table 2 thalamotomy - related complications post 1 month 3 months 6 months 1year perioral paresthesia perioral paresthesia ataxia dysartria , ataxia hemiparesis dystonia , hemiparesis resol perioral paresthesia perioral paresthesia perioral paresthesia resol dysartria , ataxia hemiparesis hemiparesis perioral paresthesia perioral paresthesia perioral paresthesia dysartria , ataxia ( improving ) hemiparesis ( improving ) perioral paresthesia resol perioral paresthesia dysartria , ataxia ( improving ) resol perioral paresthesia u under follow - up , resol resolution 1 3 884 la radiologia medica ( 2020 ) 125 : 877886 hypointense border ( zone 2 ) , and finally a blurred hyperintense area of more peripheral vasogenic edema ( zone 3 )  . 
susceptibility weighted sequences ( swi ) show the presence of hemoglobin derivatives at the level of the lesion core , which often persists even when other mr findings are reduced . 
 the same authors [ 21 ] report how , with a 3 - month followup , the perilesional edema tends to increase in the first week after treatment , and the size of zones 2 and 3 are progressively reduced within the first month . 
however , from the results of the previous studies there is no statistically significant correlation between the imaging characteristics and the number of sonications , the final energy delivered and the temperature reached , while there is a correlation between the extension of the vasogenic edema and its resolution with the presence of side effects such as paresthesias [ 39 ]  . 
 these data suggest the possibility of possibly repeating mrgfus treatment in patients with sub - optimal benefit after a first procedure , or in patients with symptom recurrences , as reported in a case described by weidman etal . currently , the use of focused ultrasound is limited to unilateral treatment . 
the enormous technical advantages of thalamotomy with mrgfus in terms of control of the effects , precision and predictability of the lesion , suggest that the use of this method in bilateral treatment , even in staged treatment sessions , merits further studies to improve the therapeutic outcome in patients with both limbs tremor or axial tremor [ 42 ]  . conclusions to date , tcmrgfus has been mainly applied in the treatment of movement disorders , it has enormous potential for application in all pathological conditions that can be treated with a stereotaxic functional neurosurgical approach . 
this application , which uses intermediate levels of energy combined with pulsed sonications and the use of circulating microbubbles injected intravenously , may allow an increase in the release of chemotherapy for the treatment of brain neoplasms [ 43 , 44 ]  . the scientific publications and clinical experiences of recent years with focused ultrasounds have enormously increased the awareness of the therapeutic potential of this method and will further accelerate the application of this innovative , versatile , and multidisciplinary technology . 
 being still an innovative and growing technique , tcmrgfus has the potential to become the primary method for new therapeutic approaches in an ever - increasing number of neurological and neuropsychiatric pathologies , drastically revolutionizing the future management of many patients . funding no financial support was received for this paper . compliance with ethical standards conflict of interest the authors have no potential conflicts of interest to disclose . human and animal rights all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the main histotypes are pleomorphic adenoma ( 70% ) and warthin tumour ( 15% ) ; epithelial malignancies ( 510% ) and lymphoma ( 23% ) are rare [ 2 ]  . 
although the diagnostic accuracy of the histological examination of salivary gland neoplasms is high [ 3 ] , * stefano colagrande stefano.colagrande@unifi.it extended author information available on the last page of the article there is an overlap between benign and malignant tumours [ 4 ]  . 
magnetic resonance imaging ( mr ) with contrast agent allows a correct locoregional staging of salivary neoplasms [ 5 ] and provides useful information regarding their characterization [ 6 ]  . 
in the last years , there has been growing interest in diffusion - weighted imaging ( dwi ) and dynamic contrast - enhanced perfusion - weighted imaging ( dce - pwi ) mr sequences in oncological imaging [ 913 ]  . 
an overlap of apparent diffusion vol . : ( 0123456789 ) 1 3 852 la radiologia medica ( 2020 ) 125 : 851863 coefficient ( adc ) values between benign and malignant neoplasms was observed [ 22 ]  . 
most of the published studies showed that dce - pwi parameters , such as time resolutions less than 10s , wash - in < 120s , and wash - out ratio > 30% , are the best parameters to characterize salivary glands neoplasms [ 30 ]  . 
however , to our knowledge the association of these parameters has never been explored to better characterize these neoplasms . we aimed at retrospectively evaluating the usefulness of the association of dwi and dce - pwi sequences in the characterization of salivary glands neoplasms with the abovementioned parameters . methods andmaterials from february 2014 to january 2019 , all patients with histological diagnosis of salivary glands neoplasms who underwent head and neck mr in the radiology department of careggi hospital ( florence , italy ) were retrospectively included . 
the mr acquisition protocol was the same for all the examinations , as follows : from 0.9 to 3 - mm slice thickness , field of view ( fov ) 230 200 / 240mm , matrix from 230 256 to 261 484 . 
sagittal t1 - w sampling perfection with applicationoptimized contrasts using different flip angle evolution ( space ) , repetition time ( tr ) 500ms , echo time ( te ) 7.2ms , acceleration factor 2 , at axial , coronal , and sagittal multiplanar reconstructions ( mpr ) ; 2 . 
fat - saturated eco - planar ( epi ) dwi ( see below )  . after gadolinium chelates contrast agent intravenous administration ( gadobutrol , bayer , germany ) 1ml / 10kg 1 3 la radiologia medica ( 2020 ) 125 : 851863 followed by 20ml saline flush at a rate of 3ml / s , we acquired 5 . 
axial t1 - w turbo spin echo , tr 440 ms , te 17 ms , acceleration factor 3 , and axial t1 - w volumetric interpolated breath - hold examination ( vibe ) , and 6 . 
dixon dce - pwi , tr 10ms , te 2.4ms at axial , coronal , and sagittal mpr ( see below )  . dwi protocol andpostprocessing dwi was obtained by fat - saturated epi technique , tr 4100ms , te 55ms , and two b values ( b50 - 800s / mm2 ) , matrix 102 128 , and acceleration factor 3 . 
adc values were divided into three groups : high values 1.4 103 , intermediate values 0.91.4 10 3 , and low values < 0.9 103mm2 / s [ 1 ]  . 
before lesion sampling , an roi was placed on the internal carotid artery to obtain the arterial input function curve , defined as the contrast concentration in vessels feeding to tissue at each point in time during the contrast passage . 
 [ 30 ] : type a curve : slow and progressive wash - in , type b curve : rapid wash - in and wash - out , type c curve : rapid wash - in and slow wash - out , type d curve : absence of enhancement ( flat curve )  . wash - in was progressive ( or rapid ) if the maximum concentration of the contrast agent was reached after ( or before ) 120s , respectively . 
wash - out degree was evaluated by washout ratio at 300s with the following formula : dcepwi protocol andpostprocessing [ ( simax si5 min ) ( simax sipre ) ] 100 ( % ) dce - pwi was obtained through two vibe t1 - w sequences , 3.5 - mm slice thickness , 0.7 interslice gap , fov 250 226 mm , matrix 139 192 , flip angles 5 and 15 , and acceleration factor 3 for baseline t1 - mapping acquisitions . 
 [ 1 ] , the association of the type a curve and adc values 1.4 103mm2 / s was tested as parameter of benignity , whereas the association of the type c curve and adc values 0.91.4mm2 / s was considered as parameter of malignancy . 
a type d curve was indicative of a benign neoplasm , whereas a type b curve was not used as a parameter reference . observers andstatistical analysis all examinations were separately evaluated by two independent radiologists with 12 and 7years of experience in head and neck imaging , respectively . 
cystic components of the tumour ( dotted arrow ) had adc values 1.4 103 mm2 / s b time / intensity curve characterized by a rapid wash - in and rapid wash - out ( type b curve )  . 
the diagnostic accuracy of the association of adc values < 0.9 103mm2 / s and a type b curve was very high for the diagnosis of warthin tumour 1 3 la radiologia medica ( 2020 ) 125 : 851863 fig . 
a the lesion showed heterogeneous low t2 signal intensity , b vivid enhancement on standard post - contrast imaging , and c average apparent diffusion coefficient ( adc ) values around 1.1 103 mm2 / s . 
d dynamic contrast - enhanced perfusion imaging ( dce - pwi ) showed adenoid - cystic carcinoma in the left submandibular gland with high ktrans values ( roi 1 in red )  . 
e dce - pwi time / intensity curve of the lesion characterized by a rapid wash - in and slow wash - out ( type c curve ) 1 3 858 discussion in our series , the efficacy of tic in the characterization was assessed by high - quality temporal resolution parameters ( time resolution 5s , wash - in < 120s , and wash - out > 30% )  . 
all lymphomas ( one diffuse b - cell , two mantel cell , and one malt non - hodgkin lymphomas ) showed low adc values < 0.9 103mm2 / s and a type c curve . 
conversely , a significant overlap for adc values < 0.9 103mm2 / s was observed between warthin tumour and lymphoma , as reported in the literature [ 14 , 17 , 2527 , 31 ]  . 
approximately , 60% of the benign neoplasms showed adc values < 1.4 103mm2 / s , including all sixteen warthin tumours , six pleomorphic adenomas with rich cellular component , and two basal cell adenomas characterized by a high cellular density and nucleo - cytoplasmic ratio . 
axial magnetic resonance images highline an oval , lobulated and well - defined lesion in the right parotid gland with pathognomonic signal features : homogeneously hypointense on t1 - weighed ( w ) sequence ( a ) , hyperintense on t2 - w ( b ) , low signal on diffusion - weighted imaging with b - 800 s / mm2 ( c ) , and very high values ( > 2 103 mm2 / s ) on apparent diffusion coefficient map ( d )  . 
perfusion - weighted imaging shows low ktrans values ( e ) , and type a time / intensity curve ( f ) 1 3 la radiologia medica ( 2020 ) 125 : 851863 neoplasms with values 1.4 103mm2 / s , as reported in the literature [ 1 , 14 , 15 ]  . 
 [ 1 ] , reflecting mixed areas of high tumour cells density and necrosis . in the present study , a type a curve was observed only in benign neoplasms and in 80% of pleomorphic adenomas . 
many studies [ 2024 , 30 ] stated that epithelial malignancies show a rapid wash - in and slow wash - out ( type c curve ) , pleomorphic adenoma has a slow and progressive wash - in ( type a curve ) , and warthin tumour presents a rapid wash - in and wash - out fig . 
axial magnetic resonance images show a rounded lesion in the left parotid gland with heterogeneous signal on t1 - weighed ( w ) sequence for the presence of hyperintense intralesional foci indicative of haemorrhage and / or cholesterol ( a ) , cystic areas with hyperintense signal on t2 - w ( b ) , high signal on diffusion - weighted imaging with b - 800s / mm2 ( c ) , and low values ( 0709 103 mm2 / s ) on apparent diffusion coefficient map ( d )  . 
perfusion - weighted imaging shows intermediate ktrans values ( e ) and type b time / intensity curve ( f ) 1 3 860 la radiologia medica ( 2020 ) 125 : 851863 ( type b curve )  . 
in the literature , different wash - in temporal references were reported ( 120s [ 2931 ] , 150s [ 23 ] , 165s [ 18 ] , and 210s [ 20 ] ) depending on different temporal resolutions . 
although dce - pwi parameters with the highest diagnostic accuracy [ 30 ] were used in the current study , accuracy of the association of dwi with dce - pwi for the detection of salivary malignant neoplasms was 82.1%. 
this value was similar to that found in previous papers , in which accuracy in distinguishing between benign and malignant neoplasms varied from 67 to 90% [ 1 , 1820 , 2731 , 33 , 34 ]  . 
the great variability in diagnostic accuracy could also be explained by the different number of lymphomas analysed in several studies , varying from 1 to 4 [ 1 , 14 , 15 , 17 , 26 , 27 , 31 ]  . 
indeed , lymphoma almost always showed adc values < 0.9 10 3mm2 / s , and therefore , they were not included in the adc range values generally considered in the literature as an index of malignancy [ 1 , 17 , 26 , 27 , 30 , 31 ]  . generally , tumours with well - defined borders tend to be benign , whereas irregular borders are suspicious for fig . 
axial magnetic resonance images show an ill - defined lesion in the left parotid gland with low signal on t1 - weighed ( w ) sequence ( a ) , very low signal on t2 - w ( b ) , intermediate signal on diffusionweighted imaging with b - 800 s / mm2 ( c ) , and intermediate values ( 1 103 mm2 / s ) on apparent diffusion coefficient map ( d )  . 
in our opinion , radiologists should not overlook conventional t1 - w and t2 - w sequences since these sequences are crucial not to incur errors in the interpretation of dwi and dec - pwi sequences for the identification of salivary glands neoplasms ( table5 )  . our study has some limitations . 
first , we used small rois to measure adc values , since this method has been reported to have lower interobserver reproducibility than sampling the entire volume of the lesion [ 9 , 10 ]  . 
however , small rois are easier to use in clinical practice and allowed us to get adc values comparable with most previous papers [ 1 , 17 , 26 , 27 , 30 , 31 ]  . 
nevertheless , since low - grade neoplasms reached smax before 120s in both the current study and ogawas paper [ 40 ] , it would have no impact on our results . 
 quantitative studies that assess the dynamic of passage of the contrast agent from the vascular to the extra - cellular systems could play an important role in the distinction between benign and malignant neoplasms . 
texture analysis examines the grey - scale distribution among voxels and could be useful to characterize salivary glands tumours in case of any doubts persisting after dwi and dce - pwi [ 41 , 42 ]  . 
future research should deal with the combination of functional and morphological data , as it could have a further increase in mri accuracy for the characterization of salivary glands neoplasms . conclusions in our study , the association of high adc values 1.4 10 3mm2 / s and a type a curve was found only in benign neoplasms , whereof most were pleomorphic adenomas . 
all lymphomas showed low adc values < 0.9 103mm2 / s and a type c curve . acknowledgements the authors have no financial affiliation ( employment , direct payment , stock holdings , retainers , consultantships , patent licensing arrangements , or honoraria ) , or involvement with any commercial organization with direct financial interest in the subject or materials discussed in this manuscript , nor have any such arrangements existed in the past 3years . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
ptcs are indolent differentiated cancers associated with low mortality and morbidity [ 2 , 6 , 7 ] , and some ptcs show aggressive behavior and recurrence [ 714 ]  . 
the risk factors and indicators of an advanced ptc include male sex , old age , increased tumor size , and extrathyroidal extension ( ete ) [ 6 , 7 , 1015 ]  . 
 the practice guidelines of the american thyroid association recommend total thyroidectomy for patients with ete and postoperative radioactive iodine ablation for patients with high - risk ptc [ 10 , 11 , 15 , 17 , 18 ]  . ete is the tumor growth outside the thyroid gland and into the nearby or surrounding tissues . 
the seventh edition of the tnm classification for thyroid carcinomas of the american joint committee on cancer divides ete vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 870876 into minimal ete ( extension to sternothyroid muscle or perithyroid soft tissues ) and extensive ete ( extension to subcutaneous soft tissue , larynx , trachea , esophagus , recurrent laryngeal nerve , or prevertebral fascia or encases the carotid artery or mediastinal vessels ) [ 17 ]  . preoperative detection of ete is very important , not only for adequate nodal staging but also for surgical planning [ 6 , 7 , 12 , 13 , 16 ]  . 
several studies have demonstrated the superiority of various imaging tools , including us , ct , and mri , in ete assessments [ 8 , 15 , 1924 ]  . 
previous studies on the diagnostic performance of preoperative us for the determination of ete of ptc reported many advantages , such as high - resolution imaging capability and ease of accessibility [ 15 , 1925 ]  . 
the aim of this study was to evaluate the feasibility of high - resolution us and mri scans in predicting ete in patients with ptc . materials andmethods study population this retrospective study was approved by the institutional review board , and written informed consents were waived . 
 a search on the hospitals database identified 233 consecutive patients with surgically confirmed ptc who underwent preoperative thyroid us and mri at our institute between may 2014 and december 2018 for ptc evaluation . 
among the 233 patients , eight were excluded for the following reasons : poor - quality mri ( n = 2 ) , small - sized masses ( i.e. , too small to be identified using mri , n = 3 ) , and preoperative thyroid diffusion - weighted imaging ( dwi ) performed at another hospital ( n = 2 )  . 
finally , 225 patients ( 82 males and 143 females ) with a mean age of 37.95years ( range 2073years ) and 246 thyroid masses ( a single mass in 204 patients and two masses in 21 patients ) were included in this study . 
the spin echo - based t1wi sequence ( repetition time ( tr ) / echo time ( te ) = 520 / 14 ms ) in axial view , the fast spin echo - based t2wi sequence ( tr / te = 3500 / 95ms ) with and without fat suppression in axial and coronal views were employed for imaging acquisitions . 
 dwi was acquired at two different b values ( 0 and 500s / mm2 ) using the stir fat - suppressed single - shot echo planar imaging spin echo sequences in three orthogonal directions . 
 the shimming adjustment has also been properly applied in the thyroid region prior to image acquisition , so that the neck area which is sensitive to local field in homogeneities can be visualized with accepted image quality . 
of all patients , contrast enhanced t1wi ( tr / te = 520 / 14ms ) was obtained with or without fat - suppression immediately after the intravenous injection of 0.1mmol / kg gd - dtpa at an injection speed of 1.5ml / s , ( magnevist , schering ag , germany )  . 
the parameters were as follows : section thickness 3mm , with a 1 - mm intersection gap , field of view ( fov ) = 40 28cm2 ; matrix = 256 256 , nex = 4 . 
all us and mr images were retrospectively and independently reviewed by the two radiologists with regard to minimal ete and invasion into the surrounding tissue of trachea , esophagus , common carotid artery ( cca ) , internal jugular vein ( ijv ) , and recurrence laryngeal nerve ( rln ) [ 8 , 1923 ]  . 
the radiologists 1 3 872 la radiologia medica ( 2020 ) 125 : 870876 were blinded to the surgical and pathological findings , but they were informed about the location and size of the index malignancy in patients with thyroid lesions . 
both reviewers worked independently and were blinded to the patients information , including clinical history , previous radiological findings , and final diagnosis . the ete of ptcs was classified according to the guidelines of the american joint committee on cancer [ 17 ]  . 
 according to these guidelines , minimal ete was defined as more than 25% of the perimeter of the lesion in contact with the thyroid capsule or loss of the echogenic capsule line at the contact site of the lesion . 
extensive ete was defined as the extension of a tumor of any size beyond the thyroid capsule and invasion of the subcutaneous soft tissues , larynx , trachea , esophagus , rln , cca , or mediastinal vessels [ 8 , 15 , 1925 ]  . statistical analysis after surgery , the pathological results were compared with the us and mri findings , and an agreement between the pathological findings and those of usand mri - identified ete was reached . 
a p value < 0.05 was considered statistically significant . results clinicopathological features according tothepresence ofete all patients with ete underwent total ( n = 40 ) and lobe ( n = 45 ) thyroidectomies . 
among these 85 patients , 47 patients with 80 masses had minimal ete , and 38 patients with 48 masses had extensive ete according to the surgical and histopathological findings . 
significant differences were not observed in the clinical features in terms of patient age , sex , location , mean maximum size , lymph node metastasis , and surgical procedure in the ptc cases with and without ete . 
figures1 and 2 show us and mri images of ptcs with minimal and extensive ete , respectively . diagnostic performances ofus andmri inassessing table3 shows the diagnostic performances of us , mri , and the combined set for the evaluation of minimal , extensive , 1 3 la radiologia medica ( 2020 ) 125 : 870876 fig . 
a transverse view of us image shows the lesion locally protruded thyroid capsule ( arrow ) , b doppler shows abundant blood flow signals in the peripheral and internal areas , c t2wi image , d fat - saturated t2wi image , e contrastenhanced t1wi image show the lesion the locally protruded thyroid capsule ( arrow ) , and f histopathological h&e ( total magnification , 10 ) image of a ptc showing minimal ete ( extension to sternothyroid muscle )  . 
a transverse view of us images shows a mass near the trachea ( blue arrow ) and the tumor is completely enveloped by thyroid parenchyma , b doppler shows abundant blood flow signals in the peripheral areas , c t2wi image , d fat - saturated t2wi image , e contrast - enhanced t1wi image show the tumor the locally protruded trachea ( arrow ) , and f histopathological h&e ( total magnification , 10 ) image of a ptc showing extensive ete ( encases trachea )  . 
in the present study , current data showed that us had higher sensitivity and npv than mri in assessing minimal ete , whereas mri had higher sensitivity than us in assessing extensive ete and higher specificity and ppv in assessing overall ete . 
preoperative us should be used as the first line in minimal ete prediction , and mri should be added in extensive ete assessment . the presence of ete is considered important and is included in almost all prognostic scoring systems as a staging variable . 
at present , preoperative us is the first investigation performed in staging ptcs , because it is relatively inexpensive , well tolerated , noninvasive , and requires no contrast agents . 
mri may also be used to assess the thyroid and nodes in the upper mediastinum when the inferior extent of disease cannot be identified using us [ 20 , 24 ]  . 
the early stage of tracheal invasion is more difficult to identify when using us than mri , because mri enables superior visualization of the tumor invasion into the central region of the aerodigestive tract , an area where detail is obscured on us due to the air in the trachea [ 24 ]  . 
unlike us , mri depicts fatty tissues in the tracheal esophageal groove due to the presence of beam - hardening artifacts caused by the clavicle and the presence of dense contrast material in the subclavian vemri is a useful method in predicting rln invasion , but it is limited by ptc size and location of rln invasion [ 24 ]  . the present study had several limitations . 
therefore , the overall accuracy rates for us alone , mri alone , and us plus mri in predicting ete cannot be estimated . in conclusion , although mri can be valuable in assessing the invasion of adjacent structures ( esophagus or trachea ) , us was selected as the first modality in evaluating minimal ete , because us is inexpensive and can predict the minimal ete of ptc . 
although mri scan had certain limitations in evaluating tiny thyroid nodules , the additional information that can be obtained from mri can increase the prediction of extensive ete of ptc . 
the method is promoting researches in areas that have not been fully addressed before in the cardiovascular system , such as flowmetry of the bloodstream across the valves , within the heart chambers , complexed flow dynamics such as vortex , helical or retrograde . 
in this review , fundamental concepts of 4d flow technique and post - processing , benefits and limitations as well as its clinical applications are discussed , and the importance of quality control and validation of the method is emphasized . 
new ideas inspired by 4d flow can help clinicians and mr scientists further understand the role of flow dynamics in health sciences , diseases and various aspects of cardiovascular physiology . keywords phase - contrast image 4d flow magnetic resonance flow analysis wall shear stress cardiovascular diseases introduction leonardo da vinci , a universal genius who played an active part five hundred years ago in italy , has been known to have an unusual interest in flow . 
three - dimensional ( 3d ) cine phase - contrast mri ( pc ) or 4d flow mri ( fig.1be ) is a new mr technique that can measure the moving speed of hydrogen nuclei ( protons ) in a region of interest in 3d fashion and phase - resolved manner with ecg gating if you wish [ 2 ]  . 
when gradient magnetic field is applied to an axis , for example , the x - axis direction , then the resonance frequency of the protons is linearly changed along the x - axis . 
following this maneuver , another gradient magnetic field with the same strength but in the opposite direction is applied along the x - axis , and then , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 838850 fig . 
d a color - coded 3d vorticity map and e 3d energy loss map can be calculated and displayed the same phenomenon occurs in the - x - axis direction . 
for protons moving on the x - axis ; however , the phase shift applied with the first magnetic field gradient cannot be canceled by the opposite gradient magnetic field , because they do not experience exactly the same local magnetic field and resultant phase shifts . 
the proton standing still experiences phase shifts due to the additional positive gradient to original static magnetic field strength ; however , the phase shift is canceled by the subsequent negative gradient of equal strength . 
when a proton is moving along the x - axis , it will experience additional static magnetic field strength , so the balance of phase shift becomes negative instead of zero . 
 phase - contrast image replaces this augmented phase shift ( = velocity ) value with signal intensity obtained phase difference is too small , which is responsible for a poor snr , thereby resulting in poor velocity resolution . 
it is because the wall shear stress ( wss ) is a differential expression of the velocity gradient that changes as it approaches the wall . there are many methods to characterize and visualize flow . 
such data require reference and three flow - encoded excitations ( vx , vy and vz ) for each phase - encoding view , spatial resolution , especially in the slice section - encoding direction , which makes its imaging time prohibitively lengthy . 
osi is parameter of fluctuation for the wss calculated by the formula shown in fig.7b. since the blood vessel is a three - dimensional structure , it is challenging to measure the wss near the vesselwall in 2d fashion . 
unlike other modality like doppler ultrasonography , the blood flow velocities of any vessels can be measured with arbitrary measurement sections evenafter patients left 1 3 842 la radiologia medica ( 2020 ) 125 : 838850 fig . 
the merit of this function is maximized in measuring the flow of each arterial branch of the transplanted kidney [ 5 ] or flow analysis for possibly responsible arteries for type ii endoleak after endovascular repair ( evar ) for the abdominal aortic aneurysm [ 6 , 7 ]  . 
an attempt to measure the flow velocity and flow rate of certain blood vessels using the mr technique started 30years ago , which had been an initial boom of mr flowmetry . 
among these studies , some researchers noticed the fluctuations in the measured flow velocity [ 17 ] , but the discussion has not been sufficiently doneon the reasonwhy the fluctuations of the blood flow velocities occur . 
5 since all the 4d ( velocity in x , y , z + cardiac phase resolve ) data are acquired en bloc , many types of visual post - processing are available . 
flow visualization employed in fluid dynamics is used to make the flow patterns visible , to get qualitative or quantitative information on thea 3d vector field is an assignment of a vector to each point in a subset of space . 
d pathline or particle trace is a similar expression , but it connects velocity vectors moving to time ( cardiac phases ) , which suggest the trajectory of the fluid movement thetime velocitypatterns measured at the similarmeasurement planes before and after the intervention was different . 
 with a close look at the streamline ; however , it was easy to understand that the vortices in the post - dilated segment of the renal artery were responsible for this fluctuation . 
therefore , when we measure the flow velocity and flow rate of specific vessels , we first perform streamline analysis with 4d flow and then determine the measurement planes that canavoid abnormal flow . 
 [ 20 ] found a fairly large whirlpool in the left atrium and theventricle ( fig.10 ) of the healthy volunteers , which was observed more often in individuals with normal cardiac function rather than degraded cardiac function [ 21 ]  . 
observing the streamline , it is noted thatthese low wss was created by nonlaminar flow , i.e. , turbulent or vortex flow la radiologia medica ( 2020 ) 125 : 838850 the kinetic energy is justconverted into heat , resulting in an energy loss ( fig.1e ) , which seems to becontributing nothing to blood circulation . 
however , it could also be assumed that the whirlpools in the heart may be helpful in maintaining the momentum of the flow during diastole , which may be analogous to the rational function of the vortices within the valsalva sinus for aortic valve closure well depicted by da vinci . vortices in the pulmonary trunk are related to pathological status . 
for the quality control of the mr system , there is a simple flow phantom analysis using a straight tube and a steady constant streaaccording to fukuyama etal . , 4d flow data acquisition should be 1 3 la radiologia medica ( 2020 ) 125 : 838850 fig . 
arterial wall shear stress over 1.5 pa is said to be required for atheroprotective effect , while vortex , turbulent or spiral flow with low velocity or low shear stress less than 0.4 pa stimulates an atherogenic phenotypes and apoptosis of vascular smooth muscle cells , which promote atherosclerosis . 
atherosclerosis ultimately leads arterial wall to various sorts of vascular diseases including aortic aneurysm or arteriosclerosis obliterans performed with a spatial resolution of a certain level or more [ 23 ]  . 
the error of the average flow velocity will be within 10% or less when a measured voxel is 30% or less than the cross - sectional area of the measured vessels . 
in the smaller tube of 3mm in diameter , when the voxel size was 0.67mm ( 22% of the straight pipe ) , the error of the cross - sectional average flow velocity increased up to 20% . 
some researchers have started to use compressed sensing [ 24 ] and deep learning [ 25 ] to reduce noise effectively . we also use in silico simulation , i.e. , cfd for the validation of 4d flow ( fig.9 ) , which is the theoretical simulation of flow dynamics using the navierstokes equation . 
to date , the cfd analysis of cerebral aneurysms is reportedlysimilar to the findings by 4d flow [ 26 ]  . the limitations of4d flow there are several limitations concerning the flowmetry with 4d flow . 
this is a problem that is often encountered solong as data are collected with use of ecg gating.therefore , it is challenging to reproduce other transient flows and fluctuations caused by respiration . 
to measure this type of abnormal renal flow dynamics , the area under the curve should be measured after an appropriate temporal resolution venc setting is too low , aliasing will occur , and if it is too high , the snr of the flow rate will deteriorate . 
for this purpose , sparse imaging such as compressed sensing and kt has already been applied , and in the future , it is desired to collect data with improved snr and improved spatial resolution by using deep learning [ 27 ]  . 
streamline analysis of the whole heart in a left anterior oblique view and b right anterior oblique view 1 3 la radiologia medica ( 2020 ) 125 : 838850 848 fig . 
there is mostly laminar flow in the normal pulmonary artery ; however , in the pulmonary hypertension , a helical flow within the right pulmonary artery and the vortex flow in the main trunk of the pulmonary artery ( arrows ) are dominant fig . 
along with this new initiative , the new concept of pandemic radiology unit was implemented as a practical solution to the emerging crisis , born out of a critical and urgent acute need . 
the present article describes logistics , planning , and practical design issues for such a pandemic radiology and critical care unit ( e.g. , space , infection control , safety of healthcare workers , etc . ) adopted in the ic hospital unit for the care and management of covid - 19 patients . keywords covid - 19 sars - cov - 2 radiology pandemic hospital introduction the coronavirus disease 2019 ( covid - 19 ) pandemic began in late 2019 in wuhan , china . 
this response is led by the italian national government in coordination and synchrony with local ( or regional ) governments and hospitals . the major hot spot of covid - 19 patients have thus far been in the north of italy , especially in the region of lombardy . 
this is not a camp hospital or acute triage fever clinic , but a real brick and mortar hospital focused on intensive care and intensive triage of the critically ill cases . 
all the services ( laboratories , radiology , etc . ) necessary to an independent functioning of over dedicated ic 200 beds were allocated in the same building with a strategic position . 
the present article describes the logistical setting , strategy , and organization for radiology services in a new dedicated covid - 19 critical care and critical triage hospital . hospital a well - equipped dedicated hospital facility to deal with covid - 19 patients with adequate protective equipment and policies for healthcare workers is the key to successful delivery of safe and optimal public health care in the setting of a pandemic . 
the hospital was designed to be practically a self - contained and self - sufficient establishment that can meet most of its daily needs with only essential and limited contact with the outside world , via predetermined limited channels for such critical pipelines as nutritional services and other supply chains . 
beds are contained in modules ( from a to h as shown in the map ( fig.2 ) ; in each module , 7 or 14 beds are located , depending on floor ) , with controlled access and unified connections to each other . 
beds are sequestered from each other as much as possible , to avoid cross - contamination , in case of different strains of covid - 19 or differing superinfections with more standard microorganisms . 
part of the radiological services is also located in red zones ( like ct , us , etc ) , laundry , access for patients , and patient triage is all located in the red zone also . 
such a staged space designation is analogous to the ante - room concept for staged doffing ppe , whereby the doffing occurs in staged locations , in very specific sequences , from very dirty to less dirty to more likely clean , in order to minimize human error and exposures . 
 likewise it is wise to designate staff as coordinators for traffic control and communications of transport issues , and educators for dissemination of sops and new policies and practicing , and runners whose sole responsibility is to transfer equipment or supplies from a clean supply or storage space to a dirty procedure room , along predetermined and pre - practiced chains of transfer and chains of communication . green zones , as illustrated in the map ( fig.1 ) , are represented by an external perimeter , surrounding the red zones . 
attention to donning and doffing education , practicing , training , and standard sops is critical to safe operation of such a covid - 19 facility . radiology service radiology unit is present in both red and green zones . 
 in the red zones are located ultrasound ( us ) machines , one for each module ; portable radiography is repeatable 1 3 896 la radiologia medica ( 2020 ) 125 : 894901 fig . 
lab laboratory , hcw healthcare workers , * donning ppe point , * * doffing ppe point and easy to decontaminate and serves as the mainstay imaging tool for emergency departments and inpatient settings . 
two ct machines are present , one for each floor : they are located in the red zone and closer to the triage to permit immediate access to the ct room , even for patients just admitted . 
a little room with a workstation is located closer to the ct room , but staffs are encouraged to do remote communications , remote interpretations , and remote consults whenever possible . 
in the green zone , a radiology office is present , in which 2 workstations are available to allow radiologists and residents to interpret images , do reconstructions , make a report , and be accessible via remote communications to the red zone staff . 
a workstation dedicated to artificial intelligence ( ai ) is also available to permit studies on chest x - rays and ct scans , for research purposes and point of care applications of novel approaches to multi - parametric data integration , all with regulatory clearances and a network of multinational partnerships . as directed by government policies , guidelines , and procedures , surgical masks must be worn by anyone who leaves home . 
screening may occur upon entry to the hospital , entry into the green zone , or entry into the red zone . all healthcare workers involved should have extensive knowledge and training in the correct donning and doffing steps , along with appropriate and safe disposal of ppe . 
videos and guidance during the donning and doffing were dedicated for every operator , and each operator was trained by senior mentor , until he / she became fully independent with verifiable metrics and certification by a mentor . 
careful hand hygiene , correct wearing of protective equipment , and strict adherence to infection control procedures ensured continued 1 3 la radiologia medica ( 2020 ) 125 : 894901 and daily activities to allow for minimization of fatigue induced errors or breaches in techniques , for example . whenever possible , teams of physicians , nurses , and technologists should work together , or as staffing allows , in staggered shifts as teams , in order to minimize potential transmission between teams , or from one patient to many staff all at once . 
careful attention to avoid group mealtimes or coffee times is made using social distancing guidelines , since mask removal is often required for such activities , which creates vulnerabilities for transmission . 
staff who enter new spaces are encountered with screening queries upon entry , to ensure the critical in - person requirement for their entry . xray the hospital is dedicated to bedridden patients ; therefore , only portable x - ray machines are present . 
technicians are usually working in their office in the green zone , and they may be called by a phone call directly by the red zone anaesthesiologists or critical care staff . 
radiology technologists ( usually 2 ) may access the red zones through the changing room , where they can donn ppe , via a ppe donning sop . a station to process images and put them online in the pacs is present in the red zone . 
in case gowns are not available , waterproof aprons should be used . the who recommends the use of particulate respirators ( n95 or ffp2 or equivalent ) for contact and airborne precautions [ 4 ]  . 
 close communication with epidemiology is encouraged . workshift shifts are employed to provide around the clock coverage for radiologists , interventional radiologists , and technologists , with as many services as possible performed remotely , via teleradiology technology . 
efforts to limit around the clock work should be made to promote eating , sleeping , in each module , a dedicated us machine is present ( fig.3 ) , each fully equipped with 3 probes . 
a convex probe is available for thorax or abdomen fast us examinations usually performed by non - radiological specialists , or by the interventional radiology team for assessment for bedside procedures if necessary . 
recently , lung ultrasound has rapidly become a tool for monitoring of patients stricken by the novel covid - 19 , helping in clinical decision making and reducing the use of both chest x - rays and computed tomography ( ct ) [ 5 ]  . 
at any time , multidisciplinary decision making and team assessments may occur , preferably remotely , with anaesthesiologist , critical care staff , and diagnostic and / or interventional radiologists to discuss clinical indications or findings . 
decision making is always a team effort . once the decision is made that a ct scan is clinically indicated , after donning ppe , a radiologist and technologist may enter the red zone . 
air exchange rates ( and negative flow ideally ) should be closely analyzed prior to implementation of such facilities , to ensure that adequate passive air exchange is allowed in between patients , especially important in the event that covid - 19 status is uncertain , or for standard practices outside of the red zone , or in outpatient or acute care facilities . 
in this specialized hospital built for isolation patients , this device may not be necessary , but in future projects and managing non - intubated patients , this may permit a ct area to be cleaner when not isolated . 1 3 la radiologia medica ( 2020 ) 125 : 894901 fig . 
 such proximity minimized patient transfers and staff exposure risk . an important concept must be kept in mind : all the devices in the red zone should never leave it nor be brought in the green zone . 
 however , such as effort should be carefully analyzed with cost - effectiveness and cost - utility metrics that have longterm comparisons and outcomes analyses , based upon the economic realities of the pandemic . 
the cost metrics should factor in the downstream cost of lives saved , quality adjusted life years saved , pain averted , and intact family units toward the strength of the fabric of society at large . 
 each transmission averted by such a dedicated covid19 - specific facility has the potential to avoid a long - term admission , ventilator use , and resources required for that admission , and each of the contacts for that covid - 19 transmission , with an r 2 . 
this could allow the virus to spread rapidly , potentially infecting health care workers and patients , and taking health care workers out of the care teathis might occur when that team is already stressed to the max , and short staffed , with demand outpacing supply across multiple fronts of staff , equipment and testing . 
when confronting a pandemic faceless enemy , focal investments toward a dedicated facility have immense economic benefits that make it overwhelmingly cost effective , especially in the early phases of a pandemic outbreak curve whose end remains blurry and ill - defined . 
such investments may be made by proactive and forward - thinking stakeholders and leaders in radiology and policy - making . conclusion a dedicated facility for the management and triage of patients with covid - 19 clusters the expertise and tools requisite for optimal care . 
the construction of this covid19 hospital also allowed relatively easy transfers to and from other icus of the milano area , with strict sops . an environment completely dedicated to isolated covid - 19 patients permit a better management of these patients and resources and promotes containment within the healthcare facility that must care for these covid - 19 patients during a pandemic outbreak . 
such prophylactic biocontainment is cost - effective and provides value for the investment in the long term , even if it is a resourceintensive affair in the short terrepeated practice sessions , training , and standardized and epidemiologically rational sops and preparation are paramount . 
all of our collective actions may substantially contribute to global health security , since each and every action by a society , government , healthcare ministry , hospital leadership , or each physician and healthcare worker may have profound and downsteam implications and impact for the neighbors and contacts of everyone , for the near future . 
 united we rise , divided we fall . acknowledgements the opinions are those of the authors in their personal capacity and do not necessarily represent the opinions of the national institutes of health nor the us government . 
devices discussed may not be cleared for any indication by the ce mark or the us food and drug administration . funding this study was not supported by any funding . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . 
the main histotypes are pleomorphic adenoma ( 70% ) and warthin tumour ( 15% ) ; epithelial malignancies ( 510% ) and lymphoma ( 23% ) are rare [ 2 ]  . 
although the diagnostic accuracy of the histological examination of salivary gland neoplasms is high [ 3 ] , * stefano colagrande stefano.colagrande@unifi.it extended author information available on the last page of the article there is an overlap between benign and malignant tumours [ 4 ]  . 
magnetic resonance imaging ( mr ) with contrast agent allows a correct locoregional staging of salivary neoplasms [ 5 ] and provides useful information regarding their characterization [ 6 ]  . 
in the last years , there has been growing interest in diffusion - weighted imaging ( dwi ) and dynamic contrast - enhanced perfusion - weighted imaging ( dce - pwi ) mr sequences in oncological imaging [ 913 ]  . 
an overlap of apparent diffusion vol . : ( 0123456789 ) 1 3 852 la radiologia medica ( 2020 ) 125 : 851863 coefficient ( adc ) values between benign and malignant neoplasms was observed [ 22 ]  . 
most of the published studies showed that dce - pwi parameters , such as time resolutions less than 10s , wash - in < 120s , and wash - out ratio > 30% , are the best parameters to characterize salivary glands neoplasms [ 30 ]  . 
however , to our knowledge the association of these parameters has never been explored to better characterize these neoplasms . we aimed at retrospectively evaluating the usefulness of the association of dwi and dce - pwi sequences in the characterization of salivary glands neoplasms with the abovementioned parameters . methods andmaterials from february 2014 to january 2019 , all patients with histological diagnosis of salivary glands neoplasms who underwent head and neck mr in the radiology department of careggi hospital ( florence , italy ) were retrospectively included . 
the mr acquisition protocol was the same for all the examinations , as follows : from 0.9 to 3 - mm slice thickness , field of view ( fov ) 230 200 / 240mm , matrix from 230 256 to 261 484 . 
sagittal t1 - w sampling perfection with applicationoptimized contrasts using different flip angle evolution ( space ) , repetition time ( tr ) 500ms , echo time ( te ) 7.2ms , acceleration factor 2 , at axial , coronal , and sagittal multiplanar reconstructions ( mpr ) ; 2 . 
fat - saturated eco - planar ( epi ) dwi ( see below )  . after gadolinium chelates contrast agent intravenous administration ( gadobutrol , bayer , germany ) 1ml / 10kg 1 3 la radiologia medica ( 2020 ) 125 : 851863 followed by 20ml saline flush at a rate of 3ml / s , we acquired 5 . 
axial t1 - w turbo spin echo , tr 440 ms , te 17 ms , acceleration factor 3 , and axial t1 - w volumetric interpolated breath - hold examination ( vibe ) , and 6 . 
dixon dce - pwi , tr 10ms , te 2.4ms at axial , coronal , and sagittal mpr ( see below )  . dwi protocol andpostprocessing dwi was obtained by fat - saturated epi technique , tr 4100ms , te 55ms , and two b values ( b50 - 800s / mm2 ) , matrix 102 128 , and acceleration factor 3 . 
adc values were divided into three groups : high values 1.4 103 , intermediate values 0.91.4 10 3 , and low values < 0.9 103mm2 / s [ 1 ]  . 
before lesion sampling , an roi was placed on the internal carotid artery to obtain the arterial input function curve , defined as the contrast concentration in vessels feeding to tissue at each point in time during the contrast passage . 
 [ 30 ] : type a curve : slow and progressive wash - in , type b curve : rapid wash - in and wash - out , type c curve : rapid wash - in and slow wash - out , type d curve : absence of enhancement ( flat curve )  . wash - in was progressive ( or rapid ) if the maximum concentration of the contrast agent was reached after ( or before ) 120s , respectively . 
wash - out degree was evaluated by washout ratio at 300s with the following formula : dcepwi protocol andpostprocessing [ ( simax si5 min ) ( simax sipre ) ] 100 ( % ) dce - pwi was obtained through two vibe t1 - w sequences , 3.5 - mm slice thickness , 0.7 interslice gap , fov 250 226 mm , matrix 139 192 , flip angles 5 and 15 , and acceleration factor 3 for baseline t1 - mapping acquisitions . 
 [ 1 ] , the association of the type a curve and adc values 1.4 103mm2 / s was tested as parameter of benignity , whereas the association of the type c curve and adc values 0.91.4mm2 / s was considered as parameter of malignancy . 
a type d curve was indicative of a benign neoplasm , whereas a type b curve was not used as a parameter reference . observers andstatistical analysis all examinations were separately evaluated by two independent radiologists with 12 and 7years of experience in head and neck imaging , respectively . 
cystic components of the tumour ( dotted arrow ) had adc values 1.4 103 mm2 / s b time / intensity curve characterized by a rapid wash - in and rapid wash - out ( type b curve )  . 
the diagnostic accuracy of the association of adc values < 0.9 103mm2 / s and a type b curve was very high for the diagnosis of warthin tumour 1 3 la radiologia medica ( 2020 ) 125 : 851863 fig . 
a the lesion showed heterogeneous low t2 signal intensity , b vivid enhancement on standard post - contrast imaging , and c average apparent diffusion coefficient ( adc ) values around 1.1 103 mm2 / s . 
d dynamic contrast - enhanced perfusion imaging ( dce - pwi ) showed adenoid - cystic carcinoma in the left submandibular gland with high ktrans values ( roi 1 in red )  . 
e dce - pwi time / intensity curve of the lesion characterized by a rapid wash - in and slow wash - out ( type c curve ) 1 3 858 discussion in our series , the efficacy of tic in the characterization was assessed by high - quality temporal resolution parameters ( time resolution 5s , wash - in < 120s , and wash - out > 30% )  . 
all lymphomas ( one diffuse b - cell , two mantel cell , and one malt non - hodgkin lymphomas ) showed low adc values < 0.9 103mm2 / s and a type c curve . 
conversely , a significant overlap for adc values < 0.9 103mm2 / s was observed between warthin tumour and lymphoma , as reported in the literature [ 14 , 17 , 2527 , 31 ]  . 
approximately , 60% of the benign neoplasms showed adc values < 1.4 103mm2 / s , including all sixteen warthin tumours , six pleomorphic adenomas with rich cellular component , and two basal cell adenomas characterized by a high cellular density and nucleo - cytoplasmic ratio . 
axial magnetic resonance images highline an oval , lobulated and well - defined lesion in the right parotid gland with pathognomonic signal features : homogeneously hypointense on t1 - weighed ( w ) sequence ( a ) , hyperintense on t2 - w ( b ) , low signal on diffusion - weighted imaging with b - 800 s / mm2 ( c ) , and very high values ( > 2 103 mm2 / s ) on apparent diffusion coefficient map ( d )  . 
perfusion - weighted imaging shows low ktrans values ( e ) , and type a time / intensity curve ( f ) 1 3 la radiologia medica ( 2020 ) 125 : 851863 neoplasms with values 1.4 103mm2 / s , as reported in the literature [ 1 , 14 , 15 ]  . 
 [ 1 ] , reflecting mixed areas of high tumour cells density and necrosis . in the present study , a type a curve was observed only in benign neoplasms and in 80% of pleomorphic adenomas . 
many studies [ 2024 , 30 ] stated that epithelial malignancies show a rapid wash - in and slow wash - out ( type c curve ) , pleomorphic adenoma has a slow and progressive wash - in ( type a curve ) , and warthin tumour presents a rapid wash - in and wash - out fig . 
axial magnetic resonance images show a rounded lesion in the left parotid gland with heterogeneous signal on t1 - weighed ( w ) sequence for the presence of hyperintense intralesional foci indicative of haemorrhage and / or cholesterol ( a ) , cystic areas with hyperintense signal on t2 - w ( b ) , high signal on diffusion - weighted imaging with b - 800s / mm2 ( c ) , and low values ( 0709 103 mm2 / s ) on apparent diffusion coefficient map ( d )  . 
perfusion - weighted imaging shows intermediate ktrans values ( e ) and type b time / intensity curve ( f ) 1 3 860 la radiologia medica ( 2020 ) 125 : 851863 ( type b curve )  . 
in the literature , different wash - in temporal references were reported ( 120s [ 2931 ] , 150s [ 23 ] , 165s [ 18 ] , and 210s [ 20 ] ) depending on different temporal resolutions . 
although dce - pwi parameters with the highest diagnostic accuracy [ 30 ] were used in the current study , accuracy of the association of dwi with dce - pwi for the detection of salivary malignant neoplasms was 82.1%. 
this value was similar to that found in previous papers , in which accuracy in distinguishing between benign and malignant neoplasms varied from 67 to 90% [ 1 , 1820 , 2731 , 33 , 34 ]  . 
the great variability in diagnostic accuracy could also be explained by the different number of lymphomas analysed in several studies , varying from 1 to 4 [ 1 , 14 , 15 , 17 , 26 , 27 , 31 ]  . 
indeed , lymphoma almost always showed adc values < 0.9 10 3mm2 / s , and therefore , they were not included in the adc range values generally considered in the literature as an index of malignancy [ 1 , 17 , 26 , 27 , 30 , 31 ]  . generally , tumours with well - defined borders tend to be benign , whereas irregular borders are suspicious for fig . 
axial magnetic resonance images show an ill - defined lesion in the left parotid gland with low signal on t1 - weighed ( w ) sequence ( a ) , very low signal on t2 - w ( b ) , intermediate signal on diffusionweighted imaging with b - 800 s / mm2 ( c ) , and intermediate values ( 1 103 mm2 / s ) on apparent diffusion coefficient map ( d )  . 
in our opinion , radiologists should not overlook conventional t1 - w and t2 - w sequences since these sequences are crucial not to incur errors in the interpretation of dwi and dec - pwi sequences for the identification of salivary glands neoplasms ( table5 )  . our study has some limitations . 
first , we used small rois to measure adc values , since this method has been reported to have lower interobserver reproducibility than sampling the entire volume of the lesion [ 9 , 10 ]  . 
however , small rois are easier to use in clinical practice and allowed us to get adc values comparable with most previous papers [ 1 , 17 , 26 , 27 , 30 , 31 ]  . 
nevertheless , since low - grade neoplasms reached smax before 120s in both the current study and ogawas paper [ 40 ] , it would have no impact on our results . 
 quantitative studies that assess the dynamic of passage of the contrast agent from the vascular to the extra - cellular systems could play an important role in the distinction between benign and malignant neoplasms . 
texture analysis examines the grey - scale distribution among voxels and could be useful to characterize salivary glands tumours in case of any doubts persisting after dwi and dce - pwi [ 41 , 42 ]  . 
future research should deal with the combination of functional and morphological data , as it could have a further increase in mri accuracy for the characterization of salivary glands neoplasms . conclusions in our study , the association of high adc values 1.4 10 3mm2 / s and a type a curve was found only in benign neoplasms , whereof most were pleomorphic adenomas . 
all lymphomas showed low adc values < 0.9 103mm2 / s and a type c curve . acknowledgements the authors have no financial affiliation ( employment , direct payment , stock holdings , retainers , consultantships , patent licensing arrangements , or honoraria ) , or involvement with any commercial organization with direct financial interest in the subject or materials discussed in this manuscript , nor have any such arrangements existed in the past 3years . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the psa value , tumor adcmin value , tumor diameter , and pi - rads score were compared between the clinically significant and nonsignificant pca groups using students t - test . 
the correlations between the serum psa level , gs , pi - rads v2 score , tumor adcmin value , and tumor diameter were evaluated separately ( pearsons correlation analysis was used for peripheral gland tumors , and spearmans correlation analysis for central gland tumors )  . 
the cut - off values for the peripheral and central gland tumors are as follows : lesion diameter , 13.5mm and 19mm ; tumor adcmin , 0.709 103mm2 / s and 0.874 103mm2 / s ; and psa level , 8.47ng / ml and 11.10ng / ml , respectively . conclusion the current pi - rads v2 scoring system can be inadequate in distinguishing clinically significant and insignificant groups in central gland tumors . 
in low - risk patients with a gleason score ( gs ) of 6 , prostate - specific antigen ( psa ) of < 10ng / ml , and clinical stage of t2a , the prognosis is better , whereas for the high - risk group , the disease has an aggressive progression and causes high rates of metastatic disease and mortality vol . : ( 0123456789 ) 1 3 828 la radiologia medica ( 2020 ) 125 : 827837 [ 2 ]  . 
the aim of pca treatment is to prevent over - treatment by avoiding the unnecessary side effects of radiotherapy , surgery , or hormone treatment in patients with slow progressive disease , as well as preventing under - treatment of those that require an aggressive approach [ 28 ]  . digital rectal examination and psa , a serum tumor marker , are used in the diagnosis and screening of pca [ 711 ]  . 
transrectal ultrasonography ( trus ) - guided 12 - core biopsy is accepted as a standard , but its effectiveness may be limited [ 4 , 5 , 9 , 12 , 13 ]  . 
in particular , anterior tumors may not be detected , or some of the clinically significant cancers can be identified as presenting low risk [ 4 , 5 , 8 , 9 , 1218 ]  . 
therefore , for the evaluation of patients suspected of having pca , multiparametric magnetic resonance imaging ( mpmri ) is recommended , and in cases where necessary , an mri - us fusion biopsy can be undertaken to better determine the characteristics of the tumor [ 46 , 8 , 9 , 12 , 13 , 1921 ]  . 
 a prostate imaging reporting and data system ( pi - rads ) was published in 2012 and revised in 2015 ( pi - rads v2 ) to ensure standardization in obtaining , interpreting and reporting mpmri images [ 22 ]  . the most important prognostic factor in pca is gs and its clinical stage [ 3 , 7 , 23 , 24 ]  . 
the aim of this study was to determine the relationship between the serum psa level , gs , pi - rads v2 score , minimum apparent diffusion coefficient ( adc ) of the tumor , and the largest tumor diameter in patients with pca that underwent rp and to comparatively evaluate these parameters in clinically significant and insignificant groups classified according to gs . materials andmethods the study was performed retrospectively with the reevaluation of prostate mpmri scans performed from january 2015 to february 2019 and obtained from the hospital image archive . 
ten cases for whom there were technical insufficiencies in imaging ( motion artifact , poor quality examination , inappropriate b - value ) or the pathology reports were not available , as well as 13 patients with a pi - rads v2 score of lower than 4 ( pi - rads 1 - 3 ) were excluded from the study . 
 the routine prostate mpmri protocol included triplanar t2 - weighted imaging without fat suppression , diffusionweighted imaging ( dwi ) in the axial plane , fat - suppressed t2 - weighted and pre / post - contrast t1 - weighted imaging in the axial plane , and dynamic contrast - enhanced ( dce ) imaging . 
measurements were performed twice , and the lower mean adc was 1 3 la radiologia medica ( 2020 ) 125 : 827837 table 1 imaging parameters of mri parameters axial t2w sagittal t2w coronal t2w axial t2w fat sat axial t1w sequence tr ( ms ) te ( ms ) slice thickness ( mm ) fov ( cm ) matrix b values ( s / mm2 ) 8300 288 288 10 , 000 288 288 9100 320 320 8500 288 288 352 224 4000 90.4 80 80 0 , 500 , 2000 lava 160 128 t2w t2 - weighted , dwe diffusion - weighted imaging , dce dynamic contrast - enhanced , epi echo planar imaging , fov field of view , fse fast spin echo , nex number of excitations , te echo time , tr repetition time used for evaluation . 
the mri findings were correlated with the pathology results . study design the final gs of the rp specimen of the lesion with the same localization in mri and pathological reports was noted . 
the relationships between the pi - rads score , adcmin value of the tumor , largest diameter of the tumor , serum psa level , and gs were investigated . statistical analysis spss software v.22.0 ( chicago , il ) was used for statistical analysis . 
 students t - test was used to investigate whether the psa value , tumor adcmin value , tumor diameter , and pi - rads score differed between the groups with clinically significant and nonsignificant pca . 
a receiver operating characteristic ( roc ) analysis was performed to evaluate the efficacy of the tumor adcmin , the largest tumor diameter and psa values in differentiating clinically significant and insignificant tumors . 
for the cut - off value of each criterion , the sensitivity and specificity values were calculated at the 95% confidence interval . results a total of 84 lesions were detected in the mpmri of 76 patients ( two lesions in eight patients )  . 
clinically significant pca ( gs 7 ) was present in nine of the central gland lesions ( 60% ) , and clinically insignificant pca ( gs 6 ) in six central gland lesions ( 40% )  . 
at a cut - off value of 0.874 103mm2 / s , we were able to distinguish between clinically significant and insignificant tumors with a sensitivity of 66.7% and specificity of 100% . 
the auc of psa was measured as 0.833 , and at the cut - off value of 11.10ng / ml , this parameter had 77.8% sensitivity and 100% specificity in the differentiation of the two tumor groups . according to the pathology results , 54 of the peripheral gland tumors ( 78.3% ) were clinically significant ( gs 7 ) and 15 ( 21.7% ) were clinically insignificant ( gs 6 )  . 
the psa values significantly differed between the two groups ( p = 0.003 ) , with the patients in the clinically 1 3 832 la radiologia medica ( 2020 ) 125 : 827837 fig . 
the tumor adcmin had an auc of 0.841 , and at the cut - off value of 0.709 10 3mm2 / s , this parameter had a sensitivity of 93.3% and a specificity of 53.7% in the differentiation of clinically significant and insignificant tumors . 
4 receiver operating characteristic ( roc ) analysis for the efficacy of the a tumor adcmin ( auc = 0.841 ) , b tumor diameter ( auc = 0.898 ) , c psa values ( auc = 0.833 ) in differentiating clinically significant and insignificant tumors in peripheral gland tumors discussion psa and gs are traditionally used for risk classification in the diagnosis , treatment and follow - up of pca [ 28 ]  . 
in recent decades , with the increasing use of mpmri , it has been reported that some findings and parameters obtained from mpmri can also contribute to risk classification [ 2933 ]  . 
 in the current study , we evaluated the correlations between the traditional risk factors of psa and gs and parameters obtained from mpmri findings , namely the pi - rads score , lesion size , and calculated adc values . 
we found correlations between psa , gs , pi - rads score , lesion size , and adc values at different levels ( weak , moderate , and high ) in both central and peripheral gland tumors . 
the clinically significant and nonsignificant groups formed according to the final gs were found to significantly differ in terms of the psa value , tumor adc value , tumor diameter , and pi - rads score in all parameters for the peripheral gland 1 3 834 la radiologia medica ( 2020 ) 125 : 827837 tumors , and tumor diameter and tumor adc for the central gland tumors . 
the tumor adc value , lesion diameter , and efficacy of psa in differentiating clinically significant and nonsignificant tumors also differed between the central and peripheral gland tumors . according to the recommendations of pi - rads v2 , determination of the lesion score is based on a subjective evaluation . 
in the literature , many studies used adc values for quantitative assessment of peripheral zone lesions , and an inverse correlation was found between gs and adc values [ 3 , 7 , 23 , 24 , 3340 ]  . 
in some of these studies , the gs data were obtained from a trus - guided biopsy , but it is known that these results are not always consistent with the final gs . 
the final gs is very important in the management of patients , especially in making an active surveillance decision ; therefore , in the current study , the gs obtained from rp was used as reference . 
except for a few studies [ 7 , 24 , 39 ] , a differentiation of clinically significant ( gs 7 ) and insignificant ( gs 6 ) pca was not made . 
in contrast , in the current study , clinical significance was considered when investigating the correlation between gs and various parameters , and the patients were evaluated in two pca groups ( significantinsignificant ) according to gs . 
there was a moderate inverse correlation between the tumor adcmin value and gs in both central zone and peripheral zone tumors , which is consistent with the studies in the literature . 
according to the results of this study , revealing that a low tumor adc value presents a higher possibility of clinically significant tumor , it can be considered to include the adc value , a quantitative mri parameter , in the pirads scoring system or use it as a predictive parameter . 
 although t2 - weighted images are the basic sequence used in the evaluation of central gland tumors , the presence of an inverse correlation between the adc values and gs suggests that diffusion examination has a diagnostic contribution for central gland tumors . 
the tumor adcmin values and the cutoff values determined for adcmin in the current study can be used to differentiate between clinically significant and insignificant disease groups and predict disease progression . the literature contains studies evaluating the diagnostic accuracy of mpmri and pi - rads in the diagnosis of pca [ 20 , 27 , 29 , 34 , 41 ]  . 
no difference was found in the pi - rads ( 4 or 5 ) score between the clinically significant and insignificant groups for the central gland tumors , but these scores significantly differed for the peripheral zone tumors . 
another reason for this result may be that the measurement of lesion size in the central gland is more subjective compared to the measurement undertaken in the peripheral gland due to the faint appearance of the lesion borders in the former . 
based on the results of the current study , it is considered that the pi - rads v2 score can be used to predict the aggressiveness of the disease in peripheral gland tumors . 
for the central gland tumors , however , the validity of the scoring system should be further investigated . in the current study , the psa values were correlated with tumor diameter and gs in both central and peripheral gland tumors . 
 although 10ng / ml is used as a common threshold value , patients with psa values between 2 and 10 are included in the gray zone [ 28 , 42 ]  . 
considering that psa is not an ideal marker and it has low specificity , the prostate health index ( phi ) has recently been developed based on propsa , the isoform of psa , to prevent unnecessary biopsies [ 43 ]  . 
in pca , the determination of a serum psa value higher than normal is not due to the increased production of psa but rather as a result of the deterioration of the prostate structure , leading to elevated psa in circulation . 
our study indicated that more psa was released into the circulation in peripheral gland tumors , which may be due to the different histopathological features of the central and peripheral glands . 
the central 1 3 la radiologia medica ( 2020 ) 125 : 827837 gland being richer than stroma may serve a barrier function in the passage of psa into circulation . in this study , for the differentiation of clinically significant and insignificant lesions , the optimal cut - off value of tumor diameter was determined as 19mm in central gland tumors and 13.5mm in peripheral gland tumors . 
another limitation may be considered as the absence of whole - mount sectioning of specimens with special equipment for the pathological examination ; however , localization was determined according to pi - rads v2 when evaluating the results ; thus , a radio - pathological localization agreement was achieved . 
despite these limitations , the study provided significant data . conclusions in conclusion , in the current treatment approach to pca , it is very important to distinguish clinically significant and insignificant tumors . 
the currently used pi - rads v2 scoring system satisfies this need to a large extent , but it may be inadequate in distinguishing cases with clinically significant and insignificant pca in central gland tumors . 
it should also be noted that when deciding on active surveillance in patients with peripheral gland tumors , it may be necessary to use a lower psa cut - off value than reported in the literature . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical statement all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments os comparable ethical standards . informed consent for this type of study , formal consent is not required . 
also , diseases that mimic the symptoms , signs or imaging characteristics of gca may only be revealed on pathology . bardi and diamantopoulos [ 1 ] conclude that imaging modalities are more sensitive than temporal artery biopsy ( tab ) in the diagnosis of giant cell arteritis ( gca )  . however , the literature on the relative sensitivity of tab versus imaging is conflicting . 
comprehensive reviews suggest that properly performed tab have a sensitivity between 77% [ 2 ] and 87% , [ 3 ] but there may be false positives when the vasculitis is segmental and the specimen does not sample an affected area . 
many of the tab in the tabul study [ 5 ] were substandard ; 7% of the attempted tab did not retrieve a temporal artery , and 43% of the tab specimens were less than 1cm in length . patients with the clinical symptoms and signs of gca can have a myriad of mimicking diseases including syphilis , sarcoidosis , metastases , amyloidosis , zoster , and granulomatosis with polyangiitis , which may not be diagnosed in an expedient fashion without pathology . 
the aim of this review is to discuss , in the light of our single - center experience , the technique , current applications , results , and future perspectives of this novel technology . keywords tremor parkinsons disease vim thalamotomy mrgfus functional neurosurgery interventional neuroradiology introduction tremor is the dominant symptom of essential tremor ( et ) and one of the most common motor symptoms of parkinsons disease ( pd )  . 
it has a prevalence of about 6.5% in the population over 65years of age , causing significant disability and limitation in patients daily activities , and resulting in social distress and isolation [ 1 , 2 ]  . 
 tremor can be treated pharmacologically when symptoms * federico bruno federico.bruno.1988@gmail.com 1 department ofbiotechnological andapplied clinical sciences , university oflaquila , via vetoio 1 , 67100laquila , italy 2 radiology department , san salvatore hospital , laquila , italy 3 neurology unit , san salvatore hospital , laquila , italy 4 department ofneurosurgery , san salvatore hospital , laquila , italy 5 neurology unit , department ofmedicine , health andenvironment sciences , laquila , italy become interfering with the patients daily activities , but many of the drugs used have variable effects and carry an increased risk of side effects . 
in fact , while et and pd tremor have different etiology and pathophysiology , several functional neurosurgical treatment showed efficacy in the treatment of the symptoms in both et an pd tremor ; currently available surgical options for the treatment of tremor include deep brain stimulation ( dbs ) , radiofrequency thalamotomy ( rf ) , and radiation therapy ( gamma - knife ) [ 3 ]  . 
these treatments are directed to specific anatomical areas involved in the neurofunctional circuits of movement control , mainly at the level of the thalamus , where the ways of movement control are most represented . 
in particular , the thalamus regulates the motor component through the pallidus - thalamus - cortical ( extrapyramidal system ) and the cerebellum - thalamus - cortical circuits ( regulation of muscle tone ) ; the ventral intermediate nucleus ( vim ) of the thalamus is the target of choice for patients with essential tremor and for some patients with tremorigenic parkinsons disease . 
recently , transcranial thalamotomy using magnetic resonance guided high - intensity focused ultrasounds ( tc - mrgfus ) has emerged as a novel vol . : ( 0123456789 ) 1 3 878 la radiologia medica ( 2020 ) 125 : 877886 minimally invasive ablation method and as an innovative and promising treatment for ablation of deep brain structures . 
ablation by focused ultrasounds , a method already used for the treatment of several pathologies , including uterine fibroids and bone tumors [ 513 ] , does not require open surgical access and determines very precise lesions that can be monitored in real - time using thermometric mr imaging [ 14 , 15 ]  . 
the very recent clinical approval of mrgfus thalamotomy for the treatment of unilateral tremor has led to a rapid expansion of preclinical and clinical research for numerous therapeutic indications in the neurological and neurosurgical fields [ 16 ]  . the system the focused ultrasound system ( neuroablate 4000 , insightec ltd , carmel - tirat , israel ) is integrated into an mr scanner for clinical applications ( 3t mr750w , ge healthcare at our institution )  . 
main contraindications to treatment are represented by the presence of other brain pathologies ( brain tumors , intracranial aneurysms ) , brain or cranial implants ( shunts , electrodes , patches ) that cannot be avoided during treatment , cerebral hemorrhages or seizures in the last year , and non - correctable hemorrhagic risk factors [ 18 ]  . patient preparation the procedure is performed in a hospitalization setting . 
the day of the procedure , the stereotaxic frame is fixed to the skull by screws positioned anteriorly at supraorbital level and posteriorly at the level of the occipital protuberance , after subcutaneous and periosteal injection of a mixture of local anesthetics ( 5ml mepivacaine 2% , 5ml ropivacaine 2% ) [ 19 ]  . 
after stereotaxic frame fixation ( b ) , the patient is positioned with the head into the helmet ( c ) 1 3 la radiologia medica ( 2020 ) 125 : 877886 a fundamental parameter during treatment , given that a low sdr causes less ultrasound transmission and focalization through the skull . 
the fusion of the images allows identifying intracranial calcifications ( choroid plexuses , basal nuclei ) and the areas containing air ( frontal sinuses , folds between the membrane and the skin ) that can block the transmission of ultrasounds and are marked as " no - pass zones " for ultrasound beams . 
 fiducial markers on the three spatial planes are placed to identify any movement of the head during treatment [ 21 ]  . subsequently , the anterior and posterior commissure ( ac , pc ) and the plane passing through them are identified . 
the first ( alignment ) includes short sonications with very low energy ( 15003000j ) , so that the temperature increase is visible in the thermometric maps without creating biological effects ; in this way it is possible to confirm that the sonication point fig . 
in the lower panel , skull score parameters ( sdr , skull area , active elements ) are displayed 1 3 880 la radiologia medica ( 2020 ) 125 : 877886 coincides with the target coordinates , and eventually correct the focus . 
 the second step ( verification ) includes sonications with increasing energy and power parameters to reach higher temperatures ( 4652c ) to obtain a neuromodulation effect , confirming the efficacy of the treatment in the target and the possible presence of adverse effects . 
the clinical response is controlled both during sonication to assess the reduction / disappearance of the tremor , and at the end of each sonication to assess the appearance of adverse effects . 
in the last step ( treatment ) the actual ablationthe energy , the sonication time , and the number of sonications are increased and modulated to reach maximum temperatures of 60c at the level of target . 
 generally , the lesion ( necrosis ) is effective with at least two sonications that have reached temperatures > 56c [ 23 ]  . at the end of the treatment , after draining the water from the helmet and removing the stereotaxic frame , the patient can stand up and undergo a final complete neurological examination before being transferred back to the ward , under observation until the following day . 
the average duration of the treatment , from the positioning to the end of the treatment , is about 3h . target the ventrolateral area of the thalamus has been the main target of stereotactic surgery for the treatment of tremor since the early 1950s . 
the target of choice was shown to be the area of the relay nuclei of the vestibular and proprioceptive afferents fibers , i.e. , the ventral intermediate nucleus ( vim ) according to hassler [ 31 ] , or the ventral and posterior part of the ventral posterior nucleus ( vlp ) , receiving cerebellar afferents , according to hirai and jones [ 28 ]  . 
3 screenshot of the console showing sonication monitoring thanks to thermometric maps ( ac ) and graphs showing energy delivery ( d , e ) and average and maximum temperature reached ( f , g ) 1 3 la radiologia medica ( 2020 ) 125 : 877886 sequences . 
the small vim is still considered " invisible " with the commonly used mr imaging techniques and can be defined more from a functional point of view than from a purely anatomical one . 
for this reason , indirect targeting based on data from stereotactic atlases and data previously obtained from the authors with substantial experience in the field of thalamotomy and deep brain stimulation ( dbs ) still represents the " gold standard " method for target localization [ 32 , 33 ]  . 
i the authors experience , in the case of an important mismatch between the distance from the midline and the wall of the fourth ventricle , we usually set the target by averaging the coordinates of the two landmarks . 
in most of the treatments we performed movement of the target to find the optimal sonication point where to obtain the maximum clinical response without side effects ; the number of shifts with respect to the initial coordinates was very variable from patient to patient , from a minimum of no displacement up to a maximum of 9 movements during a single treatment . 
have used wair ( white matter attenuated inversion recovery ) sequences and found a similar display in terms of shape , spatial orientation and signal contrast of the vim with respect to what is described in some stereotaxic atlases , and have successfully applied the mr findings for targeting direct vim in dbs in patients with essential tremor and parkinsons [ 33 ]  . 
in mrgfus thalamotomy , this limit is overcome mainly since there are no intraparenchymal electrodes , and focused ultrasound beams do not cause tissue damage trough the path , but only at the level of the focal point [ 36 ]  . 
however , precise localization of the target is also fundamental with the use of focused ultrasounds , since repeated sonications outside the target area can still lead to edema and cavitation , with consequent problems in the assessment of the response , in reaching therapeutic temperatures , or in an enlargement of the area of necrosis . 
technological advances in the future will undoubtedly be able to obtain a better visualization of the target structures , with the implementation of mr sequences such as tractography , to obtain a reduction in the duration of the procedure and the incidence of adverse effects [ 34 , 37 ]  . results the first study to report its experience in the use of mrgfus for thalamotomy described an immediate and persistent improvement in tremor in 4 treated patients , with a 90 - day follow - up [ 24 ]  . 
adverse effects reported were paresthesia of the tongue and lips ( in 9 patients , persistent at follow - up in 2 ) , balance disorders ( 5 patients ) , and gait ( 4 patients , with complete resolution at 1 - month follow - up )  . 
the safety and efficacy of the vim thalamotomy with ultrasounds have been validated by three clinical studies that have shown significant improvement in the tremor of the contralateral hand and reduction in the related disability [ 15 , 24 , 25 ]  . 
presented long - term results at 5years in a cohort of 44 et patients [ 27 ] ; their results showed a reduction in crst scores in the treated hand from the baseline ( median 19 ; range 732 , 44 patients ) to a median of 17 at 6months ( 31 patients ; p < 0.0001 ) , 15 at 1year ( 24 patients ; p < 0.0001 ) , 18 at 2years ( 15 patients ; p < 0.0001 ) , 19 at 3years , ( 10 patients ; p < 0.0001 ) , 21 at 4years ( 6 patients ; p < 0.01 ) , and 23 at 5years ( 2 patients )  . 
clinical evaluation in pd patients included also the updrs ( unified parkinsons disease rating scale ) score , with particular reference for its part iii ( motor examination )  . 
the clinical scores were recorded before treatment , immediately after treatment and with follow - up at 1 , 6 , and 12months . treatment was effective ( substantial and immediate reduction in the tremor ) in 49 patients out of 50 ( 98% )  . 
in the patient where treatment was not effective , the procedure was suspended early due to the onset of unsustainable side effects ( nausea , headache ) and the impossibility to reach ablative temperature with increasing sonication parameters . 
at the clinical follow - up , they found a progressive improvement in the updrs score by 34.1 at 1 month , 1 month , and by 46.2% at 6 months ( p = 0.009 ) , and with a parallel improvement in the quality of life scores . 
thalamotomyrelated complications from our experience occurred in 8 patients ( 16% ) , reported in table2 . imaging followup adverse events the most frequent adverse events related to sonications reported in the literature are represented by vertigo , lipotimia , headache , nausea , and scalp burning [ 29 ]  . 
the first area is represented by a central hypointense spot ( not always appreciable ) surrounded by a hyperintense zone demarcated by peripheral table 2 thalamotomy - related complications post 1 month 3 months 6 months 1year perioral paresthesia perioral paresthesia ataxia dysartria , ataxia hemiparesis dystonia , hemiparesis resol perioral paresthesia perioral paresthesia perioral paresthesia resol dysartria , ataxia hemiparesis hemiparesis perioral paresthesia perioral paresthesia perioral paresthesia dysartria , ataxia ( improving ) hemiparesis ( improving ) perioral paresthesia resol perioral paresthesia dysartria , ataxia ( improving ) resol perioral paresthesia u under follow - up , resol resolution 1 3 884 la radiologia medica ( 2020 ) 125 : 877886 hypointense border ( zone 2 ) , and finally a blurred hyperintense area of more peripheral vasogenic edema ( zone 3 )  . 
susceptibility weighted sequences ( swi ) show the presence of hemoglobin derivatives at the level of the lesion core , which often persists even when other mr findings are reduced . 
 the same authors [ 21 ] report how , with a 3 - month followup , the perilesional edema tends to increase in the first week after treatment , and the size of zones 2 and 3 are progressively reduced within the first month . 
however , from the results of the previous studies there is no statistically significant correlation between the imaging characteristics and the number of sonications , the final energy delivered and the temperature reached , while there is a correlation between the extension of the vasogenic edema and its resolution with the presence of side effects such as paresthesias [ 39 ]  . 
 these data suggest the possibility of possibly repeating mrgfus treatment in patients with sub - optimal benefit after a first procedure , or in patients with symptom recurrences , as reported in a case described by weidman etal . currently , the use of focused ultrasound is limited to unilateral treatment . 
the enormous technical advantages of thalamotomy with mrgfus in terms of control of the effects , precision and predictability of the lesion , suggest that the use of this method in bilateral treatment , even in staged treatment sessions , merits further studies to improve the therapeutic outcome in patients with both limbs tremor or axial tremor [ 42 ]  . conclusions to date , tcmrgfus has been mainly applied in the treatment of movement disorders , it has enormous potential for application in all pathological conditions that can be treated with a stereotaxic functional neurosurgical approach . 
this application , which uses intermediate levels of energy combined with pulsed sonications and the use of circulating microbubbles injected intravenously , may allow an increase in the release of chemotherapy for the treatment of brain neoplasms [ 43 , 44 ]  . the scientific publications and clinical experiences of recent years with focused ultrasounds have enormously increased the awareness of the therapeutic potential of this method and will further accelerate the application of this innovative , versatile , and multidisciplinary technology . 
 being still an innovative and growing technique , tcmrgfus has the potential to become the primary method for new therapeutic approaches in an ever - increasing number of neurological and neuropsychiatric pathologies , drastically revolutionizing the future management of many patients . funding no financial support was received for this paper . compliance with ethical standards conflict of interest the authors have no potential conflicts of interest to disclose . human and animal rights all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
identifying information about participants is not available in the article . la radiologia medica ( 2020 ) 125 : 887893 radiotherapy postmastectomy immediate breast reconstruction andadjuvant radiotherapy : long term results ofamono institutional experience chiarareverberi1 lucamarinelli1 barbaracampanella1 giovannascalabrino1 lucanicosia2 dimitrianzellini1 vitalianadesanctis1 mauriziovaleriani1 mattiaf.osti1 received : 18 december 2019 / accepted : 2 march 2020 / published online : 12 march 2020 italian society of medical radiology 2020 abstract introduction the aim of this paper is to investigate the outcome of patients treated with mastectomy , immediate breast reconstruction ( ibr ) and post - mastectomy radiotherapy ( pmrt ) and the risk of late complications . material and method all patients had post - mastectomy , immediate reconstructive surgical procedure by using autologous abdominal implant ; tissue expander ( te ) / permanent prosthesis ( pp ) ; or even combined procedures . 
the kaplan - meyer analysis evaluates patients rate of late side effects , overall survival ( os ) , progression free survival ( pfs ) , localregional free survival ( lrfs ) and metastasis free survival ( mfs )  . 
the univariate analysis investigates the correlation between late toxicity and related factors . results between november 2003 and october 2016 , 91 breast cancer patients were treated with ibr and pmrt . 
moreover , ibr followed by adjuvant radiotherapy , has showed acceptable late toxicity profile and no influence on os . keywords immediate breast reconstruction ( ibr ) post - mastectomy radiotherapy ( pmrt ) late toxicity complications breast cancer introduction literature data shows that breast cancer patients overall survival ( os ) is generally increased over time due to the development of new strategies and new systemic treatment options available . 
relative to reconstruction timing * chiara reverberi chiarareverberi87@gmail.com 1 radiation oncology department , santandrea hospital , la sapienza ii university ofrome , via di grottarossa 1035 , rome , italy 2 radiation oncology department , irccs sacro cuore don calabria hospital , negrar , verona , italy after surgery it can be immediate ( one - step surgery ) during the same session of mastectomy , delayed ( 612months after mastectomy ) or hybrid ( delayed - immediate )  . 
referring to the tissue used for reconstruction it can be autologous flap tissue or implant - based ( tissue expander or permanent prosthesis )  . the autologous reconstruction has better breast shape outcome giving the contralateral natural breast ; symmetry is usually less affected by ageing , and weight loss / gain and it can be done in a single - step surgery . 
implant - based reconstruction has shorter operation duration , hospitalizations , and recovery time ; no scar to the donor site [ 1 ]  . mastectomy is the treatment option for patients with advance disease and immediate breast reconstruction ( ibr ) has been validated also in the setting of patients candidate to post - mastectomy radiotherapy ( pmrt )  . 
according to the early breast cancer trialists collaborative group vol . : ( 0123456789 ) 1 3 888 la radiologia medica ( 2020 ) 125 : 887893 ( ebctcg ) , pmrt to the chest and loco - regional nodes have clearly demonstrated to reduce loco - regional relapse rate and cancer specific mortality in patients with advance disease , nodal involvement or not extensive axillary surgery [ 2 ]  . 
it offers several advantages : patients maintain their body imaging and they will not suffer for breast amputation trauma , good aesthetic outcome , good satisfaction and quality of life , it also reduces the costs and risks of a second surgical procedure . 
the question is whether adjuvant radiotherapy increase the risk of acute and late toxicity , and the risk of second surgery for complication . the aim of this paper is to investigate late toxicity outcome of patients treated with mastectomy , ibr and pmrt . 
 the hypothesis is that due to progress in surgical technique and radiotherapy evolution , pmrt subsequent to an immediate reconstruction surgery , guarantee a good aesthetic outcome , patients satisfaction and quality of life , with a meaningless risk of late side effects , which overall are comparable to whom who did not receive adjuvant rt or to patients candidate at delayed surgery . material andmethod breast cancer patients treated with mastectomy , breast reconstruction and adjuvant radiotherapy were retrospectively analyzed . all locally advance breast cancer patients were discussed at the multidisciplinary meeting by the breast cancer specialists team which involves oncologist , radiation oncologist , oncoplastic - surgeon , plastic surgeon , pathologist and radiologist . 
risks and benefits of procedures and timing were considered , and each patient signed consensus forall patients had post - mastectomy , immediate reconstructive surgical procedure by using autologous abdominal implant like deep inferior epigastric perforator ( diep ) or transverse rectus abdominis muscolo - cutaneus ( tram ) flaps ; tissue expander ( te ) / permanent prosthesis ( pp ) ; or even combined procedures with latissimus dorsi ( ld ) limbo and expander / prosthesis . 
in case of delayedimmediate breast reconstruction , a te saline - filled , was placed under the skin and chest muscle or implanted ld , and it was removed after radiotherapy and replaced with permanent implant . adjuvant external beam radiotherapy treatment ( ebrt ) was delivered to the reconstructed chest wall , treatment target includes skin , subcutaneous tissue and pectoralis major muscle while chest wall muscles and rib plane were excluded . 
clinical target volume ( ctv ) was contoured on 1.5 mm slices tc - scan without contrast enhancement with the patients lying supine arm - overhead , the standard wing - board immobilization device was used for minimizing inter and intrafraction uncertainties . 
planned target volume ( ptv ) coverage vary between 95 and 107% of the prescription total dose of 50gy in 25 fractions ( 2gy / fraction ) by using 3d conformal tangential fields and high - energy photons ( 615 mv ) , high risk patients received rt boost ( 36gy / 12 fractions )  . 
factors predictive for high risk recurrence were younger age , positive margins no suitable for surgery , many positive nodes ( > 4 ) and / or poor response to neo - adjuvant cht . 
the encouraged dose volume constraints to the organs at risk ( oars ) were : volume of ipsilateral lung receiving 5gy ( v5 ) < 40% , ipsilateral lung v20 15% , ipsilateral lung v30 10% , mean ipsilateral lung dose 8 - 9gy ; total lung mean dose ( dmean ) 6gy ; heart dmean 5gy , heart v5 4050% , heart v20 < 12.5% , heart v25 < 10% . patients were followed - up at our institution for a period of at least 5years , aesthetic outcome , late toxicity , complications were analyzed . 
acute and late toxicities were calculated according to the common terminology criteria for adverse events ( ctcae ) v 4.0 as mild , moderate , severe or life - threatening . 
the kaplan - meyer analysis evaluates patients rate of late side effects , overall survival ( os ) , progression free survival ( pfs ) , localregional free survival ( lrfs ) and metastasis free survival ( mfs )  . 
the cox regression model was applied to test the influence of surgery , type of reconstruction , pathological stage , histology , neoadjuvant chemotherapy , acute toxicity , patients age and menopausal status on late side effects risk . 
the statistical analysis was performed by using spss vv 24 . results between november 2003 and october 2016 , 91 breast cancer patients were treated with post mastectomy immediate or delayed - immediate reconstruction and adjuvant rt . 
all of them received an immediate surgical reconstruction 66 ( 72.5% ) by autologous implant , 17 ( 18.7% ) with a combined ld / expander and 8 ( 8.8% ) by using pp or te ( table2 )  . 
eighty - two ( 90.1% ) patients received both chest wall and supra - clavicular lympho - nodes radiations , 4 ( 4.4% ) high risk patients were treated with rt boost . the comparison between dvh data of organs at risk relative to the different reconstructive surgery procedure did not present variation based on reconstruction method table3 . table4 outlines the incidence of acute and late toxicities among patients reconstructed with prosthesis vs . 
seventeen out of 23 ( 74% ) refer mild toxicities ( grade 1 ) which do not require surgical intervention , most of them had skin atrophy , dyschromia , telangiectasia , dyspigmentation , skin and subcutaneous fibrosis , asymptomatic fat necrosis ( cytologically proved ) or lymph - edema . 
three patients had surgery for limb - threatening ischemia , 9 patients experienced capsular contracture , had capsulectomy with or without replacement of implants and 4 patients had cosmetic surgery . 
1 late toxicity 1 3 la radiologia medica ( 2020 ) 125 : 887893 table 5 the univariate analysis of late toxicity risk variable univariate analysis not reached ( range 1142months )  . 
te tissue expander , pp permanent prothesis ( p = 0.28 ) , tumour histology ( p = 0.15 ) , patients age at diagnosis ( p = 0.42 ) , menopausal status ( p = 0.68 ) , were not related with an increased risk of late toxicity and second surgery . the fishers statistical test comparing incidence of second surgery and primary breast reconstruction did not show any statistical significance . at the time of analysis 73 ( 80.2% ) patients were still alive , and for these patients the median fup was 59months ( range 6142months )  . 
twenty - eight ( 31% ) patients had metastatic disease , the media mfs was in this observational study nearly a quarter ( 25.3% ) of breast cancer patients treated at our institution with mastectomy and immediate breast reconstruction followed by adjuvant radiotherapy , experienced late flap toxicity . 
a second surgery was done for 16 patients ( 17.6% ) , patients needed a second surgery both for treating toxicities related to treatment and for improve aesthetic outcome . a retrospective study [ 3 ] of a cohort of 296 breast cancer patients treated with mastectomy and ibr stratified by timing of rt ( previously or as adjuvant treatment ) found that the rate of acute post - surgical complications was not statistically different in patients having adjuvant rt ( 28.8% ) compared to patients who did not ( 30% )  . 
and colleagues , according to the mastectomy reconstruction outcomes consortium study , underlined a very low rate of fat necrosis ( 3.7% ) in a cohort of 108 patients reconstructed with immediate diep flap and treated with pmrt . 
the timing of autologous reconstruction relative to pmrt did not influence the total incidence of complication , although it seems that delayed reconstruction had significantly lower incidence of revisional procedures [ 1 ]  . most of our patients , considered not suitable for autologous implant , did receive a permanent prosthesis rather than 1 3 892 la radiologia medica ( 2020 ) 125 : 887893 a tissue expander , because previously published literature data illustrated that the two - step reconstruction strategy for te after pmrt was associated with an increase rate of complications . a meta - analysis compared morbidity rate among implantbased and autologous - based patients treated with ibr and pmrt . 
it showed that the risk of morbidity was less for autologous tissue compared to implant tissue ( or 020 ; 95% ci 011039 ) [ 6 ]  . literature data are not homogeneous in quantify the risk of reconstruction failure by using te or pp : most of them are single - centre study and it makes difficult to compare different surgical techniques or validated questionnaire for quantifying patients satisfaction and quality of life . 
even though , despite te seems to have more risk of failure compare to permanent implant ( 18.8% vs 7% p < 0.01 ) , patients outcome is comparable [ 7 ]  . 
a 2017 meta - analysis from 899 implant - based reconstruction cases , showed that for patients having pmrt the long - term risk of severe capsular contracture was greater in te compared to pp . 
the complete inflation of the expander did not influence target dose coverage and organ at risk toxicity when pmrt is delivered with vmat technique [ 12 ]  . oconnel retrospectively investigated aesthetic outcome , satisfaction and quality of life in 476 women who have undergone diep flap reconstruction . 
but among women who require adjuvant rt , there was not significant difference [ 13 ]  . regarding the oncological outcome of ibr and pmrt , our data are in line with published data : maalouf c . 
and colleagues [ 14 ] addressed the oncologic safety of performing immediate autologous reconstructions compared to delayed reconstruction for both localregional control and distant metastasis . limitations for this study are its retrospective nature and its small and inhomogeneous sampling size of patients treated with different type of reconstructive surgery method . conclusion the results of this study confirm that immediate breast reconstruction followed by radiotherapy , first is a safe procedure : it does not influence the oncological outcome . 
on the other hand , technical developments in both surgical and radiation fields have demonstrated that there is not a reconstructions procedure which shows an absolute advantage over the others . 
once more , this study underlines the importance of multi - disciplinary team management and the relevance of patients conscious choice before them signed the consensus form . compliance with ethical standards conflict of interest the authors declare that they have no conflicts of interest . ethical standards this study is a retrospective analysis of data . 
ebctcg , ( early breast cancer trialists collaborative group ) ( 2014 ) effect of radiotherapy after mastectomy and axillary surgery on 10 - year recurrence and 20 - year breast cancer mortality : meta - analysis of individual patient data for 8135 women in 22 randomised trials . 
pont lp , marcelli s , robustillo m , song d , grandes d , martin m , iglesias i , aso j , laloumet i , daz aj ( 2017 ) immediate breast reconstruction with abdominal free flap and adjuvant radiotherapy : evaluation of quality of life and outcomes . 
el - sabawi b , ho ah , sosin m , patel km ( 2017 ) patient - centered outcomes of breast reconstruction in the setting of post - mastectomy radiotherapy : a comprehensive review of the literature . 
jagsi r , momoh ao , qi j , hamill jb , billig j , kim hm , pusic al , wilkins eg ( 2017 ) impact of radiotherapy on complications and patient - reported outcomes after breast reconstruction . 
santosa kb , chen x , qi j , ballard tns , kim hm , hamill jb , bensenhaver jm , pusic al , wilkinset eg ( 2016 ) postmastectomy radiation therapy and two - stage implantbased breast reconstruction : is there a better time to irradiate ? plast reconstr surg 1 ( 38 ) : 761769 11 . 
ogita m , nagura n , kawamori j etal ( 2018 ) risk factors for complications among breast cancer patients treated with postmastectomy radiotherapy and immediate tissue - expander / permanent implant reconstruction : a retrospective cohort study . 
oconnell rl , di micco r , khabra k , harris pa , james se , power k , ramsey kwd , rusby je ( 2018 ) comparison of immediate versus delayed diep flap reconstruction in women who require postmastectomy radiotherapy . 
maalouf c , bou - merhi j , karam e , patocskai e , danino am ( 2017 ) the impact of autologous breast reconstruction using diep flap on the oncologic efficacy of radiation therapy . 
ann chir plast esthet 62 ( 6 ) : 630636 publishers note springer nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations . 1 3 la radiologia medica ( 2020 ) 125 : 319328 neuroradiology imaging findings inhypophysitis : areview ferdinandocaranci1 sossiocirillo5 lucabrunese1 alfonsocerase6 giuseppeleone2 andreaponsiglione3 massimomuto2 , 4 fabiotortora5 mariomuto2 received : 25 june 2019 / accepted : 28 november 2019 / published online : 20 december 2019 italian society of medical radiology 2019 abstract hypophysitis ( hp ) is a rare acute or chronic inflammatory condition of the pituitary gland . 
the aim of this review is to describe the neuroradiological findings of this rare disease , providing some information regarding the possible differential diagnosis in order to avoid unnecessary surgery . 
the features suggestive for hp include an enlarged triangularor dumbbell - shaped gland with a thickened and not obviously deviated stalk , further supported by the absence of posterior pituitary bright spot on t1weighted images , particularly in patients presenting with diabetes insipidus . 
hp should be primarily differentiated from pituitary adenomas ( including pituitary apoplexy ) , from pituitary metastases , and from other sellar and parasellar tumors , e.g. , craniopharyngiomas , germinomas , gliomas , lymphomas , meningiomas , pituicytomas , chordomas , teratomas , dermoids and epidermoids , rathkes cleft cysts , and abscesses . 
a strict collaboration with endocrinologists and neurosurgeons is mandatory in order to reach a definitive diagnosis , allowing to promptly initiating an appropriate treatment . keywords adenohypophysitis diabetes insipidus granulomatous hypophysitis hypophysitis hypopituitarism infundibuloneurohypophysitis lymphocytic hypophysitis panhypophysitis pituitary adenoma pituitary diseases pituitary gland sella turcica xanthomatous hypophysitis * ferdinando caranci ferdinando.caranci@unimol.it 1 department ofmedicine andhealth sciences v . 
population - based studies report a global incidence to be about 1 in 9 million [ 14 ]  . hp is classified as primary and secondary by etiology [ 15 ]  . 
secondary hp ( shp ) includes pituitary inflammatory processes triggered by definite etiological infective or pharmacological agents or pituitary involvement from systemic diseases . according to the pattern of pituitary involvement , hp can be classified into adenohypophysitis , infundibuloneurohypophysitis , or panhypophysitis . actually , the greatest challenge in the management of hp is establishing a diagnosis through clinical criteria and non - invasive methods and predicting the patients clinical outcome . signs and symptoms at the moment of the diagnosis , as well as pituitary hormone abnormalities , depend on the degree of pituitary involvement [ 1 , 2 ]  . severe headaches , visual disturbances due to chiasmal compression , and symptoms of endocrine insufficiency are the most common presentation . 
less frequently , inflammation can primarily involve the posterior pituitary and the stalk , presenting with symptoms related to diabetes insipidus ( di ) [ 1 ]  . central di is defined as a decreased secretion of arginine vasopressin ( avp ) leading to a high urine output ( > 3l / 24h )  . 
 moreover , the association with pregnancy [ 3 ] , as well as the significant clinical improvement after high dose of glucocorticoids [ 5 , 6 ] , supports an autoimmune hypothesis . 
these conditions are rare in the pediatric age [ 7 , 8 ]  . according to the histopathological findings , php can be classified into five types : lymphocytic ( lhp ) , granulomatous ( ghp ) , xanthomatous ( xhp ) , igg4 - related ( igg4rhp ) , and necrotizing ( nhp ) hp , which are still considered truly distinct entities by some authors or only different expressions of the same disease by others due to the possible occurrence of mixed forms [ 913 ]  . lymphocytic hypophysitis lhp is the most common histological variant of php , constituting 71.8% of all causes of php [ 1 ]  . 
nevertheless , the prevalence and incidence of lhp are not precisely known , because the possibility of diagnosis varies depending on whether it is based on clinical or histopathological criteria . lhp is predominantly encountered in young females , classically during pregnancy or in the early postpartum [ 6 ]  . 
 conversely , lhp shows a later age of onset in men . it is characterized by diffuse infiltration of the pituitary gland by t and b lymphocytes that may form lymphoid follicles [ 1 , 4 ]  . in one of the largest series of lhp , analyzing 50 cases over a period of 18years , central diabetes insipidus was the most common endocrine dysfunction ( 72% ) , and hypogonadism was the most common ( 60% ) anterior pituitary dysfunction [ 9 ]  . the main goals of the treatment are to manage pituitary hormone deficiencies as well as to reduce the inflammatory pituitary enlargement . 
therefore , different options can be considered , including replacement of hormone deficiencies ( including adh ) , anti - inflammatories , surgery , radiotherapy , or a conservative approach [ 3 , 9 ]  . high - dose suppressive glucocorticoid remains the cornerstone of medical therapy , but a variety of immunosuppressive treatments have been used [ 3 ]  . surgery may be indicated for non - responder patients , or in case of severe mass effect and visual failure . 
surgical option may be also considered when a tissue diagnosis is mandatory [ 9 ]  . radiotherapy may be useful in case of relapsing disease or in those patients requiring multi - modal treatments [ 3 , 9 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 319328 granulomatous hypophysitis primary ghp is the second commonest type of php : six ghp cases were detected in 470 operations performed during a 10 - year period [ 10 ]  . it is histologically characterized by the presence of nonnecrotizing granulomas with multinucleated giant cells , histiocytes , and lymphocyte infiltration along with plasma cells . diagnosing ghp is challenging due to the fact that many physicians are not aware of the precise details of this disease [ 11 ]  . 
although it is thought that there are no gender differences in ghp , the male - to - female ratio is 1 : 2 among the 38 cases reviewed in the literature [ 12 ]  . the clinical presentation of ghp is variable [ 12 ] , and it tends to be more severe with higher incidence of visual symptoms compared to lhp . 
headache is the most common symptopatients may present with progressive chiasmal compression , hypopituitarism , amenorrhrea , galactorrhea , hyperprolactinemia , fatigue , diabetes insipidus , and blurred vision [ 13 ]  . the presence of immunological markers of systemic conditions can help in identifying the secondary granulomatous disease . glucocorticoid therapy appears to be less effective compared with lhp , while surgical resection leads to better symptoms resolution [ 14 ]  . xanthomatous hypophysitis xhp is considered the rarest histological type . 
it is unclear whether xhp constitutes a distinct entity or a possible extension of the autoimmune or lymphocytic spectruas seen with xanthomatous lesions elsewhere in the body , it is postulated that xanthomatous infiltration results from macrophage activation secondary to chronic inflammation [ 4 , 15 ]  . 
an autoimmune etiology has also been proposed for xhp , with a recent report describing autoimmune thyroiditis noted in one patient with xhp [ 16 , 17 ]  . a predominance of female is reported in xhp with a female - to - male ratio of approximately 3 : 1 [ 4 , 15 ]  . 
interestingly , patients with lhp usually present at a slightly older age than their xhp counterparts [ 4 ]  . the gross lesion appears as a cyst filled with thickorange - colored fluid with floating crystals [ 4 ]  . 
the diagnosis can be confirmed only on tissue sections demonstrating xanthoma cells or lipid - laden macrophages in the pituitary tissue . xhp cyst size is reported ranging from 10 to 21mm in diameter [ 4 , 15 ] , slightly smaller than the sizes reported for other types of hp . xhp frequently presents with symptoms similar to those seen in pituitary adenomas [ 15 ]  . 
the clinical symptoms appear to be milder and present for a longer duration compared with other types of hp [ 4 ]  . it has been suggested that xhp may be less responsive to steroid therapy as compared to lhp , but the clinical experience is extremely limited . 
given the reported lack of effectiveness of medical management , most lesions may be treated with surgery , if not already operated on for diagnostic purposes [ 18 , 19 ]  . igg4related hypophysitis igg4rhp is considered a true distinct entity by some authors and only a different expression of the same disease by others because of the possible occurrence of mixed forms [ 4 ]  . 
notably , it is an unusual manifestation of relatively recently described igg4 - related disease ( igg4 - rd ) , which is an immune - mediated systemic condition mimicking inflammatory , infectious , and malignant processes , most commonly affecting the pancreas , mediastinum , retroperitoneum , salivary and lacrimal glands , thyroid , pachymeninges , and pituitary gland [ 20 ] , requiring extensive neuroradiological and radiological work - up . 
the most common co - existent igg4 - rd associated with pituitary disease is retroperitoneal fibrosis [ 20 ]  . it is believed to be rare , but a recent retrospective histological review reclassified 41% of lhp as igg4rhp [ 18 ]  . 
 although the epidemiology of igg4 - rd in the general population is incompletely understood , the typical patient is a male aged 60years with a 2.7 : 1 male - to - female ratio [ 21 ]  . diagnosis is challenging , remaining often elusive without a high index of suspicion . 
biopsy still remain the gold standard for diagnosis with a typical histopathological pattern of igg4 - positive lymphoplasmacytic infiltration and storiform fibrosis . serum igg4 levels are often high ( > 135mg / dl ) , often over ten times than the control groups . 
however , high levels of igg4 are neither sensitive nor specific [ 20 ]  . fluorine - 18 fluorodeoxyglucose positron emission tomography ( f18fdg pet ) is assuming an important role in patients with igg4 - rd to characterize systemic involvement . 
steroids are the mainstay treatment with a beneficial early response , but recovery of endocrine function is thought to be uncommon [ 21 ]  . necrotizing hypophysitis nhp is the rarest form of hp , reported in only three patients [ 22 , 23 ] presenting with diabetes insipidus and some degree of anterior pituitary dysfunction . 
the development of immune checkpoint inhibitors immune - related hp ( irhp ) has been strongly associated with ipilimumab , i.e. , a monoclonal antibody against the cytotoxic t lymphocyte antigen - 4 ( ctla - 4 ) [ 2426 ] , even though autoimmune thyroiditis is the more frequently observed endocrinopathy , particularly with anti - pd - 1 / pd - l1 agents [ 27 ]  . 
notably , the incidence of irhp range is 0.518% , depending on drug dose and combination with an anti - pd - 1 agent ( i.e. , nivolumab ) , while it is quite rare in patients treated with a single - agent anti - pd - 1 or anti - pd - l1 . 
 irhp usually occurs 612weeks after treatment initiation and presents with headache , fatigue , dizziness , and multiple anterior pituitary hormone deficiencies ( mostly adrenocorticotropic and thyroid - stimulating hormone or adh )  . central di seems to be an extremely rare side effect of immunotherapy . 
only two cases of central di have been previously described , the first one in a patient treated with the anti - ctla - 4 ipilimumab [ 28 ] and the second one in a patient treated with the anti - pd - l1 avelumab [ 29 ] , with and without anterior pituitary damage , respectively . 
in both patients , di was transient recovering 3days and 6weeks after starting corticosteroids , respectively , in the first and second patients . as for the anterior hp , also for the infundibuloneurohypophysitis ( inhp ) the etiology remains unknown . 
 generally , mri does not show signs of intracranial metastases neither high signal intensity on t1 - weighted images of the posterior pituitary gland , i.e. , the so - called pituitary bright spot , thought to result from the t1 - shortening effect of stored vasopressthis finding may be seen in conditions resulting in depletion of vasopressin granules and has been reported in 25100% of patients with central di . 
therefore , in case of di , without involvement of anterior pituitary lobe , mri images alone cannot be sufficient , unless a previous mri scan is available showing a pituitary bright spot [ 30 , 31 ]  . 
in view of the rarity of this condition , diabetes insipidus should be investigated in the presence of symptoms such as polyuria and polydipsia , while anterior pituitary function ( mainly pituitarythyroid and pituitaryadrenal axes ) should be periodically evaluated in patients treated with checkpoint - blocking therapies as recommended by several authors and pertinent guidelines . 
moreover , a periodic screening of the pituitary function seems to be mandatory in case of combined treatments where the risk of endocrine immune - related adverse event is higher and emphasizes the need of a multidisciplinary approach for the diagnosis of di . diagnosis is presumptive , as no surgery is usually performed , and it is generally based on association of clinical signs related to tumoral syndrome or hormonal deficits , and / or hyponatremia and proven hormonal abnormalities , and / or pituitary imaging abnormalities suggestive of hp [ 32 ]  . 
 the latter occurs more frequently in men and older patients , without a female predominance , and seems to present more frequently with hypopituitarism at diagnosis [ 24 ]  . 
most notably , a normal mri does not rule out irhp [ 32 ]  . additionally , irhp must be differentiated from metastatic disease , such as all shp in patients with cancer . 
a multidisciplinary team approach including the neuroradiologist seems mandatory to achieve correct diagnosis and management of irhp , as well as the use of shared guidelines [ 33 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 319328 neuroradiological pearls andpitfalls table 1 main magnetic resonance imaging findings in hypophysitis ( the most frequent ones are underlined ) ct scan of the head may be entirely normal or show a hypodense pituitary mass , sometimes with adjacent bony changes [ 34 ]  . 
gadolinium - enhanced mri is the technique of choice for the pituitary gland . mr technique andneuroradiological assessments the aim of mr imaging is to obtain a high - spatial - resolution imaging with a reasonable signal - to - noise ratio , in order to identify the gland and separate it from the lesion . 
high - spatial detail should be achieved through thin slice ( 23mm or thinner ) , a fine matrix size ( 256 512 or more ) , and a relatively small field of view ( fov )  . 
the use of half dose ( 0.05mmol / kg ) is considered the standard choice : studies performed both on pituitary tumors and in normal gland reported no significant loss of sensitivity using a 50% reduction of the usual dose of contrast mediusmaller pituitary lesions can be recognized generally for their reduced enhancement in comparison with the contiguous normal gland , particularly immediately after contrast ( dynamic studies by consecutive series ) [ 3537 ]  . the use of a three - dimensional ( 3d ) acquisition with very thin sections ( up to 1mm ) presents important advantages as compared to conventional se sequences , including high signal - to - noise ratio [ 36 ]  . 
isovolumetric gradient echo t1 - weighted ( w ) mr sequences ( volumetric interpolated brain examination , vibe , or magnetization - prepared rapid acquisition with gradient echo , mp - rage ) have been reported to substantially improve imaging resolution and allow for multiplanar reconstructions ; however , contrast enhancement may be less conspicuous compared to spinecho images [ 35 ]  . several studies attempted to define lesion component and consistency by using conventional and some novel mri sequences with controversial results , especially regarding diffusion - weighted imaging ( dwi )  . 
this sequence has shown utility in assessing the consistency of adenomas , but with no convincing data , due to the b0 - related artifacts in the sellar region [ 36 ]  . mri features suggestive ofhp these include ( table1 ) an enlarged triangularor dumbbell - shaped gland with thickened and not obviously deviated stalk , possibly supported by the absence of posterior pituitary bright spot on t1w images , particularly in patients moderate gland enlargement ( triangular or dumbbell shaped ) symmetrical suprasellar gland extension generally homogeneous contrast enhancement empty sella as atrophic response after the inflammatory process thickened , not deviated pituitary stalk absence of posterior pituitary bright spot on t1w images adjacent dural enhancement sphenoid sinus mucosal thickening presenting with diabetes insipidus [ 34 , 38 ]  . 
the enlarged gland is typically isointense with the brain on t1w images and frequently heterogeneous on t2w images [ 4 ] , commonly associated with symmetrical suprasellar extension . the presence of pituitary stalk thickening , in the appropriate clinical setting , is perhaps the strongest predictor of an inflammatory process [ 38 ]  . 
contrast enhancement pattern is quite variable and cannot be used as a reliable feature in differentiating this condition from pituitary adenoma ( figs.1 , 2 ) [ 40 ]  . 
dural enhancement has been reported in some cases after contrast administration ( fig.2a ) [ 34 ]  . among these mri features , diffuse , mild - to - moderate pituitary expansion with significant homogeneous or fig . 
1 coronal ( a ) and sagittal ( b ) unenhanced t1 - weighted images , and gadolinium - enhanced coronal ( c ) and sagittal ( d ) t1 - weighted images show a triangular pituitary enlargement with marked inhomogeneous contrast enhancement and a small cystic component ( arrow ) , associated with thickened and markedly enhancing pituitary stalk 1 3 324 la radiologia medica ( 2020 ) 125 : 319328 heterogeneous gadolinium enhancement and thickening of the pituitary stalk are the most important findings of hp [ 34 , 3840 ]  . in a recent analysis of neuroradiological findings of php in a large cohort of patients [ 41 ] , the median pituitary height and volume were found significantly higher in adenohypophysitis and panhypophysitis , median pituitary stalk thickness ( both at insertion and optical chiasm levels ) was significantly larger in adenohypophysitis and panhypophysitis cases , while pituitary stalks ( at the optical chiasm level ) were larger in infundibuloneurohypophysitis . 
the difference between the stalk diameters evaluated at the optic chiasm and pituitary insertion levels was significantly larger in infundibuloneurohypophysitis , but not in adenohypophysitis and panhypophysitis . moreover , the neuro - pituitary bright spot on t1w images was conserved in all adenohypophysitis and lost in all panhypophysitis and infundibuloneurohypophysitis . 
2 enhanced sagittal ( a ) and coronal ( b ) t1 - weighted images showing global symmetrical pituitary enlargement with slight suprasellar extension and marked inhomogeneous contrast enhancement , extending up a thickened infundibulum to the hypothalamus , associated with thickened and enhancing dura along the clivus dorsal surface . 
enhanced sagittal ( c ) and coronal ( d ) t1 - weighted images obtained 15 days after steroid therapy showing shrinkage of the sellar content , normalization of the pituitary stalk , and reduction of the enhancing dura ; t1 hyperintense neurohypophysis is now clearly demonstrable 1 3 la radiologia medica ( 2020 ) 125 : 319328 despite the systematic scoring , the differentiation remains difficult . 
on the other hand , pituitary necrosis can be found in various conditions , most commonly in adenomas with apoplexy and sheehan syndrome . irhp presents not specific mri features [ 2734 ]  . 
in 30100% of patients , they are similar to lhp , including variable increase in the pituitary gland volume ( generally showing a convex aspect ) , intense contrast enhancement ( which is generally homogeneous and only sometimes heterogeneous ) ( fig.3 ) , sometimes associated with an enlarged pituitary stalk , and , rarely , involvement of the posterior pituitary . 
 this addresses the issue of mri images centered on the pituitary gland in the first cranial mri performed in patients undergoing immunotherapy , although this issue seems to be overcome by routinely use of volumetric sequences . the main differential diagnoses include metastases , adenoma , apoplexy , meningioma , leptomeningeal metastases , as well as other forms hp . 
despite some movement artifacts , unenhanced t1 - weighted ( a ) and gadolinium - enhanced t1 - weighted ( b ) sagittal mr images show typical enlargement and homogeneous contrast enhancement of the anterior pituitary gland . 
the arrow indicates the posterior pituitary gland showing normal high signal intensity on t1 - weighted mr images not uncommonly , the presence of an empty sella may be considered as the atrophic response after the inflammatory process [ 42 ]  . the characterization of the unusual sellar mass is not straightforward and generally results in a wide differential . 
 hp should be primarily differentiated from pituitary adenomas ( including pituitary apoplexy ) [ 43 ] , from pituitary metastases , and from other sellar and parasellar tumors , e.g. , craniopharyngiomas , germinomas , gliomas , lymphomas , meningiomas , pituicytomas , chordomas , teratomas , dermoids and epidermoids , rathkes cleft cyst , and abscesses [ 4446 ]  . 
furthermore , pituitary enlargement can occur in sheehans syndrome [ 47 ] at onset or more rarely in thyrotropic hyperplasia associated with severe , untreated primary hypothyroidism [ 48 , 49 ]  . 
additionally , the primary diagnosis should take into account paraphysiological gland modifications : physiological pituitary hypertrophy occurs in children and adolescents ( especially pubertal females ) and perimenopausal women ; pituitary hyperplasia is normally associated with pregnancy . to aid distinction between pituitary adenoma and hp , a neuroradiological scoring system has been proposed [ 5 ]  . 
the relation with pregnancy , pituitary mass volume and symmetry , signal intensity and homogeneity after gadolinium administration , posterior pituitary bright spot presence , stalk size , and mucosal swelling were used for the calculation of the score . 
the score ranges from 13 to + 8 and a 1 score was suggestive of adenoma , whereas a 0 score suggested hp [ 5 ]  . 1 3 326 la radiologia medica ( 2020 ) 125 : 319328 fig . 
four months after starting ipilimumab , there is a subtle increase in the volume of pituitary gland ( b ) followed by evolution in clear - cut empty sella 6months later on ( c )  . 
presence of an intraand suprasellar enhancing mass with thickened pituitary stalk , irregular margins , and inhomogeneous structure 1 3 la radiologia medica ( 2020 ) 125 : 319328 conclusions hp is a challenging diagnosis ; it can be made in a patient with otherwise unexplained hypopituitarism with characteristic mri findings including diffuse pituitary gland enlargement and / or a thickened pituitary stalk . 
obviously , a strict collaboration with endocrinologists and neurosurgeons is mandatory to reach a definitive diagnosis , allowing to promptly initiating an appropriate treatment . acknowledgements the authors wish to thank maria giulia pietrini , md , unit of diagnostic imaging , maria ss . 
further analysis was conducted by dividing the patient group into high - risk patients ( 20% ) and low - risk patients ( < 20% ) according to the pulmonary arterial obstruction index . 
 although pulmonary angiography is still the gold standard in diagnosis , noninvasive diagnostic methods are preferred over angiography because it is an invasive method and cannot be applied in every medical center [ 2 ]  . 
in our study , the mean paoi values of patients diagnosed as having ape using ctpa and the mean cross - sectional areas of the 4 pulmonary veins at the ostium level ( csapv ) were calculated , and the relationship between these values was evaluated . material andmethods patient selection the study protocol was approved by the local ethics committee of trakya university medical faculty . 
 the control group of the study comprised 101 patients who were examined with ctpa in the emergency radiology department with the suspicion of ape , but who had no embolisms . 
healthy controls were selected from among patients to approximately match the age and sex distribution of the patient group . the exclusion criteria were as follows : history of previous pulmonary embolism , having an accessory pulmonary vein with the exception of 4 pulmonary veins draining into the left atrium , pulmonary hypertension , right heart failure , lung or pleural malignancy , history of thoracic surgery , history of radiotherapy to the thoracic region , history of previous fibrosing mediastinitis , mediastinal mass , parenchymal consolidation or atelectasis and severe pleural or pericardial effusion . ct acquisition the patient group was scanned on an eight - channel multislice toshiba aquilion 64 ( toshiba medical systems , tokyo , japan ) computed tomography ( ct ) scanner . 
a contrast - enhanced multi - slice ct of the pulmonary arteries was performed from the lung apices to the lowest level of the hemidiaphragm with the patient in the supine position during suspended inspiration . 
a total volume of 120ml of iodine - based nonionic contrast material ( 300mgi / ml ) wasadministered intravenously using a power injector at a rate of 4ml / s . 
all axial images were viewed using standard mediastinal ( level , 40 hu ; width , 350 hu ) and lung window settings ( level , 700 hu ; width , 1000 hu )  . image analysis ape detection andpaoi evaluation ctpa images of both the patient and control groups were evaluated by two senior radiologists ( feu , ss ) who have over 10years experience in thoracic and vascular imaging . 
according to the location , each segmental artery distal to the proximal pulmonary artery ( common or lobar ) with thrombus was calculated as 1 point , and the total number of affected segmental arteries was added to the total score . 
isolated thrombi in one segmental artery were scored as 1 point . pulmonary artery occlusion evaluation was performed as follows : the filling defect in the lumen of the pulmonary artery and observation of contrast material at the same time was evaluated as partial thrombus . 
as a result , complete vascular patency was scored as 0 points , partial thrombus was scored as 1 point , and complete occlusive thrombus was scored as 2 points . 
paoi is determined by the sum of the scores of the segmental arteries ( minimum 1 , maximum 20 ) according to the degree of obstruction ( minimum 0 , maximum 2 )  . 
each measurement was performed three times , and the mean values were recorded . measurement ofright andleft atrial areas both atrial areas were calculated from the original axial images in ctpa using the methodology specified by aviram etal . 
both radiologists calculated the left atrium ( la ) and right atrium ra areas from planimetric measurements obtained from freehand delineation of the atrial borders . statistical analysis statistical analyses were performed using the spss commercial software ( spss version 16.0 , spss , chicago il , usa )  . 
data are summarized as mean standard deviation ( sd ) for continuous variables and as number of individuals for categorical variables . pearsons correlation was used to evaluate the correlations between variables and paoi . the differences of csapv between patients and control subjects and the differences among subgroups of patients based on their paoi were studied using students t test . the csapv cutoff value that maximized the accuracy for the diagnosis of ape was established using a receiver operating characteristic ( roc ) curve . 
b direct coronal reformatted image shows that the crosshair on the left superior pulmonary vein ( * ) has been rotated to generate an oblique sagittal image at the ostiuc oblique coronal image shows the left superior pulmonary vein ( arrows ) in cross section perpendicular to the long axis of the vessel . 
a : ascending aorta , ao : aortic arch , p : main pulmonary artery 1 3 268 la radiologia medica ( 2020 ) 125 : 265271 intraclass correlation coefficients ( iccs ) were used to assess interobserver agreement in mean pulmonary vein area measurements . 
 [ 13 ] evaluated pulmonary veins using ctpa in patients with ape and reported that vein diameters were reduced when compared with ctpas performed before embolishowever , in their study , diameter rather than pulmonary vein area was evaluated . 
 [ 7 ] showed the association between increased clot load in pulmonary arteries and the decrease in left atrial area and increase in right atrial area in patients with ape . 
our results , in parallel with that study , found a decrease in la area and an increase in ra area in patients with ape . pathophysiologic studies showed that pulmonary embolism increased pulmonary vascular resistance due to anatomic obstruction caused by embolisthis is due to vasoconstrictive agents and the reflex hypoxemia that occurs during embolism [ 14 ]  . 
this sudden increase in right ventricular afterload leads to an increase in right ventricular wall tension and right ventricular dilatation , causing shift toward the left ventricle in the interventricular septum and a decrease in left ventricular diastolic volume . 
as a result , reduction of cardiac output , systemic blood pressure , and coronary perfusion causes reduced left ventricular filling and ultimately circulatory collapse is inevitable [ 15 , 16 ]  . the significance of our study is its proposal of an additional parameter as csapv that reflects modifications in cardiac morphology in response to pulmonary arterial obstruction in patients with ape . lungs have a dual blood supply system formed by the bronchial and pulmonary arteries , and pulmonary venous drainage is rarely disrupted . 
after the blood flowing through the pulmonary capillary , blood reflux in pulmonary vein branch decreased , leading to decreased blood supply from pulmonary vein to the left atrium ; this was described as insufficient contrast medium filling in pulmonary vein in ctpa image by zhang etal . 
these contradictory results confirm studies indicating that the prognosis of ape may be related with the burden of embolism and the patients cardiopulmonary reserve [ 14 , 16 ]  . 
currently , the qanadli method [ 5 ] is commonly used for calculating paoi using ctpa to assess the severity of ape ; however , no studies have investigated pulmonary vein area in patients with ape . in this study , we investigated the correlation between pulmonary artery embolism burden and pulmonary vein area in patients with ape . 
in addition , csapv is an alternative measure of 1 3 270 la radiologia medica ( 2020 ) 125 : 265271 more comprehensive studies are still needed to clarify this issue . 
the negative correlation found in our study between paoi and the csapv suggests that csapv , with its higher sensitivity for differentiating high - risk ape , might provide information regarding thrombotic burden . although ctpa is noninvasive , this method can be problematic in some patient groups . 
the decrease in csapv correlates with the severity of ape ; however , it is more accurate to consider csapv measurement as an adjunct and additional method to ctpa , rather than replacing it . the interobserver variability of csapv measurement was excellent with an icc of 0.992 for the control group and 0.963 for the patient group . 
first , although many radiologic and non - radiologic parameters were used in the evaluation of ape in the literature , we analyzed only the ra and la areas to compare csapv . 
there are studies in the literature indicating that echocardiography is an important method for short - term mortality risk stratification in patients with ape [ 24 , 25 ]  . 
another limitation is the inability to provide sufficient data on the relationship between our findings and patient outcomes because most causes of death were not only due to pulmonary embolism . conclusion when evaluating the relationship between the degree of embolism - induced obstruction and the area of the pulmonary veins , high pulmonary artery thrombus burden was associated with low pulmonary vein area . 
our findings suggest that the evaluation of csapv using ctpa in patients ape may serve as an additional early parameter reflecting changes in cardiac morphology in response to the degree of pulmonary artery obstruction and may contribute to a more comprehensive risk assessment in these patients . funding this study was not supported by any funding . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance withthe ethical standards of the institutional and / or national research committee and with the 1964helsinki declaration and its later amendments or comparable ethical standards . 
computed tomography images of patients with dual left anterior descending artery were then reviewed , and the morphological features of dual left anterior descending artery were evaluated . results dual left anterior descending artery was identified in 1.3% of the patients in this study population . 
four additional cases that were not classified before were also detected . conclusion dual left anterior descending artery has a variety of subtypes reported mostly as odd cases , and gaining diagnostic awareness of dual left anterior descending artery is more critical , rather than listing and counting the subtypes . 
additional subtypes * mehmet eker hikmet.irfan@hotmail.com 1 department ofradiology , faculty ofmedicine , medipol mega hospital , istanbul medipol university , tem avrupa otoyolu gztepe k no : 1 , baclar , 34214istanbul , turkey of this anomaly were later published , especially with the use of ccta [ 614 ]  . the lad normally originates from the left main coronary artery ( lmca ) , courses in the anterior interventricular groove ( aivg ) and gives off the diagonal and septal branches . 
short lad typically terminates high in the aivg , and long lad courses outside the aivg proximally and returns to the groove in its distal course [ 3 ]  . dual lad is usually detected incidentally during cca or ccta , and most of them have little clinical importance . 
at present , a large number of ccta examinations are being performed and it has become inevitable for ct interpreters to be aware of dual lad . the aim of this study was to identify the prevalence of dual lad and define the morphological features using ccta in order to raise diagnostic awareness of dual lad among radiologists . methods study population the radiologic reports of 1912 patients who underwent electrocardiography ( ecg ) - gated ccta at our institution from october 2012 to august 2018 were retrospectively searched for the presence dual lad . 
then , ccta images of these patients were reviewed in detail for the presence and morphological features of dual lad by another radiologist with 8years of experience in cardiac imaging using multiplanar reformatting , maximum intensity projection and volume rendering . ct scans all ct scans were obtained with a 256 slice multidetector row ct scanner ( brilliance ict , philips healthcare , best , the netherlands ) with prospective ecg - gating mode ( step and shoot cardiac , philips healthcare , usa ) following the dynamic injection of nonionic low osmolar iodinated contrast material ( iohexol 350mgi / ml , omnipaque , opakim medical products inc , istanbul , turkey )  . 
the contrast material was injected intravenously via automatic power injector ( medrad stellant ct injection system , bayer healthcare llc , pittsburg , usa ) at a dose of 1 , 5ml / kg body weight , with a rate of 5ml / s , followed by 50ml of saline solution at a flow rate of 5ml / s through an upper - extremity intravenous cannula . 
the ct data acquisition time was determined with the bolus - tracking technique by placing the region of interest in the ascending aorta and setting the trigger threshold to 150 hounsfield units . in the absence of contraindications , oral beta - blockers ( 50100mg metoprolol , beloc zok , astra zeneca , istanbul , turkey ) 1h before the examination and / or intravenous beta - blockers ( 520mg metoprolol , beloc ampoule 5mg / ml , astrazeneca , istanbul , turkey ) just before the scan were used when the heart rate was greater than 70 beats per minute . ct scans were performed with detector collimation of 128 0.625mm , tube voltage of 100120kvp using automated tube current modulation , gantry rotation time of 0.27s and with a weight - based determination of mas . 
coronary images were obtained with prospective ecg gating at a phase of 75% rr interval during a single breath hold . the data were transferred to a workstation ( philips intellispace portal workstation , philips healthcare , best , the netherlands ) from picture archiving and communication system ( centricity universal viewer , ge medical systems , milwaukee , wis , usa ) for image post - processing and analysis . image evaluation the diagnosis of dual lad was made when two different vessels were identified in the aivg of the heart . 
in addition , dual lad anomalies inconsistent with any of the previously reported subtypes were also detected . in addition to determining the subtype of dual lad , length and caliber of lmca and lad , the caliber of long and short lads ( in the proximal 1 cm segments ) were measured . the diagonal and septal branching patterns were also statistical analyses were performed with a software program , spss 16.0 for windows ( spss , chicago , il , usa )  . 
of the other six cases , one was type 9 and one was type 10 ( figs.2a , b and 3 )  . beside these , four cases , including two cases that were not reported before and a case previously reported but not classified , were observed in our study . in one of these , the right coronary artery ( rca ) , the left circumflex artery ( lcx ) and the long lad originated from 1 3 la radiologia medica ( 2020 ) 125 : 247256 fig . 
three - dimensional volume rendered heart image shows long ( long arrow ) and short ( short arrow ) lads branching from the proper lad ( arrowhead ) in the anterior interventricular groove . 
the proper lad gives rise to a left ventricular diagonal branch ( curved arrow ) the right coronary sinus ( rcs ) and the short lad originated from left coronary sinus ( lcs )  . 
the long lad had a prepulmonic course anterior to the right ventricular outflow tract ( rvot ) and it finally entered the groove distally , while the aberrant lcx had a retroaortic course . 
to the best of our knowledge , this case was the second in literature [ 13 ]  . in the second of these four cases , lmca was not observed and the lcx and the proper lad originated from the lcs with separate ostia . 
three - dimensional volume rendered heart images ( a , b ) show long ( long arrow ) and short ( short arrow ) lads originating from the proper lad ( arrowhead )  . 
three - dimensional volume rendered heart image shows the long lad ( long arrow ) originating from the right coronary sinus with separate ostium than right coronary artery ( arrowhead )  . 
the short lad ( short arrow ) originates from the left main coronary artery ( curved arrow ) and terminates in the proximal aivg subtypes described in this study , but neither reported nor classified before , are summarized in table3 . the left ventricular diagonal branches originated from the long lad ( 9 / 19 ) , the proper lad ( 4 / 19 ) and from both ( 6 / 19 ) in type 1 and from the long lad ( 4 / 6 ) and from the short lad ( 2 / 6 ) in non - type 1 . in type 1 dual lad , the major septal branches arose from the short lad ( 9 / 19 ) , the proper lad ( 9 / 19 ) and from both ( 1 / 19 )  . 
in non - type 1 dual lad , the short lad ( 5 / 6 ) and both the proper and the short lad ( 1 / 6 ) gave rise to major septal branches . the length and caliber measurements of the lmca , the caliber measurements of the short , long and proper lads in the proximal 1cm segment and the diagonal and septal branching patterns of dual lad subtypes are given in table4 . coronary artery disease requiring surgical or percutaneous intervention was detected in five patients with dual lad . 
globe maximum intensity projection image ( a ) shows right coronary artery ( arrowhead ) , left circumflex artery ( lcx ) ( curved arrow ) and the long lad ( long arrow ) originating from the right coronary sinus and the short lad ( short arrow ) from the left coronary sinus . 
the long lad reaches the anterior interventricular groove ( aivg ) following a prepulmonic course , and lcx follows a retroaortic route and reaches to the normal location ( pa , pulmonary artery ; ao , aorta )  . 
threedimensional volume rendered heart image ( b ) shows short lad ( short arrow ) terminating high in the aivg and long lad ( long arrow ) reaching the distal part of the aivg after coursing outside the groove proximally 1 3 la radiologia medica ( 2020 ) 125 : 247256 fig . 
three - dimensional volume rendered heart image shows left circumflex artery ( curved arrow ) and proper lad ( arrowhead ) originating from the left coronary sinus with separate ostia . 
 the proper lad gives rise to long ( long arrow ) and short ( short arrow ) lads lad , in one patient short lad and in one patient proper lad were stenotic . 
four patients underwent successful revascularization , and the other patient had no cardiovascular intervention . discussion the prevalence of dual lad was 1.3% ( 25 dual lads among 1912 cases ) in our study . 
largest series in the existing literature using ccta [ 6 ] reported the prevalence to be 4% ( 56 dual lads among 1337 cases ) , and this is approximately four times greater than ours . 
patient selection for this study was based on radiologic reports , and although all of the images were interpreted by radiologists experienced in cardiac imaging , it cannot be warranted that all dual lad fig . 
this might be the reason for this discrepancy . the prevalence of dual lad reported in the largest series based on ccta is more than the prevalence described in the cca literature ( 4% and 1% , respectively ) [ 3 , 6 ]  . 
ccta , with the ability to obtain detailed , high - quality , motion - free , reformatted and three - dimensional images , has become the method of choice for detection and classification of congenital coronary artery anomalies [ 14 , 6 ]  . 
ccta has the advantage of being noninvasive and is also safer and faster than cca [ 1 ]  . to date , there are 10 dual lad subtypes classified in literature [ 69 , 11 , 12 ] , but there is a confusion in the definition of type 7 dual lad . 
in this case , a long lad , originating from the rcs and coursing intramyocardially within the septal crest before entering the distal aivg , and a short lad , originating from the lmca , were observed . 
the septal perforators were reported to originate from both the short and the long lad , whereas the diagonal branches originate from the short lad . apart from these , there are unclassified variations of dual lad anomaly reported as case reports in the literature . 
in one of these [ 13 ] , dual lad anomaly with a long lad , lcx and a rca sharing a common origin from the rcs and a short lad originated from the lcs were reported . 
it differs from type 5 with the existence of aberrant lcx and the long lad with a prepulmonic course ( intramyocardial course within the septal crest in type 5 ) before reaching the distal part of the aivg . other than this , there is another unclassified subtype reported by shizukuda and effat [ 14 ]  . 
in this case , a short lad originating directly from the lcs and coursing intramyocardially and a long lad branching from the lmca were described . type 1 dual lad is by far most the common subtype of dual lad , and other subtypes of dual lad are described only as case reports in literature [ 614 ]  . 
moreover , two additional cases that were not reported before and a case 1 3 254 la radiologia medica ( 2020 ) 125 : 247256 previously reported but not classified were detected . 
since they have similar characteristics with types 1 and 5 and have no additional clinical significance , it was considered appropriate to classify these as variants of types 1 and 5 ( second and third variant of type 1 , and type 5 variant , respectively ) , rather than novel dual lad types . diagonal and septal branching patterns may also differ among the dual lad subtypes . 
in type 1 dual lad , major septal branches originate from the short lad and / or the proper lad , whereas left ventricular diagonal branches originate from the long lad and / or proper lad . 
 in this study , we did not observe any short lad that gives rise to right ventricular diagonal branches in type 1 dual lad , but in the case with second variant of type 1 , right ventricular diagonal branch originated from the short lad . 
the cases of dual lad in this study were consistent with the existing literature [ 3 , 4 , 6 ]  . measurement of the length and the caliber of the lmca and the proper lad and the calibers of the short and the long lads in dual lad have been reported in only one study in the literature , and our results are largely consistent with this study [ 6 ]  . dual lad anomalies are usually asymptomatic in the absence of stenosis . 
however , in certain types there is an aberrant artery originating from the opposite coronary sinus or the rca and subsequent course of the aberrant artery may cause symptoms [ 3 , 4 , 1517 ]  . 
the presence of an interarterial course is believed to be associated with sudden cardiac death and thus is an indication for surgical correction if evidence of myocardial ischemia or previous syncope is present [ 2023 ]  . in types 4 , 5 , 6 , 8 and 10 , there is an aberrant coronary artery ( long lad and / or lmca ) originating from the rcs or the rca [ 3 , 68 , 12 ]  . 
 [ 11 ] and in the dual lad case which was classified as type 5 variant in this study , there is an aberrant coronary artery originating from the opposite side . 
the transseptal course of aberrant artery appears similar to the interarterial course , but in transseptal course the artery passes more inferiorly within the muscular septum and is generally believed to be benign . 
therefore , these may have more clinical importance than other types with a prepulmonic or a retroaortic course . dual lad subtypes with aberrant artery originating from the rcs or the rca are summarized in table5 . in addition , dual lad anomaly may be of critical importance in the presence of coronary artery disease , because the culprit stenotic lesion causing the symptoms may be present in one or both lad . 
although it is not clear whether there is a relationship between coronary atherosclerosis , and dual lad or other congenital coronary artery anomalies , because coronary atherosclerosis is prevalent , these conditions may simply coexist and lack of this information may result in either deficient or wrong revascularization [ 3 , 4 , 6 , 16 , 24 ]  . 
besides , preoperative diagnosis of dual lad can help to choose the correct site for arteriotomy and increase surgical success [ 12 , 16 ]  . in this study , five patients who had dual lad superimposed with coronary artery disease requiring surgical or percutaneous intervention were detected and there was no revascularizations gone wrong because of misdiagnosis of dual lad . 
in one of these , sajja and colleagues [ 16 ] described four successful operations of the dual lad distribution and have emphasized the incorrect placement of an arteriotomy due to misrecognition of the anomaly ; difficulties in identification and grafting of a short lad and the intramyocardial course of the aberrant vessel are of concern during surgical revascularization . in patients with acute coronary syndrome , cca is the standard method for diagnosing coronary artery disease and it is easy to miss dual lad by cca . 
in such cases , repetition of cca or utilization of ccta for full evaluation of coronary arteries may provide valuable information and help clinicians to diagnose and manage patients properly . this study has some limitations . 
first , cases for this study were selected using the keywords dual lad , double lad and congenital coronary artery anomaly in radiologic reports , and ccta images of only selected cases were examined . 
 however , it has been shown that ccta sensitivity in visualization of abnormal vessels is 100% [ 1 ]  . in conclusion , dual lad anomalies are rare congenital coronary anomalies with a variety of subtypes reported mostly as single case reports and it will not be surprising to detect additional subtypes in the future , especially due to increased familiarity with dual lad . 
the aim of this survey was to evaluate the level of awareness within the italian radiation oncologist community on this topic . materials and methods a survey was promoted by the young group of italian association of radiotherapy and clinical oncology ( airo ) with a questionnaire made up of 22 questions allowing for multiple answers , which was administered , both online and on paper version . 
it was addressed to radiation oncologists , airo members , participating in the national congress held in 2015 . results a total of 113 questionnaires were collected back and analyzed ( survey online : 50 respondents ; paper version : 63 )  . 
there is a general low rate of referral for a preliminary cardiological evaluation in patients bearing pm / icds , in line with some published surveys ; nevertheless , a focused attention to certain specific treatment factors and patient - centered point of view emerged . conclusions a generally good awareness of this topic was shown but homogeneous application of gl was not observed , possibly due to the multiplicity of available gl . 
a prospective data collection could help to better clarify the shadows on this topics . keywords cancer radiotherapy pacemaker and implanted cardioverter defibrillator italian survey introduction after 1958 , when the first implantation of a pacemaker ( pm ) in humans was performed by senning and elmqvist , cardiac implantable electronic devices ( cieds ) became * silvia chiesa silvia.chiesa@policlinicogemelli.it 1 uoc di radioterapia oncologica , dipartimento diagnostica perimmagini , radioterapia oncologica ed ematologia , fondazione policlinico universitario a . 
gemelli irccs , rome , italy 2 dipartimento di oncologia radioterapia oncologica , universit di torino aou citta della salute e della scienza , turin , italy 3 radioterapia oncologica , policlinico universitario campus biomedico , rome , italy one of the principal treatments for cardiac rhythm alterations [ 1 , 2 ]  . 
for this reason , over the last several decades , implantation rates of artificial cardiac devices have progressively increased , with the most prominent global growth observed between 2005 and 2009 [ 3 , 4 ]  . 
the 4 rem radioterapia viagrande catania , catania , italy 5 dipartimento di radioterapia oncologica , universit e asst spedali civili di brescia , brescia , italy 6 dipartimento di scienze biomediche sperimentali e cliniche mario serio , radioterapia oncologica , azienda ospedaliero - universitaria careggi , florence , italy 7 dipartimento di radioterapia oncologica , ospedale generale regionale f . 
miulli , acquavivadellefonti , bari , italy vol . : ( 0123456789 ) 1 3 330 la radiologia medica ( 2020 ) 125 : 329335 numbers are impressive with more than 700 , 000 new pms and 200 , 000 new implantable cardioverter defibrillators ( icds ) implanted worldwide each year [ 15 ]  . 
also in italy , the number of ieds reached in 2013 , about 16.519 , as 277 per million of habitants . in 2012 , the first two leading causes of deaths were cardiovascular diseases ( 17.5 million deaths ) and cancers ( 8.2 million ) [ 6 ]  . 
this phenomenon is favoured by the so - called elderly tsunami : the aging of the populations is one of the main economic and social changes of the twenty - first century . 
cardiovascular disease and cancer are both primarily associated with the elderly condition , and so with the growing of the aged population , the overlap between these two categories will continue to rise [ 3 ]  . due to these preliminary considerations , the probability that some of pm / icd patients will develop malignancies and receive radiotherapy ( rt ) treatment is increasing [ 1 ]  . rt has been considered an established treatment option in cancer care , in both curative and palliative setting : at least 60% of all cancer patients will require rt during the course of the disease [ 8 ]  . 
in 19902000 , some authors reported that 0.40.5% pm / icd patients received rt and estimated the presence at least of ten pm patients per year in a rt department [ 911 ]  . 
in fact , it is estimated that about half of pm / icd patients are not evaluated after rt and a multidisciplinary evaluation between cardiologists and radiation oncologists is frequently lacking [ 14 , 15 ]  . the aim of the pacemaker and implanted cardioverter defibrillator management in radiation therapy ( paideia ) survey , promoted by the young group of italian association of radiotherapy and clinical oncology ( airo ) , was to evaluate the awareness within italian radiation oncologists about the management of pm / icd patients requiring materials andmethods population andsetting the paideia project questionnaire was designed to investigate the level of awareness and the knowledge about the management of the pm / icd in patient undergoing rt in order to provide a global scenario on the conduct and to elaborate recommendation to be used in clinical practice . during the airo national congress held in 2015 , anonymous questionnaires were presented and given to the young ( under 40 according to airo statute ) radiation oncologist attending the congress ( both specialists and young residents )  . 
therefore , the survey was conducted both online , employing the internet - based surveymonkey platform ( ymonk ey.com ) —and on a paper version , and completion took about 20min . the survey was also open from the national congress to the next 5months to all the members of the association , and the completed questionnaires were collected and analyzed anonymously during 2016 . the present analysis and survey was conducted before the publication of the italian recommendations on this topic [ 14 ] , just to guarantee not - conditioned answers and to make a comparison with these recommendations . questionnaire development a 22 item - based , nonvalidated , self - produced questionnaire was designed by the paideia project working group ( see online resource paideia_surveyairogiovani for complete form )  . 
in order to assess validity of the questionnaire , the format was shared among the members of the airo young working group board and looked over again by two external reviewers for suggestions regarding improvement in content , wording and flow of presented questions . the items were grouped in different domains : a first part with details collection regarding the radiation oncologist filling in the questionnaire ( age , working experience , role on public or private hospital , academic or nonacademic title , working region in italy ) ; a second part focused on the level of knowledge on pm / icd characteristics and the awareness about the management according to guidelines ; and a third part about the clinical practice in terms of multidisciplinary approach , general management and personnel suggestions . inclusion anddata collection two hundred questionnaires were administered to young radiation oncologists before the start of the congress , at the time of registration at the desk . 
 among the members of the airo , more than five hundred residents and young specialists in radiation oncology were contacted by e - mail in the weeks following the national congress and asked to participate in the present study . 
a cover letter outlining the purpose of the survey together was enclosed to the questionnaire . data were collected until january 2016 . only questionnaires containing all the answers were considered for the final analysis . 
the detailed characteristics are reported in fig.1. knowledge andawareness oftheissue ninety percent of physicians were aware of the difference between pm and icd , and 64 / 113 ( 57% ) knew the american association of physicists in medicine ( aapm ) tg - 34 guidelines [ 16 ] , but only in 19 / 113 cases ( 17% ) these guidelines were used for clinical practice . 
the details about the answers are reported in fig.2. clinical practice according to the questionnaires , a multidisciplinary approach in the management of pm / icd is not routinely applied , while it is preferred to involve the cardiologist according to the clinical conditions of the patient ( 47% of cases )  . 
the manufacturing company would be generally consulted if indicated by the cardiologist ( 57% )  . regarding the clinical experience , the cumulative dose to the device is always calculated in 58% of cases , regardless of irradiation site , while in 33% of cases it is estimated only in case of the thoracic radiotherapy . approximately half of interviewed physicians ( 49% ) consider a maximum dose < 2gy to the device as a constraint , according to the guidelines [ 16 ] , while 10gy and 1gy were considered as dose limits in 17% and 34% of respondents , respectively , without differences between pm and icd . in most cases , neither the deployment ( 81% ) nor the disabling ( 83% ) of the device is reported . the last part of the questionnaire ( details reported in figs.3 , 4 and 5 ) was intended to explore the level of knowledge of the topic . 
most respondents were aware of the influence on the function of the device of dosimetric aspects such as beams direction ( 89% ) and beams energy ( 43% ) , independently of the irradiated site . 
4 clinical practice : general management of pacemaker and implanted cardioverter defibrillator management in radiation therapy the majority of the answers are oriented to the close monitoring of the patients during the delivery ( 68% ) , after the radiotherapy session in a dedicated electrophysiological service according to the manufacturer recommendation ( 80% )  . 
about one - third of specialists confirm the close monitoring at 1 , 3 and 6months after the end of the radiotherapy , while the remaining part of colleagues would manage the follow - up according to the indication of the cardiologist ( 65% )  . 1 3 la radiologia medica ( 2020 ) 125 : 329335 fig . 
5 clinical practice : personnel suggestions discussion the topic of pm / icd patients needing a rt treatment is becoming an important issue to face , not only among radiation oncologists but also cardiologists , as shown in a recent survey of the european heart rhythm association ( hera ) [ 17 ] , evaluating clinical practice regarding cardio - oncologic patients , especially those with cieds planned for rt . 
this need , as mentioned before , is based on the increasing number of patients with cieds that require rt , as result of the aging of population , with a major incidence of cardiovascular and oncological diseases . it seems there is a lack of knowledge and clear recommendations regarding the safe management of cieds , and an increasing number of papers are dealing with this topic , mainly to give answers facing oncological patients treatments [ 13 ]  . 
maybe , also the low percentage of errors , documented in the past - published experiences , is a reason of the poor adherence to guideline or the lack of national policies . 
 the summary of the potential errors induced by the influence of ionizing radiation on cieds was derived from many studies , both invitro and invivo [ 1 , 14 , 18 , 19 ] , even if an unusual total dose and beam and a total in - field irradiation were used during invitro studies [ 12 , 19 ]  . 
the mechanisms of pm / icd malfunctions could be divided into three groups : ( a ) transient effects due to interference , manifesting during the irradiation only ; ( b ) reverting to backup settings ( reset ) , recoverable after reprogramming the device ; and ( c ) permanent damage to the device [ 18 ]  . 
modern cieds contain complementary metal oxide semiconductor ( cmos ) technology , which has the advantage of a higher reliability , lower power consumption and smaller size , which translates into higher comfort and safety for patients , but with the disadvantage of being more radiosensitive [ 20 ] , leading to electronhole pairs resulting in electric leakage and shortcuts [ 13 ]  . 
these events may occur in any part of the cied , but in general the leads are considered insensitive to radiation , even if one case of shock coil failure was reported [ 21 ]  . 
the first and official international guidelines for managing pm / icd patients undergoing rt were published in 1994 by the aapm [ 16 ] , followed by other recommendations [ 2226 ] , as well as national guidelines , consensus statements or position papers [ 13 , 20 , 27 , 28 ]  . 
the last published recommendations , coming from italy [ 14 ] and promoted also by airo , provided a complete description of the possible situations that clinicians have to face daily , to answer this need . some bullet points result from all of the studies conducted and from the most important recommendations and guidelines : beams energy ( possibly 6mv ) ; not direct irradiation of cieds ( out - field ) ; cumulative dose ( possibly < 2 gy ) ; dose rate ( possibly < 1 gy / min ) ; types of radiation used ( possibly no particle therapy ) ; cardiological patients history and cieds type [ 1 , 13 , 14 , 20 ]  . 
even in the other surveys , the management is different , maybe for the lack of a unique guideline or on the difference between devices recommendations [ 11 , 17 , 27 , 28 ]  . the results of this survey promoted by the young group of airo highlight the need to create safe and complete validated policies for management of patients with cieds undergoing a rt treatment . 
despite some limitations , such as the small sample size , the data collection conducted 1 3 334 la radiologia medica ( 2020 ) 125 : 329335 before the publication of italian recommendations [ 14 ] , the bias on self - reported measures , this survey was aimed mainly at investigating the italian radiation oncologists awareness and sensitivity with respect to this issue . 
most of them worked in academic centers , as in the hera survey [ 17 ]  . about 90% of survey responders were aware of the difference between pm and icd , and more than half knew the aapm guideline . 
this result is quite similar to the american survey made in 2004 yet [ 11 ] , while less awareness was found among spanish responders centers on a recent survey [ 27 ] ; gossman and colleagues showed that the median proportion of change in rt approach due to pm / icd was only 0.8% [ 15 ] ; the uk centers involved in the 2014 audit showed a more detailed knowledge of the problem , most of them relying on internal policies [ 28 ]  . 
this result is quite similar among the surveys previous published [ 11 , 27 , 28 ] , with a higher involving in the hera survey [ 17 ] and in the uk audit [ 27 ]  . probably , the awareness among physicians regarding the issue is one of the most important points ; in particular , radiation oncologists would refer the patient for cardiological evaluation , because it constitutes first step for correct patient risk stratification ( low - , intermediateor high - risk patients ) [ 1 , 13 , 14 , 20 ]  . 
after this evaluation , a close interaction between the specialists may be required , for a correct management of the patient , also based on the type of rt treatment needed . 
a close attention emerged from the survey in patients monitoring during the treatment and also after the end of rt , in particular in a dedicated electrophysiological service , that could indicate the right follow - up of these types of patients . 
even in the other surveys , the attention to patients monitoring is outlined , especially if the patient is stratified as a high - risk one , extremely accurate the evaluation of the errors and the clinical evaluation to be made [ 11 , 27 , 28 ]  . 
a task group evaluation , made up of cardiologist , radiation oncologist , pm / icd technologist , intensive care team and clinical physicist , is fundamental for patients risk stratification and follow - up . 
about this last topic , the patient point of view in a slender group of patients was investigated : they all pointed out a perception toward a more serious healthcare - related problems with respect to cied management issues compared to rt ; at the end , they all agreed that the treating radiation oncologist and cardiologist should together decide and propose the best individualized treatment [ 16 ]  . the correct managing of patients with cieds , before , during and after a rt treatment , was not expressed with a common behavior to be followed in none of the survey , even if an even increasing awareness on the problem has been reached . 
for this reason , also in italy , airo , with the collaboration of italian cardiological and medical phisycs associations ( aiac and aifm ) , promoted the elaborations of recommendations [ 14 ] , to better manage the pm / icd patients that have to face with rt treatments . conclusion the issue of administered rt treatments on patients with pm / icd is increasing , for the aging of population and the large incidence of cardiological and oncological diseases . 
 moreover , the possibility to administer a rt treatment could become crucial for the best care of oncological patients . this italian survey and the italian recommendations express a need to better define the sides of this matter , to give the best care in oncological patients with cardiological devices . 
the in - depth knowledge of manufacturer recommendations and also national guidelines / advices is of great importance for the managing of these patients , but there is a general lack of knowledge and agreement on this topic even because of the low incidence of the errors that occurred invivo . a larger prospective data collection could be helpful to better clarify this issue and could help physicians to choose the best strategy to cure and care oncological patients . author contributions all authors contributed to the study conception and design . 
this paper aims to retrospectively assess the efficacy and safety of superselective arterial embolization in patients with high - flow priapism . materials and methods from january 2008 to march 2017 , nine patients with high - flow priapism have been treated in a single center with embolization . 
the mean follow - up time after embolization was 24 months . results eleven procedures were performed in nine patients : two of them required a second treatment session because of recurrence after 12 weeks . 
restoration of erectile function was monitored by clinical and color doppler evaluation during follow - up . conclusions superselective embolization should be the procedure of choice in patients affected by high - flow priapism ; this technique appears to be successful in preserving erectile function . 
pansini 5 , 80131naples , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 288295 the typical clinical feature is a painless partial tumescence of the cavernous bodies with corpus spongiosum remaining flaccid and the capability to increase rigidity with sexual stimulation [ 3 ]  . on the other hand , low - flow priapism ( lfp ) is characterized by fully erected and painful penis , caused by venous outflow obstruction engorging the corpora cavernosa ; this condition results in hypoxia , acidosis , penile ischemia and fibrosis , leading to erectile dysfunction . while lfp should be considered an emergency and requires immediate resolution , hfp treatment can be slightly delayed because venous outflow is preserved and so stasis and ischemia are avoided [ 4 ] ; these patients present low risk for permanent complications , even though reduced potency has been reported in patients with untreated long - standing disease [ 5 ]  . the diagnosis of hfp is based on the medical history , clinical findings , blood gas analysis and color doppler ultrasonography ( cdus )  . arterial priapism can develop early after trauma or with a delay of several days ; this can be explained by spasm of the injured pudendal branch vessel or by occlusion of the forn artery by a clot [ 1 ]  . in some cases , open surgery may be an option with the ligation of the arterial fistula [ 4 ]  . 
alternative treatments , often unsuccessful , are watchful observation , intracavernosal injection of phenylephrine or methylene blue , external compression of the perineum and local ice application [ 1 ]  . transcatheter embolization of the lacerated arterial branch was first described by wear et al . 
approximately 200 cases have been reported in the literature , mostly as case reports . the aim of this paper is to report on a single - center experience of hfp management treated by arterial embolization . materials andmethods sample over a period of 9years , nine consecutive patients ( range 1263years ; mean age 33years ) with hfp underwent endovascular embolization ( table1 )  . 
significant penile and perineal trauma was reported in eight ( six due to sexual trauma , one due to bicycle saddle trauma and one due to gym barbell ) , while only one subject had no apparent underlying cause . at clinical evaluation , all patients had painless and incomplete persistent erection for more than 6h . 
initially , an observational management was conducted with external perineal compression and local ice application associated with pharmacological therapy in hope of leading vasospasm and thrombosis of the injured vessel ; in this series , no patients benefited from this treatment . 
therefore , after a multidisciplinary evaluation with urologists and vascular surgeons , a first - line table 1 patient characteristics patient etiology idiopathic trauma trauma trauma trauma trauma trauma trauma trauma cdus color doppler ultrasonography cdus findings number of procedures angiographic sign side lesion fistula evident from diagnostic catheter embolic agent fistula fistula fistula right bilateral bilateral fistula pseudoaneurysm + fistula right bilateral pseudoaneurysm + fistula fistula fistula fistula right bilateral left right 1st procedure : yes 2nd procedure : yes 1st procedure : no 2nd procedure : yes microcoils microcoils microcoils microcoils microcoils microcoils spongel 1 3 290 la radiologia medica ( 2020 ) 125 : 288295 embolization technique before the procedure , a written informed consent was obtained ; in the only case of pediatric patient , this was signed by both parents . procedures were performed in the two angiosuites of the department ( toshiba infinix i 8000c , siemens artis zee ) by five experienced interventional radiologists ( > 5years ) in the field of embolization . 
through a monolateral femoral access ( 5 fr ) , both internal iliac arteries were investigated with a selective diagnostic 5 - fr catheters : cobra tip was adopted for contralateral district , while simmons 1 or shepherd tip was chosen for the ipsilateral . 
after choosing the best projection , a road map was conducted to reach the lesions fed by pudendal vessels as close as possible , in order to spare healthy tissues and minimize the risk of nontarget embolization . 
a superselective transcatheter arterial embolization ( tae ) was performed in all cases by a 2.7fr microcatheter ( progreat , terumo , shibuya - ku , tokyo , japan )  . 
manual compression or closure devices ( femoseal or angioseal 6vip terumo japan ) were adopted to obtain hemostasis ; a compressive femoral patch was positioned for 24h with patients lying supine . the anesthetic protocol consisted of local anesthesia and all descriptive data analyses had been performed in an excel environment ( microsoft , usa )  . results technical success , considered as no further angiographic pathological findings at the end of the procedure , was obtained in all patients ( 100% )  . 
a second procedure was required in two patients ( 22% ) because of recurrence of hfp ( patient 3 after 5days from the first treatment , while patient 5 after 4days ) for a total of 11 embolization procedures . in five procedures ( 45% ) , vascular lesions were appreciable at diagnostic digital subtraction angiography ( dsa ) , fig . 
2 selective digital subtraction angiography ( dsa ) of the right internal pudenda artery ( black arrow ) in patient 9 shows a single small tear size ( black arrowhead ) ( a ) ; injection of contrast under fluoroscopic control performed with the distal tip of microcatheter ( white arrow ) very close to the fistula ( black arrowhead ) ( b ) , this patient was successfully embolized with spongel slurry fig . 
3 superselective angiography in patient 6 shows a large pseudoaneurysm ( white arrow ) of a branch vessel of the right internal pudenda artery ( a ) ; selective dsa of the pudenda artery after embolization with microcoils ( white arrowheads ) shows no further evidence of pseudoaneurysm with preserved patency of omolateral cavernous artery ( black arrow ) ( b ) while in the others the vascular anomalies were appreciable only at superselective angiography . 
in the remnant eight patients , the follow - up lasted 24months : they had successful detumescence with preserved sexual activity and early morning erection ; the overall clinical success rate at 1year was so 88% ( n = 8 )  . discussion hfp is associated with penile or perineal trauma resulting in the laceration of cavernous artery and unregulated arterial blood flow that oozes into the vascular lacuna spaces of the corpora cavernosas erectile tissue , bypassing protective high - resistance helicine arterioles [ 8 , 9 ]  . 
4 transversal duplex us of patient 3 after the first embolization shows left - sided fistula s patency with turbulent flow and high systolic peak the first embolization of the internal pudendal artery for treating priapism was performed by wear [ 6 ]  . 
 [ 3 ] , a multicenter study comparing treatment results among embolic agents in 27 patients and assessing that the type of embolo - therapy was not the major factor affecting the recurrence of priapis bertolotto etal . 
 [ 5 ] suggested that microcoils were a more reliable agent than spongel ; on the other hand , ozturk [ 11 ] preferred adsorbable temporary agent for treating bilateral lesions , advising the use of permanent embolic agents in case of recurrence . 
these papers reported a low rate of penile erectile dysfunction , mostly due to delayed embolo - therapy resulting in secondary development of penile fibrosis . cdus is an invaluable diagnostic tool ; indeed , in our series it had a nearly 100% sensitivity rate in detecting fistulas , with a result similar to other reports [ 1214 ]  . 
treatment options are mechanical ( sustained perineal compression achieves detumescence only if used in early phase ) , pharmacological ( intracavernous administration of - adrenergic agonists or methylene blue ) , surgical ( shunt surgery , ligation of the internal pudenda artery ) and radiological ( selective tae ) [ 3 , 12 ]  . 
however , an extended delay following a period of watchful waiting may result in secondary deformities of penile vascularization [ 4 ]  . in this series , no patients solved hfp with conservative management ; this seems to be in accordance with the literature data that describe poor outcome of this strategy ; therefore , superselective tae is considered the mainstay of treatment [ 1719 ]  . embolization has demonstrated several advantages , as a brief period of treatment , short course of recovery time and definite therapeutic effect [ 17 ]  . 
even if any pathological angiographic sign is not seen from the diagnostic catheter , it is necessary performing ultra - selective angiography of the pudendal artery to detect angiographic signs . 
most of the patients in this series were embolized with detachable microcoils to achieve a definitive result because fistulas / pseudoaneurysms were 1 3 la radiologia medica ( 2020 ) 125 : 288295 fig . 
5 transversal ( a ) and longitudinal ( b ) b - mode us of patient 5 after the second embolization shows a leftsided hyperechoic area ( white asterisk ) with no evidence of distended lacunar spaces ; transversal ( c ) and longitudinal ( d ) color doppler shows no fistula sign with preserved patency of the cavernous artery ( white arrow ) too large for liquid and particulate embolic agent ; it is of paramount importance to accurately position microcoils as close as possible to the target vessel . patients 4 and 8 showed at the preliminary angiographic study multiple , small caliper fistulas : in these cases , microparticles ( 300500m ) were preferred because of the ability to penetrate the microvascular network . 
microcatheter was placed very close to the lesion , and the injection was performed under fluoroscopy ; the injection was interrupted when the blood flow through the fistula markedly decreased , as bertolotto etal . 
6 ct axial image in patient 9 before treatment shows clustering contrast agent overflowed on the right side of penis ( white arrow ) , indicating cavernous artery disruption 1 3 294 la radiologia medica ( 2020 ) 125 : 288295 the choice of spongel in patient 9 was due to the small single tear size of the injured vessel ; in this case , the embolization technique was analogue to the previous performed with pva . 
particulate embolic injection should be performed with gentle pressure in order to avoid the proximal reflux and the unintentional peripheral embolization that can lead , especially with pva , to ischemia and infection , complications not observed in this series . patients 2 and 7 , after first side embolization , showed during the procedure massive contralateral fistulas feeders : for this reason , we chose to embolize both sides during the same session . in this series , the recurrence rate was 22% ( n = 2 ) which is similar to the literature data ( 040% at 6months ) [ 8 , 10 , 13 , 20 ]  . 
patients 3 and 5 , embolized at the first session with microcoils , had recurrence of hfp because of bilateral fistulas feeders : in these cases , we preferred to perform a second ultra - selective embolization with detachable microcoils because they are more reliable agents despite their greater risk of permanent vascular occlusion and to achieve a definitive embolization . 
patient 3 , after the second tae procedure , experienced permanent irreversible occlusion of the entire cavernous artery ; this event is described in the literature with preservation of erectile function as a result of blood inflow from the pudendal artery of the opposite side [ 20 ]  . 
however , he reported penis curvature of the injured vessel side : this might be related to the blocked vessel of penis which led to atrophy of penile albuginea [ 17 ]  . 
this patient was lost at follow - up . in restorating erectile capacity , our success rate at 1year ( n = 8 ; 88% ) was similar to other studies [ 16 ]  . bilateral lesions occurred more frequently ( n = 4 ; 44% ) than other reports [ 2 , 4 , 5 , 20 ]  . cdus after embolization may reveal fistula patency despite arteriographic evidence of occlusion . 
patency of non - obliterated collateral feeding vessels can explain this discrepancy [ 1 ]  . in this series , the cdus follow - up strategy was analogue to ciampalini [ 10 ] in which the postoperative evaluation included cdus at 1day , 1month and 6months after the procedure . 
our two recurrence cases were detected 24h after the first embolization . surgery reported higher rate of erectile dysfunction than tae [ 2123 ] and a wider range of possible complications : abscess , urethral injury and penile hematoma [ 24 ]  . 
however , shunting occurs when plsvc is associated with unroofed cs , or when it directly drains into the left atriuwith an increased use of ct and mri for chest and cardiac imaging , plsvc is being more encountered by radiologists than before . 
in this article , we will discuss the embryology of plsvc , its anatomic course and drainage pathways , as well as its clinical relevance and relation to congenital heart disease and viscero - atrial situs . keywords persistent left superior vena cava coronary sinus congenital heart disease introduction normally , the left brachiocephalic vein crosses to the right side to join the right brachiocephalic vein forming the superior vena cava ( svc ) on the right side . 
multislice computed tomography ( ct ) and magnetic resonance imaging ( mri ) allow direct visualization of the complete course of the plsvc and detection of any variations in its course or drainage . with an increased use of ct and mri for chest and cardiac imaging , this anomaly is being more encountered by radiologists than before . 
in this article , we will review the literature as well as our own experience with 56 pediatric patients diagnosed by ct or mri to have plsvc in a teaching university hospital . 
non - ionic iodinated contrast material ( iohexol , 350mg iodine / ml ; omnipaque , ge health care , ireland ) was injected intravenously with a dose of 0.52ml / kg at a rate of 12ml / s . 
identification of plsvc was possible in all patients irrespective of the route of contrast injection , whether through right arm , left arm or leg ; the artifact caused by the contrast medium did not hinder diagnosis , and optimal contrast opacification of plsvc was achieved in the delayed venous phase . cardiovascular mri was obtained using 1.5 - t scanner ( philips ingenia , best , netherlands )  . 
the anterior and posterior cardinal veins on the right and left sides join to form the right and left common cardinal veins that drain into the sinus venosus [ 7 , 8 ]  . 
the coronary sinus is formed by the left horn of the sinus venosus and adjacent part of left common cardinal vein [ 1 , 7 , 8 ]  . plsvc results from failure of regression of the left anterior cardinal and part of the left common cardinal veins [ 1 ]  . 
in the midsegment , the vessel lies anterior to the left hilum and then enters the pericardium in the posterior atrio - ventricular groove and traverses along the ligament of marshall to drain into the right atrium via a dilated coronary sinus [ 1 ] , fig.2. plsvc is usually asymptomatic , and it may be discovered incidentally on cross - sectional imaging . 
among our 56 patients , 12 ( 21% ) had a bridging vein the presence of a bridging vein , the plsvc is more commonly smaller in size than the rsvc [ 2 ]  . 
on ct and mri , it is important to report the presence and size of the bridging vein . coronary sinus dilatation the normal caliber of the cs has a wide range and may vary during the cardiac cycle . 
 on the other hand , there are little data on the ranges for cs caliber in children . in our experience with ct angiography in pediatric patients , we measure the caliber of the cs at 12cm proximal to the ostiua cs < 3mm is considered non - dilated . 
less commonly , the cs draining a plsvc may be nondilated when the lsvc is small and there is a large bridging vein , and thus , the diagnosis may be missed on echocardiography in cases with non - dilated cs . 
a dilated cs in 1 3 240 la radiologia medica ( 2020 ) 125 : 237246 association with plsvc is a potential cause of arrhythmias due to stretching of the av node [ 9 ]  . 
other causes of dilated coronary sinus include right ventricular failure , right atrial hypertension , severe pulmonary hypertension , tricuspid regurgitation , a coronary arteriovenous fistula draining into the coronary sinus and cardiac tamponade [ 12 ]  . persistent lsvc withabsentright svc rarely , there is a plsvc draining into the cs with absent right svc ( fig.3 ) , due to regression of the right anterior cardinal vein with persistent of the left one . 
in this case , the cs may be markedly dilated as it receives the whole venous drainage from the upper body [ 16 ]  . persistent lsvc inassociation withchd the incidence of plsvc increases in the presence of congenital heart diseases ( 3.3 to 10% ) [ 2 , 4 , 10 , 17 ]  . 
although several studies demonstrated strong association between plsvc and aortic coarctation [ 20 , 21 ] , in our experience only 3 out of 56 patients with plsvc in our cohort had coarctation ; conversely , the prevalence of plsvc in coarctation patients was 3 out of 96 patients . in children with chd , the presence of a plsvc may affect the choice of certain surgical procedures [ 22 ]  . 
the strategy of surgical cavo - pulmonary connections ( glenn shunts ) in children with chd differs completely if plsvc is present and associated with the presence or absence of bridging vein or right svc [ 22 ]  . 
on the other hand , left isomerism refers to bilateral morphologic left atria , polysplenia and bilateral bilobed lungs . plsvc is significantly more common in association with situs ambiguous than with situs solitus or inversus , up to 6070% [ 2 , 2426 ]  . 
3 persistent left superior vena cava ( lsvc ) with absent rsvc in a 4 - month - old girl with situs solitus , dextrocardia and multiple complex congenital cardiac defects . 
in right isomerism ( fig.7 ) , plsvc drains directly into the roof of the left - sided atrium , and the cs is often absent [ 26 ]  . 
in left isomerism , drainage can be either into the cs in 50% of patients or directly into the left - sided atrium [ 2 ]  . interrupted inferior vena cava ( ivc ) in patients with situs ambiguous , ivc interruption and azygos / hemiazygos continuation are much more commonly described in association with left than right isomerism [ 23 ]  . 
 the azygos vein drains into right svc , while hemiazygos vein either joins the azygos to drain into the right svc or drains into a plsvc . accurate delineation of this anomaly in cases with chd requiring cavo - pulmonary shunt procedures is important for surgical planning . 
accordingly , surgical connection of the svc to the pulmonary artery , known as the kawashima procedure , will create a total cavo - pulmonary shunt excluding only the hepatic veins [ 22 ] , fig.5. left superior vena cava insitus inversus in situs inversus totalis , the svc is located on the left side and drains into the left - sided morphologic right atriu fig . 
volume - rendered ct image showing left unilateral cavo - pulmonary ( glenn ) shunt in a 7 - year - old girl connecting the left superior vena cava ( lsvc ) to the left pulmonary artery with large bridging vein between the 2 svcs ( arrows )  . 
coronal ( a ) and axial ( b ) ct images showing bilateral glenn shunts in a 5 - year - old girl connecting the right and left superior venae cavae ( rsvc and lsvc ) to the corresponding right and left pulmonary arteries ( rpa and lpa )  . 
note the hemiazygos vein draining into the left svc in b 1 3 242 la radiologia medica ( 2020 ) 125 : 237246 table 1 drainage of persistent left superior vena cava in 56 patients according to the viscero - atrial situs viscero - atrial situs coronary sinus to right - sided atrium direct to leftsided atrium direct to left - sided atrium ( together with ivc ) coronary sinus to rightsided atrium ( absent right svc ) situs solitus n = 31a situs solitus with dextrocardia n = 1 situs inversus with levocardia n = 1 right isomerism n = 13b left isomerism n = 10c a 1 remaining patient with situs solitus had bilateral glenn shunts b 2 remaining patients with right isomerism had glenn shunts c 3 remaining patients with left isomerism had bilateral glenn or unilateral left glenn or kawashima shunts fig . 
in patients with trisomy 18 and 21 , plsvc persistent lsvc andblood shunting plsvc draining into the right atrium via the cs will not usually cause blood shunting between the right and the left sides . 
in cases with plsvc draining into the cs , the increased pressure may predispose to unroofing of the cs , with communication between the cs 1 3 la radiologia medica ( 2020 ) 125 : 237246 fig . 
7 persistent left superior vena cava ( lsvc ) draining into leftsided atrium in a 4 - month - old girl with right isomeris a , b coronal oblique and volume - rendered ct images showing right and left svcs ( rsvc and lsvc , respectively ) ; each drains directly into the ipsilateral atrium ( white and blue asterisks : rightand left - sided atria , respectively )  . 
the shunt direction depends on atrial pressure and is usually left to right , except if the cs ostium to the right atrium is atretic , then a right - to - left shunt develops [ 29 ]  . 
an associated coronary sinus - type atrial septal defect may also develop [ 2 ]  . plsvc draining directly into the la will commonly result in a right - to - left shunt , except when there is a large bridging vein that permits shunt reversal [ 2 ]  . 
drainage of plsvc directly into the left atrium , with associated cyanosis , requires surgical disconnection of plsvc from left atriuif the diameter of the briding vein was adequate , plsvc can be simply ligated . 
in the absence of bridging vein , the plsvc is divided and connected to right svc or right atrial appendage [ 22 ]  . 1 3 244 la radiologia medica ( 2020 ) 125 : 237246 tributaries andpitfalls left superior intercostal vein the left superior intercostal vein is a tributary of the plsvc in about 20% of cases with plsvc , fig.10b. 
this vein typically drains the 2nd to 4th posterior intercostal veins , and in 75% of the accessory hemiazygos vein as well , it then courses to the left of the aortic arch to drain into the left brachiocephalic vein or the plsvc [ 2 ]  . imaging pitfalls an important pitfall on cross - sectional imaging that may mimic a plsvc is partial anomalous pulmonary venous drainage of the left upper lobe , which appears on ct as an anomalous vertical vein connected to the left brachiocephalic vein and coursing in the mediastinum lateral to the aortic arch [ 2 , 30 ]  . 
however , usually its course can be followed on axial images where its inferior end merges with the left upper lobe pulmonary veins ( fig.10 ) , rather than caudally into the cs . 
ac axial consecutive steady - state free precession mr images delineate the course of the persistent lsvc draining into the right atrium through the coronary sinus ( cs )  . 
the anomalous vein ( asterisk ) drains the superior pulmonary vein into the left brachiocephalic vein ( lbcv ) and should be differentiated from a persistent left superior vena cava . 
a 2 - year - old girl with levoatrial cardinal vea , b axial ct images showing the course of the levoatrial cardinal vein ( arrow ) posterior to the left pulmonary artery ( lpa )  . 
c volume - rendered ct image showing the connection of the levoatrial cardinal vein ( arrow ) to the left brachiocephalic vein ( lbcv ) cranially and the left atrium ( la ) caudally funding this work received no funding or grants . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee ( including name of committee + reference number ) and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
ivim perfusion fraction ( f ) , pseudo - diffusion coefficient ( d * ) , true diffusion coefficient ( d ) and apparent diffusion coefficient ( adc ) as well area under the curve at 60s ( auc60 ) were calculated for bone marrow before and after gcsf administration . 
moreover , two different ivim parametric maps ( i.e. , adc and adclow ) were generated by selecting two different intervals of b values ( 01000 and 080 , respectively )  . 
all bone metastases were clearly differentiable from hyperplastic bone marrow on adclow maps , but not on adc maps and dce - mri . conclusion mr functional imaging techniques , such as dw - , ivim dwand dce - mri are effective tools in assessing the response of bone marrow to the administration of growth factors . 
martino , university ofmessina , via consolare valeria , 1 , 98100messina , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 280287 introduction dynamic contrast - enhanced ( dce ) and diffusion - weighted ( dw ) magnetic resonance imaging ( mri ) are techniques of large interest owing to their ability to provide information on blood supply and cellularity in both normal and neoplastic tissues . 
to separate the signal arising from a diffusion sequence , such as the stejskal and tanner sequence , into a vascular and a nonvascular component [ 5 , 6 ] , allowing to estimate tissue diffusivity and tissue perfusion without using contrast medium [ 5 , 7 ]  . ivim - based studies have shown that organs in the abdomen , including liver [ 810 ] , pancreas [ 11 ] and kidneys [ 12 ] , have relatively high fractional perfusion and pseudo - diffusion ( i.e. , fast component of diffusion ) values compared with other organs , such as the brain [ 13 , 14 ]  . on the other hand , data about dw imaging of normal bone marrow and its changes after administration of hematopoietic growth factors such as granulocyte colony - stimulating factor ( gcsf ) are limited [ 15 , 16 ] and , to date , no study exists evaluating ivim parameters in normal and hyperplastic bone marrow . 
informed consent was obtained from each patient before each examination . subjects in order to evaluate gcsf effect on bone marrow , we included in our study patients who had an mri examination of the pelvis both before and after administration of gcsf according to the following inclusion criteria : ( 1 ) an mri examination of the pelvis was performed for staging of rectal or uterine cancers , ( 2 ) a second pelvic mri examination was obtained after chemotherapy no more than 3months later , ( 3 ) the second mri examination was obtained between 4 and 20days after administration of gcsf , ( 4 ) no evidence of bone metastases during 1year follow - up . according to the above reported inclusion criteria , fourteen consecutive patients ( nine female , five male ; age range 4475years ; mean age 55years ) with locoregionally recurrent or locally advanced rectal or uterine cervix cancer were included . 
the second mri examination was performed after three chemotherapy courses ( using capecitabine and oxaliplatin in rectum cancer patients and fluorouracil , cisplatin and / or taxol in uterine cervix cancer patients ) and between 4 and 18days ( median 9days ) after administration of gcsf . 
the use of two b values lower than 50s / mm2 is mandatory to obtain reliable values of perfusion - sensitive ivim parameters [ 2325 ]  . dce examination was performed with a 3d spectral attenuated inversion recovery ( spair ) t1 - weighted highresolution isotropic volume examination ( e - thrive ) sequence using the following parameters : tr , 4.4ms ; te , 2.2ms ; flip angle , 10 ; matrix , 180 180 ; acquisition time , 46s . 
an automated power injector ( mallinckrodt , hazelwood , mo , usa ) was used to inject a bolus of 0.2ml of gadoteratemeglumine ( gadolinium concentration 0.5mol / l ) per kilogram of body weight through a catheter inserted into an antecubital vein at a rate of 3ml / s , followed by a 30 - ml saline at the same flow - rate . 
the sequence was started when half the contrast medium had been injected , performing 40 samples of the tissue . imaging postprocessing anddata analysis bone marrow intensity evaluation was performed by two radiologists working in consensus . 
each measure was performed on images obtained both before and after treatment with gcsf by using the same roi through a paste and copy tool and mean value was used to perform statistical analysis . 
to permit analysis of the images obtained at different time points , pre and post - treatment images were coregistered using spm8 toolbox coregister function by using full affine transformation with 12 degrees of freedom before rois were drawn . to examine the individual contributions to the apparent diffusion changes of true molecular diffusion and incoherent motion of water molecules in the capillary network , perfusion fraction ( f ) , perfusion - free diffusion coefficient ( d ) and pseudo - diffusion ( d * ) were estimated using a least - square nonlinear fitting in matlab ( mathworks , natick , ma ) by fitting the dw signal decay in the rois to the ivim bi - compartmental model as follows [ 5 , 26 ]  . 
the following equation was employed to express the relationship between signal intensities at b = 0 ( s0 ) and at each b value ( sb ) : sbso = ( 1 fslow ) exp ( bdfast ) + fslow exp ( bdslow ) where ( 1 f slow ) represents the perfusion fraction f , dslow the perfusion - free diffusion coefficient ( i.e. , slow component of diffusion ) d , and dfast is related to the pseudo - diffusion coefficient ( i.e. , fast component of diffusion ) d * as follows : dfast = d + d *  . 
 [ 23 ] by fitting all sb data through the mono - exponential law : sb = so exp ( b adc ) moreover , two different ivim parametric maps ( i.e. , adc and adclow ) were also generated by selecting two different intervals of b values ( 01000 and 080 , respectively ) [ 8 , 28 , 29 ] ( figs.1e , f , 2gi )  . dce - mri data were calculated using a semiquantitative method , analyzing the area under the curve over the first 60s ( auc60 ) [ 13 ]  . because of the small number of patients with bone metastases , only a qualitative analysis was performed ; evaluation of ivim dwand dce - mri parameters in these patients and comparison with hyperplastic bone marrow were not performed . 
two independent radiologists , using fast - stir and t1 - weighted mr images as references , visually analyzed adc maps , adclow maps and dce - mr images of patients with pelvic bone metastases who had received gcsf administration and defined the evidence of bone metastasis into four degrees as follows : ( 1 ) definitely not appreciable , ( 2 ) probably not appreciable , ( 3 ) probably appreciable and ( 4 ) definitely appreciable . statistical analysis continuous variables were expressed as mean ( sd )  . 
differences were considered significant if the p value was < 0.05. statistical analyses were performed by using spss , version 15 ( spss , inc . , chicago , usa ) software . results the data obtained from bone marrow and hyperplastic bone marrow ( i.e. , after gcsf administration ) are summarized in table1 . 
1 axial diffusion - weighted images ( b = 1000 ) of the left iliac bone marrow obtained before ( a ) and after ( b ) treatment with gcsf show an evident post - treatment increase in the signal , suggesting increased cellularity . 
axial images obtained during arterial phase of dynamic gadolinium enhanced examination before ( c ) and after ( d ) treatment with gcsf demonstrate an intense increase of enhancement of the hyperplastic bone marrow . 
axial t1 - weighted ( a ) and fast - stir ( b ) images through the left hip show a metastasis ( arrow ) which is masquerade by hyperplastic bone marrow ( asterisks ) after treatment with gcsf ( c , d )  . 
on axial images obtained during arterial phase of dynamic gadolinium enhanced examination , the metastasis ( arrow ) is well depicted before treatment with gcsf ( e ) , but is faintly distinguishable from hyperplastic bone marrow ( asterisks ) after treatment with gcsf ( f )  . 
the lesion ( arrow ) , which on adc image through femoral neck ( n ) , is easily visible before gcsf ( g ) but became isointense with respect to hyperplastic bone marrow ( arrowheads ) ( h ) , appears hypointense ( less vascularized ) in comparison with hyperplastic bone marrow ( arrowheads ) on the adclow map ( i ) stimulation . 
to our knowledge , this was not previously well established in other studies . gcsf has a broad impact on hematopoiesis , stimulating the development and maturation of committed stem cells to neutrophils , eosinophils and monocytes [ 30 ] and , consequently , causing an increase in bone marrow cellularity . 
as a result of the administration of gcsf , hyperplastic red marrow appears darker than normal on t1 - weighted scans and may have a slightly increased signal intensity on t2 - weighted and stir sequences . 
in healthy individuals , gcsf application leads to significant signal changes of bone marrow in lumbar vertebrae that are maximal about 2weeks after discontinuation of gcsf application [ 32 ]  . 
these findings can be confused with bone 1 3 la radiologia medica ( 2020 ) 125 : 280287 table 1 ivim mono - exponential quantitative parameter ( adc ) , ivim biexponential quantitative parameters ( d , d * and f ) and auc60 , of normal bone marrow before and after the administration of granulocyte colony - stimulating factor ( gcsf ) groups 1 . 
a similar phenomenon occurs also on pet scans because of increased metabolism of hyperplastic bone marrow [ 23 ]  . our data support the opinion that hyperplastic bone marrow can simulate bone metastases or can hide the presence of bone metastases not only on pet and morphological mri scans but also on dw imaging [ 15 , 1823 ] which has recently emerged as an effective method to detect and monitor skeletal metastases [ 16 ] among other mr - based approaches ( namely , chemical shift imaging , susceptibility weighted ( t2 * ) sequences and ultrashort echo time sequences ) [ 15 , 33 , 34 ]  . 
however , the use of adclow maps allows a reliable differentiation between hyperplastic bone marrow and breast cancer bone metastases . using b values 50 / 800900 , padhani found a significant difference between adc of normal red bone marrow ( mean value 675m2 / s ) and bone marrow involved by breast cancer metastases and myeloma ( mean value 920m2 / s ) and defined 774m2 / s as the optimal adc cutoff value for separating normal and malignant bone marrow . 
on the other hand , increased vascularization was responsible of strong increase of d * ( i.e. , pseudo - diffusion ) in hyperplastic bone marrow in comparison with normal bone marrow ; furthermore , pseudodiffusion of hyperplastic bone marrow was also higher than bone metastases one , as appreciable on adclow maps . 
consequently , d * could be a useful marker in distinguishing metastases from hyperplastic bone marrow . the main limitation of our study is the fairly small cohort of patients with bone metastases that does not allow us to define the utility of adclow maps in the distinction between hyperplastic bone marrow and metastases with adequate statistical power . 
however , our data suggest the advisability that studies including a larger group of patients should be performed to confirm our results . a second weakness could be the use of a semiquantitative parameter ( auc60 ) for the evaluation of dce - mri . 
 semiquantitative parameters may not accurately reflect contrast agent concentration in the tissue of interest and can be influenced by the contrast agent injection procedure and the scanner settings ( including pulse sequence , gain and scaling factors )  . 
on the other hand , auc60 has the advantage of being relatively straightforward to acquire , has been demonstrated to parallel parameters of vessel permeability obtained using more complex mathematical modeling [ 2 ] , is a relatively robust kinetic parameter being able to characterize all enhancing regions without the problems associated with model fitting failures ( namely in the case of highly vascularized regions , very poorly perfused regions or physiological motion ) [ 35 ] ; therefore , it has been recommended as a practical substitute for k - trans in clinical studies [ 36 ]  . moreover , the reproducibility of f and d * estimations may be considered low [ 37 ] ; however , we used two b values lower than 50mm2 / s , according to a study of cohen [ 24 ] who showed relatively high d * repeatability when dw sequence includes two very low b values . finally , absence of histological correlations represents a further drawback of our work . in conclusion , the main changes in the bone marrow after administration of growth factors are related not only to an increase in cellularity but also to an enhanced vascularization , as demonstrated by the increase in ivim perfusion parameters ( i.e. , d * and f ) and of auc60 . 
thus , mr functional imaging techniques , such as dw - , ivim dwand dce - mri , are effective tools in assessing the response of bone marrow to the administration of growth factors . 
degenerative changes were found in 74.1% of the patients with radiography made , more frequently at an older age , osteophytes in 49.5% and abnormal cervical lordosis in 37.1%. conclusions there are sociodemographic factors that influence in the request for cervical radiographs in patients with vertigo and dizziness . 
the diagnostic approach to vertigo and dizziness is complex , and there are few guidelines or consensus on the adequacy of request for radiological tests . the challenge of assessing and treating the patients with vertigo and dizziness is correctly identifying the etiology of their complaint , and the differential diagnosis is relatively broad . 
the primary etiology in a persistent and recurrent vertigo is a peripheral disorder ( the most frequent are benign paroxysmal positional vertigo or meniere disease , and there is a little role for imaging when the clinical diagnoses has been established ) ; a psychiatric diagnosis is also common ; central causes account for only 511% of cases [ 4 ]  . 
however , among its diagnostic criteria , pathological radiological findings are not found [ 5 ]  . one of the diagnoses of presumption that arises mostly , especially from pc , is cervical vertigo . 
brandt and bronstein [ 6 ] state that vertigo can be accompanied by cervical pain , associated with head injury , whiplash injury or cervical spine disease , and none of these instances provides convincing evidence of a cervical mechanisthey conclude that the cervicogenic cause is more of theoretical interest than on a practical relevance . 
in medicine , almost 50% of all high - tech imaging do not provide useful information and may be unnecessary [ 7 ]  . the purpose of this study is to determine the diagnosis yield of cervical radiographs of a population of patients with vertigo and dizziness . 
we aim to quantify the number of cervical radiographs in our sample , to analyze demographic and clinical characteristics of patients who have conducted the test and to describe the radiological findings . 
we also evaluate the magnetic resonance imaging ( mri ) and the computed tomography ( ct ) of the cervical spine present in the sample . patients andmethods study population this is a retrospective study of patients evaluated for vertigo and dizziness in the hospital between january 2011 and december 2012 . 
we included 493 referred patients ( from any specialty , including pc ) with the international classification of diseases ( icd - 9 - cm ) [ 8 ] codes : 386 ( vertiginous syndromes and other disorders of vestibular system ) and 780.4 ( dizziness and giddiness ) from 780 ( general symptoms )  . the department of health on which the study is carried out serves a capita population of 153 , 526 . 
the main demographic characteristics are : increase in the population in summer period with 600 , 000 inhabitants , an aging population ( 26% over 65years old ) and an important immigrant population ( 55% are foreigners )  . lateral andanteroposterior cervical radiography we differentiate the sample into two groups : with and without cervical radiography . 
we selected the radiographs taken during a period of 5years before and after the consultation due to vertigo ( 20072017 )  . from each group , we studied demographic variables ( sex , age and country of birth ) and clinical variables ( psychiatric / psychological pathology , emergency assistance due to vertigo , other imaging tests made and hospital discharge )  . from each radiography , we studied applicant specialty , presence of degenerative changes , osteophytes , hypolordosis , misalignment , congenital defects or signs of fracture . 
 two radiologists reviewed the radiographs and determined the presence of the radiological findings . other cervical imaging test we quantified other cervical spine imaging tests made between 2007 and 2017 on the patient sample : ct and mri . 
we studied demographic and clinical variables , and described the findings from the radiology report . statistical analysis qualitative information is presented in frequencies and percentages , and quantitative information as mean and standard deviation . 
difference of frequencies in groups was determined with the chi - square test , comparison of groups with metric variables was made with analysis of variance ( anova )  . 
there was a statistically significant association between having cervical radiography and female sex , being a spanish person , having psychiatric pathology and frequenting emergency department ( ed ) because of vertigo . there was a total of 409 radiographs made in 281 patients , with an average of 1.46 radiographs per patient in this group and 0.83 in the total sample . 
there was a statistically significant relationship between having more than one x - ray made and being a spanish person , having psychiatric / psychological pathology and having frequented the ed because of vertigo . in two patients , it was not possible to access the images for their review . 
simple radiography is a cheap and easily accessible test , but it is not always indispensable and illuminating , and it is not risk free . on the other hand , the group of patients with radiography has a higher number of cervical ct and mri made . 
the cervical radiography would be a pretest before a ct or mri , more expensive tests , but that provide more accurate information on bone and neural structures of the neck . radiological tests are useful when their result helps to modify a diagnostic or therapeutic behavior , so those tests that offer irrelevant data for patient care should be avoided [ 10 ]  . 
less than 10% of patients with radiography were assessed by rehabilitation , and did not present a clear radiological pattern of referral to the department . factors influencing patients with vertigo to have a cervical radiograph are being a woman , being a spanish person , presenting psychiatric pathology and having gone to ed for the symptoas in other publications [ 11 ] , our study shows that radiography is requested more often in women . 
according to a study about unnecessary radiology in pc [ 10 ] , in 15.2% of the tests requested , the doctor felt pressured by the patient to ask for it . 
we have also detected that there are more repeated radiographs in spanish patients , with psychiatric pathology and in those who have gone to the ed because of vertigo . pc and ed requested most of the studies , 56 and 24% , respectively . 
there may also be pressure or insistence by the patient or relatives , who often go there with the expectation that those tests will be made immediately . in approximately one third of patients , a cervical radiograph was performed for the study of vertigo and dizziness . 
 according to a systematic review about vestibular disease in pc settings [ 12 ] , the pc physician might want to exclude potential life - threatening diseases by imaging . the most frequent findings on cervical radiographs were degenerative changes , which are more severe in older patients . 
nevertheless , degenerative changes in the cervical spine are common in asymptomatic individuals ; disk degeneration was found in nearly 60% and foraminal narrowing in 20% of individuals older than 40years old . 
the abnormal mri of the cervical spine in asymptomatic individuals emphasizes the dangers of predicating operative decisions on diagnostic tests without precisely matching those findings with clinical signs and symptoms [ 13 ]  . 
patients who do not present trauma , tumor or progressive neurologic deficit are best treated with a short course of conservative care before cervical spine advance imaging studies are obtained [ 14 ]  . 
even in the presence of cervical pain , if there are no red flags , imaging tests are not recommended [ 15 ] , neither in conscious patients and without pain after trauma [ 9 ]  . according to our results , radiological findings are similar on radiographs requested by vertigo and those requested for another reason . 
brandt [ 16 ] says that if this entity exists , it is obviously characterized by ataxia and unsteadiness of gait , and not by a clear rotational or linear vertigo . 
neurological , vestibular and psychosomatic disorders must first be excluded before dizziness , and unsteadiness in cervical pain syndromes can be attributed to a cervical origit has not been convincingly demonstrated that whiplash injuries or cervical pain syndromes produce such a tone imbalance with ataxia and vertigo . 
hain classified cervicogenic causes of vertigo in impingement of the vertebral arteries in the neck , whiplash - associated disorder and degenerative cervical disorders , and did not mention specifically radiographies as a test to establish a cause for cervicogenic vertigo [ 17 ]  . 
 in a review of imaging in dizziness , the section of cervical structures mentions the decrease in vertebral or basilar artery blood flow on doppler ultrasound in cervical spondylosis , but it is not confirmed ; they also doubt about the relation with impingement on neural structures , saying that osteophytes on plain radiography or ct in the dizzy patient will not certainly prove a causative relationship and may make clinicians not consider other significant causes [ 4 ]  . 
neither of the two mechanisms advocated for cervical vertigo ( abnormal sensory input from neck proprioceptors and vascular compression of the vertebral artery ) can be recognized on cervical x - ray [ 21 ]  . as an article about spine radiography in the evaluation of back and neck pain concludes [ 22 ] , a cause of the request can be the limited experience of resident physicians , who may have a lower threshold to order radiographs to minimize potential for missing diagnosis . 
other factors such as 1 3 278 la radiologia medica ( 2020 ) 125 : 272279 defensive medicine , social pressure or the possible placebo effect of the radiography may also influence . 
it is accepted among the population that imaging techniques are necessary for adequate and complete care , so in specific situations and with certain patients , unnecessary x - rays can also be cost - effective , avoiding second consultations in patients not satisfied with the attention received [ 9 ]  . 
nevertheless , the neck study , as with neuroimaging [ 25 ] , in the majority of cases diagnostic imaging procedures such fail to identify the cause of dizziness . limitations andstrengths ofthestudy this is a single - institution study and the extrapolation of our findings would require multicenter studies . 
we work with a sample of patients assessed by any specialist , and the study is not based by department protocols . conclusions our results indicate that cervical radiograph for the study of vertigo and dizziness has a low diagnostic yield . 
a correct assessment of the patient based on the best scientific evidence and an adequacy in the request for imaging tests , could reduce the exposure of patients to radiation , avoiding unnecessary treatments ( the result of incidentalomas ) and reducing costs , among other benefits . health professionals should avoid being influenced by non - clinical factors ( legal , psychological , pressure from patients ) when radiological tests are required in the diagnostic process . the study of vertigo and dizziness should be based on anamnesis and a thorough clinical examination . 
according to the proportion of solid / micropapillary components , the patients were classified into three groups : solid / micropapillary - negative ( smpn ) ( n = 258 ) , solid / micropapillary - minor ( smpm ; > 5% not predominant ) ( n = 158 ) and solid / micropapillary - predominant ( smpp ; > 5% most dominant ) ( n = 90 )  . 
241 west huaihai road , shanghai200030 , china institute formedical imaging technology , school ofbiomedical engineering , shanghai jiao tong university , shanghai200030 , china lung adenocarcinoma is the most common histologic subtype of lung cancer , accounting for more than 40% of lung cancer incidence . 
in order to better guide the management of lung adenocarcinoma patients , a histopathologic classification criteria of lung adenocarcinoma was introduced by a multidisciplinary group in 2011 [ 1 ]  . 
this classification system for the invasive type was mainly based on the six major histologic patterns ( lepidic , acinar , papillary , solid , micropapillary and rare variants ) and suggested using the term predominant to be appended to all categories of invasive adenocarcinoma . 
at present , patients with a predominantly solid / micropapillary pattern have been proved to have a relatively poor prognosis compared to those with other patterns [ 25 ] and more lymph node metastasis [ 68 ]  . however , most of lung invasive adenocarcinomas consist of mixtures of the histologic patterns . 
actually , recent studies have found that patients with micropapillary and / or solid patterns have a poorer prognosis and more lymph node metastasis even if their patterns are not predominant [ 912 ]  . 
based on the 2011 lung adenocarcinoma classification system , a previous study has found that micropapillary predominant and solid predominant adenocarcinoma had higher suvmax than other subtypes using pet / ct , reflecting malignant grade of the tumor and prognosis [ 14 ]  . 
the other two parameters might also shed light on the characteristics of the minor components of solid / micropapillary pattern subtype lung invasive adenocarcinomas . we hypothesized that solid / micropapillary lung invasive adenocarcinoma , predominant or minor , would have higher pet / ct parameters and have a close correlation with lymph node metastasis . 
therefore , the aim of this study is to investigate the pet / ct findings characteristics of lung invasive adenocarcinomas according to the proportions of solid / micropapillary component and investigate the association with lymph node metastasis . materials andmethods patients this retrospective study was approved by the institutional review board of shanghai chest hospital with a waiver of informed consent . 
between february 2016 and january 2019 , a total of 506 lung invasive adenocarcinoma ( 3cm ) patients who underwent a pet / ct examination and resection surgery with pathologic n 0 , 1 , 2 status were included . 
after fasting for 6h with the blood glucose < 7.8mmol / l , patients were intravenously injected with 18f - fdg in a dose of 0.100.15mci / kg according to body weight . 
furthermore , we added a thin - slice scanning of the lung at breath hold with a slice thickness of 1.0mm. pet / ct parameters measurement two nuclear medicine physicians with 15years of experience in chest nuclear medicine , who were blinded to the pathological diagnosis , evaluated the pet / ct images . 
suvmax , mtv and tlg for suspicious primary lung invasive adenocarcinoma were automatically calculated after delineation of the outline of the lung adenocarcinoma lesion in the pet / ct images . 
and the whole tumor size was represented by the maximum diameter of the whole tumor [ 16 ]  . pathological diagnosis resected lung adenocarcinoma specimens were reviewed by two experienced pathologists to determine the 1 3 la radiologia medica ( 2020 ) 125 : 257264 adenocarcinoma subtype according to the 2011 lung adenocarcinoma classification criteria . 
according to the proportion of solid / micropapillary components in the resected specimen , the patients were classified into three groups : solid / micropapillary - negative ( smpn ) ( n = 258 ) , solid / micropapillary - minor ( smpm ; > 5% but not predominant ) ( n = 158 ) and solid / micropapillary - predominant ( smpp ; > 5% and the most dominant ) ( n = 90 )  . 
typical images are shown in figs.1 , 2 and 3 . statistical analysis statistical tests were performed using the statistical package for social sciences ( ibm corp , armonk , ny , usa ) software for windows version 20.0. 
group difference in clinical demographics and pet / ct findings between smpn group , smpm group and smpp group was compared by one - way anova for continuous variables or chi - square test for categorical variables . 
d pet maximum - intensity - projection image shows significant fdg uptake in the left hilar lymph node metastasis which was confirmed after surgery patient pathological types andpet / ct analysis table1 shows the pathological types of the study patients according to 2011 lung adenocarcinoma classification systein the smpn group , the most common pathological type was acinar predominant type , followed by papillary predominant type and leptic predominant type . 
in the 1 3 260 la radiologia medica ( 2020 ) 125 : 257264 comparisons inclinical characteristics andpet / ct findings betweensmpn group , smpm group andsmpp group table 3 shows the clinical and pet / ct findings in the three group patients . 
furthermore , the lymph node metastasis group had higher cea , suvmax , mtv , tlg , solid proportion size , whole tumor size and more pleural invasion ( p < 0.001 ) than lymph node metastasis negative group ( table4 )  . 
consistent with our hypothesis , our study found that lung invasive adenocarcinoma with minor components of micropapillary or solid contents had higher suvmax , tlg , smpn n = 258 smpm n = 158 smpp n = 90 leptic predominant mucinous predominant acinar predominant papillary predominant solid predominant micropapillary predominant smpn solid / micropapillary - negative ; smpm solid / micropapillary - minor ; smpp solid / micropapillary - predominant fig . 
d pet maximum - intensity - projection image shows no significant fdg uptake in the lymph node which was confirmed after surgery smpp group , solid predominant type was more common than micropapillary predominant type . the optimal suv value for measuring the pet / ct parameters was firstly determined by roc analysis . 
the optimal suv value for measuring the pet / ct parameters in our study is at a threshold of 2.5 in suv , which was consistent with frequently used cutoff [ 18 ]  . 
 this was reasonable , as mtv indicates the volume of a metabolically active tumor , reflecting the whole tumor burden , while the suvmax reflected only the local changes [ 18 ]  . consistent with our hypothesis , the solid / micropapillary subtype lung invasive adenocarcinomas , predominant or minor , had higher pet / ct parameters . 
analyzing the underlying causes , it might be solid / micropapillary pathological type lung adenocarcinoma had specific pathological contents that could lead higher pet parameters and bigger solid proportion size . 
the smpn solid / micropapillary - negative ; smpm solid / micropapillaryminor ; smpp solid / micropapillary - predominant more pleural invasion in the smpp group and smpm group indicated more invasiveness of smpp and smpm pathological type . 
to be 1 3 la radiologia medica ( 2020 ) 125 : 257264 noted , as the pathological type had collinearity with pet / ct findings , we only analyzed the pathological types and clinical factors . 
future studies are warranted to further investigate the lymph node dissection strategy and prognosis of lung adenocarcinoma with minor components of micropapillary or solid contents . our study had some limitations . 
future prospective large sample size study was needed to further confirm our conclusion . in conclusion , lung invasive adenocarcinoma with micropapillary or solid contents had higher suvmax , tlg , mtv , and tumor size and was associated with lymph node metastasis , even if they were not predominant . 
we estimated the reproducibility of bsi in healthy women with different body mass index . methods we enrolled postmenopausal women ( mean age sd : 66 10years ) divided into three groups ( a , b and c ) according to body mass index ( bmi : < 25 ; 2529.9 ; 30kg / m2 ) and two groups ( d and e ) according to waist circumference ( wc : 88 ; > 88cm ) , each of 30 subjects . 
bmd is measured by means of dual - energy x - ray absorptiometry ( dxa ) and is expressed as the ratio of mineral content on area ( g / cm2 )  . 
however , there is an overlap between bmd distribution of patients with and without osteoporotic fractures [ 3 ] , suggesting that other factors play a role in the determination of bone strength . 
 among these , trabecular bone score ( tbs ) is a dxaderived gray - level bone texture parameter based on an experimental variogram of two - dimensional projection images , which provides indirect information about bone microarchitecture , and can help in predicting fracture risk [ 4 ]  . however , the density of a material and its texture do not completely explain its resistance to load . 
the distribution of the strain is defined as the spatial deformation of every single element in which the vertebra was divided before the calculation [ 6 ] , and a good correlation was found between bsi and the yield strain applied to porcine vertebrae , meaning that bsi can be a predictor of elastic and plastic changes in the mechanical response of the bone [ 5 ]  . 
applied to dxa scan of human vertebrae , bsi showed a correlation with t - score in patients presenting a t - score lower than 3.0 , with high values of bsi [ 5 ]  . 
recent clinical studies found a usefulness of bsi in identifying the osteoporotic patients subgroup particularly prone to fragility fractures [ 7 ] and characterizing young patients affected by secondary osteoporosis [ 8 , 9 ]  . a recent paper reported the invitro bsi reproducibility , which appeared worse than that of bmd , but scarcely influenced by fat mass thickness [ 10 ]  . 
the la radiologia medica ( 2020 ) 125 : 313318 present study investigated the invivo coefficient of variation and least significant change of bsi according to the international society for clinical densitometry ( iscd ) guidelines [ 11 ]  . patients andmethods this prospective study was conducted in a single center . 
 according to iscd adult official positions , ad hoc ethical committee approval was not required , as this study was part of the periodic dxa precision assessment in the setting of good clinical practice protocols . 
all patients signed an authorization for the anonymized data publication . postmenopausal women were consecutively enrolled from those who routinely performed a dxa scan for osteoporosis evaluation at our radiology department from march to june 2018 . 
if patients had no previous examinations , the high - definition modality was chosen for group c and group e , as this modality provides a better definition in obese subjects . 
for the second scan analysis , the computer suggested an automatic segmentation of the lumbar spine based on the first scan , and the operator checked the correctness of this analysis . 
bsi calculation was automatically performed on dxa dicom data using bone strain index software version 1.0.0 provided by tecnologie avanzate , avoiding further operator actions . statistical analysis the normal distribution of data was evaluated using the shapirowilk test . 
 the precision error was calculated according to the instructions of iscd official positions [ 11 ] , similarly to previous 1 3 la radiologia medica ( 2020 ) 125 : 313318 studies [ 14 ]  . 
the reproducibility of bmd and bsi was obtained as the complement to 100% of lsc% . firstly , we compared the bmd values of the two repeated scans for each scan mode , and no significant differences were found . 
comparisons were made using the one - way analysis of variance ( anova ) with tukeys post hoc test for bmi groups . we tested the bmd and bsi reproducibility by comparing their sd distributions . 
the levene test showed variance inhomogeneity for bmi groups ; thus , the welch anova with gameshowell post hoc test was used to compare bmd and bsi precision of bmi groups . 
for the remaining comparisons the classic anova was used . all calculations were performed using both excel electronic database ( microsoft excel 2010 , redmond , wa , usa ) and spss v24 ( spss inc . , chicago , il , usa )  . 
bsi reproducibility was slightly lower in group e ( 91.8% ) compared to group d ( 93.6% ) , but once again this difference was not significant ( p = 0.083 ) ( see table 3 )  . 
in fact , even when bmd is in the normal range , the occurrence of one or more lowimpact fragility fractures is considered as a sign of severe osteoporosis [ 17 ]  . 
for that reason , when assessing fracture risk , data other than bmd are taken into account , such as age , history of previous or parental fractures , the presence of diseases inducing secondary osteoporosis , corticosteroid therapy . 
these factors are accounted for by frax , which 1 3 la radiologia medica ( 2020 ) 125 : 313318 is a computer - based algorithm that estimates individual 10 - year fracture probability [ 18 ]  . 
since the emerging of this not only to bmd - related vision , research has proposed other dxa - derived parameters as indexes of fragility fracture risk , independently from bmd , exempli gratia the well - known tbs [ 19 , 20 ]  . 
while the cited well - indagated index is based on the fractal mathematical analysis , this new research line is addressed to a different analysis approach , namely finite element analysis , whose clinical application has to be validated . 
we have found that bsi absolute values proportionally increase with bmi , and this is statistically significant in those obese patients group with respect to both overweight and normal weight groups . 
the increase appears particularly evident in the obese patients , but this fact is not simply due to the fat mass , because two factors have to be considered : the first is that bsi is not influenced by fat , as indicated in a recent invitro study , where bsi did not change with the increase in fat superimposed on the phantom [ 10 ]  . 
 secondly , being bsi sensible to the weight of the patient , as it results from the mathematical formulation [ 5 ] , bsi correlates the weight of the subject with the increase in the stress of the vertebra and consequently with its resistance to the load . 
another possible factor to be considered could be the influence of the muscle - bone unit in case of overweight on vertebral stress [ 21 ]  . as regards bsi reproducibility , it significantly worsened with the increase in bmi only in the obese patients and in those with the higher abdominal circumference . 
in patients with high bmi the fat superimposed to the bone causes a worsening of the image quality , and therefore , the recognition of the vertebral silhouette in every scan , automatically executed by the software of the bone densitometer , is less precise . 
1 dxa images of one patient belonging to group c showing scan inaccuracies in recognizing the shape of the vertebrae ( on the left ) and resulting bone strain distribution ( on the right ) reproducibility of bsi compared with that of bmd represents a vulnus in the usefulness of this parameter in detecting small variations over time , limiting the clinicians in the follow - up of a disease , namely osteoporosis , that shows little variations of the bone mass over time and small increases after pharmacological treatment , with respect to what they can obtain using bmd measurements . this scenario has been already observed in the use of other bone quality parameters , suggesting that the use of dxa - derived indexes of bone structure and strain is intrinsically limited with respect to the use of bone quantity parameters in the diseases follow - up [ 22 , 23 ]  . 
moreover , another item worthwhile to be investigated is the utility of bsi in the prediction of fragility fracture risk . authors contribution cm has executed densitometric scans , performed statistical analysis and contributed to the writing of the text . 
the engineer lr , former working in politecnico of turin and now employed by the commercial company : technologic s.r.l , has extracted and tabulated the densitometric data and has applied the mathematical algorithms based on the finite element analysis to calculate the bone strain index . 
messina c , piodi lp , rinaudo l , emili i , porro f ( 2019 ) bone strain index reproducibility and soft tissue thickness influence : a dual x - ray photon absorptiometry phantom study . 
schousboe jt , shepherd ja , bilezikian jp , baim s ( 2013 ) executive summary of the 2013 international society for clinical densitometry position development conference on bone densitometry . 
geneva waist circumference and waist - hip ratio ( 2010 ) report compliance with ethical standards conflict of interest all the authors do not have conflict of interest . ethical standards all performed procedures were conducted on humans in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments . 
nevertheless , european collective dose encountered an average increase of 23% , which resulted from a growing tendency for implementation of high - dose procedures such as ct scans and interventional examinations . 
 the advances in technology have led to a growing trend in the population exposure resulting from the invention of high - dose procedures such as ct scans and interventional methods . 
undoubtedly , the benefits of these procedures in symptomatic patients outweigh their risks , but it should be noted that the collective dose due to unjustified scans is as high as one - third of the total number of examinations [ 7 , 8 ]  . although the risk induced by radiological examinations is small at the individual level , the projected risk to a large exposed population may trigger significant health issues that will not be evident for years [ 9 ]  . 
for instance , it is estimated that approximately 1.2% of cancers in norway are caused by vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 296305 radiological examinations and 2% of cancers in the usa are induced by ct scans annually [ 1013 ]  . the international commission of radiological protection ( icrp ) has categorized the effects of ionizing radiation into two classes including stochastic and deterministic effects . 
the dose in typical radiological examinations is not high enough to produce the deterministic effects ; thus , the main concern emanates from some stochastic effects such as cancer incidence and heritability anomalies . 
this quantity has been defined as a homogenous dose when the body is exposed to it ; the same biological effects are formed as the locally absorbed doses [ 14 , 15 ]  . european commission ( ec ) launched projects to provide information pertinent to medical exposures in 2004 and 2011 . 
although considerable attempts have been made to address the patients doses due to radio - graphical examinations after the last ec report , less attention has been exercised to the trends and their causes [ 1618 ]  . 
 154 and 180 were reviewed , and the frequency and dose trends for each radiological examination in european countries were discussed [ 19 , 20 ]  . effective dose , the weighted average was calculated for each procedure by multiplying each effective dose by its assigned frequency and divided by the total number of examinations . the spss ( version 16 , spss inc . , chicago , il ) was used to statistically analyze the data . 
 a probability value of less than 0.05 was considered to be significant . for a representative population , the severity of the disease concerning mortality and years of life lost is taken into consideration to determine the detriment - adjusted nominal risk coefficient from sexand age - at exposure - averaged lifetime risk coefficients . 
in icrp 103 , the risk was being considered as 5.5% per sv for carcinogenesis [ 15 ]  . results methods european commission radiation protection ( rp ) reports no . 
154 [ 19 ] and 180 [ 20 ] published the effective dose and the frequency of top 20 examination types that were supposed to present major contribution to the total population exposure in europe ; they have been classified into four categories : plain radiography , fluoroscopy , interventional and computed tomography ( ct ) , as shown in table1 . 
selected countries in rp 154 report include belgium , denmark , france , germany , luxembourg , netherlands , norway , sweden , switzerland , and the united kingdothe data out of these countries were extracted from the reports , and the average variation trend of the number of examinations and effective doses for the groups were studied . 
the results revealed intravenous urography and ct trunk bearing the lowest ( 70% ) and highest ( 206.2% ) frequency , respectively . furthermore , table2 represents the weighted average of effective dose for the 20 procedures . 
the most significant rise ( 109.2% ) and fall ( 49.9% ) of the effective dose per examination were observed in chest / thorax and ct spine , respectively . plain radiography table 1 classification of radiological examinations obtained from european commission reports plain radiography computed tomography fluoroscopy chest / thorax cervical spine thoracic spine lumbar spine mammography abdomen pelvis and hip ct head ct neck ct chest ct spine ct abdomen ct pelvis ct trunk ba meal ba enema ba follow - thorough cardiac angiography interventional ptca despite the growth in mammography utilization ( 11.9% ) , there has been a decrease in the mean frequency of the rest of plain radiography examinations . 
these variations in frequency and effective dose per examination have been schematically illustrated in fig.1. figure2 illustrates the four mentioned classifications ( plain radiography , ct , fluoroscopy , and interventional ) and their portion in the total number of examinations and collective dose , plotted using rp 180 data . 
as it is evident , the contribution of ct scans in the total number of examinations is considered as less than one - fourth , even though they consist of more than 70% of the population collective dose . the annual excess radiation - induced cancer incidence per 100 , 000 of the populations in the european countries noted earlier has been illustrated in table3 . 
according to the results , the excess radiation - induced cancer incidence has been increased by 23% , while the excess ct - induced cancer incidence has been increased by 86% . 1 3 la radiologia medica ( 2020 ) 125 : 296305 fig . 
the increase in ct scans could be attributed to its superior image quality and thus its higher diagnostic sensitivity and accuracy in diagnosis compared to conventional imaging [ 21 ]  . 
consequently , the fundamental reason for decreasing the plain radiology frequencies has been the growth of cross - sectional imaging modalities like mri and ct scan [ 4 , 22 ]  . in contrast with the rest of plain radiography examinations , the mammography frequency has undergone a growing trend of 12% . 
 for instance , in the united kingdom , the widening of the age range invited for screening has resulted in a growth in the number of these examinations [ 2 ]  . the descending trend in plain radiography dose ( 14% on average ) has stemmed from advances in technology and the introduction of digital imaging , owing to higher detective quantum efficiency ( dqe ) of digital radiography compared to film - screen and computed radiography systems . 
digital systems have been more beneficiary compared to film - screen techniques such as wide contrast dynamic range , post - processing functionality , multiple image viewing options , availability of electronic transfers , and archiving . 
furthermore , most of the digital systems are capable of recording and assessing desired parameters used to estimate patient dose so that even slight changes in patient exposure would be detectable and resolvable [ 26 ]  . nowadays , national and international protocols have restricted manufacturers for utilizing the filters at least equivalent to 2.5mm thick aluminuthe beam hardening by absorption of low energy photons due to the increasing filtration has contributed to the patient dose reduction [ 24 , 27 ]  . 
furthermore , the impact of quality control programs should not be neglected as well [ 24 , 26 , 27 ]  . it should be noted that digital systems are like a doubleedged sword ; in this sense , there is a possibility of dose increscent despite dose reduction . 
however , in the case of digital radiography ( dr ) systems , several reports state that overexposure up to 500 times which is greater than the appropriate dose has no discernible effect on the image quality . 
hence , it gives us the impression that radiologists training is essential after dr device installation [ 25 , 26 , 28 , 29 ]  . as mentioned earlier , dr utilization has been the leading cause of dose reduction in plain radiography scans , including mammography . 
in mammography , dr systems have provided an opportunity for using different target / filter 1 3 la radiologia medica ( 2020 ) 125 : 296305 combinations , thus decreasing the patient dose caused by beam hardening [ 30 ]  . 
for instance , implementation of w / rh combination , instead of mo / mo in dr systems , reduces patient dose up to 57% as reported by ranger etal . 
in spite of decreasing trend in mammography dose , in some countries such as the united kingdom ( uk ) , the mean effective dose has been raised as a result of increased number of projections in screenings . 
furthermore , according to investigations in uk , breast enlargements due to prevalence of obesity can be another cause of patient dose increscent [ 30 , 3234 ]  . fluoroscopy trend there has been over 50% decrease in barium tests originated by the development of innovative methods such as colonoscopy , flexible sigmoidoscopy , computed tomography colonography , and transnasal esophagoscopy , and their implementation as a preliminary method for diagnosis [ 3539 ]  . 
 [ 41 ] have attributed this growth , though being small , to the technology advances , increased angiography centers , and lowered threshold of invasive managements ( patients referral to angiography without electrocardiography )  . 
features like noninvasive potentiality , ability to multiple viewing and reconstruction techniques , and minimal sedation , particularly in pediatrics can be regarded as their benefits [ 4244 ]  . 
 consequently , a considerable decrease in the utilization of invasive angiography can be expected for the years to come . due to the invention of modern procedures such as unenhanced helical computed tomography , contrast - enhanced magnetic resonance urography , and endoscopy , intravenous urography ( ivu ) implementation has undergone a 70% decrease [ 45 , 46 ] ; a change in guidelines has contributed to these replacements [ 47 ]  . 
for instance , since 2016 , the european association of urology ( eau ) has recommended ct urography as a diagnostic tool mainly for hematuria patients [ 45 ]  . despite the gd - magnetic resonance urography ( gdmru ) priorities such as ionization radiation - free , which have proved higher sensitivity in diagnosis , and projected superior spatial resolution compared with ivu , they have not been used broadly due to lack of mri centers in some places and their high expenses [ 48 ]  . 
several investigators have predicted significant growth in the utilization of gd - mru due to the universality of radiation protection programs and multiplicity of mri centers . according to united nations scientific committee on the effects of atomic radiation ( unscear ) publication in 2008 [ 3 ] , the prohibition of direct fluoroscopy without using intensifying screens is regarded as the most practical reason for patients dose reduction ( 67% on average )  . 
digital systems have had the main impact on dose trend in barium examinations , in a way that better image quality has made the diagnosis uncomplicated , hence reducing the examination time and patients dose . 
moreover , the increasing impact of radiation hazards awareness , radiation protection , and quality control programs are the factors that cannot be overlooked . as it was mentioned earlier , digital systems are like a double - edged sword . 
in digital fluoroscopy , radiologists can take multiple images of the patient during fluoroscopy , with no need to change the film ; this has contributed to the increasing probability of absorbed dose by the patients [ 25 ]  . interventional trend percutaneous transluminal coronary angioplasty ( ptca ) is the only interventional procedure reported , which indicates an increasing trend in its application by more than 80% . 
 unscear 2008 has stated that digital imaging with better quality and additional features such as last image hold or road mapping facilities has resulted in the advancement of this modality and its more extensive use . 
resultantly , for all of these advantages , there has been a growing demand for these methods in comparison to surgical techniques . in interventional tests , the patient dose depends on varying factors , including interventionalist , clinical protocol , and the equipment . 
in this study , any substantial changes in dose per examination for ptca could not be observed . 1 3 302 la radiologia medica ( 2020 ) 125 : 296305 computed tomography trend the population growth cannot be considered as the leading cause of increasing demands for ct scans . 
as the radiological scans frequencies increased up to 200% , the surveyed countries have encountered a population growth to an average of 3% ( based on rp 154 and 180 reports )  . 
ct examinations are now used more widely ; the reasons for this can be attributed to as follows : ( 1 ) increase in applications such as ct angiography ; ( 2 ) improvement of ct potentials including reduced imaging time , increased spatial resolution and contrast , etc . 
 [ 49 , 50 ] ; ( 3 ) referring a patient for a ct study to obtain the correct diagnosis rather than to keep the patient for an extended period of observation [ 49 , 50 ] ; ( 4 ) more availability of ct facilities [ 49 ] ; and ( 5 ) , ct implementation for screening purposes [ 6 ]  . ct has been physicians primary choice to avoid malpractice suits due to superior diagnostic value of computed tomography . 
this is alarming because these low but real risks in large scales have the potential to lead to critical problems in the future , including carcinogenesis and heritable issues [ 79 , 51 , 52 ]  . ct dose has been affected by several factors including the number of scans , tube current , rotation time , patient size , axial scan range , pitch factor , tube voltage , and the specific design of the scanner . 
consequently , there can be a wide range for effective doses even in a particular examination , impressed by setting parameters [ 6 , 53 ]  . in the case of the patient dose resulting from ct scans , the slight observed increase ( 3.5% on average ) may be attributed to the spread of multi - section ct since ct scans would deliver more radiation dose to the patient compared to single - slice scanners , ranging from 65% to 187% higher organ dose , as indicated by thornton etal . 
current commercial techniques such as the use of tube current modulation , automatic tube potential selection as well as new image reconstruction algorithms ( e.g. , iterative reconstruction , noise reduction , etc . ) in multi - detector scanners have decreased the patient dose ; this is observable in the trends of head and chest ct scans ( table2 ) [ 4 , 53 , 55 ]  . nowadays , the regulations , clinical organizations , and manufacturers have directed their efforts to reduce the patient dose from ct scans to under 1 millisievert . 
for this reason , several technical and strategical advancements ( e.g. , compressed sensing , volume of interest and interior tomography techniques , and photon - counting detectors ) have been made , in addition to those mentioned earlier , taking advantage of which can evolve the computed tomography toward submillisievert scans . 
by keeping this in mind , an ongoing trend in patient dose from ct scans is expected for the foreseeable future . patient hazards the risks associated with the diagnostic use of x - rays are mostly confined to stochastic effects . 
according to the linear no - threshold ( lnt ) risk model and the collective dose concept mentioned by the icrp , the use of radiation may cause assured disadvantages for the aforementioned population [ 39 ]  . 
through these studies ( rp 154 and rp 180 ) , the number of induced cancers related to the radiological procedures has been increased by 23% , which has unsurprisingly been due to ct frequency raise ( table3 )  . basic principles of radiological protection include justification , optimization , and dose limitations or constraints . 
if the number of unjustified ct scans is considered as one - third of the total , approximately it stands for more than 20% of the european annual collective dose which should not be neglected . furthermore , it is noteworthy to address the procedures with no substantial significant changes in radiation dose such as ct trunk which is one of the high - dose scans . 
for these examinations , efforts on medical radiation protection should be made , such as those presented by bonn call - for - action [ 58 ] , to reduce the patient dose as much as possible . conclusion the increasing use of ionization radiations in medicine , especially in ct , has resulted in a raise in population collective dose , thus leading to an increase in radiation carcinogenesis as well as genetic abnormalities . 
technological advances and the increasing importance of audit procedures , as well as publics growing awareness of radiation risks , have all contributed to the utmost dose reduction in patients . 
 as is illustrated , the number of examinations is increasing linearly ( = 0.988 , p < 0.001 ) ( cid : 7 ) ( cid : 7 ) r = 0.9758 2003 2004 2005 2006 2007 2008 2010 2011 2012 2013 2014 2015 2009 year belgium latvia denmark lithuania hungary luxembourg iceland slovak republic tomography fails to comprise the most substantial part of the total number of radiological examinations , it contributes to the majority of population collective dose that may sometimes be unnecessary . 
inter - scanner reproducibility of t2 measurements was 36% in the tm and 85% in the tfcc , respectively . conclusion the assessment of t2 relaxation time measurements of the cartilage of the tm and the tfcc seems to be feasible and reproducible , although the inter - scanner reproducibility of t2 measurements of the tm is suboptimal . 
specifically , the trapeziometacarpal ( tm ) joint is the most affected by degenerative osteoarthritis even in relatively young patients , with pain affecting activities of daily life [ 1 ]  . 
 on the other hand , the triangular fibrocartilage complex ( tfcc ) is a quite complex anatomical area , which can be affected by traumatic conditionsespecially in younger subjectsor by degenerative processes [ 2 ]  . the diagnosis of tm osteoarthritis is quite straightforward using plain films , which , however , become positive when cartilage has already almost disappeared , and ultrasound can be used to detect joint effusion and minimal osteophytes , but is not able to evaluate the intra - articular part of the joint [ 3 ]  . 
magnetic resonance imaging ( mri ) with conventional pulse allows thorough qualitative evaluation of cartilage [ 4 , 5 ] , although early detection of joint damage may be missed . 
in this setting , conventional mri , computed tomography arthrography , and direct and indirect mr arthrography have been used with variable diagnostic performances and the drawback of needing contrast injection for better results . t2 mapping technique enables to detect early changes in mr relaxation properties of the articular cartilage [ 7 ] and soft tissues [ 8 ]  . 
 cartilage degeneration involves a decrease in water content and modifications in collagen fibre orientation of the extracellular matrix , leading to the increase in transverse relaxation time ( t2 ) measurements [ 9 ]  . 
moreover , there are no published articles on the potential application of t2 mapping of the tm joint cartilage . the rationale of our study is that the thin joint cartilage of the tfcc and tm joint could be difficult to outline on mr images , especially at 1.5 t , thus leading us to perform a feasibility study on these topics . the purpose of our work was to assess the feasibility and reproducibility of t2 relaxation time measurements of the tfcc and tm cartilage at 1.5 t on healthy subjects . materials andmethods subjects institutional review board approval was obtained for this study , and the informed consent was obtained from all individual participants included in the study . we prospectively performed mr of the wrist joints on healthy volunteers , from october 2017 to february 2018 . 
the multiecho sequence parameters were : number of echoes : 10 ; echo time : 10 , 20 , 30 , 40 , 50 , 60 , 70 , 80 , 90 and 100ms ; echo train length : 10ms ; repetition time : 2000ms ; field of view : 120 120mm ; slice thickness : 3mm ; slice gap : 0.33mm ; number of slices : 13 ; pixel bandwidth : 180hz ; flip angle : 180 ; number of averages : 1 ; and acquisition matrix : 192 192 . 
the two observers manually drew the regions of interest ( rois ) on the coregistered sequences to include the cartilage of both the tm joint and 1 3 308 la radiologia medica ( 2020 ) 125 : 306312 tfcc of each volunteer with olea sphere 3.0 software ( olea medical , la ciotat , france )  . 
1 coronal t2 - weighted image a of a 30 - year - old male healthy subject shows a normal appearance of the tm cartilage ( black arrow ) with no erosions or defects . 
2 intra - observer reproducibility of t2 relaxation time measurements of r1 of the tm joint inter - observer reproducibility in the tm was 76% ( coefficient of repeatability = 6.2 ; bias = 0.95 ; p = 0.06 ) graphical representation of blandaltman analysis is reported in figs.2 , 3 and 4 . 1 3 la radiologia medica ( 2020 ) 125 : 306312 fig . 
however , the authors did not investigate the t2 relaxation time values of the tfcc . to our knowledge , only one recent study investigated the feasibility of t2 mapping of the ulnocarpal disc at 3t [ 12 ]  . 
 t2 measurement was based on a three - dimensional gre sequence with 5 different echo times ( 2 , 4 , 8 , 16 and 32ms , respectively )  . 
our acquisition time was similar to that reported on 3 t protocol of rausher etal . , but our sequence included 10 different echoes to increase the accuracy of the measurements . 
 furthermore , our study is the first which has investigated the inter - scanner reproducibility of the t2 mapping of the tfcc ( 85% )  . tm osteoarthritis is the most common degenerative condition of the hand for which patients often seek medical treatment [ 18 ]  . 
the high prevalence of osteoarthritis of this joint combined with its biomechanical duality has long challenged orthopaedists to better understand the biomechanical basis of its movement [ 19 ]  . 
however , radiographic findings of tm osteoarthritis are evident only in the late phase of the disease . to our knowledge , this is the first paper testing the feasibility of t2 mapping on the tm . 
the analysis of t2 relaxation time values of the tm cartilage seems to be feasible at 1.5 t with good intraand inter - observer reproducibility equal to 76% and 71% , respectively . 
8 inter - observer reproducibility of t2 relaxation time measurements of the tfcc joints discussion our main finding is that the calculation of t2 relaxation time values of the cartilage of the tm and tfcc is feasible , although the inter - scanner reproducibility of t2 measurements of the tm seems to be suboptimal . the cartilage damage of the tfcc and tm in the daily practice is evaluated with only qualitative analysis . 
the palmer classification is generally used in the assessment of the tfcc injuries and is divided in two different groups : 1 , traumatic lesions and 2 , degenerative lesions [ 13 ]  . 
the outerbridge classification system adapted to mr imaging has been widely used in cartilage evaluation of the knee [ 14 ] , but its application on the wrist has been limited by the thinness of the joint cartilage . 
this could help clinicians to identify those patients who could be treated earlier with oral or infiltrative procedures like the use of hyaluronic acid which promotes decreased joint pain after few weeks [ 21 , 22 ]  . a recent study claims that t2 relaxation times decrease over time after intra - articular administration of hyaluronic acid by comparing treated patients with untreated control group and also that lower t2 relaxation times show direct correlation with the reduction in the clinical symptoms ( 19 )  . some limitations should be pointed out . 
first , intraand inter - observer reproducibility of our measurements relies on the ability to accurately draw the rois and clearly on the contrast and spatial resolution of mr images . 
then , only healthy volunteers were involved , since one of our purposes was also to assess the normal t2 values of both tfcc and tm at 1.5 t , which have been scarcely investigated in previous works . 
secondary endpoint was to compare laryngeal cartilage invasion between primary and recurrent tumours . methods pre - treatment ct of 40 patients who had undergone total laryngectomy was retrospectively evaluated and compared with histology . 
sclerosis and erosion of arytenoid and cricoid cartilages were assessed as signs of neoplastic invasion . results ct erosion showed perfect agreement for thyroid inner cortex and cricoid cartilage invasion and almost perfect agreement ( 87% ) for arytenoid cartilage invasion . 
for primary tumours , ct demonstrated good ( inner cortex 75% ; full - thickness 85% ) , substantial ( 67.5% ) , and perfect ( 100% ) accuracy in thyroid , arytenoid , and cricoid cartilage invasion , respectively . 
no ct differences were observed between primary and recurrent laryngeal tumours . conclusion tumour - like tissue extension in the extra - laryngeal soft tissues was accurate in predicting thyroid cartilage full - thickness invasion . 
no ct difference in cartilage infiltration between primary and recurrent tumours was observed . keywords head and neck imaging computed tomography laryngeal cancer tumour staging introduction laryngeal carcinoma can be treated with both non - surgical and surgical treatment options , such as total laryngectomy , partial laryngectomy , and co2 laser - assisted or roboticassisted transoral resection [ 1 ]  . 
 on the other hand , potentially organ - preserving treatment may still be performed in case of focal cartilage thyroid invasion without full - thickness extension ( t3 ) [ 68 , 1012 ]  . 
 the latest guidelines of the american society of clinical oncology state that patients with t4a tumour have better prognosis when treated with total laryngectomy than with a radio - chemotherapy combination [ 2 ]  . 
an accurate assessment of laryngeal cartilage invasion is key to making the best treatment choice in laryngeal carcinomas [ 13 , 14 ] , since it has both prognostic and therapeutic values [ 15 ]  . 
magnetic resonance imaging ( mri ) has greater diagnostic accuracy than computed tomography ( ct ) in identifying a laryngeal cartilage involvement and tumour extension in superficial soft tissues of the neck [ 16 ]  . 
however , patients with vol . : ( 0123456789 ) 1 3 1302 la radiologia medica ( 2020 ) 125 : 13011310 advanced - stage laryngeal carcinoma ( t3t4 ) often access emergency rooms complaining of significant obstructive respiratory distress [ 17 , 18 ] and need to undergo an urgent imaging technique [ 19 ]  . 
moreover , few papers exclusively take into account advanced laryngeal carcinomas [ 16 , 2527 ] , and only one explicitly includes recurrences after radio - chemotherapy [ 27 ]  . 
the aim of this retrospective study was to evaluate the diagnostic accuracy of ct in the preoperative assessment of thyroid , arytenoid , and cricoid cartilage infiltration in patients with primary and post - radio - chemotherapy recurrent advanced - stage laryngeal carcinoma . 
secondary endpoint was to investigate any differences in infiltrations of thyroid , arytenoid , and cricoid cartilages between primary and recurrence tumours . materials andmethods inclusion andexclusion criteria between january 2016 and march 2019 , 113 patients with primary and post - radio - chemotherapy laryngeal carcinoma were assessed . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
post - processing , 1 - mm - thick sections were obtained on axial , sagittal , and coronal planes oriented on the glottic plane . all ct studies were independently reviewed by two radiologists with 13 and 5years of experience in head and neck imaging , respectively . 
according to the viii edition of the american joint committee on cancer tnm staging system , erosion of the inner cortex and full - thickness infiltration of thyroid cartilage were staged as ct3 and ct4 , respectively . 
the neoplastic invasion of arytenoid ( fig.3 ) and cricoid ( fig.4 ) cartilages was defined as the presence of areas of sclerosis or cartilage erosion in contact with the tumour tissue . 1 3 la radiologia medica ( 2020 ) 125 : 13011310 1303 fig . 
axial macrosections ( 34 - mm slice thickness ) of laryngectomy specimens were used to study endolaryngeal spaces to enable better identification of the anatomical structures and their relationship with the tumours [ 31 ]  . 
the presence of multiple foci , the dissociated tumour cells , and infiltration patterns of thyroid cartilage invasion were also recorded according to the system proposed by brandwein - gensler etal . 
all statistical analyses were performed with graphpad prism 7.0 ( graphpad software , inc . , san diego , ca )  . 1 3 1304 la radiologia medica ( 2020 ) 125 : 13011310 fig . 
a , b neoplasm invades left anterior ( white arrow ) and posterior ( white striped arrow ) paraglottic space , with no contact with the inner thyroidcartilage cortex surface ( white striped arrow in b ) ; these findings are suggestive for the absence of cartilage invasion . 
d presence of tissue with tumour - like post - contrast density inside the thyroid cartilage ( white striped arrow ) with interruption of the external cartilage cortex , without extra - laryngeal extension , suggestive for full - thickness thyroid cartilage infiltration ( confirmed by histology ) fig . 
c focal erosion surrounded by sclerosis of the cricoid cartilage ( white arrow ) adjacent to the subglottic neoplastic tissue , which is highly predictive for neoplastic infiltration ( confirmed by histology ) 1 3 la radiologia medica ( 2020 ) 125 : 13011310 1305 fig . 
4 axial computed tomography ( ct ) post - contrast scan at the glottic level showing swelling of the true right vocal cord ( white arrow ) extended to the anterior commissure with no contralateral extension . 
the histological examination shows no thyroid or right arytenoid ( white striped arrow ) cartilage invasion results sensitivity , specificity , positive predictive value , negative predictive value , diagnostic accuracy , and cohen kappa coefficient of preoperative ct in detecting laryngeal cartilage infiltration are reported in table1 . 
in the evaluation of thyroid cartilage , inner cortex erosion and full - thickness infiltration were found in 18 ( 45.0% ) and 11 cases ( 27.5% ) through ct and 28 ( 70.0% ) and 9 ( 22.5% ) cases through histological examination , respectively ( table2 )  . 
in histology , the site of erosion of the thyroid cartilage was in the anterior half of the cartilage in 26 cases and in the posterior half in two cases . 
sclerosis or erosion of arytenoid cartilage was identified on ct in 16 cases ( 40.0% ) , but in only six cases ( 15.0% ) did the histological examination prove any real involvement ( table3 )  . 
nevertheless , no statistically significant difference in invasion of thyroid , arytenoid , and cricoid cartilages between primary and recurrent post - radio - chemotherapy laryngeal cancers was observed ( table4 )  . 
roc curve of cricoid cartilage invasion is not shown since ct diagnostic accuracy was 100% in identifying cricoid invasion table 2 true positives , false positives , true negatives , and false negatives for computed tomography prediction of thyroid cartilage invasion in relation to histological examination thyroid cartilage histology total invaded not invaded discussion positive negative total positive negative total 18 ( 45.0% ) 10 ( 25.0% ) 28 ( 70.0% ) 0 ( 0% ) 12 ( 30.0% ) 12 ( 30.0% ) table 3 true positives , false positives , true negatives , and false negatives for computed tomography prediction of arytenoid cartilage invasion in relation to histological examination arytenoid cartilage histology total invaded not invaded 5 ( 12.5% ) 2 ( 5.0% ) 7 ( 17.5% ) 11 ( 27.5% ) 22 ( 55.0% ) 33 ( 82.5% ) erosion of the inner cortex of thyroid cartilage and tumour extension in the extra - laryngeal soft tissue on ct showed perfect agreement with the results of histological examination in detecting ct3 and ct4 stages , respectively . 
a perfect agreement between ct and histological examination was also found for the cricoid cartilage . erosion of inner cortex of thyroid cartilage on ct was found to be a highly predictive sign of tumour infiltration , especially when associated with adjacent cartilage sclerosis . 
nevertheless , the absence of erosion of the inner cortex on ct did not exclude focal cartilage infiltration found in histological examination for tumours in contact with the thyroid cartilage . 
in the current study , ct underestimated the invasion of the inner cortex in 25.0% of patients without determining tumour downstaging , according to the tnm classification ( ct3pt3 )  . 
neoplastic invasion of the inner cortex increased the difficulty of surgical radicality during transoral resections , but may not have had an impact on the overall survival of patients [ 33 ]  . tumour extension in the extra - laryngeal soft tissues on ct showed perfect correlation with histology in predicting full - thickness infiltration of the thyroid cartilage . 
difficulties in defining full - thickness thyroid cartilage infiltration on ct could be explained by the fact that ossified cartilage commonly shows high - attenuating outer and inner cortices and a central low - attenuating medullary space , whereas fibroelastic and non - ossified hyaline cartilages have ct attenuation values similar to soft [ 34 ] and neoplastic tissues [ 28 ]  . 
moreover , ossified cartilage is much more susceptible to tumour invasion than non - ossified cartilage due to the tumour angiogenetic factor and acquired development of blood supply [ 29 ]  . 
therefore , in the absence of extra - laryngeal neoplastic tissue , even with the use of contrast medium , it is hard to differentiate the ct density of neoplastic tissues from normal thyroid cartilage , especially if the cartilage is non - ossified [ 28 ]  . 
on the other hand , contrast - enhanced ct scans are of little help when laryngeal carcinoma shows minimal signs of erosion or density similar to the cartilage tissue [ 4 ]  . sclerosis of arytenoid cartilages on ct showed a little correlation with histological examination , with a high number of false positives ( 27.5% ) in which neoplastic infiltration was absent . 
unlike sclerosis , erosion of arytenoid cartilages showed good correlation with histological examination of tumour invasion in the current study , with only two false positives ( 5% )  . 
one of these two cases was related to a partial - volume artefact that mimicked a cartilage erosion , while the other one was an arytenoid radiation - induced necrosis . 
the most specific sign of this type of necrosis is the presence of bubbles in the soft tissues surrounding the eroded portion of cartilage [ 39 ] , although we did not find such features in our cases . the relevant differences found in the current study between ct and histological examination on thyroid , arytenoid , and cricoid cartilages could be partly explained by the differences in their ossification processes [ 40 ]  . 
except for the epiglottis and arytenoid cartilage vocal process , the remaining laryngeal cartilages are made up by hyaline fibrocartilage and undergo a gradual process of enchondral ossification , which begins in the third decade of life . 
the cricoid cartilage ossifies early and homogeneously , while the thyroid cartilage ossifies in variable and inhomogeneous ways , with areas of non - ossified hyaline cartilage mixed with mineralisation spots [ 35 ]  . in the current study , no statistically significant difference was found in the diagnostic accuracy of ct in predicting cartilage invasion between primary laryngeal cancers and tumour recurrences . 
it therefore follows that patients with laryngeal tumour recurrence are at high risk of thyroid cartilage invasion . some papers evaluated the diagnostic accuracy of ct in predicting cartilage infiltration in laryngeal carcinoma ; their results are comparable to our study [ 16 , 2329 ]  . 
ct : computed tomography ; rt : radiotherapy ; ppv : positive predictive value ; npv : negative predictive value ; * : current study laryngeal carcinoma , a proper staging tumour should avoid total laryngectomy in favour of an organ - preserving protocol with radio - chemotherapy treatment . 
 [ 27 ] , the probability of arytenoid cartilage infiltration is proportional to the clinical ( endoscopic ) degree of vocal cord motion impairment ; in the case of preserved mobility , an infiltration of the arytenoid cartilage should be excluded . 
 the absence of arytenoid cartilage infiltration does not change the surgical indication in t4 laryngeal tumours ; nevertheless , it can be useful to preserve the crico - arytenoid unit by performing an open partial laryngectomy instead of a total laryngectomy [ 41 , 42 ]  . some authors evaluate the diagnostic accuracy of new ct applications in the pre - treatment staging of advanced laryngeal cancers . 
 [ 26 ] demonstrated that dynamic contrast - enhanced perfusion - weighted imaging does not show better results than conventional contrastenhanced ct in the identification of cartilage neoplastic infiltration in t3 and t4 laryngeal carcinomas . 
 [ 5 ] observed that the dual - energy ct technique has a higher specificity than mri for assessing all laryngeal cartilages . it is well known that mri has greater diagnostic accuracy than ct in the identification of neoplastic infiltration of laryngeal cartilages , especially the thyroid cartilage [ 43 , 44 ]  . 
therefore , total laryngectomy may be the only available therapy in the setting of advanced primary and recurrent laryngeal carcinoma , which means that discrepancies of diagnostic accuracy between mri and ct in detecting cartilage invasion could lose their relevance [ 17 , 18 ]  . 
a practical algorithm for ct assessment of advanced - stage laryngeal carcinoma is presented in fig.6. the main weakness of our study was that the clinical value of the discrepancy between ct and histological examination has not been fully addressed . 
another limitation was the relatively low sample size of our study in order to give a definitive opinion on the role of ct in the evaluation of neoplastic laryngeal cartilage invasion . 
in our opinion , mri should be used as problem solving in collaborating patients . conclusion ct findings of tumour extension in the extra - laryngeal soft tissues and erosions of arytenoid , cricoid , and thyroid cartilages inner cortex show a strong correlation with 1 3 la radiologia medica ( 2020 ) 125 : 13011310 1309 histological examination in predicting neoplastic infiltrations . 
despite the higher incidence of histological multiple tumour foci of dissociated neoplastic cells in post - radiochemotherapy recurrences compared to primary laryngeal carcinomas , no significant difference was observed in thyroid , arytenoid , and cricoid cartilage infiltration between primary and recurrent tumours . acknowledgement the authors have no financial affiliation ( employment , direct payment , stock holdings , retainers , consultantships , patent licensing arrangements , or honoraria ) or involvement with any commercial organization with direct financial interest in the subject or materials discussed in this manuscript , nor have any such arrangements existed in the past 3 years . compliance with ethical standards conflict of interest the authors deny any conflicts of interest related to this study . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
they were divided into two groups on the basis of therapeutic response : the significant response ( sr ) group , which contains complete response patients and partial response patients , and nonsignificant response ( non - sr ) group , which contains progressive diseases and stable diseases . 
clinical characteristics , dce - mri parameters ( ktrans , kep , ve ) , and adc values before nact were analyzed and compared between the two groups . results sr group and non - sr group were documented in 35 and 28 patients . 
 however , radiotherapy can cause severe side effects , such as myelosuppression , ureterohydronephrosis , lymphedema , symptomatic vaginal stenosis , proctitis , and cystitis , especially for young people , and it may also cause ovarian dysfunction [ 47 ]  . 
it has been reported that the rate of effectiveness for nact is approximately 70% [ 8 , 9 ] , and vol . : ( 0123456789 ) 1 3 1234 la radiologia medica ( 2020 ) 125 : 12331242 thus , how to choose effective candidates for the appropriate treatment is especially important . there are no effective methods , such as age , histology , or tumor differentiation , to predict the effect of nact on cervical cancer before treatment [ 10 ]  . 
previous studies have reported that tumor volume reduction during therapy [ 11 ] , apparent diffusion coefficient ( adc ) values [ 12 , 13 ] , and perfusion - related parameters [ 1416 ] were used to predict the effect of rt and ccrt on cervical carcinoma . 
some studies indicated that adc values were useful for predicting the therapeutic response for locally advanced cervical cancer [ 13 ] , while others concluded that they were useless [ 12 , 19 ]  . 
1 flowchart of the study design 1 3 la radiologia medica ( 2020 ) 125 : 12331242 1235 response , we used the change of maximum length before and after nact . the objective of this retrospective research was to explore the value of histogram analysis of dce - mri parameters and adc values before treatment in predicting the effect of nact for cervical cancers . materials andmethods patients our institutional review committee approved this retrospective study and waived the informed consent requirement . 
the inclusion criteria were : ( a ) patients with pathologically confirmed cervical cancer who underwent conventional mri , diffusionweighted imaging ( dwi ) , and dce - mri examinations before nact ; ( b ) no obvious enlarged lymph nodes were found on pelvic mri before therapy ; ( c ) clinically confirmed stage ib2iia2 cervical cancer ( international federation of gynecology and obstetrics ( figo ) 2018 ) [ 21 , 22 ] ; ( d ) patients with complete clinical and pathological information ; and ( e ) all of the patients completed the same nact therapy after pelvic mri examination ( consisting of three cycles of nact using paclitaxel ( 175mg / m2 ) and nedaplatin ( 80mg / m2 ) with a time interval of 58days ) and followup with conventional mri examinations . 
based on the above criteria , 63 patients were finally included in the investigation . evaluation ofthenact effect in our study , two experienced radiologists with 5 and 8years of experience in pelvic mri appraised the tumor with the largest diameter on axial and sagittal t2wi to obtain a consensus . 
tumor therapeutic responses were defined as follows : complete response ( cr , all target lesions disappeared ) , partial response ( pr , the total diameters of target lesions decreased by at least 30% ) , progressive disease ( pd , the total diameters of target lesions increase by at least 20% ) , and stable disease ( sd , neither sufficiently decrease to qualify for pr nor sufficient increase to qualify for pd )  . 
gddiethylenetriaminepenta - acetic acid ( gd - dtpa ; magnevist , bayer , berlin , germany ) was injected by an automated injector system ( stellant mr injection system , medrad , germany ) at the dose of 0.1mmol / kg with a flow rate of 3ml / s , followed by a 20ml saline flush with the same rate . 
the examination time for patients was approximately 30min . image analysis all of the dce - mri data and dwi data ( dicom format ) were processed with omnikinetics software ( ge healthcare , shanghai , china ) and firevoxel software ( cai2r ; new york university , ny , usa ) , respectively . 
after roi determination , histograms of dce - mri parameters and adc values were derived , which were used to automatically generate the following parameters : the transfer constant of contrast from plasma to tissue extracellular extravascular space [ ees ] ( ktrans ) , volume of ees space per unit tissue volume ( ve ) , rate constant between ees and blood plasma ( kep ) , apparent diffusion coefficient ( adc ) values , and the mean , maximum , minimum , 10th , 50th , and 90th percentiles of their values . 
disagreements were settled through consultation , and a third radiologist with more than 10years of experience in pelvic mri was consulted if necessary . statistical analysis statistical packages ( pasw statistics 21.0 spss inc , chicago , il , usa ) were used to perform the analyses . 
to evaluate the diagnostic performance of all values in predicting the nact effect , receiver operating characteristic ( roc ) analysis was performed , the area under the roc curve ( auc ) was calculated , and aucs were compared using nonparametric methods . 
there were seven ( 11.1% ) patients with stage ib2 , 15 ( 23.8% ) patients with stage ib3 , 18 ( 28.6% ) with stage iia1 , and 23 ( 36.5% ) with stage iia2 disease . 
patients with squamous cell carcinomas accounted for 93.7% ( 59 / 63 ) , with 94.3% ( 33 / 35 ) in the sr group , and 92.9% ( 26 / 28 ) in the non - sr group . 
during the 1 3 1238 la radiologia medica ( 2020 ) 125 : 12331242 follow - up period , tumor recurrence was observed in seven of 63 patients ( 11.1% ) , where three patients occurred in the sr , and four occurred in the non - sr . 
if we can accurately predict the therapeutic response before treatment , patients suffer from cervical carcinoma may receive tailored management by adjusting treatment regimens . trans , kmax our results showed that kmean trans , ve mean , ve 10% , and adc90% could contribute to predict nact trans comefficacy for locally advanced cervical cancer . 
k90% bined with adc90% showed the highest diagnostic value in predicting nact effectiveness for cervical cancer . trans , k90% to date , several studies have appraised the correlation between dce - mri parameters and therapeutic response in cervical cancer . 
4 roc curves of kmax trans , kmean trans , k90 trans , and adc90 1 3 1240 la radiologia medica ( 2020 ) 125 : 12331242 few studies have focused on the correlation between dce - mri parameters and nact response in cervical cancer . 
feng ys [ 27 ] trans was significantly higher , but ve research showed that kmean mean was significantly lower in the sr group compared with the non - sr group before nact . 
this is not conducive to drugs entering into tumor tissue from blood vessels , and therefore , the therapeutic response is poor in tumors with high ve . dwi can provide information about the microenvironment , including the cellularity and integrity of cellular membranes . 
feng ys [ 27 ] research also showed adc values were not significantly different between sr group and non - sr group before nact , even though adc mean and adc min in the sr group before treatment were lower . 
our research also showed that a high - percentile adc value - adc90% value is meaningful in predicting the nact effect , while adcmean , adcmax , adcmin , and other percentiles of adc values were not significantly different between the two groups . 
theoretically , a curve with substantial left shoulder may indicate a large population of highly cellular tissue , whereas a curve with a marked right shoulder may indicate substantial edematous or cystic portions [ 31 ]  . 
therefore , we speculated that the tumor in sr group tends to contain more necrotic tissues . we also compared the diagnostic efficacy in predicting trans the tumor response of nact . 
our study showed that k90 has a better diagnostic value at 0.71 , and diagnostic efficacy trans was further improved to 0.74 with the combination of k90% and adc 90% , with a sensitivity of 64.3% and a specificity of 82.9%. 
combined with the above two parameters , the microcirculation state and tumor cell density can be used to comprehensively analyze the tumor state . there are several limitations in our study . 
tumor ta was performed on each patients paraxial t2w mri in both preand post - ncrt scans , in order to extract histograms , gray - level co - occurrence matrix ( glcm ) and run - length matrix ( rlm ) texture parameters . 
for features that showed a significant difference between the two groups , a receiver operating characteristic ( roc ) curve was drawn . results overall , 62 patients with larc , treated with ncrt and resective surgery at our institution between 2013 and 2019 were identified . 
most cases are locally advanced , i.e. , clinically staged t34 or node positive , at the time of diagnosis . the gold standard for the treatment of locally advanced rectal cancer ( larc ) , according to the current guidelines , is neoadjuvant chemo - radiotherapy ( ncrt ) followed by total mesorectal excision ( tme )  . 
neoadjuvant therapy has shown to decrease the rate of local recurrences [ 2 ] , and can lead to complete pathological response ( pcr ) in some cases [ 3 , 4 ]  . 
in patients achieving a clinical complete response ( ccr ) a rectal - sparing approach could be attempted in order to spare surgery , that in case of complete response would represent an overtreatment burdened by the risk of major complications and severe impairment on bowel function and quality of life [ 3 , 5 ]  . 
to do so , a classification similar to mandards tumor regression grade ( trg ) system [ 12 ] , mrtrg , has been proposed , based on the hypointensity in the t2 - weighted sequences of the fibrotic tissue in the lesion [ 1315 ]  . 
this classification showed to predict recurrence - free survival ( rfs ) disease - free ( dfs ) and overall survival ( os ) [ 16 ] , while in other studies , mrtrg showed a low correlation with pathological trg [ 17 ]  . 
in particular , the inter - observer agreement for this type of evaluation was not satisfying in trg1 and 2 cases , which are the most relevant in the evaluation of a complete response [ 17 ] , thus an automated quantitative approach for the evaluation of the t2 - weighted signal intensity inside the lesion has been proposed showing a good inter - observer agreement and an excellent correspondence to the histopathological findings [ 18 ]  . 
 [ 19 ] reported that more than 70% of tumor volume changes detected by t2 - weighted images define tumor responses as determined by morphological evaluation by mri . however , these findings may underestimate the difficulty to determine the margin between residual tumor and surrounding normal tissues and to differentiate between residual tumor and fibrosis after ncrt , on the basis of morphological changes only . 
some studies applied texture analysis ( ta ) in order to predict pcr ; different t2 - weighted images , dwi and pet / tc features showed a significant correlation with pathological findings [ 2025 ] and some t2 - weighted images features were found to associate with dfs , rfs , os [ 22 ]  . the aim of the present study was to evaluate the correlation of firstand second - order ta features of the primary lesions volume in preand post - ncrt t2 - weighted mri images and histopathological trg . methods patient selection we retrospectively included consecutive patients with confirmed diagnosis of larc who underwent ncrt followed by curative surgery at our center between 2013 and 2019 . 
 patients with stage ii and ii rectal cancer , located at less than 11cm from the anal verge , who received preoperative radiotherapy with a total dose of 50.4gy ( in daily fractions of 1.8gy five times a week ) , with concomitant administration of 5 - fluorouracil - based chemotherapy by continuous venous infusion or oral capecitabine , and who underwent pelvic mri with a slice thickness of 3.5mm both before and after ncrt , were included in the study . 
inclusion criteria also involved the availability of the results of histopathological examination , complete with mandards trg classification on the surgical specimens . patients who did not meet these criteria , along with all patients with poor image quality and movement artifacts , were excluded . 
all the patients included gave written informed consent to use imaging data for research aims . image acquisition staging and restaging of all patients were performed using a 1.5t mri ( avanto ; siemens , erlangen , germany ) with phased - array coils . 
the examination protocol included t2 - weighted sagittal , oblique coronal ( i.e. , parallel to the long axis of the primary tumor ) and oblique axial ( i.e. , perpendicular to the long axis of the primary tumor ) images , with a repetition time ( tr ) of 37905354ms , an echo time ( te ) of 95ms , a slice thickness of 3.5mm , a field of view ( fov ) of 320 286mm and an image matrix of 320 257 . histopathological examination histopathological examination was performed by expert pathologists , specialized in gastrointestinal diseases . 
for 1 3 1218 la radiologia medica ( 2020 ) 125 : 12161224 each patient , a biopsy of the primary lesion before ncrt confirming the diagnosis of malignancy was available . 
histopathologic examination on the surgical specimen included pathological tumor stage , nodal stage ( in case of tme ) and trg according to mandards classification , with trg1 indicating complete response and trg5 indicating the absence of regressive changes in the tumor [ 12 ]  . 
patients with complete response ( trg1 ) , were classified as group 0 , while patients with residual tumor ( trg25 ) were classified as group 1 . image analysis a volume of interest ( voi ) was outlined around the rectal lesion in all paraxial t2 - weighted mri slices in which the cancer appeared , in both preand post - ncrt examinations . 
 vois were obtained for all patients by two radiologists , who manually contoured the tumor area , using a dedicated software ( pmod , pmod group , zurich , switzerland )  . 
texture analysis was performed using pmod analysis algorithms ; thirty - three parameters , derived from voxel histograms , gray - level co - occurrence matrix ( glcm ) and run - length matrix ( rlm ) analysis , were extracted for each mri scan . statistical analysis continuous variables obtained through ta were expressed as mean standard deviation ( sd )  . 
statistical analysis was performed using the r software [ 26 ]  . results patient clinicopathological characteristics sixty - two patients , 42 males ( 67.7% ) and 20 females ( 32.3% ) , were included in this study . 
 fifty patients ( n = 50 , 80.6% ) underwent tme , while 12 patients ( n = 12 , 19.4% ) underwent transanal local excision ( le )  . 
overall , 19 patients were defined as responses based on ptrg = 1 ( 30.6% ) , while 43 patients with ptrg between 2 and 5 ( 69.4% ) were defined as non - responders . 1 3 la radiologia medica ( 2020 ) 125 : 12161224 1219 table 1 patient clinicopathological characteristics features classification surgery ptrg male female 60years > 60years local excision trg1 trg2 trg3 trg4 trg5 n ( % ) 42 ( 67.7% ) 20 ( 32.3% ) 20 ( 32.3% ) 42 ( 67.7% ) 50 ( 80.6% ) 12 ( 19.4% ) 20 ( 32.3% ) 7 ( 11.3% ) 17 ( 27.4% ) 14 ( 22.6% ) 4 ( 6.4% ) 38 ( 61.3% ) 11 ( 17.7% ) 1 ( 1.6% ) 12 ( 19.4% ) 19 ( 30.7% ) 15 ( 24.2% ) 16 ( 25.8% ) 9 ( 14.5% ) 3 ( 4.8% ) ypt , histopathological t - stage after ncrt ; ypn , histopathological n - stage after ncrt ; ptrg , histopathological tumor regression grade according to mandards classification ; tme , total mesorectal excision ; le , local excision . 
histopathological examination of lymph nodes was not possible for patients who underwent le ; therefore , ypnx ( n indeterminable ) was reported for these cases comparison ofprencrt t2weighted ta parameters pre - ncrt ta parameters of the two groups are reported in table2 . 
other parameters , such as glcm homogeneity inverse different moment , glcl sum entropy and glcm entropy , approached the cut - off of p = 0.05 , without reaching significance . 
 for this parameter , a roc curve with an area under the curve ( auc ) of 0.6622 ( ci 95% 0.51280.8116 ) according to delong test was obtained [ 28 ]  . 
during the last decades , many efforts have been made in order to reach a tailored approach in the management of this disease , thus avoiding over - treatment and preserving patients quality of life . 
non - operative management ( nom ) of patients showing a ccr to ncrt can spare these patients the potential complications of major surgery , while other rectal preserving approaches , such as le , can be used in some patients with a complete or major response in order to avoid the severe impact on quality of life of conventional surgery . 
on the other hand , neoadjuvant therapy itself is associated with several side effects , and is not always beneficial for the patients in terms of reduction of tumor burden . thus , the identification of reliable markers of response to ncrt has gained growing interest . 
ta has been suggested as a promising technique to investigate intra - tumor heterogeneity attributed to various factors such as hypoxia , necrosis and angiogenesis , potentially related to tumor aggressiveness and patient prognosis [ 2025 ]  . 
both hypoxia and necrosis following chemo - radiotherapy cause fibrosis of the neoplastic tissue ; fibrous tissue is characterized by hypo - intense signal in the t2 - weighted sequences , and therefore can be differentiated from residual vital tumor [ 29 ]  . 
ta could also predict which patients will respond to ncrt even before the treatment is started , or a few weeks after the onset of treatment [ 20 , 21 , 24 , 25 ] , and may improve mri performance in the evaluation of response [ 22 ]  . different studies have investigated ta parameters of t2 - wieghted mri images as a tool to discriminate patients with a pcr and patients with residual disease . 
in a later study of the same group , pretreatment t2 - weighted images kurtosis showed a sensitivity and specificity with two different suggested cut - offs of , respectively , 100% and 67% and 83% and 83% [ 21 ]  . 
the authors considered pre - , interim and post - ncrt t2 - weighted ta , and found that skewness , entropy and energy of the pre - ncrt ta and variance , kurtosis , energy and entropy of early - ncrt ta ( at 3weeks from the beginning of ncrt ) differed significantly between responders and non - responders [ 24 ]  . 
 [ 31 ] found in 76 cases that firstorder features of ta extracted from post - ncrt t2 - weighted mr images could identify patients with complete response at histopathology . 
our results do not support the routinary use of t2 - weighted images ta for the evaluation of rectal cancer response to chemoradiation , even if one parameter obtained from mri images after ncrt showed to be a potential imaging bio - marker to identify patients with a pcr . 
in fact , among the multiple parameters obtained in both preand post - ncrt images , only one , i.e. , glcm maximum probability post - ncrt , showed significant differences between complete responders ( i.e. , group 0 = trg1 ) and non - responders ( i.e. , group 1 = trg25 )  . 
this parameter showed a low sensitivity , although a specificity of 100% was found at the roc curve youden index . 1 3 1222 la radiologia medica ( 2020 ) 125 : 12161224 af , gc , smr and qrb involved in the literature research ; gs , dc , la and sp involved in clinical studies ; fc , af , smr , dc and la involved in experimental studies / data analysis ; cc was involved in statistical analysis ; fc , af , gc , smr , dc , la and cc involved in manuscript preparation ; gs , gc , qrb , sp and rs involved in manuscript editing . funding no external funding for this manuscript . 
 there were multiple difficulties in performing mri examinations in patients with cied , linked to the precautionary approach of the medical / scientific community ( based on the theoretical possibility of even fatal complications arising from interactions with the mri environment ) [ 1 , 2 ] , as well as to legal concerns . 
until recently , in fact , the execution of mri examinations was regulated by the ministerial decree 2 august 1991 [ 3 ] , which explicitly and absolutely prohibited admitting patients with pms and implanted electronic devices of any kind into mri environments . 
however , in recent years , the scientific community and industry have shown a growing interest in the study of the interactions between cied and mri and have developed active cardiac devices of conditional type ( i.e. , implants for which the risks of performing an mri examination were considered and reduced during the vol . : ( 0123456789 ) 1 3 1312 la radiologia medica ( 2020 ) 125 : 13111321 design and construction phase )  . 
these devices are meant to allow those patients that carry them to undergo mri examination safely , as long as the cied conditions of use specified by the manufacturer and reported in the technical manual are complied [ 46 ]  . 
any other combinations from the same manufacturer or from different manufacturers are mix - and - match systems , and since they are not tested or certified , they cannot be considered mr - conditional , even when the individual components are labeled as such . executing mr examinations on patients with not mrconditional systems or with mr parameters noncompliant with the conditions set by the manufacturer constitutes an assumption of responsibility by the medr and by the medical doctor responsible for the activity of the mri site . it is important to notice that european community certification for cied is based not on fda approval but on european parliament and council directives [ 79 ] that define the safety essential requirements and the methods to prove conformity and show the preand post - market production review system related to the manufacturers and the control strategy by the competent authority ( in italy the ministry of health )  . 
another essential requirement is the obligation for the manufacturer to supply together with the device all the information necessary for its safe use . since 2011 , pms , loop recorders and mri - implantable defibrillators have been introduced to the market and implanted . 
therefore , in the current population , there are both mr - conditional and traditional devices as well as mix - and - match system . with regard to traditional cieds , the scientific literature of the last decade has shown that it is possible to perform mri examinations in nonthoracic regions with an acceptable level of risk [ 10 ] , and in 2008 , an european position paper was published where the presence of traditional cieds and mix - and - match systems is no longer classified as an absolute but instead as a relative contraindication , which therefore requires a risk / benefit analysis on a case - by - case basis [ 4 , 11 ]  . in 2015 , the istisan 15 / 9 report [ 12 ] indicated a possible strategy for performing mri examinations in patients with cied , even in the coexistence of dm 2 august 1991 . this new technological / scientific landscape was finally recently transposed by the italian legislature in the repeal of the 1991 dm [ 3 ] replaced by the dm 10 august 2018 [ 13 ] , which makes it clear that : with regard to patients with active implantable heart devices , the health structure is obliged to prepare a specific organizational model to ensure the safety of performance and health of the patient , including a process of assessing the benefit / risk ratios of execution and the failure to perform the mri exam . despite these growing technological and legislative guarantees , the italian hospital landscape is still not adequately prepared to deal with these directives and is not always able to ensure easy access to mri examinations for cied carriers . 
to date , unfortunately , a large share of patients who could benefit from diagnostic mri are in fact excluded from these investigations precisely because they have a cied , even if of the mr - conditional type [ 15 , 16 ]  . procedure forperforming mri examinations inpatients withcied at our hospital for some years , thanks to a close collaboration between the radiology , cardiology and medical physics departments , an internal procedure has been set up to safely perform mri examinations in patients carrying cied . 
the gradient system shows a maximum slew rate of 180 mt / m / ms and maximum gradient amplitude of 33 mt / m . the procedure , prior to the introduction of the recent decree , was largely inspired by what was proposed and detailed in the 2015 inail and iss joint document [ 12 ] and was based on a close collaboration between medr and medc , and in some selected cases , it also included mp advice . 
an anesthesiologist - resuscitator is also present at our facility to eventually assist in the management of any emergencies at the mri site . the procedure has five operational steps , which are described below in detail . phase oftaking care ofthepatient andscheduling theexamination the possibility of performing the mri examination must be ascertained before the booking of the examination itself , in order to avoid risks or delays in the diagnostic path and inefficiencies in the use of instrumental resources . for this purpose , the radiology administrators or those who take charge of the patients request take care to collect from the patient all the technical documentation specific to the device which the patient is bearing , in addition to the motivated request . 
in particular , the patient is required to present the badge of the implanted device or the written certification of the type / model of the device , the date of the implant and any replacements of the generator and / or catheters . the medr , after verifying the appropriateness of the request , also through an interview with the requesting doctor 1 3 la radiologia medica ( 2020 ) 125 : 13111321 1313 if necessary , must then carry out an assessment of the risk / benefit balance . 
this is not always straightforward , and especially in the case of traditional cied or mix - and - match systems , it may often require collaboration between medr , medc and mp . the medr must also assess the compatibility of the mrconditional system with the mr equipment in use in the hospital and verify the possibility of complying with the technical constraints expressed by the manufacturer of the implanted device [ 1719 ]  . evaluating theriskbenefit ratio for a correct assessment of the riskbenefit ratio , it is important to know whether the system the patient is carrying is mr - conditional or whether it is a traditional system or a mix - and - match one . 
in the case of mr - conditional systems , the medr must verify that the mr equipment and the technical parameters of the examination meet the detailed conditions in the cieds manual . with regard to traditional and mix - and - match systems , the medr must be aware that the risk of undergoing mri examinations has not been previously assessed by the manufacturer and that therefore the execution of mri examinations on patients who carry such systems constitutes an off - label situation , in which the liability for any adverse effects lies with the medr and not with the manufacturer of the device . however , it is also appropriate in these cases not to underestimate the potential benefits that can result from an mri which is often fundamental not only for a correct diagnosis but also , for example , for the correct staging of heteroplasia disease , allowing to direct the patient to the therapeutic path that leads to the best prognosis [ 20 ]  . if a given system has already been successfully evaluated in scientific publications , in conditions comparable to those being evaluated ( e.g. , sar , gradients , plant region , location to be examined ) , the risk level reasonably decreases . 
however , in the absence of such information , a high risk should be conservatively assumed . the body part to be examined also affects the risk level , as the thoracic regions are at greatest risk ( e.g. , dorsal spine , breast regions , heart and chest wall and shoulder ) , while the study of the brain , pelvis , cervical and lumbar spine has a lower risk . 
this kind of setup in some cases is expressly not recommended in the devices technical manual . in the technical manual of some mr - conditional pm / icds , it is recommended not to perform the mri examination in the presence of other cardiac or extra - cardiac metal devices longer than 5cm in length near ( < 4cm ) the epicardic stimulation catheters , due to the increased theoretical risk of overheating . in addition , since the threshold values for capture and stimulation are unstable immediately after implantation due to the healing phenomena around the apex of catheters , manufacturers generally define a minimum time ( usually 6weeks ) before mri examinations may be performed . there are also cardiological risk factors . 
in particular it is crucial to ensure that the device has optimal electrocatheter threshold and impedance values before the mri , because their increase during examination would lead to a subsequent inefficiency of the syste of course , this is even more important in pm - dependent patients , who do not have residual spontaneous cardiac activity and who may experience asistolia in the event of threshold increases that result in a failure to capture the heart rate . 
cardiological risk factors related to mechanical and geometric elements must also be considered , i.e. , those related to the type of hardware present in the patients body . in particular , the presence of fractured or abandoned catheters , even if hooded for their isolation , poses a high risk of overheating of the catheter , so much so the 2013 guidelines of the european society of cardiology [ 2123 ] exclude the execution of mri examinations on patients with abandoned and / or broken catheters . 
studies on dummies have also shown that the risk of catheter overheating is higher when the generator is positioned to the right , compared to the more common left localization [ 24 ]  . the risk of induction of arrhythmic phenomena should also be considered , but this is difficult to estimate on an individual patient basis ( i.e. , it is theoretically higher in patients with vulnerable myocardial portions , for example for acute / subacute myocardial infarction or acute myocarditis or in patients with arrhythmogenic structural alterations )  . 
it should be remembered , however , that such arrhythmic phenomena almost never pose a serious danger for the patient and to date only rare cases of benign arrhythmias during mri examination have been recorded in the literature [ 25 , 26 ]  . it is also useful to point out that as loop recorders or recorder monitors are subcutaneous devices for continuous recording of cardiac activity and do not have epicardic catheters , their handling in mri is much easier and safer than pm and / or icd . evaluation ofmrconditional compatibility withmri equipment inthestructure in the case of mr - conditional cied systems , the manufacturer has to report the conditions under which performing mri examinations is safe . 1 3 1314 la radiologia medica ( 2020 ) 125 : 13111321 table1 shows the technical specifications that are most frequently provided . 
the list is not exhaustive , and further conditions should always be verified by preferably consulting the technical manuals on the manufacturers web site . among the various parameters , it may be useful to give some details about the sar and the spatial gradient magnetic field . specific absorption rate ( sar ) is the dosimetric term used to characterize the absorption of energy from radiofrequency ( rf ) and is measured in w / kg . 
in addition , high ambient humidity and temperature , as well as the presence of heavy clothing , reduce the bodys ability to disperse heat to the environment . the technical industry legislation has set operational ranges for the sar [ 27 ] ; clinical mri systems can work within two operational ranges : zero level ( normal operating mode ) and first level ( first level controlled operating mode )  . 
in addition , in order to improve the thermal exchanges between the patient and the environment , it is important to check that the humidity and temperature in the magnet room are within the respective optimal range , that the ventilation inside the gantry works properly and to remove any blankets and items of clothing that may limit heat dispersion ( table2 )  . the spatial gradient magnetic field is the spatial variation of the static magnetic field ( b )  . 
it is measured in t / m or gauss / cm and refers to the rate at which the static magnetic field strength changes over space or distance per unit of length . 
in both cases , it is explained to the patient that all possible broken and / or abandoned leads date of the installation 6weeks use of transmitting coils and / or use of coils receivers and transmitters placed directly above the cied patients with stimulation capture threshold values > 2.0v at a pulse duration of 0.4ms patients with an electrocatheter impedance value of < 200 o > 1500 patients pacing dependent with icd where asynchronous mode cannot be set 1 3 la radiologia medica ( 2020 ) 125 : 13111321 1315 fig . 
1 informed consent for mr - conditional cieds procedures will be taken in order to reduce the risk of such complications and that his / her safety during the examination will be guaranteed by the constant presence of the medr and the medc and , in case of need , by the immediate availability of the resuscitating physician , who is always present on - site . cardiological prescan assessment and / or issues within his / her competence , the actual execution of the examination is re - discussed and re - evaluated together with the medr . the cardiological assessment consists primarily in examining the operating state of the device using a standard telemetric control in order to exclude the possibility that there may be suboptimal threshold and impedance values , which could represent a contraindication to the execution of mr examination . for convenience , the cardiological evaluation is performed by the medc specialist in electrophysiology on the day of the examination ; if the medc encounters contraindications during the examination , it is possible that any induced currents will cause a lesion of the myocardium in contact with the tip of the catheter and this could lead to an increase 1 3 1316 la radiologia medica ( 2020 ) 125 : 13111321 fig . 
each manufacturer defines the maximum allowable stimulation threshold and impedance range for their mr - conditional systems . a low battery voltage , on the other hand , could increase the risk of an electrical reset during the examination . in addition to checking the proper functioning of the cied , the medc must program the cied in the most appropriate way to conduct the examination taking into account whether the patient is pm - dependent or has a spontaneous pace . 
in the first case , in fact , an asynchronous programming of the device is preferred , i.e. , a fixed stimulation mode , independent of any inherent cardiac 1 3 la radiologia medica ( 2020 ) 125 : 13111321 1317 activity , which is not affected by possible interference and inhibitions caused from the examination . performing mri scans in pacing - dependent patients with icd and when an asynchronous programming mode cannot be set is highly critical , and in such cases , there is a tendency to rule out the possibility of performing the mri examination . performing theexamination the medr verifies that the scan meets the specific conditions of the mr - conditional system and with the help of the radiology health technician ( tsrm ) sets the scan parameters optimizing the sar values and the scan time , based on the assessment of the actual diagnostic and therapeutic benefit for the patient . 
during the examination , the patients vital parameters are constantly monitored by multiparameter equipment certified for use in an mri environment . in our experience , the simultaneous use of ecg and pulsoxymetry ensures a better chance of following the patients pace , especially in those cases where the quality of the ecg track of the multiparametric is degraded by generated mr scanner artifacts . during the examination , both the medr and medc are present and outside the magnet room a defibrillator is always readily available , which is checked every morning by the nursing staff . 
more specifically , three patients with icd , 33 patients with pm ( including two pm - dependent patients ) and three patients with loop recorder were examined . patients with icd were not pacing dependent and underwent , respectively , an ankle mri study to rule out possible osteonecrosis and a brain mri study . of the 33 pms introduced in the mr scanner , three were of the non - mr - conditional type . 
one case was that of a patient with a traditional pm who underwent a brain assessment on suspicion of amyloid vasculitis ( a condition that is difficult to diagnose without mri ) ; the other fig . 
3 internal organizational path 1 3 1318 la radiologia medica ( 2020 ) 125 : 13111321 two cases were patients with mix - and - match pm systems undergoing , respectively , an mri for suspected brain repetitive lesions ( not confirmed by the mri examination ) and a high - resolution mri study of the pelvis for locoregional stage of a uterine cervix heteroplasia with suspected parametrial invasion ( which had been found very doubtful at the clinical evaluation and was subsequently confirmed by the instrumental investigation )  . 
in all these three cases , the outcome of the mri allowed the patients to be directed to the more appropriate treatment which guaranteed the best prognosis . all the three patients were informed of the possible risks and increased health benefits deriving from the examination and signed the consent to the survey . the mri examinations of the thoracic spine ( three exams including a whole spine mri ) were carried out in accordance with the manufacturers provisions , which , in these cases , did not specify restriction zones . in cases where the same patient was subjected to the study of two segments , such as brain mri and spinal cord mri , the two examinations were separated by a 5 - min interval . the average duration of mri examinations was about 22min . under no circumstances during the examinations , there were patients complaining of ailment nor were atrial or ventricular arrhythmias recorded . in all patients , no change in stimulation / capture threshold values was recorded at the post - procedure check compared to the pre - scan values , nor any change in battery voltage was found . 
only in one case , the patient with nonconditional pm in which the cardiologist had chosen to program the cied in off mode , the estimated battery life went from 3years before the scan to 2.5years after the scan ; the voltage of the battery , however , remained unchanged . in all other cases , there were no changes in the estimated battery life . in the three patients with loop recorders ( subjected in one case to an mri of the pelvis and in the other two cases to mri examinations of the brain with added brain angio - mr evaluation in one patient ) , no malfunction of the devices was detected post - scan , nor were any recordings affected by interference with the mri environment . 
 at our radiology department , we have then continued to perform mri examinations in patients holding loop recorder after checking the compatibility conditions declared by the manufacturer ; however also in view of the fact that they are free of epicardic catheters , when not specifically required in the technical manual , the preand post - scan cardiological evaluations are not performed . 
 whenever possible , we suggest a cardiological check before performing the mri examination to ensure that the data recorded by the device until then are not lost ; however , the most popular loop recorders have an automatic system of data transmission that takes place remotely via satellite at regular intervals or after a significant event is recorded by the device itself . as a further precaution , we are considering reporting the start and the end time of the mri examination on the radiological report so that at the subsequent cardiological check any abnormal recordings may be assessed by the specialist as being due to interference with the mri environment and not to a patients pathology . table3 summarizes our case studies . we were able to directly perform a long - term cardiological follow - up of 17 patients , including two of the three patients with not mr - conditional system , at 612months after the mri examination . 
we could not register any significant ( i.e. , 0 , 5v ) variation in the stimulation / capture threshold values , nor cied malfunctions , nor variations in devices parameters . 
no adverse reports have been received from the other patients that continued their cardiological outpatient follow - up at their referral center . the main limitations of our case studies are the limited number of patients and the fact that all data have been acquired in a single center with 1.5 t equipment ( this information does not apply to 3t mri systems )  . the results of our experience are in line with the literature of the recent years regarding execution of mr examinations on patients with both mr - conditional and traditional pm and icd and which indicates that the incidence of adverse events , when examinations are performed with all the procedural precautions discussed above , is very low and the patients life is never at risk [ 26 , 3242 ]  . conclusion clinical evidence and literature based on evidence - based medicine in the coming years will probably simplify , perhaps even greatly , the procedures to perform this type of examination . 
eighty - seven out of 337 patients had a negative first rt - pcr result ; of these , 68 repeated rt - pcr testing and were included in the study . the first rt - pcr test showed se 0 , sp = 100% , ppv = nan , npv = 70% , auc = 50% , and ct showed se = 70% sp = 79% , ppv = 86% , npv = 76% , auc = 75% . the most relevant ct variables were ground glass opacity more than 50% and peripheral and / or perihilar distribution . discussion negative rt - pcr test but positive ct features should be highly suggestive of covid - 19 in a cluster or community transmission scenarios , and the second rt - pcr test should be promptly requested to confirm the final diagnosis . keywords covid - 19 rt - pcr nasopharyngeal swab computed tomography * caterina giannitto caterina.giannitto@gmail.com 1 radiology division , humanitas clinical andresearch center , irccs , via alessandro manzoni , 56 , 20089rozzano , milan , italy 2 digestive endoscopy unit , department ofgastroenterology , humanitas clinical andresearch center , irccs , via alessandro manzoni , 56 , 20089rozzano , milan , italy 3 department ofbiomedical sciences , humanitas university , pieve emanuele , milan , italy 4 training school inradiology , humanitas university , pieve emanuele , milan , italy 5 department ofcomputer science ( di ) , university ofmilan , via g . 
celoria 18 , milan , italy 6 laboratory medicine , humanitas clinical andresearch center , irccs , via alessandro manzoni , 56 , 20089rozzano , milan , italy 7 division ofthoracic surgery , humanitas clinical andresearch center , irccs , via alessandro manzoni , 56 , 20089rozzano , milan , italy 8 department ofnuclear medicine , humanitas clinical andresearch center , irccs , via manzoni 56 , 20089rozzano , milan , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 12601270 1261 introduction on may 24 , italy reported 229 , 858 confirmed cases of coronavirus disease - 19 ( covid - 19 ) and 32 , 785 deaths since the initial outbreak of the disease in codogno , italy , in late february [ 1 ]  . clinically , patients infected with severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) present fever , cough , dyspnea , muscle aches and bilateral pneumonia on imaging [ 2 ]  . real - time polymerase chain reaction ( rt - pcr ) on a nasopharyngeal swab is the most frequently used diagnostic method for detecting sars - cov - 2 [ 3 ] , with a sensitivity ranging from 60 to 71% [ 2 , 4 , 5 ]  . 
 an initial false - negative result could delay treatment and increase the risk of viral transmission to others . this study aimed to describe the diagnostic performance of chest ct in patients with a moderate or high pretest probability of covid - 19 infection , with negative rt - pcr testing . 
we also aimed at identifying imaging features typical of covid19 pneumonia diagnosis , which can help suggest a diagnosis in patients with a negative rt - pcr . materials andmethods patient population andstudy design retrospective nature of the study and the use of anonymous clinical data . data were extracted from an institutional prospectively maintained database , including consecutive patients admitted to our emergency department , from march 1 , 2020 , to march 29 , 2020 . we included symptomatic patients who underwent ct with a moderate or high pretest probability of covid - 19 infection according to the transmission scenarios ( cluster or community ) defined by the world health organization [ 19 ] with moderate or severe respiratory symptoms [ 11 ] and a negative rt - pcr swab . 
the time - interval between chest ct and the rt - pcr assay was no longer than four days . clinical data all patients who underwent ct were symptomatic , presenting with fever ( temperature > 375c ) , cough , and dyspnea . a patient was considered as covid - 19 positive or negative after a positive or negative bronchoalveolar lavage or a second nasopharyngeal rt - pcr test . the preferred choice in our hospital was the rt - pcr test from bronchoalveolar lavage after a first negative rtpcr swab . we excluded patients who did not undergo ct examination or without two rt - pcr tests . laboratory data nasopharyngeal swabs or bronchoalveolar lavage specimens were analyzed with rt - pcr technique to confirm the presence of the sars - cov - 2 virus in the upper or lower respiratory tract . 
one method is based on rna extraction through high - affinity magnetic silica ( biomrieux , france ) and amplification with allplextm 2019ncov assay ( seegene , seoul , south korea ) , a multiplex real - time pcr assay for simultaneous detection of 3 target genes of sars - cov - 2 in a single tube with the cfx96tm real - time pcr instrument ( bio - rad , france )  . 
the second system detected the same genes and was performed on the ingenius instrument ( genefinder covid - 19 plus realamp kit elitech group , south korea )  . ct acquisition technique the study was approved by our local institutional review board ( irb )  . 
informed consent was waived because of the as per our hospital covid - 19 protocol , all chest ct acquisitions were obtained with the patients in the supine position during end - inspiration without contrast medium 1 3 1262 la radiologia medica ( 2020 ) 125 : 12601270 the diagnostic performance of both first rt - pcr result and ct was evaluated by using sensitivity ( se ) , specificity ( sp ) , diagnostic accuracy , positive predictive value ( ppv ) , negative predictive value ( npv ) and area under the curve ( auc ) , considering the second rt - pcr test result as the definite result . ct findings ( and variable values ) for patients with positive or negative second rt - pcr results were compared by using nonparametric kruskalwallis test , for continuous variables , and with the pearson chi - squared test , for categorical variables . 
such aggregation was computed by iteratively using the boruta algorithm [ 21 ] and a random forest classifier [ 22 ]  . the comparison between the medians of the number of days ( time ) between the onset of symptoms and first naso - oropharyngeal rt - pcr test , chest ct examination , and second rt - pcr test was expressed through a wintieloss table , where all the wintielosses were validated by the wilcoxon rank - sign test ( 95% confidence level )  . results patient population andclinical data eighty - seven out of 337 patients had a negative first rt - pcr result . 
the following technical parameters were used : tube voltage 120kv ; tube current modulation 127 mas ; spiral pitch factor 1490 ; rotation time 04s , matrix 512 ; reconstructions had a slice thickness of 2mm . ct image analysis two radiologists with five and fifteen years of experience ( > 1000 ct per year ) in chest imaging , who were blinded to rt - pcr results , reviewed all chest ct images . 
age distribution and median standard error [ min value , max value ] are reported 1 3 la radiologia medica ( 2020 ) 125 : 12601270 1263 ct performance of 68 ct examinations , 24 were diagnosed suspected of covid - 19 pneumonia ( 14 patients had a positive second test and 10 a negative second test ) , 31 were diagnosed as non - covid - 19 pneumonia ( 6 patients had a positive second test and 25 a negative second test ) , and 13 were diagnosed as negative in consideration of the perceived likelihood of covid - 19 ( table2 )  . ct findings in suspected covid - 19 pneumonia and noncovid - 19 pneumonia are reported in tables3 and 4 . the most discriminative features were : ground glass opacities ( ggo ) more than 50% of lung patt e r n ( p va l u e = 0 0 0 0 , 0 4 0 , 6 8 7 ) , m u l t i p l e l o b e involvement ( p value = 000 , 025 , 824 ) , peripheral ( p value = 000 , 035 , 559 ) , peripheral and perihilar ( p value = 00 , 038 , 061 ) distribution , bilateral distribution ( p value = 00 , 046 , 384 ) , pleural effusion ( p value = 0010 , 927 ) , consolidation more than 50% of lung pattern ( p value = 001 , 395 ) , lymphadenopathy ( defined as lymph node with short axis > 10 mm ) ( p value = 0032 , 051 ) , while the remaining variables did not show any statistical difference between the distribution of covid - 19 - positive patients and covid - 19 - negative patients . 
note that the addition of more variables ( and rules ) to the combinations ( ground glass opacities more than 50% of lung pattern and peripheral distribution ) and ( peripheral and perihilar with peripheral distribution ) does not increase performance . 
grey bars show not statistically significant features ( p value > = 0.05 ) , violet bars highlight statistically significant features ( p value < 0.05 ) 1 3 1266 la radiologia medica ( 2020 ) 125 : 12601270 fig . 
3 a 67 - year - old man with a negative first rt - pcr result : ground glass opacities more than 50% of the lung pattern with peripheral and bilateral distribution in axial and coronal ct planes ( a , b )  . 
the extent of the aerated lung was in all batches quantified by the percent of lung voxels with attenuation < 660 hounsfield units ( c ) rt - pcr swab with the duration from onset of symptoms to second rt - pcr swab of only 55 078days . load due to the technique of sample collection or the time when the sample is collected in the course of the disease . six out of 68 patients were confirmed covid - 19 positive ( four ) or negative ( two ) by the second oro - nasopharyngeal rt - pcr swab and bal . the diagnostic performance of ct in combination with a second rt - pcr test achieved a se of 100% , sp of 79% ppv of 67% , npv of 100% , and accuracy of 85% ( table2 )  . we repeated the statistical analysis of ct performance without the 12 patients who were confirmed covid - 19 positive or negative only by the second naso - oropharyngeal rt - pcr swab , and we found se of 68% , sp of 81% , ppv of 83% , npv of 76% and accuracy of 74% that confirm the better performance of ct than first rt - pcr swab in the identification of false - negative cases . of the 20 confirmed positive covid - 19 patients , nine patients had other lung co - infection , and of the 48 confirmed negative covid - 19 patients , 34 had another lung infection ( table5 )  . the performance of ct in the differential diagnosis of suspected covid - 19 pneumonia vs . 
non covid - 19 pneumonia and negative ct showed se of 70% , sp of 79% , ppv of 59% , npv of 86% and accuracy of 76% ( table2 )  . discussion to date , nucleic acid detection with rt - pcr is the gold standard for covid - 19 diagnosis despite being associated with a false - negative rate as high as 50% in a single detection [ 14 ]  . notwithstanding the high specificity , rt - pcr tests can give false - negative results if the sample contains low viral the use of ct for covid - 19 diagnosis is controversial . 
 it can have a crucial role in the early identification of falsenegative patients , orienting medical choice and follow - up in the endemic area . a meta - analysis of kim etal . 
 [ 23 ] , the diagnostic performance of ct versus rt - pcr was evaluated in patients with positive and negative first rt - pcr , considering ct as a screening tool . we aimed to focus on patients with a first negative rtpcr test to evaluate the added value of ct in this condition . our results confirmed a higher sensitivity and lower specificity of ct ( se 70% , sp 79% ) in respect of a negative rt - pcr test ( se 0% , sp 100% )  . the limitations of rt - pcr are false - negative cases , while of ct are false - positive ones . 
in our experience , the number of false - positive ct cases was lower than the rt - pcr falsenegative cases . the low specificity of ct is due to the overlap of ct imaging features between covid - 19 and other viral pneumonia and lung conditions . 
in fact , in 3 out of 6 falsenegative ct cases , another lung infection was diagnosed . it should be noted that covid - 19 pneumonia is difficult to distinguish by imaging from influenza a virus , influenza b virus , cytomegalovirus , or other viral pneumonia 1 3 la radiologia medica ( 2020 ) 125 : 12601270 1267 fig . 
4 sensitivity , specificity , diagnostic accuracy , positive predictive value ( ppv ) , negative predictive value ( npv ) and area under the roc curve ( auc ) for statistically significant features . 
a standardized conclusion of a radiological report in terms of suspected covid - 19 pneumonia , pneumonia and negative ct could speed up the diagnostic path of patients , suggesting to clinicians to maintain the patient in isolation , to repeat rt - pcr test or to make a differential diagnosis with other lung infections or other lung diseases . we evaluated chest ct considering established imaging features that are considered typical of covid - 19 pneumonia [ 710 , 20 ] , classifying lung patterns in suspected covid - 19 pneumonia , non - covid - 19 pneumonia and negative ct [ 31 ]  . the performance of chest ct in the differential diagnosis of suspected covid - 19 pneumonia vs . 
in addition , differences in stiffness values were assessed among the five stages of ckd . materials and methods five healthy volunteers and 25 patients with ckd ( five patients in each stage ) were enrolled in the study . 
the mean stiffness in patients with ckd significantly increased with the ckd stage ( p = 0.013 ) , although it decreased in stage 5 ckd . conclusion renal tissue stiffness measured using mr elastography can be used to distinguish between patients with ckd and healthy individuals ; moreover , it can be useful in predicting the stage of ckd . keywords magnetic resonance imaging elasticity imaging techniques chronic kidney disease fibrosis renal stiffness introduction chronic kidney disease ( ckd ) is an important health problem in many countries , which is characterized by gradual reduction in renal function and ultimate destruction of the kidney . 
serum markers , such as creatinine , blood urea nitrogen , and estimated glomerular filtration rate ( egfr ) , enable practical * jhii - hyun ahn radajh@yonsei.ac.kr 1 department ofradiology , yonsei university wonju college ofmedicine , wonju severance christian hospital , 20 ilsan - ro , wonju , gangwon - do26426 , republicofkorea 2 department ofinternal medicine , yonsei university wonju college ofmedicine , wonju severance christian hospital , 20 ilsan - ro , wonju , gangwon - do26426 , republicofkorea assessment of renal function [ 4 ]  . 
however , because these serum markers are affected by age and body mass index , they cannot be used consistently to evaluate kidney function [ 5 ]  . magnetic resonance ( mr ) elastography is an mri - based technique that uses shear wave and computing wavelength to measure tissue stiffness [ 6 ] ; notably , mr elastography can be applied to evaluate the stiffness of internal organs ( e.g. , the liver ) that are closely related to the stage of fibrosis . 
the patients were classified into one of the five stages of ckd , based on disease severity , using the kidney disease outcomes quality initiative ckd classification ( table1 ) [ 7 ]  . 
the active driver produced acoustic vibrations at 60hz ; these were transmitted to the passive driver , which then transmitted the vibrations into the body , producing shear wave motion within the kidney . 
a gradient - echo mr elastography sequence was used to acquire images showing shear wave propagation within the kidney by encoding tissue motion into the phase of the measured mr signal . 
finally , we used a 95% confidence map to check if enough parts of the kidney were covered . a custom drawing program ( singo.via ; siemens , erlangen , germany ) was used by two independent radiologists ( 1 and 3years of experience in mr elastography , respectively ) to draw regions of interest ( rois ) ; both radiologists were blinded to the renal status and stage of ckd for all images . 
two readers referenced conventional mr images , wave images , and confidence maps and placed rois in the kidney inside the confidence area using the free - draw method , excluding the renal sinus . 
the mean renal stiffness values were recorded for each participant , and the relationships between renal stiffness values and stages of ckd were assessed . statistical analysis spss version 18 ( spss , chicago , il , usa ) software was used for statistical analysis . 
d manually drawn region of interest , excluding the renal sinus , placed on the elastogram 0.210.40 , and < 0.2 represented substantial , moderate , fair , and poor agreement , respectively . 
 receiver operating characteristic ( roc ) curve analysis was used to determine the cutoff values of renal stiffness in both healthy volunteers and patients with ckd . results a total of 25 patients with ckd ( five patients in each stage ; 15 men and 10 women ) and five healthy volunteers ( two men and three women ) , who had no history of renal disease , hypertension , or other vascular disease , were enrolled in this study . 
the median age of the patients was 54 ( 1984 ) years , while that of the healthy volunteers was 50 ( 3271 ) years . no technical failure was encountered , and mr elastography was successfully performed in all volunteers . 
when threshold renal stiffness values were greater than 4.86kpa , the sensitivity and specificity for ckd diagnosis were 68% ( 95% confidence interval [ ci ] 46.585.1% ) and 100% ( 95% ci 47.8100% ) , respectively in our study , the median renal stiffness of the renal parenchyma in patients with ckd was significantly higher than that in healthy volunteers with normal renal function . 
however , the adc cutoff has varied among previous studies and has demonstrated a limited ability to diagnose early stage ckd [ 10 , 1618 ]  . elastography is a developing technique that can be used for evaluating tissue elasticity . 
however , these studies showed the conflicting results , depending upon the type of technique used ( e.g. , acoustic radiation force impulse imaging or shear wave elastography ) and the researchers involved . 
although several studies have examined fibrosis of the liver , some studies in which us elastography was compared with mr elastography showed that mr elastography was more accurate than us elastography for diagnosis of fibrosis , particularly for early fibrosis [ 14 , 20 , 21 ]  . 
there have been several reports regarding evaluation of renal stiffness using mr elastography , but these have been limited to evaluation of feasibility and reproducibility of normal subjects [ 2224 ]  . 
we used mr elastography to study renal stiffness in patients with ckd and found that renal stiffness values in patients with ckd , beginning in early stages of ckd , were higher than those in normal volunteers . several studies have performed mr elastography for healthy young adults , and the normal renal stiffness values presented in those studies were 2.21kpa at 45hz , 3.5kpa at 60hz , and 3.86.0kpa at 90hz [ 22 , 23 , 25 ]  . 
this difference may be attributed to other factors affecting the renal stiffness , such as the subjects age , blood flow , and hydration status [ 15 ]  . previous studies involving us elastography did not show differences between various stages of ckd [ 11 , 12 ]  . 
however , various cutoff values have been suggested in studies on liver fibrosis staging using mr elastography [ 2630 ] ; this means that mr elastography measurements can be influenced by a number of factors . 
in this sense , our study is clinically meaningful because our results might provide an effective index to guide therapy and monitor patients with ckd during follow - up . in our study , renal stiffness generally increased with the ckd stage ; however , it decreased in stage 5 ckd . 
because of the small size of the kidney , conventional elastography using a higher frequency ( 90hz or greater ) , or tomoelastography using multiple frequencies , may be more suitable . 
furthermore , in a previous study , the difference in measured values between the renal cortex and medulla was not large [ 22 ] ; therefore , we believe that our results were not significantly affected by this issue . 
however , we recruited the volunteers with various ages and tried to reduce the difference of renal stiffness based on age . in conclusion , renal stiffness values from mr elastography can be used to differentiate patients with early - stage ckd from those with normally functioning kidneys . 
the aim of our study was to retrospectively stratify the risk of asymptomatic t2dm patients using low - dose 640 - slice coronary computed tomography angiography ( ccta )  . materials and methods ccta examinations of 62 patients ( mean age , 65years ) with previous diagnosis of type 2 diabetes and without cardiac symptoms were analyzed . 
first - line tests , indeed , are able to detect only severe cad with different rates of accuracy [ 4 ]  . therefore , the clinical need for an effective test to predict significant cad and potential complication in asymptomatic diabetic patients is currently strong , as well outlined also in a recent meta - analysis by clerc etal . 
the patients were asked about the occurrence of major adverse cardiac event ( mace ) defined as all - cause mortality or re - hospitalization for heart failure ( chf ) , re - infarction ( non - fatal ) , recurrence of angina pectoris and repeat pci or coronary artery bypass graft . our retrospective study was carried out after approval obtained by the internal review board committee of our university . 
all patients provided written informed consent . acquisition technique ccta examinations were performed using a 640 - slice ct ( toshiba aquilion one 320 - row detector of 0.5mm each ) , able to acquire up to 16cm in a single heartbeat with half scan temporal resolution of 175ms . optimal image acquisition required a hear t rate < 65bpm , spontaneous or pharmacologically induced with - blockers . 
aec ( automatic exposure control ) was applied to adjust the tube current and maintain a user - specified noise level in the image data [ 12 , 13 ]  . 
we employed an iterative reconstruction system , the aidr - 3d , which operates in both the raw data and the image domafor each patient , the system ( phasexact ; toshiba medical systems corporation , tochigi , japan ) traced a movement diagram of the sinogram and automatically selected the phase with the least movement artifact [ 13 , 14 ]  . 
to reach the best intracoronary contrast enhancement , a circular region of interest of the bolus tracking technique ( surestarttm ) was placed in the descending aorta with a start scan threshold of 300hu . 
 the effective radiation dose of each ccta study was estimated multiplying the dlp ( dose length product ) value by an organ weighting factor for the chest as the examined anatomical structure ( k = 0.014msvmgy 1cm1 ) , according to the european working group for guidelines on quality criteria in ct [ 15 ]  . image analysis each examination was analyzed by two experienced cardiac radiologists . 
the images were evaluated by multiplanar reconstruction techniques ( mpr ) , maximum intensity projection ( mip ) and volume rendering ( vr ) , with views on the short axis , 2 and 4 chambers , analyzing one coronary segment at a time , according to the american heart association ( aha ) guidelines . the presence of plaques , number and degree of stenosis were described . 
degree of stenosis was evaluated measuring the percentage of lumen narrowing and classified as normal ( absence of plaque ) , minimal ( < 25% ) , mild ( 2549% ) , moderate ( 5069% ) , severe ( 7099% ) and occluded [ 16 ]  . the atheromatous plaques were defined as a structure > 1mm2 within and / or adjacent to the lumen of the vessel , which could be clearly distinguished from the lumen and from the surrounding pericardial tissue [ 17 ]  . the plaque density was expressed in hounsfield units ( hu ) and classified as calcified ( 1501300 hu ) , fibrous ( 61149 hu ) or fatty ( density 60 hu ) [ 18 ]  . finally , risk stratification of each patient was assessed according to the esc guidelines ( table2 ) [ 19 ]  . 
 calcium score was not assessed due to the lack of cs acquisition in all examinations . 1 3 1252 table 2 definitions of risk of ccta table 3 per - patient analysis patients with cad , no . 
 ( % ) high risk intermediate risk low risk la radiologia medica ( 2020 ) 125 : 12491259 high risk significant lesion of high - risk category ( three vessel disease with proximal stenosis , lm and proximal anterior descending cad ) intermediate risk low risk significant lesion ( s ) in large and proximal coronary artery ( ies ) but not high risk normal coronary artery or plaques only ref . 
anova test was used to investigate any correlation between cardiac event and plaque characteristics . chi - squared test was used to investigate the possible correlation between mace frequencies and cad presence assessed for different risk groups and severities of diseases , as well as for testing any correlation between risk factor and cad severity . 
univariate linear regression test was used to test the potential correlation between risk definition and severity of disease only . overall survival and mace - free survival among obstructive groups only and overall risk groups are presented using kaplanmeier survival curves and compared using the logrank test . 
 ( cad extension is summarized in table3 . ) notably , of the severe / occlusive stenoses , 16 patients had severe stenosis ( 25.8% ) , while 8 patients ( 12.9% ) with cad had occlusive stenosis ; other 10 patients with non - occlusive cad showed a three - vessel distribution , and 7 patients showed a two - vessel disease . 
of 930 segments analyzed , 290 ( 31.18% ) showed an atherosclerotic plaque . notably , our analysis showed a prevalent involvement of lma and lda ; 22 plaques ( 7.59% of total plaques ) were localized in the left main artery ( segment 5 ) , 80 plaques ( 27.59% of total plaques ) were localized in the left fig . 
the patient was referred for primary pci + stenting after 14 months 1 3 la radiologia medica ( 2020 ) 125 : 12491259 1253 table 4 per - vessel analysis table 6 per - plaque analysis : degree of stenosis plaques no . 
lipid ( 30 to 60 hu ) 173 ( 59.66% ) 110 ( 37.93% ) 7 ( 2.41% ) data are expressed in numerical value and , in brackets , in % other 3 patients reported the onset of unstable angina ; they were hospitalized for chronic heart failure ( chf ) , but pci procedure did not find a primary indication , and omt was chosen by the cardiologist as the best treatment . seven patients underwent cabg , 3 of whom were further hospitalized for chf . no non - fatal stroke or death occurred . 
however , cad is frequently misinterpreted or not recognized in these patients , and a different cv risk scoring has proved inadequate in the cv stratification risk assessment of t2dm patients [ 2327 ]  . different imaging functional stress studies such as ecg stress test , myocardial scintigraphy and stress echo may help in detecting cad , but with some limitations , varying in sensitivity and specificity , spatial resolution and dose exposure [ 2831 ]  . 
moreover , different functional studies ( pet , scintigraphy and stress cmr ) may result inadequate in the presence of a three - vessel cad [ 3234 ]  . therefore , ccta could assume a dominant role in stratifying t2dm patients , considering also the excellent capability in predicting the prognosis of cad patients , in addition 1 3 la radiologia medica ( 2020 ) 125 : 12491259 1255 fig . 
they conclude that the role of coronary cta must be further assessed in order to stratify therapy according to the presence or absence and extent of cad [ 39 ]  . in line with this recent evidence , our results show how mace could be efficiently predicted once re - assessed the individual risk of t2dm patients , according to the extension of cad , with a 7.25 - fold increased risk in patient classified as high risk ( three - vessel disease with proximal stenosis , lm and proximal lad involvement )  . the primary role of ccta as a proper predictor tool for asymptomatic t2dm patients suggests the possibility to reconsider the recommendation as a should - recommendation . however , specific considerations are needed about the prevalence of disease and its progression . our data show the lack of a time - analysis correlation between mace and obstructive disease only . 
all patients included in our study were self - referring ; this results in possible errors in their selection , also considering the high prevalence of cad in our sample of study . 
however , the careful selection of the included patients could be partially responsible for a reduction in the selection bias in our patient population . conclusion in conclusion , our study confirms that ccta is a proper stratification risk predictor when more efficient tests are needed for asymptomatic t2dm patient stratification . 
ccta may be considered necessary in the clinical setting of these patients , to reduce mortality and morbidity by promoting revascularization or adequate omt , by providing other information than the mere consideration of the degree of stenosis alone . 1 3 la radiologia medica ( 2020 ) 125 : 12491259 1257 fig . 
our study wanted to assess the difference in execution and reading time between abus and hhus . methods and materials n = 221 women were evaluated consecutively between january 2019 and june 2019 ( average age 53years ; range 2489 )  . 
 time started for both procedures when the patient was ready on the examination table to be examined to the end of image acquisition and interpretation . results no patients interrupted the exam due to pain or discomfort . 
n = 221 women underwent abus and hhus ; n = 11 patients refused to undergo both procedures due to time constraints and refused abus ; therefore , 210 patients were enrolled with both abus and hhus available . 
the average time to perform and read the exam was 5min for hhus ( ds 1.5 ) with a maximum time of 11min and a minimum of 2mthe average time with abus was 17min ( ds 3.8 , with a maximum time of 31min and a minimum time of 9min )  . 
the abus technique took longer to be performed in all patients , with an average difference of 11min ( range 323min ) per patient , p < 0 , 001 . 
in addition , we can underline that time required by radiologists is longer for abus even only considering the interpretation time of the exam . conclusion a significant difference was observed in the execution and reading time of the two exams , where the hhus method was more rapid and tolerated . keywords breast density breast cancer automated breast ultrasound handheld ultrasound average time of abus introduction mammography is the gold standard examination for breast cancer ( bc ) screening ; however , breast density has a masking effect on lesions recognition and it is considered an independent risk factor for bc . 
 abus , on the other side , is a reproducible examination , both in acquisition and reading strategy , and usually , the radiologist reports only the exam and does not perform it , so abus screening is an option proposed to overcome the time - consuming and costly nature of handheld , physicianperformed whole - breast hhus . 
usually , only abnormalities noted during scanning are documented and reported with hhus ; if an abnormality is not noted during the scanning , it is missed . multiple studies have demonstrated similar sensitivity , cancer detection rate , diagnostic accuracy rate and image quality for both abus and hhus [ 11 , 12 ]  . 
the large probe of abus provides the whole coverage and characterization of the large mass , and in the follow - up of large - sized cancer after neoadjuvant chemotherapy , it might provide an accurate measurement of a cancerous tumor larger than 5cm . in addition , abus provides better detection of architectural distortions thanks to the coronal view [ 13 ]  . 
however , abus has some limitations , such as an higher rate of false positive and recall [ 14 ] compared to hhus . in general , the feasibility and image quality of the abus are good and it has been proposed as suitable for adjunct screening for breast cancer [ 15 ]  . therefore , the aim of this study is to compare the execution and interpretation time of the manual ultrasound examination with the automatic one and to understand the advantages or disadvantages in the screening setting . materials andmethods the study was approved by the ethics committee , and informed consent was obtained from all participating patients ( 102reg2016 )  . patients n = 2221 women were evaluated consecutively between january 2019 and june 2019 ( average age 53years ; range 2489 ) , within a multicentric comparative prospective trial between tomosynthesis ( dbt ) and hhus ( nct03033030 )  . 
this survey is realized with standard investigation protocol to supine patient , with arms above the head , on the cot , by medical radiology technicians dedicated to breast radiology and specially trained . 
before starting the study , they performed a 15 - day trial period , performing about 10 abus exams on voluntary patients . the high - frequency transducer is placed on the breast and exerts a slight compression to stabilize the breast . a hypoallergenic lotion and a disposable membrane were used to aid an acoustic coupling . 
standard examination consists of three scans ( antero - posterior , lateral and medial ) each lasting 1mduring the acquisition , women were asked not to move and to breathe smoothly . for the antero - posterior ( ap ) position , the arrow of the probe was placed centering the nipple and fixed before scanning . 
for the medial position , the pod was angled with thumbs to push breast from sternum toward axilla and fixed before scanning . depending on the size of the breast ( a , b , c , d , d + ) , there is the possibility to use an additional scan to ensure the coverage of the entire breast . reference frequencies were set in accordance with cup size a = 11mhz , b = 10mhz , c = 9mhz , d = 9mhz , d + = 9mhz . 
hhus scanning was performed by separating the breast into four segments ; each segment was scanned in two planes , sagittal and axial , followed by the area of the nipple and the axilla [ 17 ]  . 
 time started for both procedures when the patient was ready on the examination table to be examined to the end to image acquisition and interpretation . a database was collected inserting patients master data , breast density , cup and execution times of both methodical . 
size : size of the breast ( a , b , c , d , d + ) discussion the sensitivity of mammography depends on breast density : increased breast density is associated with reduced mammographic sensitivity [ 1 , 2 ]  . 
however , there are several barriers to implementing screening ultrasound in practice : high rates of false positives , manpower , variability in acquisition protocols , differences in hhus usage across countries ( e.g. , us characteristic histological subtype fibroadenoma cyst dcis invasive ductal carcinoma infiltrating lobular carcinoma invasive ductal carcinoma + infiltrating lobular carcinoma histological grade high ( g3 ) intermediate ( g2 ) low ( g1 ) tumor size < 10mm 1019mm 2029mm 30mm fea flat epithelial atypia , adh atypical ductal hyperplasia , dcis ductal carcinoma insitu is performed by technologists in the usa )  . 
if performed by radiologists with sub - specialization in breast imaging , hhus is time - consuming although the number of false positive could be greatly reduced as demonstrated in the astound trial : false - positive recalls ( 2.0% ) and biopsies ( 0.7% ) were acceptably low , but possibly related to incident screens ( with prior examinations available ) [ 4 , 18 ]  . its practicability has been questioned because of the lack of standardization , operator dependence and time required by the radiologist to perform the exaon the other hand , abus is an increasingly used technique for the diagnosis of breast cancer in adjunct screening [ 9 ]  . 
in the literature , total abus execution time is about 1015min by a trained radiographer [ 21 ] and for workflow and patient continuity , having the same examiner perform the mammographic and ultrasound examinations would be optimal . 
during our study , we observed that abus executions time represents about 60% of the total time and that the interpretation time represents the remaining 40% ; with a minimum interpretation time of 4.5min and a maximum time of 11m some papers show that average abus interpretation time is 3min in women with negative ultrasound examinations [ 20 ] and 510min in women with a positive examination [ 22 ]  . 
 other studies confirm similar results ; the interpretation time of abus varies between 2.9 and 9mthe reason of this variability may be the differences in experiences , presence of abnormalities and to the filled reports or protocols [ 23 ]  . 
even if the two methods have two different workflows , from our study we can observe that time required by radiologists is longer for abus even only considering the interpretation time of the exam . in our protocol , hhus interpretation was performed with knowledge of mammography differently from abus interpretation and this may cause an increase in abus reading times . 
some papers show a correlation between the bi - rads category and the reading time of the abus exam and so automated breast ultrasound is more promising for breast screening purposes where majority of women are bi - rads category 1 [ 13 ]  . 
in addition , execution times , such as reading , should be reduced following a learning curve [ 24 ] and use of cad systems can help to reduce interpretation times [ 25 ]  . 
in our study , no differences in time at the beginning and at the end of the study was observed and this is consistent with prior research showing that reading times stabilize relatively rapidly [ 20 ]  . 
the patients gender , age , cause of cirrhosis , progression of background liver cirrhosis , lesion size / location / contrast enhancement pattern , and serum aspartate transaminase to platelet ratio index were correlated with sclerotic changes of each lesion . results according to the dynamic ct features , 36 of 57 ( 63% ) hemangiomas were determined to have sclerotic changes during the follow - up period ( 1.114.4years , median : 7.8years ) , including 28 lesions ( 49% ) reduced by 20% in diameter . 
with the exception of exophytic location free from size reduction ( p = 0.023 in multivariate analysis ) , no other analyzed factors were significantly correlated with sclerotic changes . conclusion overall , sclerotic changes of hepatic cavernous hemangioma followed the morphological progression of background liver cirrhosis , while exophytic lesions tended to be free of size reduction . keywords liver hemangioma cirrhosis computed tomography introduction other than benign cyst , hemangioma is the most common hepatic tumor that has not been shown to undergo malignant transformation [ 1 , 2 ]  . 
during surveillance for hepatocellular carcinomas * jeong - sik yu yjsrad97@yuhs.ac 1 department ofradiology , gangnam severance hospital , yonsei university college ofmedicine , 211 eonju - ro , gangnam - gu , seoul06273 , southkorea in high - risk patients , imaging studies are used to exclude hemangioma [ 3 ]  . hemangiomas can be classified as hamartomas , so most do not change in size or appearance over time [ 4 ]  . 
for instance , in a recent study involving > 5 years of follow - up , cirrhotic changes of the liver parenchyma and the aging process were identified as significant factors predicting size reduction in hemangiomas [ 7 ]  . 
one autopsy series showed that the incidence of hepatic hemangiomas in patients with cirrhotic liver was much lower than that in the general population [ 8 , 11 ]  . 
in another study , due to sclerotic changes , hemangiomas found in explanted cirrhotic vol . : ( 0123456789 ) 1 3 1226 la radiologia medica ( 2020 ) 125 : 12251232 livers were difficult to detect in preoperative images [ 8 ]  . 
 some imaging follow - up studies have reported that hepatic hemangiomas in the cirrhotic liver tend to contract , probably because of surrounding hepatic fibrosis [ 79 ]  . during our own clinical practice , we have noticed that hepatic hemangiomas in the cirrhotic liver show non - uniform volume contraction or sclerotic changes which cannot be easily distinguished from hepatocellular carcinomas at a certain time point during serial follow - up imaging studies . 
for better understanding of the time - related imaging characteristics of hepatic hemangiomas in the cirrhotic liver , the present study sought to determine the intraand extralesional factors that predict sclerotic degeneration of hepatic hemangiomas in the cirrhotic liver on long - term follow - up computed tomography ( ct ) examinations . materials andmethods patients research approval was obtained from the institutional review board of our hospital , and the requirement for informed consent was waived in this retrospective study . 
in the abdominal ct reports over a 5 - year period ( january 2005december 2009 ) in our hospitals medical record archive , a total of 93 patients were suggested to have hemangiomas in the cirrhotic liver . 
for these patients , all available ct data in the picture archiving and communication system ( pacs ) captured before and after the patient selection period were extensively reviewed by a study coordinator with a 27years experience of abdominal imaging , and the reviewed images were taken over 19years ( from january 2000 to december 2018 )  . 
hemangioma was diagnosed based on the following pre - established imaging features [ 12 ] : ( 1 ) gradual centripetal globular enhancement during multiphasic dynamic imaging until the delayed phase ( dp ) ; ( 2 ) arterial phase ( ap ) homogeneous enhancement , with or without arterioportal shunt , followed by sustained enhancement until dp , with an attenuation density similar to that of intra - / extrahepatic large vessels . 
for patients who had more than two dynamic cts taken during the follow - up period , all available cts were first preliminary reviewed , and then , initial and last cts were selected for future image analysis . 
when a hemangioma showed no more globular or early homogeneous enhancement during serial ct follow - up , it was regarded as completely sclerosed [ 13 ] , representing another end point of the observation . 
the initial or final size of the lesion , defined as the transverse diameter on portal venous phase ( pvp ) images , was required to be > 5mm , with no remarkable size increase ( > 50% size increase in 6months or less ) to suggest malignant vascular or solid tumor during the follow - up period depending on the recent li - rads criteria [ 14 ]  . 
in patients with multiple hemangiomas , up to five lesions were included for analysis ; for the patients with six or more lesions , top five lesions of the largest transverse diameter were selected . 
if patients had neither of these , they were excluded from the study , even if clinical signs suggested cirrhosis [ 8 , 15 ]  . patients with lipiodol accumulation in and around the hemangioma due to chemoembolization to treat hepatocellular carcinoma during serial follow - up were also excluded ; in these patients , the last ct before the procedure was regarded as the end point of ct examination . 
patients were excluded if they had early , homogeneously enhancing lesions on their initial ct that were indistinguishable from arterioportal shunt due to similar contrast enhancement in the pvp and dp images [ 16 , 17 ]  . 
acquisition of arterial phase scans was initiated 15s after enhancement of the thoracic aorta , until 100 hounsfield unit was reached as measured with a bolus - tracking technique after injection of the contrast material . 
all ct images were acquired in the craniocaudal direction . data analysis two radiologists ( one with 20years experience of abdominal imaging and the other a second - year radiology resident ) determined various imaging features , as well as the sclerotic change in the hemangiomas over time , as indicated by the 1 3 la radiologia medica ( 2020 ) 125 : 12251232 1227 fig . 
in the axial pvp images , in which both the enhanced and unenhanced portions are well distinguished from the surrounding liver , lesion size was measured using electronic calipers to determine the longest dimension . 
if the longest dimension of the hemangioma in the final ct was 80% of that in the initial ct image , the lesion was regarded as shrunken . each lesion was ascribed a segmental location ( s1 , s2 / 3 , s4 , or right hepatic lobe ) , and when more than a half of a lesions outer border was exposed on the liver surface , not surrounded by hepatic parenchyma on axial and coronal reconstructed images , it was considered an exophytic lesion . 
the enhancement patterns were categorized into three groups according to the speed of intralesional contrast enhancement : rapid for lesions in which more than 75% of the area was enhanced on ap images and those that were almost fully enhanced on pvp images ; slow for the lesions in which more than half of the area was not enhanced until the dp ; and intermediate for other lesions . sclerotic change was determined based on the known imaging criteria for sclerosing or sclerosed hemangiomas including geographic outline , capsular retraction , decrease in size over time , and loss of previously present regions of enhancement ( figs.2 , 3 ) [ 18 ]  . 
they compared the final with the initial ct images side by side on pacs monitors , focusing on previously established gross morphological changes of cirrhosis including atrophy of segment 4 / right hepatic lobe and hypertrophy of caudate lobe / lateral segment , progression of surface nodularity , or intraparenchymal reticulations / nodularity [ 19 , 20 ]  . 
interobserver variation was calculated , and when the two initial observers differed , a third radiologist with 10years experience in abdominal imaging reviewed 1 3 la radiologia medica ( 2020 ) 125 : 12251232 1228 fig . 
a , b in the arterial phase of initial ct ( a ) shows peripheral globular enhancement ( arrowheads ) with subsequent filling ( arrow ) of contrast material in a 1.6 - cm hemangioma in the portal venous phase ( b )  . 
c , d four - year follow - up ct shows markedly shrunken hemangioma ( arrows ) with remaining minimal contrast enhancement on arterial ( c ) and portal venous phase ( d ) images . 
a , b portal venous phase ( a ) and delayed phase ( b ) images of initial ct show gradual contrast filling - in enhancement ( arrowheads ) in a 4.8 - cm exophytic hemangioma . 
c , d the lesion is not shrunken on 9.5 - year follow - up ct , but the previously enhancing area in the posterior portion of the lesion ( arrowheads ) shows no visible contrast enhancement on portal venous ( c ) and delayed phase ( d ) images . 
from the patients medical records , the aspartate transaminaseplatelet ratio index ( apri ) values within 1week of the initial and final ct were calculated using the following equation : apri = [ ( serum aspartate transaminase / upper normal value of aspartate transaminase ) / platelet count ] 100 . statistics kappa statistics were calculated to establish interobserver variation ( 0.000.20 , slight agreement ; 0.210.40 , fair agreement ; 0.410.60 , moderate agreement ; 0.610.80 , good agreement ; 0.811.00 , excellent agreement ) to determine the morphological progression of background liver cirrhosis . 
a , b in the arterial phase of initial ct ( a ) shows a homogeneously enhancing hemangioma at the peripheral portion of right hepatic lobe combined with arterioportal shunt ( arrow ) and sustaining enhancement of the lesion ( arrow ) in portal venous phase ( b )  . 
c , d final ct shows similar appearance after 8years ( arrow ) on arterial phase image ( c ) , but there is no distinguishable lesion at the corresponding area on portal venous phase ( d ) continuous variables ( patients age , follow - up interval ) were analyzed using one - way analysis of variance combined with the studentnewmankeuls test for pairwise comparisons of sclerotic changes or size contraction . 
besides the shrunken lesions , eight more lesions ( 14% ) among the not shrunken lesions showed other imaging features to suggest sclerosing or sclerosed hemangiomas in the final images ( fig.3 ) , and a total of 36 out of 57 ( 63% ) lesions were regarded to have time - related sclerotic changes ( table1 )  . 
 exophytic location of the lesion was significantly predictive of no size reduction ( odds ratio : 0.08 ; p = 0.023 ) among the various factors on the logistic regression test . discussion with regard to the mechanism by which cirrhosis affects hepatic cavernous hemangioma , it may be possible that fibrotic changes in the surrounding hepatic parenchyma mechanically compress the lesions , which consist of variably sized vascular spaces [ 8 ]  . 
except for exophytic lesion location , which was associated with significantly less time - related size reduction , no intrinsic or extrinsic factors induced significant contraction of hepatic hemangioma in the present study , indicating that it is impossible to predict size change in individual hepatic cavernous hemangiomas , even in patients with cirrhosis . 
exophytic lesions would not be affected by mechanical compression from surrounding fibrotic liver tissue and would therefore not be subjected to this rule . meanwhile , volume contraction is regarded an indication of sclerotic changes in hepatic cavernous hemangiomas [ 18 ]  . 
 hemangiomas are supplied by hepatic arterial flow and drained through the surrounding hepatic sinusoids and / or portal venules , and the gross appearance of draining portal vein often mimics arterioportal shunt for the early enhancing hyperdynamic lesions during the dynamic imaging [ 2123 ]  . 
 this hemodynamic theory could be applied to all hepatic hemangiomas , even in the case of exophytic lesions . among the early , homogeneously enhancing small hemangiomas with sustained strong enhancement on pvp and dp , some lesions became indistinguishable from background parenchyma on pvp and dp ; except one tiny ( 0.6cm ) lesion , all other lesions showing this feature were combined with size reduction in the present study ( table1 )  . 
versus , hbv hepatitis b virus infection , c1 caudate lobe ( segment 1 ) , l23 lateral segment ( segments 2 and 3 ) , q4 quadrate lobe ( segment 4 ) , rt right hemiliver , r rapid , i intermediate , s slow , n not visualized , apri aspartate transaminaseplatelet ratio index 1 3 la radiologia medica ( 2020 ) 125 : 12251232 1231 volume averaging effect with thrombus or fibrosis in the same voxel could decrease the attenuation density of the whole lesion during pvp and dp like hypervascular solid tumors . 
in the liver with advanced cirrhosis , such finding may mimic arterioportal shunt or hepatocellular carcinoma especially for small lesions [ 16 ]  . for other intraand extrahepatic factors analyzed in the present study with negative results , we assumed that hemangiomas in the macronodular cirrhosis from chronic b viral hepatitis might be less affected by rather scanty background hepatic fibrosis than in other patients with micronodular cirrhosis with thicker and concentrated fibrotic septa [ 25 ]  . 
this may have been the reason for the lack of significant difference among the different causes of cirrhosis . considering the segmental differences of fibrotic change in the liver especially for the micronodular cirrhosis , we assumed that the segmental location could affect the prevalence of sclerotic changes in hemangiomas ; however , no such significant difference was found , perhaps because only a limited number of lesions were located in the hypertrophied caudate lobe ( s1 ) or lateral segment ( s2 / 3 ) , and the majority of subjects was cirrhosis from chronic viral hepatitis b which usually shows relatively non - segmental homogeneous fibrosis throughout the liver [ 26 ]  . although gross morphological progression of liver cirrhosis was closely related to sclerotic changes in hepatic hemangiomas , the apri as a quantitative indicator of liver cirrhosis showed no significant difference in the present study . 
like the child classification , which was not analyzed in the present study due to incomplete laboratory data , the apri comprises functional parameters and is not a direct reflector of degree of hepatic fibrosis [ 27 , 28 ]  . 
the follow - up period of each hemangioma showed no correlation with size reduction or sclerotic changes in the present study , suggesting that sclerotic change , with or without size reduction , occurred at a certain time rather than as a gradual event during long - term followup . 
there may be no correlation between the apri and sclerotic change in hemangioma because we did not know exactly when the causing hemodynamic change or hepatic dysfunction induced the sclerotic change in the target lesions during the long - term follow - up . the present study had several limitations . 
secondly , because the study had a retrospective design , no histological or quantitative imaging data were available detailing background liver fibrosis status at the time of the initial and final ct examinations . 
in the present study , after the exclusion of patients without gross morphological signs of cirrhosis in the last ct , a temporal change in liver fibrosis was only considered subjectively in order to determine the progression of cirrhosis with good agreement between the observers . 
thirdly , although the temporal progression of sclerotic changes was analyzed in the present study , hemangiomas likely already had sclerotic components in the cirrhotic background at the time of initial ct . 
finally , the follow - up period was not constant across patients , and it was not possible to determine an exact timing of hemangioma sclerosis combined with progression of background liver cirrhosis to produce any quantitative results . 
ideally , the study subjects would have normal liver at the time of the initial ct , with gradual progression of cirrhosis enabling stratification on serial follow - up ct examinations . 
however , it is not feasible to meet such conditions during clinical practice . in conclusion , the results of the present study suggest that sclerotic changes of hepatic cavernous hemangioma follow the morphological progression of background liver cirrhosis or aging of the patients . 
except the exophytic lesions showing no time - related volume reduction which is relatively free from compression effect by surrounding fibrotic liver , size change of hemangioma looks rather sporadic and cannot be predictable by any other intrinsic or extrinsic factors even in the cirrhotic liver . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
it is a particularly flexible approach to perfusion imaging as the signal intensity time course allows not only rapid qualitative assessment , but also quantitative measures of intrinsic perfusion and permeability parameters . 
we examine aspects of the t1 - weighted image series acquisition , ca administration , post - processing that constitute a dcemri study in clinical practice , before considering some heuristics that may aid in interpreting the resulting contrast enhancement time series . 
while qualitative dcemri has a well - established role in the diagnostic assessment of a range of tumours , and a central role in mr mammography , clinical use of quantitative dcemri remains limited outside of clinical trials . 
lancisi , via conca 71 , 60126ancona , italy 1 radiologia diagnostica ed interventistica , azienda ospedaliera - universitaria , asst spedali civili di brescia , p.le spedali civili 1 , 25123brescia , bs , italy 6 dipartimento di neuroscienze , imaging e scienze cliniche , istituto di radiologia , universit gabriele dannunzio , ospedale ss . 
annunziata , via dei vestini , 66100chieti , italy 7 unit operativa di radiologia , ospedale san raffaele irccs , via olgettina 60 , 20132milan , italy 8 struttura complessa di radiodiagnostica universitaria ( sod 2 ) , dipartimento di scienze biomediche sperimentali e cliniche , azienda ospedaliero - universitaria careggi , largo brambilla 3 , 50134florence , italy 9 divisione di radiologia , ieo , istituto europeo di oncologia irccs , via ripamonti 435 , 20141milan , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 12881300 1289 introduction effective tissue perfusion depends on the blood - borne delivery of molecules via the capillaries and their subsequent transport across cell membranes and interstitial spaces to the cells as well as the return pathway for the products of metabolischanges in vascularization through hypoxia - driven angiogenesis , one of the hallmarks of cancer [ 1 ] , can have a substantial impact on perfusion . 
magnetic resonance imaging ( mri ) is particularly attractive for clinical application thanks to the absence of ionizing radiation , and limited volumes of contrast agent ( ca ) necessary [ 7 ]  . 
the mri techniques applied in such investigations can generally be broken down into three families : dynamic susceptibility contrast ( dsc ) imaging [ 8 ] , arterial spin labelling ( asl ) [ 9 ] and the object of this review , dynamic contrastenhanced mr imaging ( dcemri ) [ 10 ]  . physiology oftissue perfusion anddcemri dcemri involves sequentially acquiring t1 - weighted ( t1w ) images through an organ of interest during the passage of a bolus administration of ca [ 10 ]  . 
the passage of the ca through the capillaries and its transport into the surrounding tissues lead to changes in the mr signal intensity ( si ) over the time course of the acquired images . a cascade of physiological and physical processes relates the observed signal changes to perfusion . 
 the vessels resulting from cancer driven angiogenesis lack architectural integrity and are often overly permeable , favour the passive transport of molecules between the blood and tissue [ 13 ]  . 
in fact , for mr cas that do not enter cells [ 14 ] , it is correct to refer specifically to transport between the blood plasma and the extracellular extravascular space ( ees ) a term commonly used in the dcemri literature to indicate the interstitial space [ 15 ]  . 
 a number of models exist for describing the exchange of cas between the plasma and ees , each with specific contexts and conditions for use ( see for example the reviews [ 16 , 17 ] )  . 
application of these models to dce / mri data is generically referred to as permeability mapping , whereas analyses that aim to extract maps of bv and bf are commonly referred to as perfusion mapping . 
in consideration of the relatively widespread implementation of the so - called extended tofts model [ 18 ] , we will base the definitions of permeability terms used herein upon that model . 
specifically , we examine aspects of the t1w image series acquisition , ca administration , post - processing and interpretation that constitute a dcemri study in clinical practice , before considering some heuristics that may aid in interpreting the resulting contrast enhancement time series . how todoit ca administration in early dcemri studies , it was relatively common to assume that si change due to the passage of the tracer is directly proportional to the concentration of the ca [ 4 , 17 , 19 ] , similar to ct cas [ 20 ]  . 
rather , at low to modest ca concentrations t1 shortening leads to signal increases , while at high ca concentrations signal losses due to t2 * shortening occur [ 21 ]  . 
using a ca dose sufficiently low to avoid t2 * shortening effects may simplify the analysis and interpretation of the dcemri data . the use of a power injector is recommended , and thus , the provision of venous access , loading and connection of the injector is a universal procedure prior to starting scanning . 
the decisions by regulators to limit the use of so - called linear cas [ 22 ] , all but restricts dcemri to the use of macro - cyclic cas at the lowest possible dose sufficient to ensure an adequate signal change for the intended analysis . 
in most oncology imaging , 0.10.2mmol / kg of gadolinium - based ca ( mr mammography 0.10.16mmol / kg ) can be used , delivered at a flow rate of 24ml / s , in all cases followed by a saline bolus of equal volume and flow rate [ 25 ]  . 
to aid in longitudinal comparisons , it is advisable to consistently use the same ca , as well as the same dose criteria and injection protocol [ 26 ]  . 1 3 1290 imaging acquisition if quantitative analysis is to be performed , dcemri image acquisition consists of 2 steps : baseline t1 mapping and dynamic t1w imaging . 
a 3d acquisition is generally preferred to ensure a homogeneous excitation profile across the central slices of the imaging volume in order to improve the accuracy of the arterial and tissue t1 and concentration values necessary for quantitative analysis [ 30 ]  . 
of course , if fat suppression is used for the dynamic dcemri acquisition , it must also be applied to the baseline t1 mapping scans . step 1 : baseline t1 mapping the si changes in a dcemri series depend not only on ca concentration and on the flip angle , the repetition time of the imaging sequence that the operator controls , but also on the native ( pre - contrast ) t1 of the tissue [ 31 ]  . 
a baseline t1 map , acquired before ca administration , is therefore necessary for the transformation of dcemri contrast enhancement time curves into the concentrationtime curves necessary for quantitative analyses [ 26 ]  . a number of different strategies have been proposed for t1 measurements including the variable flip angle , inversion recovery and looklocker techniques [ 3234 ]  . 
at its simplest , it requires just one acquisition using the same sequence but a different flip angle ( typically in the range 46 as opposed to the 1530 used in the dynamic acquisition ) [ 25 ]  . 
to reduce intra - patient and inter - scanner variability , it is , therefore , recommended to correct for the excitation profile by creating a deweighting map using two identical low - resolution scans : one obtained with the transmitreceive body coil and the other with the coil assembly being used for the dcemri [ 37 ]  . 
at present , this recommendation is in early clinical adoption as the pulse sequences [ 38 ] and post - processing required are not yet widely available . step 2 : dynamic t1w imaging the dynamic t1w imaging for dcemri needs to start before ca arrival in order to ensure an appropriate baseline for comparison in the dynamic series . 
for quantitative and semi - quantitative analyses on the other hand , sufficient baseline images should be obtained to ensure early saturation effects are attenuated , the arrival of contrast recognized , and noise in the time series can be estimated . temporal resolution and duration of acquisition are critical considerations for dcemri . 
ideally , the temporal resolution for quantitative analysis would be less than a second to allow the shape of the peak of contrast enhancement in an artery ( the arterial input function aif ) feeding the tissue of interest to be resolved [ 39 ]  . 
as for the duration of the dynamic series , acquisitions continuing for 810min post - injection are thought to ensure adequate return from the ees for stable estimation of all model parameters in most contexts [ 25 ]  . 
in mr mammography , between 60and 120 - s temporal resolution and 57min acquisition duration are accepted for qualitative assessment [ 27 ]  . high temporal resolution demands compromises in respect to spatial resolution and snr . 
parallel imaging has improved the balance between spatial and temporal resolution for 3d acquisitions [ 30 ]  . postprocessing the 4d volume of images generated in dcemri is problematic for interpretation due to the multiple factors that drive the temporal appearance of contrast enhancement ( see the next section )  . 
subtraction of an unenhanced image from the rest of the dynamic images , followed by maximum intensity projection to produce an enhancement movie , provides an easy means for rapidly viewing the dynamics of contrast enhancement for identification of suspicious areas [ 45 ]  . qualitative analysis based on a descriptive evaluation of the shape of the timeintensity curve in voxels , qualitative analysis takes an empirical view of the passage of ca . 
the most widely used classification of enhancement kinetics [ 46 ] considers aspects of three phases ( fig.1 ) : the rate of si increase ( fast , medium or slow ) during wash - in ( up to 2min ) after the injection of ca , the height of the maximum accumulation ( peak ) and the slope and shape of the wash - out phase ( persistent , plateau or rapid wash - out )  . 
a typical pattern of malignancy is fast , intense contrast enhancement followed by a rapid wash - out referred to as type 3 enhancement by some authors [ 47 ]  . 
1 stereotypical qualitative dcemri mammography enhancement patterns associated with different risk of malignancy in mr mammography [ 28 ] 1 3 1292 la radiologia medica ( 2020 ) 125 : 12881300 directly displaying the local signal enhancement curve is most commonly used for qualitative evaluation . semiquantitative analysis semi - quantitative or model - free ( nonparametric ) analysis uses the observed data points of the dcemri timeintensity curve to derive one or more simple numerical indices that do not have a scale in physical units [ 4851 ]  . 
the main limitation of semi - quantitative analysis is that longitudinal , intersubject or cross - scanner comparisons of dcemri can be heavily confounded by differences in factors such as volume of injected ca , heart rate , sequence timing and slice profile [ 24 ]  . 
consequently , while visual assessment is straightforward , interpretation is complicated by the lack of a physiological model defining most of the parameters [ 17 ]  . quantitative analysis quantitative or model - based ( parametric ) analysis of dcemri involves evaluating ca concentration changes in the tissue in terms of a model that considers either ( a ) bulk transport of ca in the form of perfusion mapping , or ( b ) exchange of the ca between the vascular and interstitial spaces via pharmacokinetic modelling in the form of permeability mapping . 
2 illustration of semi - quantitative descriptors of dce time curves the temporal resolution be high enough ( less than 5s per dynamic ) to support the deconvolution operation , and the temporal duration of dynamic acquisition sufficiently long ( least 7min ) so that consistent estimates of the permeability parameters can be derived [ 25 ]  . if these conditions are not met , semi - quantitative analysis is likely more appropriate . perfusion mapping perfusion mapping considers the bulk transport of the ca and yields maps of net bf , bv and their ratio , the mean transit time ( mtt ) analogous to analyses in ct [ 52 ]  . 
if pre - contrast t1 mapping has not been performed , the flow and volume values remain uncalibrated and are referred to as relative blood flow ( rbf ) , relative blood volume ( rbv )  . permeability mapping permeability mapping , on the other hand , adopts a pharmacokinetic model to describe ca exchange between the blood plasma and the surrounding ees . 
quantitative permeability mapping in the presence of ca leakage requires measurement of the baseline t1 , rescaling of contrast enhancement time series of images into concentrations time series , and identification of an arterial input function ( aif )  . 
the commonly used extended tofts model is a simple 2 - compartment model describing bi - directional ca exchange between the blood plasma and ees [ 18 ] as illustrated in fig . 
four variables are involved : ktrans , kep , ve and vp , one of which , kep , can be expressed as a function of two others ( kep = ktrans / ve )  . 
examples of the semi - quantitative and quantitative pharmacokinetic modelling dcemri results obtained in two prostate imaging studies , using the protocol in table1 , can be seen in fig.3. arterial input function an image voxel represents a volume of tissue that contains a large number of capillaries . 
upper : normal enhancement pattern in a patient with a pi - rads v2.1 score of 1 , with no suspicious findings in the peripheral and transition zone visible on a t2 - weighted , b calculated b1500 images and c the corresponding adc map . 
the transition zone exhibits strong enhancement seen in d wash - in , e iauc , f per , g ktrans and h kep , but the i ve does not show particular difference between the zones . 
lower : patient with pi - rads v2.1 score 5 lesion in the transition zone , presenting j hypo - intensity on the t2 - weighted image , k hyperintensity on the calculated b1500 image , and l associated low adc . 
the suspect area shows no sign of either pathological perfusion ( m wash - in , n iauc and o per ) or permeability ( p ktrans , q kep , r ve ) alterations the arriving bolus ( the arterial input functionaif ) and the spreading experienced byan idealized short bolus passing through the voxel ( called the residue function ) that results in the observed ca concentrationtime curve of the voxel [ 39 ]  . 
in practice , the concentrationtime curve of an upstream artery as the aif is used in calculating the inverse 1 3 1294 la radiologia medica ( 2020 ) 125 : 12881300 resolved in the image , and at the same time , it must be sufficiently close to the tissues to avoid bolus dispersion during the transit from artery to voxel [ 55 ]  . 
while mathematical approaches have been proposed for reducing this latter effect [ 56 ] , dealing with the other issues affecting selection of vessels for aif definition remains a concern for operators . 
despite these biases , the population - based aifs have been found to perform at least as well as aifs derived from the individual patients , leading to their general acceptance for clinical and trial use [ 26 , 58 , 59 ]  . towards aninterpretation heuristic forquantitative dcemri for reference , the essential quantities described for semiquantitative and quantitative analyses are summarized in table2 . 
for a diffusible ca , the residue function can then be used in calculating perfusion and permeability parameters . as for injection protocol , it is important for longitudinal studies that the method of defining an aif be consistent between exams . 
this operation is used in pharmacokinetic modelling as well as the analysis of perfusion mapping data for diffusible cas 1 3 la radiologia medica ( 2020 ) 125 : 12881300 1295 table 2 summary of semi - quantitative and quantitative parameters in dcemriand their implications for qualitative appearance semi - quantitative parameters auc relative signal intensity wash - in rate wash - out rate peak enhancement ratio ( per ) tmax or time to peak ( ttp ) maximum intensitytime ratio quantitative parameters area under the timeintensity curve st / s0 maximum or average slope in the initial enhancement maximum or average slope in the wash - out phase ( smaxs0 ) / s0 time from contrast arrival to peak per / tmax quantitative analysis based on the 2 - compartment modified tofts pharmacokinetic model treats the enhancement as being generated by the combination of a central compartment consisting of the extracellular intravascular volume fraction ( blood plasma ) and a peripheral compartment formed by the extracellular extravascular space ( ees ) characterized by the following parameters : ktransthe volume transfer constant from the vascular space to the ees ( min1 ) ; it is an independent parameter and reflects the sum of all processes ( predominantly blood flow and capillary leakage ) that determine the rate of gadolinium influx from plasma into the ees vethe volume fraction of the ees per unit volume of tissue ; it is an independent parameter and a dimensionless number between 0 and 1 . 
so , an increase in kep may reflect an increase in ktrans , a decrease in ve , or both fflow of whole blood per unit mass of tissue , it represents the among of plasma distributing to the tissue . 
in many lesions , this variable is small and inconsequential , but in highly vascular tumours , its contribution to total signal may be 10% or more and cannot be ignored implications for qualitative appearance direct connections exists between ktrans , ve , kep , vp and the appearance of the signal ( concentration ) versus time curves of various tissues , that can be expressed , as follows ktrans correlates with the initial slope ( wash - in rate ) of the timeintensity curve ve correlates with the peak height and with time to peak ( tmax ) of the timeintensity curve kep controls the shape of the curve , reflected in the relative contributions of its independent components ktrans and ve vp , if small , has little effect on the curves , if large , results in a faster upslope , higher and earlier peak height , and faster wash - out of mdc , having more resemblance to the arterial input function st mr signal intensity at time t , s0 pre - contrast signal intensity , smax maximum signal intensity to baseline . 
the bf determines how quickly the available vessels fill with ca , and thus is strongly tied to the rate of enhancement , that is , the steepness of the upslope in si ( fig.6b ) [ 11 ]  . 
the bv determines the maximum quantity of ca that can be present in the voxel , and so the peak si for a blood - pool ca scales with bv ( and consequently vp ) as seen in fig.6c. 
different vessel lengths encountered by the ca passing through a voxel , on the other hand , are associated with broadening of the peak relative to the upstream input function . 
the ratio bv / bf describes the average time ( mean transit time ) spent by a molecule of ca passing through the vessels in the tissue [ 11 ]  . 
with a sufficiently short , concentrated bolus , a second smaller peak may be seen , caused by recirculation of blood carrying ca that has passed through the circulatory system re - enters the arterial inflow [ 23 ]  . 
gradually , the ca is eliminated ( typically via renal excretion ) and its concentration in the blood , and dcemri signal , return to baseline over the course of minutes to hours [ 23 ]  . diffusible cas in practice , and particularly in the presence of pathology , mr cas do exchange between the blood plasma and ees to varying degrees . 
passage of the ca from the blood plasma to the ees is driven by passive diffusion with a rate constant ktrans , dependent on the type of contrast ( size and charge of the molecule ) and the state of the vascular wall endothelium [ 60 ]  . 
the difference in concentrations between the plasma and the ees ( cpce ) and the respective volumes of these compartments ( vp and ve ) also figure in determining the overall concentration in the voxel [ 18 ]  . 
6 illustration of timeenhancement curves for a blood - pool ca ( seen as white ) through the vessels ( white traces ) contained within a voxel ( black square ) after subtraction of baseline signal during dcemri ( time moving up to right )  . 
a timepoints : a baseline signal ; barrival of the ca raises signal above the baseline noise ; signal rises during wash - into a maximum ( c ) when vessels are filled by the bolus with a plateau until the tail of the ca bolus arrives at the inlet ( d )  . 
ewash - out of the first - pass of ca ( dotted line ) is accompanied by a signal intensity drop , but recirculation ( dashed line ) prevents immediate return to baseline . 
b if the blood volume is unchanged relative to the situation in a ( grey curve ) , an increase in blood flow will fill the vessels of the voxel more quickly and the plateau will be shortened ( black curve )  . 
c if the blood flow is unchanged relative to the situation in a ( grey curve ) , an increase in blood volume will result ( black curve ) in more ca being in the voxel leading to a higher peak enhancement ( peak height relates to blood volume )  . 
the mtt being the ratio of bv / bf thus increases 1 3 la radiologia medica ( 2020 ) 125 : 12881300 1297 illustrative cases ( fig.7 ) to summarize the general effects of the individual permeability parameters [ 10 , 23 , 32 , 33 ]  . 
the difference in behaviour of cp that can arise between diffusible and non - diffusible ca passage must be kept in mind to recognize possible confounds when visually assessing the contrast enhancement time curves for a diffusible ca . vp : plasma volume gradually drives cp towards zero . 
for moderate kep ( analogous to permeability limited ktrans ) , there will be a more prolonged wash - out . as for bv with intravascular cas , increasing vp ( fig.6c ) increases the fraction of the voxel containing the highest concentration of ca during first passage . 
however , in many situations , vp is not sufficiently elevated to influence the curve shape significantly , in which case , the dominant effect is due to contrast uptake into the ees . ktrans : transfer constant as with the blood - pool agent , the initial slope of the timeintensity curve reflects the rate of arrival of ca via plasma blood flow . 
for a diffusible ca however , once the leading edge of the bolus has started to leave the voxel , the part of the ca remaining in the ees will contribute to the overall signal and ca will continue to enter the ees seeking to establish an equilibrium with cp [ 23 ]  . 
in the case of low ktrans , the passage of ca into the ees is permeability - limited ( fig.7a ) and the concentration in the ve will take longer to reach equilibrium with that in the plasma . 
when ktrans is sufficiently low ( particularly if ve is also low ) the gradient between cp and ce after first passage of the bolus may allow extravasion to persist until sufficient ca has been cleared from the blood to reverse the gradient ( steady slow enhancement )  . 
the ca effectively mixes with the ees during first passage , resulting in rapid intense enhancement , with a maximum that reflects ve . it is worth noting that ktrans is not the same as permeability , but rather reflects the combined effect of plasma blood flow , permeability and capillary surface area . 
excretion of the ca over time ve : extravascular extracellular volume as the volume of the compartment that receives ca from the blood plasma , ve determines the maximum possible peak height of the signaltime curve over and above that obtained by filling vp with ca . 
for a given , low ktrans ( see discussion of permeability - limited ktrans above ) higher ve lesions may not reach equilibrium , and thus , the maximum enhancement observed will be a fraction of that possible . 
in consequence , not only are there a wide variety of combinations of the above phenomena seen invivo , it is also possible that different combinations lead to nearly indistinguishable enhancement curves . conclusions qualitative dcemri has a well - established role in the diagnostic assessment of a range of tumours , with a central role in mr mammography . 
quantitative dcemri , on the other hand , has a well - established experimental basis , but clinical use remains limited outside of trials despite the promise it shows in tumour assessment , characterization and prediction of treatment response . 
the growing use of antiangiogenic drugs to supplement conventional therapies , and the radiomic assessment of perfusion and permeability maps may be a stimulus for wider clinical used as a noninvasive biomarker of angiogenesis . 
the recent publication of proposals for standardized acquisition and analysis protocols [ 4 ] should be seen as an opportunity to consolidate clinical practice on similar protocols and practices . 1 3 la radiologia medica ( 2020 ) 125 : 12881300 1298 fig . 
7 diffusible cas typically used for mri are limited to the vascular plasma ( vpwhite traced regions in lower left ) and the extravascular extracellular space ( veupper and lower segments in lower left )  . 
a permeability - limited transport ( black curve ) describes the situation where ktrans is sufficiently low that the concentration in the ve remains well below that of vp during first passage . 
relative to the blood - pool case ( grey curve ) , the signal enhancement is increased , but a plateau is not reached and the wash - out stage lasts longer . 
b perfusion ( or flow ) - limited transport ( black curve ) describes the situation where ktrans is high , and the concentration in the ve rapidly approaches that of the vp . 
in the perfusion - limited case ( fine solid line ) , the signal contribution from the ees ( dotted line ) rises quickly but on completion of first passage drops quickly to form an upper limit to the permeability - limited enhancement of the same ve ( dashed curve )  . 
cxrs were rated as positive ( cxr + ) or negative ( cxr ) , and features reported included presence and distribution of airspace opacities , pleural effusion and reduction in lung volumes . 
the blr confirmed as significant predictors only lactate dehydrogenase ( ldh ) , c - reactive protein ( crp ) and interval between the onset of symptoms and the execution of cxr . 
the presence of two out of three of the above - mentioned predictors resulted in cxr + in 92.5% of cases , whereas their absence in 7.4%. conclusion cxr has a low sensitivity . 
ldh , crp and interval between the onset of symptoms and the execution of cxr are major predictors for a positive cxr . keywords chest x - ray coronavirus disease 2019 ( covid - 19 ) severe acute respiratory syndrome coronavirus 2 ( sarscov - 2 ) real - time reverse transcriptase - polymerase reaction chain test ( rt - pcr ) laboratory test sensitivity introduction coronavirus disease 2019 ( covid - 19 ) is caused by severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 )  . 
 however , the multinational consensus statement from the fleischner society stated that ct scan should not be used for screening or as a first - line test for the diagnosis of covid19 [ 5 ] , also because the use of a non - dedicated scanner ct requires time - consuming and laborious decontamination procedures to limit the risk of cross infection [ 6 ]  . 
in this light , chest x - rays ( cxr ) can be considered as an alternative to ct , also for the easy and fast cleaning of the equipment vol . : ( 0123456789 ) 1 3 1272 la radiologia medica ( 2020 ) 125 : 12711279 and the large availability of portable units . 
in northern italy , the epicenter of the italian sars - cov - 2 pandemic , some emergency departments use cxr as the first line of triage in patients with suspected covid - 19 also because of the relatively long waiting time for rt - pcr . 
although , the common opinion is that cxr may not be sufficiently sensitive for the detection of covid - 19 lung disease especially in the early stages of the pathology , there are only a few studies in the literature assessing its sensitivity in respect to the current diagnostic gold standard , rt - pcr [ 712 ]  . 
furthermore , no pertinent information is available concerning the association of cxr findings with clinical and laboratory data . we considered the issue worth of further exploration and planned a study aimed to assess the reliability of cxr compared to rt - pcr in symptomatic patients with positive covid - 19 confirmed by rt - pcr . 
the secondary aim was to describe cxr findings in the context of demographics characteristics , comorbidities , and clinical / laboratory characteristics associated with positive and negative cxr . clinical andlaboratory data the demographic data , comorbidities , clinical and laboratory data of the patients were collected in accordance with the structured report released by the societ italiana di radiologia medica e interventistica ( sirm ) [ 13 ]  . 
as for comorbidities , variables included in the analysis were : presence of cardiac disease , diabetes , obesity , hypertension , smoke history , acei / sartan or fans therapy . 
as for clinical data : fever , cough , rhinitis , dyspnea , pharyngodynia , myalgias , asthenia , conjunctivitis , headache , nausea , vomit and diarrhea . regarding laboratory data : white blood cells ( wbc ) count , c - reactive protein ( crp ) , lactate dehydrogenase ( ldh ) , hepatic enzymes , creatin kinase ( ck ) , bloods ph and arterial partial pressure of carbon dioxide ( paco2 )  . 
rtpcr protocol : extraction with qiasymphony dsp virus / pathogen midi kit , amplification with seegene allplextm 2019 - ncov assay ( target genes e , n , rdrp )  . materials andmethods image acquisition andanalysis study design andpopulation the study was piloted in agreement with the 1964 helsinki declaration and its later amendments , was approved by the institutional review board . 
all cxr studies were analyzed by two observers ( mc and mg with more than 5years experience ) using a picture archiving and communication system ( pacs ) workstation [ carestream vue pacs v11.3.4 ( carestream health , inc , rochester , ny ) ]  . 
categorical variables were presented as absolute numbers and percentages . the univariate analysis used nonparametric tests : for 2 independent continuous variables the mannwhitney test , for categorical variables the 2 test ( with yatess correction for 2 2 tables ) or fishers exact test . 
binary logistic regression ( blr ) was run on variables determined as significant by the univariate analysis . continuous variables with significant differences were dichotomized by the roc curve procedure to derive the regions with the strongest association with cxr +  . 
the thresholds were obtained through three methods : maximization of the harmonic mean of sensitivity and specificity and of youdens index and minimization of the distance from the upper left corner . 
the cxr findings are summarized in table2 . the study sample of 260 patients with covid - 19 confirmed by rt - pcr were subdivided in two groups : 159 patients with positive cxr ( cxr + ) and 101 patients negative cxr ( cxr )  . 
regarding comorbidities , the presence of hypertension ( p = 0.0002 ) and a concurrent treatment with sartans ( p = 0.03 ) were more frequent in cxr +  . 
among clinical data , dyspnea ( p = 0.01 ) , myalgia ( p = 0.004 ) and a longer interval between the onset of symptoms and the execution of cxr ( p = 0.0002 ) were typical of cxr +  . 
 the blr applied to the dichotomized variables confirmed their significant value as prognostic role ( table5 )  . the presence at the cxr of all three predictors was associated to a positive cxr in 95.3% of cases , the presence of two of them to 89.2% , of one to 40.7% , and their absence to 7.4%. 
figure4 illustrates two cases without ( a and b ) and two with ( c and d ) predictor factors ( table6 )  . discussion our study investigated the role of cxr in patients with covid - 19 and its association with clinical and laboratory data . 
the main findings may be summarized as follow : cxr when compared with rt - pcr has a sensitivity of 61% ( 95%ci 5567% ) and , when positive , it usually shows the presence of bilateral airspace opacities with peripheral distribution and predominant involvement of the lower lobes . several clinical and laboratory data are associated with the outcome of cxr . 
the most significant ones ldh and crp time interval between the onset of symptoms and the cxr . to the best of our knowledge , there are only seven papers in the literature , excluding case reports and case series , la radiologia medica ( 2020 ) 125 : 12711279 evaluating the sensitivity of cxr in covid - 19 patients . 
 [ 8 ] , relative to patients admitted to urgent care centers , therefore likely to have a lower grade pathology , and the higher value reported by schiaffano etal . 
overall , the cxr is characterized by relatively low sensitivity in the identification of pulmonary alterations of covid - 19 . as for radiological findings , according to recent literature data , our study described a scenario superimposable on the one described for ct with the presence of peripherally distributed , bilateral opacity with prevalence in the lower lobes [ 14 , 15 ] and low incidence of pleural effusion . regarding relationship with clinical symptoms both univariate and multivariate analysis of our sample of patients underlined a significant difference between cxr + and cxrin the time elapsed between the onset of symptoms and the execution of cxr ; in particular patients who had a negative result performed cxr at a median of 4days after the onset of symptoms , about 3days sooner than the patients with positive cxr . the covid - 19 patients are known to have a dynamic radiological pattern which varies with their clinical evolution . 
this means that our cxr patients , who had a median interval of 4 ( 17 ) days between initial symptoms and crx , were in the early stage of the disease , characterized by the presence of ggo , which may be extremely difficult to detect on cxr [ 16 ]  . 
 [ 9 ] showed that among the laboratory parameters that assessed inflammation and cell damage , crp and ldh were significantly higher in patients with a severe disease than in patients with a non - severe disease and thus appeared to have a prognostic impact . a recent study [ 19 ] found that ldh can be recognized as an important predictive factor for severe covid - 19 manifestations . 
it must be emphasized that during the 2009 influenza a ( h1n1 ) pandemic , 77.8% of patients whose laboratory data indicated elevation of ldh , had lung involvement , suggesting that ldh elevation was associated with multiple pathogenic factors including viruses , and was important to lung injury [ 20 ]  . 
 [ 19 ] recently demonstrated that elevated ldh values were associated with the risk of developing severe disease ( sixfold increase ) and mortality ( 16 - fold increase )  . crp level significantly increases in covid - 19 patients due to inflammatory reaction and tissue destruction . 
in addition , crp values in other viral diseases , such as h1n1 influenza , were higher for patients with a serious history of the disease [ 23 ]  . according to our results , ldh and crp are major predictors of a positive cxr : in presence of both values above the respective threshold of 30mg / l and 500u / l respectively , the cxr is positive in about 90% of the patients . 
 [ 9 ] on the higher frequency of positive cxr in patients with a more severe disease . the overall scenario of our findings suggests that baseline cxr , when integrated with laboratory evaluations , can have a role in the identification of patients with more severe involvement of the pathology . 
to this end , an added value comes from the promising artificial intelligence techniques developed for improving the diagnostic accuracy of imaging and assisting radiologists and clinicians in the cxr evaluation as part of the covid - 19 triage process [ 24 ]  . 
the results of our study should also warn that when dealing with the suspicion of a positive covid - 19 in a patient admitted to the emergency room a few days after the onset of symptoms and without severe alterations of crp and ldh , physicians should not be surprised to be faced with a negative cxr . this study has some limitations . 
95%cis completely above 1 correspond to positive effect on cxr + ; completely below 1 correspond to adverse effects ; including 1 to randomity to address a differential diagnosis with classical community - acquired pneumonia , in which the alterations become manifest in the cxr within a time interval of 12h from the beginning of the symptomatology [ 17 ]  . regarding laboratory data , a marked reduction in lymphocytes and elevation of the concentrations of crp , ldh and hepatic enzyme are often observed in covid - 19 patients . 
the chest x - ray resulted positive with neither peripheral nor perihilar airspace opacification with middle and lower zone involvement it to a non - covid - 19 control group . 
third , we did not correlated the outcome of cxr with the clinical outcome and this should be the goal of further prospective studies that effectively assess the additional role of cxr in patients with suspected sars - cov - 2 infection . in conclusion , the baseline cxr performed on 260 patients with covid - 19 confirmed by rt - pcr has a sensitivity of 61.1% with a typical presence of bilateral airspace opacification more often with a lower zone and peripheral distribution . 
among demographic characteristic , comorbidities , clinical and laboratory data , ldh > 500 u / l and crp > 30mg / l and an interval between the onset of symptoms and the execution of cxr of more than 4days are the major predictors for a positive cxr . 1 3 1278 la radiologia medica ( 2020 ) 125 : 12711279 table 6 comparison among studies on cxr sensitivity in covid19 patients no . 
san luigi gonzaga di orbassano . funding open access funding provided by universit degli studi di torino within the crui - care agreement . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethics approval this study was reviewed and approved by the ethics committee of our institution . informed consent the requirement for informed patient consent was waived . 
patients information was anonymized prior to the analysis . availability of data and material all data are available on request at the department of surgical sciences , radiology unit , citt della salute e della scienza hospital , university of turin , via genova 3 , 10126 , turin , italy . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
the remaining 7080% tumors are renal cell carcinomas ( rcc ) , of which 7580% are clear cell ( ccrcc ) , 720% are papillary ( p rcc ) and 5% are chromophobe ( chrcc ) subtypes [ 4 ]  . current treatment options for all small renal masses include radical nephrectomy , nephron - sparing partial nephrectomy or thermal ablation ; since a safe differential vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 12801287 1281 diagnosis between benign and malignant tumors by imaging ( ct or mr ) is very difficult , many patients are subjected to an unnecessary surgery [ 2 ]  . renal oncocytoma ( ro ) is composed of oncocytes originating from the so - called intercalated cells of the collecting ducts [ 5 ]  . 
ro is typically described to be a hypervascular , homogenous mass with well - defined margins , without hemorrhage or calcification , that may contain a central stellate scar on ct . 
moreover , though the central stellate scar is a characteristic finding of oncocytoma , which is seen in one - third of cases , it is an unreliable feature to differentiate ro from rcc , because areas of necrosis inside the rcc can mimic a central scar [ 2 ]  . some studies reported the ct segmental enhancement inversion ( sei ) pattern on biphasic mdct is highly sensitive and specific for the diagnosis of renal oncocytomas smaller than 4cm [ 7 , 8 ]  . 
however , other investigators have reported that sei seems not to be useful for the diagnosis of ro with ct or mri [ 9 ]  . currently percutaneous biopsy may not always confirm the preoperative diagnosis , since histopathological differentiation of ro from rcc may be difficult in small tissue samples [ 6 ]  . in view of the benign course and excellent prognosis of patients with ro , active surveillance has been increasingly adopted as a treatment strategy [ 10 ]  . 
thus , it would be helpful to have a diagnostic algorithm to differentiate more confidently ro from rcc . the purpose of this study is to investigate retrospectively whether small oncocytomas can be differentiated from rccs on ct images on the basis of their enhancement patterns . materials andmethods study population radical nephrectomy . 
three clear cell rccs were diagnosed by percutaneous biopsy before surgery . ct examination all the ct examinations were obtained using a 128 - detector row scanner ( somatom definition flash siemens )  . 
all patients were instructed not to breath during ct scans to prevent motion artifacts . an intravenous injection of 1.5mlkg1 of nonionic contrast material ( iomeron 350 ; bracco diagnostics , milan , italy ) , followed by 40ml of saline solution , was administered through an 18 - gauge needle in the antecubital vein , using a semi - automated power injector , at a flow rate of 3ml / s . 
 all patients underwent multiphase contrast - enhanced ct , which included images in four phases ( plain , corticomedullary , nephrographic and excretory )  . the corticomedullary phase was defined as bright enhancement of the renal cortex and minimal enhancement of the renal medulla . 
fifty - seven patients underwent partial nephrectomy and 19 patients ct images were independently reviewed by a radiologist and a resident in radiology , with 7 and 3years of experience , respectively . maximal lesion diameter ( cm ) , margins ( well - defined / irregular ) , pole ( upper / middle / lower ) , location ( exophytic / endophytic ) , central scar , calcifications , macroscopic fat , angular interface sign , enhancement ( homogeneous / heterogeneous ) , vascular invasion and perirenal fat invasion were independently assessed by two reviewers who were blinded to the histological subtype of the tumor . a central scar was defined as a central stellate hypodensity in corticomedullary phase with progressive enhancement in nephrographic phase [ 11 ]  . 1 3 1282 la radiologia medica ( 2020 ) 125 : 12801287 the presence of macroscopic fat in the renal lesion was confirmed by attenuation value of less than 30 hu in unenhanced phase . angular interface sign is defined as pyramidal interface between exophytic renal mass and the renal parenchyma , with a definable apex within the parenchyma and an exophytic bulging of the mass beyond the renal capsule [ 12 ]  . the enhancement homogeneous or heterogeneous of renal lesion was subjectively assessed . circular regions of interest ( rois ) were drawn in the same slice both in tumor lesion and in the adjacent renal cortex , and ct attenuation values ( hounsfield units , hu ) were evaluated in the unenhanced , corticomedullary , nephrographic and excretory phases . 
the rois were positioned as large as possible , using the same size for each phase at the same site , excluding necrotic or cystic areas , bleed and calcification within the solid tumor lesion . to reduce a possible bias of the measured attenuation by technical or patient variability , absolute values were normalized by using the relative enhancement ratio ( the ratio of lesion to normal cortex attenuation , l / c )  . the two reviewers also placed a roi in the abdominal aorta on the same axial image slice ( avoiding measurements of calcifications in an atherosclerotic aorta ) to calculate the aortalesion attenuation difference ( alad ) in corticomedullary , nephrographic and excretory phases . statistical analysis descriptive statistics were used to summarize the patients baseline demographic characteristics and tumor characteristics . 
univariate analysis was performed to compare tumor radiologic features between ros and clear cell rccs and between the ros and chromophobe rccs . comparisons between the categorical variables were tested using the pearson chi - square or fisher exact probability test . 
l / c ratio was 1 on corticomedullary phase and 0.92 on nephrographic phase ro is the most common benign solid renal lesion with an overall incidence of 37% [ 5 ]  . 
 several studies [ 11 , 12 ] have described ct features that may help to differentiate ro from rcc ( i.e. , well - defined margins , homogeneous enhancement , central scar ) , even 1 3 la radiologia medica ( 2020 ) 125 : 12801287 1285 fig . 
l / c ratio was 0.56 on corticomedullary phase and 0.68 on nephrographic phase if none of these seems to be diriment because of the high overlapping between the different tumor histotypes . 
they reported that l / c attenuation , during the corticomedullary phase , was highest for oncocytoma ( 1.05 ) followed by clear cell ( 0.63 ) and chromophobe ( 0.45 ) , but the difference did not reach a statistical significance in distinguishing ro to clear cell rcc , compared to our study . 
additionally , the authors found that the percentage of washout was highest for ro followed by clear cell , chromophobe and papillary rcc [ 6 ]  . in our study , as in the study of mazzei etal . , ro presented a wash - in similar to renal cortex and clear cell rcc had a lower enhancement than ro during any given phase [ 16 ]  . on the contrary , results of our study are in disagreement with those of ren etal . 
they reported that l / c attenuation in the corticomedullary phase was significantly higher than the cutoff value of 1.0 in most rccs and lower than 1.0 in most ros ; thus , rccs showed a significantly higher degree of enhancement than ro in the corticomedullary phase . 
also found that in nephrographic phase the l / c attenuation was higher than in the corticomedullary phase in most ro , showing a prolonged enhancement pattern [ 17 ]  . 
 ( 21 ro and 25 clear cell rccs vs 14 ro and 32 clear cell rccs , respectively )  . another parameter that has been evaluated for diagnosing renal tumor in ct is alad . 
they reported that a alad threshold 1 3 la radiologia medica ( 2020 ) 125 : 12801287 1287 of > 17 hu in nephrographic phase was 93% predictive in discriminating clear cell rcc from oncocytoma [ 19 ]  . considering the alad , in our study , we found only a difference between ro and clear cell rcc , on the edge of statistical significance , in nephrographic phase ; however , the accuracy for discriminating the two tumor histotypes is essentially inadequate . 
we did not find any significant difference between chromophobe rcc and ro , considering alad ; however , the low number of chromophobe rcc ( n = 7 ) may have influenced the results . some limitations of our study should be noted . 
surely , more evidence could come from a multicenter , prospective study . conclusions in conclusion , this study demonstrated that the l / c attenuation in corticomedullary phase seems to be useful for differentiating ro from clear cell rcc . 
technical success , drainage catheter removal , jaundice remission , early and late complications , stent patency , and overall survival were analyzed . results the stent was successfully deployed in all patients . 
two cases ( 20% ) experienced early complications ( bile duct hemorrhage and cholangitis ) and two cases ( 20% ) experienced late complications ( hepatic abscess and cholangitis )  . 
in order to relieve hilar trifurcation stenosis , stent - in - stent and side - by - side deployment techniques have been developed for the percutaneous placement of tor y - configured bilateral stents , but each technique has disadvantages . 
during the stent - in - stent deployment procedure , the second stent is inserted into the first one , which may lead to the first stent becoming loose and losing lateral supporting force . 
moreover , the sparse metal mesh of the stent allows for more tumor ingrowth , and if reocclusion occurred , it is difficult to be treated by inserting another stent . 
in order to solve the above - mentioned problems , we previously vol . : ( 0123456789 ) 1 3 1000 la radiologia medica ( 2020 ) 125 : 9991007 proposed a y - configured sems with two improved designs [ 4 ]  . 
firstly , instead of using the conventional tubular stent , an l - shaped stent made with a wire diameter of 0.16mm was fabricated to improve the lateral force of support . 
this novel y - configured sems ( consisting of an l - shaped main stent and a micro - bellshaped stent ) was deployed using a stent - in - stent technique with a dual percutaneous approach and was demonstrated to be feasible and effective for hilar biliary obstruction [ 4 ]  . 
 however , this y - configured sems was uncovered , making it technically difficult to pass the guidewire and catheter through the fenestration in the mid - section of the l - shaped main stent during stent placement . 
the technical and clinical feasibilities of this partially covered t / yconfigured sems were evaluated in patients with malignant biliary obstruction . consistent with a diagnosis of biliary obstruction with jaundice ; ( 3 ) preoperative abdominal computed tomography ( ct ) or magnetic resonance imaging / magnetic resonance cholangiopancreatography ( mri / mrcp ) indicating obstructive jaundice ; ( 4 ) a diagnosis of malignant pathology or a known malignant histology from a previous surgical operation ; and ( 5 ) bismuth type ii or higher . 
the exclusion criteria included portal vein tumor thrombus , severe blood coagulation dysfunction , and massive ascites . device the newly designed partially covered sems ( micro - tech , nangjing , china ) used in this study consisted of two parts ( fig.1a ) : a l - shaped angle main stent ( 810mm in diameter ) and a limb stent ( 810mm in diameter )  . 
the midsection of the main stent was partially covered ( 2030mm in length ) and had a circular fenestration of 810mm in diameter ( as indicated by the long arrow in fig.1a ) , which was determined to be the appropriate size facilitating the insertion of the tubular limb stent into the main stent . 
the size of the introducer sheath for the stent was 6f . materials andmethods procedure patients this prospective study was approved by the institutional review board of the first affiliated hospital of zhengzhou university ( registration number was chictroon - 15006655 ) , and written informed consent was obtained from each patient . 
c lateral fluoroscopic image of the sems with radiopaque markers made of gold ( short arrows ) 1 3 la radiologia medica ( 2020 ) 125 : 9991007 1001 fig . 
for the single hepatic approach , the temporary 8.5f drainage tube was exchanged for an 8f short sheath ( cook inc . , usa ) , through which two guidewires were inserted into the contralateral biliary branch and common biliary duct ( cbd ) , respectively . 
thirdly , after withdrawing one guidewire , another one was passed through the fenestration into the cbd , the guidewire to the cbd was carefully withdrawn and the cbd was brought to pass via the fenestration , which was easier than in our previous study because of the partial covering design . 
cholangiography was performed 2weeks after the sems placement , and the temporary 8.5f drainage tube was removed if stent patency was confirmed . all patients underwent outpatient and telephone followup one month after stent placement and then every three months until november 2017 or until death from any cause . 
 serum total bilirubin was measured before stent placement and at one - month post - follow - up . study endpoints anddefinitions the following endpoints were assessed : ( 1 ) technical successdefined as successful deployment of the newly designed tor yconfigured stent ; ( 2 ) jaundice 1 3 1002 la radiologia medica ( 2020 ) 125 : 9991007 fig . 
f ct showed full expansion of the stent 2weeks after the placement remissiondefined as an obvious decrease of serum total bilirubin level ( below 75% of the preoperative level ) within four weeks after sems placement ; ( 3 ) procedure time defined as the time interval from local anesthesia to the placement of the temporary 8.5f biliary drainage catheter ; ( 4 ) complicationsclassified as early ( within 30 days after biliary stenting ) and late complication ( > 30 days after biliary stenting ) according to the society of interventional radiology clinical practice guidelines [ 5 ] ; ( 5 ) stent patencydefined as the time interval from the initial stent placement to recurrence of biliary occlusion ( symptoms of jaundice with serum total bilirubin twofold increases and detection of bile duct dilatation on medical imaging ) ; and ( 6 ) overall survivaldefined as the interval from initial biliary stenting to death due to any cause . statistical analysis all data were summarized as mean standard deviation ( sd ) and range , unless specified otherwise . 
5. discussion in this study , we evaluated a newly designed partially covered y / t - configured sems for biliary trifurcation stenosis in ten patients with bismuth type ii - iv tumor , and the results supported the technical and clinical feasibility of this sems approach . 
this design was expected to increase the capacity of the stent in terms of resistance to local compression and benefit patients receiving adjuvant brachytherapy or external irradiation . we deployed the sems using a stent - in - stent technique , which is the most widely used approach to treat hilar biliary obstruction . 
a potential problem of this technique , however , is the risk of secondary occlusion due to impaired bile flow at the overlapping area where the second stent is partially inside the first stent . 
we previously invented an uncovered y - configured sems consisting of a l - shaped main stent and a micro - bell - shaped limb stent using the stent - in - stent technique [ 4 ]  . 
 in addition , because this design prevented the limb stent from excessively inserting into the main stent , removal of the stent and re - deployment for patients with restenosis would be technically easier . this partially covered design was adapted from a previous study by gwon di etal . 
 [ 12 ] , who first reported the deployment of a vertical partially covered stent graft through the fenestration of a partially expanded polytetrafluoroethylene ( eptfe ) - covered stent graft with both bare ends to form the t configuration . 
in another study by gwon di etal . , a 6mm partially eptfecovered stent in a y configuration was deployed across the hilar trifurcation with a side - by - side technique , resulting in a median stent patency of 375days [ 13 ]  . 
table2 summarizes recent studies of fully or partially covered y / t - configured stents for hilar biliary 1 3 la radiologia medica ( 2020 ) 125 : 9991007 1005 fig . 
these studies used endoscopic or percutaneous side - by - side or stent - in - stent methods to form the biliary stents with a reported technical success ranging from 94 to 100% , a clinical success ranging from 82 to 100% , and a median patency ranging from 54 to 378days [ 1218 ]  . 
our preliminary median stent patency was 275days , which was comparable to the best of these studies . a variety of sems covering materials are commercially available , including e - ptfe , silicone , and polyurethane , each with its advantages . 
in this study , in order to further reduce the diameter of the introducer system , silicone as the covering material was used because of its good corrosion resistance and thin film thickness [ 19 ]  . 
as a result , a 6f introducer system was used in this study . the overall procedure time was shorter than in our previous study ( 52 vs 61min ) [ 4 ] , likely attributable to the partially covered stent design and the 6f delivery system making the stent deployment more convenient and simpler . 
 to make the procedure go smoothly , special attention should be given to two technical aspects : ( 1 ) expanding the stenosis completely with a balloon catheter before stent deployment and ( 2 ) advancing the guidewire to the location between the two middle radiopaque marks of the l - shaped stent for an accurate and successful limb stent deployment under fluoroscopy . 
in order to further shorten the operation time and reduce the cost to patients , four patients adopted the t - configured sems through the single hepatic approach , after a y - configured sems deployment in six of the patients . 
the t - configured stent allowed for bilateral drainage with less time consumption ( mean time of 47.8min for the t - configured stent vs 55.8min for the y - configured stent ) and no obvious difference was observed in outcomes in terms of stent patency and complications . 
long - term stent patency remains to be determined . during the follow - up , three cases ( 30% ) had stent occlusion , which fell within the previously reported rate range of 5.750.0% for uncovered stents [ 611 ] , and 733.3% for covered stents [ 1218 , 20 ]  . 
in this study , the stent was partially covered at the mid - section of the l - shaped stent with a length of coverage of 23cm , which may be insufficient to prevent tumor ingrowth . 
 designing a partially or fully covered limb stent and combining the limb stent with a partially covered main stent in a feasible and efficient manner will be our next research topics . one patient experienced hepatic abscess and the culture of the purulent fluid grew escherichia coli , indicating the occurrence of intestinal bacterial translocation . 
as such , patients with recurrent hyperthermia should have a liver ultrasound to avoid a misdiagnosis with serious complications . conclusions the results of this study should be interpreted with caution because of certain study limitations , including small sample size , a possible bias in patient selection , and no control group . 
despite these limitations , this study clearly showed that the partially covered y / t - configured sems appeared to be technically feasible and clinically effective for palliative treatment of malignant biliary trifurcation occlusion . 
images were independently evaluated by two radiologists blinded to the rt - pcr results and classified as ct positive or ct negative for covid - 19 , according to ct findings . results according to rt - pcr results , 152 patients were covid - 19 negative ( 48% ) and 162 were covid - 19 positive ( 52% )  . 
mixed ggo and consolidation pattern with peripheral and bilateral distribution , multifocal or diffuse abnormalities localized in both upper lung and lower lung , in association with interlobular septal thickening , bronchial wall thickening and air bronchogram , showed higher frequency in covid - positive patients . 
we also found a significant correlation between ct findings and patients oxygenation status expressed by pao2 / fio2 ratio . conclusion chest ct has a useful role in the early detection and in patient management of covid - 19 pneumonia in a pandemic . 
on march 11 , who declared the covid - 19 pandemic , and since march 10 , strict quarantine rules , as in china , were imposed in italy in order to reduce the infection peak . 
so far , italy has been hit harder than any other countries in europe with an average of 110.000 documented cases and 20.000 deaths related to severe acute respiratory syndrome ( sars ) [ 3 ]  . in patients with clinical features and epidemiological criteria of covid - 19 , the diagnosis is established through viral nucleic acid detection in nasal or throat swabs , sputum and lower respiratory tract secretions with reverse transcriptionpolymerase chain reaction ( rt - pcr ) [ 4 ]  . 
although rt - pcr specificity is high , sensitivity is about 4570% ; the high rate of false negatives is probably due to low viral load or limitations of sample collection [ 5 ]  . in this scenario , chest diagnostic imaging has a primary relevance in the diagnosis and severity assessment of covid - 19 together with clinical manifestations , epidemiological history and laboratory tests [ 5 ]  . 
chest computed tomography ( ct ) imaging has been demonstrated more sensitive than chest radiography ( cr ) to identify some of the manifestations of covid - 19 pneumonia [ 6 , 7 ]  . at the beginning of march , when the outbreak started in rome , we began to combine nasopharyngeal swab specimen to chest cts in patients with clinically suspected covid19 pneumonia , admitted to the emergency department in our regional hub hospital ( umberto i university hospital )  . 
 the purpose of our study was to assess the potential role of chest ct in the early detection of covid - 19 and to explore its role in patient management in an adult italian population admitted to the emergency department with suspected pneumonia . in an isolation room and tested for covid - 19 with nasopharyngeal swab sample followed by rt - pcr assay to confirm the diagnosis . 
they also underwent blood test , arterial blood gas ( abg ) examination and imaging assessment with chest ct for evaluation of covid - 19 , according to our hospitals guidelines resulting from the consent of anesthesiologists , infectivologists and radiologists as well as the chinese guidelines available at the moment [ 6 ]  . we retrospectively evaluated data from 314 patients ( 129 females , 185 males ; mean age 59 17 years ) from march 3 to 23 , 2020 , presented with clinically suspected covid - 19 . 
firstly , patients acceded to a pre - triage room where clinicians measured patients body temperature and carried out epidemiological anamnesis ( travel history or contact history with individuals tested positive for novel coronavirus infection within 14days before the onset of symptoms ) and made a clinical evaluation . 
if the suspicious of covid - 19 persisted , patients kept on going to the separate dedicated pathway and were put two radiologists ( 8 and 16years of experience , respectively ) , who were blinded to the final diagnoses and to the rt - pcr results , evaluated chest ct scans independently . 
 we considered nine ct findings , according to previous studies [ 6 , 812 ] : ground - glass opacities ( ggos ) , consolidation , mixed ggo and consolidation , single or multiple solid nodules surrounded by ground - glass opacities ( halo sign ) , bronchial wall thickening , air bronchogram , interlobular septal thickening , pleural effusion and mediastinal lymph node enlargement . ground - glass attenuation was defined as a hazy increased opacity of lung , with preservation of bronchial and vascular margins . 
consolidation was defined as a homogeneous increase in pulmonary parenchymal attenuation that 1 3 la radiologia medica ( 2020 ) 125 : 931942 obscures the margins of vessels and airway walls . 
mediastinal lymphadenopathy was judged to be present when the minimal diameter of a lymph node was larger than 10mm [ 13 ]  . the abnormalities were characterized as unilateral or bilateral . 
 [ 12 ] , we classified chest ct into four categories ( typical ct pattern , possible ct pattern , inconsistent ct pattern and negative for pneumonia ) and subsequently into ct negative ( inconsistent ct pattern and negative for pneumonia ) and ct positive ( typical and possible ct pattern ) for covid - 19 pneumonia , as shown in table1 . 
as a first step of our analysis pipeline , we computed cohens kappa for nominal variables ( 0 = sign was not detected ; 1 = sign was detected ) to assess inter - rater reliability , following the table 1 chest ct classification ct findings mixed ggo and consolidation pattern peripheral and bilateral distribution multifocal or diffuse abnormalities localized bilaterally single or multiple solid nodules surrounded by ggo ( halo sign ) absence of typical pattern single ggo opacity few very small ggo and consolidation pattern multifocal or diffuse abnormalities without peripheral distribution absence of typical / possible pattern isolated lobar / segmental consolidation smooth interlobular septal thickening with pleural effusion small centrolobular nodules with three - in - bud pattern no ct findings suggesting pneumonia procedure by hallgren ( 2012 ) , which provides point estimates and significance tests for the null hypothesis that = 0 [ 14 , 15 ]  . 
thus , using cohens kappa for nominal variables ( again , 0 = sign was not detected ; 1 = sign was detected ) we estimated the degree of agreement between readers radiological diagnosis and the results of rt - pcr . 
as a second step , we assessed the distribution of each index ( i.e. , ct findings ) in covid - 19 + and in covid - 19 patients by computing 2 . 
finally , wecomputed point - biserial correlations betweenct findings ( 0 = sign was not detected ; 1 = sign was detected ) and patients oxygenation status , expressed bypao2 / fio2ratio ( obtained by abg ) , in a subgroup of 94 patients . 
normality of distribution in the case of pao2 / fio2was tested using kolmogorovsmirnov ( ks ) test . results using rt - pcr from nasopharyngeal swab test results as a reference , we classified as covid - 19 - negative ( ) patients with negative rt - pcr results and as covid - 19 - positive ( + ) patients with positive rt - pcr results . 
the two groups were matched for gender ( 2 = 0.010 ; p = 0.918 ; cramersv = 0.006 ) : 90 males and 62 females were classified as covid - 19 ; 95 males and 67 females were classified as covid - 19 +  . 
of patients ( % ) 934 features male female range mean ( 2140 ) ( 4150 ) ( 5160 ) ( 6170 ) ( 7180 ) ( 8191 ) onset symptoms fever cough dyspnea gastrointestinal symptoms astenia thoracic pain conjunctivitis more than one symptom none underlying pathologies diabetes hypertension dyslipidemia cancer obstructive chronic bronchopulmonary disease heart failure cardiovascular and cerebrovascular disease no underlying pathologies time from symptoms onset to hospital admission ranged between 1 and 15days ; 115 patients presented 17days after symptoms onset and the remaining 199 after the first week . clinical characteristics are given in table2 . results of the inter - rater reliability are summarized in table3 . 
in brief , was significantly higher than 0 in all indexes ( all ps < 0.001 ) , suggesting that coders had a good degree of agreement . thus , the following analyses were run on one of the two raters . 
first , we estimated the degree of agreement between readers radiological diagnosis and the results of rt - pcr , finding substantial agreement between the two measurements ( = 0.751 , t = 13.328 , p < 0.000001 ) with a total of 147 covid - 19 + with ct positive and 128 covid19 with ct negative . 
in brief , mixed ggo and consolidation pattern , with peripheral and bilateral distribution , multifocal or diffuse abnormalities localized in both upper lung and lower lung , in association with interlobular septal thickening , bronchial wall thickening and air bronchogram , showed higher frequency in covid - 19 +  . 
also , interlobular septal thickening ( r = 0.435 ; p = 0.000 ) , bronchial wall thickening ( r = 0.431 ; p = 0.000 ) and air bronchogram ( r = 0.383 ; p = 0.000 ) showed a significant correlation with oxygenation impairment . 
 the purpose of this study was to assess the potential role of chest ct in the early detection of covid - 19 and to explore its role in patient management in an adult italian population admitted to the emergency department with suspected pneumonia . we comprehensively evaluated and analyzed the ct findings of 314 patients admitted to the emergency department of our regional hub hospital in rome , italy . 
using rt - pcr from nasopharyngeal swab test results as a reference , as mentioned in the results section , we classified as covid19 patients with negative rt - pcr results and as covid19 + patients with positive rt - pcr results . nasopharyngeal swab test is a widely used method to confirm covid - 19 infection , and it is recommended by who guidelines , which state that a clinically suspected case is confirmed only in the presence of a positive rt - pcr result [ 5 ]  . 
in our study , mean turnaround time for swab results was 10h , while 1 3 la radiologia medica ( 2020 ) 125 : 931942 table 3 inter - rater reliability . 
our results showed a substantial agreement between rt - pcr results and ct findings ( p < 0.000001 ) , as well as an almost perfect agreement between the two readers . in patients with covid - 19 + ( n = 162 ) , we observed a total of 147 cases classified as ct positive , according to findings interpretation . 
unlike previous studies that show prevalence of ggo pattern at the early ct scan , the mixed ggo and consolidation were the most common patterns in our study [ 23 ]  . 
this may be due to the fact that in italy , paucisymptomatic patients have mostly been managed at home by general practitioners , and only if patients worsen , they are sent to the emergency department . 
1 agreement and discrepancies between ct findings and rtpcr : 147 covid - 19 + were ct positive ; 128 covid - 19 were ct negative ; 24 cases were ct positive with negative rt - pcr results ; 15 cases were ct negative with positive rt - pcr results suspected patients must remain in isolation , hospitalized and mostly under clinical surveillance . even if chest radiography ( cxr ) , performed using portable imaging equipment , has been considered the first - line examination , due to the easy equipment disinfection , the bedridden patients accessibility [ 19 ] and the capability to differentiate between a normal and severely abnormal chest , chest x - ray findings have a lower sensitivity than initial rtpcr testing compared to ct ( 69% versus 91% , respectively ) , particularly at an early stage of the disease [ 20 ]  . 
the direction of the effect summarizes which group shows higher probability of distribution for each radiological index ( positive = higher frequency in covid + ; negative = higher frequency in covid ) the most common distribution is both peripheral and centrolobular because during the second week the disease can spread and involve even the central regions [ 24 ]  . 
however , according to other studies [ 25 ] , we observed that spatial distribution , as well as attenuation pattern , could be suggestive of covid - 19 pneumonia [ 24 , 26 ]  . 
 besides , ct imaging interpretation of symptomatic patients during the days of the peak of the pandemic spread in rome ( march 323 , 2020 ) could have affected our final diagnosis by including in the ct - positive group also the consistent , but less typical patterns ( possible ct patterntable1 )  . 
this diagnostic approach is probably not to be extended in settings different from pandemic outbreak where other causes of interstitial pneumonia must be taken into account [ 27 , 28 ]  . despite substantial agreement , we also had some discrepancies between ct and rt - pcr . in 15 cases , rt - pcr showed positive results in spite of ct negative . 
in this subgroup : one patient showed a lobar uniform consolidation strongly suggestive of lobar pneumonia ( i.e. , as seen in streptococcus pneumonia ) and was interpreted as bacterial pneumonia ( fig.4 ) ; one patient had neoplastic history and his lung alterations were interpreted as metastatic involvement with lymphangitic carcinomatosis ; and four patients showed only a single and subtle opacity that was considered an atypical ct finding , not suggestive of covid - 19 pneumonia . 
a secondary hypothesis to explain why a normal ct scan could be found associated with a positive swab is that the ct scan has been performed too early , before the development of pulmonary involvement , because frequency of ct findings is dependent on infection time course [ 29 ]  . 
 in fact , early reports have stated that initial imaging might show normal findings in 15% of individuals , so a normal chest imaging examination does not exclude the infection [ 7 ]  . 
moreover , in a study conducted in china during the first 2months of outbreak , no cr or ct abnormality was found in 17.9% patients with non - severe disease and in 2.9% patients with severe disease [ 30 ]  . 
a better understanding of the spectrum of the disease is needed , since the same study revealed that in 8.9% of the patients , 19 - ncov infection was detected before the development of viral pneumonia or viral pneumonia did not develop . 1 3 la radiologia medica ( 2020 ) 125 : 931942 fig . 
2 percentage of covid - 19 + and covid - 19 for each radiological index in 24 cases with negative swab tests ( covid - ) , ct findings were consistent with covid - 19 pneumonia ( ct positive )  . 
lung infections or inflammatory conditions can share some findings with covid - 19 pneumonia , and correct interpretation of those has probably been mistaken in a context of pandemic spread where most patients with fever and respiratory symptoms are expected to be affected by covid - 19 . in the remaining 21 cases , we observed highly suggestive ct findings for covid - 19 pneumonia , though negative rt - pcr results . 
since repeated swab tests are performed after 24h from first one , and if the latter is still negative , a third is performed the following day and so on , ct scans can give remarkable diagnostic anticipation . 
ab ct shows diffuse bilateral ground - glass opacities with prevalent peripheral distribution , septal thickening and small areas of consolidation with air bronchogram ( mixed ggo and consolidation pattern ) test ; thus , repeated sampling may be required in patients with high clinical suspicion and positive ct findings [ 31 ]  . 
 our experience confirms that when swab tests are negative , the possibility of a false - negative result should be considered in the context of a patients recent exposures and the presence of clinical and radiological signs and symptoms consistent with 2019 - ncov infection . 
for this reason , in case of epidemiological anamnesis and ct findings suggestive of covid - 19 , repeated swab test and patient isolation should be considered [ 32 , 33 ]  . 
reasons for false - negative rt - pcr may include insufficient cellular material for detection and improper extraction of nucleic acid from clinical materials [ 34 ]  . finally , as demonstrated in the correlation analysis , we found that chest ct considered ct positive and specific ct findings mentioned in the result section , significantly correlated with oxygenation impairment , expressed by pao2 / fio2ratio . 
while most people with covid - 19 develop only mild or uncomplicated illness , approximately 1 3 938 la radiologia medica ( 2020 ) 125 : 931942 negative predicted value of chest ct in early patients limit its role as an effective standalone tool to rule out covid19 [ 29 ]  . 
therefore , chest ct represents a valuable tool in identifying patients with 2019 - ncov infections at an early stage , when clinical symptoms may be unspecific or sparse [ 25 ]  . 
thus , for the timely and accurate diagnosis of covid - 19 , ct can quickly identify suspected patients and significantly help in isolating the source of infection , cutting off the route of transmission and avoiding further spread [ 34 ]  . the above - described management improves clinical decision making , especially in the emergency setting where it is of paramount importance to stratify outpatients in suspected or non - suspected cases , while waiting for the rt - pcr results [ 39 ]  . 
a management strategy based on ct results and clinical condition has already been used during the covid19 epidemic in china , when 10567 patients were treated as clinically diagnosed cases . 
in these cases , no rt - pcr test was performed but diagnosis was made based on typical symptoms , exposure history and chest ct manifestations consistent with covid - 19 pneumonia . 
we have not made a comparison with x - rays , which have been rarely performed according to our hospitals guidelines because the unit of emergency radiology has a dedicated ct room for suspected covid - 19 patients ; as a result , this diagnostic strategy probably cannot be adopted in all spoke hospitals in the region . 
in addition , according to sirm ( italian society of medical and interventional radiology ) chest ct scan is recommended in symptomatic patients [ 40 ]  . an intrinsic limit of a cohort of patients admitted to the emergency department is a large inhomogeneity , since the time of disease onset was unknown , depending on different incubation times . 
4 a 21 - year - old man with dyspnea , cough and thoracic pain in the last two days , without fever and without history of covid - 19 exposure . 
the patient , instead , was positive to the rt - pcr test 14% develop severe disease that require hospitalization and oxygen support and 5% require admission to an intensive care unit [ 35 ]  . 
a draft definition accepted worldwide proposed three mutually exclusive categories of ards based on degree of hypoxemia : mild ( pao2 / fio2 300mm hg ) , moderate ( pao2 / fio2 200mm hg ) and severe ( pao2 / fio2 100mm hg ) [ 37 ]  . 
as oxygenation impairment increases , several therapeutic options must be considered , like high - flow nasal oxygen in mildmoderate ards or endotracheal intubation and mechanical ventilation in severe cases [ 38 ]  . our study confirmed a strong correlation between swab test and chest ct findings for diagnosing or ruling out covid - 19 pneumonia and a strong relationship between clinical variables like hypoxemia and ct findings in patients considered ct positive . 
hence , our results suggest the creation of a flowchart for managing patients admitted to the emergency department with suspected infection from 2019 - ncov . patients with negative ct scan can be early discharged and isolated at home considering the low likelihood of a positive swab test and the very unlikely development of pulmonary problems . 
ct shows thin semilunar symmetric areas of peripheral subpleural increased density , bronchial wall thickness , signs of vascular congestion and cardiomegaly ; these signs were interpreted as congested interstitial spaces and poorly aerated zones secondary to bronchitis and heart dysfunction . 
instead , rt - pcr result was positive in conclusion , our study shows how chest ct has a useful role in the early detection of covid - 19 pneumonia in a pandemic . 
chest ct is particularly helpful in patient management in an emergency department because it can reliably identify suspected patients and significantly help in isolating the infected ones , cutting off the route of transmission and avoiding further spread of infection . 1 3 940 la radiologia medica ( 2020 ) 125 : 931942 fig . 
6 ab ct scan in a 43 - year - old man with fever and cough in the last 12days shows the most typical and frequent features of covid19 pneumonia : bilateral multifocal and confluent ground - glass opacities in a peripheral subpleural distribution , associated with consolidation area in the left lower lobe . 
cd a 64 - year - old man with cough and dyspnea for 10 days , treated at home with antibiotics without benefit and arrived to the hospital for the onset of fever in the last day . 
a special thanks are due to nurses and technologists of the unit of emergency radiology of umberto i university hospital for their contribution in teamwork , and also thanks are due to silvia colaiacomo for language support and to davide fogliano for data entry . compliance with ethical standards as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
the purpose of this study was to evaluate the performance of the full model - based iterative reconstruction ( mbir ) and adaptive statistical reconstruction ( asir ) algorithms in low radiation dose and low contrast dose abdominal contrast - enhanced ct ( cect ) in children . methods a total of 59 children ( 32 males and 27 females ) undergoing low radiation dose ( 100kvp ) and low contrast dose ( 270 mgi / ml ) abdominal cect were enrolled . 
the raw data were reconstructed with mbir , asir and filtered back - projection ( fbp ) algorithms into 6 groups ( mbir , 100%asir , 80%asir , 60%asir , 40%asir and fbp )  . 
the ct numbers , standard deviations , signal - to - noise ratio ( snr ) and contrastto - noise ratio ( cnr ) of liver , pancreas , kidney and abdominal aorta were measured . 
 as low - kv imaging can increase the absorption of iodide ions to improve the enhancement effect of iodine contrast agents [ 4 ] , it is often used in the double - low ct scans . 
 iterative reconstruction ( ir ) has been used in the " doublelow " ct to reduce image noise and to meet the diagnostic requirements and has been applied to ct applications in chest , abdomen , blood vessel and other areas [ 511 ]  . 
in addition , relevant studies have shown that the more sophisticated full model - based iterative reconstruction ( mbir ) algorithm is more powerful than the adaptive statistical iterative reconstruction ( asir ) in image noise reduction [ 1217 ]  . 
so far , most of the " double - low " ct studies have been focused on blood vessel ( s ) [ 3 , 4 , 6 , 8 ] , or in adults , and there are only few reports on cect in childrens abdomen , which often requires higher x - ray doses than other body regions [ 18 ]  . 
consecutive pediatric patients in our hospital from august 2015 to october 2015 were included ; all patients underwent abdominal ct scans with low radiation dose and low contrast dose scan protocol . 
the exclusion criteria were adolescent children over 14years old and / or children weighing more than 35kg . instruments andequipment all scan data were collected on a 64 - row ct scanner with gemstone detector ( discovery , hdct 750 , ge , usa )  . 
the tube current was set by automatic tube current modulation ( atcm ) in the range of 10700ma during the scan to obtain age - based image noise index ( ni ) settings : ni = 11hu for children with age of 012months ; ni = 13hu for 12years old ; and ni = 15hu for 314 years old . 
iodixanol ( 270 mgi / ml , ge healthcare , america ) was used as contrast agent , and contrast dose was adjusted according to the body weight of children ( 1.8ml / kg for 35kg , 1.6ml / kg for 510kg , 1.4ml / kg for 1015kg , 1.2ml / kg for 1535kg )  . 
the raw data were reconstructed with mbir , asir and filtered back - projection ( fbp ) reconstruction algorithms into 6 groups ( mbir , asir100% , asir80% , asir60% , asir40% and fbp ) at image slice thickness of 0.625mdifferent weights ( 100% , 80% , 60% and 40% ) were applied for the asir algorithm . subjective image quality evaluation all images of were transmitted to ge aw4.6 ct workstation for analysis and measurement ; the relevant information of children , scanning parameters and reconstruction algorithms was shielded . 
image quality evaluation and scoring were carried out by 2 experienced radiologists with 13 - year ( 3 - year imaging experience for adult , 10 - year imaging experience for children ) and 15 - year experience in imaging and radiology for children . 
 during the evaluation process , doctors can adjust window width and level according to their personal habits ; multiplanar reconstruction ( mpr ) and volume rendering ( vr ) were also available for viewing . qualitative evaluation of image quality was performed in refer to relevant studies [ 6 , 19 ] ; the 4 - point system was adopted to qualitatively evaluate image quality . 
standard for overall image noise was as follows : 4 points : image was excellent , only contained very little noise ; 3 points : image was fine , contained certain noise and could meet the diagnostic requirements ; 2 points : more image noise , could not meet the diagnostic requirements , but could determine lesion location and rough range ; 1 point : too much noise , image quality was not acceptable , and there were difficulties in distinguishing between and / or within organizational structures . 
 criteria for evaluating the display ability of abdominal tissues were as follows : 4 points : obvious enhancement in soft tissue , clear margins of organs and lesions , full diagnostic ; 3 points : adequate enhancement in soft tissue , clear margin of organs , abnormal density structures could be identified and measured , still meeting the diagnostic requirement ; 2 points : poor contrast enhancement degree in tissue or lesions , unclear margin of organs and the internal structure was not clearly demarcated , for qualitative diagnosis only ; 1 point : poor structural enhancement with marginal boundary unclear , could not meet the diagnostic requirement . objective image quality measurement after the subjective image quality evaluation was completed , the two doctors jointly measured the objective image quality : ct number and standard deviation ( sd ) value ( image noise ) ; the porta hepatis section was selected as the measuring cross section , and a region of interesting ( roi ) was used for ct number and sd measurement . 
 measurement areas were selected on both the left lobe and right lobe for liver , the head and body for pancreas , and the front and back cortex for kidney . 
moreover , signal - to - noise 1 3 920 la radiologia medica ( 2020 ) 125 : 918925 ratio ( snr ) and contrast - to - noise ratio ( cnr ) of each organ were calculated : snr = ct value of organnoise value of each organ there were 7 cases of abdominal pain to be examined and 2 cases of hematemesis . 
because of the thinner renal cortex , roi shape was changed , and roi area was reduced to 1 / 4 of the abdominal aorta area . radiation andcontrast agent dose the radiation dose and contrast agent dose were recorded . 
 the radiation dose included volumetric ct dose index ( ctdivol ) and dose length product ( dlp ) , and the contrast dose included the total volume of contrast agent used . 
the amount of iodine used was then calculated according to the concentration of the contrast agent . statistical analysis the recorded data of the objective noise and subjective scoring were represented as x sd . 
the analysis of variance ( one - way anova ) was used to compare the differences in the subjective score and objective measurement among the 6 groups of different reconstruction methods . 
for the overall image noise score , mbir was the best , followed by asir100% , both of which provided diagnostic quality images , while images of the other 4 reconstruction methods did not fully meet the diagnostic quality requirements . 
with the decrease in asir weight , the image quality gradually decreased , fbp image was the worst , and fbp images and asir40% images could no longer show clearly the boundaries of organs and lesions ; the asir60% and asir80% images could be used to identify lesions of various low contrast densities , but their edges were not clear enough for accurate size measurements . 
there was no statistically significant difference in ct numbers among the 6 reconstructed image sets ; the noise value of mbir image was the lowest , followed by asir100% ; with the decrease in asir weight , the noise value increased , and that of fbp image was the highest ; compared with fbp image , the noise value of mbir image was reduced by 64.03% ; the trends of snr and cnr were opposite to noise value , those of mbir image were the highest , and those of fbp image were the lowest , of which the cnr of mbir image increased by 165.68% in comparison with that of fbp . a total of 59 children ( 32 males and 27 females ) underwent abdominal cect examination . 
there were 18 cases of neurogenic tumors , 9 cases of renal space - occupying lesions , 4 cases of liver space - occupying lesions , 1 case of teratoma , 2 cases of pancreatic space - occupying lesions , 13 cases of postoperative reexamination , 3 cases of trauma ; moreover , discussion with the optimization of scanning protocol , reduction in tube voltage , automatic adjustment of tube current and other ways being studied and utilized , the radiation dose of ct scanning has been greatly reduced . 
on this basis , some scholars have proposed a " double - low " ct scanning protocol , that is , low radiation dose combined with low contrast dose ct , which can reduce ionization damage and kidney 1 3 la radiologia medica ( 2020 ) 125 : 918925 fig . 
image noise decreased in ir images , especially in 100%asir and mbir images , and these two groups of images had higher contrast - to - noise ratio ( cnr ) values . 
mbir could display more fine structures , such as gastric mucosa ( white arrow ) , and observe lesions more clearly , such as bile cyst and necrotic lesion ( black arrow )  . 
the rest of the images could not meet the diagnostic requirements , these images could still be used to identify different density objects , but the structure borders were not clear enough because of the high noise level and low cnr fig . 
all images had high contrast objects , such as the hepatic and hepatic vessels ( black arrow ) ; all images could display the vessels clearly , but it was difficulty to show some tiny vessels ( white arrow ) in ac because of the high image noise , which reduced the contrast - to - noise ratio ( cnr )  . 
 [ 4 ] reported that low - voltage scanning can increase the ct number of contrast agent , so it is possible to maintain ct number by reducing the dose of contrast agent in low - voltage scanning protocol . 
however , low - voltage scanning may increase image noise and adversely affect image quality . iterative reconstructions ( ir ) can reduce image noise , such as asir , and use information obtained from the fbp algorithm , combined with matrix algebra , to transform the measured value of each pixel in the image to a new estimate of pixel value and then compared against the value that the noise model predicts , and over successive cycling an ideal pixel value is created . 
mbir algorithm based on asir adds physics model and x - ray optical model in addition to the original noise mode to not only consider the noise character , but also the geometric characters of the ct detection syste it can accurately describe each volume pixel and restore the real x - ray detection mechanism . mbir has been applied in clinical practice ; through the analysis of the existing literature , mbir can greatly reduce noise and dramatically improve image quality [ 1118 ] , so we evaluated 0.625 - mm - thin slice image quality instead of routine 5 - mm images ( with asir40% ) to obtain more details . 
in addition , it has been reported that mbir can improve the recognition of necrotic lesions in children and is suitable for displaying the density difference of soft tissue [ 20 ]  . 
in terms of the display ability of organs and lesions in abdomen , the mbir images had the best ability ; due to the dramatic reduction in image noise , the contrast noise ratio of mbir images was significantly improved , which was more conducive to display small structures and low contrast objects . 
therefore , mbir could display more fine structures , such as gastric mucosa ( fig.1 ) and small intrahepatic venous vessels ( fig.2 ) even in a low contrast situation . 
the asir80% , asir60% , asir40% and fbp images could show the structure and density of lesions , but because of excessive noise , the edges of lesions with different densities and structures were blurred , and some small structures could not be observed clearly . 
at the same time , we also noticed that blurring effect could be seen on the edges of mbir images with different densities , but with low enough image noise , it could still meet the diagnostic requirements and increase the diagnostic confidence of observers . 
with the increase in asir weight , the gradually increased edge blurring effect could be seen at the edges of different densities , but we believed that this blurring effect was not enough to affect the confidence of diagnosis , and was deemed acceptable , which was similar to a previous study [ 21 ]  . 
in the abdominal cect examination of children , we believe that the reason why asir100% images could be accepted was that there were obvious density differences among different tissues in images , and these obvious density differences were due to the application of 100kv low voltage . 
under the same conditions , the ct value of contrast agent in low - tube - voltage 1 3 924 la radiologia medica ( 2020 ) 125 : 918925 images was significantly increased in comparison with that in high - tube - voltage images [ 19 , 22 ] , which is conducive to distinguish different structures in cect images . 
even though low - concentration contrast agent ( 270mgi / ml ) was used in this group of cases , which was 15.63% lower than that of the 320mgi / ml contrast agent commonly used before , it could still maintain a high contrast ratio under 100kv low - voltage condition . 
 the objective noise evaluation results showed that different reconstruction algorithms had no effect on ct number value ( f = 0.010.04 , p > 0.05 ) , but with the increase in asir weight , the objective noise of different tissues decreased in various degrees . 
combining with our practical work experience and referring to the recommendation of icrp121 [ 23 ] , 100 - kv ct scanning mode was adopted in our clinical work , which took into account the image enhancement degree and the overall noise of images ; moreover , it was easy to operate and can be applied in most childrens examinations . 
in order to avoid insufficient penetrating force of x - ray caused by the oversize of children and too much noise which may affect image quality , 120 - kv scanning scheme was still adopted for children over 14years old or weighing more than 35kg , and they were not included in the study group . there were some limitations in this study . 
the main reason was that the mbir reconstruction time was too long to meet the speed requirements of our centers daily work , while asir provides real - time images . 
considering the long reconstruction time for mbir , we are proposing a twotiered reconstruction approach : 5 - mm 100%asir images for routine diagnosis and 0.625 - mm mbir images to provide higher spatial resolution and better image quality for detailed lesion analysis . 
lastly , this study only had two observers to evaluate image quality and we did not carry out research and evaluation on abdominal cta . conclusion the double - low ct can reduce the potential risks of ionization damage and contrast agent damage , mbir or asir100% can be used to increase image cnr and provide diagnostic quality images in the abdominal cect scans in children with low radiation dose and contrast dose , and mbir algorithm provides the best performance . acknowledgements the authors would like to express our sincere thanks to jianying li for his technical support in understanding the model - based iterative reconstruction algorithm . funding this study was supported by the beijing childrens hospital young investigator program ( grant numbers bch - yipb - 201606 ) and clinical technology innovation project of beijing municipal commission ( grant numbers xmlx201407 )  . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval the present study was approved by the ethics committee of beijing childrens hospital . 
embolizations were performed with fibered coils , oversized , released stretched and not packed . results technical success , intended as occlusion of all superior hemorrhoidal artery branches , was 100% . 
at 3 - month followup , clinical improvement was obtained in four of the five patients ; hemoglobin values improved or remained stable in the whole sample . conclusions based on this limited experience , emborrhoid seems to be safe and effective at 3 - month follow - up to improve symptoms in patients with cirrhotic portal hypertension and chronic anemia due to hemorroidal bleeding ; the stretched fashion to release oversized coils provides effective embolization . keywords emborrhoid portal hypertension coiling hemorrhoids bleeding spaghetti technique introduction hemorrhoidal disease is one of the most common medical conditions in the general population , with a prevalence rate range of 435% [ 1 ]  . 
90% of patients are properly managed with conservative medical therapies , while 10% requires surgery [ 2 ]  . clinical presentation is characterized by rectal bleeding , causing anemia in the long - term , hemorrhoidal prolapse and anal itch due to tissue exudation and maceration ; pain is reported in advanced phases of disease , related to local complications ( thrombosis , fissurations , criptitis )  . 
for vessel calipers of 3 , 4 and 5mm , the coils sizes ranged 45mm , 56mm and 78mm , respectively . no risk of coils migration occurred due to oversizing and adhesion to vessel wall . results technical success , intended as occlusion of all the sha branches above the pubic symphysis , was 100% . two patients required a second session with embolization of bilateral inferior hemorrhoidal arteries because of bleeding relapse after 10 and 15days ( figs.23 ) , respectively ; in these cases , no recanalization of the sha branches was observed . according to cirse classification system [ 11 ] , no complications were reported neither pain or incontinence . la radiologia medica ( 2020 ) 125 : 10081011 materials andmethods patients five patients with chronic internal hemorrhoidal bleeding and cirrhotic portal hypertension were treated with emborrhoid . 
conventional surgery was excluded because of comorbidities . before the procedure and at 3 - month follow - up , patients were asked to fill standardized questionaires [ 6 ] to objectively evaluate their clinical conditions : bleeding severity score ; symptoms score ; and quality of life ( qol ) score . the local institution ethical committee approved this study ; all patients gave written informed consent to the procedure and data publication . procedure under local anesthesia and through a 5fr femoral access , the inferior mesenteric artery was catheterized ; the sha and each division directed to the corpus cavernosum recti were catheterized with a 2.7fr microcatheter ( progreat terumo japan ) distally ; embolization was performed with microcoils ( concerto medtronicusa micronester or tornado cook medicaldenmark ) above the symphysis pubic bony landmark . five - day oral antibiotics therapy and antinflammatory were prescribed postprocedure . spaghetti technique the customized coiling technique , named spaghetti technique , because of the angiographic shape , consisted in fig . 
oversized microcoils released stretched and unpacked into sha branches ( spaghetti technique ) to cover the whole lenght of the vessel ; this patient rejected bladder catheter table 1 patient features patient cirrhosis etiology child pugh stage preproceduralhemoglobin ( g / dl ) postproceduralhemoglobin ( g / dl ) goligher stage previoussurgery male male female male female metabolic alcoholic alcholic 10.2 embolization 1 3 1010 la radiologia medica ( 2020 ) 125 : 10081011 fig . 
a\ lateral aortography showing occlusion at the origin of the inferior mesenteric artery ( white arrow ) ; b\ recanalization of sha through the riolano arcade by superior mesenteric artery ( white asterisks ) ; c\ microcatheter navigation up to sha ; d\ postembolization arteriographic control showing procedural success at 3 - month follow - up , bleeding severity , symptoms and qol scores improved in four of the five patients , with better results obtained concerning symptoms ( table2 ) : reduction in rectal bleedings in terms of frequency and entity as well as pain decrease . 
the goligher grade remained unchanged . discussion until now , only one case report has been published about emborrhoid in a patient with portal hypertension [ 7 ]  . based on this limited preliminary experience , emborrhoid technique seems to be effective in reducing hemorrhoidal disease even in patients with portal hypertension . 
 the inferior hemorrhoidal artery ( iha ) was embolized in two of the five patients because of rebleeding ; in these cases , vascular collateralization was supposed ; therefore , bilateral coiling of the iha was performed . 
a\ left inferior hemorrhoidal arteriography ( white arrow ) showing anastomosis with left middle hemorrhoidal artery ( dotted white arrow ) ; b\ bilateral coiling of inferior hemorrhoidal arteries ( black arrows ) table 2 clinical scores before and after treatment patient bleeding severity score symptoms score quality of life score baseline follow - up baseline follow - up baseline follow - up 10 / 20 7 / 20 15 / 20 16 / 20 12 / 20 5 / 20 7 / 20 5 / 20 9 / 20 8 / 20 1 3 la radiologia medica ( 2020 ) 125 : 10081011 1011 hemorrhoidal arteries [ 9 , 12 ] ; they reported high clinical success rates with lower rate of relapse compared to the data on the conventional emborrhoid technique ( only sha embolization ) ; however , a theorical higher risk of ischemia should be taken into account . two different embolizing agents have been adopted in emborrhoid [ 312 ] , coils and particles ( > 300 micron )  . 
a theorical advantage of particles is their distalization into the corpus cavernosum recti , reducing recurrence rates but an increased risk of local ischemic complications should be considered as well , even if not reported [ 8 ]  . the rationale of releasing oversized coils in a stretched fashion ( spaghetti technique ) derives from the principle that the arterial flow can be interrupted progressively during the procedure because a sudden occlusion is not mandatory , as instead it is required in acute hemorrhages scenarios . 
finally , a small number of coils is required because one / two coils per vessel are enough . concerning patients with portal hypertension , until now only a case report has been published about the emborrhoid technique as a bridge to tips placement [ 7 ]  . 
the pathophisiology of hemorrhoidal disease in these subjects is related to reduced venous outflow [ 13 ] ; however , based on this limited preliminary experience , emborrhoid seems to be effective in the short term by reducing hemorrhoidal disease because the reduction in arterial inflow decreases the hypertension of the corpus cavernosum recti . 
compared to surgery , low invasiveness , safety and less susceptibility to coagulopathies represent potential relevant advantages . main limitations of this study are the small number of patients analyzed and the short - term follow - up ; this is a preliminary experience that aims to expand the fields of application of emborrhoid , and more data are needed on larger samples with longer follow - up . conclusions based on this limited experience , emborrhoid is safe and effective in the short term to improve symptoms in patients with cirrhotic portal hypertension and chronic anemia due to hemorroidal bleeding . 
this approach should be considered as a feasible alternative in this subset of ill patients . the stretched fashion to release oversized coils provides effective occlusion of the target vessels . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual patients included in the study . la radiologia medica ( 2020 ) 125 : 961970 neuroradiology imaging ofextraventricular neurocytoma : asystematic literature review nicolaromano1 margheritafederici1 antoniocastaldi1 received : 8 january 2020 / accepted : 13 april 2020 / published online : 25 april 2020 italian society of medical radiology 2020 abstract objective extraventricular neurocytoma ( evn ) was firstly described in 1997 . 
in this systematic review , we summarize and discuss computed tomography ( ct ) and magnetic resonance imaging ( mri ) features of evn cases described in the literature , in order to provide useful informations to neuroradiologists . 
to the best of our knowledge , this is the most extensive review about imaging of evn . materials and methods a systematic review of the literature about imaging of evn cases was done . 
after implementation of inclusion and exclusion criteria , 35 studies were considered , and a total of 79 cases of evn were analyzed . conclusion evn has not specific characteristics , with a large and variable imaging spectruusually it appears as a large tumor , with diameters superior to 40mm , frequently involving the frontal lobe . 
today , diagnosis of evn with only imaging techniques is not univocal ; neuroradiologists can only suspect this type of lesion , while the definitive diagnosis remains histological . keywords computed tomography magnetic resonance imaging neuroradiology neurocytoma brain introduction extraventricular neurocytoma ( evn ) was firstly described in 1997 , when giangaspero etal . 
prognosis is considered favorable ; however , some cases of atypical evn with higher mitotic activity and tendency to recur have been described , firstly by brat e al in 2001 [ 5 ]  . 
currently , atypical evns are defined as tumors with a ki - 67 index of > 3% or with peculiar histological features such as increased mitotic figures , focal necrosis , or endothelial cell proliferation [ 57 ] ; however , who 2016 classification does not include this histopathological entity [ 3 ]  . the current literature regarding imaging of evn is limited to sporadic case reports and case series . 
it is typically described as a circumscribed variable - sized mass ( usually large ) with a solid portion characterized by contrast enhancement , depending on the degree of cellularity ; cystic components , calcifications , hemorrhagic vol . : ( 0123456789 ) 1 3 962 la radiologia medica ( 2020 ) 125 : 961970 areas , and peritumoral edema are other recognized findings [ 8 ]  . in the present systematic review , we summarize and discuss computed tomography ( ct ) and magnetic resonance imaging ( mri ) features of evn cases described in the literature , in order to provide useful informations to neuroradiologists . 
to the best of our knowledge , this is the most extensive review about imaging of evn . methods a systematic review of the literature was done and updated on 11 march 2020 . 
the search was performed with the following strategies : ( extraventricular ) and neurocytoma on pubmed database and ( titlecombined : ( extraventricu lar neurocytoma ) ) on hinari database . 
they were also investigated , through analysis of case descriptions or figures , the characteristics of the margins and the presence of perilesional edema , cystic components , calcifications , hemorrhages , intralesional flow voids , and contrast enhancement . 
a total of 79 cases were analyzed , as summarized in table1 . the older article was published in 1999 while the majority were published after 2011 ( 80% )  . 
diffusion - weighted imaging ( dwi ) mri characteristics were discussed in 13 cases ( 16.45% ) , 5 cases ( 38.5% ) of which showed restriction of the diffusion . 
regarding spectroscopy , the results were described in 3 cases ( 3.79% ) , all with decrease in naa and elevation of choline . discussion evn has not specific characteristics , with a large and variable imaging spectruusually it appears as a large tumor , with diameters superior to 40mm , frequently involving the frontal lobe . 
ct density and mri signal intensity typically mirror the presence of cystic , solid , or calcified elements ; 1 3 la radiologia medica ( 2020 ) 125 : 961970 table 1 cases of evns included in our systematic review tortori donati etal . 
 [ 24 ] 26 m mesencephalon 10 8 10mm ct , mri la radiologia medica ( 2020 ) 125 : 961970 mri : hypointense on t1wi , hyperintense on t2wi ; edema ; cystic + ; calcification ; hemorrhage ; enhancement + diffusion : no restriction mri : hypointense ont1wi , hyperintense on t2wi ; edema + ; cystic + ; calcification + ; hemorrhage ; enhancement + diffusion : no restriction mri : hypointense ont1wi , hyperintense on t2wi ; edema ; cystic + ; calcification ; hemorrhage ; enhancement + diffusion : no restriction mri : hypointense on t1wi , hyperintense on t2wi ; edema ; cystic ; calcification ; hemorrhage ; enhancement + diffusion : no restriction mri : hypointense on t1wi , hyperintense on t2wi ; edema ; cystic + ; calcification ; hemorrhage ; enhancement + mri : hypointense on t1wi , hyperintense on t2wi ; edema ; cystic ; calcification ; hemorrhage ; enhancement + mri : isointense on t1wi , hyperintense on t2wi ; edema ; cystic ; calcification ; hemorrhage ; enhancement diffusion : no restriction mri : hypointense on t1wi , hyperintense on t2wi ; edema ; cystic ; calcification ; hemorrhage ; enhancement + diffusion : no restriction mri : hypointense on t1wi , hyperintense on t2wi ; edema ; cystic ; calcification ; hemorrhage ; enhancement mri : hypointense on t1wi , hyperintense on t2wi ; edema ; cystic + ; calcification + ; hemorrhage + ; enhancement + diffusion : restriction of diffusion isodense on ct ; irregular ; edema ; cystic ; calcification ; enhancement hypodense on ct ; mri : hypointense on mri t1wi , hyperintense on t2wi ; edema + ; cystic + ; calcification + ; enhancement + hyperdense on ct ; mri : hypointense on mri t1wi , hypointense on t2wi ; edema + ; cystic ; calcification + ; enhancement + 1 3 la radiologia medica ( 2020 ) 125 : 961970 table 1 ( continued ) age sex location size imaging techniques findings huang etal . 
 [ 32 ] 25 m sellar 39 36 30mm ct , mri hyperdense on ct ; mri : hypoinhypodense on ct ; mri : hypointense on mri t1wi , hyperintense on t2wi ; edema ; cystic + ; calcification ; enhancement + hyperdense on ct ; mri : isointense on mri t1wi , hyperintense on t2wi ; edema ; cystic ; calcification + ; enhancement + hypodense on ct ; mri : hypointense on mri t1wi , hypointense on t2wi ; edema + ; cystic + ; calcification + ; enhancement + hyperdense on ct ; mri : isointense on mri t1wi , hyperintense on t2wi ; edema ; cystic ; calcification + ; enhancement + mri : isointense on mri t1wi and t2wi ; edema ; cystic ; enhancement mri : isointense on mri t1wi ; hyperintense on t2wi ; edema + ; cystic + ; enhancement + mri : hyperintense on t2wi ; ill defined ; edema ; cystic + ; enhancement + edema + ; cystic + ; calcification + ; enhancement + diffusion : restriction of diffusion hyperintense on t2wi ; edema + ; cystic + ; calcification + ; enhancement + diffusion : restriction of diffusion rcbv + spectroscopy : naa / cr - , cho / cr + hyperintense on t2wi ; edema + ; cystic + ; calcification + ; flow void + ; enhancement + isodense on ct ; mri : hyperintense on t2wi calcification + ; enhancement + diffusion : restriction of diffusion on t1wi , isointense on t2wi well defined ; edema ; cystic ; calcification ; enhancement + tense on mri t1wi , hyperintense on t2wi ; well defined ; edema ; cystic + ; calcification ; hemorrhage ; enhancement + tense on mri t1wi , hyperintense on t2wi ; well defined ; edema ; cystic ; calcification + ; enhancement + 1 3 966 table 1 ( continued ) ji etal . 
 [ 38 ] 64 m frontal l and r 73 80 64mm mri 1 3 la radiologia medica ( 2020 ) 125 : 961970 table 1 ( continued ) age sex location size imaging techniques findings jiang etal . 
 [ 40 ] 23 m frontal l 43 35 63 ct , mri la radiologia medica ( 2020 ) 125 : 961970 mri : isointense on mri t1wi , hyperintense on t2wi ; well defined ; edema + ; cystic + ; calcification ; hemorrhage ; flow void + ; enhancement + mri : hypointense on mri t1wi , hyperintense on t2wi ; well defined ; edema + ; cystic ; calcification ; hemorrhage ; flow void ; enhancement + well defined ; edema ; cystic ; calcification ; enhancement hypodense on ct ; bone scalopping ; mri : isointense on mri t1wi , hyperintense on t2wi ; well defined ; edema + ; cystic + ; calcification ; hemorrhage ; flow void + ; enhancement + perfusion : cbv + table 2 summary of imaging features investigated features specified in n ( % ) margins perilesional edema cystic calcification hemorrhage flow void enhancement 40 ( 50.63% ) 74 ( 93.67% ) 72 ( 91.13% ) 56 ( 70.88% ) 34 ( 43.03% ) 21 ( 26.58% ) 79 ( 100% ) well defined = 24 ( 60% ) present = 37 ( 50% ) present = 45 ( 62.5% ) present = 26 ( 46.43% ) present = 15 ( 44.12% ) present = 14 ( 66.7% ) present = 69 ( 87.34% ) poor defined / irregular = 16 ( 40% ) absent = 37 ( 50% ) absent = 27 ( 37.5% ) absent = 30 ( 53.57% ) absent = 19 ( 55.88% ) absent = 7 ( 33.3% ) absent = 10 ( 12.66% ) lesions with larger cystic components appear hypodense on ct , hypointense on t1 - wi and hyperintense on t2 - wi . 
a different category is represented by sellar / parasellar evns [ 2 , 8 , 17 , 19 , 23 , 30 , 32 , 38 , 39 ] , which differential diagnosis respect to craniopharyngioma or pituitary macroadenoma may be difficult : the 91% of them ( n = 10 / 11 ) has no perilesional edema . 
data on perfusion and spectroscopy studies of evn are very poor ; however , the increase in cerebral blood volume ( cbv ) and the decrease in n - acetylaspartate ( naa ) associated with increase in choline in the solid portion of evn can be considered typical results . 
atypical evns have more aggressive imaging patterns , such as large dimensions ( 5cm ) , growth across lobes , lobulated and ill - defined margins , the presence of flow voids , areas of necrosis / cystic degeneration , and hemorrhage . 
in our review , atypical features are specified in 24 cases ( 30.37% ) and imaging features are similar to remaining evns ; however , it is evident that only 3 cases of atypical evns had well - defined margins , despite 9 cases of irregular / poorly demarcated margins . 
oligodendroglioma occurs 1 3 la radiologia medica ( 2020 ) 125 : 961970 more commonly in older patients ( 4050 y.o ) , and tends to extend toward and throughout the cerebral cortex , also eroding calvaria [ 8 , 24 ] ; calcifications are present in about 7090% of cases and are usually coarse . 
ganglioglioma commonly occurs in children or young adults and , in the vast majority of cases , has a predilection for the temporal lobe , associated with epilepsy ; it may be partially solid or cystic , with a variable contrast enhancement and low perilesional edema [ 8 , 24 ]  . 
high - grade astrocytoma usually occurs in patients aged 4050years ; typically , it is characterized by a more aggressive pattern , with mass effect and abundant peritumoral edema ; calcifications are exceedingly rare [ 824 ]  . 
 extraventricular ependymoma is a rare tumor that usually presents as a large lesion , with cystic and solid enhancing areas , associated with the presence of calcifications ; perilesional edema and hemorrhages may be present . 
in some cases , extraventricular ependymoma is characterized on unenhanced ct axial images by the periwinkle sign , resembling a flower with centripetal calcifications surrounding a central necrotic area [ 43 ]  . 
 meningioma is commonly characterized by pronounced contrast enhancement associated with encroachment on adjacent structures ; the t2 - signal is usually not high and dural tail sign with adjacent bone thickening can be typical features [ 8 , 24 ]  . 
pituitary macroadenoma arises from the pituitary gland with superior extension into the suprasellar cistern with possible compression of the chiasm ; the indentation of the diaphragma sellae leads to its typical appearance , known as snowman configuration . 
in addition , most of the articles were not supported of imaging features we wanted to investigate . conclusion this article may be useful for neuroradiologists to provide some insight into imaging diagnosis of evn . 
we can affirm that evn has not specific characteristics with a variable imaging spectruit may be suspected in young patients with large tumoral lesion , usually characterized by solid tissue with cystic components , whose presence usually influences its imaging appearance . 
97 of 843 patients had clinical and radiological signs of possible bladder injury and underwent retrograde air distension . results among 97 patients , 31 / 97 showed ct signs of bladder rupture , of which 5 / 31 ( 16% ) intraperitoneal , 25 / 31 ( 81% ) extraperitoneal and 1 / 31 ( 3% ) combined . 
among the 66 / 97 patients with no signs of bladder injury , 38 / 66 had surgery , which confirmed bladder integrity , while 28 / 66 were managed conservatively and showed no signs of bladder rupture at clinico - radiological follow - up examinations . conclusions ct evaluation of urinary bladder after retrograde air distension ( pneumo - ct - cystography ) may be a reliable diagnostic tool in the detection of bladder rupture in patients with blunt pelvic trauma . 
this technique is faster , cheaper and allows to overcome some of the limitations of conventional ct - cystography . keywords emergency radiology computed tomography ultrasound bladder rupture introduction genitourinary injuries are frequent complications of abdomino - pelvic trauma and occur in 1520% of pelvic fractures cases , especially if pubic symphysis is involved [ 13 ]  . 
camillo forlanini hospital , rome , italy 2 diagnostic imaging unit , policlinico universitario campus bio - medico , rome , italy 3 department ofemergency radiology , careggi university hospital , l.go brambilla 3 , florence , italy have been classified into five types , which are resumed in table1 ( table1 ) [ 4 ]  . 
multidetector , whole - body contrast - enhanced computed tomography ( ct ) is the gold standard technique in the evaluation of a stable polytrauma adult patient [ 1720 ]  . 
 ct - cystography with positive contrast agent retrograde bladder distension is currently the most widely accepted exam for the diagnosis of bladder rupture [ 4 , 11 , 2127 ]  . 
considering the physical properties of air and the interesting literature reports about pneumoct - cystography in the detection of bladder neoplasms , the aim of our study was to determine if bladder distension with vol . : ( 0123456789 ) 1 3 la radiologia medica ( 2020 ) 125 : 907917 908 table 1 classification , radiological findings and management of bladder injuries type injury radiological findings management contusion intraperitoneal rupture ( ip ) normal contrast extravasation in the paracolic sulci , in the pouch of douglas and surconservative surgical interstitial injury extraperitoneal rupture ( ep ) rounding bowel loops , liver and spleen contrast agent may spread into bladder wall . 
no contrast extravasation simple : contrast extravasation is limited to the perivesical space complex : contrast extravasation extends into the retroperitoneum , the anterior conservative conservative abdominal wall , the scrotum , the perineum combined rupture combination of ip and ep surgical fig . 
notice pelvic fluid ( arrowhead in a ) and left ilio - pubic branch fracture ( white arrow in d ) , as predictors of possible bladder tear air might help to overcome some of the limitations of conventional ct - cystography and increase the accuracy of ct in the detection of bladder ruptures [ 3539 ]  . materials andmethods patients between january 2010 and september 2019 , 843 patients with abdomino - pelvic trauma ( 556 males and 287 females ; age range , 1693years ; mean age , 42.3years ) were admitted to our level ii trauma center . 
41 / 843 patients underwent immediate surgical treatment because of unstable hemodynamics and / or hemoperitoneum / hemothorax / pericardial tamponade detected with efast ( extended focused assessment with sonography for trauma )  . 
2 false negative ct cystography : peri - vesical hematoma ( white arrows in a , b , c ) with active bleeding of the bladder wall , causing a misdiagnosed tear in the left lateral wall not identified at ct - cystography ( d ) and detected at surgery table 2 causes of false - negative and false - positive ct - cystography causes of false - negative study incomplete distension pelvic hematoma large rupture with massive extravasation of contrast sealing tear pelvic hematoma blood clot contraction of detrusor muscle foley catheter balloon gravity impossibility to move the patient in a prone decubitus causes of false - positive study oral or intravenous contrast agent contrast in the vagina bone fragments and underwent whole - body contrast - enhanced ct for appropriate trauma staging . 
foley catheter was positioned if no urethral injury was suspected . image acquisition all images were obtained with a 64 - row ct scanner ( somatom sensation , siemens medical systems , erlangen , germany )  . 
after unenhanced scan , 120130ml of monomeric , non - ionic , iodinated contrast agent ( xenetix 350 mgi / ml , guerbet , france ; iomeron 350 mgi / ml , bracco , italy , omnipaque 350mgi / ml , ge healthcare ) were administered intravenously through an automatic injector at a flow rate of 3ml / s , followed by 50ml of saline solution injected at the same flow rate . 
pneumo - ct - cystography signs of bladder rupture included at least one of the following : air leak , leak of contrast agent derived from urinary excretion or direct evidence of discontinuity in bladder wall . 
the presence of free abdomino - pelvic air in the baseline scan ( as occurs in penetrating injuries or bowel perforation ) led to the exclusion of 13 patients , since it could represent a confounding factor . 
air leak in peri - vesical space ( c , white arrow ) and between anterior abdominal wall and parietal peritoneum ( arrow in d ) are suggestive of extraperitoneal bladder rupture . 
air leak at the level of the anterior wall ( arrow in c ) as well as intraperitoneal free air ( arrow in d ) are pathognomonic of bladder rupture . 
31 ( 32% ) of the 97 pneumo - ct cystograms were interpreted as positive for bladder rupture : 25 were extraperitoneal ruptures , 5 intraperitoneal ruptures and 1 combined intraperitoneal and extraperitoneal rupture ( fig.4 , 5 , 6 , 7 )  . 
among the 31 patients with signs of bladder injury , 15 ( 48% ) showed air leak , 1 ( 3% ) both air and contrast agent leak , 12 ( 39% ) both air leak and bladder wall discontinuity and 3 ( 10% ) all 3 findings simultaneously . 
 among the 66 patients with no signs of bladder injury , 38 had surgery for other comorbidities ( splenicor hepatic injury , hemoperitoneum , pelvic ring fractures ) which confirmed bladder integrity in all cases , while 28 were managed conservatively and showed no signs of bladder rupture at clinical and radiological follow - up examinations . 
air distension demonstrates a tear in the anterior wall ( white arrow in d ) and free air along the inner aspect of anterior abdominal wall and left spermatic cord ( b , d , f ) , suggesting complex extraperitoneal bladder rupture discussion in the setting of bladder trauma , ct - cystography with positive iodinated contrast agent is widely accepted as the gold standard technique for the diagnosis of bladder injury . 
 reported that false - negative results may be obtained if the bladder is sub - optimally distended , as occurs in the presence of pelvic hematoma or in massive ruptures [ 4 ]  . 
it must also be considered that the effect of gravity on bladder content and the impossibility to move a polytrauma patient to a prone decubitus may cause a suboptimal distension of the anterior bladder wall , increasing the chances of not detecting a tear in that portion . 
bladder distension with air ( pneumo - ctcystography ) is an alternative technique for the evaluation of urinary bladder , which proved to be a useful tool in the 1 3 la radiologia medica ( 2020 ) 125 : 907917 not identify a rupture . 
first , it is not always possible to make a comparison between conventional ct - cystography and pneumoct - cystography in the same patient due to ethical issues and to the fact that the patients has to be treated as soon as possible , according to atls protocols [ 48 ]  . 
second , we could not provide a control group that included patients with no bladder distension , since in all cases of suspected bladder rupture a retrograde filling of the bladder ( either with contrast or air ) is mandatory ; in our opinion this is the main limitation of our study , being also a common intrinsic limitation in emergency radiology studies . 
regarding patients with extraperitoneal bladder rupture who did not undergo surgery , we considered air leak as a pathognomonic ct sign of bladder rupture , since no other explanation for the onset of abdomino - pelvic free air could be identified . 
regarding patients with ct signs of bladder integrity and no surgery , the only noninvasive criterion to classify them as true or false negatives was the result of follow - up exams , in which neither clinical nor radiological indicators of bladder injury were identified . 
first , being a negative contrast agent , air allows to overcome those conditions in which a hyperdense material ( bone , metallic fragments , contrast agent extravasation from blood ) may mimic a rupture . 
air , by gravity , tends also to go upwards placing itself over the iodinated contrast agent excreted by the kidneys and under the anterior bladder wall ( fig.3 ) , increasing the chance of detecting a lesion in that zone . 
the patient was managed conservatively , and follow - up ct performed 17days later ( c ) showed disappearance of signs of bladder rupture 1 3 914 la radiologia medica ( 2020 ) 125 : 907917 fig . 
considering the differential cost ( pneumo - ct - cystographyct - cystography ) for a single exam of 39.80 , introducing pneumo - ctcystography as an alternative to conventional ct allowed a total saving of 3.821 , 80 during the years of investigation . conclusion the literature reveals several conditions that may affect the diagnostic accuracy of ct - cystography in the detection of bladder injury , reporting both false negatives and false positive results . 
our study showed that , due to the physical properties of air , pneumo - ct - cystography may overcome some of those limitations and increase the accuracy of ct in the diagnosis of bladder injury , especially in the anterior 1 3 la radiologia medica ( 2020 ) 125 : 907917 fig . 
air distension demonstrates a tear in the anterolateral right wall ( white arrow in c ) and free air between anterior abdominal wall and parietal peritoneum ( white arrow in d ) , suggesting extraperitoneal bladder rupture . 
surgery confirmed the diagnosis of extraperitoneal anterior wall rupture wall , showing an excellent sensitivity and specificity and proving to be cheaper than conventional ct - cystography . nevertheless , due to the high complexity of patients management in the emergency setting , the study has some intrinsic limitations and biases that must be taken into account . 
exclusion criteria were age < 16years and mediastinal lymphoma lesion < 4cwe selected 108 patients ( m : f = 47 : 61 , median age 48years , range 1779 ) and divided them into a training and a validation group . 
the aucs of the best radiomic and the clinical model not differed . conclusions we developed and validated a ct - based radiomic model able to differentiate mediastinal masses on non - contrast - enhanced images , as thymic neoplasms or lymphoma . 
 therefore , the present image - derived method has the potential to noninvasively support diagnosis in patients with prevascular mediastinal masses with major impact on management of asymptomatic cases . keywords mediastinal neoplasms thymus neoplasms lymphoma image processing computer - assisted diagnostic imaging introduction a huge variety of benign and malignant lesions can manifest as a mediastinal mass [ 1 ]  . 
when evaluating a computed tomography ( ct ) scan , location , size and morphology ; attenuation , heterogeneity , enhancement patterns , presence of intralesional fat , cystic components , soft tissue and calcification , connection with or invasion of adjacent structures should be assessed [ 2 ]  . 
accordingly , the lesions within the prevascular compartment ( i.e. , anterior mediastinum ) could be distinguished by solely imaging ( i.e. , thyroid goiter , benign teratoma , cysts either pericardial or thymic , lipoma and thymolipoma and thymic hyperplasia ) or by combining imaging and clinical information ( e.g. , thymic hyperplasia , thymic epithelial neoplasms , lymphoma ) [ 2 ]  . 
 nevertheless , mediastinal mass appearance may not be straightforward or clinical presentation may be unusual vol . : ( 0123456789 ) 1 3 952 la radiologia medica ( 2020 ) 125 : 951960 resulting in a challenging diagnosis . 
moreover , considering the multitude of entities arising in the mediastinum and their low incidence , most physicians , either imagers or clinicians , have even more difficulties in achieving a diagnosis [ 1 ]  . 
the main risks in managing patients with a resectable mediastinal mass and uncertain diagnosis are surgical resection of lymphoma , which should be medically treated [ 46 ] , or tumor seeding from an encapsulated thymoma during biopsy procedure [ 7 , 8 ]  . 
however , a noninvasive approach able to differentiate lymphomas from thymic malignancies has not been developed yet . radiomics and machine learning methods have been proposed to extract data from medical images . 
radiomics consists of calculation of a multitude of parameters , which capture the intensity distribution and texture of the lesions , to be tested for correlation with clinical and biological characteristics . 
machine learning methods , comprising many different algorithms ( generally using a supervised or semisupervised approach ) , take medical images or image - derived parameters as inputs and provide a classification , clustering or prediction , in a data - driven manner . 
 however , neither radiomics nor machine learning has been used to differentiate malignant mediastinal masses . we aimed to assess the ability of radiomics , applied to baseline not - enhanced ct images , to differentiate mediastinal masses as thymic malignancies vs lymphomas . materials andmethod design andinclusion / exclusion criteria the present was an observational retrospective single - centre investigation . 
we considered for inclusion patients with pathological diagnosis of a thymic neoplasia or lymphoma , who performed the baseline chest ct scan in our institution , presenting with a prevascular mediastinal lesion . 
due to the observational retrospective design of the study , the signature of an informed consent was waived . image processing anddatasets non - contrast enhanced computed tomography images retrieval and qualitative evaluated . 
manually delineated the volume of interest ( voi ) on ct images in all patients using two different approaches : ( 1 ) lifex software and ( 2 ) smart segmentation algorithm on the eclipse workstation ( varian medical systems , palo alto , ca )  . 
we applied two different resampling settings : 1 1 4mm and 2 2 2mthe 1 1 4mm resampling setting was used within lesions contoured using both lifex and eclipse ( datasets 1 and 2 , respectively )  . 
a total of 41 features were extracted per each dataset ( histogram , co - occurrence and higher order , as detailed in supplemental table1 )  . in all patients , pathological diagnosis obtained from a biopsy or from a surgical sample was used as reference . reference standard statistical analysis patient characteristics were summarized in frequency tables , and descriptive statistics were provided . 
the association between radiomics and final diagnosis was based on linear discriminant analysis ( lda ) that is a robust machine learning classification method aimed at separation of two ( or more ) classes , by searching for a linear combination of variables [ 17 ]  . 
per models 13 , we tested ( a ) radiomic features only or ( b ) radiomics and clinical variables ( i.e. , age , sex , b symptoms , lymphadenopathies at physical examination , autoimmune disorders and white blood cells count ) combined . 
in the training group , we randomly included an equal number of thymic neoplasia and lymphoma patients : 35 cases each while the remaining 38 patients were assigned to the validation group . 
aa 52 - year - old female presenting with a mediastinal mass , no lymphadenopathies at physical examination , no b symptoms , no autoimmune disorders , white blood count ( 103 / l ) 8900resulted to be affected by hodgkin lymphoma , nodular sclerosis subtype , stage iii ; ba 70 - year - old female , presenting with a mediastinal mass , no lymphadenopathies at physical examination , no b symptoms , no autoimmune disorders , white blood count ( 103 / l ) 6900 resulted to be affected by thymoma , histological subtype b3 , stage iii ; c46 - year - old male presenting with a mediastinal mass , no lymphadenopathies at physical examination , no b symptoms , no autoimmune disorders , white blood count ( 103 / l ) 9200resulted to be affected by hodgkin lymphoma , not otherwise specified , stage ii ; da 37 - year - old male , presenting with a mediastinal mass , no lymphadenopathies at physical examination , no b symptoms , no autoimmune disorders , white blood count ( 103 / l ) 9000 resulted to be affected by thymic carcinoma , histological subtype c , stage ii was then applied to the independent validation set ( split sample validation approach )  . 
clinical information and laboratory data were retrieved from the institutional records ; it included age , sex , the presence of b symptoms , lymphadenopathies at physical examination , autoimmune disorders and white blood cells count . 
patient characteristics are summarized in table2 . table 2 baseline patient characteristics forty - five ( 33 thymic malignancy and 12 lymphoma cases ) out of 108 ( 42% ) patients presented a prevascular mediastinal mass without any other sign or symptoautoimmune disorders included myasthenia gravis ( n = 13 ) , ankylosing spondylitis ( n = 1 ) , acquired hemophilia a ( n = 1 ) and pure red cell aplasia associated with a megakaryocytic thrombocytopenia ( n = 1 ) ( table1 )  . thirty - three and 13 features radiomic resulted reproducible when comparing the segmentation software ( lifex versus eclipse ) and the resampling ( 1 1 4mm versus 2 2 2mm ) , respectively . 
details on features reproducibility results are provided in table3 . the lda selected 4 features for the model while a higher number of features ranging from 7 ( model 2b ) to 15 ( model 1b ) were selected within the radiomics models . 
2 schematic representation of the study workflowand summary of the results : 1patient selection , clinical and laboratory data collection from the institutional database ; 2non - contrast - enhanced computed tomography images retrieval and qualitative evaluation ; 3manual segmentation using two different software ; 4two different resampling settings ; 5radiomic feature calculation from the image datasets ; 6both clinical data and radiomic features tested as diagnostic predictors ; 7radiomic , clinical and radiomic + clinical models performance comparison ; 8study results significance . 
 voivolume of interest 1 3 958 la radiologia medica ( 2020 ) 125 : 951960 approach or reference standard , number of features tested heavily unbalanced compared to the number of patients , and the lack of any type of validation . 
the clinical value of pet - derived features is even more questionable since pet examination is not routinely performed to characterize mediastinal masses and the radiomic approach cannot be applied to the non - fdg - avid lesions . 
in the present study , we used non - contrast enhanced ct scans only since we intended to avoid introducing variability within the images related to the contrast medium administration . 
indeed , it is recognized that multiple factors , such as concentration , administration flow rate and ejection fraction , can affect contrast enhancement of the tissues [ 20 ]  . 
demonstrated that non - contrast - enhanced radiomicbased signature performed better compared to the contrastenhanced ct - derived signature in differentiating benign vs malignant lung nodules [ 21 ]  . 
moreover , the use of noncontrast enhanced ct images could allow easier clinical implementation related to the minor preprocessing steps and consistency among different acquisition protocols and centers [ 22 , 23 ]  . 
hundreds of parameters can be calculated from the images , but limited cohorts of patients are available , especially in one single institution , for the development and validation of predictive models . 
 finally , multicentre study design is needed to provide adequate sample size and also a more robust external validation compared to an internal or a single institution one . we have to acknowledge some limitations of our study . 
nonetheless , thymoma and lymphoma are among the most frequent conditions that represent a challenge in image interpretation . in conclusion , a ct - based radiomic model resulted to be able to differentiate mediastinal masses on non - contrastenhanced images , as thymic neoplasms or lymphoma . 
the image - derived method has the potential to support diagnosis in asymptomatic patients , with atypical clinical presentation or in the absence of suggestive imaging findings , in a noninvasive manner . acknowledgements mk phd scholarship was funded by the airc grant ( ig - 2016 - 18585 )  . 
the scientific guarantor of this publication is arturo chiti , who is the principal investigator of this retrospective trial . author contributions mk , ms and ac conceptualized the study ; gn participated to data collection and image processing ; lc performed data analysis ; ev , pz , ccs , fr participated in patient selection and were in charge of treatment ; ng and lb participated to patient selection ; mk and ms supervised image processing , critically interpreted the results and drafted the paper ; ib , lb and ac supervised the activities ; and all the authors read , commented and approved the manuscript . funding the authors state that this work has not received any funding . compliance with ethical standards conflict of interest the authors of this manuscript declare relationships with the following companies : kirienko , ninatti , voulaz , gennaro , barajon , ricci , sollini , balzarininone . 
carlo stellareceived speaker honoraria from msd , bms , amgen , janssen , astrazeneca ; acted as scientific advisor for genenta science , adc therapeutics , sanofi , boehringer ingelheim ; benefited 1 3 la radiologia medica ( 2020 ) 125 : 951960 from an unrestricted grant from rhizen pharmaceuticals . 
zucalireceived speaker honoraria from astellas , pfizer , sanofi , janssen , bms , ipsen , and novartis ; acted as scientific advisor for astellas , pfizer , bms , janssen , msd and novartis . 
chitireceived speaker honoraria from general electric and blue earth diagnostics , acted as scientific advisor for blue earth diagnostics and advanced accelerator applications , and benefited from an unconditional grant from sanofi to humanitas university . 
the acquired data were submitted to anthropological analysis . results ct enabled the identification of the bundles content : four cats with complete skeleton , one upper part of a cat mummy , one lower part of a cat mummy , one cat head with four cervical vertebrae , two crocodiles , two raptors , skeletons from one or more snakes and one mummy with dog appearance , containing long bones . 
all cats and hawks showed cervical fractures ; in one cat , the skull was collapsed inwards , and in another cat , the head was turned backwards ; one cat presented a skeleton more radiopaque than normal with evidence of cracks related to the use of the resins for mummification that were poured directly over the corpse . conclusions ct is a valuable noninvasive technique to study egyptian mummies , enabling in - depth analysis while preserving the integrity of the mummy bundles , ensuring protection of a valuable archaeological resource . keywords computed tomography ct mummy animal mummies 3d reconstructions introduction a mummy is defined as a body embalmed or treated for burial with preservatives through human intervention , followed by wrapping of the corpse in layers of linen . the ancient egyptians practiced mummification procedures on both human and animal subjects , yet the motivations for such treatment differed greatly . 
the preservation of the human dead was intended to ensure the conservation of the body considered essential for an eternal existence * michaela cellina michaela.cellina@asst - fbf - sacco.it 1 mummy project , ospedale fatebenefratelli , asst fatebenefratelli sacco , milano , piazza principessa clotilde 3 , 20121milan , italy 2 dipartimento di scienze biomediche perla salute , universit degli studi di milano , via mangiagalli 31 , 20133milan , italy 3 division ofspecial andpediatric radiology , department ofradiology , university hospital umberto i lancisi salesi , via conca 71 , 60126ancona , an , italy 4 reparto di radiologia , ospedale san raffaele , via olgettina 60 , 20121milan , italy 5 school ofearth andenvironmental sciences , university ofmanchester , oxford road , m139plmanchester , uk 6 american university incairo , auc avenue road , cairo , cairogovernorate11835 , egypt 7 akhmim mummy studies consortium ( amsc research llc ) , harrisburg , pa , usa 8 scientific investigation department , carabinieri ( r.i.s. ) rome , viale di tor di quinto , 151 , 00191rome , italy 9 reparto di radiologia , ospedale fatebenefratelli , asst fatebenefratelli sacco , milano , piazza principessa clotilde 3 , 20121milan , italy vol . : ( 0123456789 ) 1 3 944 la radiologia medica ( 2020 ) 125 : 943950 in the afterlife [ 1 ]  . 
the vast majority of animals preserved after death were intended to satisfy an incredible demand for votive offerings : communication devices acting as divine messengers between man and the gods . 
in fact , these so - called votive mummies have been found to contain a variety of materials including complete or partial animal bodies , non - skeletal animal materials ( e.g. , feathers , eggshell , dung , nest material ) and non - animal material ( e.g. , sand , sticks , stones , linen )  . 
the discovery of x - rays by wilhelm conrad roentgen on november 8 , 1895 , revolutionized the clinical study of living beings , yet some of the earliest bodies to be investigated using this technique were ancient egyptian mummified animals chosen because the primitive equipment could accommodate their small size . 
radiography allows the identification of materials hidden within wrapped mummy bundles and enables their classification as true mummies ( those containing bodily remains ) and mummies constructed from non - corporeal elements ( often referred to as pseudomummies )  . 
false mummies were produced during the late nineteenth century to meet the demand of the antiquities trade ( the so - called modern or fake mummies ) [ 2 ]  . the advances in the capability of radiographic imaging techniques have contributed to a progressive history of the use of x - rays for mummy investigation with the systematic investigation of collections from major museums beginning in the 1960s . 
however , it was in the late 1970s , with the introduction of computed tomography ( ct ) , that the radiological analysis of egyptian mummies made a radical stride : the acquisition of images in axial slices dramatically changed the approach to this type of research [ 2 ]  . 
the first ct examination of an egyptian mummy was conducted on a human mummy in toronto in 1977 [ 3 ] ; then , ct technology was applied for the examination of individual mummies and mummy collections [ 36 ]  . the main advantage of ct investigation is the complete noninvasiveness , meaning that , in order to identify the human and artificial materials included in the wrappings , there is no need to physically unwrap the irreplaceable mummies . 
therefore , mummy autopsies are now conducted virtually , leaving the mummies intact . due to the high spatial resolution , the increased contrast resolution in comparison with x - rays and the potential to obtain accurate measurements of structures and densities within mummies , ct enables many of the traditional limitations of conventional x - ray to be overcome . 
the development of multidetector ct ( mdct ) equipment enabled isotropic data to be acquired and viewed from multiple angles , allowing structures to be virtually separated and viewed more easily . 
this is particularly relevant in cases of incomplete skeletal remains , packing materials used within the body cavities and the isolation of anomalous material included within the wrappings . high - tech post - processing methods enable multiplanar and 3d reconstructions to be performed , thereby radically increasing the quality and the quantity of available information [ 7 ]  . 
3d reconstructions allow a precise visualization of the appearance of the mummies and their skeletal components , the possibility to evaluate the embalming materials and techniques , and the grade of preservation of soft tissues [ 710 ]  . 
with human mummies , the combined use of mdct and sophisticated post - processing software enables suggestive 3d reconstruction of the physiognomy of the individuals original facial features [ 11 ]  . according to a search on the literature , ct was first applied for the examination of animal mummies in 1987 : the first animal investigated was a cat [ 12 ]  . 
generally , mummified animal remains from ancient egypt have been less well researched than human mummies , even if their study can provide a valid contribution to our knowledge on species diversity and preservation techniques [ 13 ]  . in this article , we want to report our experience on ct investigation of animal mummies ; in particular , we want to focus on the practical and radiological aspects of the study , the acquisition parameters and the different reconstruction techniques . materials andmethods the mummies the mummies were part of the collection of mummies of the civic museum of natural science of brescia , italy , which consists of 27 organic , zoological and anthropological finds of egyptian origthese finds originate , not from archaeological excavations , but from private collections after being acquired through the antiquities market , meaning that their provenance is unknown . 
for many years , the collection had remained hidden , only being located in 1996 in the museums basement in sealed boxes with handwritten labels indicating that they contained egyptian mummies , actually containing mummies of animals and assorted human remains . 
the specimens were likely boxed in 1984 , as suggested by the dates of some newspaper used as packing 1 3 la radiologia medica ( 2020 ) 125 : 943950 material . 
medical - grade foam supports and sheets were used to aid in the positioning of the mummies on the ct scanner table and to prevent movement during study . preliminary scout images were executed to optimize the field of view . 
acquisition parameters were as follows : 120kv ; 140 mas ; slice thickness : 1mm ; reconstruction interval : 0.7mm ; and rotation time : 0.75s. all datasets were reconstructed by two experienced radiologists with both bone and soft tissue threshold algorithms and were archived on our picture archiving and communication system ( pacs ) using their catalogue number as an identifier , so that images were not lost or difficult to recover . 
images were then transferred on intellispace portal ( philips healthcare , best , the netherlands ) for post - processing multiplanar and 3d reconstructions . multiplanar reformation ( mpr ) into axial , sagittal and coronal planes was firstly performed , and then , maximum intensity projections ( mips ) with variable slab thickness helped improve spatial understanding and visualization of structures . curved planar reformations and mips were sometimes executed to visualize the hind leg and foot and paws , toes and claws along the axis . volume reformation was executed to perform a virtual autopsy by changing the window levels to visualize first the bundle and , gradually , manually changing the window , the soft parts , the skeleton and any other contents of the mummy , thus obtaining a virtual unwrapping of the bundle . images were analyzed to establish the content : a complete animal skeleton , a partial animal skeleton or a different content . 
mummification materials and potential foreign bodies were assessed . the acquired data were submitted to anthropological analysis . results ct enabled the identification of the wrappings content and of the species of the investigated mummies : four complete skeletons of cats , two partial feline skeletons : a cat skull and four cervical vertebrae and the lower part of a cat mummy which was broken in two pieces and catalogued with two different inventory numbers , 1 pseudo - cat mummy resembling a head , but without any skeletal materials inside , maybe representing a false head for a cat mummy , two crocodiles , two raptors , one mummy resembling a dog containing a number of long bones and what appear to be reeds or feathers and more small snakes in the same bundle . 
the evidence from ct analysis is listed in table1 . the most prevalent species represented were cats ; the animals were positioned in the classic skittle shape , sitting on the hind legs , with the front legs taut , the tail gathered around the legs or to the side of the body . 
the appearance of the shape and the bandages suggests that it is the same individual : the upper part ( head ) is mummy 05 , and the lower is mummy 07 lower part of mummy 05 the presence of unfused growth plates indicating an immature individual the yellowish fur and the foot pads are preserved . cating an immature individual the presence of hyperdense oval component ( 3cm ) representing a gastrolith cating an immature individual fracture through the cervical spine the presence of a fragment of a long bone , probably from another bird indicated by the difference in size , placed adjacent to the skull which terminates at the mid thorax level , used as a splint to keep the skull in position the beak , sclerotic rings , skeletal form and body dimensions suggest that this is a kestrel , falco tinnunculus 1 3 la radiologia medica ( 2020 ) 125 : 943950 table 1 ( continued ) pacs number of findings and type of mummy bundle content size findings find 011 raptor mummy complete and articulated bird skeleton 22cm find 012 mummy resembling a dog isolated long bones , reeds or feathers 17cm the presence of at least three long bones find 013 snake mummy vertebral bodies from at least three small snakes 16 27cm no skulls are visible ( common for snakes to be decapitated as this was an effective means of dispatch ) the head appears to be presented in an odd position , and the neck is twisted , probably through the mummification process the beak , sclerotic rings , skeletal form and body dimensions suggest that this is a kestrel , falco tinnunculus ( humerus , radius and ulna , or femur , tibia and fibula ) fig . 
 the skeletal components are ill - defined , and the skeleton is very radio - dense ; this means that the resins used for mummification were poured directly over the corpse . 
 metal pins ( white arrowheads ) were used in previous restoration procedures in all cases , the approach with volumetric reconstruction allowed the quick identification of the bundle content and of the species of the animal . the execution of the virtual unwrapping helped establish the location of the animal skeleton in the bundle and its size , in comparison with the whole envelope , the thickness of the linen layers and the presence of other components included in the mummy , and provided a first glance to the position of the corpse . mpr and mip reconstructions were useful in the bone assessment , for the presence of skeletal fractures , and the evidence of unfused epiphyses to estimate the age of the animal . 
these reconstructions also allowed a better 1 3 948 la radiologia medica ( 2020 ) 125 : 943950 visualization of the density of the skeleton that gave us useful information about the mummification technique and the use of radiopaque resins , and an accurate display of the position of the various skeletal segments , such as the feline tail . discussion when studying mummies with ct equipment , we need to understand what questions can be answered by imaging , as approval for imaging an artifact depends on a costbenefit ratio . in fact , we must consider the risk in packing the archaeological finds , the mode and duration of transport , which involves significant planning . in our case , as the content of the bundles was unknown , we needed a way to find out , and the ct study was the first choice , as it provided information regarding envelopes contents in a completely noninvasive way , preserving the integrity of these precious artifacts . a mummy bundle was expected to include the remains of a single complete individual ; however , the content of animal mummies can be variable [ 13 ] and can consist , as in our study , in just a part of an animal , or in pseudo - mummies , which do not contain skeletal remains . 
the unexpected content is not discernable by the evaluation of their external appearance ; even the mummies containing fragmented skeletal remains were modeled with the appearance of a complete animal mummy . 
as previously suggested , the explanation could be that the external appearance of the bundle was of greater importance than the real content to ancient egyptians and that the presence of a single complete body was not mandatory to the function of the mummy bundle as a votive offering . 
the limited availability of complete animal corpses and the necessity to embalm all deceased animals found on sacred sites may have contributed to the development of this type of mummies consisting of incomplete bodies [ 13 , 14 ]  . another factor that we have to consider is the organization at the study site , including staffing and time . in our case , the radiological staff was voluntary and therefore costless ; however , the cost of closing the program of a ct machine for enough time to study the findings must be considered and it must also be kept in mind that , if the study takes place in a hospital with inpatients and an emergency department , a second ct machine must be available to perform any emergencies , as in our case . another factor we have to consider is that there is no standardized system to study the mummies , particularly in case of animal mummies where few experiences are available [ 13 ] , and the acquisition protocol should be set by the radiologist in collaboration with experience technicians . 
ct showed a full thickness fracture of the distal cervical spine , leading to the detachment of the head , which was turned backwards : it was probably repositioned in the wrong direction during the restoration ( arrowhead )  . 
on mip reconstruction ( b ) skeleton results diffusely radiodense : the resins used for mummification were poured directly over the corpse , which then hardened and cracked as they dried . 
in crocodile mummy 08 , we observed the presence of a hyperdense oval component with dimensions of 30 20 mm , a gastrolith , a stone swallowed by the animal or the remains of stomach contents 1 3 la radiologia medica ( 2020 ) 125 : 943950 fig . 
a long bone , perhaps from another bird ( white arrowheads ) , can be observed in ( c ) , positioned posteriorly , adjacent to the skull and ending near the middle of the thorax . 
externally this mummy is decorated to resemble a dog ; however , the content does not correspond to the external appearance , and in fact , the envelope contains no complete animal skeleton , but at least three long bones ( humerus , radius and ulna , or femur , tibia and fibula )  . 
the dense patches ( arrowhead ) correspond to resins moreover , there is no standardized pattern for images postprocessing and image analyses and the performance of different reconstructions is time - consuming . 
the italian college of breast radiologists by sirm recommends precautions to protect both patients and healthcare workers ( radiologists , radiographers , nurses , and reception staff ) from infection or disease spread on the occasion of breast imaging procedures , particularly mammography , breast ultrasound , breast magnetic resonance imaging , and breast intervention procedures . keywords covid - 19 breast care recommendations breast cancer priority categories personal protective equipment ( ppe ) introduction at the beginning of february 2020 , only three cases of coronavirus disease 2019 ( covid - 19 ) were identified in italy , all involving people who had recently travelled to china [ 1 ]  . 
on february 20 , 2020 , a severe case of pneumonia due to severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) was diagnosed in lombardy , italy , in a man in his 30s without any history of possible exposure abroad [ 2 ]  . 
within 14days , many other cases of covid - 19 in the surrounding * francesco sardanelli francesco.sardanelli@unimi.it extended author information available on the last page of the article area were diagnosed , including a substantial number of critically ill patients [ 3 ]  . 
since then , a spread of covid - 19 was observed , especially in northern italy , with a wide severity spectrum , ranging from asymptomatic disease , minor flulike symptoms to severe pneumopathies or multiorganfailure [ 3 ]  . 
patients who are older and have comorbidities ( diabetes , cardiovascular disease , cancer , immunosuppression , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 926930 obesity , etc . ) are the most likely to develop severe forms [ 5 , 6 ]  . 
because of the combination of lockdown , need of social distancing , and reduced hospital resources , in many cases the routine outpatient breast imaging activity has been drastically reduced . 
therefore , it is crucial to define which women require urgent or nonreschedulable care , can wait reasonable time , or can wait until the pandemic is over [ 7 , 8 ]  . 
a new paradigm has been introduced by the pandemic facing , on the one hand , with best oncological management , avoiding any potential loss of opportunity [ 9 , 10 ] and , on the other , extra - protection from the risk of sars - cov - 2 infection [ 11 ]  . in this context , the italian college of breast radiologists by the italian society of medical radiology ( sirm ) provides recommendations for breast care provision and procedural prioritization , being aware that medical decisions must be currently taken balancing patients individual and community safety . 
 recommendations for oncologic imaging of whole - body staging / restaging are left to general oncologic imaging recommendations ( 2020 ; www.asco.org , 2020 ) [ 11 , 12 ]  . priority categories andsuggested practice the response to this pandemic has led to a sudden disruption of routine medical care , including breast imaging workup in asymptomatic population , symptomatic patients , and management of cancer patients [ 7 , 8 ]  . 
even early breast cancer can be a fatal disease if left untreated , so adequate surgery combined with appropriate perioperative therapies is essential to improve the outcome [ 9 , 10 ]  . 
it is well known that early detection contributes to a decrease in specific breast cancer mortality [ 1315 ] , and breast cancer outcomes are dependent on timely and high - quality multidisciplinary interventions [ 14 ]  . 
a short delay ( e.g. , 612weeks ) should not affect overall outcomes [ 9 , 10 ] , while a diagnostic delay longer than 3months potentially does [ 9 , 10 ]  . 
patients who have suspicious symptoms of breast cancer ( in particular : new onset palpable nodule ; skin or nipple retraction ; orange peel skin ; unilateral secretion from the nipple ) should request non - deferrable tests at radiology services ; 3 . 
asymptomatic women performing annual mammographic follow - up after breast cancer treatment should preferably schedule the appointment within 1year and 3months from the previous check , compatibly with the local organizational conditions ; 4 . 
asymptomatic women who have not responded to the invitation for screening mammography after the onset of the pandemic or have been informed of the suspension of the screening activity should schedule the check preferably within 3months from the date of the not performed check , compatibly with local organizational conditions . these recommendations are driven by the common goal to preserve hospital resources for covid - 19 patients by deferring breast imaging procedures without compromising long - term outcomes for individual patients . 
therefore , the risk of disease progression and compromised breast cancer - specific outcomes need to be weighed against viral exposure to patients and staff , considering each individuals comorbidities and age to predict risk of mortality because of covid - 19 . 
lastly , these are only recommendations and are not intended to supersede individual physician judgment or institutional policies and guidelines . all efforts should be made to avoid delayed diagnosis in patients considered at high priority , due to the potential impact on cancer outcome . 
preoperative imaging for local / contralateral staging in this context , the italian college of breast radiologists breast cancer [ 16 ] ; by sirm has defined the following recommendations : 1 . 
in the context of current pandemic , multidisciplinarydiscussions should take into consideration both values and preferences of any individual patient as well as the local epidemiological condition , expected to strongly vary during the next months . personal protective equipment the italian college of breast radiologists by sirm promotes the following precautions to protect both patients and healthcare workers ( radiologists , radiographers , nurses , and reception staff ) from infection or disease spread during breast imaging procedures , particularly mammography , breast ultrasound , breast mri , and breast intervention procedures , such as biopsy . 
the close proximity of both the patients and healthcare workers faces during these imaging procedures raises concern for droplet contamination in addition to blood spatter contamination , which may occur during image - guided interventions and spread by saliva while talking during imaging ( : / / apps.who.int / , 2020 )  . 
everyone involved is invited to follow the indications explainedbelow during breast imaging procedures , avoiding inappropriate , unsolicited , or redundant examinations and being compliant with the established settings . oncological / urgent outpatient , supposed sarscov2 negative all patients are considered at risk of sars - cov - 2 infection . 
 in the waiting room , the patient should be present alone without any accompanying caregiver ; close adherence to physical distancing ( at least 1m ) is required between each patient . 
asymptomatic patients should be invited to sanitize their hands , using the appropriate devices set up at the entrance of the waiting roopatients wearing gloves should be invited to replace them with new ones provided by la radiologia medica ( 2020 ) 125 : 926930 the center . 
patients must wear a surgical mask ( provided by the center if the patient does not wear it at the arrival ) , and if wearing an ffp2 or ffp3 mask with filter , they should wear a surgical mask over . all staff having close or physical contact with patients undergoing breast imaging , including interventional procedures ( breast biopsy ) , should wear surgical mask , visor or goggle protection , disposable gown , disposable cap , and disposable gloves . 
all the devices with direct contact to the patient ( e.g. , ultrasound probe cover , mammographic equipment , magnetic resonancebreast coil ) should be sanitized with a disinfectant before every patient . 
all healthcare workers ( radiologists , radiographers , and nurses ) wear an ffp2 mask , visor or goggle protection , disposable gown , disposable cap , and disposable gloves . 
further sanitization of all the devices with which the patient comes into contact ( e.g. , ultrasound probe and machine , mammographic equipment , and magnetic resonance room ) must be performed after undressing at the end procedure to be ready for next dressing . patients positive forsarscov2 infection the patient must wear a surgical mask . 
all healthcare workers ( radiologists , radiographers , and nurses ) wear an ffp2 or ffp3 mask , visor or goggle protection , disposable waterproof gown , disposable cap , double disposable gloves . 
in cases where the patient cannot wear the surgical mask , healthcare workers must wear an ffp3 mask . 1 3 la radiologia medica ( 2020 ) 125 : 926930 emotional aspects ofcancer patients duringcovid19 pandemic funding this research received no specific grant from any funding agency in the public , commercial , or not - for - profit sectors . all the commotion of the covid - 19 pandemic is anxietyprovoking among both patients and practitioners . 
the significant psychological impact on oncological patients is compounded by multiple factors : knowledge that the individual is at higher risk of serious complication if infected by sars - cov - 2 , loneliness and isolation as a result of social distancing , and the underlying constant fear of the cancer [ 26 ]  . 
to reduce uncertainty feelings affecting both clinicians and patients , structured recommendations and the adequate psychological support are essential tools for healthcare workers to aid cancer patients to overcome this difficult moment [ 27 , 28 ]  . compliance with ethical standards conflict of interest the authors declare that there is no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
the radiation dose intensification appears probably associated with a higher rate of genitourinary toxicity . keywords rectal cancer dose intensification radiotherapy surgery postoperative complications toxicity * luca nicosia luca.nicosia@sacrocuore.it 1 department ofsurgery , irccs ospedale sacro cuore don calabria , via don a . 
sempreboni 5 , 37024negrar , verona , italy 3 department ofsurgical science , university hospital ofparma , via gramsci , 14 - 43126parma , italy 4 university ofbrescia , brescia , italy introduction the treatment for locally advanced rectal cancer ( larc ) has improved in the last decades . 
nowadays , a multidisciplinary approach is strongly advocated since that improvement in pretreatment diagnostic imaging , the integration of ( neo ) adjuvant radiotherapy ( rt ) and chemotherapy ( cht ) in the therapeutic algorithm , and the routine adoption of the total mesorectal excision ( tme ) allowed to favorably modify the natural history of larc [ 16 ]  . 
in the case of resectable disease , the combination of preoperative rtcht represents the standard of care due to the possibility to obtain high tumor downstaging and downsizing rate [ 2 , 7 ]  . 
the use of long - course rt with fluoropirimidine further increased tumor downstaging and pathological complete response vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 990998 ( pcr ) , actually ranging from 13 to 25% [ 1 , 2 , 710 ]  . 
in the case of larc , available clinical data are still conflicting . given the prognostic role of tumor regression grade ( trg ) and pcr as independent factors for local control , overall survival ( os ) and disease - free survival ( dfs ) , the intensification of preoperative radiotherapy could be attempted to further improve local control and survival [ 2 , 7 , 9 , 1118 ]  . 
the evidence of a doseresponse relationship in terms of trg for rt dose > 5060gy was supposed and investigated in some papers and provided a strong rationale for intensifying rt dose in the neoadjuvant setting [ 7 , 11 , 1421 ]  . 
intensity - modulated rt and image - guided rt ( igrt ) by means of onboard imaging , including cone beam computed tomography ( cbct ) , can minimize involvement of organs at risk and may offer new opportunities for dose escalation [ 16 , 22 ]  . 
moreover , a simultaneous integrated boost ( sib ) approach could be adopted to simultaneously irradiate high - risk region and primary tumor or positive pelvic lymph nodes with different doses during the same treatment session [ 8 ]  . 
the aim of the present study was to compare the oncological outcomes between neoadjuvant standard dose rt - cht and dose - intensified rt - cht in patients affected by larc . multidisciplinary gastrointestinal and oncological tumor board discussed all patients . endpoints the primary endpoint was pathological response ( t stage , n stage , trg )  . 
patients were analyzed as follows : sdr regimen as group 1 and rdi regimen as group 2 . inclusion criteria were : age > 18years , a world health organization ( who ) performance status of 01 that allowed for long - course rt - cht and then surgery , locally advanced histologically proven adenocarcinoma of the rectum within 10cm from the dentate line . 
for both treatment groups , external iliac lymph nodes were included in the case of abnormal obturator lymph nodes that were suspicious for malignancy at imaging or in the case of ct4 disease . 
a total dose of 50.4gy in 28 fractions was prescribed to the ptv . radiation dose intensification ( group 2 ) mri and / or 18 - fdg - pet / ct were merged separately with the planning ct . 
the boost volume ( ctv - sib ) was defined including 18 - fdg - pet / ct positive areas ( primary tumor and the corresponding mesorectum and / or positive pelvic nodes ) , adding 5mm isotropic expansion to generate the 1 3 992 la radiologia medica ( 2020 ) 125 : 990998 corresponding ptv - sib , in order to minimize dose to the bladder and therefore avoiding major genitourinary toxicity . 
analyses were performed using spss v24.0 ( chicago , il ) and statase v11 ( college station , tx )  . surgery surgery was scheduled at least 8weeks after neoadjuvant therapy . 
in the intersphincteric resections , the colon - anal anastomosis was performed only in patients with a valid continence status and only after a histologically proven negative infiltration of the elevator muscles at the time of surgery . 
the severity of complications was defined according to claviendindo classification [ 23 ]  . pathology intraoperative extemporaneous histologic examination of the elevator muscle was performed in patients planned for intersphincteric resection . 
mesorectum integrity was graded for the presence of defects according to the quirke grading system [ 26 ]  . statistical analysis with a scheduled number of 22 patients per group , it was possible to detect a standardized mean value effect of 0.8 with a power of 80% and an alpha level of 5% . 
however , for the robustness of the study , we enrolled more study participants ( n = 56 )  . all continuous values were presented as the mean standard deviation . 
pearsons chi square test with yates correction and fishers exact tests have been results from january 2013 to december 2016 , 131 patients underwent surgery for rectal cancer at irccs , sacred heart hospital of negrar . 
fifty - six patients were included in the study : 25 patients in the sdr group ( group1 ) and 31 patients in the rdi group ( group2 )  . 
the two groups were homogenous in gender , bmi , american society of anesthesiologists ( asa ) status , preoperative tumor and nodal stage , median tumor diameter and distance to dentate line . 
no postoperative death was reported . discussion the evidence of doseresponse relationship in terms of local control and tumor regression grade for rt doses > 5060gy provides a valid rationale for intensified rt in patients with larc [ 1 , 7 , 915 , 19 ]  . 
to evaluate the role of rt intensification in larc , several studies with preoperative intensity - modulated rt associated with 5fu - based cht have documented encouraging results in terms of feasibility , pathological response and toxicity [ 7 , 10 , 1416 , 20 , 21 ]  . 
in their systematic review and meta - analysis quantified the pcr rate after neoadjuvant chtrt with 60gy without imrt as 20.4% associated with low ( 10.3% ) acute grade 3 toxicity and a high resectability rate ( 89.5% ) [ 9 ]  . 
 [ 7 ] showed a tumor and lymph node downstaging , respectively , in 70.8% and 67% of patients with larc treated with intensified rt and capecitabine with a pcr rate of 22% . 
in our series , pcr was 20% in sdr group and 22.6% in rdi group : radiation dose intensification did not produce a significant pathological complete response in line with literature [ 1 , 2 , 7 , 2729 ]  . 
they did not find significant difference in surgical complications between standard rt group and intensified rt group ; anastomotic leakage occurred only in four patients treated with the standard method [ 12 ]  . 
patients that were converted to open surgery had a t4 tumor with no response to neoadjuvant cht - rt . as already mentioned , surgical complications after intensified preoperative rt were rarely analyzed in the literature . 
 wound infection , anastomotic leakage , bowel obstruction and delayed healing are the main complications reported , and they range between 0 and 40% [ 9 , 12 , 13 ]  . 
the patients of rdi group had longer hospitalization and needed redo surgery ; three of these patients had a terminal colostomy as result of severe complication , and in one patient , the pull - through surgery was the only way to restore bowel continuity . 
 as before mentioned , these results about surgical complications and surgical outcomes should be critically analyzed because they are not statistically significant and because in rdi group the median age was statistically higher than that in sdr group . 
even if the patients in the two groups were 1 3 996 la radiologia medica ( 2020 ) 125 : 990998 not statistically different in clinical comorbidity and systemic therapy , the higher age of patients in rdi group could also explain the increased nonsurgical complications in this group [ 30 ]  . 
the analysis of pathological specimens of our series showed a higher rate of incomplete mesorectum in rdi group ( 8.3% in group 1 and 22.6% in group 2 )  . 
the worse quality of the mesorectum could affect long - term outcomes in terms of local relapse and disease - free survival . the toxic side effects of rt increase with the irradiated volume . 
it is recognized that the adoption of volumetric modulated arc therapy ( vmat ) and image - guided radiotherapy , by means of onboard imaging , impacts on toxicity profile in pelvic irradiation . 
in our study , in rdi group the dose constraint to 1cc of intestinal cavity ( ic ) was 60gy and the volume receiving > 45gy was < 195cc [ 34 ]  . 
however , when the ptv60 involves a lymph node which is adjacent to the ic , we accepted for planning approval d1 cc not higher than 60 gy to that adjacent segment of the intestinal cavity . 
in this case , we privileged target dose coverage by considering that the ic is a quite moving structure , and it is then unlikely to hit every day the same portion of the small bowel as depicted by planning ct . 
in male patients , ejaculation disorders and erectile dysfunctions were also recorded , while in female patients , dysmenorrhea , dyspareunia , vaginitis , vaginal dryness were the most frequent side effects . 
 the period of the late toxicity meets the time of surgery , and it is difficult to match the true responsibility of the events . a schedule of 54gy in 30 fractions ( 1.8gy per fraction ) has a biological effective dose ( bed ) similar to 50gy in 25 fractions ( 2gy per fraction ) and is appropriate for microscopic disease control . 
we choose 54gy in 30 fractions in order to deliver 60gy in standard 2gy per fraction to the macroscopic disease with simultaneous integrated boost ( sib ) , therefore avoiding the risk of acute and late toxicity associated with doses per fraction higher than 2gy . we did not consider brachytherapy or contact x - ray therapy in order to intensify the radiation treatment because we do not have brachytherapy or contact x - ray devices in our institution , so we had to rely only on external beam radiotherapy . we are aware that our study presents some limitations : the lack of randomization , the relatively small sample size and the need for a longer follow - up to achieve information about overall survival and disease - free survival . 
however , even with these limitations , this is to our knowledge the first study that deeply analyzed surgical outcomes in patients with larc that underwent neoadjuvant radiation dose intensification in terms of severity of postoperative complications and quality of surgery . conclusions the present study suggests a significant improvement in the pathological response of t3 tumors treated with intensified neoadjuvant regimen . 
several studies demonstrated the therapeutic potential of sirt , for example for hepatocellular carcinoma [ 1 ] ( hcc ) [ 2 , 3 ] , cholangiocarcinoma ( ccc ) [ 4 ] , or liver metastases from colorectal cancer [ 1 ] , uveal melanoma [ 5 , 6 ] , breast cancer [ 7 , 8 ] , vol . : ( 0123456789 ) 1 3 972 la radiologia medica ( 2020 ) 125 : 971980 neuroendocrine tumor ( net ) [ 9 , 10 ] , renal cell carcinoma ( rcc ) [ 11 ] and pancreatic adenocarcinoma [ 12 ]  . despite the widespread clinical use of sirt and promising results for tumor control , adverse events ( aes ) following sirt have been reported , including ( a ) acute side effects , such as abdominal pain [ 1315 ] , nausea [ 1315 ] , pancreatitis [ 13 ] , fever [ 13 , 15 , 16 ] , postembolization syndrome [ 14 , 17 ] and leukocytosis [ 15 ] and ( b ) late side effects , such as gastroduodenitis [ 18 ] , gastric ulcer [ 13 , 14 , 19 ] , gastrointestinal bleeding [ 20 ] , cholecystitis [ 19 ] and pneumonitis [ 21 , 22 ]  . 
 therefore , some centers perform sirt on an inpatient basis [ 20 ] , while others prefer an outpatient setting [ 1 , 23 , 24 ]  . while an inpatient scheme has the benefit of prolonged survey to identify and treat potential aes immediately , this needs to be evaluated with care due to higher cost . 
a costefficient use of resources is essential and outpatient treatment of patients is favorable , if it is not associated with a high rate of recalls or complications or high radiation burden for the environment . thus , the aim of this study is to examine whether sirt can be safely applied in an outpatient setting regarding radiation exposure to the environment and post - interventional complications , by measuring the occurrence of adverse events and the radiation dose rate after treatment . materials andmethods patient cohort between september 2008 and may 2014 , 212 patients with primary and secondary liver malignancies were treated with 90y - sir - spheres at our institution . 
inclusion and exclusion criteria were according to the eanm procedure guideline for the treatment of liver cancer and liver metastases with intra - arterial radioactive compounds [ 25 ]  . 
exclusion criteria were a life expectancy less than one month , severe chronic pulmonary disease and contraindications to hepatic artery catheterization including severe chronic renal failure [ i.e. , estimated glomerular filtration rate ( egfr ) less than 30ml / min ] , unmanageable coagulopathy and severe allergy to contrast media . 
a multidisciplinary team approved the therapy for each individual patient , and written informed consent was given by all patients . primary malignancies included hepatic hemangioendothelioma , hepatic angiosarcoma , hcc , ccc and synchronous or metachronous hcc / ccc . 
1 patient cohort that was analyzed in this study for the occurrence of ae that led to hospitalization 1 3 la radiologia medica ( 2020 ) 125 : 971980 pretreatment procedure angiography was performed between 2 and 6 weeks prior to 90y - sirt treatment . 
this was done to ( a ) determine whether there is a significant lung shunt that precludes therapy and ( b ) to embolize the right gastric artery and the gastroduodenal arteries with micro - coils . lung shunt was measured to reduce the risk of radiation pneumonitis . 
technetium - 99m - labeled macroaggregated albumin ( 99mtc - maa ) was administered into the main hepatic artery , or a branch thereof , depending on the area that was planned to be treated . 
arteriography was done with digital subtraction arteriograms ( dsa ) , and a transfemoral access was used in all patients ; none of the procedures was done via the radial artery . after angiography , patients were scanned with spect / ct ( discovery nm / ct 670ge healthcare using a low - energy high - resolution collimator ) for the lung shunt quantification . 
one reader with 3years of experience in volumetry measured the volume of the tumor and the whole liver by manually tracing the contours using dedicated volume analysis software ( voxar )  . 
dose was calculated as recommended by the vendor of the 90y - sirt microspheres ( sirtex ) with the body surface area ( bsa ) method [ 26 ]  . 
figure2 shows a typical pre - treatment procedure in a 51 - year - old male patient with liver metastases from a net . treatment : angiography and90y microsphere administration after pre - treatment procedure , 90y - microspheres ( 90y - sirspheres ; sirtex medical , sydney , australia ) were administered fig . 
the 90y - sir - spheres were prepared according to published standards . the same board - certified interventional radiologist , who had performed the pre - treatment angiography , performed the treatment angiography . 
approximately 1h after 90y - sirt , post - therapeutic bremsstrahlung spect was obtained to control and document the distribution of microspheres . figure3 shows a typical bremsstrahlung scan after treatment with 90y - sirt in the same 51 - year - old male patient with liver metastases from a net shown in fig.2. 
if symptoms persisted , the patients stayed in our hospital . 1 3 974 la radiologia medica ( 2020 ) 125 : 971980 to estimate whether the results of 36 patients are sufficient to assess average ambient dose rate after administration of 90y - sirt , sample size calculation according to eng was performed . 
assuming a sd of 2sv / h , a total width of the expected confidence interval ( ci ) of 1.5 sv / h and a statistical power of 0.95 , the estimated minimum needed sample size is 19 [ 27 ]  . collection ofclinical data andadverse events patient files were reviewed retrospectively , and the following data were collected : the treated area ( i.e. , whole liver , right lobe , left lobe , segmental ) , the first , second and third line therapy [ i.e. , liver surgery , liver ablation , transarterial chemoembolization ( tace ) , chemotherapy , none ] , the barcelona clinic liver cancer ( bclc ) stage ( i.e. , a , b , c ) , the childpugh stage ( i.e. , a , b , c ) , the tumor burden ( i.e. , < 25% , 2550% , > 50% ) , the sex of the patient and the presence / absence of portal vein thrombosis ( i.e. , none , segmental , branch , main ) , extrahepatic disease ( i.e. , yes , no ) , cirrhosis ( i.e. , yes , no ) , diabetes ( i.e. , yes , no ) , hypertension ( i.e. , yes , no ) and cardiovascular disease ( i.e. , yes , no )  . 
further , the number and type of ae ( i.e. , complications not causing hospitalization / readmission ) and sae ( i.e. , complications causing hospitalization / readmission ) after sirt were recorded . these clinical data were correlated with the occurrence of ae , and contingency coefficient and approximate significance were calculated . 
further , the group of patients with ae and no ae were compared to each other for the factors using two - sided t test : patient age , duration of sirt and applied activity . 
a p value of less than 0.05 was considered as significant . results pretreatment procedure andtreatment n ( total ) n ( female ) n ( male ) statistical analysis fig . 
four consecutive coronal slices are depicted ( ad ) confirming that the microspheres are deposited in the expected position table 1 demographics of the study population from which radiation exposure was measured all malignomas primary malignancies hepatocellular carcinoma cholangiocarcinoma hepatic hemangioendothelioma secondary malignancies ( metastasis from ) colorectal cancer anal cancer uveal melanoma gastric cancer breast cancer medullary thyroid cancer neuroendocrine tumor ovarian cancer pancreatic cancer radiation exposure measurement andsample size estimation after sirt , the ambient dose was measured in 1m distance with an ambient dosimeter . 
 none of the patients had a shunt fraction that was higher than 20% , and no shunt to nontarget organs was observed after embolization of the right gastric artery and the 1 3 la radiologia medica ( 2020 ) 125 : 971980 gastroduodenal arteries with micro - coils . 
as expected , since the majority of the energy is absorbed in the tissue , the resulting ambient dose rate was very low with a mean of 1.88 sv / h and was for all individuals below the limit values for discharge of patients . 
there are several studies published that examined the amount of ae [ 15 , 20 , 30 ] including one meta - analysis [ 19 ] ; however , to the best of our knowledge , no study hitherto has examined the amount of ae that made hospitalization necessary ( sae )  . 
these results might help to increase the cost - effectiveness of 90y - sirt and thereby the clinical value of 90y - sirt . the revenue of procedures varies widely depending on the country , the type of insurance and whether the procedure is performed on an inpatient or outpatient basis . 
in germany , for instance , it is not allowed by law to perform sirt on an outpatient basis and the patients are typically hospitalized for 34days [ 31 ]  . 
the revenue of a hospital in germany , 1 3 978 la radiologia medica ( 2020 ) 125 : 971980 if a procedure is performed on an inpatient basis , depends on the diagnosis - related groups ( drg )  . 
it has to be mentioned that the cost for the radionuclide is not taken into account in this calculation and the cost of the nuclide makes a huge proportion of the therapy . 
as mentioned above , this is different in different countries ; thus , the reduction in revenue , if sirt is performed on an outpatient basis , might make sirt economically unfeasible in some countries . in our study , we observed three patients with ae . 
pes is defined as fever without associated sepsis , nausea / vomiting and abdominal papes is a self - limiting condition although it has to be mentioned that pes is an indication for inpatient management [ 36 ]  . 
however , due to the low number of cases of three patients , the question remains , whether patients can be discharged home based on the clinical impression without developing a pes in the course . compared to all studies included in the meta - analysis of crowder etal . , our study has the highest number of cases ( 212 patients ) , and our total aes ( 5.2% ) are in the range of the published data ranging from 3 to 45% [ 19 ]  . furthermore , this study showed that neither patient age , duration of sirt , applied activity , treated area , pre - treatment , bclc stage , childpugh class , tumor burden , sex of the patient , portal vein thrombosis , extrahepatic disease , cirrhosis , diabetes , hypertension nor cardiovascular diseases are factors that identify patients prone to aes or hospitalization . 
in particular , the fact that the childpugh class is not a significant risk factor for hospitalization is remarkable , since in a recent study examining the safety of tace on an outpatient basis , a significantly higher risk of readmission for childpugh b / c patients was demonstrated [ 37 ]  . 
whether this is due to differences in the study population or because sirt is a better tolerated treatment requires further research . there seemed to be an association between diagnosis and occurrence of ae , although sample size with 10 ae / sae and 7 sae is too low to judge whether these findings are significant . 
interestingly , there was no sae observed in colorectal cancer and just one ae although sample size was with 55 patients higher than for other diagnosis in which saes were seen . 
thus , it seems possible that hypervascular lesions are a reason that aes occur more frequently , maybe because in hypovascular lesions the focal dose is lower than in hypervascular lesions ( i.e. , less pronounced tumor necrosis )  . 
the hypotension that had to be treated in icu might have been related to a carcinoid crisis caused by high levels of serotonin released from the damaged tumor cells [ 39 ]  . there are also some limitations to our study : ( 1 ) because of the retrospective design of the study , the reasons why 12 patients were planned initially as an inpatient are not evaluable since the reasons were not documented . 
additionally , due to the retrospective study design the decision why a patient had to be hospitalized , which was initially planned as an outpatient , depended on the treating physician . 
therefore , decisions might differ from clinician to clinician leading to some uncertainty in the exact value of sae needing hospitalization ; thus , our study could only examine the number of sae that caused hospitalization . 
in a group of patients with poor early responses , local disease control could not be achieved despite the use of recommended higher doses of brachytherapy . conclusion we could not determine the correlation between hpv contamination and patients who had early response intervention . 
but residual tumor of more than 2cm in diameter after external radiotherapy may be a predictor of failed local control and development of metastasis within a short time . keywords brachytherapy hpv local advanced cervical cancer residual volume introduction according to globocan 2018 data , cervical cancer is the fourth and most frequently seen cancer and cause of death among cancers observed in female population worldwide and ninth in turkey [ 1 , 2 ]  . 
in more than 90% of the patients , it has been observed that limited socioeconomic conditions have a noticeable influence in the development of cervical carcinoma [ 3 ]  . 
hpv is shown in the development of the disease , but its effect in response to treatment is not clear yet and testing of hpv is not routine in treatment . 
fourteen of * binnur dnmez ylmaz binnurdy@yahoo.com 1 department ofradiation oncology , okmeydani training andresearch hospital , stanbul , turkey 2 department ofradiation oncology , stanbul oncology hospital , stanbul , turkey more than 100 types are identified as high risk and occur most frequently with hpv16 , hpv18 , hpv45 and hpv56 [ 4 ]  . 70% of patients develop squamous cell cancer with hpv16 and cervical adenocarcinoma with poor prognosis with hpv18 [ 5 , 6 ]  . 
again , poor prognosis is reported in hpv - negative patients compared to hpv - positive patients [ 7 ]  . when the disease is diagnosed at a locally advanced stage , the patient is unable to access the option of surgical treatment and concomitant chemoradiotherapy is recommended [ 8 ]  . 
the american brachytherapy society ( abs ) treatment guidelines suggest that if residual tumor is below 4cm in diameter or a complete early radiological response is achieved , the patient responds well to external radiotherapy and recommends the total dose of eqd2 80gy sufficiently effective [ 5 ]  . 
when planning a multicenter embrace ii study in the light of the data obtained from embrace 1 and vol . : ( 0123456789 ) 1 3 982 la radiologia medica ( 2020 ) 125 : 981989 retro - embrace studies , it has been reported that local control rates cannot be increased despite high - dose radiotherapy even if the tumor volume is less than 30cm3 [ 9 ]  . 
in other words , even though a response to radiotherapy is achieved , a group of patients have treatment - resistant disease . does this small resistant group or early responders prior to brachytherapy belong to a specific hpv subgroup ? materials andmethods between 2015 and 2018 , 150 locally advanced cervical cancer patients who were treated at the university of health sciences okmeydani training and research hospital , radiation oncology clinic and the istanbul oncology hospital were evaluated with the approval of the ethics committee . 
the tests were conducted at acibadems labmed laboratories with the financial support of turkish society for radiation oncology ( apdp - trod - 2019 - 2 )  . patient andtreatment characteristics the study population consisted of 57 stage ib2 - iiic2 surgery - naive patients who were staged according to figo 2018 criteria and diagnosed as locally advanced squamous cell carcinoma of the cervix uteri . 
intensity - modulated external radiotherapy ( imrt ) was administered to our clinic volume which includes external and internal iliac lymphatics , uterus and cervix , parametrial area and upper half of the vagina at a daily dose of 1.82gy 5days a week totaling to 4550.4gy. 
the treatment dose was defined by volume and applied as a computer - based ( ct ) three - dimensional conformal confirmation , and the total dose was calculated as eqd2 . control examinations were performed quarterly after the end of treatment . 
at the subsequent control visits , evaluations with mri were performed every 6months . evaluation ofthetreatment response complete response was defined as lack of metabolic involvement observed in tumor areas in the pet - ct performed 3months after the treatment . 
 the diagnosis of local recurrence was based on examination of biopsy , and clinical findings and radiological evaluation after complete clinical and metabolic response were obtained . statistical evaluation in this study , statistical analysis was performed using ncss ( number cruncher statistical system ) 2007 statistical software ( utah , usa ) package prograin addition to descriptive statistical methods ( mean , standard deviation ) , shapirowilk normality test was used to evaluate the distribution of variables . 
for pairwise comparison of variables with normal distribution between two groups , mannwhitney u test and , for the comparison of qualitative data , chi - square test were used . area under roc curve was calculated to determine the place of variables of response rate to rt ( % ) , diameter and volume of the post - rt residual tumor ( termed as new tumor )  . 
three patients had multiple hpv , and in 24 ( 42% ) patients , hpv could not be detected ( table3 )  . in the hpv ( ) group , the mean residual tumor diameter and volume after external radiotherapy were significantly higher than the hpv ( + ) group ( p = 0.011 ) ( p = 0.046 ) ( table3 )  . 
and we found that early response to radiotherapy in a group of patients whom we investigated the possibility of treatment with a smaller dose was not due to a certain prerequisite that we still know . in the abs treatment guidelines , no specific histological subtype has been specified for doses recommended to patients with complete radiological response whose tumor regressed to a volume of less than 4cm3 [ 5 ]  . 
there was no statistically significant difference between the 3 - year survival rates , early response to external radiotherapy ( 90% ) and survivors with residual tumors ( 70% ) in the entire patient group . 
since three - dimensional conformal brachytherapy has been performed in our clinic since 2015 , we have not had our 5 - year results . the presence of hpv on the treatment response that has been reported to have an impact on the development of carcinoma of the uterine cervix was investigated [ 11 ]  . 
while inducing development of carcinoma of the cervix uteri , hpv inhibits the p53 and retinoblastoma ( prb ) tumor suppressor genes in the cell via the e6 and e7 oncoproteins . 
for this reason , squamous cell carcinomas which are more frequently seen and respond better to radiotherapy were evaluated in our study . in a french study evaluating the effect of hpv16 in response to radiotherapy , the association with radiotherapy with treatment response could not be demonstrated in squamous cell carcinoma of the cervix uteri due to variable response in the presence of hpv16 [ 14 ]  . 
the incidence rates of hpvnegative carcinoma of the cervix uteri were reported as 16% in japan , 7% in sweden and 1% in china [ 1719 ]  . when staging the patients before radiotherapy of carcinoma of the uterine cervix and subsequently evaluating the response to treatment , the interpretation of pet - ct results is decisive in the success of the treatment . 
reported that the response to treatment can be evaluated based on findings of pet - ct obtained on an average of 3months after the treatment of carcinoma of the cervix uteri and these responses will determine 5 - year survival rates [ 20 ]  . 
in particular , in patients with residual tumors over 2cm in diameter with high risk of metastasis who responded poorly to treatment in the early stages of the disease , radiobiological studies concerning fractional doses of brachytherapy or their frequency of application may be considered . conclusion because of the high risk of metastasis in patients with squamous cell carcinoma of the cervix uteri with residual tumor diameter greater than 2cm on mri after simultaneous treatment with cisplatin and external radiotherapy , radiobiological studies can be considered for non - standard brachytherapy regimens or different concomitant regimes . although concomitant chemoradiotherapy is a more successful treatment modality in patients with squamous cell carcinoma of the cervix uteri due to hpv , in the management of some variant hpv16and hpv - negative patients that we do not know , it fails in the achievement of local control and survival . 
since its effect on treatment is so controversial , it suggests that hpv indirectly affects the outcome . acknowledgements we would like to thank prof esra kaytan salam , istanbul university institute of oncology radiation oncology , prof sezer salam , gayrettepe florance nightingale hospital , rana konyaliolu , statistics , hlya yavuz , md , phd , university of health sciences zeynep kamil women and childrens diseases training and research hospital , department of pathology , prof seden kck , istanbul university institute of oncology radiation oncology , suzan deniz nol , md , phd , university of health sciences okmeydani training and research hospital radiology clinic and assoc . 
minor / major complications , hospitalization days , serum creatinine and gfr preand post - rfa ( compared using paired t test ) and post - operative pain ( evaluated with nrs after treatment ) were considered as safety indicators . 
 overall survival was also calculated ( kaplanmeier method )  . results of 35 patients , 30 / 35 had 1 treatment ( primary effectiveness rate 86% ) , 4 / 35 had 2 treatments and 1 / 35 had 3 treatments for residual disease . 
there were no relapses and no mid - long - term complications ; 3 minor ( 8% ) and 1 major ( 2.7% ) complications during perioperative period were reported . 
91.4% of all patients survived , with a median overall survival time of 65months . conclusions mid - term results show that ct - guided rfa with multitined expandable electrodes externally cooled with saline solution is an effective and safe treatment in patients with rcc - staged t1an0m0 . 
more than a half of the new cases are detected incidentally , and the number of cases of renal tumors has doubled during the past 50years [ 36 ]  . for many years , radical nephrectomy has been considered the best therapeutic approach for patients with rcc confined to the kidney . 
a mpr enhanced ct scan coronal view before rfa for esophytic rcc ( arrow ) in crossed kidneys ; b intraoperative ct scan : electrodes are well positioned within the lesion ; c 36 - month ct scan follow - up showing no contrast enhancement due to complete necrosis of the tumor 1 3 792 la radiologia medica ( 2020 ) 125 : 790797 fig . 
d 24 - month follow - up ct scan showing no contrast enhancement due to a complete necrosis of the tumor ( arrow ) with pumped saline solution ( intelliflow pump ) ( fig.3 ) ; target temperature in tissues to treat was about 100c . the needle was 25cm long and could cause variable extension of necrosis . 
in contrast with traditional devices , twenty - two tumors were on right kidney ( 56% ) , 15 on left kidney ( 38% ) , 1 on upper polar crossed kidney ( 3% ) and 1 on horseshoe kidney ( 3% )  . eleven lesions ( 28% ) were on upper pole of kidney , 18 ( 46% ) were central and 10 ( 26% ) were on lower pole ; 29 tumors ( 74% ) were exophytic , 8 ( 21% ) endophytic and 2 ( 5% ) were parahilar . rfa procedure approval of the local ethic committee was obtained . 
the treatment was performed under spinal anesthesia in all cases . thirty - one procedures ( 79% ) were performed with patient in prone position , 1 ( 5% ) on supine , 5 ( 13% ) on left side and 2 ( 5% ) on right side . 
hydrodissection was needed in 3 cases ( 10% ) as the mass tumor was too close to bowel . rfa was performed by an expert interventional radiologist . a radiofrequency monopolar system with a generation power of 250w was used ( rita medical system ) linked with a 4 - tined expandable electrode ( starburst talon ) cooled fig . 
3 multitined expandable radiofrequency electrode , externally cooled with saline solution ; note the saline drops on the tips of the electrode ( arrows ) 1 3 la radiologia medica ( 2020 ) 125 : 790797 saline solution was dropped in tissues by the 4 expandable electrode tines , to reduce tissue impedance and carbonization and to increase necrosis volume . contrast - enhanced ct scans included arterial phase , portal venous phase imaging of the ablated tumor and excretory phase to investigate the urinary tract . gantry laser and a metallic grid were used in a combined approach to target the lesion ; the position of the electrode inside the lesion was monitored with ct scan and multiplanar reconstruction images . monitoring of vital parameters ( blood pressure , heart rate and pulse oximetry ) was performed during procedure . imaging unenhanced and contrast - enhanced ct scans were done before rfa to study tumor features ( size , position , connection to adjacent organs , volume , and contrast enhancement ) and to confirm indication for treatment . a six - detector helical scanner with simultaneous acquisition ( somatom emotion 6 , siemens , erlangen , germany ) was used , with multiplanar reconstruction images for all cases in order to overcome the anatomical obstacles , with the following settings : 100kv , 90mas , 2 - mm collimation , 2.5 slice thickness with 1mm of reconstruction increment . tumors were classified as exophytic , endophytic or mixed on radiologic criteria . 
for mixed tumors , 2575% of the mass showed extrarenal extension . unenhanced and contrast - enhanced ct scans were performed at the end of the procedure to detect residual disease and to rule out perioperative complications . 
in case of residual disease , rfa was repeated in the same session . follow - up : unenhanced and contrast - enhanced follow - up ct scans were performed at 1 , 3 , 6 , 12months and every year thereafter , with the aim to detect residual disease or recurrent disease and midto long - term complications . 
4 a 86 - year - old male with left renal cell carcinoma ( arrow ) subsequently treated with rfa ; b 12 - month follow - up ct scan showing the absence of contrast - enhancing areas within the ablated tissue and the poor reduction in size of the tumor over time . 
we had 8 cases of residual disease , successfully treated with repeat ablation ( secondary effectiveness rate 100% )  . there was no recurrent disease on follow - up imaging . la radiologia medica ( 2020 ) 125 : 790797 a total of 39 rccs were treated : 28 lesions were < 3cm and 11 lesions > 3cm according to the gervais classification [ 14 ]  . after the first treatment , 24 of the 28 lesions < 3cm ( 86% ) and 8 of the 11 lesions > 3cm ( 73% ) were eradicated . 
causes of death were not related to renal cancer and were : pulmonary thromboembolism , advanced hepatocellular carcinoma and heart failure . discussion renal cell carcinoma accounts for 23% of all cancers , with a higher incidence in western countries [ 19 ]  . 
5 overall survival ( os ) evaluated using kaplanmeier curve : 91.4% of all patients treated with rfa survived , with a median os time of 65months 1 3 la radiologia medica ( 2020 ) 125 : 790797 fig . 
6 a minor complication in 86 - year - old male treated with rfa for esophytic rcc in the left kidney : subcapsular hemorrhage ( arrows ) on end procedure imaging control ; b ct scan after 6months : hemorrhage resolved ; c major complication in 70 - year - old female ( previous right nephrectomy ) , esophytic rcc in the left kidney , treated with rfa : perihilar leak of contrast medium ( arrows ) on end procedure ct scan ; d ureteral jj stenting for 15days , with no further complications there is common agreement in the literature that radical surgery and nephron - sparing surgery are equivalent in terms of both oncologic and functional outcomes [ 23 , 24 ]  . despite the number of studies reporting excellent results of the nephron - sparing techniques , investigations into ablative methods have expanded considerably , such as cryoablation and rfa . in 1997 , zlotta etal . 
 [ 25 ] reported the first clinical use of radiofrequency ablation for the treatment of localized renal masses . the american association of urology ( aua ) supports consideration for rfa , stating this technique as a viable option for t1a stage renal malignancies less than 4cm in size [ 26 ]  . the european association of urology shares consideration for rfa , reporting the recommendation to offer radiofrequency ablation to elderly and / or comorbid patients with small renal masses [ 27 ]  . in more details , clark etal . 
 [ 36 ] recorded a therapeutic success of 100% in a 3 - year follow - up . in the following years , many authors reported the safety and effectiveness of this technique [ 3743 ]  . our results , obtained by patients treated with the innovative externally cooled electrode , are in line with data reported in the literature on patients treated with other 1 3 796 la radiologia medica ( 2020 ) 125 : 790797 devices , in terms of safety , effectiveness and oncologic outcome . it is reported in the literatureand is common experiencethat tumors close to large vessels will suffer a heat sink , as regional vascular flow reduces the extent of the heatinduced damage [ 5 ]  . 
in this respect , the device used in our series ( starbust talon ) allowed monitoring of temperature by each needle inserted in the tumor mass , thus making the procedure effective even in the presence of large vessel adjacent to the targeted area . in addition , the cooling system of starbust talon helps maintain the temperature below 105c ( 221f ) thanks to a pump able to deliver precise amount of saline solution into the ablation zone . 
the final outcome was expressed as discharged or hospitalized patients into a medicine department or intensive care unit ( icu )  . results patients that had a rt - pcr positive for covid - 19 infection were 234 in total : 153 males ( 65.4% ) and 81 females ( 34.6% ) , with a mean age of 66.04 years ( range 1897 years )  . 
the following alterations were more commonly observed : 135 patients with lung consolidations ( 57.7% ) , 147 ( 62.8% ) with ggo , 55 ( 23.5% ) with nodules and 156 ( 66.6% ) with reticularnodular opacities . 
the rale score can be used in the emergency setting as a quantitative method of the extent of sars - cov - 2 pneumonia , correlating with an increased risk of icu admission . keywords infection coronavirus covid - 19 chest radiography diagnostic imaging * diletta cozzi dilettacozzi@gmail.com 1 department ofemergency radiology , university hospital careggi , largo brambilla 3 , 50134florence , italy 2 department ofclinical andexperimental medicine , institute ofdiagnostic imaging 2 , university ofsassari , sassari , italy 3 medical physics department , university hospital careggi , 4 medical physics unit , ausl toscana centro , pistoia , prato , florence , italy italy introduction at the end of 2019 a novel virus , named sars - cov - 2 ( severe acute respiratory syndrome coronavirus 2 ) , expanded globally from china with the first italian cases dating back to february 2020 [ 1 ]  . 
this new coronavirus causes a highly infectious disease , commonly called coronavirus disease 19 ( covid - 19 ) : lung infection can result in severe pneumonia up to more aggressive acute respiratory distress syndrome ( ards ) [ 2 , 3 ]  . 
genetic sequencing of sars - cov - 2 has permitted the rapid development vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 730737 of real - time reverse transcription polymerase chain reaction ( rt - pcr ) of viral nucleic acid , and nowadays this is the diagnostic gold standard [ 2 ]  . 
radiological evaluation of patients with clinicalepidemiological suspect of covid - 19 is mandatory , especially in the emergency department ( ed ) while waiting for rt - pcr results , in order to have a rapid evaluation of thoracic involvement . 
the recent covid - 19 radiological literature focuses primarily on computed tomography ( ct ) findings , which is more sensitive and specific than chest x - ray ( cxr ) : in particular , in china ct is used as a first - line diagnostic method for covid - 19 [ 4 , 5 ]  . 
nonetheless , it has to be remembered that performing ct scan is not easy during this pandemic , considering not only the excessive radiation exposure especially to younger patients but also the mandatory scanner disinfection procedures that have to take place . 
the most italian hospitals are employing cxr as the first - line method , with faster results comparing with those of rt - pcr , especially by using portable x - ray units which reduce the movement of patients and so minimizing the risk of cross - infection [ 68 ]  . 
therefore , the purpose of our study is to better understand the main radiographic features of covid - 19 pneumonia , by describing the main cxr findings in a selected cohort of patients , also correlating the radiological appearance with rt - pcr examination and patients outcome ( intended as discharged or hospitalized into a medicine department or intensive care unit )  . image acquisition andanalysis all cxrs were acquired as digital radiographs with the same portable x - ray unit ( fdr go plusfujifilm , italia ) in the isolation wards of our ed . 
an independent and retrospective review of each cxr was performed by two thoracic radiologists in order to define the number of radiological suspects of covid - 19 infection ; after this , they defined the predominant pattern of covid - 19 pneumonia presentation in patients with a positive rtpcr . 
radiographic features including consolidation , ground - glass opacities ( ggo ) , pulmonary nodules and reticularnodular opacities were diagnosed according to the fleischer society glossary of terms [ 9 ]  . 
moreover , cxrs were assessed for the presence of a specific distribution of the disease ( mostly peripheral or perihilar predominance ) , monolateral ( right or left lung ) or bilateral disease , upper or lower or diffuse predominance . 
following rale indications , each cxr was given a score between 0 and 48 , ranging from the absence of any pathological sign ( score 0 ) to the complete pathological involvement of lung parenchyma ( score 48 )  . 
the score was separately assessed by each of the two radiographers . materials andmethods patients selection andinclusion criteria statistical analysis cxrs of patients with clinicalepidemiological suspect of covid - 19 infection performed at the ed of our university hospital from march 1 to march 31 , 2020 , were retrospectively reviewed . 
inclusion criteria were : patients age between 18 and 99 years , rt - pcr nasopharyngealthroat swab and cxr performed immediately at the ed access , clinicalepidemiological data suspect for covid - 19 infection and their duration at the time of ed access ( fever , cough , dyspnea , respiratory impairment , diarrhea , asthenia , myalgia and dysgeusia )  . 
the final outcome was expressed as discharged or hospitalized patients into a medicine department or into an intensive care unit ( icu )  . statistical analysis was performed with spss ( spss chicago il , usa )  . 
analysis of variance ( anova ) was performed to detect possible differences among rale score estimated in the following groups : discharged patients , hospitalized patients into a medicine department , hospitalized patients into an icu ( respectively , group 1 , 2 and 3 in the following )  . 
homogeneity of the variance was established between groups by means of levene test , to adequately choose the post hoc test : bonferroni in case of detected significant homogeneity of variance , otherwise games - howell . 
statistical significance threshold was set at p = 0.05. 1 3 732 results we found 482 patients fulfilling the following selecting criteria : presence of clinicalepidemiological suspect of covid - 19 infection and rt - pcr and cxr performed at table 1 radiographic findings of our cohorts of covid - 19 patients covid - 19 radiological features normal baseline cxrs abnormal baseline cxrs reticularnodular opacities ground glass opacities consolidation vascular congestion signs cardiomegaly nodules pleural effusion pneumothorax distribution : peripheral perihilar diffuse basal predominance superior predominance right lung left lung bilateral la radiologia medica ( 2020 ) 125 : 730737 the ed admission . 
patients with a rt - pcr - positive results for covid - 19 infection were 234 : of these , 153 were males ( 65.4% ) and 81 females ( 34.6% ) , with a mean age of 66.04 years ( range 1897 years )  . 
the following alterations were more commonly observed : 135 patients with lung consolidations ( 57.7% ) , 147 ( 62.8% ) with ggo , 55 ( 23.5% ) with nodules and 156 ( 66.6% ) with reticularnodular opacities . 
a total of 34 ( 15.3% ) patients died in the 30 days included in this study ( 9 in group 2 and 25 in group 3 )  . descriptive statistics of rale score for each group is reported in table 4 . 
four cases of advanced lung disease with diffuse consolidations and interstitial involvement of patients older than 80 years at the emergency department inhomogeneities of variances among groups 1 , 2 and 3 ; thus , gameshowell post hoc test was adopted . 
the italian society of radiology ( sirm ) recommends using cxr as a first - line imaging tool and reserves to chest ct others additional roles as the identification of covid - 19 pneumonia typical features in selected cases [ 68 , 11 ]  . 
multiple recent studies indicate that cxr may not have the diagnostic power of ct , but it still has a role in managing the pandemic [ 6 , 12 , 13 ]  . 
in fact , although ct has a high sensitivity ( around 9798% ) , it has a very low specificity in detecting typical features of sars - cov - 2 pneumonia [ 12 , 14 , 15 ]  . 
our study reveals a cxr sensitivity substantially in accordance with the most recent literature ( 68.1% ) , where a variability between 69 and 90% is described [ 12 , 13 ]  . 
2 box and whisker plot of rale score estimated in each group defined by outcome : discharged patients ( group 1 ) , hospitalized patients into a medicine department ( group 2 ) , hospitalized patients into an intensive care unit ( group 3 )  . 
3 chest x - ray in three patients with severe respiratory failure , immediately intubated at the arrival in emergency department and transferred to icu more complex to perform ct scans , especially considering the disinfection procedures that have to take place after each examination . 
our cxr was performed in a period between 2 and 15 days after the onset of symptoms , with cases of more advanced lung involvement in patients around the tenth day of illness . 
we applied the rale score , used for the quantification of lung involvement in ards [ 10 ] , in order to standardize and objectively quantify the radiographic report and to produce a prognostic score at the patients admission . 
 we found a significant statistical correlation between rale score and patients outcome , with a rale score higher than 15 points which correlates with an increased risk of being admitted to icu . 
obviously , every hospital in the world has its own " radiological " organization and management of the patient with sars - cov - 2 infection , but it is always necessary to fig . 
images in a , b and c show three cases of male patients with subpleural consolidations and bilateral involvement 1 3 736 la radiologia medica ( 2020 ) 125 : 730737 fig . 
patient in a shows a prevalent right lung disease with diffuse reticularnodular thickening of peribroncho - vascular interstitiu patient in b shows a diffuse ground glass opacity mainly in the perihilar and subpleural region bilaterally maintain a balance between the safety of health professionals and the diagnostic resources that we can use in this pandemic [ 16 ]  . our work has several limitations : first of all , the retrospective nature of the study and the lack of a non - covid - 19 control group in the study of the prognostic score , thus limiting evaluation of sensitivity and specificity of cxr . 
in addition , there is a difference in size between the three prognostic groups and a difference in the period of time between the onset of symptoms and cxrs execution . 
although there are some data about ai and chest ct , neural network applied to chest radiographs needs further investigations and it is too early to apply this new technology in the clinical practice [ 7 , 18 , 19 ]  . in conclusion , we describe the main features of covid19 thoracic involvement on cxr in our cohort of patients . 
 the rale score can be used in the emergency setting as a quantitative method of the extent of sars - cov - 2 pneumonia , correlating with an increased risk of icu admission . 
the results of our study could help radiologists in identifying the highest risk patients , allowing for timely initiation of treatments currently available against sarscov - 2 infection . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . 
the employed modes were ovo , voo and vvi for one sheep and oao , aoo and aai for the other ( unipolar and bipolar configuration of pacing and sensing for both )  . 
histopathological examination of the cardiac tissue around the lead tip was performed 4weeks post - imaging . results no significant changes in device position or configuration were observed during or after mri . 
reasons for contraindication were due to reports of several different adverse events occurring with mri , including variations in sensing , lead impedance and capture threshold ; occurrence of poweron - reset , which is defined as the eversion of the device to a backup programming with posing a greater risk of pacing output inhibition and activation of antitachycardia therapies to the patient ; transient reed switch activation ; battery voltage decrements ; and cardiac injury due to heating at the leadtissue interface [ 26 ]  . although mri - conditional devices now exist , eight million people have a non - mri - conditional device implanted and 5075% of patients with non - conditional devices are expected to need mri during their lifetime [ 7 , 8 ]  . 
it is not clear whether removal or replacement of the cardiac device is safer than proceeding with an mri in patients with nonmri - conditional pacemakers / cardioverter defibrillators [ 9 ]  . in 2016 , camacho etal . 
despite the presence of multitude of studies that have found mri safe in patients with non - mriconditional cardiac devices [ 1121 ] , many patients with such cardiac devices are denied for mr scans [ 22 , 23 ]  . 
the situation gets even more complex when imaging of an area that contains the cardiac device , as in neck or chest mri , is required , because a larger power deposition over the field of imaging is expected , and hence , the likelihood of device displacement and / or malfunction is higher [ 24 ]  . studies regarding the safety of neck or chest mri in patients implanted with a non - mri - conditional cardiac device are scarce and inconclusive . 
to investigate the mri safety of two non - mri - conditional devices , the present study used a sheep model to examine the effects of 1.5t mri on the function of two non - mri - conditional pacemakers after imaging . 
standard diet restriction and fluid therapy were started 24h prior to pacemaker implantation . anesthesia was induced using intravenous ketamine hydrochloride ( 2.2 mg / kg ; rotexmedica , germany ) and xylazine ( 0.1mg / kg ; alfasan , estonia )  . 
after shaving , routine sterile skin preparation and draping , in sheep 1 the left jugular vein was accessed following the seldinger technique ( fig.1a ) [ 25 ]  . 
the a - channel was closed by a plastic pin . sheep 2 dual - chamber , adapta addr01#nwb 914537 ( medtronic , dubl ireland ) , voltage = 2.79 , longevity = 811.5years , battery impedance = 368 , active lead impedance = 344 ( unipolar ) and 401 ( bipolar )  . 
the v - channel was closed by using a plastic pin . materials andmethods animal preparation andpacemaker insertion mri ofthesheep following institutional animal care committee approval , this experimental study was carried out on two adult male sheep weighing 42kg ( sheep 1 ) and 53kg ( sheep 2 )  . 
a veterinarian approved the general health status of the animals . during 1 - week stay in a well - ventilated area at room temperature located within the institutions animal laboratory , on day five postoperation , the animals were transferred to the department of radiology and mri of the cervical and thoracic regions was performed using a 1.5 t machine ( magnetom avanto 18 - channel q engine ; siemens healthcare , erlangen , germany ) under general anesthesia as described earlier . 
each sequence lasted two minutes . to intensify possible effect of magnetic field on pacemaker movement / dislodgement , a 6 - element body coil and 4 - element neck matrix coil were placed around the neck and chest of the animals . 1 3 la radiologia medica ( 2020 ) 125 : 706714 pacemaker setting andinterrogation device interrogation was performed at baseline ( before imaging ) , immediately after acquiring each sequence , and 48h after mri . the pacemakers were used in the single - chamber mode . 
 during mri , the pacemaker was set to ovo , voo , vvi ( unipolar ) and vvi ( bipolar ) modes in sheep 1 and oao , aoo , aai ( unipolar ) and aai ( bipolar ) in sheep 2 . 
initial electrocardiograms showed normal sinus rhythheart rate was 92 beats / minute for sheep 1 and 84beats / min for sheep 2 . pacemaker parameters at baseline , immediately after acquiring each sequence and 48h after mri are set out in tables2 and 3 . 
six different pacemaker modes including ovo , voo and vvi , oao , aoo and aai , both with unipolar and bipolar configuration of sensing and pacing models , were tested . 
mri examination with pacemakers placed in the magnet isocenter did not cause any clinically significant adverse event or pacemaker dislodgement , torque or movement , even after using extra cervical gradient coils . 
maximum noise was seen during diffusionweighted imaging ( a ) , and minimum noise was observed during t2 - weighted imaging ( b ) no significant changes in device parameters were detected immediately after each sequence and 4weeks after mri . adverse events associated with cardiac devices are primarily due to the exposure of the device to the static magnetic field , radiofrequency ( rf ) field and / or gradient magnetic field . 
gradient magnetic fields are responsible for fluctuations in the sensing adequacy of pacemakers [ 27 , 28 ]  . proximity of the generated rf energy and magnetic gradient field to the implanted cardiac devices can increase the likelihood of complications in carriers [ 29 ]  . 
focal chronic inflammatory cells infiltration and degenerative changes in myocytes ( a , b ) and mild necrosis and fibrosis ( c ) are noted ( h&e ) associated with long - term right ventricular sensing changes in another study [ 5 ]  . 
although the authors reported no clinically significant long - term adverse events , immediately after mri patients with thoracic imaging experienced insignificant reductions in right atrial and right ventricular lead sensing . 
 [ 34 ] examined the feasibility and safety of cardiovascular mri ( 1.5t ) in patients with both mr - conditional or non - mr - conditional cardiac implantable electronic devices . 
compared to brain mri cases , thoracic mri patients were not significantly different in terms of preand post - imaging device parameters or adverse events . post - mri changes in lead parameters such as sensing , impedance and capture threshold might be partly due to heating at the lead - tissue interface and consequent myocardial thermal injury [ 4 , 29 ]  . 
cardiac troponin t did not differ significantly before and after thoracic mri examinations in patients with non - mri - conditional cardiac devices in another study [ 35 ]  . 
 however , some studies have found mri - induced temperature increases of cardiac device leads in the range of cardiac tissue ablation [ 27 ]  . besides potential clinical consequences that may result from malfunctioning cardiac devices after mri exposure , device - related artifacts that may affect accurate diagnosis are also important . 
 [ 37 ] reported the best quality of thoracic mri with fast gre sequences in patients with cardiac devices , the worst quality of image was seen during diffusion - weighted sequences in our study . 
 [ 27 ] , who reported diagnostic with artifacts in 14 / 15 studies and partially diagnostic in 1 / 15 study in patients with implanted conventional cardiac devices after thoracic mr scans . 
this finding is possibly due to rapidly and powerfully switching gradients that normally occur with dw imaging [ 38 ]  . it has been suggested that the number of sequences determines actual rf exposure and thus the severity of potential complications in association with mri in cardiac device carriers [ 33 ]  . 
in the present study , we acquired five mr sequences in each sheep with no adverse effect on the pacemaker functionality or integrity . previous studies have excluded patients with acutely ( i.e. , < 4weeks ) implanted pacemakers because of the fear of device movement in the magnetic field [ 32 ]  . 
in our study , we did not see any device dislodgement / movement after mri was conducted within 1week after pacemaker implantation , noting that the magnetic field was even enhanced by using extra cervical coils . 
likewise , in line with two other studies , we showed that the time between pacemaker implantation and imaging is not a major determinant in examining the effect of mri on the function of pacemakers [ 33 , 39 ]  . missing control groups and inability of extrapolating our results to other models of pacemakers and mri scanners that operate at different field strengths are the main limitation in this study . conclusion this study showed that 1.5t mri in sheep with non - mriconditional pacemakers placed acutely ( < 1week ) in the field of imaging was safe . 
in this letter to the editor , we would like to highlight the rising role of mrl , pointing out the advantages of both the non - contrast and contrast - enhanced approach , in lymphatic vessels study . keywords non - contrast magnetic resonance lymphangiography lymphedema segmentation volume dear editor , we have read with great interest the paper by doctor cellina m . 
and colleagues , entitled volumetric analysis of noncontrast magnetic resonance lymphangiography in patients affected by lower extremities primary lymphedema [ 1 ]  . the authors have successfully investigated non - contrast magnetic resonance lymphangiography ( mrl ) for the volume calculation of lower extremities in ten patients affected by primary lymphedema . 
since peripheral lymphedema is associated with limb swelling , a reduction in * susanna guerrini guerrinisus@gmail.com maria antonietta mazzei mariaantonietta.mazzei@unisi.it 1 department ofmedicine andsurgery , section ofradiology , azienda ospedaliera universitaria di parma , viale antonio gramsci 14 , 43126parma , italy 2 department ofradiological sciences , diagnostic imaging unit , azienda ospedaliera universitaria senese , viale bracci 10 , 53100siena , italy 3 department ofmedical , surgical andneuro sciences , diagnostic imaging , university ofsiena , azienda ospedaliera universitaria senese , viale bracci 10 , 53100siena , italy the volume of the limb can be considered an objective mark of response to treatment [ 1 ]  . as experienced radiologists in this niche field , we would like to underline that the role of mrl in patients suffering from lymphedema is also to plan the best surgical treatment , such as vascularized lymph node transfer ( vlnt ) and lymphaticovenous anastomosis ( lva ) , a super - microsurgical treatment arranged to obtain a spontaneous shunt to surpass the site of the lymphatic obstruction conducting the lymphatic flow to the venous system [ 2 ]  . 
in this context , while non - contrast mrl and in particular heavily t2 - weighted and stir sequences allow to accurately calculate the volume of the limbs and to display the location and the extension of lymphedema , on the other hand these sequences may not be sufficient for a surgical treatment planning , especially lva treatment . 
for this purpose , in our experience , contrastenhanced mrl seems to be superior to non - contrast mrl not only to identify lymphatic vessels but also to provide a lymphatic functional assessment , since the vessels that drain the contrast agent have at least a residual undamaged lymph pump [ 4 ]  . 
simultaneous venous enhancement may be a potential confounding factor ; however , morphological criteria and dynamic evaluation at different times , after contrast agent administration , usually solve the dilemma [ 2 , 5 ]  . 
at present , there is no standard consensus on how to perform mrl ; however , contrast and non - contrast mrl vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 798799 may be complementary or used on their own , on the basis of different clinical issues . anyway , the take - home message of this letter should be that today mrl is the gold standard technique to investigate primary and secondary lymphedema , easy and safe . 
 contrast - enhanced mrl can provide detailed anatomic and functional information of lymphatic vessels , useful for surgical treatment planning and complication assessment , while to follow - up the treatment results , non - contrast mrl , especially using volume calculation , as suggested by cellina and colleagues , could be sufficient itself for an objective mark of response . funding no funding was obtained for this study . compliance with ethical standards in patients affected by lower extremities primary lymphedema . 
mazzei ma , gentili f , mazzei fg , gennaro p , guerrieri d , nigri a , gabriele g , weber e , fausto a , botta g , volterrani l ( 2017 ) high - resolution mr lymphangiography for planning lymphaticovenous anastomosis treatment : a single - centre experience . 
gennaro p , borghini a , chisci g , mazzei fg , weber e , tedone clemente e , guerrini s , gentili f , gabriele g , ungari c , mazzei ma ( 2017 ) could mri visualize the invisible ? an italian single center study comparing magnetic resonance lymphography ( mrl ) , super microsurgery and histology in the identification of lymphatic vessels . 
mazzei fg , gentili f , guerrini s , cioffi squitieri n , guerrieri d , gennaro p , scialpi m , volterrani l , mazzei ma ( 2017 ) mr lymphangiography : a practical guide to perform it and a brief review of the literature from a technical point of view . 
in this study , we sought to evaluate the existence of a correlation between specific anthropometric parameters and the size of some ankle tendons measured on mri , in particular those mostly used as graft in ankle surgery . methods we recorded gender , height , weight , and body mass index ( bmi ) of 113 patients ( 57 females ; mean age : 42 18 ) who underwent ankle mri . 
mri measurements performed by a radiologist were : axial shortest diameter of achilles ( at ) , posterior tibialis ( ptt ) , flexor digitorum longus ( fdlt ) , flexor hallucis longus ( fhlt ) , peroneus longus ( plt ) , and anterior tibialis ( att ) tendons , intermalleolar distance ( id ) and talus width ( tw )  . 
gemelli , rome , italy 4 musculoskeletal section , diagnostic imaging department , hospital universitario de la fundacion santa fe de bogota , bogot , colombia 5 dipartimento di scienze biomediche perla salute , universit degli studi di milano , milan , italy 6 scuola di specializzazione inradiodiagnostica , universit degli studi di milano , milan , italy vol . : ( 0123456789 ) 1 3 764 introduction over the last years , tendon transfer has become a common surgical procedure around the ankle , used to treat chronic lateral ankle instability and to correct foot deformities [ 1 ]  . 
chronic lateral ankle instability is the most frequent complication of ankle sprains , developing in about 20% of patients after sports injury and mainly due to an anterior talofibular ligament ( atfl ) tear [ 2 ]  . 
direct repair of atfl and calcaneofibular ligament is only possible when the residual ligament is resistant ; otherwise , tendon grafting is the main surgical option to restore the anatomy [ 3 ]  . 
 in ankle surgery , anterior tibial ( att ) and posterior tibial ( ptt ) tendons are the two most frequently used as grafts , but also peroneus longus ( plt ) , flexor digitorum longus ( fdlt ) , and flexor hallucis longus ( fhlt ) tendons have been used for tendon transfer surgery [ 4 ]  . 
att transfer has been reported to provide optimal results in patients with calcaneal foot deformity secondary to myelomeningocele , post - polio correction , hallux rigidus , and in previously treated congenital clubfoot [ 5 ]  . 
this procedure is done using an ipsilateral split / turn - down autograft of the att in management of isolated att rupture having shown to be a better treatment option than other tendon autografts [ 6 ]  . 
other less common uses of the ptt have been reported in literature , including the reconstruction of the achilles tendon ( at ) in a patient suffering from cerebrotendinous xanthomatosis [ 9 ] or to repair att injuries [ 10 ]  . 
plt transfer is generally used to reconstruct the lateral ankle ligaments [ 11 ] , to augment the static stabilizers of the medial column in cases of instability secondary to spring ligament rupture [ 12 ] , and to reduce tibio - talar tilt in advanced flatfoot deformity [ 13 ]  . 
further , fdlt transfer combined with medializing calcaneal osteotomy is generally used to treat early stages of ptt dysfunction with acquired adult flatfoot deformity [ 4 ]  . although the choice of the tendon to be used in foot and ankle surgery is mainly dictated by surgical proximity of the normal function of the tendon to be transferred , graft failure depends on several factors , including the capability of the grafted tendon to adequately transfer the motor power , which in turn is related to the integrity and to the length of the tendon itself . 
in 2012 , cohen and cabral reported undetected weakness of the peroneal tendons as a possible cause of poor results in patients with plt transfer with drop - foot secondary to hansen disease [ 15 ]  . 
in this setting , although la radiologia medica ( 2020 ) 125 : 763769 ultrasound is indicated and recommended to evaluate ankle tendons [ 17 ] , magnetic resonance imaging ( mri ) is used as a valuable tool to assess ankle instability and to evaluate tendon status while providing a panoramic evaluation of all bony and soft tissue structures [ 4 , 18 ]  . following a study that reported an association between small graft size and increased risk of for anterior cruciate ligament ( acl ) reconstruction failure [ 19 ] , a recent study has investigated the correlation between anthropometric data and knee tendons size measured on knee mri [ 20 ]  . 
thus , we sought to evaluate the existence of a correlation between specific anthropometric parameters and the size of some ankle tendons , in particular those mostly used as graft in ankle surgery . materials andmethods study population this study was approved by our institutional review board with a waiver for patients informed consent . 
we included all mri scans that were performed for non - traumatic paout of them , we also excluded patients who presented with tendon abnormalities including degenerative changes ( signal intensity abnormalities , thickening , thinning , tenosynovitis ) and partial or complete tears . 
 finally , our series included 113 ankle mri examinations of 113 patients ( 57 females , 56 males ; mean age standard deviation 42 18years , range 1878years )  . 
these records are routinely acquired by a nurse before every mri examination . mri protocol andimage analysis ankle mri examinations were obtained with a 1.5t mri unit ( avanto system ; siemens , erlangen , germany ) using a dedicated coil . 
our imaging protocol included : sagittal t1 - weighted [ repetition time ( tr ) / echo time ( te ) of 500 / 9.2ms , slice thickness 3mm ] , sagittal stir ( tr / te 3990 / 29ms , inversion time 160ms , slice thickness 3mm ) , axial t2 - weighted ( tr / te 4500 / 81 ms , slice thickness 1 3 la radiologia medica ( 2020 ) 125 : 763769 3mm ) , axial fat - saturated proton - density weighted ( tr / te 4120 / 32ms , slice thickness 3mm ) , coronal t2 - weighted ( tr / te 4500 / 81ms , slice thickness 3mm ) , and coronal fat - saturated proton - density weighted ( tr / te 4120 / 32ms , slice thickness 3mm )  . 
our ankle mri protocol had an average scan time of 16ma radiologist with 6years experience in musculoskeletal radiology performed all ankle mri measurements using a routine picture archive and communication system workstation ( sectra , stockholm , sweden )  . since no previous mri studies attempted to investigate the role of ankle tendon graft sizes , no standard criteria exist to perform these measurements . 
to standardize our results , we decided to measure the shortest axial diameter of all involved tendons ( at , ptt , fdl , fhl , plt , and att ) on the two consecutive slices immediately distal to the myotendinous junction when the muscle belly disappears . 
intermalleolar distance ( id ) and talus width ( tw ) were measured as the shortest distance between the inner side of each malleolus and between the lateral walls of the talar dome , respectively . 
we also calculated the time needed to perform all measurements . figure 1 shows a representative case from our study population . statistical analysis continuous variables are reported as mean standard deviation . 
full data is summarized in table1 . after having chosen the axial slices to perform the measurements , an average time of 21s and 9s were required to measure once all ankle tendons and bony diameters , respectively . discussion our main finding was that some anthropometric / demographic data were associated with ankle tendons diameters , each to a different extent , thus confirming the potential predictive influence of this data on the measure of the grain particular , ptt and fdlt showed a significant correlation with id and tw , att with weight , id and tw , while plt and at only with id and weight , respectively . in the wide range of surgical procedures existing for correction of both congenital and acquired pathologic conditions involving the ankle , tendon transfer plays a main role [ 21 ]  . 
an important chapter is that consisting of the so - called anatomic repair in chronic lateral ankle instability , which involves the use of synthetic grafts as well as tendon autografts or allografts . 
several previous studies , mainly related to acl reconstruction , have shown that the graft diameter has a great impact on complications after surgery [ 19 , 20 , 2227 ]  . 
in literature , we found several studies performed both on anatomical cadavers and on mri studies to establish length and size of the tendon graft , but only few specifically focused on the ankle [ 28 ]  . 
although the impact of ankle tendons diameter on the efficacy of the grafts has been scarcely investigated , it is reasonable to think that , as for acl reconstruction , also in these procedures the size of the tendons used for transfer could affect the outcomes of surgery , as also postulated by cohen and cabral [ 15 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 763769 766 fig . 
axial fat - saturated proton density - weighted images show the measurements of the shortest axial diameter of theankle tendons at two different levels ( a , b ) , specifically at , ptt , fdlt and att at a proximal level ( a ) , fhl and plt at a more distal level ( b )  . 
note : at achilles tendon , ptt posterior tibial tendon , fdlt flexor digitorum longus tendon , att anterior tibial tendon , fhlt flexor hallucis longus tendon , plt peroneus longus tendon , id intermalleolar distance , tw talar width in our study , id has demonstrated to be the strongest parameter associated to ptt , fdlt , att and plt diameters . 
this data is in line with previous studies reporting a lower average graft size in female patients subjected to acl reconstruction with hamstring grafts [ 19 , 29 ]  . 
however , it is still unclear whether gender could be an independent predictor for graft failure , since controversial results have been reported in this setting , with some authors having considered female gender a risk factor for hamstring graft failure after acl reconstruction [ 19 , 30 , 31 ]  . the choice of using a tendon or another for grafting is strictly dependent on the type of planned procedure . 
indeed , biomechanical and clinical studies have demonstrated the important predictive role of graft size and resistance with clinical outcome after surgery , especially for acl reconstruction [ 19 , 32 ]  . 
thus , preoperative awareness of graft size is desirable to have a good outcome after surgery or also to consider alternative repair approaches . mri is a repeatable examination , usually performed before ankle surgery , and the measurements of tendons size and of tw and id are easily and quickly obtained with mri . 
we decided to include in our analysis only those tendons generally used as graft for ankle surgery , thereby excluding the peroneus brevis , the extensor hallucis longus , and extensor digitorum longus tendons . 
 mri can also be helpful in pre - operative setting to assess the status of the remaining tendons , ligamentous , retinacula , bony and osteochondral structures , in order to evaluate abnormalities that can predispose to ankle instability , thus adding essential information for patients management [ 33 ]  . 
indeed , the most frequent anatomic variants such as peroneus quartus muscle , flat / convex retromalleolar groove , os peroneum , and pseudosubluxation of the peroneus brevis tendon , do not hinder our tendon and bony measurements . 
another common variant that , however , was not observed in our series , is the low - lying peroneus brevis muscle belly that could partly affect the axial measurement of the peroneus brevis tendon itself . 
in these cases , we can postulate that coronal images could be helpful to measure the tendon size distal to the myotendinous junction . some limitations of this study should be taken into account . 
although this was outside the scope of this paper , future studies may be aimed to understand whether ultrasound could reliably provide the same information of mri on tendon sizes at lower costs [ 35 , 36 ]  . 
these results might be helpful for preoperative planning by orthopedic surgeons who use healthy tendons for surgical stabilization procedures in order to identify the best grafuture studies could investigate the graft failure risk associated with tendon graft measurements obtained by mri . funding this study did not receive any funding . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval this study was approved by our institutional review board with a waiver for patients informed consent . 
four datasets were constructed : 109 images from hospital #1 for training ( set 1 : 1 - mm image slice thickness ) , 47 images from hospital #1 for internal validation ( sets 2 and 3 : 1 - mm and 10 - mm image slice thicknesses , respectively ) , and 47 images from hospital #2 for external validation ( set 4 : vastly different from training dataset )  . 
while radiomics is an objective and quantitative way to assess various imaging features , it may also provide great potential to capture more information than conventional imaging features , thereby providing valuable information for personalized therapy [ 3 , 4 ]  . a pubmed / medline search revealed that over 100 studies have been published which show prognostic information for tumor outcome based on radiomics features . 
several authors have published promising results in computed tomography ( ct ) , suggesting that radiomics features are potentially useful for predicting patient outcome or treatment response in several tumor types , including liver [ 5 , 6 ] , lung [ 79 ] , breast [ 10 ] , oropharynx [ 11 ] , head and neck [ 8 ] , and rectal [ 12 ] cancer . 
however , a systematic review of radiomics studies [ 13 ] underlined the need for validating radiomics models using independent patient cohorts in vol . : ( 0123456789 ) 1 3 698 la radiologia medica ( 2020 ) 125 : 697705 multicenter settings [ 13 ]  . 
therefore , analysis by using clinical patient images acquired with different ct scanners , different protocols , and potential anatomical and physiological differences could impair results [ 2224 ]  . 
some authors have advised that the conclusions must be treated with caution because several radiomics features can vary greatly with slight changes in the image [ 2 , 14 ]  . 
this is obviously a severe limitation for the reproducibility of radiomics models and their transfer to clinical practice . in view of the potential variability of radiomics models , among different datasets , there is a need of studies testing the reproducibility of radiomics features on different imaging data , considering the variability of imaging protocols . 
 some authors found that the peritumoral region captured by radiomics analysis may possess valuable predictive information for treatment response and outcome in glioblastoma multiforme , breast cancer , and rectal cancer [ 10 , 12 , 25 ]  . 
in a previous study , our group built a ct - based peritumoral radiomics ( pt - ro ) prediction model and demonstrated its efficiency in predicting early recurrence of hepatocellular carcinoma ( hcc ) [ 26 ]  . 
the aim of the study was to test the reproducibility of this ct - based pt - ro prediction model with an independent external validation cohort and preliminarily explore its possible influence factors . materials andmethods patients anddatasets the study cohort included patients who underwent resection or ablation with hcc ( histopathologically confirmed ) from january 2010 to september 2015 in hospital #1 and from january 2015 to september 2015 in hospital #2 . inclusion criteria : ( 1 ) patients with hcc , histopathologically confirmed , who had resection or ablation with curative intention ; and ( 2 ) those who had preoperative ct performed within one month prior to treatment . 
exclusion criteria : ( 1 ) those who had a history of previous hcc treatment or a combination of other malignancies ; ( 2 ) those who received a combination of other anti - tumor treatments , such as transarterial chemoembolization ( tace ) , targeting therapy , and radiotherapy , or palliative care ; ( 3 ) those who had major thrombosis in a branch of the portal vein , hepatic vein thrombosis , abdominal lymph node metastasis , or distant metastases that were confirmed with pathology or imaging ; or ( 4 ) those who were followed up for < 2years after curative therapy . the study population included 156 patients in hospital #1 , randomly divided into a training dataset ( 109 cases ) and an internal validation dataset ( 47 cases ) with a ratio of 7 : 3 , and 47 patients from hospital #2 as the external validation cohort . 
figure1 depicts the patient grouping flow diagram . followup andearly recurrence ofhcc the endpoint of the study was early recurrence of hcc , which was defined as the presence of new intrahepatic fig . 
1 patient grouping flow diagrahcc hepatocellular carcinoma , icc interclass correlation coefficients , pt - ro peritumoral radiomics 1 3 la radiologia medica ( 2020 ) 125 : 697705 lesions or metastasis with typical imaging features of hcc or / and with histopathological confirmation , within 2years after curative resection or ablation of hcc [ 27 , 28 ]  . 
our post - treatment tumor surveillance program consisted of physical examination and laboratory tests , including serum alpha - fetoprotein ( afp ) , performed 1month after surgery and every 3months thereafter . 
in addition , abdominal contrast - enhanced ct ( cect ) or contrast - enhanced magnetic resonance imaging ( cemr ) or contrast - enhanced ultrasound ( ceus ) imaging was performed every 3months . ct scan protocols cect was performed at hospital #1 with one of the following equipment : a 64 - detector row ( aquilion cxl , toshiba medical system , tokyo , japan ) or 320 - detector row ct machine ( aquilion one , toshiba medical system , tokyo , japan )  . 
unenhanced , hepatic arterial phase and portal venous phase ct images of the largest cross - sectional area of the tumor were collected ( fig.2a ) , and images were recorded as digital imaging data and communications in medicine ( dicom ) files . 
differences in ct scan protocols between the training cohort and the external validation cohort are listed in table1 . in summary , four datasets were included : 109 images from hospital #1 for training ( set 1 : 1 - mm image slice thickness ) , 47 images from hospital #1 for internal validation fig . 
c roi of pt - ro automatically extended by 2 cm around the lesion , with manual deletion of the roi that extended beyond the parenchyma of the liver table 1 differences in ct scan protocols between the training cohort and the external validation cohort ct scan protocols dataset 1 training cohort ( n = 109 ) dataset 2 same - slicethickness internal validation ( n = 47 ) dataset 3 different - slicethickness internal validation ( n = 47 ) dataset 4 external validation ( n = 47 ) machine detector row scanning parameters ( tube toshiba aquilion 64 / 320 120kv / 250ma toshiba aquilion 64 / 320 120kv / 250ma toshiba aquilion 64 / 320 120kv / 250ma toshiba aquilion 64 120kv / 300ma voltage / tube current ) contrast material hepatic arterial phase / portal ultravist 35s / 65s venous phase tion interval slice thickness / reconstruc1mm ultravist 35s / 65s 1mm ultravist 35s / 65s 10mm omnipaque , or ultravist 25s / 90s 2mm 1 3 700 la radiologia medica ( 2020 ) 125 : 697705 ( sets 2 and 3 : 1 - mm and 10 - mm image slice thicknesses , respectively ) , and 47 images from hospital #2 for external validation ( set 4 : vastly different from training dataset )  . radiomics model construction dataset ( set 4 : images of 47 patients in hospital #2 with differences in many aspects compared with hospital #1 ) compared with that in the training dataset ( set 1 : 1 - mm slice thickness images of 109 patients in hospital #1 )  . 
a significantly lower area under the curve ( auc ) ( p < 0.05 ) indicated overfitting of the model . radiomics model construction was conducted with a standard procedure by target segmentation and feature extraction , followed by feature selection and model construction . calibration deviation test target segmentation andfeature extraction two radiologists with 15years of abdominal ct interpretation independently evaluated the imaging traits . 
software automatically with computing algorithms and recorded as comma - separated value files . feature selection andmodel construction fifty patients of the 156 patients in hospital #1 were randomly selected , and their rois in the selected dicom images ( 1 - mm slice thickness ) were delineated by two radiologists , separately . 
 features with an icc greater than 0.6 ( indicating moderateexcellent interoperator agreement ) were recorded for further analysis . in the training set , the least absolute shrinkage and selection operator ( lasso ) regression [ 29 , 30 ] was performed to further select features among the features with icc greater than 0.6. 
finally , the pt - ro model was built based on the selected features . radiomics reproducibility test poor reproducibility of the radiomics model was defined as significant overfitting and calibration deviation when validated with another dataset . overfitting test calibration deviation was indicated by poor conformity between predicted and follow - up results in the external validation dataset . 
p value of < 0.05 ( two - sided ) was considered statistically significant . receiver operating characteristic ( roc ) curves were plotted to show the accuracy in predicting early recurrence and quantified with the auc . 
the calibrationcurves package was used for the calibration test . possible overfitting was evaluated by the area under the curve [ 31 ] of the radiomics model in the external validation this retrospective study was approved by our institutional review board . 
the study was approved by the ethics committees of the hospitals . greylevelrunemphasis_alldirection_offset8_sd ( portal venous phase )  . radiomics reproducibility test results there were 50 patients who had early recurrence of hcc in the training cohort ( 50 / 109 , 45.9% ) , 25 in the internal validation cohort ( 25 / 47 , 53.2% ) , and 24 in the external validation cohort ( 23 / 47 , 48.9% ) , with no significant statistical difference . 
2 2 6 8 5 * i nv e r s e d i f fe r e n c e m oment_alldirection_offset2_sd ( routine unenhanced phase ) + 1.004993 10 5 * clustershade_ alldirection_offset9_sd ( routine unenhanced phase ) + 1.827011 10 5 * clustershade_alldirection_ offset1_sd ( hepatic arterial phase ) 2.826571 * longrunemphasis_angle90_offset5 ( hepatic arterial phase ) 6.908005 10 6 * clustershade_alldirection_ offset5 ( portal venous phase ) + 1.170673 10 2 * highvalues of the auc were measured to investigate possible overfitting of the pt - ro model between the training set and the different validation sets ( table2 )  . 
u statistics showed reliable results in the internal validation set ( u : p = 0.33 ) , meaning that the pt - ro model showed good agreement between prediction and observation after validation by the same - slice - thickness internal validation set . 
performed in the same - slice - thickness internal validation set ( a ) , the external validation set ( b ) and the different - slice - thickness internal validation set ( c ) discussion radiomics feature quantification may be sensitive to several technical factors . 
however , due to reasons such as high cost , excessive effort , differences in data collection practice , and privacy issues between institutes , acquiring a validation dataset is not always feasible [ 11 ]  . 
we used an independent external validation cohort with considerable image heterogeneity from our center and found that the ct - based pt - ro model had poor reproducibility between centers . overfitting or poor reproducibility of a prediction model is indicated by close or exact correspondence with a particular set of data , thus failing to fit additional data . 
in our study , ct images of the external validation cohort were different from those of the internal validation cohort in terms of the scanners used , scanning parameters , contrast agent doses , scanning phases , and slice thicknesses . 
testretest analyses of ct reported in studies have often been carried out to test radiomics feature reproducibility by using the same ct acquisition parameters ( inter - ct analysis ) [ 9 , 1821 ] , and the concordance correlation coefficient ( ccc ) was used to analyze the reproducibility of the features . 
however , the methods of feature extraction used in each center were different and to date ; only a few studies have compared the features from different centers directly [ 22 , 24 ]  . 
 [ 19 ] found that only 1330% of features had ccc [ 4 ] 0.90 ( high reproducibility ) between repeat ct scans with the same imaging settings conducted within 15min of each other . 
although the proportion of features with high reproducibility varied , the prediction model based on these features still achieved good prediction efficiency [ 9 , 18 , 19 ]  . 
the significance of the heterogeneity caused by different ct scanners , differences of contrasts injection protocol between two centers , and potential anatomic and physiologic differences in clinical cases remained to be studied and has been done in our study . due to the limitations of a small sample size and the characteristics of this retrospective study , we could not explore 1 3 la radiologia medica ( 2020 ) 125 : 697705 the influence of every possible factor on radiomics reproducibility . 
we used relatively homogeneous image sources from our hospital and extracted radiomics features from thin and thick reconstructed images separately to explore the effects of image thickness on radiomics reproducibility . 
there are many other variables related to ct imaging acquisition that were not studied , for example , different detector rows , detector types , and reconstruction , which can considerably affect image quality . 
as this was a retrospective study , the ct technologists who performed the scans were not specifically instructed on patient centering for the acquisition of the image series in this study . 
whats more , there are also intrinsic limitations due to voxel volume averaging between acquisitions , hydration status , and patient size and weight , and due to the tube performance and shielding ( even due by clothes & blankets )  . 
all data was from routine clinical test , and there was no clinical intervention for the participants in the study . informed consent all informed consent for the routine clinical tests were obtained from participants . 
tumors were manually segmented on ct images followed by the application of three image preprocessing techniques ( laplacian of gaussian , wavelet filter , and discretization of the intensity values ) on delineated tumor volumes . 
multivariate analysis involved the use of machine learning ( ml ) algorithms and the following three feature selection algorithms : the least absolute shrinkage and selection operator , students t test , and minimum redundancy maximum relevance . 
these selected features were then used to construct three classification models ( svm , random forest , and logistic regression ) to discriminate high from low - grade ccrcc at nephrectomy . 
the most common types of renal cancer cells are clear cells rcc ( ccrcc ) , papillary rcc ( prcc ) , and chromophobe rcc ( chrcc ) [ 2 , 3 ]  . 
approximately 70% of kidney cancers are made up of ccrcc , prcc accounts for 1015% of kidney cancers , whereas chrcc is the least common type with only 5% of kidney cancer cases [ 4 ]  . 
 ccrcc has a survival rate of less than 5years and a higher risk of metastasis compared to prcc and chrcc [ 5 ]  . one of the most important tasks in cancer diagnosis and treatment is tumor staging and grading . 
grades i and ii are considered as low - grade tumors with a favorable prognosis , while grades iii and iv account for high - grade tumors commonly having unfavorable prognosis [ 7 ]  . currently , fine - needle aspiration ( fna ) and imagingguided biopsies are the gold - standard methods for preoperative kidney tumor grading . 
because of intra - tumoral heterogeneity in ccrcc [ 8 ] , biopsy underestimated the fuhrman grade in 55% of the cases [ 9 ]  . a number of noninvasive therapeutic strategies for rcc have been devised during the last decade , including radiofrequency ablation , cryoablation , and active surveillance [ 10 , 11 ]  . 
however , a proper criterion for patient management using these noninvasive / minimally invasive treatment methods is still lacking , as most patients are often treated surgically post - diagnosis [ 12 , 13 ]  . 
therefore , it is desirable to recommend individualized treatment strategies , where radical approaches ( e.g. , surgery ) are kept only for aggressive or high - grade ccrcc tumors ( iii , iv ) , whereas conservative management ( e.g. , active surveillance ) is applied for lowgrade ( i and ii ) lesions [ 14 ]  . 
 to this end , two promising approaches have been adopted in clinical settings , namely mri - guided derivation of apparent diffusion coefficient ( adc ) values [ 15 ] and ct - based semiquantitative and quantitative techniques [ 16 , 17 ]  . radiomics serve as the bridge between medical imaging and personalized medicine [ 18 ] and refers to the comprehensive quantification of tumor phenotype to uncover disease characteristics that fail to be revealed by the naked eye [ 1921 ]  . 
in fact , radiomics is a new era of science which faces many challenges , including image acquisition [ 22 ] , reconstruction and processing [ 23 , 24 ] , and model development to provide robust and reproducible representations . 
this study aims to construct a radiomics featurebased machine learning model to predict the fuhrman grade of ccrcc patients preoperatively . materials andmethods figure1 presents the workflow followed in the current study . patient population two hundred and twenty - two clinical studies from the cancer image archive database [ 28 ] were included in the study protocol . 
table1 provides the demographics of the patient population . ct scanning protocol all patients underwent a three - phase ct scan , including ( 1 ) a routine unenhanced ct scan , ( 2 ) a corticomedullary phase ( cmp ) contrast - enhanced scan starting 40s after injection of the contrast material , and ( 3 ) a nephrographic phase ( np ) contrast - enhanced scan performed 7090s after intravenous injection of iodinated contrast material . 
all subjects were scanned on ge healthcare and siemens healthineers ct scanners with a tube voltage of 120kvp and a tube current of 150300ma using daily clinical reconstruction parameters . tumor segmentation in this study , manual volume of interest ( voi ) segmentation was performed and verified by an experienced radiologist using the 3d slicer software package [ 29 ]  . 1 3 756 la radiologia medica ( 2020 ) 125 : 754762 fig . 
furthermore , first - order statistic features describe the distribution of voxel intensities within tumor volumes , including mean , median , maximum , and minimum values of the voxel intensities . 
secondand higher - order statistic features ( known as textural features ) are used to measure inter - relationships between voxel distributions within tumor volumes , reflecting changes in image space gray levels . 
these features include gray - level cooccurrence matrix ( glcm ) , gray - level run length matrix ( glrlm ) , gray - level size - zone matrix ( glszm ) , and graylevel dependence matrix ( gldm ) features . 
to control the false discovery rate ( fdr ) in multiple hypothesis testing , the benjaminihochberg ( fdr ) correction method was applied on the resulting p values to ultimately report q - values [ 32 ]  . prior to feature extraction , the voxel size resampling method was applied on the images to create an isotropic dataset . 
laplacian of gaussian ( log ) , wavelet decomposition ( wav ) , and discretization into 32 , 64 , and 128 bins preprocessing were performed to generate a different set of features . 
wavelet filtering yields 8 decompositions per level : all possible combinations of applying either high ( h ) or a low ( l ) - pass filtering in each of the three dimensions , including hhh , hhl , hlh , hll , lhh , lhl , llh , and lll . 
 the preprocessing steps ( including discretization , log , and wavelet ) were also performed on all intensity , histogram , and textural features . 1 3 la radiologia medica ( 2020 ) 125 : 754762 table 2 summary of radiomic features used in this work first - order statistics ( fos ) gray - level co - occurrence matrix ( glcm ) gray - level run length matrix ( glrlm ) energy total energy entropy minimum 10th percentile 90th percentile maximum mean median interquartile range range mean absolute deviation ( mad ) robust mean absolute deviation ( rmad ) root - mean - squared ( rms ) skewness kurtosis variance 19 . 
uniformity shape features volume surface area surface area to volume ratio sphericity spherical disproportion maximum 3d diameter maximum 2d diameter ( slice ) maximum 2d diameter ( column ) maximum 2d diameter ( row ) major axis minor axis least axis elongation flatness autocorrelation joint average cluster prominence cluster shade cluster tendency contrast correlation difference average difference entropy difference variance joint energy joint entropy informal measure of correlation ( imc ) 1 informal measure of correlation ( imc ) 2 inverse difference moment ( idm ) inverse difference moment normalized ( idmn ) inverse difference ( id ) inverse difference normalized ( idn ) inverse variance maximum probability sum average sum entropy 23 . 
sum of squares gray - level size - zone matrix ( glszm ) small area emphasis ( sae ) large area emphasis ( lae ) gray - level non - uniformity ( gln ) gray - level non - uniformity normalized ( glnn ) size - zone non - uniformity ( szn ) size - zone non - uniformity normalized ( sznn ) zone percentage ( zp ) gray - level variance ( glv ) zone variance ( zv ) zone entropy ( ze ) low gray - level zone emphasis ( lglze ) high gray - level zone emphasis ( hglze ) small area low gray - level emphasis ( salgle ) small area high gray - level emphasis ( sahgle ) large area low gray - level emphasis ( lalgle ) 16 . 
large area high gray - level emphasis ( lahgle ) short - run emphasis ( sre ) long - run emphasis ( lre ) gray - level non - uniformity ( gln ) gray - level non - uniformity normalized ( glnn ) run length non - uniformity ( rln ) run length non - uniformity normalized ( rlnn ) run percentage ( rp ) gray - level variance ( glv ) run variance ( rv ) run entropy ( re ) low gray - level run emphasis ( lglre ) high gray - level run emphasis ( hglre ) short - run low gray - level emphasis ( srlgle ) short - run high gray - level emphasis ( srhgle ) long - run low gray - level emphasis ( lrlgle ) 16 . 
 feature selection three different feature selections methods were implemented in this framework ( table 3 ) , namely enhanced 1 3 758 la radiologia medica ( 2020 ) 125 : 754762 variable selection algorithms based on the least absolute shrinkage and selection operator methods [ 34 ] , students t test , and the minimum redundancy maximum relevance ( mrmr ) algorithm . multivariate machine learning classifier the following three classifiers were implemented and compared ( table3 ) : logistic regression , random forest , and support vector machines ( svm )  . model evaluation the cross - validation ( cv ) technique was applied to tune the model parameters . 
however , mri is not as widely available as ct and a wide range of adc values for ccrcc have been reported in the literature [ 41 , 42 ]  . 
these studies showed that ct is a promising method for classification of lowand highgrade ccrcc . the radiomics approach converts medical images into quantitative , high - dimensional , and mineable features enabling to predict tumor status . 
given that a number of previous radiomic studies [ 17 , 25 ] for fuhrman grade prediction did not include shape features in their analyses , this study combined shape features and texture features to differentiate low and high grades of ccrcc . 
it was observed that shape features cannot be ignored from multivariate machine learning models . univariate analysis of the extracted radiomic features demonstrated that among filtered and non - filtered images , only the 128 bin - discretized images showed statistically significant texture parameters . 
auc : area under receiver operating characteristic curve , lr : logistic regression , svm : support vector machine , rf : random forest and found effective quantitative parameters to evaluate the heterogeneity of ccrcc . 
these features include long - run high gray - level emphasis from glrlm , cluster tendency from glcm , contrast from ngtdm , and dependence non - uniformity from gldm matrix . 
it was observed that among the three different feature selection methods , the best results for the logistic regression model was obtained when using the lasso algoriththese results suggest that the auc logistic regression model is approximately similar to results obtained in previous studies . 
 [ 43 ] extracted radiomic features from corticomedullary ( cmp ) and nephrographic phases ( np ) of ct images of 161 and 99 patients diagnosed with lowand high - grade ccrccs . 
it uses a weighted average of these trees for the final decision [ 44 ] , commonly resulting in a good outcome for a large range of data , but is susceptible to overfitting . 
in a similar single - center retrospective study [ 25 ] , the performance of quantitative ct texture analysis combined with different ml - based classifiers was evaluated for discriminating lowand high - grade ccrcc . 
in summary , both studies support each other with a common conclusion that ct texture analysis is a useful and promising noninvasive method to predict the fuhrman grades of ccrccs preoperatively . 
the noninvasive identification of ccrcc grading could help in defining appropriate treatments , especially for patients with small mass and could potentially serve as an alternative for fna in renal cancer . this work bears a number of limitations . 
future studies should consider the effect of volume segmentation to provide a repeatable study for clinical multicentric studies . conclusion the results of this study show that ct - based svm classifier with t test features selection could be a useful and promising noninvasive approach for the prediction of low and high fuhrman nuclear - grade ccrccs . 
moreover , the results demonstrated that 128 bin - discretized preprocessing is an effective method under these conditions . acknowledgments this work was supported by the shahid beheshti university of medical sciences under grant number 388 and the swiss national science foundation under grant snrf 320030_176052 . compliance with ethical standards conflict of interest the authors have no conflict of interest to declare . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . informed consent informed consent is not needed for this study . research involving human participants and / or animals all human subject studies were downloaded from the cancer imaging archive 1 3 la radiologia medica ( 2020 ) 125 : 754762 ( tcia ) , an open - access database of medical images for cancer research . 
in the era of sars - cov - 2 outbreak , lung ultrasound seems to be strongly adapting to the follow - up for lung involvement of patients with ascertaining infections , till to be used , in our opinion emblematically , as a screening test in suspected patients at the emergency triage or at homemedical visit . 
patricia henwood , in her heartfelt experience during the epidemicebola outbreak in west africa , perfectly summarizes the potential role of lus in critically ill patients : half my patient died . 
after a decade of honing my ability to quickly determine sick or not sick and allocating time and resources accordingly , i learned that when managing a ward of patients with ebola , clinical appearance did not always predict survival . 
layers of impermeable and stifling personal protective equipment ( ppe ) constitute an enormous physical barrier to patient care , complicating management of ebola virus disease ( evd )  . 
we lacked on - site diagnostic capacity , so as i worked to secure critical resources to improve over all care , i also sought and received approval to incorporate point - of - care ultrasonography [ 1 ]  . 
these claims are so much actually in these days of severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) pandemic spread so that lus seems to be strongly adapting to the follow - up for lung involvement of patients with ascertaining coronavirus disease 19 ( covid - 19 ) up to , in our opinion emblematic , use of lus at the emergency triage or at home medical visit as a screening imaging test of suspected covid - 19 patients [ 24 ]  . 
if on one hand , many studies have shown the efficacy of lus in diagnosing pulmonary pathology , with increased sensitivity compared to that of chest x - ray ( cxr ) [ 57 ] , on the other hand , little is discussed about its limits and pitfalls especially in generic and off label clinical contest . 
by evaluating 8 zones of the chest4 on each side ( 2 anterior and 2 lateral ) ( fig.1a ) , using both low frequency and high - frequency probes with the best combination of sector or curved array probe ( 3.55mhz ) and a small - parts linear probe ( 510mhz ) , an assessment for various pathologies can be made by examining the pleural line ( sliding , thickness , regularity ) , the sub - pleural regions ( presence or absence of echogenic changes ) and whether there are a - lines or b - lines present ( with the amount and location of b - lines assessed ) ( table2 ) [ 12 ]  . 
the hyperechoic pleural line ( fig.1b , c ) , constituted by the summation of parietal pleura , pleural space , and visceral pleura , it refers to an artifact generated between tissues with different acoustic impedance , as soft subcutaneous tissues and air underneath the lung [ 14 ]  . 
1 schematic representation of the chest ultrasound zone ( a ) and chest ultrasound examination performed with a high - frequency linear probe ( 157mhz ) ( b , c )  . 
8 zones of the chest4 on each side ( 2 anterior and 2 lateral ) ( a ) : the anterior zones ( 1 , 2 , 5 , 6 ) are delimited medially by the hemi - clavicular line and laterally by the anterior axillary line whereas the lateral ones ( 3 , 4 , 7 , 8 ) are included between the anterior and posterior axillary lines . 
thoracic anatomy , longitudinal view acquired with linear probe ( b ) , and schematic representation ( c ) : there is a good anatomical definition of the pleural hyperechoic reflection ( pleural line , c ) between the two ribs ( c , 1 ) and their shadow cone artifacts ( c , 2 )  . 
the cutaneous ( c , 4 ) , subcutaneous ( c , 5 ) and muscular planes ( c , 6 ) are well represented table 2 the alphabet of thoracic ultrasound lines type findings lung and pleural lines a - line ( reverberation ) b - line ( ring down artifact ) vertical hyperechoic artifact originating from the pleural line that extend to the edge of the screen , follow the lung horizontal parallel hyperechoic linear artifact depicted at regular intervals below the pleural line z - line short , ill - defined vertical hyperechoic lines arising from the pleural line that do not reach the edge of the screen comet tail artifact short , triangular artifact with caudal apex lines arising from the pleural line following the lung sliding without sliding and erase the a - lines nor erase the a - lines nor follow the lung sliding reaching the edge of the screen superficial lines e - line screen vertical hyperechoic artifact arising superficial to and obscuring the pleural line and extending to the edge of the 1 3 la radiologia medica ( 2020 ) 125 : 738753 table 3 artifacts dichotomy a - lines normal b - lines z - lines and comet tail lung sliding abnormal normal abnormal normal abnormal normal abnormal healthy patients atelectasis normal finding degrees of interstitial normal finding also present healthy patients lung pulse pneumothorax apnoea asthma copd pneumothorax disease pneumonia pneumothorax ( possible ) gliding sign or lung sliding can indicate the absence of pneumothorax with accuracy close to 100% ( table3 ) [ 1517 ]  . 
is a dynamic lus sign refers to the rhythmic movement of the pleura in synchrony with the cardiac rhythit is best viewed in areas of the lung adjacent to the heart , at the pleural line due to cardiac vibrations transmitted to the lung pleura in poorly aerated lung and it is an early ultrasound sign of complete atelectasis or consolidation as well as indirectly exclude pneumothorax in absence of lung sliding in this critical point ( table3 )  . 
in normal well - aerated lung , the lung pulse is not present , as lung sliding becomes dominant and resistant to cardiac vibrations [ 17 , 18 ]  . lus semeiotic include also other artifacts derived by air / tissue interface such as horizontal and longitudinal / vertical reverberations . 
the horizontal reverberations , known as a - lines , are multiple repeating horizontal lines that are parallel and equidistant from the pleura ( fig.2a , b ) ( table2 ) ; these are the result of repeated reflections of the linear hyperechoic structure caudally to the pleural hyperechoic line , usually interpreted as a normal finding in the healthy patient ( table3 )  . 
 a - lines ( a ) with schematic representation ( b ) : there is a good anatomical definition of the pleural hyperechoic reflection ( b thickened blue line ) with evidence of multiple horizontal reverberation artifacts or a - lines ( b , transparent blue boxes ) parallel to the hyperechoic pleural line and equidistant between theb - lines ( c ) with schematic representation ( d ) : multiple hyperechogenic linear structures or ring - down artifacts ( c ) come from the hyperechoic pleural line ( d thickened blue line ) caudally for several cm ( d blue vertical trapezoids ) 1 3 742 la radiologia medica ( 2020 ) 125 : 738753 in patients with atelectasis , asthma , copd ( positive lung sliding at the pleural line ) , and pneumothorax ( negative lung sliding at the pleural line ) ( table2 ) [ 1416 ]  . 
longitudinal / vertical reverberations , known as b - lines or ring - down artifacts ( rda ) , are transient , hyperechoic vertical lines that extend from the pleura to the bottom of the screen , at a maximum depth of 16cm , erasing a - lines and moving in concert with lung sliding ( fig.2c , d ) ( table2 )  . 
in the case , three or more b - lines between two ribs are called lung - rockets and correlate with the interstitial syndrome with 93% accuracy using alveolar - interstitial radiographic changes as a reference , and full accuracy using computed tomography ( ct ) [ 8 ]  . 
up to 3 b - lines are called septal rockets , correlated with kerley b - lines at chest - x - ray that represents thickened interlobular septa during the interstitial syndrome ( fig.3a , b ) [ 8 ]  . 
in general , in validated clinical contexts , focal b - lines arranged peripherally to a consolidation area may suggest pneumonia , whereas diffuse b - lines in three or more zones on both sides of the chest suggests a diffuse alveolar interstitial syndrome such as pulmonary oedema or acute respiratory distress syndrome ( ards ) ( fig.4 ) ( table3 ) [ 816 ]  . 
 the evaluation of diaphragmatic excursions can be an useful tool in ventilated patients as well as its indisputable additional role as a guide during interventional biopsy or drainage procedures too [ 816 ]  . 
all these findings are well summarized in the management of critically ill patients through an accurate clinical synthesis that is a pivotal element in some validated lus protocols such as [ 20 ] : fig . 
up to 3 b - lines ( a ) with schematic representation ( b ) in an interstitial congestive heart failure : multiple hyperechoic linear structures or ring - down artifacts ( a ) in a septal rockets configuration come from the hyperechoic pleural line ( b thickened blue line ) caudally for several cm ( b blue vertical trapezoids )  . 
 many b - lines ( c ) with schematic representation ( d ) in an alveolar - interstitial congestive heart failure ( same patient as before at follow - up ) : multiple hyperechogenic linear structures or ring - down artifacts ( c ) in a ground - glass rockets configuration come from the hyperechoic pleural line ( d thickened blue line ) caudally for several cm ( d blue vertical trapezoids ) 1 3 la radiologia medica ( 2020 ) 125 : 738753 fig . 
4 integrated ultrasound ( a , c ) and chest x - ray ( b ) with schematic representation ( d , e , f ) of an elderly patient admitted for acutedecompensatedheart failure : the opacity at the right base on chest x - ray ( b , eblue area ) corresponds to a pleural effusion on lung ultrasound ( a , dblue area ) ; a ground - glass rockets configuration ( c , fblue vertical trapezoid ; pleural line : thickened blue line ) was also observed in all lung fields ( b , e )  . 
consolidative area ( a ) with schematic representation ( b ) in bacterial pneumonia : the tissue like sign ( b blue area ) with hyperechoic spots inside ( b yellow arrowheads ) 1 3 744 la radiologia medica ( 2020 ) 125 : 738753 blue protocol ( bedside lung ultrasonography in emergency ) [ 8 , 21 ] : emergency protocol for immediate diagnosis of acute respiratory failure . 
this protocol describes specific sonographic findings associated with major conditions , such as pneumonia , congestive heart failure , chronic obstructive pulmonary disease , asthma , pulmonary embolism , and pneumothorax , with more than 90% diagnostic accuracy . 
it consists in the identification of ten signs : the pleural line ; the lung sliding ; the a - lines ( horizontal artifact ) ; the pleural effusion ; the tissue - like sign indicating lung consolidation ; the b - lines and lung rockets indicating interstitial syndromes ; abolished lung sliding suggesting pneumothorax and the lung point with the absence of b - lines and lung pulse indicating with pneumothorax . 
two more signs , the lung pulse , and the dynamic air bronchogram , are used to distinguish atelectasis from pneumonia . falls protocol ( fluid administration limited by lung sonography ) [ 8 , 21 ] : emergency protocol designed to sequentially rule out differential diagnoses such as cardiogenic and hypovolemic shock , and allowing an early diagnosis of septic shock . 
it adapts the blue - protocol to acute circulatory failure and consists in studying the change from a - lines to lung rockets at a threshold of 18mm hg of pulmonary artery occlusion pressure , providing a direct biomarker of clinical blood volume . 
the appearance of b - lines , schematically , is considered as the endpoint for fluid therapy . cause protocol ( cardiac arrest ultrasound exam ) protocol [ 13 , 22 ] : this protocol normalizes the use of ultrasonography in cardiac arrest management . 
this approach , incorporating lus to manage a cardiac arrest , aids in the diagnosis of the most common and easily reversible non - cardiac causes of arrest , such as severe hypovolemia , tension pneumothorax , cardiac tamponade , and massive pulmonary embolus . furthermore , lus can be also used as a diagnostic tool for assessing positive end - expiratory pressure ( peep ) , induced lung recruitment . 
lus permits also an ultrasound dynamic assessment of lung injury in a patient with extra - corporealmembraneoxygenation ( ecmo ) [ 25 ]  . lung ultrasound virtual anatomic dependent exam : onlyartifacts as seen , although the axiom that lus is something impossible is now abundantly overcome , it is equally important strongly affirm that lus has such intrinsic , patients and radiologists / other specialists correlate limits , and therefore its ultra - diagnostic use with an everything and anything imperative can similarly be a dangerous claim : the truth of lus is in the middle . 
some fine diagnoses still need a more detailed approach as well as a high - resolution ct scan [ 26 ]  . lus intrinsic limitations lus , in optimal conditions , assesses only the 70% of lung surface , which is only about 1 / 16 of the total lung , due to the anatomical constraints of the thoracic cage , and even in areas subject to a lus examination , only the alterations closely related to the pleural surface may be visualized ( fig.6 ) [ 27 ]  . 
 this condition partly explains the rather low sensitivity of lus to detect intra - parenchymal pneumonia , not - adherent to the pleural surface such as some consolidations or tumours , that can be medially located and surrounded by the aerated fig . 
the blue box ( a ) schematizes the ultrasound field of view ( b ) in relation to the ct 1 3 la radiologia medica ( 2020 ) 125 : 738753 lung , or some pulmonary interstitial syndrome from different aetiologies , which may spare the subpleural space [ 27 , 28 ]  . 
besides , the sensitivity of thoracic ultrasound , in the presence of an alterations that affects the pleural compartment , can be considered high , but the specificity is always discreetly low , as lus cannot characterize alterations : a pneumonia , a tumour or atelectasis may show the same echographic pattern ( fig.7 ) [ 27 ]  . 
according to our opinion , only a ct , and sometimes not even a ct , can be considered a certainty investigation to diagnosing a pulmonary alteration , in such cases only a biopsy can confirm the clinical - diagnostic data . patients dependent limitations obese patients may be more difficult to examine due to the thickness of their ribcage and soft tissues , as well as it is difficult to perform lus in burn patients . 
moreover , the coexistence of several pathologies that increase or reduce the sub - pleural air content such as emphysema or atelectasis respectively or an existing fibrotic interstitial lung disease can be confounding factors in the interpretation of the lus findings in the acute setting that are also strongly depending on the age of the observed patient [ 29 ]  . variability interpretation ofthedata andconfusing findings lus is often considered the imaging methods with a shorttrainingcourse [ 8 , 30 ] , and this is largely due to its poor , more intuitive , and not anatomical findings , wrongly understood as a very simple procedure . 
7 chest ultrasound convex multi - frequency probe ( a ) with schematic representation ( b ) of inferior right lobar pneumonia : inhomogeneous consolidation adhered to the pleura ( blue area , b ) with infected pleural effusion ( circled area , b )  . 
enhanced chest ct ( c , mediastinal window ) clearly demonstrates drainage tube with a better visualization of the pleural effusion and extensive right lobar consolidation with air and fluid bronchogram in context 1 3 746 la radiologia medica ( 2020 ) 125 : 738753 inadequacy of the lus in inexperienced hands can cause more harm than good . 
when lus is used inappropriately by novice or inexperienced physicians , its findings become easily confounding ; for example , the b line are often misdiagnosed as z - lines which are vertical , band - like echogenic reinforcements , fixed on the lung fields , which do not delete the a - lines without any pathological correlation ( fig.8 ) ( tables2 , 3 )  . 
the interstitial syndrome is often defined as more than three b - lines between two ribs , but we just remember that b - lines are not always pathological findings since healthy people have b - lines , and various disease can often create similar ultrasound findings , which are non - specific if there is no adequate clinical , anamnestic and laboratory evaluation ( figs.9 , 10 ) ( table3 ) [ 26 ]  . 
this appears to be true because the main distance of two adjacent b - lines at the lung surface should be never less than 7mm to be significant and not only when b - lines are numerous or tend to merge [ 32 ]  . 
b - lines can resolve rapidly in response to treatment , and , therefore , lus data must be interpreted in the context of previous interventions [ 33 , 34 ]  . 
b - lines can be seen in several of pulmonary conditions , including pulmonary fibrosis or interstitial lung disease , ards , trauma , asthma , and pneumonitis ( table3 ) [ 31 , 32 , 3539 ]  . 
z - line ( a ) and b - line ( c ) with schematic representation ( bd ) in two different healthy patient ( a , c ) : hyperechogenic linear structures ( a arrow ) come from the hyperechoic pleural line ( b thickened blue line ) caudally for few cm ( b transparent blue vertical trapezoid ) without deleting the a - lines ( b transparent blue box )  . 
otherwise , the b - lines extend deeper than z - line ( d blue vertical trapezoid ) and deletes the a - lines ( d transparent blue box ) 1 3 la radiologia medica ( 2020 ) 125 : 738753 fig . 
9 chest ultrasound linear multi - frequency probe ( a ) and convex multi - frequency probe ( b ) with schematic representation ( c , d ) in patient affected by miliary tuberculosis : marked irregularity and notched appearance of pleural line ( cd irregular thickened blue line ) with multiple b - lines ( cd blue vertical trapezoids ) that realize a non - specific pattern . 
chest ct ( e lung window ) clearly demonstrates multiple very small nodules in both lungs in a patient with miliary tuberculosis presence of scattered shred sign could help in diagnosing multifocal pneumonia complicated by ards on the related severe degree of hypoxemia , but the ultrasound findings for a consolidation are not specific and must necessarily be correlated with the clinical history , as in the case of aspiration pneumonia ( fig.11 ) [ 40 ]  . 
 lung consolidations do not necessarily mean pneumonia : hemodynamic pulmonary oedema , pulmonary embolism , all kinds of atelectasis , contusion , tumour , drowning and others generate consolidations [ 26 ]  . 
furthermore there is no clear evidence in the literature that the hyperechoic spots and / or lines inside consolidations correlate to the ct imaging of air bronchogram nor they can be only considered in the differential diagnosis between atelectasis and inflammation consolidation , since also in the tumours , can be detected the air bronchograms [ 27 ]  . 
 furthermore the b - lines detection does not exclude the presence of the pneumothorax : in fact bubbles placed in the air / effusion interface at the parietal and pleura specially in hydro - pneumothorax may cause a vertical reverberation artifact mimicking a b - line although such artifacts do not originate from the pleural line as the b lines by definition ( table3 ) [ 41 ]  . 
indeed , the presence of emphysema in the subcutaneous tissue does not allow the us beam to reach the pleural line , thus preventing the visualization of any image , as well as misunderstanding the so - called e - lines such as the reverberations of air in depth tissue , due to subcutaneous emphysema which extend down to the edge of the screen and erase the pleural line ( table2 )  . 
 a correct sequential approach , which could be right for diagnosis of pneumothorax , provides to recognize the a - lines first ( anteriorly in supine patients ) and then looking for the lung point ( the junction point between absent pleural sliding with a - lines and presence of pleural sliding with b - lines ) ( fig.12 ) [ 26 , 41 ]  . 
10 chest ultrasound linear multi - frequency probe ( a ) and convex multi - frequency probe ( b ) with schematic representation ( c , d ) in patient affected by chronic hypersensitivity pneumonia ( chp ) : marked irregularity and thickened appearance of pleural line ( c , d irregular thickened blue line ) with multiple b lines ( c , d blue vertical trapezoid ) with a coalescence appearances that realizes a nonspecific pattern . 
the imaging pattern reflects variable lung attenuation that results in a heterogeneous appearance of the parenchyma in acute pulmonary embolism and inferior vena cava for volume status assessment in cardiac ultrasound ; lung point and lung pulse misinterpretations and mirror artifacts vs . 
deep vein thrombosis or acute right strain in vascular ultrasound [ 43 ]  . the training and advanced study of ultrasound techniques , thorough knowledge of human anatomy , the study of us artifacts , and ultrasonographic semiotics are all crucial tools for radiologists and other physicians . 
this is particularly true because the availability of quality and portable ultrasound machines , often used in intensive care units , has led to the application of various techniques in the investigation of a given pathology by professionals from different backgrounds [ 14 ]  . 
such risks have been amplified by an increase in borderline and off - label approaches to the study of pleuro - pulmonary pathology [ 14 ]  . confounding terminology the term comet tail artifact in lus , as such as , has caused confusion simply because it is used to describe any vertical artifact , particularly b - lines , otherwise defined as rda ( table2 )  . 
as already specified by lichtenstein , in a critical review of lus for expertise , the comet - tail artifact does not exist being itself an oxymoron [ 26 ]  . 
11 chest ultrasound linear multi - frequency probe ( a , b ) with schematic representation ( c , d ) and chest x - ray ( e ) in patient affected by respiratory distress syndrome : on the left ( a ) inhomogeneous consolidation ( c transparent blue areas ) adhered to the pleura with multiple b - lines in coalescence aspect ( c circled area ) ; on the right ( b ) multiple small consolidation ( d blue areas ) closely connected to the pleura in aspiration pneumonia ( milk ) with shred sign ( d circled area )  . 
they are generated by distinct mechanisms : while reverberation due to acoustic impedance difference ( soft tissue / metals ; bile / cholesterol ; soft tissue / gas ) is the mechanism of generating comet tail artifacts , the b lines are caused by resonant vibration due to bubble tetrahedral complexes or their equivalents ( fig.14c , d ) [ 14 , 37 ]  . 
using pneumothorax and interstitial syndrome as examples , the lung comets and b - lines have distinct roles in disease diagnosis and the potential pitfalls if they are simply lumped together and called comet tail artifacts ( table3 ) [ 44 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 738753 750 fig . 
comet tail artifacts ( c ) with schematic representation ( d ) : comet tailartifacts are the result ofcholesterolcrystals deposited in rokitanskyaschoff sinuses ( d blue truncated cone ) conclusion this brief review outlines the need to consider lus exclusively into clinical and laboratory assessment according to validated protocols , as a synthesis of an already known acute clinical condition . 
15 axial chest ct scan in lung window view ( a , d , g ) at the pulmonary apices ( a ) , upper lobes ( d ) and lower lobes ( g ) of a 65yearsold female patient with fever shows : multiple , extensive areas of ground glass opacities in both lung ( a , d ) , coexisting with consolidative opacities and dark bronchogram sign ( g ) , consistent with covid - 19 rapid progression stage ( positive for covid - 19 nasalpharyngeal swap rt - pcr )  . 
the corresponding ultrasound scanswith low - frequency convex probe at right apex ( b ) , linear high - frequency probe at right upper chest zone ( e ) and convex low - frequency probe at the right lower chest zone ( h ) show : vertical artifacts originate from the pleura linewith a coalescence aspect similar to white lung pattern ( blue trapezoid , c ) at the right apex ( b ) ; multiple b lines ( f blue trapezoids ) at the right superior lobe ( e ) ; area of consolidation ( i blue area ) withair bronchogram ( i yellow arrowheads ) at the right base ( h ) narrow the differential diagnosis in the acutely dyspnoeic patient , who is too unstable to leave the department for further imaging exams . 
given to its intuitive semeiotic , lus is easy to perform in critical clinical contexts and can provide a wealth of information for the emergency physician , as well as to assess for fluid overload and whether a patient is a fluid tolerant for resuscitative measures . 
therefore , we recommend its use as a clinical and diagnostic complementary and monitoring tool . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . informed consent all procedures followed were in accordance with the ethical standards of the responsible committee on human experimentation ( institutional and national ) and with the helsinki declaration of 1975 , and its late amendments . 
in 111in - pentetreotide spect , tumour / non - tumour ratio was measured at 4and 24 - h post - injection and the per cent difference was calculated ( t / nt% )  . 
the presence of irregular margins , bronchial obstruction , lymph nodes and metastases was significantly correlated with a higher grade of ki - 67 index . conclusions mdct and nuclear molecular imaging are important to characterize lung tcs . 
the association of mdct and nuclear medicine imaging may be useful in predicting proliferative activity and prognosis of lung tcs . keywords typical lung carcinoids multi - detector computed tomography spect with 111in - pentetreotide 18fluorodeoxyglucose positron emission tomography ki - 67 index introduction bronchopulmonary neuroendocrine neoplasms comprise a spectrum of tumours that arise from pulmonary neuroendocrine cells and represent 25% of primary lung neoplasia * silvia pradella pradella3@yahoo.it extended author information available on the last page of the article [ 13 ]  . 
they include small - cell lung carcinoma ( sclc ) , large - cell neuroendocrine carcinoma ( lcnec ) , atypical carcinoids ( acs ) and typical carcinoids ( tcs ) [ 4 , 5 ]  . 
all of these lung tumours are malignant , but tcs and acs present morphologic criteria of lowand intermediate - grade malignancy neuroendocrine neoplasms ( nens ) , respectively , while sclc and lcnec are clustered into high - grade malignancy tumours [ 6 , 7 ]  . 
the world health organization vol . : ( 0123456789 ) 1 3 716 la radiologia medica ( 2020 ) 125 : 715729 ( who ) classification system of 2015 attempts to distinguish tcs from acs and small - cell carcinoma from large - cell carcinoma [ 13 ]  . the mitotic count and the presence or the absence of necrosis are currently the main criteria for the differentiation of tcs from acs . 
in particular , tcs have a mitotic count of less 2 / 2mm2 and necrosis is absent ; on the other side , acs have a mitotic count of 210 / 2mm2 and present necrosis , usually punctate [ 812 ]  . ki - 67 index is a marker of cell proliferation that identifies proliferating cells spanning from growth ( g1 ) to the mitotic ( m ) phase . 
in the grading system of lung nens , ki - 67 index is mainly used to separate the high - grade scls and lcnec from the carcinoid tumours ; data are conflicting regarding the use of ki - 67 index in separating tc from ac tumours , so actually it is not currently used [ 1317 ]  . tcs are rare primary lung neoplasms , accounting for only 12% of all pulmonary tumours [ 5 ]  . 
currently , contrastenhanced multi - detector computed tomography ( mdct ) , somatostatin receptor scintigraphy with 111indium - pentetreotide ( 111in - octreoscan ) and 18f - fluorodeoxyglucose positron emission tomography ( 18f - fdg - pet ) are the most widely used imaging modality for the localization and characterization of tcs [ 1821 ]  . 111indium - pentetreotide ( octreoscan ) , also known as somatostatin receptor scintigraphy ( srs ) , uses a radiolabeled somatostatin analogue that diagnoses , detects and stages lung tcs by binding to somatostatin receptors ( sstr2 ) , characteristically visualized on the surface of lung tc cells [ 2225 ]  . 
nearly 80% of tcs may be visualized with this technique , especially the most differentiated forms [ 22 ]  . 18f - fdg - pet imaging has usually a marginal role in determining the disease extent of the disease for welldifferentiated lung nens because of their generally lower proliferative activity . 
nevertheless , it may be more sensitive than srs in poorly differentiated tumours ; in fact , higher fdg uptake , expressed as standardized uptake value ( suv ) , has a key role in the characterization of this kind of lung tumours [ 26 , 27 ]  . to the best of our knowledge , in the literature there has not been reported any correlation between mdct and nuclear medicine imaging features of lung tcs with ki - 67 proliferation activity index . 
in our retrospective study , we aimed first to highlight the relationship between mdct and nuclear medicine imaging and then to identify a possible correlation between imaging and ki - 67 activity index . materials andmethods patients with a query ( pulmonary and neuroendocrine tumours ) of the patients medical records database in our department , a radiologist resident selected retrospectively all patients with pathologically proven tcs of lung diagnosed between january 2009 and june 2019 . 
only patients who underwent contrast - enhanced mdct and nuclear medicine imaging ( 111in - octreoscan and / or 18f - fdgpet ) in the immediate preoperative period ( 1 month ) were included in our study . 
an additional histopathological parameter is ki - 67labelling index that is required for an adequate diagnosis of tcs , although it is not currently used in the grading syste in fact , in the 2015 who classification , the ki - 67 prognostic role is not established and is considered valuable in biopsy or cytology samples only [ 6 ]  . mdct imaging all ct investigations were carried out on a 64 detector helical ct ( somatom sensation 64 , siemens healthcare , germany )  . 
a standard protocol was used ; the patients were scanned in supine with craniocaudal breath - hold scans ; all cases underwent non - contrast and contrast - enhanced mdct . 
iodinated contrast medium ( ultravist 370 , bayer schering pharma , berlin , germany ) was injected in the antecubital vein at the flow rate of 34ml / using an automatic injector , immediately followed by a saline flush ( 4050ml ) with a rate of injection of 34ml / s . 
the dose 1 3 la radiologia medica ( 2020 ) 125 : 715729 of contrast medium was administered according to the patients body weight ( ml / kg body weight : 80100ml ( < 80kg ) or 100120ml ( > 80kg ) )  . 
dual - phasic contrastenhanced images were obtained during the arterial phase ( 3035s after the start of injection ) and portal venous phase ( 7075s after the initiation of the injection )  . 
the parameters for both non - contrast and contrast - enhanced ct examination were tube voltage , 120kv ; tube current , 200250 mas , depending on the patients size ; beam collimation , 64 0.5mm ; rotation time , 0.4s ; pitch , 1 ; and reconstruction interval , 1mm . somatostatin receptor scintigraphy imaging patients were well hydrated before and for at least one day after injection . 
patients were administered 222mbq ( 6mci ) of 111in - pentetreotide , a [ 111in - dtpa - d - phe - ] conjugate of octreotide and a long - acting somatostatin analogue ( octreoscan )  . 
whole - body scan ( wb ) and single - photon emission computed tomography ( spect ) imaging were performed 4 and 24h after injection according to the following parameters : wb scan for 20cm / min using 256 256 matrix and spect images of the appropriate regions using 64 64 matrix , 360 rotation , 40s / frame . 18ffdgpet / ct imaging all patients fasted for at least 4h before examination . 
images were obtained on a dedicated pet / ct scanner ( philips gemini tf 16 pet / ct ) , 60min after intravenous injection of 3.6mbq / kg of fdg from skull base to mid - thigh . 
ct acquisition ( 120kv , 30150mas ) was performed on spiral 16 slice ct with a slice thickness of 4mafter transmission scan , 3d pet acquisition was taken for 2min / field with an axial field of view ( fov ) of 57.6cct - based attenuation correction of the emission images was performed . 
after completion of pet acquisition , the reconstructed attenuation corrected pet images , ct images and fused images of matching pairs of pet and ct images were available for review in axial , coronal and sagittal planes and in maximum intensity projections ( mips )  . imaging andanatomicpathological analysis all lung tcs were retrospectively assessed for the mdct intra - pulmonary and extra - pulmonary signs . 
among intra - pulmonary signs , we evaluated morphological features classifying the lesions as the following , in accordance with the existing literature [ 11 , 13 ] : nodule or mass with regular or irregular margins , the type of enhancement ( homogeneous or heterogeneous ) , the intensity of enhancement ( mild or intense ) and the presence of calcifications and bronchial obstruction . 
the patients were divided into two groups according to each of these characteristics by identifying the following : nodule / mass , regular / irregular margins , homogeneous / heterogeneous enhancement , mild enhancement / intense enhancement / , calcifications / no calcifications , bronchial obstruction / no bronchial obstruction , lymph nodes / no lymph nodes and metastases / no metastases . in accordance with the existing literature [ 18 ] in tcs , distant metastases usually involve the liver , bone and bra hepatic metastases usually appear to be hypervascular , similar to the primitive tumour , while bone metastases are generally osteoblastic [ 18 ]  . concurrently , two expert nuclear medicine physicians ( 10 and 20years of practice , respectively ) retrospectively analysed nuclear medicine aspects of all tcs with either focal fdg uptake or srs uptake and those were confirmed as tumour lesions based on mdct images were analysed . 
 among these , eleven patients did not undergo contrastenhanced mdct and / or 111in - octreoscan and 18f - fdg - pet in the immediate preoperative period and four patients were table 1 demographic data and neoplasms localization of the study population with tcs number ( % ) 44 / 68 ( 65% ) 24 / 68 ( 35% ) 34 / 68 ( 50% ) 34 / 68 ( 50% ) 45 / 68 ( 66% ) 23 / 68 ( 34% ) 53 / 68 ( 78% ) 15 / 68 ( 22% ) 20 / 68 ( 29% ) 24 / 68 ( 35% ) 13 / 68 ( 19% ) 15 / 68 ( 22% ) bold values indicate that the most frequently encountered data excluded for poor mdct and / or nuclear medicine images quality . 
forty - eight out of 68 patients have undergone 111in - octreoscan and 18f - fdg - pet , 8 / 68 patients 111inoctreoscan and 12 / 68 patients 18f - fdg - pet . 
extrapulmonary signs were absent in 52 / 68 ( 76.5% ) cases of our range ( years ) 3894 mean ( years ) 69.7 number ( % ) 23 / 68 ( 34% ) 45 / 68 ( 66% ) number ( % ) 52 / 68 ( 76.5% ) 16 / 68 ( 23.5% ) 44 / 68 ( 65% ) 24 / 68 ( 35% ) 13 / 68 ( 19% ) 12 / 68 ( 18% ) 19 / 68 ( 28% ) 10 / 68 ( 15% ) 1 / 68 ( 1% ) 13 / 68 ( 19% ) patients patients male female forms central peripheral pulmonary site right left lobe site right upper lobe middle lobe right lower lobe left upper lobe lingula left lower lobe bold values indicate that the most frequently encountered data 1 3 la radiologia medica ( 2020 ) 125 : 715729 fig . 
1 axial ( a ) , sagittal ( b ) , coronal ( c ) mdct images demonstrate a well - defined nodule ( white arrows ) of 15mm with regular margins located in the right upper lobe . 
we observed 13 / 68 ( 19% ) cases with regional lymph nodes and 15 / 68 ( 22% ) with distant metastases ; of these , 9 patients present both hypervascular liver and osteoblastic bone metastases , 4 show only hypervascular liver metastases , 1 has isolated osteoblastic bone metastases and 1 has multiple brain metastases . relationship betweenmdct andnuclear medicine imaging features oflung tcs we found a series of statistically significant correlations between the main imaging techniques used for the identification of tcs . 
2 axial ( a ) and coronal ( b ) mdct images demonstrate a welldefined endobronchial nodule ( white arrows ) of 23mm with regular margins located in the antero - basal segment of the right lower lobe . 
tcs represent a rare type of lung neoplasms , accounting for only 12% of all pulmonary tumours [ 5 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 715729 fig . 
3 axial ( a ) mdct lung window image reveals a mass of 35mm with irregular margins located in the left lower lobe ( white arrows ) which determines bronchial obstruction . 
arterial phase ( d ) and portal venous phase ( e ) contrast enhancement mdct images show multiple hypervascular liver metastases that become almost isodense on the portal venous phase except for the central region of necrosis . 
4 correlation between metabolic activity of 18f - fdg - pet ( suv ratio ) and 111in - octreoscan sstr density ( t / nt% ) among imaging modalities , mdct , 111in - octreoscan and 18f - fdg - pet play an important role in the diagnosis and staging of tcs [ 10 , 19 ]  . regarding the relationship between mdct and nuclear medicine imaging features of lung tcs , as explained in the literature [ 22 ] , we found a significant negative correlation between metabolic activity of 18f - fdg - pet ( suv ratio ) and 111in - octreoscan sstr density ( t / nt% )  . 
 this is due to the fact that well - differentiated tcs are more likely to express the somatostatin receptors at high density and thus may be more susceptible to detection by 1 3 722 la radiologia medica ( 2020 ) 125 : 715729 table 4 suv ratio values divided into groups according to mdct features ( significant differences are indicated with * ) mdct features significance ( p < 0.05 ) nodule irregular margins homogeneous enhancement intense enhancement calcification bronchial obstruction lymph nodes metastases 1.04 bold values indicate that statistically significant differences 111in - octreoscan . 
poorly differentiated tcs may display a lower density of somatostatin receptors but are generally more metabolically active , thus potentially making them better visualized by 18f - fdg - pet . 
in particular , fdg uptake might reflect the grade of malignancy and proliferation , while sstrs uptake , revealing the expression of somatostatin receptors , could reflect the degree of differentiation . 
this deduction is consistent with the different roles of 18f - fdg - pet and 111in - octreoscan in the evaluation of tcs [ 22 , 29 ]  . in the recent literature concerning tcs , no correlation between mdct and nuclear medicine imaging features is reported . 
 in particular , we found that high sstr density at 111inoctreoscan was associated with more benign tc characteristics at mdct , such as regular margins , presence of calcifications and absence of distant metastases . 
on the other hand , our results also revealed that higher metabolic activity is associated with more malignant signs at mdct , such as mass appearance , irregular margins , heterogeneous fig . 
at 111in - octreoscan imaging ( c , d ) this neoplasm shows a higher uptake ( white arrows ) suggesting a well - differentiated lung tc due to the conspicuous expression of somatostatin receptors . 
 ki - 67 index of this lesion is 3% enhancement , bronchial obstruction , lymph nodes and metastases . necrosis are the main criteria for categorizing these lung tumours [ 8 ]  . we did not find a statistically significant difference regarding enhancement intensity ; this result could suggest that further radiomic analyses are needed , such as the evaluation of enhancement pattern characteristics with texture analysis . the who 2015 classification system is currently well accepted by clinicians as a simple , reproducible and prognostic effective grading of tcs [ 6 ]  . 
the who classified tcs into tumours with low - grade malignancy , and actually the mitotic count ( < 2 / 2mm2 ) and the absence of regarding the role of ki - 67 proliferation index for lung tcs , the literature reports conflicting evidence . 
as opposed to gastrointestinal nens and pancreatic nens where ki - 67 labelling index is an integral part of the current grading system [ 2 , 15 ] , data are conflicting regarding the use of ki - 67 index in tcs , so actually it is not currently used in this setting [ 6 ]  . in our study , some statistically significant correlations emerged between ki - 67 index and mdct and nuclear medicine imaging features . 1 3 724 la radiologia medica ( 2020 ) 125 : 715729 fig . 
7 axial a pre - contrast mdct image shows a well - defined nodule of 15 mm with intralesional calcification ( white arrow ) located in the upper right lobe . 
these imaging characteristics are associated with the low percentage value of ki - 67 index suggesting a well - differentiated form of lung tc in fact , comparing mdct features and ki - 67 activity index we found a statistically significant correlation between higher proliferation activity index and the following mdct features : irregular margins , heterogeneous enhancement , bronchial obstruction , lymph nodes and metastases . 
moreover , as regarding nuclear medicine imaging and activity proliferation index has emerged a negative statistically significant correlation between ki - 67 index and 111in - octreoscan sstrs density ( t / nt% ) and a positive statistically significant correlation between ki - 67 index and 18f - fdg - pet metabolic activity ( suv ratio )  . these latest results could be related to the fact that ki - 67 index reflects the proliferation and invasiveness of tumour cells [ 7 , 9 , 30 ] , so it is significantly associated with more malignant characteristics at mdct and nuclear medicine imaging . one of the possible further developments of this study would be to follow our series of lung tcs to find the prognostic value of imaging methods combining it with that of the ki - 67 proliferative activity index in the evolution of the disease . 
in fact , in lung tcs , the main clinical question concerns the need for patient risk stratification on the basis of tumour aggressiveness , especially in the setting of metastatic disease where the morphology on small - sized diagnostic materials could be misleading . 
therefore , together with the overall clinical profiles ( radiology and nuclear medicine imaging , symptoms and individual risk for evolving disease ) ki - 67 proliferative activity index could potentially be a decisional factor to stratify patients into more defined 1 3 la radiologia medica ( 2020 ) 125 : 715729 fig . 
8 axial a pre - contrast mdct image shows a mass of 40 mm with irregular margins located in the middle lobe ( white arrow ) which is associated with supra - centimetric right hilar lymph node ( dashed arrow ) at 18f - fdg - pet imaging b the lesion and right hilar lymph node show high fdg uptake ( white and dashed arrows )  . 
9 axial ( a ) , coronal ( b ) , sagittal ( c ) mdct lung window reveal a mass of 42 mm with irregular margins located in left lower lobe ( white arrows )  . 
at 18f - fdg - pet imaging e the lesion ( white arrows ) shows high fdg uptake , and similar uptake is present in a left hilar lymph node ( f ) ( white arrows )  . 
10 axial ( a ) , coronal ( b ) , sagittal ( c ) mdct lung window show a mass ( 30mm ) located in the left lower lobe with irregular margins that determine bronchial obstruction ( white arrows )  . 
the combination of all these aspects suggests a poorly differentiated form of lung tc clinical categories for precision medicine and appropriate treatments . several criticisms may be raised with respect to our study . 
 first , this study is retrospective . second , 48 / 68 patients have undergone both nuclear medicine examinations ( 111in - octreoscan and 18f - fdgpet ) , but some of them have carried out only one of the two investigations ( 8 / 68 patients only 111in - octreoscan and 12 / 68 patients only 18f - fdg - pet )  . finally , all of our patients were selected because they had histological confirmation of tcs after surgical resection . 
the association of mdct and nuclear medicine imaging may be useful in predicting proliferative activity and prognosis of lung tcs . 1 3 la radiologia medica ( 2020 ) 125 : 715729 fig . 
11 axial ( a ) lung window mdct reveals a mass of 35 mm with irregular margins in the lumen of the left main bronchus ( white arrow ) ; it determines bronchial stenosis and atelectasis of adjacent pulmonary parenchyma . 
at 18f - fdg - pet imaging the lung lesion ( red pointer ) shows high fdg uptake ( d , e ) ; also , the liver metastasis e presents high fdg uptake ( black arrow )  . 
at 111in - octreoscan imaging f this neoplasm shows a moderate uptake ( black arrow ) suggesting a poorly differentiated lung tc due to the reduced expression of somatostatin receptors . 
13 correlation between 18f - fdg - pet metabolic activity ( suv ratio ) and ki - 67 proliferation activity index 1 3 728 la radiologia medica ( 2020 ) 125 : 715729 compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . 
no funding was received for this study . ethical approval all procedures performed in the studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
the protocol number is 14776_oss . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2020 ) 125 : 784789 ultrasonography preprocedural shear wave elastography onprediction ofhemorrhage afterpercutaneous realtime ultrasoundguided renal biopsy mehmetburakilda1 mustafagk1 oguzabdullayev1 received : 28 may 2019 / accepted : 16 march 2020 / published online : 21 march 2020 italian society of medical radiology 2020 abstract purpose to evaluate the relationship between renal elasticity which was determined with shear wave elastography ( swe ) and hemorrhage in patients who undergone percutaneous renal parenchyma biopsy ( prb )  . materials and methods in total , 60 patients who were performed ultrasound - guided prb after the b - mode ultrasonography and swe assessment were recruited in this study . 
there was no other statistically significant demographic , ultrasonographic or laboratory value differences between two groups . conclusion although shear wave velocities have low sensitivity for hemorrhage after renal biopsy , high specificity and statistically significant difference in hemorrhage and non - hemorrhage group suggest that patients who have lower renal cortical shear wave velocity have a tendency to hemorrhage after prb . keywords renal shear wave elastography renal biopsy hemorrhage introduction chronic kidney disease ( ckd ) can be defined as any condition that causes reduced kidney function over a period of time . 
ultrasound - guided prb with an automated spring - loaded biopsy device has become * mehmet burak ilda mbcildag@yahoo.com 1 department ofdiagnostic andinterventional radiology , adnan menderes university , aydn09100 , turkey the standard method for kidney biopsies . 
also , according to the society of interventional radiology , kidney biopsies are procedures with significant bleeding risk , difficult to detect or control ( category 3 ) [ 7 ]  . 
 previous studies have shown risk factors for bleeding such as hypertension , reduced glomerular filtration rate , anemia , vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 784789 older age , acute kidney disease and use of a larger biopsy needle [ 812 ]  . shear wave elastography ( swe ) is an imaging technology sensitive to tissue stiffness . 
swe uses short - duration high - intensity acoustic pushing pulse to displace tissue in the normal direction , and the displacement within a specified roi is subsequently measured by ultrasound transducer . 
previous studies using swe to evaluate ckd have shown that the swv of the renal parenchyma in ckd patients was significantly different from normal patients [ 1416 ]  . although there are studies about the risk factors for hemorrhage after prb , there is no obvious correlation between renal parenchyma elasticity and hemorrhage . 
in this study , we investigated the feasibility of swe before a renal biopsy in predicting hemorrhage and the relationship between hemorrhage size and swe , ultrasonographylaboratory findings in patients who had undergone real - time ultrasound - guided prb . material andmethods institutional review board approval was obtained for this retrospective study . 
patients undergoing hemodialysis , peritoneal dialysis , renal transplant recipients , as well as patients with unilateral or bilateral hydronephrosis , kidney stones , right side renal biopsies and renal tumors were excluded . 
biopsy procedures were canceled in patients with high blood pressure ( systolic blood pressure greater than 140mmhg and / or diastolic blood pressure greater than 90mmhg ) and bleeding diathesis ( prothrombin time greater than 14s , activated partial thromboplastin time greater than 39s , international normalized ratio ( inr ) greater than 1.5 and platelets lower than 50 , 000 ) in accordance with our clinical approach because of high risk of hemorrhage . 
as swe is not suitable for kidneys with a depth of 5cm or more , these patients were excluded from the study because of the limitation of swe . patients who had b - mode ultrasonography and swe before renal biopsy were included in the study . 
the ultrasound examination was performed in each subject in the same session with swe measurements before renal biopsy , using rs - 80a ( s - shearwave ; samsung medison , hongcheon , korea ) , with a convex array probe of ca1 - 7a ( 17mhz )  . 
in each patient , 10 valid measurements of kidney were obtained and a median value was calculated , the result being expressed in meters / second ( m / s )  . 
b - mode ultrasonography and swe findings were reviewed from the radiology database of the hospital . in all patients with ckd , a renal biopsy was performed after the b - mode ultrasonography and swe assessment . 
 renal biopsy of the left inferior pole of the kidney parenchyma was performed using an 18g biopsy needle of a bard automatic biopsy device ( bard peripheral vascular inc . , tempe , az , usa ) under ultrasonic guidance in prone position under local anesthesia by prilocaine 2% in all patients . 
all examinations and renal biopsies were made by a board - certified radiologist who has 5years of experience in genitourinary imaging and interventions . in all patients , serum creatinine , blood urea nitrogen , coagulation tests such as the prothrombin time ( pt ) , activated partial thromboplastin time ( aptt ) , inr and platelet counts before at most 6h of biopsy were recorded from hospital archives . 
also , the greatest dimensions of hemorrhage were recorded in patients who developed this after biopsy . the patients were divided into two groups , those who did and those who did not develop a hemorrhage after biopsy . 
 statistical analysis was carried out to detect whether there was any relationship between hemorrhage size and swe , ultrasonographylaboratory findings in patients with postprocedural hemorrhage . statistical analysis statistical analyses were performed using the statistical package for the social sciences ( spss ) 17.0 statistical software for windows ( spss inc , chicago , il , usa )  . 
roc curve for swv with cutoff value of 1.21 is shown in fig.1. the two groups demographic , ultrasonographic and laboratory characteristics and p values according to statistical difference analysis are summarized in table 1 . 
statistical analyses of the relationship between hemorrhage size and swe including ultrasonographylaboratory findings in patients with postprocedural hemorrhage are summarized in table2 . statistical study was not performed between pathological diagnoses and laboratory findings , ultrasonographic measurements and cortical swv due to the small number of study patients and wide variety of pathological variation . 
statistical significance was obtained when comparing group hemorrhage ( ) and hemorrhage ( + ) group ( p : 0.004 ) discussion ultrasound elastography is the most remarkable advance in the field of ultrasonography in recent decades . 
because of the small number of patients and wide variety of pathological alteration , no statistical evaluation was made between smw and pathological alteration in this study . renal biopsy is often required for histological diagnosis and to choose treatment for ckd . 
reduced gfr , anemia , older age , high blood pressure , the use of a larger biopsy needle , frequency of puncture , bleeding diathesis , small kidneys and acute kidney disease were known risk factors for bleeding in several previous investigations [ 4 , 812 ]  . 
we did not perform renal biopsy on patients with high blood pressure ( systolic blood pressure greater than 140mmhg and / or diastolic blood pressure greater than 90mmhg ) and bleeding diathesis in accordance with our clinical approach because of high risk of hemorrhage . 
needle size and number of biopsies were same in all patients . kidneys have rich perfusion , receiving 20% of cardiac output despite only constituting < 1% of body mass , and stiffness may be affected by rich perfusion . 
in contrast to what we expected from the findings in previous studies , we have observed that patients with post - procedure hemorrhage had statistically significant lower mean shear wave velocity compared with patients with no hemorrhage . 
for an swv of less than 1.21m / s , we could predict the presence of hemorrhage with sensitivity of 39.1% and specificity of 97.3%. there were certain limitations within our study : firstly , the sample size was small ( n : 60 )  . 
secondly , there were technical difficulties in shear wave elastosonography , including the fixed dimensions of the roi box compared to the variable small area of the renal cortex as well as difficulty in placing the long axis of the roi box in parallel orientation to the medullary pyramids . 
thirdly , the study was of retrospective nature . in conclusion , this retrospective study indicates that patients with post - procedure hemorrhage have statistically 1 3 la radiologia medica ( 2020 ) 125 : 784789 significant lower renal cortical shear wave velocity compared with patients with no hemorrhage after percutaneous real - time ultrasound - guided renal biopsy . 
we considered all patients with diagnosis of ovarian cancer and preoperative ct , who had undergone upfront cytoreductive surgery between 2008 and 2010 and had post - operative clinical follow - up to december 2015 . 
two radiologists reviewed ct scans and assessed ct - pci using sugarbakers diagrawe assessed the discriminatory capacity of the ct - pci score on the surgical outcome by roc curve analysis . 
ct - pci is positively correlated with both dfs and os and may be used as an independent prognostic factor , for example in patients with high figo stages . keywords ovarian cancer peritoneum pci surgical outcome survival * giacomo avesani giacomo.avesani@policlinicogemelli.it 1 uoc radiologia diagnostica e interventistica generale , dipartimento di diagnostica perimmagini , radioterapia oncologica ed ematologia , fondazione policlinico universitario a . 
given that the tumour - related symptoms , such vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 770776 as bloating , abdominal pain or urinary symptoms , are not specific and relatively common in general population , oc is often diagnosed at advanced stages with high - volume disease . 
one commonly adopted score is the peritoneal cancer index ( pci ) , firstly proposed by sugarbaker [ 4 ] to standardise the quantification of peritoneal spread in gastrointestinal cancer . 
in gastroenterological cancer - specific setting , pci is widely used to guide therapeutic strategies , as it is correlated with the probability of complete cytoreduction after surgery [ 5 ] and with prognosis [ 6 ]  . 
previous investigations showed a good performance of this surgical score also in the setting of ovarian cancer [ 7 , 8 ] , indicating good correlation with surgical [ 9 ] and clinical outcome [ 10 , 11 ]  . 
pci is assessed at peritoneal inspection during laparotomy or diagnostic laparoscopy , and in the case of high pci , the surgeon may decide not to proceed with immediate surgical cytoreduction [ 12 ]  . the aim of this study was to test whether pci assessed on conventional routinely performed preoperative ct ( ct - pci ) can be used as a reliable non - invasive tool to predict surgical outcome and help the surgeons to allocate patients to the ideal treatment strategies , i.e. , primary surgery versus neoadjuvant chemotherapy . 
furthermore , we wanted to evaluate its potential value as prognostic factor for both disease - free survival ( dfs ) and overall survival ( os )  . materials andmethods this is a retrospective , observational cohort study performed in a single institution . 
the local institutional review board approved the study , and requirement for informed consent was waived . all consecutive patients with a diagnosis of ovarian cancer who underwent primary cytoreductive surgery in our tertiary referral hospital for gynaecological oncology between 2008 and 2010 were considered for enrolment . 
the inclusion criteria were as follows : ( 1 ) preoperative ct of the whole abdomen in portal venous phase after intravenous contrast injection available ; ( 2 ) upfront cytoreductive surgery ; and ( 3 ) clinical and biochemical follow - up to december 2015 . patients demographics and tumour - related characteristics as well as follow - up data were obtained from a prospectively acquired digital database . exclusion criteria were : ( 1 ) previous surgical procedures for gynaecological cancers ; ( 2 ) too short period of followup ( < 3months ) because patients did not come to follow - up visits . the ct examinations were performed using various ct equipments from different vendors . 
images were acquired during breath hold by utilising the following acquisition parameters : 120 kvp ; automatic milliampere setting ( depending on patient size ) , with a range of 240400ma ; slice thickness between 1 and 3mm ; and pitch less than 1 . 
patients did not have any preparation , except for 600800ml of diluted iodine contrast ( diatrizoate diluted at 5% ) given 4060min before scan . two radiologists ( respectively , 16 and 4years of experience in gynaecological imaging ) independently reviewed anonymised ct scans and assessed radiological preoperative pci , blinded to any other information about patients surgical and clinical outcome . 
inter - rater agreement was calculated by using icc ( interclass correlation coefficient )  . complete surgical resection was called when no visible residual disease was present at the end of surgery . correlation between ct - pci and surgical outcome was performed using logistic regression ; receiving operator characteristic ( roc ) curve analysis was then performed to investigate test accuracy . ct - pci was correlated with os and dfs in two different independent analyses : the first considering the absolute value of ct - pci and the second one considering the regions of involvement , independently by the value of ctpci . 
this partition was chosen to gather patients in more homogeneous groups in order to simplify results and obtain a higher statistical power , given that ct - pci can vary between 0 and 39 . 
os and dfs of these groups were analysed using the kaplanmeier estimator for univariate analysis and cox - regression model for multivariable analysis ( considering also age , stage , histology and residual disease after surgery )  . 
an example of peritoneal localisation in left iliac fossa of 28mm ; in this case the score of the section5 ( left lower ) was 2 , as the lesion measured between 0.5cm and 5cm if the necessary information for statistical analysis was not available , the patient was excluded from that specific analysis . 
this partition was chosen because it recalls the figo stages of ovarian cancer . statistical analysis was performed using stata v14.0 ( stata corp , college station , tx )  . 
 ( we considered the last ct before surgery . ) the surgical procedure included a total hysterectomy and bilateral salpingo - oophorectomy , omentectomy , lymphadenectomy in case of bulky lymph nodes and careful evaluation of all peritoneal surface with resection of any suspicious peritoneal lesions or other tumour involved organs or structures . 
a diaphragmatic stripping or full thickness resection was performed in 168 ( 61% ) of patients , a splenectomy in 50 ( 18% ) , a liver capsule resection in 102 ( 37% ) , a bowel resection in 174 ( 63% ) , a pelvic lymphadenectomy in 119 ( 43% ) , and a para - aortic lymphadenectomy in 119 ( 43% )  . total macroscopic tumour clearance was achieved in 213 ( 77% ) of the patients . 
the median ct - pci of patients with residual disease after surgery was 16 ( interquartile range , iqr 620 ) , while among patients with complete tumour cytoreductive surgery , it was 7 ( iqr 019 )  . 
survival analysis according to cox - regression model showed that figo stage ( hr 529 , 95% ci 17.41600 ; p < 0.001 ) , histological subtype ( endometriod tumour has hr 81.3 , 95% ci 3.1214.6 ; p < 0.01 ) and the value of ct - pci ( hr 1.03 , 95% ci 1.001.05 ; p < 0.05 ) were significant independent predictors of dfs . 
 stage and histological subtype were time - dependent variables , while their estimate as prognostic markers of recurrence was maximal at the time of surgery ; it declined with time . 
this means their strength as prognostic factor for recurrence is very high at the time of surgery but declines afterwards ; in contrast , a relatively higher ct - pci maintained the risk of recurrence stable across time , compared to a lower ct - pci . similar findings were obtained for os , where in multivariate cox - regression analysis , figo stage ( hr 3.45 , 95% ci 1.67.3 ; p < 0.001 ) and histology ( hr 3.7 , 95% ci 1.68.6 ; p < 0.01 ) and ct - pci ( hr 1.03 , 95% ci 1.011.06 ; p < 0.05 ) were independent predictors of os . 
moreover , we showed that serous histology was significantly associated with higher ct - pci scores , with the higher prevalence in upper abdominal and bowel involvement compared to other histological subtypes , an expected finding . 
we failed , however , to demonstrate ct - pci as a reliable tool in successfully identifying patients who would not benefit from cytoreductive surgery in terms of total macroscopic tumour clearance . our results partly correspond with data from previous authors . 
 [ 14 ] found that in gastrointestinal cancers sensitivity of ct in detecting peritoneal implants depends on lesion size and that ct - pci is significantly lower than surgical pci . 
 tick marks on each line represent drop - outs 1 3 la radiologia medica ( 2020 ) 125 : 770776 value of odds ratio of ct - pci for incomplete cytoreduction may seem low but , considering that it indicates the relative risk for each point of ct - pci and that ct - pci has a wide spectrum of values ( 039 ) , the difference of relative risk may differ consistently . the prognostic value of surgical pci is well known among general surgeons , and recent papers have stated that it is valuable also in ovarian cancer [ 10 , 11 , 20 ]  . 
in particular , patients with serosal bowel involvement , which is a challenging site for complete tumour resection especially when the mesentery is involved in a diffuse fashion , are at increased risk , with a demonstrated shorter os , as recently reported by rosendahl etal . 
the negative impact of high radiological tumour burden on patients clinical outcome was expected since high tumour burden indicates more aggressive and more advanced disease that inherently will be associated with poorer outcome . 
they concluded that initial disease burden was a significant prognostic factor even after adjusting for residual disease [ 23 ]  . our study has the limitations of a retrospective analysis with some parts of the patients data being lost to follow - up or being incomplete , generating censored data . 
most importantly , we could not directly correlate ct - pci with surgical pci because surgeons did not systematically report it . in conclusion , while radiological pci assessed on preoperative ct is associated with the probability of residual disease after cytoreductive surgery , it has low performance and reliability as a triage test to preoperatively identify patients that will end up with residual disease after primary cytoreductive surgery for advanced ovarian cancer . 
ct - pci is , however , positively correlated with both dfs and os and may be used as auxiliary prognostic factor , especially in patients with advanced figo stages . acknowledgements the authors also acknowledge programmatic support from uk medical research council ( ea , ar ) and ovarian cancer action ( cf )  . funding this article is an independent research funded by the national institute for health research ( nihr ) , imperial biomedical research centre ( brc ) , the imperial college experimental cancer medicine centre ( ecmc ) and imperial college london tissue bank . 
tick marks on each line represent drop - outs reported that , even if ct - pci is lower than surgical pci , the clinical significance of this difference is limited and suzuki etal . 
 [ 17 ] stated that in gastrointestinal cancer ct is helpful to predict resectability and survival . in ovarian cancer , the application of preoperative radiological assessment of pci is scarce . 
 [ 19 ] stated that ct can be used as single technique to select patients for a primary cytoreductive or a neoadjuvant chemotherapy , if performed with a dedicated protocol and read by an expert radiologist . 
however , even if it cannot be used alone as a reliable triage tool to avoid suboptimal surgery , the positive association between ct - pci and post - operative residual disease supports further investigation , as it may be an auxiliary predictor of patients at high risk of residual disease . 
the 1 3 776 la radiologia medica ( 2020 ) 125 : 770776 expressed are those of the author ( s ) and not necessarily those of the nhs , the nihr or the department of health . compliance with ethical standards conflict of interest none of the authors has conflict of interest to declare . ethical standard ethical committee approved this study involving human participants . informed consent all patients gave informed consent for the study . la radiologia medica ( 2020 ) 125 : 777783 radiotherapy incidental testicular doses duringvolumetricmodulated arc radiotherapy inprostate cancer patients cemonal1 recepbozca1 yemlihadolek1 ozancemguler1 gungorarslan1 received : 7 november 2019 / accepted : 19 february 2020 / published online : 3 march 2020 italian society of medical radiology 2020 abstract purpose to compare the incidental testicular doses during volumetric - modulated arc therapy ( vmat ) in patients receiving prostate - only and pelvic lymphatic irradiation . materials and methods testicular doses in 40 intermediateand high - risk prostate cancer patients were determined on treatment planning system ( tps ) using the vmat technique at 6mv . 
the mean cumulative scattered dose for prostate - only field delivering 78gy was 1.8gy and that for pelvic field irradiation was 2.6gy , consistent with the reported findings . conclusions the patients with prostate - only irradiation received lower testicular doses than those with additional pelvic field irradiation possibly due to the increased scattered doses in large field irradiation using the vmat technique . 
the clinical response to increased incidental testicular doses due to pelvic field irradiation remains unknown , and it warrants further investigation . keywords prostate cancer radiotherapy testicular doses dosimetry volumetric - modulated arc therapy introduction radiotherapy ( rt ) is an important treatment of choice for locally advanced prostate cancer patients [ 1 , 2 ]  . 
threedimensional conformal rt was traditionally used in prostate cancer treatment ; however , volumetric - modulated arc therapy ( vmat ) and intensity - modulated rt ( imrt ) , which can generate conformal isodoses in target volumes and can reduce normal tissue toxicity , are more frequently used and are accepted as standards of care in prostate rt [ 35 ]  . 
during prostate rt planning , the rectum , bladder , sigmoid , penile bulb , and femur doses are evaluated , but * cem onal hcemonal@hotmail.com 1 adana turgut noyan research andtreatment center , department ofradiation oncology , baskent university faculty ofmedicine , 01120adana , turkey incidental testicular doses are usually ignored . 
studies demonstrated that the range of incidental testicular doses during a full - course prostate rt is 84630cgy depending on the distance between the testes and the target volume [ 10 , 11 ]  . besides the systemic effects of testosterone levels , a decrease in serum testosterone levels exerts confounding effects on prostate - specific antigen after rt [ 12 , 13 ]  . 
this phenomenon is significant particularly in techniques such as pelvic field irradiation and dose - escalation trials , which potentially deliver high scattered testicular doses [ 10 , 14 , 15 ]  . 
vmat is an innovative form of imrt and is optimized for efficient delivery of radiation dose using a dynamic vol . : ( 0123456789 ) 1 3 778 la radiologia medica ( 2020 ) 125 : 777783 modulated arc . 
dosimetric studies demonstrated that surrounding organs are spared better in vmat technique than in imrt ; also , treatment time is shorter and the needed monitor units are fewer in the former [ 4 , 16 , 17 ]  . 
moreover , most studies evaluated the incidental testicular doses with treatment planning system ( tps ) , but scattered doses to the testes during prostate irradiation have rarely been evaluated with dosimetric measurements . this study compared the incidental testicular doses during vmat using the monte carlo algorithm - based tps in patients treated with prostate - only irradiation and pelvic lymphatic irradiation . 
to validate the accuracy of the tps , we performed invivo dosimetric measurements using metaloxidesemiconductor field - effect transistor ( mosfet ) detectors . materials andmethods patient simulation this study included 40 intermediateand high - risk patients treated for prostate cancer in our institution . 
for treatment planning , all patients underwent computed tomography ( optima 580 ct scanner , ge healthcare , waukesha , wi , usa ) at 2.5 - mm slice thickness with a comfortably full bladder and empty rectum , and the entire scrotum was included in the scan . 
the ctv was expanded to 8mm in all directions except posteriorly , extending by 5mm to this direction , to create a planning target volume ( ptv ) [ 15 , 17 ]  . 
the testes were contoured as one volume , excluding the skin , soft tissues , and epididymis . treatment plans the plans were calculated with the monaco treatment planning system ( elekta ltd , crawly , uk ) using the monte carlo algorithm and the sliding window multileaf collimator ( mlc ) delivery technique . 
a dose of 78gy was prescribed for the prostate and seminal vesicles in the intermediate - risk group , whereas an additional 54gy was prescribed for the pelvic lymphatics in the high - risk group ; the doses were delivered in 39 fractions . 
all treatment plans met the criteria for the ptv and the organs - at - risk dose constraints , and they were clinically acceptable for treatment delivery , which was previously described [ 17 ]  . dose verification withmosfet detectors the mosfet dose verification was performed for accuracy of doses between doses calculated with tps and doses measured with mosfet detector . 
the tps - predicted data were verified with the doses measured by the mosfet detectors ( tn - 1002 - rdh ; best medical canada , ottawa , canada )  . 
the mosfet detectors were put into the mosfet calibration jig , which was placed at 10 cm depth , sandwiched between the solid phantom plates , and irradiated with the prescribed dose . 
at 10 - cm - depth measurements , the doses calculated by the tps at field center was 100.8% in concordance with doses measured with mosfet detectors with vmat plans using 6mv photon energy . 
doses were measured from the isocenter of the plate phantom , field margin , and to 15cm with 5cm distances for both small field ( 10cm 10cm ) and large field ( 16cm 16cm ) [ 18 ]  . a second verification was performed to analyze the geometric errors of the mosfet detectors by using an anthropomorphic phantom ( rando , the phantom laboratory , salem , ny )  . 
for each measurement , we placed five detectors in the appropriate anatomic location on the rando phanto two detectors are placed at mid - testes , two at the base of testes , and one at apex . 
a correction factor was derived by dividing the measured doses from mosfet detectors and doses calculated from tps for same phantom and was then applied to the calculated testes doses for the study patients . testicular dose measurements the mean distance between the prostate and the testes was measured on tps by drawing a straight line between the midpoints of these two organs . 
additionally , scattered testicular doses were measured by mosfet detectors placed at the middle of the scrotufor each patient , mosfet 1 3 la radiologia medica ( 2020 ) 125 : 777783 measurements were taken on the first five treatment days , and the median doses were used for analysis . 
similarly , the mosfet readings significantly differed at 12 , 1214 , and > 14cm . phantom measurements for the first measurements of the vmat plan with solid phantom plates , the calculated dose for a single fraction by the tps at the isocenter was 252.4cgy , and the doses measured by the mosfet detectors at the isocenter were 259.7cgy , which is 2.9% higher than dose calculated with tps . 
the mean cumulative scattered dose for prostate - only field delivering 78gy was 176.3cgy , whereas that for pelvic field irradiation was 1 3 la radiologia medica ( 2020 ) 125 : 777783 and 255.8cgy , consistent with the reported findings [ 15 , 18 , 19 ]  . the contribution of scattered dose to the testes was relatively small ; however , the doses can add up to a potentially incidental dose that is toxic to leydig cells . 
data suggest that in older patients , the detrimental effect of irradiation on leydig cells may manifest even at doses as low as 24 gy [ 9 , 21 ]  . 
the hormonal changes caused by testicular radiation include a significant increase in luteinizing hormone and follicle - stimulating hormone , resulting in a decrease in testosterone levels by as much as 30% [ 9 , 2022 ]  . 
testicular doses are important because the negative effect on testosterone production is proportional to the dose to the leydig cells , and therefore , the time to testosterone recovery is proportional to testicular dose . 
a reduction in the mean serum testosterone level by 2030% relative to the baseline levels was observed within weeks of rt , and it persisted for months afterward [ 7 , 24 ]  . 
the proportional impact of field size and the consequent testicular scatter dose that translates into a dose - dependent effect on testicular function is consistent with the subset analysis of rtog 94 - 13 [ 25 ]  . 
 in another subset analysis of rtog94 - 13 , it was shown that with pelvic field irradiation , the mean time to recover the normal testosterone levels after treatment in patients with normal pretreatment levels was 1114months , and approximately 38% of the cases never recovered to normal levels [ 13 ]  . 
incidental testicular doses are important because of the indirect effect of testicular doses on testosterone recovery time , resulting in delayed onset of biochemical failure . several dosimetric studies evaluated incidental testicular doses mostly in rectal cancer patients [ 11 , 2123 , 26 ]  . 
in these studies , the testicular doses differ because different measurement techniques were used ( e.g. , dosimetric measurement or tps readings ) or due to the differences in testes positions in each rt fraction . 
additionally , radiation field size , photon energy , irradiation technique , and daily conebeam ct delivery directly affect incidental testicular doses [ 10 , 14 , 15 , 17 ]  . 
they found that the testes received 0.7cgy during the prostate imrt , and they also received 2.9cgy from the same cone - beam ct scan , addressing effects of cone - beam ct on testicular doses . 
 they concluded that incidental testicular doses during prostate imrt can be minimized by restricting the use of elective pelvic nodal fields , by choosing photon energies < 10 mv , and by using the smallest port sizes necessary for daily image guidance . 
computed tomography ( ct ) is essential to display the anatomy of the aortic valve complex ( including aortic annulus , valsalva sinuses , coronary arteries ostia , sinotubular junction ) , thoracoabdominal aorta , and vascular access . 
more recently , advanced computer modeling image - based techniques can be used to support the evaluation of the feasibility and safety of tavi procedures . keywords aortic valve stenosis computed tomography magnetic resonance imaging transcatheter aortic valve implantation introduction aortic valve stenosis ( as ) is the most common valvular heart disease ( vhd ) accounting for about 35% of moderate to severe native as [ 1 ]  . 
tavi is approved by several international societies in patients with severe symptomatic as at high surgical risk and with a life expectancy of more than 1year ( euroscore ii > 1520% or society of thoracic surgeons score > 810% ) [ 5 , 6 ]  . 
 giaccone , via del vespro 127 , palermo , italy 2 department ofbiomedicine , neuroscience andadvanced diagnostic ( bind ) , university ofpalermo , palermo , italy 3 department ofengineering , university ofpalermo , palermo , irccs istituto ortopedico galeazzi , milan , italy 5 department ofradiology , area vasta 1 / asur marche , 6 cardiovascular imaging unit , sdn foundation irccs , italy urbino , italy naples , italy 7 department ofradiology , fondazione istituto giuseppe giglio cefal , cefal , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 11481166 1149 before the intervention should be made by a multidisciplinary team of experts in vhd , including cardiologists , cardiac surgeons , geriatricians , anaesthesiologists , and cardiac radiologists [ 7 ]  . 
a poor outcome ( mortality rate ~ 50% ) is reported in the first two years , if patients are not treated or refuse the intervention because of the high peri - operative risk [ 9 ]  . 
since the introduction in 2002 , the tavi technique has revolutionized the treatment of severe as in high - risk inoperable patients because of low invasiveness [ 10 ]  . 
overall procedural risks and contraindications should be carefully taken into account by a heart team with specific competence in vhd ( table1 ) [ 4 , 7 , 11 ]  . 
surgery was associated with higher rates of acute kidney injury , atrial fibrillation , and transfusion requirements , whereas tavi had higher rates of residual aortic regurgitation and need for pacemaker implantation [ 14 ]  . 
transoesophageal echocardiography ( toe ) is considered the gold standard , especially when transthoracic echocardiography ( tte ) has poor acoustic window or in the suspicion of complications such as endocarditis . 
 in case of low flow ( stroke volume index < 35ml / m2 ) and low gradient ( < 40mmhg ) , the parameter of ejection fraction should be carefully evaluated with dobutamine stress echocardiography . nevertheless , echocardiography may have technical limitations in clinical practice due to poor acoustic windows of patients or lack of three - dimensionality of the method . 
 the quantification of aortic valve calcifications using the agatston score method ( based on a non - contrast ct ) can be useful , because the as severity increases with the amount of calcifications [ 21 ]  . 
 otherwise , cmr may deploy several modalities in the assessment of as : ava planimetry , using in - plane systolic images ; pressure transvalvular gradients , with phase - contrast velocity mapping ; left ventricular function , from ssfp cine sequences . 
heavy calcium load may affect the identification of the ava planimetry with cmr [ 23 ]  . nowadays , ct and mr are considered fundamental in the selection of candidates to tavi . 
an experienced radiologist should always integrate other experts of vhd in a dedicated team , as emphasized by main consensus documents [ 7 , 24 ]  . ct scan protocols in a scenario of extreme variation of ct technology between centers , the standardization of the scanning protocols should be pursued for tavi planning . a baseline acquisition is not necessary , but it can support the detection and quantification of calcifications similarly to the coronary arteries [ 25 ]  . 
the technological improvements in spatial and temporal resolution of recent years expanded the role of ct in the pre - tavi assessment , especially in the evaluation of aortic valve complex and annular size , which are essential for the choice of the prosthetic valve [ 24 ]  . initially , the role of ct was limited to the evaluation of peripheral vascular access for the interventional procedures . 
depending on the ct scanner technology ( 64 slices ) , cct and ct angiography of the aorta and peripheral vascular access can be obtained from a single acquisition ; however , in most cases two separate acquisitions during the same session are preferable [ 26 ]  . 
similar results were obtained also with modern single source ct scanners with novel high - pitch protocol , which allowed ct angiography for tavi planning with a similar radiation dose ( 3.3msv ) and contrast agent volume ( 60ml ) of dualsource ct [ 30 ]  . a contrast - enhanced ct acquisition protocol includes an ecg - gated scan of the aortic root ( slice thickness 1mm or less ; a systolic phase is mandatory )  . 
a retrospectively ecg - gated or prospectively ecg - triggered protocol should be used to assess the aortic valve complex including left ventricular outflow tract , annulus , sinuses of valsalva , coronary ostia , sinotubular junction , and ascending aorta . 
depending on 1 3 la radiologia medica ( 2020 ) 125 : 11481166 1151 the scanner technology , ecg - synchronized ct scan can be limited to the heart , or extended to the chest or the entire thoracoabdominal volume with increasing radiation dose . a volume of 5080ml of contrast is usually sufficient at a flow rate of 4 - 6ml / s , but it should be adapted to the scanner technology and body habitus of the patient . 
flow rate should be increased if the assessment of the coronary arteries is performed . cct oftheaortic valve complex cct became the technique of choice for evaluating the aortic anatomy and size . 
the measurement of the valve annulus area ( in mm2 or cm2 ) can be carried out manually or by means of semiautomatic software [ 24 ]  . annulus shape should be measured in systole . 
the use of the perimeter of the annulus rather than the area could lead to the choice of a larger prosthesis at higher risk of complications [ 32 ]  . 
this condition can be treated with tavi , although a higher risk of conduction disturbances and pacemaker implantation is associated [ 33 ]  . another fundamental parameter is the presence of calcifications in the so - called device landing zone which includes valve cusps , annulus and left ventricular outflow tract . it has been proved that the presence of robust calcifications is associated with an increased risk of paravalvular leaks or conduction disturbances [ 34 ]  . 
the amount of calcifications is usually evaluated qualitatively ( absent , mild , moderate , severe ) , with reference to the number ( single or multiple ) , extent ( symmetric , asymmetric , circumferential ) , position ( annular or sub - annular ) , and thickness ( linear , nodule - like )  . 
 severe as is considered likely with scores 2000 for men and 1200 for women , while it is reported unlikely with scores < 1600 for men and < 800 for women [ 4 , 21 , 25 ]  . a short coronary height from the annulus ( < 12mm ) is associated with an increased risk of periprocedural coronary occlusion due to the dislocation of the calcified native cusp over the coronary ostium [ 36 ]  . 
coronary obstruction remains a rare but potentially life - threatening complication of tavi and occurs often in females with no prior cabg and in patients receiving a balloon - expandable prosthetic valve . 
 the dimension of the sinuses of valsalva and the presence of protruding calcification might also play an important role in the occurrence of this complication ( fig.4 ) [ 37 ]  . sinus of valsalva , sinotubular junction , and ascending aorta diameters should be evaluated on a transverse and double - oblique plane . 
 the sinotubular junction can be damaged using balloonexpandable prosthetic valve in short height anatomies [ 24 ]  . ct can be used to identify patient - specific optimal c - arm angulations for tavi procedure , reducing multiple predeployment aortograms and associated increased procedural time , contrast volume and radiation dose [ 38 ]  . measurements should be performed accurately for viv procedures in case of failure of a previous surgical valve . 
 in this regard , the distance to the coronary ostia should be carefully measured because of the increased risk of coronary obstruction by the leaflets or struts of the previous surgical valve . 
nevertheless , the simultaneous acquisition of the aortic valvular complex and coronary arteries can avoid the administration of a second dose of contrast media and reduce the risk of induced nephropathy . 
 advanced ct scanner technology allowed the evaluation of the coronary arteries with a good diagnostic accuracy despite a relatively lower specificity in patients with severe coronary calcifications ( table2 ) [ 4249 ]  . 
cct should be considered to exclude obstructive cad or anomalous coronary arteries , when local expertise is available and optimal image quality is achieved [ 24 , 5052 ]  . 
4 the panel shows a 84years old woman undergoing ct for pretavi evaluation : aortic annulus ( a ) , tricuspid aortic valve with severe asymmetric calcifications ( b ) , ascending aorta ( c ) , right coronary height ( black arrow ) ( d ) , left coronary height ( black arrow ) ( e ) , aortic valve and coronary calcifications ( f ) 1 3 la radiologia medica ( 2020 ) 125 : 11481166 1155 fig . 
cross - sectional views of the aortic annulus in absence of calcifications ( g ) , tricuspid valve at non - contrast ct ( h ) and at contrast ct with severe calcium amount ( i ) 1 3 1156 la radiologia medica ( 2020 ) 125 : 11481166 table 2 diagnostic accuracy of computed tomography angiography for the detection of coronary artery disease in patients referred to tavi slices population ( n ) stenosis ( % ) sensitivity ( % ) ppv ( % ) npv ( % ) specificity strong etal . 
6 evaluation of vascular access routes at ct ( ac ) and mri ( d ) : patient with normal aorto / ilio / femoral vasculature ( a ) , patient with large abdominal aorta aneurysm ( white arrowhead ) and left iliac occlusion ( black arrowhead ) ( b ) , patient with multiple aorto - iliac endoprosthesis ( c ) , patient with regular subclavian access routes ( d ) revascularization should be considered in patients undergoing tavi with a stenosis > 70% in proximal coronary segments according to current esc guidelines [ 4 ]  . 
in this regard , radiologists should be encouraged to include the assessment of coronary arteries in tavi planning reports . assessment ofvascular access the anatomical evaluation of vascular accesses remains an important step for the choice of the interventional approach . 
it is recommended to evaluate the minimal diameter ( 5.5mm ) of the ilio - femoral system and describe the parietal calcifications , especially that in the anterior wall at the possible site of puncture . 1 3 la radiologia medica ( 2020 ) 125 : 11481166 1157 fig . 
7 the panel shows post - contrast ct of an iliac arteries occlusion in pre - tavi planning : multiplanar reconstructions ( a , c ) and axial ct images ( b , d ) extracoronary findings lastly , radiologists should report non - cardiac and nonvascular relevant incidental findings . 
at present , ct imaging following tavi is not recommended , because of the additional dose of contrast media in a population at high - risk of acute kidney failure [ 24 ]  . 
ct may also evaluate postoperative findings of the aorta and peripheral vessels including dissections , pseudoaneurysms and bleeding at the puncture site [ 58 ]  . ct reporting should be standardized and structured to ensure that relevant features and measurements are clearly provided ( table3 )  . 
non - contrast , navigator gated 3d - mri angiographies ( mra ) have been used for the assessment of aortic annulus , coronary ostia heights and vascular accesses in patients undergoing tavi [ 60 ]  . 
 in case of renal failure , 3d steady - state free precession ( ssfp ) navigator - echo and ecg - gated sequence can be applied for the thoracic aorta evaluation . 
the use of ssfp sequences in long axis and short axis allows obtaining images with an in - plane spatial resolution close to that of toe for the dynamic evaluation of the aortic valve and left ventricle [ 61 ]  . cmr with late gadolinium enhancement technique provides optimal assessment of the myocardial characteristics including fibrosis and ischemic conditions of the left ventricle with additional prognostic information regardless of the presence of cad . 
if contrast medium can be administered , a multi - step contrastenhanced mr angiography ( ce - mra ) can be done starting from the aortic arch to proximal femoral arteries . 
one of the greatest advantages of using cmr is related to the use of phase - contrast sequences that allow flow quantification and distinguish between supra - valvular and subvalvular stenosis . 
showed that the evaluation of effective orifice area with cmr phase - contrast sequences for bioprosthetic aortic valves is accurate and may add an important additional parameter to doppler assessment [ 64 ]  . a comprehensive mri protocol should include several sequences as depicted in table4 . mri can be a valid alternative to ct for pre - tavi evaluation , especially in patients with renal failure or allergy to iodinated contrast medium when ct cannot be performed . 
 potentially , a free ionizing radiation technique should be more extensively taken into account if younger groups of patients will undergo tavi in the future . pretavi computer simulation high - resolution volumetric ct image datasets can be integrated with computer modeling techniques to provide a virtual evaluation of the feasibility and safety of tavi . 
9 cardiac magnetic resonance of a patient with severe aortic stenosis : signal void artefact in left ventricle outflow tract in ssfp sequence ( a , b ) ; the patient showed sub - epicardial delay enhancement in the inferior wall of middle - distal tract ( c , d ) analysis ( fea ) , which correlates the spatial and geometrical position of the aortic root to the biomechanical response . 
for computer modeling , ct imaging is the most attractive method , because it allows fast and accurate acquisition of 3d - data of the aortic root with higher spatial resolution compared to echocardiography or mri . numerical simulations of tavi demonstrated the presence of stress concentration induced by the contact between the device frame and the aortic wall [ 65 ]  . 
10 cardiac magnetic resonance of a patient with unknown severe ischemia : left ventricular dilatation with a severe impaired function ( ejection fraction of 14% ) in ssfp sequence ( a ) ; trans - mural hyperintensity in short axis delayed enhancement sequences ( b , c ) with a thrombus showed in panel b table 4 magnetic resonance imaging sequences for tavi planning sequences ssfp white or black blood ecg - gated half - fourier fse images target chest evaluation cardiac function analysis evaluation of aortic root , annular and sinus measurements , height of coronary ostia evaluation of aortic root , annular and sinus measurements , height of coronary ostia phase - contrast contrast - enhanced mr angiography ( ce - mra ) ; 3d - ssfp navigator - echo and ecg - gated ; nonvalvular evaluation vascular evaluation of access route contrast - enhanced mra delayed enhancement short and long - axis ir t1 - weighted images myocardial characterization and fibrosis ssfp steady - state free precession ; fse fast spin - echo ; mra magnetic resonance angiography the impact of aortic root anatomy on the tilt angle of the device , and the influence of the calcification patterns and native leaflet morphology on the outcome of tavi were also highlighted [ 67 ]  . 
11 framework for the computer simulation of tavi : ct imaging , anatomic reconstruction , analysis of biomechanical properties and output results of the device conformation to the bicuspid anatomy [ 69 ]  . 
computer simulations of the pressure generated by the metallic device frame on the atrioventricular conduction pathway can predict patients with high risk of conduction abnormalities [ 70 ]  . tavi simulation and modeling can pre - operatively inform clinicians on the optimal size and positioning of device , partly surpassing the basic ct - derived anatomical measurement . 1 3 la radiologia medica ( 2020 ) 125 : 11481166 1163 fig . 
12 simulation of tavi with different device sizes : scenario #1 shows the deformed shape of the 23 mm edwards sapien 3 ultra device ( a ) , while scenario #2 shows results with the 26mm edwards sapien 3 ultra device ( b )  . 
in hypertrophic forms , cmr provides : precise evaluation of wall thickness in all segments , ventricular function and size and evaluation of possible presence of areas of fibrosis as well as changes in myocardial tissue ( measurement of t1 mapping and extracellular volume values )  . 
cmr highlights also the potential alterations of the myocardial tissue . keywords cardiac magnetic resonance ( cmr ) myocardium cardiac hypertrophy cardiac dilatation late gadolinium enhancement ( lge ) t1 mapping introduction cardiomyopathy ( cmp ) is a disease that primarily affects the heart muscle with a heterogeneous clinical presentation and natural history [ 1 , 2 ]  . 
primary forms of cmp must be distinguished from secondary forms , in which the myocardial alteration is caused by a different pathology , such as a ventricular dilatation post - myocardial infarction associated with coronary artery disease ( cad )  . 
the recognition of familial cmp is important in creating a patients pathway , highlighting when screening of relatives is necessary , and distinguishing familial cmp from non - genetic forms of the disease ( i.e. , post - viral , autoimmune , immune - mediated * silvia pradella pradella3@gmail.com 1 department ofradiology , careggi university hospital , largo brambilla 3 , 50134florence , italy sporadic cmps , or from toxicity linked to endogenous or exogenous causes such as drugs and toxic agents )  . 
since the world health organization ( who ) provided the first definition of cmp , there have been numerous classifications based on the morphology , origin ( genetic and non - hereditary ) , and on a more complex functional morphology and classification scheme [ 1 , 3 ]  . 
a continual drive to acquire a more in - depth knowledge of the various phenotypes , and how these are linked to the etiology of cmp and its genetic basis , has led to imaging in cmps playing an increasing role . 
when considering imaging , it is easier to follow a morphological classification that recognizes the following cmps : the most frequent hypertrophic cmps ( hcm ) associated with ventricular thickening ; dilated cmps ( dcm ) , associated with an increase in ventricular volume ; and the remaining cmps associated with specific characteristics including arrhythmogenic right ventricular cmp ( arvc ) , restrictive cmp ( rcm ) , and unclassified cmps [ 3 , 5 , 6 ]  . 
cmp may remain asymptomatic for a long time , but as the disease progresses , disorders relating to heart failure vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 10561071 1057 may appear , such as breathing difficulties ( both under stress and at rest ) , swelling in the legs , ankles , and feet , coughing , fatigue , arrhythmias or palpitations , dizziness , and syncopation . 
the use of 3d echo reduces some of the limitations of the standard two - dimensional technique , and with dedicated applications , it is possible to evaluate deformations of the ventricular wall . 
 furthermore , echocardiography provides for the evaluation of the diastolic function as well as an accurate assessment of the valve systehowever , all these possibilities are sometimes limited by a suboptimal acoustic window and interobserver variability . 
conversely , cardiac magnetic resonance ( cmr ) imaging is not only the gold table 1 cardiomyopathy imaging features standard for measuring volumes and cardiac mass , but also the only method that allows for tissue characterization [ 12 , 13 ]  . 
the most modern sequences , such as the mapping of t1 and t2 , allow us to measure the values of myocardial t1 ( native t1 ) , the extravascular cellular volume ( ecv ) on post - contrast maps , and t2 values [ 1 , 10 , 14 , 15 ]  . 
however , technological advancements also make this method a valid tool for anatomical ( e.g. , measurement of volumes and ventricular thicknesses ) and functional ( e.g. , using multi - phasic cine ct images global and regional kinetic ) evaluation . 
furthermore , with the most advanced scanning techniques it is possible to study dynamic perfusion and , with the use of dedicated software , to obtain iodine distribution maps [ 1622 ]  . in this review , we will describe the contribution of imaging in the diagnosis of the most common primitive forms of the disease : hypertrophic and dilated cmps ( table1 )  . 
elevated t2 values have been reported in patients with idiopathic dcm 1 3 1058 la radiologia medica ( 2020 ) 125 : 10561071 dysfunction and structural alterations such as the disarray of myocardial fibers and interstitial and focal fibrosis [ 3 , 4 ]  . 
in 70% of cases , it has a familial orig earlier and more severe phenotype of hcm is associated with mutations in the - myosin heavy chain gene , myh7 . 
most commonly , this is observed as an asymmetrical thickening of the septuhowever , hypertrophy can also affect the apex of the left ventricle ( lv ) , can be concentric , predominantly posterior , or also involve the right ventricle ( rv ) [ 24 ]  . 
atrial fibrillation is the most frequent arrhythmia in patients with hcm , and left atrium ( la ) dilation predisposes patients to the risk of atrial fibrillation [ 12 , 25 ]  . 
cmr imaging provides information concerning the stratification and prediction of risk of atrial fibrillation ( af ) and heart failure ( hf ) [ 2 , 4 , 26 ]  . 
the presence and extent of fibrosis in lge correlates with the risk of scd / implantable cardioverter - defibrillator ( icd ) [ 27 ]  . cmr provides key information in relation to hcm pathology by making use of anatomicalfunctional sequences and tissue characterization sequences . 
traditionally , cine sequences , steady - state free precession ( ssfp ) , have been used to evaluate the volumes , thicknesses , and function of lv and rv in the cardiac planes ( short axis , 2 , 3 , and 4 chambers ) , usually acquired with patient breath - hold or with new techniques in free breathing [ 14 ]  . 
the volume of the left atrium must also always be calculated in these patients ( using the biplane arealength method and indexed for body surface area ) [ 12 , 28 ]  . in hcm , the thickness of the lv wall is increased in a predominantly asymmetrical manner ( > 15mm in one or more myocardial segments ) , typically involving the septum in 70% of patients [ 1 , 2 ]  . 
different types of hcm are described according to the location in the heart of the thickened area of muscle [ 7 , 8 ]  . asymmetrical septal hypertrophy it is the most common presentation of the disease . 
when surgically correcting obstructive forms , it is often necessary to repair not only the septal thickening but also the mitral alteration [ 35 ]  . apical hypertrophy the thickened area is at the apex ( 1% ) of the heart ; it is also known as yamaguchi syndrome . 
in the japanese population , apical hcm accounts for approximately 15% of cases , while in caucasian populations , it accounts for up to 2% of cases [ 36 ]  . midventricular hypertrophy obstructive cardiomyopathy andlv apical aneurysm mid - ventricular hypertrophic obstructive cardiomyopathy ( hcm - mvo ) is characterized by asymmetric left ventricular hypertrophy with mid - ventricular obstruction . 
hcm - mvo is a rare type of cardiomyopathy ( incidence about 1% ) ; several studies suggest that this subtype has worse outcomes than the common type of hcm and different genetic basis ( fig.4 ) [ 37 , 38 ]  . this form may be present in patients who also have apical hypertrophy or apical aneurysthe 2% of hcm patients have an apical aneurysin these cases , the ventricle wall can be thinned or hypokinetic . 
it is important to demonstrate the possible presence of cmr on regional scaring and to exclude the presence of apical thrombosis ( fig.5 ) [ 39 , 40 ]  . symmetrical hypertrophy the thickening affects the whole of the lv , reducing its volume . 
in these cases , the cmr contributes to get differential diagnosis from other causes of symmetrical myocardial hypertrophy , including mild or moderate hypertrophy in hypertensive heart disease and aortic stenosis or athletes heart and other causes of myocardial hypertrophy ( e.g. , infiltrative diseases as cardiac amyloidosis or fabry disease ) ( fig.6 ) [ 41 ]  . right hypertrophy when we talk about hypertrophic cmp , we are usually referring to a thickening of the lv , even if we must not forget that 1 3 la radiologia medica ( 2020 ) 125 : 10561071 1059 fig . 
1 asymmetric hypertrophy of the middle septum with a maximum thickness of 24 mm ( white line ) on the cine short - axis ( a ) and cine 4 - chamber ( b ) view . 
2 a 55 - year - old female : asymmetric hypertrophy with maximum thickness at level of basal and middle septum ( 21 mm ) ( white line ) ( a ) ; lateral wall of lv with a thickness of 10mm and hyper - trabeculated and spongy appearance ( white arrowhead ) ( a ) ; signs obstruction in the outflow tract ( black arrow ) ( a , b )  . 
a 40 - year - old male : thickening of septum at the basal segment ( 24mm ) ( white line ) with obstruction in the outflow tract and elongated aspect of the anterior mitral flap ( white arrowhead ) ( c ) the rv can also be involved ( fig.7 ) [ 42 ]  . 
the wall of the rv may be affected by fibrosis , and a detailed description of the alterations affecting 1 3 1060 la radiologia medica ( 2020 ) 125 : 10561071 fig . 
3 hypertrophy of apical segments on cine 2 - chamber ( a ) and 4 - chamber ( b ) ( white arrow ) with a reduction in the ventricular cavity at this level ; enhancement of hypertrophic segments on lge sequences ( white arrowhead ) ( c , d ) fig . 
4 medium ventricular hypertrophy with globular aspect of the apex of the lv ( star ) ( a ) and dimensional reduction in the ventricular cavity ( white arrow ) ( b ) 1 3 la radiologia medica ( 2020 ) 125 : 10561071 1061 fig . 
5 a 63 - year - old male with medium ventricular hypertrophy and dilated globular aspect of the apex of the lv , with the presence of apical thrombosis ( white arrow ) ; also , pericardial effusion is present ( a , b )  . 
7 a 73 - year - old male : hypertrophy of the rv especially at the apical ( white arrow ) ( a ) and infundibular ( white arrowhead ) site where the thickness is 6.7mm ( b ) 1 3 1062 la radiologia medica ( 2020 ) 125 : 10561071 the rv should be part of the evaluation of a patient with hcm . late gadolinium enhancement additional morphological findings when the hypertrophic phenotype is slight ( mild phenotype ) , there are additional findings that may be present . 
that are typical of hcm such as anterior mitral valve leaflet elongation , myocardial crypts , para - septal muscle bundle , and abnormal apical trabeculation often found in both evident and mild hypertrophic forms ( fig.8 ) [ 31 ]  . 
 the sequences for the evaluation of the lge can also assist in the follow - up of patients to determine the evolution of the pathology [ 44 , 45 ]  . t2weighted sequences andt2 maps role ofcardiac ct the role of the classic t2 fat suppression sequences ( which highlight the presence of edema areas ) is currently debated . 
 the presence of focal hyperintensity areas in t2 , possibly confirmed by t2 maps , can be important for arrhythmic risk stratification ( figs.9 , 10 ) [ 43 ]  . a noninvasive study of coronary arteries can be useful in these patients . 
the new ct applications also present an alternative to cmr in demonstrating perfusion alterations and the presence of fibrosis [ 21 , 46 , 47 ]  . differential diagnosis t1 mapping the t1 values measured in the native maps in hypertrophic cmps are increased , as well as the expansion of the extracellular volume ( ecv ) obtained from the preand post - contrast maps . 
native t1 values are significantly elevated in both non - hypertrophic and hypertrophic segments of hcm patients compared with controls [ 15 ]  . it is important to be able to differentiate the forms of hcm from the paraphysiological and pathological conditions in which vs is hypertrophic . 
in athletes , there may be an increase in heart mass with a thickening of the lv which , unlike the typical form of hcm , is symmetrical , rarely exceeds 14mm , and fig . 
8 a 72 - year - old male with deep crypt at the basal inferior region in end - diastole ( white arrow ) ( a ) and hypertrophy of the middle and basal septum ( white arrow ) ( b ) 1 3 la radiologia medica ( 2020 ) 125 : 10561071 1063 fig . 
9 a 48 - year - old male with asymmetrical hypertrophy - involved anterior septum and anterior wall at the basal level of the lv ( a ) ; presence of edema as focal hyperintensity areas within the thickened region ( white arrow ) on t2 fat suppression sequence ( b ) ; enhancement of the hypertrophic segments of lv on lge sequences 2 - chamber ( c ) and short - axis ( d ) ( white arrowhead ) regresses after a rest period ( usually as early as 3months ) [ 48 , 49 ]  . 
in infiltrative pathologies such as fabry disease ( fd ) or cardiac amyloidosis ( ca ) , cmr with tissue characterization sequences ( e.g. , mapping ) can be decisive [ 5052 ]  . 
the prevalence of dcm ranges from 1 in 25 , 00 to 1 in 250 people , mainly due to changes in diagnostic criteria and geographical variations [ 7 , 23 ]  . 
advances in pharmacological and surgical treatment have significantly improved the prognosis of dcm with an estimated survival of up to 85% at 10years free from heart transplantation [ 57 ]  . 
 lv reverse remodeling ( lvrr ) , defined as an improvement in lv ejection fraction ( lvef ) and a reduction in lv enlargement , is one of the main determinants of prognosis in dcm , and it is the key therapeutic goal . 
cardiac adverse remodeling characteristics in dcm include lv dilation and wall thinning , lv dyssynchrony manifested by left bundle branch block , functional mitral regurgitation , myocardial fibrosis , remodeling of other cardiac chambers , and rv dysfunction . detailed characterization of these parameters has a pivotal role in the prognostic stratification of dcm patients and in improving clinical management [ 23 , 58 ]  . 
diffuse hypertrophy asymmetric with a maximum thickness at the level of the septum of 28mm ( a ) and diffuse hyperintensity areas in t2 - weighted sequence ( white arrowhead ) ( b ) ; on lge sequences 4 - chamber intra - myocardial enhancement of septum and lateral wall ( white arrow ) ( c ) ; cine 4 - chamber sequence shows the presence of a deep crypt in the lateral wall at the medium level ( white arrow ) ( d ) rather an end - stage manifestation of complex interactions between environmental insults and genetic predisposition is gaining acceptance [ 23 , 58 ]  . 
mutations in over 40 different genes , encoding cytoskeletal , sarcomeric , mitochondrial , desmosomal , nuclear membrane , and rnabinding proteins , have been implicated in the pathogenesis of dcm . 
mutations in the lmna gene ( encoding lamin a / c ) cause up to 10% of dcm characterized by conduction system disease ( atrioventricular block ) and increased risk of life - threatening ventricular arrhythmias [ 59 ]  . 
secondary causes of dcm include infectious agents ( particularly viruses often producing myocarditis ) , toxins ( including chronic excessive consumption of alcohol , chemotherapeutic agents , cocaine ) , autoimmune and systemic disorders ( including sarcoidosis , hemosiderosis , vasculitis , connective tissue disorder ) , neuromuscular disorders ( such as duchenne / becker muscular dystrophies ) , metabolic , endocrine ( i.e. , cushing disease ) and nutritional disorders ( i.e. , carnitine , selenium deficiencies ) , and the presence of persistent tachyarrhythmia and pregnancy ( peripartum cmp ) [ 7 ]  . 
since the term dcm refers to a spectrum of genetic and acquired disorders that manifest as dilated phenotype , identification of a specific underlying etiology is crucial so that targeted disease - specific therapy may be given to improve prognosis . 
in addition , echocardiography is an important tool for prognostic stratification allowing the identification of many aspects of cardiac remodeling , such as functional mitral regurgitation [ 57 ]  . recent advances in technology , such as strain analysis and 3d echocardiography , have improved the diagnostic and prognostic capabilities of this technique . 
cmr not only represents the gold standard for an accurate and reproducible assessment of ventricular volumes and function , but it is also the only technique that provides noninvasive tissue characterization . 
11 asymmetric hypertrophy of the whole septum with a maximum thickness of 32 mm ( white line ) on the cine short - axis ( a ) and cine 4 - chamber ( b ) sequences . 
diffused enhancement of the interventricular septum on lge sequences ( white arrow ) ( c , d ) techniques such as lge and qualitative / quantitative parameters including t1 mapping , t2 mapping , and t2 * mapping , tissue characterization is useful in the differential diagnosis of secondary causes of dcm and in the assessment of the probability of lvrr with a potential role in guiding individualized treatment strategies [ 54 , 55 , 61 ]  . an accurate and reproducible cardiac evaluation always includes chamber size quantification , myocardial wall thicknesses , ventricular function and mass measurement with traditional cine sequences , steady - state free precession ( ssfp ) , in short and long axis ( 2 , 3 , and 4 chamber ) view . 
at present , lvef is considered one of the most important prognostic factors in dcm , and current guidelines recommend icd in symptomatic heart failure with lvef less than 35% . 
in addition , velocityencoded cmr is a useful alternative to echocardiography for evaluating functional mitral regurgitation , another aspect of adverse myocardial remodeling . the use of tissue characterization cmr sequences is fundamental in this pathology . t2weighted sequences andt2 maps t2 - weighted sequences with fat suppression highlight the presence of myocardial edema in inflammatory cmp or in acute myocardial infarction . 
t2 - weighted short - tau inversion recovery ( t2w - stir ) ecg - gated triple inversion recovery ( ir ) technique is recommended [ 1 , 62 ]  . 
also , if a pathology 1 3 1066 la radiologia medica ( 2020 ) 125 : 10561071 such as acute or chronic myocarditis , takotsubo syndrome , sarcoidosis , or acute myocardial infarction is suspected the t2 imaging is mandatory [ 54 , 61 ]  . as an early imaging marker of adverse outcomes before the presence of lge [ 7 ]  . late gadolinium enhancement t1 mapping t1 mapping and extracellular volume calculation allow for the noninvasive detection of diffuse fibrosis . 
furthermore , an increased native t1 value seems to be present the pattern of lge allows for the differential diagnosis between ischemic and non - ischemic dcm with good specificity . 
on the other hand , approximately 30% of dcm cases have a characteristic linear midwall pattern of lge in a non - coronary distribution , predominantly within the interventricular septum ( fig.13 ) [ 8 , 24 , 64 ]  . 
12 a 53 - year - old female with dilated cmp : on cine short - axis sequence , the inferiorlateral wall appears markedly thinned ( white arrow ) ( a ) , due to the presence of an ischemic alteration ( white arrow ) seen as an area of hyper - enhancement on lge sequences , in short ( b ) and long - axis 2 - chamber ( c ) fig . 
13 patient affected by primary dilated cmp : on short ( a ) and long - axis 4 - chamber ( b ) characteristic linear midwall pattern of lge ( white arrow ) within the interventricular septum , in a non - coronary distribution 1 3 la radiologia medica ( 2020 ) 125 : 10561071 1067 therapeutic implications . 
 randomized trials , such as the recent danish trial , have not shown that icd implantation guided by lvef alone is associated with improved clinical outcomes [ 27 ]  . 
these findings have increased the interest on the potential role of cmr in the prognostic stratification of dcm helping to assess the risk for sudden cardiac death and the probability of lvrr ( fig.14 ) [ 2 , 7 , 61 ]  . 
myocardial fibrosis is a pathophysiologic component of dcm and can be detected by cmr in two forms : as lge , which corresponds to irreversible replacement fibrosis , and as t1 mapping alterations corresponding to diffuse interstitial fibrosis . 
in a study of lamin a / c mutation carriers having undergone cmr , typical midwall myocardial fibrosis in the lv septum was observed in 88% of lmna mutation carriers , and this correlated significantly with the presence of conduction abnormalities . 
14 a 49 - year - old male with end - stage dilated cmp ( 24% ejection fraction ) ( a , b ) with markedly thinned and unpacked wall ( white arrow ) ( c ) ; presence of enhancement in most cardiac segments on lge sequences ( white arrowhead ) ( d ) 1 3 1068 la radiologia medica ( 2020 ) 125 : 10561071 lge may be used to guide icd implantation . 
it may be reasonable to postpone icd implantation in dcm patients without lge because they have a high chance of lvrr and a low risk of scd even when lvef is < 35% [ 7 ]  . further studies are required to confirm the role of cmr in the risk stratification of dcm and to be able to assess if cmr - guided icd implantation is able to improve survival in dcm . 
however , cmr parameters , such as lge and t1 and t2 mapping , used as part of a multiparametric approach , promise to improve clinical outcomes and management in dcm [ 1 , 2 , 54 ]  . role ofcardiac ct in the diagnostic workup of systolic dysfunction , cct is recommended in order to rule out ischemic heart disease as an alternative to invasive coronary angiography in patients with low pretest probability . 
however , cct is emerging as an alternative method to cmr for the detection of myocardial fibrosis in patients with contraindications to perform cmr [ 18 , 47 , 68 , 69 ]  . 
cct may be useful in patients with suboptimal echocardiography and who are unable to undergo cmr due to contraindications , such as pacemakers and defibrillators [ 21 ]  . differential diagnosis the identification of a reversible cause appears essential to promote targeted disease - specific treatment to induce lvrr and improve clinical outcome . 
the diagnosis of cmp related to cardiotoxins , such as alcohol , cocaine , amphetamines , or anabolic steroid , can be made in the presence of lv dilation and dysfunction in patients with history of substance abuse and no other known causes of myocardial disease ( fig.15 ) [ 53 , 56 ]  . 
the onset of hf toward the end of pregnancy , or in the months after delivery , suggests peripartum cmp but in order to confirm the diagnosis alternative causes of cmp should be excluded . 
cmr with tissue characterization sequences aids the differential diagnosis of secondary causes of dcm , including inflammatory , autoimmune , neuromuscular diseases and toxic forms or several end - stage cmps [ 62 , 70 ]  . 
lge positivity , edema on t2 - weighted images , and hyperemia on early postgadolinium t1 - weighted sequences represent the so - called lake louise criteria [ 70 , 71 ]  . 
cmr can identify early cardiac involvement in autoimmune cmp , such as systemic lupus erythematosus or rheumatoid arthritis , showing evidence of inflammation [ 56 ]  . conclusions the use of cmr in cmps is of crucial importance today . 
mapping sequences add significant quantitative data , with both t1 and t2 maps . funding the authors received no financial support for the research , authorship , and / or publication of this article . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethics approval although the nature of our study is a review regarding the material used ( images ) , all procedures performed involving 1 3 la radiologia medica ( 2020 ) 125 : 10561071 1069 fig . 
15 a 53 - year - old male with dilated cmp related to abuse of anabolic steroid and ejection fraction of 15% ; on 4 - chamber cine sequence lv is markedly dilated ( a ) ; sub - epicardial and meso - cardial alteration in lateral wall ( white arrowhead ) ( b ) and linear midwall enhancement within the interventricular septum ( white arrowhead ) ( c ) on lge ; increased native t1 values at the altered segments ( 1063 22ms ) ( d ) human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
although the cardiac imaging with interventional procedures is responsible for approximately 40% of the cumulative effective dose in medical imaging , a relevant radiation dose reduction over the last decade was obtained , with the beginning of the sub - msv era in ctca . 
the main technical basis to obtain a radiation dose reduction in ctca is the use of a low tube voltage , the adoption of a prospective electrocardiogram - triggering spiral protocol and the application of the tube current modulation with the iterative reconstruction technique . 
finally , because anatomical evaluation not adequately predicts the hemodynamic relevance of coronary stenosis , a low radiation dose in routine ctca would allow the greatest use of the myocardial ct perfusion , fractional flow reserve - ct , dual - energy ct and artificial intelligence , to shift focus from morphological assessment to a comprehensive morphological and functional evaluation of the stenosis . 
 therefore , the aim of this work is to summarize the correct use of the technical basis in order that ctca becomes an established examination for assessment of the coronary artery disease with low radiation dose . keywords cardiac ct coronary ct dual - source ct high - pitch protocol radiation dose radiation reduction introduction cardiac imaging has emerged over the past two decades as one of the most important and dynamic advances in radiology , and the computed tomography coronary angiography ( ctca ) has become a cornerstone in the diagnostic process of heart disease . 
in particular , for patients with suspected coronary artery diseases , the ctca has high sensitivity and negative predictive value to rule out obstructive stenosis and it allows avoiding many invasive coronary angiography [ 1 , therefore , the number of ctca is rapidly increasing and cardiac imaging with interventional procedures is * marco fogante marco.fogante89@gmail.com 1 radiology department , azienda ospedaliero universitaria ospedali riuniti , 60126ancona , italy 2 radiology department , azienda ospedaliero universitaria san salvatore , 60126laquila , italy responsible for approximately 40% of the cumulative effective dose ( ed ) in medical imaging . 
in this regard , the cumulative radiation exposure during ctca has to be taken into account , because this is known to amplify long - term carcinogenesis in a dosedependent stochastic manner [ 1 , 3 , 4 ]  . the 2017 international dose survey described a tremendous radiation dose reduction ( 78% ) over the last decade in cardiovascular ct , and the many works reported case studies with mean eds lower than one msv [ 5 ]  . 
however , the low radiation dose in cardiovascular ct imaging requires several other modifiable factors , such as the experience of radiologist , the availability of modern ct scanners and radiation dose - efficient protocol . 
therefore , ctca examinations are characterized by a wide range of radiation doses between different radiology vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 10241039 1025 departments , and despite some patients receiving extremely low radiation doses , many others still receive considerably higher doses [ 2 , 5 ]  . 
moreover , the dose exposure in ctca is extremely important because the benefitrisk calculus in comparison with other modalities also depends on the radiation dose , and although several studies have evaluated strategies to obtain this goal , the radiation dose reduction in ctca , while maintaining image quality , is still a challenging task [ 2 , 5 , 6 ]  . therefore , the aim of this work is to summarize the correct use of the technical basis in order that ctca becomes an established examination for assessment of the coronary artery disease with low radiation dose . technical basis related toradiation dose the ed is the radiation value most commonly used to compare ionizing radiation burden between different imaging modalities and protocols . 
in accordance with the formulation of the international commission on radiological protection , ed is defined as the sum of weighted organ - absorbed doses , where weights reflect both the relative sensitivity of each organ to radiation and the radiation source . 
the k - factor adopted by the european commission guidelines and the american association of physicists in medicine for adult chest ct scans is 0.014msvmgy1cm1 [ 2 , 3 ]  . the technical basis to reduce radiation dose , in ctca , is related to the recent advances on technology of the new ct scanners . 
technical basis to reduce radiation dose is summarized in table1 . scanner technology the shorter scan times and higher resolution were the driving forces behind the development of the ct technology . 
 new ct scanners have greater gantry rotation speed , higher pitch value , more rows to the detector panel and better performance of the x - ray tubes [ 8 ]  . 
ct scanners with 256 - , 320 - slice and over have a wide - area detector large enough to cover the entire heart in a single prospectively sequential acquisition , and they have the potential to acquire dynamic volume data by repeatedly scanning the same anatomical range without table movement [ 9 , 10 ]  . 
on the other side , to obtain a higher - speed acquisition acting on the pitch , the conventional single - source ct scanners are limited in increasing its pitch factor because of an interpolation artifact problethe dual - source computed tomography ( dsct ) scanners , with two x - ray tubes and two detectors arranged at an angle of about 90 , allow increasing pitch values , up to 3.4 , without interpolation artifact . 
moreover , because only one - quarter rotation of the gantry is required to acquire the data for one cross - sectional image , dsct scanners double the temporal resolution than of the single - source ones [ 4 , 1114 ]  . tube voltage lower tube voltage allows high radiation dose reduction , because it roughly changes with the square of the tube voltage . 
moreover , tube voltage reduction with 7080kvp can be successfully used in ctca with beneficial effects on image quality and improved vascular attenuation because effective photon energy is closer to the k - edge of iodine ( 33.2kev ) [ 15 ]  . 
therefore , the clinical applicability was limited by the maximum tube current output , particularly in patients with history of bypass aorto - coronary or stenting and with high calcium score due to the beam - hardening artifacts and in obese patients where the disadvantage of decreasing tube voltage is more evident . 
this issue has been overcome with the introduction of ct with higher tube current output ( up to 1300ma ) , which enables the frequently use of low tube voltages in ctca [ 16 ]  . prospective ecgtriggering spiral protocol ( or highpitch protocol ) cardiac imaging must be performed with ecg synchronization , in order to freeze all images in defined time points of the cardiac cycle . 
with the introduction of dsct scanners , prospective ecg - triggering spiral protocol , or highpitch protocol ( php ) , became feasible in addition to the conventional retrospective ecg - gating spiral protocol ( rp ) and to the prospective ecg - gating sequential protocol ( psp ) [ 17 ]  . 
the php yields a snapshot scan of the entire volumetric dataset of the heart within a fraction of a single cardiac cycle , usually during diastole , with very low radiation exposure . 
 in this mode , data are acquired in a spiral fashion , while the table runs with a high pitch ( 3.2 with third - generation 1 3 1026 la radiologia medica ( 2020 ) 125 : 10241039 1 3 la radiologia medica ( 2020 ) 125 : 10241039 1027 dsct , equivalent to a table feed of 737cm / s )  . 
this is possible because a dsct system contains a second x - ray tube at about 90 , which facilitates a maximum pitch of 3.23.4 ; instead , in the single - source ct system the pitch is limited to values of approximately 1.5 to ensure gapless volume coverage along the z - axis [ 18 ]  . 
differently of psp , where additional x - ray exposure is generated at every slice , the php generates superfluous x - rays only at the beginning and at the end of the spiral path and , in contrast to the rp , the x - ray beam is turned on for only a short portion of diastole , and it is turned off during the rest of the rr cycle . 
it is commonly employed with arrhythmia or high heart rhythm , as it leaves more flexibility to choose the portion of the cardiac cycle with the least cardiac motion , or if it needed the functional assessment of the myocardium or the valves . 
due to this slow - pitch application ( usually around 0.2 ) , which enables the acquisition of oversampled datasets that allow interrogation of the entire cardiac anatomy across the rr interval , rp is characterized by high radiation dose , and this explains the reduction of radiation exposure when using the php mode . 
the ed remains frequently below or near at one msv , approximately 1 / 10 of the radiation exposure with the rp and 1 / 2 to 1 / 3 with the psp . 
the main limitations in its use are the presence of high or arrhythmic heart rate given that it is not possible to reconstruct any cardiac phase beyond that acquired [ 19 ]  . tube current modulation tube current is usually modulated during cardiac phase . 
tube current is maximal during the cardiac phase that is expected to yield diagnostic results , and it is reduced during cardiac phases that are not useful for anatomical and morphological evaluation . 
for the faster heart rate , the most suitable phase for reconstruction becomes more difficult to predict and may vary from 30 to 80% and it is necessary to set the full - dose period from 30 to 80% , which increases the likelihood of including the optimal reconstruction phase in the full - dose window , albeit with increased radiation dose . 
ecg - based dose modulation is activated prospectively , according to an automated analysis of the preceding heartbeats ; therefore , a limitation associated with its use is that the exact occurrence of systolic and / or diastolic phases cannot be reliably predicted with arrhythmia or irregular rhythhowever , recent sophisticated algorithms that automatically detect premature contraction of the heart and suspend ecg - based tube current modulation during the scan have overcome this limitation [ 2022 ]  . iterative reconstruction iterative reconstruction ( ir ) algorithm is developed almost two decades ago , and its advantages over traditional filtered back projection ( fbp ) reconstruction have long been recognized . 
when available , the use of ir is recommended because it reduces image noise and significantly improves image quality in terms of snr and cnr compared to routinely used fbp [ 23 ]  . ir algorithms , based on original images , generate new projection data with the use of prior information concerning the scanner geometry , the x - ray spectrum , the detector characteristics and a noise model . 
ir has several advantages and disadvantages [ 24 , 25 ]  . the main advantage is noise reduction , which offers the opportunity to acquire images at lower tube voltage and / or tube current with image quality comparable to routine radiation dose levels . 
however , the advancements in this field have limited the reconstruction time and it is not likely to result in clinically relevant delays , not even in the emergency setting . 
 this is caused by low noise levels and is more pronounced in higher noise reduction settings [ 26 ]  . scan length andheart rate control scan length , or z - axis coverage , represents an important factor for reducing the radiation dose . 
therefore , the region of the carina is frequently used as the upper border and the cardiac apex as the lower border , and the scan length is planned by adding around 1cm to the upper and to the lower border to account for possible changes in 1 3 1028 la radiologia medica ( 2020 ) 125 : 10241039 inspiration depth . 
however , scan length optimization solely based on the scout view may be difficult , as the heart position may vary with diaphragmatic motion , and some patients may have difficulty keeping the same respiratory state for successive acquisitions . 
if a non - contrast calcium - scoring scan is acquired before cct , the landmarks obtained might be used for more exact planning of the scan range [ 27 ]  . in spite of the advances in ct scanner technology , the level of radiation exposure due to the possible use of php and due to the better tube current modulation is still influenced by heart rate . 
it cannot be administered in other rhythms than in sinus rhyththe protocol of administration consists in an oral dose of 7.5mg dose over a 5 - day period prior to ctca or iv administration before ctca [ 28 , 29 ]  . beyond thectca anatomical evaluation not adequately predicts the hemodynamic relevance of coronary stenosis , and increasing efforts aim at determining the functional relevance of lesions by ctca . 
the low radiation dose and the development of ct scanner technology allowed to shift focus from morphological assessment to a comprehensive morphological and functional evaluation , with the introduction of the perfusion ct imaging , fractional flow reserve ( ffr ) - ct , dual - energy ( de ) ct and artificial intelligence ( ai ) [ 30 ]  . 
perfusion ct imaging offers the possibility to directly detect the presence of perfusion defects in the myocardium , during both rest ( baseline ) and stress ( hyperemia ) conditions , using the distribution of contrast medium ( cm ) in the myocardium as a surrogate for myocardial blood flow . 
dynamic datasets acquisition is performed using a single - tube ct scanners with 256 or 320 detector rows , which cover the whole cardiac volume while the table is stationary or secondand third - generation dsct scanners , able to perform dynamic ctp imaging by moving the scanner table back and forth ( shuttle mode ) between two scanning positions . 
in both cases , image acquisition is performed during the systolic phase of the cardiac cycle when apicalbasal length is shorter and myocardial wall is at maximal thickness [ 3134 ]  . 
the ffr represents the ratio of average coronary artery pressure distal to stenosis to the average thoracic aortic pressure measure during highest coronary blood flow and can help determine the hemodynamic significance of coronary artery stenosis . 
ctca and ffr - ct can provide combined anatomic information on coronary artery stenosis and functional significance of coronary lesions without the need for additional image acquisition , radiation burden or administration of contrast agent . 
a physiologic model of the coronary microcirculation is derived from patient - specific data on the basis of three main principles : resting coronary flow is proportional to myocardial mass , microvascular resistance is inversely proportional to vessel size and microvascular resistance is reduced to simulate maximal hyperemia [ 35 , 36 ]  . 
based on the specific attenuation spectral characteristics of the different tissues when exposed to two different photon energy levels , dect enables distinguishing the features of the tissue and evaluating the myocardial blood supply by mapping iodine distribution within the myocardiuiodine map provides a measure of per - voxel iodine myocardial concentration expressed in mg / ml , which improves accuracy when compared to standard visual analysis . 
moreover , a delayed phase dataset in dect can be acquired 8 to 10min after cm injection to evaluate late myocardial enhancement , expression of myocardial fibrosis with the low kev virtual monoenergetic images generated from dect acquisition . 
moreover , dect can provide noninvasive plaque composition analysis , allowing to distinguish between soft and hard plaques , myocardial iron quantification and the calculation of extracellular volume fraction [ 3739 ]  . ai algorithms in ctca can be used for a wide variety of applications , such as image optimization , classification , segmentation , prognosis and outcome prediction . 
for example , by creating labels with a maximum a posteriori probability model , a network can be trained to create clean images out of noisy , reducing the amount of noise in the reconstructed ct images . 
the radiation dose related to a single ctca adds only a small , negligible additional risk to lifetime cancer risk , and the diagnostic information and the clinical consequences resulting outweigh this very small theoretical additional cancer risk . 
this becomes even more evident when the 0.05% estimated risk of fatal malignancy from a 10msv ct scan is compared with the 50% reduction in fatal and non - fatal myocardial reduction observed already 3years after a ctca [ 3 ]  . 
1 67 - year - old male patient with body mass index of 26.4kg / m2 and rhythmic heart rate of 70bpthe figure shows a ctca examination with dual - source ct scanner with prospective ecg - triggered spiral high - pitch ( 3.2 ) protocol at 90 kvp . 
2 52 - year - old female patient with body mass index of 22.5kg / m2 and rhythmic heart rate of 59bpthe figure shows a ctca examination with dual - source ct scanner with prospective ecg - triggered spiral high - pitch ( 3.2 ) protocol at 70 kvp . 
the image quality is excellent third - generation dsct scanner with de technology used in routine clinical setting . materials andmethods in our experience , from the database of our hospital , consecutive patients undergoing ctca with php or psp were retrospectively enrolled to rule out coronary artery disease . 
study populations characteristics are summarized in table2 . all examinations were performed with a third - generation 192 2 slices dsct ( somatom force , siemens healthcare , germany ) scanner with the same contrast medium ( iopamidol , 370mg i / ml , bracco imaging , italy ) , injected from the superficial vein of the right antecubital fossa . an ecg - synchronized scan was performed . 
3 59 - year - old female patient with body mass index of 24.1kg / m2 and rhythmic heart rate of 66bpthe figure shows a ctca examination with dual - source ct scanner with prospective ecg - triggered spiral high - pitch ( 3.2 ) protocol at 80 kvp . 
images a and b show the curved planar reformations , respectively , of the right coronary artery without significant stenosis and of the anterior descending artery with a moderate stenosis ( 40 - 60% ) due to a high attenuation plaque with a positive remodeling ( image b , yellow arrow )  . 
images c and d show , respectively , the volume rendering of the entire heart and the coronary tree isolated from the heart , in which it is illustrated the exact position of the coronary plaque ( yellow arrows ) , that is , at the begin of the third part of the anterior descending artery ( color figure online ) 70bpm ; the psp was used with arrhythmic heart rate or greater than 70bpm . a bolus test technique was used to evaluate cm peak time in the ascending aorta . 
 for analysis , image datasets were transferred to a dedicated workstation equipped with cardiac post - processing software ( syngo.via ct cardiac ; siemens healthcare , germany ) for curved multiplanar and volume rendering reconstructions . 1 3 la radiologia medica ( 2020 ) 125 : 10241039 1033 fig . 
4 78 - year - old male patient with body mass index of 23.5kg / m2 and rhythmic heart rate of 68bpthe figure shows a ctca examination with dual - source ct scanner with prospective ecg - triggered spiral high - pitch ( 3.2 ) protocol at 70 kvp . 
images c and d show , respectively , the volume rendering of the entire heart and the coronary tree isolated from the heart , in which it is illustrated the exact position of the patent stent ( yellow arrows ) ( color figure online ) between two groups were compared sex , age , bmi , heart rate , volume computed tomography dose index ( ctdivol ) , dose length product ( dlp ) and ed , using parametric tests for statistical analysis . 
5 36 - year - old female patient with body mass index of 25.8 kg / m2 and rhythmic heart rate 62 bp the figure shows a ctca examination with dual - source ct scanner with prospective ecgtriggered spiral high - pitch ( 3.2 ) protocol at 80 kvp . 
images a - b - c show the curved planar reformations , respectively , of the right coronary artery , the anterior descending artery and circumflex artery without significant stenosis . 
images d - ef show the volume rendering of the entire heart , respectively , from a superior , inferior and lateral point of view , in which it is possible to evaluate a malignant coronary artery anomaly due to the origin of the right coronary artery from the left coronary sinus with an interarterial course ( image d , yellow arrow ) ( color figure online ) 1 3 la radiologia medica ( 2020 ) 125 : 10241039 1035 1 3 1036 fig . 
6 61 - year - old male patient with body mass index of 31.3kg / m2 and rhythmic heart rate of 65bpthe figure shows a ctca examination with dual - source ct scanner and de technology with prospective ecg - triggered high - pitch ( 3.2 ) protocol at 90 kvp . 
moreover , the reduction of the radiation dose during the routine ctca allowed us to introduce the use of de technology for the study of the myocardium obtaining iodine maps and the evaluation of the late myocardial enhancement . 
figures1 , 2 , 3 , 4 , 5 and 6 show examples of ctca examinations performed with dsct with de technology in our radiology department . other studies reported similar experiences . 
 [ 46 ] , with a third - generation dsct scanner reported an ed reduction of 35.6% for cardiovascular examinations , when they compared it with the previous us of 64 - slice ct scanner . 
 [ 43 ] reported an ed of 0.63msv , despite a high overall proportion of overweight or obese patients . several studies demonstrated the feasible use of 7080 kvp for patients with a bmi < 25kg / m2 , maintaining the diagnostic value and quantitative image quality parameters . 
 however , in daily clinical routine , a considerable amount of la radiologia medica ( 2020 ) 125 : 10241039 overweight or obese patients is observed [ 45 , 48 ]  . 
the possibility to increase the tube current up to 1300 mas allows overcoming or limiting this problem and automatic tube voltage modulation , according to patients size , allows setting the tube voltage in order to obtain the better image quality with the lower radiation dose [ 45 ]  . 
second , radiation dose has a linear relation with mas and so tube current does not have an important role in decreasing patient dose [ 16 ]  . the use of ir can reduce image noise by up to 80% as compared with fbp , and it can improve the image quality with low tube voltage in patients with bmi < 30kg / m2 [ 6 ]  . 
unlike , the use of ir resulted in fewer blooming artifacts and it induces less overestimation of degree of stenosis , especially in heavily calcified vessels and stents [ 25 , 49 ]  . the choice of the correct ecg - synchronized approach , between rp , psp and php is needed in order to obtain the lower radiation dose with the better image quality . 
indeed , several previous studies concluded that the php is most appropriate with a stable sinus rhythm up to 65bpm and image quality decreases above these limits [ 42 , 43 , 5052 ]  . 
however , if with the arrhythmia it is necessary to use a rp rather than a php , the choice of the heart rate threshold beyond which the php causes an image quality reduction deserves a discussion . 
 therefore , the high heart rate , without arrhythmia , does not seem a limit of the php use but it is needed to set the acquisition phase with least motion that is mid - diastolic ( 6075% of the rr interval ) for heart rate 70 bpm and end systolic ( 4045% of the rr interval ) for heart rate > 70bpm [ 54 , 55 ]  . in spite of these considerations , the level of radiation exposure is still influenced by the heart rate control . 
the correct preparation of the patients with the use of - blocker to control patients heart rate is an argument of debate . although the shorter acquisition times have significantly reduced the use of these drugs , the presence of a regular and low heart rate can reduce the radiation dose for two main 1 3 la radiologia medica ( 2020 ) 125 : 10241039 1037 reasons . 
second , with regular and low heart rate is increased the effectiveness of ecg - based tube current modulation [ 5658 ]  . finally , with the improved capabilities of ct systems , there is a general tendency to increase the area of coverage , due to faster acquisition and less limitation of tube power ; instead , it is important to check that the scan acquisition field is correctly set . 
in effect , if the scan is too long , there will be unnecessary radiation delivered to the thyroid gland or to the abdominal organs and , if the scan length is too short , excluding a portion of the coronary artery tree , the repeat scanning will increase cumulative radiation [ 19 ]  . conclusion the combined effects of imaging technology evolution , greater awareness of radiation risk and , at least in europe , changes in legislation forcing laboratories to communicate in writing the dose administered during the examination and the application of the correct technical basis allowed the beginning of the sub - msv era in ctca [ 59 ]  . 
 the single exposure to the individual examination may be negligible , but all doses add up in determining the lifetime radiation exposure , and considering age and gender , more restrictive radiation dose protection criteria should be applied to younger and female patients , and those who received already a significant exposure in the past . 
due to the need of the last generation ct technology and the experience in cardiac ct imaging , there is a large variability in radiation doses between different centers and it might be useful to certify the centers in which ctca can be performed with the lower radiation dose . 
moreover , because anatomical evaluation not adequately predicts the hemodynamic relevance of coronary stenosis , the low dose in routine ctca and the last ct scanner technology will be the main driving forces for the development and the diffusion of the myocardial ct perfusion , ffr - ct , dect and ai that will allow the noninvasive functional assessment of stenosis . in the near future , the ctca will be a one - stop noninvasive imaging modality for both morphological and functional evaluation of coronary stenosis . 
imaging plays a crucial role in the diagnosis and management of this population as a key component of patient care at all stages , especially in those patients who survived into adulthood . 
over the last decades , noninvasive imaging techniques , such as cardiac magnetic resonance ( cmr ) and cardiac computed tomography ( cct ) , progressively increased their clinical relevance , reaching stronger levels of accuracy and indications in the clinical surveillance of chd . 
the current review highlights the main technical aspects and clinical applications of cmr and cct in the setting of congenital cardiovascular abnormalities , aiming to address a state - of - the - art guidance to every physician and cardiac imager not routinely involved in the field . keywords cardiac magnetic resonance congenital heart disease cardiac computed tomography pediatric imaging introduction congenital heart disease ( chd ) is a group of lesions with an incidence of 6 - 8 per 1000 at birth [ 1 ]  . 
therefore , most of these patients currently survive into adulthood , and the number of subjects with congenital heart disease has dramatically increased [ 2 ]  . imaging plays a crucial role in the diagnosis and management of chd , and it is a key component of patient care * aurelio secinaro aurelio.secinaro@opbg.net 1 department ofimaging , advanced cardiovascular imaging unit , bambino ges childrens hospital , irccs , piazza s . 
 onofrio 4 , 00165rome , italy 2 pediatric cardiology andpediatric cardiac surgery department , bambino ges childrens hospital ircss , rome , italy 3 radiology unit , irccs policlinico san donato , sandonatomilanese , italy 4 department ofbiomedical sciences forhealth , universit degli studi di milano , sandonatomilanese , italy 5 radiology unit , irccs istituto giannina gaslini , genoa , italy at all stages [ 35 ]  . 
from the fetal life onward , imaging is a mainstay defining anatomy and physiology of these conditions , helping to refine management , and guiding prognosis . the main imaging techniques in chd are echocardiography ( echo ) , cardiac magnetic resonance ( cmr ) , cardiac computed tomography ( cct ) , and cardiac catheterization . 
 due to its portability , wide availability and noninvasive nature , transthoracic echo remains the first - line imaging technique in chd [ 6 ] , and especially in the neonatal age , it can define diagnosis and guide management by itself [ 7 ]  . 
 however , transthoracic echo may be limited by poor acoustic window , especially in adults , operator - dependency and limited capacity for characterization of extracardiac anatomy [ 5 ]  . 
however , it is invasive and exposes the patient to ionizing radiation , even if it offers the possibility of treatment during the same procedure . over the last decades , noninvasive imaging techniques such as cmr and cct are progressively fulfilling much of the diagnostic role of catheterization [ 8 ]  . 
cmr provides high - resolution imaging of intracardiac and extracardiac anatomy in any imaging plane , giving complete visualization of complex vol . : ( 0123456789 ) 1 3 1168 la radiologia medica ( 2020 ) 125 : 11671185 cardiac anomalies , without the use of ionizing radiation [ 6 , 9 , 10 ]  . 
moreover , it can assess vascular and valvular flow [ 11 ] enabling reliable quantification of intracardiac shunts [ 12 ] , and it is able to measure myocardial function with high reproducibility regardless of ventricular morphology [ 5 ]  . 
thus , imaging these patients requires dedicated cmr staff with expertise in chd and trained to optimize pulse sequences in this setting [ 5 ]  . cct also plays a significant role in patients with chd . 
furthermore , it can represent an alternative for patients where cmr is not suitable because of the presence of cardiac devices . this review focuses on the role of cmr and cct in chd , and it aims to summarize their main clinical indications in this setting . technical aspects ofdifferent imaging techniques cardiovascular magnetic resonance cmr acquisition in patients with chd needs important cooperation , to avoid motion and respiratory artifacts [ 14 ]  . 
a standard cmr protocol in patients with chd is outlined in fig.2. t1 blackblood fast spin echo t1 black - blood fast spin - echo two - dimensional ( 2d ) and three - dimensional ( 3d ) sequences generate images where flowing blood appears dark , while more stationary tissues show various shades of gray depending on signal intensity . 
ef ejection fraction , cemra contrast - enhanced magnetic resonance angiography , qp pulmonary flow , qs systemic flow , pas pulmonary arteries , ssfp steady - state free precession they are used to provide detailed information of cardiothoracic anatomy and are less susceptible to metallic artifacts [ 15 , 16 ]  . ecggated cine imaging qualitative assessment of valvular function [ 17 ]  . 
gradient - echo ( gre ) sequences can be alternatively performed in case of metal artifacts . ecg - gated balanced steady - state free - precession ( ssfp ) cine images , acquired in any plane during breathhold , allow the evaluation of cardiac function and the 1 3 1170 la radiologia medica ( 2020 ) 125 : 11671185 magnetic resonance angiography magnetic resonance angiography ( mra ) is a powerful tool to investigate complex vascular patterns in chd [ 15 ]  . 
 compared to cct and invasive angiography , cmr can produce , with a volumetric acquisition , images of the great vessels without using ionizing radiation , both with and without contrast injection [ 18 ]  . 
asd atrial septal defect , vsd ventricular septal defect , papvr partial anomalous pulmonary venous return , pda patent ductus arteriosus , rv right ventricle , lv left ventricle , ao ascending aorta , mpa main pulmonary artery , pas pulmonary arteries , pvs pulmonary veins , svc superior vena cava , ivc inferior vena cava , cemra contrast - enhanced magnetic resonance angiography , qp pulmonary flow , qs systemic flow , rvot right ventricular outflow tract , gre gradient echo , ssfp steady - state free precession , lge late gadolinium enhancement , pr pulmonary regurgitation , rvol regurgitant volume , rf regurgitant fraction , dao descending aorta , lvot left ventricular outflow tract , sam systolic anterior motion , tr tricuspid regurgitation , av atrio - ventricular is flow independent and requires use of contrast media ( 0.10.2mmol / kg ) with a fast 3d gradient - echo sequence . 
recently , faster k - space data filling algorithms allow to acquire multiple 3d volume sets as contrast agent flows through the vessels , producing a time - resolved mra [ 19 ]  . 
 thanks to the high spatial and contrast resolution , ecgtriggered and respiratory - gated 3d navigated ssfp sequence is helpful to delineate coronary artery origin and pathway as well as great vessel and small collaterals [ 20 ]  . phase contrast accurate quantification of flow is crucial in patients with known or suspected chd . 
for volume quantification , a free - breathing or breath - held velocity - encoded phase - contrast ( pc ) sequence is used , with a temporal resolution of at least 30 frames per cardiac cycle . 
ventricular stroke volume combined with the relative forward arterial flow volume from that ventricle allows for calculation of atrio - ventricular valve regurgitation [ 11 ]  . late gadolinium enhancement late gadolinium enhancement ( lge ) is a useful tool for fibrosis detection , based on differences in the volume of distribution of gadolinium , an extracellular contrast agent . 
lge is also detected when myocardial injury occurs as a complication of chd repair involving coronary artery re - implantation [ 24 , 25 ]  . perfusion andstress imaging myocardial perfusion cmr can be performed at rest and during pharmacological stress . 
indications for perfusion cmr in the pediatric age group include suspected ischemia following surgical transfer of coronary arteries during repair of chd , for instance in arterial switch operation and ross procedure [ 26 ]  . cardiac computed tomography cct in chd patients can be used to investigate complex cardiovascular morphology and function in three dimensions with high spatial resolution [ 27 , 28 ]  . 
cct in chd needs extensive technical knowledge because of technical challenges due to low patient compliance with breath holding , high heart rates , radiation exposure , complex anatomy , circulatory dynamics , and scan timing [ 29 ]  . patient preparation all external metallic objects / devices should be removed from the expected scan region to reduce streak artifacts and potential increased noise when prescribing low - dose parameters . a peripheral intravenous catheter is required for contrast injection . 
the ability to safely administer contrast is directly dependent upon adequate gauge and placement , in particular in newborns . cct acquisition protocol non - contrast scans are usually unnecessary , optimizing and reducing patient radiation exposure [ 29 , 30 ]  . 
aortic flow is obtained using 3 - chamber and coronal left ventricular outflow tract views and positioning the imaging plane at the level of the sino - tubular junction , orthogonal to the vessel long axis ( red lines , panel a ) ; resultant magnitude and phase images used for qs measurement ( panel b ) ; similarly , pulmonary flow is obtained using two orthogonal views of the right ventricular outflow tract ( blue lines , panel c ) , with the resultant phase - contrast images used for qp measurement ( panel d )  . 
alternative flows can be obtained for qs ( superior vena cava svc + inferior vena cava ivc ) and qp ( right pulmonary artery rpa + left pulmonary artery lpa or pulmonary veins pvs ) measurements synchronization should be the method of choice in this setting to reduce radiation exposure . 
however , when irregularly high heart rates are encountered or functional parameters are needed , retrospective ecg - scanning should be used , at the cost of an increased dose [ 31 ]  . postprocessing high - quality post - processing is mandatory for cct in chd due to the complexity of the anatomy . 
curved planar reformations are needed to evaluate vessel lumen and walls . cmr andcct inuncooperative patients in order to improve the image quality of cmr , it is relatively safe to perform the examination in uncooperative patients under ga [ 5 , 32 ]  . while sedation is rarely necessary and only lasts a short period of time for cct , cmr faces many difficulties in this setting . 
the small dimensions of intraand extracardiac structures , the high heart rates , the necessity to perform breath - old sequences may prolong scan time and require a deep adaptation of sequences parameters . 
finally , the risks related to an unfavorable magnetic environment in case of adverse events are not negligible . different strategies can be considered in uncooperative children to avoid ga during cct examinations : feed - andwrap technique in newborns and oral glucose or pacifiers in infants ; physical immobilization devices ( soft weights , restraining bands ) ; parental assistance and or audio / video support in young children . 
in some cases , mild sedation with short - acting benzodiazepines may be performed [ 29 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 11671185 1173 fig . 
balanced ssfp axial and 4 - chamber views showing sinus venosus asd ( arrows , panel a , b ) ; oblique coronal view obtained from cemra demonstrates papvr of right superior and middle lobe veins connected to the svc ( arrowhead , panel c ) ; cine short - axis view depicts severe dilatation of the right ventricle due to left - to - right shunt ( panel d ) ; quantification of pulmonary and systemic flow with through - plane pc sequences ( panel ef ) ; comparison of flow curves reveals significant systemic - to - pulmonary shunt with high qp / qs ratio ( panel g ) main cmr clinical indications selected chds with their specific postoperative common complications , cmr protocol , and key reporting elements are summarized in fig.3. shunt assessment cmr plays a pivotal role in the assessment of both intra and extracardiac shunts , identifying the site of the abnormal communication between cardiac structures or great vessels , quantifying shunt volume and the effects of volume overload on the heart chambers [ 15 , 33 ]  . ostium secundum atrial septal defect ( asd ) is the most common type of asd ( 80% ) localized in the region of fossa ovalis , followed by ostium primum ( 15% ) , also named partial atrio - ventricular septal defect and associated with mitral valve abnormalities , and sinus venosus asd ( 5% ) , frequently combined with partial anomalous pulmonary venous return . ventricular septal defect ( vsd ) is the most common congenital cardiac anomaly in children ( 37% of all chd ) , but in most cases , it may eventually close spontaneously so the incidence is significantly lower in adults [ 34 ]  . 
perimembranous / subaortic vsd is the most common type ( 80% ) , located at the level of membranous septum and sometimes partially covered by accessory tricuspid tissue which reduces shunt volume . 
when restrictive , vsd can generate flow turbulence well recognized as a dephasing jet on ssfp images ( signal void artifact )  . 1 3 1174 la radiologia medica ( 2020 ) 125 : 11671185 fig . 
cine sagittal plane through the rvot during diastole depicts free pulmonary regurgitation ( panel a ) , with eccentric retrograde flow seen on phase image through the mpa ( arrow , panel b ) ; 4 - chamber cine view shows the effect of volume overload on the right ventricle , which is significantly dilated ( panel c ) ; 3d vr reconstruction of the rvot and pulmonary arteries , with acute take - off and narrowing of the lpa origin ( panel d ) ; cine systolic images demonstrate severe rvot obstruction at the level of the pulmonary valve remnant ( panel e ) , with hypertrophic rv and flattening of interventricular septum ( panel f ) ; anomalous origin of the left coronary artery ( lad ) from the right coronary artery , with prepulmonary course ( t1 black - blood fast spin - echo image , panel g ) ; anterior course of lad in close proximity to the pulmonary valve ( arrowhead , panel h ) other vsds are the muscular / trabecular type ( 15% , sited in the muscular septum ) , the inlet type ( 8% , frequently seen in patients with down syndrome ) , and the outlet / infundibular type ( 6% , above the crista supraventricularis , in some cases causing aortic valve prolapse / regurgitation )  . patent ductus arteriosus ( pda ) and partial anomalous pulmonary venous return ( papvr ) are best appreciated with conventional cemra and 3d ssfp mra . 
the most common types of papvr are the aberrant connection of the left upper pulmonary vein to the left innominate vein or of the right upper pulmonary vein to the superior vena cava ( svc )  . shunt assessment requires qp / qs ratio calculation with phase - contrast sequences ( fig.4 ) : the easiest method is acquiring conventional 2d through - plane pc sequences at the level of the ascending aorta ( ao = qs ) and main pulmonary artery ( mpa = qp )  . 
other pc sequences could be acquired to confirm ao and mpa flow volumes : for example , qs corresponds to the flow of superior and inferior vena cava , while qp could be also calculated as the global net flow of the right and left pulmonary arteries or pulmonary veins . normally , at rest , intraand extracardiac communications generate a systemic - to - pulmonary ( left - to - right ) shunt , with pulmonary overflow and qp / qs ratio > 1 . 
evidence of a net left - to - right shunt with qp / qs > 1.5 or leading to significant right chamber dilatation ( fig.5 ) , is considered for intervention [ 35 ]  . cardiac shunts cause atrial and ventricular overload and dilatation : pre - tricuspid shunts ( asd and papvr ) generate rv enlargement , while post - tricuspid shunts ( vsd and pda ) produce left ventricle ( lv ) overload . 
circumferential fibrocalcific ridge at the level of the pulmonary venous baffle causing severe stenosis ( yellow arrows , panel a , b ) ; distal narrowing of the superior caval venous baffle ( arrowhead , panel c ) with associated collateral flow through the dilated azygos vein ( dashed arrows in mip reconstruction obtained from cemra , panel d ) ; through - plane phase image reveals flow reversal in the azygos vein ( dotted arrow , panel e ) ; hypertrophic and dilated systemic right ventricle with tricuspid regurgitation and leftward systolic bowing of the interventricular septum ( cine images , panel f , g ) ; dynamic outflow obstruction of the sub - pulmonic left ventricle with systolic anterior motion of the mitral valve apparatus ( cine 3 - chamber view , panel h ) obstruction and to evaluate the presence of pulmonary regurgitation ( pr ) , a common sequela after surgical correction in repaired tof ( rtof ) [ 36 ]  . 
severe rv dilatation ( rv end diastolic volume > 150160ml / m2 , rv end systolic volume > 85ml / m2 ) and rv / lv systolic dysfunction ( ef < 45% ) are some of the accepted cutoffs for valve replacement , to obtain rv volume normalization without exposing patients to an early prosthetic valve implantation with the risk of rapid valve deterioration [ 38 ]  . 
cmr can also help in selecting the most appropriate strategy between surgical and percutaneous pulmonary valve implantation [ 39 ]  . assessment of branch pulmonary arteries ( pas ) is also mandatory in rtof . 
in case of significant unilateral stenosis , pulmonary flow increases in the contralateral lung ( normal flow ratio between right and left pulmonary arteries rpa / lpa = 55% : 45% ) [ 40 ]  . furthermore , cmr allows the identification of myocardial scar and diffuse fibrosis in rtof , which seem to be related to adverse outcomes including ventricular dysfunction and arrhythmias [ 41 ]  . aortic coarctation aortic coarctation ( coa ) accounts for 58% of all chds [ 5 ]  . 
severe obstruction of the neo - pulmonary root ( arrow ) , with hypertrophic right ventricle ( cine rv 3 - chamber view , panel a ) ; hypoplastic and stretched left pulmonary artery with metallic stent inside ( cine gre image , panel b )  . 
 however , cct may be preferable in this setting [ 45 ]  . cmr is also able to quantify the degree of vascular re - stenosis both with anatomical and flow measurement : a vessel narrowing 50% relative to the aortic diameter measured at the diaphragm or a peak systolic gradient greater than 20mmhg with a diastolic tail is considered for intervention [ 46 ]  . 
moreover , collateral circulation can be visualized with mra and also quantified with pc sequences [ 3 ]  . transposition ofthegreat arteries transposition of the great arteries ( tga ) is the second most common cyanotic chd with an estimated incidence of 1 per 35005000 live births [ 47 ]  . 
atrial and arterial switch operation are the two surgical techniques used to restore a physiological inseries circulatory system [ 48 ]  . cmr is routinely used in patients with tga for periodical postoperative follow - up [ 49 ]  . tga afteratrial switch atrial switch operation ( mustard and senning techniques ) was the first surgical procedure used for correction of tga . 
pulmonary venous return goes from the left atrium to the right atrium through a large atrial septal communication ( panel a ) ; circumferential subendocardial late enhancement consistent with lv endocardial fibroelastosis ( panel b ) ; anastomosis between vascular roots as a part of surgical palliation of hlhs ( cine frame of the outflow tracts , panel c ) ; oblique coronal cine image displays regular morphology and caliber of the superior cavo - pulmonary connection ( arrow ) and extracardiac conduit ( arrowhead , panel d ) ; coronal mip reconstruction confirms tcpc patency and reveals the presence of a major veno - venous collateral from the left innominate vein draining into the superior left pulmonaryvein ( dashed arrows , panel e ) ; congestive hepatopathy with enlargement and reticular enhancement pattern of the liver . 
there is a hypervascular nodule in the right lobe , suspicious for malignancy ( panel f ) parameters to confirm anatomical data ( normal ivc / svc flow ratio in adults = 2 : 1 ) [ 50 ]  . baffle leaks could be difficult to recognize in cine and mra sequences . 
flow analysis with qp / qs calculation is mandatory to exclude an intracardiac shunt that requires further assessment . moreover , dilatation and dysfunction of the systemic right ventricle with tricuspid valve regurgitation are longterm potential complications in patients after atrial switch and should be carefully assessed with cmr . tga afterarterial switch nowadays , arterial switch operation ( aso ) is the treatment of choice in patients with tga , ensuring both physiological and anatomical correction : the great vessels are reconnected to the appropriate ventricular chamber above the level of the sinuses of valsalva , with the pulmonary arteries transposed anteriorly ( lecompte maneuver ) , followed by translocation of the coronary arteries to the neo - aortic root . cmr allows careful evaluation of potential complications following aso ( fig.8 ) , including supravalvular neopulmonary obstruction and branch pas stenosis , neo - aortic root dilatation and valve regurgitation , stenosis / occlusion of re - implanted coronary arteries with consequent inducible ischemia or myocardial infarction [ 4 , 5 , 26 ]  . functional single ventricle heart afterfontan operation functional single ventricle heart represents a broad spectrum of complex chd not amenable to biventricular repair , such as anomalies where only one ventricle is connected to the atria , diseases with an underdeveloped ventricular chamber 1 3 1178 la radiologia medica ( 2020 ) 125 : 11671185 fig . 
 cmr allows identification of major collaterals with angiographic imaging and quantification of systemic - to pulmonary collateral flow with pc sequences , by subtracting the 1 3 la radiologia medica ( 2020 ) 125 : 11671185 1179 fig . 
severe hypoplastic pulmonary trunk with atretic pulmonary valve ( circle ) , and diminutive branch pulmonary arteries ( arrowsaxial mip reconstruction , panel a ) ; major aorto - pulmonary collateral arising from the aortic arch and feeding both lungs ( arrowheadscoronal mip reconstruction , panel b ) ; other mapcas originating from the proximal descending aorta and directed to the left lung ( dotted arrows , mip reconstruction panel c ) , and to the right lung ( dashed arrows , mip reconstruction panel d ) ; 3d vr reconstructions depict the complex vascular anatomy and spatial relationships with the other mediastinal structures , providing useful information for surgical planning ( posterior and anterior coronal views , panel e , f , respectively ) blood flow volume through the branch pulmonary arteries from the total pulmonary venous return [ 55 ]  . also , the complex hemodynamics of tcpc is associated with progressive systemic venous congestion , potentially resulting in extracardiac complications such as chronic liver congestion and cirrhosis , hepatocellular carcinoma , pleural effusion , and lymphatic abnormalities . 
moreover , the relationship between the native pulmonary arteries , the mapcas , and other mediastinal structures , such as the airways and the esophagus , can be offered with targeted segmentation tools and vr reconstructions ( fig.11 ) [ 58 ]  . 
total anomalous pulmonary venous return can lead to rapid death if oxygenated pulmonary venous drainage is obstructed , in which case sectional imaging by cct may be urgently required [ 59 ]  . 1 3 1180 la radiologia medica ( 2020 ) 125 : 11671185 fig . 
high take - off of the right coronary artery ( rca ) above the sino - tubular junction , with an acute angle between the proximal coronary tract and the aortic wall ( dotted arrow , panel a ) associated with a slit - like appearance of the vessel lumen at this level , suspicious for intramural tract ( arrowhead , panel b ) ; normal rounded lumen morphology of the rca downstream ( dashed arrow , panel c ) ; volume rendering reconstructions clearly display the anomalous origin with interarterial course of the rca ( panels d , e ) ; intracavitary view demonstrates the high position of the right coronary ostium ( green arrow ) , above the intercoronary commissure ( blue arrow ) , while the left coronary artery arises from the left aortic sinus ( yellow arrow ) ( panel f ) coronary anomalies congenital anomalies of origin and course entail variation in the number , shape and location of the coronary ostia . 
 in particular , anomalous origin of the left coronary artery from the pulmonary artery ( alcapa ) can cause myocardial ischemia , heart failure and ventricular arrhythmias from the early neonatal period [ 25 ]  . 
a less dramatic but still potentially fatal condition is the inappropriate origin of a coronary artery with interarterial or intramural course ( fig.12 ) , which is particularly dangerous if it involves the left coronary artery [ 60 ]  . 
congenital coronary fistulas are rare and comprise abnormal termination of coronary arteries ( most frequently the right ) into a cardiac chambers or low - pressure vascular structures such as coronary sinus or pulmonary arteries [ 62 ]  . in children with chd , the most common conditions to consider include tof and tga . 
tga has a typical coronary pattern with the left coronary artery arising from the left anterior facing sinus and the right coronary artery originating from the right - posterior facing sinus , but other arrangements with anomalous take - off and abnormal interarterial / intramural course of the coronary vessels are frequently encountered and are associated with significantly increased mortality and higher rate of late cardiac events [ 59 ]  . posttreatment cct investigation cct is valuable in evaluating immediate postoperative complications such as fluid collections including seromas , hematomas , and abscesses but also entities such as pulmonary 1 3 la radiologia medica ( 2020 ) 125 : 11671185 1181 fig . 
oblique sagittal and coronal cct images showing right aortic arch with severe isthmic narrowing ( arrow , panel a , b ) ; associated aberrant left subclavian artery arising from kommerells diverticulum ( arrowhead ) , which is also connected to the ligamentum arteriosus , thus creating a complete vascular ring ( axial cct image and vr reconstruction , panel c , d ) ; tracheal compression and narrowing is well demonstrated with virtual bronchoscopy ( panel e ) and 3d vr reconstruction ( dashed arrow , panel f ) embolism , pneumonia , pleural effusion , pericardial effusion , and pneumothorax . surgical grafts and conduits can be evaluated for thrombosis , occlusion , or aneurysm formation . 
after endovascular treatment with stent placement , cct is better than cmr to define stent patency and degree of neointimal hyperplasia , stent recoil or fracture , and aortic wall injuries ( dissection , rupture , pseudoaneurysm ) [ 66 ]  . in tga following aso , cct is useful in the assessment of coronary artery stenosis at the re - implanted site , stenosis of pulmonary arteries , and neo - aortic root dilatation [ 4 ]  . in addition , cct could be used for detailed anatomical and physiological evaluation when cmr is contraindicated or considered at high risk . 
in this context , cct can be used to calculate ventricular function and volumes in rtof , tga after atrial switch and fontan patients who have contraindications for cmr ( e.g. , mr unsafe implanted pacemakers / defibrillator ) [ 67 , 68 ]  . 
moreover , cct could be indicated when susceptibility artifacts produced by mr - conditional medical devices may void the diagnostic value of cmr study . combined assessment ofvessels andairways extrinsic airway compression has been found frequently in patients with vascular rings ( fig.13 ) , absent pulmonary valve syndrome , and after aortic arch reconstructions compared to other forms of chd [ 69 ]  . 
cct is particularly helpful for complete evaluation 1 3 1182 la radiologia medica ( 2020 ) 125 : 11671185 of pulmonary arterial sling , because it is often accompanied by abnormal configuration of the tracheobronchial tree , tracheobronchomalacia , and other aberrant pulmonary vascular configurations [ 71 ]  . 
in the last two decades , the ccta has evolved into a valuable diagnostic test in todays patient care , changing the official existing guidelines and clinical practice with a pivotal role to exclude significant cad , in the referral of patients to the cath - lab , in the follow - up after coronary revascularization , and finally in the cardiovascular risk stratification . keywords coronary ct angiography coronary artery disease chronic coronary syndrome acute chest pain coronary stent coronary artery bypass graft cardiovascular risk stratification cardiovascular prevention introduction the cardiovascular diseases ( cvd ) are the principal cause of death and health expenditure in western countries , more than all cancers combined and with the coronary artery disease ( cad ) still the leading killer [ 1 ]  . 
the cad is a longterm pathological process characterized by a progressive atherosclerotic plaque accumulation along the wall of the epicardial arteries , whether obstructive or non - obstructive and with a more or less long subclinical phase [ 2 ] , which can be modified by lifestyle adjustments , pharmacological therapies , and invasive interventions aimed to reach disease stabilization or regression . 
the cad is a chronic disease with long and stable periods but most often progressive , even in clinically apparently silent periods and can become unstable at any time , typically due to an acute atherothrombotic event caused by plaque rupture or erosion [ 2 ]  . 
following the recent guidelines of the european society of cardiology ( esc ) , the dynamic nature of the cad results in various clinical presentations , classifiable as acute coronary syndrome ( acs ) or chronic coronary syndrome ( ccs ) [ 2 ]  . 
in general , in stable patients , a high suspicion of cad with a clinical indication to invasive coronary angiography ( ica ) , in order to pursue an invasive treatment , is placed by the pretest probability assessment ( ptp ) of disease based on appropriate clinical risk scores such as the framingham risk score ( frs ) [ 4 ] or the diamond and forrester score modified and updated [ 5 ]  . 
to date , in clinical practice , between one half and two - thirds of elective ica are completed without intervention [ 6 ] , which indicates that current diagnostic strategies for stable patients suspected of having cad may overestimate disease [ 7 ]  . 
since the first ccta multicenter / multivendor studies [ 1114 ] , the common denominator has been its high negative predictive value ( npv ) , identifying the ccta as the only one noninvasive diagnostic method able to rule out significant cad and the consequent need for further tests or revascularization procedures . 
furthermore , its capability to differentiate healthy coronary arteries ( i.e. , free from any atherosclerotic plaques ) from atherosclerotic coronary arteries ( obstructive / non - obstructive ) and to assess the coronary plaque burden [ 15 ] has progressively opened the door to its potential role in the stratification of the cardiovascular risk in the individual patient unlike what is offered by population - based clinical scores . ccta asthefirst test inpatient withstable angina in the last 15 years , many scientific guidelines , statements , or appropriateness criteria have proposed / indicated the diagnostic role of ccta in different clinical scenarios , 1103 proposing this technique initially to support and subsequently to replace secondor higher - level diagnostic tests in the patients diagnostic workflow with suspected cad . 
the assessment of cad by ccta was initially based on the exclusion or confirmation of stenosis using a binary approach ( greater or lesser ) with a significance threshold set at the 50% reduction in the vessel lumen diameter , but subsequently transformed into a multi - grade approach [ 16 , 17 ] with different stenosis values ( 0 , < 25% , 2549% , 5069% , 7089% , 90% ) in order to stratify at best the severity of disease and put stronger indications on further functional tests or treatments procedures [ 16 ]  . 
despite the availability of quantitative analysis sw from several years , the cad assessment by ccta is performed in clinical practice by means of a visual evaluation , which rarely differs from the quantitative analysis of coronary angiography ( qca ) by more than one range of stenosis . 
generally , ccta stenoses < 50% rarely require consideration for revascularization , while intermediate stenoses ( 5069% ) are associated with qca stenosis 70% in 15% of cases ; so , additional assessment of myocardium ischemia may significantly impact patient management . 
anyway , it has been demonstrated that the visual evaluation during ica ( mostly performed in clinical practice in the majority of the cath - labs ) yields higher stenosis degrees compared with qca [ 18 ]  . 
the state - of - art ct scanners ( i.e. , > 64 - row ct ) for optimal ccta allow to evaluate not only the patency / stenosis of the coronary lumen but also an accurate evaluation of all the main plaques characteristics in terms of composition , attenuation pattern , and high - risk features useful to assess the so - called plaque burden ( table1 ) [ 15 ] and with proved prognostic significance [ 10 ]  . 
plaque burden proximal / mid / distal eccentric / concentric focal / segmental non - obstructive / obstructive [ binary * non - calcified ( lipid and fibrous ) / mixed / calcified positive ( outward remodeling ) / negative ( inward remodeling ) homogeneous / heterogeneous / napkin - ring sign ( nrs ) 1 + 2 + 3 + 4 + 5 + 6 + 7 or multi - grade# approach ] binary : < 50% ( non - obstructive ) / 50% ( obstructive ) # multi - grade : < 25% or 2549% ( non - obstructive ) ; 5069% ( intermediate ) ; 7089% or 90% ( obstructive ) plaques features helpful to detect high - risk plaques as well as to assess the prognosis the basis of their density values ( hounsfield units , hu ) such as the low - density core ( < 60hu or even < 30uh ) , considered nowadays an hallmark finding suggestive for unstable plaque , in particular , if associated with other findings as the positive remodeling ( pr ) [ 19 ] and the napkin - ring sign ( nrs ) [ 10 , 20 ]  . 
even if interesting , these quantitative analyses are still time - consuming and strongly influenced by the overlapping hu - values of the different plaque components , with ct - attenuation values still depended by different scan and technical parameters ( scan protocols , slice thickness , kvp , reconstruction algorithms / filters , noise , hu - threshold values ) , by the iodine concentration of the contrast agent administered intravenously and consequent adjacent vessel lumen contrast - enhancement [ 21 ]  . 
 figure2 shows the typical diagnostic workflow and the role of ccta in symptomatic patient at low / intermediate pretest likelihood of cad , underlining the well - recognized limitations of such noninvasive anatomical test in the evaluation of intermediate stenosis ( 6070% ) , in which a functional test is often required . 
the recent 2019 esc guidelines for the diagnosis and management of ccs [ 2 ] as well as the latest update of the national institute for health and care fig . 
2 diagnostic workflow and the clinic role of ccta in symptomatic patient at low / intermediate pretest likelihood of cad ( ats atherosclerosis , cad coronary artery disease , lma left main artery , rfs risk factors , 3vd three - vessel disease ) 1 3 la radiologia medica ( 2020 ) 125 : 11021113 1105 excellence ( nice ) clinical guidelines [ 28 ] put an end to doubts and discussion about the ccta , officially recognizing its diagnostic role in this clinical setting . 
in particular , ccta is nowadays recommended as the initial test for diagnosing cad in symptomatic patients in whom obstructive cad cannot be excluded by clinical assessment alone ( class i ) , with functional imaging for myocardial ischemia recommended if ccta has shown cad of uncertain functional significance or is not diagnostic ( class i )  . 
 differently , ccta is not recommended when extensive coronary calcification [ 15 ] , irregular heart rate , significant obesity , reduced respiratory compliance , or any other conditions make good image quality unlikely ( class iii ) [ 2 ]  . 
to this acknowledgment corresponds a significant limitation of the role of exercise - ecg , now recommended for the evaluation of exercise tolerance , symptoms , arrhythmias , blood pressure response , and event risk in selected patients ( class i ) or as an alternative test to rule - in / rule - out cad when other noninvasive or invasive imaging methods are not available ( class iib ) [ 2 ]  . 
the continuous evolution of ct technology has also recently allowed the development and execution of functional analysis of coronary flow , in a sort of hybrid imaging , through the evaluation derived from ct of the fractional flow reserve ( ffrct ) [ 2931 ] or myocardial perfusion ( ct perfusion , ctp ) [ 32 ] , with the advantage of reducing the false positive ( fp ) test results , mainly in the assessment of the intermediate stenoses ( 5070% ) and thus increasing both the positive predictive value ( ppv ) and specificity [ 33 , 34 ] ( tables2 and 3 )  . 
the rationale behind the assessment of ischemia is given by the fact that although the severity of the stenosis is one of the factors capable of predicting the presence / absence of ischemia , the association between anatomy and ischemia is poor . 
a recent meta - analysis on the diagnostic performance of different invasive and noninvasive cardiac imaging techniques compared to invasive ffr [ 36 ] , considered the reference - standard for the functional assessment of cad [ 37 ] , showed higher specificity and diagnostic accuracy for the ffrct alone or even higher if associated with ccta compared to cardiological ( ica and stress echocardiography ) or nuclear medicine techniques . 
the first realworld experience of ccta with ffrct as gatekeeper to the cath - lab in non - emergent symptomatic patients with intermediate cad [ 38 ] showed that a conclusive ffrct result has obtainable in 98% of patients who had ct scans referred for ffrct testing ( i.e. , very low dropout rate ) and that the implementation of ffrct for clinical decision making may influence the downstream diagnostic workflow . 
the advance - registry has shown that ffrct modifies the treatment recommendation in two - thirds of subjects as compared to ccta alone , is associated with less negative ica , predicts revascularization , and identifies subjects at low - risk of mace [ 39 ]  . 
a recent nxt - trial sub - study [ 40 ] has shown that a ffrct value 0.8 in individuals with stable cad is a strong predictor of long - term clinical outcomes and superior to the anatomical detection of significant stenosis on ccta , while a normal ffrct is associated with favorable clinical outcome and that the ffrct numeric value is an independent predictor of outcomes . 
the presence of gross parietal calcifications or calcified plaques extended circumferentially for more than 180 still constitute today , for the so - called beam - hardening artifacts , a limit of the method and the main cause of overestimation of stenoses [ 15 ]  . 
it has even recently shown that ffrct provides high and superior diagnostic performance compared with ccta alone in patients with high coronary artery calcium scores ( cacs ) [ 41 ] as well as at all levels of cacs [ 42 ]  . 
further analysis from the discover - flow [ 43 ] and the nxt [ 44 ] trials also demonstrated how the analysis and implementation of the ffrct allow a cost reduction of 3032% improving the clinical outcomes ( 1219% less events ) at 1 - year follow - up ( versus ica visual strategy )  . ccta forrisk stratification the ica is not an accurate predictor of the acs . 
most of the mi occur on coronary arteries affected by stenosis < 70% [ 45 ] , while the angiographic severity of stenosis may be inadequate to predict time and location of a subsequent occlusion that will produce a mi [ 46 ]  . 
the clinical risk scores evaluate simply and easily measurable risk factors ( rfs ) variables predicting ( a priori ) the 10 - year risk of cad for a population , dividing arbitrarily subjects into three categories of risk : low ( < 10% ) , intermediate ( 1020% ) and high risk ( > 20% ) [ 4 ]  . 
anyway , these guidelines have never been validated through randomized controlled trials , but their simplicity , low cost , and reasonable prognostic accuracy have made this approach the standard template for prevention . 
in addition , the frs underestimates the variability of the magnitude of atherosclerotic burden between subjects with similar levels / profiles of rfs , presumably related to other known / unknown genetic / environmental factors [ 48 ]  . 
most of the subjects with sudden cardiac death ( scd ) or non - fatal mi do not experience prior chest pain or exertional dyspnea , emphasizing the importance of early detection and treatment of underlying subclinical atherosclerosis ( ats )  . 
more than 75% of all hard - coronary events occur in people misclassified at low / intermediate risk by the traditional rfs - based approach and , consequently , this not offers optimal preventive therapy [ 49 , 50 ] , while others are misclassified as high risk and advised to take drugs that reduce rfs they do not need and remain under medical treatment for the rest of their lives . 
in particular , the current guidelines in primary prevention provide an initial assessment and risk stratification ( rs ) based on the analysis of traditional rfs , followed by goal - directed therapy when necessary [ 51 ]  . 
from histology and intravascular imaging ( intravascular ultrasound , ivus ; optical coherence tomography , oct ) studies , distinct features of vulnerable plaques at higher risk of rupture have been identified [ 54 ] : large plaque volume , large necrotic core , thin fibrous - cap atheroma ( tfca ) , spotty calcification , and pr [ 55 ]  . 
the currently emerging research is focusing on improving coronary rs tools using ccta parameters based on what we learned from invasive imaging [ 56 , 57 ] , given the high correlation described between the histological and ivus / oct plaque features ( tcfa , plaque burden ) more frequently observed in patients with acute mi or acs than stable angina [ 56 ] , with those plaques showing low - attenuation core , pr , and nrs at ccta [ 19 , 57 ]  . 
the technical evolution and the considerable radiation dose reduction ( even < 1msv ) offered by state - of - art ct scanners allow to scan subjects with less restricted inclusion criteria for ccta , with a further compelling application in the field of cad - detection in addition to the role of gatekeeper to ica : the rs of asymptomatic individuals to target / personalize medical therapy to prevent chd . 
the recent 2019 acc / aha guidelines on the primary prevention of cardiovascular disease [ 58 ] state that the assessment of cacs can be indicated ( class ii ) in case of uncertainty about the initiation of preventive interventions ( e.g. , statin therapy ) in patients classified at intermediate risk for cad ( 7.5% to < 20% 10 - year ) or in selected adults at borderline risk ( 5% to < 7.5% 10 - year )  . 
but what if in these patients the cacs was 0 and the ccta documented a non - calcific and non - obstructive plaque ? the guidelines say nothing about it and while they recognize the cacs as a risk modifier in asymptomatic subjects ( class iib ; level b ) , they do not recognize this role to ccta in individuals at borderline or intermediate risk . 
the ccta is the only diagnostic technique able to noninvasively detect the subclinical ats , with the advantage to go beyond the simple luminal stenosis assessment analyzing all other cad features suggestive for high - risk plaque ( hrp ) like the lowdensity non - calcified plaque ( ld - ncp ) , total plaque volume ( tpv ) , spotty calcifications , pr , and the nrs both visually and with semiautomated coronary plaque quantification / characterization analysis [ 59 ]  . 
all these plaques characteristics have been shown to be independent predictors [ 1921 ] as well as the strongest mace predictors , thus suggesting their integration into the coronary rs and intensification of individual preventive measures [ 13 ]  . 
two other recent studies from the nxt trial have shown that differences in plaque volumes and composition may explain the discordance between coronary stenosis severity and ischemia , being the plaque volumes inversely proportional to the ffr irrespective of stenosis severity and with a strong association between stenosis severity , plaque characteristics , ffrct and ffr , suggesting some threshold values of quantitative plaque analysis as predictors of ffr < 0.80 ( ld - ncp volume > 30mm3 , ncp volume > 185mm3 , tpv > 195mm3 , and plaque length > 30mm ) [ 60 ] and that the adding total vessel hrp - volume to stenosis severity improves discrimination of ischemia in ccta performed in patients with stable angina pectoris [ 61 ]  . 
recently , the development and first application of artificial intelligence ( ai ) with an integrated machine - learning ( ml ) ischemia risk score seem to improve the prediction of lesion - specific ischemia by invasive ffr , over stenosis , plaque measures , and pretest likelihood of cad [ 62 ]  . 
summarizing , hrp - features can be easily determined during routine evaluation of ccta and should be included in standardized reports in accordance with the current guideline recommendations [ 17 ] , offering relevant prognostic information , with incremental value in comparison with clinical scores and other imaging modalities ( cacs or myocardial perfusion imaging , mpi )  . 
ccta will have a pivotal role in guiding preventive therapeutic strategies in the next future , encouraging clinicians to careful management of the associated rfs , to intensify the prophylactic treatment , and carefully follow - up patients to prevent future mi . ccta intheemergency department acute chest pain ( acp ) is one of the most common reasons for admission in the emergency department ( ed ) ; initial triage has on one hand to rapidly identify acs for immediate treatment , on the other to identify very low - risk patients that can be safely discharged . 
however , clinical presentation , common rfs , and risk scores are not sufficient , and the mace rate of very low - risk patients is about 2% [ 63 ]  . 
consequently , noninvasive tests are mandatory : the introduction of high - sensitive troponins ( hs - tn ) sampling deeply modified and accelerated patients triage , increasing sensitivity ; nevertheless , the specificity of a mild troponins increase is not so high , and in this scenario , ccta can play a significant role , because of its wellknown high npv . 
the first trial was the romicat [ 67 ] , whose results were published in 2009 ; 368 patients with acp , normal serum markers , and negative or non - conclusive ecg underwent 1 3 1108 la radiologia medica ( 2020 ) 125 : 11021113 ccta : 50% of patients showed normal coronary arteries , 31% non - obstructive cad and 19% showed non - conclusive results or obstructive cad . 
in 2011 , the ct - stat trial [ 68 ] was the first published multicenter randomized trial comparing ccta or mpi and soc triage , in 699 patients , having as primary and secondary endpoints efficacy and safety and costs , respectively . 
primary endpoint was safety at 30days , while secondary endpoints were length of stay in ed ( lower in ccta group ) and direct discharge ( increased in ccta group )  . 
hospitalization length was lower and discharge rate higher in the ccta group , without differences in the outcome at 28days , but with increase in downstream exams and no costs reduction in the ccta group . 
however , not all randomized clinical trials demonstrated similar results in terms of better outcome ; on the other hand , quite all trials showed decreased length of stay in ed , decreased admission rates , and reduced costs in the ccta groups . 
in 2015 , the prospect trial [ 72 ] compared ccta and stress - mpi in 400 patients , randomized 1 : 1 , having as primary endpoint the selection of patients to invasive management within 1year . 
this trial did not demonstrate any significant statistical difference between the two arms , neither for the primary endpoint , nor for the secondary one ( length of stay , costs , clinical events )  . 
in terms of outcome , the catch trial ( median follow - up 18.7months ) [ 73 ] , demonstrated that a ccta - guided treatment strategy improves clinical outcome in patients with recent acp and normal ecg and troponin values compared to soc with a functional test ( mpi , myocardial perfusion imaging )  . 
the beacon trial , published in 2016 [ 75 ] , was the first one that compared ccta and soc ( including stress - ecg or mpi or direct discharge ) with hs - tn available in both arms ( total population 500 patients )  . 
no significant differences were found in terms of primary endpoint ( revascularization rate ) , and secondary endpoints as readmission to ed or mace , while costs and further testing rate were reduced in the ccta arhowever , further trials are needed to evaluate the impact of the association of hs - tn and ccta in outcome evaluation . 
we can conclude that nowadays the triage in ed is based on hs - tn and in case of high clinical suspicion in patients with mildly elevated values and low to intermediate risk , ccta should be performed . ccta postcoronary revascularization timing of follow - up of revascularized patients has been object of debate for a long time . 
3 ccta in patient with acp : 3d vr a and curved mpr b well show non - calcified plaques in proximal and mid lad with pr ( bd ) , suggesting for vulnerable plaques ( acp acute chest pain , lad left anterior descending artery , mpr multiplanar reconstruction , 3d vr three - dimensional volume rendering , pr positive remodeling ) 1 3 la radiologia medica ( 2020 ) 125 : 11021113 1109 fig . 
3d vr c , curved de and stretched f mpr in mid - distal occlusion of lad stent with hypodensity of the lumen , absent run - off proximal to the distal edge of the stent ( arrowhead in df ) , and thin enhancement of distal lad ( arrow in df ) due to collaterals ( mpr multiplanar reconstruction , lma left main artery , lad left anterior descending artery , 3d vr three - dimensional volume rendering ) ( c ) no indications exist for lower temporal intervals . in case of coronary stent , the major limitation for the assessment of in - stent restenosis ( isr ) is represented by the blooming artifact , caused by the high density stent structure that obscures the stent lumen ; possible solution is the use of high convolution reconstruction algorithms ; however , the final result depends on stent material and thickness of stent strut ( better if 100 m ) and works better in case of higher diameter of the stent ( > 3mm ) [ 76 ]  . 
other factors limiting stent imaging are bifurcation stenting and elevated heart rate ; in the last case , the use of scanners > 64 slices and or higher temporal resolution can improve accuracy . in case of cabgs , ccta is able to clearly depict the patency or occlusion of the graft ( fig.5 ) , the origin or its anastomosis on the ascending aorta , the body of the graft , 1 3 1110 la radiologia medica ( 2020 ) 125 : 11021113 fig . 
5 3d vr ac and curved mpr df in multiple ( 5 ) cabgs : patent lima to lad , patent rima to ri with a retro - aortic course , patent svg to right - pl branch with a sequential anastomosis on om branch ( arrow in b ) , and 2 svg occluded at the proximal anastomosis on ascending thoracic aorta ( arrowheads in a ) ( 3d vr three - dimensional volume rendering ; mpr multiplanar reconstruction ; lsa left subclavian artery ; lima left internal mammary artery ; lad left anterior descending artery ; rca right coronary artery ; rima right internal mammary artery ; ao aorta ; svg saphenous vein graft , ri ramus intermedius ; om obtuse marginal branch ; pl posterior - lateral branch ) and the anastomosis to native coronary artery [ 77 ] ; furthermore , native coronaries distal to grafts have to be assessed . 
 ccta in cabgs assessment is robust and effective , as demonstrated by many studies , without significant differences between 64 - slice scanners and > 64 slice ones [ 78 ]  . going beyond current appropriateness criteria , ccta in cabgs could be applied also : in asymptomatic patients with a positive stress - test ; in patients with atypical chest pain and inconclusive stress - tests ; in preoperative planning for redo cardiac surgery ( lima / rima insitu graft course ; rv anatomy )  . 1 3 la radiologia medica ( 2020 ) 125 : 11021113 1111 conclusions world of cardiac imaging is proposing to physicians an everincreasing spectrum of options and tools with the disadvantages of patients presently submitted to multiple , sequential , time - consuming , and costly diagnostic procedures and tests , sometimes with contradicting results . 
many studies investigate the potential role of ai to support cardiac radiologist in their day - to - day tasks , assisting in segmentation , quantification , and reporting tasks . 
since these algorithms will play an important role in the field of cardiac radiology , it is increasingly important for radiologists to be familiar with the potential applications of ai . 
the main focus of this article is to provide an overview of cardiac - related ai applications for ct and mri studies , as well as non - imaging - based applications for reporting and image optimization . keywords cardiac imaging artificial intelligence computed tomography magnetic resonance imaging introduction the concept of artificial intelligence ( ai ) has first been mentioned in the 1950s [ 1 , 2 ]  . 
along with these technological developments , there has been a significant increase in attention to ai research and development by government , academic , and private sectors resulting in an increase in investment of resources [ 37 ]  . 
the clinical acceptance and recommendations for the standardized use of coronary computed tomography angiography ( ccta ) , calcium scoring , and interest in screening programs [ 814 ] are expected to further increase the number of cardiac examinations . 
this increased workload puts a heavy demand on the radiologist , where studies estimate that an average radiologist may have to interpret up to one image every 34s over an 8 - h workday [ 15 , 16 ]  . current cardiac ai applications are mostly designed to be integrated in the current radiology workflow , with the main goal being to assist radiologists with routine tasks , reducing workload , and increasing efficiency of patient care . 
dependent on the application , human support or supervision is needed [ 17 ]  . this article will provide an overview of cardiac - related ai applications for analysis of ct and mri images , as well as some general applications for reporting and image optimization . 
1 simplified schematic overview of the radiology workflow where ai applications offer assistance overview of the status of ai in the field of cardiac imaging in order to pave the road to clinical implementation of these applications . basic ai principles to optimally understand the function of ai applications , some basic knowledge of the core pillars of ai is highly desired . 
the core ingredients of ai are computing resources and infrastructure , data , and algorithms . computing resources andinfrastructure the amount of computational power available for ai development and training has doubled every 3.4months since 2012 [ 18 ]  . 
the development of the field of ai has been made possible by the availability of faster cpus , the use of graphics processing units ( gpu ) , and overall better software infrastructure for distributed computing . 
in addition , when on - site computing power is not available , cloud computing services are now available for off - site training . data in order to create clinically relevant ai algorithms , it is essential to have access to large datasets . 
the ideal dataset should include data from all manufacturers , scanner systems , and clinical settings ( e.g. , hospitals and outpatient imaging centers ) and be a good representation of the clinical population to allow for generalization over multiple centers , cities , and countries . 
the training dataset is used to learn the parameters of the algorithm and form the general structure of the algorithafter training the algorithm , the validation set is used to optimize the learning behavior of the algoriththe test set is used to evaluate the performance of the optimized algorithoften only a training and test set is used , where 7080% is used for model training ( training and validation set combined ) and 2030% is used for performance evaluation . 
it is essential that the test set is independent of the data used for training and validation without overlapping observations [ 19 ]  . algorithms a term commonly used in ai - related research is machine learning ( ml ) , which refers to the ability of machines to learn . 
for a more elaborate overview of ai algorithms , tasks , and development , we refer to the following review paper [ 20 ]  . 1 3 1188 la radiologia medica ( 2020 ) 125 : 11861199 nonimaging applications reporting workflow andimage reconstruction several ai algorithms have been developed with the main goal of optimizing image quality and reconstruction . 
in these algorithms , a diagnostic - quality or clean data sample is the desired output , while a corrupted data sample is given as input . image reconstruction applications utilizing ai can optimize image quality from images taken with lower quality settings ( e.g. , a low - dose ct acquisition )  . 
trained a generator convolutional neural network ( cnn ) to make image quality from low - dose ct images nearly equivalent to those of regular dose ct images with the use of an anthropomorphic phantom , noncontrast cardiac ct images taken at 20% and 100% of normal radiation dose [ 21 ]  . 
 their study confirms that their ai approach performs either better or comparably in terms of noise suppression and structural fidelity and is much faster than commercial iterative reconstruction algorithms [ 22 ]  . for cardiac magnetic resonance imaging ( mri ) , these algorithms mainly focus on the reconstruction of undersampled images and the detection of corrupted or incorrectly segmented data . 
their algorithm performs heart coverage estimation , inter - slice motion detection , and image contrast estimation in the cardiac region , which are all aspects important for quality control . 
this will allow timely exclusion of these scans and can trigger the need for a new acquisition within the same examination [ 25 ]  . with increasing imaging volumes and complexity , there is a significant clinical interest optimizing the reporting process in order to improve workflow efficiency . 
thus , it reduces time spent on reporting . considering the increasing numbers of ccta , and the high pretest probability showing that prevalence of coronary artery disease ( cad ) is extremely low [ 2628 ] , this will result in a huge number of could be negative for ccta images for cad evaluation . 
for this purpose , the coronary artery disease - reporting and data system ( cad - rads ) was developed by the society of cardiovascular computed tomography ( scct ) , the american college of radiology ( acr ) , and the north american society for cardiovascular imaging ( nasci ) in 2016 . 
cadrads has been endorsed by the american college of cardiology ( acc ) [ 29 ]  . therefore , in the next future , we see and expect a further focus of ai application to optimize reporting and reduce time needed for this process . accordingly , research and development of ai applications aimed at optimizing cad - rads reporting have been published . 
developed a deep learning - based ai algorithm allowing to discriminate patients without cad ( cad - rads 0 ) and patients with cad ( cad - rads > 0 ) in 1.40mresults show an excellent performance with a sensitivity , specificity , negative predictive value , positive predictive value , accuracy , and area under curve of 66% , 91% , 92% , 63% , 86% , 89% [ 30 ]  . 
therefore , the authors speculate that in the future , this approach could be helpful in clinical practice allowing preselect ccta acquisitions that need to be reported in detail for positive cad findings [ 30 ]  . imaging applications calcium scoring coronary artery calcium ( cac ) scoring is a robust technique for cad identification and risk stratification and is considered as an independent predictor of adverse cardiovascular events [ 3136 ]  . 
semiautomatic segmentation and 1 3 la radiologia medica ( 2020 ) 125 : 11861199 1189 quantification of agatston scores , calcium volume , and mass are a time - consuming process , but automatic quantification is not always accurate and reproducible [ 38 ]  . 
in total , the cac scoring process is often a time - consuming process , making it an ideal candidate for time - saving ai applications . excellent results were reported in the study performed by sandstedt etal . 
describing the application of ai - based automatic calcium score evaluation on non - contrast ct images , compared to semiautomatic software as references in 315 patients [ 39 ]  . 
after a calcium score was calculated , 93.4% of patients were classified into the correct risk category [ 41 ]  . calcium score may be also used as an initial step for cad distribution . 
sensitivity and a specificity of 100% and 69.8% were reported , while the npv and ppv were 100% and 38% , respectively . although previous studies used dedicated calcium scoring scans , with the increasing numbers of non - gated chest ct for lung cancer screening , several studies have shown the feasibility of cac scoring in non - cardiac scans as well . 
applied a machine learning approach that identified coronary calcifications and calculated the agatston score using a supervised pattern recognition system with k - nearest neighbor and support vector machine classifiers in low - dose , non - contrast enhanced , non - ecg - gated chest ct within a lung cancer screening progratheir results show that their fully automated cac scoring algorithm was able to perform cac scoring in non - gated chest cts with acceptable reliability and agreement . 
however , the absolute calcium volume was underestimated when compared to dedicated ecg - triggered cac score acquisitions [ 43 ]  . additionally , calcium score quantification can be performed on coronary ct angiography ( ccta ) images using ai algorithms . 
the first step was to create a bounding box algorithm employing a combination of three cnns , each detecting the heart in a different orthogonal plane ( axial , sagittal , coronal ) on a training dataset of 50 patients . 
the study included 7240 participants who underwent various types of non - enhanced cardiac / chest ct examinations including cac scoring ct , pet attenuation correction ct , radiation therapy treatment planning ct , and low - dose and standard - dose ct of the chest . 
this study indicates that ai algorithms can assist in the quantification of coronary calcium in a clinical setting using a wide variety of ct acquisitions , proving its clinical potential . ccta stenosis degree andplaque morphology the role of ccta in the evaluation of coronary stenosis has been extensively investigated both quantitatively and functionally [ 4650 ]  . 
the analysis of ccta scans for manifestations of coronary artery disease allows excellent visualization of the coronary arteries with high spatial resolution , but nevertheless , its analysis can also be time - consuming and susceptible to inter - observer variability . the recent development of ai - based algorithms in cardiac applications , including plaque characterization , may accelerate the clinical implementation of quantitative automated imaging technology aiding the diagnosis and prognosis of cad . the management of patient with cad may differ based on plaque morphology and percent stenosis . 
 1 3 1190 la radiologia medica ( 2020 ) 125 : 11861199 used a 3d convolutional neural network to extract coronary artery features by using 98 patients for the training and 65 patients for the validation sets [ 51 ]  . 
 in a study by hell etal . , they utilized an ai - based software ( autoplaq ) to derive the contrast density difference ( cdd ) , defined as the maximum percent difference of contrast densities within an individual lesion to help predict the hemodynamic relevance of a given coronary artery lesion [ 55 ]  . 
they found that cdd was significantly increased in hemodynamically relevant lesions and could predict hemodynamical significance of the lesions with a specificity of 75% and negative predictive value of 73% when compared to invasive ffr . 
using the same software , another group used imaging features provided to a logitboost algorithm to generate an integrated ischemia risk score to predict hemodynamic significance of coronary stenoses [ 56 ]  . 
their approach resulted in higher auc ( 0.84 ) compared to manual ccta analysis of individual features . another approach for the evaluation of stenosis significance was shown by van hamersvelt etal . 
this finding is interesting because it changes the paradigm of ischemia detection based on anatomical evaluation of coronaries using a rest ccta acquisition . currently , several vendors are developing ai - based software package for comprehensive cardiac ct evaluation , including cac scoring and stenosis evaluation , see fig.2. 
 although vendor specific , these packages offer workflow integrated options for fully automated quantitative analysis . ctffr invasive fractional flow reserve ( ffr ) performed during invasive coronary angiography is considered the reference standard for assessing the hemodynamic significance of coronary lesions . 
initial results of ct - ffrml were described in the retrospective multicenter machine registry study , where a machine learning approach was performed on 525 vessels from 5 sites in the usa , europe , and asia . 
 [ 63 ] compared ct - ffrml to coronary ct angiography and quantitative coronary angiography ( qca ) , showing a per - lesion sensitivity and specificity of 79% and 94% , respectively . 
2 comprehensive ai analysis of cardiac ct images including coronary calcium scoring ( left ) , and automatic quantitative stenosis ( right top and bottom ) analysis using ai software from siemens healthineers in addition , a change in the proposed therapeutic management was seen in 167 patients ( 14.9% ) after ct - ffrml results , concluding that ct - ffrml may guide therapeutic decision - making and potentially improving the utilization of ica [ 68 ]  . 
from a per - vessel analysis , auc was significantly greater for ct - ffr than for ccta stenosis 50% or 70% [ 69 ]  . combining ct - ffr with machine learning provides anatomical and functional information that may increase diagnostic accuracy for hemodynamically significant stenoses and cad severity in a single noninvasive test . 
it should be mentioned that ai - based ct - ffr is currently only used as prototypes in a research setting and is mostly vendor specific , hampering widespread use . 
the use of a local software solution allows for user - variation and can influence per center accuracy , depending on user experience . besides quantification and automatization tasks , ai can also play a role in the prognostication of cardiovascular outcomes fig . 
the left ccta image shows a lad lesion corresponding to a significant drop in ct - ffr ( 0.54 ) a machine learning approach may also guide therapeutic decision - making and correlate with patient outcomes . 
 [ 70 ] evaluated an ai - based approach for prognostication in a large population consisting of 10 , 030 patients with suspected cad who underwent ccta imaging and 5 - year follow - up , with mortality as a main outcome of interest . 
their ai - based prediction method showed higher auc ( 0.79 ) compared to the framingham risk score ( 0.61 ) or ccta severity scores alone ( 0.620.64 ) in the prediction of 5 - year mortality rate . 
 [ 71 ] used the multicenter confirm registry , which included 8844 patients with complete ccta risk score information and at least 3 - year follow - up for myocardial infarction and death . 
cine images are considered fundamental sequences in cmr and allow evaluation of wall motion abnormalities , myocardial thickness , and ventricular volumes [ 73 , 74 , 77 , 78 ]  . 
there has been significant development in semi - automated and fully automated methods for analyzing cine cmr images [ 8287 ]  . in order to choose the best ai approach for automatic segmentation , several recent competitions have been conducted [ 88 ]  . 
for example , during the automatic cardiac diagnosis challenge ( acdc ) that took place during the 20th international conference on medical image computing and computer assisted intervention ( miccai ) , isensee etal . 
however , they also mention that although the results obtained on the lv are competitive , the results for the right ventricle and the myocardium are still sub - optimal [ 88 ]  . despite the high accuracy of the methods tested during the miccai competitions , one of the major limitations is represented by the small sample size used for training of segmentation networks [ 88 ]  . 
 these authors demonstrated high dice coefficients for the left ventricle cavity ( 0.94 ) , left ventricular myocardium ( 0.88 ) , and right ventricle ( 0.90 ) [ 90 ]  . 
showed that a cnn , depending on dataset heterogeneity , is able to quantify lv function parameters with high accuracy compared to experts with a correlation of 0.98 and an average perpendicular distance of approximately 1mm , which was comparable to intraand inter - observer variability [ 91 ]  . 
during recent years , tissue characterization with cardiac mri was strictly confined to t1 or t2 black blood images and late gadolinium enhancement ( lge ) sequences [ 9599 ]  . 
t1 black blood ( t1bb ) images are useful for tissue characterization of cardiac masses and evaluation of myocardial fibrofatty infiltration or replacement [ 100 , 101 ] , while t2 black blood ( t2bb ) sequences are more often used for depiction of water content in cardiac masses or damaged myocardium [ 101 , 102 ]  . 
the only significant difference between the manual ( b ) and ai segmentation ( a ) was the presence of hinge points images are acquired 1015min after the administration of gadolinium - based contrast material [ 103 , 104 ]  . 
the latter reflects a slow accumulation of gadolinium contrast agent in the damaged tissues and could be the expression of replacement fibrosis [ 105 ]  . despite the clinical adaptation of t1bb and t2bb sequences , these sequences are becoming less used . 
increased values of native t1 mapping can reflect an increase in extracellular space ( amyloidosis , acute inflammation , replacement fibrosis ) , while decreases in native t1 mapping values are associated with myocardial diseases such as fabrys disease or iron overload [ 108 ]  . 
conversely , increased values of t2 mapping are extremely specific and sensitive for edema [ 109 ]  . in some specific cardiomyopathies , the quantification of lge could play a key role in determining their prognosis [ 110 ] ; therefore , a correct quantification could be fundamental . 
several strategies have been developed for accurate lge quantification ; however , all currently used strategies require manual segmentation and consequently a time - consuming approach . the application of ai for tissue characterization is mainly focused on reducing the time of analysis and improving quantitation by optimizing the image acquisition and reducing artifacts [ 111115 ]  . 
the authors compared the results obtained from ai with manual segmentation , and they found a dice similarity coefficient ( dsc ) of 0.94 [ 116 ] , confirming that a 3d cnn approach and manual segmentation provide similar results [ 116 ]  . 
the possibility to obtain lge images from non - contrast cine images could represent a cornerstone in the future of myocardial tissue characterization without the use of a gadolinium - based contrast agent . besides lge in the left ventricle , another interesting application of ai is left atrial scar tissue segmentation [ 118 , 1 3 1194 la radiologia medica ( 2020 ) 125 : 11861199 119 ]  . 
the association of left atrium scar and the development of atrial fibrillation is well described [ 120 ] , and therefore , the possibility to have an improved segmentation using ai may be useful in certain clinical scenarios . 
 the authors found that using a gray - level non - uniformity ( glevnonu ) architecture , it was possible to distinguish patients with hcm from normal patients with a sensitivity and specificity of 94% and 90% , respectively [ 111 ]  . 
considering that the ai algorithm would be biased by the presence of lge , the authors combined their ai algorithm with textural analysis , showing increased sensitivity and specificity of 100% and 90% for identification of hcm , being able to capture even subtle myocardial changes [ 111 ]  . prognosis cardiac mri plays a fundamental role in the management of some cardiomyopathies [ 110 , 121 ]  . 
evaluation of tissue characterization analysis combined with ventricular function can be used for the prediction and risk stratification of patients at risk of death and sudden cardiac events [ 121 , 122 ]  . 
they showed that the right atrial median area and right ventricular long axis strain were accurate predictors of outcome [ 127 ]  . beyond the classic imaging data useful for prognostication and risk stratification , the use of ai algorithms shows promise in providing a prognostic evaluation for myocardial diseases . future directions as many times before , the field of cardiothoracic imaging is again faced with new technological developments that have the potential to fundamentally change the field . 
with the increased imaging volumes and new insight into quantitative biomarkers , ai offers the possibility to improve radiology workflow , providing pre - readings for the detection of abnormalities , accurate quantifications , and prognostication . 
 however , it should be noted that many of the applications described above are currently only being used in a research setting and are still far from being implemented into standard care . 
as a result of the fast - developing ai technology , most algorithms are developed and validated by only one group before they move on to a new and improved ai approach . 
the first will use transfer learning , where the algorithm will be developed and trained on a specific dataset and then distributed to other centers where the algorithm can be trained further and be refined to optimize accuracy for that specific population . 
this approach will be especially convenient for situations where the differences in population are large , or when data sharing , due to , for example , privacy reasons , is difficult . 
this will allow for the development of more accurate , generalizable algorithms . however , for ai to truly play a role in the daily clinical practice of the cardiothoracic imaging community , several issues require attention . 
first , ai applications will need to be tested and validated in a clinical setting , while assessing the true efficiency and accuracy in clinical workflows and a representative population . 
the medical and ai communities are currently working together to optimize the legal framework for clinical ai applications . currently , in the usa , supporting ai applications that only assist in quantitative analysis tasks are covered by the u.s. 
however , if an ai application is used for clinical interpretation of radiological images , it will require fda pre - market approval ( pma ) , which requires 1 3 la radiologia medica ( 2020 ) 125 : 11861199 1195 extensive proof of accuracy and safety from clinical trials . 
 the european commissions white paper on medical ai , published in february 20 [ 20 , 130 ] , understated that current eu regulations already provide a high level of protection through medical device laws and data protection laws . 
 additionally , the eu commission for medical ai proposes to add specific regulations aimed for medical ai applications that include requirements on training data , record - keeping of used datasets , transparency , robustness and accuracy , and human oversight . additionally , there are some ethical considerations such as discrimination issues along the lines of race or economical groups due to disparities in the training populations . 
a statement of the joint european and north american multisociety task force discusses this in detail , emphasizing that more research is needed to investigate how to implement ai optimally in clinical practice [ 131 ]  . conclusion in summary , ai is being increasingly used for cardiac radiological applications . 
while ct is on the forefront of these developments , mostly due to the rapidly increasing number of ccta and calcium scoring examinations , cardiac mri is rapidly following , with its main focus on segmentation and functional analysis . 
the future steps of cardiac ai applications should focus on clinical implementation by assessing clinical accuracy in relevant representative populations , cost - effectiveness , and clinical efficiency in reducing time . 
 cardiac imagers , together with ai specialists , are responsible for creating the optimal framework for the next steps of ai implementation , ensuring the optimal use of ai leading to optimal clinical workflows that benefit both radiologists and patients . compliance with ethical standards conflict of interest de cecco receives institutional research funding from siemens healthineers . 
all recommendations were collected in a dataset , including the class of recommendation , the level of evidence ( loe ) , the specific imaging technique , the clinical purpose of the recommendation and the recommending society . 
among the 43 included guidelines ( esc : n = 18 , acc / aha : n = 25 ) , 26 ( 60.4% ) contained recommendations for ct scan or mri ( 146 recommendations : 62 for ct and 84 for mri )  . 
the use of cardiac ct and cardiac mr in the risk assessment , diagnosis , therapeutic and procedural planning is in continuous development , driven by an increasing need to evolve toward an imaging - guided precision medicine , combined with cost - effectiveness and healthcare sustainability . 
these developments must be accompanied by an increased availability of high - performance scanners in healthcare facilities and should emphasize the need of increasing the number of radiologists fully trained in cardiac imaging . keywords aha / acc guidelines esc guidelines cardiovascular magnetic resonance cardiac computed tomography angiography introduction non - invasive cardiovascular imaging with computed tomography ( ct ) and magnetic resonance imaging ( mri ) has become integral part of the clinical routine , following the extraordinary technical evolution of the last 1015years . along with molecular and genomic studies , the recognized importance of cardiac imaging in early disease phenotyping , risk stratification and therapeutic guidance has brought to the development of an imaging - targeted precision medicine , which aims to change paradigms in various cardiological settings . a crucial step of the process has been the translation of the clinical - radiological evidences into practice guidelines which allow to improve the value ( quality and cost - effectiveness ) of healthcare [ 1 , 2 ]  . 
a full list of included guidelines along with the number of recommendations made in each document are reported in table1 . all recommendations were collected in a dataset , including the class of recommendation , the level of vidence ( loe ) ( table2 ) , the specific imaging technique , the clinical purpose of the recommendation and the recommending society . 
 as a systematic review of all esc and acc / aha clinical guidelines is beyond the scope of this report , some equally important cardiovascular imaging fields including vascular studies were not included in the search . when the same recommendation was reported in more than one guideline from the same society , only the most recent was included . 
namely , research was expanded to consensus reports to comprehensively include the most relevant applications without formal recommendation ( paragraph 4 )  . the current landscape ofclinical cardiovascular guidelines of the 43 included guidelines ( esc : n = 18 , acc / aha : n = 25 ) , 26 ( 60.4% ) contained recommendations regarding the clinical use of ct or mri imaging ( table1 )  . 
 scope oftherecommendation diagnosis was the most common clinical purpose of imaging recommendations ( 61.0% ) , for both ct ( 61.3% ) 1 3 1016 la radiologia medica ( 2020 ) 125 : 10131023 table 2 summary of predefined scales regarding " classes of recommendations " and " level of evidence " as adopted by the esc guidelines . 
 only minor differences exist in the definitions of predefined scales adopted by the acc / aha guidelines classes of recommendations levels of evidence evidence that the procedure is clinically useful conflicting evidence that the procedure is clinically useful class i class ii class iia weight of evidence in favor of efficacy class iib class iii efficacy less well established evidence that the procedure is not clinically useful level a data from multiple rcts or meta - analysis level b data from a single rct or large non - randomized studies level c expert consensus , data from small non - randomized studies fig . 
all the recommendations have been divided between the recommending society , and then both esc and aha / acc recommendations have been classified among imaging technique ( ct and mri ) and clinical purpose of the recommendation ( light green boxes ) and mri ( 60.7% ) , in both esc and acc / aha guidelines . 
pie charts on the left show the clear prevalence of recommendations rates of contrast - enhanced cardiac / coronary ct angiography among the other ct techniques in both esc and acc / aha guidelines . 
over mri techniques ( pie charts on the right ) , contrast - enhanced cmr is the most represented among recommendations , followed by stress cmr with similar rate fig . 
rates of recommendations for ct and mri divided by clinical category , represented by pie charts , show the predominance of ischemic heart disease among all of the others , with similar patterns between esc and acc / aha guidelines recommendations bottom line : specific settings ofclinical use primary prevention current recommendations in this setting concern 1 3 1018 la radiologia medica ( 2020 ) 125 : 10131023 fig . 
scope of the recommendation , illustrated by pie charts , defines ct and mri as crucial tools in the initial clinical workup of patients , for both diagnosis and risk stratification . 
of notice , a single recommendation is addressed to preprocedural planning , highlighting a huge gap between guidelines and clinical practice detection of subclinical coronary atherosclerosis and detection of obstructive / ischemia - causing coronary atherosclerosis among at risk asymptomatic individuals . regarding the former goal , coronary artery calcium ( cac ) is a highly specific marker of atherosclerotic burden [ 5 ] , able to improve atherosclerotic cardiovascular disease event prediction among asymptomatic individuals over traditional risk factors [ 69 ]  . 
the approach of esc and acc / aha guidelines to cac score diverges , with esc guidelines expressing weak recommendations for cac as a risk modifier among low - to - intermediate risk individuals based on clinical assessment ( iib , b )  . 
acc / aha conversely embraces a broader use of cac as a potential tool to refine lipid - lowering therapy allocation among patients with uncertain predicted benefit from treatment initiation ( iia , b )  . regarding the detection of obstructive disease among asymptomatic individuals , no recommendations are expressed by acc / aha guidelines , while a weak ( iib , b ) recommendation for the use of either coronary ct angiography or functional tests ( including stress cmr ) in patients with diabetes , strong family history or high clinical risk is made by esc guidelines . 
the use of coronary ct angiography or functional imaging in patients not fulfilling these requirements is contraindicated ( iii , c )  . ischemic heart disease in the setting of chronic coronary syndromes ( ccs ) , 2019 esc guidelines recommend either coronary ct angiography or stress cmr or their combined use to diagnose and to risk stratify obstructive disease among symptomatic patients based on their pre - test disease probability , local expertise and availability , and anticipated quality of the exam ( i to iia , b to c ) [ 10 ]  . 
less emphasis on coronary ct angiography use for ccs diagnosis is posed by the outdated 2012 acc / aha guidelines , which overall favors functional imaging tests as the exam of choice [ 11 ]  . among patients with a prior ccs diagnosis who needs risk assessment ( new / worsening symptoms or high clinical prognostic risk ) , esc guidelines highlight functional imaging tests as the exam of choice ( i , b )  . 
of note , acc / aha guidelines formally contemplate the use of coronary ct angiography for the assessment of patency of bypass grafts or of coronary stents 3mm in diameter in patients with new / worsening symptoms ( iib , b ) ; a similar statement is made by esc guidelines without a formal recommendation . in the setting of non - st - segment elevation acute coronary syndromes , esc guidelines recommend stress imaging to look for inducible ischemia before coronary angiography among patients with suspected low - risk unstable angina ( i , a )  . 
for both esc and acc / aha guidelines , among patients without prior history of coronary artery disease presenting with chest pain and having an inconclusive diagnostic assessment , coronary ct angiography should be considered as an alternative to coronary angiography ( iia , a ) [ 12 , 13 ]  . according to esc guidelines , among patients with stelevation myocardial infarction , stress cmr may be performed following primary percutaneous coronary intervention ( pci ) to assess residual ischemia and viability ( iib , c )  . 
 furthermore , cmr should be considered when echocardiography is suboptimal , both in - hospital ( after primary pci ) and after discharge , for the quantification of left ventricular function ( iia , c ) [ 14 ]  . 
no recommendations in this setting are provided by the outdated 2013 acc / aha guidelines [ 15 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 10131023 1019 valvular disease echocardiography plays a leading role in the study of valvular disease , according to both esc and acc / aha guidelines [ 16 , 17 ]  . in this setting , current acc / aha guidelines indicate ct and cmr as second - level examination in patients with a poor acoustic window that does not allow the correct evaluation of valve function and / or morphology . esc guidelines do not provide a specific class of recommendations for the use of ct and cmr , although their potential clinical value is acknowledged in the documents . 
 similarly , esc guidelines on infective endocarditis do not contain formal recommendation for ct or cmr , although ct findings are listed in the modified duke diagnostic criteria [ 18 ]  . 
the application of ct and cmr in these settings is still not included in the aforementioned guidelines , but in some cases is part of the clinical routine and is supported 1 3 1020 la radiologia medica ( 2020 ) 125 : 10131023 by appropriateness criteria suggested by dedicated expert consensus documents , as reported below . transcatheter procedure andstructural interventions restrictive cardiomyopathy according to a recent expert consensus document from european association of cardiovascular imaging ( eacvi ) and the working group on myocardial and pericardial diseases of the esc [ 27 ] , cmr is recommended for the diagnosis of restrictive cardiomyopathy thorough an accurate assessment of cardiac chambers volume and mass , beside myocardial tissue characterization . no formal recommendations have been reported about the use of mapping in this setting , although the clinical experience and the most recent literature suggest that tissue relaxometry imaging , particularly with t1 and t2 * mapping , may play a fundamental role in infiltrative cardiomyopathies and iron overload , respectively . moreover , when echocardiography is nondiagnostic and cmr contraindicated , ct can be adopted for the evaluation of cardiac chambers volume , myocardial mass , myocardial scar and extracellular volume fraction ( ecv ) quantification . inflammatory cardiomyopathies according to the recent expert consensus document on inflammatory nonischemic cardiomyopathy [ 28 ] , cmr may be considered as a first - line diagnostic tool for diagnostic workup of acute myocardial inflammation . 
the use of mapping to detect myocardial inflammation is strongly suggested in this setting , because it has a positive impact on diagnostic accuracy [ 29 ] that could be further improved through a mapping - based assessment of myocardial hyperemia [ 30 ]  . 
 similarly , cmr may be useful for the identification of various chronic inflammatory conditions , ranging from chronic myocarditis to sarcoidosis to human immunodeficiency virus disease , and to exclude inflammatory substrate of new onset arrhythmias [ 31 ]  . 
as previously indicated cmr has a role in identifying myocardial inflammation in patients with new onset or established heart failure [ 19 ]  . arrhythmogenic cardiomyopathy according to the recent expert consensus of the eacvi [ 32 ] , cmr is indicated to support the diagnosis of arrhythmogenic cardiomyopathy together with ecg , histological and functional evaluation , both in the early and advanced disease . because of its progressive nature , repeated cardiac imaging is needed to follow disease progression and for risk assessment of life - threatening ventricular arrhythmias . over the last years , the field of transcatheter valve and structural interventions has experienced a huge expansion supported by enormous technical development . 
 recent expert consensus documents , from both cardiological and radiological societies [ 33 , 34 ] , recommend ct for procedural planning in the setting of transcatheter aortic valve replacement ( tavr ) and valve - in - valve procedures . ct is widely used for procedural planning ( vascular accesses , annular sizing , determination of risk of annular injury and coronary occlusion , fluoroscopic angle prediction ) and patients selection . 
similarly , a recent expert consensus [ 35 ] stated the importance of ct in procedural planning of transcatheter mitral valve replacement , and in the transcatheter closure of paravalvular leakage , atrial septal defect , left atrial appendage and oval foramen . 
there is no consensus regarding the role of ct after tavr , although ct may adjuvate the diagnosis in case of valve thrombosis , infective endocarditis or structural degeneration . final remarks the esc and aha / acc guidelines convey few general remarks : 1 . 
cmr is generally considered appropriate when myocardial tissue characterization ( scar , infiltrative disease , inflammation , etc . ) is pivotal for the diagnosis and when echocardiography fails to provide an accurate morphofunctional assessment ; 2 . 
this observation highlights the urgent need of financial supports to large randomized controlled trials , in order to obtain unbiased results supporting the clinical value of cardiac ct and cmr in real clinical world . beyond these main messages , several additional considerations could be raised . 1 3 la radiologia medica ( 2020 ) 125 : 10131023 1021 the number of class i recommendations is significantly higher for cmr than coronary ct angiography ( fig.2 ) , likely reflecting the younger age of coronary ct and a more established attitude of cardiologists to use a nonionizing echocardiography - like imaging method . 
this scenario is likely to change in the next future , as a consequence of the development and standardization of new promising ctderived techniques , such as ct perfusion [ 36 ] , ct delayed enhancement [ 37 , 38 ] , ct - based extracellular volume quantification [ 39 ] and ct - based fractional flow reserve [ 40 ]  . although cmr has several formal recommendations in both esc and acc / aha guidelines , the role of parametric mapping techniques is still not established . 
this could be surprising considering the growing evidences about the positive impact of mapping in the diagnostic and prognostic evaluation of several conditions , as t2 * mapping for iron overload , t1 mapping in fabry disease , ecv in cardiac amyloidosis and parametric mapping in myocarditis [ 41 , 42 ]  . 
nevertheless , t2 * mapping is currently recommended in disease - specific consensus statement of experts [ 43 ] , as well as both t1 and t2 mapping technique in expert consensus about the use of cmr in inflammatory myocardial diseases [ 28 ]  . 
this could be shocking , considering that the diagnostic accuracy of stress cmr to detect significant coronary artery disease and to guide revascularization has been proved also by controlled randomized trails [ 45 , 46 ]  . 
on the other hand , the esc guidelines [ 18 ] recognize the role of cmr to detect myocardial ischemia , equally to nuclear medicine , but more investments are probably needed in the next future to increase the availability and the technological level of the mr scanners . although endovascular or mini - invasive preprocedural planning represent one of the most rapidly evolving application of three - dimensional cardiac imaging techniques , particularly in the settings of structural heart interventions and arrhythmias ablation , formal recommendations provided by the major cardiological society are very limited ( fig.5 ) , due to the lack of large randomized trial confirming their value . 
 however , several evidences and specific consensus statements have defined ct and cmr as useful tools to support extra - coronary heart interventions [ 33 , 34 , 48 , 49 ]  . in conclusion , the use of cardiac ct and cardiac mr in the risk assessment , diagnosis , therapeutic and procedural planning is in continuous development , driven by an increasing need to evolve toward an imaging - guided precision medicine , combined with cost - effectiveness and healthcare sustainability . 
a clear sign of this evolution is the new role recently recognized to the coronary ct angiography in the 2019 esc guidelines on chronic coronary syndromes , as recommended initial test for patients with a low to moderate clinical likelihood of disease . 
however , these developments must be accompanied by an increased availability of highperformance scanners in healthcare facilities and should emphasize the need of increasing the number of radiologists fully trained in cardiac imaging , exploiting and reinforcing different solutions , including the exchanging programs for residents , the education programs of the national and international scientific societies , as well as the dedicated master classes . authors contributions ae and mf contributed equally to the writing and editing of the final manuscript . funding open access funding provided by universit degli studi di roma la sapienza within the crui - care agreement . availability of data and material not applicable for that section.code availability not applicable for that section . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article contains data extracted from published papers . 
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the sustainability of the healthcare systems , considering the high economic burden of modern cardiac imaging equipments , makes cost - effective analysis an important tool , currently used for weighing different costs and health outcomes , when policy makers have to allocate funds and to prioritize interventions , getting the most out of their financial resources . 
this review aims at evaluating cost - effective analysis in the more recent literature , focused on the role of calcium score , coronary computed tomography angiography and cardiac magnetic resonance . keywords coronary computed tomography angiography ( ccta ) calcium score ( cs ) cardiac magnetic resonance ( cmr ) cost - effectiveness analysis ( cea ) introduction an ideal sustainable healthcare system delivers high quality care and improves public health without exhausting man - power and financial resources . 
nowadays , we have to face an increased awareness on the costs related to healthcare systems in which the most frequently used tool for decision - making is evidence - based medicine ( ebm )  . 
in this scenario , cardiovascular diseases ( cvd ) still comprise one of the predominant causes of death globally ( near 18 million * maurizio centonze maurizio.centonze@apss.tn.it 1 department ofdiagnostic imaging , apss oftrento , trento , italy 2 radiology department , experimental imaging center , irccs san raffaele scientific institute , milan , italy 3 school ofmedicine , vita - salute san raffaele university , 4 radiology unit , department ofsurgical science , university milan , italy ofturin , turin , italy worldwide ) and contribute predominantly to a decrease in quality of life [ 1 ]  . 
in the second - half of the last decade , the costs of cvd in the usa corresponded to $300 billion a year and in the european union 210 billion a year [ 2 ]  . 
between 1993 and 2002 , cardiovascular imaging represented nearly 30% of the worldwide imaging and had risen more twice compared to non - cardiac - related imaging ; in 2005 , it reached nearly one - third of the total imaging examinations [ 3 , 4 ]  . 
these considerations are at the basis of the recent framework of cost - effectiveness analysis ( cea ) which guides the use of diagnostic imaging with advanced technology and therefore high costs , such as cardiac computed tomography ( cct ) and cardiac magnetic resonance ( cmr )  . 
the national institute for health and clinical excellence ( nice ) defines a cea as an economic study design , in which consequences of different interventions are measured using a single outcome ( i.e. , life years gained , heart attacks or deaths avoided ) ; alternative interventions are then compared in terms of cost per unit of effectiveness [ 5 ]  . 
in order to evaluate this correctly , it is mandatory to differentiate between independent and mutually exclusive interventions : in the first case , the outcome and cost of an intervention are not affected by the introduction of another intervention , and it is sufficient to calculate the average cost - effectiveness ratio ( cers ) , which considers net cost over health outcomes . 
to correctly identify such differences , the ratios of the delta in costs over delta in health effects between interventions , the incremental cost - effectiveness ratios ( icers ) , are calculated . 
 the estimated value is based on calculating icer which should not be higher than the willingness - to - pay ( wtp ) , a threshold defined as the maximum cost at or below which a consumer or an institution is willing to pay for one unit of a given intervention . 
there is no broadly accepted threshold for additional costs for correct diagnosis : world health organization recommends a wtp threshold between one and three times a nations gross domestic product percapita ( for example , 40 , 000 in italy , 20 , 00030 , 000 in the united kingdom and $50 , 000 in the usa ) [ 6 ]  . 
the mathematical combination of values allocated to health as a function of years of life ( length ) and its quality yields the benefit of a given intervention as a numerical value , the quality - adjusted life years ( qaly )  . 
 the utility value is calculated based on health in a year , with a year in perfect health considered with a value of 1 ( 0.5 if a patient is bedridden ; death has a value of 0 ) , which is then multiplied by years lived in that state . 
the plane is divided into four quadrants : most cost - effectiveness analyses deliver results in ne quadrant , in which new intervention generates more health gains ( effectiveness measured in qaly ) but are more expensive ( cost )  . 
only new interventions that lay below this line can be adopted ( accept ) 1 3 1202 la radiologia medica ( 2020 ) 125 : 12001207 issues on evaluation arise from the different approaches and processes employed , potential variations in effect and cost estimates or the reproducibility of the modalities with which the events are observed over time ( for example , final outcomes or multiple time - points ) and how these can be applied to different patient subsets or populations without additional validation [ 7 ]  . 
moreover , studies which derive calculations from patients enrolled in clinical trials , inadvertently are potentially bias , with observations which last far over the defined timeframe for data collection and have limited generalizability . 
this probabilistic analysis tests all the assumptions used in the model and allows to quantify the impact of changes on the baseline [ 8 ]  . calcium score ( cs ) in a head - to - head comparison in the multi - ethnic study of atherosclerosis ( mesa ) , cs proved to be the best prognostic factor of cad compared to other traditional risk factors and a useful tool to stratify patients into lower or higher risk groups [ 912 ]  . 
cs is a good method to quantify the presence and burden of coronary atherosclerosis , and provides robust risk stratification above and beyond traditional risks scores in the setting of primary prevention [ 13 , 14 ]  . 
several studies have demonstrated that a significant proportion of statin candidates , defined according to current guidelines , have no detectable cs and subsequently these individuals have a low risk for cad [ 1517 ]  . 
moreover , while statins are highly effective , they have been linked to some side effects , such as muscle pain , digestive problems , arthralgia , headache and rarely liver damage . 
in this perspective , six recent ceas of cs screening ( populations in intermediate - risk and primary prevention setting ) , with well - constructed state - transition microsimulation models , which also considered real - life adherence rates and risks of adverse events associated with statin treatment , were selected . 
 [ 18 ] , based on results of the rotterdam study , tried to assess the cost - effectiveness of cs screening in an asymptomatic elderly population at intermediate risk of cad . 
four different strategies were compared : current practice ( no additional intervention modeled ) , current prevention guidelines for cardiovascular disease ( statin therapy when baseline ldl cholesterol exceeds 130mg / dl ; antihypertensive medication when baseline systolic blood pressure exceeds 140mm hg ) , cs and statin therapy for all individuals . 
women are more likely to be receive less aggressive treatments as they tend to be re - classified to a low - risk category which has a higher incidence of cad when compared to the opposite sex , potentially explaining this difference . 
however , in cases of disutility and high costs of statins ( $365 / year ) , cs was cost - effective ( < $50 , 000 / qaly )  . 
the multi - ethnic study of atherosclerosis treatment based on cs was compared to that of all intermediate - risk patients , and to that on the basis of the us guideline ( adult treatment panel iii , the current one at the time of the study ) [ 20 ] : cs was both effective and cost saving as a risk - stratification tool , particularly if there were adverse effects of long - term statin use , providing a better tailored preventive treatment to patients with risk of cardiovascular disease . 
 [ 22 ] compared the cost - effectiveness of four novel risk markers for screening asymptomatic individuals to prevent cad in the us population : high sensitivity c - reactive protein ( hscrp ) , cs , carotid artery intima media thickness on ultrasound ( cimt ) and ankle - brachial index ( abi )  . 
assuming a substantial disutility from taking daily statin therapy , screening men with cs is likely to be cost - effective ( $32 , 900 / qaly ) whereas screening with hscrp has more value in women ( $32 , 467 / qaly )  . 
even the individual perceived disutility in taking daily medication should play a key role in decisionmaking : a recent cea of cs as marker for administering long - term statin therapy versus treating all eligible patients , according to 2013 american college of cardiology / american heart association cholesterol management guidelines for atherosclerotic cardiovascular disease , showed that qalys and costs were similar between the two interventions [ 23 ]  . 
in the setting of primary prevention in intermediate - risk patients , the studies highlight the importance of evaluating individual needs and preferences when considering the proper treatment strategy for long - term use . 
in the 1 3 la radiologia medica ( 2020 ) 125 : 12001207 1203 above - mentioned ceas , the driving factors are the price of statins and cs , the perceived disutility linked to a life - long preventive treatment and side effects of statin administration . 
these studies found that cs is cost - effective when the cost of statins is higher , the cost of cs is low , and there is a disutility in statin treatment [ 19 , 23 ]  . coronary ct angiography ( ccta ) in a risk / cost - benefit evaluation , proper patient selection in the diagnostic use of invasive coronary angiography ( ica ) for excluding cad has been given increasing attention . 
 despite the increase in appropriateness criteria to evaluate the choice of ica and subsequent percutaneous coronary intervention ( pci ) , there is a wide variation in the quality of this assessment , which yields rates of inappropriateness of up to 55% [ 24 ]  . 
these findings can be used as a basis to suggest improvements for screening patients for ica , a procedure prescribed for more than 1 million patients in the usa per year , at an average cost of $9000 per procedure . 
 moreover , the clinical benefit of ica is unclear in patients without evident ischemic symptoms , and its broad use in asymptomatic patients seems to lead frequently to an inappropriate use of pci [ 2527 ]  . 
as gatekeepers for ica , the various stress tests for inducible ischemia have limitations due to reduced diagnostic accuracy compared to the gold standard , with a rate of nonobstructive cad in 59% of patients with a positive test [ 28 ]  . 
over the past 10years , ccta has gained acceptance among physicians as a valid non - invasive diagnostic tool for the evaluation of asymptomatic patients with a suspect of cad . 
the literature reports its high diagnostic accuracy compared with conventional stress testing , and may therefore be able to more effectively identify patients with cad , who in turn will most likely be candidates for ica [ 2932 ]  . 
moreover , in the recent nice and european society of cardiology ( esc ) guidelines , ccta represents the first line approach for the diagnosis of suspected stable angina [ 33 , 34 ]  . 
 [ 35 ] evaluated the treadmill tests of 3950 fire - fighters which identified 495 abnormal tests which in turn warranted additional cardiology evaluation : the costs of myocardial perfusion imaging ( mpi ) followed by ica were compared with those of cs followed by ccta and ica if needed . 
the combination of ccta and stress - imaging ( echo , spect , pet or mr ) , in patients with suspected stable cad and with a low prevalence of disease , were also cost - effective gatekeepers to ica and can therefore be successfully used as interventions for early revascularization candidate selection [ 37 ]  . 
it is well known that ccta can only provide an anatomical assessment of cad , but some high - grade stenoses seen on ccta are not flow limiting [ 3840 ]  . 
in an analysis of data obtained from the discover - flow study ( diagnosis of ischemiacausing stenoses obtained via non - invasive fractional flow reserve ) , which evaluated the costs of ffr - ccta in different clinical management settings , ccta seems to be an effective gatekeeper of ica , but only with poor advances in saving costs and in patient management [ 41 ] , whereas the use of ffr - ccta in identifying patients who needed pci improves outcome while reducing costs against describing stenosis via visual assessment alone . 
in other words , the model suggests that a strategy based on use of ffrccta as a gatekeeper for ica ( with an additional cost of $10001500 ) and pci in a lesion - specific manner would lower costs , because it would reduce the rate of invasive procedures ( far more costly ) in patients without flow - limiting stenosis . 
 [ 42 ] compared ccta with diagnostic methods other than the ica , in a retrospective cohort study in patients with suspected cad and a pre - test probability between 10 and 90% : the study showed that ccta was generally more effective in terms of qaly and cost than single - photon emission computed tomography ( spect )  . 
 the cost - effectiveness of ccta was significantly reduced in patients with higher pre - test probability ( 6190% ) , confirming what described also in previous studies [ 43 , 44 ]  . 
these results were re - confirmed recently by the same authors in a korean patient cohort with intermediate risk , stable chest pain , in which ccta was more cost - effective than spect , associated with fewer icas , and with no difference in clinical outcome [ 45 ]  . 
spect did not result as cost - effective even in a previous cea , in which ccta was superior in terms of anatomical diagnostic strategy for cad diagnosis [ 46 ]  . 
 [ 47 ] when comparing ccta with exercise stress testing ( est ) in improving the health - related quality of life in patients with stable chest pain : ccta increases qaly and decreases costs . 
the probability of ccta cost - effectiveness 1 3 1204 la radiologia medica ( 2020 ) 125 : 12001207 was highest in patients with < 30% likelihood of cad and least in patients with > 60% likelihood of cad , in which ica is recommended as first line diagnostic tool . cardiac magnetic resonance ( cmr ) to date , limited literature exists on cea of cmr . 
unlike ct - based imaging , which is used for the diagnosis of single specific conditions ( cs identifies calcified plaque , ccta coronary stenosis ) , cmr is a multi - parametric tool which assesses concomitantly multiple features such as ventricular function , myocardial perfusion , and viability , among others . 
the available data , therefore , does not discriminate the cost - effectiveness of the intervention in its main diagnostic applications , such as assessment of myocardial ischemia ( mi ) using stress cmr or myocardial viability ( mv ) using late gadolinium enhanced - cmr , but as overall intervention in cad . 
even echocardiography ( echo ) and nuclear medicine imaging techniques have been used to evaluate mi and mv : unlike echo , cmr does not present the limitations of the acoustic window , offers more spatial and temporal resolution than nuclear medicine modalities , better tissue characterization and does not use ionizing radiation [ 48 , 49 ]  . 
 thanks to these characteristics , cmr provides quantitative information on cardiac perfusion , viability and function , as well as on delayed enhancement and , more recently , mapping techniques provide quantification of edema and fibrosis . 
 considering only the cost minimization , in the setting of suspected cad , a cmr - driven strategy followed in case of positivity by ica , compared to ica ( without or with ffr ) as a single test , allows a saving of resources [ 5052 ]  . 
cea based on data collected in the clinical evaluation of magnetic resonance imaging in coronary heart disease study ( cemarc ) , evaluated 8 different diagnostic strategies alone or in combination ( est , spect , cmr and ica ) using uk sterling - based costs : in a population with low - intermediate risk of cad , only 2 of these strategies resulted potentially cost - effective for diagnosis , both including cmr ( est positive or inconclusive + cmr ; cmr positive or inconclusive followed by ica ) [ 53 ]  . 
in a subsequent cea of diagnostic strategies for cad , even derived from the ce - marc population , conclusions were slightly different : based on healthcare costs in switzerland , the most effective and least costly approach resulted est followed by ica if positive or followed by cmr if the est result was inconclusive and then followed by ica if the cmr result was positive . 
 data from a cea of the non - invasive cardiac testing trial ( cecat ) , which assessed 3 functional tests ( stress echo , stress - spect and stress cmr ) as gatekeeper for ica , showed that in an outpatient population with stable chest pain each of the interventions test can be used to delay ica , without detrimental variations in clinical outcome or significant increase in costs [ 49 ]  . 
this result was confirmed even in a head - to - head comparison of stress cmr as gatekeeper against direct ica [ 55 ] : this strategy significantly reduced costs in ruling out suspect cad , and saved 12 , 466 of hospital costs per life year . 
a systematic review that assessed the clinical and cost - effectiveness of stress cmr compared to late gadolinium - enhancement cmr stated that the latter was the optimal strategy , even over pet and spect [ 56 ]  . 
 in the wider concept of value in healthcare , as defined by michael e porter the patient health outcomes achieved per dollar spent [ 57 ] , a retrospective review conducted on 361 patients who underwent cmr showed a significant clinical impact in 71% of all patients , 27% in new diagnosis ; in addition , 11% avoided invasive procedures and 7% did not have to undergo additional diagnostic testing with net cost savings per patient of $2308 [ 58 ]  . this review has focused on cad ceas , but there are numerous other fields of application of the ccta and cmr , in particular acute chest pain and transcatheter aortic valve implantation ( tavi ) planning , thanks to their significant clinical implications . 
regarding the first , some recent studies show that prior to ica , use of ccta and cmr can be a cost - effective gatekeeping tool in low - risk ( < 30% cad prevalence ) acute chest pain patients in emergency department . 
tavi is nowadays an established treatment for inoperable and high - risk symptomatic patients with severe aortic stenosis , with indications continuously expanding to include intermediate and even low - risk patients [ 63 ]  . 
 the integration of tavi and ct imaging into clinical practice has become extremely deep : cardiac - ct represents the fundamental and cost - effective diagnostic imaging investigation for the selection of eligible patients and the appropriate prosthesis and size , for choosing the safest intervention access , and in the follow - up [ 63 , 65 ]  . 
although the topic is beyond the aim of this review , few words regarding the fully cardiological use of ct and mr equipment : considering the favorable cost - effectiveness ratio , it remains to assess whether an exclusive use of ct and mr equipments for cardiac imaging could be really economically convenient . 
as far as we know , currently in italy , there is a single center in which these equipments are completely dedicated to cardiac 1 3 la radiologia medica ( 2020 ) 125 : 12001207 1205 imaging and also in other western countries there are few similar examples . 
this technique provides a high - spatial - resolution tomographic evaluation of the heart , which allows studying accurately the ventricular volumes , identifying even segmental kinetic anomalies and properly detecting diffuse or focal tissue alterations through an excellent tissue characterization , while depicting different patterns of fibrosis distribution , myocardial edema or fatty substitution . 
through these capabilities , cmr has a pivotal role for the adequate management of the arrhythmic patient , allowing the identification of those phenotypic manifestations characteristic of structural heart diseases . 
therefore , cmr provides valuable information to reclassify the patient within the wide spectrum of potentially arrhythmogenic heart diseases , the definition of which remains the major determinants for both an adequate treatment and a poor prognosis . 
these rhythm anomalies can include supraventricular arrhythmias , which will not be extensively treated in this paper even if represent * pierpaolo palumbo palumbopierpaolo89@gmail.com 1 department ofbiotechnological andapplied clinical sciences , university oflaquila , via vetoio 1 , 67100laquila , aq , italy 2 radiology unit , san salvatore hospital , laquila , italy 3 department ofmorphology , surgery andexperimental medicine , university offerrara , ferrara , italy 4 department ofradiology , azienda ospedaliero - universitaria , ospedali riuniti di ancona , ancona , italy 5 department oflife , health andenvironmental sciences , university oflaquila , laquila , italy extremely frequent and clinical relevant arrhythmic patterns or ventricular arrhythmias which can be associated with a structural pathology . the extensive spectrum of ventricular arrhythmias ( vas ) ranges from isolated premature ventricular contractions ( pvcs ) to sustained ventricular tachycardia ( vt ) or ventricular fibrillation ( vf ) leading to sudden cardiac death ( scd )  . the most severe forms are the major determinants of morbidity and mortality in structurally diseased hearts . 
moreover , it can be a reactive interstitial and perivascular response , as it occurs in dilated cardiomyopathy or an interstitial deposit and replacement scarring in hypertrophic cardiomyopathy [ 6 ]  . in all these cases , disturbed cell - to - cell contact causes discontinuous propagation and non - uniform conduction , which results in slow conduction , electrogram fractionation and unidirectional block that favors arrhythmogenicity . in a fibrotic area that is completely deprived of myocardium , as in the presence of a localized scar , the main mechanism is the re - entry , which determines an arrhythmia when three contemporary events concur : parallel conduction ways such as bifurcated purkinje fibers ( the circuit ) , a unidirectional block and a slow conduction way . 
the conduction runs in zigzags among the bundles and is more vulnerable to arrhythmias [ 7 ]  . instead , abnormal automaticity exhibits parasystole : an ectopic rhythm that marches through the same cycle length , independent of the underlying rhythm due to electric isolation [ 8 ]  . main clinical characteristics andecg pattern even if arrhythmogenic cardiomyopathies can present with scd , the latter can be sometimes anticipated by symptoms or by such minor arrhythmias as pvcs . the clinical presentation varies widely : patients may complain palpitations , chest discomfort and syncope or presyncope , but may also present indirectly with symptoms of heart failure and volume overload . in the presence of one of these symptoms , the routine diagnostic workup generally includes 12 - lead surface electrocardiogram ( ecg ) , transthoracic echocardiography ( tte ) , 24 - h holter monitoring and stress test or coronary angiography when ischemia is suspected . the transthoracic echocardiography is the first step for cardiac imaging . 
it shows biventricular dilatation in dilated cardiomyopathy or increased wall thickness , papillary muscle abnormalities , lvot obstruction , or mitral valve systolic anterior motion ( sam ) that produces a dynamic jet of regurgitation in hypertrophic cardiomyopathy , and mitral valve prolapse ( mvp ) or mitral anulus disjunction ( mad )  . 
 anyway with echocardiography the assessment of right ventricle volumes or kinesis may be limited by suboptimal acoustic window ; right or left ventricle fibrosis indeed cannot be precisely identified due to the methodic poor contrast resolution . the ecgs , or the 24 - h holter monitoring can help identify the underlying cardiomyopathy but also give some clues on arrhythmia localization [ 9 ]  . from the basal ecg , we can obtain some important information . 
we can appreciate reduction of qrs voltage or presence of q waves that can add the suspect of fibrosis replacement or infiltration : low qrs voltages ( < 0.5mv ) in the limb leads are frequently observed in ac patients with fibrosis of the left ventricle ( lv ) , diffuse low qrs voltages can be found in extracellular amyloid infiltration and pathological q waves are present in infarct or in sarcoidosis [ 10 ]  . furthermore , distinctive ecg features can be related to specific cardiomyopathy such as t wave inversion in precordial leads , epsilon waves and right precordial qrs prolongation with delayed s wave that are typical in ac or inverted t waves in the inferior leads ( ii , iii , avf ) that can be associated with mitral valve prolapse . in addition , ecg can show benign features such as incomplete right bundle branch block ( rbbb ) , increased in qrs voltages and early repolarization : variant that can be often observed in the athletes heart . the ecg showing the pvc / vt can give an idea of localization of the ventricular arrhythmia . 
lbbb with negative qrs complexes in both avl and avr and positive qrs in inferior leads with a precordial transition 1 3 la radiologia medica ( 2020 ) 125 : 10871101 1089 fig . 
1 ecg patterns of right and left ventricular arrhythmia : a shows a right ventricular arrhythmia : ecg evidences a lbbb with negative qrs complexes in avl and avr ( black arrowheads ) and positive qrs in dii , diii and avf ( black asterisks ) expression of a rvot origin ( dotted white arrow )  . 
b shows a left ventricular arrhythmia : ecg shows a rbbb characterized by a secondary r wave ( r ) in the right precordial leads ( v13 ) ( black asterisks ) and a wide , slurred s wave in v4v5v6 ( black lines ) expression of a left ventricle origin ( white arrow ) that occurs at v4 or later identifies rvot origin that may lead to an idiopathic benign rvot arrhythmia but also a minor diagnostic criterion for ac [ 11 , 12 ]  . besides , vt with a lbbb pattern and a late - precordial transition with a positive avr and avl and negative in the inferior leads suggests right ventricle ( rv ) free wall origin and this morphology is more specific for ac , and is classified as a major diagnostic criterion . 
rbbb arrhythmia , characterized by positivity in inferior leads , can originate from the papillary muscle or from the lv infero - basal wall . finally , also the number of pvc ( > 500 / 24h ) or the presence of more than one morphologies can be associated with a more diffuse or multi - focus fibrosis . arrhythmogenic cardiomyopathy ( ac ) ac is an inherited cardiomyopathy with variable expressivity and penetrance , characterized by loss of myocytes with progressive fatty and fibrous tissue replacement [ 13 ]  . this rare condition ( prevalence ranging from 1 : 1000 to of 1 : 5000 ) recognizes the mutation of some desmosomal proteins [ 1416 ]  . 
the etiopathogenetic mechanism determines a mechanical detachment of myocytes from which derives an electrical uncoupling and consequent ventricular arrhythmias , structural and functional ventricular anomalies and increased risk of scd [ 17 , 18 ]  . the definition of arrhythmogenic cardiomyopathy has been discussed upon for years . 
at the beginning , ac went under the name of dysplasia , hinting to the congenital defect in the development of the right ventricular myocardium ( arrhythmogenic right ventricular dysplasia or arvd )  . 
when it became evident that this pathological condition was the result of a genetic defect in the cardiac desmosomes , it was recognized as a cardiomyopathy ( arrhythmogenic right ventricular cardiomyopathy or arvc ) and included in the american heart association classification of cardiomyopathies [ 19 ]  . 
although 1 3 1090 la radiologia medica ( 2020 ) 125 : 10871101 representing a matter of controversy , the term dysplasia has been commonly used since it was first recognized by marcus and colleagues in 1982 [ 20 ]  . traditionally , ac has been defined as a cardiomyopathy with predominant involvement of rv , although with frequent involvement of lv . 
recent studies have shown that lv involvement is much more common than previously thought and that isolated rv disease and lv involvement were present in 13% and 87% of ac - related deaths , respectively ( the latter in particular includes 17% of isolated forms and 70% of biventricular forms ) , as shown by miles etal . 
these symptoms are related to electrical anomalies including late potentials , pvcs , t waves inversion and epsilon wave ; the latter was considered pathognomonic , though its poor presentation and reproducibility [ 2325 ]  . 
in this context , scd may be the first clinical manifestation of ac , as observed in some young athletes where prolonged exercise induces an increase in tension of the myocardium leading to cellular disruption and leaking of cardiac enzymes , and may even result in transient rv dilatation and dysfunction , which significantly raises the risk of clinical onset of the disease determining about 20% of cases of scd [ 2628 ]  . because of this clinical heterogeneity , the diagnosis of ac is often difficult , especially in the early stages of the disease where electrical anomalies pre - date any structural manifestation suggestive of ac [ 18 , 21 , 29 ]  . 
for these reasons , in the absence of a real gold standard , in 2010 the task force criteria revised ( rtfc ) the former criteria used in the clinical practice for the diagnosis of ac [ 23 ]  . 
the rtfc consists of a composite score divided into major and minor criteria , which include structural , histological , electrical and genetic characteristics capable of defining the diagnosis of ac as definite , borderline , possible or absent . 
the novelties in the rtfc in respect to the previous document published in 1994 was based on the formal introduction of cardiac magnetic resonance ( cmr ) as a method for an accurate morphological study of rv [ 30 ] ( table1 )  . among advanced multimodality imaging which has reached high accuracy in the evaluation of thoracic and cardiovascular pathologies [ 2950 ] , cmr has indeed established as a clinical tool of fundamental importance for diagnosis and correct prognostic stratification of the arrhythmic patient . cmr allows to evaluate biventricular morphology , volumes , myocardial mass , wall thicknesses , fibro - adipose replacement , regional and global kinesis , flows and myocardial edema that usually is not observed in ac , but may be fig . 
end - diastolic and end - systolic short - axis ( a , b ) and long - axis ( c , d ) cine cmr shows dilated right ventricle and biventricular dyskinesia ( arrows )  . 
g , h lge acquisition reveals focal fibrosis on the same cardiac segments ( arrows and arrowheads ) 1 3 la radiologia medica ( 2020 ) 125 : 10871101 1091 useful for differential diagnosis with myocarditis . 
all these data are obtained with good spatial resolution , independently of the patients morphotype ( i.e. , limited acoustic window )  . subsequent cmr experiences provided an excellent specificity achieved by the rtfc criteria ( 94% and 96% of specificity for major and minor criteria , respectively ) , although relatively low sensitivity reported by many authors [ 51 , 52 ]  . in particular , the rtfc focuses on the dilation of the rv and / or global dysfunction , associated with anomalies of the regional contraction . 
in this regard , a role may be played by standardizing the strain by means of feature tracking , which provides excellent reproducibility and accuracy in identifying early anomalies of motility , even in the presence of a preserved global functionality [ 5355 ]  . among the main differential diagnoses with ac , biventricular dilation can be also observed as an often - reversible ventricular remodeling response to some electrical anomalies , such as the pvc observed in cases of rvotvt , or even in excessive workout athletes . particular mention deserves the role played by mri in tissue characterization through the use of appropriate pulse sequences . 
d , e positive lge sequence in the same region of the right lateral wall ( arrowheads ) 1 3 1092 la radiologia medica ( 2020 ) 125 : 10871101 more recently , tandri etal . 
reported the possibility of rv wall focal fibrosis identification using late gadolinium enhancement ( lge ) sequences [ 58 ] , an important finding considering that fibrosis replacement has been identified as one of the main arrhythmic substrates in ac , constituting a target for electrophysiological studies and biopsy . however , other conditions can present areas of fibrous substitution ( e.g. , myocarditis , rheumatic disease and sarcoidosis ) other that several studies have shown that this component may not be evident in the earliest stages of ac . current studies suggest that cmr significantly contributes to the diagnosis of ac even in pediatric patients , also considering that the slight cardiac alterations present in the pre - symptomatic forms can be barely evident to other methods such as echocardiography . however , caution should be used in cmr evaluation in pediatric patients as the evolving nature of the disease resulted in a low - yield test in children , thus recommended follow - up studies [ 59 ]  . 
similarly to the rtfc proposed for the adult population in 2010 , mri diagnosis is generally only related to morpho - functional data ( including the same major and minor criteria reported by the task force )  . 
showed a 7% of diagnostic yield [ 24 ]  . differential diagnosis ac often presents with heterogeneous and non - specific clinical and structural spectrum , overlapping with numerous other pathological conditions such as myocarditis , fig . 
 fatty infiltration ( c ) and lge ( d ) were evident on cmr ( white arrows ) 1 3 la radiologia medica ( 2020 ) 125 : 10871101 1093 sarcoidosis , right overload conditions or even para - physiological alterations such as athletes heart or cardiac displacement . although the multidisciplinary approach remains essential for an adequate differential diagnosis , cmr is considered the best diagnostic tool for a diagnosis of ac or to identify potential conditions that mimic ac . indeed , the combination of tissue characterization and functional images allows to significantly increase the diagnostic validity of cmr in identifying cardiac structural anomalies and thus the potential arrhythmogenic substrate . 
on a large study population including 946 consecutive patients submitted to cmr for deepening of ventricular arrhythmia diagnosed by electrophysiological assessment [ 62 ]  . in this regard , all those conditions characterized by fibrosis replacement are of particular interest considering that myocardial scar assumes a central role in the genesis and maintenance of re - entry arrhythmias commonly associated with structural heart diseases including ischemic and non - ischemic causes . even if ac may show non - specific fibrosis distribution , cmr is able to identify distributions considered pathognomonic to differentiate ac - type scars from non - ac - type forms , as subendocardial ischemic type or global subendocardial lge , as in the amyloidosis . cmr is also fundamental in the identification of areas of myocardial inflammation , also considered as important arrhythmic triggers causing qt lengthening associated with malignant ventricular tachycardias [ 63 ]  . among the main conditions that enter into differential diagnosis with ac for morphological characteristics and clinical presentation , myocarditis and rheumatic diseases are listed , including cardiac sarcoidosis . although myocarditis and ac are recognized as two distinct nosological entities , recent evidence has shown a suggestive continuum between both pathologies , recognizing in the infectious / inflammatory process one of the potential triggers capable of explaining the clinical onset of ac and the different phenotypic expressions of the disease [ 64 ]  . one of the most accredited etiopathogenetic hypotheses recognizes an intense inflammatory infiltrate in the so - called hot phase of disease in up to 2 / 3rd of cases promoting the decoupling of myocytes [ 65 ]  . 
however , although an inflammatory process can be an ac trigger , numerous evidences show that myocarditis is a distinct pathology . mri promises the noninvasive diagnosis ofmyocarditis , through the lake louis criteria and the revised lake louis criteria , with an auc close to 96% [ 66 , 67 ]  . 
two are the main typical features of myocarditis : edema , absent in the ac , and distribution , if we consider that myocarditis rarely affects the right ventricle . moreover , post - myocarditis ventricular arrhythmias seem to be significantly less frequent than ac , as reported in the study by pieroni etal . , with consequent difference in patient management [ 68 ]  . undoubtedly , differentiation remains difficult , if we consider that post - necrotic adipose replacement can be observed even after myocarditis . particular mention goes to rheumatic diseases , given that ventricular arrhythmias is often associated with these pathologies . the term of arrhythmogenic inflammatory cardiomyopathies among non - ischemic cardiomyopathies has been recently proposed to describe all those cases of ventricular arrhythmias with incidence of acute myocardial inflammation [ 63 ]  . 
myocardial inflammation , isolated or in the context of systemic inflammatory conditions , is often observed in numerous rheumatic pathologies related to different mechanisms such as coronary artery disease , microvascular anomalies , vasculitis and myocarditis [ 69 ]  . 
reported up to 21% of cases of scd in patients with systemic sclerosis [ 70 ]  . the identification of the arrhythmogenic substrate is of fundamental importance for an adequate management of the patient with rheumatic disease confirming a primary role for cmr [ 71 , 72 ]  . 
in particular , cmr is essential for recognizing potential fibrotic and inflammatory substrates [ 73 ]  . in this regard , the most common cause of fibrotic substrate in rheumatic pathologies is the microvascular damage , although structural anomalies can be found even in the absence of ischemic pathology . 
in fact , the evidence of dilated cardiomyopathies as well as infiltrative diseases such as in sarcoidosis and amyloidosis has been found in cases of rheumatoid arthritis . among the systemic inflammatory diseases , cardiac sarcoidosis ( cs ) shows important affinities with ac . 
it can mimic ac in many ways , as described in the study by vasaiwala etal . , who showed that sarcoidosis can share with ac also phenotypic characteristics , included in the major criteria [ 74 ]  . 
the authors conclude that it was possible to identify cases of cs in 15% of the patients included in the study population with definite diagnosis of ac . cs and ac can share important clinical and ecg characteristics , especially in case of right ventricle involvement , and therefore differentiation based on clinical criteria alone may be inadequate . cs primarily affects the free wall of the left ventricle and the basal interventricular septum , with patchy distribution , observed in up to 70% of cases , although an even larger involvement of the free wall of the right ventricle has been described in several cases . 
as reported in the vasaiwala study , however , the primary characteristic of cs is the dysfunction of the left ventricle , while the most frequent findings in ac are the dilation of the right ventricle and 1 3 1094 la radiologia medica ( 2020 ) 125 : 10871101 its dysfunction . 
conversely , the exclusive cs of the right ventricle remains rare . prerogative of cmr in cs diagnosis is the identification of the lge areas usually in the basal lv segments of the subepicardial interventricular septum , although patchy localization may also be evident in other segments and myocardial regions . finally , the identification of the lymph node involvement at the level of the mediastinal stations is also typical characteristic of cs . mitral valve prolapse ( mvp ) mvp is the most frequent structural cardiac anomaly , estimated in 23% of the general population [ 75 ]  . 
this disease is associated with a heterogeneous prognosis , depending on numerous factors ( e.g. , degree of mitral valve regurgitation and ejection fraction , also accounted as major predictor of mortality ; number of involved leaflet ; atrial enlargement ) [ 76 ]  . 
among the most common adverse events are either atrial or ventricular arrhythmias , present in 5060% of cases and scd , with an estimated risk of 0.4 to 2% per year . 
the wide scd variability incidence in mvp reported by the many autopsybased studies can be related to the rare univocal causeeffect relationship recognized between them . nevertheless , a 21 - year prospective registry on postdeath cardiac findings reported by basso etal . 
notably , trigger mechanisms should be differentiated from potential substrates . pvcs are generally trigger mechanism for arrhythmia in mvp , which are induced by acute myocardial stretch as occurs in the papillary muscles during leaflets prolapse ; early stretch - induced after - depolarization can occur as an abnormal automatism in the purkinje fibers distal to the papillary muscles . on the other hand , fibrosis represents the common substrate for arrhythmias , increasing vulnerability through both trigger activities and re - entry mechanisms . cmr can help both diagnose mvp and identify specific arrhythmic substrate . 
in this regard , numerous factors seem to be responsible for an increased risk of malignant arrhythmias , some described within the anatomical anomalies related to the mitral complex , others as direct consequences of the myocardium involvement , allowing identification of the entity known as arrhythmic mvp [ 77 , 78 ]  . recognized in the study by nordhues etal . , conducted on 18 , 786 patients , divided almost equally into bi - leaflets and single leaflet involvement . 
a high risk of ventricular tachycardia in patients with bi - leaflets involvement was detected , although no increased risk of cardiac arrest / icd implantation was demonstrated [ 79 ]  . 
however , the up - regulation of fibrosis markers has also been proposed as a potential phenomenon responsible for fibrotic replacement thus becoming a marker itself in identifying the risk of scd in mvp patients . 
in particular , in the study by bui etal . , a non - focal subclinical fibrosis associated with complex ventricular arrhythmias was identified , an aspect that is partially reflected in the study by pradella etal . , where areas of impaired t1 relaxation were identified even in patients without lge , independently of valve dysfunction [ 83 , 84 ]  . athlete heart intense and prolonged exercise induces specific remodeling of the ventricular chambers so as to recognize the athletes heart as a well - defined clinical entity , characterized by a reduced heart rate and an increase in ventricular cavity size . 
the causes are most commonly inherited , and in young people < 35years mainly include hypertrophic cardiomyopathy ( hcm ) and ac . substances of abuse may also have a significant impact through the induction of fibrosis . among the anatomical factors related to the mitral complex , the number of leaflets involved in the prolapse is myocardial response to physical exercise does not seem to be univocal , since concentric or eccentric myocardial 1 3 la radiologia medica ( 2020 ) 125 : 10871101 1095 fig . 
 a shows a bi - leaflet prolapse , with a paradoxical annular dynamics duringsystole and annulus disjunction ( whitetwoheaded arrow ) ; mitral valve regurgitation is also present ( black asterisks )  . 
however , c , d images evidence fibrotic area ( arrows ) on the basal posterolateral myocardial wall in both cases ( whitearrows ) remodeling can be observed , depending on the type of exercise ; in particular , increase in ventricular volumes seems more marked in endurance disciplines ( morganton hypothesis ) , while strength exercise seems to be associated with wall thickening , although this remains a controversial hypothesis . 
in any case , ac and hcm should be excluded , respectively , especially in subjects with arrhythmic episodes or with familiarity for arrhythmic events [ 85 , 86 ]  . in this scenario , cardiac imaging plays a primary role in the identification of structural cardiac anomalies ; in particular , as underlined by the european society of cardiology ( esc ) recommendations , cmr has proved to be superior to other methods [ 85 ]  . however , the diagnostic accuracy of cmr appears to be very limited by using endoventricular volumes as discriminators , since there is no real cutoff between healthy competitive and pathological athletes . 
however , the limits of the volumetric approach are evident and accurate detraining and follow - up studies are often recommended for a differential evaluation between the athletes heart and arrhythmic phenotypes . the main advantages derive from the analysis of ventricular kinetics as well as from tissue characterization . 
reported that further evaluation of the strain analysis can provide an objective real advantage also in subjects with preserved ef [ 89 ]  . finally , the tissue characterization study often plays a pivotal role in the differential diagnosis with arrhythmic phenotype . 
in fact , fibrosis is often considered as a primary sign of heart disease , although it can sometimes occur at the hinge point in response to the ventricular overload . 
furthermore , although focal fibrosis detectable with 1 3 1096 la radiologia medica ( 2020 ) 125 : 10871101 lge , cmr appears to be absent especially in the early stages of ac , an increase in pre - clinical interstitial fibrosis can often be found with t1 mapping technique [ 90 ]  . 
therefore , the multimodality imaging approach should be reserved for those athletes with high suspicion of cardiac pathology , including symptomatic athletes or athletes with first level investigation anomalies [ 85 , 93 ]  . structurally normal heart specific considerations must be made about the anomalies of conduction in structurally normal hearts . 
these include the rvot - vt , considered among the main differential diagnoses with ac , sharing similar lbbb morphology to the vt , the frequent pvc and the inferior axis . in fact , frequent pvcs are often responsible for a reversible ventricular remodeling , which poses problems of differential diagnosis with ac . while in the past there was the belief of a link between ac and rvot - vt , recent works have shown profound differences between these conditions . 
documented a more depressed rv functionality in the ac , as well as larger ventricular volumes and greater mechanical dispersion , which reflects a greater underlying electrical dispersion , thus denying the hypothesis of rvot - vt as a fruste form of ac [ 95 ]  . conversely , brugada syndrome ( brs ) has been considered for years as a disorder in the absence of cardiac fig . 
b , d show volume - rendered reconstruction of biventricular volumes obtained by segmentation of cine mr images on end - diastole , where the rv cavity is shown in yellow and the lv in bordeaux . 
 [ 23 ] ac arrhythmogenic cardiomyopathy , rv right ventricle , lv left ventricle , plax parasternal long - axis view , psax parasternal short - axis view , rvot right ventricle outflow tract , bsa body surface area , mri magnetic resonance imaging structural abnormalities . 
 confirms these early considerations , more recent evidences suggest the possibility that brugada ecg pattern may be marker of an underlying structural anomaly [ 96 , 97 ]  . in particular , this evidence involves patients with brs ecg patterns and positive for scn5a mutation , associated with a higher incidence of clinical events . 
study , who demonstrated evidence of mesocardial lge , suggestive of the hypothesis of underlying structural anomalies in brs patients [ 99 ]  . conclusions cmr has a key role in the diagnosis of patients with vas . 
cmr furthermore allows an accurate detection of lv involvement , which is observedmore than frequentlyandisnot always associated with severe rv abnormalities . cmr is also diriment when differentiation is neededamong arrhythmic conditions ( e.g. , myocarditis , rheumaticandinfiltrative diseases , mitral valve prolapse , athlete heart and idiopathic arrhythmic conditions )  . 
moreover , cmr has a pivotal role in confirming or excluding fibrotic myocardial tissue replacement by lge , which is a strong predictor of ventriculartachyarrhythmiaevents . 1 3 1098 la radiologia medica ( 2020 ) 125 : 10871101 a combination of clinical characteristics , electrophysiologicaland imaging data may provide useful information toimprove risk stratification . 
in this context , cardiac magnetic resonance ( cmr ) may play a crucial role in defining the diagnosis and guiding treatments , by offering a robust myocardial characterization based on the inherent magnetic properties of abnormal tissues , thus limiting the use of endomyocardial biopsy . 
in this review article , we explore the role of cmr in the assessment of a wide range of myocardial diseases causing restrictive patterns , from iron overload to cardiac amyloidosis , endomyocardial fibrosis or radiation - induced heart disease . 
here , we emphasize the incremental value of novel relaxometric techniques such as t1 and t2 mapping , which may recognize different storage diseases based on the intrinsic magnetic properties of the accumulating metabolites , with or without the use of gadolinium - based contrast agents . 
finally , we describe the useful role of cardiac computed tomography for diagnosis and management of restrictive cardiomyopathies when cmr is contraindicated . keywords restrictive cardiomyopathies infiltrative cardiomyopathies cardiovascular magnetic resonance cardiac imaging introduction restrictive cardiomyopathy ( rcm ) is a myocardial disorder that is usually caused by increased myocardial stiffness which results in impaired ventricular filling . 
rcm include primary or idiopathic ( a rare familial or sporadic genetic condition associated with the accumulation of desmin and * riccardo faletti riccardo.faletti@unito.it 1 department ofexperimental medicine , sapienza university ofrome , rome , italy 2 department ofradiological , oncological andpathological sciences , sapienza university ofrome , rome , italy 3 unit ofradiodiagnostics ii , university hospital policlinico vittorio emanuele , catania , italy 4 department ofsurgical sciences , radiology unit , university ofturin , turin , italy collagen type iii ) and secondary forms , which include infiltrative , non - infiltrative and storage disorders . rcms are generally caused by processes causing abnormal deposition of proteins , glycogen and iron within the myocardium , leading to ventricular stiffness with diastolic dysfunction . the most common classification system [ 1 ] in adults divides restrictive cardiomyopathies on the basis of etiology in : 1 . 
endomyocardial : endomyocardial fibrosis ( emf ) , radiation - induced , drugs , carcinoid , metastatic tumor . the most common initial clinical manifestations are exertional dyspnea , exercise intolerance due to inability of vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 10721086 1073 the ventricular filling , fatigue and lower extremity edema , whereas heart failure symptoms occur only in advanced stage ; atrial enlargement can lead to arrhythmias and concomitant thromboembolic complications are not uncommon [ 1 ]  . transthoracic echocardiography ( tte ) is the first - line examination . 
the most common tee findings are its normal right and left systolic function until advanced stage ( normal ejection fraction ) , normal or reduced left ventricular ( lv ) volume and bi - atrial enlargement , with abnormal diastolic compliance characterized by increased early diastolic filling velocity due to elevated left atrial pressure . wall thickness is generally normal , except for infiltrative and storage processes in which case it is typically increased . cardiovascular magnetic resonance ( cmr ) can combine the morphologic and functional evaluation with an accurate characterization of the myocardial changes on the basis of the intrinsic magnetic properties of different tissues ( t1 , t2 and t2 * values )  . 
moreover , the use of gadolinium - based contrast agents ( gbca ) may improve the evaluation of myocardial damage based on late gadolinium enhancement ( lge ) technique and post - contrast t1 mapping sequences , which permit to calculate extracellular volume ( ecv ) [ 2 ]  . 
 the lge phenomenon is due to the accumulation of gbca in the extracellular space that can be increased in case of fibrosis , deposition of pathologic proteins or acute myocardial damage . 
cardiac computed tomography ( cct ) could be a valid alternative for diagnosis and management of infiltrative cardiomyopathies when cmr is contraindicated . in this review , we illustrate the importance of these cmr techniques and their great support when contrast media administration is contraindicated . 
finally , we describe the emergent role of cct . cmr approach torestrictive cardiomyopathies in case of suspected rcm , cmr protocol should encompass cine steady - state free precession ( ssfp ) electrocardiography - gated sequences to assess atrial and ventricular volumes , wall motion anomalies and morphologic abnormalities such as atrial enlargement or lv wall thickening [ 3 ]  . lge imaging is mandatory for differential diagnosis between forms of cardiomyopathies , because enhancement patterns may address distinct conditions . 
in traditional lge imaging , the inversion time ( it ) to null the signal of healthy myocardium is manually chosen by the operator using a specific sequence ( look looker , for instance )  . 
this operator - dependent choice might be challenging in case of massive infiltration of the heart , for example in case of amyloidosis , and may result in erroneous choices resulting in non - diagnostic examinations ( fig.1 ) [ 4 ]  . 
cine - ssfp sequences ( a short axis view ; b 4 - chamber view ) showed a thickening of the left ventricular myocardium wall ( 19 mm in the septum ) with global and moderate hypokinesia ( left ventricular ejection fraction 46% )  . 
inversion recovery turbo field echo sequences ( d and e short axis view ; f and g 4 - chamber view ) with a wrong myocardium null time ( red box and arrow ) and the one with the correct null time ( green box and arrow ) ; these last showed a diffuse areas of circumferential subendocardial pattern enhancement . 
the final diagnosis was light chain ( al ) cardiac amyloidosis 1 3 1074 la radiologia medica ( 2020 ) 125 : 10721086 of phase - sensitive inversion recovery ( psir ) sequences by all vendors , a lge reconstruction technique less sensitive to operator choice of it , has made it easier to obtain accurate lge images and to determine the extent of cardiac involvement [ 5 ]  . as they are currently available by all vendors , t1 and t2 mapping techniques should be used to characterize in a quantitative and reproducible way the tissue signal alterations in icm and rcm [ 4 , 5 ]  . 
conventional t2 - weighted imaging and t2 mapping enable the detection of myocardial edema . finally , in case of suspected iron overload cardiomyopathy ( ioc ) - specific gradient echo sequences designed to measure t2 * relaxation time should be incorporated into the cmr protocol in order to detect the excessive myocardial iron deposition ( see specific section )  . main cmr features of rcm are summarized in table1 . amyloidosis amyloidosis is a group of diseases caused by protein misfolding resulting in aggregation and deposition of amyloid fibrils [ 7 ]  . 
ca was thought to be a rare disease , but is currently considered an underdiagnosed condition [ 8 ]  . more than 30 proteins are known to cause amyloidosis , and two types are predominantly responsible for cardiac involvement : immunoglobulin light chain amyloid ( al ) and transthyretin amyloid ( attr )  . 
attr amyloidosis is divided into a hereditary form associated with mutations of ttr protein ( attrm ) , and a more common non - hereditary wild - type form ( attrwt ) , a late - onset disease affecting predominantly men . 
attrwt almost exclusively affects the heart , while attrm has a wide range of presentations [ 7 ]  . al amyloidosis , the most frequent form of systemic amyloidosis , has an estimated prevalence of 812 cases per million person - years , and cardiac involvement occurs in 5075% of cases [ 9 ]  . 
ca is characterized by remodeling of the myocardium extracellular matrix , expansion of ecv , edema , reduction in capillary density , modifications in cardiomyocyte volume and even macroscopic changes in cardiac structure and function with the increase in lv mass and wall thickness resulting in diastolic dysfunction [ 5 ]  . the reference standard for the diagnosis of ca is endomyocardial biopsy , an invasive procedure not widely available . 
in addition , the biopsy sample may not be representative of the infiltration status of the whole myocardiuimaging offers a noninvasive alternative to evaluate the whole heart [ 4 ]  . as ca is an important predictor of poor outcome , early diagnosis is crucial in both al and attr amyloidosis . 
in particular , cmr seems a promising tool to track different disease mechanisms ( such as edema , infiltration and cardiomyocyte response ) and to evaluate cardiac involvement progression or regression during the course of the therapy [ 10 ]  . 
the identification of ca in attr patients permits to start treatment with targeted anti amyloid therapies . cmr is a useful tool to differentiate the diagnosis between ca and other conditions ( e.g. , hypertrophic cardiomyopathy , hypertensive cardiopathy , afd ) [ 11 ]  . 
 asymmetrical septal hypertrophy is divided in two morphological subtypes : sigmoid septum ( in 55% of attr patients ) and reverse septal contour ( in 24% of attr cases )  . 
symmetrical and concentric lv hypertrophy is present in only 18% of attr cases , while it is present in 68% of al patients [ 12 ]  . the evaluation of ventricular morphology and function in ca should be performed with cine images obtained using ssfp sequences acquired in long axis and short axis planes covering the lv . lge imaging with inversion recovery sequences is a fundamental technique to diagnose ca [ 11 ]  . 
the introduction of psir , an lge technique less sensitive to operator choice of null point , has made lge easier to perform on ca patients [ 13 ]  . 
these patterns are correlated with the degree of infiltration of the lv and provide prognostic information , since a greater burden of infiltration is related to poorer prognosis [ 12 ]  . t1 mapping demonstrates an increased nt1 time in ca ( fig.2 ) and is related to markers of systolic and diastolic dysfunction [ 14 ]  . 
post - contrast t1 mapping and ecv estimation demonstrate markedly elevated 1 3 la radiologia medica ( 2020 ) 125 : 10721086 1075 1 3 1076 la radiologia medica ( 2020 ) 125 : 10721086 fig . 
cine - ssfp sequences ( a short axis view ; b 4 - chamber view ) , which show a thickening of both the left ventricular myocardium ( 18 mm in the septum ) and the right ventricle , but also of the atrial walls with global and severe hypokinesia ( left ventricular ejection fraction 26% )  . 
inversion recovery turbo field echo sequences ( c short axis view ; d 4 - chamber view ) for late gadolinium enhancement ( lge ) analysis ; there are diffuse areas of circumferential subendocardial pattern enhancement even with transmural extension in the basal segment . 
the patient was then scanned with 99mtc - dpd ( image g ) , where the abnormal and diffuse presence of the osteotropic indicator is observed in the left and right ventricle with a perugini score = 3 . 
 ecv also provides insight into myocardial response to fibril deposition : total myocyte cell volume , calculated from ecv and indexed lv myocardial volume , is higher in attr than al patients , suggesting possible compensatory myocyte hypertrophy that might be protective [ 16 ]  . 
diagnosis is challenging as ecg abnormalities are shown in just 3.28.6% of patients with clinically silent cs [ 20 ] , and diagnostic criteria include different imaging modalities and histological confirmation [ 19 ]  . 
in this setting , cmr represents a useful tool to better characterize myocardial tissue , with a reported negative predictive value of 100% , sensitivity of 100% , specificity of 78% , and diagnostic accuracy of 83% [ 20 ]  . 
several studies also showed a significant increase in native t1 , t2 mapping and ecv values in patients with biopsy - proven extra - cardiac sarcoidosis as compared with healthy controls [ 19 ]  . 
mapping techniques improve the accuracy of cs diagnostic criteria and represent a helpful strategy to evaluate patients response to treatment , since mapping values seem to recover after immunosuppressive therapy in active cs [ 20 ]  . 
although cmr can investigate several aspects of cardiac involvement in sarcoidosis , the diagnosis remains challenging as its different features are often superimposable to that of acute or chronic myocarditis or to myocardial infarction . 
the novel hybrid imaging techniques like pet - cmr seem promising in the identification of active granulomatous lesions with high sensitivity [ 22 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 10721086 1077 fig . 
3 57 - year - old female with frequent syncopal episodes and ventricular tachycardia , lv dilation and severe reduction in ef at tte , with no obstruction of coronary arteries at coronary angiography . 
 cmr revealed no edema on t2w - stir images ( a short axis view and d lv long axis view ) and extensive areas of late gadolinium enhancement at ir - tfe images ( b short axis view and e lv long axis view ) , with a non - ischemic pattern of distribution . 
the fdg - pet ( c short axis view , f long axis view ) confirmed the diagnosis of sarcoidosis with the identification of areas of fdg uptake ( i.e. , active inflammation ) within the myocardium and in the mediastinal lymph nodes . 
lv left ventricle , ef ejection fraction ; tte transthoracic echocardium lysosomal storage disease the lysosomal storage disorders ( lsd ) and in particular the glycosphingolipidoses ( gaucher , niemannpick and afd ) , glycogen storage diseases ( pompe , danon disease and prkag2 deficiency ) and mucopolysaccharidosis frequently involve cardiac structures , causing infiltrative cardiomyopathies [ 23 ]  . 
afd cardiomyopathy is a major determinant in patients survival and occurs in both classical phenotype ( complete absence of enzymes activity ) and variants ( with very low residual - galactosidase activity ) , which include the isolated form ( cardiac variant ) mimicking a sarcomeric hypertrophic cardiomyopathy . afd often appears as concentric lv hypertrophy with a variable degree of myocardial wall thickening and papillary muscles prominence , which lately ( ? ) may lead to arrhythmias , myocardial ischemia or heart failure [ 1 ]  . 
afd usually becomes clinically apparent in the third decade of life in males , whereas in females it may be silent until much later in life [ 24 ]  . 
while afd diagnosis is often delayed , the prognosis is highly influenced by the timely start of enzymatic replacement therapy ( ert ) , as ert inhibits the development and progression of myocardial damage [ 25 ] on tte , afd phenotype overlaps many other hypertrophic conditions ; therefore , the diagnosis may be challenging when not supported by specific ecg signs , positive familiar history or other manifestations of afd . 
cmr has rapidly gained a crucial role in the diagnostics , as it combines the assessment of cardiac function and the characterization of tissue abnormalities [ 1 ]  . lge has been found in up to 50% of afd patients [ 26 ] ; usually at the lv inferolateral wall with subendocardial involvement , which represents the typical hallmark on cmr ( fig.4 ) [ 26 ] , this typical lge distribution is useful for differentiating diagnosis in the spectrum of lv symmetrical 1 3 1078 la radiologia medica ( 2020 ) 125 : 10721086 fig . 
4 andersonfabry diseasecine - ssfp in short axis ( a ) and four - chamber ( b ) views acquired on end - diastolic phase demonstrate an asymmetrical hypertrophy with predominant involvement of septum ( ivs maximal thickness : 20mm )  . 
stir t2 - weighted image ( d ) shows an area of myocardial edema located in lv antero - lateral wall , with a subendocardial distribution pattern ( white arrow ) , confirmed by the blue area ( t2 ratio > 2 ) in the panel at the botto the analysis of nt1 ( e ) map demonstrates severe reduction in global nt1 ( reddish brown color , nt1 : 877 23ms , normal value for our scanner 9701020ms ) except for the focus of increased nt1 at inferolateral wall ( nt1 : 1116 ms , black arrowhead ) matching the area of increase in ecv ( white arrowhead , ecv : 48% ) on relative map ( f , global ecv : 27% )  . 
cine - ssfp steady - state free precession images ; ivs interventricular septum ; lge late gadolinium enhancement ; stir short tau inversion recovery ; lv left ventricle ; nt1 native t1 map ; ecv extracellular volume fraction hypertrophy [ 27 ]  . 
lge has been explained as myocardial fibrosis due to the focal imbalance between the increase in collagen synthesis and decrease in metalloproteinases , caused by glycosphingolipids [ 28 ]  . 
lge together with the maximal wall thickness and cardiac mass represented the best predictor of cardiac events [ 29 ] , even if in women lge frequently occurs before lv hypertrophy development [ 30 ]  . as validated in various studies [ 3134 ] , myocardial nt1 values are globally decreased , as a consequence of the myocardial accumulation of glycosphingolipids [ 31 ] , and may discriminate from other infiltrative cardiomyopathies that , apart from iron overload , are usually associated with normal or incremented t1 values [ 32 , 33 ]  . in a study performed on 123 patients , nt1 distinguished afd from hypertrophic cardiomyopathy ( hcm ) and healthy controls ( sensitivity 88% and 88% , specificity 92% and 86% , respectively ) using a cutoff value of 940ms on a 1.5 t scanner and modified locklocker inversion ( molli ) recovery sequence , whereas a better diagnostic performance is obtained with 3.0t scanner ( sensitivity 97% , specificity 93% , threshold of 1220ms ) [ 35 ]  . 
myocardial nt1 lowering has also been observed in 4159% of afd patients with no lv hypertrophy [ 32 , 36 ] , thus appearing an early marker of disease progression and predictor of clinical worsening at a 12 - month follow - up [ 36 ]  . 
myocardial ecv is generally preserved in afd patients ( with lower values in males compared to females [ 33 ] )  . in a recent study , an increase in t2 - weighted signal was found in 24 / 78 afd patients reflecting myocardial edema , whereas myocardial inflammation was confirmed by histology in 44 / 78 patients [ 34 ]  . 
other authors found an elongation of t2 relaxation time ( global or localized to segments with lge ) as compared to hcm and controls [ 37 ] , associated with chronic troponin elevation , suggesting the presence of an underlying chronic inflammatory cardiomyopathy [ 34 ]  . although systolic function assessed by ejection fraction is generally normal in afd patients , different studies reported myocardial strain reduction assessed with feature tracking ( ft ) technique . 
in particular , afd patients show impairment in global longitudinal strain ( gls ) correlated with myocardial damage degree ( presence of lge and cardiac biomarkers ) and nt1 values , even at pre - hypertrophic stage [ 38 ]  . 
furthermore , afd is characterized by reduction in global circumferential strain ( gcs ) and in gcs gradient from the lv base to the apex [ 39 ]  . finally , the role of cmr to assess the response to ert is under investigation . 
it has been found that ert induces a decrease in myocardial t2 values , and in lv mass and wall thickness of patients with little or no lge at baseline [ 25 ]  . 
 1 3 la radiologia medica ( 2020 ) 125 : 10721086 1079 ert also causes a slight increase in t1 mapping values , especially in patients at earlier stages of the disease , while its effects seem less effective in more advanced disease [ 25 ]  . iron overload iron overload or hemochromatosis indicates accumulation of iron in the body due to genetic metabolic disorders with increased intestinal iron absorption ( primary form ) or repeated blood transfusions ( secondary form ) [ 40 ]  . 
when involved , the heart can develop a secondary cardiomyopathy , the ioc , which is the leading cause of death and is characterized by cardiac dysfunction , initially diastolic and then systolic , secondary to increased deposition of iron in the myocardium [ 40 ]  . myocardial iron overload is a progressive process depending on the increasing levels of serum iron , regulated through transferring mediated uptake mechanisms . 
in the cardiomyocytes , iron deposition initially occurs in the perinuclear lysosomes , but when the overload exceeds , iron can accumulate throughout the sarcoplasm [ 40 , 41 ]  . myocardial iron deposition initially begins within the epicardium and then extends toward the endocardium , which helps explain the preservation of systolic function until very late in the disease . 
the excess of iron may be removed with chelation therapy , even though the reversibility of myocardial damage is reduced in the more advanced stages of the disease [ 41 ]  . clinical presentation of ioc varies from the total absence of any symptoms or only exertional dyspnea at early phase to heart failure symptoms , when the damage severely affects lv systolic function and determines dilated cardiomyopathy [ 41 ]  . 
iron deposition can also occur in the pericardium , and if extensive enough , it results in clinical signs and symptoms [ 42 ]  . tte is commonly used to screen the patients and for clinical follow - up . 
at tte , lv usually shows normal wall , biventricular dilatation and progressive evidence of a restrictive pattern . cmr has emerged as the best noninvasive method to quantitatively assess the myocardial iron load [ 40 , 42 ]  . 
t2 * measured in a full - thickness region of interest within the interventricular septum is considered highly representative of global myocardial iron [ 43 ]  . a value of 20 ms is considered the best performing threshold to define myocardial siderosis at 1.5t scanner [ 41 ]  . 
t2 * imaging has also emerged as the best quantitative parameter to guide and assess response to chelation therapy [ 45 ] and to monitor disease progression , and is currently the only parametric mapping technique recommended in disease - specific clinical guidelines [ 46 ]  . although the t2 * technique remains the reference technique for clinical assessment of iron overload , great advantages are offered by the novel t1 and t2 mapping sequences , since myocardial values are reduced in both sequences [ 46 ]  . in addition , in patients with only mild increases in cardiac iron , nt1 showed a superior reproducibility as compared to t2 * measurements ( about 2.57 fold t2 * ) [ 47 ]  . lge was also detected in the 15 , 619% of patients with thalassemia major and the extent of myocardial fibrosis was comparable in patients that developed heart failure and patients who did not [ 48 ]  . finally , ecv may be increased in patients with cardiac iron overload , as it reflects diffuse interstitial myocardial fibrosis that occurs in more advanced phases of the disease [ 46 ]  . endomyocardial fibrosis emf is characterized by deposition of fibrous tissue in the endocardium leading to restrictive pattern , with the reduction in ventricular volumes and increase in atrial volumes , normal wall thickness or apical obliteration due to fibrous endocardial thickening [ 49 ]  . emf was initially described in tropical countries , in young adults with a bimodal distribution peaking at 10 and 30years of age , mainly in rural and poor populations [ 49 ]  . although the pathogenesis is unclear , malnutrition , parasitic infestation ( malaria , schistosoma , filariasis ) , genetic factors have been proposed as potential causes triggering 1 3 1080 la radiologia medica ( 2020 ) 125 : 10721086 fig . 
5 cardiac iron overloada 42 - year - old woman with cooleys disease and moderate reduction in ventricular function ( ef : 42% ) show a global myocardial hypointensity on stir image ( a ) and a diffuse inhomogeneous abnormal signal on lge imaging ( b ) , with no evidence of clear focal areas of enhancement . 
analysis of t2 * map ( c ) , generated by traditional multiecho gradient echo t2 - weighted sequence , shows a diffuse and marked reduction in the global myocardial t2 * relaxation time ( t2 * = 01.5ms , normal value > 20ms )  . 
 nt1 map ( d ) shows a significant reduction in global nt1 value ( nt1 535ms , normal value 9701020ms ) , affected by susceptibility effect of intramyocardial iron accumulation . 
hypereosinophilia , infection disease and autoimmunity may act as a profibrotic role by promoting the synthesis of collagen by fibroblasts , with progressive endomyocardial damage and scarring . emf usually starts with active diffuse inflammation with endothelial damage , myocardial edema , eosinophilic infiltration and subendocardial necrosis and vasculitis , frequently associated with pericardial effusion and thrombi adherent to endocardial surfaces . 
when the inflammatory activity declines , it evolves in a progressive interstitial fibrosis and myocyte hypertrophy ( chronic phase ) causing rcm , whose phenotype is characterized by biventricular volume reduction and atrial dilatation , and subsequent isolated right - sided heart involvement with apical retraction . extensive emf may cause restrictive patterns , apex obliteration ( differential diagnoses includes apical hcm ) and diastolic dysfunction . cmr offers a comprehensive evaluation of ventricular function and morphology ( including an excellent visualization of the ventricular apex ) , endocavitary thrombus detection and assessment of tissue abnormalities . lge typically involves the endocardial and subendocardial layers of both ventricles ; with a non - coronary pattern , and the subvalvular apparatus and chord , lge is typically a continuous hyperintense stria extending from the subvalvular region to the apex , where it is usually more prominent ( fig.6 ) [ 50 ]  . in this setting , cmr has a role not only for diagnosis and staging , but also in assessing response to treatment , in inhibiting inflammation and solving thrombosis , and in prognostic stratification [ 49 ]  . radiationinduced heart disease radiation therapy is a valuable therapeutic option , which improves clinical outcome and reduces post - surgery recurrences in various thoracic malignancies ( e.g. , hodgkin or non - hodgkin lymphomas , breast or esophageal cancer )  . 
among potential complications , cardiovascular diseases are among the most serious and for a long time were underestimated . 1 3 la radiologia medica ( 2020 ) 125 : 10721086 1081 fig . 
lge images in 4 chambers ( e ) and short axis ( f ) demonstrate a diffuse subendocardial hyperintensity and a circumferential pericardial effusion the term radiation - induced heart disease ( rhd ) depicts a complex entity that can manifest in a large number of conditions , such as accelerated atherosclerosis , valve disease , cardiomyopathies , conduction system abnormalities and pericarditis [ 51 ]  . 
rhd is influenced by many factors ( e.g. , the dose , interval between irradiations , concomitant chemotherapy ) and its incidence is ranging from 0.5 to 37% among patients treated for breast cancer and 49.554.6% for lymphoma , with an overall estimated prevalence of 10% [ 52 ]  . 
commonly , rhd patients remain asymptomatic for a long time , and only 10% manifest symptoms or signs decades after treatment [ 53 ]  . a spectrum of different phenotypes are associated with rhd , including myocardial fibrosis with wall motion anomalies , lv hypertrophy , diastolic dysfunction with restrictive phenotype and congestive heart failure , and are quite common in patients who received more than 60gy or chemoradiotherapy [ 52 ]  . in this clinical setting , the role of cmr for the assessment of rhd has not been fully established . cmr appears promising in anticipating the rhd diagnosis by depicting the early myocardial tissue changes related to the radiation - induced damage before the 1 3 1082 la radiologia medica ( 2020 ) 125 : 10721086 occurrence of functional impairment , with consequent impact in patient management and treatment strategy [ 54 ]  . very few studies investigated rhd using cmr . 
 [ 55 ] found lge in 52% of 24 patients treated for esophageal cancer with a predominant mid - layer myocardial distribution , associated with hypokinesia of lge + segments . 
 [ 56 ] on 31 patients with history of mediastinal rht for hodgkins disease reported subendocardial or transmural lge in 26% of patients , and perfusion defects , evaluated with stress cmr , in 61% of the patients . the quantitative biventricular functional assessment offered by cine sequences is recommended in those with suboptimal tte or discrepant results on 2016 esc position paper on cancer treatments and cardiovascular toxicity [ 57 ]  . 
pericardial thickening is also frequent in those patients [ 58 ]  . novel t1 and t2 mapping techniques could open new perspectives in the early detection of diffuse myocardial inflammation and fibrosis following rht . 
however , systematic studies are still lacking and preliminary experiences have been reported only as isolated case reports [ 59 ]  . differential diagnosis betweenrcm andconstrictive pericarditis the distinction between constrictive pericarditis ( cp ) and rcms could be challenging , as the two manifest with overlapping clinical presentations and restrictive flow patterns with diastolic dysfunction at tte [ 60 ]  . rcms are associated with increased stiffness and reduced relaxation of ventricular walls , which alter the elastic properties or the extracellular matrix of the myocardial tissue . conversely , cp is typically a complication of chronic pericarditis or pericardiotomy and determines an encasement of cardiac chambers in a rigid pericardial sac , resulting in interventricular dependence and dissociation between intracardiac and intrathoracic pressures during respiration [ 61 ]  . cmr provides useful information that helps to differentiate the diagnosis between cp and rcms . first of all , in cp black blood t1 - weighted sequences and cine - ssfp can demonstrate a diffuse thickening of pericardial layers with calcifications ( typically hypointense ) [ 62 ] , even if almost 20% of cp patients have normal pericardial thickness [ 61 ]  . pericardial effusion can be present in both cp and rcm ( i.e. , in amyloidosis ) , but in rcm it does not show septa or loculations , which are typical of cp [ 62 ]  . 
atrial enlargement is a characteristic feature of rcms , together with ventricular wall hypertrophy [ 62 ]  . contrast enhancement of the pericardial layers has been reported in 4873% of patients with cp and is supposed to be associated with neovascularization and chronic inflammation . 
on the other hand , the presence of hyperintense pericardial signal on t2 - short tau inversion recovery is a sign of active inflammation , and it has been reported in just 3% of patients with cp [ 63 ]  . free - breathing real - time cine sequences are able to depict in cp interventricular septal flattening or bouncing during inspiration . 
cct can also identify thickening , calcification or enhancement of the pericardial layers or pericardial effusion , helping the diagnosis of pericardial diseases , which may go in differential diagnosis with restrictive cardiomyopathies [ 68 ]  . lge is the cornerstone of differential diagnosis of cardiomyopathies in cmr and can be demonstrated also with cct [ 69 ]  . 
the late iodine enhancement ( lie ) can be imaged in ccta because iodine contrast medium and gbca have similar kinetics resulting in comparable washin and washout for both healthy and pathologic myocardium [ 70 ]  . 
lie imaging with ct can be obtained 515min after contrast injection [ 71 ]  . although lie can be demonstrated with single energy scanners [ 72 ] , dual energy ct scanners with techniques of material decomposition may also provide iodine maps for an even more confident diagnosis [ 73 ]  . ecv has been demonstrated to be a robust indicator of disease burden and a prognostic marker in ca and its results are altered in other icm [ 4 ]  . 
7 constrictive pericarditistse t1 - weighted images acquired on short axis view before ( a ) and 3 min after gadolinium administration ( b ) demonstrate a diffuse thickening of pericardial layer with minimal effusion and slight enhancement of the visceral pericardial layer . 
on stir t2 - weighted image ( c ) , a focal area on myocardial edema ( white arrowhead ) is found in the lv inferior wall corresponding to the area of pathological enhancement ( black arrowhead ) on lge image ( d ) by demonstrating a condition of active myocarditis . 
 on free - breathing real - time cine - ssfp acquired in end - expiration ( e ) and end - inspiration ( f ) , a bouncing and leftward shifting of ivs is seen during inspiration ( white arrow ) due to the inversion of interventricular pressure ratio combined with inextensibility of the pericardial sac . 
tse turbo spin echo ; stir short tau inversion recovery ; lge late gadolinium enhancement ; lv left ventricle ; ssfp steady - state free precession ; ivs interventricular septum cmr [ 71 ]  . 
nevertheless , it is important to emphasize that the operators experience is crucial to identify lie [ 74 ]  . the advantages of cct imaging consists in wide scanner availability , reduced costs and examination time , simultaneous evaluation of the coronary arteries and the possibility to perform in patients with cmr contraindications . 
disadvantages are a less robust tissue characterization compared with cmr and the patient exposure to ionizing radiations and iodinated contrast medium . conclusion cmr is emerging as a robust and powerful noninvasive imaging modality for the diagnosis of various forms of icms and rcthe myocardial tissue characterization offered by cmr and strengthened by the novel t1 e t2 mapping technique , may identify those storage or infiltrative forms that are associated with characteristic alterations of the myocardial relaxometric properties or detect other restrictive conditions , where myocardium is subject to diffuse inflammation or fibrosis . 
when the clinical scenario is unclear , a cmr multiparametric approach may help to reach the correct diagnosis with a significant impact on clinical decision making . funding open access funding provided by universit degli studi di torino within the crui - care agreement . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in 1 3 1084 la radiologia medica ( 2020 ) 125 : 10721086 the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
 the aim of this paper is to review the technical basis of cmr , from cardiac imaging planes to cardiac imaging sequences . keywords cardiac mri sequences technique cmr cardiac mr cardiac magnetic resonance ( cmr ) imaging is an effective method for noninvasively imaging the heart . 
but mr technology significantly changed since clinical introduction in late 80s : in the last two decades cmr impressively enhanced spatial and temporal resolution , broadening its spectrum of applications in cardiovascular disease [ 1 ]  . one of the improvement has been the introduction of fast imaging techniques . 
conventional imaging techniques acquire only one line of the k - space per heartbeat , so the tr ( repetition time ) for those pulse sequences is defined by the patients heart rate and correspond to the rr interval . 
with such intrinsic features , cmr is suitable for diagnosis , follow - up and longitudinal monitoring after treatment of cardiovascular diseases , and the aim of this paper is to provide an overview on cardiac mr technique , covering acquisition planes and imaging techniques . if compared with other body parts , cmr deals with specific issues arising from cardiac and respiratory motion . 
 to overcome motion artifacts , cmr requires synchronous cardiac and respiratory gating or breath - holding techniques . cardiac synchronization is achieved by using the patients ecg signal : the r wave of the ecg is detected and used to generate a synchronization pulse for mr data acquisition [ 3 ]  . 
the standard three orthogonal planes normally used for mr imaging do not match with the cardiac axes : specific sections parallel and orthogonal to cardiac axes ( mainly short axis and long axis of the heart ) are mandatory for cardiac imaging [ 4 , 5 ]  . longaxis , twochamber view this plane ( fig.1b ) is easily obtained from a midventricular localizer through a centerline from apex to left atrium ( fig.1a ) and is used to evaluate the left heart structures , in particular for anteroposterior and superoinferior anatomic details ; it is also useful for evaluating the mitral valve . longaxis , fourchamber view this stack of images , derived from the left ventricular long axis ( two - chamber view ) through an ideal line connecting the posterior wall of the left atrium , mitral valve , and left ventricular apex , shows the relationship of the four cardiac 1041 chambers to each other on a single image , as well as mitral and tricuspid valve . 
1 ae the scheme shows how to obtain cmr anatomic planes starting from an axial ( a ) or oblique - sagittal ( c ) localizer : every line represent the planned and desired plane , while arrows address to the results ( b , d , e )  . 
lv = left ventricle , la = left atrium , rv = right ventricle , ra = right atrium , = mitral valve 1 3 1042 la radiologia medica ( 2020 ) 125 : 10401055 fig . 
2 ac the scheme shows how to obtain the three - chamber plane starting from a two - chamber long axis ( a ) and two - chamber short axis ( b ) plane : every line represent the planned and desired plane , while arrows address to the results ( c )  . 
lv = left ventricle , la = left atrium , rv = right ventricle , = mitral valve and * = aorta cardiac imaging sequences black blood fast ( or turbo ) spin echo performing a cmr study , two major groups of sequences are roughly distinguishable on a feature basis : one encompass morphology , function and flow , while the other is focused on tissue characterization . morphology , function andflow in this list of cmr sequences , we have two mayor subgroups : black blood and bright blood images . the most commonly used pulse sequence for morphologic ( anatomical ) cardiac imaging combines the black - blood preparation scheme with the fast or turbo se pulse sequence providing high contrast between the blood pool and the heart and vessel walls . while conventional se pulse sequence generates a single spin echo signal by the use of an excitation pulse followed by a 180 refocusing pulse , the fast se pulse sequence generates multiple echoes by applying multiple 180 pulses after 1 3 la radiologia medica ( 2020 ) 125 : 10401055 1043 the initial 90 pulse [ 6 , 7 ]  . 
because each echo is used to fill a new line of k - space , the number of echoes acquired for each excitation pulse is known as echo train length ( etl ) or turbofactor . 
with this technique two or more slices can be acquired during a single breath - hold ( the so - called single shot )  . in combination with the se pulse sequence , a black blood magnetization preparation scheme is used in order to improve the effectiveness of black blood imaging [ 8 , 9 ] .this scheme is based on the addition of two 180 radio frequencies ( rf ) inversion before the se pulse sequence . 
the first 180 pulse inverts the magnetization of all tissues and blood , while the second 180 pulse re - inverts the magnetization only within the slice of tissue to be imaged . 
there is a time delay before the excitation pulse ( inversion time , ti ) during that the inverted blood magnetization recovers ( due to t1 relaxation ) from its initial negative value : at that time , the 90 excitation pulse of the fast or turbo se pulse sequence is applied . 
it is a technique that displays the cardiac motion in a cine loop fashion taking images of the heart in motion throughout the cardiac cycle ; therefore , periodic changes of the cardiac chambers and ventricular walls can be visualized . 
the bssfp sequence ensures high signal intensity of the images despite very short tr due to the fact that the phase shift induced by the imaging gradients is exactly zero at the time of tr [ 12 ]  . because of these advantages , cine mri can assess cardiac function with high accuracy and reproducibility and has been considered the gold standard in the assessment of systolic biventricular function [ 13 ]  . 
 accurate quantification is important for congenital heart disease such as tetralogy of fallot , transposition of great arteries and for diagnosis of different cardiomyopathy such as arrhythmogenic right ventricular dysplasia or hypertrophic cardiomyopathy [ 14 , 15 ]  . 
the mass - to - volume ration is a useful index of lv remodeling or is considered helpful to differentiate forms of lv hypertrophy and is calculated by the ratio of the lv mass divided by the edv . 
in addition to volumetric quantification , cine images acquired in specific planes also allow evaluation of the valvular insufficiency , outflow tract obstruction , dyssynchrony or asynchrony of the ventricular wall , or mobility of the cardiac tumors . cine bssfp images can also be used to assess global and regional myocardial mechanics through the so - called feature - tracking cine mr ( cmr - ft ) analysis . 
cmr - ft relies on software analogous to speckle - tracking echocardiography that tracks intramyocardial features detected 1 3 1044 la radiologia medica ( 2020 ) 125 : 10401055 fig . 
 endocardial and epicardial borders of left ventricle and endocardial border of right ventricle are depicted both in end - diastolic ( a ) and end - systolic frames ( b )  . 
green line and red lines indicate left ventricles epicardial and endocardial border , respectively , while yellow line depicts right ventricle endocardial border between the epicardial and endocardial myocardial tissue boundaries . 
cmr - ft analysis allows to follow changes of dimensions such as velocities , displacement , strain and strain rate and offers incremental clinical information in comparison with volume analysis and wall motion score index [ 16 ]  . 
the three most commonly measured strain parameters are longitudinal strain ( ls ) , radial strain ( rs ) and circumferential strain ( cs ) : ls represents the longitudinal shortening from the base to the apex ; rs is the radially directed myocardial deformation toward the center of the lv cavity and indicates the lv thickening and thinning motion during the cardiac cycle ; cs expresses lv myocardial fiber shortening along the circular perimeter observed on a short axis [ 17 ]  . 
 feature - tracking analysis can potentially differentiate normal from abnormal heart function ; therefore cmrft represents a novel tool to investigate heart failure pathophysiology , disease progression and risk stratification not only in ischemic heart disease [ 18 ] , but also in a variety of other cardiovascular disease such as hypertrophic cardiomyopathy heart failure and reduced ejection fraction , perimyocarditis , aortic valve stenosis or heart transplanted patient [ 19 ]  . bright blood mr angiography ( mra ) mra of the heart could be performed with ( contrastenhanced mra ) or without contrast media . 
this latter , whichindeedrepresents the latest technology improvement in this field , should be preferable in many circumstances , because it does not modify the typical cmr protocol and could be done at the end of the study . 
this technique , also known as whole heart , is an isotropic 3d dataset of a ssfp sequence acquired with ecg - triggering and respiratory navigator gating ( free - breath )  . 
the basic sequence is a 3d acquisition of t1 - weighted fast gradient echo or turbo field 1 3 la radiologia medica ( 2020 ) 125 : 10401055 1045 fig . 
5 ae example of evaluation of left ventricle feature - tracking evaluation : endocardial and epicardial are tracked during the cardiac cycle ( a ) and the vectors are depicted ( green and red lines , respectively )  . 
global analysis of longitudinal , circumferential and radial strain can be performed ( a , c and d , respectively ) as well as segmental analysis ( e ) echo with a flip angle of 4045 and very short tr and te , so that the vessels appear bright because of gd while the background signal is suppressed due to a saturation effect . 
 more vessel details are appreciable if a subtraction mask ( pre - contrast mra images ) is applied and if power injector is used in order to increase the bolus concentration and , thus , vessel conspicuity [ 22 , 23 ]  . 
when only the visualization of the target vessel ( s ) is required , two different methods can be used : mr fluoroscopy or time - resolved ce - mra . 
the first is a real - time monitoring during bolus injection [ 24 , 25 ] , similar to bolus tracking of ct angiography , while the second is a multiphasic acquisition which can display multiple time frames of volumetric images with a temporal resolution of 12s , due to data sharing technique and reduced spatial resolution . 
most frequent cardiovascular application of ce - mra is aortic diseases , aortic graft patency , pulmonary thromboembolism and vessel anomalies [ 26 ]  . flow imagingconventional phase contrast cine mri ( pcmri ) pc - mri is acquired similarly to conventional cardiac gated cine mr but , in addition to magnitude images , phase images are also acquired to indicate flow velocity . 
phase images are obtained adding a bipolar velocity - encoding gradient and , since the phase shift is proportional to the flow velocity along the direction of the gradient , it is possible to quantify the phase shift caused by the flowing blood . 
in phase - contrast cine , the stationary tissue appears intermediate signal intensity on the phase contrast image , while the flowing blood would appear white or black signal intensity , depending on the direction of the flow relative to the velocity - encoding gradients [ 27 ]  . 
 the technique allows for quantification of cardiac output , valve regurgitation , severity of vascular and valvular stenosis , pulmonary to systemic flow ratio ( i.e. , qp / qs ratio , which reflects shunting of blood ) and shunting flow in congenital heart disease . the total blood flow in a cardiac cycle can be calculated as the sum of the blood flows at all the cardiac phases . 
the peak pressure gradient is then estimated by using the modified bernoulli equation p = 4 2 , where p is the peak pressure gradient in millimeters of mercury and is the peak blood flow velocity in meters per second . 
a disadvantage of mri , however , for pressure gradient estimations compared to echocardiography is its lower temporal resolution [ 32 ]  . 1 3 1046 la radiologia medica ( 2020 ) 125 : 10401055 fig . 
6 ac isotropic 3d ssfp whole heart images showing different cardiovascular applications : evaluation of the thoracic aorta ( a ) , congenital aortic disease ( b ) and coronary artery evaluation ( c )  . 
 ao = aorta , # = right aortic arch , * = aberrant left subclavian artery , = left coronary artery arising from the ascending aorta ( abnormal origin ) 1 3 la radiologia medica ( 2020 ) 125 : 10401055 1047 multiple axes , so it allows the dynamic visualization of flowing blood through large and complex cardiovascular territories . 
post - processing of a 4d flow sequence is complex and is based on the generation of vector plots or particle trace techniques such as streamlines and pathlines ( fig.9 ) as well as calculation of a wide range of quantitative hemodynamic parameters , or biomarker . the most commonly evaluated biomarkers to describe flow and its interaction with vessel walls are : pulse wave velocity ( pwv ) that indicates the speed at which the systolic pulse propagates through the cardiovascular tree and is defined as the distance traveled by the pulse wave divided by the time it takes to travel that distance ( pwv = distance / time ) ; turbulence that can be depicted by flow streamlines or pathlines [ 33 ] ; pressure that is expressed as peak estimated gradient applying the modified bernoulli equation to 4d flow data through a given structure ; wall shear stress ( wss ) that is the frictional force that flowing blood exerts on the vessel wall ; flow eccentricity that is depicted in 4d acquisition more easily than in doppler echocardiography and conventional pc - mri . 4d flow visualization helped to produce flow - based hypotheses of different disease such as negative impact of flow eccentricity on the aortic wall , for example , eccentric flow in bicuspid aortic valve has been correlated with increased growth rate of ascending aortic diameter [ 33 ]  . 
7 a , b volume rendering ( a ) and mip ( b ) ce - mra images of the thoracic aorta after surgical repair : ascending aorta and aortic arch replacement ( * ) plus frozen elephant trunk ( fet ) in the proximal descending aorta ( )  . 
the lumen along the endovascular portion of the fet is apparently reduced due to artifacts generated by the metallic material of the stent graft ( nitinol ) 4d flow imaging in recent years the so - called four - dimensional ( 4d ) flow sequence had been introduced in clinical practice . 
flow through the aortic valve plane is than calculated as the product of measured velocities by time within the valve ( panel c ) 1 3 1048 la radiologia medica ( 2020 ) 125 : 10401055 mechanism of the delayed enhancement in cmr is based on the kinetics of gadoliniuthis paramagnetic contrast agent , once injected intravenously , diffuses from the plasma to the interstitial spaces of tissues , with a typical extracellular distribution , than is completely washed away in 1020m when myocardial tissue is damaged , the wash - out is reduced because of the augmented distribution volume of gadolinium due to cell membranes ruptures as in infarcted lesions or to the expanded interstitial space like in tissue fibrosis or inflammation . 
this delayed wash - out is emphasized by mri acquiring a t1 - weighted sequence generally 1015min after gadolinium injection to differentiate bright areas of contrast medium accumulation ( lge ) from normal myocardial areas , where gadolinium has already been washed away [ 35 ]  . 
in fact , gadolinium shortens the longitudinal relaxation time ( t1 ) and the t1 - dependent acquisition enhances the areas of contrast medium accumulation ( hyper - intensity )  . the conventional lge sequence is an ecg - gated segmented inversion recovery fast low angle shot ( flash ) gradient - echo acquisition [ 36 ]  . 
it starts with a trigger delay after the r - wave ( to acquire in diastole ) applying a non - selective 180 - degrees inversion pulse to prepare longitudinal magnetization ( t1 dependent ) and the acquisition starts after an inversion time ( ti ) that approximates the zero crossing of magnetization recovery to null the signal of normal myocardium that appears black . 
this approach achieves high - quality images with high spatial resolution allowing for the evaluation of thin walls ( right ventricle ) , the analysis of subtle lesions or the identification of the lesion borders for the quantification of the area at risk of myocardial infarcts . 
anyway , breath - hold acquisitions may suffer from respiratory artifacts especially in patients of older age or affected by cardiopulmonary deficiency , while in case of arrhythmias the rr interval variation could affect the signal intensity over a breath - hold and generate artifacts . 
the creation of vortices below the level of the coaction is clearly depicted ( white arrow ) tissue characterization advanced myocardial tissue characterization may be achieved by mri using both contrast - enhanced sequences ( late gadolinium enhancement imaging ) and parametric myocardial mapping techniques ( t1 , t2 mapping )  . lge imaging since its introduction about two decades ago , lge has represented a milestone in cardiac mri examination . 
the 1 3 la radiologia medica ( 2020 ) 125 : 10401055 1049 sequence is the single - shot navigated free - breathing sequence that uses multiple repeated measurements averaging to correct respiratory motion and may enhance its snr , because of the less time constraints . 
highly arrhythmic patients and respiratory irregularity may cause motion artifacts with image blurring [ 39 ]  . considering clinical applications , lge provides optimal evaluation of myocardial infarcts and scarring . 
the transmurality and pattern of distribution associated with a high spatial resolution of the technique is a unique modality to differentiate ischemic cardiopathy from nonischemic cardiomyopathies [ 40 ] , but also from myocarditis ( typically subepicardial or midwall lge )  . 
alternatively , the presence of elements with paramagnetic properties like iron of gadolinium chelates strongly shortens the t1 . t1 mapping andecv the t1 mapping sequences similarly to the lge acquisitions start with a 180 degrees inversion pulse to excite magnetization , a series of single - shot t1 weighted images are acquired at different ti with a temporal pre - defined scheme related to the heart - beats . 
the process is repeated following a pause for complete t1 recovery with a slight variation of ti to sample more points on the relaxation curve until all the pixel of cardiac image are covered . 
a t1 map of the slice is created with an estimate of t1 of each pixel that is encoded as signal intensity in the map [ 49 ]  . there are different t1 mapping sequences whose duration depends on heart rate . 
the most used and solid sequences are the modified look - locker imaging ( molli ) and shortened molli ( shmolli ) acquisitions that derive from the original looklocker sequence as the acronym suggest . 
the shmolli has a reduced breath - hold time that anyway best fits with long pre - contrast t1 [ 50 , 51 ]  . another application is the saturation recovery singleshot acquisition ( sasha ) that uses a saturation recovery pulse instead of the inversion pulse . 
the estimation of t1 is more precise and it is less dependent from cardiac rhythm , but the image noise is exacerbated by a reduced cnr . the mapping technique may be acquired as a pre - contrast application ( native t1 ) that can investigate diffuse pathological changes of myocardiunative t1 values may differentiate the cardiac involvement from specific disease like andersonfabry disease [ 52 , 53 ] and can help differential diagnosis of hypertrophic phenotypes as in the case of hypertensive cardiopathy and hypertrophic cardiomyopathy [ 54 ] , but the range of values among various disease is still partially overlying and attention must be paid to give a fig . 
moreover , the epicardial fat create a chemical shift artifact that may partially cover the subepicardiua fatwater separated lge may be achieved with a different read - out technique and allows for the distinction of these different tissue components [ 47 ]  . myocardial mapping despite its undoubted value , lge imaging is based on the contrast resolution between different areas of the myocardium so that it may identify a focal fibrosis ( scar ) or a segmented lesion ( infarction ) while diffuse fibrosis processes or inflammation of the myocardium may be difficult to be depicted . 
furthermore , for smoother alterations like the peri - infarct edematous zone ( the so - called area at risk ) , the absence of a precise threshold limits the reproducibility of myocardial scars quantifications . 1 3 la radiologia medica ( 2020 ) 125 : 10401055 1051 definite diagnosis . 
the most robust parameter to quantify diffuse fibrosis is the ecv [ 55 , 56 ] that represents the distribution volume of the gadolinium in the myocardium and it is less sensitive to the various confounding factors that affect native and post - contrast t1 like gadolinium clearance rate and injection parameters , body composition and others . 
ecv could also help differentiate various cardiac disease in addition to native t1 and t2 . t2 mapping the t2 maps are obtained through the application of different potential t2 - weighted sequences with a multiecho approach . 
13 follow - up of an eosinophilic myocarditis ( subacute phase ) : short axis basal ( a ) and midventricular ( b ) conventional stir ( t2 - weighted ) , corresponding t2 color map ( c ) and midventricular free breathing 3d lge image ( d ) : stir images show suspected residual inflammation of basal interventricular septum , quantitative t2 map confirm elevated values of t2 in the basal septum ( 6070ms ) , but also slight elevation in the mid - septulge image shows a scar ( no edema on the t2 map ) on the anterior segment 1 3 1052 la radiologia medica ( 2020 ) 125 : 10401055 fig . 
14 adenosine stress mrifast spoiled gradient - echo frame of an apical slice on short axis view at stress ( a ) and rest ( b ) : see the subendocardial perfusion deficit of the antero - lateral wall ( asterisk ) in the stress image , completely disappeared in the rest acquisition indicating an inducible ischemia perfusion imaging recently , cmr has become a non - invasive competitor of scintigraphic techniques in the assessment of myocardial perfusion , that is important in the diagnosis and evaluation of ischemic cardiopathy . 
the absence of ionizing radiation and the superior spatial resolution are great advantages over scintigraphy , especially if perfusion imaging is combined with lge and even coronary imaging . the perfusion sequence is made by a pre - pulse ( inversion or saturation pulse ) for nulling the myocardium signal and the t1 dependence for exalting the first pass of gadolinium through the myocardium after a bolus injection [ 35 ]  . 
a fast spoiled gradient - echo sequence is generally applied . the typical scheme of the perfusion imaging consists of a two sets of bolus injections , the first after an adequate pharmacologic stress to explore the presence of perfusion defects ( segmental hypointensity )  . 
in addition , ccta , by providing detailed information on coronary plaque morphology and composition with identification of specific high - risk plaque features , may further improve the risk stratification beyond the assessment of coronary stenosis . 
the development of new ccta applications , such as stress myocardial ct perfusion and computational fluids dynamic applied to standard ccta to derive ct - based fractional flow reserve ( ffr ) values have shown promising results to guide revascularization , potentially improving clinical outcomes in stable chest pain patients . 
in view of its diagnostic and prognostic performance , the current european guidelines advocate the use of ccta in patients with suspected cad with a class i recommendation ( level of evidence b ) [ 6 ]  . 
this aligns with previously published guidance document of the 2016 update to the national institute for health and care excellence ( nice ) chest pain guidelines [ 7 ] , whereby ccta is considered as first - line tool for all patients presenting with chest pain of suspected cardiac origthe health economic assessment in the nice guidelines demonstrated that a ccta - guided strategy is the most cost - effective imaging - based strategy [ 7 ]  . 
moreover , a large body of evidence is available indicating that quantification of coronary calcification by means of coronary artery calcium score ( cacs ) is a useful tool for predicting cardiovascular morbidity and mortality in asymptomatic subjects [ 8 ]  . 
the current 64 - slice ccta systems provide relatively high temporal ( up to 66ms ) and isotropic spatial ( ~ 0.20.3mm ) resolution , which allow a good assessment of significant coronary artery stenosis and plaque characterization , with vol . : ( 0123456789 ) 1 3 1136 la radiologia medica ( 2020 ) 125 : 11351147 low radiation dose [ 9 ]  . 
importantly , an additional strength of ccta is the identification of patients with nonobstructive cad , which are associated with an intermediate risk of hard events and may represent the target population of preventive pharmacotherapy [ 10 , 11 ]  . 
newer applications , such as myocardial ct perfusion , ct - derived fractional flow reserve ( ffr - ct ) , and the identification of high - risk plaque features may further refine and improve risk assessment for future cardiac events [ 1215 ]  . 
the aim of the present review is to illustrate the available literature evidence on the prognostic value of ccta for cardiac risk assessment in asymptomatic as well as symptomatic stable chest pain patients . prognostic value ofcoronary artery calcium score coronary artery calcium score ( cacs ) , determined with non - contrast ct , is a highly specific marker of atherosclerotic plaque , and it has been considered a surrogate measure of the total atherosclerotic plaque burden [ 16 ]  . 
 the most widely utilized method for calculation of cacs is the agatston score , first introduced with cardiac - gated electron - beam computed tomography ( ebct ) in the 1990s [ 8 ]  . 
cacs is manually identified and automatically quantified in less than 2min 1 3 la radiologia medica ( 2020 ) 125 : 11351147 1137 observational studies have demonstrated the strong prognostic value of cacs in asymptomatic patients for the prediction of major adverse cardiovascular events ( [ mace ] , i.e. , myocardial infarction [ mi ] , coronary death , and all - cause mortality ) [ 8 , 17 ]  . 
cacs provides consistent predictive information beyond the traditional cardiovascular risk factors and clinical risk scores ( i.e. , framingham risk score or the euro risk score ) in several heterogeneous populations who were followed long tercategories of absolute cacs have been shown to perform better than age - , sex - , and race / ethnicity - specific percentiles [ 18 ]  . 
according to a pooled data analysis from six studies of 27 , 622 asymptomatic patients , the 35year risk of cardiac death or mi was nearly four times higher in patients with any detectable cacs compared with patients without any cacs ( p < 0.0001 ) [ 19 ]  . 
importantly , the patients without detectable calcium ( cacs = 0 ) have a very low rate of cardiac death or mi ( 0.4% ) over 3 to 5years of observation , whereas increasingly higher cacs are associated with increasingly higher risk of hard cardiac events [ 19 ] , table1 . 
the absence of cacs ( cacs = 0 ) has been shown to have a very high negative predictive value ( achieving 99% in most studies ) for ruling out obstructive cad ( also referred to as : the power of zero ) , with excellent prognosis at 15 - year follow - up in asymptomatic individuals at low and intermediate risk , and with no significant differences regarding age and sex [ 21 ]  . 
 however , it is important to bear in mind that the absence of cacs does not mean the absence of atherosclerosis , since non - calcified fibro - lipid plaque could not be detected by unenhanced ccta . 
according to a meta - analysis from 18 studies including 10 , 355 symptomatic patients , the presence of cacs was highly sensitive ( 98% ) in predicting obstructive cad ( defined as luminal stenosis > 50% ; prevalence of 56% ) by invasive coronary angiography , although the specificity was low ( 40% )  . 
the summary negative predictive value was 92% ( range 68100% ) [ 22 ]  . moreover , several large population - based cohort studies such as the heinz nixdorf recall study and the multi - ethnic study of atherosclerosis ( mesa ) have proved that cacs is a strong predictor of cerebrovascular events including stroke in asymptomatic subjects at low - to - intermediate risk , independently of standard risk factors [ 23 ]  . 
moreover , cacs is well known to provide superior discrimination and reclassification beyond other useful markers , such as carotid intima - media thickness , ankle - brachial index , brachial flowmediated dilation , or c - reactive protein [ 24 ]  . 
this highlights the concept that cacs plays an important role in the cardiovascular risk prediction as a marker of total subclinical atherosclerosis . recently , the coronary artery calcium - data and reporting system ( cac - drs ) has been proposed from the society of cardiovascular computed tomography ( scct ) to provide a standardized method ( based on either visual or quantitative assessment ) to communicate findings of cacs scanning on all non - contrast ct scans ( both gated and non - gated ) , irrespective of the indication , with the aim to improve communication of cacs and facilitate clinical decision - making [ 25 ]  . 
a large retrospective observational study on 54 , 678 patients from the coronary artery calcium consortium , followed for over 12years , has demonstrated that cac - drs combining the agatston score and the number of vessels with cacs provides better stratification of risk of cardiac , cardiovascular , and all - cause death than the agatston score alone [ 26 ] , fig.2. 
these prognostic data strongly support new scct guidelines recommending the use of cac - drs scoring . current european and american guidelines incorporate the above evidences and advocate the use of ct for cacs estimation for the clinical risk assessment in appropriate asymptomatic patients . 
the new 2019 american college of cardiology / american heart association ( acc / aha ) prevention guidelines assigned a class iia recommendation ( level of evidence b ) for cacs testing in individuals aged 40 to 75years at intermediate 10 - year risk ( 7.5% to < 20% ) and in selected adults with borderline ( 5% to < 7.5% ) predicted risk to guide individualized management decisions [ 27 ]  . 
in these groups , cacs measurement can reclassify risk upward ( particularly if cacs score is 100 agatston units or 75th age / sex / race percentile ) or downward ( if cacs = 0 ) in a significant proportion of individuals [ 27 ]  . 
 curved multiplanar reconstruction ( mpr ) image of the right coronary artery ( rca ) b and left anterior descending coronary artery ( lad ) c showing the extensive calcification on a per vessel basis . 
the total agatston cacs was 3006 and calcium volume was 2312 , indicating a very high risk of major cardiovascular events of dyslipidemias give a class iib ( may be considered ) recommendation ( level of evidence b ) to cacs as a risk modifier in patients at low or moderate risk [ 28 ]  . 
this indicates that the presence and the extent of cacs may guide the decision to intensify risk factor modification and initiate / implement or defer preventive pharmacotherapy ( i.e. , statin and / or aspirin ) , in view of a better therapy individualization with the aim to improve outcome [ 29 , 30 ]  . prognostic value ofccta : realworld evidence besides the high diagnostic accuracy of ccta in detecting and excluding obstructive cad when compared to invasive angiography , several longitudinal studies have demonstrated that ctca holds important prognostic value in both patients with known and suspected cad [ 3136 ]  . 
 most of the key answers on the prognostic utility of ccta are derived from the coronary ct angiography evaluation for clinical outcomes : an interrnational multicenter registry , or confirm . 
this registry currently includes more than 32 , 000 consecutive adults with suspected cad who underwent 64 - slice ccta at 12 centers in 6 countries between 2005 and 2009 , offering important insights on our understanding on the link between cardiovascular risk factors , symptoms , coronary atherosclerotic plaque burden , and outcome [ 3 ]  . 
the confirm registry has demonstrated that the presence , extent , and severity of cad on ccta result in increased future risk to the patient , across age , gender , and other several clinical sub - analyses [ 3 , 3840 ]  . 
a very low annual event rate for those with normal ccta findings has been consistently demonstrated , which is comparable to the background event rate among healthy low - risk individuals ( < 1% )  . 
the confirm data highlights the clinical importance of nonobstructive cad which comprises a significant number of patients for whom functional testing might be expected to be negativeand its strong relationship with all - cause mortality [ 3 ]  . 
in a way similar for quantification of cacs , a variety of prognostic scores have been proposed to improve the predictive value of ccta , such as the segment stenosis score ( sss ) , which reflects the number of coronary segments with plaque , weighted for stenosis severity ; the segment - involvement score ( sis ) , which reflects the number of segments with plaque irrespective of stenosis severity ; and the modified duke prognostic index - accounting for stenosis severity , plaque distribution , and plaque location [ 41 ]  . 
in symptomatic patients with suspected cad , all these ccta variables adds incremental discriminatory power over cacs for discrimination of individuals at risk of death or acute mi at 25 - months follow - up [ 41 ]  . 
another confirm study in asymptomatic diabetic subjects has demonstrated the value of ccta measures of cad severity in improving risk prediction , discrimination , and reclassification beyond clinical risk factors and cacs [ 44 ]  . 
these findings suggest that ccta may provide further incremental value in appropriately selected cohort of asymptomatic subjects at intermediate - high risk . to date , the factor - 64 trial ( screening for asymptomatic obstructive coronary artery disease among high - risk diabetic patients using ct angiography , following core 64 ) is the only randomized controlled trial evaluating the role of ccta in asymptomatic subjects [ 45 ]  . 
the trial recruited 900 asymptomatic patients with diabetes considered at high risk ( based on age and diabetes duration ) without a previous history or symptoms of cad , who were randomized to either undergo ccta or standard care . 
however , the lack of benefit to ccta arm may be related to the small sample size and unexpected lower event rate , thus the patients in this study were not actually at high risk . 
moreover , the low incidence of adverse events may be related to the excellent preventive therapy of the study population at baseline , with 75% of trial participants already on a statin therapy at baseline . 
 larger forthcoming studies are needed to clarify its potential role in primary prevention . outcomes instable chest pain patients assessed inrandomized controlled trials recently , two large multicenter randomized controlled trials have evaluated the prognostic impact of ccta on outcome , namely the scottish computed tomography of the heart trial ( scot - heart ) [ 4 , 46 ] , and the prospective multicenter imaging study for evaluation of chest pain ( promise ) trial [ 5 , 47 ] , table3 . 
the scot - heart recruited 4146 patients in scotland with suspected cad who were randomized to standard care ( including exercise - ecg in 85% of cases ) or standard care plus ccta . 
the scotheart trial showed an improvement in clinical outcomes in the ccta group , with a reduction in fatal and non - fatal mi compared to the standard group at both 2years ( hazard ratio [ hr ] 0.62 , 95% confidence interval [ ci ] 0.381.01 , p = 0.0527 ) and 5 years ( hr 0.59 , 95% ci , 0.410.84 , p = 0.004 ) , without an increase in coronary angiography or revascularization [ 4 , 46 ]  . the promise trial recruited 10 , 003 north american patients with suspected cad who were randomized to anatomical testing with ccta or functional testing ( i.e. , nuclear stress imaging , stress echocardiography , or exercise - ecg , respectively in 67% , 23% , 10% of cases )  . 
at 25 - month of follow - up , there were no differences in the composite endpoint of death , non - fatal mi , hospitalization for unstable angina and major procedural complication between the ccta and functional care groups ( hr 1.04 , 95% ci 0.831.29 , p = 0.75 ) [ 5 ]  . 
randomization primary endpoint la radiologia medica ( 2020 ) 125 : 11351147 pre - test probability follow - up ( months ) scot - heart [ 4 , 2015 , 2018 12 in scotland 4146 standard care ( exproportion of 20 , 58 1140 promise [ 5 , 47 ] 2015 , 2017 193 in north 10 , 003 functional testing 25 , 26 america ecg 85% ) ( spect 67% ; se 23% ; ex - ecg 10% ) functional testing in a 2 : 1 ratio ( execg 95% ) patients diagnosed with angina secondary to coronary heart disease at 6weeks composite of allcause mortality , myocardial infarction , hospitalization for unstable angina , or major procedural complication clinical effectiveness : absence of chest pain complaints difference in the change in scores within the saq domains from baseline to 3months angina - specific health status crescent [ 48 ] 2016 4 in the netherlands capp [ 49 ] 2015 1 in uk ex - ecg min etal . 
number , ex - ecg exercise stress electrocardiography test , spect singlephoton emission ct , se stress echocardiography , saq seattle angina questionnaire management of patients with suspected cad with ccta is safe and non - inferior to functional imaging . 
moreover , by identifying nonobstructive cad ( 169% stenosis ) , ccta can identify an at - risk group of patients , in which the majority of events ( 54% ; 3.0% event rate ) in the ccta arm occurred . 
in contrast , most of the events in the functional arm group ( 57% of all events ) occurred in those with completely normal functional tests ( 2.09% event rate ) , with a lack of increment in risk between normal and mildly abnormal stress test findings [ 47 ]  . 
these indicate that a significant risk burden may be undetected by functional arm . the recent dutch multicenter randomized crescent trial demonstrated that a tiered cardiac ct protocol , which include a cacs scan followed by ccta if the cacs was in the range of 1 - 400 , is a safe alternative strategy to functional testing ( represented by exercise - ecg in 95% of cases ) among stable angina patients [ 48 ] , table 3 . 
two smaller randomized controlled trials , the capp ( cardiac ct for the assessment of pain and plaque ) trial ( n = 448 ) [ 49 ] , which compared ccta and exercise - ecg , and the study by min etal . 
moreover , the evidence derived from large registry studies and randomized controlled trials confirmed that a ccta - guided management can lead to a change in treatment and improve use of preventive therapy such as statin , aspirin , and ace - inhibitors [ 10 , 50 , 52 ]  . 
however , a major strength of ccta is its excellent negative predictive value that would allow for the deferral or cessation of unnecessary medical treatment for patients who have normal coronary arteries [ 29 ]  . 
indeed , in the confirm study , the use of statin therapy at baseline was associated with reduced mortality only for patients with nonobstructive cad , but not in patients with normal coronary arteries [ 11 ]  . recently , the conserve trial , a multinational , randomized clinical trial of patients referred to invasive coronary angiography ( ica ) for nonemergent indications , randomized 808 subjects to a routine ica and 823 subjects to a selective referral for ica after initial ccta [ 53 ]  . 
importantly , rates of normal ica were 24.6% in the selective referral arm compared with 61.1% in the direct referral arm of the trial ( p < 0.001 ) [ 53 ]  . 
these highlight that ccta can be an effective and safe gatekeeper for cardiac catheterization procedures in stable chest pain patients . recently , the ischemia ( international study of comparative health effectiveness with medical and invasive approach ) trial failed to show that routine invasive therapy reduces the mace rate compared with optimal medical therapy among patients with stable ischemic heart disease and moderate - to - severe ischemia on non - invasive stress testing [ 54 ]  . 
according to the algorithm of the trial , a blinded ccta was performed in most enrolled patients to identify and exclude participants with either significant unprotected left main disease or those with nonobstructive cad . 
in particular , the ischemia trial confirmed the ccta reliability as a good gatekeeper to invasive angiography ( 434 patients were screened out because ccta showed left main disease as well as 1218 patients were excluded for having no obstructive cad despite chest pain symptoms ) , highlighting the importance of ccta vessel disease evaluation before conservative initial management [ 54 ]  . ccta plaque characterization andoutcomes several studies have demonstrated that specific coronary plaque characteristics are correlated with vulnerable plaques at risk of rupture , which confers a significantly heightened risk of acute coronary syndrome ( acs ) [ 12 ]  . 
 these high - risk features include the low - attenuation plaque , positive remodeling , spotty calcification , and the napkin ring sign [ 12 , 55 ] , fig.3. 
 have shown in 1168 patients with suspected cad that low - attenuation plaque volume ( density < 30 hu ) , total non - calcified plaque volume ( < 150 hu ) , napkin ring sign and remodeling index were all predictors of mace at 5.7years follow - up [ 57 ]  . 
the strongest association was observed for low - attenuation plaque volume ( hr 1.12 , p < 0.0001 ) as measured by semi - automated technique , which improved the prediction of the model based on morise score , agatston score , and sss [ 57 ]  . 
moreover , specific plaque compositions including positive remodeling and non - calcified plaque volume have been recently shown to predict ischemia independent of stenosis severity as compared to invasive ffr and quantitative myocardial perfusion obtained using [ 15o ] h2o positron emission tomography ( pet ) [ 58 ]  . 
a recent meta - analysis demonstrated that the risk of future acs was significantly higher in high risk than in low - risk plaques ( hr 12.1 , 95% ci : 5.2428.1 ; p = 0.0001 ) [ 59 ]  . 
accordingly , a recent post hoc analysis of the scot - heart trial demonstrated that the low - attenuation plaque burden ( i.e. , % plaque to vessel volume ) was the strongest predictor of fatal or non - fatal mi irrespective of cardiovascular risk score , cacs , or coronary artery area stenosis ( hr 1.60 , 95% ci : 1.102.34 per doubling ; p = 0.014 ) [ 61 ]  . 1 3 1142 la radiologia medica ( 2020 ) 125 : 11351147 fig . 
curved multiplanar reconstruction ( mpr ) ct image of the right coronary artery ( rca ) ( a ) showing long circumferential non - calcified plaque with positive remodeling and spotty calcium at the proximal segment ( arrow in a ) , with the corresponding orthogonal view ( b ) , and eccentric non - calcified plaque with the napkin ring signi.e. , a ring of high attenuation around a central low - attenuation areaat the midsegment ( asterisk in a ) , with the corresponding orthogonal views ( e , f )  . 
curved multiplanar reconstruction ( mpr ) image of the left anterior descending coronary artery ( lad ) ( c ) showing proximal non - calcific plaque with napkin ring sign and spotty calcification ( white arrowhead in c ) , with the corresponding orthogonal view ( g ) , causing irregular lumen without significant stenosis . 
angiographic evaluation of the rca ( d ) and lad ( h ) performed at 10 - month follow - up after the onset of precordial pain due to ulceration of the plaque at the proximal lad ( h , black arrowhead )  . 
l : vessel lumen functional evaluation withmyocardial ct perfusion andffrct new generation ct scanners 64 slices enable static ( single - phase ) and dynamic ( multiphase ) myocardial ct perfusion ( ctp ) with both qualitative and quantitative assessment of perfusion parameters of ischemia , such as the myocardial blood flow and volume [ 62 ]  . 
computational fluid dynamics ( cfd ) algorithms could enable prediction of changes in coronary flow and pressure for the non - invasive estimation of ffr ( ffr - ct ) [ 62 , 63 ]  . 
several studies and first randomized prospective trials have demonstrated that ccta combined with perfusion imaging or ffr - ct could have huge potential to evaluate both morphology and functional significance of stenosis , as a one - stop shop non - invasive modality . 
the core320 demonstrated that a combined approach with coronary ctca and ctp enables similar prediction of 2 - year major adverse cardiac events and event - free survival , when compared to that provided by combining invasive coronary angiography and spect [ 64 ]  . 
moreover , stress dynamic ctp has incremental predictive value for future major adverse cardiac events over clinical risk factors and the detection of coronary stenosis at ccta [ 62 , 6567 ]  . 
finally , ffr - ct , besides an improved accuracy for the detection of hemodynamically relevant lesions , may have favorable clinical 1 3 la radiologia medica ( 2020 ) 125 : 11351147 1143 fig . 
myocardial spect polar bulls eye map showing no significant perfusion defects in the territory of the left anterior descending coronary artery but inducible ischemia in the territory of the right coronary artery and left circumflex coronary artery ( b , d )  . 
ivp : posterior interventricular coronary artery ; pl1 and pl2 : first and second posterolateral branch , respectively ; da : anterior descending coronary artery ; d1 : first diagonal branch ; mo : obtuse marginal branch ; cx : circumflex coronary artery outcomes , similar quality - of - life , and lower costs and radiation exposure , when compared with usual care over 1 - year follow - up [ 62 , 68 , 69 ]  . outcomes inacute chest pain patients assessed inrandomized controlled trials several prospective single - center studies and randomized controlled trials have demonstrated the prognostic value of ccta in the context of acute chest pain patients with lowto - intermediate risk of acs ( thrombolysis in myocardial infarction [ timi ] risk score 04 ) table4 [ 7081 ]  . 
many trials focused on efficiency of ccta - based strategy demonstrating a benefit in terms of length of stay and the costs of acute care [ 70 , 71 ]  . 
however , most of the trials occurred prior to the adoption of high - sensitivity tropon according to a recent meta - analysis , the ccta approach has been proven to have a similar outcome compared to other standard - of - care approaches in all - cause mortality , mace and mi [ 71 ]  . 
therefore , ccta appears to be a safe and viable alternative to standard - of - care approach , although a significantly increased use of invasive coronary angiography and revascularization with ccta - based strategy has been observed [ 71 ]  . 
curved multiplanar reconstruction ( mpr ) of the right coronary artery ( rca ) ( a ) and of the left anterior descending coronary artery ( lad ) ( b ) showing a non - calcified plaque with intermediate stenosis at the middledistal rca and mixed plaques with positive remodeling causing two obstructive stenoses on proximal and middle - distal lad , confirmed by invasive coronary angiography ( arrows , f )  . 
note the first pass hypoperfusion of the septum ( arrowheads in c and e ) and of the inferior left ventricular myocardium ( arrowhead in d ) , color - coded in blue at the myocardial ct perfusion maps table 4 randomized controlled trials of prognostic value of ccta in acute chest pain patients with low - tointermediate risk trial year patients no . randomization soc follow - up ( months ) goldstein etal . 
the ccta offers a series of advantages by combining in a single technique the accurate assessment of coronary anatomy , plaque morphology , atherosclerotic plaque burden , and coronary flow . 
comprehensive cad assessment by advanced medical imaging such as radiomics , machine learning , and deep learning [ 82 ] will further increase the amount of information extracted from ct datasets . 
in this paper are described role and techniques in diagnosis of ischemia , myocardial infarction and its sequelae . keywords cardiac magnetic resonance ischemic heart disease stress perfusion cardiac magnetic resonance myocardial infarction introduction despite the high incidence of acute myocardial infarction in the world , new therapies and new imaging modality have increased survival and reduced cardiovascular events . in italy , acute myocardial infarction ( ami ) entails an in hospital mortality of 4.12% and 1 - year mortality of 10% . cardiovascular magnetic resonance ( cmr ) has been always more often used in the last 10years in evaluation of many end point due to its peculiar features that represent surrogate markers of end points itself [ 1 , 2 ]  . definition ofmyocardial infarction definition of myocardial infarction ( mi ) has been changed in the course of last 15years . 
the fourth universal definition of myocardial infarction ( fudmi ) published in 2018 underlines new concepts in order to differentiation between myocardial infarction and myocardial injury and , among others , * vitaliano buffa vbuffa@scamilloforlanini.rm.it paolo di renzi padire57@gmail.com 1 department ofradiology , azienda ospedaliera san camillo 2 department ofradiology , ospedale san giovanni calibita forlanini , rome , italy fbf , rome , italy in order to highlight peri - procedural myocardial injury after cardiac and noncardiac procedures as discrete from myocardial infarction . 
in the new fudmi , cardiovascular magnetic resonance ( cmr ) is now clearly considered in the assessment of myocardial injury [ 3 ]  . myocardial injury , defined by an elevated cardiac troponin ( ctn ) value above the 99th percentile upper reference limit ( url ) , is frequently encountered clinically and is associated with an adverse prognosis [ 4 , 5 ]  . 
myocardial injury must to be considered as a prerequisite for the diagnosis of mi , but , on the other hand , it is to be considered a separate specific entity . 
nonischemic myocardial injury may arise secondary to many cardiac conditions such as myocarditis , heart failure , or may be associated with noncardiac conditions such as renal failure [ 6 ] and in a patient with symptoms and increased cardiac troponin ( ctn ) values , it is mandatory to distinguish between nonischemic myocardial injury and one of the mi subtypes . 
finally , in the cited fudmi consensus document new sections have been added due to the clinical impact they represent as , among others , takotsubo cardiomyopathy ( ttc ) , and myocardial infarction with nonobstructive coronary artery disease ( minoca )  . 
cine sequences allow an optimal evaluation of myocardial kinesis and wall thickening / thinning , an accurate evaluation ( actual gold standard ) of ventricular volumes , ventricular masses and systolic function of both ventricles [ 7 ]  . 
on the other hand , many studies have confirmed the reliability of cmr in the assessment of lvef and its prognostic impact as an independent predictor of mace since its advent in the clinical scenario [ 8 , 9 ]  . furthermore , the relatively recent advent of feature tracking and tissue tracking allows a simple method to improve the assessment of systolic and diastolic function in the analysis of myocardial strain using the cine - rm stack in short and long axis . 
evaluation of the three myocardial component of strain ( circumferential , longitudinal and radial ) improve the accuracy in detecting myocardial dysfunction if compared to global levf and qualitative analysis of kinesis not only at level of area of myocardial infarction but also at level of remote myocardium that contributes to ventricular remodeling . 
 once again , although this field of application is usually relevant for echocardiography , cmr may play an important and alternative rule in the assessment of myocardial straglobal longitudinal strain was demonstrated to provide strong validity for the prediction of major adverse cardiovascular events ( mace ) post - stemi , incremental to lv ejection fraction and infarct severity markers [ 10 ]  . the use of contrast media with late gadolinium enhancement ( lge ) allows to define the amount of myocardial damage ( in the acute phase due to cellular death and increased interstitial edema and in chronic phase due to the increased extracellular space )  . 
once the myocardial damage ( loss or rupture of myocardial cells ) in the acute phase has settled , the gadolinium administration allows , after about 1020min , to assess the infarct size ( is ) that is normally expressed as percentage loss of global myocardial mass . 
the extension of is may be performed by means of qualitative ( manual ) analysis as well as semi - quantitative methods based on 26 standard deviation of remote myocardium signal or full width at half maximum ( fwhm )  . 
the latter seems to be the best choice due to better inter and intra - observer variability , less overestimation of is in case of contemporaneity edema and less partial volume effects as well as agreement with lvef . 
despite the entity of is may vary rapidly in few days lge evaluation of is has been emphasized and recommended as primary cmr endpoint measure in experimental and clinical trials [ 11 ]  . in the acute phase has a great importance the use of triple inversion recovery t2 ( t2w stir ) sequences that allow to evaluate the extend of myocardial edema that is the first consequence of myocardial ischemia and that is a potential reversible phenomenon . 
alternative evaluation of aar may be performed by contrast - enhanced cine mr sequences in order to overcame some intrinsic limits of stir sequences ( low signal - to - noise ratio , motion artifacts and incomplete blood suppression )  . 
in stir images lge in same sites ( green arrows ) la radiologia medica ( 2020 ) 125 : 11141123 microvascular injury as known , even in case of rapid pci and reperfusion therapy and optimal restore of myocardial coronary flow , microvascular injury occurs in a considerable number of ami ( specially in case of stemi )  . 
cmr allows to correctly assess the two major processes linked to microvascular injury : microvascular obstruction ( mvo ) and intra - myocardial hemorrhage ( imh )  . mvo or no reflow refers to the small vessel changes and is thought to be caused by an abrupt release of cytotoxic factors inducing vasoconstriction , myocardial cellular edema , capillary endothelial cells swelling and distal microembolization of atherosclerotic debris and begins in the infarcted core and can increase in size for up to 48h [ 13 , 14 ]  . the best technical choice for mvo is still lge which underlines its extension as a hypointense area inside the bright area of lge . 
in fact , mvo is associate with worse systolic and diastolic function , larger is , lack of functional recovery , adverse remodeling ( an increase in lv end - diastolic volume 20% at 6months from baseline ) even in case of preserved lvef at the onset of ami [ 14 , 15 ]  . 
the crucial role of mvo has been recently emphasized with the observation that every 1% of increment of mvo is associated with a relative increase of 14% and 8% in terms of mortality and hospitalization for heart failure , respectively [ 16 ]  . in the last years , the use in the clinical scenario of parametric imaging ( t1 mapping , extracellular volume , t2 mapping and t2 * mapping ) has increased the diagnostic capability in the assess of diffuse fibrosis . 
recently , its use has been proposed also in the evaluation of ami due to the fact that in case of infarcted and edematous myocardium there is a prolonged pre - contrast t1 values and reduced post - contrast t1 values compared with normal myocardium , allowing infarct visualization and quantification [ 1719 ]  . despite the completely different physical basis ( evaluation without and with contrast media injection ) , native t1 mapping has been proposed in comparison with mvo in the evaluation of core infarct of 288 stemi patients [ 20 ]  . 
on the other hand , parametric imaging plays a pivotal role in the assess the other major finding of microvascular injury , imh . 1 3 la radiologia medica ( 2020 ) 125 : 11141123 1117 at the same time , the evaluation of remote myocardium ( rm ) in the course of ami may play an important role . 
furthermore , some authors have demonstrated , using cmr in early phase of reperfused ami and after 6months that the increase of ecv was correlated with increasing of lv end - diastolic volumes . 
these data open new diagnostic possibilities about patho physiologic assessment on left ventricular dysfunction and myocardial remodeling in after ami [ 2123 ]  . in case of severe microvascular injury and delayed reperfusion therapy , imh is almost present inside the is . 
 mvo may lead to endothelial damage with leakage of red cells into the interstitial space , leading to imh or imh may occur as a part of ischemia reperfusion injury and hemorrhage leading to greater myocardial swelling and compression of microvasculature with worse mvo [ 24 ]  . on the basis of published results , imh is more closely associated with mace than mvo [ 25 , 26 ] and the presence of imh has an incremental worse prognostic significance in comparison with ami without mvo and in ami with mvo . 
 microvascular injury depicted by mvo and imh is an important finding in the early prognostic assessment on ami and their presence assumes a worse outcome . in comparison with standard assessment of ami ( grace score , ctn and echo - based lvef ) , cmr technical options have stimulated the development of scores for risk stratification . 
integration of cmr - based lvef , is , msi and mvo are potential powerful option in order to obtain more prognostic information on the adverse outcome of ami [ 27 , 28 ]  . additional findings other important findings obtainable by the use of cmr in the acute phase of ami and to be considered for prognostic implications are left atrial function and strain [ 29 ] , presence or not of thrombus in the left ventricular cavity [ 30 ] , pericardial effusion [ 31 ] and right ventricular infarction and function [ 32 ]  . 
the use of cine - rm ( and strain ) , stir ( and t2 / t2 * mapping ) and lge sequences allow to evaluate these particular findings which have demonstrated to assume a prognostic value . differential diagnosis formyocardial injury intheacute phase as mentioned above , in last fudmi have been underlined two causes of myocardial injury often in differential diagnosis with ami . takotsubo cardiomyopathy ( ttc ) or transient left ventricular apical ballooning syndrome often mimic ami despite its incidence is about 12% of ami but mortality is quite similar to the latter ( 45% )  . 
cmr shows myocardial edema , parietal wall abnormalities and usually absent lge pattern and it is routinely used when a patient ( usually female ) shows symptom of ami , negative coronarography and parietal wall abnormalities [ 33 ]  . also in minoca the use of cmr has grown significantly due to abovementioned characteristics ( morphofunctional and tissue substrate )  . 
there is the need of exclude all causes of ctn increase , to overlook obstructive coronary disease and to exclude nonischemic causes for myocite injury ( in primis myocarditis )  . 
 many studies have demonstrated that cmr allows a definitive diagnosis in 71% of minoca and for this reason cmr within 4weeks after hospital admission is recommended [ 34 ]  . chronic myocardial infarction ( cmi ) contrast - enhanced cmr plays an important role in cmi by the use of lv functional analysis , perfusion abnormalities and the presence of scar with lge . in the clinical scenario , cmr may be requested for evaluate viability ( contractile reserve with potential recovery ) , for late complications of ami ( thrombi and aneurysms / pseudo - aneurysms ) and to distinguishing chronic mi from other nonischemic cardiomyopathies , particularly in case of congestive cardiac failure . cine mr sequences allow to evaluate function and thinning of parietal wall in the affected coronary territory . 
 1 3 1118 la radiologia medica ( 2020 ) 125 : 11141123 cardiac magnetic resonance perfusion imaging intheevaluation ofischemia cardiac magnetic resonance ( cmr ) has a defined role in the assessment of ischemic heart disease . 
in addition to morphological - functional evaluations related to acute myocardial infarction and its sequelae ( impairment of contractility , myocardial remodeling , fibrosis ) , cmr is an accurate test for diagnosis of ischemia induced by physical or pharmacological stress in the presence of coronary stenosis or microvascular alteration . recent guidelines have identified a second - line role for functional myocardial perfusion imaging ( mpi ) after ct , in assessment of patients with high probability of coronary artery disease ( cad ) or as gatekeeper for coronarography [ 39 ] , in this setting placing as the main competitor of the myocardial perfusion spect ( mp - spect ) [ 40 ]  . 
many trials show , however , that mri , over a tool for identifying ischemia , it also has a prognostic value and can be a surrogate of invasive frr in the definition of patients with chronic coronary syndrome to undergo angioplasty . assessment of cardiac flow reserve ( cfr ) , the rate of cardiac blood flow ( cbf ) in stress and rest condition , is on basis for diagnosis of ischemic cardiopathy . 
the regulation of coronary flow takes place at various levels , especially at the level of pre - intermediate arterioles and intramural arterioles , responding , respectively , to pressure or to demand for oxygen , basically with vasodilation . 
the self - regulatory mechanisms of cbf can be altered in the presence of epicardic coronary stenosis or microvascular damage , resulting in an inefficient oxygen support to the myocardial that triggers ischemic cascade and symptoms [ 41 , 42 ]  . the myocardial concentration of the paramagnetic contrast media and consequently the signal intensity reflects both the intravascular concentration and the dilation of the microvascular bed and therefore changes under conditions of myocardial stress . the alterations induced by ischemia ( electric , kinetic ) are the basis of non - invasive exercise ecg - testing and stress echocardiography , while cmr identifies the perfusion defects as well as kinetic alterations . the alteration of perfusion can be analyzed both qualitatively and quantitatively through post - processing techniques ( discrepancy of intensity between cardiac segments , time - intensity curve )  . volumes and lvef assessed by cmr represents the gold standard . 
a wall thinning lower to 5.5mm is a marker of nonviable myocardiufurthermore , a percentage thickening of less than 30% is correlated with reduced cine - rm evaluation , associated to lge images , is a robust tool also in order to evaluate thrombus and aneurysm ( or pseudoaneurysm due to rupture of a wall buffered by pericardial reaction ) , often associated , as consequence of extensive mi ( usually apical - antero - septal ) and in anticipation of surgical treatment . increase of extracellular interstitial volume due to collagenous scar may be optimally evaluated by lge . 
in chronic phase is expressed as degree of transmurality ( 025% , 2650% , 5175% , 76100% ) as well as loss of lge myocardial mass ( lge mass / total lv mass ) are simple and accurate methods in order to evaluate potential effect of revascularization therapy . 
in lge images , a transmurality up to 50% may be a good assumption for recovery [ 35 ]  . the accurate evaluation cmr allows of lge scarring can predict survival and all - cause mortality independent of lv ejection fraction , predicts adverse lv remodeling and can predict ventricular tachycardia in comparison with lv ejection fraction or volumes , as scars are a substrate for arrhythmia [ 36 ]  . a peculiar clinical aspect cmr plays an important role due to high sensitivity of lge images is on evaluation of unrecognized mi . 
the presence of even a small scar in patients without a history of mi is associated with a high risk of adverse events and presence of even minimal lge presence represent a stronger predictor of outcomes than other evaluations even based on catheterization data [ 37 ]  . technical developments on t1 and t2 mapping , strain , dark blood lge are already availed and used . 
their obvious next more extensive application in the clinical scenario will allow to better evaluate acute and chronic myocardial infarction , to increase prognostic impact of cmr and to prepare the road to deep learning [ 38 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 11141123 1119 scan protocols myocardial perfusion study consists in visualization of progressive uptake ( wash - in ) and dismission ( wash - out ) of contrast media after bolus injection with high temporal resolution sequences , in condition of pharmacologicalinduced stress . 
continuous acquisition of 35 planes ( at least 3 short axis or a combination short axis and long axis ) is achieved on multiple heartbeats ( typically at least 5060 heartbeats ) , covering all ventricular segments , with a prepulse to minimize signal intensity of myocardium , triggered on qrs complex . first pass study is a part in a comprehensive cmr study including evaluation of cardiac kinetics under stress and classical morphological and functional parameters ( cine short - axis images ) and stir images for late gadolinium enhancement ( lge )  . 
wa 12 - lead electrocardiogram is usually performed before and after the study with continuous monitoring of pressure and ecg . sequences sequences for perfusion imaging are various and include steady state free precession ( ssfp ) , gradient - echo ( gre ) , hybrid gre - echo planar imaging ( epi ) , steady state free precession ( ssfp )  . 
critical factors influencing the image quality are temporal resolution , acquisition window spatial resolution anatomic coverage and high t1 - signal . temporal resolution determines the time between the image acquisition of the same plane , to identify the modification of signal intensity . 
in plane resolution has to be less than 3mm with readout temporal resolution of 100125ms or shorter [ 4346 ]  . contrast media standardized bolus administration ( 0.050.1mmol / kg at injection speed approximately 25ml / s ) is mandatory to obtain adequate signal intensity of myocardium on first pass images , followed by a bolus saline flush . 
dobutamine is administrated in graded doses starting at 5g / kg / min and increasing at 3 - min intervals to 10 , 20 and 30 with a maximum dose of 40g / kg . 
in relation to the inotropic activity , dobutamine can be used , at lower doses , for the evaluation of myocardial viability [ 49 ]  . adequate stress for starting contrast media administration and image acquisition is considered when cardiac rate rise is of 10 or more heartbeats / min and / or pressure drops of 10mmhg [ 43 ]  . 
this standardized method not always guarantee the correct grade of hyperemia to detect perfusional defect and inadequacy of pharmacologic induction of stress ( for interaction , ad ex with caffeine or beta - blockers , or inadequate administration ) is potential cause of elevate rate of false - negative results . 
a good parameter of quality in the post - procedural evaluation , when adenosine is used , is considered the splenic with - off criteria , the inversion of signal intensity of the spleen ( darker in stress images compared to rest images )  . 
failed splenic switch - off is common finding in false - negative stress cmr [ 50 ]  . image interpretation the evaluation of perfusion is usually performed in a qualitative manner and can be performed in a semi - automatic or automatic manner . 
 presence of late gadolinium enhancement is relative to postnecrotic fibrosis and is expression of low vascular supply of fibrotic tissue and is associated to a non - reversible perfusion defect . 
 occlusion of right coronary artery ( white arrow ) with hypertrophied collateral vessel ( green arrow ) la radiologia medica ( 2020 ) 125 : 11141123 dark rim artifact ( dra ) , principally a susceptibility magnetic artifact , can be confused with genuine perfusion defect . 
high concentration contrast media bolus and limited spatial resolution are the common causes [ 51 ]  . quantitative assessment the analysis of upslope of myocardial wash - in can be obtained with dedicated software that identifies segmental increasing of signal intensity . 
automated quantitative assessment is a new promising tool in the quantification of ischemia . diagnostic performance the accuracy of cmr in the diagnosis of ischemic heart disease is high , both in relation to coronary artery and to functional examinations , in particular spect . 
increased accuracy has shown studies with adenosine as stress vs dipyridamole , and 3t equipment towards 1.5 t , positive likelihood ratio 4.184.43 and negative likelihood ratio 0.120.15 [ 52 54 ]  . 
this study indicates mri as a selection criterion for patients to be initiated to revascularization . prognostic role is described in meta - analysis of lipinski ( 11.636 pts ) [ 62 ]  . 
 due to its noninvasive ability to detect the presence of myocardial edema , hyperemia and necrosis / fibrosis , cardiac mr imaging is routinely used in the clinical practice for the diagnosis of acute myocarditis . 
our paper will review the role of mr imaging in the diagnosis of acute myocarditis . keywords myocarditis myocardial inflammation cardiac mr magnetic resonance imaging introduction in 1995 the world health organization ( who ) / international society and federation of cardiology ( isfc ) defined myocarditis as an inflammatory disease of the heart muscle , diagnosed by histological , immunological , and immunohistochemical criteria [ 1 ]  . myocarditis diagnosis is often challenging because of the heterogeneity of clinical presentations . 
the real incidence of myocarditis is difficult to work out as endomyocardial biopsy ( emb ) , the diagnostic gold standard , is employed infrequently [ 13 ]  . several published studies report a highly variable autopsy variation . prevalence of myocarditis ( 242% )  . thanks to its unique ability to directly image myocardial necrosis , fibrosis and edema , cardiac magnetic resonance * iacopo carbone iacopo.carbone@uniroma1.it 1 radiology unit , ospedale del marea.s.lna1 - centro , 80147 , naples , italy 2 department ofmedical andsurgical specialties , radiological sciences , andpublic health , university ofbrescia asst spedali civili ofbrescia , brescia , italy 3 department ofprecision medicine , university ofcampania luigi vanvitelli , 80138naples , italy 4 department ofradiological , oncological andpathological sciences , sapienza university ofrome , i.c.o.t. 
eosinophilic - lymphocytic myocarditis can also occur after smallpox vaccination [ 7 ]  . autoimmune diseases with systemic implication such as churg - strauss syndrome or hypereosinophilic syndrome ( loefflers disease ) can be associated with eosinophilic myocarditis . 
murine models of enteroviral myocarditis suggest that the course of viral myocarditis is characterized by 3 phases , which might be simplified as follows [ 10 ] : the entry of the virus into the myocytes , mediated through a specific receptor is responsible for acute cell injury , induced by virus replication leading to necrosis , exposure of intracellular antigens like cardiac myosin and activation of the hosts immune system , which is characterized by the invasion of natural killer cells and table 1 etiological causes of myocarditis in relation to literature data macrophages followed by t lymphocytes . 
in the case of viral agents , a respiratory or gastrointestinal syndrome , with or without increased systemic inflammatory markers and fever , may precede ( days or weeks ) the clinical onset of cardiac signs and symptoms . fulminant forms , presenting with unexplained acute heart failure . chronic forms ( about 25% of myocarditis ) manifest with persistent cardiac dysfunction and in 1225% may progress to end - stage inflammatory dcm . 
in these cases , patients present with symptoms of chronic or acute heart failure ; more severe forms meet the indications for heart transplantation [ 12 ]  . cmr targets ofmyocarditis cmr is able to identify 3 diagnostic targets during an acute inflammatory process of the myocardium : edema , hyperemia , and necrosis or fibrosis ( table2 )  . 
these 3 targets were proposed for the diagnosis of acute myocarditis by the first consensus on cmr in myocardial inflammation in 2009 , the lake louise criteria ( llc ) [ 13 ]  . since their introduction the llc were used by the majority of centers in the world in their daily clinical practice and have changed the clinical management of patients with a suspect of acute myocarditis [ 13 ]  . edema is the hallmark of inflammation in all soft tissues . 
more in detail , in the setting of myocarditis , edema results from an imbalance between microvascular filtration , induced by microvascular endothelial barrier dysfunction , and lymphatics fluid removal ; it is both intracellular and interstitial and can persist for several months [ 14 ]  . on cmr , the increased tissue water content causes prolongation of both t1w and t2w relaxation times . edema can be assessed with traditional t2 - weighted imaging and by means of t2 mapping techniques . 
on stir t2 - w images edema can be detected qualitatively but should always be assessed with t2 ratio : comparing the signal of the entire myocardium with the intensity of skeletal muscles on the same image . 
on cmr , this mechanism can be evaluated using the early gadolinium enhancement ( ege ) technique , which consists in measuring the early contrast uptake of the myocardium acquiring t1w images within the first minutes after the administration of gadolinium - based contrast agent . 
 signal intensity of the myocardium can be normalized to a normal skeletal muscle : in this case , a ratio of 4 or more is considered indicative of myocardial inflammation . 
alternatively , avoiding normalization , myocardial inflammation may be suggested by signal increase of the myocardium higher than 45% compared to pre - contrast scan . necrosis or fibrosis are both consequences of prolonged or severe tissue damage . 
mapping is complementary to lge because it enables to detect milder and more diffuse fibrosis . in the setting of clinically suspected myocarditis , according to the llc , myocardial inflammation can be diagnosed if at least two out of the three above mentioned cmr criteria are present . 
left ventricular ( lv ) dysfunction and / or pericardial effusion , common in these patients , are considered ancillary findings . diagnostic accuracy ofcmr the original lake louise criteria [ 13 ] provided a good overall diagnostic performance , better than any of the individual cmr parameters , and after 10years of application , their sensitivity , specificity and da in the clinical suspect of acute myocarditis increased from 67% , 91% and 7880% , 87% and 84% , respectively [ 16 ]  . 
consequently , they should remain in use in centers that have good experience with their application . however , llc seems to perform better in myocarditis with infarct - like presentation compared to cases manifesting with heart failure or arrhythmias ( se = 80% vs 57% and 40% , respectively ) [ 17 ]  . 
due to this drawback and to the increasing clinical potential of pixel - wise mapping of t1 and t2 relaxation time , in 2018 , lake louise criteria have been updated . 
pericardial effusion in cine cmr images or high signal intensity of the pericardium in lge , t1 mapping or t2 mapping to detect pericardial inflammation and systolic lv wall motion abnormality in cine cmr to detect lv dysfunction are considered supportive criteria . 
1 a 57 year old female with sudden onset of retrosternal chest pat2 - w stir image shows an hyperintense subepicardial rim representing myocardial edema in the inferior wall of the lv ( arrow )  . 
mapping images confirm the findings of acute myocardial inflammation : t2 mapping value is higher than 60ms ; nt1 value is higher than 1100ms and ecv is higher than 32% . 
 the diagnosis of acute myocarditis cannot be obtained with the original llc ( 0 criteria out of 3 ) , but is provided by applying the revised llc ( 2 criteria out of 2 ) the revised llc is a free gadolinium protocol , when the injection of gadolinium is contraindicated ( e.g. , : patients with an history of allergic reaction to gadolinium - based contrast media ; pregnant women ; patients with end - stage renal insufficiency )  . due to the recent introduction of the revised llc into clinical practice , to be best of our knowledge there is only one prospective study investigating their diagnostic yield [ 18 ]  . 
diagnostic accuracy improves significantly combining parameters two by two , as recently reported by ferreira and coworkers in a meta - analysis available as supplemental material of the revised llc paper [ 19 ]  . 
the position statement of the european society of cardiology suggests the need for long - term follow - up of patients , including those presenting with infarct - like symptoms and no lv functional 1 3 la radiologia medica ( 2020 ) 125 : 11241134 1129 fig . 
cmr scan performed in the acute phase ( upper row ) shows hypersignal of the septum and mid - apical lateral wall , mirrored by prolonged t2 on mapping ; these findings are consistent with edema . 
early follow - up scan obtained 30 days later shows normalization of t2 and regression of the enhancement of the myocardium ; near complete resolution of the pericardial effusion impairment ; timeline and modalities of the follow - up schedule , though , are not specified [ 5 ]  . 
echocardiography provides accurate assessment of lv and right ventricular function [ 21 ] , but is outperformed by cmr for the evaluation of structural abnormalities of the myocardium . cmr may play a role in the stratification of the prognosis : two recent meta - analyses proved that lvef and lge are strong predictors of major adverse cardiac events ( mace )  . 
cut - off values of lge ( 17 grams , or 13% of myocardial mass ) [ 22 , 23 ] were associated with mace , although such thresholds are not validated for routine application in clinical practice . 
noticeably , in a group of 203 patients with biopsy - proven acute myocarditis , none of the patients with lge had sudden cardiac death in the long term , regardless of lvef or lv dilatation . 
lge persists , although its extent may decrease : it is unclear whether partial regression has clinical significance or not . thus far , there are no evidences on the prognostic value of any of the modern quantitative techniques ( t2 , t1 and ecv mapping )  . 
relaxation times of the myocardium are influenced by a number of factors ( vendor , type of sequence , and homogeneity of the magnetic field ) that affect reproducibility and comparability of the results in different studies . myocardial inflammation andcovid19 during the current sars - cov2 pandemic several cases of covid - 19 myocarditis were observed , some of which fatal [ 24 ]  . 
furthermore , cases of myocarditis were reported during the previous outbreaks of sars and mers - cov [ 25 , 26 ]  . similar to other viral agents , the pathophysiology of covid - 19 myocarditis is the result of both cell infection damage and ( auto ) immune reaction . 
sars - cov - 2 enters human cells binding its spike protein to angiotensin - converting enzyme - 2 ( ace - 2 ) , which can be found on the membrane of epithelial respiratory cells , cardiomyocytes and pneumocytes ( type - 2 )  . activated t - cells are responsible for cell - mediated cytotoxicity . 
noteworthily , cytokine storm , which is known to exacerbate the clinical course of covid - 19 , promotes the activation of t - cells , which releasing cytokines maintain the exaggerated immune response . cardiomyocyte injury , pericardial inflammation with effusion and microvascular damage may be the substrate of arrhythmia in covid - 19 myocarditis . 
 there is no data on the performance of the revised llc in this scenario ; however , the myoracer trial showed that , in patients with chronic symptoms , t2 mapping was the only sequence able to differentiate patients with acute myocardial inflammation . chronic myocarditis chronic immune activation may occur in several conditions , including persistence of viral genome in myocytes , autoimmune diseases eosinophilic syndromes and sarcoidosis and may manifest with organ dysfunction . chronic myocarditis tends to occur in older subjects and has more subtle clinical manifestation than the acute for the onset of symptoms occurs generally more than 30days prior to presentation and cardiac biomarkers show minimal abnormalities . 
 [ 17 ] observed it in 28% of patients with cardiomyopathic pattern of presenis there arole forct inpatients withacute andchronic myocarditis ? clinical presentation of myocarditis is heterogeneous thus the assessment of the coronary arteries is often required to rule out acute coronary syndrome . 
multi detector computed tomography ( mdct ) plays a pivotal role in this setting , for its low invasiveness combined with an excellent npv , as high as 99% for significant coronary artery stenosis [ 30 ]  . as the pharmacokinetics of iodinated and gadoliniumbased contrast agents are similar , the technique of late myocardial enhancement could be applied also on mdct scans [ 31 , 32 ]  . from a technical point of view , cmr has a significant fig . 
 clinical findings and ef ( 43% ) suggested acute fulminant for on a follow - up scan ( lower row ) performed 55days later near complete regression of radiological findingsis documented tation , as opposed to 81% of patients with infarct - like presentation . 
overall , the sensitivity and specificity of cmr for chronic myocarditis are significantly inferior to acute advantage over mdct , due to the possibility to null the signal of the myocardium and consequently to increase the conspicuity of hyperenhancing areas . 
on the other hand , mdct is hampered by low signal - to - noise ratio and contrast resolution . decreased tube voltage ( 7080 kvp ) and increased contrast agentvolume may strengthen damagedmyocardial 1 3 la radiologia medica ( 2020 ) 125 : 11241134 1131 fig . 
furthermore , pericarditis may be triggered by direct pericardial injury ( surgery , radiation therapy on the encompassing the mediastinum ) and cardiac damage ( transmural infarct and dressler syndrome )  . 
up to 30% of cases have no defined cause and , consequently , are classified as idiopathic . ct and cmr can equally demonstrate pericardial effusion and pericardial thickening : 4mm thickness is conventionally indicated as the upper limit of normal , although it must be emphasized that pericarditis may be present also fig . 
it has been demonstrated that monochromatic images ( 7090kev ) with optimal energy levels , derived by multi - energetic acquisition , yield better contrast - to - noise ratio than conventional single - energy polychromatic images commonly used for late enhancement [ 33 ]  . similar to cmr , cardiac mdct images acquired in a delayed phase allow to measure myocardial ecv ; the agreement between ecv values provided by these two techniques is good [ 3436 ]  . bouleti and colleagues demonstrated an excellent overall accuracy ( 95% ) of dual energy / spectral ct in the acute myocarditis assessment compared to cmr , in a large population of patients , admitted for chest pain with a final diagnosis of acute myocarditis [ 37 ]  . 1 3 1132 la radiologia medica ( 2020 ) 125 : 11241134 when the pericardium is within normal limits . 
in this condition , the stiffening of the pericardium has effect on ventricular filling : in detail , during inspiration rv filling prevails whereas during expiration lv filling is enhanced . 
cmr , however , permits direct demonstration of functional alterations : real - time cine sequences acquired during free - breathing show flattening of the interventricular septum at inspiration , followed by return of normal convexity at end expiration ( septal bounce )  . conclusion the protean clinical presentation and varied etiology contribute to make myocarditis a challenging diagnosis , in many cases . 
7 cine mri scan on 4 - chamber ( a ) and short - axis ( b ) view , shows circumferential pericardial effusion with multiple linear septa within the pericardial sac , indicating fibrin deposition . 
ct before ( c ) and after contrast ( d ) shows diffuse thickening and enhancement of the pericardium in a patient affected by lung carcinoma 1 3 la radiologia medica ( 2020 ) 125 : 11241134 1133 ethical standards since this is a review article neither human patients nor animals were directly enrolled by the authors . 
for the same reason there was no need to obtain informed consent . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
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according to features classification , n = 5 / 23 features were shape - based , n = 7 / 23 were first - order features , n = 11 / 23 features were classified as gray level run length matrix . 
nine of the selected features showed an auc higher that 0.7 : minimum auc of 0.74 ( 95% ci 0.610.89 ) for sum variance and maximum auc of 0.90 ( 95% ci 0.820.99 ) for zone entropy . conclusion features analysis demonstrated statistically significant differences between normal and pathological nerve . 
 recently , magnetic resonance imaging ( mri ) and ultrasound ( us ) gained a relevant role in the diagnostic work - up of peripheral neuropathies , such as entrapment neuropathies ( en ) [ 13 ]  . 
indeed , these techniques allow detailed evaluation of peripheral nerves architecture consisting of fascicles and surrounding epineurium . in entrapment neuropathies ( en ) , changes in the inner texture due to the alterations of the fascicular pattern have been considered signs of pathology on both mri and us [ 413 ]  . 
 the most common en are carpal tunnel syndrome ( ct ) , that vol . : ( 0123456789 ) 1 3 198 la radiologia medica ( 2020 ) 125 : 197203 is the entrapment of the median nerve at the level of the wrist and the cubital tunnel syndrome ( cuts ) , that is the entrapment of the ulnar nerve at the level of the elbow . 
in recent years , a more thorough research of the peripheral nerve evaluation has been conducted , introducing new parameters in the nerve texture analysis , such as cross - sectional area ( csa ) and nerve density , that is the ratio between the hypoechoic and hyperechoic areas of nerves . 
indeed , diffusion tensor imaging ( dti ) , fascicular ratio and nerve density have been extensively used to assess the inner texture of peripheral nerves [ 810 ]  . 
 however , quantitative imaging of peripheral nerves on mri is not a standard of care at the present time due to lack of standardization in image processing and acquisition . a recent evolution of texture analysis has been represented by the advent of radiomics [ 1416 ]  . 
radiomics is an advanced quantitative image features analysis and it is actually a field of imaging research which implies the analysis and extraction of large amount of data from medical images , with the final outcome of providing prognostic informations that cannot be visible to human eyes [ 1416 ]  . 
the possibility to study the phenotype of peripheral nerves on standard - of - care images , acquired with standard protocols and to analyze the images with widely available software packages for radiomics could open new insights into peripheral nerve pathology evaluation far beyond simple cross - sectional area evaluation [ 7 , 9 , 10 , 18 ]  . 
in clinical practice , the radiological differentiation on mri of normal and pathological nerves in mild carpal and cubital tunnel syndrome is still difficult and several attempts have been made [ 1 , 3 , 7 , 8 ]  . 
however , mri can determine both false positives due to increased nerve t2 signal increase even in healthy subjects [ 13 ] and false negative due to lack of nerve caliber increase on t1 - weighted ( t1w ) in mild en such as carpal tunnel ( ct ) and cubital tunnel syndrome ( cuts ) [ 1113 ]  . 
in addition , mri of peripheral nerves is challenging mostly due to the thin nature of the nerves , for example due to the difficulties in selecting appropriate nerve boundaries , to the difficulties in image interpretation and to the difficult anatomy [ 1 , 3 , 7 ]  . 
therefore , due to the potential of radiomics to unveil even subtle abnormalities on clinical images , the aim of this study was to assess texture analysis ( radiomics ) in the two most common entrapment neuropathies ( en ) of the upper limb such as cts and cuts as a model system of mild focal nerve injury . methods patients the study protocol was approved by our institutional review board ( 411reg2016 ) and conducted in accordance with the declaration of helsinki . 
we retrospectively reviewed all patients who underwent clinical mri examinations for mild carpal and cubital tunnel syndrome ( confirmed by clinical and neurophysiological studies ) in our university hospital between january 2016 and january 2019 . 
from institutional electronic and printed track records , clinical examination , standard electrodiagnostic tests including sensory , motor amplitudes and conduction velocities were used to identify patients with mild cts and cuts . 
inclusion criteria for patients are summarized as follow : mild carpal and cubital tunnel syndrome according to padua and gus classification . mri examinations for mild carpal and cubital tunnel syndrome available between january 2016 and january 2019 . no major artifacts on mri . exclusion criteria applied before analysis were : moderate and severe ct and cuts according to padua and gus score . mri poor images qualities due to the present of artifacts ( e.g. , motion artifacts or phase - encoded motion artifact )  . the lack of information about clinical examination and / or standard electrodiagnostic tests . standard mri protocol all patients were examined by using a 1.5 - tesla scanner ( magnetom avanto , siemens ) with a standard protocol including fast spin - echo t1 - weighted images and t2 - weighted sequences in three orthogonal planes . 
to recognize peripheral nerves and to differentiate them from eventual adjacent vessels , fast 1 3 la radiologia medica ( 2020 ) 125 : 197203 spin - echo axial t1 - weighted images were selectively used . 
 indeed , fast spin - echo t1 - weighted images are better for the detection of anatomical detail such as the typical fascicular pattern appears within the perineurium surrounding by the hyperintense perineural fat tissue . images analysis andradiomics workflow radiomics was performed on fast spin - echo axial t1 - weighted images that had been archived in the pacs ; all images were read and processed in the raw dicom format . 
to standardize measurement , we selected axial t1 - weighted images at the level of the cubital tunnel for the ulnar nerve evaluation ; median nerve was evaluated at the level of the proximal carpal tunnel . 
median nerve was examined just before the carpal tunnel inlet as well as the ulnar nerve , just before the cubital tunnel at the point where maximal enlargement should be present . table 1 mri parameters manufacturer t1 - weighted mr imaging repetition time / echo time ( tr ms / te ms ) slice thickness ( mm ) slice gap field of view ( fov mm ) ( mm ) phase fov fat saturation respiratory state flip angle ( fa ) degree matrix ( pixels ) t2 - weighted mr imaging repetition time / echo time ( tr / te ) slice thickness ( mm ) slice gap field of view ( fov ) ( mm ) phase fov fat saturation respiratory state flip angle ( fa ) degree matrix ( pixels ) t1 - weighted mr imaging and t2 - weighted mr imaging field strength : 1.5 tesla 480 / 11 160200 68 , 8 free 269 384 3600 / 60 160200 free 384 512 statistical analysis from the total of n = 104 features , z - score normalization was applied making the range of the features more uniform and removing features that had high similarity with other features . 
therefore , we selected strongly correlated features ( p value below 0.05 ) and eliminated the redundancies as normally done in the literature with least absolute shrink age and selection operator ( lasso ) method [ 17 ]  . 
mannwhitney u test for unpaired data with 1000 bootstraps samples was used to compare radiomics features of normal and pathological peripheral nerves of the upper extremities to identify the features with statistically significant differences . 
accuracy was measured using receiver operating characteristic ( roc ) analyses to estimate the area under the curve ( auc ) and by estimating thresholds for sensitivity and specificity for the radiomics features that significantly differed between patients and controls , considering the mean value , to avoid over - fitting . 
no statistically significant differences were found between male and female during evaluation of nerves cross - sectional area . a total of n = 104 radiomics features were computed for each patient and control . 
finally , data are organized and collected in the database before analysis 1 3 la radiologia medica ( 2020 ) 125 : 197203 and pathological median and ulnar nerves were found in n = 23 / 104 features . 
a gray level run length matrix ( glrlm ) quantifies gray level runs ( the length in number of pixels , of consecutive pixels that have the same gray level value )  . 
there was no statistically significant difference in the segmentation of normal and pathologic nerves . no significant correlations were found among radiomics features and sensory , motor amplitudes or conduction velocities . 
no significant differences in aucs for median and ulnar nerve en were found . intra - observer agreement resulted to be 0.71 ( 95% lower confidence limit : 0.51 ) and was deemed acceptable for the purpose of the study . discussion diagnostic assessment of peripheral nerve neuropathy is commonly based on clinical findings and electrophysiological testing . 
we selected of 40 patients with diagnosis of mild carpal ( n = 25 ) and cubital tunnel ( n = 15 ) to assess inner texture changes with radiomics corresponding to the loss of the fascicular pattern due to intraneural edema , fibrosis or fascicular alterations [ 10 , 24 ]  . 
in these examples of mild en , the alteration of the nerve cross - sectional area is usually minimal [ 9 ] and even skilled radiologists could have difficulties in diagnosis . 
indeed , in mild en such as cts and cuts , the nerve size could not be affected , but there is a change in the ratio between fascicles and perifascicular tissue that is difficult to assess on conventional imaging [ 6 , 7 ]  . 
see text for detailed results la radiologia medica ( 2020 ) 125 : 197203 in these challenging cases , we showed that a radiomics analysis could extract an array of features useful to differentiate a pathological from a normal nerve . 
this data could be useful to confirm the diagnosis , to help in difficult cases , to detected abnormalities when human eye fails and to give a classification of cts and cuts severity . 
a total of n = 11 / 22 features belonged to gray level run length matrix ( glrlm ) class that quantifies gray level runs of consecutive pixels with the same gray level value . 
mathematical algorithms demonstrated that this type of features could give many information derived from neighboring voxels : this could be another opportunity to characterize the nerve beyond human eye capabilities [ 2327 ]  . 
this problem is typical of mri and only partially solved using ultrasound where a long nerve segment could be evaluated on a single exam [ 23 ]  . the retrospective nature of our study is a known limitation of the study . 
we are not aware of any existing software package to automatically contour peripheral nerves for radiomic analysis fully integrated in radiological workflow , but promising results were reported for the sciatic nerve [ 2830 ]  . 
in conclusion , radiomics analysis on mri of en found 1 3 la radiologia medica ( 2020 ) 125 : 197203 statistically significant differences between normal and pathological nerves in patients with mild cts and cuts . 
 the results suggested that radiomics analysis is feasible and could assess the median and ulnar nerve inner structure changes due to the loss of the fascicular pattern , intraneural edema , fibrosis or fascicular alterations in mild carpal tunnel and mild cubital tunnel syndromes even in difficult cases , for example when the nerve cross - sectional area does not change . acknowledgements one author has received research grants from the european society of musculoskeletal radiology ( essr ) , young researchers grant 2018 . authors contribution scientific guarantor : at . 
two radiologists ( blinded and independent ) semi - qualitatively scored vascular enhancement and image noise according to a fivepoint visual scoring systequantitative analysis was performed by regions of interest quantifying densitometric parameters , such as central and peripheral pulmonary arteries vascular contrast enhancement ( ce , threshold for diagnostic ce 250 hu ) , and metrics for image noise . 
agreement on nondiagnostic semi - qualitative parameters was seen in 9 / 102 ( 8.8% ) ulv ctpas , in particular associated with massive pe ( 2 / 9 ) , pleuro - pulmonary abnormalities ( 5 / 9 ) or without major abnormalities ( 2 / 9 )  . 
quantitative analysis showed that mean ce was lower in ulv group ( p < 0.001 ) , though greater than the diagnostic threshold of 250 hu in both groups . conclusions diagnostic vascular ce ( > 250 hu ) was obtained in both 20ml and 40ml ctpas . 
barbieri , via gramsci 14 , 43126parma , italy 2 section ofradiology , diagnostic department , university hospital ofparma , parma , italy introduction pulmonary embolism ( pe ) is a major cause of hospitalization , morbidity and mortality [ 1 ]  . 
the estimated incidence of pe mortality in six eu countries is 12% , the 93% of which is either sudden fatal pe or undiagnosed venous thromboembolism [ 2 ]  . diagnostic imaging plays a pivotal role in the workup of acute pe . 
sensitivity and specificity of ctpa vol . : ( 0123456789 ) 1 3 138 la radiologia medica ( 2020 ) 125 : 137144 range from 83 to 100% and 89 to 97% , respectively [ 1 , 3 ]  . 
 the exceptional accuracy of ctpa comes with drawbacks related to nephrotoxicity from iodinated contrast medium ( cm ) , which is more commonly observed among patients at high risk for pe ( e.g. , elderly and patients with systemic disease that impair glomerular function ) [ 4 ]  . 
recently , the relationship between the intravenous ( iv ) administration of cm and the development of postcontrast acute kidney injury ( pc - aki ) has been debated in the literature [ 5 ]  . 
nonetheless , various patient - related risk factors for pc - aki have been reported and some of them cannot be overcome ( e.g. , age , chronic kidney disease , congestive heart failure , diabetes or recent acute myocardial infarction ) [ 6 ]  . 
notably , strategies to optimize ctpa technical parameters ( e.g. , cm volume , iodine concentration and osmolality ) could be beneficial in potentially comorbid individuals , especially in the emergency setting where complete availability of anamnestic information may be difficult to be obtained [ 5 , 7 ]  . 
the technical advance in ct hardware and acquisition protocols ( e.g. , reduced acquisition time , increased contrast - to - noise ratio , cnr ) allows for further reduction in cm volume , which is particularly suitable for angiographic ct acquisition , like ctpa [ 16 ]  . 
1 axial ct images showing the vascular enhancement of main pulmonary arteries on ctpa by 20ml ( a ) or 40ml ( b ) of high - concentration contrast medium which was assigned according to medical decision of the attending radiologist [ 6 ]  . 
this retrospective study was approved by the ethical review board . ct technique ctpa was performed with a 64 - row ct scanner ( somatom sensation cardiac , siemens healthcare , forchheim , germany )  . 
 the ctpa was performed at 100 kvp to optimize the vessel opacification from iodinated cm , and with automatic exposure control ( aeccaredose , siemens medical solutions , forchheim , germany ) for tube current modulation ( 150 ref mas )  . 
pre - warmed ( 37c ) high - concentration cm ( iomeprol 400 mgi / ml , iomeron 400 , bracco , it ) was 1 3 la radiologia medica ( 2020 ) 125 : 137144 fig . 
4 pulmonary consolidation in the right upper lobe reducing the overall image quality of a ctpa by 20ml of high - concentration contrast mediuthe parenchymal consolidation is associated with progressive reduction of contrast enhancement , from segmental to subsegmental and further pulmonary artery branches ( white arrow ) administered with idr 1.2 gi / s ( injection rate 3.0ml / s ) , followed by a saline chaser ( 30ml ) using a dual - syringe injector ( medrad stellant , bayer ag , germany )  . 
the scan trigger was followed by shallow breath - hold command ( no deep inspiration ) to reduce the collateral flow from inferior vena cava , and the ctpa scan started 4s after the trigger . 
 the total iodine load ( til ) was calculated as the product of cm volume and iodine concentration [ 19 ] , thus 8gi in ulv group and 16gi in lv group . image analysis multiplanar imaging ( including both coronal and sagittal reformatted images ) was utilized by two radiologists ( cmand rc with 7 and 14years of experience in cardiovascular imaging , respectively ) who were blinded to the administered cm volume . 
the study readers analyzed images with predefined vascular window setting ( wl 300 and ww 700 ) , but they were allowed to manipulate it . diagnosis ofpe the two readers independently reviewed the ctpa scans for signs of pe , namely endovascular clots ( fig.2 ) [ 20 ]  . 
3 massive pulmonary embolism reducing peripheral vascular enhancement in ctpa by 20 ml of high - concentration contrast mediuthe axial image shows a large filling defect involving lobar and segmental arteries , with reduced contrast enhancement onward ( white arrow ) 1 3 140 la radiologia medica ( 2020 ) 125 : 137144 fig . 
in an emergency setting , patients with clinically suspected pulmonary embolism , whose risk factors for pc - aki cannot be assessed , may benefit from a unenhanced ct scan guiding further management . 
individuals without pleuro - parenchymal abnormalities could be safely scanned with 20ml of contrast media , while those displaying major findings ( e.g. , pleural effusion , consolidations ) should be referred for 40ml scan . 
readers scores were averaged and classified as diagnostic ( overall score 3 ) or nondiagnostic ( overall score < 3 )  . quantitative image analysis the mean vascular density ( in hounsfield units , hu ) was measured by one of the two readers ( cm ) by a circular roi into eight predefined vascular branches : mpa , right pulmonary artery ( rpa ) , right upper lobar artery ( rul - a ) , right upper - lobe apical segmental artery ( rul - asa ) , right upper - lobe apical subsegmental artery ( rul - assa ) , left lower lobar artery ( lll - a ) , left lower - lobe posterior segmental artery ( lll - psa ) and left lower - lobe posterior subsegmental artery ( lll - pssa )  . 
diagnostic ce was defined by density > 250 hu [ 22 ]  . extravascular rois were placed in the paraspinal muscles at the level of the mpa in order to calculate mean density , standard deviation ( sd ) of density as a metric of background noise , contrast - to - noise ratio ( cnr ) and snr . 
cnr was defined as vessel enhancement [ hu ] minus adjacent muscle tissue enhancement [ hu ] , divided by adjacent muscle tissue enhancement sd ; snr was defined as vessel enhancement in hu divided by vessel enhancement sd [ 23 ]  . 
the doselength product ( dlp ) was recorded for each patient . 1 3 la radiologia medica ( 2020 ) 125 : 137144 table 2 qualitative scale for the evaluation of central vascular enhancement , peripheral vascular enhancement and image noise diagnosis ofpe central vascular enhancement qualitative scoring system peripheral vascular enhancement qualitative scoring system none minimum , low confidence for diagnosis moderate , sufficient for diagnosis good excellent image noise qualitative scoring system no subsegmental or segmental artery enhancement < 25% of subsegmental or segmental arteries enhanced 2550% of subsegmental or segmental arteries enhanced 5075% of subsegmental or segmental arteries enhanced > 75% of subsegmental or segmental arteries enhanced major , no diagnosis possible major , diagnosis possible but with low confidence moderate , sufficient for diagnosis minor , diagnosis not influenced undetected statistical analysis descriptive statistics were used to report normally distributed continuous variable as mean and its standard deviation ( sd )  . 
inter - observer agreement for the presence of pe , breathing artifacts and qualitative image analysis was calculated by the weighted kappa test , with strength of agreement expressed by the k value as follows : poor ( k 0.20 ) , fair ( k = 0.210.40 ) , moderate ( k = 0.410.60 ) , good ( k = 0.610.80 ) , excellent ( k = 0.811.0 ) [ 24 ]  . 
the agreement dropped to fair for both veperipheral ( k = 0.324 ) and image noise in ulv group ( k = 0.325 ) , whereas it remained good in lv group ( k = 0.516 and k = 0.406 , respectively ) ( table3 )  . both study readers recorded at least one nondiagnostic parameter in 9 / 102 ( 8.8% ) ulv , in particular : 5 / 9 ( 55.6% ) nondiagnostic veperipheral , 2 / 9 ( 22.2% ) high noise , 1 / 9 ( 11.1% ) nondiagnostic vecentral and veperipheral and 1 / 9 ( 11.1% ) with all parameters rated as nondiagnostic . 
the quality decay was seen in 2 / 9 patients ( 22.2% ) with massive pe which weakened the peripheral vessel opacification , in 5 / 9 ( 55.6% ) with associated pleuro - parenchymal abnormalities , and in 2 / 9 ( 22.2% ) cases , no major finding was detected . 
the limited number of nondiagnostic ctpas by 20ml protocol was mostly due to major coexisting massive pe or pleuro - parenchymal abnormalities . the clinical relevance of pc - aki is still under debate [ 25 , 26 ]  . 
analyzed til reduction by means of high volume of low - concentration cm ( 100ml of 150 iodine mg / ml , til 15gi ) to expand the temporal window of first pass ; however , they could not reach the densitometric diagnostic threshold for pe despite high injection rate ( 5ml / s , idr 0.75 gi / s ) [ 27 ]  . 
our data show that small volume of highconcentration cm is diagnostically appropriate and convenient because it grants appropriate vascular opacification by high idr ( 1.2gi / s ) for a sufficient temporal window , while preserving low til ( 8gi ) [ 28 , 29 ]  . 
the rationale of ctpa protocol for pe is particularly intended for first - pass examinations , notably the ct angiography of small vascular compartment with minimal variability in cm dynamics [ 17 ]  . 
of note , cardiac diseases and other causes of hemodynamic changes may challenge the optimization of vascular enhancement by adding variability in bolus timing , especially when using as small as 20ml volume ; hence , the bolus trigger technique appears mandatory for first - pass arterial study with such small cm volume , while larger cm volume might also be safely managed by fixed delay of scanning . 
 moreover , the small 20ml volume of cm is also conditioned by moderate injection rate that allows sufficient temporal window , whereas 40ml volume of cm allows sufficient temporal window even with higher injection rate . 
nonetheless , a moderate injection rate might be especially convenient in the setting of emergency department where limitations can be encountered in catheterization of veins for higher injection rate ( e.g. , 5ml / s ) , especially in elderly or oncologic patients that are at higher risk of pe . in our study , the inter - observer agreement for the detection of pe was excellent ; in particular , the agreement by 20 ml was not lower than with 40 ml . 
we propose to include precontrast ct scan by acknowledging the drawback of an increased radiation exposure , which , however , might yield minor mutational impact in older patients that represent the majority of subjects with suspected pe and relatively high risk of pc - aki [ 31 ]  . 
nonetheless , it should be underscored that unenhanced ct should be kept at minimal dose for reduction in radiation burden , which new scanners can easily manage with equivalent dose to conventional chest radiography for the evaluation of major parenchyma abnormalities ( i.e. , ultra - low dose ct ) [ 32 , 33 ]  . 
we report correlation between bmi and ce for both 20ml ( moderate negative correlation ) and 40ml ( weak negative correlation ) protocols , while preserving diagnostic ce was possible in both groups 1 3 la radiologia medica ( 2020 ) 125 : 137144 in an average overweight population . 
recently , the adjustment of cm amount by considering body weight and scan duration showed that a substantial reduction of cm can be obtained in low - weight individuals [ 14 ]  . 
 the perspective of personalized ctpa protocol is progressively emerging , algorithms for systematic calculation of the optimal cm volume and kvp are being proposed on the basis of pretest quantitative data and 80kvp might be safely warranted by automatic selection of tube voltage [ 35 ]  . our study presents several limitations . 
first , the retrospective design affected patients selection : patients age was higher in the ulv group because in our clinical setting the reporting radiologist evaluated the clinical status of the patients admitted to ctpa to identify those that could benefit from the 20ml protocol . 
the relatively small population was a consequence of the strict inclusion criteria , notably pregnant women were not included and therefore the ulv protocol should not be intended in such peculiar condition . 
md in each site , and ed parameters , such as volume ct dose index ( ctdivol ) , ssde , dose length product ( dlp ) , effective dose ( e ) , were compared between two protocols with a t test . 
coronary computed tomography ( cct ) is most useful at ruling out coronary disease , in patients with low to intermediate pre - test probability for cad , with a very high negative predictive value ( 8399% ) [ 25 ]  . however , some studies revealed that the increased use of ct scanners and , consequently , of ionizing radiations , correlates with the major risk of radiation - induced malignancy . 
 furthermore , radiation dose ( rd ) during cct examination is of particular concern because four of the most radiosensitive organs ( thyroid gland , lung , bone marrow and breast ) are within or near the scan range [ 610 ]  . 
dual - source ( ds ) ct technology allowed reducing rd for cct , with two x - ray tubes into the ct gantry positioned at 95 degrees from one another . 
tfp is suitable for patient with regular heart rate , lower than 65 beats per minute ( bpm ) and allowed rd reduction compared with the retrospective protocol ( rp ) [ 1418 ]  . the european council directive on medical exposures 2013 / 59 / euratom emphasizes the radiologists responsibility to prevent high radiation exposure during diagnostic exams and underlines the importance of collecting and analyzing rd [ 19 ]  . 
the most widely used approach in ct scanner is based on software estimated dose ( ed ) parameters , such as , volume ct dose index ( ctdivol ) ; size - specific dose estimate ( ssde ) , which , corrected for the patients size , is more accurate than ctdivol in rd estimation ; dose length product ( dlp ) and effective dose ( e ) [ 2023 ]  . 
however , these parameters only reflect ct radiation output , allowing comparison between different scanners , but do not provide the rd absorbed by patients [ 24 , 25 ]  . 
indeed , the absorbed dose , especially in radiosensitive organs and the risk of radiation - induced malignancy , can be measured only applying dosimeters , directly placed on cutaneous surface at organ level . 
unfortunately , invivo measured dose ( md ) requires many resources and it is not practical during the routine clinical scan [ 2628 ]  . the aim of this study is to compare invivo md with thermoluminescent dosimeters ( tdls ) , software ed parameters and image quality between tfp and rp in cct and correlate , in each protocol , md with ssde . materials andmethods patients selection the institutional review board approved this study . 
written informed consent was obtained from all patients before they entered in the study . in this prospective study , 68 consecutive patients undergoing cct were enrolled between september and december 2018 . 
exclusion criteria were : previous medical history of cad ; previous cardiac surgery ; previous breast surgery ; allergy to iodinated contrast medium ; estimated glomerular filtration rate < 60ml / min / 1.73m2 ( according to european society of urogenital radiology ) [ 29 , 30 ]  . clinical data collected were age , gender , weight and height . 
body mass index was calculated for each patient . cct protocol all cct examinations were performed with third - generation 192 2 slices dsct ( somatom force , siemens healthineers , forcheim , germany ) , with patients in the supine position and feet toward the gantry . 
a 20 - gauce cannula was inserted into the superficial vein of the right antecubital fossa , connected to a two - way injector ( empowercta + injector system , bracco engineering , lausanne , switzerland ) : one with contrast medium ( cm ) , ( iopamidol , 370mg i / ml , bracco imaging , milano , italia ) and the other with saline solution . an ecg - triggered scan was performed . 
tfp was used with regular heart rate , equal or lower than 65bpm ; rp was used with arrhythmic heart rate or greater than 65bpm . a bolus test technique was used to evaluate cm peak time in the ascending aorta . 
md in each site was the average from the couples tld doses , applying a correct calibration factor for the specific x - ray energy . for each patient , ctdivol , and dlp were recorded directly from the ct software dose watch ( ge healthcare , buc , france ) , and ssde was calculated by the same software from the scanogram at the middle of the scan . the european commission guidelines document had provided two different chest k factors for e calculation [ 31 ]  . 
tdl placement on cutaneous surface of patient in antero - posterior a , left latero - lateral b , and oblique c visuals 1 3 120 la radiologia medica ( 2020 ) 125 : 117127 according to these latter guidelines , e was calculated by multiplying dlp value by k factor ( k = 0.014msv * mgy1 * cm1 )  . for each patient , mean md value between heart level and left hemi - thorax was calculated to correlate with ssde . 
we decided to exclude from mean md value the absorbed dose at thyroid level because out of scan range , and the absorbed dose at left breast areola because ssde do not always considers shape and size of mammary gland . image quality assessment quantitative image quality quantitative image quality was assessed evaluating intravascular attenuation , signal - to - noise ratio ( snr ) , and contrastto - noise ratio ( cnr )  . 
for each examination , one radiologist ( with 10years experience in cta ) measured , with a region of interest ( roi ) , the attenuation and standard deviation ( sd ) in ascending aorta ( aa ) , in proximal segments of the right coronary artery ( rca ) , in left main coronary artery ( lmc ) , in left anterior descending artery ( lad ) , in left circumflex artery ( lcx )  . 
mediastinal fat attenuation was also evaluated by positioning a roi in the same slice of intravascular attenuation measurement . in both protocol , mean attenuation and mean sd in all arteries sites , and mean mediastinal fat attenuation , were calculated . 
mean sd in aa was defined as image noise ( in )  . snr and cnr of every vessel were calculated according to the following equations [ 31 ] : snr = mean intravascular attenuationin cnr = ( mean intravascular attenuation mean mediastinal fat attenuation ) in semiqualitative image quality semiqualitative image quality was independently evaluated on a per - vessel basis by two independent reader radiologists with 10years experience ( reader radiologist 1 ) and 15years experience ( reader radiologist 2 ) in cardiovascular imaging . 
likert score system , with a 5 - point ranking scale , was used to classify image quality : ( 1 ) high noise level , poor vessel definition ; ( 2 ) considerable noise , partially limited vessel wall delineation ; ( 3 ) little noise and good delineation of vessel borders ; ( 4 ) very little noise and clear delineation of vessel walls ; ( 5 ) excellent delineation of vessel walls , high attenuation in the vessel . 
then , the inter - observer agreement between two reader radiologists was evaluated . statistical analysis statistical analyses were performed using medcalc for windows , version 16.2 ( medcalc software , ostend , belgium )  . 
categorical data are given as absolute numbers and percentages . in each protocol , mean md in each site , mean ctdivol , ssde , dlp , e , mean intravascular attenuation , snr and cnr were calculated and compared between tfp and rp , with student t test . 
in both protocols , for each patient , mean md between heart level and left hemi - thorax was calculated and correlated with ssde , with pearson correlation coefficient ( r )  . semiqualitative image quality scores were compared between two protocols with mannwhitney u test . 
cohen kappa coefficient was evaluated as k value < 0.40 , poor agreement ; 0.410.60 , moderate agreement ; 0.610.80 , good agreement ; 0.811.00 , very good agreement . results the patient demographics are shown in table 2 . 
excellent correlation between measured dose and size - specific dose estimates with turbo - flash protocol la radiologia medica ( 2020 ) 125 : 117127 r = 0.9298 ; p < 0.0001 measured dose * ( mgy ) note . 
ctdivol , ssde , dlp and e provide ct radiation output but not provide patient absorbed rd and the risk of radiation - induced malignancy , especially in radiosensitive organs [ 1620 , 3640 ]  . 
thus , the purpose of this study is to compare invivo md with tlds , software ed parameters and image quality between tfp and rp in cct and correlate , in each protocol , md with ssde . in this study , comparing tfp with rp , we obtained significantly lower md values at thyroid gland level , heart level , left breast areola and left hemi - thorax . 
 a possible explanation of these results is that the thyroid gland is the only site , monitored with tdls , out of cct scan range , and being at the scan field upper limit its md is more subject to acquisition range variability . 
these results indicate that the tfp , compared to rp , allows to obtain lower absorbed dose and , consequently , radiation - induced malignancy risk reduction for organs within or near the scan range . 
furthermore , special attention should be given to fix the upper limit of cct scan range to avoid unwanted radiation to the thyroid gland that is particularly sensitive to the long - term effects of radiation exposure , as demonstrated in previous studies [ 41 ]  . 
these results indicate that dsct scanner , equipped with two x - ray tubes positioned at 95 degrees from one another , allows use of very high pitch values in tfp ( pitch factor , 3.2 ) compared to rp ( pitch factor , 0.15 ) and guarantees very high reduction in patient radiation exposure . 
 these findings suggest that ssde , in cct examinations , allows comparing the absorbed dose by different patients . in this work , for both observers , mean intravascular attenuation , cnr and snr in all evaluated sites ( aa , rca , lmc , lad , lcx ) were not significantly different with tfp compared to rp , and similarly , there were no statistically significant differences in semiqualitative image quality . 
as consequence , the results suggest that choosing the correct protocol , based on the heart rhythm , is possible to obtain a good diagnostic quality examination without movement artifacts . to date , in the scientific literature , only in few works was measured the absorbed dose with tld during diagnostic ct examinations . 
they obtained an excellent correlation between md and ssde ( r = 0.99 ) with a very low sample size ( number of patients , 11 ) , and without statistical significance evaluation of their measurements . 
 [ 45 ] , in their work , with a ct scanner equal to ours , compared tfp with prospective step and shot protocol , obtaining with the first one , snr values similar to ours in all artery segments , but using a slightly higher dose of cm ( 50ml )  . this study has some limitations . 
to compare , more accurately , tld results to ssde , the localizer contributions should be subtracted from the tld values , even 1 3 la radiologia medica ( 2020 ) 125 : 117127 fig . 
curved reformation images of right coronary artery a , left anterior descending artery b , and left circumflex artery c , and volume rendering reconstruction d if the absorbed dose during the localizer scan is very low . 
 second , cct protocols could not be compared intra - individually , as it was deemed unethical to subject each patient to more than one ct acquisition ; however , there were no statistically significant differences in patients demographics between two groups . in conclusion , in cct , with tfp , md was significantly lower at thyroid level , heart level , left breast areola and left hemi - thorax compared to rp . 
therefore , with 192 2 dsct , in cct , tfp should be used as much as possible with regular heart rate lower than 65 bmp , to reduce the rd delivered and obtaining a comparable image quality , to rp . 
particularly important is to fix correctly the upper limit of scan range ; otherwise , 1 3 126 la radiologia medica ( 2020 ) 125 : 117127 the risk is to administer to thyroid high rd while using tfp . our study may inspire to identify additional dose reduction strategies with the dsct scanners and improve the radiologists confident with new ultra - fast cct protocol . funding this research did not receive any specific grant from funding agencies in the public , commercial , or not - for - profit sectors . compliance with ethical standard conflict of interest the authors declared no potential conflicts of interests associated with this study . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
findings were classified as related to or not related to genitourinary system and divided into three classes , according to their clinical significance , as follows : group 1 , not significant or scarcely significant ; group 2 , moderately or potentially significant ; and group 3 , significant . 
statistical significance level was set at p < 0.05. results incidental findings ( n = 461 ) were present in 341 ( 52.7% ) patients , while 306 ( 47.3% ) patients did not have any extra - prostatic if . 
twenty - seven ( 4.2% ) of the 647 patients underwent surgical treatment for ifs not directly related to prostate cancer . conclusion ifs not related to prostate cancer may be frequently encountered on multiparametric prostate mri , and they are significantly more common in patients > 65years old . keywords prostate cancer magnetic resonance imaging incidental findings collateral findings * roberto cannella rob.cannella89@gmail.com 1 sezione di scienze radiologiche , dipartimento di biomedicina , neuroscienze e diagnostica avanzata ( bind ) , university ofpalermo , via del vespro 129 , 90127palermo , italy 2 department ofmedical oncology , dichirons , university ofpalermo , palermo , italy 3 unit operativa di urologia , dipartimento di discipline chirurgiche , oncologiche e stomatologiche , university ofpalermo , palermo , italy introduction prostate cancer is the most common malignancy and the second leading cause of cancer - related mortality in men [ 1 ]  . 
this leads to numerous problems and sampling errors like detection of clinical insignificant lesions , missed clinically significant prostate cancers ( for example in anterior prostate ) or attribution of clinically significant lesions as low risk [ 6 ]  . in 2015 , the promis group proposed a new diagnostic pathway in which multiparametric prostate magnetic resonance imaging ( mri ) is used as a triage test for men at a risk of prostate cancer [ 6 ]  . 
promis study [ 6 ] proposed multiparametric prostate mri before prostate biopsy in order to avoid unnecessary biopsy , to perform a targeted biopsy with the reduction of false - negative results and to increase the identification of clinically significant prostate cancer not identified at digital rectal exploration or located in occult areas of the gland ( apical distal , midline , subcapsular and anterior areas ) [ 7 , 8 ]  . the widespread request of multiparametric prostate mri has increased the identification of incidental findings ( ifs ) not always related to the primary aim of the investigation [ 912 ]  . 
the major problem is related to the identification of ifs that are not clinically significant , potentially leading to an increased public health burden and to an increase in stress for patients . the aim of our study is to evaluate the prevalence and distribution of ifs identified on multiparametric prostate mri examination according to a classification model based on clinical significance . materials andmethods the institutional review board approved this retrospective single - institution study . 
examinations were performed for at least one of the following clinical reasons : ( a ) elevated psa level ( > 4ng / ml ) ; ( b ) abnormal digital rectal examination and / or transrectal ultrasound ; ( c ) follow - up postradiation therapy ; ( d ) psa level > 0.2ng / ml in patients with prostate cancer who have undergone radical prostatectomy . 
our imaging protocol includes axial turbo - spin echo ( tse ) t1 - weighted sequence acquired to exclude the presence of postbiopsy blood residues , which may be appreciated as hyperintense foci ; axial , sagittal and coronal tse t2 - weighted sequences , oriented according to the major axis of the prostate ; diffusion - weighted images ( dwi ) performed through the acquisition of single - shot ecoplanar sequences ( epi ) with a maximum b value of 1400s / mm2 . 
in addition , perfusion imaging was 1 3 206 la radiologia medica ( 2020 ) 125 : 204213 performed after intravenous administration of gadoliniumbased contrast agent , 1mmol / kg of gadoteric acid ( gddota , dotarem , guerbet , usa ) at a flow of 3ml / sec followed by infusion of 30ml of saline solution , to evaluate the presence of hypervascular lesions by acquiring 3d t1 - weighed axial sequences . classification ofincidental findings multiparametric prostate mri reports and images were reviewed jointly by two radiologists ( with 10 and 4years of experience on prostate imaging , respectively ) to record the presence of all extra - prostatic findings . 
according to the american college of radiology [ 14 ] , incidental findings were defined as an incidentally discovered mass , lesion or abnormality detected by prostate mri performed for an unrelated reason . 
conditions directly related to prostate cancer such as seminal vesicle invasion , bladder invasion , rectal invasion , bone metastasis and lymph node metastasis were not considered as ifs as they are part of the standard prostate cancer staging . 
 enlarged lymph ( > 10mm in short axis diameter ) nodes with equivocal imaging features were considered indeterminate for metastasis . ifs were classified into related to or not related to the genitourinary system and subsequently divided into three groups according to a progressive scale of clinical significance as reported in prior studies [ 16 , 17 ] : group 1 : not significant or scarcely significant , if they have not requested further evaluations or treatments . group 2 : moderately or potentially significant , if they have requested further diagnostic investigations , followup or medical / surgical treatment . group 3 : significant , if they require immediate treatment or if they change the patients prognosis . statistical analysis continuous variables are expressed as mean and standard deviation , and categorical variables are expressed as numbers and percentages . 
the mannwhitney u test was performed to assess the difference of mean number of incidental findings according to patients age group . statistical significance level was set at p < 0.05. 
overall , 242 ( 37.4% ) patients had only one if , 80 ( 12.4% ) patients had two ifs , 17 ( 2.6% ) patients had three ifs , and two ( 0.3% ) patients had four findings . 
 ifs were significantly more common in patients > 65years old ( n = 225 , 57.0% ) compared to patients 65years old ( n = 116 , 46.0% , p = 0.007 ) ( table 1 )  . 
for all patients included in the final population , the medical records were scrutinized to collect information about further follow - up , pathological confirmation or management changes after the detection of ifs . 
particularly , patients > 65 years old had significantly more common group 1 ifs ( n = 183 , 46.3% ) compared to 65 - year - old patients ( n = 95 , 37.7% , p = 0.031 ) ( table1 )  . 
similarly , group 3 ifs were almost exclusively present in patients > 65years old ( n = 11 , 2.8% ) as opposed to patients 65years old ( n = 1 , 0.4% , p = 0.034 ) ( table1 )  . 
bladder wall thickening ( n = 22 ) and indeterminate ( not definitively metastatic ) enlarged lymph nodes ( n = 36 ) were the most common ifs in group 2 . 
bladder carcinoma ( n = 7 ) and testicle tumor ( n = 3 ) were the most common ifs in group 3 . of the 106 ifs belonging to groups 2 and group 3 , 36 ( 33.0% ) required follow - up after appropriate medical therapy , 34 ( 32.1% ) required other diagnostic investigation ( colonoscopy , bone scintigraphy , ct , ultrasound ) , 18 ( 17.0% ) underwent ultrasound follow - up , 10 ( 9.4% ) needed clinical anamnestic correlation , and finally , 8 ( 7.6% ) were followed up with mri . 
 categorical variables were compared using the fishers exact test or chi - squared test directly related to prostate cancer ( 7 bladder carcinomas ; 3 testicle tumors ; 2 rectal cancers ; 15 bladder wall thickening )  . 
a 63 - year - old man with intramuscular lesion consistent with peripheral nerve sheath tumor ( fig.8 ) underwent 2 - year mri follow - up which demonstrated its stability . 
overall , we observed that 102 ( 15.7% ) patients undergoing multiparametric prostate mri had potentially significant ( group 2 ) or definitively significant ifs ( group 3 ) which often required a management change , including surgical treatment for incidentally discovered extra - prostatic cancers . 
although definitively significant ifs were rare ( group 3 , 1.8% ) , they were almost exclusively detected in patients > 65years old ( p = 0.034 ) and their correct identification carried important clinical implications . 
only one cancer was incidentally discovered in the 65years old group , which was a bladder carcinoma in a 64 - year - old man ( close to the 65 cutoff age )  . 
our results underline the importance of specialized abdominal radiologists interpreting multiparametric prostate mri examinations which should not need only to assess the prostate lesions but also scrutinize the presence of other possible significant lower abdomen and pelvis pathologies . 
the frequency of these ifs on multiparametric prostate mri may grow in the general population due to the rapid diffusion of multiparametric prostate mri and the increased spread of this imaging technique even in old patients . to the best of our knowledge , only few prior studies [ 9 , 10 ] have assessed the presence of ifs in multiparametric prostate mri . 
 [ 9 ] , such as indeterminate enlarged lymph nodes ( not definitively metastatic ) , pelvic free fluid , bone alterations ( not metastatic ) and dolichocolon , which represented 25.8% of all ifs not related to genitourinary systealthough sherrer etal . 
axial t1 - weighted ( a ) and sagittal t2 - weighted ( b ) images depict a 2.1 - cm lesion ( arrows ) in the right testis , which was proven to be a germ cell tumor after orchiectomy analyze the distribution of each ifs in different patients age group . 
moreover , their results may also be skewed by the different study protocol with the inclusion of postcontrast imaging of the entire abdomen [ 9 ] , a protocol not routinely adopted at our institution where the imaging is limited to the pelvis , in accordance with pi - rads v 2.1 recommendation [ 18 ]  . incidentally discovered non - prostatic tumors ( 7 bladder carcinomas , 3 testicular tumors and 2 rectal cancers ) fig . 
axial ( a ) , sagittal ( b ) and coronal ( c ) t2 - weighted images demonstrated a 1.1 - cm bladder wall vegetating lesion ( arrows ) which was confirmed as bladder urothelial carcinoma after transurethral resection 1 3 la radiologia medica ( 2020 ) 125 : 204213 fig . 
axial ( a ) , sagittal ( b ) and coronal ( c ) t2 - weighted images show an irregular wall thickening ( arrows ) in the middle rectum , which was confirmed as rectal adenocarcinoma at endoscopy fig . 
axial ( a ) and sagittal ( b ) t2 - weighted images show a 3.2 - cm lesion located between the left pectineus and adductor brevis muscles , consistent with peripheral nerve sheath tumor ( arrows )  . 
 ( c ) mri follow - up after two years confirmed the lesions size stability ( arrow ) 1 3 212 la radiologia medica ( 2020 ) 125 : 204213 accounted for all the group 3 ifs in our study . 
the detection of bladder carcinoma resulted in the modification of patients management who underwent transurethral resection ( n = 5 ) or radical cystectomy ( n = 2 )  . 
 [ 10 ] reported an incidence of 0.8% ( n = 25 ) of incidentally detected bladder lesions on a large series of multiparametric prostate mri ( n = 3147 ) , with 13 cases ( 0.4% ) finally proven to be bladder cancers . 
to the best of our knowledge this is the first study reporting the prevalence of incidentally discovered rectal cancers or testicle tumors in a large population images with multiparametric prostate mri . 
 however , synchronous prostate and rectal cancers have been occasionally reported in patients undergoing mri staging of primary rectal cancers [ 20 ]  . this study has several limitations that need to be acknowledged . 
first , all of the included patients were obviously men , so the percentages of ifs of the lower abdomen may not be applicable to entire population of both men and women . 
second , the majority of not significant or potentially significant ifs were not pathologically proven and the diagnosis was based only on the review of the imaging findings , radiological and clinical reports . 
the lack of pathological analysis may have particularly influenced the evaluation of indeterminate lymph nodes due to the low specificity of multiparametric prostate mri for the detection of small lymph nodes metastases [ 21 ]  . 
finally , our study did not include an analysis of sensitivity and specificity of each mri sequence performed for the detection of incidental findings according to their group of clinical significance . 
different mri protocols and the number of sequences with large field of view may influence the prevalence and type of ifs detected when performing multiparametric prostate mri , including the possibility to discover other ifs when abdominal sequences are included in the prostate cancer mri staging [ 22 ]  . in conclusion , incidental findings not related to prostate cancer may be frequently encountered on multiparametric prostate mri , especially in patients older than 65years . 
one approach to assign the red map consists of segmenting the daily magnetic resonance image into five different density levels and assigning a red bulk value to each level to generate a synthetic ct ( sct )  . 
the aim of this study is to evaluate the dose calculation accuracy of this approach for applications in mrgrt . methods a planning ct ( pct ) was acquired for 26 patients with abdominal and pelvic lesions and segmented in five levels similar to an online approach : air , lung , fat , soft tissue and bone . 
two scts were generated assigning different bulk values to the segmented levels on pct : the scticru uses the red values recommended by icru46 , and the scttailor uses the median patient - specific red values . 
the mean difference in estimating v95 ( ptv ) was equal to 0.2% using scttailor and 1.2% using scticru , respect to pct values conclusions the bulk sct guarantees a high level of dose calculation accuracy also in presence of magnetic field , making this approach suitable to mrgrt . 
gemelli , irccs , largo agostino gemelli 8 , 00168rome , italy vol . : ( 0123456789 ) 1 3 158 introduction online adaptive radiotherapy ( art ) represents a new promising resource in the frame of personalised medicine , allowing to modify the radiation treatment ( rt ) according to patients daily anatomy [ 1 , 2 ]  . several authors have recently demonstrated that this procedure can effectively manage the inter - fraction organs variability that represents one of the main sources of uncertainty conditioning the treatment outcome [ 3 , 4 ]  . online art can today be administered by means of hybrid rt machines , able to join a magnetic resonance ( mr ) scanner with a rt delivery system [ 5 , 6 ]  . mr - guided rt systems allow to elaborate the rt treatment plan directly on the daily mr image ( mri ) acquired by the on - board scanner , taking into consideration the actual patient anatomy and so addressing the inter - fraction organ variability . 
planning on mr images allows a clearer visualisation of the target and organs at risk ( oars ) , due to the superior soft tissue contrast provided by mri as compared to computed tomography ( ct )  . 
mri , however , requires the assignment of a relative electron density ( red ) map to allow for accurate dose calculation [ 7 , 8 ]  . the daily red map assignment is particularly critical in mr - guided rt , because the treatment delivery is administered in presence of magnetic field ( b ) and the effects of b on the dose distribution can be very significant , especially in presence of tissue inhomogeneities [ 912 ]  . different approaches have been developed to assign red map to mri during online adaptive mrgrt . 
this curve was used to convert the hu values to red values . synthetic cts andrt plans generation the analysis on dose calculation accuracy was performed generating the synthetic ct starting from the pct image , to avoid potential bias due to the different patients imaging setup that may occur between ct and mr positioning [ 21 , 24 ]  . two different sct images were generated by assigning red bulk values to the levels segmented on the pct . 
 a first synthetic ct ( scticru ) was created using the red values suggested by icru report 46 ( air = 0.001 ; lung = 0.26 ; fat = 0.89 ; soft tissue = 1.02 ; bone = 1.12 ) as bulk values [ 25 ]  . a tailored synthetic ct ( scttailor ) was also generated replacing the red values recommended by icru for fat , soft tissue and bone with patient - specific median red values . 
red values for air and lung were maintained as suggested by icru 46 , considering the anatomical sites analysed in this study . median value was preferred to the mean because the distribution of the grey levels in the analysed region of interest could not be distributed according to a gaussian statistic [ 26 ]  . a total of three intensity modulated radiation therapy ( imrt ) treatment plans were calculated for each patient using the mridian tps . 
the original treatment plan was calculated on the pct image and considered as reference . the same treatment plan was then recalculated , without applying any optimisation or normalisation , on the scticru and scttailor images . dose distribution was calculated using a graphical processing unit ( gpu ) - accelerated monte carlo platform , taking into account the effect of the magnetic field and using a grid size equal to 0.1cm for dose calculation [ 27 ]  . dosimetric evaluation ofsct dose distributions obtained on the sct images were compared to the one calculated on the pct in terms of gamma analysis and dose volume histogram ( dvh ) parameters [ 28 ]  . gamma analysis was realised using the verisoft software ( ptw , freiburg , germany ) and considering the following tolerance criteria : 1% / 1mm , 2% / 2mm , 20cgy / 1mm and 50cgy / 1mthe two gamma criteria considering percentage values as dose difference ( 1% / 1mm and 2% / 2mm ) were chosen in consideration of other studies performing gamma analysis to evaluate calculated dose distributions [ 29 , 30 ]  . 
the mean value of the gamma passing rate calculated on these three planes was considered as 3d gamma indicator . the dose calculation accuracy was furthermore investigated comparing different dvh indicators , as reported in several works dealing this topic [ 18 , 19 , 31 , 32 ]  . 
1 example of trufi image : the intensity difference between fat , soft tissue and air is clearly defined 1 3 160 la radiologia medica ( 2020 ) 125 : 157164 the wilcoxonmannwhitney ( wmw ) test for paired samples was performed to evaluate the statistical significance of the differences under analysis [ 33 ]  . bonferroni correction was applied to take into account the problem of multiple comparisons . 
the reason of such disagreement can be attributed to the presence of a pancreatic stent in proximity of the target region , whose actual median red value ( equal to 1.43 ) is very different from the assigned one . 
5 box - plot analysis related to the dose differences of scttailor and scticru respect to the reference pct for different dvh parameters related to ptv coverage ( v95 , d98 , d2 ) and oar sparing ( d98 , mean dose and d1 cc )  . 
6 dose distributions calculated on pct , scttailor and scticru for patient 10 conclusions la radiologia medica ( 2020 ) 125 : 214219 radiotherapy is multidisciplinary management possible inthetreatment oflung cancer ? areport fromthree italian meetings alessiobruni2 paoloborghetti3 niccolgiajlevra4 sararamella5 luciobuffoni6 davidefranceschini1 serenabadellino7 mariaandolina2 camillacomin8 emanuelavattemi9 michelabezzi10 marcotrov11 antoniopassaro12 alessandrabearz13 ritachiari14 franchinatindara15 katiaferrari16 gaiapiperno17 andreariccardofilippi18 domenicogenovesi19 vieriscotti20 received : 17 july 2019 / accepted : 1 october 2019 / published online : 11 october 2019 italian society of medical radiology 2019 abstract purpose to report criticisms and barriers to the real - life application of international guidelines and recent developments in the management of locally advanced non - small cell lung cancer ( nsclc ) in italy . methods three 2 - day courses were organized . 
the aim was to stimulate the discussion on practical issues in the management of nsclc patients in the real - life practice . results a total of 196 physicians were involved in the courses as learners . 
invasive diagnosis of nodal disease for staging purposes , a priori definition of surgical resectability and a regular mdt with all crucial participants available were the three main key points identified for a good management of these patients . 
the main barriers to the clinical application of a good diagnostic and therapeutic approach to the patient were the absence of a regular and complete mdt in the south and centre of italy , while in the north of italy , time for discussion of clinical cases in the mdt and waiting lists for staging and therapeutic interventions were deemed as the major concerns . conclusion the meetings showed that diagnosis and treatment of locally advanced nsclc are still extremely variable between different italian regions . 
logistic issues , waiting lists , paucity of well - trained staff and expertise seem to be the main barriers to international guidelines application . keywords non small cell lung cancer stage iii multidisciplinary evaluation introduction lung cancer is the leading cause of cancer death in men and the second leading cause of cancer death in women worldwide [ 1 ]  . 
being mostly related to tobacco smoking , lung cancer incidence and mortality are decreasing in those countries in which smoking cessation campaigns began earlier , such as usa or most european countries . 
the definition of locally advanced nsclc includes a wide spectrum of clinical presentations , ranging from patients with very invasive primary tumors even if without nodal pathological invasion , to patients with various primary lesions accomplished with massive mediastinal nodal involvement . 
there are several different causes behind this heterogeneity , including logistic , historical reasons , economic issues and many others . in 2018 , the italian association of radiotherapy and clinical oncology ( airo ) thoracic oncology study group promoted a survey on the management of locally advanced nsclc . 
therefore , we organized three 2 - day courses , one in the north , one in the south and one in the centre of italy , aiming at discussing the results of this survey , debating available guidelines and analyzing clinical cases as in a multidisciplinary team ( mdt )  . 
 in the present paper , we wish to present the results of this national experience , focusing on the major critical lacks . materials andmethods three courses were organized in 2018 in different parts of italy ( one in the north , one in the centre and one in the south )  . 
in the first day of the course , experts in different fields of thoracic oncology gave their lecture on radiology , pathology , medical oncology , surgery and radiotherapy on stage iii nsclc . 
every group included different specialists , to represent a multidisciplinary teaeach group had two facilitators ( experts chosen within the faculty ) , who should stimulate the discussion and collect answers from participants . 
though these cases come from real experiences , the aim was to stimulate the discussion on practical issues in the management of these patients in the real - life practice . apart from the clinical aspects , which were not the major endpoints of the meetings , three questions were addressed to each group : how could you improve the management of the clinical case ? which kind of behaviors should have been avoided in the management of the clinical case ? what are the main barriers that could prevent from the application of the international guidelines in the management of the clinical case in the daily practice ? as the objectives were focused , a consensual hunch has been formed that releases an action plan which was presented in the plenary session . 
each group presented their results and answers , so that every participant could further debate on different clinical situations not faced in his workgroup . results overall , 196 physicians participated in the three courses as learners , 89 in milan meeting , 42 in catania meeting and 65 in rome meeting . 
in addition , 24 faculty members were involved in each course , but did not express any opinion for the management of the clinical cases , not to influence participants decisions . 
treatment chosen by majority of participants , main controversies and final agreement for the proposed clinical scenarios are shown in table1 . in the plenary discussion of clinical cases , focusing on the three questions that were common to all groups , it emerged a significant agreement independently from the different clinical cases or the different participants region of provenience . 
 answers are summarized in table2 . discussion we reported an experience derived from three different meetings that took place in italy in 2018 focusing on the management of locally advanced nsclc . 
on the contrary , the aim is to take a picture of the real - life management of these patients in italy , trying to identify possible criticisms and barriers that could preclude an optimal clinical management . 
since in italy there are major economic , cultural and logistic differences in different regions , the same course with the same structure was repeated in three different parts of the country to be even closer to the real life . interestingly , some points were deemed as critical , independently from the meeting site and the different type of participants . 
indeed , in all cases a precise definition of tumor staging with ebus , navigational bronchoscopy or mediastinoscopy was required in both operable and inoperable patients , as per international guidelines [ 5 ]  . despite this almost complete agreement , the presented clinical cases , but also the personal experiences of the participants , showed that these minimally invasive methodologies are often not employed in the real clinical life . 
the availability of these technologies ( particularly ebus ) , low expertise and the waiting times emerged as main barriers to obtain a complete tumor staging . considering the increasing use of neoadjuvant therapies in locally advanced nsclc , staging either at first diagnosis and restaging before surgery have become even more important than in the past . 
indeed , it is well known that patients with persistent n2 disease or progression of cancer after neoadjuvant therapy have a worse prognosis and they could not derive much benefit from surgery [ 911 ]  . 
 therefore , insituations in which an accurate restaging of the nodal status is crucial to define the therapeutic intervention , a minimally invasive staging is suggested , independently from metabolic and radiological imaging . 
however , the participants in the three courses stressed the idea that histological restaging is the only trustable approach when a decision for surgery is pending . another major controversy in locally advanced nsclc management is the definition of surgical resectability . 
 according to esmo guidelines [ 5 ] , there are three resectable situations : single - station n2 disease where other nodal stations have been biopsied and proved to be not involved . 1 3 la radiologia medica ( 2020 ) 125 : 214219 table 2 answers from plenary discussion to the three questions proposed question answer ( s ) how could you improve the management of the clinical case ? which kind of behaviors should have been avoided in the management of the clinical case ? what are the main barriers that could prevent from the application of the international guidelines in the management of the clinical case in the daily practice ? invasive nodal staging ( and restaging after neoadjuvant treatment ) an objective definition of surgical resectability regular mdt with all crucial participants available ( at least surgeons , medical oncologists , radiation oncologists , pneumologists ) solitary decisions incomplete definition of the staging no patient involvement in the clinical decision absence of a regular and complete mdt ( southern and central italy ) time for discussion of clinical cases in the mdt and waiting lists for staging and therapeutic interventions ( northern italy ) t4n0 tumors where nodal disease had been excluded by invasive methods when a r0 resection is considered to be feasible . after induction therapy , when there has been nodal downstaging , a pneumonectomy can be avoided . the definition of unresectable tumor is even more loose , including all the situations in which a complete resection ( r0 ) would not be possible . 
this issue emerged also in the three meetings as a crucial point , since it creates a disparity between the different members of the mdt and a great disparity between different centers . 
essentially , the surgeons experience commonly drives the therapeutic decision in many intermediate situations , between the resectable single - station n2 disease and the clearly unresectablen3 tumor with bulky nodal involvement . 
all participants highlighted that resectability must be defined before starting with induction therapies ( systemic or local ) , because the decisions about induction are strictly related to the possibility of a future surgical intervention . 
from the literature , it is well known that a sequential approach is better tolerated but less effective than a concomitant treatment [ 13 ]  . a regular mdt including all the relevant specialties is still not present in some parts of italy with significant difference between the north and the south . 
this sounds unacceptable , since more and more literature data pointed out that a regular mdt has a significant impact on patients survival , particularly in challenging cases like most of locally advanced nsclc [ 14 , 15 ]  . considering that approximately 50% of nsclc patients are 70years of age at diagnosis , and approximately 15% are over 80years of age [ 16 ] , most participants suggested also that a geriatric evaluation should be included in the multidisciplinary evaluation of nsclc patients . 
both the international society for geriatric oncology and the national comprehensive cancer network recommend that elderly cancer patients perform a geriatric assessment a priori to treatment decisions to detect problems not promptly identifiable by routine physical examinations or medical history , predict treatment - related toxicities and survival , and support treatment decisions [ 17 , 18 ]  . conclusion the three italian meetings organized last year about the management of locally advanced nsclc showed that there is still great variability in the diagnostic management and treatment of locally advanced nsclc patients between different centers . 
although all participants know and approve the available international guidelines such as nccn , esmo and estro , in some cases that recommendations could not be completely adopted in the real clinical life due to logistic issues , waiting lists , paucity of well - trained staff and expertise represent the main barriers to their application . 
 a major educational effort both for physicians and stakeholders is needed in the next months and years to improve 1 3 218 la radiologia medica ( 2020 ) 125 : 214219 homogeneity and to offer state - of - the - art treatment to all patients . compliance with ethical standards conflict of interest dr alessio bruni - astra zeneca : support for conference participation , advisory board . 
the goal was to ensure conceptually equivalence with the original version and maintain clarity , ease of use and understanding . methods we conducted a multi - step linguistic process ( forward translation , backward translation and patient testing ) to generate and validate an italian translation of the vhnss . results two intermediate italian versions were created : the first italian version was derived from a reconciliation of the three forward translations , and the second italian version was derived from changes in the first version after the backward translation step . 
all investigators involved actively discussed possible solutions to produce a translated instrument that maintained a reading and comprehension level accessible by most respondents , without altering the meaning and content of the original source . 
this phase allowed patients to give suggestion in order to make items clearer and easier to understand : 43% of patients proposed a revision of the survey during the face - toface interview , and most of these suggestions were retained . conclusions a valid multi - step process leads to the creation of the final version of the vhnss - it , a suitable instrument to screen for symptoms in the italian hnc patients population and an official measurement tool that can be used in cooperative research group . keywords patient reported outcomes ( pro ) head and neck cancer symptoms screening radiotherapy introduction a symptom is a sensation or perception of change related to ones health . 
although some symptoms are common to all cancers , head and neck * marta maddalo marta.maddalo@gmail.com 1 department ofradiation oncology , asst spedali civili di brescia brescia university , piazzale spedali civili 1 , 25123brescia , italy 2 department ofradiation oncology , ospedale di esine asl vallecamonica - sebino , esine , italy 3 department ofmedicine , vanderbilt university medical center , nashville , tn , usa cancer ( hnc ) patients experience a host of unique problems which require special consideration : pain , dysphagia , xerostomia , dysgeusia and dysarthria are just some of them [ 13 ]  . 
other symptoms , instead , could be assessed both by subjective and objective measures : for example , dysphagia is a symptom related to alterations in swallowing which can be assessed subjectively by patient self - report or objectively by a modified barium swallow study . patient reports have the benefit of being brief , inexpensive and amenable to repeated measures . 
an instrument sensitive to hnc symptoms could lead to their accurate identification vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 228235 and quantification , allow earlier interventions for individual patients and serve as a research tool to compare the symptom burdens associated with various treatment options . 
the vhnss was designed and tested in a series of five studies involving 332 patients over a seven - year period ( 20002007 ) , by the pain and symptom management program research team ( psmp - rt ) of the vanderbilt ingram cancer center ( nashville , tn ) , showing excellent psychometric properties [ 5 ]  . 
 at the beginning of the questionnaire 3 yes or no questions identify the presence or use of a feeding tube , dentition and dentures : this information was deemed important in the interpretation of subsequent questions . 
several questions have the option for not applicable because they are not pertinent to all patients . the aim of this prospective observational study was to linguistically validate the italian translation of the vhnss and to conduct a pilot test on the translated survey to assess both the feasibility and utility of its administration in clinical practice . 
the developers of the vhnss were contacted and asked for permission to use the instrument , and they were involved in the study design and process and into the writing and review of this manuscript . 
the protocol was approved by the ethical committee of the spedali civili di brescia hospital , and the study was activated in february 2015 ( id number 1925 )  . 
results on the pilot study on feasibility and utility will be discussed in a companion paper . materials andmethods study design at the ispor ( the international society for pharmacoeconomics and outcomes research ) third annual european congress , which took place in 1999 in antwerp , belgium , the translation and cultural adaptation group ( tca group ) was formed to create guidelines and standards for the translation and cultural adaptation of patient - reported outcome ( pro ) measures . 
this group reviewed available translation methods , and in 2005 published a report principles of good practice for the translation and cultural adaptation process for patient - reported outcomes ( pro ) measures on the appraisal of their strengths and weaknesses , suggesting a multi - step linguistic validation process [ 6 ]  . 
this study followed this multi - step linguistic validation process , herein reported in its three major steps : the forward translation , the backward translation and the patient testing . 
the aim of this linguistic validation was to produce a translated version of the vhnss into italian language , which was conceptually equivalent to the original version , clear and easy to understand . forward translation step the forward step is the translation of the questionnaire from the source language ( us english ) into the target language ( italian )  . 
three radiation oncologist of the head and neck radiation oncology team of the radiation oncology department of brescia university ( here called forward translators ) independently produced a forward translation of the original items , instructions and response choices . 
 it was felt that content experts were more appropriate for translation than professional translators because they were familiar with the content , they were proficient in the hnc literature and guidelines and they were involved in editing papers in the english language . 
the choice of the three forward translators met the guidelines definition : translators are individuals who have been formally trained as translators and have training or experience in translating questionnaires , or they are individuals who have not necessarily undergone formal training in translation but who have the necessary skill , knowledge , and professional experience in the conduct of survey translation that is necessary to produce a professionally translated data collection instrument [ pany , de la puentem . 
 this step aimed to produce a single reconciled version , conceptually equivalent to the original questionnaire , in a colloquial and easy to understand italian language . backward translation step the backward step is the translation of the forward reconciled version back into the source language ( english )  . 
it was performed by a professional , native speaker of the target language and fluent in the source language ( here called backward translator ) , without having access to the original source . 
1 flow diagram la radiologia medica ( 2020 ) 125 : 228235 mistranslations or inaccuracies in the intermediary forward version of the questionnaire . patient testing step the aim of this preliminary test was to administer the translated questionnaire to a sample of 35 respondents to determine whether the translation was clear ( instructions , items and response choices ) , simple and appropriate . 
the sample size was calculated following the formula [ 7 ] : n = z2x p ( 1 p ) d2 where n = sample size , z = z statistic for a level of confidence , p = expected prevalence and d = precision . 
 p was the prevalence of comprehension problems per single itesince the vhnss survey was already tested for reliability and validity in the original language ( comprehension test of the first version of the questionnaire performed on 23 patients ) , it was estimated a low prevalence ( < 10% ) of comprehension problems due exclusively to the translation process . eligibility criteria included : ( 1 ) 18 and over years of age ; ( 2 ) diagnosis of hnc ( first diagnosis , recurrence or metastatic settings ) : all histology and all cancer sites ( rhinopharynx , oropharynx , hypopharynx , larynx , oral cavity , salivary gland , nasal cavity and paranasal sinus ) were accepted ; and ( 3 ) native speakers of the target language . 1 3 la radiologia medica ( 2020 ) 125 : 228235 participants were asked to fill the italian version of the questionnaire in a paper format . 
the forward translator inquired whether the patient had any difficulty in understanding the questionnaire and checked the patients interpretation of all items , in order to identify and correct errors introduced through the translation process . 
the aim of this step was to outline the difficulties encountered by patients , the solutions suggested and retained and to provide the final version of the italian questionnaire ( vhnss - it )  . 
finally , to ensure the strength of the translation process , a 10 - member team of reviewers with skills and professional experience in the field of head and neck cancer treatment was asked to rate the items in order to define the content validity index ( cvi )  . 
all members were asked to rate each question and item with yes and no , where yes was given a score of one and no was given a score of zero according to a binary scoring system [ 8 ]  . 
both the item - level cvi for single items ( number of experts answering yes divided by the number of total experts involved ) and the scale - level cvi for the overall scale ( sum of all items cvi divided by the total number of items ) were calculated [ 9 ]  . results forward translation the three forward translators independently produced a translation of the vhnss ( forward translation a , b , c )  . 
they all found the majority of the items easy to translate , and they all encountered problems with the following questions : 1st yes or no question : i currently have a feeding tube in place . 
the pi and the forward translator agreed on mentioning both the peg and the nasogastric tube in order to include all patients undergoing enteral nutrition . items 9 and 10 : i choke or strangle on liquid and i choke or strangle on solid foods . 
on this purpose , subject and direct object were reverted . items 12 , 13 and 47 : subject and direct object were reverted in order to make the question easier to understand in italian language . backward translation the backward translator translated the first italian version back into english , without having access to the original us english version of the questionnaire . 
during a meeting with the forward translators , all the items were re - discussed , comparing the backward version with the original source , in order to explore alternative italian translations . 
as it was expected , the backward translation was different from the original source : the translators although agreed that there were not differences attributable to error in the translation process and that the meaning of the original source was maintained . 
 the backward translator was concerned that the verbiage of the first version of the italian questionnaire was still scholarly because the forward translations were made as close to the original version as possible : the discussion between the forward and the backward translators basically centered on making the items easier to understand . 
included in the table are the original items , their italian translation in the initial version derived from the forward translation and the changes made based on the backward translation . patient testing thirty - five hnc patients have been recruited between march and april 2015 . 
all patients approached were willing to participate in the study , and all of them completed both the questionnaire and had the face - to - face interview with one of the forward translators . 
nine patients ( 26% ) asked the permission to fill the questionnaire with the help of the caregiver : median age of this group of patients was significantly higher than the median age of patients who filled the questionnaire by themselves ( 76 years versus 61years , p = 0 , 004 )  . 
one patient 86years old was alone when he completed the questionnaire : at the time of the face - to - face interview , he told the pi that he had had difficulties with most of the questions , especially understanding the yes or 1 3 232 la radiologia medica ( 2020 ) 125 : 228235 table 1 changes of item translation between the first and the second italian version original item ( us english ) first italian translation second italian translation 7 . 
problems with dry mouth make chewing il cibo mi rimane a lungo in bocca il cibo mi rimane a lungo in gola i problemi di secchezza della bocca mi renil cibo mi rimane fermo in bocca il cibo mi rimane fermo in gola la bocca secca mi rende difficile masticare e and swallowing difficult dono difficile masticare e deglutire deglutire 16 . 
problems with dry mouth affect my ability i problemi di secchezza della bocca influenla bocca secca mi rende difficile dormire to sleep to talk zano la mia capacit di dormire zano la mia capacit di parlare 17 . 
i have less desire to eat due to taste change ho perso la voglia di mangiare a causa il gusto alterato dellalterazione del gusto i sapori sono alterati ho meno voglia di mangiare a causa dellalterazione dei sapori 35 . 
my taste changes have altered the foods lalterazione del gusto ha modificato la scelta lalterazione dei sapori ha modificato i cibi che that i choose to eat dei cibi che mangio scelgo di mangiare 36 . 
my taste changes have caused me to lalterazione del gusto mi ha portato a ridurre lalterazione dei sapori mi ha indotto a ridurre decrease the amount of food i eat 37 . 
i have altered what i eat due to a change in la quantit di cibo che mangio il mio senso dellolfatto cambiato ho modificato quello che mangio a causa del la quantit di cibo che mangio la percezione degli odori alterata ho modificato quello che mangio a causa my sense of smell cambiamento nel senso dellolfatto dellalterazione nella percezione degli odori 49 . 
i have limitations in the ability to open or ho dei limiti nella capacit di aprire e muofaccio fatica ad aprire e muovere la bocca move my jaw vere la mandibola 50 . 
i have limitations in the ability to move ho dei limiti nella capacit di muovere il collo faccio fatica a muovere il collo e le spalle my neck and shoulders e le spalle no question on the feeding tube dependency and items 3 , 4 , 9 , 10 , 13 , 15 , 16 , 17 , 22 , 27 , 31 , 34 , 35 , 36 , 38 and 47 . 
one patient 70years old , who completed the questionnaire with the caregiver help , did not understand the meaning of the question 47 ( in the original source : burning pain in the lining of my mouth and throat changes when i eat ; in the second italian version : ho modificato quello che mangio a causa del bruciore allinterno della bocca e della gola )  . 
the caregiver said that the question was clear and they both had no suggestions for changing the item . all the other patients found both the meaning of the questions and the response choices to be clear . 
among these 33 patients , 18 did not recommended any change , while 15 suggested minor revision to the forward translator , mostly related to the graphic aspect of the translated survey : table3 reports these suggestions , if investigators decided to retain or reject them , and an explanation about the decision . 
with changes to the second italian version , made on the basis of the retained patients suggestions , the translators produced the final and official version of the italian questionnaire , the vhnss - it . content validity all 10 reviewers independently rated the three yes / no questions and the 50 items of the questionnaire in order to define the cvi . 
the scale - level cvi for the overall scale was 0.95. discussion symptoms experienced by hnc patients may be profound and have enduring impact on long - term survivors [ 1012 ]  . 
 this is in large part related to the fact that hnc arises from and involves anatomical structures that are critical for vital activities such as swallowing , speaking and even breath . 
the multidimensionality of qol refers to the coverage of a broad range of content usually encompassing physical , functional , psychological , social and spiritual domains : symptoms are a component of qol assessment , but the emphasis of qol assessment is on the overall sense of well - being , not on specific contributing factors . 
however , in this setting , the goal is to garner an understanding of overall well - being , not to understand a specific symptom control issue or symptom complex . 
thus , qol tools and symptom tools provide important but distinctive information . a number of tools have also been developed to assess symptoms in the hnc population [ 19 , 20 ] , but none of them was available in italian language at the time of the present study . 
anderson symptom inventory ( mdasi ) was designed to measure multiple symptoms related to cancer and its treatment and represents a 13 - item core that includes a basis for judging the burden of symptoms for all patients . 
the principal goal of the ideators of the vhnss was to develop a quick tool that can help healthcare providers to identify symptoms in hnc patients in a timely manner allowing early referral for specialty care , educational materials and pharmaceutical or non - pharmaceutical intervention . 
the items can be grouped into 10 subscales ( mouth pain , general pain , swallow solid , swallow liquid , nutrition , mucus , dry mouth , speech / communication , taste / smell and dental health ) and three single items ( hearing , jaw range of motion and neck / shoulder range of motion )  . the aim of the present paper was to report the linguistic validation process that has led to the creation of the vhnssit . 
 two intermediate italian versions were created during the process : the first italian version was derived from a reconciliation of the three forward translations , and the second italian version was derived from changes in the first version after the backward translation step . 
all investigators involved in these two phases actively discussed possible solutions to produce a translated instrument that maintained a reading and comprehension level accessible by most respondents , even of a low education level , without altering the meaning and content of the original source . 
during the patient testing step , only two patients reported problems with items comprehension and the rate of comprehension problems per single item was lower than expected : 2.9% in 16 items and 5.7% in 1 iteduring this phase of the study , patients were allowed to give suggestion to the investigators in order to make items clearer and easier to understand : 43% of patients proposed a revision of the survey during the face - to - face interview , and most of these suggestions were retained . the expert panel evaluating the content validity of the scale found the vhnss - it to be a suitable and an equivalent of the original instrument to measure symptoms in italian hnc patients , with a cvi higher than 90% for the scalelevel cvi and for almost all the single item - level cvis . thus , the linguistic validation process resulted in an official instrument , the vhnss - it , that can be included in international clinical trials and cooperative research studies [ 22 ]  . conclusions a valid multi - step process leads to the creation of the final version of the vhnss - it . 
a pilot study on the vhnss - it to assess feasibility and utility , both for patients and for clinicians , of its administration in clinical practice has already been carried on and results will be available in an upcoming paper . 1 3 234 la radiologia medica ( 2020 ) 125 : 228235 1 3 la radiologia medica ( 2020 ) 125 : 228235 acknowledgements all authors gratefully thank the 10 - member team of reviewers for their precious help : a . 
grisanti from the medical oncology unit , department of medical and surgical specialties , radiological sciences , and public health , university of brescia and asst spedali civili , brescia , italy ; f . 
the least absolute shrinkage and selection operator ( lasso ) was used to select radiomics features , and then , the logistic regression ( lr ) model was established using fivefold cross - validation to predict the ki - 67 index . 
the performance was evaluated by receiver - operating characteristic ( roc ) analysis , accuracy , sensitivity and specificity . results quantitative imaging features ( n = 1029 ) were extracted from adc maps , and 11 features were selected to construct the lr model . 
gallen panel suggests using immunohistochemical ( ihc ) biomarkers including estrogen receptor ( er ) , progesterone receptor ( pr ) , human epidermal growth factor receptor 2 ( her2 ) and ki - 67 as substitutive molecular subtypes [ 2 ]  . ki - 67 is a non - histone nuclear protein expressed during every active phases of the cell cycle , except g0 , and also an important factor in the synthesis of ribosomes in dividing cells . 
for breast cancer , ki - 67 has been proposed as a clinically valuable marker to distinguish the two subtypes of er - positive and her2 - negative breast cancers as luminal a and luminal b breast cancers . 
luminal a subtypes were vol . : ( 0123456789 ) 1 3 110 la radiologia medica ( 2020 ) 125 : 109116 less responsive to chemotherapy , whereas luminal b subtypes were responsive not only to chemotherapy but also to endocrinotherapy plus molecular - targeted therapy [ 4 ]  . 
 from 41 studies ( including 64 , 196 breast cancer patients ) was reported that there was a distinct correlation between ki - 67 expression and disease - free survival and overall survival [ 5 ]  . therefore , early detection of such highly malignant breast cancer has great significance in aspects of patients prognosis , diagnosis and treatment . 
on the contrary , imaging can provide overall anatomical and functional properties of tumor tissue . diffusion - weighted imaging can use the diffusion motion of water molecule invivo to display the spatial information and cell density in human tissues at molecular level [ 6 ]  . 
moreover , adc values are related to the ki - 67 index according to previous studies [ 7 ]  . at present , the technology of imaging has gradually developed toward the direction of automated analysis and high - throughput extraction of quantitative features which perfectly concluded the conception of radiomics [ 810 ]  . 
radiomics is a procedure which is designed to extract a great number of quantitative features from digital images , and further , highly diversified statistical analysis is used to obtain the key information from the data pool . 
recently , most studies on radiomics mainly focus on topics in respects of tumor molecular subtype [ 11 ] , diagnosis [ 12 , 13 ] , stage classification [ 14 ] , genetic phenotype prediction [ 15 ] , treatment selection [ 16 ] and tumor prognosis [ 17 ]  . 
in a study by liang , c , a radiomics classifier based on t2wi was an important predictor of ki - 67 index in breast cancer patients [ 18 ] which suggested that noninvasive evaluation of the ki - 67 index can be performed preoperatively by radiomics . no studies have been done so far to evaluate the correlation between dwi - mri and the ki - 67 index based on radiomics . 
therefore , our work aims to assess the accuracy of adc - based radiomics to noninvasively predict the ki - 67 index in patients with breast cancer preoperatively . materials andmethods patients our institutional review board approved this retrospective study and abandoned the informed consent requirement . 
 inclusion criteria include : ( 1 ) all patients had undergone dwi - mri ; ( 2 ) no treatment received before surgery ; ( 3 ) pathologically verified invasive ductal breast cancer ; ( 4 ) ihc examination including the ki - 67 index . ultimately , 128 patients were analyzed and randomly divided into the training dataset ( n = 101 ) and the test dataset ( n = 27 ) by 80% and 20% . immunohistochemistry ofki67 the expression status of ki - 67 was measured via standard ihc examinations . 
less than 14% positive staining was identified as negative expression , while more than 14% positive staining was identified as positive expression [ 2 ]  . mr data acquisition magnetom verio 3.0t system ( siemens , erlangen , germany ) ( 81 patients ) or a discovery mr750w 3.0t system ( general electric healthcare , ge , milwaukee , usa ) ( 47 patients ) was applied together with an eight - channel phasedarray breast coil which was placed under the patient in a prone position . 
then , the computer automatically generated the three - dimensional volume of interest ( voi )  . intensity normalization the inconsistency in intensity information is unavoidable in imaging and storage of medical images . 
we normalized the intensity of the mri image using the following formula to minimize the intensity inconsistency [ f ( x ) the normalized intensity , x the original intensity , mean value , variance , s optional scaling , by default , it is set to 1 ] [ 19 ]  . f ( x ) = x x radiomics feature extraction a total of 1029 features were extracted and divided into three categories : first order statistic , shape - based and texture . 
the latter includes gray level co - occurrence matrix ( glcm ) , gray level run length matrix ( glrlm ) and gray level size zone matrix ( glszm )  . 
the features were extracted using radcloud platform ( huiying medical technology ( beijing ) co . , ltd ) [ 20 ]  . statistical analyses statistical analysis of the characteristic of patients in the training and validation sets was assessed using spss software ( version 24 , ibm )  . 
a two - sided p value < 0.05 was used to indicate statistical significance . all of the other analysis was performed using radcloud platform ( huiying medical technology ( beijing ) co . , ltd ) [ 20 ]  . least absolute shrinkage and selection operator ( lasso ) controls the complexity of the model through a series of parameters to avoid overfitting . 
for example , it has a tuning parameter to control the penalty of the linear model , which guarantees the minimum penalty when obtaining a model with a smaller number of features , where the penalty is mean square error ( mse )  . 
the optimization goal of lasso is 2n_samples y xw 2 + alpha x the matrix of radiomic features , y the vector of the sample labels , n the number of samples , w the coefficient vector of the regression model , alpha w , lasso penalty . the best parameter set was computed using a crossvalidation method with fivefolds . 
logistic regression is a classification model that mainly solves the two - classification problethe process of logistic regression is to establish a cost function for a regression or classification problem and then iteratively obtain the optimal model parameters through the optimization method . the function of the logistic regression model is t x f ( x ) = g 1 + et x among them , g ( z ) = 1 the l1 regularized logistic regression solves the fol1 + ez lowing optimization problem : y = min 1 + c i w + c i = 1 x the matrix of radiomic features , y the vector of the sample labels , w the coefficient vector of the lr model , c inverse of regularization strength . the training data were randomly divided into five groups , of which every four groups were chosen as the training set and the remaining group as the validation set . 
the average value of the five results was adopted to assess the generalization of the classification models and the accuracy of the algorithm . 1 3 112 la radiologia medica ( 2020 ) 125 : 109116 we evaluated the performance of selected features in classifying patients according to their ki - 67 level . 
we evaluated the performance of selected features in classifying patients according to their ki - 67 level by receiveroperating characteristic ( roc ) analysis , and calculated the area under the roc curve ( auc ) , accuracy , sensitivity and specificity . result the radiomics workflow and study flowchart of the study are depicted in fig.1. patients characteristics a total of 128 patients ( 53 11years ) were recruited in this study . 
the detailed clinical characteristics of patients in the training and validation sets are listed in table2 . table 2 characteristics of patients in the training and validation sets characteristic training set validation set p value no . 
a mean squared error ( mse ) path , b lasso path using lasso model , 11 features which are correspond to the optimal alpha value were selected discussion exponential_firstorder_median , original_firstorder_minimum , original_shape_surfacevolumeratio , original_glcm_clustershade , square_glcm_idmn , square_firstorder_skewness ( table3 )  . in this study , we investigated whether features derived from adc maps of patients with invasive ductal breast cancer could be used as a preoperative predictor of the ki - 67 index . 
 the radiomics classifier demonstrated high performance for differentiation between low and high ki - 67 index . many previous studies have mentioned immunohistochemical expression of ki - 67 as a prognostic and predictive marker for breast cancer [ 21 ]  . 
but as we mentioned , core needle biopsy testing only takes part of the tumor sample table 3 description of the selected radiomic features radiomics feature radiomic group feature class filter skewness robustmeanabsolutedeviation runlengthnonuniformitynormalized skewness correlation median minimum surfacevolumeratio clustershade idmn skewness firstorder firstorder glrlm firstorder glcm firstorder firstorder shape glcm glcm firstorder wavelet - lll squareroot exponential wavelet - hlh wavelet - lhh exponential original original original square square 1 3 114 la radiologia medica ( 2020 ) 125 : 109116 density , proliferation index and more aggressive . 
in previous studies of invasive duct cancer , adc showed negative correlations with the ki - 67 index , as by li , l and colleagues on 124 patients , and molinari and colleagues on 115 patients [ 7 , 24 ]  . 
another reason for us to compute the radiomic features on adc maps is the ability to assess the motion of water molecules shows good reproducibility between different mr systems with same field strength and the same range of b - values [ 25 , 26 ]  . 
this characteristic indicates that they are useful in multicenter studies because the scanners are usually different . the concept of radiomics was first proposed by dutch scholar lambin , the idea of which originated from tumor heterogeneity , in 2012 [ 27 ]  . 
breast cancer has a high degree of heterogeneity , and there are different image performance because of its different lesion size , shape , brightness and texture features values [ 29 ]  . 
in our study , we used radiomics to quantitatively extract the characteristics of the tumors internal diffusion based on the adc map , thereby reflecting the inhomogeneous characteristics of the tumors internal structure . 
in our research , three - dimensional analysis of the entire tumor was used , which can take full account of the heterogeneity of the breast cancer . this study used lr to construct a radiomics model for predicting the ki67 index of invasive ductal breast cancer . 
fusco [ 30 ] reported that a multiple classifier system combining decision tree and bayesian classifier can optimize the accuracy for breast lesion classification ( twenty - six malignant and 22 benign breast lesions )  . 
thus , there is room for radiological improvement to assist in assessing the actual ki - 67 index . dwi as a supplementary diagnostic sequence for breast lesions shows an important clinical role [ 22 ]  . 
the pathological mechanism of adc value applied to breast tumors is that the proliferation of tumor cells can lead to an increase in cell quantity , a disordered tissue structure and the narrowing of extracellular space , which eventually result in a restricted motion of water molecules in the intercellular spaces of tissues [ 23 ]  . 
tumors with lower adc values have a higher cell 1 3 la radiologia medica ( 2020 ) 125 : 109116 used in our study and more algorithms should be tested in future research . the limitation of this study is that the number of patients is not large enough . 
it must be emphasized that even if a radiomics classifier shows good results for a small number of patients , it must be validated with a larger sample before it can be extended to clinical use [ 35 ]  . 
however , we believe that these data are sufficient enough to prompt a larger clinical research on the value of radiomics based on adc maps in the ki - 67 index , allowing better decisions on preoperative prediction indications . 
in the end , future studies are required to assess the value as well as feature repeatability of radiomics biomarkers in independent and prospective validation cohorts by using larger sample size . in summary , our adc - based radiomics classifier can effectively predict ki - 67 index in patients with invasive ductal breast cancer before surgery . 
this radiomics classifier may help to preoperatively predict ki - 67 index in breast cancer patients . acknowledgements this research was supported in part by grants from the national natural science foundation of china ( #81771804 )  . compliance with ethical standards conflict of interest the authors have declared that no competing financial interests exist . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
this article does not contain any studies with animals performed by any of the authors . informed consent for this type of study , formal consent is not required . la radiologia medica ( 2020 ) 125 : 220227 radiotherapy acute andlate toxicity andpreliminary outcomes report ofmoderately hypofractionated helical tomotherapy forlocalized prostate cancer : amonoinstitutional analysis francescocuccia1 gianlucamortellaro2 giovannatrapani1 vitovalenti1 luciaognibene3 giorgiadegregorio1 emanuelequartuccio1 nicolettaluca1 antonellatripoli1 vincenzoserretta4 antoniolocasto5 giuseppeferrera2 received : 9 august 2019 / accepted : 2 october 2019 / published online : 22 october 2019 italian society of medical radiology 2019 abstract aims to assess toxicity and clinical outcomes of moderately hypofractionated helical tomotherapy ( ht ) for the curative treatment of localized prostate cancer ( pc )  . methods from december 2012 to may 2018 , 170 patients were treated with definitive intent for pc . 
all patients received 70gy in 28 fractions to the prostate ; 61.6gy were delivered to the seminal vesicles for ir ; pelvic lymph nodes irradiation for a total dose of 50.4gy was added in the hr subgroup . 
at the time of analysis , 2and 3 - year biochemical relapse - free survival rates were 90% and 87.5% and 2and 3 - year overall survival rates were 96.4% and 90% , respectively . 
the radiobiological rationale for the use of > 2gy per fraction lies on the low / ratio of prostate cancer ( about 1.5gy ) compared to the nearby healthy structures [ 3 ] ( i.e. , 3gy for rectum and 510gy for bladder ) ; besides the favorable therapeutic ratio of a tumor more sensitive to higher doses per fraction , hypofractionated schedules may be more attractive in terms of vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 220227 patients compliance and cost - effectiveness for the shortening of the overall treatment time [ 4 ]  . 
currently , mature data from several phase iii randomized trials confirmed that moderately hypofractionated schedules ( 2.24.0gy per fraction ) reported similar tumor control and toxicity rates compared to conventional fractionation [ 5 ] , and recent aua / astro guidelines recommend their routine use [ 6 ]  . herein , we report the results of our retrospective study evaluating 170 patients with localized prostate cancer treated with moderate hypofractionation in simultaneous integrated boost ( sib ) using helical tomotherapy ( ht , accuray , inc . , sunnyvale , ca , usa )  . materials andmethods this is a retrospective analysis of 170 patients with biopsyproven diagnosis of prostate adenocarcinoma who were treated at our center with moderately hypofractionated radiotherapy . primary endpoints of the present study were acute and late genitourinary and gastrointestinal toxicities . 
patients characteristics are summarized in table1 . pre - treatment evaluation consisted of physical examination including digital rectal examination , blood tests including psa levels , bone scan and abdominal ct or mri , if needed for staging . 
inclusion criteria were : histologically confirmed diagnosis of prostate cancer , karnofsky performance status 60 , no history of prior pelvic radiotherapy and absence of active chronic inflammatory bowel disease . 
androgen deprivation therapy was prescribed according to nccn guidelines for all intermediateand high - risk patients , respectively , for 6months and 23years . for radiotherapy treatment planning , a 2.5 - mm - slicethick ct scan , from the fourth lumbar vertebra to 2cm below the femoral neck , was acquired with the patient in supine position with flexed legs and kneeankle immobilization devices . 
to obtain a reproducible rectal emptying and bladder filling , patients were required to perform a fleet enema 2hours prior to the examination and to drink 500ml of water 30min before the scan . 
the same protocol was applied during treatment for each fraction . regarding target volume delineation , for low - risk patients only a ctv1 consisting of the prostate gland was contoured . 
for all the target volumes , the prescription dose was 95% of ptv covered by at least 95% of the prescribed dose . rectum , bladder , femoral heads and intestinal loops were delineated as organs at risk ( oars ) , and the following constraints were applied : v65 < 15% for rectum and v55 < 50% and v60 < 30% ; v56 < 35% , v60 < 25% for bladder ; dmax < 50gy and v46.2 < 5% for femoral heads ; for intestinal loops , the prescription was to reduce the dose as low as reasonably achievable . 
treatment planning was performed using the tomotherapy planning systeradiotherapy was delivered with helical tomotherapy ; the image - guided system was based on the daily execution of a megavoltage ct scan ( mvct ) prior to each fraction in order to verify setup accuracy and rectal and bladder preparation . 
during the treatment course , a weekly evaluation of the patients was carried out ; after rt , follow - up visits were scheduled every three months for the first year and then at biannual intervals . acute and late toxicities were prospectively collected and assessed using common terminology criteria for adverse events ( ctcae ) v4.0 , defining acute events as any rtrelated symptom occurring within 90days from the start of treatment . 
health - related quality of life ( hrqol ) in particular for bladder and gastrointestinal function was assessed with expanded prostate cancer index composite ( epic - 26 ) questionnaire at baseline , at 3 - month follow - up and then at annual intervals . 1 3 222 la radiologia medica ( 2020 ) 125 : 220227 concerning clinical outcomes , biochemical failure was defined following phoenix criteria as the identification of the nadir value of psa + 2ng / ml after radiotherapy with / without androgen deprivation therapy . medians and ranges were calculated for continuous variables . 
the following clinical parameters were evaluated : age 75years , comorbidities ( hypertension , diabetes , inflammatory bowel disease , previous abdominal surgery , turp ) and pelvic rt administration ; for dosimetric parameters , we investigated : rectal dmax , v56gy , v60gy and v65gy ; bladder dmax , v55gy , v60gy , v70 gy and for ptvs mean , maximum and minimum dose . 
among these 12 cases , five subjects ( one low risk , two intermediate risk and two high risk ) developed distant metastases , consisting of three nodal recurrences , successfully treated with stereotactic body radiotherapy , and two bone metastases who underwent palliative treatment . 
our radiotherapy schedule was adopted from the favorable results of the largest series of moderately hypofractionated radiotherapy [ 7 , 8 ] , and we reported excellent rates of acute and late toxicity , similar to other experiences reported in the literature [ 918 ] ( table3 ) ; also in terms of biochemical control , our rates are in agreement with previous studies . 
no clinical or dosimetric parameters were found to be predictive of late toxicity ; more specifically , in our series whole pelvis irradiation did not have an impact on gi adverse events incidence . 
 [ 20 ] , observing that larger volume of nodal ctv and increased age were predictive factors of acute bowel toxicity . this finding is also reported in a recent study by jorgo etal . 
 among the randomized trials of comparison between moderate hypofractionation and conventional fractionation , only the fox chase experience included whole pelvis irradiation , reporting similar gi rates with a negligible impact on quality of life [ 22 ]  . the controversial role of pelvic lymph nodes irradiation in high - risk disease is also confirmed by three randomized trials [ 2325 ] that reported no advantages in terms of biochemical control or os , and one reporting on the contrary a gain in biochemical relapse - free survival by adding pelvic lymph nodes radiotherapy [ 26 ]  . 
recently , preliminary data from the pivotal trial were published : this trial randomizes patients to prostate only radiotherapy versus prostate + pelvic lymph nodes rt with the aim to address the real impact of whole pelvis irradiation on clinical outcomes for locally advanced disease . 
despite the lack of a cohort of comparison with conventional fractionation , these data report a mild profile of toxicity , in agreement with a metaanalysis conducted by carvalho etal . 
the authors underline the role of igrt for the safe delivery of moderate hypofractionation , also providing a cost - effectiveness advantage in terms of overall treatment time , and a favorable impact on biochemical control . 
nowadays , there is weak evidence that hypofractionation may be superior to conventional treatment in terms of biochemical relapse - free survival , but non - inferiority trials [ 1012 ] have demonstrated that moderately hypofractionated schedules are not worse than 2gy per fraction regimens , providing an iso - effective and iso - tolerable therapeutic option . this study has several limitations : the retrospective nature limits the statistical power of the present series , despite toxicity being prospectively collected ; in a large part of our population , especially for intermediate - risk patients , adt has been administered following previous guidelines recommendations that now have changed , so this factor might have an impact on our results in terms of biochemical control ; furthermore , we have already mentioned the lack of a cohort of comparison with a conventionally fractionated schedule , and our follow - up time is relatively short , although being comparable to other literature series . conclusions the use of moderate hypofractionation with sib by means of helical tomotherapy reports mild acute and late toxicity . 
we acknowledge their contribution to the literature on using tridimensional endoanal ultrasound ( 3d - eaus ) for preoperative assessment of simple and complex anorectal fistulas , a topic worthy of discussion with potential clinical implications . we would like to add a few points for consideration . 
in our centre , we primarily use endoanal ultrasound for prostate biopsy , and in our experience , performing these examinations even under sedation was challenging due to pain from the anal distension , and this is exacerbated in anxious patients . 
in addition , one of the biggest advantages that mri offers is its ability to evaluate the fistulas relationship to the anal sphincter complex , the presence of secondary tracts and abscesses , and detection of any possible extension to the supralevator fossa or ano / recto - vaginal fistulous involvement [ 3 ]  . 
 additional limitations with 3d - eaus when compared to mri include inability to differentiate between scar and inflammatory tissue in patients with prior surgery while acoustic shadowing deep to the track from gas bubbles produced by hydrogen peroxide limits assessment deep to the inner surface of the track [ 4 ]  . 
the authors also do not comment on the ability of 3d - eaus to determine whether the fistula is intersphincteric or transsphincteric , an important component of fistula characterization that is well evaluated on mri [ 5 ]  . the authors mention that based on their results 3d - eaus appeared superior to mri in the detection of the internal opening . 
could this be because no gadolinium contrast was used for the mri protocol at the authors institution ( many institutions perform mri with gadolinium as standard for vol . : ( 0123456789 ) 1 3 156 la radiologia medica ( 2020 ) 125 : 155156 perianal fistula assessment ) , as studies have shown that mri is superior to endoanal ultrasound for identification of the internal opening [ 5 ]  . 
all 480 cases were assessed by four different methods , as follows : complete pan with clinical examination of each tooth available and not available , respectively , and small portion of pan in which a root with crown and root without crown were displayed , respectively . 
as regards teeth without endodontic treatment , accuracy was higher for complete pan in the upper / lower incisive area and for small portion of pan in the upper molar area . 
2 , university offlorence azienda ospedaliero - universitaria careggi , largo brambilla 3 , 50134florence , italy 2 department ofhealth science , university offlorence , viale morgagni 48 , 50134florence , italy 3 department ofexperimental andclinical biomedical sciences , nuclear medicine unit , university offlorence azienda ospedaliero - universitaria careggi , largo brambilla 3 , 50134florence , italy 4 department ofradiology , university offlorence azienda ospedaliero - universitaria careggi , viale morgagni 85 , 50134florence , italy vol . : ( 0123456789 ) 1 3 146 introduction apical periodontitis ( ap ) is a periapical bone lesion caused by microorganisms penetrating into the root canal up to the apex [ 1 ]  . 
ap lesions are infrequently present with clear clinical signs and are almost always identified by incidental findings during routine examinations carried out by periapical radiography and panoramic radiography ( pan ) [ 3 ]  . 
since an ap might be present even when it is not radiographically identified , cone - beam computed tomography ( cbct ) imaging is currently considered to be the most powerful tool to recognize periapical bone lesions [ 710 ]  . 
cbct is only moderately affected by metal artifacts [ 1114 ] and has a high spatial resolution [ 15 ] with a relatively low radiation dose compared to multi - slice computed tomography [ 16 , 17 ]  . 
it must be performed only in patients with unclear or contradictory clinical signs / symptoms and when additional information can potentially change the treatment planning or postoperative outcomes [ 23 , 24 ]  . 
 therefore , knowing the capability of detecting a periapical bone lesion via two - dimensional imaging is crucial . several papers that assessed the diagnostic accuracy of pan in identifying ap lesions employed analog x - ray units [ 5 , 25 , 26 ]  . 
since the breakdown of a picture causes an improvement in the image quality as perceived by the human eye [ 28 , 29 ] , in the analysis of ap lesions it could be beneficial to assess the role of digital panoramic radiographs which , thanks to efficient software systems , enable effortless electronic processes opening the way to new diagnostic methods . the aim of this retrospective study was to evaluate the diagnostic accuracy of both digital complete and small portion of pan in the detection of clinically / surgically confirmed asymptomatic ap lesions with and without endodontic treatment . la radiologia medica ( 2020 ) 125 : 145154 materials andmethods patients between november 2011 and december 2017 , we enrolled via cbct imaging 480 patients divided in four groups , as follows : patients with at least one ap in teeth with ( 120 ) and without ( 120 ) endodontic treatment and patients without periapical bone lesions in teeth with ( 120 ) and without ( 120 ) endodontic treatment . 
the clinical queries for cbct examinations were implant planning , dental extractive planning , maxillary sinusitis , focal bone lesions , endodontic planning , post - traumatic fracture , and osteomyelitis . 
 all the 240 patients without endodontic treatment were the same as a previous study [ 31 ] , whereas the 240 patients with endodontic treatment were randomly selected by a larger sample from another previous study [ 32 ]  . 
each of the 480 patients underwent a pan first and a cbct scan within 40days of the pan . devices pan was performed via the orthoceph oc200 d ( instrumentarium dental , tuusula , finland )  . 
it was a digital panoramic radiograph with a rotation time of 17.6s , 66kv , and 4.27.5ma. cbct imaging was performed via the newtom 5g ( qr srl , verona , italy ) equipped with a pulsed pyramidal x - ray beam ( 360 rotation ) , a very small focal spot ( 0.3mm ) , and an amorphous silicon flat - panel detector ( 20 25cm )  . 
 the protocols used for imaging , called hi - res - regular and hi - res - enhanced by the producer , lasted 26 and 36s and comprised 360 and 480 basis image frames , respectively . 
pan and cbct images were displayed on a 20 - inch medical monitor with a 3 - megapixel barco display ( barco , 1 3 la radiologia medica ( 2020 ) 125 : 145154 kortrijk , belgium ) and 2048 1536 resolution . 
the software programs originally supplied with the systems were used for image evaluation . study design andassessment ofap lesions the study design followed the method of our two abovementioned papers on ap lesions [ 31 , 32 ]  . 
finally , the lesions affecting the cortical bone were separated from those affecting only the cancellous bone . in cbct imaging , the patients with teeth that showed no change in periapical bone structure ( healthy periapex ) or those clearly had a well - defined periapical radiolucent area ( diseased periapex ) were included . 
therefore , cbct periapical health status was assessed by means of a dichotomous scale , that is , presence and absence of a bone lesion corresponding to the diseased group and healthy group , respectively . 
the clinical diagnoses were made by endodontists and oral / maxillofacial surgeons . the method used to measure ap lesions on cbct imaging made the intersection between the sagittal and coronal planes coincide with the longitudinal axis of the tooth in question . 
the possible thin rim of cortical bone bordering the radiolucent lesion was excluded from the measurements . after the diseased and healthy teeth were chosen on reference standard cbct scans , the corresponding pan images were retrieved . 
 [ 35 ] , which is a 5 - score scale based on radiographic aspects of the periodontal ligament : ( 1 ) normal periapical structures ; ( 2 ) small changes in bone structure ; ( 3 ) changes in bone structure with some mineral loss ; ( 4 ) periodontitis with a well - defined radiolucent area ; and ( 5 ) severe periodontitis with exacerbating features . 
 this condition represents the most common occurrence in a dental clinical center , where pan was carried out after an oral examination and the overall status of the patients mouth was known . method 3 : a portion of pan ( cropped pan )  . 
pan was electronically cut to display only dental roots ( no crown should be shown ) and surrounding tissues up to 8mm mesially and distally from the investigated root apex . 
each image ( complete pan and portion of pan ) was independently assessed by three radiologists skilled in dental maxillofacial imaging ( 33 , 20 , and 14years of experience )  . 
the pai values of the portions of pan with the presence of the only root ( method 4 ) were retrieved from our previous papers [ 31 , 32 ]  . 
the assessment of the pan images by the other three methods was carried out with a gap of 3months from each other . sensitivity , specificity , positive predictive value , negative predictive value , and diagnostic accuracy for pan images with respect to the cbct reference standard images were calculated for each of the four methods . 
these analyses 1 3 148 la radiologia medica ( 2020 ) 125 : 145154 were fulfilled in the total sample and stratified for size of lesion , anatomical area , and bone resorption type . 
a complete pan used for the analysis of the methods 1 and 2 , b and c small portion of pan used for the analysis of the methods 3 and 4 . 
 the complete pan clearly showed that the radiolucent area had a larger size than the width of the crop area , also involving the periapex of the lower right medial and lateral incisors . 
 differences among the four methods were practically inexistent in cases of teeth with endodontic treatment , and in the upper and lower canine / premolar areas and lower molar area of the teeth without endodontic treatment . 
regarding the lesion size and bone resorption type , a slightly higher 1 3 la radiologia medica ( 2020 ) 125 : 145154 in a diagnostic imaging center ( no clinician performs the oral examination and no radiologists aware of the clinical examination of each individual tooth ) and in a dental clinical center ( dentists know the health status of each individual tooth ) , respectively . 
in each of the four methods , the presence or absence of endodontic treatment was a determining factor for the evaluation of ap lesions , especially for the differences between complete pan ( methods 1 and 2 ) and small portion pan ( methods 3 and 4 )  . 
that was mainly noted in the upper and lower incisive areas where the overall view in cropped pan is lacking with consequent difficulties in isolating ap lesions from anatomic and electronic noises typical of two - dimensional imaging . 
it was because the projection on the image of structures with obvious morphologic diversities among people , such as nasal bones / cartilages and chin / mental fossa , may have a larger size than the width of the crop area and , consequently , shows such structures beyond the borders of small cropped images . 
similarly , plow - dragged artifacts originating from the intrinsic technique unique to the curved rotational tomography during the image formation may extend outside the borders of the crop area . 
in our opinion , evaluating a limited size area by means of cropping , as is the case in image decomposition [ 28 , 29 ] , helps radiologists and dentists pay more attention to an area difficult to interpret because of its anatomic complexity . 
the overall view of the maxillary sinus floor with its radiopaque undulating outline around root apexes protruding in the sinus radiolucency was blended into the projection of the periapical lamina dura . 
a complete pan used for the analysis of the methods 1 and 2 , b and c small portion of pan used for the analysis of the methods 3 and 4 . 
the methods 1 and 2 simulated what happens 1 3 152 la radiologia medica ( 2020 ) 125 : 145154 treatment root fillings marked the pulp canal up to the apex drawing the morphology of the whole root and apical periodontiuthis was the main reason why in treated tooth any difference in accuracy among the four methods was found . 
nevertheless , a little reduction in the accuracy of the incisive areas and especially the lower incisive area was observed for the same reasons as indicated above about untreated tooth . in both treated tooth and untreated tooth , anatomical and projective factors were crucial in determining the accuracy of ap lesions in the different areas . 
the different morphologies of the upper and lower arches caused a lack in the focus on the upper molar area for technical and rotational reasons of the panoramic x - rays unit , with consequent high geometric distortion effect . 
the air within the maxillary sinus , the numerous roots infrequently orthogonal to the x - ray beam , the irregular morphology of the maxillary sinus floor , and the anterior part of the zygomatic arch superimposed on root apexes , made it difficult to identify ap lesions in the upper molar area and to a lesser extent in the upper canine / premolar area . 
also the analysis of the lower and upper incisive areas was difficult because of the variable morphology of chin / mental fossa and superimposition of the hard palate , skull base , nasal bone / cartilage / air , and cervical spine . 
both for complete pan and small portion of pan , ap lesions in the lower canine / premolar and molar areas were better recognizable since roots were more orthogonal to the x - ray beam , a lower superimposition of the extraoral anatomic structures was found and no nasal / sinusal air was obviously visible . since in the upper molar area of the teeth without endodontic treatment cropped pan showed a higher accuracy than complete pan , it is recommended for radiologists and clinicians to perform a quick and easy additional process cutting out electronically a portion of digital image as valuable diagnostic aid . we did not assess the diagnostic accuracy resulting from the combination of complete pan and portions of pan . 
 despite the fact that periapical radiography is affected by typical disadvantages of two - dimensional imaging ( difficulty in the patients positioning , morphological variations of the periapical area , bone mineralization , x - ray angulations , and radiographic contrast [ 36 , 37 ] ) , it has greater spatial resolution and higher diagnostic accuracy than pan in identifying ap lesions because of its more detailed delineation of the continuity and shape of the lamina dura [ 25 ]  . 
additional comparisons among periapical radiography and pan are necessary for continuous technological innovations of the digital age . the choice of the right examination to be carried out in the detection of ap lesions is complicated by radioprotection reasons . 
despite the possibility to use low dose protocols for endodontic patients characterized by low exposure parameters , limited field of views , and half scans , cbct imaging remains a second - level examination that should be recommended in individual cases and cannot replace pan and periapical radiography for any suspected periapical bone lesion [ 40 , 41 ]  . 
cutting an image out of a pan does not entail using additional radiation doses , can always be done in digital imaging , and could be also successfully used in bone lesions of a different nature . the very good accuracy of pan in recognizing ap lesions in the lower canine / premolar and molar areas can conclude diagnostic procedures in such areas . 
on the contrary , the low accuracy and npv in the upper arch and lower incisive area proved that the probability of a true negative diagnosis is low and that more than one - third of ap lesions are missed by pan . 
therefore , in selected cases a diagnostic in - depth analysis by using cbct is needed . the analysis of the four methods examined in the current study proved that the knowledge of the patients oral status influenced the radiologic diagnosis of a healthy / diseased periapex . 
because of poor reproducibility of pan [ 37 ] , in the follow - up for ap lesions it is recommended that examinations are performed by the same medical and technical staffs to ensure standardization of the execution method . 
in addition , digital storages of images enable both to perform complementary simple electronic processing and avoid damaging re - exposure in case examinations are no longer found . the hypothesis put forward by the authors in their previous study [ 31 ] for the lack of a clear agreement between the observers on the effects of electronically cut pan was not confirmed in the current study since the agreement was also substantial in the assessment of complete pan . 
furthermore , the results of the current study performed on digital pan confirmed what had been proved by a previous paper [ 25 ] that had used analog pan in which large interobserver variations were found . 
therefore , clinicians should carefully judge the results of both complete and cropped pan by taking its low reproducibility and a high probability of missed diagnosis into account . a limitation of our study was represented by the enrollment of only periapical bone lesions with sizes between 2 and 7mwe did not investigate the diagnostic accuracy of both complete and cropped pan in not uncommon bone lesions 1 3 la radiologia medica ( 2020 ) 125 : 145154 less than 2mm and especially more than 7mm ; in our opinion , it should increase the false negatives and true positives , respectively . 
one more weakness was to gather ap lesions in only three anatomic areas for each arch , in particular to gather canines with premolars because of the obvious different morphology and local anatomy . 
we hope that further work will analyze ap for each individually studied tooth . furthermore , we suggest further work that compares direct digital periapical radiography , direct digital pan ( complete and cropped pan ) , and cbct in both non - periapical and non - inflammatory lytic jaws periapical bone lesions . 
digital imaging enabled various functions and processing , such as enlargement , white / black inversion , and coloring that could help to identify ap lesions . such applications were not investigated in the current study and could be the subject of additional analysis . conclusions in our series , both digital complete and small portion of pan showed high specificity , low sensitivity , and good diagnostic accuracy in the detection of ap lesions with and without endodontic treatment . 
complete and small portion of pan had greater accuracy in the upper / lower incisive area and upper molar area of untreated teeth , respectively , whereas no difference was found in treated teeth . funding this research did not receive any specific grant from funding agencies in the public , commercial , or not - for - profit sectors . 
aim was to assess the diagnostic performance of lie - ct according to readers experience , scar pattern and contrast - to - noise ratio ( cnr ) using late gadolinium enhancement mri ( lge - mri ) as reference . methods lie - ct and lge - mri images of 40 consecutive patients were analyzed . 
two readers with different experience ( 8 and 2years ) independently analyzed lie - ct images defining the presence / absence of scar and scar cnr , segmental involvement , transmural pattern and scar etiology . 
the same parameters were extracted from lge - mri by two expert readers in consensus , blinded to the lie - ct results . results scars were identified at lge - mri in 29 / 40 patients and 141 / 680 segments . 
therefore , an accurate and prompt identification of myocardial scars is fundamental to diagnose ischemic and non - ischemic cardiomyopathies and to address the best clinical management for each patient . however , regardless of its indisputable clinical role , cmr is not so widely available , especially in the acute setting . 
although more recent devices are mr - conditional , the presence of implantable cardioverter defibrillator ( icd ) or permanent pacemaker ( ppm ) may significantly impair lge images assessability due to generator related artifacts [ 5 ]  . moreover , patients suffering from claustrophobia or patients unable to tolerate long scanning time are not able to receive cmr . hence , a valid and effective imaging alternative to lge - mri is useful . 
in recent years , thanks to technological improvement , computed tomography ( ct ) has progressively transformed from noninvasive coronary angiography into an imaging tool able to comprehensively assess the heart , offering also the possibility to identify and characterize myocardial scars . iodinated contrast media share the same kinetics and dynamics with gadolinium chelates , with a delayed washout in scarred myocardium compared to normal myocardiuthis generates different iodine concentrations between scarred and non - scarred areas that can be highlighted as areas of late iodine enhancement ( lie ) with a 1015min delayed ct scan ( lie - ct ) [ 6 ]  . based on some recent studies which showed the possibility to identify myocardial scars in ct with promising results , lie - ct could be used in case of cmr contraindications [ 7 ]  . 
however , previous studies always investigated lie in specific clinical settings or referring to a specific cardiomyopathy , like sarcoidosis [ 8 ] , hypertrophic cardiomyopathy ( hcm ) [ 9 ] , myocardial infarction [ 10 , 11 ] and heart failure [ 12 ]  . despite the promising results highlighted , the diagnostic value of lie - ct in the clinical routine is not completely established , namely in unselected patients with different cardiac diseases reported by physicians with variable expertise . the question is : is lie - ct a robust diagnostic alternative for myocardial scar imaging ? how much does the cardiac disease and the readers experience impact on the reliability of the diagnostic evaluation performed using lie - ct ? the purpose of the present study was to evaluate the role of lie - ct in the detection and characterization of myocardial scars , using lge - mri as standard of reference , in a population of consecutive unselected patients . materials andmethods the study was piloted in agreement with the 1964 helsinki declaration and its later amendments , and it was approved by the institutional review board . 
all subjects provided written informed consent . this is a single - center observational study . lie - ct and lge - mr images , acquired between march 2016 and july 2019 in forty consecutive adults ( > 18years ) without contraindication to contrast agent administration or impaired renal function ( egfr 30ml / min ) at a tertiary referral center and university hospital , for routine clinical exclusion of coronary artery disease and structural cardiomyopathy , were retrospectively analyzed . 
patients suffered from suspected coronary artery disease ( 15 / 40 ) , ventricular arrhythmias ( 12 / 40 ) , dilated cardiomyopathy of unknown origin ( 6 / 40 ) , acute chest pain ( 3 / 40 ) , atrial fibrillation ( 2 / 40 ) , resuscitated sudden cardiac death ( 2 / 40 )  . cardiac ct protocol ct was acquired on a second - generation dual - source scanner ( somatom definition flash , siemens , germany ) during a triphasic bolus injection of iodinated contrast agent ( ca ) ( ultravist 370 , bayer healthcare pharmaceutical ; 370mg iodine / ml )  . 
a second dose of ca was injected immediately after the acquisition of the cta , in order to reach a total iodine dose of 0.6 iodine grams per kilogram of body weight [ 13 ] ( range 97140ml of total ca )  . 
normal myocardium was defined qualitatively as a region of myocardium without any apparent lge . all patients underwent cmr on a 1.5 t scanner ( ingenia , philips medical systems , eindhoven , the netherlands ) equipped with a 32 - channel body coil , within 2weeks after ct . 
the percentage of lie was quantified as the ratio of lie to entire lv mass . statistical analysis continuous data are expressed as mean sd or median ( interquartile range ( iqr ) ) , according to their distribution . 
 the correlation between scar burden ( % ) in lie - ct and lge - mri was assessed using spearmans correlation test . cohens kappa ( ) coefficient ( < 0.20 : poor ; 0.200.40 : fair ; 0.400.60 : moderate ; 0.600.80 : good ; 0.801.00 : very good agreement ) was calculated for the assessment of inter - observer agreement in lie - ct evaluation and for the assessment of segmental and per - patient agreement between lie - ct and lge - mri . mannwhitney u test was used to compare the cnr of lie - ct according to scar transmurality and clinical diagnosis . statistical analyses were performed using spss v.25.0. a p value of < 0.05 was considered statistically significant . results the patients demographics and clinical characteristics are shown in table1 . 29 / 40 ( 72.5% ) patients had lge at mri , mostly with non - ischemic pattern ( 20 / 29 , 69% ) rather than ischemic pattern ( 9 / 29 , 31% )  . 
1 diagnostic performance of lie - ct in the identification of myocardial scars in relation to readers experience at per - patient ( a ) and segmental ( b ) analysis , using lge - mri as standard of reference 1 3 la radiologia medica ( 2020 ) 125 : 128136 132 fig . 
lie - ct images show a large post - ischemic scar with subendocardial distribution involving the midand basal inferolateral wall ( arrows in ac ) , associated to a thin mesocardial scar in the basal septum ( arrowheads in ac )  . 
myocardial scars at lie - ct closely agree with corresponding myocardial scars in short - axis ( d , e ) and long - axis ( f ) lge - mri images lge - mri . 
short - axis lie - ct ( a ) and lge - mri images ( b ) show patchy septal enhancement ( arrowheads ) , especially prominent in the anterior and posterior right ventricle insertion point , associated to asymmetric hypertrophy of the septum , suggestive of hcm fig . 
the box - plots of cnr in relation to the transmural pattern of the scar ( a ) show higher cnr in transmural rather than in subendocardial , mesocardial and epicardial scars . 
moreover , lge amount is associated to incremental risk of major adverse cardiac events and adverse ventricle remodeling [ 16 , 17 ]  . the continuous improvement in ct technology , in terms of increased spatial and temporal resolution , has led to a further expansion of clinical application of ct . 
this combined with improvements in detectors technology and iterative reconstruction algorithm allowed a significant noise reduction for images acquired at low energy , expanding the application of ct to myocardial scar characterization . similarly to gadolinium - based ca , iodinated ca accumulates in scarred myocardium at equilibrium phase [ 6 ] , and a low - energy ct scan is able to enhance differences in iodine concentration between scarred and non - scarred myocardium . a combined evaluation of myocardial scar and coronary arteries anatomy and patency is highly desirable , allowing to simultaneously detect the culprit lesion and its associated myocardial infarction [ 18 ] , to identify non - ischemic causes of acute chest pain [ 18 ] , and to evaluate patients with contraindication to mri ( i.e. , icd , ppm , claustrophobia , low compliance ) [ 13 ] with a short examination time . the routine application of lie - ct in the clinical practice is still limited . 
this is mainly due to the lack of data confirming the diagnostic value of lie - ct in unselected patient populations with clinical indication for scar imaging . considering the potential relevance of scar imaging with ct in clinical practice , the aim of the present study was to evaluate the diagnostic accuracy of lie - ct in the identification of scarred myocardium in a real - world population , also in relation to different readers experience . the results of our study showed that the agreement between lie - ct and lge - mri is dependent on readers experience , with a per - patient overall accuracy of 95% and 88% for the most and the least experienced observer , respectively . 
therefore , lie - ct can correctly determine the cardiomyopathy underlying the detected scars . 1 3 la radiologia medica ( 2020 ) 125 : 128136 lie - ct is notoriously affected by lower contrast resolution in respect to lge - mri , due to the inability of ct to null the normal myocardium , resulting in significantly lower cnr values and a more challenging identification of scars . 
the possibility of acquiring a ct scan at the equilibrium phase with low voltages has the double advantage of improving ct delayed scan contrast resolution and of saving dose , in fact the reduction in tube voltage from 120 to 80kvp accompanies a change in photon energy levels from approximately 66 to 52kev and improves the attenuation of iodine [ 19 ] , enhancing scarred myocardiuhowever , kvp reduction as well as bmi increase are both associated to an increase in image noise . 
for this reason , patients with low bmi have been scanned at 80kvp , while beam energy was increased to 100kvp in patients with bmi 30 . the median cnr value found in our study is comparable with previous studies which were using single - energy lowdose lie scan ( 80kvp ) [ 20 ]  . 
however , comparing different types of scars , we found that cnr was lower in nicm scars than in icm scars , thus leading to a lower detection rate for nicm scars . 
the reason of lower cnr in nicm scars could be explained by the well - known coexistence of fibrotic tissue embedding a variable number of viable myocytes within the nicm scars , while the icm scars usually include a large central dense scar eventually surrounded by a smaller area of less - dense border - zone scar . 
in fact , non - ischemic scars demonstrated a lower cnr than ischemic scars also at lgemri , but differently form ct , the median cnr of lgecmr remain in any case sufficient to detect non - ischemic scars thanks to the capability of lge - mri inversion recovery sequences to null the signal of normal myocardiu moreover , missed scar at lie - ct were characterized by low scar burden ( always < 6% ) , making it challenging to be distinguished from the grainy background , which can be sometimes experienced in low - energy scans [ 21 ]  . readers experience seems able to partially overcome the cnr limits in small and shaded scar . 
in fact , the most experienced reader missed only two scars , which were subepicardial and involving a very small amount of myocardial mass ( 2% ) , whereas the least experienced reader missed 4 subepicardial and 1 mesocardial scars , all involving a small percentage of lv mass . regardless of similar cnr and segmental extent , the detection rate of mesocardial scars was slightly higher than for subepicardial scars , probably because the surrounding normal myocardium improves the detectability of mesocardial hyperdensity . some limitation must be considered when interpreting the present results . 
the inter - observer agreement among expert readers is beyond the scope of the present study , but it remains an important issue considering the good results achieved by our single expert observer . 
the reason of this choice lies on different considerations : scanners with dual - energy capability based on rapid kvp switching , dual - layer detectors or dualsource technology do not have a widespread diffusion . 
 [ 12 ] reported a median dlp of 258.3mgycm ( iqr : 258.3285.3mgycm ) , considerably higher than what we found in our study , despite comparable populations in terms of bmi . 
finally , the advantages of the dual - energy approach for lie detection and quantification are not clearly established , especially on dual - source scanners , because of the halving of temporal resolution and the increase in motion artifacts , originating by the overlapping of two beam energies temporally misaligned by 75ms [ 20 ] , in respect to the single - energy approach . conclusion in conclusion , our results suggest that lie - ct may represent an excellent alternative to lge - mri , especially in expert hands . 
a normal accessory bone appearance on x - ray does not exclude that the accessory bone is the source of the discomfort ; because of this , mri examination can later be applied as part of the diagnosis . methods we retrospectively analysed cases of 64 patients with recognized 70 symptomatic accessory bones of the foot . 
we investigated the following radiological features of the bone ( structural and signal ) in relation to soft tissue . results the most constant symptoms identified in our study were bone marrow oedema ( 93% ) and soft tissue oedema ( 77% )  . 
 changes in structures in which accessory bones were located or in adjacent structures to accessory bone were identified : tendon changes 51% , fluid adjacent to bone 51% and tenosynovitis 46% . 
mri revealed changes in bone structure that are not seen on x - ray , including changes in contour ( 28% ) , sclerosis ( 3% ) or osteonecrosis ( 3% )  . conclusions mri plays an important role in determining whether accessory bones cause symptoms because it shows specific and accurate changes in accessory bone and / or in adjacent soft tissue . keywords symptomatic accessory bone painful accessory bone mri foot mri bone bone marrow oedema introduction the foot is the most common location in the human skeleton for an accessory bone . 
 this large variation is due to the fact that not all ossification centres fuse with the main ossification centre during development and potentially can be separate ( as an accessory bone articulated with the main bone )  . 
x - ray examination is important due to the exclusion of other pathologies such as fracture [ 2 , 4 ]  . most accessory bones do not produce any symptoms , however . 
it is not fully evident why some cause symptoms , but it seems that location , type of articulation with the main bone , relationship with a tendon or proximity to a joint space , diameter and degree of mobility may be important factors [ 10 , 11 ]  . 
patients are referred for radiological examinations to determine the cause of the pain and examine the vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 188196 foot for irritation or oedema [ 12 ]  . 
thus , we decided to investigate the role of radiological examinations to describe the relationship between the accessory bone of the foot and its symptoms . materials andmethods using a hospital radiological database search engine , we retrospectively analysed cases of patients with recognized accessory bones of the foot between 1 january 2012 and 31 december 2018 . 
mri examination protocols ( ankle or ankle and foot ) could differ between cases , but we included only patients with at least : t1 coronal ( no fat saturation ) , t2 fat saturation coronal and axial , sagittal short - t1 inversion recovery ( stir ) and proton density fat saturation axial . 
we excluded all cases in which a bone fracture or metal fixation was present . we investigated the following radiological features of the bone ( structural and signal ) in relation to soft tissue like tendon , joint capsule and other important structures such as vessels and nerves . all patients consented to have their medical data used for retrospective analysis . table 1 distribution of the accessory bones sixty - nine patients meeting our inclusion criteria were identified , 36 of whom were males and 33 females . 
 the following accessory bones were found : os trigonum , os naviculare accessorium , os peroneum , os vesalianum , os talotibiale , os calcaneus secundarius , os subfibulare , os sustentaculi and os intermetatarseuone patient had two symptomatic accessory bones only on one side ( os trigonum and os naviculare )  . results the x - ray is good at detecting accessory bones , while mri is better at detecting structural and signal changes in accessory bones . 
 in the case of those accessory bones that can be assessed by x - ray , majority do not show any abnormality ( figs.1 , 2 , 3 , 4 and 6 )  . 
in our study , only 10% of symptomatic accessory bones showed changes on x - ray ; they were cases of os naviculare accessorium and os peroneum . abnormal findings were detected mostly on mri ( table2 )  . 
in the case of the os calcaneum secundarium , os subfibulare ( fig.4 ) , os intermetatarseum ( fig.5 ) and os vesalianum ( fig.6 ) , we noticed bone marrow oedema and fluid in the soft tissue . 
 b coronal cross section at the level shown on a with the dotted line marked with b shows medial os trigonuc coronal cross section at the level shown on a with the dotted line marked revealed a lateral os trigonud sagittal cross section at the level shown on a with the dotted line marked c . 
gi x - rays : f ( lateral ankle projection ) , g ( antero - posterior ankle projection ) , h ( dorsal plantar projection , foot ) , i ( oblique projection , foot )  . 
it seemed to impinge on the tibialis posterior tendon and the flexor digitorum longus tendon . discussion the authors mentioned the use of almost all radiological modalities ( x - ray , computed tomography and mri ) and nuclear medicine methods in their diagnoses [ 1720 ]  . 
normal appearance on x - ray does not exclude that it can be a symptomatic accessory bone [ 2 , 46 ]  . mri was employed because they allow one to see changes in the bone marrow and soft tissue , and the presence of lesions is considered objective [ 15 , 21 , 22 ]  . 
some authors use other methods like spect / ct to diagnose cases as predictors of surgical management , but we decided to use methods available to practitioners in a general hospital [ 17 ]  . 1 3 192 la radiologia medica ( 2020 ) 125 : 188196 fig . 
 1os peroneum , 2tendo musculi peroneus brevis as other authors have also concluded , bone marrow oedema is the most constant symptom of symptomatic accessory bones [ 2 , 3 , 18 , 21 ]  . 
the remaining bones ( os vesalianum , os sustentaculi , os calcaneum accessorium , os talotibiale and os intermetatarseum ) will be discussed together at the end . the os naviculare accessorium is the most common accessory bone identified . 
type ii bones seem to cause the most complications ; this could be explained by the connection to the navicular , the bone diameter , the course of the tibialis posterior tendon and the skeletal maturity [ 2730 ]  . 
the relationship between the development of a flat foot and the presence of an os naviculare accessorium is unclear , as many authors report 1 3 la radiologia medica ( 2020 ) 125 : 188196 fig . 
1malleolus lateralis , 2os subfibulare , 3tendo musculi peronei longi that the bone in a flat foot is the same as in a normal foot ; however , none of our patients had evidence of flat foot [ 3 ]  . symptomatic os trigonum bones may result from bone mobility . 
this can explain why the bone can conflict with soft tissue in a relatively tight space between the flexor hallucis longus , kagers fat pad and adjacent bones [ 31 ]  . 
mri revealed similar manifestations as with the symptomatic accessory navicular : signal change with bone marrow oedema , fluid , oedema of the soft tissue and , in the chronic stage , sclerosis . 
one sign was specific for the symptomatic os trigonum : more effusion in the posterior recess of the ankle joint and in the flexor hallucis longus synovial sheath , probably as a consequence of direct contact [ 32 ]  . 
 table 2 features of the accessory bones accessory bone bone changes bone marrow oedema osteonecrosis fracture sclerosis changes in contour tendon changes tenosynovitis fluid oedema in soft tissues os naviculare accessorium os trigonum os subfibulare os peroneum os vesalianum os sustentaculi os talotibiale os calcaneum secundarium os intermetatarseum number of bones is 70 soft tissue changes abnormality on x - ray 51% 77% 1 3 194 la radiologia medica ( 2020 ) 125 : 188196 fig . 
1basis ossis metatarsalis v , 2os vesalianum , 3tendo musculi peroneus brevis 1 3 la radiologia medica ( 2020 ) 125 : 188196 os trigonum syndrome described by many authors can result from microinjuries in the posterior ankle caused by repetitive plantar flexion stress , often seen in ballet dancers and soccer players [ 3133 , 37 ]  . a large variation of radiological signs occurred in the case of the os peroneupresence of changes in the os peroneum can be explained by the following factors : size and location . 
fracture and sclerosis were specific to the os peroneum ; we associate this finding with the location of this accessory bone on the lateral edge of the foot , relating most to weight bearing and gait [ 34 ]  . 
fracture , osteonecrosis and secondary fragmentation can be explained by its location within the peroneus longus tendon at the edge of the foot and traction [ 35 , 36 ]  . 
repetitive microinjuries cause changes in the bone , resulting in altered shape and structure [ 36 , 37 ]  . in regard to the os vesalianum , os sustentaculi , os calcaneum accessorium , os talotibiale and os intermetatarseum , the bones diameter is usually less than the other discussed bones , making detection of bone changes more challenging [ 2 ]  . 
os intemetatarseum and os calcaneus secundarius are located between bones , but we did not notice changes in these larger bones [ 2 ]  . conclusion due to their low incidence , it is challenging to determine if accessory bones can in fact cause symptoms . 
 further studies are needed to solve this problem , and multidisciplinary teams should deal with diagnosis and treatment once an accessory bone is detected . clinical diagnosis of symptomatic accessory bones can be challenging . 
the histogram parameters ( 10th percentile , 90th percentile , median , mean , standard deviation , skewness , and kurtosis ) of pre - crt and post - crt were compared using a paired students t test in the cr and non - cr groups , respectively . 
a receiver operating characteristic ( roc ) analysis was performed to evaluate the diagnostic performance . results the histogram parameters of ktrans values were observed to have significantly decreased after chemoradiotherapy in the cr group . 
 pre - ktrans - 10th showed the best diagnostic performance in predicting the chemoradiotherapy response . conclusions the histogram parameters of ktrans are useful in the assessment and prediction of the chemoradiotherapy response in patients with advanced esophageal squamous cell carcinoma . 
dce - mri could serve as an adjunctive imaging technique for treatment planning . keywords dynamic contrast - enhanced mri esophageal cancer chemoradiotherapy response histogram analysis introduction esophageal cancer has a high mortality rate ( 84% ) and poor 5 - year survival rate ( 1534% ) [ 15 ]  . 
 however , patients who cannot tolerate surgery because of their poor physical condition or those with unresectable late - stage esophageal cancer usually cannot benefit * xi - sheng liu liuxisheng2118@126.com 1 department ofradiology , the first affiliated hospital ofnanjing medical university , no . 
however , a few patients cannot benefit from crt and have to bear its side effects including bone marrow suppression , esophagitis , pericarditis , and pneumonia [ 7 , 8 ]  . 
thus , pre - treatment prediction and post - treatment assessment for patients response to crt have become increasingly significant for identifying patients who can benefit from crt while avoiding unwanted adverse events [ 9 ]  . 
dynamic contrast - enhanced mr imaging ( dce - mri ) , as a functional mr imaging modality , has been proven to be useful in evaluating vascular perfusion vol . : ( 0123456789 ) 1 3 166 la radiologia medica ( 2020 ) 125 : 165176 and endothelial permeability which can be used for monitoring and predicting chemoradiotherapy responses [ 1 , 6 , 1215 ]  . in previous studies , dce - mri markers were used as the mean or median quantitative parameters over regional regions of interest ( rois ) [ 13 , 14 , 16 ]  . 
a whole - lesion histogrambased analysis of tumor mri measurements may provide accurate markers of tumor heterogeneity at the genetic , cellular , and molecular levels [ 7 , 8 , 10 , 17 , 1926 ]  . 
at present , some studies have investigated tumor heterogeneity which might be an important potential use of functional imaging techniques in differential diagnosis [ 10 , 18 , 27 ] , analyzing reproducibility capability [ 21 ] , discriminating tumor histological grades [ 20 , 28 ] , assessing tumor aggressiveness [ 29 ] , and evaluating and predicting anticancer therapy [ 15 , 19 , 22 ]  . 
histogram parameters , including the 10th percentile , 90th percentile , median , mean , standard deviation , skewness , and kurtosis , were used in this study to evaluate the heterogeneity of advanced esophageal cancer and chemoradiotherapy response . while some studies on esophageal cancer using dcemri have been reported [ 1 , 6 , 13 ] , to the best of our knowledge , no study has used a histogram analysis of dce - mri parameters for evaluating the chemoradiotherapy response thus far . 
the goal of this study was to quantify heterogeneity in advanced esophageal cancer for predicting and evaluating chemoradiotherapy responses by histogram analysis of dce - mri parameters . materials andmethods patients this retrospective study was reviewed and approved by the institutional review board of our hospital . 
the patients were first divided into four response categories : complete response ( cr ) , partial response ( pr ) , stable disease ( sd ) , and progressive disease ( pd )  . 
the patients with cr were defined as the cr group , whereas the patients with pr , sd , and pd were defined as the non - cr group . chemoradiotherapy radiotherapy was delivered to the primary tumor at a dose of 60gy ( 2gy / fraction , 5 fractions / week )  . 
 the scanning parameters were as follows : repetition time ( tr ) : 5.22ms ; echo time ( te ) : 1.81ms ; matrix : 256 138 ; field of view ( fov ) : 21 38cm2 ; and slice thickness : 3m 1 3 la radiologia medica ( 2020 ) 125 : 165176 when the scan of the third phase was performed , the contrast medium ( 0.1mmol / kg , omniscan , ge healthcare ) was injected intravenously as a bolus injection at the rate of 2.5ml / s by using an mr - compatible power injector ( spectris ; medrad , pittsburgh , pa ; stellant mr injection system , medrad , germany ) , followed by 15 - ml saline flush at the same injection rate . dcemri analysis all the dce - mri data in the digital imaging and communication in medicine ( dicom ) format were transferred to an omni - kinetics workstation ( ge healthcare , lifescience , china ) for analysis by an extended tofts linear model . 
all the regions of interest ( rois ) of esophageal cancer were manually drawn to cover the entire tumor area by referring to the t2 - weighted and the contrast - enhanced t1 - weighted images . 
the histogram analysis of each parameter included the following : mean , median , standard deviation ( sd ) , skewness , kurtosis , and the 10th and 90th percentiles . 
sd reflected the dispersion of the histogram ; kurtosis represented the peakedness of the histogram , and skewness described the asymmetry of the histograthe sd value was high if the histogram distribution showed a broad pattern and low if the histogram distribution showed a narrow pattern . 
a positive skewness value implied that most of the data were concentrated on the left of the histogram , and a negative skewness value denoted that most of the data were concentrated on the right . data processing was performed by two radiologists ( reader 1 , with 10years of clinical experience in digestive radiology ; reader 2 , with 5years of clinical experience in digestive radiology )  . 
paired students t test was applied to identify the significant differences in the dce - mri parameters between pre - crt and postcrt in both the cr and the non - cr groups . 
a p value of < 0.05 was considered to be statistically significant in the comparisons . the intra - reader and inter - reader agreements of the dcemri histogram parameters were evaluated using the interclass correlation coefficient ( icc ) with a 95% confidence intervals . 
the patients with cr were defined as the cr group , whereas the other 29 patients with pr , sd , and pd were defined as the non - cr group . 
there was no statistically significant difference between the cr group and the non - cr group in gender , mean age , location , and clinical t - stage and n - stage . statistical analysis agreement analysis all statistical analyses were performed using the spss 21.0 statistical software ( ibm corporation , armonk , ny , usa )  . 
the detailed intra - reader and 1 3 168 la radiologia medica ( 2020 ) 125 : 165176 table 1 demographic data of 72 patients demographic data cr group ( n = 43 ) non - cr group p value ( n = 29 ) inter - reader agreements for each histogram parameter are shown in tables2 and 3 . 
for the ktrans measurements , the median , mean , sd , and 10th and 90th percentile values of ktrans were observed to have significantly decreased after chemoradiotherapy in the cr group , while no change was identified in the non - cr group . 
for the kep measurement , there were statistically significant decreases from pre - crt to post - crt in the median , mean , and the 10th percentile histogram values of the cr group ; a significant difference was also observed in the median , mean , and the 10th and 90th percentile values of kep in the non - cr group . 
the histograms of ktrans ( fig.4 ) show the changes from a broad pattern to a narrow one with a decrease in sd in the cr patient and a broader pattern in the non - cr patient after chemoradiotherapy . 
the changes observed in the two above - mentioned cases revealed a decrease in the tumor heterogeneity in the cr patient and an increase in the non - cr patient after crt . diagnostic performance ofhistogrambased dcemri parameters the roc analyses of the role played by ktrans , kep , and ve in predicting the chemoradiotherapy response were performed ( table 6 )  . 
furthermore , we observed that the pre - ktrans - 10th percentile value might be the most promising parameter for predicting the chemoradiotherapy response . the ktrans value reflects the endothelial permeability of tumor microcirculation . 
we detected that the histogram parameters of ktrans with a significant difference demonstrated a marked reduction after chemoradiotherapy in the cr group , while no change was indentified in the non - cr group . 
consistent with the past several findings , higher pre - ktrans values and lower post - ktrans values indicated a good response to therapy [ 15 , 16 , 31 , 32 ]  . 
the investigators explained that the decreased ktrans value of dce - mri was associated with a lower micro - vessel density of the tumor after chemoradiotherapy [ 3336 ]  . 
the decrease in micro - vessel density in the cr patients after chemoradiotherapy was more obvious than that in the non - cr patients ; thus , the decrease of ktrans value was also more obvious than that in the non - cr patients . 
meanwhile , our findings showed that some histogram parameters ( mean , median , and the 10th and 90th percentiles ) of prektrans were statistically higher in the cr group than those in the non - cr group . 
the results corresponded well to the findings in the recent studies that higher pre - ktrans values were correlated with a better treatment response [ 13 , 15 , 31 , 37 , 38 ]  . 
the investigators interpreted that the tumors in good responders might obtain a better delivery of the chemotherapeutic agents and show greater radiosensitivity [ 15 , 31 , 37 , 38 ]  . 
thus , we postulated that the lower pre - ktrans value in the non - cr group might be associated with more necrosis in tumors which implies relatively low blood perfusion and effectiveness of chemoradiation . 
therefore , in our opinion , esophageal cancer with a higher pre - ktrans and lower post - ktrans values indicated good treatment response to crt ; thus , the ktrans values are valuable in response evaluation . 
in contrast to the ktrans values , an obvious reduction in the kep histogram parameters cannot offer useful information on differentiating between the cr and the non - cr responses . 
however , the roles of the kep and ve histogram parameters in assessing the therapy response are divergent without reaching any agreement , and further investigation is required . in the past , several investigators have observed divergent histogram parameters ( median , mean , standard deviation , mode , skewness , kurtosis , minimum , maximum , percentiles , and entropy ) derived from dce - mri , reaching contrasting results [ 22 , 24 , 25 ]  . 
n just stated that this fact could result in inadequate knowledge on the available parameters and the lack of the literature references to standardized histogram methods [ 17 ]  . 
meanwhile , a histogram analysis could be complementary to the recist guideline [ 24 ]  . standard deviation reflects the dispersion of the histogram and accurately evaluates the width of the distribution . 
the results presented in the above - mentioned papers implied that sd changed from a high value before treatment to a low value after treatment , which meant the heterogeneity of tumors decreased after treatment . 
these studies were in agreement with the view that the good responders showed obvious changes in histograms from more to less heterogeneous distributions after treatment , and a decrease in the sd value . 
our results are in accordance with those reported in the previous studies that the sd value of the ktrans value strongly decreased after crt in the cr group but not in the non - cr group . 
furthermore , a review concerning tumor heterogeneity mri assessment by histograms revealed that skewed distributions tended to the left with lower sd and higher kurtosis after treatment in the good responders [ 17 ]  . 
 our findings bore some similarities to the view that the skewness values in the cr group demonstrated an upward tendency after crt , which meant that the distribution of the histogram showed positive skewness with a predominant left distribution . 
therefore , it warrants a further investigation of the skewness and the kurtosis of the dce - mri histogram parameters in patients with advanced esophageal cancer receiving chemoradiotherapy . our results indicated that only ktrans - kurtosis and kep10th showed statistical significance after crt in the cr group when compared with those of the non - cr group . 
the best diagnostic performance of predicting the chemoradiotherapy cr response could be achieved at pre - ktrans - 10th > 0.065 as the threshold ( auc , 0.824 ; sensitivity , 76.7% ; specificity , 75.9% ) 1 3 la radiologia medica ( 2020 ) 125 : 165176 be associated with the sample size . 
a further study of the correlation analysis of cellular morphology ( dwi ) and angiogenic processes ( dce - mri ) is necessary for esophageal carcinoma . in conclusion , most of the ktrans histogram parameters are crucial in evaluating and predicting the chemoradiotherapy response in patients with locally advanced esophageal squamous cell carcinoma . 
research in the past decade has improved diagnosis and treatment of these frequent and potentially devastating complications of diabetic foot which often remain difficult to be diagnosed and treated despite the availability of various clinical , serological , and imaging modalities . 
although the reference standard for diagnosis remains microbiologic analysis of bone specimens , in most clinical practice , soft tissue and bone infection involving the diabetic foot is diagnosed solely on the basis of a combination of clinical evaluation , serum inflammatory markers , and imaging modalities . 
thus , the primary purpose of this review article was to provide radiologist and clinician with important clinical knowledge and relevant radiological semiotics , respectively , in order to facilitate a prompt diagnosis and personalised treatment of diabetic foot infections . keywords diabetes diabetic foot soft tissue infection osteomyelitis mr imaging personalised medicine introduction almost all diabetes - related foot infections originate from an infected foot ulcer [ 1 ]  . 
available data suggest that diabetic patients have a 25% lifetime prevalence of foot ulceration , which is the greatest risk factor for subsequent osteomyelitis and amputation [ 2 , 3 ] ; furthermore , clinical findings of infection are seen in more than 50% of diabetics with skin ulcer of the foot [ 4 , 5 ]  . 
gemelli 1 , 00168rome , italy 3 unit di radiologia , universit degli studi magna graecia , catanzaro ( aks ) , italy often make decisions without adequate evidence - based data [ 6 ]  . 
peripheral neuropathy can diminish symptoms and thus mask the severity of the disease with a considerable diagnostic and therapeutic delay ; once an infection is established in a diabetic foot , lacking blood supply and impaired immune system make it difficult to treat . 
radiography is almost always the first - line imaging modality , and magnetic resonance ( mr ) imaging is the modality of choice in this context , although hybrid imaging modalities such as positron emission tomography ( pet ) / ct play an increasing role [ 7 ]  . 
 thus , the diagnosis and management of diabetes - related foot infections are challenging and a multidisciplinary team with a shared knowledge base for treatment team members rather than a compartmentalised view is required to ensure an effective and tailored management . 
the disease typically occurs in long - standing diabetic patients with peripheral neuropathy and vascular disease leading to varying degrees and patterns of bone destruction , deformity with altered biomechanics , increased new bone formation , cartilage damage , and joint instability . 
altered biomechanics leads to callus formation because of chronic repetitive biomechanical stress on the insensate foot at weight - bearing sites such as the head of the first and fifth metatarsal bones , the tip of the great toe , and the plantar aspect of the posterior calcaneus . 
clinicians frequently request the evaluation of the diabetic foot for osteomyelitis since inflammatory signs and symptoms may be blunted because of diabetes - related peripheral vascular disease and peripheral neuropathy . 
furthermore , ( 1 ) the presence of osteomyelitis complicates treatment and may decrease the probability of a successful outcome ; ( 2 ) prompt diagnosis and optimal therapy are of paramount importance for avoiding future complications and poor outcomes [ 9 , 10 ]  . 
 bone biopsy , with a histopathologic and microbiologic examination of the bone specimen , remains the reference standard for diagnosing osteomyelitis and determining the responsible organism and its antibiotic susceptibility [ 6 ]  . 
nevertheless , many clinicians consider bone biopsy an invasive procedure with the risk of seeding and / or impairing potentially not infect tissue ; moreover , bone biopsy may result in a false - negative response due to prior medical therapy or specimen poorness . 
an ulcer cross - sectional area > 2cm2 and an ulcer depth > 3mm are more likely to be associated with infections of the underlying bone [ 10 , 11 ] , but the presence of a skin ulcer has a relatively low positive predictive value for osteomyelitis . 
an erythrocyte sedimentation rate ( esr ) > 70mm / h increases the probability of osteomyelitis ; however , this clinical feature is highly specific for osteomyelitis , but has a sensitivity of only 28% [ 12 ]  . 
 another useful clinical finding is the probe - to - bone test which is well recognised as a predictive and efficient tool la radiologia medica ( 2020 ) 125 : 177187 for detecting osteomyelitis of the foot , and some authors [ 9 , 1315 ] suggested that after a positive probe - to - bone test , the evaluation may proceed directly to microbiologic and histologic confirmation of osteomyelitis . 
the probeto - bone test is a simple , minimally invasive , and low - cost test consisting in the insertion of a sterile blunt metal into the ulcer depth ; if bone is palpated on probing , it almost confirms the diagnosis of osteomyelitis [ 9 ]  . 
given this uncertainty , the clinical diagnosis of diabetic pedal osteomyelitis can be difficult even in the presence of a foot ulcer , and imaging may be essential for the diagnosis and staging of diabetes - related osteomyelitis [ 12 , 17 ]  . 
radiography and mr imaging are the modalities of choice in diabetic patients with suspected foot infections ; however , the role of 18fluorine - fluorodeoxyglucose - positron emission tomography / ct ( 18f - fdg - pet / ct ) is evolving rapidly and could redefine the diagnostic workup of diabetesrelated foot infections . imaging features radiography radiography is almost always the first - line imaging modality when evaluating for bone involvement in the diabetic foot , but its sensitivity for bone and soft tissue infections is rather low in the early stages of infection [ 18 ]  . 
useful information can be obtained by performing serial radiographs to detect progressive bony changes ( fig.1 ) , but we are not aware of any studies of the role of serial radiographs to diagnose osteomyelitis . 
nevertheless , imaging workup of suspected bone infection should begin right with radiography , because it is cheap , widely available and , even when not diagnostic , provides an anatomical overview of the area of interest and any pre - existing conditions that could influence the selection and interpretation of subsequent procedures . utrasound thanks to its high spatial resolution , and new - generation devices fitted with high - frequency probes , ultrasound is indicated for detecting joint synovitis , effusions , and fluid collections [ 20 ]  . 
it can be used in providing guidance for joint aspiration and drainage procedures ; however , the ultrasoundguided technique requires experience and good manual skills 1 3 la radiologia medica ( 2020 ) 125 : 177187 and bone infection involving the diabetic foot [ 7 , 2325 ] , with high sensitivity and high specificity ( 90% and 82.5% , respectively ) in the diagnosis of osteomyelitis [ 26 ]  . 
in the last several years , technical improvements have allowed the application of diffusion - weighted imaging which can help to discriminate between pure oedema and infection , and dixon sequences which improve fat suppression , with increased depiction of bone marrow oedema and infectious complications [ 25 ]  . 
also plane selection should be customised to each single examination , and at least two planes should be obtained to best visualise the area of interest [ 27 ]  . 
 t1 - weighted images provide anatomical details and are the most specific in the detection of osteomyelitis , whereas the fluid - sensitive fat - suppressed images are sensitive for oedema within bone and soft tissues [ 23 , 24 ]  . 
contrastenhanced imaging , often requiring one sequence in each plane , is helpful in the detection of soft tissue changes such as sinus tracts and abscesses [ 23 , 24 ]  . 
furthermore , post - contrast imaging provides invaluable information for pre - operative planning of limited limb resection , allowing distinction between enhancing regions of viable soft tissue and bone from non - enhancing and non - viable regions [ 23 , 26 ]  . 
however , a finding of a region of hyperintense bone marrow on fluid - sensitive fat - suppressed images and post - contrast enhancement has high sensitivity for the diagnosis of osteomyelitis , but relatively low specificity unless it is accompanied by a corresponding region of hypointensity on t1 - weighted images which is the most important sign of osteomyelitis ( figs.2 , 3 ) [ 8 , 2831 ]  . 
other pedal conditions such as reactive bone marrow oedema , stress changes related to altered weight bearing ( fig.4 ) , recent surgery , and neuropathic osteoarthropathy can simulate infection at mr imaging by showing bone marrow oedema and post - contrast enhancement , thus reducing mr imaging specificity . 
b corresponding radiograph obtained about 3months later shows marked progressive changes of bone fragmentation , cortical destruction , and dislocation of the fifth metatarsal - phalangeal joint ( rectangle ) on the part of the operator , and above all , it is not currently recommended by the diabetic foot guidelines of the american college of radiology [ 21 ]  . ct soft tissue contrast resolution is inferior to that of mr imaging and ultrasound ; furthermore , early changes of osteomyelitis such as bone marrow oedema cannot be distinguished in a ct examination . 
however , diabetes patients are at high risk of contrastinduced nephropathy having up to a 40% incidence of renal impairment , with 50% of type 1 diabetes patients having diabetic nephropathy progressing to end - stage renal disease [ 22 ]  . 
in summary , the ct role in the imaging of diabetesrelated foot complications is very limited , remaining a choice when mr imaging is contraindicated or unavailable . mr imaging because of the excellent spatial resolution and precise anatomical details , mr imaging is widely accepted as the modality of choice for imaging evaluation of soft tissue 1 3 180 la radiologia medica ( 2020 ) 125 : 177187 fig . 
a sagittal post - contrast t1 - weighted fat - suppressed , b axial t1 - weighted , and c corresponding post - contrast t1 - weighted fat - suppressed mr images show a plantar ulcer appearing as a focal skin interruption with peripheral post - contrast enhancement ( arrow in a ) , and a sinus tract with rim - like enhancement that extends to the first metatarsophalangeal joint ( small arrows in a , c )  . 
diffuse decreased signal intensity in the first metatarsal ( long arrow in b ) with post - contrast enhancement ( long arrow in a , c ) is indicative of osteomyelitis infection , but lack of surrounding soft tissue change is helpful in differentiating it from infection [ 32 ]  . ulcer manifests as focal cutaneous interruptions with raised margins ( secondary to pre - existing callus formation ) and associated with a soft tissue defect , on any imaging sequence or plane . 
unlike callus , ulcer appears hyperintense on fluid - sensitive fat - suppressed images , with marked peripheral enhancement a finding indicative of granulation tissue at the base of the ulcer ( figs.3 , 5 ) [ 7 , 23 , 32 ]  . sinus tract usually results from ulcers penetrating deeply and represents a route for subsequent spread of infection leading to abscesses and / or osteomyelitis [ 33 ]  . 
a coronal t1 - weighted , b t2 - fat - saturated , and c t1 fat - saturated post - contrast mr images clearly show that the marrow in the head of the fifth metatarsal has low signal on t1 - weighted image ( arrow in a ) , increased signal on fluid - sensitive fat - suppressed image ( arrow in b ) , and post - gadolinium enhancement ( arrow in c ) , findings indicative of osteomyelitis criterion , mr imaging may not be very specific . 
nevertheless , several secondary findings may serve as useful discriminators and help to augment diagnostic confidence ; the presence of skin callus , subtending skin ulcer , sinus tract , abscess , septic arthritis , or tenosynovitis supports the diagnosis of osteomyelitis . skin callus usually appears as a focal subcutaneous mass with low signal intensity on t1 - weighted images and intermediate / low signal intensity on fluid - sensitive images . 
 post - contrast fat - suppressed t1 - weighted images clearly demonstrate the unique rim enhancement demarcating the fluid collection within ( figs.8 , 9 , 10 ) ; that is one of the reasons why the routine use of contrast material - enhanced imaging in all diabetics with an estimated glomerular filtration rate of more than 30ml / min is advocated [ 33 , 35 , 36 ]  . septic arthritis of the foot in diabetics mainly occurs around the metatarsophalangeal and interphalangeal joints , secondary to an adjacent soft tissue infection such as abscess , tenosynovitis , sinus tract , and most often ulcer ( fig.3 ) [ 33 ]  . 
radiographic findings are difficult to be visualised in early stages of infection , and mr imaging features such as complex joint effusion with distension of joint recesses and synovial thickening with contrast enhancement are non - specific , and may also be seen in non - infectious inflammatory arthropathies . 
 septic arthritis may also demonstrate adjacent secondary bone marrow oedema with post - contrast enhancement on both sides of the joint ; however , this finding can be caused by either reactive osteitis or superimposed osteomyelitis . 
 bone marrow enhancement is not reliable in discriminating between the two entities [ 23 , 24 , 28 ]  . distinguishing osteomyelitis from neuropathic osteoarthropathy is clinically and radiologically challenging since one condition may mimic the other . 
most of the time , neuropathic osteoarthropathy involves tarsometatarsal and intertarsal joints ( 60% of cases ) followed by the metatarsophalangeal joints ( 30% of cases ) [ 37 ] , whereas distribution of osteomyelitis usually has a focal involvement : the calcaneus , malleoli , and weight - bearing surfaces of the toes . 
furthermore , neuropathic osteoarthropathy is primarily periarticular ( fig.4 ) and bone marrow involvement is limited to juxta - articular locations , whereas osteomyelitis almost invariably results from an ulcer or abscess in contiguous soft tissue and bone marrow changes are larger and more significant ( figs.3 , 11 ) [ 38 ]  . neuropathic osteoarthropathy and osteomyelitis may also coexist and the clinical and radiological differentiation of infected from non - infected neuropathic osteoarthropathy could be extremely challenging , so much that in many cases it is necessary to perform a biopsy . 
this finding disappeared after 3months off - loading of the affected foot soft tissues showed high specificity ( average , 85% ) for the diagnosis of osteomyelitis in the adjacent bone . 
thus , this secondary sign should be actively sought in cases of questioned osteomyelitis of the foot . septic tenosynovitis occurs mainly in tendons underlying ulcers , especially the flexor tendons of the forefoot as a result of plantar forefoot ulcerations [ 29 ] , as well as the peroneal and achilles tendons from lateral malleolus and calcaneal ulcers , respectively [ 23 ]  . 
however , these findings are non - specific for the presence of a tendon infection ; they also may be seen with other inflammatory , degenerative , or post - traumatic conditions [ 23 , 32 , 34 ]  . abscess manifests as a focal fluid collection frequently contiguous with sinus tracts that communicate with skin ulcers , tendon sheaths , bones , or joints . 
on mr imaging , an abscess is hypointense on t1 - weighted images , hyperintense on fluid - sensitive fat - suppressed images , with peripheral thick rim enhancement , due to the presence of granulation tissue . 
thus , an abscess may not be distinguishable from dense soft tissue oedema seen in cellulitis or from soft tissue 1 3 la radiologia medica ( 2020 ) 125 : 177187 182 fig . 
a sagittal t1 - weighted and bd postcontrast t1 - weighted fatsuppressed mr images show a large plantar ulcer that extends to the calcaneus ( * in ad )  . 
an enhancing deep sinus tract with tram - track pattern extending from the plantar ulcer to the ankle joint is also seen ( arrowhead in bd ) ; thus , the joint effusion with thick rim enhancement is indicative of septic arthritis ( arrows in bd ) however , an ulcer that extends to the bone , sinus tracts , fluid collections , and extensive bone marrow changes suggest superimposed infection ( figs.8 , 10 , 11 ) [ 7 , 23 ]  . 
this mr sign refers to bones that disappear on t1 - weighted images ( the ghost sign ) and then reappear on fluid - sensitive fat - suppressed or post - contrast images . 
in uncomplicated neuropathic osteoarthropathy , there is destruction of bones which could be oedematous , but there is no infiltration of the marrow by inflammatory cells resulting in absence of the ghost sign [ 23 , 24 ]  . 
the most commonly performed radionuclide procedures include bone scintigraphy , hybrid single - photon emission computed tomography / ct using the fusion of scintigraphic and morphologic images , and the radiolabeled leucocyte imaging which remains a key investigation in the assessment of diabetes - related foot infections [ 39 ]  . 
however , the role of 18 fluorine - fluorodeoxyglucose ( 18f - fdg ) - positron emission tomography ( pet ) - ct is evolving rapidly and becoming increasingly important in the diagnostic workup of this specific clinical setting [ 40 ]  . 
 its advantages include : short acquisition time ; preferential 18f - fdg accumulation in the infection site , facilitating the detection of osteomyelitis and the differential diagnosis from neuropathic osteoarthropathy ; whole - body analysis ; lack of metallic hardware artifacts ; high resolution enabling precise 1 3 la radiologia medica ( 2020 ) 125 : 177187 fig . 
a axial t1 - weighted and b corresponding post - contrast t1 - weighted fat - suppressed mr images show an abnormal increase in fluid within the peroneus longus tendon sheath , and a thick rim enhancement around the tendon , due to inflamed synovium ( arrow in a , b )  . 
coronal gadoliniumenhanced t1 - weighted fat - suppressed mr image shows phlegmonous plantar soft tissue characterised by diffuse post - contrast enhancement ( arrows ) and a thick rim enhancement around the tendons indicating tenosynovitis ( arrowheads ) fig . 
a coronal t1 - weighted , b t2 - weighted fat - suppressed , and c gadoliniumenhanced t1 - weighted fat - suppressed mr images show a large plantar soft tissue fluid collection ( arrows in ac ) that is hypointense on the t1 - weighted image and hyperintense on the t2 - weighted fat - suppressed image , with a thick rim - like layer of enhancement in c . 
hypointensity ( * in a ) and post - contrast enhancement ( * in c ) in the first metatarsal are indicative of osteomyelitis tracer recognition in small bones as the distal forefoot [ 39 ]  . 
a axial t2 - weighted fat - suppressed , b corresponding post - contrast t1 - weighted fat - suppressed , and c sagittal post - contrast t1 - weighted fat - suppressed mr images show an intra - osseous abscess in the first metatarsal that is hyperintense on the t2 - weighted fat - suppressed image ( arrow in a ) , with a thick rim - like layer of enhancement ( arrow in b , c )  . 
other two large plantar soft tissue fluid collections are also seen ( small arrows in b , c ) the diagnostic performances of mr imaging , radiolabeled white blood cell scintigraphy and 18f - fdg - pet / ct and reported that 18f - fdg - pet / ct as well as 99mtc - hmpaolabelled leucocyte spect / ct offer the highest specificity ( 92% ) for diagnosing diabetic foot osteomyelitis while demonstrating comparable sensitivity to the other imaging modalities . 
kagna etal [ 42 ] , basing the final diagnosis on histopathologic and microbiologic examination of bone specimens , imaging or clinical follow - up , evaluated the role of 18f - fdg - pet / ct in the diagnosis of osteomyelitis in 39 diabetics with 46 sites suspicious for infections . 
in this study , the sensitivity , specificity , and accuracy , using lesion analysis , were 100% , 93% , and 96% , respectively ; using patient - based analysis , the sensitivity , specificity , and accuracy were 100% , 92% , and 95% , respectively . 
 [ 44 ] , using visual and semi - quantitative analysis , and bone biopsy or tissue culture for final diagnosis , conducted a study on 13 patients with very high pre - test probability fig . 
b axial t1 - weighted , and c corresponding post - contrast images show replacement of the normal plantar fat by soft tissue ( circle in b ) and a thick rim enhanced plantar fluid collection ( circle in c ) , respectively of osteomyelitis ( seven with ulcers , six with exposed bone )  . 
the authors found 18f - fdg - pet / ct to have a lower diagnostic accuracy ( 5462% ) for osteomyelitis compared to 99mtc - exametazime - labelled leucocyte scintigraphy ( 92% )  . 
 schwegler etal [ 45 ] conducted a prospective study in 20 diabetic patients with a chronic foot ulcer without antibiotic pre - treatment and without clinical signs for osteomyelitis , to 1 3 la radiologia medica ( 2020 ) 125 : 177187 fig . 
a axial t1 - weighted , b t2 - fat - saturated , and c postcontrast t1 - weighted fatsuppressed mr images show diffuse bone marrow oedema in the calcaneus with low signal on t1 - weighted image ( arrows in a ) , increased signal on fluidsensitive fat - suppressed image ( arrows in b ) , and post - gadolinium enhancement ( arrows in c )  . 
the diffuse bone marrow oedema in the calcaneus , the plantar fluid collection ( see fig.7 ) , and the tenosynovitis ( see fig.10 ) indicates a superimposed osteomyelitis fig . 
b sagittal post - contrast t1 - weighted fat - suppressed mr image shows the osseous structures of the midfoot , which appear more regular and better defined than in a . 
note fluid collections in the ankle joint and thick synovial enhancement ( small arrows ) as well as the deep sinus tract with a rim - like enhancement that extends up from the plantar soft tissue planes to the midfoot ( arrow )  . 
the sinus tract was visible only after the administration of contrast material assess the prevalence of clinically unsuspected osteomyelitis and to compare the value of mr imaging , 18f - fdg - pet / ct , and 99mtc - labelled monoclonal antigranulocyte antibody scintigraphy . 
nevertheless , the literature focusing on the use of 18f - fdg - pet / ct in this setting remains still limited and discordant ; thus , further large multicenter studies using bone biopsy as reference standard are warranted . treatment diabetes - related foot infections require a multidisciplinary foot - care team paying attention to local and systemic issues . 
in some clinical situations , such as foot infection associated with substantial bone necrosis , patient non - ambulatory , at particularly high risk for antibiotic - related problems , or with strong preference for surgery , surgical treatment is clearly more appropriate . 
vice versa , in other clinical situations such as an infection confined to small forefoot 1 3 186 la radiologia medica ( 2020 ) 125 : 177187 lesion and with minimal soft tissue loss , no availability of skilled surgeon , patient too clinically unstable for surgery or with a strong preference for medical therapy , it is clear that antibiotics choice is the most appropriate . 
while many cases of osteomyelitis require , or benefit from surgical procedures , several retrospective and prospective studies [ 4648 ] have demonstrated that osteomyelitis can be treated successfully by medical therapy . 
in a randomized comparative trial of initial medical versus surgical treatment for diabetic foot osteomyelitis by lzaro - martnez etal [ 48 ] , antibiotic therapy and surgical treatment had similar outcomes in terms of healing rates , time to healing , and shortterm complications in patients with neuropathic forefoot ulcers complicated by osteomyelitis without ischemia or necrotizing soft tissue infections . 
debridement is the removal of devitalised , and / or contaminated soft tissue from within or adjacent to a wound and is also widely regarded as an effective intervention to speed up ulcer healing . 
according to the international working group on the diabetic foot - guidelines , surgical bone resection is recommended in cases of bone exposure , progressive bone destruction , and spreading of infection along soft tissues [ 18 ]  . 
in most cases , however , the optimum approach is currently being debated [ 49 ]  . conclusion in a person with diabetes and suspected foot infection , using a combination of the probe - to - bone test , serum inflammatory markers , especially erythrocyte sedimentation rate , and radiographic examination as the initial studies to diagnose osteomyelitis are recommended . 
mr imaging is the primary imaging modality for the investigation of osteomyelitis and associated soft tissue complications providing accurate information regarding the presence and extent of infection in this subset of patients . 
in the setting where mr imaging is not available , contraindicated , or not conclusive , the use of 18f - fdg - pet / ct is justified because of its high sensitivity and specificity . 
if clinical and imaging evaluation is not conclusive , or if the confidence that a patient has osteomyelitis is high , histopathologic and microbiologic examination of bone specimen after discontinuation of antibiotic therapy for 2weeks is recommended . 
a signal intensity ratio was calculated using the inferior temporal cortex and the background noise . results one hundred and forty - three subjects were evaluated for a total of 210 ears . 
due to a possible residual / recurrent disease that may go * andrea romano andrea.romano@uniroma1.it 1 department ofodontostomatological andmaxillo - facial sciences , umberto i hospital , university sapienza , via di grottarossa , 00135rome , italy 2 nesmos , department ofotorino - laringoiatry , s . 
andrea hospital , university sapienza , rome , italy 5 neuroradiology unit , imaging department , bambino ges childrens hospital , rome , italy undiagnosed with an exclusive clinical examination , secondlook surgery is frequently planned [ 1 ]  . non - echo - planar ( epi ) diffusion - weighted magnetic resonance imaging ( dwi - mri ) has become the gold - standard imaging technique for detection of middle ear cho . 
surgical notes and pathologic results were available for all the cases . the study was approved by the institutional ethics board and adhered to the tenets of the declaration of helsinki . 
the haste - dwi was obtained in the coronal plane with the following parameters : repetition time ( tr ) / echo time ( te ) , 2080 / 105ms ; 2 and 3mm slice thickness without gap ; number of excitation ( nex ) , 3 ; matrix , 192 75% ; field of view ( fov ) 230mm ; average time : 2.06mone b value was obtained ( b = 1000 )  . 
 coronal t1 - weighted imaging was performed with a tr / te , 569 / 10ms ; flip angle , 150 ; nex , 3 ; 3mm slice thickness , fov , 230mm ; matrix , 384 80% . 
axial tse t2 - weighted imaging was obtained with tr / te , 2200 / 112ms ; flip angle , 180 ; nex , 4 ; slice thickness , 3mm ; fov , 230mm ; matrix , 384 70% . 
coronal tse t2 - weighted imaging was obtained with tr / te , 3280 / 110ms ; flip angle , 180 ; nex , 4 ; slice thickness , 3mm ; fov , 230mm ; matrix , 384 70% . imaging evaluation two radiologists independently evaluated the images of the patients and reported whether an enhanced signal inside the middle ear was present . 
 ( the size of the roi was related to the tissue dimensions . ) the mean ( si ) and maximum ( simax ) si values on the dwi images were recorded from this roi for each patient . 
a signal intensity ratio ( sir ) was calculated using , as a reference , the inferior temporal cortex ( sirt ) and the background noise ( sirn ) with the following formulas : sirt = si / si la radiologia medica ( 2020 ) 125 : 7579 temporal cortex , sirtmax = simax / si temporal cortex , sirn = si / si noise , sirnmax = simax / si noise . 
the background noise roi was placed far from the skin profile , due to the presence of slight artefacts . both observers performed all the measurements , separately and independently for the assessment of inter - observer agreement . 
a two - sample t test was performed to compare dwi values of different parameters used ( si , simax , sirt , sirtmax , sirn , sirnmax )  . 
 their main clinical symptoms were recurrent purulent discharge ( n = 22 ) , perforated tympanic membrane with and without discharge ( n = 4 ) and chronic ear discharge with signs of increased intracranial tension ( n = 1 )  . 
thirty - six ears were confirmed to be affected by residual / recurrent cho ( size range 322mm ) ; in four ears ( all undergoing canal wall - up mastoidectomy ) , only inflammatory tissue ( purulent in one ) was found . 
turbo - spin - echo dwi ( haste - dwi , siemens , erlangen , germany ) allows the use of thinner sections , a higher imaging matrix and a refocusing pulse for every measured echo allowing an improvement of spatial resolution whilst reducing susceptibility artefacts . 
residual / recurrent middle ear cho represents a diagnostic challenge mostly due to the small size of these tissues , to the different kinds of surgical procedures and to the non - specific signal intensity characteristics on mr imaging . 
although not frequent , false - positive cases could be dependent on many causes , especially in the post - operative period ( dental braces artefact , bone dust , cartilage , tympanosclerosis , mucosal disease / granulation tissue , proteinaceous fluid , purulent content / abscess , cholesterol granuloma , wax in the adjacent external auditory canal and squamous cell carcinoma of the external auditory canal ) [ 3 , 14 ]  . 
a recent meta - analysis of 1152 patients ( both preand post - surgical cases ) [ 14 ] showed that the use of dwi images alone led to 3.4% of false - positive cases with a lower specificity for the post - operative controls . 
a single prospective study reported a sensitivity and specificity of 90 and 100% in the detection of residual and recurrent and primary cho , with good interobserver agreement amongst experienced radiologists [ 15 ]  . 
the same authors also reported that the main limitation of this evaluation was related to the size of the lesions since those less than 5mm are difficult to be demonstrated by adc and their values cannot be measured or used as a diagnostic tool . 
for this reason , in the present study it has been decided to evaluate dwi using absolute values and their ratios with brain tissue ( temporal lobe ) and background noise . 
according to the roc analysis , si , sirt and sirtmax showed the best statistical values in comparison with the other parameters ( area under curve = 1 ) involving the areas where the rois were placed have precluded the measurement of the si values ( table1 )  . 
in this retrospective 3t mri study , si and sir sensitivity and specificity were higher than adc quantification , as expected . another relevant result observed in our study is the significance of t1 - weighted mr signal . 
it has been reported that chronic granulation tissue / inflammation may lead to high t1 signal compared with brain parenchyma in the post - operative period [ 17 ] ; this finding , in combination with dwi scores , could be helpful for an appropriate diagnosis of recurrent cho . 
in our study , all patients with high signal dwi and high signal on t1 , at revision surgery , were found to have inflammatory tissue rather than cho . the surgical treatment of cho consists in its eradication with a tympanoplasty procedure . 
 this rate of residual pathology motivates the need to find a diagnostic method that enables the identification of residual cho before undergoing a second - look surgery [ 14 ]  . 
however , in our cohort of patients , no significant differences were evident when comparing the incidence of recurrent cho and the selected surgical technique . one of the limitations of this study is related to the small number of subjects that , at the present , impedes us to confirm that quantitative dwi together with t1 evaluation of these patients could be the first choice after surgery . 
since false - negative dwi - mri in post - surgical population is reported in only 3% of cases [ 17 ] , the design of this study excluded the patients with normal dwi from further surgery . 
these falsenegative dwi could also be related to the paucity of keratin necessary to return the required signal on dwi and , in fact , most were due to tiny cholesteatomas ( less than 3mm )  . 
the aim of this study was to determine the feasibility and safety of ct - guided microcoil insertion followed by uniportal vats wedge resection ( wr )  . materials and methods retrospective study in a single institution , including patients undergone ct - guided microcoil insertion prior to uniportal vats resection between may 2015 and december 2018 . 
many authors have described intraoperative localization with ultrasonography , preoperative percutaneous insertion of hook wire and suture , microcoils , preoperative percutaneous injection of radiolabeled aggregates or liquid / contrast agents [ 8 ]  . the aim of this study was to determine the feasibility and safety of ct - guided microcoil insertion followed by uniportal vats resection for small , deep , solid pulmonary nodules or ggo . methods we designed a retrospective , non - comparative singlecenter study , enrolling 46 consecutive consenting patients among those scheduled to undergo ct - guided microcoil insertion prior to uniportal vats lung resection over the period may 2015 to december 2018 . 
all cases were performed using a ge healthcare ct scan . the exact nodule position was found with a preliminary scout view and axial scan of the chest while the patient was in a prone , supine or lying on the lateral decubitus depending on nodule location . 
the patient was instructed to breathe regularly avoiding any movement ; no breath hold was required . the ct scan was obtained after placing an adhesive marker plate with radiopaque coordinates ( beekley medicals guidelines , bristol , connecticut ) to determine the needles route from the entry point on the skin to the nodule . 
oxygen supplementation was administered if necessary . surgical procedure the surgical procedure was scheduled for the day following microcoil positioning , as first case of the day . the patient was transferred to the operating room , and general anesthesia was administered . 
 in all other cases ( not diagnostic , benign or unable to discriminate between primary vs secondary cancer in frozen section ) , a wedge resection ( wr ) was considered satisfying waiting for permanent pathological section and a 24ch chest tube was placed through the incision port . 
twenty patients had a history 1 3 la radiologia medica ( 2020 ) 125 : 2430 of smoking ( 43% ) , of which 7 were current smokers ( 15% )  . 
thirty - five patients ( 76% ) had a history of previous cancer : 17 patients had previously had colon cancer ( 37% ) ; 5 patients had had kidney / urinal tract cancer ( 13% ) ; 6 patients had a history of genital cancer ( 15% ) ; 4 patients were affected by previous breast cancer ( 9% ) , and 3 patients reported another previous type of cancer : 2 lung cancer ( 4% ) and 1 case of retroperitoneal sarcoma ( 2% )  . 
pneumothorax and parenchymal bleeding did not hamper the surgical procedure . the characteristics of the nodules on ct were as follows : 5 pure ggo , 2 semisolid ggo and 39 solid nodules . 
however , for patients who only underwent wr , the average operative time was 105min ( range 50150min ) including the time needed by the pathologist for the frozen section ( average time 20 min )  . 
no patients required intraoperative staple line re - resection for positive margins . postoperative complication rate was 8.7% ( 4 / 46 ) : 1 episode of atrial fibrillation in a patient who undergone wr followed by a right lower lobectomy ; 1 case of pneumonia after wr , treated and resolved with antibiotic therapy ; 1 case of prolonged air leak managed by chest tube and 1 case of bleeding treated and resolved with infusion of 1 unit of red blood cells . 
the pathological diagnosis of the 46 cases included 18 primary lung cancers ( 39% ; 9 adenocarcinomas , 1 squamous cell carcinoma of the lung , 6 typical carcinoids , 1 atypical carcinoid , 1 large - cell neuroendocrine carcinoma ) , 22 cases ( 48% ) were secondary from other cancers and 6 benign lesions ( 13% )  . 
however , these methods are limited by nodule size , small tissue samples and challenging location for conventional approach [ 9 ] , and therefore , surgical resection is often needed to reach a diagnosis . with the diffusion of vats procedures , surgeons start using this approach to perform wr and lobectomies , making this procedure progressively widespread worldwide . 
pneumothorax and parenchymal bleeding did not hamper the surgical procedure . furthermore , the planning of microcoil positioning should always be done by the interventional radiologist and the surgeon to establish the route and the delivery point . 
moreover , the microcoil should be positioned deeper in the parenchyma with respect to the nodule to ease the surgeon and avoid an insufficient resection . microcoil - guided vats resection of spns was previously described in a large series by mayo showing that spns can be safely localized by using one coil end positioned adjacent to the suspicious nodule and the other end in the pleural space [ 12 ]  . 
indeed , the entire microcoil was deployed immediately adjacent to or within the nodule , without pleural marking showing a reduced ct procedure time and radiation dose , equivalent complete resection rates and equivalent procedural and surgical complication [ 14 ]  . in our study , we avoided to mark the pleural surface , appearing easier , shorter to perform and equally guaranteeing excellent results . 
in particular , microcoil was deployed medially to the deepest tumor boundary in a line connecting the nodule and the pulmonary hilum , in order to guarantee the complete excision of the nodule with negative surgical margin . using this technique , we achieved a successful diagnosis rate of 100% of small lung nodules resected , and all surgical margins of wr specimens were negative microscopically . 
furthermore , no cases of conversion to thoracotomy and microcoil dislodgement were recorded . recently , in order to guide the intraoperative identification of a pulmonary nodule , ujiie et al . 
the study suggested that this approach may help surgeons to localize nonvisible , nonpalpable intrapulmonary nodules through direct indocyanine green fluorescence imaging without the use of fluoroscopy , resulting in a complementary technique to preoperative microcoil placement . to date , in addition to the approach described , many techniques were described that have aided in the localization of small pulmonary nodules before vats resection , such as ct - guided insertion of localizer , intraoperative ultrasound , injection of liquid / contrast agents or radiolabeled aggregates [ 8 ]  . as reported in a recent study that reviewed 181 patients undergoing ct - guided hook - wire insertion , localization of spns has been described as a safe technique with a high success rate and low thoracotomy conversion rate [ 16 ]  . 
 however , as reported in a large review recently published , hook - wire localization compared to the other techniques had a lower successful target rate in the operative field because of dislodgement ; it also had the highest rates of pneumothorax and hemothorax [ 17 ]  . furthermore , these previously described techniques require a preoperative invasive procedure that may cause discomfort to the patient as well as complications and radiation exposure . 
investigated the use of intraoperative ultrasound , a noninvasive and potentially complication - free procedure able to also localize pulmonary ground - glass opacities in a completely deflated lung [ 18 , 19 ]  . 
if the nodules were not visible , they were directly identified sonographically [ 18 ]  . 1 3 la radiologia medica ( 2020 ) 125 : 2430 other techniques have been described , e.g. , percutaneous injection of methylene blue , colored collagens , lipiodol , radiotracer [ 8 ]  . as reported by lenglinger etal . 
 [ 20 ] , percutaneous staining of pulmonary nodules with methylene blue is an accurate technique for localizing nodules before vats , subsequently confirmed in a larger study conducted by kleedehn etal . 
this problem could be solved using a colored collagen that stays at the injected site for a long - lasting period , making it possible to perform a delayed surgical operation [ 23 ]  . the same advantage was obtained with lipiodol that was a safe , useful tool for localizing ggos and spns prior to vats and enabled them to even localize one nodule that had been marked 7days before the surgical procedure [ 24 ]  . 
 radio - labeled aggregates have also been evaluated showing a high rate of success [ 25 , 26 ]  . to date , an optimal method of preoperative localization for pulmonary nodules has not been established yet , and local expertise and multidisciplinary preference should drive technique selection . 
although the insertion of a hook wire under ct guidance seems to remain the most widespread technique to localize small and deep nodules , it is not so ideal during vats approach , due to the more frequent dislodgement occurred during lung manipulation . therefore , we preferred to use ct - guided microcoil insertion to localize small pulmonary nodule due to its advantages compared to the other techniques : they are commonly used , easy to acquire and inexpensive compared with radionuclides ; they can also be placed safely in the lung for days , despite the delay between the ct - guided insertion and the start of the operation ; after implantation , they are radiopaque , offering surgeons the ease of localization of nonvisible , nonpalpable intrapulmonary nodules ; furthermore , according to our experience , the radiological placement is safe and repeatable , showing a very low complication rate and absence of dislodgment . our preliminary findings have a number of limitations . 
secondly , there is no comparison group even though our results are similar to those previously published , resulting in 100% of successful diagnosis , short length of stay and duration of chest tube and operative time . 
furthermore , having this bias , we are not able to conclude which vats approach ( uniport vs multiport ) is better to identify sub - centimetric , deep lung nodule . 
 both radiological and surgical procedures are safe and suitable strategies , showing a very low associated complication rate and allowing to achieve a diagnosis in 100% of patients . therefore , ct - guided microcoil insertion should be considered for all patients with small , deep pulmonary nodules prior to vats resection . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval the study was conducted on already available data and ethical approval was not required dependent on the law and the national ethical guidelines of the country . 
the goal of this prospective study was to assess the feasibility of dual - energy ct ( dect ) with iodine quantification at equilibrium phase in the evaluation of significant fibrosis or cirrhosis . methods thirty - eight cirrhotic patients ( according to childpugh and meld scores ) , scheduled for liver ct , were enrolled in the study group . 
fecs was calculated as the ratio of the iodine concentration of liver parenchyma to that of the aorta , multiplied by 1 minus hematocrit . results final study and control group were , respectively , composed of 22 and 20 patients . 
roc curves analysis yielded an optimum fecs cutoff value of 26.3% for differentiation of control group and cirrhotic patients ( auc 0.88 ; 86% sensitivity , 85% specificity )  . conclusions dual - source dect is a feasible , noninvasive method for the assessment of significant liver fibrosis or cirrhosis . keywords dual - source dual - energy ct iodine concentrationfractional extracellular space fibrosiscirrhosis introduction liver fibrosis is a wound - healing response that involves inflammatory cells and mediators for circumscribing the parenchymal injury [ 1 , 2 ]  . 
therefore , physicians tend to be more prone to noninvasive approaches and several diagnostic algorithms are today employed in clinical practice , safer methods in detecting liver fibrosis [ 5 ] ; however , serum enzyme panels and metabolic tests do not reliably quantify hepatic parenchymal injury such as fibrosis [ 6 , 7 ] , while transient elastography is impaired by an unclear estimation of intermediate - grade fibrosis on the other vol . : ( 0123456789 ) 1 3 8 la radiologia medica ( 2020 ) 125 : 714 hand , elastographic quantitative techniques such as magnetic resonance and ultrasound imaging have demonstrated promising results , but may require complex modifications of general performed protocols and additional operator expertise and specific equipment [ 8 ]  . 
moreover , cutoff values can vary according to the different us technologies , with consequent low inter - equipment reproducibility [ 9 ]  . contrast - enhanced ct ( cect ) has been shown capable of quantifying hepatic fibrosis using the same protocol routinely performed in focal liver lesions surveillance [ 10 ]  . at ct imaging , normal liver can be schematically divided in three main spaces : the intravascular space ( ivs ) , the intracellular space ( ics ) and the extracellular extravascular or interstitial space ( ees ) [ 5 , 6 ]  . as fibrosis and inflammation occur within the liver , stellate cells activate and start to proliferate , while collagen and inflammatory debris increase . 
this finding is one of the essential features used for histopathologic assessment of diffuse liver disease severity [ 4 ]  . all water - soluble ct contrast agents , also known as extracellular contrast media , freely pass from the blood plasma into the interstitium , without crossing hepatocyte cell membranes [ 5 , 6 ]  . 
the combination of ivs and ees is also known as hepatic fractional extracellular space ( fecs ) [ 11 ]  . while the measurement of hepatic extracellular extravascular space is challenging , fecs can be quantified as the ratio of the enhancement of the liver parenchyma to the one of the blood pools ( such as blood in the aorta ) multiplied by 1 minus hematocrit at the equilibrium phase [ 8 ]  . encouraging results about both identification and grading of liver fibrosis have been reached by conventional single - energy ct in several [ 6 , 8 , 1012 ]  . dual - energy ct ( dect ) ideally represents the optimal technique in evaluating diffuse and focal liver disease . 
studies on first - generation dual - source dect demonstrated higher contrast - to - noise ratio and better lesion conspicuity at 80 kvp versus 80 / 140kvp mixed image [ 13 , 14 ] ; further advancement in terms of lesion conspicuity has been obtained on second - generation dual - source dect scanners thanks to the introduction of the noiseoptimized algorithm for monochromatic images ( monochromatic plus , siemens healthineers ) , which improved the image quality at low kev [ 15 ]  . 
beyond the better iodine detection , dect allows iodine density quantification on single contrast - enhanced acquisition , without the need of measurements on unenhanced and post - contrastographic images as required on single - energy ct [ 5 , 16 ]  . although the usefulness of dect in the evaluation of liver fibrosis has been already reported [ 9 , 17 , 18 ] to the best of our knowledge , no evaluation of fecs based on iodine concentration using dual - source dect has been described so far . the purpose of this prospective study is to assess the potential of dual - source dect with iodine quantification at a equilibrium phase performed at 10min for high - grade fibrosis or cirrhosis assessment . materials andmethods approval for this prospective study was obtained from the institutional review board of our hospital . 
all patients gave a written informed consent prior to entering the ct study . study population from march 2017 to march 2018 , we enrolled in our study 38 consecutive cirrhotic patients ( study group ) scheduled for abdominal ct for hepatocarcinoma ( hcc ) suspicion and / or portal systemic circulation assessment . 
all patients were referred to our institution by the unit of clinical and molecular hepatology and had clinically confirmed cirrhosis with portal hypertension , documented by clinical history , laboratory analysis , upper endoscopy , ultrasound , ct or mri examination . 
liver cirrhosis was classified according to both the childpugh and the meld scores [ 19 , 20 ]  . of 38 patients , 16 were excluded from the study for technical reasons : 5 patients with portal thrombosis , 2 patients with a large ( > 5cm ) hcc for the potential alteration of the measurement of fecs ( i.e. , tissue compression and / or changes in perfusion ) , 4 poorly collaborative patients with significant artifacts at ct imaging and 5 obese patients ( bmi > 27 )  . twenty - four consecutive patients underwent ct urography for clinical purposes were included in the control group . 
 the inclusion criteria for the control group were : absence of altered liver function or macroscopic vascular hemodynamic modifications , no history of alcohol - related liver disease , no prior liver disease such as hepatitis b or c and no evidence of portal vein thrombosis [ 18 ]  . ct urography was chosen because a 10 - min excretory phase was considered substitutive of equilibrium phase , avoiding an unnecessary radiation dose increase in those subjects [ 8 ]  . four subjects of the control group were excluded from the study because of steatosis and for the presence of hepatic focal lesions . 1 3 la radiologia medica ( 2020 ) 125 : 714 imaging technique all ct examinations of the liver were performed with a dual - source mdct system ( somatom definition dual source ; siemens healthcare , forchheim , germany )  . 
in our hospital , the routine ct study protocol for cirrhotic patients consists of non - contrast , portal venous and equilibrium phases , acquired in single - energy mode , and late hepatic arterial phase , obtained in dual - energy mode . dual - energy scanning parameters are as follows : detector collimation : 14 1.2 ; tube currenttime product : 95 and 510mas , respectively , for 140 and 80kvp with automatic current modulation ( care dose siemens ) ; gantry rotation time : 0.5s ; pitch : 0.8 ; reconstruction algorithm : filtered backprojection with a dedicated de soft tissue reconstruction kernel ( d30f )  . for this study , we replaced the single - energy equilibrium phase at 3min with a dual - energy equilibrium phase at 10min . the choice to acquire images at 10min was made to obtain approximately the same concentration of contrast medium in the ees and in the ivs . 
a further circular roi was drawn on the same section within the abdominal aorta , excluding aortic walls and atheromatous plaques , thus obtaining vascular iodine concentration in mg / ml . iodine concentration ( ic ) of fecs was calculated using the following formula : ic fecs = ( 1 hematocrit ) ( ic liveric aorta ) fig . 
rois were manually drawn , respectively , on the left ( 1 ) and the right lobes of the liver ( 2 ) avoiding macroscopic intrahepatic vascular structures and on the aorta ( 3 )  . 
rois were manually drawn , respectively , on the left ( 1 ) and the right lobes of the liver ( 2 ) avoiding macroscopic intrahepatic vascular structures and on the aorta ( 3 )  . 
 ( roc curves results are reported in fig.4. ) discussion the diagnosis and staging of significant hepatic fibrosis are extremely important for monitoring of disease progression and therapy response assessment . 
an appropriate treatment , in certain etiologies , could reverse fibrosis or prevent the progression to cirrhosis [ 11 ]  . table 2 fecs mean value per each group of patients with relative standard deviation ( sd ) and p - value differences between groups yielded by anova tests . 
4 roc curve between control and study population yielded a cutoff value of 26.3% ( p < 0.05 ; auc : 0.88 ) 1 3 12 la radiologia medica ( 2020 ) 125 : 714 although liver biopsy remains the standard of reference for the diagnosis of liver fibrosis , its role in clinical practice is debated today and noninvasive methods are generally preferred [ 5 ]  . overall , several studies investigated the value of conventional single - energy ct in the measurement of fecs for hepatic fibrosis evaluation , basing on the strict connection between the extracellular matrix proliferation with collagen deposition and extracellular space expansion [ 6 , 8 , 12 ]  . in a murine study , varenika etal . 
 [ 10 ] in comparison with histological and clinical references reported that fractional extracellular volume values higher than 28.7% have 87% sensitivity and 71% specificity in differentiating normal , f0 , f1 from f2 to f4 hepatic fibrosis and that patients with childpugh class a showed significantly lower fecs values than the patients in childpugh b or c class did . in a retrospective study , zissen etal . 
 [ 8 ] found that fecs values obtained from ct presented correlation with meld score . however , several drawbacks of conventional ct must be because liver attenuation measurements at both unenhanced and equilibrium scans , often taken with different technical parameters and using two rois with possible misregistration errors , can theoretically lead to inaccurate measurements [ 13 ]  . these impairments could be overcome using dect , which takes advantage from material decomposition algorithms . 
 [ 10 ] , no statistical difference was found between childpugh a and childpugh b grade . finally , in our cohort there was a positive correlation between hepatic fecs and meld score ( r = 0.64 , p < 0.05 ) [ 9 , 231 24 ]  . to our knowledge , only one study assessed fecs with dect [ 26 ]  . 
 however , in this study , iodine density was obtained by the difference between equilibrium and non - contrast phases , because iodine density values measured on the unenhanced scan were higher than zero . 
the authors attributed this pitfall to the two material decomposition algorithms used in singlesource rapid kilovoltage switching scanners [ 26 ]  . in our study , fecs assessment was performed with a dual - source dect scanner , with a three - material decomposition algorithm , allowing more accurate evaluation of iodine amount in tissues . in fact invitro studies , for low , moderate and high iodinecaused attenuations , showed that vnc image provide reliable attenuation measurements [ 16 , 17 ]  . 
this permits to perform a single post - contrast acquisition dual - energy phase , avoiding possible misregistrations coming from imprecise roi placement on different series [ 16 ]  . however , iodine quantification techniques are not immune to error and several acquisition parameters impact accuracy of iodine density [ 27 ]  . 
 [ 28 ] using a first - generation dual - source dect found that accuracy of iodine concentration is influenced by patient size and concentration of iodine ; marin etal . 
 [ 27 ] using a second - generation dual - source dect demonstrated dramatic improvement on iodine density quantification accuracy with the use of additional tin filtration on high - energy tube , hybrid iterative reconstruction and the use of stellar detector . our iodine density measurements can be considered reliable since they are considerably higher than the lower detectability threshold previously found [ 28 ]  . 
in our opinion , this could be explained by the different dect technologies employed and , mainly , by the different timing of equilibrium phase acquisition : 3min in the study of sofue etal . 
versus 10min in our study . in order to maximize the balance of contrast medium concentration between intravascular and interstitial compartments , we choose this timing basing on the fact that a 10 - min 1 3 la radiologia medica ( 2020 ) 125 : 714 delay corresponds in average to a 610 times recirculation , time that allows diffusion of contrast medium even in areas of liver where extracellular space is particularly large relative to the quantity and distribution of blood vessels [ 8 , 29 ]  . certainly this choice involves a variation of the standard ct protocol for cirrhotic patients , while it would be preferable including fecs evaluation on conventional equilibrium phase ( performed at 180s )  . 
although recent papers have demonstrated that fecv using scans at 180 - s images may be sufficient to detect significant hepatic fibrosis [ 10 , 12 , 26 ] , no studies performed a fecs evaluation comparing conventional 180 - s equilibrium phase images with more delayed phase images , and therefore , further studies are mandatory [ 26 ]  . 
limitations of our study must be acknowledged . first , this study included only patients with advanced liver disease ( i.e. , liver cirrhosis ) and did not analyze subjects in pre - cirrhotic phase with different degrees of liver fibrosis . secondly , our purpose consists in demonstrating feasibility of dual - source dect with iodine quantification for fecs assessment at a delayed equilibrium phase performed at 10min , considering the well - established role of fecs estimation resulted from comparison of liver biopsy with both singleand dual - energy ct [ 8 , 10 , 12 ]  . moreover , this investigation reflects our preliminary experience with a relative small population . 
the limited number of patients included in the study and the relative low number of early cirrhosis cases in our opinion explain the lack of statistical difference between childpugh class a and b ; a necessary validation would come from further studies with larger patients cohort . another limitation comes from the use of first - generation dect ; as already discussed , iodine quantification takes advantage from most recent dual - source dect technologies and further studies with secondand third - generation dual - source dect are encouraged for validating our results [ 10 , 12 , 26 ]  . conclusions our study showed that fecs measurement with dual - source dect represents a feasible and reliable noninvasive quantitative imaging - based biomarker in patients with liver significant fibrosis or cirrhosis . funding this study did not receive any funding . compliance with ethical standards conflict of interest antonio bottari declares that he has no conflict of interest . 
all procedures performed on human participants were in accordance with the ethical standards of the institutional research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2020 ) 125 : 8086 neuroradiology gray matter nuclei damage inacute carbon monoxide intoxication assessed invivo using diffusion tensor mr imaging wenqianjiang1 qingyuwu1 chunzhou1 ziruzhao1 yongmingtan1 received : 3 july 2019 / accepted : 4 september 2019 / published online : 16 september 2019 italian society of medical radiology 2019 abstract objective to observe the structural changes of gray matter nuclei in patients with acute carbon monoxide intoxication by diffusion tensor imaging ( dti ) , quantify the degree of deep gray matter damage in the brain by adopting imaging technology and research the characteristics of the damage and its pertinence with memory and cognitive impairment . methods twenty - five patients with acute carbon monoxide intoxication and 25 healthy volunteers matched in sex and age were examined by routine head mri and diffusion tensor imaging ( dti )  . 
 it found that the change of diffusion coefficient ( adc ) and its clinical correlation with cognitive impairment were generated by carbon monoxide intoxication . results compared with the healthy control group , the fa values of bilateral globus pallidus , hippocampus , dater nucleus and putamen decreased , while the fa values of amygdala and thalamus had no statistical significance ; the md values and adc values of hippocampus , globus pallidus and putamen increased , while the md and adc values of dater nucleus , thalamus and amygdala had no statistical significance , either . conclusion dti is capable of sensitively reflecting the damage of gray matter nuclei caused by acute carbon monoxide intoxication and quantifying the degree of hypoxic brain damage in a certain extent , and may be related to cognitive impairment . keywords acute carbon monoxide intoxication gray matter nucleus apparent diffusion coefficient average diffusion coefficient anisotropic fraction introduction acute carbon monoxide intoxication is resulted in sudden inhalation of large quantities of carbonic oxide ( co ) gas , leading to the binding of co molecules with hemoglobin invivo , followed by secondary hypoxic brain injury and so on ; the mortality and disability rate are extremely high [ 1 ]  . 
diffusion tensor imaging ( dti ) is a quantitative , noninvasive and objective technique for evaluating the integrity of fiber bundles [ 2 ] , which is spread by taking into account other scalar measures derived from diffusion tensor feature analysis , for instance apparent diffusion coefficient ( adc ) , fractional anisotropy ( fa ) , average diffusion coefficient ( md ) [ 3 ]  . 
at present , most of the researches on the brain of co intoxication patients focus on white matter , but in other gray matter has not been reported as frequently as that in the globus pallidus . 
therefore , this study regards hippocampus , parahippocampal gyrus , thalamus , amygdala , globus pallidus and putamen as regions of interest ; the changes of dti parameters were observed to reveal the mechanism of brain injury in patients with acute co poisoning , search for imaging indicators related to acute co poisoning brain injury , and compare them with cognitive function scores , so as to provide an objective and effective basis vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 8086 for clinical evaluation and prognosis prediction of patients with acute co poisoning . data andmethods research object acute co intoxication patients were diagnosed in the first affiliated hospital of nanchang university , jungian province from january 2016 to march 2018 . 
after admission , all patients in the acute co poisoning group were treated with oxygen , electrolyte disorder correction and diuretic therapy , and the symptoms and signs were slightly reduced , but not up to the standard of recovery , and the intelligence and cognitive level were significantly reduced . 
 all the patients have signed the informed consent . standards fortheapplication oftheclinical cognitive function scale ( 1 ) simple mental state examination scale ( mmse ) can comprehensively , accurately and rapidly reflect the subjects and kaposi , mental status and cognitive impairment . 
mmse scale ( total score 30 ) : 17 points in illiterate group , 20 points in primary school group , 24 points in junior high school and above group were divided into boundaries . 
the lower the score , the greater the cognitive impairment . mri data acquisition mr images were collected by using 16 - channel phased array head coils ( 3.0t trio , siemens , ladyfinger , germany )  . 
the subjects remained awake during the scan , covered their eyes with an eye mask , fixed their head , and placed sponge covers and silence plugs in both ears . 
dti data were scanned by echo plane imaging ( epi ) sequence axes , with 65 layers , 2.5mm thickness , tr 7200ms , te 104ms , nex 1 time , matrix 128 128 , fov230mm 230mm , 64 nonlinear dispersion gradients ( b = 0 , 1000s / mm ) were applied , and the scanning duration was 8 min 45 s . 
compared with the healthy control 1 3 82 la radiologia medica ( 2020 ) 125 : 8086 group , the fa values of globus pallid , hippocampus , dater nucleus and putamen decreased ( p < 0.05 ) , the fa values of the amygdala and thalamus were not statistically significant ( p > 0.05 ) , the md and adc values of hippocampus , globus pallid , putamen increased ( p < 0.05 ) and there was no significant difference in the md or adc values of dater nucleus , thalamus and amygdala ( p > 0.05 ) ( table1 )  . 
 correlation analysis betweenchanges ofdti parameters inhippocampus ofacute co poisoning group andmmse andmoca scales fa and md values in hippocampus of patients with co intoxication were extracted , and pearson correlation analysis was performed on mmse scores of patients with acute co intoxication . 
the high activity and high blood supply of neurons in gray matter make it more sensitive than white matter to cerebral hypoxia caused by co intoxication [ 5 ]  . 
structural damage of gray matter nuclei in the brain can also be detected by dti . many studies adopt dti parameters to analyze and quantify leukoencephalopathy mainly relying on hand - drawn region - of - interest ( roi ) method . 
however , there are still many problems in this method , for instance the lack of uniform criteria for roi size and location , resulting in poor repeatability and comparability of results [ 6 ] , and the lack of appropriate degree of spatial smoothing [ 2 ]  . 
therefore , this 1 3 la radiologia medica ( 2020 ) 125 : 8086 design uses software to sketch mask automatic matching , avoiding manual random error . many studies used dti parameters to analyze and quantify leukoencephalopathy , mainly relying on the method of manually plotting roi [ 7 ]  . 
in the dti parameter detection of gray matter nucleus , fa decreased , which may be related to axonal transection injury and dendrite loss in gray matter nucleus [ 8 ]  . 
under the action of excitatory amino acid and oxidative stress injury , acute co poisoning brain tissue causes denaturation injury of neuron cells , and invasion leads to the loss of neurons and dendrites . 
the isotropy of microglia is lower than that of normal tissue [ 10 ] , giving rise to the decrease in fa value of neurons . the adc and md values reflect the overall dispersion level and the overall dispersion resistance of the molecule , indicating the size of the dispersion . 
md refers to the average value of diffusion amplitude in each direction of mr imaging voxel , represents the size and degree of diffusion of water molecules in a voxel and reflects the range of diffusion movement of water molecules in a unit time . 
when the patient is poisoned by co , the cells are in the low - oxygen phase , the cell toxicity is easy to occur , the cells are swollen , the diffusion of water is limited , revealing the decrease in adc and md values . 
 with the persistence of the disease , the breakdown of cell membranes will cause the diffusion of water - promoting molecules , while the adc and md values will rise . 
li zili and other studies have shown that brain tissue is more vulnerable to oxygen free radicals , because brain cells are the most active metabolism , the most sensitive to hypoxia , the most likely to produce oxygen free radicals , and nerve cells are rich in polysaturated fatty acids and the most vulnerable to oxygen free radicals attack [ 11 ]  . the results displayed that the values of md and adc in hippocampus , globus pallidus and putamen increased in patients with co intoxication . 
at the same time , the fa values also decreased in these regions , indicating that acute co intoxication had a significant effect on the hippocampus , globus pallidus and putamen , mainly affecting pathological alters in these nuclei . 
cao yizhans [ 12 ] results showed that pyramidal cell layer in hippocampal ca1 region of copoisoned rats became thinner , sparse , pyramidal cells that disappeared on both sides of the cell layer , and intermediate pyramidal cells that are atrophied and degenerated . 
we can found in these results that the expression of heme oxygenase ( ho - 1 ) in hippocampus of patients with co intoxication and delayed encephalopathy was significantly increased , and apoptotic cells were significantly increased as well , which is consistent with the expression of ho - 1 [ 13 ]  . 
the elevation of ho - 1 has the reason to believe that it is involved in the mechanism of co intoxication on brain injury , indicating that co intoxication has a significant impact on the hippocampus . 
as further development of vascular edema can form cysts , this fluidfilled cystic area increases the free movement of water , leading to rapid increase in md [ 14 ]  . 
 the pathological basis of the effect of co intoxication on the globus pallidus may be that the globus pallidus appears to be softened or necrotic , and the globus pallidus presents ischemic changes . 
owing to hypoxia , the tissue hypoxia and the dysfunction of sodium and potassium ion pump in the cell membrane lead to the retention of na + and water in the cell , leading to the toxic edema in the cell [ 17 ]  . 
the pathological basis is similar to that of globus pallidus . the prospects and shortcomings of this paper are as follows : deficiencies : ( 1 ) because the diffusion of water molecules in gray matter is isotropic in three - dimensional space , the signal attenuation of water molecules simulated by conventional dti model has great errors , so dti has limitations in the quantitative evaluation of gray matter damage after co intoxication [ 19 ]  . 
 ( 2 ) to shorten the detection time , we should further optimize the inspection technology ; ( 3 ) lack of epidemiological data to support the design of the experiment ; ( 4 ) lack of follow - up survey of the experimental group . 
prospect : diffusional kurtosis imaging ( dki ) is 1 3 86 la radiologia medica ( 2020 ) 125 : 8086 a new diffusion technology developed on the basis of dti . 
dki , as an extension and development of dti technology , has been confirmed in previous studies that dki is more sensitive and specific than dti in evaluating changes in gray and white matter structure of the brain the study of acute co intoxication , dki will be more sensitive than dti . 
in the experiment , the globus pallidus and nucleus putamen located in the basal ganglia of the brain , the hippocampus and paramygdala located in the cerebral cortex and the thalamus and amygdala located near the temporal lobe were selected as the regions of interest . 
is it possible to follow up ? in conclusion , our study suggests that acute co intoxication is characterized by vascular edema in multiple gray matter nuclei , resulting in loss of neurons and dendrites . 
in order to achieve an accurate solution , a two - stage automated method was developed : decision forests for a rough prediction of vertebral bodies position , and morphological image processing techniques to refine the previous detection by locating the position of the spinal canal . results the mean distance error between the predicted vertebrae centroid position and truth was 13.7mthe identification rate was 79.6% on the thoracic region and of 74.8% on the lumbar segment . conclusion the algorithm provides a new method to detect and identify vertebral bodies from arbitrary field - of - view body ct scans . keywords artificial intelligence decision forest spine computed tomography introduction in clinical routine practice dealing with spinal abnormalities and pathologies , the localization and identification of the vertebral bodies is a crucial step for an appropriate clinical diagnosis , surgical planning and follow - up assessment . 
despite they did not require a high computational burden , they required some anatomical landmarks . the main difficulties to create a fully automated system to robustly locate and identify the vertebral bodies in ct images are related to the similarity among anatomical landmarks of the spinal column , variability in spine curvature and shape , possible artifacts caused by metal implants , the presence of different bone abnormalities and pathologies and restrictions in the z - axis field of view ( fov ) with acquisitions not covering all vertebrae in the longitudinal axis , based on the specific region of interest being studied . 
additionally , the use of real - world data ( rwd ) , that is , the use of studies coming directly from the hospital image repository , acquired with the inherent variability and biases of daily practice conditions , is a key point to develop a methodology directly applicable in clinical routine . some previous methods were focused on specific regions of the spine [ 46 ] or relied on prior knowledge about which region was examined and visible [ 7 ]  . 
introduced a similar methodology by using the same image features extraction steps as in [ 10 , 11 ] ; however , a novelty on the classification task was introduced , and it was used a feed - forward deep neural network ( dnn )  . 
prior to the fully connected layers , with classification purposes , there are several layers based on convolutional filters extracting from very simple features , such as brightness and edges , to most complex features that uniquely define the image . 
 [ 13 ] introduced a hybrid method based on the combination of a random forest classifier to roughly locate vertebra candidates with a joint convolutional neural network ( j - cnn ) for a more accurate vertebra localization . 
 [ 14 ] developed a method based on a deep image - to - image network ( di2in ) to initialize vertebra locations combined with a sparsity regularization refinement step . 
 [ 15 ] proposed a method which combined a 3d fully convolutional neural network ( fcn ) to extract short - range contextual information around the target vertebra , with a bidirectional recurrent neural network ( bi - rnn ) to extract long - range contextual information to encode the spatial and contextual information among the vertebrae of the whole fov . machine learning ( ml ) applications , as a branch of artificial intelligence ( ai ) , have grown significantly in the last decade . 
decision forests are a supervised ml technique composed by decision trees , the word supervised means that an associated set of output data is needed for each set of training data . 
a significant advantage of ml over other ai techniques , such as deep learning ( dl ) , is that they do not require high computational loads when training a model , and additionally , they offer better performance when leading with a small training dataset . we aimed to propose a novel method for vertebrae centroid localization and identification on ct images . 
the method might be able to predict the vertebral bodies position present on ct exams where no assumptions about the scanned region is made . materials andmethods dataset the dataset was collected retrospectively through an observational study approved by the ethics committee and waived from informed consent collection . 
the data finally included and used for the development of the algorithm consisted of 232 multi - detector ct scans acquired both with 64 and 256 detector systems ( philips ct brilliance and ict , best , the netherlands ) with different arbitrary field - of - views . 
the population series were patients that underwent either thoracic , abdominopelvic or cervical - thoracic - abdominopelvic ct examinations in a single longitudinal continuous acquisition in a period of 12months ( may - 2015 to may - 2016 ) , including patients between 18 and 80years old . 
the labeling was done , by 1 3 50 la radiologia medica ( 2020 ) 125 : 4856 an expert in the radiological field , by selecting the centroids of all vertebrae present on the images . 
the set of annotated vertebrae was defined as c = { t1 , , t12 , l1 , , l5 , s1 } , which contained both whole thoracic and lumbar regions and one additional sacrum vertebra . for each image , the annotated centroids were stored in a matrix which included the absolute coordinates ( ci 3 ) and the specific label of each vertebra ( ci ) present on the image . 
 all these images were manually annotated by a radiology expert using an application designed ad hoc . methodology the method was developed using both python 3.5 and matlab r2016a ( mathworks inc . , natick ma , usa ) in a scientific computing server with an intel i7 processor running at 3.6ghz and 54gb of ram memory . the approach was developed on two stages by combining rrf with image - based algorithms . 
the second phase points to refine the prior detection considering the spine morphology by obtaining the spinal cord position using voxel - wise operations . detection based onrandom regression forests an initial approach to locate the centroids position of all the vertebral bodies present in the images was performed by training a rrf network . 
it was trained a single rrf for all vertebral centroids present on an image . for the image labeling phase , an in - house software application was developed to visualize and label the centroids of all vertebrae in the datasets of the study . 
the goal was to learn a mapping function : d3 . for the feature extraction , n voxels ( x 3 ) were randomly chosen within the fov of the image , being their relative displacement ( d 3 ) the information to be predicted , i.e. , their offset to each vertebra centroid : di = ci xi . 
then , from each block , the mean intensity was calculated , having f intensity - based features associated with each training voxel . the mean intensities over cuboidal regions are computed in a short time using the integral image [ 17 ]  . 
the advantage of this technique is that the sum of the voxels over any subvolume can be calculated in constant time once the integral image over the whole ct volume is obtained , no matter how big the volume is . 
the integral image is an intermediate representation of an image , where each voxel ( x , y , z ) is the sum of the voxels immediately adjacent ( left , front and up ) to x , y , z in the original image . 
the mean intensity of any block can be computed as : e [ x ] = ( iig iie iih + iif ) ( iic iia iid + iib ) where { a , , h } 3 are the eight vertices of the block and n is the number of voxels within de block . for the testing stage , once the rrf is trained , given a new unseen image , m voxels ( x 3 ) were randomly selected on the image , and f intensity - based features ( fj d ) were extracted in the same way as on the training stage . 
knowing the location of the reference voxel and the predicted relative distance vector to the center of a specific vertebral body , the predicted location was computed as cj = dj + xj . from each testing voxel , a predicted location was obtained . 
the global maximum of the density function was considered as the predicted location of the vertebral body centroid in the image . refinement based onvoxelwise operations due to the expected population variability in spine curvatures , a refinement step was added in order to adapt the centroid detection to the patient - specific spine morphology . 
at this point , the background was removed and the spinal canal was isolated removing regions with an area lower than 500mm3 and adding a boundary condition to detect the spinal canal only in the posterior region of the image . 
g spinal canal centerline training several options , obtaining the best performance adjusting the displacement to 2cm . with the spine centerline detection , the previously obtained centroid coordinates ( x , y , z ) were transformed to the final ( x , y , z ) coordinates . 
as a last refinement step , for each z = z point , its corresponding ( x , y ) coordinates were changed to ( x , y ) , adapting each predicted vertebra centroid to the spine curvature . the parameters used in the trainingtesting stages can be appreciated in table1 . therefore , considering the whole training dataset , the rrf was trained with 45.824 samples , having 256 features each one . 
all these features were used to train the rrf , with a total training time of 3h . table 1 parameters used in the trainingtesting steps parameter description [ px py pz ] [ bx by bz ] n . 
the lower rows show the parameters used to build the rrf 1 3 la radiologia medica ( 2020 ) 125 : 4856 testing andperformance evaluation to test a new image , unseen on the training stage , 50.000 random voxels were selected , with 256 features for each testing voxel . 
total testing time was 3min . to evaluate the performance of the network , the distance between the predicted position of each centroid and the real one , defined by previous expert annotations , as well as the identification rate was calculated . 
it is a case of a patient with a significant scoliosis ; this is the reason why some vertebrae are not visible on the sagittal view 1 3 54 la radiologia medica ( 2020 ) 125 : 4856 fig . 
in the lumbar region , the localization error is very similar for all vertebrae . this rate increases in both regions , increasing mainly in the thoracic region . the localization error and the identification rate obtained after rough detection and after refinement are summarized in table2 . in table2 , it can be seen the improvement of both the distance between the predicted vertebrae position and the real one and the identification rate after refinement . 
after the rough detection , the identification rate is similar both in thoracic and lumbar regions ; however , after refinement , discussion in this work , an approach for the automatic localization and identification of the vertebral bodies in ct scans has been proposed using rrf . 
the algorithm has been tested using a dataset including both healthy and pathological cases and where no assumptions about the visible region have been made , therefore working with arbitrary fovs . 1 3 la radiologia medica ( 2020 ) 125 : 4856 fig . 
7 median localization error per vertebrae table 2 localization errors in mm obtained after rough detection ( left ) and after refinement ( right ) region rough detection refined detection median mean id . 
therefore , in our method , cervical vertebrae can be present in the images under study ; however , their position will not be predicted . conclusion rrf allows a reliable vertebrae localization and identification in real - world ct data . 
due to the high variability in the field of view and anatomical landmarks between different ct scans , it might be very difficult to consistently obtain a high - accuracy prediction of vertebrae position . 
the aim of this study was to develop prediction models of radiotherapy - induced toxicities in prostate cancer patients based on computed tomography ( ct ) radiomics , clinical and dosimetric parameters . methods in thisprospective study , prostate cancer patients were included , and radiotherapy - induced urinary and gastrointestinal ( gi ) toxicities were assessed by common terminology criteria for adverse events . 
goodness of fit of the models and performance of classifications were assessed using hosmer and lemeshow test , 2log ( likelihood ) and area under curve ( auc ) of the receiver operator characteristic . results sixty - four prostate cancer patients were studied , and 33 and 52 patients developed grade 1 gi and urinary toxicities , respectively . 
many different studies have been made to model these complications based on the dosimetric and clinical features [ 35 ] , but there are several limitations regarding shayan.mostafaei@kums.ac.ir * shayan mostafaei * hamid abdollahi hamid_rbp@yahoo.com extended author information available on the last page of the article these models including variations in patient radiosensitivity , uncertainties in dosimetric and planning parameters of the models . based on clinical and radiobiological points of view , patients response to radiotherapy is an individualized issue and incorporating patients ( inherent ) radiosensitivity into radiation treatment from patient selection to planning could enhance final therapy outcomes [ 6 ]  . 
however , gene expression profiling is dependent on the surgical procurement ( or blood capture ) , yielding a host vol . : ( 0123456789 ) 1 3 88 la radiologia medica ( 2020 ) 125 : 8797 of risks and potential complications , and making it an unrealistic option for every cancer patient [ 9 ]  . proctitis and grade 1 cystitis were assigned as main toxicities for rectum and bladder , respectively . recently , a considerable amount of literature has been published on radiomics , which refers to mathematical and statistical methods used to extract a large number of features from medical images in order to associate them with clinical and biological parameters [ 1012 ]  . 
studies have demonstrated that different features extracted from medical images , alone or in combination with clinical / dosimetric parameters , could improve the prediction of radiation toxicities in organs including rectum [ 13 ] , bladder [ 14 ] , lung [ 15 ] , ear [ 16 ] and parotid [ 17 ]  . 
these developed radiomics models have coped on previous models limitations by incorporating phenotypically patients features ( radiomic features )  . to date , little evidence has been found associating computed tomography ( ct ) image features with radiation toxicities in rectal and bladder . 
in the present study , we aimed to analyze the performance of ct radiomic features with and without clinical / dosimetric parameters to predict cystitis as an acute urinary toxicity and proctitis as a gi toxicity by stacking ensemble machine learning algorithto the best of our knowledge , this is the first study on this issue . materials andmethods study design andpatients this prospective study was approved by the local ethics committee , and the informed consent requirement was waived . 
 regarding 3dcrt , patients received 70gy in 35 fractions and plans were made using isogray tps . radiation - induced proctitis and cystitis were assessed weekly during the therapy and a month after that based on the common terminology criteria for adverse events ( ctcae ) version 4.03. 
the radiation - induced grade 1 clinical features for each patient , clinical features including stage , gleason score , age , prostate - specific antigen ( psa ) , prostate volume , planning target volume ( ptv ) , conformity index , heterogeneity index , mean / min / max prostate dose , rectal and bladder dose volume including total volume and wall volume and d5d95 and v5v75 for both total volume and wall volume weremeasured . 
ct images were obtained using kv = 110 , mas = 225 , field of view ( fov ) = 380 380mm , matrix = 512 512 , thickness = 3.0mm and gap = 0.8.mm. regionofinterest delineation all images were analyzed by a radiologist with 10years of experience in pelvic imaging . 
the regions of interest ( rois ) were created manually via the itk - snap software ( ap.org ) including the rectal and bladder walls and excluding the rectal lumen and bladder entity . 
figure1 shows delineated rois on rectal and bladder walls . radiomic feature extraction ct images for each patient were normalized with z - score in order to obtain a standard normal distribution of image fig . 
before feature extraction , three preprocessing steps including wavelet and laplacian of gaussian ( log ) filters ( filter value : 0.51.0 ) and 64 - bin normalization were applied on ct images . feature selection in order to overcome overfitting problem , remove irrelevant and redundant features that do not contribute to the accuracy of a predictive model , and provide faster and more costeffective models , we used stacking algorithm and elastic net penalized logistic regression for feature selection and prediction , simultaneously . first - order statistics ( fos ) gray - level co - occurrence matrix ( glcm ) gray - level run length matrix ( glrlm ) table 1 radiomic features 1 . 
we developed and compared different predictive models based on the ct image features , and clinical features by using stacking algorithm and elastic net penalized logistic regression , in order to feature selection and binary classification . 
stacking as a meta - ensemble machine learning algorithm is a collective decision - making system , which is able to combine the predictions of learned classifiers in order to create prediction of new instances . 
but , stacking was used to improve predictive performance by a compromise between la radiologia medica ( 2020 ) 125 : 8797 bias and variance like penalized logistic regression [ 18 ]  . 
in the stacking , all of the other algorithms , as base learners , are trained using the available data , and then a combiner algorithm , as a meta - learner , is trained to make a final prediction using all the predictions of the other algorithms as additional inputs . 
goodness of fit ( gof ) of the models and performance of classifications were assessed using hosmer and lemeshow test , 2log ( likelihood ) and area under the curve ( auc ) of receiver operator characteristic ( roc )  . 
the repeated k - fold cross - validation is another way to bring down the high variability of cross - validation , to aims stability selection [ 19 ]  . 
however , this study attempt to fill that the sensitivity of feature selection algorithms to variations in the training and testing sets by repeated 100 times 5 - fold cross - validation . 
a flowchart of stacking algorithm via repeated 100 times 5 - fold crossvalidation is shown in fig.2. data set feature selec ( cid : 31 ) on base learners random forest neural network meta learner penalized logis ( cid : 31 ) c regression 5 - cv : 4 sub samples as train predic ( cid : 31 ) on model calculate i 1 : 5 5 - cv : other sub samples as test select best predic ( cid : 31 ) on model based on average of i 1 : 5 fig . 
2 a flowchart of stacking algorithm via repeated 100 times 5 - fold cross - validation 1 3 la radiologia medica ( 2020 ) 125 : 8797 results sixty - four prostate cancer patients were studied , and 33 patients developed grade 1 proctitis . 
for radiomics models , features including large - dependence low gray - level emphasis , gray - level variance , short - run low gray - level emphasis and small - area low gray - level emphasis were selected . 
the features are maximum 3d diameter , skewness , inverse different momentum and joint entropy , and dosimetric parameters are median - db ( median dose received by bladder ) , db - 40 ( dose received by 40% of volume of bladder ) and vw - 45 ( percent of bladder wall volume , which received 45gy )  . 
for clinicalradiomics model , one dosimetric ( modal - dr ) and three radiomic features including elongation , 90 percentile and long - run low gray - level emphasis were selected . 
selected radiomic features are smalldependence low gray - level emphasis , high gray - level zone emphasis and small - area low gray - level emphasis , which belong to gldm and glszm feature set . models performances for prediction of cystitis are given in table5 . 
our results showed the feasibility and good performance of pre - treatment ct image features as new table 2 patients characteristics characteristic value proctitis grade 1 value cystitis grade 1 value no . 
for both radiation proctitis and cystitis , we showed image features alone or in combination with clinical / dosimetric parameters could enhance the prediction performance ( auc )  . to the best of our knowledge , this is the first study for prediction of radiotoxicity using ct imaging and clinical\ dosimetric features in prostate cancer patients . 
 for cystitis , we showed that the combination of radiomic features with clinical / dosimetric features could enhance the predictive performance form 0.71 ( for radiomic model ) and 0.67 ( for clinical model ) to 0.77. 
however , for proctitis modeling , results are different and combination of radiomics and clinical features has lower performance than the radiomic model . there are several interesting works on radiomics modeling for predicting radiotherapy - induced normal tissue complications and tissue structural changes . 
in another work , they also developed predictive models based on ct image features and clinical parameters for prediction of late patient - rated moderate - to - severe xerostomia and sticky saliva after radiotherapy [ 23 ]  . 
 [ 24 ] also demonstrated that incorporation of organand dose - shape descriptors is beneficial for xerostomia prediction in highly conformal radiotherapy treatments . since none of the single classifiers worked properly , as was indicated that stacking classifier reduce the models variance and its bias by powerful process of group averaging or majority vote [ 18 , 25 ] , this ensemble algorithm can be better than the single classifiers in prediction and classification [ 26 ]  . 
other advantage of stacking algorithm is applicable of this algorithm to combine models and algorithms of different types [ 18 ]  . in recent years , radiotherapy outcome modeling has been evaluated to develop models based on the parameters which have contribution to the development of radiotherapy endpoints without over / underfitting trends in the data . 
for this purpose , pre - treatment factors such as radiomics features extracted from the patients images could help clinicians to identify candidate patients for dose escalation or dose reduction [ 27 ]  . 
our study is an outcome modeling work to predict toxicity based on the high - quality ct images which is an easy to use , noninvasive and costbenefit approach . although the results of this study are significant , there are five main limitations . 
although our imaging protocol was similar for all patients , it is better to find robust features against radiomics challenges such as roi delineation size and shape as was discussed by some previous studies [ 2832 ]  . 
third , interpretability of the results in ensemble learning method ( stacking ) may be difficult [ 33 ] , but it is a new feasible approach to develop predictive models . 
in addition , we suggest researchers to perform these radiomics analysis with a standard ct scanner including standard simulation ct which has applications before the radiotherapy to perform treatment planning . conclusions the results presented here indicate that ct image features are new markers for prediction of radiation - induced gi and urinary toxicities . 
moreover , we showed that the inclusion of the clinical , dosimetric and imaging features in the cystitis model might improve the model predictive performance . acknowledgements this work was supported by shahid beheshti university of medical sciences and behnam daheshpour charity organization . 
then , the correlation between t1 relaxation time and fsf was assessed . results t1 relaxation times of pancreatic parenchyma and bone marrow on the t1 map images without fat suppression showed significantly negative correlation with fsf ( pancreas , r = 0.394 , p = 0.007 ; bone marrow , r = 0.550 , p < 0.001 ) , while there were no significant correlations between them on the t1 map images with fat suppression . 
conversely , on the t1 map images with fat suppression , no significant differences in t1 relaxation times were found between two groups . conclusion t1 relaxation time of the pancreas on t1 mapping was influenced by the presence of fat deposition . 
therefore , fat suppression technique in t1 mapping will be essential for evaluating t1 relaxation time of pancreatic parenchyma . keywords pancreas dual - flip - angle t1 mapping fat suppression technique introduction t1 mapping on mr imaging has shown the potential to be a valuable tool for determining disease severity based on pathological changes such as fibrosis , edema and fat deposition in each organ [ 15 ]  . 
for example , t1 mapping has been successfully used for assessment in a number of cardiac conditions , including myocardial fibrosis and myocardial deposition diseases [ 6 , 7 ] , and the measurement of the t1 relaxation time using fast volumetric t1 mapping techniques is used for the quantitative evaluation of liver fibrosis [ 8 ]  . 
however , it is known that the t1 relaxation time of the * katsuyoshi ito itokatsu@yamaguchi - u.ac.jp 1 department ofradiology , yamaguchi university graduate school ofmedicine , 1 - 1 - 1 minami - kogushi , ube , yamaguchi755 - 8505 , japan organs could be affected by the deposition of iron and collagen , and possibly by fatty infiltration [ 9 ]  . increased fatty infiltration in the pancreas has been seen in many conditions , including obesity , increased age , cushings syndrome , cystic fibrosis and lipomatous pseudohypertrophy [ 10 ] , and can be observed even in the pancreatic parenchyma in patients with chronic pancreatitis . 
recent studies have reported that t1 relaxation time of the pancreatic parenchyma measured on t1 mapping is significantly longer in patients with mild chronic pancreatitis than in patients with a healthy pancreas [ 11 , 12 ]  . 
however , the influence of fat deposition on the t1 relaxation time of the pancreatic parenchyma has not been fully understood because little has been reported on the effect of fat suppression techniques on t1 mapping of the pancreas . 
fifty - six consecutive patients who were suspected of having biliary or pancreatic diseases based on clinical history or previously performed ultrasonography or computed tomography ( ct ) underwent upper abdominal mr imaging including t1 mapping at our institution between october 2017 and december 2017 . 
 among these 56 patients , two patients with chronic pancreatitis were excluded from the analysis since the fibrotic change in chronic pancreatitis can , r1 - 1 , substantially affect the t1 value of the pancreatic parenchyma . 
patients with pancreatic ductal dilatation ( n = 3 ) , postoperative recurrence of pancreatic cancer ( n = 1 ) and severe motion artifacts ( n = 5 ) were also excluded . finally , forty - five patients ( mean age , 68years ; range 6280years ) were included in our study , which consisted of 22 men ( mean age , 68years ; range 6378years ) and 23 women ( mean age , 74years ; range 6181years )  . 
these included patients with pancreatic diseases ( n = 31 ) , including intraductal papillary mucinous neoplasms ( n = 20 ) , pancreatic cyst ( n = 5 ) , suspected serous cystic neoplasm ( n = 1 ) , groove pancreatic lesion ( n = 1 ) and a small nodule on the papilla of vater ( n = 1 ) ; and patients with biliary diseases ( n = 12 ) , including common bile duct stone ( n = 3 ) , benign biliary stricture ( n = 2 ) , cholangitis ( n = 1 ) , adenomyomatosis ( n = 3 ) , cancer ( n = 2 ) and a gall bladder polyp ( n = 1 ) ; and patients with no pathological disease ( n = 5 )  . mr imaging technique all mr imaging was performed with a 3.0t clinical mr system ( magnetom prisma , siemens healthcare , erlangen , germany ) and an 18 - channel body coil . 
the imaging parameters were as follows : thirtysix axial slices of 4mm thickness were acquired within a 19 - s breath hold with the following parameters : repetition time ( tr ) , 8.72ms ; echo time ( te ) , 2.463.92ms ; flip angle , 3 and 19 ; acquisition matrix , 135 224 ; parallel imaging factor , 3 ; field of view , 305 380mm ; and bandwidth , 300hz / pixel . 
the reviewers measured the t1 relaxation time of the pancreatic parenchyma on the t1 map images with and without fat suppression using operatordefined regions of interest ( rois )  . 
attention was given to drawing roi circles as large as possible in a homogeneous region of the pancreatic parenchyma avoiding volume averaging from the pancreatic duct , vessels , and retroperitoneal fat . 
the fat signal fraction ( fsf ) of the pancreas and bone marrow was also measured on fat fraction images obtained by six - point dixon t1 - weighted imaging at the same location as the t1 map images . 
 conversely , on the t1 map images without fat suppression , the t1 relaxation times of the pancreatic parenchyma in patients with fsf 10% were significantly shorter [ 822ms ( range 700907ms ) ] than those in patients with fsf < 10% [ 933ms ( range 8751030ms ) , p = 0.041 ] ( table1 )  . 
however , when a cutoff level of fsf was set at 5% , the difference in the t1 relaxation time of the pancreatic parenchyma was not significant between patients with fsf 5% and those with fsf < 5% on both t1 map images with fat suppression [ 909ms ( range 8121014ms ) vs . 
955ms ( range 8741024ms ) , p = 0.256 ] ( table2 )  . regarding bone marrow , the t1 relaxation time of the bone marrow in patients with fsf 10% was also significantly shorter [ 669ms ( range 626726ms ) ] than that in patients with fsf < 10% [ 859 ms ( range 732954 ms ) , p = 0.005 ] on the t1 map images without fat suppression . 
there was no significant correlation between fsf and t1 relaxation time ( r = 0.047 , p = 0.760 ) table 1 comparison of t1 relaxation times of the pancreatic parenchyma between patients with fsf 10% and patients with fsf < 10% fsf < 10% ( n = 36 ) fsf 10% ( n = 9 ) 845 ( 791986 ) 880 ( 833947 ) 0.514 933 ( 8751030 ) 822 ( 700907 ) 0.041 t1 map image with fat suppression ( ms ) t1 map image without fat suppression ( ms ) data are median with 25th and 75th percentiles in parentheses fsf fat signal fraction table 1 shows the comparison of the t1 relaxation times of the pancreatic parenchyma between patients with fsf 10% and patients with fsf < 10% . 
the t1 relaxation time can provide valuable information on a variety of pathological conditions of each organ , including the liver and the pancreas [ 9 , 13 ]  . 
another study using a multivariate regression analysis showed that the t1 relaxation time of the pancreas was independently associated with the diagnosis of mild chronic pancreatitis [ 12 ]  . 
however , a previous study indicated that pancreatic fibrosis may be accompanied by pancreatic steatosis [ 14 ] , and additionally , increased fat deposition in the pancreatic parenchyma can be observed in many conditions , including aging and obesity . 
in this context , we designed this study to assess the influence of fat deposition on the t1 relaxation time of the pancreatic parenchyma using dual - flip - angle t1 mapping with and without fat suppression . 
in this study , the t1 relaxation time of the bone marrow was also measured as a reference organ with abundant fat deposition because of the small number of patients with severe fatty infiltration of the pancreas . in this study , on the t1 map images without fat suppression , the t1 relaxation time of the pancreatic parenchyma showed a significant negative correlation with the fsf . 
these findings suggest that the t1 relaxation time of the pancreatic parenchyma is likely to decrease with an increase in fat deposition on the t1 map images without fat suppression . 
our findings demonstrated that the t1 relaxation time of the pancreatic parenchyma was less likely influenced by increased fat deposition on the t1 map images with fat suppression , which indicates that the application of a fat suppression technique in t1 mapping would be indispensable for accurately evaluating the t1 relaxation time of the pancreatic parenchyma . similar results were obtained when we assessed the correlation between fsf and the t1 relaxation time of the bone marrow , which has a relatively higher fsf value . 
these results suggested that the t1 relaxation time of the pancreas with abundant fat deposition will be strongly influenced by the presence of fat deposition on t1 map images without fat suppression , and that the application of a fat suppression technique in t1 mapping will be essential for the evaluation of the t1 relaxation time of the pancreas with severe fatty infiltration in patients with chronic pancreatitis . conversely , when a cutoff level of fsf was set at 5% , no significant difference was observed between the t1 relaxation times of the pancreatic parenchyma in patients with fsf 5% and those in patients with fsf < 5% on both the t1 map images with and without fat suppression . 
these facts indicated that the t1 relaxation time of the pancreas will be less likely influenced by the presence of minimal fat deposition on t1 map images , and can be evaluated by both the t1 map images with and without fat suppression . previous studies have reported the usefulness of different imaging techniques such as diffusion weighted imaging , mrcp with spatially selective ir pulse , secretin stimulated mrcp and mr elastography for the diagnosis of chronic pancreatitis [ 12 , 1518 ]  . 
thus , multiparametric mr imaging with the combination of these techniques and t1 mapping with a fat suppression technique should be conducted for the surveillance of patients who are considered to have a high risk of developing chronic pancreatitis . the present study was associated with several limitations . 
first , a selection bias may have been inevitable as our study was retrospective with a relatively small number of patients , and there was no correlation with bioptic samples of the pancreas . 
although this technique is a simple and generic method that is reported to give similar data from the sampling of an inversion curve [ 19 ] , further investigation and comparison among different methods will be needed to validate our results . 
the validity of our results should be investigated in cases involving severe fat infiltration of the pancreatic parenchymal tissue in patients with pancreatic endocrine or exocrine insufficiency in a future study . 
 fourth , although the roi measurements were obtained from the head ( 1 roi ) and the body or tail ( 1 roi ) of the pancreas in this study , it would have been better to measure the t1 relaxation time of the head , the body and the tail separately ( 3 rois ) for more precise evaluation , using thinner 1 3 6 la radiologia medica ( 2020 ) 125 : 16 slice sections . 
finally , validation study for the accuracy of this method as well as further study in patients with chronic pancreatitis will be necessary for clinical application of t1 mapping of the pancreas . conclusion in conclusion , the t1 relaxation time of the pancreas on t1 mapping without fat suppression was influenced by the presence of fat deposition . 
thus , the application of a fat suppression technique in t1 mapping will be essential for evaluating the t1 relaxation time of the pancreatic parenchyma . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 declaration of helsinki and its later amendments or comparable ethical standards . 
secondary endpoints were : safety , liver toxicity , 1 - month percentage of tumor necrosis according to the modified recist criteria . results two hundred and sixty - seven dsms - tace were performed in 137 hcc patients ( 33 patients in bclc stage a , 84 patients in bclc stage b , and 20 in stage c )  . 
certainly , the literature suggests that efficiency and success of these treatments are mainly dependent upon the ability of the interventional radiologist to perform selective or super - selective embolization with a complete embolization of tumor feeding vessel ( tfv ) [ 5 ]  . 
permanent occlusion of tfv or an incomplete embolization could induce intraand intercellular signaling processes counteracting and reversing hypoxia [ 6 ] , as vascular - endothelial - growth - factor ( vegf ) stimulation [ 7 ]  . 
 [ 13 ] in 2017 reported encouraging results from initial experience of repeated transarterial chemoembolization with dsms - tace in 24 patients with unresectable hepatocellular carcinoma . primary end point of this study is to describe the longterm outcome , in terms of ttp and os , in a large clinical cohort of patients with unresectable hcc treated with repeated dsms - tace . 
secondary endpoints are : safety , liver toxicity , 1 - month percentage of tumor necrosis according to the modified recist criteria [ 14 ]  . materials andmethods patient selection this is a single - center consecutive patients cohort study . 
 after evaluation of a multidisciplinary team ( mdt ) of hepatologists , surgeons and interventional radiologists [ 15 ] , dsms - tace was proposed for patients who fit the selection criteria , as shown in table1 . percutaneous ablation was not performed due to tumor location or patient intolerance . in 24 patients , dsms - tace was successfully performed as bridging therapy or as down - staging therapy to orthotopic liver transplantation ( olt )  . 
all patients underwent a contrast - enhanced ct , and cross - sectional imaging or mri at least 2weeks before each treatment , to stage or re - stage diseases . dsmstace procedures all procedures were performed by one interventional radiologist with more than 20years of chemoembolization experience in a dedicated angio - suite rooall patients received a premedication consisting of a proton - pump inhibitor , a prokinetic drug and an analgesic drug ; if necessary a conscious sedation was performed during procedures . the flow diagram of procedure is graphically reported in fig.1. when possible , a super - selective ( segmental or sub - segmental ) approach was obtained using a microcatheter . 
however , in case of multiple ( > 3 ) hcc in the same lobe or when the selective catheterization of the feeding artery was not technically feasible , we performed a lobar embolization paying particularly attention to prevent non - target embolization . as previously described [ 13 ] , dsms were mixed with non - ionic contrast mediusix milliliters of non - ionic contrast was used per 4ml of dsms prior to injection . 
 dsms and doxorubicin were injected until initial stasis of this mixture was observed on tumor feeding vessels . as a result , dsms alone were slowly and continuously injected until complete embolization was obtained . 
unenhanced cone beam ct , acquired directly after dsmstace , was used to assess deposition in hepatocellular carcinoma of temporary embolization agent . treatment evaluation : shortterm results the follow - up assessment included detailed history taking and physical examination , laboratory tests , and an abdominal contrast - enhanced ct or mr examination . 
all patients underwent imaging follow - up 1month after initial table 1 inclusion and exclusion criteria inclusion criteria exclusion criteria age > 18years mono or multifocal measurable hcc nodules total bilirubin < 3mg / dl no evidence of extrahepatic metastasis prior surgical or loco - regional treatment only if performed more than evidence of severe liver function deterioration ( childpugh score > 11 ) complete thrombosis of the main portal vein incorrigible coagulopathy serum creatinine levels > 2.0mg / dl any preexisting medical conditions of sufficient severity to prevent full 3months before the study compliance with the study 1 3 100 la radiologia medica ( 2020 ) 125 : 98106 fig . 
sma superior mesenteric artery dsms - tace and mrecist criteria were used to assess response after all treatments [ 14 ]  . the safety of all the patients , who underwent dsmstace , was assessed by using the society of interventional radiology classification system [ 16 ]  . repeat dsms - tace procedures were performed when follow - up imaging studies showed residual or recurrent hcc and patients continued to be within the selection criteria . 
 repeated sessions of dsms - tace were considered if residual viable or newly developed tumors were identified on images1month after the previous procedure and were performed on an on - demand basis depending on individual tumor response and hepatic functional reserve . 
 criteria for discontinuation - repeated dsms - tace were decompensated liver diseases , development of tumor thrombosis of main portal veins without collateral vessels , and development of major complications or patient refusal . 1 3 la radiologia medica ( 2020 ) 125 : 98106 treatment evaluation : longterm results table 2 patients characteristics os was estimated from the first treatment date until death or last follow - up . 
patients undergoing olt were censored at the time of transplant . we analyzed both ttp , time from randomization to radiological progression based on mrecist ( appearance of new enhancement whether in the treated tumor or untreated tumor ) , both os . 
at 1month follow - up , all the cases with progression disease ( pd ) or stable disease ( sd ) were recorded as local tumor recurrences . statistical analysis statistical analysis was performed with graphpad prism 7.0c. data were analyzed via descriptive statistics ( median and standard deviation , sd )  . the chi - square or fishers exact tests were used for the categorical data and paired t test for the continuous data . ttp and os probabilities were estimated using the kaplanmeier method . 
a mean dose of 40mg doxorubicin was administered in each dsms - tace session . there was one death within 30days from treatment due to massive hepatic artery occlusion and liver failure . 
after the fourth treatment , performed in 12 patients , cr was achieved in 8.3% of cases , pr in 16.7% , sd 1 3 102 la radiologia medica ( 2020 ) 125 : 98106 fig . 
ct after 1month shows pr with partial necrosis of 2 small hcc nodules ( e , f , white arrows ) and complete necrosis of larger lesions ( f )  . 
after third dsms - tace j performed after 6 weeks from second procedure , c.e.ct k , l shows cr of in all target lesions with disappearance of any intratumoral arterial enhancement ( white asterisk ) in 50% and pd in 25% of cases . 
first dsms - tace is performed with segmental technique ( c ) and no - contrast cone beam ct ( d ) at the end of embolization shows lesion satisfactory embolized . 
ct after 1month ( arterial and venous phase , e , f ) shows pr of lesion with decrease of contrast - enhanced viable target lesion , associated with a significant volumetric reduction of lesion ( white asterisk )  . 
 [ 22 ] , using dsm - tace in 50 hcc patients , reported an objective response rate lower than our results ( 44 vs 85% ) with a disease control rate of 70% . 
 in our study , a sustained percentage of stable disease was observed , with not significant worsening of liver function , in patients who underwent subsequent treatments ( until five treatments in nine patients ) with a disease control in more than 80% of patients . our findings support the statements from georgiades etal . 
 [ 25 ] treating 47 hcc patients with dsm and lipiodol mixed with doxorubicin and cisplatin reported a median survival rate of 26months and 1 - year survival rate of 75% . 
 b kaplanmeier survival curves showing significant differences in os between patients in bclc stage a ( blue line ) versus stage b ( red line ) versus stage c ( green line )  . 
 [ 26 ] , the initial and the best response could predict os and ttp effectively and achievement of treatment response at early time - points is still the robust predictor for favorable outcomes . 
 [ 27 ] in a study evaluating factors affecting survival following dee - tace for inoperable hcc concluded that the presence of more than 50% necrosis after dee - tace was an independent predictor for progression - free survival ( pfs ) and os . 
 hepatic abscess occurred in two patients that underwent four repeated dsms - tace . regarding the impact of dsms - tace on liver function , our results are similar to results from bargellini etal . 
the feature of degradability of dsms would seem to be related to lower damage to normal liver tissue [ 10 ] , and thus the lower incidence of adverse events could be explained . this study has certain limitations . 
such variations included segmental , subsegmental or lobar embolization technique , which could have affected the degree of response to treatment , as also the judgment of end point of stasis . 
thus , the amount of chemotherapy agent could be taken into consideration as a variable and therefore one of the limitations of this study . 1 3 la radiologia medica ( 2020 ) 125 : 98106 fig . 
 b kaplanmeier survival curves showing significant differences in ttp between patients in bclc stage a ( blue line ) versus stage b ( red line ) versus stage c ( green line )  . 
two radiologists ( 25 and 11years of experience , respectively ) , blinded to clinical data , evaluated the presence labral tears on virtual - blended 120kv standard cta and on de - cta images . 
magnetic resonance arthrography ( mra ) is a reliable imaging vol . : ( 0123456789 ) 1 3 40 la radiologia medica ( 2020 ) 125 : 3947 tool for the diagnosis of glenoid , labrum , and rotator cuff lesions [ 37 ]  . 
 although mra has demonstrated to be superior for the identification of partial or intra - substance rotator cuff tears , cta represents a more reliable imaging tool for the evaluation of glenoid rim fractures and inferior glenohumeral ligaments injuries , including humeral avulsion of glenohumeral ligament ( hagl ) [ 14 ]  . 
also , ct can be used in case of shoulder dislocation or shoulder instability in order to evaluate the presence of glenoid bone loss , which is a crucial factor for treatment choice [ 17 ]  . dual - energy ct ( dect ) has been recently proposed in musculoskeletal imaging : potential advantages are the virtual noncalcium images for detection of bone marrow edema or the use of monoenergetic images of varying kiloelectron volts for image contrast optimization and metal artifact reduction [ 1821 ]  . 
even though suggested by previous authors [ 22 ] , there are no papers describing the role of dect arthrography ( de - cta ) of the shoulder . dect features such as the reduction in metal artifacts in operated shoulders , or the optimal visualization of contrast material injected , choosing the best kv values during postprocessing , could increase the overall diagnostic accuracy with respect to standard cta [ 1921 ]  . the purposes of our study were therefore : ( 1 ) to investigate the diagnostic accuracy values of de - cta in detecting glenoid labrum tears , compared with mra , using surgery as the standard of reference ; ( 2 ) to assess the possible increase in diagnostic accuracy allowed by the de - cta images with respect to standard cta virtual - blended 120 - kv images . patients andmethods patient population this prospective study was approved by the institutional review board . 
 the mean interval between the imaging studies and surgery was 32days ( range , 365days )  . mra imaging technique a 1.5 tesla scanner ( siemens magneton avanto , siemens medical systems , erlangen germany ; sq - engine ; gradient strength 45 mt / m ; slew rate 200 t / m / s ) was used . 
patients were imaged supine with the humerus in a neutral position and the thumb pointing upward , by using a flexible four - channel body matrix phased - array surface coil ( siemens body matrix ) and a six - channel spine matrix coil ( siemens spine matrix ) which was integrated into the examination table . 
postprocessing was performed on a dedicated 3d processing workstation ( syngo mmwp ve36a , siemens ag , berlin , germany ) ; 3d images were reconstructed on the desired imaging planes with variable image thickness ( usually 0.82mm ) according to radiologists choice and depending on the case analyzed . 
 decta imaging technique the dect examinations were performed with a thirdgeneration 384 - slice dual - source ct scanner ( somatom definition force , siemens healthcare , forchheim , germany )  . 
the predefined tube currenttime product was set at a ratio of 1.6 : 1 ( tube a , 220 quality reference mas ; tube b , 138 quality reference mas )  . 
soft - tissue kernel ( qr32 ) 80 - kvp and 150kvp set images were transferred to an off - line workstation ( syngovia vb20 ; siemens , erlangen , germany )  . 
each reader was free to adjust the kv values in the post - processing phase in order to reduce metal artifacts or to enhance the visualization of contrast material injected between articular cavity . image analysis the images were reviewed by three experienced radiologists ( readers 1 , 2 , and 3 , with 21 , 11 , and 24years of experience in musculoskeletal radiology , respectively ) blinded to clinical and surgical data . 
in order to assess the possible advantages of dect images over virtual standard cta images , the readers 1 and 2 reviewed the virtual - blended 120 - kv cta images first . 
an additional reading session was performed by the readers 1 and 2 for the calculation of intra - observer agreement , with a 8 - week delay , in order to reduce recall bias . each dataset was assessed for superior labral anteriorposterior ( slap ) tears and anterior or posterior labral tears . 
slap tears that extended anteriorly or posteriorly were defined as slap tears and not anterior or posterior labral tears [ 8 ]  . labral lesions were diagnosed in case of partial - thickness tears ( represented by the visualization of a partial defect of the labrum , enhanced by the passage of contrast material , or by the presence of abnormal morphology or partial dislocation ) , and in case of full - thickness tears ( represented by the visualization of a complete defect of the labrum or its absence ) , and in case of detachment of labrum from its usual location [ 23 ]  . labral fraying , which may correlate with a degenerative process , was scored as negative [ 24 ]  . a binary classification was used ( 0 , no labral tear ; 1 , presence of labral tears ) , without grading or subclassifying the lesions . 
an arthroscopic approach was adopted in 44 patients , whereas in three cases , an open approach was needed . statistical analysis the distribution of continuous variables was reported as mean and range ( minimum to maximum values )  . 
categorical variables were presented as numbers and percentages . 1 3 42 la radiologia medica ( 2020 ) 125 : 3947 data were analyzed with the receiver operating characteristic ( roc ) method and 95% confidence intervals ( cis )  . 
the sensitivity , specificity , positive predictive values ( ppv ) , negative predictive values ( npv ) , and accuracy ( acc ) for all types of labral tears were calculated for each dataset analyzed . 
the degree of agreement was categorized as follows : a k value of less than 0 indicated poor agreement ; a k value of 00.20 , slight agreement ; a k value of 0.210.40 , fair agreement ; a k value of 0.410.60 , moderate agreement ; a k value of 0.610.80 , substantial agreement ; and a k value of 0.811.0 , near - perfect agreement . additional non - labral findings , including rotator cuff or capsular tears , were recorded both for cta and mra . 
we had no case of extravasation or insufficient articular cavity distension . table 2 clinical data of patients enrolled parameter age ( years ) a age of male ( years ) = n 28a age of female ( years ) = n 19a mean interval surgery range interval labral tears anterior superior posterior associated findings rotator cuff tears hagl posterior impingement slap + sst partial tear previous surgery re - tears metal - induced artifacts value 34 . 
eleven of 47 patients had previous surgery ( with 8 / 11 diagnosed with a re - tear )  . a total of 11 additional non - labral findings were detected at surgery in 11 / 47 ( % ) patients . 
in particular , among the nine patients without labral tears , the following surgical diagnoses were obtained : rotator cuff tears ( n = 5 ) ; hagl ( n = 2 ) ; posterior capsular impingement ( n = 2 )  . 
the remaining two patients presented at surgery slap and a partial tear of sovraspinatus tendon ( sst )  . the diagnostic accuracy values obtained by readers 1 , 2 , and 3 in diagnosing labral tears are described in table3 . 
all cta and decta allowed us to sufficiently reduce or remove the metal artifacts , whereas 9 / 11 mra examinations ( 81.8% ) suffered from significant metal - induced artifacts . 
on the axial tse t1 - weighted mr image ( c ) , the presence of metal - induced artifacts does not allow to correctly evaluate the anterior aspect of labrum ( dotted arrow )  . 
on the corresponding axial reconstructed de - cta image ( d ) , thanks to the absence of artifacts , the involvement of anterior labrum can be clearly depicted ( dotted arrow ) fig . 
on the corresponding reconstructed axial dect map ( c ) , some mild bone marrow edema is coded on the anterior aspect of glenoid as an area or slightly increased density ( red arrow )  . 
cartilage and labrum , coded in blue on this map , are not visualized on the anterior aspect of glenoid 1 3 44 la radiologia medica ( 2020 ) 125 : 3947 fig . 
the reader 1 correctly identified 9 / 11 additional findings , missing a case of posterior impingement and a partial rotator cuff tear , whereas the reader 2 correctly identified 9 / 11 additional findings , missing a case of posterior impingement and a case of hagl . discussion in this paper , we compared the diagnostic capabilities of mra , de - cta , and standard virtual - blended 120kv cta images of the shoulder in diagnosing labral lesions , using surgery as the reference standard . 
a nonsignificant increase in diagnostic accuracy in the assessment of glenoid labral tears was achieved by analyzing de - cta dataset compared with mra and standard virtual - blended 120kv images . in the study by acid etal . 
also cta did better than mra in detecting anterior labral periosteal sleeve avulsion lesions , showing a better agreement with surgery ( = 0.89 ) than mra ( = 0.74 ) [ 26 ]  . in the paper by omoumi etal . 
although three - dimensional isotropic sequences have been successfully used in clinical practice to increase the accuracy of mra dataset in the shoulder and in the hip [ 6 , 24 , 25 , 27 ] , isotropic mr images remain prone to artifacts . 
for example , the isotropic vibe pulse sequences used in our dataset , with an acquisition time of at least 4min , could be inadequate because of motion artifacts that are virtually absent on a cta scan . 
conversely , the artifacts were well controlled on cta , allowing us to correctly classify the presence versus absence of labral tears in ten of eleven cases for reader 1 and in all cases for reader 2 . when comparing de - cta to cta dataset ( virtualblended 120kv images ) , only a little increase in diagnostic accuracy was obtained by both readers . 
it must be underlined that this increase in diagnostic accuracy was mainly due to an increase in sensitivity , with two additional tears detected for reader 1 , and three additional tears detected for reader 2 . 
the use of different lookup tables , coding the contrast material injected in different colors , may help in doubtful cases in confirming the presence of contrast material within a tear or ruling out the presence of calcifications . 
moreover , monoenergetic plus application , allowing to adjust the kv values to enhance or even decrease the brightness of intra - articular contrast material according to radiologist choice , was employed in selected cases . 
however , in our study , the majority of previously operated patients underwent relatively conservative surgical procedures , performed using small anchors , and the artifacts were adequately controlled on standard cta images as well . 
for this reason , the possible impact of metal - induced artifacts reduction , allowed by dedicated dect application ( by using the best kv values ) , could not been investigated . conversely , as a consequence of its high contrast resolution , mra was superior to cta and de - cta in the assessment of non - labral findings , with 10 / 11 findings correctly diagnosed . 
however , in a highly selected population , when a labral tear is suspected , these results may 1 3 46 la radiologia medica ( 2020 ) 125 : 3947 not impact significantly on patient management . 
in particular , the main advantage of mra over cta could be represented by the possibility to correctly identify rotator cuff intra - substance tears and partial bursal - sided tears . 
 ( a posterior capsule impingement and a partial bursal - sided sst tear were missed , respectively . ) although not sufficient for a detailed analysis , these data show that in clinical practice , an additional imaging study could be necessary only in few selected cases . 
a combination of standard mri of the shoulder for the evaluation of bursal - sided rotator cuff tears and cta for the evaluation of glenoid labrum and articular - sided tears could represent a possible approach . 
in addition , in our experience , many patients are referred for cta before surgery , after performing an inconclusive standard mri of the shoulder . although the mean radiation dose for shoulder de - cta is usually relatively limited , and on average inferior to that of a standard non - contrast shoulder ct at our institution , the problem of radiation exposure should be underlined . 
 for this reason , in clinical practice , we habitually perform mra for the evaluation of young patients or when seriate control studies could be needed , in order to avoid radiation exposure . this study has some limitations . 
first , all the enrolled patients were sent by orthopedic surgeons with a concrete suspect of labral tear and subsequently received surgery , possibly introducing a selection bias with respect to patient population . 
other imaging findings including bony bankart and hillsachs lesions and articular cartilage defects were not considered in our statistical analysis , even though they were relatively uncommon in our study population . in conclusion , de - cta and mra were not different in terms of diagnostic performance in our study . 
however , thanks to its high spatial resolution and to the possibility of reducing metal - induced artifacts , a nonsignificant increase in diagnostic accuracy in diagnosing labral tears was obtained by using cta in comparison with mra . 
pc should be considered in the differential diagnosis of pulmonary nodules / masses . keywords pulmonary cryptococcosis immunology computed tomography introduction pulmonary cryptococcosis ( pc ) is a fungal infection that occurs after inhalation of cryptococcus neoformans or cryptococcus gattii spores [ 1 ]  . 
pc is not a rare infectious disease in patients with impaired immunity , such as those with hiv infection and * wei song cjr.songwei@vip.163.com 1 department ofradiology , peking union medical college hospital ( east ) , chinese academy ofmedical sciences , shuaifuyuan wangfujing dongcheng district no . 
1 , beijing100730 , china 2 department ofepidemiology andbiostatistics , institute ofbasic medical science , chinese academy ofmedical sciences andschool ofbasic medicine , peking union medical college , beijing , china solid organ transplant recipients [ 2 ]  . 
also , reports of pc and its incidence in immunocompetent patients have increased in recent years [ 4 ]  . although the radiographic manifestations of pc are documented , those studies mostly focused on immunocompromised patients or small samples of immunocompetent patients [ 48 ]  . 
so far , we have identified only one study that dealt with thin - section ct characteristics of pc in 22 non - aids patients ( 13 immunocompetent and 9 immunocompromised patients ) [ 4 ]  . 
patient consent was waived because the investigation and management were part of the routine patient care , and it was a retrospective study of anonymized images and clinical data . a definite diagnosis of cryptococcosis was made if the patient met at least one of the following conditions : ( 1 ) positive histopathology from tissue samples acquired by open lung biopsy , percutaneous lung biopsy or transbronchial biopsy ; and ( 2 ) positive culture of cryptococcus from cerebrospinal fluid or blood . 
probable diagnostic criteria were : patients with a positive cryptococcal capsular polysaccharide antigen test in cerebrospinal fluid or serum and patients who presented with typical clinical manifestations [ 9 , 10 ]  . 
patients in whom other pathogens were isolated from the lungs were excluded . ct scanning chest ct was performed using a somatom definition flash scanner ( siemens healthcare , germany )  . 
in all of the patients , the ct scan was obtained 110days before diagnosis of pc . two radiologists ( xs and ws with 8 and 25 years experience , respectively , interpreting chest ct ) independently evaluated the ct images and were blinded to the clinical information for nodules , masses , ground - glass opacity ( ggo ) , consolidation , number ( single or multiple ) and distribution ( central , peripheral or random ) of lesions , cavitations and air bronchograms , halo sign , reticular opacity , bronchial wall thickening , lymphadenopathy and pleural effusion . 
nodules were 3cm in maximum diameter and masses were > 3cggo was identified as a lesion with the hazy increased attenuation of the lung , but with preservation of bronchial and vascular margins . 
peripheral distribution was considered to be the abnormalities that were mostly located in the outer third of the lung , and central distribution was considered to be the abnormalities located in the inner third of the lung . statistical analysis different patterns of ct findings between immunocompetent and non - aids immunocompromised patients were compared by fishers exact test . 
in the immunocompetent patients , only three patients with history of breeding pigeons were diagnosed with pc primitively ; the initial diagnosis was lung cancer in nine patients ; the initial diagnosis was benign or infectious lesions in six . 
after 4 months , the followup ct scan shows interval resolution of the previous consolidations , leaving residual parenchymal fibroses ( b ) comparing ct characteristics betweenthetwo groups comparison of ct abnormalities between immunocompetent and non - aids immunocompromised patients is summarized in table 2 . 
 follow - up interval for ct performed after antifungal therapy ranged from 2weeks to 12months in 37 patients ( 12 patients underwent surgical resection and 25 did not )  . 
after 6months , the follow - up ct image shows interval improvement of the previous lesions ( b ) table 2 comparison of ct characteristics of immunocompetent and non - aids immunocompromised patients discussion features immunocompetent patients immunocompromised patients nodules masses consolidation well - defined ill - defined tree - in - bud with air bronchogram with cavitation with halo sign reticular opacity ground - glass opacity associated findings lymphadenopathy pleural effusion lesion distribution solitary multiple unilateral bilateral peripheral central location random distribution the ct findings showed improvement during 16months follow - up . 
the main observations were that nodules were the most common ct finding , and multiple nodules / masses and cavities were more frequent in immunocompromised than in immunocompetent patients . some previous studies showed that pc was more frequent in men than women [ 4 ]  . 
pc had a variety of clinical presentations , from asymptomatic ( seven of 42 patients ) to mild or acute infection , chest pain , shortness of breath , cough with sputum and fever , as in previous studies [ 7 ]  . 
in the present study , cough and fever were the most frequent symptoms for the immunocompromised group , and cough was the most frequent for the immunocompetent group , which was in agreement with previous studies [ 10 ]  . 
pc clinical presentation is nonspecific and should be differentiated from tuberculosis , lung cancer and other respiratory conditions . although the ct characteristics of pc have been well described , only a few studies have focused on ct findings of non - aids patients thus far [ 2 , 4 , 7 ]  . 
 our results concur with previous ct studies [ 2 , 3 , 7 , 8 , 11 , 12 ] ( table3 ) , in which multiple nodules / masses were the most common pattern of pc . 
but in their study , only one 1 3 36 la radiologia medica ( 2020 ) 125 : 3138 nodules or masses consolidation lymph nodes multiple lesions cavitation location table 3 ct feature of pc in previous study author ( reference ) immune system wei - chou etal . 
 [ 12 ] 26 immunocompetent patients 12 immunocompetent and 11 non - aids immunocompromised patients patients 18 immunocompetent and 24 immunocompromised patients no mention peripheral predominance no prediction lower lobe and peripheral predominance peripheral predominance peripheral predominance middle and upper lobe predominance the left lower lobe peripheral predominance this study peripheral predominance immunocompetent patients were included . 
we found that nodules / masses were mostly ill - defined ( 78.6% ) , and cavities were described in 33.3% of all patients , which was similar to previous studies [ 3 , 7 , 12 ]  . 
 [ 3 ] showed that the incidence of air bronchograms was higher in non - aids immunocompromised than immunocompetent patients , whereas we found no difference in the incidence of air bronchograms between our two groups . 
most of the lung abnormalities of pc in our study were without calcification , with no diffused miliary nodules and with only a few cases of lymphadenopathy and pleural effusion , resulting in only two cases being misdiagnosed as tuberculosis . 
however , some nodules 1 3 la radiologia medica ( 2020 ) 125 : 3138 and masses were ill - defined or eccentric with irregularly thick - walled cavities , resulting in misdiagnosis of malignancy . 
pulmonary metastasis could not be excluded in three patients with malignant tumors because of the presence of pulmonary nodules with ill - defined margins ( one solitary nodule and two patients with multiple nodules )  . 
thus , pc should be taken into consideration even in patients with a history of malignancy , and histopathological diagnosis should be performed for tissue confirmation . ct characteristics suggestion of lung cancer can be found coincidentally in benign conditions , such as pulmonary infection . 
therefore , a history of breeding pigeons can provide a diagnostic clue for pc . of the 25 patients who had follow - up ct scans and did not undergo surgical resection , 23 showed slow progression or no change in their pulmonary lesions , and only two patients showed complete clearance of their lesions . 
the unavailability of histological specimens for all patients limited the pathologicalradiological correlation . in conclusion , the most common thin - section ct feature of pc was pulmonary nodules / masses , which were ill - defined and located peripherally . 
receiver operating characteristic analysis was performed . results the li - rads scale obtained an accuracy of 80% , a sensitivity of 72% , a specificity of 93% , a positive predictive value ( ppv ) of 93% and a negative predictive value ( npv ) of 70% , while the likert scale achieved an accuracy of 79% , a sensitivity of 73% , a specificity of 87% , a ppv of 89% and a npv of 70% . 
the inter - observer agreement was strong ( k = 0.89 ) between the li - rads evaluators and moderate ( k = 0.69 ) between the likert evaluators . conclusions there was no statistically significant difference between the performances of the two scales ; nevertheless , we suggest that the li - rads scale be used , as it appeared more objective and consistent . keywords liver cirrhosis carcinoma , hepatocellular magnetic resonance imaging early detection of cancer data interpretation , statistical * andrea esposito andrea.esposito@policlinico.mi.it 1 division ofradiology , foundation irccs ca granda maggiore policlinico hospital , via f.sforza 35 , milan , italy 2 division ofradiology , santandrea hospital , corso m . 
celoria 18 , milan , italy 5 departement ofspecialty andtransplant medicine , gastroenterology , hepatology andtransplant unit , papa giovanni xxiii hospital , piazza oms 1 , bergamo , italy 6 division ofradiology , abano terme policlinico hospital , piazza c . 
in most of africa and asia , hbv is the single leading risk factor for hcc , whereas in japan , northern europe and the usa , hcv is the major risk factor [ 5 ]  . in 8090% of cases , hcc occurs in the setting of cirrhosis [ 6 ]  . 
however , a stepwise progression of hepatocarcinogenesis has been established [ 7 ] , so when a hepatocellular nodule is detected , monitoring is recommended , in order to diagnose premalignant nodules and early hcc , when effective therapy can be applied . periodic serologic and imaging tests for patients known to be affected by chronic liver diseases are recommended and widely implemented in current clinical practice . 
however , the optimal surveillance interval and surveillance tools for hcc have not yet been standardized [ 8 ]  . ct and mr are the imaging techniques that often allow making a definite diagnosis of hcc without a need to biopsy the lesion . 
hcc is the only tumor that can be diagnosed with imaging alone , without the need for histopathological confirmation [ 9 ]  . mri has been proposed as a sensitive ( 81% ) and specific ( 85% ) imaging modality for the evaluation of liver nodules in patients with cirrhosis [ 10 , 11 ]  . this is based on the unique properties of mr imaging resulting in a high intrinsic soft tissue contrast between normal liver parenchyma and liver lesions , which can be further enhanced with intravenous administration of non - specific ( extracellular ) and liver - specific ( hepatobiliary ) gadoliniumbased contrast agents [ 12 ]  . several scientific organizations and societies have proposed diagnostic systems for the interpretation of liver examination , in order to reduce imaging interpretation variability and improve communication with clinicians [ 13 ]  . since march 2011 , the liver imaging reporting and data system ( li - rads ) scale has been adopted by many clinical practices [ 14 ]  . 
the first version of the li - rads was launched in march 2011 , an update was released in 2013 and 2014 [ 14 ] , and the latest update was released in 2018 [ 15 ]  . a different scale of diagnostic interpretation , adopted in many fields of research , is the likert one [ 17 , 18 ]  . 
our purpose was to compare the performance of readers using a li - rads scale with that of readers using a likert scale , in a cohort of patients with chronic liver disease who had undergone mri for the discovery of a nodule in the sonography examination , using the histopathologic results from biopsy / liver transplant or an mri follow - up over 4years as reference standards . materials andmethods patients this retrospective study was approved by our institutional review board . 
we reviewed patients with cirrhosis , with no history of previous hcc , who underwent a mr examination , between february 2006 and march 2012 , for the presence of new nodules , discovered with sonography . 
we identified 39 patients ( m / f : 24 / 15 ; mean age of 73.1years ; and age range of 5491years ) with a total of 44 lesions . for each patient , we registered the following data : age , date of the mr examination , number of nodules , segmental location of nodules , nodule size , radiologist evaluation for each nodule and the definitive diagnosis . 
this diagnosis was expressed as 0 to indicate non - evidence of hcc and as 1 for histological confirmation of hcc . mri technique all mr examinations were performed on a 1.5 - t system ( avanto ; siemens medical systems , erlangen , germany ) using a phased - array coil for signal detection . 
t1 - weighted imaging included a breath - hold in - phase gradient echo sequence ( 175 / 5 tr / te , 256 112 matrix , 70 flip angle ) and an out - of - phase gradient echo sequence ( 175 / 2.38 tr / te , 256 112 matrix , 70 flip angle )  . 
t2 - weighted imaging included non - fat - suppressed ( 3945 / 66 tr / te , 320 195 matrix ) and fat - suppressed sequences ( 4185 / 53 tr / te , 320 184 matrix )  . 
gadolinium ( gadobenate dimeglumine ; multihance , bracco , milan , italy ) was injected at a dose of 0.2mmol / kg at a rate of 2ml / second , followed by 0.2ml / kg of normal saline flush , with a second syringe ( medradstellant , bayer , germany ) at the same injection rate . 
a breath - hold in - phase and out - ofphase t1 - weighted sequence ( 175 / 2.3 tr / te , 256 134 matrix ) and a t1 three - dimensional volumetric breath - hold sequence were performed 2h after contrast injection ( hepatocyte phase )  . image interpretation mri studies were analyzed independently by two radiologists with , respectively , 10 and 20years of experience in liver mri , and they were independently analyzed by two radiologists with , respectively , 1 and 3months of experience in liver mri , using synapse ( pacs , fujifilm medical systems , japan )  . 
two of these radiologists , with 1month ( iradiolir ) and 10years ( eradiolir ) of experience , evaluated the lesions using the li - rads scale v.2018 , while the other two , respectively , with 3months ( iradiolik ) and 20years ( eradiolik ) of experience in liver mri , evaluated the lesions using the likert scale ( scores 15 )  . 
at mri follow - up , a lesion was considered benign when it showed stable or reduced diameters . statistical analysis before choosing the optimal scale and score for hcc detection , the evaluation of inter - reader agreement was performed by computing linear weighted k coefficients and pearson correlation coefficients . 
the k coefficient was interpreted as an indication of poor agreement when k was 0.40 or lower , as an indication of moderate / substantial agreement when k coefficient was higher than 0.40 and lower than 0.80 and as an indication of strong agreement when k coefficient was greater than 0.80. 
pearson correlation coefficients were also employed to evaluate the inter - reader agreement and to confirm the results obtained by the k coefficient : values lower or equal to 0.30 were an indication of poor agreement , values higher than 0.30 and lower or equal to 0.70 indicated moderate agreement , and values higher than 0.70 were evidence of strong inter - reader agreement . both for the li - rads v.2018 and likert scales , receiver operating characteristic ( roc ) curve analysis was performed to identify , for each evaluator , the optimal score for hcc detection , defined as the score that maximized the evaluator accuracy ( acc )  . 
evaluations from each scale were classified as positive for hcc if the evaluation was equal to or higher than the derived optimal score ; otherwise , they were classified as negative for hcc . 
with this aim , a logistic regression model ( using the scoresfrom 1 to 5of each evaluator as independent variable and the scores of the gold standard0 or 1as dependent variable ) was used in each case to derive the probability of each lesion being hcc ; fitted data were used to compute roc curves . 
furthermore , for both the li - rads and likert scales , the scores from the two readers were pooled to derive a single optimal score between evaluators using the same scale . 
to simulate the use of pooled data , for each scale we employed a multiple regression model fitted to the scores of both radiologists as independent variable and the scores of 1 3 18 la radiologia medica ( 2020 ) 125 : 1523 the gold standard as dependent variable . 
the z test for the difference between two proportions was applied to check the statistically significant difference among the performance ratios , achieved by the readers of the same scale . 
the statistical analysis software was coded in matlab . results since five patients had two lesions to characterize , we evaluated a total of 44 lesions , 26 hcc and 18 non - hcc . using the li - rads scale , 34 lesions ( 19 hcc + 15 non - hcc = 77.27% of all the 44 lesions ) obtained the same score . 
the k coefficient between the two evaluators of lirads scale was 0.89 , while the estimated pearson correlation coefficient equaled 0.90. using the likert scale , 22 lesions ( 11 hcc + 11 nonhcc = 50% of all lesions ) were classified with equal scores . 
the k coefficient and the pearson correlation coefficient computed to evaluate the likert scale inter - reader variability were much lower than those computed for the li - rads scale ; they equaled , respectively , k = 0.69 and pearson = 0.63. the roc curves computed to assess reader performance for hcc detection ( fig.1 ) had the following area under the curves ( aucs ) : using the li - rads scale , the aucs were 0.87 ( eradiolir ) , 0.75 ( iradiolir ) , 0.91 ( pooled data ) ; using the likert scale , the aucs were 0.79 ( eradiolik ) , 0.83 ( iradiolik ) , 0.87 ( pooled data )  . when pooled data were not considered , roc analysis showed that the optimal threshold criterion , which allowed maximizing both the accuracy as well as the average of sensitivity ( sens ) and specificity ( spec ) in the detection of hcc , was a score of 4 or higher for all the evaluators , using either the li - rads or the likert scale . 
1 roc curves for each evaluator and for pooled data both for the li - rads and likert scale 1 3 la radiologia medica ( 2020 ) 125 : 1523 score , we calculated accuracy ( acc ) , sensitivity ( sens ) , specificity ( spec ) , positive predictive value ( ppv ) and negative predictive value ( npv ) ( table1 )  . at the optimal score , all the evaluators and pooled data achieved also the maximum average of sens and spec . for both the scales , the reader performance improved when a cooperative diagnostic procedure was simulated by employing pooled data . 
specifically , for the li - rads and likert scales , the optimal pooled scores , which are composed by eradio and iradio scores , were , respectively , equal to ( 3 , 2 ) and ( 2 , 4 ) ( table1 )  . to compare the two scales in terms of the achieved radiologist performances , for each scale the mean of the performance values ( acc , sens , spec , ppv and npv at the optimal scores , auc ) achieved by the two radiologists and the pooled data were computed . the computed averages were similar , and the z test did not find any statistically significant difference between thefor the li - rads scale , we obtained : acc = 0.80 , sens = 0.72 , spec = 0.93 , ppv = 0.93 , npv = 0.70 , auc = 0.85 ; for the likert scale , the results were : acc = 0.79 , sens = 0.73 , spec = 0.87 , ppv = 0.89 , npv = 0.70 , auc = 0.83. the comparability of the achieved results suggests that neither scale is guaranteed to achieve a better performance than the other . discussion mr is a noninvasive diagnostic modality with a high sensitivity ( 81% ) and specificity ( 85% ) for the detection and evaluation of liver nodules in patients with high risk of hcc [ 10 ]  . 
these characteristics make mri relevant for the management of patients with suspicion of hcc , mostly for the detection of early hcc , usually composed of well - differentiated hepatocytes [ 22 ] , thereby avoiding more invasive examinations such as fine - needle biopsy ( fnb ) samples [ 9 , 21 ]  . however , these results are influenced by the experience of the radiologists who examine the images and some clinicians complain of the lack of standardization in reporting liver mri nodules . in an effort to improve consistency of interpretations among radiologists , the introduction of a standardized scheme with fixed criteria , already applied for other organs such as breast , thyroid and prostate , has also been proposed for the liver . the li - rads scale was created to standardize the reporting and data collected in patients with cirrhosis or other risk factors for developing hcc , both with ct and mri , stratifying the risk of malignancy of a nodule with a scale of scores 15 ( lr 1 - lr 5 ) [ 1316 ]  . 
in particular , a nodular arterial phase hyper - enhancement is a very important feature , as , if equal or superior to 2cm or if in association with at least one of these three major features : the presence of nonperipheral washout , the presence of an enhancing capsule or a threshold growth , is to be considered either probably hcc ( lr 4 ) or definitely hcc ( lr 5 ) [ 15 , 16 , 23 ]  . the likert scale is a quicker and easier method , based on an analysis of items . 
in our study , we used five items ( scores 15 ) to express a positive or a negative opinion to delineate the probability of a liver nodule to be hcc , based on dynamic enhancement and other features such as corona enhancement , capsule appearance and threshold growth [ 13 ]  . to study the performance of the li - rads scale , we compared the diagnostic performance of readers using the latest version of the li - rads scale , updated in 2018 , with that of readers using the likert system . with this aim , gastroenterologists gave us a homogeneous cohort of patients with chronic liver disease . 
they selected only patients with no previous hcc , with the first discovery of a nodule in the sonography examination , successively studied with mri . in both scales , radiologists performed well and accuracy was high . visual analysis of the roc curves computed to assess reader performances for hcc would suggest that the lirads scale provides the better performance values , since the mean auc achieved by readers employing the li - rads scale equals 0.85 , while the one achieved by readers employing the likert scale is 0.83. 
moreover , pooling data of readers employing the li - rads scale obtains auc = 0.91 , while the auc achieved by evaluations made by pooled data of likert scale equals 0.87. a similar study was completed by zhan etal . 
 [ 24 ] , using an earlier li - rads version ( v2014 )  . these authors obtained substantial variations in liver observations between reporting by the li - rads and likert methods . 
 [ 27 ] demonstrated that li - rads v2014 lr - 5 on gadoxetate disodium - enhanced mri exhibited an excellent ppv for the diagnosis of hcc in patients with chronic liver disease and for some authors , it should be incorporated into li - rads as a major feature [ 9 , 28 , 29 ]  . evaluating readers using the same scale , both for lirads v.2018 and likert scale , we found that the differences between the sens , spec and npv values were statistically significant , but when we compared the performance achieved by employing different scales , we did not find any statistically significant difference between the aforementioned average performances , as obtained by barth etal . 
 [ 31 ] , the li - rads scale produces strong reliability and validity , while aiming to a primary goal and motivation for the development of the li - rads scale is to reduce the inter - reader variability . clinicians have expressed serious concern over the inconsistency in liver lesion reporting among radiologists owing to the readers experience level , differences in interpretation as well as differing personal preferences [ 32 ]  . in our study , the li - rads scale has demonstrated the potential to reduce inter - reader variability and to enhance the communication with referring clinicians , as also observed by other authors [ 33 ]  . there are several limitations in our study . 
second , the radiologists are from the same hospital and may have similar perspectives in terms of interpretation , and third , the experience of the radiologists involved in the study varied greatly . 
finally , as a contrast medium , for the evaluation of wash - in and washout and the hepatobiliary phase , we used only gadobenate dimeglumine and not gadoxetate disodium . conclusions according to our results , there was not a statistically significant difference between li - rads v.2018 scale and likert scale in the evaluation of liver nodules and detection of hcc ; nevertheless , we suggest the use of li - rads v.2018 scale , because it appears more objective and consistent . our results reached the goal of li - rads which is to improve the consistency of radiology reports in imaging of high - risk patients for hcc . additional studies are warranted to evaluate the performance of these scales across radiologists from different institutions with different levels of experience . funding this study did not receive any funding . 1 3 22 la radiologia medica ( 2020 ) 125 : 1523 compliance with ethical standards conflict of interest all the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with animals performed by any of the authors . 
based on bone mineral density ( bmd ) measurements obtained from dexa , the vertebrae were divided into three groups as follows : normal ( n = 52 ) , osteopenic ( n = 92 ) , and osteoporotic ( n = 36 )  . 
if not treated correctly , these fractures are associated with high mortality and morbidity [ 4 ]  . presently , osteoporosis is diagnosed primarily by determination of bone mineral density ( bmd ) [ 1 , 3 , 5 ]  . 
although dexa is noninvasive and cost - effective , it has a low sensitivity rate [ 4 , 6 ]  . recent evidence has shown that an increase in bone marrow fat is related to a reduction in bone marrow density [ 1 ]  . 
numerous studies have reported that the bone marrow density decreases progressively with age , and fat cells replace the missing trabecular tissue and fill the bone marrow [ 5 ] .this increase in bone marrow fat can be used as an index of lost bone trabecular tissue [ 1 ]  . furthermore , increased bone marrow fat levels can lead to errors in dexa assessments and t - score evaluations [ 9 ]  . 
one such method is diffusion - weighted imaging ( dwi ) mri , which has been recently proposed due to its high diagnostic value [ 1 ]  . the high spatial resolution and excellent soft tissue contrast provided by mri make it a powerful method to determine the amount of fat in the bone marrow and monitor bone marrow alterations in normal and pathologic conditions [ 10 , 11 ]  . 
newer techniques in mri , such as dwi , allow noninvasive radiation - free evaluations that can replace or complement dexa in quantitative and qualitative bone marrow assessments [ 1 , 5 ]  . 
dwi measures the random water molecule movements in a biological tissue , allowing assessment of the microstructure and diffusivity of the tissue [ 7 , 12 ]  . limited studies about the correlation between diffusivity and bmd in vertebral bones with various bone marrow density levels have been performed and have yielded conflicting results [ 14 , 7 , 8 , 1215 ]  . 
since lumbar mri is frequently requested , lumbar mr examinations performed due to other indications can also be used as a complementary method for bone marrow density assessment . methods this was an analytical epidemiologic study on a population of menopausal women referred to the ahvaz golestan hospital . 
after receiving ethical and legal approval and patient consent , dexa assessments were performed for 60 women ( age > 50years ) with suspected osteoporosis on the basis of the rheumatologists recommendations . 
after obtaining informed consent , we excluded patients with malignant tumors , hematologic and bone disorders such as metastasis or severe osteoarthritis , vertebral body fractures , patients with metallic devices in their body , and those who used medications that influence bone marrow physiology . 
dxa scans are used to quantify bone mass that is expressed in standard deviations from the normal 1 3 70 la radiologia medica ( 2020 ) 125 : 6874 fig . 
the roi ( region of interest ) resonance imaging was put on the anterior and central part of the vertebra body and the adc value was calculated automatically mr imaging mri was performed right after dexa . 
dwi was performed on lumbar vertebra with these parameters : spin - echo single - shot echo - planar imaging sequence ( tr : 1300ms , te : 80ms , inversion time : 180 ms , nex : 6 , b - values , 0 , 600 , and 1000mm2 / s , slice thickness = 5mm , field of view : 150mm , matrix : 128 93 )  . 
the roi ( region of interest ) was put on the anterior and central part of the vertebra body and the adc value was calculated automatically . analysis spss version 22 was used . 
the accuracy , sensitivity , specificity , positive predictive value ( ppv ) , and negative predictive value ( npv ) of the dwi technique in the diagnosis of osteoporosis and osteopenia were calculated . results for the l2 to l4 vertebra of all patients , and the bmd and adc results are described in table1 . 
using this value , 12 cases in the normal group were diagnosed incorrectly ( false - negative ) and eight cases in the osteopenic group were incorrectly classified as normal ( false - positive )  . 
4 the receiver operating characteristic ( roc ) curve using quantitative adc as the test variable and the diagnosis osteoporosis based on dualenergy x - ray absorptiometry ( dxa ) as the state variable . 
the area under the curve was 0.912 , indicating that mri had very high ability to diagnose osteoporosis ( p = 0.001 ; az = 0.912 ) method were confirmed . 
 [ 1 ] at 2015 studied l3 vertebra and concluded that adc values of the bone marrow ( in 106 mm2 / s ) in the osteoporotic group ( 338 70 ) and the osteopenic group ( 408 68 ) are significantly lower than those in the 1 3 72 la radiologia medica ( 2020 ) 125 : 6874 normal group ( 464 60 )  . 
they found a meaningful difference in bmd levels among the osteopenic ( 0.740.99g / cm2 ) , osteoporotic ( 0.440.84 g / cm2 ) , and normal ( 0.941.19g / cm2 ) groups . 
this difference could be due to the low sampling volume ( 16 persons ) and the absence of a steady bmd distribution ( no case in the osteopenic group )  . 
these results are in agreement with the results from our current study . histomorphometric and mr spectroscopic studies indicate that the relationship between adc and bmd can be attributable to bone marrow fat . 
with increasing age , the levels of fat in the bone marrow composition would increase , osteoclast activity would increase , and osteoblast activity would decrease , leading to osteoporosis [ 13 ]  . 
reported that using bone marrow fat as a new diagnostic index , and this method is as precise as bmd in osteoporosis diagnosis the bone marrow fat / bmd ratio is a significant diagnostic indicator of bone weakening [ 21 ]  . 
these findings suggest that bone marrow fat is an important factor in osteoporosis . other studies using histomorphometry and mr spectroscopy have suggested that an increase in bone marrow fat leads to a decrease in diffusion capability and adc values [ 1 , 2 , 7 , 22 , 23 ]  . 
however , they found no meaningful difference in diffusion restriction among the normal , osteopenic , and osteoporotic vertebra and no correlation between adc and bmd , which is probably due to the perfusion effect and dwi settings . normally , the adc value is not only affected by cellularity , but also by other factors such as the perfusion effect . 
thus , an active hematopoietic bone marrow ( cellular bone marrow ) has more intracellular and free extracellular water in comparison to the less active bone marrow [ 13 ]  . 
furthermore , the perfusion effect seems to be more significant at low b - values , and one of the limitations during evaluation of osteoporosis is b - value selection . 
 however , the current study and other similar studies suggest that dwi and adc values have high diagnostic capability in osteoporosis . our current study had some limitations such as a low sample volume even though we assessed more cases than other previous studies . 
although we used 3 b - values for more accurate results , better device setting could be possible . conclusion this study revealed that dwi sequence and adc values have a significant correlation with bmd and that they show meaningful differences in normal , osteopenic , and osteoporotic vertebra . 
furthermore , this technique is comparable with dexa , which is the 1 3 la radiologia medica ( 2020 ) 125 : 6874 gold standard of osteoporosis diagnosis , but does not involve any x - ray - related damage . authors contributions study conception and design : ma , mm , km , mmg , mgh . 
to retrospectively evaluate technical and clinical outcomes of the adapt as first - line treatment for anterior circulation acute ischemic stroke with large - bore reperfusion catheters . methods a multicentric data collection from 14 medical centers was retrospectively analyzed . 
baseline characteristics , technical and clinical variables were collected , including nihss , thrombolysis in cerebral infarction ( tici ) , peri - procedural complications , 90 - day mrs and 90 - day mortality . results overall , 501 patients were treated . 
several randomized stroke clinical trials [ 15 ] demonstrated the superiority of mechanical thrombectomy ( mt ) from large vessel occlusion when compared with the standard intravenous thrombolysis alone in patients with acute stroke . 
compared with other endovascular approaches , the technique of a direct aspiration first pass technique for the endovascular treatment of stroke ( adapt ) vol . : ( 0123456789 ) 1 3 58 la radiologia medica ( 2020 ) 125 : 5765 for acute ischemic stroke has obtained growing acceptance as it is thought to facilitate a high rate of recanalization , and potentially at lower costs when used either alone or as an adjunct to stent retriever , and promising clinical results , especially when used in intracranial large vessel occlusion [ 610 ]  . 
although no comparative studies demonstrated better efficacy of contact aspiration versus the validated sr technique , some authors suggest noninferiority or superiority of the adapt technique to achieve better reperfusion rates [ 14 , 15 ]  . the purpose of this multicentric study is to retrospectively assess revascularization efficacy , duration of the procedure and early and 90 - day clinical outcome of the adapt technique as first - line treatment for anterior circulation acute ischemic stroke with large - bore reperfusion catheters . materials andmethods patient selection from june 2016 to march 2018 , a multicentric data collection through the italian registry of thromboaspiration ( rita - 2 ) website was retrospectively analyzed to find all patients who received adapt from fourteen medical centers . 
inclusion criteria were age 18years , large artery occlusion in the anterior circulation , a time window < 8h , no intracerebral hemorrhage ( ich ) , presence of an existing or preexisting large territory infarction and aspects score 6 at baseline ct . all patients were evaluated by a stroke - dedicated neurologist and an interventional neuroradiologist before proceeding to diagnostic imaging . unenhanced ct was obtained in all patients to exclude hemorrhage and assess aspects score ; ct angiography ( cta ) was performed to detect large vessel occlusions . 
 informed consent was obtained from all individual participants included in the study . revascularization technique the adapt technique consisted of a large guide catheter advanced as distally as possible to reach the cervical or proximal petrous segment of the ica ; the aspiration catheter of caliber to fit in the vessel was selected for each case ( distal ica or proximal middle cerebral artery ) ; three different types of large aspiration catheters were used : ace 64 or 68 ( penumbra , alameda , california , usa ) , or sofia plus ( microvention , tustin , california , usa )  . 
the reperfusion catheter was advanced in front of the thrombus , coaxially over a microwire and a microcatheter , and then aspiration was applied either manually with a 60 - ml syringe or through a penumbra aspiration pump , depending on the operator experience . 
the choice of aspiration catheter and number of attempts was up to the primary operator . imaging andclinical assessment all digital subtraction angiography ( dsa ) were analyzed after the procedure , and the thrombolysis in cerebral infarction ( tici ) score was applied . 
the nih stroke scale ( nihss ) score at admission and discharge and the modified rankin scale ( mrs ) score after 90days of follow - up were assessed by the same stroke - dedicated neurologist . 
before treatment , informed consent was obtained from the patient ( if conscious ) or a legal representative . statistical analysis continuous parameters were compared between patients using the student t test for normally distributed data , the mannwhitney u test for non - normally or ordinal distributed data and the chi - square test ( with yates correction , if necessary ) for binomial data . 
1 acute left facio - brachial hemiparesis ( nihss = 19 ) in a 18 - year - old boy with unknown onset of symptoms and a misunderstood dilatative cardiomyopathy . 
the patient rapidly underwent mri , which revealed diffusion restriction involving the left frontoparietal lobe ( circle in d ) with no tissue abnormalities in flair sequence ( dwi - flair mismatch ) , where hyperintense vessel sign is visible ( arrowhead in e and f )  . 
the patient was considered eligible for endovascular therapy , and successful recanalization of the occluded left middle cerebral artery ( arrow in g ) was obtained after two attempts of thromboaspiration , achieving a tici score = 3 ( arrow in h )  . 
before evt , tpa administration was attempted in 53.1% of patients ( n = 266 / 501 )  . the median nihss score at baseline was 16 ( iqr : 1220 ; range 031 ) and 12.6% ( n = 63 / 501 ) of patients had a baseline nihss < 6 . 
2 wake - up stroke in a 40 - year - old woman with history of patent foramen ovale and acute right brachial hemiparesis and motor aphasia ( nihss = 9 )  . 
ct perfusion maps revealed mild reduction in cerebral blood volumecbv ( b ) and increased mean transit time mttin left mca territory , consistent with large penumbra tissue ( white arrow in c )  . 
the patient was considered eligible for endovascular therapy , and successful recanalization of the occluded left mca ( arrowhead in d ) was obtained after one attempt of thromboaspiration , achieving a tici score = 3 ( arrow in e )  . 
technical and clinical outcomes are summarized in table3 . discussion as already reported , among endovascular techniques for large vessel occlusions , adapt appears a feasible technique resulting in faster revascularization time and lower cost when used as first attempt in comparison with stent retriever technique [ 6 , 16 , 17 ]  . 
these guidelines come from trials based on the use of stent retriever as first choice in all cases ; it also reported that more studies should examine which systems provide the highest recanalization rates with the lowest risk for nontarget embolization [ 2 , 4 , 5 , 18 ]  . 
however , the latest european stroke organization guidelines found no evidence that contact aspiration alone could increase the rate of reperfusion over thrombectomy using a stent retriever [ 19 ]  . table 3 technical and clinical outcomes of all patients are described . 
adapt , or contact aspiration , involves the first - line use of aspiration through a large - bore catheter [ 20 ] then adding a stent retriever if necessary . about technical outcomes , in our multicentric study , adapt alone demonstrated to be successful in achieving revascularization of the occluded vessel with a tici 2b / 3 in 71.8% of patients , a mean ptr of 43min and a median aspiration attempts < 2 . 
these results are in accordance with the range of the landmark randomized control trials [ 2 , 4 , 5 , 18 ] and similar to the adapt arms in the aster [ 21 ] and compass [ 22 ] randomized controlled trials ; moreover , angiographic and clinical results of the aster ( successful recanalization in 85.4% in the contact aspiration vs 83.1% in the stent retriever group ) and compass trials ( 90 - day mrs 02 was achieved by 52% in the aspiration group and 50% in the stent retriever group ) , showing that aspiration as first pass was non - inferior to the stent retriever first - line approach [ 22 ]  . in our study , in the majority of cases ( 89.8% ) , only one aspiration attempt was required . 
these results are in accordance with other recent published article [ 6 , 23 , 24 ] , due to the concept that adapt should take less time to recanalize the target artery because a stent retriever must be passed through the clot . 
efficacy of adapt technique with ace 60 / 64 for large vessel occlusion in anterior circulation was also reported in a large study on 347 patients , showing that only two factors positively influenced success of the adapt : an isolated middle cerebral artery occlusion ( p < 0.001 ) and a shorter time from stroke onset to clot contact ( p = 0.018 ) [ 25 ]  . the aster randomized clinical trial [ 21 ] reported a significantly shorter time from clot contact to revascularization in the contact aspiration group . 
moreover , the compass [ 22 ] trial indicated that the time to tici 2b or greater was shorter in the adapt arm than in the stent retriever arm , with 22 versus 33min , respectively . in a study on 524 patients , anadani etal . 
 [ 26 ] demonstrated that first attempt recanalization ( far ) with ace 64 or 68 was associated with better functional outcome , lower mortality and hemorrhagic transformation rate also because time from onset to recanalization was significative shorter in the far group . 
nevertheless , a recent meta - analysis [ 27 ] , comparing first - line adapt versus first - line stent retriever , could not evaluate whether procedure time was significantly different between techniques , because most of the studies did not provide detailed statistical data of time to recanalization . 
in terms of tici 2b / 3 , our study demonstrated no statistical difference in distal inner diameter between ace 64 , ace 68 and sofia plus ( p < 0.001 ) , supporting the use of the larger - bore catheters in adapt when available . 
these rates of embolic complications are within the range of previous reports either invitro or on patients cohorts [ 25 , 32 ] , and we found statistically significant difference on behalf of the adapt one ( p = 0.0026 ) ; use of a stent retriever requires that it be passed through the clot and therefore might result in a higher rate of distal emboli [ 33 ] ; moreover , in our study this data may be also associated with the absence of a 1 3 la radiologia medica ( 2020 ) 125 : 5765 balloon guide catheter to arrest proximal flow . 
the estimated cost reduction ( a mean of $4541 about 4000compared with the stent retriever first - line group ) has the potential to substantially reduce the cost of thrombectomy procedures worldwide [ 22 ]  . 
moreover , a non - randomized data support the concept of a cost advantage for the aspiration first pass approach , demonstrating that adapt technique had a lower device - related cost than stent - assisted thrombectomy leading to an overall saving about 2700 [ 9 ]  . our study had several limitations : first , the retrospective design ; then , the lack of homogeneous patient selection and standardized ct technique . 
another limitation in our study is the fact that preoperative perfusion weighted imaging was not performed in all patients ; in fact , it has been shown that evaluating the extent of salvageable brain tissue and the degree of collateral blood supply may better stratify the population and identify patients who could preferentially benefit from evt [ 4 ]  . 
 given the lack of a standardized approach , our data cannot be compared in terms of outcome and procedure times with recent large randomized trials using stent retrievers as a first - line option . 
longterm follow - up and direct comparative studies are required to determine whether adapt approach can be a suitable alternative to stent retriever technique for acute ischemic stroke . conclusions for acute ischemic stroke due to anterior circulation large vessel occlusion , adapt is a valid technique with respect to the rates of tici 2b / 3 recanalization and 90 - day mrs scores . 
given the reduced procedural time and time to tici 2b / 3 recanalization with similar functional outcomes , an initial attempt at recanalization with adapt may be warranted prior to stentriever thrombectomy . 
in this letter to the editor , we would like to highlight the proper role of tus and its pitfalls . keywords ultrasound interstitial lung disease b - lines dear editor , we read with great interest the review by marwin gutierrez etal . 
the connective tissue diseases ( ctds ) related interstitial lung disease ( ild ) early diagnosis by transthoracic ultrasound ( tus ) , as the authors stated in the discussion , still arises several issues . ild is one of the pulmonary manifestations of ctds which can lead to significant morbidity and mortality . 
we completely agree with the authors conclusions , as they specify that additional studies are needed in order to consider tus as one of the screening imaging techniques for pulmonary fibrosis [ 1 ]  . the early detection and quantification of parenchymal abnormalities is crucial to improve the quality of life of patient affected by ctd and the related prognosis [ 1 ]  . 
 indeed , in the last few years , tus has gained a growing * elisabettamaria frongillo elisabettamaria.frongillo@gavazzeni.it 1 unit ofthoracic surgery , cliniche humanitas gavazzeni , via mauro gavazzeni , 21 , 24125bergamo , bg , italy 2 department ofrespiratory diseases , university ofbari , bari , italy 3 unit ofinterventional ultrasound ofinternal medicine , irccs fondazione casa sollievo della sofferenza , sangiovannirotondo , fg , italy 4 department ofmedical science , chieti - pescara university , chieti , italy interest among both clinicians and radiologist as a useful , noninvasive , real - time , ionizing radiation diagnostic tool for the study of pleuro - pulmonary disease . 
the tus signs described by the authors are suggestive of earlystage lung parenchymal involvement in ctd : the thickening and irregularity of hyperecoic pleural line , the presence of pleural / subpleural nodules and the increased number of b - lines artifacts in relation to the severity of the underlying pathology [ 1 , 2 ]  . 
we agree that clinicians may apply tus as a potential screening tool in ild evaluation and as excellent methodology for establishing the correct timing of high - resolution computed tomography ( hrct ) , remaining hrct the gold standard for appropriate detection , characterization and radiological diagnosis [ 2 ]  . 
the number and the intensity of the visible vertical artifacts also depend on the type and frequency of the probe used , as well as the degree of total gain compensation ( tgc ) , electronic focus and tissue harmonics [ 3 ]  . 
moreover , ring - down generation is affected by the relationship between the probe curve and the curved thoracic surface and by the respiratory rate [ 3 , 4 ]  . 
 b - lines are very sensitive , but unfortunately non - specific us artifacts , because they are detectable in many other pulmonary conditions such as pneumonia , atelectasis , acute lung injury , acute respiratory distress syndrome , ground glass opacity , chronic obstructive pulmonary disease , pulmonary fibrosis , lymphangitis and in post - pneumonectomy space vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 6667 tool for the assessment of interstitial lung disease in rheumatic patients . 
sperandeo m , de cata a , molinaro f , trovato fm , catalano d , simeone a , varriale a , martines gf , trovato g ( 2015 ) ultrasound signs of pulmonary fibrosis in systemic sclerosis as timely indicators for chest computed tomography . 
sperandeo m , rotondo a , guglielmi g , catalano d , feragalli b , trovato gm ( 2014 ) transthoracic ultrasound in the assessment of pleural and pulmonary diseases : use and limitations . 
sperandeo m , frongillo e , dimitri lmc , simeone a , de cosmo s , taurchini m , cipriani c ( 2019 ) video - assisted thoracic surgery ultrasound ( vats - us ) in the evaluation of subpleural disease : preliminary report of a systematic study . 
another crucial point about us semeiotics in patients with pulmonary fibrosis is that , during intraoperative lung ultrasound ( ilu ) examination with a linear probe placed directly on lungs without any interposed interface , b - lines are not present [ 5 ]  . 
rates of global perceived utility and future intention to use the questionnaire were 100% . conclusions the vhnss - it has demonstrated to be a useful measurement of symptoms burden for patients with hnc . 
 the survey can be easily completed during the clinic routine without interfering with doctors visits schedule , and it can help healthcare providers to identify symptoms that require referral , education or intervention . keywords head and neck cancer patient - reported outcome measure symptoms screening * marta maddalo marta.maddalo@gmail.com 1 department ofradiation oncology , asst spedali civili di brescia brescia university , brescia , italy 2 department ofradiation oncology , ospedale di esine asl vallecamonica - sebino , esine , italy 3 department ofradiation oncology , university hospital ofudine , asuiud , udine , italy 4 department ofmedicine , vanderbilt university medical center , nashville , tn , usa 5 department ofradiation oncology , brescia university istituto del radio o . 
alberti , spedali civili hospital , piazzale spedali civili 1 , 25123brescia , italy introduction head and neck cancer ( hnc ) patients experience a broad array of symptoms , which could be related both to treatment and to the cancer itself [ 1 , 2 ]  . 
an instrument sensitive to head and neck cancer symptoms should lead to their accurate identification and quantification , allow earlier interventions for individual patients and serve as a research tool to compare the symptom burdens associated with various treatment options . 
 the large majority of tools available at the present time have been developed predominantly as research tools to assess a specific phenomenon of interest ( example : quality of life )  . 
 most of these tools were not designed to be used in clinical vol . : ( 0123456789 ) 1 3 424 la radiologia medica ( 2020 ) 125 : 423431 practice . 
the revised version of the questionnaire ( vhnss 2.0 ) includes 50 questions ranked using a likert scale between 0 ( no symptom ) and 10 ( severe symptoms )  . all reasonable tools must demonstrate adequate psychometric properties : a significant level on consensus has been reached on how to assess and critically analyze the metrological properties ( validity , reliability and sensitivity ) of a questionnaire , and many of the commonly used and available tools , including the vhnss [ 3 ] , have shown to match these criteria . 
when the primary aim of a tool is screening in clinical practice rather than clinical research , however , a pros tool needs to meet also a different set of criteria . 
a tool meant to be used for screening in clinical practice has to be in fact easy to use , in - context , actionable and useful . a pilot study on the italian translated version of the vhnss ( vhnss - it ) was performed to assess both the feasibility and utility of its administration in clinical practice . 
herein are reported the results of the pilot test on feasibility and utility that was meant to verify the properties of the screening tool to be easy to use , in - context and useful . the protocol was approved by the ethical committee of the spedali civili di brescia hospital , and the study was activated in february 2015 ( id number 1925 )  . materials andmethods patients inclusion / exclusion criteria eligibility criteria included ( 1 ) 18 and over years of age ; ( 2 ) diagnosis of hnc ( first diagnosis , recurrence or metastatic settings ) : all histology and all cancer sites ( rhinopharynx , oropharynx , hypopharynx , larynx , oral cavity , salivary gland , nasal cavity and paranasal sinus ) were accepted ; and ( 3 ) italian native speakers . study design andstatistical analysis this pilot study was designed to test the feasibility for both patients and clinicians of implementing the vhnss - it in a facilitys routine and to investigate its utility among clinicians , who are supposed to administer and review the questionnaire and then act on the information thus guiding management . the objectives of this pilot test were to analyze : ( 1 ) the feasibility to recruit patients ; ( 2 ) the feasibility to complete the questionnaire ; ( 3 ) the feasibility to review the questionnaire ; ( 4 ) the utility perceived by clinicians ; and ( 5 ) the distribution of patients answers reflecting symptoms intensity . the size of the patients sample ( n = 35 ) was calculated following the formula [ 4 ] : n = z2 p ( 1 p ) d2 where n = sample size , z = z statistic for a level of confidence , p = expected prevalence and d = precision . 
 sample size was related to rate of adhesion , one of the primary objectives of the study : in order to validate the italian version of the vhnss as a symptom screening procedure , the patients refusal rate ( p ) was requested to be < 10% . 
the maximum error of estimate ( d ) was set at 10% . all eligible patients were asked to sign the informed consent , even if they were not interested in participating to the study , in order to identify the number of refusals ( feasibility to recruit )  . 
time to completion was recorded using a timer ( feasibility to complete the questionnaire )  . six clinicians of a radiation oncology department , who were routinely involved in hnc patients treatment management and follow - up , were asked to recruit patients . 
clinicians were also asked to complete a dedicated questionnaire answering questions on acceptability of time burden ( feasibility to review ) , ease of use and identification of potential problems that were previously unrecognized ( utility )  . 
clinician had to list the unaddressed symptoms and to quantify their clinical relevance rating them on a 10 - point scale , where 0 represented no relevance and 10 represented critical relevance . 
global perceived utility and future intention to use or not to use the questionnaire in clinic were investigated ( utility )  . demographic and background information , data of the hnc disease and treatment , of the questionnaire for clinician and of the vhnss - it were double entered into the statistical software package spss version 17.0. 
descriptive statistics were used to describe the sample and to summarize 1 3 la radiologia medica ( 2020 ) 125 : 423431 the distributions of the study variables , including demographic information , hnc disease / treatment information and measures of symptom by the vhnss - it . 
required time to complete ( patients ) and required time to review ( clinicians ) were described using median and 25th75th inter - quartile ranges ( iqr ) , minimum and maximum values . 
in order to validate the feasibility of administering the tools as a symptoms screening measure in clinic , a median time to complete of 15min , a time to complete < 20min in at least 80% of patients , a median time to review of 3min and a time to review < 5min in at least 80% of reviews ( 18 total , three for each clinician ) were hypothesized . 
given this possible bias , this datum was not meant for validation purposes and deliberately set at a low rate : in fact , a fair number of positive answers , hypothesized as > 50% , was conjectured . 
even if the symptom screening and management could be a prerogative of only some of the clinician involved in the treatment and follow - up of patients with hnc a rate of positive answers on the question of future intention to use the tool > 50% ( 3 / 6 clinicians ) was considered desirable . results between april and may 2015 , 38 patients were screened and they were found to meet inclusion criteria . 
time burden was perceived to be table 1 patients , tumor and treatment characteristics gender kps at the time of the questionnaire grade of education employment status smoke alcohol cancer location stage t stage n stage m stage radiotherapy surgery women median [ range ] primary school middle school high school university full - time part - time unemployed retired quit quit nasopharynx oropharynx hypopharynx larynx oral cavity salivary glands neck recurrence other n2an2b n2cn3 curative postoperative palliative ( high dose ) 68 [ 4587 ] 1 3 426 table 1 ( continued ) chemotherapy acceptable for all clinicians ; they all also found the questionnaire easy to use . 
unrecognized symptoms and their clinical relevance rated by clinicians are listed in table2 . table 2 unrecognized symptoms with their clinical relevance reported by clinicians item la radiologia medica ( 2020 ) 125 : 423431 for the last three patients , clinicians were allowed to review the questionnaire during the visit . 
 median age of this group of patients was significantly higher than that of patients who completed the questionnaire by themselves : 77.4 years ( range 6687 ) versus 65.6 years ( range 4583 ) , p < 0001 . 
i have limitations in the ability to move my neck and shoulders 347 348 347 279 3510 338 1 3 la radiologia medica ( 2020 ) 125 : 423431 helped by caregivers and the group of patients who filled the questionnaire by themselves ( p = ns )  . time of completion was influenced by age , grade of education and employment status , as shown in fig.1. 
 the number of missing answers on the entire questionnaire per single patient was of three items ( 6% ) in one patient , of two items in one patient ( 4% ) and of one item ( 2% ) in six patients . 
rate of missing answers on all questionnaires per single item was 3% in items 4 , 10 , 15 , 16 , 19 , 21 , 27 , 28 , 39 , 40 and 45 . the distribution of patients answers reflecting symptoms intensity was described using box plot . 
2 distribution of patients answers ( symptoms intensity ) treated with radiotherapy alone compared with those who were treated with concurrent chemo - radiation . discussion arnould proposed a definition of a pros questionnaire developed for clinical practice as a standardized questionnaire through which a patient reports about her / himself in order for the healthcare provider to optimize the service delivered to her / him [ 5 ]  . 
even if a 50 - question survey could be considered lengthy , all the recruited patients in the present pilot study completed the questionnaire within an acceptable amount of time , with a median time of completion less than half of the one hypothesized in the study design . 
the inter - quartile range of the time of completion was also fairly uniform ( 544814 ) , demonstrating that the survey can be easily completed during the clinic routine without interfering with doctors visits schedule . 
the rate of missing answers on the vhnss - it was also extremely low , and it was therefore hypothesized that most cases of missing data were random , as previously reported during the process of validation of the english source [ 6 ] , meaning that the aim to make the translation clear and simple was effective . as to be expected , time of completion was found to correlate with patients age , with longer time in elderly . 
moreover , time of completion was found to correlate with patients educational level ( shorter in patients who attended high school or university ) and employment status ( longer in retired )  . 
only one patient refused to complete the survey : the adherence rate was thereafter extremely high ( 97% )  . it is important to notice that a screening tool has to be easy to use not just for the patient but also for the person administering the screening tool , usually the clinician . 
as previously reported in the literature , these symptoms are typically worse during treatment and during the first months after the end of treatment [ 79 ] , and this confirms the ability of the tool to identify symptoms changes over time . 
nonetheless , cross - sectional study is not meant to investigate the ability of a questionnaire to detect clinically important changes in health status over time and the responsiveness should be tested in a larger longitudinal study . it is well known that symptoms may vary depending on the therapeutic modality . 
classically , neck and shoulder dysfunction has been associated with surgical procedures in which the spinal accessory nerve is removed leading to shoulder problems characterized by shoulder droop , winged scapula , weak abduction and inability to shrug [ 10 , 11 ]  . 
only 2% of patients with a hnc have trismus at the time of diagnosis due to tumor growth [ 13 ] , and trismus is more likely known as a complication of hnc treatment . 
surgery and radiation can induce damage in muscles involved in mastication , such as the masseter and the pterygoid , in their neural innervation , in the temporal mandibular joint and / or in other supportive tissues , leading to a decrement of the jaw range of motion . 
average scores on head and shoulder range of motion , trismus and nutrition were found to be higher in patients who underwent surgery before radiotherapy : these are symptoms that are more closely related to the loss of functionality due to the surgical procedure [ 1418 ]  . in conclusion , the vhnss - it has demonstrated to be a useful measurement of symptoms burden for patients with hnc . 
this sign is considered a hallmark sign of pancreatic cancer on magnetic resonance cholangiopancreatography , but it can also be identified in patients with chronic pancreatitis or with other conditions . 
 the aim of this article was to describe the strong ct and mr imaging features or integrated imaging features that can help to differentiate between pancreatic cancer and focal chronic pancreatitis . keywords imaging features differentiation focal chronic pancreatitis pancreatic cancer introduction pancreatic adenocarcinoma is typically seen as a hypoenhancing mass that deforms or that does not deform the pancreatic contour . 
this hypoenhancing mass is best identified by computed tomography ( ct ) in the pancreatic phase at about 45s after contrast media injection ( 2ml / kg ) at a rate of 34ml / s , which provides the best contrast between the tumor and the pancreas . 
 the ancillary signs associated with the tumor itself that are crucial for diagnosis include dilatation of biliary and pancreatic duct ( double - duct sign ) , peripancreatic vascular invasion , and upstream parenchymal atrophy . 
typical imaging findings of chronic pancreatitis include generalized parenchymal glandular atrophy , diffuse pancreatic calcifications , dilatation of the main pancreatic duct , and occasionally pancreatic pseudocysts [ 1 ]  . 
 calcification in the pancreaticduct is highly specific for chronic pancreatitis . however , differential diagnosis between pancreatic cancer and focal chronic pancreatitis usually in pancreatic head is not clinically or radiologically straightforward because there are overlapping features [ 2 ]  . 
among the imaging signs , the only one with high specificity for malignancy is the presence of metastasis . however , there are other imaging signs that can enhance our ability to differentiate between pancreatic cancer and chronic pancreatitis , and this potentially improved diagnostic accuracy may lead to improved management and outcomes in this vulnerable patient population . 
accordingly , the aim of this article was to describe the strong ct and mr imaging features or integrated imaging features that can help to distinguish between focal chronic pancreatitis and pancreatic cancer . imaging signs since no one imaging sign has been shown to conclusively and reliably determine the presence of pancreatic cancer or focal chronic pancreatitis , the imaging signs and / or features described here need to be used in combination to improve the probability of an accurate diagnosis . 
however , in some cases , tissue confirmation may be required to confirm the diagnosis . doubleduct sign andsingleduct dilatation double - duct sign is the imaging sign that describes the simultaneous dilatation of the main pancreatic duct and the bile duct . 
the double - duct sign is often detected in association with pancreatic head cancer [ 4 ] ( fig.1 ) ; however , it is not specific , and it can be observed in benign processes , such as chronic pancreatitis and choledocholithiasis [ 5 ]  . 
specifically , in focal chronic pancreatitis , common bile duct ( cbd ) stenosis at the levelof the pancreatic head mass tends to be longer and more gradually tapered than inmalignant obstructions [ 7 ]  . 
in rare cases , pancreatic head cancer and focal chronic pancreatitis strict only the cbd , and only the bile ducts are dilated . there are several causes of isolated main pancreatic duct dilatation or single - duct dilatation . 
the two major causes are pancreatic cancer and chronic pancreatitis , and the other include intraductal papillary mucinous tumor and idiopathic dilatation ( about 15% of cases have no identifiable cause ) [ 8 ]  . 
in chronic pancreatitis , ct may lead to underestimation of the degree of parenchymal loss because abundant interlobular and periductal fibrosis and chronic inflammatory infiltrate can replace functioning parenchyma in some cases so that there is little or no loss of total pancreatic parenchymal volume . 
if the ratio criteria is satisfied , then the investigation for pancreatic cancer should focus on the head , neck , or even uncinate process of the pancreas [ 12 ]  . 
a thick slab mrcp shows double - duct sign with abrupt narrowing or ductal cutoff at the narrowest part that resembles a rat tail ( circle ) , which can be identified in malignant cause or pancreatic cancer . 
b coronal t2 - weighted image shows smooth tapering of distal cbd resembling pencil tip ( arrow ) which can be identified in benign stricture or narrowing main pancreatic duct dilatation or single - duct dilatation had benign pancreatic diseases [ 8 ]  . 
patients with single - duct dilatation also had a 35% chance of having pancreatic malignancy if there was no chronic pancreatitis . duct / parenchyma ratio it is very difficult to differentiate chronic pancreatitis from pancreatic cancer based on the degree of pancreatic duct dilatation alone ; however , pancreatic duct dilatation may be slightly more prominent in patients with pancreatic cancer . 
 there was a significant difference in the caliber of the pancreatic duct , with larger caliber observed in patients with pancreatic cancer , and the degree of pancreatic gland atrophy was more pronounced in patients with pancreatic cancer compared to patients with chronic pancreatitis [ 10 ]  . 
when superior mesenteric artery ( sma ) / superior mesenteric vein ( smv ) ratio invasion of the sma and smv has traditionally been considered an imaging sign for differentiating pancreatic cancer from chronic pancreatitis and other benign conditions . 
this may be another helpful criterion for distinguishing between chronic pancreatitis and pancreatic cancer [ 14 ]  . penetrating duct sign , ductal cutoffsign , andicicle sign previous studies found that a nondilated main pancreatic duct coursing through a pancreatic mass is most likely to indicate a diagnosis of focal chronic pancreatitis . 
this sign can be assessed on mrcp or endoscopic retrograde cholangiopancreatography ( ercp ) , and it is necessary for evaluating the caliber and morphology of the pancreatic duct coursing through the area of the focal mass [ 15 ]  . 
the duct penetrating sign on ct and mrcp is more helpful for differentiating between pancreatic cancer and chronic pancreatitis than a delayed enhancing pattern on ct or mr [ 16 ]  . pancreatic cancer usually starts in the ductal epithelium and grows centrifugally , which explains its manifestation as ductal cutoff sign , and this sign may be observed even when there is no obvious mass formation . 
the appearance of interruption or cutoff of the duct is a major element and can be the principal sign if the lesion is isodensity or isosignal intensity ( 1114% of adenocarcinoma ) [ 17 ]  . in contrast , the icicle sign or ice pick sign , a smooth tapered narrowing of the upstream pancreatic duct is frequently seen in autoimmune pancreatitis [ 18 ]  . 
focal chronic pancreatitis is likely 1 3 360 la radiologia medica ( 2020 ) 125 : 356364 smudged margins between the inflamed and normal pancreas might also contribute to the icicle sign of pancreatic duct [ 19 ]  . 
another clue for diagnosis of autoimmune pancreatitis ( aip ) is involvement of extrapancreatic organs , such as the biliary tree , retroperitoneum , salivary gland , and kidney . morphology ofpancreatic duct andcollateral duct ( caliber andcontour ) the upper limit of normal pancreatic duct diameter in previous publications ranges from 2mm to 8mthere is no consensus regarding the diameter size criteria that defines pancreatic duct dilatation , but a diameter of greater than 3mm in the head , and greater than 2mm upstream to the head is often considered dilated [ 21 ]  . 
contour irregularity with dilatation of pd , which indicates the presence of periductal fibrosis , is the cardinal sign of chronic pancreatitis ( figs.6b ) , whereas smooth or beaded dilatation of the pd upstream to the mass is more likely to be seen in pancreatic cancer [ 23 ]  . on mrcp , the chain of lakes sign can be identified in typical diffuse chronic pancreatitis . 
an irregularity dilated pancreatic duct is detected along with multiple calcifications mainly in side branches of the pancreatic duct through the body and tail of pancreas ( arrow ) direct vascular invasion vascular invasion is the sign that strongly suggests pancreatic cancer over focal chronic pancreatitis . 
in the absence of distant metastatic disease , vascular invasion is the single most common criterion for unresectability in patients with pancreatic adenocarcinoma [ 28 ]  . thickening oftheceliac axis and / orsuperior mesenteric artery ( sma ) soft tissue thickening around the celiac artery and / or sma in the retropancreatic space is observed in 3060% of ct in pancreatic cancer . 
inset axial ct scan venous phase shows teardrop sign that represents the tethering of the mass to smv , which produces a teardrop shape of smv ( arrow ) that indicates local invasion of the smv fig . 
a axial t2 - weighted image with fat suppression shows focal mass at pancreatic head with dilated small side branches present inside the mass ( arrow ) and patent smv ( arrowhead )  . 
b axial t1 - weighted post - gadolinium image shows hypovascular enhancement of this inflammatory mass ( arrow ) with mild spiculated border ( arrowhead ) responsible for this finding . 
this finding was associated with tumors of the body of the pancreas in 52% of cases , and with tumors of its head in 25% of cases [ 29 ]  . 
this sign is occasionally the main discriminating or helpful sign in the case of an isodense pancreatic cancer , but cannot be considered a pathognomonic sign ( fig.9 ) since it is also identified in cases of chronic pancreatitis or peripancreatic disease , such as lymphoma [ 30 ]  . 
this is particularly true in cases of autoimmune or ig g 4 pancreatitis with extrapancreatic manifestations , such as sclerosing mesenteritis and retroperitoneal fibrosis , in which perivascular fat soft tissue thickening can be observed [ 31 ]  . 
although this finding is less common in cases of chronic pancreatitis , infiltration of perivascular fat of sma is likely to be the result of extension of the inflammatory process welldefined demarcation due to fibrosis found in both pancreatic cancer and focal chronic pancreatitis , both show more gradually progressive hypovascular enhancement . 
when fibrotic component is diffusely present throughout the 1 3 362 la radiologia medica ( 2020 ) 125 : 356364 alcohol - induced chronic pancreatitis and hereditary chronic pancreatitis show calcifications in the pancreas at a relatively earlier stage and in larger size ( 25cm ) than in other causes of chronic pancreatitis , such as obstructive chronic pancreatitis and cystic fibrosis - related chronic pancreatitis [ 37 ]  . 
in the context of chronic pancreatitis , calcifications displaced by the mass , any abnormal contour bulge , and / or change in the form of mass effect are classic signs that suggest carcinoma [ 39 ]  . diffusionweighted image ( dwi ) andapparent diffusion coefficient ( adc ) image only a few studies have reported the usefulness of dwi in pancreatic cancer . 
one previous study reported that pancreatic cancer has high signal intensity on high b value dwi and lower adc value , which made it distinguishable from benign mass - forming chronic pancreatitis [ 40 ]  . 
the other study found no significant high signal intensity on dwi or lowering of adc in either mass - forming chronic pancreatitis or pancreatic cancer compared with the rest of the pancreatic parenchyma . 
note the normal enhancement of uninvolved pancreatic head around the mass with clear demarcation at the interface ( black arrowhead ) pancreas , there is no or less demarcation of the pancreatic mass due to focal chronic pancreatitis [ 32 ]  . 
in pancreatic carcinoma , the pancreas surrounding the mass lesion usually shows normal enhancement on pancreatic phase , and normal high signal intensity on both t1 - weighted image with fat suppression and dynamic gd - enhanced images . 
any abnormal contour bulge or change in the morphology in the form of mass effect , and / or alteration or disappearance of preexisting calcification should increase suspicion for pancreatic cancer [ 34 ]  . calcifications pancreatic calcifications are the most specific and reliable ct sign of chronic pancreatitis . 
the sensitivity , specificity , positive predictive value ( ppv ) , and negative predictive value ( npv ) of 64 - mdct in detecting periampullary duodenal diverticula were calculated . 
indications of ercp were common bile duct stricture ( n = 62 ) or stone ( n = 41 ) , biliary cholestasis ( n = 16 ) and acute cholangitis ( n = 1 )  . 
the size of diverticula was the only predictor of 64 - mdct performance , with better results observed in larger ( > 20mm ) diverticula . conclusion 64 - mdct is a highly specific imaging modality in detecting periampullary duodenal diverticula . 
the diagnostic performance of 64 - mdct increases for larger diverticula . keywords endoscopic retrograde cholangiopancreatography multidetector computed tomography periampullary duodenal diverticula introduction diverticula are small outpouchings of the gastrointestinal tract wall , which comprise mucosa , submucosa , and discrete muscular cells [ 1 , 2 ]  . 
in the duodenum , the majority of these diverticula are located inside a radius of 2cm of the major papilla , the protrusion of the ampulla of vater into the duodenum , and so - called periampullary duodenal diverticula . 
 in essence , periampullary duodenal diverticula are acquired * daniel fadaei fouladi dfoulad1@jhmi.edu 1 medical radiation sciences research group , tabriz university ofmedical sciences , tabriz , iran 2 department ofgastroenterology , imam reza teaching hospital , tabriz university ofmedical sciences , tabriz , iran 3 neurosciences research center , tabriz university ofmedical sciences , tabriz , iran lesions and develop more frequently with the advanced age [ 3 ]  . 
furthermore , food impaction in a duodenal diverticulum may cause pancreaticobiliary problems such as obstruction , inflammation , and infection [ 7 , 8 ] , and in rare cases , diverticulitis develops following the perforation of a diverticulum [ 9 , 10 ]  . endoscopic retrograde cholangiopancreatography ( ercp ) is the method of choice in detecting and treating duodenal diverticula [ 11 ]  . 
therefore , ercp is rarely used during the early management of symptomatic patients with suspected duodenal diverticula [ 13 ]  . some authors suggest computed tomography ( ct ) as a safer surrogate for ercp in such patients . 
1 measurement of the size of a periampullary duodenal diverticulum in a 69 - year - old female with biliary cholestasis by 64 - slice multidetector computed tomography on axial ( a ) , sagittal ( b ) , and coronal ( c ) planes . 
periampullary duodenal diverticula were classified according to a previously described system [ 17 ] as follows : type a , the major papilla and the diverticulum are located far from each other ; type b , the papilla is located table 2 the size and type of periampullary duodenal diverticula ( n = 100 ) defined by using endoscopic retrograde cholangiopancreatography variable size small ( 10mm ) medium ( > 10mm , 20mm ) large ( > 20mm ) type no ( % ) 13 ( 13 ) 43 ( 43 ) 44 ( 44 ) 8 ( 8 ) 79 ( 79 ) 7 ( 7 ) 6 ( 6 ) adjacent to the diverticulum ; type c , the papilla is located at the edge of the diverticulum ; and type d , the papilla is located inside the diverticuluthe diverticula were categorized by their largest measured diameter as small ( 10mm ) , medium ( > 10mm , 20mm ) , and large ( > 20mm )  . multidetector computed tomography protocol contrast - enhanced computed tomographic studies were performed with a 64 - slice multidetector ct scanner ( somatom sensation 64 , siemens , germany ) using the following parameters : collimation , 1mm ; pitch , 0.8 ; reconstruction increment , 1mm ; rotation time , 0.33s ; 120kv per slice ; and 120140 mas . 
the oral contrast agent was 76% gadoterate meglumine ( gd - dota , dotarem ; guerbet , roissy cdg cedex , france ) , which was administrated as 40ml in 3l of water 68h before ct imaging in all patients . 
the intravenous contrast agent was iodixanol ( visipaque 320mg / ml , nycomed amersham imaging , oslo , norway ) , which was administered at a dose of 12ml / kg body weight and at a flow rate of 2ml / s just before ct imaging . 
imaging was performed in the portal phase , 6070s after the contrast agent was injected . images were generated as automated 2 - mm axial , sagittal , and coronal reformats and reviewed using dedicated software ( syngofast view , siemens ag medical solution , siemens , germany ) by an attending radiologist with over 15 years of academic experience who was blind to the results of ercps . 
the same classification described for sizing of a diverticulum by ercp was also used here . statistical analysis the spss software version 19.0 ( ibm corporation , new york , usa ) was used for the statistical analysis . 
2 a 65 - year - old male with common bile duct stone and a periampullary duodenal diverticulum ( arrows ) , depicted by 64 - slice multidetector computed tomography on axial ( a ) , sagittal ( b ) and coronal ( c ) planes . 
 the endoscopic appearance of the diverticulum is also shown ( arrow ) ( d ) la radiologia medica ( 2020 ) 125 : 339347 by using 64 - mdct , periampullary duodenal diverticula were detected correctly in 76 patients ( figs.2 , 3 , 4 ) and missed in 24 patients . 
the highest agreement between the two methods was found for large diverticula , followed by for small and for medium ones , respectively . to determine potential factors related to 64 - mdct failure in detecting periampullary duodenal diverticula , study variables are compared between cases with true - positive and false - negative results in table5 . 
the majority of them , however , remain asymptomatic for a lifetime [ 19 ] , and therefore , they are not usually present in the differential diagnoses list during exploratory imaging studies in symptomatic patients [ 21 ]  . cross - sectional imaging techniques such as ct are useful modalities in detecting duodenal pathologies including diverticula [ 21 , 22 ]  . 
3 periampullary duodenal diverticulum ( arrows ) in a 72 - year - old male depicted by 64 - slice multidetector computed tomography on axial ( a ) , sagittal ( b ) and coronal ( c ) planes unless a regional surgical intervention was undertaken or the diverticulum became symptomatic [ 23 ]  . reformations has been found more accurate than conventional ct in detecting duodenal diverticula [ 28 ]  . because of the location of periampullary duodenal diverticula , they can cause technical difficulties during endoscopic sphincterotomy and ercp or may interfere with the accurate diagnosis of other conditions in that region such as cystic or pseudocystic pancreatic lesions [ 24 , 25 ]  . invasive endoscopic procedures such as ercp are not preferred as the initial diagnostic step even when a periampullary duodenal diverticulum is suspected to be the culprit in a symptomatic patient . 
mdct using multiplanar and curved planar like other diverticula in the gastrointestinal tract , duodenal diverticula manifest as the thickened wall of the duodenal bulb with stranding of the periduodenal fat on ct images . 
the observation of the neck of a diverticulum along with air - fluid levels and retained debris inside it is essential for distinguishing diverticula from other duodenal cystic lesions such as duplication and periampullary cystic neoplasms [ 31 , 32 ]  . comprehensive studies regarding the accuracy of ct in detecting duodenal diverticula are scarce in the literature . 
4 another patient ( 64 - yearold female ) with a periampullary duodenal diverticulum ( arrows ) depicted by 64 - slice multidetector computed tomography on axial ( a ) , sagittal ( b ) and coronal ( c ) planes la radiologia medica ( 2020 ) 125 : 339347 of duodenal diverticula in three patients . 
size : small ( 10 mm ) , medium ( > 10mm , 20mm ) , large ( > 20mm ) more accurate if images had been examined meticulously by experienced readers . to the best of the authors knowledge , there are only two studies in the literature that have examined the diagnostic role of mdct in patients with periampullary duodenal diverticula . 
 due to conservative approaches , none of the patients in this study underwent ercp or surgical intervention . despite high specificity , the sensitivity of 64 - mdct was intermediate in our study . 
this might be due to the inability of ct in depicting a collapsed diverticulum , or when there is substantial inflammation in the area [ 38 ]  . we also showed that the size of a diverticulum is the only independent predictor of 64 - mdct failure in detecting periampullary duodenal diverticula . 
fortunately , small duodenal diverticula are less likely to become symptomatic [ 19 , 28 ]  . despite its novelty and using rather large sample size , the present study bears a limitation that should be acknowledged . 
nonetheless , symptomatic patients who are considered candidates for ercp may drive benefit from the results of the present study by suggesting 64 - mdct as the initial screening modality to investigate the presence of a periampullary duodenal diverticulum as the source of their symptoms . conclusion multidetector computed tomography is a highly specific imaging modality in detecting periampullary duodenal diverticula . 
lymphatic system brings macromolecules and fluids that extravasated from the blood vessels back into the * michaela cellina michaela.cellina@asst - fbf - sacco.it 1 reparto di radiologia , ospedale fatebenefratelli , asst fatebenefratelli sacco , milano , piazza principessa clotilde 3 , 20121milan , italy 2 dipartimento di scienze biomediche perla salute , universit degli studi di milano , via mangiagalli 31 , 20133milan , italy 3 department ofradiology , division ofspecial andpediatric radiology , university hospital umberto i lancisi salesi , via conca 71 , 60126ancona , an , italy systemic circulation to maintain the fluid balance , plasma volume and tissue pressure . its malfunctioning leads to accumulation of fluid in the interstitium and activation of the inflammatory cascade , resulting in deposition of subcutaneous fat , fibrosis and skin changes [ 2 ]  . le can be classified as primary or secondary . 
traditionally , lymphoscintigraphy with intradermal injection of a radioactive colloid has been used ; this technique involves the acquisition of initial dynamic flow images and static images at 1h and up to 6 or 24h , and its main limitations are long acquisition time and ionizing radiation exposure [ 4 ]  . 
non - contrast mr lymphangiography ( ncmrl ) is based on heavily t2 - weighted sequences , with a very long tr / te , like that used in cholangiopancreatography , able to enhance fluidfilled structures , as lymphatic vessels , with a suppression of the background signal . 
since the response to conservative and surgical treatments in le is based only on clinical evaluation , we want to propose a new approach with ncmrl to calculate the lower extremities volumes in patients affected by le . materials andmethods the study had been approved by the local ethical committee and follows local and international laws and guidelines ( helsinki declaration ) , and all participants had given their informed consent . ten female patients affected by praecox primary le of the lower limbs ( mean age 33 5years ; age range 1642 ) underwent ncmrl in september 2019 . 
the examination was obtained in various steps to cover all the anatomical stations of the lower limbs [ 7 ] ; then , the images were combined with the composing function to show the whole lower extremities ( siemens medical systems , erlangen , germany )  . 
the dicom image series of stir sequences was imported to the open - source software itk - snap software ( version 3.4 , university of pennsylvania , united states ) [ 810 ]  . 
the volume of each extremity was automatically calculated in the volume and statistics window , where the value represents the product of the number of segmented voxels multiplied by the voxel volume . mean segmentation time was calculated . 
image showing the segmentation procedure of the lower extremities volumes table 1 calculated volumes of different portions of left and right lower limbs and total volumes thigh knee ankle total right 3833 6875 2927 13.635 left 4185 5005 1808 10.998 total 8018 11 , 880 4735 24.633 however , there is no consensus about the imaging technique suitable for these aims . 
however , cemrl is limited by a suboptimal visualization of the larger lymphatic vessels and by possible confounding effect of the venous enhancement ; moreover , the subcutaneous gadolinium injection is still off - label , and the evidence of gadolinium deposition pushed towards totally non - invasive techniques that do not involve contrast media administration , as ncmrl . 
ncmrl is based on heavily t2 - weighted sequence , able to highlight static or slow - moving fluid - filled structures , such as the lymphatic vessels , with a suppression of background tissue signal [ 6 , 7 ] , usually combined with morphological sequences for dimensional assessment of the affected limbs ; therefore , with a single examination , information regarding the characteristics of le and lymphatics appearance and objective measurements of the limbs volumes can be obtained . the current approach to le dimensional assessment is based on clinical exam and on limb tape circumferential measurement , consisting in measurements taken at predetermined anatomical points , whereas no imaging techniques has been applied to calculate le volumes . itk - snap is an open - source software that has been successfully used for segmentation of biomedical images [ 810 , 12 , 13 ]  . for assessment of lower limbs volumes , fully automatic and semiautomatic segmentation algorithms cannot be applied ; therefore , manual segmentation is the only available choice . with our preliminary study , we demonstrated that manual segmentation through itk - snap of ncmrl images is a quick , reliable and reproducible method to calculate limbs volumes , and this represents an additional information that this imaging exam can provide and can be used as a starting point to measure the response of the body to treatment . this is a preliminary study ; therefore , our main limitation is the limited number of patients . 
body tissue molecules vary for their specific atomic numbers and electron density , and the interaction with different sets of radiations results in different attenuations , allowing to their final distinction . 
for instance , contrast resolution improvement and metal artifact reduction can be obtained through virtual monoenergetic images , dose reduction by virtual non - contrast reconstructions and iodine distribution highlighting through iodine overlay maps . 
although lung perfusion is one of the most investigated , this evaluation has been extended to narrowly fields of application , such as musculoskeletal , head and neck , vascular and cardiac . 
this type of configuration allows an independent setting of each x - ray beam , with the possible use of different filters in order to increase the image quality . the kvp values usually employed are 80100kvp and 140150kvp . the main limits are related to the hardware components placement , which result in a restricted field of view and in cross - scattering phenomena between the two detector layers . 
the temporal misregistration ( 71125ms ) between the two sources also increases the susceptibility to motion artifacts [ 1 , 3 , 5 , 9 , 11 , 12 ]  . ( b ) single - source ct scanner with fast kilovolt peak switching technology ( ge healthcare , waukesha , wi , usa )  . this type of scanner uses a single radiation source that dynamically and rapidly switches from the high ( 80kvp ) to the low ( 140kvp ) energy peak and vice versa and provided with a single detector layer . unlike the former one , this technology is not impaired by a limited fov and motion artifacts . 
the limits consist in the trapezoidal shape of the radiation beam , which in practice determines the levels of energy lower than the nominal values [ 1 , 3 , 5 , 9 , 11 ]  . ( c ) layered detector dect ( philips healthcare , andover , ma , usa ) it is composed of a single source and two different layers , made of different materials , placed one on top fig . 
main post - processing reconstruction algorithms : ( a ) non - material specific ( a ) linear blending allows combining in one set the high contrast obtained at low energies and the little noise derived from the high levels . 
in order to obtain an image quality similar to the 120 kvp on sect , the ratio commonly employed is 0.3 ( 30% of data from low and 70% from high energy ) [ 5 , 8 , ( b ) nonlinear blending ( or sigmoid blending ) uses a different reconstruction algorithm that demonstrated a higher contrast rather than linear blending images , maintaining the noise reduction resulted from high energies [ 14 , 15 ]  . ( b ) material specific include three material decomposition for dual - source and two - material decomposition for fast - switching scanners . 
these differences can be exploited for emphasize ( i.e. , iodine maps , iron quantification ) or understate their contrast ( i.e. , virtual non - contrast or vnc , or bone removal images ) [ 2 , 5 , 6 , 810 ]  . la radiologia medica ( 2020 ) 125 : 384397 ( c ) energy specific enables one to reconstruct virtual monochromatic ( or monoenergetic ) images ( vmi ) within a wide range of energies . 
the endovascular thrombus is visible on the axial angiographic standard ct scan ( a ) , while iodine map ( b ) and 3d perfusion reconstruction ( c ) provide a wider overview of the lung perfusion 1 3 la radiologia medica ( 2020 ) 125 : 384397 tep is a clinical condition consisting in a complete or partial occlusion of the pulmonary arteries by circulating vascular clots due to several clinical reasons [ 19 ]  . on iodine maps , the emboli cause ventilationperfusion mismatches , displayed as perfusion defects ( pds ) and characterized by a typical triangular shape with a subpleural ( segmental or lobar ) distribution [ 19 ]  . numeric schedules are also automatically generated by the software , showing the iodine concentration on a mgi / ml or hu scale . 
these tables can further split the total amount into smaller parts , differentiating the side ( right and left ) and the lung segments ( upper , medium and lower )  . although not well distinguishable from the acute form , perfusion images have also shown a high degree of sensitivity and good specificity in the evaluation of pulmonary hypertension due to chronic thromboembolism ( cteph ) [ 21 ]  . nevertheless , cteph is usually associated with a bronchial and systemic circulation supply that leads to a hyperenhancement of the lobes or segments involved in the delayed phases of the examination [ 19 , 21 ]  . pds can also be detected in subjects with no thromboembolism on pulmonary ct angiography , as a possible consequence of chronic or residual embolism [ 17 ]  . beyond the first diagnosis , iodine perfusion maps can also be exploited for pe follow - up . in fact , the evaluation of the therapy response takes advantage not only from the mere visual appearance , but also from the comparison of the numerical values between the former and the latter dect scans , allowing a more objective and trustful appraisal [ 23 ]  . however , for what concern the risk stratification of the patients with tep , dual energy has not shown higher advantages than morphological measurements ( i.e. , ventricular diameters ratio ) yet [ 24 ]  . 
moreover , the higher detection degree of dect rather than angiography ct is still under debate , since the additional findings had a segmental or subsegmental localization , whose clinical significance is still unclear [ 17 , 25 ]  . in order to perform an accurate evaluation , true pds have to be distinguished from not perfused areas , such as parenchymal anomalies ( emphysema , atelectasis , consolidations , tumors and aberrant vascular supply ) and artifacts . diaphragmatic and cardiac movements represent the major artifacts in iodine maps . 
they usually appear as crescent - shaped , blurring or double lines in the lung bases or in the paramediastinal regions . if the former can be decreased through the performance of good breath - hold scan , cardiac motions are difficult to avoid . 
iodine overlay with iodine quantification allowed differentiating the neoplastic component ( arrowheads ) , mainly necrotic , from the surrounding atelectasis lung parenchyma ( arrows ) , characterized by higher iodine content fig . 
6 dect follow - up scan performed in a 62 - year - old male patient previously operated for adenocarcinoma of the right lung , in which a new groundglass nodule was detected within the right lower lobe ( a )  . 
the different iodine content can be explained by the higher necrotic component within the left 1 3 390 la radiologia medica ( 2020 ) 125 : 384397 ( g ) other thoracic application fields dect can also be considered a complementary tool in the differentiation of benign from malignant mediastinal mass , with the iodine concentration measurement in the early and delayed phases being more accurate than the mean attenuation values [ 42 ]  . the dect evaluation of airways diseases using inhalational contrast agents , due to their expensiveness , up to now is still far away from the daily clinical routine , and its discussion is beyond the purpose of this paper [ 20 ]  . the dect evaluation of the breast is also currently emerging . 
dynamic acquisitions can be also performed , although the radiation dose inevitably increases . iodine maps seem to be more accurate than cardiac mri , spect and angiography [ 4651 ]  . perfusion images , basing on tissue characterization , could assess the hemodynamic significance of coronary stenosis , allowing in differentiating between chronic reversible ischemia and infarct . however , a standardization of these reconstruction algorithms is still missing . ( b ) virtual monoenergetic imaging ( vmi ) vmi reconstructions can be exploited at two different ranges for different purposes : at low energies ( 70kev for traditional vmi , up to 40kev for > vmi + ) in order to increase the snr and cnr of iodine , and above 100kev to reduce blooming artifacts near hyperdense structures ( i.e. , coronary metal stents and calcified plaques ) ( figs.8 and 9 ) [ 52 ]  . in particular , a range comprised between 130 and 150kev seems to be optimal for the evaluation of the lumen , even in the presence of stents with a caliber smaller than 3mhowever , differences can be found due to the different types and brands of the stents [ 53 , 54 ]  . it is important to remember that at high energy levels , although the visualization of the vascular lumen is improved , the visualization of the high - density structures , such as the fig . 
rather than axial ( a ) and coronal ( b ) m_0.6 images , iodine map ( c ) and noise - optimized low kev vmi + ( d ) provide improved visualization of the hypoperfused myocardial tissue . 
10 71 - year - old male patient with thoracic aortic aneurysa hyperdense component is detectable within the aneurysm sac is detectable on both contrast - enhanced linearly blended image ( a ) and virtual non - contrast reconstruction ( b )  . 
compared to vmi 70kev image ( a ) , vmi 140kev reconstruction ( b ) shows a significant decrease in beam - hardening artifacts , improving the evaluation of the surrounding soft tissues courtesy of l . 
in this paper , we present a novel method to classify the malignant from benign lung nodules based on ct images using squeeze - and - excitation network and aggregated residual transformations ( se - resnext )  . 
the state - of - the - art se - resnext module , which integrates the advantages of senet for feature recalibration and resnext for feature reuse , has great ability in boosting feature discriminability on imaging pattern recognition . 
the method is evaluated on the public available lung nodule analysis 2016 ( luna16 ) database with 1004 ( 450 malignant and 554 benign ) nodules , achieving an area under the receiver operating characteristic curve ( auc ) of 0 . 
to our best knowledge , the effectiveness of se - resnext on lung nodule classification has not been extensively explored . keywords lung nodule classification squeeze - and - excitation ct images deep learning introduction lung cancer has become the leading cause of cancer death around the world with the highest number of mortalities . 
 according to the cancer statistics in the year of 2019 , 142 , 670 lung cancer deaths ( 23.51% of the total cancer patient ) are projected to occur in the united states [ 1 ]  . 
 therefore , early lung cancer diagnosis is critical to increase survival effectively . a lung nodule is a rounded opacity circumscribed parenchymal lesions with a diameter smaller than 3clung * shan jiang shanjmri@tju.edu.cn 1 school ofmechanical engineering , tianjin university , tianjin300350 , china 2 centre foradvanced mechanisms androbotics , tianjin university , 135 yaguan road , jinnan district , tianjin300350 , china nodules can be classified into malignant and benign nodules as shown in fig.1. 
generally , lung nodules can be detected on various medical images such as magnetic resonance imaging ( mri ) , positron emission tomography ( pet ) , and computed tomography ( ct )  . 
the national lung screening trial ( nlst ) also proved that using ct screening achieved a 20% reduction in the mortality of lung cancer [ 3 ]  . nodule diagnosis by radiologists is a complex and timeconsuming task , because they need to analyze masses of nodule information ( margin , size , texture , and shape , etc . ) from numerous ct images to obtain an accurate interpretation . 
computer - aided diagnosis ( cad ) systems , which consist of computer - aided detection ( cade ) and computer - aided diagnosis ( cadx ) vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 374383 fig . 
the number below each nodule is the nodule size ( mm ) systems , have been proven to be an efficient tool in both lung cancer detection and diagnosis [ 4 , 5 ]  . 
this paper mainly discusses cadx systems , which are aimed at characterizing and classifying the suspicious lesions with ct images . a popular cadx system mainly consists of four major steps : data acquisition , nodule segmentation , feature extraction , and nodule classification . 
one category classifies malignant and benign nodules based on handcrafted features which extracted by traditional feature descriptors , the other is based on deep features learned by various deep convolutional neural networks ( dcnns )  . handcrafted features usually include texture , shape ( geometry ) , intensity , and morphology . 
 [ 9 ] calculated texture , shape , and intensity features based on the gray - level co - occurrence matrix ( glcm ) , local binary pattern ( lbp ) , and gabor filter methods to characterize lung nodules and applied them to an improved random forest ( rf ) algorithm to classify malignant and benign nodules . 
 [ 15 ] reported on sixteen morphological and statistical features , and an ensemble of three classifiers consisting of multilayer perceptron ( mlp ) , k - nearest neighbor ( knn ) , and svm to classify benign or malignant lung nodules . 
 [ 17 ] used shape , size , and texture - based features to characterize nodules , they proven that ensemble classifiers with svm and rf base classifiers achieved the best performance compared to lda , knn , and adaboost base classifiers . though handcrafted features are popular in characterizing lung nodules , there are still many limitations . 
with the development of deep learning techniques , more and more networks were optimized based on cnns , such as 3d multi - view convolutional neural networks ( mv - cnn ) [ 22 ] and 3d multicrop convolutional neural network ( mc - cnn ) [ 23 ]  . 
compared with the 2d networks , 3d cnns can encode richer 1 3 376 la radiologia medica ( 2020 ) 125 : 374383 spatial information from ct images to learn more distinguishable features . 
 [ 28 ] presented a network named 3d dense convolutional binary - tree network ( densebtnet ) , which was based on densenet , to tackle the task of nodule classification . 
moreover , 3d dual path network ( dpn ) [ 29 ] , which integrated the advantages of resnet and densenet , was applied in the work [ 30 ] for lung nodule detection and classification . 
 [ 35 ] fused the shape , texture , and deep features at the decision level , employed an adaboosted back propagation neural network ( bpnn ) for nodule classification . 
 [ 36 ] found that combining size , shape , texture features , and deep features ( learned by alexnet ) to represent nodules could lead to a promising performance . 
thought the fused feature - based classification techniques achieved promising results , the limitations suffered in handcrafted feature - based methods were also occurred . in this paper , a novel 3d dcnn - based framework is presented to study the performance of malignant and benign nodule classification . 
to our best knowledge , the effectiveness of seresnext on lung nodule classification has not been extensively explored . in the present work , methods section introduce the proposed method in the classification of malignant and fig . 
finally , discussion and conclusion are given in discussion and conclusion sections . methods the proposed method for the classification of benign and malignant lung nodules consists of three major stages : ( 1 ) image data acquisition from the luna16 database ; ( 2 ) nodule extraction ; and ( 3 ) training se - resnext for nodule classification . 
a short summary of the proposed method is presented in fig.2. data acquisition the image database employed in this work for both training and testing is based on the luna16 database [ 38 ] , which is refined from the publicly available lung image database consortium image collection ( lidcidri ) [ 39 , 40 ]  . 
on top of that , nodules whose size is smaller than 3mm are also removed because these nodules are usually not dangerous according to doctors experience [ 42 , 43 ]  . 
to better capture most of selected nodules , the size of input patch is set to 32 32 32 . seresnext the se - resnext adopted in this work for nodule classification combines the resnext and senet . 
figure3 provides a structure of a resnext block with cardinality of 32 . a resnext module can be defined as : ures = x + i ( x ) is the output . 
the operation x + i = 1 i ( x ) represents the aggregated transformation , where c is the size of the set of transformations , x is the input and ures i = 1 i ( x ) is performed by a shortcut connection and element - wise addition . 
n is the number of channels of the residual mapping , l , w , and h represent the spatial length , width , and height of ures to utilize the aggregated information acquired in the squeeze operation efficiently , the excitation operation is employed to fully capture channel - wise dependencies . 
to address this objective , a gating mechanism is proposed , which can be described as s = fex ( z , w ) = ( w2 ( w1z ) ) the gating mechanism is parameterized by two fc layers to reduce the model complexity and enhance generalization , which are dimensionality - reduction layer with parameters 1 and reduction ratio r = 16 , a relu and a dimensionality - increasing layer with parameters 2 c r  . 
 after excitation operation , the final output of the se block xres n is obtained by rescaling the residual feature map ures with the activations : xres n = fscale ( ures n , sn ) = sn xres xres = [ 1 , xres where n ] represents the final calibrated residual feature , and fscale is the channel - wise multiplication . 
therefore , the used 3d se - resnext is reliable and effective in learning high discriminative features to classify malignant and benign nodules from raw ct images automatically . nodule classification network architecture the network for lung nodule classification based on 3d seresnext is shown in fig.5. 
finally , the predicted malignant probability ( pmp ) of each lung nodule can be acquired after the softmax . experiments andresults the proposed method was evaluated on the luna16 database with 1004 ( 554 benign and 450 malignant ) nodules . 
for each fold , nine subsets were selected for training and one subset for testing . for nodule - level experiments , a binary classification was performed by calculating the average level for each selected nodule and defined that if the final average level is equal to 3 , it is considered to be uncertain about malignant or benign nodules and hence is removed . 
besides , the se - resnext also achieved a better performance than se - resnet with the best classification accuracy of 91.67%. an additional way of measuring the performance of the proposed method was used . 
it was observed that the predicted malignant probability of each nodule was greatly consistent with the average diagnosis level . discussion in this paper , a novel cadx scheme for lung nodule classification with ct images is presented . 
the number below each nodule is shown as predicted malignant probability , the average malignancy level of four professional radiologists and the nodule diameter ( mm ) proposed method achieves promising performance with a classification accuracy of 91.67% and auc of 0.9563. 
to further illustrate the superiority of the proposed method in the diagnosis of lung nodules , several existing stateofthe art methods based on handcrafted features and deep features are selected for comparison as follows . comparison oftheproposed method withother methods based onhandcrafted features table2 provides a comparison of our method with stateof - the - art methods based on handcrafted features and various classifiers . 
though the classification accuracies achieved were promising , only using one kind of handcrafted feature is unwise , which might affect the generalization ability of classifiers , especially when worked on different public databases . 
besides , few training data were used in [ 36 ] and the auc value was not given . table 2 comparison of the proposed with other methods based on handcrafted features authors year feature ( s ) classifier ( s ) database samples auc accuracy ( % ) akram etal . 
though several proposed methods achieved promising classification accuracies , the performance was uncertain when using different databases . comparison oftheproposed method withother methods based ondeep features the major advantage of deep learning techniques is the ability to learn high discriminative features from various raw ct image automatically . 
the 3d mc - cnn proposed in [ 23 ] was based on cnn and it was optimized with the multi - crop pooling strategy which cropped different regions from convolutional feature maps and then applied max - pooling different times . 
the proposed 3d cnns in [ 33 ] , by contrast , achieved a high auc than 2d cnns and mtanns , because 3d cnns can encode richer spatial information from ct images to learn more distinguishable features . 
the 2d resnet used in [ 25 ] focused on feature reusage to reduce the feature redundancy with the skip connection , but it was limited to explore new features . 
it was better at exploring new features but it might suffer from feature redundancy due to its densely connected mechanistherefore , the classification accuracies achieved by resnet and densebtnet were lower than dpn , which integrated the advantages of resnet for feature reuse and densenet for exploring new features . 
 [ 31 ] proposed the 2d dsdae for nodule classification , but the experiments were performed on private database , which prevented the replication of the results for comparison . analysis oftheproposed methods performance in the handcrafted feature - based cadx systems , extracting and choosing features are time - consuming and complex . 
deep learning techniques have strong ability to boost feature discriminability of lung nodules automatically , and the learned features have the potential in maintaining a sustainable and reliable performance on the ever - changing database . 
 the se - resnext integrated the advantages of resnext for feature reuse and senet for feature recalibration , showed a table 3 comparison of the proposed with other methods based on deep features authors method ( s ) database samples auc accuracy ( % ) shen etal . 
experimental results demonstrate that the proposed method is robust in the nodule diagnosis task and it has the potential to help radiologists to interpret diagnostic data and make decision . conclusion in this paper , we develop a novel cadx scheme for lung nodule malignancy classification with ct images . 
 experimental results on the luna16 database demonstrate that the proposed method achieves a promising performance with an auc of 0.9563 and accuracy of 91.67% , which are more accurate than current methods based on traditional features and deep features . 
the imaging protocol included a dual - energy acquisition ( hd - dect , 90 / 150snkvp ) and fast , lowdose , long - pitch ct , dual - source scan at 100snkvp ( ldct )  . 
subjective ( likert scales ) and objective ( signal - to - noise and contrast - to - noise ratios , snr and cnr ) analyses were performed ; radiation dose and acquisition times were recorded . 
qualitative analysis demonstrated significant reduction in motion artifacts ( p = 0.031 ) with comparable diagnostic reliability between hd - dect and ldct . conclusions ultra - low - dose , dual - source , fast ct protocol provides highly diagnostic images for covid - 19 with potential for reduction in dose and motion artifacts . keywords covid - 19 2019 - ncov dual - source ct spectral shaping low - dose ct chest radiology introduction in december 2019 , a pneumonia of unknown origin outbreak in wuhan , hubei province ( china ) ; the responsible pathogen was identified as the novel coronavirus ( 2019ncov ) , and the related pulmonary syndrome was named as covid - 19 ( coronavirus disease 2019 ) by the world health organization ( who ) [ 1 , 2 ]  . 
common presenting * alessandra borgheresi alessandra.borgheresi@gmail.com 1 department ofclinical , special anddental sciences , university politecnica delle marche , ancona , an , italy 2 division ofspecial andpediatric radiology , department ofradiology , university hospital umberto i lancisi salesi , via conca 71 , 60126ancona , an , italy clinical symptoms are fever and cough in addition to other unspecific symptoms including , fatigue , dyspnea , muscle soreness and headache [ 3 ]  . 
intriguingly , a small percentage ( 5% ) case is asymptomatic ( i.e. , with normal body temperature or minor discomfort ) [ 4 , 5 ] , while reverse - transcription polymerase chain reaction ( rt - pcr ) from swab samples has demonstrated high specificity but relatively low sensitivity ( 6070% ) [ 6 , 7 ]  . 
therefore , the rt - pcr from swab samples is still the standard of reference in the diagnosis of covid - 19 , while unenhanced , high - resolution chestcomputed tomography ( ct ) has a central role in detection , diagnosis and follow - up of the disease [ 810 ]  . ct is a widely available technique allowing for highquality and standardized evaluation of the lung parenchyma . 
to reduce motion artifacts in uncooperative patients ( e.g. , pediatric patients or patients with dyspnea ) , fast acquisitions are obtained by lowering the rotation time of the tube - detector system with high pitch and wide collimation values [ 12 ]  . 
the dualsource ct scanners ( dsct , siemens healthineers , erlangen , germany ) are equipped with two asymmetrical tubedetector systems ( i.e. , different scan field of view , fov ) , mounted in the gantry with an offset of ~ 90 . 
the two tubedetector systems work at different kvp settings for dualenergy acquisitions or at the same kvp setting for ultrafast acquisitions at long pitch ( pitch 1.53 , flash or turbo flash mode , siemens healthineers , erlangen ) [ 14 , 15 ]  . 
moreover , the x - ray tubes in the secondand third - generation scanners ( respectively , the somatom flash and force , siemens healthineers , erlangen ) have additional tin filtration [ 16 , 17 ]  . 
in particular , the more aggressive tin filtration in the somatom force provides the best spectral separation in dual - energy ( dect ) acquisitions by increasing the mean energy of high - kvp spectrum ( i.e. , 150snkvp ) [ 17 ]  . 
moreover , the spectral shaping with tin filter ( i.e. , 100snkvp ) allows for reduction in the low - energy component of the x - ray spectrum , leading to significant dose reduction [ 18 , 19 ]  . 
coupling an ultra - low - dose , fast , long - pitch dual - source acquisition with spectral shaping may be of relevant value in serial evaluations in dyspneic or coughing patients with covid - 19 . the aim of this work is to test the feasibility , with subjective and objective analysis , of an ultra - low - dose , fast , longpitch , dual - source acquisition on third - generation dsct ( somatom force , siemens healthineers , erlangen ) for the lung evaluation in patients affected by covid - 19 related pneumonia . materials andmethods ethical standards this study was approved by the local ethical board , and the informed consent was not collected in written form because of the specific disease . patient population inpatients > 18 years old , positive for covid - 19 of the upper respiratory tract swab from the division of infectious disease , referred to the department of radiology for a chest high - resolution ct between feb 24 , 2020 and march 4 , 2020 , with nobasal chest x - ray performed , were prospectively included to be scanned on the thirdgeneration dsct ( somatom force , siemens healthineers )  . 
patients with pneumonia other than covid - 19 , or with contraindication to ct were excluded . image acquisition andreconstruction the imaging protocol on the third - generation dsct ( somatom force , siemens healthineers , erlangen ) was composed by a spiral high - resolution dual - energy acquisition ( hd - dect ) and by an ultra - low - dose acquisition ( ldct ) in deep inspiration when possible ; no contrast material was administered . 
in the ultra - lowdose , fast acquisition ( ldct ) , both the tubes worked at 100kvp with 0.6 - mm tin filter ( 100snkvp ) , with a wide collimation ( 2 192 0.6mm ) , a rotation time of 0.25s , an ultra - long pitch ( pitch = 3 , turboflash mode , siemens healthineers ) , with modulated ma at 180 mas reference . both the hd - dect and ldct datasets were reconstructed with the available iterative reconstruction algorithm admire , strength 4 ( advanced modeled iterative reconstruction , siemens healthineers , erlangen )  . 
the lung parenchyma was reconstructed with sharp kernels ( hd - dect : bl64 ; ldct : bl57 ) , with linear blending of 0.7 at slice thickness / spacing of 1.5 / 1mm and a window / level of 1200 / - 600 hu ( named lung images , lung )  . 
the mediastinal structures were evaluated with softer kernel ( br40 for both acquisitions ) with linear blending of 0.7 , slice thickness / spacing of 3 / 1.5mm and a window / level of 350 / 50 hu ( named mediastinal images , med )  . 
sagittal and coronal reconstructions were obtained . dect datasets were reconstructed with different linear blending ratios ( blending ratio 0.2 ) in order to reduce beam - hardening artifacts in uncooperative patients on a dedicated workstation ( syngo.via va20 , dual energy , siemens healthineers , erlangen )  . 1 3 la radiologia medica ( 2020 ) 125 : 365373 radiation dose evaluation andacquisition time the ct dose index ( ctdivol ) and dose length product ( dlp ) for each scanned patientwere recorded . 
 [ 22 ] based on the following formula : ed = dlp k finally , the acquisition ( exposure ) times for hd - dect and ldct were recorded . subjective image analysis two independent radiologists with 15 and 10 years of experience evaluated the quality of the ct images on a pacs workstations ( picture archiving and communication system ; centricity radiology , ge healthcare , milwaukee ) , after removing personal and technical data from the images . 
the lung parenchyma and airways were evaluated on lung images , while the mediastinal structures ( e.g. , lymph nodes ) were evaluated on the mediastinal images , in hd - dect and ldct . the subjective analysis was performed by using 5 - points likert scale and included three sections : general quality of the image ( mediastinum and lung images ) , anatomical structures ( lung images ) , pathological findings ( lung or mediastinal images )  . the evaluation of general quality included the following parameters and scales : 1 . 
sharpness , where sharpness was rated as : 1 = unacceptable , 2 = significantly reduced with blurring of adjacent structures , 3 = minimally reduced sharpness with blurring of adjacent structures , 4 = sharpness minimally reduced , 5 = excellent sharpness ; 2 . 
small anatomical structures ( bronchi < 2mm and septae ) ; in both cases , the likert scale was defined as follows : 1 = unacceptable ( landmarks not visible ) ; 2 = poor ( < 25% landmarks visible ) ; 3 = fair ( 2575% landmarks visible ) ; 4 = good ( > 75% landmarks visible ) ; 5 = excellent ( all landmarks visible )  . finally , a third radiologist ( 10 years of experience ) detected main lung pathological findings related to covid - 19 on hd - dectlung and hd - dectmed images and the other two radiologists were asked to evaluate the same finding on the ultra - low - dose acquisitions , in particular : 1 . 
lymph nodes ( on hd - dectmed ) ; the relative likert scale was set as follows : 1 = finding not detected ; 2 = barely detected , unreliable interpretation ; 3 = visible finding with marked blurring and uncertain interpretation ; 4 = visible finding , blurred , with no influence on diagnosis ; 5 = finding clearly visible with good demarcation . objective image analysis signal - to - noise ratio ( snr ) and contrast - to - noise ratio ( cnr ) were evaluated by the third radiologist ( 10years of experience ) by placing 1 0.05cm2 circular region of interest ( roi ) for the following structures : 1 . 
hd - dectmed and ldctmed : descending aorta , trachea , paraspinal muscle . the evaluation of anatomic structures included the parameters : snr and cnr were calculated considering average and standard deviation ( sd ) of the hu from the placed roi as follows [ 13 ] : 1 3 368 la radiologia medica ( 2020 ) 125 : 365373 snr = |average huanatomical structure sdanatomical structure results |average huanatomical structure average hufat cnr = sdfat statistical analysis quantitative parameters were expressed as median and interquartile ranges ( 2575p , iqr )  . 
a dedicated statistical software was used ( medcalc v19.1.6 , medcalc software , ostend , belgium )  . table 1 main radiological findings in 10 covid - 19 positive patients patient population andradiological findings onct in this study were included 10 patients ( m / f = 7 / 3 ) with a median age of 53 ( iqr : 4783 ) and a median bmi of 28 ( iqr : 2630 )  . 
two of 10 patients ( 20% ) had a bmi > 30 and 3 / 10 ( 39% ) had severe symptoms ( temperature > 38c , dyspnea and respiratory failure ) and were not able to maintain the arms raised during the ct examination . 
the radiological findings of each patient at presentation are summarized in table1 and are comparable to those previously reported [ 8 ]  . radiation dose andacquisition time table2 summarizes the applied radiation dose and acquisition time . 
the beam - hardening artifacts minorly affected the 100sn kv . discussion in the present study , we included a small sample of patients affected by covd - 19 - related pneumonia with variable clinical and radiological manifestation of the disease , and comparable findings described in the literature [ 8 , 9 ]  . 
c , e have a linear blending of 0.7 while d , f have linear blending of 0.2 resulting in reduction in artifacts in mediastinum ( d ) and left lung parenchyma ( f ) as sars and mers ( which demonstrated the development of air trapping and fibrosis [ 21 ] ) , the presence of air trapping was searched in the first three cases , with negative results and thus not investigated any more . 
further studies on follow - up of covid - 19 should be performed to clarify possible chronic lung injuries . 1 3 la radiologia medica ( 2020 ) 125 : 365373 fig . 
c , d demonstration of reverse halo and linear opacities in hd - dect and ldct in these10 patients with covid - 19 , we evaluated the feasibility of an ultra - low - dose , long - pitch , dual - source , fast ct acquisition to be implemented for serial follow - up examinations in symptomatic patients with covid - 19 . 
at baseline , a dect acquisition was chosen as internal reference standard . previous studies in the literature demonstrated significant dose reduction with spectral shaping in chest ct , achieving a dosecomparable to a chest x - ray examination [ 12 , 13 , 18 , 19 , 23 , 24 ]  . 
in our population , the effective dose of the ultra - low - dose , long - pitch , dual - source fast acquisition was comparable to the values reported in previous studies and close to a chest x - ray examination . 
in these patients , chest x - ray examination at baseline was not performed to avoid unnecessary radiation exposure . the rationale behind the dect choice was to couple a relatively fast acquisition ( 22.5s ) with the possibility of postprocessing for eventual artifact reduction with different blending combinations in uncooperative patients unable to maintain arms raised . 
the feasibility , the quality and the diagnostic performance of ultra - low - dose chest ct with spectral shaping , and other technical solutions have already been demonstrated [ 12 , 13 , 18 , 19 , 24 ] sometimes with questionable results about the pathological findings [ 25 ]  . 
to our knowledge , this is the first study evaluating a long - pitch , dual - source acquisition with spectral shaping in acute setting in patients with covid - 19 . 
as expected from a low - dose acquisition , the ldct images had trend , though poorly significant , to be evaluated as more noisy than the hd - dect images ( table4 )  . 
again , this can be explained by considering the relatively high mean energy of the 100snkvp spectrum contributing to lowering the noise together with the radiation dose ( table2 , fig.2 ) [ 19 ]  . 
moreover , in this protocol , the reconstructions have been kept as similar as possible , in particular the slice thickness , the slice spacing and the iterative reconstructions while for ldct a slightly softer kernel was used . 
the small size of the sample did not allow for more sophisticated statistical analysis , such as inter - reader agreement or the relation between bmi , radiation dose and image quality . concluding , a compromise including preserved image sharpness within lung parenchyma , with minimally blurred mediastinal structures in the face of a median dose reduction of more than 90% may be acceptable when performing serial ct controls in severely ill young patients [ 26 ]  . conclusions the study demonstrated the feasibility of an ultra - lowdose , fast chest ct acquisition with spectral shaping at 100kvp ( 100snkv ) and dual - source acquisition with ultra - long pitch ( turbo flash , siemens healthineers ) in patients affected by covid - 19 with good diagnostic reliability and potential for reduction in radiation dose and motion artifacts . funding this study was not supported by any funding . compliance with ethical standards conflict of interest a.a. 
the lesions were classified visually and also based on the peak of llcr into the following groups : ( 1 ) early arterial , ( 2 ) middle arterial and ( 3 ) late arterial . 
based on the peak of llcr , 17 ( 55% ) fnhs were classified into early , 11 ( 35% ) in middle and only 3 ( 10% ) in late arterial phase groups . 
there was a good agreement between qualitative analysis and llcr in 85% of cases . conclusion the optimal visualization of fnh has been detected in early and middle arterial phases while hcc has been best observed during middle and late arterial phases . keywords multiple arterial phase hepatocellular carcinoma ( hcc ) focal nodular hyperplasia ( fnh ) magnetic resonance imaging gadoxetic acid * marco gatti marcogatti17@gmail.com 1 department ofsurgical sciences , radiology unit , university ofturin , via genova 3 , 10126turin , italy 2 department ofoncology , radiology unit , university oftorino , turin , italy 3 department ofradiology , university ofbrescia spedali civili , p.le spedali civili 1 , 25123brescia , italy 4 division ofinterventional radiology , department ofradiology , madonna delle grazie hospital , 75100matera , italy 5 school ofmedicine , university ofmilano - bicocca , milan , italy 6 department ofdiagnostic radiology , h . 
gerardo monza , via pergolesi 33 , 20900monza , mb , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 348355 introduction materials andmethods in the last few years , magnetic resonance imaging ( mri ) has become by far one of the best non - invasive imaging modality for detection and diagnosis of focal liver lesions [ 1 , 2 ]  . 
recently , several new imaging techniques have been developed in order to further improve mri diagnostic accuracy , such as diffusion - weighted imaging , multiple arterial phase imaging , hepatobiliary mri using contrast agents , perfusion mri , magnetic resonance elastography and radiomics [ 3 ]  . the enhancement pattern is a key feature that allows the differential diagnosis of different hepatic lesions ; according to the international guidelines , the arterial phase hyperenhancement is essential diagnostic criteria for many hypervascular lesions such as hepatocellular carcinoma , hepatocellular adenoma , focal nodular hyperplasia and hypervascular metastasis [ 1 , 2 ]  . the use of gadoxetic acid is increasing and progressively changing the standard of diagnosis of hepatic lesions [ 4 ]  . 
 several studies proposed some tips in order to obtain the optimal timing for arterial phase and consecutively high lesion - to - liver contrast [ 5 , 6 ] , such as lowering the contrast injection rate ( 1ml / s ) , doubling the injected dose and diluting the contrast agent created prolonged aortic enhancement . 
moreover , multiphase arterial imaging technique compared to conventional single arterial acquisition provides more adequate [ 7 ] and robust [ 8 ] images with less artefacts [ 9 ]  . for both hepatocellular carcinoma [ 2 ] and focal nodular hyperplasia [ 1 ] , the arterial hyperenhancement is major diagnostic criteria . 
1 study design flow chart la radiologia medica ( 2020 ) 125 : 348355 flush injection at the same flow rate using an automated injector ( spectris solaris ; medrad warrendale , pa )  . 
a triple arterial phase with a t1 high - resolution isotropic volume examination ( thrive ) contrast - enhanced timing robust angiography ( centra ) keyhole sequences with spir fat suppression was acquired using the bolus tracking technique . 
all the rois were selected among the arterial phases . the lesions were categorized based on the peak of llcr into three groups : ( 1 ) early arterial , ( 2 ) middle arterial and ( 3 ) late arterial . 
the outcome of the qualitative analysis was then compared to the reference standard of llcr . two representative cases are shown in fig.4. statistical analysis continuous variable ( cer and llcr ) did not pass the shapirowilks normality test and thus were expressed as median , first quartile q1 and third quartile q3 . 1 3 la radiologia medica ( 2020 ) 125 : 348355 fig . 
3 lesion - to - liver contrast ratio ( llc ) was calculated with the following formulas : llcrlesion n = ( silesion nsiliver n ) siliver n 100  . 
non - contrast ( a ) , early ( b ) , middle ( c ) and late ( d ) and siliver is the mean signal intensity of a roi placed in the healthy liver parenchyma in the n arterial phases the existence of statistical difference between matched data was investigated with nonparametric test : wilcoxons test for n = 2 correlated variables and friedmans test for n > 2 . 
categorical variables , reported as counts and percentages , were arranged in cross - correlation tables and studied with the 2 test ( with yates correction for 2 2 ) or fishers exact test . concordance between readers was estimated by cohens coefficient k with linear weighting . statistical significance was set at two - tails p < 0.05. 
in the fnh group , 15 ( 68% ) patients with one lesion , 5 ( 23% ) patients with two lesions and 2 ( 9% ) patients with three lesions were identified . 
top panel : a 68 - year - old woman with hcv infection and a hypervascular liver lesion ( hepatocellular carcinoma ) in the segment iv / viii ; the lesion enhancement increased qualitatively and quantitatively throughout the arterial phases . 
these results are in line with our cer analysis , although we should consider the possible effect of mean age and gender differences between two groups : younger and healthier people usually have a better cardiac function , while the older cirrhotic population tends to have a higher arterial perfusion that may compensate the lower blood flow . 
the llcr analysis presented a significant difference between hcc and fnh in the early arterial phase with higher value for fnh , which is related to the different behaviour during three arterial phases . 
 [ 10 ] highlighted the role of double arterial phase to improve detection of hypervascular hccs and to reduce false - positive lesions : in their study , the results of late arterial imaging were more consistent than the early and it was shown that when the late arterial phase images were appropriate enough , the early arterial phase images could be eliminated . 
moreover , in the llcrhcc there was a significant increase between early and middle phase ( p = 0.009 ) , whereas in the llcrfnh , there was a decrease between the middle and the late phase ( p = 0.004 ) the llcr analysis revealed a more visible arterial enhancement in early arterial phase for fnh compared to hcc , but more importantly , the best phases for optimal visualization of fnh were the early and middle arterial phases , whereas for hcc were the middle and late arterial phases . several hemodynamic changes have been known in cirrhosis , particularly a decrease in portal perfusion due to an increase in intrahepatic vascular resistance partially compensated with the arterial perfusion . 
 [ 17 ] showed that ct perfusion and in particular the 1 3 354 la radiologia medica ( 2020 ) 125 : 348355 hcc detection using triple arterial phase mri , with results comparable to those of whole triple arterial phase imaging . furthermore , our results were in line with the literature regarding fnh . 
 [ 14 ] demonstrated a higher visual signal intensity of fnh in early arterial phase and a higher llcr in the first two arterial phases using an extracellular agent ( gadoteric acid )  . these vascular patterns could reflect the different pathogenesis and angioarchitecture of hcc and fnh . 
because of the malignant nature of hcc , neovascularisation is induced by hypoxia during tumour growth and newly formed tumour vessels are structurally and functionally abnormal compared to normal blood vessels [ 18 ]  . 
differently , fnh is characterized with anomalous arteries located in fibrous septa , that is otherwise histologically normal [ 19 , 20 ]  . the concordance ( 85% ) between qualitative and quantitative analysis stressed out the importance of triple arterial phase imaging also in improving the qualitative detection of hypervascularity , which is a prominent factor in the clinical setting , as the diagnosis of focal liver lesion is mainly qualitative [ 1 , 2 ]  . from a clinical point of view , this study suggests to acquire a multiple arterial phase mr imaging in case of hcc and fnh lesions and if not possible , it is essential to be aware of the pre - test condition of the patient . 
moreover , the use of a multiple arterial phase acquisition technique could be useful to increase the detection rate of hepatic lesion and to reduce the artefacts in the arterial phase providing adequate arterial phase imaging for gd - eob - dtpa liver mri [ 7 , 9 ]  . nevertheless , this study has some limitations ; first , it is a retrospective study carried out in a single centre on a limited number of patients . 
third , due to the lack of histopathological analysis , it is not evident whether the different subclasses of hcc were associated with the degree of malignancy or not ; it was described that in the advanced stage of cancer the arterial blood supply significantly decreased in all arterial phases . in conclusion , this study highlighted the different arterial enhancement patterns of hcc and fnh . 
fnh was more evident during early arterial phase and was best visualized in early and middle arterial phases , whereas hcc was best observed in middle and late arterial phases . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standard all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . la radiologia medica ( 2020 ) 125 : 416422 neuroradiology investigating dynamic susceptibility contrastenhanced perfusionweighted magnetic resonance imaging inposterior fossa tumors : differences andsimilarities withsupratentorial tumors simonagaudino1 massimobenenati1 , 2 antoniomarrazzo1 , 2 antoniaramaglia1 , 2 giammariamarziali1 , 2 pamelaguadalupi1 , 2 cesarecolosimo1 , 2 matiamartucci3 annibalebotto4 amatoinfante5 received : 10 august 2019 / accepted : 27 december 2019 / published online : 8 january 2020 italian society of medical radiology 2020 abstract purpose to assess the accuracy of dynamic susceptibility contrast - enhanced perfusion - weighted magnetic resonance imaging in glioma grading and brain tumor characterization of infratentorial tumors , and to investigate differences from supratentorial tumors . methods this retrospective study , approved by the institutional review board , included 246 patients with brain tumors ( 184 supratentorial , 62 infratentorial ) , grouped by tumor type : high - grade gliomas ( hgg ) , low - grade gliomas ( lgg ) , metastases ( met ) , and primary central nervous system lymphoma ( pcnsl )  . 
the main differences were the optimum threshold rcbv values ( 3.04 for supratentorial , 1.77 for infratentorial tumors ) and the mean psr , which was significantly higher in lgg than in hgg in supratentorial ( p = 0.035 ) , but not infratentorial gliomas . 
proper cutoff values were important in the accuracy of perfusion - weighted imaging in posterior fossa tumors . keywords brain tumors gliomas dynamic susceptibility contrast mri ( dsc ) perfusion - weighted mri ( pwi ) supratentorial infratentorial * massimo benenati dr.massimo.benenati@gmail.com introduction 1 uoc radiodiagnostica e neuroradiologia , dipartimento di diagnostica perimmagini , radioterapia , oncologia ed ematologia , fondazione policlinico universitario a . 
 gemelli irccs , rome , italy istituto di radiologia , universit cattolica del sacro cuore , rome , italy 3 uoc di neuroradiologia , azienda ospedaliera universit di padova , padua , italy 4 uoc di neuroradiologia , aou s . 
 however , with conventional mri alone , it can be challenging to characterize and differentiate brain tumors , due to considerable overlap in different tumor features [ 2 ]  . 
this technique detects signal changes that occur when vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 416422 paramagnetic contrast agents pass through the cerebrovascular system [ 3 ]  . 
in fact , it was demonstrated that mri measurements of relative cbv ( rcbv ) correlated with both conventional angiographic assessments of tumor vascular density and histologic measurements of tumor neovascularization [ 4 , 5 ]  . 
however , due to overlapping rcbv values in some malignant brain lesions , newer hemodynamic variables , such as the percentage of signal recovery ( psr ) , are currently used in differentiating brain tumors [ 7 ]  . 
psr represents the percentage of signal intensity recovered at the end of the first pass of contrast agent , relative to baseline ( the signal intensity before administration of contrast ) [ 2 ]  . 
to date , dsc - pwi has been widely used for characterizing supratentorial tumors ( st ) , due to its demonstrated reliability and the availability of validated cutoff values for the differential diagnosis . however , dsc - pwi is used much less frequently for characterizing infratentorial tumors ( it )  . 
this reluctance may arise from the anatomicalfunctional complexity of the posterior fossa ( pf ) and the presence of numerous artifacts , due to the proximity of the lower limits of the coil and the skull base , which distorts dsc perfusion studies that are based on echo - planar imaging . 
as a result , there is little clinical experience in the use of perfusion mr imaging for it , particularly in adult patients , which infrequently present pf neoplasms [ 8 ]  . 
this retrospective study group included all cases of supratentorial and infratentorial low - grade gliomas ( lgg ) , high - grade gliomas ( hgg ) , metastases ( met ) , and primary central nervous system lymphomas ( pcnsl ) , for which optimum perfusion imaging and histological data were available . 
 gliomas were divided into low ( who grades iii ) and high ( who grades iiiiv ) grades [ 9 , 10 ]  . mri protocol mri was performed on a 1.5 t scanner ( signa excite 2 echospeed , general electric medical systems ) , equipped with a sensitivity - encoding eight - channel head coil . 
conventional sequences included axial t2 flair , t1 fse , gradient - recalled echo , t2 fse , and post - contrast t1 fse images in 3 planes and / or 3d - fspgr . 
the parameters were tr / te = 1500 / 35ms , flip angle = 35 , nex = 1 , matrix size = 128 128 , section thickness = 4mm , gap = 0.4ma total of 60 image volumes were acquired . 
at the end of the 10th image volume acquisition , 0.2mmol / kg of gadobenate dimeglumine ( 0.5m , multihance bracco ) was injected with a power injector at a rate of 45ml / s through a 20 - ga or 18 - ga intravenous catheter . 
in all cases , patients received a pre - bolus of 0.05mmol / kg of gadolinium ( 710min before the dynamic phase ) to reduce the t1 effects of bbb disruption . dscpwi image processing data from dsc - pwi were processed using olea sphere software ( v 2.3 olea medical solutions , la ciotat , france ) , based on the singular value decomposition ( svd ) algorithm for deconvolution . 
two neuroradiologists ( with 10 and 4years of experience ) evaluated , in consensus , the color maps of the cbv and the corresponding morphological images ( t2 fse , t2 flair , and post - contrast t1 fse and / or 3d - fspgr ) , automatically coregistrated by performing a transformation of the datasets . 
based on those 1 3 418 la radiologia medica ( 2020 ) 125 : 416422 evaluations , three regions of interest ( rois ) were drawn in the solid areas of lesions that showed the highest cbv values . 
relative cbv ( rcbv ) of the lesions was obtained by normalizing mean cbv values to the cbv values derived from the contralateral normalappearing white matter ( nawm ) in the centrum semiovale . 
psr values were normalized to the contralateral nawm , for st , or the contralateral middle cerebellar peduncle , for it . statistical analysis lesions were divided into two groups according to their location : st or it . 
in addition , rcbv was evaluated for accuracy , sensitivity , specificity , table 1 number of tumors in different subgroup classes based on location and histology ; n = 246 metastasis high - grade gliomas low - grade gliomas primary cns lymphoma infratentorial supratentorial total ppv , and npv based on receiver operating characteristic ( roc ) curves for distinguishing between lgg and hgg in the overall population and in the st and it subgroups . 
 for rcbv and psr , the cutoff value was assessed through the analysis of receiver operating characteristic curve ( roc curve )  . mean psr was evaluated for accuracy , sensitivity , specificity , ppv , and npv , based on roc curves for distinguishing between hgg and met , between hgg and pcnsl , and between pcnsl and met in the overall population and in the st and it subgroups . a 1 - way anova with logistic analysis was performed to compare the rcbv and psr with these parameters ( location , histology , and grading ) , and where useful , bonferronis post hoc correction was applied to study each single variable correlation . 
a p - value less than 0.05 was the criterion for significance . results characteristics features independent from tumor location , perfusion parameters in the four lesion subgroups showed characteristic features . 
1 mean psr curves : a mean psr curve in a met , which shows approximately 40% of recovery ; b mean psr curve in a hgg ( proved to be gbm on histopathology ) , which shows approximately 75% of recovery ; c mean psr curve in a pcnsl , which shows overshoot from baseline 1 3 la radiologia medica ( 2020 ) 125 : 416422 fig . 
abbreviations : relative cerebral blood volume ( rcbv ) , high - grade gliomas ( hgg ) , low - grade gliomas ( lgg ) , area under the curve ( auc ) , positive and negative predictive values ( ppv and npv , respectively ) 1 3 420 la radiologia medica ( 2020 ) 125 : 416422 we tested different rcbv threshold values to determine the effect of the cutoff value on rcbv sensitivity and specificity in each location ( st + it , st , and it )  . 
among supratentorial gliomas , mean psr was significantly higher for lgg than for hgg ( p = 0.035 ) ( table2 )  . we examined the accuracy of the mean psr values in differentiating between hgg , met , and pcnsl , in different brain locations ( table5 )  . mean psr values were significantly different between hgg and met and between pcnsl and met , independent of the location . 
 table 4 relative cbv sensitivity and specificity for differentiating hgg from lgg with different rcbv cutoff thresholds threshold sensitivity ( % ) specificity ( % ) st + it a . 
met st + it from threshold mean psr values were derived receiver operating characteristic ( roc ) curve analyses , which included the overall population of tumors ( st + it ) , supratentorial tumors ( st ) , and infratentorial tumors ( it ) mean psr values were not significantly different between hgg and pcnsl . we calculated the optimum threshold , sensitivity , and specificity for the mean psr in differentiating hgg and pcnsl from met . 
those comparisons that did not show a good accuracy were not reported ( table6 )  . discussion this study was the first to demonstrate the accuracy of dsc - pwi in assessing infratentorial malignant brain tumors . 
these features should be taken into account in grading primary brain tumors and in table 6 optimum thresholds , sensitivities , and specificities for mean psr in differentiating hgg and pcnsl from met threshold sensitivity ( % ) specificity ( % ) hgg vs . 
dsc - pwi allows assessment of two main parameters , rcbv and psr , whose roles in brain tumor grading and differentiation were clearly demonstrated in previous studies [ 2 , 13 ]  . 
nevertheless , this technique is susceptible to artifacts , in particular in the pf , where skull base structures ( e.g. , boneair interfaces in the mastoids ) distort the magnetic field , and the lower limit of the coil reduces the quality of the signal ( lower s / n ratio ) [ 6 , 8 ]  . 
our results confirmed the importance of these parameters , and we also demonstrated that both rcbv and psr could be applied in pf tumor grading and differentiation . however , we found that rcbv and the differentiation thresholds depended on location . 
thus , tumor location should be considered , when interpreting dsc - pwi results . first , we found higher rcbv values in st compared to it , even when specific subgroups were compared between the two locations . 
consequently , the cerebellum and brainstem have relatively higher cbf / cbv ratios , physiologically , compared to the cerebral cortex and the deep white matter [ 15 ]  . second , we detected a large difference in the rcbv thresholds for glioma grading , between the st and the it . 
the explanation probably relies on the fact that our subgroup of hgg included glioblastomas ( grade iv in the who classification ) , which might be expected to increase the mean rcbv values in cerebral hemispheres , where they occur with high frequency . 
of note , the accuracy of the rcbv threshold for brain tumor grading is highly important in the pf , because performing a pf biopsy is often difficult or impossible , and neuroradiological grading represents the only possibility for defining the aggressiveness of the lesion and selecting the appropriate treatment strategy . 
to confirm that the tumor location could affect the interpretation of results , we applied the three different optimal rcbv thresholds to the overall population , to the st , and to the it ( table4 )  . 
however , we did not find significant differences in mean psr between pcnsl and hgg , probably because many of our hgg were who grade iii gliomas , which showed high psr . 
therefore , although the entity that psr represents remains unclear ( even in the more recent literature ) , psr thresholds could be considered reliable in the differential diagnosis of brain tumors , even in the pf . 
however , our finding that the psr values were relatively higher in all st suggests that psr isin some wayalso related to vascularization . the major limitations of this study were the relatively small population size ( above all , the number of pcnsl in the pf group ) , the monocentric setting , and the lack of molecular features analysis , which were recently introduced in the revised who 2016 classification of tumors of the cns . 
another limit is due to the dsc gradient - recalled t2 * - weighted echo - planar imaging sequence , which is susceptible to artifacts , especially in the pf , and whose reproducibility is limited by technical inhomogeneities , mainly due to the lack of standardized acquisition protocols and different software available for post - processing [ 20 ]  . 
hence , homogenizing these variables ( single scanner , same acquisition protocol , and post - processing software for all tumors ) , we attempted to increase the reproducibility of the data . 
the defect volumes were estimated by point counting ( pc ) , manual segmentation ( ms ) and semiautomatic segmentation ( sas ) methods at 0.3 - mm section thickness without any intersection gap . 
both ms and sas are valid methods for volume estimation ; however , sas may be preferred due to its practicability . keywords cone beam computed tomography quantitative evaluation femur dentistry computer - assisted image analysis introduction cone beam computed tomography ( cbct ) was developed to be an alternative equipment to computed tomography in order to own a cheaper device and acquire images faster . 
the volume estimation accuracy of cbct was demonstrated via the goldstandard methods in several studies [ 5 , 6 ]  . stereological techniques , such as the cavalieri principle , can estimate the volume of any anatomical structure in living organisms . 
then , the total area of the constructed sections and the distance between each consecutive section are multiplied , and the volume of the related object can be practically estimated . 
after that , the points overlapping the counting grid are counted and the volume is estimated by multiplying the section thickness and the estimated total area [ 11 , 12 ]  . with the use of image - guided diagnosis , operators have become familiar with segmentation processes . 
for example , the density scale of a particular tissue or organ may not be limited to a specific range , or the density of adjacent tissue may overlap with the density of the investigated tissue . 
in other words , it may not be possible to distinguish the whole part of any specific tissue from surrounding tissues by using the threshold process alone [ 13 , 14 ]  . 
to the best of our knowledge , there has been no study comparing the efficacy of the pc , ms , and semiautomatic segmentation ( sas ) methods to measure the volume of bone defects on cbct images yet . 
this study will serve the purpose of testing the efficiencies of the traditional stereological methods and the sas method , which is more commonly used in the current clinical practice , in volume measurement . 
by this way , the feasibility of the use of traditional stereological methods in clinics deprived of special software to apply the sas method will be tested with the help of cbct images . in this study , via cross - sectional images of scanned intraosseous defects captured using the cbct , pc , ms , and sas methods were used to estimate the defects volumes . 
all institutional and national guidelines for the care and use of laboratory animals were followed . firstly , femur condyles were cut with a grinding machine to obtain hat - shaped bone covers . 
in addition , the bones were placed into the plexiglass during image acquisition to represent soft tissue . the defects were scanned with a tomography device ( kodak cs 9300 cone beam 3d system , kodak dental systems , carestream health , inc . , rochester , ny , usa )  . 
 during bone defect scanning , 90kvp , 4ma , 0.3mm voxel size , 17 13.5cm field of view ( fov ) , 11.30s scan time , and 360 rotation features were used . 
in the software , the images of the defects were cross - sectioned at a width of 0.3mm and the cross - sectional images were consecutively sorted to form an image stack . 
a square grid system available in the software was applied on the images , and each structure in the form of a small dashed square on the grid was determined as a single point . 
the point counting grid belonging to software was randomly applied to sectional images , and overlapped points with the surface area of bone defect were counted by an examiner on each section . 
when the volume on the pc method was estimated , the result can be demonstrated by the formula : where v is the volume , t is the section thickness ( including intervals ) , a ( p ) is the unit area between four points , and p is the number of overlapped points in each sections counting grid [ 15 ]  . 
the t value of our study has already been determined ; a ( p ) value , on the other hand , was set in the relevant software ; the p value was calculated by counting the points corresponding to bone defects on each cross section . 
all data were recorded in a spreadsheet of microsoft excel ( microsoft , redmond , usa ) , and the final volume result of bone defects was obtained by using the formula mentioned above . manual segmentation method firstly , sectional images of defects were converted to dicom format and imported into imagej software ( us national institutes of health , bethesda , maryland , usa )  . 
 a stack with consecutive continuity was formed by means of the software using the cross - sectional images with a crosssectional width of 0.3mm. the boundaries of each defect were delineated by the examiner who performed the pc volume estimates with a mouse pointer on each section manually . 
the volume is estimated in the ms method using the formula : v = t a where t is the section thickness ( including intervals ) and a is the total of bounded cross - sectional areas [ 15 ]  . 
cavalieris principle - based formulas have been performed to estimate bounded areas using the pc and ms methods . 1 3 la radiologia medica ( 2020 ) 125 : 398405 fig . 
4 a , b applied semiautomatic segmentation method on cross - sectional image and c three - dimensional modeling of intraosseous defect areas were estimated by the software , the obtained data were recorded in a spreadsheet and the volume of bone defects was calculated by the formula mentioned above . semiautomatic segmentation method mouse - controlled pointer where there was any discrepancy in the segmented area between the software and examiner . 
 the volume of the three - dimensional design created using the segmentation process was estimated by the software . the dicom files imported into 3d doctor ( able software corp . , lexington , ma , usa ) software for the segmentation process and a stack with consecutive were formed by means of the software using the cross - sectional images with a cross - sectional width of 0.3mthen , a region of interest ( roi ) contour was drawn around the bone defects on each section from start to finish using the manual tracing method with the help of a mouse pointer . 
while the volume in the sas method was estimated , defect areas were colored by the software at each slice according to density scale , and the borders of the segmented areas were analyzed by the examiner . 
the investigated area was adjusted manually , with widening or restricting of the border conducted at each slice with a archimedes method after all of the volume estimation processes of the defects images were completed , gold - standard measurement results were provided by using archimedes method and the results were compared with the results of the pc , ms , and sas methods . 
initially , silicon - based measurement materials ( speedex heavy body , coltene ag , altstetten , switzerland ) were placed into all bone defects to completely fill thethe pre - prepared covers were placed over the measurement material with no space in between the two before the material was hardened . 
the time spent performing volume estimation for each method was determined as an interval from the first process , importing defect images to related software to the last process , obtainment of volume results . 
in addition , the average time spent performing measurements by the pc , ms , and sas methods was determined and compared . a friedmans two - way analysis of variance test was performed to compare statistically the results of the pc , ms , sas , and archimedes method . 
 according to the friedmans two - way analysis of variance test results , the volume estimation values in ms and sas methods were not statistically different from the values 1 3 la radiologia medica ( 2020 ) 125 : 398405 in archimedes method . 
however , the pc method values were statistically different from the values in archimedes method ( p = 0.768 , p = 0.140 , and p < 0.001 , respectively ) ( table 2 )  . 
a tendency for underestimation was followed in the measurements taken by the pc method . the average time spent during volume measurements of the pc , ms and sas methods was evaluated ( table3 )  . 
by comparing newly developed , automatically computed segmentation techniques with pc and ms methods , there is an opportunity to consider the object border measurement ability of an algorithm - dependent procedure . 
an objects border whose volume is measured by ms can be drawn according to magnetic resonance imagings ( mri ) gray scale and the hounsfield unit ( hu ) in computed tomography ( ct )  . 
as a result , this process is very timeconsuming and prone to measurement errors [ 19 ]  . in cbct devices , viewed pixels may not reflect the objects borders , which are measured according to the partial volume effect . 
segmentation difficulties may be caused by noise and image distortion in the peripheral parts of the scanned volume , the latter of which stems from the cone beam effect [ 1 ]  . 
due to notable noise , different artifact types , conical beam geometry , and a limited viewing field , hu cannot be calibrated in most cbct systems [ 20 ]  . 
in the event that osseous tissue corresponds to any hu value in the automatic segmentation process performed by cbct , it may be possible that equivalent osseous tissues in different locations can correspond to different hu values . 
therefore , the capability and experience of the user are essential to the success of segmentations that are managed by cbct . in case any object is scanned by the same cbct with the same technical parameters twice , captured hu values from the same locations do not represent the same values due to inherent artifacts of cbct [ 21 ]  . 
according to the results , there was a linear correlation between ct and cbct results , and both of these scanning techniques were considered as fairly good predictors for evaluating new bone formation in this study [ 22 ]  . 
however , due to the instability of hu values of cbct , ct with superior hu uniformity should be used for clinical follow - up events . a few studies have studied volume estimation with the cavalieris principle on cbct systems [ 57 ]  . 
analyzing these findings and those of our study , it can be stated that a minimum of 0.3 - mm section thickness , including intervals , should be selected for volume estimation of irregularly shaped objects . 
as clarified by the studies [ 23 , 24 ] , the volume results of irregularly shaped objects obtained from cbct were compatible with the ct and micro - ct results . 
in other words , cbct is a reliable device for measuring the volume of any object . there are also reports where sas was used to estimate the volumes of a molar tooth , a mandibular condyle , and an alveolar socket by using cbct [ 8 , 25 , 26 ]  . 
however , no reference measurements as archimedes method were used [ 27 ]  . in related studies [ 10 , 15 , 18 , 2729 ] , a tendency for underestimation was followed for the pc method compared with the ms , sas , anthropometric and archimedes methods . 
based on these examples , the pc method may be ineffective at measuring the volume of not only irregularly shaped objects , but also regularly shaped objects in some cases . in our study , sas and ms results did not show a statistically significant difference from reference volumes , but pc results did show a significant difference . 
it is clear that other methods overcame the previously mentioned labors . conclusion in conclusion , the volume of irregularly shaped bone defects imaged by cbct at 0.3 - mm section thickness should be estimated by using the sas and ms methods and not the pc method . 
also , it can be stated that the usage of the sas method is more practical for routine clinical volume measurements . authors contribution all authors contributed to the study conception and design . 
all authors read and approved the final manuscript . funding this research did not receive any specific grant from funding agencies in the public , commercial or not - for - profit sectors . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all applicable international , national and / or institutional guidelines for the care and use of animals were followed . 
to avoid the potential bias in studies using a cytological standard of reference , here we aimed to meta - analyze data from studies adopting histological diagnosis as the gold standard . methods a comprehensive literature exploration of pubmed and scopus was conducted . 
pooled sensitivity , specificity , ppv , and npv of ceus were calculated by dersimonian and laird method ( random - effects model )  . results the literature search retrieved 1885 articles , and 14 were included for the study . 
there was publication bias for sensitivity and npv . conclusions ceus reaches good performance in discriminating between malignant and benign thyroid lesions . keywords thyroid nodule carcinoma contrast - enhanced ultrasound ( ceus ) meta - analysis * vito cantisani vito.cantisani@uniroma1.it 1 clinic fornuclear medicine andcompetence center forthyroid diseases , imaging institute ofsouthern switzerland , ente ospedaliero cantonale , bellinzona , switzerland 2 faculty ofbiomedical sciences , universit della svizzera italiana ( usi ) , lugano , switzerland 3 department ofemergency andorgan transplantation , section ofinternal medicine , endocrinology , andrology andmetabolic diseases , university ofbari aldo moro , bari , italy 4 department ofmedico - surgical sciences andbiotechnologies , sapienza university ofrome , latina , italy 5 norwegian psc research center , department oftransplantation medicine , division ofcancer medicine , surgery , inflammatory diseases andtransplantation , oslo university hospital , oslo , norway 6 department ofmechanical andaerospace engineering , sapienza university ofrome , rome , italy 7 department ofradiological sciences , policlinico umberto i , sapienza university , rome , italy 8 department ofbiomedical imaging andimage - guided therapy , medical university ofvienna , vienna general hospital , whringergrtel , vienna , austria 9 department oftranslational andprecision medicine , sapienza university , rome , italy 10 diagnostic radiology institute paula stradina clinical university hospital , radiology research laboratory , university oflatvia , riga stradins university , riga , latvia 11 department ofimaging diagnostics , policlinico umberto i , university sapienza , rome , italy vol :  . ( 1234567890 ) 1 3 la radiologia medica ( 2020 ) 125 : 406415 introduction ultrasound ( us ) is the pivotal tool to detect and characterize thyroid nodules . 
it is worth noting that , at the time of writing , regulatory agencies have still not approved the contrast agents for use in clinical practice in all countries , and this has resulted in limiting the diffusion of thyroid ceus , too [ 9 ]  . 
as a consequence , despite several studies on the reliability of ceus in detecting and excluding malignancy in thyroid nodules , a high level of evidence in the literature is currently lacking . the present study was undertaken to systematically review the available data on ceus in evaluating thyroid nodules for the risk of thyroid carcinoma . 
importantly , to avoid the potential bias present in several studies reporting the performance of ceus using fine - needle aspiration cytology ( fnac ) as standard of reference , only those studies adopting histological diagnosis as the gold standard were selected to carry out the meta - analysis . materials andmethods conduct ofreview the thyroid gland . 
to try to expand our search , references of the retrieved articles were also screened to identify additional studies . study selection only original articles with complete data on thyroid nodules with histological diagnosis and their preoperative ceus evaluation were eligible for inclusion . 
specifically , to be included in the present meta - analysis a study should aim to classify a nodule as positive or negative on ceus by us examiners ( i.e. , a true clinical study undertaken to give information for practice ) and not basing on a particular feature of ceus ( i.e. , experimental study searching which ancillary characteristic of ceus could be the most reliable one )  . 
exclusion criteria were : studies reporting nodules with particular condition ( i.e. , inconclusive or indeterminate fnac report , specific echostructure or vascular presentation ) ; studies using non - histological standard of reference ; studies with no categorical results ( i.e. , positive and negative ceus evaluation ) ; studies with overlapping patient or nodule data ; cases report and case series ( i.e. , less than 15 cases ) ; studies using first - generation us contrast ; nonenglish language studies . 
three researchers ( pt , mc , and cv ) independently and in duplicate reviewed titles and abstracts of the retrieved articles , applying the above criteria ; then , all authors independently reviewed the full text of the remaining articles to determine their final inclusion . data extraction for each included study , the following information was extracted independently and in duplicate by three researchers ( pt , mc , and cv ) in a piloted form : ( 1 ) study data ( authors , year of publication , and country of origin ) ; ( 2 ) number of patients evaluated ; ( 3 ) number of lesions ; ( 4 ) histological diagnosis ; ( 5 ) preoperative ceus classification . 
data were cross - checked , and any discrepancy was mutually discussed . this present systematic review was conducted according to prisma guidelines . study quality assessment search strategy a comprehensive literature search in pubmed and scopus was conducted by searching the following terms : ( ( contrast ) and ultrasound ) and thyroid . 
this allowed us to retrieve the largest number of manuscripts of ceus in assessing the risk of bias of included studies was assessed independently by two reviewers ( pt and mc ) through the quality assessment of diagnostic accuracy studies ( quadas - 2 ) tool for the following aspects : patient selection ; index test ; reference standard ; flow and timing . 
risk of bias and concerns about applicability were rated as low ( l ) , high ( h ) , or unclear ( u )  . 1 3 408 la radiologia medica ( 2020 ) 125 : 406415 fig . 
beomonte zobel1 1interdisciplinary center for biomedical research , university campus bio - medico of rome , radiology , via alvaro del portillo 21 , 00159 rome , italy 2irccs fondazione santa lucia , department of radiology , via ardeatina 306 , rome , italy 3interdisciplinary center for biomedical research , university campus bio - medico of rome , complex system and security laboratory , rome , italy correspondence to : f . 
twenty - three patients affected by cancer with malignant focal bone lesions underwent dynamic gadolinium - enhanced magnetic resonance ( mr ) imaging using the following protocol : t1 - weighted turbo spin - echo sequences ( time to repeat [ tr ] 600 ms , time to echo [ te ] 8.6 ms , field of view [ fov ] 4040 cm ) before and after intravenous injection of gadolinium - containing contrast agent . 
ventitre pazienti oncologici con lesioni ossee focali maligne sono stati sottoposti ad esame di risonanza magnetica dinamica utilizzando sequenze turbo spin echo t1 - pesate ( tempo di ripetizione [ tr ] 600 ms , tempo di eco [ te ] 8 , 6 ms , campo di vista [ fov ] 4040 cm ) prima e dopo somministrazione endovenosa di mezzo di contrasto paramagnetico . 
i parametri pi , 60slope , 60i e fi hanno mostrato valori con differenza statisticamente significativa tra lesioni neoplastiche e tessuto osseo apparentemente normale ( p < 0 , 001 )  . 
the semiautomated technique we report appears to be accurate for identifying neoplastic tissue and for mapping perfusion parameters , with the added value of a consistent measurement of perfusion parameters on colour - coded maps . keywords contrast - enhanced magnetic resonance bone neoplastic lesion tumour perfusion specificit e laccuratezza calcolate si sono mostrate rispettivamente del 94% , 93% e 94% ad un valore soglia di pi di 100 ( signal to noise ratio , snr ) , con valori predittivi positivi e negativi rispettivamente del 93% e 94% . 
la tecnica di analisi semiautomatica utilizzata appare accurata nellidentificazione di tessuto neoplastico e nellelaborazione di mappe parametriche perfusionali , con il valore aggiunto di una valida misura dei parametri perfusionali sulle mappe colorimetriche stesse . parole chiave risonanza magnetica dinamica lesione ossea neoplastica perfusione del tessuto neoplastico introduction introduzione dynamic contrast - enhanced magnetic resonance ( dcemr ) imaging allows the characterization of tissue microvasculature , providing information about tumour microvessel structure and function [ 1 ]  . 
determination of perfusion parameters may be used to differentiate neoplastic from apparently normal tissue and also viable from necrotic tissue [ 2 ]  . several studies using dce - mr imaging demonstrate that malignant tumours generally show faster and stronger contrast enhancement than normal tissue [ 1 , 3 ]  . 
moreover , the neovascular network in tumours displays an architecture that can significantly differ from normal tissue : tumour vasculature is often highly heterogeneous , with extremely coarse capillaries of irregular diameter , distorted with twisting and sharp bends . vessel walls have numerous openings , widened interendothelial junctions and discontinuous or absent basement membrane making tumour capillaries extremely leaky [ 4 ]  . following intravenous administration , the contrast agent travels through the vascular system reaching the neoplastic tissues where it immediately starts to leak from the tumour vasculature , accumulating in the extracellularextravascular space through a passive diffusion process driven by the contrast concentration [ 5 ]  . mr imaging represents an important diagnostic tool in assessing musculoskeletal lesions , and dce - mr imaging may play an important role in characterizing a lesion , grading disease , planning and guiding biopsy , monitoring response to radioand / or chemotherapy and detecting early local recurrence [ 6 ]  . 
qualitative , semiquantitative and la risonanza magnetica ( rm ) dinamica ( dce - mri ) permette la caratterizzazione della microvascolarizzazione tissutale , fornendo informazioni sulla struttura e funzione della vascolarizzazione tumorale [ 1 ]  . 
in molti studi che hanno utilizzato la dce - mri stato dimostrato che i tumori maligni mostrano generalmente un potenziamento post - contrastografico pi precoce e di maggiore entit rispetto al tessuto sano [ 1 , 3 ]  . 
il potenziamento post - contrastografico riflette le caratteristiche della vascolarizzazione tumorale , in funzione di una maggiore densit microvasale e di unaumentata permeabilit endoteliale alle molecole del mezzo di contrasto rispetto al tessuto normale . 
inoltre la neo - vascolarizzazione tumorale presenta unarchitettura significativamente differente rispetto al tessuto osseo normale : spesso molto eterogenea , con capillari di diametro irregolare , con morfologia distorta e a decorso tortuoso . 
dopo la somministrazione endovenosa , il mezzo di contrasto raggiunge , attraverso il sistema circolatorio , il tessuto neoplastico dove diffonde rapidamente attraverso i vasi tumorali e si accumula nello spazio extracellulare - extravascolare attraverso un meccanismo di diffusione passiva guidato dalla differenza di concentrazione del mezzo di contrasto tra lume vasale e spazio extracellulare - extravascolare [ 5 ]  . la rm riveste un importante ruolo diagnostico nellidentificazione delle lesioni ossee e la rm dinamica pu assumere un ruolo importante nella caratterizzazione della 806 radiol med ( 2010 ) 115 : 804814 quantitative methods have been described to analyse tissue perfusion parameters [ 7 ]  . 
the aim of this study was to clinically validate , in focal malignant bone lesions , the reliability and accuracy of a semiautomated technique for analysing time - intensity curves and estimating the resulting perfusion parameters . 
 materials and methods patients a total of 23 patients ( 9 men , 14 women ; age range 4880 years ; mean age 65.7 years ) met the inclusion criteria and were examined in between june 2006 and november 2007 . all patients had a clinicalinstrumental diagnosis of primary tumour or metastatic malignant bone lesions and underwent standard and dce - mr imaging . 
standard mr images of the bony pelvis and appendicular skeleton were acquired by using t1 - weighted tse sequences ( tr 600 ms , te 8.6 ms , fov 4040 cm ) in coronal planes , t2 - weighted tse sequences ( tr 4 , 000 ms , te 122 ms , fov 3030 cm ) in coronal and axial planes , and stir sequences ( tr 3 , 300 ms , te 65 ms , fov 5050 cm ) in coronal planes . dce - mr images were acquired by using t1 - weighted tse sequences ( tr 485 ms , te 8.5 ms , fov 4040 cm ) in sagittal planes for vertebral lesions and in coronal planes for the bony pelvis and appendicular skeleton . 
six sequences were acquired every 60 s over a total period of 6 min ; the acquisition time for each sequence was 40 s , and each sequence was followed by a 20 - s pause . 
lo scopo di questo studio la validazione clinica , in lesioni ossee focali maligne , di una tecnica semiautomatica come strumento affidabile e accurato nellelaborazione e nellanalisi della curva di potenziamento post - contrastografico ( curva intensit / tempo ) e dei relativi parametri perfusionali . 
 materiali e metodi pazienti un totale di 23 pazienti ( 9 uomini , 14 donne ; et compresa tra 48 e 80 anni ; et media pari a 65 , 7 anni ) rientrava nei criteri di inclusione ed stato studiato nel periodo compreso tra giugno 2006 e novembre 2007 . 
tutti i pazienti avevano una diagnosi clinico - strumentale di neoplasia primitiva o di lesione ossea maligna metastatica e sono stati sottoposti ad un esame di rm standard e dinamica . 
i criteri di inclusione prevedevano la presenza di lesione ossea secondaria prevalentemente osteolitica o osteoaddensante da neoplasia mammaria , polmonare e prostatica o di lesione primitiva osteolitica da mieloma multiplo . 
i criteri di esclusione comprendevano la presenza di insufficienza renale cronica ( creatinina sierica > 1 , 5 mg / dl ) , la presenza di dispositivi metallici in prossimit del segmento scheletrico da studiare e la presenza di controindicazioni assolute allesposizione a campi magnetici elevati . protocollo rm le immagini sono state ottenute utilizzando un magnete da 1 , 5 t ( magnetom symphony , siemens , erlangen , germania )  . 
nello studio del rachide , le immagini standard sono state acquisite utilizzando sequenze turbo spin echo ( tse ) t1 - pesate ( tempo di ripetizione [ tr ] 600 ms , tempo di eco [ te ] 8 , 6 ms , campo di vista [ fov ] 4040 cm ) su piani sagittali , tse t2 - pesate ( tr 4000 ms , te 122 ms , fov 3030 cm ) su piani sagittali e assiali e sequenze short time inversion recovery ( stir ) ( tr 3300 ms , te 65 ms , fov 5050 cm ) su piani sagittali . 
nello studio del bacino e dello scheletro appendicolare , le immagini standard sono state acquisite utilizzando sequenze tse t1 - pesate ( tr 600 ms , te 8 , 6 ms , fov 4040 cm ) su piani coronali , tse t2pesate ( tr 4000 ms , te 122 ms , fov 3030 cm ) su piani coronali e assiali e sequenze stir ( tr 3300 ms , te 65 ms , fov 5050 cm ) su piani coronali . le sequenze dinamiche sono state acquisite utilizzando sequenze tse t1 - pesate ( tr 485 ms , te 8 , 5 ms , fov 4040 radiol med ( 2010 ) 115 : 804814 bma , omniscan , ge healthcare , usa ) was administered using an injection pump with a flow rate of 3 ml / s through a needle in the antecubital vein and was followed by a 15 - ml bolus of isotonic saline solution with a flow rate of 3 ml / s . the total injection time was 10 s . mr image postprocessing dce native images were reviewed on an independent workstation by two radiologists supervised by an expert radiologist who , identifying the most eligible image for lesion analysis ( image in which lesion appeared largest ) , selected it in each of the six serial acquisitions and exported all the selected images in the digital imaging and communications in medicine ( dicom ) format . 
after loading the dicom formatted images , dycoh automatically arranges the images to obtain a coherent time sequence , allowing the user to watch the image sequence in a cine mode and to select an area including the lesion of interest . 
the software , by analysing the entire sequence of images , estimates values of perfusion parameters such as area under the curve ( auc ) , peak intensity ( pi ) , time to peak ( ttp ) and 60 - s slope ( first minute of the time - intensity curve rise ) at each single pixel . 
nei 20 secondi tra la prima e la seconda acquisizione , veniva iniettato un bolo di mezzo di contarsto di 0 , 1 mmol / kg di peso corporeo di gadodiamide ( gd - dtpa - bma , omniscan , ge healthcare , usa ) mediante iniettore alla velocit di flusso di 3 ml / s attraverso un accesso venoso a livello della vena antecubitale e seguito dallinfusione di un bolo di 15 ml di soluzione fisiologica ad una velocit di flusso di 3 ml / s . 
il tempo totale di iniezione era di 10 secondi . analisi delle immagini le immagini ottenute in rm dinamica sono state analizzate , su una workstation dedicata , da due radiologi con la supervisione di un radiologo esperto ; dopo aver identificato limmagine pi adatta per lanalisi ( quella in cui la lesione era visualizzata nelle sue dimensioni maggiori ) , la stessa veniva selezionata in ciascuna delle sei acquisizioni seriali e il totale delle 6 immagini ottenute veniva esportato in formato digital imaging and communications in medicine ( dicom )  . 
the auc colour - coded map reproduces the value of the area under the time - intensity curve ( auc ) at 5 min after contrast agent injection for each pixel , encoding higher and lower permeability surface - area product values , with lighter ( white - yellow ) or darker ( redblack ) colours . 
the pi colour - coded map reproduces the value of the maximum signal intensity reached at each pixel . the ttp colour - coded map reproduces the time ( seconds ) employed to reach the maximum pi at each pixel . 
dopo aver caricato le immagini in formato dicom , il software dycoh le organizza automaticamente in una sequenza temporale coerente , permettendo la visualizzazione della sequenza di immagini in modalit cine e la selezione di unarea che includa la lesione da esaminare . 
il software , analizzando lintera sequenza delle immagini , calcola i valori di parametri perfusionali come larea sotto la curva ( auc ) , lintensit di picco ( pi ) , il tempo di picco ( ttp ) e la pendenza della curva intensit / tempo al primo minuto dopo somministrazione di mezzo di contrasto ( 60slope ) , per ciascun singolo pixel . 
la mappa colorimetrica dellauc riproduce , per ciascun pixel , il valore dellarea sotto la curva intensit / tempo a 5 minuti dopo la somministrazione del mezzo di contrasto , codificando con colori pi chiari ( biancogiallo ) e pi scuri ( rosso - nero ) i valori rispettivamente pi alti e pi bassi di permeabilit vascolare nella regione analizzata . 
la mappa colorimetrica del pi riproduce i valori della massima intensit di segnale raggiunta in ciascun pixel . la mappa colorimetrica del ttp riproduce il tempo ( in secondi ) impiegato per raggiungere i valori di massima intensit di segnale ( pi ) in ciascun pixel . 
2a - g selezione delle roi ( a - f ) a livello di una lesione da mieloma multiplo che interessa diffusamente il soma vertebrale , ed interfaccia grafica del software dycoh ( g ) che mostra la curva intensit / tempo ed i relativi parametri perfusionali . radiol med ( 2010 ) 115 : 804814 software dycoh reproduces the size and location of the rois by exactly repositioning them on the sequential images . 
to make the data homogeneous between examined lesions , final intensity ( fi ) and pi values were calculated by subtracting initial intensity , respectively , to signal intensity on the last acquisition and to signal intensity at curve peak . the initial intensity value measured conventionally 0 . lesion classification the 86 lesions were classified in two categories according to their density features , so computed tomography ( ct ) images of each lesion were analysed . 
the ct image selected for density measurement was defined on the basis of the mr image used for semiautomated analysis , obtaining the nearest image of the same lesion . data analysis the values of the measured parameters were classified , and students t test was performed for statistical comparison of perfusion parameters obtained in the group of apparently normal bone tissue and in the group of pathological bone tissue . 
sensitivity , specificity , accuracy , positive ( ppv ) and negative ( npv ) predictive values were calculated for pi and 60 - s slope by varying the thresholds . 
 results patient and lesion distributions are presented in table 1 . with regard to lesions , 57% ( n = 49 ) were located at the thoracic - lumbar spine , 31% ( n = 27 , of which 15 were at the iliopubic - ischiopubic bones and 12 at sacrum ) at bony pelvis and 12% ( n = 10 all at femur ) at the appendicular skeleton . 
according to their density values ( hu ) on ct evaluation , 58% ( n = 50 ) of bone lesions were predominantly osteolytic and 42% ( n = 36 ) predominantly osteosclerotic . median values and interquartile ranges ( 25%75% ) of perfusion parameters are presented in fig . 
larea di tessuto osseo apparentemente normale su cui veniva posizionata la seconda roi , era situata a livello del soma di un metamero adiacente che presentava caratteristiche tipiche del tessuto osseo sano in tutte le sequenze dello studio standard e dinamico : 1 . 
al fine di rendere i dati omogenei tra le lesioni esaminate , il valore di intensit finale e il valore di intensit di picco venivano calcolati sottraendo lintensit iniziale rispettivamente ai valori di intensit di segnale nellultima acquisizione e ai valori di intensit di segnale al picco della curva . 
il valore dellintensit iniziale risultava quindi per convenzione posto pari a 0 . classificazione delle lesioni le 86 lesioni sono state classificate in due categorie in base alle proprie caratteristiche densitometriche ; a tale scopo , sono state analizzate le corrispettive immagini di tomografia computerizzata ( tc ) di ciascuna lesione . 
tramite la selezione di una roi ( 0 , 5 cm2 ) su immagini ottenute in fase postcontrastografica venosa , sono stati ottenuti i corrispondenti valori di densit ( uh )  . 
utilizzando un valore soglia pari a 300 uh , le lesioni sono state suddivise in due categorie : le lesioni con valori di densit minori di 300 uh sono state classificate come prevalentemente osteolitiche , quelle con valori di densit maggiori o uguali a 300 uh sono state classificate come prevalentemente osteoaddensanti [ 9 ]  . 
limmagine tc utilizzata per la misurazione della densit veniva definita sulla base della corrispondente immagine rm selezionata per lanalisi semiautomatica , in modo da effettuare la misurazione sulla stessa sezione della lesione . 
the apparently normal bone tissue showed a very slow increase in enhancement , test t di student stato utilizzato per la comparazione statistica dei diversi parametri perfusionali ottenuti rispettivamente nel gruppo di tessuto osseo patologico e tessuto osseo apparentemente normale . stata calcolata la mediana ed il range interquartile ( 25%75% ) di ciascun parametro sia per il tessuto osseo radiol med ( 2010 ) 115 : 804814 patologico che per il tessuto osseo normale . 
sono stati poi calcolati la sensibilit , specificit , accuratezza , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) per i parametri pi e 60slope al variare dei valori soglia . risultati nella tabella 1 presentata la distribuzione dei pazienti e delle lesioni . 
in relazione alle caratteristiche densitometriche valutate mediante esame tc , il 58% ( n = 50 ) delle lesioni ossee mostrava caratteristiche prevalentemente osteolitiche mentre il restante 42% ( n = 36 ) mostrava caratteristiche prevalentemente osteoaddensanti . 
le lesioni ossee mostravano valori pi elevati di pi ( p < 0 , 001 ) , intensit al primo minuto dopo la somministrazione di mezzo di contrasto ( 60i ) ( p < 0 , 001 ) , intensit finale ( fi ) ( p < 0 , 001 ) e 60slope ( p < 0 , 001 ) rispetto al tessuto osseo apparentemente normale ; i valori di ttp , invece , non mostravano una differenza statisticamente significativa tra tessuto osseo patologico e tessuto osseo apparentemente normale ( p = 0 , 09 )  . 
il valore mediano di fi era pi basso rispetto a quello del pi , ad indicare un wash - out del mezzo di contrasto dopo 360 secondi dalla somministrazione endovenosa . 
il tessuto osseo apparentemente normale mostrava un incremento molto lento dellintensit di segnale con una morfologia della curva intensit / tempo molto diversa rispetto al pattern evidenziato nelle lesioni tumorali . 
 discussione i parametri valutabili con la dce - mri possono essere utilizzati come indicatori della farmacocinetica di un mezzo di contrasto endovenoso , permettendo di analizzare le caratteristiche perfusionali delle lesioni neoplastiche . 
4 curve intensit / tempo ottenute con i valori mediani e con range interquartili dei parametri perfusionali ( pi ; ttp ; fi ) valutati nel tessuto osseo patologico e nel tessuto osseo apparentemente normale . with a curve shape markedly different from the lesion pattern . 
contrast enhancement , in fact , allows one to define the microvascular characteristics of a lesion , in particular by providing information about tissue microvessel density and permeability [ 10 ]  . 
the anatomical basis of this has been explained by a high endothelial density and permeability to contrast agent . several qualitative and quantitative methods have been used to analyse contrast enhancement in dce - mr imaging [ 1 , 1419 ]  . 
 in this study , perfusion analysis of focal bone malignant lesions was performed using a semiautomated technique . through the determination of the time - intensity curve , values of some perfusion parameters were obtained ; in particular , for pi , 60 - s slope and fi , a statistically significant difference was observed between the values obtained in pathological and normal tissue samples . 
our method proved to be a reliable tool for perfusion analysis of focal bone malignant lesions , reaching a maximal accuracy of 94% for 812 radiol med ( 2010 ) 115 : 804814 densit tissutale e sulla permeabilit dei microvasi [ 10 ]  . molti autori hanno dimostrato che le neoplasie maligne , contrariamente al tessuto sano , mostrano un potenziamento post - contrastografico pi rapido e di maggiore entit [ 1013 ]  . 
molti metodi qualitativi e quantitativi sono stati utilizzati per lanalisi del potenziamento postcontrastografico in rm dinamica [ 1 , 1419 ]  . in questo studio lanalisi perfusionale delle lesioni ossee focali stata effettuata utilizzando una tecnica semiautomatica . 
attraverso lelaborazione di curve intensit / tempo , sono stati ottenuti i valori di alcuni parametri perfusionali ; in particolare stata osservata una differenza statisticamente significativa tra i valori di pi , 60slope e fi ottenuti rispettivamente nel tessuto patologico e in quello sano . 
il nostro metodo si mostrato uno strumento affidabile nellanalisi delle caratteristiche perfusionali delle lesioni ossee focali maligne , raggiungendo un valore massimo di accuratezza del 94% per il parametro pi e del 91% per il parametro 60slope nella differenziazione tra tessuto osseo patologico e tessuto osseo apparentemente sano . lanalisi perfusionale deve necessariamente tenere in considerazione leterogeneit della architettura vascolare tumorale [ 10 ]  . 
il risultato ottenuto dallanalisi effettuata attraverso la selezione di ununica roi delle dimensioni dellintera lesione esprime lincremento di segnale risultante dalla media degli incrementi di ciascun pixel di tutta larea e potrebbe compromettere lattendibilit della misura [ 15 ]  . 
stato infatti dimostrato come tale approccio risulti inadeguato , in particolare nello studio delle lesioni maligne , ove la presenza di aree a diverso pattern di potenziamento post - contrastografico nel contesto delle lesioni maligne rende difficoltosa una corretta caratterizzazione dei parametri perfusionali tissutali [ 20 , 21 ]  . uno dei vantaggi pi importanti della post - elaborazione delle immagini effettuata utilizzando la tecnica semiautomatica descritta , rappresentato dalla possibilit di disegnare delle roi direttamente sulle mappe colorimetriche elaborate . 
la mappa colorimetrica , cio lelaborazione di una mappa effettuata tramite un procedimento di codifica colorimetrica dei valori misurati per ciascun pixel dellimmagine anatomica , permette infatti di apprezzare leterogeneit del potenziamento post - contrastografico e di selezionare quindi larea della lesione pi rappresentativa , riducendo cos il rischio di perdere importanti informazioni diagnostiche . 
un ulteriore vantaggio rappresentato dalla possibilit di eseguire una pi precisa valutazione del potenziamento post - contrastografico stesso , in quanto il software , nellesecuzione dellanalisi dinamica , assegna automaticamente la medesima roi selezionata a tutte le immagini , rendendo consistente la misura parametrica ; il fig . 
i pi alti valori di sensibilit e specificit sono stati ottenuti con valori soglia di 100 per il parametro pi ( a ) e di 0 , 85 per il parametro 60slope ( b ) ; nella tabella sottostante ( c ) sono quindi illustrati i corrispondenti valori di sensibilit , specificit , accuratezza , valore predittivo positivo e negativo . pi and 91% for 60 - s slope in the differentiation of pathological versus apparently normal tissue . perfusion analysis needs to take into account the heterogeneity of tumour vascular architecture [ 10 ]  . 
user - defined , whole - tumour rois are unable to evaluate lesion heterogeneity , providing mean values of the entire lesion and thus affecting the reliability of measurements [ 15 ]  . 
wholetumour rois have been shown to be inappropriate , particularly for evaluating malignant lesions , in which heterogeneous areas of enhancement are crucial for a correct characterisation of tissue perfusion parameters [ 20 , 21 ]  . radiol med ( 2010 ) 115 : 804814 one of the most relevant advantages of image postprocessing using the semiautomated technique described is represented by the ability to draw rois directly on elaborated colour - coded parametric maps . 
pixel mapping , in fact , makes it possible to appreciate the heterogeneity of enhancement and to select the most representative area of the lesion , thus decreasing the risk of missing important diagnostic information . 
another advantage is the consistency of the area examined because of the softwares ability to exactly reposition the roi on the sequential images . manual segmentation , in fact , is one of the main limitations on dynamic perfusion analyses because of roi size and position variability . in this study , tse sequences were used in place of gradient - echo sequences , which are more widely used in the analysis of dynamic contrast enhancement [ 2225 ]  . 
this choice was driven by the possibility of increasing the signalto - noise ratio and spatial resolution with tse sequences , giving higher reliability to segmentation of the area inside a heterogeneous neoplastic lesion . 
this technique allowed us to build time - intensity curves with a relatively low number of measurements ( n = 6 ) , which we still consider an acceptable compromise in the analysis of heterogeneously enhancing lesions . 
however , the lack of a significant difference between normal and malignant bone ttp values could be explained by the lower temporal resolution of the dynamic sequences we chose . analysis of perfusion parameters in malignant bone lesions after selecting the most vascularised area allows a more accurate evaluation of malignancy . 
also , pixelby - pixel parametric assessment may play an important role in preand post - treatment evaluation : colour - coded maps , in fact , may allow more accurate detection of small nests of residual tumour tissue that may be missed using manual segmentation . 
our semiautomated technique is suitable for daily clinical practice because time for dynamic mr imaging post - processing is considerably shortened , allowing a perfusion analysis in 12 min ( data not shown )  . in conclusion , we demonstrated elevated reliability and accuracy in distinguishing between perfusion parameters of malignant and apparently normal bone tissue . 
data resulting from this study represent the basis for prospective studies of perfusion modifications after chemoand / or radiotherapy in cancer patients . posizionamento manuale delle roi infatti uno dei principali limiti dellanalisi perfusionale manuale , a causa della conseguente variabilit di posizione e di dimensioni delle roi . questo studio stato condotto utilizzando sequenze turbo spin echo anzich gradient echo , di pi ampio utilizzo in rm dinamica [ 2225 ]  . 
questa scelta stata guidata dalla possibilit di ottenere , con le sequenze turbo spin echo , un rapporto segnale / rumore ed una risoluzione spaziale pi elevati consentendo una pi affidabile identificazione dellarea da analizzare nel contesto di una lesione neoplastica eterogenea . 
tale impostazione della fase dinamica dello studio rm ha condotto allelaborazione di curve intensit / tempo utilizzando un numero relativamente basso di misurazioni ( n = 6 ) , che pu essere comunque considerato un compromesso accettabile nellanalisi di lesioni con potenziamento post - contrastografico eterogeneo . 
tuttavia , la mancanza di una differenza significativa dei valori del ttp tra tessuto osseo neoplastico e sano potrebbe essere spiegata dalla pi bassa risoluzione temporale delle sequenze dinamiche che abbiamo utilizzato . lanalisi dei parametri perfusionali in lesioni ossee maligne condotta attraverso la selezione dellarea intralesionale maggiormente vascolarizzata , permette una pi accurata caratterizzazione della lesione stessa . 
inoltre , tale tecnica potrebbe rappresentare un valido supporto nella pianificazione delle procedure bioptiche [ 6 ] consentendo lidentificazione ed il prelievo mirato delle aree di tessuto tumorale vitale , cio quelle maggiormente vascolarizzate e con potenziamento post - contrastografico pi precoce e rapido , nellambito della lesione . 
lelaborazione parametrica pixel - by - pixel delle immagini potrebbe inoltre assumere un ruolo rilevante nel monitoraggio pree post - trattamento : le mappe colorimetriche , infatti , possono permettere una pi accurata identificazione di piccoli noduli di tessuto neoplastico residuo / recidivo che potrebbero invece sfuggire utilizzando una tecnica di analisi manuale . 
la nostra tecnica di analisi potrebbe essere adatta per un utilizzo quotidiano nella pratica clinica , in quanto il tempo necessario per la post - elaborazione delle immagini di uno studio in rm dinamica risulta considerevolmente ridotto , permettendo di effettuare lanalisi perfusionale in 12 minuti ( dati non mostrati )  . in conclusione , abbiamo dimostrato una elevata affidabilit e accuratezza della nostra tecnica nella distinzione tra tessuto osseo neoplastico e tessuto osseo apparentemente normale mediante lanalisi di parametri perfusionali . 
lagalla dipartimento di biotecnologie mediche e medicina legale , sezione di diagnostica per immagini , policlinico universitario , via del vespro 127 , 90127 palermo , italy correspondence to : t . 
for each lesion , they assessed : ( a ) nature ( benign , malignant , not assessable ) , ( b ) specific diagnosis and ( c ) need for further radiological evaluation . 
a total of 167 / 187 ( 89.3% ) lesions were correctly assessed as benign or malignant at ceus , whereas 14 / 187 ( 7.5% ) lesions remained undetermined and 6 / 187 ( 3.2% ) were incorrectly assessed . 
lecocontrastografia ha consentito una corretta diagnosi ( benigne vs maligne ) in 167 / 187 ( 89 , 3% ) casi . quattordici / 187 ( 7 , 5% ) lesioni sono rimaste indeterminate e 6 / 187 ( 3 , 2% ) non sono state correttamente caratterizzate dopo ecocontrastografia , con valori di sensibilit , specificit , valore predittivo positivo , negativo e accuratezza diagnostica pari , rispettivamente , all89% , all89 , 6% , all89% , all89 , 6% e all89 , 3% . 
dopo ecocontrastografia , la necessit di ricorrere a ulteriori indagini radiologiche si ridotta a 46 / 187 casi ( 24 , 6% ) ( p < 0 , 001 )  . radiol med ( 2010 ) 115 : 714731 an effective alternative to mdct and mri and reduce the need for further radiological workup . keywords contrast - enhanced sonography liver ultrasound contrast media neoplasms conclusioni . 
lecocontrastografia pu essere considerata , in casi selezionati , una valida alternativa alla tcmd ed alla rm , riducendo il ricorso ad ulteriori indagini radiologiche . parole chiave ecografia con mezzo di contrasto fegato ecografia mezzo di contrasto ecografico neoplasie introduction introduzione despite the remarkable improvements in spatial and contrast resolution brought about by technological progress , greyscale ultrasonography ( us ) remains burdened by limited specificity in the characterisation of focal liver lesions ( fll ) [ 1 , 2 ]  . 
in addition , the presence of cardiac or respiratory motion artefacts and the difficulty studying small or deepseated lesions strongly restrict its diagnostic potential , even after administration of sonographic contrast material [ 3 ]  . the introduction of effective contrast - specific sonographic techniques that are highly sensitive to the nonlinear motion of the new microbubble - based sonographic contrast media has allowed better evaluation of both the microand macrocirculation in liver tumours [ 4 ]  . 
many studies have demonstrated the high diagnostic potential of contrast - enhanced us ( ceus ) in detecting and characterising fll , with sensitivity and specificity values comparable with those of computed tomography ( ct ) and magnetic resonance imaging ( mri ) [ 58 ]  . 
since those studies were published , however , ct and mri have benefited from major technological innovations that have improved their overall diagnostic quality in assessing liver lesions [ 9 , 10 ]  . the aim of our work was to evaluate the role of ceus in characterising fll compared with state - of - the - art ct and mri equipment . lecografia in scala di grigi , nonostante i continui progressi tecnologici ne abbiano notevolmente migliorato sia la risoluzione spaziale sia quella di contrasto , rimane una metodica poco specifica nella caratterizzazione delle lesioni focali epatiche ( lfe ) [ 1 , 2 ]  . 
lintegrazione con i moduli color doppler e doppler pulsato , sebbene possa talvolta fornire indicazioni utili ai fini della diagnosi , presenta il limite di consentire esclusivamente la valutazione del macrocircolo . 
inoltre , la presenza di artefatti da movimento , cardiaco o respiratorio , nonch la difficolt di studiare lesioni di piccole dimensioni o localizzate in sede profonda , ne limitano fortemente le possibilit diagnostiche , anche dopo somministrazione di mezzo di contrasto ecografico [ 3 ]  . lintroduzione di efficaci tecniche ecografiche contrastospecifiche , molto sensibili al comportamento non lineare dei nuovi mezzi di contrasto ecografici a base di microbolle , ha consentito una migliore valutazione sia del microche del macrocircolo delle neoplasie epatiche [ 4 ]  . 
numerosi studi hanno ormai dimostrato lelevata capacit diagnostica dellecografia con mezzo di contrasto ( ceus ) nella detezione e nella caratterizzazione delle lfe con valori di sensibilit e specificit comparabili a quelli di tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) [ 58 ]  . 
rispetto a tali studi , tuttavia , queste ultime due metodiche si sono recentemente giovate di notevoli innovazioni tecnologiche , che ne hanno migliorato la qualit diagnostica complessiva nella valutazione delle lesioni epatiche [ 9 , 10 ]  . scopo del presente lavoro stato quello di valutare il ruolo dellecocontrastografia nella caratterizzazione delle lesioni focali epatiche confrontandola con apparecchiature tc e rm allo stato dellarte . materials and methods patients materiali e metodi pazienti after obtaining the approval of the institutional ethics committee , over a period of 2 years , we prospectively evaluated 159 patients ( 72 men and 87 women ; age range 1887 years , mean age 57.7 years ) with 187 fll ( diameter 0.413.1 cm ; mean 3.2 cm ) identified but not characterised on grey - scale us , 91 of which were malignant and 96 benign ( table 1 )  . 
inclusion criteria were : ( a ) presence of at ottenuta lapprovazione da parte del comitato etico istituzionale , sono stati prospetticamente valutati , durante un periodo di due anni , 159 pazienti ( 72 uomini e 87 donne ; et : 1887 anni , media : 57 , 7 anni ) , con 187 lfe ( diametro 0 , 413 , 1 cm ; media : 3 , 2 cm ) identificate ma non caratterizzate allecografia di base in scala di grigi , 91 delle quali maligne e 96 benigne ( tabella 1 )  . 
tutti i pazienti sono stati sottoposti a ceus nella stessa giornata delleffettuazione dellindagine tc e / o rm , immediatamente prima o radiol med ( 2010 ) 115 : 714731 immediately after ct and / or mri examination performed by independent operators . 
informed consent was obtained from all patients prior to ceus study , according to the procedure described in the declaration of helsinki [ 11 ]  . dopo lesecuzione delle stesse , da parte di operatori indipendenti . 
complessivamente , 135 / 159 pazienti hanno avuto valutata una singola lesione , 20 / 159 due lesioni e 4 / 159 tre . settantanove / 187 lfe sono state riscontrate in fegato sano , 75 / 187 in fegato steatosico e le rimanenti 33 / 187 in fegato cirrotico . 
la procedura stata effettuata in accordo con la dichiarazione di helsinki [ 11 ]  . examination technique ceus was performed on sonographic units ( hdi 5000 , atl , bothell , wa , usa , iu - 22 , philips ultrasound , bothell ) equipped with multifrequency convex - array transducers and contrast - specific pulse - inversion technology [ 4 ]  . prior to ceus , in all cases , the liver parenchyma was studied with grey - scale and colour doppler us and , if necessary , with pulsed doppler us to identify and define the lesion and select an appropriate scanning plane . 
patients were administered intravenously a bolus of 2.4 ml , corresponding to 0.003 ml / kg per 70 kg of body weight , of contrast medium ( sonovue , bracco , milan , italy ) , followed by 510 ml of saline solution injected through a 20to 22 - gauge needlecannula inserted into the antecubital vein of the ar to minimise microbubble rupture and enable continuous realtime imaging , we used a low frame rate ( 5 hz ) and low mechanical index ( 0.050.08 ) , and the focus was placed below the lesion to be examined . 
in patients with multiple lesions , a separate study was performed for each lesion , with an interval of at least 15 min between injections of contrast mediu digital cine loops were acquired before and after contrast - medium administration in the arterial , portal - venous and delayed phases ( also known as extended portal - venous phase ) at 2530 , 5580 and 235260 s after the beginning of the injection . image analysis all cine loops were digitally stored as raw data . 
two radiologists with at least 10 years experience with ceus , not involved in the scanning and not aware of patients clinical history or final diagnosis , consensually reviewed the images off line . 
baseline echogenicity relative the surrounding parenchyma ( hyperechoic , hypoechoic and isoechoic ) tecnica desame la ceus stata eseguita con apparecchiature ( hdi 5000 , atl , bothell , wa , usa , iu - 22 , philips ultrasound , bothell , wa , usa ) dotate di sonde convex multifrequenza e di tecnologia contrasto - specifica ad inversione di impulso [ 4 ]  . prima della ceus , stato sempre effettuato uno studio ecografico del parenchima epatico , sia in scala di grigi che con color - power doppler ed eventualmente doppler pulsato , al fine di individuare e definire la lesione stessa e selezionare un adeguato piano di scansione . 
si proceduto quindi alla somministrazione endovena di un bolo di 2 , 4 ml , corrispondente a 0 , 003 ml / kg per 70 kg di peso corporeo , di mezzo di contrasto ( sonovue , bracco , milano , italia ) seguito dalliniezione di 510 ml di soluzione salina mediante unagocannula da 2022 gauge posizionata in una vena antecubitale del braccio . 
al fine di minimizzare la rottura delle microbolle e realizzare uno studio continuo in tempo reale stato utilizzato un basso frame - rate ( 5 hz ) , cos come un basso indice meccanico , compreso tra 0 , 05 e 0 , 08 , e il fuoco stato posizionato al di sotto della lesione da esaminare . 
sono stati acquisiti dei filmati digitali prima e dopo somministrazione di mdc , in fase arteriosa , portale - venosa e tardiva ( anche definita portalevenosa estesa ) , rispettivamente a 2530 , a 5580 ed a 235260 secondi dallinizio della somministrazione . analisi delle immagini tutti i filmati sono stati archiviati come dati grezzi in forma digitale . 
due radiologi esperti nella ceus ( almeno dieci anni ) , non coinvolti nellesecuzione degli esami e non a conoscenza della storia clinica dei pazienti n della diagnosi finale , hanno valutato in consenso off - line le immagini ottenute . 
in primo luogo , stato loro chiesto di fornire una diagnosi di natura ( benigna , indeterminata , maligna ) in base a criteri diagnostici prestabiliti ( tabella 2 ) [ 7 , 1215 ] ; in secondo luogo , sulla base degli stessi criteri , stato loro chiesto di caratterizzare , se possibile , la lesione . 
infine , i lettori sono stati tenuti a indicare se , dopo la ceus , fossero necessarie ulteriori indagini radiologiche ( tc e / o rm con mdc ) per caratterizzare le lesioni . 
once the threshold had been reached , three scans were performed with delays of 2025 s ( arterial phase ) , 4550 s ( portal - venous phase ) and 180300 s ( delayed phase ) , respectively . 
the mri study was done with a 1.5 - t scanner ( signa excite , general electric , health care , milwaukee , wi , usa ) using a phased - array multicoil . the protocol included precontrast breath - hold t2 - weighted fast spin - echo ( fse ) sequences in the axial plane with and without fat saturation , and t1 - weighted in - phase and out - ofutilizzando il bolus tracking . 
una volta raggiunta questultima sono state effettuate tre scansioni impostando un ritardo , rispettivamente , di 2025 s ( fase arteriosa ) , 4550 s ( fase portale - venosa ) e 180300 s ( fase tardiva )  . 
lo studio rm stato realizzato con apparecchiatura da 1 , 5 t ( signa excite , general electric , health care , milwaukee , wi , usa ) usando bobine multiple di ricezione ( phased array )  . 
il protocollo includeva , prima della somministrazione del mdc , sequenze fast spin echo ( fse ) t2 - pesate in apnea secondo piani di scansione assiali con e senza la soppressione del grasso e sequenze gradient echo ( gre ) t1 - pesate in fase e in opposizione di fase . 
a triphasic dynamic study was obtained after the administration of 0.1 mmol / kg of gadobenate dimeglumine ( multihance , bracco , italy ) injected at a flow rate of 2 - 2 - 5 ml / s and flushed by 20 ml of saline using an automated injector . 
the scanning delays after automatic detection of the contrast bolus were 14 s ( arterial phase ) , 50 s ( portal - venous phase ) and 3 min ( equilibrium phase ) , respectively . 
differences in the results obtained with the different modalities were evaluated using stato effettuato dopo somministrazione di 0 , 1 mmol / kg di gadobenato dimeglumina ( multihance , bracco , italia ) iniettato alla velocit di 22 , 5 ml / s seguito da 20 ml di soluzione salina usando un iniettore automatico . 
il ritardo di scansione era , rispettivamente , di 14 s ( fase arteriosa ) , 50 s ( fase portale - venosa ) e 3 minuti ( fase allequilibrio ) dalla detezione automatica del bolo di mdc . 
per la valutazione delle immagini tcmd e rm , stato impiegato il picture archiving and communication system ( pacs ) in dotazione alla nostra istituzione ( impax , agfa - gevaert , milano , italia )  . 
le differenze nei risultati ottenuti con le diverse metodiche sono state valutate mediante il test z sulle frequenze con livello di significativit statistica fissato a p radiol med ( 2010 ) 115 : 714731 tabella 3 criteri diagnostici impiegati in tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) per la caratterizzazione delle lesioni focali epatiche lesioni cisti angioma aspetti pre - contrastografici aspetti contrastografici densit liquida ( 10 uh ) , ipointensit in t1 e netta iperintensit in t2 omogenea iperintensit in t2 iperplasia nodulare focale isointensit al fegato in t1 / t2 cicatrice centrale iperintensa in t2 adenoma epatocellulare area indenne da steatosi area di steatosi focale nodulo di rigenerazione componente lipidica ( riduzione del segnale nelle immagini t1 pesate fuori - fase ) o emorragica ( disomogenea iperdensit o iperintensit in t1 ) iperdensa nel contesto di un parenchima a densit ridotta elevato segnale nelle immagini t1 fuori - fase ipodensa nel contesto di un parenchima a densit normale riduzione del segnale nelle immagini t1 fuori - fase iperdenso o iperintenso in t1 / ipointenso in t2 carcinoma epatocellulare modica e disomogenea iperintensit in t2 noduli satellite , presenza di quota lipidica metastasi colangiocarcinoma avascolare durante tutte le fasi contrastografiche captazione globulare periferica o ad anello durante la fase arteriosa , con progressivo riempimento centripeto in fase portale - venosa e / o allequilibrio ; iso - densit / intensit ai vasi omogeneamente e nettamente ipervascolare in fase arteriosa , aspetto iso - ipervascolare in fase portalevenosa e / o allequilibrio , enhancement tardivo della cicatrice centrale ; aspetto iso - ipervascolare in fase epatospecifica in rm enhancement omogeneo e diffuso o eterogeneo durante la fase arteriosa , enhancement simile a quello del parenchima epatico durante le fasi portale - venosa e allequilibrio , omogeneo o eterogeneo . 
 aspetto ipovascolare in fase epatospecifica in rm isovascolare rispetto al circostante parenchima epatico durante tutte le fasi vascolari isovascolare rispetto al circostante parenchima epatico durante tutte le fasi vascolari ipoo isovascolare in fase arteriosa , indistinguibile dal circostante parenchima epatico nelle fasi portalevenosa e allequilibrio enhancement diffuso , omogeneo o eterogeneo , durante la fase arteriosa con wash - out in fase portale - venosa e / o allequilibrio captazione periferica , vascolarizzazione variabile durante la fase arteriosa , aspetto ipovascolare in fase portale - venosa e / o allequilibrio enhancement disomogeneo prevalentemente periferico , impregnazione contrastografica allequilibrio a z - test on the frequencies , with statistical significance set at p < 0.05. 
ceus provided the correct diagnosis of the nature of the lesion ( benign or malignant ) in 167 / 187 ( 89.3% ) fll , 86 of which were benign and 81 malignant . 
fourteen out of 187 ( 7.5% ) fll ( nine hcc , three haemangiomas , one fnh and one cyst with corpuscular content ) remained undetermined , even after ceus . 
la ceus ha consentito una corretta diagnosi natura ( in termini di benignit o malignit ) in 167 / 187 ( 89 , 3% ) lfe , 86 benigne e 81 maligne . 14 / 187 ( 7 , 5% ) lfe ( 9 hcc , 3 angiomi , 1 inf e 1 cisti a contenuto corpuscolato ) sono rimaste indeterminate anche dopo ceus . 
on the basis of these findings , we were able to classify 32 / 33 fnh as benign , 14 ( 42.4% ) of which were correctly characterised at ceus . 
after sonovue administration , the two larger adenomas showed a homogeneously hyperechoic appearance during the arterial phase before becoming isoechoic ridotta a 46 / 187 casi ( 24 , 6% ) ( p < 0 , 001 )  . 
le rimanenti 32 erano invece lesioni classificate come benigne ( n = 27 ) o maligne ( n = 5 ) ma non ulteriormente caratterizzabili ( p < 0 , 001 )  . 
 lesioni benigne e pseudolesioni sulla base degli aspetti ecocontrastografici ( tabella 4 , fig . 1 ) , 22 / 34 ( 64 , 7% ) angiomi sono stati correttamente caratterizzati , 6 / 34 ( 17 , 6% ) sono stati classificati come lesioni benigne , ma non ulteriormente caratterizzati , 3 / 34 ( 8 , 8% ) sono risultati indeterminati e 3 / 34 ( 8 , 8% ) sono stati erroneamente caratterizzati come metastasi . 
dopo somministrazione di sonovue i due adenomi di maggiori dimensioni hanno mostrato un aspetto omogeneamente iperecogeno in fase arteriosa diventando poi isoecogeni nelle restanti fasi , mentre ladenoma pi piccolo apparso costantemente isoecogeno rispetto al circostante parenchima epatico . 
a allecografia di base si apprezza una lesione isoecogena , lievemente disomogenea , del diametro di 4 , 6 cm , localizzata in corrispondenza del vi segmento epatico ( calipers )  . 
c alla rm , dopo somministrazione di mdc , si conferma la captazione globulare periferica in fase arteriosa con progressivo riempimento centripeto in fase portale ( d ) , completo nella fase allequilibrio ( e ) ( frecce )  . during the remaining phases , whereas the smaller adenoma appeared constantly isoechoic relative to the surrounding hepatic parenchyma . 
lascesso alla ceus ha mostrato una captazione di mdc perifericamente e in corrispondenza di qualche fine sepimento presente nel suo table 5 ceus findings in 33 focal nodular hyperplasias no . 
lesions arterial phase tabella 5 aspetti alla ceus delle 33 inf numero lesioni fase arteriosa hypervascular hypervascular hypervascular ipervascolare ipervascolare ipervascolare portal phase isovascular hypervascular hypervascular fase portale isovascolare ipervascolare ipervascolare radiol med ( 2010 ) 115 : 714731 delayed phase isovascular isovascular hypervascular fase tardiva isovascolare isovascolare ipervascolare fig . 
at 31 s after sonovue injection , the lesion appears homogeneously and markedly hypervascular ( white arrow ) appearing ( b ) isoechoic ( black arrow ) in the late phase ( black arrowhead : inferior vena cava )  . 
a allecografia di base si apprezza una lesione del diametro di 3 , 5 cm isoecogena rispetto al circostante parenchima epatico ( freccia nera ) , localizzata in corrispondenza del iv segmento adiacente alla vena cava inferiore ( punta di freccia bianca )  . 
b at ceus , the lesion is hypovascular in the arterial phase ( arrows ) and isovascular with respect to the remaining hepatic parenchyma in the portalvenous phase ( c )  . 
alecografia di base rivela la presenza di una lesione modicamente ipoecogena localizzata in corrispondenza del vi segmento in sede sottocapsulare del diametro di 1 , 3 cm ( calipers )  . 
e - g dopo somministrazione di mdc , la lesione non presenta captazione dello stesso in fase arteriosa ed isointensa rispetto al circostante parenchima epatico , rispettivamente , nelle fasi portale - venosa ed epatospecifica a 2 ore ( frecce )  . 726 table 6 ceus findings in 33 hepatocellular carcinomas no . 
lesions arterial phase portal phase delayed phase radiol med ( 2010 ) 115 : 714731 hypervascular hypervascular isovascular hypovascular isovascular hypervascular with central hypovascular area hypovascular isovascular hypovascular hypovascular isovascular hypervascular with central hypovascular area hypovascular isovascular hypovascular hypovascular isovascular hypervascular with central hypovascular area tabella 6 aspetti alla ceus dei 33 hcc numero lesioni fase arteriosa fase portale fase tardiva ipervascolare ipervascolare isovascolare ipovascolare isovascolare ipervascolare con area centrale ipovascolare ipovascolare isovascolare ipovascolare ipovascolare isovascolare ipervascolare con area centrale ipovascolare ipovascolare isovascolare ipovascolare ipovascolare isovascolare ipervascolare con area centrale ipovascolare remaining two appeared constantly isovascular to the hepatic parenchyma . 
in all three cases , ceus led to a diagnosis of malignancy without further characterisation . on ceus , the haemangioendothelioma showed heterogeneous uptake of contrast medium predominantly in the more peripheral regions , with generally hypoechoic appearance in the other vascular phases . 
even in this case , ceus provided a diagnosis of malignancy without further lesion characterisation . ad unerronea caratterizzazione di malignit alla ceus . infine , tutte le 13 aree indenni sono apparse costantemente isovascolari al parenchima epatico adiacente alla ceus , cos come le tre aree di steatosi focale , consentendone la corretta caratterizzazione . lesioni maligne dopo la somministrazione di sonovue ( tabella 6 ) , 20 / 33 ( 60 , 6% ) hcc sono stati correttamente caratterizzati , 9 / 33 ( 27 , 3% ) sono rimasti indeterminati , 1 / 33 ( 3% ) stato erroneamente caratterizzato come nodulo di rigenerazione ( fig . 4 ) e 3 / 33 ( 9 , 1% ) sono stati correttamente classificati come lesioni maligne ma caratterizzate come metastasi . 
sulla scorta dei reperti contrastografici ( tabella 7 ) , tutte le metastasi sono state correttamente caratterizzate alla ceus . allo studio contrastografico due colangiocarcinomi hanno mostrato un enhancement disomogeneo in fase arteriosa con wash - out in fase portale - venosa e tardiva , mentre un colangiocarcinoma si presentato costantemente ipovascolare . 
in tutti e tre i suddetti casi stata posta alla ceus diagnosi di malignit ma senza ulteriore caratterizzazione . alla ceus , lemangioendotelioma ha presentato disomogenea impregnazione di mdc prevalentemente nella regione pi periferica con aspetto nel complesso ipoecogeno nelle altre fasi vascolari . 
anche in questo caso stata posta alla ceus diagnosi di malignit ma senza caratterizzare la lesione . discussione lo studio da noi condotto ha confermato lelevata sensibilit e specificit della ceus , in termini di diagnosi radiol med ( 2010 ) 115 : 714731 fig . 
e , f alla rm , dopo somministrazione di mdc , la lesione nettamente ipervascolare in fase arteriosa e ipointensa in fase tardiva ( frecce )  . 728 table 7 ceus findings in 54 metastases no . 
lesions arterial phase tabella 7 aspetti alla ceus delle 54 mts numero lesioni fase arteriosa isovascular hypovascular hypervascular rim hypervascular dotted appearance isovascolare ipovascolare orletto ipervascolare ipervascolare aspetto puntato portal phase hypovascular hypovascular hypovascular hypovascular hypovascular fase portale ipovascolare ipovascolare ipovascolare ipovascolare ipovascolare radiol med ( 2010 ) 115 : 714731 delayed phase hypovascular hypovascular hypovascular hypovascular hypovascular fase tardiva ipovascolare ipovascolare ipovascolare ipovascolare ipovascolare discussion our study confirmed the high sensitivity and specificity of ceus in differentiating between benign and malignant fll , even when compared with state - of - the - art ct and mri equipment [ 1622 ]  . 
compared with the latter , however , ceus offers advantages related to the absence of ionising radiation , the use of a contrast medium with a better tolerability profile compared with iodine - based agents , lower costs and the possibility of replying to the clinical query in a very short time . 
in addition , compared with baseline us , our experience confirms a statistically significant reduction , > 75% , in the need for further imaging workup after ceus [ 20 ]  . 
on the other hand , ceus was unable to provide a definitive diagnosis in 46 cases , 14 of which it could not characterise at all and 32 of which it could only partially classify as benign ( n = 27 ) or malignant ( n = 5 ) but not characterise with any precision . 
six of these , all capillary haemangiomas ( diameter : 1.21.7 cm ; mean 1.4 cm ) were nonetheless classified at ceus as benign lesions due to their hypervascularity during the arterial phase and absence of washout in the following phases . 
in evaluating such haemangiomas , the multiparametric capabilities of mri proved particularly useful , as they demonstrated the characteristic high signal intensity on t2 - weighted images . however , we are unable to provide any real and proven explanation for this discordance , although the different pharmacokinetics of sonographic contrast material , which does not leave the vascular bed unlike the typically extradifferenziale tra lesioni focali epatiche benigne e maligne , anche quando confrontata con apparecchiature tc e rm allo stato dellarte [ 1622 ]  . 
rispetto a queste ultime , tuttavia , la ceus offre i vantaggi relativi allassenza di radiazioni ionizzanti , allimpiego di un mezzo di contrasto con un profilo di tollerabilit migliore rispetto ad un prodotto organo - iodato , ai costi pi limitati ed alla possibilit di rispondere ad un quesito diagnostico in tempi molto brevi . 
inoltre , rispetto allecografia di base , nella nostra esperienza risulta confermata una riduzione , superiore al 75% e statisticamente significativa , della necessit di ricorrere ad esami diagnostici supplementari dopo leffettuazione di un esame ecocontrastografico [ 20 ]  . 
daltra parte , la ceus non stata in grado di porre diagnosi definitiva in 46 casi , in 14 dei quali la lesione non risultata caratterizzabile tout court , mentre nei rimanenti 32 , pur essendo stato possibile classificare correttamente alla ceus una data lesione come benigna ( n = 27 ) o maligna ( n = 5 ) , non stato tuttavia possibile caratterizzarla con esattezza . 
in particolare , la ceus non risultata dirimente in nove angiomi , tutti correttamente caratterizzati dalla tcmd o dalla rm . sei di questi ultimi ( diametro : 1 , 2 cm1 , 7 cm ; media : 1 , 4 cm ) , di tipo capillare , sono stati comunque classificati alla ceus come lesioni benigne perch ipervascolari in fase arteriosa in assenza del segno del wash - out nelle fasi seguenti , mentre tre angiomi ( diametro : 0 , 8 cm1 , 3 cm ; media : 1 cm ) sono rimasti indeterminati perch costantemente ipovascolari . 
tuttavia , non abbiamo una reale e dimostrata spiegazione di tale discrepanza , per quanto la diversa farmacocinetica del mdc ecografico , che non fuoriesce dal letto vascolare a differenza dei mezzi di contrasto usati in mdct o rm , tipicamente extracellulari , possa contribuire alla spiegazione di tale reperto [ 2325 ]  . radiol med ( 2010 ) 115 : 714731 cellular mdct or mri agents may in part account for this finding [ 2325 ]  . eighteen fnh ( diameter 16 cm ; mean 2.4 cm ) and the three adenomas ( table 1 ) were correctly classified as benign lesions at ceus . 
further characterisation was impossible , as the fnh lacked the typical spoke - wheel appearance in the arterial phase or the hypoechoic central scar , and the adenomas lacked subcapsular vessels with centripetal or mixed fill in [ 2628 ]  . 
one fnh ( diameter 4.8 cm ) remained undetermined because , located deep in a bright fatty liver , it showed a thin hypoechoic peripheral rim in the delayed phase despite appearing hypervascular in the arterial phase and isovascular in the delayed phase . 
in these cases , mri , with demonstration of uptake of liver - specific contrast medium in the delayed phase , proved particularly useful [ 29 , 30 ]  . the ability of ceus to demonstrate the benign or malignant nature of a lesion was also evident in the evaluation of pseudolesions , such as areas of focal fatty change and fatty sparing . 
in all these pseudolesions , ceus was able to demonstrate substantial isovascularity relative to the liver parenchyma , thus confirming their benign nature [ 12 , 31 ]  . even other benign lesions ( but with a risk of neoplastic degeneration , such as regenerative nodules in a cirrhotic liver ) , were correctly characterised by ceus , thanks to the typical lack of hypervascularity in the arterial phase and isovascularity relative to the surrounding parenchyma in the remaining phases [ 32 ]  . 
seven hcc ( diameter 1.38.3 cm ; mean 4.2 cm ) , despite appearing hypervascular in the arterial phase , showed no washout sign , most likely because of the relatively good degree of differentiation of these lesions . 
it is indeed known that well - differentiated hcc , even though hypervascular in the arterial phase , may fail to appear hypoechoic in the portal - venous or delayed phase , and this is the main cause of misinterpretation at ceus [ 33 ]  . 
in our series , at mdct and mri , these hcc displayed the classic washout sign in the portal and / or equilibrium phase ( n = 4 ) or hypointensity relative to the surrounding parenchyma ( n = 3 ) in the liver - specific phase . 
the washout sign was distinctive in all liver metastases and in the three cholangiocarcinomas studied with ceus , regardless of the degree of vascularity seen in the arterial phase [ 3437 ]  . ceus led to a misdiagnosis in six cases . 
in particular , one hcc ( diameter 8 mm ) , with isoechoic appearance in all phases of ceus , was wrongly classified as a regenerative nodule , whereas mri demonstrated hypervascularity in the arterial phase and hypointensity in the liver - specific phase , both suggestive of hcc . 
one abscess and one haeman ( table 1 ) were wrongly considered giopericytoma diciotto ifn ( diametro : 16 cm ; media : 2 , 4 cm ) e i tre adenomi studiati ( tabella 1 ) , sono stati correttamente valutati alla ceus come lesioni benigne , tuttavia non stato possibile caratterizzarli ulteriormente , non presentando le prime il caratteristico aspetto a ruota di carro in fase arteriosa o la cicatrice centrale ipoecogena e , i secondi , vasi arteriosi subcapsulari con riempimento centripeto o misto [ 2628 ]  . 
una ifn ( diametro di 4 , 8 cm ) rimasta indeterminata perch , localizzata profondamente in fegato brillante come da steatosi , pur presentandosi ipervascolare in fase arteriosa e isovascolare in fase tardiva , ha mostrato , in questultima fase , un sottile orletto periferico ipoecogeno . in questi casi risultata particolarmente utile lindagine rm , in grado di dimostrare la caratteristica captazione del mezzo di contrasto epatospecifico in fase tardiva [ 29 , 30 ]  . la capacit della ceus di dimostrare la benignit o la malignit di una lesione si dimostrata evidente anche nella valutazione di pseudolesioni , quali le aree di steatosi focale e quelle indenni da steatosi . 
in tutte queste pseudolesioni , la ceus stata in grado di dimostrare la sostanziale isovascolarit rispetto al rimanente parenchima epatico , confermandone la natura benigna [ 12 , 31 ]  . 
anche altre lesioni benigne , ma passibili di progressione neoplastica , come i noduli di rigenerazione in fegato cirrotico , nella nostra esperienza , sono state correttamente caratterizzate alla ceus grazie alla tipica assenza di ipervascolarit in fase arteriosa e lisovascolarit rispetto al fegato circostante nelle rimanenti fasi [ 32 ]  . in sette hcc ( diametro : 1 , 38 , 3 cm ; media : 4 , 2 cm ) , pur essendo evidente alla ceus lipervascolarit in fase arteriosa , non stato osservato il segno del wash - out , probabilmente in relazione alla relativamente buona differenziazione di tali lesioni . 
noto , infatti , che gli hcc ben differenziati , seppur ipervascolari in fase arteriosa , possono non presentarsi ipoecogeni nelle fasi portale - venosa o tardiva e questa la principale causa di errori interpretativi alla ceus [ 33 ]  . 
nella nostra casistica , tali hcc hanno presentato , alla tcmd o alla rm , il classico segno del wash - out in fase portale e / o allequilibrio ( n = 4 ) , oppure lipointensit rispetto al circostante parenchima epatico ( n = 3 ) in fase epatospecifica . 
il segno del wash - out stato quello che ha invariabilmente caratterizzato tutte le metastasi epatiche ed i tre colangiocarcinomi da noi studiati alla ceus , indipendentemente dal grado di vascolarizzazione apprezzabile in fase arteriosa [ 3437 ]  . la ceus ha condotto ad una diagnosi erronea in sei casi . 
in particolare , un epatocarcinoma ( diametro : 8 mm ) , isoecogeno al parenchima epatico in tutte le fasi , stato erroneamente classificato come nodulo di rigenerazione , mentre alla rm , veniva dimostrata lipervascolarit in fase arteriosa e lipointensit in fase epatospecifica , entrambe suggestive di hcc . 
un ascesso e un emangiopericitoma ( tabella 1 ) , sono stati erroneamente considerati maligni per la presenza , rispettivamente , di un orletto perilesionale iperecogeno in fase arteriosa nel primo e per laspetto 730 radiol med ( 2010 ) 115 : 714731 malignant : in the first case , this was due to the presence of a hyperechoic perilesional rim during the arterial phase and , in the second , to a heterogeneous appearance with enhancing and nonenhancing areas . 
finally , three haemangiomas ( diameter 2.84.4 cm ; mean 3.6 cm ) were misdiagnosed as malignancies due to the presence of a partial hyperechoic rim in the arterial phase ( n = 2 ) or a constantly nonenhancing central area within a hypervascular lesion ( n = 1 )  . ceus shares many of the limitations of conventional us , so that obesity , bowel gas , suboptimal acoustic window , motion artefacts or poor clinical condition of the patient may affect or even invalidate the quality of the examination . 
in addition , small lesions deeply seated in the liver parenchyma may prove difficult to evaluate with ceus , especially those located at a depth > 12 cm within a fatty liver [ 20 , 31 ]  . 
multiple injections of contrast material may be necessary to evaluate lesions located in different hepatic segments and , in some cases , to evaluate the same lesion . our study has a few limitations . 
firstly , the reference standard was not liver biopsy in all cases , but the mdct and / or mri criteria , which are , however , well - established and commonly used in clinical practice . 
moreover , the readers reviewed the images by consensus so that it was not possible to assess the degree of concordance between independent readers . in conclusion , based on our experience , ceus can be considered a valuable alternative to mdct and mri for correct diagnosis of benignity or malignancy in fll , thus optimising patient management and limiting the use of more costly and less readily available imaging modalities . however , in a nonnegligible number of lesions especially small and benign lesions ceus is not able to provide a correct diagnostic characterisation . 
in tre angiomi ( diametro : 2 , 84 , 4 cm ; media : 3 , 6 cm ) , infine , veniva erroneamente posta diagnosi di malignit a causa della presenza , rispettivamente , di un parziale orletto iperecogeno in fase arteriosa ( n = 2 ) o di unarea centrale costantemente avascolare nel contesto di una lesione ipervascolare ( n = 1 )  . la ceus condivide molte limitazioni con lecografia convenzionale , per cui lobesit , laria contenuta nelle anse intestinali , una finestra acustica non ottimale , artefatti da movimento o condizioni cliniche generali scadenti del paziente possono limitare , fino addirittura ad inficiarla , la qualit dellesame . 
inoltre , piccole lesioni profondamente indovate nel parenchima epatico possono risultare di difficile valutazione con la ceus , specialmente ad una profondit superiore ai 12 cm e in fegati steatosici [ 20 , 31 ]  . multiple iniezioni di mezzo di contrasto possono rendersi necessarie per valutare lesioni situate in segmenti diversi dello stesso fegato e , a volte , anche per valutare una stessa lesione . il nostro studio presenta delle limitazioni . 
in primo luogo lo standard di riferimento non stato , in tutti i casi , la biopsia epatica , bens i criteri semeiologici alla tcmd e / o alla rm , ancorch noti in letteratura e comunemente impiegati nella pratica clinica . 
inoltre , da parte dei lettori stata effettuata una valutazione in consenso e , pertanto , non stato possibile valutare il grado di correlazione tra lettori indipendenti . in conclusione , nella nostra esperienza , la ceus pu essere considerata una valida alternativa alla tcmd ed alla rm al fine di una corretta diagnosi di benignit o malignit delle lfe , ottimizzando la gestione del paziente e riducendo , al contempo , il ricorso a metodiche di diagnostica per immagini pi costose o meno diffuse sul territorio . 
sardanelli universit degli studi di milano , dipartimento di scienze medico - chirurgiche , irccs policlinico san donato , servizio di radiologia , via morandi 30 , 20097 san donato milanese , milano , italy correspondence to : f . 
after approval from the ethics committee , we retrospectively evaluated 21 consecutive patients ( 6110 years ) with a healed myocardial infarction who underwent 1.5 - t magnetic resonance ( mr ) imaging using an inversion - recovery - prepared turbo gradient - echo sequence 10 minutes after injection of 0.1 mmol / kg of gdbopta . 
signal intensity ( si ) was measured in arbitrary units ( au ) for im , ib , vm , and outside the patient . contrast - to - noise ratio ( cnr ) was calculated for im to ib and im to vm . 
seven consecutive patients ( 596 years ) with a healed myocardial infarction studied with similar technique but with 0.1 mmol / kg of gadoterate meglumine ( gd - dota ) served as the control group . 
dopo approvazione del comitato etico , abbiamo valutato retrospettivamente 21 pazienti consecutivi ( et 6110 anni ) con infarto miocardico cronico studiati mediante risonanza magnetica ( rm ) a 1 , 5 t con sequenza inversion - recovery turbo gradient - echo 10 minuti dopo somministrazione di 0.1 mmol / kg di gdbopta . 
abbiamo misurato lintensit di segnale ( is ) in unit arbitrarie ( ua ) del mi , del sv , del ms e allesterno del paziente e calcolato il rapporto contrasto - rumore ( cnr ) tra mi e sv e tra mi e ms . 
una serie consecutiva di sette pazienti con infarto miocardico cronico ( et 596 anni ) , studiati con tecnica analoga e 0.1 mmol / kg di gadoterato meglumina ( gd - dota ) stata utilizzata come gruppo di controllo . 
no significant difference was observed for im to ib cnr . keywords cardiac magnetic resonance ( cmr ) delayed enhancement ( de ) gadobenate dimeglumine ( gdbopta ) gadoterate meglumine ( gd - dota ) myocardium conclusioni . 
il cnr tra mi e sv non significativamente diverso . parole chiave risonanza magnetica ( rm ) cardiaca delayed enhancement ( de ) gadobenato dimeglumina ( gd - bopta ) gadoterato meglumina ( gd - dota ) miocardio introduction introduzione myocardial delayed enhancement ( de ) on magnetic resonance ( mr ) imaging has emerged as a reliable indicator of myocardial infarction and scar extent [ 1 ]  . 
its value as a marker of myocardial fibrosis has also been shown to be advantageous for evaluating patients with myocardial infectious diseases , cardiomyopathies , cardiac neoplasms and congenital or genetic cardiac diseases [ 4 ]  . inflammatory and myocardial de is commonly evaluated using an inversion recovery ( ir ) t1 - weighted gradient - echo sequence 1020 minutes after an intravenous injection of a gadoliniumbased contrast agent . 
at this time point , nonviable myocardium typically demonstrates a strong hyperintense signal due to local high uptake and slow washout of contrast agent , whereas viable myocardium ( vm ) appears as strongly hypointense because of the nulling effect of the ir preparation and rapid washout of contrast agent [ 4 ]  . 
the time interval between contrast injection and mr imaging is not crucial for accurately estimating the size of the myocardial de , as stated by judd and kim [ 5 ]  . a controversial aspect is the dose of contrast material to be injected . 
 [ 6 ] compared identical double ( 0.2 mmol / kg body weight ) doses of a high - relaxivity mr contrast agent ( gadobenate dimeglumine , gd - bopta ) and a standard - relaxivity agent ( gadopentetate dimeglumine , gd - dtpa ) in patients with healed myocardial infarction using a prospective intraindividual study design . 
they found that the higher t1 - relaxivity of gd - bopta led to higher signal intensity ( si ) values for both infarcted myocardium ( im ) and intraventricular blood ( ib )  . 
nevertheless , the resulting contrast - to - noise ratio ( cnr ) between im and ib was significantly reduced in comparison with that obtained with the double dose of gd - dtpa [ 6 ]  . 
 [ 6 ] is that the dose of gdbopta used ( 0.2 mmol / kg ) was too high , given the greater in risonanza magnetica ( rm ) , il delayed enhancement ( de ) miocardico un indicatore affidabile di infarto miocardico e di estensione della corrispondente cicatrice [ 1 ]  . 
il de miocardico diffusamente considerato lapproccio non invasivo di prima scelta per valutare la vitalit miocardica dopo infarto [ 2 , 3 ] mentre la capacit di evidenziare fibrosi miocardica si pu rivelare vantaggiosa nello studio di patologie miocardiche infiammatorie o infettive , cardiomiopatie , neoplasie e patologie cardiache congenite o genetiche [ 4 ]  . comunemente il de miocardico valutato mediante sequenze gradient - echo inversion - recovery ( ir ) pesate in t1 acquisite 1020 minuti dopo iniezione endovenosa di mezzo di contrasto ( mdc ) a base di gadolinio . 
tipicamente il miocardio non vitale caratterizzato da un segnale altamente iperintenso dovuto a elevato uptake e lento wash out locale del mdc , mentre il miocardio sano ( ms ) appare nettamente ipointenso sia per effetto della preparazione ir sia per il rapido wash out del mdc [ 4 ]  . 
 [ 6 ] hanno confrontato luso di doppia dose ( 0 , 2 mmol / kg peso corporeo ) di mdc ad alta relassivit ( gadobenato dimeglumina , gd - bopta ) rispetto alla stessa dose di mdc a relassivit standard ( gadopentetato dimeglumina , gd - dtpa ) con uno studio prospettico intraindividuale in pazienti con infarto miocardico cronico . 
i loro risultati mostrano come lalta relassivit del gd - bopta comporti valori di intensit di segnale ( is ) pi elevati sia per il miocardio infartuato ( mi ) che per il sangue ventricolare ( sv )  . 
 [ 6 ] lutilizzo della doppia dose di gd - bopta ( 0 , 2 mmol / kg ) , probabilmente eccessiva a causa dellelevata relassivit t1 di questo mdc [ 7 ]  . 
questa caratteristica , infatti , determina a tale dose una marcata riduzione del t1 del sv che provoca un effetto paradosso sul cnr [ 7 ]  . radiol med ( 2010 ) 115 : 693701 t1 - relaxivity of this agent [ 7 ]  . 
the greater t1 - relaxivity of gd - bopta , leading to a larger t1 - shortening of ib , has been defined as resulting in a paradoxical effect on cnr if a too high ( double ) dose is used [ 7 ]  . 
findings were compared with a series of patients who received an equivalent single dose of a standard - relaxivity agent ( gadoterate meglumine , gd - dota )  . materials and methods study design and population institutional review board approval was received for this retrospective analysis , and patient informed consent was waived . 
from march 2005 to march 2006 , 21 consecutive patients [ 18 males , three females ; age 6110 years ( meanstandard deviation ) ] with healed myocardial infarction ( at least 4 weeks from the acute event [ 9 ] ) underwent cardiac mr imaging for myocardial de using 0.1mmol / kg body weight of gd - bopta ( multihance , bracco imaging spa , milan , italy ) as a contrast agent . 
a consecutive series of seven patients [ five men , two women ; age 596 years ( meanstandard deviation ) ] with healed myocardial infarction who underwent cardiac mr imaging between march 2004 and june 2004 with the same equipment and the same imaging technique but with 0.1 mmol / kg of gd - dota ( dotarem , guerbet , paris , france ) served as control group . mr imaging all mr examinations were conducted using a 1.5 - t unit with 40 - mt / m gradient power ( magnetom sonata , siemens , enlargen , germany ) and a four - channel cardiothoracic coil . images were acquired with an electrocardiographically triggered shortand long - axis ir - prepared turbo gradient - echo ( fast low - angle shot ) sequence acquired with the following technical parameters : repetition time , depending on the r - r interval of the cardiac cycle , acquiring every heartbeat ; echo inoltre , balci et al . 
 [ 8 ] hanno dimostrato che 0 , 1 mmol / kg di gd - bopta e 0 , 2 mmol / kg di gd - dtpa hanno la stessa efficacia nella valutazione del de miocardico , confermando quindi che con gd - bopta possibile ridurre la dose di mdc impiegata . lapproccio nellottimizzazione della dose di mdc quello di massimizzare il cnr tra mi e sv per migliorare la visualizzazione di piccoli infarti subendocardici che altrimenti potrebbero non essere diagnosticati . 
scopo di questo studio preliminare stato quindi misurare i valori di is di ms , sv e mi ottenuti con singola dose ( 0 , 1 mmol / kg ) di gd - bopta in pazienti consecutivi con infarto miocardico cronico e calcolare il cnr tra mi e sv e tra mi e ms . i risultati sono stati poi confrontati con quelli ottenuti in una serie di pazienti ai quali era stata somministrata una singola dose di mdc a relassivit standard ( gadoterato meglumina , gd - dota )  . materiali e metodi disegno dello studio e popolazione per questo studio retrospettivo stata ottenuta lapprovazione del comitato etico locale ( consenso informato non necessario )  . 
da marzo 2005 a marzo 2006 , 21 pazienti consecutivi [ 18 maschi , 3 femmine ; et 6110 anni ( mediadeviazione standard ) ] con infarto miocardico cronico ( almeno quattro settimane intercorse dallevento acuto [ 9 ] ) sono stati sottoposti a rm con somministrazione endovenosa di 0 , 1 mmol / kg di gd - bopta ( multihance , bracco imaging spa , milano , italia ) per la valutazione del de miocardico . 
una serie consecutiva di sette pazienti [ 5 maschi , 2 femmine ; et 596 anni ( mediadeviazione standard ) ] con infarto miocardico cronico , sottoposti a rm cardiaca tra marzo 2004 e giugno 2004 con la medesima apparecchiatura e analoga tecnica , ma con 0 , 1 mmol / kg di gd - dota ( dotarem , guerbet , parigi , francia ) , stata impiegata come gruppo di controllo . indagine rm tutte le indagini sono state eseguite mediante apparecchiatura a 1 , 5 t e gradienti di campo 40 mt / m ( magnetom sonata , siemens , enlargen , germania ) con una bobina cardio - toracica a quattro canali . 
sono state acquisite immagini asse lungo e asse corto con sequenze ir turbo gradient - echo ( fast low angle shot ) sincronizzate al tracciato elettrocardiografico , con i seguenti parametri tecnici : tempo di ripetizione in base allintervallo r - r del ciclo cardiaco acquisendo in ogni battito cardiaco ; tempo di eco da 1 , 0 a 4 , 3 ms ; flip angle 10 ; spessore di strato 5 mm ; ampiezza di banda 260 hz / pixel . 
both contrast agents were administered at a rate of 2 - 3 ml / s and were followed by a saline flush of 20 ml injected at the same rate . image analysis image analysis was performed on a remote workstation ( leonardo , siemens , enlargen , germany )  . 
the size of the roi inside the im needed to be small given the small de extent ( at least in transmural direction )  . as a consequence , to calculate a cnrs with an uncertainty of the same order as for de of im , rois inside the ib , inside the vm and outside the patient also needed to be small . 
per i pazienti ai quali stato somministrato gd - dota , il campo di vista impiegato risultato compreso tra 230350 mm2 e 400400 mm2 e la matrice tra 125192 e 168256 ( pixel tra 1 , 951 , 37 mm2 e 2 , 782 , 08 mm2 )  . 
il tempo dinversione , ottimizzato per ciascun paziente , risultato compreso tra 190 e 310 ms per i pazienti ai quali stato somministrato gd - bopta e tra 260 e 300 ms per i pazienti ai quali stato somministrato gd - dota . 
le immagini sono state acquisite circa dieci minuti dopo iniezione endovenosa di mdc , somministrato ad un flusso di 23 ml / s e seguito da 20 ml di soluzione fisiologica allo stesso flusso . analisi delle immagini lanalisi delle immagini stata eseguita su workstation dedicata ( leonardo , siemens , enlargen , germania )  . 
di conseguenza , per calcolare il cnr con lo stesso ordine di incertezza del de del mi , le roi nel sv , nel mi e allesterno del paziente dovevano essere di dimensioni altrettanto ridotte . 
1a , b short - axis inversion - recovery prepared fast low - angle shot images showing myocardial delayed enhancement obtained 10 minutes after an intravenous injection of 0.1 mmol / kg body weight of gadobenate dimeglumine ( a ) and 0.1 mmol / kg of gadoterate meglumine ( b ) in two different patients . 
1a , b immagini asse corto ( sequenza inversion - recovery fast low angle shot ) che mostrano delayed enhancement miocardico 10 minuti dopo liniezione intravenosa di 0.1 mmol / kg di gadobenato dimeglumina ( a ) e 0.1 mmol / kg di gadoterato meglumina ( b ) in due pazienti diversi . 
sia in a che in b sono visibili quattro regioni di interesse : nel miocardio infartuato ( 1 ) , allinterno del sangue ventricolare vicino alla superficie endocardica dellarea infartuata ( 2 ) , allinterno del miocardio sano ( 3 ) e in una regione esterna al paziente ( 4 )  . gd - bopta and gd - dota groups using the mannwhitney u test for asymmetric distributions . 
2. lis media del mi nel gruppo gd - bopta ( 4416 ua ; range 1872 ua ) risultata significativamente ( p < 0 , 001 ) pi elevata rispetto al gruppo gd - dota ( 206 ua ; range 1329 ua )  . 
il cnr medio tra mi e sv risultato lievemente maggiore dopo gd - bopta rispetto a quello dopo gd - dota ( 107 versus 85 , rispettivamente ) , sebbene la differenza non sia significativa ( p = 0 , 836 )  . 
2a , b signal intensity of infarcted myocardium ( im ) , intraventricular blood ( ib ) , and viable myocardium ( vm ) ( a ) as well as contrast to noise ratio between im and ib and between im and vm ( b ) for 21 patients who received 0.1 mmol / kg body weight of gadobenate dimeglumine and seven patients who received 0.1 mmol / kg of gadoterate meglumine ( inversion - recovery fast low - angle shot sequence ; te = 1.37 ms , flip angle = 10 , slice thickness = 5 mm )  . 
2a , b in a mostrata lintensit di segnale del miocardio infartuato ( im ) , del sangue ventricolare ( ib ) e del miocardio sano ( vm ) in 21 pazienti studiati con 0.1 mmol / kg di gadobenato dimeglumina e sette pazienti studiati con 0.1 mmol / kg di gadoterato meglumina ( sequenza inversion - recovery fast low angle shot con te = 1.37 ms , flip angle = 10 e spessore di strato = 5 mm )  . 
conversely , more recent intraindividual crossover studies evaluating gd - bopta at 0.1 mmol / kg versus gddtpa at 0.2 mmol / kg for both cnr and signal - to - noise ratio of im revealed equivalence between the two protocols il presente lavoro mostra che con 0 , 1 mmol / kg di gdbopta il cnr tra mi e ms maggiore rispetto a quello ottenuto con la stessa dose di gd - dota , mentre il cnr tra mi e sv non risulta significativamente differente . le implicazioni cliniche di questi risultati si basano sullimportanza del de nellimaging cardiaco . 
 [ 10 ] riportano che nel 28% dei casi impiegata una dose minore o uguale di 0 , 05 mmol / kg , mentre nel 42% e nel 21% dei casi sono impiegate dosi di 0 , 1 e 0 , 2 mmol / kg , rispettivamente . 
lampia variabilit tra gli studi analizzati suggerisce come non vi sia consenso sul dosaggio ottimale di mdc da utilizzare per lo studio del de miocardico . la visualizzazione di piccoli infarti subendocardici dipende prevalentemente dal cnr tra mi e sv e in rm cardiaca la scelta della dose ottimale di mdc molto importante soprattutto quando si utilizza un mdc ad alta relassivit quale il gd - bopt a . 
uno studio intraindividuale di confronto tra 0 , 2 mmol / kg di gd - bopta e la stessa dose di gd - dtpa ha evidenziato che con il primo mdc non si ottengono benefici , ma addirittura effetti negativi sul cnr tra mi e sv e sulla visualizzazione dellinfarto [ 6 ]  . 
viceversa , studi intraindividuali pi recenti che hanno confrontato 0 , 1 mmol / kg di gd - bopta con 0 , 2 mmol / kg di gddtpa nella valutazione sia del cnr che del rapporto segnale - rumore del miocardio infartuato hanno mostrato che i due protocolli sono equivalenti [ 8 ] oppure che la radiol med ( 2010 ) 115 : 693701 [ 8 ] or a superiority of gd - bopta at the low dosage [ 11 ]  . bassa dose di gd - bopta migliore [ 11 ]  . due to a weak and transient interaction of the gdbopta contrast - effective moiety with serum albumin , this agent has a roughly two - fold t1 - relaxivity in vivo when compared with gd - dtpa and other standard - relaxivity gadolinium - based agents [ 1215 ]  . 
on the other hand , the mean si of the ib after gd - bopta ( 3515 au ) was also more than double that after gd - dota ( 145 au )  . finally , the difference between the mean si of vm after gd - bopta and after gd - dota ( 73 au versus 52 au , respectively ) was not significantly different . 
the higher t1 - relaxivity of gd - bopta creates a limit for the effective dose for myocardial de , as the presence of residual contrast material in the ventricle during imaging of myocardial de reduces the im to ib cnr . 
firstly , it is a retrospective analysis rather than a prospective study . secondly , we compared two different series of patients who , despite being similar in terms of clinical presentation , age and sex , were nevertheless imaged over different time periods and without randomization . 
however , this approach has the double drawback of an unvaoidable lack of ( histopathological ) reference standard and the possible variability of the incidence of subendocardial infarctions in the two study arms . 
a il gd - bopta , grazie a una debole e transitoria interazione con lalbumina serica , dotato in vivo di relassivit t1 circa doppia rispetto al gd - dtpa e agli altri mdc a base di gadolinio dotati di relassivit standard [ 1215 ]  . 
nel nostro studio lis media del mi dopo somministrazione di gd - bopta ( 4416 ua ) risultata pi che doppia rispetto a quella dopo gd - dota ( 206 ua )  . 
daltro canto , anche lis media del sv dopo gd - bopta ( 3515 ua ) risultata pi che doppia che dopo gd - dota ( 145 ua )  . 
infine , non abbiamo rilevato differenza significativa tra lis media del ms dopo gd - bopta e quella dopo gd - dota ( 73 ua versus 52 ua , rispettivamente )  . 
tuttavia , il cnr tra mi e ms calcolato dopo gd - bopta ( 4527 ) significativamente maggiore ( p = 0 , 012 ) rispetto a quello dopo gd - dota ( 186 )  . 
lalta relassivit in t1 del gd - bopta pone un limite alla dose efficace da utilizzare per lo studio del de miocardico poich la presenza di mdc residuo nella cavit ventricolare riduce il cnr tra mi e sv . 
probabilmente questo limite stato raggiunto nello studio di schlosser et al . [ 6 ] perch con 0 , 2 mmol / kg di gd - dtpa il cnr tra mi e sv risultato significativamente maggiore rispetto a quello ottenuto con la stessa dose di gd - bopta [ 6 ]  . 
 [ 6 ] un ridotto cnr tra mi e sv potrebbe comportare una peggiore visualizzazione di piccoli infarti subendocardici , riducendo cos i potenziali vantaggi della maggiore risoluzione spaziale della rm rispetto a tecniche alternative , come ad esempio la scintigrafia miocardica , nella valutazione della vitalit del miocardio [ 16 , 17 ]  . 
 tuttavia , sebbene i nostri risultati suggeriscano che la singola dose ( 0 , 1 mmol / kg ) di gd - bopta possa consentire un elevato enhancement del mi senza limitare il riconoscimento degli infarti subendocardici , si dovrebbe considerare anche la possibilit che la singola dose ( 0 , 1 mmol / kg ) del mdc a relassivit standard ( gd - dota ) sia stata troppo bassa . 
tuttavia , questo approccio ha una duplice limitazione : linevitabile mancanza di uno standard di riferimento ( istopatologico ) e la possibile variabilit nei due bracci dello studio dellincidenza dellinfarto subendocardico . 
in due recenti studi [ 8 , 11 ] stato invece scelto un approccio alternativo , intraindividuale , 700 radiol med ( 2010 ) 115 : 693701 possible alternative approach is the intraindividual design , administering both contrast agents to each patient , as was done in two recent studies [ 8 , 11 ]  . 
at any rate , our study should be regarded as a preliminary retrospective evaluation of the differences between gd - bopta and a standard relaxivity contrast agent ( gd - dota ) at the single dose of 0.1 mmol / kg , which provides a rationale for planning a randomized or an intraindividual study . 
moreover , consecutive patients with healed myocardial infarctions ( at least 4 weeks from the acute event ) were evaluated in both series and the methodological approach was similar in both series . the small difference in spatial resolution used in the two patient series requires a comment . 
at any rate , a lower voxel volume for the gd - bopta group , reducing the signal to noise ratio and probably the cnr , can work only against the hypothesis of a better contrast performance of this agent . thus , this aspect makes our results in favor of gd - bopta more reliable . the need for a lower overall dose of gd - bopta might have important clinical implications in terms of safety , clinical and economic issues . 
a lower overall dose of contrast material may prove especially advantageous for certain patient populations undergoing cardiac mr , particularly given the reports about the association between high doses of contrast material and nephrogenic systemic fibrosis in patients with severe renal impairment [ 1820 ]  . however , this dose reduction should not affect the diagnostic performance , i.e. 
therefore , a potential advantage of the higher gdbopta relaxivity is that a lower overall dose is needed to achieve sufficient de of nonviable myocardium with adequate im to ib cnr . 
advantages and drawbacks of using gd - bopta as contrast agent for myocardial mr imaging at 3 t should be investigated , as already done for gd - dota [ 21 ]  . in conclusion , our preliminary results support the hypothesis that a dose of 0.1 mmol / kg of gd - bopta is more suitable than 0.1 mmol / kg of gd - dota for myocardial de . 
da questo punto di vista , il presente studio va inteso come una valutazione retrospettiva preliminare delle differenze tra una singola dose di 0 , 1 mmol / kg peso corporeo di gd - bopta e la stessa dose di un mdc a relassivit standard ( gd - dota ) nella prospettiva di uno studio randomizzato o intraindividuale . 
del resto , lapproccio metodologico stato simile per entrambe le serie , costituite da pazienti consecutivi con pregresso infarto miocardico ( ad almeno 4 settimane dallevento acuto )  . la piccola differenza di risoluzione spaziale utilizzata nelle due serie di pazienti richiede un commento . 
dato lo spessore di strato di 5 mm e considerando il valore mediano di entrambi gli intervalli ( ossia 3 , 75 mm2 e 4 , 25 mm2 ) le dimensioni dei voxel erano pari a 18 , 75 mm3 per il gruppo gd - bopta e 21 , 25 mm3 per il gruppo gd - dota con una differenza di 2 , 5 mm3 , ossia solo il 12 , 5% del volume medio del voxel ( 20 mm3 )  . 
in ogni caso , il voxel di minori dimensioni impiegato nel gruppo gd - bopta riduce comunque il rapporto segnale / rumore e probabilmente anche il cnr agendo a sfavore dellipotesi di una migliore performance contrastografica di questo mdc . 
ci rende pi affidabili i nostri risultati in favore del gd - bopta . la necessit di impiegare una minore dose di gd - bopta potrebbe avere importanti implicazioni per la sicurezza del paziente , oltre che cliniche ed economiche . 
una dose inferiore pu rivelarsi vantaggiosa soprattutto in alcuni sottogruppi di pazienti sottoposti a cardio - rm , in particolare dopo le segnalazioni dellassociazione tra elevate dosi di mdc e fibrosi nefrogenica sistemica in pazienti con insufficienza renale severa [ 1820 ]  . 
tuttavia , la riduzione della dose non dovrebbe ridurre la performance diagnostica , come ad esempio la capacit di visualizzare piccoli infarti subendocardici che , in definitiva , dipende dal cnr tra mi e sv . dal punto di vista clinico si dovrebbe anche considerare la possibilit che sia eseguito uno studio di perfusione ( a riposo e sotto stress farmacologico ) prima della valutazione del de miocardio . 
lelevata relassivit del gd - bopta rappresenta quindi un potenziale vantaggio in quanto rende necessaria una dose complessiva inferiore per ottenere un sufficiente de del miocardio non vitale con adeguato cnr tra mi e sv . vantaggi e svantaggi dellutilizzo del gd - bopta come mdc per limaging a rm del miocardio a 3 t dovranno essere valutati con studi dedicati , come ad esempio stato gi fatto per il gd - dota [ 21 ]  . 
 in conclusione , i nostri risultati preliminari supportano lipotesi che una dose di 0 , 1 mmol / kg di gd - bopta sia pi efficace di 0 , 1 mmol / kg di gd - dota nella valutazione del de miocardico . 
beomonte zobel1 1department of radiology , interdisciplinary center for biomedical research , 3endocrinology and diabetology unit , university campus bio - medico of rome , via alvaro del portillo 21 , 00128 rome , italy 2irccs , fondazione santa lucia , via ardeatina 306 , rome , italy correspondence to : f . 
we identified 166 women with the presence of at least one vertebral fracture . a questionnaire was administered to these women to collect information about diagnosis of osteoporosis , history of malignancy , systemic diseases , osteoporosis - inducing drugs and pharmacological , radiological or surgical treatment received . 
most of the patients were on menopause ( 97.1% , 98 / 101 ) with an average age of menopause of 48 , 2 years ( 6 years )  . 
attualmente non esistono linee guida che raccomandino uno screening nella popolazione di et avanzata e molte fratture rimangono non diagnosticate . lobiettivo del nostro studio quello di valutare prospetticamente la prevalenza delle fratture vertebrali visualizzate alla radiografia del torace e determinarne il ruolo diagnostico e prognostico calcolando il rischio di nuove fratture due anni dopo la prima diagnosi radiologica . 
da marzo 2004 ad ottobre 2005 , presso il nostro dipartimento di diagnostica per immagini , sono state eseguite 4045 radiografie del torace su donne che si sottoponevano a tale esame per svariate indicazioni . dallo studio di tali referti sono state individuate 166 donne con fratture vertebrali secondarie ad osteoporosi . 
delle 166 pazienti individuate ( et media 73 anni10 , 5 ) , con diagnosi di deformazioni o fratture 816 radiol med ( 2010 ) 115 : 815825 in 23.7% ( 24 / 101 ) of cases . 
a new skeletal fracture occurred in 20.5% ( 5 / 27 ) of patients receiving treatment against a frequency of 20.8% ( 16 / 74 ) in patients without treatment . 
for these reason we discuss about the evaluation of an adeguate therapeutic approaches in prevention of osteoporosis - induced fractures . keywords osteoporosis chest x rays vertebral fracture bisphosphonates vertebrali secondarie ad osteoporosi , sono state intervistate 101 donne ; 13 sono decedute e 52 non sono state intervistate per difficolt nel reperirle . 
la maggior parte di queste risultata in menopausa ( 97 , 1% , 98 / 101 ) e let media della menopausa stata di 48 , 2 anni ( 6 anni )  . 
delle 101 pazienti al corrente della malattia , il 23 , 7% ( 24 / 101 ) ne venuto a conoscenza solo in occasione della radiografia del torace da noi eseguita . 
un nuovo evento fratturativo si verificato nel 20 , 5% ( 5 / 27 ) delle pazienti in terapia contro una frequenza del 20 , 8% ( 16 / 74 ) delle pazienti che non avevano mai intrapreso alcun trattamento per losteoporosi . 
per tale ragione risulta necessario valutare le cause dellassenza di un adeguato approccio terapeutico nella prevenzione delle fratture indotte dallosteoporosi . parole chiave osteoporosi radiografia del torace frtture vertebrali bifosfonati introduction introduzione osteoporosis is a skeletal disorder characterised by compromised bone strength predisposing a person to an increased risk of fracture . 
in 1994 , an operational definition of osteoporosis was proposed by the world health organization ( who ) , with diagnostic criteria of fragility based on the measurement of bone mineral density ( bmd ) and the presence of fractures [ 1 ]  . 
based on the who criteria , 30% of postmenopausal caucasian women have osteoporosis of the hip , lumbar spine or distal forear the same frequency is observed fracture at one of these three sites in 50 - year - old women . 
during the first years after menopause , bone loss is accelerated , initially in the trabecular , then in the cortical compartment , and then it slows down [ 4 ]  . 
bone loss continues throughout losteoporosi rappresenta un disordine scheletrico caratterizzato da una compromissione della resistenza ossea che predispone un individuo ad un aumentato rischio di fratture . la rigidit ossea riflette principalmente una corretta integrazione tra le caratteristiche quantitative e qualitative dellosso . nel 1994 , unulteriore definizione venne proposta dallorganizzazione mondiale della sanit ( who ) con criteri diagnostici di fragilit basati sulla misura della densit minerale ossea ( bmd ) e sulla presenza di fratture [ 1 ]  . 
usando i criteri della who , il 30% delle donne caucasiche in post - menopausa affetto da osteoporosi alle anche , alla colonna lombare e a livello della porzione distale dellavambraccio . 
 la perdita ossea legata allet dipende dal sesso : durante i primi anni dopo la menopausa , la perdita ossea accelerata , inizialmente nel compartimento trabecolare , poi in quello corticale , per poi diminuire [ 4 ]  . 
the appearance of the vertebral endplate is helpful because the presence of areas of sclerosis in the middle portion of the endplate raises suspicion of a vertebral fracture , compared with spondylosis in with the endplates are well defined [ 8 ]  . 
a vertebral fracture appears as an alteration in the shape and size of the vertebral body , with a reduction in vertebral body height giving rise to wedge , endplate ( monoor biconcave ) or crush deformities . 
to improve evaluation , classification and description of vertebral fractures in clinical trials and epidemiological studies , grading techniques have been developed , and the term deformity is frequently used . 
a deformity is considered a fracture if visual inspection indicates a reduction in vertebral height of 20%25% or more and if deformities due to other causes ( congenital , developmental or degenerative ) are excluded [ 9 ]  . 
to our knowledge , no current guidelines recommend screening among the elderly population at large with formal spine radiographs ( perhaps because the cost is thought to be prohibitive or because of concerns about radiation exposure ) , and many fractures go undetected [ 10 ]  . 
inoltre negli uomini il picco di bmd pi elevato e la perdita ossea di minore entit ( 20%30% ) : per tale motivo lincidenza di fratture inferiore rispetto alle donne . 
un utile aiuto , nella diagnosi di fratture vertebrali , dato dallaspetto della limitante somatica del piatto vertebrale , poich la presenza di aree di sclerosi nella porzione centrale del piatto vertebrale depone per la diagnosi di frattura osteoporotica , a differenza di quanto avviene nelle spondilolisi , in cui il piatto vertebrale ha una superficie ben definita ed integra [ 8 ]  . 
una frattura vertebrale consiste in unalterazione nella forma e nelle dimensioni del corpo vertebrale , con una sua riduzione in altezza tale da costituire una deformazione a cuneo , a lente bi - concava o un crollo vertebrale . 
al fine di migliorare la valutazione , la classificazione e la descrizione delle fratture vertebrali nei trials clinici e negli studi epidemiologici sono state sviluppati diversi metodi di classificazione che utilizzano spesso il termine di deformazione vertebrale descrivendo il tipo e il grado di deformit . 
una deformazione viene definita frattura se il soma vertebrale presenta una riduzione daltezza superiore al 20%25% escludendo in tale classificazione le deformit congenite e quelle degenerative [ 9 ]  . 
al momento non esistono linee guida che raccomandino lo screening nella popolazione di et avanzata anche mediante una semplice radiografia della colonna vertebrale ( costi elevati , considerazioni legate al rischio da esposizione alle radiazioni ) e molte fratture rimangono non diagnosticate [ 10 ]  . 
una strategia potenzialmente utile potrebbe essere quella di analizzare studi radiografici eseguiti per altri motivi , come ad esempio la radiografia del torace ( cxr ) , e valutare leventuale presenza di lesioni vertebrali da osteoporosi . 
 lobiettivo dello studio dunque quello di : determinare lutilit delle radiografie del torace per diagnosticare fratture vertebrali precedentemente misconosciute ; e calcolare il rischio di nuove fratture , con e senza terapia , in un campione di donne italiane . materials and methods patients and study population materiali e metodi pazienti from march 2004 to october 2005 , 4 , 045 women underwent a chest radiograph for any clinical indication in our da marzo 2004 ad ottobre 2005 , presso il nostro dipartimento di diagnostica per immagini , sono state eseguite 818 radiol med ( 2010 ) 115 : 815825 department of radiology . 
non sono state considerate parte dello studio le pazienti con patologie neoplastiche , infiammatorie , metaboliche e degenerative , al fine di escludere le altre cause di fratture vertebrali non correlate allosteoporosi . tecnica diagnostica le radiografie del torace sono state effettuate in ortostatismo e nella massima apnea inspiratoria in due proiezioni : postero - anteriore ( distanza focale : 180 cm ; tensione 90 kv ; carico radiologico 100 ma ; tempo di esposizione 0 , 04 s ) e latero - laterale ( distanza focale : 180 cm ; tensione 90 kv ; carico radiologico 160 ma ; tempo di esposizione 0 , 05 s )  . interpretazione delle immagini per classificare le fratture vertebrali da osteoporosi stato utilizzato il metodo visivo semiquantitativo ( sq ) , descritto da genant et al . 
si caratterizza per una riduzione dellaltezza anteriore 4 mm rispetto a quella posteriore ; deformazione a lente biconcava : riduzione dellaltezza centrale del corpo vertebrale 4 mm rispetto allaltezza anteriore posteriore ; crollo vertebrale : riduzione di oltre 4 mm rispetto alla media delle altezze posteriori delle due vertebre adiacenti , superiore ed inferiore [ 12 , 13 ]  . we interviewed patients 2 years after detecting a vertebral deformity on cxr using a specific questionnaire including questions about awareness of osteoporosis and its related risks and occurrence of osteoporosis - related fractures in the time interval between the cxr and the questionnaire . information was also elicited regarding age at menopause , questionario le pazienti sono state intervistate due anni dopo lesecuzione della radiografia del torace che diagnosticava la deformazione vertebrale facendo uso di uno specifico questionario allo scopo di comprendere quante di loro fossero realmente a fig . 
1a - c deformit vertebrali indotte da osteoporosi ed individuate alla radiografia del torace : a deformazione a cuneo ; b deformazione a lente biconcava ; c crollo vertebrale . radiol med ( 2010 ) 115 : 815825 presence of pathological conditions increasing the risk of osteoporosis ( diabetes , hyperthyroidism , cushings disease , parathyroid disease ) , impaired intestinal absorption of calcium ( gastrectomy , colectomy , coeliac disease , malabsorption and lactose intolerance ) , autoimmune diseases and previous or ongoing medical treatments ( steroids , chemotherapy , oestrogen analogues )  . 
moreover , information was acquired regarding diagnostic integration by computerized bone mineralometry , quantitative computed tomography ( ct ) bone densitometry , scintigraphy , blood tests and medical , surgical or ongoing treatments . statistical analysis data were entered on an excel spreadsheet , and statistical tests were applied using the spss software package ( spss 14.0 version , chicago , il , usa )  . 
differences between groups were tested using the chi - square nonparametric test . two - by - two tables were used to estimate relative risk ( rr ) and odds ratios ( or )  . results patients among the 4 , 045 patients undergoing cxr for any reason from march 2005 to october 2006 , we identified 166 patients ( 4.1% ) with images and reports showing a vertebral fracture . 
in four patients , multiple ( up to three ) deformities were detected ; in 29 cases , kinking of the superior or inferior vertebral plates with reduction of the central height and marked reduction of bone attenuation were reported . 
 conoscenza della patologia in atto , e di risalire ad informazioni anamnestiche correlate alla patologia e ai rischi ad essa correlati , allo sviluppo di fratture correlate allosteoporosi nellintervallo di tempo tra la radiografia del torace e la data del questionario . 
inoltre sono state richieste informazioni sullet della menopausa , la presenza di condizioni patologiche correlabili ad un aumentato rischio di osteoporosi come diabete , ipertiroidismo , malattia di cushing , patologie paratiroidee , condizioni di alterato assorbimento intestinale di calcio come gastrectomia , colectomia , malattia celiaca , malassorbimento ed intolleranza al lattosio , patologie autoimmuni , precedente o concomitante assunzione di farmaci steroidi , chemioterapici o analoghi degli estrogeni . 
 stato inoltre chiesto alle pazienti se avessero trascorso lunghi periodi a letto o immobilizzate e in relazione allo stile di vita , in relazione ad una alimentazione povera di calcio , dal fumo di sigaretta e dallassunzione di alcolici . 
ulteriori informazioni sono state ottenute in merito allesecuzione di esami strumentali quali : mineralometria ossea ( moc ) , tomografia computerizzata ( tc ) quantitativa , scintigrafia e dosaggi ematici e alla terapia medica e chirurgica , nonch agli effetti dei presunti trattamenti . analisi statistica ai dati ottenuti , ordinati in una tabella excel , sono stati applicati test statistici utilizzando il sistema software statistical package for the social sciences ( spss ) ( versione spss 14.0 , chicago , usa )  . 
tabelle 22 sono state utilizzate per calcolare il rischio relativo e gli odds ratio . risultati pazienti delle 4045 radiografie del torace eseguite nel periodo compreso tra marzo 2004 e ottobre 2005 sono state individuate 166 pazienti ( 4 , 1% ) con immagini e referto radiologico diagnostici per frattura vertebrale . 
per tali ragioni la coorte da noi analizzata costituita da 101 pazienti , la maggior parte di queste in menopausa ( 97 , 1% ) e let media della menopausa di 48 , 2 anni ( 6 anni )  . 
the presence of these conditions , as well as of cardiovascular diseases such as hypertension , coronary artery disease , heart failure , valve disease and atrial fibrillation ( 40.3% ) was age dependent . 
among all 101 women , the diagnosis of osteoporosis was reported in the discharge sheet in only 36.3% of the cases , and only 35.1% of patients were prescribed medical treatment for osteoporosis . evaluation of risk of new fractures of the 101 patients interviewed , 34.6% ( 27 / 101 ) received pharmacological treatment for osteoporosis , whereas 65.4% ( 74 / 101 ) did not . 
a new fracture event ( pelvis , femur , vertebral bodies ) occurred in 20.5% ( 5 / 27 ) of patients in the first group versus 20.8% ( 16 / 74 ) in radiol med ( 2010 ) 115 : 815825 da : deformazioni a cuneo ( 43 , 9% ) ; deformazioni a lente biconcava ( 24 , 9% ) ; crolli vertebrali ( 11 , 4% )  . 
in 4 pazienti sono state individuate contemporaneamente la presenza di pi lesioni ; in 29 pazienti deformazioni delle limitanti somatiche , dismorfismi del margine inferiore o superiore dei piatti vertebrali con iniziali fenomeni di avvallamento delle limitanti somatiche , riduzione dampiezza dei corpi vertebrali e marcata porosi dei somi vertebrali con netta riduzione del tono calcico . campione analizzato ed informazioni ottenute tutti i risultati del questionario sono stati sintetizzati nella tabella 1 . 
tra i pazienti al corrente dellosteoporosi ( gruppo a : 76 , 2% ; et media 73 , 99 , 0 ) , le malattie riscontrate pi spesso sono rappresentate da : patologie tiroidee ( 32 , 5% ) , patologie gastriche quali ernia iatale , malattia da reflusso gastro - esofageo , gastrite ed ulcera ( 22 , 1% ) , dal diabete ( 18 , 2% ) e dalla gastrectomia ( 13 , 0% )  . 
tali patologie associate a patologie cardiovascolari ( 40 , 3% ) rappresentano i fattori correlati allet come lipertensione arteriosa , la cardiopatia ischemica , le valvulopatie , la fibrillazione atriale e laterosclerosi . 
un dato significativo rappresentato da pazienti con osteoporosi che riferiscono lunghi periodi di immobilizzazione ( 23 , 4% ) , storia di neoplasia mammaria ( 16 , 9% ) , e storia di patologie autoimmuni quali artrite reumatoide , lupus eritematoso sistemico , tiroiditi , atopie ed allergie alimentari ( 9 , 1% ) e lunghi periodi di assunzione di farmaci corticosteroidei ( 7 , 8% )  . per quanto riguarda il gruppo di pazienti che non erano al corrente della malattia ( gruppo b : 23 , 8% ; et media 68 , 611 , 7 ) , le condizioni patologiche pi frequentemente osservate , sono state : patologie cardiovascolari ( 29 , 2% ) , diabete , lunghi periodi di immobilizzazione ( 29 , 2% ) , patologie tiroidee ( 20 , 8% ) , patologie gastriche , gastrectomie ( 16 , 7% ) e terapia corticosteroidea ( 4 , 2% )  . 
nel gruppo a i farmaci pi frequentemente prescritti sono stati assunti calcio e vitamina d ( 25 , 5% ) mentre la terapia con aminobifosfonati solo nel 9% dei casi . le pazienti si sono sottoposte a trattamento chirurgico nel 5 , 1% dei casi con sintomi post - terapia sostanzialmente invariati nel 39 , 4% dei casi . 
the lateral projection of the cxr is able to show osteoporotic vertebral deformities on the dorsal spine , such as wedge , endplate or compression deformity , as recently confirmed [ 14 ]  . our study showed the absence of a significant difference in rr of new fractures between treated and untreated patients . 
these results raised doubts regarding the medical awareness of osteoporosis and its guidelines and , in general , showed a lack of clear information about the increased risk of new fractures in these patients and the purpose of osteoporosis treatments . most fractures we observed were wedge deformities ( 47% )  . 
vertebral fractures are strong predictors of future fractures and , in particular , in the study of osteoporotic fractures ( sof ) , fractures of the hip , pelvis , humerus and ribs have all been associated with increased mortality rates [ 16 , 17 ]  . 
the primary goal in the clinical settings is to evaluate the risk of mortality following a fracture ; in particular , the relative risk of death following a hip fracture has been estimated to be almost sixfold and ninefold higher among individuals who have experienced a spine fracture [ 18 ]  . 
demonstrated increased mortality rates following a hip and spine fracture in a group of relatively healthy older woman , supporting previous evidence of excess mortality following a hip fracture [ 18 ]  . valutazione del rischio di nuove fratture nel campione di 101 pazienti intervistate , il 34 , 6% ( 27 / 101 ) assumeva una terapia per la cura dellosteoporosi contro il 65 , 4% ( 74 / 101 ) che non aveva mai intrapreso alcun tipo di trattamento . 
un nuovo evento fratturativo ( bacino , femore , somi vertebrali ) si verificato nel 20 , 5% ( 5 / 27 ) delle pazienti appartenenti al primo gruppo , e nel 20 , 8% ( 16 / 74 ) delle pazienti appartenenti al secondo . 
in relazione a questi due parametri si pensato di calcolare il rischio di sviluppare una nuova frattura tra le pazienti in trattamento rispetto al rischio di nuova frattura nelle pazienti non in terapia . 
il rischio relativo di nuove fratture stato stimato corrispondere ad 1 , 17 indicando che le pazienti che non hanno fatto terapia hanno una probabilit del 17% pi alta di riportare nuove fratture rispetto alle pazienti in terapia . 
la proiezione latero - laterale della radiografia del torace permette di individuare le deformazioni vertebrali da osteoporosi , quali deformazioni a cuneo , a lente biconcava e crolli vertebrali nel tratto dorsale del rachide [ 14 ]  . il nostro studio ha mostrato lassenza di una differenza significativa del rischio di nuove fratture tra le pazienti trattate e non trattate . 
tra le donne con diagnosi alla radiografia del torace di deformazioni vertebrali , solo il 35% ha ricevuto la prescrizione di un trattamento medico adeguato per losteoporosi , suggerendo una bassa considerazione della patologia nellambito medico . 
tali risultati ci hanno portato a dubitare sulla validit delladesione alla terapia medica e le linee guida ad essa relativa hanno mostrato scarsa chiarezza delle informazioni riguardanti laumentato rischio di nuove fratture in queste pazienti e gli obiettivi del trattamento per losteoporosi . la maggior parte delle fratture riscontrate sono state le deformazioni a cuneo ( 47% ) : tale fenomeno , non ancora dimostrato , potrebbe essere correlato allazione meccanica indotta dalla fisiologica cifosi del rachide dorsale [ 15 ]  . 
le fratture vertebrali sono altamente predittive di insorgenza di fratture secondarie , in particolare dallo studio delle fratture da osteoporosi ( study of osteoporotic fractures , sof ) emerso un aumento del tasso di mortalit secondario a fratture di femore , bacino , omero e coste [ 16 , 17 ]  . 
il principale obiettivo nella valutazione clinica di tali pazienti infatti quello di valutare il rischio di mortalit successivo ad una frattura ; in particolare il rischio relativo di decesso 824 radiol med ( 2010 ) 115 : 815825 vertebral fractures are often asymptomatic . 
this may cause an underestimation of the problem and lead to underreporting on routine chest radiographs [ 19 ] or to inadequate treatment following incidental detection on cxr examinations [ 20 ]  . 
population - based studies have estimated that 12%25% of people between 50 and 60 years old have one or more osteoporotic vertebral fractures , whereas only 30% of these are documented in the medical reports . 
in our case , the relatively low prevalence ( 4.1% ) could in part be explained by the lack of evaluation of other skeletal segments of the spine , such as the lumbar tract [ 21 ]  . 
our analysis showed that 38% of the women aware of osteoporosis underwent bmd or quantitative ct as a more specific diagnostic examination for bone density in comparison to only 12% of patients unaware of osteoporosis . 
 the international guidelines on osteoporosis [ 22 ] indicate that after a diagnosis of osteoporosis - related fractures or in the presence of t scores > 2.0 , drug treatment should be initiated with alendronate , risedronate and generally all bisphosphonates as first - line therapy . 
alternatively , parathyroid hormone ( teriparatide ) has been shown to improve bmd and reduce the risk of new vertebral and nonvertebral fractures in women with a previous vertebral fracture [ 23 , 24 ]  . 
in contrast to the guidelines , the patients interviewed in our study received calcium and vitamin d supplementation in 25.5% of cases and bisphosphonates alone or combined with calcium and vitamin d supplementation in only 9% of cases . in summary , this retrospective study suggests that this population received low consideration regarding the diagnosis of osteoporosis , as well as inadequate medical treatment according to the established international guidelines . 
evaluation and diagnosis of vertebral fractures at cxr could represent a first step to increased medical awareness of osteoporosis . secondario a frattura di femore stato stimato essere 67 volte maggiore dopo una frattura vertebrale [ 18 ]  . 
 [ 18 ] hanno dimostrato un aumento del tasso di mortalit dopo una frattura di femore successiva ad una frattura vertebrale in un gruppo di pazienti di et avanzata supportando levidenza di un eccesso di mortalit successivo a tali fratture [ 18 ]  . le fratture vertebrali sono spesso asintomatiche . 
per tale ragione potrebbero rimanere misconoscute ed essere sottovalutate nella refertazione delle radiografie del torace [ 19 ] o seguite da un trattamento inadeguato successivo al loro occasionale riscontro [ 20 ]  . 
gli studi basati sulla popolazione hanno stimato che il 12%25% degli individui tra 50 e 60 anni di et hanno una o pi fratture vertebrali da osteoporosi , sebbene solo il 30% di queste siano state documentate nei referti medici . 
nel nostro caso la bassa prevalenza di tali lesioni , pari al 4 , 1% pu essere spiegata anche in relazione ad una mancata valutazione degli altri segmenti scheletrici del rachide [ 21 ]  . 
il nostro studio ha dimostrato che il 38% delle donne al corrente della patologia ha eseguito una moc o una tc quantitativa rispetto al solo 12% delle pazienti nel gruppo non al corrente della malattia . 
 le linee guida internazionali sullosteoporosi [ 22 ] indicano che dopo la diagnosi di fratture vertebrali correlate allosteoporosi o in presenza di un t - score > 2 , 0 , deve essere intrapreso il trattamento farmacologico con alendronato , risedronato o con bifosfonati di prima linea . 
in alternativa lormone paratiroideo ( teriparatide ) ha mostrato un incremento della densit minerale ossea e una riduzione del rischio di nuove fratture vertebrali e non in donne con una precedente diagnosi di frattura vertebrale [ 23 , 24 ]  . 
diversamente da quanto espresso dalle linee guida , le pazienti intervistate hanno eseguito una terapia con calcio e vitamina d ( 25 , 6% ) e con aminobifosfonati ( 9 , 0% ) peraltro assunti saltuariamente e per brevi periodi . questa analisi retrospettiva ci suggerisce che tale popolazione ha ricevuto una scarsa considerazione in relazione alla diagnosi di osteoporosi ed un inadeguato trattamento medico rispetto alle linee guida stabilite in ambito internazionale . 
passariello1 1department of radiological sciences , university of rome sapienza , policlinico umberto i , viale regina elena 324 , 00161 rome , italy 2department of radiology , duke university medical center ; durham , nc , 27710 , usa 3 ospedale icot , university of rome sapienza , via franco faggiana 34 , 04100 latina , italy correspondence to : a . 
the aim of this study was to assess the accuracy of translucency rendering ( tr ) in computed tomographic ( ct ) colonography without cathartic preparation using primary 3d reading . 
for faecal tagging , all patients ingested 140 ml of orally administered iodinated contrast agent ( diatrizoate meglumine and diatrizoate sodium ) at meals 48 h prior to ct colonography examination and two h prior to scanning . ct colonography was performed using a 64 - section ct scanner . 
per marcare il materiale fecale era stato somministrato per os , a tutti i pazienti , un quantitativo di 140 ml di mezzo di contrasto iodato ( diatrizoato di dimeglumina e diatrizoato di sodio ) nelle 48 ore precedenti lesame di colografia con tc . 
le formazioni endoluminali sono state suddivise nei seguenti gruppi : formazioni piccole ( di dimensioni 5 mm ) , intermedie ( di dimensioni comprese tra 6 e 9 mm ) e grandi ( di dimensioni 10 mm ) , al fine di rendere possibile lanalisi statistica in base alle dimensioni . 
il tr uno strumento diagnostico accurato che permette di agevolare linterpretazione delle immagini ottenute con unanalisi primaria 3d , facilitando la distinzione tra polipi e formazioni pseudopolipoidi . parole chiave colografia con tc translucency rendering analisi tridimensionale ( 3d ) introduction introduzione computed tomographic ( ct ) colonography is a minimally invasive , total colonic examination that is increasingly used to detect colorectal polyps and colorectal cancer [ 1 , 2 ]  . 
 recently , a large multicentre clinical trial has shown no significant difference in the diagnostic accuracy of ct colonography for adenomas > 10 mm using either a primary 2d or 3d reading [ 3 ]  . 
although remarkable improvements in ct colonography systems have led to increasingly faster automated 3d fly - through analyses of the colon [ 4 , 5 ] , the 3d approach tends to be hampered by longer interpretation times [ 3 ]  . 
this is further compounded by the fact that 3d analysis needs to be invariably supplemented by 2d analysis to characterise identified colonic lesions [ 4 , 7 ]  . translucency rendering ( tr ) , a 3d tool developed as part of ct colonography software package ( v3d - colon , viatronix , stony brook , ny , usa ) can be easily applied during primary 3d analysis to provide real - time analysis of colonic endoluminal lesion density . 
 la colografia con tomografia computerizzata ( tc ) rappresenta un esame minimamente invasivo per lo studio completo del lume colico ed attualmente una metodica di crescente utilizzo per la diagnosi dei polipi e del cancro colorettale [ 1 , 2 ]  . 
questa tecnica pu essere condotta con limpiego sia di una visualizzazione bidimensionale ( 2d ) del lume colico sia di una visualizzazione tridimensionale ( 3d ) ; attualmente entrambe le modalit di visualizzazione sono essenziali per una corretta valutazione del lume colico . recentemente , un importante trial clinico multicentrico non ha evidenziato alcuna differenza statisticamente significativa riguardo laccuratezza diagnostica della colografia con tc per adenomi di dimensioni 10 mm , sia che fosse utilizzata una lettura delle immagini 2d primaria sia una in 3d [ 3 ]  . 
sebbene i notevoli miglioramenti apportati ai sistemi di visualizzazione di colografia con tc abbiano contribuito a velocizzare la navigazione virtuale e , di conseguenza , lanalisi 3d del colon [ 4 , 5 ] , lo studio 3d del colon resta ancora caratterizzato da tempi di interpretazione pi lunghi [ 3 ]  . 
infatti , per consentire al lettore una visualizzazione completa del lume colico , lanalisi 3d richiede assolutamente di una navigazione bidirezionale ( retrograda ed anterograda ) del lume colico [ 6 ]  . 
il translucency rendering ( tr ) uno strumento 3d integrato in un software specifico , dedicato allinterpretazione della colografia con tc ( v3d - colon system , viatronix , stony brook , ny ) , che pu essere facilmente applicato durante la navigazione 3d in modo da fornire unistantanea analisi della densit di una lesione colica endoluminale . 
il tr permette di distinguere una vera lesione ( sia polipi che formazioni neoplastiche ) dalle formazioni pseudopolipoidi di pi frequente impatto clinico ( residuo fecale , valvola ileo - cecale [ icv ] , lipoma , diverticolo impattato da materiale fecale ) [ 8 ] quando le feci vengono marcate con un 760 radiol med ( 2010 ) 115 : 758770 although one preliminary study has suggested the clinical usefulness of tr for interpreting ct colonography examinations [ 8 ] , to our knowledge , the diagnostic accuracy of this tool for lesion characterisation has not yet been determined . 
the purpose of our study was to retrospectively assess the sensitivity , specificity , and diagnostic accuracy of tr in differentiating polyps from pseudopolyps using a primary 3d endoluminal analysis . 
con lutilizzo di un approccio di visualizzazione 3d primario , il tr potrebbe agevolare la caratterizzazione delle lesioni coliche endoluminali e ridurre il numero delle correlazioni lesione per lesione 2d supplementari . per quanto ci risulta , laccuratezza diagnostica di questo strumento per la caratterizzazione delle lesioni coliche non stata ancora valutata , sebbene uno studio preliminare abbia gi suggerito limpiego e lutilit clinica del tr nellinterpretazione della colografia con tc [ 8 ]  . 
il presente studio stato condotto con lo scopo di analizzare retrospettivamente la sensibilit , la specificit e laccuratezza diagnostica del tr nella differenziazione tra polipi e formazioni pseudopolipoidi endoluminali utilizzando un approccio di visualizzazione 3d primario . study group and lesion selection materiali e metodi a total of 350 patients with 482 endoscopically verified polyps underwent ct colonography . 
by using a random number table , a subset of 50 adenomatous colorectal polyps and 50 pseudopolyps , consisting of 40 faecal residues and ten icvs , were selected in 39 patients ( 24 men and 15 women ; mean age 62 years ; age range 3580 years )  . 
polyp morphology was sessile for 32 lesions ( 64% ) , pedunculated for 12 ( 24% ) and flat for six ( 12% )  . subsequently criteria for residual faecal material included lack of size or location matching or both at optical colonoscopy , and at least one of the following findings : ( 1 ) lesion mobility when the patient was moved from the prone to the supine position , per questo studio retrospettivo stata ottenuta lapprovazione del nostro consiglio di istituto con esonero dallacquisire il consenso informato del paziente . popolazione di studio e selezione delle lesioni trecentocinquanta pazienti con 482 polipi verificati endoscopicamente sono stati sottoposti ad esame di colografia con tc . 
utilizzando una tabella di numeri casuali 50 polipi , adenomatosi colorettali e 50 formazioni pseudopolipoidi endoluminali , che includevano 40 residui fecali e 10 valvole ileo - cecali , sono stati selezionati in 39 pazienti ( 24 uomini e 15 donne , et media 62 anni , fascia di et 3580 anni )  . 
i criteri di inclusione dei polipi sono stati i seguenti : ( i ) lesione localizzata in un segmento colico ben disteso daria , ( ii ) inequivocabile corrispondenza positiva alla colonscopia ottica e ( iii ) la disponibilit della diagnosi istopatologica . 
una corrispondenza positiva tra i due esami si verificava quando la lesione , che era localizzata nello stesso segmento colico , mostrava le stesse dimensioni ( con un margine derrore del 50% ) e si riscontrava una morfologia simile nei due esami [ 12 ]  . 
importante sottolineare che , durante lanalisi 3d , in colografia con tc la misurazione delle lesioni potrebbe essere influenzata dal valore di soglia del surface rendering ( per quelle lesioni polipoidi sommerse , quando la tecnica del fecal tagging viene utilizzata ed il software 3d non dispone di uno strumento per la rimozione elettronica del materiale fecale marcato ) [ 13 ]  . 
tutti i polipi sono stati verificati e conseguentemente rimossi allesame di colonscopia ottica eseguito entro due settimane dopo lesame di colografia con tc ( intervallo medio , 8 giorni ; range , 214 giorni )  . 
le diagnosi istologiche definitive comprendevano : adenoma tubulare ( n = 28 ) , adenoma villoso ( n = 10 ) ed adenoma tubolovilloso ( n = 12 )  . 
trentadue lesioni radiol med ( 2010 ) 115 : 758770 ( 2 ) angled borders or geometric morphology on 3d endoluminal view and ( 3 ) areas of either low or high attenuation on 2d images using a soft - tissue window , likely related to trapped gas and retained particles of orally administered contrast material ( see below , ct colonography ) , respectively . 
criteria for an icv included : ( 1 ) a polypoid morphology on 3d endoluminal view and on 2d images , ( 2 ) demonstration of direct communication with the terminal ileum and / or ( 3 ) substantially lower internal attenuation compared with that of the adjacent colonic wall [ 1416 ]  . 
 to enable size - dependent statistical analysis , lesions were stratified into the following size categories : small ( 5 mm ) , intermediate ( 69 mm ) and large ( 10 mm )  . 
 i criteri di inclusione per i residui fecali comprendevano la mancanza di una corrispondenza positiva delle dimensioni e della localizzazione o entrambe alla colonscopia ottica ed almeno uno dei seguenti reperti : ( 1 ) la mobilit della lesione al cambiamento di decubito del paziente da prono a supino , ( 2 ) i bordi angolari o una morfologia geometrica alla rappresentazione 3d , e ( 3 ) nelle immagini 2d , applicando la finestra per i tessuti molli , la presenza di aree con valori di bassa o alta attenuazione riferibili rispettivamente a bolle gassose e particelle di contrasto ( vedi sotto , paragrafo colografia tc )  . 
i criteri di inclusione per le valvole ileo - cecali includevano ( i ) levidenza di una morfologia polipoide allanalisi 3d endoluminale e , nelle immagini 2d , ( ii ) la dimostrazione di una diretta comunicazione con il tratto terminale dellileo , e / o ( iii ) la presenza di pi bassi valori di attenuazione internamente alla formazione rispetto alla parete colica adiacente [ 1416 ]  . 
 le formazioni polipoidi sono state suddivise nei seguenti gruppi : formazioni piccole ( di dimensioni 5 mm ) , intermedie ( di dimensioni comprese tra 6 e 9 mm ) , grandi ( di dimensioni 10 mm ) , al fine di rendere possibile lanalisi statistica in base alle dimensioni . 
c , cieco ; ac , colon ascendente ; sf , flessura splenica ; tc , colon trasverso ; hf , flessura epatica ; dc , colon discendente ; sc , colon sigma ; r , retto . cathartic agent was administered to the patients . 
scanning was performed craniocaudally during a single breath - hold ( scanning time 49 s ) , both in the prone and supine positions . before the examination , the colon was gently distended by means of a standard hand - held enema bulb attached to a small flexible rectal catheter positioned in the rectum , according to the patients tolerance . 
to improve distension of the colon , 20 mg of n - butylbromide ( buscopan , boehringer , ingelheim , germany ) or , when contraindicated , 1 mg of glucagon hydrochloride ( glucagen , novo - nordisk , bagsvaerd , denmark ) was administered intravenously prior to the examination . 
 optical colonoscopy optical colonoscopy was performed by a gastroenterologist ( blinded for the review process ) with experience of > 2 , 000 cases using a video colonoscope ( cv - 1 ; olympus , tokyo , japan )  . 
during scope withdrawal , the operator recorded the number , site , size , and morphology of the identified lesions . lesion sites were determined using endoscopic references at la marcatura delle feci stata ottenuta istruendo tutti i pazienti ad ingerire per os 140 ml di mezzo di contrasto iodato diluito ( 20 ml tre volte al giorno ai pasti durante le 48 ore prima dellesame di colografia con tc e le rimanenti 20 ml due ore prima dellesame [ 9 , 17 ] )  . 
 la colografia con tc stata eseguita utilizzando un apparecchio multidetettore 64 strati ( sensation 64 , siemens medical solutions , erlangen , germania ) con i seguenti parametri : collimazione , 640 , 6 mm ; spessore di strato , 1 mm ; intervallo di ricostruzione , 1 , 5 mm ; tempo di rotazione del gantry , 0 , 33 secondi ; mas effettivi , 50 ; e kvp , 120 . 
la scansione stata eseguita in senso cranio - caudale durante una singola apnea respiratoria ( tempo di scansione , da 4 a 9 secondi ) in entrambi i decubiti , prono e supino . 
prima della scansione tc , il colon stato disteso con attenzione , utilizzando una pompetta a mano , attaccata ad un catetere rettale flessibile posizionato nel retto , secondo la tolleranza del paziente . 
per migliorare la distensione del colon , 20 mg di n - butilbromuro ( buscopan , boehringer , ingelheim , germania ) o , quando controindicato , 1 mg di glucagone cloridrato ( glucagen , novo - nordisk , bagsvaerd , danimarca ) stato somministrato per via endovenosa prima dellesame . prima di ogni scansione tc ladeguata distensione del colon stata accertata dallacquisizione di unimmagine scout tc anteroposteriore . 
quando uno o pi segmenti colici non erano chiaramente identificati , aria aggiuntiva veniva insufflata nel colon . colonscopia ottica la colonscopia stata eseguita da un gastroenterologo ( non nominato per il processo di revisione ) con unesperienza di pi di 2000 casi utilizzando un videocolonscopio ( cv - 1 , olympus , tokyo , giappone )  . 
however during optical colonoscopy , image distortion in the periphery of an endoscopic field associated with the wide - angle lens of an endoscope can cause size underestimation [ 18 ]  . 
 image analysis images were analysed on a commercially available ct colonographic workstation ( v3d - colon system ) , which allows analysis with both endoluminal 3d surface - rendered images and 2d multiplanar reformations following automated digital subtraction of high - attenuating tagged faecal material , known as electronic cleansing [ 8 ]  . with knowledge of ct colonographic and colonoscopic data , a radiology resident ( m.d.m. ) positively marked all individual lesions , either polyps or pseudopolyps , by adding a bookmark to indicate their location on the corresponding 3d endoluminal image . 
before image interpretation , readers were informed of the location and maximum diameter of each endoluminal lesion , but they were unaware of whether an individual lesion represented either a true polyp or a pseudopolyp , as well as the relative percentages of polyps and pseudopolyps in each study group . 
readers were instructed to characterise all annotated lesions according to a four - point confidence scale : ( 1 ) definite pseudopolyp ; ( 2 ) probable pseudopolyp ; ( 3 ) probable polyp ; ( 4 ) definite polyp . 
a polyp was unequivocally diagnosed if a lesion showed a soft - tissue density that increased progressively from the periphery towards the centre as multiple concentric rings of different colours ( from blue to red , respectively )  . 
a faecal residue was diagnosed if a lesion fulfilled either of the two following criteria : ( 1 ) internal areas of markedly increased attenuation ( assigned a white colour at tr display ) that were considered to correspond with retained high - density contrast material , or ( 2 ) internal areas of air attenuation ( assigned a blue colour at tr display ) due to trapped gas bubbles . 
for the purpose of this study , an icv was diagnosed only if a caecum lesion showed internal areas of fat attenuation ( assigned a green colour at tr display ) , corresponding to regions of valve lipohyperplasia . 
tuttavia , durante la colonscopia ottica , la distorsione spaziale dovuta allobiettivo grandangolare dellendoscopio pu , a volte , precludere una corretta misurazione delle dimensioni , sottostimando il diametro delle lesioni [ 18 ]  . analisi delle immagini le immagini sono state analizzate mediante lutilizzo di una workstation dedicata per la colografia con tc ( v3d - colon system , viatronix , stony brook , ny , usa ) , disponibile sul mercato , che ha permesso lanalisi delle immagini 3d e multiplanari 2d avvalendosi di uno strumento per la rimozione elettronica del materiale fecale marcato con il mezzo di contrasto , tecnica conosciuta come electronic cleansing [ 8 ]  . uno specializzando in radiodiagnostica ( m.d.m. ) , avendo a conoscenza i dati della colografia con tc e della colonscopia ottica , ha evidenziato tutte le lesioni , polipi e formazioni pseudopolipoidi , localizzandole con una freccia nella corrispondente immagine 3d endoluminale . 
prima dellinterpretazione delle immagini , gli stessi lettori erano informati della localizzazione e del massimo diametro di ogni formazione endoluminale , senza tuttavia venire a sapere se la singola formazione rappresentasse un polipo o una formazione pseudopolipoide n quale fosse la percentuale dei polipi e delle formazioni pseudopolipoidi in ogni gruppo di studio . 
i lettori sono stati istruiti a definire le lesioni in base ad una scala di 4 punti di confidenza ( 1 pseudopolipo ; 2 , probabile pseudopolipo ; 3 probabile polipo ; 4 , polipo ) valutando lanalisi densitometrica ottenuta sovrapponendo il tr allimmagine 3d endoluminale . 
un polipo era diagnosticato con certezza se , nellimmagine 3d con il tr sovrapposto , si evidenziavano anelli concentrici di colore differente corrispondenti a valori densitometrici che aumentavano progressivamente dalla periferia verso il centro ( dal blu al rosso in sequenza ) della lesione . 
un residuo fecale veniva diagnosticato quando la formazione endoluminale rispettava uno dei due seguenti criteri : ( i ) aree interne con valori di attenuazione elevati ( rappresentate dal colore bianco nellimmagine con il tr ) che corrispondevano a particelle di contrasto ad elevata 764 radiol med ( 2010 ) 115 : 758770 a polypoid endoluminal lesion was classified as a probable pseudopolyp or probable polyp when a nonspecific tr colour pattern was represented , although the readers were more confident with a pseudopolyp diagnosis or polyp diagnosis on the basis of which colour pattern was predominant . these diagnostic criteria were based on knowledge gained from our own prior clinical experience with tr and were corroborated by similar evidence in the literature [ 8 ]  . 
 finally , following lesion interpretation , each reader evaluated the overall effectiveness of tagging by visually assessing the mean percentage of faecal labelling ( from 0% to 25% , poor ; from 25% to 50% , moderate ; from 50% to 75% , good ; from 75% to 100% , excellent ) for all colonic segments on 2d images without electronic cleansing [ 19 ]  . to determine the reasons for any diagnostic errors , the three readers in consensus retrospectively reviewed both falsenegative and false - positive findings using a combined 2d / 3d image analysis . 
 statistical analysis to determine sensitivity and specificity , all polyps were classified as positive findings , whereas pseudopolyps , i.e. faecal residues and icvs , were classified as negative findings . 
the three readers reported five false - negative misinterpretations , including a 6 - mm sessile polyp of the transverse colon for all readers , a 5 - mm pedunculated polyp of the rectum for reader 2 and a 5 - mm flat polyp of the densit trattenute nel residuo , o ( ii ) aree con valori di bassa attenuazione riferibili a bolle di aria ( rappresentate dal colore blu nellimmagine con il tr )  . 
per i fini dello studio , la valvola ileo - cecale veniva diagnosticata solo se una formazione localizzata nel cieco mostrava aree con valori di attenuazione relativi al tessuto adiposo ( rappresentate dal colore verde nellimmagine con il tr ) corrispondenti a lipoiperplasia della valvola . 
 una lesione endoluminale veniva invece classificata come probabile pseudopolipo o probabile polipo quando non presentava nellimmagine 3d con il tr il rispettivo specifico pattern di colori sebbene i lettori potessero avere una maggiore confidenza diagnostica rispettivamente di formazione pseudopolipoide o polipo sulla base del pattern di colori prevalentemente rappresentata . 
 infine , dopo lanalisi delle immagini 3d con il tr , ogni lettore ha valutato nelle immagini 2d senza electronic cleansing , lefficacia complessiva della marcatura per tutti i segmenti colici riportando visivamente la percentuale media della marcatura del materiale fecale ( da 0% a 25% , povera ; da 25% a 50% , moderata ; da 50% a 75% , buona ; da 75% a 100% , ottima ) [ 19 ]  . 
per determinare la causa di tutti gli errori diagnostici i tre lettori hanno rivalutato retrospettivamente in consenso sia i falsi negativi sia i falsi positivi con lanalisi delle immagini combinata 2d / 3d . analisi statistica al fine di determinare la sensibilit e la specificit del tr , tutti i polipi sono stati classificati come reperti positivi , mentre le formazioni pesudopolipoidi , ad esempio , residui fecali e valvole ileo - cecali , sono stati considerati come reperti negativi . 
i valori di kappa4 evidenziavano poca concordanza tra i lettori ; invece valori tra 0 , 410 , 80 e > 0 , 81 indicavano rispettivamente una buona ed ottima concordanza . 
lintera analisi statistica stata eseguita adottando il software sas ( versione 9.1.3 , sas , cary , usa )  . risultati la sensibilit media per i lettori 1 , 2 e 3 del tr per la caratterizzazione dei polipi risultata del 98% ( 0 , 890 , 99 ) , 96% ( 0 , 860 , 98 ) , e 96% ( 0 , 860 , 98 ) , rispettivamente ; radiol med ( 2010 ) 115 : 758770 table 1 sensitivity for polyp ( n = 50 ) characterisation and specificity for pseudopolyp ( n = 50 ) characterisation according to lesion size for each of the three readers . 
numbers of lesions used to calculate percentages are in brackets lesion size ( mm ) reader 1 reader 2 reader 3 69 10 69 10 tabella 1 sensibilit per la caratterizzazione dei polipi ( n = 50 ) e specificit per la caratterizzazione delle formazioni pseudopolipoidi ( n = 50 ) , riportate per dimensioni , rispettivamente dai tre lettori . 
at retrospective analysis of the corresponding 2d images , these polyps showed tiny areas of markedly increased attenuation that were interpreted as small particles of orally administered contrast material adherent to the polyp surface . 
i tre lettori hanno riportato complessivamente cinque interpretazioni false negative : un polipo sessile di 6 mm di diametro localizzato al colon trasverso , erroneamente interpretato da tutti i lettori , un polipo peduncolato di 5 mm di diametro localizzato nel retto , erroneamente interpretato dal secondo lettore , ed un polipo piatto localizzato nel colon - sigma erroneamente interpretato dal terzo lettore . 
b on corresponding 3d image with tr , this lesion demonstrates the typical colour pattern of a polyp characterised by multiple concentric rings of progressively increased tissue density from the lesion periphery towards the centre ( from blue to red , respectively )  . 
b nella corrispondente immagine 3d con il tr sovrapposto , questa lesione appare con il tipico pattern di colori di un polipo al tr , caratterizzato da multipli anelli concentrici di diversi colori , che rispecchiano il progressivo aumento di densita dalla periferia della lesione verso il suo centro ( raffigurati rispettivamente dal blu al rosso )  . 
b on the corresponding 3d image with tr , this lesion demonstrates areas of markedly increased attenuation ( assigned a white colour at tr display ) indicative of retained , high - density contrast material , subsequently confirmed . 
b nella corrispondente immagine 3d con il tr sovrapposto , questa lesione mostra aree con elevati valori di attenuazione ( assegnati al colore bianco ad una visualizzazione con il tr ) , indicative di ritenzione di particelle di mezzo di contrasto ad elevata densit . 
 with the exception of only two patients for whom the average labelling score was moderate ( between 25% and 50% ) , faecal tagging was judged excellent in all cases , with an average labelling score > 75% . 
 che corrispondevano a particelle di contrasto iodato adese alla superficie del polipo . i tre lettori hanno riportato complessivamente tredici interpretazioni false positive , che hanno incluso : due valvole ileo - cecali ( di 15 mm e 19 mm di diametro ) , erroneamente interpretate da tutti i lettori , due residui fecali ( di 6 mm e 9 mm di diametro ) , erroneamente interpretate dal primo e terzo radiol med ( 2010 ) 115 : 758770 fig . 
5a , b ct colonography of a 65 - year - old man with a 7 - mm polyp of the cecua the 3d endoluminal image shows a 7 - mm polypoid lesion ( arrow ) adjacent to a prominent ileocaecal valve ( arrowheads )  . 
b nella corrispondente immagine 3d con il tr sovrapposto questa lesione mostra il tipico pattern di colori del polipo al tr , i.e. , anelli concentrici di crescente densitatissutale dalla periferia verso il centro della lesione . 
notare la predominante presenza di aree a densita adiposa ( assegnata al colore verde nella visualizzazione con il tr ) nella valvola ileocecale suggestive di zone di lipoiperplasia allinterno della valvola ileocecale . 
b on the corresponding 3d image with tr , this lesion demonstrates uniform , soft - tissue attenuation ( assigned a red colour at tr display ) that was considered indicative of a polyp by two readers . 
b nella corrispondente immagine 3d con il tr sovrapposto , questa lesione mostra unarea con uniformi valori di attenuazione tissutale ( assegnata ad un colore rosso nella visualizzazione con il tr ) , considerata indicativa per la diagnosi di polipo per due lettori . 
 discussion our results demonstrate that tr is an excellent tool for characterising colonic lesions using a primary 3d reading at ct colonography , with mean sensitivity for polyp characterisation and mean specificity for pseudopolyp characterisation ranging from 96% to 98% and 90% to 92% , respectively , for our three readers . 
laccuratezza diagnostica ( auc ) del tr per la caratterizzazione delle formazioni coliche endoluminali stata di 0 , 97 ( 0 , 900 , 99 ) , 0 , 97 ( 0 , 910 , 99 ) e 0 , 98 ( 0 , 920 , 99 ) per il primo , secondo e terzo lettore rispettivamente , con una buona concordanza tra i tre lettori ( tabella 2 )  . con la sola eccezione di 2 pazienti , per i quali il punteggio medio complessivo della marcatura risultato moderato ( tra 25 e 50% ) , la marcatura delle feci stata giudicata ottima in tutti i restanti casi , con un punteggio di marcatura medio maggiore del 75% . 768 radiol med ( 2010 ) 115 : 758770 table 2 agreement among readers for endoluminal polypoid lesion characterisation using tr discussione reader 1vs . 
contrast adherence to the polyp surface has been demonstrated to occur in approximately 15% of cases and is more likely associated with a villous histology of the polyp and faecal tagging protocols using barium solutions [ 20 ]  . 
 we also found a low number ( n = 3 ) of false - positive interpretations due to polypoid - like faecal residues that showed an attenuation profile comparable with that of a true polyp at tr display . 
we postulate that these diagnostic errors could be partly a result of the failure of tr to either characterise suboptimally tagged faecal residues or demonstrate small air bubbles within these lesions . 
 in our study , six ( 46% ) of the 13 false - positive interpretations were caused by two of ten icvs that were mistakenly considered polyps by the three readers based on the absence of visible internal areas of fat attenuation at tr display . 
although the ct attenuation profile has been shown to represent the single , most important determinant for characterising icvs , other imaging features such as volume , morphology and location of a colonic lesion can provide useful information for correct identification of this anatomical structure [ 16 ]  . 
therefore , we believe that as an adjunct to a lesions ct attenuation profile , this additional imaging information can further improve reader confidence for characterising icvs using a primary 3d endoluminal analysis . 
this is of practical importance , because icv is i nostri risultati dimostrano che il tr un ottimo strumento 3d per la caratterizzazione delle lesioni coliche nella colografia tc con analisi 3d primaria , evidenziando una sensibilit media per la caratterizzazione dei polipi e specificit media per la caratterizzazione delle formazioni pseudopolipoidi che oscillava rispettivamente tra il 96% ed il 98% e tra il 90% ed il 92% . 
nel nostro studio , solo 3 polipi ( due di 5 mm ed uno di 6 mm di diametro massimo ) sono stati erroneamente interpretati come pseudopolipi ( falsi negativi ) sullevidenza di piccole aree di elevata densit riscontrate nelle immagini 3d con il tr sovrapposto . 
 stato dimostrato che la superficie dei polipi pu essere ricoperta dal mezzo di contrasto in un 15% dei casi , evento pi frequentemente associato con unistologia villosa del polipo ed allutilizzo di un mezzo di contrasto baritato [ 20 ]  . lo studio ha inoltre rilevato un basso numero di interpretazioni false positive dovute a residui fecali con morfologia polipoide che mostravano un profilo di valori di attenuazione ed un pattern di colori , nelle immagini 3d con il tr sovrapposto , comparabile a quello dei polipi . 
probabile che questa similitudine di comportamento allanalisi con il tr stata causata dallalta efficienza del protocollo per la marcatura delle feci ( punteggio superiore al 75% ) riportata in questo studio . 
tuttavia nostra ipotesi che questi errori di interpretazione possano essere , almeno in parte , riferiti al non corretto funzionamento dello strumento o dovute alla presenza di piccole bolle di aria allinterno delle formazioni endoluminali . 
peraltro importante sottolineare che nel nostro studio tutte le interpretazioni false positive sono rimaste indeterminate anche ad allanalisi retrospettiva in 2d . nel nostro studio , 6 ( 46% ) delle 13 interpretazioni false positive sono state causate da due delle 10 valvole ileocecali che sono state erroneamente caratterizzate come polipi dai tre lettori , in maniera indipendente , sulla base dellassenza di aree di densit relativa al tessuto adiposo nelle immagini 3d con il tr . 
i nostri dati concordano con i risultati riportati dalla letteratura recente che indicano lassenza di lipoiperplasia in approssimativamente il 20% delle valvole ileo - cecali [ 14 , 21 ]  . 
sebbene sia stato dimostrato che il profilo dei valori di attenuazione in tc rappresenti il pi importante discriminante per la caratterizzazione delle valvole ileo - cecali con aspetto polipoide , altri parametri allimaging come il volume , la morfologia e la localizzazione delle lesioni coliche possono fornire importanti informazioni per la corretta identificazione di questa struttura anatomica [ 16 ]  . 
 nostra convinzione che , se si utilizza una visualizzazione primaria 3d , queste ulteriori informazioni in aggiunta al profilo di attenuazione tc della lesione possano accrescere la confidenza del radiologo nella caratterizzazione delle valvole ileo - cecali . 
ci di particolare importanza , dal momento che la valvola ileocecale rappresenta una causa comune di interpretazioni false positive alla colografia con tc [ 16 , 21 , 22 ]  . radiol med ( 2010 ) 115 : 758770 known to represent a cause of false - positive interpretations at ct colonography [ 16 , 21 , 22 ]  . 
second , our analysis did not include some well - recognised pitfalls at 3d endoluminal image analysis [ 2224 ] , such as impacted diverticula , submucosal lipoma or intraluminal mass effect from extrinsic extracolonic lesions . 
additionally , based on our personal experience and preliminary evidence from previous investigations , most of these pseudopolyps can be confidently diagnosed using tr because of their very characteristic attenuation pattern [ 8 ]  . 
third , due to our study design , where lesions were positively marked prior to image analysis , we could not evaluate the possible benefit of tr for decreasing readers interpretation time using a primary 3d analysis [ 25 , 26 ]  . 
although our approach is the result of daily clinical experience with > 500 cases per year at our tertiary referral hospital and has been validated in recent clinical studies [ 9 , 17 ] , we believe that further investigations are warranted to assess the effects of different faecal tagging protocols on tr diagnostic accuracy . 
 in summary , tr represents an accurate tool for lesion characterisation using a primary 3d endoluminal analysis . by limiting the need of a supplemental 2d analysis , tr has the potential to decrease 3d reading interpretation time , thus possibly leading to increased clinical acceptance of a primary 3d approach for ct colonography . 
in secondo luogo , linterpretazione delle immagini 3d non teneva presenti alcuni pittfalls ben noti [ 2224 ] , come diverticoli impattati da materiale fecale , lipomi sottomucosi o immagini di masse intraluminali per effetto di una lesione estrinseca extracolica . 
riteniamo che questi reperti , sebbene siano ampiamente descritti nella letteratura , raramente causano interpretazioni false positive allanalisi 3d endoluminale . inoltre , sulla base della nostra esperienza clinica e dallevidenza di studi precedenti , molte di queste formazioni pseudopolipoidi sarebbero facilmente diagnosticabili ad unanalisi con il tr , poich sovrapponendo lo strumento 3d , esse presentano un pattern di attenuazione molto caratteristico [ 8 ]  . 
terzo , poich il metodo adottato consisteva nel valutare solo le immagini 3d statiche indicate da una freccia , non stato possibile investigare il possibile vantaggio del tr nel ridurre i tempi di interpretazione nellanalisi 3d primaria [ 25 , 26 ]  . 
sebbene il protocollo di fecal tagging adottato nello studio rappresenti il risultato di unesperienza clinica quotidiana con pi di 500 casi allanno eseguiti nel nostro ospedale , oltre che validato in studi clinici recenti [ 9 , 17 ] , sosteniamo che siano opportune ulteriori indagini al fine di verificare gli effetti dei diversi protocolli del fecal tagging sullaccuratezza diagnostica del tr . in conclusione , il tr rappresenta uno strumento accurato per la caratterizzazione delle lesioni endoluminali se utilizzata una visualizzazione 3d primaria . 
the occupational health physician plays a key role in identifying and managing the impaired radiologist . keywords impairment blood - borne pathogens fitness to practise alcohol , drugs riassunto il concetto di medico malato un ossimoro . 
il medico , per scelta , portatore di salute , e ci pu indurre a trascurare la possibilit che egli possa , a sua volta , contrarre una malattia che ne riduca la capacit diagnostica e terapeutica , con conseguente pericolo per la salute dei pazienti . 
i motivi clinici per i quali un radiologo pu risultare pericoloso per i pazienti appartengono a due categorie : le malattie infettive a trasmissione ematogena , che possono essere trasmesse al paziente nel corso di attivit di radiologia interventistica , e le malattie neurodegenerative e psichiatriche , comprese le dipendenze da alcol e droghe , che alterano transitoriamente o definitivamente la capacit di giudizio . 
a questa responsabilit individuale verso i propri pazienti si aggiungono gli obblighi di salute e sicurezza che le norme europee prevedono per i radiologi che siano datori di lavoro , dirigenti o preposti . 
il medico del lavoro ha un ruolo chiave nellidentificazione e nella gestione dei radiologi con compromissione della capacit di giudizio . parole chiave compromissione della capacit di giudizio infezioni ematogene idoneit al lavoro alcol , droghe introduction introduzione physicians are by definition bearers of health . 
this definition could lead to possibility that they may become ill being overlooked and that as a consequence of this illness , their il medico , per missione , un portatore di salute . 
ci potrebbe indurre a trascurare leventualit che egli possa contrarre una malattia , e che in conseguenza di questa radiol med ( 2010 ) 115 : 826838 patients health may suffer . 
in some cases , this illness can lead to temporary or permanent reduction in his or her ability to function professionally , which can translate into a health risk for his or her patients . 
this possibility is a threat to public health and even more so to the image of medical professionals . although medicine has a very long history , illness of the physician that interferes with his or her diagnostic / therapeutic skills is an issue that has only recently been acknowledged and which is extremely controversial . 
there clearly is an ethical dilemma arising from a conflict of legitimate interests : the patient has the right to choose autonomously and with fully informed consent the physician who offers the best guarantee of providing the correct standard of care ; the ill physician has the legitimate interest of continuing his or her career or maintaining a role in the occupational organisation without being discriminated against and with the due level of privacy in terms of personal data . 
society as a whole also has a legitimate interest in maintaining efficient health - care services at limited costs and to not bear the burden that is the inevitable outcome of failing to resolve the conflict . in english - speaking countries , where the legal system ( common law ) is founded on unwritten laws and develops through the precedence of judicial sentences , the courts have tackled this issue and traced outlines for the development of a policy that takes into consideration the rights of the individual and the collective . 
in contrast , in latin countries , the legal systems of which are based on written laws ( civil law ) , the absence of specific intervention by the legislator has left the field open to behaviour that not always respects ethical principles . 
ma naturalmente anche il medico , come ogni essere umano , pu ammalarsi . in alcuni casi , questa malattia pu determinare una riduzione temporanea o permanente della capacit di svolgere la propria funzione e tradursi in un rischio per la salute del paziente . 
palese difatti il dilemma etico che si origina dal conflitto di interessi legittimi : il paziente ha il diritto di scegliere , in autonomia e tramite un consenso pienamente informato , il medico che dia le migliori garanzie di sottoporlo al corretto standard di cure ; il medico malato , dal canto suo , ha il legittimo interesse di proseguire la propria carriera o mantenere il ruolo nellorganizzazione lavorativa , senza essere discriminato e con la dovuta riservatezza dei propri dati personali . 
anche la societ nel suo insieme ha un legittimo interesse al mantenimento di servizi sanitari efficienti e a costi contenuti , e a non sopportare gli oneri che inevitabilmente deriverebbero dalla mancata risoluzione del conflitto . 
 nei paesi anglosassoni , il cui ordinamento giuridico ( common law ) fondato su leggi non scritte e si sviluppa attraverso i precedenti delle decisioni giurisprudenziali , le corti hanno affrontato questa tematica , tracciando le linee attraverso le quali si deve realizzare una policy che tenga conto dei diritti dei singoli e delle comunit . 
viceversa nei paesi latini , nei quali il diritto dipende dallesistenza di leggi scritte ( civil law ) , la mancanza di un intervento specifico del legislatore ha lasciato campo aperto a comportamenti che non risultano sempre rispettosi dei principi etici . lesigenza di trovare e condividere le modalit operative attraverso le quali sia possibile garantire il mantenimento della salute dei pazienti e degli operatori sanitari malati , senza pregiudizio per i diritti civili di questi ultimi , ha motivato la costituzione del gruppo di studio la.r.a. 
the emotional shockwave this episode produced led to close attention being paid to the possibility that health - care professionals can infect their patients with blood - borne infections , and in particular , hepatitis b ( hbv ) and c ( hcv ) and acquired immunodeficiency . the interventional radiologist presents a risk profile that with regard to blood - borne infections puts him or her on a par with surgical specialties . 
a case of hepatitis c transmission from a radiologist to a patient was reported by smith and berlin [ 3 ] , who provided a detailed analysis of the medicolegal consequences of the incident . 
under the ethical profile , it was felt that the principle of nonmaleficence ( primum non nocere ) had been violated and there was failure to provide the patient with full information , a necessary condition for the validity of consent . 
the litigation proceedings that took place in the united states involved not only the radiologist but the entire medical team and hospital , in line with the principle of collective responsibility that has only recently been adopted in the italian legal syste the proceedings were concluded with an out - ofcourt settlement involving the payment of us $500 , 000 in compensation for both the biological damage suffered by the patient ( the infection ) and the psychological consequences of the event and material damages relating to the social and reproductive life changes resulting from the disease . the probability that an infected patient transmits a bloodborne infection to radiological or nuclear medicine personnel is well known and quantified [ 46 ]  . 
high - risk surgical procedures are those in which the surgeon operates within a body cavity and has no visible control over his or her hands , which can come into contact with sharp surgical tools , needles or bone parts present in the operating field without the surgeon being aware of it , thus infecting the patient . 
activities performed by the radiologist do not generally come under this category , even though numerous activities such as ultrasound - guided biopsies , central venous catheter placement , embolisations , etc . 
involve the risk of puncture or cuts . in recent years , the generalised adoption of standard preventive measures has helped reduce not only the risk of transmission from patient to physician but also that from physician to patient . 
the rate of hiv infection after a puncture with a contaminated needle is estimated to be in the order of malaugurato caso di un dentista canadese portatore di virus dellimmunodeficienza umana ( hiv ) che , con modalit ancora non accertate ( e che non escludono la volontariet ) , ha infettato alcuni suoi pazienti [ 2 ]  . 
londata emotiva che scaturita da questo episodio ha portato a considerare con particolare attenzione la possibilit che loperatore sanitario possa trasmettere al paziente le infezioni ematogene , e in particolare lepatite b , lepatite c e limmunodeficienza acquisita . il radiologo interventista presenta un profilo di rischio che , per quanto riguarda le infezioni ematogene , lo assimila alle specialit chirurgiche . 
un caso di trasmissione di virus dellepatite c da un radiologo ad un paziente riportato da smith e berlin [ 3 ] , che analizzano in modo approfondito le conseguenze medico - legali dellincidente . il fatto che il radiologo sapesse di essere portatore di una malattia infettiva , e che avesse accidentalmente trasmesso questa malattia ad un paziente nel corso di un esame diagnostico , stato ritenuto un comportamento negligente . sotto il profilo etico , si ritenuto violato il principio di non maleficenza ( primum non nocere ) e non ottemperata la piena informazione del paziente , necessaria per la validit del consenso . 
nel processo statunitense stato coinvolto , oltre al radiologo , lintera equipe medica e lospedale , in virt del principio anglosassone di responsabilit collettiva che stato recentemente adottato anche dal nostro ordinamento . 
la contesa si conclusa con un accordo extragiudiziale , che ha comportato il pagamento di un risarcimento di 500000 dollari , riferito sia al danno biologico subito dal paziente ( linfezione ) , sia alle conseguenze psicologiche dellevento ed ai danni materiali relativi ai cambiamenti della vita sociale e riproduttiva conseguenti alla malattia . la probabilit che un paziente infettivo trasmetta linfezione ematogena al personale di radiologia o medicina nucleare ben nota e quantificata [ 46 ]  . 
le procedure chirurgiche ad alto rischio sono quelle nelle quali il chirurgo , operando allinterno di cavit corporee , non ha il controllo visivo delle mani e queste possono entrare in contatto con strumenti chirurgici taglienti , aghi o parti ossee presenti nel campo operatorio , senza che loperatore se ne avveda , contaminando cos il paziente . 
le attivit svolte dal radiologo non rientrano generalmente in questa categoria , anche se evidente che numerose attivit invasive , come biopsie ecoguidate , posizionamento di cateteri venosi centrali , embolizzazioni , ecc . , comportino la possibilit di punture o tagli . negli ultimi anni , ladozione generalizzata delle misure standard di prevenzione ha contribuito a ridurre non solo il rischio di trasmissione da paziente a medico , ma anche quello da medico a paziente . 
this rate increases to 0.41.8% in the case of an individual infected with hcv and much higher ( between 3% and 30% ) in the case of hbv [ 8 ]  . in 1991 , the centers for disease control and prevention ( cdc ) in atlanta , ga , usa published the first guidelines regarding health - care professionals infected with hiv and hbv [ 9 ]  . 
in summary , the cdc guidelines state that : infected health - care professionals who use standardised protective devices and who do not perform high - risk procedures pose no risk for the transmission of bloodborne infections ; infected health - care professionals who perform high - risk procedures pose a low risk of transmission of bloodborne infections ; compulsory testing is not envisaged for health - care professionals , but the physician who is aware of being infected has the obligation to submit himself / herself to a committee that will evaluate whether he or she should perform high - risk procedures ; even after having received authorisation , the infected physician is obliged to inform patients of his or her condition . as one would expect , the american guidelines provoked significant reactions . 
the experience during these years shows that the guidelines have been poorly applied , partly due resistance by professional specialities that have failed to cooperate with the cdc in defining high - risk procedures that are particularly exposed to accidents . 
in addition , disclosure by the physician to the patient of his or her seropositive status has been considered an inadmissible violation of personal privacy that is not in proportion to the degree of risk for public health [ 12 ]  . while taking into consideration the broad lines drawn up by the cdc , european countries [ 10 ] have focused more on establishing preventive measures in the workplace and on verification ( preventive and after accidents ) of the serological status of health - care professionals . 
the indication appears to be to avoid removing the worker if the measured viral load is below the infection threshold , the level at which transmission of the disease either does not occur or is highly improbable . 
it should be noted that the difficulties of reliably measuring viral load over time and uncertainties in defining a threshold have led to failure to apply these indications , which at any rate have an indicative and not a binding characteristic . letteratura [ 7 ] , ha confermato che i casi di trasmissione da operatore sanitario a paziente sono estremamente rari . 
tale tasso sale allo 0 , 4%1 , 8% nel caso di un soggetto affetto da epatite c , ed molto pi alta ( tra il 3% ed il 30% ) nel caso di un portatore di virus dellepatite b [ 8 ]  . nel 1991 i centers for disease control and prevention ( cdc ) di atlanta hanno pubblicato le prime linee guida relative agli operatori sanitari infetti da hiv e virus dellepatite b ( hbv ) [ 9 ]  . 
in anni pi recenti la maggior parte degli organismi scientifici europei ha elaborato linee guida nazionali , e nel 2003 si giunti alla definizione di un documento di consenso europeo [ 10 ]  . in sintesi , le linee guida dei cdc stabiliscono che : gli operatori infetti che utilizzano dispositivi di protezione standardizzati e che non effettuano procedure ad alto rischio non pongono alcun rischio per la trasmissione di infezioni ematogene ; gli operatori infetti che eseguono procedure ad alto rischio pongono un basso rischio di trasmissione di infezioni ematogene ; non sono previsti test obbligatori per i medici , ma il medico che sa di essere infettivo ha il dovere di rivolgersi ad un comitato , che valuter se il caso che egli effettui operazioni ad alto rischio . 
anche dopo aver ottenuto lautorizzazione , il medico infettivo ha il dovere di informare i pazienti sul proprio stato . le linee guida statunitensi hanno provocato , come facile immaginare , notevoli reazioni . 
lesperienza di questi anni insegna che esse sono scarsamente applicate , anche per la resistenza degli ordini professionali che non hanno collaborato con i cdc alla definizione di quali siano le operazioni ad alto rischio che espongono particolarmente ad infortuni . 
la rivelazione dello stato di sieropositivit del medico ai pazienti , inoltre , stata considerata una inammissibile violazione della riservatezza dei dati personali , non commisurata allentit del pericolo per la salute pubblica [ 12 ]  . i paesi europei [ 10 ] , pur tenendo conto della impostazione dei cdc , hanno puntato con pi decisione alla realizzazione di misure preventive negli ambienti di lavoro e allaccertamento ( preventivo e dopo incidenti ) dello stato sierologico dei lavoratori . 
lindicazione che emerge quella di evitare lallontanamento del lavoratore nei casi in cui sia rilevabile una carica virale inferiore alla soglia di 830 radiol med ( 2010 ) 115 : 826838 the question of just who should evaluate the fitness of infected physicians to practise is yet to be fully defined , both in the united states and europe . 
this is not always a suitable choice due to the possibility of a conflict of interest among components of the committee and the physicians under examination [ 13 ] and to the limited competence of the presumed experts [ 12 ]  . 
regardless , the choice is made in the exclusive interests of patients and health - care facilities , thus failing to safeguard the privacy of ill health - care professionals and their civil rights . 
for this reason , this procedures abolition has been proposed [ 14 ]  . in europe , too little light has been shed on who should take on the responsibility of the decision , with the solution perhaps being left up to an automatism with the definition of the infection threshold . 
it therefore seems that the decision can be taken by the head of a public hospital trust , or the general manager , or the medical director , or the head of a department . 
it is surprising that no thought has been given to involving the individual who in all european countries is institutionally required to express a judgement on fitness to practise : the occupational health physician in charge of workplace health surveillance . the radiologist with compromised clinical skills whereas the problems of blood - borne diseases opens up such delicate and complex scenarios , despite the truly limited number of patients that could be involved , consider how much greater the danger can be of radiologists who have lost their faculty of judgement due to a neurodegenerative or psychiatric disorder or to substance abuse . 
it has been estimated that in the time span of a professionals life , some 8%15% of physicians may find themselves in a position where they pose a risk to their patients [ 1517 ]  . 
unfortunately , this problem has been given less attention in mediterranean countries than would be desirable , and a framework for evaluating and preventing consequences of the phenomenon is sorely lacking [ 18 ]  . the experience of english - speaking countries instead shows that preventive action is both possible and advantageous . 
the obligation to answer for ones past and future actions and decisions , to justify them and be sanctioned in the event of incorrect behaviour significantly influences the management of health - care facilities and health governance . 
as a result , all things that can interfere with provision of a standard level of care must be analysed and made available to the public . infettivit , in corrispondenza della quale la trasmissione della malattia non avviene o improbabile . 
si pu osservare che le difficolt di misurare in modo affidabile nel tempo la carica virale , e le incertezze nella definizione di una soglia , hanno di fatto disatteso lapplicazione di tali indicazioni , che hanno comunque sempre un carattere indicativo e non cogente . non compiutamente definita , negli stati uniti come in europa , la questione di chi debba occuparsi di valutare lidoneit dei medici infettivi . 
questa scelta non risultata sempre felice , per la possibile insorgenza di conflitti di interesse tra componenti dei comitati e medici da esaminare [ 13 ] e anche per la scarsa competenza dei presunti esperti [ 12 ]  . 
in ogni caso , si tratta di una scelta operata nellesclusivo interesse dei pazienti e delle case di cura , che non tutela la riservatezza degli operatori sanitari malati , n i loro diritti civili . 
per questo motivo ne chiesta labolizione [ 14 ]  . anche in europa non si pensato a chiarire chi debba assumersi la responsabilit della decisione , puntando forse a determinare un automatismo mediante la definizione della soglia infettante . 
sorprendente che non si sia pensato di coinvolgere come naturale destinatario delle linee - guida la figura che istituzionalmente , in tutti i paesi europei , deve esprimere il giudizio di idoneit al lavoro : il medico competente incaricato della sorveglianza sanitaria . il radiologo con compromissione delle capacit cliniche se la problematica delle malattie trasmissibili per via ematogena apre scenari cos delicati e complessi , nonostante il numero davvero esiguo di pazienti che potrebbe essere coinvolto , bisogna considerare quanto maggiore possa essere il pericolo connesso con i radiologi che abbiano perduto la propria capacit di giudizio per effetto di una malattia neurodegenerativa o psichiatrica , o di un abuso di farmaci . 
 stato stimato che nellarco della vita professionale una percentuale compresa tra l8% ed il 15% dei medici possa trovarsi in una condizione suscettibile di recare danno ai pazienti [ 1517 ]  . 
sfortunatamente questo problema ha finora incontrato nei paesi mediterranei attenzione minore di quella che sarebbe stata desiderabile , e manca una struttura finalizzata a valutare e prevenire le conseguenze del fenomeno [ 18 ]  . in 1973 , the american medical association defined policies to be adopted with regard to the impaired physician i.e. 
il principio di accountability , cio lobbligo di rendere conto delle radiol med ( 2010 ) 115 : 826838 reasonable skill and safety to patients because of mental or physical illness , including cognitive deterioration related to age , loss of motor skills or abuse of drugs and alcohol [ 19 ]  . substance abuse was initially treated under a disciplinary profile [ 20 ]  . 
moreover , it has been observed that many procedures adopted by boards for granting or withdrawing a license to practise medicine violate the rights of the individual with the disability [ 21 ]  . 
however , early recognition of the problem prompted american medical organisations to propose measures that minimise damage to the career and profession of the impaired physician , all the while guaranteeing patient health and functioning of health - care services . for more than 25 years in each american state , as in many english - speaking countries , programmes have been in place impaired physicians . 
these for programmes are partially funded by professional associations , and in many american states , there are laws in place that provide for the suspension of disciplinary actions ( including withdrawal of the licence to practise ) for all physicians who take part in rehabilitation programmes [ 22 , 23 ]  . rehabilitation of a similar process of verifying professional medical skill is in place in the british national health service . 
revalidation involves reconfirmation of the ability to practise medicine ( relicensure ) , which corresponds to verifying the conservation of the faculty of judgement and confirming the specialisation ( recertification ) based on professional competence in relation to the standards [ 24 ]  . 
in this delicate process , close attention is paid to evaluating cognitive skills [ 25 , 26 ] and recovery of these skills after treatment [ 27 ]  . the occupational health physician is seen as a key figure in appraising performance and identifying problem cases [ 28 , 29 ]  . pathological conditions that can cause temporary or permanent loss of a physicians professional skills are numerous and include a large number of neuropsychiatric disorders ( table 1 )  . 
this natural process is of particular relevance in italy , more so than in other european countries . due to a series of legal provisions , such as the establishment of the national health service that , by setting an optimal patient - list size , has limited the number of young physicians entering general practice , and the freeze on new posts in public hospitals that has been in place for approximately 15 years , the mean physician age in the public health system is high and rising . 
according to the italian federation of azioni e decisioni passate e future , di giustificarle e di essere sanzionati in caso di condotta scorretta , informa profondamente le modalit di gestione delle aziende e la governance sanitaria . 
 lamerican medical association sin dal 1973 ha definito le politiche da adottare nei confronti del medico impaired , che cio sia incapace di praticare la medicina con ragionevole abilit e sicurezza per i pazienti a causa di una malattia mentale o fisica , inclusi il deterioramento cognitivo correlato allet , la perdita di abilit motoria o labuso di droghe e alcol [ 19 ]  . 
labuso di alcol e droghe stato inizialmente trattato sotto il profilo disciplinare [ 20 ]  . stato osservato , peraltro , che molte delle procedure adottate dai boards per la concessione o il ritiro della licenza di esercizio della professione medica violano i diritti dei soggetti con disabilit [ 21 ]  . 
ma laver preso coscienza tempestivamente del problema ha spinto le organizzazioni mediche statunitensi ad adoperarsi per proporre misure che limitino per quanto possibile i danni per la carriera e la professione del medico incapacitato , pur garantendo la salute dei pazienti e la funzionalit dei servizi sanitari . 
da oltre 25 anni in ciascuno degli stati americani , cos come in molti paesi di lingua inglese , sono operativi programmi di recupero per i medici con compromissione , finanziati parzialmente dalle associazioni professionali , e in molti stati americani sono vigenti leggi che consentono la sospensione delle azioni disciplinari ( comprendenti la revoca della licenza professionale ) per tutti i medici che si affidano ai programmi di recupero [ 22 , 23 ]  . un analogo processo di verifica della capacit professionale medica in atto nel sistema sanitario nazionale inglese . 
la verifica ( revalidation ) consta di una riconferma della capacit di praticare la medicina ( relicensure ) , che corrisponde ad una verifica della conservazione della capacit di giudizio , ed in una conferma della specializzazione ( recertification ) , basata sulla competenza professionale in relazione con gli standard [ 24 ]  . 
una particolare attenzione , in questo delicato processo , viene riservata alla valutazione della capacit cognitive [ 25 , 26 ] e al recupero di tali capacit dopo il trattamento [ 27 ]  . 
il medico del lavoro ritenuto una figura chiave nella valutazione della performance e nellidentificazione dei casi con problemi [ 28 , 29 ]  . le condizioni morbose che possono determinare una perdita transitoria o definitiva della capacit professionale di un medico sono piuttosto numerose e comprendono , oltre ai comportamenti addittivi , numerose malattie neuropsichiatriche ( tabella 1 )  . 
daltra parte , occorre considerare che anche numerose altre malattie che non alterano le funzioni superiori possono 832 radiol med ( 2010 ) 115 : 826838 table 1 main pathological conditions that can compromise a physicians judgement alcoholism and substance dependence psychiatric disorders psychosexual disorders neurological diseases with cognitive impairment neurovascular diseases , dementia behavioural disturbances tabella 1 principali condizioni morbose che possono determinare una condizione di compromissione della capacit di giudizio di un medico dipendenza da alcol , farmaci o droghe malattie psichiatriche malattie psicosessuali malattie neurologiche con compromissione cognitiva malattie neurovascolari , demenze disturbi comportamentali general practitioners , the 47 , 000 general practitioners in the ministry of health database had a mean age of 48 years in 1998 , but by 2000 , it was already > 49 years . 
ageing of the medical profession is a concern for public health , as elderly physicians are more prone to suffer from the so - called four ds dementia , drugs , drink , and depression [ 32 ]  . it should be borne in mind that cognitive deterioration is to a certain extent related to organisational and psychosocial factors . 
a recent study indicated that italian radiologists suffer significant distress arising from the organisation of their work , and many of them are immersed in a highly tense working environment . 
the most pressured are the younger physicians with less work experience and lower hierarchical positions , women and those working in public facilities as opposed to their counterparts in the private sector [ 33 ]  . 
per effetto di una serie di provvedimenti di legge , quali listituzione del servizio sanitario nazionale , che tramite il rapporto ottimale tra medici e assistiti ha limitato la possibilit di convenzionamento dei giovani medici , e il blocco delle assunzioni nellospedalit pubblica , in vigore ormai da circa 15 anni , let media dei medici che svolgono un servizio pubblico elevata ed in sensibile aumento . 
secondo la federazione italiana medici di medicina generale ( fimmg ) i 47000 medici di famiglia che risultano dai database del ministero della salute avevano nel 1998 una et media di 48 anni , ma nel 2000 essa sfiorava gi i 49 anni . analoga situazione si rileva nelle aziende ospedaliere [ 30 ]  . nel 2009 il 56% dei medici iscritti allalbo ha pi di 50 anni e tra questi oltre l11 , 5% ha pi di 65 anni [ 31 ]  . 
linvecchiamento della classe medica preoccupante per la salute pubblica , perch i medici pi anziani sono proni a soffrire delle cosiddette quattro d : demenza , droghe , drink e depressione [ 32 ]  . importante tenere presente che il deterioramento cognitivo in qualche misura correlato a fattori organizzativi e psicosociali . 
i pi pressati risultano i soggetti pi giovani , con minore anzianit lavorativa e con ruoli gerarchici inferiori , le donne , e coloro che operano nelle strutture pubbliche rispetto a coloro che operano nel privato [ 33 ]  . 
poich tra stress lavorativo e comportamenti di abuso o disturbi psichiatrici esiste una relazione complessa , emerge la necessit di valutare , caso per caso , le condizioni nelle quali maturato il disagio . tale indagine particolarmente utile e delicata nel caso dei cosiddetti disruptive behaviours , che possono essere sia la causa che leffetto di un clima lavorativo difficile . 
il comportamento distruttivo , un insieme che comprende luso di linguaggio scurrile , specie verso il personale parasanitario e gli specializzandi , luso di alcol e di farmaci sul posto di lavoro , il comportamento discriminante verso alcuni colleghi , gli atti di molestia sessuale , le maldicenze verso i colleghi , le condotte non professionali verso i pazienti , la litigiosit e un generale atteggiamento passivoaggressivo in relazione ai propri doveri , pu essere difatti collegato alle stesse cause dellimpairment . nella ricerca dei fattori causali in un ambiente di lavoro , non bisogna tralasciare neppure gli agenti chimici . 
stato dimostrato che la dipendenza da farmaci negli anestesisti radiol med ( 2010 ) 115 : 826838 towards ones duties can in fact be linked to the same causes of the impairment . the search for causative factors in the workplace should not overlook chemical abuse . 
it has been shown that drug dependency in anaesthetists ( a category with a higher rate of dependence than other specialties ) can be secondary to chemical contamination in operating environments caused by anaesthesia - inducing aerosols such as propofol or analgesics such as fentanyl , which can induce dependence [ 34 , 35 ]  . 
as the source of exposure is expiration by the anaesthetised patient , radiologists working in contaminated environments would clearly be exposed to the same risk . experience in the united states and other countries ( united kingdom , australia , new zealand , canada ) that have had specific prevention programmes in place for some time show that most cases of alcohol or drug dependence positively respond to treatment and achieve high rates of return to professional activity . 
data concerning treatment of psychiatric or neurodegenerative conditions , however , appear to be less effective , although fortunately the number of cases is limited . the issue of the radiologist with a disease that alters his or her judgement is still more complex from an ethical point of view than the radiologist with an infectious disease . whereas in this case the physician has the moral duty to assess his or her own state of health , undergo health checks and impose self - limitations to activity when his or her state of health could pose a threat to patients , it should be borne in mind that the very impairment of the physicians judgement can hinder self - diagnosis of the problein the more severe cases of psychosis or cognitive degeneration , but even in the course of some addictions , the individual may not be aware of his or her own inability to provide services compatible with the professional standard . 
regardless , there is the tendency to underestimate and deny ones own health problems , in part due to the social and economic repercussions that could ensue . at this point , a crucial factor is intervention by colleagues , who are the first to recognise a deviation from professional standards . 
in english - speaking countries , the responsibility of supervising the health and professional skill of each physician falls upon colleagues , who are called on to intervene in the event of behaviour not complying with good professional practice or when they suspect an untreated pathological condition or substance abuse [ 36 , 37 ]  . 
the first step should be to amicably approach the colleague to ask whether he or she has any problems and to advise him or her on the appropriate steps to take . 
in the united states , there is the risk of civil and disciplinary sanctions , which can include suspension and being struck off the register , in the case of a failure to ( categoria che presenta una maggiore frequenza di dipendenza rispetto alle altre specializzazioni ) pu essere secondaria alla contaminazione chimica degli ambienti operatori da parte di aerosol di induttori dellanestesia , come lisopropil - fenolo ( propofol ) , o di analgesici come il fentanyl , che possono indurre dipendenza [ 34 , 35 ]  . 
poich la sorgente di esposizione lespirazione da parte del paziente anestetizzato , anche i radiologi che si trovassero ad operare in ambienti contaminati sarebbero evidentemente esposti allo stesso rischio . lesperienza statunitense , o di altri paesi ( gran bretagna , australia , nuova zelanda , canada ) che hanno da tempo messo in opera programmi di prevenzione specifici , dimostra che le condizioni di dipendenza da alcol o droghe risentono positivamente del trattamento nella grande maggioranza dei casi e ottengono tassi elevati di ripresa delle attivit professionali . 
meno soddisfacenti sembrano sinora i dati relativi al trattamento delle condizioni psichiatriche o neurodegenerative , che riguardano fortunatamente una percentuale modesta di casi . il tema del radiologo con malattie che ne alterano la capacit di giudizio ancora pi complesso , sotto il profilo etico , di quello del radiologo infettivo . 
se anche in questo caso si deve considerare che il medico ha il dovere morale di auto - valutare il proprio stato di salute e quindi di sottoporsi a controlli del proprio stato sanitario e ad auto - limitare la propria attivit qualora questa possa risultare pericolosa per i pazienti , si deve tenere conto del fatto che proprio la compromissione della capacit di giudizio pu impedire di auto - diagnosticare il problema . 
nei casi pi gravi di psicosi o degenerazione cognitiva , ma anche nel corso di talune dipendenze , il soggetto potrebbe non essere cosciente della propria incapacit a fornire prestazioni compatibili con lo standard professionale . 
c in ogni caso la tendenza a sottovalutare e a negare il proprio problema di salute , anche per il timore delle possibili ripercussioni sociali ed economiche che esso potrebbe comportare . cruciale , a questo punto , lintervento dei colleghi , che sono i primi a rilevare la deviazione dagli standard professionali . 
nei paesi anglosassoni la responsabilit di vigilare sulla salute e sulla capacit professionale di ciascun medico attribuita ai colleghi , che sono chiamati a intervenire in ogni caso in cui evidenzino un comportamento non conforme alle buone pratiche professionali , o sospettino una condizione morbosa non trattata o un abuso di alcol o droghe [ 36 , 37 ]  . 
negli stati uniti possibile incorrere in sanzioni civili e disciplinari , che possono arrivare sino alla sospensione e alla radiazione dallalbo , qualora si sia 834 radiol med ( 2010 ) 115 : 826838 intervene after notification is given ( even anonymously ) of aberrant behaviour . omesso di intervenire dopo la segnalazione ( anche anonima ) di un comportamento anomalo . the radiologist is a bad patient il radiologo un cattivo paziente the problem of diseases that impact on diagnostic / therapeutic skills is aggravated by a condition that can be considered endemic in the medical profession : physicians are decidedly averse to undergoing medical treatment . 
recent studies show that physicians tend to deny having a disease and avoid seeking medical care in fear of the conflict that could ensue between their role as patient and their role as physician [ 38 ]  . 
in addition , as physicians often place medical practice at the centre of their lives , they are induced to mitigate the impact of a disease on their professional life and prefer to sacrifice their social and family life . 
in this way , when the impairment becomes evident , it is usually already in a well - advanced stage without the possibility of recovery [ 15 ]  . on the other hand , physicians are often reluctant to treat a colleague because they fear a conflict of roles . 
it therefore appears that on the whole , the medical profession is not equipped for optimal management of the impairment of one of its members and tends to adopt discriminatory behaviour rather than facilitating recovery [ 17 ]  . the pilot study mentioned above [ 33 ] , in which the lifestyles and level of physical health of italian radiologists and radiotherapists were investigated , showed that none of the interviewees has adopted the best possible lifestyle . 
this finding is surprising , considering that these professionals are subject to health surveillance in the workplace more often and for longer than other physicians , at least in terms of radiological risk . 
this therefore begs the question as to why such preventive measures have apparently failed to promote a healthy lifestyle . physicians who follow a healthy lifestyle are more inclined to advise their patients to adopt similar behaviour . the concept of the wounded healer , which dates back to the myths of chiron and asclepius and was used by jung to indicate the possibility that the analytical consultation awakens ancient wounds in the physician , thus causing countertransference [ 39 ] , can also apply to the physician with problems , who therefore needs special attention and prevention [ 40 ]  . il problema delle patologie che influenzano la capacit diagnostico / terapeutica aggravato da una condizione che si pu considerare endemica nella classe medica : quella di essere molto restii a sottoporsi a cure mediche . 
indagini recenti dimostrano che i medici tendono a negare le malattie ed evitano di chiedere assistenza medica , temendo il conflitto di ruolo che scaturisce dal contrasto tra il ruolo di paziente e quello di medico [ 38 ]  . 
molti medici di successo sono compulsivi e perfezionisti e rifiutano di essere controllati da altri ; per questo non possono cedere ad un altro medico il controllo delle proprie cure . 
inoltre i medici sono spesso portati ad attribuire un ruolo centrale nella propria vita alla pratica medica , e sono quindi indotti a mitigare limpatto della malattia sulla vita professionale , preferendo sacrificare la vita sociale e familiare . 
 daltro canto , bisogna tenere conto del fatto che spesso i medici sono riluttanti a prendere in cura un collega , perch temono di andare incontro ad un conflitto di ruolo . 
si pu dire quindi che la classe medica nel suo insieme non sembra orientata a gestire nel modo migliore linabilit di un suo membro e tende ad adottare comportamenti discriminatori piuttosto che a favorirne il recupero [ 17 ]  . nel gi citato studio - pilota [ 33 ] , nel quale sono stati indagati gli stili di vita e lo stato di salute fisica dei radiologi e radioterapisti italiani , risultato che nessuno degli intervistati adotta lo stile di vita migliore . 
tale risultato sorprendente , se si considera che tali categorie sono sottoposte a sorveglianza sanitaria sul luogo di lavoro con maggior frequenza e da maggior tempo rispetto agli altri medici , almeno per quanto attiene al rischio radiologico . 
il concetto del guaritore ferito ( wounded healer ) , che risale ai miti di chirone e di asclepio ed stato usato da jung per indicare la possibilit che il colloquio analitico risvegli nel medico antiche ferite , cos determinando un contro - transfer [ 39 ] , pu riguardare anche il medico con problemi , che abbisogna quindi di particolare attenzione e prevenzione [ 40 ]  . responsibility le responsabilit the responsibility towards patients and the moral le responsabilit verso il paziente , e gli imperativi morali radiol med ( 2010 ) 115 : 826838 imperatives of nonmaleficence and beneficence in their regard oblige the physician to maintain a state of health compatible with providing standard care . 
as a consequence , the physician who is aware of suffering from a problem that even temporarily places at risk his or her clinical judgement has the moral obligation over and above the legal obligation of turning to a qualified person for advice and support . these principles of responsibility take on even greater importance in the case of a radiologist who has his or her own practice and is therefore an employer , or a radiologist who is the head of a department and as such has the functions of health and safety delegated by his employer . 
in particular , they are obliged to evaluate workrelated risks , including work - related stress and behaviour indicative of substance abuse , and set up and implement the relative measures of control . 
81 / 08 attributes specific responsibility for health and safety in the workplace to all radiologists operating in a health - care facility who , regardless of their role within the organisation , perform managerial functions or at least have a position of authority . 
therefore , all radiologists operating within a facility could , under varying levels of responsibility , become involved in a compensation claim for damage caused by a colleague with impaired clinical judgement . last of all , it should be recalled that the public hospital trust , which in the past in italy was considered exempt of criminal liability in virtue of the principle of roman law , according to which societas delinquere non potest ( a legal entity cannot commit crimes ) , is fully obliged to implement prevention and control in accordance with the principle of the social liability of legal entities , which is clearly influenced by practice in english - speaking countries . di non maleficenza e di beneficenza nei suoi confronti , obbligano il medico a mantenere uno stato di salute compatibile con lerogazione di cure standard . 
conseguentemente il medico che avverta di soffrire di un problema che pu mettere a rischio , anche temporaneamente , la propria capacit di discernimento clinico , ha lobbligo morale prima che giuridico di rivolgersi ad una persona qualificata , per ottenere consiglio e sostegno . questi principi di responsabilit assumono maggiore rilevanza nel caso di radiologi che siano titolari di uno studio medico e quindi siano datori di lavoro o che , come direttori di una struttura , abbiano ricevuto delega delle funzioni di salute e sicurezza dal proprio datore di lavoro . 
in particolare , essi hanno lobbligo di valutare i rischi da lavoro e , tra questi , lo stress da lavoro e la presenza di comportamenti di abuso di alcol e di droghe , e di predisporre e attuare le relative misure di controllo . 
81 / 08 a tutti gli altri radiologi che operano in una struttura sanitaria in quanto , qualunque sia il loro ruolo nellorganizzazione , esplicano funzioni di dirigente o almeno di preposto . 
in definitiva , tutti i radiologi che operano in una struttura potrebbero essere coinvolti sotto diversi profili di responsabilit per danni causati da un collega con compromissione delle capacit di giudizio clinico . si deve infine ricordare che anche lazienda sanitaria , che in passato nel nostro paese era ritenuta esente da responsabilit penali in virt del principio di diritto romano secondo cui societas delinquere non potest pienamente compresa da obblighi di prevenzione e controllo , in accordo al principio della responsabilit sociale delle aziende , di chiara mutuazione anglosassone . 
 the need for proactive intervention necessit di un intervento proattivo in italy , the measures adopted against impaired physicians have been prevalently reactive and substantially belated . there is clearly a need to plan preventive action focused primarily on identifying the possible cases from among all possible individuals demonstrating problems in interpersonal relations , as well as the inability to achieve predefined objectives , to participate in teamwork or to change and adapt to a transition . 
the task of identifying these at - risk individuals should be shared among all health - care professionals in a measure proportional to their role within the organisational structure , without excluding anyone from the responsibility . regardless of the size of the health - care facility in which the impaired physician is operating , the first reference nel nostro paese le azioni nei confronti dei medici affetti da malattie che ne riducano la capacit di giudizio sono state sinora prevalentemente reattive e sostanzialmente tardive . palese la necessit di programmare interventi preventivi , focalizzati innanzi tutto ad identificare i possibili casi tra tutti quei soggetti che dimostrino problemi nelle relazioni interpersonali , incapacit a raggiungere gli obiettivi fissati , a partecipare al lavoro di squadra , a cambiare o adattarsi ad una transizione . 
il compito di identificare questi soggetti a rischio dovrebbe essere condiviso da tutti i sanitari , in misura proporzionale al ruolo che ciascuno di essi ricopre allinterno della struttura organizzativa , ma senza escludere le responsabilit di nessuno . qualunque sia la dimensione dellazienda sanitaria in 836 radiol med ( 2010 ) 115 : 826838 person for evaluation of the fitness to practise is the occupational health physician [ 41 ]  . 
it is not uncommon that the occupational health physician is able to identify those signs of difficulty to adapt to the work requirements mentioned above or is able to receive indications from the impaired physician regarding his or her illness and its negative effects on professional activity . 
therefore , the occupational health physician is most likely the first health - care professional to approach the issue of how the illness is affecting the professional activity of the impaired physician and prompt that physician to undertake a treatment programme [ 43 ]  . the need therefore arises to offer each impaired physician a diagnostictherapeutic and rehabilitative pathway that safeguards rights to privacy and autonomy . 
in the interim , until specialised facilities such as those present in in italy , english - speaking countries are established programmes to address the problem need to be entrusted to the facilities of the national health service . 
the occupational health physician should follow the treatment progress , maintaining close contact with treating physicians , and after recovery , closely monitor the treated physician to obviate possible relapse of the condition that had impaired the physicians judgement [ 44 , 45 ]  . regardless , the judgement of fitness to practise should take into account not only the possibility that exposure to work - related risk might aggravate the condition present in the impaired physician but also the possible effects for third parties ( patients , visitors , colleagues ) caused by the altered abilities of the impaired physician . it should be borne in mind that according to italian law , the task of the occupational health physician is formally circumscribed to aspects that do not imply a judgement on the individuals fitness to practise but only refer to workrelated risk for the health - care professional and third parties [ 46 ]  . 
in the event the condition from which the physician is suffering causes loss of ability to work , the evaluation should not be performed by the occupational health physician but by the public body to which the health - care professional should be sent upon request by the employer , in accordance with italian law no . 
italy is one of the few countries to have this dual level of judgement , thus guaranteeing and further safeguarding the civil rights of the health - care professional and having the aim of promoting recovery and limiting possible damage . it should nonetheless be recalled that the central role of the occupational health physician in managing the impaired radiologist should not be seen to limit the responsibility of other players within the health - care syste conversely , correct management of the impaired physician implies involvement of hospital management , the prevention and cui il medico ammalato si trova ad operare , la prima figura di riferimento per la valutazione dellidoneit lavorativa il medico competente [ 41 ]  . 
non infrequente che proprio il medico competente possa identificare quei segnali di difficile adattamento alle richieste lavorative cui sopra si faceva cenno , o ricevere dal collega ammalato indicazioni sulle patologie da cui questo affetto e sulle difficolt che ne derivano nelle attivit professionali . 
in definitiva , probabile che proprio il medico competente sia il sanitario che per primo pu affrontare il tema dellinterferenza della malattia con lattivit professionale del medico malato , ed indurlo ad accettare un programma di trattamento [ 43 ]  . sorge quindi la necessit di offrire a ciascun medico malato un percorso diagnostico - terapeutico e riabilitativo rispettoso dei diritti di riservatezza e di autonomia . 
nellattesa della realizzazione , anche nel nostro paese , di strutture specializzate del tipo esistente nei paesi anglosassoni , il percorso di recupero deve essere affidato alle strutture del servizio sanitario nazionale . 
il medico competente seguir i progressi del trattamento , tenendosi in stretto contatto con i medici curanti , e dopo lavvenuto recupero controller attentamente il collega , onde scongiurare possibili recidive della condizione che aveva determinato compromissione delle capacit di giudizio [ 44 , 45 ]  . il giudizio di idoneit , in ogni caso , terr conto non solo della possibilit che lesposizione ai rischi professionali possa aggravare la patologia presente nel medico malato , ma anche dei possibili effetti che potrebbero derivare ai terzi ( pazienti , visitatori , altri colleghi ) dallalterazione delle capacit del medico malato . occorre ricordare che nella nostra legislazione il compito del medico competente formalmente circoscritto ad aspetti che non implicano un giudizio sulla capacit lavorativa del soggetto , ma attengono appunto solo ai rischi professionali per il lavoratore e per terzi [ 46 ]  . 
nel caso che la patologia da cui il medico colpito dovesse determinare la perdita della capacit lavorativa , lorganismo competente a valutare non pi il medico competente , ma lente pubblico , al quale il lavoratore deve essere avviato su richiesta del datore di lavoro , ai sensi della legge 300 / 70 ( statuto dei lavoratori ) [ 47 ]  . 
il nostro paese uno dei pochi ad avere previsto questo doppio livello di giudizio , a garanzia e maggiore tutela dei diritti civili del lavoratore e nella finalit di favorire il recupero e limitare le possibilit di danno . in ogni caso , bene ricordare che il ruolo centrale del medico competente nella gestione del radiologo malato non deve tradursi in una deresponsabilizzazione delle altre figure aziendali . 
la corretta gestione del medico malato implica al contrario il coinvolgimento del management aziendale , del servizio di prevenzione e protezione , dei radiol med ( 2010 ) 115 : 826838 protection service and the other health - care professionals and their representatives in a process of consensus that determines the policy of the public hospital trust . 
it would be appropriate that the policy of each health - care facility be defined in detail and displayed prior to the occurrence of impairment , because formulating mutual decisions is much more difficult in the wake of concrete problems . 
81 / 08 makes explicit reference , should in the public hospital trusts explicitly involve the procedures set up to tackle the problem of the impaired physician , with a detailed outline of measures regarding informed consent , right to privacy , autonomy and responsibility of physicians , communication of patient risk and nondiscrimination of and support for the ill health - care professional [ 48 ]  . lavoratori e dei loro rappresentanti , in un processo di consenso che determini la politica dellazienda sanitaria . sarebbe opportuno che la policy di ciascuna struttura sanitaria venisse dettagliatamente definita ed esposta in anticipo rispetto al verificarsi di problemi di impairment , perch formulare decisioni condivise molto pi difficile nellincalzare di problemi concreti . 
multidetector ct coronary angiography ( mdctca ) permits , through curved multiplanar reconstructions and three - dimensional reformatting , noninvasive visualisation of the coronary tree and its variants and anomalies , providing a more accurate alternative to conventional coronary angiography ( cca )  . 
the purpose of this pictorial essay is to describe the main variants and anomalies of the coronary arteries using mdct imaging with multiplanar and three - dimensional reconstructions . keywords mdct - coronary angiography coronary anomalies coronary variants miocardial bridging fistula riassunto le anomalie delle arterie coronariche sono presenti alla nascita nella maggior parte dei casi asintomatiche ma possono manifestarsi con sintomatologia severa quale angina pectoris o addirittura larresto cardiaco . langiografia coronarica mediante tomografia computerizzata multistrato ( tcms ) permette , tramite ricostruzioni multiplanari secondo piani curvilinei e riformattazioni 3d , la visualizzazione dellalbero coronarico e delle sue varianti ed anomalie in maniera non invasiva , fornendo migliore e pi accurata alternativa alla angiografia coronarica ( ac )  . 
lo scopo di questo pictorial consiste nella descrizione mediante immagini tcms con ricostruzioni multiplanari e 3d delle principali varianti e anomalie delle arterie coronarie . parole chiave angiografia coronarica - tcms anomalie coronariche varianti coronariche ponte miocardico fistola introduction introduzione most of the coronary anomalies are incidental findings , without any reliable clinical correlation with possible symptoms . 
although the vast majority of anomalies are asymptomatic , some may manifest with symptoms such as angina pectoris , myocardial infarction , syncope , arrhythmia of varying severity or even cardiac arrest and sudden death [ 1 ]  . la maggioranza delle anomalie coronariche ( ac ) costituiscono reperti occasionali per le quali ancora non esiste una correlazione clinica ampia e affidabile tra queste ed eventuali sintomi . 
la stragrande maggioranza di esse asintomatica , tuttavia alcune di esse possono manifestarsi con sintomi come angina pectoris , infarto miocardico , sincope , 680 radiol med ( 2010 ) 115 : 679692 the most widely used method to study the coronary arteries and hence visualise coronary variants and anomalies is conventional coronary angiography ( cca )  . 
multidetector ct coronary angiography ( mdct - ca ) , by allowing curved multiplanar reconstructions ( mpr ) and 3d reformatting , provides a noninvasive tool to depict the coronary tree and its variants and anomalies . 
it has therefore become an accurate and valuable alternative to cca in determining the presence of atherosclerosis and assisting cardiologists , haemodynamicists and heart surgeons in evaluating normal , variant or anomalous coronary circulation [ 2 ]  . 
moreover , with its multiplanar and volume - rendered ( vr ) reformations , mdct - ca outperforms cca in determining the relative position of vessels , thus providing a better view of the coronary vascular anatomy , whether normal , variant or anomalous . 
the purpose of this pictorial essay is to describe the main variants and anomalies of the coronary arteries using mdct imaging with multiplanar and 3d reconstructions . classification coronary variants occur in less than 1% of the population and are completely asymptomatic ; coronary anomalies , instead , affect 1.3% of the general population [ 3 ]  . 
ad oggi la metodica pi utilizzata per lo studio delle arterie coronariche , e quindi per la visualizzazione delle varianti e anomalie , langiografia coronarica convenzionale ( acc )  . langiografia coronarica mediante tomografia computerizzata multistrato ( tcms ) permette , tramite ricostruzioni multiplanari secondo piani curvilinei e riformattazioni 3d , la visualizzazione dellalbero coronarico e delle sue varianti ed anomalie in maniera non invasiva , fornendo valida e accurata alternativa alla acc per determinare la presenza o meno di malattia aterosclerotica e fornire un valido supporto alla valutazione del circolo coronarico normale variante o anomalo da parte del cardiologo , dellemodinamista e del cardiochirurgo [ 2 ]  . 
inoltre , grazie alle riformattazioni multi planarie e volume rendered , la actcms riesce meglio della coronarografia a proiettare adeguatamente la posizione dei vasi permettendo una migliore visualizzazione dellanatomia vascolare coronarica sia essa normale , variante o anomala . 
lo scopo di questo pictorial consiste nella descrizione mediante immagini tcms con ricostruzioni multiplanari e 3d delle principali varianti e anomalie delle arterie coronarie . classificazione le varianti del circolo coronarico rappresentano evenienza inferiore all1% dei casi e sono del tutto asintomatiche ; le anomalie invece coinvolgono l1 , 3% della popolazione generale [ 3 ]  . 
nell80%90% dei casi ci spetta alla arteria coronaria destra che a livello della crux si biforca in arteria interventricolare posteriore e ramo postero laterale ben radiol med ( 2010 ) 115 : 679692 fig . 
coronary dominance refers to which coronary system supplies the base of the heart and , in particular , the inferolateral wall of the left ventricle . in 80%90% of cases , this function is performed by the right coronary artery ( curved arrow in a - c ) , which bifurcates at the crux ( asterisk in c , e ) into the posterior interventricular artery ( arrowhead in c , e ) and the posterolateral branch ( arrow in c , e ) , which is well developed when the terminal portion of the circumflex artery is hypoplastic ( large arrow in a , d )  . 
with the 3d volume - rendered and 3d reconstructions of the coronary tree alone ( 3d tree ) , the atrioventricular course of the right coronary artery is displayed up to the intersection of the four cardiac chambers ( crux ) where the posterior interventricular artery and the posterolateral branch originate . 
la dominanza del circolo coronarico indica quale sistema dei vasi coronarici vicaria il flusso sanguigno alla base del cuore ed in particolare la parete inferolaterale del ventricolo sinistro . nell80%90% dei casi ci spetta alla arteria coronaria destra ( freccia curva in a - c ) che a livello della crux ( asterisco in c , e ) si biforca in arteria interventricolare posteriore ( testa di freccia in c , e ) e ramo postero laterale ( freccia in c , e ) ben sviluppato quando il tratto terminale dellarteria circonflessa ipoplasico ( freccia grossa in a , d )  . 
mediante ricustruzioni 3d volume rendered e 3d del solo albero coronarico ( 3d tree ) si visualizza il decorso atrioventricolare dellarteria corona destra fino alla intersezione delle 4 camere cardiache ( crux ) ove prendono origine larteria interventricolare posteriore e il ramo postero laterale . 
the 3d volumerendered and 3d reconstructions of the sole coronary tree ( 3d tree ) show a hypoplastic right coronary artery ( curved arrow in a , b , d ) and the origin of the posterior interventricular artery ( arrow in b - d ) from the circumflex artery at the level of the crux ( asterisk in c ) fig . 
ricostruzione dellalbero coronarico mediante ricustruzioni 3d volume rendered e 3d del solo albero coronarico ( 3d tree ) ove lipoplas dellarteria si visualizza coronaria destra ( freccia curva in a , b , d ) e la origine dallarteria circonflessa a livello della crux ( asterisco in c ) dellarteria interventricolare posteriore ( freccia in b - d )  . 
 emerging from the proximal third of the right coronary artery or from the proximal circumflex artery , or it may , instead , receive a balanced supply from both arterial systems . 
however , the easiest to apply is that proposed by rigatelli [ 4 ] , which also considers patient management and follow - up . class i : benign coronary anomalies the most frequent anomalies in this group tend to be clinically asymptomatic and are not correlated with myocardial ischaemia or sudden death , although an association with varying degrees of atherosclerotic disease has often been reported . 
normalmente il nodo seno atriale vascolarizzato da un vaso che emerge dal terzo prossimale dellarteria coronaria destra ma che pu originare anche dal tratto prossimale dellarteria circonflessa o avere invece vascolarizzazione bilanciata da entrambi i sistemi arteriosi . per classificare invece le anomalie del circolo coronarico molti autori hanno proposto una possibile classificazione anatomo - clinica delle anomale in maggiori e minori [ 58 ] , ma quella di pi semplice utilizzo quella proposta da rigatelli [ 4 ] che considera anche la gestione ed il follow - up . 
 classe i : ac benigne quelle pi frequenti di questo gruppo sono in genere silenti dal punto di vista clinico e non sono state correlate allischemia miocardica o alla morte improvvisa , sebbene sia radiol med ( 2010 ) 115 : 679692 fig . 
nel 5% dei casi la vascolarizzazione della base del cuore sostenuta sia dal sistema coronarico destro che da quello sinistro . ricostruzione dellalbero coronarico di 2 casi ( a , d - f ) mediante mappa 2d , ricustruzioni 3d volume rendered e 3d del solo albero coronarico ( 3d tree ) che dimostrano origine del ramo postero laterale ( testa di freccia in a - d ) dallarteria circonflessa e ramo interventricolare inferiore ( freccia in a , b , d - f ) originante dallarteria coronaria destra . 
 [ 10 ] into different subtypes based on the distribution and course of septal and diagonal branches within the interventricular groove , is not associated with adverse events in the absence of coexisting atherosclerosis . myocardial bridging was first described by reyman in 1737 as a coronary artery coursing within the myocardium . che si pu confondere con un vaso collaterale pervio , indicativo di una probabile ostruzione dellarteria coronaria . unorigine indipendente della arteria discendente anteriore ( ada ) sinistra e della arteria circonflessa ( acx ) pu essere relativamente frequente . 
la sua rilevanza clinica correlabile alla possibilit di compressione durante un intervento chirurgico di sostituzione valvolare . la presenza di un doppio ramo interventricolare anteriore ( discendente anteriore ) , classificato da spindola - franco et radiol med ( 2010 ) 115 : 679692 fig . 
the second branch originating from the right coronary artery ( curved arrow in a , b ) is the sinus artery , so called because it supplies the sinoatrial node . maximum intensity projections , 3d volumerendered images and volume - rendered images of the coronary tree alone ( vr tree ) show normal and variant origins of the sinus artery . usually , the sinoatrial node is supplied by a vessel ( arrow ) emerging from the proximal third of the right coronary artery but may also originate from the proximal portion of the circumflex artery ( arrowhead in c , d )  . 
le immagini ottenute in mip , volume rendering 3d , volume rendering del solo albero coronarico ( vr tree ) dimostrano lorigine normale e variante dellarteria del seno . normalmente il nodo seno atriale vascolarizzato da un vaso ( freccia ) che emerge dal terzo prossimale dellarteria coronaria destra ma che pu originare anche dal tratto prossimale dellarteria circonflessa ( testa di freccia in c , d )  . 
3d volume - rendered ( a , c ) and , 2d map ( b , d ) reconstructions showing a common branch of the right ( arrow in b , d ) and left coronary arteries emerging from the right sinus of valsalva . 
whereas the course of the right coronary artery correctly follows the right atrioventricular groove , the left coronary artery ( arrowhead ) surrounds the trunk of the pulmonary artery and courses upwards along the anterior interventricular groove , giving rise to the circumflex artery . 
ricostruzioni vr in a , c , 2d map che dimostrano lemergenza comune dal seno di valsalva destro di arteria coronaria destra ( freccia in b , d ) e sinistra . mentre il decorso dellarteria coronaria destra regolarmente disposto a livello del solco atrioventricolare destro larteria coronaria sinistra ( testa di freccia ) circonda il tronco dellarteria polmonare e risale il solco interventricolare anteriore dando origine allarteria circonflessa . 
the ostium of the right coronary artery may arise abnormally from the left sinus of valsalva ( arrow ) separately from the left coronary artery , in which case it courses between the aortic pedicle and the trunk of the pulmonary artery . 
7a - e anomalie di origine / ostio separato / decorso interarterioso . lostio dellarteria coronarica destra pu originare in modo anomalo dal seno di valsalva sinistro ( freccia ) separatamente rispetto allarteria coronaria sinistra , in questo caso il decorso tra il peduncolo aortico e il tronco dellarteria polmonare . 
la potenziale compressione di questo vaso in condizioni di base o di iperaflusso ( attivit sportiva , stress ) pu risultare asintomatica o provocare episodi ischemici , infarto miocardico e morte improvvisa . it is characterised by systolic compression of the tunnelled segment , a condition that is , however , completely asymptomatic in the vast majority of cases . 
myocardial bridges mainly involve the intermediate segment of the anterior descending artery , even though diagonal and marginal branches may be affected in 18% and 40% of cases , respectively [ 11 , 12 ]  . 
 class ii : coronary anomalies related ischaemia to myocardial coronary anomalies causing myocardial ischaemia in the absence of coronary disease are considered clinically relevant : coronary fistula is an anomaly capable of causing or predisposing to myocardial ischaemia and congestive heart failure , since , by draining into the right ventricle , it may lead to leftright shunt with volume overload ( fig . 9 ) [ 13 , 14 ]  . the ectopic origin of the left coronary artery from the pulmonary artery apparently influences the survival of affected children and in 90% of cases requires early surgical correction . 
 [ 10 ] in differenti sottotipi , in base alla distribuzione e al decorso nel solco interventricolare dei rami settali e diagonali , non associabile ad eventi sfavorevoli se non coesiste una malattia aterosclerotica . i ponti miocardici sono stati descritti per la prima volta da reyman nel 1737 come una arteria coronaria il cui decorso sia tunnelizzato nel contesto del miocardio . 
i ponti miocardici coinvolgono prevalentemente il segmento intermedio della ada anche se possono essere coinvolti i rami diagonali e marginali nel 18% e 40% dei casi rispettivamente [ 11 , 12 ]  . 
 8a - d course myocardial bridging . in 10% of cases , coronary vessels course within the myocardial musculature rather than along the epicardial surface [ 7 ]  . this tunnelling may be either superficial ( arrows in a , b ) or deep ( arrows in c , d ) and may cause anginal symptoms . 
 segmento ove pi frequentemente si osserva un ponte intramiocardico il tratto intermedio dellarteria discendente anteriore . ciated with myocardial ischaemia , with a higher risk of coronary disease and cardiac overload . the presence of a single coronary artery , divided into r or l subtypes ( i - ii - iii ) , is associated with myocardial ischaemia due to an insufficient ability to support the normal coronary circulation [ 15 ]  . 
 coronary atresia , which is considered benign although is a possible cause of myocardial ischaemia , is usually associated with other congenital malformations in children with rubella syndrome , hurler syndrome , and friedereichs ataxia . class iii : association between coronary disease and sudden death depending on their origin , course and distribution , coronary anomalies have recently been considered the main cause of 5%35% of sudden death in the youth [ 16 ] , whereas an abrupt and sharp angulation in the proximal portion of a coronary artery and the presence of valve - like septa close to the ostium may lead to sudden death in the lorigine ectopica dellarteria coronaria sinistra dallarteria polmonare sembra influenzare la sopravvivenza dei bambini portatori , e nel 90% dei casi , necessita di una correzione chirurgica precoce . 
nelladulto questanomalia si pu associare ad ischemia miocardica , ad un pi elevato rischio di malattia coronarica e ad un sovraccarico cardiaco . la presenza di ununica arteria coronaria , distinta in diversi sottotipi r o l ( i - ii - iii ) , si associa ad ischemia miocardica per la inadeguata capacit di sostenere adeguatamente la normale circolazione coronarica [ 15 ]  . 
 unulteriore ac da considerarsi benigna , sebbene in grado di provocare ischemia miocardica , latresia coronarica che , di solito , si associa ad altre malformazioni congenite nei bambini con sindrome da rubeola , di hurler e di friederich . classe iii : associazione tra malattie coronariche e morte improvvisa le ac in quanto ad origine , decorso e distribuzione sono state , recentemente , ritenute la principale causa del 5%35% 688 radiol med ( 2010 ) 115 : 679692 fig . 
coronary fistula is an anomaly capable of causing or predisposing to myocardial ischaemia and congestive heart failure , as , by draining into the right cardiac sections , it may lead to left - right shunt with volume overload [ 9 , 10 ]  . 
la fistola coronarica una anomalia coronarica in grado di determinare o predisporre ad un evento ischemico miocardico ed a scompenso cardiaco congestizio , in quanto , drenando nelle sezioni cardiache di destra , pu determinare uno shunt sinistro destro con sovraccarico di volume [ 9 , 10 ]  . 
tramite fistoloso ( freccia rossa ) del secondo ramo settale dellarteria discendente anteriore nel tratto medio con il tronco comune dell`arteria polmonare . absence of coronary disease [ 17 ]  . 
nineteen per cent of sudden deaths in young athletes are attributed to a coronary anomaly , as intense physical exertion in the presence of coronary anomaly can lead to sudden death [ 1 ]  . subtypes of single coronary arteries are rare conditions in which cardiac perfusion is completely delegated to a right coronary artery originating from a left coronary artery , generally passing between the pulmonary artery and the aorta . 
this coronary anomaly carries a high risk of fatal event . the clinical significance of the ectopic origin of the left coronary artery from the right sinus of valsalva depends on its position and anatomical course relative to the aorta and pulmonary artery . 
in cases in which the right coronary artery arises ectopically from the left sinus of valsalva , the vessel runs between the aorta and the pulmonary artery . possible coronary occlusion during systolic expansion of the aorta is a potentially dangerous event . 
 [ 4 ] , patients with this anomaly are at di morti improvvise nei giovani [ 16 ] , mentre una brusca ed acuta angolazione nel tratto prossimale di unarteria coronaria e la presenza di setti simili a delle valvole in prossimit del suo ostio , in assenza di malattia coronarica , possono essere la causa di una morte improvvisa [ 17 ]  . 
il 19% delle morti improvvise nei giovani atleti sono da considerare imputabili alla presenza di una ac , infatti , in presenza di una ac , un intenso sforzo fisico pu essere causa di morte improvvisa [ 1 ]  . 
i sottotipi di arterie coronarie uniche rappresentano una rara condizione nella quale la perfusione cardiaca totalmente affidata ad unarteria coronaria destra che origina da una coronaria sinistra , passando , generalmente , tra arteria polmonare e aorta . 
quando presente questa ac il rischio di un evento fatale per il soggetto portatore elevato . il significato clinico dellorigine ectopica dellarteria coronaria sinistra dal seno di valsalva destro , dipende dalla sua posizione e dal decorso anatomico rispetto allaorta e allarteria polmonare . 
nei casi in cui larteria coronaria destra ha unorigine ectopica dal seno di valsalva sinistro , il vaso decorre fra laorta e larteria polmonare . la possibilit di unocclusione coronarica , durante lespansione sistolica aortica , rappresenta un evento radiol med ( 2010 ) 115 : 679692 10a - d intrinsic increased coronary fig . 
coronary vessels have a well - known mean calibre of 45 mm at their emergence from the sinuses of valsalva to 2 mm in the distal portions of the two main systems [ 8 ]  . 
in these cases , stenosis of a segment is always measured as a ratio of the luminal diameter of the stenotic segment and that of the segments before and after the stenosis . 
i vasi coronarici presentano un calibro medio ben definito , pari a circa 45 mm allemergenza dai seni di valsalva fino ai 2 mm nei tratti distali dei due sistemi principali [ 8 ]  . 
vi possono essere delle condizioni quali la malattia di kawasaki , liperafflusso coronarico in cui i vasi appaiono ectasici in toto ( frecce ) o presentano dilatazioni sacciformi in alcuni suoi tratti . 
in questi casi la stenosi di un segmento viene sempre misurata come rapporto del calibro del lume nel tratto stenosico e nel segmento a monte e a valle della stenosi . 
alcuni autori suggeriscono che la chiave nella formazione dellectasia coronarica stia nello strato medio anormale del vaso che pu portare ad un processo abnorme di aterosclerosi intimale . increased risk of malignant ventricular arrhythmia and require prompt treatment . the anomalous origin of the right coronary artery from the pulmonary artery is a rare , usually benign occurrence , which may nonetheless be associated with sudden death , especially following physical exertion [ 18 ]  . 
first described by morgagni in 1761 and subsequently reported by bourbon in 1812 , it was categorised by markis [ 19 ] based on the extent of involvement of the coronary vessels . 
type i indicates diffuse ectasia of two or three vessels ; type ii , diffuse ectasia of one vessel and focal disease in another ; type iii , diffuse ectasia of one vessel only ; type iv , segmental or focal involvement only . 
 [ 4 ] , i pazienti con tale anomalia hanno un alto rischio di aritmie ventricolari maligne e devono essere tempestivamente trattati . lorigine anomala dellarteria coronaria destra dallarteria polmonare unevenienza rara , pi frequentemente a decorso clinico benigno , ma , talvolta , associato a morte improvvisa , soprattutto da sforzo fisico [ 18 ]  . 
descritta per la prima volta da morgagni nel 1761 , e riportata poi da bourbon nel 1812 con la descrizione di un caso , stata classificata da markis [ 19 ] in categorie a seconda del coinvolgimento dei vasi coronarici . 
il tipo i rappresenta una diffusa ectasia di due o tre vasi , il tipo ii una ectasia diffusa in un vaso e una malattia focale in un altro , il tipo ii una ectasia diffusa in solo un vaso e il tipo iv rappresenta infine solo un coinvolgimento segmentarlo o focale . 
this condition is exacerbated by dilatation of the ascending aorta due to exertion , such that the circular ostium of the coronary vessel is turned into a valve - like ridge causing vessel closure . 
extrinsic compression of the anomalous coronary artery along its course between the aorta and the pulmonary artery after exertion , such that the aortic arch and the trunk of the pulmonary artery become dilatated . 
this hypothesis is contradicted by the fact that during exertion , diastolic pressure in the trunk of the pulmonary artery is usually lower than coronary diastolic pressure . this condition may be different if it is superimposed with atherosclerosis or a change in the ostium configuration , which reduces perfusion pressure of the anomalous coronary artery . 
although previous studies have described substantial atherosclerotic involvement in the event that the left coronary artery [ 21 ] and circumflex artery [ 16 , 17 ] follow a posterior course , topaz [ 22 ] showed no significant increase in the risk of developing atherosclerosis in these patients . 
 class iv : association between coronary anomaly and coronary disease although no studies have demonstrated which coronary anomaly is linked to a preferential incidence of coronary disease , there have been a few interesting observations in this regard . 
 [ 25 ] first suggested that an anomalous circumflex artery has a higher degree of stenosis than normal arteries , but the location and degree of stenosis in the la patogenesi di tale condizione non del tutto nota . 
questa condizione diviene esasperata con la dilatazione dellaorta ascendente secondaria a sforzi , modificando lapertura circolare del vaso coronarico in una sorta di soffietto a valvola in modo da portare alla chiusura del vaso . 
sebbene gi precedenti studi abbiano descritto un buon grado di coinvolgimento aterosclerotico nel caso di decorso posteriore della coronaria di sinistra [ 21 ] e della circonflessa [ 16 , 17 ]  . 
 classe iv : associazione tra ac e malattia coronarica sebbene non esistano studi che dimostrano quale ac determini una incidenza preferenziale della malattia coronarica , un certo numero di autori riporta alcune osservazioni interessanti a questo proposito . 
 [ 23 ] hanno riscontrato che la presenza di unanomalia dellarteria circonflessa espone pi precocemente e con maggiore estensione ad un processo aterosclerotico rispetto allo stesso vaso in assenza di anomalie . 
 [ 24 ] , anche se le arterie coronarie sono soggette agli stessi fattori di rischio sistemici , laterosclerosi coronarica focale ed eccentrica , ed ogni lesione ha unevoluzione indipendente . 
 [ 25 ] hanno per primi suggerito che unarteria circonflessa anomala presenta un maggiore grado di stenosi rispetto alle arterie normali , ma la radiol med ( 2010 ) 115 : 679692 anomalous artery do not influence the individuals survival . 
 [ 22 ] reported an incidence of 28%33% of coronary disease in anomalous arteries and , more importantly , a 66%68% incidence of coronary disease in patients with coronary anomalies , suggesting that these two conditions are mutually independent . localizzazione ed il grado di stenosi nellarteria anomala non influenzano la sopravvivenza del soggetto . 
 [ 22 ] , hanno rilevato unincidenza del 28%33% di malattia coronarica nelle arterie anomale e , soprattutto , unincidenza di malattia coronarica in pazienti con ac pari al 66%68% , suggerendo che queste due condizioni sono indipendenti . conclusions mdct - ca can provide highly accurate anatomical imaging of the cardiac vessels . 
in all those applications in which knowledge of the anatomy of the cardiac vessels is especially important , mdct - ca represents a noninvasive diagnostic modality capable of visualising the largest number of coronary segments , in particular , distal segments . 
furthermore , because coronary anomalies are a relatively frequent finding in the setting of noninvasive diagnostic coronary imaging , it is reasonable to expect that mdct - ca , with its rapidity , noninvasiveness and low cost , will become the ideal tool with which to evaluate patients at low risk of coronary diseases and in the followup of percutaneous and / or surgical procedures in the coronary vessels . 
in tutte quelle applicazioni nelle quali la conoscenza della anatomia dei vasi del cuore importante , la coronarografia tc costituisce ad oggi la metodica diagnostica non invasiva in grado di visualizzare il maggior numero di segmenti coronarici ed in particolare anche quelli distali . 
obstruction site was recognised in all cases ( 5 / 27 ascending colon ; 1 / 27 transverse colon ; 11 / 27 descending colon ; 10 / 27 sigma - rectum )  . 
sono state valutate le immagini tcmd di 27 pazienti con occlusione neoplastica del colon e sono stati ricercati : sede dellostruzione ; morfologia della parete colica ; alterazione del contenuto endoluminale ; diametro trasversale del colon destro . 
la sede dellocclusione stata riconosciuta in tutti i casi ( 5 / 27 colon destro ; 1 / 27 traverso , 11 / 27 colon sinistro ; 10 / 27 tratto sigma - retto )  . 
il contenuto endoluminale risultato prevalentemente gassoso in 3 / 27 pazienti , prevalentemente fluido in 11 / 27 , e di tipo misto , con livelli idroaerei , in 13 / 27 . 
il riconoscimento di livelli idroaerei ha indicato prognosi infausta in 7 / 13 casi . la presenza di pneumatosi parietale ( 7 / 9 deceduti ) e un diametro del colon destro 10 cm ( 7 / 7 deceduti ) sono risultati indici prognostici sfavorevoli . 
la tcmd consente di riconoscere presenza e sede di unocclusione neoplastica del grosso intestino e pu fornire utili valutazioni prognostiche . parole chiave occlusione intestinale colon prognosi tomografia computerizzata tcmd 748 introduction intestinal occlusion is one of the most common causes of acute abdomen , being responsible for its onset in 20%25% of cases . 
obstruction occurs in the small bowel in 60% of cases and is most commonly due to postoperative adhesions ( 38.5% ) and hernia ( 21.7% ) [ 1 , 2 ]  . 
occlusion of the large bowel is less common and differs in aetiology ( generally malignant ) , pathophysiology , treatment and prognosis , with a mortality rate around 20% [ 3 ]  . 
in terms of histology , 98% of malignant occlusions are caused by adenocarcinoma of the large bowel , which is also the most frequent tumour affecting the gastrointestinal tract , accounting for around 70% of all cancers in this region [ 4 ]  . upon suspicion of intestinal occlusion , plain abdominal x - rays are generally the first examination to be performed . this technique has an accuracy of 75%80% and sensitivity of 84% [ 5 ]  . 
nonetheless , in the presence of malignant disease , the technique can be considered incomplete , as it provides no useful information for local and distant staging of the tumour [ 5 ]  . 
 ( 82%98% the diagnosis upon clinical suspicion of occlusion or in the presence of known occlusion identified with abdominal x - rays , ultrasound ( us ) can provide useful information for sensitivity , confirming 80%100% specificity ) and defining the site ( 70%85% of cases ) and nature ( 20%80% of cases ) of the occlusion , especially in paediatric patients [ 79 ]  . 
magnetic resonance imaging ( mri ) has also been proposed in the literature for studying small - bowel occlusion , and the technique is specifically indicated in pregnant patients [ 1012 ]  . 
multidetector - row computed tomography ( mdct ) , as the numerous studies in the literature demonstrate , is the most widely used imaging modality in the evaluation of large - bowel obstruction . 
mdct , when associated with multiplanar reconstructions ( mpr ) and volume rendering ( vr ) , is accurate in defining the presence , level and he nature of the occlusion and has a sensitivity of 83% , specificity of 93% and accuracy of 91% in identifying the presence of ischaemic complications [ 1416 ]  . the aim of our study was to evaluate ct findings appreciable in malignant occlusions of the large bowel and identify possible correlations with postoperative prognosis . radiol med ( 2010 ) 115 : 747757 introduzione locclusione intestinale una delle cause pi frequenti di addome acuto e ne determina linsorgenza in circa il 20%25% dei casi . 
lostacolo alla canalizzazione intestinale localizzato in corrispondenza del tenue nel 60% dei casi ed pi spesso determinato da aderenze post - operatorie ( 38 , 5% ) ed ernie ( 21 , 7% ) [ 1 , 2 ]  . 
lostruzione del grosso intestino meno frequente e differisce per eziologia , in genere neoplastica , fisiopatologia , terapia e prognosi , con un tasso di mortalit di circa il 20% [ 3 ]  . 
da un punto di vista istologico , il 98% delle ostruzioni neoplastiche sono determinate da adenocarcinoma del grosso intestino , che peraltro rappresenta il tumore del tratto gastrointestinale pi frequente , circa il 70% di tutte le neoplasie [ 4 ]  . nel sospetto di occlusione intestinale lesame rx diretto delladdome la prima indagine che viene generalmente eseguita e presenta unaccuratezza del 75%80% ed una sensibilit del 84% [ 5 ]  . 
in passato , nel sospetto di unostruzione del colon veniva utilizzato il clisma opaco , che nel riconoscimento di unocclusione ha una sensibilit del 96% ed una specificit del 98% ; tale indagine , comunque , in presenza di una patologia neoplastica da considerare incompleta , poich non consente una stadiazione locale ed a distanza del tumore [ 5 ]  . nel sospetto clinico od in presenza di occlusione intestinale gi accertata mediante rx diretto delladdome , lecotomografia ( us ) pu fornire utili informazioni nella conferma della diagnosi ( sensibilit 82%98% , specificit 80%100% ) e nel definire la sede ( 70%85% dei casi ) e la natura ( 20%80% dei casi ) dellostruzione , anche e soprattutto in et pediatrica [ 79 ]  . 
nello studio delle occlusioni intestinali del tenue stato proposto in letteratura anche limpiego della risonanza magnetica ( rm ) e tale indagine trova precise indicazioni nelle pazienti in stato gestazionale [ 1012 ] ; allo stato attuale , comunque , per quanto di nostra conoscenza , non sono state riportate esperienze riguardanti il suo utilizzo nelle occlusioni del colon . 
la tomografia computerizzata multidetettore ( tcmd ) , come ampiamente riportato in letteratura , attualmente la metodica pi utilizzata per valutare unocclusione del grosso intestino con una sensibilit del 96% , una specificit del 94% , ed un valore predittivo positivo del 100% [ 2 , 13 ]  . 
tale indagine , infatti , associando alla valutazione assiale ricostruzioni multiplanari ( mpr ) e volume rendering ( vr ) , accurata nel definire la presenza , il livello e la natura dellocclusione e mostra una sensibilit del 83% , una specificit del 93% ed unaccuratezza del 91% nel riconoscere eventuali complicanze ischemiche [ 1416 ]  . 
 scopo del presente lavoro valutare le alterazioni tomodensitometriche riconoscibili nelle occlusioni neoplastiche del grosso intestino , e ricercare una loro eventuale correlazione prognostica post - operatoria . radiol med ( 2010 ) 115 : 747757 materials and methods we retrospectively reviewed the mdct examinations of 27 patients ( 15 men and 12 women ) aged 5780 ( mean 66 ) years suffering from adenocarcinoma of the colon who were studied between january 2006 and december 2008 . 
in this way , we obtained a list of 36 patients , of whom nine with distant metastases were excluded ( five with hepatic metastases ; four with hepatic and pulmonary metastases )  . definitive diagnosis was made surgically with histological analysis of the resected tumour in all cases , and surgery was performed after mdct examination with a delay between 10 and 48 h . 
in all cases , scans were performed before and after intravenous injection of contrast material ( 120140 ml injected at a rate of 3.03.5 ml / s ) , with image acquisition in the arteriolar phase , with a delay of 3040 s from the beginning of contrast material administration ; and in the venous phase , with a delay of 6070 s from the beginning of contrast material administration . 
postprocessing included mpr and vr and took around 15 m analysis of axial and reconstructed images was performed in a blind fashion by two radiologists ( ga , aasi ) and included the following parameters : evidence and site of the occlusion bowel - wall morphology ( thickness , enhancement , pneumatosis intestinalis ) at the site of disease and in the proximal bowel loops ; bowel - wall thickness was quantitatively evaluated and classified as pathological when > 5 mm ; presence of pneumatosis intestinalis was considered an indicator of parietal ischaemia changes in colonic content , classified according to the materiali e metodi sono stati esaminati retrospettivamente gli esami tc di 27 pazienti ( 15 uomini , 12 donne ) , di et compresa tra 57 e 80 anni ( et media 66 anni ) , affetti da adenocarcinoma del colon , studiati nel periodo compreso tra gennaio 2006 e dicembre 2008 . 
stata in tal modo ottenuta una lista di 36 pazienti , da cui ne sono stati esclusi 9 con metastasi a distanza ( in 5 casi epatiche , in 4 epatiche e polmonari )  . 
la diagnosi definitiva stata confermata chirurgicamente , con istologia del segmento asportato , in tutti i casi e lintervento stato eseguito dopo lesame tc con un ritardo compreso tra le 10 e le 48 ore . 
per quanto riguarda la stadiazione del tumore , considerando esclusivamente il parametro t , sono risultati 9 casi t2 ( 33 , 3% ) , 12 t3 ( 44 , 5% ) e 6 t4 ( 22 , 2% )  . 
levoluzione prognostica del paziente stata valutata 2 mesi dopo lintervento chirurgico . gli esami tc sono stati eseguiti con apparecchiature tcmd a 16 strati ( tsx - 101a , aquilion 16 , toshiba medical system , tokio , giappone ) , tcmd a 4 strati ( mx 8000 , philips medical systems , royal philips electronic , best , olanda ) , utilizzando , rispettivamente , i seguenti parametri di acquisizione : spessore di strato 1 e 2 , 5 mm ; pitch 1 , 75 e 1 , 25 ; increment 0 , 8 e 0 , 6 mm ; tempo di rotazione del tubo 0 , 5 s ; kv / mas 120 / 250 . 
in tutti i casi sono state eseguite scansioni prima e dopo iniezione endovenosa di mezzo di contrasto ( 120140 ml iniettati alla velocit di 33 , 5 ml / s ) , con acquisizione delle immagini in fase arteriolare , con ritardo compreso tra 3040 s dallinizio della somministrazione del mezzo di contrasto , ed in fase venosa , con ritardo compreso tra 6070 s dallinizio della somministrazione del mezzo di contrasto . 
le immagini assiali e quelle ricostruite sono state analizzate in cieco da due radiologi ( ga , aasi ) considerando i seguenti parametri : evidenza e sede dellostruzione . morfologia parietale ( spessore , enhancement , pneumatosi parietale ) , nella sede della patologia e nelle anse a monte . 
lo spessore parietale stato valutato quantitativamente e considerato patologico quando superiore a 5 mla presenza di pneumatosi stata considerata significativa di ischemia parietale . alterazione del contenuto colico , differenziata rapporto alla comparsa di sovradistensione gassosa , riempimento fluido , livelli idroaerei . 
1a - c occlusione del grosso intestino con alterazione del contenuto endoluminale : gassoso ( a ) , prevalentemente fluido ( b ) e di tipo misto , con evidenza di livelli idroaerei ( c )  . 
successivamente , al fine di confrontare le alterazioni tomodensitometriche riscontrate con la prognosi dei pazienti , stato applicato il test del chi quadrato sui valori percentuali e calcolato il valore di p . 
no additional diagnostic information was obtained from the 3d vr images with respect to the mpr . the occlusion was located at the level of the ascending colon in five patients ( 18.6% ) , the transverse colon in one ( 3.7% ) , the descending colon in 11 ( 40.7% ) and the le alterazioni riscontrate allesame tc sono riportate nella tabella 1 . 
pneumatosis intestinalis at the level of the ascending colon was found in nine patients ( 33% ) , whereas locoregional lymphadenopathies were present in 12 ( 44% )  . the overall mortality rate in our series was 37% and was correlated with some of the ct changes identified . 
in particular , the presence of gaseous distension correlated with a favourable prognosis ( all patients exhibiting this change were alive 2 months after surgery ) , as was a prevalently fluid - filled bowel , which was associated with death in 3 / 11 patients ( 27% )  . 
il tumore , responsabile dellostruzione , era riconoscibile in tutti i casi e determinava la comparsa di un ispessimento parietale medio di 1 , 4 cm ( range 13 , 2 )  . 
dopo liniezione di mezzo di contrasto , il tessuto neoplastico presentava un incremento di densit disomogeneo in 26 casi ( 96% ) e omogeneo in 1 ( 4% )  . 
linfoadenopatie locoregionali erano presenti in 12 / 27 pazienti ( 44% )  . il tasso di mortalit complessivo nel nostro campione stato del 37% ed risultato correlabile ad alcune alterazioni tomodensitometriche riscontrate . 
in particolare , levidenza di una distensione gassosa ha mostrato una correlazione prognostica favorevole ( tutti i pazienti con tale alterazione erano viventi a due mesi dallintervento ) , cos pure la distensione prevalentemente liquida , associata al decesso soltanto in 3 / 11 pazienti ( 27% )  . 
da un punto di vista strettamente statistico , comunque , la tipologia del contenuto intestinale , in rapporto al numero limitato di pazienti , ha mostrato una insufficiente significativit ( p > 0 , 05 )  . 
la presenza di pneumatosi parietale , sempre ed esclusivamente localizzata in corrispondenza del colon destro , si associata a morte del paziente in 7 / 9 casi ( 78% ) ed risultata un indice prognostico sfavorevole , con significativit statistica ( p = 0 , 002 )  . 
un diametro del colon destro 10 cm ha rappresentato un altro indice prognostico fortemente sfavorevole , essendo stato riscontrato in 7 pazienti , tutti deceduti a 2 mesi dallintervento ( p = 0 , 0001 )  . 
il grado di concordanza ottenuto tra i due lettori nella valutazione dei suddetti parametri risultato quasi perfetto ( k = 0 , 85 )  . discussion discussione in intestinal occlusions , the obstruction involves the colon in around 40% of cases [ 1 ] , and the stenosis is produced in nelle occlusioni intestinali lostacolo alla canalizzazione si localizza in corrispondenza del colon in circa il 40% dei radiol med ( 2010 ) 115 : 747757 fig . 
therefore , despite the broad awareness casi [ 1 ] e la stenosi pu essere determinata in ordine di frequenza da adenocarcinoma del colon - retto nel 47 , 4% dei casi , da aderenze nel 36 , 3% dei casi , da tumori retroperitoneali nel 5 , 5% , da ernie nel 2 , 7% [ 17 ]  . 
il carcinoma del colon - retto pertanto la causa pi frequente di occlusione del grosso intestino e rappresenta circa l85% delle 754 radiol med ( 2010 ) 115 : 747757 fig . 
c la ricostruzione coronale evidenzia la stenosi neoplastica ( freccia ) e la marcata dilatazione delle anse coliche a monte . of preventive measures , colorectal cancer is still diagnosed late , with the onset of occlusion in 7%47% of cases [ 19 , 2124 ]  . as mentioned above , ct has become a widely used imaging modality in patients with suspected intestinal occlusion , given its accuracy in defining presence , site and nature of the obstruction [ 15 ]  . 
in one comparative study [ 1 ] of ct , us and plain abdominal radiography in identifying intestinal occlusion , the reported sensitivity and specificity values were , respectively , 93% and 100% for ct , 83% and 100% for us and 77% and 50% for plainfilm radiography . 
lastly , accuracy in defining the nature of the occlusion was 97% for ct , 23% for us and 7% for abdominal x - ray . from a pathophysiological point of view , intestinal occlusion sets in motion a chain of events with rapid progression , which in the absence of adequate timely treatment leads inevitably to patient death . 
there are a number of associated risk factors that can worsen postoperative mortality , including sepsis , hypercreatininaemia both before and after surgery , and postoperative cardiopulmonary complications , the latter with an incidence of 15% [ 2 , 25 ]  . as our findings suggest , changes identifiable with ct can provide useful information for the prognosis , as the type of intestinal content , diameter of the bowel loops and presence of bowel - wall ischaemia are correlated with advanced - stage disease . 
in contrast , in our experience , tumour t stage , presence or otherwise of locoregional lymphadenopathy and patient age ( 5780 years ) are not postoperative risk factors . the intestinal content in the presence of a large - bowel emergenze coliche chirurgiche [ 1820 ]  . 
nonostante la diffusione della cultura della prevenzione , quindi , il carcinoma del colon - retto viene ancora diagnosticato tardivamente , con la comparsa di unocclusione in una percentuale compresa tra il 7%47% dei casi [ 19 , 2124 ]  . come gi precedentemente sottolineato , la tc ormai divenuta indagine ampiamente utilizzata nel paziente con sospetta occlusione intestinale , poich la pi accurata nel definire presenza , sede e natura dellostacolo alla canalizzazione intestinale [ 15 ]  . 
in uno studio comparativo [ 1 ] tra tc , us ed rx diretto delladdome nel riconoscimento di occlusione intestinale , i valori di sensibilit e specificit riportati sono stati rispettivamente di 93% e 100% per la tc , 83% e 100% per lus , 77% e 50% lrx diretto delladdome . 
 da un punto di vista fisiopatologico , in presenza di unocclusione si determina una serie di eventi , rapidamente evolutivi , che in assenza di un tempestivo adeguato intervento terapeutico portano inesorabilmente allexitus del paziente . anche nei pazienti trattati , comunque , esistono fattori di rischio che aggravano la mortalit post - operatoria , rappresentati da complicanze settiche , ipercreatininemia prima e dopo lintervento , complicanze cardio - polmonari post - operatorie , con unincidenza queste ultime del 14% [ 2 , 25 ]  . come deducibile dai nostri risultati , anche le alterazioni riconoscibili allesame tc possono fornire elementi di valutazione prognostica , poich la tipologia del contenuto intestinale , il diametro delle anse coliche e la presenza di segni di ischemia parietale si correlano allo stadio evolutivo della patologia . 
an exclusively gaseous content was identified in 11% of patients and was due to swallowed air , bacterial fermentation and the breaking down of bicarbonate into carbon dioxide [ 26 ]  . 
it is considered indicative of a recent intestinal occlusion when the ability of the intestinal wall to absorb fluid is preserved . its presence proved to be a favourable prognostic indicator and was associated with survival at 2 months after surgery in 100% of cases . a predominantly fluid content was identified in 11 patients ( 41% ) , and this also proved to be a favourable prognostic indicator , being associated with survival at 2 months after surgery in 73% of cases . 
its presence in patients with carcinoma of the ascending colon is probably due to reduced intestinal absorption surface , whereas in other locations , it is the result of reduced absorptive ability associated with secretions of water and electrolytes in the intestinal lumen . 
fluid accumulation can also occur within the bowel wall itself and , when associated with changes in venous return , this can cause submucosal oedema [ 26 , 27 ]  . 
in this phase , there is less gas in the intestinal lumen , probably because partly it is eliminated upwards , thanks to antiperistalsis and partly because it manages to pass beyond the stenosis . the appearance of abundant fluid and gaseous content , with the formation of airfluid levels , was encountered in 48% of cases , but it does not appear to be a significant prognostic indicator , as it was associated with survival in 46% of cases and death in 65% . 
this finding should nonetheless be considered indicative of a long - standing stenosis , and it is due to excessive bacterial proliferation with progressive distension of the intestinal lumen [ 2729 ]  . pneumatosis intestinalis , the onset of which in an occluded patient is indicative of bowel - wall ischaemia , was found in 33% of cases , was an unfavourable prognostic indicator and was associated with patient death within 2 months after surgery in 78% of cases . 
its location exclusively in the ascending colon is explained by the greater distension of that segment during occlusion , with a consequent obstruction of venous flow [ 3033 ]  . last of all , large - bowel distension proved to be a fundamental prognostic indicator : a diameter of the ascending colon 10 cm was considered highly unfavourable , as it was associated with patient death in 100% of cases . 
the unfavourable prognostic value of marked distension of the large bowel , associated with airfluid levels and pneumatosis intestinalis , can be easily explained in that it is indicative of advanced - stage disease . 
un contenuto esclusivamente gassoso stato riconosciuto nel 11% dei casi ed in rapporto allaria deglutita , alla fermentazione batterica ed alla neutralizzazione del bicarbonato in anidride carbonica [ 26 ]  . 
 un contenuto fluido stato riconosciuto in 11 pazienti ( 41% ) ed risultato anchesso un segno prognostico favorevole , associandosi ad una sopravvivenza a due mesi dallintervento nel 73% dei casi . 
la sua presenza nei pazienti affetti da carcinoma del colon destro da considerare in rapporto alla ridotta superficie di assorbimento intestinale , mentre , nelle altre localizzazioni , in rapporto ad una ridotta capacit di assorbimento parietale , associata a secrezione di acqua ed elettroliti nel lume intestinale . 
laccumulo dei liquidi si pu verificare anche nello spessore parietale ed , in associazione ad alterazioni del ritorno venoso , pu determinare edema sottomucoso [ 26 , 27 ]  . 
in tale fase , probabilmente , il gas gi presente nel lume intestinale meno rappresentato , poich in parte si elimina verso lalto , grazie alla spinta dellantiperistaltismo , in parte riesce a superare la stenosi . 
 la comparsa di abbondante contenuto fluido e gassoso , con formazione di grossolani livelli idroaerei , stata riscontrata nel 48% dei casi , ma non rappresenta un indice prognostico significativo , essendo associato alla sopravvivenza del paziente nel 46% dei casi ed al decesso nel 54% . 
il riscontro di tale alterazione deve , comunque , essere considerato significativo di una stenosi protratta nel tempo ed riferibile ad una eccessiva proliferazione batterica , responsabile di una progressiva distensione del lume intestinale [ 2729 ]  . nella nostra esperienza la pneumatosi parietale , la cui comparsa in un paziente occluso significativa di sofferenza ischemica , stata riconosciuta nel 33% dei casi , ha un significato prognostico sfavorevole ed riconoscibile nel 78% dei pazienti deceduti entro due mesi dallintervento chirurgico . 
 per quanto riguarda infine la distensione colica , essa rappresenta un elemento prognostico fondamentale ed un diametro del colon destro pari o superiore a 10 cm da considerare altamente sfavorevole , essendo stato riscontrato nel 100% dei pazienti deceduti . 
la sovradistensione , infatti , si determina per la 756 radiol med ( 2010 ) 115 : 747757 our study validates the role of ct in the study of intestinal occlusions but does suffer from a number of important limitations : it was a retrospective review of a case series and above all reviewed a small number of patients , which compromises the statistical validity of the results obtained . 
in addition , the patient population consisted of individuals with little anthropometric heterogeneity ( 5780 years ) , such that a reliable evaluation of the possible influence of age on final prognosis could not be made . proliferazione batterica ed causa di un danno ischemico della tonaca mucosa , che facilita una traslocazione batterica transparietale , causa di evoluzione settica sino al decesso del paziente [ 27 , 34 ]  . 
 la nostra ricerca avvalora il ruolo della tc nello studio delle occlusioni intestinali , ma presenta certamente importanti limiti , poich riporta unanalisi retrospettiva della casistica e , soprattutto , considera un esiguo numero di pazienti , che inficia la validit statistica dei risultati ottenuti . 
inoltre , il gruppo considerato comprende soggetti con scarsa disomogeneit antropometrica ( 5780 anni ) , per cui non stato possibile valutare in maniera attendibile leventuale influenza dellet sulla prognosi finale . 
prevalently gaseous or fluid intestinal content is indicative of recent occlusion and is characterised by low postoperative mortality , although this finding needs to be validated by larger case series to achieve statistical significance . 
 in contrast , signs of parietal ischaemia in the large bowel and especially dilatation of the ascending colon 10 cm associated with air - fluid indicative of unfavourable prognosis and were found , respectively , in 78% and 100% of patients who died within 2 months after surgery . levels are conclusioni la tcmd rappresenta una metodica accurata nel riconoscimento di presenza , sede e natura di unocclusione del grosso intestino e pu anche fornire informazioni utili nella valutazione prognostica post - operatoria . 
un contenuto endoluminale gassoso o prevalentemente fluido indice di occlusione recente gravata da bassa mortalit post - operatoria , anche se tale dato , per raggiungere una significativit statistica , deve essere avvalorato su pi ampie casistiche . 
ettorre1 1sezione di scienze radiologiche dipartimento dogira , azienda ospedaliero universitaria policlinico vittorio emanuele , via santa sofia 78 , catania , italy 2unit operativa di gastroenterologia ed endoscopia digestiva azienda ospedaliera santa maria degli angeli , via montereale 24 , pordenone , italy 3endoscopia digestiva azienda ospedaliera policlinico vittorio emanuele , via plebiscito 628 , catania , italy 4cattedra di diagnostica e chirurgia endoscopica , azienda ospedaliero universitaria policlinico g . 
forty - five patients ( 26 men , mean age 57 years ) with extrahepatic biliary dilatation , as shown by transabdominal ultrasound , with or without elevated biliary and pancreatic serum indices , were prospectively studied with mrcp and eus between september 2007 and october 2008 . 
la cprm ha dimostrato accuratezza diagnostica , sensibilit e specificit rispettivamente dell88 , 9% , 91 , 9% e 75% , con valore predittivo positivo del 94 , 4% e valore predittivo negativo del 66 , 7% . 
cprm ed eus non presentano differenze statisticamente significative nellaccuratezza diagnostica . la cprm metodica accurata non invasiva nella patologia biliare extraepatica ; la eus particolarmente attendibile nei pazienti con ostruzione biliare extra - epatica da sludge . parole chiave colangiopancreatografia - rm malattia biliare extraepatica ecografia endoscopica introduction introduzione the last two decades have seen considerable progress in the diagnosis of biliary and pancreatic disease , thanks to the development and consolidation of magnetic resonance cholangiopancreatography ( mrcp ) , an accurate and noninvasive diagnostic modality in biliary imaging [ 15 ]  . 
mrcp is able to provide a complete and reliable anatomical map of the biliary tree without relying on ionising radiation or the use of contrast agents [ 6 ]  . 
 since its inception in 1980 , endoscopic ultrasonography ( eus ) has progressively increased its potential and come to play a remarkable role in diagnosing biliary and pancreatic diseases [ 79 ]  . 
eus is an invasive diagnostic modality that allows characterisation procedures such as fine needle aspiration ( fna )  . the introduction of mrcp and eus into clinical practice stemmed from the need for a diagnostic alternative to endoscopic retrograde cholangiopancreatography ( ercp ) , a technique that , despite allowing for therapeutic procedures , is limited by a risk of potentially life - threatening complications , such as acute pancreatitis , cholangitis , perforation and haemorrhage [ 1012 ]  . 
the incidence of ercp complications ranges from 3% to 5% , and increases to 8%10% when sphincterotomy is performed ; overall mortality rate may exceed 1% [ 12 , 13 ]  . 
the aim of this study was thus to compare the diagnostic accuracy of contrast - enhanced mrcp and eus in identifying the cause of extrahepatic biliary dilatation in patients with or without elevated pancreatic and biliary serum indices . materials and methods the study was conceived through the collaboration of the nelle ultime due decadi si assistito ad un notevole progresso nella diagnosi della patologia biliare e pancreatica , grazie allo sviluppo ed al successivo consolidamento della colangiopancreatografia con risonanza magnetica ( cprm ) , metodica diagnostica accurata e non invasiva nellimaging biliare [ 15 ]  . 
la cprm in grado di fornire una mappa anatomica completa ed affidabile dellalbero biliare , senza dover ricorrere allutilizzo di radiazioni ionizzanti o alla somministrazione di mezzi di contrasto [ 6 ]  . 
 lecoendoscopia ( endoscopic ultrasonography , eus ) , dal momento della sua comparsa , nel 1980 , ha incrementato progressivamente le proprie potenzialit , ed ha assunto un notevole ruolo diagnostico nella diagnosi delle patologie biliari e pancreatiche [ 79 ]  . 
leus una metodica diagnostica dotata di un approccio invasivo , capace allo stesso tempo di effettuare un intervento di caratterizzazione ad esempio la fine needle aspiration ( fna )  . lintroduzione della cprm e delleus nella pratica clinica nasce dalla necessit di ricercare una metodica diagnostica alternativa alla colangiopancreatografia retrograda endoscopica ( cpre ) la cpre , infatti nonostante il vantaggio di poter eseguire un trattamento terapeutico gravata da possibili complicanze quali la pancreatite acuta , le colangiti , le perforazioni e le emorragie , che in alcuni casi possono portare alla morte del paziente [ 1012 ]  . 
le complicanze legate alla cpre variano dal 3% al 5% , ed aumentano sino all8%10% quando viene eseguita una sfinterotomia ; la mortalit complessiva riportata pu superare l1% [ 12 , 13 ]  . 
 in letteratura non vi sono molti studi che hanno confrontato le capacit diagnostiche della cprm e delleus nella medesima casistica [ 12 , 1418 ] ; scopo del nostro lavoro quello di confrontare laccuratezza diagnostica della cprm con mezzo di contrasto ed eus nellidentificare la causa di dilatazione della via biliare extra - epatica , in pazienti con o senza innalzamento degli indici sierologici pancreatici e biliari . 734 radiol med ( 2010 ) 115 : 732746 department of radiology and the gastroenterology division of the department of surgery . 
the majority of patients with abnormal pancreatic and biliary serum indices had raised cholestasis and cell - damage markers ; three patients only had exclusive elevation of cell - damage markers with extrahepatic biliary dilatation . 
nella maggior parte dei pazienti con alterazione di tali valori sierologici pancreatici e biliari , stato riscontrato un incremento sia degli indici di colestasi che degli indici di sofferenza cellulare ; solamente in 3 casi stato riscontrato un incremento esclusivo degli indici di sofferenza cellulare con dilatazione della via biliare extra - epatica . 
sono stati considerati criteri di esclusione : la presenza di controindicazioni alla risonanza magnetica ; la presenza di anastomosi bilio - digestive ; la presenza di pancreatiti acute biliari in cui era indicata una papillosfinteromia endoscopica non rinviabile ; le condizioni generali scadenti , a rischio di vita ; il rifiuto o limpossibilit a firmare il consenso informato . lordine temporale con cui realizzare le indagini ( cprm ed eus ) stato randomizzato secondo criterio semplice , attraverso la generazione di una sequenza di numeri casuali ( numeri pari = prima metodica cprm ; numeri dispari = prima metodica eus )  . 
al fine di ridurre al minimo possibili variazioni legate alla migrazione di calcoli , lecoendoscopia e la cprm sono state eseguite con intervallo di tempo , luna dallaltra , non superiore alle 24 ore . 
 radiol med ( 2010 ) 115 : 732746 the time sequence of imaging investigations ( mrcp and eus ) was determined by simple randomisation , with generation of a sequence of random numbers ( even numbers = mrcp first ; odd numbers = eus first )  . 
 validation of the diagnoses formulated with the two techniques was achieved with ( 1 ) ercp performed within 36 h after the first examination ( eus or mrcp ) ; ( 2 ) surgery with histological examination ( intraoperative or of resected specimen ) ; ( 3 ) clinical and serological follow - up 3 months after ercp in patients who received no treatment . 
indications for ercp were : ( 1 ) diagnosis and treatment of gallstone - related obstruction ( calculus or sludge ) ; ( 2 ) diagnosis and characterisation of a neoplastic biliary stricture ( with cytology of the biliopancreatic juice ) ; ( 3 ) diagnosis and characterisation of a suspicious ampullary mass ; ( 4 ) determination of extrahepatic biliary dilatation aetiology in cases with no apparent cause of stricture or obstruction at cholangiopancreatography and / or eus . 
all studies were done with a 1.5tesla mr scanner ( general electric signa hdx , milwaukee , wi , usa ) using an 8 - channel phased - array coil and breath - hold or respiratory - gated sequences . 
between six and ten sequences were acquired for each examination . these included mrcp sequences to visualise the biliary tree and morphological sequences to evaluate organs containing biliopancreatic structures , such as the liver and the pancreas . 
the 2d ssfse were acquired with thin spin - echo ( frfse ) protocollo di studio cprm gli esami cprm sono stati eseguiti previa firma del modulo di consenso informato . 
tutti gli studi sono stati realizzati con apparecchio di risonanza magnetica ( rm ) da 1 , 5 tesla ( general electric signa hdx , milwaukee , wisconsin , usa )  . i pazienti sono stati esaminati con bobina phased - array ad 8 canali ; le sequenze sono state acquisite in apnea od in modalit triggerata . 
per ogni esame stato acquisito un numero di sequenze compreso tra sei e dieci ; sono state effettuate sequenze colangiopancreatografiche rm per la visualizzazione delle vie biliari e sequenze morfologiche per la valutazione degli organi contenenti le strutture biliopancreatiche , quali fegato e pancreas . 
nel protocollo desame sono state acquisite sequenze : assiali fast spoiled gradient - echo ( fspgr ) t1 in fase e fuori fase ( tempo di eco [ te ] rispettivamente di 2 , 2 e 4 , 4 ms , thickness 6 mm , spacing 1 mm ) ; assiali steady state free precession ( ssfp fiesta ) a sangue bianco , ( tempo di ripetizione [ tr ] 3 , 9 ms , te 1 , 7 ms , thickness 6 mm , spacing 0 , 61 mm ) ; assiali fast spin echo ( fse ) t2 ( tr 2150 ms , te 102 ms , thickness 5 mm , spacing 1 mm ) ; coronali ed assiali single - shot fast spin - echo ( ssfse ) t2 assiali ( thickness 6 mm , spacing 1 mm ) ; assiali fse t2 con soppressione del segnale adiposo , con te fino a 140 ms ( thickness 6 mm , spacing 1 mm )  . per la visualizzazione del sistema biliare e pancreatico , sono state adoperate sequenze colangiopancreatografiche ssfse 2d e fast recovery fast spin - echo ( frfse ) 3d . 
le ssfse 2d sono state acquisite con spessore sottile ( thin multisection ) , con tecnica half fourier single - shot turbo spin - echo ( haste ) ( tr infinito , te 90 ms e spessore di 4 mm ) e con acquisizioni single - shot rapid acquisition with relaxation enhancement ( rare , con slab di 50 mm , tr infinito e te 1100 ms )  . 
le ssfse 2d thick - slab sono state realizzate centrando un loop radiale in corrispondenza della convergenza biliare primaria ed a livello della confluenza bilio - pancreatica ; la prima immagine del loop radiale stata posta lungo il margine posteriore del lobo epatico destro ; le immagini sono state acquisite in apnea espiratoria . lo studio colangiopancreatografico - rm stato completato con sequenze frfse 3d effettuate sia in apnea espiratoria che in modalit triggerata , con spessore rispettivamente di 3 mm e 2 , 2 mm , ( tr 4000 ms , te 722 ms ) ; le acquisizioni 3d sono state effettuate secondo un piano coronale obliquo ( parallelo al decorso della via biliare principale ) [ 6 ] e / o secondo piani assiali , con estensione a coprire il volume epato - pancreatico di interesse ai fini della valutazione dei dotti biliari e pancreatici . 
per evitare la sovrapposizione di liquidi gastrici e duodenali , in 38 dei pazienti esaminati sono stati somministrati per os 100200 ml di un agente superparamagnetico negativizzante il contenuto intestinale ( ferumoxsil - lumirem , guerbet ) ; la somministrazione avvenuta sino ad un massimo di circa 20 minuti prima delle acquisizioni colangiopancreatografiche . 
 736 radiol med ( 2010 ) 115 : 732746 multisection half - fourier single - shot turbo spin echo ( haste ) with tr infinite , te 90 ms and thickness 4 mm ; and single - shot rapid acquisition with relaxation enhancement ( rare ) with slab 50 mm , tr infinite and te 1100 ms . 
the first image in the radial loop was placed along the posterior margin of the right liver lobe , and the images were acquired during expiratory breath - holding . mrcp was completed with breath - hold or respiratorygated 3d frfse , with slice thickness of 3 mm and 2.2 mm , respectively ( tr 4000 ms , te 722 ms )  . 
the 3d scans were acquired in a coronal oblique plane [ 6 ] ( parallel to the course of the main bile duct ) and / or in the axial plane , with coverage of the hepatopancreatic region of interest in order to permit evaluation of the biliary and pancreatic ducts . 
to avoid superimposition of gastric and duodenal fluid , 38 patients received 100200 ml of oral superparamagnetic medium to suppress interference from intestinal contents ( ferumoxsil , lumirem , guerbet )  . 
 thin - slice 2d ssfse and 3d frfse sequences were postprocessed with multiplanar reconstruction ( mpr ) and maximum intensity projection ( mip ) using dedicated software ( advantage workstation , general electric )  . 
where necessary , examinations were completed with t1 3d fspgr sequences obtained before and after intravenous administration of gadolinium dimeglumine ( gd - bopta ) ( 0.1 mmol / kg , multihance 0.5 m , bracco imaging spa , milan , italy ) ; the 3d fspgr sequences were acquired with fat saturation ( tr 4.2 ms , te 2.0 ms , thickness 3 mm )  . after gadolinium administration , the examination was performed with dynamic multiphase technique , with acquisitions at 20 , 70 and 180 s . 
to improve transmission of ultrasound waves , a water - filled balloon was attached to the tip of the us transducer , and degassed water was instilled into the lumen of the duodenum and stomach . us scans to evaluate the pancreas and biliary tree were performed by placing the transducer initially in the second le sequenze colangiopancreatografiche 2d ssfse a strato sottile e 3d frfse sono state rielaborate con tecnica delle ricostruzioni multi - planari ( mrp ) e delle proiezioni di massima intensit ( mip ) , mediante limpiego di software dedicato ( advantage workstation , general electric )  . 
nei casi in cui ritenuto necessario , gli esami sono stati completati con sequenze fspgr t1 3d , ottenute prima e durante la somministrazione endovenosa di gadopentato dimeglumina ( gd - bopta ) ( 0 , 1 mmol / kg , multihance 0 , 5 m , bracco imaging spa , milano , italia ) ; le sequenze fspgr 3d sono state effettuate con soppressione del segnale adiposo ( tr 4 , 2 ms , te 2 , 0 ms , thickness 3 mm )  . 
tutte le procedure sono state realizzate in sedazione cosciente ( midazolam 510 mg , ev ) , con posizionamento del paziente in decubito laterale sinistro , previa acquisizione del consenso informato . 
per migliorare la trasmissione delle onde ultrasonografiche stato utilizzato il metodo del riempimento del palloncino , montato su sonda ecografica posizionata nel terminale distale dello strumento , e dellinstillazione di acqua degassificata nel lume del duodeno e dello stomaco . le scansioni ecografiche per la valutazione del pancreas e della via biliare sono state acquisite posizionando inizialmente lo strumento nel ii duodeno ed utilizzando come punto di repere endoscopico la papilla e come punto di riferimento ecografico laorta e la cava . 
lo strumento stato gradualmente ritirato fino al piloro , dopo aver valutato ecograficamente la regione del processo uncinato , la testa del pancreas , la porzione cefalica del wirsung , la porta e lilo epatico . 
in tutti i pazienti , dellalbero biliare extraepatico stata effettuata una valutazione sistematica del coledoco , del dotto cistico e del dotto epatico comune , ai fini del confronto con cprm . 
a completamento della procedura , stata condotta , attraverso lo stomaco , una valutazione ecografica del corpo , dellistmo e della coda del pancreas , del wirsung ( tratto corpo - coda ) , della piccola ala del fegato e del tripode celiaco . 
la via biliare extra - epatica con diametro superiore a 7 mm stata ritenuta ectasica ; nel caso di pregressa colecistectomia , stata considerata aumentata di calibro una via biliare extra - epatica con diametro maggiore di 10 mm . radiol med ( 2010 ) 115 : 732746 portion of the duodenum and using the papilla as an endoscopic landmark and the aorta and vena cava as sonographic landmarks . 
the transducer was then gradually withdrawn to the pylorus after evaluating the region of the uncinate process , the pancreatic head , the cephalic segment of wirsungs duct , the portal vein and the hepatic hiluin all patients , the entire extrahepatic biliary system , including the common bile duct , cystic duct and common hepatic duct , was evaluated systematically to allow comparison with mrcp . 
at the end of the procedure , a sonographic assessment was obtained through the stomach of the isthmus and tail of the pancreas , the wirsung duct ( headtail ) , the left liver lobe and the coeliac trunk . 
evaluation of stone - related biliary obstruction was based on preliminarily defined diagnostic criteria for the presence of endoluminal gallstones or sludge . with regard to gallstones , the finding of one or more rounded or oval areas of hypointensity within a hyperintense biliary lumen was considered diagnostic for the presence of one or more biliary stones at mrcp . 
the finding , instead , of one or more hypoechoic areas with posterior shadowing inside a bile duct was considered a valid criterion for one or more stones at eus . 
with regard to sludge , the mrcp diagnosis was established in the presence of slightly hypointense particulate material with a diameter < 2 mm , whereas the eus diagnosis was based on visualisation of small echoic areas without posterior shadowing , or the presence of echoic material arranged in layers within the main bile duct [ 14 ]  . a dilatated choledochus with abrupt narrowing in correspondence with an area of irregular enhancement after contrast - medium administration and with infiltrative pattern and predominantly hypointense signal due to hypovascularity and desmoplastic reaction located within the extrahepatic bile duct and / or pancreatic parenchyma , was considered diagnostic for biliary or pancreatic neoplastic stricture on mrcp . 
likewise , abrupt narrowing of the choledochus in correspondence with a focal hypoechoic change with infiltrative pattern and ill - defined margins located along the extrahepatic bile duct and / or in the pancreatic parenchyma was considered diagnostic for biliary or pancreatic neoplasm on eus . an enlarged papilla with irregular enhancement after contrast medium administration was considered suggestive of an ampullary mass on mrcp ; similarly , an enlarged nella valutazione della patologia ostruttiva litiasica della via biliare , sono stati stabiliti preventivamente i criteri diagnostici per indicare la presenza di eventuali calcoli o di sludge endoluminale . 
nelle acquisizioni colangiopancreatografiche , la presenza di una o pi immagini rotondeggianti , ovalari e con bassa intensit di segnale , nel contesto delliperintensit del lume biliare , stata diagnostica per la presenza rispettivamente di una o pi formazioni calcolotiche . 
nella diagnosi di sospetta ostruzione litiasica in eus , la visualizzazione di una o pi immagini ecografiche iperecogene con cono dombra posteriore allinterno della via biliare stata considerata criterio valido per la diagnosi rispettivamente di uno o pi calcoli . 
la diagnosi di sludge biliare stata posta nelle acquisizioni cprm in presenza di materiale particolato debolmente ipointenso con diametro inferiore ai 2 mm ; in eus stato considerato positivo per sludge la visualizzazione di piccole immagini ecogene , senza cono dombra acustico , o la presenza di materiale ecogeno disposto in maniera stratificata nella via biliare principale [ 14 ]  . la presenza di un coledoco ectasico , con brusco restringimento del calibro in corrispondenza di unarea di irregolare enhancement dopo somministrazione di gadolinio ev con caratteristiche infiltrative e segnale prevalentemente ipointenso in relazione al carattere ipovascolare ed alla reazione desmoplastica centrata nella via biliare extraepatica e / o nel parenchima pancreatico , sono stati adoperati come criteri cprm per la diagnosi di stenosi neoplastica biliare o pancreatica . 
in maniera analoga in eus , un brusco restringimento del coledoco in corrispondenza di unalterazione focale ipoecogena a caratteristiche infiltrative e margini sfumati , localizzata lungo la via biliare extraepatica e / o a livello del parenchima pancreatico , sono stati considerati criteri validi per formulare lipotesi diagnostica di lesione eteroformativa neoplastica della via biliare o del pancreas . una papilla di volume aumentato rispetto alla norma e con irregolare impregnazione dopo somministrazione di gadolinio , stata considerata suggestiva in cprm per la presenza di una formazione espansiva ampollare ; allo stesso modo in eus il riscontro di una papilla aumentata di dimensione , con caratteristiche espansive , morfologia irregolare e perdita dei rapporti con la tonaca muscolaris del duodeno , sono stati interpretati come criteri validi per la diagnosi di processo espansivo ampollare . 
lirregolare dilatazione del dotto pancreatico principale con aspetto a corona di rosario la riduzione dello spessore del parenchima pancreatico , il riscontro di aree calcifiche e di raccolte fluide intrapancreatiche , sono stati i criteri pi frequentemente impiegati per la diagnosi di pancreatite cronica , sia negli studi di cprm che di eus . 
la protrusione intraduodenale del tratto distale della via biliare , sottoforma di struttura a contenuto fluido localizzata medialmente rispetto alla testa del pancreas ed in continuit con il coledoco , stata considerata diagnostica per la presenza di coledococele . 
il riscontro di formazioni a contenuto fluido o con livelli idro - aerei nel contesto , localizzate in sede adiacente alla via biliare principale , in comunicazione con il lume duodenale , stato considerato criterio 738 radiol med ( 2010 ) 115 : 732746 papilla with expansile appearance , irregular morphology and loss of relations with the duodenal tunica muscularis was interpreted as a sign of expansile ampullary mass on eus . 
irregular dilatation of the main pancreatic duct with string - of - beads appearance , reduced thickness of the pancreatic parenchyma , areas of calcification and fluid collections within the pancreas were the most frequent criteria used for diagnosing chronic pancreatitis on both mrcp and eus . 
intraduodenal protrusion of the distal biliary tree in the form of a fluid - containing structure located medial to the pancreatic head and continuous to the choledochus was considered diagnostic for the presence of choledochocele . 
the possible presence of cystic formations of the biliary system was diagnosed in accordance with the modified todani classification . statistical analysis sensitivity , specificity , diagnostic accuracy , and positive ( ppv ) and negative ( npv ) predictive value in the identification of biliopancreatic disease were calculated for both mrcp and eus . 
leventuale presenza di malformazioni cistiche delle vie biliari stata diagnosticata in accordo alla classificazione modificata di todani . analisi statistica sia per cprm che per eus , sono stati calcolati i valori di sensibilit , specificit , accuratezza diagnostica , valore predittivo positivo e negativo , nella capacit di identificare la patologia bilio - pancreatica . 
sensibilit , specificit , accuratezza diagnostica , valore predittivo positivo ( vpp ) e negativo ( vpn ) sono stati calcolati anche in relazione alla capacit di identificare la presenza di litiasi . 
in 6 casi non stata identificata alcuna patologia . cprm la cprm con mezzo di contrasto ha dimostrato unaccuratezza diagnostica pari all88 , 9% , con sensibilit e specificit rispettivamente del 91 , 9% ( 95% ci = 0 , 8311 , 007 ) e del 75% ( 95% ci = 0 , 4501 , 050 ) ( tabella 2 )  . 
accuratezza diagnostica , sensibilit , specificit , vpp e vpn sono stati nella diagnosi di ostruzione litiasica rispettivamente del 95 , 6% , dell89 , 5% , del 100% , del 100% e del 92 , 7% . la cprm ha riportato 3 falsi negativi , in 2 dei quali stata identificata come causa della dilatazione della via biliare principale la presenza di sludge biliare . 
nellaltro falso positivo , la presenza di una papilla aumentata di dimensioni , in un paziente con dilatazione cistica del coledoco , stata considerata positiva per patologia espansiva neoplastica ampollare ; la cpre radiol med ( 2010 ) 115 : 732746 fig . 
a image shows dilatation of the main bile duct ( thin white arrow ) and wirsung duct ( white arrowheads ) caused by an expansile process of the pancreatic head ( thin white arrow in b )  . 
3a - c cprm ( a ) , immagine rm assiale t1 dopo gadolinio ( b ) ed eus ( c ) in un paziente con ittero e dilatazione biliare extraepatica . 
in a sono rappresentate la dilatazione della via biliare principale ( freccia bianca sottile ) e del wirsung ( teste di freccia bianca ) , causate da una formazione espansiva della porzione cefalica del pancreas ( freccia bianca sottile in b ) ; riconoscibile anche la sovradistensione della colecisti ( asterisco bianco in b )  . 
mrcp succeeded in identifying only two out of four cases of biliary sludge . the 15 cases of stone - related obstruction of the main bile eseguita successivamente in tale paziente non ha riscontrato cellule neoplastiche alle indagini bioptiche ; laspetto ipertrofico della papilla stato ricondotto ad unalterazione cronica iperplastica su base infiammatoria . radiol med ( 2010 ) 115 : 732746 fig . 
4a - e mr cholangiopancreatography ( a ) , axial t1 mr images postgadolinium ( b , d ) and eus images ( c , e ) in a patient with ampullary neoplas a image shows dilatation of the extrahepatic bile duct ( empty white arrow ) and wirsung duct ( white arrowheads ) , with large choledochowirsungocele ( thin white arrow )  . 
b the choledocho - wirsungocele is shown in the axial plane , with the main bile duct and the wirsung duct ( white arrow and black arrow , respectively )  . 
4a - e cprm ( a ) , immagini rm assiali t1 dopo gadolinio ( b , d ) ed immagini ecoendoscopiche ( c , e ) in un paziente con neoplasia dellampolla . in a mostrata la dilatazione del dotto biliare extra - epatico ( freccia bianca vuota ) e del wirsung ( teste di freccia bianca ) , con ampio coledoco - wirsungocele ( freccia bianca sottile )  . 
in b mostrato il coledoco - wirsungocele nel piano assiale , con la via biliare principale ed il wirsung ( rispettivamente freccia bianca e freccia nera ) ; unimmagine simile riconoscibile nellimmagine endoscopica di c ( frecce bianche )  . 
d mostra lenhancement della papilla major ( frecce bianche sottili ) ; riconoscibile anche il duodeno ( testa di freccia bianca ) ; nellimmagine ecoendoscopica ( e ) si osserva spessore aumentato della papilla , che aggetta nel lume duodenale ( freccia bianca sottile )  . 
in the other false positive case , papillary enlargement in a patient with cystic choledochal dilatation was considered to indicate an expansile ampullary neoplassubsequent ercp with biopsy failed to identify neoplastic cells . 
hypertrophic appearance of the papilla was explained by a chronic hyperplastic change due to inflammation . eus results ( 95% ci = 0.9211.025 ) eus had slightly higher diagnostic accuracy than mrcp , with a value of 93.3%. 
the false negative was due to failure to identify a case of small juxtapapillary diverticulu one false positive was related to an enlarged papilla ( as occurred with mrcp ) that was interpreted as having neoplastic appearance . 
the second false positive related to a case diagnosed as pancreatic tumour ( as occurred with mrcp ) , where histopathological analysis revealed an inflammatory infiltrate of lymphocytes and plasma cells associated with glandular fibrosis , leading to a diagnosis of chronic focal pancreatitis due to autoimmune abnormality . it is noteworthy that the presence of stones or sludge in the extrahepatic bile ducts was correctly identified by eus in all 19 cases observed . 
endoluminal sludge with dilatation of the extrahepatic bile ducts was correctly identified in all four cases observed , whereas mrcp identified only two cases of dilatation due to endoluminal sludge . 
 discussion in gastroenterological clinical practice , us , computed tomography and mrcp have become widely available [ 19 ] , whereas eus is only present in a limited number of specialised centres despite its validated excellent diagnostic capabilities [ 15 ]  . 
this different availability may be lecoendoscopia ha evidenziato unaccuratezza diagnostica lievemente superiore rispetto alla cprm , con valore pari al 93 , 3% ; la sensibilit e la specificit riportate dalla metodica ecoendoscopica sono state rispettivamente del 97 , 3% ( 95% ci = 0 , 9211 , 025 ) e del 75% ( 95% ci = 0 , 4501 , 050 ) ( tabella 2 )  . 
il valore predittivo positivo stato del 94 , 7% , mentre il valore predittivo negativo del 85 , 7% ( tabella 2 )  . lecoendoscopia ha riportato un falso negativo : in un caso non stato identificato un piccolo diverticolo paravateriano . 
due i falsi positivi riscontrati con eus ; il primo caso legato ( analogamente a quanto osservato per la cprm ) alla presenza di una papilla aumentata di volume , interpretata come di aspetto neoplastico : le biopsie condotte successivamente durante cpre hanno identificato cellule infiammatorie e non neoplastiche ; il secondo caso , analogamente a quanto verificatosi per cprm , stato diagnosticato come tumore pancreatico , ma lesame istopatologico ha identificato un infiltrato infiammatorio di linfociti e plasmacellule associato a fibrosi della ghiandola , ed ha pertanto posto diagnosi di pancreatite cronica focale su base immunitaria . interessante sottolineare che la calcolosi della via biliare extraepatica o la presenza di sludge endoluminale sono state correttamente identificate dalla metodica ecoendoscopica nei 19 casi osservati . 
la presenza di sludge endoluminale con dilatazione della via biliare extraepatica stata correttamente identificata dalleus nei 4 casi osservati , mentre con cprm sono stati rilevati solo 2 casi di dilatazione da sludge endoluminale . 
 discussione nella pratica clinica gastro - enterologica lecografia ( us ) , la tomografia computerizzata ( tc ) e la cprm hanno avuto una larga diffusione [ 19 ] , mentre leus disponibile solo in alcuni centri specialistici , nonostante le elevate e verificate capacit diagnostiche [ 15 ]  . 
la differente diffusione nella pratica clinica pu essere ricondotta a diversi fattori : lecoendoscopia infatti una metodica diagnostica invasiva , fortemente operatore - dipendente , che necessita di sedazione per essere eseguita [ 15 , 16 ]  . 
sicuramente un vantaggio dellecoendoscopia rispetto alla cprm la possibilit di eseguire la cpre nella stessa seduta o immediatamente dopo , con il paziente sdraiato nel lettino , ancora sotto anestesia [ 15 ]  . 
leus possiede un campo di visualizzazione pi limitato , in quanto manca della profondit di esplorazione necessaria per lo studio della regione biliare intra - epatica ed ilare [ 16 ] ; un valore aggiunto della eus rappresentato dalla possibilit di effettuare un prelievo per la caratterizzazione di una sospetta lesione neoplastica mediante fine needle aspiration ( fna ) [ 20 ]  . radiol med ( 2010 ) 115 : 732746 explained by several factors : eus is an invasive , heavily operator - dependent modality that requires patient sedation [ 15 , 16 ]  . 
no doubt one advantage of eus over mrcp is the possibility of performing ercp during the same session or immediately after , with the patient lying on the bed and still under sedation [ 15 ]  . 
an added value of eus is the possibility of performing fine - needle aspiration to characterise a suspicious neoplastic lesion [ 20 ]  . the greater availability of mrcp is related to the techniques reliability and lack of invasiveness [ 1 , 3 , 4 ]  . 
sensitivity , specificity and diagnostic accuracy were , respectively , 91% , 94% and 92% for mrcp and 97% , 88% and 94% for eus . no significant difference in sensitivity and specificity was observed between the two methods . 
the two false positive results at eus one case of choledochal sludge and one of a 3 - mm choledochal stone were not detected at ercp performed 3 days later . 
iterated the importance of not leaving too wide an interval between the two modalities ( mrcp or eus ) and the final diagnostic technique ( ercp ) , so as to avoid the risk of migration in cases of choledocholithiasis or sludge . 
in addition , they showed how the presence of sludge was the main cause of false positive and false negative results [ 14 ]  . in our study , the greater diagnostic capability of eus compared with mrcp in identifying sludge was supported by the relatively short interval between examinations , with ercp being performed within 36 h of the first modality . on the other hand , mrcp and eus were always performed within 24 h of each other to avoid errors due to spontaneous passage of stones through the papilla and influencing the sensitivity of either modality . 
 [ 17 ] studied 30 patients with a clinical suspicion of extrahepatic biliary disease : ercp , performed as the gold la maggiore diffusione della cprm legata allaffidabilit della metodica ed allassenza di invasivit [ 1 , 3 , 4 ] ; lesame non richiede alcuna sedazione ed pi tollerato dai pazienti . 
i valori di sensibilit , specificit ed accuratezza diagnostica per la cprm sono stati rispettivamente del 91% , 94% e 92% , mentre i corrispondenti valori per leus sono stati del 97% , 88% e 94% ; non stata riscontrata alcuna differenza statisticamente significativa tra i valori riportati per le due metodiche [ 14 ]  . 
nei falsi negativi in tale studio ( 2 casi cprm ed 1 caso cprm ed eus ) , il riscontro diagnostico finale con cpre stato di sludge biliare ; la cpre in tal caso stata eseguita lo stesso giorno della cprm e della eus . 
nello stesso studio stato considerato falso positivo in cprm un coledoco dilatato con sludge nel contesto , non confermato dalla cpre eseguita il giorno dopo la cprm [ 14 ]  . 
i due falsi positivi riscontrati alla eus un coledoco positivo per sludge ed un coledoco con calcolo di 3 mm non sono stati riscontrati alla cpre eseguita 3 giorni dopo [ 14 ]  . 
 [ 14 ] emerge limportanza di un intervallo di tempo temporale fra le due metodiche ( cprm o eus ) e la diagnosi finale ( cpre ) non eccessivamente ampio , in modo da evitare nei casi di coledocolitiasi o sludge il rischio di possibile migrazione ; si evince inoltre come la presenza di sludge sia stata la principale causa di falsi positivi e di falsi negativi [ 14 ]  . nel nostro studio la maggiore capacit diagnostica delleus rispetto alla cprm nellidentificazione dello sludge avvalorata dallutilizzo di un intervallo di tempo piuttosto ristretto , in quanto la cpre stata eseguita in un intervallo di tempo mai superiore alle 36 ore rispetto allesecuzione della prima metodica . 
cprm ed eus del resto non sono state mai eseguite con intervallo di tempo superiore alle 24 ore , in modo da evitare errori legati al passaggio spontaneo dei calcoli attraverso la papilla ed influenzare diversamente la sensibilit delluna o dellaltra metodica . 
 la presenza di calcoli di piccola dimensione , oltre allidentificazione dello sludge endoluminale , restano secondo diversi studi i fattori pi importanti in grado di discriminare la sensibilit delle due metodiche . 
 [ 17 ] sono stati studiati 30 pazienti con sospetto clinico di malattia biliare extra - epatica : la cpre , eseguita come gold standard dopo eus e cprm , ha evidenziato coledocolitiasi in 5 pazienti , stenosi biliare in 3 , vie biliari di calibro regolare in 20 [ 17 ]  . 
in tale studio la media dimensionale del calcolo stata piuttosto bassa ( 4 mm ) e ben tre dei 4 falsi negativi riscontrati con la cprm sono stati determinati dalla presenza di calcoli di piccola dimensione . 
anche nello 744 radiol med ( 2010 ) 115 : 732746 standard after eus and mrcp , showed choledocholithiasis in five patients , biliary stricture in three and normal biliary tree in 20 . 
in this study , the mean stone size was relatively small 4 mm and no less than three of the four false negative results at mrcp were caused by small stones . also in the study by kondo et al . 
 [ 18 ] false negative results at mrcp were related to stones < 5 m stone size is not , however , always a discriminant factor between mrcp and eus . 
 [ 16 ] found no significant difference in the ability of the two modalities to detect small stones : mrcp succeeded in identifying 4 / 6 stones with diameter 5 mm , whereas eus diagnosed 5 / 6 . 
in addition , stones may be obscured by the hyperintensity of bile on mip images and by the thickness of coronal sequences acquired with a single - shot imaging technique [ 1 , 15 ]  . the use of different cholangiopancreatographic sequences thin - section 2d ssfse , slab - thickness 2d ssfse , native and mip 3d frfse and imaging planes ( axial and coronal ) in our study protocol increases the ability to detect small stones . 
despite the different cholangiopancreatographic acquisition techniques , mrcp is not always able to depict biliary sludge as a fluidfluid level of different signal intensity or as hypointense particulate material with diameter < 2 mm . with regard to identifying neoplastic disease , all tumours were correctly evaluated by eus , whereas mrcp misdiagnosed an ampullary neuroendocrine tumour . 
it is possible that the neuroendocrine ampullary tumour was misdiagnosed because of its association with a gross choledochocelewirsungocele : the periampullary enhancement typical of ampullary expansile lesions , especially in delayed acquisitions , was erroneously interpreted as a sign of concurrent inflammatory reaction . 
cprm stata in grado di identificare 4 dei 6 calcoli con diametro 5 mm , mentre leus ha diagnosticato 5 calcoli su 6 con diametro 5 mm [ 16 ]  . 
 nel nostro studio sono stati correttamente identificati con cprm i calcoli con diametro uguale o inferiore a 4 mm ( ben 2 calcoli di 3 mm e 3 calcoli di 4 mm ) ; lelevata capacit diagnostica della cprm nellidentificazione dei calcoli di piccola dimensione riconducibile alla tecnica colangiopancreatografica utilizzata nellacquisizione delle immagini [ 1 , 15 ] : i calcoli di piccola dimensione sono meglio evidenziati nelle immagini native assiali , in quanto in tale maniera sono perpendicolari rispetto allasse del coledoco ; inoltre essi possono essere oscurati dalla iperintensit della bile nelle immagini mip e dallo spessore delle sequenze coronali single - shot acquisite [ 1 , 15 ]  . limpiego di diverse sequenze colangiopancreatografiche nel nostro protocollo di studio ssfse 2d thin section , ssfse 2d slab - thickness , frfse 3d native e mip in diversi piani ( assiali e coronali ) aumenta la capacit di identificazione dei piccoli calcoli . 
in particolare maggiore contributo diagnostico nel sospetto di calcoli di piccola dimensione stato ricavato dallimpiego delle sequenze ssfse 2d a strato sottile e dalla visualizzazione delle immagini native delle frfse 3d , questultime acquisite con spessore compreso tra 2 , 2 e 3 mm . il limite diagnostico della cprm nel nostro studio legato pertanto non allidentificazione dei calcoli di piccola dimensione , piuttosto alla visualizzazione dello sludge biliare , quel particolato endoluminale di 12 mm di diametro che leus identifica come un livello fluido endoluminale , di aspetto debolmente ecogeno . 
malgrado le diverse tecniche di acquisizione colangiopancreatografica , non sempre la cprm riesce ad apprezzare lo sludge biliare come un livello fluido - fluido di differente intensit di segnale o come un materiale particolato ipointenso di calibro inferiore ai 2 mm . per quanto riguarda lidentificazione della patologia neoplastica , nel nostro studio nessun tumore stato considerato come falso negativo dalleus , mentre con cprm stato misconosciuto un tumore neuroendocrino ampollare . sappiamo che la risonanza magnetica possiede elevata accuratezza nellidentificazione del carcinoma ampollare [ 21 ]  . 
possibile che il tumore neuroendocrino ampollare sia stato misconosciuto in quanto associato ad un vistoso coledoco - wirsungocele : lenhancement periampollare , tipico delle formazioni espansive ampollari , soprattutto nelle acquisizioni tardive dopo mezzo di contrasto ( mdc ) , stato erroneamente interpretato come espressione di unalterazione infiammatoria reattiva concomitante . 
 [ 12 ] radiol med ( 2010 ) 115 : 732746 [ 12 ] reported on the findings of a study comparing the diagnostic value of eus and mrcp in a much larger patient series ( 153 patients )  . 
in their study , patients were divided into two groups , the first comprising patients with biliary dilatation unexplained by sonography , and the second comprising patients with a strong suspicion of choledocholithiasis without biliary dilatation [ 12 ]  . 
the patient population considered in our study is partially representative of individuals with extrahepatic biliary disease in that no one with normal extrahepatic biliary tree and raised cholestasis markers was included . 
our future goal is to evaluate the accuracy of the two modalities in a larger patient series , possibly grouped according to defined categories of biliopancreatic disease ( presence of extrahepatic biliary dilatation or normal ducts with elevation of cholestasis markers )  . hanno riportato i dati di uno studio condotto per raffrontare il valore diagnostico delleus e della cprm in una casistica di pazienti ben pi ampia ( 153 pazienti ) rispetto alla nostra ; in tale studio i pazienti sono stati suddivisi in due gruppi : nel primo sono stati inclusi soggetti con dilatazione della via biliare senza una precisa causa rilevata allecografia e nel secondo soggetti con forte sospetto di coledocolitiasi , senza dilatazione della via biliare [ 12 ]  . 
la popolazione oggetto del nostro studio parzialmente rappresentativa dei soggetti con malattia della via biliare extra - epatica : non sono stati inclusi infatti soggetti con regolare calibro della via biliare extraepatica e rialzo degli indici di colestasi . 
il nostro obbiettivo futuro rimane quello di poter valutare laccuratezza delle due metodiche in un numero pi ampio di pazienti , eventualmente suddivisi in pi gruppi , secondo diversi criteri di definizione di malattia bilio - pancreatica ( presenza di dilatazione della via biliare extraepatica o calibro regolare con rialzo degli indici di colestasi )  . conclusions conclusioni in patients with sonographically detected extrahepatic biliary dilatation , both mrcp and eus proved to be valuable methods for establishing the cause of the dilatation . our findings show that both modalities have high diagnostic accuracy . 
in consideration of the essentially equivalent performance of the two modalities , mrcp is to be preferred as a first choice after transabdominal ultrasonography owing to its noninvasiveness and panoramic capabilities . 
eus proved to be particularly reliable in patients with lithiasis , as it also enabled recognition of biliary sludge . nei pazienti con dilatazione della via biliare extraepatica , accertata mediante us , sia la cprm che leus sono risultate metodiche valide per la definizione della causa eziologica . 
a fronte di risultati pressappoco equivalenti tra le due metodiche , la cprm , in relazione alla bassa invasivit ed alla panoramicit , rimane la scelta da realizzare in prima istanza dopo lecografia trans - addominale . 
cademartiri1 , 2 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria , parma , italy 2radiology and cardiology department , erasmus medical centre , rotterdam , the netherlands 3dipartimento di radiologia , universit degli studi di napoli federico ii , napoli , italy 4dipartimento di radiologia , sdn fondazione irccs , napoli , italy 5dipartimento di radiologia , universit di verona , verona , italy correspondence to : f . 
cademartiri , dipartimento di radiologia e diagnostica per immagini , c / o piastra tecnica piano 0 , azienda ospedaliero - universitaria , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 0521 - 703516 , fax : + 39 - 0521 - 704838 , e - mail : filippocademartiri@hotmail.com received : 24 april 2009 / accepted : 7 july 2009 / published online : 22 february 2010 springer - verlag 2010 abstract purpose . 
for mri , we used two - dimensional cine balanced steady - state free precession ( b - ssfp ) sequences , and for ct we used multiphase short - axis reconstructions . 
per la cardio - rm abbiamo utilizzato sequenze 2d cine b - steady - state free - precession ( ssfp ) e per la tc abbiamo utilizzato delle ricostruzioni multifasiche in asse corto . 
gli esami cardio - rm e cardio - tc mostrano radiol med ( 2010 ) 115 : 702713 keywords cardiac magnetic resonance cardiac computed tomography left ventricular volumes quantitative software ejection fraction una eccellente concordanza per la valutazione dei parametri funzionali del vsin e possono quindi essere utilizzati indifferentemente nella pratica clinica . parole chiave risonanza magnetica cardiaca tomografia computerizzata cardiaca volumi del ventricolo sinistro software quantitativo frazione di eiezione introduction introduzione accurate and reproducible assessment of left ventricular ( lv ) function parameters , and in particular of ejection fraction ( ef ) , is fundamental in diagnostic , therapeutic and prognostic classification of patients with cardiac disease [ 16 ]  . 
by offering a high temporal , spatial and contrast resolution in a single technique , magnetic resonance imaging ( mri ) completely fulfils the requirements of a gold standard in assessing lv volumes [ 7 , 8 ]  . 
in recent years , the possibility of obtaining a noninvasive evaluation of the coronary tree and heart in general with computed tomography ( ct ) has led numerous researchers to investigate the ability of ct to assess lv function parameters in comparison with mri [ 918 ]  . these studies have , however , been conducted on small patient populations , and mr and ct images were analysed with different software applications . 
we report on our routine clinical experience in 181 patients in whom lv function and mass were studied with both mri and ct and analysed using the same quantitative software . materials and methods patients between april 2007 and april 2009 , we enrolled 181 patients ( mean age 5517 years ; 111 men and 70 women ) ( table 1 ) who underwent coronary angiography with multislice ct to rule out the presence of coronary disease . 
in particular , patients were excluded from the ct study if they had a heart rate ( hr ) > 65 beats per minute ( bpm ) unresponsive to beta blockers , atrial fibrillation and high ventricular response , known allergy to contrast media , kidney failure and / or una valutazione corretta e riproducibile dei parametri funzionali del ventricolo sinistro ( vsin ) , ed in particolare della frazione di eiezione ( fe ) , rappresenta un momento fondamentale nellinquadramento diagnostico , terapeutico e prognostico del paziente con patologie cardiache [ 16 ]  . 
grazie alla possibilit di ottenere con una sola tecnica una elevata risoluzione temporale , spaziale e di contrasto , la risonanza magnetica ( rm ) soddisfa a pieno i requisiti di gold standard per la valutazione dei volumi del vsin [ 7 , 8 ]  . recentemente , grazie alla possibilit di ottenere una valutazione non invasiva dellalbero arterioso coronarico , e del cuore in genere , molteplici studi sono stati condotti per valutare leffettiva capacit della metodica di tomografia computerizzata ( tc ) nel fornire , al pari della rm , anche i parametri funzionali del vsin [ 918 ] ; tuttavia tali studi sono stati condotti su casistiche limitate ed inoltre le immagini rm e tc sono state sempre analizzate utilizzando software differenti per le due metodiche . 
out of 200 patients enrolled prospectively , ten were excluded a priori , as they met the exclusion criteria for cardiac ct , whereas nine were eligible for ct but not for mri due to claustrophobia . 
the study was approved by the local ethics committee , and written informed consent was obtained from all patients . ct scan protocol on the patients arrival , blood pressure and hr were monitored . 
in particular , patients with hr > 65 bpm received an intravenous beta blocker ( atenolol ) to lower the hr to < 65 bp all scans were performed with retrospective electrocardiographic ( ecg ) gating on a radiol med ( 2010 ) 115 : 702713 sono stati rispettati i criteri di esclusione pi volte riportati in letteratura per i pazienti non adatti ad un esame tc e / o rm [ 1921 ] ; in particolare , per lo studio tc sono stati esclusi i pazienti con frequenza > 65 battiti per minuto ( bpm ) non responsivi ai farmaci beta - bloccanti , i pazienti con fibrillazione atriale ad elevata risposta ventricolare , quelli con nota allergia ai mezzi di contrasto , con insufficienza renale e / o con compromissione della funzionalit respiratoria ; per lo studio rm sono stati esclusi i pazienti con claustrofobia , quelli portatori di pace - maker e / o di qualunque altro dispositivo non compatibile con lambiente rm [ 20 ]  . 
su un totale di 200 pazienti arruolati prospetticamente , 10 pazienti sono stati esclusi a priori in quanto rientravano nei criteri di esclusione per lesame cardio - tc , mentre in 9 pazienti siamo stati in grado di portare a termine lesame tc , ma non siamo riusciti a portare a termine lacquisizione rm per claustrofobia . 
lo studio stato approvato dal comitato etico locale e tutti i pazienti hanno fornito per iscritto il loro consenso informato . protocollo di scansione tc allarrivo di ogni paziente stata monitorata la pressione arteriosa e la frequenza cardiaca ( fc ) ; in particolare i pazienti con fc > 65 bpm sono stati beta - bloccati con somministrazione di atenololo endovena ( ev ) fino al raggiungimento di una fc < 65 bptutte le acquisizioni , sincronizzate retrospettivamente con traccia elettrocardiografica ( ecg ) , sono state effettuate con una apparecchiatura tc 64 strati ( sensation 64 , siemens , forchheim , germania )  . 
per ( collimazione detettoriale : lacquisizione angiografica 320 , 6 mm abbinata a tecnologia z - flying focal spot ; tempo di rotazione del gantry : 330 ms ; risoluzione temporale effettiva : 165 ms ; avanzamento del lettino porta - pazienti : 3 , 84 mm / rotazione ; tensione del tubo : 120 kvp ; corrente 800850 mas ; direzione della scansione cranio - caudale ) sono stati preventivamente somministrati per via sub - linguale 0 , 3 mg di nitroderivati ( trinitrina ) e sono stati iniettati ev 100 ml di mezzo di contrasto ( mdc ) iodato idrosolubile ( iomeprol , iomeron 400 , bracco spa , milano , italia ) ad una velocit di 5 ml / s ( 2 gi / s ) , seguiti da una iniezione alla stessa velocit di 30 ml di soluzione salina . 
per la sincronizzazione del bolo di mdc , stata utilizzata una tecnica di bolus tracking con posizionamento di regioni di interesse ( roi ) nellaorta ascendente e partenza dellacquisizione dopo il rilevamento di un incremento densitometrico di 100 uh rispetto al valore misurato nelle scansioni senza mdc . 
sui dati grezzi sono stati effettuati due tipi di retro - ricostruzioni entrambi utilizzanti un algoritmo di ricostruzione half scan con dati ottenuti dalla rotazione del tubo di 180 ( dati ottenuti da un solo ciclo cardiaco ) , un campo di vista ( fov ) radiol med ( 2010 ) 115 : 702713 scanner 64 - detector ct ( sensation 64 , siemens , forchheim , germany ) with the following parameters : detector collimation 320.6mm combined with z - flying focal spot technology , gantry rotation time 330 ms , effective temporal resolution 165 ms , table feed 3.84 mm / rotation , tube voltage 120 kvp , current 800850 mas , scan direction craniocaudal . 
prior to the angiographic scan , patients received 0.3 mg sublingual nitroglycerin ( trinitrin ) and 100 ml of water - soluble iodinated contrast medium ( iomeprol , iomeron 400 , bracco s.p.a. , milan , italy ) injected intravenously at a rate of 5 ml / s ( 2 gi / s ) , followed by 30 ml of saline at the same rate . 
to synchronise the scan with the arrival of the bolus , the bolus - tracking technique was used , with a region of interest ( roi ) placed in the ascending aorta and scan trigger set at 100 hu over baseline . 
two types of reconstruction were used , both using a half - scan algorithm with data from a tube rotation of 180 ( data from a single cardiac cycle ) , a field of view ( fov ) restricted to the area of interest and a smooth convolution filter ( b30f ) [ 22 ]  . 
a multiphase , multiplanar reconstruction ( mpr ) was obtained in a four - chamber ( 4ch ) plane ; multiphase short - axis views were generated from the heart base to the apex such that they were perpendicular to the lv long axis in the 4ch view with the aim of acquiring 20 phases with 2 - mm slice thickness and 1 - mm increment throughout the cardiac cycle . mr scan protocol all acquisitions were performed on a 1.5 - t scanner ( achieva , philips medical systems , best , the netherlands ) with a maximum achievable gradient of 66 mt / m and a maximum slew rate of 180 mt / m / ms . 
during the cine balanced steady - state free precession ( b - ssfp ) sequences , the maximum gradient achieved was 33 mt / m and the maximum slew rate was 180 mt / m / ms . 
a fiveelement coil and a vector electrocardiogram were used for signal reception and cardiac synchronisation , respectively . a standard scan protocol was used to identify the true lv short axis , and subsequently a 2d cine b - ssfp sequence was acquired along that axis with sampling of the lv from base to apex . 
un protocollo di scansione standard stato seguito per individuare il vero asse corto del vsin , dopodich la sequenza 2d cine bsteady - state free - precession ( ssfp ) stata acquisita lungo questultimo asse campionando il vsin dalla base allapice ; tutte le acquisizioni sono state effettuate in massima espirazione , per evitare il non corretto allineamento delle singole sezioni , cos come gi descritto in letteratura [ 23 , 24 ]  . i parametri relativi alla sequenza 2d utilizzata sono stati : tempo si ripetizione ( tr ) 3 , 1 , tempo di eco ( te ) 1 , 53 ; flip angle 60 ; banda 1249 , 7 hx / pixel ; risoluzione in plane 22 , 3 mm ; spessore di strato 8 mm ; intervallo tra strati 2 mm ; risoluzione temporale 326 ms ( dipendente dalla frequenza cardiaca ) ; fasi cardiache 30 ; sense off ; half scan on . analisi dei dati trecentosessantadue data - set di volume in asse corto , 181 ottenuti dalle acquisizioni rm e 181 dalle ricostruzioni mpr multi - fasiche tc , sono stati inviati alla medesima consolle ( syngo mmwp , siemens ) su cui era implementato il software di analisi argus va60c ( siemens , forchheim , germania ) ( fig . 1 ) capace di gestire file in formato digital imaging and communications in medicine ( dicom ) provenienti da 706 radiol med ( 2010 ) 115 : 702713 maximum expiration to avoid incorrect alignment of the single sections , as described in the literature [ 23 , 24 ]  . 
an experienced observer analysed all images in a blinded fashion to calculate ef , end - diastolic volume ( edv ) , end - systolic volume ( esv ) , stroke volume ( sv ) and lv mass , according to published criteria [ 25 ]  . 
the first image of the cardiac cycle ( acquired at r wave ) was considered to be end diastolic , whereas the image displaying the smallest lv cavity was considered end systolic [ 9 ]  . 
after identifying the correct end - diastolic and end - systolic phases , the endocardial and epicardial contours were traced on the end - diastole images , and the endocardial contours were then propagated to end - systole with the aid of semiautomated software . 
un operatore esperto ha analizzato in cieco tutte le immagini con il fine di calcolare la fe , il volume tele - diastolico ( vtd ) , il volume tele - sistolico ( vts ) , la gittata sistolica ( gs ) , e la massa del vsin , secondo i criteri pubblicati in letteratura [ 25 ]  . 
la prima immagine del ciclo cardiaco ( acquisita in corrispondenza dellonda r ) stata considerata essere tele - diastolica , mentre limmagine con la pi piccola cavit del vsin visibile stata considerata tele - sistolica [ 9 ]  . dopo aver individuato la corretta fase tele - diastolica e la corretta fase tele - sistolica , sono stati tracciati i contorni endocardici ed epicardici sulle immagini in tele - diastole e successivamente i contorni endocardici sono stati propagati in tele - sistole con laiuto del software semi - automatico ; correzioni manuali sono state effettuate dove necessario ; i muscoli papillari e la trabecolatura sub - endocardica sono stati inclusi nella cavit del vsin [ 2628 ]  . 
la sezione pi apicale del vsin con cavit visibile stata considerata essere lapice , mentre la sezione pi basale circondata da almeno il 50% di miocardio stata considerata essere la base [ 14 ]  . 
screenshot della piattaforma software utilizzata per lanalisi dei parametri del vsa schermata utilizzata per la definizione dei contorni endocardici ed epicardici ; b schermata in cui vengono visualizzati i risultati . radiol med ( 2010 ) 115 : 702713 fig . 
mref , frazione di eiezione misurata con rm ; mrmass , massa del vsin misurata con rm . lumen was considered to be the apex , whereas the most basal section surrounded by at least 50% myocardium was considered to be the base [ 14 ]  . 
 il vtd e la massa del vsin hanno mostrato differenze significative tra le due metodiche ( p < 0 , 05 ) , tuttavia lerrore standard non ha avuto alcun impatto clinico ( bias vtd = 3 , 7% ; bias massa = 11 , 9% )  . 
 discussion a correct and reproducible assessment of lv function parameters , in particular , ef , is a fundamental step in establishing diagnosis , therapy and prognosis of patients with una valutazione corretta e riproducibile dei parametri funzionali del vsin , ed in particolare della fe , rappresenta un momento fondamentale nellinquadramento diagnostico , clinico e prognostico del paziente con patologie cardiache . molteplici studi hanno dimostrato che nei pazienti coronaropatici ed in quelli non coronaropatici laspettativa di vita correlata con il rimodellamento negativo e con la ridotta fe ; in conseguenza di ci , per il management dei pazienti coronaropatici e non , sono state stilate delle linee guida ampiamente basate sui valori di fe . 
many studies have demonstrated that in patients with and without coronary disease , life expectancy is correlated with negative remodelling and reduced ef . as a consequence , guidelines based on ef values have been developed to assist in the management of patients with or without coronary disease . 
although our results showed excellent concordance of mri and ct in assessing lv function , it is very unlikely that ct can be used as a first - line investigation owing to exposure to ionising radiation and intravenous iodinated contrast material . 
however , if the same raw data provided by ct coronary angiography are used to reconstruct a multiphase data set , lv function can be assessed without exposing the patient to any further dose of radiation or contrast material , and the anatomical study can be integrated with a functional study that has the same accuracy as mri . 
ct was given an appropriateness score of 5 in evaluating lv function following myocardial infarcimages tion in patients with technically limited ionizzanti ed alla somministrazione del mdc iodato endovena ; tuttavia , utilizzando gli stessi dati grezzi disponibili per una angiografia coronarica tc , possibile ricostruire un data - set multifasico con cui valutare la funzionalit del ventricolo sinistro senza necessit di una ulteriore esposizione a radiazioni ionizzanti e / o di una quantit aggiuntiva di mdc , permettendo cos di integrare il dato anatomico con un dato funzionale accurato al pari della rm . 
recentemente sono stati pubblicati i criteri di appropriatezza per lesecuzione di un esame cardio - rm e cardio - tc [ 29 ] ; questultima ha ottenuto un livello di appropriatezza 5 nella valutazione della funzione del vsin dei pazienti colpiti da infarto miocardico in cui non si riescono ad ottenere immagini diagnostiche allecocardiografia ; crediamo che la cardio - tc possa essere utilizzata per la valutazione della funzione del vsin dei pazienti colpiti da infarto miocardico , non solo in quelli con finestra ecocardiografica non ottimale , ma anche in quelli portatori di pace - maker ( fattore importante in pazienti cardiopatici ) , claustrofobici e / o con altri materiali ferromagnetici indovati nel proprio corpo in quanto la cardio - tc riesce a by - passare anche queste controindicazioni relative ad un esame rm ; in definitiva la tc , quindi , potrebbe radiol med ( 2010 ) 115 : 702713 fig . 
the box - and - whiskers plot shows the median ( middle line ) , lower and upper quartiles ( 25th and 75th percentile ; main box ) and the minimum and maximum values for ejection fraction and myocardial mass ( vertical lines )  . 
an outside value is defined as a value that is smaller than the lower quartile minus 1.5 times the interquartile range , or greater than the upper quartile plus 1.5 times the interquartile range ( empty square )  . 
a far - out value is defined as a value smaller than the lower quartile minus 3 times the interquartile range , or greater than the upper quartile plus 3 times the interquartile range ( black dot )  . 
il grafico box - and - whiskers mostra la mediana ( linea di mezzo ) , il quartile inferiore e superiore ( 25 e 75 percentile ; box principale ) , ed il valore minimo e massimo di frazione di eiezione e massa miocardica ( linee verticali )  . 
un outside value viene definito come un valore che pi piccolo del quartile inferiore meno 1 , 5 volte il range interquartile , o pi grande del quartile superiore pi 1 , 5 volte il range interquartile ( valori rappresentati con un quadratino vuoto )  . 
un far out value viene definito come un valore pi piccolo del quartile inferiore meno 3 volte il range interquartile , o pi grande del quartile superiore pi 3 volte il range interquartile ( valori rappresentati con un puntino nero )  . 
we believe that cardiac ct can be used to assess lv function following myocardial infarction not only in patients with suboptimal echocardiographic window but also in those with a pacemaker ( an important factor in patients with heart disease ) and / or other ferromagnetic materials , as well as in claustrophobic patients because cardiac ct is not limited by the contraindications of mri . 
ct might even be considered an alternative to mri in assessing ventricular function in selected cases . in our study , there was a statistically significant difference ( though without clinical impact ) in edv , with ct showing a tendency to underestimate edv . 
in our view , this underestimation cannot be attributed to limited temporal resolution , as it was not supported by a simultaneous overestimation of esv , which is theoretically more heavily dependent on temporal resolution ( volume changes are clearly faster at end - systole than at enddiastole )  . 
we believe that this significant and systematic underestimation of edv combined with a systematic albeit not significant underestimation of esv is related to the different respiratory phases in which the data sets are acquired with the two modalities : maximum expiration addirittura assumere un ruolo alternativo alla rm anche per la sola valutazione della funzione ventricolare in alcuni casi selezionati . nel nostro studio abbiamo osservato una differenza statisticamente significativa ( anche se non accompagnata da impatto clinico ) con una sottostima del vtd da parte della metodica tc ; a nostro avviso tale sottostima non riconducibile ad una limitata risoluzione temporale in quanto non supportata da una contemporanea sovrastima del vts che in teoria dovrebbe essere maggiormente condizionato dalla risoluzione temporale ( in tele - sistole i cambiamenti di volume sono sicuramente pi repentini che in tele - diastole ) ; crediamo che questa significativa e sistematica sottostima del vtd collegata ad una sistematica sebbene non significativa sottostima del vts siano da relazionare alla differente fase respiratoria in cui i data - set vengono acquisiti con le due differenti metodiche , e cio massima espirazione in rm e massima inspirazione in tc ; in particolare in massima inspirazione si ha una fisiologica riduzione del ritorno venoso al vsin con riduzione del vtd e conseguente riduzione del vts ; grazie a questa differenza sistematica riscontrata sia nel vtd che nel vts , la fe , parametro fondamentale nel decision making del paziente con patologie cardiache , risultata praticamente identica tra 710 radiol med ( 2010 ) 115 : 702713 fig . 
il grafico dimostra la dispersione dei dati raccolti utilizzando le due differenti metodiche ( rm e tc ) per lanalisi dei parametri del vsejection fraction , frazione di eiezione ; myocardial mass , massa del vsin misurata in tele - diastole ; edv , volume tele - diastolico ; esv , volume tele - sistolico ; mr , risonanza magnetica ; ct , tomografia computerizzata . at mri and maximum inspiration at ct . 
ventricular mass is calculated for each slice at end - diastole by le due metodiche ( 53%14% con rm vs 53%15% con tc ) , mostrando un alto grado di concordanza ed un bias ottimale per linterscambiabilit nella pratica clinica routinaria delle due metodiche ( bias < 1% )  . 
crediamo che la sistematica sottostima della massa del vsin sia anchessa dovuta alla differente fase del respiro in cui vengono acquisiti i data - set con le differenti metodiche ; la massa ventricolare viene calcolata per singola sezione in tele - diastole sottraendo larea delimitata dal contorno endocardico dallarea delimitata dal contorno epicardico ; la massa ottenuta dalle singole sezioni viene poi sommata per ottenere la massa totale del vsin ; intuitivo che se per i motivi di cui sopra larea delimitata dal contorno endocardico si riduce in inspirazione , diminuir anche larea delimitata dal contorno epicardico , tuttavia questultima si radiol med ( 2010 ) 115 : 702713 fig . 
analisi di bland - altman dei parametri del vsin ottenuti dai data - set rm e tc ; sono stati utilizzati dei limiti di concordanza di 1 , 96 ds . 
edv , volume tele - diastolico ; esv , volume tele - sistolico ; lv mass , massa ventricolo sinistro ; sd , deviazione standard ; ejection fraction , frazione di eiezione del ventricolo sinistro . subtracting the area delimited by the endocardial borders from that delimited by the epicardial borders . 
it is clear that if , for the reasons stated above , the area delimited by the endocardial borders is reduced at inspiration , the area delimited by the epicardial borders will also be reduced , but this reduction will occur in an exponential quadratic fashion and hence faster than the area within the endocardial borders , leading to a smaller difference between the two areas and to an underestimation of myocardial mass compared with that estimated with mri during maximum expiration . even though we made no quantitative assessment of the time required to analyse the mri and ct data sets , we ridurr in maniera esponenziale quadratica e quindi maggiore rispetto allarea delimitata dal contorno endocardico , portando ad una minore differenza tra le due aree ed in ultimo ad una sottostima della massa miocardica relativamente alla stessa calcolata con metodica rm in massima espirazione . anche se non abbiamo effettuato una analisi quantitativa del tempo impiegato per analizzare i data - set ottenuti dalla rm e dalla tc , ci sembra opportuno segnalare un evidente minor tempo di analisi per la metodica tc dovuto a nostro avviso alla maggiore facilit con cui il software riuscito a riconoscere automaticamente il bordo endocardico , verosimilmente grazie alla migliore risoluzione spaziale ottenuta con tc , che ci ha permesso di limitare 712 radiol med ( 2010 ) 115 : 702713 should point out that the analysis was evidently faster for ct . 
non abbiamo riportato una analisi regionale della funzione del vsin in quanto nel nostro centro non viene eseguita routinariamente su tutti i pazienti sottoposti ad una angiografia coronarica con tc multistrato . 
 conclusioni abbiamo riscontrato unottima concordanza tra i parametri funzionali del vsin studiati con cardio - rm e con cardio - tc in una vasta popolazione di pazienti ; riteniamo , pertanto , che la metodica tc oltre a fornire delle ormai validate ed indiscutibili informazioni sullo stato dellalbero arterioso coronarico , possa , al pari della rm , fornire preziose informazioni anche sulla funzione ventricolare sinistra . 
lintegrazione pertanto dei dati morfologici dovrebbe essere sempre accoppiata alla valutazione funzionale nei pazienti sottoposti ad esame cardio - tc . limitations we did not evaluate intraand interobserver variability , as we aimed to describe our routine clinical experience and because the intraand interobserver variability of the two modalities has already been widely investigated [ 817 , 24 , 25 , 27 , 28 ]  . 
we therefore believe that , in addition to its validated and indisputable role in coronary tree imaging , ct is as valuable as mri in providing information on lv function . 
altinok4 1izmir education and research hospital , radiology department , izmir , turkey 2ege university medical school , department of radiology , izmir , turkey 3tepecik education and research hospital , radiology department , izmir , turkey 4buca medical center , radiology department , izmir , turkey correspondence to : o . 
no : 35 daire no : 31 karsiyaka izmir , tel . : + 90 - 532 - 3330201 , fax : + 90 - 532 - 2505050 , e - mail : oztekinozgur@gmail.com received : 21 may 2009 / accepted : 3 september 2009 / published online : 22 february 2010 springer - verlag 2010 abstract purpose . 
of 25 patients with spinal brucellosis , eight had thoracic , ten had lumbar , five had both thoracic and lumbar and two had both lumbar and sacral vertebral involvement . we detected posterior longitudinal ligament elevation in 11 patients , epidural abscess formation in 11 and paravertebral abscess formation in nine . 
i corpi vertebrali , i piatti vertebrali e i dischi intervertebrali erano ipointensi e radiol med ( 2010 ) 115 : 794803 hypointense and heterogeneous in the subacute and chronic stages on t1and t2 - weighted images , respectively . 
although conventional mri has several advantages over other imaging modalities and is very useful in the differential diagnosis between brucellar spondylodiscitis and other spinal pathologies , it has some difficulties in discriminating acute and chronic forms of spondylodiscitis . 
dwi is a sensitive , fast sequence that has the potential for differentiating acute and chronic forms of spondylodiscitis , which makes it crucial in spinal imaging . keywords brucellosis spondylodiscitis magnetic resonance imaging diffusion - weighted imaging vertebrae iperintensi nello stadio acuto , mentre erano ipointensi e eterogenei negli stadi subacuto e cronico , rispettivamente nelle sequenze t1e t2 dipendenti . 
nonostante la rm convenzionale abbia parecchi vantaggi rispetto ad altre metodiche di immagine e sia molto utile nella diagnosi differenziale tra la spondilodiscite brucellare e altre patologie spinali , tale metodica presenta delle difficolt nel differenziare le forme acute e croniche della spondilodiscite . 
limaging pesato in diffusione una sequenza sensibile e veloce che possiede il potenziale per differenziare le forme acute e croniche di spondilodiscite rendendola pertanto fondamentale nella diagnostica per immagini spinale . parole chiave brucellosi spondilodiscite imaging di risonanza magnetica imaging pesato in diffusione vertebre introduction spondylodiscitis is an infection of the intervertebral disc and the adjacent vertebrae , with or without associated epidural or psoas abscesses [ 1 ]  . 
it is frequently caused by staphylococcus aureus and , in endemic areas , by mycobacterium tuberculosis and brucella spp [ 1 ]  . brucellosis is a common zoonosis , which still remains a major health problem in the mediterranean region , the middle east , and parts of latin america [ 2 ]  . 
it is not only an occupational disease in developed countries but also a common health problem in endemic countries owing to consumption of unpasteurised milk or milk products from infected animals [ 3 ]  . 
osteoarticular manifestations , including sacroiliitis , peripheral arthritis , spondylitis , osteomyelitis , and bursitis , are the most frequent complications of brucellosis and occur in one third of the patients [ 4 ] .diagnosing brucellar spondylodiscitis is often difficult ; clinical findings are usually nonspecific , and radiological features may mimic those of other bacterial , fungal , inflammatory , and neoplastic diseases . 
as spondylodiscitis may be a serious disease due to diagnostic delay and inadequate treatment , early diagnosis and differentiation of acute and chronic forms of spondylodiscitis are crucial in the management of the disease [ 5 ]  . the aim of this study was to evaluate the contribution and role of diffusion - weighted imaging ( dwi ) in differentiating acute and chronic forms of brucellar spondylodiscitis . we also describe the distinguishing features and some confusing mri findings associated with brucellar spondylodiscitis . 
 materials and methods this retrospective study included 25 cases ( 14 women and 11 men ; mean age 56.8 years ; age range1885 years ) of brucellar spondylodiscitis , which were recruited from the archive system of two different imaging services among 147 patients with presumed spondylodiscitis between 2002 and 2009 . 
sagittal spinal dwi were acquired using a single - shot echoplanar imaging sequence ( ssh - epi ) and reversed fast imaging with steady - state precession sequences ( psif ) on the philips and siemens systems , respectively . 
when the onset of disease symptoms was < 3 months , between 3 and 12 months , or > 12 months , it was considered to be acute , subacute or chronic brucellosis , respectively . mris were evaluated by two radiologists ( oo , cc ) , and the following lesions were sought on mri : ( 1 ) dwi characteristics of vertebral lesions ; ( 2 ) disc lesions ; ( 3 ) vertebral lesions ( bone marrow oedema and type and quantification of tissue destruction ) ; ( 4 ) facet - joint involvement ; ( 5 ) spinal compression and its mechanism ( backwards displacement of the posterior wall , epidural abscess ) ; ( 6 ) radicular compression ; and location and size of abscesses ( epidural or paravertebral )  . 
data were analysed using spss for windows ( microsoft ) , version 10.0 ( statistical package for the social sciences , chicago , il , usa )  . results this study evaluated 25 patients with spondylitis and spondylodiscitis due to brucellosis . 
of the 25 patients with spinal brucellosis , eight had thoracic , ten had lumbar , five had both thoracic and lumbar and two had both lumbar and sacral vertebral involvement . 
in the subacute and chronic stages , mri revealed hypointense and heterogeneous signal intensities in the t1and t2 - weighted images , respectively . on stir images , all patients in the subacute and chronic stages had high signal intensities . 
c sagittal t1 - weighted image after iv injection of gadoliniud diffusion - weighted imaging reveals extensive bone destruction at the l4 vertebra , and the l4 - 5 disc is destroyed and replaced by abscess formation . 
d la sequenza pesata in diffusione dimostra estesa erosione ossea a carico del corpo di l4 ; il disco intervertebrale tra l4 e l5 distrutto e sostituito dalla presenza di un ascesso . 
infectious spondylitis is an infection by a specific organism of one or more components of the spine , namely , the vertebrae , intervertebral discs , paraspinal abnormal soft tissues , and epidural space . 
in brucellosis , sacroiliitis and involvement of the hip joints are seen mostly in the acute stage of the disease in young patients , whereas spondylitis and spondylodiscitis usually occur in the chronic stage of the disease in adults the elderly . 
this may be the reason for the higher mean age ( 56.8 years ) in our series than the mean age previously reported by pourbagher et al . in their series of brucellosis patients with osteoarticular involvement in which only 10.4% of patients had spondylodiscitis [ 4 ]  . although the initial clinical signs of brucella infection appear 24 weeks after inoculation , the earliest radiological signs may appear as late as 12 weeks or more after symptom onset [ 2 , 6 ]  . 
due to its high blood supply , the superior end plate is the usual starting point in most cases of spinal brucellosis , although the inferior end plate may also be involved [ 2 ]  . 
a the t1 - weighted image reveals complete signal loss at the t5 and t6 vertebrae bodies , a defect on the inferior end plate of the t5 vertebra mimicking schmorls nodules and abscess formation at the t5 - 6 intervertebral disc space and epidural space . 
a limmagine t1dipendente dimostra la perdita completa del segnale a carico di corpi vertebrali di d5 e d6 , un difetto del piatto vertebrale inferiore di d5 imita dei noduli di schmorl e la formazione di ascesso nello spazio discale intervertebrale tra d5 - d6 e lo spazio epidurale . 
d la sequenza pesata in diffusione dimostra ridotta diffusione a carico dello spazio discale intervertebrale tra d5 e d6 e alta ed eterogenea intensit di segnale delladiacente corpo vertebrale , che conferma la diagnosi . 
d limmagine pesata in diffusione mostra alta intensit di segnale delle vertebre vicine , che conferma la diagnosi di spondilodiscite acuta . the lumbar region is the most frequent site of occurrence , whereas the cervical region is the least affected site of spondylodiscitis in patients with brucellosis . 
 [ 15 ] , noncontiguous multifocal spinal involvement was observed in seven patients ( 28% ) in our study , a figure higher than those reported in the literature [ 7 , 10 ]  . 
even in extensive cases , vertebral collapse and gibbus deformity are rare findings , and the vertebral body is usually morphologically intact . none of our patients had vertebral gibbus formation , which is in agreement with the literature . 
paravertebral and epidural abscess formation and spinal cord and root compression are considered very rare findings in brucellar spondylodiscitis and are generally considered to be findings for tuberculosis and pyogenic features 800 radiol med ( 2010 ) 115 : 794803 spondylodiscitis . 
 [ 2 ] as a distinguishing feature of brucellar spondylodiscitis in 27% of patients in their series . we also had three patients with facet joint involvement , which might be due to primary facet joint involvement , a reactive process or a spontaneous process . radiographs of the spine , bone scans and computed tomography ( ct ) all provide useful information in the diagnosis of brucellar spondylodiscitis . 
however , none of these modalities can provide as much useful information as mri . multiplanar capability and superior tissue contrast make mri the modality of choice in evaluating patients with infectious spondylitis , as well as for follow - up examinations in such patients [ 12 , 14 , 15 ]  . 
mri has various advantages over other imaging modalities , including discriminating spondylodiscitis from other spinal pathologies and brucellar spondylodiscitis from other causes of spondylodiscitis . differentiation of the acute form from the subacute and chronic forms of the disease , however , is a matter of question with conventional sequences . 
diffusion is the term used to describe the random motion ( or brownian motion ) of water molecules and dw - mri measures the mobility of water protons in tissues . 
 [ 5 ] is the only study in the literature that directly compares diffusion characteristics and apparent diffusion coefficient ( adc ) values in infections with those of malignant lesions , concluding that the diffusion technique is not useful due to an overlap in adc values . 
in previous studies , it was concluded that patients with spondylodiscitis were considered to have a benign disease , and they showed the characteristics of malignant lesions with respect to diffusion characteristics [ 5 , 18 ]  . 
it has been shown that dwi reveals hyperintensity in the affected vertebrae and paravertebral infectious soft tissue in acute spondylodiscitis , whereas in the chronic stage , it reveals hypointensity . 
it can be suggested that in acute spondylodiscitis , increased inflammatory cell packing may lead to a smaller and more restricted extracellular space , resulting in increased signal from restricted water protons . 
this decreased amount of free water , as well as restricted mobility due to hypercellularity , may result in increased signal intensity on dwi ( as has been observed in vertebral metastatic infiltration )  . 
after integrating dwi , the diagnostic accuracy reached 100% in differentiating acute and chronic forms of the disease , but the subacute form could not be differentiated in all cases . in conclusion , although conventional mri has various advantages over other imaging modalities and is very useful in obtaining the differential diagnosis between brucellar spondylodiscitis and other spinal pathologies , it has some difficulties in discriminating acute and chronic forms of spondylodiscitis . 
dw - mri is a sensitive , fast sequence and has the potential for differentiating acute and chronic forms of spondylodiscitis , which makes it crucial in spinal imaging . radiol med ( 2010 ) 115 : 794803 fig . 
muzzio1 , 3 1dipartimento di scienze medico - diagnostiche e terapie speciali , 2dipartimento di scienze oncologiche e chirurgiche , clinica chirurgica ii , universit di padova , via giustiniani 2 , 35128 padova , italy 3istituto oncologico veneto ( iov - irccs ) , sezione di radiodiagnostica oncologica , via gattamelata 64 , 35128 padova , italy correspondence to : f . 
anal endosonography and fistulography with radiopaque markers are important complements to surgical exploration for investigating anal sepsis and may be of value to the surgeon in planning a therapeutic strategy . 
i pazienti sono stati sottoposti , prima dellintervento , ad ecografia endoanale e / o fistolografia . la tecnica fistolografica stata modificata perch utilizza anche un catetere di foley endorettale ed un anello metallico anale , con funzione di reperi radiopachi . 
lecografia e la fistolografia hanno diagnosticato la presenza e decorso del tramite principale rispettivamente nell82 , 2% e nel 100% dei casi , la presenza e sede dellorifizio interno nel 79% e nel 74 , 2% , la presenza e sede di tramiti secondari nel 98% e 91 , 8% , la presenza di ascessi nel 92 , 9% e 87 , 8% . 
lecografia endoanale e la fistolografia con reperi radiopachi sono tecniche diagnostiche valide nella diagnosi preoperatoria delle fistole anali e possono essere utili per il chirurgo nella pianificazione della strategia terapeutica . parole chiave fistola anale ecografia endoanale fistolografia chirurgia 772 introduction anal fistula is a surgical condition with a prevalence rate of 8.6 cases per 100 , 000 [ 1 ] ; 10%15% of anal fistulas have a complicated course and are classified as complex . 
a fistula is defined as complex if it involves a large portion of the anal sphincter ( high transsphincteric , suprasphincteric ) , is anterior in a female patient or has multiple tracks or a horseshoes shape [ 2 ]  . 
there is evidence that patients may benefit from specialised preoperative imaging , especially in cases of complex sepsis and fistula crossing the puborectalis muscle [ 4 , 5 ]  . 
computed tomography ( ct ) , especially with the multidetector - row technique , is known for its inherent high spatial resolution but usually fails to accurately assess the sphincters , active fistulas and fibrotic fistulous tracks because of its inadequate soft - tissue contrast resolution [ 6 , 7 ]  . 
the advantages of magnetic resonance imaging ( mri ) include excellent intrinsic soft - tissue resolution showing the track system in relation to surrounding anatomical structures , together with multiplanar imaging capabilities [ 8 , 9 ]  . 
as a result , comparison with other diagnostic techniques and the clinical outcome after surgery is necessary for a confident final classification of the fistula [ 11 , 12 ]  . anal endosonography ( aes ) is safe , rapid and well tolerated by patients . 
usually , aes is able to identify the sphincters and intersphincteric plane [ 15 ] , but infection cannot be distinguished from fibrosis , and insufficient depth penetration results in a failure to identify secondary ramifications and deep abscesses [ 13 , 14 ]  . however , aes combined with hydrogen peroxide as a contrast material , which enhances the fistulous track , and three - dimensional aes have proved useful in improving the reliability of ultrasound imaging of fistula - in - ano [ 1620 ]  . finally , fistulography ( fg ) is a radiological technique that has been used with conflicting results [ 21 , 22 ]  . 
the technique may be helpful in assessing the presence and extent of the fistula - in - ano but does not show the relationship of the fistula to the sphincter muscles because the sphincter muscles themselves are not directly imaged . 
several studies have compared aes with mri [ 14 , 23 ] , with some reporting better results with aes [ 23 ] and others with mri [ 14 ]  . 
in another study , some authors showed that aes , mri and surgical exploration were all accurate tests for determining fistula anatomy in patients with perianal fistulas [ 20 ]  . 
we found only one study comparing aes and fg , and the authors concluded that fg has no place in the radiol med ( 2010 ) 115 : 771783 introduzione la fistola anale una patologia chirurgica con prevalenza pari a 8 , 6 casi per 100000 [ 1 ]  . 
una fistola anale definita complessa se interessa unampia porzione dello sfintere anale ( transfinterica alta , sovrasfinterica ) , anteriore nel sesso femminile , ha tramiti multipli o ha conformazione a ferro di cavallo [ 2 ]  . 
vi evidenza che i pazienti possono trarre beneficio dalla diagnostica strumentale preoperatoria , in particolare nei casi di sepsi complesse e di fistola che attraversa il muscolo puborettale [ 4 , 5 ]  . 
la tomografia computerizzata ( tc ) , soprattutto quella multidetettore , ha elevata risoluzione spaziale , ma spesso non valuta con precisione gli sfinteri , le fistole attive ed i tramiti fistolosi fibrotici per una risoluzione di contrasto inadeguata [ 6 , 7 ]  . 
i vantaggi della risonanza magnetica ( rm ) sono leccellente risoluzione di contrasto , in grado di dimostrare i rapporti del tramite fistoloso con le strutture anatomiche circostanti , e la rappresentazione anatomica multiplanare [ 8 , 9 ]  . 
la rm per imprecisa nellidentificare la sede dellorifizio interno , perch non riconosce la linea dentata [ 10 ] ; perci , per la corretta classificazione finale della fistola , necessario il confronto con altre tecniche diagnostiche e con lesito dellintervento chirurgico [ 11 , 12 ]  . 
molti studi [ 13 , 14 ] hanno dimostrato la relativa inadeguatezza della valutazione clinica delle fistole , se paragonata ai riscontri ottenuti con leea . leea generalmente individua gli sfinteri ed il piano intersfinterico [ 15 ] , ma non in grado di differenziare un processo infiammatorio attivo dalla fibrosi ; inoltre tramiti secondari ed ascessi profondi possono non essere individuati per insufficiente profondit di penetrazione del fascio ultrasonoro [ 13 , 14 ]  . 
comunque , leea con perossido didrogeno come mezzo di contrasto e leea tridimensionale si sono rivelati utili per migliorare laffidabilit degli ultrasuoni nello studio delle fistole anali [ 1620 ]  . 
la tecnica pu essere utile nel valutare la presenza e lestensione della fistola , ma non mostra i rapporti della fistola con gli sfinteri , perch non li visualizza direttamente . 
in un altro studio gli autori hanno dimostrato che eea , rm ed esplorazione chirurgica sono tutte modalit accurate nel definire radiol med ( 2010 ) 115 : 771783 preoperative diagnosis of fistula - in - ano [ 24 ]  . 
the purpose of our study was to compare the results of aes and modified fg with surgical findings and to assess the agreement between ultrasound and radiology in the preoperative classification of anal fistulas . materials and methods patients a retrospective review of 113 patients who had undergone aes and / or fg in their preoperative management of fistulain - ano was carried out . 
all ultrasound studies were performed by the same team of four colorectal surgeons , all radiological studies were performed by the same gastrointestinal radiologist and surgery was performed by the same colorectal surgeon . 
the ultrasound equipment used was a type - 2001 bk medical scanner ( copenhagen , denmark ) with a type - 1850 , 360 rotating endosonic probe mounted with a type - 6005 multifrequency transducer ( 5 mhz , 7 mhz and 10 mhz )  . 
the frequency used was usually 10 mhz ( focal range 24.5 cm ) , although occasionally , extensions from the primary track were visualised with a 7 - mhz frequency . 
 fistulography fg was performed with a previously described technique involving the use of anorectal radiopaque markers [ 25 ]  . briefly , a 22 - fr foley catheter was inserted into the rectum through the anal canal and retained at the anorectal junction by means of the catheter balloon , which was filled with water - soluble radiopaque contrast material . 
abbiamo trovato un unico studio di confronto fra eea e fg ; gli autori hanno concluso che la fg non ha un ruolo nella diagnostica preoperatoria della fistola anale [ 24 ]  . 
scopo del nostro studio di confrontare i risultati delleea e della fg con i reperti chirurgici e di valutare la concordanza tra ecografia e radiologia nella classificazione preoperatoria delle fistole anali . materiali e metodi pazienti abbiamo realizzato uno studio retrospettivo in 113 pazienti affetti da fistola anale ed indagati preoperatoriamente con eea e / o fg . 
tutte le indagini ecografiche sono state condotte dallo stesso gruppo di quattro chirurghi colorettali , tutti gli studi radiologici sono stati eseguiti dallo stesso radiologo gastrointestinale e la chirurgia stata eseguita dallo stesso chirurgo colorettale . ecografia unora prima di eseguire lo studio ecografico , tutti i pazienti sono stati sottoposti a pulizia rettale standard con un clistere di 250 ml . 
lecografo utilizzato un apparecchio b & k medical ( copenhagen , danimarca ) dotato di sonda 1850 , rotante a 360 e di trasduttore 6005 multifrequenza ( 5 mhz , 7 mhz e 10 mhz )  . 
 sempre stata utilizzata la frequenza di 10 mhz ( distanza focale di 24 , 5 cm ) , sebbene occasionalmente sia stata utilizzata quella di 7 mhz per lo studio dellestensione a distanza dellinfezione . 
 fistolografia la fg stata eseguita con una tecnica gi descritta in letteratura e che utilizza dei reperi anorettali radiopachi [ 25 ]  . in breve , un catetere di foley di 22 fr inserito nel retto attraverso il canale anale ; il palloncino allestremit del 774 radiol med ( 2010 ) 115 : 771783 catetere posizionato alla giunzione anorettale e riempito di mezzo di contrasto radiopaco idrosolubile . 
a seconda della sua dimensione , lorifizio esterno della fistola incannulato con un catetere endovenoso flessibile o un catetere di foley ; essi sono collegati ad una siringa contenente 10 ml di mezzo di contrasto radiopaco idrosolubile . 
la modifica consiste nel dividere le fistole transfinteriche in alte , medie o basse , in rapporto allanatomia ecografica del canale anale o alla sua suddivisione in tre parti nelle immagini radiografiche [ 17 , 29 ] ; 3 . 
depending on its size , the external opening of the fistulous track was cannulated with a flexible intravenous tube or a foley catheter connected to a syringe containing 10 ml of water - soluble contrast material for fg . 
because of the different surgical options , this classification was modified to determine the level of the fistula relative to the radiol med ( 2010 ) 115 : 771783 fig . 
a fistulography performed via an 8 - fr foley catheter after filling the balloon ( white arrowhead ) with water . frontal fistulogram revealing transsphincteric fistula ( black arrows ) , internal opening ( black arrowhead ) into the upper third of the anal canal ( high transsphincteric fistula ) and secondary track ( white arrow )  . 
b a 22 - fr foley contrast - enhanced balloon ( f ) at the anorectal junction , foley tube ( t ) in the anal canal , metal ring ( r ) around the foley tube close to the anus , puborectal muscle ( pm ) , water - filled balloon at the tip of the 8 - fr foley catheter ( white arrowhead ) , transsphincteric fistula ( black arrows ) , internal opening ( black arrowhead ) and secondary track ( white arrow )  . 
il fistologramma frontale dimostra la fistola transfinterica ( frecce nere ) , lorifizio interno ( punta di freccia nera ) al terzo superiore del canale anale ( fistola transfinterica alta ) ed un tramite secondario ( freccia bianca )  . b il disegno mostra il palloncino ( f ) di un catetere di foley da 22 fr riempito di contrasto alla giunzione anorettale , il tubo del foley ( t ) allinterno del canale anale , un anello metallico ( r ) attorno al tubo del foley vicino allano , il muscolo puborettale ( pm ) , il palloncino riempito dacqua allestremit del catetere di foley da 8 fr ( punta di freccia bianca ) , la fistola transfinterica ( frecce nere ) , lorifizio interno ( punta di freccia nera ) ed un tramite secondario ( freccia bianca )  . 
il canale anale idealmente suddiviso in tre segmenti uguali ( linee tratteggiate ) : alto ( h ) , medio ( m ) , basso ( l )  . risultati ecografia novantanove pazienti ( 58 maschi , 41 femmine ; et media , 44 anni ; range 2179 anni ) sono stati sottoposti ad eea . lintervallo medio fra lindagine e lintervento era di 72 giorni ( range 0288 giorni )  . 
dei 99 pazienti analizzati preoperatoriamente con eea , 33 avevano una fistola semplice , 31 una fistola giudicata complessa e 35 una recidiva di fistola trattata inizialmente in altri ospedali . 
nella valutazione dellorifizio interno , sono stati esclusi 37 / 99 ( 37 , 4% ) pazienti che al momento dellesame presentavano fistole drenate da setoni , in quanto il riconoscimento della comunicazione col canale anale sarebbe stato facilitato dagli echi riferibili ai drenaggi . 
nei 62 / 99 casi considerati , leea ha dimostrato un orifizio interno in 31 / 62 ( 50% ) pazienti ; in 29 ( 93 , 5% ) di essi c stata la conferma chirurgica . 
nella classificazione delle fistole anali , le percentuali peggiori di accuratezza delleea si sono avute per le fistole transfinteriche basse ( 63 , 3% ) e per quelle sottomucose ( 66 , 7% ) ( tabella 2 )  . 
per quanto riguarda gli ascessi , sono stati diagnosticati con eea in 35 / 99 ( 35 , 4% ) pazienti ; 33 ( 94 , 3% ) di essi sono stati confermati dalla chirurgia . 
intraoperatoriamente sono stati identificati due ascessi misconosciuti con eea , mentre non sono state osservate cinque raccolte evidenziate alleea ( tabella 1 )  . leea ha dimostrato un tramite a ferro di cavallo in 18 / 99 ( 18 , 2% ) pazienti , in 17 ( 94 , 4% ) dei quali c stata la conferma chirurgica . 
i falsi negativi per tramite a ferro di cavallo sono stati 12 / 99 ( 12 , 1% ) ( tabella 1 ) : quattro fistole avevano un decorso tortuoso ed otto erano recidive . 
la causa dellunico falso positivo stata lerrata diagnosi di fistola attiva in presenza di tessuto cicatriziale postchirurgico . fistolografia sono stati studiati con fistolografia 49 pazienti ( 31 maschi , 18 femmine ; et media 44 anni ; range 2174 anni )  . 776 radiol med ( 2010 ) 115 : 771783 extent of the anal canal . 
con ecografia , sono visibili un tramite ipoecogeno nello sfintere anale esterno ( eas ) posteriormente e lorifizio interno ad ore 6 ( freccia )  . a total of 99 patients underwent aes ( 58 men , 41 women ; mean age 44 years ; range 2179 years )  . 
at preoperative aes , 33 / 99 patients had a simple fistula , 31 had a complex fistula and 35 who had been initially treated at other institutions had a recurrent fistula . 
on assessing the internal opening , 37 / 99 ( 37.4% ) seton - catheter - drained fistulas were excluded because the echoic seton can facilitate identification of the internal opening . 
among the remaining 62 / 99 patients , the internal opening was diagnosed with aes in 31 / 62 ( 50% ) , and 29 of them ( 93.5% ) were confirmed by surgery . 
regarding the accuracy of aes in classifying fistula - in - ano , the worst results were obtained for low transsphincteric ( 63.3% ) and submucosal ( 66.7% ) tracks ( table 2 )  . 
abscesses were detected with aes in 35 / 99 lesame stato eseguito in regime ambulatoriale , ad un intervallo medio di 83 giorni ( range , 1252 giorni ) prima dellintervento chirurgico . 
nella valutazione dellorifizio interno , sono state escluse 18 / 49 ( 36 , 7% ) fistole che al momento dellesame erano drenate da setoni perch la presenza del setone avrebbe potuto facilitare il riconoscimento della comunicazione con il canale anale . 
nei restanti 31 / 49 pazienti , la presenza di un orifizio interno stata diagnosticata in 15 / 31 ( 48 , 4% ) casi con la fistolografia ; in 14 ( 93 , 3% ) di essi c stata la conferma chirurgica . 
false negative findings were noted in 12 / 99 ( 12.1% ) cases of horseshoe fistula ( table 1 ) , tortuous in four cases and recurrent in eight cases . in the only false positive case , aes was unable to distinguish postsurgical scar tissue from active fistula . 
in the remaining 31 / 49 individuals , internal openings were diagnosed in 15 / 31 ( 48.4% ) cases with fg , and 14 of them ( 93.3% ) were confirmed by surgery . 
analogamente , tutte le nove fistole a ferro di cavallo individuate radiograficamente sono state confermate dalla chirurgia , mentre altri tre casi diagnosticati con la chirurgia non erano stati riconosciuti con fg ( tabella 3 )  . ecografia e fistolografia associate trentacinque pazienti sono stati sottoposti sia ad eea che fg . 
leea stata eseguita prima della fg in 23 / 28 ( 82 , 1% ) dei casi considerati . leea ha fornito risultati migliori della fg nella diagnosi della sede dellorifizio interno , dei tramiti secondari e ascessi ( tabella 4 ) , senza tuttavia differenze statisticamente significative . 
la concordanza diagnostica tra le due tecniche dindagine stata buona , soprattutto nella diagnosi dei tramiti secondari e delle fistole a ferro di cavallo ( tabella 5 )  . discussione il successo del trattamento chirurgico di una fistola dipende dalla valutazione accurata del tramite principale , del suo orifizio interno e delle eventuali estensioni secondarie . 
nel nostro studio la valutazione clinica non stata in grado di differenziare fistole transfinteriche medie o alte da tramiti intersfinterici , n di individuare i tramiti secondari alti o pelvici ( ovvero , sopra il piano del muscolo elevatore ) e le fistole a ferro di cavallo . 
leea e la rm sono le principali tecniche utilizzate attualmente . usando i criteri della medicina basata sullevidenza , un recente lavoro di revisione della letteratura , ha concluso che la rm superiore sia allesame clinico che alleea nella classificazione della complessit delle fistole anali [ 13 ]  . 
il fistologramma obliquo dimostra una fistola complessa : tramite principale ( frecce ) , ascesso ( asterisco ) nella fossa ischioanale destra ed orifizio interno ( punta di freccia ) alla giunzione anorettale che testimonia lestensione della fistola oltre il piano del puborettale . 
using evidence - based medicine methods , a recent review concluded that mri is superior to both clinical examination and aes in classifying the complexity of anal fistulas [ 13 ]  . 
the concordance rate between aes and surgery in detecting the internal opening ranges from 31% to 92% using a 10 - mhz transducer [ 14 , 32 , 33 ]  . the accuracy rate in our study was 79% . 
la percentuale di concordanza tra eea e chirurgia nel riconoscimento dellorifizio interno varia da 31% a 92% , utilizzando un trasduttore da 10 mhz [ 14 , 32 , 33 ]  . 
tale differenza di valori percentuali poterebbe essere dovuta ai criteri utilizzati per diagnosticare lorifizio interno , ai criteri dinclusione dei pazienti ( esempio : in alcuni studi sono stati esclusi i pazienti con fistole semplici basse ) e allesperienza delloperatore . 
in our study , the concordance rate between aes and surgical findings was 82.8% ( table 2 )  . we think that this variation may also be related to the anatomical course of the anal fistulas . 
this finding is consistent with results from a previous study reporting a similar accuracy rate of 80% in 76 patients with recurrent disease , 50 ( 65.8% ) of whom had transsphincteric fistulas [ 14 ]  . 
regarding secondary tracks , abscesses and horseshoe fistulas , the imbalance between the proportion of true positive and true negative cases ( table 1 ) may have contributed to the discrepancy between our findings and those reported by other authors [ 14 , 32 , 33 ]  . 
the two false positive findings could have been due to a long interval between fg and surgery ( 153 and 154 days , respectively ) , with probable spontaneous healing . 
our radiographic findings seem to be in contrast with those of some authors , who found that preoperative fg was of little use in the surgical treatment of fistula - in - ano [ 22 , 24 ]  . 
for example , by subdividing the anal canal into three equal segments , we could identify a high fistula which means the levator plate was reached and the level of risultati possa anche essere imputata alla tipologia delle fistole anali pi rappresentata nelle differenti casistiche . 
la prevalenza delle fistole transfinteriche nel nostro campione ( 65 / 99 ; 65 , 7% ) probabilmente pu spiegare la buona percentuale di accuratezza ( 82 , 8% )  . 
tale risultato coerente con quello di un precedente studio che riporta una percentuale di accuratezza ( 80% ) , sovrapponibile alla nostra , in 76 pazienti con malattia ricorrente 50 dei quali ( 65 , 8% ) con fistole transfinteriche [ 14 ]  . 
per quanto riguarda i tramiti secondari , gli ascessi e le fistole a ferro di cavallo , lo squilibrio tra la percentuale di casi veri positivi e veri negativi ( tabella 1 ) pu aver contribuito alla differenza tra i nostri risultati e quelli riportati da altri autori [ 14 , 32 , 33 ]  . 
lalta percentuale di casi veri negativi nellidentificazione di tramiti secondari ( 89 / 99 ; 89 , 9% ) , ascessi ( 59 / 99 ; 59 , 6% ) e fistole a ferro di cavallo ( 69 / 99 ; 69 , 7% ) probabilmente giustifica lelevata percentuale di specificit ( rispettivamente 98 , 9% , 92 , 2% ed 85 , 2% ) nel nostro campione ( tabella 1 )  . 
inoltre lalta percentuale di accuratezza del nostro studio ( rispettivamente 98% , 91 , 9% ed 86 , 9% ) pu dipendere dal basso numero di casi positivi ( rispettivamente 8 / 99 , 33 / 99 e 17 / 99 ) relativamente a quello dei negativi ( tabella 1 )  . 
la fg , cos modificata , ha individuato il tramite principale in tutti i 99 pazienti e lo ha sempre classificato correttamente in basso , medio ed alto rispetto al canale anale identificato dai reperi radiopachi . 
i nostri risultati radiografici sembrano essere in contrasto con quelli di alcuni autori che hanno giudicato la fg preoperatoria di scarsa utilit per il trattamento chirurgico della fistola anale [ 22 , 24 ]  . la differenza tra risultati ottenuti pu essere spiegata dalla diversa tecnica utilizzata nel nostro studio . 
depending on the size of the external opening , we used intravenous or foley catheters of different sizes so that contrast medium injected under pressure could not leak out through the external opening . 
moreover , there was good overall agreement between the techniques investigated in the group of 28 patients who underwent both aes and fg . one limitation of the study was the long interval between aes and surgery ( mean 72 days ) as well as between fg and surgery ( mean 83 days )  . 
 although retrospective , our single - centre study demonstrates that results of aes and fg in detecting the internal opening , primary track , secondary extensions and abscesses were very similar in classifying the complexity of the anal fistulas . 
therefore , we conclude that aes and fg are valuable diagnostic tools for selecting the appropriate surgical option in the treatment of fistula - in - ano . fistola alta , ovvero una fistola che ha raggiunto il piano dellelevatore , ed il livello dellorifizio interno . 
complessivamente , i nostri risultati sulla capacit delleea e della fg di riconoscere : orifizio interno , tramite principale , tramiti secondari , ascessi e fistole a ferro di cavallo sono sovrapponibili . 
 un limite di questo studio il lungo intervallo tra eea e chirurgia ( media , 72 giorni ) e tra fg e chirurgia ( media , 83 giorni )  . 
il terzo limite che solo parte dei pazienti sono stati sottoposti sia a eea sia a fg ; per questo motivo il confronto tra eea e fg meno consistente . anche se retrospettivo , il nostro studio monocentrico dimostra che i risultati di eea e fg nella visualizzazione di : orifizio interno , tramite principale , tramiti secondari ed ascessi sono pressoch simili nella classificazione della complessit delle fistole anali . 
grassi2 1 uoc diagnostica per immagini po dei pellegrini , via boezio 19 , 80124 napoli , italy 2 sezione di radiologia , dipartimento magrassa - lanzara , seconda universit di napoli , napoli , italy 3 ii clinica neurologica , seconda universit di napoli , napoli , italy correspondence to : s . 
vus can be integrated into the diagnostic protocol for evaluating swallowing in patients with als , as it has higher sensitivity than vfs in assessing the dynamic factors that represent the early signs of dysphagia . keywords dysphagia amyotrophic lateral sclerosis ultrasound videofluoroscopy riassunto obiettivo . 
lecovideografia pu essere integrata nel protocollo diagnostico dello studio della deglutizione nei pazienti con sla grazie alla maggiore sensibilit rispetto alla vfs nel valutare i reperti dinamici che rappresentano segni precoci di disfagia . parole chiave disfagia sclerosi laterale amiotrofica ecografia videofluoroscopia radiol med ( 2010 ) 115 : 784793 introduction in patients with amyotrophic lateral sclerosis ( als ) , or lou gehrigs disease , dysphagia is caused by degeneration of bulbar motor neurons and mainly involves difficulty initiating the voluntary oral phase of deglutition [ 1 , 2 ]  . 
assessing dysphagia in patients affected by als relies on a multidisciplinary approach involving neurologists , gastroenterologists , speech therapists that aims at evaluating the symptoms and signs of dysphagia and providing indications for treatment . despite the poor prognosis of als , it is possible to control dysphagia by adequately modifying the diet and adopting postural compensation manoeuvres to maintain oral feeding and defer the need for percutaneous endoscopic gastrostomy ( peg ) for as long as possible [ 37 ]  . radiologists and the aerodigestive the swallowing act is divided into three successive phases : the oral ( preparatory and propulsive ) phase , the pharyngeal phase ( oropharyngeal and hypopharyngeal ) and the oesophageal phase ( cervical and thoracoabdominal ) , all of which are functionally related and interdependent [ 2 ]  . 
videofluoroscopy ( vfs ) consists in videorecording fluoroscopic images obtained during ingestion of a barium sulphate suspension and allows morphological , dimensional and dynamic evaluation of bolus passage through tract . 
however , although excellent for depicting the pharyngeal and oesophageal phases , vfs is limited in the study of the oral phase , as it is unable to evaluate the muscular structure of the tongue and floor of the mouth [ 2 , 7 , 911 ]  . 
were the first to suggest the use of video ultrasonography ( vus ) for documenting tongue motility , hyoid elevation and formation and appearance of the lingual bolus [ 12 ]  . 
the aim of our study was to determine the role of vus in diagnostic assessment of dysphagic patients with als . introduzione la disfagia , difficolt a deglutire alimenti solidi o liquidi , nei pazienti con sclerosi laterale amiotrofica ( sla ) , o malattia di lou gehrig , causata dalla degenerazione dei neuroni motori bulbari e trova la sua causa principale nella difficolt nel dare avvio alla fase orale , volontaria , della deglutizione [ 1 , 2 ]  . 
la valutazione del paziente disfagico affetto da sla si avvantaggia di un approccio multidisciplinare , con il coinvolgimento del neurologo , del gastroenterologo , del radiologo e del logopedista , al fine di valutare la sintomatologia disfagica e fornire lindicazione terapeutica . malgrado la prognosi infausta della malattia , possibile arginare il disturbo disfagico modificando adeguatamente la dieta e adottando manovre di compenso della postura al fine di mantenere il pi a lungo possibile lalimentazione orale e ritardare il ricorso alla gastrostomia endoscopica percutanea ( peg ) [ 37 ]  . la funzione deglutitoria viene suddivisa in tre fasi cronologicamente successive : fase orale ( preparatoria e di trasporto ) , fase faringea ( oroed ipofaringea ) e fase esofagea ( cervicale e toraco - addominale ) tra loro funzionalmente correlate ed interdipendenti [ 2 ]  . 
tuttavia la vfs , mentre risulta ottimale per la documentazione delle fasi faringea ed esofagea , non consente uno studio ottimale della fase orale , non potendo valutare la struttura muscolare della lingua e del pavimento buccale [ 2 , 7 , 911 ]  . 
 [ 12 ] proposero per primi limpiego della registrazione ecovideografica ( evg ) nella documentazione della motilit linguale , della risalita dellosso ioide , della modalit di formazione e dellaspetto del bolo linguale [ 12 ]  . 
scopo del nostro lavoro stabilire quale ruolo abbia levg nel protocollo diagnostico dei pazienti disfagici affetti da sla . materials and methods patients materiali e metodi pazienti this study , approved by the ethics committee , was conducted over 12 months ( january - december 2008 ) in cooperation with the referral centre for motor neuron diseases , which follows approximately 70 als patients lo studio , approvato dalla commissione etica , ha avuto una durata di 12 mesi ( gennaio - dicembre 2008 ) ed stato svolto in collaborazione con il centro di riferimento per le malattie dei motoneuroni che segue annualmente circa 70 pazienti con sla . 
of these 35 patients , nine ( m : f = 5 : 4 ) , aged 3376 ( mean 60 ) years , underwent simultaneous vus to complement the vfs study . 
disease duration ranged from 6 to 33 ( mean 15 ) months , and the average time between initial als symptoms and the diagnostic study was 16 months . ultrasound system and technique vus was carried out with a profocus system ( b - k medical ) equipped with a 5 - mhz microconvex probe ( type 8803 ) and direct video - capturing software featuring 25 frames / s , possibility of slowing down the frame rate to 1 / 30 of normal speed , and possibility of obtaining freezeframe shots . 
longitudinal and transverse scans were performed through the submental acoustic window , with the patient in a seated position . transverse evaluation of the oral cavity was performed with the microconvex transducer placed in the cavity of the thyroid cartilage . 
each patient was administered three water boluses ( 5 , 10 , and 15 ml ) and instructed to hold the bolus in the mouth until told to swallow . ultrasound evaluation criteria during swallowing of the water boluses ( 5 , 10 and 15 ml ) , the oral phase of deglutition was considered to be physiological when : 1 . 
dei 35 pazienti sottoposti a vfs , 9 ( m : f = 5 : 4 ) , di et compresa tra 33 ed 76 anni ( media 60 anni ) previo consenso informato , sono stati sottoposti contestualmente ad integrazione con esame evg della deglutizione . 
dei 9 pazienti sottoposti ad esame evg , 5 presentavano sla con forma classica , cio con coesistenza del coinvolgimento del primo e del secondo neurone di moto , 4 presentavano forma bulbare , cio con segni e sintomi confinati al distretto bulbare . 
clinicamente 8 erano disfagici ; lepoca di esordio della malattia variava da 6 a 33 mesi ( media 15 mesi ) , il tempo medio trascorso tra comparsa dei primi sintomi di sla ed esame strumentale era di 16 mesi . 
 apparecchiatura e tecnica ecografica stato usato un ecografo b - k medical ultrasound system profocus con sonda da 5 mhz di tipo microconvex ( type 8803 ) e software di video - acquisizione diretta con le seguenti caratteristiche : 25 immagini / s , velocit di scorrimento dimmagine rallentabile fino a 1 / 30 della velocit normale , possibilit di fermo immagine . 
ad ogni paziente sono stati somministrati 3 boli di acqua ( 5 , 10 , 15 ml ) con listruzione di tenerla in bocca e poi di deglutire al comando . 
a bolo ( c ) tra lingua ( a ) e palato duro ( b , linea iperecogena ) ; b della fase propulsiva : addossamento della punta ( * ) della lingua al palato duro ed avvallamento del dorso ( ^ ) della lingua ; c propulsione posteriore del bolo ; d ritorno alla posizione di riposo . the biphasic technique , which studies the static ( morphological ) and dynamic ( propulsive ) components . 
during the static phase , we examined tongue atrophy , abnormal bolus position ( below the tongue , dipper swallow ) and inability to retain the bolus inside the oral cavity . 
during the dynamic phase , we assessed reduced ( less lowering of back of tongue ) or disorganised ( no appreciable lowering ) tongue movement , fragmented swallowing ( bolus swallowed in more than one swallowing act ) and pooling of ingested material ( pooling of contrast agent even after two swallows )  . videofluoroscopy system and technique condotta con tecnica bifasica che valuta la componente statica ( morfologica ) e dinamica ( propulsiva )  . 
nella fase statica sono stati esaminati latrofia della muscolatura linguale , lanomala disposizione del bolo ( sotto la punta della lingua ) , lincapacit a trattenere il bolo nella cavit orale . 
nella fase dinamica sono stati valutati per ognuno dei boli di acqua : il movimento linguale ridotto ( ridotto avvallamento del dorso della lingua ) o disorganizzato ( senza avvallamento apprezzabile ) , la deglutizione frammentaria ( bolo deglutito in pi atti ) , il ristagno degli ingesti ( ristagno di mezzo di contrasto [ mdc ] anche dopo due atti )  . 
 apparecchiatura e tecnica videofluoroscopica we used a dyno compact computerised system ( menfis biomedica s.r.l. , bologna , italy ) equipped with : ( 1 ) graphics stato impiegato il sistema computerizzato dyno compact ( menfis biomedica srl , bologna , italia ) dotato di : 1 . scheda grafica per la gestione di immagini ecografiche o 788 radiol med ( 2010 ) 115 : 784793 card for managing sonographic or radiographic images ; ( 2 ) a.vi.u.s. 
dedicated software , which enables digital - quality recording ( pal / ntsc , composite video or s - video ) of the vfs study in avi format with 320240 resolution and 25hz acquisition frequency . 
following acquisition , the video can be analysed during real - time reproduction at reduced or increased speed , or it can be paused for a frame - by - frame analysis [ 7 ]  . vfs begins with a unenhanced , baseline assessment of vocal cord and soft palate motility . 
the examination was videorecorded in the anteroposterior and laterolateral view and subsequently reviewed frame by frame . criteria for videofluoroscopic assessment the preparatory phase of vfs was compared with static vus , whereas the propulsive phase of vfs was compared with dynamic vus . 
during the propulsive phase , we assessed for reduced or disorganised tongue movement , fragmented swallowing and pooling of ingested material ( table 1 )  . results analysis of the static phase was based on three sonographic and two videofluoroscopic parameters ( table 1 )  . 
reduced tongue movement was detected in 5 / 9 patients at vus , even with the smallest amount of water ( 5 ml ) , and in 2 / 9 at vfs . 
disorganised tongue movement was observed in 3 / 9 patients at vus ( in two patients with 15 ml of water and in one with 10 ml ) and in 2 / 9 at vfs . 
software dedicato , attraverso il quale possibile registrare in qualit digitale ( pal / ntsc , video composito o svideo ) la vfs , in filmati avi con risoluzione 320240 e con frequenza di acquisizione di 25 hz ; il ritardo introdotto dal processo di digitalizzazione dellimmagine dellordine dei 200 ms . 
una volta acquisito lo studio , lanalisi pu essere effettuata in riproduzione tempo reale , a velocit ridotta o aumentata ; inoltre possibile lanalisi frame per frame mediante messa in pausa degli specifici frames di interesse [ 7 ]  . lesame vfs inizia con una valutazione di base ( senza mdc ) per lo studio della motilit delle corde vocali e del palato molle . 
per lindagine vfs stato utilizzato come mezzo di contrasto una sospensione baritata ( prontobario hd , bracco spa , milano , italia ) in 65 cc di acqua , con paziente in ortostatismo , salvo casi in cui la compromissione della funzione statica dei pazienti ha reso necessaria lacquisizione dellesame in posizione seduta . 
per motivi radioprotezionistici sono stati somministrati boli di mdc , in quantit ottimizzate in relazione alla compliance del paziente ( o 5 , o 10 , o 15 ml )  . 
lesame stato poi rivalutato mediante analisi frame by frame . criteri di valutazione videofluoroscopica la fase preparatoria della vfs stata correlata alla fase statica dello studio ecografico , mentre la fase di trasporto della vfs stata correlata allo studio dinamico dellevg . nella fase preparatoria stata valutata la disposizione del bolo , lincapacit del paziente di trattenere il bolo nella bocca . 
nella fase di trasporto sono stati valutati il movimento linguale ridotto o disorganizzato , la presenza di deglutizione frammentaria , il ristagno degli ingesti ( tabella 1 )  . risultati la valutazione della fase statica ha considerato 3 parametri ecografici e 2 videofluoroscopici ( tabella 1 )  . 
la disorganizzazione del movimento linguale stata osservata in 3 / 9 pazienti allevg ( in 2 pazienti per 15 ml di acqua e in 1 per 10 ml ) e in 2 / 9 alla vfs . 
la deglutizione frammentaria radiol med ( 2010 ) 115 : 784793 table 1 videoultrasonographic ( vus ) and videofluoroscopic ( vfs ) static and dynamic parameters patients patients atrophy of tongue muscles static study bolus position bolus position inability to retain bolus in oral cavity inability to retain bolus in oral cavity dynamic study tongue movement tongue movement disorganised tongue movement disorganised tongue movement fragmented swallow fragmented swallow pooling of ingested material pooling of ingested material normal abnormal 3 normal reduced yes normal ( tipper swallow ) abnormal ( dipper swallow ) normal reduced ( 5 ml , 10 ml 15 ml ) 5 ( 5 ml ) yes ( 5 ml , 10 ml , 15 ml ) 3 ( 2 at 15 ml , 1 at 10 ml ) yes ( 5 ml , 10 ml , 15 ml ) 4 ( 2 at 15 ml , 2 at 10 ml ) yes water and in two with 10 ml . 
as a vus contrast agent , we used only progressive amounts of water ( from 5 to 15 ml ) , which we found to provide excellent visualisation , which is in contrast to other authors who preferred to use a cola beverage [ 17 ]  . levg si dimostrata unindagine utile per la valutazione morfologica e funzionale della lingua [ 2 ] , fornendo informazioni sulle iniziali alterazioni dei fattori statici e dinamici della fase orale della deglutizione . 
per levg abbiamo utilizzato come mdc solo dosi crescenti di acqua da 5 a 15 ml , ottenendone unottima visualizzazione , bench altri autori abbiano utilizzato la cola , ritenendola migliore [ 17 ]  . 
la ripetibilit 790 radiol med ( 2010 ) 115 : 784793 tabella 1 parametri statici e dinamici ecovideografici / videofluoroscopici pazienti pazienti studio statico disposizionie del bolo atrofia della muscolatura linguale disposizione del bolo incapacit di trattenere il bolo in cavit orale incapacit di trattenere il bolo in cavit orale studio dinamico movimento linguale movimento linguale movimento linguale disorganizzato movimento linguale disorganizzato deglutizione frammentaria deglutizione frammentaria ristagno degli ingesti ristagno degli ingesti normale anormale 3 normale ridotto normale ( sulla punta della lingua ) anormale ( sotto la punta della lingua ) normal reduced ( 5 ml , 10 ml 15 ml ) 5 ( 5 ml ) 3 ( 2 15 ml , 1 10 ml ) 4 ( 2 15 ml , 2 10 ml ) s ( 5 ml , 10 ml , 15 ml ) s ( 5 ml , 10 ml , 15 ml ) repeatability of the examination during the same session with progressive amounts of water and during follow - up and rehabilitation is ensured by the lack of ionising radiation . static evaluation is based on three parameters : tongue atrophy , bolus position and inability to retain the bolus inside the oral cavity . 
in our study , tongue atrophy , which was only measured subjectively , was always associated with at least one of the dynamic abnormalities , supporting the link between dynamic and morphological factors . 
according to several authors [ 15 ] , a bolus position below the tongue ( dipper swallow ) is rare in the normal population in the absence of dynamic abnormalities . 
in fact , although observed in only one patient with dynamic abnormalities , a bolus position below the tongue was constantly associated with reduced tongue movement or fragmented swallowing in all cases . 
the performance of vus in identifying patients unable to retain the bolus dellesame intesa non solo nella stessa seduta per dosi crescenti di mdc , ma anche nel follow - up durante la riabilitazione , possibile poich non vengono utilizzate radiazioni ionizzanti . la valutazione statica dellevg prende in considerazione tre parametri : latrofia linguale , la disposizione del bolo e lincapacit di trattenere il bolo nella cavit orale . 
nel nostro studio latrofia linguale , valutata sulla base di un criterio puramente soggettivo , risultata sempre associata ad almeno una delle alterazioni di tipo dinamico , evidenziando quindi il legame tra il fattore dinamico e quello morfologico . 
infatti bench tale reperto sia stato osservato in un solo paziente in assenza di alterazioni dinamiche , in tutti gli altri casi la disposizione del bolo al di sotto della punta della lingua risultata sempre associata a movimento linguale ridotto o a deglutizione frammentaria . 
a disposizione del bolo sotto la punta della lingua ; b movimento linguale ridotto con mancato avvallamento del dorso della lingua ; c disorganizzazione linguale nellazione propulsiva ; d ritorno alla posizione di riposo . inside the mouth was almost equal to that of vfs , and both techniques depicted anterior bolus loss as a positive imaging sign . dynamic evaluation is based on four parameters : reduced or disorganised tongue movement , fragmented swallowing and pooling of ingested material . 
reduced and / or disorganised tongue movement is correlated with abnormal lowering of the back of the tongue during bolus formation , leading to a failure to model the bolus [ 2 ]  . 
furthermore , fragmented swallowing was always associated with reduced tongue movement . pooling of ingested material inside the oral vestibule was visualised at vfs only due to the inability of ultrasound to penetrate bone ; however , the same patients has positive findings on vus , with evidence of trophic or functional abnormalities . capacit dellevg nel definire i pazienti con incapacit nel trattenere il bolo nella cavit orale risultata sovrapponibile alla vfs , entrambe le metodiche hanno come segno positivo per limaging la perdita anteriore del bolo . nella valutazione dinamica sono stati considerati quattro parametri : il movimento linguale ridotto o disorganizzato , la deglutizione frammentaria ed il ristagno degli ingesti . 
il movimento linguale ridotto e / o disorganizzato sono correlati allalterazione del normale avvallamento del dorso linguale durante la formazione del bolo , con conseguente non modellamento del bolo stesso [ 2 ] ; tale reperto potrebbe rappresentare il primum movens delle alterazioni della fase orale della deglutizione . 
inoltre , la deglutizione frammentaria risultata sempre associata a ridotta motilit linguale.il ristagno degli ingesti a livello del vestibolo stato visualizzato solo con la vfs a causa dellincapacit degli ultrasuoni di attraversare le strutture ossee , tuttavia negli stessi 792 radiol med ( 2010 ) 115 : 784793 all abnormalities observed , whether static or dynamic , reflected injury to the nervous system involving abnormalities in swallowing reflex or motor nerve supply mainly from the seventh and twelfth cranial nerves [ 2 ]  . the main limitations of our study are the small number of patients examined , which were nonetheless 26% of all als patients referred for swallowing investigations , the use of a fluid contrast agent for both vus and vfs and the impossibility of evaluating pharyngeal and oesophageal phases with vus . comparison with vfs findings shows that the ability of vus to demonstrate tongue atrophy may have no implication for clinical - therapeutic management , as this is a late finding that may only be useful in patients who had not previously undergone vfs . 
in contrast , a more significant result of vus was the ability to identify patients with abnormal bolus position below the tongue in static evaluation in that this was constantly associated with other dynamic abnormalities . 
the role of vus in evaluating dysphagic als patients is to provide an earlier and more sensitive detection of dynamic abnormalities of the oral phase compared vfs , in particular , as concerns reduced or disorganised tongue movement and fragmented swallowing . 
the use of vus in evaluating dysphagic als patients is proposed on the basis that it can be performed at the patients beside ; it is repeatable , as it does not use ionising radiation ; it is able to depict reflex swallowing in poorly cooperating patients unable to undergo vfs ; and it permits dysphagia to be evaluated with progressive amounts of contrast material ( water ) and without additional costs . conclusions vus of the tongue is complementary to vfs , as it provides accurate depiction of the oral phase of swallowing [ 2 ]  . biphasic vus provides a static / morphological evaluation of the oral cavity and real - time assessment of the mechanisms of bolus formation and propulsion . 
vus can be added to the diagnostic protocol to evaluate swallowing in patients with als either before or at the same time as vfs , thanks to its greater sensitivity in evaluating dynamic factors that represent early signs of dysphagia . 
moreover , the use of vus in evaluating dysphagia in als is proposed on the grounds that it can be performed at the patients bedside and is able to demonstrate reflex swallowing in uncooperative patients . pazienti levg stata comunque positiva mostrando alterazioni trofiche o funzionali . le alterazioni da noi osservate , sia statiche che dinamiche , sono espressione di lesioni del sistema nervoso che comportano alterazione del riflesso deglutitorio o dellinnervazione motoria prevalentemente sotto il dominio del vii e xii paio di nervi cranici [ 2 ]  . fra i limiti del nostro studio , sottolineiamo il basso numero di pazienti esaminati , malgrado rappresentino il 26% dei pazienti con sla sottoposti ad uno studio per imaging della deglutizione , luso di mdc solo liquido sia per levg che per la vfs , limpossibilit di valutare con levg la fase faringea e quella esofagea . dal confronto con i dati ottenuti alla vfs si evince che la capacit dellevg di evidenziare latrofia linguale pu non avere risvolti clinico - terapeutici in quanto un reperto tardivo , pu essere utile solo nei pazienti che non hanno eseguito precedentemente un esame vfs . 
pi significativa nella valutazione statica allevg invece la capacit di individuare i pazienti con disposizione anomala del bolo sotto la punta della lingua in quanto sempre associato ad altre alterazioni di tipo dinamico . 
il vero ruolo dellevg nella valutazione dei pazienti disfagici con sla quello di individuare precocemente e con maggiore sensibilit rispetto alla vfs le alterazioni dinamiche della fase orale della deglutizione , in particolare il movimento linguale ridotto o disorganizzato e la deglutizione frammentaria . 
lutilizzo dellevg nella valutazione della disfagia dei pazienti con sla pu essere proposto per la possibilit di eseguire lesame al letto del paziente , per la sua ripetibilit non utilizzando radiazioni ionizzanti , per la possibilit di documentare una deglutizione riflessa nei pazienti non collaboranti per la vfs , per valutare senza costi aggiuntivi la disfagia con dosi crescenti di mdc ( acqua )  . conclusioni lo studio evg della lingua un esame complementare allo studio radiologico permettendo una documentazione accurata della cinetica della fase orale [ 2 ]  . 
lecografia bifasica inoltre , consente di effettuare una valutazione statica / morfologica del cavo orale e di seguire in real - time i meccanismi di formazione e propulsione del bolo . 
lutilizzo dellevg pu essere integrato nel protocollo diagnostico dello studio della deglutizione dei pazienti con sla , se non precedentemente almeno contestualmente allesame vfs , grazie alla maggiore sensibilit nel valutare i reperti dinamici che rappresentano i segni precoci di disfagia . 
bucci3 1unit of radiotherapy , 2unit of general surgery , 3unit of medical oncology , multimedica clinical institute , viale piemonte 70 , 21053 castellanza , italy correspondence to : g . 
water equivalence of the gel was verified by comparing the gels computed tomography ( ct ) number [ hounsfield units ( hu ) ] and density with the corresponding values for water and another commercial bolus device . 
thus , it is recommendable as a practical tool for most irregular sites . further investigations are warranted to validate this solution in more complex irradiation techniques . keywords electron bolus skin irradiation external ear radiotherapy riassunto obiettivo . 
lequivalenza del gel rispetto allacqua stata verificata confrontando il numero di tomografia computerizzata ( ct , unit hounsfield , hu ) e la sua densit con i rispettivi valori dellacqua e di un altro bolus prodotto commercialmente . 
pertanto , sembra uno strumento raccomandabile in molte sedi irregolari ; sono comunque necessarie ulteriori esperienze per 976 radiol med ( 2010 ) 115 : 975982 confermarne la validit con tecniche di irradiazione pi complesse . parole chiave bolus per elettroni irradiazione cutanea radioterapia dellorecchio esterno introduction introduzione in skin cancer , radiation therapy is usually performed in the case of large lesions where surgical resection would cause poor cosmetic results or in the case of surgical contraindications . 
to compensate for patient contour irregularities or the presence of missing tissue , for example due to surgical defects , the use of beam modification devices is standard . tissue - equivalent materials have been used to produce a flat surface . 
as is known , whenever compensators are used , it is always important to consider their density , because the thickness of high - density materials significantly affects beam attenuation and absorbed dose . therefore , low - density materials are preferred when the purpose is to compensate for missing tissue . as far as electrons are concerned , beam energy is usually selected to ensure that the deepest part of the lesion is effectively irradiated with a clinically significant dose while sparing healthy tissues within the field . 
as a consequence , the bolus must conform as much as possible to the curvature of patients skin surface . commonly used materials include various home - made mixtures of water , glycerine and gelatine , or commercial synthetic gels with a density very close to that of water [ 5 ]  . clearly , the ideal bolus material should be tissueor lirradiazione delle neoplasie cutanee generalmente eseguita in caso di lesioni estese , dove la resezione chirurgica causerebbe risultati cosmetici deludenti , o in caso di controindicazioni chirurgiche . 
in passato , neoplasie di dimensioni limitate erano trattate in modo efficace con fotoni di bassa energia , mentre gli elettroni erano generalmente preferiti per lesioni estese , situate su superfici piane e regolari . 
attualmente , specie su superfici curve ed irregolari , possibile eseguire trattamenti adeguati con tecniche di brachiterapia interstiziale , mentre gli elettroni continuano a rappresentare la metodica alternativa di elezione . 
in particolare , per una definita profondit , la dose di radiazioni effettivamente assorbita pu essere minore o maggiore a seconda che il fascio incidente attraversi rispettivamente una maggiore o minore quantit di tessuto , risultando pi o meno attenuata . per compensare leventuale irregolarit del profilo del paziente o in caso di difetti consistenti di tessuto , legati per esempio a esiti chirurgici , sono generalmente impiegati dei dispositivi di compensazione del fascio . 
materiali con densit acqua - equivalente , come la cera e la paraffina , sono utilizzati allo scopo di ottenere una superficie piatta , nellarea della incidenza del fascio [ 14 ]  . 
tutte le volte che si utilizzano compensatori del fascio importante considerarne la densit , poich lutilizzo di materiali ad elevate densit pu incidere in maniera significativa sulla attenuazione del fascio e , conseguentemente , sulla dose assorbita . 
pertanto , nei casi in cui lobiettivo primario la compensazione di perdita di tessuto , sono preferiti materiali a bassa densit . per quanto riguarda lirradiazione con elettroni , lenergia del fascio scelta in fase di elaborazione del trattamento allo scopo di garantire che la porzione pi profonda del bersaglio sia adeguatamente irradiata ; nel contempo , le strutture sane allinterno del campo di irradiazione devono essere risparmiate . 
conseguentemente , il bolus deve adattarsi quanto pi possibile alle irregolarit del profilo del paziente . materiali comunemente utilizzati sono rappresentati da varie miscele artigianali di acqua , glicerina , in forma gelatinosa ; radiol med ( 2010 ) 115 : 975982 water - equivalent and adequately pliable so as to conform to body contour irregularity and not deform the patients profile . 
finally , it should be cheap as well as easy , and quick to prepare and apply during each irradiation schedule . materials and methods we describe a very easy solution for irradiation of a complex surface such as the external ear by using ultrasound ( us ) transmission gel to compensate for shape irregularities of the concha and external auditory canal in the context of fractionated postoperative electron beam irradiation of a skin cancer ( merkel cell carcinoma )  . in this clinical setting , the radiotherapy target volume was the entire ear auricle , with specific indication for complete inclusion of the helix edge and with particular attention to avoid underdosing the most superficial layers of the skin due to tissue penetration . 
as is usual in conventional electron beam irradiation , the source - to - skin distance was 110 c treatment planning was based on conventional percentage depth dose tables , as the computerised treatment planning system ( pinnacle3 , philips medical system , madison wi , usa ) was not commissioned to calculate electron beam dose . nevertheless , a planning computed tomography ( ct ) scan was performed with the patient in the treatment position , and electron energy was chosen on the basis of helix thickness . 
chemical components of the gel were demineralised deionised water , carbomer as a thickening agent , ethylenediaminetetraacetate ( edta ) as a complexing agent , sodium hydroxide as a neutralising agent and methylisothiazolinone / methylchloroisothiazolinone as a preservative . 
infine , esso dovrebbe essere sufficientemente economico , semplice e veloce nella sua preparazione e posizionamento durante ciascuna sessione giornaliera di trattamento . materiali e metodi si descrive una semplice soluzione per la irradiazione di una superficie irregolare come lorecchio esterno , utilizzando gel ecografico come compensatore delle irregolarit di profilo del padiglione auricolare e del canale uditivo esterno , nel contesto di un trattamento post - operatorio , eseguito con elettroni , di una neoplasia cutanea ( carcinoma a cellule di merkel )  . in questa specifica situazione clinica si considerato come volume bersaglio del trattamento lintero padiglione auricolare , con la specifica indicazione alla completa inclusione dellelice e con particolare attenzione ad evitare il sottodosaggio degli strati pi superficiali della cute , dovuto alla penetrazione del fascio . 
come di consueto nelle irradiazioni con elettroni , la distanza sorgente - cute stata di 110 cla pianificazione del trattamento ( planning ) stata eseguita mediante le convenzionali tabelle di trasmissione della dose in profondit , poich il sistema computerizzato di elaborazione generalmente utilizzato per la pianificazione dei trattamenti ( pinnacle3 , philips medical system , madison wi , usa ) non impostato per la dosimetria con fasci di elettroni . ciononostante , stata eseguita una tomografia computerizzata ( tc ) di pianificazione , con il paziente in posizione di trattamento , e la energia del fascio di elettroni stata selezionata in relazione allo spessore misurato dellelice . 
i componenti del gel sono : acqua demineralizzata e deionizzata , carbomero come agente consolidante , acido etilendiamminotetraacetico ( edta ) come agente complessante , idrossido di sodio come neutralizzante , addizionato con un conservante ( metilsotiazolinone / metilcloroiosotiazolinone )  . 
ciononostante , limpatto del gel sulla attenuazione del fascio stato estrapolato attraverso la misura del numero tc ( in unit hounsfield , hu ) e della densit ( g / cm3 ) del gel e attraverso il confronto di questi valori con i rispettivi valori di acqua e di un altro tipo di bolus di comune utilizzo . i numeri tc derivano da una specifica tabella di correlazione con le densit dei tessuti , che generalmente definita durante il commissioning ( la installazione ) del tps , allo scopo di considerare la attenuazione del fascio nei tessuti . 
pertanto , stata eseguita una ulteriore scansione tc con una quantit nota di gel , e il numero tc del gel ecografico stato confrontato con i rispettivi valori , relativi alla stessa quantit di acqua e di un sistema bolus prodotto commercialmente ( superflab )  . 
nevertheless , the impact of the us gel on dose attenuation was extrapolated from its ct number in hu and its density ( g / cm3 ) and from the comparison of these values with the corresponding values for water and another commonly used bolus device . ct numbers derive from a ct number - density correlation table , which is usually defined during commissioning risultati fig . 
2a , b tomografia computerizzata pre - trattamento e ricostruzione tridimensionale della sede di trattamento con : a gel ecografico ; b calco personalizzato con alginato . radiol med ( 2010 ) 115 : 975982 of the treatment planning system , to consider beam attenuation within tissues . 
thus , a second ct scan with a predefined volume of us gel was performed , and the ct number of the gel was compared with corresponding values of a similar amount of water and a commercial bolus device ( superflab )  . 
 results a dose of 54 gy in 27 daily fractions of 1.8 gy was delivered over a 44 - day treatment time ; treatment was well tolerated , with low acute skin toxicity . 
prolongation of daily treatment time was negligible , with only few minutes added to the usual setup due to placement of the gauze and filling of the concha . with regard to evaluation of the gel relative to other materials , comparison of the ct number showed that both us gel and water had a comparable attenuation value , with an hu value of 0 for both . 
exploring these possibilities , we also tested an alternative setup to compensate for the irregular contours of the auricle , and in particular , an alginatebased mould shaped on the ear . 
one possibility would have been be pour water into the patients ear auricle , as described elsewhere [ 6 ] ; however , although effective , water would probably have been unstable , with a risk of leaking out of the ear during couch movements . 
furthermore , it was giornaliere da 1 , 8 gy , in un tempo complessivo di 44 giorni ; clinicamente , il trattamento stato , nel complesso , ben tollerato , con comparsa di tossicit cutanea di lieve intensit ( grado 2 , secondo i criteri di tossicit acuta radiation therapy oncology group , rtog )  . 
il sistema di compensazione utilizzato risultato semplice , veloce e ben tollerato dal paziente e con un buon grado di accettazione , in termini di semplicit di preparazione e velocit di applicazione , da parte degli operatori . 
laumento del tempo richiesto a ciascuna frazione di trattamento stato trascurabile , con un prolungamento di pochi minuti al consueto set - up , dovuto al posizionamento della garza ed al riempimento del padiglione auricolare con il gel . per quanto concerne la valutazione del gel rispetto ad altri materiali , dal confronto dei numeri tc emerge come sia il gel che lacqua abbiano confermato un analogo potere di attenuazione del fascio , con un valute di hu di 0 per entrambi ; per contro , il valore corrispondente al sistema commerciale stato , anche se di poco , superiore , con un valore di hu di 80 . 
a questi valori tc corrisponde una densit rispettivamente di 1 g / cm3 per lacqua e il gel ecografico ; per quanto riguarda il bolus commerciale la densit certificata dal produttore di 1 , 02 g / cm3 , per fasci radiazioni a energie terapeutiche . discussione il metodo proposto pu essere considerato come una soluzione facilmente applicabile per ottenere una efficace compensazione di superfici irregolari . 
inizialmente , era stata infatti immaginata una possibilit di set - up alternativa per compensare i contorni irregolari del padiglione auricolare , ed era stato allestito un calco in alginato , conformato sullorecchio . 
sfortunatamente , per questo tipo di soluzione sono emerse delle limitazioni ; la densit del calco si rivelata troppo elevata ( 1 , 12 g / cm3 ) , incidendo sulla dose assorbita sottostante . 
in questo senso , una possibilit aveva immaginato di introdurre nel padiglione una quantit dacqua sufficiente a riempirlo completamente , come del resto gi descritto in altre esperienze [ 6 ] ; anche in questo caso sono emersi dei limiti in quanto lacqua colava facilmente dallorecchio , durante le manovre di applicazione o a seguito di piccoli movimenti , senza considerare il possibile disagio per il paziente . nel tentativo di cercare un altro materiale , il gel ecografico sembra quindi rappresentare la soluzione pi appropriata : economico , facile da applicare , pi resistente dellacqua alla gravit e ben adattabile ai contorni del padiglione auricolare . 
per ultimo , un materiale del tutto acquaequivalente . 980 radiol med ( 2010 ) 115 : 975982 considered less comfortable for the patient . among other possible materials , us transmission gel was considered to best fulfil the requirements : it was cheap , easy to apply , more resistant to gravity and highly adaptable to the auricle contours . 
additionally , its hu value is water equivalent . although economic aspects did not constitute specific end points of our investigation , which was limited to the practical advantages of us gel over other devices , it should be kept in mind that commercial bolus sheets may be expensive ( ranging from 100 to 300 euro , depending on dimensions ) and are subject to deterioration . 
they also applied water as an effective bolus compensator in ear electron - beam irradiation , achieving a more homogeneous dose distribution and a reported maximum dose reduction of 25% compared with similar treatments delivered without compensation systems [ 6 ]  . interestingly , the authors reported a remaining dose increase , mainly due to scatter off the protruding helix and tragus , and claimed to reduce it by flattening the ear . although not experimentally proved , it is likely that the same improvement in homogeneity might be achieved by filling with the entire concha with water and not only the ear canal , as described . 
with this tool , the authors claimed to obtain a better than 90% isodose conformation to the planning target volume , especially in patients with irregular body contours or surgical defects [ 8 , 9 ]  . the importance of bolus appropriateness in electron beam irradiation is highly topical if we consider a recent report from australia , where authors simulated a perturbation of the dose distribution due to air gaps between bolus and body contours . 
a very accurate dosimetry by means of a water phantom with an electron diode allowed a close correlation to be demonstrated between central axis depth dose distribution and beam energy , field size , bolus thickness and air gap size . 
hanno descritto luso del bolus come compensatore in caso di aree soggette a perdita di tessuto [ 7 ] ; in aggiunta , hanno utilizzato lacqua come un efficace metodo di compensazione per lirradiazione con elettroni dellorecchio esterno , riportando una maggiore omogeneit della distribuzione della dose , ed una riduzione della dose massima del 25% , rispetto ad analoghi trattamenti in assenza dei sistemi di compensazione [ 6 ]  . 
 interessante notare che gli autori riferiscono una persistenza di aree con un sovradosaggio indesiderato , prevalentemente dovuto alla diffusione della dose intorno alle strutture pi irregolari come lelice ed il trago , e ipotizzano , un possibile miglioramento in tale senso con lappiattimento di queste aree pi prominenti . 
anche se non provato , possibile che un effetto analogo possa essere ottenuto riempiendo di acqua non solo il canale anale ( come descritto nello studio citato ) , ma tutto il padiglione auricolare . 
pi recentemente , lo stesso gruppo ha riportato i risultati dosimetrici di irradiazioni pi complesse , eseguite attraverso la preparazione di compensatori di cera , personalizzati e conformati con lausilio di specifiche apparecchiature . 
con questi dispositivi , sono riportate migliori distribuzioni di dose , con maggiore conformazione della isodose del 90% al planning target volume , specialmente in pazienti con profili corporei irregolari o perdite di tessuto meta chirurgiche [ 8 , 9 ]  . limportanza di un corretto utilizzo del bolus nella irradiazione con elettroni sembra comunque estremamente attuale , se si considerano i risultati di una recente esperienza , dove gli autori hanno simulato le alterazioni della distribuzione di dose , dovute alle bolle daria presenti tra il bolus e il corpo del paziente . 
in tal senso , stata condotta una dosimetria estremamente accurata , mediante fantoccio ad acqua e dosimetri a diodo , che ha confermato la presenza di una stretta correlazione tra la distribuzione di dose sullasse centrale del fascio e , rispettivamente , lenergia del fascio , lestensione del campo di irradiazione , lo spessore del bolus utilizzato e lampiezza delle bolle daria eventualmente presenti , che gli autori raccomandano di evitare per quanto possibile [ 10 ]  . queste esperienze , condotte con controlli di qualit molto rigidi , rafforzano limportanza di una appropriata conformazione dei bolus utilizzati ai profili irregolari del corpo del paziente , situazione non sempre ottenibile con i sistemi commerciali disponibili ; daltro canto , non in tutte le radiol med ( 2010 ) 115 : 975982 achievable with standard commercial devices . 
per tali motivi , una soluzione intermedia che concili una preparazione semplice , un posizionamento pratico , una buona conformazione al profilo corporeo e una equivalenza allacqua , pu verosimilmente trovare una efficace applicabilit . conclusions conclusioni us transmission gel is a simple , quick and cheap tool to provide satisfactory compensation in electron beam irradiation of irregular surfaces . 
its greatest advantage is the absolute adaptability to most sites , whereas other standard bolus devices may be difficult to place in small anatomical cavities , such as skin folds or tissue defects after surgical intervention . 
 from this limited experience , it is not possible to advocate the use of this tool for photon - beam irradiation , but there appears to be no reason to preclude the use of the gel in these cases . 
furthermore , although our report refers to a very simple irradiation technique , no limitations seem to exist to investigate the use of the gel , even in more complex techniques , such as three - dimensional conformal irradiation or intensity - modulated radiotherapy , provided that more stringent quality assurance programmes and more precise dosimetry are ensured , which are indispensable for a wider application and a clinical validation of the method . il gel ecografico uno strumento semplice , veloce ed economico , per ottenere una adeguata compensazione del fascio , nei casi di irradiazione con elettroni di superfici irregolari . relativamente alla attenuazione del fascio , il valore di hu di 0 rende il gel equivalente allacqua . 
il vantaggio maggiore la sua assoluta adattabilit alla maggior parte delle sedi , a differenza di altri bolus commerciali che possono essere difficili da posizionare in cavit di piccole dimensioni , come pieghe cutanee o deficit di tessuto meta chirurgici . da questa esperienza limitata non possibile consigliare lutilizzo di questo presidio nei casi di irradiazione con fotoni , ma non sembrano essere presenti limitazioni per limpiego del gel anche in queste situazioni . 
virtual touch tissue quantification is an implementation of ultrasound ( us ) acoustic radiation force impulse ( arfi ) imaging that provides numerical measurements ( wave - velocity values ) of tissue stiffness . the aim of this study was to define the normal values of shear - wave speed for the healthy liver , gallbladder , pancreas , spleen and kidneys . 
sono state effettuate 140 misurazioni su fegato , pancreas , milza e reni , 70 nel lume della colecisti e 20 nel phantoconfrontando tutte le misurazioni eseguite da ciascun operatore in differenti parti dei vari organi addominali , non sono risultate differenze statisticamente significative . 
il valore medio della velocit di propagazione dellonda nel parenchima pancreatico inferiore rispetto a quella misurata nel fegato e nei reni , mentre la milza caratterizzata da valore medio pi alto . nei fluidi semplici , come lacqua , viene sempre riscontrato 890 radiol med ( 2010 ) 115 : 889897 simple fluids such as water , the value identified by the system with xxxx or 0 , is always measured . il valore di 0 o non numerico indicato dal sistema con xxxx . keywords arfi ultrasound imaging virtual touch tissue quantification healthy abdominal organs parole chiave arfi ecografia virtual touch tissue quantification fegato pancreas milza reni introduction introduzione in recent decades , there has been an increasing interest in assessing the viscoelastic properties of tissues with ultrasound ( us ) [ 13 ]  . 
us tissue - strain analysis can be performed under compression using hitachi real - time tissue elastography ( hi - rte , hitachi medical systems europe , zurich , switzerland ) , esie touch ( siemens , erlangen , germany ) or elasticity imaging ( siemens ) [ 4 , 5 ] , or without compression using acoustic radiation force impulse ( arfi ) imaging [ 6 , 7 ] and its new implementations , virtual touch tissue imaging ( siemens ) and virtual touch tissue quantification ( siemens )  . 
 arfi imaging is a new us imaging modality to evaluate the stiffness of deep tissues by short - duration acoustic radiation forces that produce localised displacements in a pushed region of interest ( roi ) [ 810 ]  . 
the response , monitored with us , depends on youngs modulus , which viscoelastic properties of tissues [ 810 ] and causes tissue deformation related to the resistance offered by the tissue to the wave propagation [ 13 , 14 ]  . reflects virtual touch tissue quantification provides numerical measurements ( wave - velocity values ) of tissue stiffness at a precise image - based anatomical location . 
thus , the aim of this study was to define the normal values of shear - wave speed for the healthy liver , gallbladder , pancreas , spleen and kidneys . 
 materials and methods this prospective study was conducted in accordance with the principles of the declaration of helsinki . study population negli ultimi decenni , la valutazione ecografica delle propriet visco - elastiche dei tessuti ha ricevuto crescente interesse [ 13 ]  . 
lanalisi ecografica dellelasticit dei tessuti pu essere effettuata con tecniche di immagine che richiedono una compressione esterna , come hitachi realtime tissue elastography ( hi - rte , hitachi medical systems europe , zurigo , svizzera ) , esie touch ( siemens , erlangen , germania ) o elasticity imaging ( siemens , erlangen , germania ) [ 4 , 5 ] , o con tecniche di immagine che non necessitano compressioni utilizzando acoustic radiation force impulse ( arfi ) imaging [ 6 , 7 ] come ( siemens , erlangen , virtual touch germania ) e virtual touch tissue quantification ( siemens , erlangen , germania )  . 
 imaging tissue la nuova tecnica dimmagine ecografica arfi in grado di valutare lelasticit dei tessuti profondi attraverso lapplicazione di impulsi di onde meccaniche di breve durata , che producono circoscritte modificazioni nella regione di interesse ( roi ) colpita [ 810 ] fornendo in un predefinito target misure qualitative e quantitative della velocit di propagazione dellonda [ 11 , 12 ]  . 
la tecnica , monitorata ecograficamente , genera risposte dipendenti dal modulo di elasticit che riflette le propriet visco - elastiche dei tessuti [ 810 ] con deformazioni tissutali correlate alla resistenza offerta dal tessuto alla propagazione dellonda [ 13 , 14 ]  . il virtual touch tissue quantification consente lo studio quantitativo con valori numerici ( velocit di propagazione dellonda ) dellelasticit dei tessuti in esame identificati su unimmagine ecografica convenzionale . 
pertanto , lo scopo di questo studio definire i valori normali di velocit di propagazione dellonda in fegato , colecisti , pancreas , milza e reni di soggetti sani . materiali e metodi questo studio prospettico stato condotto secondo le norme della dichiarazione di helsinki . the study population consisted of 35 healthy volunteers ( 17 men and 18 women ) with a mean age of 34.7 ( range 2546 ) years who underwent virtual touch tissue quantification after having signed informed consent . 
the inclusion criteria were : ( a ) absence of any history of focal or diffuse disease at any of the examined organs , assessed by patients history , laboratory data and conventional us ; ( b ) good visualisation of the liver , gallbladder , pancreas , spleen and kidneys on conventional us . imaging technique system conventional us and virtual touch tissue quantification were performed after a 4to 6 - h fast , using a siemens acuson s2000 us ( siemens , erlanger , germany ) , with convex probes ( 4c1 ) , tissue harmonic imaging ( thi ; 4 mhz ) and mechanical index of 1.7. 
then , an acoustic push pulse was transmitted immediately on the right side of the roi where the shear - wave speeds were calculated and expressed with a numerical value ( metre / second ) as a result of multiple measurements made for the same spatial location . 
for the liver study , the operator performed one measurement with subcostal scans on the deep left and one on the deep right liver lobes at the maximum depth ( about 5.5 cm ) evaluable by the system with the roi completely and perfectly inside the liver parenchyma , constantly taking care not to capture any vascular or biliary structures within the roi . 
ten measurements were obtained with the entire roi included inside the phantofor the pancreatic study , the operator performed two measurements per subject : one on the head and the other on the body - tail , taking care not to include any vessels within the roi . 
for the spleen study , the operator performed two measurements per subject : at the hilum and on one pole , taking care not to include any vascular structures within the roi . 
for the renal study , the operator performed two measurements per subject in the renal parenchyma , always being careful not to include any vascular or pelvic structures within the roi . 
poich lo scopo del nostro lavoro era descrivere i valori normali di velocit di propagazione dellonda in fegato , colecisti , pancreas , milza e reni definiti sani , solamente soggetti giovani sono stati arruolati nello studio . 
per lo studio del fegato , ciascun operatore , mediante scansioni sotto - costali , ha effettuato una misurazione nel lobo destro ed una nel lobo sinistro alla profondit massima ( circa 5 , 5 cm ) valutabile dal sistema , con la roi completamente e perfettamente compresa nel parenchima epatico , avendo cura di non includervi strutture vascolari o biliari . 
a tale scopo , stato preparato un palloncino completamente riempito con acqua facendo attenzione a far uscire le bolle di aria e sono state eseguite dieci misurazioni sempre includendo completamente la roi allinterno del palloncino . 
per lo studio del pancreas , ciascun operatore ha effettuato due misurazioni per soggetto , una alla testa e laltra al corpo - coda pancreatico , avendo sempre cura di non comprendere strutture vascolari allinterno della roi . 
per lo studio dei reni , ciascun operatore ha effettuato due misurazioni per soggetto a livello del parenchima renale , facendo attenzione a non comprendere strutture vascolari o pelviche allinterno della roi . 
1a - d tecnica ecografica arfi con virtual touch tissue quantification degli organi addominali superiori sani : fegato ( a ) , pancreas ( b ) , milza ( c ) e reni ( d )  . radiol med ( 2010 ) 115 : 889897 2 . 
confrontando separatamente tutte le misure eseguite da ciascun operatore nelle differenti porzioni di fegato , pancreas , milza e reni , non sono emerse differenze statisticamente significative ( valore di p > 0 , 05 )  . 
il confronto tra i valori medi risultati da tutte le misurazioni eseguite da entrambi gli operatori su ciascun organo addominale studiato non ha fornito differenze statisticamente significative ( valore di p > 0 , 05 )  . 
the viscoelastic properties of tissues have been widely evaluated since the development of elasticity imaging [ 5 , 15 ] , which by utilising gentle propagazione dellonda e riportato nella tabella 2 . 
le propriet visco - elastiche dei tessuti sono state ampiamente studiate a partire dallo sviluppo della tecnica di elasticity imaging [ 5 , 15 ] , che attraverso lapplicazione di una minima compressione esterna , valuta la durezza dei tessuti superficiali , con alta risoluzione elastografica [ 4 , 5 ]  . 
in letteratura sono gi state riportate numerose applicazioni cliniche dellelasticity imaging : come tecnica diagnostica e per la diagnosi bioptica nella mammella [ 16 ] e nella prostata [ 17 ] ; per differenziare noduli tiroidei benigni e maligni [ 18 ] ; per la valutazione strutturale e funzionale del tessuto miocardico [ 19 ] ; per distinguere placche arteriose molli e dure e migliorare la diagnosi ed il management della trombosi venosa [ 20 ] ; per differenziare linfonodi benigni e maligni [ 21 ] ; e per identificare e quantificare le modificazioni nel fegato cirrotico [ 22 , 23 ]  . radiol med ( 2010 ) 115 : 889897 compression assesses the stiffness of superficial tissues , enabling high - resolution elastography [ 4 , 5 ]  . 
several clinical applications of elasticity imaging have been described in the literature : for diagnostic purposes and biopsy targeting in the breast [ 16 ] and prostate [ 17 ] ; for differentiating benign from malignant nodules in the thyroid gland [ 18 ] ; for structural and functional evaluation of the myocardial tissue [ 19 ] ; for distinguishing soft from hard arterial plaques and improving the diagnosis and management of venous thrombosis [ 20 ] ; for differentiating benign from malignant lymph nodes [ 21 ] ; for detecting and quantifying cirrhosis changes [ 22 , 23 ]  . the mechanical - strain properties of deep tissues can now also be assessed since the development of arfi imaging [ 6 , 7 ]  . 
by means of short - duration ( < 1 ms ) acoustic radiation forces [ 25 ] , the detection pulse passes through a roi , producing localised displacements [ 810 ]  . 
the response is monitored with us and is mainly related to the viscoelastic properties of tissue , the local magnitude of radiation force and the generation and propagation of shear waves [ 8 ]  . 
thus , different tissues show different transient responses to the arfi pushing beams [ 14 , 25 ] : the more elastic a given tissue , the more displacement it experiences . depending on interactions with the transducer , the generated shear waves can provide qualitative visual or quantitative value measurements [ 12 , 25 , 26 ]  . virtual touch tissue imaging qualitatively implements arfi technology by providing a greyscale map of the tissue stiffness for a user - defined roi [ 11 ] : a bright shade identifies relatively soft ( elastic ) tissue , whereas a darker shade characterises relatively stiff ( nonelastic ) tissue . 
virtual touch tissue quantification quantitatively implements arfi technology by providing on a conventional us image numerical measurements ( wave - velocity values ) of tissue stiffness for a userdefined roi . 
it is the worlds first and only application for obtaining a numerical value of shear - wave speed related to tissue stiffness at a precise image - based anatomical location . in our study , we performed virtual touch tissue quantification on healthy subjects to describe the normal wavevelocity values of healthy liver , gallbladder , pancreas , spleen and kidneys . 
in base alle interazioni con il trasduttore , gli impulsi generati possono fornire risposte qualitative o quantitative [ 12 , 25 , 26 ]  . visco - elastiche dei il virtual touch tissue imaging una applicazione qualitativa della tecnica arfi che fornisce per una data regione di interesse una mappa in scala di grigi dellelasticit del tessuto [ 11 ] : unarea chiara identifica un tessuto relativamente molle ( elastico ) , mentre unarea scura caratterizza un tessuto relativamente duro ( non elastico )  . 
il virtual touch tissue quantification una applicazione quantitativa della tecnica arfi che fornisce , per una definita regione di interesse identificata su unimmagine ecografica convenzionale , misure numeriche ( velocit di propagazione dellonda ) dellelasticit del tessuto . 
questa la prima ed unica tecnica in grado di fornire un valore numerico della velocit di propagazione dellonda , correlato allelasticit del tessuto e riferito ad una precisa sede anatomica identificata allecografia convenzionale . 
 nel nostro studio il virtual touch tissue quantification stato effettuato su soggetti sani per descrivere i valori normali di velocit di propagazione dellonda su fegato , colecisti , pancreas , milza e reni sani . la valutazione intra - operatore non risulta influenzata dalla localizzazione della roi nelle differenti porzioni degli organi parenchimatosi addominali superiori esaminati . 
 interoperator evaluation confirmed no significant differences between all mean wave - velocity values resulting from the measurements performed on each organ by both operators , thus proving the reproducibility of virtual touch tissue quantification . 
the highest mean wave - velocity value was measured in the spleen parenchyma ( 2.44 m / s )  . to date , arfi imaging has been tested to evaluate only solid tissues [ 13 ]  . 
in normal conditions , the gallbladder may be judged as a homogeneous fluid structure because of the very small dimensions of the particles contained in bile , which can move freely within its physiologically distended lumen . in homogeneous fluids , such as water , we observed that virtual touch tissue quantification always provides nonnumerical values , expressed as xxxx / 0 . 
this nonnumerical value is due to the lowest shear waves generation in simple fluids and to an excessively large variation of the individual velocity estimates between tracking beams resulting from excessive motion within the roi preventing a reliable reading and from the mainly attenuation of shear waves in fluids . 
so , the wave speed measured in the healthy gallbladder is always a nonnumerical xxxx / 0 value . the fixed box dimension of the target roi , the limited depth evaluable by the system ( maximum about 5.5 cm ) and the sensitivity to movement artefacts are the main limitations encountered in the application of this new technique . moreover , another limit of our study is that the phantom fluid model was not realised with the same content of the gallbladder . 
the mean shear - wave speed is lower in the pancreatic parenchyma than in the liver and kidneys , whereas the la valutazione inter - operatore conferma lassenza di differenze significative tra tutti i valori medi di velocit di propagazione dellonda risultati dalle misurazioni effettuate dai due operatori su ciascun organo , dimostrando cos la riproducibilit del virtual touch tissue quantification . 
il valore medio maggiore stato misurato nel parenchima splenico ( 2 , 44 m / s )  . finora , la tecnica arfi stata applicata solamente per la valutazione dei tessuti solidi [ 13 ]  . 
in condizioni normali , la colecisti pu essere considerata come una struttura fluida omogenea , a causa delle esigue dimensioni delle particelle contenute nella bile , libere di muoversi nel lume fisiologicamente disteso . 
nei fluidi omogenei , come lacqua , abbiamo osservato che il virtual touch tissue quantification ottiene sempre valori non numerici , espressi come xxxx / 0 . questo valore non numerico dovuto alla esigua componente delle onde trasversali nei fludi ed alla grande variazione delle velocit individuali stimate determinata da un movimento allinterno della roi eccessivo per poter ottenere un risultato leggibile . 
cos , la velocit di propagazione dellonda misurata nella colecisti sana sempre un valore non numerico , espresso come xxxx / 0 . le dimensioni fisse del box della roi , il limite di profondit massima misurabile dal sistema ( massimo di circa 5 , 5 cm ) e la sensibilit agli artefatti da movimento sono i principali limiti incontrati nellapplicazione di questa nuova metodica . 
il valore medio della velocit di propagazione dellonda nel parenchima pancreatico inferiore rispetto a quella misurata nel fegato e nei reni , mentre la milza caratterizzata da valore medio pi alto . radiol med ( 2010 ) 115 : 889897 spleen is characterised by the highest mean value . 
petralia1 1divisione di radiologia , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy 2facolt di medicina e chirurgia , universit degli studi di milano , via festa del perdono 7 , 20122 milano , italy correspondence to : m . 
the aim of this paper is to describe our personal experience and review the literature on the applications of ctp in tumours of different body regions , with particular regard to fields of development for new research . 
additional and ideally multicentre studies are necessary to define the role of this technique . keywords ct perfusion kinetic models oncology therapy monitoring prediction of tumour response to theraphy solid body tumours riassunto la tomografia computerizzata perfusionale ( tcp ) ha dimostrato potenzialit nella diagnosi dei tumori , nella valutazione della risposta alla terapia e nella previsione di risposta ed oggetto di numerosi studi sperimentali e clinici . 
la sua sempre pi ampia disponibilit sul territorio e la semplicit di esecuzione la rendono una tecnica che affianca limmagine morfologica e rende pi completa la valutazione delle lesioni neoplastiche . 
scopo di questo lavoro descrivere i risultati personali e i dati descritti in letteratura sulle applicazioni della tcp nei tumori dei diversi distretti , con un particolare accento ai possibili campi di sviluppo per nuove ricerche in questo ambito . 
ulteriori studi , possibilmente multicentrici , sono necessari per definire levidenza del ruolo di questa tecnica . parole chiave tc perfusionale modelli cinetici oncologia monitoraggio della terapia previsione di risposta alla terapia tumori solidi del corpo introduction introduzione perfusion computed tomography ( ctp ) is used in oncology given its ability to indicate tumour angiogenic activity . tumour angiogenesis is defined as the formation of new vessels by pre - existing vessels [ 1 ]  . 
in theory , ctp is able to la tomografia computerizzata perfusionale ( tcp ) utilizzata in oncologia perch si ritiene che essa possa fungere da indicatore dellattivit angiogenetica dei tumori . 
langiogenesi tumorale , per definizione , la formazione di nuovi vasi da radiol med ( 2010 ) 115 : 858874 measure the blood volume ( bv ) within the newly formed microvasculature in that it attributes a numerical value to the bv parameter , which is expressed in millilitres / 100 g of tissue . 
in this setting , ctp offers an estimate of capillary permeability by calculating the permeability surface ( ps ) or the extraction fraction ( ef ) , expressed in millilitres / 100g of tissue / mfor these reasons , ctp is theoretically able to quantify tumour angiogenesis . 
with respect to other potential angiogenesis biomarkers , such as measuring microvessel density ( mvd ) , vascular endothelial growth factor ( vegf ) or circulating endothelial cells ( cec ) ( appendix 1 ) , ctp offers the indisputable advantages of being noninvasive , relatively inexpensive and widely available . correlations between perfusion parameters calculated with ctp and other potential angiogenesis biomarkers have been investigated in a number of studies . 
several authors have noted a correlation between ctp parameters and mvd in patients with tumours of the lung [ 3 , 4 ] , pancreas [ 5 ] and colon - rectum [ 6 ] , and between ctp and vegf in patients with tumours of the lung [ 4 ] and rectum [ 7 ]  . 
other authors , however , have been unable to show a correlation between ctp parameters and other angiogenesis biomarkers [ 8 , 9 ]  . heterogeneity of findings reported in the literature can be explained in part by the limited number of cases described and in part by the fact that ctp provides a functional measure of the effects that angiogenesis produces on tumour perfusion , which is different from the morphological information given by mvd and the biological information provided by vegf and cec . ctp in neoplastic tissues ctp - measured perfusion values significantly higher than healthy tissue of the same organ have been noted in hepatocellular carcinoma ( hcc ) [ 10 ] and tumours of the rectum [ 9 , 11 ] , lung [ 12 ] and neck [ 13 , 14 ]  . 
a higher measure of blood flow ( bf ) ( or perfusion , depending on the model used ) in the tumour than in the healthy tissue may be an expression of a large number of arteriovenous shunts , and as these are low - resistance compartments , they cause increased flow in the microvasculature . 
as bf increases , there is a corresponding decrease in the mean transit time ( mtt ) of blood in the microvasculature of the studied volume as measured with ctp . 
lastly , a higher permeability value ( or ps , according to the model used ) in the tumour than in healthy tissue could be indicative of greater permeability of wall endothelium of the newly formed vessels vasi pre - esistenti [ 1 ] ; la tcp , in teoria , in grado di misurare il volume di sangue ( bv ) allinterno dei microvasi neoformati , in quanto attribuisce un valore numerico al parametro del bv , espresso in ml / 100 g di tessuto . 
i vasi neoformati , inoltre , hanno una parete alterata e perci sono tipicamente iperpermeabili [ 2 ] e la tcp in grado di offrire una stima della permeabilit capillare attraverso il calcolo della permeability surface ( ps ) o della frazione di estrazione ( fe ) , espressi in ml / 100g di tessuto per minuto . 
per questi motivi la tcp sarebbe teoricamente in grado di quantificare il fenomeno dellangiogenesi nei tumori : rispetto ad altri potenziali biomarkers dellangiogenesi , come la misura della densit dei microvasi ( mvd ) , dei livelli circolanti di fattori di crescita angiogenetici ( vegf ) o di cellule endoteliali circolanti ( cec ) ( appendice 1 ) , essa presenta gli innegabili vantaggi di essere non invasiva , poco costosa e disponibile sul territorio . le correlazioni tra i parametri di perfusione calcolati con tcp e altri potenziali biomarkers dellangiogenesi sono state indagate da diversi autori . 
alcuni autori hanno osservato una correlazione dei parametri della tcp con la mvd , in pazienti con tumori del polmone [ 3 , 4 ] , pancreas [ 5 ] e colon - retto [ 6 ] e con il vegf , in pazienti con tumori al polmone [ 4 ] ed al retto [ 7 ]  . 
la disomogeneit dei risultati riportati in letteratura pu essere ricondotta in parte alla scarsa numerosit delle casistiche descritte , in parte pu essere dovuta al fatto che la tcp fornisce una misura funzionale degli effetti che langiogenesi determina sulla perfusione del tumore , che diversa dalle informazioni morfologiche definite dalla mvd e da quelle biologiche fornite dalla determinazione di vegf e cec . tcp nei tessuti neoplastici valori di perfusione misurata con tcp significativamente pi elevati rispetto al tessuto sano dello stesso organo sono stati osservati negli epatocarcinomi [ 10 ] , nei tumori del retto [ 9 , 11 ] , del polmone [ 12 ] , del tratto aerodigestivo superiore [ 13 , 14 ]  . 
un valore maggiore di flusso sanguigno ( o perfusione , in accordo con il modello cinetico utilizzato ) nel tumore rispetto al tessuto sano potrebbe essere espressione di un numero elevato di shunts artero - venosi che , essendo un compartimento a bassa resistenza , determinano un aumento del flusso nei microvasi . 
allaumentare del flusso sanguigno , diminuisce il tempo di transito medio del sangue nei microvasi del volume analizzato , misurato dalla tcp con il valore del mean transit time ( mtt )  . 
un valore maggiore di bv nel tumore rispetto al tessuto sano potrebbe essere espressione dellaumento del letto microvascolare nel tumore dovuto alla formazione di nuovi vasi [ 15 ] , in relazione al processo dellangiogenesi . 
a colour map for bf : tumour shows a greater presence of yellow and red nuances , which indicate higher numerical values than normal tissues , where green and blue nuances are more present . 
b colour map for bv : tumour shows a greater presence of yellow and red nuances , which indicate higher numerical values than normal tissues , where green and blue nuances are more present . 
c colour map for mtt : tumour shows a greater presence of green and blue nuances , which indicate lower numerical values than normal tissues , where yellow and red nuances are more present . 
mappe colore di bf , bv , mtt e ps : in queste mappe i valori elevati sono rappresentati dai colori tendenti al giallo ed al rosso e i valori bassi sono rappresentati dai colori tendenti al verde e al blu . 
a mappa colore del bf : nel tumore sono pi rappresentati colori tendenti al giallo ed al rosso , che indicano valori pi elevati rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al verde e al blu  . 
b mappa colore del bv : nel tumore sono pi rappresentati colori tendenti al giallo ed al rosso , che indicano valori pi elevati rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al verde e al blu . 
c mappa colore del mtt : nel tumore sono pi rappresentati colori tendenti al verde e al blu , che indicano valori pi bassi rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al giallo e al rosso . 
d mappa colore del ps : nel tumore sono pi rappresentati colori tendenti al giallo ed al rosso , che indicano valori pi elevati rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al verde e al blu . compared with that of the normal microvasculature ( fig . 1 ) [ 16 ]  . in high - grade lymphomas [ 17 ] and brain tumours [ 18 ] , significantly higher perfusion values have been observed than in low - grade tumours . 
in contrast , in high - grade hepatocellular carcinoma ( hcc ) , significantly lower perfusion values have been reported ( probably due to the greater presence of central necrosis ) [ 10 ]  . 
there appears to be little agreement between the findings reported to date , such that further studies are required to draw significant conclusions . grado sono stati osservati valori dei parametri di perfusione significativamente pi elevati rispetto ai tumori di basso grado . 
viceversa negli epatocarcinomi di alto grado sono stati osservati valori dei parametri di perfusione significativamente pi bassi ( probabilmente in relazione alla presenza maggiore di necrosi centrale ) [ 10 ]  . 
i risultati delle esperienze oggi disponibili sono relativamente discordanti e sono necessari ulteriori studi per trarre conclusioni significative , ma , se studi pi ampi confermassero le differenze di perfusione misurata con tcp in tumori con grado differente , la tcp potrebbe contribuire allo studio delle radiol med ( 2010 ) 115 : 858874 however , if larger studies were to confirm perfusion differences measured with ctp in tumours with different grades , then ctp could contribute to the study of biological characteristics of tumours in a noninvasive , relatively inexpensive and widely available technique . monitoring treatment several studies have reported significant reduction in perfusion parameters following chemotherapy in tumours located in various body regions : rectum [ 9 , 11 ] , liver [ 19 , 20 ] , lung [ 21 ] and neck [ 22 , 23 ]  . 
findings of these studies provide preliminary evidence that changes produced by chemotherapeutic agents on tumour vascularity [ 2427 ] can be identified from changes in tumour perfusion measured with ctp . 
if the chemotherapeutic agent produces a reduction in arteriovenous shunts in the tumour , which offer low - resistance flow , this could be identified as reduced bf ( or perfusion , according to the model used ) in the microvasculature . 
therefore , a tool is required that can monitor the effects of these treatments on tumour perfusion , because in these cases , monitoring tumour size alone is of little value [ 28 ]  . 
indeed , the literature reports that the efficacy of an antiangiogenic agent cannot be determined by measuring changes in mvd [ 29 ] , whereas monitoring circulating levels of angiogenic growth factors [ e.g. vegf , basic fibroblast growth factor ( bfgf ) or hematopoietic growth factor ( hgf ) ] or cec has produced heterogeneous results [ 28 , 30 , 31 ]  . 
in contrast , ctp has demonstrated its ability to identify reduced perfusion after a single administration of antiangiogenic / antivascular agent in rectal tumours [ 7 ] and hcc [ 20 ] , in a relatively early phase in a variety of solid tumours [ 3234 ] and after only a few hours [ 35 ] in experimental studies . 
these preliminary findings suggest a potential role for ctp as a noninvasive tool for monitoring antiangiogenic / caratteristiche biologiche dei tumori attraverso unanalisi non invasiva , poco costosa e disponibile sul territorio . monitoraggio della terapia alcune esperienze hanno documentato una riduzione significativa dei parametri di perfusione dopo chemioterapia in tumori di distretti diversi : nei tumori del retto [ 9 , 11 ] , del fegato [ 19 , 20 ] , del polmone [ 21 ] e del tratto aerodigestivo superiore [ 22 , 23 ]  . 
i risultati di questi studi forniscono levidenza preliminare che i cambiamenti determinati dagli agenti chemioterapici sulla vascolarizzazione dei tumori [ 2427 ] sono rilevabili attraverso variazioni della perfusione tumorale misurata con la tcp : la tcp , pertanto , potrebbe avere un ruolo importante nel monitoraggio di tali terapie . 
qualora lagente chemioterapico determinasse nel tumore una riduzione degli shunts artero - venosi , che offrono bassa resistenza al flusso , essa potrebbe essere rilevata come riduzione del flusso sanguigno nei microvasi ( misurato con i parametri bf o fe , secondo il modello cinetico utilizzato )  . 
la riduzione del flusso sanguigno nei microvasi determinerebbe un aumento del tempo di transito medio nel microcircolo , misurato con il parametro mtt . uneventuale riduzione numerica e di volume dei microvasi tumorali dopo terapia pu essere rilevata dalla tcp con una diminuzione del volume sanguigno allinterno dei microvasi nel tumore , misurato con il parametro bv . 
 le terapie anti - angiogenetiche / vascolari sono finalizzate soprattutto a ridurre lapporto di sangue al tumore e a stabilizzarne le dimensioni ( con un effetto detto citostatico ) ; il loro effetto sulle dimensioni del tumore secondario . sarebbe pertanto necessario uno strumento in grado di monitorare gli effetti di queste terapie sulla perfusione dei tumori , perch in questi casi il solo monitoraggio delle dimensioni del tumore ha poco significato [ 28 ]  . 
il monitoraggio dei biomakers istologici o sierici dellangiogenesi nei pazienti sottoposti a terapie anti - angiogenetiche / vascolari potrebbe non essere adeguato : stato infatti riportato in letteratura che lefficacia di un farmaco anti - angiogenetico non pu essere determinata misurando le variazioni della mvd [ 29 ] , mentre il monitoraggio dei livelli circolanti di fattori di crescita angiogenetici ( come il vegf , il b - fgf o lhgf ) o di cellule endoteliali circolanti ( cec ) ha dato risultati poco omogenei [ 28 , 30 , 31 ]  . 
la tcp , invece , stata dimostrata essere in grado di evidenziare una riduzione della perfusione dopo una singola somministrazione del farmaco anti - angiogenetico / vascolare nei tumori del retto [ 7 ] e nellepatocarcinoma [ 20 ] , in maniera precoce in diversi tumori solidi [ 3234 ] e gi dopo poche ore [ 35 ] in ambito di laboratorio . 
queste preliminari evidenze suggeriscono il potenziale ruolo della tcp come strumento non invasivo per il monitoraggio delle terapie anti - angiogenetiche / vascolari in ambito clinico , in grado di identificare 862 radiol med ( 2010 ) 115 : 858874 antivascular treatments in the clinical setting . 
antiangiogenic / antivascular sion agents are in fact usually active at low doses , and identifying the optimal biological dose is crucial , rather than using the maximum tolerated dose , as in conventional cytotoxic chemotherapeutic agents . in each predicting treatment response several studies have demonstrated low perfusion values in patients who fail to respond to chemotherapy or radiation therapy in tumours of the neck [ 23 , 36 , 37 ] , rectum [ 38 ] and lung [ 39 ]  . 
these preliminary findings seem to show that low tumour perfusion produces a poor response to chemotherapy on the one hand because the antitumoral agents have difficulty reaching poorly perfused tumours , and on the other hand , poor response to radiation therapy because poorly perfused tumours are hypoxic and therefore characterised by low radiosensitivity . 
the high clinical impact of predicting response prior to the beginning of chemotherapy or radiation therapy and the encouraging results of studies published to date are an incentive for further investigations . them expensive and ineffective application of ctp in solid tumours of different body regions head and neck tumours generally high perfusion values have been demonstrated in squamous - cell carcinoma ( scc ) of the upper aerodigestive tract than in corresponding healthy tissue [ 13 ] , benign lesions [ 14 ] or muscular tissue of the tongue [ 4042 ]  . 
i farmaci anti - angiogenetici / vascolari , infatti , sono solitamente attivi a basse dosi ed cruciale lidentificazione della dose biologicamente attiva ( obd , optimal biological dose ) , piuttosto che la massima dose tollerata ( mtd , maximum tollerate dose ) , come nei chemioterapici citotossici convenzionali . previsione di risposta alla terapia alcuni studi hanno dimostrato valori bassi di perfusione nei pazienti non responsivi a trattamenti chemioe radio - terapici , affetti da tumori del tratto aero - digestivo superiore [ 23 , 36 , 37 ] , del retto [ 38 ] e del polmone [ 39 ]  . 
da queste preliminari evidenze sembrerebbe che una bassa perfusione tumorale determini una cattiva risposta alla chemioterapia , perch i tumori poco perfusi sono raggiunti difficilmente dai farmaci antitumorali , e alla radioterapia , perch i tumori poco perfusi sono ipossici , con conseguente ridotta radiosensibilit . 
una tcp eseguita prima dellinizio della terapia potrebbe , in teoria , identificare i pazienti con tumori poco perfusi , candidati a una cattiva risposta a chemioe radio - terapia , per indirizzarli a trattamenti personalizzati o alternativi , evitando loro trattamenti inefficaci e costosi . sono necessarie , tuttavia , esperienze assai pi ampie di quelle oggi presenti in letteratura per trarre conclusioni significative : lelevato impatto clinico del predire la risposta prima dellinizio del trattamento chemioo radioterapico e i risultati incoraggianti degli studi pubblicati fino a oggi sono uno stimolo per ulteriori ricerche . applicazioni della tcp nei tumori solidi di diversi distretti corporei tumori di testa e collo sono stati osservati valori dei parametri di perfusione generalmente pi elevati nel carcinoma squamocellulare ( scca ) del tratto aerodigestivo superiore rispetto al tessuto sano corrispondente [ 13 ] , alle lesioni benigne [ 14 ] o al tessuto muscolare della lingua [ 4042 ]  . 
 tutti gli studi pubblicati [ 20 , 13 ] hanno osservato una riduzione dei valori dei parametri di perfusione misurati con tcp nei scca del tratto aerodigestivo superiore dopo chemioterapia di induzione . 
2a - h a 61 - year - old patient with invasive poorly differentiated squamous cell carcinoma of the right pyriform sinus ( white arrow with black border )  . 
a , b colour maps for bf before ( a ) and after ( b ) induction chemotherapy : tumour shows a greater presence of yellow and red nuances before therapy and a greater presence of green and blue nuances after therapy . 
c , d colour maps for bv before ( c ) and after ( d ) induction chemotherapy : tumour shows a greater presence of yellow and red nuances before therapy and a greater presence of green and blue nuances after therapy . 
e , f colour maps for mtt before ( e ) and after ( f ) induction chemotherapy : tumour shows a greater presence of green and blue nuances before therapy and a greater presence of yellow and red nuances after therapy . 
g , h colour maps for ps before ( g ) and after ( h ) induction chemotherapy : tumour shows a greater presence of yellow and red nuances before therapy and a greater presence of green and blue nuances after therapy . 
a , b mappe colore del bf prima ( a ) e dopo ( b ) chemioterapia di induzione : nel tumore sono pi rappresentati colori tendenti al giallo ed al rosso prima della terapia e colori tendenti al verde e al blu dopo la terapia . 
c , d mappe colore del bv prima ( c ) e dopo ( d ) chemioterapia di induzione : nel tumore sono pi rappresentati colori tendenti al giallo ed al rosso prima della terapia e colori tendenti al verde e al blu dopo la terapia . 
e , f mappe colore del mtt prima ( e ) e dopo ( f ) chemioterapia di induzione : nel tumore sono pi rappresentati colori tendenti al verde ed al blu prima della terapia e colori tendenti al giallo e al rosso dopo la terapia . 
g , h mappe colore del ps prima ( g ) e dopo ( h ) chemioterapia di induzione : nel tumore sono pi rappresentati colori tendenti al giallo ed al rosso prima della terapia e colori tendenti al verde e al blu dopo la terapia . 
tale reperto indica riduzione del valore di ps dopo terapia . 864 radiol med ( 2010 ) 115 : 858874 all published studies [ 20 , 13 ] have observed reduced perfusion parameter values measured with ctp in scc of the upper aerodigestive tract after induction chemotherapy . in addition , a correlation has been shown in these tumours between reduced bf and bv after therapy and reduced tumour volume , as measured with a reference technique such as endoscopy [ 43 ] and volumetric computed tomography ( ct ) [ 13 ]  . 
these findings suggest that monitoring perfusion parameters can be proposed as an integration to the standard technique . lastly , some studies have shown lower bv values in patients with upper aerodigestive tract scc who are poorly or non - responsive to induction chemotherapy [ 23 , 36 , 42 ]  . a study by hermans et al . 
 [ 23 ] performed on 105 patients with upper aerodigestive tract scc undergoing radiation therapy showed lower perfusion parameter values , thus suggesting that low perfusion values in upper aerodigestive tract scc prior to the beginning of chemotherapy or radiation therapy may be predictive of poor treatment response . pulmonary tumours a study conducted by sitarchouk et al . 
other published studies report terapia e la riduzione di volume tumorale , misurata con metodiche di riferimento come lendoscopia [ 43 ] e la tc volumetrica [ 13 ]  . 
tali risultati suggeriscono che il monitoraggio dei parametri di perfusione possa essere proposto come integrazione delle metodiche standard . alcuni studi , infine , hanno dimostrato valori di bv pi bassi nei pazienti con scca del tratto aerodigestivo superiore , poco responsivi o non responsivi alla chemioterapia di induzione [ 23 , 36 , 42 ]  . 
uno studio di hermans et al . [ 23 ] , che includeva 105 pazienti con scca del tratto aerodigestivo superiore sottoposti a radio - terapia , ha dimostrato valori dei parametri di perfusione pi bassi nei pazienti che non raggiungevano il controllo locale della malattia . 
dalle esperienze della letteratura , quindi , sembra che bassi valori di perfusione dei scca del tratto aerodigestivo superiore prima dellinizio della chemioo della radioterapia possano predire una loro cattiva risposta . tumore del polmone uno studio condotto da sitarchouk et al . 
3a - c a 56 - year - old patient with a benign solid lesion ( white arrow with red border ) of the upper lobe of the right lung . 
given the increasing use of antiangiogenic / antivascular agents in treating nonoperable pulmonary tumours [ 50 ] , ctp for the monitoring these treatments is desirable . hepatic tumours zhu et al . 
 [ 20 ] demonstrated higher perfusion values in hcc than in surrounding healthy hepatic parenchyma and observed significantly lower bf , bv and ps values in moderately to poorly differentiated hcc than in well - differentiated hcc . 
this is probably due to the rapid growth of hight grade hcc , which , in theory , can lead to the formation of poorly or nonperfused internal necrotic areas . 
the same authors [ 20 ] also observed a significant reduction in bf , bv and ps and a significant increase in mtt after administration of an antiangiogenic agent ( bevacizumab ) in patients with advanced hcc . although derived from a single study , these findings provide preliminary evidence that ctp is able to demonstrate the antiangiogenic effect of the agent in this group of patients through reduced perfusion values and therefore suggest a potential role of ctp in monitoring antiangiogenic / antivascular treatment in patients with hcc . 
clearly , further studies are needed to validate ctp in monitoring the functional response of hcc to these therapies . lastly , no studies are available that evaluate the potential of ctp in predicting hcc response to medical therapies . 
 [ 39 ] hanno osservato che i valori di bv e di ps aumentano nel tumore del polmone dopo radioterapia , nella periferia maggiormente rispetto al centro . questi risultati confermano quanto precedentemente osservato in alcuni studi di laboratorio , in cui descritto un aumento della perfusione in diverse linee cellulari tumorali dopo lesposizione a radiazioni ionizzanti [ 4749 ]  . 
nessuno studio ha valutato in maniera adeguata il ruolo della tcp nel monitoraggio della chemioterapia in pazienti con tumore del polmone ; con lutilizzo sempre pi frequente di farmaci anti - angiogenetici / vascolari per la terapia dei tumori polmonari non operabili [ 50 ] sarebbe auspicabile lutilizzo della tcp per il monitoraggio di tali terapie . tumori epatici zhu et al . 
 [ 20 ] hanno dimostrato valori di perfusione dellepatocarcinoma ( hcc ) pi elevati rispetto a quelli del parenchima epatico circostante e hanno osservato valori di bf , bv e ps significativamente pi bassi negli hcc mediamente o scarsamente differenziati rispetto agli hcc ben differenziati . 
ci probabilmente in relazione alla rapida crescita degli hcc di alto grado che , in teoria , pu determinare la formazione di aree necrotiche interne che sono poco o per nulla perfuse . 
gli stessi autori [ 20 ] hanno inoltre osservato una significativa riduzione di bf , bv e ps e un significativo aumento del mtt dopo la somministrazione di un farmaco anti - angiogenetico ( bevacizumab ) in pazienti con hcc avanzato . questi risultati , anche se relativi a una singola esperienza , forniscono levidenza preliminare che la tcp stata in grado di dimostrare leffetto anti - angiogenetico del farmaco in questo gruppo di pazienti attraverso la riduzione dei valori di perfusione e suggeriscono , quindi , un potenziale ruolo della tcp nel monitoraggio delle terapie antiangiogenetiche / vascolari in pazienti con hcc . 
b colour map for bf : lesions show a greater presence of green nuances , which indicate higher numerical values of bf than the surrounding normal hepatic parenchyma , where a blue homogeneous nuance is the only colour present . c colour map for bv : lesions show a greater presence of green and yellow nuances , which indicate higher numerical values of bf than surrounding normal hepatic parenchyma , where a blue nuance is more present . 
d colour map for mtt : lesions show a greater presence of blue nuances , which indicate lower numerical values of mtt than surrounding normal hepatic parenchyma , where green nuances are more present . 
b mappa colore del bf : nelle lesioni sostitutive sono pi rappresentati colori tendenti al verde , che indicano valori pi elevati rispetto al parenchima epatico sano , ove rappresentato un colore omogeneo blu . 
c mappa colore del bv : nelle lesioni sostitutive sono pi rappresentati colori tendenti al verde e giallo , che indicano valori pi elevati rispetto al parenchima epatico sano , ove sono pi rappresentati colori tendenti al blu . 
d mappa colore del mtt : nelle lesioni sostitutive sono pi rappresentati colori tendenti blu , che indicano valori pi bassi rispetto al parenchima epatico sano , ove sono pi rappresentati colori tendenti al verde . 
e mappa colore del ps : nelle lesioni secondarie sono pi rappresentati colori tendenti al rosso , che indicano valori pi elevati rispetto al parenchima epatico risparmiato , ove sono pi rappresentati colori tendenti al blu . pancreatic tumours higher perfusion values have been demonstrated in the normal pancreas [ 55 , 56 ] than in the pancreas of patients with diabetes . 
the reliability of ct perfusion measurements in adenocarcinoma of the pancreas has also been shown , and these correlate well with perfusion measurements done with xenon ct [ 57 ]  . 
the increasing use of neoadjuvant treatment in locally advanced adenocarcinoma [ 58 ] and the widespread use of medical therapies in endocrine tumours of the pancreas may , nonetheless , suggest a role for ctp in monitoring these treatments , as reported in tumours of other body regions . higher bf values measured with xenon ct have been reported in adenocarcinoma responsive to chemotherapy and with a positive prognosis [ 59 ]  . 
therefore , it may be hypothesised that in pancreatic tumours , as well , low perfusion values are predictive of poor treatment response given that a correlation between bf values measured with xenon ct and ctp has been shown [ 57 ]  . renal tumours miles et al . 
 [ 60 ] demonstrated differences in perfusion measured with ctp between normal renal parenchyma and diseased parenchyma ( renal tumour , renal infarction and two patients with cyclosporin - related nephrotoxicity )  . a correlation between perfusion estimate of renal tumours obtained by analysing the enhancement curve [ 61 , 62 ] and mvd values has been reported . 
these findings suggest the feasibility of ctp at the level of the kidneys and a possible role of the technique in studying renal tumour perfusion , although no study has been published in the literature . no studies report the use of ctp in monitoring renal tumours in patients undergoing chemotherapy . 
such studies are , however , desirable , particularly for monitoring antiangiogenic / antivascular treatments , the use of which is increasing in clinical practice in patients with metastatic renal tumours [ 63 ]  . lastly , it would be extremely useful to study the possible role of ctp in predicting the response to treatment and the prognosis of patients with renal tumours treated with antiangiogenic / antivascular therapies , as these are often highly expensive and subject to side effects . 
a number of studies demonstrate a possible predictive role of perfusion values measured with delayed contrast - enhanced magnetic resonance imaging ( dce - mri ) [ 64 , 65 ] in patients with renal cell carcinoma treated with antiangiogenic therapy , but there is still no evidence for the role of ctp . colorectal tumours sahani et al . 
rispetto al parenchima pancreatico normale potrebbero essere ipotizzati valori di perfusione pi bassi nelladenocarcinoma , dal confronto dei valori numerici dei parametri di perfusione riportati in studi differenti per adenocarcinoma e pancreas normale [ 5 , 56 , 57 ] , e pi alti per i tumori endocrini , dalla singola esperienza riportata da miles et al . 
 [ 55 ] , ma necessaria senza dubbio una casistica pi ampia per trarre conclusioni . non esistono esperienze in letteratura sullutilizzo della perfusione tc nel monitoraggio delle terapie ai tumori del pancreas ; lutilizzo sempre maggiore di terapie neoadiuvanti negli adenocarcinomi localmente avanzati [ 58 ] e lampio utilizzo di terapie mediche nei tumori endocrini del pancreas potrebbero , tuttavia , suggerire un ruolo per la tcp nel monitoraggio di tali terapie , come riportato in tumori di altri distretti . sono stati riportati valori di flusso sanguigno misurati con xenon tc pi elevati negli adenocarcinomi responsivi a chemioradioterapia e con prognosi migliore [ 59 ]  . 
stata dimostrata correlazione tra i valori di flusso sanguigno misurati con la xenon tc e con la tcp [ 57 ]  . tumore del rene in uno studio condotto da miles et al . 
 [ 60 ] sono state dimostrate differenze di perfusione , misurate tramite tcp , tra parenchima renale normale e affetto da alcune condizioni patologiche ( tumore renale , infarto renale e due pazienti con tossicit causata da ciclosporina )  . 
questi dati suggerirebbero la fattibilit tecnica della tcp a livello dei reni e un suo potenziale ruolo nello studio della perfusione delle neoplasie renali , ma non esistono a oggi esperienze pubblicate in letteratura . non esistono esperienze che riportino lutilizzo della tcp nel monitoraggio delle neoplasie renali in pazienti sottoposti a chemioterapia : queste sarebbero , tuttavia auspicabili soprattutto per il monitoraggio delle terapie antiangiogenetiche / vascolari , sempre pi utilizzate nella routine clinica in pazienti con tumori renali metastatici [ 63 ]  . infine , sarebbe assai utile studiare un eventuale ruolo della tcp nel predire la risposta alla terapia e la prognosi in pazienti con tumore del rene trattati con terapie antiangiogenetiche / vascolari , le quali sono spesso assai costose e possono indurre effetti collaterali : esistono alcuni lavori che dimostrano un possibile ruolo predittivo dei valori di perfusione misurati con la dinamica dellenhancement contrastografico in risonanza magnetica ( dce - mri ) [ 64 , 65 ] in pazienti con carcinoma renale trattati con terapia antiangiogenetica , ma non esiste ancora nessuna evidenza del ruolo della tcp . 868 radiol med ( 2010 ) 115 : 858874 the rectum than in the healthy rectal wall . 
5a - e a 69 - year - old patient with a locally advanced adenocarcinoma of the lower ( white arrow ) with lymphadenopathy in the right aspect of the mesorectal fat tissue ( red arrow with white border )  . 
b colour map tumour and for bf : lymphadenopathy show a greater presence of yellow and red nuances , which indicate than normal higher numerical values tissues , where blue nuances are more present . 
c colour map for bv : tumour and lymphadenopathy show a greater presence of yellow and red nuances , which indicate higher numerical values than normal tissues , where blue nuances are more present . 
d colour map for mtt : tumour and lymphadenopathy show a greater presence of blue nuances , which indicate lower numerical values than normal tissues , where yellow and red nuances are more present . 
5a - e paziente di 69 anni affetto da adenocarcinoma del retto distale ( freccia bianca ) localmente avanzato con linfoadenopatia nel versante destro del mesoretto ( freccia rossa con bordo bianco )  . 
b mappa colore del bf : nel tumore e nella linfoadenopatia sono pi rappresentati colori tendenti al giallo ed al rosso , che indicano valori elevati rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al blu  . 
c mappa colore del bv : nel tumore e nella linfoadenopatia sono pi rappresentati colori tendenti al giallo ed al rosso , che indicano valori pi elevati rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al blu . 
d mappa colore del mtt : nel tumore e nella linfoadenopatia sono pi rappresentati colori tendenti al blu , che indicano valori pi bassi rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al giallo e al rosso . 
e mappa colore del ps : nel tumore e nella linfoadenopatia sono pi rappresentati colori tendenti al giallo ed al rosso , che indicano valori pi elevati rispetto ai tessuti sani , ove sono pi rappresentati colori tendenti al blu . radiol med ( 2010 ) 115 : 858874 observed after neoadjuvant chemotherapy / radiotherapy by sahani et al . 
these findings strongly suggest that neoadjuvant chemotherapy / radiotherapy produces a significant change in perfusion in locally advanced rectal cancer , probably due to the effect of chemotherapy on tumour vascularity [ 25 ] and therefore on tumour perfusion . in addition , ctp could prove highly useful in monitoring antiangiogenic treatment administered in patients with rectal cancer , as the only study reported in the literature clearly suggests [ 7 ]  . 
further studies investigating the role of ctp in monitoring antiangiogenic / antivascular treatment in patients with colorectal cancer are desirable , given that such treatment is becoming increasingly common in a variety of centres [ 66 , 67 ]  . two studies evaluated the ability of ctp to predict the locally to chemotherapy / radiotherapy response advanced rectal cancer . 
 [ 9 ] demonstrated significantly higher bf and bv values prior to starting treatment in rectal cancer patients with a positive response to neoadjuvant chemotherapy / radiotherapy , in line with similar studies performed with dce - mri [ 68 , 69 ]  . 
 [ 11 ] , on the other hand , demonstrated significantly lower bf and higher mtt values in responsive patients . prostate tumours a higher mvd has been observed in prostatic adenocarcinoma than in healthy parenchyma [ 70 ] , and perfusion differences have been demonstrated when measured with ctp [ 71 , 72 ] and dce - mri [ 73 , 74 ] between tumour and normal prostatic parenchyma . 
if ctp were able to reliably identify neoplastic foci in the prostate , it would theoretically be possible to target radiation therapy and minimise radiation dose to surrounding healthy tissue . gynaecological tumours the only study in the literature to report ctp use in gynaecological tumours noted a positive correlation between bf and tumour oxygenation in cervical scc . 
given the recognised role of hypoxia [ 75 , 76 ] as an unfavourable prognostic factor for cervical scc and the invasiveness of identifying such hypoxia ( measured with an eppendorf electrode ) , further studies are needed to confirm the role of bf in evaluating tissue oxygenation and correlating perfusion values measured with ctp with treatment response and survival . 
da queste esperienze sembra evidente che la chemio - radioterapia neoadiuvante determini una significativa variazione della perfusione nei tumori del retto localmente avanzati , probabilmente in relazione alleffetto della chemioterapia sulla vascolarizzazione dei tumori [ 25 ] e , quindi , sulla perfusione degli stessi . la tcp , inoltre , potrebbe essere assai utile nel monitoraggio delle terapie antiangiogenetiche somministrate ai pazienti con tumore del retto , come evidente nellunica esperienza riportata in letteratura [ 7 ] , che ha dimostrato una riduzione dei parametri di perfusione in pazienti trattati con bevacizumab , evidente con la tcp gi dopo 12 giorni e una singola somministrazione del farmaco . 
sono auspicabili ulteriori esperienze che indaghino il ruolo della tcp nel monitoraggio delle terapie anti - angiogenetiche / vascolari in pazienti con tumori del colon - retto , dato che tali terapie sono sempre pi spesso adottate in diversi istituti [ 66 , 67 ]  . esistono solo due esperienze che hanno valutato la capacit della tcp nel predire la risposta alla chemio - radioterapia neoadiuvante nei tumori del retto localmente avanzati . 
 [ 9 ] hanno dimostrato valori significativamente pi elevati di bf e bv prima dellinizio della terapia nei tumori al retto dei pazienti responsivi alla chemio - radioterapia neoadiuvante , in accordo ad esperienze similari condotte con dce - mri [ 68 , 69 ]  . 
 [ 11 ] , invece , hanno documentato valori significativamente pi bassi di bf e pi elevati di mtt nei pazienti responsivi . tumore della prostata nelladenocarcinoma prostatico stata osservata una densit di microvasi pi elevata rispetto al parenchima normale [ 70 ] e sono state dimostrate differenze nella perfusione misurata con tcp [ 71 , 72 ] e dce - mr [ 73 , 74 ] tra tumore e parenchima prostatico normale . 
se la tcp fosse in grado di identificare in maniera affidabile i foci neoplastici nella prostata , sarebbe in teoria possibile mirare la terapia radiante su questi e minimizzare la dose ai tessuti circostanti . tumori ginecologici lunico studio in letteratura che descrive lutilizzo della tcp in tumori ginecologici ha osservato una correlazione positiva tra bf e ossigenazione tumorale nel scca della cervice . 
considerando il riconosciuto ruolo dellipossia [ 75 , 76 ] come fattore prognostico sfavorevole per i scca della cervice e linvasivit della sua determinazione ( attraverso puntura con lelettrodo di eppendorf ) , sarebbero 870 radiol med ( 2010 ) 115 : 858874 and therefore hypoxic tumours with an unfavourable prognosis [ 77 ]  . no studies report the application of ctp in studying other gynaecological tumours . 
 [ 77 ] , showed that bf and ps values are higher in women with cervical cancer and enlarged locoregional lymph nodes , thus suggesting a correlation between angiogenesis intensity and the probability of metastasis . limitations of the technique ctp has a number of limitations . 
an effective equivalent dose of 8 msv has been described for a ctp study of a solid tumour , which is greater than the expected dose for a conventional ct protocol ( 5 msv ) for studying a similar type of tumour [ 1 ]  . 
the radiation dose to which patients are exposed is high , especially when considering that ctp is often performed in the same session as conventional diagnostic ct [ 13 , 43 , 78 ]  . 
exposure to a high dose of ionising radiation is one of the main factors limiting the widespread application of ctp , which in oncology should be performed only within research protocols approved by the ethics committee . 
this makes it difficult to reach large numbers of homogeneous patients , with a consequent delay in acquiring experience in the technique and in drawing valid scientific conclusions . random and systematic errors in acquisition technique and image and data analysis can be difficult to identify and can significantly compromise reliability of the results . indeed , specific training is required for all operators performing ctp . 
even though encouraging preliminary results are available regarding reproducibility and intraand interobserver variability [ 9 , 79 ] , they only refer to some regions of the body and some ctp techniques . further studies in different regions and with different techniques are required to confirm the reliability of this imaging modality . lastly , multicentre applications of ctp are lacking , and these are required to validate the currently available results . conclusions auspicabili ulteriori studi che confermino la capacit del bf nel valutare lossigenazione tissutale e che correlino i valori di perfusione della tcp con la risposta alla terapia e con la sopravvivenza . 
in teoria , la tcp potrebbe identificare i scca della cervice poco perfusi e , quindi , ipossici e con prognosi sfavorevole [ 77 ]  . non esistono esperienze in letteratura che riportino lapplicazione della tcp nello studio di altri tumori ginecologici . lunico studio presente , condotto da haider et al . 
 [ 77 ] , ha dimostrato che i valori di bf e di ps sono elevati nelle donne affette da tumore della cervice uterina con linfonodi loco regionali ingranditi , suggerendo una correlazione tra lintensit dellangiogenesi e la probabilit di metastasi . limiti della metodica la tcp presenta dei limiti . 
descritta una dose equivalente effettiva di 8 msv per una tcp di un tumore del corpo , la quale superiore a quella attesa per un protocollo tc convenzionale ( 5 msv ) per lo studio dello stesso tumore [ 1 ] : la dose di radiazioni ionizzanti a cui i pazienti sono sottoposti elevata , soprattutto se si considera che la tcp spesso eseguita nella stessa seduta della tc convenzionale diagnostica [ 13 , 43 , 78 ]  . 
lesposizione a una elevata dose di radiazioni ionizzanti uno dei principali fattori che limitano applicazioni ampie della tcp , la quale in ambito oncologico dovrebbe essere eseguita solo allinterno di protocolli di ricerca approvati dal comitato etico : questo rende difficile raggiungere grandi numeri di pazienti omogenei , con conseguente lentezza nellacquisire esperienza nella metodica e nel trarre valide conclusioni scientifiche . la presenza di errori casuali e sistematici nella tecnica di acquisizione e nellanalisi di immagini e dati pu essere difficile da identificare e pu inficiare pesantemente laffidabilit dei risultati : necessario un training specifico per tutti gli operatori che eseguono la tcp . 
anche se esistono risultati preliminari incoraggianti sulla riproducibilit della metodica , cos come sulla determinazione della variabilit intrae inter - osservatore nellanalisi dei dati [ 9 , 79 ] , essi , tuttavia , riguardano solo alcuni distretti corporei e alcune tecniche di tcp : sono necessarie altre esperienze , in diversi distretti e con differenti tecniche di tcp per confermare laffidabilit di questa metodica . 
 infine , mancano le applicazioni multicentriche della tcp , le quali sono necessarie per validare i risultati oggi disponibili . increasing use of ctp in oncology and the integration of the technique in standard ct protocols are foreseeable , as a functional evaluation of tumour perfusion will become indispensible in clinical practice . 
perfect understanding of the mechanisms underlying ctp analysis , the pathophysiology conclusioni ipotizzabile che la tcp trovi un sempre pi ampio utilizzo in oncologia e che la tecnica sar integrata nei protocolli tc standard , perch nella pratica clinica diventer sempre pi indispensabile una valutazione funzionale della perfusione dei tumori . 
la tcp presenta innegabili vantaggi rispetto agli altri strumenti oggi disponibili come potenziale radiol med ( 2010 ) 115 : 858874 of tumour angiogenesis and mechanisms of new antiangiogenic agents will allow the radiologist to effectively use this technique and accurately report the findings to the clinical oncologist . appendix 1 biomarkers of angiogenesis measuring mvd involves counting the microvessels present per unit of area of a histological section [ 80 ] immunostained with antibodies ( cd 34 , 31 , 105 , f8ra / vwf ) against the molecules selectively expressed at the vascular level . 
mvd is an operator - dependent technique in that the microvessel count is performed by the operator , who subjectively selects the angiogenic spot to analyse and can overestimate the number of vessels for example , by counting a vessel with a tortuous course several times , as the sections are much thinner than the length of the vessels [ 81 ]  . 
whereas it has been shown that their serum concentration can be correlated with prognosis in some types of tumours , their effectiveness in evaluating treatment response , even response to antiangiogenic treatment , has not been demonstrated [ 28 , 30 ]  . measuring cec , indicators of endothelial damage correlated with a number of pathological conditions including tumours [ 83 ] , may play an important role in the basic tumour evaluation . 
the validity of the technique has been demonstrated both in the laboratory and the clinical setting [ 31 ] , but it is expensive , difficult to perform and not widely available . 
la perfetta conoscenza dei meccanismi alla base dellanalisi di tcp , della fisiopatologia della neoangiogenesi neoplastica e dei meccanismi di azione dei nuovi farmaci anti - neoplastici permettono al radiologo di valorizzare questa tecnica e di comunicare con efficacia e accuratezza i risultati agli oncologi clinici . appendice 1 biomarkers dellangiogenesi la misura della densit dei microvasi ( mvd ) consiste nella conta dei microvasi presenti per unit di area della sezione istologica [ 80 ] , opportunamente preparata marcatura con anticorpi ( cd 34 , 31 , 105 , f8ra / vwf ) contro le molecole elettivamente espresse a livello vascolare . 
la mvd una tecnica operatore - dipendente , in quanto la conta dei microvasi effettuata dalloperatore , il quale soggettivamente sceglie lo spot angiogenetico da analizzare e pu sovrastimare il numero dei vasi , ad esempio , contando pi volte un vaso tortuoso , in quanto le sezioni sono assai pi sottili rispetto alla lunghezza dei vasi [ 81 ]  . 
la misura dei livelli circolanti di fattori di crescita angiogenetici , come il vegf , il b - fgf o lhgf , stata ampiamente indagata [ 82 ]  . stato dimostrato che la misura della loro concentrazione sierica , in alcuni tipi di tumore , pu essere correlata alla prognosi , ma , al contrario , la loro efficacia nella valutazione della risposta alla terapia , anche antiangiogenetica , non stata dimostrata [ 28 , 30 ]  . 
la misura delle cellule endoteliali circolanti ( cec ) , che rappresentano un indicatore di danno endoteliale correlato a diverse patologie tra le quali anche quelle neoplastiche [ 83 ] , sembra possa ricoprire un ruolo importante sia nella valutazione basale dei tumori e la sua validit stata dimostrata in laboratorio ed in clinica [ 31 ] essa tuttavia una metodica costosa , di difficile esecuzione e poco disponibile sul territorio . 
cova unit clinico operativa di radiologia , universit degli studi di trieste , ospedale di cattinara , strada di fiume 447 , 34149 trieste , italy correspondence to : m . 
it therefore appears that the evaluation should focus not only on the image reconstructions to identify vascular disease , but also on the native axial images to detect incidental findings . keywords ct angiography abdominal aorta runoff collateral findings riassunto obiettivo . 
sono state valutate retrospettivamente le immagini di 500 pazienti sottoposti ad aa - cta e ai - cta , per un totale di 536 esami , mediante apparecchiatura a 64 strati per sospetta patologia vascolare aortica e periferica . due radiologi hanno valutato separatamente le immagini assiali a 5 mm utilizzando finestre di vista adeguate al distretto valutato . 
su 500 pazienti , solo in 97 non sono stati riscontrati reperti collaterali ( 19 , 4% ) ; sono stati identificati 821 reperti accessori , dei quali 43 ( 5 , 24% ) sono stati reputati significativi ; 135 ( 16 , 44% ) meritevoli di approfondimento e 643 ( 78 , 32% ) non significativi . 
appare quindi necessario effettuare una valutazione dei reperti accessori sulle immagini assiali native , senza limitarsi alla sola valutazione delle ricostruzioni focalizzate alla valutazione vascolare . parole chiave angiografia tc aorta addominale runoff reperti collaterali 984 introduction recent developments in the technology of multislice computed tomography ( msct ) , with the increasing spread of scanners using 16 and subsequently 64 slices , have allowed their use for the study of arterial and venous vascular structures , supporting and in part replacing invasive angiographic modalities based on arterial catheterisation and noninvasive techniques such as colour doppler ultrasound and magnetic resonance angiography ( mra ) [ 14 ]  . 
although the protocols for image acquisition and contrast administration are optimised for studying vascular structures , the volume acquired during ct angiography ( cta ) includes many other structures , such as parenchymatous organs , hollow viscera or musculoskeletal structures that may represent the sites of potentially significant pathology . 
therefore it is precisely the broader views afforded by msct when compared with digital subtraction angiography and mra that highlight the need for the radiologist to pay special attention to extravascular structures during the assessment of images acquired in the course of cta . 
this may lead to the identification of a number of possible collateral or incidental findings that are of varying importance in the diagnostic and therapeutic management of the patient . a collateral or incidental finding refers to an abnormality seen on the images that is not related to the original indication for the examination . 
nellesame di angio - tc , per quanto esso risulti ottimizzato come protocollo e come metodica di somministrazione del mezzo di contrasto ( mdc ) allo studio delle strutture vascolari , vengono comunque comprese nel volume acquisito numerose altre strutture quali organi parenchimatosi , visceri cavi o strutture facenti parte dellapparato muscolo - scheletrico che possono essere sedi di patologia , talvolta significativa . 
proprio in virt quindi della maggiore panoramicit della tcms rispetto allangiografia digitale ed allangio - rm si evidenzia la necessit che , nella valutazione delle immagini acquisite in corso di angio - tc , il radiologo ponga particolare attenzione anche alle strutture extravascolari . 
si possono evidenziare quindi una serie di eventuali reperti collaterali o incidentali che rivestono unimportanza diversa nelliter diagnostico e terapeutico del paziente . con il termine di reperto collaterale o incidentale si intende quel reperto presente nelle immagini che non appare correlato alloriginale indicazione dellesame stesso . 
questi reperti possono fornire informazioni aggiuntive riguardo alla patologia di base del paziente , essere causa di ulteriori indagini diagnostiche e portare a trattamenti terapeutici con il potenziale beneficio ad esempio , di un precoce riconoscimento di una lesione neoplastica ancora asintomatica [ 1 ]  . scopo del presente lavoro quello di valutare la prevalenza dei reperti collaterali in corso di esecuzione di indagini di angio - tc dellaorta addominale e del run - off degli arti inferiori . materiali e metodi popolazione esaminata sono stati valutati retrospettivamente mediante uno studio monocentrico 500 pazienti consecutivi ( 362 maschi e 138 femmine , et media 71 , 412 , 7 anni ) sottoposti ad angio - tc per lo studio dellaorta addominale ( 319 esami eseguiti in 283 pazienti ; 209 di sesso maschile e 74 di sesso femminile ) o per lo studio dellaorta addominale e delle arterie degli radiol med ( 2010 ) 115 : 983996 inclusion and exclusion criteria patients who underwent cta for clinical indications other than direct investigation of the abdominal aorta and vascular axes of the lower extremities ( polytrauma , haematoma following a surgical and / or interventional procedure , acute abdomen due to suspected bowel infarction , etc . ) , that is , cases in which the radiologists attention was necessarily given over to assessment of all the anatomical structures included in the acquisition volume , were excluded from the study . 
patients with the following indications were included : preoperative evaluation of the abdominal aorta in patients with an aneurysm of the abdominal aorta previously identified using ultrasonography ; follow - up assessment of an unoperated abdominal aortic aneurysm ; follow - up assessment of an abdominal aortic aneurysm treated with placement of aortic endograft or conventional graft ; evaluation of the renal arteries in hypertensive patients ; evaluation of splanchnic arteries in patients with abdominal claudication ; patient preparation prior to examination , patients were required to fast for at least 4 h , and a vein in the arm , preferably an antecubital vein , was cannulated with an 18 - gauge needle cannula . patients were studied in the supine position ( during inspiratory breath - hold )  . 
to study the abdominal aorta , the survey was conducted from the diaphragm down to the pubic symphysis , whereas for the lower limbs , the scan extended from the renal arteries down to the vessels of the foot . ct angiography cta examinations were performed using a 64 - slice scanner ( aquilion64 , toshiba medical systems , japan )  . 
the scanning parameters were the same for all patients : slice thickness 0.5 mm for 64 slices ; pitch factor 0.828 ( helical pitch 53 ) ; rotation time 0.4 s , and standard exposure modulation ( using sure exposure ) based on attenuation values of the two scout views ( anteroposterior and laterolateral )  . 
a contrast medium with a high iodine concentration ( iomeprol 350400 mgi / ml ; iomeron bracco , milan , italy ) was administered using an automatic dual - head injector ( stellant sct 211 , medrad , indianola , ia , usa )  . 
acquisition protocols differed according to the clinical query . arti inferiori ( 217 esami eseguiti su 217 pazienti ; 153 di sesso maschile , 64 di sesso femminile ) , per un totale di 536 esami , in un intervallo di tempo compreso fra il gennaio 2006 ed il gennaio 2008 , archiviati nel picture archiving and communication system ( pacs ) ospedaliero . criteri di inclusione ed esclusione sono stati esclusi dallo studio i pazienti sottoposti ad esame angio - tc con indicazione clinica diversa dalla diretta analisi dellaorta addominale e degli assi vascolari degli arti inferiori ( pazienti politraumatizzati , ematomi successivi a procedure chirurgiche e / o interventistiche , quadri addominali acuti da sospetto infarto intestinale , ecc . ) , omettendo quindi i casi in cui lattenzione del radiologo fosse necessariamente rivolta alla valutazione di tutte le strutture anatomiche incluse nel volume di acquisizione . 
sono stati esclusi inoltre pazienti con elevati valori di creatininemia , ( > 1 , 2 mg / 100 ml ) , con allergia nota al mezzo di contrasto e pazienti in gravidanza . 
sono stati inclusi pazienti con la seguente indicazione : valutazione preoperatoria dellaorta addominale in paziente portatore di aneurisma dellaorta addominale identificato precedentemente in ecografia ; controllo di aneurisma dellaorta addominale non controllo di aneurisma dellaorta addominale operato mediante posizionamento di endoprotesi aortica o protesi tradizionale ; valutazione delle arterie renali in paziente iperteso ; valutazione delle arterie splancniche in paziente con claudicatio abdominis ; valutazione dellaorta addominale e delle arterie degli arti inferiori in paziente con arteriopatia periferica . preparazione del paziente per lesecuzione dellindagine stato richiesto un digiuno da almeno 4 ore prima dellesame e viene previsto lincannulamento di una vena del braccio preferibilmente in sede antecubitale con agocannula da 18 gauge . 
i pazienti sono stati studiati in posizione supina ( in apnea inspiratoria ) ; per lo studio dellaorta addominale lindagine stata condotta dal diaframma fino alla sinfisi pubica , per lo studio degli arti inferiori dal livello dellemergenza delle arterie renali fino ai vasi del piede . 
i parametri di scansione per lesecuzione degli esami sono comuni : spessore di strato di 0 , 5 mm per 64 evaluation of the abdominal aorta and lower - limb arteries operato ; in patients with peripheral arterial disease . 986 radiol med ( 2010 ) 115 : 983996 to study the abdominal aorta , the protocol involves administration of 80 ml of contrast medium at a flow rate of 45 ml s , followed by 40 ml of saline at the same rate . 
an arterial - phase acquisition is obtained with the bolus - triggering technique in which the scan is synchronised with the arrival of the contrast bolus in a region of interest ( roi ) placed at the level of the abdominal aorta ( in subdiaphragmatic position )  . 
when studying patients with aortic endografts , a second acquisition is performed with a delay of 60 s from the start of the intravenous injection of contrast material with a view to identifying any endoleaks that can only be evaluated on delayed scans . 
the axial images are then reconstructed in a data set with a slice thickness of 1 man additional data set is reconstructed with 5 - mm - thick slices to assess collateral findings . for studying vascular axes of the lower limbs , the patient is placed in the supine position with the ankles in the headrest and the knees and pelvis in a neutral position in order to reduce motion artefacts during image acquisition . 
a dose of 100110 ml of contrast medium is injected , depending on the height and physique of the patient , with a flow rate of 45 ml / s , followed by 40 ml of saline at the same rate . 
the arterial - phase acquisition is achieved with the bolus - triggering technique in which the scan is synchronised with the arrival of the contrast bolus in an roi placed at the level of the distal abdominal aorta ( just upstream of the aortic bifurcation )  . 
images are then reconstructed in a data set with a slice thickness of 1 mm as far as the level of the knee and thereafter with a thickness of 0.5 mm to preserve maximum detail in the distal segments of the leg vessels . 
to standardise image assessment , strati , pitch factor di 0 , 828 ( helical pitch : 53 ) , tempo di rotazione di 0 , 4 secondi e modulazione esposimetrica ( sure exposure ) standard basato sui valori di attenuazione delle 2 scout ( antero - posteriore , a - p , ed latero - laterale , l - l )  . 
 stato somministrato mezzo di contrasto ad elevata concentrazione di iodio ( iomeprolo 350400 mgi / ml ; iomeron bracco , milano italia ) mediante iniettore automatico a doppia testa ( stellant sct 211 , medrad , indianola , usa )  . sono stati utilizzati differenti protocolli di acquisizione per lo studio dei diversi quesiti clinici . il protocollo di acquisizione per lo studio dellaorta addominale prevede la somministrazione di 80 ml di mdc con flusso di 45 ml / s , seguiti da 40 ml di soluzione fisiologica al medesimo flusso e consta nellesecuzione di una scansione in fase arteriosa , ottenuta mediante sincronizzazione con il bolo di mezzo di contrasto mediante tecnica di bolus triggering con posizionamento di una regione di interesse ( roi ) a livello dellaorta addominale ( in sede sottodiaframmatica ) e partenza automatica al superamento di 100 uh rispetto ai valori densitometrici basali ; il tempo di acquisizione in media di 7 s . 
nel caso dello studio di pazienti portatori di endoprotesi aortica , una seconda acquisizione viene quindi effettuata con ritardo di 60 s dallinizio delliniezione di mdc , con il fine di evidenziare eventuali endoleak valorizzabili solo con scansioni tardive . il volume acquisito comprende una regione anatomica dal diaframma alla sinfisi pubica . 
le immagini assiali sono state quindi ricostruite in un dataset con spessore di strato da 1 mm ; stato ricostruito un ulteriore dataset con spessore di strato di 5 mm al fine della valutazione dei reperti collaterali . per lo studio degli assi vascolari degli arti inferiori , il paziente viene posto in posizione supina con posizionamento delle caviglie dentro al poggiatesta e con ginocchia e bacino in posizione neutra , al fine di limitare gli artefatti da movimento durante lacquisizione delle immagini . 
vengono iniettati 100110 ml di mdc , a seconda dellaltezza e della costituzione fisica del paziente ad un flusso di 45 ml / s , seguiti da 40 ml di soluzione fisiologica con il medesimo flusso . 
la scansione in fase arteriosa ottenuta mediante sincronizzazione con il bolo di mezzo di contrasto mediante tecnica di bolus triggering con posizionamento di una roi a livello dellaorta addominale distale ( poco a monte del carrefour aortico ) e partenza automatica al superamento di 200 hu rispetto ai valori densitometrici basali ; tale soglia maggiormente elevata consente , associata ad un ulteriore ritardo nella partenza della scansione di 1215 secondi , una ottimale opacizzazione dei settori distale delle arterie a livello della gamba ; il tempo di acquisizione in media di 20 s . 
le immagini sono state quindi ricostruite in un dataset con spessore di strato da 1 mm sino a livello delle ginocchia e con spessore di 0 , 5 mm nei settori distali per conservare il massimo dettaglio a livello dei settori distali dei vasi della radiol med ( 2010 ) 115 : 983996 only the reconstructed 5 - mm - thick axial sections acquired during arterial - phase angiography and sent to pacs were taken into account . 
for this reason , lung scans were evaluated using a window both for the mediastinum ( width 350 ; level 30 ) and for the lung parenchyma ( width 1 , 500 ; level 550 ) , whereas for scans of the abdomen and legs , a window and level suitable for evaluating both parenchymatous organs ( width 420 ; level 50 ) and bone structures ( width 1 , 800 ; level 400 ) was employed . two radiologists evaluated the images in a double blind manner at reporting stations ( ebit - aet , esaote , genoa , italy ) equipped with three , three - megapixel monitors and recorded all collateral findings , dividing them into three categories according to their clinical significance : nonsignificant , significant and meriting further investigation ( table 1 )  . 
the accuracy of the classification of findings as significant and meriting further investigation was verified by assessing any previous or subsequent imaging studies ( x - rays , ultrasound , ct and mri ) and any additional information ( surgical or pathology reports , etc . ) that could be obtained from the hospitals radiology information system ( ris )  . results the collateral findings observed in the various organs and systems are listed according to their clinical significance in table 2 . 
since then , only few published papers have dealt with collateral findings during cta of the abdominal aorta and lower - limb arteries [ 69 ] , whereas the issue has been more widely addressed in the setting of cta of the coronary arteries [ 1014 ]  . 
it should also be noted that similar assessments had already been gamba ; stato ricostruito un ulteriore dataset con spessore di strato di 5 mm al fine della valutazione dei reperti collaterali . successivamente , le immagini ottenute sono state inviate ad una workstation con software dedicato ( vitrea , vital images , minnetonka , usa ) , ed elaborate mediante ricostruzioni in proiezione di massima intensit ( mip ) , multiplanari curve ( cmpr ) lungo il decorso dei vasi di interesse e 3d . elaborazione dei dati e valutazione delle immagini tutti i datasets sono stati ricostruiti con un kernel di ricostruzione ottimizzato per imaging vascolare , che garantisce comunque una buona risoluzione di contrasto e spaziale anche a livello dei parenchimi . 
per uniformare la valutazione delle immagini sono state prese in considerazione solo le ricostruzioni di 5 mm di spessore sul piano assiale eseguite dallapparecchiatura tcms ed inviate al sistema di archiviazione digitale pacs , acquisite nella fase arteriosaangiografica ; quando incluse nel protocollo , sono state valutate anche le ricostruzioni di 5 mm di spessore sul piano assiale acquisite in fase tardiva . 
le immagini sono state valutate con finestre e livelli adeguati alle strutture in esame : per tale motivo le scansioni a livello polmonare sono state valutate con una finestra sia per mediastino ( finestra : 350 ; livello : 30 ) sia per parenchima polmonare ( finestra : 1500 ; livello : - 550 ) , le scansioni a livello addominale e di arti inferiori con una finestra e livello adatti alla valutazione degli organi parenchimatosi ( finestra : 420 ; livello : 50 ) e delle strutture ossee ( finestra : 1800 ; livello : 400 )  . due radiologi hanno valutato le immagini in doppio cieco su stazioni di refertazione ( ebit - aet , esaote , genova , italia ) a 3 schermi con monitor da refertazione da 3 megapixel ed hanno registrato tutti i reperti collaterali che , secondo la loro importanza clinica sono stati ripartiti in 3 categorie : non significativi , significativi , meritevoli di approfondimento ( tabella 1 )  . 
dei reperti significativi e meritevoli di approfondimento stata considerata la loro correttezza mediante la valutazione di eventuali indagini radiologiche ( radiogrammi , ecografie , tc ed rm ) precedenti o successive allesame angio - tc oggetto di questo studio e di tutti gli ulteriori elementi ( referti di interventi chirurgici , referti di biopsie , etc ) ricavabili dal radiology information system ( ris ) aziendale . risultati nella tabella 2 sono riportati i reperti collaterali riscontrati nei vari organi ed apparati , anche tenendo conto della 988 radiol med ( 2010 ) 115 : 983996 table 1 classification of collateral findings : all collateral findings , arranged by organ / system and their clinical relevance . organ / system significant findings nonsignificant findings findings meriting further investigation liver angioma > 4 cm focal lesion of uncertain nature gall - bladder and bile ducts mbd lithiasis and dilatation biliary dilatation pericholecystic fluid spleen adrenal glands urinary system aneurysm of the splenic artery solid focal mass accessory spleen mass > 4 cm mass < 4 cm bladder lithiasis ureteral lithiasis hydronephrosis polypoid bladder lesion atypical renal cysts solid mass bladder - wall thickening pancreas lymphatic system mesenteric lymphadenopathy inguinal lymph node > 4 cm chronic pancreatitis cystic or solid mass atrophy genital system large fibroleiomyoma solid uteroadnexal mass digestive system free fluid free fluid solid mass abdominal wall , soft tissues loops soft - tissue mass hernia not involving bowel cysts angiomas < 4 cm calcification lithiasis cholecystectomy calcification of the walls scleroatrophic gallbladder simple cysts total nephrectomy partial nephrectomy renal hypertrophy horseshoe kidney transplanted kidney calcified lymph node enlarged prostate fibroleiomyoma calcified fibroleiomyoma diverticulosis evidence of previous resection hiatal hernia lipoma incisional hernia hernia involving intestinal loops evidence of previous fracture musculoskeletal system vertebral collapse marked spondylodiscitis severe gonarthrosis indeterminate osteolytic lesion intra - articular knee effusion thorax solid pulmonary lesion pulmonary consolidation mbd , main biliary duct conducted in patients undergoing ct colonography or unenhanced ct for renal colic [ 16 , 22 ]  . 
moreover , some of these case series [ 16 , 1823 , 25 ] reviewed non - contrast - enhanced ct , which provides inferior diagnostic information than that afforded by contrast - enhanced ct . 
it should also be stressed that the cta protocols adopted in our study tend to favour a relatively early angiographic phase , which is suboptimal for the correct study of the different parenchymas . 
solo in 97 su 500 pazienti ( 19 , 4% ) non sono stati riscontrati reperti accessori . discussione il primo lavoro che si occupato di reperti collaterali in radiol med ( 2010 ) 115 : 983996 tabella 1 classificazione dei reperti collaterali : reperti collaterali riscontrati , differenziati per organo e loro rilevanza clinica organo / apparato rep . 
non significativi fegato angioma > 4 cm lesione focale di natura incerta colecisti e vie biliari litiasi vbp con dilatazione dilatazione delle vie biliari versamento pericolecistico milza surrene apparato urinario pancreas sistema linfatico aneurisma dellarteria splenica tumefazione solida focale milza accessoria tumefazione > 4 cm litiasi vescicale litiasi ureterale idronefrosi lesione vegetante vescicale tumefazione < 4 cm cisti renale atipica tumefazione solida ispessimento parietale vescica pancreatite cronica tumefazione cistica o solida atrofia linfoadenopatia mesenterica linfonodo inguinale > 4 cm apparato genitale fibroleiomioma importante tumefazione utero - annessiale solida apparato digerente versamento libero versamento libero tumefazione solida parete addominale , parti molli tumefazione delle parti molli cisti angioma < 4 cm calcificazione litiasi colecistectomia calcificazione di parete colecisti scleroatrofica cisti semplice nefrectomia totale nefrectomia parziale ipertrofia renale rene a ferro di cavallo rene trapiantato linfonodo calcifico aumento di volume prostatico fibroleiomioma fibroleiomioma calcifico diverticolosi esiti di resezione ernia jatale ernia senza impegno di anse lipoma laparocele ernia con impegno di anse esiti di frattura apparato muscoloscheletrico crollo vertebrale spondilodiscartrosi marcata gonartrosi severa lesione osteolica di ndd versamento intra - articolare ginocchio torace lesione polmonare solida addensamento polmonare vbp , via biliare principale within the field of hepatic imaging , for example , the arterial phase allows for excellent depiction of hypervascular lesions ( such as hepatocellular carcinoma ) but may not prove appropriate for characterisation of hypovascular lesions ( such as , for example , most metastases ) [ 28 , 29 ]  . only in a few cases ( such as checking for endoleaks during the follow - up of aortic endografts ) do our protocols include a delayed phase at 60 s that is comparable with an early portal phase . 
da allora sono comparsi in letteratura solo pochi lavori concernenti questo tipo di valutazione in corso di indagini di angio - tc a livello di aorta addominale e di arterie degli arti inferiori [ 69 ] mentre tale problematica stata affrontata da un maggior numero di autori in ambito di esame angio - tc delle arterie coronarie [ 1014 ]  . 
va peraltro ricordato che valutazioni simili erano gi state effettuate in pazienti sottoposti ad esami di colon - tc o ad esame tc diretto per 990 radiol med ( 2010 ) 115 : 983996 table 2 collateral findings , arranged by organ or system organ / apparatus nonsignificant meriting further investigation significant total liver gall bladder and bile ducts spleen adrenal glands urinary system pancreas lymphatic system prostate genital system digestive system abdominal wall peritoneum musculoskeletal system thorax total fegato colecisti e vie biliari milza surrene apparato urinario pancreas sistema linfatico prostata apparato genitale apparato digerente parete addome peritoneo apparato muscolo - scheletrico torace totale tabella 2 reperti collaterali osservati : i differenti reperti collaterali divisi per organo o apparato organo / apparato non significativi da approfondire significativi totale abdominal aorta performed by iezzi et al . 
for this reason , we added to the two main categories of significant and nonsignificant findings a further group termed meriting further investigation , which included all nonconclusive cases deserving further attention and testing , as reported by other authors [ 10 ]  . 
findings were deemed significant in all lesions for which there was an indication for some form of medical treatment or surgery . compared to the categories proposed by iezzi et al . 
with regard to lung lesions , we distinguished between colica renale [ 1622 ] ; si tratta in entrambi i casi di indagini eseguite con spessore sottile : in queste casistiche lincidenza di reperti significativi variava dal 4% al 17% [ 8 , 1626 ]  . 
in alcune di tali casistiche [ 16 , 1823 , 25 ] inoltre , faceva riferimento ad indagini tc dirette , con informazioni diagnostiche inferiori rispetto a quanto possibile ottenere negli esami tc eseguiti con il mdc . 
va anche sottolineato come i protocolli angio - tc da noi adottati prediligano una fase contrastografica angiografica relativamente precoce , sub - ottimale per uno studio corretto dei differenti parenchimi . 
il numero e la tipologia dei reperti emersi in corso desame sono quindi potenzialmente influenzati dalla tempistica contrastografica dellesame , dal numero di fasi e dalla ridotta preparazione preliminare del paziente allesame ( non somministrazione di mdc o acqua per os ) [ 27 ]  . nellambito dellimaging epatico , ad esempio , la fase arteriosa consente unottima delineazione delle lesioni radiol med ( 2010 ) 115 : 983996 fig . 
1a - d significant collateral findings of neoplastic origa hepatocellular carcinoma nodule ( arrow ) ; b in the late phase , lesion washout ( arrowhead ) can be appreciated . 
a nodulo di hcc ( freccia ) ; b nella fase tardiva si apprezza washout lesionale ( testa di freccia ) ; c adenocarcinoma a livello del cieco ( freccia ) ; d grossolano pacchetto linfonodale in paziente con adenocarcinoma prostatico . areas of evident consolidation with air bronchogram ( classified as meriting further investigation ) from solid lesions highly suspicious for malignancy ( and considered significant findings )  . 
in our experience , collateral findings were identified in about 80% of the examinations reviewed . of the 821 findings identified , after omitting those classified as nonsignificant , 178 ( 21.7% ) findings deemed significant or meriting further investigation remained that were worthy of mention in the radiological report . 
i nostri protocolli prevedono solo in alcuni casi ( ricerca di endoleak nel controllo delle endoprotesi aortiche ) una fase tardiva a 60 s assimilabile ad una fase portale precoce . simili considerazioni si possono applicare alle eventuali lesioni spleniche [ 30 ] ed a carico della midollare renale [ 30 ] ; la mancanza di fase diretta invece ostacola la caratterizzazione di masse surrenaliche e di micro litiasi a livello delle vie urinarie . 
although the incidental findings often fall completely outside the remit of the clinical indication , this may not represent sufficient justification for any failure to report them . it should be stressed that the number of requests for cta of the abdominal aorta and lower - limb arteries , in relation to the increasing availability of msct equipment , as well as the ageing population , is destined to rise . 
abdominal aortic aneurysms have a prevalence rate of 2% in the general population , rising to 5% if one considers the over - 65 age group [ 31 ]  . the incidence of lower - limb arterial obstructive disease reaches approximately 2.5% in individuals between 50 and 65 years of age and exceeds 8% in the over - 65 age group [ 32 ]  . the search for collateral findings undeniably involves an additional workload for the radiologist already engaged in the evaluation of vascular structures . 
on the other hand , the radiation dose delivered to the patient is not negligible , and relazione allelevato numero di pazienti ambulatoriali con conseguente scarsa anamnesi , non stata possibile : per questo motivo ai due gruppi principali , denominati reperti significativi e non significativi , stato aggiunto un gruppo denominato meritevoli di approfondimento in cui hanno trovato posto tutti i casi non conclusivi , comunque meritevoli di attenzione e verifica , similmente a quanto riportato da altri autori [ 10 ] , considerando reperti significativi tutte quelle lesioni per le quali vi lindicazione a una qualche forma di trattamento medico o chirurgico . 
 [ 8 ] abbiamo inoltre incluso alcuni ulteriori reperti , peraltro non significativi , quali cospicui aumenti dimensionali della prostata o gravi patologie artrosiche ; per le lesioni polmonari si distinto fra le aree di franco addensamento , con presenza di broncogramma aereo ( classificate come meritevoli di approfondimento ) dalle lesioni solide altamente sospette per la presenza di processi produttivi ( considerate reperti significativi )  . 
nella nostra esperienza si evidenzia che circa l80% delle indagini da noi rivalutate presentava reperti collaterali . degli 821 reperti individuati , se si trascurano quelli da noi ritenuti non significativi , rimangono 178 ( 21 , 7% ) reperti significativi o meritevoli di approfondimento che meritano di essere inclusi nel referto radiologico relativo allesame . 
 [ 8 ] che segnalano unincidenza del 3 , 9% di patologia tumorale confermata . il riconoscimento e la segnalazione di patologie rilevanti pu modificare la prognosi o la terapia del paziente e questo enfatizza limportanza di una lettura il pi possibile accurata e completa dellindagine e , sebbene spesso i reperti accessori esulino completamente dallindicazione clinica dellesame , ci non pu essere giustificazione sufficiente alla mancata segnalazione degli stessi . va fatti evidenziato come il numero di richieste per indagini di questo tipo , in relazione alla crescente disponibilit di apparecchiature tcms , ed anche a causa dellinvecchiamento della popolazione destinato ad aumentare . gli aneurismi dellaorta addominale presentano un tasso di prevalenza del 2% nella popolazione generale , e del 5% se si considera la fascia det oltre i 65 anni [ 31 ]  . 
lincidenza di arteriopatia ostruttiva degli arti inferiori raggiunge il 2 , 5% circa nei soggetti det compresa tra i 50 e 65 anni , superando l8% in persone di et superiore ai 65 anni [ 32 ]  . indubbiamente la ricerca di reperti collaterali comporta un carico di lavoro aggiuntivo per il radiologo , gi impegnato nella valutazione delle strutture ; daltro canto la dose di radiazioni erogata al paziente non trascurabile , e 994 radiol med ( 2010 ) 115 : 983996 table 3 pathologies encountered . 
nella tabella sono elencati i reperti collaterali osservati divisi per patologia e rilevanza clinica assessment of collateral findings assessment of collateral findings significant angioma > 4 cm hepatocarcinoma gallbladder and biliary stones splenic artery aneurysm adrenal mass > 4 cm urinary stones chronic pancreatitis conglomerate mass of lymph nodes large fibroleiomyoma polypoid bladder lesion ascites intestinal diverticulosis with inflammation solid intestinal mass vertebral collapse solid pulmonary lesion findings meriting further investigation focal hepatic lesion biliary dilatation pericholecystic fluid focal splenic lesion adrenal mass < 4 cm solid renal lesion complex renal cyst angiomyolipoma pancreatic mass equivocal lymphadenopathy enlarged prostate solid uterine mass ovarian mass bladder - wall thickening intra - articular knee effusion articular osteolytic lesion vertebral osteolytic lesion area of pulmonary consolidation hepatic cysts hepatic calcifications small angiomas cholecystectomy gall - bladder stones accessory spleen renal cyst horseshoe kidney partial / total nephrectomy pancreatic atrophya calcified lymph nodes prostate calcifications spinal scoliosis evidence of a previous pelvic fracture evidence of previous bowel surgery diverticulosis coli abdominal hernia calcified fibroma reperti significativi angioma > 4 cm epatocarcinoma calcolosi colecisti e via biliare aneurisma a . 
splenica massa surrenalica > 4 cm calcolosi vie urinarie pancreatite cronica tumefazioni linfonodali a pacchetto fibroleiomioma importante lesione vegetante vescicale versamento ascitico diverticolosi intestinale con flogosi tumefazione solida intestinale crollo vertebrale lesione polmonare solida reperti meritevoli di approfondimenti lesione focale epatica dilatazione vie biliari versamento pericolecistico lesione focale splenica massa surrenalica < 4 cm lesione solida rene cisti complessa rene angiomiolipoma tumefazione pancreatica tumefazione linfonodale dubbia tumefazione prostata tumefazione solida uterina tumefazione ovarica ispessimento parete escicale versamento articolare ginocchio area osteolitica articolare area osteolitica vertebrale area addensamento polmonare cisti epatiche calcificazioni epatiche angiomi di piccole dimensioni colecistectomia calcolosi colecisti milza accessoria cisti renale rene a ferro di cavallo nefrectomia parziale / totale atrofia pancreaticaa linfonodi calcifici calcificazioni prostatiche rachide scoliotico esiti frattura bacino esiti intervento intestinale diverticolosi colica ernie addominali fibroma calcifico nonsignificant findings reperti non significativi athickness of pancreatic body < 1 cm and fatty infiltration aspessore corpo < 1 cm ed infiltrazione adiposa radiol med ( 2010 ) 115 : 983996 focusing attention only on the vascular aspect means part of this exposure risks remaining unused , nullifying the opportunity to discover possible collateral findings . concentrando solo lattenzione sul comparto vascolare una parte di questa rischia di rimanere inutilizzata , annullando lopportunit , di scoprire eventuali reperti collaterali . in conclusion , collateral findings discovered in the course of cta of the abdominal and lower - limb arteries are not to be neglected , with a rate of significant findings in around 5% of cases , and for this reason , we believe that evaluation of the cta examinations should be accompanied by a careful assessment of all extravascular diagnostic elements present in the survey . 
ctu was accurate for urinary tract evaluation , but it cannot replace cystoscopy in patients in whom a malignant bladder disease is suspected . keywords multislice computed tomography ct urography urinary tract kidney bladder riassunto obiettivo . 
tra le 322 uro - tc eseguite , 169 hanno individuato significative alterazioni a carico dellapparato urinario e 153 non hanno evidenziato aspetti di rilievo , con buona concordanza al follow - up . 
luro - tc si dimostrata un esame accurato per lo studio della via escretrice , ma non pu sostituirsi allesecuzione di un esame cistoscopico nello studio dei pazienti con sospetta patologia neoplastica vescicale . parole chiave tomografia computerizzata multistrato uro - tc via escretrice urinaria rene vescica radiol med ( 2010 ) 115 : 920935 introduction introduzione intravenous urography ( ivu ) has been the imaging modality of choice for morphological study of the urinary tract ever since its introduction into clinical practice in the 1930s . 
however , in recent decades , its role has been progressively downgraded as a result of the technological advances of other imaging techniques , such as ultrasound , computed tomography ( ct ) and magnetic resonance imaging ( mri ) [ 14 ]  . 
this consisted of either a ct study followed by ivu during the same session to obtain detailed and panoramic information about the urinary tract , or ct targeted at the kidneys and urinary sites of the findings identified at the previous ivu study [ 1 , 5 ]  . 
these solutions are clearly demanding in organisational terms , as they require the coordinated availability of two different radiology sections and expose the patient to a substantial dose of ionising radiation . the development of multidetector ct ( mdct ) systems has provided the possibility of obtaining a high spatial resolution in the three cartesian axes and , combined with advanced postprocessing techniques , allows for urogramlike , diagnostic - quality images of the urinary tract associated with the typical renal and extrarenal information of a ct examination [ 59 ]  . 
these advances have led to ct urography , defined by the members of the ct urography working group of the european society of urogenital radiology ( esur ) as a diagnostic examination optimized for imaging the kidneys , ureters and bladder . 
the examination involves the use of multidetector ct with thin - slice imaging , intravenous administration of a contrast medium , and imaging in the excretory phase [ 9 ]  . 
ct urography , especially when performed with the multiphase technique , is associated with high radiation doses ( 1035 msv , depending on the number of phases ) , and this is the main barrier to its widespread use [ 4 , 911 ]  . 
however , as with ivu , ct cannot be considered a standardised examination , and optimisation of ct urography to limit radiation dose involves the use of protocols employing fewer scans and modulation of the study based on the clinical question . 
 the aim of this study was to evaluate the diagnostic accuracy of ct urography performed with a 64 - slice ct scanner and using a dose - limiting technique consisting of a biphasic , unenhanced nephrographicand excretory - phase protocol involving injection of contrast material as a split bolus after intravenous administration of a diuretic ( furosemide )  . lurografia stata la metodica radiologica utilizzata in modo elettivo per lo studio morfologico delle vie escretrici urinarie fin dalla sua introduzione nella pratica clinica nel 1930 , ma negli ultimi decenni il suo ruolo si progressivamente ridimensionato alla luce degli sviluppi tecnologici e dellintroduzione di altre tecniche radiologiche , in particolare ecografia , tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) [ 14 ]  . 
con lavvento della tc alcuni autori proposero una tecnica ibrida per lo studio delle vie escretrici , in cui nella stessa seduta era eseguito un esame tc con successiva documentazione urografica per ottenere informazioni dettagliate e panoramiche sulla via escretrice , oppure un approfondimento mediante tc mirata dopo lurografia con lo studio dei reni e delle sedi ove erano stati individuati eventuali reperti [ 1 , 5 ]  . 
tali soluzioni risultano ovviamente impegnative dal punto di vista organizzativo , perch richiedono la disponibilit coordinata di due diverse sezioni radiologiche ed esponengono inoltre il paziente ad una dose di radiazioni considerevole . lo sviluppo di sistemi tc multidetettore ha ora fornito la possibilit di ottenere unelevata risoluzione spaziale sui tre assi cartesiani ed essa , in associazione ad un postprocessing avanzato , consente di ottenere immagini delle vie escretrici di qualit diagnostica simil - urografica cui si associa il bagaglio informativo renale ed extra - renale tipico dellesame tc [ 59 ]  . 
nata cos luro - tc , definita dai membri del ct urography working group della societ europea di radiologia urogenitale ( esur ) , come un esame diagnostico ottimizzato per limaging dei reni , degli ureteri e della vescica , che necessita luso di unapparecchiatura tc multidetettore , con acquisizione di immagini a strato sottile , somministrazione endovenosa di mezzo di contrasto ed una scansione ottenuta in fase escretoria [ 9 ]  . 
luro - tc , in particolare quando eseguita con tecnica multifasica , un esame ad elevata dose di radiazioni ( da 10 a 35 msv a seconda del numero di fasi ) ed attualmente questo il vero problema che ne pu limitare lutilizzo [ 4 , 911 ]  . 
lottimizzazione delluro - tc prevede infatti lutilizzo di protocolli a minor numero di scansioni , con modulazione dellesame in base al quesito clinico , e ci contribuisce a contenere la dose di radiazioni . 
 lo scopo di questo studio stato quello di valutare laccuratezza diagnostica dellesame uro - tc eseguito con apparecchiatura tc a 64 strati utilizzando una tecnica tesa materials and methods patients the study was conducted from january 2006 to june 2008 on 317 consecutive patients ( 111 women and 206 men ) , mean age 64.6 ( range 18 - 92 ) years . 
we focused our correlation analysis on the 264 patients assessed for a possible urothelial neoplasm , because for this category of patients , we often had available a subsequent finding capable of validating the ct urography result . 
we therefore considered patients referred to our centre for haematuria , unexplained urinary tract dilatation , cytology positive for the presence of atypical or malignant cells , positive cystoscopy and those being followed up for previous urothelial neoplasm . radiol med ( 2010 ) 115 : 920935 a limitare considerevolmente la dose al paziente , ovvero con un protocollo a due fasi , diretta e nefro - escretoria , che richiede liniezione del mezzo di contrasto a doppio bolo ( split bolus technique ) , dopo somministrazione per via endovenosa di diuretico ( furosemide )  . materiali e metodi pazienti lo studio stato condotto da gennaio 2006 a giugno 2008 su 317 pazienti consecutivi ( 111 di sesso femminile e 206 di sesso maschile ) , con et media di 64 , 6 anni ( range 1892 anni )  . 
essi sono stati sottoposti ad uro - tc , per un totale di 322 esami , in quanto cinque pazienti sono stati sottoposti allindagine due volte nel corso dei 30 mesi di studio . 
abbiamo table 1 computed tomography urography indications indications ( 322 cases ) number percent haematuria known urothelial neoplasm previous urothelial neoplasm hydronephrosis positive urine cytology acute / chronic flank pain stones positive or doubtful ultrasound chronic or recurrent infections postsurgical follow - up congenital anomalies iatrogenic trauma other ematuria nota neoplasia uroteliale pregressa neoplasia uroteliale dilatazione delle vie escretrici citologia urinaria postiva dolore al fianco / colica litiasi ecografia positiva o dubbia infezioni croniche o ricorrenti controllo post intervento chirurgico anomalie anatomiche danni iatrogeni altro 56.8 56 , 8 tabella 1 indicazioni allesecuzione dellesame uro - tc indicazioni ( 322 casi ) numero percentuale radiol med ( 2010 ) 115 : 920935 ct urography all ct urography studies were conducted on a 64 - slice mdct system ( aquilion 64 , toshiba medical systems , tokyo , japan )  . 
patients were placed in a supine position on the ct patient table , and an arm vein was cannulated with an 16 - gauge needle cannula through which 0.1 mg / kg furosemide was injected immediately before obtaining the scout images . 
the diuretic was used in all but the first eight patients ; subsequently , given the poor results obtained in these cases , it was decided to introduce diuretic administration as an integral part of the study protocol . 
 in almost all patients , a preliminary low - dose unenhanced scan extending from the upper pole of the kidneys to the bladder base was acquired at 120 kv and with automatic scans were current modulation . 
contrast - enhanced performed with the split - bolus technique whereby a first dose of contrast medium of 400 mgi / kg was injected at 2 ml / s , followed by an interval of 7 min , and a second bolus of 200 mgi / kg at a rate of 2 ml / s . 
we used nonionic contrast media at concentrations varying between 320 and 370 mgi / ml ( visipaque 320 , iomeron 350 , ultravist 370 )  . the nephrographic - excretory phase scan was acquired at 110 s after the beginning of injection of the second bolus , with the following parameters : collimation 640.5 mm , pitch 0.828 , 120 kv , automatic current modulation based on the scout image with sure exposure software , standard smooth reconstruction kernel ( type 13 ) with accepted standard deviation ( sd ) of 12.5 ( for patients with suspected neoplasm or papillary disease ) and smooth kernel ( type 11 ) with accepted sd of 12.5 ( for studies of anatomy or recurrent stone disease )  . 
in 48 patients ( 14.9% ) , we obtained a second scan in the prone position with coverage of either the entire urinary system or the bladder only , owing to delayed opacification of the urinary tract or the presence of equivocal findings on the first scan . image processing axial images were reconstructed to 5 - mm slice thickness for documentation purposes only . 
reconstructions included 3d volume rendering , 3d and thick - slab maximum intensity projection ( mip ) , average intensity projection ( aip ) mpr in the true coronal plane of the kidney and curved mpr ( cmpr ) along the course of the ureters using vessel probe software and focalizzato lanalisi di correlazione sui 264 pazienti sottoposti allesame per la valutazione di una possibile lesione neoplastica uroteliale , in quanto questa categoria di pazienti ci consentiva spesso un successivo riscontro in grado di validare il reperto delluro - tc . 
sono stati quindi presi in considerazione i pazienti giunti alla nostra osservazione per ematuria , dilatazione delle vie escretrici inspiegata , esame citologico positivo per la presenza di cellule atipiche o carcinomatose , reperto cistoscopico positivo , oppure nellambito del follow - up di una pregressa neoplasia uroteliale . esame uro - tc tutti gli esami uro - tc sono stato condotti utilizzando unapparecchiatura tc a 64 strati ( aquilion 64 , toshiba medical systems , tokyo , giappone )  . 
i pazienti sono stati quindi posti in decubito supino sul lettino dellapparecchiatura tc e si proceduto ad incannulamento di una vena dellarto superiore con ago - cannula da 18 g attraverso la quale stata iniettata furosemide alla dose di 0 , 1 mg / kg , immediatamente prima di ottenere le immagini scout . 
il diuretico stato utilizzato in tutti i pazienti ad eccezione dei primi 8 ; in seguito , visti i risultati non ottimali ottenuti in questi casi , si deciso di introdurne la somministrazione come parte integrante del nostro protocollo di studio . 
 in quasi tutti i pazienti stata acquisita una preliminare scansione diretta a bassa dose , a 120 kv e con modulazione automatica della corrente , estesa dal polo superiore dei reni alla base vescicale . 
per la scansione contrastografica stato utilizzato il metodo split - bolus con una prima iniezione di mezzo di contrasto di 400 mgi / kg , a 2 ml / s , seguita da una pausa di 7 minuti , e quindi da un secondo bolo di 200 mgi / kg a 2 ml / s . 
sono stati utilizzati mezzi di contrasto non ionici a concentrazione variabile fra 320 e 370 mgi / ml ( visipaque 320 , iomeron 350 , ultravist 370 )  . la scansione nefro - escretoria stata eseguita a 110 secondi dallinizio delliniezione del secondo bolo , con i seguenti parametri di acquisizione : collimazione 64 ? 0 , 5 mm , pitch 0 , 828 , 120 kv , modulazione automatica della corrente in base allimmagine scout con software sure exposure , filtro di ricostruzione di tipo 13 ( standardsmooth ) con deviazione standard accettata di 12 , 5 ( per i pazienti con sospetto neoplastico o di patologia della papilla ) e filtro 11 ( smooth ) con deviazione standard accettata di 12 , 5 ( in caso di studio anatomico o per patologia litiasica recidivante )  . 
in 48 pazienti ( 14 , 9% ) stata necessaria lesecuzione di una seconda scansione in posizione prona , estesa a tutto lapparato urinario o alla sola vescica , subsequent manual correction . 
the evaluation was done on the mpr images and image volume visualised at a thickness of 3 mm in the axial , coronal and sagittal planes . a causa di un ritardo di opacizzazione della via escretrice o per la presenza di reperti dubbi . radiol med ( 2010 ) 115 : 920935 follow - up for each patient , we considered the study indications and results , which were then assessed in the light of previous and subsequent investigations . 
this approach required analysis of laboratory and imaging tests , such as urine cytology , ultrasound and abdominal ct , cystoscopy retrograde pyelography and histological reports of any surgical procedures . 
we considered the findings of examinations performed in the month prior to ct urography and during a mean follow - up of 16.7 ( range 434 ) months . results of 322 ct urography studies , 169 had evidence of significant urinary tract changes , and 153 had no significant findings . 
the 169 abnormal studies showed the following findings , some of which were in the same study : 11 congenital anomalies , 15 renal neoplasms , 103 urothelial neoplasms ( eight calyceal , two pelvic , 30 ureteral and 63 bladder ) , 38 cases of lithiasis , six cases of renal infection , 14 cases of ureteropelvic junction syndrome , three cases of medullary sponge kidney , two cases of medullary necrosis , two cases of calyceal fornix fissuring , one calyceal diverticulum and one ureterocoele . 
the 11 congenital anomalies included five cases of unilateral ureteral duplication ; two of bilateral ureteral duplication ; one of ureteral triplication ; one of agenesis of the kidney , ipsilateral ureter and seminal vesicle ; and two of horseshoe kidney . 
all histologically proven renal neoplasms ( 100% ) were identified on ct urography . with regard to urothelial neoplasms ( table 2 ) , a calyceal process was depicted in eight cases . 
in one case , the lesion was not confirmed by histology on the surgical specimen after nephroureterectomy in a patient with other localisations of urothelial tumour , so the 3 - mm finding was therefore probably related to a clot or fibrin flake . 
one case of suspicious thickening of the calyceal wall was not confirmed by subsequent workup , and the histological diagnosis was inflammation of the pelvicalyceal collecting syste in two cases , the urothelial neoplasm was located in the renal pelvis ; one of these cases was confirmed by postoperative histology , whereas the other was not followed up at our hospital . in 30 patients , the finding involved the ureter . 
sono state eseguite ricostruzioni volume rendering 3d , maximus intensity projection ( mip ) 3d e mip a strato spesso , average intensity projection ( aip ) mpr sul piano coronale vero del rene e mpr curve ( cmpr ) con utilizzo del pacchetto software dedicato allo studio vascolare vessel probe lungo il decorso degli ureteri , con successiva correzione manuale . 
la valutazione stata eseguita utilizzando le ricostruzioni mpr eseguite e il volume di immagini visualizzate ad uno spessore di 3 mm sui piani assiale , coronale e sagittale . follow - up per ciascun paziente sono state considerate le indicazioni allesecuzione dellesame ed il suo esito , che stato poi valutato alla luce delleventuale precedente e successivo iter diagnostico seguito dal paziente stesso . 
questo tipo di approccio ha richiesto la presa visione di esami sia laboratoristici sia strumentali , quali citologia urinaria , ecografia e tc addominale , cistoscopia , cistouretrografia retrograda , e , se presenti , di interventi chirurgici con relativa diagnosi istologica . 
sono stati presi in considerazione i reperti degli esami eseguiti nel mese precedente luro - tc e per un follow - up medio successivo di 16 , 7 mesi ( range 434 mesi )  . risultati tra le 322 uro - tc eseguite , 169 hanno evidenziato significative alterazioni a carico dellapparato urinario e 153 non hanno evidenziato aspetti di rilievo . 
tra i 169 esami uro - tc positivi sono stati riscontrati , in alcuni casi nello stesso esame , i seguenti reperti : 11 varianti anatomiche , 15 processi neoplastici renali , 103 processi produttivi uroteliali ( 8 a livello caliceale , 2 a livello della pelvi renale , 30 a livello delluretere e 63 in sede vescicale ) , 38 casi di litiasi , 6 casi di infezione renale , 14 casi di sindrome del giunto , 3 casi di rene a spugna , 2 casi di necrosi midollare , 2 casi di fissurazione dei fornici caliceali , un diverticolo caliceale e un ureterocele . 
le 11 varianti anatomiche comprendono 5 casi di doppio radiol med ( 2010 ) 115 : 920935 table 2 comparison between neoplastic urothelial lesions recognised by ctu and patients clinical history . 
thirteen patients , not included , were lost to follow - up ctu diagnosis of urothelial neoplasm calyx - pelvis ( n = 6 ) ureter ( n = 23 ) bladder ( n = 61 ) true positive false positive veri positivi falsi positivi tabella 2 confronto fra la diagnosi di neoplasia uroteliale in uro - tc e la storia clinica del paziente ; in 13 casi , non presentati in tabella , il paziente stato perso al follow - up calico - pieliche ( n = 6 ) ureterali ( n = 23 ) vescicali ( n = 61 ) distretto unilaterale , 2 casi di doppio distretto bilaterale , 1 caso di triplo distretto , unagenesia renale , ureterale e della vescichetta seminale omolaterale e 2 casi di rene a ferro di cavallo . 
in un caso la lesione non stata confermata allesame istologico effettuato sul pezzo anatomico dopo una nefroureterectomia , eseguita in un paziente con altre localizzazioni di tumore uroteliale . pertanto il reperto , delle dimensioni di 3 mm , era verosimilmente espressione di un coagulo o di un fiocco di fibrina . 
in due casi il processo produttivo uroteliale si localizzava a livello della pelvi renale , uno di essi confermato dallesame istologico post - intervento ed laltro senza successivo follow - up presso il nostro ospedale . in 30 pazienti il reperto era a sede ureterale . 
in 16 di essi ci si era orientati per una franca neoplasia , mentre in 14 era stato segnalato un ispessimento parietale di dubbia natura in pazienti con altre localizzazioni di processo produttivo uroteliale . 
as regards the remaining 14 cases , in ten we are unaware of any specific ureteral histology being performed after endoscopic transurethral bladder surgery , whereas four were lost to follow - up . 
2a , b curved multiplanar reconstructions in the sagittal ( a ) and coronal ( b ) planes of the right ureter showing a pelvic ureteral wall thickening with luminal stricture ( arrows ) ; the urothelial neoplasm was confirmed by surgery . 
2a , b ricostruzioni cmpr sul piano sagittale ( a ) e coronale ( b ) delluretere destro che evidenziano un ispessimento della parete ureterale con riduzione del lume nel tratto pelvico ( frecce ) ; al successivo intervento di resezione stata confermata la presenza di un tumore uroteliale . 
in one case , the diagnosis was lithiasic pyonephrosis , which was confirmed by histology on the surgical specimen , whereas another patient had an active fungal infection , which had been suspected due to clinical history and ct finding of mobile filling defects and confirmed by subsequent ct studies and by response to therapy . 
in four patients , there was evidence of scarring due to previous renal infections , including one case of renal tuberculosis ; three of them were confirmed by subsequent follow - up , whereas one did not undergo other investigations . 
in three patients , the finding of risulta sia stata eseguita una verifica specifica in sede ureterale al successivo intervento di resezione vescicale endoscopica transuretrale , mentre in 4 casi non si hanno notizie del paziente al follow - up . 
per quanto riguarda la patologia non neoplastica , sono stati evidenziati 38 casi di patologia litiasica , confermati in base alla storia del paziente successiva allesame in 21 di essi , mentre per 17 pazienti non abbiamo riscontro ulteriore , per quanto lesame possa essere considerato sicuramente positivo anche senza ulteriore validazione da parte della storia clinica . 
in un caso stata posta diagnosi di pionefrosi metalitiasica confermata allesame istologico del pezzo operatorio , mentre in un altro paziente stata riconosciuta uninfezione micotica attiva , sospettata in base alla clinica ed al reperto uro - tc di radiol med ( 2010 ) 115 : 920935 fig . 
3a - c curved multiplanar reconstruction in the coronal plane ( a ) showing a focal wall thickening of the left ureter close to the bladder junction ( arrow ) , also visible on the axial image ( arrow in b ) , in a patient with surgically confirmed urothelial bladder neoplasm ( arrow in c )  . 
3a - c immagine cmpr sul piano coronale ( a ) che mette in evidenza un focale ispessimento delluretere nel suo tratto prevescicale ( freccia ) , visibile anche nellimmagine sul piano assiale ( freccia in b ) , diagnosticata al successivo intervento come flogosi cronica del corion , in paziente con evidenza di localizzazione vescicale di neoplasia uroteliale ( freccia in c ) , confermata allesame istologico . difetti di riempimento a livello pelvi - caliceale mobili con il decubito , confermata dagli esami tc successivi e dalla risposta alla terapia . 
in 4 pazienti erano riconoscibili gli esiti cicatriziali di infezioni renali pregresse , compreso un caso di tubercolosi renale ; 3 di essi sono stati confermati al successivo follow - up mentre uno non ha eseguito ulteriori esami . 
4 immagine aip sul piano assiale che mette in evidenza un piccolo difetto di riempimento ( freccia ) posteriormente al meato ureterale sinistro ; tale informazione si rilevata particolarmente utile per il cistoscopista , non essendo la lesione immediatamente visualizzabile ( conferma istologica di neoplasia vescicale )  . 
 la panoramicit dellesame tc ha permesso la stadiazione del tumore urinario , con il riconoscimento in 11 casi di interessamento linfonodale secondario , in un caso di trombosi neoplastica della vena renale e della vena cava inferiore , in un caso di multiple metastasi ossee , polmonari , epatiche , nonch lidentificazione in 3 casi di varianti anatomiche dei vasi renali , importanti per la programmazione dellintervento chirurgico . 
sono state riconosciute inoltre patologie extra - urinarie di diversa gravit in 143 / 322 casi ( 44 , 4% )  . dei 153 casi di uro - tc che non hanno evidenziato patologie di rilievo , in 79 casi non abbiamo un riscontro nella storia successiva del paziente , in 62 casi la negativit stata confermata ai successivi esami cistoscopici ed istologici , in un caso anche con esame istologico a livello ureterale , in 4 casi la negativit stata confermata da successivi esami di imaging , mentre in 8 casi lesame risultato falsamente negativo . 
il rilievo patologico in questi ultimi pazienti stato evidenziato in corso di cistoscopia per la presenza di sottili frange papillari in due casi , di lesioni papillomatose millimetriche in due casi , di unarea arrossata estesa per alcuni centimetri , ma non rilevata , in un caso . 
in tre pazienti nemmeno la cistoscopia era stata in grado di rilevare la formazione neoplastica , riconosciuta solo dallesame istologico su mapping vescicale , giustificato dalla presenza di cellule carcinomatose nelle urine . considerando le lesioni neoplastiche istologicamente accertate , nessuna lesione a livello della via escretrice intrarenale ed ureterale stata misconosciuta in corso di esame uro - tc . in 125 pazienti stato possibile effettuare un confronto fig . 
two patients with a history of previous urinary diversion had medullary necrosis , in one case with the presence of endoureteral blood clots , but no data from subsequent workup were available . 
6a , b left bladder - wall thickening visible on axial ( a ) and coronal ( b ) images in a patient with previous destructive pelvic surgery due to infiltrating rectal cancer . 
6a , b ispessimento parietale sinistro della vescica , visibile nelle immagini assiale ( a ) e coronale ( b ) , in paziente con esiti di intervento demolitivo pelvico per carcinoma infiltrante del retto , il quadro , giudicato sospetto alluro - tc , non stato confermato alla successiva cistoscopia . 
7a - c renal pelvis dilatation with delayed opacification and filling defects that were mobile with position changes [ axial images in supine ( a ) and prone ( b ) positions ] in a patient with pelvic junction syndrome complicated by clots and debris in the renal pelvis . 
7a - c dilatazione della pelvi renale con ritardo di opacizzazione e presenza di difetti di riempimento mobili con il decubito ( immagini assiali a paziente supino in a e prono in b ) per la presenza di detriti e coaguli , in paziente con sindrome del giunto . 
one patient showed evidence of blood clots in the bladder without additional wall lesions , a finding confirmed by subsequent cystoscopy . the panoramic capabilities of ct enabled staging of urinary neoplasms , with identification of nodal involvement in 11 cases , of neoplastic thrombosis of the renal vein and inferior vena cava in one and of multiple bone , lung and liver metastases in one . 
dei 51 pazienti valutati come positivi per patologia neoplastica vescicale , 47 sono stati riconosciuti positivi alla cistoscopia e 4 negativi ; dei 74 pazienti valutati come negativi alluro - tc , 66 hanno avuto un referto cistoscopico concorde e 8 discorde . 
i casi falsamente positivi corrispondono alla segnalazione di dubbi ispessimenti della parete vescicale , mentre negli 8 casi falsamente negativi la cistoscopia ha riconosciuto la presenza di un tumore papillomatoso di pochi millimetri in 2 casi , la presenza di frange papillari in 2 casi , la presenza di unarea arrossata non rilevata di alcuni centimetri in un caso e in 3 casi stato lesame istologico su mapping vescicale a dimostrare la presenza di neoplasia . 
9 immagini mip a strato sottile su piani obliqui , coronale ( a ) e sagittale ( b ) veri del rene destro ; si rileva diverticolo caliceale a partenza da un calice minore del gruppo superiore con formazione litiasica nel contesto . were confirmed negative by subsequent cystoscopy and histology , including in one case ureteral histology , and four were confirmed negative by subsequent imaging examinations . 
by contrast , in eight cases , ct examination proved to be false negative , and the pathological finding was revealed by cystoscopy , with the presence of thin papillary fronds in two cases , millimetre - sized papillomatous lesions in two discussione 94% , un valore predittivo positivo del 92% , un valore predittivo negativo dell89% , per una accuratezza diagnostica del 90% . luro - tc si affermata negli ultimi anni come eccellente radiol med ( 2010 ) 115 : 920935 and a reddened but not raised area extending over several centimetres in one . 
in three patients , cystoscopy failed to identify the neoplastic formation , which was only recognised at histological examination after bladder mapping due to the presence of malignant cells in the urine . 
considering the histologically proven neoplastic lesions , none of the intrarenal or ureteral lesions was missed at ct urography . for 125 patients , we performed a direct comparison between imaging findings at the bladder level and results of cystoscopy ( in some cases with histology ) performed within 110 days after ct urography ( table 3 )  . 
the four false positive cases correspond to the finding of a doubtful thickening of the bladder wall , whereas in the eight false negative cases , cystoscopy detected a millimetre - sized papillary bladder tumour in two cases , papillary fronds in two and a nonraised reddened area extending over several centimetres in one . 
these data correspond to a sensitivity of 85% , a specificity of 94% , a ppv of 92% and an npv of 89% , leading to a diagnostic accuracy of 90% . discussion ct urography has recently established itself as an excellent modality for studying the urinary system , and the technique is rapidly replacing ivu , which will probably survive only in centres not equipped with multislice ct scanners [ 4 , 9 , 11 , 12 ]  . 
compared with ivu , ct urography has the advantage of being far better tolerated by patients , as modalit di studio dellapparato urinario e questa tecnica sta rapidamente sostituendo lurografia tradizionale la quale probabilmente sopravvivr a breve solo nelle strutture prive della tc multistrato [ 4 , 9 , 11 , 12 ]  . infatti nel nostro istituto lurografia non viene pi eseguita dal maggio 2006 , pochi mesi dopo listallazione della tc multistrato a 64 strati . 
rispetto allurografia , luro - tc ha il vantaggio di essere estremamente meglio tollerata dal paziente , necessitando del solo digiuno preliminare , senza ulteriori preparazioni ( dieta , purganti , clismi evacuativi )  . 
anche lesecuzione della procedura pi rapida e pi confortevole dellurografia , non essendovi necessit di compressione ureterale , che oltretutto controindicata nei pazienti con aneurisma aortico o sottoposti a recente intervento chirurgico addominale . 
la maggior rapidit della procedura ha evidenti risvolti positivi sotto il profilo organizzativo [ 911 , 13 ]  . luro - tc un esame panoramico , che consente nella stessa seduta di valutare non solo le vie escretrici , ma anche il parenchima renale e le altre strutture addominali , come testimoniato dallelevato numero di reperti collaterali , anche di notevole impatto clinico , che abbiamo riscontrato . 
lutilizzo della tecnica di iniezione split - bolus per la somministrazione del mezzo di contrasto , con lacquisizione di una fase combinata nefro - urografica , consente di ridurre notevolmente la dose di esposizione al paziente , a fronte di un elevato numero di informazioni diagnostiche [ 4 , 10 , 11 , 13 ]  . 
nei 264 pazienti del nostro studio che si presentavano con sospetto di tumore uroteliale , quindi in presenza di ematuria , dilatazione delle vie escretrici inspiegata , esame citologico positivo per la presenza di cellule atipiche o carcinomatose , reperto cistoscopico positivo o nel follow - up di una pregressa table 3 comparison between computed tomograpjy urography ( ctu ) and cystoscopy and / or pathology diagnoses in bladder evaluation cystoscopy and / or pathology positive negative uro - tc positive negative total positiva negativa totale tabella 3 confronto fra la diagnosi delluro - tc e della cistoscopia e / o istologia a livello vescicale cistoscopia e / o referto istologico positivi negativi total totale 932 radiol med ( 2010 ) 115 : 920935 it requires only a preliminary fast without further preparation ( diet , laxatives , cleansing enemas )  . 
even the performance of ct urography is faster and more comfortable than ivu , as there is no need for ureteral compression , which is in any case contraindicated in patients with aortic aneurysm or recent abdominal surgery . 
the greater rapidity of the procedure leads to clear advantages in organisational terms [ 911 , 13 ]  . ct urography is a panoramic study that allows simultaneous evaluation not only of the urinary tract but also of the renal parenchyma and other abdominal structures , as testified by the large number of collateral findings some also clinically very relevant identified in our series . 
the use of the split - bolus technique for contrast administration , with acquisition of a combined nephrographic and excretory phase , enables considerable reduction in radiation dose to the patient while providing a large amount of diagnostic information [ 4 , 10 , 11 , 13 ]  . 
for the 164 patients ( 62% ) for whom we had subsequent diagnostic data ( table 4 ) , considering the overall result of the examination and the single findings , positive diagnoses were confirmed in 93 cases ( 97.8% ) and refuted in two ( 2.2% ) , whereas negative results were confirmed in 64 cases ( 92.8% ) , and refuted in five ( 7.2% ) , in which the patient effectively had a small urothelial tumour of the bladder , which was missed at ct . 
these values are in line with our data , from which we can determine , although imprecisely given the lack of confirmatory evidence in some patients , a sensitivity per patient of 95% , a specificity of 97% , a ppv of 98% and a npv of 93% , leading to a diagnostic accuracy of 96% . 
given the frequency of synchronous urothelial neoplasms in our series , in patients with other positive urothelial findings , we decided to report even those cases of ureteral thickening without clear signs of malignancy , such as uniform thickening causing neither stenosis nor luminal irregularity , to enable them to be further investigated . 
it is clear that this sort of finding should not lead directly to ureteral resection or nephroureterectomy procedures but requires further evaluation with ureteroscopy and neoplasia uroteliale , stata riconosciuta una patologia urinaria in 135 casi ( 51 , 1% )  . 
in particolare si trattava di patologia neoplastica in 92 pazienti ( 68 , 1% ) e di altro tipo di patologia ( rene a spugna , litiasi , infezione , sindrome del giunto , stenosi cicatriziale ) in 43 casi ( 31 , 9% )  . 
per i 164 pazienti ( 62% ) di cui possediamo un riscontro diagnostico successivo ( tabella 4 ) , considerando lesito generale dellesame e non i singoli reperti , la diagnosi positiva stata confermata in 93 casi ( 97 , 8% ) e smentita solo in 2 pazienti ( 2 , 2% ) , la negativit stata confermata in 64 casi ( 92 , 8% ) , mentre in 5 casi ( 7 , 2% ) il paziente presentava in realt una neoplasia uroteliale a livello vescicale , seppur di dimensioni ridotte , che non era stata riconosciuta . 
 [ 9 ] , analizzando la letteratura , hanno riportato una sensibilit nellidentificazione della causa di ematuria variabile fra il 92 , 4% e il 100% , con una specificit dell89 , 0%97 , 4% , in linea , quindi , con i nostri dati dai quali si pu calcolare , seppure in modo impreciso per lassenza di una conferma dei reperti in tutti i pazienti , una sensibilit per paziente del 95% , una specificit del 97% , un valore predittivo positivo del 98% e negativo del 93% , per unaccuratezza diagnostica del 96% . 
nella nostra casistica , alla luce della frequenza di lesioni neoplastiche uroteliali sincrone , si deciso di segnalare nei pazienti con altra positivit uroteliale anche quegli ispessimenti ureterali senza segni chiari di malignit , quali gli ispessimenti uniformi che non determinano n stenosi n irregolarit del lume , affinch venissero sottoposti ad ulteriori accertamenti . 
appare evidente come un rilievo di questo tipo non debba condurre direttamente ad un intervento di resezione ureterale o di nefroureterectomia , ma debba richiedere una valutazione mediante ureteroscopia ed eventuale biopsia , prima di programmare liter terapeutico del paziente . la possibilit di avere un riscontro diretto dei reperti uro - tc , sia positivi che negativi , nei pazienti sottoposti anche a cistoscopia nei giorni prossimi allesame , ci ha permesso di calcolare in modo accurato la validit diagnostica delluro - tc nel riconoscimento della patologia vescicale , che risulta particolarmente elevata , in linea con i migliori risultati presenti in letteratura [ 4 , 9 , 20 ] , con una sensibilit dell85% , una specificit del 94% , un valore predittivo positivo del 92% , un valore predittivo negativo dell89% , per una accuratezza diagnostica del 90% . 
bisogna sottolineare , inoltre , come i casi falsamente positivi da noi individuati corrispondano a quei pazienti in cui era stato riscontrato un reperto dubbio a livello vescicale , con consiglio di verifica cistoscopica , mentre i casi radiol med ( 2010 ) 115 : 920935 table 4 comparison between computed tomography urography ( ctu ) and patient history in 164 of 264 patients with suspected urinary neoplasm and available follow - up positive patient history negative positive negative total uro - tc positiva negativa totale positiva storia clinica negativa total totale tabella 4 confronto fra esito dellesame uro - tc e successiva storia clinica nei 164 dei 264 pazienti con sospetta patologia neoplastica urinaria di cui possediamo riscontro al follow - up possibly biopsy before planning the treatment strategy . the possibility of having direct confirmation of both positive and negative ct urography findings for patients who underwent cystoscopy within a few days of the examination allowed us to accurately calculate the diagnostic performance of ct urography in detecting bladder disease . 
this was found to be particularly high , in keeping with the best results published in the literature [ 4 , 9 , 20 ] , with a sensitivity of 85% , a specificity of 94% , a ppv of 92% , an npv of 89% and a diagnostic accuracy of 90% . 
moreover , it should be noted that the false positive cases refer to patients with doubtful bladder findings who were recommended for cystoscopy , whereas the true positive cases were all confirmed . 
its sensitivity is burdened , however , by a limitation that probably cannot be overcome and is related to the detection of small millimetre - sized protruding tumours or lesions that do not cause wall thickening . 
in our series , in addition to the five cases in which cystoscopy identified findings undetected at ct urography such as a urothelial discolouration ( n = 1 ) , urothelial irregularity in the form of thin papillary fronds ( n = 2 ) or millimetre - sized protruding lesions ( n = 2 ) there were three cases in which neither ct urography nor cystoscopy succeeded in identifying the lesions responsible for positive urine cytology , lesions that were only identified by histology after bladder mapping with random sampling . 
in addition , ct urography findings can guide the performance of cystoscopy as demonstrated in two of our patients : in one , a small neoplastic lesion located posterior to the ureterovesical junction in a bladder with extensive considerati sicuramente positivi sono stati tutti confermati . 
accanto allelevata specificit , lesame uro - tc presenta anche una buona sensibilit nella valutazione della vescica , gravata per da un limite , probabilmente invalicabile , rappresentato dal riconoscimento di tumori aggettanti di dimensioni di pochi millimetri , oppure di lesioni che non determinano un aumento dello spessore di parete . 
nella nostra casistica abbiamo rilevato 5 casi in cui la cistoscopia ha riconosciuto lesioni non visibili in uro - tc , come la presenza di unalterazione cromatica dellurotelio ( 1 caso ) , la sua irregolarit sottoforma di sottili frange papillari ( 2 casi ) , o millimetrici processi aggettanti ( 2 casi ) , ma in 3 casi n luro - tc n la cistoscopia sono state in grado di identificare la lesione responsabile della positivit citologica urinaria , individuata invece dallesame istologico su mapping vescicale con prelievi randomizzati . 
i reperti uro - tc possono , inoltre , guidare lesecuzione della cistoscopia come dimostrato in due pazienti della nostra casistica , ove in un caso una lesione neoplastica di piccole dimensioni localizzata posteriormente al meato ureterale in una vescica con ampie trabecolature stata individuata grazie alla precisa indicazione radiologica , mentre in un altro caso la biopsia effettuata in corrispondenza dellispessimento parietale descritto dalluro - tc , pur in assenza di alterazioni visibili dellurotelio , risultata positiva per neoplasia . 
 [ 4 ] luro - tc , grazie al suo elevato valore predittivo negativo , sembra poter giocare un importante ruolo come unico esame nei pazienti con 934 radiol med ( 2010 ) 115 : 920935 trabeculation was identified thanks to the precise radiological indication ; in the other , a biopsy at the site of wall thickening identified by ct , though in the absence of visible urothelial changes , proved to be positive for neoplas according to silverman et al . 
 [ 4 ] , ct urography , with its high npv , appears able to play an important role as the sole examination required in patients with microscopic haematuria and a low risk of bladder cancer . 
in selected patients , this examination showed a high level of diagnostic accuracy , higher than that of conventional ct urography , especially in lesions < 5 mhowever , the examination is rather laborious and fails to exhaustively answer the clinical question regarding the cause of haematuria , as it is limited to the bladder ( which is readily , albeit invasively , studied by the urologist ) and excludes evaluation of the upper urinary tract . the major barrier to ct urography is not its diagnostic accuracy but radiation dose . 
in our clinical practice , ct urography is not considered a standardised examination but it is always adapted to the clinical question and to the patients age as regards both number of phases and scan parameters . 
whenever possible , we omit the unenhanced scan and use the split - bolus technique to obtain information on both the renal parenchyma and urinary tract with a single scan . 
with this approach , we are able to deliver a dose ranging between 6 and 30 msv ( 1416 msv on average depending on patient size ) that is , at the lower end of the spectrum reported in the literature . ematuria microscopica ma a basso rischio per neoplasia vescicale , sebbene questa considerazione si basi sui dati pubblicati da sadow et al . 
tale esame ha dimostrato unelevata accuratezza diagnostica in pazienti selezionati , maggiore rispetto allesame uro - tc convenzionale , particolarmente nelle lesioni sotto i 5 mm , va peraltro rilevato come tale esame sia piuttosto indaginoso e soprattutto come non risponda completamente al quesito clinico di ricerca della causa di ematuria , limitandosi allo studio vescicale , agevolmente , seppur invasivamente effettuato dagli urologi , mentre le alte vie escretrici rimangono escluse dalla valutazione . il limite pi importante allutilizzo delluro - tc non risulta essere laccuratezza diagnostica , ma la dose di radiazioni cui vengono sottoposti i pazienti . 
nella nostra pratica clinica luro - tc non considerato un esame standardizzato , ma viene sempre modulato in base al quesito clinico e allet del paziente sia per quanto riguarda il numero di fasi che i parametri di scansione . 
quando possibile evitiamo di eseguire la scansione diretta , utilizzando la tecnica del doppio bolo otteniamo informazioni sia sul parenchima renale che sulla via escretrice con ununica scansione e solo in un numero molto limitato di casi si ricorsi allesecuzione di un ulteriore scansione , comunque limitata per estensione allo studio del solo reperto dubbio . questi accorgimenti fanno s che la dose da noi erogata vari in un range tra 6 e 30 msv ( in media 1416 msv in base alle dimensioni del paziente ) , ai limiti inferiori dei valori riportati dalla letteratura . conclusioni conclusions data collected over 30 months of experience with ct urography performed with 64 - slice ct equipment demonstrated the high diagnostic value of the examination both for benign and for malignant diseases . 
ct urography may shorten the diagnostic workup of patients with a definite ct finding of bladder neoplasm by the direct recommendation of patients for rigid cystoscopy and thus for a combined diagnostic and therapeutic procedure in a single session . i dati relativi allesperienza acquisita in 30 mesi di uro - tc eseguite mediante apparecchiatura a 64 strati hanno dimostrato lelevato valore diagnostico dellesame sia nella patologia benigna che in quella maligna . 
medica , villaricca ( na ) , 2010 isbn 978 - 88 - 90021 - 21 - 2 published online : 20 september 2010 springer - verlag 2010 defined as a hand - book by the chief editor , this easy to read text was conceived and planned as a practical guide to ultrasound ( us ) evaluation of the gastrointestinal tract in children . 
the opening chapter describes gastrointestinal embryology , us technique and normal findings of the gastrointestinal tract and is followed by chapters on the oesophagus , gastro - oesophageal reflux , hypertrophic pyloric stenosis , malrotation and volvulus , intussusception , appendicitis , chronic inflammatory bowel disease and infectious enteritis . each chapter deals with the clinical , pathological and us findings of the treated condition . 
he describes all possible diagnostic problems of this difficult , sometimes elusive clinical entity , and tricks to resolve these in order to advance the final correct diagnosis and avoid unnecessary surgery to children . the style used throughout the text is colloquial , practically a direct conversation between the author ( and his coauthors ) and the reader : this is highlighted in special comments and warning boxes , planned to draw attention to important diagnostic details . 
these are properly correlated with the images , which are well chosen and clearly reproduced . in the dedication of the book ( amongst others ) , to his daughters , the author cites them as a cause of delay in its preparation . 
i would also add that they may have been a possible source of carelessness in the draft review process and the ensuing at large misprints to be found in the text as well as in the references layout and format , misprints that surely will be corrected in a future second edition . definito dallautore come un manuale questo volumetto , agile e di facile lettura , stato concepito e programmato come una guida pratica alla valutazione ecografia dellapparato digerente nellet pediatrica ed i suoi nove capitoli sono dedicati allattuazione e chiarimento di tale proponimento . il capitolo iniziale descrive lembriologia dellapparto digerente , le tecniche ed i reperti normali dello studio ecografico ed seguito dai capitoli dedicati ad esofago , reflusso gastro - esofageo , stenosi ipertrofica del piloro , malrotazione e volvolo , invaginazione , appendicite , malattie infiammatorie croniche dellintestino ed enteriti infettive . ciascun capitolo tratta il quadro clinico - patologico , ed i reperti ecografici tipici dellaffezione in studio . 
questultimo argomento sembra essere il cavallo di battaglia dellautore che descrive tutti i possibili problemi diagnostici di questa difficile e talvolta elusiva entit clinica nonch i trucchi per risolverli , in modo tale da poter porre diagnosi finali corrette e precise ed evitare cos inutili interventi chirurgici . lo stile di presentazione della materia lungo tutto il testo colloquiale , praticamente come un discorso diretto tra lautore ( ed i suoi co - autori ) ed il lettore : ci messo ben in evidenza in appositi riquadri di commento ed avvertimento , concepiti per porre lattenzione su di importanti aspetti diagnostici . 
a questi riquadri ben si correlano le immagini , scelte con cura e ben riprodotte . nella dedica al volume viene fatto cenno , tra gli altri , alle figlie dellautore , chiamate in causa quale possibile motivo di ritardo nella preparazione del testo . 
fineschi crc press , taylor & francis group boca raton , fl , usa , 2010 isbn 978 - 1 - 4398 - 0064 - 5 published online : 20 september 2010 springer - verlag 2010 it is unusual to review a book dealing in a radiological journal that relates to autopsies , but the development of diagnostic imaging in all areas of medicine has led radiologists to use the most advanced diagnostic methods , applying them also to the fields of forensics and autopsy . 
as was brought to the fore at the recent sirm congress in verona , virtual autopsy has made its powerful entry into the world of radiology , and our colleagues involved in legal medicine , as well as the judicial authorities , increasingly request the use of ct as a diagnostic aid during autopsies . 
 in many cases , the imaging technique is referred to as the virtopsy ; that is to say , it is a virtual autopsy accomplished using ct , which can substitute for the autopsy undertaken on a dissecting table . 
however , as evidenced in the book , conventional autopsy remains irreplaceable , and cooperation between the two professions forensic pathology and radiology remains essential for the proper interpretation of any findings . 
 in this handsome volume , aimed primarily at forensic pathologists , there is a chapter on postmortem radiology and digital imaging , edited by professor giuseppe guglielmi , which covers this topic well and which may prove extremely useful to radiologists who are required to deal with this procedure . 
 in the immediate future , if radiologists choose not to become involved in the virtopsy field , they risk losing professional and scientific research opportunities that will be increasingly in demand as the area of legal medicine develops . insolito recensire in una rivista di radiologia un libro che tratta di autopsie , ma levoluzione della diagnostica per immagini in tutti gli ambiti di attivit medica ha portato i radiologi ad utilizzare anche in campo forense ed autoptico le metodiche diagnostiche pi avanzate . 
come ben trattato al recente congresso della societ italiana di radiologia medica ( sirm ) di verona , lautopsia virtuale ha fatto prepotentemente ingresso nel mondo radiologico e sempre pi spesso richiesto , dai colleghi medico legali o dalla autorit giudiziaria , di utilizzare la tomografia computerizzata ( tc ) come ausilio diagnostico per le autopsie . in molti casi si ritiene che la virtopsy , cio lautopsia virtuale compiuta con la tc , possa sostituire quella effettuata al tavolo anatomico , ma , come dimostrato nel libro , lesame autoptico rimane insostituibile e la collaborazione tra le due figure professionali del medico legale e del radiologo risulta essere indispensabile per la corretta interpretazione dei reperti . in questo bel volume , dedicato soprattutto ai medici legali , vi un capitolo dedicato postmortem radiology and digital imaging , curato dal prof  . 
bellomi1 , 2 1divisione di radiologia , istituto europeo di oncologia irccs , via ripamonti 435 , 20141 milano , italy 2facolt di medicina e chirurgia , universit degli studi di milano , via festa del perdono 7 , 20122 milano , italy correspondence to : m . 
perfusion computed tomography ( ctp ) is a readily available and widely used tool that allows an objective measurement of tissue perfusion through the mathematical analysis of data obtained from repeated scans performed after administration of contrast agent . 
recently , ctp has been increasingly used in the oncological field , being studied as a potential marker of neoplastic angiogenesis , which is one of the main targets of new tumour therapies . 
the aim of this paper was to provide the theoretical background and practical guidance for accurately performing ctp and interpreting results of examinations in solid - body tumours . ctp could be a valid tool for functional imaging of tumours if the acquisition technique is robust , if image and data analysis is accurate and if interpretation of results is adequately inserted within a clinical context . keywords ct perfusion oncology therapy monitoring therapy response solid tumors riassunto limaging funzionale sta acquisendo un ruolo sempre pi importante , sia nella ricerca che nellattivit clinica della diagnostica per immagini . 
la tomografia computerizzata perfusionale ( tcp ) una tecnica ampiamente disponibile e diffusa sul territorio , che permette di misurare oggettivamente la perfusione di un tessuto , attraverso lanalisi matematica dei dati ottenuti da scansioni ripetute nel tempo dopo la somministrazione di mezzo di contrasto . la tcp ha recentemente visto ampliare il suo impiego in ambito oncologico , perch viene studiata come possibile marcatore della angiogenesi neoplastica , che uno dei principali target delle nuove terapie dei tumori . 
la tcp potrebbe essere uno valido strumento per limaging funzionale dei tumori , se la tecnica di acquisizione robusta , se lanalisi di immagini e dati accurata e se linterpretazione dei risultati adeguatamente inserita nel contesto clinico . parole chiave tc perfusionale oncologia monitoraggio della terapia risposta alla terapia tumori solidi del corpo introduction introduzione images obtained with computed tomography ( ct ) in baseline conditions and after intravenous administration of le immagini ottenute con la tomografia computerizzata ( tc ) in condizioni basali e dopo la somministrazione 844 radiol med ( 2010 ) 115 : 843857 iodinated contrast material allow for high accuracy levels in diagnosing and characterising numerous tumour types . the relatively low costs , the broad spectrum of diseases that can be investigated , the simple standardisation of protocols and the wide availability of scanners have made ct the main diagnostic technique for staging tumours and monitoring antitumour therapy . 
the techniques high spatial resolution enables precise and repeatable measurements [ 1 ] of tumour dimensions such that in many regions they are comparable with pathology findings [ 25 ] and are able to fulfil criteria for monitoring tumour response to universally recognised treatment regimens : unidimensional for the response evaluation criteria in solid tumours ( recist ) and bidimensional for the world health organization ( who ) [ 6 ]  . however , research has always been centred on tumour biology . 
potential biomarkers of angiogenesis used immunohistochemical to date biomarkers such as microvessel density ( mvd ) and vascular endothelial growth factor ( vegf ) ; and serum biomarkers such as circulating endothelial cells ( cec ) have produced encouraging results , albeit somewhat inhomogeneous [ 11 ]  . 
in addition , these potential biomarkers involve expensive , invasive and not widespread techniques , such that they seem poorly suitable for serial monitoring of anti - angiogenic therapies in routine clinical practice . 
there is , therefore , tremendous interest in the development of a relatively inexpensive , noninvasive and widely available tool that can provide information on the angiogenic characteristics of tumours and monitor the effects of anti - angiogenic therapies . in recent years , imaging modalities have been developed that can noninvasively obtain both qualitative and quantitative information regarding angiogenic characteristics of tumours , such as perfusion computed tomography ( ctp ) , dynamic contrast - enhanced magnetic resonance imaging ( dce - mri ) and dynamic contrast - enhanced ultrasound ( dce - us )  . 
the number of scientific publications that describe ctp applications in oncology is constantly increasing , both due to the growing use of anti - angiogenic therapies in routine clinical practice and to the widespread availability of multislice ct systems , which has made ctp decidedly competitive with respect to other imaging modalities [ 12 , 13 ]  . 
even though dce - mri and dce - us are in theory preferable to ctp given the absence of ionising radiation , they are in reality less used , most likely due to the lack of standardisation of examination technique and data analysis . endovenosa di mezzo di contrasto ( mdc ) iodato permettono di ottenere elevati livelli di accuratezza nella diagnosi e caratterizzazione di numerosi tumori . 
i costi relativamente bassi , lampio spettro di patologie indagabili , la facile standardizzazione dei protocolli e lampia disponibilit sul territorio , hanno fatto s che la tc sia la tecnica diagnostica principale nella stadiazione dei tumori e nel monitoraggio delle terapie anti - tumorali . 
lelevata risoluzione spaziale consente misurazioni esatte e ripetibili [ 1 ] delle dimensioni delle lesioni neoplastiche , tanto da essere paragonabili a quelle dellanatomia patologica in molti distretti [ 25 ] e da soddisfare i criteri di monitoraggio della risposta dei tumori alle terapie universalmente riconosciuti : monodimensionali per il response evaluation criteria in solid tumors ( recist ) e bidimensionali per il world health organization ( who ) [ 6 ]  . la ricerca tuttavia , sempre pi indirizzata allo studio della biologia dei tumori : in particolare , langiogenesi neoplastica ritenuta un importante fattore prognostico [ 79 ] e un promettente target di nuove terapie [ 10 ]  . 
la valutazione dellattivit angiogenetica dei tumori ancora oggetto di studio : i potenziali biomarker dellangiogenesi fino a oggi utilizzati , sia immunoistochimici , come la conta dei microvasi ( mvd ) e la determinazione dei recettori per il fattore di crescita vascolare endoteliale ( vegf ) , che sierici , come la conta delle cellule endoteliali circolanti ( cec ) , hanno dato risultati incoraggianti , ma poco uniformi [ 11 ]  . 
questi potenziali biomarker , inoltre , richiedono tecniche costose , invasive e non diffuse sul territorio : essi sembrano poco adatti per il monitoraggio seriale delle terapie anti - angiogenetiche nella routine clinica . 
c pertanto un grande interesse per lo sviluppo di uno strumento poco costoso , non invasivo e disponibile sul territorio , che sia in grado di fornire informazioni sulle caratteristiche angiogenetiche dei tumori e di monitorare leffetto delle terapie anti - angiogenetiche . sono state sviluppate negli ultimi anni metodiche di imaging che permettono di ottenere in maniera non invasiva informazioni sia qualitative che quantitative sulle caratteristiche angiogenetiche dei tumori , come la tc perfusionale ( tcp ) , la risonanza magnetica dinamica ( dce - mr ) e lecografia dinamica ( dce - us ) con mezzo di contrasto . 
il numero di pubblicazioni scientifiche che descrivono applicazioni della tcp in oncologia in continuo aumento , sia per il crescente utilizzo di terapie anti - agiogenetiche nella routine clinica , sia per lelevata disponibilit sul territorio della tc multistrato , che ha reso la tcp assai competitiva rispetto alle altre metodiche di imaging [ 12 , 13 ]  . 
sebbene la dce - mr e la dce - us siano in teoria favorite rispetto alla tcp per lassenza di radiazioni ionizzanti , esse sono in radiol med ( 2010 ) 115 : 843857 the aim of this paper is to provide the reader with a brief theoretical background and a practical guide to performing ctp examinations . realt meno utilizzate , probabilmente per la mancanza di una standardizzazione nella tecnica di esecuzione e nellanalisi dei dati . theoretical background perfusion is defined as blood flow through a unit volume of tissue per unit of time [ 14 ]  . 
ctp is a theoretical tool able to objectively quantify ( with the use of mathematical models and dedicated software ) the real perfusion of tissues in that it only measures the density difference produced by the contribution of contrast material ( and therefore of blood ) to tissues . 
ctp is based on two indispensable technical requirements . the first is the performance of repeated ct scans of the volume being analysed ( also known as dynamic , cine or perfusion scans )  . 
these need to be acquired before , during and after intravenous administration of iodinated contrast material to enable the study of density variations over time . the density measured by ct in the unit volume ( voxel ) , i.e. attenuation of x - rays expressed in hounsfield units ( hu ) , is directly proportional to the quantity of contrast material present within it [ 15 ]  . 
the contrast material contained within the tissue volume being studied is due to contrast material in vessels and contained in the extravascular / cellular space ( or more simply , interstitial space ) due to passive diffusion [ 16 , 17 ]  . the second requirement is the selection of the arterial input . 
for a description of other kinetic models , the reader is invited to consult specific publications [ 15 , 19 ]  . two - compartment ( or patlak ) analysis sees the vascular compartment and the extravascular / cellular compartment as distinct and quantifies exchange between them [ 20 ]  . 
it gli scopi di questo lavoro sono di fornire al lettore un breve background teorico e una guida pratica per la esecuzione degli esami di tcp . background teorico la perfusione definita come il trasporto di sangue allunit di volume di tessuto nellunit di tempo [ 14 ]  . 
essa si riferisce , pertanto , al trasporto attraverso il sangue di ossigeno e nutrienti ai tessuti , che avviene a livello dei microvasi capillari , ed nettamente diversa dal concetto di velocit del sangue , che si applica a livello dei grossi vasi . 
la tcp uno strumento teoricamente in grado di quantificare ( attraverso lutilizzo di modelli matematici ) in maniera oggettiva ( grazie allutilizzo di software dedicati ) la perfusione reale dei tessuti , in quanto essa misura solo la differenza di densit prodotta dallapporto di mdc ( e quindi di sangue ) ai tessuti . 
 il primo lesecuzione di scansioni tc ripetute nel tempo del volume in analisi ( dette anche scansioni dinamiche , cineo perfusionali ) : queste devono essere acquisite prima , durante e dopo la somministrazione endovenosa di mdc iodato , in modo da poter studiare le variazioni della densit nel tempo . 
grazie a questo paragone possibile distinguere la quantit di mdc allinterno dei vasi ( compartimento vascolare ) da quella presente nellinterstizio ( compartimento extra - vascolare / cellulare )  . 
 in questo lavoro sono descritti i modelli cinetici utilizzati nei software commerciali per la tc perfusionale dei tumori del corpo [ 18 ] ; per la descrizione degli altri modelli cinetici , si rimanda alle pubblicazioni specifiche [ 15 , 19 ]  . 
 846 radiol med ( 2010 ) 115 : 843857 il modello cinetico di tipo bi - compartimentale ( o di patlak ) considera distinti il compartimento vascolare e il compartimento extravascolare / cellulare ( o interstizio ) e ne quantifica gli scambi [ 20 ]  . 
esso fornisce una stima del volume di sangue allinterno dei microvasi ( blood volume , bv ) e della frazione di estrazione ( fe ) , detta anche costante di transito ( ktrans ) , che la somma del flusso allinterno dei microvasi e della permeabilit capillare ( appendice 1 )  . 
la perfusione pu essere calcolata come il rapporto tra la massima pendenza della curva densit / tempo del tessuto e il picco di densit raggiunto dallarteria selezionata come input arterioso . 
il vantaggio principale di questo metodo quello di consentire il calcolo della perfusione con scansioni di breve durata , in quanto la curva densit / tempo del tessuto raggiunge la sua massima pendenza assai prima del suo picco di densit . 
le scansioni di breve durata sono definite in modo da includere solo il primo passaggio del mezzo di contrasto nel volume in analisi ( first pass ) , per evitare che il ricircolo del sangue possa interferire con la quantificazione della perfusione ; esse , inoltre , offrono il vantaggio di poter essere effettuate a respiro sospeso nei distretti critici , limitando la possibilit di avere artefatti da movimento . 
la perfusione , infatti , calcolata utilizzando solo quattro immagini : la basale , quella nel momento del picco di densit dellarteria e le due successive , che mostrano le maggiori differenze di densit nei tessuti . 
la presenza di rumore in una di queste immagini pu inficiare la quantificazione della perfusione ( appendici 1 e 2 ) [ 19 ]  . il modello cinetico della deconvoluzione applica unoperazione matematica di deconvoluzione per paragonare le curve densit / tempo ottenute dallinput arterioso e dal tessuto in analisi , al fine di ottenere una curva teorica di concentrazione ( di mdc nel tessuto in analisi ) / tempo , detta funzione dellimpulso residuo ( irf ) [ 21 ]  . 
utilizzando la prima parte della curva di concentrazione del mdc nel tessuto applicabile lassunto che il mdc sia solo allinterno del compartimento vascolare ; cos possibile calcolare il flusso di sangue ( bf ) , il volume di sangue ( blood volume , bv ) e il tempo di transito medio del sangue ( mean transit time , mtt ) allinterno dei microvasi secondo il central volume principle bf = bv / mtt . 
nella realt il mdc si distribuisce nel solo compartimento vascolare nel parenchima encefalico sano , dove la barriera emato - encefalica ne impedisce extravascolare / cellulare , nel testicolo e nella retina ; in tutti gli altri organi il mdc diffonde attraverso i capillari nellinterstizio [ 22 ]  . 
il grafico riporta in ordinata le hu e in ascissa il tempo , espresso in millisecondi ( ms )  . provides an estimate of blood volume ( bv ) within the microvasculature and the extraction fraction ( ef ) , also known as the transit constant ( ktrans ) , which is the sum of the flow within the microvasculature and capillary permeability ( appendix 1 )  . one - compartment analysis ( or slope method ) enables the calculation of perfusion with short - duration perfusion scans . perfusion can be calculated as the ratio between the maximum slope of the density / time curve of tissue and the peak density reached by the artery selected as arterial input . the main advantage of this method is that it allows the calculation of perfusion with short - duration scans , in that the density / time curve of tissue reaches its maximum slope well before peak density . 
in addition , they offer the advantage of being able to be performed in conditions of breath - hold in critical regions , thus limiting the possibility of motion artefacts . 
perfusion is , in fact , calculated by using only four images : the baseline image , radiol med ( 2010 ) 115 : 843857 the image obtained at peak density of the artery and the two subsequent images that show the greatest differences in tissue density . 
the presence of noise in one of these images can invalidate perfusion quantification ( appendices 1 , 2 ) [ 19 ]  . deconvolution - based perfusion analysis applies a mathematical operation of deconvolution to compare the density / time curves obtained from the arterial input and from the tissue being studied to obtain a theoretical concentration curve ( of contrast material in the tissue being studied ) / time , known as the residual impulse response function ( irf ) [ 21 ]  . 
in this fashion , blood flow ( bf ) , bv and mean transit time ( mtt ) of blood within the microvasculature can be calculated according to the central volume principle , whereby bf = bv / mtt . 
in reality , the contrast material is distributed in the vascular compartment only exclusively in the healthy brain parenchyma ( where the bloodbrain barrier hinders its passage into the extravascular / cellular compartment ) , in the testicles and in the retina . 
it can therefore be theoretically assumed that the contrast material is only in the vascular compartment in all other parenchyma if only the early scans are used for perfusion analysis ( within the first 4560 s from contrast material administration ) , with a maximum error of 15% [ 23 ]  . 
lawrence and lee adiabatic approximation , passage of contrast material into the interstitial compartment can be quantified , with inclusion in the perfusion analysis of the ct scans performed after the first pass ( therefore known as the interstitial phase )  . 
calculating the permeability surface ( ps ) is done according to the following equation : ps = bf [ ln ( 1e ) ] , where e is the fraction of contrast material that leaks into the interstitium from the vascular space ( ef ) ( appendix 3 )  . practical guide acquisition technique selection of volume of interest diffonde durante il suo primo passaggio ( first pass ) ; si pu assumere , pertanto , che il mdc sia in teoria solo nel compartimento vascolare anche in tutti gli altri parenchimi , se sono utilizzate per lanalisi di perfusione solo le scansioni precoci ( entro i 4560 secondi dallinizio della somministrazione del mdc ) , con un errore massimo del 15% [ 23 ]  . 
lawrence e lee , possibile quantificare il passaggio del mdc nel compartimento interstiziale , includendo nellanalisi di perfusione anche le scansioni tc effettuate dopo il first pass , nella fase detta , appunto , interstiziale . il calcolo della superficie di permeabilit ( ps ) avviene secondo la seguente equazione : ps = bf [ ln ( 1e ) ] , dove e rappresenta la frazione di mdc che fuoriesce nellinterstizio dallo spazio vascolare ( frazione di estrazione ) ( appendice 3 )  . guida pratica tecnica di acquisizione selezione volume di interesse necessario acquisire preliminarmente immagini tc senza mdc , con spessore di 2 , 55 , 0 mm per localizzare il tumore e selezionare il volume su cui effettuare le scansioni perfusionali . 
tale volume limitato lungo lasse z dal numero di detettori della tc utilizzata ( ad esempio , 20 mm per le apparecchiature tc a 16 strati e 40 mm per quelle a 64 strati [ 24 ] ) , se si decide di studiare il first pass , perch sono richieste scansioni ad elevata risoluzione temporale ( 1 secondo utilizzando un protocollo definito per lanalisi della perfusione con il modello cinetico della deconvoluzione ; 35 secondi utilizzando un protocollo definito per lanalisi della perfusione con il modello cinetico monocompartimentale o bi - compartimentale ) , possibili solo con il lettino fermo in una singola posizione . una maggiore copertura lungo lasse z possibile se si decide di studiare solo la fase interstiziale , perch sono sufficienti scansioni con bassa risoluzione temporale ( 1020 secondi ) [ 25 ]  . 
qualora il tumore avesse un volume maggiore rispetto a quello che le scansioni perfusionali possano includere , necessario identificare la sezione con la massima area visualizzabile del tumore e posizionare su di essa il centro del volume utilizzato per lo studio perfusionale . somministrazione del mezzo di contrasto baseline ct images without contrast material and with a thickness of 2.55.0 mm need to be acquired to locate the tumour and select the volume on which perfusion scans are to be done . 
this volume is limited along the z - axis by the utilizzato il mdc iodato convenzionale : preferibile un mdc con elevata concentrazione di iodio ( 370400 mg / l ) , perch esso determina un enhancement pi elevato nei tessuti e pu determinare benefici nella quantificazione della perfusione [ 25 ]  . 
in the event the tumour volume is greater than the volume that can be included in the perfusion scans , the section with the maximum visible area of the tumour should be identified and the centre of the perfusion study volume should be positioned over it . contrast material administration conventional iodinated contrast material is used . 
contrast material with a high iodine concentration ( 370400 mg / l ) is preferable because it produces greater tissue enhancement and can be beneficial in quantifying perfusion [ 25 ]  . 
contrast material is administered according to the short sharp bolus technique , whereby a short and concentrated bolus is obtained by administering a limited quantity of contrast material ( 4050 ml ) at high injection rate ( 46 ml / s ) , followed by 40 ml of saline at high injection rate ( 46 ml / s )  . this method is appropriate for perfusion analysis with the oneand two - compartment models , as well as with deconvolution . 
for longitudinal studies , where ctp is done on several occasions in the same patient at different times during treatment , administration of contrast material is best done via the same peripheral vein to avoid a possible source of variation . perfusion scan perfusion scans performed during the first pass ( up to 4560 s after the beginning of contrast material administration ) require high temporal resolution ( 1 s when using a protocol defined for deconvolution - based perfusion analysis ; 35 s when using protocols defined for oneor twocompartment analysis )  . 
perfusion scans performed during the interstitial phase after the first pass study with deconvolution need to done with a temporal resolution of 10 s and have a duration no greater than 2 min after the beginning of contrast material administration in order to apply the st . 
lawrence and lee adiabatic approximation . perfusion scans performed during the interstitial phase after the first - pass study with oneor two - compartment analysis need to be done with a temporal resolution between 10 and 20 s and duration between 2 and 10 min short sharp bolus , cio di un bolo breve e concentrato , ottenuto con la somministrazione di una quantit ridotta di mdc ( 4050 ml ) ad alto flusso ( 46 ml / s ) , seguito da 40 ml di soluzione fisiologica ad alto flusso ( 46 ml / s )  . 
tale modalit di somministrazione del mdc adeguata per lanalisi della perfusione sia con i modelli cinetici mono - compartimentale e bi - compartimentale , che con il modello cinetico della deconvoluzione . 
per gli studi longitudinali , in cui la tcp eseguita pi volte sullo stesso paziente in momenti diversi durante terapia , preferibile che la somministrazione del mdc avvenga sempre attraverso la stessa vena periferica , per escludere una possibile fonte di variabilit . scansioni perfusionali le scansioni perfusionali eseguite durante il first pass ( fino a 4560 secondi dallinizio della somministrazione del mdc ) necessitano di una elevata risoluzione temporale ( 1 secondo per i protocolli definiti per lanalisi di perfusione con il modello cinetico della deconvoluzione e 35 secondi per quelli definiti per lanalisi di perfusione con il modello cinetico di tipo monoo bi - compartimentale )  . 
le scansioni perfusionali eseguite durante la fase interstiziale dopo lo studio del first pass secondo il modello cinetico della deconvoluzione devono essere eseguite con risoluzione temporale di 10 secondi e avere una durata non superiore ai 2 minuti dopo linizio della somministrazione di mdc , in modo da applicare lapprossimazione adiabatica di st . 
le scansioni perfusionali eseguite durante la fase interstiziale dopo lo studio del first pass secondo il modello cinetico di tipo monoo bi - compartimentale devono essere eseguite con risoluzione temporale compresa tra i 10 e i 20 secondi e avere una durata compresa tra i 2 e i 10 minuti dopo linizio della somministrazione di mdc [ 18 , 25 ]  . ai fini del risparmio di dose , sono consigliati valori relativamente bassi di voltaggio ( 80100 kvp ) e di amperaggio ( 120200 ma ) per le scansioni perfusionali , come la maggior parte degli studi recentemente pubblicati riporta per diversi distretti corporei [ 2628 ]  . 
 [ 29 ] ha dimostrato che le scansioni perfusionali condotte con 80 kv permettono una riduzione della dose del 300% rispetto a quelle con 120 kv , a fronte di una perdita nel rapporto segnale / rumore soltanto dell11% . infine , consigliato , e pressoch universalmente utilizzato negli studi pubblicati [ 30 ] , uno spessore degli strati non inferiore ai 5 mm , che garantisce un equilibrio tra le esigenze di risoluzione spaziale e di rapporto segnale / rumore nelle scansioni perfusionali . correzione del movimento per unaffidabile analisi della perfusione con tc necessario limitare al massimo i movimenti del volume di tessuto radiol med ( 2010 ) 115 : 843857 after the beginning of contrast material administration [ 18 , 25 ]  . relatively low voltage ( 80100 kvp ) and current ( 120200 ma ) are recommended for dose - sparing purposes during perfusion scans , as most recently published studies report for different body regions [ 2628 ]  . 
 [ 29 ] showed that the dose of perfusion scans done with 80 kv is 300% less than the dose with 120 kv , whereas the loss in signalto - noise ratio ( snr ) is only 11% . 
lastly , a slice thickness of no less than 5 mm is advisable and is almost universally used in the published studies [ 30 ] , as this guarantees a balance between the needs of spatial resolution and snr in perfusion scans . motion correction a reliable analysis of perfusion with ct requires that the motion of the tissue volume being studied be kept to an absolute minimum during scans . 
the anatomical regions most subject to motion are the lower thorax and upper abdomen , due to diaphragmatic motion during breathing . to perform perfusion scans in these regions , the patient is best positioned supine with their arms behind their head , and the use of immobilisation devices is recommended . performing first - pass perfusion scans ( if a protocol defined for analysis with the deconvolution model is used ) with breath - hold is also recommended , after the patient has received adequate training in performing the technique . bowel peristalsis can cause motion artefacts : the administration of a hypotonic agent can reduce such artefacts . swallowing can cause significant motion artefacts in perfusion scans of the upper respiratory and digestive tracts , so patients should be prepared for the sensation of warmth due to the administration of contrast material and avoid swallowing . 
motion artefacts can also be corrected after acquisition of perfusion scans with the use of motion correction software , which improves the reliability of the ctp study . image and data analysis perfusion parameters are calculated with the use of dedicated software . 
per lesecuzione di scansioni perfusionali in queste regioni indicato porre il paziente in posizione supina con le braccia distese dietro la testa e avvolgere tali regioni con bande contenitive che ne riducano i movimenti ; inoltre raccomandabile eseguire le scansioni perfusionali del first pass ( se si utilizza un protocollo definito per lanalisi con il modello cinetico della deconvoluzione ) a respiro sospeso , dopo adeguato training del paziente . 
la deglutizione pu determinare importanti artefatti da movimento nelle scansioni perfusionali del tratto aero - digestivo superiore : il paziente deve essere preparato alla sensazione di calore dovuta alla somministrazione del mdc ed evitare la deglutizione . 
 possibile correggere il movimento anche dopo lacquisizione delle scansioni perfusionali , utilizzando software per la correzione del movimento , che migliorano laffidabilit dellanalisi della perfusione con tc . analisi di immagini e dati il calcolo dei parametri di perfusione avviene tramite lutilizzo di software dedicati . 
alcuni di essi sono in commercio , proposti da siemens ( erlangen , germania ) , philips ( best , olanda ) e general electric ( milwaukee , wi , usa ) [ 18 ] ; essi , pertanto , sono diffusi in molti centri e , in teoria , affidabili , perch gi validati prima della loro introduzione nel mercato ; altri software sono sviluppati autonomamente allinterno di singoli centri e , perci meno diffusi e , in teoria , sottoposti a un processo di validazione meno ampio . tali software sono di tipo semiautomatico , perch richiedono lintervento delloperatore per il posizionamento delle roi e lottimizzazione del processo , ma svolgono automaticamente lanalisi matematica dei dati . selezione dellinput arterioso deve essere posizionata una roi in corrispondenza di un vaso arterioso compreso nel volume di scansione . 
questa in teoria la condizione ideale per unaffidabile analisi di perfusione tc , in quanto linput arterioso specifico per ogni paziente e per ogni esame effettuato dallo stesso paziente in momenti diversi ; tuttavia , la selezione dellinput arterioso pu introdurre una fonte di variabilit . 
 una questione aperta , ad esempio , se il posizionamento della roi su unarteria dei tronchi sovra - aortici , destra vs sinistra o omolaterale vs contro laterale alla sede del tumore , possa essere fonte di variazioni nelle misure di perfusione , in relazione alle diversit anatomiche tra il lato destro e 850 radiol med ( 2010 ) 115 : 843857 operator input for to replace the roi and to optimise the process , but they automatically perform mathematical analysis of the data . selection of the arterial input an roi needs to be placed in a position corresponding to an artery included in the scan volume . 
this is , in theory , the ideal condition for reliable perfusion analysis in that the arterial input is specific for each patient and for each examination performed on the same patient at different times . 
it is an open question , for example , whether placement of an roi on an artery of supra - aortic trunks , right versus left or ipsilateral versus contralateral to the tumour , can be the source of variations in perfusion measurements , given the anatomical difference between the left and right side . 
for example , significant differences in perfusion parameters have been noted in patients with squamous cell carcinoma of the upper respiratory and digestive tracts when arterial input was placed on the external right or left carotid artery [ 31 ]  . 
another open question is artery selection , whether large calibre to avoid flow artefacts due to vessel tortuosity or small calibre because it is a direct tributary of the tumour . 
flow artefacts due to vessel tortuosity are considered negligible for arteries with a diameter > 45 mm [ 3234 ] , and no significant differences have been found in ctp parameters if arterial input is positioned on the external or internal carotid artery in patients with squamous cell carcinoma of the upper digestive tract , whether a tributary or nontributary artery of the tumour [ 32 ]  . 
in addition , many studies with ctp in various body regions successfully used the aorta or arteries that were not direct tributaries of the tumour [ 28 , 35 ]  . we therefore recommend that the arterial input selected be an artery with adequate diameter ( > 45 mm ) and well visualised in perfusion scans but not necessarily a tributary of the tumour itself . 
some software packages automatically define the first pass , although this automatic identification can prove to be inexact for protocols with perfusion scan duration greater than that of the first pass . 
sono state riscontrate , ad esempio , differenze significative nei parametri di perfusione in pazienti con carcinoma squamocellulare ( scca ) del tratto aero - digestivo superiore sottoposti a tcp quando linput arterioso posizionato sullarteria carotide esterna destra o sinistra [ 31 ]  . 
unaltra questione aperta la selezione dellarteria , se di grosso calibro , per evitare artefatti da tortuosit del flusso , o di piccolo calibro , perch direttamente tributaria del tumore . 
gli artefatti da tortuosit del flusso sono stati considerati trascurabili per le arterie con un calibro superiore a 45 mm [ 3234 ] e non sono state riscontrate differenze significative nei parametri di perfusione tc se linput arterioso posizionato sull arteria carotide esterna ( eca ) o interna ( ica ) in pazienti con scca del tratto digestivo superiore , rispettivamente , tributaria e non tributaria del tumore [ 32 ] ; inoltre , molti studi con tcp in vari distretti hanno utilizzato con successo come input arterioso laorta o arterie non tributarie direttamente del tumore [ 28 , 35 ]  . pertanto , consigliabile selezionare come input arterioso unarteria di calibro adeguato ( > 45 mm ) e ben visualizzata nelle scansioni perfusionali , ma non necessariamente tributaria del tumore stesso . 
la selezione dellinput arterioso , infine , deve evitare artefatti da movimento e da volume parziale , che potrebbero pesantemente inficiare laffidabilit dellanalisi di perfusione con tc . identificazione della fine del first pass necessaria per un calcolo affidabile dei parametri di perfusione . 
alcuni software definiscono in modo automatico la fine del first pass ; per i protocolli con scansioni perfusionali di durata superiore a quella del first pass , tuttavia , tale identificazione automatica pu risultare inesatta ed necessario impostare manualmente la fine del first pass , che dovrebbe essere fatta corrispondere , per standardizzare lanalisi , al punto pi basso dopo il picco della curva densit / tempo ottenuta dallinput arterioso . 
alcuni autori , infine , hanno applicato per gli studi con tcp dellencefalo e formule matematiche per standardizzare lidentificazione della fine del first pass [ 36 ]  . posizionamento delle roi questo passaggio consiste nel disegnare manualmente una roi lungo i margini del tumore in modo che il software quantifichi i valori di perfusione allinterno di essa . 
b correct selection of the end of the first pass on the lowest point after density / time curve peak obtained from the arterial input roi ( bf value is indicated by a yellow ellipse )  . 
b selezione corretta della fine del first pass , nel punto pi basso dopo il picco della curva densit / tempo derivata dalla roi posizionata sullinput arterioso ( il valore di bf evidenziato da unellisse gialla )  . 
in placing the roi , special attention should be consiste nellanalisi delle mappe colore , che sono generate automaticamente dal software per ogni parametro di 852 radiol med ( 2010 ) 115 : 843857 paid to ensuring that it does not include large vessels , air or surrounding adipose tissue . 
therefore , all images of the study need to be carefully analysed , preferably in cine - loop modality , to ensure that the roi does not extend beyond tumour margins in any of them . clinical interpretation qualitative analysis this involves analysis of the colour maps , which are automatically generated by the software for each perfusion parameter . 
qualitative analysis of the colour maps provides panoramic visualisation of perfusion distribution within the entire volume studied , as well as an immediate representation of the different perfusion within the tumour , with the simple identification of possible angiogenic spots ( in theory , the most perfused areas ) or areas of possible necrosis or hypoxia ( in theory , the least perfused areas )  . 
this superimposition can be helpful when identifying tumour margins is difficult , such as in the presence of complex anatomy or after chemotherapy or radiation therapy . quantitative analysis this involves interpretation of numerical values of perfusion , which the software calculates for the volume bounded by the roi placed over the tumour . 
this quantification method has on the one hand the advantages of providing an estimate of overall perfusion of the tumour volume selected and of guaranteeing a high level of interobserver repeatability [ 37 , 38 ] , whereas on the other hand , it has the disadvantage of masking the differences in perfusion within the tumour ( i.e. the heterogeneity of its perfusion ) , in that they are lost in the calculation of the mean between the values of the individual voxels . 
the heterogeneity of tumour perfusion can be evaluated in a subjective manner , when the operator visually assesses the heterogeneity of the colours generated on the colour maps ; or in an objective manner , with the graphical representation of the distribution in classes of perfusion values of each voxel ( histograms )  . 
infine , la maggior parte dei software disponibili in commercio consente di sovrapporre la mappa colore allimmagine tc nativa ; tale sovrapposizione pu essere daiuto quando lidentificazione dei margini del tumore difficile , come , ad esempio , in presenza di unanatomia complessa o dopo terapia ( chemioo radioterapia )  . analisi quantitativa consiste nellinterpretazione dei valori numerici di perfusione che il software calcola per il volume delimitato dalla roi che loperatore posiziona sul tumore . 
questo metodo di quantificazione ha , da una parte , i vantaggi di fornire una stima della perfusione complessiva del volume tumorale selezionato e di garantire una ripetibilit elevata tra osservatori diversi [ 37 , 38 ] , ma , dallaltra , ha il difetto di mascherare le differenze di perfusione allinterno del tumore ( cio , leterogeneit della sua perfusione ) , in quanto queste vengono perse nel calcolo della media tra i valori dei singoli voxel . la valutazione delleterogeneit della perfusione tumorale pu essere eseguita in maniera soggettiva , quando loperatore valuta visivamente leterogeneit dei colori generati sulle mappe colore , o in maniera oggettiva , tramite la rappresentazione grafica della distribuzione in classi dei valori di perfusione di ciascun voxel ( grafici a istogrammi ) : un tumore con elevata eterogeneit di perfusione presenta in teoria un numero di colori e classi pi ampio rispetto ad un tumore con perfusione omogenea . 
in letteratura , tuttavia , non vi sono studi che abbiano utilizzato il metodo dei grafici a istogrammi per valutare leterogeneit della perfusione tumorale misurata con la tcp . conclusioni la tecnica di esecuzione dellesame perfusionale rappresenta un fattore critico che pu influenzare in modo radiol med ( 2010 ) 115 : 843857 fig . 
software automatically generates colour maps for each perfusion parameter , in which every pixel is assigned a colour representing a numerical value for the perfusion parameter calculated for that voxel . 
le mappe colore sono generate automaticamente dal software per ogni parametro di perfusione , nelle quali ad ogni pixel assegnato un colore , che rappresenta il valore numerico del parametro perfusionale calcolato per quel pixel . 
in queste mappe colore i valori elevati sono rappresentati dai colori tendenti al giallo ed al rosso e i valori bassi sono rappresentati dai colori tendenti al verde e al blu . 
c mappa colore del mtt , che documenta un tempo di transito medio relativamente elevato nellepatocarcinoma , tale reperto riferibile alla presenza di aree ipoperfuse intratumorali , che sono possibile espressione di necrosi . 
tale reperto riferibile ad unaumentata permeabilit dellendotelio dei vasi neoformati rispetto a quello dei microvasi normali . 854 radiol med ( 2010 ) 115 : 843857 colours and classes than a tumour with homogeneous perfusion . 
however , no studies have been published that use histograms to evaluate the heterogeneity of tumour perfusion measured with ctp . conclusions the technique used to perform the perfusion study is a critical factor that can significantly influence numerical values of parameters used as perfusion indices . 
to obtain accurate and repeatable results , specific training is required for all operators who perform ctp , to eliminate possible casual or systematic errors in acquisition technique and image and data analysis . appendix 1 the siemens ( erlangen , germany ) software for body tumours uses the one - compartment ( or slope ) method to analyse images during the first pass , and the two - compartment ( or patlak ) method to analyse images acquired during the interstitial phase . 
an appropriate scan protocol for the siemens software , therefore , should include scans with a 3to 5 - s temporal resolution for the first pass ( up to 4560 s after the beginning of contrast material administration ) and scans with a 10to 20 - s temporal resolution for the interstitial phase ( with a duration between 2 and 10 min after the beginning of contrast material administration )  . 
the following perfusion parameters are calculated : perfusion ( also called blood flow ) , expressed in ml / 100 ml / m this is quantified with the one - compartment analysis as the ratio between the maximum slope of the time / density curve of the tissue and the peak density reached by the artery selected as arterial input . patlak blood volume ( bv ) , expressed in ml / 100 ml . 
the amount of stagnant blood is not included in this measure of bv . permeability , corresponding to the extraction fraction ( ef ) or the transit constant ( ktrans ) and expressed in ml / 100 ml / m this is calculated with the twocompartment analysis and measures the fraction of contrast material present at the end of the arterial capillaries with the potential to diffuse into the significativo i valori numerici dei parametri utilizzati come indici di perfusione . 
esistono risultati preliminari incoraggianti sulla riproducibilit della metodica e sulla determinazione della variabilit intrae inter - osservatore nellanalisi dei dati [ 31 , 33 ] : tuttavia questi riguardano solo alcuni distretti corporei e alcune tecniche di tcp . 
per ottenere risultati accurati e riproducibili necessario un training specifico per tutti gli operatori che eseguono la tcp , per eliminare eventuali errori casuali e sistematici nella tecnica di acquisizione e nellanalisi di immagini e dati . appendice 1 il software siemens ( erlangen , germania ) per i tumori del corpo utilizza il modello cinetico di tipo mono - compartimentale ( o dello slope method ) per lanalisi delle immagini acquisite durante il first pass e il modello cinetico di tipo bicompartimentale ( o di patlak ) per lanalisi delle immagini acquisite nella fase interstiziale . 
un protocollo di scansione adeguato per il software siemens , pertanto , dovrebbe prevedere scansioni con risoluzione temporale di 35 secondi per il first pass ( fino a 4560 secondi dopo linizio della somministrazione del mdc ) e scansioni con risoluzione temporale di 1020 secondi per la fase interstiziale ( con una durata compresa tra i 2 e i 10 minuti dopo linizio della somministrazione di mdc )  . 
sono calcolati i seguenti parametri di perfusione : perfusione ( chiamata anche blood flow ) , espressa in ml / 100 ml / minuto ; quantificata con il modello cinetico di tipo mono - compartimentale . 
essa calcolata come il rapporto la massima pendenza della curva densit / tempo del tessuto e il picco di densit raggiunto dallarteria selezionata come input arterioso . tra volume sanguigno ( chiamato patlak blood volume ) , espresso in ml / 100 ml ; calcolato con il modello cinetico di tipo bi - compartimentale . 
la quantit si sangue stagnante non inclusa nella misura del volume sanguigno . permeabilit ( chiamata permeability ) , corrispondente alla frazione di estrazione ( fe ) o costante di transito ( ktrans )  . 
essa misura la frazione di mdc presente nelle estremit capillari arteriose con il potenziale di diffondere nello spazio extravascolare - extracellulare [ 39 ] , che viene effettivamente trasferita dal sangue allo spazio interstiziale durante un singolo passaggio di sangue dallestremit arteriosa a quella venosa dei capillari di un tumore . 
esso non consente di separare il flusso allinterno dei vasi radiol med ( 2010 ) 115 : 843857 extravascularextracellular space [ 39 ] , which is effectively transferred by the blood to the interstitial space during a single pass of blood from the arterial end to the venous end of the capillary of a tumour . 
an appropriate scan protocol for the philips software , therefore , involves scans with a 3to 5 - s temporal resolution for the first pass ( up to 4560 s after the beginning of contrast material administration )  . 
the following perfusion parameters are calculated : perfusion , expressed in ml / 100 g of tissue / m this is calculated as the ratio between the maximum slope of the time / density curve of the tissue and the peak density reached by the artery selected as arterial input . blood volume ( bv ) , expressed in ml / 100 g of tissue . this measures blood that flows in the tissue being studied . 
this indicates the time interval between the arrival of contrast material in the arterial input and the peak density in the tissue being studied . appendix 3 general electric ( milwaukee , wi , usa ) software for body tumours uses deconvolution for to analyse images acquired during the first pass , and the st . 
an appropriate scan protocol for general electric software , therefore , should involve scans with a 1 - s temporal resolution for the first pass ( up to 4560 s after the beginning of contrast material administration ) and scans with a 10 - s temporal resolution for the interstitial phase ( with a duration no greater than 2 min after the beginning of contrast material administration )  . 
the following perfusion parameters are calculated : blood flow ( bf ) , expressed in ml / 100 g of tissue / min . this is calculated with deconvolution and represents bf that passes through the vascular bed of the tumour . 
it also includes flow at the level of il software philips ( best , olanda ) per i tumori del corpo utilizza il modello cinetico di tipo mono - compartimentale ( o dello slope method ) per lanalisi delle immagini acquisite durante il first pass . 
un protocollo di scansione adeguato per il software philips , pertanto , dovrebbe prevedere scansioni con risoluzione temporale di 35 secondi per il first pass ( fino a 4560 secondi dopo linizio della somministrazione del mdc )  . 
essa calcolata come il rapporto tra la massima pendenza della curva densit / tempo del tessuto e il picco di densit raggiunto dallarteria selezionata come input arterioso . volume sanguigno ( bv )  . 
indica il tempo che intercorre tra larrivo del mezzo di contrasto nellinput arterioso e il picco di densit nel tessuto in analisi . appendice 3 il software general electric ( milwaukee , wi , usa ) per i tumori del corpo utilizza il modello cinetico della deconvoluzione per lanalisi delle immagini acquisite durante il first pass e lapprossimazione adiabatica di st . 
un protocollo di scansione adeguato per il software general electric , pertanto , dovrebbe prevedere scansioni con risoluzione temporale di 1 secondo per il first pass ( fino a 4560 secondi dopo linizio della somministrazione del mdc ) e scansioni con risoluzione temporale di 10 secondi per la fase interstiziale ( con una durata non superiore ai 2 minuti dopo linizio della somministrazione di mdc )  . 
sono calcolati i seguenti parametri di perfusione : flusso sanguigno ( bf ) , espresso in ml / 100 g di tessuto / minuto ; calcolato con il modello cinetico della deconvoluzione . 
inoltre , viene incluso anche il flusso a livello degli shunt artero - venosi , che sono assai pi presenti nei tessuti neoplastici rispetto a quelli sani . 856 radiol med ( 2010 ) 115 : 843857 arteriovenous shunts , which are more common in neoplastic tissue than in healthy tissue ; blood volume ( bv ) , expressed in ml / 100 g of tissue . this is calculated with deconvolution and measures blood that flows in the tissue being studied . 
if bf is high , then mtt will be low . permeability surface ( ps ) , expressed in ml / 100 g of tissue / mthis is calculated using the st . 
lawrence and lee adiabatic approximation and measures the product between the permeability and the total surface of the capillary endothelium in a unit mass of the tumour ( normally 100 g )  . 
the ps can therefore be interpreted as the unidirectional flow of contrast material from the vascular compartment to the extravascular - extracellular compartment ( the interstitium )  . volume sanguigno ( bv ) , espresso in ml / 100 g di tessuto ; calcolato con il modello cinetico della deconvoluzione . 
la quantit di sangue stagnante non inclusa nella misura del volume sanguigno . tempo di transito medio ( mtt ) , espresso in secondi ; calcolato con il modello cinetico della deconvoluzione . 
se il flusso di sangue elevato , lmtt sar basso . superficie di permeabilit ( ps ) , espressa in ml / 100 g di tessuto / minuto ; calcolata utilizzando lapprossimazione adiabatica di st . 
knauth springer - verlag , berlin , heidelberg , 2010 isbn 978 - 3 - 540 - 85531 - 6 published online : 20 september 2010 springer - verlag 2010 among the many broad uses for magnetic resonance imaging ( mri ) in diagnostic imaging , the gastrointestinal tract is one of the most difficult on the basis of technical and fascinating diagnostic grounds . 
 i progressi intercorsi sia nelle macchine che nella elaborazione dei dati hanno permesso di superare in parte alcuni di questi problemi cosicch , allo stato attuale , la rm dellapparato digerente si affermata come uno strumento importante nella diagnosi di malattie dellintestino tenue ( tipo il morbo di crohn ) , dei tumori del colon ( per esempio , del retto ) e delle malattie dellano . 
 i progressi tecnici hanno anche permesso una valutazione corretta delle anse intestinali mediante la rm dinamica e la rm della motilit intestinale , associate a tecniche di diffusione e perfusione rm che contribuiscono nel loro insieme ad importanti informazioni diagnostiche . 
 tenuto poi conto dellassenza di radiazioni ionizzanti , la rm dimostra la sua forza ed importanza sia nello studio di malattie croniche e / o infiammatorie che necessitano di controlli seriati nel tempo , soprattutto nei bambini e nei giovani adulti ( morbo di crohn , per esempio ) che nella valutazione nel tempo di pazienti portatori di neoplasie . da questo punto di vista il radiologo riveste oggi cosa ben messa in evidenza in pi di un capitolo un ruolo molto , sempre pi , importante , nel gruppo multi - specialistico dei curanti : non solo perch pone e conferma la diagnosi , ma anche perch pu suggerire , in funzione dei risultati delle sue indagini , ulteriori possibilit terapeutiche ( in particolare in caso di recidive ) a chirurghi , oncologi , radioterapisti e gastroenterologi . il volume diviso in due parti ben precise : la prima , di 4 capitoli in 63 pagine , dedicata e discute i problemi tecnici inerenti alla rm ; la seconda , di 15 capitoli in 283 pagine , presenta le applicazioni cliniche della rm partendo dallesofago per giungere via via allano . 
 1000 radiol med ( 2010 ) 115 : 9991000 each chapter is exhaustive , enriched by very impressive and well reproduced images ; the reference list is up - to - date including references from 2009 . dealing with mri the reader should be conscious of the technical use of each sequence , what results one can expect from each of these , how important it is to properly correlate and use these . 
in this respect , each chapter in the clinical application section of the book , encompasses tables reporting in full detail the sequences parameters to be used to obtain the best imaging and diagnostic results . 
in any case , if one is not familiar with these parameters he / she become easily lost , battling with the large use of acronyms . this book will be very much appreciated by the radiologists and surely become a primary reference source not only for them but for all those dealing with bowel diseases : gastroenterologists , surgeons , oncologists . i envision a brilliant future for this text and congratulate the editor and his robust team of internationally well - known co - authors for the fine work and the results obtained . ciascun capitolo esauriente e completo , arricchito da immagini di grande effetto , molto ben riprodotte ; le voci bibliografiche sono precise ed aggiornate fino al 2009 . trattandosi di rm il lettore deve essere a conoscenza dellimpiego tecnico di ciascuna sequenza , dei risultati che pu ottenerne e quanto sia importante correlarle ed impiegarle correttamente . 
torricelli1 1department of radiology , 2department of oncology , 3department of nuclear medicine , 4department of pathology , university of modena and reggio emilia , via del pozzo 71 , 41100 modena , italy correspondence to : f . 
among 200 patients scheduled for ct follow - up , 60 ( 48 low risk ; 12 high risk ) were selected due to ct findings suspicious for or suggestive of local recurrence . 
nel gruppo di 200 pazienti sottoposti a follow - up con tc dopo trattamento chirurgico di carcinoma rettale sono stati selezionati 60 pazienti ( 48 basso rischio ; 12 alto rischio ) con quadro tc di sospetta o di probabile recidiva locale che sono quindi sono stati sottoposti , entro 2 settimane , a rm con mezzo di contrasto paramagnetico e a pet - tc . 
la presenza di recidiva stata evidenziata dalla biopsia in 15 casi ( 7 basso rischio , 8 alto rischio ) ed esclusa in 21 casi dal follow - up e in 24 dallistologia . 
sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) ed accuratezza diagnostica sono risultati rispettivamente : 86 , 7% , 68 , 9% , 48 , 1% , 93 , 9% e 73 , 3% per la rm ; 93 , 3% , 68 , 9% , 50% , 96 , 9% e 75% per la pet - ct . 
la rm e la pet - tc possono contribuire alla detection di recidiva , anche se il loro ruolo nella diagnosi precoce rimane dibattuto dato che lutilit di tali metodiche nei correnti protocolli di sorveglianza tuttora da definire . 
early diagnosis of local recurrence is important because chemotherapy , separately or integrated into a multidisciplinary approach , may improve survival and quality of life . only 20%30% of recurrences are suitable for curative reoperation , and 60% of these are detected thanks to imaging techniques [ 13 ]  . radiotherapy surgery , further unfortunately , no standard follow - up schedule is available for patients with rectal cancer treated with curative resection . 
until 2002 , no significant benefits on long - term survival had been proved for patients undergoing intensive follow - up and , although effective for early diagnosis of recurrence and curative reoperation , most proposed schedules did not offer a worthwhile costbenefit ratio [ 3 ]  . 
on the other hand , three recent meta - analyses comparing the results of low - intensity and high - intensity surveillance programmes for all patients after curative - intent surgery demonstrated the survival benefit of intensive follow - up with a reduction of absolute mortality of 10% [ 47 ]  . 
 [ 3 ] demonstrated that a risk - adapted follow - up tailored to the different risk categories of patients resulted in improved targeting of curative reoperation and overall survival . computed tomography ( ct ) is the diagnostic imaging modality routinely used in follow - up of crc , and our institutional guidelines recommend abdominal and pelvic ct every 6 months for 2 years after surgery [ 1 , 2 ]  . 
however , despite its high accuracy in detecting distant metastases , ct has a medium - to - low accuracy in detecting local recurrence of crc ( 68%76% ) [ 1 ] ; ct findings are often unclear , and many patients require further investigation with other imaging techniques or biopsy . 
however , few published reports have established the role of magnetic resonance imaging ( mri ) or positron emission tomography ct ( petct ) in the follow - up schedule of crc , even though the recent literature emphasises their accuracy and , at the same time , their underutilisation by current surveillance policies [ 1 , 2 , 811 ]  . the primary aim of our study was to analyse the value of contrast - enhanced mri ( ce - mri ) and pet - ct in the assessment of local crc recurrence after curative - intent surgery in patients with suspicious findings at follow - up ct . 
secondarily , we assessed the results of these techniques in different risk subgroups of patients . introduzione il cancro del colon - retto ( ccr ) la seconda neoplasia per incidenza nei paesi industrializzati e la seconda causa di morte correlata al cancro . 
circa l80% dei pazienti con ccr localizzato si sottopongono ad intervento chirurgico a scopo curativo , ma la percentuale di pazienti che sviluppano una recidiva locale relativamente alta ( 3%47% )  . 
la diagnosi precoce di recidiva locale importante perch il conseguente intervento chirurgico , radio - chemioterapico , singolarmente o integrato in approccio multidisciplinare , pu migliorare la sopravvivenza e la qualit della vita . 
solo il 20%30% dei pazienti con recidiva locale presenta caratteristiche che consentono di effettuare un secondo intervento curativo ed il 60% di questi casi diagnosticato grazie alle metodiche di imaging [ 13 ]  . in letteratura non esistono per linee guida univoche per il follow - up di pazienti con cancro colon - rettale sottoposti ad intervento chirurgico curativo . 
fino al 2002 non sono stati dimostrati significativi benefici sulla sopravvivenza a lungo termine in pazienti sottoposti a follow - up intensivo e la maggior parte degli studi proposti , nonostante lefficacia nella diagnosi precoce di recidiva ed una seconda possibilit di intervento chirurgico curativo , non offrivano un rapporto costo - beneficio accettabile [ 3 ]  . 
tre recenti metanalisi , confrontando i risultati di programmi di sorveglianza a bassa intensit e ad alta intensit per pazienti con ccr sottoposti ad intervento curativo , hanno tuttavia dimostrato un miglioramento della sopravvivenza nel follow - up intensivo con una riduzione del 10% della mortalit assoluta [ 47 ]  . 
 [ 3 ] hanno dimostrato che un follow - up adattato al rischio di recidiva , basato cio su diverse categorie di rischio dei pazienti , permette un significativo aumento della sopravvivenza totale e lindividuazione di un maggior numero di casi trattabili con un secondo intervento curativo . 
 la tomografia computeruizzata ( tc ) la metodica di imaging comunemente usata nel follow - up del ccr e le linee guida del nostro istituto raccomandano una tc addominale e pelvica ogni 6 mesi per 2 anni dopo lintervento chirurgico [ 1 , 2 ]  . 
tuttavia , nonostante lelevata accuratezza nel rilevare metastasi a distanza , la tc presenta unaccuratezza medio - bassa nellidentificare recidive locali di ccr ( 68%76% ) [ 1 ] ; i reperti tc sono spesso poco chiari e molti pazienti devono essere ulteriormente studiati con altre metodiche di imaging o con lesame istologico . pochi studi in letteratura hanno valutato il ruolo della risonanza magnetica ( rm ) o della tomografia ad emissione di positroni - tc ( pet - tc ) nel protocollo di follow - up del ccr , nonostante recenti lavori sottolineino laccuratezza di tali metodiche e , allo stesso tempo , il loro scarso impiego nelle attuali politiche di sorveglianza [ 1 , 2 , 811 ]  . lo scopo principale di questo studio valutare il ruolo 908 materials and methods patient population from january 2000 to october 2008 , 200 patients underwent follow - up for rectal cancer . 
our institutional guidelines for follow - up after curative resection of rectal cancer generally recommend clinical assessment every 36 months , including serum tumour markers carcinoembryonic antigen ( cea ) and cancer antigen ca 19.9 ; colonoscopy at 6 months , 2 years and 5 years after surgery and every 35 years thereafter ; and endorectal ultrasound scan every 6 months for 23 years and yearly thereafter . 
in 60 / 200 patients , ct follow - up was unable to rule out local crc recurrence due to extraluminal or intramural findings both suspicious for and suggestive of relapse . 
the curative resection surgery performed in this selected population was as follows : anterior resection in 51 ( 85% ) and abdominoperineal amputation according to miles in nine ( 15% )  . 
all 60 patients underwent neoadjuvant therapy based on chemotherapy and radiotherapy with different protocols , depending on initial disease stage ( 35 with 5 - fluorouracil [ 5 - fu ] , 14 with capecitabine , 9 with oxaliplatin and 5 - fu and 2 with cetuximab )  . 
adjuvant chemotherapy was used in 54 / 60 patients ( 33 with 5 - fu , 10 capecitabine , 2 cetuximab and 9 oxaliplatin and 5 - fu )  . 
ct findings suspicious for local relapse were classified as extraluminal in 38 cases ( 36 involving the pericolic fat around the tumour bed , two pericolic lymph nodes ) and intramural in 22 ( involving the region of the bowel anastomosis ) [ 1 ]  . all 60 patients ( 60% men , mean age 65.610.3 years ) underwent ce - mri and pet - ct in a randomised order within 2 weeks . 
readers of the second examination were blinded to the results of the first examination but not to the radiol med ( 2010 ) 115 : 906919 della rm e della pet - tc nella diagnosi di recidiva locale di ccr in pazienti che hanno subito intervento chirurgico curativo e con sospetto di recidiva alla tc . 
secondariamente , definire i risultati ottenuti da queste tecniche nei pazienti divisi in sottogruppi di rischio . materiali e metodi popolazione da gennaio 2000 a ottobre 2008 , 200 pazienti sono stati sottoposti al follow - up per cancro del colon - retto . 
i parametri tecnici per la tc a 16.slice sono i seguenti : spessore 3 , 75 mm , intervallo 3 , 75 mm ; per la tc a 64 - slice : spessore 2 , 5 mm , intervallo 2 , 5 min 60 / 200 pazienti la tc del follow - up non stata in grado di escludere la recidiva di ccr a causa di reperti extra o intra - luminali sia sospetti che indicativi di recidiva . 
in questa popolazione selezionata , gli interventi chirurgici curativi sono stati : resezione anteriore in 51 pazienti ( 85% ) e amputazione addomino - perineale secondo miles in 9 casi ( 15% )  . 
tutti i 60 pazienti hanno effettuato terapia neoadiuvante basata su chemio - radioterapia con diversi protocolli a seconda dallo stadio iniziale della neoplasia ( 35 con 5 - fluorouracile , 14 con capecitabina , 9 con oxaliplatino e 5 - fluorouracile e 2 con cetuximab )  . 
la chemioterapia adiuvante stata utilizzata in 54 / 60 pazienti ( 33 con 5 - fluorouracile , 10 capecitabina , 2 cetuximab , e 9 con oxaliplatino e 5 - fluorouracile )  . 
all patients gave written informed consent and the local ethics committee approved the study protocol . following the idea of risk - adapted follow - up proposed by secco et al . 
 [ 3 ] , patients were considered at high risk ( hr ) of local recurrence if they presented at least 3 of the following risk factors : adenocarcinoma of the low rectum ( < 10 cm from the external anal orifice ) treated by low anterior resection , a preoperative cea value 7.5 ng / ml , dukes stage c , poorly differentiated carcinoma ( g3 ) and mucinous adenocarcinoma or signet - ring cells . 
 study protocol all patients underwent dedicated pelvic ce - mri examination with a 1.5 - tesla unit ( philips medical systems , best , the netherlands ) using a phased - array , five - channel coil ( cardiac synergy coil , philips )  . 
sequences were acquired before and after administration of paramagnetic contrast medium [ gadolinium - tetra - azacyclo - dodecane - tetra - acetic acid ( gd - dota ) , 0.2 ml / kg at 3 ml / s , dotarem , laboratoire guerbet , aulnay - sous - bois , france ]  . 
all patients were administered 20 mg butyl - scopolamine ( buscopan , schering , ingelheim am rhein , germany ) intravenously before the examination to prevent peristalsis artefacts , except when contraindicated . 
 diagnosis of recurrence was based on morphology , different signal intensity and enhancement at the dynamic contrast study : nodular lesions or asymmetric masses with irregular borders , high signal intensity ( higher than muscle tissue ) on t2 - weighted sequences and an increase of at least 50% in signal intensity over baseline values on postcontrast sequences were considered malignant [ 2 ]  . 
 pet - ct images were acquired with an integrated petct device ( ge , discovery lsa ) composed of an advance nxi pet scanner and a 16 - slice light speed plus ct scanner . 
before administration of [ 18f ] fluorodeoxyglucose ( fdg ) , all patients fasted from midnight , underwent blood glucose tests ( glycaemia < 150 mg / ml ) and , to avoid artefacts caused by muscle activity , were instructed not to do any physical activity or to talk prior to the examination . the acquisition of images started approximately 50 min after intravenous injection of 37 mbq / 10 kg body weight fdg . 
ct acquisition parameters were : 340 ma , 120 kv , slice thickness 3.75 mm , tube rotation time 0.8 ms , fov collimation 50 c ct stati classificati come extra - luminali in 38 casi ( 36 casi coinvolgevano il tessuto adiposo pericolico attorno al letto tumorale ed in 2 casi i linfonodi pericolici ) o intra - murali in 22 casi ( coinvolgenti la regione intestinale dellanastomosi ) [ 1 ]  . 
tutti e 60 i pazienti ( 60% maschi , et media 65 , 610 , 3 anni ) sono stati sottoposti entro 2 settimane a rm con mezzo di contrasto e pet - tc , in ordine randomizzato . 
il medico con il compito di effettuare il referto per la seconda metodica di imaging non era a conoscenza dei risultati del primo esame , considerando i criteri di inclusione . 
 [ 3 ] , i pazienti sono stati considerati ad alto rischio ( ar ) di sviluppare recidiva locale se presentavano almeno 3 dei seguenti fattori di rischio : adenocarcinoma del basso retto ( considerato al di sotto di 10 cm dallorifizio anale esterno ) trattato con resezione anteriore bassa , valore preoperatorio di cea7 , 5 ng / ml , stadio c di dukes , carcinoma scarsamente differenziato ( g3 ) e adenocarcinoma mucinoso o con cellule ad anello con castone . 
 protocollo di studio tutti i pazienti sono stati sottoposti a rm pelvica dedicata con un magnete da 1 , 5 tesla ( philips medical systems , best , olanda ) equipaggiato con bobina phased - array a cinque canali ( cardiac synergy coil , philips medical systems )  . 
le sequenze sono state acquisite prima e dopo la somministrazione di mezzo di contrasto paramagnetico ( gadoliniumtetra - azacyclo - dodecane - tetra - acetic acid [ gd - dota ] , 0 , 2 ml / kg a 3 ml / s , dotarem , laboratoire guerbet , aulnaysous - bois , francia )  . 
a tutti i pazienti sono stati somministrati endovena 20 mg di butil - scopolamina ( buscopan , schering , ingelheim am rhein , germania ) prima dellesame per prevenire artefatti da peristalsi , se non controindicato . 
il protocollo di rm riportato in tabella 1 . la diagnosi di recidiva stata basata sulla morfologia , sulla diversa intensit di segnale ed enhancement allo studio dinamico di contrasto : lesioni nodulari o masse asimmetriche con bordi irregolari , alta intensit di segnale ( maggiore di quella del tessuto muscolare ) nelle sequenze t2 - pesate ed un aumento di almeno il 50% dellintensit di segnale oltre il valore base alla fine della prima fase dinamica sono stati considerati maligni [ 2 ]  . le immagini pet - tc sono state acquisite con metodica pet - tc combinata ( ge , discovery lsa ) che integra uno scanner pet ( advance nxi ) ad un sistema tc a 16 - slice ( light speed plus )  . 
la sequenza 3d inversion recovery ( ir ) - gradient echo ( ge ) stata acquisita nelle quattro differenti fasi dinamiche relative alliniezione endovenosa del contrasto : basale , arteriosa ( 30 secondi ) , venosa ( 60 secondi ) , e tardiva ( 120 secondi ) sequenza piano te ( ms ) spessore ( mm ) intervallo ( mm ) matrice tse , turbo spin echo ; spair , spectral presaturation attenuated inversion - recovery ; nex , number of excitation ; ir , inversion recovery ; te , tempo di eco images were reconstructed with a filtered back - projection syste ct data were used for attenuation correction of the pet scan that was performed immediately after the ct acquisition , without changing the patients position . 
the pet scan was acquired in the caudocranial direction with 3d interactive reconstruction . the maximum standardised uptake value ( suv ) was considered significant if > 2.5 on the standard of the scanner . 
fdg uptake at , or close to , the site of surgical anastomosis within the pelvis , presacral region , abdominal walls and pelvic lymph nodes were considered probably or certainly malignant . bladder , ureteral and intestinal uptake was considered physiological , as was uptake in stomas or recent surgical incisions . the gold standard was histological biopsy in 39 cases ( in 24 cases guided by ct and in 15 by endorectal ultrasound ) and follow - up at 6 and 12 months in the remaining 21 ( considering local relapse as lesion progression and fibrosis lesion stability at 6 and 12 months follow - up without therapy )  . 
diagnostic sensitivity , specificity , accuracy , positive predictive value ( ppv ) and negative predictive value ( npv ) in diagnosing local recurrence were evaluated for ce - mri and pet - ct both globally and separately in the different risk subgroups . 
lacquisizione dellimmagine stata ottenuta circa 50 minuti dopo liniezione endovenosa di 37 mbq / 10 kg di fdg ; la scansione stata effettuata dal meato acustico esterno fino alla radice della coscia , in pazienti supini con mani sopra la testa . 
i parametri di acquisizione tc sono stati : 340 ma ( auto ) , 120 kv , spessore di strato 3 , 75 mm , tempo di rotazione del tubo 0 , 8 ms , collimazione campo di vista ( fov ) di 50 c le immagini tc sono state ricostruite con un sistema di back - projection filtrata . 
 i siti di uptake sono stati valutati come maligni o benigni in base alla forma , localizzazione ed intensit di captazione . siti di uptake a livello o in adiacenza allanastomosi chirurgica , o regione presacrale , nella parete addominale od a livello dei linfonodi pelvici sono stati considerati come probabilmente o certamente maligni . 
 table 2 therapy in the selected patients characteristics statistics patients male surgery neoadjuvant therapy ct + rt adjuvant chemotherapy 60 ( 100% ) 36 ( 60% ) 65.610.3 years 51 ( 85% ) 9 ( 15% ) 1 ( 1.7% ) 2 ( 3.3% ) 57 ( 95% ) 54 ( 90% ) ar , anterior resection ; apa , abdominoperineal amputation according to miles ; ct , chemotherapy ; rt , radiotherapy tabella 2 caratteristiche e terapia dei pazienti selezionati caratteristiche statistiche pazienti maschi et intervento chirurgico terapia neoadiuvante ct + rt chemioterapia adiuvante 60 ( 100% ) 36 ( 60% ) 65 , 610 , 3 anni 51 ( 85% ) 9 ( 15% ) 1 ( 1 , 7% ) 2 ( 3 , 3% ) 57 ( 95% ) 54 ( 90% ) ra , resezione anteriore ; aap , amputazione addomino - perineale secondo miles ; ct , chemioterapia ; rt , radioterapia livello vescicale , ureterale e intestinale stata considerata fisiologica , cos come non sono stati inclusi siti di uptake a livello di stomie od incisioni chirurgiche recenti . 
 i dati ottenuti dalle due metodiche sono stati confrontati in 39 casi con lesame istologico ( in 24 casi prelievo tcguidato e in 15 casi con guida ecoendoscopica ) ritenuto il gold standard e nei restanti 21 casi valutandone il follow - up a 6 e 12 mesi ( considerando come recidiva locale la progressione della lesione e come fibrosi se invariata a 6 e 12 mesi di follow - up senza effettuare alcuna terapia )  . 
la sensibilit , specificit , accuratezza , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) nella diagnosi di recidiva locale di cancro colon - rettale sono stati calcolati per la rm e per la pet - tc , sia globalmente che singolarmente per le diverse classi di rischio . 
lintervallo medio tra lintervento chirurgico iniziale e la recidiva locale stato di 33 , 324 , 2 mesi ( intervallo 575 mesi )  . nel 73 , 3% ( 11 / 15 pazienti ) i risultati ottenuti con la rm e la pet - tc sono stati confermati dal gold standard ( biopsia ) nellindividuare la recidiva locale . 
nel 68 , 9% ( 31 / 45 ) i risultati rm e pet - tc sono stati confermati dal gold standard ( biopsia o follow - up ) nellescludere la presenza di recidiva . 
 adattando la classificazione del rischio precedentemente descritto , 12 ( 20% ) pazienti sono stati considerati ad alto rischio ( ar ) di recidiva e 48 ( 80% ) a br . 
rm sequenza t2 - pesata ( tempo di ripetizion [ tr ] 3500 tempo di eco [ te ] 90 ) ( c ) e sequenza t1 - pesata con mezzo di contrasto ( gadolino tr 4 , 4 te 2 , 1 ) ( d ) : larga massa con intensit di segnale ed caratteristiche di enhancement indicative di recidiva . 
laccuratezza della rm e della pet - tc era per entrambe del 91 , 7% nei pazienti ad ar contro rispettivamente il 68 , 8% e 70 , 8% nei pazienti a br . 
nei pazienti ad ar i migliori risultati sono stati ottenuti per specificit e vpp ( 100% ) sia per la rm che per la pet - tc , mentre nei pazienti a br sensibilit e vpn hanno dato i risultati pi alti ( rispettivamente per la rm e pet - tc 85 , 7% , 94 , 6% e 100% )  . 
tutti questi pazienti erano vivi al termine dello studio , dopo 159 , 6 mesi dallintervento . discussione la recidiva locale in pazienti operati per ccr rappresenta radiol med ( 2010 ) 115 : 906919 fig . 
rm sequenza t2 - pesata ( tr 3500 te 90 ) ( c ) : inspessimento della parete colica con raggi spiculati nel grasso peri - colico , enhancement dopo somministrazione di gadolinio ( tr 4 , 4 te 2 , 1 ) ( d ) indicativo di recidiva ( freccia )  . 
in fact , only 10%15% of local recurrences can be completely debulked , levento che maggiormente condiziona la prognosi , infatti solo il 10%15% delle recidive locali pu esser radicalmente asportata e solo il 10% dei pazienti sopravvive pi di 2 anni , mentre gli altri hanno una sopravvivenza media inferiore ad un anno [ 2 ]  . 
tuttavia anticipando la diagnosi di recidiva locale , ancora possibile intervenire chirurgicamente in modo radicale , migliorando la qualit della vita e prolungando la sopravvivenza oltre i 2 anni [ 1214 ]  . 
gli obiettivi primari delle strategie di sorveglianza post - operatoria sono la valutazione dellefficacia della terapia sulla lesione primitiva , la diagnosi precoce di recidive locali e / o di metastasi di piccole dimensioni potenzialmente curabili e lindividuazione di neoplasie metacrone rettali . il ruolo del follow - up rimane tuttavia controverso in quanto nessuna strategia di sorveglianza postoperatoria ha finora dimostrato inequivocabilmente di migliorare la radiol med ( 2010 ) 115 : 906919 fig . 
rm sequenza t2 - pesata ( tr 3500 te 90 ) ( b ) e dopo somministrazione di gadolinio ( tr 4 , 4 te 2 , 1 ) ( c ) : non presenta segni riferibili a recidiva locale . 
thanks to early diagnosis , it is possible to detect local recurrence when this is still confined and curative surgery is still feasible , improving quality of life , and overall survival by > 2 years [ 1214 ]  . 
the fundamental surveillance targets of postoperative programmes are to assess the efficacy of the initial therapy , to detect new or metachronous malignancies and to identify potentially curable local recurrence . the role of follow - up is still controversial , as no single strategy of postoperative surveillance has been unequivocally shown to improve survival or cure rate . 
expense is also a significant factor in this follow - up evaluation , and the significant investment in time and money required for intensive follow - up almost a decade ago seemed not to be justified by the minimal increase in survival rates after curative reoperation [ 15 ]  . 
showed that based on the available data and current costs , intensive follow - up ( that did not include either cemri or pet - ct ) after curative resection for crc was economically justified and should have been normal practice [ 16 ]  . in 2002 , secco et al . 
circa un decennio fa , considerando il significativo impiego di tempo e risorse economiche necessario , il ricorso a follow - up intensivo non sembrava esser giustificato dal minimo miglioramento del tasso di sopravvivenza successivo a un secondo intervento chirurgico curativo [ 15 ]  . 
 [ 16 ] hanno invece dimostrato che , basandosi solo sui dati disponibili e sui costi correnti , un follow - up intensivo ( che non comprendeva n rm n pet - tc ) dopo la resezione chirurgica di ccr era economicamente giustificato e che avrebbe anzi dovuto esser di normale routine [ 16 ]  . 
 [ 3 ] hanno documentato il significativo miglioramento del tasso di sopravvivenza nei pazienti seguiti con follow - up intensivo se confrontati con pazienti sottoposti a follow - up di routine , grazie ad un maggior numero di re - interventi curativi . 
ct ( a ) : presacral hypodense tissue suspicious for local recurrence ( arrow )  . pet - ct ( b ) : hypermetabolic area in the centre of this tissue . 
tc ( a ) : tessuto ipodenso pre - sacrale sospetto per recidiva locale ( freccia )  . pet - tc ( b ) : area ipermetabolica al centro di questo tessuto . 
rm sequenza t2 - pesata ( tr 3500 te 90 ) ( c ) : tessuto iperintenso nella regione presacrale con area centrale di ipervascolarizzazione dopo somministrazione di gadolinio ( tr 4 , 4 te 2 , 1 ) ( d ) indicativo di recidiva ( freccia )  . 
current european society for medical oncology ( esmo ) [ 17 ] and american society of clinical oncology ( asco ) [ 18 ] guidelines do not recommend the use of ce - mri or pet - ct in the routine followup for crc . in our study , adapting the risk criteria used by secco et al . , we considered the possible role of ce - mri and petct in patients with suspected local relapse of crc , especially in hr patients , in whom local recurrence is shown to be more frequent . 
 nel nostro studio , adattando i criteri di rischio usati da secco , abbiamo considerato il ruolo che potrebbe avere lintroduzione della rm e della pet - tc in pazienti con sospetta recidiva locale di crc , specialmente nei pazienti ad ar dove , come dimostrato , la recidiva locale pi frequente . 
nel cancro rettale la maggioranza di recidive locali origina dal letto tumorale , il che sottolinea limportanza di poter visualizzare direttamente il tessuto perirettale come parte del follow - up post - operatorio . 
nel nostro studio la rm ha mostrato unaccuratezza del 73 , 3% , nei limiti dei risultati riportati in letteratura ( 68%95% ) [ 1 ] , e ha consentito uneccellente individuazione di recidive pelviche nei pazienti ad ar grazie ad un vpp del 100% . 
in our study , ce - mri showed an accuracy of 73.3% , that is , within the range reported in literature ( 68%95% ) [ 1 ] and enabled an excellent detection of pelvic recurrence in hr patients , thanks to its 100% ppv . 
the 14 false positive results detected by ce - mri were related to the presence of inflammatory tissue , which can have the same ce - mri signal intensity and contrast enhancement as neoplastic tissue . 
 pet - ct helps to overcome some of the limitations of ce - mri , thanks to the characteristics of this hybrid technique , which provides morphological and functional information . 
crc is known to be fdg avid , and the literature reports excellent results in detecting rectal recurrence , with an accuracy that ranges from 74% to 96% [ 1 ]  . 
pet cannot identify small tumours due to its limited spatial resolution of 46 mmucinous adenocarcinomas have poor fdg uptake , and radiation - induced inflammation in the first 12 months after radiotherapy 14 falsi positivi diagnosticati dalla rm erano correlati alla presenza di tessuto infiammatorio che ha la stessa intensit di segnale ed enhancement del mezzo di contrasto del tessuto neoplastico . 
i 2 falsi negativi erano legati alla presenza di unintensa reazione desmoplastica e un basso numero di cellule tumorali , che ha reso la lesione indistinguibile dal tessuto fibrotico alla valutazione con le metodiche di imaging . 
 noto che il tumore del colon - retto avido di fdg e in letteratura sono riportati eccellenti risultati di questa metodica nellindividuare recidive locali , con unaccuratezza compresa tra il 74% il 96% [ 1 ]  . 
la pet non in grado di identificare tumori di piccole dimensioni , dovute alla limitata risoluzione spaziale di 4 - 6 mm ; gli adenocarcinomi mucinosi hanno uno scarso uptake di fdg ed inoltre linfiammazione indotta dalle radiazioni nei primi 12 mesi dopo radioterapia ne riduce la specificit . 
 [ 19 ] recently analysed the use of contrastenhanced pet - ct ( ce - pet - ct ) in detecting recurrent crc , describing higher accuracy and therapeutic impact when this technique was compared with ce - ct and petct alone , suggesting that ce - pet - ct might be considered as the first - line diagnostic tool for restaging patients with rectal cancer . 
in our study , the accuracy of pet - ct was 75% , but npv was very high ( 96.9% ) , especially considering the division in risk groups : in lr patients , npv was globally 100% , proving pet - ct to be excellent for excluding the presence of local recurrence in patients that should be relapse free . despite all the reported limitations , pet - ct generally demonstrated better results compared with ce - mri . nevertheless , this technique is not widely available , especially in small centres , and ce - mri proved to be an excellent alternative . 
statistical results were globally the same for the two examinations considering the entire population enrolled , but subsequent classification into risk groups showed different statistical values as the two populations were numerically different ( 12 hr and 48 lr )  . 
however , no previous study using secco et al.s proposed risk factors can be found in literature so that the exact percentage of the different categories cannot be estimated in the overall population undergoing follow - up for rectal cancer . 
comparing results of ce - mri and pet - ct in the two risk groups , we can state that ce - mri and pet - ct both yielded a ppv of 100% in the hr group and a npv of 94% and 100% , respectively , in the lr group . 
these results emphasise the superiority of these two techniques if compared with the use of ct alone , leading to a higher number of curative reoperations . in a recent study , potter et al . 
 [ 20 ] demonstrated that a serial review of ct and mr images in cases of suspected recurrence at pet - ct had the same accuracy ( 92% ) if compared with pet - ct results alone . 
nel nostro studio laccuratezza della pet - tc stata del 75% , ma il vpn stato molto alto ( 96 , 9% ) , in particolare considerando la divisione nei gruppi di rischio : nei pazienti a br il vpn stato globalmente del 100% , dimostrando di essere eccellente nellescludere la presenza di recidiva locale nei pazienti che pi probabilmente dovrebbero esserne liberi . 
 nonostante tutte le limitazioni riportate , la pet - tc ha generalmente dimostrato di dare risultati migliori se confrontata con la rm ; tuttavia questa tecnica non ampiamente disponibile , specialmente nei piccoli centri e la rm ha dimostrato di esserne una eccellente alternativa . 
considerando tutti i pazienti arruolati , i risultati statistici si sono dimostrati sovrapponibili per le due metodiche di imaging , ma la successiva suddivisione per gruppi di rischio ha mostrato valori statistici differenti , in quanto le due popolazioni erano numericamente diverse ( 12 ar e 48 br )  . 
non sono tuttavia presenti in letteratura precedenti studi che utilizzino le categorie di rischio proposte da secco , quindi non possibile stimare lesatta percentuale delle diverse categorie di rischio nella popolazione totale di pazienti sottoposti a follow - up per ccr . 
ovviamente introdurre la stratificazione del rischio proposta identificando cos sottogruppi numericamente equivalenti , potrebbe aiutare nel definire il vero ruolo di queste due metodiche di alto livello nei protocolli di sorveglianza attuali . 
 i dati del nostro studio hanno dimostrato che la suddivisione dei pazienti in alto e basso rischio di recidiva , secondo i fattori prognostici analizzati , razionale e clinicamente affidabile [ 3 ] , considerando che nei pazienti ad alto rischio lincidenza di recidiva stata del 71 , 4% rispetto al 13 , 8% del gruppo a br . 
confrontando i risultati ottenuti dallanalisi statistica di rm e pet - tc nei due gruppi , possiamo affermare che la rm e la pet - tc presentano entrambe nel gruppo ar un vpp del 100% , e nel gruppo br un vpn rispettivamente del 94%100% . 
 [ 20 ] hanno dimostrato che una revisione seriale delle immagini ottenute con tc e rm in casi sospetti di recidiva in pazienti sottoposti a pettc , ha la stessa accuratezza ( 92% ) se confrontata con i risultati ottenuti esclusivamente dalla pet - tc . 
la revisione di immagini seriali pu individuare lesioni nuove o gi note ma di dimensioni aumentate che potrebbero esser facilmente sorvolate o considerate non importanti senza un attento 918 radiol med ( 2010 ) 115 : 906919 can punctually detect a new or enlarging lesion that could easily be overlooked or considered unimportant without a careful comparison of an entire series of studies . 
this timeconsuming method is recommended by the authors only in the event of equivocal findings or unexplained cea elevation , and therefore , pet - ct should be performed only when the serial review is still equivocal or when cea elevation remains unexplained [ 20 ]  . our study has some limitations . 
another limitation lies in the follow - up protocol adopted in our department , which does not include the use of ce - mri and pet - ct , which are , additionally , highly costly techniques . 
 in conclusion , in agreement with the recent literature , we confirm the importance of ce - mri and pet - ct in evaluating suspected local recurrence of crc in patients who have undergone curative surgery . 
based on the results of our study , we suggest that surveillance protocols be differentiated on the basis of the risk of recurrence , with intensive follow - up inclusive of ce - mri and pet - ct being limited to patients at hr only . although negative pet - ct excluded recurrence in lr patients in our study , thus obviating subsequent follow - up and / or biopsy , the number of false positive results could increase the economic and follow - up burden . 
questo metodo , che richiede molto tempo , raccomandato dagli autori solo in caso di indagini sospette per recidiva locale o di un aumento inspiegato del valore sierico del cea ; pertanto la pet - tc dovrebbe essere effettuata solo quando la revisione delle immagini seriali rimane equivoca o permane ingiustificato laumento dei livelli sierici dei markers neoplastici [ 20 ]  . 
la popolazione selezionata era piccola , con sottogruppi numericamente discordanti e bisogna considerare la presenza di diversi stadi tumorali al momento della divisione iniziale . un altro limite risiede nel protocollo di follow - up adottato nel nostro dipartimento che non prevede luso n della rm n della pet - tc ; inoltre necessario considerare limpatto economico dellutilizzo di queste metodiche . in conclusione , in linea con la recente letteratura , confermiamo limportanza della rm e della pet - tc nella valutazione di sospette recidive locali di ccr in pazienti sottoposti a intervento chirurgico curativo . 
basandoci sui risultati del nostro studio , suggeriamo di differenziare i protocolli di sorveglianza sulla base di alto e basso rischio di recidiva , limitando il follow - up intensivo , che comprende rm e pet - tc , solo per i primi pazienti . 
nel nostro studio una pet - tc negativa si dimostrata in grado di escludere la presenza di recidiva nei pazienti a basso rischio , evitando cos un successivo follow - up e / o esame istologico ; tuttavia va considerato che lalto numero di falsi positivi legato alla metodica potrebbe comportare un aumento dellimpegno economico e dellintensit del follow - up . 
the authors sought to determine the influence of two different iodine concentrations of nonionic contrast media ( cm ) on contrast enhancement in pancreatic computed tomography angiography ( cta )  . 
the contrast agent was injected with iodine concentrations of 400mgi / ml ( iomeron 400 ) in group a and 300mgi / ml ( iopamidol 300 ) in group b with the same total iodine dose ( 36 g )  . 
in the arterial and portal venous phase , the highly concentrated cm led to significantly greater enhancement in the abdominal main vessels , pancreas and pancreatic carcinoma than did the low concentrated cno statistically significant attenuation differences were measured between pancreatic carcinomas and the pancreatic parenchyma in the arterial and portal venous phase between group a and b . the overall trend for both readers was to assign higher scores to group a than group b . 
il mezzo di contrasto stato iniettato con una concentrazione iodica di 400 mgi / ml ( iomeron 400 ) nel gruppo a , e di 300 mgi / ml ( iopamidol 300 ) nel gruppo b , con la stessa dose totale di iodio ( 36 gr )  . 
nella fase arteriosa e portale il mdc ad alta concentrazione ha portato ad un enhancement significativamente maggiore dei principali vasi addominali , del pancreas e dei carcinomi del pancreas , rispetto al mdc a pi bassa concentrazione . 
una concentrazione di iodio pi elevata porta ad un maggiore enhancement dei vasi addominali e degli organi nella cta pancreas . lindividuazione e la definizione del carcinoma radiol med ( 2010 ) 115 : 898905 hypovascular pancreatic carcinoma was not found to be improved by the higher iodine concentration . pancreatico ipovascolarizzato non risultata migliore con concentrazioni iodiche pi elevate . keywords pancreas pancreatic neoplasm contrast media x - ray computed tomography parole chiave pancreas tumore del pancreas mezzi di contrasto tomografia introduction multidetector computed tomography ( mdct ) allows acquisition of multiple slices within subsecond rotation times , which makes multiphasic imaging possible . 
recently , multiphasic pancreatic contrast - material - enhanced helical ct has been suggested as an accurate technique for detecting and staging pancreatic ductal adenocarcinoma [ 1 ]  . contrast enhancement of the pancreatic parenchyma after intravenous injection is determined by many interacting factors , e.g. 
total iodine dose , iodine concentration , injection rate and scanning delay ; the use of a saline flush after contrast material administration ; and patient characteristics such as age , sex , weight , height , cardiovascular status and renal function . 
recently , there have been several attempts to optimise the use of contrast material for pancreatic imaging mainly with regard to total iodine dose , injection rate and scanning delay [ 27 ]  . 
this study focused on the influence of iodine concentration on contrast enhancement in pancreatic ct angiography ( cta ) in patients with known or suspected pancreatic tumours and patients after pancreatic surgery . materials and methods patients from march to july 2007 , 60 consecutive patients referred to our department for pancreatic cta because of known or suspected pancreatic tumours or for postoperative follow - up after pancreatic surgery were enrolled in this prospective randomised parallel - group study after having given their written informed consent . 
excluded were patients with hypersensitivity to iodinated contrast agents , hyperthyroidism , malignant thyroid tumours , renal or heart failure or insulin - dependent diabetes mellitus ; pregnant patients or nursing women , patients < 18 years of age and patients who had participated in another study within the past 30 days . the patient population consisted of 28 women and 32 men 1882 years old ( median 60 years )  . 
the study was approved by the institutional review board , and informed consent was obtained from all patients before ct examinations . ct protocol ct examination was performed after oral administration of water ( 800 ml )  . 
the nonionic contrast agents iomeron and iopamidol ( bracco altana pharma gmbh , konstanz , germany ) were applied , with an iodine concentration of 400 mgi / ml ( iomeron 400 ) and a volume of 90 ml in group a and an iodine concentration of 300 mgi / ml ( iopamidol 300 ) and a volume of 120 ml in group b . 
the nonionic contrast agents were heated to 37c and injected with a flow rate of 3 ml / s with an automatic injector through a 20 - gauge plastic cannula placed in a cubital vein in both groups . mdct ( lightspeed 16 , ge ) of the pancreas was performed in all patients prior to contrast medium administration as well as in the arterial and portal venous phases following contrast administration . 
cta image acquisition used a bolus - tracking program ( smartprep , ge healthcare ) , which monitored contrast enhancement of the aorta after injection of contrast media before initiation of the diagnostic scans . the region of interest ( roi ) cursor for bolus tracking was placed in the aorta at the level of the diaphragmatic dome . real - time low - dose ( 120 kvp , 50 ma ) serial monitoring scanning was initiated 1012 s after the start of the contrast injection , and the scanning threshold values were set at 80 hu . 
when ct values of the aorta were > 80 hu , the arterial phase acquisition was triggered , and 30 s after the end of arterial phase acquisition , the portal phase acquisition was triggered . 
for quantitative assessment of contrast enhancement , circular rois with diameters between 5 mm and 2 cm , depending on the size of the anatomical structure , were placed on the aorta , coeliac trunk , superior mesenteric artery ( sma ) , portal vein , superior mesenteric vein ( smv ) , liver , spleen , pancreas and pancreatic carcinomas . 
attenuation values ( in hounsfield units ) were measured in the above - named organs , blood vessels and pancreatic carcinomas at three different locations before contrast medium administration and in the arterial and portal venous phases , and mean attenuation values were calculated . 
visible blood vessels , bile ducts , the pancreatic duct , possible hepatic or pancreatic lesions and artefacts were carefully excluded from roi measurements in the liver , pancreas and spleen . contrast enhancement of organs , blood vessels and pancreatic carcinomas was calculated as the absolute difference between contrast - enhanced scans in the arterial and portal venous phases and unenhanced scans . 
in patients with proved pancreatic carcinoma , differences between mean attenuation values of the aorta , coeliac trunk , sma and pancreatic carcinoma during the arterial phase and differences between mean attenuation values of the portal vein , smv and pancreatic carcinoma during the portal venous phase were calculated . 
additionally , differences between mean normal pancreatic parenchymal attenuation values and attenuation values of pancreatic carcinoma that is , the tumour - to - pancreatic parenchymal contrast ( tpc ) were calculated during the arterial and portal venous phase . 
the contribution of the contrast agent to the overall diagnostic value , enhancement of each organ and depiction of blood vessels were assessed on a 5 - point visual analogue scale : excellent ( 5 ) , good ( 4 ) , sufficient ( 3 ) , insufficient ( 2 ) and poor ( 1 )  . 
criteria included tumour delineation from surrounding tissue , evaluation of infiltration of organs adjacent to the pancreas , evaluation of vessels in the arterial phase and the portal venous phase . 
tumour delineation from surrounding tissue and evaluation of infiltration of organs adjacent to the pancreas were evaluated only for patients with proved pancreatic malignancies , whereas evaluation of vessels in the arterial and portal venous phase was assessed for all patients . 
in all images , window width was 200 hu and the centre was 40 hu . statistical analysis for statistical analyses of contrast enhancement , mean enhancement values and standard deviations ( sds ) were calculated for the above - named organs , pancreatic carcinomas and vessels for each group . 
mean attenuation differences and sds between the aorta , coeliac trunk , sma and pancreatic carcinomas and between the portal vein and pancreatic carcinomas and between the pancreas and pancreatic carcinomas during the arterial and portal venous phases were calculated for each group . 
 results four patients were excluded from the evaluation due to technical failures during the scan ( two in group a for contrast agent spill over and two in group b for machine fault ) .there were no statistically significant differences in weight , height and body mass index ( bmi ) between the 56 patients evaluated in the two groups ( table 1 )  . 
of the 46 pancreatic lesions , 32 were proved pancreatic carcinomas ( 13 in group a ; 19 in group b ) and seven were pancreatic cystic lesions , including cystadenoma , solid pseudopapillary tumour , intraductal papillary mucinous neoplasm , pseudocyst and tuberculosis ( four in group a ; three in group b )  . 
two patients showed signs of pancreatitis ( one in group a ; one in group b ) , four had pancreatic endocrine tumours ( two in group a ; two in group b ) and one presented with an expected postoperative appearance after pancreatic surgery in group a . 
in the portal venous phase , significantly higher contrast enhancement was found for the portal vein , smv , splenic vein , pancreas , pancreatic carcinomas , liver and spleen in group a compared with group b . attenuation differences in the arterial phase between the aorta and the pancreatic carcinomas , the coeliac trunk and the pancreatic carcinomas , the sma and the pancreatic carcinomas and the splenic artery and the pancreatic carcinomas were significantly higher in group a compared with group b ( table 4 )  . attenuation differences in the portal venous phase between the splenic vein and the pancreatic carcinomas were higher in group a compared with group b , and no statistically significant attenuation differences were measured between the portal vein and the pancreatic carcinomas and the smv and the pancreatic carcinomas ( table 5 )  . 
no statistically significant attenuation differences were measured between pancreatic carcinomas and pancreatic parenchyma in the arterial and portal venous phase between group a and group b ( table 5 )  . differences in organ and blood vessel contrast enhancement between group a and group b are demonstrated in figs . 
concerning qualitative image assessment , the contribution of the contrast agent to the diagnostic value was assessed on a scale from 1 to 5 ( 1 = poor , 2 = insufficient , 3 = sufficient , 4 = good , 5 = excellent )  . 
detailed results of the qualitative image assessment are summarised in table 6 . discussion mdct offers high volumetric coverage , speed and spatial resolution , so it is now widely used to acquire reliable images for diagnosis , preoperative evaluation and follow - up of pancreatic lesions . 
si dimostra maggior enhancement con il primo mdc ( a , b ) rispetto al secondo mdc ( c , d ) nelle grandi e piccole arterie , vene , pancreas e fegato sia nella fase arteriosa che portale . 
2a - d a 67 - year - old woman with carcinoma of the pancreatic body and tail after injection of 400 mgi / ml contrast medium : ( a ) arterial phase scan , ( b ) portal venous phase scan . 
a 59 - year - old man with carcinoma of the pancreatic body and dilation of the pancreatic duct who received 300 mgi / ml contrast medium : ( c ) arterial phase scan , ( d ) portal venous phase scan . 
2a - d donna di 67 anni con carcinoma del corpo - coda del pancreas dopo somministrazione di mdc ad alta concentrazione ( 400 mgi / ml ) : ( a ) fase arteriosa , ( b ) fase portale . 
donna di 59 anni con carcinoma del corpo del pancreas e dilatazione del dotto pancreatico , cui stato somministrato mdc a minore concentrazione ( 300 mgi / ml ) : ( c ) fase arteriosa , ( d ) fase portale . 
patient - related factors for contrast enhancement after intravenous injection on pancreatic cta include age , sex , weight , height and heart rate . in our study , we focused on contrast agent concentration and determined the influence of two different iodine concentrations of nonionic contrast media ( 400 mgi / ml vs . 300mgi / ml ) on contrast enhancement in pancreatic cta . injection rate ( 3 ml / s ) , total amount of iodine ( 36 g ) and 904 radiol med ( 2010 ) 115 : 898905 injection technique were kept constant in both groups , and both contrast agents were heated to 37c before injection . many investigators have studied helical ct scanning protocols for pancreatic imaging . 
as our study aimed to determine the effects of iodine concentration on pancreatic cta , we used a dual - phase scanning protocol including an early arterial phase to maximise contrast in the abdominal main arteries and a portal venous phase to obtain maximum mesenteric and portal venous as well as hepatic enhancement and maximum tumour conspicuity . contrast enhancement measurements revealed significantly greater enhancement of the aorta , coeliac trunk , spleen artery , sma , pancreas , pancreatic carcinomas and spleen in the arterial phase with an iodine concentration of 400 mgi / ml compared with 300 mgi / ml . 
 [ 9 ] : after injection of a nonionic contrast agent with an iodine concentration of 300 mgi / ml in group a and 400 mgi / ml in group b ( amount of iodine 39 g , flow rate 5 ml / s ) , the higher concentration led to a significantly higher arterial phase contrast enhancement of the abdominal main arterials and organs . 
 [ 6 , 11 ] also reported similar results : after injection of a nonionic contrast agent with an iodine concentration of 370 mgi / ml in one group and 300 mgi / ml in a second group , the higher concentration led to a significantly higher arterial - phase contrast enhancement of the aorta and pancreas . 
higher contrast enhancement of arteries and organs with higher iodine concentrations during the arterial phase can be explained by the theory that with more highly concentrated contrast agents , more iodine is applied per time under the same injection rate , thus leading to a higher concentration of contrast material in arteries , organs and pancreatic malignancies . 
 the effect of various iodine concentrations on contrast enhancement during the portal venous phase was also the subject of fenchel et al.s study [ 9 ] .the higher concentration led to a significantly higher portal venous phase contrast enhancement of the abdominal main veins and organs . 
in detail , the higher concentration required less iodine volume and was totally injected in less time with the same amount of injected iodine ( 36 g ) and at the same injection rate ( 3 ml / s )  . 
therefore , the dose of contrast agents circulating to the veins and organs was higher in the same amount of time , thus leading to a higher concentration of contrast material in veins , organs and pancreatic malignancies . concerning the 32 pancreatic carcinomas in our study , there were no statistically significant tumour - to - pancreatic parenchymal attenuation differences between the two groups during the arterial or portal venous phase . 
this can be explained by the fact that pancreatic carcinomas as well as normal pancreatic parenchyma showed higher contrast enhancement with higher iodine concentration during the arterial and portal venous phase . the contribution of the contrast agent to the overall diagnostic value , enhancement of each organ and depiction of blood vessels were assessed qualitatively by two blinded independent readers . 
the superiority of the 400 mgi / ml concentration for these criteria is presumably due to the generally greater contrast enhancement of the abovementioned vessels and organs in distinct perfusion phases with the higher iodine concentration and the consecutively higher contrast between certain organs and vessels . 
 [ 3 ] found that the sensitivity for detecting pancreatic adenocarcinoma was significantly greater during the pancreatic than the arterial phase and the mean attenuation of the pancreas in all patients was greatest in the pancreatic phase , at 107 hu vs . 
 [ 13 ] found that the mean absolute tumour - to - gland attenuation difference was significantly higher ( p < 0.05 ) in the pancreatic phase ( 4053 hu and 3456 hu ) than in the arterial phase ( 3138 hu and 2643 hu )  . 
further studies will be necessary to assess this issue . in summary , the higher iodine concentration leads to a greater contrast enhancement of large and small vessels in radiol med ( 2010 ) 115 : 898905 the pancreatic cta and improves the evaluation of vessels in the arterial and portal venous phase . 
scuro , verona , italy 2istituto of gastroenterologia , universit di verona , verona , italy 3istituto di radiologia , new york university medical center , new york , ny , usa correspondence to : r . 
the aim of this study was to review the computed tomography ( ct ) features of the pancreatic parenchyma and ducts in patients with gene - mutationassociated pancreatitis ( gmap )  . 
patients were divided into two groups according to the time interval between the onset of symptoms and the first ct examination ( group a 24 months and group b > 25 months )  . 
in group b patients , pancreatic duct stones were detected in 12 / 12 with gmap . stones were calcified in 10 / 12 cases and noncalcified ( protein plugs ) in 2 / 12 ; in 5 / 10 cases , the calcified stones were heterogeneous with noncalcified central core ( bullseye appearance )  . 
nel nostro studio retrospettivo , i pazienti sono stati suddivisi in 2 gruppi in base allintervallo di tempo intercorso tra insorgenza della sintomatologia ed esecuzione della prima indagine tc ( gruppo a24 mesi e gruppo b > 25 mesi )  . 
nel gruppo b erano presenti calcoli endoduttali in 12 / 12 pazienti con gmap ; in 10 / 12 casi i calcoli endoduttali erano calcifici , 2 / 12 non calcifici ( plugs ) ; in 5 / 10 casi i calcoli calcifici erano eterogenei con core centrale non calcifico ( bulls eye )  . 
il diametro medio del dotto pancreatico principale nella testa e nel corpo / coda era rispettivamente di 4 , 8 mm e 4 , 9 mm nei pazienti con gmap . 
in patients with gmap and time interval between symptom onset and first ct scan 24 months ( group a ) , ct identified normal or slightly increased parenchymal thickness and a main pancreatic duct of normal calibre and without duct stones . 
in contrast , in patients with gmap and time interval between symptom onset and first ct scan > 25 months ( group b ) , it identified large - calibre duct stones with bulls - eye appearance . 
in conclusione , la tc identifica nei pazienti con gmap e intervallo di tempo tra insorgenza della sintomatologia e prima indagine tc24 mesi ( gruppo a ) uno spessore parenchimale normale o lievemente aumentato e un dotto pancreatico principale con calibro normale senza calcoli endoduttali . 
al contrario nei pazienti con gmap e intervallo di tempo tra insorgenza della sintomatologia e prima tc > 25 mesi ( gruppo b ) calcoli endoduttali con grande diametro e morfologia a bulls eye . 
 parole chiave pancreas pancreatite cronica pancreatite genetica tomografia computerizzata introduction introduzione pancreatitis may be associated with gene mutations and , in particular , with mutations of the cystic fibrosis transmembrane regulator ( cftr ) gene [ 14 ] , serine protease inhibitor kazal type 1 ( spink1 ) gene [ 5 , 6 ] and cationic trypsinogen ( prss1 ) gene [ 7 , 8 ]  . 
patients with gene - mutation - associated pancreatitis ( gmap ) manifest clinical symptoms at an earlier age compared with patients with chronic pancreatitis due to other causes [ 9 ]  . 
a correct diagnosis of gmap guides the clinician towards appropriate treatment , which is aimed at slowing the natural progression of the disease and delaying the onset of functional pancreatic insufficiency and diabetes . 
in addition , the risk of developing pancreatic adenocarcinoma is particularly high in gmap patients [ 11 ] , probably as a result of long - standing exposure to pancreatic inflammation . 
follow - up by imaging is therefore required to detect the neoplasm at an early stage [ 12 , 13 ]  . computed tomography ( ct ) is the most commonly used modality in patients with a clinical suspicion or known diagnosis of pancreatic disease [ 1416 ] in view of its high sensitivity in detecting duct stones , which in some cases of gmap present with a noncalcified central core [ 1720 ]  . however , very few published reports have described ct features of gmap [ 21 ] owing to the rarity of this condition [ 13 ]  . 
the aim of this paper is to describe changes seen in the pancreatic parenchyma and ducts during the initial stages and follow - up of gmap , with a view to identifying the distinctive features of this disease . la pancreatite pu associarsi ad alcune mutazioni , in particolare del gene regolatore del canale transmenbrana della fibrosi cistica ( cftr ) [ 14 ] , del gene inibitore delle proteasi seriniche kazal tipo 1 ( spink1 ) [ 5 , 6 ] e del gene del tripsinogeno cationico ( prss1 ) [ 7 , 8 ]  . 
i pazienti con pancreatite associata a una di queste mutazioni genetiche manifestano sintomi clinici ad una et pi giovane rispetto a quelli con pancreatite cronica di altra eziologia [ 9 ]  . 
la diagnosi clinica di tale affezione difficile e spesso tardiva . riportato che pazienti con pancreatite associata alla mutazione del gene cftr mediamente vanno incontro a 12 ospedalizzazioni prima di arrivare alla corretta diagnosi [ 10 ]  . 
una corretta diagnosi di gmap indirizza il clinico ad una corretta terapia , volta a rallentare la naturale progressione della malattia e ritardare linsorgenza dellinsufficienza funzionale pancreatica e di diabete . 
il rischio di sviluppare un adenocarcinoma pancreatico peraltro particolarmente elevato nei pazienti con gmap [ 11 ] , probabilmente in relazione alla prolungata esposizione a flogosi ghiandolare causata dalla pancreatite cronica ; il follow - up mediante imaging perci necessario per individuare la neoplasia in fase precoce [ 12 , 13 ]  . la tomografia computerizzata ( tc ) la tecnica pi comunemente utilizzata nei pazienti con sospetto o diagnosi di patologia pancreatica [ 1416 ] , in particolare per la sua elevata sensibilit ad identificare i calcoli duttali , che in alcuni casi di gmap presentano un core centrale non calcifico [ 1720 ]  . 
lobiettivo del nostro studio di descrivere le modificazioni a cui vanno incontro il parenchima e i dotti pancreatici , nelle fasi iniziali e successivamente nel follow - up , nei pazienti con gmap , al fine di identificare le caratteristiche peculiari di tale affezione . radiol med ( 2010 ) 115 : 875888 materials and methods patient population this retrospective study included all patients with a diagnosis of gmap ( acute , recurrent or chronic ) referred to us between may 1992 and december 2006 . 
inclusion criteria were previous episodes of pancreatitis ( as demonstrated by an elevation of serum amylase and lipase three times above the upper reference limit , associated with abdominal pain ) and the presence of gene mutations . 
all gene mutations were identified on 50 mg of dna extracted from 200 ml of blood treated with ethylene diamine tetraacetic acid ( edta ) using a commercial kit ( qiagen , hilden , germany )  . 
all patients underwent contrast - enhanced ct , specifically , multislice spiral ( n = 5 ) , single - slice ( n = 13 ) and conventional ( n = 7 ) ct . twelve out of 25 ( 48% ) patients were followed up with ct ( at least two examinations ) for an average of 59.3 ( range 6120 ) months ; another 6 / 25 ( 24% ) were excluded from our follow - up because they underwent surgical procedures in the following years [ pancreaticojejunal anastomosis ( n = 3 ) , whipple resection ( n = 1 ) , distal pancreatectomy ( n = 1 ) , total pancreatectomy ( n = 1 ) ]  . 
 the time interval between the first documented clinical episode of pancreatitis and the first ct scan showed wide variations due to the heterogeneity of the retrospective patient population ; it ranged from 1 to 192 months , with a median of 24 months . 
we therefore used 24 months as a cutoff value to divide the patients into two groups : group a with early observation ( 24 months between symptom onset and ct ) and group b with delayed observation ( > 25 months between symptom onset and ct )  . imaging ct studies performed between may 1992 and december 1996 were done with conventional ct systems ( somatom dr or somatom hq , siemens , erlangen , germany )  . images were acquired in the craniocaudal direction . 
after materiali e metodi popolazione di pazienti nello studio retrospettivo abbiamo incluso tutti i pazienti con diagnosi di gmap ( in fase acuta , ricorrente o cronica ) giunti alla nostra osservazione da maggio 1992 a dicembre 2006 . lo studio stato approvato dal comitato etico , poich per la natura retrospettiva del nostro lavoro , non stato possibile ottenere il consenso informato da tutti i pazienti . 
i criteri di inclusione comprendono : precedenti episodi di pancreatite ( attestata mediante lincremento dei livelli sierici di amilasi e lipasi di tre volte rispetto al limite superiore della norma , associato a dolore addominale ) e la presenza di mutazioni genetiche . 
tutte le mutazioni genetiche sono state identificate su 50mg di dna genomico , estratto da 200 ml di sangue trattato con acido etilene - diammine - tetracetato ( edta ) , utilizzando un kit commerciale ( qiagen , hilden , germania )  . 
i criteri di esclusione comprendono precedenti procedure endoscopiche o chirurgiche . la popolazione di pazienti include 25 soggetti , 19 maschi e 6 femmine , con et media di 40 , 8 anni ( range 1068 anni ) alla prima indagine tc . 
tutti i pazienti sono stati sottoposti alla diagnosi a indagine tc con somministrazione di mezzo di contrasto endovenoso , in particolare tc spirale multistrato ( 5 pazienti ) , tc spirale monostrato ( 13 pazienti ) e tc convenzionale ( 7 pazienti )  . 
dodici su 25 ( 48% ) sono stati seguiti con un follow - up tc ( almeno due indagini ) per un periodo medio di 59 , 3 mesi ( range 6120 mesi ) ; altri 6 / 25 ( 24% ) pazienti sono stati esclusi dallo studio che riguardava il follow - up perch hanno subito negli anni successivi procedure chirurgiche ( pancreatico - digiuno anastomosi in 3 pazienti , resezione di whipple in 1 paziente , pancreasectomia distale in 1 paziente e pancreasectomia totale in 1 paziente )  . 
 lintervallo di tempo compreso tra il primo episodio clinico documentato di pancreatite e la prima indagine tc ha mostrato ampia variabilit in relazione alla disomogeneit della casistica retrospettiva con range compreso tra 1 e 192 mesi ; il suo valore mediano risultato di 24 mesi . 
abbiamo pertanto utilizzato tale valore di 24 mesi per differenziare i pazienti in un gruppo ad osservazione precoce ( gruppo a ) e uno ad osservazione pi tardiva ( gruppo b ) rispettivamente caratterizzati da un intervallo di tempo tra linsorgenza della sintomatologia e la prima tc24 mesi o > 25 mesi . immagini le indagini tc eseguite tra maggio 1992 e dicembre 1996 sono state realizzate mediante tc convenzionale ( somatom dr o somatom hq ; siemens , erlangen , germania )  . 
alla fase pre - contrastografica seguita una fase post - contrastografica utilizzando mezzo di contrasto iodato non ionico 878 radiol med ( 2010 ) 115 : 875888 precontrast imaging , a contrast - enhanced scan was obtained with intravenous administration of a 50 - ml bolus ( 2 ml / s ) of nonionic iodinated contrast material ( omnipaque 350 , amersham health , princeton , nj , usa ; iopamiro 370 , bracco , milan , italy ) via an injector ( mark v plus , medrad , pittsburgh , pa , usa ) , immediately followed by a further infusion of 100 ml ( 0.8 ml / s ) during data acquisition . 
scanning included an initial set of 8 - mmthick , partially overlapping scans ( 6 - mm table feed ) acquired 3040 s after the beginning of contrast infusion ( early phase ) , followed by a second set of scans of the pancreatic region obtained immediately after the end of the contrast infusion ( delayed phase )  . ct studies performed between january 1997 and january 2005 were acquired with a single - slice spiral ct scanner ( somatom p1us 4 , siemens )  . 
precontrast imaging of the pancreas ( thickness : 5 mm ; pitch 1.5 ) was followed by biphasic acquisition ( pancreatic arterial phase and portal phase ) after intravenous administration of a 120 - ml bolus ( 3 ml / s ) of nonionic iodinated contrast agent ( ultravist 370 , schering , berlin , germany ; visipaque 320 , amersham health ; xenetix 350 guerbet , paris , france ) via an injector ( envision ct 711 , medrad )  . 
 ct scans performed between january 2005 and december 2006 were done with a 6 - slice multidetector ct scanner with a rotation time of 0.75 ( brillance ct ; philips , eindhoven , holland )  . 
precontrast imaging was followed by a triphasic postcontrast study ( arterial pancreatic , portal and delayed phases ) acquired after intravenous administration of a 120 - ml bolus ( 4 ml / s ) of nonionic contrast material ( ultravist 370 ) via an injector ( stellant d dual syringe , medrad ) followed by 50 ml of saline ( 4ml / s )  . 
portal - phase images were acquired from the upper margin of the diaphragm to the kidneys or pelvis with a mean delay of 70 s after contrast administration ( collimation : 60.75 mm ; pitch 0.9 ) ; reconstruction thickness was 1 mm , with an interval of 0.50 mm in the arterial pancreatic phase and somministrato per via endovenosa attraverso iniettore ( mark v plus , medrad , pittsburgh , pa , usa ) con un bolo di 50 ml ( 2 ml / s ) ( omnipaque 350 , amersham health , princeton , nj ; iopamiro 370 , bracco , milano , italia ) , immediatamente seguito da infusione endovenosa di 100 ml ( 0 , 8 ml / s ) durante lacquisizione dei dati . 
inizialmente stato effettuato un set di scansioni con spessore di 8 mm con parziale overlapping ( 6 mm di velocit movimento del tavolo ) acquisite 3040 secondi dopo linizio dellinfusione del mezzo di contrasto ( fase precoce )  . 
sullarea pancreatica un secondo set di scansioni stata effettuata subito dopo la fine dellinfusione del mezzo di contrasto ( fase tardiva )  . le indagini tc eseguite tra gennaio 1997 e gennaio 2005 , sono state acquisite mediante una tc spirale singolo strato ( somatom p1us 4 , siemens , er1angen , germania )  . le immagini in fase pre - contrastografica ( spessore 5 mm , pitch 1 , 5 ) del pancreas sono state seguite da unacquisizione bifasica ( fase pancreatica arteriosa e fase portale ) utilizzando un mezzo di contrasto iodato non ionico ( ultravist 370 , schering , berlino , germania ; visipaque 320 , amersham health princeton , nj ; xenetix 350 guerbet , parigi , francia ) somministrato per via endovenosa attraverso un iniettore ( envision ct 711 , medrad , pittsburgh , pa , usa ) in un bolo di 120 m1 ( 3 ml / s )  . 
le immagini in fase pancreatica arteriosa ( spessore 3 mm , pitch 1 , 5 ) sono state acquisite 3550 secondi ( ritardo medio ) dallinizio del bolo di contrasto . 
 le tc eseguite tra gennaio 2005 e dicembre 2006 , sono state acquisite mediante una tc multidetettore a 6 strati ( tcms ) con un tempo di rotazione di 0 , 75 ( brillance ct , philips , eindhoven , olanda )  . 
mezzo di contrasto non ionico ( ultravist 370 , schering , berlino , germania ) somministrato per via endovenosa attraverso un iniettore ( stellant d dual syringe , medrad , pittsburgh , usa ) in un bolo di 120 ml ( 4 ml / s ) seguito da 50 ml di soluzione fisiologica ( 4 ml / s )  . 
i parametri di scansione sono 120 kvp , 250 ma , a 0 , 9 pitch e collimazione di 61 , 5 mle immagini in fase pancreatica arteriosa sono state acquisite da 1 cm sopra il tripode celiaco fino a comprendere lintera ghiandola pancreatica dopo 40 secondi ( ritardo medio ) dallinizio del bolo di contrasto ( collimazione : 60 , 75 mm ; pitch 0 , 9 )  . 
le immagini in fase portale sono state acquisite dal margine superiore del diaframma fino a comprendere i reni o la pelvi dopo 70 secondi ( ritardo medio ) dallinizio del bolo di contrasto ( collimazione : 60 , 75 mm ; pitch 0 , 9 ) ; lo spessore di ricostruzione stato di 1 mm nella fase arteriosa pancreatica e portale con un intervallo di 0 , 50 mle immagini in fase tardiva sono state acquisite dal margine superiore del diaframma fino al processo uncinato del pancreas dopo 120 radiol med ( 2010 ) 115 : 875888 portal phase . 
delayed - phase images were acquired from the upper margin of the diaphragm to the uncinate process of the pancreas after a mean delay of 120 s from the beginning of contrast administration ( collimation : 61.5 mm ; pitch : 0.9 ) ; reconstruction thickness was 2 mm , with an interval of 1 mm . image analysis images were reviewed by three radiologists ( rm , rg , cc ) with > 10 years experience in gastrointestinal imaging . images were reviewed as hard copies in 7 / 25 patients or as soft - copy displays on the workstation in 18 / 25 . 
thirteen of 25 patients with gmap underwent the first ct scan within 24 months of symptom onset ( median 16 , range 124 months ) , whereas 12 / 25 la mutazione del gene del cftr stata riscontrata in 13 / 25 ( 52% ) pazienti , quella del gene spink1 in 9 / 25 ( 36% ) pazienti e quella del gene prss1 in 3 / 25 ( 12% ) pazienti . 
tredici su 25 pazienti con gmap hanno effettuato la prima tc entro 24 mesi dallinsorgenza della sintomatologia ( mediana 16 mesi , range 124 mesi ) , mentre 12 / 25 pazienti con gmap hanno effettuato la prima tc dopo 25 mesi ( mediana 100 mesi , range 26192 mesi )  . 
nel gruppo di pazienti con tc > 25 mesi , 4 / 12 ( 33% ) sono risultati positivi alla mutazione per il gene spink1 880 radiol med ( 2010 ) 115 : 875888 patients underwent the first ct scan after 25 months ( median 100 , range 26192 months )  . 
 analisi qualitativa la variabilit interosservatore ha dato una concordanza ottima per i seguenti parametri : presenza / assenza di calcoli endoduttali ( 0 , 948 ) , calcificazione dei calcoli endoduttali ( 1 , 00 ) , sede dei calcoli nella testa ( 1 , 00 ) e nel corpo / coda ( 0 , 949 ) , localizzazione dei calcoli nel dotto pancreatico principale ( 0 , 897 ) e nei dotti collaterali ( 0 , 947 ) , struttura dei calcoli endoduttali ( 0 , 847 )  . 
1a - d gene - mutation - associated pancreatitis ( spink1 : a , b ; cftr : c , d ) with time interval between symptom onset and first ct scan 24 months ( group a )  . 
ct performed 12 months after symptom onset shows increased parenchymal thickness ( a , b ) , normal thickness ( c , d ) and enhancement of the body / tail ( a , c ) and head ( b , d ) , similar to that of the renal cortex . 
1a - d pancreatite associata a mutazione genetica ( spink1 : a , b ; cftr : c , d ) con intervallo tra linsorgenza della sintomatologia e la prima indagine tc24 mesi ( gruppo a )  . 
lindagine tc espletata a 12 mesi dallinsorgenza della sintomatologia dimostra dimensioni del parenchima pancreatico aumentate in a , b , normali in c , d e unimpregnazione nel corpo / coda ( a , c ) e nella testa ( b , d ) analoga a quella della corticale renale . 
in entrambi i pazienti era presente un lieve aumento del diametro del dotto pancreatico principale ( a , c : frecce ) , assenza di calcoli duttali in a , b , qualche piccolo calcolo ( c : teste di frecce ) nel dotto pancreatico principale della coda in c , d . radiol med ( 2010 ) 115 : 875888 fig . 
2a - d gene mutation associated pancreatitis ( spink1 : a , b ; cftr : c , d ) with time interval between symptom onset and first ct scan > 25 months ( group b )  . 
ct scan : precontrast ( a ) postcontrast pancreatic phase ( b - d ) ; axial images ( a , c , d ) ; curved multiplanar reconstruction ( b )  . 
ct scan ( a , b ) performed 112 months after symptom onset in a patient with gmap associated with spink1 gene mutation shows dilatation of the main pancreatic duct and multiple large duct stones in the pancreatic head and body / tail ; parenchymal thickness is significantly reduced . 
axial image ( a ) and curved multiplanar reconstruction ( b ) with bone window settings demonstrate the heterogeneous structure of stones with hypodense central core ( bulls - eye pattern )  . 
ct scan ( c , d ) obtained 62 months after symptom onset in a patient with gmap associated with cftr gene mutation ; the pancreatic parenchyma appears hypoattenuating compared with the renal cortex . 
2a - d pancreatite associata a mutazione genetica ( spink1 : a , b ; cftr : c , d ) con intervallo tra linsorgenza della sintomatologia e la prima indagine tc > 25 mesi ( gruppo b )  . 
indagine tc : fase pre - contrastografica ( a ) , fase contrastografica pancreatica ( b - d ) ; immagini assiali ( a , c , d ) ; ricostruzione multiplanare curvilinea ( b )  . 
a , b lindagine tc espletata a 112 mesi dallinsorgenza della sintomatologia in paziente con gmap associata alla mutazioni del gene spink1 dimostra una dilatazione del dotto pancreatico principale e presenza di multipli calcoli endoduttali nella testa e nel corpo / coda della ghiandola di cospicue dimensioni ; lo spessore del parenchima pancreatico molto assottigliato . 
nellimmagine assiale ( a ) e nella ricostruzione multiplanare curvilinea ( b ) con valori di finestra per il tessuto osseo si dimostra la struttura eterogenea dei calcoli caratterizzata dalla presenza di core centrale ipodenso ( bulls eye )  . 
c , d allindagine tc espletata a 62 mesi dallinsorgenza della sintomatologia tc in paziente con gmap associata alla mutazione del gene cftr il parenchima ghiandolare risulta ipovascolare rispetto alla corticale renale . 
il parenchima pancreatico , comparato alla corticale renale in fase pancreatica ( fig . 1 ) , risultato ipovascolare in 7 / 13 ( 54% ) pazienti e isovascolare in 6 / 13 ( 46% ) gmap pazienti . gruppo b ( tc > 25 mesi dallinsorgenza della sintomatologia ) calcoli endoduttali sono risultati presenti in tutti i pazienti 12 / 12 con gmap . 
3a - d gene mutation associated pancreatitis ( prss1 : a , b ; cftr : c , d ) with time interval between symptom onset and the first ct scan > 25 months ( group b )  . 
ct scan : precontrast image ( a ) , postcontrast pancreatic phase ( b ) and portal phase ( c ) ; curved multiplanar reconstruction ( b ) , axial images ( a , c )  . magnetic resonance imaging : axial image , t2 - weighted sequence ( d )  . 
ct performed 88 months after symptom onset ( a , b ) in a patient with gmap associated with prss1 gene mutation shows dilatation of the main pancreatic duct with multiple large duct stones in the pancreatic head and body / tail ; parenchymal thickness is significantly reduced . 
contrast - enhanced ct ( c ) shows dilatation of the main duct at the level of the pancreatic body / tail ; solid , hypodense , noncalcified intraductal defects are appreciated ( protein plugs : arrows )  . 
3a - d pancreatite associata a mutazione genetica ( prss1 : a , b ; cftr : c , d ) con intervallo tra linsorgenza della sintomatologia e la prima indagine tc > 25 mesi ( gruppo b )  . 
indagine tc : fase pre - contrastografica ( a ) , fase contrastografica pancreatica ( b ) e fase contrastografica venosa ( c ) ; ricostruzione multiplanare curvilinea ( b ) , immagini assiali ( a , c )  . 
a , b lindagine tc espletata a 88 mesi dallinsorgenza della sintomatologia tc in paziente con gmap associata alla mutazione del gene prss1 dimostra una dilatazione del dotto pancreatico principale con presenza di multipli calcoli endoduttali , nella testa e nel corpo / coda della ghiandola pancreatica con diametro cospicuo ; lo spessore del parenchima pancreatico molto assottigliato . 
la ricostruzione multiplanare curvilinea ( b ) e le immagini assiali utilizzando valori di finestra per il tessuto osseo ( a ) dimostrano la presenza di calcoli con morfologia omogenea e senza core centrale ipodenso . 
c , d lindagine tc in fase contrastografica ( c ) dimostra la dilatazione del dotto pancreatico principale a livello del corpo / coda del pancreas ; sono presenti difetti endoduttali solidi , ipodensi , non calcifici ( plugs : frecce )  . 
lindagine rm con sequenza t2 dipendente ( d ) dimostra difetti endoduttali ( frecce ) che corrispondono ai calcoli endoduttali non calcifici ( plugs ) , erroneamente interpretati come vegetazioni di tumore intraduttale mucino - papillare ( ipmt )  . group b ( ct > 25 months after symptom onset ) duct stones were detected in 12 / 12 gmap patients . 
4a - d progression of gene mutation associated pancreatitis ( cftr : a , b ; spink1 : c , d ) with time interval between symptom onset and first ct scan 24 months ( group a : a , b ) and > 25 months ( group b : c , d )  . 
initial ct performed in 1999 24 months after symptom onset ( a ) demonstrates a normal - size main pancreatic duct and the absence of duct stones . follow - up ct performed 8 years later , in 2007 , ( curved multiplanar reconstruction : b ) shows dilatation of the main duct in the pancreatic tail with evidence of multiple duct stones in the pancreatic head and body / tail ( arrows )  . 
initial ct scan performed > 25 months after symptom onset in 1997 ( c ) demonstrated a few stones inside the dilatated main duct in the pancreatic body / tail . 
4a - d evoluzione della pancreatite associata mutazione genetica ( cftr : a , b ; spink1 : c , d ) con intervallo tra linsorgenza della sintomatologia e la prima indagine tc 24 mesi ( a , b : gruppo a ) e > 25 ( c , d : gruppo b )  . 
a , b lindagine tc iniziale eseguita a meno di 24 mesi dallinsorgenza della sintomatologia , espletata nel 1999 ( a ) dimostra un dotto pancreatico principale di calibro normale ed assenza di calcoli endoduttali . 
lindagine tc di follow - up espletata 8 anni dopo ( 2007 ) ( ricostruzione multiplanare curvilinea : b ) dimostra la dilatazione del dotto pancreatico principale nella coda con evidenza di multipli calcoli endoduttali nella testa e nel corpo / coda del pancreas ( frecce )  . 
c , d lindagine tc iniziale eseguita a pi di 25 mesi dallinsorgenza della sintomatologia , espletata nel 1997 ( c ) dimostra qualche calcolo nel contesto del dotto pancreatico principale dilatato nel corpo / coda del pancreas . 
il diametro massimo dei calcoli intraduttali risultato di 5 884 radiol med ( 2010 ) 115 : 875888 table 1 imaging findings in patients with gene - mutation - associated pancreatitis ( gmap ) and time interval between symptom onset and first computed tomography ( ct ) scan 24 months ( group a )  . 
mean diameter of the main pancreatic duct at the head and body / tail was 4.8 mm ( range 110 mm ) and 4.9 mm ( range 110 mm ) , respectively . 
mean diameter of the choledochus at the hepatic hilum and in the intrapancreatic segment was 7.8 mm ( range 120 mm ) and 5.8 mm ( range 510 mm ) , respectively . mil numero medio di calcoli intraduttali per paziente risultato di 0 , 8 ( range 07 , numero totale 10 )  . 
il diametro medio del coledoco misurato allilo epatico e nel tratto intrapancreatico risultato rispettivamente di 7 , 8 mm ( range 120 mm ) e 5 , 8 mm ( range 510 mm )  . gruppo b ( tc > 25 mesi dallinsorgenza della sintomatologia ) lo spessore medio del parenchima pancreatico nella testa , radiol med ( 2010 ) 115 : 875888 table 3 imaging findings during follow - up of patients with gene - mutation - associated pancreatitis with time interval between symptom onset and first computed tomography ( ct ) scan 24 months ( group a ) and > 25 months ( group b )  . 
quantitative image analysis number of stones parenchymal thickness head ( mm ) parenchymal thickness body ( mm ) parenchymal thickness tail ( mm ) mean diameter of stones diameter of main duct head ( mm ) diameter of main duct body / tail ( mm ) group a first ct 284 228 157 last cta 1818 224 155 107 amean time interval between first and last ct study 6129 months ( range 26120 ) bmean time interval between first and last ct study 6641 months ( range 40116 ) tabella 3 caratteristiche imaging nel follow - up dei pazienti con gmap con un intervallo di tempo tra linsorgenza della sintomatologia e la prima tomografia computerizzata ( tc ) 24 mesi ( gruppo a ) e > 25 mesi ( gruppo b )  . 
mean diameter of the main pancreatic duct at the head and body / tail was 18.8 mm ( range 140 mm ) and 13.9 mm ( range 230 mm ) , respectively . 
mean diameter of duct stones was 21.9 mm ( range 250 mm ) ; only one patient had duct stones < 5 mmean number of duct stones per patient was 11.4 ( range 330 , total number 137 )  . 
the time interval between the first and last ct scan was 6129 ( range 26120 ) months in group a and 6641 ( range 30144 ) months in group b , with no difference between groups . 
in 5 / 6 ( 83% ) , the stones appeared at nel corpo e nella coda stato rispettivamente di 12 , 3 mm , 11 , 8 mm e 11 , 1 mil diametro medio del dotto pancreatico principale nella testa e nel corpo / coda rispettivamente di 18 , 8 mm ( range 140 mm ) e 13 , 9 mm ( range 230 mm )  . il diametro medio dei calcoli endoduttali risultato 21 , 9 mm ( range 250 mm ) ; solo un paziente aveva calcoli intraduttali con diametro inferiore ai 5 mil numero medio di calcoli intraduttali per paziente risultato 11 , 4 ( range 330 , numero totale 137 )  . 
lintervallo di tempo tra la prima e lultima tc stato di 6129 mesi ( range 26120 mesi ) nei pazienti del gruppo a e 6641 mesi ( range 30144 mesi ) nei pazienti del gruppo b senza nessuna differenza tra i due gruppi . 
lo spessore parenchimale ha subito solo una modesta riduzione ( tabella 3 )  . discussion discussione some rare forms of chronic pancreatitis that occur in the absence of risk factors [ 9 ] are associated with gene mutations [ 14 ] , including mutation of the cftr gene ( the most common ) , the spink1 gene and the prss1 gene . 
in our study , cftr mutation was the most frequent ( 52% ) , followed by the less common spink1 mutation ( 36% ) and the rare prss1 mutation ( 12% )  . 
of the 25 patients in our study , 76% were males . patients with gmap experience early symptom onset compared with patients with obstructive pancreatitis [ 15 ]  . in our series , the mean age of patients at symptom onset was 40.8 years , which is similar to the age reported by cohn et al . 
despite earlier symptom onset , the diagnosis of gmap was established late in these patients , with each patient being hospitalised several times before the disease was correctly identified [ 2 ]  . 
 ct is a commonly used imaging modality in patients with chronic pancreatitis owing to its excellent performance in identifying duct stones or protein plugs [ 19 , 20 ]  . however , no published study has reported on the specific ct features of gmap . 
ct features of gmap in patients with time interval between symptom onset and first ct scan > 25 months ( group b ) are the alcune forme rare di pancreatite cronica che insorgono in assenza di fattori di rischio [ 9 ] sono associate ad alcune mutazioni genetiche [ 14 ] ; la mutazione del gene cftr la pi frequente , la mutazione del gene spink1 e del gene prss1 . 
nel nostro studio , la mutazione del gene del cftr risultata la pi comune ( 52% ) , la mutazione spink1 meno frequente ( 36% ) e quella prss1 pi rara ( 12% ) ; il 76% del nostro gruppo di pazienti erano maschi . i pazienti con gmap mostravano uninsorgenza della sintomatologia precoce se comparata con le altre pancreatiti ostruttive [ 15 ]  . 
nel nostro studio lintervallo di tempo intercorso tra linsorgenza dei sintomi e la diagnosi risultato di 56 , 2 mesi . una corretta diagnosi di pancreatite associata a mutazione genetica particolarmente importante in questi pazienti poich hanno un rischio di sviluppare un adenocarcinoma pancreatico pi alto rispetto ai pazienti affetti da altre forme di pancreatite cronica [ 12 , 13 ]  . 
were the first to report the presence of stones with a dense peripheral margin and radiolucent central core at plain abdominal radiography in three patients with chronic pancreatitis ; these stones had a diameter > 23 mm [ 17 ]  . 
described three generations of patients with chronic pancreatitis who at endoscopic retrograde cholangiopancreatography showed large stones distributed along the entire gland and with bulls - eye appearance due to the presence of a central radiolucent core [ 18 ]  . 
another limitation is the possibility that atrophy of the pancreatic parenchyma relative to normal values was due to advanced age of some patients . in conclusion , in patients with gmap and time interval between symptom onset and first ct scan 24 months ( group a ) , ct identified a normal or slightly increased parenchymal thickness and a normal - size main pancreatic duct without duct stones . 
by contrast , in patients with gmap and time interval between symptom onset and first ct scan > 25 months ( group b ) , ct showed large - size duct stones with bulls - eye appearance . 
 [ 18 ] , nel 1999 , hanno descritto 3 generazioni di pazienti , studiati con colangio - pancreatografia endoscopica retrograda , tutti con pancreatite cronica che presentavano calcoli di grandi dimensioni , distribuiti lungo tutta la ghiandola , con aspetto a bulls eye per la presenza di un centro radiotrasparente . 
altro limite riguarda la possibilit che latrofia del parenchima ghiandolare nei pazienti con gmap correlato ai valori normali sia dovuta allet avanzata di alcuni pazienti . in conclusione , la tc identifica nei pazienti con gmap e intervallo di tempo tra insorgenza della sintomatologia e prima indagine tc24 mesi ( gruppo a ) uno spessore parenchimale normale o lievemente aumentato e un dotto pancreatico principale con calibro normale senza calcoli endoduttali . 
al contrario nei pazienti con gmap e intervallo di tempo tra insorgenza della sintomatologia e prima tc > 25 mesi ( gruppo b ) calcoli endoduttali con grande diametro e morfologia a bulls eye . 
the treatments were performed with a microwave generator with 45 w and 915 mhz connected to a 14.5 - gauge antenna for 10 min . antenna placement was performed with computed tomography ( ct ) fluoroscopy guidance or xperguide . 
this study shows that in selected patients , mwa is a valid alternative to other ablative techniques . further studies are required to demonstrate the shortand long - term effects of this technique and to make a comparison with other available ablation systems , especially with radiofrequency . keywords microwave ablation lung tumour riassunto obiettivo . 
lo scopo dello studio stato quello di valutare il successo tecnico , la sicurezza , lefficacia della metodica del trattamento ablativo mediante microonde ( mw ) in 9 pazienti affetti da neoplasia polmonare non trattabile chirurgicamente . 
stato utilizzato un sistema ablativo costituito da un generatore di mw a 45 w e 915 mhz connesso ad un antenna 14 , 5 g , per un tempo di ablazione totale di 10 minuti . 
sono tuttavia necessari ulteriori studi per confermare a breve e lungo termine lefficacia di questa metodologia e permettere un confronto con altri sistemi ablativi , in particolare rispetto alla radiofrequenza . parole chiave ablazione con microonde tumore polmonare radiol med ( 2010 ) 115 : 962974 introduction surgery is still the treatment of choice for non - small - cell lung cancer ( nsclc ) [ 1 , 2 ]  . 
over the years , various ablation techniques have been developed , including ethanol ablation , laser ablation , cryoablation and radiofrequency ablation ( rfa ) [ 3 , 4 ]  . 
the most widely used technique is radiofrequency ablation [ 512 ]  . microwave ablation ( mwa ) therapy is a relatively new technique that can be applied to different types of tumours . it is able to offer all the benefits of rfa as well as some substantial advantages . 
these include larger volumes of cellular necrosis , reduced procedure times , greater temperatures delivered to the target lesion , the possibility of the simultaneous use of multiple antennae , efficacy on lesions with cystic components and / or in proximity to vascular structures > 3 mm in diameter with a reduction in the heat - sink effect , and less intraprocedural pain [ 5 , 6 , 1322 ]  . in the radiation spectrum , microwaves lie between infrared and radio waves , with a frequency between 900 and 2 , 450 mhz [ 6 ]  . 
microwaves induce the oscillation of water molecules at a speed between 2 and 5 billion times per second , depending on the frequency of the microwaves themselves [ 5 , 6 , 16 , 17 ]  . 
cell death is produced by thermocoagulation and necrosis as a result of the heat generated by oscillations of ions induced by the microwaves , the degree of which is proportional to the intensity and frequency of the microwaves themselves [ 6 , 7 ]  . 
the aim of this study was to demonstrate the technical success , safety and efficacy of mwa in nine patients affected by unresectable lung cancer . introduzione la terapia chirurgica rimane il trattamento di scelta per il carcinoma polmonare non a piccole cellule ( nsclc ) [ 1 , 2 ]  . tuttavia , solo il 20% di tutti i nsclc diagnosticati risulta essere chirurgicamente resecabile [ 1 , 2 ] ci ha pertanto spinto verso la ricerca di metodi alternativi al trattamento chirurgico , quali le tecniche ablative , per consentire il controllo locale di tumori non resecabili [ 3 , 4 ]  . 
nel corso degli anni sono state sviluppate diverse tecniche ablative : ablazione con etanolo , laserablazione , crioablazione e termoablazione mediante radiofrequenza ( rfa ) [ 3 , 4 ]  . attualmente la metodica pi diffusamente impiegata nella pratica clinica la radiofrequenza [ 512 ]  . la tecnologia delle microonde ( mw ) un trattamento ablativo relativamente nuovo applicabile a differenti tipologie di neoplasie , in grado di offrire tutti i benefici della radiofrequenza , presentando inoltre sostanziali vantaggi , quali : volumi di necrosi cellulare pi ampi , riduzione del tempo di procedura , maggiori temperature alla lesione target , possibilit di utilizzare multiple antenne simultaneamente , efficacia su lesioni con componente cistica e / o in prossimit di strutture vascolari > 3 mm di diametro con riduzione dellheat sink effect , minore dolore intraprocedurale [ 5 , 6 , 1322 ]  . 
le microonde , inducendo loscillazione delle molecole dacqua con movimenti di rotazione su se stesse in avanti ed indietro ad una velocit di 25 miliardi di volte al secondo dipendente dalla frequenza delle onde stesse [ 5 , 6 , 16 , 17 ]  . 
la morte cellulare avviene attraverso necrosi termocoagulativa grazie al calore generato dalloscillazione degli ioni indotta dalle microonde in proporzione allintensit ed alla frequenza delle onde stesse [ 6 , 7 ]  . 
lo scopo dello studio stato quello di dimostrarare il successo tecnico , la sicurezza , lefficacia della metodica del trattamento ablativo mediante mw in 9 pazienti affetti da neoplasia polmonare non trattabile chirurgicamente . 
nine patients ( seven men , two women ) with a mean age of 78 ( range 6988 ) years who underwent percutaneous mwa of ten intraparenchymal pulmonary masses ( mean 1.1 lesions per patient ) in ten ablation sessions between 26 november 2008 and 12 august 2009 were enrolled in the study ( table 1 )  . 
 all selected patients had neoplastic disease that was judged to be inoperable on the basis of tumour stage , comorbidities , advanced age and / or refusal to undergo surgery . 
dal 26 novembre 2008 al 12 agosto 2009 sono stati arruolati nello studio 9 pazienti ( 7 maschi , 2 femmine ) con unet media di 78 anni ( range 6988 anni ) e sottoposti a trattamento termoablativo percutaneo con mw di 10 masse intraparenchimali polmonari ( media di 1 , 1 lesioni per paziente ) in 10 sessioni dablazione ( tabella 1 )  . 
of masses location long - axis diameter ( mm ) follow - up ( months ) squamous cell carcinoma apicoposterior segment left upper lobe 2a ( postmwa recurrent lesion ) 2a ( recidiva 45 lesione post - mwa ) 82 m squamous cell carcinoma 77 m adenocarcinoma 78 m squamous cell carcinoma 69 m neuroendocrine carcinoma 79 m adenocarcinoma 82 m adenocarcinoma 88 m squamous cell carcinoma squamous cell carcinoma iv ( m1 ) 1 iv ( m1 ) 1 iv ( m1 ) 1a apical segment of left lower lobe right lower lobe right lower lobe right lower lobe right middle lobe left upper lobe right lower lobe left upper lobe 3 deceased m , male ; f , female ; mwa , microwave ablation tabella 1 pazienti e caratteristiche delle lesioni tumorali numero pazienti sesso istologia stadio numero masse sede diametro massimo lesione ( mm ) follow - up ( mesi ) carcinoma squamoso segmento apico - dorsale lobo superiore sinistro m carcinoma squamoso m adenocarcinoma m carcinoma squamoso m carcinoma neuroendocrino m adenocarcinoma iv ( m1 ) iv ( m1 ) iv ( m1 ) m adenocarcinoma m carcinoma squamoso carcinoma squamoso m , maschio ; f , femmina ; mwa , ablazione con microonde segmento apicale lobo inferiore sinistro lobo inferiore destro lobo inferiore destro lobo inferiore destro lobo medio destro 3 morte lobo superiore sinistro lobo inferiore destro lobo superiore sinistro were discussed with all patients prior to treatment . 
i pazienti in terapia anticoagulante e / o antiaggregante hanno sospeso il trattamento almeno 7 giorni prima della procedura , radiol med ( 2010 ) 115 : 962974 baseline imaging pretreatment imaging consisted of a thoracic multidetectorrow computed tomography ( mdct ) scan extending to the abdomen ( aquilion 64 , toshiba , japan ) with and without contrast administration . 
the contrast - enhanced scans were acquired after injection of 100 ml of iodinated contrast agent ( visipaque 320 , ge healthcare , usa ) at an injection rate of 3 ml / s , followed by injection of 40 ml saline at a rate of 2 ml / s . 
one week prior to the ablation treatment , all patients underwent percutaneous pulmonary biopsy under ct guidance , with histological confirmation of nsclc for all lesions . pretreatment procedure before the beginning of each procedure , local anaesthesia of the antenna entrance site was achieved with subcutaneous injection of a 10 - ml solution of 2% carbocaine . 
each patient was kept in a state of moderate sedation through intravenous administration of a combination of midazolam ( 0.070.08 mg / kg ) , propofol ( 0.52.0 mg / kg / h ) and fentanyl ( 12 g / kg )  . 
adequate antibiotic prophylaxis was achieved with intravenous administration of 1 g of cefazolin sodium ( ancef , smithkline beecham pharmaceuticals , philadelphia , usa ) given every 8 h for 24 h , beginning shortly before the procedure . equipment imaging guidance introducendo eparina frazionata se necessario . 
 baseline imaging limaging pre - trattamento stato ottenuto mediante indagine con tomografia computerizzata ( tc ) multistrato toracica con estensione addominale ( aquilion 64 , toshiba , giappone ) , con e senza iniezione di mezzo di contrasto ( mdc )  . 
le scansioni con mdc sono state eseguite iniettando 100 ml di contrasto iodato ( visipaque 320 , ge healthcare , usa ) ad una velocit di 3 ml / s seguito dalliniezione di 40 ml di soluzione salina ad una velocit di 2 ml / s . 
una settimana prima del trattamento ablativo tutti i pazienti sono stati sottoposti a biopsia polmonare percutanea sotto guida tc con conferma istologica di nsclc per tutte le lesioni . procedure pre - trattamento prima dellinizio di ciascuna procedura stata eseguita unanestesia locale in sede dingresso dellantenna attraverso liniezione sottocutanea di una soluzione di 10 ml al 2% di carbocaina . 
ciascun paziente stato mantenuto in regime di sedazione moderata , ottenuta mediante la somministrazione per via endovenosa di una combinazione di midazolam ( 0 , 070 , 08 mg / kg ) , propofol ( 0 , 52 mg / kg / h ) e fentanil ( 12 g / kg )  . 
unadeguata profilassi antibiotica stata raggiunta mediante la somministrazione endovena di 1 g di cefazolina sodica ( ancef , smithkline beecham pharmaceuticals , philadelphia , usa ) somministrata ogni 8 ore per 24 ore , iniziando poco prima della procedura . in eight out of ten sessions ( 7 / 10 lesions ) , the antenna was placed under ct fluoroscopy guidance , whereas in the remaining two sessions ( 3 / 10 lesions ) , the procedure was performed with xperguide . 
the choice of imaging guidance was made on a random basis . equipaggiamento imaging guidance microwave equipment and percutaneous microwave ablation procedure an ablation system was used comprising a microwave generator ( evident microwave ablation system , covidien ltd ) capable of producing 45 w at 915 mhz , connected by coaxial cable to a 14.5 - gauge straight microwave antenna with a 3.7 - cm radiating section . 
the antennae were continuously perfused with saline solution at room temperature at 60 ml / min to avoid possible thermal damage along the proxin 8 sessioni su 10 ( 7 / 10 lesioni ) il posizionamento dellantenna stato eseguito sotto guida fluoro - tc , mentre nelle restanti due sessioni ( 3 / 10 lesioni ) la procedura stata eseguita sotto guida xperguide . 
 apparecchiatura per microonde e procedura ablativa percutanea mediante microonde stato utilizzato un sistema ablativo costituito da un 966 radiol med ( 2010 ) 115 : 962974 imal semiaxis of the antenna . 
according to manufacturer specifications , ablation was performed by inserting the antenna within the lesion and maintaining a power of 45 w for a total ablation time of 10 min in order to obtain a necrosis volume of approximately 3.5 cm in diameter ( table 2 )  . 
at 2 h from the procedure , each patient underwent chest radiography to evaluate the presence of immediate complications . follow - up all patients underwent ct follow - up with and without contrast administration at 1 , 3 and 6 months in combination with complete blood and metabolic tests . 
the contrast - enhanced scans were obtained after administration of 100 ml of iodinated contrast agent ( visipaque 320 , ge healthcare ) injected at a rate of 3 ml / s , followed by 40 ml of saline solution at a rate of 2 ml / s . 
the following imaging characteristics were evaluated : maximum postablation diameter of the mass ; presence of cavitation ; absent lesion enhancement ( < 15 hu ) ; pleural effusion ; adenopathy ( short axis > 1 cm ) ; total volume of the ablated area ( calculated with volume analysis software , vitrea 2 , software 3.8 , vital images inc , minnesota , usa )  . outcomes : technical success , safety and efficacy of the technique technical success was defined as the correct positioning of the antennae within the lesion . 
all patients were evaluated for the presence of postablation syndrome [ 24 ]  . pain was evaluated on the basis of a visual analogue scale ( vas ) [ 25 ]  . 
the effectiveness of the technique was defined as complete absence of enhancement ( hu < 15 ) within the ablation zone on contrast - enhanced ct images [ 13 ]  . results tumours were measured in the three dimensions obtaining a mean index of the maximum diameter of 29.5 mm ( range 1469 mm ) ( table 3 )  . 
come suggerito dalla casa costruttrice , il trattamento ablativo stato eseguito inserendo lantenna allinterno della lesione , mantendendo una potenza di 45 w per un tempo di ablazione totale di 10 minuti , al fine di ottenere un volume di necrosi approssimativo di 3 , 5 cm di diametro ( tabella 2 )  . 
le lesioni con diametro massimo 3 cm ( 8 / 10 lesioni ) sono state trattate con singola antenna , mentre nel caso di lesioni con diametro massimo > 3 cm ( 2 / 10 lesioni ) sono state posizionate due antenne simultaneamente ad una distanza di circa 1 cm luna dallaltra per ottenere unadeguata necrosi . 
al termine di ogni procedura , eseguita sia sotto guida fluorotc che xperguide , stato eseguito un controllo fluoro - tc . dopo lablazione i pazienti sono stati trasferiti presso la recovery room radiologica in osservazione . 
 follow - up i pazienti sono stati sottoposti a follow - up mediante tc senza e con iniezione di mdc ad 1 , 3 e 6 mesi dalla procedura in associazione ad indagini sieroematiche e metaboliche complete . 
le scansioni con mdc sono state eseguite iniettando 100 ml di contrasto iodato ( visipaque 320 , ge healthcare ) ad una velocit di 3 ml / s seguito dalliniezione di 40 ml di soluzione salina ad una velocit di 2 ml / s . 
sono state valutate le seguenti caratteristiche allimaging : diametro massimo post - ablazione della massa ; presenza di cavitazione ; assenza di ehnancement della lesione ( < 15 h ) ; soffusione pleurica ; adenopatia ( asse corto > 1 cm ) , volume totale dellarea ablata ( calcolato mediante lutilizzo di un software , vitrea 2 , software 3.8 , vital images inc , minnesota , usa )  . outcomes : successo tecnico , sicurezza ed efficacia della metodica il successo tecnico stato definito come il corretto posizionamento dellantenna allinterno dell lesione . 
lefficacia della metodica stata definita come la completa assenza di ehnancement ( h < 15 ) allinterno della zona ablata alle scansioni tc con iniezioni di mdc [ 13 ]  . 968 radiol med ( 2010 ) 115 : 962974 the tumours were metastases from primary pulmonary tumours located in the contralateral lung ( stage iv , m1 )  . risultati technical success safety technical success was 100% . 
there was one death at 3 months of a 69 - year - old male patient affected by stage iv neuroendocrine carcinoma of the left lobe caused by a combination of factors related to the systemic disease associated with comorbidities . 
there were no cases of symptomatic grade 2 pneumothorax , nor were there any cases of skin burns induced by microwave - related thermal damage [ 12 , 21 ]  . 
complete necrosis was observed in nine out of ten lesions . imaging characteristics of lesions during follow - up ct fluoroscopy scans obtained in the periprocedural period showed the presence of tumour necrosis as a result of the thermal effect induced by the microwaves . 
additional ct scans were performed at intervals of 1 ( all patients ) , 3 ( 8 / 9 patients ) and 6 months ( 3 / 9 patients )  . after an initial increase of 0.67 cm in maximum diameters , there was a persistent reduction in diameter of the ablated areas at subsequent examinations , consistent with consolidation of the pulmonary parenchyma . 
secondo lanalisi istologica tutte le lesioni considerate sono risultate essere neoplasie polmonari nsclc : 6 carcinomi polmonari a cellule squamose , 3 adenocarcinomi , 1 carcinoma neuroendocrino ( tabella 1 )  . 
 successo tecnico sicurezza il successo tecnico stato del 100% : in tutti i casi lantenna stata correttamente posizionata allinterno della lesione [ 6 ]  . non abbiamo riportato complicanze maggiori nel periodo intrae peri - procedurale . 
a 3 mesi dal trattamento si verificata morte in un paziente maschio di 69 anni , affetto da carcinoma neuroendocrino stadio iv del lobo sinistro , causata dalla combinazione di fattori legati alla patologia sistemica in associazione a comorbidit . 
of masses pre - mwa long - axis diameter ( mm ) long - axis diameter at 1 month ( mm ) contrast enhancement ( hu ) cavitation effusion pleural adenopathy 2a recurrent 45 2a recidiva 45 1 - 72 - f 2 - 82 - m 3 - 77 - m 4 - 78 - m 5 - 69 - m 6 - 79 - m 7 - 82 - m 8 - 88 - m 9 - 75 - f 1 - 72 - f 2 - 82 - m 3 - 77 - m 4 - 78 - m 5 - 69 - m 6 - 79 - m 7 - 82 - m 8 - 88 - m 9 - 75 - f long - axis diameter at 3 months ( mm ) patient death at 3 months after mwa absent absent present present present absent absent absent present absent present absent absent absent present present absent absent absent absent absent absent absent absent < 1 cm absent absent absent absent absent absent absent absent morte paziente < 15 a 3 mesi da mwa assente assente presente presente presente assente assente assente presente assente presente assente assente assente presente presente assente assente assente assente assente assente assente assente < 1 cm assente assente assente assente assente assente assente assente m , male ; f , female ; mwa , microwave ablation ; fu , follow - up tabella 3 caratteristiche delle lesioni al follow - up mediante tc numeroet - sesso numero masse dimensioni lesioni premwa ( mm ) dimensioni lesioni fu 1 mese ( mm ) dimensioni lesioni fu 3 mesi ( mm ) contrast ehnancement cavitazione soffusione linfoadepleurica nopatia m , maschio ; f , femmina ; mwa , ablazione con microonde ; fu , follow - up several days after the procedure . 
the total follow - up period was recorded in all patients as the time from the date of the procedure to the most recent ct scan , with mean duration being 3.6 ( range 19 ) months . discussion over the years , several ablation techniques have been developed for local control of unresectable tumours : ethanol ablation , laser ablation , cryoablation and radiofrequency therdella massa tumorale come effetto termico indotto dalle microonde . 
ad intervalli di 1 ( tutti i pazienti ) , 3 ( 8 / 9 pazienti ) e 6 mesi ( 3 / 9 pazienti ) sono state eseguite ulteriori scansioni tc . 
 stato quindi osservato un incremento iniziale dei diametri massimi nel periodo peri - procedurale , con un aumento del diametro massimo di 0 , 67 c ai successivi controlli si notato una persistente riduzione del diametro dellarea ablata , conforme al consolidamento del 970 radiol med ( 2010 ) 115 : 962974 fig . 
mwa is a relatively new technique that can be applied to different types of tumours and offers all the benefits of rfa as well as some substantial advantages . these include a larger volume of cellular necrosis , reduction in procedure times , greater temperatures delivered to the target lesion , the possibility of using multiple antennae simultaneously , efficacy on lesions with a cystic component and / or in proximity to vascular structures > 3 mm in diameter with a reduction in the heat - sink effect , and less intraprocedural pain [ 5 , 6 , 1221 ]  . 
in rfa , direct tissue heating is confined to an area of only a few millimetres surrounding the active electrode , whereas heating of the remaining target zone takes place through simple thermal conduction [ 3 , 5 , 6 , 17 , 21 , 26 ]  . 
in contrast , microwaves induce oscillation of water molecules at a speed between 2 and 5 billion times per second , depending on the frequency of the microwaves themselves , thus producing a better convection profile and causing more uniform coagulation and necrosis of the target [ 5 , 6 , 15 , 16 , 21 ]  . 
as microwaves generate an electromagnetic wave electrically independent of the antenna , they do not seem to be subject to an increase in impedance , thanks to the nature of the waves themselves [ 2 , 5 , 6 , 21 , 27 , 28 ]  . 
la paziente stata quindi sottoposta ad ulteriore trattamento ablativo con microonde a 3 dal primo , determinando la completa necrosi della recidiva valutata mediante tc a pochi giorni dalla procedura . 
la durata media del follow - up stata di 3 , 6 mesi ( range 19 mesi ) , registrando in tutti i pazienti il periodo a partire dalla data della procedura fino alla scansione tc pi recente . discussione nel corso degli anni sono state sviluppate diverse tecniche ablative per il controllo locale di neoplasie inoperabili : ablazione con etanolo , laserablazione , crioablazione e termoablazione mediante radiofrequenze [ 3 , 4 ]  . 
le mw sono un trattameno ablativo relativamente nuovo applicabile a differenti tipologie di neoplasie , in grado di offrire tutti i benefici della radiofrequenza , presentando inoltre radiol med ( 2010 ) 115 : 962974 fig . 
c tc a 3 mesi dal secondo trattamento con mw : completa ablazione della lesione ( freccia )  . up to 6 cm and therefore exceeding the dimensional limitations of rfa [ 5 , 6 , 14 , 21 ]  . 
a comparison of the findings of our study with those reported in the literature with regard to rfa shows that the mean necrosis diameter obtained with microwaves is greater ( mean diameter 3.5 cm ) than with rfa ( 1.7 cm ) [ 3 , 29 ]  . 
 [ 20 , 21 ] shows that mean diameter and mean transverse area of necrosis are greater with mwa than with rfa : mean diameter by 25% and mean transverse area by 50% ( table 4 )  . sostanziali vantaggi , quali : volumi di necrosi cellulare pi ampi , riduzione del tempo di procedura , maggiori temperature alla lesione target , possibilit di utilizzare multiple antenne simultaneamente , efficacia su lesioni con componente cistica e / o in prossimit di strutture vascolari > 3 mm di diametro con riduzione dellheat sink effect , minore dolore intraprocedurale [ 5 , 6 , 1221 ]  . 
nelle ablazioni con radiofrequenze lattivit diretta di surriscaldamento dei tessuti limitata ad una zona che circonda lelettrodo attivo per soli pochi millimetri , mentre laumento della temperatura nella restante zona target avviene attraverso semplice conduzione termica [ 3 , 5 , 6 , 17 , 21 , 32 ]  . 
le microonde invece , inducendo loscillazione delle molecole dacqua con movimenti di rotazione su se stesse ad una velocit di 25 miliardi di volte al secondo dipendente dalla frequenza delle onde stesse , permettono di ottenere un migliore profilo convettivo , determinando una necrosi coagulativa al target pi uniforme [ 5 , 6 , 15 , 16 , 21 ]  . 
le ablazioni con radiofrequenze sono inoltre limitate dallincremento dellimpedenza con ebollizione e carbonizzazione del tessuto , a causa dellevaporazione delle molecole dacqua che funge da isolante elettrico , le microonde , generando unonda elettromagnetica elettricamente indipendente dallantenna , non sembrano inceve essere soggette ad aumento di impedenza , grazie alla natura stessa delle onde [ 3 , 5 , 6 , 21 , 33 , 34 ]  . 
il sistema ablativo mediante microonde consente il posizionamento simultaneo di multiple antenne , ognuna connessa al proprio generatore , al fine di ottenere aree di necrosi fino a 6 cm , superando quindi i limiti dimensionali della rfa [ 5 , 6 , 14 , 21 ]  . 
comparando i dati riscontrati in questo studio con i dati presenti in letteratura in merito alla rfa si nota come il diametro medio di necrosi ottenuto mediante limpiego delle microonde maggiore ( diametro medio 3 , 5 cm ) rispetto al diametro medio post - rfa ( diametro medio 1 , 7 cm ) [ 3 , 26 ]  . 
 [ 20 , 21 ] si nota come il diametro medio e larea trasversale media di necrosi presentino maggiori dimensioni con microonde rispetto alla radiofrequenza : diametro medio maggiore del 25% ed area trasversale media maggiore del 50% con le microonde rispetto alla radiofrequenza ( tabella 4 ) [ 20 ]  . 
lo sviluppo di linfoadenopatia non significativamente correlata al table 4 studies reporting microwave ablation ( mwa ) therapy of lung tumours radiol med ( 2010 ) 115 : 962974 clinical studies author ( year ) no . 
 [ 12 ] 50 / 66 percutaneous 14.5 - gauge straight antenna at 1 year : local control 67% mortality at 30 days : 0% technical success : 95% local complications : 9.1% pneumothorax : 39% haemoptysis : 6.6% skin burns : 36% experimental studies author ( year ) approach ablation results no . 
 [ 20 ] 3 swine / 18 ablations percutaneous 17 - gauge triaxial ( 9 mwa + 9 rfa ) transverse diameter of necrosis 50% larger and necrosis volume 133% greater than with rfa antenna + 17 - gauge single straight antenna ( mwa ) + 17 - gauge electrode ( rfa ) mwa , microwave ablation ; rfa , radiofrequency ablation tabella 4 letteratura sulle microonde nel trattamento del polmone studi clinici autore ( anno ) numero pazienti / numero ablazioni wolf et al . 
 [ 12 ] 50 / 66 percutaneo 14 , 5 g antenna dritta approccio ablazione risultati follow - up mortalit a 30 giorni : 0% successo tecnico : 95% complicanze locali : 9 , 1% pneumotorace : 39% emottisi : 6 , 6% ustioni : 36% ad 1 anno : controllo locale 67% studi sperimentali autore numero pazienti / numero ablazioni 8 maiali / 24 ablazioni durick et al . 
 [ 20 ] 3 maiali / 18 ablazioni percutaneo ( 9 mwa + 9 rfa ) mwa , ablazione con microonde ; rfa , ablazione con radiofrequenza triassiale + 17 g antenna singola diritta 17 g antenna triassiale ( mwa ) + 17 g elettrodo ( rfa ) diametri di necrosi coagulativa ottenuti con antenna triassiale di maggiori dimensioni rispetto ai diametri ottenuti con singola antenna diametri trasversali di necrosi maggiori del 50% , con un volume di necrosi maggiore del 133% rispetto alla rfa radiol med ( 2010 ) 115 : 962974 lesion dimension had no influence on cancer - specific mortality and survival rates . 
the presence of cavitation is statistically correlated with the cancer - specific mortality rate ( p = 0.02 ) [ 12 ]  . lymphadenopathy was not significantly correlated with the cancer - specific and non - cancer - specific mortality rate . 
evaluation of the safety of microwaves shows that the 30 - day postmwa mortality rate ( 0% ) is markedly lower than both the post - rfa mortality rate ( 3.9% , 6 / 153 patients ) and postsurgical mortality rate ( 2.0% , 1 / 66 patients ) [ 3 , 31 ]  . 
 [ 33 ] was the mortality rate dependent on treatment : death ( 1 / 66 patients ) was caused by postoperative infectious complications . in our study , asymptomatic grade 1 pneumothorax occurred in 2 / 9 patients ( 22% )  . 
they reported no cases of skin burns induced by microwave - related thermal damage . each patient in our study was evaluated for the presence of postablation syndrome , a common and transitory post - rfa phenomenon consisting of flu - like symptoms ( fever , malaise , pain , myalgia , nausea and vomiting ) [ 14 ]  . 
intraprocedural pain during mwa was less than during rfa , most likely due to the absence of the passage of an electrical current through the patients body . in conclusion , our preliminary experience supports the studies available in the literature regarding mwa , which demonstrate that the technique is safe and effective and enables local control of solid lung masses in patients who are not candidates for surgical resection [ 6 , 12 , 21 ]  . tasso di mortalit cancro - specifica e non . 
valutando la sicurezza delle microonde si osserva come il tasso di mortalit a 30 giorni post - ablazione mw ( 0% ) nettamente inferiore rispetto al tasso di mortalit post - rfa ( 3 , 9% , 6 di 153 pazienti ) e post - chirurgia ( 2 , 0% , 1 di 66 pazienti ) [ 3 , 31 ]  . 
il tasso di mortalit risultato essere dipendente dal trattamento : la morte ( 1 su 66 pazienti ) stata causata da complicanze infettive post - resezione chirurgica [ 33 ]  . in questo studio si riscontrato pneumotorace in 2 / 9 pazienti ( 22% ) , di grado i / asintomatico . 
la sindrome post - ablazione un fenomeno transitorio e comune post - rfa associato a ( febbre , malessere , sintomatologia simil - influenzale dolore , mialgia , nausea e vomito ) [ 14 ]  . 
the purpose of this paper is to review the impact of ct on the management of renal trauma , stressing the importance of this technique and the role of the radiologist in the timing of decisions . finally , we discuss the diagnostic approach to the followup of renal trauma . riassunto i traumi renali rientrano nel complesso e vasto capitolo dei traumi retroperitoneali . 
nonostante la semeiotica in tomografia computerizzata ( tc ) del trauma sia nota da tempo , ancora oggi si discute sui tempi , lapproccio diagnostico e le modalit di gestione . 
infine verr discusso lapproccio diagnostico nel follow - up dei traumi renali . keyword renal injuries ct management parole chiave traumi renali tc gestione introduction introduzione renal injuries may be included in the broad and complex subject of retroperitoneal traumas , in which at least one kidney is involved in 10% of cases [ 13 ]  . 
the mean age of patients is between 20 and 30 years [ 2 , 4 ] , such that renal injury may be substantially regarded as occurring in young adults . 
although data from the united states estimate the average number of renal injuries to be approximately 245 , 000 per year worldwide , no detailed or reliable epidemiological evaluation of such events in fact appears possible [ 4 ]  . 
the low incidence of major renal i traumi renali rientrano nel complesso e vasto capitolo dei traumi retroperitoneali , nei quali in circa il 10% interessato almeno un rene [ 13 ]  . 
dal punto di vista epidemiologico , bench negli stati uniti alcuni dati stimino in circa 245000 per anno la media dei traumi renali nel mondo , una dettagliata ed attendibile valutazione epidemiologica di tali eventi risulta , di fatto , impossibile [ 4 ]  . 
la bassa incidenza di traumi renali maggiori si spiega con la favorevole radiol med ( 2010 ) 115 : 936949 injuries is explained by the favourable position of the kidneys , which are the retroperitoneum , surrounded by fat tissue ( gerotas fat ) and protected posteriorly by the psoas and quadratus lumborum muscles and , in part , by the ribs . located a fundamental step in diagnosing renal trauma is to define the mechanism by which the injury was produced . on the basis of the mechanism , renal traumas are divided into direct blunt , penetrating ( gunshot or stab wounds ) , iatrogenic ( renal biopsies , interventional procedures such as percutaneous nephrostomy or renal artery angioplasty ) and intraoperative injuries [ 6 , 7 ]  . 
between 80% and 97% of renal injuries [ 2 , 4 , 7 ] are caused by blunt trauma to the back , flank or lower chest or by sudden rapid accelerationdeceleration events [ 79 ] in urban settings , most commonly due to motor vehicle accidents , falls , fights or sports activities . 
whereas the majority of blunt traumas produce lowgrade renal injury [ 6 ] , penetrating traumas , which account for 10% of all cases [ 7 ] , cause major renal injuries and frequently require invasive treatment , as they are more likely to be associated with haemodynamic instability due to either damage to major renal vessels ( 15%33% ) [ 3 ] or involvement of other abdominal organs ( around 80% of cases ) [ 2 , 4 , 79 ]  . 
finally , the incidence of renal injuries increases in the event of pre - existing congenital or acquired renal pathology , such as horse - shoe kidney , renal cysts , hydronephrosis or tumour . clinical features haematuria is the most common presenting sign of traumatic renal injury and is seen in approximately 95% of patients . 
haematuria may , however , be absent in around 10%25% of high - grade renal injuries [ 2 , 7 ] and in 24%50% of injuries to the ureteropelvic junction and renal vascular pedicle [ 2 , 3 , 7 , 8 ]  . 
reported the absence of gross or microscopic haematuria in injuries to the renal vascular pedicle [ 10 ] , and in 1989 , pollack and wein stated that it might be imprudent to withhold renal imaging from blunt trauma victims based on whether there is evidence of haematuria [ 8 ]  . 
finally , the poor correlation between the presence of haematuria and the severity of anatomical damage emphasises the importance of diagnostic imaging for evaluating and managing renal trauma . localizzazione topografica di tali organi : infatti , essi sono localizzati nel retroperitoneo , circondati da tessuto adiposo ( grasso di gerota ) e protetti posteriormente dai muscoli psoas , quadrato dei lombi e , in parte , dalle coste . indispensabile nei casi di trauma renale definire il meccanismo con cui esso si sia verificato . 
in base al meccanismo di azione i traumi del rene si possono suddividere in chiusi diretti , penetranti ( ferite da arma da fuoco o da taglio ) , iatrogeni ( biopsie renali , procedure interventistiche come nefrostomie percutanee o angioplastiche dellarteria renale ) ed intraoperatori [ 6 , 7 ]  . 
in una percentuale compresa tra l80% e il 97% dei casi [ 2 , 4 , 7 ] la patologia traumatica renale determinata dal cosiddetto trauma chiuso , diretto al dorso , al fianco , alla parte inferiore del torace o ad improvvisa e brusca accelerazione - decelerazione [ 79 ] , come accade frequentemente nelle nostre realt metropolitane , in scontri automobilistici e motociclistici , nelle cadute , nelle colluttazioni o nelle attivit sportive . 
se la maggior parte dei traumi diretti determina un trauma renale di basso grado [ 6 ] , i traumi penetranti , che risultano essere pari al 10% di tutti i traumi renali [ 7 ] , sono responsabili di danni renali maggiori e pi spesso richiedono un trattamento invasivo in quanto maggiormente associati ad instabilit emodinamica o per lesioni traumatiche dei vasi renali maggiori ( tra il 15% e il 33% ) [ 3 ] o per coinvolgimento di altri organi addominali , come avviene in una percentuale stimata intorno all80% [ 2 , 4 , 79 ]  . 
infine , lincidenza di traumi renali aumenta in caso di patologie renali preesistenti congenite o acquisite , come per esempio la presenza di un rene a ferro di cavallo , di cisti renali , idronefrosi o la presenza di un tumore . aspetti clinici lematuria rappresenta il segno pi indicativo in caso di trauma renale ed presente in circa il 95% dei pazienti . 
in circa il 10%25% dei traumi renali di grado elevato , tuttavia , lematuria pu essere assente [ 2 , 7 ] e una percentuale compresa tra il 24% e il 50% dei traumi della giunzione pieloureterale e del peduncolo vascolare renale si presenta , di fatto , con assenza di ematuria [ 2 , 3 , 7 , 8 ]  . 
gi nel 1976 , infatti , stables et al . [ 10 ] riscontrano assenza di macroe microematuria in lesioni del peduncolo vascolare renale e , nel 1989 , pollack e wein [ 8 ] affermano che sarebbe imprudente negare una valutazione strumentale alle vittime di un trauma chiuso con evidenza di ematuria . 
infine , in considerazione della scarsa correlazione tra la presenza di ematuria e la gravit del danno anatomico , risulta evidente limportanza che riveste la diagnostica per immagini nella valutazione del trauma renale e del suo management . imaging several published papers recommend that diagnostic imaging be performed in patients with penetrating trauma imaging alcuni lavori presenti in letteratura suggeriscono la 938 radiol med ( 2010 ) 115 : 936949 and haematuria , with blunt trauma associated with gross haematuria , with microscopic haematuria and hypotension ( arterial pressure < 90 mmhg ) , with microscopic haematuria associated with other traumatic injuries or after blunt trauma with associated injuries potentially causing renal damage ( contusion or haematoma to the flank soft tissues , fractures of the lower ribs , vertebral transverse processes or thoracic - lumbar spine ) [ 2 , 5 , 9 , 1013 ]  . 
recommended diagnostic imaging in patients with gross or microscopic haematuria associated with shock , a clinical suspicion of multiorgan involvement or in patients sustaining rapid deceleration injuries [ 7 ]  . 
there is , however , general agreement that imaging should be reserved for haemodynamically stable [ 8 ] or semiunstable trauma patients , whereas unstable patients should proceed directly to exploratory surgery . 
in all cases , the aim of imaging in renal trauma is to address a series of questions that are fundamental for planning patient management : detecting and accurately staging renal injuries seeking out first any life - threatening injuries ( vascular lesions ) , documenting the function of the contralateral kidney , demonstrating pre - existing pathology of the injured kidney and identifying associated thoracoabdominal lesions . 
 the imaging modality of choice for evaluating polytrauma patients with suspected renal injury is contrastenhanced computed tomography ( ct ) , whether the patient is clinically stable [ 9 ] or semiunstable . 
the value of ct for demonstrating the pathology and extent of injury in polytrauma patients was first highlighted in the late 1970s [ 14 ]  . in 1980 , mitty reported that ct was more sensitive than intravenous urography ( ivu ) in detecting urinary extravasation [ 15 ]  . 
it is since the mid - 1980s , however , [ 6 , 7 , 1619 ] that ct has definitively become the primary imaging modality in abdominal trauma and particularly in suspected renal injury , replacing ivu [ 1 , 6 ] , which is less sensitive and specific than ct [ 20 ] , and restricting the use of ultrasound ( us ) to patients considered affected by minor renal trauma in view of its high negative predictive value ( npv ) [ 21 ]  . 
also , the diagnostic role of renal angiography has been reconsidered over the years , above all in consideration of the technological evolution of ct scanners with the advent of the spiral technique and development of multidetector scanners with 16 or 64 detector rows [ 1 , 2 , 4 , 7 , 8 , 2224 ]  . despite its potential and theoretical applications in specific settings , magnetic resonance ( mr ) imaging has limited use in the initial evaluation of renal trauma . 
mr imaging cannot be used in the acute assessment of polytrauma because , beyond motion artefacts and markedly longer acquisition times than modern ct scanners [ 4 , 7 ] , it fails to provide all the answers required in a trauma setting and is therefore not valutazione radiologica nei pazienti con trauma penetrante ed ematuria , con trauma diretto associato ad ematuria macroscopica , microematuria ed ipotensione ( pressione arteriosa < 90 mmhg ) , microematuria in associazione ad altre lesioni traumatiche o dopo trauma diretto con lesioni associate potenzialmente responsabili di danno renale ( contusione od ematoma ai tessuti molli del fianco , fratture delle coste inferiori , dei processi trasversi vertebrali o del rachide dorso - lombare ) [ 2 , 5 , 9 , 1013 ]  . 
altri autori , invece , riassumono le indicazioni allimaging nei casi in cui sia presente genericamente ematuria o ci si trovi di fronte ad un trauma posteriore o in caso di traumi da decelerazione . 
 [ 7 ] suggeriscono la valutazione radiologica nei pazienti con macroematuria o microematuria con shock , sospetto clinico di interessamento multiorgano o in pazienti con trauma da rapida decelerazione [ 7 ]  . 
c comune accordo , comunque , che la valutazione strumentale sia riservata al paziente traumatizzato emodinamicamente stabile [ 8 ] o semi - instabile , laddove in caso di instabilit si procede direttamente alla esplorazione chirurgica . 
in ogni caso la diagnostica per immagini nel trauma renale deve rispondere ad una serie di domande che risultano indispensabili per il successivo planning gestionale quali : identificare e stadiare accuratamente le lesioni renali evidenziando , in primis , quelle che mettono in pericolo la vita del paziente ( le lesioni vascolari ) , documentare la funzionalit del rene controlaterale , mostrare patologie pre - esistenti a carico del rene lesionato , identificare lesioni toraco - addominali associate . 
 attualmente , la metodica di scelta nella valutazione dei pazienti politraumatizzati e con sospetto trauma renale la tomografia computerizzata ( tc ) con somministrazione endovenosa di mezzo di contrasto ( mdc ) , sia in caso di stabilit [ 9 ] che in situazioni di semi - instabilit emodinamica . 
ma dalla seconda met degli anni 80 [ 6 , 7 , 1619 ] che il ruolo della tc nei pazienti con trauma addominale ed in particolare con sospetto di trauma renale stato definitivamente sancito , rendendo marginale [ 1 , 6 ] il ruolo della ue , meno sensibile e specifica della tc [ 20 ] , e limitando quello dellecografia ( us ) ai pazienti considerati affetti da un trauma renale minore , per il suo alto valore predittivo negativo [ 21 ] ; anche il ruolo diagnostico dellangiografia renale si , nel corso degli anni ridimensionato , soprattutto in considerazione dellevoluzione tecnologica che hanno subito le apparecchiature tc sia con lavvento della tecnica spirale che con il successivo sviluppo delle macchine multidetettore a 16 o a 64 canali [ 1 , 2 , 4 , 7 , 8 , 2224 ]  . 
viceversa , la rm non pu essere utilizzata nella valutazione acuta del politrauma , perch , aldil degli artefatti da movimento e dei tempi di acquisizione decisamente pi lunghi radiol med ( 2010 ) 115 : 936949 effective in terms of guiding patient management . 
mr imaging does , on the other hand , play a role along with colour doppler us ( cdus ) and / or contrast - enhanced us ( ceus ) in the follow - up of patients with renal trauma , as will be described below . a correct ct acquisition technique is important for optimal evaluation of the entire urinary system , which is composed of vascular structures and a collecting system as well as a parenchymal portion . 
thus , the ct protocol for suspected renal trauma includes an initial arterial phase with a scanning delay of 2030 s to identify vascular damage , followed by a nephrographic phase at 7080 s to identify parenchymal lesions and a possible late phase at 320 min to detect lesions to the urinary tract [ 25 ]  . 
this multiphasic study protocol , based on the whole - body ct for trauma technique [ 26 ] , should be preceded by an unenhanced , thick - section scan . 
bolus tracking is preferred to the manual technique for timing of the arterial phase , as haemodynamic status may vary significantly among patients [ 9 ]  . the most appropriate a correct ct study allows for optimal staging of renal injuries with identification of type , location and extent of parenchymal damage , detection of nonviable devascularised parenchymal fragments and the size and site of retroperitoneal haematoma , evaluation of the integrity of the vascular pedicle and of active bleeding or urinary extravasation and it reveals the existence of underlying renal pathology or abnormalities [ 5 , 8 ] , directing the physician towards determining treatment strategy . 
in addition , ct enables evaluation of contralateral kidney function and detection of concomitant involvement of other abdominal organs [ 7 ] , thereby helping to identify priorities in patient management . 
the wide availability of ct scanners , the possibility of acquiring large volumes in short scan times with consequently fewer motion artefacts , the high spatial resolution guaranteeing accurate anatomical detail and the panoramic capabilities resulting in part from multiplanar and three - dimensional image reconstruction [ 1 , 9 ] , make ct the first - line imaging modality in patients with suspected renal injury and a robust decision - making tool for selecting the most appropriate treatment . classification of renal injuries not all renal injuries have equal clinical significance , and different lesions thus require different treatment rispetto alle moderne apparecchiature tc [ 4 , 7 ] , non risponde completamente a tutti i quesiti diagnostici che la malattia - trauma pone in discussione e , pertanto , non risulta efficace in termini di gestione . 
diverso , invece , il ruolo che la rm e gli lus , con lapplicazione del color doppler ( ecd ) e / o lutilizzo del mdc ( ce - us ) , svolgono nellambito del follow - up dei pazienti con trauma renale , come riportato in seguito . 
 le modalit di esecuzione dellesame tc sono importanti per una valutazione ottimale dellintero apparato urinario , composto oltre che da una porzione parenchimale anche da strutture vascolari e dal sistema collettore . 
pertanto , il protocollo tc per sospetto trauma renale prevede inizialmente una fase arteriosa con ritardo di acquisizione compreso tra 20 s e 30 s per lidentificazione del danno vascolare , seguita da una fase nefrografica tra 70 s e 80 s per lidentificazione delle lesioni parenchimali e completato eventualmente da una valutazione tardiva tra 3 e 20 minuti per il riconoscimento dei danni delle vie urinarie [ 25 ]  . 
a tale protocollo di studio multifasico , che si rif alla tecnica whole body ct for trauma [ 26 ] , utile far precedere una fase di studio senza mdc endovena ( ev ) , con ampio spessore di strato . 
lo spessore di strato prevede collimazioni sottili ( 0 , 53 mm ) per la valutazione dei vasi e delle vie escretrici mentre il parenchima renale sufficientemente valutabile anche a spessori compresi tra 3 mm e 5 m la quantit di mdc deve essere compresa tra i 100 ml e i 130 ml ad una velocit di flusso di 35 ml / s . 
per la fase arteriosa la tecnica con bolus tracking preferibile a quella manuale in quanto la condizione emodinamica pu variare in maniera significativa da paziente a paziente [ 9 ]  . un esame tc condotto correttamente consente di stadiare le lesioni renali , identificando il tipo , la localizzazione e lestensione del danno parenchimale , di individuare i frammenti parenchimali devascolarizzati non vitali , la quantit e la sede dellematoma retroperitoneale , valutando lintegrit del peduncolo vascolare , la presenza di sanguinamenti attivi o di stravasi urinari , e permette di rivelare lesistenza di patologie o anomalie renali preesistenti [ 5 , 8 ] , indirizzando il paziente verso il pi opportuno e sollecito programma terapeutico . 
inoltre , e non ultimo , la tc consente di valutare la funzione del rene controlaterale e di identificare leventuale contemporaneo interessamento di altri organi addominali [ 7 ] , mettendo a fuoco quali siano le priorit gestionali del caso . 
la larga disponibilit di apparecchiature sul territorio , la possibilit di acquisire grandi volumi in breve tempo con conseguente sensibile riduzione degli artefatti da movimento , lelevata risoluzione spaziale che garantisce un accurato dettaglio anatomico , e la panoramicit anche grazie alla possibilit di ricostruire le immagini secondo riformattazioni multiplanari e tridimensionali [ 1 , 9 ] rendono la tc indagine di primo livello nei pazienti con sospetto trauma del rene , ed un robusto strumento decisionale per il conseguente tipo di trattamento da adottare . 940 radiol med ( 2010 ) 115 : 936949 approaches . 
after the first classification formulated by kster in 1896 , many others have been proposed or modified , with none of them , however , gaining general acceptance [ 27 ]  . 
 [ 28 ] developed for the american association for the surgery of trauma ( aast ) organ injury scale ( ois ) , which provided and still provides an accurate description of major renal injuries [ 4 ]  . 
grade i injuries are the most common , accounting for around 80% of renal injuries , and include : normal imaging associated with haematuria ; contusions , mostly ill - defined areas with reduced contrast enhancement and excretion , at times ill - defined and spontaneously hyperattenuating on unenhanced ct images , due to haemorrhage ; stable subcapsular haematomas , which appear on unenhanced ct images as spontaneously hyperattenuating collections , with biconvex shape , located between an intact renal capsule and opacified parenchyma [ 9 , 13 ]  . 
grade ii and grade iii renal injuries include : lacerations , appearing as linear or wedge - shaped opacification defects that are particularly evident in the nephrographic phase , are associated with ill - defined capsular profile , and may have a depth < 1 cm ( grade ii ) or > 1 cm ( grade iii ) without involvement of the collecting system ; in most cases , there is associated perirenal haematoma , a hyperattenuating fluid collection in the gerota fat [ 7 ]  . 
a topographical criterion for ct recognition of injury to the calyceal system is the detection on delayed postcontrast ct images of urinary extravasion in the posterolateral perirenal space , in contrast to what happens in injuries to the renal pelvis , ureteropelvic junction or ureters , in which the urine typically collects medially [ 7 , 8 , 29 , 30 ] , at times along the course of the ureter . 
 [ 28 ] also included segmental infarctions among grade iv injuries ; these are caused by thrombosis , dissection or laceration of segmental arteries and appear as nonperfused wedgeshaped areas with apex facing the renal hilum and base facing the capsule , the profile of which appears sharp , regular and well delimited [ 7 , 9 , 13 ]  . 
grade v renal injuries are characterised by shattering of the renal parenchyma , rupture of the kidney into three or more separate fragments , thrombosis or dissection of the renal artery or vein , which are more commonly found in deceleration traumas with avulsion of the vascular pedicle [ 7 ] ; rupture or thrombosis of the renal vein is a rare , albeit recognised , occurrence [ 31 ]  . 
the absence of the nephrographic effect and retroperitoneal haematoma , especially in medial location , should raise the presence of an extensive classificazione dei traumi renali non tutti i traumi renali sono ugualmente significativi dal punto di vista clinico e pertanto richiedono modalit di trattamento differenti . 
dopo la prima classificazione formulata da kster nel 1896 , molte altre sono state proposte o modificate senza che nessuna di esse venisse generalmente riconosciuta e adottata [ 27 ]  . 
 [ 28 ] una classificazione di danno dorgano , lorgan - injury severity scale ( ois ) , che permetteva e permette tuttora , unaccurata descrizione dei maggiori traumi renali [ 4 ]  . 
dei traumi di grado i fanno parte i traumi pi comuni , approssimativamente l80% dei traumi renali ed include : reperti radiologici di negativit associati ad ematuria ; contusioni , aree nella maggior parte dei casi mal definite , con ridotto enhancement post - contrastografico e ridotta escrezione di urina iodata , talvolta sfumate e spontaneamente iperdense nellesame pre - contrastografico per la presenza di emorragia ; ematomi subcapsulari stabili , ovvero raccolte spontaneamente iperdense allesame diretto , a morfologia biconvessa , tra capsula renale integra e parenchima opacizzato [ 9 , 13 ]  . dei traumi renali di grado ii e iii fanno parte : lacerazioni , cio difetti di opacizzazione particolarmente evidenti nella fase nefrografica , lineari o cuneiformi , associati a profilo capsulare mal definito e che presentano profondit < 1 cm ( grado ii ) o > 1 cm ( grado iii ) che non determinano rottura del sistema collettore ; nella maggior parte dei casi si associa un ematoma perirenale , ovvero una raccolta fluida ad elevata densit nel grasso di gerota [ 7 ]  . 
criterio topografico di riconoscimento alla tc di un trauma del sistema caliceale lidentificazione , nelle fasi tardive di studio postcontrastografico , di stravaso di urina iodata nello spazio perirenale postero - laterale , a differenza di quello che succede nei traumi della pelvi , della giunzione pielo - ureterale o propriamente ureterali in cui lurina iodata si raccoglie , classicamente , in sede mediale [ 7 , 8 , 29 , 30 ] , talora distribuendosi lungo il decorso dello stesso uretere . 
 [ 28 ] riportano come traumi di grado iv anche gli infarti segmentari , aree non perfuse cuneiformi con apice allilo e base rivolta verso la capsula renale il cui profilo appare netto regolare e ben delineato , causati da trombosi , dissezione o lacerazioni di arterie segmentarie [ 7 , 9 , 13 ]  . 
i traumi renali di grado v sono caratterizzati dallo spappolamento del parenchima renale , frattura del rene in tre o pi frammenti separati , devascolarizzazione del rene per rottura , trombosi o dissezione dellarteria o della vena renale , pi frequentemente riscontrabili nei traumi decelerativi in cui si verifica lo stiramento del peduncolo vascolare [ 7 ] ; la rottura o la trombosi della vena renale un evento raro , ma descritto in letteratura [ 31 ]  . 
lassenza delleffetto nefrografico e la presenza di un ampio ematoma radiol med ( 2010 ) 115 : 936949 suspicion of injury to the vascular pedicle ; a typical finding in devascularisation , but more in general in arterial infarctions , is the so - called rim sign , which is due to opacification of the capsule and subcapsular parenchyma by intact collateral capsular vessels [ 7 , 22 ]  . 
traumatic occlusion of the renal vein presents with swelling of the kidney with consequent reduction of nephrographic effect and diminished or absent excretion of iodinated urine [ 7 ]  . in 1989 , federle proposed a ct - based classification [ 17 ] that subdivided renal injuries into three broad categories : minor , major and catastrophic . 
the classification considers some important traumatic injuries not explicitly mentioned in the ois and that have , however , a strong impact on management : avulsion of the ureteropelvic junction ( considered as grade iv and currently defined by ois as grade v ) , injuries to the segmental renal arteries and active bleeding [ 1 ] , which is a crucial sign for patient management , as described below . 
special attention should be paid to the distinction between complete lacerations of the ureteropelvic junction , a possible indication for surgical repair , and partial lacerations : ureteral opacification is absent in the former , whereas in the latter , the lumen of the ureter distal to the lesion is partially opacified [ 7 , 32 ]  . the most widespread and generally recognised classification is the anatomical - surgical classification proposed by the aast , which is supported by numerous studies that have validated its effectiveness in predicting the morbidity and mortality of blunt and penetrating renal traumas [ 33 , 34 ] and which consider it a powerful and valuable tool for predicting the clinical outcome of patients with renal trauma [ 35 ]  . 
moreover , an additional factor to be considered is the presence of pathological conditions , such as urinoma , perirenal abscess , posttraumatic bleeding , pseudoaneurysm and arteriovenous fistula , which represent the main early and delayed complications of renal trauma and which the radiologist must recognise and differentiate to be able to indicate the most appropriate treatment . 
even though urinary extravasation associated with deep lacerations resolves spontaneously in the vast majority of cases [ 36 ] , 1%7% of cases may produce asymptomatic urine collections , more frequently in subcapsular location or within the gerota fascia in the perirenal space [ 37 ] , whereas urine in the peritoneal cavity is usually the result of penetrating or iatrogenic traumas . at unenhanced ct , urinomas appear as hypoattenuating fluid collections ; however , in delayed scans obtained 520 min after contrast injection , the iodinated urine typically increases their attenuation . 
posttraumatic active bleeding develops at a mean interval of approximately 12 days after trauma [ 38 ] , though delayed onset at 36 days retroperitoneale , specie se in sede mediale , deve far sospettare un trauma del peduncolo ; caratteristico della devascolarizzazione , ma pi in generale degli infarti arteriosi , il cosiddetto segno dellorletto , dovuto alla opacizzazione della capsula e dal parenchima sottocapsulare da parte di vasi capsulari collaterali integri [ 7 , 22 ]  . 
locclusione traumatica della vena renale si presenta con un rigonfiamento del rene con conseguente riduzione delleffetto nefrografico e ridotta o assente escrezione di urina iodata [ 7 ]  . nello stesso anno 1989 , federle propone una classificazione basata sui reperti tc [ 17 ] , suddividendo i traumi renali in tre grandi categorie : traumi minori , maggiori e catastrofici . 
essa prende in considerazione alcune importanti lesioni traumatiche non esplicitamente specificate nella ois e che hanno , tuttavia , un grosso impatto sulle scelte gestionali quali : avulsione della giunzione pieloureterale ( considerata come trauma di categoria iv e attualmente identificata dallois come trauma di grado v ) , lesioni delle arterie renali segmentarie ed il sanguinamento attivo [ 1 ] che un segno cruciale nella gestione del paziente , come verr riportato in seguito . 
particolare attenzione va fatta nel riconoscere le lacerazioni complete della giunzione pielo - ureterale , che rappresentano una possibile indicazione alla riparazione chirurgica , da quelle parziali : nel primo caso lopacizzazione delluretere assente , nel secondo , invece , il lume delluretere distale alla lesione risulta parzialmente opacizzato [ 7 , 32 ]  . attualmente la classificazione pi diffusa e generalmente riconosciuta risulta essere quella anatomo - chirurgica proposta dalla aast , supportata , peraltro , da numerosi studi che validano la sua efficacia nel predire morbilit e mortalit dei traumi diretti e penetranti renali [ 33 , 34 ] e che la considerano un potente e valido strumento per prevedere loutcome clinico dei pazienti con trauma renale [ 35 ]  . da tener presente , inoltre , lesistenza di alcune condizioni patologiche come gli urinomi , gli ascessi perirenali , il sanguinamento post - traumatico , gli pseudoaneurismi e le fistole arterovenose che rappresentano le principali complicanze di un trauma renale , ad insorgenza precoce o tardiva , che il radiologo deve riconoscere e saper differenziare , s da poter indicare , anche in questo caso , il trattamento pi idoneo . 
anche se lo stravaso di urina associato a lacerazioni profonde si risolve nella stragrande maggioranza dei casi spontaneamente [ 36 ] , dall1% al 7% dei casi pu dar luogo a raccolte urinose asintomatiche , maggiormente apprezzabili in sede sottocapsulare o confinate nello spazio perirenale contenute generalmente nella fascia di gerota [ 37 ] , laddove lurina nel cavo peritoneale pi frequentemente conseguenza di traumi penetranti o iatrogeni . 
allesame tc diretto , gli urinomi si presentano come raccolte fluide a bassa densit ; tuttavia , caratteristicamente , nelle scansioni tardive eseguite tra i 5 min e i 20 min dopo la somministrazione del mdc , esse aumentano il proprio valore densitometrico in quanto rifornite da urina iodata . 
il sanguinamento attivo post - traumatico ha un intervallo medio di insorgenza di circa 12 giorni [ 38 ] con 942 radiol med ( 2010 ) 115 : 936949 has also been reported [ 39 ] and shows attenuation values between 80 and 370 hounsfield units ( hu ) [ 5 ]  . 
pseudoaneurysms are , instead , characterised by incomplete laceration of the arterial wall ; have rounded , circumscribed and relatively wellmarginated appearance ; and are isoattenuating relative to vessels in the different multiphase scans . 
both active bleeding and pseudoaneurysms are treated with arteriography and superselective embolisation , as are any arteriovenous fistulas that do not resolve spontaneously [ 40 ]  . riscontri tardivi anche a 36 giorni dal trauma [ 39 ] e presenta valori di attenuazione compresi tra 80 e 370 uh [ 5 ]  . 
esso si differenzia dagli pseudoaneurismi in quanto lineare , a morfologia filiforme e per definizione si rifornisce nelle successive acquisizioni essendo il vaso completamente lesionato ; diversamente , gli pseudoaneurismi si caratterizzano per incompleta lacerazione della parete arteriosa , presentano aspetto rotondeggiante , circoscritto e a margini pressocch regolari , e sono isodensi rispetto ai vasi nelle diverse acquisizioni multifasiche . 
as early as 1989 , pollack and wein stated that a clear dichotomy existed between urologists who preferred an aggressive surgical approach to major renal injuries and those who preferred an attendant conservative approach [ 8 ]  . 
today , the majority of renal injuries are treated conservatively [ 2 , 4 , 5 , 40 ] , and most of them , 75%85% of cases , fall into federles category i [ 2 ]  . 
intermediate - grade injuries ( grade iii and iv in the ois ) may also be treated conservatively in 76%87% of cases [ 4 , 5 , 36 , 41 , 42 ]  . 
also , knudson and maull advocate adopting a conservative approach , reporting a higher rate of nephrectomies in cases undergoing exploratory surgery compared with patients undergoing a conservative initial approach [ 42 ]  . 
the international literature considers uncontrolled life - threatening haemorrhage , avulsion of the renal pedicle and a pulsating and / or expanding retroperitoneal haematoma as absolute indications for immediate surgical exploration [ 4 , 5 , 22 ]  . 
relative indications for surgical exploration are [ 4 ] : ( 1 ) extensive laceration of the renal pelvis and / or transection of the ureteropelvic junction that cannot be treated with ureteropelvic stenting and persisting urinary leakage that cannot be controlled with nephrostomic treatment , ( 2 ) presence of devitalised parenchymal fragments removal of which could , according to some authors , reduce complication - related morbidity , such as delayed bleeding , urinomas and abscesses [ 43 ] , ( 3 ) thrombosis of one or both renal arteries if total or partial renal ischaemia time is < 3 h or 6 h , respectively [ 44 ] ; arteriography with stenting has a limited role in that it requires anticoagulation , which is not always possible in polytrauma patients . 
 however , despite the recent treatment advances , only 14%35% of patients with renovascular trauma can benefit from renal artery reconstruction with recovery of la gestione dei traumi renali stata ampiamente dibattuta nella letteratura . 
gi nel 1989 pollack e wein [ 8 ] affermano una chiara dicotomia esistente tra quegli urologi che , in maniera aggressiva , trattavano chirurgicamente i traumi renali maggiori , e quelli che invece preferiva adottare un trattamento attendistico - conservativo [ 8 ]  . 
oggi la maggior parte dei traumi renali trattato conservativamente [ 2 , 4 , 5 , 40 ] e rientra , tra il 75% e l85% dei casi , nella categoria i secondo federle [ 2 ]  . 
i traumi a severit intermedia ( grado 3 e 4 secondo lois ) possono essere trattati , allo stesso modo , conservativamente in una percentuale compresa tra il 76% e l87% [ 4 , 5 , 36 , 41 , 42 ]  . 
anche i dati presentati da knudson e maull [ 42 ] suggeriscono di mantenere la linea di condotta conservativa , riportando un tasso di nefrectomie pi alto nei casi in cui si procede ad esplorazione chirurgica rispetto ai casi in cui il trattamento iniziale di tipo conservativo [ 42 ]  . attualmente , la letteratura internazionale identifica come indicazioni assolute allimmediata esplorazione chirurgica la presenza di emorragia incontrollabile con imminente pericolo di vita , lavulsione del peduncolo renale e la presenza di un ematoma retroperitoneale pulsante e / o in espansione [ 4 , 5 , 22 ]  . 
 nonostante i progressi terapeutici degli ultimi anni , per , nei traumi renovascolari solamente il 14%35% dei pazienti si giova della ricostruzione dellarteria renale con conseguente ripristino della funzionalit renale [ 40 ]  . 
 [ 45 ] stated that conservative management may also have a role in grade v injuries , with nephrectomy being performed in only 22% cases of major vascular trauma , in some cases deferred to 21 days after injury . 
finally , it should also be noted that surgical repair of renal injuries may initially be avoided in favour of more recent and less invasive therapeutic procedures , such as embolisation during arteriography or percutaneous nephrostomy , and thus be used as the last resort these once ineffectiveness or unfeasibility of the lavoro del 2009 , eassa et al . 
 [ 45 ] , affermano che il management conservativo pu avere un ruolo anche nei traumi di grado v , ricorrendo in caso di trauma vascolare maggiore alla nefrectomia solo nel 22% dei casi , peraltro differita anche di 21 giorni . 
tutte le altre lesioni maggiori , dallo shattered kidney allavulsione della giunzione pielo - ureterale , non rappresentano , in senso stretto , indicazioni allapproccio chirurgico immediato , ma , viceversa , possono essere differibili . 
bisogna , infine , considerare anche che gli interventi di riparazione chirurgica delle lesioni renali possono essere inizialmente by - passati da quelle che sono le pi recenti procedure terapeutiche , meno invasive , quali lembolizzazione in corso di arteriografia o la nefrostomia percutanea , costituendo lextrema ratio una volta verificate linefficacia o limpossibilit di attuare tali fig . 
axial contrast - enhanced ct scans in the arterial phase ( a ) and portal phase ( b ) show shattered right kidney with multiple foci of active bleeding and a large perirenal haematoma . 
le scansioni assiali tc in fase arteriosa ( a ) e portale ( b ) mostrano rene destro spappolato , con multipli foci di stravaso attivo localizzati medialmente , anteriormente e posteriomente rispetto al parenchima renale danneggiato e vasto ematoma perirenale . 
il trattamento di tale lesione renale ( di grado v secondo lorgan injury scale dellaast ) prevede la rimozione chirurgica dellematoma e del rene , profondamente danneggiato e perci funzionalmente irrecuperabile . 
the first priority is to evaluate the trauma in its entirety and correct any life - threatening conditions . only then can one focus on preserving the injured organ by adopting all the necessary clinical and therapeutic measures . more specifically , preserving a kidney ( even if injured ) and avoiding surgery ( especially nephrectomy ! ) means first of all not performing laparotomy and not allowing the trauma to impact in all its complexity the surviving kidney . 
this significantly improves morbidity , mortality and outcomes in the shortand long - ter finally , because deceleration trauma typically occurs in the young , it should be recalled that even badly injured renal tissue may have an incredibly high capacity for anatomical - functional healing . 
this explains why , once severe haemorrhage and haemodynamic instability have been ruled out , conservative treatment is successful in 80% of patients with high - grade injuries [ 46 ] and why , whatever the type of injury , intervention should always be deferred as long as possible to allow the acute stage of trauma and organ injury to subside . 
nello specifico , salvaguardare un rene , anche danneggiato , evitando il trattamento chirurgico ( tanto pi la nefrectomia ) , significa , in primis , evitare che il paziente sia sottoposto ad una laparotomia e che la malattia trauma ricada , nella sua complessit , sullunico rene superstite , il che migliora sensibilmente la morbilit , la mortalit e la prognosi nel breve e nel lungo periodo . 
infine , non bisogna dimenticare che essendo il trauma decelerativo tipicamente una malattia del giovane , un tessuto renale , anche gravemente danneggiato , pu presentare una capacit di restitutio anatomofunzionale incredibilmente elevata . 
questo spiega come , una volta esclusa la condizione di una grave emorragia in atto e di instabilit emodinamica , il trattamento conservativo abbia successo nell80% dei pazienti con lesioni di alto grado [ 46 ] e che , qualunque sia la tipologia delle lesioni , lintervento debba essere , per quanto possibile , sempre differito , in modo che la malattia trauma superi la fase acuta e con essa anche lorgano lesionato . 
however , it should be considered that 3%33% of patients [ 7 ] have a risk of early ( 3672 h ) or late complications arising during the course of conservative management . 
primary imaging modalities in the follow - up are us ( cdus / ceus ) and mr imaging , which , although limited in emergency settings , are no doubt valuable for following the evolution of traumatic injuries confined to the kidney , in cases of minor trauma or when repeated se non vi sono dubbi sullimportanza del valore che la tc riveste nella stadiazione dei traumi renali in fase acuta , sugli obiettivi che limaging deve realizzare e sul decisivo ruolo che il radiologo assume nellindicare quale sia il trattamento pi opportuno da attuare , qualche linea dombra persiste sul follow - up di questi pazienti , che nella maggior parte dei casi vengono rivalutati nel corso del ricovero con controlli ripetuti , eseguiti esclusivamente per controllare nel tempo la normale evoluzione di una lesione traumatica . 
necessario innanzitutto considerare che in corso di management conservativo , vi sia la possibilit che in una percentuale di casi compresa tra il 3% e il 33% [ 7 ] , insorgano complicanze sia precoci ( 3672 ore ) che tardive . 
un ruolo di primo piano per il follow - up ricoperto dallus ( ecd\ce - us ) e dalla rm , il cui utilizzo , se risulta limitato in condizioni di urgenza , senza dubbio valido nel seguire levoluzione delle lesioni radiol med ( 2010 ) 115 : 936949 fig . 
2a - f a 35 - year - old man experiencing a high - energy deceleration injury ( road worker run over by a car on an highway )  . 
subdural haematoma with subfalcial herniation ( a ) , multiple fractures of the basicranium ( b , arrows ) , laceration of the spleen with haemoperitoneum ( c ) , mesenteric root avulsion ( d ) with active extravasation of contrast medium ( arrowheads ) , bilateral renal trauma with segmental infarction of the right kidney ( e ) and urinoma from partial laceration of the ureteropelvic junction ( f )  . 
ematoma subdurale con ernia subfalciale ( a ) , fratture multiple del basi cranio ( b , frecce ) , lacerazione del polo splenico superiore con emoperitoneo ( c ) , avulsione della radice del mesentere ( d ) con segni di stravaso ematico attivo ( teste di freccia ) , in presenza di trauma renale bilaterale con infarti segmentari nel rene di destra ( e ) e lesione parziale del giunto pieloureterale di sinistra con urinoma ( f )  . 
in questo caso , si dimostra il valore dellesame tc nella diagnosi e nelle scelte decisionali : in questo caso le lesioni renali non rappresentano la priorit gestionale , il primo problema da dover risolvere : difatti , le lesioni cerebrali e addominali sono state trattate immediatamente per via chirurgica mentre gli infarti segmentari renali sono strati trattati conservativamente e lurinoma con il posizionamento di uno stent pielo - ureterale . examinations are required in the course of a major injury [ 47 ]  . 
cdus , for example , is very useful for identifying posttraumatic pseudoaneurysms [ 48 ] or monitoring the evolution of urine collections . several different indications exist for the use of ct , not traumatiche confinate al rene , nei casi di traumi minori o quando , in corso di trauma maggiore , siano necessari controlli ripetuti nel tempo [ 47 ]  . 
un valido ausilio dallecd si ha , per esempio , nellindividuazione delleventuale formazione di pseudoaneurismi postraumatici [ 48 ] o 946 radiol med ( 2010 ) 115 : 936949 fig . 
absence of active blood extravasation , urinoma in the late excretory phase ( c ) and stability of the lesion during follow - up suggested conservative treatment of this renal injury ( grade iii according to the american association for the surgery of trauma organ injury scale )  . 
lassenza di stravaso ematico attivo , di urinoma in fase tardiva ( c ) e la stabilit della lesione nei controlli hanno consentito lattuazione del trattamento conservativo della lesione renale ( di grado iii secondo lorgan injury scale dellamerican association for the surgery of trauma )  . 
have proposed the following indications for ct follow - up of adults with blunt renal trauma : large retroperitoneal haematoma , large urinomas , major devascularised fragments , shattered kidney , possible interventional endovascular treatment or renal injury in a suspected pre - existing renal disease [ 22 ]  . 
in our opinion , ct should be used in the follow - up only in the event of deteriorating clinical and / or laboratory status , with the goal of promptly identifying any vascular or urinary complications or superinfections [ 25 ]  . 
finally , it should be recalled that an acute abdomen arising in a patient with a clinically stable renal injury may be not only a peritoneal per la valutazione dellevoluzione di raccolte urinose . diverso , ma non sempre condivisibile , appare il ricorso allutilizzo della tc . 
 [ 22 ] hanno proposto alcune indicazioni per il follow - up con tc nelladulto con trauma renale chiuso quali : vasto ematoma retroperitoneale , ampi urinomi , grandi frammenti devascolarizzati , rene spappolato , possibile trattamento endovascolare interventistico o danno renale su sospetta patologia preesistente [ 22 ]  . 
a nostro avviso , il follow - up con tc deve essere effettuato solo in caso di peggioramento della sintomatologia clinica e / o laboratoristica del paziente per la tempestiva identificazione di eventuali complicanze vascolari , urinose o da sovra - infezione [ 25 ]  . 
infine , non dimentichiamo , che un addome acuto radiol med ( 2010 ) 115 : 936949 reaction due to blood filtration / diffusion from the retroperitoneum into the peritoneal cavity but also a delayed manifestation of a traumatic bowel injury , which may have subtle or absent clinical signs at presentation and is associated with a mortality rate of 65% if diagnosed late [ 23 ]  . 
 follow - up imaging therefore involves us ( cdus / ceus ) and mr imaging in situations where the injury is confined to the kidney ( especially high - grade injuries ) , with the aim of monitoring the evolution of lesions and identifying promptly the onset of subclinical complications . 
instead , ct , with its panoramic capabilities and high spatial resolution , should be used to establish the causes of deterioration of the patients clinical and laboratory status . che insorge in un paziente con trauma renale clinicamente stabile , pu essere non solo dovuto a reazione peritoneale per filtrazione / diffusione di sangue dal retroperitoneo alla cavit peritoneale , ma anche alla manifestazione tardiva di una lesione traumatica intestinale la cui sintomatologia al momento del trauma pu essere sfumata o assente e la cui diagnosi ritardata aumenta il tasso di mortalit del 65% [ 23 ] : in altre parole , determinare la causa del peggioramento della sintomatologia significa rivalutare il tipo di management , adottare le misure terapeutiche alla luce di fatti nuovi e migliorare loutcome del paziente . 
 limaging nel follow - up , pertanto , prevede lutilizzo dellus ( ecd\ce - us ) e della rm nei casi in cui la patologia traumatica sia confinata al rene ( lesioni di alto grado specialmente ) , con lo scopo di monitorare levoluzione delle lesioni , identificando precocemente leventuale insorgenza di complicanze sub - cliniche , laddove la tc , per la sua panoramicit e risoluzione spaziale , dovrebbe essere impiegata per accertare le cause di un deterioramento del quadro clinico - laboratoristico del paziente . conclusions conclusioni whereas immediate exploratory surgery is recommended in penetrating trauma in consideration of the higher prevalence of associated lesions , the trend in blunt renal trauma is increasingly towards conservative management , with the goal of preserving organ integrity and reducing the incidence of complications . 
despite the recent technological progress of ct equipment and the undeniable role of ct in diagnosing and managing trauma , it must be emphasised that the radiologist plays a key role in emergency settings , a role that cannot be confined to the mere reporting of imaging findings , which would be ineffective and pointless unless properly interpreted in the light of its impact on management . 
this information can only be provided by the emergency radiologist , a professional devoted to emergency care who knows the effects of such trauma in all their complexity and multiple facets and , for this reason , is able to knowledgeably interact with the other members of the trauma team , responding effectively and promptly to the many complex diagnostic and management questions the trauma raises [ 49 , 50 ]  . in conclusione , si pu affermare che , se nei traumi penetranti lesplorazione chirurgica immediata raccomandata per la maggiore prevalenza di lesioni associate , lorientamento attuale sulla gestione dei traumi renali chiusi rivolto sempre di pi al management di tipo conservativo , con lo scopo di preservare lintegrit dorgano , riducendo lincidenza di complicanze . 
nonostante gli avanzamenti tecnologici che hanno riguardato le apparecchiature tc negli ultimi anni e lindubbio valore che la metodica ha assunto nella diagnosi e nella gestione del trauma , si deve sottolineare il ruolo chiave del radiologo nellemergenza che non pu limitarsi alla sola , asettica descrizione del reperto strumentale , che risulterebbe inefficace e afinalistico se non opportunamente interpretato alla luce del suo valore gestionale . 
unenhanced ct scans of 100 consecutive cancer patients were retrospectively reviewed by four readers to identify all solid , noncalcified pulmonary nodules ranging from 3 to 30 mm in diameter . the sensitivity and reading time of each reader and of cad alone were calculated at 3 - mm and 5 - mm thresholds with respect to the reference standard , consisting of a consensus reading by the four radiologists involved in the study . 
the mcnemar test was used to compare the sensitivities obtained by reading without cad ( readers 1 and 2 ) , with cad as sr ( readers 1 and 2 with a 2 - month delay ) , and with cad as cr ( readers 3 and 4 )  . 
le tcms non contrastografiche di 100 pazienti oncologici consecutivi sono state retrospettivamente analizzate da 4 lettori alla ricerca di noduli non calcifici di diametro compreso tra 3 e 30 mm . utilizzando come standard di riferimento la lettura in consenso effettuata da 4 radiologi , sono stati calcolati sensibilit e tempi di lettura di ogni lettore e del cad da solo , ai valori soglia dei noduli di 3 e 5 m stato utilizzato il test di mcnemar per confrontare i valori di sensibilit ottenuti dalla lettura senza cad ( lettori 1 e 2 ) , con cad come sl ( lettori 1 e 2 dopo 2 mesi ) , con cad come lc ( lettori 3 e 4 )  . 
sono stati identificati 258 e 224 noduli rispettivamente alla soglia di 3 e 5 mil cad da solo ha presentato una sensibilit del 62 , 79% e 67 , 41% ai valori soglia di 3 e 5 mm , rispettivamente con 4 , 15 e 2 , 96 falsi positivi per esame . 
lutilizzo del cad come lc , senza un significativo aumento dei tempi di lettura , non comporta un aumento significativo della sensibilit nellidentificazione dei noduli polmonari rispetto alla lettura senza cad ( p > 0 , 05 ) ; lutilizzo del cad come sl , a prezzo di un allungamento dei tempi di lettura , garantisce un significativo aumento della sensibilit rispetto alla lettura senza cad ( p < 0 , 001 ) e con cad come lc ( p < 0 , 025 )  . parole chiave tomografia computerizzata ( tc ) noduli polmonari cad introduction introduzione the lung is among the most frequent sites of metastatic disease , which appears in the form of pulmonary nodules [ 1 ]  . 
however , in addition to substantially increasing reading times and costs , double reading is rarely implemented in clinical practice due to organisational problems . numerous recent publications have shown that computeraided detection ( cad ) systems are able to assist the radiologist in identifying pulmonary nodules in chest ct , thus ensuring a higher sensitivity in nodule detection [ 1121 ]  . however , different studies have demonstrated a broad range of variability in the sensitivity values of cad systems in detecting pulmonary nodules ( 35%88% ) , a variability that is probably due to differences in examination technique , software and diagnostic criteria used [ 1726 ]  . 
in the former approach , two readings are done , the first without the assistance of the software and the il polmone rappresenta uno degli organi pi frequentemente interessati da metastasi sotto forma di noduli polmonari [ 1 ]  . 
lintroduzione dei moderni scanner per la tomografia computerizzata ( tc ) multi - detettore ( mdct ) ha comportato un progressivo aumento delle diagnosi di noduli polmonari di piccole dimensioni [ 25 ]  . 
allo scopo di ridurre il tasso di falsi negativi ( fn ) stato proposto limpiego del doppio lettore : questa scelta , tuttavia , oltre a comportare un sensibile aumento del tempo di lettura e dei costi , in realt raramente utilizzato nella pratica clinica per problemi organizzativi . 
numerose pubblicazioni recenti hanno dimostrato che i sistemi di diagnosi computer - assistita ( cad ) sono in grado di aiutare il radiologo nellidentificazione dei noduli polmonari nelle indagini tc del torace , garantendo un aumento della sensibilit nella identificazione dei noduli [ 1121 ]  . 
tuttavia diversi studi hanno dimostrato una grande variabilit dei valori di sensibilit dei sistemi cad nellidentificazione dei noduli polmonari ( compresa fra 35% e 88% ) probabilmente dovuta alle diverse tecniche desame , ai differenti software ed ai criteri diagnostici 952 radiol med ( 2010 ) 115 : 950961 second with the software activated to evaluate possible findings overlooked during conventional reading . 
the ideal approach to the use of cad software , however , has not yet been defined . to date few studies have compared the findings obtained using cad as sr and as cr [ 27 ]  . 
the aim of this study was to compare the sensitivity and reading times obtained with the use of cad as sr and cr in pulmonary nodule detection , using the consensus reading by four radiologists involved in the study as the reference standard . materials and methods a retrospective review of our centres database from september 2008 to february 2009 identified 125 cancer patients who were studied with unenhanced chest ct . 
we excluded 14 patients who suffered from lung disease severe enough to invalidate the correct segmentation by the cad software ( extensive pneumonia , effusion , pulmonary fibrosis ) ; seven patients with poor compliance to breath - hold instructions , which produced significant segmentation errors , and four patients who had undergone lung surgery ( segmentation errors due to surgical outcomes )  . atelectasis , pleural our study population therefore consisted of 100 patients ( 52 males , 48 females , mean age 62 years , range 1686 years )  . 
unenhanced scans were obtained during a single breath - hold using the following parameters : slice thickness , 1 mm ; feed 1 mm ; 200 mas ; 120 kv ; fov variable according to patient characteristics ; lung parenchyma reconstruction filter ( b50f )  . 
i sistemi cad sono prevalentemente utilizzati in qualit di secondo lettore ( sl ) o di lettore concorrente ( lc ) : nel primo caso si effettuano due letture , una senza ausilio del software e una dopo lattivazione dello stesso per valutare eventuali rilievi sfuggiti alla lettura tradizionale ; nel secondo caso invece , dopo aver attivato il software , si effettua una sola lettura avvalendosi dei rilievi forniti dal cad come base per individuazione dei noduli . 
lo scopo di questo studio confrontare la sensibilit ed i tempi di lettura dellesame ottenuti grazie al sistema cad della nostra apparecchiatura tc in qualit di sl e di lc nella identificazione dei noduli polmonari , utilizzando come standard di riferimento i risultati ottenuti dalla lettura in consenso dei 4 radiologi coinvolti nello studio . materiali e metodi lanalisi retrospettiva del database del nostro istituto nel periodo compreso fra settembre 2008 e febbraio 2009 , ha evidenziato 125 pazienti oncologici studiati con tc non contrastografica del torace . 
sono stati esclusi 14 pazienti che soffrivano di gravi patologie polmonari tali da invalidare la corretta segmentazione da parte del software cad ( estese polmoniti , atelettasie , versamenti pleurici , fibrosi polmonare ) , 7 pazienti poco collaboranti che hanno comportato importanti errori di segmentazione ( incapacit a mantenere lapnea ) e 4 pazienti sottoposti a chirurgia polmonare ( per errori di segmentazione correlati agli esiti chirurgici )  . la nostra popolazione di studio pertanto rappresentata da 100 pazienti ( 52 maschi , 48 femmine , et media : 62 anni , range : 1686 anni )  . 
i noduli con diametro inferiore ai 3 mm o superiore ai 30 mm ( masse ) sono stati esclusi dallo studio perch al di fuori del range da noi considerato . 
 image analysis protocollo mdtc two radiologists experienced in chest ct ( readers 1 and 2 , tutti i pazienti sono stati indagati con unapparecchiatura radiol med ( 2010 ) 115 : 950961 with 11 and 7 years of experience , respectively ) reviewed the ct studies independently and in standard working conditions : window settings for lung parenchyma , with centre = 600 and width = 1 , 600 hu ; multiplanar maximum intensity projection ( mip ) reconstructions with thickness between 5 and 20 meach image was assessed for solid noncalcified nodules suspicious for metastasis and with a diameter between 3 and 30 mto reduce the risk of recall bias , readers 1 and 2 repeated the evaluation at a distance of two months : after an initial conventional reading , the cad software was activated as sr to evaluate possible additional findings . 
in a subsequent phase , another two radiologists ( readers 3 and 4 , with 4 and 3 years of experience , respectively ) independently reviewed all examinations using the cad software as cr . 
to facilitate comparison , all nodules of each patient were measured and photographed on the work station , and their position on the x and y axes with respect to the patient table was recorded . 
only those findings that were accepted by all radiologists in agreement were considered true positive ( tp )  . the following parameters were determined : number of nodules per patient and mean number of nodules per patient ; mean diameter of nodules detected and their site ( isolated , perivascular and juxtapleural ) ; sensitivity , calculated as the ratio between the number of tp findings identified by each reader and cad alone and the tp findings of the reference standard , at 3 - mm and 5 - mm threshold values ; number of fp findings detected by each reader and by cad alone ; mean reading time during the different evaluation phases by each reader , with and without cad . cad system images provided by the cad software ( lung nodule ) and visualised on a dedicated screen were automatically processed with an mip reconstruction algorithm with thickness freely modifiable by the operator ( usually within the range of 515 mm )  . 
tutti gli esami sono stati archiviati su supporti mobili di registrazione ( dvd ) , per poter essere rivisti in qualsiasi momento su una workstation dedicata . analisi delle immagini due radiologi esperti in tc del torace ( lettori 1 e 2 , rispettivamente 11 e 7 anni di esperienza ) , indipendentemente , in condizioni di lavoro standard ( finestra di visualizzazione delle immagini per parenchima polmonare , con centro pari a 600 e ampiezza pari 1600 hu , ricostruzioni in proiezione di massima intensit [ mip ] multiplanari con spessore compreso fra 5 e 20 mm ) hanno revisionato le indagini tc alla ricerca di noduli solidi non calcifici di diametro compreso fra 3 e 30 mm , sospetti per secondariet . 
successivamente , a distanza di 2 mesi per ridurre il rischio di bias da memoria latente , i lettori 1 e 2 hanno ripetuto la valutazione utilizzando il cad come sl , attivandolo dopo aver effettuato una lettura tradizionale per valutare eventuali rilievi segnalati dal software . 
nella fase successiva , altri 2 radiologi ( lettori 3 e 4 , rispettivamente 4 e 3 anni di esperienza ) , indipendentemente , hanno revisionato tutti gli esami utilizzando il software cad come lc : in questo caso stata effettuata una lettura tradizionale simultaneamente alla valutazione dei rilievi forniti dal cad . 
stata inoltre registrata la posizione dei noduli sullasse x ed y rispetto al tavolo porta paziente per favorire il successivo confronto . tutti i radiologi coinvolti nella lettura erano a conoscenza del quadro clinico dei pazienti , ma erano alloscuro dei risultati ottenuti dai colleghi . 
il gold standard per la diagnosi stato determinato nel seguente modo : inizialmente tutti i rilievi sospetti individuati anche da un solo radiologo sono stati inclusi nel database principale : ogni nodulo stato dunque passato in rassegna dai 4 lettori in consenso : qualsiasi rilievo non accettato come vero nodulo anche da parte di un solo operatore stato rigettato e considerato un falso positivo ( fp ) ; solo i rilievi accettati da tutti gli operatori in consenso sono stati considerati veri noduli ( veri positivi , vp )  . sono stati calcolati i seguenti parametri : numero di noduli per paziente e numero medio di noduli per paziente ; diametro medio dei noduli rilevati e relativa localizzazione ( isolati , iuxta - vascolari e iuxta - pleurici ) ; sensibilit , calcolata come rapporto fra il numero di vp individuati da ogni lettore e dal cad da solo rispetto ai vp dello standard di 954 radiol med ( 2010 ) 115 : 950961 fig . 
axial images are automatically reconstructed with mip algorithm with variable thickness ( a )  . nodules are visualised on a menu ( yellow oval ) and by means of green boxes on the main screen ( a )  . 
il software fornisce una ricostruzione mip del nodulo selezionato , liberamente ingrandibile e ruotabile per valutare i rapporti con le strutture circostanti ( freccia in b - d )  . 
the software does not normally accept findings with nonnodular morphology and dimensions or density beyond its detection limits , thus limiting the number of fp findings due to reader error . to objectively evaluate statistical analysis the mcnemar test was used to compare sensitivity values obtained by the different readers with and without cad . the students t test was used to compare reading times of the different readers with and without cad . 
 altro aspetto fondamentale dato dalla possibilit di marcare in modo semplice e veloce eventuali noduli persi dal sistema di identificazione automatica per farli includere nella lista dei noduli accettati e valutarne in modo obiettivo le caratteristiche morfo - dimensionali . 
il software solitamente 956 radiol med ( 2010 ) 115 : 950961 372 suspected findings of noncalcified solid nodules with a diameter between 3 and 30 m during the consensus reading , 114 nodules ( 36.64% ) were excluded because they were considered fp by at least one of the readers . 
sensitivity values and fp results of each reader and cad alone , calculated with the different threshold values ( 3 mm and 5 mm ) , are summarised in table 2 . 
in non accetta rilievi con morfologia non nodulare e con dimensioni o densit al di fuori dei suoi limiti di identificazione , limitando i fp generati per errore dal lettore . analisi statistica il test di mcnemar stato utilizzato per confrontare i valori di sensibilit ottenuti dai vari lettori con e senza ausilio del cad . 
despite having higher sensitivity at the 5 - mm threshold , cad provided a greater diagnostic contribution at the 3 - mm threshold , as it assisted in the diagnosis of 30 ( 11.62% ) and 32 ( 12.4% ) nodules at this threshold against the 20 ( 8.92% ) and 25 ( 11.16% ) nodules at the 5 - mm threshold , which readers 1 and 2 , respectively , missed at conventional reading . 
reading with cad as cr , done by readers 3 and 4 , produced a nonsignificant increase in sensitivity with respect to the reading without cad by radiologists 1 and 2 ( p = 0.06 at 3 mm and p = 0.075 at 5 mm )  . 
the mean reading times with cad as risultati la valutazione indipendente da parte dei 4 radiologi ha fornito un totale di 372 rilievi sospetti per noduli solidi non calcifici di diametro compreso fra 3 e 30 m durante la lettura in consenso , 114 noduli ( 30 , 64% ) sono stati esclusi perch considerati fp da uno o pi lettori . 
pertanto lo standard di riferimento , alla soglia di 3 mm , consiste in 258 noduli ( media di 2 , 58 noduli per studio ; range 038 noduli )  . 
i valori di sensibilit ed i fp di ogni lettore e del cad da solo , calcolati a diversi valori soglia ( 3 mm e 5 mm ) sono riassunti nella tabella 2 . 
in totale , la valutazione automatizzata da parte del sistema cad ha messo in evidenza un totale di 162 / 258 noduli ( 62 , 79% ) alla soglia di 3 mm e di 151 / 224 noduli ( 67 , 41% ) alla soglia di 5 mpur presentando una sensibilit superiore alla soglia di 5 mm , il cad ha fornito un contributo diagnostico superiore alla soglia di 3 mm , avendo favorito la diagnosi di 30 ( 11 , 62% ) e 32 ( 12 , 40% ) noduli a questa soglia , contro 20 ( 8 , 92% ) e 25 ( 11 , 16% ) noduli alla soglia di 5 mm , sfuggiti rispettivamente ai lettori 1 e 2 nel corso della lettura tradizionale . 
il cad ha per evidenziato 415 fp ( media di 4 , 15 fp per caso con un range di 028 fp ) alla soglia di 3 mm , e 296 fp ( media 2 , 96 fp per caso , range 024 fp ) alla soglia di 5 m lutilizzo del cad come sl ha comportato un aumento statisticamente significativo di sensibilit nellidentificazione di noduli polmonari rispetto alla lettura senza cad sia per il lettore 1 ( da 75 , 19% a 86 , 82% con p < 0 , 001 alla soglia di 3 mm ; da 79 , 91% a 88 , 83% con p < 0 , 001 alla soglia di 5 mm ) che per il lettore 2 ( da 72 , 09% a 84 , 49% con p < 0 , 001 alla soglia di 3 mm ; da 75 , 89% a 87 , 05% con p < 0 , 001 alla soglia 5 mm ) ; la lettura con cad come lc , operata dai lettori 3 e 4 , ha comportato un aumento statisticamente non significativo della sensibilit rispetto alla lettura senza cad da parte dei radiologi 1 e 2 ( p = 0 , 06 a 3 mm e p = 0 , 075 a 5 mm )  . 
infine dal confronto dei risultati ottenuti dalla lettura con cad come sl da parte dei lettori 1 e 2 e della lettura con cad come lc da parte dei lettori 3 e 4 emerso una differenza di sensibilit statisticamente significativa a favore del cad come sl sia alla soglia di 3 mm ( p < 0 , 025 ) che alla soglia di 5 mm ( p < 0 , 05 )  . 
i tempi medi di lettura con cad come sl ( 330 secondi ) sono risultati essere significativamente superiori rispetto a quelli della lettura senza cad ( 135 secondi , p > 0 , 001 ) e a quelli con cad come lc ( 195 secondi , p > 0 , 001 ) ( tabella 3 )  . discussione lidentificazione di metastasi polmonari nei pazienti 958 radiol med ( 2010 ) 115 : 950961 sr ( 330 s ) were significantly greater than those without cad ( 135 s , p > 0.001 ) and those with cad used as cr ( 195 s , p > 0.001 ) ( table 3 )  . discussion detection of pulmonary metastases in cancer patients has a significant bearing on treatment decisions and prognosis [ 28 ]  . 
the greater number of images obtained with modern mdct systems has increased the detection rate of small lesions , but it has also increased the risk of fp diagnoses by depicting nodules that are not clinically significant . 
a significant improvement in sensitivity in detecting pulmonary nodules , particularly if they are small in size , has been demonstrated in a number of recently published studies [ 1121 ]  . 
despite the notably shorter reading times , cad as cr led to a significant loss in sensitivity with respect to cad as sr , with results identical to those of the reading without cad . 
our findings are in partial agreement with those obtained by beyer et al . : the use of cad as sr produced a significant increase in sensitivity for pulmonary nodule detection both for reader 1 ( p < 0.001 at the 3 - mm and 5 - mm threshold ) and reader 2 ( p < 0.001 at the 3 - mm and 5 - mm threshold )  . 
the reading with cad as cr , performed by readers 3 and 4 , led to a nonsignificant increase in sensitivity with respect to the reading without cad performed by radiologists 1 and 2 ( p = 0.06 at 3 mm and p = 0.075 at 5 mm )  . 
with respect to beyer et al . , we obtained sensitivity values for cad as cr that were , on average , higher both in the absolute sense and relative to oncologici ha un significato importante sullapproccio terapeutico e la prognosi [ 28 ]  . 
laumento del numero di immagini ottenute con le moderne tcms ha favorito lindividuazione di un numero crescente di lesioni di piccole dimensioni , ma ha aumentato il rischio di diagnosi fp , evidenziando noduli non significativi da un punto di vista clinico . 
i sistemi cad di diagnosi assistita per la tc del torace stanno incontrando un crescente interesse : un aumento significativo della sensibilit nella diagnosi di noduli polmonari , soprattutto se di piccole dimensioni , stato dimostrato da vari lavori recentemente pubblicati [ 1121 ]  . 
lutilizzo del cad come sl stata quella maggiormente valutata in studi recenti [ 8 , 11 , 12 , 1417 , 2023 , 26 ] : questa modalit garantisce solitamente i risultati migliori ma richiede tempi di lettura pi lunghi . 
 [ 27 ] hanno confrontato la sensibilit nellidentificazione di noduli polmonari ottenuta utilizzando il sistema cad come sl e come lc : il cad come lc , pur garantendo una sensibile riduzione dei tempi di lettura , comportava una significativa perdita di sensibilit rispetto allutilizzo del cad come sl , mentre i risultati erano sovrapponibili a quelli della lettura senza cad ; il cad come sl garantiva al contrario un aumento significativo della sensibilit rispetto alle altre modalit , a costo di un notevole allungamento dei tempi di lettura . 
 [ 27 ] : lutilizzo del cad come sl ha comportato un aumento statisticamente significativo di sensibilit nellidentificazione dei noduli polmonari sia per il lettore 1 ( p < 0 , 001 alla soglia di 3 e 5 mm ) che per il lettore 2 ( p < 0 , 001 alla soglia di 3 e 5 mm ) ; la lettura con cad come lc , operata dai lettori 3 e 4 , ha comportato un aumento statisticamente non significativo della sensibilit rispetto alla lettura senza cad da parte dei radiologi 1 e 2 ( p = 0 , 06 a 3 mm e p = 0 , 075 a 5 mm )  . 
la lettura con cad come sl ha dimostrato inoltre una sensibilit significativamente superiore rispetto alla lettura con cad come lc sia alla soglia di 3 mm ( p < 0 , 025 ) che alla soglia di 5 mm ( p < 0 , 05 )  . rispetto a beyer et al . 
 [ 27 ] abbiamo ottenuto mediamente valori di sensibilit mediante lettura con cad come lc lievemente superiori sia in senso assoluto che relativamente al confronto con la lettura senza cad . 
this difference may be due to the fact that reading times with cad as cr were slightly longer in our study , thus facilitating the detection of more findings missed by the computer . 
the fp rate was on average low ( two per examination ) in highly compliant patients , whereas it was much higher ( 12 per examination ) in poorly compliant patients with possible segmentation errors or in patients with a high number of nodules . 
the most common causes of fp results were findings that can be readily excluded : vessel crossings ( 58% ) ; pleural and fissure thickening ( 24% ) ; calcified nodules or lesions with subsolid density ( 18% )  . 
in our experience , cad proved to be very useful in two particular clinical settings : firstly , in patients free from disease , in whom without ever yielding a high number of fp results cad can help to increase the operators diagnostic confidence regarding thus confirming the diagnosis ; and secondly , in patients with a large number of lesions , because by facilitating the count , cataloguing and localisation of the lesions , the system facilitates comparison at follow - up . the effective absence of nodules , there were several limitations to our study . 
secondly , we dipendere dal fatto che i tempi di lettura con cad come lc sono stati lievemente pi lunghi nel nostro studio , favorendo lindividuazione di pi reperti sfuggiti al computer . 
dal nostro punto di vista , tuttavia , il notevole allungamento dei tempi medi di lettura associati alluso del cad come sl ( 330 secondi ) rispetto allutilizzo come lc ( 195 secondi ) e alla lettura tradizionale ( 135 secondi ) rende ancora dubbia la scelta della modalit di utilizzo nella pratica clinica . il sistema cad della nostra apparecchiatura tc ha mostrato una sensibilit pari a 62 , 79% e 67 , 41% rispetto al gold standard , rispettivamente ai valori soglia di 3 e 5 mm . questi valori sono nella media rispetto ai valori descritti in letteratura . 
tuttavia il numero di rilievi fp segnalati dal software rimane ancora alto ( 4 , 15 e 2 , 96 per caso , rispettivamente considerando le soglie dimensionali di 3 e 5 mm ) : i fp sono comunque risultati mediamente pochi ( 2 per esame ) nei pazienti molto collaboranti , mentre stato significativamente pi alto ( 12 per esame ) nei pazienti poco collaboranti , con possibili errori di segmentazione o con un elevato numero di noduli . 
le cause pi frequenti di fp sono state rappresentate da rilievi facilmente escludibili : incroci vasali ( 58% ) , ispessimenti pleurici e scissurali ( 24% ) , noduli calcifici o lesioni con densit sub - solida ( 18% )  . 
inoltre , laumento di sensibilit stato maggiore alla soglia di 3 mm ( 11 , 6% e 12 , 4% rispettivamente per lettori 1 e 2 ) che alla soglia di 5 mm ( 8 , 9% e 11 , 2% rispettivamente per lettori 1 e 2 ) , confermando che i potenziali vantaggi offerti dal software in termini di sensibilit crescono al diminuire del diametro soglia considerato . tra i vantaggi offerti dal software bisogna inoltre sottolineare limportanza di poter calcolare le dimensioni dei reperti studiati ( diametro massimo , area e volume ) , grazie al software in dotazione , in modo rapido , oggettivo e ripetibile [ 2933 ] , fatto essenziale nel paziente oncologico per una eventuale valutazione della risposta alla terapia medica secondo i criteri response evaluation criteria in solid tumors ( recist ) [ 3436 ]  . 
nella nostra esperienza il cad si rilevato molto utile in due contesti clinici particolari : primo , nei pazienti liberi da malattia , dove , senza mai fornire un elevato numero di fp , il cad pu permettere di aumentare la confidenza diagnostica delloperatore sulleffettiva assenza di noduli , confermandone la diagnosi ; secondo , nei pazienti con un elevato numero di lesioni , perch agevolandone il conteggio , la catalogazione e la localizzazione , facilita la comparazione nel caso di follow - up . 
secondo , abbiamo effettuato un confronto fra i risultati ottenuti da 2 960 radiol med ( 2010 ) 115 : 950961 performed a comparison between the results obtained by two groups of readers with very different levels of experience ( 11 and 7 years against 4 and 3 years , respectively )  . thirdly , the reference standard was the consensus reading by the four radiologists , as the final diagnoses were lacking due to insufficient surgical , pathology and followup data , a limitation that also hindered evaluation of the real clinical impact of the results obtained . 
fourthly , recall bias might have affected readers 1 and 2 during the reading with cad as sr , even though the time between the two readings ( 2 months ) should have reduced or eliminated this problem . in conclusion , the use of cad as cr , with no significant increase in reading times , does not produce a significant increase in sensitivity in detecting pulmonary nodules with respect to a reading without cad . 
the use of cad as sr guarantees a significant increase in sensitivity with respect to the approach without cad and with cad as cr , with the drawback of an increase in reading times . gruppi di lettori con esperienza molto differente ( 11 e 7 contro 4 e 3 anni rispettivamente )  . 
terzo , lo standard di riferimento stato rappresentato dalla lettura consensuale dei 4 lettori , mancando una diagnosi finale delle lesioni studiate , per insufficienza dei dati chirurgici , anatomopatologici o di follow - up : questo ha impedito inoltre di valutare il reale impatto clinico dei risultati ottenuti . quarto , un bias da effetto memoria potrebbe essere insorto nel corso della lettura con cad come sl da parte dei lettori 1 e 2 , anche se il tempo intercorso tra le due letture ( 2 mesi ) dovrebbe aver ridotto o evitato questo problema . 
the possible sources of incidents in the radiological process are exposed , due to human errors and to system errors connected both to the organization and to the dissemination of information technology in the radiological world . 
it also describes the most common methods and tools for risk analysis in health systems , together with some application examples presented in part riassunto il presente contributo , in veste di editoriale , affronta il tema della sicurezza dei pazienti nel processo radiologico : tale argomento , di grande attualit nazionale e regionale , ha stimolato una crescente attenzione agli incidenti e agli errori in medicina e la diffusione di procedure di gestione del rischio clinico ( o risk management ) in tutte le strutture sanitarie . 
vengono inoltre descritti i pi comuni metodi e strumenti di analisi del rischio nei sistemi sanitari , insieme ad alcuni esempi applicativi , presentati nella parte ii . keywords radiology error malpractice clinical risk management parole chiave radiologia errore malpractice gestione del rischio clinico 1122 radiol med ( 2010 ) 115 : 11211146 introduction : epidemiology of healthcare risk and the origin of clinical risk management one of the most controversial aspects of healthcare is the potential for disability and harm : wherever healthcare is delivered , the patient is at risk of suffering harm as an unintended consequence of that care . 
medical errors are confirmed as the main problem perceived by italians served by the national health service ( nhs ) : alleged cases of malpractice were the subject of 18% of reports ( > 25 , 000 ) to the italian patients association in 2008 . 
the alleged errors reported by citizens relate especially to surgical procedures ( 53% ) and misdiagnoses ( 26% ) , and the majority ( 88% ) occur in public health facilities [ 5 ]  . in the usa , it has been estimated that 1 million individuals per year are harmed by medical errors occurring during a hospital stay , and 120 , 000 deaths result as a consequence [ 6 ]  . 
these figures are substantially higher than those for deaths due to road traffic accidents ( > 43 , 000 ) and accidental falls ( 15 , 000 ) and are 1 , 000 times higher than deaths due to civil aviation accidents ( > 300 )  . 
on the basis of these data , it has been calculated that of 8 million patients admitted to hospital every year in italy , 320 , 000 ( around 4% ) may sustain avoidable harm [ 7 ] , and some 14 , 00050 , 000 may die because of errors made by physicians or caused by inadequate organisation of healthcare facilities [ 8 , 9 ]  . 
this extrapolation has been questioned by both the italian national federation of medical doctors , surgeons and dentists ( fnomceo ) and the association of physicians unjustly accused of malpractice ( amami ) [ 10 ] , on the grounds that no such data are available for italy . 
however , if this estimate were accurate , the italian nhs would incur economic damage in the order of around 260 million euros per year for prolonged hospitalisation only , in addition to increased insurance costs for public healthcare . 
the increased expenditure of all healthcare systems in the western world due to alleged malpractice and medical errors should not necessarily be interpreted as a sign of a declining healthcare . 
gli errori medici si confermano come il primo problema avvertito dagli italiani alle prese con il servizio sanitario nazionale ( ssn ) : presunti casi di malpractice sono stati loggetto del 18% delle segnalazioni ( oltre 25000 ) giunte durante il 2008 al tribunale per i diritti del malato . 
i supposti errori segnalati dai cittadini riguardano soprattutto interventi chirurgici ( 53% ) , seguiti da diagnosi sbagliate ( 26% ) , e la maggioranza ( 88% ) si registra in strutture pubbliche [ 5 ]  . negli usa si stima che ogni anno un milione di persone sia danneggiato da errori medici avvenuti durante un ricovero ospedaliero e 120000 siano i decessi conseguenti [ 6 ]  . questi numeri sono nettamente superiori a quelli relativi alle morti per incidenti stradali ( oltre 43000 ) , per cadute accidentali ( 15000 ) e sono superiori di 1000 volte ai decessi per incidenti aerei civili ( oltre 300 )  . 
sulla base di tali dati si calcolato che in italia , su 8 milioni di persone che ogni anno vengono ricoverate in ospedale , 320000 ( circa il 4% ) possano subire danni che potrebbero essere evitati [ 7 ] ed un numero variabile tra 1400050000 possano morire per errori compiuti dai medici o causati da uninadeguata organizzazione delle strutture sanitarie [ 8 , 9 ]  . 
tale estrapolazione stata contestata sia dalla federazione degli ordini dei medici e odontoiatri ( fnomceo ) sia dallassociazione medici accusati ingiustamente di malpractice ( amami ) [ 10 ] , in quanto in italia non sono disponibili dati di tal genere . 
se questa stima fosse reale , per il ssn si avrebbe un danno economico di circa 260 milioni di euro allanno solo per il prolungamento dei tempi di degenza a cui si aggiungerebbe lincremento dei costi assicurativi della sanit pubblica . 
attualmente le regioni spendono in media circa 30 milioni di euro ogni anno per le polizze assicurative [ 8 ] e dal 1994 al 2002 si registrato un forte incremento delle denunce e delle richieste di risarcimento ( le cause attualmente aperte sono 12000 , con richieste di indennizzi per circa 2 , 5 miliardi di euro )  . 
nello stesso periodo si osservato un incremento del costo medio dei sinistri per colpa professionale del 21% e di quello relativo alle strutture sanitarie del 67% [ 8 ]  . 
 the health system is made up of processes that are complicated by several variables ( specificity of the individual patient , complexity of interventions , different management procedures and models , etc ) , just like other organisations , such as aviation , military defence and nuclear plants . 
in these settings , human error must be contemplated as a possible event , and it is fundamental firstly to ensure ideal working conditions and implement measures that make it difficult for errors to occur [ 1116 ]  . 
secondly , a defence mechanism must be created that is capable of limiting the consequences of error while correcting the performance of the system in order to prevent the error from occurring agathe system itself may generate the circumstances leading to error ( stress , unfamiliar technology , etc )  . some 77% of physicians and 62.5% of nurses have experienced at least one adverse event in their working life , mainly due to stress and fatigue ( 42.3% ) , inadequate work organisation or staffing ( 16.6% ) and poor communication ( 9.5% ) [ 17 ]  . 
faced with an adverse event , the question to be asked is : why did the barriers to error fail ? were they inadequate ? the likelihood of error is also influenced by a lack of awareness of the potential risks of the healthcare process : an increased awareness of the culture of clinical risk is therefore fundamental . 
 from a recent survey carried out in the radiological community , it emerged that radiologists have little knowledge of crm techniques and require training in this field [ 16 ]  . 
in radiology , the first step is to become aware of the errors and adverse events that may occur during diagnostic activity : in daily practice , around 3%5% of radiological interpretations contain errors , but risks and possible adverse events may be identified at all levels of a radiological process . 
the many literature reviews on the main causes of errors describe risks related to problems of technique , perception , knowledge , evaluation and judgement , communication and interventional radiology procedures [ 7 , 1827 ]  . a recent survey conducted on a sample of 206 italian radiologists reported that the factors contributing to error in radiology were , in order of consensus , excessive workload come indice di una sanit in crisi , ma piuttosto il risultato dellevoluzione della relazione medico - paziente , che da decenni caratterizzata dallo sgretolamento del rapporto di fiducia ( conseguente alla mutata percezione sociale della disgrazia - malattia e della potenzialit della medicina , ritenuta infinita ) e dallaumento dei contenziosi , indipendentemente dalla qualit del sistema sanitario . 
per contenere questi costi e per migliorare la sicurezza dei pazienti , i sistemi sanitari su impulso nazionale e regionale hanno risposto sviluppando il sistema di governo del rischio clinico ( grc ) , incluso nelle attivit di governo clinico , mediante il quale lattivit medica viene sottoposta ad analisi e controllo di tutti i passaggi critici del processo produttivo ed in molti casi subisce un processo di reingegnerizzazione . 
 il sistema sanitario si compone di processi complicati da diverse variabili ( specificit dei singoli pazienti , complessit degli interventi , procedure e modelli gestionali diversi , ecc . ) , al pari di altre organizzazioni , quali ad esempio laviazione , la difesa militare , le centrali nucleari e , come queste , richiede un elevato controllo dei rischi . 
in tali contesti , lerrore umano deve essere contemplato come evento possibile ed fondamentale , in primo luogo , garantire le condizioni lavorative ideali e porre in atto azioni che rendano difficile per luomo sbagliare [ 1116 ] ed , in secondo luogo , attuare un sistema di difese in grado di arginare le conseguenze di un errore che si verificato , correggendo la performance di sistema per prevenire il suo ripetersi . 
il 77% dei medici e il 62 , 5% degli infermieri hanno vissuto almeno un evento avverso nella loro vita lavorativa , soprattutto per colpa di stress e affaticamento ( 42 , 3% ) , cattiva organizzazione del lavoro o personale inadeguato ( 16 , 6% ) e scarsa comunicazione ( 9 , 5% ) [ 17 ]  . 
di fronte ad un evento avverso la domanda importante da porsi : come mai le barriere allerrore hanno fallito ? erano forse insufficienti ? anche la mancata consapevolezza dei rischi potenziali del processo sanitario incide sulla probabilit di errore : pertanto indispensabile una maggiore diffusione della cultura del rischio clinico . 
 da una recente indagine svolta nel mondo radiologico emerge che i radiologi hanno una scarsa padronanza delle tecniche di grc e necessitano di attivit formative in questo settore [ 16 ]  . 
in campo radiologico , il primo processo quello di conoscere gli errori e gli eventi avversi che possono occorrere nellattivit diagnostica : nella pratica quotidiana , circa il 3%5% delle interpretazioni radiologiche contiene errori , ma rischi e possibili eventi avversi possono identificarsi ad ogni livello di un processo radiologico . 
nelle diverse revisioni della letteratura sulle principali cause di possibili errori , vengono descritti rischi 1124 radiol med ( 2010 ) 115 : 11211146 ( considered very important by 67% of responders ) , insufficient reporting times ( 88.6% ) , inability to consult colleagues ( 84.4% ) , poor work organisation ( 82.8% ) , uncooperative and stressful work setting ( 82.5% ) , obsolete equipment ( 78.6% ) , insufficient continuing education ( 75.6% ) and imprecise requests from referring physicians ( 74.2% ) [ 18 ]  . there are two different approaches to tackling adverse events in healthcare : 1 . 
system - oriented : in this approach , errors are seen as a failure of the system ( intended as a set of individuals , technologies and communications )  . 
attention is focused on the conditions under which the error occurs , and the solution is to address the deep and hidden problems and remodel processes in order to set up organisational defences [ 2831 ]  . ten years ago , the institute of medicine report stated that the majority of errors in healthcare are not due to human incompetence but to the system that needs to be made safer . in the analysis of possible adverse events , the international scientific community recommends a culture of openness , communication and cooperation among operators and between the operators and patients : this helps to gain awareness of the weaknesses in the organisation and make it safer , striving to constantly improve the quality of healthcare ( tables 13 ) [ 32 , 33 ]  . 
move to a model in which accountability is universal and reciprocal , not top down . several fundamental principles and individual and system strategies for addressing and preventing risk are shown in tables 1 and 2 . all healthcare organisations have received guidelines for the development of preventive risk analyses , which incorporate spontaneous incident reporting of near misses or accidents [ sentinel events ( se ) ] ( table 3 ) as a means to sterilise potentially dangerous situations , combined with actions to support professionals who adopt open organisalegati a : problemi tecnici , di percezione , di conoscenza , di valutazione e di giudizio , di comunicazione e correlati a procedure di radiologia interventistica [ 7 , 1827 ]  . 
lattenzione focalizzata sulle condizioni nelle quali avviene lerrore ed il rimedio indirizzato verso problemi nascosti e profondi del sistema e verso un rimodellamento dei processi , per la costruzione di difese organizzative [ 2831 ]  . gi nel 2000 il rapporto dellorganizzazione mondiale della sanit ( oms ) dichiarava che la maggior parte degli errori in campo sanitario non risiede nellincapacit degli uomini , ma nel sistema che deve essere reso pi sicuro . nellanalisi dei possibili eventi avversi la comunit scientifica internazionale propone come efficace la cultura dellapertura , della comunicazione e della collaborazione fra operatori e fra questi e i pazienti : ci aiuta a conoscere i punti deboli dellorganizzazione e a metterla in sicurezza , operando per il miglioramento continuo della qualit delle cure ( tabelle 13 ) [ 32 , 33 ]  . 
il modello di cura deve basarsi non pi sulla performance indipendente individuale , ma sul lavoro di gruppo interdipendente , collaborativo ed interprofessionale ; radiol med ( 2010 ) 115 : 11211146 1125 table 1 principles to be referred to for preventing clinical risk [ 34 ] 1 . 
integrarsi nellambiente di lavoro e rispondere alle legittime incarichi dei colleghi attese dei pazienti tional behaviour patterns based on learning from error and preparedness to analyse what might have gone wrong or , indeed , went wrong [ 3437 ]  . 
alcuni fondamentali principi e strategie di sistema ed individuali per fronteggiare e prevenire i rischi sono riportate nelle tabelle 1 e 2 . attualmente tutte le organizzazioni sanitarie hanno ricevuto linee di indirizzo per sviluppare analisi preventive dei rischi , utilizzando sistemi di segnalazione spontanea ( incident reporting ) di situazioni pericolose ( near miss ) o incidenti ( eventi sentinella , es ) ( tabella 3 ) per sterilizzare le situazioni individuate come pericolose , associate ad azioni di sostegno per i professionisti che adottano comportamenti organizzativi aperti , basati sullinsegnamento fornito dallerrore , con disponibilit ad analizzare quello che poteva andare o andato male [ 3437 ]  . 
studio degli eventi avversi per individuare i punti deboli sul lavoro ed individuazione delle cause di errore mediante gli strumenti di analisi del rischio : root cause analysis ( rca ) , analisi di processo ( failure mode and effect analysis , fmea ) ; 3 . 
addestramento e formazione del personale alla cultura del rischio clinico . lerrore umano , lerrore di sistema e limportanza delle teorie cognitive nellattivit medica lerrore in medicina ha tradizionalmente due aspetti rilevanti [ 21 ] : 1 . 
gli errori della medicina , considerata come insieme di teorie che riguardano la salute e lo stato di malattia delluomo , per la cui rappresentazione scientifica ci si avvale soprattutto della statistica e del teorema di bayes [ 38 ]  . 
il riconoscimento degli errori che comportano falsi negativi e falsi positivi consente di quantificare e confrontare la validit delle indagini mediche e dare loro un significato applicativo : dallanalisi degli errori si costruiscono i dati scientifici pi importanti ; 2 . 
gli specialisti della sanit non sono particolarmente inclini a sbagliare , ma ormai riconosciuto che lambiente di lavoro , nella complessit operativa , oltre allattuale mole di conoscenze in medicina in continuo divenire , a rendere il loro operato sempre pi esposto ad errori , molteplici e di varia natura . 
 1126 table 3 brief glossary of clinical risk radiol med ( 2010 ) 115 : 11211146 adverse event : unexpected event correlated with the health / welfare process that causes unintentional and undesired harm to a patient . adverse events can be preventable or unpreventable . 
an adverse event attributable to a mistake must be regarded as a preventable adverse event clinical risk : the probability that a patient will become a victim of an adverse event , i.e. 
suffer any harm or injury that can be attributed , even involuntarily , to medical care during hospitalisation and that causes prolongation of hospital stay or worsened health or death [ 6 ] danger : characteristics or intrinsic quality of a given entity ( material , equipment , work methods and processes ) having the potential to cause damage harm : temporary or permanent alteration of a part of the body or a physical / psychic function ( including the perception of pain ) human error : failure of actions planned in order to reach an expected objective incident : event that caused ( or had the capability of causing ) unintentional and / or unnecessary harm with respect to a patient near miss : incident occurring without harm , latent error bearing the potential to cause an adverse event , which does not occur by fortuitous chance because intercepted or because devoid of adverse consequences for the patient risk : the product of the probability ( p ) that a specific adverse event can happen ( danger ) and the severity of the resulting damage ( d )  . risk calculation also takes into account the capability of the human factor to identify in advance and contain the consequences of the potentially harmful event ( k factor )  . 
the intrinsic risks are correlated with the type of activity ; the external risks depend on the organisational , technological and environmental context in which the process takes place ( competences , novel technologies , proper use of techniques and devices  . ) risk profile : the mass of risks of a company , institution or department at a defined historical time risk management : process through which risk is measured and strategies are subsequently developed to control it . 
the risk management process has three main aims : ( a ) learning about the intrinsic risks in order to control them ; ( b ) identifying external risks to govern them and limit the possibility of errors and incidents ; ( c ) recognising the deep causes of incidents in order to avoid their repetition sentinel event : adverse event of particular seriousness , potentially avoidable and indicating a serious system malfunctioning , which can cause death or serious injury to the patient and which leads to a loss of confidence of the citizens towards the healthcare systeoccurrence of a single case is sufficient to make it appropriate for the organisation to promote : ( a ) a prompt investigation to ascertain which avoidable or reducible factors could have caused or contributed to it ; ( b ) implementation of adequate corrective measures [ 1 ] 1 . 
educating and training staff in the culture of clinical risk . human error , system error and the importance of cognitive theories in medical activity la stessa definizione di errore non trova unanime consenso : la pi adeguata quella che in primo luogo lo mette in relazione ad azioni e comportamenti osservabili [ 13 ]  . 
senders e moray [ 39 ] hanno proposto di definire come errore un accadimento non accettabile da una serie di regole oppure da un osservatore esterno dopo accurata valutazione . in campo medico unaltra definizione introdotta da reason [ 12 , 13 ] etichetta lerrore come il fallimento nel portare a termine , come nelle intenzioni , unazione precedentemente pianificata ( errore di esecuzione ) oppure luso di una pianificazione sbagliata per raggiungere un obiettivo ( errore di pianificazione )  . 
nel primo caso , la pianificazione stata perfettamente adeguata , ma le azioni non si sono svolte come previsto per errori attivi da distrazioni e dimenticanze ; nel secondo , le azioni seguono alla lettera i piani , ma tali piani si rivelano inadeguati per il raggiungimento degli obiettivi , perch non sono state previste sufficienti informazioni o mancano adeguate misure preventive ( errori latenti )  . 
 traditionally , two relevant aspects have been identified in errors in medicine [ 21 ] : la tassonomia degli errori umani di rasmussen [ 40 ] ed il modello del formaggio svizzero di reason [ 12 ] sono la radiol med ( 2010 ) 115 : 11211146 tabella 3 breve glossario del rischio clinico 1127 danno : alterazione temporanea o permanente , di una parte del corpo o di una funzione fisica o psichica ( compresa la percezione del dolore )  . errore umano : fallimento di azioni pianificate in relazione al raggiungimento degli obiettivi previsti . evento ( incident ) : accadimento che ha dato o aveva la potenzialit di dare origine ad un danno non intenzionale e / o non necessario nei riguardi di un paziente . evento avverso : evento inatteso correlato al processo assistenziale e che comporta un danno al paziente , non intenzionale e indesiderabile . 
un evento avverso attribuibile ad errore un evento avverso prevenibile . evento evitato quasi evento ( near miss ) : incidente avvenuto senza danno che ha la potenzialit di causare un evento avverso , che non si verifica per caso fortuito , perch intercettato o perch non ha conseguenze avverse per il paziente . 
 evento sentinella ( sentinel event ) : evento avverso di particolare gravit , potenzialmente evitabile ed indicativo di un serio malfunzionamento del sistema , che pu comportare morte o grave danno al paziente e che determina una perdita di fiducia dei cittadini nei confronti del servizio sanitario . 
 pericolo : propriet o qualit intrinseca di una determinata entit ( materiale , attrezzature di lavoro , metodi e pratiche di lavoro ) avente il potenziale di causare danni . profilo di rischio : insieme dei rischi di unazienda / impresa / reparto in un determinato momento storico . rischio : indica il prodotto fra la probabilit ( p ) che accada uno specifico evento avverso ( pericolo ) e la gravit del danno ( d ) che ne consegue . 
i rischi esterni dipendono dal contesto organizzativo , tecnologico ed ambientale in cui il processo si svolge ( competenze , tecnologie allavanguardia , corretto utilizzo di tecnologie e presidi )  . rischio clinico : la probabilit che un paziente sia vittima di un evento avverso , cio subisca un qualsiasi danno o disagio imputabile , anche se in modo involontario , alle cure mediche prestate durante la degenza , che causi un prolungamento del periodo di degenza o un peggioramento delle condizioni di salute o la morte [ 6 ]  . 
errors of medicine , in which medicine is considered as the collection of theories regarding the state of health and disease in humans , which is scientifically represented by using statistics and bayes theorem [ 38 ]  . 
errors of physicians , who as humans are subject to error . although healthcare specialists are not particularly prone to error , it is well known that the work environment with its operational complexity and the sheer volume and continuous evolution of medical knowledge make their work increasingly prone to errors of varying nature . 
 base teorica pi nota per lo studio degli errori e per lanalisi sistematica degli incidenti e rappresentano una modalit per costruire la catena degli errori finalizzata al miglioramento del sistema e non alla ricerca della responsabilit professionale . 
errore attivo : per lo pi ben identificabile , prossimo , in senso spazio - temporale , al verificarsi dellevento avverso ; spesso riconducibile ad unazione sbagliata commessa da un operatore o ad un incidente , ad esempio il malfunzionamento di uno strumento . 
gli errori attivi sono associati alle prestazioni degli operatori di prima linea in diretto contatto con il paziente : i loro effetti sono immediatamente percepiti e , dunque , facilmente individuabili 1128 radiol med ( 2010 ) 115 : 11211146 moreover , the very definition of error is still debated : the most satisfactory definition relates error to observable actions and behaviour [ 13 ]  . 
senders and moray [ 39 ] proposed to define error as an event that is not desired by a set of rules or an external observer after careful evaluation . in medicine , another definition introduced by reason [ 12 , 13 ] considers error as the failure to carry out a planned action as intended ( error of execution ) or application of an incorrect plan to achieve an aim ( error of planning )  . 
in the first case , planning is perfectly adequate , but the actions are not carried out as intended as a result of active errors due to distraction and inattention . 
in the second , the actions reflect the plan to the letter , but the plans prove to be inadequate for the intended aims because of a lack of sufficient information or sufficient preventive measures ( latent errors )  . 
 rasmussens taxonomy of error [ 40 ] and reasons swiss cheese model [ 12 ] are the best known theoretical models for the study of error and systematic analysis of accidents . 
active error : this is mostly identifiable and close in space and time to the occurrence of the adverse event . often , it can be traced to an incorrect action by an operator or to an incident ; for example , equipment failure . active errors are related to the performance of first - line operators in direct contact with the patient . 
latent errors are associated with distant activities ( both in space and time ) from the place of the accident , such as managerial , regulatory , organisational or even planning activities . 
the consequences of latent errors may lie dormant in the system for long periods of time and only become manifest when they combine with other factors capable of breaching the systems defences [ 41 ]  . the swiss cheese model was proposed by reason [ 12 ] to illustrate how error is generated in a complex systethe theoretical assumption is that , if error is foreseen , management activities must necessarily focus on the system and the setting where the professional works , trying to plan and put into place operational conditions and measures that make it difficult for people to do the wrong thing and easy to do the right thing . 
gli errori latenti sono legati ad attivit distanti ( sia in senso fisico che temporale ) dal luogo dellincidente , come le attivit manageriali , normative e organizzative o addirittura progettuali . 
le conseguenze degli errori latenti possono restare silenti nel sistema anche a lungo e diventare evidenti solo quando si combinano con altri fattori in grado di rompere le difese del sistema stesso [ 41 ]  . il modello del formaggio svizzero stato proposto da reason [ 12 ] per esplicitare in modo definito le modalit di generazione dellerrore in un sistema complesso . 
lassunto teorico di questo modello che , se lerrore atteso , le attivit di gestione devono necessariamente essere indirizzate sul sistema e sullambiente in cui il professionista lavora , cercando di progettare e realizzare dispositivi e condizioni operative che rendano difficile alle persone fare le cose sbagliate e , viceversa , facile fare le cose giuste . 
i sistemi di difesa possono essere di tipo hard ( allarmi , strumenti tecnologici , dispositivi di protezione ) e / o di tipo soft ( procedure , protocolli )  . 
i buchi duraturi nelle fette di formaggio ( errori latenti ) rappresentano le falle nel sistema di difesa : in virt della loro permanenza , incombono su tutte le attivit e pertanto sono pi rilevanti dei fori transitori e mobili ( errori attivi )  . 
questo modello applicato nei diversi settori del processo radiologico identifica la filiera dei possibili errori latenti o attivi delle diverse componenti del sistema . holes , which open and close very rapidly , continually shift location on the surface of the slice and do not usually leave any trace or major consequence ( such as the incorrect administration of a drug , an incorrect treatment procedure , instead , are represented by longetc )  . 
latent errors , standing , less mobile holes , which are dependent on the organisation and the rules governing work procedures ( e.g. lack of written procedures or shift work to ensure continuity of care )  . 
the long - standing holes in the cheese slices ( latent errors ) represent flaws in the defence system : owing to their permanent nature , they threaten all activities and are therefore more important than the transient and mobile holes ( active errors )  . 
skill - based actions : these refer to tasks carried out in an automatic fashion , governed by predefined schemes and lapproccio allerrore secondo le moderne teorie cognitive ha permesso di individuare i meccanismi della mente che ci portano a sbagliare , che riconoscono tre tipi fondamentali di azione , ognuna correlata a caratteristici pattern mentali ed ognuna fonte di errori specifici . 
si riferiscono a compiti svolti in modo automatico , governato da schemi e modelli predefiniti , effettuati senza lintervento della coscienza e di semplice esecuzione per chi abbia acquisito una particolare abilit nel settore . 
in generale , si tende a preferire le soluzioni rule - based poich richiedono minor sforzo cognitivo : se il processo rulebased non risolve il problema , in situazioni nuove o poco conosciute o quando le regole di cui si dispone non sono sufficienti ed adeguate ( ad esempio , intervenire su un quadro clinico insolito ) , si deve fare riferimento al sistema knowledge - based . 
slips : sono errori da carente esecuzione pratica di atti1130 radiol med ( 2010 ) 115 : 11211146 vit routinarie ed automatiche , da azione non coerente con le intenzioni . 
lautomatismo dellazione fallisce quando qualcosa di imprevisto interferisce con essa ( il medico si distratto ed ha prescritto un farmaco diverso da quello che aveva in mente ; il paziente riferisce di unallergia allinfermiere , che dimentica di segnalarlo al medico )  . 
errori durante la fase di pianificazione ( mistakes ) : le azioni si realizzano secondo le intenzioni e come sono state pianificate , ma la pianificazione stessa a non essere valida , poich conseguente a valutazione sbagliata , non idonea al raggiungimento dellobiettivo . 
il rule - based mistake ( r ) avviene quando si sceglie di applicare una regola o una procedura errata che non permette il conseguimento di un determinato obiettivo , a causa di unerrata percezione della situazione ( es . farmaco sbagliato rispetto alla patologia da trattare ) oppure nel caso di applicazione erronea di buone regole ( il farmaco adeguato , ma le dosi e il tipo di somministrazione non sono corrette oppure il farmaco non si pu somministrare al dosaggio prescritto )  . 
il knowledge - based mistake ( k ) conseguente alla mancanza di conoscenze , alla dimenticanza o alla scorretta applicazione di alcune applicazioni critiche , oppure ad un errore di giudizio o incapacit di utilizzare in maniera ragionevole le informazioni disponibili , con conseguente piano dazione sbagliato , sebbene le singole azioni eseguite siano corrette . 
the accident pyramid proposes that for every 300 , 000 unsafe acts there are 3 , 000 near misses , 290 minor injuries and , at the apex , 10 major injuries and one clai fig . 
rule - based actions : these are performed on the basis of stored rules that are voluntarily and autonomously implemented ( the pattern reflects the model if xthen y )  . 
the automatic performance of the task fails when something unexpected interferes with the action ( the physician was distracted and prescribed a different drug radiol med ( 2010 ) 115 : 11211146 1131 che sia possibile ) , spesso indotte da norme e regole difficili da osservare ; b . 
violazioni eccezionali , percorrendo lunica via possibile che permetta di fronteggiare situazioni inconsuete ed impreviste . lerrore umano in radiologia le specificit degli errori del radiologo e in radiologia riguardano , sul versante umano , lapproccio percettivo - interpretativo delle immagini e , sul versante del sistema , limpiego di tecnologie avanzate e complesse in continuo progresso . gli errori vengono distinti in errori di percezione e di interpretazione , bench vi sia unassoluta interdipendenza tra le due azioni . 
errori da mancata identificazione : sono i pi frequenti e responsabili di almeno il 60% del totale delle cause legali [ 43 ] ; si verificano in tutte le attivit radiologiche , anche se con diversa incidenza percentuale . 
sono inquadrabili in due tipologie : da cause non specifiche , ricollegabili alla limitatezza dellessere umano [ 44 ] , e da cause specifiche , suddivisibili in quattro diverse tipologie : i . 
da errore tecnico , in cui limmagine la fonte dellerrore per cattiva qualit tecnica , per una scorretta metodologia dindagine o mancanza di qualit dei materiali o delle procedure esecutive ; ii . 
da anomalie al di fuori dellarea dellesame : lerrore relativo a mancato riscontro di lesioni per la presenza di altre immagini , al di fuori del campo di studio ( come in caso di una lesione alle basi polmonari in corso di studio delladdome ) , che attirano lattenzione del radiologo , distraendolo ; iii.da conoscenza incompleta : sono errori spesso di difficile definizione , in quanto non sempre possibile stabilire se derivanti da scarsa competenza dellosservatore o da mancato rilevamento . 
da soddisfazione di ricerca ( satisfaction of search )  . tale errore si verifica per mancato rilevamento di lesioni addizionali ; losservatore ha colto una prima lesione che ha catturato la sua attenzione , lascianfig . 
errors of planning ( mistakes ) : these occur when the actions are carried out according to plan , but the plan itself is the result of misjudgement and is inadequate to achieve the goal . 
a knowledge - based mistake results from a lack of knowledge , biased memory or the wrong application of some critical knowledge , or misjudgement or inability to use the available information in a reasonable manner , with the result that the plan of action is wrong , even though the single actions are correct . medical negligence falls within this type of error : the negative outcome of the action originates from the inadequate knowledge that prompted the action . 
the error is intrinsic in limited rationality or in the difficulty in finding solutions to problems that present with a wide range of possible choices . 1132 radiol med ( 2010 ) 115 : 11211146 3 . 
exceptional violations , intended as the only possible course of action in novel or unfamiliar situations . human error in radiology the specific nature of errors of radiologists and in radiology concern , on the human front , perception - interpretation of images , and , on the systems front , the use of advanced and complex technology that is incessantly evolving . 
perceptual misses : the most frequent , these are responsible for at least 60% of all litigations [ 43 ] ; they occur in all fields of radiology , albeit with different frequencies . 
for pulmonary nodules , there is a minimum error rate of 20% , whereas error rates of 3%6% have been reported for emergency radiology . two types are recognised : ( 1 ) errors due to nonspecific causes , related to human fallibility [ 44 ] , and ( 2 ) those due to specific causes . 
sullargomento sono stati elaborati numerosi test con lesioni di disturbo , con la verifica , sperimentata , dellimpatto negativo di pi lesioni in un unico studio [ 21 ] ; b . 
le sviste del radiologo possono tradursi in un mancato riconoscimento di segni e quindi in una mancata diagnosi , collegandosi pertanto allerrore percettivo , oppure in fase di refertazione nellutilizzo di una semantica impropria ( errore di descrizione , description error ) , non coerente allindagine eseguita ( ad esempio , densit anzich ecogenicit per unindagine ecografica )  . 
in radiologia sono soprattutto errori di riconoscimento e decisionali , connessi a tunnel mentali che alterano la capacit di giudizio , che viene distorta . i tunnel mentali , da alcuni autori [ 45 ] chiamati pi scherzosamente vizi capitali , sono costituiti , per il radiologo , dagli aspetti legati allesperienza personale , individuale , alla storia clinica del allemotivit paziente . 
lapplicazione della diagnosi ad unimmagine in base al ricordo di un caso simile precedente , radiol med ( 2010 ) 115 : 11211146 1133 detect additional lesions ; the reader has identified one lesion that has captured his or her attention , leaving him or her satisfied with his or her performance . 
for the radiologist , mental tunnels , also called deadly sins by some authors [ 45 ] , refer to aspects related to personal experience , individual affectivity and the patients clinical history . 
il tunnel della memoria influenzata pu essere accompagnato da un eccesso di sicurezza delle proprie capacit ( overconfidence ) o della validit euristica ( availability euristic ) che induce ad usare solo la prima informazione che giunge alla mente , senza confrontare la diagnosi con stime probabilistiche ( cecit probabilistica o probability blindness ) ; ii . 
influenza emotiva ( regret bias ) : una distorta probabilit di diagnosi viene influenzata dallinconscio desiderio di allontanare qualcosa che dispiace e , contro ogni evidenza scientifica , la mente accetta che la prognosi pi grave sia poco probabile e quindi lontana . 
linfluenza dellemotivit prevale nelle diagnosi su persone legate affettivamente allosservatore o , pi generalmente , in quelle pi giovani ; iii.influenza del contorno ( framing bias ) : il contorno , come storia clinica , quesito del curante o confronto con i radiogrammi precedenti , incide pesantemente nelle diagnosi radiologiche [ 46 ] ed influenza il referto . 
studi sperimentali [ 47 ] dimostrano ampie variazioni di interpretazione delle immagini , a seconda se il radiologo sia a conoscenza o meno delle informazioni cliniche , specie in caso di radiogrammi incerti . 
test condotti su pazienti pediatrici ai fini del riscontro di bronchiolite , enfatizzano come lanamnesi rappresenti un fattore di distorsione , sia in casi con storia positiva che negativa per la malattia . 
laltro punto cruciale che influenza la diagnosi radiologica il confronto con i radiogrammi precedenti , che comunque costituisce , anche secondo lamerican college of radiology ( acr ) lo standard di una buona pratica e una parte integrante dellindagine radiologica e della formulazione del referto . 
regret bias : a distorted probability of diagnosis is influenced by the unconscious desire to keep something unpleasant away and , against all scientific evidence , the mind accepts that the worse prognosis is unlikely and hence remote . 
experimental studies [ 47 ] have shown wide variations in the interpretation of images depending on whether or not the radiologist was aware of the clinical information , especially in the case of uncertain radiographs . 
tests on paediatric patients being imaged for bronchiolitis have highlighted that the clinical history is a distortion factor , whether positive or negative for disease . the other crucial factor that influences the radiological diagnosis is the comparison with previous examinations , which , according also to the american college of radiology ( acr ) , remains a good practice standard and an integral part of imaging examinations and reports . 
this condition can be prevented by following the advice of berlin [ 48 , 49 ] : ( a ) the radiologist should , indeed , consult previous examinations and reports , but the latter only after having thoroughly evaluated the new examination ; ( b ) previous reports should only be used for consultation and should therefore not influence the radiologist but help by providing new clinical alternative diagnostic hypotheses . 
a specific psychological error related to framing may occur within screening settings . quality indicators in screening mammography , such as reduced recall rates , influence the radiologist who may underestimate some minimal signs or signs of presumed benignity and fail to recall the woman [ 21 ]  . 
failure to recall may be considered an error due to distorted judgement , which only double reading or the help of computer - assisted diagnosis ( cad ) systems may reduce . information or these mechanisms introduce the other aspects , those of system errors . richiamo , influenzano lattivit del radiologo che pu sottovalutare per questo alcuni segni minimi o di presunta benignit , non richiamando la donna [ 21 ]  . 
 tali meccanismi introducono alle problematiche degli errori di sistema . lerrore di sistema in radiologia si pu definire come sistema radiologico linsieme delle fasi organizzativo - gestionali e operative del processo di acquisizione , descrizione ed interpretazione delle immagini , che ha per scopo la diagnosi . 
lapproccio sistematico consente di valutare la presenza ed il numero delle situazioni rischiose , anche se da esse non sono derivati danni o altre conseguenze per i pazienti , e di proporre azioni adeguate , nella logica che solo la conoscenza di un pericolo potenziale pu aiutare a prevenirlo . 
per quanto attiene la radiologia e i relativi rischi specifici radiologici ( rsr ) la sezione di studio della sirm di etica e radiologia forense si assunta lonere e la responsabilit della prima stesura di un elenco tipo di rsr , che ogni unit operativa ( uo ) pu monitorare , a cadenze mensili e / o trimestrali [ 50 ]  . 
fase pre - procedura , differenziata per pazienti ricoverati o ambulatoriali : i passaggi successivi possono essere individuati nella richiesta , nella prenotazione , nelle istruzioni al paziente per la preparazione e linformazione sulle modalit desecuzione dellesame . 
lidentificazione del paziente nella corrispondente documentazione costituisce , anche sotto il profilo medico - legale , la condizione che conferisce autenticit alla prestazione radiologica ; diversamente il documento risulta falso . 
altri aspetti riguardano laccettazione acritica di richieste non appropriate o incongruenti rispetto allindicazione , specie quando comportano la somministrazione di mezzo di contrasto o manovre interventistiche , per le quali obbligatorio il consenso informato espresso in forma scritta . 
fase della procedura , dove si sviluppano i processi specifici per ogni singola tecnica o gruppi di tecniche affini . radiological work can be divided into three interconprima del referto ; radiol med ( 2010 ) 115 : 11211146 system error in radiology a radiology system may be defined as the series of organisational , managerial and operational phases of the process of image acquisition , description and interpretation with the aim of diagnosis . 
a systematic approach allows evaluation of the presence and number of hazardous situations , even when these have produced no harm or ill - effects on the patient , and to propose adequate actions with the rationale that only awareness of a potential danger may help to prevent its consequences . 
with regard to radiology and its specific radiological risks ( srrs ) , the societ di radiologia medica ( sirm ; italian society of medical radiology ) study group on ethics and forensic radiology drafted a list of srrs , which every radiology division can monitor at monthly or 3 - monthly intervals [ 50 ]  . 
preprocedure phase , which is differentiated into inpatient and outpatient setting : the steps in this phase are the examination request , booking , patient preparation instructions and information about the examination procedure . 
another aspect regards the noncritical acceptance of requests that are inappropriate or inconsistent with the indication , especially when they involve the use of contrast material or interventional procedures , both of which require written informed consent . 
mancata comunicazione al curante di reperti importanti quanto inattesi o non ricercati . la gestione del rischio connesso al sistema radiology information system ( ris ) - picture archiving and communication system ( pacs ) : requisiti tecnologici minimi per la sicurezza le moderne uo di radiologia , con i loro intensi carichi di lavoro e dotate di moderne metodiche multi - immagine , non possono pi essere gestite senza un solido supporto informatico , indispensabile sia per la gestione dei dati anagrafici , amministrativi e di esecuzione degli esami , sia per la memorizzazione delle migliaia di immagini afferenti ad un singolo studio , sia per la sempre pi complessa attivit di refertazione . 
purtroppo , il supporto di ris e pacs , anche nelle realt pi illuminate in cui un team di specialisti dedicati si occupa routinariamente della loro manutenzione , non privo di punti critici che , in una sfortunata sequenza di circostanze , possono portare ad errori diagnostici con conseguenze terapeutiche [ 51 ]  . 
lattivit di unuo di radiologia deve venir considerata come un processo : la mancanza di questa visione dinsieme dellattivit radiologica e la conseguente impossibilit di inserire questa attivit allinterno di un ospedale comporta errori latenti di sistema con conseguenze che tutti conoscono . 
considerare lattivit radiologica come un processo porta a suddividere le funzioni quotidiane in una serie di passi , ciascuno motivato e da ciascuno dei quali atteso un prodotto , concatenato in sequenza logica . 
questo approccio comporta due conseguenze principali : la possibilit di suddivisione in blocchi 1136 radiol med ( 2010 ) 115 : 11211146 available means of communication , in the most appropriate and timely manner . 
failure to communicate important findings to the referring physician when the findings are unexpected or not looked for . risk management connected to the ris - pacs system : minimum technological requirements to ensure security modern radiology departments , with their intensive workloads and modern multi - imaging equipment , cannot be managed without a reliable computerised system , which is indispensable for handling demographic , administrative and imaging data , for storage of the thousands of images produced by a single study and for increasingly complex reporting activity . 
the radiology information system ( ris ) and picture archiving and communications system ( pacs ) , even in the most enlightened settings where it is routinely maintained by a team of dedicated specialists , is not free of critical features that , in a unfortunate sequence of circumstances , could lead to diagnostic errors with consequences on treatment decisions [ 51 ]  . 
the activity of a radiology department should be viewed as a process : failure to view it as an integrated whole and the resulting inability to incorporate its activity within a hospital involves latent system errors with the consequences we are all aware of . considering radiological activity as a process implies subdividing daily tasks into a series of logically interrelated steps , each motivated by and responsible for producing an outcome . 
this approach has two main implications : the possibility of subdividing activities into logical blocks , which facilitates planning , and the possibility of effectively controlling the single steps in the process , which allows identification of the critical areas and factors causing potential error . 
moreover , viewing radiological activity as a process makes it possible to incorporate computer systems , whether radiological ( ris - pacs ) or hospital information systems , into the logical process , enabling control over both planning and results . 
the former , which are common to all those who use computer logici delle attivit , con una maggior facilit nella progettazione , e di un controllo effettivo ed efficace sulle singole tappe del processo , potendo identificare i punti critici ed i fattori di potenziale errore . 
inoltre , lattivit radiologica valutata come processo permette di inserire fattivamente i sistemi informativi , sia dedicati alla radiologia ( ris , pacs ) , sia di pertinenza aziendale , allinterno del percorso logico , anche in questo caso con controllo sia della progettazione che del risultato . 
i primi , comuni a tutti coloro che , anche in ambiente non sanitario , utilizzano sistemi informativi , riguardano la sicurezza fisica e logica degli apparati , rischi nella trasmissione dei dati , problemi di riservatezza e privacy , problemi di alterazione , perdita o distruzione dei dati . 
i secondi sono peculiari dellattivit sanitaria , radiologica in particolare , e comprendono la gestione dei dati anagrafici , delle immagini diagnostiche e del prodotto del processo radiologico , ovvero del referto . 
da ci discende che la gestione del rischio nellutilizzo di un sistema ris - pacs non pu e non deve essere demandata solo ad un radiologo , poich le competenze richieste per questa attivit sono troppo distanti dalla sua formazione culturale . 
la legge prevede che per ogni sistema che tratti in forma informatica dati sensibili e quelli sanitari lo sono per definizione venga redatto il documento programmatico sulla sicurezza ( dps ) [ 53 ] con la descrizione degli eventi potenzialmente dannosi e le procedure in atto per prevenire o contrastare il danno . 
la stesura del dps appannaggio degli specialisti dalle competenze non radiologiche oltre che del radiologo , che deve essere coinvolto nelle attivit di prevenzione dei rischi , poich egli solo conosce il processo nei suoi dettagli , potendo indirizzare i progettisti verso la strada maestra . 
la possibilit di inquadrare temporalmente la sequenza di eventi in esame riveste una particolare importanza specie nel caso di consulti ed in ogni attivit in cui i sistemi siano fisicamente distanti tra loro : poich ogni sistema informatico possiede un proprio orologio , necessario che tutti gli orologi di un sistema integrato segnino la stessa ora . 
il tempo di sistema per tale motivo tipicamente una procedura aziendale , che varca i confini della radiologia , di pertinenza dei sistemi informatici ospedalieri , che si devono far carico della sua radiol med ( 2010 ) 115 : 11211146 1137 systems , whether or not in a healthcare setting , regard the physical and logical security of the hardware , risks of data transmission , problems of confidentiality and privacy and problems of tampering , loss or destruction of data . 
the latter are unique to healthcare settings , and in particular to radiology , and comprise management of demographic data , diagnostic images and of the product of the diagnostic process the report . 
thus , ris - pacs risk management cannot and must not be entrusted only to a radiologist , as the required competences are too far removed from his or her background and training . 
the law establishes that for each computerised system handling sensitive data and health data are sensitive by definition ! a security policy document is prepared [ 53 ] that describes all potential risks and the procedures in place to prevent or contrast the damage . drafting the security policy document is the task not only of specialists with nonradiological expertise but of the radiologist , who must necessarily be involved in risk prevention , as he or she alone is familiar with the process in all its details and thus able to offer guidance to the nonradiological specialists . 
system time : the possibility of establishing the time of a sequence of events is especially important in peer - to - peer consultations and in any activity in which the systems are physically distant from each other . 
thus , system time is typically a procedure that goes beyond the boundaries of the radiology department and is carried out by the hospital information systems that see to its distribution . for devices that are physically distant from one another , the system clocks should be synchronised with external reference clocks typically available on the internet that ensure time equality even outside the premises of the healthcare institution . 
in most italian hospitals , many patient microdatabases coexist due to the presence of computer applications that handle small segments of the healthcare workflow , each one being independent and run by the clerical staff of the various departments , where any distribuzione . 
per apparecchi fisicamente distanti tra loro , si consiglia la sincronizzazione con orologi esterni di riferimento , tipicamente disponibili sulla rete internet , che assicurino luguaglianza del tempo anche al di fuori della struttura fisica aziendale . 
nella maggioranza degli ospedali italiani coesistono numerose micro - anagrafi , dovute alla presenza di applicativi informatici che gestiscono piccole parti del workflow sanitario , ognuna autonoma ed alimentata dal personale di sportello dei vari reparti , dove vengono registrate le variazioni dei dati del paziente ed immesse in un sottosistema anagrafico ( ad esempio allanagrafe della radiologia )  . 
generalmente , al di sopra di queste anagrafi locali incombe unanagrafe ospedaliera , frutto in gran parte degli applicativi che gestiscono il centro unico di prenotazione ( cup ) , ma che raramente comunica variazioni ai sottosistemi di reparto . 
si pu assistere , quindi , alla presenza di un numero finito di posizioni anagrafiche dello stesso paziente , al quale viene attribuito un diverso identificativo da ogni sottosistema del medesimo nosocomio che svolga esami strumentali ( esempio per una colonscopia ed una tomografia computerizzata [ tc ] addome ) e le informazioni demografiche possono non essere coincidenti ; risulta estremamente difficile poi stabilire quale posizione sia quella corretta o la pi corretta , anche per dettagli ( quale il numero di telefono , la cui correttezza indispensabile per comunicazioni urgenti ) , la cui inesattezza pu creare disservizi organizzativi anche gravi , con ricadute cliniche ( ad esempio , limpossibilit di riconvocare pazienti per integrazioni o completamento di esami )  . 
la soluzione organizzativa per strutture ospedaliere di dimensioni mediograndi , quella di istituire un ufficio predisposto al controllo , integrazione e correzione dellanagrafe aziendale ; tale provvedimento non adottabile dalle strutture di piccole dimensioni . 
comunque indispensabile prevedere laggiornamento e il controllo periodico ( pulizia ) delle posizioni anagrafiche dei pazienti , che comporta anche la trasmissione ai diversi sottosistemi delle variazioni e modifiche introdotte . 
per i dati anagrafici si deve fare riferimento allo standard hl7 , protocollo di messaggistica che 1138 radiol med ( 2010 ) 115 : 11211146 variations in patient data are recorded and entered into a patient subsystem ( e.g. , radiology department patient database )  . 
generally , on top of all these local patient databases is a larger hospital patient database , which is commonly generated by booking - system applications but which rarely communicates with the single subsystems . 
this leads to the presence of a number of records for the same patient , who is assigned a different identification code by each hospital subsystem that performs imaging procedures [ e.g. 
the organisational solution for medium - to - large hospitals is to set up an office to check , integrate and correct the hospitals patient database , a solution that is not feasible in small hospitals . 
for patient databases , reference must be made to the health level 7 ( hl7 ) standard , a messaging protocol that allows both propagation of the information and notification of message receipt and data correction . 
firstly , a well - established and shared procedural protocol must be in place , which clearly specifies who will receive data from whom and the location where data will be corrected and propagated to the other points of care . 
admission and request management : the above discussion on patient databases assumes the existence of a hospital - wide system for managing admissions , an application that correctly identifies the user and assigns him or her a status relative to the healthcare services delivered inpatient , outpatient , preadmission . 
in prima istanza , deve funzionare un percorso procedurale stabilito e condiviso : chi raccoglie i dati e da chi e dove vengono inseriti correttamente e propagati agli altri punti di cura . 
le precedenti riflessioni sulle anagrafiche comportano la presenza di un sistema aziendale di gestione ricoveri , applicativo informatico che si occupa di identificare correttamente lutente e di assegnargli lo status con il quale vengono erogate le prestazioni sanitarie : ricoverato , esterno , pre - ricovero . 
 , infatti , questo sistema ( pi noto con la sigla adt , acronimo di admittance , discharge and transfer : - hl7 , 2.3.1 : il sistema amministra anche le procedure di trasferimento e di dimissione dei pazienti ) che si occupa della scelta del nominativo da un elenco ( anagrafe ) e propaga questa informazione ai restanti pezzi del sistema ospedaliero . 
in esso possono essere registrati ( e trasmessi a valle ) i nomi di coloro che prendono in carico il paziente , i medici prescrittori o comunque i medici di riferimento , oltre che essere annotati dati clinici di importanza generale ( ad esempio , le allergie ) che possono migliorare il livello qualitativo dellinformazione disponibile e quindi la qualit del prodotto finale , anche radiologico . 
sicuramente importante per un sistema adeguato allo stato dellarte , un applicativo di gestione degli ordini , ovvero un sistema aziendale di richiesta elettronica delle prestazioni diagnostiche , che riceve i dati demografici del paziente dal sistema adt e seleziona dallelenco delle prestazioni disponibili lesame necessario , completando la richiesta con lindispensabile quesito diagnostico ed eventuali notizie cliniche accessorie . 
definitely crucial to a state - ofthe - art system is an application for request handling , that is , a hospital - wide system for electronic orders for diagnostic services , which receives the demographic data from the adt system and selects the requested examination from a list of available services , completing the request with the indispensable diagnostic question and any additional clinical data . 
work list : this refers to the formation , by the ris , of a list of names and univocally associated services transmitted to the radiological system ( also called modality ) that will perform the examination and that are grouped by booking date . 
in practice , the use of a work list simplifies the radiographers work by displaying on the modality console the list of patients to be imaged during the work shiit is very important that the work lists be generated and transmitted to the modalities correctly and that their presence does not become a possible source of error in routine work . 
the system must be able to eliminate the name of the patient from the console after completion of the examination ( see part ii ) , to provide names for 1 day only and to allow for possible reinsertion of names from previous days that need to be monitored and possibly justified . 
procedure status and confirmation of data storage : the digital imaging and communications in medicine ( dicom ) messaging standard [ 56 ] allows for the possibility of indicating to the various systems making up the radiology work chain the status of a procedure ( modality performed procedure step ) [ 57 ]  . 
the ris can therefore da parte del sistema ris , di un elenco di nominativi e di prestazioni a loro univocamente associate , trasmesse allapparecchiatura radiologica ( anche chiamata modalit ) che dovr eseguire lesame , raggruppate per data di prenotazione . 
nella pratica , lutilizzo delle worklist agevola il tecnico di radiologia nella routine quotidiana , presentandogli sulla console di comando della modalit lelenco dei pazienti che debbono sostenere lesame in quel turno di lavoro . 
molto importante non soltanto che le worklist vengano correttamente generate ed inviate allapparecchiatura che eseguir lesame , ma che la loro presenza non sia possibile fonte di errore nellattivit quotidiana . 
 necessario che il sistema sia in grado di eliminare il nome del paziente dalla console della modalit una volta che lesame sia concluso ( vedi parte ii ) , che sia in grado di fornire i nominativi di una giornata e solo di quella e che eventuali ripescaggi da giornate precedenti siano possibili , ma monitorati ed eventualmente giustificati . 
la messaggistica dello standard imaging and communications in medicine ( dicom ) [ 56 ] prevede la possibilit di indicare ai vari sistemi componenti la catena lavorativa radiologica , lo stato di esecuzione di un esame ( modality performed procedure step ) [ 57 ]  . 
oltre ad una migliore gestione dei flussi di lavoro , il tracciamento di questi messaggi rappresenta unulteriore garanzia di sicurezza ed una possibilit di controllo sul prodotto , fornendo precise indicazioni sui tempi di esecuzione di un esame ( si pensi ad un eventuale contenzioso su esami eseguiti in urgenza ) e la valutazione dei tempi totali di processo radiologico . 
altrettanto importante la corretta gestione del messaggio di avvenuta archiviazione ( storage committment ) [ 57 ] inviato dal pacs alla modalit ad avvenuta ricezione delle immagini componenti lo studio . necessario che le immagini vengano rimosse dallapparecchiatura che le ha generate solo dopo che questo messaggio sia stato ricevuto , onde evitare la loro irrimediabile perdita . 
per gestire questi messaggi necessaria unavveduta implementazione dei moduli dicom sulle apparecchiature , elemento non scontato e generalmente non previsto nei capitolati di appalto o di acquisto delle modalit : necessaria unesplicita richiesta per la loro attivazione , poich ancor oggi alcune funzionalit di base dello standard non sono automaticamente fornite dalle ditte produttrici . 1140 radiol med ( 2010 ) 115 : 11211146 be automatically notified of the modality - performed status of a procedure . 
in addition to better management of workflow , the log of these messages provides further guarantee of safety and possibility for product control by supplying precise information on the time taken to perform a procedure ( consider a possible litigation regarding emergency examinations ) and assessment of the total time of a radiological process . 
uncontrolled distribution can introduce many risk factors : special care must go into the construction of the distribution system , in particular with regards to correct matching of patient details with images and updating data when these are modified on the source systeany variation must be propagated to the distribution systems in real time to prevent dangerous misalignments . 
the presence of these systems presupposes adherence of the machines being controlled to the safety requirements listed above , especially as concerns the timing of events ( system time )  . 
to ensure the true safety of processes , it is more important to have a solid temporal coherence and event infrastructure recording than simply placing a date and time stamp on the radiology report [ 59 ]  . 
the date and time stamp is an electronic process through which the document is marked with a reference that attests , in a definite and incontrovertible manner , that the document was produced before placing of the reference . 
una distribuzione non controllata pu introdurre numerosi fattori di rischio : necessaria una particolare attenzione alla costruzione del sistema deputato alla distribuzione , in particolare per la corretta corrispondenza sia del dato anagrafico che del contenuto ed alle procedure di aggiornamento dei dati qualora essi siano modificati sul sistema di origine . 
ogni sistema informativo dovrebbe prevedere la possibilit di monitoraggio e registrazione degli eventi , controllando le attivit degli utenti e dei sistemi in caso di necessit [ 51 ]  . 
la presenza di questi sistemi presuppone laderenza , da parte delle apparecchiature sottoposte a controllo , ai requisiti di sicurezza precedentemente elencati , specie per ci che riguarda la collocazione temporale degli eventi ( tempo di sistema )  . 
al fine di assicurare una reale sicurezza dei processi , riveste maggiore importanza una solida infrastruttura di coerenza del tempo e di registrazione degli eventi che non la semplice apposizione al referto di una marca temporale [ 59 ]  . 
la marca temporale un processo informatico mediante il quale si appone ad un documento un riferimento che attesta , in modo certo ed inoppugnabile , che il documento stato prodotto prima dellapposizione del riferimento stesso . essa ha valore di prova in giudizio e non contestabile ( non opponibile a terzi )  . 
infatti , per poter ricostruire una sequenza di eventi necessario registrare tutte le operazioni compiute , anche sulle immagini , sia da personale umano che da sistemi informatici in modo automatico . 
si deve pertanto prestare attenzione , in fase di progetto , allinclusione nel capitolato di gara dei sistemi di audit , che , anche se comporta un aumento dei costi iniziali , porter ad un beneficio certo in termini di controllo e sicurezza dellattivit quotidiana . 
con tale complessit si deve radiol med ( 2010 ) 115 : 11211146 1141 the technological events , one has to record all the operations performed , even on the images , both by personnel and information systems . 
thus , care must be taken in the planning phase to include in the tender specifications audit systems that , although entailing initial costs , will lead to definite benefits in terms of control and safety of daily operations . 
this complexity has become part of our daily working lives , as it is impossible to imagine running a radiology department without an ris or using a multislice ct scanner without a pacs . 
it will therefore be necessary to set up a multidisciplinary team of professionals who , each drawing upon their own competence , can collaborate and contribute to the maintenance and development of the systems that are routinely used in healthcare ( see part ii )  . tools for analysing risk in healthcare systems risk analysis tools are used to analyse processes to prevent events in a proactive approach or to analyse events that have occurred through a reactive approach . 
risk identification usually involves analysing administrative and informative data , through incident reporting , or evaluating claims and reports . risk identification , which uncovers the frequency of events , is followed by risk analysis , which involves assessing the severity of the impact of events , rating risks on a priority scale and indicating possible solutions on the basis of validity , feasibility and cost - effectiveness . 
proactive analysis : this aims at identifying and eliminating critical elements in the system before incidents occur ; the processes making up the activity are analysed to identify possible critical elements [ 28 , 29 ]  . 
it consists i breaking down the process into macro phases ( temporal sequence ) ; ii defining activities and tasks ; iii defining potential faults ; iv quantifying faults in terms of severity , probability and detectability . 
 the main techniques adopted in proactive analysis are quotidianamente fare i conti , non essendo pi pensabile gestire una radiologia senza un sistema ris o una tc multistrato senza un archivio pacs . 
sar quindi indispensabile dotarsi di una struttura multidisciplinare di professionisti che , ognuno per le proprie competenze , collaborino e concorrano al mantenimento ed allo sviluppo dei sistemi con i quali si svolge quotidianamente lattivit sanitaria ( vedi parte ii )  . gli strumenti di analisi del rischio nei sistemi sanitari gli strumenti per lanalisi del rischio analizzano i processi per prevenire gli eventi con modalit di tipo proattivo , oppure analizzano gli eventi , quando occorsi , con metodi di tipo reattivo . 
dopo lidentificazione , che evidenzia sostanzialmente la frequenza degli avvenimenti , si passa allanalisi del rischio , che comporta una valutazione della gravit delle conseguenze degli avvenimenti , la collocazione su una scala di priorit dei rischi e lindicazione di possibili soluzioni in base alla loro validit , realizzabilit e convenienza . 
mira allindividuazione e alleliminazione delle criticit del sistema prima che gli incidenti avvengano : si basa sullanalisi dei processi che costituiscono lattivit , individuandone i possibili punti di criticit [ 28 , 29 ]  . 
 le principali tecniche adottate nellanalisi proattiva sono la failure mode and effect analysis ( fmea ) , metodologia che analizza le modalit di difetto di un processo , prodotto o sistema , e la failure mode and effect criticality analysis ( fmeca , analisi dei modi , degli effetti e della criticit dei guasti ) , che include anche unanalisi di criticit usata per valutare , mediante opportuni diagrammi , la 1142 radiol med ( 2010 ) 115 : 11211146 failure mode and effect analysis ( fema ) , a method that analyses the modes of failure of a process , product or system ; and failure mode and effect criticality analysis ( fmeca ) , which also includes criticality analysis to evaluate , through appropriate diagrams , the severity of the effects of a failure in relation to the likelihood of the failure occurring . 
this method , developed in the united states in 1949 in the sectors of industrial planning and military airforce ( see part ii ) , started to be applied with the necessary modifications for healthcare settings in the 1990s . 
it is therefore a systematic qualitative analysis performed by a multidisciplinary team with the aim of identifying critical areas in a process and assessing human reliability prospectively in order to redesign them [ 60 ]  . the characteristic elements of fmea / fmeca are : creating a multidisciplinary team ; developing a flowchart of the process ; utilising a severity / probability / detectability matrix ( index of probability of risk , ipr ) gravit delle conseguenze di un difetto correlata con la probabilit del suo verificarsi . 
tale metodologia , nata negli stati uniti nel 1949 nei settori di progettazione industriale e nellaviazione militare ( vedi parte ii ) , stata applicata con opportuni adattamenti in ambito sanitario a partire dagli anni 90 . 
reactive analysis : this begins with the adverse event and reconstructs a posteriori the sequence of events with a view to identifying the factors that caused or contributed to the event and obtaining a reconstruction that identifies not only the active errors but also the risk factors ; the final goal is to learn about the deep , organisational causes that generated the event ( latent errors ) : i . 
starting from errors detected in a system , the causes of these errors are sought through an inductive method that attempts to investigate the deep causes by asking why questions for each action and its possible deviation . 
as an event - analysis technique , rca was first used in engineering and other systems such as aviation and the aerospace industry due to the need to gain knowledge about high - risk factors . 
parte da un evento avverso e ricostruisce a posteriori la sequenza di avvenimenti per identificare i fattori che lo hanno causato o che hanno contribuito al suo verificarsi , ottenendo una ricostruzione che , oltre agli errori attivi , individui i fattori di rischio ed il cui risultato finale mirato a conoscere le cause profonde , organizzative , che lo hanno generato ( errori latenti )  . 
la root cause analysis ( rca ) lo strumento pi utilizzato a tal fine : a partire dagli errori riscontrati in un sistema se ne ricercano le cause attraverso un metodo induttivo che procede in profondit mediante domande che esplorano il perch di ogni azione e di ogni sua possibile deviazione . 
incident reporting is another method of reactive analysis and consists of structured collection of sponfrom operators taneous and voluntary regarding incidents and near misses rather than harms , adverse events or organisational problems . 
any event that caused harm ( or had the potential to cause harm ) to patients and healthcare workers can be reported , as can those regarding equipment malfunction or damage or any event with a potential to justify some form of litigation . 
the professionals involved can bring the case to attention by means of an incident reporting forthe form is handed in to the department facilitator and stored in a database , subsequently , in collaboration with the crm division , an assessment is made as to whether an audit is required . 
it is important to report not only incidents that actually occurred but also and above all near misses , as these are numerically more frequent , there is no emotional involvement , it is easier to learn from them and it is easier to ensure the anonymity of these reports , which may be barometers of serious risks . 
il sistema di segnalazione ( incident reporting ) unaltra modalit di analisi reattiva che consiste nella raccolta strutturata delle segnalazioni spontanee e volontarie da parte degli operatori di incidenti e quasi incidenti ( near miss ) piuttosto che solo di danni ed eventi avversi o problemi organizzativi . 
i professionisti coinvolti possono porre il caso allattenzione tramite una scheda di segnalazione dellevento avverso . la scheda deve essere consegnata al facilitatore del reparto e viene archiviata in un database : successivamente , in collaborazione con luo di grc , si valuter se sia necessario o meno effettuare un audit . 
va ricordata limportanza di segnalare non solo gli eventi avversi avvenuti ma soprattutto i near miss in quanto questi sono numericamente pi frequenti , non c coinvolgimento emotivo , si pu imparare pi facilmente dal quasi errore ed pi facile tenere anonimi i dati da questo tipo di segnalazioni , che possono costituire un barometro dei rischi seri . 
quanti pi eventi si segnalano , tanto meglio funzioner il sistema di segnalazione [ 36 , 6264 ]  . il sistema di incident reporting uno strumento semplice che permette di : delineare profili di rischio di specifiche realt operative ; settings ; coinvolgere tutti gli operatori e renderli sensibili al involve all of the operators and sensitise them to the tema della sicurezza del paziente ; the evolution of segnalati / segnalabili ; issue of patient safety ; time monitor over reported / reportable events ; provide an objective basis for implementing corrective actions . the strengths of the system lie in detecting events that are uncommon or emerging and therefore difficult to prevent and identifying cross - sectional issues with the immediate opportunity for handling individual cases . 
i punti di forza del sistema di incident reporting sono rappresentati dallindividuazione di eventi poco frequenti o emergenti e quindi difficilmente prevenibili e dallidentificazione di problematiche trasversali con possibilit immediata di gestione di singoli casi . 
i punti di debolezza sono la variabilit nel numero delle segnalazioni e nella 1144 radiol med ( 2010 ) 115 : 11211146 series , limited epidemiological reliability and difficulty identifying the reference universe ( denominators )  . 
 the culture of patient safety is part of a broader cultural change that encompasses a more open and direct relationship among the various operators and a climate of integration and collaboration ( tables 1 , 2 ) [ 30 , 31 , 65 ]  . 
it should be clear , especially to front - line operators , that the focus of the investigation is not the behaviour of the individual but the systems in place to guarantee the safety of the patient . 
to this end , it is fundamental that the system become official and acknowledged . casistica , la ridotta affidabilit epidemiologica e la difficile individuazione delluniverso di riferimento ( denominatori )  . 
 la cultura della sicurezza del paziente rientra in un pi ampio cambiamento culturale che prevede un rapporto aperto e diretto tra i vari operatori ed un clima di integrazione e collaborazione ( tabelle 1 , 2 ) [ 30 , 31 , 65 ]  . 
deve essere chiaro , soprattutto allo staff in prima linea , che loggetto dellindagine non sono i comportamenti individuali ma i sistemi messi in atto per la sicurezza del paziente . 
ariyurek2 1dicle university school of medicine , department of radiology , 21280 , diyarbakir , turkey 2hacettepe university school of medicine , department of radiology , sihhiye 06100 , ankara , turkey correspondence to : c . 
the aim of this study was to describe visualisation rate and appearance of all pericardial sinuses and recesses and to evaluate whether there is a significant difference between visualisation of these sinuses and recesses on 2 - , 4 - , 16and 64 - slice multidetector computed tomography ( mdct )  . 
age , and 4 - , 16and 64slice mdct versus 2 - slice mdct and the presence of pleural effusion appeared as significant predictors of the presence of any recess . 
la differenza nella frequenza di identificazione dei recessi pericardici risultata significativa tra la tcms a 2 strati e le tcms con differente numero di strati ( p < 0 , 01 )  . 
di conseguenza necessario approfondire la conoscenza degli aspetti variabili dei recessi pericardici con la tcms per evitare diagnosi errate . parole chiave recessi pericardici tcms anomalie anatomiche imaging del torace radiol med ( 2010 ) 115 : 10381046 introduction pericardial recesses are potential spaces formed by extensions of the pericardial cavity at the reflections of the serous pericardium between the great vessels at the base of the heart . 
in a cross - sectional anatomical study , vesely and cahill [ 1 ] systematically described and named the pericardial recesses as the transverse sinus ( aortic recess and pulmonic recess ) , oblique sinus , postcaval and pulmonary venous recesses . 
although the larger and well - known recesses may be easily diagnosed and do not constitute a diagnostic challenge for radiologists , the less well - known recesses may be misinterpreted as lymphadenopathy or another mediastinal disease process . familiarity with these normal anatomical structures is essential to prevent misdiagnosis . 
to our knowledge , there is no report describing the prevalence and appearance of all pericardial recesses on mdct systems with a different number of rows , which are being increasingly used in radiology practice . 
ct images of the remaining 588 patients ( mean age 53.618.0 years ; female - to - male ratio 330 / 258 ) were analysed . 1039 imaging parameters ct scans were obtained with siemens multidetector ct ( mdct ) scanners ( siemens medical solutions , erlangen , germany ) ; siemens somatom duo ( 2 detector rows , 2.5mm collimation , 120 kv , 150 mas ) , siemens volume zoom ( 4 detector rows , 2 - mm collimation , 120 kv , 150 mas ) , siemens sensation 16 ( 16 detector rows , 1.5 - mm collimation , 120 kv , 150 mas ) and philips brilliance ( brilliance ct scanner , philips healthcare ) ( 64 - detector rows , 1mm collimation , 120 kv , 210 mas )  . 
one hundred millilitres of nonionic iodinated contrast material ( 300 mg / ml ) was injected iv through an antecubital vein at 4 ml / s flow rate using a power injector . 
fluid in a pericardial sinus and recess was accepted as well - marginated homogenous nearwater attenuation ( 10 to 25 hounsfield units ) without a wall or rim of material , with higher attenuation in an expected location of a sinus or recess . 
we measured attenuation values to confirm that they were consistent with fluid , determined the volume ( small , moderate , or large ) and the shape of every pericardial fluid pocket ( band , crescent , hemisphere , ovoid , round , triangle , rhomboid or irregular )  . 
 description of recesses and sinuses we evaluated the pericardial sinuses and recesses , as described by previous researchers ( table 1 ) [ 1 , 2 , 8 ]  . 
transverse sinus contains several recesses that extend as diverticula between the major vessels and the atriuthe anterior superior aortic recess ( asar ) is located anterior to the left pulmonary artery and ascending aorta . 
seventy - two patients were excluded from the study due to the presence of pericardial effusion , mediastinal lymphadenopathy , mediastinal mass , pleural effusion or consolidation adjacent to recesses , and artefacts compromising evaluation of the table 1 classification of sinuses and recesses tabella 1 classificazione dei seni e recessi 1 . 
transverse sinus superior aortic recess anterior superior aortic recess ( asar ) posterior superior aortic recess ( psar ) inferior aortic recess ( iar ) left pulmonic recess ( lpr ) right pulmonic recess ( rpr ) 3 . 
pericardial cavity proper postcaval recess ( pcr ) left pulmonary venous recess ( lpvr ) right pulmonary venous recess ( rpvr ) 1040 radiol med ( 2010 ) 115 : 10381046 superior aortic recess ( psar ) lies posterior to the ascending aorta . 
visualisation rates of the lpvr and pcr were not significantly different among all groups ( table 2 ) , and that of the transverse sinus ( presence of any asar , psar , iar , rpr , lpr or pcr ) was 83.8%. radiological appearances and volumes of pericardial recesses are given in table 3 . 
2a , b con tcms a 64 strati si visualizza recesso polmonare sinistro a forma di rombo sotto larteria polmonare sinistra ( freccia ) in ricostruzione assiale ( a ) e sagittale ( b )  . radiol med ( 2010 ) 115 : 10381046 1041 fig . 
all these factors substantially increase diagnostic accuracy of the examination but at the cost of some potential problems in the differential diagnosis of normal structures and pathological lesions [ 8 ]  . 
protopapas and westcott [ 3 ] reported visualising the left pulmonic recess in 23% of 61 patients without pericardial effusion , the superior pericardial recess in 43% and the transverse sinus in 49% . thin - section ct has contributed to a high depiction rate of pericardial recesses . 
identified pericardial recesses in 2.530.4% of patients ( 15.9% for asar , 30.4% for psar , 3.4% for iar , 12.5% for lpr , 7.9% for rpr , 7.7% for os , 2.7% for pcr , 2.5% for lpvr and 4.7% for rpvr ) [ 8 ]  . 
thin - section ct resulted in a significant increase in recognition of pericardial recesses in their study , with a prevalence of 41.4% for asar , 44.7% for psar , 16.7% for iar , 36.8% for lpr , 29.7% for rpr , 28.7% for os , 16.8% for pcr , 19.8% for lpvr and 10.8% for rpvr [ 8 ]  . as electron beam ct is less affected by cardiac motion artefacts , it offers better image quality . 
 [ 11 ] reported 95% and 89% depiction rate for the transverse sinus and oblique sinus , respectively , in 100 patients without pericardial effusion using electrocardiographically ( ecg ) - triggered electron - beam ct and 1.5 - mm section thickness . 
ecg - triggered acquisition as applied in cardiac mdct for coronary ct angiography has been used commonly in radiologic practice and may have a possible role in determining visualisation of pericardial recesses . 
 [ 8 ] included images obtained with mdct , the percentage of patients evaluated with mdct and visualisation rate of recesses on mdct were not reported [ 8 ]  . although all studies of pericardial recesses have used the term prevalence on ct , we prefer to use visualisation rate , as recesses are potential pockets created by reflection of pericardium , which may be visualised when filled with fluid . in our study , all recesses but the pcr were detected at a greater frequency in comparison with previous reports [ 2 , 3 , 8 ]  . 
fewer motion artefacts due to shorter acquisition time , decreased partial volume effects provided by thin sections and superior image resolution of mdct may be the causes of the high visualisation rate in this study . 
6a , b triangular anteriorsuperior aortic recess ( asar ) containing a small amount of fluid is seen anterior to the ascending aorta on the coronal reformatted image ( arrow ) of 64 - row multidetector computed tomography ( mdtc ) ( a )  . 
6a , b con tcms a 64 strati si visualizza il recesso aortico antero - superiore triangolare ( asar ) contenente una piccola quantit di fluido davanti allaorta ascendente sulle ricostruzioni coronali ( freccia ) ( a )  . 
 in this study , pericardial recesses shapes were variable . as the volumes of asar and psar increased , their shapes changed from triangular and crescentic to rhomboid and hemispheric , respectively . 
with increased volume from small to large , crescentic iar became round , band - shaped lpr became rhomboid , band - shaped rpr became irregular , band - shaped os became ovoid and band - shaped lpvr became round . 
although there is no consensus regarding shape and nomenclature among studies , most pericardial recess shapes in our study were similar to previous reports [ 3 , 8 ]  . 
 the appearance of normal pericardial recesses on ct may lead to their misdiagnosis as abnormal processes . sometimes , they can be misinterpreted as aortic dissection , mediastinal mass , pericardial cyst , thymic cyst , thymus or mediastinal or hilar lymphadenopathy [ 4 , 1419 ]  . 
hyperattenuating appearance of most lymph nodes , an enhanced rim of necrotic isodense lymph nodes and lack of contrast enhancement of recesses are valuable signs to distinguish lymph nodes from pericardial recesses [ 2 , 19 ]  . 
shifting from a collimation of 2 mm ( 4 rows ) to 1.5 ( 16 rows ) or 1 mm ( 64 rows ) does not affect pericardial recess visualization , whereas a significant difference was found only with the shift from 2.5 ( 2 rows ) to 2 mm or less ( 4 , 16 , 64 rows )  . 
this finding may be due to a possible cutoff set at 2 - mm collimation for the overall visualisation rate of pericardial recesses . we also observed that patients with pleural effusion had higher visualisation rates of pericardial recesses than those without . 
the higher visualisation rate of iar and os on 64 - channel mdct cannot be explained by the ct technique used in our study or by recess features . to our knowledge , this is the first study evaluating the visualisation rate of all pericardial recesses on thin sections with mdct systems with a different number of detector rows . our study has several limitations . 
first , the 64 - slice scanner has a slightly lower visualisation rate than scanners with a lower number of detector rows because of higher number of cases evaluated compared with those evaluated with 4and 16 - slice scanners . 
lastly , because the aim of imaging was to detect thromboembolism , 64 - slice ct acquisitions were not ecgtriggered , which could improve pericardial sinus visualisation . in conclusion , mdct scans provide improved pericardial sinus and recess visualisation . 
cademartiri1 , 2 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia , universit degli studi di napoli federico ii , napoli , italy 4dipartimento di radiologia , sdn fondazione irccs , napoli , italy 5dipartimento di radiologia , universit di verona , verona , italy correspondence to : f . 
abbiamo incluso 450 pazienti ( 284 uomini ; et media 6412 anni ; 1288 ) che sono stati sottoposti a tc e a ecc per sospetta malattia coronarica ; per la tc abbiamo utilizzato delle ricostruzioni multifasiche secondo un piano asse corto e le abbiamo valutate con un software dedicato , basato sul calcolo dei volumi del vsin con la regola di simpson ; per lecc abbiamo utilizzato un calcolo basato sulla regola di simpson biplanare . 
sono state osservate differenze statisticamente significative , anche se con buona correlazione , tra le misurazioni effettuate ( r = 0 , 71 ; p < 0 , 05 )  . 
lecc ha mostrato una lieve tendenza a sovrastimare la fe . dividendo la nostra popolazione in sotto - gruppi , la fe stata sottostimata dallecc nel sotto - gruppo con valori di fe > 50% , ed stata sovrastimata nei sotto - gruppi con fe 1016 radiol med ( 2010 ) 115 : 10151027 provides significantly different data from ct , with a bias that increases proportionally to lv systolic dysfunction . keywords cardiac computed tomography echocardiography left ventricular ejection fraction real world compresa tra 35% e 50% ed in quello con fe < 35% , con differenze tra tc ed ecc che si sono rivelate sempre significative ( p < 0 , 05 ) con una concordanza progressivamente pi bassa . 
 parole chiave tomografia computerizzata del cuore ecocardiografia frazione di eiezione del ventricolo sinistro mondo reale introduction introduzione the importance of cardiac ejection fraction ( ef ) as a necessary parameter for establishing diagnosis , prognosis and treatment of patients with cardiovascular disease has been defined in numerous studies [ 19 ]  . 
in particular , left ventricular ef ( lvef ) is commonly used to stratify risk in patients with suspected or known coronary disease and assess functional recovery during medical therapy or after myocardial revascularisation . 
ef evaluation is therefore a fundamental step in routine cardiological practice , and many methods are available that provide varying degrees of accuracy and reproducibility for determining ef [ 1020 ]  . 
two - dimensional transthoracic echocardiography ( ecc ) has been used for decades for ef measurement as a result of its noninvasiveness , low cost , ease of use , beside availability and lack of ionising radiation , but the method suffers from poor intraand interobserver reproducibility [ 21 ]  . 
thanks to recent technological progress , ef values obtained with multislice computed tomography ( msct ) have demonstrated high levels of agreement with those provided by magnetic resonance imaging ( mri ) , the current standard of reference [ 19 ]  . 
the purpose of this paper is to report on our experience in evaluating agreement between ecc and msct determinations of ef by analysing real - world data from a large patient population . molteplici studi hanno definito limportanza della frazione di eiezione cardiaca ( fe ) quale parametro necessario per linquadramento diagnostico , prognostico e terapeutico del paziente con malattie cardio - vascolari [ 19 ]  . 
in particolare , la fe del ventricolo sinistro viene abitualmente utilizzata per la stratificazione del rischio dei pazienti con malattia coronarica sospetta o nota , per la valutazione del recupero funzionale in corso di terapia medica o dopo rivascolarizzazione miocardica . 
la valutazione della fe rappresenta quindi un momento fondamentale nella pratica clinica cardiologica di routine ; attualmente disponiamo di numerose metodiche capaci di misurare la fe in maniera pi o meno accurata e riproducibile [ 1020 ]  . 
per la sua non invasivit , il basso costo , la facilit di utilizzo anche al letto del paziente e la non esposizione a radiazioni ionizzanti , per decenni la fe stata misurata con lecografia trans - toracica 2d ( ecc ) , metodica peraltro gravata da una limitata riproducibilit intraed inter - osservatore [ 21 ]  . grazie ai recenti progressi tecnologici , la fe ottenuta con tomografia computerizzata ( tc ) multistrato ha mostrato una elevata concordanza con i valori ottenuti con risonanza magnetica , attuale standard di riferimento [ 19 ]  . 
nel valutare il grado di concordanza della fe calcolata con ecc e tc , abbiamo voluto riportare la nostra esperienza analizzando dati ricavati dal mondo reale . materials and methods patients materiali e metodi pazienti between january 2006 and may 2009 , we recruited 450 patients ( mean age 6412 years ; 284 male and 166 female ; table 1 ) who underwent msct coronary angiography to exclude the presence of coronary disease [ 2226 ] , which was followed by ecc to evaluate cardiac function . 
exclusion criteria for the msct examination were a heart rate da gennaio 2006 a maggio 2009 abbiamo arruolato nel nostro studio 450 pazienti ( et media 6412 anni ; 284 maschi e 166 femmine ) ( tabella 1 ) che sono stati sottoposti ad una angiografia coronarica mediante tomografia computerizzata multistrato ( tcms ) con lo scopo di escludere la radiol med ( 2010 ) 115 : 10151027 table 1 patient demographics population characteristics total number age ( meansd ; median ; range ) male / female cardiovascular risk factors 6412 ( 66 ; 1288 ) 284 / 166 hypertension dyslipidaemia diabetes smoking family history bmi ( kg / m2 ; meansd ) bsa ( m2 ; meansd ) sd , standard deviation ; bmi , body mass index ; bsa , body surface area ( mosteller formula ) tabella 1 caratteristiche dei pazienti popolazione totale numero pazienti studiati et ( mediads ; mediana ; intervallo ) uomini / donne 6412 ( 66 ; 1288 ) 284 / 166 fattori di rischio cardiovascolare 292 ( 65 ) 215 ( 48 ) 80 ( 19 ) 123 ( 27 ) 225 ( 50 ) 274 1.90.2 292 ( 65 ) 215 ( 48 ) 80 ( 19 ) 123 ( 27 ) 225 ( 50 ) 274 1 , 90 , 2 ipertensione dislipidemia diabete fumo di sigaretta familiarit bmi ( kg / m2 ; mediads ) bsa ( m2 ; mediads ) ds , deviazione standard ; bmi , body mass index ; bsa , body surface area ( formula di mosteller ) ( hr ) > 65 bpm unresponsive to beta - blockers , atrial fibrillation with high ventricular response , known allergy to contrast media , renal insufficiency and / or impaired respiratory function [ 27 ]  . 
the study was approved by the local ethics committee , and all patients provided written informed consent . multislice computed tomography the msct scan protocol is the same as that used in previous investigations evaluating ef with msct [ 19 ]  . patients with hr > 65 bpm received a beta - blocker ( atenolol , 5 mg repeatable ) administered intravenously under blood pressure and hr monitoring . 
all acquisitions [ obtained with retrospective electrocardiographic ( ecg ) gating ] were performed with a 64 - slice ct system ( sensation 64 , siemens , forchheim , germany )  . 
per lo studio tc sono stati esclusi i pazienti con frequenza cardiaca ( fc ) > 65 battiti per minuto ( bpm ) non responsivi ai farmaci beta - bloccanti , i pazienti con fibrillazione atriale ad elevata risposta ventricolare , quelli con nota allergia ai mezzi di contrasto , con insufficienza renale e / o con compromissione della funzionalit respiratoria [ 27 ] ; per lo studio ecocardiografico , la scarsa qualit di immagine non ha rappresentato un criterio di esclusione dallo studio , in quanto la nostra intenzione stata quella di riportare i risultati desunti dalla pratica clinica di routine . 
lo studio stato approvato dal comitato etico locale e tutti i pazienti hanno fornito per iscritto il loro consenso informato . tomografia computerizzata multistrato il protocollo di scansione tc stato analogo a quello adottato in precedenti lavori volti alla valutazione della fe tramite tc [ 19 ]  . 
i pazienti con fc > 65 bpm sono stati sottoposti a trattamento beta - bloccate con somministrazione di atenololo endovena ( ev ; 5 mg ripetibile ) sotto monitoraggio della pressione arteriosa e della fc . 
tutte le acquisizioni ( gating elettrocardiografico [ ecg ] retrospettivo ) , sono state effettuate con una apparecchiatura tc 64 strati ( sensation 64 , siemens , forchheim , germania )  . 
sono stati preventivamente somministrati per via sub - linguale 0 , 3 mg di nitroderivati ( trinitrina ) e sono stati iniettati ev 100 ml di mezzo di contrasto ( mdc ) iodato ( iomeprolo , iomeron 400 , bracco spa , milano , italia ) ad una velocit di 5 ml / s , seguiti da 30 ml di soluzione salina . 
per la sincronizzazione del bolo di mdc , stata utilizzata una tecnica di bolus tracking con posizionamento di regioni di interesse ( roi ) nellaorta ascendente ( soglia + 100 hu )  . 
sui dati grezzi sono stati effettuati due tipi di retro - ricostruzioni entrambi utilizzanti un algoritmo di ricostruzione half scan con dati ottenuti dalla rotazione del tubo di 180 ( dati ottenuti da un solo ciclo cardiaco ) , un campo di vista ( fov ) ristretto allarea di interesse ed un filtro di smoothing b30f [ 28 ] : 1 . 
synchronisation with the contrast bolus was obtained with the bolus - tracking technique , with a region of interest ( roi ) placed in the ascending aorta ( threshold + 100 hu )  . all images were acquired during an inspiratory breath - hold of approximately 11 s ( 112 s )  . 
raw data were processed with two types of reconstruction , both using a half - scan algorithm with data obtained from a 180 rotation of the tube ( data from a single cardiac cycle ) , a field of view ( fov ) confined to the area of interest and a smooth b30f kernel [ 28 ] : 1 . 
the first image of the cardiac cycle ( acquired in correspondence with the r wave ) was considered to be end diastolic , whereas the image displaying the smallest lv cavity was considered to be end systolic [ 30 ]  . 
after the correct end - diastolic and endsystolic phases were identified , the endocardial and epicardial borders were traced on the end - diastolic images , and the endocardial borders were subsequently propagated to end systole with the aid of the semiautomated software . manual corrections were made where necessary . 
the most apical lv section with a visible cavity was considered to be the apex , whereas the most basal section surrounded by at least 50% of myocardium was considered to be the base [ 14 ]  . 
un operatore esperto ha analizzato in cieco tutte le immagini con il fine di calcolare la fe , il volume telediastolico ( vtd ) , il volume tele - sistolico ( vts ) , la gittata sistolica ( gs ) , e la massa del vsin , secondo i criteri pubblicati in letteratura [ 28 ]  . 
la prima immagine del ciclo cardiaco ( acquisita in corrispondenza dellonda r ) stata considerata essere tele - diastolica , mentre limmagine con la pi piccola cavit del vsin visibile stata considerata tele - sistolica [ 30 ]  . 
dopo aver individuato la corretta fase tele - diastolica e la corretta fase tele - sistolica , sono stati tracciati i contorni endocardici ed epicardici sulle immagini in tele - diastole e successivamente i contorni endocardici sono stati propagati in tele - sistole con laiuto del software semi - automatico ; correzioni manuali sono state effettuate dove necessario ; i muscoli papillari e la trabecolatura subendocardica sono stati inclusi nella cavit del vsin [ 3133 ]  . la sezione pi apicale del vsin con cavit visibile stata considerata essere lapice , mentre la sezione pi basale circondata da almeno il 50% di miocardio stata considerata essere la base [ 14 ]  . 
il vtd ed il vts sono stati calcolati con la regola di simpson . ecocardiografia tutte le scansioni sono state effettuate in decubito laterale sinistro , utilizzando una sonda da 3 mhz collegata ad un apparecchio ecografico ie33 ( philips medical systems , andover , ma , usa )  . 
le immagini sono state acquisite rispettando le proiezioni apicali e para - sternali standard secondo le linee guida raccomandate dalla societ americana di ecocardiografia [ 34 , 35 ]  . 
dopo aver tracciato manualmente i bordi endocardici nella proiezione due camere e quattro camere in tele - diastole ed in tele - sistole , includendo i muscoli papillari nella cavit del vsin , il software implementato nellecografo ha automaticamente diviso il vsin in radiol med ( 2010 ) 115 : 10151027 1019 fig . 
a schermata utilizzata per la definizione dei contorni endocardici ed epicardici ; b schermata in cui vengono visualizzati i risultati . echocardiography all scans were obtained with the patient in left - lateral decubitus and using a 3 - mhz transducer connected to an ie33 ultrasound system ( philips medical systems , andover , ma , usa )  . 
all evaluations were done by an expert cardiologist unaware of the msct results . statistical analysis after evaluating the overall data , we divided our patient population into three subgroups : ( 1 ) ef < 35% , ( 2 ) ef 35%50% and ( 3 ) ef > 50% [ 20 ]  . 
tutti i dati sono stati analizzati mediante test t di student per dati appaiati , test di correlazione lineare ( r ) e test di bland - altman . risultati nella nostra popolazione formata da 450 pazienti , 284 uomini e 166 donne , sono stati somministrati beta - bloccanti per via endovenosa nell83 , 5% dei pazienti ( 376 / 450 )  . la fe misurata con tc stata 52%15% , quella misurata con ecc stata 55%13% ( p < 0 , 05 )  . 
il bias si dimostrato differente nei diversi sotto - gruppi ed in particolare nei pazienti con fe > 50% stato del 4 , 2% , nei pazienti con 35% < fe < 50% stato del 17 , 3% mentre nei pazienti con fe < 35% stato del 32 , 5 . 1020 radiol med ( 2010 ) 115 : 10151027 fig . 
the bias proved to vary across subgroups and , in particular , it was 4.2% in patients with ef > 50% , 17.3% in patients with ef 35%50% and 32.5% in patients with ef < 35% . discussion ef is an important parameter for establishing diagnosis , prognosis and treatment of patients with cardiovascular disease . 
in particular , the mortality rate of postinfarction patients with nonischaemic heart disease , ventricular arrhythmia and valve disorders was found to be inversely correlated with ef [ 3640 ]  . 
ecc has been used to evaluate lv function for decades , and discussione la fe rappresenta un parametro importante per linquadramento diagnostico , prognostico e terapeutico del paziente con malattie cardio - vascolari ; numerosi studi ne hanno evidenziato il valore prognostico in differenti tipologie di pazienti affetti da patologie cardiache ; in particolare la mortalit dei pazienti post - infartuati , con cardiomiopatie non - ischemiche , con aritmie ventricolari e disordini valvolari risultata essere inversamente correlata alla fe [ 3640 ]  . 
per decenni la funzione del vsin stata valutata con lecc , e le misurazioni hanno spesso risentito di campi di vista non adeguati , di un non corretto allineamento al maggior asse cardiaco ( foreshortening ) e di assunzioni geometriche che sono risultate spesso inadeguate in particolare nei pazienti con anomalie segmentarie della cinesi ventricolare come i pazienti con sospetta malattia coronarica . 
thanks to recent technological advances , ct has proved to produce optimal images for visualising the coronary tree while providing data sets allowing volumetric analysis of lv function , without geometrical assumptions and without the need to expose patients to a further dose of ionising radiation and / or iodinated contrast material . 
ct images , characterised by high definition of endocardial contours , have allowed for marked reduction in intraand interobserver variability in ef evaluation [ 41 ]  . this paper reports on our real - world experience in comparing ef values calculated with ct and ecc in a large patient population . 
this could be easily explained by the different temporal resolution of the two techniques , and in particular , by the possibility that the lower temporal resolution of ct does not capture iodato ; le immagini tc , dotate di una elevata definizione dei bordi endocardici , hanno dimostrato una variabilit intraed inter - osservatore notevolmente ridotta nella valutazione della fe [ 41 ]  . 
in particular , in patients with ef < 35% and those with ef 3550% , ecc markedly overestimated ef with a bias directly proportional to the degree of systolic dysfunction . 
our opinion appears to be supported by the concordance values obtained in the group particolare nei pazienti con fe < 35% ed in quelli con 35% < fe < 50% lecc ha nettamente sovrastimato la fe con un bias direttamente proporzionale al grado di disfunzione sistolica ; la sovrastima della fe non stata mantenuta nei pazienti con fe > 50% , come ci saremmo aspettati . 
crediamo che alla base della discordanza rilevata tra le due metodiche ci siano le assunzioni geometriche utilizzate necessariamente in ecc per calcolare la fe ; ci potrebbe essere stato particolarmente influente nella nostra popolazione formata da pazienti con sospetta malattia coronarica e con anomalie segmentarie della cinesi parietale . 
la nostra tesi sembrerebbe avvalorata anche dai valori di concordanza riscontrati nel gruppo di pazienti con fe > 50% ; in questo gruppo di persone , con fe praticamente normale , verosimile che le misurazioni ecc non abbiano risentito dei difetti segmentari della cinesi parietale ; la fe misurata con ecc risultata essere lievemente pi bassa rispetto alla tc , molto probabilmente a causa delle conosciute problematiche relative al foreshortening cui questa metodica soggetta , con un bias di appena 4 , 2% , valore peraltro accettabile nella radiol med ( 2010 ) 115 : 10151027 1023 fig . 
3 box - and - whisker plot shows median ( middle line ) , lower and upper quartile ( 25 and 75 percentile ; main box ) and minimum and maximum values ( extended lines ) for ejection fraction . 
an outside value is defined as a value smaller than the lower quartile minus 1.5 times the interquartile range or larger than the upper quartile plus 1.5 times the interquartile range ( inner fences )  . 
a far out value is defined as a value smaller than the lower quartile minus 3 times the interquartile range or larger than the upper quartile plus 3 times the interquartile range ( outer fences )  . 
3 il grafico box - and - whiskers mostra la mediana ( linea di mezzo ) , il quartile inferiore e superiore ( 25 e 75 percentile ; box principale ) , ed il minimo e massimo ( linee estese ) per la frazione di eiezione . 
un valore outside definito come pi piccolo del quartile inferiore meno 1 , 5 volte il range interquartile , o maggiore del quartile superiore pi 1 , 5 volte il range interquartile ( marcatori quadrati )  . 
un valore far out definite come pi piccolo del quartile inferiore meno tre volte il range interquartile , o maggiore del quartile superiore pi tre volte il range interquartile ( marcatori rotondi )  . 
ef , ejection fraction ; edv , end - diastolic volume ; esv , end - systolic volume ; ct , computed tomography ; ecc , ecocardiography . of patients with ef > 50% . 
ef measured with ecc was only slightly lower compared with ct , most probably because of the known foreshortening problems this technique is prone to , with a bias of only 4.2% , which is acceptable in routine clinical practice . although other studies comparing ct and ecc considered only a small number of patients and were thus unable to carry out any subanalyses , their findings agree with ours in that ecc overestimated ef compared with ct and mri in their study populations consisting of patients with a mean ef < 50% [ 12 , 14 ]  . 
altri lavori scientifici volti a confrontare tc ed ecc hanno esaminato soltanto un numero ristretto di pazienti , senza avere quindi la possibilit di effettuare una sub - analisi , ma tuttavia concordano con noi nellevidenziare una sovrastima della fe da parte dellecc rispetto alla tc ed alla rm nelle loro popolazioni formate da pazienti con una media di fe < 50% [ 12 , 14 ]  . 
tuttavia , anche se i nostri pazienti hanno eseguito lecc dopo la tc , dobbiamo precisare che in base alla fc prima dellesame tc , abbiamo pi o farmaci beta - bloccanti ev che meno somministrato possono in qualche modo aver provocato valori discordanti nella misurazione della fe rispetto alle misurazioni effettuate con lecc . 1024 radiol med ( 2010 ) 115 : 10151027 fig . 
4 bland - altman plot of lvef from the comparison between computed tomography and echocardiography ; the analysis was done with 1.96 sd limits of agreement for the overall population and for subgroups with ef < 35% , 3550% and > 50% . 
analisi di bland - altman della frazione di eiezione risultante dal calcolo dei volumi del ventricolo sinistro con tc ed ecc ; lanalisi stata effettuata utilizzando dei limiti di concordanza di 1 , 96 ds ed analizzando sia la popolazione generale , sia i sotto - gruppi di pazienti divisi in fe < 35% , 35% < fe < 50% e fe > 50% . 
ejection fraction , frazione di eiezione ; ef , frazione di eiezione ; sd , deviazione standard . on their hr before the ct scan , they either received or did not receive intravenously administered beta - blockers , which may have caused discordant results in ecc determinations of ef . prospettive cliniche clinical perspective in light of the appropriateness criteria that rate as uncertain the use of ct for evaluating lv function , our data may further reinforce the fact that ecc is not always capable of providing an adequate determination of the ef [ 42 ]  . 
this limitation of ecc becomes more marked as lv function progressively deteriorates . limiti i nostri dati , alla luce delle correnti linee guida di appropriatezza che definiscono come incerto lutilizzo della tc per la valutazione della performance del ventricolo sinistro , possono rinforzare il fatto che lecocardiografia non ha sempre la capacit di definire adeguatamente la frazione di eiezione [ 42 ]  . 
questo limite della metodica ecc si accentua con la progressiva riduzione della funzionalit ventricolare sinistra . limitations we did not analyse intraand interobserver variability , as non abbiamo analizzato la variabilit intraed inter - osservatore , in quanto era oltre lo scopo del nostro studio dal momento che volevamo riportare la nostra esperienza desunta dalla pratica clinica di routine . 
non abbiamo radiol med ( 2010 ) 115 : 10151027 1025 this was beyond the scope of our study , the aim of which was to report our experience in routine clinical practice . 
however , in a recent paper , we demonstrated that in patients with suspected coronary disease , ct can provide ef values that are highly concordant with those provided by mri ( bias < 1% ) [ 19 ]  . 
finally , use of intravenously administered betablockers during ct examination may have affected the discrepancies noted between the two techniques . utilizzato un gold standard per la validazione della fe in quanto la maggior parte dei nostri pazienti non aveva indicazioni allesecuzione di una rm ; pur tuttavia , in un recente lavoro scientifico , abbiamo dimostrato che nei pazienti con sospetta malattia coronarica , la tc in grado di fornire valori di fe altamente concordanti con quelli forniti dalla rm ( bias < 1% ) [ 19 ]  . 
lutilizzo dei beta - bloccanti per via endovenosa durante lesame tc potrebbe condizionare la discrepanza osservata tra le due metodiche . conclusioni conclusions in a real - world setting , ecc provides ef values that differ significantly from those provided by ct in patients with ef < 50% , with a bias directly proportional to the degree of systolic dysfunction . 
centonze , dipartimento di radiodiagnostica , apss di trento , l.go medaglie doro , 38100 trento , italy , tel . : + 39 - 0461 - 903502 , fax : + 39 - 0461 - 903501 , e - mail : maurizio.centonze@apss.tn.it received : 20 july 2009 / accepted : 27 november 2009 / published online : 17 september 2010 springer - verlag 2010 abstract with the aim of providing a clearer understanding of the tools used for evaluating risk in the radiological setting and how they are applied , this second part presents two practical examples . 
the first is a proactive analysis applied to ct , whereas the second is a reactive analysis performed following a sentinel event triggered by a ct study allocated to the wrong patient in the ris - pacs system . riassunto al fine di una pi chiara comprensione dellapplicazione delle modalit e degli strumenti di valutazione del rischio in ambito radiologico , in questa seconda parte vengono descritti due esempi pratici : il primo costituito da unanalisi proattiva applicata alla procedura della tc , il secondo da unanalisi reattiva effettuata dopo un evento sentinella , scatenato da unindagine tc erroneamente attribuita nel sistema ris - pacs . keywords radiology error clinical risk management parole chiave radiologia errore gestione del rischio clinico example of proactive analysis : risk assessment in ct esempio di analisi proattiva : la valutazione del rischio in tc proactive analysis aims at identifying and eliminating critical features of the system before an incident occurs and scrutinising activities that constitute a process . 
in radiology , this analysis aims to identify risks linked to the diagnostic process and , in particular , to provide information for their evaluation , lanalisi proattiva mira allindividuazione ed eliminazione delle criticit del sistema prima che lincidente si verifichi ed basata sulla disanima delle attivit che costituiscono un processo , con lobiettivo finale di progettare sistemi sicuri [ 1 , 2 ]  . 
in campo radiologico , tale analisi ha lo scopo di 1148 radiol med ( 2010 ) 115 : 11471164 illustrate methods and instruments for the description of organisational processes capable of preventing risks linked to the diagnostic process and lastly to guarantee elements for effective risk management by adopting improvements . 
the ultimate aim is to create an organisation capable of taking preventative decisions to lower the level of risk and therefore minimise the probability of error and maximise the possibility of intercepting error before it occurs , thus improving the knowledge and individual training of each professional . 
the proactive technique can be successful and effective only when the complex organisation considers the recommendations provided by the working group analysing the processes . the final aim is patient safety in healthcare , and for this to be achieved , the various professional figures need to be appropriately trained and their professional expertise synergistically coordinated . 
 at the department of diagnostic radiology in treviso , a proactive analysis of the risks associated with the ct process was carried out in the framework of a multicentre risk management project involving four other radiology departments ( como , rome , naples and catania ) , called project iradar : analysis of the ct process and results . the aim of the project was to identify risks associated with managing all phases ( activities ) of the ct process , to perform measurements and therefore implement prevention and control actions . 
the study began with risk analysis in elective contrast - enhanced ct examinations and attempted to identify the possible problems that could arise throughout the process : administrative ( booking , information ) , radiation protection , pharmacological ( allergy , consent , etc . ) ; use of dedicated techniques vs standardisable techniques ( ct urography , ct colonography , etc . ) ; high volume of images to be analysed , reproduced and archived ; numerous postprocessing options ; need for comparison with previous ct studies ; report writing . the analysis then took into account the participants and the definition of their roles , with the involvement of a representative for each professional figure involved in the ct examination : a radiologist , a radiology technician , a professional nurse and an administrator . 
 the instrument used for the proactive analysis was failure mode and effect analysis ( fmea ) , a qualitative technique that aims at prospectively determining possible failures and their effects on the stability of the entire system , with the aim of redesigning the process itself . 
in detail , the individuare i rischi legati al processo di diagnosi e , in particolare , fornire conoscenze per la loro valutazione , illustrare metodi e strumenti per la descrizione dei processi organizzativi per la prevenzione dei rischi legati allattivit diagnostica e , infine , garantire elementi per una gestione efficace del rischio con ladozione di azioni di miglioramento . 
il fine ultimo quello di creare unorganizzazione in grado di assumere preventivamente decisioni per abbassare il livello di rischio e , quindi , minimizzare la probabilit di errore e massimizzare la possibilit di intercettarlo prima che questo accada , migliorando la conoscenza e la formazione individuale di ogni figura professionale . 
 presso lunit operativa ( uo ) di radiologia diagnostica di treviso stata effettuata unanalisi proattiva dei rischi connessi al processo tc nellambito di un progetto multicentrico di risk management con altre quattro uo di radiologia ( como , roma , napoli e catania ) , denominato progetto iradar : analisi del processo tc e risultati . 
scopo del progetto stato quello di identificare i rischi legati alla gestione di tutte le fasi ( attivit ) del processo tc , di effettuarne la misurazione e , quindi , di impostare azioni di prevenzione e controllo . 
il lavoro iniziato con lanalisi del rischio per esami tc con somministrazione di mezzo di contrasto eseguiti in elezione , cercando di rilevare le possibili problematiche che si potevano riscontrare nellintero processo : amministrative ( prenotazione , informazione ) ; radioprotezionistiche ; farmacologiche ( allergia , consenso , ecc . ) ; utilizzo di tecniche dedicate vs . 
tecniche standardizzabili ( uro - tc , colon - tc , ecc . ) ; elevato volume di immagini da analizzare , riprodurre e archiviare ; ampie possibilit di elaborazione ; necessit di confronto con tc precedenti ; formulazione del referto ( comunicazione )  . 
si passati quindi allindividuazione dei partecipanti ed alla definizione del loro ruolo , coinvolgendo un rappresentante per ciascuna figura professionale implicata nellindagine tc : un radiologo , un tecnico sanitario di radiologia medica ( tsrm ) , un infermiere professionale e un amministrativo . 
 lo strumento utilizzato per lanalisi proattiva stato la failure mode and effect analysis ( fmea , analisi dei modi e degli effetti dei guasti ) , una tecnica qualitativa che mira a determinare prospetticamente i possibili inconvenienti e i radiol med ( 2010 ) 115 : 11471164 1149 probability of occurrence and severity of the error that may derive from the critical event ( to the patient , to an operator or to the organisation ) and the possibility of detecting its occurrence with specific instruments or by direct observation was calculated for each critical event . 
fmea and failure mode and effect criticality analysis ( fmeca ) ( see part i ) are strategies developed for identifying the potential errors of a product / process , evaluating the associated risk and assigning a value in terms of importance . 
fmea was developed by the us armed forces in 1949 to classify faults on the basis of their impact on the success of a mission and the safety of personnel and equipment . 
subsequently , it was applied in the 1960s for the apollo space missions , whereas in the 1980s it was used by the ford motor company to reduce the risks of motor vehicle breakdowns . 
then , the failures of each building block are identifying a series of basic data : analysed by object / subject of the process , its function , deficit of the object / subject , cause and effect of the deficit , control measures in place , list of all possible failure modes , and for each of them , all possible causes , all possible effects and all possible control measures . 
in order to determine the pri , three characteristics are needed : p ( probability of the event occurring ) , s ( severity of the event ) , r ( possibility of detecting critical aspects or identifying the failure through controls before the event has produced its negative effects )  . actions to improve the product , process or system should be oriented mainly on the failure modes that have the highest pri values . 
 the fmea process , therefore , has the following steps : create an evaluation team generate the fundamental rules obtain and analyse the relevant information identify the objects / subjects or processes to be analysed and for each analyse the function , the error , the cause of the error and the controls in place evaluate the risk associated with the error define the priorities and assign the corrective actions distribute , review and update the analysis , if considered appropriate . fmea / fmeca is relatively simple and requires limited training . 
in addition , it is an easy method to loro effetti sulla stabilit dellintero sistema , con lo scopo di ridisegnare il processo stesso , cui si aggiunge unanalisi quantitativa per stimare il livello di criticit degli inconvenienti individuati , attribuendo loro un indice , volto a facilitare lassunzione di decisioni coerenti . 
pi nel dettaglio , per ogni evento critico stato calcolato il livello di probabilit di insorgenza e di gravit dellerrore che ne poteva derivare ( al paziente , ad un operatore o allorganizzazione ) e la possibilit di rilevare , attraverso strumenti specifici o losservazione diretta , la sua comparsa . 
la fmea e la failure mode and effect criticality analysis ( fmeca ) ( vedi parte i ) sono strategie sviluppate per identificare potenziali errori di un prodotto / processo , valutandone il rischio associato e assegnandone un valore in termini di importanza , al fine di condurre azioni correttive per affrontare i problemi pi seri . 
la fmea fu sviluppata dalle forze armate statunitensi nel 1949 , allo scopo di classificare i guasti in base allimpatto sul successo di una missione e sulla sicurezza del personale e degli equipaggiamenti . 
successivamente , nellanalisi dei guasti di ogni sottosistema , occorre identificare una serie di informazioni base : oggetto / soggetto del processo , sua funzione , deficit delloggetto / soggetto , causa ed effetto del deficit , controlli in atto , elencazione di tutti i possibili modi di guasto , per ciascuno di essi tutte le possibili cause , tutti i possibili effetti e tutti i controlli in essere . 
il rischio associato ad ogni terna viene quantificato attraverso un indice di priorit del rischio ( ipr = pgr ) ; per determinare lipr necessario conoscere tre caratteristiche : p ( probabilit di accadimento dellevento ) , g ( gravit associata al verificarsi dellevento ) , r ( possibilit di rilevare lesistenza della criticit o di individuare il guasto da parte dei controlli prima che levento abbia determinato il suo effetto negativo )  . le azioni di miglioramento del prodotto , processo o sistema dovranno essere orientate principalmente sui modi di guasto che presentano i pi alti valori di ipr . 
la fmea pu essere poi ripetuta a seguito delle azioni migliorative , per verificare se i valori di ipr sono diminuiti [ 4 ]  . un processo fmea procede , quindi , secondo i seguenti steps : creare il team valutatore ; generare le regole di base ; ottenere ed analizzare le informazioni rilevanti ; identificare gli oggetti / soggetti o i processi da analizzare e 1150 radiol med ( 2010 ) 115 : 11471164 fig . 
1 esempio di analisi proattiva in radiologia : scomposizione del processo in fasi e loro analisi . understand , it is very flexible and can be used to evaluate the active errors of both the individual operators and the work team and it enables identification of latent errors correlated with management choices and decisions . 
the analysis of the event according to a cognitive ( active errors ) and sociotechnical ( organisational ) approach does not aim at identifying individual liability ( negligence , lack of expertise , carelessness )  . in the diagnostic radiology department in treviso , the analysis technique was applied for 3 months . 
it was initiated by jointly reconstructing the usual process for carrying out a ct examination , by classifying the various sequences and identifying the responsibilities of the professional figures involved in each activity . 
micro - process a : booking and admission activity : receiving and evaluating the request activity : recording on the information system activity : patient history and clinical information regarding the examination activity : informed consent and information regarding its signature activity : premedication protocol in the case of activity : handing in of examination booking docuknown allergies ments 2 . 
micro - process b : organising activities activity : preparing documents : work list for the radiology suite ; di ognuno di essi analizzare la funzione , lerrore , la causa dellerrore ed i controlli in atto ; valutare il rischio associato allerrore ; definire le priorit ed assegnare le azioni correttive ; distribuire , rivedere ed aggiornare lanalisi , se ritenuto appropriato . un processo fmea / fmeca relativamente semplice e richiede un training limitato . 
inoltre , un metodo facile da capire e molto flessibile , utilizzabile per valutare gli errori attivi sia dei singoli operatori sia dei team di lavoro , e consente di individuare gli errori latenti correlati alle scelte e alle decisioni del management . 
inoltre , pu essere facilmente applicato a tutto il processo di lavoro o a parti selezionate . lanalisi dellevento secondo un approccio cognitivo ( errori attivi ) e socio - tecnico ( organizzazione ) non ha il carattere inquisitorio , mirato alla ricerca delle responsabilit del singolo ( negligenza , imperizia , imprudenza )  . nellesperienza delluo di radiologia diagnostica di treviso , lanalisi , applicata per un periodo di tre mesi , iniziata con la ricostruzione collegiale della modalit abituale di svolgimento delliter degli esami tc , con la classificazione delle varie sequenze e con lindividuazione delle diverse responsabilit professionali coinvolte per ciascuna attivit . 
micro - processo a : prenotazione ed accettazione : attivit : ricevimento della richiesta e sua valutazione ; attivit : registrazione sul sistema informatico ; attivit : informazioni clinico - anamnestiche sullindaattivit : consenso informato ed informazioni sulla gine ; sottoscrizione ; radiol med ( 2010 ) 115 : 11471164 1151 inpatient examination requests and faxes received attivit : protocollo di premedicazione in caso di ( outpatients bring the requests themselves ) ; allergie note ; labels bearing first name , surname and personal details , user + booking number , type and date of examination ; activity : preparing the patient for the examination ( performing laboratory workup , preparing in the event of known allergies ) 3 . 
micro - process c : greeting patient and preparation phase of the examination activity : verifying required documents ( request and informed consent dated and signed by the referring physician and patient , laboratory examinations requested , previous examinations or clinical tests pertaining to the diagnostic query ) ; medical records must be available for inpatients activity : verifying patient conditions ( observance of the required preparation : fasting , premedication protocol in the case of known allergies ) activity : verifying pregnancy status in reproductiveage women 4 . 
micro - process d : preparing the diagnostic session activity : finding a vein for administration of contrast material or in the case of inpatients already with needle inserted verifying its diameter and patency activity : in the case of creatinine levels above normal , intravenous hydration with saline solution before and after the examination attivit : consegna documenti prenotazione esame ; 2 . 
micro - processo b : organizzazione delle attivit : attivit : preparazione documenti : lista di lavoro per sala ; richieste dei pazienti ricoverati e fax pervenuti ( se esterno le impegnative vengono portate direttamente dal paziente ) ; etichette che riportano : nome , cognome e dati anagrafici utente + numero di prenotazione , tipo e data dellesame ; attivit : preparazione paziente allindagine ( esecuzione esami di laboratorio , eventuale preparazione in caso di allergie note ) ; 3 . 
micro - processo c : accoglimento paziente e fase di preparazione dellindagine : attivit : verifica documenti necessari ( impegnativa e consenso informato , datato e firmato da medico richiedente e paziente , esami di laboratorio richiesti , indagini di esami precedenti o esami clinici attinenti al quesito diagnostico )  . 
per i pazienti interni deve essere disponibile la cartella clinica : attivit : verifica condizioni del paziente ( rispetto delle modalit di preparazione previste : digiuno , protocollo di pre - medicazione in caso di allergie note ) ; attivit : verifica delleventuale stato di gravidanza per le donne in et fertile ; activity : replacing the infusion set for each patient 4 . 
micro - processo e : seduta diagnostica : attivit : collegamento deflussore allago e preparazione per somministrazione del mdc ; attivit : informazione al paziente sulle sensazioni images on film / cd for the patient durante la somministrazione ; for each micro - process , we defined what could go wrong , possible causes of critical events and possible effects . 
we then quantified them according to severity , probability and detectability by estimating the risk of severity and probability of error that could be caused to the patient , an operator or the organisation , as well as estimating the possibility of detecting an error before it causes negative effects . the activities with the highest pri values were the following : attivit : avvio indagine radiologica come da protocolli specifici ; 6 . 
micro - processo f : validazione seduta diagnostica e chiusura : attivit : informazioni al paziente sulle modalit da adottare in caso di reazione tardiva al mdc ; attivit : invio immagini al pacs e stampa immagini su pellicola / cd per il paziente . per ogni micro - processo stato definito cosa poteva non funzionare , le cause dellinsorgenza degli eventi critici ed i 1152 radiol med ( 2010 ) 115 : 11471164 1 . 
in micro - process a : preliminary information provided at the time of booking ( incomplete information with the risk of developing allergic reactions , pri : 192 )  . 
in micro - process f : sending images to the pacs ( use of a different accession number between performing and reporting the examination , pri ; 108 )  . no activities with a significant pri value were identified in micro - process c . in light of the results , improvement projects were implemented aimed at changing behaviour patterns and activities with an associated high pri level . 
the ultimate aim is to plan and manage an organisation able to reduce the probability of errors occurring , whether they be conscious ( for example , due to stress and excessive workload ) or unconscious , and therefore unperceived , errors . example of reactive analysis : root - cause analysis of a sentinel event , considerations and provisions adopted 1 . 
description of the event [ 5 ] on 5 july 2007 , a 54 - year - old patient ( dl ) attended the casualty ward of a university teaching hospital complaining of left low back pa an ultrasound ( us ) study was performed that revealed the presence of a slight dilatation of the left ureter and a 13 - mm renal angiomyolipoma . 
on 13 august 2007 , the treating physician referred dl to the radiology department of the university teaching hospital to perform a ct urography with the diagnostic query of suspected renal tumour ( critical element upstream of the event : inappropriate request )  . 
the next day , on 14 august , an 86 - year - old female patient ( tl ) having surname homonymy with dl and affected by tumour of the prevesical segment of the left ureter with consequent grade iiiiv hydroureteronephrosis underwent ct urography . 
on this occasion , the images were also possibili effetti , quantificandoli per gravit , probabilit e rilevabilit , effettuando la stima del rischio di gravit e di probabilit dellerrore che poteva derivare al paziente , ad un operatore o allorganizzazione nonch la stima della possibilit di evidenziare laccadimento di un errore prima che questo causi i suoi effetti negativi . le attivit con maggior valore ipr sono risultate : 1 . 
nel micro - processo a , le informazioni preliminari fornite allatto della prenotazione ( informazioni incomplete con rischio di sviluppo di fenomeni allergici , ipr : 192 ) ; 2 . 
nel micro - processo d , la preparazione della siringa di mdc ( reflusso di mdc nella soluzione fisiologica con rischio di contaminazioni , ipr : 108 ) ; 4 . 
 non sono state individuate attivit con valore di ipr significativo nel micro - processo c . alla luce di tali risultati sono stati messi in atto dei progetti di miglioramento atti a modificare comportamenti e attivit dove si individuato un elevato ipr , cercando di progettare e gestire unorganizzazione in grado di ridurre la probabilit che si verifichino errori , sia consapevoli ( dovuti , ad esempio , a stress e a carichi di lavoro elevati ) che inconsapevoli , quindi non percepiti . esempio di analisi reattiva : root cause analysis di un evento sentinella , riflessioni e provvedimenti adottati 1 . 
descrizione dellevento [ 5 ] il 5 luglio 2007 , una paziente ( dl ) di 54 anni , si recava al pronto soccorso di unazienda ospedaliero - universitaria , lamentando una lombalgia sinistra per la quale veniva eseguita unindagine ecografica che dimostrava la presenza di lieve dilatazione delluretere sinistro e di angiomiolipoma renale di 13 mm , rilievi confermati alcune settimane dopo da una seconda ecografia , effettuata in un ospedale privato . 
il 13 agosto 2007 , su richiesta del medico di medicina generale con il quesito diagnostico di sospetta neoplasia renale , dl veniva sottoposta presso la radiologia dellazienda ospedaliero - universitaria ad esame uro - tc ( elemento critico a monte dellevento : inappropriatezza della richiesta ) : al termine dellindagine al doppio server del sistema ris - pacs veniva inviato automaticamente lintero studio . 
il giorno successivo , il 14 agosto , veniva sottoposta radiol med ( 2010 ) 115 : 11471164 1153 automatically sent to the dual server of the ris - pacs at the end of the examination , although they were incorrectly allocated to patient dl studied the day before ( first critical element )  . 
this error was made because dls name still appeared in the work list of the ct console , in the line adjacent to that of tl ( second critical element : system deficiency )  . 
the error was immediately identified and corrected by the radiology technician , x : patient details and id of patient dl were corrected in the details of tl , and the entire study with the correct data was sent to the ris - pacs . 
shortly thereafter , the radiology technician intervened on the two servers of the pacs with the intention of eliminating the images incorrectly allocated to patient dl from the server of the pacs accessible from the radiology department and which sends the images to the robot for cd burning the sequence of images corresponding to the real examination of patient dl was cancelled : only the images of patient tl remained ( third critical element )  . 
on the second web server , which sends the images to all workstations situated in the various hospital departments for clinician consultation , sequence of incorrect images was instead correctly cancelled and the real images of patient dl remained available . 
also on 17 august , 4 days after it had been performed ( fifth critical element ) : if the report had been made on the same day the examination was performed , the chain of errors would have been broken because the cancellation of the images by radiology technician x . 
the same findings were recorded in the report ( grade iii left hydroureteronephrosis resulting from neoplastic stenosis of the distal ureter protruding into the bladder , with a proposed exploratory cystoscopy / ureteroscopy )  . 
the images from the us study performed previously and in disagreement with the ct findings were not available for visualisation in the ris - pacs ( sixth critical element )  . 
when the report was collected , patient dl was also given the cd containing the incorrect images . patient dl then underwent cystoscopy / ureteroscopy by ad uro - tc la paziente di sesso femminile tl di 86 anni ( omonima per cognome rispetto alla paziente dl ) , affetta da neoplasia del segmento pre - vescicale delluretere sinistro con conseguente idro - ureteronefrosi di iii - iv grado . 
anche in questo caso , al termine dellesame le immagini vennero inviate automaticamente al doppio server del pacs , ma attribuite erroneamente alla paziente dl , studiata il giorno precedente ( 1 elemento critico )  . 
tale errore fu effettuato poich il nominativo dl compariva ancora nellelenco della worklist della consolle della tc , nella riga adiacente a quella della paziente tl ( 2 elemento critico : deficienza del sistema )  . 
x : sulla consolle della tc i dati anagrafici e lidentificativo ( id ) della paziente dl furono corretti in tl e lintero studio con i dati corretti venne inviato al ris - pacs . 
poco dopo il tsrm sig . x intervenne sui due server del pacs con lintento di eliminare le immagini attribuite erroneamente alla paziente dl . dal server del pacs consultabile dalla radiologia ed inviante le immagini ai robot per la masterizzazione dei cd fu cancellata la sequenza di immagini corrispondente al vero esame della paziente dl : rimasero quindi solo le immagini della paziente tl ( 3 elemento critico )  . 
sul secondo server , quello web , che invia le immagini a tutte le postazioni situate nei vari reparti ospedalieri per la consultazione da parte dei clinici , venne invece correttamente effettuata la cancellazione della sequenza di immagini sbagliate e restarono disponibili le vere immagini della paziente dl . 
a sempre il 17 agosto , 4 giorni dopo la sua esecuzione ( 5 elemento critico ) : se la refertazione fosse avvenuta nello stesso giorno dellesecuzione la cascata degli errori si sarebbe interrotta poich la cancellazione delle immagini da parte del tsrm sig . 
sul referto venivano effettuati i medesimi rilievi ( quadro di vistosa idro - ureteronefrosi sinistra di iii grado per stenosi neoplastica delluretere distale aggettante in vescica , con consiglio di effettuare cisto - ureteroscopia di approfondimento )  . 
b , considerato pi esperto in uro - radiologia : questultimo non si rese conto che il caso che gli veniva sottoposto possedeva le medesime 1154 radiol med ( 2010 ) 115 : 11471164 procedure performing the same urologists who later operated on her : given the macroscopic negativity of the endoscopic findings , the considered the urologist ureteroscopy unnecessary . 
the disagreement between the ct findings ( positive ) and the cystoscopy and us findings ( negative ) prompted the urologist to send a colleague to the radiology department to verify the images contained on the cd and to request radiological consultation . 
the consultation was provided by the radiologist on duty during that shift , c . , who verified the presence of disease and the disagreement between the positive ct findings and those of the other negative diagnostic techniques ( seventh critical element )  . 
during the procedure , performed with the laparoscopic approach , after having clamped and sectioned the renal vessels , the urologist realised the discrepancy between the nonpathological kidney and the dilatation of the ureter as it appeared on the ct images contained on the cd ( the only technique evaluated in the preoperative phase )  . 
he then searched for the case on the web system and for the first time visualised the correct images , which showed a totally different condition from the one present on the cd , with substantially normal renal findings . 
analysis of the event the proactive method , reactive analysis unlike performed a posteriori , starting from the adverse event and performing reverse reconstruction of the sequence of facts and elements with the aim of identifying all the factors ( critical elements ) that caused or at least contributed to the event itself [ 4 ]  . 
in the specific case , after having identified a working group that included those who were directly involved in the sentinel event , the information necessary for understanding the event was gathered . 
in the second phase , an open discussion was held within the working group that highlighted all the factors that contributed to the sentinel event , and a caratteristiche di quello da lui refertato poco prima ( paziente tl )  . 
la paziente dl fu quindi sottoposta a cisto - ureteroscopia dagli stessi urologi che in seguito la operarono : in considerazione della macroscopica negativit del quadro endoscopico , lurologo esecutore ritenne di non dover effettuare lureteroscopia . 
la discordanza tra i reperti tc ( positivi ) , cistoscopici ed ecografici ( negativi ) , indusse lurologo ad inviare un collega in radiologia per verificare le immagini contenute nel cd e per richiedere una consulenza radiologica . 
durante lintervento , eseguito per via laparoscopica , dopo avere clampato e sezionato i vasi renali , lurologo si rese conto della discrepanza del quadro renale non patologico , con assente dilatazione delluretere ( che invece appariva nelle immagini tc contenute nel cd , unica metodica valutata in fase preoperatoria ) e ricerc sul sistema web il caso , visualizzando per la prima volta le immagini corrette e rinvenendo una condizione totalmente diversa da quella presente sul cd , con una sostanziale normalit dei reperti renali . 
analisi dellevento diversamente dal metodo proattivo , lanalisi reattiva viene effettuata a posteriori , partendo dallevento avverso e ricostruendo a ritroso la sequenza di fatti ed avvenimenti , al fine di identificare tutti i fattori ( elementi critici ) che hanno causato o quantomeno contribuito al verificarsi dellevento stesso [ 4 ]  . 
nel caso specifico , dopo aver identificato un gruppo di lavoro , che comprendeva anche coloro che furono direttamente coinvolti nellevento sentinella , sono state raccolte le informazioni necessarie per la sua comprensione . il gruppo di lavoro ha successivamente effettuato un sopralluogo nella sede dellincidente e rivisto le procedure e le modalit organizzative in uso . 
the diagram graphically visualises the relationships between the various factors influencing the event , identifies the causal areas of a phenomenoneffect and specifies the possible causes , ordered according to differing levels . 
 in addition , a clinical audit was performed whereby the working group worked together with a team of experts in the radiological field with the aim of identifying the divergences from the pre - established references or standards . the critical elements of radiological interest of the sentinel event described are listed in table 1 and inserted in the ishikawa diagram in fig . 
critical element upstream linked to the appropriateness of the request ( element m ) : analysis of the sentinel event reveals a number of errors regarding the prescription of the diagnostic imaging examination . 
first , the initial us study was done to investigate left low back pa lumbar pain is not an indication for us , whereas conventional radiography of the lumbar - sacral spine may be sufficient . 
therefore , both the us and the ct urography studies were inappropriate . the term appropriateness ( in italian appropriatezza ) is becoming familiar to healthcare workers , partly because , in a number of ways , it is one of the key concepts underlying the italian national healthcare plan . 
nella seconda fase , allinterno del gruppo di lavoro stato effettuato un aperto confronto che ha messo in evidenza tutti i fattori che avevano contribuito al verificarsi dellevento sentinella con lidentificazione dei vari elementi critici . 
allo scopo di comprendere il grado di correlazione tra i vari momenti critici stato utilizzato il diagramma a spina di pesce di ishikawa , che consente di visualizzare graficamente le relazioni tra i vari fattori che hanno influito sullevento , identificando gli ambiti causali di un fenomeno - effetto e specificando le ipotetiche cause , ordinate in vari livelli . 
 a tutto ci si aggiunto un audit clinico durante il quale lquipe si confrontata con un team di esperti dellambito radiologico con lobiettivo di identificare gli scostamenti rispetto a riferimenti o standard prefissati . 
innanzitutto , la prima indagine ecografica fu eseguita per indagare una lombalgia sinistra : il dolore lombare non unindicazione allecografia mentre pu essere bastevole effettuare un esame radiografico convenzionale del rachide lombo - sacrale ; in presenza di unirradiazione sciatalgica , lesame radiografico pu essere completato con uno studio con risonanza magnetica ( rm ) del tratto lombo - sacrale . 
in base ai riscontri ecografici , anche lindagine uro - tc non era indicata : il sospetto diagnostico di angiomiolipoma di 13 mm poteva essere adeguatamente risolto con un esame tc senza mdc o con un esame rm : infatti , entrambe le metodiche presentano unelevata accuratezza diagnostica nellidentificazione del tessuto adiposo , che quello nella maggior parte dei casi pi rappresentato in questo amartoma [ 611 ]  . pertanto sia lecografia che luro - tc non erano indagini appropriate . 
il vocabolo appropriatezza sta diventando 1156 radiol med ( 2010 ) 115 : 11471164 table 1 critical elements of the radiologically relevant sentinel event upstream from the event u booking through the centralised booking service of an inappropriate examination ( deficient preliminary justification ) codeterminants of the event 1 . 
cancellation of the images of the real examination and allocation of the images of the homonymous patient in the pacs server ( but persistence of the images correctly allocated in the web server ) 4 . 
subsequent extemporaneous consultation between the clinician and a third radiologist ct , computed tomography ; pacs , picture archiving and communications system tabella 1 gli elementi critici dellevento sentinella di pertinenza radiologica a monte dellevento m . 
cancellazione delle immagini del vero esame e cambio di attribuzione alla paziente omonima nel pacs - server ( ma persistenza delle immagini con corretta attribuzione nel web - server ) 4 . 
2 diagramma di ishikawa con gli elementi critici dellevento sentinella di pertinenza radiologica.tc , tomografia computerizzata ; ris - pacs , radiology information system and picture archiving and communications system . radiol med ( 2010 ) 115 : 11471164 1157 adopted by healthcare workers at various levels , with the aim of improving the quality of healthcare provided to the general public . 
the concept of appropriateness is founded on adherence to indications based on available evidence of efficacy but also and above all of inefficacy as well as evaluation of safety and the concept of harm and benefit . 
it is therefore a measure of adherence of the healthcare system ( from each healthcare worker to departments and beyond ) to shared best practices at the local or international level [ 12 ]  . 
from the theoretical point of view , there are two types of complementary and interdependent appropriateness : ( i ) professional appropriateness ( service of proven efficacy , only applied for correct clinical indications , with a favourable harmbenefit ratio ) , and ( ii ) organisational appropriateness ( service provided with an acceptable use of resources ) [ 12 ]  . 
with regard to professional appropriateness , as with any other healthcare service , a diagnostic imaging examination should be performed only if and when it is effective and useful and provided the harm even only potential harm does not exceed the benefits . 
in this field , inappropriateness in excess ( of service provision , timing or complexity of a diagnostic service ) is undeniably more common than inappropriateness due to deficiency , which although not to be underestimated is , at least quantitatively , not as significant [ 13 ]  . 
 ( elements 1 , 2 , 3 , 6 ) : the ris - pacs system of the hospital where the sentinel event occurred is one of the most technologically advanced available on the market today , as it has a standard configuration , with regular integrating the healthcare enterprise ( ihe ) integration profiles , as well as a good interface with the diagnostic modalities . 
the system annually handles over 350 , 000 radiology examinations of varying types , originating , at the time of the event , from 47 radiological devices : five ct scanners , two mri scanners , 22 digital conventional radiographic devices , one direct radiography , nine remote - controlled devices , three positron emission tomography ( pet ) scanners and five us scanners , as well as five gamma cameras . 
the system is composed of two central servers ( a local level - one archive and a legal archive ) , which are connected to an additional server ( web ) containing the on - line memory for the previous 6 months and that allows images to be sent for consultation by clinicians in 72 wards . 
critical elements linked to the ris - pacs system familiare agli operatori della sanit , anche in considerazione del fatto che , per diversi aspetti , uno dei cardini della costituzione del piano sanitario nazionale . 
il termine entrato in uso attraverso la lingua inglese ( appropriateness ) e riassume un insieme di comportamenti che andrebbero posti in essere da parte degli operatori sanitari ai vari livelli , al fine di migliorare la qualit dellassistenza ai cittadini : per citare gli aspetti pi importanti ed evidenti , sintetizza lefficacia , lottimizzazione del rapporto costo / beneficio e la definizione delle priorit . 
il concetto di appropriatezza si fonda sulladerenza alle indicazioni basate sulle prove disponibili di efficacia ma anche , e soprattutto , di inefficacia , sulla valutazione della sicurezza , sul concetto di danno e di beneficio . 
 , quindi , una misura delladerenza del sistema sanit ( dal singolo operatore alle strutture dipartimentali ed oltre ) alle best practice condivise a livello locale o internazionale [ 12 ]  . 
da un punto di vista teorico si distinguono due tipi di appropriatezza , complementari e interdipendenti : unappropriatezza professionale ( prestazione di provata efficacia , applicata solo per le indicazioni cliniche corrette , con rapporto danno / beneficio favorevole ) ed una organizzativa ( prestazione erogata con un consumo di risorse accettabile ) [ 12 ]  . 
rispetto al concetto di appropriatezza professionale , un esame di diagnostica per immagini , come qualsiasi altra prestazione sanitaria , va erogato solo se e quando efficace , utile e qualora i danni anche solo potenziali siano superati dai vantaggi . 
in questo campo , linappropriatezza in eccesso ( di erogazione , di timing , di complessit di una prestazione diagnostica ) sicuramente assai pi frequente dellopposta ipotesi di uninappropriatezza in difetto , che se non va sottovalutata non , almeno quantitativamente , altrettanto significativa [ 13 ]  . 
elementi critici legati al sistema ris - pacs ( elementi 1 , 2 , 3 , 6 )  . il sistema ris - pacs dellospedale in cui si verificato levento sentinella uno dei pi tecnologicamente avanzati tra quelli presenti sul mercato , dotato di una configurazione standard , con regolari profili di integrazione ihe e buona interfaccia con le modalit diagnostiche . 
tale sistema gestisce annualmente oltre 350000 esami radiologici di vario tipo , provenienti , al momento dellevento , da 47 apparecchiature radiologiche ( 5 tc , 2 rm , 22 apparecchiature radiologiche tradizionali digitalizzate , 1 direct radiography , 9 apparecchiature telecomandate , 3 tomografia ad emissione di positroni [ pet ] , 5 ecografi ) oltre che da 5 gamma camere . 
il sistema si compone di due server centrali ( un archivio di primo livello e uno per la memoria legale ) che si connettono con un server aggiuntivo ( web server ) , che contiene in linea la memoria 1158 radiol med ( 2010 ) 115 : 11471164 average of 3 , 300 accesses per week . 
therefore , for inpatients , the personal data in the system come directly from the e - request of the booking ward ( first name , surname and date of birth )  . 
for outpatients , who book directly at the radiology department or through the central booking service , the personal data are inserted by the administrative personnel when the booking is made . 
 analysis of the critical organisational features led to an overall redefinition of the responsibility profiles at all levels of the ris - pacs , with the adoption of a structured and formalised quality management organisin its turn , this body adopted a new organisational model to manage the critical activities of the ris - pacs . 
in particular , radiology technicians were identified who , after receiving special training , are now exclusively dedicated to all of the more critical and delicate operations ( correction of patient identity details , accession numbers , incorrect allocation of images , notifications by the clinical departments , etc . ) in a separate and protected environment , placed in close proximity to the ris - pacs system administrator . 
all examinations subject to correction on the pacs server ( personal details , changes to allocations , etc . ) are now highlighted by the appearance of an automatic marker ( post - it ) that alerts the radiologist during the reporting phase . 
in addition , each notification of an allocation error , after its correction , is recorded as a near miss in the incident report forthe overall analysis of the ris - pacs with respect to the sentinel event also emphasised the need for project management each time a complex and articulated project is faced , such as acquisition and degli ultimi 6 mesi e consente linvio delle immagini per la consultazione da parte dei clinici a 72 reparti di degenza : in tali reparti sono installati 127 nuovi pc e configurati 1300 utenti con una media di 3300 accessi alla settimana . in radiologia le immagini , provenendo dalla memoria del server centrale ( archivio di i livello ) , vengono visualizzate sulle workstation . 
pertanto , per i pazienti interni lidentificazione anagrafica nel sistema proviene direttamente dalla e - request del reparto prenotante ( nome , cognome e data di nascita ) mentre per i pazienti esterni , che si rivolgono allo sportello radiologico o al cup , i dati anagrafici vengono immessi dal personale amministrativo al momento stesso della prenotazione . nellevento sentinella descritto il ris - pacs ha mostrato alcune carenze strutturali - tecnologiche ed organizzative ma anche di progettazione dellintero sistema . 
attivare , in presenza di omonimie o quasi - omonimie , un segnale automatico di avviso agli operatori sanitari ed amministrativi , che compare in fase di accettazione , esecuzione e refertazione ( elemento critico 1 ) ; ii . 
semplificare le worklist sulle modalit diagnostiche ( con persistenza del solo nominativo del paziente in studio ed eliminazione dei nominativi del giorno precedente ; elemento critico 2 ) ; iii.infine , ad allineare i server pacs e web , in modo tale da garantire una simultanea correzione di eventuali errori ( elemento critico 3 )  . 
 lanalisi delle criticit organizzative ha comportato una ridefinizione complessiva dei profili di responsabilit a tutti i livelli del ris - pacs con ladozione di un organismo di gestione della qualit , strutturato e formalizzato . 
a sua volta tale struttura ha adottato un nuovo modello organizzativo per la gestione delle attivit critiche del ris - pacs : nello specifico , stato identificato personale tsrm che , dopo specifica formazione , si dedica esclusivamente a svolgere tutte le azioni pi critiche e delicate ( correzioni degli identificativi , dei numeri di accesso , delle errate assegnazioni di immagini , delle segnalazioni da parte delle uo cliniche , ecc . ) in un ambiente appartato e protetto , posto in stretta adiacenza allamministratore del sistema ris - pacs . 
tutte le indagini che sono state oggetto di correzione sul server del pacs ( di dati anagrafici , di modifica delle assegnazioni , ecc . ) vengono attualmente evidenziate dalla comparsa di un marker automatico ( post - it definito : note adesive ) , che allerta il radiologo nella fase di refertazione . 
since projects in the healthcare setting are becoming increasingly complex and important such that the risk of failure due to faulty methodology has become extremely relevant [ 14 ] , the implementation of a ris - pacs requires a real business plan to guarantee collection of objective information and scientific evidence , which is indispensable for making informed decisions and not simply based on the opinions of individuals , regardless of their authority . 
in this sense , project management , seen as systemic management of a single , complex undertaking of a certain duration , aimed at achieving a clear and predefined objective through a continuous process of planning and control of different resources and with interdependent constraints of costtimequality , is an extraordinary instrument [ 15 ]  . 
the principal aims of project management can be summarised as follows : provide a realistic vision of the project during its entire life cycle make all of the actors involved responsible outline the expected project activities monitor the continuity of the activities highlight the critical areas and propose solutions integrate partial and general objectives of the project . the coordination of these objectives is the responsibility of a project manager , who in the case of a rispacs can be none other than a radiologist possessing the necessary specific skills and experience . 
it has become increasingly clear that the radiologist has a central role in medicalsurgical activity and that clinicians cannot be abandoned in the overall evaluation of diagnostic imaging , which has reached such a level of complexity ( and number of images ) that evaluation has become difficult for a those not specialised in imaging . 
this rimarcare la necessit del project management ogni qual volta si debba affrontare un progetto complesso ed articolato , come per lappunto lacquisto e la strutturazione di un sistema ris - pacs . 
poich in ambito sanitario i progetti sono sempre pi spesso complessi e dimensionalmente importanti che il rischio di insuccesso per difetto di metodologia di approccio diventato estremamente rilevante [ 14 ] , limplementazione di un ris - pacs necessita di un vero e proprio business plan , che garantisca la raccolta di informazioni obiettive e prove scientifiche , indispensabili per prendere decisioni circostanziate e non basate sulle opinioni , seppure autorevoli , dei singoli . 
in tale direzione , il project management , inteso come gestione sistemica di unimpresa complessa , unica e di durata determinata , volta al raggiungimento di un obiettivo chiaro e predefinito mediante un processo continuo di pianificazione e controllo di risorse differenziate e con vincoli interdipendenti di costi - tempi - qualit , rappresenta uno straordinario strumento di gestione manageriale dei progetti [ 15 ]  . 
gli obiettivi essenziali del project management si riassumono fondamentalmente in : fornire una visione realistica del progetto durante lintero ciclo di vita ; responsabilizzare tutti gli attori coinvolti ; tracciare un quadro previsionale delle attivit del progetto ; monitorare la continuit delle attivit ; evidenziare le criticit e proporre soluzioni ; integrare obiettivi parziali e generali del progetto . 
 il coordinamento di tali obiettivi in capo ad un project manager , che nel caso di un sistema ris - pacs non potr che essere un medico radiologo , in possesso di specifiche competenze ed esperienza sullargomento . 
sempre pi evidente che il radiologo svolge un ruolo centrale nellattivit medico - chirurgica e che i colleghi clinici non possono essere abbandonati nella valutazione globale della 1160 radiol med ( 2010 ) 115 : 11471164 prompts the need to constantly support clinicians in the evaluation of complex cases ( especially in cancer or surgery patients ) for a correct overall assessment . 
the need to revitalise contacts between the referring physician and the radiologist is mandatory , not only in the preliminary process of justification , but also downstream in the interand multidisciplinary comparison of the diagnostic findings . 
programmed and structured meetings between clinicians and radiologists , whether one - to - one or in groups , should be increased , in that the different specialist skills offer a substantial contribution to patient management . 
the reactive analysis of the sentinel event emphasises a severe shortfall in communication , even within the radiology department itself , in particular between the radiology technician who made the corrections on the server of the ris - pacs and the radiologist responsible for interpreting the images . 
whereas it is true that the communication of an error is a delicate moment , given the generally widespread and deep - rooted idea of individual liability , a cultural revolution is absolutely vital to reach a stage in which an error can be seen as an opportunity for learning , capable of prompting further reports . 
good therefore , together with teamwork , is essential for the success of a clinical risk management programme and , more generally , for implementing clinical governance policies [ 18 ]  . 
in this sense , the introduction of a briefing at the beginning of a working shift may help to improve internal communication , and not only for patient safety . the briefing consists of a short discussion ( maximum 5 min ) , which is both informal and structured , regarding the potential safety risks within the department . 
the moderator , who usually but not necessarily is also the head of the department , must be able to explain motivations and objectives even though every healthcare professional should take on a proactive attitude aimed at personal involvement and the involvement of other team members [ 4 ]  . 
critical elements linked to organisation and workload ( element 5 ) : a further critical element , which emerges from the analysis of the sentinel event , regards the significant workload of the ct section where the examinations of the two patients with similar names took place , an i contatti rivitalizzare diagnostica per immagini , che ha raggiunto una complessit ( ed una numerosit di immagini ) difficile da valutare per i non specialisti dellimaging . 
da qui la necessit di affiancare costantemente i clinici nella valutazione dei casi complessi ( in particolare i pazienti neoplastici o chirurgici ) per una corretta visione dinsieme del paziente . 
la tra medico necessit di curante / prescrivente e radiologo irrinunciabile non solo nel preliminare processo di giustificazione ma , soprattutto , a valle , nel confronto intere multi - disciplinare sui reperti diagnostici . 
riunioni clinico - radiologiche , di gruppo o singole , programmate e strutturate , vanno incrementate , in quanto le diverse competenze specialistiche apportano un sostanziale contributo al management del paziente . lanalisi reattiva dellevento sentinella ha messo in luce gravi carenze anche della comunicazione allinterno delluo di radiologia , in particolare tra tsrm che ha effettuato la correzione sui server del sistema ris - pacs e medico radiologo responsabile dellatto medico - radiologico . 
se pur vero che la comunicazione dellerrore rappresenta un momento delicato , poich nel sentimento generale radicata lidea di responsabilit individuale , assolutamente indispensabile una rivoluzione culturale per giungere a considerare lerrore come occasione di apprendimento , in grado di favorire ulteriori segnalazioni . 
pertanto , una buona comunicazione interna , unita al lavoro di gruppo , essenziale per il successo di un programma di gestione del rischio clinico e , pi in generale , per lattuazione delle politiche della clinical governance [ 18 ]  . 
in tale direzione , lintroduzione di un briefing allinizio del turno lavorativo rappresenta uno strumento in grado di migliorare la comunicazione interna , non solo per la sicurezza del paziente . 
il briefing consiste in un breve confronto ( massimo 5 minuti ) , colloquiale ma nello stesso tempo strutturato e formalizzato , riguardo i potenziali rischi per la sicurezza allinterno delluo . 
il moderatore , che solitamente ma non necessariamente coincide con il direttore delluo , deve essere in grado di spiegare motivazioni ed obiettivi anche se ogni professionista deve assumere un atteggiamento proattivo puntando al proprio coinvolgimento e a quello degli altri membri dellquipe [ 4 ]  . 
elementi critici legati allorganizzazione e ai carichi di lavoro ( elemento 5 )  . un ulteriore elemento critico , che emerge dallanalisi radiol med ( 2010 ) 115 : 11471164 1161 element which undoubtedly predisposes to error , as reported in the literature [ 19 ]  . 
prior to the event , during each 6 - h working shift ( 814 and 1420 ) , between 18 and 20 patients were studied , which according to the indications of the document for determining activity and productivity volumes of radiologists compiled by the italian society of medical radiology ( sirm ) and the italian national union of radiologists ( snr ) in 2006 [ 20 ] corresponds to the workload of two radiologists . 
thanks to the development of speech recognition systems , significant progress has been made in the reporting phase over the past 10 years , and deferring the production of the report no longer seems justifiable , except for a small percentage of patients requiring a more thorough analysis or the comparison with previous examinations not available on ris - pacs [ 21 , 22 ]  . 
whereas on the one hand , reporting with speech recognition improves the overall quality of the diagnostic procedure , it should be noted that , especially with ct and mri techniques , it takes up more time than the traditional system of dictation and subsequent transcription . dellevento sentinella , riguarda il notevole carico di lavoro della sezione tc in cui furono effettuati gli esami alle due pazienti con cognome analogo , elemento che indubbiamente predispone allerrore , come noto e riportato in letteratura [ 19 ]  . 
prima dellevento , per ogni turno lavorativo di 6 ore ( 814 e 1420 ) venivano studiati 1820 pazienti che , se ci si attiene a quanto indicato del documento di determinazione dei volumi di attivit e della produttivit dei medici radiologi edito dalla societ italiana di radiologia medica ( sirm ) e dal sindacato nazionale radiologi ( snr ) nel 2006 [ 20 ] , corrisponde al carico di lavoro di 2 medici radiologi . 
infatti , nel documento sirm - snr sui volumi di attivit , il tempo medio per latto medico radiologico sul singolo paziente sottoposto ad esame tc senza e con mdc di 45 , 6 minuti . 
ne consegue che , in base a quanto stabilito dallattuale contratto collettivo di lavoro della dirigenza medica , nelle 34 ore di lavoro previste per lattivit assistenziale non siano studiabili pi di 910 pazienti al giorno ( 5 giorni lavorativi ) , cui corrispondono 15 esami , stante il rapporto prestazione tc senza e con mdc / paziente di 1 , 5 . 
la fase di refertazione , grazie allo sviluppo dei riconoscitori vocali , si significativamente evoluta nellultima decade e non pare pi giustificabile un differimento nella produzione del referto , fatta salva una minima quota di pazienti con quadri complessi che richiedano un approfondimento di informazioni o il confronto con esami precedenti non disponibili sul sistema rispacs [ 21 , 22 ]  . 
se da un lato la refertazione vocale migliora la qualit complessiva della prestazione diagnostica non va dimenticato come , soprattutto per quanto riguarda le tecniche tc e rm , costringa ad un maggior consumo di tempo rispetto al sistema di dettatura e successiva trascrizione tradizionale . conclusions conclusioni the reactive analysis of the principal critical radiological elements that contributed to the sentinel event described emphasises the pressing need to change the management of healthcare services . 
this requires a shift from a paternalistic doctorpatient relationship to a new organisational model centred on the patient and not on the needs of the doctor and which is able to promote direct interaction and communication between the radiologist and the lanalisi reattiva dei principali elementi critici radiologici che hanno contribuito a determinare levento sentinella descritto fa emergere la cogente necessit di mutare la gestione dei servizi sanitari , passando da un rapporto paternalistico medico - paziente ad un nuovo modello organizzativo , in unottica orientata al paziente ( patient - centered ) anzich alle esigenze del medico , che pu giungere alla diretta interazione e comunicazione tra il radiologo ed il paziente , come 1162 radiol med ( 2010 ) 115 : 11471164 patient , as outlined in new working models [ 2325 ]  . 
in this sense , even clinical risk management requires an integrated vision of the problem , one that is difficult to achieve in the short terin current experience , the individual actions ( use of structured and scientifically validated diagnostictherapeutic protocols , review of medical records , incident reporting and monitoring of errors , maintenance and calibration of medical equipment , prevention of infection , analysis of litigation proceedings with patients ) , although important , do not seem to be enough to reach the objective of real risk prevention . indeed , clinical risk management is a complex process that requires a coordinated and multidisciplinary approach . 
in the absence of such a development , it will be impossible to take the structural actions required and have an impact on a sector that , without doubt , is highly professional but also highly compartmented . 
reconciling the absence of a consolidated culture of risk management with the evident difficulties and in some cases resistance to the introduction of radical organisational changes in complex and consolidated structures such as healthcare facilities is without doubt a difficult and ambitious task . 
the anticipatory techniques of fmea and fmeca nonetheless seem to ensure an improvement in results over time , since these are the only analysis tools capable of improving knowledge of healthcare processes and assisting each healthcare worker to reflect on and evaluate their everyday activities . in addition , an improvement in healthcare processes introduces real preventive and safety barriers able to impact on the frequency and detectability of adverse events , as well as ensuring a saving of resources resulting from the preventive actions that are put in place . 
the validity of the proactive approach is shown by the fact that fmeca is included in some of the most important and accredited quality management systems , both in the healthcare setting and elsewhere [ 26 ]  . 
however , it should be noted that there are no ideal techniques or tools for clinical risk management and that the most appropriate approach for each healthcare setting and organisation should be adopted . 
this should take into account the knowledge , awareness and readiness to implement changes , with the aim of instituting integrated management of the various instruments capable of creating synergism between them . prospettato in nuovi modelli lavorativi [ 2325 ]  . 
nellesperienza attuale i singoli contributi ( utilizzo di percorsi diagnostico - terapeutici strutturati e scientificamente validati , revisione delle cartelle cliniche , incident reporting e monitoraggio degli errori , manutenzione e taratura dei dispositivi medici , prevenzione delle infezioni , analisi dei contenziosi con i pazienti ) , seppure importanti , non sembrano sufficienti per raggiungere lobiettivo di una reale prevenzione dei rischi . 
in assenza di questa evoluzione culturale sar impossibile realizzare azioni strutturali e incidere su un settore caratterizzato certamente da professionalit elevatissime , ma altrettanto compartimentate . la mappatura degli eventi non deve riguardare solo quelli noti ma soprattutto quelli sconosciuti , dove la mancanza di esperienza rende la gestione del rischio pi difficile . 
conciliare lassenza di una cultura consolidata di risk management a fronte delle indubbie difficolt ancorch vere e proprie resistenze allintroduzione di radicali mutamenti organizzativi in strutture complesse e consolidate quali le strutture sanitarie sicuramente un obiettivo difficile ed ambizioso . 
la tecnica previsionale propria delle fmea e fmeca sembra tuttavia garantire , nel tempo , migliori risultati , poich realmente lunico metodo di analisi in grado di migliorare la conoscenza dei processi assistenziali , aiutando ciascun operatore a riflettere e valutare su tutto ci che viene realizzato quotidianamente . 
inoltre , migliorando i processi assistenziali , introduce delle vere e proprie barriere preventive e di sicurezza in grado di incidere sulla frequenza e sulla rilevabilit degli eventi avversi nonch di consentire un risparmio di risorse , stante le eventuali azioni preventive che vengono messe in campo . 
la validit dellapproccio proattivo testimoniata dal fatto che la fmeca prevista anche in alcuni tra i pi importanti ed accreditati sistemi di gestione della qualit , in ambito sanitario e non sanitario [ 26 ]  . 
occorre tuttavia considerare che per la gestione del rischio clinico non esistono strumenti o tecniche ideali , ma che dovrebbe essere adottato lapproccio pi idoneo al singolo contesto aziendale ed alle caratteristiche delle relative organizzazioni , principalmente in termini di conoscenza , consapevolezza , e disponibilit al cambiamento , con lobiettivo di attivare una gestione integrata dei diversi strumenti che possono risultare tra loro sinergici . 
il radiol med ( 2010 ) 115 : 11471164 1163 the change will take place only when the organisational factors , the healthcare workers and the patient who is still seen as not being involved or participating work together to achieve the objective of making both the setting and the content of the treatment safer . 
 lastly , since the request for diagnostic imaging services in the western world is constantly growing , with an associated increase in the latent risks linked to the activity , there is urgent need to review the role and tasks of the radiologist , who constitutes a sort of common thread throughout the entire diagnostictherapeutic pathway of the patient . 
the radiologist should have increasing contact with the clinician , with a specific and clear recognition of all phases of activity centred on the patient [ 4 ] , precisely with a view to preventing errors . 
the creation of diagnostictherapeutic pathways dedicated the main diseases and the introduction of the clinical microsystem that involves a single team of several professional figures [ 27 ] may be the future organisational frontiers for improving the safety of treatment . cambiamento si realizzer solo quando il fattore organizzativo , gli operatori sanitari e il paziente , ancora oggi pi pensato che non coinvolto e compartecipe , si alleeranno per raggiungere lobiettivo di rendere pi sicuri sia il contesto che il contenuto delle cure . 
 infine , poich nel mondo occidentale laumento della richiesta di prestazioni di diagnostica per immagini in continua crescita , e ci incrementa i rischi latenti connessi allattivit , urgente una rivisitazione del ruolo e dei compiti del radiologo , che costituisce una sorta di fil rouge nellintero percorso diagnostico - terapeutico del paziente . 
il radiologo deve sempre di pi interfacciarsi con il clinico , con uno specifico e chiaro riconoscimento di tutte le fasi dellattivit centrata sul paziente [ 4 ] , proprio nellottica di prevenire gli errori . 
after undergoing ultrasound ( us ) , contrast - enhanced us ( ceus ) and contrastenhanced computed tomography ( cect ) examinations , dogs with grade iiiiv injury received the minimally invasive therapy . 
in the survival group , animals underwent ceus and cect examinations to observe the short - term healing outcome and complications at 3 , 7 , 14 , and 21 days after the injection . 
before injection , ceus examinations showed anechoic and / or hypoechoic perfusion defects and active bleeding at the injury sites , and cect showed traumatic lesions as low - density regions without enhancement . 
laparotomy showed that the greater omentum had moved upwards and partly covered the wound in four animals , and the injury sites had completely riassunto lo scopo di questo studio la valutazione di eventuali complicanze delliniezione degli agenti emostatici nei traumi splenici chiusi . 
in questo studio , un gruppo di cani con traumi splenici di grado iii e iv , dopo essere stati sottoposti a indagini con ecografia , ecografia con contrasto ( ceus ) e tomografia computerizzata con contrasto ( cect ) , hanno ricevuto la nuova terapia miniinvasiva , che consiste nelliniezione di agenti emostatici ceus - guidata . 
dopo il trattamento , stato utilizzato il ceus per osservare i cambiamenti nelle sedi trattate . i cani hanno subito inoltre una laparotomia 30 minuti dopo il trattamento per osservarne leffetto emostatico . gli animali sopravvissuti sono stati sottoposti poi a esami ceus e cect per valutarne la guarigione a breve termine e le complicanze a distanza di 3 , 7 , 14 e 21 giorni dopo liniezione . 
dopo gli esami diagnostici , sono stati 12 i cani con traumi di iiiiv grado a essere stati arruolati in questo studio e sottoposti alla nuova terapia miniinvasiva . prima delliniezione , gli esami ceus mostravano lesioni anecogene e / o ipoecogene e sanguinamento attivo nelle sedi del trauma e la cetc mostrava le lesioni traumatiche come regioni a bassa densit senza enhancement . dopo il trattamento , il ceus ha dimostrato la scomparsa del sanguinamento attivo , e la comparsa di spots iperecogeni nelle sedi delle lesioni traumatiche . la cect ha rilevato delle aree di densit disomogenea e irregolare . 
le aree trattate si presentavano ricoperte di coaguli di sangue e di una membrana emostatica . dopo tre settimane , il ceus ha mostrato un decremento radiol med ( 2010 ) 115 : 10801086 1081 healed . 
ceus - guided haemostatic injection is not only effective in stopping active bleeding immediately , but it is also safe in that no complications occurred during the 3 weeks of follow - up . 
non sono comparse complicanze , come emorragie spleniche tardive , ascessi splenici , pseudoaneurismi splenici , ostruzione intestinale , aderenze intestinali . liniezione emostatica ceus - guidata non efficace solo nel bloccare immediatamente un sanguinamento acuto , ma anche un metodo sicuro che d la garanzia che non si manifesti nessuna complicanza durante le tre settimane di follow up . 
questo studio indica che liniezione percutanea ceus - guidata pu rappresentare una terapia realizzabile , sicura , efficace per i traumi splenici chiusi . parole chiave ecografia con comtrasto milza trauma agente emostatico introduction material and methods treatment of splenic trauma includes surgical and nonsurgical options . 
although sae is an effective and safe procedure for delayed vascular complications , sae may lead to various complications , such as bleeding , infarction , abscess , contrastinduced renal insufficiency , fever , pleural effusions and coil migration [ 13 ]  . 
laparoscopic splenectomy for splenic trauma has been reported and patients recovered well , but reports are infrequent . conservative treatment is the most common management method for haemodynamically stable patients , regardless of the severity of the injury . 
therefore , for patients with active bleeding and stable haemodynamics , it is necessary to find a new haemostatic method that is safe , effective and causes as little pain as possible . based on this therapeutic principle , our study team developed a new minimally invasive haemostatic method for abdominal solid - organ injury . 
we designed this animal experiment to explore the effectiveness and safety of this new method to treat blunt splenic trauma . in this method , because haemocoagulase atrox and alphacyanoacrylate are preserved in liquid and can be directly injected into injury sites under the ceus guidance , we chose them as haemostatic agents after substantial previous experiments . 
during open animal experiments , as alphacyanoacrylate has avery strong bonding force , we found that alpha - cyanoacrylate not only can rapidly solidify on contact with blood to close the splenic wound and stop bleeding , it also binds surrounding tissue , such as the omentu the most important factor for a new haemostatic method is effectiveness and safety , so we designed this animal experiment to observe whether ceus - guided percutaneous injection of alpha - cyanoacrylate could lead to complications or side effect in blunt splenic trauma . 
 all experiments were performed in accordance with the ethical committees regulations of our institutional animal care and use committee and guidelines issued by the us national institutes of health for the care of laboratory animals . animal model for blunt splenic trauma sixteen dogs ( weighing 1722 kg ) were deeply anaesthetised by intramuscular injection of pentobarbital sodium ( 30mg / kg ) and received 1 , 000 ml of sodium chloride through the femoral vein during anaesthesia . 
dogs were fixed in a supine position with their limbs fixed to the table , and the body hair 1082 radiol med ( 2010 ) 115 : 10801086 in correspondence with the spleen was completely removed . the spleen position was targeted by conventional ultrasound ( us )  . 
firstly , we installed the impact ammunition into the shell of impactor , then placed the miniature impactor head firmly against the surface of the spleen , then strike the impactor trigger , propelling the impact head . 
 ultrasound contrast agent to accurately guide the injection needle into the haemorrhagic site , all animals were administered second - generation us contrast agent sonovue ( bracco , milan , italy ) consisting of sulphur hexafluoride ( sf6 ) microbubbles stabilized by a phospholipid shell . 
scan settings for the examination , including the gain , scanning depth and time gain control ( tgc ) , were optimized for each region independently and the focus was set to the deeper aspect of the lesion being examined . 
 ct examination basal abdominal ct and contrast - enhanced computer tomography ( cect ) ( ge twin - scan , general electric medical systems , milwaukee , wi , usa ) were performed after impact to observe injuries and active bleeding . 
scan range was the diaphragmatic muscle to the pubic symphysis ( 2 mm5 mm collimation , 1 - s speed rotation , 15 - mm / s table feed , 140 - kv , automatic ma setting )  . 
ct images were consensually analysed by two experienced diagnostic radiologists in our hospital with an experience of 3 and 7 years , respectively , who were blinded to the experimental animal models . ceus examination and schedule for haemostatic agent injection under ceus guidance after ct examinations , ceus was performed to detect the injury sites and active bleeding by cps mode at low acoustic power . 
a contrast agent bolus of 0.61.0ml for cps was injected intravenously through the femoral vein , followed by a 5 - ml saline flush ( using a three - way stopcock ) to ensure that no residual contrast remained in the intravenous catheter . 
according to the american association for the surgery of trauma ( aast ) organ injury scale and the results of ceus and cect exams , two experienced readers made the final conclusion about injury grade . 
two readers were registered diagnostic radiologists with an experience of 5 and 12 years , respectively , and they were all involved in creating all animal models . to decrease tissue injury caused by the needle , a 21gauge ethanol injection therapy needle ( eight optical ltd , japan ) was chosen to create the trauma . 
in the survival group , animals underwent ceus and cect examinations to observe the short - term healing outcome and complications at 3 , 7 , 14 , and 21 days after the injection . 
digital images were recorded as single - frame pictures and multiple cine - loops on the scanner for off - line analysis . histopathological examination histopathological examination was analysed by an experienced pathologist . 
 results after blunt impact , two grade v dogs died before treatment , two dogs with iii injury were excluded and other 12 dogs with iiiiv injury were enrolled in the treatment group . 
b visibile la fuoriuscita di contrasto , con aspetto iperecogeno a partenza dalla linea di confine della lesione traumatica ( freccia )  . 1084 radiol med ( 2010 ) 115 : 10801086 fig . 
4 la cect mostra la discontinuit della capsula splenica e le aree prive di contrasto nel parenchima splenico ( frecce )  . lase atrox for in injection , fibrin glue ( fg ) and alphacyanoacrylate , et al . 
many scholars have verified the advantages of alpha - cyanoacrylate , including good biocompatibility , absorbability , non - toxic , non - teratogenic , no antigen and carcinogenic , it also can be degradated gradually in the period of 34 weeks and no remains in body [ 1922 ]  . 
 based on the findings of the previous experiments , we found that the blood clot formed by haemocoagulase atrox for in injection was soft and loose , and was easily washed away by bleeding from wound . 
under the guidance of cps , in order to adhere and close the injury site and stop bleeding completely , we injected alpha - cyanoacrylate into the active bleeding sites following haemocoagulase atrox for in injection injection . 
5 larea trattata appare ricoperta dai coaguli di sangue e dalla membrana emostatica ( frecce )  . and as sensitive as ct in the detection of traumatic lesions . our animal studies also indicated that ceus was able to clearly show injury size , completeness of injury extension , involvement of the organ capsule and active bleeding , and it showed high levels of concordance with cect [ 7 , 10 ]  . under the guidance of ceus , radiofrequency ablation ( rfa ) and percutaneous microwave coagulation therapy ( pmct ) have developed very quickly and made satisfied therapeutic effects in recent years [ 11 , 12 ]  . 
 nowadays , haemostatic agents have been applied widely and successfully in stopping local blood loss , especially used in laparotomy and endoscope , such as haemocoaguradiol med ( 2010 ) 115 : 10801086 1085 fig . 
in our study , slight dose of alpha - cyanoacrylate were used , and alphacyanoacrylate mainly injected into injury sites and active bleeding sites , therefore , no ileus and adhesions observed in 4 animals even greater omentum moved up and partly covered the injury sites . 
all animals histopathologic examinations did not show that alpha - cyanoacrylate entered in the arterial vessel and appeared intra - arterial embolization . this experiment results proved that this mini - invasive haemostatic therapy was safe , feasible and effective . 
cademartiri1 , 2 1department of radiology and cardiology , academic hospital / azienda ospedaliero - universitaria , parma , italy 2department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands correspondence to : f . 
cademartiri , dipartimento di radiologia e diagnostica per immagine , c / o piastra tecnica piano 0 , azienda ospedaliero - universitaria , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703516 , fax : + 39 - 052 - 1703630 , e - mail : filippocademartiri@hotmail.com received : 25 may 2009 / accepted : 26 june 2009 / published online : 10 march 2010 springer - verlag 2010 abstract purpose . 
a 64 - slice ct system was used to perform first - pass coronary angiography with a tube current of 15 mas / kg [ arterial phase ( art ) ] followed by two delayed - enhancement ( de ) scans 15 min after contrast material administration , with a tube current of 15 mas / kg and 37.5 mas / kg , respectively ( de1 and de2 )  . 
ct values expressed in hounsfield units ( hu ) were measured using five regions of interest ( roi ) : de , no reflow , remote lv , lv cavity ( lv lumen ) and in air , respectively . 
in 5 maiali domestici ( peso medio 24 kg ) , il ramo circonflesso dellarteria coronarica sinistra stato occluso mediante pallone e sottoposto a riperfusione a distanza di 2 h . 
le scansioni sono state eseguite mediante tc a 64 - strati : la prima , angiografia - coronarica convenzionale di primo passaggio , eseguita ad una corrente del tubo di 15 mas / kg ( art ) ; le restanti due scansioni de - ct eseguite 15 min dopo somministrazione di agente di contrasto iodato , ad una corrente del tubo di 15 mas / kg e 37 , 5 mas / kg , rispettivamente ( de1 e de2 )  . 
i valori di attenuazione tc ( espressi in unit hounsfield [ uh ] ) sono stati misurati in cinque regioni dinteresse : de , noreflow , lv remoto , cavit ventricolare sinistra ( lv lume ) e in aria , rispettivamente . 
significative differenze sono state trovate tra le attenuazioni dellarea de , no - reflow e lv remoto , in ogni protocollo di scansione ( p < 0 , 001 )  . 
 parole chiave infarto miocardico acuto riperfuso tc - 64 strati corrente del tubo dose di radiazione delayed enhancement modello animale introduction introduzione the ability to distinguish viable myocardium from necrotic tissue after reperfused acute myocardial infarction is a long - term predictor of the function and geometry of the left ventricle ( lv ) , as well as a predictor of the probability of cardiovascular events and mortality in patients who have suffered an acute ischaemic event [ 1 , 2 ]  . 
for many years , delayed - enhancement ( de ) imaging performed with magnetic resonance ( de - mr ) has been validated as a reference technique for semiquantitative evaluation of myocardial infarction and used as a noninvasive clinical method for assessing the extent of myocardial infarction [ 35 ]  . recent developments in multidetector - row computed tomography ( ct ) technology have broadened its applications , potentially making it a noninvasive diagnostic tool for evaluating myocardial infarction [ 68 ]  . 
however , ct data have been principally used to evaluate atherosclerotic coronary artery disease , where they have shown excellent accuracy , especially in ruling out significant coronary artery stenosis [ 9 , 10 ]  . only a small number of studies have reported preliminary data on the evaluation of ischaemic myocardial damage with the use of iodinated contrast material [ 11 ]  . nonetheless , many studies in this field have provided a comprehensive quantitative evaluation of myocardial necrosis and microvascular obstruction ( no reflow ) with ct la capacit di distinguere il miocardio vitale dal tessuto necrotico dopo infarto miocardico acuto riperfuso un fattore predittivo a lungo termine della funzione e della geometria del ventricolo sinistro , nonch della probabilit di eventi e mortalit nei pazienti che hanno subito un evento ischemico acuto [ 1 , 2 ]  . 
da molti anni , limaging delayed enhancement eseguito mediante risonanza magnetica ( derm ) stato validato come tecnica di riferimento per la valutazione semi - quantitativa dellinfarto miocardico ed utilizzato come metodo clinico non - invasivo per la valutazione delle dimensioni dellarea di miocardio infartuato [ 35 ]  . 
i recenti sviluppi della tecnologia di tomografia computerizzata ( tc ) multi - strato hanno esteso il suo spettro di applicazione come potenziale strumento diagnostico noninvasivo per la valutazione di infarto miocardico [ 68 ]  . tuttavia , i dati tc sono stati ampliamente utilizzati per la valutazione della malattia coronarica aterosclerotica mostrando uneccellente accuratezza diagnostica soprattutto nellesclusione della stenosi coronarica significativa [ 9 , 10 ]  . attualmente , solo un limitato numero di studi hanno riportato esperienze preliminari di valutazione di danno miocardico ischemico mediante agente di contrasto iodato [ 11 ] ; tuttavia , molti studi eseguiti in questo campo hanno fornito una comprensiva valutazione quantitativa di necrosi radiol med ( 2010 ) 115 : 10031014 1005 ( de - ct ) , even though the accuracy of the technique is yet to be validated [ 1215 ]  . 
under fluoroscopic guidance , the circumflex branch of the left coronary artery was balloon - occluded . two hours after the event , reperfusion was obtained with balloon deflation and demonstrated by conventional coronary angiography . 
the study was carried out in accordance with the regulations of the ethics committee for the protection of animals of the erasmus medical center ( rotterdam , netherlands ) and the national institutes of health publication , guide for the care and use of laboratory animals , 1996 . ct scan protocols and parameters miocardica ed ostruzione microvascolare ( no - reflow ) mediante tc ( de - tc ) , anche se laccuratezza diagnostica della tecnica non ancora chiara [ 1215 ]  . 
infatti , al momento non si conosce lesatta combinazione dei parametri di scansione tc , quali : mas , kv , quantit di agente di contrasto iodato e time - delay ( tempo tra la somministrazione dellagente di contrasto iodato e la scansione )  . lo scopo di questo studio di valutare la qualit dimmagine della tecnica de - tc nella valutazione dellinfarto miocardico acuto riperfuso eseguito con differente corrente del tubo ( mas ) , su modello animale . materiali e metodi modello animale cinque maiali yorkshire - landrace ( et , 23 mesi ; peso , 22 kg ) sono stati sedati ( iniezione intramuscolare di ketamina 20 mg / kg e midazolam 1 mg / kg ) , anestetizzati ( tiopentale 12 mg / kg ev ) , intubati e meccanicamente ventilati ( miscela di ossigeno e azoto 1 : 2 )  . 
lo studio stato eseguito nel rispetto delle norme del comitato etico di protezione animale dellospedale erasmus medical center ( rotterdam , olanda ) e del national istitutes of health pubblication ( guide for the care and use of laboratory animals , 1996 )  . five days after induction of the myocardial infarction , all animals were anaesthetised as described above and underwent ct study of the coronary arteries . 
scans were performed with a 64 - slice ct system ( sensation 64 , siemens , germany ) and the following scan parameters : detector collimation 32 0.6 mm ( z - flying focal spot ) ; slices / rotation 64 ; individual detector width 0.6 mm ; gantry rotation time 330 ms ; effective temporal resolution 165 ms . three consecutive ct scans were obtained : art ; ctca : conventional first - pass ( arterial phase ) ct coronary angiography ( with bolus tracking technique ) de1 : de - ct imaging , performed with 15 mas / kg ( 350 de2 : de - ct imaging , performed with 37.5 mas / kg ( 900 mas ) mas ) protocolli e parametri di scansione tc cinque giorni dopo linduzione dellinfarto miocardico , tutte le cavie sono state anestetizzate come precedentemente descritto e sottoposte a studio tc delle coronarie . 
le scansioni tc sono state eseguite con apparecchiatura tc a 64strati ( sensation 64 , siemens , germania ) avente le seguenti caratteristiche : numero file di detettori 322 mm ( tecnica zflying focal spot ) ; numero strati / rotazione 64 ; ampiezza individuale del detettore 0 , 6 mm ; tempo di rotazione del gantry 330 ms ; risoluzione temporale effettiva 165 ms . 
 sono state eseguite consecutivamente tre scansioni tc : art : ac - tc , angiografia - coronarica convenzionale di primo - passaggio ( mediante tecnica bolus tracking ) ; de1 : de - tc imaging , eseguita a 15 mas / kg ( 350 mas ) ; 1006 radiol med ( 2010 ) 115 : 10031014 iodinated contrast material was injected with peripheral iv access at a flow rate of 1.5 ml / s ( 400 mgi / ml iomeprol ; 1.25 gi / kg at first pass followed by 2.50 gi / kg = 3.75 gi / kg ; iomeron , bracco , italy )  . 
the following scan parameters were used : tube current 350 / 900 mas with voltage 120 kv ; table feed per rotation 3.84 mm ; scan direction craniocaudal and retrospective electrocardiographic ( ecg ) gating . 
the voxel size during acquisition was 0.30.30.4 mwith the application of dose parameters used for humans , the radiation exposure should correspond to 15 / 21 msv for a male / female individuals in the de1 protocol and three times the same value in the de2 protocol ( windose , institute of medical physics , erlangen , germany ) [ 13 , 14 ]  . mean heart rate was lowered to 519 bpm with iv administration of zatebradine ( 10 mg / kg )  . 
de - ct data sets were reconstructed at 300 ms , 350 ms and 400 ms prior to the subsequent r wave ( enddiastolic phase of the cardiac cycle )  . 
axial images were reconstructed from data sets with optimal image quality with a 1 - mm thickness and increment of 0.5 mm using a 150150 mm field of view , a 512512 matrix and a medium - smooth convolution kernel ( b30f )  . data analysis one day after the ct scans , all test animals were sacrificed . axial images were exported and transferred to a separate workstation with dedicated software ( leonardo siemens )  . the areas were manually selected on axial images by two experienced observers working in consensus . 
remote lv was obtained by the difference between the total area of myocardium and the infarcted area . de2 : de - tc imaging , eseguita a 37 , 5 mas / kg ( 900 mas )  . liniezione dellagente di contrasto iodato stata eseguita mediante accesso periferico intravenoso ad una velocit di flusso di 1 , 5 ml / s ( 400 mgi / ml iomeprol ; 1 , 25 gi / kg al primo - passaggio seguiti da 2 , 50 gi / kg = 3 , 75 gi / kg ; iomeron , bracco , italia )  . 
sono stati utilizzati i seguenti parametri di scansione : corrente del tubo , 350 / 900 mas ad una tensione del tubo di 120 kv ; avanzamento / rotazione , 3 , 84 mm ; direzione di scansione , cranio - caudale e modalit di acquisizione elettrocardiogramma ( ecg ) - gated retrospettivo . 
la dimensione del voxel durante lacquisizione era 0 , 30 , 30 , 4 mapplicando i parametri di dose utilizzati per un soggetto umano , lesposizione alla dose di radiazione dovrebbe corrispondere a 15 / 21 msv per un soggetto maschile / femminile nel protocollo de1 e approssimativamente 3 volte lo stesso valore nel protocollo de2 ( windose , istitute of medical physics , erlangen , germania ) [ 13 , 14 ]  . la frequenza cardiaca media stata ridotta a 519 battiti per minuto ( bpm ) mediante somministrazione intravenosa di zatebradine ( 10 mg / kg ev )  . 
i dataset de - tc sono stati ricostruiti a 300 ms , 350 ms , e 400 ms prima della successiva onda r ( fase tele - diastolica del ciclo cardiaco )  . 
le immagini assiali sono state ricostruite dai dataset con qualit dimmagine ottimale , con spessore di 1mm ed incremento di 0 , 5 mm utilizzando un campo di vista ( fov ) di 150150 mm , una matrice di ricostruzione di 5122 , ed un kernel di convoluzione medium - smooth ( b30f )  . 
de is the area of infarction without microvascular obstruction and is defined as a region of hyperattenuation or area of hyperintense tissue due to the higher concentration of contrast material ( arrowheads ) ; no - reflow is the area of infarction with microvascular obstruction and is defined as a region of hypoattenuation located in the subendocardial portion of de ( thin arrows )  . 
in particular , the area of hyperattenuation can be seen in the inferolateral wall of the left ventricle , which corresponds to the region perfused by the left circumflex artery . 
de larea dinfarto senza ostruzione microvascolare e definita come una regione di iperdensit o unarea di tessuto iperintenso per la pi alta concentrazione di agente di contrasto ( teste di frecce ) ; il no - reflow larea di infarto con ostruzione microvascolare e definita come una regione di ipodensit localizzata nella porzione sub - endocardica di de ( freccie sottili )  . 
in particolare , si pu osservare larea di iperdensit nella parete infero - laterale del ventricolo di sinistra , in corrispondenza del territorio di perfusione del ramo circonflesso dellarteria coronarica di sinistra . 
image quality was calculated as the signal - to - noise ratio ( snr ) and contrast resolution as the contrast - to - noise ratio ( cnr )  . 
signal intensity was defined as the ct attenuation value ( hu ) measured in the roi placed in the infarcted area and calculated as the relationship between de attenuation and relative standard deviation ( sd )  . 
differences between areas , attenuation values , snr and cnr were calculated with a t test for paired data and pearsons r coefficient in the de , no - reflow and remote lv regions . 
la qualit dellimmagine stata calcolata come rapporto segnale / rumore ( s / n ) , mentre la risoluzione di contrasto come rapporto contrasto / rumore ( c / n )  . 
lintensit di segnale stata definita come il valore tc ( uh ) misurato nella roi posizionata nellarea di infarto e calcolata come il rapporto tra lattenuazione di de e la relativa deviazione standard ( sd )  . 
i grafici di bland - altman mostrano una buona concordanza per lanalisi di s / n ( qualit dimmagine ) e c / n ( risoluzione di contrasto )  . 
s / n , rapporto segnale / rumore ; c / n , rapporto contrasto / rumore ; de , miocardio infartuato ; no - reflow , miocardio infartuato , con ostruzione microvascolare ; de1 e de2 , de - ct , acquisito a 15 / 37 , 5 mas / kg ( de1 / de2 ) , rispettivamente . 
art , adaptive radiation therapy ; first - pass computed tomography coronary angiography ( ctca ) ; de1 and de2 , delayed enhancement ct acquired at 15 / 37.5 mas / kg ( de1 / de2 ) , respectively ; de , delayed enhancement or infarcted myocardium ; no reflow , infarcted myocardium with microvascular obstruction ; de / total , lv relationship between de and total myocardium ; no reflow / de , relationship between no reflow and de no - reflow de / total lv no - reflow / de 0 , 20 , 2 0 , 40 , 4 0 , 40 , 4 49 , 820 , 7 55 , 619 , 9 54 , 220 , 5 0 , 920 , 84 1 , 681 , 59 1 , 561 , 30 dimensione delle aree de e no - reflow , espresse in cm2 . 
art , ac - tc di primo - passaggio ; de1 e de2 , de - ct , acquisito a 15 / 37 , 5 mas / kg ( de1 / de2 ) , rispettivamente ; de , delayed - enhancement , o miocardio infartuato ; no - reflow , miocardio infartuato , con ostruzione microvascolare ; de / total lv , relazione tra delayed - enhancement e miocardio totale ; no - reflow / de , relazione tra no - reflow e delayed - enhancement reperfused acute myocardial infarction was visible in all scan protocols . 
measurements were made of differenze tra le aree , i valori di attenuazione , s / n e c / n sono state calcolate mediante test t di student per dati appaiati ed r di pearson nelle regioni di de , no - reflow e lv - remoto . 
la riproducibilit inter - / intra - osservatore stata valutata mediante correlazione di pearson ( intercooled stata , versione 6.0 ; stata , college station , tex , usa )  . 
 scans scans radiol med ( 2010 ) 115 : 10031014 1009 de and no - reflow areas de and no - reflow areas de area no - relow area de area / total lv area no - reflow area / de area fig . 
de , delayed - enhancement , o miocardio infartuato ; no - reflow , miocardio infartuato , con ostruzione microvascolare ; lv totale , miocardio totale ; art , ac - tc di primo - passaggio ; de1 e de2 , de - ct , acquisito a 15 / 37 , 5 mas / kg ( de1 / de2 ) , rispettivamente . computed tomography ( ct ) attenuation values of different regions of interest , expressed in hu ( meansd )  . 
i valori tc di de sono significativamente pi alti dei valori di no - reflow , in ogni protocollo di acquisizione ( a ; p < 0 , 001 )  . in particolare , un valore di attenuazione leggermente maggiore stato ottenuto utilizzando la pi bassa dose di radiazione ( b ; de1 )  . 
infatti , sono state misurate anche larea totale ( lv , 25 , 35 , 7 cm2 ) ed endocavitaria del ventricolo sinistro ( lv lume , 11 , 94 , 4 cm2 ) , e larea totale di miocardio ( lv totale , 13 , 52 cm2 )  . 
i valori s / n e c / n sono significativamente maggiori nei protocolli de , se comparati a quelli del protocollo art ( r = ~0 , 6 ; p < 0 , 001 ) ( tabella 3 ) , tuttavia in de1 vs . 
art , adaptive radiation therapy ; first - pass ct coronary angiography ( ca ) ; de1 and de2 , de - ct , acquired at 15 / 37.5 mas / kg ( de1 / de2 ) , respectively tabella 3 rapporto segnale / rumore ( s / n ) e contrasto / rumore ( c / n ) 3 , 791 , 74 1 , 071 , 36 6 , 322 , 35 3 , 721 , 72 6 , 092 , 39 3 , 541 , 6 lintensit di segnale stata valutata come valore tc della roi posizionata nellarea de e calcolata come relazione tra lattenuazione di de e la relativa deviazione standard . 
art , ac - tc di primopassaggio ; de1 e de2 , de - ct , acquisiti a 15 / 37 , 5 mas / kg ( de1 / de2 ) , rispettivamente vascularisation of the myocardial infarction ( acute and / or subacute phase ) during the time between iodinated contrast material administration and scan ( time delay )  . 
 [ 11 ] hanno eseguito uno studio tc per la valutazione dellinfarto miocardico non - riperfuso in un modello animale porcino e hanno dimostrato le limitazioni della metodica nella valutazione dellinfarto determinate dal basso segnale di densit o dallipo - opacizzazione ottenuta dalla fase di primo - passaggio dellagente di contrasto . 
 limaging de - tc fattibile grazie alla passiva ridistribuzione ( slow wash - out ) dellagente di contrasto iodato allinterno dellaumentata matrice extracellulare caratterizzante le zone di vascolarizzazione dellinfarto miocardico ( fase acuta e / o subacuta ) , durante il tempo di intercorrenza tra la somministrazione dellagente di contrasto iodato e la scansione ( time - delay )  . 
precedenti studi [ 3 , 4 ] hanno dimostrato che le regioni con segnale ipodenso ( ipo - enhancement ) riflettono la porzione di infarto con ostruzione microvascolare ( no - reflow ) , mentre le regioni con segnale iperdenso ( iper - enhancement ) riflettono il miocardio necrotico non permanentemente danneggiato ( de )  . 
de - tc , il pi basso contrasto dellimmagine non permette una chiara e netta caratterizzazione tissutale ( miocardio sano , miocardio infartuato con e senza ostruzione microvascolare )  . dimostrato che lestensione dellinfarto un importante valore predittivo sul recupero della funzionalit del fig . 
art , ac - tc di primo passaggio ; de1 e de2 , de - ct , acquisito a 15 / 37 , 5 mas / kg ( de1 / de2 ) , rispettivamente . 1012 radiol med ( 2010 ) 115 : 10031014 indicative of necrotic myocardium which is not permanently damaged ( de )  . ctca scans , in contrast , are characterised by limited redistribution of iodinated contrast material within the infarcted myocardiu given ctca hypoattenuation of necrotic tissue vs . 
in fact , in de scans , the size of areas of de and microvascular obstruction remained unchanged ( table 1 )  . we found that an increase in radiation exposure does not always correspond with an increase in image quality . 
the higher radiation dose shows no improvement in the limited ct contrast of the soft tissues . limitations the study was done on a limited number of test animals . nonetheless , the small sample size was balanced by the high number of measurements obtained for data analysis . 
con lutilizzo di una dose di esposizione convenzionale ( 37 , 5 mas / kg ) , lestensione dellarea di infarto ed ostruzione microvascolare rimangono sottostimate ( tabella 1 )  . 
tuttavia , i valori di attenuazione e dellarea di no - reflow non sono significativamente influenzati dalla differente dose di radiazione . infatti , nelle scansioni de , le dimensioni del delayedenhancement e di ostruzione microvascolare sono rimaste quasi invariate ( tabella 1 )  . noi troviamo che un aumento di esposizione alle radiazioni non sempre corrisponde ad un aumento della qualit dimmagine . 
le regioni di interesse ( roi ) utilizzate per la valutazione dei valori di attenuazione tc non hanno le stesse dimensioni , ma sono state adattate al massimo alle dimensioni della regione sottoposta a misurazione . 
tuttavia , tra i parametri di acquisizione determinanti la dose e laccuratezza diagnostica nelle apparecchiature tc , non stata eseguita la radiol med ( 2010 ) 115 : 10031014 1013 influence dose and diagnostic accuracy in ct systems , no evaluation of the impact of different kilovoltage settings was done , which could be a possible topic for future research ( especially with the introduction of dual - source ct systems ) [ 19 , 20 ]  . valutazione dellimpatto di differenti dosi di kv , che potr essere potenziale argomento di studio in indagini future ( soprattutto con lintroduzione delle apparecchiature tc a doppia energia ) [ 19 , 20 ]  . 
 conclusioni conclusions this study demonstrates that in de imaging with ct , the radiation dose does not significantly influence image quality , contrast resolution , and size of the infarcted area . further studies are required to evaluate the impact of our findings on humans and possible improvements that could be obtained with the introduction of dual - source ct systems [ 2123 ]  . questo studio rileva che nellimaging de eseguito mediante tc , la dose di radiazione non influenza significativamente la qualit dimmagine , la risoluzione di contrasto e le dimensioni dellarea di infarto . 
torricelli1 1dipartimento integrato dei servizi diagnostici e per immagine , 2dipartimento di chirurgia , universit degli studi di modena e reggio emilia , policlinico via del pozzo 71 , 41100 modena , italy correspondence to : a . 
all patients were imaged with the following sequences : axial t1 - weighted and axial and coronal t2 - weighted , 2d spin echo ( se ) breath - hold radial cholangiography , and coronal 3d single - shot turbo spin echo ( ss - tse ) with respiratory triggering . 
when biliary complications were present , diagnostic confirmation was obtained by endoscopic retrograde cholangiopancreatography ( ercp ) ( n = 13 ) , percutaneous transhepatic cholangiography ( ptc ) ( n = 20 ) , ultrasonography ( n = 10 ) or computed tomography ( ct ) ( n = 2 )  . 
mrc detected biliary complications in 44 / 78 patients , in particular , 42 biliary strictures ( 37 anastomotic and five intrahepatic ) , 40 of which were confirmed by other imaging modalities . 
other mrc - detected biliary complications were biliary sludge ( n = 4 ) , biloma ( n = 5 ) , and biliary stones ( n = 3 )  . 
settantotto pazienti sottoposti a olt con sospetto clinico di complicanza biliare sono stati sottoposti a studio rm del fegato mediante magnete a 1 , 5 t con bobina di superficie . 
in tutti i pazienti sono state eseguite sequenze assiali t1 pesate , assiali e coronali t2 pesate , sequenza colangiografica radiale 2d - spin echo ( se ) in apnea e sequenza 3d - turbo spin echo ( tse ) single shot ( ss ) sul piano coronale triggerata con il respiro . quando lesame rm risultato negativo i pazienti sono stati sottoposti a follow - up clinico - ecografico . 
le complicanze identificate allesame rm sono state confermate mediante colangiografia retrogada endoscopica ( 13 casi ) , colangiografia percutanea transepatica ( 20 casi ) , ecografia ( 10 casi ) , tomografia computerizzata ( tc ) ( 2 casi )  . 
in 44 / 78 pazienti lesame rm ha evidenziato una complicanza chirurgica , in particolare 42 stenosi biliari ( 37 anastomotiche e 5 intraepatiche ) , 40 delle quali confermate dalle altre metodiche . 
le altre complicanze biliari identificate alla colangio - rm sono state : fango e detriti biliari ( 4 casi ) , bilomi ( 5 casi ) e calcoli biliari ( 3 casi )  . 
in 4 casi la colangiografia trans epatica ha mostrato la presenza di complicanze biliari non 1066 radiol med ( 2010 ) 115 : 10651079 strictures of the intrahepatic ducts and biliodigestive anastomosis ( false positive results )  . 
i nostri risultati hanno confermato che la colangio - rm una metodica ottimale per la visualizzazione della sede di anastomosi e per identificare eventuali complicanze biliari nel paziente sottoposto a olt . 
the former occur within 3 months after transplantation and account for almost two thirds of all complications , with a marked prevalence of bile collections . late complications may arise a few months to several years after transplantation and account for one third of the total , with a marked prevalence of anastomotic strictures [ 1 , 11 ]  . the diagnosis of biliary complications in transplant patients is complex owing to the nonspecific clinical presentation and biohumoural changes . 
direct cholangiography procedures , such as endoscopic retrograde cholangiopancreatography ( ercp ) and percutaneous transhepatic cholangiography ( ptc ) , are highly reliable for diagnosing biliary complications and at the same time have a potential for allowing possibly definitive therapeutic intervention . 
however , they are invasive techniques that are not free from complications and must consequently be used with caution , and only in selected cases , in patients with clinical and biohumoural alterations appearing in the immediate posttransplant period [ 1 , 2 , 12 ]  . ultrasonography ( us ) is the standard modality for posttransplant follow - up , even though its diagnostic accuracy in detecting biliary complications is low given that it rarely allows direct visualisation of the anastomotic site [ 1 ]  . computed tomography ( ct ) has only moderate accuracy in detecting and characterising biliary complications owing to le complicanze biliari rappresentano ancora oggi una delle principali cause di morbilit e mortalit nei pazienti sottoposti a trapianto ortotopico di fegato ( olt ) [ 1 , 2 ] , nonostante i miglioramenti del tasso di sopravvivenza e i progressi nella tecnica chirurgica . 
le tardive invece si possono verificare da pochi mesi a diversi anni dal trapianto e sono circa 1 / 3 con netta prevalenza delle stenosi anastomotiche [ 1 , 11 ]  . la diagnosi di complicanza biliare nel paziente trapiantato problematica , in quanto le manifestazioni cliniche e le alterazioni bioumorali sono spesso aspecifiche e , di conseguenza , la diagnostica per immagini gioca un ruolo fondamentale per il corretto inquadramento diagnostico del paziente e la successiva pianificazione terapeutica [ 1 , 2 ]  . 
le procedure colangiografiche dirette , quali la colangiopancreatografia retrograda endoscopica ( ercp ) e la colangiografia transepatica percutanea ( ptc ) , sono molto affidabili nella diagnosi delle complicanze biliari e hanno al tempo stesso potenzialit terapeutiche a volte risolutive . sono tuttavia tecniche invasive e non scevre di complicanze , da utilizzarsi pertanto con cautela , e solo in casi selezionati , nel paziente con alterazioni clinico - bioumorali comparse nellimmediato periodo post - trapianto [ 1 , 2 , 12 ]  . 
 lecografia la metodica che di routine viene impiegata nel follow - up post - trapianto , ma ha bassa accuratezza diagnostica nella identificazione delle complicanze biliari , anche perch solo raramente consente la visualizzazione diretta della sede di anastomosi [ 1 ]  . 
la tomografia radiol med ( 2010 ) 115 : 10651079 1067 its relative inability to provide detailed and panoramic views of the entire biliary tree and of the anastomotic site [ 1 ]  . 
in addition , ct imaging of olt patients poses problems related to radiation exposure , especially in children , and to the use of contrast agents , given that renal failure is a common complication of olt ( 12%70% ) [ 13 ]  . in recent years , the technological advances in magnetic resonance ( mr ) imaging , in particular , the use of units with high - performance gradients and surface coils , have allowed us to obtain t2 - weighted images with a high spatial and temporal resolution able to define type , site and degree of biliary complication with an accuracy comparable with direct cholangiography procedures . 
published studies [ 1 , 2 , 1217 ] investigating the role of mr cholangiography ( mrc ) in detecting post - olt biliary complications report a sensitivity ranging from 87.5% to 100% and a specificity from 92% to 100% , values that justify a possible central role of this technique in the follow - up of olt patients . 
the aim of this study was to evaluate the role of mrc compared with direct cholangiography techniques in detecting biliary complications in adult patients who underwent olt . materials and methods from august 2004 to august 2008 , 201 patients underwent olt . 
of these , 78 ( 53 men and 25 women ; mean age 55.4 years ) with a clinical suspicion of biliary complications following olt ( increased cholestasis or abnormal liver function ) were studied by mri . 
la tc inoltre nel paziente sottoposto ad olt ha problematiche legate allesposizione alle radiazioni ionizzanti , specie nella popolazione pediatrica , ed allimpiego del mezzo di contrasto , in relazione al fatto che linsufficienza renale una comune complicanza in questi pazienti ( 12%70% ) [ 13 ]  . negli ultimi anni i progressi tecnologici della risonanza magnetica ( rm ) , in particolare luso di apparecchi con gradienti performanti e bobine di superficie , hanno consentito di ottenere immagini t2 pesate con elevata risoluzione spaziale e temporale , in grado di definire , con accuratezza paragonabile alle procedure colangiografiche dirette , tipo , sede e grado di complicanza biliare . 
i contributi della letteratura [ 1 , 2 , 1217 ] che hanno valutato il ruolo della colangio - rm nella detection delle complicanze biliari postolt , riportano valori di sensibilit variabili tra 87 , 5% e 100% e di specificit variabili tra 92% e 100 , valori che costituiscono la premessa per attribuire un ruolo chiave a questa metodica nel follow - up del paziente sottoposto ad olt . 
scopo del presente lavoro valutare , a confronto con le metodiche colangiografiche dirette , il ruolo della colangio - rm nella diagnostica delle complicanze biliari nel paziente adulto sottoposto a olt . materiali e metodi nel periodo compreso tra agosto 2004 e agosto 2008 , 201 pazienti sono stati sottoposti ad olt . 
di questi , 78 pazienti , 53 maschi e 25 femmine , con et media di 55 , 4 anni , che hanno presentato , dopo il trapianto , rialzo degli indici di colestasi o alterazione degli indici di funzionalit epatica , tali da indurre il sospetto clinico di complicanza biliare , sono stati sottoposti a rm . 
in tutti i pazienti sono state eseguite le seguenti sequenze pre - colangiografiche : assiale sdual fast field echo ( ffe ) t1 pesata ( tempo di ripetizione [ tr ] 241 , 58 ms ; tempo di eco [ te ] 2 , 30 ms e 4 , 60 ms ; campo di vista [ fov ] 3838 cm , slice thikness 5 mm ; flip angle [ fa ] 80 ) ; assiale single shot ( ss ) t2 pesata ( tr 429 ms , te 80 ms ; fov 3838 cm ; slice thikness 5 mm ; fa 90 ) ; coronale ss t2 pesata ( tr 756 ms ; te 80 ms ; fov 37 , 537 , 5 cm ; slice thikness 5 mm ; fa 90 ) ; 3d ss - tse cholangiography in the paracoronal plane with respiratory triggering ( tr 1 , 800 ms , te 650 ms , fa 90 , voxel size 0.590.590.8 , thickness 12 mm ) , fat assiale spin echo ( se ) t2 pesata ( tr 432 ms ; te 80 ms ; fov 3838 cm ; slice thikness 5 mm ; fa 90 ) con soppressione del segnale del grasso . 1068 radiol med ( 2010 ) 115 : 10651079 to visualise suppression with the spir technique and a mean duration of 2 : 37 min . subsequently , the anastomotic sites , maximum intensity projection ( mip ) and multiplanar reconstructions ( mpr ) of the biliary tree were obtained . 
the images were evaluated jointly by two radiologists ( 10 and 8 years , respectively , of experience in liver mri ) who subdivided the mri findings into two groups : ( 1 ) absence of complications and ( 2 ) presence of complications . 
in group 2 , the following complications were specified : severe or obstructive anastomotic stricture ( with upstream biliary dilatation ) mild or nonobstructive anastomotic stricture ( without upstream biliary dilatation ) stricture of the intrahepatic biliary tree biloma biliary sludge cholelithiasis patients with negative mri findings underwent monthly clinical , biohumoural and sonographic follow - up for 1 year ; normalisation of the clinical and biohumoural findings was considered evidence of the absence of biliary complications . 
in patients with mri evidence of biliary complications , diagnostic confirmation was obtained from ercp in 13 cases , ptc in 20 , us in ten and ct in two . confirmation was also obtained from surgery in 11 patients who underwent surgical treatment of the complication . ercp , ptc , us , ct and surgery were considered the standards of reference for diagnostic confirmation . 
subsequent clinical , biohumoural and sonographic follow - up showed normalisation of the findings in all of these individuals , and this was considered sufficient to rule out biliary complications . 
in 44 / 78 patients , mri detected the presence of biliary complications ( group 2 : presence of complications ) : severe or obstructive anastomotic strictures : 25 mild or nonobstructive anastomotic strictures : 12 intrahepatic biliary tree strictures : 5 biloma : 9 biliary sludge : 5 cholelithiasis : 4 le sequenze colangiografiche eseguite sono state le seguenti : colangiografica radiale 2d - se , in breath hold , ( tr : 8000 ms , te : 800 ms , fa : 90 , voxel size : 0 , 59 ? 0 , 59 ? 20 mm , slice thickness : 20 mm , angolo radiale di 12 ) , soppressione del segnale del grasso ottenuta con tecnica spectral presaturation inversion recovery ( spir ) e durata media di 1 min 36 s . colangiografica 3d turbo spin echo ( tse ) ss , sul piano paracoronale con trigger respiratorio ( tr di 1800 ms , te di 650 ms , fa di 90 , dimensioni del voxel di 0 , 590 , 590 , 8 , thickness di 12 mm ) , soppressione del segnale del grasso con tecnica spir e durata media di 2 min 37 s . sono poi state eseguite , per meglio visualizzare la sede di anastomosi , ricostruzioni in proiezione di massima intensit ( mip ) e multiplanari ( mpr ) dellalbero biliare . 
nel gruppo 2 sono specificati i seguenti tipi di complicanze : stenosi anastomotiche severe o ostruttive ( con dilatazione della via biliare a monte ) ; stenosi anastomotiche lievi , non ostruttive ( senza dilatazione della via biliare a monte ) ; stenosi delle vie biliari intraepatiche ; bilomi ; sludge biliare ; litiasi coledocica . in presenza di rm negativa il paziente stato sottoposto a follow - up , clinico - bioumorale ed ecografico , con cadenza mensile per 1 anno ; la normalizzazione del quadro clinico e bioumorale stata considerata espressione di assenza di complicanze bilari . 
in presenza di complicanze biliari evidenziate dalla rm , si ottenuta conferma diagnostica mediante ercp in 13 casi , ptc in 20 casi , ecografia in 10 casi e tc in 2 casi . 
alla luce delle tecniche di riferimento , sono state calcolate sensibilit , specificit , valore predittivo negativo ( vpn ) , valore predittivo positivo ( vpp ) ed accuratezza diagnostica della colangio - rm nella identificazione delle complicanze biliari nel paziente trapiantato . risultati in tutti i casi la colangio - rm ha consentito di identificare correttamente il tipo e la sede dellanastomosi biliare , sia radiol med ( 2010 ) 115 : 10651079 1069 fig . 
in 44 / 78 pazienti la rm ha evidenziato la presenza di complicanze biliari ( gruppo 2 : presenza di complicanze ) : stenosi anastomotiche severe o ostruttive : 25 ; stenosi anastomotiche lievi , non ostruttive : 12 ; stenosi vie biliari intraepatiche : 5 ; bilomi : 9 ; sludge biliare : 5 ; litiasi coledocica : 4 . la complicanza di pi frequente riscontro stata la stenosi . 
trentatre / 42 stenosi si sono verificate dopo tre mesi dal trapianto , classificabili quindi come complicanza tardiva . in 9 / 42 casi la stenosi stata precoce , ovvero si verificata entro tre mesi dal trapianto ; di queste 7 coinvolgevano lanastomosi coledoco - coledocica e 2 lanastomosi biliodigestiva . 
la diagnosi di complicanze formulata dalla colangio - rm stata confermata mediante ptc ( 20 casi ) , ercp ( 13 casi ) , ecografia ( 10 casi ) , tc ( 2 casi ) e chirurgia ( 11 casi )  . 
in due casi ( 1 stenosi dellanastomosi bilio - digestiva , 1 stenosi delle vie bilari intraepatiche ) la complicanza identificata alla colangio - rm non stata confermata dallecografia e dallercp eseguite successivamente pertanto sono state considerate falsi positivi della rm . 
ptc e ercp hanno evidenziato 4 complicanze biliari non evidenziate alla colangio - rm , casi pertanto considerati come falsi negativi rm : in un 1 paziente con diagnosi rm di stenosi singola delle radiol med ( 2010 ) 115 : 10651079 1070 fig 2a - d radial mr cholangiography se 2d images ( a , b ) and mip reconstructions ( c , d ) show a marked focal decrease in calibre of the common bile duct at the anastomotic site , due to a significant stricture of choledocho - choledocho anastomosis ( arrows in b e d )  . 
2a - d nelle immagini radiali colangiografiche ( a , b ) apprezzabile una significativa riduzione del lume del coledoco in corrispondenza della sede di anastomosi , reperto compatibile con stenosi dellanastomosi ( freccia ) ed evidente anche nelle ricostruzioni mip ( c , d , frecce )  . surgical conversion from choledochocholedochal to biliodigestive anastomosis was necessary in only 1 / 9 cases of early stricture . 
in two cases ( one stenosis of the biliodigestive anastomosis and one stenosis of the intrahepatic biliary tree ) , the complications identified at mrc were not confirmed by us and at ercp and were consequently vie biliari intraepatiche la ptc ha evidenziato anche concomitante stenosi dellanastomosi bilio - digestiva e sludge biliare ; in 1 paziente con diagnosi rm di stenosi ostruttiva dellanastomosi la ptc ha evidenziato concomitanti stenosi multiple delle vie biliari intraepatiche ; in 1 paziente con diagnosi rm di stenosi dellanastomosi coledoco - coledocica la ercp ha mostrato anche la presenza di biloma , successivamente confermato anche da tc e ptc . i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) ed accuratezza diagnostica della colangio - rm sono riportati in tabella 3 . discussione nei pazienti sottoposti a olt non infrequente , sia radiol med ( 2010 ) 115 : 10651079 1071 fig . 
3a - h in patient with bilio - enteric anastomosis post - olt , axial and coronal ss t2 - w images ( a , b , arrow ) show dilatation of biliary systemultiple smooth signal voids were also seen inside the biliary ducts ( arrow in b )  . 
3a - h in paziente sottoposto ad olt , con anastomosi bilio - digestiva , gi nelle sequenze assiali e coronali t2 pesate ( a , b , freccia ) si osserva dilatazione delle vie biliari soprattutto in sede periiliare in corrispondenza della conflueza dei dotti . 
nella sequenza colangiografica 3d sul piano coronale ( c , d , freccia ) e nella ricostruzione mip ( e ) si confermano la dilatazione delle vie biliari , i difetti di segnale allinterno dei rami biliari di maggiore calibro e la stenosi dellanastomosi bilio - enterica . 
4a - e le immagini della sequenza colangiografica radiale e coronale ( a - c ) e le ricostruzioni mip ( d ) mostrano la presenza di stenosi anulare dellanastomosi coledocica termino - terminale con conseguente sistema biliare a monte dellanastomosi ( freccia in b )  . 
allesame rm sono inoltre apprezzabili alcuni difetti di segnale compatibili con la natura litisiaca nel coledoco subito a monte dello sbocco nellansa duodenale ( freccia in c )  . lesame colangiografica eseguito per via percutanea ( e ) conferma la stenosi dellanastomosi , la dilatazione del sistema biliare preanastomotico ed evidenzia presenza di formazioni litiasiche subito a monte dellanastomosi ( freccia in e ) non visualizzabili alla colangio - rm . radiol med ( 2010 ) 115 : 10651079 1073 fig 5a - e axial and coronal ss t2 - w images ( a , b ) show huge fluid collection with regular borders and homogeneous high signal intensity ( biloma )  . 
5a - e nelle sequenze assiali e coronali t2 pesate ( a , b ) apprezzabile in sede sottoepatica una grossolana raccolta a margini ben definiti e a segnale omogeneamente elevato . 
ptc and ercp demonstrated four biliary complications that had been missed at mrc and were consequently considered false negative mri results : in one patient with an mri diagnosis of single stricture of the intrahepatic biliary tree , ptc demonstrated a concomitant stricture of the biliodigestive anastomosis and biliary sludge ; in one patient with an mri diagnosis of obstructive stenosis of the anastomosis , ptc demonstrated concomitant multiple strictures of the intrahepatic biliary tree ; in one patient with an mri diagnosis of stenosis of the choledochocholedochal anastomosis , ercp also demonstrated the presence of a biloma , later confirmed by ct and ptc . sensitivity , specificity , ppv , npv and diagnostic accuracy of mrc are reported in table 3 . discussion detecting biohumoural alterations in liver function parameters , especially increased cholestasis , is not uncommon in either the immediate postoperative period or several months after olt . 
similarly , biliary complications have a nonspecific clinical and biohumoural presentation characterised by vague abdominal pain , fever or simply progressive asymptomatic cholestasis , with increased serum alkaline phosphatase levels [ 18 ]  . 
this setting calls for a panoramic , possible noninvasive , imaging modality capable of visualising the entire biliary tree to allow for a highly accurate detection or exclusion of biliary complications , as this will heavily influence patient management . mrc fully meets these requirements , and its role in the study of biliary complications post - olt has been widely nellimmediato post - trapianto che a distanza , la comparsa di alterazioni bioumorali dei parametri di funzionalit epatica in particolare degli indici di colestasi . 
tali alterazioni sono del tutto aspecifiche , potendo indifferentemente essere secondarie a rigetto , colestasi farmacologia , epatite virale , e recidiva della patologia epatica nativa [ 18 ] e possono in alcuni casi risolversi del tutto spontaneamente . 
in modo del tutto analogo anche le complicanze biliari hanno solitamente una presentazione clinica e bioumorale del tutto aspecifico , caratterizzata da vago dolore addominale , febbre o anche semplicemente colestasi asintomatica progressiva , con rialzo dei livelli sierici di fosfatasi alcalina [ 18 ]  . 
in questo contesto si rende necessaria una metodica di imaging panoramica , possibilmente non invasiva , che visualizzi lintero albero biliare permettendo , con elevata accuratezza , lindividuazione o lesclusione di complicanze biliari dato che condiziona fortemente il successivo management del paziente . la colangio - rm risponde pienamente a questi requisiti diagnostici e dalla fine degli anni 90 ad oggi il suo ruolo nello studio delle complicanze biliari in pazienti sottoposti a olt stato valutato da numerosi contributi della letteratura [ 1 , 2 , 12 , 14 , 15 ] che ne hanno enfatizzato gli eccellenti risultati . 
nel nostro lavoro sono stati valutati con colangiorm pazienti trapiantati di fegato , con alterazione degli indici bioumorali di funzionalit epatica , tali da indurre il sospetto clinico di complicanza biliare . 
il protocollo desame da noi utilizzato ha comunque sempre previsto anche limpiego di sequenze non colangiografiche dedicate alla valutazione del parenchima epatico , indispensabili per lindividuazione e la caratterizzazione di eventuali alterazioni estrinseche alle vie biliari , ( raccolte biliari , sierose o emorragiche ) e dei loro rapporti con il sistema biliare , in particolare con la sede di anastomosi , nonch di lesioni focali parenchimali , secondarie alla complicanza biliare . 
 un primo rilevante risultato del nostro studio stato la possibilit di identificare e valutare , in tutti i casi , lanastomosi biliare , sia di tipo bilio - enterica che coledoco - coledocica . 
nelle immagini rm - colangiografiche lanastomosi coledoco - coledocica viene individuata come focale radiol med ( 2010 ) 115 : 10651079 1075 investigated since the late 1990s [ 1 , 2 , 12 , 14 , 15 ] with excellent results . 
the scanning protocol always involved acquisition of noncholangiographic sequences for evaluation of liver parenchyma , which are essential to identify and characterise any extrinsic alterations of the biliary tree ( bile , serum or blood collections ) , and their relationship with the biliary tract , in particular , with anastomosis site , and with parenchymal focal lesions secondary to biliary complications . the first important outcome of our study was the ability to constantly identify and analyse the biliary anastomosis , whether bilioenteric or choledochocholedochal . 
at the level of the anastomosis , a regular concentric thickening of the walls of the common bile duct , normally characterised by low signal intensity , may be observed on axial t1and t2 - weighted sequences [ 1 , 3 , 18 ]  . in the presence of biliodigestive anastomosis , a technique only used when choledochocholedochal anastomosis is not possible or when complications of the standard anastomosis cannot be treated with percutaneous corrective procedures , mrc shows a shorter common bile duct that ends below the hepatic hilum in continuity with a loop characterised by a jejunal - type fold pattern [ 1 , 3 , 18 ]  . 
furthermore , the residual native segment of the recipients common bile duct may be recognised distally at the intrapancreatic level down to its opening into the duodenum . biliary strictures are the most frequent complication of olt , and they are usually classified as anastomotic or nonanastomotic [ 1 ]  . 
anastomotic strictures , identified in 37 / 78 patients in our series , appear on mrc as a marked focal decrease in calibre of the common bile duct and , in the most severe cases , complete disappearance of the hyperintense signal of the postanastomotic common bile duct . 
the presence of stenosis must always also be verified on axial images , which will show a more or less marked concentric thickening of the common bile duct wall due to fibrosis , which shows low signal intensity both on t1and t2 - weighted sequences . in the case of biliodigestive anastomosis , strictures appear on mrc as a focal absence of biliary signal in the segment immediately above the jejunal loop , corresponding to the anastomosis site . 
furthermore , in these patients , dilatation of the upstream biliary tract is always present . the presence or absence of significant preanastomotic variazione di calibro localizzata di solito al terzo medio del coledoco , tra i segmenti pree post - anastomotico . 
a livello anastomotico , nelle sequenze assiali t1 e t2 pesate si pu osservare un regolare ispessimento concentrico delle pareti dellepatocoledoco che normalmente caratterizzato da bassa intensit di segnale [ 1 , 3 , 18 ]  . nellanastomosi bilio - digestiva , tecnica riservata a casi in cui non sia possibile eseguire lanastomosi coledococoledocica o in caso di complicanze dellanastomosi classica non trattabili con le tecniche correttive percutanee , la colangio - rm mostra un coledoco pi corto , che termina al di sotto dellilo epatico in continuit con unansa caratterizzata da plicatura di tipo digiunale [ 1 , 3 , 18 ]  . 
distalmente inoltre possibile riconoscere il tratto nativo residuo del coledoco del ricevente a livello intrapancreatico , sino al suo sbocco nellansa duodenale . le stenosi biliari sono la pi frequente complicanza dellolt e sono classicamente distinte in anastomotiche e non anastomotiche [ 1 ]  . 
la stenosi anastomotica , riscontrata in 37 / 78 pazienti della nostra serie , appare alla colangio - rm come netta e focale riduzione di calibro della via biliare che pu giungere , nelle forme pi serrate , alla completa scomparsa del segnale iperintenso del coledoco a valle . 
la presenza della stenosi deve comunque essere verificata anche nelle immagini assiali , dove si pu riscontrare ispessimento concentrico , pi o meno marcato , della parete del coledoco dovuto alla fibrosi , a bassa intensit di segnale sia nelle sequenze t1 che t2 pesate . nellanastomosi bilio - digestiva , la stenosi si visualizza , nelle immagini colangiografiche , come focale assenza del segnale biliare nel tratto subito a monte dellansa digiunale , corrispondente alla sede di anastomosi cui , nelle immagini assiali , corrisponde ispessimento focale di basso segnale della parete dellepatocoledoco prima dellansa digiunale . 
in questi pazienti inoltre sempre presente dilatazione del sistema biliare a monte . la presenza o assenza di significativa dilatazione del sistema biliare a monte della sede di anastomosi ( valutata sia nelle immagini colangiografiche che in quelle assiali ) consente di distinguere tra stenosi severe o ostruttive e non severe o non ostruttive . 
nella nostra serie una significativa dilatazione biliare pre - anastomotica stata riscontrata in tutti i casi di stenosi dellanastomosi bilio - digestiva e in 8 / 11 casi di stenosi dellanastomosi termino - terminale che hanno poi richiesto una correzione chirurgica mediante conversione dellanastomosi in bilio - digestiva . 
nella nostra serie abbiamo riscontrato 5 1076 radiol med ( 2010 ) 115 : 10651079 biliary dilatation ( identified both on cholangiographic and axial images ) allows distinction to be made between severe or obstructive and mild or nonobstructive strictures . 
in our series , significant preanastomotic biliary dilatation was seen in all cases of biliodigestive anastomotic stricture and in 8 / 11 cases of termino - terminal anastomotic stricture , which later required surgical repair with conversion into a biliodigestive anastomosis . 
in our series , we identified five cases of nonanastomotic stricture , most of which had involvement of the intrahepatic bile ducts , which appear on mrc as linear areas of abrupt decrease in duct calibre and , in the most severe cases , as complete disappearance of the signal . 
at stenoses sites , axial images may show low - signal circumferential thickening of the duct wall . if the origin is ischaemic , the finding of other associated complications such as bilomas ( five cases in our series ) or areas of intrahepatic abscess formation is also frequent . 
bilomas are early complications that generally appear in the immediate postoperative period and are caused [ 13 ] by focal necrosis or tensions at the anastomosis site or , more rarely , by thrombosis of the hepatic artery or sphincter of oddi dysfunctions , which increase intraductal pressure , in particular , at the anastomosis site . at mri , bilomas appear as circumscribed collections with high signal intensity on t2 - weighted images , which are not always easy to distinguish from ascites or serous collections . 
the biliary nature of the collection should be suspected on the basis of the site perihilar or periductal and demonstration on cholangiographic or axial images of an interruption between the collection and the duct lumen , usually at the level of the anastomosis [ 1 ]  . 
sludge and stones are rather frequent , and they are usually associated with stenosis , bacterial or fungal infection , biliodigestive anastomosis and ischaemia [ 1 , 2 ]  . 
they appear on cholangiographic images as signal defects prevalently located in the larger bile ducts . whereas all complications of the typical choledochocholedochal anastomosis identified in our series were correctly depicted by mrc , the technique yielded two false positive results : one stenosis of the biliodigestive anastomosis with preanastomotic dilatation , and one stenosis of the intrahepatic biliary tree ; both were unconfirmed by the subsequent diagnostic examinations . 
one possible reason for these errors is that the peculiar anatomical configuration of the biliodigestive anastomosis makes it difficult to identify at diagnostic imaging , as reported in the literature [ 1 , 20 , 21 ]  . 
although the jejunal loop is antiperistaltic , its motility may frequently form casi di stenosi non anastomotiche , con prevalente interessamento delle vie biliari intraepatiche che , nelle immagini colangiografiche , si presentano come zone lineari di brusca riduzione del calibro biliare , sino alla scomparsa del segnale nelle forme pi serrate . 
il biloma una complicanza precoce che generalmente insorge nellimmediato post - trapianto ed dovuta [ 13 ] a focale necrosi o tensioni a livello della sede di anastomosi , pi raramente a trombosi dellarteria epatica o a disfunzioni dello sfintere di oddi che aumentano la pressione endocoledocica , in particolare in sede di anastomosi . 
la natura biliare della raccolta va sospettata sulla base della sede , peri - ilare e peri - coledocica , e sulla dimostrazione , nelle immagini colangiografiche o assiali , di una soluzione di continuo tra la raccolta e il lume coledocico in genere a livello dellanastomosi [ 1 ]  . 
sludge e litiasi sono piuttosto frequenti e generalmente si associano a stenosi , infezioni batteriche o fungine , anastomosi bilio - digestiva , ischemia [ 1 , 2 ]  . 
 mentre tutte le complicanze a carico dellanastomosi classica coledoco - coledocica riscontrate nella nostra casistica sono state correttamente identificate e descritte allesame di colangio - rm , due sono stati i falsi positivi della colangio - rm : 1 stenosi dellanastomosi bilio - digestiva con dilatazione pre anastomotica e 1 stenosi delle vie biliari intraepatiche , entrambe non confermate ai successivi esami diagnostici eseguiti . 
un possibile motivo di tali errori che lanastomosi bilio - digestiva , come anche riportato in letteratura [ 1 , 20 , 21 ] di pi difficile valutazione agli esami di imaging per la sua particolare configurazione anatomica . 
 frequente , nonostante lansa digiunale sia antiperistaltica , che la sua motilit possa causare angolature e ripiegamenti temporanei della sede di anastomosi che possono mascherarla negli esami di imaging o causare transitorie ectasie del sistema biliare a monte . 
a tal proposito in letteratura [ 20 , 21 ] vengono enfatizzati i vantaggi dellimpiego di mezzi di contrasto ad escrezione epato - biliare , non impiegati nella nostra casistica , che , accentuando il segnale della bile , migliorano la visualizzazione dellanastomosi bilio - digestiva e la detection delle complicanze a tale livello . 
 la bassa risoluzione spaziale , limite della sequenza radiol med ( 2010 ) 115 : 10651079 1077 transient angulations and folds at the anastomosis site , which may obscure it on imaging or cause transient ectasia of the upstream biliary tract . 
in this respect , the literature [ 20 , 21 ] emphasises the advantages of using contrast agents with hepatobiliary excretion ( not used in our series ) , which enhances the bile signal , thus facilitating visualisation of the biliodigestive anastomosis and detecting complications at this site . the low spatial resolution , a limitation of cholangiography that has been reported [ 12 ] to cause underor overestimation of strictures , was improved in our study by using additional axial and coronal t1and t2 - weighted sequences , which allowed a more precise evaluation of strictures and anastomoses , particularly in patients in whom superimposed abdominal fluid , collections or bilomas could hamper anastomotic site assessment . in our series , we had four false negative results : one stenosis of the biliodigestive anastomosis , one of the intrahepatic ducts , one case of biliary sludge and one biloma , all of which were demonstrated at subsequent ptc and ercp . 
in one case , mri showed multiple strictures of the intrahepatic ducts , and for this reason , the patient underwent ptc , which demonstrated the concurrent presence of biliary sludge and biliodigestive stenosis , which were not visualised on mri due to a suboptimal visualisation of the anastomosis site . 
in another patient with obstructive stenosis of the choledochocholedochal anastomosis , ptc showed the concomitant presence of stenosis of the intrahepatic bile ducts not seen on mri because of artefacts due to poor patient cooperation in maintaining the breathhold . 
direct cholangiography , whether endoscopic or percutaneous , has the dual advantage of affording high - quality images of the biliary tree , which facilitates detecting biliary complications and providing a therapeutic option for nonsurgical management of olt patients . 
however , as reported in the literature [ 2 , 3 ] , these procedures are invasive and associated with a major complication rate of 3.4% in the case of ptc and 5% in the case of ercp . 
in our series , only in two cases did we have to perform direct cholangiography due to complications seen at mri but subsequently not confirmed , whereas in all other cases , mrc proved to be colangiografica , emerso in altri lavori [ 12 ] dove ha comportato una sotto o sovra stima delle stenosi , nel nostro studio stata recuperata dallesecuzione di sequenze aggiuntive assiali e coronali , t1 e t2 pesate , che hanno consentito una pi precisa valutazione delle stenosi e delle anastomosi , in particolare nei pazienti in cui la sovrapposizione di liquidi addominali , raccolte o bilomi poteva creare problemi di valutazione della sede di anastomosi nella sequenza colangiografica . quattro sono stati i casi falsi negativi della nostra serie : 1 stenosi dellanastomosi bilio - digestiva , 1 stenosi delle vie biliari intraepatiche , 1 caso di sludge biliare e 1 biloma tutti evidenziati dalle successive ptc ed ercp . 
in un caso la rm ha evidenziato la presenza di stenosi multiple delle vie biliari intraepatiche per le quali il paziente stato sottoposto a ptc , che ha evidenziato la concomitante presenza di fango biliare e stenosi della bilio - digestiva , non visualizzata allrm per la non ottimale visualizzazione della sede di anastomosi ; in questo caso la dilatazione delle vie biliari intraepatiche stata interpretata come conseguenza delle stenosi intraepatiche . 
in un altro paziente con stenosi ostruttiva dellanastomosi coledoco - coledocica , la successiva ptc ha mostrato la concomitante presenza di stenosi delle vie biliari intraepatiche non visualizzate in rm per la presenza di artefatti da scarsa collaborazione del paziente in particolare a mantenere lapnea . 
in un terzo caso la rm ha evidenziato una stenosi dellanastomosi termino - terminale confermata dalla ercp , nello stesso caso ptc e tc hanno mostrato la concomitante presenza di un biloma , non visualizzato in rm per presenza di abbondante liquido periepatico . complessivamente laccuratezza diagnostica della colangio - rm nel nostro studio stata del 93 , 9% , la sensibilit del 93 , 5% , la specificit del 94 , 4% , il valore predittivo positivo e negativo rispettivamente del 96 , 7% e del 89 , 5% , valori sostanzialmente sovrapponibili a quelli dei vari lavori analoghi riportati in letteratura [ 1 , 2 , 12 , 1417 , 22 ]  . le tecniche colangiografiche dirette , sia endoscopiche che percutanee , hanno il vantaggio di fornire immagini di alta qualit dellalbero biliare che consentono di identificare agevolmente le complicanze biliari ed al tempo stesso offrono possibilit terapeutiche che in un alta percentuale di casi permettono una gestione non chirurgica del paziente sottoposto ad olt . 
tuttavia come riportato in letteratura [ 2 , 3 ] tali procedure sono invasive e possono comportare complicanze maggiori in circa il 3 , 4% dei casi per la ptc e nel 5% dei casi per la ercp . 
nella nostra casistica in soli due casi stato necessario ricorrere alle tecniche colangiografiche dirette per complicanze evidenziate allesame rm e non confermate successivamente , mentre in tutti i restanti casi la colangio - rm ha fornito un quadro diagnostico ottimale che ha permesso di selezionare i pazienti candidati allesecuzione delle procedure dirette con finalit terapeutica , ed al tempo stesso di scegliere la tecnica 1078 radiol med ( 2010 ) 115 : 10651079 an excellent diagnostic tool that enabled both selection of candidates for direct procedures for therapeutic purposes and choice of the most appropriate direct technique ( percutaneous or endoscopic )  . limitations of our study include the lack of a reference test having absolute accuracy to verify the negative mri findings , which were ascertained by clinical , biohumoural and sonographic follow - up only . 
surgical confirmation of mri findings was available for 11 cases only . diretta pi indicata , percutanea o endoscopica . tra i limiti del nostro lavoro , vanno citati la mancanza di un test di riferimento del tutto accurato per la verifica dei reperti negativi della rm che sono stati controllati solo mediante follow - up clinico - bioumorale ed ecografico . 
analogamente i risultati positivi della colangio - rm sono stati verificati mediante il ricorso ad altre metodiche di imaging considerate come indagini di riferimento ovviamente anche esse soggette a limiti di accuratezza , mentre solo in 11 casi abbiamo ottenuto riscontro chirurgico del reperto rm . 
its diagnostic accuracy and lack of invasiveness justify its systematic use in the presence of liver - function alterations to exclude or demonstrate the presence of biliary complications , select patients for direct cholangiographic procedures for therapeutic purposes and to choose the most appropriate direct therapeutic technique . 
this way , it is possible to limit the number of direct procedures performed without therapeutic purposes in symptomatic patients who do not have biliary complications and to correctly select the most appropriate treatment on the basis of mrc images . 
furthermore , compared with direct cholangiographic techniques , mri has the advantage of a more precise evaluation of extrinsic alterations of the biliary tree that are frequently associated with biliary complications in olt patients and the presence of which may affect treatment strategies . i risultati del nostro studio confermano le evidenze della recente letteratura sul contributo diagnostico della colangio - rm nello studio delle complicanze biliari del paziente trapiantato . 
la sua accuratezza diagnostica e la non invasivit ne giustificano limpiego sistematico in presenza di alterazione degli indici di funzionalit epatica , al fine di escludere o evidenziare la presenza di complicanza biliare , selezionare i pazienti candidati a procedure colangiografiche dirette , con finalit terapeutica e scegliere lapproccio diretto pi indicato . 
in questo modo possibile ridurre il numero di procedure dirette eseguite senza finalit terapeutica , in pazienti sintomatici ma senza complicanza biliare , e scegliere correttamente il tipo di trattamento pi indicato sulla base delle immagini fornite dalla colangio - rm . 
radiological detection of carcinoid tumours is limited by typical tumour location throughout the gastrointestinal tract or appendix and is therefore dependent on the tumour being large enough to make it recognisable in that site . 
a particularly important role is played by intraoperative ultrasound in defining the exact number of lesions , their relationship with adjacent vascular structures and the pancreatic duct for the purposes of correct surgical planning ( enucleation or resection )  . 
in the setting of nonfunctioning endocrine tumours ( nfets ) , which manifest late as large masses causing compression symptoms or as incidental findings , imaging is not primarily aimed at tumour detection , as this is relatively easy given the large size of the lesions . 
rather , its role is to characterise the tumour and , in particular , to differentiate pancreatic nfet from ductal adenocarcinoma , as in comparison , malignant nfets have a more favourable prognosis ( 5 - year survival rate 40% compared with 3%5% for adenocarcinoma ) and therefore require different treatment approaches . 
in 80% of cases , nfets have a typical imaging appearance : location in the pancreatic head , large dimensions ( diameter between 5 and 15 cm , > 10 cm in 30% of cases ) , capsule , sharp and regular margins owing to the expansile and noninfiltrative growth riassunto nei tumori endocrini funzionanti ( tef ) , il ruolo dellimaging principalmente volto alla loro identificazione , intesa come precisazione del numero e della topografia delle lesioni . 
nel carcinoide lidentificazione con imaging limitata dalla sua tipica sede in corrispondenza della parete gastro - intestinale o appendicolare ed pertanto vincolata a dimensioni sufficienti a renderlo riconoscibile in tali sedi . 
il tef pi frequente linsulinoma , che comunemente si presenta con un aspetto tipico di lesione ipervascolarizzata alle indagini di tomografia computerizzata multidetettore ( tcms ) e di risonanza magnetica ( rm )  . 
particolare importanza riveste lindagine ecografica ( us ) intra - operatoria al fine di precisare lesatto numero di lesioni , i loro rapporti vascolari e con il dotto pancreatico principale , per una corretta pianificazione della strategia chirurgica ( enucleazione o resezione )  . 
nei tumori endocrini non funzionanti ( tenf ) , che si manifestano tardivamente come masse voluminose con sintomi compressivi , o come reperti occasionali , i quesiti allimaging sono rappresentati non tanto dalla identificazione , agevole per le cospicue dimensioni , ma dalla tipizzazione , in particolare nelle forme pancreatiche nei confronti delladenocarcinoma duttale , rispetto al quale anche i tenf maligni hanno prognosi migliore ( sopravvivenza a 5 anni del 40% versus quella delladenocarcinoma del 3%5% ) , per cui richiedono strategie terapeutiche diverse ; in queste lesioni necessario inoltre un corretto bilancio , essendo spesso tumori maligni , ed infine il loro follow - up . 
nell80% le forme non funzionanti hanno un aspetto imaging peculiare ( o tipico ) : sede cefalo - pancreatica , cospicue dimensioni ( diametro tra 5 e 15 cm ; nel 30% dei casi > 10 cm ) , capsulate , a contorni 1048 radiol med ( 2010 ) 115 : 10471064 pattern , solid density and arterial hypervascularity . 
lastly , a small percentage of nfets has yet a different appearance ( unusual ) due to the cystic nature and / or diffuse location throughout the pancreatic parenchyma . keywords neuroendocrine tumours pancreas computed tomography magnetic resonance imaging netti e regolari per il tipo di crescita espansiva e non infiltrativa , densit solida , con ipervascolarizzazione arteriosa . 
in una minima percentuale i tumori neuroendocrini non funzionanti infine mostrano un aspetto ancora diverso ( inusuale ) per la loro natura cistica e / o diffusa a tutto il parenchima pancreatico . parole chiave tumori neuroendocrini pancreas tomografia computerizzata risonanza magnetica introduction introduzione given their anatomopathological characteristics , gastroenteropancreatic ( gep ) tumours [ 1 ] pose distinctive diagnostic imaging and prognostic problems . 
in functioning endocrine tumours ( fets ) , the role of imaging [ 2 , 3 ] is mainly to detect the tumour that is , verify lesion number and location . 
imaging does , however , play role in patient follow - up . in contrast , in nonfunctioning endocrine tumours ( nfets ) , which manifest late as large masses causing compression symptoms or as incidental findings , imaging is not primarily aimed at tumour detection [ 2 , 3 ] , as this is relatively easy given the large size of the lesions . 
rather , its role is to characterise the tumour and in particular to differentiate pancreatic nfet from ductal adenocarcinoma , as in comparison , malignant nfets have a more favourable prognosis ( 5 - year survival rate 40% compared with 3%5% for adenocarcinoma )  . 
as they are often malignant [ 4 ] nfets also require accurate staging and appropriate follow - up . pathological premise to imaging in relazione alle loro caratteristiche anatomo - patologiche , i tumori neuroendocrini gastro - entero - pancreatici ( gep ) [ 1 ] pongono problematiche di imaging diagnostiche e prognostiche peculiari . 
nei tumori endocrini funzionanti ( tef ) , i quesiti allimaging [ 2 , 3 ] sono principalmente volti alla loro identificazione , intesa come precisazione del numero e della topografia delle lesioni , non interessano la tipizzazione , gi espressa dalla sindrome clinica , poco riguardano il bilancio di lesione , essendo frequentemente benigni ; in ultimo , limaging deve infine rispondere al quesito del follow - up . al contrario , nei tumori endocrini non funzionanti ( tenf ) , che si manifestano tardivamente come masse voluminose con sintomi compressivi , o come reperti occasionali , i quesiti allimaging [ 2 , 3 ] sono rappresentati non tanto dalla identificazione , agevole per le cospicue dimensioni , ma dalla tipizzazione , in particolare nelle forme pancreatiche nei confronti delladenocarcinoma duttale , rispetto al quale anche i tenf maligni hanno prognosi migliore ( sopravvivenza a 5 anni del 40% versus quella delladenocarcinoma del 3%5% ) , per cui richiedono strategie terapeutiche diverse ; in queste lesioni richiesto quindi un corretto bilancio , essendo spesso tumori maligni [ 4 ] , ed infine il loro follow - up . regardless of their functioning state [ 1 , 3 ] , neuroendocrine gep tumours often present with constant features ( typical appearance ) : solid , well - circumscribed and large ( with the exception of insulinomas ) masses , with rounded appearance or with lobulated borders , often with a partial or complete pseudocapsule and richly vascular due to poor stromal component . 
as they have expansile growth margins , they tend the adjacent anatomical structures , compressing them rather than invading them . to respect premesse anatomo - patologiche allimaging indipendentemente dallo stato funzionale [ 1 , 3 ] , si presentano frequentemente con caratteristiche costanti ( aspetto tipico ) : neoformazioni solide , ben circoscritte , voluminose , ad eccezione degli insulinomi , rotondeggianti o con margini policiclici , spesso dotate parzialmente o completamente di pseudocapsula , riccamente vascolarizzate , per presenza di scarso stroma tumorale . possono essere presenti aree di emorragia e di necrosi , la quale se estesa conferisce un aspetto cistico alla neoplasia . 
avendo margini di crescita di tipo espansivo , radiol med ( 2010 ) 115 : 10471064 1049 these characteristics of shape and vascularity justify the macroscopic differences between these tumours and pancreatic ductal adenocarcinoma . 
in some cases , they may show the typical appearance of a malignant neoplasm , with involvement of the surrounding fat tissue , neoplastic satellite nodules [ 5 ] , invasion of the bowel wall or adjacent organs ( common bile duct , spleen ) or may present neoplastic thrombosis of large - diameter vascular structures . more rarely , they display different features ( atypical appearance ) : considerable dimensions , firm texture , whitish in colour due to highly abundant fibrotic stroma , indistinct margins and invasive behaviour similar to pancreatic forms of adenocarcinomas . 
the presence of abundant stroma , which endows the tumour with an invasive nature , and the particular location along the pancreatic duct , has recently made possible the detection of small pancreatic nonfunctioning endocrine tumours , causing marked dilatation of the pancreatic duct and onset of pancreatic symptoms . although regressive cystic changes are rather common in large solid endocrine masses , cystic endocrine tumours are rare , accounting for some 5%10% of the cases reported in the literature [ 1 ]  . 
when they appear as cystic lesions ( unusual appearance ) , they are generally unilocular , consisting of a single cystic cavity lined with endocrine cells and frequently separated from the remaining parenchyma by a fibrous pseudocapsule . 
they rarely appear multilocular , with sparse fibrous septations lined with endocrine cells . although most gep tumours are well - differentiated , a minority are poorly differentiated , with marked cellular atypia , prevalence of solid areas , presence of necrosis and a high mitotic index . 
negative prognostic indicators include large dimensions of the primary lesion , invasive tumour growth , presence of tumour necrosis , vascular invasion , marked cytological atypia , elevated mitotic index evaluated on the bases of the mitotic count [ number of mitoses per high power field ( hpf ) ] and cell proliferation marker ( ki67 protein ) ( expressed only in cycling cells )  . in an effort to provide a clearer prognosis and on the basis of the classification proposed by the world health organization ( who ) in 2000 [ 1 , 4 ] , two main categories of pancreatic endocrine identified with completely different prognoses : a clearly minority group ( 2%5% ) of poorly differentiated endocrine tumours comprising carcinomas with high - grade malignancy and unfavourable prognosis ; and a much larger group consisting tumours were tendono a rispettare le strutture anatomiche adiacenti , nei confronti delle quali hanno un atteggiamento compressivo piuttosto che infiltrativo . queste caratteristiche di forma e vascolarizzazione giustificano la loro diversit macroscopica rispetto alladenocarcinoma duttale pancreatico . 
talora possono mostrare aspetti propri di una neoplasia maligna : coinvolgimento del tessuto adiposo circostante , noduli neoplastici satelliti [ 5 ] , infiltrazione della parete intestinale , di organi vicini ( coledoco , milza ) , o presentare fenomeni di trombosi neoplastica di strutture vascolari di grosso calibro . pi raramente mostrano caratteristiche diverse ( aspetto atipico ) : dimensioni considerevoli , consistenza sostenuta e colorito biancastro a causa dello stroma fibrotico molto abbondante , margini indistinti , atteggiamento infiltrativo , analogamente nelle forme pancreatiche agli adenocarcinomi . 
la presenza di stroma abbondante , che conferisce loro un atteggiamento di tipo infiltrativo , e la particolare sede a ridosso del dotto di wirsung ha consentito negli ultimi anni lidentificazione di tumori endocrini non funzionati pancreatici di ridotte dimensioni , causa di marcata dilatazione del dotto di wirsung e responsabili di sintomatologia di tipo pancreatitico . sebbene modificazioni cistiche di tipo regressivo siano abbastanza frequenti in neoplasie endocrine solide di grandi dimensioni , le neoplasie endocrine cistiche vere e proprie sono rare , rappresentando circa il 5%10% dei casi riportati in letteratura [ 1 ]  . 
quando si presentano come lesioni cistiche ( aspetto inusuale ) , sono generalmente uniconcamerate , costituite da una singola cavit cistica tappezzata da cellule endocrine , frequentemente separate dal restante parenchima da una pseudocapsula fibrosa . raramente appaiono pluriconcamerate , con radi setti fibrosi rivestiti da cellule endocrine . nella maggior parte i gep sono ben differenziati ; una minoranza di casi presenta tuttavia un grado di differenziazione istologica scarsa con marcate atipie cellulari , prevalenza di aree solide , presenza di necrosi ed elevato indice mitotico . 
sulla base del quadro istologico risulta difficile predirne il comportamento biologico ; si considerano pertanto inequivocabili segni di malignit linvasione degli organi circostanti , la presenza di metastasi linfonodali , epatiche [ 5 ] ed a distanza . 
elementi prognostici negativi sono considerati le grandi dimensioni della lesione primitiva , la crescita tumorale infiltrativa , la presenza di necrosi tumorale , di invasione vascolare , le atipie citologiche di grado marcato , lelevato indice mitotico , valutato in base alla conta mitotica ( numero di mitosi per campo a forte ingrandimento , cfi ) e lindice proliferativo o ki67 ( espressione di proteine legate al ciclo cellulare )  . 
 ai fini di una maggior chiarezza prognostica , in base ad una classificazione proposta dallworld health 1050 radiol med ( 2010 ) 115 : 10471064 of well - differentiated endocrine tumours , which include benign lesions and low - grade carcinomas . 
the only real criteria for malignancy , which are easier to document , are the presence of nodal and / or hepatic metastases and the extrapancreatic extension of the tumour with invasion of adjacent organs and / or structures . however , as most of these tumours at diagnosis show no signs of metastasis and appear confined , the problem arises of obtaining information regarding their biological behaviour , as metastases can appear even many years later . 
this is why the who proposed several histopathological criteria as indicators of malignancy , with the aim of dividing the tumours into prognostic groups according to their probable biological behaviour . 
the parameters taken into consideration are : diameter ( 2 cm ) ; angioinvasion ; perineural invasion ; number of mitoses / 10 per hpf ; cell proliferation marker ( ki67 )  . neuroendocrine tumours are therefore subdivided into three categories : 1 . 
carcinoids : according to this classification , carcinoids belong to the group of well - differentiated endocrine tumours . functioning neuroendocrine tumours carcinoid imaging detection [ 3 , 6 ] is limited by its typical location in the gastrointestinal tract at the level of the appendix , ileum organization ( who ) nel 2000 [ 1 , 4 ] , sono state individuate per le neoplasie endocrine del pancreas due principali categorie a prognosi completamente diversa : un gruppo nettamente minoritario ( 2%5% ) di neoplasie endocrine scarsamente differenziate , costituite da carcinomi ad alto grado di malignit ed a prognosi infausta ; un gruppo maggiormente rappresentato di neoplasie endocrine ben differenziate che includono lesioni benigne e i carcinomi a basso grado di malignit . 
per predire il comportamento biologico di queste neoplasie non si utilizzano pi pertanto i tradizionali criteri istopatologici di malignit ( atipie citocariologiche , mitosi , necrosi ) ; gli unici veri criteri di malignit , pi facili da documentare sono la presenza di metastasi , linfonodali e / o epatiche , lestensione extrapancreatica della neoplasia , intesa come infiltrazione di organi e / o strutture adiacenti . 
 poich tuttavia , la maggior parte di queste neoplasie al momento della diagnosi non presenta metastasi ed appaiono confinate , si pone il problema di avere informazioni circa il loro comportamento biologico , dal momento che le metastasi potranno comparire anche a molti anni di distanza . 
per questo sono stati proposti dalla who come indicatori di malignit alcuni criteri istopatologici , allo scopo di dividere tali neoplasie in gruppi prognostici in funzione del loro probabile comportamento biologico . 
i parametri considerati sono : il diametro ( 2 cm ) langioinvasione linvasione perineurale il numero di mitosi 10 per cfi lindice proliferativo cellulare ( ki67 ) le neoplasie neuroendocrine vengono pertanto suddivise in tre categorie : 1 . 
carcinomi endocrini scarsamente differenziati o carcinomi a piccole cellule : sono altamente maligni , si presentano spesso con metastasi a distanza , hanno pi di 10 mitosi per campo o un ki67 maggiore del 15% , spesso con angioinvasione o invasione perineurale . 
when it reaches a diameter of at least 15 mm , the carcinoid appears as a solid mass , often with irregular morphology due to the presence of dense strands radiating out into the tumour periphery . these strands result from mesenteric fibrosis in response to the release of serotonin from the carcinoid . 
multidetector - row computed tomography ( mdct ) : pancreatic contrast phase , axial images ( a - c , f ) , mip , d and vr , e . 
a , b ileal carcinoid ( a , arrow ) of considerable size ( 40 mm ) with vascular pattern ; calcified mesenteric adenopathies ( a , short arrows ) ; multiple liver metastases with vascular pattern ( b )  . 
ce small ileal carcinoid ( 5 mm ) with hypervascular pattern ( arrow ) and nodular morphology arising from the wall of an ileal loop and protruding into the lumen , which is distended by water . 
a , b carcinoide ileale ( a freccia ) di considerevoli dimensioni ( diametro : 40 mm ) , vascolarizzato ; adenopatie mesenteriali calcifiche ( a frecce corte ) ; multiple metastasi epatiche vascolarizzate ( b )  . 
c - e carcinoide ileale di piccole dimensioni ( diametro : 5 mm ) , ipervascolarizzato ( freccia ) , con morfologia nodulare , ad origine dalla parete di unansa ileale , protrudente nel lume intestinale , disteso da acqua . 
diagnosi istologica su pezzo operatorio di splenopancreasectomia per pancreatiti ricorrenti . 1052 radiol med ( 2010 ) 115 : 10471064 typically located in the right iliac fossa if arising from the appendix or ileum and is hypervascular , with enhancement in the pancreatic phase on computed tomography ( ct ) ( fig . 1a ) ; and hyperintense in t2 - weighted sequences , with intense - to - moderate enhancement on magnetic resonance ( mr ) imaging . 
lesions may be solitary or multiple ; located deep within the pancreas or superficially ; or seen modifying the pancreatic profile , with solid density and arterial hypervascular pattern [ 10 ]  . they therefore typically appear hypoechoic at ultrasound ( us ) , often with transient enhancement at contrastenhanced us ( ceus )  . 
sono pertanto tipicamente ipoecogeni allindagine ecografica ( us ) con impregnazione spesso fugace dopo lutilizzo di mezzi di contrasto ecografici ; particolare importanza riveste tale metodica intra - operatoria [ 11 ] al fine di precisare lesatto numero di lesioni , i loro rapporti vascolari e con il dotto pancreatico principale , per una corretta pianificazione della strategia chirurgica ( enucleazione o resezione )  . radiol med ( 2010 ) 115 : 10471064 1053 fig . 
a - d typical appearance : small lesion ( arrow ) located in the pancreatic tail in a , b and isthmus in c , d , with hypervascular pattern , hyperattenuating in the pancreatic phase at mdct ( a ) and mr imaging ( d ) , and more hypoattenuating due to washout in the ct venous phase ( b )  . e , f atypical appearance . 
tc multistrato ( a , b , e , f ) ; fase contrastografica pancreatica ( a , e ) , venosa ( b , f ) ; ricostruzioni mpr curvilinee ; risonanza magnetica ( c , d ) : sequenza t1 - dipendente in fase pre ( c ) e post - contrastografica ( d ) sul piano assiale . 
piccola lesione ( freccia ) localizzata alla coda in a , b e allistmo in c , d del pancreas , ipervascolarizzata , iperdensa in fase contrastografica pancreatica tc ( a ) e rm ( d ) , pi ipodensa per wash - out in fase venosa tc ( b )  . 
pi raramente gli insulinomi mostrano caratteristiche imaging morfologiche e densitometriche differenti dallaspetto tipico ( o atipico ) , rappresentate principalmente dagli insulinomi a 1054 radiol med ( 2010 ) 115 : 10471064 12 ] , lesions appear moderately hyperintense in t2 - weighted sequences and hypervascular after contrast - agent administration . cystic insulinomas are relatively uncommon lesions that appear hypoattenuating in the preand postpancreatic and venous phases at mdct and with fluid - type signal given their cystic nature at mr imaging . 
they may be unior multilocular , delimited by a peripheral wall and show contrast enhancement at both mdct and mr imaging and are often more evident in the late phase [ 10 ]  . calcified insulinomas , or pedunculated insulinomas , protrude from the pancreatic surface and are connected to the pancreatic tissue by a thin pedicle , and insulinomas with extrapancreatic location are all very rare lesions . because only 10% of insulinomas are malignant at diagnosis , there is rarely a need to stage the tumour . 
mdct is useful in the short - term follow - up of insulinomas immediately after surgical or laparoscopic resection for identifying and monitoring complications in the immediate postoperative period ( purulent collections secondary to superinfections , haematomas secondary to vascular lesions )  . imaging ( mdct and mr ) is rarely warranted for long - term follow - up , which is only required in malignant forms . gastrinoma gastrinomas [ 3 ] also have a more frequent ( typical ) imaging appearance . 
they display low signal intensity in t1 - weighted mr sequences , high signal intensity in t2 - weighted sequences and enhancement in the pancreatic phase [ 7 , 12 ]  . 
in 30%40% of cases , these lesions have an atypical appearance , with location in the pancreas or duodenal wall , smaller size ( diameter 1 cm ) , solid density and arterial hypervascularity . 
 as 60% of gastrinomas is malignant [ 1 ] , ct and mr imaging play an important role in evaluating locoregional spread of the disease ( invasion of adjacent organs , arterial and venous invasion ) and identifying locoregional and distant adenopathies and , above all of liver metastases , which appear as solid lesions with a hypervascular ( fig . 3c , d ) or hypovascular pattern . 
 infine , rari sono gli insulinomi calcifici , quelli peduncolati , protrudenti dalla superficie pancreatica e connessi al tessuto ghiandolare pancreatico da sottile peduncolo , e quelli infine a sede extra - pancreatica . solo il 10% degli insulinomi sono maligni al momento della diagnosi . 
la tcms utile metodica di imaging nel followup degli insulinomi a breve termine , subito dopo trattamento di resezione , sia chirurgica che laparoscopica di tali lesioni , al fine di identificare e monitorare complicanze dellimmediato post - operatorio ( raccolte purulente secondarie a sovrainfezioni , ematomi secondari a lesioni vasali )  . raro lapporto dellimaging ( tcms ed rm ) nel follow - up a lungo termine , richiesto infatti solo nelle forme maligne . 
small nodular lesions ( a , b arrow ) 20 - mm in diameter located in the gastrinoma triangle with hypervascular pattern and adhering to the third through fourth portions of the duodenua single liver metastasis ( a arrowhead ) with hypervascular pattern is also visible . 
multiple liver metastases , some appearing with hypervascular pattern ( short arrow ) and others enhanced by opaque contrast agent ( lipiodol ) due to chemoembolisation ( arrowhead ) are also visible . 
solid mass appearing with hypervascular pattern bordered by a more vascular peripheral ring in mdct pancreatic phase ( e , f arrow ) , with periampullary location in the pancreatic head . 
dilatation of the main pancreatic duct ( f ) and common bile duct , in the lumen of which a stent can be seen ( e , f arrowhead )  . 
tc multistrato : fase contrastografica pancreatica ; mpr coronale ( a ) , sagittale ( b ) , curvilinea ( f ) ; immagini assiali ( c - e )  . 
piccola lesione nodulare ( a , b freccia ) con diametro di 20 mm localizzata nel triangolo dai gastrinomi , ipervascolarizzata , adesa alla parete della terza - quarta porzione duodenale . 
neoformazione solida , ipovascolarizzata , delimitata da cercine periferico pi vascolarizzato allindagine tc in fase contrastografica pancreatica ( e , f freccia ) in sede cefalopancreatica peri - papillare ; dilatazione del dotto pancreatico principale ( f ) e del coledoco , nel cui lume presente stent ( e , f testa di freccia )  . 
metastasi epatica ( f freccia corta ) parzialmente contrastata da mdc opaco ( lipiodol ) per chemioembolizzazione . 1056 radiol med ( 2010 ) 115 : 10471064 the immediate postoperative period ( purulent collections secondary to superinfections ; haematomas secondary to vascular lesions )  . 
they are located in the pancreas [ glucagonomas more frequently bodytail ; adrenocorticotropic hormone ( acth ) omas and pancreatic polypeptide ( pp ) omas more frequently in the head ] , are generally solitary , large in size and have a hypovascular or hypervascular pattern that is often heterogeneous due to areas of liquefactive necrosis produced by haemorrhagic phenomena . 
this group of tumours tends to be malignant ( 60%75% ) , presenting with adenopathies and liver and bone metastases [ more common in vasoactive intestinal peptide ( vip ) omas ] at diagnosis . 
in all of these lesions , the role of imaging in staging and follow - up is similar to that played in gastrinomas , both in resectable and nonresectable forms . tcms ha un ruolo nel follow - up a breve termine , dopo trattamento di resezione sia chirurgica che laparoscopica , per identificare e monitorare le complicanze dellimmediato post - operatorio ( raccolte purulente secondarie a sovrainfezioni , ematomi secondari a lesioni vasali )  . 
glucagonomi , vipomi , acthomi , ppomi : sono neoplasie neuroendocrine funzionanti rare [ 3 ] clinicamente diverse tra loro , ma accomunate da un aspetto imaging aspecifico : sede pancreatica ( glucagonomi pi frequenti al corpo - coda ; acthomi e ppomi pi frequenti alla testa ) , generalmente uniche , cospicue dimensioni , con ipoo ipervascolarizzazione arteriosa , spesso disomogenea per presenza di aree colliquate , necrotiche per fenomeni emorragici . 
anche in tutte queste lesioni le problematiche imaging di bilancio e follow - up sono analoghe a quelle dei gastrinomi , sia nelle forme resecabili che in quelle non resecabili . 
they are found in the pancreas , usually in the head , and are large ( diameter 515 cm , in 30% of cases > 10 cm ) , solid , hypervascular and capsulated , with smooth and regular margins given their expansile and noninvasive growth pattern [ 2 , 15 ]  . 
large tumours are characterised by rapid and long - lasting enhancement in dynamic phases , with an accumulation of contrast microbubbles in the late phase . mediumsmall tumours show an initial intense enhancement ( or capillary blush ) followed by a progressive washout and hypoechoic appearance in the late phase . 
lastly , these lesions can cause dilatation of the pancreatic duct at the bodytail , with atrophy of the pancreatic parenchyma due to chronic obstructive pancreatitis , as well as dilatation of the common bile duct . 
in larger nfets with intratumoural haemorrhage , t1 - weighted sequences may reveal hyperintense foci related to haemosiderin deposits [ 7 , 12 ]  . a rare imaging finding of a nfet is a typical appearance , with hypervascular pattern , nodular morphology , but small in size . 
mostrano ecostruttura ipoecogena solitamente disomogenea per la presenza di aree di necrosi o emorragia intratumorali dovute alle loro dimensioni o degenerazione cistica ; talora possono formarsi piccole calcificazioni . quando si utilizzano mezzi di contrasto ecografici , hanno tipico enhancement risultando iperecogeni , tuttavia con diversi patterns di impregnazione in base alle dimensioni della neoplasia ed alla presenza di vasi intratumorali . 
i tumori di dimensioni cospicue si caratterizzano per la rapida e duratura impregnazione nelle fasi dinamiche con vero e proprio accumulo di microbolle di mezzo di contrasto ecografico in fase tardiva . 
nei tumori di dimensioni medio - piccole allimpregnazione ecografica intensa ( o capillary blush ) , segue una progressiva dismissione del mezzo di contrasto ecografico con quindi aspetto ipoecogeno della lesione in fase tardiva . 
possono presentare unarea centrale necrotica o fibrotica , ipodensa in fase contrastografica pancreatica o di degenerazione cistica con valori densitometrici di tipo liquido ; nei tenf pi voluminosi a causa di fenomeni emorragici , possono essere presenti calcificazioni in sede centrale . 
nei tenf pi voluminosi , in seguito a fenomeni emorragici , possono essere presenti focolai iperintensi in t1 , in relazione a depositi emosiderinici [ 7 , 12 ]  . raro il riscontro imaging di tenf con quadro tipico , con ipervascolarizzazione arteriosa , morfologia nodulare , ma con ridotte dimensioni , responsabili , a causa della loro 1058 radiol med ( 2010 ) 115 : 10471064 fig . 
a - c large mass situated in the pancreatic head , with hypervascular pattern , hyperattenuating in the pancreatic phase ( a ) , more hypoattenuating in the venous phase ( b ) , with little washout in the late phase ( c ) , indicative of malignant nfet . 
this unresectable nfet was shown at fine - needle - aspiration cytology ( fnac ) to be a poorly differentiated endocrine carcinoma [ mitoses / high - power field ( hpf ) > 10 , ki67 > 15% ]  . 
d - f large hypervascular mass of the bodytail appearing hyperintense in the mr pancreatic phase ( d ) , less intense in the venous phase ( e ) , with washout in the late phase ( f ) , where the lesion presents signal reduction ( prevalently stromal nfet )  . 
risonanza magnetica ( d - f ) : sequenze t1 - dipendenti in fase post - contrastografica pancreatica ( d ) , venosa ( e ) , tardiva ( f ) sul piano assiale . 
a - c voluminosa massa cefalopancreatica ipervascolarizzata , iperdensa in fase contrastografica pancreatica ( a ) , pi ipodensa in fase venosa ( b ) , con scarso washout in fase tardiva ( c ) , tenf maligno . 
la lesione infiltra il duodeno ( testa di freccia ) , la vena mesenterica superiore ( freccia ) e la vena porta ( freccia corta ) : tenf non resecabile ; allesame citologico mediante fnab : carcinoma endocrino scarsamente differenziato ( cfi > 10 ; ki67 > 15% )  . 
d - f voluminosa massa del corpo - coda ipervascolarizzata , iperintensa in fase contrastografica rm pancreatica ( d ) , meno intensa in fase venosa ( e ) , con wash - out in fase tardiva ( f ) , in cui la lesione presenta riduzione del segnale ( tenf a prevalenza stromale )  . 
la lesione infiltra i vasi splenici non pi riconoscibili ; sono presenti circoli collaterali ( freccia ) gastro - epiploici ( tenf resecabile ) ; allesame istologico dopo intervento resettivo di splenopancreasectomia : carcinoma endocrino ben differenziato ( cfi : 5 ; ki67 : 7% )  . 
these include mucinous cystic tumours , pseudocysts , the rare variants of ductal adenocarcinoma with cystic features such as the anaplastic type , and noncystic mucinous adenocarcinoma . lenta crescita , di dilatazione del dotto di wirsung e atrofia del corpo - coda con linsorgenza di pancreatite cronica ostruttiva a monte . 
a , b a large mass located in the pancreatic bodytail with 120 - mm diameter and hypervascular pattern , hypoattenuating in the pancreatic phase due to the prevailing stromal component , invading the splenic vessels and stomach ( a , arrow )  . 
at ct follow - up after chemotherapy ( b ) , a hypovascular liver metastasis is visible ( arrowhead ) , along with more evident gastric invasion ( arrow ) ( disease progression )  . 
the parenchyma appears to be replaced by the large , prevalently solid , hypervascular mass in d , which is depicted as a solid - cystic type mass invading the splenic veins in e , consisting of microcysts ( arrow ) , macrocysts ( some with thickened and vascular walls ) , septations ( short arrows ) and solid hypo / hypervascular nodular areas ( dotted arrow )  . 
the mass is displacing the second portion of the duodenum and adheres to the superior mesenteric artery ( arrowhead ) and vein ( dotted arrow ) , which it compresses without invasion ( cystic nfet ) fig . 
a , b voluminosa massa del corpo - coda pancreatici con diametro di 120 mm , ipovascolarizzata , ipodensa in fase contrastografica pancreatica per prevalente componente stromale , infiltrante i vasi splenici e lo stomaco ( a freccia )  . 
al controllo tc dopo trattamento chemioterapico ( b ) , comparsa di metastasi epatica ipovascolarizzata ( testa di freccia ) ; pi evidente linfiltrazione ( freccia ) gastrica ( progressione di malattia )  . 
cospicuo aumento in dimensioni di tutta la ghiandola pancreatica ( d , e ) , a profili bozzuti ; il parenchima sostituito da voluminosa massa prevalentemente solida , iper - / ipovascolarizzata in d , infiltrante i vasi splenici di tipo solidocistico in e , costituita da microcisti ( freccia ) , macrocisti alcune con parete ispessita , vascolarizzata e setti ( frecce corte ) , e da aree nodulari solide ipo - / ipervascolarizzate ( freccia tratteggiata ) ; numerose calcificazioni . 
delimitata da una spessa capsula periferica ( freccia ) , vascolarizzata , iperdensa in fase pancreatica ; al suo interno presente sottile setto ( freccia corta ) vascolarizzato in fase pancreatica . 
the aim is to guide the clinician and the surgeon in distinguishing nfets from other pancreaticduodenal masses , particularly ductal adenocarcinoma , and then to choose the most appropriate treatment [ 16 , 19 , 20 ]  . 
when presented with an imaging pattern of a pancreatic mass with typical , atypical or unusual appearance and that is nonetheless resectable , an advisable approach in the absence of distant metastases is radical resection with curative intent . 
the cytological examination is indicative of a well - differentiated endocrine carcinoma ( proliferation index or ki67 > 5% ; number of mitoses per hpf between 2 and 10 ) , palliative surgical resection of the pancreatic mass and liver metastasis is also indicated . 
in the presence of multiple liver metastases , the combination of surgical resection of the pancreatic mass and chemoembolisation of the liver metastases is recommended [ 2 , 16 , 19 , 20 ]  . in contrast , in the presence of cytological findings of a poorly differentiated endocrine carcinoma ( proliferative index or ki67 > 15% ; number of mitoses per hpf > 10 ) , the unfavourable prognosis suggests medical treatment with chemotherapy , somatostatin analogues or radiometabolic therapy , possibly associated with cytoreductive surgery with palliative intent to control symptoms [ 2 ]  . lastly , in the event of a mass with typical , atypical or unusual features that is locally advanced and unresectable due to vascular invasion and / or distant metastases , fnac and cytological examination still play a role . 
if the mass is an nfet , establishing the degree of differentiation of the lesion can be useful for deciding on the best chemotherapeutic options , with somatostatin analogues or radiometabolic therapy [ 2 ]  . 
in the presence of a generally poorly differentiated nfet that is either locally advanced and / or has distant metastases and is recurrent or unresponsive to treatment , nuclear medicine is able to select patients for 4 . 
 le indagini di imaging ( us , tc , rm ) , spesso espletate in prima battuta , si affiancano pertanto alla medicina nucleare , recentemente anche in associazione ( tomografia computerizzata a emissione di fotoni singoli [ spect ] - ct ) [ 21 ] nonch allindagine citologica di prelievo ottenuto mediante agoaspirazione con ago sottile ( fnab ) , al fine di guidare il clinico e il chirurgo nel distinguere i tenf da altre neoformazioni pancreatico - duodenali in particolare dalladenocarcinoma duttale , per poter scegliere il tipo di terapia pi corretto [ 16 , 19 , 20 ]  . 
a fronte di un quadro imaging di neoformazione pancreatica con aspetto tipico , atipico o inusuale , ma comunque resecabile , in assenza di metastasi a distanza suggeribile il ricorso alla chirurgia resettiva radicale con intento curativo . 
in presenza di un quadro citologico suggestivo per adenocarcinoma o altre neoplasie le possibilit terapeutiche sono solo di tipo chemioterapico . se al contrario lesame citologico indicativo di un carcinoma endocrino ben differenziato ( indice proliferativo o ki67 > 5% ; numero di mitosi per cfi tra 2 e 10 ) , trova ugualmente [ 4 ] indicazione un trattamento chirurgico resettivo della massa pancreatica con intento palliativo e della metastasi epatica ; in presenza di molteplici metastasi epatiche preferibile associare alla resezione chirurgica della massa pancreatica la chemioembolizzazione delle metastasi epatiche [ 2 , 16 , 19 , 20 ]  . in presenza al contrario di un quadro citologico di un carcinoma endocrino scarsamente differenziato ( indice proliferativo o ki67 > 15% ; numero di mitosi per cfi > 10 ) , date le sfavorevoli prospettive prognostiche , suggeribile un trattamento medico di tipo chemioterapico o con analoghi della somatostatina o radiometabolico , associato ad un eventuale trattamento chirurgico di debulking a scopo palliativo per un controllo dei sintomi [ 2 ]  . nellevenienza infine di una massa con caratteristiche tipiche , atipiche , inusuali localmente avanzata in quanto non resecabile per infiltrazione vascolare e / o con metastasi a distanza trova ancora utilit il ricorso alla fnab e allesame citologico , al fine di stabilire nel caso si tratti di un tenf il 1062 radiol med ( 2010 ) 115 : 10471064 radiometabolic treatment with somatostatin analogues labelled with beta - emitting isotopes , which enables highdose irradiation of the primary tumour while sparing healthy organs [ 22 ]  . as these lesions are often malignant , staging [ 2 , 10 , 16 , 19 , 20 ] performed by mdct and mr imaging principally involves determining the t parameter for locoregional spread , i.e. 
the presence of collateral compensatory circulation may be associated . also important for correct staging is the n parameter , i.e. identification of locoregional retroperitoneal adenopathies or distant adenopathies ; as well as the m parameter , which indicates the presence of liver metastases . 
they are often numerous and of large dimensions . a rare event is the finding of bone metastases , which appear as areas of bone lysis of various skeletal segments [ 22 ]  . short - term follow - up in resectable lesions after surgical or laparoscopic resection is always aimed at identifying and monitoring possible infectious or vascular complications in the immediate postoperative period . 
long - term follow - up is aimed at spatial and morphological evaluation of recurrent lesions and their response to medical and / or chemotherapeutic and radiometabolic treatment , as well as detecting liver metastases and evaluating their response to medical and / or chemotherapeutic treatment with chemoembolisation , thermoablation and radiometabolic therapy [ 19 , 20 ]  . another important aim is to identify and subsequently monitor any extrahepatic metastases , especially bone metastases . 
 grado di differenziazione della lesione e decidere per la pi opportuna tra le varie opzioni terapeutiche di tipo chemioterapico , con analoghi della somatostatina , o di tipo radiometabolico [ 2 ]  . 
si associa la presenza di circoli collaterali di compenso . importante nel bilancio anche il parametro n , ovvero lidentificazione di adenopatie retroperitoneali loco - regionali o a distanza e infine il parametro m , che si identifica nelle metastasi epatiche . 
the recist system [ 8 , 23 ] differentiates between measurable lesions ( long - axis diameter > 10mm ) and nonmeasurable lesions ( long - axis diameter < 10 mm )  . 
il sistema recist [ 8 , 23 ] distingue infatti le lesioni in misurabili ( diametro maggiore superiore a 10 mm ) e non misurabili ( diametro maggiore inferiore a 10 mm ) ; valuta solo il diametro maggiore della lesione pi grande , mediante immagine tc acquisita con modalit standardizzate ( collimazione di almeno 5 mm )  . 
musumeci2 1dipartimento di radiologia cardiovascolare , 2dipartimento di cardiochirurgia , ospedale san camillo - forlanini , roma , italy 3dipartimento di scienze radiologiche , universit di roma sapienza , ospedale sant andrea , via di grottarossa 1035 , 00189 roma , italy 4dipartimento di medicina sperimentale , universit di roma sapienza , roma , italy correspondence to : c.n. 
the aim of our work was to assess the role of dual - source computed tomography ( dsct ) in the preoperative evaluation of coronary artery disease in patients scheduled for noncoronary cardiac surgery . 
patients positive for significant lesions or with nondiagnostic image quality due to artefacts or severe calcifications underwent coronary angiography ( n = 19 ) and were excluded from the study . 
no maces were recorded during the perioperative period ; three noncardiac complications ( one surgical revision for bleeding , one cardiac tamponade and one respiratory insufficiency ) and one death related to severe respiratory insufficiency were observed . 
lo scopo di questo lavoro analizzare il ruolo dellangiografia coronarica mediante tomografia computerizzata dual source ( tcds ) nella valutazione preoperatoria del rischio cardiovascolare in pazienti che devono essere sottoposti ad intervento di cardiochirurgia non coronarica . 
i pazienti risultati negativi sono stati inviati direttamente allintervento chirurgico ( n = 81 ) ; i pazienti positivi per stenosi significative o in cui la qualit delle immagini risultava non diagnostica sono stati sottoposti ad angiografia coronarica invasiva ( n = 19 ) ed esclusi dallo studio . 
nei pazienti operati e studiati solo con tcds stata valutata la frequenza di eventi cardiaci avversi maggiori ( ecam ) peri - operatoria e ad un follow - up di 3 mesi . 
nel periodo peri - operatorio non sono stati osservati ecam e si sono registrate 3 complicanze non cardiache quali una revisione chirurgica per sanguinamento , una mediastinite ed una insufficienza respiratoria ; in tale periodo si verificato un solo decesso per cause non cardiache correlato ad una severa insufficienza respiratoria . 
lo studio coronarico mediante tcds permette di escludere la presenza di malattia ateromasica significativa nei pazienti che devono essere sottoposti ad radiol med ( 2010 ) 115 : 10281037 1029 keywords dual - source computed tomography coronary disease cardiac surgery major adverse cardiac events coronary angiography interventi di cardiochirurgia non coronarica e non necessita di una conferma tramite angiografia invasiva , se lo studio presenta una qualit dimmagine diagnostica . nei pazienti in cui si osservano stenosi significative o non possibile la valutazione di tutti i segmenti necessaria lesecuzione di una coronarografia . parole chiave tomografia computerizzata dual - source malattia coronarica cardiochirurgia eventi avversi cardiaci maggiori coronografia introduction introduzione multidetector - row computed tomography ( mdct ) provides accurate evaluation of coronary atherosclerosis [ 14 ]  . 
in particular , the latest generation of 64 - detector - row ct systems has a high negative predictive value ( npv ) in ruling out the presence of coronary artery disease ( cad ) in patients with a heart rate < 65 bpm [ 59 ]  . 
various studies have validated the accuracy of coronary ct in the preoperative evaluation of cardiovascular risk in patients scheduled for cardiac valve surgery , with conventional coronary angiography as the reference standard [ 1014 ]  . 
current dual - source ct systems ( dsct ) , which are equipped with two tube - detector arrays mounted on a single gantry and offset by 90 , achieve a temporal resolution of 83 ms , thus freeing image quality from heart rate and obtaining elevated study quality at a broad range of heart rates without the need for pharmacological control [ 1519 ]  . on the basis of this experience , it was decided at our centre to include dsct coronary angiography in the preoperative evaluation of cardiovascular risk in patients scheduled for noncoronary heart surgery . 
therefore , a diagnostic algorithm was developed according to which if dsct ruled out the presence of significant cad , the patient would immediately undergo surgery without the need for invasive angiographic confirmation . 
if , instead , the examination proved to be positive or doubtful due to artefacts or calcification , the patient would undergo conventional coronary angiography . the aim of this paper is to report the frequency of major adverse cardiac events ( maces ) that occurred during the perioperative period and 3 months of follow - up in patients who underwent heart surgery after significant cad had been ruled out by dsct alone . materials and methods patient population between october 2007 and april 2008 , 100 patients la tomografia computerizzata multidetettore ( tcmd ) ha dimostrato di essere una metodica che permette unaccurata valutazione dellaterosclerosi coronarica [ 14 ]  . 
in particolare , lultima generazione di apparecchi per tomografia computerizzata ( tc ) a 64 detettori possiede un elevato valore predittivo negativo nellescludere la presenza di malattia coronarica in pazienti con frequenza cardiaca inferiore ai 65 bpm [ 59 ]  . 
diversi lavori hanno validato laccuratezza della tc coronarica nella valutazione pre - operatoria del rischio cardiovascolare nei pazienti che devono essere sottoposti ad interventi di chirurgia cardiaca valvolare in comparazione con la coronarografia [ 1014 ]  . 
attualmente la tecnologia tc dual source ( tcds ) , nella quale sono presenti due tubi radiogeni con i corrispondenti detettori montati sul medesimo gantry ad un angolazione di 90 , permette di ottenere una risoluzione temporale di 83 millisecondi , svincolando la qualit delle immagini dalla frequenza cardiaca ed ottenendo una elevata qualit di studio in un ampio range di frequenze cardiache senza la necessit di controllo farmacologico [ 1519 ]  . 
 sulla base di tali esperienze , nel nostro centro stato deciso di inserire la coronarografia mediante tcds nella valutazione pre - operatoria del rischio cardiovascolare nei pazienti che devono essere sottoposti ad interventi di cardiochirurgia non coronarica . 
per tale ragione stato sviluppato un algoritmo diagnostico per cui se la tcds esclude la presenza di malattia coronarica significativa il paziente viene sottoposto direttamente allintervento senza lesecuzione di unangiografia coronarica di conferma ; se invece lesame risulta positivo o dubbio , per la presenza di artefatti o calcificazioni , il paziente viene inviato ad eseguire una coronarografia tradizionale . 
 lo scopo di tale lavoro di riportare la frequenza di eventi cardiaci avversi maggiori ( ecam ) intercorsi nel periodo peri - operatorio e ad un follow - up di tre mesi nei pazienti che sono stati indirizzati direttamente allintervento cardiochirurgico dopo lesclusione di patologia coronarica significativa mediante lesecuzione della sola tcds . 
the patients in whom significant stenosis or the presence of motion artefacts or diffuse calcifications prevented evaluation of one or more coronary segments underwent coronary angiography and were excluded from follow - up . 
in patients who underwent dsct alone , the onset of maces during the perioperative period ( up to 30 days ) and during 3 months of follow - up was evaluated . 
exclusion criteria for dsct study were known allergy to iodinated contrast material , nephropathy ( creatinine > 120 mol / l ) , nonsinus rhythm , haemodynamic instability , age < 40 years , presence of cad and prior myocardial infarction . 
the study protocol was approved by the local ethics committee , and all subjects provided written informed consent . study protocol the study was performed using a dual - source scanner ( somatom definition , siemens medical solutions , forchheim , germany )  . 
the scan was acquired in the craniocaudal direction from 1 cm below the level of the tracheal bifurcation to the diaphragmatic dome using the following parameters : detector collimation 320.6 mm ; acquisition slices 640.6 mm acquired with the z - flying focal spot technique and adaptive pitch ( 0.20.35 ) ; gantry rotation time 330 ms . 
a voltage of 120 kv and tube current of 350 mas for both tubes was applied . automatic tube current modulation ( electrocardiographic pulsing ) was used , with maximum intensity applied between 30% and 80% of the cardiac cycle [ estimated computed tomography dose index volume ( ctdivol ) 44 mgy ]  . 
dsct coronary angiography was performed with the biphasic intravenous injection of 80 ml of contrast material ( iomeron 400 , 400 mgi / ml , bracco , milan , italy ) followed by 40 ml of saline solution at an injection rate of 5 ml / s . 
the scan was begun 6 s after an attenuation threshold of 100 hu was reached . image reconstruction and analysis retrospective reconstruction of raw data was performed with a monosegment reconstruction algorithm using data obtained from a quarter rotation of both detectors . 
to evaluate coronary arteries , images were reconstructed in the 5% phases of the rr interval within the window of materiali e metodi popolazione di pazienti sono stati studiati prospetticamente 100 pazienti sottoposti ad angiografia coronarica con tcds e successivamente ad intervento di cardiochirurgia non coronarica al fine di escludere la presenza di malattia ateromasica significativa , nel periodo compreso tra ottobre 2007 ed aprile 2008 . 
i pazienti nei quali stata riscontrata una stenosi significativa o in cui la presenza di artefatti da movimento o di diffuse calcificazioni non permettevano la valutazione di uno o pi segmenti sono stati sottoposti ad angiografia coronarica ed esclusi dal follow - up . 
nei pazienti sottoposti alla sola tcds , stata valutata linsorgenza di eventi cardiaci avversi maggiori nel periodo peri - operatorio ( fino a 30 giorni ) , e ad un follow - up di 3 mesi . 
sono stati classificati come ecam il decesso per cause cardiache [ 20 ] , linfarto miocardico acuto , larresto cardiaco o lesecuzione di una procedura di rivascolarizzazione coronarica non elettiva . 
i criteri di esclusione alla tcds comprendevano : allergia al mezzo di contrasto iodinato , nefropatia ( cretinina > 120 mmol / l ) , ritmo non sinusale , instabilit emodinamica , et inferiore ai 40 anni , presenza di malattia coronarica e pregresso infarto miocardico . 
il protocollo di studio stato approvato dalla commissione etica locale e tutti i soggetti esaminati hanno fornito il consenso informato scritto . protocollo di studio lesame stato eseguito utilizzando uno scanner dual source ( somatom definition , siemens medical solutions , forchheim , germania )  . 
la scansione stata eseguita in direzione cranio - caudale partendo 1 cm sotto il livello della biforcazione tracheale sino al domo diaframmatico , utilizzando i seguenti parametri : collimazione dei detettori , 320 , 6 mm ; strati di acquisizione , 640 , 6 mm acquisiti mediante macchia focale mobile e pitch adattativo ( 0 , 20 , 35 ) ; tempo di rotazione del gantry , 330 ms . 
 stata utilizzata una modulazione automatica della corrente del tubo ( elettrocardiographic [ ecg ] pulsing ) , con la massima intensit applicata tra il 30% e 80% del ciclo cardiaco ( computed tomography dose index volume [ ctdivol ] stimato : 44 mgy )  . 
langiografia coronarica mediante tcds stata eseguita con una iniezione intravenosa bifasica di 80 ml di mezzo di contrasto ( mdc ; iomeron 400 , 400 mgi / ml , bracco , milano , italia ) seguito da 40 ml di soluzione salina a un flusso di 5 ml / s . 
per monitorare il passaggio del mdc stata utilizzata la tecnica del bolus tracking con la regione di interesse posizionata a livello della radiol med ( 2010 ) 115 : 10281037 1031 maximum tube - current intensity ( 30%80% ) , with a slice thickness of 0.75 mm and a reconstruction increment of 0.4 m no manual correction of the echocardiogram ( ecg ) was performed . 
two radiologists worked in consensus to evaluate image quality of coronary segments according to a 2 - point scale : grade 0 , not assessable due to motion artefacts or diffuse calcification ; grade 1 , diagnostic quality sufficient to rule out the presence of significant cad . 
 ricostruzione ed analisi delle immagini per le ricostruzioni retrospettive dei dati grezzi stato utilizzato un algoritmo di ricostruzione mono - segmentario che utilizza i dati ottenuti da un quarto di rotazione di entrambi i detettori . 
per le valutazione delle arterie coronarie , le immagini sono state ricostruite in fasi del 5% dell intervallo rr allinterno della finestra di massima intensit della corrente dei tubi ( 30%80% ) , con uno spessore di strato di 0 , 75 mm ed un incremento di ricostruzione di 0 , 4 m non stata effettuata nessuna correzione manuale dellecg . 
le immagini sono state trasferite ad una workstation dedicata ( leonardo , siemens medical solutions ) equipaggiata con un software commerciale di post - processing cardiaco ( syngo circulation ii , siemens medical solutions )  . 
sono state analizzate le arterie coronarie ed i rami collaterali con un diametro maggiore o uguale ad 1 , 0 mper la valutazione delle coronarie stata utilizzata la classificazione in quindici segmenti dellamerican heart association [ 21 ]  . 
due radiologi in consenso hanno valutato la qualit delle immagini dei segmenti coronarici mediante una scala graduata in 2 punti : grado 0 , non valutabile a causa di artefatti da movimento o diffuse calcificazioni ; grado 1 , immagine di qualit diagnostica sufficiente per escludere la presenza di patologia coronarica significativa . 
1a , b stenosi significativa della coronaria destra ( freccia ) diagnosticata con la tcds ( a ) e confermata allangiografia ( b )  . 1032 radiol med ( 2010 ) 115 : 10281037 and in two patients with diffuse calcifications or severe artefacts . 
in tale gruppo , langiografia ha confermato la presenza di stenosi significativa in 5 dei 6 pazienti in cui era stata posta diagnosi mediante tcds ed in due dei pazienti che presentavano diffuse calcificazioni o severi artefatti . 
i pazienti selezionati presentavano le seguenti caratteristiche demografiche : 50 maschi e 31 femmine ; et media , 60 , 212 , 3 anni ( range , 3284 ) ; frequenza cardiaca media durante lesame , 76 , 512 , 6 bpm ( range , 47106 bpm )  . 
3a - f arterie coronarie esenti da patologia ateromasica , frequenza cardiaca media durante lesame stata di 86 bpm . arteria discendente anteriore ( a , d ) , arteria circonflessa ( b , d ) ed arteria coronaria destra ( c , e , f )  . radiol med ( 2010 ) 115 : 10281037 1033 fig . 
selected patients consisted of 50 men and 31 women with a mean age 60.212.3 ( range 3284 ) years and mean heart rate during examination of 76.512.6 ( range 47106 ) bpunderlying disease and the type of surgical procedure are summarised in table 1 . frequency of major adverse cardiac events during follow - up no maces were observed in the 81 patients included in the study during the perioperative period . 
no maces were observed in the remaining 80 patients during the 3 months of follow - up . discussion patients scheduled for major cardiac surgery undergo a routine preoperative evaluation of coronary risk with conventional angiography , since the concomitant presence of cad worsens the perioperative outcome . 
in this group of patients , mdct in the preoperative evaluation of coronary risk had sensitivity and npv of 100% [ 1014 ] , allowing frequenza degli eventi cardiaci avversi maggiori nel follow - up negli 81 pazienti inclusi nello studio non sono stati osservati eventi cardiaci avversi maggiori intercorsi nel periodo peri - operatorio e si sono registrate 3 complicanze non cardiache quali una revisione chirurgica per tamponamento , una mediastinite ed una insufficienza respiratoria ; in tale periodo si verificato un solo decesso per cause non cardiache correlato ad una severa insufficienza respiratoria . 
 discussione i pazienti che devono effettuare interventi di cardiochirurgia maggiore vengono sottoposti di routine ad una valutazione pre - operatoria del rischio coronarico mediante angiografia , dato che la concomitante presenza di coronaropatia peggiora la prognosi peri - operatoria . 
in tale gruppo di pazienti , la tcmd ha dimostrato di possedere nella valutazione pre - operatoria del rischio coronarico una sensibilit ed un valore predittivo negativo del 100% [ 1014 ] , in tal modo sarebbe possibile evitare lesecuzione dellangiografia invasiva nel 70%80% dei soggetti che devono essere sottoposti allintervento . 
 tali dati concordano con i risultati del nostro studio per table 1 patient disease and surgical technique 1034 disease mitral valve disease aaa + aortic valve disease aortic valve disease mitro - aortic valve disease mitro - tricuspidal valve disease congenital heart disease patologia valvulopatia mitralica aaa + valvulopatia aortica valvulopatia aortica valvulopatia mitro - aortica valvulopatia mitro - tricuspidalica cardiopatia congenita radiol med ( 2010 ) 115 : 10281037 surgical procedure valvolate tube sec . 
indeed , even in centres of excellence , the technique is associated with a small but relevant percentage of complications , both major ( death , stroke , coronary dissection , haemorrhage ) and minor ( inguinal haematoma , pseudoaneurysm at the site of vascular access ) , which overall correspond to a morbidity of 1.8% and mortality of 0.1% [ 20 , 21 ]  . 
tale metodica anche in centri di eccellenza si associa comunque ad una piccola ma rilevante percentuale di complicanze maggiori ( decesso , ictus , dissezione coronarica , emorragie ) e minori ( ematoma inguinale , pseudoaneurisma nel sito di accesso vascolare ) , che corrispondono complessivamente ad una morbilit dell1 , 8% ed una mortalit dello 0 , 1% [ 22 , 23 ] ; inoltre , come dimostrato da stacul et al . 
this demonstrates that dsct can correctly classify patients into a low coronary risk category , with no increase in morbidity and mortality related to maces following noncoronary cardiac surgery . the use of the new dual source technology , thanks to the possibility of studying patients with elevated heart rates , also broadens the patient population eligible for examination by obtaining a greater number of coronary segments of diagnostic quality . 
 [ 14 ] with a 16 - detector syste this frequency is similar to that of other studies done with 64detector systems and heart rate < 65 bpnonetheless , the presence of diffuse coronary calcifications remains the main limitation in evaluating and quantifying atherosclerotic disease , with reduced npv of the technique [ 25 ]  . 
for this reason , we are in agreement with previous findings [ 11 , 12 , 14 ] according to which patients with an elevated agatston score ( > 1 , 000 ) should be sent directly to conventional coronary angiography without performing a ct coronary angiography , which would prove to be nondiagnostic . study limitations the main limitation to performing mdct study with retrospective cardiac gating is the high radiation dose ( 714 msv ) [ 26 ] to which the patient is exposed compared with conventional angiography , which uses on average 7 msv [ 27 ]  . 
for this reason , we recently modified our study protocol with by introducing the step - and - shoot technique in patients with a stable heart rate < 70 bpm and limited calcifications . 
in this way , a diagnostic quality examination can be obtained with much lower radiation doses between 3 and 5 msv which is significantly lower than invasive angiography . in our study , a lower frequency of cad was observed with respect to other studies . 
this may be explained by the fact that in the other studies , the patients selected had severe valve calcification and a much higher mean age , whereas our population was more heterogeneous due to the presence of different heart diseases and a lower mean age . day - surgery e richiede una sorveglianza del paziente da parte di personale specialistico . 
 nella nostra esperienza , nei pazienti risultati negativi alla tcds e sottoposti direttamente allintervento chirurgico non si registrato nessun evento cardiaco avverso maggiore durante il periodo peri - operatorio e ad un follow - up di tre mesi . 
tale risultato dimostra come unesame tcds possa correttamente inquadrare il paziente in una classe di rischio coronarico bassa , senza nessun incremento della morbilit e mortalit correlata ad eventi cardiaci avversi maggiori dopo interventi di chirurgia cardiaca non coronarica . lutilizzo della nuova tecnologia dual source , grazie alla possibilit di studiare soggetti con frequenze cardiache elevate , permette inoltre di ampliare la popolazione di pazienti che pu essere sottoposta allesame ottenendo un maggior numero di segmenti coronarici di qualit diagnostica ; come riportato nel nostro studio infatti solo il 4% dei soggetti risultato non valutabile a causa di artefatti , rispetto al 12 , 1% riportato nello studio di russo et al . 
tale frequenza risulta simile a quello osservata negli studi effettuati con tc a 64 detettori con frequenze inferiori ai 65 bpnonostante ci la presenza di diffuse calcificazioni coronariche rimane il limite maggiore nella valutazione e quantificazione della malattia aterosclerotica , riducendo il valore predittivo negativo della metodica [ 25 ]  . 
per tale ragione siamo concordi con quanto riportato da diversi autori [ 11 , 12 , 14 ] per cui i pazienti con agatson score elevato ( > 1000 ) devono essere inviati direttamente alla coronarografia senza eseguire unangio - tc delle coronarie che risulterebbe non diagnostica . 
 limiti dello studio la maggiore limitazione allesecuzione della tcmd con tecnica di sincronizzazione cardiaca retrospettica risulta essere lelevata dose di radiazioni ( 714 msv ) [ 26 ] a cui il paziente sottoposto rispetto ad una angiografia coronarica , che impiega in media 7 msv [ 27 ]  . 
per tale motivo recentemente abbiamo modificato il protocollo di studio con lintroduzione della tecnica step - and - shoot in pazienti con frequenza stabile inferiore ai 70 bpm e limitate calcificazioni , in tal modo possibile ottenere esami di qualit diagnostica con dosi di radiazioni molto basse comprese tra i 3 e 5 msv , significativamente inferiori rispetto ad un angiografia invasiva . nel nostro studio stata osservata una frequenza di malattia coronarica inferiore rispetto ai precedenti lavori , tale riscontro pu essere spiegato dal fatto che negli altri studi sono stati selezionati pazienti con severa patologia valvolare calcifica ed una et media molto elevata , mentre la nostra popolazione risultava maggiormente eterogenea per la presenza di soggetti con differenti patologie cardiache e con una et media inferiore . 1036 conclusions radiol med ( 2010 ) 115 : 10281037 conclusioni dsct study of the coronary arteries , if of diagnostic quality , is able to rule out the presence of cad in patients scheduled for noncoronary major heart surgery and does not require confirmation with invasive angiography . 
our study confirms the possibility of obtaining a significant reduction in the number of invasive angiographic examinations in patients requiring a preoperative assessment of coronary risk , thus reducing the costs and morbidity associated with this examination . lo studio coronarico mediante tcds , se di qualit diagnostica , permette di escludere la presenza di malattia coronarica nei pazienti che devono essere sottoposti ad intervento di cardiochirurgia non coronarica , e non necessita di una conferma tramite angiografia invasiva . 
il nostro lavoro conferma la possibilit di ottenere una significativa riduzione del numero di angiografie invasive nei pazienti che necessitano una valutazione pre - operatoria del rischio coronarico , riducendo i costi e la morbilit associati a tale esame . 
twenty patients ( 16 women and four men , mean age 55.012.9 years ) with clinical and laboratory evidence of early rheumatoid arthritis ( mean disease duration < 12 months ) were included in our study . mr imaging of the atlantoaxial joint was performed in all patients within 3 months from diagnosis . 
in questo studio , sono stato inclusi 20 pazienti ( 16 donne e 4 uomini ; et media , 55 , 012 , 9 anni ) con diagnosi clinica e di laboratorio di early arthritis reumatoide . 
questultimo risultato positivo in 12 dei 20 pazienti ( 66% ) e gli anticorpi anti - ccp in 15 ( 83% )  . 1112 radiol med ( 2010 ) 115 : 11111120 higher disease activity are likely to be at higher risk of presenting early involvement of the atlantoaxial joint . 
therefore , mr imaging should be included in the diagnostic workup in order to provide reliable guidance for treatment choices . keywords spine atlo - axial joint mr imaging rhaumatoid arthritis conclusioni . 
pertanto , la rm del rachide cervicale dovrebbe essere inclusa nel work - up diagnostico anche per guidare le scelte terapeutiche . parole chiave rachide articolazione atlo - assiale studio rm artrite reumatoide introduction introduzione rheumatoid arthritis ( ra ) is a chronic autoimmune inflammatory disease that selectively involves the joints and that if not treated or not completely controlled by therapy can lead to deformation and destruction of the joint through erosive changes to the cartilage and the subchondral bone [ 1 ]  . 
the prevalence of the disease in italy is in the order of 0.33%0.46% [ 2 ] , with a clear predilection for women ( male / female ratio 1 : 3 )  . 
ra is accompanied by involvement of the cervical spine in 55% of cases and , in particular , by an anterior atlantoaxial subluxation in 25% of cases , whereas involvement of other segments of the spine is rare [ 3 ]  . 
anterior subluxation of the atlantoaxial joint is caused by a weakening or deterioration of the transverse , alar and apical ligaments , and anterior slippage of the atlas can lead to stenosis of the spinal canal and cause compression of the spinal cord [ 4 ]  . controlled clinical trials have shown that an aggressive therapeutic approach can contrast the progression of ra if performed in the initial phases of the disease [ 5 ]  . 
of particular importance , therefore , is the concept of the window of opportunity the initial period when the disease is especially susceptible to disease - modifying antirheumatic drugs ( dmards ) and there is the possibility of halting the pathological process before the damage becomes irreversible [ 6 ]  . damage to the joint occurs very early , and around 75% of patients with recent - onset ra develop erosive changes within the first 2 years of disease [ 7 ]  . 
in the etude et suivi des polyarthrites indiffrencies rcentes ( espoir ) study [ 9 ] performed on 813 patients with early arthritis , radiographically evident erosive changes were present in 20% of patients ( mean duration of disease 107 days )  . magnetic resonance ( mr ) imaging has been shown to be lartrite reumatoide ( ar ) una malattia infiammatoria cronica autoimmune , che colpisce elettivamente le articolazioni e che se non trattata o se non completamente controllata dalle terapie porta alla deformazione e alla distruzione articolare attraverso lerosione della cartilagine e dellosso subcondrale [ 1 ]  . 
la prevalenza della malattia in italia nellordine dello 0 , 33%0 , 46% [ 2 ] con netta predilezione per il sesso femminile ( rapporto uomini : donne di 1 : 3 )  . 
lar si accompagna , nel 55% dei casi , ad un coinvolgimento del rachide cervicale , ed in particolare , ad una sublussazione atlo - assiale anteriore nel 25% dei casi , mentre raro il coinvolgimento degli altri tratti rachidei [ 3 ]  . 
la sublussazione atlo - assiale anteriore dovuta allindebolimento o alla distruzione dei legamenti trasverso , alare ed apicale e lo scivolamento anteriore dellatlante pu portare alla stenosi del canale spinale e provocare compressione del midollo spinale [ 4 ]  . 
assume pertanto valore il concetto di window of opportunity , cio di quel periodo iniziale di malattia particolarmente sensibile allazione dei disease modifying antirheumatic drugs ( dmards ) in cui si ha ancora lopportunit di arrestare il processo patologico prima che il danno che esso provoca diventi irreversibile [ 6 ]  . il danno articolare molto precoce e circa il 75% dei pazienti con ar di recente insorgenza sviluppano erosioni articolari entro i primi 2 anni di malattia [ 7 ]  . 
in un altro studio [ 9 ] condotto sugli 813 pazienti con early arthritis delletude et suivides polyarthrites indiffrencies rcentes ( espoir ) , erosioni radiograficamente evidenti radiol med ( 2010 ) 115 : 11111120 1113 an extremely important modality , given its ability to provide useful information for the clinical management of the patient , in that it is able to evaluate the state of the synovial membrane , the presence of oedema and the degree of vascularity [ 10 ]  . 
the technique has a sensitivity greater than radiography [ 11 ] and is highly useful in the study of changes of the cervical spine in that it is able to depict the synovial pannus causing spinal cord compression and the bone in an early phase of the disease [ 12 , 13 ]  . 
in addition , it has been shown [ 14 ] that an asymptomatic synovitis precedes the clinical manifestations of ra in the early phases of the disease . thus , it is possible that when the disease becomes clinically evident , it is already in the chronic phase . 
the main aims of this study were to define the involvement of the atlantoaxial joint in patients with asymptomatic early ra [ 15 ] ( duration of disease < 12 months ) using mr imaging of the craniovertebral joint and to evaluate the role of mr imaging in detecting early joint involvement . materials and methods in this study , 20 consecutive patients attending the early arthritis clinic of the rheumatology division of the universit cattolica underwent a cervical mr study within 3 months of diagnosis . 
all patients ( 16 women and four men ; age range 3175 years ; mean age 55 years ) met the criteria of the american college of rheumatology ( acr ) for the diagnosis of ra , and symptom onset was less than 1 year [ 16 , 17 ]  . 
all patients were evaluated between june 2007 and january 2009 with a complete physical examination , including evaluation of the number of swollen and painful joints and calculation of the ritchie index and the disease activity score ( das ) [ 18 , 19 ] , a composite index that comprises erythrocyte sedimentation rate ( esr ) levels , global health ( gh ) status , number of swollen joints and the ritchie index . 
in addition , all patients enrolled in the study completed the health assessment questionnaire ( haq ) , which evaluates the functional capacity of the patients in their daily activities , the gh ( analogue scale from 0 to 100 ) and the visual analogue score ( vas ) scale for pain severity ( analogue scale from 0 to 100 )  . 
clinical and demographic data were also collected , as well as smoking habit , family history of rheumatic and / or cardiovascular diseases , comorbidity , extra - articular involvement and haematochemical parameters . 
 la risonanza magnetica ( rm ) risultata una metodica di estrema importanza perch in grado di fornire informazioni utili alla corretta gestione clinica del paziente , in quanto in grado di valutare lo stato della membrana sinoviale , leventuale imbibizione edematosa e lentit della vascolarizzazione [ 10 ] e presenta una sensibilit maggiore rispetto a quella dellesame radiografico [ 11 ] ed inoltre di grande utilit nello studio delle alterazioni del rachide cervicale in quanto permette la visualizzazione del panno sinoviale che provoca la compressione della corda midollare , del midollo spinale e dellosso in una fase molto precoce di malattia [ 12 , 13 ]  . 
il tempo di esposizione delle articolazioni al processo patologico gioca , quindi , un ruolo decisivo e , di conseguenza , molto importante effettuare una diagnosi precoce ed intraprendere un ottimale trattamento terapeutico . 
gli scopi principali di questo studio sono stati quelli di definire il coinvolgimento dellarticolazione atloassiale in pazienti con early artrite reumatoide [ 15 ] ( durata di malattia < 12 mesi ) asintomatici mediante esame rm della giunzione cranio - cervicale e di valutare il ruolo della rm nellevidenziare tale precoce coinvolgimento articolare . materiali e metodi in questo studio 20 pazienti consecutivi afferenti alla early arthritis clinic della divisione di reumatologia delluniversit cattolica sono stati sottoposti entro 3 mesi dalla diagnosi a valutazione mediante rm cervicale . 
tutti i pazienti , ( 16 donne e 4 uomini ; range di et , 3175 anni ; et media , 55 anni ) rispettavano i criteri dellamerican college of rheumatology ( acr ) per la diagnosi di ar e lesordio dei sintomi era inferiore ad un anno [ 16 , 17 ]  . 
all patients at the time of diagnosis for the first 3 months had begun treatment with 1520 mg of methotrexate weekly and low doses of methylprednisolone ( 5 mg daily )  . laboratory tests the esr ( expressed in mm / h ) was measured with the westergren method and c - reactive protein ( crp ) ( expressed in mg / l ) with nephelometry . 
in addition , immunoglobulin ( ig ) a and igm rheumatoid factor ( rf ) and anti - citrulline antibodies ( anti - ccp ) were evaluated with enzyme - linked immunosorbent assay ( elisa ) in all patients . 
following the indications of the manufacturers , for rf ( orgentec diagnostika gmbh , mainz , germany ) , a value > 20 u / ml was considered positive , whereas for anti - ccp ( diastat axis - shield diagnostic , dundee , great britain ) , a value > 5 was considered positive . all patients within 3 months of diagnosis underwent mr imaging of the cervical spine with a 1.5 - t superconductive magnet ( signa , ge medical system , milwaukee , wi , usa ) and phased - array coil . 
mr examinations were targeted at the medial and lateral atlantoaxial joint , and the following sequences were used : sagittal t1 - weighted fast spin echo ( fse ) sequences ; axial and sagittal t2 - weighted fse sequences ; contrast - enhanced sagittal , axial and coronal t1weighted fse sequences ; t1 - weighted fast spoiled gradient echo ( fspgr ) sequences with fat saturation or axial , sagittal and coronal t1 - weighted turbo spin - echo sequences with fat saturation . 
all mr images were analysed in a blinded fashion by two musculoskeletal radiologists who assessed the images for changes in the arthritic joint and disease activity through evaluation of the extent of synovitis and structural erosive changes . 
in addition , the analysis considered the presence of the rheumatoid pannus ( isohypointense on the t1 - weighted images , hyperintense on the t2 - weighted images and with marked enhancement after contrast material administration ) , obliteration of the subarachnoid space , compression of the spinal cord and areas of myelomalacia . 
al momento della prima visita nessun paziente riferiva dolore a livello della colonna cervicale e sintomi o segni di interessamento della cerniera cervicale . durante la visita nessun paziente presentava allesame obiettivo neurologico deficit di forza e / o sensibilit . 
sono stati inoltre raccolti i dati clinici e demografici dei pazienti , eventuale abitudine al fumo , familiarit per malattie reumatiche e / o cardiovascolari , comorbilit , coinvolgimento extra - articolare , parametri ematochimici . 
tutti i pazienti allesordio presentavano una malattia attiva , definita con un das > 3 , 7 e la durata media di malattia di 6 , 73 , 0 mesi . al momento della diagnosi i pazienti sono stati sottoposti a radiografia convenzionale delle mani e dei polsi . 
le radiografie sono state valutate da due radiologi indipendenti che hanno analizzato le immagini in cieco . tutti i pazienti al momento della diagnosi per i primi 3 mesi hanno iniziato terapia con metotressato 1520 mg a settimana e basse dosi di metilprednisolone 5 mg / die . esami laboratoristici sono stati valutati i livelli della ves , con un metodo derivato westergren della pcr , mediante metodo nefelometrico . 
sono stati inoltre valutati in tutti i pazienti i livelli del fattore reumatoide ( fr ) iga ed igm e degli anticorpi anti - citrullina ( anticcp ) , mediante meto ( elisa )  . dica enzyme - linked seguendo le indicazioni delle case produttrici , per il fr ( orgentec diagnostika gmbh , mainz , germania ) , stato considerato positivo il valore > 20 u / ml , mentre per gli anticcp ( diastat axis - shield diagnostic , dundee , inghilterra ) valori > 5 . immunosorbent assay tutti i pazienti sono stati sottoposti , entro 3 mesi dalla diagnosi , ad esame rm del rachide cervicale . 
categorical and quantitative variables were described respectively by numbers , percentages and meanstandard deviation ( sd ) , or by the median and range of the 25th and 75th percentile according to data distribution . 
values of p < 0.05 were considered statistically significant . results data gathered on the 20 patients revealed that five ( 25% ) had da 2 radiologi muscolo - scheletrici che hanno analizzato le immagini in cieco , ricercando le modificazioni dellarticolazione artritica e contestualmente lattivit di malattia , attraverso la valutazione dellintensit della sinovite ed il danno strutturale erosivo . 
 stata , inoltre , ricercata la presenza del panno reumatoide ( iso - ipointenso nelle immagini t1 - pesate , iperintenso nelle t2 - pesate e con marcato enhancement post - contrasto ) , leventuale obliterazione dello spazio subaracnoideo , la compressione del midollo spinale , le aree di mielomalacia . 
1 allesame rm sono risultati positivi per coinvolgimento del rachide cervicale 5 pazienti ( 25% ) sul totale di 20 pazienti esaminati ; tutti i pazienti positivi presentavano sinovite attiva nellarticolazione atlo - epistrofea . analisi statistica i dati sono stati analizzati con spss 15.0 ( spss , chicago , il , usa )  . 
le variabili categoriche e quantitative sono state rispettivamente descritte come numeri , percentuali e mediadeviazione standard ( ds ) , o come mediana e range del 25 e 75 percentile , secondo la distribuzione dei dati . 
a limmagine rm assiale e b coronale fse t1 - pesate post - contrasto e con soppressione del segnale adiposo mostrano impregnazione dei tessuti molli della regione peri - odontoidea , prevalentemente del recesso di sinistra , da sinovite infiammatoria ( cerchio in a e b ) ( osteitis )  . 
overall , rf was positive in 12 patients ( 66% ) and anti - ccp in 15 ( 83% ) , whereas at least one sign of erosive changes in the hands and feet was found in ten patients ( 50% ) at radiography ( table 2 )  . discussion involvement of the cervical spine is found in more than 50% of patients with ra [ 3 , 2022 ] and it is not always correlated with specific symptoms and even less so with neurological symptoms . 
globalmente , il fr risultato positivo in 12 pazienti ( 66% ) , gli anti - ccp in 15 pazienti ( 83% ) , mentre almeno una lesione erosiva articolare , a livello di mani e piedi , stata riscontrata in 10 pazienti ( 50% ) allesame radiografico ( tabella 2 )  . discussione il coinvolgimento del rachide cervicale si riscontra in pi del 50% dei pazienti con ar [ 3 , 2022 ] e non sempre correlato a sintomi specifici e ancor meno a sintomi neurologici , fatto questo che rende ancor pi subdola linsorgenza di sublussazioni che possono necessitare poi di trattamenti chirurgici . 
larticolazione atlo - assiale la sede di coinvolgimento pi comune e precoce [ 20 ] ; nella fase iniziale della malattia , una sublussazione atlo - assiale anteriore stata riscontrata nel 10% dei casi [ 23 ]  . 
lelevata sensibilit della rm nel documentare il coinvolgimento rachideo gi stata dimostrata [ 3 ] anche se , per mantenere alta questa sensibilit , i radiol med ( 2010 ) 115 : 11111120 1118 fig . 
4a - c a 67 - year - old woman with early rheumatoid arthritis and cervical paa t2 - weighted fse magnetic resonance ( mr ) image show no changes in the atlantoaxial joint . 
in the initial phase of the disease , an anterior atlantoaxial subluxation is found in 10% of cases [ 23 ]  . the high sensitivity of mr imaging in documenting spinal involvement has already been shown [ 3 ] , even though to maintain this high sensitivity , mr findings must be integrated with patient history and clinical data . 
mr and power doppler have been shown to be highly sensitive and accurate in imaging the peripheral joints for identifying active synovitis at disease onset and during treatment [ 24 ]  . 
our study assessed 20 patients with a diagnosis of early rheumatoid arthritis ( mean disease duration < 12 months ) and demonstrated early involvement of the atlantoaxial joint in 25% of patients , with more aggressive disease characteristics , such as higher das and inflammatory indices . 
la rm insieme con leco - power doppler sono risultate metodiche molto sensibili ed accurate , in corrispondenza delle articolazioni periferiche , per lidentificazione della sinovite attiva allesordio della malattia e durante il trattamento [ 24 ]  . 
il nostro studio ha valutato 20 pazienti con diagnosi di early artrite reumatoide ( durata media di malattia inferiore a 12 mesi ) e ha permesso di mostrare un precoce interessamento dellarticolazione atlo - epistrofea nel 25% dei pazienti , con caratteristiche di malattia pi aggressive , quali das e indici di flogosi pi elevati . 
our findings , based on a population of patients with disease duration < 12 months , are in agreement with those of other studies [ 20 , 23 ] , which show involvement of the atlantoaxial joint in patients with a longer disease duration correlated with disease activity and the presence of erosive arthritis of the peripheral joints . 
despite the limited number of patients enrolled in this study , the presence of active disease with high inflammatory indices and erosive changes in the peripheral joints at conventional radiology since onset appears to identify the group of patients at risk of developing a compromised atlantoaxial joint . 
mr imaging , therefore , is useful in identifying early involvement of the atlantoaxial joint , and its use is desirable in patients with active disease at onset , even in the absence of the characteristic symptoms of cervical involvement . 
the presence of cervical involvement demonstrated by mr imaging could guide patient management towards more aggressive treatment malattia inferiore a 12 mesi sono in accordo con quelli di altri studi [ 20 , 23 ] che hanno dimostrato un coinvolgimento dellarticolazione atlo - assiale in pazienti con una pi lunga durata di malattia correlato allattivit di malattia e alla presenza di artrite erosiva a carico delle articolazioni periferiche . 
nonostante il limitato numero di pazienti arruolati in questo studio , la presenza di una malattia attiva con elevati indici di flogosi e con erosioni a livello delle articolazioni periferiche alla radiologia tradizionale , fin dallesordio , appare individuare il gruppo di pazienti a rischio di sviluppare una compromissione dellarticolazione atlo - assiale . 
la rm , quindi , utile nellindividuare un precoce coinvolgimento dellarticolazione atlo - assiale e il suo utilizzo auspicabile nei pazienti con una malattia attiva allesordio anche in assenza di una sintomatologia caratteristica di un interessamento cervicale . 
la presenza di un eventuale interessamento cervicale dimostrato dalla rm potrebbe guidare la scelta della terapia verso un trattamento pi aggressivo per 1120 radiol med ( 2010 ) 115 : 11111120 in order to achieve complete disease control both in peripheral joints and in the spine . 
further studies with a larger number of patients and with imaging follow - up will better define the importance of cervical involvement in the treatment programme . raggiungere un completo controllo della malattia a livello periferico e assiale . 
ospedali galliera , mura delle cappuccine 14 , 16128 genova , italy 2department of medical imaging , chu de montpellier , avenue augustin fliche 80 , 34295 montpellier , france 3centre rgional de lutte contre le cancer val daurelle , rue des apothicaires 208 , 34298 montpellier , france correspondence to : l . 
this study compared superparamagnetic ironoxide - enhanced magnetic resonance imaging ( spio - mri ) and combined fluorodeoxyglucose positron emission tomography and computed tomography ( fdg - pet / ct ) in evaluating liver metastases from colorectal adenocarcinoma following chemotherapy . 
scopo del presente lavoro stato confrontare la superparamagnetic iron oxid - risonanza magnetica ( spiorm ) e la tomografia computerizzata associata a tomografia a emissione di positroni con fluorodesossiglucosio ( tc - pet - fdg ) nella valutazione delle metastasi epatiche di adenocarcinoma colorettale dopo chemioterapia . 
considerando tutti i pazienti : analisi per lesione sensibilit del 92% per spio - rm e del 52% per tc - pet ( p < 0 , 001 ) , analisi per segmento epatico sensibilit del 99% e del 79% ( p < 0 , 001 ) rispettivamente . nei pazienti operati : analisi per lesione sensibilit del 85% per spio - rm e del 58% per tc - pet ( p < 0 , 05 ) , analisi per segmento epatico sensibilit del 97% e del 63% ( p < 0 , 05 ) rispettivamente . 
nei pazienti non operati in follow - up : analisi per lesione sensibilit del 97% per spio - rm e del 47% per tc - pet ( p < 0 , 001 ) , analisi per segmento epatico sensibilit del 100% e del 63% ( p < 0 , 007 ) rispettivamente . 
the worldwide variability of outcome is proportional to access to specialists and availability of modern drug therapy ; the overall 5 - year survival rate in the usa exceeds 60% but is < 40% in less developed countries [ 1 ]  . the liver is the most common site of distant metastases in colorectal cancer [ 2 ]  . 
a prospective study carried out from 1980 to 1990 on 484 consecutive patients with untreated liver lesions reported an average survival rate of 31% at 1 year , 7.9% at 2 years , 2.6% at 3 years and 0.9% at 4 years [ 3 ]  . 
resection of liver metastases has shown its ability to improve patient survival : according to some authors , a survival rate up to 43% at 5 years can be obtained [ 4 ]  . 
the eligibility criteria for liver surgery are debated because of the difficulty in identifying precise prognostic factors for the long - term outcome of hepatic resection ; furthermore , patients may become eligible surgery after chemotherapy [ 5 ]  . 
 for today , assessment of liver metastases relies mainly on ultrasound ( us ) , computed tomography ( ct ) , magnetic resonance imaging ( mri ) and combined fluorodeoxyglucose positron emission tomography and computed tomography ( fdg - pet / ct ) , with reported sensitivities of 55% , 72% , 76% and 90% , respectively [ 6 ]  . 
 us may integrate ct in the assessment of liver lesions . ct in the portal phase has been reported as a good test for detecting hepatic metastases and represents probably the most commonly used modality [ 7 ]  . 
mri has been shown by some authors to be equal in sensitivity and specificity to ct in detecting focal liver lesions , but in recent papers , a higher sensitivity was reported for both unenhanced mri and superparamagnetic iron - oxide - enhanced mri ( spio - mri ) secondo lorganizzazione mondiale della sanit ogni anno si verificano 945000 nuovi casi di carcinoma colorettale , con 492000 morti [ 1 ]  . 
oggi il carcinoma del colon - retto , nel mondo , il terzo tumore per frequenza e la quarta pi frequente causa di morte per neoplasia [ 1 ]  . 
la variabilit della prognosi di tale patologia proporzionale alla possibilit di accesso a specialisti dedicati e a terapie farmacologiche moderne ; la sopravvivenza a 5 anni negli usa supera il 60% , ma non arriva al 40% nei paesi meno sviluppati [ 1 ]  . il fegato la sede pi frequente di metastasi a distanza da carcinoma colorettale [ 2 ]  . 
uno studio prospettico realizzato fra il 1980 ed il 1990 su 484 pazienti consecutivi con metastasi epatiche non trattate osserv una sopravvivenza media del 31% ad un anno , del 7 , 9% a due anni , del 2 , 6% a tre anni e dello 0 , 9% a quattro anni [ 3 ]  . 
la resezione delle metastasi epatiche ha dimostrato di poter migliorare la sopravvivenza di questi pazienti : alcuni autori riportano una sopravvivenza fino al 43% a 5 anni [ 4 ]  . 
i criteri di elezione per la chirurgia resettiva epatica sono non ben definiti a causa della difficolt nellidentificare sicuri fattori prognostici ; in alcuni casi inoltre le metastasi possono divenire resecabili solo dopo chemioterapia [ 5 ]  . 
 oggi la valutazione delle secondariet epatiche si basa prevalentemente su ecografia , tomografia computerizzata ( tc ) , risonanza magnetica ( rm ) e tomografia computerizzata associata a tomografia a emissione di positroni con fluorodesossiglucosio ( tc - pet - fdg ) ; nella loro metanalisi kinkel et al . 
i risultati riportati in letteratura sono per variabili e , come kinkel ed i suoi colleghi sottolineano , mancano studi che confrontino le diverse tecniche di imaging nello stesso gruppo di pazienti [ 6 ]  . 
la tc al tempo portale considerata un buon esame per lidentificazione di metastasi epatiche e rappresenta probabilmente la metodica pi utilizzata [ 7 ]  . la rm , secondo alcuni autori , presenta sensibilit e specificit sovrapponibili alla tc nella detezione di lesioni radiol med ( 2010 ) 115 : 10871100 1089 [ 810 ]  . 
fdg - pet has been reported as an important adjunctive modality for staging colorectal malignancies and planning treatment [ 12 ]  . different authors and two different meta - analyses report high sensitivity in assessing liver metastases from colorectal cancer for fdg - pet / ct [ 6 , 12 , 13 ]  . 
however , the value of fdg - pet / ct appears overestimated for precise lesion depiction , particularly versus mangafodipir - enhanced mri , as shown by sahani e al . 
 we retrospectively reviewed the imaging findings , surgical reports , pathology reports and / or follow - up data in patients with colorectal malignancy who underwent both spio - mri and whole - body fdg - pet / ct to compare these two modalities in assessing liver metastatic disease following chemotherapy . 
 materials and methods a search was undertaken within the picture archiving and communication system ( pacs ) of our department to retrieve data on patients with liver metastases from colorectal adenocarcinoma who underwent spio - mri and fdg - pet / ct following chemotherapy to evaluate eligibility for resection of liver metastases . 
approval of our ethics committee was not required for this retrospective study of the clinical workup of liver metastases . patients assessing from march 2005 to february 2006 , 19 patients with liver metastases from colorectal carcinoma ( eight women and 11 men ; 17 colonic and two rectal adenocarcinomas ) were included in this study comparing spio - mr and fcgpet / ct following chemotherapy . 
all patients received chemotherapy prior to imaging evaluation of elibigility for reseaction of liver metastases : six patients received 5 - fluorouracil ( 5 - fu ) + irinotecan , six received 5 - fu + oxaliplatin and seven received 5 - fu + irinotecan + oxaliplatin . liver metastases imaging techniques mri technique mri of the liver was performed on a 1.5 - t system ( intera , philips medical systems , best , the netherlands )  . 
unenhanced t1 - weighted images were obtained using a breathepatiche , ma in lavori recenti una sensibilit pi alta stata evidenziata dalla rm prima e dopo somministrazione di superparamagnetic iron oxide ( spio ) [ 810 ]  . 
 [ 11 ] i risultati della rm dopo somministrazione di mangafodipir nellidentificazione di metastasi epatiche sono simili a quelli ottenuti dalla rm dopo somministrazione di spio ( spio - rm ) [ 11 ]  . 
il valore della pet - fdg appare per sopravvalutato riguardo allesatta identificazione della lesione , in particolare rispetto alla rm dopo somministrazione di mangafodipir come evidenziato da sahani et al . 
 in questo contesto abbiamo rivalutato retrospettivamente i risultati delle metodiche di imaging , i referti chirurgici , i referti di anatomia patologica e / o il follow - up di pazienti con neoplasie colorettali che erano stati sottoposti a spiorm e a tc - pet - fdg per confrontare i risultati di queste due modalit nella valutazione di metastasi epatiche dopo chemioterapia . 
 materiali e metodi abbiamo cercato nel nostro picture archiving and communication system ( pacs ) i pazienti con metastasi epatiche da carcinoma colorettale che erano stati sottoposti a spio - rm e a tc - pet - fdg dopo chemioterapia per valutare se era possibile sottoporli a chirurgia epatica resettiva . 
non stata necessaria lapprovazione del nostro comitato etico per svolgere questo studio retrospettivo sullattivit clinica svolta nella valutazione dei pazienti con metastasi epatiche . pazienti nel periodo di tempo compreso fra marzo 2005 e febbraio 2006 19 pazienti con metastasi epatiche da carcinoma colorettale ( 8 donne e 11 uomini ; 17 adenocarcinomi del colon e 2 del retto ) sono stati valutati ed inclusi in questo studio che confronta la spio - rm e la tc - pet - fdg nella valutazione di metastasi epatiche dopo chemioterapia . 
t2 - weighted respiratorycompensated axial sequences included t2 - weighted singleshot fast spin - echo ( t2 - ssfse ) [ tr / te 658 / 80 ; slice thickness 6 mm ; interslice gap 1 mm ; acquisition matrix 352265 ; turbo spin - echo ( tse ) factor 72 ] and t2weighted spectral presaturation with inversion recovery ( t2 spir ) ( tr / te 1 , 800 / 70 ; slice thickness 6 mm ; interslice gap 1 mm ; acquisition matrix 272211 ; echo train length 22 )  . 
the ct parameters were 130 mas , 130 kv , 5 - mm slice width and 8 - mm table feed per rotation . the pet component of the combined imaging system offers an in - plane spatial resolution of 4.6 mm ( matrix 128128 )  . ct data were used for pet attenuation correction . 
the patients were advised to fast for at least 6 h before the study , and capillary blood glucose levels were checked before injection ( no fdg - pet / ct was performed if the blood glucose was > 160 mg / dl )  . 
they were then positioned supine in the scanner , and one helical ct acquisition was performed ( without iodinated contrast medium injection ) , followed by the acquisition of pet images ( 34 min per bed position ) in six to seven bed positions from cranial vault to mid thigh level . 
 image analysis one senior radiologist in abdominal imaging and one senior nuclear medicine physician independently interpreted all tecniche di imaging tecnica rm gli esami rm del fegato sono stati realizzati con unapparecchiatura di 1 , 5 t ( intera , philips medical systems , best , olanda )  . 
sono state eseguite sequenze t1 pesate senza mezzo di contrasto in apnea 2d assiali gradient echo in fase e fuori fase ( tempo di ripetizione [ tr ] / primo - eco tempo di eco [ te ] , secondo eco te : 180 / 2 , 3 , 4 , 6 ; spessore di strato : 6 mm ; intervallo : 1 mm ; matrice : 240168 ; flip angle : 80 )  . le sequenze t2 pesate assiali con gating respiratorio includevano : t2 single - shot fast spin - echo ( ssfse ) ( tr / te : 658 / 80 ; spessore di strato : 6 mm ; intervallo : 1 mm ; matrice : 352265 ; turbo - spin echo [ tse ] factor : 72 ) e t2 spectral presaturation inversion recovery ( spir ) ( tr / te : 1800 / 70 ; spessore di strato : 6 mm ; intervallo : 1 mm ; matrice : 272211 ; echo train length : 22 )  . 
dopo 30120 minuti dalla fine dellinfusione endovena ( ev ) lenta ( in circa 20 minuti ) di spio ( endorem 0 , 5 mol / kg , guerbet , villepinte , francia ) sono state eseguite sequenze t2 pesate gradient echo ( gre ) in apnea assiali e coronali ( tr : 100 ; te : 9 , 2 assiale , 8 , 6 coronale ; spessore di strato : 6 mm ; intervallo : 1 mm ; matrice , 208166 ; flip angle : 15 )  . tecnica tc - pet - fdg le tc - pet - fdg sono state realizzate con unapparecchiatura tc - pet ( biograph emotion duo , siemens medical solutions , erlangen , germania )  . 
i pazienti dovevano mantenere il digiuno per almeno 6 ore prima dellesame , la glicemia capillare veniva controllata prima dellesame ( lesame tc - pet - fdg non veniva eseguito se la glicemia risultava superiore a 160 mg / dl )  . 
dopo unora i pazienti venivano posizionati supini allinterno dellapparecchiatura e veniva prima eseguita la tc ( senza mezzo di contrasto iodato ) , poi veniva acquisita la pet ( 34 minuti per posizione del lettino ) in 67 posizioni del lettino dalla volta cranica fino al terzo medio delle cosce . 
 ecografia intraoperatoria le ecografie intraoperatorie ( ious ) sono state eseguite da un radiologo esperto con sonda lineare di 7 , 5 mhz sterilizzata ed applicata direttamente sulla superficie epatica ( b&k medical , marlborough , ma , usa )  . 
both readers were blinded to all patient data and were aware only of the main inclusion criteria : assessement of liver metastases from colorectal adenocarcinoma . presence , location , dimension and number of metastatic lesions were evaluated and recorded on a diagram of the liver . 
spio - mr images were reviewed and analysed on a pacs workstation equipped with 1 , 2801 , 024 - pixel flat - screen monitors . fdg - pet / ct images were displayed in the axial , coronal and sagittal planes on a workstation , and unenhanced ct images were used to aid in lesion localisation . 
consensus were considered sessions with another radiologist were performed in the event of discordance between spio - mri and fdg - pet / ct in lesion localisation . standards of reference in 11 patients , the standards of reference were surgical exploration , ious and pathology results . 
time delay in days between spio - mri or fdg - pet / ct ( considering the most recent ) and surgery was 71.552.9 , 15168 ( meansd , range )  . 
ct was performed with a 64 - detector multislice ct ( aquilion 64 , toshiba medical systems corporation , tokyo , japan )  . the ct protocol included three helical acquisitions ( tube voltage 120 kv , tube current 300 ma , rotation time 0.4 s , collimation 640.5 mm , 3 - mm reconstruction ) after injection of 2 ml / kg of iodinated contrast medium ( iomeron 350 , bracco , milan , italy ) at 3ml / s : the first of the thorax in the arterial phase , the second of the abdomen in the portal phase and the third of the liver in the late phase ( 3to 5 - min delay )  . 
time delay in days between spio - mri or fdgpet / ct ( considering the most recent ) and follow - up was 400.5239.1 , 55728 ( meansd , range )  . 
when possible , the longer follow - up was considered for patients without progression and the follow - up with the most unfavourable evolution for patients with progression of liver metastases . 
to differentiate between the appearance of a lesion that was not present at the previous examination ( true negative ) and the progression of a lesion that was retrospectively already present at the previous examination ( false negative ) , a consensus analisi delle immagini un radiologo esperto ed un medico nucleare hanno valutato indipendentemente tutte le spio - rm e le tc - pet - fdg rispettivamente , entrambi non erano a conoscenza della storia clinica del paziente e conoscevano solo il criterio di inclusione nello studio : valutazione di metastasi epatiche di carcinomi colorettali . 
presenza , dimensioni , numero e sede delle metastasi venivano riportate su uno schema del fegato . la dimensione delle lesioni stata misurata in rm nelle sequenze t2 ssfse o t2 gre , utilizzando il diametro maggiore di una delle due sequenze . 
la dimensione delle lesioni in tc - pet - fdg stata stimata in 3 taglie ( 010 mm , 1030 mm , > 30 mm ) , ma non utilizzata per lanalisi delle dimensioni . 
le immagini della tc - pet - fdg sono state visualizzate nei tre piani ortogonali su una workstation , le immagini tc sono state utilizzate come aiuto nella localizzazione delle lesioni . 
nei casi di discordanza sulla localizzazione della stessa lesione fra la spio - rm e la tc - pet - fdg una rilettura congiunta con un terzo radiologo veniva svolta . standard di riferimento in 11 pazienti gli standard di riferimento sono stati : lesplorazione chirurgica , lious ed i risultati anatomo patologici . 
il tempo ( in giorni ) trascorso fra la spio - rm o la tcpet - fdg ( considerando la pi recente ) e la chirurgia risultato : 71 , 552 , 9 , 15168 ( mediads , range )  . 
il protocollo tc includeva 3 acquisizioni elicoidali ( 120 kv , 300 ma , tempo di rotazione 0 , 4 secondi , collimazione 640 , 5 mm , ricostruzioni a 3 mm ) dopo iniezione ev 2 ml / kg di mezzo di contrasto iodato ( iomeron 350 , bracco , milano , italia ) a 3 ml / s : la prima sul torace al tempo arterioso , la seconda sulladdome al tempo portale e la terza sul fegato al tempo tardivo ( 35 minuti di ritardo )  . 
quando possibile veniva scelto il follow - up pi lungo per i pazienti senza progressione ed il follow - up con levoluzione peggiore per i pazienti con progressione delle metastasi epatiche . 
per distinguere fra la comparsa di una lesione che non era presente allesame precedente ( vero negativo ) e la progressione di una 1092 radiol med ( 2010 ) 115 : 10871100 session of the three readers with review of the previous examination was obtained . 
a lesion was considered true positive if it had increased > 25% in size at follow - up or if it had been proved to be malignant on previous examinations . false positive lesions were defined in accordance with all imaging examinations of the patient . the gold standard for lesion localisation was ious when available . 
in patients who did not undergo surgery , the third reader compared all studies with the follow - up , and in the event of location mismatch , the location was defined by consensus between the three readers . 
nei casi non sottoposti a chirurgia il terzo lettore ha confrontato tutti gli esami disponibili con il follow - up ed in caso di discordanza la localizzazione era definita dallaccordo fra i tre lettori . 
specificity can , in fact , be calculated only per segment , as no true negative lesions may be defined in our study that evaluates results of different modalities in depicting liver metastases . 
la specificit pu essere in effetti solo definita per segmento dato che non possibile definire lesioni vere negative nel nostro lavoro che confronta due diverse modalit nellidentificazione delle metastasi epatiche . 
lanalisi per segmento stata realizzata utilizzando la classica classificazione in 8 segmenti di couinaud . i risultati delle due metodiche sono stati confrontati con il t test di student ed il test di mcnemar . 
lesion dimensions in millimetres were 16.19.23 , 555 ( meansd , range ) ; in one patient who underwent right hepatectomy with segment ivb resection , 26 lesions were found at pathology , and therefore , analysis of lesion dimensions was not possible . 
fdg - pet / ct detected 71 lesions ( true positive ) and missed 65 ( false negative )  . lesion relocalisation was necessary in one patient for spio - mri , in three patients for fdg - pet / ct and in six patients for both modalities , according to the surgical findings . 
the percentage of lesions that needed to be relocalised were significantly ( p < 0.001 , mc nemar ) more for fdgpet / ct ( 18 / 71 ) than for spio - mri ( 14 / 125 )  . as our study population was heterogeneous with regard to the standards of reference ( surgical exploration and ious or follow - up ) , we performed three different kinds of analysis : one considered the entire study population , one the 11 patients who underwent surgery and ious and one the eight patients who underwent follow - up . 
la dimensione delle lesioni ( in millimetri ) risultata di : 16 , 19 , 23 , 555 ( mediads , range ) ; in un paziente sottoposto ad epatectomia destra con resezione del segmento ivb sono state individuate 26 lesioni alla valutazione anatomo patologica e quindi non stato possibile lanalisi delle loro dimensioni . 
la tcpet - fdg ha identificato 71 lesioni ( veri positivi ) e non evidenziato 65 lesioni ( falsi negativi )  . la rilocalizzazione di lesioni stata necessaria in : 1 paziente per la rm - spio , in 3 pazienti per la tc - pet - fdg ed in 6 pazienti per entrambe le modalit in accordo con i reperti chirurgici . 
it must be noted , however , that in three patients ( with two , ten and six lesions each ; 5 mm , 15.4 mm and 15 mm mean size , respectively ) , fdg - pet / ct did not identify the liver metastases . 
i nostri risultati dimostrano che la sensibilit ( per lesione e per segmento ) della spio - rm e della tcpet - fdg differiscono significativamente allinterno di tutti e tre i gruppi di pazienti ( intera popolazione di studio , pazienti operati e pazienti in follow - up )  . 
we divided the 110 lesions of known dimensions into three groups and calculated the sensitivity of fdg - pet / ct and of spio - mri . as expected , the sensitivity of fdg - pet / ct decreased as the size of the lesion decreased . 
la rm - spio presenta una sensibilit significativamente differente ( p < 0 , 001 , mcnemar ) rispetto alla tcpet - fdg per le lesioni comprese fra 15 e 30 mm e per le fig . 
1 sensibilit della superparamagneti oxid - risonanza magnetica ( spio - rm ) e della tomografia computerizzata associata a tomografia a emissione di positroni con fluorodesossiglucosio ( tc - pet - fdg ) per range di dimensioni delle metastasi . radiol med ( 2010 ) 115 : 10871100 1095 fig . 
piccola lesione metastatica del segmento iv non visibile alla tc - pet - fdg ( a ) ed individuata come una lesione iperintensa ( freccia bianca ) nella sequenza rm t2 * gre dopo somministrazione di spio ( b )  . 
il paziente venne trattato mediante epatectomia destra e radiofrequenza intraoperatoria della lesione al segmento iv ; la tc post - operatoria al tempo portale ( c ) dimostra unarea ipodensa ( freccia bianca ) come esito del trattamento con radiofrequenza . 1096 radiol med ( 2010 ) 115 : 10871100 extrahepatic findings were identified by fdg - pet / ct in six patients : in one case , an elastofibroma dorsi was depicted ; four patients had lung metastases ( well appreciated also on the ct scan of the fdg - pet / ct ) ; and in one patient , fdg - pet / ct was false positive for peritoneal carcinomatosis . discussion liver metastases assessing patients with colorectal following chemotherapy to determine surgical eligibility requires an integrated evaluation of clinical data and imaging findings . 
portal - phase contrast - enhanced ct represents the most commonly used modality , but us , mri ( with different types of contrast media ) , fdg - pet and fdg - pet / ct have also shown good results [ 6 , 7 , 10 , 1417 ]  . 
in recent years , the improved performance of ct and mri has reduced discordances with ious , which remains the imaging standard of reference for liver metastases from colorectal adenocarcinoma [ 18 ]  . our study addressed assessing liver metastases from colorectal adenocarcinoma with spio - mri and fdgpet / ct in a relatively small series of 19 patients with 136 metastases . 
mean lesion dimension ( 16.1 mm ) in our study appears to be comparable with that reported in other studies [ 14 , 19 , 20 ]  . mean age of our study population ( 60.5 years ) is in line with other studies reported in the literature [ 13 , 14 , 19 , 20 ]  . spio - mri and fdg - pet / ct examination techniques are in agreement with the current standards and literature [ 14 , 21 ]  . 
some authors reported the technical feasibility of iodinated contrast - enhanced fdgpet / ct , and this point deserves to be validated in the future and could possibly improve the results of fdgpet / ct [ 2224 ]  . 
in follow - up , 64 - slice ct in the portal and late phases was considered sufficient , in line with the current literature , even though the relevance of the latephase interest may be debated [ 7 , 25 ]  . 
ious was lesioni < 15 mm , invece nessuna differenza significativa in sensibilit fra le due metodiche stata osservata per le lesioni 30 mm , i dettagli sono riassunti nelle figure 13 . in 6 pazienti la tc - pet - fdg ha individuato dei reperti extraepatici : in 1 caso un elastofibroma del dorso , in 4 pazienti metastasi polmonari ( ben visibili alla tc della tcpet - fdg ) ed in un paziente la tc - pet - fdg risultata falsamente positiva per carcinosi peritoneale . discussione la valutazione dei pazienti con metastasi epatiche da adenocarcinoma del colon - retto dopo chemioterapia per definire lindicazione chirurgica richiede una valutazione integrata dei dati clinici e dei risultati dellimaging . 
 diverse modalit di imaging sono state proposte per la valutazione dei pazienti , la tc dopo iniezione ev di mezzo di contrasto iodato al tempo portale rappresenta la modalit pi usata ma lecografia , la rm ( con diversi tipi di mezzo di contrasto ) , la pet - fdg e la tc - pet - fdg hanno dimostrato buoni risultati [ 6 , 7 , 10 , 1417 ]  . 
possiamo notare che negli ultimi anni i miglioramenti ottenuti dalla tc e dalla rm hanno permesso di ridurre le discordanze con la ious , che rimane lo standard di riferimento per le metastasi epatiche da adenocarcinoma colorettale [ 18 ]  . questo lavoro valuta , in un gruppo di pazienti relativamente piccolo , i risultati della rm - spio e della tc - petfdg nella detezione delle metastasi epatiche da adenocarcinoma colorettale . 
la nostra popolazione di studio include 19 pazienti con 136 metastasi , il numero medio di metastasi per paziente 7 e risulta superiore rispetto a lavori simili : sahani et al . 
let media dei pazienti ( 60 , 5 anni ) appare anchessa sovrapponibile ad altri lavori [ 13 , 14 , 19 , 20 ]  . le tecniche di esame della rm - spio e della tc - petfdg appaiono in accordo con gli standard e con la letteratura [ 14 , 21 ]  . 
la tc - pet - fdg stata eseguita senza iniezione ev di mezzo di contrasto iodato come da nostro protocollo standard , alcuni autori hanno riportato la fattibilit tecnica della tc - pet - fdg con mezzo di contrasto iodato ed in futuro questo punto merita di essere rivalutato e dovrebbe migliorare i risultati della tc - petfdg [ 2224 ]  . 
nel follow - up la tc con apparecchiatura a 64 detettori al tempo portale e tardivo stata considerata radiol med ( 2010 ) 115 : 10871100 1097 performed according to current standards , with no us contrast medium being used , even though recent reports have shown a higher sensitivity compared with standard ious [ 18 , 26 ]  . in ten patients , lesion relocalisation was necessary before analysing the results . 
there was a significant difference in the number of lesions requiring relocalisation between spio - mri and fdg - pet / ct , a finding accounted for by the lower spatial resolution of pet and the absence of good anatomical liver landmarks on the unenhanced ct scan of the fdg - pet / ct study [ 14 ]  . 
a significant difference in sensitivity per lesion and per segment was found between spio - mri and fdg - pet / ct in the entire study population , as reported by rappeport et al . 
these results allowed us to be more confident in comparing the results of spio - mri and fdg - pet / ct in our study population , which had two different standards of reference ( surgery and follow - up )  . sensitivity of spio - mri per lesion was comparable with that reported in the literature , which ranges from 77% to 97% [ 11 , 19 , 20 , 23 , 27 ]  . 
instead , the sensitivity of fdg - pet / ct in our study appears lower than that reported by other reports and reviews ( 65%100% ) , but again , similar to the recent paper by rappeport et al . , in which it was 54% [ 23 ]  . 
in our work , the lesion detection capabilities of fdg - pet / ct appear to be inadequate for defining the surgical strategy , as was also reported by other authors [ 28 ]  . sensitivity per patient was not within the goals of our study , although it must be noted that in 3 / 19 patients , fdgpet / ct did not identify any liver lesion , whereas spiomri depicted lesions in all patients . 
this result is in contrast with the higher per - patient sensitivity of fdg - pet / ct for colorectal liver metastases reported in the meta - analysis of bipat et al . 
 sensitivity per segment appears to be an interesting result of our work , which further confirms the good performance of spio - mri in assessing affected segments with high sensitivity ( 99% ) , therefore allowing surgical planning . 
the sensitivity per segment of fdg - pet / ct ( 79% ) is higher than the sensitivity per lesion of fdg - pet / ct ( 52% ) but still significantly lower than the sensitivity per segment of spio - mri . specificity per segment was high for both modalities ( 95% for spio - mri and 98% for fdg - pet / ct ) and did not vary significantly between the two techniques . 
this could be well expected for fdg - pet / ct because of the low sensitivity for lesion depiction , whereas for spio - mri , the good sufficiente , in accordo con la letteratura , anche se il valore del tempo tardivo pu essere discusso [ 7 , 25 ]  . 
lious stata eseguita in accordo con gli standard attuali , non stato utilizzato il mezzo di contrasto ecografico anche se lavori recenti hanno dimostrato che pu migliorare la sensibilit rispetto allious standard [ 18 , 26 ]  . in 10 pazienti stata necessaria una rilocalizzazione delle lesioni prima di analizzare i risultati ; si osservata una differenza significativa nel numero di lesioni che dovevano essere rilocalizzate fra la rm - spio e la tc - pet - fdg . 
la minore risoluzione spaziale della pet e lassenza di buoni reperi anatomici epatici della tc senza contrasto della tc - petfdg spiegano questo aspetto in accordo con la letteratura [ 14 ]  . 
considerando lintera popolazione di studio una differenza significativa di sensibilit per lesione e per segmento stata osservata fra la spio - rm e la tc - pet - fdg , in accordo con un lavoro simile di rappeport et al . 
questa valutazione ci rende pi tranquilli nel confrontare la spio - rm e la tc - pet - fdg nella nostra popolazione di studio che ha diversi standard di riferimento ( chirurgia e follow - up )  . la sensibilit della spio - rm per lesione sovrapponibile a quella riportata in letteratura che varia fra il 77% ed il 97% [ 11 , 19 , 20 , 23 , 27 ]  . 
invece la sensibilit per lesione della tc - petfdg nel nostro lavoro risulta inferiore a quella di altri lavori e revisioni ( 65%100% ) , ma simile al 54% ottenuto in un lavoro simile da rappeport et al . 
nel nostro studio la detezione delle lesioni con tc - pet - fdg appare inadeguata per la definizione di una strategia chirurgica , in accordo anche con altri autori [ 28 ]  . la sensibilit per paziente non era fra gli obiettivi del nostro lavoro , bisogna per sottolineare che in 3 / 19 pazienti la tc - pet - fdg non ha identificato lesioni mentre la spio - rm ha identificato lesioni in tutti i pazienti . 
questo risultato contrasta con la maggiore sensibilit per paziente della tc - pet - fdg riportata nella metanalisi di bipat per la detezione di metastasi epatiche colorettali [ 13 ]  . 
 la sensibilit per segmento appare un risultato interessante del nostro lavoro che ulteriormente conferma come la spio - rm ( con una sensibilit per segmento del 99% ) sia in grado di permettere unaccurata pianificazione chirurgica . la sensibilit per segmento della tc - pet - fdg ( 79% ) maggiore della sensibilit per lesione della tc - pet - fdg ( 52% ) ma sempre significativamente inferiore alla sensibilit per segmento della spio - rm . la specificit per segmento alta per entrambe le modalit ( 95% per la spio - rm e 98% per la tc - pet - fdg ) e non differisce significativamente ; alti valori sono riportati anche da altri autori [ 12 ]  . 
questo era prevedibile per la tc - pet - fdg a causa della bassa sensibilit nella detezione delle lesioni , invece per la spio - rm appare riferibile alla capacit di caratterizzazione tissutale . 1098 radiol med ( 2010 ) 115 : 10871100 result can be related to the tissue characterisation capabilities of spio - mri . as could be expected , false negative results of both techniques were more likely for small lesions , although sensitivity for small lesions of fdg - pet / ct ( 3370% ) was significantly lower than that of spio - mri ( 95100% )  . 
however , spatial resolution also appears to affect breath - hold gre 2d axial and coronal t2 * - weighted spio - mri imaging ( 6 - mm slice thickness with 1 - mm interslice gap ) , as the mean dimension of spio - mri false negative in this study was 8 mbetter results could be expected with 3d gre t1 - weighted mangafodipir - enhanced mri , but two investigations reported no significant difference between spio - mri and mangafodipir - enhanced mri in detecting liver metastases [ 11 , 29 ]  . 
in fact , all of our study population was treated with chemotherapy prior to imaging ( with at least a 3 - week delay between the last session and fdg - pet / ct ) , and cooling down of the lesion may therefore represent a nonnegligible effect , as reported also by akhurst et al . 
it must be noted that , to the best of our knowledge , no fixed interval is agreed upon between chemotherapy and fdg - pet / ct to avoid possible pet false negative results . 
as the value of pet in assessing the efficacy of chemotherapy ( metabolic response ) and as a prognostic factor has been well established for several malignancies ( lymphoma , non - small0cell lung cancer , oesophageal cancer ) , further evaluation for other forms of malignancy , such as colorectal cancer , appears necessary [ 31 ]  . 
a longer follow - up of our study population and more patients are needed to address these issues at our institution . the added value of fdg - pet has often been related to the identification of extrahepatic disease , but a lack of studies comparing fdg - pet and ct in this assessment may be noted . 
in our work , no significant extrahepatic secondary lesions were identified at fdg - pet / ct only . the pulmonary metastases observed in four patients were all well visible on the ct images of fdg - pet / ct . 
the elastofibroma dorsi , found in one patient , is a known hypermetabolic benign lesion at fdg - pet that has to be differentiated from metastases in the adjacent structures [ 33 , 34 ]  . 
gastrointestinal foci of fdg uptake may be physiological or related to underlying processes , benign or malignant ; in some cases , the differential diagnosis with peritoneal carcinomatosis may be difficult [ 35 ]  . come prevedibile , i falsi negativi di entrambe le metodiche sono pi frequenti per lesioni piccole , la sensibilit della tc - pet - fdg per le lesioni piccole ( 33%70% ) significativamente minore di quella della spio - rm ( 95%100% )  . 
la risoluzione spaziale rappresenta per anche un limite delle sequenze gre 2d in apnea assiali e coronali t2 * pesate ( spessore di strato 6 mm ed 1 mm di intervallo ) dato che la dimensione media dei falsi negativi della spio - rm in questo lavoro di 8 mrisultati migliori possono essere attesi con lutilizzo di sequenze 3d gre t1 pesate dopo iniezione di mangafodipir , ma due diversi lavori non evidenziano nessuna significativa differenza fra questultima e la spio - rm nella detezione delle metastasi epatiche [ 11 , 29 ]  . 
in effetti tutti i pazienti del nostro studio erano stati trattati con chemioterapia prima delle metodiche di imaging ( con un intervallo di almeno 3 settimane fra lultima sessione e la tc - pet - fdg ) e quindi un raffreddamento della lesione pu rappresentare un effetto non trascurabile , come riportato anche da akhurst et al . 
il valore della pet nello stabilire lefficacia della chemioterapia ( risposta metabolica ) e come fattore prognostico stata ben dimostrata per diverse neoplasie maligne ( linfoma , tumore polmonare non a piccole cellule , tumore dellesofago... ) , nel contesto del carcinoma colorettale ulteriori studi appaiono necessari [ 31 ]  . 
un follow - up pi lungo ed un maggior numero di pazienti sono necessari per affrontare questi aspetti presso il nostro centro . il valore aggiunto della pet - fdg stato spesso relazionato allidentificazione di lesioni extraepatiche ma si pu notare che mancano studi che confrontino la tc e la petfdg nella ricerca di tali lesioni . 
nel nostro lavoro non sono state individuate significative lesioni secondarie extraepatiche visibili con la sola tc - pet - fdg , le metastasi polmonari riscontrate in 4 pazienti erano tutte ben visibili con la tc della tc - pet - fdg . 
lelastofibroma del dorso , osservato in un paziente , una nota lesione benigna ipercaptante alla pet - fdg che deve essere differenziata da metastasi nelle strutture adiacenti [ 33 , 34 ]  . 
aree gastrointestinali di iperaccumulo di fdg possono essere fisiologiche o patologiche ; in alcuni casi la diagnosi differenziale con la carcinomatosi peritoneale pu essere difficile [ 35 ]  . cinque limiti principali possono essere identificati in questo lavoro ; in primo luogo la natura retrospettiva dello radiol med ( 2010 ) 115 : 10871100 1099 five main limitations of this study may be identified . first , its retrospective nature accounts for a relative inhomogeneity of imaging order and delay . 
second is the heterogeneous reference standards ( surgery and follow up ) , which may account for the better results obtained by spio - mri , even though considering the surgical group and follow - up group separately the results of spio - mri and fdgpet / ct are similar to those achieved in the entire study population . 
third is the follow - up criteria , as in some cases , it was difficult to assess whether a lesion was metastatic , though the consensus reading was able to solved these situations . 
fourth is the absence of a fourth independent reader to interpret spio - mri and fdg - pet - ct together to assess sensitivity and specificity of the two imaging modalities in combination ; however , given the results obtained in our study , no substantial improvement would be expected . finally , the small study population represented a limitation to robust data analysis . 
the effect of chemotherapy on fdg - pet / ct lesion depiction and the potential prognostic impact of fdg - pet / ct following chemotherapy in this setting appear to need further evaluation and a larger study population . studio correla con la disomogeneit dellordine di esecuzione delle metodiche di imaging e degli intervalli di tempo fra le stesse . 
il secondo problema rappresentato da standard di riferimento eterogenei ( chirurgia e follow - up ) che pu in parte spiegare i migliori risultati ottenuti dalla spio - rm , anche se considerando indipendentemente i pazienti sottoposti a chirurgia e quelli in follow - up i risultati della spio - rm e della tc - pet - fdg sono simili a quelli ottenuti nellintera popolazione di studio . 
il terzo problema dovuto ai criteri del follow - up , in alcuni casi stato difficile valutare se la lesione era metastatica ma una valutazione in consenso stata capace di risolvere tali situazioni . 
il quarto problema riguarda lassenza di un quarto lettore indipendente che dovrebbe aver interpretato insieme la spio - rm e la tc - pet - fdg per valutare la sensibilit e la specificit delle due indagini integrate , anche se dati i risultati del nostro lavoro non dovrebbe essere atteso un miglioramento . 
guglielmi2 , 3 1department of internal medicine metabolic bone disease unit , university of palermo , via del vespro 147 , 90143 palermo , italy 2department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 3department of radiology , scientific institute hospital casa sollievo della sofferenza , viale cappuccini 1 , 71013 san giovanni rotondo , foggia , italy correspondence to : g . 
vertebral fractures ( vfs ) are the hallmark of osteoporosis and are responsible for almost 70 , 000 hospital admissions yearly , implying social costs and impaired quality of life for patients . 
in recent years , several techniques , both qualitative and quantitative , have been proposed for vf diagnosis , but a gold standard is not yet available and the visual semiquantitative ( vsq ) assessment proposed by genant remains the most validated . 
in 283 postmenopausal women referred to our clinic for osteoporosis screening , we performed a clinical examination , plain spinal radiographs ( for vsq assessment ) and digital computerised morphometry ( dcm ) to assess vfs . 
forty - seven percent of patients had a t score < 2.5 standard deviations ( sd ) , and 35.2% were osteopenic , but no significant correlations between t score and grade or number of fractures were found . 
le fratture vertebrali ( fv ) rappresentano il segno caratteristico dellosteoporosi e sono responsabili di circa 70000 ricoveri ospedalieri ogni anno , con notevoli implicazioni per quel che concerne i costi sociali e la scadente qualit di vita dei pazienti . 
negli ultimi anni diverse tecniche , sia qualitative che quantitative , sono state proposte per la diagnosi di fv , ma allo stato attuale non ancora disponibile una metodica considerata gold standard e la valutazione visiva semiquantitativa ( vsq ) proposta da genant , resta la pi validata . 
scopo del nostro studio stato quello di valutare la percentuale di fv non diagnosticate nella pratica clinica in una popolazione italiana , usando il metodo vsq e una nuova tecnica morfometrica . 
per la valutazione delle fv , in 283 donne in et postmenopausale giunte alla nostra osservazione per lo screening dellosteoporosi , abbiamo effettuato : lesame clinico , i radiogrammi tradizionali del rachide ( per il metodo vsq ) e la morfometria digitale computerizzata ( mdc )  . 
il 47% dei pazienti presentava un t score < 2 , 5 deviazioni standard ( ds ) ed il 35 , 2% presentava una condizione osteopenica , tuttavia non stata riscontrata 1102 radiol med ( 2010 ) 115 : 11011110 conclusions . 
vfs went undetected in 55.5% according to the vsq method on standard spinal radiographs . therefore , the morphometric technique may be helpful when performed with the semiquantitative approach to improve recognition of vfs . 
 parole chiave fratture vertebrali rachide osteoporosi morfometria digitale computerizzata dxa raggi x introduction introduzione osteoporosis is a major public health concern associated with considerable medical , social and financial burdens . 
low bone mass and microarchitectural deterioration of bone tissue increase bone fragility and the consequent risk of disabling fractures , mainly of the vertebrae , femur , pelvis and wrist , as well as pain , deformity and even death . 
nevertheless , vfs are considered the highest predictors of femoral fractures , the consequences of which may be even lethal , mostly in the elderly [ 2 , 3 ]  . 
unlike hip or wrist fractures , vfs are often asymptomatic and occur in the absence of specific trauma , which contributes to the problem of underdiagnosis and undertreatment [ 46 ]  . 
an existing vf , independent of bone mineral density ( bmd ) , increases the risk of a subsequent fracture ; in fact , many fragility fractures occur in patients with bmd within normal limits because the techniques for bmd measurement such as dual - energy x - ray absorptiometry ( dxa ) , despite allowing an accurate and early diagnosis of osteoporosis [ bmd 2.5 standard deviations ( sd ) below the mean peak values for normal bone according to the world health organization ] , provide only a quantitative estimation that does not account for bone structure and quality of residual bone , which may significantly affect the risk of fractures [ 79 ]  . plain spinal radiographs remain the most commonly used losteoporosi rappresenta uno dei maggiori problemi inerenti la salute pubblica con conseguenti oneri medici , sociali e finanziari . 
la ridotta massa ossea ed il deterioramento della microarchitettura del tessuto osseo in tale condizione patologica aumenta la fragilit ossea ed il conseguente rischio di fratture invalidanti , principalmente a carico dei corpi vertebrali , del femore , delle ossa del bacino e del polso come pure dolore , deformit e morte . 
a differenza delle fratture del femore o del polso , le fv sono spesso asintomatiche e si verificano anche in assenza di uno specifico evento traumatico il che contribuisce al problema della mancata diagnosi e del trattamento tardivo [ 46 ]  . 
given the lack of a standardised method , in recent years , several techniques , both qualitative and quantitative , have been proposed , but a gold standard is not yet available . 
in the last few years , several quantitative approaches , such as morphometric x - ray radiography and morphometric x - ray absorptiometry have been used with a view to reducing the operator bias in the vsq method [ 11 , 12 ]  . 
qualitative assessment , despite the advantage of discrimination between osteoporotic fractures and other vertebral deformities ( osteoporosis , trauma , degenerative disease , scheuermanns disease , congenital anomaly , neoplastic disease , haematopoietic disorders , infectious disease and pagets disease ) , is limited by subjectivity of the diagnosis and overestimation of vertebral deformities [ 1 , 13 ]  . unfortunately , as recently reported , in clinical practice , the diagnosis of vfs is often missed , and patients are not correctly assessed . 
the aim of our study was to estimate the percentage of vfs not detected in clinical practice by using semiquantitative assessment by an expert musculoskeletal radiologist and a new morphometric technique . materials and methods we enrolled 283 postmenopausal women referred to our clinic for osteoporosis screening . 
these women were referred by their family physicians as outpatients for their programmed specialist visit and met the following inclusion criteria : age > 45 years and at least 1 year postmenopause . patients were excluded if they were taking antiosteoporotic drugs ( apart from calcium / vitamin d supplementation ) and if they had a previous radiological diagnosis of vf . a conventional lateral and anteroposterior spine radiograph of both thoracic and lumbar vertebrae was performed in each individual . 
patients underwent a clinical examination by a physician , and bone mass was measured by the dxa system ( dpx pro , ge medical system , madison , wi , usa )  . 
a preliminary vsq assessment of the radiographs was performed using the genant method . subsequently , each t4l4 radiograph was centrally digitised using a twain scanner ( umax power look 1000 , techville , inc . , dallas , tx , usa ) connected via usb port to a desktop pc . 
the images were then assessed by digital computerised morphometry ( dcm ) using dedicated software ( spine - x analyzer , cam diagnostics , milan , italy ) that calculates the vertebral height ratios of each vertebra based on a standard six - point identification method of the three vertebral heights . 
data lassenza di una metodica standardizzata , negli ultimi anni sono state proposte diverse tecniche , sia qualitative che quantitative , ma ad oggi non ancora disponibile un approccio ideale . 
negli ultimi anni , sono stati utilizzati diversi approcci quantitativi come la morfometria radiografica e la morfometria assorbimetrica con lintento di ridurre gli errori di valutazione operatore - dipendenti che inficiavano il metodo vsq [ 11 , 12 ]  . 
la valutazione qualitativa , nonostante il vantaggio della diagnosi differenziale tra fratture da osteoporosi ed altre deformit vertebrali ( osteoporosi , trauma , malattie degenerative , malattia di scheuermann , anomalie congenite , patologia neoplastica , disordini emolinfopoietici , malattie infettive e morbo di paget ) , limitata dalla soggettivit diagnostica e dalla sovrastima delle deformit vertebrali [ 1 , 13 ]  . 
lo scopo del nostro lavoro stato quello di stimare la percentuale di fv non diagnosticate nella pratica clinica , utilizzando la valutazione semiquantitativa effettuata da un radiologo esperto di radiologia muscolo - scheletrica ed una nuova tecnica morfometrica . materiali e metodi duecentoottantatre donne in et post - menopausale afferenti al nostro istituto per lo screening dellosteoporosi sono state arruolate nel presente lavoro . 
tali pazienti ambulatoriali , indirizzate dai propri medici di medicina generale per le loro visite specialistiche programmate , soddisfacevano i seguenti criteri di inclusione : et > 45 anni ed inizio della menopausa da almeno un anno . 
le pazienti venivano escluse dal nostro studio se in trattamento con farmaci antiosteoporotici ( fatta eccezione per la supplementazione di calcio / vitamina d ) e se presentavano una pregressa diagnosi radiologica di fv . per ciascun paziente stata effettuata una radiografia del rachide in proiezione laterale ed antero - posteriore valutando sia le vertebre toraciche che lombari . 
tutte le pazienti 1104 radiol med ( 2010 ) 115 : 11011110 sono state , inoltre , sottoposte ad un accurata valutazione clinica da parte di un medico di medicina interna e misurazione della massa ossea mediante apparecchiatura dxa ( dpx pro , ge medical system , madison , usa )  . 
una preliminare valutazione vsq dei radiogrammi ottenuti stata effettuata utilizzando il metodo di genant e successivamente ciascun radiogramma del rachide da t4 ad l4 stato digitalizzato utilizzando uno scanner twain ad alta risoluzione ( umax power look 1000 , techville , inc . , dallas , usa ) connesso mediante porta usb ad una workstation dedicata e quindi effettuando la morfometria digitale computerizzata ( mdc ) con lausilio di un software dedicato ( spine - x analyzer , cam diagnostics , milano , italia ) in grado di calcolare i rapporti tra le altezze vertebrali per ciascuna vertebra mediante un metodo di identificazione standard a 6 punti delle 3 altezze vertebrali . 
la riduzione del 20% di unaltezza vertebrale stata scelta come valore soglia per la definizione di deformit vertebrale ; le deformit sono state definite lievi , moderate e severe sulla base di una riduzione del rapporto delle altezze del 20%25% , 25%40% e pi del 40% , rispettivamente [ 13 ]  . 
i vantaggi nellutilizzo della mdc sono i seguenti : ingrandimento delle immagini ad un determinato livello e selezione dei livelli di contrasto e luminosit per unottimale visualizzazione della corticale ossea , capacit particolarmente utile quando la pellicola di modesta qualit . 
tuttavia , la mdc non permette di distinguere le fv su base osteoporotica dalle deformit legate ad altri fattori , come la patologia degenerativa disco - somatica meglio valutabile da un occhio esperto . 
 inoltre , i radiogrammi tradizionali sono stati esaminati in cieco da un radiologo esperto in patologia muscolo - scheletrica ( gg ) con 20 anni di esperienza nel campo delle patologie metaboliche dellosso , utilizzando la valutazione vsq secondo genant per lo studio delle fv . 
valori di kappa score inferiori a 0 , 40 indicano uno scarso livello di concordanza tra le due metodiche , valori tra 0 , 41 e 0 , 60 indicano una discreta concordanza e valori compresi tra 0 , 61 e 0 , 80 sono indicativi di una buona concordanza . 
1 conventional lateral radiograph of the thoracic spine showing a diffuse osteopoenic condition , increased density along the endplates and several wedge - like vertebral deformities ( grade 1 : 20%25% )  . 
1 il radiogramma del rachide dorsale in proiezione laterale mostra una diffusa condizione osteopenica , accentuata radiopacit delle limitanti somatiche e plurime deformit vertebrali cuneiformi ( grado 1 : 20%25% ) non indicate nei corrispettivi referti . 
la mdc meglio delimita laltezza posteriore , mediana e anteriore di ciascuna vertebra , quantificando la perdita in altezza di ogni corpo vertebrale a livello di t5t8 . each vertebral body to describe vertebral shape . 
a 20% reduction of any vertebral height ratio was chosen as a threshold for the definition of vertebral deformity ; deformities were defined as mild , moderate and severe based on a height ratio decrease of 20%25% , 25%40% and > 40% , respectively [ 13 ]  . 
the advantages in performing dcm are the following : magnification of the images to a specific level and selection of the contrast and brightness levels for optimum visibility of the cortical bone , a capability that is especially valuable when the film is of less than optimal quality . 
on the other hand , dcm is unable to distinguish osteoporotic vfs from vertebral deformities due to other factors , such as degenerative spine and disc disease , which is best evaluated by an expert eye . 
 in addition , the x - ray films were blindly analysed by a senior musculoskeletal radiologist ( gg ) , with 20 years of experience in the field of metabolic bone disease , using genants semiquantitative grading scheme ( vsq ) for assessing vfs . 
analysis was performed on data of quantitative morphometry . finally , the kappa ( k ) score was calculated for interle caratteristiche cliniche della popolazione studiata sono radiol med ( 2010 ) 115 : 11011110 1105 riportate nella tabella 1 . 
il 47% delle pazienti aveva un t score < 2 , 5 ds , il 35 , 2% era osteopenico ed il 17 , 6% era normale . non stata riscontrata alcuna correlazione significativa tra il t score e il grado o numero di fv . 
in accordo con la valutazione vsq 53 pazienti avevano una frattura , 39 pazienti avevano > 2 fv ; la mdc ha identificato una frattura in 65 pazienti , > 2 fv in 44 . 
 la percentuale di discordanza tra la mdc e la valutazione vsq era esigua in tutti i casi di deformit di grado moderato ; non vi era alcuna differenza quando erano analizzate deformit di grado severo mentre si osservava una discordanza significativa tra le due tecniche quando si consideravano deformit di grado lieve . 
2 conventional lateral radiograph of the lumbar spine showing a grade 1 deformity ( 20% ) , with mild anterior wedging of l1 and l4 ; dcm best quantified the loss in height of these vertebral bodies . 
3 prevalenza delle fratture vertebrali identificate sia mediante la morfometria digitale computerizzata ( dcm ) che mediante valutazione visiva semiquantitativa ( vsq ) blindly analysed the x - ray films using the genant criteria ( vsq ) , the prevalence was 32.5%. 
according to the vsq assessment , 53 patients had one fracture , 39 had > 2 vfs ; dcm identified one fracture in 65 patients , > 2 vfs in 44 . overall , 280 vfs were detected by dcm , whereas 236 vfs were diagnosed by the vsq method . 
importantly , reading the radiography reports , only 105 vfs were noted by the referring radiologist . the rate of disagreement between dcm and vsq assessment was reduced in all cases of moderate deformities . there was no difference when considering severe deformities , and there was a significant disagreement among the two techniques when mild deformities were taken into account . 
both methods showed that most fractures occurred in the t6t8 interval and l1l2 . end - plate fractures were the most common ( 68.9% by dcm , 58.4% , by vsq )  . 
 discussione in questo studio abbiamo valutato la percentuale delle fv , non identificate nella pratica clinica , utilizzando la valutazione semiquantitativa ed una nuova tecnica morfometrica . abbiamo dimostrato che le fv , nella pratica clinica , sono diagnosticate solo nel 35% dei casi . 
inoltre , abbiamo osservato che nel 55 , 5% dei casi le fv erano misconosciute mediante la valutazione vsq effettuata sui radiogrammi standard del rachide che rappresentano ancora la sola metodica approvata per la diagnosi delle fratture vertebrali dalla food and drug administration ( fda ) americana . 
in aggiunta , la tecnica morfometrica ( mdc ) stata in grado di identificare le fv nel 38 , 5% dei nostri pazienti ( rispetto al 32 , 5% mediante i criteri di genant )  . i nostri dati sulla percentuale delle fv misconosciute confermano i risultati di due importanti studi : lo studio di gelbach et al . 
delle 934 donne in et post - menopausale ricoverate , fratture vertebrali di grado moderato o severo sono state identificate nel 14% dei radiol med ( 2010 ) 115 : 11011110 discussion in this study , we estimated the percentage of vfs not detected in clinical practice by using the semiquantitative assessment and a new morphometric technique . 
we also observed that vfs went undetected in 55.5% of cases by vsq assessment on standard spine radiograms , which are still the only modality approved by the us food and drug administration for diagnosing vfs . 
of 934 postmenopausal women admitted to one hospital , moderate to severe vertebral fractures were identified in 14% on routine chest radiographs . furthermore , only half of the official radiology reports documented these fractures . 
importantly , the impact study was a global study , and a well - defined protocol had been provided in advance to avoid ambiguity in fracture definition and emphasise the importance of a standardised method . 
different studies that aimed to compare morphometric techniques with vsq assessment have been conducted , although a comparison between these studies is difficult owing to the use of different qualitative and quantitative methods [ 20 ]  . the study populations vary widely in these reports , and the large variation depends also on differences in the number , type and severity of prevalent deformities detected in each study . 
in our study , the percentage of deformities identified by dcm and not by vsq assessment may be important for a further follow - up of patients . in fact , even if vfs are not identified at initial analysis , they may be taken in consideration at subsequent evaluation . 1107 radiogrammi del torace eseguiti di routine . 
tuttavia , la prevalenza delle mancate diagnosi era sovrapponibile . anche lo studio impact , condotto in tutto il mondo su 2000 donne in et post - menopausale , ha mostrato che il 30% delle fv non veniva diagnosticato . 
rilevante che limpact era uno studio mondiale ed un protocollo ben definito era stato preventivamente fornito onde evitare ambiguit nella definizione di fratture e sottolineando limportanza di una metodica standardizzata . 
oltre a ci , stata riscontrata una buona concordanza tra le due differenti tecniche nellidentificazione e classificazione delle fv , differendo maggiormente quando laltezza delle vertebre era di poco ridotta . 
sono stati eseguiti diversi studi con lobiettivo di confrontare le tecniche morfometriche e la valutazione vsq , sebbene un confronto tra questi studi risulta difficile per luso di differenti metodiche qualitative e quantitative [ 20 ]  . 
nel nostro studio , la percentuale delle deformit identificate mediante mdc e non con la valutazione vsq pu essere importante nel follow - up dei pazienti . infatti anche se le fv non sono identificate ad una prima analisi , possono essere considerate in una successiva valutazione . le fv su base osteoporotica hanno importanti ripercussioni sulla salute pubblica , compresa disabilit ed aumentata mortalit . 
la fondazione internazionale dellosteoporosi ( iof ) stima che pi del 40% delle donne di media et in europa saranno affette da una o pi fratture da osteoporosi durante il resto della loro vita [ 21 ]  . 
attualmente , la valutazione clinica delle fv basata sullapproccio semiquantitativo ( basato sui criteri di genant ) che , tuttavia , presenta una sensibilit ed una specificit parzialmente influenzate dallabilit delloperatore . osteoporosis - related vfs have important health molti studi hanno valutato lassociazione tra fv e il 1108 radiol med ( 2010 ) 115 : 11011110 consequences , including disability and increased mortality . the iof ( international osteoporosis foundation ) estimates that > 40% of middle - aged women in europe will be affected by one or more vfs in their life [ 21 ]  . 
however , vfs often do not produce symptoms , and diagnostic evaluation has excessively low sensitivity [ 3 ]  . currently , clinical assessment for vfs is based on a semiquantitative approach ( genants criteria ) that has a sensitivity and specificity partially influenced by the skill of the operator . many studies have investigated the association between vfs and impairment of quality of life , which leads to a greater risk of limited activity , days confined to bed and increased number of physician visits [ 3 , 22 ]  . 
in the hizen - oshima study , a strong association [ odds ratio ( or = 4.1 ) ] of deformities with physical impairment was observed among 584 japanese women aged 4089 years . 
impaired function was measured by a selfadministered questionnaire to evaluate selected basic and instrumental activities of daily living ( adl test ) , and it was considered significant when at least three functions were impaired [ 24 ]  . 
therefore , an early diagnosis of vertebral deformities may be important to prevent further progression of the deformity or to avoid , by treating the patient , progression of the pathological process to other vertebral bodies . 
the individuals enrolled came to our clinic for back pain or for a previous diagnosis of osteoporosis , and thus formed a selected cohort of symptomatic patients and not a randomised postmenopausal population . 
this technique , despite reduced x - ray exposure and the feasibility of the procedure and analysis , has the limitation of point placement , dependence on a trained operator and lack of information . 
moreover , dcm may be performed in obese persons or persons with scoliosis or severe arthritis , which is difficult to analyse with dxa . the initial results obtained with dcm do not allow us to use quantitative morphometry alone . 
this technique , if performed together with the semiquantitative approach , can deterioramento della qualit di vita , che conduce ad un maggior rischio di inabilit , periodi di allettamento ed incremento del numero di visite mediche [ 3 , 22 ]  . 
nello studio hizen - oshima stata osservata una notevole associazione ( odd ratio [ or ] = 4 , 1 ) tra deformit e deterioramento fisico in 584 donne giapponesi di et compresa tra 40 e 89 anni . 
uno scadimento delle abilit stato stimato mediante un questionario di autovalutazione atto a valutare selezionate attivit di base ed attivit strumentali della vita quotidiana ( adl tests ) ed stato considerato significativo quando almeno tre funzioni erano inficiate [ 24 ]  . 
perci , una diagnosi precoce delle deformit vertebrali pu essere importante per prevenire unulteriore progressione della malattia onde evitare , previo trattamento del paziente , lestensione del processo patologico ad altri corpi vertebrali . 
infatti , i pazienti con una fv hanno un pi elevato rischio di sviluppare nuove fratture [ 26 ]  . con questo studio noi vogliamo enfatizzare la necessit di una attenta valutazione clinica e limportanza di una diagnosi precoce e corretta delle fv , che spesso risultano misconosciute dai medici . 
i soggetti arruolati afferivano alla nostra clinica per dolore lombare o per pregressa diagnosi di osteoporosi , rappresentando una coorte selezionata di pazienti sintomatici e non una popolazione post - menopausale randomizzata . sfortunatamente , non esiste una metodica considerata gold standard per la diagnosi di fv . 
questa tecnica , anche se ha una ridotta esposizione alle radiazioni ionizzanti e facile riproducibilit ed analisi , ha il limite del corretto posizionamento dei punti , la dipendenza da un operatore esperto e lassenza di ulteriori informazioni diagnostiche . 
infatti , i radiogrammi tradizionali hanno il vantaggio di un ampio spettro di elementi diagnostici , compresa la possibilit di effettuare una diagnosi differenziale con altri processi patologici . inoltre , la mdc pu essere eseguita in soggetti obesi o con scoliosi , o con importanti artropatie difficilmente analizzabili mediante dxa . 
the combination of a qualitative and a quantitative method may be the best choice , above all during clinical trials or for the follow - up , in order to benefit from the respective advantages of each method [ 30 ]  . 
 trials clinici o per il follow - up , lassociazione di una metodica qualitativa e quantitativa pu rappresentare la scelta migliore al fine di utilizzarne i rispettivi vantaggi [ 30 ]  . 
la tecnica morfometrica pu essere un utile metodica da realizzarsi unitamente allapproccio semiquantitativo , per ottimizzare la diagnosi delle fv migliorando cos la selezione dei pazienti da trattare . comunque , ulteriori studi sarebbero necessari per supportare la validit di questa nuova tecnica morfometrica nella pratica clinica . conflict of interest none congenital diseases and syndromes . 
reiser springer - verlag , berlin , heidelberg , 2009 isbn 978 - 3 - 642 - 00159 - 8 published online : 30 march 2010 springer - verlag 2010 according to the author of this text radiology is to me an art more than a science : an art of imaging the human body , and an art of extracting information from an image . the aim of the book is to present to the reader , in a concise , easy to read and easy to reference style the results of years of research in the field of congenital diseases and syndromes . 
 there are six fields of interest [ central nervous system ( cns ) , head and neck , chest and heart , abdomen and pelvis , musculoskeletal system , phakomatoses ( neurocutaneous syndromes ) ] to cover in a 195 page text ( plus a well structured index ) 80 malformations and syndromes . each topic is concisely and precisely described , illustrated by well chosen radiological images and when deemed necessary well prepared drawings ( the first author is a medical illustrator ) ; diagnostic boxes for the significant clinical and radiological diagnostic points and sometimes question boxes regarding possible differential diagnostic points , plus a very short reference list for further reading are included . clearly this book cannot compete with more extensive ones on the matter ( for example lachmanss taybi and lachmans radiology of syndromes , metabolic disorders and skeletal dysplasias ) and this is clearly stated : it should be considered a first - aid crib in daily practice for young doctors and trainees and is recommended reading for clinicians as well as radiologists . secondo quanto affermato nella prefazione : radiology is to me an art more than a science : an art of imaging the human body , and an art of extracting information from an image . 
a total of 106 magnetic resonance cholangiopancreatography ( mrcp ) examinations performed between december 2007 and september 2008 were evaluated with a comparison of 2d ssfse ( thin section and thick slab ) , breath - hold 3d frfse and respiratory - triggered 3d frfse sequences . 
the biliary tract was divided into seven segments : right hepatic duct , left hepatic duct , common hepatic duct , cystic duct , common bile duct , cystic duct junction and biliarypancreatic confluence . 
centosei esami di colangiopancreatografia in risonanza magnetica ( rm ) eseguiti tra dicembre 2007 e settembre 2008 sono state analizzati confrontando ssfse 2d ( con spessore sottile e con slab ) , frfse 3d breath - hold e frfse 3d triggerate con il respiro . 
lalbero biliare stato suddiviso in 7 segmenti : dotto destro , dotto sinistro , dotto epatico comune , dotto cistico , coledoco , inserzione cistico - coledocica e confluenza coledoco - pancreatica . 
rispetto alle ssfse 2d , frfse triggerate hanno evidenziato migliore visualizzazione dellepatico destro ( p = 0 , 0277 ) , del cistico ( p = 0 , 0081 ) , della giunzione cistico - coledocica ( p = 0 , 0010 ) e delle varianti biliari ( p = 0 , 0198 ) ; nel confronto 3d frfse breath - hold versus ssfse 2d , stata rilevata differenza statisticamente significativa nella visualizzazione del cistico ( p = 0 , 027 ) , del punto dinserzione del cistico ( p = 0 , 020 ) , della confluenza coledoco - pancreatica ( p = 0 , 0338 ) e delle varianti biliari ( p = 0 , 0311 )  . 
frfse 3d rappresentano un importante valore aggiunto allimaging convenzionale 2d . 468 radiol med ( 2010 ) 115 : 467482 keywords magnetic resonance cholangiopancreatography biliary and pancreatic imaging parole chiave risonanza magnetica colangiopancreatografia imaging biliare e pancreatico introduction introduzione the aim of our study was to compare visualisation of the biliopancreatic system obtained with cholangiopancreatography 3d fast recovery fast spin - echo ( frfse ) sequences and 2d single - shot fast spin - echo ( ssfse ) sequences . 
the intention was to emphasise the added value of the 3d frfse sequences , which are better able to visualise the biliopancreatic system than are conventional 2d sequences . since the introduction of magnetic resonance cholangiopancreatography ( mrcp ) in 1991 , a number of studies in the literature have emphasised its noninvasive diagnostic role in the study of biliopancreatic disease [ 16 ]  . semiinvasive surgery , such as laparoscopic cholecystectomy , oncological surgery and liver transplant surgery , have found mrcp to be a valuable and indispensable aid in both preoperative and postoperative phases for accurate visualisation of the preand postsurgical anatomy [ 7 , 8 ]  . the need for accurate biliary imaging also derives from the notable anatomical variability in the biliopancreatic system [ 911 ]  . various published studies have investigated the acquisition techniques of mrcp [ 1214 ]  . 
in our study , we evaluated visualisation of the biliopancreatic system and compared 2d ssfse sequences with 3d frfse sequences acquired with both the breath - hold and respiratory - triggered techniques . 
 the 2d ssfse sequences are largely used in mrcp and acquired with a variable slab ( generally between 50 and 60 mm ) in extremely short acquisition times ( an acquisition every 12 s )  . 
the 3d frfse sequences are characterised by a high signal - to - noise ratio ( snr ) and are acquired with both the breath - hold and respiratory - triggering techniques . 
in frfse acquisitions a 90 flip - back pulse is applied prior to the subsequent excitation , which brings the magnetisation vector back into the longitudinal plane , with a resulting increase in snr . 
with postprocessing the 3d frfse , sequences are able to satisfy a number of clinical and surgical requirements for hepatic , biliary and pancreatic imaging . in the various study planes , reconstructions demonstrate scopo del nostro lavoro confrontare la visualizzazione del sistema bilio - pancreatico ottenuta mediante sequenze colangiopancreatografiche fast recovery fast spin - echo 3d ( frfse ) e mediante sequenze single - shot fast spin - echo 2d ( ssfse )  . 
si vuole , infatti , sottolineare il valore aggiunto delle sequenze 3d frfse , che mostrano capacit di visualizzazione del sistema bilio - pancreatico a tratti superiore rispetto alle convenzionali sequenze 2d . 
 sin dalla sua introduzione , nel 1991 , diversi studi in letteratura hanno sottolineato il ruolo diagnostico non invasivo della colangiopancreatografia in risonanza magnetica ( rm ) nella patologia bilio - pancreatica [ 16 ]  . 
la chirurgia semi - invasiva , quale la colecistectomia laparoscopica , la chirurgia oncologica e la chirurgia dei trapianti del fegato , hanno trovato nella colangio - rm un prezioso ed indispensabile strumento di indagine , non soltanto in fase prechirurgica , ma anche post - chirurgica , al fine di ottenere una visualizzazione accurata dellanatomia pree postintervento [ 7 , 8 ]  . 
nel nostro studio valutiamo la visualizzazione del sistema bilio - pancreatico , mettendo a confronto sequenze ssfse 2d , sequenze frfse 3d acquisite con tecnica breath - hold e sequenze frfse 3d acquisite in modalit triggerata . le ssfse 2d sono sequenze largamente adoperate nella colangio - pancreatografia rm , acquisite con slab variabile ( generalmente tra i 50 e i 60 mm ) , in tempi estremamente bassi ( unacquisizione ogni 12 secondi ) ; nella maggior parte dei casi , al fine di aumentare la panoramicit di visualizzazione , vengono acquisite in un loop radiale , centrato o sulla convergenza biliare primaria o a livello della confluenza bilio - pancreatica . 
le frfse 3d sono sequenze dotate di un elevato rapporto segnale - rumore , acquisite sia con tecnica breath - hold che in modalit triggerata con il respiro ; nelle acquisizioni frfse lapplicazione di un impulso di rifocalizzazione a 90 alla fine del treno di echi fse riconduce nel piano longitudinale il vettore di magnetizzazione , con aumento del rapporto segnale / rumore . 
tali sequenze vengono facilmente ricostruite secondo piani dedicati di studio , in modo da ottenere immagini multi - planar reformatting ( mpr ) e maximum intensity projection ( mip )  . radiol med ( 2010 ) 115 : 467482 the anatomy and presence of anatomical variants of the bile and / or cystic ducts . 
correct identification of anatomical variants of the biliary tract is vital for adequate preoperative planning in the case of gallbladder ( laparotomic or laparoscopic cholecystectomy ) or biliary - tract surgery . 
accurate visualisation of the hepatic hilum , and in particular of the biliary structures at that level , is one of the fundamental aims in liver transplantation imaging , and the possibility of dedicated reconstruction planes offers advantages to both the radiologist and the surgeon in preoperative planning and follow - up of liver transplant patients . materials and methods examination protocol and study population we reviewed 106 mrcp examinations performed at our centre between december 2007 and september 2008 . 
images were acquired with an eight - channel phased - array body coil . prior to each examination , written informed consent was obtained for all patients . for image evaluation , we included patients with different indications for undergoing mrcp . 
in most cases , the mr examination was performed on the basis of clinical and / or instrumental diagnostic suspicion of biliary disease ( choledocholithiasis , cholangiocarcinoma , etc . ) , identified with laboratory tests ( elevated cholestasis markers ) or following other examinations ( transabdominal ultrasound )  . 
in other cases , the mr examination was requested based on clinical and / or instrumental diagnostic suspicion of pancreatic disease ( pancreatitis , pancreatic tumour , etc . ) following the finding of abnormal laboratory markers [ pancreatic amylase , pancreatic lipase , markers of extrahepatic cholestasis , increase in carbohydrate antigen 19 - 9 ( ca 199 ) ] or an abnormal finding at ultrasound or multidetectorrow computed tomography ( mdct )  . 
patients with a history of a prior biliodigestive anastomosis and patients with a biliary prothesis were excluded from the evaluation . the study protocol involved the acquisition of between six and ten sequences . 
therefore , each mrcp study not only included specific sequences for visualisation of the biliary tract but also morphological sequences aimed at studying the organs containing biliopancreatic structures , i.e. 
 le ricostruzioni dimostrano secondo piani dedicati lanatomia di eventuali varianti biliari e / o del dotto cistico . la corretta identificazione delle varianti anatomiche biliari e cistiche si rende necessaria per unidonea pianificazione pre - operatoria nel caso di interventi riguardanti la colecisti ( colecistectomia laparotomica o laparoscopica ) o le vie biliari . 
unaccurata dimostrazione dellanatomia dellilo epatico , ed in particolare delle strutture biliari a tale livello , uno degli obiettivi fondamentali da perseguire nellimaging dei trapianti epatici , e la possibilit di piani di ricostruzione dedicati offre vantaggi sia al radiologo che al chirurgo nella pianificazione pre - operatoria che nel follow - up del trapianto di fegato . materiali e metodi protocollo desame e popolazione di studio sono stati analizzati 106 esami di colangiopancreatografia rm eseguiti presso la nostra unit operativa nel periodo compreso da dicembre 2007 sino a settembre 2008 . 
gli esami sono stati eseguiti con apparecchiatura rm da 1 , 5 tesla ( signa hdx mr system ge - general electric ) ; le immagini sono state acquisite con bobine body 8ch phased array . 
prima di ogni esame stato acquisito un modulo di consenso informato allesecuzione della metodica rm . nella valutazione delle immagini sono stati inclusi pazienti con indicazioni diverse allesecuzione di una colangiopancreatografia rm . 
in molti casi , infatti , lesame rm stato eseguito in relazione al sospetto clinico e / o diagnostico strumentale di malattia biliare ( coledocolitiasi , colangiocarcinoma , ecc . ) , rilevato per mezzo di indagini di laboratorio ( rialzo degli indici di colestasi ) o a seguito di altri esami ( ecografia trans addominale ) ; in altri casi lindicazione alla rm scaturita dal sospetto clinico e / o diagnostico strumentale di malattia pancreatica ( pancreatite , neoformazione pancreatica , ecc . ) , a seguito del riscontro di unalterazione dei parametri di laboratorio ( amilasi pancreatica , lipasi pancreatica , indici di colestasi extraepatica , aumento del marker ca 19.9 ) o di unalterazione rilevata allecografia o alla tomografia computerizzata ( tc ) multidetettore ; in alcuni pazienti stata posta lindicazione allesame per ottenere una valutazione pre - operatoria del sistema biliare ( ad esempio prima di interventi di anastomosi bilio - digestiva o di colecistectomia laparoscopica )  . 
the 2d ssfse ( singleshot fast spin - echo ) sequences were obtained with thin multisection acquisitions with tr infinite , te 90 ms , thickness 4 mm , matrix 320320 ; and with thick section acquisitions with 50 - mm slab , tr infinite , te 1 , 100 ms , matrix 512384 . 
the thick - slab sequences were acquired with a radial loop being centred at the level of the primary biliary convergence and at the biliopancreatic confluence . the first image of the radial loop was placed along the posterior border of the right hepatic lobe . 
the 3d frfse sequences were performed both during breath - hold at end expiration and in respiratory - triggering modality in an oblique coronal plane ( parallel to the common bile duct ) and in axial planes , with coverage of the hepatic - pancreatic volume of interest for the evaluation of the biliary and pancreatic ducts . breath - hold 3d frfse sequences were carried out with the following parameters : tr 4 , 000 ms , te 722 ms , thickness 3 mm , matrix 256192 , field of view ( fov ) 3636 . duration of the acquisitions performed with the breath - hold technique was 2026 s ( 2224 s in 85 examinations )  . 
respiratory - triggered 3d frfse sequences were done with acquisitions at each respiratory interval with effective tr corresponding to 1 r - r respiratory cycle ( one respiratory interval generally around 4 , 000 ms , with te 722 ms ) , thickness 23 mm , matrix 256256 , fov 3636 . 
duration of the respiratory - triggered 3d frfse sequences , with 2.2mm thickness , was around 2 min 40 s in a patient with a normal respiratory cycle ( around 15 breaths / min )  . 
the order of the three types of mrcp sequences 2d ssfse , breathhold 3d frfse and respiratory - triggered 3d frfse was randomised . where necessary , the studies were completed with t1weighted 3d fspgr sequences obtained in baseline conditions and after the intravenous administration of a 0.1mmol / kg dose of gadolinium benzyloxyproprionicnumero di sequenze tra sei e dieci ; pertanto ogni studio di colangio - pancreatografia rm non ha incluso solamente sequenze colangio - rm specifiche per la visualizzazione delle vie biliari , ma anche sequenze morfologiche rivolte allo studio degli organi contenenti le strutture biliopancreatiche , quali fegato e pancreas ( il cosiddetto contenente )  . 
nel protocollo desame sono state effettuate : sequenze assiali fast spoiled gradient - echo ( fspgr ) t1 in fase e fuori fase ( tempo di eco [ te ] rispettivamente di 2 , 2 e 4 , 4 ms , thickness 6 mm , spacing 1 mm ) ; sequenze steady state free precession ( ssfp ) a sangue bianco , secondo piani coronali ed assiali ( tempo di ripetizione [ tr ] 3 , 9 ms , te 1 , 7 ms , thickness 6 mm , spacing 0 , 61 mm , matrice 224320 ) ; sequenze fast spin - echo ( fse ) t2 , secondo piani di scansione assiali ( tr 2150 ms , te 102 ms , thickness 5 mm , spacing 1 mm ) ; ssfse t2 realizzate secondo piani coronali ed assiali ( thickness 6 mm , spacing 1 mm , matrice 320288 ) ; sequenze fse t2 assiali anche con soppressione del segnale adiposo e con te fino a 140 ms ( thickness 5 mm , spacing 1 mm )  . la visualizzazione delle vie biliari stata effettuata con sequenze ssfse 2d e frfse 3d . 
le ssfse 2d sono state condotte con acquisizioni a spessore sottile thin multisection ( con tr infinito , te 90 ms , spessore di 4 mm , matrice 320320 ) e con acquisizioni a strato spesso ( con slab di 50 mm , tr infinito , te 1100 ms , matrice 512384 )  . 
le sequenze thick - slab sono state acquisite centrando un loop radiale a livello della convergenza biliare primaria ed in corrispondenza della confluenza bilio - pancreatica ; la prima immagine del loop radiale stata posta lungo il margine posteriore del lobo destro del fegato ; le immagini sono state acquisite in apnea espiratoria . 
le sequenze frfse 3d sono state effettuate sia in apnea espiratoria che in modalit triggerata , secondo un piano coronale obliquo ( parallelo al decorso della via biliare principale [ vbp ] ) e secondo piani assiali , con estensione a coprire il volume epato - pancreatico di interesse ai fini della valutazione dei dotti biliari e pancreatici . 
 le frfse 3d con tecnica breath hold sono state acquisite con i seguenti parametri : tr 4000 ms , te 722 ms , spessore 3 mm , matrice 256192 , campo di vista ( fov ) 3636 ; la durata delle acquisizioni effettuate con tecnica breath - hold stata compresa tra i 20 ed i 26 secondi ( 2224 secondi in 85 degli esami oggetto di studio )  . 
the 3d fspgr sequences were performed with fat suppression ( tr 4.2 ms , te 2.0 ms , thickness 3 mm ) and extended to cover the entire hepaticpancreaticbiliary volume . 
contrast material was administered with a dual - head automatic injector ( medrad spectris )  . thin - section 2d ssfse and the 3d frfse sequences were reconstructed with mpr and mip techniques using a dedicated software package ( ge advantage workstation , general electric )  . 
la somministrazione per os di un agente superparamagnetico negativizzante il contenuto intestinale ( ferumoxsil - lumirem , guerbet ) si resa necessaria al fine di evitare la sovrapposizione di liquidi gastrici e duodenali . 
lordine di acquisizione dei tre tipi di sequenze colangiopancreatografiche ssfse 2d e frfse 3d stato preventivamente randomizzato . gli studi sono stati completati , nei casi in cui ritenuto necessario , con acquizione di sequenze fspgr t1 3d , ottenute in condizioni di base e durante la somministrazione endovenosa di gadopentato dimeglumina ( gd - bopta ) alla dose di 0 , 1 mmol / kg ( multihance 0 , 5 m , bracco imaging spa , milano , italia ) ; le sequenze fspgr 3d sono state effettuate con soppressione del segnale adiposo ( tr 4 , 2 ms , te 2 , 0 ms , thickness 3 mm ) , estese a coprire lintero volume epato - pancreatico - biliare ; le immagini dopo somministrazione di mezzo di contrasto sono state acquisite in modalit dinamica multifasica , con tempi di acquisizione a 20 , 70 e 180 secondi dallinizio della somministrazione di gadolinio . il mezzo di contrasto stato somministrato mediante iniettore automatico a doppia testata ( medrad spectris )  . 
of patients ( % ) choledocholithiasis neoplasms gallbladder stones gallbladder stones + choledocholithiasis cystic duct stones acute pancreatitis chronic pancreatitis no disease 24 ( 24.5 ) 12 ( 12.2 ) 16 ( 16.3 ) 6 ( 6.1 ) 1 ( 1 ) 2 ( 2 ) 13 ( 13.3 ) 24 ( 24.5 ) tabella 2 riscontri diagnostici rilevati nella revisione retrospettiva dei 98 pazienti oggetto di confronto tra le sequenze mrcp diagnosi nu . 
dei pazienti ( % ) coledocolitiasi neoplasie calcolosi della colecisti calcolosi della colecisti + coledocolitiasi calcolosi del dotto cistico pancreatiti acute pancreatiti croniche assenza di patologia 24 ( 24 , 5 ) 12 ( 12 , 2 ) 16 ( 16 , 3 ) 6 ( 6 , 1 ) 1 ( 1 ) 2 ( 2 ) 13 ( 13 , 3 ) 24 ( 24 , 5 ) biliary tract stones , 12 / 98 cases of biliopancreatic tumour and 2 / 98 cases of acute pancreatitis . 
the reference standard for the diagnostic hypotheses formulated with mrcp was at least one of the following modalities , when available : ( 1 ) endoscopic retrograde cholangiopancreatography ; ( 2 ) surgery and histological examination ( intraoperative or on the surgical specimen ) ; ( 3 ) clinical and laboratory findings and possibly an additional mrcp study performed at 3 months in cases where no treatment was provided . statistical techniques and data analysis different segments of the biliopancreatic tract were analysed . 
the biliary system was subdivided into seven segments : right hepatic duct , left hepatic duct , common hepatic duct , cystic duct , common bile duct , cystic duct junction and biliary - pancreatic confluence . 
nella tabella 1 viene riproposto il protocollo di studio impiegato , con i parametri tecnici delle sequenze colangiopancreatografiche . sono stati analizzati 98 dei 106 esami ( 8 pazienti sono stati scartati per inadeguatezza tecnica desame ) ; nei 98 esami utilizzati per la comparazione sono state sempre eseguite le tre sequenze colangiopancreatografiche ssfse 2d , frfse 3d breath hold e frfse 3d triggerate . nella revisione retrospettiva dei casi , sono state valutate sia colangiopancreatografie rm positive per malattia biliopancreatica , sia colangiopancreatografie rm nelle quali non stata riscontrata alcuna patologia . 
le diagnosi formulate con la rm sono state : calcolosi della colecisti in 16 / 98 casi , litiasi della via biliare in 24 / 98 casi , neoplasie bilio - pancreatiche in 12 / 98 casi e pancreatiti acute in 2 casi ; in un paziente stato identificato un calcolo del dotto cistico ; in 6 casi stata riscontrata litiasi coledocica associata a calcolosi della colecisti , mentre in 13 / 98 pazienti sono stati riscontrati quadri rm di pancreatite cronica . 
il sistema biliare stato suddiviso in sette segmenti : dotto destro , dotto sinistro , dotto epatico comune , dotto cistico , punto di inserzione del cistico a livello della via biliare , coledoco e confluenza coledoco - dotto pancreatico principale . 
anche la visualizzazione ed interpretazione di eventuali varianti anatomiche dellalbero biliare o del sistema pancreatico stato oggetto di studio fra le sequenze , ottenendo in totale 11 classi di segmenti a confronto . 
a ciascun segmento stato attribuito un punteggio secondo la seguente scala di valutazione , rivolta a considerare la maggiore o minore capacit di visualizzazione delle sequenze : 0 mancata visualizzazione ; 1 visualizzazione inferiore a 1 / 2 tratto ; 2 visualizzazione incompleta ma > 1 / 2 del tratto ; 3 tratto visualizzato in maniera completa . al valore ottenuto dalla prima scala di valutazione , stato aggiunto uno score ricavato da una seconda scala di radiol med ( 2010 ) 115 : 467482 pancreatic system was studied , thus making a total of 11 classes of segments to be compared . 
each segment was attributed a score according to the following evaluation scale , which indicates the greater or lesser visualisation by the sequences : 0 no visualisation 1 visualisation < 1 / 2 of the tract 2 incomplete visualisation but > 1 / 2 of the tract 3 complete visualisation of the tract . the value obtained with the first scale was added to a score derived from a second evaluation scale regarding the quality of visualisation of biliopancreatic segments , according to the following point system : 0 poor visualisation with low signal intensity of the biliopancreatic structures and / or blurring artefacts valutazione riguardante la qualit di visualizzazione del segmento bilio - pancreatico , secondo il seguente punteggio : 0 , scarsa visualizzazione , con bassa intensit di segnale delle strutture bilio - pancreatiche e / o artefatti da blurring ; 1 , visualizzazione di grado buono , con intensit di segnale di grado moderato ed assenza di artefatti da blurring ; 2 , visualizzazione di grado eccellente , con alta intensit di segnale delle strutture bilio - pancreatiche e rapporto segnale / rumore elevato . 
 per confrontare le tecniche stato adoperato il test t di student per dati numerici quantitativi appaiati : per ogni segmento sono stati analizzati in maniera appaiata i punteggi numerici di tutti gli esami . 
sono state messe a confronto : sequenze ssfse 2d versus frfse 3d con tecnica 1 good visualisation with moderate signal intensity and breath - hold ; absence of blurring artefacts sequenze ssfse 2d versus frfse 3d acquisite in 2 excellent visualisation with high signal intensity of the modalit triggerata ; biliopancreatic structures and high snr . the techniques were compared with a students t test for quantitative data pairs ; for each segment , a paired analysis was done of the numerical scores for all the examinations . the comparisons were : 2d ssfse sequences versus breath - hold 3d frfse sequenze frfse 3d con tecnica breath - hold versus frfse 3d triggerate . valori di p < 0 , 05 sono stati considerati statisticamente significativi . 
i punteggi sono stati assegnati da due radiologi indipendenti ; lordine di visualizzazione delle sequenze stato preventivamente randomizzato . 2d ssfse sequences versus respiratory - triggered 3d sequences frfse sequences breath - hold 3d frfse sequences versus respiratory - triggered 3d frfse sequences a p value < 0.05 was considered statistically significant . the scores were assigned independently by two radiologists . 
sequences were visualised in random order . risultati results with regard to anatomical variants of the biliary tract , we took as reference the classification of variants proposed by yoshida et al . 
we identified normal confluence in 48 / 98 cases , triple confluence in 28 / 98 cases , presence of a right posterior duct draining into the left duct in 16 / 98 cases , an accessory right duct emptying into the common hepatic duct in 2 / 98 cases , an aberrant right posterior duct draining into the common hepatic duct in 3 / 98 cases and a cystic duct draining into a right aberrant duct ( table 3 )  . anatomical variants of the cystic duct were classified according to drainage site , morphology and course . 
in 61 cases , normal anatomy was identified , with the cystic duct draining along the lateral profile of the middle third of the main bile duct , with regular course . 
abbiamo identificato in 48 / 98 casi una convergenza regolare , in 28 / 98 casi un aspetto a triforcazione ; la presenza di un dotto dorso - caudale slittato sul dotto biliare sinistro stata identificata in 16 / 98 casi , mentre in 2 / 98 casi abbiamo evidenziato un dotto accessorio destro slittato sul dotto comune . 
in 3 / 98 casi stato riscontrato un dotto aberrante dorso - caudale con confluenza nel dotto epatico comune , ed infine in 1 / 98 casi stato dimostrato un cistico impiantato su un dotto destro aberrante ( tabella 3 )  . 
in 6 pazienti abbiamo rilevato un dotto cistico con impianto laterale , altezza regolare e decorso spiraliforme , in 4 pazienti stato visualizzato un dotto cistico di altezza regolare , con impianto anteriore ed in 2 casi un cistico impiantato ad altezza regolare lungo la parete posteriore . 
there were five cases of cystic duct with parallel course and more caudal confluence on the lateral profile , whereas a parallel caudal course with confluence on the medial wall was identified in six cases . only in one case did a cystic duct drain into a right aberrant hepatic duct . 
lastly , in 12 cases , the cystic duct was not identified ( patients with prior cholecystectomy )  . the presence of motion artefacts was encountered more often in breath - hold 3d frfse acquisitions and 2d ssfse acquisitions . 
the 2d sequences both with thin slice and thick slab were flawed by motion artefacts in 22 cases due to the poor breath - hold by the patients , who were often unable to cooperate and correctly perform the instructions provided by the mr operator , even in the case of the short - duration , thick - slab acquisitions . 
in the case of breath - hold 3d frfse acquisitions , the image quality was degraded in 24 cases owing to motion artefacts due to poor patient compliance and the relatively lengthy duration of the breath - hold required for acquisition of the sequences used ( 2224 s )  . 
le sequenze 2d sia con spessore sottile che con thick slab sono state in 22 casi inficiate da artefatti da movimento per lo scarso mantenimento dellapnea da parte del paziente , spesso incapace a collaborare e ad eseguire correttamente le istruzioni fornite delloperatore rm , persino nel caso delle acquisizioni di breve durata thick slab . 
nel caso delle 3d frfse acquisite con tecnica breath hold , in 24 casi la qualit delle immagini stata degradata dalla presenza di artefatti da movimento , dovuti per lo pi a pazienti scarsamente collaboranti ed alla durata relativamente ampia dellapnea necessaria allacquisizione di tal sequenze da noi utilizzata ( 2224 secondi )  . 
1 results of comparison between 2d single - shot fast spin - echo ( ssfse ) and respiratory - triggered 3d frfse sequences , results of the scoring system for visualisation of biliary segments can be observed . 
si osservano differenze statisticamente significative nella visualizzazione del dotto destro , del dotto cistico , del punto di inserzione del cistico a livello del dotto coledocico e della confluenza coledoco - dotto pancreatico . 
no statistically significant difference ( p > 0.05 ) was noted regarding visualisation of the main bile duct and the pancreatic duct , the latter being analysed in all three segments ( head , body and tail )  . 
riguardo la visualizzazione del punto di inserzione del dotto cistico sulla vbp stata osservata una differenza statisticamente significativa a favore delle sequenze 3d con valori di p = 0 , 0010 . 
non si apprezza alcuna differenza statisticamente significativa ( p > 0 , 05 ) riguardo la visualizzazione del dotto coledocico e del dotto pancreatico , questultimo analizzato considerando il tratto cefalico , del corpo e della coda . 
with regard to the pancreatic duct system , no statistically significant difference was found in visualisation of the pancreatic duct at the level of the head and body of the pancreas , whereas the ductal segment in the tail of the parenchyma appeared to be better visualised with 2d sequences , although this finding was not statistically significant . 
per quanto riguarda il sistema duttale pancreatico , non esiste alcuna differenza statisticamente significativa nella visualizzazione del dotto pancreatico a livello del tratto cefalico e del corpo ; la porzione duttale della coda del parenchima , appare meglio visualizzata con le sequenze 2d , seppur con valore statisticamente non significativo . 
3a - e biliary tract variant , with right aberrant duct emptying into the common hepatic duct : 2d ssfse thick - slab acquisitions show cystic duct with caudal insertion and spiraliform course , parallel to common bile duct ( white empty arrow ) ; the aberrant duct draining into the common bile duct is barely visible ( white arrow ) ( a , b )  . 
in a e b ( acquisizioni ssfse 2d thick - slab ) si visualizza il dotto cistico con inserzione caudale e decorso spiraliforme , parallelo al dotto coledocico ( freccia bianca vuota ) ; la confluenza del dotto aberrante nel coledoco scarsamente intuibile ( freccia bianca )  . 
5a , b visualizzazione del dotto cistico lungo la via biliare ; si osserva in a ( acquisizione ssfse thick slab ) il decorso lievemente spiraliforme , con inserzione al terzo medio del dotto coledocico ( freccia bianca ) ; in b ( frfse 3d breath - hold ) dimostra il decorso del dotto cistico con intensit di segnale elevata ( freccia bianca ) ; evidente anche lo slittamento del dotto dorso - caudale destro alla convergenza biliare ( frecce bianche vuote )  . radiol med ( 2010 ) 115 : 467482 fig . 
6a - c an example of biliary anatomical variant compared with 2d ssfse thick - slab ( a ) and breath - hold 3d frfse ( b , c ) sequences . 
3d fspgr acquisitions clearly show the course of this variant parallel to the cystic duct ( white arrow cystic duct , empty white arrow biliary variant in b )  . 
6a - c esempio di variante anatomica delle vie biliari confrontato con sequenze 2d ssfse thick slab ( a ) e 3d frfse ( b , c ) acquisite con tecnica breath - hold . 
le acquisizioni frfse 3d dimostrano chiaramente il decorso di tale variante parallela al cistico ( freccia bianca , dotto cistico ; freccia bianca vuota , variante biliare in b )  . 
in the first comparison , a statistically significant difference was reported in favour of 3d sequences in visualisation of the right hepatic duct , the left hepatic duct , the cystic duct , the common hepatic duct and the pancreatic duct ( in all three segments )  . 
in the second comparison , however , no significant difference was reported with regard to visualisation of the cystic duct , the right hepatic duct , the left hepatic duct and the common hepatic duct . 
only the common bile duct was better visualised with 3d sequences , and there was even an opposite trend in visualisation of the pancreatic duct , with 2d sequences proving superior to 3d sequences . 
in our study , the score attributed to 2d and 3d sequences was derived from visualisation of native and reconstructed images to take advantage of the added value supplied by mpr and mip postprocessing , which are typical features of 3d frfse sequence . 
postprocessing of native images enables clear depiction of the biliary anatomy in dedicated planes , even in several critical points such as the confluence of the cystic duct along the main bile duct . 
 [ 17 ] compared 2d single - ssfse , 2d multissfse and 3d frfse sequences in evaluation of the biliopancreatic syste they analysed visualisation of the first - , secondand third - order branches of the intrahepatic ducts , in addition to the pancreatic duct , the cystic duct and the extrahepatic bile duct the latter being divided into three segments ( middle , upper and lower )  . 
visualisation of the intrahepatic ducts , the extrahepatic duct in the upper and middle segments , the cystic duct and the pancreatic duct was qualitatively higher with 3d frfse sequences ( p < 0.05 ) [ 17 ]  . 
the 3d frfse sequences were acquired with the respiratory - triggered modality . when first introduced , the 3d technique was unable to produce significant advantages in biliopancreatic imaging , in that it required lengthy execution times for image acquisition . 
 [ 18 ] , made it possible to reduce acquisition times and cover a sufficiently large anatomical volume to study the entire biliary syste in addition to reducing acquisition times , the introduction of echoplanar imaging in 3d sequences increased the snr and spatial resolution [ 18 ]  . techniques , according imaging use of parallel imaging has further reduced acquisition frfse e ssfse . 
gli autori hanno confrontato la visibilit ottenuta per segmento prima con sequenze frfse 3d versus sequenze thin section - ssfse 2d , e successivamente con sequenze frfse 3d mip versus sequenze thick slabssfse 2d ; viene riportata una differenza statisticamente significativa a favore delle sequenze 3d nella visualizzazione del dotto destro , del dotto sinistro , del dotto cistico , del dotto epatico comune e del dotto pancreatico ( nelle tre componenti ) , nella comparazione tra le sequenze 2d a strato sottile e le sequenze 3d . 
nel confronto 3d mip versus thick slab 2d , non si rileva invece alcuna differenza significativa riguardo la visualizzazione del cistico , del dotto epatico destro , sinistro e dellepatico comune ; solamente il dotto coledocico stato meglio visualizzato con le 3d , ed addirittura nella visualizzazione del dotto pancreatico si osserva uninversione del trend con 2d thick slab superiori alle 3d . nel nostro studio il punteggio attribuito alle sequenze 2d e 3d stato ricavato dalla visualizzazione delle immagini native e ricostruite , in modo da sfruttare il valore aggiunto dal post - processing mpr e mip , proprio delle sequenze 3d frfse . 
 [ 17 ] hanno confrontato sequenze 2d singlessfse , 2d multi - ssfse e 3d frfse nella valutazione del sistema bilio - pancreatico ; viene analizzata la visualizzazione delle branche di primo , secondo e terzo ordine dei dotti intraepatici , ed inoltre del dotto pancreatico , del dotto cistico e del dotto biliare extra - epatico questultimo ripartito in tre porzioni ( tratto medio , superiore e inferiore )  . 
la visualizzazione dei dotti biliari intra - epatici , del dotto biliare extraepatico nel tratto superiore e medio , del dotto cistico e del dotto pancreatico risultata qualitativamente pi elevata con le frfse 3d ( p < 0 , 05 ) [ 17 ]  . 
le sequenze frfse 3d sono state acquisite in modalit triggerata con il respiro . la tecnica 3d dapprima non aveva prodotto vantaggi significativi nella visualizzazione bilio - pancreatica , in quanto richiedeva lunghi tempi di esecuzione per lacquisizione delle immagini . 
 [ 18 ] di ridurre i tempi di acquisizione , in modo da coprire un volume anatomico ampio e sufficiente a studiare tutto il sistema biliare ; oltre alla riduzione dei tempi , imaging nelle sequenze 3d aumenta il rapporto segnale rumore e la risoluzione spaziale [ 18 ]  . 
 lintroduzione dellecho - planar limpiego dellimaging parallelo ha ulteriormente ridotto i tempi di acquisizione : nelle attuali sequenze 3d frfse radiol med ( 2010 ) 115 : 467482 in current times . 
 respiratory - triggered 3d frfse sequences , the signal reduction associated with the use of array spatial sensitivity encoding technique ( asset ) is compensated by the application of a fast recovery pulse a 90 flip back pulse is applied prior to the subsequent excitation capable of bringing the magnetization vector back in the longitudinal plane with an associated increase in the snr [ 17 , 19 ]  . comparison between the respiratory - triggered and breath - hold 3d sequences shows that mean visualisation scores obtained with respiratory - triggered sequences are higher than those obtained with the breath - hold technique , although the difference is not statistically significant . 
use of asset in 3d acquisitions with the breath - hold technique produced a reduction in acquisition time and therefore in the length of the breath - hold , with the possibility of obtaining good quality images with a 3 - mm thickness . 
the better visualisation obtained with respiratory - triggered 3d sequences and the higher snr of these sequences can be explained by the modality of filling the k - space , which in the triggered sequences occurs at end expiration , thus avoiding motion artefacts that may flaw image quality obtained with the breath - hold technique , given the lengthy duration of the breath - hold ( 2224 s )  . 
in addition , respiratory - triggered 3d frfse sequences were acquired in times ranging from 2 to 3 min and a slice thickness up to approximately 2 mm , thus enabling more detailed visualisation of the biliary anatomy . anatomical variants of the biliary anatomy were better visualised with 3d sequences than with 2d sequences . 
in our experience , although the thick - slab 2d sequences offer a good panoramic appearance of the biliopancreatic anatomy , they do not always offer immediate and easy identification of the anatomical variants of the cystic and biliary ducts . 
correct placement of these targeted slabs is often operator dependent in that it is linked to the ability of the radiologist to identify or suspect a variant during the examination . 
interpretation of an anatomical variant with the use of 3d technique is much simpler in that the volume of the data set is sufficiently broad to cover the entire biliary tract . 
during postprocessing , the biliary and pancreatic anatomy acquired in the 3d volume is analysed with mpr capable of precisely demonstrating any variants , according to dedicated reconstruction planes . it should be borne in mind that native images of 3d frfse sequences are particularly important in identification of possible pathological changes : mip reconstructions , which provide a clear and immediate view of the triggerate la riduzione di segnale legata allimpiego di array spatial sensitivity encoding technique ( asset ) compensata con lapplicazione di un impulso fast recovery , un impulso di 90 applicato alla fine del treno di echi fse , capace di ricondurre nel piano longitudinale il vettore di magnetizzazione , con aumento del rapporto segnale / rumore [ 17 , 19 ]  . 
 dai risultati ricavati nel confronto tra sequenze 3d acquisite in modalit triggerata e con tecnica breath - hold , si rileva che i valori medi di visualizzazione ottenuti con le sequenze triggerate sono lievemente pi elevati rispetto a quelli delle sequenze acquisite con tecnica breath - hold , senza per che si osservi alcuna differenza statisticamente significativa . 
limpiego di asset nelle acquisizioni 3d con tecnica breath - hold ha consentito una riduzione del tempo di acquisizione e dunque di apnea , con la possibilit di ottenere immagini di buona qualit con spessore di 3 m la migliore visualizzazione ottenuta con le sequenze 3d triggerate ed il rapporto segnale / rumore mediamente pi elevato di tali sequenze rispetto alle frfse acquisite con tecnica breath - hold possono essere spiegati dalla modalit di riempimento del k - spazio , che nelle sequenze triggerate avviene alla fine dellespirazione , evitando artefatti da movimento che con tecnica breath - hold rischiano talvolta di inficiare la qualit delle immagini , vista la durata del tempo di apnea ( 2224 secondi )  . 
inoltre le frfse 3d triggerate con il respiro sono state acquisite con tempi tra i due ed i tre minuti e spessore sino a 2 mm circa , consentendo di rilevare un dettaglio anatomico di visualizzazione talvolta pi fine . riguardo le varianti biliari , le 3d hanno evidenziato capacit di visualizzazione superiori rispetto alle sequenze 2d ; le sequenze 2d thick slab nella nostra esperienza pur offrendo una buona panoramica bilio - pancreatica , non sempre permettono una facile e pronta identificazione delle varianti dei dotti biliari e del dotto cistico . 
la visualizzazione di tali varianti spesso dimostrata con il posizionamento di slab mirati durante lo svolgimento dellesame : la corretta disposizione di questi slab mirati talvolta operatore - dipendente , in quanto legata alla capacit del radiologo di identificare o sospettare nel corso dellesame una variante . 
linterpretazione di una variante anatomica con limpiego della tecnica 3d stata pi agevole , in quanto il volume del pacchetto di studio sufficientemente ampio a coprire tutto lalbero biliare ; il post - processing eseguito a conclusione dellesame svincola dalloperatore - dipendenza e dalla necessit di unimmediata lettura dellimmagine durante lo svolgimento dellesame . 
nella rielaborazione delle immagini lanatomia biliare e pancreatica acquisita nel volume 3d viene analizzata con piani di riformattazione multipli , in grado di dimostrare con esattezza le eventuali varianti , secondo piani di ricostruzione dedicati . 
necessario ricordare che le immagini native delle frfse 3d mantengono unelevata importanza nellidentificazione di eventuali alterazioni patologiche : le ricostruzioni mip , capaci di fornire una 482 radiol med ( 2010 ) 115 : 467482 biliary anatomy , can in fact hide the presence of calculosis or other disease . panoramica biliare chiara ed immediata , rischiano infatti di mascherare eventuali calcoli o patologie . conclusions conclusioni in conclusion , we can state that 3d frfse sequences ( breath - hold and respiratory - triggered ) present the same level of manageability as 2d ssfse sequences and are better able to visualise certain segments of the biliary tract compared with thick - section rapid acquisition with relaxation enhancement ( rare ) ssfse sequences , which at the end of the 1990s was the technique of choice for biliary tract imaging . 
in light of our findings , we suggest considering the use of 3d sequences in the biliopancreatic imaging study protocol alongside conventional 2d sequences . in conclusione , possiamo affermare che le sequenze 3d frfse ( breath - hold e respiratory triggered ) attualmente presentano la stessa maneggevolezza delle ssfse 2d , con capacit di visualizzazione a tratti superiori rispetto alle ssfse thick - section rapid acquisition with relaxation enhancement ( rare ) , sequenze che alla fine degli anni 90 si sono imposte come imaging di scelta biliare . 
the aim of this article is to describe the main technical principles of cad and cadx systems , their applicability and influence in clinical practice and new prospects for their future development . keywords lung nodules cad computed tomography riassunto i sistemi computed aided detection ( cad ) applicati alla tomografia computerizzata ( tc ) del torace , permettono lidentificazione automatica dei noduli polmonari , fornendo una seconda lettura al giudizio del radiologo e la valutazione volumetrica automatizzata delle lesioni , estremamente importante soprattutto in campo oncologico . la nuova frontiera nello sviluppo di questi sistemi rappresentata dallintroduzione dei sistemi cad di diagnosi ( computed aided diagnosis ) in grado non solo di effettuare lidentificazione dei noduli , ma anche una loro caratterizzazione , con lelaborazione di un indice della probabilit di malignit o benignit della lesione . 
lo scopo di questo articolo quello di esporre i principi tecnici generali che regolano il funzionamento dei sistemi cad , la loro applicabilit e influenza nella pratica clinica , e le nuove prospettive per il loro sviluppo nel panorama radiologico odierno in continua evoluzione . parole chiave noduli polmonari cad tomografia computerizzata introduction introduzione a pulmonary nodule ( pn ) is defined as a rounded or ovoid , at least moderately well - marginated , parenchymal lesion < 3 cm in diameter and of varying aetiology [ 1 , 2 ]  . 
detection of a pn is an extremely important event owing to the opportunity of diagnosing early stage and therefore potentially si definisce nodulo polmonare ( np ) una lesione parenchimale rotondeggiante od ovalare , a limiti netti o parzialmente netti , di dimensioni inferiori a 3 cm , a varia eziopatogenesi [ 1 , 2 ]  . 
la sua identificazione rappresenta un evento estremamente importante per la possibilit di effettuare diagnosi 386 radiol med ( 2010 ) 115 : 385402 curable cancers [ 3 , 4 ]  . 
the introduction of increasingly high - performance computed tomography ( ct ) scanners , while helping detect a larger number of pn [ 5 , 6 ] , has considerably increased the number of images to be reviewed by the radiologist , with the risk of missing some nodules , especially when they are small or in a central location [ 7 ]  . this has led to the development , since the 1990s , of automated systems for pn detection known as computer - aided detection ( cad ) systems . 
because it is widely reported that only 1% of pn < 5 mm represent malignancies , the general approach in clinical practice is to closely monitor the lesion over time to establish its nature [ 8 , 9 ]  . consequently , in recent years , research has focused on the development of new automated systems enabling not only pn detection but also characterisation at a very early stage of growth ( computer - aided diagnosis , or cadx )  . 
this review illustrates the technical principles and potential clinical applications of cad and cadx systems from their introduction up to the more recent applications . computer - aided detection of pulmonary nodules technical principles all cad systems rely on a discrimination mechanism based on densitometric grey - level thresholding [ 10 ]  . 
segmentation of thorax from the background in each section : in each section , a grey - level profile constructed along a diagonal extending from the upper corner to the centre of the image . 
segmentation of lungs within the thorax : a binary image is constructed in which pixels with a grey level greater than the selected threshold are turned on , and those with a lower level are turned off . 
selection of regions of interest ( roi ) with threshold values between 50 and 225 hu : in the segmented lung volumes , pixels ranging in value from 50 to 225 hu are automatically turned off and excluded from the analysis , so all structures that are nodule candidates are visualised . di neoplasie in stadi precoci e quindi potenzialmente curabili [ 3 , 4 ]  . 
lintroduzione di apparecchiature di tomografia computerizzata ( tc ) sempre pi performanti , se da un lato ha contribuito alla identificazione di un maggior numero di noduli [ 5 , 6 ] , dallaltro ha portato ad un notevole incremento del numero di immagini sottoposte alla valutazione del radiologo , con la possibilit di non identificare alcuni noduli , specie se di piccole dimensioni o localizzati in posizione centrale [ 7 ]  . 
dagli anni 90 sono quindi stati sviluppati sistemi automatici per la identificazione dei noduli polmonari , denominati computed aided detection ( cad )  . uno dei principali problemi riscontrato nellapplicazione clinica di questi sistemi lelevato numero di piccoli noduli identificati . 
molti studi hanno riportato infatti che solo l1% dei noduli di diametro < 5 mm identificati rappresenter realmente un tumore maligno e la pratica clinico - radiologica si pertanto indirizzata verso follow - up ravvicinati per una diagnosi di natura [ 8 , 9 ]  . 
 negli ultimi anni la ricerca stata quindi dedicata allo sviluppo di nuovi sistemi automatici non solo per la identificazione dei noduli , ma anche per la loro caratterizzazione in fasi di crescita ancora molto precoci . 
in questa revisione vengono riportati i principi tecnici e le potenziali applicazioni cliniche dei sistemi cad sia di identificazione che di diagnosi , dalla loro introduzione fino alle applicazioni cliniche pi recenti . i sistemi cad di identificazione dei noduli polmonari principi tecnici il funzionamento dei sistemi cad accomunato da un meccanismo di discriminazione basato su valori densitometrici soglia per le gradazioni di grigio [ 10 ]  . 
segmentazione dei polmoni allinterno del torace : viene costruita unimmagine binaria nella quale i pixel con valore superiore alla soglia prefissata vengono accesi ( on ) , mentre quelli con un valore inferiore vengono spenti ( off )  . 
immagini modificate da [ 10 ] , con autorizzazione . candidates : each pixel of interest ( on pixel ) is evaluated in relation to the ten pixels surrounding it in the three spatial planes , that is , the eight pixels bordering it in the same section and the two pixels located in the sections immediately above and immediately below the pixel of interest . 
selezione delle aree di interesse con valori soglia compresi tra 50 e 225 hu : sui volumi polmonari segmentati i pixel che posseggono valori minori di 50 o maggiori di 225 hu vengono automaticamente spenti e quindi eliminati dalla valutazione . 
reported a sensitivity of 94% and an average of 1.25 candidabili come noduli : ogni pixel di interesse ( non spento ) viene valutato in relazione ad altri 10 pixel circostanti nelle tre dimensioni dello spazio : gli 8 che lo circondano e i 2 situati rispettivamente nella sezione subito sottostante e subito soprastante . 
discriminazione con metodi automatici e identificazione dei noduli : per la riduzione del numero dei falsi positivi , le formazioni ricavate possono essere sottoposte ad ulteriori sistemi discriminativi : i metodi pi utilizzati sono quelli di discriminazione lineare ed i sistemi a reti neurali . 
 applicazioni cliniche i sistemi cad nella identificazione dei noduli polmonari numerosi studi hanno dimostrato che linserimento dei radiol med ( 2010 ) 115 : 385402 tabella 1 influenza dellintroduzione dei sistemi cad nellidentificazione dei noduli polmonari con i risultati riportati da 15 autori . 
despite their encouraging results , these systems could only be applied on thicksection imaging ( > 10 mm ) and a limited number of images . compared with earlier - generation scanners , spiral scanners produced a large number of thin - slice images for each ct study and , consequently , the detection of a greater number of lesions < 1 cthis led to widespread use of cad and increased research efforts to improve performance and clinical applicability . 
fin dallintroduzione delle apparecchiature tc di terza generazione , in grado di effettuare studi per la valutazione del torace con intervalli di ricostruzione sottili in tempi discretamente brevi , ci si resi conto dellelevato numero di noduli subcentimetrici identificati : di qui lattenzione per la ricerca e lo sviluppo dei primi prototipi di sistemi cad . 
 [ 17 ] in un piccolo studio effettuato su 8 pazienti ( totale di 48 noduli ) , riportarono risultati promettenti , con una sensibilit del 94% e una quota di falsi positivi di 1 , 25 per caso valutato [ 17 ]  . 
rispetto alle apparecchiature di precedente generazione , lintroduzione della tecnologia spirale ha condotto , per ogni singolo studio , alla produzione di un elevato numero di immagini con spessori di 390 radiol med ( 2010 ) 115 : 385402 fig . 
the spread of new - generation ct scanners capable of acquiring hundreds of images for each chest study with a substantial increase in the detection of nodules < 1 cm has made the issue of thin - section imaging particularly crucial . manufacturers are aligned with this trend and have increased the diagnostic power of cad to ensure detection of nodular structures < 5 mm , virtually eliminating falsenegative results , though with a higher rate of false positives . a number of studies have analysed the actual impact of cad by assessing radiologists performance when detecting nodules with and without the aid of cad [ 20 ]  . strato ridotti e ad un consequenziale incremento delle lesioni di diametro subcentimetrico evidenziate : si pertanto assistito ad una estesa diffusione dei sistemi cad ed ad un notevole aumento delle ricerche per migliorarne le performance e lapplicabilit clinica . 
compared the performance of three radiologists and cad in a ct study of 195 nodules 3 msensitivity values significantly increased with the use of cad ( mean 76% )  . 
even with three false - positive detections per scan , cad identified a greater number of nodules missed by the first reader than achieved by double reading [ 21 ]  . 
sensitivity values did not differ significantly between the two methods but were considerably improved with cad as the second reader , suggesting the possibility of using cad in low - dose ct studies in screening populations [ 22 ]  . advantages and limits of cad in daily radiological practice with more than 10 years of experience with automated detection systems , we are in a position to start analysing how cad fits into the complex scenario of clinical practice . 
to of true diagnostic assistance , cad must meet certain requirements : it must be integrated in or connected to the picture archiving and communication system ( pacs ) , it must have high levels of sensitivity and specificity and it must be fast and easy to use . 
although many ct manufacturers already integrate cad into the viewing workstation , its integration into the reporting workstation , with possible connection to image archiving systems , would be an important additional advantage . 
this problem , especially as regards the second group , may be easily addressed during the reporting stage , when the reader can quickly exclude false positives from the final evaluation . 
clinical practice is , however , still characterised by excessive caution in managing small nodules and a high number of reported abnormalities , with the patient being directed towards repeated examinations over time . finally , there should be integration with software allowing detection of small nodules with ground - glass appearance , the possibility of serial comparisons with volumetric calculations and the development of doubling indices quickly and intuitively . 
questo studio ha dimostrato la significativa diminuzione dei valori di sensibilit allaumentare dello spessore di strato e il loro incremento con la riduzione dellintervallo di ricostruzione [ 19 ]  . 
la diffusione di macchinari tc di ultima generazione , che permettono lacquisizione di centinaia di immagini per ogni singolo studio del torace con un sostanziale incremento dei noduli millimetrici identificati , ha reso centrale la questione del ridotto spessore di strato . 
le case produttrici si sono allineate a questa tendenza , incrementando le potenzialit diagnostiche dei sistemi cad , in grado di evidenziare strutture nodulari anche di diametro < 5 mm con una pressoch totale scomparsa dei falsi negativi , a fronte per di una elevata quota di falsi positivi . 
 [ 21 ] hanno posto in confronto le performance di tre radiologi e di un sistema cad in una valutazione con tc di 195 noduli del diametro minimo di 3 mi valori di sensibilit sono significativamente incrementati con lausilio del sistema cad ( valore medio 76% )  . 
anche se con un numero di falsi - positivi pari a 3 per scansione , il sistema cad stato in grado di identificare noduli non riconosciuti dal primo lettore in quota maggiore rispetto a quelli ottenuti attraverso una doppia lettura di due radiologi [ 21 ]  . 
recentemente altri autori hanno documentato il significativo vantaggio che deriverebbe dallinserimento dei sistemi cad nei programmi di screening , dimostrandone laccuratezza in particolare nella valutazione di noduli di piccole dimensioni e con lutilizzo di una ridotta dose di radiazioni . 
i valori di sensibilit non hanno riportato differenze statisticamente significative tra le due metodiche , ma sono notevolmente incrementati dall utilizzo del cad come secondo lettore , indicando pertanto la possibilit di effettuare studi a basso dosaggio cad - assistiti nei pazienti in screening [ 22 ]  . vantaggi e limiti del cad nella pratica radiologica quotidiana giunti ad oltre 10 anni di esperienza effettiva con i sistemi di identificazione automatica , siamo oggi in grado di iniziare a tracciare un bilancio che si inserisca nel complesso panorama della pratica clinica attuale . 
un sistema cad per essere di reale ausilio diagnostico deve soddisfare alcuni punti : essere inserito o collegato ad un picture archiving and 392 radiol med ( 2010 ) 115 : 385402 radiological follow - up to evaluate possible size changes over time by measuring the maximum diameter in the axial plane . the early lung cancer action project ( elcap ) guidelines for lung cancer screening recommends repeating the ct scan at 12 months if the lesion is < 2 mm , at 6 months if it is 5 mm , at 3 months if it is 8 mm and at 1 month if it is 10 mm [ 23 ]  . such intensive follow - up is , however , a significant source of stress and anxiety for patients and produces a very heavy workload for radiologists . 
this issue is especially serious considering that : ( 1 ) the number of detected nodules is growing with the spread of new equipment , ( 2 ) the extremely low doubling times of small lesions implies a need to repeat the follow - up scans at very long intervals and ( 3 ) the high intraand interobserver variability when reviewing pn on subsequent scans . 
additionally , considering lesions < 1 cm , even with accurate measurements at the workstation ( with automated size determination ) , the diameter in the axial plane may not represent the longest diameter and accuracy of the measurement may not be satisfactory on a millimetre scale . 
subsequent developments in the clinical application of cad led to the incorporation into a single software system of a function for automated detection and a function for three - dimensional measurement , with the possibility of viewing the baseline and follow - up scans with their respective volume measurements on a double monitor . 
in 14 out of 50 patients , nonvolumetric measurements were significantly discordant : some nodules were judged as being in remission by some observers and as progressive disease by others . 
the principal factors are variations in slice thickness , the use of different reconstruction algorithms , variations in tube current and different respiratory phases of the patient during the scan . 
thus , there is a need to standardise the radiological examination to ensure accurate comparisons , objective and consistent judgements of response to treatment and the possible characterisation of lesions based on even minimal volume changes on follow - up scans [ 29 , 30 ]  . communication system ( pacs ) ; avere elevati livelli di sensibilit e specificit ; essere di utilizzo rapido ed intuitivo . molte case produttrici di apparecchiature tc gi forniscono sistemi cad integrati nelle consolle di visualizzazione delle immagini , ma il loro inserimento anche nelle consolle di refertazione possibilmente interconnesse ai sistemi di archiviazione delle immagini rappresenterebbe un ulteriore considerevole vantaggio . 
tale problema , in particolare per il secondo gruppo , pu essere per routinariamente gestito con facilit nella refertazione , in cui losservatore pu scartare rapidamente i fp eliminandoli dalla valutazione finale . 
permane tuttavia nella pratica clinica un eccessivo prudenzialismo nella gestione dei noduli di piccole dimensioni identificati e dellelevato numero di altre alterazioni parenchimali segnalate , indirizzando il paziente verso la ripetizione di controlli nel tempo . 
infine necessaria lintegrazione con un software di analisi che consenta anche lidentificazione di noduli di piccole dimensioni con aspetto a vetro smerigliato , la possibilit di effettuare confronti nel tempo con calcoli volumetrici e lelaborazione di indici di raddoppiamento in modo rapido ed intuitivo . 
 i sistemi cad nel follow - up dei noduli e delle metastasi la gestione dei noduli polmonari di diametro < 1 cm problematica a causa della difficolt di caratterizzazione di lesioni cos piccole . 
le linee guida delineate dallearly lung cancer action project ( elcap ) per lo screening del cancro del polmone , indicano la necessit di ripetere lesame tc in follow - up a 12 mesi se la lesione < 2 mm , a 6 mesi se di 5 mm , a 3 mesi se di 8 mm e ad un mese se di 10 mm [ 23 ]  . controlli cos ravvicinati rappresentano per una significativa fonte di stress ed ansia per il paziente e conducono ad una mole di lavoro estremamente ampia per il radiologo . 
3a , b cad system and follow - up : the same nodule is evaluated in two subsequent examinations , with system providing an automated assessment of bidimensional and volumetric modifications and percentage of volumetric variation . 
3a , b sistema cad e follow - up : lo stesso nodulo viene valutato in due studi successivi ; vengono fornite automaticamente le modificazioni dimensionali nelle due e tre dimensioni e la percentuale di variazione volumetrica . a valutazione in follow - up di un nodulo aumentato nelle dimensioni in due studi successivi . 
b valutazione di un nodulo diminuito nelle dimensioni in due studi successivi . new algorithms and characterisation systems background with the development and dissemination of cad in pn detection , radiologists were faced with an increasingly large number of images and lesions ( especially small lesions ) to review . 
considerando infatti lesioni millimetriche , anche con accurate misurazioni su consolle ( che permettono una misurazione automatica del calibro ) , la misurazione sul piano assiale pone levidente limite della scelta del piano dove pu essere osservato il maggior diametro , oltre che unaccuratezza di misurazione non sempre soddisfacente in scala millimetrica . 
levoluzione successiva nellapplicazione clinica dei sistemi cad ha portato 394 radiol med ( 2010 ) 115 : 385402 table 2 cad systems in the characterization of lung nodules ( cadx )  . 
for each study are reported : author and year of publication ; number of nodules evaluated ( benign and malign ) ; method of evaluation and overall performance level author year database ( nodules ) evaluation method performance level ayoama et al . 2002 mcnitt - gray et al . 
 ( 3 ) the system provides a probability estimate of nodule malignancy or benignity , which is combined with the radiologists final judgement to arrive at the diagnosis [ 3133 ]  . 
 ( 2 ) study of nodule vascularity and enhancement patterns after administration of intravenous contrast mediu ( 3 ) use of ann . statistical processing based on nodule morphology and the patients clinical history some automated systems discriminate malignant from benign lesions by statistically evaluating the presence and repetition of previously extracted features / parameters . these parameters originate from a combination of predefined data derived from both the imaging features of the allintegrazione in uno stesso software della funzione automatica di identificazione e quella di misurazione volumetrica delle lesioni , con possibilit di avere su un doppio monitor lo studio basale e di follow - up , con i rispettivi volumi . 
 [ 26 ] hanno dimostrato la superiorit delle valutazioni volumetriche effettuate con un sistema automatico cad rispetto alla tradizionale misurazione manuale uni o bi - dimensionale su un campione di 50 pazienti in follow - up per metastasi polmonari ( totale di 202 noduli )  . 
in 14 su 50 pazienti le misurazioni non volumetriche sono risultate discordanti in maniera statisticamente significativa : alcuni noduli erano giudicati in remissione da alcuni osservatori ed in progressione da altri . 
come dimostrato da diversi radiol med ( 2010 ) 115 : 385402 autori , alcuni fattori tecnici ed altri legati al paziente , possono per influenzare la misurazione volumetrica delle lesioni in studi successivi . 
i principali fattori coinvolti sono i seguenti : la variazione dello spessore di strato , lutilizzo di differenti algoritmi di ricostruzione , le modificazioni della corrente del tubo , nonch la diversa fase respiratoria del paziente durante lesecuzione dello studio . 
4 segmentazione di un nodulo maligno : delimitazione della sua area e definizione dellaarea esterna di 5 mmodificata da [ 34 ] con autorizzazione . introduzione nuovi algoritmi e sistemi di caratterizzazione nodule ( shape , size , density ) and the patients clinical history , allowing the radiologist to judge the likelihood of malignancy or benignity [ 34 , 35 ]  . 
5 two histograms based on grey levels of the inside and outside regions of a malignant and a benign nodule : correlation between the hounsfield values in the two regions and the corresponding fraction of pixels . 
5 due istogrammi basati sui livelli di grigio dellarea interna ed esterna di un nodulo maligno e di un nodulo benigno : relazione tra valori hu riscontrati e la frazione di pixel corrispondenti . 
the final differentiation process ( done by statistical linear discriminant analysis ) was based on a group of significant discriminants derived from : ( a ) effective lesion diameter , ( b ) attenuation of inside and outside regions , ( c ) overlap measure of the two grey - level histograms for the inside and outside regions and ( d ) clinical information ( sex , age ) [ 34 ]  . 
 [ 35 ] developed a differentiation scheme ( tested on 19 malignant and 16 benign nodules ) that also includes evaluation of the contrast - enhancement pattern and information on the surrounding ground - glass - like component . the scheme may be summarised as follows : ( 1 ) ct acquisition and automated segmentation of nodules and ( 2 ) extraction of 31 features ( based on shape , surrounding groundglass - like component and enhancement due to contrast injection ) that , applied to each nodule , allows differentiation of benign and malignant nodules through computerised statistical analysis . 
the reported level of performance was equal to az = 0.92. automated study of nodule vascularity angiogenesis has a fundamental role in both growth and metastasis of lung cancer , with many studies showing that early and intense vascular growth is correlated with a worse prognosis [ 36 , 39 ]  . 
studied 35 malignant and 27 benign nodules using an automated computer - aided discrimination system whereby each nodular lesion is studied three times : before contrast - medium administration and 2 and 4 min after contrast - medium injection . 
nodule density features ( studied volumetrically ) are evaluated using three parameters : ( 1 ) nodule attenuation during the three study phases , ( 2 ) shape ( shape index , ranging from 0 to 1 ) and ( 3 ) curvedness ( ranging from 0 to 1 )  . 
shape index and curvedness values are defined by the three - dimensional curved surface : in three - dimensional reconstruction , as the shape index approaches 0 , convex surfaces predominate , and as the index approaches 1 , flat or depressed surfaces predominate ; as the curvedness value approaches 0 , the surface appears flatter and consequently has a greater degree of regularity . 
 i sistemi cad di diagnosi proposti nel corso del tempo si sono sviluppati su diversi binari di ricerca , in cui sono state sfruttate le pi avanzate conoscenze sui caratteri anatomopatologici e funzionali delle lesioni tumorali polmonari ( tabella 2 )  . 
i principi di discriminazione utilizzati possono essere cos elencati : ( 1 ) processazione con analisi statistiche basate sui caratteri dellimmagine dei noduli e sulla storia clinica del paziente ; ( 2 ) studio della vascolarizzazione dei noduli e del loro comportamento contrastografico dopo iniezione endovenosa di mezzo di contrasto ; ( 3 ) utilizzo di reti neurali artificiali . processazione con analisi statistiche basate sui caratteri dellimmagine dei noduli e la storia clinica del paziente alcuni sistemi automatici effettuano una analisi discriminativa delle lesioni in studio attraverso una valutazione statistica computerizzata basata sulla presenza e ripetizione di determinati caratteri / parametri preliminarmente ricavati . questi parametri nascono da una combinazione di informazioni pre - impostate derivate sia dalle caratteristiche intrinseche dellimmagine del nodulo ( forma , dimensioni , densit ) che dalla storia clinica dei pazienti , fornendo in pochi istanti al radiologo un giudizio di probabilit di malignit o benignit [ 34 , 35 ]  . 
 [ 34 ] e si basa sulla processazione delle immagini bidimensionali delle lesioni . sono state studiate 74 lesioni maligne e 413 benigne , derivate da un programma di screening per il tumore del polmone . 
questo sistema , nonostante gli ottimi livelli di prestazioni ( az = 0 , 86 ) , possiede tuttavia il limite di non includere alcune caratteristiche del nodulo come ad esempio aree a vetro smerigliato ( ggo ) e di effettuare lanalisi unicamente sulle immagini 2d . 
potendo considerare lo studio tc con mezzo di contrasto come misura del grado di neo - vascolarizzazione intra - lesionale del tumore del polmone , mori et al . [ 38 ] hanno applicato questa tecnica ad una popolazione di noduli ( 35 maligni e 27 benigni ) , utilizzando un sistema di discriminazione automatica computerizzata in cui ogni lesione nodulare viene studiata per 3 volte : prima senza mezzo di contrasto , e poi dopo 2 e 4 minuti dalla somministrazione . dopo un processo di segmentazione automatica delle immagini , ogni nodulo viene ricostruito in tre dimensioni . 
gli ultimi due sono definiti dal grado di curvatura e dalla regolarit della superficie della lesione : nella ricostruzione tridimensionale del nodulo , quando lo shape index prossimo allo 0 prevalgono aree convesse , quando invece prossimo ad 1 sono maggiormente rappresentate zone piane o depresse ; se il valore di curvedness pi vicino allo 0 la superficie si presenta pi piana , e quindi maggiore sar il suo grado di regolarit . 
con ladozione di questo sistema i valori pi alti di sensibilit si sono ottenuti operando una combinazione dei tre parametri in esame [ 38 ]  . utilizzo di reti neurali artificiali numerosi studi per la differenziazione dei noduli polmonari fig . 
analysis of the relationship between grey levels in the nodule and surrounding area reveals a larger dispersion and variability in the malignant nodule ( which appears poorly defined on both shape - index and curvedness reconstructions ) ; the benign nodule appears well - delimited from the surrounding area , with a more regular grey - level distribution . 
nellanalisi dei rapporti della distribuzione dei grigi tra il nodulo e larea circostante , si assiste ad una maggiore dispersione e variabilit nel caso del nodulo maligno ( che appare mal definito sia nella ricostruzione shape index che curvedness ) mentre appare ben delineato rispetto alla periferia il nodulo benigno , con una distribuzione dei grigi pi uniforme . 
i 12 neuroni che costituiscono questo sistema sono in grado di effettuare una classificazione in base a dati acquisiti durante la fase di training ( attuata con lutilizzo di 140 modelli esplicativi ) ricavati da diversi caratteri delle immagini dei noduli e dallo stato clinico del paziente : diametro della lesione , valori di attenuazione , presenza di spiculazioni , caratteri dei margini , presenza di halo - sign , et , sesso , storia di emissione di espettorato ematico . 
 studi pi recenti sulla adozione dei sistemi a matrici neurali hanno permesso di applicare questi complessi algoritmi matematici non solo alle relazioni esistenti tra i caratteri dellimmagine e le informazioni cliniche del paziente , ma direttamente allimmagine stessa , modulando le interconnessioni esistenti tra i diversi pixels . 
locchio umano infatti in grado di differenziare solo 16 tonalit di grigio : una vastissima mole di informazioni che potrebbero essere estremamente utili nella formulazione di una diagnosi differenziale delle lesioni nodulari polmonari e contenute nella immagine tc , vengono perdute nella pratica radiologica quotidiana . 
 sin dalle prime fasi di crescita tumorale , i processi inflitrativi a livello del tessuto sano circostante da parte delle cellule neoplastiche , sono accompagnati dai fisiologici meccanismi della difesa immunitaria e dellinfiammazione , con richiamo di cellule , vasodilatazione , edema e danno tissutale . 
questi fenomeni portano a delle modificazioni nella distribuzione dei livelli di grigi nellimmagine tc estremamente fini ( il cosiddetto halo sign ) , e non sufficientemente marcate da poter essere colte in una semplice output fig . 
7 schematizzazione di una valutazione effettuata da una rete neurale : dopo il processo di training loggetto in studio viene sottoposto allanalisi dei diversi neuroni che costituiscono la rete ; al termine della valutazione viene fornito un output con la misura della probabilit di benignit o malignit della lesione . 
the 12 neurons making up this system perform a classification based on the information acquired from the training sample set ( 140 models ) and relating to the imaging features of the nodules and the patients clinical status : lesion diameter , attenuation values , presence of spiculations , contours , halo sign , age , sex and history of bloody spututhe systems output is a range of values from 0 to 1 , indicators of the probability of malignancy . 
 more recent studies on the adoption of neural matrix systems have enabled these complex mathematical algorithms to be applied not only to relations between imaging features and clinical data but directly to the image itself by modulating the interconnections between the different pixels . 
the human eye is able to discern only 16 different tones of grey : this means that a huge amount of information that could be useful in differentiating pn and contained in the ct image is lost in daily practice . 
8 differenti processazioni con sistema acm per lesaltazione delle modificazioni alla periferia del nodulo . from the earliest stages of tumour growth , infiltration of healthy surrounding tissue by neoplastic cells is accompanied by physiological defence mechanisms and inflammation , with infiltration of immune cells , vasodilatation , oedema and tissue damage . 
these processes are reflected in changes in the distribution of grey levels on the ct image ( halo sign ) that are , however , too subtle to be appreciated on plain visual inspection . 
at the end of each processing cycle , an output image ( called by the system ) is generated , which contains a more or less marked and early modification of the nodule outline in the source image [ 45 ]  . preliminary studies in a sample of 25 patients ( 13 malignant and 12 benign nodules ) showed significant differences analisi ad occhio nudo . 
ad ogni pixel costituente limmagine tc viene assegnato uno specifico valore ( direttamente correlato al suo livello di grigio ) e questo viene poi inserito nel sistema matrice , una sorta di rete in cui ogni pixel collegato ai pixel circostanti e attraverso questi anche ai pixel pi distanti ; il valore di questi legami pu essere pi o meno forte , in base alla similitudine riscontrata tra i livelli di grigio di ogni singolo pixel . 
a questo punto il sistema evolve secondo un numero preimpostato di cicli elaborativi : durante ciascun ciclo vengono rielaborati i valori di tutti i pixel in base alla forza delle loro connessioni con i pixel circostanti ; al termine di ogni ciclo di elaborazione viene prodotta una immagine output ( denominata dal sistema ) che riporta una modificazione pi o meno marcata e precoce dei margini del nodulo dellimmagine originaria [ 45 ]  . 
studi preliminari su un totale di 25 pazienti ( 13 noduli maligni e 12 benigni ) , hanno riportato differenze significative tra le immagini output prodotte dal sistema : i margini dei noduli maligni presentavano modificazioni notevolmente pi pronunciate e soprattutto pi precoci rispetto a quelle dei noduli benigni , i cui limiti apparivano conservati , con limitate variazioni solo nelle fasi pi tardive di 400 radiol med ( 2010 ) 115 : 385402 fig . 
although these early evaluations were very encouraging , further studies are needed to assess the effectiveness of this system and its clinical applicability . conclusions cad systems represent a fundamental aid in radiological practice . 
the automated characterisation of these lesions is thus the new challenge in radiological research , and the first results appear very encouraging . further studies are needed to refine these systems , but given their tremendous potential , it is highly likely that in the very near future , cad and cadx systems will be introduced into routine radiological practice with into reporting systems and used as a second reader . 
queste prime valutazioni si sono dimostrate molto incoraggianti , ma sono necessari ulteriori studi per valutare leffettiva efficacia di questo sistema e la sua applicabilit clinica . conclusioni i sistemi cad rappresentano oggi un ausilio di fondamentale rilevanza nella pratica radiologica : il loro inserimento nei sistemi di refertazione migliora significativamente le performance degli operatori nel corretto riconoscimento dei noduli polmonari anche di piccolo diametro , permettendo una identificazione in stadi pi precoci di crescita di lesioni potenzialmente maligne . 
sono ancora necessari ulteriori studi e ricerche per il perfezionamento di questi sistemi , ma date le loro grandi potenzialit facile immaginare un inserimento dei sistemi cad di identificazione e diagnosi nella pratica radiologica quotidiana in un futuro molto prossimo , con la loro integrazione nei sistemi di refertazione ed impiego come secondo lettore . 
sartor springer - verlag , berlin , heidelberg , 2009 isbn 978 - 3 - 540 - 34618 - 0 in this fascinating book , the authors discuss and describe the possible contribution of magnetic resonance imaging ( mri ) to the field of lung diagnostic radiology . 
due to problems inherent to the use of this sophisticated instrument the reader will find a robust portion of the text discussing technical details and possible contributions towards improvements according to the latest discoveries . 
hyperpolarized gases use in mri pulmonary ventilation is discussed in depth highlighting their potential in diagnosis as well as their limitations due either to high costs or difficulties in their handling . following the five long technical chapters ( 103 - pages ) the reader is introduced to the clinical diagnostic use of mri . 
this part of the book is discussed and presented in 10 chapters ( pulmonary hypertension and thromboembolic disease ; vascular anomalies and diseases ; asthma ; cystic fibrosis ; lung cancer ; mediastinal disease ; pulmonary infections pneumonia ; interstitial lung disease ; disease of the pleura and the chest wall ) presenting how , where and when mri of the lung will produce the best results . 
in this respect , an in depth discussion is presented in order to help the reader understand how to properly employ one or the other instrument when both are available . 
surely radiologists and clinicians should keep in their mind the radiation dose that the patient is exposed to by mdct , while mri is the perfect war - horse in follow - up and monitoring of chronic diseases , such as cystic fibrosis or chronic obstructive lung diseases avoiding unnecessary radiation burden in these patients . furthermore , all benefits offered by functional mri imaging , coupled with its ability to visualize changes in lung structure enhance mri diagnostic horizons . 
a causa delle problematiche insite nelluso di questo delicato strumento diagnostico , il lettore trover una significativa parte del testo dedicata alla discussione dei dettagli tecnici e dei possibili contributi al loro miglioramento nellutilizzo pratico , in funzione dei ritrovamenti e delle scoperte pi recenti . viene cos descritta in dettaglio la ventilazione polmonare rm mediante luso dei gas iperpolarizzati , dimostrandone tutte le potenzialit diagnostiche ma anche le limitazioni dovute o al costo o alle difficolt pratiche nellutilizzo di queste sostanze . 
in 10 capitoli ( dal titolo : pulmonary hypertension and thromboembolic disease ; vascular anomalies and diseases ; asthma ; cystic fibrosis ; lung cancer ; mediastinal disease ; pulmonary infections pneumonia ; interstitial lung disease ; disease of the pleura and the chest wall ) viene infatti discusso e presentato come , dove e quando la rm del polmone produrr i migliori risultati . oltre ai problemi tecnici la rm del polmone ha un grande nemico : tomografia computerizzata multidetettore ( tcmd )  . 
da questo punto di vista parecchi argomenti di discussione vengono affrontati in modo tale da far capire al radiologo ed al clinico come utilizzare e nel migliore dei modi luna o laltra metodica nel caso di averle entrambe a disposizione . 
di sicuro bisogna tener ben presente la dose radiante al paziente da parte della tcmd , mentre la rm pu essere considerata il perfetto cavallo da battaglia nei controlli a distanza e nel monitoraggio di malattie croniche tipo la fibrosi cistica o le malattie ostruttive croniche polmonari , evitando cos un inutile carico di radiazioni ai pazienti che ne sono affetti . 
 infatti tutti i vantaggi offerti dalla rm funzionale , associati alla capacit della rm di mettere in evidenza possibili alterazione della struttura dei polmoni , ampliano significativamente lorizzonte delle possibilit diagnostiche della rm . 
nei vari capitoli del volume sono ritrovabili protocolli che 504 radiol med ( 2010 ) 115 : 503504 out the book one will find protocols to utilize and very impressive images of the obtained results . as clearly stated by baert in his foreword to the book it is : highly recommendable to radiologists ( certified and in training ) , pneumologists and chest surgeons , a sentiment i completely agree with . rendono facile lesecuzione delle indagini ed immagini molto belle dei risultati da esse ottenibili . come scritto a chiare lettere dal prof . 
baert nella sua prefazione al volume , questo libro altamente raccomandabile ai radiologi , siano essi in formazione o gi strutturati , agli pneumologi ed ai chirurghi toracici , affermazione cui mi associo in pieno . 
ct coronary angiography for the diagnosis of coronary artery disease : a real - world experience stress - ecg vs coronarografia tc nella diagnostica della malattia coronarica : esperienza nel mondo reale e . 
cademartiri1 , 2 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria di parma , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands correspondence to : f . 
cademartiri , dipartimento di radiologia e diagnostica per immagini , azienda ospedaliero - universitaria di parma , c / o piastra tecnica , piano 0 , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703516 , fax : + 39 - 052 - 1704838 , e - mail : filippocademartiri@hotmail.com received : 4 march 2009 / accepted : 3 april 2009 / published online : 9 november 2009 springer - verlag 2009 abstract purpose . 
a total of 236 consecutive patients ( 159 men , 77 women ; mean age 62.810.2 years ) at moderate risk and with suspected coronary artery disease ( cad ) were enrolled in the study and underwent stress ecg , ctca and ca . 
the prevalence of disease demonstrated at ca was 62% ( n = 220 ) , 51% in the population with comparable stress ecg and ctca ( n = 147 ) and 84% in the population with equivocal stress ecg ( n = 73 )  . 
scopo del presente lavoro stato valutare laccuratezza diagnostica dellelettrocardiogramma sotto stress ( stress - ecg ) e dellangiografia coronarica con tomografia computerizzata ( ct - ca ) nellindividuazione delle stenosi coronariche significative ( riduzione del lume coronarico 50% ) vs langiografia coronaria convenzionale ( cag ) basando la valutazione sulla refertazione clinica . 
duecentotrentasei pazienti consecutivi ( 159 maschi , 77 femmine , et media 62 , 810 , 2 anni ) a rischio intermedio con sospetta malattia coronarica sono stati arruolati per lo studio e sottoposti a stress - ecg , ct - ca e cag . 
la prevalenza di malattia risultata del 62% nella popolazione complessiva ( n = 220 ) , del 51% nella popolazione con stress - ecg e ct - ca confrontabili ( n = 147 ) , e dell84% nella popolazione con stress - ecg dubbio ( n = 73 )  . 
settantatre ( 33 , 2% ) stress - ecg sono stati classificati come dubbi , 69 ( 31 , 4% ) sono stati classificati radiol med ( 2010 ) 115 : 354367 ( ppv ) 51% and negative predictive value ( npv ) 49% . 
ctca in the real world has significantly higher diagnostic accuracy compared with stress ecg and could be used as a first - line study in patients at moderate risk . keywords computed tomography coronary angiography stress ecg exercise ecg conventional coronary angiography coronary artery disease come positivi e 78 ( 35 , 5% ) sono stati classificati come negativi . 
quaranta ( 27 , 2% ) pazienti sono stati erroneamente classificati come negativi . trentaquattro ( 23 , 1% ) pazienti che non avevano stenosi significative sono stati incorrettamente classificati come positivi . 
i valori dellaccuratezza diagnostica della ct - ca sono risultati : sensibilit 96% , specificit 65% , valore predittivo positivo 74% , valore predittivo negativo 94% . tre ( 2% ) pazienti sono stati erroneamente classificati come negativi . 
 parole chiave angiografia coronarica con tomografia computerizzata ecg sotto stress test ergometrico coronarografia convenzionale malattia coronarica introduction introduzione computed tomography coronary angiography ( ctca ) is increasingly gaining acceptance for the diagnosis of coronary artery disease ( cad ) in clinical practice [ 16 ]  . 
the studies that have demonstrated the diagnostic accuracy of 64 - slice ctca have used methods suitable for validating the technique , but little research has been done on its real effectiveness in the clinical setting . 
in particular , no study has performed clinical comparisons with other diagnostic techniques , with the exception of conventional coronary angiography ( ca ) used as the standard of reference . 
this is a very common and relatively cheap test that provides functional information on inducible ischaemia . the current recommendations , guidelines and international panels suggest the use of ctca in patient populations at low to moderate risk , with equivocal stress test or unable to exercise [ 8 ]  . 
in cardiological practice , especially in europe , stress ecg is regarded as the first - line functional test in the diagnostic algorith however , this technique suffers a number of well - known limitations , including a progressive loss of sensitivity and specificity as the pretest probability of disease decreases [ 7 ]  . this study aimed to assess the diagnostic performance of langiografia coronarica mediante tomografia computerizzata ( ct - ca ) sta progressivamente entrando nella pratica clinica per la diagnosi di malattia coronarica ostruttiva [ 16 ]  . 
in particolare , pochi studi si sono focalizzati sul confronto clinico con altre metodiche diagnostiche , ad eccezione della coronarografia convenzionale ( cag ) utilizzata di routine come standard di riferimento . 
tra queste quella di maggiore diffusione il test da sforzo ( test ergometrico o prova da sforzo o elettrocardiogramma sotto stress [ stress - ecg ] ) [ 7 ]  . 
le attuali raccomandazioni , linee guida ed i panel internazionali raccomandano lutilizzo della ct - ca in popolazioni di pazienti a rischio basso - intermedio con test provocativi dubbi o non eseguibili [ 8 ]  . 
tuttavia , sono ben noti i limiti di questa metodica e soprattutto la progressiva perdita di sensibilit e 356 radiol med ( 2010 ) 115 : 354367 ctca in comparison with ca in the detection of cad by comparing the clinical reports of the two techniques in a hospital where ctca is routinely implemented . materials and methods study population from january 2006 to june 2007 , 236 consecutive patients with suspected cad ( stable angina , atypical chest pain and silent ischaemia ) who had undergone stress ecg , ctca and ca were retrospectively enrolled in the study ( table 1 )  . 
the ethics committee of our centre approved the study protocol , and all patients gave informed consent . patient preparation patients with a heart rate ( hr ) > 60 beats per minute ( bpm ) and without specific contraindications received a 5 - mg ( repeatable ) intravenous dose of beta blockers ( atenolol , tenormin , astrazeneca , germany )  . 
in addition , in the absence of contraindications , patients received a 5 - mg sublingual dose of nitrate ( dinitrate isosorbide , carvasin , wyeth lederle , italy ) a few minutes prior to the scan . 
the parameters used for the calcium quantification ( a ) and coronary angiography ( b ) scans were : ( a ) number of slices per rotation 322 , gantry rotation time 330 ms , feed / rotation 6 mm ( pitch 0.2 ) , tube voltage kv 120 and tube current mas 150 . 
the images were reconstructed with the following parameters : effective slice thickness 3 mm , reconstruction increment 1.5 mm , field of view ( fov ) 150180 mm , and convolution kernel for the calcium score . 
the time windows were positioned at 350 ms of the subsequent r wave . ( b ) number of slices per rotation 322 , slice thickness 0.6 mm , rotation time 330 ms , feed / rotation 3.84 mm ( pitch 0.2 ) , tube voltage 120 kv , tube current 850950 specificit al diminuire della probabilit pre - test di malattia [ 7 ]  . questo studio volto a confrontare la performance diagnostica della ct - ca rispetto alla cag nella rilevazione di stenosi coronariche confrontando i referti clinici delle due metodiche in un ospedale dove questa metodica gi stata implementata . materiali e metodi popolazione esaminata da gennaio 2006 a giugno 2007 , 236 pazienti consecutivi con sospetta malattia coronarica ( angina stabile , dolore toracico atipico e ischemia silente ) che hanno eseguito stress - ecg , ct - ca e cag sono stati retrospettivamente arruolati per lo studio ( tabella 1 )  . 
i pazienti con sindrome coronarica acuta e quelli nei quali esistevano delle controindicazioni assolute alla somministrazione endovenosa di mezzo di contrasto iodato ( allergia nota , insufficienza renale o disordini tiroidei ) sono stati esclusi dallo studio . 
il comitato etico della nostra istituzione ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . preparazione del paziente ai pazienti con una frequenza cardiaca ( fc ) superiore a 60 battiti per minuto ( bpm ) e senza controindicazioni stata somministrato per via endovenosa del beta - bloccante ( atenololo , tenormin , astrazeneca , germania ; 5 mg ripetibile )  . 
inoltre , in assenza di contro indicazioni , pochi minuti prima della scansione stato somministrato del nitrato sublinguale ( isosorbide dinitrato , carvasin 5 mg , wyeth lederle , italia )  . 
 protocollo di scansione ct - ca e ricostruzione delle immagini per lo studio mediante tc stato utilizzato uno scanner a 64 strati ( sensation 64 , siemens , forchheim , germania )  . tutti i pazienti sono stati sottoposti ad acquisizione diretta per la quantificazione del calcio coronarico e ad acquisizione angiografica con somministrazione endovenosa di mezzo di contrasto iodato . 
prospective modulation of the x - ray tube was not used . ( pitch 0 , 2 ) , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 150 mas . 
le immagini sono state ricostruite con i seguenti parametri : spessore di strato effettivo 3 mm , incremento di ricostruzione 1 , 5 mm , campo di vista ( fov ) 150180 mm , filtro di convoluzione dedicato per il calcium score . 
le finestre temporali sono state posizionate a - 350 ms della successiva onda r ; ( b ) numero di strati per rotazione 322 , spessore di strato 0 , 6 mm , tempo di rotazione 330 ms , avanzamento per rotazione 3 , 84 mm ( pitch 0 , 2 ) , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 850950 mas , spessore di strato effettivo ricostruito 0 , 60 , 75 mm , incremento di ricostruzione 0 , 4 mm , fov 150180 mm , filtro di convoluzione medium - smooth . 
 utilizzando un software dedicato ( windose , istituto di fisica medica , erlangen , germania ) stata calcolata la dose di radiazioni ionizzanti alla quale i pazienti sono stati esposti durante la scansione angiografica ( 15 , 2 msv per le donne e 21 , 4 msv per gli uomini )  . 
la tecnologia con doppia macchia focale oscillante sullasse z ( flying focal spot ) permette di sovra - campionare due volte per ogni posizione angolare del tubo radiogeno le 32 file di detettori dello spessore minimo di 0 , 6 mquesta geometria di scansione consente di ottenere unimmagine con voxel isotropico di 0 , 4 mm3 . 
sono stati somministrati 80100 ml di mezzo di contrasto iodato ( iomeprol , iomeron 400 , bracco , milano , italia ) alla velocit di 45 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 1820 gauge preventivamente posizionata in una vena antecubitale . allo scopo di ottimizzare lopacizzazione dei vasi arteriosi coronarici stata utilizzata la tecnica del bolustracking ( care bolus , siemens , forchheim , germania ) per sincronizzare larrivo del mezzo di contrasto nelle arterie coronarie con linizio della scansione . 
le finestre temporali utilizzate sono state la fase mesoe telediastolica ( da - 300 a 450 ms prima della successiva onda r e / o dal 60% al 70% dellintervallo r - r )  . 
quando ritenuto necessario ( per esempio in caso di persistente movimento cardiaco residuo che riduce la qualit diagnostica dellimmagine ) sono state analizzate altre ricostruzioni in differenti finestre temporali di ricostruzioni del ciclo cardiaco , generalmente dal 25% al 35% dellintervallo r - r ( oppure + 225 ms , + 275 ms , e + 325 ms dopo la precedente onda r )  . 
 358 radiol med ( 2010 ) 115 : 354367 a dedicated software package ( windose , medical physics institute , erlangen , germany ) was used to calculate radiation dose to patients during the angiographic scan ( 15.2 msv for women and 21.4 msv for men )  . 
the time windows used were the midand end - diastolic phases ( from 300 to 450 ms before the subsequent r wave and / or from 60% to 70% of the r - r interval )  . 
the reconstruction algorithm records data from a single heartbeat obtained during half a gantry rotation . stress ecg stress ecg was performed using a bicycle ergometer and a protocol involving an initial 25 w workload followed by 25 w increments every 2 min [ 9 ]  . 
stress ecg was classified as positive in the presence of horizontal or down - sloping st segment depression 1 mm or greater , 80 ms after the j - point . 
negative stress ecg in patients who had not achieved peak exercise capacity considered normal for age , sex and weight was classified as equivocal . conventional coronary angiography stress - ecg lo stress - ecg stato eseguito utilizzando un cicloergometro ed un protocollo con 25 w iniziali , seguiti da incrementi di 25 w ogni 2 minuti [ 9 ]  . 
lo stress - ecg stato classificato positivo in presenza di un sotto - slivellamento ( orizzontale o discendente ) del tratto st di almeno 1 mm 80 ms dopo il punto j . 
loperatore era a conoscenza dei dati derivanti dal referto e dalle immagini relative alla ctca essendo le procedure effettuate in contesto clinico . loperatore ha identificato i segmenti coronarici utilizzando una classificazione in 17 segmenti modificata da quella fornita dallamerican heart association [ 10 ]  . 
i segmenti sono stati classificati come non significativamente stenotici ( normali o con irregolarit della parete o con stenosi non critica < 70% ) o significativamente stenotici ( stenosi critica 70% ) , utilizzando le classificazioni convenzionali e linee guida . 
le stenosi coronariche sono state valutate dalloperatore durante la seduta angiografica nella proiezione di massima stenosi mediante valutazione visiva . valutazione dellimmagine di ct - ca tutte le ct - ca sono state analizzate da un osservatore con 5 anni di esperienza nel settore non a conoscenza dei risultati della cag . 
i segmenti sono stati classificati come non significativamente stenotici ( normali o con irregolarit della parete o con stenosi non critica < 50% ) o significativamente stenotici ( stenosi critica 50% ) , utilizzando le classificazioni comunemente applicate . ca was performed 2 weeks after ctca with a conventional technique . 
the operator identified coronary segments using a 17 - segment analisi statistica le variabili continue sono state espresse come medie pi o radiol med ( 2010 ) 115 : 354367 modified american heart association classification [ 10 ]  . all segments , without diameter limits , were included for comparison with ctca . 
the segments were classified as not significantly stenotic ( normal or with wall irregularities or noncritical stenosis < 70% ) or significantly stenotic ( critical stenosis 70% ) , according to the conventional classifications and guidelines . 
the operator visually assessed coronary stenoses during the angiographic session in the projection of maximal stenosis . evaluation of ctca images all ctca scans were analysed by an observer with 5 years of experience in the field and who was blinded to the ca findings . 
all of the standard visualisation techniques were used by the operator [ axial , multiplanar reconstruction ( mpr ) , curved multiplanar ( cmpr ) , maximum intensity projection ( mip ) , volume rendering ( vr ) ]  . 
segments were classified as not significantly stenotic ( normal or with wall irregularities or noncritical stenosis < 50% ) or significantly stenotic ( critical stenosis 50% ) , according to the commonly applied classifications . reconstruction statistical analysis continuous variables were indicated as mean and standard deviation ( meansd )  . 
using quantitative ca as the standard of reference , the diagnostic accuracy of stress ecg and ctca in detecting significant cad was assessed by measuring sensitivity , specificity , positive ( ppv ) and negative ( npv ) predictive values , positive ( sensitivity / [ 1 - specificity ] ) and negative ( [ 1 - sensitivity ] / specificity ] ) likelihood ratios with the corresponding 95% confidence intervals ( ci ) calculated with binomial expansion . 
utilizzando la cag quantitativa come standard di riferimento per laccuratezza diagnostica per lo stressecg e per la ct - ca nella rilevazione di malattia ostruttiva coronarica significativa , sono state calcolate sensibilit , specificit , valore predittivo positivo ( vpp ) e negativo ( vpn ) , likelihood ratio ( lr ) positivo ( sensibilit / [ 1 - specificit ] ) e negativo ( [ 1 - sensibilit ] / specificit ] ) con i corrispondenti intervalli di confidenza ( ic ) al 95% ( calcolati mediante espansione binomiale )  . 
 stress - ecg tutti settantatre ( 33 , 2% ) stress - ecg sono stati classificati come dubbi , 69 ( 31 , 4% ) sono stati classificati come positivi e 78 ( 35 , 5% ) sono stati classificati come negativi . 
ca was analysed ct - ca tutti stress ecg : patients ( n = 147 ) in whom the stress test was either positive or negative , and the diagnostic accuracy of stress ecg vs . 
come risultato la frequenza cardiaca media durate la scansione stata di 63 , 110 , 3 bp il tempo medio di scansione stato di 11 , 51 , 5 secondi . 
in tutti i sottogruppi analizzati la ct - ca mostra elevata sensibilit e valore predittivo negativo ( vpn ) che vengono bilanciati da valori inferiori di specificit e valore predittivo positivo ( vpp )  . 
3 positive and negative likelihood ratios ( lr ) in the populations studied with computed tomography coronary angiography ( ctca ) and stress electrocardiography ( ecg ) with 95% confidence intervals . 
3 likelihood ratio ( lr ) positivo e negativo nelle popolazioni studiate per coronarografia mediante tomografia computerizzata ( ct - ca ) e test ergometrico con elettrocardiogramma ( stress - ecg ) con gli intervalli di confidenza ( ic ) al 95% . 
i valori di lr per la ct - ca sono alti per il lr + e bassi per il lr - , che tradotto significa una buona predittivit positiva e negativa indipendentemente dalla prevalenza di malattia . 
per lo stress - ecg , invece , in valori rimangono attorno a 1 , che significa scarso valore predittivo sia positivo che negativo . radiol med ( 2010 ) 115 : 354367 were wrongly classified as positive . 
three patients were wrongly classified as negative ( 2% ; 3 / 147 ) , and 25 ( 17% ; 25 / 147 ) patients who had no significant stenosis were incorrectly classified as positive . 
this approach , which has already been adopted , allows for a greater transferability of findings to clinical practice [ 11 ]  . the results of our study show that in patients at moderate risk , ctca is by far superior to the more commonly used stress ecg . 
the diagnostic accuracy values were very low ( sensitivity 47% ; specificity 53% ; npv 49% ) , with a high prevalence of equivocal results ( 33.2% ; 73 / 220 )  . with such results , we might as well limit ourselves to performing normal risk stratification based on risk score sheets . 
in contrast , ctca , as shown by the conditional probability graphs , provides a more accurate stratification of the posttest probability of patients at moderate risk la ct - ca una metodica diagnostica robusta ed ampiamente validata [ 16 ]  . 
altri studi prima di questo hanno dimostrato la superiorit della ct - ca rispetto al test da sforzo in popolazioni di pazienti a rischio intermedio [ 7 , 9 ]  . 
questo approccio gi utilizzato in precedenza consente una maggiore trasferibilit dei risultati nella pratica clinica [ 11 ]  . i risultati dello studio dimostrano come anche nella popolazione di pazienti a rischio intermedio , la ct - ca sia ampiamente superiore al comunemente usato stress - ecg . lutilit dello stress - ecg risulta essere , dai dati presentati , molto criticabile . 
i valori di accuratezza diagnostica sono risultati per questo test molto bassi ( sensibilit 47% ; specificit 53% ; vpn 49% ) e con una elevata prevalenza di test dubbi ( 33 , 2% ; 73 / 220 )  . 
la ct - ca invece , come dimostrato anche dai grafici di probabilit condizionale , stratifica molto meglio la probabilit post - test dei pazienti a rischio intermedio ( sensibilit 96% ; specificit 65% ; valore predittivo negativo 94% )  . limpatto diretto che tali osservazioni hanno sulla pratica clinica evidente . 
 consolidato lutilizzo dello stress - ecg per la valutazione del paziente a rischio intermedio ed anche nella valutazione di screening dei pazienti che si sottopongano ad attivit sportive in assenza di sintomi . 
the curve shows the excellent performance in ruling out the disease , in particular at the level of the actual prevalence of disease in the population ( prevalence 60% )  . 
the bottom graphs show the diagnostic performance of ctca ( left ) and stress ecg ( right ) in patients who underwent both tests ( n = 147 patients ; prevalence 51% )  . 
il grafico mette in rapporto la probabilit pre - test e la probabilit post - test di una determinata metodica ( per test positivo linea grigia , per test negativo linea nera )  . 
il grafico in alto a destra mostra invece la performance della ct - ca nei pazienti con test ergometrico con elettrocardiogramma ( stress - ecg ) dubbio ( n = 73 ; prevalenza 83% )  . 
i grafici in basso mostrano la performance diagnostica della ct - ca ( a sinistra ) e dello stress - ecg ( a destra ) nei pazienti nei quali erano presenti entrambe le metodiche ( n = 147 ; prevalenza 51% )  . 
la differenza tra le due metodiche appare significativa sia in caso di test positivo ( teste di freccia nere ) che in caso di test negativo ( teste di freccia grigie )  . 
however , as reported by previous studies [ 7 , 9 ] , the performance of stress ecg in these populations is largely suboptimal , and hence the need to introduce new , more sensitive tests capable of ruling out the presence of cad with greater accuracy . 
among them , stress myocardial perfusion scintigraphy with technetium tracers [ stress single photon emission computed tomography ( spect ) ] has been used for the longest period of time and with the best results [ 12 , 13 ]  . 
tra questi test la scintigrafia miocardica di perfusione da stress con traccianti tecneziati ( stressspect ) sicuramente quella che stata utilizzata per pi tempo e con ottimi risultati [ 12 , 13 ]  . 
questo problema abbastanza semplice da spiegare . infatti , se il gold standard anatomico ( cag ) ed il test ( stress - ecg , stress - spect ) , utilizzato funzionale radiol med ( 2010 ) 115 : 354367 problem of conflicting results persists also when comparing ctca and stress spect [ 12 , 13 ]  . 
in questo algoritmo il test anatomico ( ct - ca ) viene effettuato inizialmente per stratificare i pazienti tra coloro che hanno coronarie indenni da ateromasia , coloro che sono portatori di ateromasia non significativa ( riduzione del lume < 50% ) , coloro che sono portatori di ateromasia attorno al 50% , e coloro che sono portatori di ateromasia francamente ostruttiva ( 50% )  . 
tuttavia molteplici esperienze recenti , con hardware e sofware di nuova generazione ( tc a doppia sorgente , triggering prospettico ecg ) dimostrano come sia fattibile eseguire una ct - ca con dosi di radiazioni < 5 msv , ed in alcuni casi di circa 1 , 2 msv [ 1620 ]  . conclusions the diagnostic accuracy of ctca is superior to that of stress ecg in symptomatic patients with suspected cad and moderate cardiovascular risk . 
fdr , fattori di rischio ; cag , coronarografia convenzionale ; pci , angioplastica coronarica / stenting ; cabg , by - pass aorto - coronarico . deliver lower radiation doses may lead to an extensive use of this modality in the diagnostic workup for suspected cad . 
the evaluation of nonobstructive coronary disease raises questions regarding the correct management of therapeutic and prognostic aspects [ 2124 ]  . potranno consentire un utilizzo estensivo della metodica come primo passo nellalgoritmo diagnostico della sospetta malattia coronarica . 
kizilkaya1 1 gata haydarpasa military hospital , department of radiology , istanbul , turkey 2 gata haydarpasa military hospital , department of ear nose throat , istanbul , turkey 3 gata military school of medicine , department of public health , ankara , turkey correspondence to : o . 
sildiroglu , department of radiology , gata haydarpasa military hospital , 34668 , uskudar , istanbul , turkey , tel . : + 90 - 532 - 6709048 , e - mail : sildiroglu@yahoo.com received : 21 december 2008 / accepted : 27 january 2009 / published online : 28 december 2009 springer - verlag 2009 abstract purpose . 
t1 - weighted , t2 - weighted and parasagittal three - dimensional fourier transformation constructive interference in steady state ( 3dft - ciss ) reconstruction images of all cases were evaluated . 
larea sulla sezione trasversale del cn nel gruppo di pazienti con snhl era pari a 0 , 0232 cm2 mentre nel gruppo di controllo era pari a 0 , 0252 cm2 . 
sebbene i punteggi di discriminazione del linguaggio mostrassero differenze significative , non stata evidenziata nessuna differenza statisticamente significativa per larea trasversale del cn ( p = 0 , 0616 )  . 
la snhl acquisita pu non presentare cambiamenti significativi delle dimensioni del cn alla risonanza magnetica . parole chiave nervo cocleare perdita delludito risonanza magnetica 484 introduction developments in magnetic resonance imaging ( mri ) have allowed detailed evaluation of the anatomical structure within the internal auditory canal ( iac )  . 
combined use of high - resolution t2 - weighted mri together with new imaging algorithms provides excellent depiction of the cerebellopontine angle , the nerves and their branches within the internal auditory canal by way of the high contrast formed by the surrounding cerebrospinal fluid . 
the facial nerve and branches of the vestibulocochlear nerve ( vcn ) can be identified in the lateral portion of the iac , particularly on the cross - sectional images of the nerve [ 1 ]  . 
as a certain degree of neuronal loss is expected with increasing age , a reduction is expected in the diameter of the cochlear nerve ( cn ) [ 2 ]  . we aimed to determine any differences , if present , between the cross - sectional area of the cn of elderly patients with snhl and of young patients with normal hearing . 
 materials and methods the study had a prospective design , and the control and study groups were formed according to age , medical history , otoscopic examination and audiometric evaluation . study group the study group included ten patients with age - related snhl and no previous history of hearing impairment . 
this group included individuals aged 60 years or older with symptoms of hearing loss but normal otoscopic evaluation , with air and bone conduction thresholds above 25 db and speech discrimination score below 90% . control group the control group included 14 volunteers with normal hearing undergoing mri for another reasons excluding ear or neurological disease . 
air and bone conduction thresholds were above 20 db , and speech discrimination scores were above 95% . audiometric evaluation tests were performed in the silent room by a blinded radiol med ( 2010 ) 115 : 483487 operator using ac 40 clinical audiometry and thd - 39 earphones . 
each word repeated correctly was valued at 2% , and scores were calculated as a percent - correct value . mr and measurements the vestibulocochlear nerve measurements were done by a radiologist who was blinded both to the study and the hearing level of the subjects . 
the imaging procedure was a routine inner ear study with 7 - mm - thick axial planes acquired with t1 - weighted sequences [ 640 / 14 ( tr / te ) , matrix 192256 ] and t2 - weighted sequences [ 3 , 900 / 99 ( tr / te ) 264512 ]  . 
additionally , parasagittal three - dimensional fourier transformation constructive interference in steady state ( 3dft - ciss ) reconstruction images ( 15 / 21 , 65 flip angle , 256256 matrix , 170 mm field of view ) on the course of the vestibulocochlear nerve were obtained in all cases . 
all measurements were made by the same radiologist in a patient - blinded fashion for consistency . statistical analysis the results were presented as frequency and median ( minmax )  . 
although speech discrimination scores differed significantly , there was no significant difference between the cn cross - sectional area of the two groups ( p = 0.616 ) ( table 1 )  . 
there was no significant difference between cn cross - sectional area values of female and male patients when each group was evaluated separately or in combination ( table 2 )  . 
although ct images provide excellent resolution and anatomical details of the osseous structures of the temporal bone , it is unable to visualise soft tissue details of the brain and nerves lying in the iac [ 5 ]  . mri is recently being employed to visualise neuronal structures in iac and inner - ear morphology , particularly in children with congenital snhl [ 1 , 38 ]  . 
at the lateral aspect of the iac , the facial nerve lies in the anterosuperior portion , the cn lies in the anteroinferior portion , the superior vestibular nerve lies in the posterosuperior portion and the inferior vestibular nerve lies in the posteroinferior portion [ 5 , 7 ]  . 
with this information on detailed anatomy and by applying the above - mentioned mri technique , it is possible to determine cochlear nerve anomalies . in our study , cn was larger than the branches of the vestibular nerve and equal to or larger than the facial nerve , 486 radiol med ( 2010 ) 115 : 483487 fig . 
1a sequenza 3dft - ciss sul piano assiale in corrispondenza dellangolo ponto - cerebellare e del canale uditivo interno ( iac ) , con i piani corrispondenti alle sezioni parasagittali verticali alle strutture nervose delliac . 
no abnormality was detected in iac caliber of any cases . direct injury due to a vascular , traumatic or infectious etiology can cause acquired snhl by reducing cn caliber . cn injury may indirectly lead to cn fibre degeneration . other causes such as mechanical destruction , ototoxic antibiotics , acoustic trauma and anoxia can lead to approximately 5%10% loss in neuronal mass , whereas neural infection and vascular insufficiency can cause 100% neuronal destruction [ 11 ]  . 
pathophysiological changes after the first injury involve development of oedema in the neuronal fibres that leads to tears in the myelin sheath . collapsed fibre causes reduction in the cn cross - sectional area in the long term [ 12 ]  . age - related hearing loss has also been reported to cause neuronal loss , which could cause reduction in the cn crosssectional area [ 13 , 14 ]  . 
however , almost all of them were conducted on children with congenital snhl [ 2 , 7 ]  . these studies , conditions other than cn aplasiahypoplasia , including vestibular dysplasia , mondini malformations and atretic iac , were also reported [ 1 , 3 , 5 , 7 ]  . 
in this study , reduction in caliber of the cn was reported in six out of ten patients , and four of them had unilateral nerve deficiency . in our study , no significant difference was observed between cn caliber in the study group and control group . likewise , there was no difference in cn caliber between male and female patients . 
we believe that tears of the myelin sheath might not be observed in age - related acquired snhl , as neural loss develops over a rather long time so that no difference in caliber may be observed by mri . 
all these factors may explain why we did not detect significant cn deficiency in age - related snhl . in conclusion , 3dft - ciss sequence provides superior results in cn imaging . 
scuro 10 , 37134 verona , italy 2departement of radiology , casa di cura pederzoli , via monte baldo 8 , peschiera del garda , verona , italy 3department of pathology , university hospital g.b. 
images were assessed for the following parameters , according to the scoring system described by fischer in 1999 : tumour shape , margins , internal enhancement , signal intensity increase , signal intensity course and overall fischer score . 
evaluated histopathological prognostic factors included histological type , associated extensive intraductal component , diameter , lymph node metastasis , tumour grade , and oestrogen receptor ( er ) , progesterone receptor ( pgr ) , ki67 proliferation , oncogene c - erbb - 2 ( her2 / neu ) expression . 
a significant correlation ( p = 0.02 ) was found between stellatedendritic shape and the presence of an associated extensive intraductal component ( eic ) , which was found in 78% of stellate tumours vs . 
le immagini rm sono state analizzate secondo i seguenti criteri descritti nel 1999 dal sistema di fischer : forma , margini , pattern di impregnazione , incremento e andamento del segnale , e punteggio di fischer complessivo . 
una correlazione significativa ( p = 0 , 02 ) emersa fra laspetto morfologico spiculato - dendritico e la presenza di estesa componente intraduttale ( eci ) ( stata rilevata nel 78% dei tumori spiculati vs 49% dei tumori con morfologia rotonda - ovale )  . 
i reperti rm che correlano significativamente con i fattori patologici prognostici del tumore mammario sono la morfologia e landamento della curva del segnale . il sistema di fischer un utile modello interpretativo dei reperti rm , presentando una sensibilit del 93% . parole chiave tumore della mammella risonanza magnetica della mammella fischers score fattori prognostici introduction introduzione breast cancer is the second - highest cause of death from cancer in women , with an incidence that increases with age and peaks around 50 years [ 1 ]  . 
breast cancer is an extremely heterogeneous disease embracing a wide range of clinical patterns and stages of presentation , biological behaviour , histological features , radiological appearances , prognostic characteristics and response to the different types of treatment [ 2 ]  . 
the prognostic role of many features has been defined and used to delineate individual risk profiles at diagnosis in patients with breast cancer and to choose optimal local and systemic treatment modalities . resonance contrast - enhanced magnetic ( ce - mr ) imaging has a high sensitivity in the detection breast carcinoma [ 35 ] and is performed to detect additional foci and to stage the tumour [ 6 , 7 ]  . 
in 1999 , also known as the gttingen score [ 8 ] , based on both mr imaging morphological and functional findings , has been developed and adopted in clinical practice to assess the degree of malignancy of breast disease . only few reports investigating the relationship between the quantitative measurement of enhancement and prognostic factors in invasive breast cancer can be found in the literature [ 913 ]  . 
more encouraging results have emerged from the relationship between microvessel density and enhancement pattern [ 14 , 15 ]  . however , these reports have limited clinical application because of the different and complex methods used to calculate the various parameters . 
the gttingen scoring system , which is available on common workstations and il carcinoma della mammella la seconda causa di morte per cancro nella donna con incidenza che aumenta con lavanzare dellet presentando un picco attorno ai 50 anni [ 1 ]  . 
il carcinoma della mammella una patologia estremamente eterogenea comprendendo una vasta gamma di quadri e stadi di presentazione , comportamento biologico , caratteristiche istologiche , aspetti radiologici , caratteristiche prognostiche e risposta ai diversi tipi di trattamento [ 2 ]  . 
nelle donne con tumore al seno , sono stati individuati molti fattori che giocano un ruolo prognostico e vengono utilizzati per delineare i singoli profili di rischio al momento della diagnosi e per scegliere gli adeguati trattamenti a livello locale e sistemico . 
 lindagine di risonanza magnetica della mammella ( rmm ) con iniezione di mezzo di contrasto ( mdc ) si dimostrata , nel corso di questi anni , metodica efficace nellidentificazione di tumori , sia primitivi che recidivi , con elevata sensibilit che pu raggiungere valore del 100% [ 35 ]  . 
nel 1999 e conosciuto anche come punteggio di gttingen ( dal nome della citt ) [ 8 ] , che associa un punteggio alle caratteristiche morfologiche e funzionali del reperti rmm e che viene adottato nella pratica clinica per valutarne il grado di sospetto di malignit . in letteratura vi sono solo pochi lavori che indagano la relazione tra la valutazione quantitativa dellimpregnazione tumorale e i fattori prognostici del carcinoma invasivo della mammella [ 913 ]  . 
da tali studi emergono risultati variabili e controversi riguardanti la comparazione dellandamento quantitativo dellimpregnazione tumorale nel tempo con gli indicatori prognostici del cancro invasivo della mammella . conclusioni pi incoraggianti emergono da un gruppo di studi che hanno dimostrato una correlazione tra la densit radiol med ( 2010 ) 115 : 421433 applicable in daily activities , represents an alternative to these methods . 
the purpose of our study was to verify whether the mr imaging morphological and dynamic features according to fischers scoring system could significantly correlate with histopathological prognostic factors and identify breast cancers with different biological characteristics . materials and methods patients between january 2006 and december 2008 , 125 patients with a diagnosis of invasive breast cancer underwent cemr imaging for preoperative evaluation . 
the exclusion criteria were : invasive breast cancer without a surgical diagnosis ( 12 breast cancers diagnosed on core biopsy or fine - needle - aspiration biopsy ) , other breast tumours ( 14 cases of carcinoma in situ , two phyllodes tumours ) , multifocal tumour ( ten cases ) , and patients treated with neoadjuvant chemotherapy ( 15 cases )  . 
in the 19 cases treated with tumourectomy only , the surgical margins were disease free at pathological examination of the surgical specimen . ce - mr imaging protocol ce - mr imaging was performed with a 1.5 - t superconductive unit ( symphony ; siemens , erlangen , germany ) on days 714 of the menstrual cycle in premenopausal women ( 35 in postpatients ) and without menopausal women ( 37 patients )  . 
tali esperienze soffrono di limitata applicazione clinica a causa dei diversi e complessi metodi utilizzati per il calcolo dei vari parametri . per questo motivo , nel presente studio , stato adoperato il sistema di punteggio fischer , che comunemente disponibile alla work station e applicabile nella attivit quotidiana . lo scopo di questo studio verificare se esistono aspetti morfologici e dinamici descritti dal sistema fischer che possano significativamente correlare con i fattori istologici prognostici del tumore mammario , ovvero identificare carcinomi mammari con diverse caratteristiche biologiche . materiali e metodi pazienti nel periodo compreso tra gennaio 2006 e dicembre 2008 , sono state studiate consecutivamente , con indagine rmm pre - operatoria , 125 pazienti . 
tutte le pazienti sono state sottoposte a intervento chirurgico entro 2 mesi dallindagine rm sono stati inclusi in questo studio tutti i casi con diagnosi istologica su pezzo operatorio di carcinoma infiltrante a crescita monofocale . 
sono stati esclusi da questo studio i casi di carcinoma infiltrante senza diagnosi istologica su pezzo operatorio ( 12 casi con diagnosi microistologica o citologica di carcinoma infiltrante ) , i casi con diagnosi istologica diversa da carcinoma infiltrante ( 14 casi di carcinoma in situ , 2 casi di tumore filloide ) , i casi di tumore multifocale ( 10 casi ) e quelli trattati con chemioterapia neoadiuvante ( 15 casi )  . 
lintervento di mastectomia stato eseguito in caso di tumori superiori a 5 cm , tumori la cui dimensione in rapporto al volume del seno non consentiva una chirurgia conservativa , o per scelta della paziente . 
nei 19 casi sottoposti a tumorectomia , i margini chirurgici sono risultati esenti da malattia allesame patologico del pezzo operatorio . protocollo rmm lo studio rmm stato effettuato con un magnete da 1 , 5 t ( symphony , siemens medical system , erlagen , germania ) nel periodo compreso fra il 714 giorno del ciclo mestruale in 35 casi e senza limitazioni temporali nelle 37 424 radiol med ( 2010 ) 115 : 421433 was performed with three - dimensional t1 - weighted gradient recalled echo ( gre ) acquisition in the coronal plane ( tr / te : 12 / 5.65 ms ; flip angle 25 ; matrix 254320 ; field of view 38075 ; slice thickness 1.24 mm ; acquisition time 60 s ) obtained before and for six times after intravenous bolus injection of 0.1 mmol / kg body weight gadoterate meglumine ( dotarem ; guerbet co . , japan ) at a rate of 2.5 ml / s followed by 20 ml of saline flush . image analysis images were transferred to a workstation for postprocessing . in all cases , the baseline acquisitions were subtracted from the postcontrast dynamic images to detect the enhancing areas of the breast and to evaluate their shape , margins and enhancement pattern . 
for each lesion , the ce - mr imaging features were evaluated according to the fischer scoring system to evaluate suspicion for malignancy of the enhancing areas detected at breast mr imaging ( table 1 ) [ 8 , 16 , 17 ]  . time - signal intensity curves were constructed by placing a region of interest ( roi , 59 pixels ) in the area of strongest enhancement on the second contrast - enhanced image . 
lo studio dinamico stato eseguito con una sequenza gradient echo ( gre ) 3d sul piano coronale ( tr / te : 12 / 5 , 65 ms ; flip angle 25 ; matrice 254320 pixel ; field of view ( fov ) 38075 ; spessore 1 , 24 mm ; tempo di acquisizione 60 secondi ) acquisita prima della somministrazione di mdc e ripetuta per sei volte dopo liniezione endovenosa di 0 , 1 mmol / kg di gadoterate meglumina ( dotarem , guerbet co . , giappone ) alla velocit di 2 , 5 ml al secondo e di 20 ml di soluzione fisiologica . analisi delle immagini le immagini sono state elaborate mediante sottrazione delle acquisizioni pre - contrasto da quelle post - contrasto e analizzate secondo i parametri forma , margini e cinetica dellimpregnazione . 
le aree di aumentata impregnazione sono state analizzate secondo gli aspetti morfologici e dinamici descritti dai parametri di fischer nel 1999 ( tabella 1 ) [ 8 , 16 , 17 ]  . 
 posizionando una regione dinteresse ( roi ; estesa 59 pixels ) sulle aree di impregnazione di mdc visualizzate nella seconda acquisizione dopo mdc sono state costruite curve delle variazioni di intensit di segnale / tempo . 
histopathological type of carcinoma ( ductal , lobular , tubular , mucinous , medullary , papillary ) defined according to the world health organization ( who ) classification [ 19 ] 2 . 
axillary lymph node involvement ( negative / positive )  . nodal status was ascertained with sentinel node biopsy in the case of tumours 20 mm without macroscopically suspicious nodes and axillary nodal dissection in the remaining cases 5 . 
staining for er , pgr and ki67 was assessed by counting the percentage of the stained cancer - cell i seguenti fattori istologici prognostici sono stati valutati sulle sezioni dei pezzi operatori : 1 . 
lo stato ascellare stato esaminato con biopsia del linfonodo sentinella in caso di neoplasie 20 mm senza segni macroscopici suggestivi di coinvolgimento ascellare e con svuotamento ascellare nei rimanenti casi . 
lespressione dei recettori per gli estrogeni ( er ) , dei recettori per il progesterone ( pgr ) , dellindice di proliferazione ki67 e delloncogene c - erbb - 2 ( her2 / neu )  . 
 il valore dellespressione di er , pgr e ki67 stato assegnato contando la percentuale di nuclei di cellule radiol med ( 2010 ) 115 : 421433 table 1 fischer multifactorial evaluation protocol ( gttingen score ) imaging feature criterions 1 shape 2 margins 3 enhancing pattern dynamic criterions initial signal increase 5 postinitial signal course aspetti semeiologici parametri morfologici 1 forma 2 margini 3 pattern di impregnazione parametri dinamici incremento iniziale del segnale 5 curva del segnale nel tempo round oval polygonal linear branching spiculated well defined indistinct homogeneous inhomogeneous septated ring enhancement < 50% 50%100% > 100% steady increase plateau washout rotonda ovale poligonale lineare dendritica spiculata ben definiti mal definiti omogeneo disomogeneo settato ad anello < 50% 50%100% > 100% costante aumento plateau washout points tabella 1 valutazione multifattoriale della rmm secondo fischer ( gttingen score ) punteggio nuclei . 
il punto di cut - off per la positivit per er e pgr era 10% mentre per ki67 era 20% . lespressione delloncogene c - erbb - 2 stata assegnata secondo una scala semiquantitativa compresa tra 0 e 3 +  . solo la categoria 3 + stata considerata positiva . 426 statistical analysis fishers exact test was used to correlate the ce - mr imaging parameters with the histopathological findings . morphological and functional features on ce - mr imaging were categorised according to the fischer scoring system ( table 1 )  . 
statistical significance was set at a p value < 0.05. radiol med ( 2010 ) 115 : 421433 analisi statistica tramite fishers exact test si valutata la possibile esistenza di correlazione fra i parametri morfologici e dinamici dellindagine rmm e i fattori prognostici istopatologici . 
il pattern di impregnazione interna della lesione stato dicotomizzato considerando separatamente omogeneo da una parte e disomogeneo e ad anello dallaltra parte ; lincremento dellintensit di segnale nei primi tre minuti stata dicotomizzata in lento e medio da una parte e rapido dallaltra parte . 
la intensit di segnale dopo due minuti stata dicotomizzata prendendo in considerazione la curva di tipo i persistente e quella di tipo ii a plateau insieme vs la curva di tipo iii wash out . 
 gli aspetti istopatologici analizzati sono stati : il tipo istologico , dicotomizzato in carcinoma duttale infiltrante vs altri istotipi di carcinoma infiltrante ( lobulare , midollare , mucinoso , papillare e tubulare ) , la presenza di eci vs tumori senza eci , linfiltrazione dei linfonodi ascellari ( negativa vs positiva ) , il grado istologico , dicotomizzato in basso - intermedio ( g1 e g2 ) vs elevato ( g3 ) , recettori er e pgr considerati positivi ( colorazione 10% ) , o in caso contrario negativi , indice proliferativo , dicotomizzato in alto ( colorazione ki6720% delle cellule tumorali ) e basso ( colorazione ki67 < 20% delle cellule tumorali ) , sovraespressione her2 , considerata presente nei tumori con punteggio 3 + o assente nei tumori con punteggio 0 , 1 + or 2 +  . dato che le dimensioni della neoplasia costituiscono uno dei principali fattori prognostici e dallaltra parte sono correlate con gli aspetti rmm ( in particolare con il pattern di impregnazione ) sono state valutate separatamente per ogni pattern di impregnazione . la associazione fra i fattori patologici prognostici e i caratteri rmm stata analizzata con fishers exact test . 
la significativit statistica stata fissata a un valore p < 0 , 05 . results ce - mr imaging features morphological parameters risultati rilievi rmm parametri morfologici all breast carcinomas were described as focal masses on mr imaging . 
per quanto riguarda gli aspetti morfologici , nei 72 casi esaminati , la forma era rotonda o ovale in 49 / 72 ( 68% ) casi e stellata - dendritica in 23 / 72 ( 32% ) casi . 
the behaviour of the time - signal intensity curves was continued or plateau in 24 / 72 ( 33% ) cases and with washout in 48 / 72 ( 66% ) cases . 
a comparison of histopathology and ce - mr imaging features is shown in tables 2 and 3 . pathological and immunohistochemical analysis pathological analysis revealed the following prognostic factors : 1 . 
histological type was invasive ductal carcinoma not otherwise specified in 54 / 72 ( 75% ) patients and other histological types in 18 / 72 ( 25% ) : lobular carcinoma in 15 / 72 ( 21% ) , tubular in 0 / 72 ( 0% ) , mucinous in 0 / 72 ( 0% ) , medullary in 1 / 72 ( 1.4% ) and papillary in 2 / 72 ( 3% ) 2 . 
we found 53 / 72 ( 74% ) cases were er positive , 52 / 72 ( 72% ) were pgr positive , 28 / 72 ( 39% ) were ki67 positive ( 20% ) and 12 / 72 ( 17% ) were her2 ( + 3 )  . analysis of ce - mr imaging and pathological features results of the statistical analysis are reported in detail in tables 2 and 3 . 
24 / 49 ( 49% ) of roundoval tumours showed an associated ductal in situ component . no significant correlation but frequent association ( p = 0.054 , borderline value ) was found between enhancement pattern and histological type . 
all tumours with omogeneo in 11 / 72 ( 15% ) casi , disomogeneo o con segno dellanello periferico 61 / 72 ( 85% ) casi ( disomogeneo in 46 e con anello periferico in 15 casi )  . 
i tumori con impregnazione omogenea avevano diametro medio di 7 mm , quelli con impregnazione disomogenea 19 mm , mentre i tumori che presentavano anello periferico di impregnazione dimensioni di 21 m parametri dinamici per quanto riguarda gli aspetti dinamici , lincremento relativo dellintensit di segnale nei primi due minuti dalla somministrazione di contrasto stato in media del 200% ( range fra 80% e 530% )  . 
in particolare , lincremento dellintensit di segnale nei primi due minuti stato medio ( inferiore al 100% ) in 2 casi ( 3% ) , rapido ( > 100% ) in 70 / 72 casi ( 97% )  . 
landamento delle curve di impregnazione intensit - tempo era di tipo i e ii con impregnazione progressiva e a plateau in 24 / 72 ( 33% ) casi e di tipo iii con wash out in 48 / 72 ( 66% ) casi . 
cinquantatre / 72 tumori ( 74% ) presentavano recettori er di superficie e 52 / 72 ( 72% ) avevano recettori pgr . ventotto casi su 72 ( 39% ) erano positivi per la proliferazione del ki67 ( 20% ) e 12 / 72 casi ( 17% ) mostravano sovraespressione delloncogene her2 ( + 3 )  . analisi degli aspetti rmm e dei fattori anatomopatologici i risultati dellanalisi statistica fra aspetti rmm e fattori prognostici istologici sono riportati in dettaglio nelle tabelle 2 e 3 . 
 discussion the purpose of our study was to verify whether mr imaging morphological and dynamic features evaluated according to the fischer scoring system could significantly correlate with histopathological prognostic factors and identify breast cancers with different biological characteristics . axillary lymph node status is the most important prognostic factor ; other prognostic factors of invasive breast cancer are a high tumour grade , high proliferation status , her2 overexpression and er and pgr receptor positivity [ 21 ]  . 
her2 overexpression correlates with a high grade and hormone - receptor negativity and establishes patients eligibility for treatment with the monoclonal antibody trastuzumab [ 22 , 23 ]  . in this study , we considered the preoperative ce - mr imaging features of surgically proven invasive breast cancer in order to correlate the ce - mr imaging findings with prognostic histopathological factors . 
this protocol includes morphological criteria dendritica mentre solo in 24 / 49 ( 49% ) tumori con morfologia rotonda - ovalare . il pattern di impregnazione e listotipo tumorale hanno dimostrato frequente associazione , priva di significativit statistica ( p = 0 , 054 , borderline value )  . 
i carcinomi duttali infiltranti sono stati il 100% dei tumori con impregnazione omogenea e 43 / 61 ( 70% ) dei tumori con impregnazione disomogenea o ad anello ( i rimanenti 18 / 61 ( 30% ) erano di altri istotipi )  . 
la maggior parte dei tumori con curva a wash out , 23 / 48 ( 81% ) , rispetto a 5 / 24 ( 21% ) tumori con curva di tipo continuo - plateau , risultata associata a elevata espressione di ki67 ( p = 0 , 039 )  . 
si soprassiede allanalisi dellincremento dellintensit del segnale dicotomizzato fra il gruppo con incremento medio ( 2 casi , che risulta troppo esiguo ) e laltro con incremento rapido osservato nei rimanenti 70 casi . 
 discussione lo scopo di questo studio verificare se esistono aspetti morfologici e dinamici descritti dal sistema fischer che possano significativamente correlare con i fattori istologici prognostici del tumore mammario , ovvero identificare carcinomi mammari con diverse caratteristiche biologiche . la prognosi del tumore mammario correlata a ben noti indicatori prognostici , fra cui il pi importante risulta il coinvolgimento tumorale , linfonodale , seguito dal grado dallindice replicativo , dallespressione delloncogene her2 , e dei recettori ormonali di superficie cellulare ( er e pgr ) [ 21 ]  . 
recentemente altri marcatori biologici sono stati proposti come significativi di proliferazione e come indicatori di differenziazione , della invasivit e della capacit metastatica delle cellule tumorali . laumentata espressione delloncogene her2 indice di maggior aggressivit del tumore e caratterizza un distinto sottogruppo di tumori che rappresenta il 25%30% i tutti i casi . 
questo gruppo si distingue per aumentata espressione di her2 , alto grado tumorale e mancanza di recettori ormonali di superficie ed pertanto candidato a trattamento con lanticorpo monoclonale trastuzumab [ 22 , 23 ]  . nel presente studio , abbiamo analizzato gli aspetti del tumore mammario invasivo rilevabili allindagine rmm e le loro possibili correlazioni con gli indicatori istologici prognostici . 
i rilievi rmm sono stati considerati secondo il sistema di valutazione di fischer et al . , conosciuto anche come radiol med ( 2010 ) 115 : 421433 ( form , margins , enhancement pattern ) and dynamic criteria ( initial signal increase , signal intensity course ) , and each parameter is assigned a point value . 
this limitation was also observed in our study in which 19% of invasive tumours had a fischer score of 04 . in particular , 5 / 72 invasive tumours ( false negative ) had a point value of 3 , resulting in 93% sensitivity of the fischer score . 
the ce - mr imaging protocol used in this study is a compromise between spatial and temporal resolution ( 60 s per sequence , 1.24 - mm slice thickness ) that provides accurate assessment of all parameters . 
the current suggested in - plane resolution is < 1 mm , accepting a trade - off in terms of temporal resolution , which can reach 120 s without significant negative impact on dynamic analysis [ 26 ]  . 
 although previous authors [ 12 ] reported no correlation between quantitative evaluation of enhancement and histological type , a frequent but not significant association between enhancement pattern and histological type was observed in our series . 
this is a limitation of this study , which due to small sample size did not have sufficient power to reach significance . regarding kinetic parameters , we found a correlation between washout curve and ki67 expression , as previously reported [ 27 ]  . 
il sistema di punteggio di fischer introduce un protocollo di valutazione multifattoriale con lo scopo di facilitare la differenziazione delle lesioni iper - vascolarizzate rmad ogni criterio morfologico della lesione ( forma , margini , pattern di impregnazione ) e per ogni criterio dinamico ( iniziale aumento del segnale , e successivo andamento ) stato assegnato un punteggio da sommare agli altri . 
un punteggio totale superiore a 3 punti sospetto di malignit ( tabella 1 ) [ 8 ]  . tuttavia , tale sistema di punteggio soffre di una considerevole sovrapposizione tra il comportamento delle lesioni benigne e maligne . 
questo risultato simile a quello ottenuto da parte del gruppo di gttingen riguardo questa valutazione multifattoriale applicata su un grande studio retrospettivo che ha riportato sensibilit del 93% [ 25 ]  . 
daltro canto , almeno cinque misurazioni dopo liniezione di mezzo di contrasto , con risoluzione temporale di 12 minuti per sequenza , sono necessarie per la discriminazione tra la neoangiogenesi tumorale e il parenchima ghiandolare circostante . 
lo studio rmm stato condotto con sequenze che rappresentano un compromesso tra risoluzione spaziale e temporale ( 60 secondi per sequenza , 1 , 24 mm di spessore ) per fornire una valutazione per quanto possibile accurata di tutti i parametri . 
attualmente , la risoluzione in - plane proposta inferiore a 1 millimetro , accettando di pagare un compromesso in termini di risoluzione temporale che pu arrivare a 120 secondi senza significative ripercussioni negative sullanalisi dei criteri dinamici [ 26 ]  . 
la limitata risoluzione in - plane utilizzata in questo lavoro potrebbe spiegare alta percentuale di casi con morfologia rotonda / ovalare ( 68% ) riportati utilizzando lo score di gttingen . 
il parametro morfologia stellatadendritica risultato significativamente associato alla presenza di estesa componente intraduttale accanto alla componente infiltrante , ma a differenza di precedenti lavori non risultato correlato con lo stato her2 [ 27 ]  . 
 sebbene non sia stata riportata correlazione tra il pattern di impregnazione e listotipo tumorale [ 12 ] , in questa serie si osservata una frequente , ma non significativa , associazione ( p = 0 , 054 , valore borderline ) fra il parametro impregnazione omogenea e listotipo duttale infiltrante . 
ventitr casi su 48 ( 48% ) con la curva a wash out avevano elevata espressione del ki67 e 19 / 24 ( 80% ) tumori con curva a plateau hanno mostrato bassa espressione del ki67 ( p = 0 , 039 )  . 
in comparison with previous reports [ 28 ] , the peculiarity of this study derives from the fact that all cases included had a pathological diagnosis on the surgical specimen rather than on the core biopsy , which makes it an extremely homogeneous series with regard to pathological diagnosis . 
firstly , because it is retrospective and reflects the natural distribution in the population , each histological type of tumour is not equally and numerically well represented , except for infiltrative ductal carcinoma . 
secondly , the introduction of fischers score as an evaluation method suffers from problems of reproducibility related to the experience of the radiologist . the use of the fischer scoring system could appear questionable ; the fisher score was devised before the breast imaging reporting and data system ( bi - rads ) mr imaging classification , and some criteria of the bi - rads classification such as mass / nonmass should be evaluated . 
in order to avoid misunderstandings , we analysed only unifocal invasive tumours with mass - like enhancement for which the fischer score and evaluation of dynamic patterns have great relevance . considering that highly vascularised tumours have greater metastatic capacity and a poorer prognosis , different combinations of morphological and dynamic criteria could be supported by subtypes of cancer with different prognosis . further investigations should prospectively analyse the capabilities of ce - mr for preoperatively predicting the behaviour and biological activity of breast cancers in a noninvasive manner . 
 imaging in conclusion , correlating mr imaging morphological and dynamic features evaluated according to the fischer scoring system and the histopathological prognostic factors , we found that stellate shape predicts an associated extensive ductal in situ component , and washout curves correlate with high ki67 expression . 
however , considering that 19% of tumours had fischer scores 4 , the evaluation of all diagnostic imaging modalities is essential in deciding on the appropriate diagnostic procedure and patient management . 
a differenza dello studio citato [ 28 ] , sono stati inclusi solo casi con diagnosi patologica su pezzo chirurgico ed esclusi quelli con diagnosi micro - istologica al fine di avere una serie estremamente omogenea per diagnosi patologica . lo studio presenta alcuni limiti . 
luso del sistema di punteggio fischer potrebbe inoltre apparire discutibile sia perch antecedente rispetto allintroduzione della classificazione breast imaging reporting and data system ( bi - rads ) sia in considerazione del fatto che alcuni criteri della classificazione birads , come limpregnazione di tipo massa e non - massa , sono di interessante valore . 
per lo stesso motivo , laspetto dendritico potrebbe essere attribuibile sia al pattern di impregnazione di tipo non - massa che alla morfologia di una lesione con impregnazione di tipo massa . 
al fine di evitare fraintendimenti , abbiamo analizzato solo tumori invasivi a crescita monofocale con impregnazione di tipo massa per i quali lo score di fischer e la valutazione degli aspetti dinamici hanno ancora significato ragionevole . 
 considerando che i tumori altamente vascolarizzati hanno capacit metastatica superiore e peggior prognosi , differenti combinazioni dei criteri morfologici e dinamici potrebbe essere sostenuti da sottotipi di tumore con prognosi diversa . 
tali informazioni potrebbero rivelarsi utili per lottimale pianificazione del trattamento dei pazienti affetti da tumore al seno . in conclusione , dalla correlazione fra gli aspetti rmm dei tumori invasivi secondo il sistema fischer e gli indici istologici prognostici emerso che il parametro morfologia stellata - dendritica associato alla presenza di estesa componente intraduttale e che i tumori con curva di impregnazione con andamento a wash out sono associati a elevata espressione di ki67 . 
orsola malpighi , azienda ospedaliero universitaria di bologna , via massarenti 9 , 40138 bologna , italy 2servizio sanit pubblica , direzione generale sanit e politiche sociali , regione emilia - romagna , via a . 
this paper illustrates the annual trends in medical radiation exposure due to conventional radiography ( cr ) , computed tomography ( ct ) and nuclear medicine ( nm ) procedures of the emilia - romagna population from 2001 to 2006 materials and methods . 
in particular , numerical values of the following dosimetric parameters were requested : entrance skin dose for cr , ct dose index and dose - length product for ct and activity administered for nm . 
the 13 diagnostic imaging procedures that were the greatest contributors to the emilia - romagna population dose between 2001 and 2006 were identified and , for the year 2006 , their percentage contribution to total procedures and population dose are indicated . 
this type of study relies heavily on the analysis of field data and as such , the growing attention paid in recent years to procedure optimisation should continue , and expand even for the justification of the riassunto obiettivo . 
si sono acquisite informazioni relative alla tipologia ed alla frequenza degli esami di rc , tc e mn eseguiti nelle 17 aziende sanitarie dellemiliaromagna ed alle dosi medie per ogni tipologia di procedura . 
si sono indicate le 13 procedure radiodiagnostiche che ogni anno , dal 2001 al 2006 , hanno fornito i pi elevati contributi di dose alla popolazione emiliano - romagnola e per il 2006 sono stati esplicitati i relativi contributi alla dose ed al numero totale di prestazioni . 
in questa tipologia di studi fondamentale radiol med ( 2010 ) 115 : 488498 procedures themselves as justification has a significant impact on the reduction of s and per - caput doses . keywords dosimetry exposure measurements patient radiation protection poter analizzare dati raccolti sul campo : pertanto la sempre maggiore attenzione rivolta in questi anni allottimizzazione delle procedure deve continuare ed espandersi anche alla giustificazione delle stesse , che ha un impatto molto rilevante sul contenimento dei valori di s e della dose pro - capite . parole chiave dosimetria misura esposizione radioprotezione paziente introduction introduzione the use of ionising radiation for medical purposes is by far the greatest source of radiation exposure of anthropic origin . therefore , the evaluation and quantification of this exposure in terms of population dose due to radiological procedures is a very useful tool for a variety of purposes . 
these include comparing the dose delivered by radiology with the dose due to natural background radiation ; verifying whether there are significant differences between the dose delivered in different regions or nations ; and , last but not least , providing information regarding the individual contributions to total dose of the different types of radiological examinations or different medical imaging modalities . different countries have published the findings of evaluations of the population dose through diagnostic imaging procedures [ 15 ] , but no similar study has been produced with regard to the italian population . 
italian legislation [ 6 ] dictates that each italian region is responsible for evaluating its populations exposure to radiodiagnostic ionising radiation every 5 years and for transmitting the relevant data to the ministry of health . 
in addition to respecting this legal obligation , since 2000 ( the year in which the european directive 97 / 43 / euratom [ 7 ] was incorporated in the national legislation ) the emilia - romagna region , in particular , has had in place a series of campaigns for collecting data regarding dosimetry and frequency of radiological procedures [ 810 ] with the aim of monitoring the dose to the regional population from medical and diagnostic imaging exposure in the procedures of conventional radiology ( cr ) , computed tomography ( ct ) and nuclear medicine ( nm )  . 
and diagnostic nuclear medicine in vivo . the aim of this study was to demonstrate the trend over the years of the dose to the emilia - romagna region population due to radiation exposure from diagnostic imaging and compare this with similar studies performed in other countries to evaluate whether there are certain sectors where efforts should be concentrated for dose reduction and luso delle radiazioni ionizzanti a scopo medico costituisce di gran lunga la pi grande sorgente di esposizione alle radiazioni tra quelle di origine antropica . 
pertanto il valutare e quantificare tale esposizione , in termini di dose alla popolazione dovuta alle procedure radiodiagnostiche , uno strumento molto utile per varie finalit : confrontare il contributo della dose dovuta alla radiologia con quella dovuta al fondo naturale ; verificare se esistono differenze significative tra le dosi erogate in differenti regioni o nazioni ; ultimo in ordine di elenco , ma non certo meno importante , fornire informazioni sui singoli contributi alla dose totale da parte dei diversi tipi di esami radiologici oppure delle diverse tipologie di imaging medico . diverse nazioni hanno pubblicato i risultati delle valutazioni delle dosi alla popolazione per esposizioni mediche [ 15 ] , ma nessuno studio stato prodotto relativamente alla popolazione italiana . 
la nostra legislazione [ 6 ] stabilisce che le regioni sono gli organismi preposti ad effettuare ogni 5 anni la valutazione delle esposizioni mediche a radiazioni ionizzanti con riguardo alla popolazione e ad inviare i relativi dati al ministero della salute . 
la regione emilia - romagna , in particolare , oltre ad ottemperare a tale obbligo normativo , si attivata fin dal 2000 ( anno di recepimento della direttiva europea 97 / 43 / euratom [ 7 ] ) per effettuare diverse campagne di raccolta dati dosimetrici e di frequenza delle prestazioni [ 810 ] con il fine di monitorare la dose alla popolazione regionale dovuta ad esposizioni mediche di radiodiagnostica nelle procedure di radiologia convenzionale ( rc ) , tomografia computerizzata ( tc ) e medicina nucleare ( mn ) : infatti importante notare che nel d . 
e alla medicina nucleare diagnostica in vivo . scopo di questo lavoro illustrare landamento negli anni della dose alla popolazione della regione emiliaromagna dovuta ad esposizioni mediche di radiodiagnostica e confrontarla con indagini analoghe condotte in altre nazioni , per valutare se esistano settori in cui concentrare gli sforzi volti alla riduzione delle dosi ed allottimizzazione 490 radiol med ( 2010 ) 115 : 488498 optimisation of radiation protection in patients , as well as the complete application of the ethical principle of justification . della radioprotezione del paziente , nonch ad una piena applicazione del principio di giustificazione . materials and methods materiali e metodi the dose from medical exposure of the emilia - romagna population was evaluated on the basis of several preliminary methodological choices : we initiated a data collection campaign despite being aware that maximum evaluation accuracy at the outset would not be possible but knowing that , over time , accuracy would improve due to subsequent approximations , thanks to the diffusion of a culture of patient radiation protection and procedure optimisation throughout the region . the doses delivered for radiation therapy were excluded , whereas those delivered in the major radiodiagnostic examinations were included . in cr and ct , we included examinations that provided a relevant contribution to the collective dose in that they are the most commonly performed or have a relevant dose impact for the individual patient , with the identification of 12 broad categories . in nm , we included examinations for which reference diagnostic levels have been defined [ 6 ] , with the addition of three positron emission tomography ( pet ) examinations for a total of 35 examinations differing by type , radiotracer used or patient age . interventional radiological procedures were not included . we then began to acquire information regarding the type and frequency of cr , ct and nm examinations performed in the 17 hospitals in emilia - romagna and regarding the mean effective doses for each type of examination . 
in the first year of data collection ( 2000 ) , the number of outpatient examinations was requested from the different hospitals , whereas the number of inpatient examinations was extrapolated to the entire region from a sample taken from two hospitals ( cesena and modena )  . 
in the following years ( 20012006 ) , the hospitals were requested to supply the number of examinations ( both inand outpatient ) for each type of procedure subdivided by type and grouped by nomenclature code . 
any incomplete data provided by the hospitals were integrated by extrapolations based on data supplied by other hospitals and by a regional database ( assistenza specialistica ambulatoriale asa )  . 
with regard to nm examinations , the relative frequency was requested directly from the ten nm departments operating in the region . dose evaluations were aided by the fact that legislative decree 187 / 2000 obligates radiological departments to have experts in medical physics verify the reference diagnostic levels every 2 years . 
therefore , the various hospitals were requested , with regard to examinations included in our per valutare la dose alla popolazione da esposizioni mediche in emilia - romagna si sono preliminarmente effettuate alcune scelte metodologiche : si deciso di procedere a campagne di raccolta dati pur essendo consapevoli che non sarebbe stato possibile avere fin dallinizio la massima accuratezza nelle valutazioni effettuate , ma che questa sarebbe migliorata nel tempo per approssimazioni successive , grazie alla diffusione di una cultura di radioprotezione del paziente e di ottimizzazione delle procedure su tutto il territorio regionale ; le dosi somministrate per fini radioterapeutici sono state escluse e sono invece state considerate le dosi somministrate nei principali esami radiodiagnostici ; in rc e tc sono stati presi in considerazione gli esami che forniscono un contributo rilevante alla dose efficace collettiva in quanto sono i pi diffusi oppure quelli che hanno un impatto dosimetrico rilevante per il singolo paziente , identificando dodici differenti macroaggregati ; in mn sono stati presi in considerazione gli esami per cui sono stati definiti [ 6 ] i livelli diagnostici di riferimento ( ldr ) ai quali sono stati aggiunti tre esami di tomoscintigrafia tramite tomografia ad emissione di positroni ( pet ) per un totale di 35 esami , differenti per tipologia , per radiofarmaco utilizzato o per et del paziente ; le procedure di radiologia interventistica non sono state prese in considerazione . successivamente si proceduto ad acquisire informazioni relative alla tipologia ed alla frequenza degli esami di rc , tc e mn eseguiti nelle 17 aziende sanitarie ( as ) dellemilia - romagna ed alle dosi efficaci medie per ogni tipologia di esame . 
nel primo anno di raccolta dati ( 2000 ) il numero delle prestazioni ambulatoriali stato richiesto alle diverse as , mentre quello delle prestazioni in regime di degenza stato estrapolato a tutta la regione da un campione riferito a 2 realt ( cesena e modena )  . 
negli anni successivi ( 20012006 ) per ognuna delle procedure considerate stato richiesto alle as il numero di prestazioni ( in regime sia ambulatoriale sia di degenza ) suddivise per tipologia e raggruppate per codice del nomenclatore ministeriale . 
i dati eventualmente incompleti forniti dalle strutture sanitarie sono stati integrati tramite estrapolazioni basate sui dati trasmessi dalle altre as e dalla banca dati dellassistenza specialistica ambulatoriale regionale ( asa )  . 
after having calculated e for the various procedures , population dose trend was performed for each year from 2001 to 2006 with an evaluation of the collective dose s [ 15 ] and per - caput dose ( = s in a given year / number of inhabitants in emilia - romagna in the same year )  . 
with regard to 2000 , we also performed a dosimetric estimation according to the methods described in earlier studies [ 8 , 9 ]  . results table 1 summarises the 13 diagnostic imaging procedures that over the study period accounted for the greatest contribution to dose delivered to the emilia - romagna population . figure 1 shows the data with regard to the last year of data collection 2006 ( the other years show similar trends , with some slight differences in the order , as reported in table 1 )  . the figure shows the 13 procedures that contributed most to the dose , with their relative percentages , as well as the percentage contribution to each procedure to the total number of examinations . 
1 account for approximately 97% of the collective e due to medical exposure analysed in this study . figure 2 shows the trend over time of s and the per - caput dose in the years in which the collection of dosimetric data and examination frequency of both inand outpatient procedures was performed , i.e. 
data from 2000 are also included , with the understanding that data referring to inpatient procedures were extrapolated from data of only two hospitals and that the calculation methods were slightly different from those of later years . figure 3 shows the most recent subdivision ( 2006 ) of the contribution to the three modalities ( cr , ct and nm ) to collective dose and total examinations . 
it should be noted that cr accounts for 12% of s and 83% of examinations , whereas ct accounts for 78% of s ( nearly six times greater ) and only 15% of examinations ( nearly six time less )  . 
pertanto alle varie as sono stati richiesti , relativamente agli esami presi in considerazione , i valori numerici dei parametri dosimetrici misurati durante queste verifiche : dose di ingresso ( entrance skin dose , esd ) per la rc , indice di dose tc ( computed tomography dose index , ctdi ) e prodotto dose - lunghezza ( doselength product , dlp ) per la tc , attivit somministrata per la mn . 
dopo aver effettuato il calcolo di e per le varie procedure , per studiare landamento nel tempo della dose alla popolazione si infine effettuata per ogni anno dal 2001 al 2006 la valutazione delle grandezze dosimetriche dose efficace collettiva ( s ) [ 15 ] e dose pro - capite ( s in un dato anno / numero degli abitanti dellemilia - romagna nello stesso anno )  . 
 risultati nella tabella 1 sono riportate le 13 procedure radiodiagnostiche che hanno fornito , nei vari anni , i pi elevati contributi alla dose della popolazione emiliano - romagnola . in figura 1 tale dato viene esplicitato relativamente allultimo anno di raccolta dati , il 2006 ( gli altri anni mostrano comunque andamenti analoghi , con qualche lieve differenza nellordine secondo quanto riportato in tabella 1 ) : sono illustrate le 13 procedure che forniscono i pi alti contributi alla dose , con le relative percentuali , e contestualmente vengono indicati anche i contributi percentuali delle stesse procedure al numero totale di prestazioni . linsieme di tutti i contributi riportati in figura 1 rappresenta circa il 97% della dose efficace collettiva alla popolazione dellemilia - romagna dovuta alle esposizioni mediche analizzate nel presente lavoro . in figura 2 viene mostrato landamento temporale di s e della dose pro - capite negli anni in cui sono state effettuate le campagne di raccolta dati dosimetrici e di frequenza delle prestazioni in regime sia ambulatoriale sia di degenza , 492 radiol med ( 2010 ) 115 : 488498 radiol med ( 2010 ) 115 : 488498 494 radiol med ( 2010 ) 115 : 488498 fig . 
2 andamento temporale dallanno 2000 allanno 2006 della dose efficace collettiva e della dose pro - capite relativamente alle prestazioni considerate in questo studio ( i dati relativi allanno 2000 sono stati parzialmente estrapolati come descritto nel testo )  . discussion recently , the international scientific community tackled the problem of the validity of continuing to use the physical quantity e as a parameter for quantifying and studying radiation protection in patients [ 1618 ]  . 
we believe that the recent recommendations of the international commission on radiological protection [ 19 ] are extremely clear with regard to this issue : the use of e is critical when e is used in a general manner to quantify the radiological risk of subjects who undergo medical exposure , in that in this case , the distribution of age and health of these subjects can be substantially different from similar distributions in workers and the population in general , on the basis of which the concept of e has been defined . 
sono stati aggiunti per confronto anche i dati dellanno 2000 , con la consapevolezza che in quella occasione il numero di prestazioni in regime di degenza stato estrapolato dai dati di 2 sole realt e che le modalit di calcolo sono state leggermente diverse rispetto a quelle degli anni successivi . in figura 3 si illustra graficamente la suddivisione pi recente ( anno 2006 ) dei contributi delle tre metodiche ( rc , tc e mn ) alla dose efficace collettiva ed al numero di prestazioni . 
si nota che la rc contribuisce per il 12% a s e per l83% alla frequenza di prestazioni : invece il contributo della tc a s circa 6 volte maggiore ( 78% ) e quello alla frequenza di prestazioni circa 6 volte minore ( 15% )  . infine , la mn contribuisce a s per il 10% e soltanto per il 2% al numero di prestazioni totali . radiol med ( 2010 ) 115 : 488498 collective effective dose frequency of examinations fig . 
3a , b contributi alla dose efficace collettiva ( a ) ed al numero di prestazioni ( b ) da parte di rc , tc e mn nel 2006 . continues to be very useful for a number of comparisons : doses delivered by different medical procedures ; similar radiological systems and practices performed in different centres and situated in different cities and countries ; and different imaging modalities applied to the same clinical procedure . 
since e has been used in this study for comparisons of this type , we believe that the adoption of this quantity ( and the quantity s derived from it ) is perfectly appropriate for studies of this type . once the metric has been defined for measuring the collected data , it is clear that the information regarding the different shares of total dose to the population of the different radiological examinations can provide useful indications with regard to the areas in which efforts would be best concentrated to reduce the dose or to most efficiently and effectively rationalise radiation protection in patients . 
it is therefore vital , especially for this imaging modality , that the appropriateness of each individual examination is guaranteed in that even a small reduction in the number of ct procedures could produce a significant reduction in dose to the population . 
more generally , optimisation plays a critical role in the discussione recentemente stato affrontato dalla comunit scientifica internazionale il problema della validit di continuare ad usare la grandezza fisica dose efficace come parametro per quantificare e studiare la radioprotezione del paziente [ 1618 ]  . 
riteniamo che le recenti raccomandazioni dellinternational commission on radiological protection [ 19 ] rappresentino un punto di estrema chiarezza relativamente a questa problematica : lutilizzo della dose efficace critico quando e viene usata in maniera generalizzata per quantificare il rischio radiologico degli individui sottoposti ad esposizioni mediche , in quanto in questo caso la distribuzione dellet e dello stato di salute di tali individui possono differire anche notevolmente dalle omologhe distribuzioni dei lavoratori e della popolazione in generale , in funzione delle quali il concetto di dose efficace stato definito . 
luso di e , per , continua ad essere molto utile per confrontare : dosi risultanti da procedure mediche diverse tra di loro ; tecnologie e pratiche radiologiche simili eseguite in strutture sanitarie differenti e situate in diverse citt e nazioni ; tecnologie diverse applicate ad una uguale procedura clinica . 
poich nel presente lavoro e stato usato esattamente per confronti come quelli appena 496 radiol med ( 2010 ) 115 : 488498 reduction and appropriate use of ionising radiation in diagnostic imaging , although placing particular attention on the justification of radiological practices ( i.e. , the reduction of unnecessary examinations ) undoubtedly has an even more significant impact on limiting the value of s and the percaput dose . the dose delivered to patients during radiological examinations largely depends on the type of examination ( and also on the equipment used ) , and therefore , the dose to the population can change with technological development . however , technological development does not always lead to a reduction in dose in that the possibility of performing some medical imaging procedures more easily or more quickly is accompanied by the risk of an unjustifiable increase in the number of examinations . the data gathered should not be seen as crystallised in time given the possibility that some information may be supplied even months after the end of the data collection campaign . 
it is therefore possible that some data are subsequently updated several times on the basis of the availability of new values directly supplied by the hospitals and that end up substituting the interpolated data . 
quality and reliability ( and therefore accuracy of the information supplied by each hospital ) has improved over time , in part thanks to the development of the culture of patient radiation protection mentioned above . 
when considering a reference year ( in our case , 2005 ) , this analysis reveals that the net patient inflow concerns less than 40 , 000 examinations and that with regard to ct , there is a net outflow ( i.e. , in 2005 , the number of citizens from emilia - romagna who left the region for these examinations was greater than the number who entered )  . evaluation of the net inflow in terms of total number of examinations recorded reveals that in general , the impact of patient mobility is < 3% of the estimated doses presented in this study . validity of the per - caput dose may also be debatable , as the distribution of diagnostic imaging examinations within the population is far from being homogeneous in that a small number of subjects undergo almost all of these procedures . 
nonetheless , the utility of this quantity essentially lies in the fact that it enables comparison of practices between countries with a similar level of health care [ 4 ]  . 
the table shows that the value of the dose per capita in the emilia - romagna region is in line with the values obtained in other evaluations descritti , si ritiene del tutto adeguata ladozione di questa grandezza ( e della grandezza derivata s ) per studi di questo tipo . una volta definita la metrica con cui misurare i dati raccolti , si evidenzia che le informazioni sul contributo differenziale dei diversi tipi di esami radiologici alla dose alla popolazione possono fornire utili indicazioni relativamente ai settori in cui pi opportuno concentrare gli sforzi per ridurre la dose oppure per razionalizzare nel modo pi efficiente ed efficace la radioprotezione dei pazienti . 
per quanto riguarda le prestazioni considerate nel presente lavoro , attualmente la tc ne rappresenta il 15% in termini di frequenza ma contribuisce per il 78% alla dose efficace collettiva della popolazione dellemilia - romagna dovuta ad esposizioni mediche : pertanto fondamentale , a maggior ragione in questa metodica , che sia garantita lappropriatezza dei singoli esami in quanto anche una piccola riduzione del numero di procedure tc eseguite rappresenta potenzialmente un elevato risparmio di dose alla popolazione . 
pi in generale , lottimizzazione gioca un ruolo importante nella riduzione e nellutilizzo appropriato delle radiazioni ionizzanti in radiodiagnostica , per sicuramente il dare una particolare attenzione alla giustificazione delle pratiche radiologiche ( cio , in ultima analisi , ridurre gli esami inutili ) ha un impatto ancora pi importante sul contenimento del valore di s e della dose efficace procapite . la dose erogata ai pazienti durante lesecuzione di esami radiologici dipende fortemente dalla tipologia dellesame ( ed anche dallapparecchiatura usata ) e quindi la dose alla popolazione pu cambiare con levoluzione tecnologica : questultima , per , non sempre porta ad una riduzione della dose , in quanto la possibilit di eseguire pi facilmente , o pi velocemente , alcune procedure radiodiagnostiche rischia di avere come conseguenza laumento non sempre giustificato del numero di esami . i dati raccolti non devono intendersi cristallizzati nel tempo in quanto possibile che alcune informazioni siano fornite anche diversi mesi dopo la fine temporale della campagna di raccolta : quindi possibile che alcuni dati vengano aggiornati successivamente pi volte in base al reperimento di nuovi valori , direttamente forniti dalle as , che vanno cos a sostituire quelli interpolati . 
la qualit e lattendibilit ( e quindi in ultima analisi laccuratezza delle informazioni fornite dalle as ) migliorata nel tempo , grazie anche allo sviluppo di quella cultura di radioprotezione del paziente sopra ricordata . 
it is thought that this type of procedure accounts for approximately 15%20% of the total dose , although an undoubtedly more accurate estimate can only be obtained once the relative dosimetric data and the number of procedures have been collected , a data collection campaign that the emiliaromagna region initiated this year . conclusions the constant monitoring of medical exposure to the population , in addition to being a requirement by law , is undoubtedly a highly useful tool for keeping diagnostic imaging procedures optimised without excessively weighing on the individual hospitals while at the same time using field data , not only theoretical calculations . 
in the setting of the diffusion of a culture of patient radiation protection , the next step should therefore be performing analyses of the type presented in this study but that also consider other procedures with a significant impact on patient dose , such as interventional radiological procedures . della banca dati asa , nella consapevolezza che esistono flussi di pazienti in ingresso ed in uscita dal territorio regionale . 
da questo approfondimento risulta che , prendendo un anno di riferimento ( nel nostro caso il 2005 ) , il saldo attivo di mobilit riguarda meno di 40000 prestazioni e che , per quanto riguarda le tc , il saldo passivo ( cio in quellanno il numero di cittadini emiliano - romagnoli che sono andati fuori regione per queste prestazioni stato maggiore di quelli che sono entrati )  . 
valutando il saldo attivo rispetto al totale delle prestazioni conteggiate , si evince che in generale la mobilit incide meno del 3% sulle stime di dose presentate in questo lavoro . la validit dellutilizzo della dose pro - capite pu essere un ulteriore oggetto di discussione , perch la distribuzione degli esami radiodiagnostici allinterno della popolazione non affatto omogenea , in quanto un numero esiguo di persone vengono sottoposte alla quasi totalit di tali procedure : per lutilit di questa grandezza risiede essenzialmente nel permettere il confronto di pratiche tra paesi che hanno un livello di cure sanitarie simile [ 4 ]  . 
si pu notare che il valore di dose pro - capite della regione emilia - romagna in linea con quelli ottenuti nelle altre valutazioni effettuate presso paesi con servizi sanitari nazionali ben sviluppati . la mancanza di informazioni relative alla radiologia interventistica impedisce di valutare la dose alla popolazione nella sua completezza : si ritiene che il contributo alla dose totale dovuto a questa tipologia di procedure sia dellordine del 15%20% , ma una stima sicuramente migliore sar ottenuta dopo la raccolta dei relativi dati dosimetrici e di frequenza delle prestazioni che la regione emilia - romagna ha iniziato ad effettuare da questanno . conclusioni il monitoraggio costante delle esposizioni mediche alla popolazione , oltre ad essere un obbligo di legge , sicuramente uno strumento utilissimo per mantenere ottimizzate le procedure radiodiagnostiche , senza pesare eccessivamente sulle singole as ed allo stesso tempo utilizzando dati raccolti sul campo e non soltanto calcolati teoricamente . lattenzione sempre maggiore data in questi anni allottimizzazione delle procedure ( ad esempio con luso dei livelli diagnostici di riferimento ) deve continuare ed allargarsi anche alla giustificazione delle procedure stesse ( ad esempio nel caso della tc )  . 
nieder springer - verlag , berlin , heidelberg , 2009 isbn 978 - 3 - 540 - 73231 - 0 published online : 30 march 2010 springer - verlag 2010 among the different types of cancers , head and neck is one of the most difficult to diagnose in its early stages and extremely difficult to treat : weapons against this type of neoplasm include surgery , radiotherapy , chemotherapy , chemo / radiotherapy , but all have pros and cons and drawbacks for patient quality of life ( qol )  . the aim of this book is to discuss and present to the reader most of all and most importantly to health - care providers the updated clinical and epidemiological research and results in this field . there are 28 short , decisive chapters divided into three domains : epidemiology and treatment outcome ; treatment techniques with potential impact on qol ; toxicity , quality of life , prevention , rehabilitation , and supportive care . management strategies , advantages and disadvantages of the different sorts of therapies , their possible benefits coupled with related toxicities inherent to each and their impact on qol are precisely presented and discussed . 
 the discussion is focused on how to prevent and avoid immediate or late sequelae such as the very frequent xerostomia , dysgeusia , dysphagia , and possible , severe hearing loss , mastoid necrosis , and blindness following radiotherapy or chemio / radiotherapy . hints are given on rehabilitation , supportive care and quality of life after finishing treatment . 
communication between the patient and health - provider ( often doctors are not properly trained in this most important aspect of their daily work , particularly when confronted with the task of announcing to a patient that his life is approaching its end ) and organized supportive care for patients and their families are presented in an easy to grip and unforgettable way . in conclusion , this is an important , impressive , relevant tra tutti i vari tipi di malattie neoplastiche , il cancro della testa e del collo tra i pi difficili da diagnosticare nelle sue fasi precoci e perci difficile da curare . 
le possibili armi a disposizione chirurgia , radioterapia , chemioterapia , chemio / radioterapia hanno tutte dei pro e dei contro , soprattutto svantaggi sulla qualit della vita ( qol ) del paziente . scopo del volume proprio quello di discutere e presentare al lettore in particolare a coloro che hanno in cura questi pazienti i risultati aggiornati dei dati clinici ed epidemiologici in questo campo . il volume diviso in 28 brevi ma succosi capitoli raccolti in tre campi : epidemiology and treatment outcome ; treatment techniques with potential impact on qol ; toxicity , quality of life , prevention , rehabilitation , and supportive care . nei singoli capitoli vengono presentate con chiarezza e discusse , con laiuto di ottime figure , tabelle e schemi , le strategie dei vari comportamenti terapeutici , i vantaggi e gli svantaggi degli stessi ed i loro possibili benefici , associati per anche alla tossicit riscontrabile in ciascuno di essi e di conseguenza sulla qualit della vita dei singoli pazienti . la discussione fa il punto su come prevenire ed evitare sequele immediate o tardive , purtroppo assai frequenti come xerostomia , disgeusia , disfagia , nonch sulle possibili e ben pi gravi perdite delludito , necrosi mastoidea , e cecit conseguenze dalla radio o chemio / radioterapia . un accento significativo posto sulla riabilitazione e sulla terapia di sostegno riguardo la qualit della vita dei pazienti una volta che si giunti al termine del ciclo terapeutico . 
vengono presentati a questo proposito , in modo chiaro , ben difficile da dimenticare le modalit di comunicazione e relazione tra il paziente ed il curante ( spesso i medici non sono stati preparati in modo appropriato nei loro studi e nella pratica quotidiana a confrontarsi con un paziente cui annunziare la prossima fine della vita ) nonch le strutture di supporto esterne sia per i pazienti che per le loro famiglie . in conclusione , questo un volume importante , valido e di grande effetto che dovrebbe essere letto e ben digerito da 502 radiol med ( 2010 ) 115 : 501502 book , that should be read and properly digested by all members of large specialized teams of experts who care for these patients , very often at the end of their life , due to the late discovery of the disease . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , universit di tor vergata , viale oxford 81 , 00133 roma , italy 2cattedra di cardiologia , dipartimento di medicina interna , universit di tor vergata , roma , italy correspondence to : c . 
per - patient analysis in the remaining 62 patients identified 24 cases ( 38.7% ) of negative ct findings ( no stenoses or stenoses < 50% ) , 35 cases of positive ct findings ( 56.4% ) with identification of the culprit lesion , two cases in which the culprit lesion was not identified and one patient with unconfirmed stenosis . 
lanalisi per paziente dei rimanenti 62 ha visto 24 pazienti ( 38 , 7% ) negativi allo studio tc ( stenosi assenti o < 50% ) , 35 pazienti ( 56 , 4% ) positivi , con identificazione della lesione culprit , 2 pazienti dove non stato possibile identificare la lesione culprit ed 1 paziente con stenosi non confermata ; sensibilit e specificit sono risultate del 94 , 6% e del 96% . 
lutilizzo della coronaro - tc nella pratica clinica , in questo tipo di emergenze , potrebbe incidere in maniera ragguardevole sui costi del sistema sanitario , stratificando i pazienti privi di patologia coronarica o di altra patologia e consentendone la dimissione in tempi immediati , senza necessit di ulteriori indagini diagnostiche . parole chiave tcms coronarografia virtuale sindrome coronarica acuta tc coronarica introduction introduzione acute chest pain is one of the most common and important causes of presentation to the emergency department ( ed ) in industrialised countries . 
in the usa , some 6 million people are evaluated for acute chest pain in the ed each year , and in italy , chest pain accounts for 6.5% of healthservice utilisation , a percentage that is progressively increasing . 
the causes of acute chest pain are many and characterised by different degrees of urgency and severity . however , the cause associated with the highest morbidity is no doubt acute coronary syndrome ( acs ) , including stelevation myocardial infarction ( stemi ) , non - st - elevation myocardial infarction ( nstemi ) and unstable angina ( ua ) [ 1 , 2 ]  . 
the diagnostic and therapeutic management of frank acs includes coronary angiography , which should be performed immediately in the case of stemi or deferred by 2448 h in the case of ua or nstemi . however , some patients for whom coronary angiography is deferred may develop a potentially fatal acute myocardial infarction ( ami ) within 48 h . 
on the other hand , a substantial number of acs patients evaluated with coronary angiography are found not to be affected by significant stenoses ( > 50% ) , so that coronary angiography is not followed by any interventional procedure . 
moreover , some patients with stenosis < 50% do not require coronary revascularisation and should be spared an invasive and unnecessary coronary examination that is not aimed at percutaneous angioplasty [ 3 , 4 ]  . 
negli usa ogni anno circa 6 milioni di persone vengono esaminate nei dipartimenti di emergenza per dolore toracico acuto ; in italia la percentuale di prestazioni sanitarie effettuate per dolore toracico si attesta attualmente intorno al 6 , 5% ed in progressivo aumento . 
le cause di dolore toracico acuto sono molteplici e caratterizzate da differenti gradi di urgenza e gravit , tuttavia quella che sicuramente rappresentata da una maggiore morbilit la sindrome coronarica acuta ( sca ) , che comprende linfarto stemi ( st elevation myocardial infarction ) , linfarto nstemi ( non st elevation myocardial infarction ) e lai ( angina instabile ) [ 1 , 2 ]  . 
liter diagnostico - terapeutico delle sca accertate prevede una procedura coronarografica , che deve essere immediata in caso di infarto stemi e che invece pu essere differibile di 2448 ore in caso di ai o infarto nstemi . tuttavia alcuni dei pazienti differiti possono andare incontro , nelle 48 ore , ad ima ( infarto miocardico acuto ) , talvolta anche fatale . 
bisogna considerare invece che un buon numero di pazienti con sca sottoposti a coronarografia non affetta da stenosi significative ( > 50% ) ed in questi casi la procedura coronarografica non seguita da step interventistico ; inoltre esistono pazienti con stenosi < 50% che non necessitano di rivascolarizzazione coronarica , ai quali sarebbe ottimale evitare un esame coronarografico invasivo ed inutile perch non finalizzato al trattamento angioplastico percutaneo [ 3 , 4 ]  . 
 unindagine diagnostica che consenta di differenziare precocemente i pazienti con sca di tipo nstemi e ai ( identificando la presenza di stenosi preocclusive o di trombosi endoluminali , nonch di coronarie prive di stenosi significative ) , che necessitano di una rivascolarizzazione durgenza , dai pazienti che invece possono essere differiti nelle 48 ore ( portatori di lesioni monovasali ) o non trattati ( stenosi assenti o < 50% ) potrebbe essere utile nella gestione delle sca , in particolare nei centri dove non disponibile un servizio di urgenza emodinamica . la tomografia computerizzata ( tc ) volumetrica 64 strati , con le sue caratteristiche di bassa invasivit e di radiol med ( 2010 ) 115 : 341353 equipped with emergency haemodynamic services . sixty - four - slice computed tomography ( ct ) , with its low level of invasiveness and high quality images of the coronary tree , has been shown to be a useful complement in the triage of patients with chest pain of possible ischaemic origin and especially in the diagnosis of acs [ 2 ]  . 
since 1998 when coronary imaging with 4 - slice multidetectorrow ct scanners ( mdct ) was first attempted technological advancements have dramatically improved the techniques spatial and temporal resolution , leading to a very high diagnostic potential in the study of the coronary arteries [ 5 ]  . 
 the purpose of our study was to assess the feasibility , sensitivity and specificity of 64 - slice ct in identifying haemodynamically significant stenoses ( > 50% ) of the coronary arteries in subjects with suspected acute coronary syndrome ( nstemi or ua ) by correlating the ct findings with the clinical event and data obtained with conventional coronary angiography ( cca )  . 
the aims of coronary ct angiography in this group of patients are twofold : ( 1 ) to exclude significant coronary stenoses , thereby sparing patients cca and guiding them towards exclusively medical therapy , and ( 2 ) to identify among patients with acs ( nstemi or ua ) those with preocclusive stenoses necessitating immediate revascularisation . materials and methods between november 2006 and december 2007 , 64 patients ( 38 men and 26 women ; mean age 65 years10 ) presenting to our hospitals ed with chest pain suggestive for acs were enrolled in this study . 
suspected unstable angina in the presence of angina - like chest pain of variable duration ( range 1030 min ) ; one or more associated symptom such as dyspnoea , fatigue , nausea , cold sweat ; absence of st - segment elevation and / or st - segment depression and / or t - wave inversion ( ecg ) ; negative cardiac on electrocardiography enzymes ( troponin t < 0.2 ng / ml ; troponin i < 0.003 ng / ml ; myoglobin < 90 ng / ml ; creatine kinase - mb < 2% of total ) elevata qualit delle immagini dellalbero coronarico , si rivelata un utile complemento nel triage dei pazienti con dolore toracico di possibile origine ischemica ed in particolare nella diagnosi di una sca [ 2 ]  . 
dal 1998 , anno in cui si effettuarono i primi tentativi di studi coronarici con apparecchiature tc multidetettore ( tcmd ) a 4 strati , ad oggi sono state compiute innovazioni tecnologiche tali da consentire un miglioramento decisivo della risoluzione spaziale e temporale e potenzialit diagnostiche notevolmente elevate per lo studio delle coronarie [ 5 ]  . 
 lobiettivo del nostro studio valutare la fattibilit , la sensibilit e la specificit della tc volumetrica a 64 file di detettori nellidentificazione di stenosi emodinamicamente significative ( > 50% ) delle arterie coronarie in soggetti con sospetta sca di tipo nstemi e ai , correlando il reperto tc con levento clinico del paziente e confrontando successivamente i dati ottenuti con quelli della coronarografia convenzionale ( cc )  . 
nellarco di 24 ore dalla presentazione in ps , questi pazienti ( dai quali era stato ottenuto il preventivo consenso informato per linserimento nel presente studio ) sono stati sottoposti , presso il nostro dipartimento , a tc volumetrica a 64 strati e ad un successivo esame coronarografico . pi precisamente , ai pazienti che attendevano di effettuare la coronarografia convenzionale su indicazione clinica , per valutare la presenza o meno di una lesione ostruttiva dellalbero coronarico , stato chiesto se volevano sottoporsi ad una preliminare indagine angio - tc del cuore . 
lo studio stato concordato con i medici del ps e con i cardiologi ed ha ricevuto lapprovazione del comitato etico locale ; tutti i pazienti hanno fornito il proprio consenso informato allesame dopo chiara spiegazione dei benefici e potenziali rischi . 
pazienti con sospetta angina instabile in presenza di dolore toracico anginoso di durata variabile ( range 1030 minuti ) , uno o pi sintomi associati ( dispnea , astenia , nausea , sudorazione algida ) , allecg assenza di sopraslivellamento del tratto st e / o presenza di sottoslivellamento del tratto st e / o inversione della onda t , enzimi cardiaci negativi ( troponina t < 0 , 2 ng / ml ; troponina i < 0 , 003 ng / ml ; mioglobina < 90 ng / ml ; creatinchinasi ( ck ) - mb < 2% ck totale ) ; 2 . 
pazienti con sospetta sca di tipo nstemi in presenza di dolore toracico anginoso per pi di 30 minuti , sintomi 344 radiol med ( 2010 ) 115 : 341353 2 . 
suspected ( nstemi ) acs in the presence of angina - like chest pain for > 30 min ; associated symptoms such as dyspnoea , heavy fatigue , palpitations , cold sweat , nausea , vomiting ; absence of st - segment elevation , presence of st - segment depression and / or t - wave inversion ; positive cardiac enzymes . patients with absolute contraindications to ct angiography , such as serious arrhythmia , known allergy to iodinated contrast agents , kidney failure , respiratory failure or severe cardiac decompensation were excluded from the study . the following known risk factors for coronary heart disease were identified in the study population : family history of ami in 17.2% ( 11 / 64 ) , smoking in 29.7% ( 19 / 64 ) , dyslipidaemia in 59.3% ( 38 / 64 ) and arterial hypertension in 67.1% ( 43 / 64 )  . 
all patients underwent coronary ct angiography with a 64 - slice ct scanner ( lightspeed vct , general electric medical systems , milwaukee , wi , usa ) and retrospective synchronisation technique . 
the ct study was performed on average 5 h ( 3 h ) prior to cca . a preliminary unenhanced scan was done to determine the scan extent and calculate the calcium score ( smartscore protocol )  . 
the acquisition stack extended from the ascending aorta superiorly ( approximately 1 cm above the tracheal bifurcation ) and the heart apex inferiorly ( lower portion of the lowest hemidiaphragm ) , therefore enabling evaluation of the entire cardiac volume . 
scan parameters for the unenhanced baseline scan were beam collimation 82.5 mm , slice thickness 2.5 mm , table feed 1 cm / 4 slices , tube rotation speed 0.35 s , tube voltage 120 kv , intensity 300 ma , fov 25 cm , craniocaudal scan direction . 
a second image stack was then acquired after intravenous administration of iodinated contrast material using a dual - head automated injector ( stellant , medrad , pittsburgh , pa , usa )  . 
a dose of 80 ml of nonionic iodinated contrast material ( iomeron 400 , bracco , milan , italy ) was administered through an 18gauge needle cannula placed in an antecubital vein , followed by 40 ml of saline solution , both at a rate of 5 ml / s . 
parameters for the contrast - enhanced scan were beam collimation 640.625 mm , slice thickness 0.625 mm , reconstruction increment 0.625 mm , table feed 2.9 mm / rotation , tube rotation 0.35 s , tube voltage 120 kv , intensity 400800 ma , fov 25 cm , craniocaudal scan direction . 
 image reconstruction was carried out using three temporal windows at 70% , 75% and 80% of the cardiac associati ( dispnea , astenia profonda , palpitazioni , sudorazione algida , nausea , vomito ) , allecg assenza di sopraslivellamento del tratto st , presenza di sottoslivellamento del tratto st e / o inversione dellonda t ; enzimi cardiaci positivi . sono stati esclusi dalla presente valutazione i pazienti nei quali esistevano controindicazioni assolute allesecuzione dellangio - tc , quali : presenza di gravi aritmie , allergia nota al mezzo di contrasto organoiodato , insufficienza renale , insufficienza respiratoria e scompenso cardiaco di grado severo . per quanto riguarda i fattori di rischio noti per cardiopatia coronarica , sono stati riscontrati nella popolazione di studio : familiarit per ima nel 17 , 2% ( 11 / 64 ) , fumo attivo nel 29 , 7% ( 19 / 64 ) , dislipidemia nel 59 , 3% ( 38 / 64 ) e ipertensione arteriosa nel 67 , 1% ( 43 / 64 )  . 
tutti i pazienti sono stati sottoposti a studio angio - tc coronarico mediante tc volumetrica a 64 strati ( lightspeed vct , general electric medical systems , usa ) e tecnica di sincronizzazione di tipo retrospettivo . 
lo studio tc stato effettuato in media 5 ore ( 3 ore ) prima della coronarografia . preliminarmente stata effettuata una scansione senza mezzo di contrasto che permette di definire con precisione il punto dinizio e fine del volume da includere nellacquisizione e di calcolare il calcium score ( protocollo smartscore )  . 
il pacchetto di acquisizione include laorta ascendente superiormente ( 1 cm circa al di sopra della biforcazione tracheale ) e la punta del cuore inferiormente ( porzione inferiore dellemidiaframma pi basso ) , cos da poter esaminare lintero volume cardiaco . 
in questa fase pre - contrastografica , i principali parametri di scansione sono stati : collimazione del fascio 82.5 mm , spessore di strato 2 , 5 mm , traslazione del lettino di 1 cm ogni 4 acquisizioni da 2 , 5 mm , velocit di rotazione del tubo radiogeno 0 , 35 s , voltaggio del tubo 120 kv , intensit del fascio di radiazioni 300 ma , campo di vista ( fov ) 25 cm , direzione di scansione cranio - caudale . 
si quindi proceduto allacquisizione di un secondo pacchetto dopo somministrazione per via endovenosa di mezzo di contrasto organo - iodato , mediante un iniettore automatico a doppia testa ( stellant , medrad , pittsburgh , pa , usa ) , attraverso una agocannula di 18 gauge posizionata in una vena antecubitale del braccio . 
sono stati somministrati 80 ml di mezzo di contrasto organo - iodato non ionico ( iomeron 400 , bracco , milano , italia ) , seguiti da infusione di 40 ml di soluzione fisiologica , entrambi ad un flusso di 5 ml / s . 
nella fase contrastografica , i principali parametri di scansione sono stati : collimazione del fascio 640 , 625 mm , spessore di strato 0 , 625 mm , incremento di ricostruzione 0 , 625 mm , velocit di avanzamento del lettino 2 , 9 mm / rotazione , velocit di rotazione del tubo radiogeno 0 , 35 s , voltaggio del tubo 120 kv , intensit del fascio di radiazioni tra 400 e 800 ma , fov 25 cm , direzione di scansione craniocaudale . 
 la ricostruzione delle immagini stata eseguita con lutilizzo di tre finestre temporali fissate al 70% , al 75% e all80% del ciclo cardiaco , periodo compreso tra due onde radiol med ( 2010 ) 115 : 341353 cycle , corresponding to the r - r interval or midto end diastole . 
in the event of motion artefacts due to sudden changes in heart rate , other reconstruction windows were used ( from 40% to 65% of the r - r cycle )  . consecutive r - r del tracciato ecg , corrispondenti alla fase meso - telediastolica . 
nel caso di artefatti da movimento , dovuti ad un aumento o ad una modificazione improvvisa della frequenza cardiaca durante lacquisizione , sono state utilizzate altre finestre di ricostruzione ( dal 40% al 65% del ciclo r - r )  . conventional coronary angiography coronarografia convenzionale cca was performed using a philips flat - panel system ( medical philips system , the netherlands ) with multiple projections . 
a value 50% was considered a significant stenosis . image analysis in the per - patient analysis , ct results were judged as positive for coronary disease when a stenosis > 50% was identified in at least one vessel , and negative when a stenosis < 50% was found in all vessels . 
in the event of multiple stenoses in the same patient and in the same vessel , the most extensive and narrowest stenosis was selected for comparison with cca , i.e. 
in the per - vessel analysis , each vessel was judged as negative for coronary disease in the presence of one stenosis < 50% or multiple stenoses < 50% , and positive in the presence of one stenosis > 50% or multiple stenoses < 50% . statistical analysis all data were entered into a database for statistical processing . 
during the first phase of the study , involving the analysis of the entire lesame coronarografico convenzionale stato effettuato mediante un apparecchio flat panel philips ( medical philips system , olanda ) usando multiple proiezioni . 
le stenosi sono state valutate come percentuale del diametro di riferimento determinato in due proiezioni ortogonali utilizzando la media dei due campioni come valore finale . un valore 50% ha indicato una stenosi significativa . analisi delle immagini nellanalisi per paziente , il risultato della coronaro - tc stato giudicato : positivo per coronaropatia in presenza di una stenosi > 50% in almeno un vaso ; negativo per coronaropatia in presenza di una stenosi < 50% in tutti i vasi . 
nel caso di stenosi multiple nello stesso paziente e nello stesso vaso stata considerata , per il confronto con la coronarografia , la lesione pi estesa e stenosante , quella cio probabilmente responsabile dellevento acuto ( culprit lesion ) , anche in base ai criteri elettrocardiografici . nellanalisi globale per coronaria , ciascun vaso stato giudicato : negativo per coronaropatia , in presenza di una stenosi < 50% o di multiple stenosi < 50% ; positivo per coronaropatia , in presenza di una stenosi > 50% o di multiple stenosi < 50% . analisi statistica tutti i dati sono stati inseriti in un data - base computerizzato per poi essere trattati statisticamente . 
i dati sono stati espressi come media pi una deviazione standard o come percentuale . sono state calcolate sensibilit , specificit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) per la valutazione della stenosi significativa confrontando cc con tcmd . 
durante la prima fase dello studio , che ha previsto lanalisi di tutto lalbero coronarico nellidentificazione e nel grading delle stenosi coronariche , 2 pazienti ( 3 , 1% ) sono stati totalmente esclusi . 
le cause dellesclusione sono state ricondotte ad artefatti da movimento in 1 paziente ( 1 , 5% dei casi ) , 346 radiol med ( 2010 ) 115 : 341353 fig . 
 coronary tree to identify and grade the coronary stenoses , two patients ( 3.1% ) were excluded : one patient ( 1.5% ) because of motion artefacts due to an increase in heart rate of more than 10 bpm during the acquisition , and the other ( 1.5% ) because of respiratory artefacts . 
in particular , the lesions were imputabili allinnalzamento della frequenza durante lacquisizione ( aumento della frequenza tra inizio e fine acquisizione superiore ai 10 bpm ) e in 1 paziente ( 1 , 5% dei casi ) ad artefatti da respiro . 
2a - d paziente con sintomi da sindrome coronarica acuta con presenza di multiple placche aterosclerotiche di varia natura a carico della circonflessa ( a , b ) e della coronaria destra ( c , d ) con la stenosi di maggiore entit a livello della circonflessa ( freccia rossa )  . 
in two patients ( 3.2% ) , the lesion could not be identified owing to the presence of large concentric wall calcifications ( n = 1 ; 1.6% ) and multiple similar stenoses in the same branch ( n = 1 ; 1.6% ) ( false - negative results )  . 
in one patient ( 1.6% ) ( stenosis of the middle segment of the lad ) , the ct finding of significant stenosis was not confirmed at cca ( false positive )  . 
in 2 pazienti ( 3 , 2% ) non stato possibile identificare la lesione per la presenza di estese calcificazioni parietali concentriche ( in 1 caso , 1 , 6% ) e per la presenza di multiple stenosi simili nel medesimo ramo ( nellaltro caso , 1 , 6% ) ( falsi negativi )  . 
in 1 paziente ( 1 , 6% , stenosi del tratto medio dellarteria discendente anteriore ) il riscontro tc di stenosi significativa non stato confermato dal reperto coronarografico ( falso positivo )  . 
in relazione alla presenza di 2 falsi negativi e 1 falso positivo , lanalisi per paziente ha mostrato sensibilit 94 , 6% , specificit 96% , vpp 97 , 2% e vpn 92 , 3% . nellanalisi globale per coronaria , considerando nel computo complessivo i 3 principali rami coronarici , abbiamo osservato nel totale di 186 vasi , che 17 vasi ( 9 , 1% ) sono risultati non valutabili per presenza di artefatti da movimento ; in particolare 8 ( 47% ) a livello dellarteria coronaria destra , 6 ( 35 , 2% ) a livello dellarteria circonflessa e 3 ( 17 , 6% ) a livello dellarteria discendente anteriore.61 vasi ( 32 , 8% ) hanno rivelato stenosi tc > 50% , dato confermato allesame coronarografico ( veri positivi )  . 
tc multistrato ( a - e ) e coronarografia ( f ) mostrano reperti concordanti . presence of motion artefacts ; in particular , eight ( 47% ) in the rca , six ( 35.2% ) in the lcx and three ( 17.6% ) in the lad . 
a total of 61 vessels ( 32.8% ) had stenoses > 50% at ct , a finding confirmed by cca ( true positives ) ; seven vessels ( 3.7% ) with stenoses > 50% at ct were found to have nonsignificant lesions at cca ( false positives ) , three ( 1.6% ) with nonsignificant stenoses ( < 50% ) at ct had stenoses > 50% at cca ( false negatives ) , whereas in 98 ( 52.6% ) neither ct nor cca identified stenoses ( true negatives )  . 
alla luce di questi risultati , lanalisi globale per coronaria ha mostrato : sensibilit 95 , 3% , specificit 93 , 3% , vpp 89 , 7% e vpn 97% . discussione le sca rappresentano una sfida impegnativa per il medico , in quanto il numero di pazienti che si presenta al pronto soccorso con questo tipo di sintomatologia in costante aumento . 
where these noninvasive studies indicate a high risk for steno - obstructive coronary disease , cca becomes essential for both diagnostic and therapeutic purposes ( percutaneous angioplasty and stenting )  . 
nonetheless , although cca remains the reference standard in the study of coronary arteries , it is an invasive procedure that provides no information on wall structure or plaque composition . 
in addition , it may lead to an underestimation of disease severity , especially sulla base di informazioni derivanti da anamnesi , esame obiettivo , ecg e dosaggio degli enzimi cardiaci [ 6 ] ; qualora queste indagini non invasive diano riscontro di un indice di rischio elevato per patologia steno - ostruttiva dellalbero coronarico , risulta indispensabile il successivo ricorso alla coronarografia , sia con finalit diagnostiche che eventualmente terapeutiche ( angioplastica percutanea e stenting )  . 
tuttavia la coronarografia , pur rappresentando tuttora la tecnica di riferimento per lo studio delle coronarie , una procedura invasiva che non permette di acquisire informazioni sulla struttura delle pareti arteriose e sulla composizione delle placche aterosclerotiche ; inoltre , talvolta pu portare a sottovalutare la gravit della malattia , particolarmente in segmenti con stenosi eccentriche ed in presenza di rimodellamento vascolare positivo . per queste motivazioni , e per le consistenti implicazioni socio - economiche associate , sono sorte delle forti 350 radiol med ( 2010 ) 115 : 341353 fig . 
5a - d severe stenosis ( arrow ) of the left anterior descending artery in a patient with acute myocardial infarction ( non - st - elevation myocardial infarction ) treated with immediate revascularisation . 
 with new - generation 64 - slice mdct scanners capable of acquiring 4 cm of body volume simultaneously with a collimation thickness of 0.625 mm per gantry rotation at a rotation speed of 320 ms , the entire cardiac volume can be imaged in only 5 s . 
such a short acquisition time overcomes aspettative circa lindividuazione di una tecnica di studio panoramica e non invasiva dellalbero coronarico , di rapida e semplice esecuzione , tale da registrare un impatto positivo sul trattamento e sulla prognosi di questa patologia . 
la tcmd si imposta come una delle metodiche non invasive pi promettenti per il riconoscimento , la quantificazione e la caratterizzazione della placca coronarica nellambito della valutazione del rischio [ 712 ]  . 
 con lintroduzione dellultima generazione di tcmd a 64 strati , che permettono di acquisire contemporaneamente 4 cm di volume corporeo con uno spessore di collimazione di 0 , 625 mm per ogni rotazione del gantry e una velocit di rotazione di 320 ms , possibile acquisire lintero volume cardiaco in soli 5 secondi . 
la durata di acquisizione cos breve consente di risolvere alcuni problemi che , nelle precedenti generazioni , determinavano linsorgenza di artefatti da movimento inficianti la valutazione di alcuni segmenti / arterie ; infatti linnalzamento della frequenza in fase di acquiradiol med ( 2010 ) 115 : 341353 some problems that led to motion artefacts with previousgeneration equipment . 
an increase in heart rate during the acquisition becomes extremely rare , as this has been shown to occur after 1015 s of initial stability ; the likelihood of arrhythmias ( extrasystoles ) occurring during a 5 - s acquisition is extremely low ; and finally , all patients , including those with serious respiratory insufficiency , are normally able to maintain a breath - hold of at least 5 s . 
 a number of published studies investigating the 64 - slice ct for studying the coronary tree , with cca used as the reference standard , reported high sensitivity and specificity values , with an npv exceeding 95% in detecting haemodynamically significant stenoses [ 1318 ]  . 
our aim was to assess the potential of the technique to identify , among true acs , cases of nstemi and ua , which , like those of stemi , require immediate revascularisation . 
 with regard to risk stratification , we are addressing a new field of study that has been investigated by a limited number of studies only [ 15 , 1722 ]  . 
the task of mdct in this group of patients should be to distinguish at an early stage those cases that necessitate emergent revascularisation ( presence of preocclusive stenoses , intraluminal thrombosis ) from those for whom cca can instead be deferred by 48 h ( with moderately stenosing lesions )  . results of this preliminary study , based on a per - patient and per - vessel analysis , showed that the potential and capability of mdct to detect the culprit lesion are very high , with sensitivity ( 94.6% ) and specificity ( 96% ) values approaching those of cca . 
in the two cases of falsenegative results , although the culprit lesion could not be identified immediately owing to extensive calcifications and multiple stenoses in the same vessel , we were nonetheless able to identify the vessel responsible for the symptoms . 
in 13 cases , sizione diventa un evento estremamente raro perch , dalle esperienze fatte , si riscontrato che nella quasi totalit dei casi interviene dopo 1015 secondi di iniziale stabilit ; inoltre assai bassa la possibilit che in 5 secondi di acquisizione intervengano aritmie ( extrasistoli ) ; infine tutti i pazienti , anche quelli con grave compromissione respiratoria , mantengono in genere almeno 5 secondi di apnea . 
la progressiva evoluzione delle apparecchiature ha consentito anche di ridurre notevolmente la quantit di mezzo di contrasto da somministrare al paziente durante lesecuzione degli esami . al momento attuale , sono stati pubblicati vari studi riguardanti lo studio coronarico mediante tc a 64 file di detettori , che mostrano , usando come standard di riferimento la coronarografia convenzionale , elevati valori di sensibilit e di specificit , con un valore predittivo negativo superiore al 95% nel riconoscimento di stenosi emodinamicamente significative a carico dei rami coronarici [ 1318 ]  . il nostro studio ha valutato , mediante tc volumetrica a 64 file di detettori , 64 pazienti in attesa di essere sottoposti a coronarografia per sospetta sca . 
si sono volute esaminare le potenzialit della tcmd a 64 strati in queste tipologie di pazienti , nel riconoscere , nellambito delle vere sca , quelle di tipo nstemi e lai che necessitano , parimenti allo stemi , di una rapida rivascolarizzazione . per quanto riguarda la stratificazione del rischio , ci troviamo di fronte ad un nuovo oggetto di studio e sono ancora pochi i lavori in letteratura indirizzati verso questo scopo [ 15 , 1722 ]  . 
normalmente nei dipartimenti di emergenza , in presenza di un paziente gi diagnosticato come affetto da ai o sca di tipo nstemi , il protocollo prevede leffettuazione di un esame coronarografico al fine di identificare la stenosi culprit , ovvero la stenosi pi significativa nel vaso indicato dallecg che risulta essere quella probabilmente responsabile della sintomatologia . 
il compito della tcmd in questo tipo di pazienti dovrebbe essere quello di differenziare precocemente i soggetti che necessitano di una rivascolarizzazione durgenza ( presenza di stenosi preocclusive , trombosi endoluminale ) , da quelli che invece possono essere differiti nelle 48 ore ( lesioni modestamente stenosanti )  . 
dai risultati ottenuti in questo nostro lavoro preliminare , attraverso lanalisi sia per paziente che per coronaria , emerso che le potenzialit e le capacit della tcmd di evidenziare la lesione culprit , risultano essere estremamente elevate , con valori di sensibilit ( 94 , 6% ) e specificit ( 96% ) che si avvicinano a quelli dellesame coronarografico . 
nei 2 pazienti risultati come falsi negativi , se da un lato vero che non stato possibile identificare direttamente la lesione culprit , per la presenza di estese calcificazioni e di multiple stenosi interessanti il medesimo vaso , dallaltro si comunque riusciti a riconoscere il vaso affetto dalla patologia responsabile della sintomatologia in atto . 
this noninvasive approach in fact modifies the treatment strategy , enabling cca to be omitted in patients with stenoses < 50% who will benefit from exclusively anticoagulant and fibrinolytic therapy . finally , mdct proved very useful in characterising and managing long - term risk by identifying patients who , although not necessitating emergent procedures , had stenoses < 50% due to fibrofatty plaque , an indication for cholesterol - lowering treatment with fibrates and statins . effettuata prima dellesame coronarografico , ha modificato loutcome del paziente ; in particolare , ha permesso di eseguire una procedura di rivascolarizzazione in urgenza in pazienti stabili ( nstemi ) nei quali , tuttavia , la lesione culprit era preocclusiva , riducendo cos il rischio di una successiva complicanza , come un reinfarto acuto sul vaso di interesse . lelevato valore predittivo negativo ottenuto per coronaria e per paziente testimonianza di come la tc multistrato pu svolgere in questo gruppo di pazienti un altro importante ruolo : escludere patologia vasale > 50% e quindi evitare anche nel paziente acuto esami coronarografici negativi ovvero non seguiti da step terapeutico . 
questo tipo di approccio non invasivo modifica di fatto il trattamento terapeutico consentendo di evitare la coronarografia a pazienti con stenosi < 50% e permettendo di instaurare esclusivamente terapia anticoagulante e fibrinolitica . inoltre , la tcmd si rivelata molto utile nella caratterizzazione e nella gestione del rischio a lungo termine , identificando quei pazienti che pur non necessitando di un trattamento durgenza , presentavano una stenosi fibrolipidica < 50% e quindi unindicazione ad una terapia ipocolesterolemizzante con fibrati e statine . conclusions sixty - four - slice mdct , with its high npv , enables immediate exclusion of significant coronary disease not deserving intravascular or surgical treatment , and stratification of acs patients with nstemi and ua by identifying those at greater risk and thus requiring emergent revascularisation . therefore , 64 - slice mdct is a feasible and reliable technique , even in emergency settings , where it provides a correct early prognostic classification of acs patients , allowing treatment to be planned in the most appropriate way . 
this leads to a lower number of invasive examinations and a faster diagnostic workup . conclusioni alla luce di quanto scritto , la tc a 64 strati , avendo elevato vpn , consente unimmediata esclusione di malattia coronarica significativa , non meritevole di un trattamento endovascolare o chirurgico , e permette inoltre di stratificare i pazienti con sca di tipo nstemi e ai , identificando precocemente quelli a rischio pi elevato che richiedono una rivascolarizzazione in urgenza . 
la tc a 64 strati risulta , quindi , una metodica applicabile ed affidabile anche in condizioni di emergenza consentendo un corretto e precoce inquadramento prognostico della sca nelle sue differenti espressioni , per modulare di conseguenza lintervento terapeutico nel modo pi appropriato . 
sartor springer - verlag , berlin , heidelberg , 2009 isbn 978 - 3 - 540 - 22097 - 8 published online : 30 march 2010 springer - verlag 2010 when the reader arrives to the last lines of the last chapter of this book he / she should be tempted to say : ill perform some of the procedures described in the 18 chapters . just give me the patients and the equipment and ill show you what i can do . 
easily said , not as easy to translate this thought into reality . this book , in a way , resembles a small bible , devoted to percutaneous intervention , in all its multifaceted aspects , and is one of the few on the market to update with the latest conquests the matter of percutaneous musculoskeletal procedures . 
a great deal of experience comes from those ( all internationally known and reputed experts ) who wrote the chapters delineating the pros and cons of the various musculoskeletal procedures . 
procedures intended to heal osteoporotic fractures , bone metastases or vascular malformations as well as acute or chronic low back pain or just to be used as biopsy tools are thoroughly described . the introductory chapter deals with basic and novel guidance techniques . 
most of the following chapters delineate how to perform all types of procedures according to clinical presentation , from bone biopsy to spinal facet and sacroiliac joint injection , to discography , joint injection , cementoplasty and kyphoplasty , cysts ( particularly in paediatric age patients ) or tumour management , and painful shoulder management . 
the last chapters deal with vascular lesions and the use of ultrasound in the musculoskeletal domain showing , in detail how ultrasound can be very successfully employed in foreign body retrieval , abscess aspiration or tendon problems . as indicated above is not easy to translate thought into reality : those who deal with these sorts of techniques must be highly trained and able to immediately recognize when a procedure must be terminated due to its possible negaarrivando alla fine di questo volume il lettore tentato di dire o pensare : mi sento in grado di eseguire alcune delle manovre descritte nei suoi 18 capitoli . 
facile da dire , difficile per tradurre nella pratica questo pensiero o intendimento . questo volume in qualche modo rappresenta una piccola bibbia dedicata alle procedure interventistiche percutanee in tutti i loro multipli aspetti ed uno dei pochi sul mercato che aggiorna largomento con le ultime conquiste in materia . una notevole messe di esperienza pratica viene messa in campo da coloro ( per la maggior parte esperti di fama internazionale ) che hanno scritto i vari capitoli delineando anche i pro ed i contro delle varie manovre di interventistica muscolo - scheletrica . 
le procedure destinate ad intervenire sulle fratture da osteoporosi , metastasi scheletriche , malformazioni vascolari , dolori acuti e cronici del terzo inferiore del rachide o solo da utilizzare come semplici biopsie sono ben descritte in ogni loro dettaglio . il capitolo introduttivo descrive gli elementi di base ed i consigli circa le differenze modalit tecniche impiegabili . 
la maggior parte dei capitoli successivi descrive tra laltro come eseguire , in funzione della presentazione clinica , ogni tipo di procedura in particolare dalla biopsia ossea , alliniezione delle superfici articolari e della articolazioni sacro - iliache , alla discografia , alliniezione endoarticolare , alla cementoplastica e cifo - plastica , al trattamento delle cisti ( soprattutto in et pediatrica ) o dei tumori ossei , od al trattamento della spalla dolorosa . 
gli ultimi capitoli trattano poi delle malformazioni vascolari e dellimpiego degli ultrasuoni nel campo della patologia muscolo - scheletrica dimostrando in particolare come il loro impiego pu essere di grande utilit nella localizzazione ed asportazione dei corpi estranei , oltre che nel drenaggio di ascessi o nella patologia tendinea . come scritto sopra non facile tradurre il buon pensiero in realt pratica . 
coloro infatti che devono trastullarsi con questo tipo di metodiche devono essere ben preparati , allenati e capaci di rendersi conto quando una procedura debba essere immediatamente sospesa in moda tale da evitare conseguenze negative per il paziente , in particolare in quelle riguardanti il rachide . 500 radiol med ( 2010 ) 115 : 499500 tive consequences to the patient , especially during spinal procedures . 
a cohort of very impressive radiological images , detailed anatomical images and detailed procedures enrich and clarify the text . clearly those who already are interventional radiologists will find the book useful and a complementary tool in their daily activity . 
general or musculoskeletal radiologists and orthopaedic surgeons will enhance their knowledge and thus be able to properly use or guide possible musculoskeletal interventions providing benefit and improved outcome for their patients . 
una gran quantit di immagini radiologiche di grande qualit e di immagini anatomiche che seguono nei dettagli le varie tappe delle procedure arricchiscono e rendono chiaro e comprensibile ci che descritto nel testo . chiaramente coloro che gi lavorano nel campo della radiologia interventistica muscolo - scheletrica e non , troveranno il volume utile strumento complementare nella loro attivit quotidiana . 
ghanei , tel : + 98 - 218 - 8600067 , fax : + 98 - 218 - 8600067 , e - mail : m.ghanei@bmsu.ac.ir received : 6 may 2009 / accepted : 26 june 2009 / published online : 30 january 2010 springer - verlag 2010 abstract purpose . 
three groups of patients with sulfur - mustard - induced lung injury ( bo ) , severe chronic asthma ( resistant asthma ) and smoking habit , respectively , were recruited . 
numerosi precedenti studi di anatomia patologica hanno dimostrato come la bronchiolite obliterante ( bo ) sia la conseguenza a lungo termine pi frequente allesposizione alle mostarde azotate ( iprite )  . 
sono stati reclutati tre gruppi di pazienti , rispettivamente affetti da bronchiolite obliterante indotta da mostarde azotate ( bo ) , affetti da asma cronica ( asma refrattaria ) e fumatori . 
there is no common consensus about the pathophysiological basis of chronic pulmonary disease caused by mustard gas , but bronchiolitis obliterans ( bo ) has been proposed as the underlying cause [ 1 ]  . 
 airway remodelling is often considered to contribute to the element of irreversible airflow obstruction , which is a feature of some patients with asthma , bo and chronic obstructive pulmonary disease [ 2 ]  . 
lung diseases such as resistant asthma and cigarette smoking can change the structure of the small airways and cause irreversible airflow obstruction and thus interfere with proper diagnosis of mustard lung by causing similar clinical features . 
highresolution computed tomography ( hrct ) may reveal these abnormalities in symptom - free patients as well [ 3 ]  . different studies have reported hrct findings , but these studies were limited to a single disease or compared the diseases with healthy individuals [ 46 ]  . 
 in this study , we attempted to identify hrct features that may help in differentiating between mustard lung ( as a subtype of bo syndrome ) , resistant asthma and lung injuries due to cigarette smoking . azotate , lasma refrattaria ed il danno polmonare indotto dal fumo . parole chiave hrtc asma bronchiolite obliterante mostarde azotate mustard gas during the iran - iraq conflict in 1988 . 
they were all from sardasht , a city in western iran , and were randomly selected from the medical records available at our university hospital that provides tertiary medical care and maintains a large database of patients exposed to chemical warfare agents during the war . 
 group 2 : patients with severe chronic asthma ( resistant asthma ) thirty consecutive patients with documented resistant asthma according to the american thoracic society definition [ 7 ] were chosen from our pulmonary clinic . 
inclusion criterion was a need for permanent treatment ( > 50% in year ) with high - dose orally administered or inhalant steroids to remain in a mild or moderate phase . 
exclusion criteria were gastrooesophageal reflux disease and sinusitis . group 3 : smokers this group consisted of patients referred to the pulmonary clinic with various respiratory problems , especially dyspnoea and cough , and a history of smoking . 
 group 1 : sulfur - mustard - induced lung injury ( bronchiolitis obliterans ) study design and procedure participants were patients suffering from pulmonary disorders due to previous exposure to a single high dose of sulfur for the 90 patients in the three groups ( bo , resistant asthma and smokers ) , a patient history , complete physical examination and pulmonary function tests ( pft ) were performed on radiol med ( 2010 ) 115 : 413420 referral to the pulmonary clinic . 
another form was created in which hrct findings were documented . all hrct scans were obtained at near total lung capacity , with breath - holding rehearsed before commencement of the scan . 
patients were imaged with a section thickness of 1.0 mm with 10 mm intervals in the supine position using a high speed advantage scanner ( general electric medical system , milwaukee , wi , usa )  . 
images were reconstructed using the bone algorithm and were viewed at a window level of 450 and window width of 1 , 400 hu , which is the best choice for viewing lung images [ 8 ]  . 
intraand interrater variability parameters were not measured , but error probability is assumed to be low due to high interobserver agreement of hrct images . hrct aspects investigated in this study were : 1 . 
for these two patterns , both lungs were divided into three parts ( upper , middle and lower ) , and in each part , images were separately observed in terms of extent of involvement ( < 25% = negative ; > 25% = positive )  . emphysema was categorised as centrilobular , panacinar and paraseptal . 
other complications such as ground - glass pattern , mucoid impaction , bulla , atelectasis , narrowing and parenchymal nodule were evaluated subjectively and the results entered in the provided forms . statistical analysis data were analysed using spss software version 15 . 
the cumulative frequency of all findings is summarised in table 6 . discussion different studies have reported hrct findings in several groups similar to our groups [ 1012 ] , but these studies were performed separately on a single disease or in comparison with healthy individuals . 
as mentioned , these three groups of patients could have the same clinical manifestations , leading to difficulties establishing the correct diagnosis and planning appropriate treatment if relying solely on the clinical manifestations and pft . 
in this study , we collected all hrct indexes that were used separately in previous studies and reviewed hrct images of our patients and controls in terms of these indexes . 
fev1 value in carr et al.s study [ 17 ] was lower , but they showed that there is a direct relationship between the prevalence of bronchiectasis and asthma severity . 
patients with refractory asthma and status asthmaticus may have hypertrophy of the airway smooth muscles and distended mucus plaque and small and large airway inflammation , which can result in bwt . in our asthmatic group , however , bwt frequency was lower than in previous similar studies . 
in normal cases the lung shows increased attenuation in the expiration phase , but when air trapping exists , the more translucent areas in expiration are seen in low attenuation . 
this pattern is often seen in some lobes or the whole lung , with generalised involvement of the small airways , but if it is seen as focal involvement , it may be related to smallairway abnormality [ 22 ]  . 
in some other studies , the frequency of emphysema was reported to be higher among asthmatic patients in comparison with healthy populations [ 24 ]  . centrilobular and subpleural parenchymal nodules were seen on hrct images of smokers . 
orsola - malpighi , bologna , italy 2dottorato di scienze pneumo - cardio - toraciche di interesse medico e chirurgico , universit di bologna , bologna , italy 3dipartimento di scienze cliniche , sezione di radiologia , universit di parma , parma , italy 4unit operativa di chirurgia esofago - polmonare delluniversit di bologna , villa maria cecilia e san pier damiano hospitals , cotignola e faenza , italy 5servizio di radiologia e diagnostica per immagini , istituto ortopedico rizzoli , bologna , italy 6radiologia i , policlinico s . 
the volumes of 100 solid intraparenchymal nodules ( mean volume 88.10 mm3 ; range 7.36595.25 mm3 ) studied with the same multidetector computed tomography ( mdct ) protocol were determined using two different versions of the same volumetric software ( lungcare 2006g and lungcare 2007s )  . 
i volumi di 100 noduli polmonari solidi intraparenchimali ( volume medio di 88 , 10 mm3 ; range 7 , 36595 , 25 mm3 ) sottoposti a tomografia computerizzata ( tc ) multidetettore con lo stesso protocollo desame sono stati misurati con 2 versioni diverse dello stesso software di volumetria ( lungcare 2006g e lungcare 2007s )  . 
la versione 2006g e la versione 2007s con algoritmo smallsizenodule hanno dato un risultato sovrapponibile solo in 2 casi su 100 ed hanno esibito una variabilit volumetrica media dell1.66% ( range 0%8 , 78% )  . 
la valutazione computerizzata del tasso di crescita di un nodulo polmonare andrebbe eseguita utilizzando nei vari controlli sempre la stessa versione del software di volumetria ed il medesimo algoritmo di segmentazione . parole chiave nodulo polmonare volumetria 3d tc multidetettore introduction introduzione volumetric evaluation using dedicated software proposed as the method of choice for the dimensional follow - up of indeterminate pulmonary nodules . 
these computer - aided methods are preferred to two - dimensional measurements made by hand or using electronic callipers because of the limitations deriving from the intraand interobserver variability ( reproducibility ) of these techniques [ 1 ]  . 
however , several studies have found that the results of computer - aided volume measurements may be influenced , at times even heavily , by a variety of factors , including the type of computed tomography ( ct ) scanner [ 2 ] , image acquisition and reconstruction parameters [ 3 , 4 ] and type of software used [ 5 ]  . 
following an update of the software used on the ct image reconstruction workstation of our centre , we assessed whether there is a variability of results capable of affecting assessment of pulmonary nodule growth between different versions of the same volumetric software . materials and methods two subsequent versions of the same software for volumetric evaluation of pulmonary nodules ( lungcare 2006g and lungcare 2007s ) included in the postprocessing software ( syngoct , siemens , erlangen , germany ) supplied image reconstruction workstation ( wizard , with our siemens , erlangen , germany ) were compared . 
the software provides a semiautomated measurement system in which the radiologist , after loading the data set of thin - section axial lanalisi volumetrica con software dedicati attualmente proposta come la modalit di scelta nel follow - up dimensionale dei noduli polmonari di natura indeterminata . 
diversi studi hanno comunque evidenziato come anche i risultati delle misurazioni volumetriche computerizzate possano essere influenzate , talora in maniera considerevole , da diversi fattori quali il tipo di scanner per la tomografia computerizzata ( tc ) impiegato , [ 2 ] i parametri tecnici di acquisizione e ricostruzione dellimmagine [ 3 , 4 ] ed anche dal tipo di software utilizzato [ 5 ]  . 
a seguito di aggiornamento software della workstation di ricostruzione delle immagini tc in uso presso il nostro centro , abbiamo voluto valutare se anche tra versioni diverse di uno stesso programma di volumetria computerizzata esista una variabilit dei risultati in grado di influenzare la valutazione di crescita dei noduli polmonari . materiali e metodi sono state valutate comparativamente 2 versioni successive di uno stesso software di analisi volumetrica per noduli polmonari ( lungcare 2006g e lungcare 2007s ) presente nel pacchetto di software di post - processing ( syngoct , siemens , erlangen , germania ) installato sulla workstation di ricostruzione delle immagini tc del nostro centro ( wizard , siemens , erlangen , germania )  . 
si tratta di un sistema di misurazione semiautomatica in cui il medico radiologo , una volta caricato il dataset di immagini assiali a strato sottile nellinterfaccia del programma , deve definire un volume di interesse ( volume of interest , voi ) al cui radiol med ( 2010 ) 115 : 403412 images to the software interface , defines a volume of interest ( voi ) containing the nodule to be assessed . 
the software then generates a 3d image of the lesion to be segmented , i.e. the nodule is separated from the surrounding parenchymal structures for the final volumetric calculation . whereas the previous version lungcare 2006g included a single automatically activated segmentation algorithm , the new 2007s release features three different algorithms , named smallsizenodule , allsizenodule , subsolidnodule , which have to be manually selected before volume determination . 
with regard to the two segmentation algorithms for solid nodules the focus of our study the user manual provides no clear dimensional cutoff value guiding the decision as to which algorithm to select . 
it only states that the smallsizenodule algorithm should be used for the follow - up of patients previously studied with the 2006g version [ 6 ]  . ct images of 100 noncalcified solid intraparenchymal nodules detected in 48 patients studied with the 2006g version were retrieved from our hospitals picture archiving and communication system ( pacs ) ( kodak carestream pacs client suite version 10.1 , sp1 ) and sent to the workstation of the ct scanner . 
all examinations had been performed using the same 16 - slice multidetector ct ( mdct ) scanner ( somatom sensation cardiac 16 , forchheim , germany ) , with the following acquisition parameters : 120 kv ; 150 mas with tube current modulation ; collimation 161.5 mm and single breath - hold scan . volumetric evaluation was based on the data sets of the unenhanced scans reconstructed with 2 - mm - thick sections and 1 - mm increments , field of view ( fov ) of 36 cm , with midfrequency convolution filter ( siemens b41 )  . 
we compared nodule volumes calculated with the 2006g version to those obtained with the 2007s version with the smallsizenodule algorithm , as well as results obtained with the two different segmentation algorithms of the 2007s version . 
il software genera unimmagine tridimensionale della lesione su cui va eseguita la segmentazione , ovvero la separazione del nodulo dalle strutture parenchimali circostanti per il calcolo volumetrico finale . mentre nella precedente versione 2006g era previsto un unico algoritmo di segmentazione , attivato in maniera automatica , nella nuova release 2007s sono disponibili 3 differenti modalit definite smallsizenodule , allsizenodule , subsolidnodule , da selezionare manualmente prima del calcolo volumetrico . 
per quanto concerne i 2 algoritmi di segmentazione per noduli solidi , oggetto del nostro studio , il manuale di istruzioni non fornisce cut - off dimensionali che indichino in maniera univoca quando impiegare luna o laltra modalit . 
viene unicamente consigliato di utilizzare lalgoritmo smallsizenodule per esami di controllo in pazienti precedentemente studiati con la versione 2006g [ 6 ]  . le immagini tc di 100 noduli polmonari solidi non calcifici a sede intraparenchimale , riscontrati in 48 pazienti precedentemente studiati con la versione 2006g del software sono state richiamate dal picture archiving and communication system ( pacs ) del nostro ospedale ( kodak carestream pacs client suite version 10.1 sp1 ) sulla workstation di ricostruzione dello scanner tc . 
tutti gli esami sono stati eseguiti su di una stessa tc multidetettore a 16 banchi ( somatom sensation cardiac 16 , forchheim , germania ) con i seguenti parametri di acquisizione ( 120 kv ; 150 mas con sistema di modulazione della corrente ; collimazione 161 , 5 mm ) durante una singola apnea inspiratoria del paziente . per lanalisi volumetrica sono stati utilizzati i datasets delle scansioni senza mezzo di contrasto con immagini ricostruite ad uno spessore di strato di 2 mm con 1 mm di incremento , un campo di vista ( field of view , fov ) di 36 cm , impiegando un filtro di convoluzione a media frequenza ( siemens b41 )  . 
a tale proposito i 100 noduli sono stati suddivisi in 5 categorie sulla base dei volumi ottenuti con la versione 2006g , ovvero noduli di divided into five categories based on the volumes obtained with the 2006g version , i.e. 
there were 24 nodules < 25 mm3 , 28 between 25 and 50 mm3 , 19 between 50 and 75 mm3 , 11 between 75 and 100 mm3 and 18 > 100 mm3 . volumes calculated with the 2006g version and the smallsizenodule algorithm of version 2007s were the same in two nodules only . 
recent technological advances with the introduction of the spiral technique and mdct scanners have greatly improved anatomical detail and sensitivity of this modality , which is now capable of detecting even nodules as small as 12 mm [ 7 ]  . 
this situation has , however , raised significant diagnostic dilemmas over the correct management of these frequent findings , which are detected in 43%76% of patients depending on the case series [ 8 , 9 ]  . statistically , most nodules < 10 mm turn out to be benign ( for nodules above and below that dimensional threshold , the malignancy rates are 5% and 50% , respectively ) [ 10 ] , radiol med ( 2010 ) 115 : 403412 volume inferiore a 25 mm3 , tra 2550 mm3 , tra 5075 mm3 , tra 75100 mm3 e superiori ai 100 mm3 . risultati i 100 noduli studiati presentavano un volume medio di 88 , 10 mm3 ( range 7 , 36595 , 25 mm3 )  . 
erano presenti 24 noduli di volume inferiore a 25 mm3 , 28 noduli tra 2550 mm3 , 19 tra 5075 mm3 , 11 tra 75100 mm3 e 18 noduli superiori ai 100 mm3 . 
dal punto di vista numerico stata rilevata una differenza media in valore assoluto di 1 , 22 mm3 ( range 020 , 17 mm3 ) , mentre in termini percentuali la discrepanza volumetrica in valore assoluto risultata globalmente dell1 , 66% ( range 0%8 , 78% ) con differenze inferiori all1% in 51 noduli , tra l1%2% in 27 noduli , tra il 2%5% in 15 noduli e superiori al 5% in 7 noduli ( tabella 1 )  . 
le maggiori variazioni volumetriche in termini percentuali sono state riscontrate nel sottogruppo di noduli di minori dimensioni ( < 25 mm3 ) in cui la variazione media in valore assoluto risultata del 3 , 23% ( range 0%8 , 78% ) , decisamente superiore a quella degli altri sottogruppi in cui le variazioni sono risultate inferiori ( mediamente tra 0 , 95% e 1 , 37% ) e con range di variabilit pi ridotti ( tabella 1 )  . per quanto concerne il confronto tra i volumi calcolati con i diversi algoritmi di segmentazione della versione 2007s , i volumi ottenuti con la modalit allsizenodule sono risultati essere mediamente superiori del 71 , 08% ( range 6 , 8%218 , 8% ) rispetto a quelli calcolati con la modalit smallsizenodule . 
il progresso tecnologico degli ultimi anni , con lintroduzione della tecnica spirale e delle tc multidetettore , ha notevolmente migliorato il dettaglio anatomico e la sensibilit della metodica consentendole di identificare anche noduli dellordine dei 12 mm [ 7 ]  . 
tutto ci ha per aperto importanti dilemmi diagnostici circa la corretta gestione di tali reperti che risultano di riscontro assai frequente , con incidenze variabili dal 43% al 76% dei pazienti a seconda delle casistiche [ 8 , 9 ]  . 
1a - f pulmonary nodules evaluated using lungcare version 2006g ( left ) and version 2007s version with the smallsizenodule algorithm ( right ) a , b nodule with the same volume on both versions . 
1a - f noduli polmonari valutati con la versione 2006g del software ( immagini a sinistra ) e con la versione 2007s con algoritmo smallsizenodule ( immagini a destra ) a , b nodulo che presenta lo stesso volume con entrambe le versioni del software . 
this is especially true for nodules < 1 cm , for which the diagnostic techniques routinely used with success with larger nodules [ contrast - enhanced ct , positron emission tomography ( pet ) and ct - guided needle biopsy ] prove suboptimal . 
in clinical practice , indeterminate nodules < 1 cm undergo dimensional follow - up with serial ct scans in accordance with the international benigni da forme iniziali di neoplasia maligna . 
ci maggiormente vero per i noduli di dimensioni inferiori ad 1 cm per i quali risultano subottimali quelle tecniche diagnostiche come la tc con mezzo di contrasto , la tomografia ad emissione di positroni ( pet ) e lagobiopsia tc - guidata , che invece sono normalmente utilizzate con successo nei noduli di dimensioni maggiori . 
nella pratica clinica i noduli subcentimetrici di natura indeterminata vengono quindi sottoposti a follow - up dimensionale con tc seriate in accordo a linee guida internazionali che tengono conto 408 radiol med ( 2010 ) 115 : 403412 table 1 comparison between the lungcare 2006g and lungcare 2007s with the smallsizenodule algorith extent of percentage variation in volume and distribution among nodule subgroups variation all nodules < 25 mm3 2550 mm3 5075 mm3 75100 mm3 > 100 mm3 1%2% 2%3% 3%4% 4%5% 5%6% 6%7% 7%8% 8%9% no . 
consequently , the manual technique cannot be considered reliable for dimensional follow - up of nodules , as such variability ranges may lead to incorrect evaluation of lesion growth . for example , an excess of 1 mm in the evaluation of the maximum diameter of a 10 - mm nodule is sufficient to give rise to a 39% overestimation of volume [ 12 ] , and a diameter change from 4 mm to 5 mm leads to a volume doubling [ 13 ]  . 
for these reasons , computer - aided volumetric analysis techniques have been developed that ensure greater interand intraobserver reproducibility [ 14 , 15 ] and provide greater accuracy in assessing the dimensional evolution of nodules [ 16 ] , thereby allowing delle dimensioni del nodulo e dei dati anamnestici del paziente [ 11 ]  . la misurazione manuale dei noduli , anche se eseguita con calibri elettronici , presenta evidenti limiti di riproducibilit con una variabilit intraosservatore tra 1 , 32 e 1 , 7 mm ed una variabilit interosservatore di 1 , 73 mm [ 1 ]  . 
la tecnica manuale appare dunque poco attendibile per il follow - up dimensionale dei noduli in quanto tali range di variabilit possono indurre in errate considerazioni diagnostiche circa la crescita o meno delle lesioni . 
basti pensare che sufficiente un eccesso di 1 mm nella valutazione del diametro massimo di un nodulo di 10 mm per determinare una sovrastima volumetrica del 39% [ 12 ] e che addirittura si assiste ad un esatto raddoppiamento del volume se il diametro di un nodulo di 4 mm viene sovrastimato a 5 mm [ 13 ]  . 
per queste ragioni sono state sviluppate tecniche di analisi volumetrica computerizzata che garantiscono una maggior riproducibilit intered intraosservatore dei risultati [ 14 , 15 ] e risultano pi accurate nella valutazione evolutiva dimensionale dei noduli [ 16 ] permettendo di caratterizzare i noduli sulla base del loro tempo di radiol med ( 2010 ) 115 : 403412 + 105% + 26% fig . 
la sovrastima volumetrica dellalgoritmo allsizenodule risulta decisamente maggiore nei noduli di piccole dimensioni ( a , b ) ma risulta comunque elevata anche nei noduli di dimensioni minori ( c , d )  . table 2 comparison between the smallsizenodule and the allsizenodule segmentation algorithms of lungcare 2007s . 
entit delle differenze volumetriche percentuali nei sottogruppi di noduli esaminati variazione ogni nodulo < 25 mm3 2550 mm3 5075 mm3 75100 mm3 > 100 mm3 media minima massima 71 , 08% 6 , 02% 218 , 80% 122 , 08% 56 , 95% 218 , 80% 69 , 64% 29 , 34% 100 , 56% 43 , 20% 22 , 15% 71 , 73% 38 , 42% 13 , 66% 59 , 32% 23 , 76% 6 , 02% 40 , 23% characterisation based on doubling time ( dt )  . 
dt is calculated on the basis of volume changes between baseline and follow - up examinations and has a negative predictive value ( npv ) of 98% in the diagnosis of malignant pulmonary nodules when it exceeds 500 days [ 17 ]  . 
for dt calculation to be reliable , however , volume measurements must be accurate and reproducible . computer - aided measurements are not entirely free from variability and , as many authors have demonstrated , may be affected by several factors . 
technical image acquisition parameters such as slice thickness , reconstruction interval , fov and convolution filters may affect calculated volumes [ 3 , 4 ] , so that the same imaging protocol should always be used both at baseline and at follow - up examinations . 
this is due to the different segmentation and volume calculation methods adopted by the various commercial packages . the purpose of our study was to assess whether the use of different versions of the same software may affect the volume measurements of pulmonary nodules . 
to this end , all patients were studied using the same protocol and the same ct scanner , and all volume measurements with the two software versions were always performed on the same image data set . 
this prevented data contamination due to interscan variability related to the ct scanner or the patient ( possible motion or acquisition artefacts in different phases of the respiratory and cardiac cycles ) [ 1921 ]  . our data show that the volume measurements provided by different versions of the same software package are not completely identical . 
even though in most cases the percentage variations were apparently very small ( 1.66% on average ) , they may nonetheless be sufficient to influence the calculation of dt of a nodule on serial examinations . 
volume variability introduced by the use of different software versions may add to the possible growth in size of a nodule between baseline and follow - up scans , thereby dove ti = intervallo di tempo trascorso tra i 2 esami espresso in giorni ; vi = volume iniziale ; vf = volume finale . il calcolo del doubling time integrato nellinterfaccia di alcuni software di volumetria o comunque calcolabile su siti internet di libero accesso mediante inserimento manuale dei necessari valori numerici [ 18 ]  . 
i parametri tecnici di acquisizione dellimmagine quali lo spessore di strato , lintervallo di ricostruzione , il campo di vista e i filtri di convoluzione possono influire sui volumi nodulari calcolati [ 3 , 4 ] ed pertanto necessario che sia sempre utilizzato lo stesso protocollo tra esame di base ed esami di controllo . 
 [ 5 ] , in cui diversi noduli polmonari sono stati valutati con 6 diversi programmi di volumetria , spesso esistono differenze significative nei risultati forniti da differenti software ( in tale lavoro sono state infatti riscontrate sistematiche discrepanze volumetriche nel 73 , 3% delle comparazioni effettuate ) ; ci dovuto alle differenti modalit di segmentazione e calcolo volumetrico impiegate dai diversi pacchetti commerciali . lo scopo del nostro lavoro stato di verificare se anche a parit di software utilizzato , il semplice impiego di versioni diverse possa essere in grado di influenzare i risultati delle misurazioni volumetriche dei noduli . al fine di sottolineare questo aspetto abbiamo studiato tutti i pazienti con il medesimo protocollo sullo stesso scanner tc e le misurazioni volumetriche con le 2 versioni del software sono state effettuate sempre sullo stesso dataset di immagini ; ci ha evitato che i dati potessero essere inquinati da fenomeni di variabilit interscansione relativi allapparecchiatura tc usata o al paziente ( eventuali artefatti da movimento o acquisizione in diverse fase del ciclo respiratorio e del ciclo cardiaco ) [ 1921 ]  . i nostri dati evidenziano come i risultati volumetrici forniti da diverse versioni dello stesso software non siano perfettamente sovrapponibili . 
anche se nella maggioranza dei casi le variazioni percentuali riscontrate sono risultate di entit apparentemente molto modesta ( mediamente dell1 , 66% ) , queste possono essere sufficienti per influenzare il calcolo del doubling time di un nodulo nei controlli seriati . 
la variabilit volumetrica introdotta dallutilizzo di versioni diverse del software pu infatti sommarsi ad un eventuale reale crescita radiol med ( 2010 ) 115 : 403412 affecting dt calculations and risking having it artificially cross the threshold of 500 days , in one direction or the other . 
for these reasons , in contrast with what is stated in the software user manual , it is not advisable to compare results obtained with different software versions , not even if the same segmentation algorithm is used . 
 any possible source of variability in volume measurements may indeed be responsible for incorrect diagnostic conclusions regarding the growth rate of a nodule and may have serious consequences in patient management and treatment . 
where volumes were previously calculated with a different software version , the baseline images should be retrieved from the pacs , and the volume of the nodule should be recalculated on those images using the same version as used in the follow - up scan . 
firstly , being an in vivo study , it lacks data on the real volume of the nodules studied , so that we were unable to establish which of the segmentation algorithms yielded the most accurate results . 
this issue could be further investigated by a phantom study capable of ascertaining which segmentation algorithm is to be preferred and in which dimensional range of nodules it performs best . 
in addition , we restricted our study to intraparenchymal nodules and excluded other types of nodules , such as juxtapleural or juxtavascular lesions , to avoid the influence of additional segmentation errors . 
in fact , during segmentation , the nodules are often poorly separated from the surrounding structures , leading to incorrect volume determination [ 22 , 23 ]  . nonetheless , it is reasonable to assume that the differences intrain volume calculation observed with parenchymal nodules would be similar if not greater in the other categories of pulmonary nodules . conflict of interest none dimensionale del nodulo tra lesame di base e quello di follow - up , finendo per modificarne il calcolo del tempo di raddoppiamento e rischiando di fargli varcare artificiosamente , in un senso o nellaltro , il valore soglia di 500 giorni . 
tale rischio risulta pi concreto nel caso di confronto tra risultati ottenuti con modalit di segmentazione differenti , data la forte discrepanza dei valori volumetrici riscontrati tra gli algoritmi smallsizenodule ad allsizenodule ( i volumi calcolati con questultimo algoritmo sono risultati mediamente superiori del 71 , 08% )  . per questi motivi , contrariamente a quanto suggerito dal manuale di istruzioni del programma , il confronto tra risultati ottenuti con diverse versioni del software non a nostro parere consigliabile nemmeno se si impiega lo stesso algoritmo di segmentazione . ogni possibile fonte di variabilit nelle misurazioni volumetriche pu infatti essere responsabile di errate conclusioni diagnostiche circa il reale tasso di crescita di un nodulo ed avere serie ricadute sulla gestione ed il trattamento terapeutico del paziente . 
per il controllo evolutivo volumetrico di un nodulo polmonare , appare pi corretto impiegare sempre la stessa versione del software con la medesima modalit di segmentazione ; nel caso di volumi calcolati in precedenza con una diversa versione del software , risulta necessario richiamare le immagini dellesame di base dal pacs e ricalcolare su di esse il volume del nodulo con la stessa versione utilizzata nellesame di follow - up . 
trattandosi di uno studio in vivo mancano dati circa le reali dimensioni volumetriche dei noduli studiati ; non pertanto possibile verificare quale dei differenti algoritmi di segmentazione impiegati abbia fornito i risultati pi precisi . 
questa problematica potr essere oggetto di ulteriori ricerche ; sarebbe necessario uno studio su fantoccio per appurare quale algoritmo di segmentazione sia preferibile ed in quale range dimensionale di noduli fornisca le migliori prestazioni . 
il nostro studio stato inoltre condotto testando un unico software commerciale ; ne deriva pertanto che i risultati ottenuti sono unicamente applicabili allo specifico programma di volumetria impiegato ed andrebbero verificati anche su altri pacchetti commerciali . 
abbiamo limitato lo studio ai soli noduli intraparenchimali , mentre altre tipologie di noduli come quelli iuxtapleurici o iuxtavascolari non sono stati valutati per evitare che ai nostri risultati si sommassero anche eventuali errori di segmentazione . 
come emerge dalla letteratura , la vicinanza del nodulo alle strutture vascolari o alle limitanti pleuriche pu influenzare il calcolo volumetrico finale ; spesso , infatti , nella fase di segmentazione tali noduli possono essere mal dissociati dalle strutture circostanti portando ad unerrata stima volumetrica [ 22 , 23 ]  . 
cademartiri1 , 2 1dipartimento di radiologia e del cardio - polmonare , azienda ospedaliero - universitaria di parma , c / o piastra tecnica , piano 0 , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia e cardiologia , ospedale san gennaro , napoli , italy 4cpc centro prevenzione cardiovascolare , ospedale san raffaele , milano , italy 5dipartimento di radiologia e cardiologia , azienda asl , carrara , italy correspondence to : f . 
a total of 1 , 372 patients ( 882 men , 490 women ; mean age 59.311.9 years ) in sinus rhythm were studied with ct - ca ( 64 - slice technology ) and cca . 
cca demonstrated the absence of significant coronary artery disease in 46.6% ( 639 / 1372 ) , single - vessel disease in 24.7% ( 337 / 1372 ) and multivessel disease in 28.9% ( 396 / 1372 ) of patients . 
in per - patient analysis sensitivity , specificity and positive and negative predictive value of ct - ca were 99% [ confidence interval ( ci ) 9799 ] , 92% ( ci 8994 ) , 94% ( ci 9195 ) and 99% ( ci 9799 ) , respectively . 
obiettivo di questo lavoro stato valutare laccuratezza diagnostica dellangiografia coronarica non invasiva con tomografia computerizzata ( ct - ca ) a 64 strati nellindividuazione delle stenosi coronariche significative ( riduzione del lume coronarico 50% ) confrontata con la coronarografia convenzionale ( cag ) in un registro e revisionare i risultati dei trials multicentrici . 
sono stati studiati 1372 pazienti ( 882 uomini , 490 donne , et media 59 , 311 , 9 anni ) in ritmo cardiaco sinusale con ct - ca ( tecnologia 64 strati ) e cag . la ct - ca stata eseguita secondo i protocolli comunemente utilizzati . 
il 46 , 6% ( 639 / 1372 ) mostravano coronarie indenni o con lesioni che determinavano stenosi < 50% , il 24 , 7% ( 337 / 1372 ) mostrano malattia critica di un solo vaso , ed il 28 , 9% ( 396 / 1372 ) dei pazienti mostrava coronaropatia critica multivasale . 
nellanalisi per paziente la sensibilit , specificit , valore predittivo radiol med ( 2010 ) 115 : 368384 ( lr + = 12.4 and lr = 0.011 ; lr + = 18.3 and lr = 0.064 , respectively ) , were good . 
ct - ca is a reliable diagnostic modality both in terms of sensitivity and negative predictive value . differences in trial results are also due to the different parameters used for patient inclusion . keywords multislice computed tomography conventional coronary angiography coronary artery disease 64 - slice ct registry large population multicentre trials positivo e negativo della ct - ca sono risultati 99% ( intervallo di confidenza [ ic ] 9799 ) , 92% ( ic 8994 ) , 94% ( ic 9195 ) , 99% ( ic 9799 ) , rispettivamente . 
i risultati dei trials sono variabili anche alla luce dei parametri principali di inclusione utilizzati . parole chiave tomografia computerizzata multistrato a 64 strati angiografia coronarica convenzionale malattia aterosclerotica coronarica registro ampia popolazione trials multicentrici introduction introduzione computed tomography coronary angiography ( ct - ca ) is one of the major innovations in the field of diagnostic medicine in recent decades [ 19 ]  . 
from the early studies with 4slice ct , we now stand at the dawning of the age of ct - ca with low doses of ionising radiation [ 1013 ]  . 
this means that the last and greatest drawback that to date has limited the extensive application of the imaging modality is about to be overcome . nonetheless , wide - ranging and reliable evidence regarding the effective role of ct - ca in the field of the consolidated diagnostic algorithms of cardiovascular medicine is still missing . 
the ct - ca literature is witnessing a real explosion of data , and it is highly likely that we will see the arrival of series numbering thousands of patients . 
nonetheless , the formation of large registries among high - volume centres would be opportune to adequately respond to these emerging queries regarding the modality . in this study , we present the first series derived from a multicentre registry of ct - ca that studies the diagnostic accuracy of ct - ca compared with conventional coronary angiography ( cca )  . 
in addition , we provide a critical review of the most recent multicentre trials on the same topic [ 1822 ]  . langiografia coronarica con tomografia computerizzata ( ct - ca ) costituisce una della maggiori innovazioni in campo medico diagnostico degli ultimi dieci anni [ 19 ]  . 
dalle prime esperienze con tomografia computerizzata ( tc ) a 4 strati siamo oggi allalba dellera della ct - ca a bassa dose di radiazioni ionizzanti [ 1013 ]  . 
questo significa che sta per essere abbattuta lultima e la maggiore riserva che ha , fino ad oggi , limitato lapplicazione estensiva di questa modalit . mancano , tuttavia , ancora ampie ed affidabili evidenze scientifiche su quale sia effettivamente il ruolo della ct - ca nellambito dei consolidati algoritmi diagnostici in medicina cardio - vascolare . 
mancano anche delle vere e proprie linee guida di utilizzo , ma ci si riferisce per il momento a raccomandazioni di utilizzo e documenti condivisi [ 1417 ]  . la letteratura della ct - ca sta vedendo una vera e propria esplosione di dati e molto probabilmente vedremo emergere casistiche con migliaia di pazienti da ora in avanti . 
pochi sono i centri di riferimento in grado di produrre e mantenere un database clinico costante delle attivit della ct - ca . tuttavia , sarebbe auspicabile la formazione di ampi registri tra centri ad alto volume di prestazioni per poter rispondere adeguatamente ai quesiti emergenti sulla metodica . 
 in questo lavoro presentiamo la prima casistica derivante da un registro multicentrico di ct - ca studiando laccuratezza diagnostica della ct - ca confrontata con la coronarografia convenzionale ( cag )  . 
inoltre , forniamo una revisione critica dei pi recenti trials multicentrici sul medesimo argomento [ 1822 ]  . 370 registry materials and methods materiali e metodi registro radiol med ( 2010 ) 115 : 368384 data presented are drawn from a multicentre registry . 
the participating centres are characterised by ct - ca examination volume > 300 / year ; presence of a haemodynamic laboratory on site or directly attached ; experience of operators > 5 years ; ability to maintain a detailed prospective longitudinal database of all the characteristics of patients undergoing ct - ca ; homogeneous protocols for scanning and image analysis ( pharmacological preparation of the patients , scan / reconstruction parameters and administration of contrast material ) ; systematic evaluation of the examinations by at least two expert operators in 90% of cases ( double reading )  . i dati presentati derivano da un registro multicentrico . 
i centri partecipanti sono caratterizzati da : volume di esami ct - ca > 300 / anno ; presenza di laboratorio di emodinamica in loco o direttamente afferente ; esperienza degli operatori > 5 anni ; capacit di mantenere un database dettagliato longitudinale prospettico di tutte le caratteristiche dei pazienti che effettuano ct - ca ; impostazione omogenea dei protocolli di scansione ed analisi delle immagini ( preparazione farmacologica del paziente , parametri scansione / ricostruzione e somministrazione del mezzo di contrasto ) ; valutazione sistematica delle indagini da parte di almeno due operatori esperti nel 90% dei casi ( doppia lettura )  . study population popolazione studiata from may 2004 to december 2006 1 , 372 consecutive patients ( 882 men , 490 women ; mean age 59.311.9 years , median 59 years , range 2186 years ) referred for cca with the aim of determining the presence and extension of coronary artery disease ( cad ) underwent a ct - ca examination . 
patients included in the registry had sinus rhythm , had never undergone percutaneous angioplasty or coronary artery bypass graft surgery and were able to maintain breath - hold for at least 12 s . 
the ethics committee approved the protocol , and all patients gave informed consent . patient preparation the technique for patient preparation is one of the most variable parameters among the participating centres . 
in general , in the absence of absolute contraindications , patients with a heart rate ( hr ) > 60 beats per minute ( bpm ) received a single oral 100 - mg dose of metoprolol tartrate 4560 min prior to the scan . alternatively , patients were given intravenous beta - blockers ( atenolol 100 mg , propranolol 5 mg , metoprolol 5 mg , esmolol 0.5 mg / kg ) directly in the diagnostic suite with da maggio 2004 a dicembre 2006 , sono stati studiati mediante ct - ca 1372 pazienti consecutivi ( 882 di sesso maschile , 490 di sesso femminile , et media 59 , 311 , 9 anni ; mediana 59 anni ; range 2186 anni ) candidati allesecuzione di una cag allo scopo di determinare la presenza e lestensione della malattia coronarica . 
i pazienti elegibili , ma non inclusi nel registro derivano da situazioni nelle quali i dati non sono stati completamente raccolti ( paziente che effettua cag in altro centro ed alla quale non si riesca a risalire su supporto digitale , raccordo anamnestico parziale / incompleto , perdita di dati primari ) e costituiscono l8 , 5% ( 128 / 1500 )  . 
sono stati inclusi pazienti con ritmo sinusale , mai sottoposti ad angioplastica percutanea o ad intervento chirurgico per il posizionamento di by - pass e capaci di trattenere il respiro per almeno 12 secondi , sono stati inclusi nello studio . 
i pazienti con sindrome coronarica acuta nei quali la scansione tc avrebbe provocato un ritardo nellesecuzione della terapia di rivascolarizzazione o quelli nei quali esistevano delle controindicazioni assolute alla somministrazione intravenosa di mezzo di contrasto iodato ( allergia nota , insufficienza renale o disordini tiroidei ) sono stati esclusi dallo studio . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . preparazione del paziente la tecnica di preparazione del paziente uno dei parametri pi variabili tra i centri partecipanti . 
in generale , in assenza di contro - indicazioni assolute , nei pazienti con una frequenza cardiaca ( fc ) superiore a 60 battiti per minuto ( bpm ) stata somministrata 45 / 60 minuti prima della scansione , se non presenti delle controindicazioni , una singola dose orale di 100 mg di radiol med ( 2010 ) 115 : 368384 constant electrocardiographic ( ecg ) and pressure monitoring . 
patients displaying evident anxiety were given an oral dose of 1 mg of lorazepam . immediately prior to the scan , a single sublingual dose of isosorbide dinitrate ( 2 mg ) was administered . scan protocol and image reconstruction examinations were performed with a 64 - slice ct scanner ( sensation 64 , siemens , forchheim , germany ; vct , general electric , milwaukee , wi , usa ) according to a protocol described elsewhere [ 6 , 23 ]  . 
field of view used for evaluation of the coronary arteries was the minimum allowed by the individual anatomy of the patient ( 120 160 mm )  . retrospective reconstructions based on the ecg signal were performed to obtain an image quality without motion artefacts . 
in alternativa , sono stati utilizzati beta - bloccanti per via endovenosa ( atenololo 100 mg , propanololo 5 mg , metoprololo 5 mg , esmololo 0 , 5 mg / kg ) direttamente in sala diagnostica con monitoraggio elettrocardiografico e pressorio costante . 
nei pazienti con controindicazioni assolute ai beta - bloccanti ( stenosi valvolare aortica severa , asma bronchiale in trattamento con steroidi , blocchi atrio - ventricolari ) sono stati utilizzati calcio antagonisti ( diltiazem 5 mg , verapamil 5 mg ) per via endovenosa . 
nei pazienti con evidente componente ansiosa stata somministrata per via orale una dose di 1 mg di lorazepaimmediatamente prima della scansione stato somministrata una singola dose sub - linguale di isosorbide dinitrato ( 2 mg )  . protocollo di scansione e ricostruzione delle immagini per lindagine sono stati utilizzati scanner tc a 64 strati ( sensation 64 , siemens , forchheim , germania ; vct , general electric , milwaukee , usa ) secondo protocolli standard gi descritti [ 6 , 23 ]  . 
i parametri di scansione hanno sfruttato la minore collimazione disponibile , il pitch ridotto adeguato al sovra - campionamento delle informazioni , 120 kv , 600900 mas . sono stati somministrati 80100 ml di mezzo di contrasto iodato ( iomeprolo , iomeron 400 mgi / ml , bracco ; iomeprolo , iomeron 350 mgi / ml , bracco ; iodixanolo , visipaque 320 mgi / ml , ge healthcare ; ioexolo , omnipaque 350 mgi / ml , ge healthcare ; iopromide , ultravist 370 mgi / ml , bayer healthcare ) alla velocit di 46 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 1820 gauge preventivamente posizionata in una vena antecubitale . 
allo scopo di ottimizzare lopacizzazione dei vasi arteriosi coronarici stata utilizzata la tecnica del bolus - tracking per sincronizzare larrivo del mezzo di contrasto nelle arterie coronarie con linizio della scansione ed il bolo di salina di seguito al bolo di mezzo di contrasto [ 2426 ]  . le immagini sono state ricostruite con il minimo spessore di strato disponibile o in alternativa con lo spessore di strato ottimale per il mantenimento di un adeguato rapporto segnale / rumore ( 0 , 50 , 75 mm )  . 
 sono state effettuate delle ricostruzioni retrospettive basate sul segnale elettrocardiografico ( ecg ) per ottenere una qualit dellimmagine priva di artefatti da movimento . le finestre temporali utilizzate sono state la fase mesoe telediastolica ( da 300 a 450 ms prima della successiva onda r e / o dal 60%70% dellintervallo r - r )  . 
evaluation of coronary stenosis was done with an exclusively visual score . segments were classified as normal / not significantly diseased ( healthy or with lumen irregularities or reduction < 50% ) or significantly diseased ( 50% lumen reduction )  . conventional coronary angiography cca was performed within 4 weeks of ct - ca . 
utilizzando un software dedicato ( windose , istituto di fisica medica , erlangen , germania ) stata calcolata la dose di radiazioni ionizzanti alla quale i pazienti sono stati esposti durante la scansione angiografica ( valore medio 15 , 2 msv per le donne e 21 , 4 msv per gli uomini )  . 
sulle singole lesioni sono state effettuate quindi ricostruzioni multiplanari longitudinali ed assiali per classificare le lesioni come significative o non - significative . la valutazione delle stenosi coronariche stata effettuata con score esclusivamente visivo . 
i segmenti sono stati classificati come normali / non significativamente malati ( indenni o con irregolarit del lume o con riduzione del diametro < 50% ) o significativamente malati ( stenosi del lume 50% )  . angiografia coronarica convenzionale la cag stata eseguita entro 4 settimane dalla ct - ca . un singolo osservatore , non a conoscenza dei risultati della ct - ca , ha identificato i segmenti coronarici utilizzando la medesima classificazione in 17 segmenti [ 27 ]  . tutti i segmenti , senza limiti di diametro , sono stati inclusi per il confronto con la ct - ca . 
i segmenti sono stati classificati come normali ( con pareti e lume regolari ) , non significativamente malati ( con irregolarit del lume o con riduzione del diametro < 50% ) o significativamente malati ( stenosi del lume 50% )  . 
le stenosi coronariche sono state quantificate in due proiezioni ortogonali utilizzando un algoritmo di misurazione validato per langiografia coronarica ( caas , pie medical , maastricht , olanda ) , e classificate come significative se la riduzione del diametro del lume era 50% . 
rca , coronaria destra ; lca , coronaria sinistra ; lm , tronco comune sinistro ; cx , arteria coronaria circonflessa ; lad , arteria coronaria discendente anteriore . analisi statistica i dati sono presentati come prevalenze , medie e deviazioni standard . 
la performance diagnostica dellangiografia coronarica mediante ct - ca nellindividuazione delle lesioni aterosclerotiche coronariche significative , utilizzando la cag come tecnica di riferimento di seguito radiol med ( 2010 ) 115 : 368384 included for comparison with ct - ca . 
segments were classified as normal ( with regular walls and lumen ) , not significantly diseased ( with lumen irregularities or reduction < 50% ) or significantly diseased ( 50% lumen reduction )  . 
coronary artery stenoses were quantified in two orthogonal views using a measurement algorithm validated for coronary angiography ( caas , pie medical , maastricht , the netherlands ) and classified as significant if the lumen reduction was 50% . statistical analysis data are presented as prevalence , means and standard deviations ( sd )  . 
diagnostic performance of ct - ca in identifying significant coronary artery atherosclerotic lesions , with cca as the reference standard , is reported in terms of sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) with 95% confidence intervals ( ci ) calculated with binomial expansion . 
positive likelihood ratio ( lr + ) and negative likelihood ratio ( lr ) were calculated , as were positive posttest probability ( ptp + ) and negative posttest probability ( ptp )  . 
mean hr during the examination was 58 bp almost half of the population suffered from stable angina ( 48% ; 644 / 1 , 372 ) , with one quarter of patients arriving at hospital with symptoms of acs ( 25% ; 339 / 1 , 372 ) and 10% ( 132 / 1 , 372 ) being high - risk asymptomatic . 
a total of 47% ( 639 / 1 , 372 ) presented with health coronary arteries or arteries with lesions classified as < 50% lumen reduction , 25% ( 337 / 1 , 372 ) had singlevessel disease and 29% ( 396 / 1 , 372 ) were affected by multivessel disease ( table 1 )  . diagnostic accuracy of ct - ca in identifying significant riportata come sensibilit , specificit , valore predittivo positivo e negativo con intervalli di confidenza ( ic ) al 95% calcolati con espansione binomiale . 
sono stati calcolati i likelihood ratio positivo e negativo ( lr + e lr - , rispettivamente ) e i valori di probabilit post - test positiva e negativa ( ptp + e ptp - , rispettivamente )  . 
la frequenza cardiaca media durante lesame era pari a 58 bpda notare che quasi il 50% della popolazione soffriva di angina stabile ( 48% ; 644 / 1372 ) , che circa un quarto dei pazienti arrivavano in ospedale con sintomatologia inquadrata come sindrome coronarica acuta ( 25% ; 339 / 1372 ) e che circa il 10% ( 132 / 1372 ) dei pazienti erano asintomatici ad alto rischio . sono stati inclusi per il confronto con langiografia coronarica convenzionale 1372 pazienti , 5488 vasi e 19136 segmenti . 
il 47% ( 639 / 1372 ) mostravano coronarie indenni o con lesioni che determinavano stenosi < 50% , il 25% ( 337 / 1372 ) mostrano malattia critica di un solo vaso , ed il 29% ( 396 / 1372 ) dei pazienti mostrava coronaropatia critica multivasale ( tabella 1 )  . laccuratezza diagnostica della ctca nellindividuazione delle lesioni significative mostrata in tabella 2 . nellanalisi per paziente la sensibilit , specificit , valore predittivo positivo e negativo sono risultati 99% ( ic 9799 ) , 92% ( ic 8994 ) , 94% ( ic 9195 ) , 99% ( ic 9799 ) , rispettivamente . 
nellanalisi per segmento la sensibilit , specificit , valore predittivo positivo e negativo sono risultati 94% ( ic 9294 ) , 95% ( ic 9495 ) , 64% ( ic 6165 ) , 99% ( ic 9999 ) , rispettivamente . 
per quanto riguarda i lr , valori elevati sono stati riscontrati nella valutazione per paziente ( lr + = 12 , 4 e lr = 0 , 011 ) e nella valutazione per segmento ( lr + = 18 , 3 e lr = 0 , 064 )  . 
i valori pi bassi di lr sono stati rilevati nella valutazione per vaso sulla coronaria discendente anteriore tronco comune ( lr + = 4 , 5 e lr = 0 , 037 )  . 
in the per - patient analysis , sensitivity , specificity , ppv and npv were 99% ( ci 9799 ) , 92% ( ci 8994 ) , 94% ( ci 9195 ) and 99% ( ci 9799 ) , respectively . 
le variabilit intered intra - osservatore , espresse come valori di e calcolate su una sotto - popolazione ( 300 / 1372 ) , per lindividuazione delle lesioni significative sono risultate essere rispettivamente dello 0 , 78 e 0 , 85 . 
in particolare la sensibilit ed il valore predittivo per paziente sono risultati del 99% e 99% , rispettivamente , con valori di specificit e valore predittivo positivo al di sopra del 90% . 
these data decisively strengthen the known information on the technique in that they were derived from a longitudinal study of several centres over a significant time period and with a large number of patients . 
this is the population in which the use of ct - ca is considered appropriate [ 1417 ]  . centri molto estesa nel tempo e su un numero di pazienti elevato . 
in passato sono stati pubblicati trials con risultati buoni sulla coronarografia effettuata mediante risonanza magnetica , ai quali non hanno fatto seguito ulteriori esperienze analoghe [ 28 ]  . 376 radiol med ( 2010 ) 115 : 368384 fig . 
absolute and cumulative distribution of hr bpm ; a , b , bmi ( c , d ) and coronary artery calcium ( cascore ; e , f ) in the registry population . 
absolute frequency is expressed as a number ( a , c , e ) , whereas cumulative frequency is expressed as a percentage of the total population ( b , d , f )  . 
the graphs for hr and bmi ( a - d ) show a near - normal distribution , whereas the distribution in the cascore graphs does not appear normal ( e , f )  . 
i grafici a barre della distribuzione assoluta e cumulativa della frequenza cardiaca ( bpm ; a , b ) , body mass index ( bmi ) ( c , d ) e calcio coronarico ( cascore ; e , f ) nella popolazione del registro . 
la frequenza assoluta viene espressa come numero ( a , c , e ) mentre la frequenza cumulativa viene espressa in percentuale della popolazione totale ( b , d , f )  . 
per la frequenza cardiaca ed il bmi ( a - d ) si osserva una distribuzione pressoch normale mentre per il calcio coronarico la distribuzione appare non normale ( e , f )  . 
inoltre , si osserva facilmente dalle frequenze cumulative come i valori considerati ideali di ogni parametro corrispondano al 60% della popolazione globale ; frequenza cardiaca < 60 bpm , bmi < 30 , cascore < 400 ( teste di freccia in b , d , f )  . 
in the past , trials have been published with good results on coronary angiography per la ct - ca , sono stati pubblicati almeno 5 trials di cui 4 multicentrici e 2 multivendor [ 1822 ]  . 
utilizzando semplici parametri come la radiol med ( 2010 ) 115 : 368384 378 radiol med ( 2010 ) 115 : 368384 ct - ca pre - test probability of disease 100 - specif icity fig . 
computed tomography coronary angiography ( ct - ca ) ] , the probability that a patient effectively has a coronary stenosis 50% increases significantly , even with a low or very low pretest probability ( range 0%30% )  . 
per un test ( ct - ca ) positivo aumenta significativamente la probabilit che un paziente sia effettivamente portatore di una stenosi coronarica 50% anche con probabilit pre - test bassa o molto bassa ( range 0%30% )  . 
il grafico a destra mostra la curva roc , che dimostra lampia area sotto la curva ( auc = 0 , 955 ; intervallo di confidenza del 95% ( ic ) 0 , 940 , 96 )  . 
with regard to ct - ca , at least five trials have been published , of which four are multicentre and two multivendor [ 1822 ]  . interpretation of data from multicentre trials , however , is not always a simple task . 
as can be seen in table 3 , differences between studies can in some cases be quite marked . simple parameters such as disease prevalence , prevalence of male subjects , body mass index ( bmi ) and so on can be used to attempt to explain differences between studies . the first useful parameter in this sense is disease prevalence . 
in short , using a diagnostic test to study patients with a disease prevalence of 10% or 90% is very different , and the resulting accuracy will generally be different . 
this implies a spectrum of probability ranging from low to high risk . prevalenza di malattia , la prevalenza degli individui di sesso maschile , lindice di massa corporea ( bmi ) , e cos via , si possono provare ad individuare le possibili spiegazioni relative alle differenze tra gli studi . il primo parametro meritevole di approfondimento la prevalenza di malattia . 
questo implica uno spettro di probabilit che va dal basso allalto rischio . tra i parametri specifici in grado di modulare laccuratezza diagnostica se ne possono identificare almeno 3 in letteratura : il bmi , la frequenza cardiaca ed il calcio coronarico ( calcium score secondo agatston )  . 
in some cases , the classic form or twin peaks can be seen ( cactus , accuracy , meijboom ) , whereas in other cases ( nimiscad and core - 64 ) a flat appearance of the accuracy parameters can be appreciated . 
dai grafici a barre si osservano differenti profili di accuratezza diagnostica . in alcuni casi , si osserva la classica forma a due picchi ( cactus , accuracy , meijboom ) mentre in altri casi ( nimiscad e core - 64 ) si osserva un aspetto flat dei parametri di accuratezza diagnostica . 
in the first case , the above - described lesions tend to be judged as positive and accuracy parameters take on a twin - peak appearance on sensitivity and npv , to the detriment of specificity and ppv . 
nel primo caso si tende a giudicare le lesioni sopra descritte come positive e i parametri di accuratezza assumono un aspetto a doppio picco , su sensibilit e valore predittivo negativo , a scapito della specificit e del valore predittivo positivo . 
for example , the low prevalence of disease in the accuracy study is very evident , as is the low cascore in the cactus and core - 64 studies [ 1822 ]  . 
in the third case , parameters take on a central peak appearance , which favours the values of specificity and ppv . the first approach is more in line with a test that aims to identify all patients with disease ( sensitivity ) and exclude with certainty patients without disease ( npv )  . 
the second approach in a certain sense tends to be more correct from a formal point of view in that it judges ct - ca in a manner consistent with the imaging findings of the technique . 
the third approach tends to evaluate ct - ca as if it were cca and tends to define the lesions as significant only when there is certainty ( 50% lumen reduction ) , even at the expense of sensitivity . 
il secondo atteggiamento tende ad essere per certi versi pi corretto dal punto di vista formale , in quanto giudica la ct - ca in modo coerente al reperto di imaging della metodica . 
il terzo atteggiamento tende a valutare la ct - ca come se fosse una cag e tende a definire le lesioni come significative solo quando sono certe ( riduzione del lume 50% ) , anche a scapito della sensibilit . 
only in one study [ non invasive multicenter italian study for coronary artery disease ( nimis - cad ) ] did the authors provide both readings [ 18 ]  . this information is of particular interest because it shows that there is an impact on the evaluation by operators who are aware of the patient . 
indeed , a much longer period and higher number of examinations would appear to be required to achieve the levels of accuracy commonly reported in the literature by the reference centres [ 5 , 3133 ]  . this parameter cannot be extrapolated from the series reported in the trials , even though core - lab evaluation should guarantee expert operators . 
in addition , not even the level of expertise of the individual centres can be extrapolated , and this can influence the evaluation of the most expert operator . study limitations the major limitation of ct - ca remains radiation exposure . in studies performed in recent years , measured dose values have been at the heart of major criticisms of the technique in the international setting . 
however , the introduction of new hardware and software capable of providing adequate image quality using prospective triggering based on the ecg signal enables dose values to be brought below 5 msv [ 1013 ]  . 
with regard to this feature , whereas hr was and is important for optimal image quality , the introduction and use of prospective protocols only reinforce its importance . the quality of the ct - ca examination performed with prospective triggering is , in fact , influenced by an hr that should be as low as possible ( ideally < 60 bpm at all times )  . a limitation of the study derives from the registry design , which does not offer the same characteristics of a trial or a prospective study . 
solo in uno studio ( non invasive multicenter italian study for coronary artery disease , nimis - cad ) gli autori hanno fornito entrambe le letture [ 18 ]  . 
sulla base di decennale esperienza maturata in alcuni centri questo appare non realistico . infatti , sembrerebbe necessario un periodo molto pi lungo ed un numero molto pi elevato di indagini effettuate per raggiungere i valori di accuratezza diagnostica comunemente riportati in letteratura dai centri di riferimento [ 5 , 3133 ]  . 
inoltre , anche il livello di perizia esecutiva dei singoli centri non estrapolabile e pu condizionare la valutazione delloperatore pi esperto . limiti allo studio la maggiore limitazione della ct - ca e rimane ancora oggi la dose di radiazioni . 
tuttavia , lintroduzione di nuovi hardware e software in grado di fornire adeguata qualit di immagine utilizzando il triggering prospettico basato sul segnale ecg consentono di portare i valori di dose al di sotto dei 5 msv [ 1013 ]  . 
in merito a questo punto , se la frequenza cardiaca era e rimane importante per una qualit ottimale delle immagine , lintroduzione e lutilizzo di protocolli prospettici non fa altro che rinforzarne limportanza . 
la qualit dellindagine ct - ca effettuata con triggering prospettico infatti condizionata da una frequenza cardiaca che sia la pi bassa possibile ( idealmente sempre < 60 bpm )  . 
daneman ( eds ) springer - verlag , berlin , heidelberg , 2010 isbn 978 - 3 - 540 - 89384 - 4 published online : 30 march 2010 springer - verlag 2010 this could be called a first - aid emergency booklet to be used by surgeons and clinicians troubled by doubts when confronted with a problematic patient , and by radiologists trying to resolve these questions with all available imaging weapons . eighty diagnoses are discussed : on the left page , one will find surgeon / clinician problems and clinical data , on the right page how the radiologist can solve these . the clinicians page has relevant boxes with clinical insights , warnings , controversies , urgency , what the surgeons needs to know , clinical differential diagnoses ; the radiologists page shows images confirming the diagnosis and imaging options , imaging findings , tips , radiological differential diagnoses . out of the 80 diagnoses presented only eight are listed as emergency cases . this informative booklet is easy to read , yet has some drawbacks : not all images shown are perfectly reproduced ; often the use of black arrows ( so tiny sometimes ! ) on a nearly black imaging background renders them nearly impossible to see ; hospital jargon and acronyms become brain teasers even if a list of many ( not all ) may be found in two of the opening pages . the book is recommended for young doctors in training to test their skills and more experienced doctors to refresh their knowledge . il volumetto in questione pu essere definito un manuale di pronto soccorso da utilizzare da chirurghi e clinici che devono risolvere i loro dubbi di fronte a casi difficili e problematici e dai radiologi che tentano di risolvere questi dubbi e problemi mediante tutte le possibili armi di studio per immagini a loro disposizione . 
 sono presi in considerazione ottanta casi diagnostici : sulla pagine di sinistra vengono elencate le problematiche del chirurgo / clinico , sulla pagina destra cosa pu fare il radiologo per risolverle . 
 la pagina del clinico mette in evidenza in appositi riquadri schematici i dati clinici , le avvertenze , le controversie , il grado di urgenza , cosa ci si aspetta dal radiologo , e le possibili diagnosi differenziali ; la pagina del radiologo evidenzia le immagini significative necessarie per confermare la diagnosi , le opzioni diagnostiche , i riscontri ottenibili con le singole modalit di immagine , i suggerimenti e le diagnosi radiologiche differenziali . della 80 diagnosi presentate , solo 8 sono considerate come emergenze . questo volumetto ricco di informazioni di facile lettura , ha tuttavia alcuni inconvenienti . 
non tutte le immagini sono riprodotte perfettamente ; spesso luso di frecce nere ( talvolta cos piccole ! ) e poste su uno sfondo di per se stesso gi scuro dellimmagine , le rendono quasi impossibili da riconoscere ; luso di gergo ospedaliero e di acronimi ( anche se un lungo , ma non completo elenco degli stessi , presente in due delle pagine iniziali ) crea rompicapi . 
 il volume raccomandabile sia ai giovani medici in via di tirocinio e specializzazione , onde mettere alla prova le loro capacit diagnostiche che ai pi anziani per rinfrescare le loro conoscenze . 
salvatore dipartimento di scienze biomorfologiche e funzionali ( dsbmf ) , universit degli studi di napoli federico ii ( unina ) , istituto di biostrutture e bioimmagini ( ibb ) , consiglio nazionale delle ricerche ( cnr ) , fondazione sdn ( irccs ) , napoli , italy correspondence to : s . 
maurea , via ernesto murolo 5 , 80123 napoli , italy , tel . : + 39 - 081 - 7463560 , fax : + 39 - 081 - 5457081 , e - mail : maurea@unina.it received : 11 february 2009 / accepted : 12 may 2009 / published online : 15 january 2010 springer - verlag 2010 abstract purpose . 
the majority of patients ( 31 / 40 , 78% ) had proven malignant pancreatic tumours ( 24 ductal adenocarcinoma , six mucinous cystadenocarcinoma , one intraductal papillary mucinous carcinoma ) , whereas the remaining patients ( 9 / 40 , 22% ) were found to have benign lesions ( eight chronic pancreatitis , one serous cystadenoma )  . 
results of the imaging studies were compared with biopsy ( n = 33 ) and / or histology ( n = 7 ) findings to calculate sensitivity , specificity , accuracy and positive ( ppv ) and negative ( npv ) predictive value for correct identification of tumours and evaluation of resectability of malignancies . 
both for tumour identification and resectability , msct and mri had comparable diagnostic accuracy , with no statistically significant differences between them . tumour identification ct / mri : accuracy 98 / 98% , sensitivity 100 / 100% , specificity 88 / 88% , ppv 97 / 97% , npv 100 / 100% ; tumour resectability ct / mri : accuracy 94 / 90% , sensitivity 92 / 88% , specificity 100 / 100% , ppv 100 / 100% , npv 78 / 70% . 
mri represents a valid diagnostic alternative to ct in the evaluation of patients with pancreatic masses , both for correct identification and characterisation of primary lesions and to establish resectability in the case of malignancies . 
scopo del nostro studio stato effettuare un confronto dei risultati della tomografia computerizzata ( tc ) multistrato e della risonanza magnetica ( rm ) ad alto campo nella valutazione diagnostica di pazienti con masse pancreatiche . 
sia per lidentificazione delle lesioni neoplastiche che per la valutazione della resecabilit chirurgica , la tc e la rm hanno mostrato valori di accuratezza diagnostica comparabili senza differenze statisticamente significative ; identificazione del tumore tc / rm : accuratezza = 98% / 98% , sensibilit = 100% / 100% , specificit = 88% / 88% , vpp = 97% / 97% , vpn = 100% / 100% ; resecabilit del tumore tc / rm : accuratezza = 94% / 90% , sensibilit = 92% / 88% , specificit = 100% / 100% , vpp = 100% / 100% , vpn = 78% / 70% . 454 radiol med ( 2010 ) 115 : 453466 optimal imaging quality with good contrast resolution in evaluating the upper abdomen . keywords computed tomography magnetic resonance pancreatic masses identification resectability conclusioni . 
la rm rappresenta una valida alternativa diagnostica allesame tc nei pazienti con lesioni espansive del pancreas ; in particolare , la rm consente sia la corretta identificazione e caratterizzazione delle masse pancreatiche che la valutazione delleventuale resecabilit chirurgica in caso di malignit ; lalto campo magnetico delle nuove apparecchiature permette di ottenere unottima qualit delle immagini rm che mostrano unelevata risoluzione di contrasto nello studio delladdome superiore . parole chiave tomografia computerizzata risonanza magnetica masse pancreatiche identificazione resecabilit introduction introduzione noninvasive evaluation of pancreatic masses relies on several imaging modalities , such as ultrasonography , computed tomography ( ct ) , magnetic resonance ( mr ) imaging and ct combined with positron emission tomography ( pet - ct ) [ 1 , 2 ]  . 
technological advances in the field of ct have led to the development of multislice or multidetector imaging , with considerable improvements in the techniques diagnostic potential [ 3 ]  . 
moreover , mr imaging has been proposed as an alternative to ct , as the new highmagnetic - field scanners offer optimal contrast resolution for studying the upper abdomen [ 3 ]  . 
the choice between ct and mr imaging for diagnostic evaluation of pancreatic masses is controversial , as the majority of studies in the literature suggests that ct and mr imaging have comparable diagnostic accuracy [ 49 ] , whereas other studies report conflicting results [ 1013 ]  . pancreatic masses are solid or cystic expansile lesions that may be benign or malignant . 
the most common ( 95% ) malignancy is ductal adenocarcinoma , which arises more frequently in the pancreatic head and rarely in the body or tail [ 1417 ]  . 
patients with pancreatic adenocarcinoma present with nonspecific , subtle symptoms , and serological makers have little diagnostic significance , so that only 30% of tumours are potentially resectable at the time of diagnosis . 
surgery is in fact not an option in cases of invasion of vascular structures of the splenicmesenteric - portal axis , especially of the superior mesenteric the pancreatic vein due parenchyma , and in cases of advanced disease with hepatic , nodal , peritoneal and / or distant metastases . its close proximity the aim of our study was to compare the results of multila valutazione dei pazienti con masse pancreatiche mediante tecniche non invasive di diagnostica per immagini si avvale di diverse metodiche quali lecografia , la tomografia computerizzata ( tc ) , la risonanza magnetica ( rm ) e la tc abbinata alla tomografia ad emissione di positroni ( pet / tc ) [ 1 , 2 ]  . 
in particolare , linnovazione tecnologica in tc ha proposto la metodica multi - detettore o multi - slice ( mdct ) ampliandone notevolmente le potenzialit diagnostiche [ 3 ] ; inoltre , la rm stata proposta come tecnica alternativa allesame tc in quanto le nuove apparecchiature con campi magnetici di elevata intensit offrono unottima risoluzione di contrasto estremamente vantaggiosa nello studio delladdome superiore [ 3 ]  . 
attualmente , la scelta tra le due metodiche per la valutazione diagnostica dei pazienti con masse pancreatiche risulta controversa ; in base agli studi presenti in letteratura [ 49 ] , la maggioranza dei dati suggerisce unaccuratezza diagnostica simile della tc e della rm in tali pazienti , mentre alcuni studi mostrano risultati discordanti [ 1013 ]  . 
 le masse pancreatiche sono formazioni espansive con struttura di tipo solido o cistico , possono essere sia di natura benigna che maligna e , in particolare , tra le forme maligne quella pi frequente ( 95% ) rappresentata dalladenocarcinoma duttale ; la maggioranza di tali lesioni si localizza a livello della testa , mentre linteressamento del corpo e della coda pi raro [ 1417 ]  . 
i pazienti con adenocarcinoma del pancreas presentano una sintomatologia subdola e gli esami sierologici hanno scarso significato diagnostico , per cui solo nel 30% dei casi il tumore potenzialmente resecabile al momento della diagnosi . 
le principali problematiche diagnostiche nei pazienti con sospetto di tumore pancreatico sono rappresentate dallidentificazione della lesione e dalla valutazione della sua resecabilit radiol med ( 2010 ) 115 : 453466 slice computed tomography ( msct ) and mr imaging in detecting and evaluating resectability of expansile malignant lesions in a group of patients with pancreatic masses . materials and methods population over a period of 2 years , we prospectively evaluated 40 patients ( 22 men , 18 women ) aged 2872 ( mean age 6213 ) years with clinical and ultrasonographic evidence of a pancreatic mass . 
all patients gave informed consent , and the study protocol was approved by the institutional ethics committee . computed tomography ct examinations were performed with a four - detector row msct scanner ( mx 8000 - marconi ) with a rotation time of 0.5 s allowing acquisition of eight sections per second . 
da tutti i pazienti stato ottenuto consenso informato per lesecuzione degli esami di diagnostica per immagini dopo approvazione del progetto di studio da parte del comitato etico . tomografia computerizzata gli esami sono stati eseguiti con uno scanner mdct con 4 file di detettori ( mx 8000 - marconi ) con tempo di rotazione di 0 , 5 s che permette lacquisizione di 8 sezioni al secondo . 
tutti i pazienti sono stati invitati a bere , 1015 min prima dellesecuzione dellesame , 750 ml di acqua al fine di migliorare la definizione dei rapporti tra la regione cefalica del pancreas e la ii porzione duodenale . 
 stata eseguita una prima acquisizione in fase pre - contrastografica della regione pancreatica in direzione cranio - caudale dal diaframma fino alle creste iliache utilizzando i seguenti parametri : collimazione = 41 mm , intervallo di ricostruzione = 3 mm , pitch = 0 , 875 , kv = 120 , mas = 260 e campo di vista ( fov ) = 25 csuccessivamente in fase post - contrastografica sono state eseguite scansioni della regione pancreatica in senso craniocaudale utilizzando i seguenti parametri : collimazione = 41 mm , intervallo di ricostruzione = 1 , 25 mm , pitch = 0 , 875 , kv = 120 , mas = 260 e fov = 25 cm ; lacquisizione delle scansioni post - contrastografiche in fase arteriosa stata 456 radiol med ( 2010 ) 115 : 453466 material was achieved with an 18to 20 - gauge needle cannula placed in an antecubital vein of the aran initial unenhanced baseline scan of the pancreatic region was obtained in the craniocaudal direction from the diaphragm down to the iliac crests , with the following parameters : collimation 41 mm , reconstruction interval 3 mm , pitch 0.875 , kv 120 , mas 260 and field of view 25 c after contrast - medium administration , the pancreatic region was imaged in the craniocaudal direction using the following parameters : collimation 41 mm , reconstruction interval 1.25 mm , pitch 0.875 , kv 120 , mas 260 and field of view 25 c acquisition of scans in the arterial phase was synchronised with the passage of contrast through the arterial tree using real - time bolus tracking to calculate scan delay . 
the contrast medium used was nonionic iodinated iopromide ( ultravist , schering ) with an iodine concentration of 370 mgi / ml administered at a rate of 3 ml / s via an automatic power injector . magnetic resonance imaging mr study was performed with a 1.5 - tesla scanner ( philips , gyroscan intera )  . 
after receiving 900 ml of oral superparamagnetic contrast material consisting of a suspension of silicon - coated iron oxide crystals ( ferumoxil , lumirem , guebert ) , all patients were studied with dedicated t1and t2 - weighted breath - hold ( bh ) sequences using a phasedarray synergy body coil . 
precontrast t1 - weighted fast - field echo ( t1 ffe - bh ) without fat saturation sequences were acquired in the axial plane using the following parameters : tr / te 214 / 46 ms , flip angle 80 , matrix 192512 and slice thickness 5 mm ; t2 - weighted single - shot turbo spin echo ( ss - tse ) ( with and without fat saturation ) were acquired with tr / te 417 / 80 ms , flip angle 80 , matrix 192512 and slice thickness 5 m the examination was completed by the acquisition of a magnetic resonance cholangiopancreatography ( mrcprad - bh ) with a 40 - mm - thick single - slab half - fourier sequence , with acquisition matrix 256 , reconstruction matrix 256512 , field of view 25 cm , effective echo time ( teeff ) 1 , 050 ms and repetition time ( tr ) 2 , 600 ms . 
the t1 ffe - bh sequences were complemented with contrast - enhanced acquisitions using a multiphase dynamic technique with fat saturation and intravenous administration of 0.1 mmol / kg body weight of paramagnetic contrast medium ( gadopentetic acid , magnevist , schering )  . 
le sequenze t1 ffe - bh sono state infine integrate dalla fase post - contrastografica eseguita con soppressione del segnale del tessuto adiposo e somministrazione endovenosa con tecnica dinamica multifasica di mdc paramagnetico ( acido gadopentetico , magnevist , schering ) al dosaggio di 0 , 1 mmol / kg peso corporeo ; la tecnica dinamica multi - fasica prevedeva lacquisizione delle scansioni in fase arteriosa in sincronizzazione con il transito arterioso del mezzo di contrasto paramagnetico utilizzando la tecnica del bolus tracking in tempo reale per il calcolo del ritardo di scansione ; successivamente sono state acquisite le fasi di studio pancreatica ( 4045 s ) e portale ( 7080 s )  . analisi delle immagini le immagini ottenute sono state analizzate separatamente radiol med ( 2010 ) 115 : 453466 image analysis images were reviewed separately by two radiologists who read the ct and mr images , respectively . 
 each reader used a score from 1 to 5 for identifying and characterising the pancreatic masses ( 1 = definitely benign , 2 = probably benign , 3 = indeterminate , 4 = probably malignant , 5 = definitely malignant )  . 
the readers also evaluated the resectability of the malignant lesions ( n = 32 ) , according to previously reported criteria [ 18 ] , using a score from 1 to 3 ( 1 = resectable , 2 = indeterminate , 3 = unresectable )  . 
malignant masses were considered unresectable in all cases of direct or indirect evidence of peripancreatic vascular involvement . vessels evaluated were the coeliac trunk , mesenteric vessels ( vein and artery ) and splenic - mesenteric - portal confluence . direct signs of vascular invasion were the degree of circumferential involvement ( > 180 ) or a tear - drop appearance of involved vessels . 
involvement of the splenic vessels ( artery and vein ) was considered to be an absolute contraindication for surgical resection . other unresectability criteria were the invasion of adjacent tissues or organs , the presence of distant metastasis and the presence of peritoneal carcinosis . results of the ct and mr imaging studies were compared with biopsy ( n = 33 ) and / or histology ( n = 7 ) , which were considered the reference standards against which the diagnostic accuracy of ct and mr imaging was measured . in particular , histological reports were available for all resectable malignancies , whereas biopsy reports were available for unresectable malignancies or patients with chronic pancreatitis . 
in particular , we tested whether there was a statistically significant difference between results provided by the two modalities , as confirmed by the reference standards . results results of the ct and mr imaging studies in patients with ductal adenocarcinoma or cystic tumours of the pancreas , along with biopsy ( n = 25 ) and / or histology ( n = 7 ) results , are da due radiologi che hanno interpretato rispettivamente le scansioni tc e rm ; gli osservatori hanno valutato indipendentemente le immagini e nella loro analisi non erano a conoscenza dei dati clinico - ecografici dei pazienti ; in caso di discordanza dei risultati della valutazione delle scansioni tc e / o rm , un terzo osservatore stato invitato a valutare ulteriormente le immagini . 
 ciascun osservatore ha utilizzato un punteggio da 1 a 5 per lidentificazione e la caratterizzazione delle masse pancreatiche ( 1 = sicuramente benigna , 2 = probabilmente benigna , 3 = indeterminata , 4 = probabilmente maligna , 5 = sicuramente maligna )  . 
gli osservatori hanno inoltre valutato la resecabilit o meno delle lesioni nei pazienti con neoplasia maligna ( n = 32 ) in base a criteri precedentemente utilizzati [ 18 ] ; stato impiegato un punteggio da 1 a 3 ( 1 = resecabile , 2 = indeterminato , 3 = non resecabile ) ; le masse maligne sono state considerate certamente non resecabili in tutti i casi in cui esisteva unevidenza diretta o indiretta di coinvolgimento vascolare peri - pancreatico ; i vasi valutati sono stati il tripode celiaco , i vasi mesenterici ( vena e arteria ) e la confluenza spleno - mesenterico - portale ; i segni diretti di infiltrazione vascolare erano rappresentati dal grado di coinvolgimento circonferenziale ( > 180 ) o dalla deformazione di calibro a goccia dei vasi interessati ; segni indiretti di infiltrazione vascolare sono stati considerati lectasia delle arcate pancreatico - duodenali e / o del tronco venoso gastrocolico ; il coinvolgimento dei vasi splenici ( arteria e vena ) non stato considerato controindicazione assoluta alla resezione chirurgica ; altri criteri di non resecabilit delle lesioni maligne sono stati linfiltrazione dei tessuti e / o degli organi adiacenti al pancreas e / o la presenza di metastasi a distanza o , infine , la presenza di carcinosi peritoneale . 
 i risultati degli esami tc ed rm sono stati confrontati con i dati bioptici ( n = 33 ) e / o istologici ( n = 7 ) , considerati lo standard di riferimento per lattribuzione del risultato vero o falso delle immagini tc e / o rm ; in particolare , i dati istologici sono stati disponibili nei casi di tumori maligni resecabili , mentre i dati bioptici sono stati ottenuti nei casi di tumori non resecabili o nei pazienti con pancreatite cronica ; gli esami bioptici con ago sottile sono stati eseguiti sotto guida tc . 
successivamente sono stati calcolati per le due metodiche i valori di sensibilit , specificit , ed accuratezza diagnostica e i valori predittivo positivo e negativo sia per lidentificazione del tumore pancreatico che per la sua resecabilit . 
in the remaining eight patients , the pancreatic masses corresponded to tissue degeneration due to chronic pancreatitis , which was diffuse in the majority of patients ( 7 / 8 cases ) and focal in one case only . with regard to identification and localisation of pancreatic masses , the overall results of ct and mr imaging are shown in table 4 . 
figure 1 shows and example of concordant findings of ct and mr imaging in a patient with resectable serous cystadenoma of the pancreatic tail ( patient 8 , table 3 )  . 
figure 2 shows an example of concordance between ct and mr imaging in a patient with a resectable intraductal mucinous papillary neoplasm in the pancreatic body ( patient 7 , table 3 )  . i risultati degli esami tc e rm nei pazienti con adenocarcinoma duttale o con tumori cistici del pancreas sono illustrati rispettivamente nelle tabelle 2 e 3 ; sono inoltre riportati i dati relativi al risultato della biopsia ( n = 25 ) e / o dellistologia ( n = 7 )  . 
sono stati riscontrati 31 casi di tumori maligni pancreatici , di cui 24 adenocarcinomi duttali , 6 cistoadenocarcinomi mucinosi e 1 tumore mucinoso papillifero intraduttale ; in un caso la lesione era di tipo benigno , cistoadenoma sieroso . 
thus , the diagnostic accuracy of ct and mr imaging in the judgement of tumour resectability was similar , with values of 94% and 90% , respectively ( p = not significant )  . 
there were two cases in which both ct and mr imaging provided a false negative result , and one case in which mr imaging only provided a false negative result . 
3 shows an example of concordance between ct and mr imaging in a patient with unresectable adenocarcinoma of the pancreatic body with invasion of the coeliac trunk ( patient 17 , table 2 )  . neoplastica sia alla tc che alla rm . 
la figura 1 mostra un esempio di risultato concordante tra tc e rm in un paziente con cistoadenoma sieroso resecabile della coda del pancreas ( n = 8 , tabella 3 )  . 
la figura 2 mostra un esempio di risultato concordante tra tc e rm in una paziente con tumore mucinoso papillifero intra - duttale resecabile del corpo del pancreas ( n = 7 , tabella 3 )  . per quanto riguarda la valutazione della potenziale resecabilit dei tumori pancreatici , i risultati globali della tc e della rm sono riportati nella tabella 5 . 
sono stati osservati in totale 25 pazienti con tumori pancreatici non resecabili , 13 pazienti presentavano infiltrazione neoplastica di entrambi i vasi mesenterici , in un caso erano presenti anche metastasi epatiche ; 9 pazienti hanno mostrato coinvolgimento neoplastico della sola vena mesenterica superiore , con anche in questo gruppo un solo caso di metastasi epatiche ; 1 paziente , con una neoplasia del corpo pancreatico , mostrava infiltrazione del tripode celiaco ; infine , in 2 pazienti la non resecabilit del tumore era dovuta alla presenza di metastasi epatiche . 
malignancies accounted for 78% of cases in our series and included 24 ductal adenocarcinomas , six cystadenocarcinomas and one intraductal mucinous papillary neoplasoverall , ct and mr imaging had similar diagnostic accuracy . 
considering that the most common pancreatic malignancy is ductal adenocarcinoma , a delle lesioni neoplastiche risultata simile , rispettivamente 94% e 90% ( p = non significativo [ ns ] ) ; sono stati osservati due casi in cui il risultato sia della tc che della rm stato falsamente negativo , mentre in un caso solo il risultato della rm stato falsamente negativo ; la minima differenza in accuratezza diagnostica tra tc e rm non ha mostrato significativit statistica . 
la figura 3 mostra un esempio di risultato concordante tra tc e rm in una paziente con adenocarcinoma non resecabile del corpo del pancreas con infiltrazione del tripode celiaco ( n = 17 , tabella 2 )  . radiol med ( 2010 ) 115 : 453466 table 4 performance of multislice computed tomography ( msct ) and magnetic resonance imaging ( mri ) in identifying pancreatic tumours discussione msct tabella 4 risultati degli esami dimaging nella identificazione del tumore pancreatico sensitivity ( % ) specificity ( % ) positive predictive value ( % ) negative predictive value ( % ) accuracy ( % ) p = not significant sensibilit ( % ) specificit ( % ) valore predittivo positivo ( % ) valore predittivo negativo ( % ) accuratezza ( % ) p = non significativa fatal cancer that is potentially curable by surgical resection [ 16 , 17 ] , an early diagnosis and accurate evaluation of resectability are fundamental . 
despite availability of numerous diagnostic modalities , the majority of lesions are generally detected at an advanced stage , as the patient is initially asymptomatic and does not undergo diagnostic investigations . 
on the other hand , symptomatic patients oggetto di trattazione la nostra esperienza in una valutazione comparativa tra tc e rm nel localizzare e caratterizzare in termini di resecabilit chirurgica le lesioni espansive maligne del pancreas ; nel nostro studio le lesioni maligne costituivano il 78% dei casi ed erano rappresentate da 24 adenocarcinomi duttali , 6 neoplasie maligne di tipo cistico ed 1 tumore mucinoso papillifero intraduttale . 
globalmente , i risultati della nostra valutazione hanno dimostrato unaccuratezza diagnostica analoga della tc e della rm sia nella localizzazione che nella formulazione del giudizio di resecabilit delle masse maligne ; tra queste essendo ladenocarcinoma duttale del pancreas la neoplasia pi frequente con elevata mortalit in cui la completa resezione chirurgica costituisce lunico trattamento terapeutico potenzialmente efficace [ 16 , 17 ] , gli aspetti diagnostici fondamentali sono la diagnosi precoce e laccurata valutazione della sua resecabilit . 
attualmente , nonostante la disponibilit di numerose metodiche diagnostiche la maggior parte delle lesioni generalmente identificata in fase avanzata in quanto inizialmente il paziente non sintomatico per cui gli esami di diagnostica per immagini non sono eseguiti ; al contrario , nel caso di pazienti sintomatici spesso non possibile intervenire terapeuticamente in quanto gli esami diagnostici dimostrano infiltrazione vascolare loco - regionale o la presenza di metastasi a distanza . 
1a , b a 48 - year - old man with resectable serous cystadenoma of the pancreatic tail with concordant ct and mr imaging results ( patient 8 , table 3 )  . 
a axial ct image obtained in the portal phase after intravenous administration of contrast agent shows a large ( 8 cm ) and homogeneous cystic lesion of the pancreatic tail with regular margins suggestive of a benign mass . 
1a , b paziente maschio di 48 anni con cistoadenoma sieroso resecabile della coda del pancreas con risultato concordante degli esami tc ed rm ( n = 8 , tabella 3 )  . 
a limmagine assiale tc multistrato ottenuta in fase portale dopo la somministrazione del mezzo di contrasto iodato endovena mostra una grossolana formazione espansiva di tipo cistico localizzata a livello della coda pancreatica , di circa 8 cm , con margini netti e regolari e contenuto omogeneo , caratteristiche dunque indicative di benignit . 
b limmagine rm single - shot t2 tse ottenuta in scansione assiale mostra un risultato analogo a quello della tc in quanto la lesione presenta la tipica ed omogenea iperintensit di segnale delle formazioni cistiche di tipo benigno . 462 radiol med ( 2010 ) 115 : 453466 fig . 
2a - c a 71 - year - old woman with resectable intraductal mucinous papillary tumour of the pancreatic body with concordant ct and mr imaging results ( patient 7 , table 3 )  . 
a axial ct image obtained in the portal phase after intravenous administration of contrast agent shows a small ( 2 cm ) , oval , hypodense lesion with cystic features in apparent communication with wirsungs duct and collateral ducts at the level of the pancreatic body . 
2a - c paziente femmina di 71 anni con tumore mucinoso papillifero intraduttale resecabile del corpo del pancreas con risultato concordante degli esami tc ed rm ( n = 7 , tabella 3 )  . 
a limmagine assiale tc multistrato ottenuta in fase portale dopo la somministrazione del mezzo di contrasto mostra una piccola lesione intra - parenchimale , di morfologia ovalare , nettamente ipodensa , di circa 2 cm , con dunque caratteristiche di tipo cistico in apparente comunicazione con il dotto di wirsung a livello del corpo pancreatico e con i dotti collaterali di pari livello . 
b limmagine assiale rm t1 pesata ottenuta in fase portale dopo la somministrazione del mezzo di contrasto paramagnetico con soppressione del segnale del tessuto adiposo mostra un risultato perfettamente sovrapponibile rispetto alla tc ; la lesione appare tipicamente ipointensa come da componente cistica con analoghi rapporti con le strutture duttali . 
c limmagine rm single - shot t2 tse in scansione assiale in fase pre - contrastografica conferma il risultato delle due precedenti immagini mostrando il segnale tipicamente iperintenso della lesione analogo al segnale delle strutture duttali con cui appare in comunicazione . often cannot be treated because the diagnostic investigations show locoregional vascular invasion or distant metastases . 
 ultrasonography represents the first - line investigation , as it is widely available , noninvasive and allows complete evaluation of the upper abdomen , which is useful for locoregional staging of neoplastic masses . 
consequently , in patients with pancreatic masses , ultrasonography must necessarily be integrated by a second - line investigation such as ct or mr imaging [ 13 ]  . invasivo e consente una valutazione completa degli organi delladdome superiore , utile nella stadiazione loco - regionale delle masse neoplastiche ; tuttavia , essa pu presentare alcune limitazioni tecniche nei pazienti obesi , anche il meteorismo intestinale pu interferire con la qualit delle immagini ecografiche ed inoltre essendo una tecnica fortemente operatore - dipendente pu essere influenzata dalla maggiore o minore esperienza nellesecuzione dellesame , pertanto nei pazienti con masse pancreatiche certamente lesame ecografico deve essere integrato da una tecnica di secondo livello diagnostico quale la tc o la rm [ 13 ]  . ct is the most commonly employed imaging modality la tc la tecnica di imaging pi utilizzata per la radiol med ( 2010 ) 115 : 453466 table 5 performance of multislice computed tomography ( msct ) and magnetic resonance imaging ( mri ) in the evaluation of the pancreatic tumour resectability msct tabella 5 risultati degli esami dimaging nella valutazione della possibile resecabilit o non resecabilit dei tumori pancreatici sensitivity ( % ) specificity ( % ) positive predictive value ( % ) negative predictive value ( % ) accuracy ( % ) p = not significant sensibilit ( % ) specificit ( % ) valore predittivo positivo ( % ) valore predittivo negativo ( % ) accuratezza ( % ) p = non significativa for the identification and preoperative staging of pancreatic malignancies , where it is highly reliable in determining the unresectability of lesions [ 3 , 20 , 21 ]  . 
ct imaging exploits the difference between arterial hypervascularity of the pancreas and hypovascularity of the ductal adenocarcinoma identificazione e la stadiazione pre - operatoria delle masse pancreatiche maligne mostrando unelevata accuratezza nella determinazione della non resecabilit delle lesioni [ 3 , 20 , 21 ]  . 
la tc sfrutta la differenza tra la ricca vascolarizzazione di tipo arterioso del pancreas e lipovascolarizzazione delladenocarcinoma duttale per ottenere , dopo aver raggiunto la massima impregnazione del parenchima ghiandolare , lottimale differenza di contrasto tra tumore e tessuto pancreatico sano ; inoltre , lopacizzazione dei vasi peri - pancreatici essenziale per lidentificazione del coinvolgimento vascolare e lestensione loco - regionale del tumore . 
negli ultimi anni sono stati proposti diversi protocolli di acquisizione tc per lo studio delle lesioni pancreatiche maligne , allo scopo di migliorare laccuratezza globale della metodica sia nellidentificazione che nella valutazione della sua resecabilit [ 22 ]  . 
lacquisizione multi - fasica , in fase arteriosa ( 2530 s ) , pancreatica ( 4045 s ) e portale ( 7080 s ) rappresenta lapproccio metodologico ottimale consentendo di acquisire informazioni diagnostiche sulla presenza della neoplasia e riguardo i rapporti della lesione con le strutture vascolari arteriose e venose adiacenti , requisito questultimo indispensabile ai fini di una corretta pianificazione pre - operatoria . 
in particolare , la recente introduzione nella pratica clinica della tc multidetettore ha notevolmente ampliato le potenzialit diagnostiche della tecnica e anche se i risultati di uno studio recente hanno mostrato che la qualit diagnostica delle fig . 
3a , b a 73 - year - old man with unresectable adenocarcinoma of the pancreatic body and evidence of coeliac trunk infiltration with concordant ct and magnetic resonance ( mr ) imaging results ( patient 17 , table 2 )  . 
a axial ct image obtained in the portal phase after intravenous administration of contrast agent shows a large and irregular lesion originating from the anterior border of the pancreatic body with vascular infiltration of the celiac trunk , which appears proximally dilated and tortuous and indistinguishable from the antral - pyloric region . 
3a , b paziente maschio di 73 anni con adenocarcinoma non resecabile del corpo del pancreas per infiltrazione del tripode celiaco con risultato concordante degli esami tc ed rm ( n = 17 , tabella 2 )  . 
a limmagine assiale tc multistrato ottenuta in fase portale dopo la somministrazione del mezzo di contrasto mostra una formazione espansiva di morfologia irregolare ad origine dal profilo anteriore del corpo pancreatico che infiltra il tripode celiaco che appare ectasico e tortuoso nel suo tratto prossimale , risultando non dissociabile dalla regione antrale - pilorica . 
b limmagine assiale rm t1 pesata ottenuta in fase portale dopo la somministrazione del mezzo di contrasto paramagnetico con soppressione del segnale del tessuto adiposo mostra un risultato analogo a quello della tc . 464 radiol med ( 2010 ) 115 : 453466 to achieve , after maximal enhancement of the pancreatic parenchyma , optimal differentiation between the lesion and the healthy pancreatic tissue . 
in recent years , several ct protocols have been proposed to improve the overall accuracy of ct in identifying and evaluating the resectability of pancreatic malignancies [ 22 ]  . 
multiphase acquisition with scans in the arterial ( 2530 s ) , pancreatic ( 4045 s ) and portal ( 7080 s ) phases is an excellent technique that provides diagnostic information on the presence of the tumour and its relationship with adjacent arterial and venous structures a crucial requirement for preoperative planning . 
in particular , the recent introduction of multidetector ct has considerably expanded the techniques diagnostic potential and , even though it has recently been demonstrated that the diagnostic quality of images obtained with multislice and single - slice ct is comparable , multislice ct has the advantage of significantly faster acquisition times [ 20 ]  . mr imaging has been suggested as an alternative to ct in the diagnostic evaluation of patients with pancreatic masses , as it offers accurate locoregional anatomical assessment of both parenchymal and vascular structures with high contrast resolution . 
t1 - weighted volumetric gradient - echo sequences acquired with a multiphase dynamic technique after intravenous administration of paramagnetic contrast medium allow simultaneous visualisation of the pancreatic vasculature and parenchyma in patients with malignancies . finally , the dedicated cholangiographic sequence depicts the anatomy of bile and pancreatic ducts with high contrast resolution [ 3 , 23 , 24 ]  . 
in addition , the short acquisition time of the sequences allows for fewer technical artefacts and better image quality , which is further improved by highfield - strength systems and the use of multichannel coils that provide very good contrast resolution . the overall concordance we observed between ct and mr imaging , as demonstrated by the lack of statistical significance of the small differences identified , is similar to that reported by previous studies . 
 [ 9 ] in patients with intraductal papillary mucinous neoplasms , and similar results were also reported for other types of pancreatic neoplasms , such as islet cell tumours of the pancreas [ 7 ]  . 
in contrast , a immagini acquisite con tecnica tc multistrato comparabile a quella delle immagini acquisite con tc a singolo strato , giocano a favore della prima i tempi significativamente ridotti di acquisizione delle immagini [ 20 ]  . la rm stata proposta come tecnica alternativa allesame tc nella valutazione diagnostica dei pazienti con masse pancreatiche offrendo unaccurata valutazione anatomica loco - regionale sia delle strutture parenchimali che vascolari con una elevata risoluzione di contrasto ; in particolare , la sequenza volumetrica t1 pesata gradientecho acquisita dopo la somministrazione endovenosa di mezzo di contrasto paramagnetico , con tecnica dinamica multi - fasica , consente simultaneamente la valutazione angiografica e parenchimografica delle lesioni neoplastiche in pazienti con tumori pancreatici maligni ; infine , la sequenza dedicata colangiografica riproduce con elevata risoluzione di contrasto lanatomia delle vie biliari e dei dotti pancreatici [ 3 , 23 , 24 ]  . 
in particolare , levoluzione tecnologica delle apparecchiature rm attualmente utilizzate consente di eseguire lesame delladdome in tempi ragionevolmente rapidi con sequenze veloci in apnea respiratoria della durata di pochi secondi certamente confortevoli per il paziente ; del resto la rapidit di esecuzione delle sequenze impiegate permette inoltre di ridurre gli artefatti tecnici con un significativo aumento della qualit delle immagini , ulteriormente migliorata dai campi magnetici di elevata intensit e dallimpiego delle bobine multi - canale che consentono di ottenere immagini di ottima qualit con risoluzione di contrasto certamente favorevole . la concordanza globale dei risultati osservati nel nostro studio tra tc ed rm , supportata dalla non significativit statistica delle minime differenze nei valori diagnostici delle due tecniche , risulta simile ai dati riportati in altri studi di confronto fra le due metodiche ; in dettaglio , sheridan et al . [ 4 ] hanno riscontrato risultati comparabili tra tc e rm nellidentificazione dei tumori pancreatici , con una superiorit della rm rispetto alla tc nel giudizio di resecabilit delle lesioni ; arslan et al . 
 [ 5 ] hanno osservato unanaloga efficacia della tc e della rm nella valutazione dellinfiltrazione vascolare dei tumori pancreatici ; risultati concordanti tra tc e rm sono stati inoltre osservati da fukukura et al . 
 [ 9 ] in pazienti con tumori mucinosi papilliferi intraduttali ; risultati simili tra tc ed rm sono stati infine riportati anche in altri tipi di tumori del pancreas , quali le lesioni maligne pancreatiche di tipo endocrino [ 7 ]  . 
 [ 10 ] suggeriscono la rm rispetto alla tc come esame di scelta in pazienti con piccoli ( 2 cm ) adenocarcinomi del pancreas ; analogamente , nello studio di andersson et al . 
 [ 11 ] la rm risulta maggiormente accurata della tc nella differenziazione tra lesioni benigne e maligne in pazienti con tumori radiol med ( 2010 ) 115 : 453466 number of studies in the literature have reported conflicting results . 
 [ 13 ] showed that mr imaging has better diagnostic performance than ct for differentiating intraductal papillary mucinous neoplasms from other cystic lesions of the pancreas . in our study , in the evaluation of lesion resectability , both ct and mr imaging produced false negative results in two malignant lesions of the pancreatic head ( a ductal adenocarcinoma and a mucinous cystadenocarcinoma ) , as the involved vessels had preserved flow signal . 
despite these erroneous results of both ct and mr imaging , statistical analysis did not reveal statistically significant differences between modalities in identifying or evaluating resectability of malignant masses , so we may hypothesise that either technique can be used in these patients , depending on availability . 
however , because our study was limited by a small study sample affected by neoplastic lesions of different histological type , our preliminary results need to be validated by larger studies conducted on more homogeneous patient populations . in conclusion , on the basis of our experience and the results reported in the literature we believe that mr imaging of the pancreas performed with state - of - art - equipment and a dedicated study protocol represents a valuable alternative to ct in the diagnostic assessment of patients with pancreatic masses as it provides both accurate identification and characterisation of lesions and an appropriate evaluation of resectability in the case of malignant masses . periampullari ; mehmet erturk et al . 
 [ 12 ] hanno dimostrato una superiorit della tc multistrato integrata con ricostruzioni multiplanari rispetto alla rm sia per la diagnosi che per la valutazione della estensione loco - regionale di malattia ; infine , song et al . 
 [ 13 ] hanno dimostrato che la rm ha una migliore capacit diagnostica nel differenziare rispetto alla tc i tumori mucinosi papilliferi intra - duttali da altri tipi di lesioni cistiche del pancreas . nel nostro studio , nella valutazione del giudizio di resecabilit delle lesioni maligne , in due casi di neoplasie maligne della testa pancreatica ( un adenocarcinoma duttale ed un cistoadenocarcinoma mucinoso ) sia il risultato della tc che quello della rm stato falsamente negativo in quanto i vasi coinvolti mostravano nelle immagini segnale di flusso conservato ; in un solo paziente , il risultato falsamente negativo ha riguardato unicamente la rm . 
infine , in un paziente affetto da pancreatite cronica focale il risultato sia della tc che della rm stato falsamente positivo per massa neoplastica di tipo maligno ; a tale proposito , a tutti noto come lincremento volumetrico ed il dimorfismo propri della pancreatite cronica di tipo focale possano simulare una neoplasia maligna [ 25 ]  . 
nonostante questi risultati incorretti , sia della tc che della rm , lanalisi statistica dei dati non ha mostrato differenze statisticamente significative tra le due metodiche , sia per identificazione che per il giudizio di resecabilit delle masse maligne , per cui ipotizzabile in base alla disponibilit un uso alternativo di entrambe le tecniche in tali pazienti ; necessario , tuttavia , sottolineare un limite del nostro studio rappresentato da una casistica di pazienti non ampia , comprendente tra laltro lesioni neoplastiche di diverso tipo istologico , per cui per confermare i nostri risultati preliminari sono necessari ulteriori studi di confronto su gruppi di pazienti pi numerosi ed omogenei per patologia . in conclusione , possiamo certamente suggerire , sia in base alla nostra esperienza che ai risultati degli studi riportati in letteratura , che la rm del pancreas , eseguita con le pi avanzate apparecchiature e con protocollo dedicato , rappresenta attualmente una valida alternativa allesame tc nella valutazione diagnostica dei pazienti con masse pancreatiche , sia per laccurata identificazione e caratterizzazione delle lesioni che per un appropriato giudizio di resecabilit chirurgica in caso di malignit . conflict of interest none 1 . 
guney1 1department of radiology , maltepe university school of medicine , maltepe , i 2department of radiology , haydarpasa numune training and research hospital , kadiky , i correspondence to : r . 
cubuk , feyzullah cad , no : 39 , 34843 , maltepe , i fax : + 90 - 216 - 3830271 , e - mail : rahmicubuk@yahoo.com stanbul , turkey stanbul , turkey , tel . : + 90 - 216 - 3999 - 7502016 , stanbul , turkey received : 24 march 2009 / accepted : 11 may 2009 / published online : 15 january 2010 springer - verlag 2010 abstract purpose . 
the mammograms were retrospectively reviewed for overall breast density according to the four - point scale ( iiv ) of the breast imaging reporting and data system ( bi - rads ) classification . 
in questo studio retrospettivo sono state incluse 26 pazienti ( media di et 51 , 5411 , 5 ; range 3779 anni ) , sottoposte sia a rm sia a mammografia convenzionale . 
la percentuale di valori con intensit del segnale aumentato durante i primi minuti non risultata variare in rapporto alla densit mammografica del seno , e i valori radiol med ( 2010 ) 115 : 434441 kinetic features of the different groups based on bi - rads breast density category and menopausal status were similar . 
 keywords breast breast density mammography magnetic resonance imaging medi di velocit di enhancement in fase precoce sono risultati simili tra i gruppi di densit del seno ( p = 0 , 942 )  . non sono emerse differenze significative tra gruppi pre e post - menopausa . le cinetiche di enhancement dei differenti gruppi basati sulla classificazione di densit del seno ( bi - rads ) e sullo stato menopausale , sono risultati simili . 
non abbiamo rilevato correlazione tra la densit del seno in mammografia e il cosiddetto background enhancement in risonanza magnetica , n per quanto riguarda donne in pre - menopausa , n in postmenopausa . 
il tessuto fibroghiandolare in rm non pu essere correlato alla densit mammaria mammografica . parole chiave seno densit mammaria mammografia immagini di risonanza magnetica introduction radiographically , the breast consists mainly of two component tissues : fibroglandular tissue and fat . 
it is different from the other breastscreening modalities ( conventional mammography and ultrasonography ) in that it adds functional information to the morphological data on normal fibroglandular tissue ( nft ) [ 12 ]  . 
in addition , we questioned the predictability of nft contrastenhancement dynamics at mr mammography according to mammographic breast density . materials and methods patients seventy - nine patients who underwent both mr mammography and conventional mammography at our institution were included in this retrospective study . 
we excluded women who were in the perimenopausal period ( n = 2 ) , in the third or fourth week of their menstrual cycle ( n = 14 ) , had an irregular cycle ( n = 12 ) , were postmenopausal and on hormone replacement therapy at the time of the study and / or within the previous 6 months ( n = 12 ) and who had received chemotherapy within the previous 6 months . 
as premenopausal women usually undergo breast mr imaging and conventional mammography between the fifth and 12th day after the start of the menstrual cycle , the same time frame was used [ 13 , 19 , 20 ]  . 
patients with breast cancer underwent mr mammography for preoperative staging ( n = 3 ) , for evaluating the remaining breast after mastectomy ( n = 4 ) and for examining both breasts after conservative breast surgery ( n = 3 )  . 
in patients with breast cancer , evaluations were performed on the other breast , which was not affected by cancer or radiation therapy . patients without breast cancer underwent mr mammography as a problem - solving tool to characterise lesions detected at ultrasonography and conventional mammography . 
in these cases , evaluation was not performed on the breast with suspicious lesions but on the contralateral breast . with the criteria described above , only one breast for each patient was included in the study . mr mammography breast mr imaging was performed on a 1.5 - t imager ( intera , philips medical systems , best , the netherlands ) with a dedicated double - breast surface coil and bilateral scans . 
an additional transverse t2 - weighted fat suppressed spin echo sequence ( te / tr 110 / 7548 ms ; inversion delay spair 80 ms ; flip angle 90 ; fov 380380 mm2 , acquired voxel size 1.061.743.0 mm3 , reconstructed voxel size 0.940.943.00 mm3 , total acquisition time 242 s ) was performed before administration of contrast material . 
postcontrast three - dimensional t1 - weighted fast gradient - echo dynamic mr images were acquired after administration 0.1 mmol / kg gadolinium diethylenetriamine pentaacetic acid ( gd - dtpa )  . 
 image interpretation one author ( bn ) retrospectively reviewed the conventional mammography results for overall breast density according to the four - point scale ( iiv ) of the breast imaging reporting and data system ( bi - rads ) classification [ 21 ]  . the density scoring system has four categories : bi - rads 1 indicates a predominantly fatty breast , bi - rads 2 scattered fibroglandular densities , bi - rads 3 heterogeneous density fig . 
1 enhancement del tessuto fibroghiandolare normale in un seno normale : il tessuto si impregna gradualmente durante la fase iniziale , ma continua anche nelle fasi successive . radiol med ( 2010 ) 115 : 434441 determination of the signal intensity of normal glandular tissue before and after injection of gadopentetate dimeglumine . 
the early - phase enhancement rate was calculated according to the enhancement formula [ ( si postsi pre / si pre ) ] 100% ( si pre : baseline signal intensity , si post : signal intensity after contrast injection )  . at dynamic mr mammography , be was evaluated visually in all the postcontrast series of the same breast of each patient and enhancement kinetic features were analysed . patients were divided into four subgroups according to be [ 12 ]  . 
if nft enhanced strongly and diffusely , it was categorised as severe be ; slight or no enhancement ( even in the late postcontrast phase ) was defined as absent or minimal be . 
to compare preand postmenopausal patients , we used the mannwhitney u test , and to compare bi - rads breastdensity groups ( 2 , 3 and 4 ) we used the kruskalwallis test . to compare the relationship between breast - density groups and contrast pattern ( initialand late - enhancement phases ) and be , e used the chi - square test . results at conventional mammography , there were 11 cases ( 42% ) with bi - rads breast density category 2 , nine ( 35% ) with bi - rads category 3 and six ( 23% ) with bi - rads category 4 . 
patients with bi - rads 4 were all in the premenopausal period , and the age range was 3749 years . no patient was considered to have fatty breast parenchyma ( table 1 )  . 
the difference between the two groups was statistically significant ( p = 0.001 ) ( table 2 ) during enhancement kinetic curve assessment , two cases ( 8% ) were had medium contrast enhancement at the initial phase , whereas slow enhancement was determined in the remaining 24 cases ( 92% )  . 
2 curva tempo - intensit del segnale della dinamica contrastografica , basata sulle caratteristiche cinetiche di impregnazione in rm secondo lamerican college of radiology brest imaging reporting end data system bi - rads -  . and bi - rads 4 extremely dense breast tissue . mr images were interpreted by two radiologists experienced in breast mr imaging , who were blinded to the mammographic breast density . 
two authors ( rc , nt ) with 4 and 7 years experience , respectively , reading breast mr images reviewed the studies to reach a consensus regarding the findings . 
before be assessments nft , enhancement kinetic features ( enhancement curve , early - phase enhancement rate ) were measured in a region of interest ( roi ) containing entirely nft to evaluate contrast - medium enhancement at 06 min after gadopentetate dimeglumine injection . 
enhancement kinetic curve evaluation was based on the initial phase ( within the first 2 min or when the curve began to change ) and the late phase ( after 2 min or after the change )  . 
with these results , we concluded that enhancement kinetic features of the different groups , which were created according to bi - rads breast density category and menopausal status , were similar . be values were mild in five cases ( 19% ) , moderate in 13 ( 50% ) and severe in eight ( 31% )  . 
in 14 premenopausal cases , moderate enhancement was defined in six and severe enhancement in eight , whereas 12 postmenopausal cases showed moderate ( n = 7 ) or mild ( n = 5 ) enhancement ( table 1 )  . 
after the contrast - medium injection , in the early few minutes , breast cancer shows a contrast enhancement peak because of its highly vascularised structure , which helps delineate its borders on nft in this particular phase . 
however , sometimes , nft may enhance quickly and intensely in the initial phase and may mask the underlying cancer [ 8 , 12 , 17 ]  . therefore , initial studies in the 1990s claimed that mr mammography had low sensitivity , especially in women with secretory diseases , inflammatory processes , proliferating changes or who were premenopausal [ 27 , 28 ]  . nonetheless , recent studies have shown that for detecting breast cancer , mr imaging has the greatest sensitivity of all imaging techniques [ 9 , 11 , 25 ]  . 
especially in cases of diffusely growing invasive cancers or in medullar cancers with benign morphological appearance , mr mammography has greater sensitivity compared with conventional mammography [ 2932 ]  . 
compared with the postmenopausal group , higher mammographic breast density premenopausal women may cause difficulties in detection or may obscure the cancer in conventional mammography imaging method is an effective [ 24 ]  . 
in our study , to equalise the hormonal factors affecting be , mr mammography and conventional mammography were performed between the fifth and 12th day of the menstrual cycle in all premenopausal cases . 
3 confronto tra valori medi di enhancement in fase precoce in donne in pre e post - menopausa . this study had a limited number of subjects because it is difficult to recruit patients who underwent both conventional and mr mammography during the same period of their cycle . 
zompatori1 1department of radiology , 2department of digestive diseases and internal medicine , 3department of surgery , santorsola - malpighi hospital , university of bologna , via massarenti 9 , 40138 bologna , italy correspondence to : l . 
this study was performed to describe the possible presence of extrapancreatic neoplasms in patients with intraductal papillary mucinous neoplasm ( ipmn ) and to evaluate whether the extrapancreatic tumours were synchronous or metachronous to ipmns . 
one hundred and forty - two patients ( 56 men and 86 women ; mean age 69.5 years , range 3798 ) with ipmn diagnosed using the sendai criteria were enrolled . 
sono stati studiati 142 pazienti con diagnosi di npi utilizzando i criteri di sendai ; dei 142 pazienti , 56 erano maschi e 86 femmine ; let media era di 69 , 5 anni ( range 3798 ) anni . 
la dimensione media della lesione cistica era ( mediadeviazione standard [ ds ] ) 1 , 91 , 9 cm ( range 0 , 58 , 0 cm )  . 
la distribuzione delle varie malattie pancreatiche o extrapancreatiche era simile nelle npi tipo i , ii e iii ( p = 0 , 776 )  . radiol med ( 2010 ) 115 : 442452 extrapancreatic cancers occur before the diagnosis of ipmns is made and is not related to the type of ipmn . keywords pancreatic diseases intraductal papillary mucinous tumours pancreas chronic pancreatitis neoplasms radiology conclusioni . 
la maggior parte dei tumori pancreatici o extrapancreatici si manifesta prima della diagnosi di npi e non correlato al tipo di npi . parole chiave malattie pancreatiche neoplasie papillari intraduttali papillari mucinose del pancreas pancreatite cronica neoplasie radiologia introduction introduzione intraductal papillary mucinous tumours ( ipmns ) of the pancreas were first described in the 1980s by ohhashi et al . [ 1 , 2 ] as mucin - producing tumours of the pancreas . 
these tumours arise from the epithelium of the pancreatic ducts with the production of atypical mucin and segmental or diffuse dilation of the main pancreatic duct ( mpd ) , cystic dilation of the secondary branches or both . 
an aggressive approach is required , including total pancreatectomy with dissection of the lymph nodes for invasive ipmns [ 5 ] , whereas a limited resection is suggested for benign ipmns and carcinomas in situ [ 6 ]  . 
 even though the search for predictive factors for malignancy at imaging is still underway [ 79 ] , many authors agree that several features are suggestive of malignancy , namely , the main duct type with mpd dilation > 1015 mm , the branch - duct type with tumour size > 3 cm and mural nodules [ 1016 ]  . 
considering that the branch duct type is associated with a lower risk of carcinoma than mpd type [ 17 , 18 ] , resection is recommended for the mpd type and the combined types when malignancy is suspected , whereas the branch ductal type with benign features ( tumour size < 3 cm , thin wall and absence of mural nodules ) can be followed up with imaging techniques [ 16 , 19 ]  . the slow growth of ipmns suggests the importance of a long follow - up both for nonresected ipmns and for lesions resected due to recurrent disease [ 20 , 21 ]  . 
there is no evidence in the literature indicating the best imaging modality for following up ipmns , although many authors consider magnetic resonance cholangiopancreatography ( mrcp ) to be the most suitable imaging technique for diagnosis ( with secretin administration ) and follow - up ( without secretin administration ) for managing branch ductal type [ 19 , 22 , 23 ]  . 
in our experience , a diagnosis of ipmns is made using multidetector computed tomography ( mdct ) , i primi casi segnalati di neoplasia intraduttale papillare mucinosa ( npi ) del pancreas sono stati descritti nel 1980 da ohhashi et al . 
le npi derivano dallepitelio dei dotti pancreatici , iniziano a produrre mucina e questa determina dilatazioni segmentarie o diffuse del dotto pancreatico principale ( mpd ) , dei dotti secondari o di entrambi e sono classificati come npi del dotto principale , del dotto secondario e misti [ 4 ]  . 
in presenza di npi invasiva necessario un approccio aggressivo fino alla pancreatectomia totale con linfoadenectomia accurata [ 5 ] ; per la npi benigna o con carcinoma in situ stata consigliata una resezione subtotale [ 6 ]  . la ricerca dei fattori predittivi di malignit della npi con le tecniche di imaging tuttora oggetto di studio [ 79 ] ; molti autori suggeriscono che devono essere considerate neoplasie maligne la npi localizzata nel dotto principale che presenta una dilatazione superiore a 1015 mm e la npi localizzata nel dotto secondario di dimensioni superiori a 3 cm nel cui contesto si apprezzano noduli murali [ 1016 ]  . 
la npi del dotto secondario associata ad un minor rischio di carcinoma pancreatico rispetto alla npi del dotto principale [ 17 , 18 ] ; la resezione pancreatica raccomandata per la npi del dotto pancreatico principale e per la npi mista , mentre se la npi localizzata in un dotto secondario ed di dimensioni inferiori a 3 cm , con parete sottile e senza apprezzabili noduli murali pu essere seguita in follow - up con le sole tecniche di imaging [ 16 , 19 ]  . 
 la crescita lenta della npi suggerisce limportanza di un lungo follow - up sia per npi non resecate che per lesioni operate nelle quali possibile una ricorrenza di malattia [ 20 , 21 ]  . 
in letteratura non vi sono evidenze che suggeriscano quale sia la migliore modalit di imaging per il follow - up delle npi dei dotti secondari , anche se molti autori considerano la colangiopancreatografia in risonanza magnetica 444 radiol med ( 2010 ) 115 : 442452 whereas the imaging technique of choice for the follow - up is mrcp with or without secretin [ 24 ]  . 
 an open question about this particular type of pancreatic neoplasm is the reported association with other pancreatic and extrapancreatic synchronous as well as metachronous diseases [ 5 , 10 ]  . 
thus , the aim of this study was to describe the possible presence of extrapancreatic neoplasia in patients with ipmn and to evaluate whether the extrapancreatic tumours are synchronous or metachronous to ipmns . materials and methods all consecutive patients admitted to our unit from january 2005 to december 2007 with a clinical suspicion of ipmn detected at imaging for routine check - up or oncological follow - up were enrolled in the study . 
 mdct was carried out using a siemens sensation 16slice cardiac ct scanner ( siemens ag , erlangen , germany ) that uses somatom sensation images ( siemens medical solutions , siemens ag , berlin , germany )  . 
we routinely use the following examination protocol : before the examination , the patient drinks about 800 ml of water so that the stomach and duodenum can be better visualised , and the first acquisition is carried out ; then a contrast agent ( iobitridol xenetix , guerbet , france ) containing an iodine concentration of 350 mg / ml is intravenously infused ; 150 ml of contrast agent is then administered ( 90 ml at 3 ml / s followed by 60 ml at 2ml / s ) , together with 40 ml of 0.9% saline solution at 2 ml / s . 
three consecutive image acquisitions are carried out : the pancreatic phase 40 s after contrast medium infusion , the venous phase with an 80 - s delay and the late phase with a 180 - s delay . 
the images acquired undergo postprocessing via multiplanar reconstruction ( mpr ) , angio maximum intensity projection ( mip ) , inspace and volume rendering ( vr )  . mr imaging and mrcp were carried out using a commercially available system ( signa 1.5 t , ge medical systems , milwaukee wi , usa )  . 
all patients fasted for at least 5 h before the examination , and approximately 200 ml of superparamagnetic contrast medium ( ferumoxsil lumirem , guerbet s.p.a. , genova , italy ) or pure pineapple juice was given orally 30 min before the procedure to elim ( mrcp ) la tecnica radiologica pi idonea sia per la diagnosi ( in questo caso la mrcp deve essere eseguita con stimolo secretinico ) che per il follow - up ( solitamente la mrcp pu essere eseguita senza stimolo secretinico ) [ 19 , 22 , 23 ]  . 
nella nostra esperienza per la diagnosi di npi si dovrebbe utilizzare la tomografia computerizzata multidetettore ( mdct ) , mentre la tecnica di imaging di scelta per il follow - up la mrcp con o senza secretina [ 24 ]  . 
pertanto , lobiettivo di questo studio stato quello di descrivere leventuale presenza di malattie pancreatiche ed extrapancreatiche in pazienti con npi e di valutare se le neoplasie pancreatiche ed extrapancreatiche associate siano sincrone o metacrone . materiali e metodi in questo studio sono stati arruolati tutti i pazienti giunti alla nostra osservazione da gennaio 2005 a dicembre 2007 con sospetto clinico di npi rilevate in seguito a check - up o per follow - up oncologico . 
in breve , lecografia stata effettuata al mattino dopo un digiuno di almeno 12 ore utilizzando un apparecchio ultrasonografico convex ( technos mpx , esaote spa , genova , italia )  . 
 la mdct stata effettuata utilizzando con apparecchio siemens sensation 16 banchi ( siemens ag , erlangen , germania ) che utilizza un software somatom sensation immages ( siemens medical solutions , siemens ag , berlino , germania )  . 
abbiamo sempre utilizzato il seguente protocollo : prima dellesame , il paziente beve circa 800 ml di acqua in modo che lo stomaco ed il duodeno possano essere meglio visualizzati e viene quindi eseguita lacquisizione pre - contrastografica . 
viene poi somministrato per via endovenosa il mezzo di contrasto ( iobitridol xenetix , guerbet , francia ) contenente iodio alla concentrazione di 350 mg / ml ; 150 ml di mezzo di contrasto somministrato ( 90 ml a 3 ml / s seguiti da 60 ml a 2 ml / s ) cui seguono 40 ml di soluzione fisiologica allo 0 , 9% alla velocit di 2 ml / s . 
sono quindi effettuate tre acquisizioni consecutive di immagini ; la fase pancreatografica viene effettuata 40 secondi dallinizio dellinfusione di mezzo di contrasto , la fase venosa effettuata con un radiol med ( 2010 ) 115 : 442452 inate interference from organs containing fluid on the biliopancreatic tree [ 25 ]  . 
the following parameters were used to study the pancreatic gland : in - phase axial fast spoiled - gradient echo ( fspgr ) with fat suppression , field of view ( fov ) 40 ( range 3644 ) , in - phase echo time ( te ) , repetition time ( tr ) 180 , flip angle 90 , matrix 256160 ; t2 single - shot fast spin echo ( ssfse ) t2 with matrix 256224 , te 80 with automatically calculated tr . 
for morphological pancreatic ductal assessment , secretin ( 1 clinical unit / kg ; secrelux , goldham - bioglan , zusmarhausen , germany ) was administered before the examination , and the appropriate evaluation of the ductal system was assessed by t2 ssfse with fat saturation , tr3 , 000 , te 1 , 300 . 
after secretin administration , paramagnetic contrast medium ( gadoterate meglumine , dotarem , guerbet s.a. , roissy , france ) was also administered to improve the quality of diagnostic assessment . 
images were also assessed for the presence of pancreas divisum and other anatomical variants , ductal dilation , ductal irregularities , strictures , stones and alterations of side - branch morphology . 
on conventional imaging ( i.e. ct or mrcp ) , dilation of the main duct 1 cm strongly suggests main - duct ipmn , whereas the presence of a pancreatic mucinous cyst communicating with the pancreatic duct without main - duct dilation suggests branch - duct ipmn . 
patients with branch - type ipmn < 1 cm need to be followed with imaging techniques every year ; those with branch - type ipmn 13 cm and without high - risk stigmata ( mural nodules , dilated main duct , positive cytology ) need to be carefully followed up with imaging every 36 months and patients with branch - type ipmn with size at imaging > 3 cm should undergo resection because of the high possibility of malignancy [ 6 ]  . statistical analysis fishers exact test , mann - whitney u test and pearson chisquared test were applied . 
le immagini acquisite sono sottoposte ad elaborazione mediante ricostruzioni multiplanari ( mpr ) , langio - intensit massima di proiezione ( mip ) e volume rendering inspace ( vrt )  . 
 la risonanza magnetica ( rm ) e la mrcp sono state eseguite utilizzando lapparecchio signa 1 , 5 t ( ge medical systems , milwaukee , wisconsin , usa )  . 
a tutti i pazienti , a digiuno da almeno 5 ore prima dellesame , sono somministrati per via orale circa 200 ml di mezzo di contrasto superparamagnetico ( ferumoxsil lumirem , guerbet spa , genova , italia ) o succo puro di ananas 30 minuti prima della procedura per eliminare le interferenze da parte di organi contenenti liquidi [ 25 ]  . 
le sequenze utilizzate per lo studio della ghiandola pancreatica sono le seguenti : assiali fast spoiled gradient echo ( fspgr ) in fase con soppressione del grasso , con field of view ( fov ) 40 ( range 3644 ) ; te ( in phase echo time ) , tr ( repeat time ) 180 , flip angle 90 matrix 256160 ; single shot fast spin echo ( ssfse ) t2 : matrice 256224 , te 80 con tr calcolato automaticamente . 
la mrcp dinamica con stimolo secretinico ( secretina 1 unit clinica / kg ; secrelux , goldhambioglan , zusmarhausen , germania ) viene eseguita per una migliore definizione della morfologia duttale pancreatica . infine , a completamento di indagine , viene somministrato il mezzo di contrasto paramagnetico ( gadoterate meglumina , dotarem , guerbet sa , roissy , francia ) al fine di migliorare la qualit della valutazione del parenchima pancreatico . 
lanalisi diagnostica comprende anche la valutazione della presenza di pancreas divisum ed altre varianti anatomiche , dilatazione duttale , irregolarit duttali , stenosi , calcoli e alterazioni morfologiche dei dotti secondari . leffettuazione dellesame richiede circa 45 minuti . 
il tipo ed i risultati ottenuti con tali tecniche di imaging sono stati registrati al momento del primo studio , nonch negli esami di follow - up . i criteri radiologici utilizzati per la diagnosi e la stadiazione delle npi sono stati quelli suggeriti dalle linee guida internazionale per la gestione di tali neoplasie [ 6 ]  . 
in breve , le npi sono state classificate come npi del dotto principale ( npi tipo i ) , npi dei dotti secondari ( npi di tipo ii ) e npi di tipo misto ( npi tipo iii )  . 
la dilatazione del dotto principale 1 centimetro suggerisce fortemente una npi del dotto principale , mentre la presenza di una cisti pancreatica in comunicazione con il dotto pancreatico principale non dilatato suggerisce una npi del dotto secondario . 
i pazienti con npi dei dotti secondari di dimensione inferiore ad un centimetro necessitano di essere seguiti con tecniche di imaging annualmente ; quelli con npi tipo ii con lesione compresa tra 1 e 3 cm e senza segni di rischio di malignit ( noduli murali , dilatazione del dotto principale , citologia positiva per cellule displastiche ) devono essere seguiti con mr / mrcp ogni 36 mesi ; infine , i pazienti con npi di tipo 446 radiol med ( 2010 ) 115 : 442452 ( range 3798 ) years . 
as shown in table 1 , we found that , in evaluating the distribution of pancreatic or extrapancreatic diseases according to the type of ipmn , one patient with type i had an associated pancreatic adenocarcinoma ( 5.0% ) ; 13 ( 65.0% ) with type ii had associated pancreatic or extrapancreatic diseases and the remaining six ( 30% ) with type iii had associated pancreatic or extrapancreatic diseases . 
 analisi statistica le tecniche statistiche utilizzate in questo studio sono state il test esatto di fisher , il test di mann - whitney ed il test del chi - quadrato di pearson . 
in particolare , 4 pazienti erano stati operati per un adenocarcinoma del pancreas ( 2 , 8% ) , 7 avevano una pancreatite cronica ( 4 , 9% ) , 1 aveva un lipoma pancreatico ( 0 , 7% ) , 2 erano stati operati per tumore endocrino del pancreas non funzionante ( 1 , 4% ) , uno era stato operato per cancro al polmone ( 0 , 7% ) , 3 erano stati precedentemente operati per un carcinoma del colon ( 2 , 1% ) , un paziente era stato operato due volte rispettivamente per un carcinoma renale ed un carcinoma polmonare , ed uno per una metastasi peritoneale da tumore a sede non conosciuta ( 0 , 7% )  . 
dei 13 pazienti che avevano altre neoplasie associate alla npi , 12 pazienti avevano tumori sincroni o metacroni ed uno aveva un tumore pancreatico benigno ( lipoma ) ; tutti i pazienti avevano una diagnosi istologica della neoplasia . 
come riportato nella tabella 1 , abbiamo riscontrato malattie pancreatiche ed extrapancreatiche associate in un paziente con npi di tipo i ( 5 , 0% ) , in 13 ( 65 , 0% ) con npi di tipo ii ed in 6 ( 30% ) con npi di tipo iii . 
la distribuzione delle varie malattie associate del pancreas o extrapancreatiche non era significativamente diversa tra le npi di tipo i , ii e iii ( p = 0 , 776 )  . 
inoltre , let dei pazienti senza malattie associate extrapancreatiche o pancreatiche ( 69 , 610 , 8 anni ) era sovrapponibile a quella dei pazienti con malattie extrapancreatiche o pancreatiche ( 69 , 29 , 1 , p = 0 , 732 )  . 
la distribuzione delle neoplasie pancreatiche o extrapancreatiche in base al tipo di npi non era significativamente diversa tra i tipi i , ii e iii ( p = 0 , 740 )  . 
inoltre , let dei pazienti senza neoplasie extrapancreatiche o pancreatiche ( 69 , 410 , 9 anni ) era simile a quelli dei pazienti che avevano tumori extrapancreatici o pancreatici ( 70 , 66 , 7 ; p = 0 , 950 )  . 
infine , il sesso dei pazienti senza cancro extrapancreatico o pancreatico ( maschi : 52 , 40 , 0% , femmine : 78 , 60 , 0% ) non era statisticamente differente da quelli che avevano un 448 radiol med ( 2010 ) 115 : 442452 fig . 
4 type ii intraductal papillary mucinous neoplasia localised in the tail of the pancreas associated with lipoma of the pancreatic head ( multidetector computed tomography on the right side )  . 
in fact , sugiyama et al . found a prevalence of extrapancreatic cancer ( mainly colorectal and gastric cancer ) of 32% in 42 patients operated on for ipmn [ 5 ]  . 
found a prevalence of 30% in 61 patients operated on for ipmn who developed an extrapancreatic cancer , mainly gastric ( 44% ) and colorectal ( 22% ) [ 10 ]  . 
the same prevalence ( 35% ) was also cancro extrapancreatico o pancreatico ( maschi : 4 , 33 , 3% , femmine : 8 , 66 , 7% ; p = 0 , 764 )  . per ultimo , 7 pazienti con npi avevano una pancreatite cronica ed uno un lipoma pancreatico . 
la distribuzione di queste malattie benigne pancreatiche in funzione del tipo di npi non era significativamente differente tra i diversi tipi di npi ( p = 0 , 720 )  . 
let dei pazienti senza malattia benigna del pancreas ( 69 , 710 , 5 anni ) era sovrapponibile a quelli dei pazienti con malattia benigna del pancreas ( 67 , 112 , 1 ; p = 0 , 658 )  . 
il sesso dei pazienti senza malattia benigna ( maschi : 50 , 89 , 3% , femmine : 84 , 97 , 7% ) non era statisticamente diverso da quei pazienti che avevano malattie pancreatiche ( maschi : 6 , 10 , 7% , femmine : 2 , 2 , 3% ; p = 0 , 058 )  . 
hanno riportato una prevalenza simile ( 30% ) in 61 pazienti operati per npi che hanno sviluppato un cancro extrapancreatico principalmente localizzato allo stomaco ( 44% ) ed al colon ( 22% ) [ 10 ]  . 
hanno riscontrato una frequenza di neoplasia extrapancreatica del radiol med ( 2010 ) 115 : 442452 450 radiol med ( 2010 ) 115 : 442452 found by kamisawa et al . 
these authors also found that the most frequent types of tumour in patients with ipmns were those of the breast ( 30% ) , prostate ( 10% ) and colon / rectum ( 10% )  . 
in our study , we found an incidence of extrapancreatic cancer in ipmn patients of 8.5% , a rate similar to that reported by baumgaertner [ 29 ] and much lower than that found by the japanese authors . 
the difference between the western and the japanese studies is difficult to explain , but it may be due to regional differences in the incidence of individual cancers , it is well known that gastric cancer has become a relatively rare cancer in north america and in most of northern and western europe , but not in east asia [ 30 ]  . however , the association of pancreatic and extrapancreatic cancer in ipmn patients suggests the involvement of particular carcinogenic mechanisms or common environmental risk factors in patients with ipmn . 
another point of interest of our study is that the distribution of pancreatic or extrapancreatic neoplasms was not related either to ipmn type or the age of patients with or without extrapancreatic cancer . finally , we found that benign pancreatic diseases may be associated with ipmn : seven patients had chronic pancreatitis and one had a pancreatic lipoma . 
even though lipoma is a rare casual association , it is possible that chronic pancreatitis may be a factor eliciting the development of this slow - growing neoplasm , as happens for pancreatic adenocarcinoma [ 31 ]  . 
in studi sulla popolazione occidentale , riall et al . , in uno studio osservazionale hanno rilevato unincidenza di cancro extrapancreatico nel 10 , 3% di pazienti con npi invasivo [ 28 ] e baumgaertner et al . , in uno studio caso - controllo , confrontando 178 pazienti con npi resecata e 356 controlli comparabili per sesso , hanno trovato unincidenza di cancro extrapancreatico nel 16 , 8% dei pazienti con npi [ 29 ]  . 
lincidenza di cancro extrapancreatico nei pazienti con npi ( 30 su 178 , 16 , 8% ) era significativamente superiore a quello della popolazione di controllo ( 30 / 356 , 8 , 4% )  . 
questi ultimi autori hanno inoltre riportato che i tipi di tumori pi frequenti nei pazienti con npi erano quelli localizzati al seno ( 30% ) , alla prostata ( 10% ) , ed al colon - retto ( 10% ) ; tuttavia non hanno riscontrato alcuna correlazione tra la presenza di cancro extrapancreatico ed il tipo di npi . 
nel nostro studio , abbiamo osservato che lincidenza di cancro extrapancreatico in pazienti con npi era dell8 , 5% ; questa frequenza simile a quella riportata da baumgaertner [ 29 ] ed molto inferiore a quello riportata dagli autori giapponesi . 
la differenza tra i dati riportati nei paesi occidentali e quelli riportati dai ricercatori giapponesi difficile da spiegare , ma pu essere dovuta a differenze regionali : infatti noto che il cancro gastrico divenuto un tumore relativamente raro nel nord america e nella maggior parte dei paesi europei , ma non altrettanto raro nei paesi asiatici [ 30 ]  . 
sembra quindi importante sottoporre a screening i pazienti con tumore del colon - retto , al fine di migliorare la diagnosi di npi , soprattutto in quei pazienti esposti a fattori di rischio per un periodo prolungato . 
un altro punto interessante del nostro studio che la distribuzione delle neoplasie pancreatiche o extrapancreatiche non sono correlate n al tipo di npi n allet dei pazienti con o senza cancro extrapancreatico . 
 infine , abbiamo riscontrato che le malattie pancreatiche benigne possono essere associate a npi : 7 pazienti con npi avevano una pancreatite cronica e ad un paziente era stato diagnosticato un lipoma pancreatico . 
anche se il lipoma pu essere unassociazione rara e casuale , possibile che la pancreatite cronica possa essere un fattore favorente lo sviluppo della npi cos come avviene per ladenocarcinoma pancreatico [ 31 ]  . 
in the first week after olt , cdus examination was performed daily in patients with anastomoses at a high risk of thrombosis , and on the basis of clinical and laboratory findings in other patients . 
sono stati studiati retrospettivamente 134 pazienti , 102 maschi e 32 femmine di et compresa tra 21 e 68 anni , trapiantati tra maggio 2007 ed aprile 2008 . nella prima settimana post - olt i controlli eco color doppler sono stati giornalieri per le anastomosi a rischio di trombosi , ed in base al quadro clinico - laboratoristico negli altri casi . 
sensibilit , specificit , valore predittivo positivo , valore predittivo negativo ed accuratezza diagnostica dellindagine sono stati rispettivamente : 79 , 2% , 97 , 3% , 86 , 3% , 95 , 5% , 94% ( b ) , 100% , 100% , 100% , 100% , 100% ( v ) e 100% , 96 , 9% , 42 , 8% , 100% , 97% ( lf )  . 
diagnosticare precocemente una complicanza pu condizionare lintegrit del graft e la sopravvivenza del paziente . parole chiave ecografia color doppler trapianto di fegato follow - up complicanze radiol med ( 2010 ) 115 : 13041313 introduction introduzione 1305 the first human orthotopic liver transplantation ( olt ) was performed by starzls group in 1963 [ 1 ]  . 
since then , the survival rates of transplant patients have constantly increased , thanks to improved surgical technique , availability of more suitable immunosuppressive drugs and more effective clinical and imaging postoperative surveillance [ 2 ]  . 
the purpose of post - olt monitoring is to provide an early diagnosis of vascular complications ( thrombosis , stenosis and dilatation of the hepatic artery , portal vein and vena cava ) [ 3 ] , biliary complications ( fistulas , intrahepatic and anastomotic strictures , abscess formation and lithiasis ) , sacculated collections ( haemorrhagic , biliary , ascitic , purulent ) , and de novo malignancies induced by immunosuppression . 
adequate postoperative surveillance based on clinical examination , blood chemistry and diagnostic imaging aims at preserving graft integrity and patient well - being . modern follow - up protocols involve colour doppler ultrasonography ( cdus ) as a first - line modality . 
this is a noninvasive , inexpensive modality that is easily performed at the patients bedside in the intensive care unit ( icu ) and provides qualitative and quantitative morphological and functional information . 
the aim of this study was to analyse the technical aspects and diagnostic role of cdus during the first year of follow - up after olt in our experience compared with the literature and critically assess the limitations of the modality compared with reference standards in detecting biliary , vascular and neoplastic complications . il trapianto ortotopico di fegato ( olt ) venne eseguito per la prima volta nelluomo nel 1963 dallequipe di starzl [ 1 ]  . a partire da allora si assistito ad un continuo incremento delle percentuali di sopravvivenza dei pazienti trapiantati , correlabile oltre che allaffinarsi della tecnica chirurgica ed alla disponibilit di pi idonei farmaci immunosoppressori anche ad una sempre pi efficace sorveglianza clinicostrumentale post operatoria [ 2 ]  . 
scopo del monitoraggio post - olt diagnosticare tempestivamente : complicanze vascolari [ 3 ] ( trombosi , stenosi ed ectasie dellarteria epatica , della vena porta , e della vena cava ) , complicanze biliari ( fistole , stenosi intraepatiche ed anastomotiche , ascessi e calcolosi ) , raccolte saccate ( emorragiche , biliari , ascitiche , purulente ) e neoplasie di nuova comparsa favorite dallimmunosoppressione . 
unadeguata sorveglianza multispecialistica , basata sulla visita clinica , su riscontri ematochimici e sullimaging mira a preservare lintegrit del graft ed il benessere del paziente . in corso di follow - up i moderni protocolli prevedono come metodica di imaging di primo livello leco color doppler ; la metodica non invasiva , ha un basso costo , di rapida esecuzione anche al letto del paziente in unit di terapia intensiva ed in grado di fornire informazioni sia morfologiche sia funzionali qualitative e quantitative . 
scopo di questo lavoro discutere , confrontandoli con i dati della letteratura , gli aspetti tecnici e lattuale ruolo diagnostico dellesame ecotomografico nel i anno di follow - up del trapianto epatico ed analizzare criticamente i limiti della metodica nei confronti delle indagini considerate gold standard nellidentificazione di complicanze biliari , vascolari e neoplastiche . 
 materials and methods materiali e metodi our retrospective study included 134 adult patients 102 men ( 76.1% ) and 32 women ( 23.9% ) , age range 2168 ( mean 55.3 ) years who underwent olt between may 2006 and april 2007 . 
the decision to limit the follow - up period to 1 year was based on the fact that all olt patients were studied at our institution for 1 year only , after which they were followed up at other referral centres . indications for olt included hepatitis c virus ( hcv ) related cirrhosis ( n = 73 ) , hepatocellular carcinoma ( n = 48 ) , hbv - related cirrhosis ( n = 28 ) , exotoxic cirrhosis ( n = 12 ) , cirrhosis of unknown origin ( n = 10 ) , acute liver failure ( n = 6 ) , primary biliary cirrhosis ( n = 3 ) , primary sclerosing cholangitis ( n = 3 ) and budd - chiari syndrome ( n = 2 )  . 
la decisione di limitare il tempo di follow - up ad un solo anno scaturita dal fatto che solo in questo lasso di tempo tutti i trapiantati sono stati studiati presso il nostro istituto . 
successivamente i pazienti sono stati seguiti presso altri centri di riferimento . le indicazioni per il trapianto erano rappresentate da cirrosi epatica correlata al virus dellepatite c ( hcv ) ( n = 73 ) , carcinoma epato - cellulare ( n = 48 ) , cirrosi epatica correlata al virus dellepatite b ( hbv ) ( n = 28 ) , cirrosi esotossica ( n = 12 ) , cirrosi ad eziologia sconosciuta ( n = 10 ) , epatite fulminante ( n = 6 ) , cirrosi biliare primitiva ( n = 3 ) , colangite sclerosante primitiva ( n = 3 ) , sindrome di budd - chiari ( n = 2 )  . ciascun paziente stato sottoposto , nel post - trapianto , a terapia immunosoppressiva di induzione con ciclosporina o fk + prednisoneazatioprina o micofenolato mofetile , seguita 1306 radiol med ( 2010 ) 115 : 13041313 mmf + sirolimus , according to individualised treatment regimens . 
examinations were conducted by two experienced radiologists who used a technos mpx scanner equipped with a 5 - 2 - mhz convex - array transducer ( esaote , genoa , italy ) located in the department of radiodiagnostics , and a portable hdi 3000 ultrasound system with a 4 - 2 - mhz convex - array transducer ( atl , bothell , wa , usa ) that can be used at the patients bedside in the icu . serial us examinations were performed every other day during the first week of icu stay , except in case of anastomoses at risk for thrombosis ( due to associated coagulopathy or complex reconstructions on small - calibre vessels ) , which were deemed to require daily monitoring . after discharge , follow - up examinations were performed at 1 , 3 , 6 and 12 months from the intervention , unless otherwise clinically indicated ( elevated liver enzymes and / or bilirubinaemia , leukocytosis , fever , abdominal pain or dyspnoea )  . 
pulsed doppler us was performed using a 4060 angle of insonation , a sample volume > 50% of the vessel diameter , prf ranging from 1.5 to 2 mhz and a 100 - hz filter . 
turbulent flows with focal increase in velocity > 2 m / s at the site of anastomosis associated with a tardusparvus pattern of intrahepatic arterial flow , characterised by longer sat and lower psv , were considered as indicative of stricture . 
lesame stato condotto da operatori esperti utilizzando unapparecchiatura technos mpx con sonda convex da 25 mhz ( esaote , genova , italia ) ubicata presso il reparto di radiodiagnostica ed un ecografo hdi 3000 con sonda convex da 24 mhz ( atl , bothell , wa , usa ) trasportabile al letto del paziente in unit di terapia intensiva . i controlli tramite ecografia ( us ) seriati sono stati effettuati a giorni alterni per la prima settimana di ricovero in unit di terapia intensiva , tranne nei casi di anastomosi a rischio di trombosi ( per coagulopatie associate o ricostruzioni complesse su vasi di piccolo calibro ) , per le quali si ritenuto indicato un monitoraggio giornaliero . 
dopo la dimissione , salvo diversa indicazione clinica ( rialzo degli enzimi epatici e / o della bilirubinemia , leucocitosi , febbre , algie addominali o dispnea ) , il follow - up ha previsto controlli a 1 , 3 , 6 e 12 mesi dallintervento . 
le focalit parenchimali di nuova comparsa , non tipizzabili con certezza allindagine us , sono state tutte sottoposte ad approfondimento diagnostico tramite tomografia computerizzata ( tc ) ed eventualmente a biopsia percutanea . 
sono state ritenute sospette per stenosi biliare unectasia dei dotti biliari intraepatici > 3 mm ed un diametro della via biliare principale superiore a 7 mi pazienti sono stati comunque inviati alla colangiorisonanza magnetica ( rm )  . 
tredici pazienti sono giunti alla nostra osservazione per un incremento degli indici di colestasi ed 1 paziente per colangiti recidivanti . lo studio della perfusione epatica preliminare stato condotto con il color doppler , utilizzando una pulse repetition function ( prf ) variabile tra 0 , 5 e 1 , 5 mhz ed il power doppler per la visualizzazione di flussi molto lenti con segnale di debole intensit . 
per il successivo doppler pulsato sono stati utilizzati un angolo dinsonazione compreso tra 40 e 60 , un volume campione superiore al 50% del diametro del vaso , una prf di 1 , 52 mhz ed un filtro di 100 hz . 
sono stati valutati il picco di velocit sistolica ( psv ) e lanalisi spettrografica dei pattern di flusso ; non abbiamo considerato invece altri parametri suggeriti dalla letteratura come lindice di resistenza ( ir ) e tempo di accelerazione sistolico ( sat ) , con cut - off rispettivamente di 0 , 5 e 0 , 08 [ 47 ]  . 
 stato considerato indicativo di stenosi un flusso turbolento con aumento focale della velocit > 2 m / s sul sito di anastomosi , associato ad un tracciato arterioso intraepatico con morfologia di tipo tardus parvus , caratterizzato da un un incremento del tempo di accelerazione sistolica e da una riduzione del picco di velocit sistolica . 
the presence of intraluminal echoic material and total absence of cdus signal in the portal vein were considered to be pathognomonic for thrombosis . ectasia of the iliaccaval venous system , characterised by a flow pattern with poor phasicity , and the presence of marked perianastomotic acceleration ( threeto fourfold faster than in the common iliac veins ) were considered to reflect stricture of the retrohepatic vena cava . 
two patients with markedly increased transaminase levels were referred for emergency cdus owing to suspected hepatic artery thrombosis , whereas three patients with worsening ascites and nonspecific liver enzyme alterations were referred to rule out portal thrombosis and / or impaired ivc flow . 
subsequently , we investigated the presence of abdominal fluid collections , a frequent finding in the immediate postoperative period , but omitted to include these results in the statistical analysis . the characterisation of fluid collections was based on the us appearance of the fluid and on the morphology of the collection . 
in the case of suspected biloma , diagnostic workup involved trans - kehr cholangiography , mrc or percutaneous puncture . deponenti per la diagnosi di trombosi dellarteria epatica sono stati : la totale assenza di segnale color doppler dellarteria epatica propria associata ad assente o scarsa visualizzazione di rami intraparenchimali caratterizzati da assai modesta ampiezza di tracciato . 
stato considerato indicativo di stenosi anastomotica un flusso turbolento con velocit superiore a 50 cm / s e 3 volte maggiore rispetto a quella rilevata 2 cm al di sopra delloliva portale . 
lectasia del sistema iliaco - cavale , caratterizzato da flusso scarsamente fasico , e la presenza di vistosa accelerazione perianastomotica ( velocit di 34 volte maggiore rispetto alle vene iliache comuni ) , sono state considerate sinonimo di stenosi della cava retroepatica . delle vene sovraepatiche sono state considerate sia la perviet che il tracciato ; sono stati considerati patologici i flussi lenti privi di fasicit o con netto incremento della componente reflua . 
in 2 pazienti con notevole incremento delle transaminasi lindicazione alleco color doppler in regime di urgenza stato il sospetto di trombosi dellarteria epatica , mentre in 3 pazienti con ascite ingravescente e alterazione aspecifica degli enzimi epatici lesame stato richiesto per escludere la trombosi portale e / o deficit di scarico della vena cava inferiore . 
nei casi di sospetto biloma il successivo iter diagnostico ha previsto a seconda dei casi la colangiografia trans - kehr , la colangio - rm o la puntura percutanea . statistical analysis analisi statistica we measured sensitivity ( sn ) , specificity ( sp ) , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy ( da ) of follow - up cdus with a view to assessing its diagnostic reliability . 
second - line diagnostic modalities were considered the standards of reference : trans - kehr cholangiography or mrc for suspected biliary complications , four - phase ct for suspected vascular complications and four - phase ct with possible us - guided biopsy for suspected neoplastic complications . per valutare lattendibilit diagnostica dellesame ecotomografico di follow - up sono state calcolate la sensibilit ( sn ) , la specificit ( sp ) , il valore predittivo positivo ( vpp ) , il valore predittivo negativo ( vpn ) e laccuratezza diagnostica ( ad ) della metodica . 
sono stati assunti come gold standard di riferimento gli esami diagnostici di secondo livello : colangiografia trans - kher o colangio - rm in caso di sospetto di complicanze biliari , tc quadrifasica in caso sospetto di complicanze vascolari , tc quadrifasica ed eventuale biopsia sotto guida us in caso di sospetto di complicanze neoplastiche . 1308 results at 1 - year follow - up after olt , us findings raised the diagnostic suspicion of complications in 38 cases : biliary complications ( 22 patients ) , vascular complications ( nine patients ) and focal hepatic malignancies ( 7 patients )  . regarding suspected biliary complications , in all cases , us demonstrated ectasia of the intrahepatic biliary tree , which was confirmed in 19 / 22 patients by second - line examinations ( mrc or cholangiography )  . 
ectasia was caused by stenosis of the surgical anastomosis in 19 cases , nine of which were associated with sludge or stones , and in one case by extrinsic compression by an expansile intrahepatic lymphomatous lesion . 
four - phase ct with three - dimensional reconstructions , table 1 statistical analysis of colour doppler ultrasound ( cdus ) results radiol med ( 2010 ) 115 : 13041313 risultati in un anno di follow - up post - olt lesame ecografico ha posto il sospetto diagnostico di complicanza in 38 casi : in 22 pazienti si supposta una complicanza biliare , in 9 pazienti una complicanza vascolare ed in 7 pazienti stata individuata una lesione focale epatica di possibile natura evolutiva . 
per quanto concerne i sospetti di complicanza biliare , in tutti i casi lus ha dimostrato unectasia delle vie biliari intraepatiche , confermata in 19 / 22 pazienti da indagini di secondo livello ( colangio - rm o esame colangiografico ) , determinata da una stenosi dellanastomosi chirurgica in 19 casi , di cui 9 associati a sludge o litiasi , e in 1 caso da compressione estrinseca per lesione espansiva intraepatica linfomatosa . 
i falsi negativi ecografici ( fn ) sono stati 5 : in questi pazienti , tutti con segni di colestasi , gli esami radiologici di secondo livello hanno rivelato 5 stenosi anastomotiche , di cui 2 associate a litiasi . 
 pertanto riassumendo lecotomografia nello studio delle vie biliari ha rivelato : una sn del 79 , 2% , una sp del 97 , 3% un vpp del 86 , 3% , un vpn del 95 , 5% ed una ad del 94% ( tabella 1 )  . 
c four - phase ct scan with multiplanar maximum intensity projection ( mip ) reconstructions performed to complete the diagnostic algorithm confirms the us suspicion of tight perianastomotic stenosis of the hepatic artery fig . 
c la tc quadrifasica con ricostruzioni in proiezione di massima intensit ( mip ) multiplanari , eseguita a completamento diagnostico , conferma il sospetto us di stenosi serrata perinanastomotica dellarteria epatica . 
nello studio delle complicanze neoplastiche lecotomografia ha rilevato : una sn del 100% , una sp del 96 , 9% , un vpp di 42 , 8% , un vpn del 100% , una ad del 97% ( tabella 1 )  . 
b ct scan performed after us confirms the presence of hepatic metastasis of unknown origc to obtain cytological characterisation of the hepatic metastasis , needle biopsy of a lesion in segment iv is performed with a , 18 - gauge , tru - cut needle percutaneous fig . 
c al fine di ottenre la tipizzazione citologica della neoplasia si procede quindi alla biopsia percutanea us - guidata con ago tru - cut di 18 g di una lesione a carico del iv segmento . 
regarding collections , us readily depicted 16 abdominal haematomas ; in 4 / 8 patients , the clinical and / or sonographic suspicion of biliary collection was subsequently confirmed . il numero , lincidenza delle complicanze riscontrate ed il tempo intercorso tra la loro comparsa e lolt sono rappresentate nella tabella 2 . 
per quanto concerne le raccolte , lus ha agevolmente dimostrato 16 ematomi addominali ; in 4 / 8 pazienti il sospetto clinico e / o ecografico di raccolta biliare stato poi confermato . discussion discussione our study showed a low overall incidence of complications , in line with the findings reported in the literature . the most frequent complications were biliary strictures , which generally arose more than 3 months after transplantation and were frequently associated with lithiasis . 
in the remaining ten cases ( 41.7% ) , the origin of the intrahepatic biliary damage could not be traced back to either arterial strictures / occlusions or to prolonged cold ischaemia time ( > 12 h ) , as reported in the literature [ 8 , 9 ]  . 
other possible contributing factors such as abo blood group il nostro studio ha evidenziato una bassa incidenza globale di complicanze , in linea con i migliori riscontri riportati in letteratura ; le pi frequenti complicanze rilevate sono state le stenosi biliari , insorte nella maggior parte dei casi dopo un intervallo di tempo dal trapianto superiore a 3 mesi ed associate frequentemente a litiasi . 
the presence of concomitant kehr - tube dislodgement in three patients emphasises the importance of the surgical tube to protect the anastomosis . lithiasis should be regarded as an element in a vicious cycle that comprises strictures , cholestasis and cholangitis . the biliary ectasias depicted by us but not confirmed by second - line imaging in patients with clear signs of cholestasis could reflect a transient hindrance to the flow of high - density bile rather than actual fp results . 
overall , in our experience cdus proved to be highly effective for diagnosing biliary complications , showing very good results even better than those reported in other published works [ 13 ]  . 
the use of codified parameters for the study of hepatic perfusion ( peak velocity , spectral analysis of flow patterns , flow - tracing morphology and blood flow ) allowed us to achieve excellent sn , sp and da values , as previously described by several authors [ 47 ]  . 
particularly important in clinical terms is the early diagnosis of both hepatic artery thrombosis , which represents the most severe and common vascular complication , affects up to 12% of adult patients and is associated with a 73% mortality rate unless retransplantation is performed ; and of anastomotic stricture , which may lead to severe ischaemic damage to the intrahepatic biliary tree . esaminati altri possibili fattori suggeriti da differenti autori come limperfetta compatibilit del gruppo sanguigno ab0 per i trapianti eseguiti in regime durgenza [ 8 , 9 ] , il tipo di soluzione di preservazione utilizzata [ 10 ] , il rigetto cronico , le infezioni da citomegalovirus , un danno citotossico mediato dai sali biliari e la terapia immunosoppressiva con ciclosporina [ 1113 ]  . 
la presenza in 3 pazienti di concomitante sposizionamento del kehr ribadisce limportanza della presenza del tubo chirurgico a protezione dellanastomosi . le calcolosi devono essere considerate uno degli elementi di un circolo vizioso che comprende oltre la stenosi anche la colestasi e la colangite . 
le ectasie biliari segnalate dallus e non confermate dallimaging di ii livello , in pazienti peraltro con evidenti segni di colestasi , potrebbero essere espressione pi di un transitorio impaccio al deflusso di bile ad elevata densit che di veri e propri fp . 
lutilizzo di parametri codificati per lo studio della perfusione epatica ( velocit di picco , analisi spettrografica dei pattern di flusso , morfologia del tracciato e portata ) ha garantito di ottenere ottimali sensibilit , specificit ed accuratezza diagnostica , cos come gi segnalato da diversi autori [ 47 ]  . 
particolare rilevanza clinica riveste la diagnosi tempestiva sia di trombosi dellarteria epatica , che la pi grave e comune complicanza vascolare la cui incidenza giunge nelladulto sino al 12% con mortalit del 73% senza ritrapianto , sia di stenosi serrata dellanastomosi , che pu 1312 radiol med ( 2010 ) 115 : 13041313 cdus allowed ready depiction of blood collections and their characterisation on the basis of their morphology , which changes over time : homogeneously anechoic depositions , inhomogeneous with gravity - dependent hyperechoic depositions , solid and organised . 
in the event of suspected biloma and even more of probably superimposed infectious ascites , us findings are rarely conclusive , and further diagnostic investigations by means of cholangiography ( either trans - kehr or mrc ) and / or diagnostic puncture are required . in our experience , the incidence of post - olt malignancies was 3.7% , lower than that reported in other series [ 14 ]  . in addition to the hepatic focal lesions , we also detected a malignant colonic polyp in a patient with sclerosing cholangitis , and a lymphoma of waldeyers ring . 
the use of azathioprine was related to skin cancer development [ 15 , 16 ] , whereas cyclosporin a is thought to promote the onset of lymphomas and leukaemias [ 17 , 18 ]  . 
posttransplant lymphoproliferative disorders ( ptld ) have the highest incidence , accounting for up to 57% of new tumours in some patient populations [ 19 ] ; they are closely followed by skin malignancies ( up to 15% [ 19 ] ) , gastrointestinal neoplasms , lung and cervical cancers [ 20 ]  . 
we believe the statistical results of our oncological follow - up to have limited significance in that they are invalidated by the short follow - up period considered and the small sample size . 
in fact , to obtain more relevant data , we need to perform a longer clinical and radiological surveillance , bearing in mind that the cumulative risk for de novo malignancy , except for ptld , increases with the amount of time since transplantation [ 14 , 2124 ]  . conclusions cdus is a first - line modality in the follow - up of olt patients , as it is inexpensive , widespread , noninvasive and a frequently repeatable technique that can be performed at the patients bedside . 
 lecotomografia ha consentito di dimostrare agevolmente e tipizzare le raccolte ematiche in base al dettaglio morfologico , che muta nel tempo : anecogeno omogeneo , disomogeneo con sedimento declive ipercogeno , solido organizzato . 
nel sospetto di biloma ed ancor pi nei casi di probabile sovrapposizione infettiva dellascite il pattern ecografico solo di rado dirimente e pertanto necessita di approfondimento diagnostico mediante colangiografia ( trans - kehr o rm ) e / o puntura diagnostica . 
 nella nostra esperienza lincidenza di neoplasie postolt stata del 3 , 7% , inferiore ad altre casistiche [ 14 ]  . oltre alle focalit epatiche vi sono stati un polipo degenerato del colon , in paziente affetto da colangite sclerosante , ed un linfoma dellanello del waldayer ; entrambi non sono stati considerati falsi negativi e pertanto esclusi dal calcolo statistico , in quanto non diagnosticabili con lus . 
luso di azatioprina stato correlato con lo sviluppo di tumori della cute [ 15 , 16 ] , mentre la ciclosporina a favorirebbe linsorgenza di linfomi e leucemie [ 17 , 18 ]  . 
i disordini linfoproliferativi post - trapianto ( ptld ) sono le neoplasie a pi alta incidenza , rappresentando fino al 57% dei tumori a nuova insorgenza in alcune casistiche [ 19 ] ; seguono in senso decrescente le discariocinesi cutanee ( fino al 15% [ 19 ] ) , le neoplasie gastrointestinali , i tumori polmonari e del distretto cervicale [ 20 ]  . 
riteniamo che i risultati statistici del nostro follow - up oncologico abbiano un modesto significato scientifico , in quanto inficiati dal breve lasso di tempo considerato e da un piccolo campione . 
per ottenere dati maggiormente rilevanti infatti indispensabile una pi protratta sorveglianza clinico - radiologica , considerando che il rischio cumulativo di insorgenza di tumori de novo , fatta eccezione per i ptld , aumenta con il trascorrere del tempo dal trapianto [ 14 , 2124 ]  . 
 conclusioni lecotomografia lindagine strumentale di primo livello nel follow - up del trapianto epatico , in quanto poco costosa , ampiamente diffusa , non invasiva , frequentemente ripetibile ed attuabile anche al letto del paziente . 
la metodica in mani esperte pu garantire una pi che soddisfacente accuratezza diagnostica , particolarmente elevata nello studio della perfusione epatica , per il quale possibile avvalersi oltre che dellanalisi morfologica anche di dati color doppler quantitativi e pertanto meno soggetti a valutazione arbitraria . laver considerato un campione di pazienti studiati da operatori esperti con tecnica standardizzata secondo i dettami della recente letteratura , riteniamo consenta di esprimere una valutazione obiettiva del ruolo fondamentale delleco color doppler post - olt , la cui esecuzione non pu comunque prescindere dalla conoscenza della tecnica chirurgica , radiol med ( 2010 ) 115 : 13041313 1313 surgical technique and clinical and laboratory findings . effective monitoring of the olt patient relies on the concrete collaboration of multiple specialists , and the early and accurate diagnosis of complications may influence graft integrity and patient survival . dallintegrazione con la visita clinica e con gli esami ematochimici . 
un efficace monitoraggio del paziente trapiantato deriva da una fattiva collaborazione multispecialistica ; la diagnosi puntuale e precoce di complicanza pu condizionare lintegrit del graft e la sopravvivenza del paziente . 
patients with a cta diagnosis of basilar artery thrombosis were considered for endovascular treatment . cta accuracy was evaluated by considering the 12 patients who underwent endovascular angiography ( the gold standard )  . 
questo studio retrospettivo considera 59 pazienti non traumatizzati con rapida compromissione dello stato di coscienza sottoposti a tc dellencefalo senza mezzo di contrasto ed , esclusa unemorragia parenchimale , ad angio - tc del circolo intracranico ( tomografo a 16 detettori )  . 
esclusi i pazienti con diagnosi di emorragia parenchimale e subaracnoidea la casistica costituita da 26 pazienti sottoposti ad angio - tc , sono stati diagnosticati 15 casi di trombosi della basilare , dei quali 12 trattati presso il nostro ospedale . 
lo studio angio - tc per disponibilit sul territorio e rapidit di esecuzione rappresenta lesame pi indicato per confermare , nel pi breve tempo possibile , un sospetto clinico di trombosi di basilare . 
pur in assenza di studi prospettici randomizzati e controllati per indicare 1220 radiol med ( 2010 ) 115 : 12191233 basilar artery thrombosis , our study lends weight to the role of interventional neuroradiology in the treatment of this condition . lapproccio terapeutico ottimale , la nostra esperienza avvalora il ruolo delle tecniche di neuroradiologia interventistica . keywords basilar artery thrombosis ct angiography ( cta ) intra - arterial lysis mechanical clot removal parole chiave trombosi dellarteria basilare angio - tc trombolisi intra - arteriosa rimozione meccanica del trombo introduction introduzione strokes involving the posterior circulation represent about 20% of all cerebral ischaemic events [ 1 ]  . 
the clinical presentation is variable : a rapid onset of motor and bulbar symptoms with either reduced consciousness to the point of coma or a gradual progression of the various signs of vertebrobasilar insufficiency ( blurred vision , diplopia , dysarthria , vertigo and bilateral muscle weakness )  . 
the second , more common in elderly patients , is a consequence of an atherosclerotic occlusion of the middle and / or proximal sections of the artery [ 2 , 3 ]  . basilar artery occlusion forms the basis for the most devastating type of ischaemia involving the posterior circulation , with mortality and disability rates of 80%90% in the absence of treatment [ 4 , 5 ]  . in the event of a clinical suspicion of ischaemia of the posterior circulation , unenhanced computed tomography ( ct ) can rule out a haemorrhagic event and corroborate the suspicion by showing hyperdensity of the basilar artery [ 68 ]  . 
with its rapid execution times and widespread availability , cta of the intracranial circulation is well placed as a diagnostic tool that can rapidly confirm or rule out occlusion of the vessel lumen without having to resort to conventional angiography of the vertebral arteries [ 9 , 10 ]  . once the diagnosis has been obtained , the next goal is to recanalise the artery . 
however , the low incidence of the disease , the availability of a range of thrombolytic agents for systemic or intra - arterial use and the continuous development of new angiographic devices for thrombus removal all account for the lack of prospective randomised studies comparing the various treatment strategies and identifying those that are most effective [ 1117 ]  . 
lesordio clinico variabile : rapido instaurarsi di sintomi motori e bulbari con riduzione dello stato di coscienza fino al coma , oppure progressione graduale dei vari segni di insufficienza vertebro - basilare ( visione offuscata , diplopia , disartria , vertigini e deficit di forza bilaterali )  . 
la seconda , pi frequente nei pazienti anziani , la conseguenza dellocclusione su base aterosclerotica dei segmenti medio e / o prossimale del vaso [ 2 , 3 ]  . 
locclusione dellarteria basilare il substrato per la forma pi devastante di ischemia del circolo posteriore , gravata da tassi di mortalit e disabilit in assenza di trattamento dell80%90% [ 4 , 5 ]  . nel sospetto clinico di ischemia del circolo posteriore la tomografia computerizzata ( tc ) dellencefalo senza somministrazione di mezzo di contrasto esclude un evento emorragico e pu avvalorare il sospetto clinico dimostrando liperdensit dellarteria basilare [ 68 ]  . 
lo sviluppo degli apparecchi di tomografia computerizzata multistrato ha aperto nuove frontiere nello studio dei vari distretti vascolari . langio - tc del circolo intracranico , di rapida esecuzione e con buona disponibilit nel territorio , si propone come lindagine diagnostica in grado di confermare , in breve tempo , locclusione del lume vasale senza ricorrere allo studio agiografico delle arterie vertebrali [ 9 , 10 ]  . ottenuta la diagnosi , lobiettivo ricanalizzare larteria , tuttavia la bassa incidenza di questa patologia , la disponibilit di diversi agenti trombolitici per uso sistemico od intrarterioso ed il continuo sviluppo di nuovi dispositivi angiografici per la rimozione del trombo giustificano la scarsit di studi prospettici randomizzati che confrontino le varie modalit di trattamento per indicare la pi efficace [ 1117 ] : se la letteratura concorda sulla necessit di ottenere nel pi breve tempo possibile la ricanalizzazione della basilare , vi sono invece opinioni contrastanti su quale sia lapproccio terapeutico ottimale . the aim of this paper is to report our experience in diagnosing basilar artery thrombosis with cta and its treatment with endovascular procedures . scopo di questo lavoro riportare la nostra esperienza nella diagnosi angio - tc e nel trattamento endovascolare del paziente con trombosi dellarteria basilare . radiol med ( 2010 ) 115 : 12191233 materials and methods between march 2005 and january 2009 , 59 nontrauma patients exhibiting rapid deterioration of consciousness and / or the onset or sudden worsening of signs of vertebrobasilar insufficiency underwent unenhanced brain ct , when no parenchymal haemorrage was detected , to intracranial cta . 
patients with evidence on cta of an occlusion of the basilar artery were considered for endovascular treatment with the following exclusion criteria : patients > 80 years of age , those with clinical onset more than 8 h previously and those with unstable vital signs or with a high risk of bleeding . ct examinations were performed using a 16 - detector scanner ( somaton sensation 16 , siemens medical systems , erlangen , germany )  . 
for the cta study , the following acquisition and reconstruction parameters were used : axial scan extending from the body of the first cervical vertebra to the vertex , collimation 0.75 mm , rotation time 0.5 s , field of view [ fov ] 230 mm , feed / rotation 6.5 , 120 kv , 210 mas , with real - time reconstruction of 33 mm - fov 120 and postprocessing reconstruction of 10.5 mm - fov 80 . 
to achieve arterial opacification , an 80 - ml intravenous bolus delivery of iodinated nonionic contrast material ( iomeron 350 mgi / ml , bracco , milan , italy ) was administered antecubitally at a flow rate of 4 ml / s , followed by 50 ml of saline at the same rate . 
images were transferred to the postprocessing workstation ( leonardo , siemens medical systems , erlangen , germany ) and analysed interactively by a radiologist who used a range of twoand three - dimensional postprocessing techniques : multiplanar reconstruction ( mpr ) , maximum intensity projection ( mip ) and volume rendering ( vrt )  . 
the development of an allergic reaction to the contrast medium , deterioration of renal function and extravasation of contrast medium around the injection site were considered complications of the examination . as the study was retrospective , the accuracy of cta in the diagnosis of basilar artery occlusion was evaluated by comparing data for 12 patients who also underwent conventional angiography , which was considered the gold standard . 
angiographic procedures were performed on a 1221 materiali e metodi da marzo 2005 a gennaio 2009 , 59 pazienti non traumatizzati con rapido deterioramento dello stato di coscienza e / o con esordio / aggravamento improvviso dei segni di insufficienza vertebro - basilare sono stati sottoposti a tc dellencefalo senza mezzo di contrasto ed , esclusa unemorragia parenchimale , ad angio - tc del circolo intracranico . 
i pazienti con evidenza angio - tc di occlusione dellarteria basilare sono stati considerati per il trattamento endovascolare con i seguenti criteri di esclusione : paziente ultraottantenne , esordio clinico superiore ad 8 ore , parametri vitali instabili o rischio emorragico elevato . gli esami tc sono stati eseguiti con un tomografo a 16 detettori ( somaton sensation 16 , siemens medical systems , erlangen , germania )  . 
per lo studio angio - tc sono stati utilizzati i seguenti parametri di acquisizione e ricostruzione : scansione sul piano assiale estesa dal soma della prima vertebra cervicale al vertice , collimazione 0 , 75 mm , tempo di rotazione 0 , 5 s , campo di vista ( fov ) 230 mm , feed / rot 6 , 5 , 120 kv , 210 mas , con ricostruzione in tempo reale 3 mm / 3 mm - fov 120 e ricostruzione per il post - processing 1 mm / 0 , 5 mm - fov 80 . 
per lopacizzazione arteriosa sono stati somministrati in bolo , per via endovenosa antecubitale , 80 ml di mezzo di contrasto iodato non ionico ( iomeron 350 mgi / ml , bracco , milano , italia ) al flusso di 4 ml / s seguiti da 50 ml di soluzione salina allo stesso flusso . 
la sincronizzazione della scansione con il passaggio arterioso del mezzo di contrasto stata effettuata in tempo reale mediante la tecnica del bolus tracking ; il volume campione stato posizionato in arteria carotide interna con un valore soglia di + 30 unit hounsfield [ 9 ]  . lanalisi delle immagini , dopo trasferimento alla stazione di ( leonardo , siemens medical systems , elaborazione erlangen , germania ) , stata eseguita interattivamente dal medico radiologo utilizzando varie tecniche di rielaborazione bie tridimensionali : ricostruzioni multiplanari ( mpr ) , proiezione di massima intensit ( mip ) e volume rendering technique ( vrt )  . 
sono state considerate complicanze dellesame lo sviluppo di una reazione allergica al mezzo di contrasto , il deterioramento della funzione renale e lo stravaso del mezzo di contrasto nella sede di iniezione . trattandosi di uno studio retrospettivo laccuratezza dellangio - tc nella diagnosi di occlusione dellarteria basilare stata valutata confrontando i dati relativi ai 12 pazienti che hanno eseguito anche uno studio angiografico , assunto quale gold - standard . 
le procedure agiografiche sono state eseguite con angiografo digitale ( multistar plus top , siemens medical systems , erlangen , germania ) e 1222 radiol med ( 2010 ) 115 : 12191233 digital angiography system ( top multistar plus , siemens medical systems , erlangen , germany ) by three radiologists ( bg , ht and nl ) with experience in interventional neuroradiology . 
two treatment methods were employed : intra - arterial lysis ( ial ) and mechanical clot removal ( mcr ) associated with locoregional thrombolytic infusion with , in both cases , intravenous administration of 5 , 000 iu heparin following cta confirmation of basilar artery occlusion . condotte da tre radiologi ( bg , ht , nl ) con esperienza interventistica e neuroradiologica . 
sono state utilizzate due modalit di trattamento : la trombolisi intrarteriosa e la rimozione meccanica del trombo associata allinfusione loco - regionale di trombolitico accomunate dalla somministrazione endovenosa di 5000 ui di eparina alla conferma angio - tc dellocclusione di basilare . trombolisi intrarteriosa intra - arterial lysis after selective catheterisation of the basilar artery as far as the thrombus by means of a microcatheter ( vasco + 18 , balt extrusion , montmorency , france ; guidewire transend 0.014 , 205 cm , boston scientific , natick , ma , usa ) , up to 800900 , 000 units of urokinase ( mayne pharma ) were infused over a period of 90 min . mechanical clot removal after catheterisation of the basilar artery and crossing the occlusion with the tip of the microcatheter ( vasco + 21 , balt extrusion ; guidewire transend 0.014 , 205 cm ) , the thrombus was removed by withdrawing the basket device ( catch , balt extrusion )  . 
additionally , in the event of partial removal and to improve microcirculatory perfusion , up to 800 , 000 units of urokinase ( mayne pharma ) were infused locoregionally . following the interventions , postprocedural angiography was used to document the degree of reperfusion and identify any signs of microembolisation resulting from fragmentation of the thrombus . 
at the end of the procedure , all patients underwent brain ct and , haemorrhagic complications having been excluded , were started on heparin therapy with the continuous infusion of 1 , 000 iu / h for 24 h . 
in caso di rimozione parziale del trombo e per migliorare la perfusione del microcircolo si infondono loco - regionalmente fino a 800000 unit di urokinasi ( mayne pharma )  . al termine di entrambe le modalit di intervento un controllo angiografico ha documentato il grado di riperfusione del microcircolo evidenziando eventuali segni di microembolizzazione conseguenti alla frammentazione del trombo . 
a procedura completata tutti i pazienti hanno eseguito una tc dellencefalo ed , escluse complicanze emorragiche , hanno intrapreso una terapia eparinica con infusione continua di 1000 ui / ora per 24 ore . 
il successo procedurale , valutato sullo studio angiografico finale , stato graduato con una scala 03 , analogamente alla valutazione della rivascolarizzazione del miocardio infartuato ( thrombolysis in myocardial infarction , timi ) [ 18 ] : 0 : assenza di ricanalizzazione ; 1 : ricanalizzazione dei vasi di calibro maggiore senza visualizzazione del microcircolo ; 2 : ricanalizzazione dei vasi di calibro maggiore con parziale visualizzazione del microcircolo ; 3 : ricanalizzazione dei vasi di calibro maggiore con buona visualizzazione del microcircolo . sono state considerate complicanze legate alla procedura lo sviluppo di unemorragia parenchimale e la dissezione arteriosa vertebrale o basilare ; a queste vanno affiancate le complicanze proprie di ogni procedura angiografica ( reazione allergica al mezzo di contrasto , ematoma inguinale o retroperitoneale , pseudoaneurisma femorale )  . 
the degree of neurological impairment at the time of diagnosis was assessed with the glasgow coma scale ( gcs ) , whereas clinical outcome at 3 months was classified according to the modified rankin scale ( mrs )  . results of the 59 patients who underwent unenhanced brain ct for clinical suspicion of basilar artery thrombosis , 33 were excluded from the study as a result of a diagnosis of parenchymal or subarachnoid haemorrhage ( 12 and 21 patients , respectively )  . 
the series thus consisted of 26 patients ( 16 men , 10 women , mean age 54.3513.7 years ) undergoing cta of the intracranial circulation to confirm the ct finding of basilar artery hyperdensity ( n = 19 ) or to clarify a negative ct finding in the presence of severe neurological impairment ( n = 7 )  . 
among the 19 patients with a ct finding of basilar artery hyperdensity , cta revealed 14 cases ( 73.7% ) of arterial occlusion , whereas among the seven patients with a negative finding , it revealed only one case ( 14.3% ) of basilar artery occlusion . all cta examinations were technically evaluable , being unaffected by motion artefacts and demonstrating good opacification of skull - base circulation . 
paracoronal mip reconstructions in the plane of the basilar artery allowed recognition of the location and extent of the occluded segment , as well as providing crucial information on the distal vertebral arteries ( hypoplasia , occlusion , dominant artery ) needed for planning the interventional procedure . we did not record any complications due to the cta examinations . the six patients with negative ct and cta findings underwent further diagnostic workup that consisted of brain magnetic resonance imaging ( mri ) with diffusion - weighted acquisitions and time of flight mr angiography within 48 h of the acute infarction . 
in this instance comparative assessment of the scans with and without contrast medium demonstrated that calcification of the tip of the basilar artery masked the hyperdensity of a thrombus located in the adjamomento della diagnosi stato valutato attraverso la glasgow coma scale ( gcs ) , mentre loutcome clinico a tre mesi stato classificato in base alla scala di rankin modificata ( modified rankin scale , mrs )  . risultati dei 59 pazienti sottoposti a tc dellencefalo senza somministrazione di mezzo di contrasto nel sospetto clinico di trombosi dellarteria basilare , 33 sono stati esclusi dallo studio per diagnosi di emorragia parenchimale o subaracnoidea ( 12 e 21 pazienti )  . 
la casistica quindi costituita da 26 pazienti ( 16 maschi , 10 femmine ; et media 54 , 3513 , 7 anni ) sottoposti ad angio - tc del circolo intracranico per confermare il reperto tc di iperdensit dellarteria basilare ( 19 pazienti ) o per chiarire un reperto tc negativo a fronte di una grave compromissione neurologica ( 7 pazienti )  . 
tra i 19 pazienti con rilievo tc di iperdensit dellarteria basilare langio - tc ha evidenziato 14 casi ( 73 , 7% ) di occlusione arteriosa ; mentre tra i 7 pazienti con reperto negativo stato diagnosticato un solo caso ( 14 , 3% ) di occlusione dellarteria basilare . 
le ricostruzioni mip paracoronali secondo il piano dellarteria basilare hanno permesso di riconoscere sede ed estensione del tratto occluso e di ottenere alcune indicazioni sul tratto distale delle arterie vertebrali ( ipoplasia , occlusione , arteria dominante ) utili per il radiologo interventista nella pianificazione della procedura interventistica . 
non abbiamo registrato alcuna complicanza conseguente allesecuzione degli esami angio - tc . i 6 pazienti con negativit dei reperti tc ed angio - tc hanno proseguito liter diagnostico eseguendo una risonanza magnetica ( rm ) cerebrale con acquisizioni in diffusione ed angio - rm per tempo di volo ( tof ) entro 48 ore dallevento acuto . 
in tutti i casi stata confermata la perviet dellarteria basilare ed in 4 si sono evidenziate aree ischemiche minori nel territorio vertebro - basilare ( cervelletto , ponte e talamo )  . 
the paracoronal and parasagittal mpr and mip reconstructions along the axis of the basilar artery proved particularly useful in making the diagnosis . among the 15 patients with a cta diagnosis of basilar artery occlusion , a woman > 80 was not treated ( case 4 ) and died the next day as a result of the acute event . 
two were transferred to other centres ( cases 2 and 5 ) , as there was no one of the three interventional radiologists experienced in neuroradiological procedures , whereas 12 ( eight men , four women , mean age 58.6612.83 years ) continued the diagnostic and therapeutic workup at our hospital . 
we do not have data on the treatment and outcome of the transferred patients . table 1 shows patients demographic and clinical data , time elapsed since symptom onset and location and extent of the occlusion . 
ial procedures were on average shorter than paracoronali e parasagittali secondo lasse della basilare . tra i 15 pazienti con diagnosi angio - tc di occlusione dellarteria basilare , una donna ultraottantenne non stata trattata ( caso 4 ) ed deceduta il giorno seguente levento acuto . 
per i restanti 14 pazienti stata posta indicazione alla terapia endovascolare : 2 sono stati trasferiti non essendo presente uno dei tre radiologi interventisti esperti in procedure neuroradiologiche ( casi 2 e 5 ) , 12 ( 8 maschi , 4 femmine ; et media 58 , 6612 , 83 anni ) hanno proseguito liter diagnostico - terapeutico nel nostro ospedale . 
non disponiamo dei dati relativi alla modalit di trattamento ed alloutcome dei pazienti trasferiti . in tabella 1 sono riportati i dati anagrafici e clinici dei pazienti , il tempo trascorso dellesordio sintomatologico nonch sede ed estensione dellocclusione . 
le procedure di lisi intrarteriosa sono risultate in media pi brevi rispetto a quelle di rimozione meccanica del trombo ( 111 , 628 , 4 vs 11544 , 2 min )  . 
in only two cases was visualisation of the microcirculation at postprocedural angiography found to be unsatisfactory ( case 9 treated with mcr and case 11 treated with ial ) , and the outcome of the urokinasi risultato in media significativamente maggiore nei pazienti trattati con iat rispetto a quelli sottoposti a mt ( 716000 vs 360000 unit ) , ciononostante abbiamo registrato una sola complicanza emorragica nel primo gruppo e due nel secondo gruppo ( tabella 2 )  . in 10 / 12 pazienti trattati ( 83 , 3% ) stata ottenuta una buona ricanalizzazione della basilare ( timi 2 - 3 ) , solo in 2 casi la visualizzazione del microcircolo al controllo angiografico finale stata poco soddisfacente ( caso 9 trattato con mt , caso 11 trattato con iat ) e loutcome dei pazienti a tre mesi stato scadente ( caso 9 : mrs 4 , caso 11 : mrs 5 )  . 
due 1226 radiol med ( 2010 ) 115 : 12191233 table 2 type of endovascular procedure and technical and clinical outcomes urokinase dosage ( u ) procedure time ( min ) timi result technical failure and complications outcome 3 months ( mrs ) type of procedure ial ( pta ) mcr ( stent ) iat ( pta ) mt ( stent ) 800 , 000 800 , 000 900 , 000 800 , 000 100 , 000 800 , 000 700 , 000 500 , 000 600 , 000 200 , 000 100 , 000 500 , 000 800000 800000 900000 800000 100000 800000 700000 500000 600000 200000 100000 500000 haemorrhage haemorrhage timi , thrombolysis in myocardial infarction ; mrs , modified rankin scale ; ial , intra - arterial lysis ; mcr , mechanical clot removal ; pta , angioplasty ; rh , retroperitoneal haematoma tabella 2 tipologia di intervento endovascolare , risultati procedurali e clinici tipo di procedura dosaggio urochinasi durata procedura ( min ) risultato timi insuccesso tecnico e complicanze outcome 3 mesi ( mrs ) timi , thrombolysis in myocardial infarction ; mrs , modified rankin scale ; iat , trombolisi intrarteriosa ; mt , rimozione meccanica del trombo ; pta , angioplastica ; erp , ematoma retroperitoneale ; ie , infarcimento emorragico patients at 3 months was poor ( case 9 mrs 4 ; case 11 mrs 5 )  . 
in un paziente ( caso 11 ) con occlusione del tratto prossimale della basilare , nel quale le immagini angio - tc avevano gi evidenziato lesioni stenosanti al tratto intracranico delle arterie vertebrali , avendo ottenuto una ricanalizzazione poco soddisfacente radiol med ( 2010 ) 115 : 12191233 1227 fig . 
cta ( b ) shows thrombosis of the proximal and middle portions of the basilar artery , findings confirmed with angiography of the left vertebral artery ( c )  . 
la tc nativa ( a ) evidenzia liperdensit dellarteria basilare , lo studio angio - tc ( b ) documenta la trombosi dei tratti prossimale e medio dellarteria basilare , tale reperto confermato con angiografia vertebrale sinistra ( c )  . 
un controllo angio - tc in 38a giornata confermava la stenosi basilare ed a fronte di un ottimo recupero psico - motorio del paziente ( mrs 1 ) , stato deciso di procedere , a tre mesi dallevento acuto , al posizionamento di uno stent ( pharos 2 , 5 - 10 , micrus endovascular )  . 
il controllo angiografico dopo infusione loco - regionale di 800000 unit di urokinasi ( c ) dimostra la ricanalizzazione dellarteria basilare con opacizzazione delle arterie cerebrali posteriori e discreta visualizzazione del microcircolo ( timi 2 )  . for angiography ( 12 / 12 ) : in 6 / 7 ( 85.7% ) ial procedures , recanalisation of the basilar artery and restoration of the microcirculation were satisfactory ( timi 23 ) , whereas in only one case was basilar artery recanalisation obtained with unsatisfactory visualisation of the microvasculature ( timi 1 )  . 
similarly , in 4 / 5 ( 80% ) mechanical removal procedures , recanalisation of the basilar artery and restoration of the microcirculation were satisfactory ( timi 23 ) , whereas in one case only did we achieve basilar artery recanalisation alone ( timi 1 )  . the mortality rate in our case series was 21.4% ( 3 / 13 ) for patients followed in our hospital and 16.6% ( 2 / 12 ) if only the patients treated were considered . 
there were three complications : two ( 16.6% ) of haemorrhage of ischaemic brainstem lesions ( cases 14 and 15 ) and one ( 8.3% ) of retroperitoneal haematoma , which was treated conservatively ( case 9 )  . discussion controllo angio - tc , a sei mesi dal posizionamento , ha confermato la perviet dello stent . in tutti i pazienti inviati in sala angiografica ( 12 / 12 ) stato possibile completare la terapia endovascolare : in 6 / 7 ( 85 , 7% ) procedure di lisi intrarteriosa la ricanalizzazione della basilare e del microcircolo stata soddisfacente ( timi 2 - 3 ) , mentre in un solo caso stata ottenuta la ricanalizzazione della basilare con insoddisfacente visualizzazione del microcircolo ( timi 1 ) , analogamente in 4 / 5 ( 80% ) procedure di rimozione meccanica del trombo la ricanalizzazione della basilare e del microcircolo stata soddisfacente ( timi 2 - 3 ) ed in un solo caso stata ottenuta la sola ricanalizzazione della basilare ( timi 1 )  . il tasso di mortalit della nostra casistica del 21 , 4% ( 3 / 13 ) per i pazienti seguiti nel nostro ospedale , e del 16 , 6% ( 2 / 12 ) se consideriamo solo i pazienti trattati . 
abbiamo registrato tre complicanze : 2 casi ( 16 , 6% ) di infarcimento emorragico di lesioni ischemiche truncali ( caso 14 e 15 ) ed 1 ( 8 , 3% ) di ematoma retroperitoneale trattato conservativamente ( caso 9 )  . the outcome of patients with basilar artery thrombosis depends on the severity of the clinical picture , location and extent of the occlusion , timeliness of therapeutic intervention and degree of recanalisation achieved [ 11 , 19 , 20 ]  . discussione loutcome dei pazienti con trombosi dellarteria basilare dipende dalla gravit del quadro clinico allesordio , dalla radiol med ( 2010 ) 115 : 12191233 1229 fig . 
4a - f paziente femmina , 45 anni . langio - tc ( a ) evidenzia locclusione dellapice dellarteria basilare , langiografia vertebrale destra ( b ) conferma sede ed estensione dellocclusione . 
il controllo angiografico dopo il ritiro del dispositivo e linfusione loco - regionale di 100000 unit di urochinasi ( e , f ) dimostra la ricanalizzazione dellarteria basilare con buona visualizzazione del microcircolo ( timi 3 )  . the first two factors are beyond intervention , but the time needed to reach a definitive diagnosis can be reduced . 
however , our data demonstrate that in 6 / 7 patients , cta confirmed the negative results of the ct brain scan and , in particular , the lack of evidence of basilar artery hyperdensity , the negative predictive value of which was 86% . 
 [ 7 ] who , in a larger case series , reported a negative sede e dallestensione dellocclusione , dalla rapidit dellintervento terapeutico e dal grado di ricanalizzazione ottenuto [ 11 , 19 , 20 ] : non possiamo intervenire sui primi due fattori ma possiamo ridurre il tempo necessario per formulare una diagnosi di certezza . 
tuttavia dai dati raccolti emerge che in 6 / 7 pazienti langio - tc ha confermato la negativit del quadro tc ed in particolare la negativit del segno della basilare iperdensa il cui valore predittivo negativo risultato dell86% . 
cta ( a ) and angiography of the right vertebral artery ( b ) show thrombosis in the proximal portion of the basilar artery . postprocedural angiography ( c ) after mechanical clot removal and local infusion of 200 , 000 u of urokinase demonstrates recanalisation of the basilar artery , with a short stenosis in its proximal portion ( arrowhead )  . 
cta 1 month after the acute event ( d ) demonstrates patency of the basilar artery , with persistence of the proximal stenosis , which was treated with angioplasty and stent positioning ( e )  . 
il controllo angiografico dopo rimozione meccanica del trombo ed infusione loco - regionale di 200000 unit di urochinasi ( c ) dimostra la ricanalizzazione dellarteria basilare con stenosi breve al tratto prossimale ( punta di freccia )  . 
langio - tc eseguita ad un mese dallevento acuto ( d ) documenta la perviet dellarteria basilare con persistenza della stenosi prossimale che viene trattata con angioplastica e posizionamento di stent ( e )  . 
il controllo angiotc dopo sei mesi ( f ) conferma la perviet dello stent . radiol med ( 2010 ) 115 : 12191233 1231 predictive value of 95.2% for the finding of basilar artery hyperdensity . 
this means that carrying out cta in a patient with suspected posterior circulation ischaemia and a negative ct brain scan fails to provide additional diagnostic information in 8595% of cases . 
faced with a ct brain scan that is negative for basilar artery hyperdensity , it is recommended that cta be carried out immediately only when the patients clinical condition is compatible with a basilar occlusion . 
if , however , the symptoms are suggestive of posterior circulation insufficiency , then it is recommended to pursue the diagnostic workup with elective mri . in our series , the positive predictive value of basilar artery hyperdensity was 73.7% , the false - positive results being 5 / 19 . 
if we compare the values of basilar artery density by separating , a posteriori , patients with or without basilar artery thrombosis , we note that the average value for the two groups was 57.45 hu and 396 hu , respectively . this element prompts us to raise the lowest suspicion threshold to 50 hu . 
we point out , however , that the evidence of basilar artery hyperdensity is not based on the quantification of vessel density only , the measurement of which may be impeded by ct artefacts typical of the posterior cranial fossa or from haematocrit values that are too high . 
in our opinion , the threshold value is only indicative , and to confirm a finding of basilar hyperdensity , one should also compare density values measured at the middle cerebral arteries . 
on the other hand , appears to be more difficult to reduce errors resulting from the presence of wall calcifications that can both produce an overestimation of mean basilar density as well as masking the hyperdensity of a thrombus closely adjacent to the calcification . 
in our opinion , symptomatic patients with evidence of atherosclerotic calcification of the basilar artery on brain ct have an indication for cta . ct study of the intracranial circulation , as a result of the previously mentioned benefits , seems , in our opinion , to represent the most appropriate test for confirming , as rapidly as possible , a clinicalradiological suspicion of occlusion of the basilar artery . to our knowledge , no randomised controlled prospective studies exist that indicate the optimal therapeutic approach , the only prospective randomised study having been suspended as a result of low recruitment after collecting data from just 16 patients [ 21 ]  . 
questi dati suggeriscono un possibile cambiamento nellatteggiamento diagnostico : a fronte di un quadro tc dellencefalo negativo per iperdensit dellarteria basilare indicato eseguire immediatamente langio - tc solo quando le condizioni cliniche del paziente sono compatibili con un quadro di occlusione di basilare , mentre se la clinica suggestiva per insufficienza del circolo posteriore indicato proseguire liter diagnostico in elezione mediante rm . nella nostra casistica il valore predittivo positivo del segno della basilare iperdensa stato del 73 , 7% avendo riportato 5 / 19 falsi positivi . 
se confrontiamo il valore di densit dellarteria basilare dividendo a posteriori i pazienti con o senza trombosi di basilare constatiamo che il valore medio per i due gruppi rispettivamente 57 , 45 hu e di 396 hu : questo dato ci spinge ad innalzare il valore soglia minimo sospetto a 50 hu . 
va sottolineato come il reperto di iperdensit della basilare non si basi solo sulla quantificazione della densit del vaso che pu essere inficiata dagli artefatti tc tipici della fossa cranica posteriore o da valori di ematocrito troppo elevati . 
a nostro giudizio il valore soglia indicativo , per confermare un reperto di iperdensit della basilare ci si deve avvalere anche del confronto dei valori di densit misurati a livello delle arterie cerebrali medie : se tali valori sono sovrapponibili verosimilmente si tratta di una falsa positivit . 
pi difficile appare invece ridurre gli errori indotti dalla presenza di calcificazioni parietali che possono causare sia una sovrastima del valore medio di densit della basilare , sia mascherare liperdensit di un trombo in stretta adiacenza alla calcificazione . 
a nostro giudizio nei pazienti sintomatici con evidenza alla tc dellencefalo di malattia aterosclerotica calcifica della basilare vi indicazione a procedere con langio - tc . lo studio tc del circolo intracranico , per i vantaggi gi citati , appare , a nostro giudizio , lesame pi indicato per confermare , nel pi breve tempo possibile , un sospetto clinico - radiologico di occlusione dellarteria basilare . non esistono , a nostra conoscenza , studi prospettici randomizzati e controllati per indicare lapproccio terapeutico ottimale , lunico studio prospettico randomizzato intrapreso stato sospeso per low recruiment dopo aver raccolto i dati di 16 pazienti [ 21 ]  . 
i lavori presenti in letteratura sono spesso retrospettivi ed inficiati da una scarsa numerosit del campione ( spesso < 10 ) , essi sono inoltre difficilmente confrontabili per la variabilit dei criteri di inclusione ( in particolare per il tempo dallesordio sintomatologico ) e per la variabilit delle modalit di trattamento ( anticoagulazione , lisi endovenosa o intra - arteriosa con urochinasi o rtpa , rimozione meccanica del trombo , angioplastica )  . 
in this respect , data collected in the basilar artery international cooperation study ( basics ) multicentre registry completed in september 2007 should allow the design and proposal of a prospective randomised controlled trial , even though many experts agree that randomised placebo - controlled trials in the treatment of basilar artery occlusion are not ethically correct [ 15 ]  . 
in our experience , the use of devices for mcr reduce the required dose of thrombolytic agent and thus , hypothetically , the risk of bleeding complications . however , this does not emerge clearly from our case series , which showed a similar incidence of brainstem haemorrhage for the two types of treatment ( 1 / 7 ial , 14.3% ; 1 / 5 mcr , 20% )  . 
in addition , perhaps due to the small sample size , we found no correlation between time from symptom onset and technical success , between technical success and clinical outcome or between severity of the clinical picture and occlusion location . 
instead , worse results in terms of clinical outcome at 3 months were seen in patients > 60 years ( mrs < 3 in 100% of patients < 60 as against an mrs < 3 in 16.6% of those > 60 ) , even though recanalisation rates for the two age groups were similar . 
this finding may support a more aggressive treatment approach in younger patients . although it is beyond the scope of this paper to suggest the best therapeutic choice , it should be emphasised that compared with systemic fibrinolysis , the endovascular approach offers the additional advantage of allowing dilatation / stenting of tight stenoses that represent a possible cause of early reocclusion . basilar artery international cooperation study ( basics ) , completato nel settembre 2007 , dovrebbero consentire di disegnare e proporre uno studio prospettico randomizzato controllato anche se oggi molti esperti sono concordi nel sostenere che studi randomizzati e placebo - controlled nel trattamento dellocclusione di basilare non siano eticamente corretti [ 15 ]  . 
le linee guida sono in continua evoluzione ed allapproccio endovascolare si sta affiancando anche quello del bridging terapeutico dove alla terapia sistemica si affiancano quelle endovascolari litica o meccanica e langioplastica percutanea / stenting in caso di stenosi residua severa [ 22 ]  . i nostri risultati sono sovrapponibili a quelli riportati in letteratura per quanto riguarda il tasso di ricanalizzazione ( 83 , 3% ) , loutcome a tre mesi , la mortalit ( 16 , 6% ) e le complicanze ( minori 8 , 3% , maggiori 16 , 6% ) dei pazienti trattati con approccio endovascolare . 
tuttavia questo dato non emerge dalla nostra casistica dove abbiamo registrato unincidenza di infarcimento emorragico truncale sovrapponibile per i due tipi di trattamento ( 1 / 7 iat , 14 , 3% ; 1 / 5 mt , 20% )  . 
non abbiamo neppure registrato , forse anche per la bassa numerosit del campione , una correlazione tra tempo dallesordio sintomatologico e successo tecnico , tra successo tecnico ed outcome clinico o , tra gravit del quadro clinico alla diagnosi e sede dellocclusione . 
al contrario abbiamo registrato risultati peggiori in termini di outcome clinico a tre mesi nei pazienti ultrasessantenni ( mrs < 3 nel 100% degli infrasessantenni ; mrs < 3 nel 16 , 6% degli ultrasessantenni ) a fronte di tassi di ricanalizzazione sovrapponibili per le due fasce di et . 
questo dato pu supportare un approccio terapeutico pi aggressivo nei pazienti pi giovani . questo lavoro esula da voler indicare quale sia la scelta terapeutica da seguire , tuttavia va sottolineato come lapproccio endovascolare offra il vantaggio , rispetto alla fibrinolisi sistemica , di eseguire la dilatazione / stenting di stenosi serrate , possibili causa di riocclusione precoce . conclusions multislice ct plays an essential role in diagnosing this severe form of stroke , as it allows a fast and accurate angiographic demonstration of arterial thrombosis immediately after the initial unenhanced brain scan . 
given the severity of the disease , a better distribution of facilities capable conclusioni la tcms svolge un ruolo essenziale nella diagnosi di questa grave forma di ictus permettendo , immediatamente dopo lo studio nativo , lesecuzione di uno studio angiografico con rapida ed accurata dimostrazione della trombosi arteriosa . 
nella nostra esperienza hanno trovato spazio sia la trombolisi locoregionale sia la rimozione del trombo con dispositivi meccanici , ed in un singolo caso , il trattamento di una stenosi dellarteria basilare con stent metallico . 
cademartiri1 , 2 1dipartimento di radiologia e del cardio - polmonare , azienda ospedaliero - universitaria di parma , c / o piastra tecnica , piano 0 , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di fisica sanitaria , ospedale niguarda , milano , italy 4dipartimento di radiologia , ospedale borgo roma , universit degli studi , verona , italy 5dipartimento di radiologia e cardiologia , ospedale san gennaro , napoli , italy 6dipartimento di radiologia , universit di palermo , palermo , italy 7dipartimento di radiologia , azienda ospedaliero - universitaria di genova , genova , italy 8dipartimento di radiologia e cardiologia , universit di foggia , foggia , italy correspondence to : f . 
in particular , we focus on issues concerning technological development , radiation dose , implementation , training and organisation . keywords computed tomography coronary angiography conventional coronary angiography coronary artery disease radiation dose training riassunto langiografia coronarica con tomografia computerizzata ( ctca ) passata in 10 anni da strumento di ricerca investigativa a strumento clinico di uso routinario . 
la causa di questo risiede probabilmente nel fatto che la velocit dellevoluzione tecnologica ha superato ampiamente la capacit del mondo scientifico di sviluppare dati che definiscano meglio il campo di utilizzo . 
a questo si aggiunge il fatto che ad ogni nuova generazione di apparecchi per la tomografia computerizzata ( tc ) le reali e potenziali applicazioni si espandono ulteriormente . abbiamo revisionato lo stato dellarte corrente sulla ctca . 
in particolare , vengono approfonditi gli aspetti inerenti levoluzione tecnologica , la dose da radiazioni ionizzanti , limplementazione , il training e lorganizzazione . parole chiave angiografia coronarica con tomografia computerizzata angiografia coronarica convenzionale malattia aterosclerotica coronarica dose di radiazioni formazione 1180 introduction computed tomography coronary angiography ( ctca ) has been one of the major innovations in medical diagnostics over the past 10 years [ 1 ]  . 
from the initial studies performed with 4 - slice ct scanners , we have arrived at the dawn of the era of low - dose ctca [ 24 ]  . 
the major issues that need to be addressed with regard to the clinical use of ctca include radiation dose , operator training , organisation and implementation . these issues are interrelated and will have a significant impact on the future scenarios of diagnostic imaging and radiology departments . 
in particular , we paid special attention to issues of technological development , dose of ionising radiation , implementation , operator training and organisation . results and appropriateness criteria / guidelines ctca is characterised by high sensitivity ( > 90% ) and a high negative predictive value ( npv ) ( > 98% ) [ 911 ]  . 
this is supported by several documents published by the european society of cardiology ( esc ) and the american heart association / american college of cardiology ( aha / acc ) [ 58 ]  . settings in which performing a ctca for suspected cad is desirable or appropriate consist of patients at intermediate cardiovascular risk with equivocal or nondiagnostic stress test ( e.g. , submaximal stress test ) or individuals in whom stress tests are unfeasible [ 58 ]  . 
other areas of use are the evaluation of coronary stents , provided they are of sufficiently large diameter ( 3.03.5 mm ) and sufficiently proximal , and postoperative evaluation of coronary artery bypass graft ( cabg ) surgery [ 58 ]  . limitations the main limitations of ctca are linked to the reduction in radiol med ( 2010 ) 115 : 11791207 introduzione langiografia coronarica con tomografia computerizzata ( ctca ) costituisce una della maggiori innovazioni in campo medico diagnostico degli ultimi dieci anni [ 1 ]  . dalle prime esperienze con la tomografia computerizzata ( tc ) a 4 strati siamo oggi allalba dellera della ctca a bassa dose da radiazioni ionizzanti [ 24 ]  . 
mancano , tuttavia , ampie ed affidabili evidenze scientifiche su quale sia effettivamente il ruolo della ctca nellambito dei consolidati algoritmi diagnostici in medicina cardio - vascolare . mancano anche delle vere e proprie linee guida di utilizzo , ma ci si riferisce per il momento a raccomandazioni di utilizzo e documenti condivisi [ 58 ]  . 
tra i problemi maggiori che devono essere affrontati per lutilizzo clinico della ctca hanno un ruolo essenziale : la dose di radiazioni , il training , la logistica e limplemetazione . 
in particolare , vengono approfonditi gli aspetti inerenti levoluzione tecnologica , la dose di radiazioni ionizzanti , limplementazione , il training e lorganizzazione . risultati e linee guida / raccomandazioni di utilizzo allo stato delle conoscenze la ctca caratterizzata da una elevata sensibilit ( > 90% ) ed un elevato valore predittivo negativo ( > 98% ) [ 911 ]  . 
la ctca pu quindi rappresentare uno strumento elettivo per lesclusione di malattia coronarica ( cad ) ed caratterizzata da molti vantaggi ed alcuni svantaggi rispetto alla angiografia coronarica convenzionale ( cag ) ( tabella 1 )  . 
questa tesi supportata da alcuni documenti della societ europea di cardiologia ( european society of cardiology , esc ) , delle societ americane di cardiologia ( america heart association , aha , ed american college of cardiology , acc ) [ 58 ]  . 
i casi nei quali si ritiene opportuno o appropriato effettuare una ctca per sospetta malattia coronarica consistono in quelle situazioni nelle quali il paziente a rischio intermedio abbia eseguito test provocativi dubbi o non diagnostici ( per esempio , stress elettrocardiogramma [ ecg ] non massimale ) o quelle nelle quali i test provocativi non siano fattibili [ 58 ]  . 
over the years , the aggressiveness and confidence of operators in the use of beta - blockers in various forms and with various strategies have increased such that today all referral centres have adopted this approach [ 17 ]  . 
dose remains the major criticism of the technique , particularly in the field of cardiology . the harsh criticism in this sense has prompted manufacturers to develop new systems having not only more slices but also capabilities for modulating dose utilisation in many ways . 
the result today is that a ctca examination can be performed with a mean effective dose of 0.8 msv under ideal conditions and with a mean dose of 17 msv according to the complexity and compliance of the patient population enrolled in the study [ 2123 ]  . 
toshiba , instead , has concentrated on increasing the number of slices to the point of achieving complete coverage of the cardiac range with the detector [ 2528 ]  . 
siemens has adopted solutions based on detector oversampling to improve spatial resolution and the introduction of dual - source systems capable of drastically reducing temporal resolution [ 2932 ]  . 
negli anni laggressivit e la confidenza degli operatori nellutilizzo dei beta - bloccanti in varie forme e con varie strategie aumentata ed oggi tutti i centri di riferimento utilizzano questo approccio [ 17 ]  . 
quando le calcificazioni hanno elevata densit e / o dimensioni queste tendono ad oscurare il lume del vaso rendendo difficoltoso o talvolta impossibile la valutazione del grado di stenosi [ 18 ]  . 
le probabili soluzioni a questo problema consistono in risoluzioni spaziali e di contrasto pi elevate ottenibili mediante detettori e tecniche innovative ( nuovi materiali del detettore , doppia energia )  . il problema della dose di radiazioni ha condizionato lo sviluppo della metodica fin dai primi anni [ 19 , 20 ]  . 
le forti critiche in questo senso hanno spinto le case produttrici allo sviluppo di apparecchiature non solo dotate di pi strati ma anche capaci di modulare lutilizzo della dose in molti modi . 
il risultato che oggi possibile effettuare una indagine di ctca somministrando una dose efficace media pari a 0 , 8 msv nella migliore delle ipotesi , e con 17 msv in media a seconda della complessit e della compliance delle popolazioni di pazienti che vengono arruolate per lindagine [ 2123 ]  . 
dopo un lungo periodo ( ossia fino alla generazione a 64 strati ) nel quale la progressione tecnologica per le applicazioni cardiologiche della tomografia radiol med ( 2010 ) 115 : 11791207 1183 fig . 
there are basically two ctca synchronisation techniques : a prospective ecg triggering in which the scan is acquired in sequential axial modality ( step - and - shoot ) , whereby the position of the time window is calculated on the rr interval of the heartbeat prior to the acquisition itself ; b , c retrospective ecg gating in which the scan is acquired in low - pitch spiral modality and the images are retrospectively synchronised with the phase of the cardiac cycle . 
the former technique is characterised by a reduction in radiation exposure but it is also more sensitive to motion artefacts due to reduced or absent flexibility in the reconstruction phase . 
le tecniche di sincronizzazione per la ctca sono essenzialmente due : a triggering ecg prospettico nel quale la scansione viene eseguita con modalit assiale sequenziale ( stepand - shoot ) calcolando la posizione della finestra temporale sullintervallo rr del battito precedente lacquisizione stessa ; b , c gating ecg retrospettivo nel quale la scansione viene eseguita con modalit spirale a basso pitch e le immagini vengono retrospettivamente sincronizzate con la fase del ciclo cardiaco . 
with the advent of 64 - slice systems , the mean effective dose was around 12 msv ( range 818 msv ) in a phase when the prospective technique had already been introduced [ 16 , 35 ]  . prior to the introduction of the prospective scan technique , computerizzata era definita in base al numero di strati ed al tempo di rotazione del sistema tubo detettore , le ditte produttrici hanno deciso di seguire sviluppi diversificati . nel caso di general electric , ad esempio , ha prevalso un approccio focalizzato alla tecnologia del detettore associata a miglioramenti negli algoritmi di ricostruzione [ 24 ]  . per toshiba ha prevalso la logica dellincremento degli strati fino a raggiungere la copertura completa del range cardiaco con il detettore [ 2528 ]  . 
siemens ha adottato soluzioni basate sul sovra - campionamento del detettore per una migliore risoluzione spaziale e sullintroduzione di sistemi a due tubi che consentono una drastica riduzione della risoluzione temporale [ 2932 ]  . 
philips ha scelto di perseguire la logica degli strati abbinata ad un incremento della risoluzione temporale e ad un sovra - campionamento del detettore [ 33 , 34 ]  . 
con le apparecchiature a 64 strati la dose efficace media di circa 12 msv ( range 818 ) in una fase nella quale la tecnica prospettica gi stata introdotta [ 16 , 35 ]  . 
prima dellintroduzione della tecnica di scansione prospettica la dose efficace media di radiazioni senza adottare particolari strategie era di circa 15 msv ( maschi ) e 21 msv ( femmine ) , con una ampia variabilit . modulazione prospettica ecg triggerata la prima strategia di riduzione della dose consiste nella modulazione prospettica della corrente del tubo ( amperaggio ) ecg triggerata . 
la riduzione della dose con questa tecnica pu raggiungere il 50% a seconda della frequenza cardiaca ( ossia la riduzione tanto maggiore quanto pi bassa la frequenza cardiaca ) [ 36 ]  . 
these phases correspond to around 400 ms prior to the r - wave ( 65% of the rr interval ) and 275 ms after the r - wave ( 30% of the rr interval ) , respectively . 
in ctca le immagini possono essere ricostruite o acquisite in due fasi principali del ciclo cardiaco : la tele - diastole e la tele - sistole ( pannello superiore )  . 
the advantage of this approach is that it maintains the scan in spiral modality , thus favouring correspondence between the expected temporal window and the window effectively modulazione della dose basata sul profilo di attenuazione del paziente nel momento in cui lapparecchiatura di tomografia computerizzata effettua il topogramma possibile acquisire il profilo di attenuazione longitudinale del paziente . 
in questo modo possibile calcolare quanti fotoni sono necessari per ottenere immagini di qualit diagnostica a seconda della conformazione e dellanatomia radiol med ( 2010 ) 115 : 11791207 1185 fig . 
one radiation dose reduction technique used in ctca performed with retrospective gating consists of modulating the tube current such that the maximum dose is delivered only during the phase of the cardiac cycle in which the diagnostic images are most likely to be reconstructed . 
una tecnica di riduzione della dose di radiazioni in ctca eseguita con tecnica spirale ecg retrospettiva , consiste nel modulare la corrente del tubo per fare in modo che la massima dose sia veicolata solo durante la fase del ciclo cardiaco nella quale pi verosimilmente saranno ricostruite le immagini diagnostiche . 
the main advantage of prospective tube - current modulation ( ctca technique with retrospective gating ) is that the maximum dose exposure window can be regulated by the operator such that the reconstruction of multiple data sets in the same cardiac cycle can be done in search of the data set in which the coronary arteries show the least residual motion . 
il vantaggio principale della modulazione prospettica della corrente ( tecnica ctca spirale ecg retrospettiva ) consiste nel fatto che la finestra di esposizione alla dose massima pu essere regolata dalloperatore in modo da consentire la ricostruzione di multipli dataset iso - cardio - fasici alla ricerca di quello nel quale le coronarie mostrano il minor movimento residuo . 
la riduzione della dose ottenibile mediante lapplicazione di questa tecnica di circa il 33% [ 37 ]  . dose modulation based on patient attenuation profile ( aec ) basso voltaggio when the ct system performs the scout scan , the longitunegli ultimi anni emerso che per effettuare una ctca 1186 radiol med ( 2010 ) 115 : 11791207 fig . 
automatic exposure control exploits the scout scan to calibrate patient attenuation along the z axis ( a ) and in the axial plane ( b ) and adjusts the peak according to patient profile . 
il controllo automatico dellesposizione sfrutta la scansione del tomogramma per calibrare lattenuazione del paziente lungo lasse z ( a ) e sul piano assiale ( b ) , differenziando il picco di corrente a seconda del profilo . 
this technique is also known as automatic exposure control ( aec )  . the dose reduction that can be achieved with aec is around 33% [ 37 ]  . low voltage in recent years , it has been found that ctca can be performed using 100 kv instead of the conventional 120140 kv . 
questo pu essere fatto a condizione che lattenuazione globale del paziente non sia eccessiva , ossia che lindice di massa corporea ( bmi ) non sia > 28 [ 38 , 39 ]  . da notare che lindice di massa corporea un surrogato dellattenuazione del paziente a livello del torace inferiore e che possono esistere discrepanze anche notevoli tra il bmi del paziente e leffettiva attenuazione in quella regione anatomica ( donne con bmi nella norma ed abbondante tessuto mammario )  . 
tuttavia , come abbiamo visto , necessario adottare un pitch molto basso ( 0 , 20 , 35 ) per sovra - campionare le informazioni e questo radiol med ( 2010 ) 115 : 11791207 1187 increase in image noise , which needs to be counterbalanced by an increase in tube current ( mas )  . 
nonetheless , as we have seen , this requires a very low pitch ( 0.20.35 ) to oversample the information , which necessarily leads to a concomitant increase in radiation dose [ 1 ]  . 
the technique has been used with electron - beam ct systems ( ebct ) , which are widely available throughout north america and asia , to stratify risk by quantifying coronary calcium ( calcium score )  . 
ebct is able to capitalise on extremely high temporal resolution ( 50100 ms ) and therefore does not require all of the phases of the cardiac cycle to halt the motion of the coronary arteries during a heartbeat . 
the 4 - slice and 16 - slice ct generations had a temporal resolution of 250 ms and 200 ms , respectively , and were therefore unable to use prospective ecg triggering . 
with the advent of 64 - slice systems , the temporal resolution dropped to 165175 ms , with a simultaneous improvement in the management of heart rate by the operators . 
con questa tecnica le immagini vengono acquisite con modalit sequenziale solo nella fase di interesse del ciclo cardiaco ( ossia la diastole ) con una drastica riduzione della dose di radiazioni [ 3 , 16 , 21 , 4042 ]  . 
tale tecnica stata per molti anni utilizzata sulle apparecchiature di tomografia computerizzata ad emissione di positroni ( ebct ) , ampiamente diffusa in nord america ed in asia , per la stratificazione del rischio mediante quantificazione del calcio coronarico ( calcium score )  . 
lebct pu sfruttare una elevatissima risoluzione temporale ( 50100 ms ) e per questo non necessit di tutte le fasi del ciclo cardiaco per fermare il movimento delle coronarie durante il battito cardiaco . 
le generazioni di tomografia computerizzata a 4 strati ed a 16 strati avevano risoluzione temporale pari a 250 ms e 200 ms , rispettivamente , e non potevano quindi utilizzare il triggering ecg prospettico . 
si tratta infatti di una scansione effettuata con tavolo in movimento ad alta velocit ( pitch > 3 ) ed acquisizione triggerata con lecg in modo prospettico [ 29 , 30 , 32 , 43 ]  . 
the time needed will therefore be equal to half of the gantry rotation time ( left panel )  . with dual source systems , the 180 of rotation can be divided between the two sources and the time required , i.e. 
con le apparecchiature a doppia sorgente , i 180 di rotazione possono essere suddivisi tra le due sorgenti ed il tempo necessario , ossia la risoluzione temporale , per ottenere una singola immagine corrisponder ad un quarto del tempo di rotazione del gantry ( pannello a destra )  . 
currently , the window of the cardiac cycle ( around 600 ms at 60 bpm ) within which data can be acquired in spiral retrospective gating mode lies within end systole and end diastole ( a , upper panel )  . 
this needs to be done because the width of the acquisition time window in single - source systems is around 135175 ms . with dual - source systems , the acquisition time window is 7083 ms , and this allows multiple time windows to be included within a single end - diastolic phase ( c )  . 
correntemente la finestra del ciclo cardiaco ( 600 ms circa a 60 bpm ) allinterno della quale possibile acquisire dati con modalit spirale ecg retrospettiva compresa tra la tele - sistole e la tele - diastole ( a , pannello superiore )  . 
con le apparecchiature a doppia sorgente , la finestra temporale di acquisizione di 7083 ms e questo consente di comprimere multiple finestre temporali allinterno di una sola fase tele - diastolica ( c )  . 
the scan is in fact performed with the patient table moving at high speed ( pitch > 3 ) and the acquisition prospectively triggered with the ecg [ 29 , 30 , 32 , 43 ]  . 
tuttavia , lelevatissima risoluzione temporale consente di ottenere immagini di qualit diagnostica analoghe a quelle delle precedenti tecnologie a parit di condizioni operative ( frequenza cardiaca bassa e regolare )  . 1190 radiol med ( 2010 ) 115 : 11791207 heart scan alone [ 29 , 30 , 32 , 43 ]  . 
a further disadvantage of the technique is that it can be used to acquire only one series of images without even minimum flexibility in the variation in the temporal window . 
nonetheless , the very high temporal resolution makes it possible to obtain diagnostic - quality images similar to those of preceding techniques with similar operating conditions ( low and regular heart rate )  . iterative reconstruction algorithms the ideal reconstruction modality of images at ct is perhaps the exact modality whereby the attenuation value of the pixels / voxels is reconstructed by exploiting all the available information [ 44 ]  . 
they will , in fact , make it possible to obtain elevated spatial and contrast resolution at much higher levels than we are currently accustomed to seeing [ 44 ]  . 
this , then , translates into the possibility of using lower radiation doses than currently required to obtain the same image quality [ 44 ]  . further considerations on dosimetry and management of the costbenefit relationship in light of the abovementioned techniques , the problem of radiation dose in ctca is clearly multifactorial . 
questo si traduce nella possibilit di utilizzare dosi radianti inferiori a quelle correntemente necessarie per ottenere la medesima qualit di immagine [ 44 ]  . considerazioni dosimetriche ulteriori e sulla gestione del rapporto costi benefici alla luce delle tecniche descritte sopra , emerge come il problema della dose di radiazioni in ctca sia decisamente multi - fattoriale . 
esiste il campo dei calcio - antagonisti da utilizzare in caso di controindicazioni al beta - bloccante ( asma documentato del paziente ) , quello dei nitroderivati da somministrare appena prima della scansione per ottenere una dilatazione del circolo coronarico , quello della lidocaina utilizzata per sopprimere le extra - sistolie frequenti , quello delle benzodiazepine utilizzate per ridurre la componente emozionale dellindagine in pazienti particolarmente ansiosi . 
a questi devono essere associati anche i farmaci di rilevanza cardiologica di emergenza ( atropina , adrenalina , ecc . ) che in futuro potranno entrare maggiormente in uso per lutilizzo che si far della ctca nel contesto del dolore toracico acuto . 
si potrebbe dire che per tutte queste ragioni necessario lavorare in costante collaborazione con un cardiologo e che le competenze farmacologiche descritte vanno al di l di quelle radiologiche convenzionali . 
with the new systems and sequential prospective ecg triggering , the dose can be brought below the levels of all the other modalities that use ionising radiation ( < 5msv )  . 
la ctca a 16e 64 - strati con tecnica spirale ecg retrospettiva si pone allo stesso livello della scintigrafia da stress con tecnezio e tallio ( attorno ai 1020 msv )  . 
con le nuove apparecchiature e le tecniche sequenziali ecg prospettiche si scende al di sotto di tutte le altre metodiche che fanno uso di radiazioni ionizzanti ( < 5 msv )  . 
ctca , angiografia coronarica con tomografia computerizzata ; cag , angiografia coronarica coronarografa convenzionale ; cxr , radiogramma del torace in 2 proiezioni ; tc , tecnezio ; tal , tallio ; mr , risonanza magnetica ; echo , ecocardiografia ; stress ecg , test ergometrico . the setting of acute chest pa this suggests the need to work in constant cooperation with a cardiologist and to develop pharmacological knowledge that goes beyond conventional radiological competences . 
it should be noted that the increasing use of ctca will limit the possibility of having a cardiologist available , that resources are limited and that a full ctca procedure requires pharmacological knowledge that , with the exception of resuscitation , the radiologist as physician is not lacking . dose management should also take into account other factors , such as patient build . 
it should be borne in mind that if patients with a bmi > 2830 are referred for ctca , the dose should be increased or the examination should not be performed to avoid unnecessary radiation exposure for the patient . 
attention should nonetheless be paid to difficilmente consentir di poter avere a disposizione un cardiologo , le risorse sono limitate ed inoltre la procedura completa di ctca richiede le competenze farmacologiche che , fatta eccezione per quelle strettamente rianimatorie , al radiologo , in quanto medico , non mancano . 
bene sottolineare che se i pazienti con bmi > 2830 vengono sottoposti a ctca la dose deve essere aumentata oppure lindagine non deve essere eseguita per evitare di sottoporre il paziente ad una inutile esposizione . 
using 100 kv a 30% reduction in dose is expected , with an increased mas at contrast / noise bthe end - systolic spot is available in spiral mode young patients and , in particular , young women [ 45 ]  . however , as described in the next section , evidence supporting the carcinogenic effects of dose levels typically associated with ctca is practically absent . one of main criticisms of ctca from the field of cardiology is that the associated radiation dose is greater than the dose required for performing cag . 
current techniques and caratteristici della ctca sono pressoch assenti . una delle maggiori critiche alla ctca da parte del mondo cardiologico riguarda il fatto che la dose di radiazioni superiore a quella necessaria per effettuare una coronarografia convenzionale diagnostica ( cag )  . 
utilizzando 100kv si ottiene una ulteriore riduzione del 30% in concomitanza con un incremento dellamperaggio per mantenere costante il rapporto contrasto / rumore . bla finestra di ricostruzione tele - sistolica generalmente disponibile nel modo spirale . those available in the near future show that these criticisms can no longer be sustained [ 46 , 47 ]  . elementi normativi regulatory issues it should not be forgotten that cardiology procedures are non si pu trascurare il fatto che le procedure cardiologiche rientrano tra le procedure radiologiche a dose medioalta e che pertanto anche gli aspetti dosimetrici e i conseguenti rischi specifici rivestono rilevanza non trascurabile 1194 radiol med ( 2010 ) 115 : 11791207 fig . 
al di sotto dei 20 anni di et si osserva la maggiore sensibilit alle radiazioni per entrambi i generi . tuttavia , al di sopra dei 40 anni ( freccia ) di et il rischio similare per entrambi i generi e diventa rapidamente trascurabile se confrontato con la necessit di ottenere una informazione diagnostica . among the mediumhigh - dose radiological procedures and as such dosimetry issues and the consequent specific risks must be taken into account during an appropriateness evaluation . 
in the case of medical exposure , however , this attempt at simplification presents a number of shortcomings that significantly limit its use . firstly , the use of the concept of effective dose appears to be inappropriate in light of the uncertainties surrounding the demographic differences ( health status , age and sex ) between the populations of irradiated patients and the populations used for establishing the nominal risk coefficients . these uncertainties could lead to underestimating the health detriment to young patients by a factor of 2 and overestimating the health detriment among adult patients by a factor of 5 [ 48 ]  . 
added to this is the fact that precisely the uncertainty surrounding our knowledge of the doseeffect relationship at low doses is one of the main reasons the nellambito della valutazione dellappropriatezza . 
il concetto di dose efficace rappresenta il tentativo di stimare , con un solo valore , il detrimento sanitario , vale a dire quellindice di rischio che rappresenta il bilancio tra cancerogenesi , diminuzione della durata della vita ed effetti ereditari . 
in primo luogo lutilizzo del concetto di dose efficace non appare appropriato a seguito delle incertezze indotte dalle differenze demografiche ( stato di salute , et e sesso ) tra le popolazioni di pazienti irradiati rispetto alle popolazioni dalle quali sono ricavati i coefficienti nominali di rischio : tali incertezze potrebbero portare a sottostimare il detrimento sanitario sui pazienti giovani di un fattore 2 e a sovrastimare il detrimento sanitario sui pazienti adulti almeno di un fattore 5 [ 48 ]  . 
a ci si aggiunga che proprio lincertezza della conoscenza della relazione dose - effetti alle basse dosi viene citata come uno dei motivi per non ritenere appropriato , nel caso di dosi molto piccole somministrate ad un numero grande di radiol med ( 2010 ) 115 : 11791207 1195 calculation of a hypothetical number of cancer cases or hereditary effects using the concept of collective dose which is strictly connected with that of effective dose is not considered appropriate in the case of very small doses administered to a large number of people [ 4951 ]  . into consideration together , these factors suggest that collective - effective dose estimates for medical exposure should not be used for assessing radiation risks to populations of patients by simple application of the nominal probability coefficients for radiation - induced cancer given by the international commission on radiological protection ( icrp ) , which have been derived for a general population [ 52 ]  . there is , of course , no intention to underestimate the risk of medical exposure to ionising radiation . 
the intention is simply to point out that even in this setting , it would be more appropriate take riskbenefit relationship in a similar manner as is done for other medical procedures characterised by other risk factors or , to stay within the field of radiology , as is done in the evaluation of fatal and nonfatal adverse effects following administration of contrast material . 
for a specific individual risk assessment , in the case of medical exposure , the equivalent dose absorbed by the irradiated tissue should be evaluated , although this is difficult and uncertain given the fact that the organs and tissues involved are often irradiated only partially and in a very heterogeneous manner . 
rather than being used for extrapolating a hypothetical number of radiation - induced tumours , the concept of effective dose should only be used for making comparisons of different procedures , different systems and procedures in different centres or different countries , and different systems provided that the patient or reference population are similar in age and sex [ 4951 ]  . recently , two opposing points of view were published on the mechanism of carcinogenesis from ionising radiation [ 53 , 54 ]  . 
on the one hand , the evidence has been reviewed with the conclusion that the linear model is the best , given the lack of better evidence [ 54 ]  . 
a common feature of the theories is that it is difficult ( if not impossible ) to demonstrate with the available data the existence of a direct relationship between carcinogenesis and radiation doses used for diagnostic medical purposes [ 53 , 54 ]  . 
the fact that there are still two theories is in itself an indication of the marked difficulty in approaching the problem , which as a rule tends to be oversimplified . persone , calcolare un numero ipotetico di casi di tumore o di effetti ereditari utilizzando il concetto di dose collettiva , strettamente connesso a quello di dose efficace [ 4951 ]  . 
 linsieme di tali circostanze fa s che collective effective dose estimates for medical exposures should not be used for assessing radiation risks to populations of patients by simple application of the nominal probability coefficients for radiation - induced cancer given by icrp , which have been derived for a general population [ 52 ]  . 
con ci naturalmente non si vuole sottovalutare il problema del rischio da radiazioni ionizzanti nelle esposizioni mediche : si vuole semplicemente evidenziare come , anche in questo ambito , vada pi propriamente preso in considerazione il rapporto rischio beneficio analogamente a quanto accade o in altre procedure mediche caratterizzate da altri fattori di rischio o , per restare in ambito radiologico , a quanto accade nella valutazione degli effetti avversi fatali e non fatali a seguito della somministrazione di mezzo di contrasto . 
per una valutazione del rischio specifico individuale , nel caso delle esposizioni mediche , dovrebbe essere valutata la dose equivalente assorbita dal tessuto irradiato , valutazione resa difficoltosa e incerta dal fatto che gli organi ed i tessuti interessati risultano spesso irradiati solo parzialmente e in maniera molto eterogenea . 
il concetto di dose efficace , pi che al fine di estrapolare un ipotetico numero di tumori radioindotti , dovrebbe invece essere utilizzato solo per effettuare confronti tra diverse procedure , confronti tra tecnologie e procedure in centri diversi o paesi diversi , confronti tra diverse tecnologie a condizione che il paziente o la popolazione di riferimento siano simili per sesso ed et [ 4951 ]  . recentemente sono stati pubblicati due punti di vista opposti sul meccanismo della cancerogenicit da radiazioni ionizzanti [ 53 , 54 ]  . 
in comune tra le due tesi , si osserva come risulti difficile ( se non impossibile ) dimostrare con i dati disponibili la relazione diretta tra la carcinogenesi e le dosi di radiazioni impiegate per scopi medicali diagnostici [ 53 , 54 ]  . 
il fatto che tuttora esistano due ipotesi di per se indice di una netta difficolt di approccio ad un problema che di regola viene troppo semplificato . apparso di recente uno ampio studio sulla modalit di irraggiamento della popolazione sottoposta a prestazioni medicali [ 55 , 56 ]  . 
the study , performed over a 2 - year period ( 20052007 ) on 952 , 420 patients ( 655 , 613 of whom were exposed to at least one medical procedure with ionising radiation ) , showed that around 80% of patients receive an annual dose of < 3 msv ( 42% of men and 21% of women receive no dose at all ) and that three procedures accounted for around 50% of the annual dose : stress myocardial scintigraphy ( 22.1% ) , abdominal ct ( 18.3% ) and pelvic ct ( 12.2% ) [ 56 ]  . 
these data are of interest to the extent in which they better frame the problem of medical radiation exposure and focus attention on the objective that ideally should be concentrated on . the accompanying editorial , michael lauer ( renowned opponent of ctca due to the associated radiation exposure ) of the national heart , lung and blood institute of bethesda ( usa ) expresses his reservations regarding the increase in diagnostic procedures characterised by the use of ionising radiation and appeals to the medical community to take on greater responsibility in informing patients and in using diagnostic imaging with caution [ 55 ]  . 
there is without doubt a broad consensus with regard to these considerations , even though radiology and diagnostic procedures in general have become , at least in part , an instrument with which many physicians reassure both patients and themselves . cost - effectiveness according to a cost - effectiveness analysis based on italian data , ctca accounts for a total cost of 230.03 euros , whereas the cost associated with cag is 2 , 027.88 euros ( with significant variation from one italian region to another ) [ 57 ]  . 
in an american cost - effectiveness analysis , ctca proved superior to stress single - photon - emission ct ( spect ) when performed as a first examination in patients with suspected cad [ 5861 ]  . 
 nelleditoriale associato al lavoro , michael lauer ( noto oppositore della ctca a causa delle radiazioni ) del national heart , lung , and blood institute di bethesda ( usa ) esprime le sue riserve relative allaumento delle prestazioni diagnostiche caratterizzate da radiazioni ionizzanti e chiede una maggiore assunzione di responsabilit da parte della comunit medica nellinformare i pazienti e nellutilizzare con attenzione limaging [ 55 ]  . 
queste considerazioni sono sicuramente condivisibili anche se la radiologia e la diagnostica in generale sono diventati , almeno in parte , lo strumento con cui molti medici rassicurano il paziente e se stessi . costo - efficacia secondo una analisi di costo - efficacia basata su dati italiani la ctca fa registrare un costo totale di 230 , 03 euro mentre la coronarografia fa registrare un costo totale 2027 , 88 euro ( esiste una ampia variabilit tra regioni ) [ 57 ]  . 
la ctca presenta un rapporto costo - efficacia pi favorevole rispetto alla coronarografia fino all86% di probabilit pretest ossia il rischio cardiovascolare basso ed intermedio ( fig . 11 ) [ 57 ]  . 
studi recenti meta - analitici e di costo - efficacia inglesi dimostrano come la strategia migliore per la diagnosi di malattia coronarica ostruttiva sia quella basata su test da sforzo seguito da ctca oppure lesecuzione diretta della ctca [ 11 ]  . 
in una analisi di costo - efficacia americana la ctca risultata superiore alla stress - spect , se eseguita come primo esame in pazienti con sospetta cad [ 5861 ]  . nello stesso studio la ctca risultata superiore alla stress spect anche dal punto di vista prognostico [ 58 ]  . 
the figure shows the relationship between preand posttest probability ( conditional probability curves ) in different categories of pretest risk with the three main diagnostic modalities ( ecg , mpi , ctca ) in patients with suspected coronary artery disease . 
in patients with a high pretest risk , all three modalities show excellent performance for a positive test , whereas for a negative pretest , ctca has the highest negative predictive value . 
the diagnostic advantage of ctca in this category of patients is nonetheless minimal , as out of 100 ctcas performed , disease will be ruled out in only 1020 patients . 
in patients with intermediate risk , ctca and mpi perform better than ecg for a positive test , whereas for a negative test , ctca has the highest negative predictive value . 
in patients with a low pretest risk , ctca outperforms both mpi and ecg for a positive test , and for a negative test , ctca has the highest negative predictive value . 
la figura mostra il rapporto tra probabilit pree post - test ( curve di probabilit condizionale ) in diverse categorie di rischio pre - test con le tre principali metodiche di diagnosi ( ecg , mpi , ctca ) nei pazienti con sospetta malattia coronarica . 
nei pazienti ad alto rischio pre - test , per un test positivo tutte e tre le metodiche hanno una ottima performance , mentre per un test negativo la ctca ha il pi elevato valore predittivo negativo . 
nei pazienti a rischio intermedio , per un test positivo la ctca e la mpi risultano superiori allecg , mentre per un test negativo la ctca ha il pi elevato valore predittivo negativo . 
nei pazienti a basso rischio , per un test positivo la ctca risulta superiore alla mpi ed allecg , mentre per un test negativo la ctca ha il pi elevato valore predittivo negativo . 
these forecasts are feasible only in a context of adequate clinical governance with constant di adeguato governo clinico con un monitoraggio costante dellappropriatezza delle indicazioni ed una adeguata verifica degli standard di qualit nellesecuzione delle prestazioni . 
le valutazioni di costo - efficacia , tuttavia , devono tenere conto che il codice di rimborso della ctca attualmente non commisurato al reale valore complessivo ( economico , tecnologico , umano )  . 
ctca was introduced in the parma hospital as a clinical instrument in 2005 . data should be interpreted with care , as in recent years , the absolute prevalence of patients undergoing pci has increased . the percentage of procedures that terminated as cag went from 57% in 2002 to 23% in 2008 . 
if in the future the repayment increases , then the general costs and the cost - effectiveness will need to be reviewed . implementation the process of implementing ctca requires major investments in both technology and human resources and a medium to long time frame . 
associated with this is the constant improvement and change in reference standards , which produces a relatively rapid obsolescence of implementazione il processo di implementazione della ctca richiede grandi investimenti sia tecnologici che di risorse umane ed un tempo medio - lungo . 
a questo bisogna associare il costante miglioramento e cambiamento degli standard di riferimento che determina una relativamente rapida obsolescenza delle tecnologie ( vedi ad esempio i cambiamenti avvenuti in pochi anni nellambito della gestione della dose )  . 
inoltre , in non tutti i centri radiol med ( 2010 ) 115 : 11791207 1199 ct systems ( see , for example , changes that occurred in only a few years in the field of dose management )  . 
this can take place in the setting of several specialty schools , for which there are nonetheless difficulties in dedicating a single resource to ctca imaging alone for a year . 
these factors can significantly influence the success of hospital implementation of ctca , and they must be governed appropriately . training as suggested above , training in cardiac radiology and ctca is the greatest challenge facing the technique . 
several american and european scientific societies have defined training sufficient for certifying the operator as being six cumulative months and 400 cases , with 100 being viewed as they ae being performed and 300 evaluated in the presence of an expert examiner [ 5 , 7 ]  . 
these criteria have been defined in an arbitrary fashion and without any preliminary weighting of the real difficulty of guaranteeing the diagnostic performance expected on the basis of the results in the literature . 
 [ 65 ] verified whether 1 year of intensive training in a highly specialised centre with high volumes was sufficient to allow the operators to achieve the expected level of diagnostic accuracy . 
on the basis of these findings , which are currently the only ones of this type , there is a need to structure intensive and relatively long - term training pathways in centres with the appropriate requirements for training personnel . another aspect of training regards pharmacology . 
in this case , the operating universitari sono disponibili risorse tecnologiche ed expertise specialistico adeguato . limplementazione presuppone anche , e al pari degli investimenti strettamente radiologici , degli investimenti di natura organizzativa e gestionale che riguardano i percorsi dei pazienti ( collaborazione e condivisione delle indicazioni con i reparti di medicina nucleare , di cardiologia , di cardiochirurgia , con le divisioni mediche ad indirizzo cardiologico , con il pronto soccorso , ecc . ) , la capacit di garantire un servizio non solo elettivo ma anche in regime di urgenza ( la formazione necessaria per pi di una persona dello staff della radiologia ) , la condivisione dei sistemi informativi sui quali transitano le informazioni di pertinenza cardiologica ( cartella elettronica dei reparti , sistemi ris / pacs cardiologici ) , il personale tecnico ed infermieristico . 
questi fattori sono in grado di condizionare in modo significativo il successo di un processo di implementazione ospedaliera della ctca e devono essere governati in modo appropriato . training come gi anticipato il training nella cardio - radiologia e sulla ctca rappresenta la sfida pi grande in questo momento storico . 
alcune societ scientifiche americane ed europee hanno definito come training adeguato per certificare loperatore 6 mesi cumulativi e 400 casi , di cui 100 visti mentre venivano eseguiti e 300 valutati in presenza di esaminatore esperto [ 5 , 7 ] .questi criteri sono stati definiti in modo arbitrario e senza aver preliminarmente pesato la reale difficolt di garantire le performance diagnostiche attese sulla base dei risultati della letteratura . 
in un recente studio pugliese et al . [ 65 ] hanno verificato se con training intensivo di un anno in un centro di elevata specializzazione e con alti volumi gli operatori potevano raggiungere laccuratezza diagnostica attesa [ 65 ]  . 
sulla base di questa evidenza , per il momento unica , bisogna strutturare dei percorsi di training intensivi e relativamente duraturi in centri che abbiano i requisiti adeguati alla formazione di coloro che andranno ad effettuare queste prestazioni diagnostiche . un altro capitolo della formazione riguarda la farmacologia . 
health risks from exposure to low levels of ionizing radiation : beir viiphase 2 , washington dc , national academies press , 2006 ; icrp103 the 2007 recommendations of the international commission on radiological protection . 
this must take place under the expert monitoring of a cardiologist or at least of a professional able to manage the possible acute complications of the procedure . with regard to ctca , the main pharmacological agents are beta - blockers . 
la presenza del cardiologo non appare quindi un requisito determinante per la preparazione dei pazienti alla ctca . nuove applicazioni le nuove tecnologie messe a disposizione ( vedi sopra ) introducono miglioramenti prestazionali in aree gi note ( visualizzazione delle stenosi coronariche )  . 
the introduction of dual - source systems and dual energy in the scan phase by siemens has reopened a chapter that was closed at the beginning of the 1990s due to technical limitations [ 66 ]  . currently , philips and general electric are introducing technological platforms that offer offer dual - energy scans ( coaxial geometry of the radiation beam )  . 
in practice , this energia in fase di scansione da parte di siemens ha riaperto un capitolo che si era chiuso allinizio degli anni 90 a causa di limitazioni tecniche [ 66 ]  . 
sar inoltre possibile portare nelluso clinico lo studio della vitalit miocardica con tecnica di enhancement 1202 radiol med ( 2010 ) 115 : 11791207 contrast material used for the angiographic scan . 
the technique would also bring the study of myocardial viability into clinical practice with delayed enhancement or conventional techniques , which to date have only demonstrated their feasibility [ 67 ]  . the combined use of faster systems that use a lower dose and exploit dual - energy geometries on cardiac - synchronised scans , together with the probable introduction of new ct contrast media , will in the next few years make the study of myocardial viability a reality in clinical practice [ 68 ]  . 
in this sector , evidence still needs to be provided . the combination of all these potential features suggests a real role for ctca as a one - stop - shop for thoracic vascular disease . 
numerous experiences have demonstrated that ctca has optimal diagnostic value in the setting of acute chest pain [ 70 ]  . tardivo ( delayed enhancement ) che con le tecniche convenzionali ha mostrato per ora solo la fattibilit [ 67 ]  . lutilizzo combinato di macchine pi veloci , in grado di utilizzare meno dose , capaci di sfruttare geometrie a doppia energia sulle scansioni cardio - sincronizzate , e la probabile introduzione di nuovi mezzi di contrasto per tomografia computerizzata consentir nei prossimi anni di effettuare lo studio di vitalit miocardica in ambito clinico [ 68 ]  . le prime esperienze di imaging da stress con ctca utilizzando ladenosina come stressor sono gi state pubblicate [ 69 ]  . 
lo studio da stress effettuato mediante ctca stato molto limitato fino ad ora dalla risoluzione temporale relativamente bassa della metodica ( se confrontata con lecocardiografia e la risonanza magnetica )  . 
in questo settore le evidenze dovranno essere prodotte . sommando queste potenzialit emerge come il ruolo della ctca possa diventare seriemente un one - stop - shop per la patologia vascolare toracica . 
with the introduction of low - dose ctca , an increasing number of patients will undergo examinations that will enable evaluation of the coronary arteries ( with or without specific indication )  . 
con lintroduzione della ctca a bassa dose un numero sempre maggiore di pazienti sar sottoposto ad indagini nella quali sar possibile valutare le coronarie ( con o senza indicazione specifica )  . 
the radiation dose required would not , however , be greater than that normally used for chest ct performed for suspected pulmonary embolisin radiology , however , events of this kind have already happened . 
with the advent of multislice ct , and today with the broad diffusion of 16and 64 - slice scanners , any chest and / or abdominal ct performed in the arterial phase is implicitly a cta . 
in presenza di tc multistrato , ed oggi in particolare con la larga diffusione di apparecchiature a 16 e 64 strati , qualunque tc del torace e / o delladdome effettuata in fase arteriosa diventa implicitamente una cta . 
in alcuni anni da oggi probabile che il referto standard del torace includer una descrizione del cuore e delle coronarie . stratificazione del rischio the practical consequence of all of the above is that contrast - enhanced chest ct could also become a ctca . la conseguenza pratica di quanto detto consiste nel fatto che 1204 radiol med ( 2010 ) 115 : 11791207 in the light of the latest data on the techniques prognostic value , this implication is not only important for the possibility of revealing significant stenoses or coronary occlusions during examinations performed for other indications , but also because even in the absence of significant stenoses or occlusions the prognostic value of subcritical coronary atherosclerosis ( lumen reduction < 50% ) is essential for quantifying the cardiovascular risk in the patient [ 71 ]  . 
nonetheless , what appears to be an incidental finding may be the pathophysiological basis of mortality due to cardiovascular disease ( 40%50% of the total in the western world )  . 
it also appears clear that ctca can be used for risk stratification in an incremental manner with respect to the agatston coronary calcium score and with respect to spect [ 58 , 76 , 77 ]  . fusion imaging with the development of advance cardiovascular imaging techniques , a number of hybrid systems have appeared over the last 10 years [ i.e. 
this fusion technology is based on the concept that the information provided by two or more systems is , in end effect , complementary , not only from the clinical point of view but also from the logistical standpoint [ 78 ]  . 
the real impact of this technology in the field of cardiology , or rather , its costeffectiveness , still needs to be verified , although the preliminary findings are very encouraging and add important information on the individual patient [ 78 ]  . however , these are very expensive systems in the broad sense ( both initially and in terms of technical and medical management ) , and they could easily be replaced by separate systems and a software fusion platforwhat needs to be verified , in addition to the clinical impact , is whether it is worth hybridising the devices or whether it is enough to hybridise the competences on separate devices [ 79 ]  . tc torace con mezzo di contrasto potrebbe diventare anche una ctca . 
alla luce dei dati emergenti sul valore prognostico della metodica , questo risvolto non solo importante per il fatto che possono essere rilevate stenosi significative o occlusioni coronariche nel contesto di indagini effettuate con altre indicazioni , ma anche perch , pur in assenza di stenosi significative o occlusioni , il valore prognostico dellaterosclerosi coronarica sub - critica ( riduzione del lume < 50% ) essenziale per linquadramento del rischio cardiovascolare del nostro paziente [ 71 ]  . 
tuttavia , quello che potrebbe apparire come un reperto collaterale , rappresenta la base fisiopatologica che sostiene la mortalit per malattie cardiovascolari ( 40%50% di quella totale nel mondo occidentale )  . 
appare inoltre evidente come la ctca possa stratificare il rischio in modo incrementale rispetto al calcium score coronarico secondo agatston e rispetto alla spect [ 58 , 76 , 77 ]  . imaging di fusione con lo sviluppo delle metodiche di imaging avanzato cardiovascolare sono nate negli ultimi 10 anni anche le macchine ibride ( pet - ct , spect - ct ) [ 78 ]  . 
questa fusione tecnologica basata sul concetto che le informazioni fornite da 2 o pi apparecchiature siano in ultima analisi complementari , non solo dal punto di vista clinico ma anche dal punto di vista logistico [ 78 ]  . 
limpatto reale di queste tecnologie in ambito cardiologico , o meglio la loro costo - efficacia ancora da verificare ma i primi risultati appaiono molto promettenti ed in grado di aggiungere un consistente contenuto informativo nel singolo paziente [ 78 ]  . 
tuttavia , si tratta di apparecchiature molto costose in senso lato ( sia inizialmente che dal punto di vista della gestione tecnica e medica ) e che potrebbero essere facilmente surrogate da apparecchiature separate e da una piattaforma software di fusione . 
quello che andr verificato , oltre allimpatto clinico , se convenga ibridare la macchina o se sia sufficiente ibridare le competenze su macchine separate [ 79 ]  . conclusioni conclusions in conclusion , new ctca technologies have opened the way to a new paradigm shift in diagnostic imaging . 
in particular , after the first paradigm shift induced by the noninvasive study of coronary arteries , a further paradigm shift lies in the potential extension of cardiac ct to all patients undergoing chest ct , without an additional dose of radiation . in conclusione , le nuove tecnologie di ctca aprono la strada ad un ulteriore cambio di paradigma nel contesto della diagnostica per immagini . 
in particolare , dopo il primo cambio di paradigma indotto dalla possibilit di studiare in modo non invasivo le coronarie , un ulteriore cambio di paradigma consiste nella potenziale estensione degli studi cardiologici mediante tc a tutti i pazienti che eseguono un tc del torace senza dose da radiazioni aggiuntiva . 
passariello1 1department of radiologial sciences , policlinico umberto i , university sapienza , viale regina elena 324 , 00161 rome , italy 2department of urology , policlinico umberto i , university sapienza of rome , italy correspondence to : v . 
panebianco tel + 39 - 06 - 4455602 / 4468587 , e - mail : valeria.panebianco@gmail.com received : 13 august 2009 / accepted : 16 december 2009 / published online : 17 september 2010 springer - verlag 2010 abstract purpose . 
the purpose of this study was to evaluate the role of magnetic resonance spectroscopic imaging ( mrsi ) and dynamic contrast - enhanced magnetic resonance imaging ( dce - mri ) in detecting tumour foci in patients with elevated prostate - specific antigen ( psa ) and negative transrectal ultrasonography ( trus ) - guided biopsy . 
this prospective randomised trial was conducted on 150 patients who underwent [ 1h ] mrsi and dce - mri and targeted biopsies of suspicious areas on mri associated with random biopsies . 
the combined study with [ 1h ] mrsi and dce - mri showed promising results in guiding the biopsy of cancer foci in patients with an initial negative trusguided biopsy . 
scopo del nostro lavoro stato valutare il ruolo della risonanza magnetica ( rm ) con spettroscopia ( mrsi ) e studio dinamico ( dcemr ) nellindividuazione di foci tumorali in pazienti con elevati valori di antigene prostatico specifico ( psa ) e biopsia prostatica guidata tramite trus ( trans - rectal - ultrasound ) - guidata negativa . 
dopo la seconda biopsia , la diagnosi di adenocarcinoma prostatico stata effettuata in 64 / 150 casi . nella nostra popolazione , su una base patient by patient , lmrsi ha mostrato i seguenti valori : sensibilit 82 , 8% ; specificit 91 , 8% ; valore predittivo positivo ( ppv ) 88 , 3% ; valore predittivo negativo ( npv ) 87 , 8% ; accuratezza 85 , 7% . 
la dcemr ha mostrato i seguenti valori : sensibilit 76 , 5% ; specificit 89 , 5% ; ppv 84 , 5% ; npv 83 , 7% ; accuratezza 82% . 
lassociazione delle due metodiche , mrsi e dcemr , aumenta la sensibilit ( 93 , 7% ) , la specificit ( 90 , 7% ) , il ppv ( 88 , 2% ) , il pnv ( 95 , 1% ) e laccuratezza ( 90 , 9% ) nel predire lindividuazione del carcinoma prostatico se paragonata alla sola metodica mrsi o dcemr . radiol med ( 2010 ) 115 : 13141329 1315 keywords prostate cancer biopsy magnetic resonance spectroscopy conclusioni . 
 parole chiave tumore della prostata biopsia risonanza magnetica spettroscopia introduction introduzione thanks to prevention programmes , screening with prostatespecific antigen ( psa ) testing and advances in diagnostic imaging , the presentation of prostate carcinoma ( pc ) has significantly changed over the last 30 years . 
until now , pc screening has involved digital rectal examination ( dre ) and serum psa measurement in association with transrectal ultrasonography ( trus ) , which allows for targeted biopsies when the lesion is visible at ultrasound ( us ) [ 1 ]  . 
psa alone is not a reliable marker for diagnosing pc , as psa levels may increase even in the presence of benign disease , which is extremely frequent in men older than 50 years [ 2 ]  . 
on the other hand , the imaging techniques available to urologists us and magnetic resonance imaging ( mri ) present several limitations in pc diagnosis , and the use of computed tomography ( ct ) for staging purposes is now declining . several recent studies [ 4 , 5 ] reported that mri has a high diagnostic accuracy in evaluating pc when two techniques are combined : spectroscopy ( [ 1h ] magnetic resonance spectroscopic imaging , [ 1h ] mrsi ) and dynamic imaging [ dynamic contrast - enhanced mri ( dce - mri ) ] [ 6 ]  . 
the main advantage of spectroscopy is its ability to provide metabolic information on prostatic tissue by measuring the concentrations of chemical compounds inside contiguous small volumes of interest ( voxels )  . 
at a practical level , pc can be distinguished from normal tissue in the peripheral zone on the basis of the ( cho + cr ) / cit ratio [ 79 ]  . 
whereas increased vascularity in normal tissue appears well grazie ai programmi di prevenzione , alla diffusione del dosaggio dellantigene prostatico specifico ( psa ) come strumento di screening ed ai progressi della diagnostica per immagini , la modalit di presentazione del carcinoma prostatico ( cp ) oggi significativamente cambiata rispetto a 30 anni fa . 
lo screening del cp stato fino ad oggi affidato allesplorazione digito - rettale ( edr ) ed al dosaggio sierico del psa in associazione allecografia trans - rettale ( trus ) , mediante la quale possibile effettuare prelievi bioptici mirati quando la lesione risulta di rilievo ecografico [ 1 ]  . 
il solo psa non risulta un marker affidabile nella diagnosi di neoplasia prostatica in quanto il suo valore pu aumentare anche nella patologie benigne , peraltro molto frequenti nella popolazione maschile ( > 50 anni ) [ 2 ]  . 
daltra parte le tecniche di imaging a disposizione dellurologo , lecografia ( us ) e la risonanza magnetica ( rm ) , mostrano alcuni limiti nella diagnosi del cp e la tomografia computerizzata ( tc ) viene utilizzata sempre meno per la stadiazione . 
 recentemente alcuni studi [ 4 , 5 ] hanno messo in evidenza lelevata accuratezza diagnostica della rm utilizzando la combinazione di due tecniche di studio quali lesame spettroscopico ( 1h - mrsi ) e lesame dinamico ( dcemr ) , nella valutazione del cp [ 6 ]  . 
il vantaggio della spettroscopia risiede nel fatto che essa fornisce informazioni sullattivit metabolica del tessuto prostatico , rilevando le concentrazioni dei composti allinterno di piccoli e contigui volumi di interesse ( voxels )  . 
i metaboliti che nella prostata vengono analizzati con lo studio spettroscopico sono il citrato ( cit ) , la creatina ( cr ) e la colina ( cho )  . 
da un punto di vista pratico , il cp pu essere differenziato dal tessuto sano a livello del mantello periferico sulla base del rapporto ( cho + cr ) / cit [ 79 ]  . 
nel tessuto della zona periferica normale tale rapporto ha valori < 0 , 8 mentre il sospetto di tessuto neoplastico viene avanzato per voxel con valori > 0 , 8 [ 10 , 11 ]  . 
furthermore , as the amount of interstitial space is greater in cancerous than in normal tissue , there is a greater difference in the concentration of contrast agent between plasma and interstitiuthis characteristic results in different enhancement patterns between cancerous and normal tissue [ 12 ]  . trus - guided random biopsy is now the method of choice for histological diagnosis of pc . 
some studies found , however , that up to 30% of tumours may be missed [ 8 ]  . patients with abnormal serum psa levels after a first negative random biopsy pose a major diagnostic challenge to radiologists and urologists [ 13 ]  . 
there is thus a need for a more sensitive and accurate imaging technique to guide the biopsy towards the tumour foci . the purpose of this randomised trial was to prospectively assess the role of [ 1h ] mrsi and dce - mri in identifying pc foci in patients with persistently abnormal serum psa levels ( > 4 ng / ml ) and with a negative first trus - guided random biopsy [ 17 ]  . 
all patients had undergone an initial trusguided random biopsy that had proved negative for adenocarcinoma or for high - grade prostatic intraepithelial neoplasia ( hgpin ) , and all had persistently elevated psa levels ( total psa 4 ng / ml ) and positive or negative dre . exclusion criteria were previous hormonal treatments with luteinising hormone - releasing hormone ( lhrh ) analogues , surgery or radiotherapy for prostate disease and contraindications to mri . 
inclusion criteria were a negative initial prostate biopsy ( no histological diagnosis of pc or precancerous lesions ) and total psa levels persistently 4 ng / ml . all initial biopsies were performed by the same urologist at our department as part of the urological workup . 
il razionale si basa sullindividuazione di tessuto con anormale vascolarizzazione dovuta a fenomeni di neoangiogenesi , principale caratteristica dei tessuti neoplastici [ 12 ] ; mentre nel tessuto sano i fenomeni di aumentata vascolarizzazione si configurano come un evento ben organizzato , nel tessuto neoplastico , questi risultano disorganizzati . 
inoltre , poich la quantit di spazio interstiziale maggiore nel tessuto canceroso rispetto al tessuto normale , vi un divario pi ampio nella concentrazione di mdc tra plasma e questultimo . 
da quanto emerge dai dati di letteratura , serie addizionali di biopsie random convenzionali non migliorano la percentuale di identificazione del tumore , cos da portare ad elevate percentuali di falsi negativi per cp [ 1416 ]  . 
 lo scopo di questo studio randomizzato di analizzare in maniera prospettica il ruolo della 1h - mrsi e della dcemr nellindividuazione di foci di tessuto tumorale prostatico in pazienti con persistente alterazione dei valori sierici di psa ( > 4 ng / ml ) con prima biopsia random trus - guidata negativa [ 17 ]  . materiali e metodi questo studio prospettico monocentrico ha preso in considerazione pazienti con valori di psa persistentemente elevati e con una prima biopsia random trus - guidata negativa . 
lo studio stato effettuato previa approvazione del protocollo da parte del comitato etico e previo ottenimento da parte di tutti i pazienti del consenso informato per linclusione nel gruppo di studio . 
sono stati reclutati inizialmente in questo studio 180 pazienti consecutivi , che si erano rivolti alla clinica urologica del nostro nosocomio in un periodo compreso tra gennaio 2007 e giugno 2009 . 
let dei pazienti era compresa tra 46 e 78 anni ( media 61 , 2 anni ) e tutti avevano effettuato una prima biopsia prostatica random trus - guidata , risultata negativa per adenocarcinoma o per neoplasia prostatica intraepiteliale di alto grado ( hgpin ) ; tutti presentavano livelli di psa persistentemente elevati ( psa totale 4 ng / ml ) ed edr positiva o negativa . 
i criteri di esclusione per lo studio sono stati : precedenti terapie ormonali con analoghi del luteinizing hormone - releasing hormone radiol med ( 2010 ) 115 : 13141329 table 1 patient characteristics parameters population total psa ( ng / ml ) prostatic volume ( cc ) prostatic cancer familiarity age range ( mean ) psa , prostate specific antigen tabella 1 caratteristiche dei pazienti parametri 9 , 423 , 91 42 , 177 , 47 4678 anni ( 61 , 2 ) popolazione psa totale ( ng / ml ) volume prostatico ( cc ) familiarit per carcinoma prostatico range et ( media ) 9 , 423 , 91 42 , 177 , 47 4678 anni ( 61 , 2 ) psa , antigene prostatico specifico scan . 
all examinations were performed with dedicated sequences for morphological , spectroscopic and dynamic assessments . morphological images of the gland were obtained with t2 - weighted turbo spin - echo ( tse ) sequences in the sagittal , axial and coronal planes with the use of parameters optimised for a better spatial resolution [ repetition time ( tr ) 5 , 190 ms , echo time ( te ) 95 ms , flip angle 150 , average 3 , field of view ( fov ) 256 mm , fov phase 100 , thickness 3 mm , section gap 0 , matrix 512512 , 1317 ( lh - rh ) , terapie chirurgiche o radianti per patologie prostatiche ; casi in cui lesame rm era controindicato . 
i criteri di inclusione sono stati : una prima biopsia prostatica negativa ( nessuna diagnosi istologica di tumore della prostata o lesioni pre - cancerose ) ; livelli di psa totale persistentemente 4 ng / ml . 
le caratteristiche dei pazienti sono descritte nella tabella 1 . tutti i pazienti sono stati sottoposti ad un esame 1h - mrsi e dcemr ( a distanza di almeno 30 giorni dalla prima biopsia )  . 
nei casi in cui mrsi e / o dcemr hanno rilevato sospetti foci tumorali , i campioni orientati su queste aree sono stati associati alla biopsia rando requisiti tecnici e protocollo dimaging studio morfologico , spettroscopico e dinamico - perfusionale tutti gli esami sono stati eseguiti con apparecchiatura rm a 1 , 5 t ( magnetom avanto , siemens medical solutions , erlangen , germania ; gradient strength , 45 mt / m ; slew rate , 346 t / m / s ; rise time , 400 micro / s ; featuring total imaging matrix - tim1 technology ) , dotato di bobina di superficie phased - array ( body matrix , siemens medical solutions ) e bobina endorettale , successivamente distesa con 7090 ml di aria in base alla tolleranza del singolo paziente ( e - coil , medrad , pittsburgh , pa , usa , combined with endo - interface , siemens medical solutions )  . 
nei casi in cui il volume di interesse ( voi ) non riuscisse a ricoprire lintero volume prostatico , come in presenza di marcato aumento del volume ghiandolare , la sequenza stata ripetuta 1318 radiol med ( 2010 ) 115 : 13141329 fig . 
in the cases where the volume of interest ( voi ) failed to cover the entire prostate volume , as in the presence of marked glandular enlargement , the sequence was repeated twice : once for the right and once for the left hemigland . dce - mri was obtained using t1 - weighted gradientecho ( gre ) sequences during the intravenous injection of a contrast bolus of 1.0 mmol / ml of gadobutrol ( gadovist , bayer shering pharma ag , berlin , germany ) ( tr 2.0 ms , te 1.0 ms , flip angle 19 , average 1 , thickness 4 mm , section gap 0 , time resolution 12 sections / 3 s , matrix 256256 , scan time 3.50 min , measurement 80 )  . 
sono stati somministrati 0 , 1 mmol / kg peso corporeo di mezzo di contrasto mediante iniettore ( spectris , medrad ) a 3 , 0 ml / s e seguito dalliniezione di 15 ml di soluzione fisiologica . durante la somministrazione di mdc , sono state ottenute immagini in sottrazione generate da un algoritmo automatico che utilizza i primi 3 secondi della sequenza come baseline per le successive misurazioni . 
come in altri studi [ 18 , 19 ] , per effettuare la comparazione dei dati rm con i dati anatomo - patologici , la zona periferica della prostata stata suddivisa in sestanti in accordo con i seguenti criteri : la base stata definita come il terzo superiore , che si estende dal margine radiol med ( 2010 ) 115 : 13141329 1319 fig . 
a curve 1 in b shows abnormal vascularity patterns on the right side of the tissue volume located between 7 and 8 h roi 1 in a , the arrow indicates the area suspicious for prostate cancer ; curve 2 in b corresponds to the portion contralateral to the suspicious area ( roi 2 in a ) ; curve 3 in b corresponds to the central area ( roi 3 in a ) and curve 4 in b to the reference baseline ( pelvic muscle , roi 4 in a )  . 
the dynamic perfusion study shows marked contrast - enhancement at the level of the nodular lesion ( arrow , roi 1 ) , with typically malignant enhancement pattern as documented by the time - intensity curves , which show early enhancement with downward slope of the curve ( washout , curve 1 )  . 
la curva 1 in b corrisponde allalterazione dei pattern di vascolarizzazione in sede laterale destra nel volume di tessuto compreso tra ore 7 ed ore 8 ( roi 1 in a ) la freccia indica larea sospetta per cp , la curva 2 in b corrisponde alla porzione contro laterale allarea soapetta ( roi 2 in a ) , la curva 3 in b corrisponde alla zona centrale ( roi 3 in a ) e la curva 4 in b alla baseline di riferimento ( muscolo pelvico , roi 4 in a )  . 
lo studio dinamico - perfusionale dimostra spiccato potenziamento post - contrastografico a livello dellalterazione nodulariforme ( freccia , roi 1 ) con andamento tipico di malignit come documentabile dalle curve di elaborazione intensit / tempo , che si caratterizzano per precoce enhancement con tendenza alla caduta della curva ( wash out , curva 1 ) ( tr 2 , 0 ms , te 1 , 0 ms , flip angle 19 , average 1 , thickness 4 mm , section gap 0 , time resolution 12 sections / 3 s , matrice 256256 , scan time 3 , 50 min , measurement 80 )  . 
 analysis of [ 1h ] mrsi and dce - mri data mr images were analysed in consensus by two radiologists with 10 and 5 years of experience , respectively , in urogenital mri . 
as in other studies [ 18 , 19 ] , to correlate mri data with pathology findings , the peripheral zone of the prostate was divided into sextants according to the following criteria : the base was identified as the upper third , which extends from the vesical margin of the prostate to the axial level with the largest transverse diameter ; the mid region was defined as the central third from the axial level to the level of the ejaculatory duct orifices at the verumontanum ; the apex was defined as the remaining inferior portion of the gland . 
the right and left sides of the prostate were separated by the median sagittal plane through the verumontanum . the location of the mrsi and dce - mri voxels used in the combined analysis was overlaid on the sextants defined by mri . 
the absolute values ( ppm ) of cho , cr and citrate cit were calculated for each voxel , as was the value of the cho + cr / cit ratio for both groups of patients . 
voxels were classified as suspicious when the cho + cr / cit ratio was vescicale della prostata al livello assiale con il diametro trasverso maggiore ; la regione mediana , definita come il terzo centrale dal livello assiale con il diametro trasverso maggiore al livello degli orifizi del dotto eiaculatore al veru montanum ; lapice stato definito come la porzione inferiore rimanente della ghiandola . 
le parti destra e sinistra della prostata sono state separate dal piano sagittale mediano passante per il veru montanula localizzazione dei voxel della mrsi e della dcemr usate per lanalisi combinata stata sovrapposta ai sestanti definiti dalla rm . 
per ciascun voxel sono stati calcolati i valori assoluti ( ppm ) di cho , cr e cit ed stato calcolato il valore del rapporto ( cho + cr ) / cit in tutti e due i gruppi di pazienti . i voxels sono stati classificati come sospetti se il rapporto ( cho + cr ) / cit risultava > 0 , 8 [ 20 ] e poi localizzati nella zona periferica in accordo con lo schema precedentemente descritto . 
i voxels con rapporto elevato sovrapposti a zone con segnale iperintenso in sequenze t1 - pesate non sono stati considerati sospetti , ma sono stati riferiti ad artefatti da emorragia post - bioptica [ 21 ]  . 
allesame mrsi , il sospetto di carcinoma prostatico stato posto nel caso in cui venivano 1320 radiol med ( 2010 ) 115 : 13141329 > 0.8 [ 20 ] and were then localised in the peripheral zone according to the described scheme . 
on mrsi , pc was suspected if one or multiple suspicious voxels were identified . postprocessing of dynamic mri took 10 min per patient , and the same radiologists reviewed the subtracted dce - mr images on the basis of maximum and minimum enhancement regions . 
four rois were placed , respectively , on a pelvic reference ( pelvic muscle ) , on an enhancing region ( suspicious for malignancy ) , on the region contralateral to the suspicious enhancing region ( apparently healthy prostate tissue ) and on the central portion ( likely adenoma )  . 
in particular , the pc foci within the peripheral zone ( pz ) were identified based on signal hypointensity in the morphological mri t2 - weighted sequences and greater enhancement values in subtraction images ( qualitative method ) , in accordance with the described sitescheme . 
in cases where multiple enhancing regions were detected , the time - intensity curve of the roi showing the greatest enhancement among those placed in the area was considered for the analysis . after placement of the rois , time - intensity curves [ 22 ] were generated to assess the following parameters : onset time ( ot ) , time between contrast injection and onset of signal enhancement curve , expressed in seconds ( s ) ; time to peak ( ttp ) , time taken by the curve to reach its maximum peak , expressed in seconds ( s ) ; peak enhancement ( pe ) , the highest concentration of contrast material in the roi , expressed in millimoles per kilogram ( mmol / kg )  . 
 tumour vascularity patterns are characterised by marked enhancement relative to the surrounding parenchyma , and this can be objectively demonstrated and semiquantitatively assessed on time - intensity curves that show : early ot in the arterial phase , suggestive of arterial vascularity due to neoangiogenesis ; high pe values ; early ttp and washout , reflected in the steep fall of the curve . the entire gland was studied , and the dynamic images were assessed independently from the morphological t2weighted sequences . 
 il post - processing dello studio rm dinamico stato effettuato in 10 minuti per paziente e gli stessi radiologi hanno valutato le immagini dcemr sottratte sulla base di regioni di potenziamento massimo e minimo . 
quattro roi sono state posizionate rispettivamente : su un muscolo pelvico di riferimento , su una regione di potenziamento post contrastografico ( sospetta di lesione tumorale ) , sulla regione controlaterale opposta alla regione sospetta di potenziamento ( tessuto prostatico apparentemente sano ) e sulla porzione centrale ( verosimilmente adenoma )  . 
in particolare , i focolai di cp allinterno della zona periferica ( zp ) sono stati identificati sulla base di una ipointensit di segnale nelle sequenze morfologiche t2 - pesate e valori di potenziamento pi elevati nelle immagini sottratte ( metodo qualitativo ) , in accordo con lo schema delle localizzazioni gi esposto . 
nei casi in cui sono state identificate pi regioni con potenziamento post - contrastografico , stata presa in considerazione per questo tipo di analisi la curva intensit - tempo della roi con potenziamento pi significativo tra le roi posizionate in quella regione . dopo il posizionamento delle roi sono state ottenute le curve intensit / tempo ( i / t ) [ 22 ] sulle quali sono stati valutati i seguenti parametri : onset - time ( ot ) , tempo che intercorre tra la somministrazione del mdc e linizio della crescita della curva , espresso in secondi ( s ) ; time to peak ( ttp ) , tempo impiegato affinch la curva raggiunga il suo picco massimo , espresso in secondi ( s ) ; peak enhancement ( pe ) ovvero la massima concentrazione del contrasto nella zona dinteresse , espresso in millimoli per chilogrammo ( mmol / kg )  . 
 i pattern di vascolarizzazione del tumore sono caratterizzati da uno spiccato potenziamento rispetto al restante parenchima obiettivamente dimostrabile e semiquantitativamente valutabile sulle curve i / t che presentano : precoce ot in fase arteriosa , indicativo di vascolarizzazione arteriosa da neoangiogenesi ; elevati valori di pe ; precoce ttp e relativo wash - out , rappresentato dalla fase di rapida discesa della curva . stata campionata lintera ghiandola e sono state valuindipendentemente dalle immagini dinamiche tate sequenze morfologiche t2 - pesate . 
all trus scans and biopsies were performed by using an end - fire us transducer and tutte le biopsie prostatiche dello studio , anche le prime biopsie risultate negative , sono state effettuate nel nostro dipartimento da un unico operatore , con esperienza del settore > 10 anni . 
3 schema per indicare i potenziali siti di prelievo bioptico sulla base delle alterazioni morfo - metaboliche e di vascolarizzazione rm . an 18 - gauge needle ( esaote technos mp with a c10 / c5 transducer )  . 
at our centre , biopsies are performed using the standard technique consisting of ten random , laterally directed cores ( two cores from the basal , lateral and paramedial portions ) , two cores from the midgland ( lateral and paramedial ) and one from the apex ( on each side of the gland ) [ 16 ]  . 
in each patient , the biopsy was directed to areas corresponding to those identified on mrsi and dce - mri on the basis of x and z coordinates obtained in the t2 - weighted sequences , as previously described ( fig . 3 ) [ 15 ]  . 
 correlation of mr images with pathology findings and statistical analysis the correspondence of mrsi and dce - mri findings with the pathological examination was determined independently by two readers and subsequently reviewed by a third reader who had not previously analysed the mr images . 
the correspondence was demonstrated on the basis of x , y , and z coordinates obtained on morphological t2 - weighted sequences gauge ( esaote technos mp con trasduttore c10 - 5 )  . 
il volume prostatico stato valutato mediante prolate ellipsoid method . nel nostro istituto le biopsie sono state effettuate con le tecnica standard , 10 campioni random diretti lateralmente ( 2 dalla porzione basale ; laterale e paramediana ) , 2 dalla zona media ( laterale e paramediana ) e 1 dallapice ( su ogni lato della ghiandola ) [ 16 ]  . 
 correlazione delle immagini rm con i risultati anatomo - patologici e analisi statistica il riscontro della corrispondenza tra i risultati della mrsi e dcemr e la valutazione anatomo - patologica stata effettuata in maniera indipendente in tutti i casi da due osservatori , e successivamente rivalutata da un terzo osservatore , che non aveva analizzato precedentemente le immagini rm . 1322 radiol med ( 2010 ) 115 : 13141329 and according to the division into sextants of the peripheral zone of the prostate , as described above ( analysis of mrsi and dce - mri data )  . statistical analysis questa corrispondenza stata effettuata sulla base delle coordinate x , y e z ottenute sulle sequenze morfologiche t2pesate e sulla base della divisione in sestanti della zona periferica della prostata , come descritto nel paragrafo precedente . statistical analysis was performed using the statistical software medcalc software demo for windows , version 9.3 ( mariakerke , belgium )  . 
contingency tables ( 22 ) were used to calculate the sensitivity , specificity , negative predictive value ( npv ) , positive predictive value ( ppv ) and diagnostic accuracy of each method . 
sono state utilizzate tabelle ( 22 ) per calcolare la sensibilit ( sen ) , la specificit ( spec ) , il valore predittivo negativo ( pnv ) , il valore predittivo positivo ( ppv ) e laccuratezza di ciascuna metodica . 
 stato effettuato anche il confronto tra le curve receiver operating characteristics ( roc ) per ciascuna fase dellanalisi . i pazienti sono stati suddivisi in 4 gruppi : gruppo 1 , in cui sia lesame spettroscopico che lesame dinamico sono risultati normali , corrispondente a 80 / 150 casi ( 53 , 33% ) ; gruppo 2 ( mrsi sospetta e dcemr normale ) 12 / 150 casi ( 8% ) ; gruppo 3 ( con mrsi normale e dcemr sospetta ) 10 / 150 casi ( 6 , 67% ) e gruppo 4 ( mrsi e dcemr entrambi sospetti ) 48 / 150 casi ( 32% ) ( tabella 2 )  . al momento della seconda biopsia , stata effettuata diagnosi istologica di adenocarcinoma prostatico in 64 / 150 ( 42 , 6% ) dei casi ( p = 0 , 01 )  . 
in particolare , stato riscontrato un adenocarcinoma prostatico in 4 / 80 casi ( 5% ) in cui sia la mrsi che la dcemr risultavano normali ( gruppo 1 ) , in 11 / 12 casi ( 91 , 5% ) con mrsi sospetta e dcemr normale ( gruppo 2 ) , in 7 / 10 casi ( 70% ) con mrsi normale e dcemr sospetta ( gruppo 3 ) e in 42 / 48 casi ( 87 , 5% ) con mrsi e dcemr entrambe sospette ( gruppo 4 )  . 
la auc risultata pi significativa ( p < 0 , 001 ) nella combinazione delle due metodiche rispetto alle singole metodiche di mrsi e dcemr . radiol med ( 2010 ) 115 : 13141329 1323 fig . 
4a - d in a , the morphological acquisition obtained with a high - resolution t2 - weighted turbo spin - echo sequence shows a focal hypointensity ( arrow ) with a lobular appearance in the lateral portion of the right peripheral zone . 
in c , the perfusion study performed during the intravenous administration of contrast material shows marked contrast enhancement in the region of the nodule [ roi 1 ] , with d typical patterns of malignancy characterised by early downward slope of the curve ( washout ) , as demonstrated by the time - intensity curves . 
4a - d in a nellacquisizione morfologica ottenuta con lutilizzo di sequenza tse t2 pesate ad alta risoluzione apprezzabile ipointensit focale a morfologia lobulariforme ( freccia ) localizzata a livello della porzione laterale dellemi - mantello destro . 
in b spettro dei metaboliti ottenuto con sequenza 1h - mrsi , che dimostra un aumento del metabolismo della colina ( picco ) rispetto agli altri due metaboliti , rappresentati dalla creatina e dal citrato . 
in c lesame perfusionale eseguito durante somministrazione endovena di mdc ha dimostrato spiccato potenziamento post - contrastografico a livello del nodulo ( roi 1 ) che presenta andamento tipico di malignit come documentabile dalle curve di elaborazione intensit / tempo ( d ) caratterizzate da precoce caduta della curva ( wash out )  . 
in particular , prostate adenocarcinoma was identified in 4 / 80 cases ( 5% ) with normal findings on both mrsi and dce - mri ( group 1 ) ; in 11 / 12 cases ( 91.5% ) with suspicious mrsi findings and normal dce - mri ( group 2 ) ; in 7 / 10 cases ( 70% ) with normal mrsi and suspicious dce - mri ( group 3 ) ; and in 42 / 48 cases ( 87.5% ) with suspicious findings on both mrsi and dce - mri ( group 4 )  . 
in all cases with suspicious mrsi and / or dce - mri results and a positive finding at the nella nostra popolazione , dalla valutazione patient by patient , lmrsi ha riportato valori di sensibilit = 82 , 8% , specificit = 91 , 8% , ppv = 88 , 3% , npv = 87 , 8% e accuratezza = 85 , 7% . 
at multivariate analysis , only mrsi ( p = 0.001 ) and combined mrsi and dce - mri ( p = 0.0001 ) were found to be significant and independent predictors of pc at the second biopsy . 
to reduce the false - negative rate , biopsy strategies prostatico non sono stati significativamente correlati ( p > 0 , 05 )  . nellanalisi multivariata solamente la mrsi ( p = 0 , 001 ) e lassociazione mrsi + dcemr ( p = 0 , 0001 ) sono risultate significative e predittori indipendenti per lindividuazione di carcinoma prostatico al momento della seconda biopsia . 
biopsie ripetute in pazienti con persistente alterazione dei livelli sierici di psa mostrano una graduale riduzione di risultati proporzionalmente allaumento del numero di rebiopsie , partendo dal 23% di capacit di individuazione del tumore alla prima serie di prelievi bioptici fino al 17 , 6% , 11 , 7% , 8 , 7% e 0% rispettivamente alla seconda , terza , quarta e quinta serie di prelievi [ 15 ]  . 
sono state proposte strategie bioptiche con un numero aumentato di campioni , anche fino a 25 , per ridurre la percentuale di falsi negativi [ 21 ]  . comunque , la biopsia a saturazione pu essere associata ad aumentata morbilit dei pazienti e la decisione relativa allutilizzo di pi campioni nella diagnosi di pi tumori con caratteristiche di basso rischio rimane controversa [ 24 , 25 ]  . 
 [ 26 ] hanno riportato il 29% di identificazione del tumore con una procedura di biopsia a saturazione in una popolazione di studio di pazienti che hanno effettuato biopsie ripetute . 
il test diagnostico ideale nel work - up iniziale di questo tipo di pazienti dovrebbe essere in grado di identificare i casi in cui i siti prostatici sospetti per cancro siano realmente presenti al fine di garantire una pi alta percentuale di successo delle biopsie [ 21 ]  . 
a the high - resolution morphological t2 - weighted turbo spin - echo sequence shows a nodular focal hypointense signal ( arrow ) in the volume of tissue between 7 and 8 h at a mid / basal level ; b spectroscopic analysis showed low choline levels at the level of the morphological abnormality with moderate enhancement , as documented by c , d time - intensity curves showing borderline trends . 
nellimmagine morfologicatse t2 pesata ad alta risoluzione ( a ) apprezzabile ipointensit di segnale focale a morfologia nodulariforme ( freccia ) localizzata nel volume di tessuto compreso tra ore 7 e 8 a livello mediobasale ; a livello dellalterazione morfologica sono apprezzabili nello studio spettroscopico bassi valori di colina ( b ) con modesto potenziamento a livello dellalterazione morfologica come documentabile dalle curve di elaborazione i / t che presentano andamento di tipo borderline ( c , d )  . 
la biopsia ha posto diagnosi istologica di atypical small acinar proliferation ( asap )  . with an increased number of random biopsy samples up to 25 have been suggested [ 21 ]  . 
however , saturation biopsy may be associated with increased patient morbidity , and the issue of whether obtaining more cores results in the diagnosis more tumours with low - risk characteristics remains controversial [ 24 , 25 ]  . 
the ideal diagnostic test in the initial workup of this type of patient should be able to identify the cases in which the prostate sites suspicious for cancer are reliably identified to ensure studio dimostra che , in pazienti con una prima biopsia prostatica negativa e livelli sierici di psa persistentemente elevati , la combinazione di uno schema bioptico standard con 10 prelievi e con una strategia di sovra - campionamento nei siti selezionati sulla base delle indicazioni della rm , ha determinato percentuali significativamente pi elevate di individuazione del tumore . 
 [ 28 ] hanno proposto lutilizzo prospettico della rm per guidare le biopsie , dimostrando un lieve beneficio con una sensibilit dal 70% all83% e un ppv dal 12% al 53% . 
 [ 13 ] hanno realizzato uno studio per determinare se la rm morfologica combinata con la mrsi possa individuare meglio i foci 1326 radiol med ( 2010 ) 115 : 13141329 a higher rate of success by guiding biopsies [ 21 ]  . 
it shows that in patients with a negative initial prostate biopsy and persistently elevated psa levels , the combination of a standard ten - core biopsy scheme with an oversampling strategy in sites targeted by mri indications significantly increases cancer detection rates . 
 [ 13 ] conducted a study to establish whether morphological mri combined with mrsi could improve detection of cancer foci in 24 patients with previous negative trus - guided biopsy . 
 [ 29 ] reviewed all available databases for prospective studies of patients undergoing combined mri / mrsi and prostate biopsy with negative previous biopsies and persistently elevated serum psa levels . 
 our study was the first to investigate the use of mrsi and dce - mri alone and in combination in this clinical setting ; we also examined the entire prostate volume with two separate acquisitions of the right and left portions of the gland , obtaining complete and accurate images of the entire prostate volume . 
in our study , at the second biopsy , pc foci were detected in 42.6% of cases ( 64 / 150 )  . the suspicion raised by the combined mrsi / dce - mri study was validated by histological examination in 100% of cases . 
in our population , per - patient assessment showed that the combination of mrsi and dce - mri increases sensitivity ( 93.7% ) , specificity ( 90.7% ) , ppv ( 88.2% ) , npv tumorali in 24 pazienti con precedente biopsia trus - guidata negativa . 
le conclusioni di tale studio hanno dimostrato che rm morfologica e mrsi hanno la capacit di mirare la biopsia in questo tipo di pazienti con una sensibilit del 100% , una specificit del 70 , 6% , un ppv del 58 , 3% , un npv del 100% e unaccuratezza del 79 , 2% nellindividuazione del cp . 
 [ 14 ] in una popolazione di 42 casi con biopsie prostatiche negative e valori di psa > 4 ng / ml , hanno riportato valori di sensibilit , specificit , ppv , pnv e accuratezza della mri / mrsi nella individuazione del cp rispettivamente di 73 , 3% , 96 , 3% , 91 , 6% , 86 , 6% e 88% . 
 [ 21 ] hanno ottenuto il 100% di sensibilit , il 51 , 4% di specificit , il 48 , 6% di ppv , il 100% di pnv e il 66 , 7% di accuratezza dalla combinazione delle due tecniche ( mri / mrsi )  . 
 [ 24 ] hanno rivisto tutti i database disponibili per quanto riguarda studi prospettici in cui stata utilizzata la combinazione mri / mrsi e in cui sono state effettuate biopsie prostatiche con precedenti biopsie negative e valori sierici di psa persistentemente elevati . 
le popolazioni di tutti gli studi sono risultate di numero limitato , la pi ampia era di 93 casi ; in questultima esperienza i pazienti sono stati studiati con sequenze morfologiche t2 pesate e sequenze dinamiche , riportando una sensibilit dell83 , 5% [ 7 ]  . la sensibilit della combinazione mri / mrsi rilevata nei vari studi stata del 57%100% , la specificit del 44%96% e laccuratezza del 67%85% . 
 nel nostro studio per la prima volta , sono state investigate , in questo ambito clinico non solo la mrsi , ma anche la dcemr e la combinazione mrsi / dcemr ; inoltre , come descritto precedentemente , abbiamo esaminato lintero volume prostatico con due acquisizioni separate dellemiporzione destra e sinistra , ottenendo un campionamento completo e preciso dellintero volume prostatico . 
in questo studio , al momento della seconda biopsia , il focolaio di cp stato riscontrato nel 42 , 6% dei casi ( 64 / 150 )  . il sospetto riscontrato allesame combinato di mrsi e dcemr , stato validato dallesame istologico nel 100% dei casi . 
nella nostra popolazione , dalla valutazione patient by patient , lassociazione della mrsi con la dcemr aumenta la sensibilit ( 93 , 7% ) , la specificit ( 90 , 7% ) , il ppv ( 88 , 2% ) , il pnv ( 95 , 1% ) e laccuratezza ( 90 , 9% ) nel predire lindividuazione del carcinoma prostatico se paragonata alla sola tecnica mrsi utilizzata singolarmente . 
 , altres , importante sottolineare che tutti i carcinomi della prostata individuati sulla base dei risultati della combinazione mrsi / dcemr hanno mostrato un gleason score6 ( 3 + 3 ) e il 58 , 6% un gleason score 7 ( 4 + 3 )  . 
secondly , all random biopsies were performed by the same surgeon and all following a ten - core trus - guided biopsy scheme , as in previous studies [ 16 ]  . 
in to mrsi , we used a particular , with 0.340.340.34 - cm isotropic voxel and a 0.8 cutoff value for the cho + cr / cit ratio as suspicious for cancer , in accordance with the literature [ 14 , 21 ]  . 
 reference one of the limitations of the technique is detecting cancer foci in the transition zone [ 12 , 29 ] ; matching trus and mri results may also pose limits in biopsy guidance [ 21 ]  . 
on the other hand , difficulties in ensuring accurate spatial matching between trus - guided biopsies and suspicious sites at mri ( mrsi / dce - mri ) have been debated in several studies [ 13 ]  . 
in our analysis , however , in order to compare mr images with pathology findings , the peripheral zone of the prostate was divided into sextants according to stringent criteria [ 18 , 19 ]  . 
assessment of the spatial correlation between mrsi and dcemri findings and the pathological examination was performed by a single observer blinded to the mr images . our choice of method was supported by the 100% correspondence between the histological localisation of the cancer and the suspicious sites at mrsi / dce - mri in patients who proved positive for pc at biopsy . 
however , it is well established that the optimal correspondence between the mri site and the biopsy site is certainly better validated by the correlation at pathology in patients treated with radical prostatectomy [ 13 ]  . il risultati positivi del nostro studio hanno dimostrato il promettente ruolo dellimaging rm nellidentificazione di neoplasie clinicamente significative della zona periferica della prostata . 
pertanto le biopsie guidate dai risultati della rm potrebbero individuare in maniera significativa questi tumori rispetto a schemi standard di biopsia rando la significativit dei risultati di questo studio potrebbe essere dovuta ai criteri utilizzati per disegnare lo studio e per valutare i risultati ottenuti con la combinazione mrsi / dcemr . innanzitutto , questo uno studio prospettico randomizzato su una popolazione ampia e omogenea . 
in secondo luogo , tutte le biopsie random sono state effettuate in maniera omogenea dallo stesso operatore e tutte quante seguendo uno schema di biopsia trus - guidata a 10 campioni , come in studi precedenti [ 16 ]  . 
in particolare , per quanto riguarda la mrsi abbiamo utilizzato un voxel isotropico di 0 , 340 , 340 , 34 cm e il cut - off di 0 , 8 del rapporto ( cho + cr ) / cit come sospetto di tumore , in accordo con i dati in letteratura [ 14 , 21 ]  . 
 [ 14 ] hanno riscontrato una significativa riduzione nei valori di specificit e ppv della mrsi nel ridurre la soglia del rapporto da 0 , 8 a 0 , 75 , e ci sembra dovuto allaumento del numero di falsi positivi ( fp ) con lindagine mrsi . 
 tra i limiti della metodica vi lidentificazione di foci neoplastici a livello della zona di transizione [ 12 , 24 ] ; anche la corrispondenza tra trus e rm pu presentare dei limiti al fine di guidare la biopsia [ 21 ]  . 
daltra parte le difficolt nellottenere lesatta corrispondenza spaziale tra biopsia trus - guidata e sedi sospette alla rm ( mrsi / dcemr ) argomento dibattuto in diversi studi [ 13 ]  . 
nella nostra analisi , comunque , per il confronto tra le immagini rm e i dati anatomo - patologici , la zona periferica della prostata stata divisa in sestanti in relazione a rigidi criteri [ 18 , 19 ]  . 
la valutazione della corrispondenza spaziale tra i risultati della mrsi e della dcemr con la valutazione anatomo - patologica stata effettuata da un unico osservatore che non ha avuto modo di visionare le immagini rm . 
la corrispondenza del 100% tra la localizzazione allesame istologico del tumore e il sito indicato dalla combinazione mrsi / dcemr nei casi con combinazione mrsi / dcemr sospetta , risultata poi positiva per carcinoma prostatico alla biopsia ha supportato la nostra scelta metodologica . 
comunque consolidato che il dato di ottima corrispondenza tra il sito rm e la sede del prelievo bioptico certamente meglio validato dalla correlazione anatomopatologica per quei pazienti sottoposti a prostatectomia radicale [ 13 ]  . conclusions conclusioni mri of the prostate is currently not included in the guidelines for patients with abnormal clinical - laboratory findlo studio della prostata con rm attualmente non rientra nelle linee guida per i pazienti con positivit clinico - laboratoristica 1328 radiol med ( 2010 ) 115 : 13141329 ings ( psa > 4 ng / ml ) who are candidate for trus - guided biopsy . 
this could be a reasonable approach for a group of patients often experiencing significant psychological and physical stress following uncertain diagnoses because of repeated negative random biopsies and persistently abnormal psa values [ 13 ]  . 
a targeted biopsy based on combined mrsi / dce - mri could , in the future , be compared with saturation biopsy with a view to assessing its accuracy , morbidity and cost - effectiveness . 
in this specific case , this would mean establishing the diagnosis with mri ( morphological , preserving the role of trus as a method providing realtime guidance for biopsy , especially in highly suspicious cases . and dynamic ) spectroscopic ( psa > 4 ng / ml ) candidati alla biopsia trus - guidata . 
nella nostra popolazione , la combinazione tra mrsi e dcemr ha mostrato risultati veramente promettenti nellindividuazione di foci neoplastici da sottoporre a biopsia in pazienti con una precedente biopsia trus - guidata negativa . 
questo dovrebbe rappresentare un approccio ragionevole in un gruppo di pazienti che ha spesso importanti stress psicologici e fisici in seguito a diagnosi incerte a causa di ripetute biopsie random negative e valori di psa persistentemente alterati [ 13 ]  . 
una biopsia mirata dallo studio combinato mrsi / dcemr potrebbe essere in futuro comparata con una procedura di biopsia a saturazione al fine di valutare i rispettivi valori di accuratezza , ma anche la morbilit e il rapporto costo - efficacia . 
david2 1dipartimento di radiologia cardiovascolare , 3radiologia demergenza , ospedale san camillo - forlanini , circonvallazione gianicolense , 87 , 00152 roma , italy 2dipartimento di scienze radiologiche , universit di roma sapienza ospedale santandrea , via di grottarossa 1035 , 00189 roma , italy 4dipartimento di scienze radiologiche , universit di roma sapienza polo pontino , via franco faggiana 34 , 04100 latina , italy correspondence to : c.n. 
twenty consecutive patients ( mean age 54.719.9 years ) prospectively underwent abdominal dect to assess the liver using a triphasic protocol consisting of precontrast , arterial - phase and portal - phase acquisitions . 
axial vne images were reconstructed based on the portal data set using a collimation and an increment of 5 mm and were compared with tne images reconstructed with the same parameters . 
sono stati studiati prospettivamente venti pazienti consecutivi ( et media 54 , 719 , 9 anni ) mediante tcde addominale per lo studio del fegato con lacquisizione di un protocollo trifasico comprendente una fase pre - contrastografica , arteriosa e portale . 
i criteri di esclusione erano : allergia al mezzo di contrasto , nefropatia e body mass index ( bmi ) > 35 kg / m2 . lacquisizione portale stata effettuata in modalit dual energy con una modulazione automatica della dose ( care dose 4d )  . 
dal data - set portale sono state ricostruite delle immagini pcv utilizzando una collimazione ed un incremento di 5 mm e sono state comparate con le immagini pcr ricostruite con i medesimi parametri . 
non stata osservata nessuna differenza statisticamente significativa ( p > 0 , 05 ) tra la qualit delle immagini pcr ( 4 , 350 , 58 ) e pcv ( 4 , 000 , 85 )  . 
una qualit diagnostica sufficiente stata osservata in totale nel 95 , 0% ( 19 / 20 ) delle immagini pcv e nel 100% delle radiol med ( 2010 ) 115 : 12581266 1259 conclusions . 
nevertheless , a few technical limitations related to the small field of view of the second detector in patients with a high bmi and heterogeneous iodine subtraction restrict the application of this technique to selected patients only . keywords dual - energy computed tomography liver iodine radiation dose immagini reali . 
nonostante ci , la presenza di alcune limitazioni tecniche correlate al field of view ( fov ) ridotto del secondo detettore nei pazienti con elevato bmi e ad una non omogenea sottrazione dello iodio limitano lapplicabilit della tecnica a pazienti selezionati . 
 parole chiave tomografia computerizzata a doppia energia fegato rimozione iodio dose radiazione introduction introduzione dual - energy computed tomography ( dect ) is based on the simultaneous acquisition of two data sets of the body area under study using different voltage ( 80 kv and 140 kv )  . unlike single - energy ct , where image acquisition is based on attenuation of the radiation beam by anatomical structures having different densities , dect with the use of a highand low - energy radiation beam allows one to distinguish among chemical elements having different absorption spectra based on atomic number and therefore to differentiate among materials with similar density but different atomic composition [ 1 , 2 ]  . 
although the initial studies on de acquisition date back to the 1970s , the technology has only recently been incorporated into clinical practice due to technical obstacles [ 3 , 4 ]  . 
currently , the diagnostic applications of dect include evaluation of hepatic and cardiac iron concentration , differentiation of calcium from iodine and thus optimisation of automated bone - subtraction algorithms in vascular studies , identification of uric acid stones and assessment of tissue distribution of iodine in perfusion studies [ 510 ]  . the ability to differentiate iodine from other materials makes it possible to subtract iodine from contrast - enhanced images to obtain virtual nonenhanced images ( vne )  . acquisition of true nonenhanced images ( tne ) could therefore be avoided , thereby reducing radiation dose to the patient . 
 the purpose of this study was to evaluate the quality and noise of vne and tne images in patients undergoing dect of the liver . la tomografia computerizzata ( tc ) a doppia energia ( tcde ) si basa sullacquisizione contemporanea di due data - set a differente voltaggio ( 80 e 140 kv ) del distretto corporeo in esame . 
a differenza della tc a singola energia , in cui lacquisizione dellimmagine basata sullattenuazione del fascio di radiazioni a seconda della differente densit delle strutture in esame , lutilizzo di due fasci di radiazioni ad alta e bassa energia permette di distinguere elementi chimici che presentano un differente spettro di assorbimento in base al numero atomico , distinguendo quindi materiali con simile densit ma composizione atomica differente [ 1 , 2 ]  . 
gli studi iniziali sullacquisizione de risalgono agli anni settanta , ma a causa di ostacoli tecnici solo recentemente stato possibile integrare tale tecnologia nella pratica clinica [ 3 , 4 ]  . 
attualmente le applicazioni diagnostiche della tcde permettono di valutare laccumulo di ferro epatico e cardiaco , di distinguere il calcio dallo iodio permettendo di ottimizzare gli algoritmi di sottrazione automatica dellosso negli studi vascolari , di riconoscere i calcoli di acido urico e di valutare la distribuzione tissutale dello iodio negli studi perfusionali [ 510 ]  . la possibilit di distinguere lo iodio da altri materiali ne rende inoltre possibile la sottrazione dallimmagine postcontrastografica , ottenendo cos delle immagini pre - contrastografiche virtuali ( pcv )  . 
in tal modo sarebbe possibile evitare lacquisizione dimmagini pre - contrastografiche reali ( pcr ) riducendo quindi la dose di radiazioni somministrata al paziente ; tale aspetto riveste una particolare importanza nei protocolli di studio multifasici del fegato [ 11 , 12 ] , specialmente in corso di follow - up e nei soggetti giovani . 
 1260 materials and methods patient population radiol med ( 2010 ) 115 : 12581266 lo scopo del presente lavoro di valutare la qualit ed il rumore delle immagini pcv e pcr in pazienti sottoposti a tcde del fegato . between february and march 2009 , 20 consecutive patients underwent abdominal dect of the liver . 
the study was conducted in accordance with the principles of the declaration of helsinki , and all patients gave their written informed consent . dect protocol the study was performed using a dect scanner ( somatom definition , siemens medical solutions , forcheim , germany )  . 
le indicazioni allesame riguardavano prevalentemente lo studio di lesioni focali epatiche o il follow - up di pazienti con lesioni secondarie . sono stati utilizzati i seguenti criteri di esclusione : allergia al mezzo di contrasto ( mdc ) iodato , nefropatia ( creatinina > 120 mmol / l ) e bmi > 35 kg / m2 . 
tutti i soggetti esaminati hanno fornito il consenso informato scritto . protocollo tcde lo studio stato effettuato utilizzando una tcde ( somatom definition , siemens medical solutions , forcheim , germania )  . 
inizialmente , stata acquisita una scansione pre - contrastografica delladdome utilizzando la seguente configurazioni di detettori : collimazione 640 , 6 mm , pitch 1 , 2 , voltaggio del tubo 120 kvp , 240 mas come valore di riferimento e modulazione automatica della dose . 
conseguentemente , stato somministrato tramite un iniettore a doppia testa del mezzo di contrasto iodato ( iomeron 400 , 400 mgi / ml , bracco , milano ) ad un flusso di 3 , 5 ml / s , il tutto seguito da 50 ml di soluzione salina . 
stata utilizzata una dose di 0 , 625 gi / kg [ 13 , 14 ] con un limite inferiore di 100 ml per i pazienti di peso minore di 60 kg ed un limite superiore di 130 ml per pazienti di peso maggiore di 85 kg . 
firstly , an abdominal nonenhanced scan was taken with the following detector configurations : collimation 640.6 mm , pitch 1.2 , tube voltage 120 kvp , reference value 240 mas and automatic dose modulation . 
subsequently , iodinated contrast material ( iomeron 400 , 400 mgi / ml , bracco , milan , italy ) was administered via a dual - head injector at a flow rate of 3.5 ml / s , followed by 50 ml of saline solution . 
the bolus tracking technique was used to monitor the arrival of contrast material in a region of interest ( roi ) placed at the level of the abdominal aorta just below the diaphrag the scan started 18 s after the attenuation threshold of 100 hu was reached to obtain a late arterial phase , and a second de acquisition was performed 70 s after contrast administration to obtain portal - phase images . arterial acquisition was performed using a single tube with a voltage of 120 kvp , 200 mas , pitch 1.2 and a detector collimation of 640.6 mportal acquisition was obtained using the de mode with tube a working with a peak voltage of 140 kvp and a reference value of 96 mas and tube b with a peak voltage of 80 kvp and a reference value of 404 mas . 
the 5 - mm vne and tne axial images were sent to a dedicated workstation ( leonardo , siemens medical solutions ) and analysed separately during different reporting sessions by two experienced abdominal radiologists . 
the quality of liver vne and tne images was evaluated on a five - point scale : grade 1 nonevaluable ; grade 2 poor quality ; grade 3 sufficient quality ; grade 4 good quality ; grade 5 excellent quality . 
a score 3 passaggio del mdc stata utilizzata la tecnica del bolus tracking con la regione di interesse ( roi ) posizionata a livello dellaorta addominale subito al di sotto della cupola diaframmatica . 
la scansione iniziata 18 secondi dopo che stato raggiunto un valore limite di attenuazione di 100 hu al fine di ottenere una fase arteriosa tardiva ed stata effettuata una seconda acquisizione in modalit dual energy a 70 s dallinizio della somministrazione del mdc per ottenere una fase portale . 
lacquisizione arteriosa stata effettuata in modalit singolo tubo con un voltaggio di 120 kvp , 200 mas , pitch 1 , 2 ed una collimazione dei detettori di 640 , 6 m lacquisizione portale stata effettuata in modalit dual energy con il tubo a operante ad una intensit di 140 kvp ed un valore di riferimento di 96 mas , e dal tubo b ad una intensit di 80 kvp ed un valore di riferimento di 404 mas ; stata utilizzata per entrambi i tubi una collimazione dei detettori di 141 , 2 mm ed un pitch 0 , 55 mas . 
le immagini pcv e pcr assiali di 5 mm sono state inviate ad una workstation dedicata ( leonardo , siemens medical solutions ) ed analizzate separatamente in differenti sedute di refertazione da due esperti radiologi addominali . 
la qualit delle immagini pcv e pcr del fegato stata valutata mediante una una scala graduata in 5 punti : grado 1 , immagine non valutabile ; grado 2 , scarsa qualit dellimmagine ; grado 3 , immagine di qualit sufficiente ; grado 4 , immagine di buona qualit ; grado 5 , immagine di eccellente qualit . 
1a - c post - processing dellacquisizione dual energy ; a immagine portale acquisita in modalit de , b immagine di fusione dei data sets a 80 e 140 kv con mappa colorimetrica della distribuzione tissutale di iodio , c immagine pre - contrastografica virtuale dopo sottrazione dello iodio . 
il rumore nelle immagini pcr e pcv stato calcolato come la deviazione standard del grasso retroperitoneale misurata con una roi di 1 cm2 . analisi statistiche scarsa le variabili quantitative della qualit delle immagini sono state espresse come mediadeviazione standard ( ds ) e le variabili categoriche come frequenze e percentuali . 
la concordanza inter - osservatore per la qualit delle immagini stata calcolata mediante la kappa ( k ) di cohen concordanza ; 0 , 210 , 40 , discreta ; ( < 0 , 20 , 0 , 410 , 60 , moderata ; 0 , 610 , 80 , buona ; 0 , 811 , 00 , eccellente )  . 
il test t di student a doppia coda per dati appaiati stato utilizzato al fine di rilevare eventuali differenze tra la qualit delle immagini ed il rumore dei due gruppi in esame . 
the noise in the tne and vne images was calculated as the standard deviation for retroperitoneal fat as measured with an roi of 1 cm2 . tutti gli esami di questa serie sono risultati tecnicamente adeguati . 
 una valutazione completa degli organi addominali ( fegato , pancreas , milza e reni ) stata possibile in 11 pazienti . in 9 pazienti acquisizione il rene di sinistra e la milza non radiol med ( 2010 ) 115 : 12581266 statistical analyses quantitative variables of image quality were expressed as means standard deviation ( sd ) and categorical variables as frequencies and percentages . 
all statistical analyses were performed with the spss statistical software package ( version 14.0 , statistical package for the social sciences spss , chicago , il , usa )  . results all examinations were found to be technically adequate . vne images could be generated in all cases . 
in nine patients , the left kidney and spleen were not entirely included in the scan , and in four patients , the liver could not be studied in its entirety . 
the vne group contained no examinations considered nonevaluable ( grade 1 ) and only 5% of sono stati completamente compresi nella scansione ; in 4 pazienti non stato possibile studiare interamente il fegato . 
 1263 qualit delle immagini e rumore non stata osservata nessuna differenza statisticamente significativa ( p > 0 , 05 ) tra la qualit delle immagini pcr ( 4 , 350 , 58 ) e pcv ( 4 , 000 , 85 )  . 
quindi una qualit desame accettabile per un utilizzo clinico stata osservata in totale nel 100% delle immagini pcr e nel 95 , 0% ( 19 / 20 ) delle immagini pcv . 
nel caso delle immagini virtuali non sono stati osservati esami non valutabili ( grado 1 ) , mentre solo nel 5% dei casi stata osservata la presenza di una qualit scarsa dell immagine ; tale risultato stato riscontrato in particolare nei pazienti con un bmi ai limiti superiori dei criteri di inclusione dello studio . i nostri risultati sulla qualit delle immagini concordano quindi con quelli ottenuti da altri gruppi di ricerca per quanto riguarda lutilizzo delle immagini pcv nella valutazione delle lesioni renali e nellanalisi degli endoleak aortici [ 1517 ]  . 
 la rumorosit delle immagini risultata pi elevata nellacquisizione pcr rispetto a quella virtuale , sebbene tale differenza non sia risultata statisticamente significativa ; la minor rumorosit delle immagini virtuali da ascriversi allutilizzo di filtri addizionali durante il post - processing che determinano una riduzione del rumore di fondo [ 15 ]  . 
qualit media e rumore delle immagini pre - contrasto virtuali ( pcv ) e reali ( pcr ) qualit poor - quality images , in particular , in patients with a bmi close to the upper limits of our inclusion criteria . 
our results with regard to image quality therefore agree with those reported by other research groups who investigated the use of tne images in the evaluation of kidney lesions and in the analysis of aortic endoleaks [ 1517 ]  . 
 image noise was higher in tne as opposed to vne acquisitions , although this difference was not statistically significant ; the lower noise of virtual images can be attributed to the use of additional filters in postprocessing , which lead to lower background noise [ 15 ]  . 
in other previous reports , this difference was significant , and we believe that our result can be attributed to the small number of patients examined . in almost 50% of patients , dect acquisition did not , however , provide coverage of all abdominal organs , because for geometrical reasons , the second tube has an fov of only 26 cm , i.e. 
in particular , when centring the scan on the liver , coverage of the spleen and the left kidney appears problematic ; additionally , acquisition of the left lobe may be incomplete in patients with enlarged liver . finally , as shown in our study , the de technique can generate vne images of the liver of a quality comparable with that of true images and with less noise . 
si apprezza unerronea sottrazione del calcio della parete aortica ( freccia )  . addominali , tale risultato dovuto al fatto che per motivi geometrici il secondo tubo presenta un fov di soli 26 cm che risultano insufficienti a coprire lintero addome se non in pazienti con un bmi basso . 
in particolare , effettuando un centraggio mirato allo studio del fegato risulta problematica la copertura della milza e del rene di sinistra ; inoltre nei pazienti con un fegato di volume aumentato pu risultare incompleta anche lacquisizione del lobo di sinistra . in conclusione , come dimostrato dal nostro studio , con la tecnica de possibile ottenere delle immagini pcv del fegato di qualit sovrapponibile a quella delle immagini reali e con una minor rumorosit . 
in tal modo verrebbe meno la necessit di acquisire una fase pre - contrastografica e sarebbe quindi possibile ottenere una significativa riduzione della dose somministrata al paziente , compresa , come riportato da precedenti lavori , tra il 35 , 05% ed il 61% [ 1517 ] a seconda del protocollo utilizzato . 
 di pitfall diagnostici in assenza di immagini reali . i limiti maggiori dello studio sono rappresentati dal basso numero di pazienti e dallutilizzo di una differente collimazione , dovuto a limitazioni tecniche , dellacquisizione de ( 141 , 2 mm ) rispetto a quella pre - contrastografica ( 640 , 6 ) che potrebbe aver influito sulla valutazione della qualit dell immagine e del rumore . 
despite a few technical limitations in patients with a high bmi related to the smaller fov of the second detector and to heterogeneous iodine subtraction , this approach would make acquisition of nonenhanced phases unnecessary , thereby significantly reducing radiation dose to the patient . 
rotondo dipartimento di internistica clinica e sperimentale magrassi - lanzara , sezione di radiodiagnostica e radioterapia , seconda universit degli studi di napoli , p.zza miraglia 2 , 80138 napoli , italy correspondence to : g . 
the procedure was successful in all patients . follow - up imaging was carried out at 12 h , 24 h , 15 days , 3 months , 6 months and 12 months . 
 parole chiave endometriosi aspirazione alcolizzazione introduction introduzione endometriosis is a chronic and complex pathological condition that arises from the anomalous presence of implants of lendometriosi rappresenta una condizione patologica cronica e complessa che prende origine dalla presenza radiol med ( 2010 ) 115 : 13301339 1331 functional endometrial glands and stroma outside of the uterus in anatomical sites such as ovaries , tubes , peritoneum , vagina , intestines and ureters [ 13 ]  . 
the condition affects 10% of fertile european women , usually aged between 25 and 29 years , and can have considerable psychological and socioeconomic implications , since it is the cause of 30%40% of infertility and is characterised by a high rate of recurrence [ 4 ]  . 
although aggressive surgery is considered the treatment of choice for endometrioma and its recurrence , patients young age and desire for pregnancy call for a conservative procedure that is adequately supported by preand postoperative hormone treatment . 
this requires finding therapeutic techniques alternative to surgery . deferring pregnancy , medical treatment with hormone therapy and ultrasound ( us ) - guided aspiration of the endometrial cysts have , to date , made up the main alternative treatment options [ 712 ]  . 
recent studies have demonstrated the high rate of shortand long - term recurrence associated with these approaches , which runs counter to their noninvasiveness and simplicity [ 13 ]  . 
the aim of our study was to demonstrate that ethanol sclerotherapy , after usor laparoscopy - guided aspiration [ 8 , 14 ] can be a valid treatment option for endometriomas . materials and methods between 2006 and 2008 , 50 patients with a diagnosis of ovarian endometrial cysts were enrolled and underwent usguided aspiration and ethanol sclerotherapy of a total of 54 endometriomas . 
twenty patients ( 40% ) had already undergone surgery for other endometrial cysts ; five ( 10% ) had undergone pelvic surgery for conditions other than endometriosis ; three ( 6% ) were treated during the first trimester of pregnancy . 
the inclusion criteria were endometrial cysts between 2 and 5 cm , refusal to undergo surgical treatment and contraindications to laparoscopy or laparotomy ( adhesions , pregnancy , high anaesthesia risk )  . all selected patients underwent aspiration and ethanol sclerotherapy . 
in total , 54 cysts were aspirated and treated with ethanol sclerotherapy 40 with the transabdominal approach ( virgo intacta , cranially displaced ovaries ) and 14 with the transvaginal approach . 
we identified , located and characterised all endometrial cysts with a us study done with suprapubic , endovaginal or endorectal insonation ( with adequate preparation ) in virgo intacta patients , three of whom had already undergone anomala di impianti di ghiandole e stroma endometriali funzionali esternamente alla cavit uterina , in siti anatomici quali ovaie , tube , peritoneo , vagina , intestino , uretere [ 13 ]  . 
lendometriosi colpisce circa il 10% delle donne europee nel periodo fertile , solitamente nella fascia di et compresa tra i 2529 anni e determina notevoli implicazioni di ordine psicologico e socio - economico , essendo la causa del 30%40% dei casi di infertilit femminile e presentando un alto tasso di recidive [ 4 ]  . 
sebbene la chirurgia demolitiva sia considerata il trattamento di elezione dellendometrioma e delle sue recidive , la giovane et delle pazienti ed il loro desiderio di gravidanza fanno propendere per un intervento conservativo , adeguatamente supportato da terapia ormonale pre e post - operatoria . 
 lattesa di una gravidanza , lapproccio medico con terapia ormonale e laspirazione sotto guida ecografica delle cisti endometriosiche hanno rappresentato , sino al giorno doggi , le principali alternative terapeutiche [ 712 ]  . i pi recenti studi hanno dimostrato lalto tasso di recidive a breve e lungo termine connesso a tali pratiche , in contrapposizione allassenza di invasivit ed alla semplicit di esecuzione [ 13 ]  . 
lobiettivo del nostro studio dimostrare che lalcolizzazione con etanolo , dopo opportuna aspirazione sotto guida ecografica o laparoscopica [ 8 , 14 ] , pu rappresentare una valida soluzione terapeutica nel trattamento terapeutico delle cisti endometriosiche . 
 materiali e metodi nel periodo compreso tra il 2006 e il 2008 , 50 pazienti consecutive con diagnosi di cisti endometriosica a localizzazione ovarica sono state arruolate e sottoposte ad aspirazione ed alcolizzazione ecoguidata di 54 cisti endometriosiche . 
venti pazienti ( 40% ) erano state gi sottoposte ad intervento chirurgico per il trattamento di altre cisti endometriosiche ; 5 pazienti ( 10% ) erano state sottoposte a intervento chirurgico agli organi pelvici per patologie diverse dallendometriosi ; 3 donne ( 6% ) sono state trattate durante il primo trimestre di gravidanza . 
i criteri di inclusione utilizzati per la selezione delle pazienti sono stati : cisti endometriosiche di dimensioni comprese tra 2 e 5 cm , rifiuto del trattamento chirurgico , controindicazioni a laparoscopia o a laparotomia ( aderenze , gravidanze , rischio anestesiologico elevato )  . la procedura di aspirazione e alcolizzazione stata realizzata in tutte le pazienti selezionate . 
sono state aspirate 1332 radiol med ( 2010 ) 115 : 13301339 confirmed pelvic magnetic resonance ( mr ) imaging in another centre , which the us diagnosis of ovarian endometriosis , and who therefore came to our centre for the interventional procedure [ 15 ]  . 
the main us features for the characterisation of endometrial cysts are the following : hypoanechoic masses with fine , low - level internal echoes located prevalently in the inferior portion ; hypoechoic masses with diffuse , fine , low - level internal multilocular hypoanechoic masses with internal septaechoes ; tions ; multilocular hypoechoic masses with internal septations ; in rare cases , anechoic masses with fine diffuse internal echoes ( early - phase endometrioma )  . presumably malignant lesions were excluded with the support of colour doppler , power doppler , high - flow or contrast - enhanced us [ 16 ] , as well as extemporaneous cytological examination of the cystic aspirate . 
two carcinogenic antigens ( ca ) were assayed [ 16 ] : ca 125 and ca 19.9 ( the former as a nonspecific marker for endometriosis and the latter to rule out the presence of ovarian malignancy )  . 
all patients gave written informed consent and underwent the procedure after consultation with the radiologist . the procedure was performed in the presence of anaesthesiological assistance but without the use of a local anaesthetic : the possible passage of ethanol into the pelvic cavity can cause sharp pain that requires the prompt administration of analgesics , particularly in pregnant women ( paracetamol by mouth , intramuscular ketorolac )  . 
in cases of transvaginal approach , vaginal disinfection was performed with iodine lavage ( at the time of the procedure , vaginal disinfection is carried out with iodine swabs )  . prior to the procedure , patients underwent us study with a toshiba ssa 250a system with 3.75 mhz convex transducers and 6 mhz transducers with biopsy needle guides . the following single - use materials required for the procedure were positioned on the service trolley : sterile gel , sterile transducer sheaths , needle - guide attachments and a set comprising tubular connector for syringes with conetipped catheter , phial of sterile ethanol , saline solution and 18to 20 - gauge needles with echogenic tip . 
 in cases of us - guided transvaginal access , the patient was placed in the gynaecological position , whereas in cases of us - guided or us - assisted transabdominal access , the patient was positioned supine with a full urinary bladder . the cystic mass was reached either by transvaginal or transabdominal approach in the latter case with the puncture of the anterior and posterior wall of the bladder . 
tutte le cisti endometriosiche sono state da noi identificate , localizzate e caratterizzate con esame ecografico condotto con insonazione sovrapubica , endovaginale o endorettale ( previa preparazione ) in pazienti virgo , tre delle quali erano state gi sottoposte ad esame pelvico con risonanza magnetica ( rm ) in altra sede , che aveva confermato la diagnosi ecografica di endometriosi ovarica e giungevano quindi alla nostra osservazione per lesecuzione della procedura interventistica [ 15 ]  . 
le principali caratteristiche ecografiche per la individuazione delle cisti endometriosiche sono state : formazioni ipoanecogene con echi fini e fittamente stipati , localizzati prevalentemente nella parte inferiore ; formazioni ipoecogene con echi fini e fittamente stipati in tutta la formazione ; formazioni ipoanecogene , con trabecolature e multiloculazioni ; zioni ; formazioni ipoecogene , con trabecolature e multiloculain rari casi , formazioni anecogene con echi diffusi fini non stipati ( cisti endometriosica in fase iniziale )  . sono state escluse lesioni presumibilmente maligne attraverso il supporto del color doppler , del power doppler , di tecniche hiflow , eventualmente ecografia con mezzo di contrasto [ 16 ] e con esame citologico estemporaneo del contenuto endocistico aspirato . 
sono stati dosati due antigeni [ 16 ] : antigene carboidratico ca - 125 e ca - 19.9 ( il primo come marcatore aspecifico dellendometriosi ; il secondo per escludere la presenza di una patologia maligna a carico dellovaio )  . 
 la procedura viene realizzata in presenza di assistenza anestesiologica , ma senza lutilizzo di anestetico locale : leventuale passaggio di etanolo nello scavo pelvico pu provocare vivo dolore che necessita talora della pronta somministrazione di analgesici , specie nelle donne gravide ( paracetamolo per os , ketorolac im )  . 
in caso di accesso transvaginale , stata praticata disinfezione del canale vaginale con lavanda allo iodio ( al momento della procedura viene effettuata la disinfezione del canale vaginale con tamponi iodati )  . le pazienti sono state sottoposte previamente ad esame radiol med ( 2010 ) 115 : 13301339 1333 dense , the contents need to be diluted with lukewarm saline solution and then aspirated . 
us follow - up was performed at 1224 h to evaluate possible early bleeding and then at 15 days and 3 , 6 and 12 months to detect any late complications and / or recurrence . results us follow - up was performed in all patients at 1224 h . there were no signs of bloody effusion , either at the level of the anatomical site treated with ethanol or within the surrounding tissue . 
at 15 days from the procedure , us study showed similar findings to the study done at 1224 h in terms of postprocedure complications , although the appearance and organisation of a finely hypoechoic tissue was appreciable replacing the original endometrial cyst . 
after 36 months , us follow - up showed in all patients the absence of local recurrence and disease in the remaining anatomical sites that could be explored with us . 
in three of the four unsuccessful cases , ethanol sclerotherapy was repeated . the repeated procedures were successful in all cases , showing complete regression of ovarian recurrences at shortand long - term follow - up . 
at 24 months from aspiration and ethanol sclerotherapy , ten women had become pregnant , and they all successfully brought the pregnancy to term ( table 1 )  . discussion although surgical resection of endometrioma still remains the reference standard , it should be noted that the invasive approach to endometrial cysts is a radical operation that is not without risks associated with the procedure itself , which given its invasiveness can damage part of the healthy adnexa containing the oocytes [ 57 ]  . 
the surgical approach , ecografico con apparecchiatura ultrasonografica toshiba ssa 250a con trasduttori convex da 3 , 75 mhz e trasduttori microconvex da 6 mhz con dispositivo di allineamento per le biopsie . 
sul carrello servitore , con telo sterile per il materiale monouso , sono stati posizionati per la procedura interventistica gel sterile , guaine sterili per le sonde , dispositivi per ecoguida , set costituito da raccordo tubulare per siringhe con cono catetere , fiale di etanolo sterile , soluzione fisiologica , aghi di grosso calibro con punta ecoriflettente 1820 g . in caso di accesso transvaginale ecoguidato il decubito adottato dalle pazienti stato in posizione ginecologica ; in caso di accesso transaddominale ecoguidato o eco - assistito , le pazienti sono state posizionate in decubito supino ed a vescica piena . 
si penetra nella formazione e si aspira il contenuto . in caso di contenuto denso , necessario diluirlo con soluzione fisiologica tiepida , aspirare e ripetere la procedura fino alla completa eliminazione del materiale ematico . 
sono stati effettuati controlli ecografici a 1224 h , per valutare eventuali sanguinamenti precoci e successivamente a 15 giorni , 3 , 6 e 12 mesi per la diagnosi di complicanze tardive e / o recidive . risultati in tutte le pazienti sono stati effettuati controlli ecografici a 1224 h che non hanno dimostrato segni di stravaso ematico , n a livello del sito anatomico alcolizzato con etanolo n allinterno dei tessuti circostanti . 
nei tre giorni successivi alla procedura , in cinque donne stata riscontrata la presenza di un piccolo versamento nel douglas ; in una paziente stato riscontrato un ascesso intracistico . dopo 15 giorni dalla manovra terapeutica la valutazione ecografica ha determinato analoghi risultati rispetto al controllo ecografico a 1224 h in merito alle complicanze post - alcolizzazione , sebbene abbia apprezzato la comparsa e lorganizzazione di un tessuto finemente ipoecogeno in sostituzione alla cisti endometriosica originaria . 
dopo 36 mesi , in tutte le pazienti , il monitoraggio ecografico ha dimostrato lassenza di recidiva locale e di patologia nei restanti siti anatomici eco - esplorabili evidenziando , inoltre , la scomparsa dellimmagine ipoecogena intraovarica precedentemente descritta nel controllo ecografico a 15 giorni , esito table 1 : database of 50 patients diagnosed with endometrial cyst ( ec ) through ultrasonography and subsequently treated with ultrasound - guided aspiration ( us - guided aspiration ) and ethanol sclerotherapy ( es ) location pregnant pain previous ec surgery complications within 3 days recurrence within 1 year radiol med ( 2010 ) 115 : 13301339 23 l ; 31 r 3 retreated with aspiration / es ; 1 surgically treated ( 5.5 cm ) moderate fluid in the rectouterine pouch ( 5 patients ) ; intracystic abscess ( 1 patient ) 1334 no . 
postsurgical adhesions can also be a frequent cause of pelvic pain and can lead to costiveness or intestinal occlusion / subocclusion arising from obstruction of the small bowel loops . the literature reports a recurrence rate of endometrial cysts after conservative laparotomy or laparoscopy that varies between 0.5% and 52% , and important studies report a recurrence rate with the need of repeated surgery in 23% of cases [ 5 , 6 ]  . 
in addition , the possibility of refusal to undergo surgery by a large number of young patients is neither negligible nor infrequent due to the significant psychological pressure created by the disease , which can of course lead to infertility . 
pharmacological treatment that acts on the hormonal front , and percutaneous puncture with aspiration of the endometrial cyst , have over the years shown a high rate of recurrence ( around 50% ) , whereas the approach with laser and radiofrequency ablation has proved to be excessively aggressive , with damage to the healthy adnexal parenchyma [ 712 ]  . we propose sclerotherapy with 95 ethanol following aspiration of the endometrial cyst contents under us guidance as a valid alternative for treating endometriomas [ 8 , 14 ]  . 
la ripetizione dellalcolizzazione con etanolo stata conseguita con successo in tutti i casi precedentemente falliti , dimostrando nel follow - up a breve e lungo termine una regressione completa della recidiva ovarica . 
a 24 mesi dal trattamento terapeutico con agoaspirazione della cisti endometriosica ed alcolizzazione con etanolo , 10 donne sono divenute gravide e tutte hanno portato a termine con successo la gravidanza ( tabella 1 )  . 
 discussione chirurgica lescissione sebbene dellendometrioma rimanga al giorno doggi lapproccio terapeutico gold standard , occorre precisare che lapproccio invasivo sulla cisti endometriosica , per quanto rappresenti un intervento radicale , non scevro da rischi connessi alla procedura stessa radiol med ( 2010 ) 115 : 13301339 1335 fig . 
1a donna di 29 anni , alla xv settimana di gravidanza ; cavit uterina ( freccia sottile ) ; vescica ( punta di freccia ) ; cisti endometriosica ( freccia spessa ) ; b ago ecoriflettente visualizzato in tutto il suo tragitto ( attraversamento completo della vescica e della parete cistica ) ( frecce lunghe )  . we used two different approaches transabdominal and transvaginal [ 17 , 18 ]  . 
in the us - assisted approach [ 17 ] , che , a causa della sua invasivit , pu danneggiare parte dellannesso sano che contiene ovociti [ 57 ]  . 
lapproccio chirurgico , sia esso in laparoscopia che in laparotomia , pu indurre la formazione di sinechie aderenziali che possono a loro volta essere causa di infertilit , ostacolando il fisiologico rilascio di ovociti da parte delle ovaie ed ostacolando la perviet al lume delle tube di falloppio . 
le aderenze post - chirurgiche rappresentano , peraltro , una causa frequente di dolore pelvico e possono indurre stipsi o stadi di occlusione / subocclusione intestinale per lostruzione di anse dellintestino tenue . la letteratura moderna riporta un tasso di recidiva di cisti endometriosiche dopo interventi di chirurgia laparotomica o laparoscopica conservativa dellendometriosi variabili tra lo 0 , 5% ed il 52% ed importanti studi riferiscono circa il 23% di recidive con necessit di reintervento [ 5 , 6 ]  . inoltre , tuttaltro che infrequente e trascurabile leventualit di rifiuto allintervento chirurgico da parte di un gran numero di giovani pazienti , a causa del notevole coinvolgimento psicologico sotteso alla patologia che , come ben noto , pu indurre infertilit . 
nellapproccio ecoassistito [ 17 ] , attraverso lesecuzione di opportune scansioni ultrasonografiche , viene visualizzata la corretta ubicazione spaziale della formazione cistica ed introdotto a tale livello un ago di grosso calibro con punta eco - riflettente che , dopo aver aspirato il contenuto cistico , introduce la composizione di etanolo terapeutica . 
e , f aspetto della cisti dopo aspirazione e alcolizzazione definitiva . us scans are done to visualise the correct position of the cystic mass into which a large - diameter needle with an echogenic tip was inserted and through which the cyst contents were aspirated and the ethanol introduced . 
the correct placement of the needle with respect to the us transducer is fundamental in that only by following the course of the echogenic tip along the entire needle track can the laceration of adjacent vascular and nerve structures be avoided . the transvaginal approach [ 18 , 19 ] involves the use of a dedicated us transducer with a needle guide ( us - guided procedure ) , which allows the certainty of visualising the needle throughout the procedure . 
lastly , unlike the transabdominal approach , the transvaginal approach is characterised by the possible formation of synechiae , which can obstruct oocyte passage and uterine tube patency . quanto , solo seguendo il decorso della sua punta eco - riflettente lungo tutto il tragitto di penetrazione , viene evitata la lacerazione delle strutture vascolari e nervose viciniori . 
la modalit transvaginale [ 18 , 19 ] prevede lutilizzo di una sonda ecografica dedicata sulla quale viene montato un supporto dotato di porta - ago ( procedura eco - guidata ) , consentendo la certezza di visualizzazione durante la manovra terapeutica . 
infine , a differenza che nellapproccio transaddominale , la modalit di approccio transvaginale si caratterizza per la possibile formazione di sinechie aderenziali che possono ostacolare la progressione degli ovociti e la perviet tubarica . lagoaspirazione , sia eco - assistita che eco - guidata , rappresenta di per s una procedura semplice , poco radiol med ( 2010 ) 115 : 13301339 1337 fig . 
whether us - assisted or us - guided , it is in itself a simple and inexpensive procedure that can be performed as a day - hospital procedure and has virtually no associated significant complications ( moderate and transient pain , rapidly reabsorbed haematomas )  . 
the patient presented low - grade late - afternoon fever ( 37.5c ) that progressed in the space of a week into fever with earlyafternoon and late - afternoon peaks ( 38.038.5 ) , with pain at the treatment site . 
la donna presentava febbricola serotina ( 37 , 5c ) con evoluzione , dopo circa una settimana , in febbre con picchi pomeridiano - serotini ( 3838 , 5c ) con sintomatologia algica gravativa in sede del trattamento . 
dopo ripetuti lavaggi stato iniettato in cavit antibiotico a largo spettro . il trattamento con etanolo al 10% per 10 minuti realizzerebbe il suo meccanismo terapeutico grazie alla capacit di indurre fenomeni di sclerosi a carico delle strutture microvascolari , bloccando linsorgenza di fenomeni neoangiogenetici [ 20 ] e preservando il tessuto ovarico ai fini della follicologenesi . 
the possibility of choosing between a transabdominal and a transvaginal approach , between an us - guided and us - assisted approach , allows treatment to be personalised with a low lalcolizzazione con etanolo 95 previa aspirazione delle cisti endometriosiche rappresenta una valida alternativa terapeutica allintervento chirurgico . 
la possibilit di scegliere tra un approccio transaddominale e uno transvaginale , tra una procedura eco - guidata o eco - assistita consente di realizzare un intervento personalizzato con 1338 radiol med ( 2010 ) 115 : 13301339 fig . 
4 grafico che mostra la riduzione del tasso di recidiva in caso di come aspirazione / alcolizzazione , riportato dagli studi di messalli et al . [ 14 ] , hiesh et al . 
 [ 8 ] e dal nostro studio , rispetto alla semplice aspirazione [ 21 , 22 ] o alla sola alcolizzazione [ 23 , 24 ]  . pz , numero di pazienti ; rec , numero di pazienti con recidiva ; ns , nostro studio rate of procedure - related complications in the short and long terthe technique is simple if performed by expert operators and overcomes the main disadvantages and possible complications associated with surgery . 
recurrences , which are associated more with the natural history of the disease rather than the interventional procedure used , can be newly treated with the same procedure , thus avoiding especially in young women invasive and aggressive surgery basso tasso di complicanze ( legate alla metodica ) a breve e a lungo termine . 
la metodica , di semplice esecuzione se eseguita da operatori esperti , consente di superare i principali svantaggi , le possibili complicanze legate allintervento chirurgico nonch i suoi costi e permette una completa e rapida risoluzione della patologia . 
simonetti dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , universit di tor vergata , viale oxford 81 , 00133 rome , italy correspondence to : c . 
in the 115 venous grafts , mdct showed a sensitivity , specificity and accuracy of 100% in evaluating occluded grafts and a sensitivity of 94.4% , specificity of 98.4% and accuracy of 96.9% in evaluating significant stenoses . 
sono stati sottoposti a studio con tc 64 strati 78 pazienti ( 45 maschi , 33 femmine ; et media 59 anni ) per un totale di 213 bypass ( 115 innesti venosi e 98 arteriosi )  . 
i 212 bypass presi in esame dei rimanenti 77 soggetti ( 98 , 7% ) , erano costituiti da 115 ( 54% ) innesti venosi e 97 ( 46% ) innesti arteriosi . 
nei 115 by - pass venosi , la tc ha mostrato una sensibilit , una specificit ed una accuratezza diagnostica del 100% nella valutazione dei bypass occlusi e una sensibilit del 94 , 4% , una specificit del 98 , 4% ed unaccuratezza diagnostica del 96 , 9% nella valutazione delle stenosi significative . 
come dimostrato dai risultati ottenuti , la correttezza delle informazioni fornite dalla tc si avvicina 1168 radiol med ( 2010 ) 115 : 11671178 keywords coronary artery bypass grafting multislice computed tomography noninvasive coronary angiography coronary ct a quelle della cc consentendo una completa valutazione del circolo chirurgico e nativo e risultando completamente esaustivo nellescludere o confermare la presenza di patologia vasale nel follow - up post - operatorio . parole chiave bypass aorto - coronarici tcms coronarografia virtuale tc coronarico introduction introduzione coronary artery bypass grafting ( cabg ) is one of the most common methods of treating coronary artery disease ( cad ) in symptomatic individuals [ 1 ]  . 
in patients with multivessel disease , cabg is the treatment of choice and is associated with an improvement in quality of life and an increase in survival [ 2 , 3 ]  . 
the merit of 16 - slice mdct systems is that they provide high accuracy in identifying vascular stenosis and distinguishing between patency and occlusion in cabg [ 912 ]  . 
a significant improvement in image quality has been achieved with the introduction of 64 - slice scanners , which , thanks to the acquisition of the entire cardiac volume in 810 s , have made possible a more accurate evaluation of cabg and the native coronary arteries in surgical patients . the aim of this study was to evaluate the accuracy , sensitivity and specificity of 64 - slice mdct in assessing occlusions and stenosis of arterial and venous bypasses and disease progression in the native vessels distal to the grafting site , and to compare the results with those of cca . la rivascolarizzazione chirurgica miocardica mediante confezionamento di bypass coronarici ( coronary artery bypass grafting , cabg ) uno dei pi comuni metodi di trattamento della patologia coronarica nei soggetti sintomatici [ 1 ]  . 
nei pazienti con malattia multivasale , essa rappresenta il trattamento delezione ed associata ad un miglioramento della qualit di vita ed ad un aumento della sopravvivenza [ 2 , 3 ]  . 
tuttavia la storia naturale dei cabg prevede una percentuale di perviet a 10 anni del 60% per linnesto venoso e del 90% per quello arterioso [ 4 ]  . langiografia coronarica convenzionale ( acc ) considerata il gold standard nella valutazione dello shunt . 
i limiti intrinseci della tecnica sono rappresentati dal fatto che rimane una procedura invasiva , con percentuali di complicanze maggiori nell1 , 7% dei casi ed un tasso di mortalit dello 0 , 11% [ 57 ]  . 
la tomografia computerizzata multidetettore ( tcmd ) costituisce una ormai convalidata alternativa alla coronarografia , in quanto metodica non invasiva , nella valutazione della perviet dei cabg [ 8 ]  . 
il merito delle generazioni di tcmd a 16 strati quello di aver consentito unelevata accuratezza nellindividuazione delle stenosi vasali , nonch nella distinzione tra perviet e occlusione del cabg [ 912 ]  . 
laccuratezza diagnostica nella valutazione dellanastomosi e della progressione di malattia del circolo nativo distale risulta essere , infatti , sensibilmente minore rispetto a quella ottenuta con il corpo del bypass . 
un significativo miglioramento della qualit dimmagine avvenuto con lintroduzione dei nuovi scanner a 64 strati che , grazie allacquisizione dellintero volume cardiaco in 810 secondi , hanno reso possibile una valutazione pi accurata del cabg e delle arterie coronarie native nei pazienti sottoposti a tale trattamento chirurgico . lo scopo di questo studio di valutare laccuratezza diagnostica , la sensibilit e la specificit della tcmd a 64 strati nella valutazione contemporanea delle occlusioni e delle stenosi di bypass arteriosi e venosi e delleventuale radiol med ( 2010 ) 115 : 11671178 materials and methods patients progressione di malattia a carico dei vasi nativi distali allanastomosi chirurgica , rapportando i risultati ottenuti con i reperti coronarografici . 1169 our study included 78 patients ( 45 men , 33 women ) with a mean age 59 ( range15 ) years for a total of 213 bypass grafts ( 115 venous and 98 arterial )  . 
those with unstable angina , cardiac arrhythmias and contraindications to administration of contrast agents [ creatininaemia > 2.0 mg / dl ( 177 mol / l ) ] were excluded . 
to reduce cardiac motion artefacts and obtain images of optimal diagnostic quality , the patients with a baseline heart rate ( hr ) > 70 beats per minute ( bpm ) were given premedication with 50100 mg of beta - blockers ( atenolol ) by mouth 6090 min prior to the examination , with close monitoring of arterial pressure ( ap ) and hr . 
all patients provided informed consent after a clear explanation of the benefits and potential risks . scan protocol all patients underwent ct angiography with a 64 - slice mdct scanner ( lightspeed vct , general electric medical systems , usa )  . 
a preliminary baseline scan was acquired to precisely define the volume to be included in the acquisition and to calculate the coronary artery calcium score ( smartscore protocol )  . 
the main scan parameters in the precontrast phase were the following : beam collimation 82.5 mm , slice thickness 2.5 mm , table feed 1 cm every four acquisition of 2.5 mm , gantry rotation speed 0.35 s , tube voltage 120 kv , tube current 300 ma , fov 25 cm , acquisition volume extending from the carina to the diaphragmatic surface of the heart , scan direction craniocaudal . 
an automatic injector ( stellant , medrad , pittsburgh , pa , usa ) was used for the intravenous administration of 80 ml of nonionic iodinated contrast agent ( ultravist 370 schering ag , berlin , germany ) , followed by an infusion of 40 ml of saline solution , both at an injection speed of 5 ml / s . 
the bolustracking technique was used to synchronise arrival of contrast agent in the coronary arteries with the beginning of acquisition . scan parameters in the contrast phase were the following : beam collimation 640.625 mm , slice thickness 0.625 mm , reconstruction increment 0.625 mm , table feed 2.9 mm / rotation , gantry rotation speed 0.35 s , tube voltage 120 kv , tube current 400800 ma roentgen modulation , fov 25 cm , acquisition volume 1220 cm according to materiali e metodi pazienti sono stati inclusi nello studio 78 pazienti ( 45 maschi , 33 femmine ; et media 5915 anni ) per un totale di 213 bypass ( 115 innesti venosi e 98 arteriosi )  . 
sono stati reclutati soggetti in lista dattesa per essere sottoposti a acc , escludendo quelli con angina instabile , aritmia cardiaca , controindicazioni alla somministrazione di agenti contrastografici ( creatininemia > 2 , 0 mg / dl [ 177 mol / l ] )  . 
con lintento di ridurre gli artefatti da movimento cardiaco ed ottenere cos la massima qualit diagnostica , i pazienti con una frequenza cardiaca ( fc ) basale > 70 battiti per minuto ( bpm ) sono stati pre - medicati con 50100 mg di - bloccante ( atenololo ) per os , assunto circa 6090 minuti prima dellesame , sotto stretto monitoraggio della pressione arteriosa ( pa ) e della fc . 
lo studio stato concordato con i cardiologi ed ha ricevuto lapprovazione del comitato etico locale ; i pazienti hanno fornito il proprio consenso informato allesame dopo chiara spiegazione dei benefici e potenziali rischi . protocollo di scansione tutti i pazienti sono stati sottoposti a studio angio - tc coronarico mediante tcmd a 64 strati ( lightspeed vct , general electric medical systems , usa )  . 
una preliminare scansione basale senza mezzo di contrasto ha permesso di definire con precisione il volume da includere nellacquisizione e di calcolare il calcium score coronarico ( protocollo smartscore )  . 
i principali parametri di scansione nella fase pre - contrastografica sono stati : collimazione del fascio 82 , 5 mm , spessore di strato 2 , 5 mm , traslazione del lettino di 1 cm ogni 4 acquisizioni da 2 , 5 mm , velocit di rotazione del tubo radiogeno 0 , 35 s , voltaggio del tubo 120 kv , intensit del fascio di radiazioni 300 ma , campo di vista ( fov ) 25 cm , volume di acquisizione esteso dalla carena alla superficie diaframmatica del cuore , direzione di scansione cranio - caudale . 
attraverso un iniettore automatico ( stellant , medrad , pittsburgh , usa ) , sono stati somministrati per via endovenosa 80 ml di mezzo di contrasto organo iodato non - ionico ( ultravist 370 schering ag , berlino , germania ) , seguiti dallinfusione di 40 ml di soluzione fisiologica , entrambi ad un flusso di 5 ml / s . 
per sincronizzare larrivo del contrasto nelle arterie coronarie con linizio dellacquisizione stata utilizzata la tecnica del bolus track . i parametri di scansione nella fase contrastografica sono stati : collimazione del fascio 640 , 625 mm , spessore di strato 0 , 625 mm , incremento di ricostruzione 0 , 625 mm , 1170 radiol med ( 2010 ) 115 : 11671178 the presence or otherwise of internal mammary artery grafts , scan direction craniocaudal . 
the acquisition volume in the presence of internal mammary artery grafts should include the origin of the arterial branch up to the diaphragm , whereas in cases of only venous bypass grafts , a smaller volume can be acquired , extending from the aortic anastomosis of the most cranial bypass to the diaphragmatic surface of the heart [ 13 ]  . image reconstruction with retrospective gating was performed with the use of three fixed time windows set at 70% , 75% and 80% of the r - r interval , corresponding to the mid - to - end diastolic phase . 
in the presence of motion artefacts , due to an increase or sudden change in hr during acquisition , end systolic windows were used ( from 40% to 65% of the r - r interval )  . data analysis acquisition of raw data was followed by image evaluation and reconstruction at a workstation ( advantage work station 4.1 , general electric medical system , milwaukee , wi , usa ) with dedicated cardiovascular software ( card iq )  . 
all data were visualised and analysed using a number of reconstruction techniques : ( a ) axial scans , ( b ) multiplanar reformations ( mpr ) , ( c ) maximum intensity projections ( mip ) , ( d ) curved multiplanar reconstructions and ( e ) three - dimensional volume rendering ( 3d - vr )  . 
the images were independently evaluated by a radiologist and a cardiologist , each with at least 3 years of experience in coronary artery imaging , and were compared double - blind with the findings of the cca . 
in two cases of disagreement , consensus was reached following a joint evaluation of the two examinations . both the bypass grafts ( arterial and venous ) and the native vessels distal to the surgical anastomoses were evaluated in the framework of a 15 - segment anatomical subdivision of the coronary arteries [ 7 ]  . 
after having evaluated the presence or otherwise of calcifications in each coronary segment , the analysis then regarded the presence of significant stenoses ( 50% ) , nonsignificant stenoses ( < 50% ) and total occlusions . 
these values were calculated separately for venous grafts , arterial grafts and coronary segments considered . conventional coronary angiography cca was performed with a philips flat - panel system ( medical philips system , the netherlands ) using multiple velocit di avanzamento del lettino 2 , 9 mm / rotazione , velocit di rotazione del tubo radiogeno 0 , 35 s , voltaggio del tubo 120 kv , intensit del fascio di radiazioni compresa tra 400 e 800 ma roengten modulation , fov 25 cm , volume di acquisizione compreso tra 12 e 20 cm a seconda della presenza o meno di bypass arteriosi in mammaria interna , direzione di scansione cranio - caudale . 
il volume di acquisizione in presenza di bypass arteriosi in mammaria interna deve includere lorigine del suddetto ramo arterioso sino al diaframma , mentre nel caso di bypass esclusivamente venosi pu essere acquisito un volume corporeo inferiore , esteso dallanastomosi aortica del bypass pi craniale sino alla superficie diaframmatica del cuore [ 13 ]  . la ricostruzione delle immagini , attraverso sincronizzazione retrospettiva , stata eseguita con lutilizzo di tre finestre temporali fissate al 70% , al 75% e all80% del ciclo cardiaco , periodo compreso tra due onde consecutive r - r del tracciato elettrocardiografico ( ecg ) , corrispondenti alla fase meso - telediastolica . 
nel caso di artefatti da movimento , dovuti ad un aumento o ad una modificazione improvvisa della frequenza cardiaca durante lacquisizione , sono state utilizzate finestre di ricostruzione telesistoliche ( dal 40% al 65% del ciclo r - r )  . analisi dei dati allacquisizione dei dati grezzi ha fatto seguito la valutazione e la ricostruzione delle immagini mediante una workstation ( advantage work station 4.1 , general electric medical system , milwaukee , wisconsin , usa ) con software dedicato allo studio cardiovascolare ( card iq )  . 
le immagini sono state analizzate , in maniera indipendente , da un radiologo ed un cardiologo , ciascuno con esperienza di almeno 3 anni nellimaging coronarico e rapportate in doppio cieco ai risultati della acc . 
 sono stati esaminati sia i cabg ( arteriosi e venosi ) che il circolo coronarico nativo a valle delle anastomosi chirurgiche , tenendo conto della suddivisione anatomica delle coronarie in 15 segmenti [ 7 ]  . 
dopo aver valutato la presenza o meno di calcificazioni in ciascun segmento coronarico in esame , si passati a documentare leventuale presenza di stenosi significative ( 50% ) , non significative ( < 50% ) e delle occlusioni totali . 
 stata successivamente calcolata la sensibilit , la specificit e laccuratezza diagnostica della tcmd nella quantificazione delle occlusioni e delle stenosi significative , in corrispondenza dei graft e del circolo nativo distale allanastomosi chirurgica . 
hr measured during mdct acquisition was around 634 bp of the 212 bypass grafts , 115 ( 54% ) were venous and 97 ( 46% ) were arterial fashioned from the left ( lima ) and right ( rima ) internal mammary artery . 
 venous grafts of the 115 venous grafts , 25 ( 22% ) were anastomosed to the left anterior descending coronary artery ( lad ) , 43 ( 37% ) to the left circumflex artery ( lcx ) and 47 ( 41% ) to the right coronary artery ( rca )  . 
in one case , the mdct examination overestimated the severity of stenosis by attributing the classification of occlusion to a preocclusive stenosis of the proximal anastomosis ( false positive )  . in light of these findings , the sensitivity of mdct in our series was 100% , specificity 100% and accuracy 100% in the identification of occlusions . 
 arterial grafts of the 97 arterial grafts , 84 ( 86.6% ) were anastomosed with the lad , 12 with the lad and the first diagonal branch ( 12.4% ) and one with the lad and lcx ( 1% )  . sono stati calcolati separatamente per i bypass venosi , arteriosi e per i segmenti coronarici considerati . coronarografia convenzionale lesame coronarografico convenzionale stato effettuato mediante un apparecchio flat panel philips ( medical philips system , olanda ) usando multiple proiezioni . 
le stenosi sono state valutate come percentuale del diametro di riferimento determinato in due proiezioni ortogonali utilizzando la media dei due campioni come valore finale . un valore 50% ha indicato una stenosi significativa . risultati dei 78 pazienti arruolati per eseguire la tc , 1 di essi ( 1 , 3% ) stato escluso per linsorgenza di un episodio aritmico durante lacquisizione dellesame . 
i restanti 77 soggetti ( 98 , 7% ) hanno effettuato lesame senza presentare complicanze e successivamente sono stati sottoposti ad esame acc . la frequenza cardiaca durante lacquisizione tc si attestata intorno ai 634 bpdei 212 cabg rimanenti presi in esame , 115 ( 54% ) erano costituiti da innesti venosi e 97 ( 46% ) da innesti arteriosi , confezionati utilizzando larteria mammaria interna sinistra ( amis ) e destra ( amid )  . 
 bypass venosi dei 115 bypass venosi , 25 ( 22% ) erano anastomizzati alla discendente anteriore sinistra ( da ) , 43 ( 37% ) allarteria circonflessa ( cx ) e 47 ( 41% ) allarteria coronaria destra ( cdx )  . 
per quanto riguarda invece lidentificazione delle stenosi , ne sono state correttamente identificate 31 su 34 ( 91 , 1% ) ( fig . 2 ) ; sono state invece sottostimate 2 stenosi ( 6% ) , localizzate in prossimit della anastomosi distale per la presenza di estese calcificazioni del circolo coronarico nativo ( falsi negativi )  . 
alla luce di questi risultati , nella nostra casistica la tcmd ha mostrato una sensibilit del 100% , una specificit del 100% ed una accuratezza diagnostica del 100% nella identificazione delle occlusioni . 
in riferimento invece alle stenosi occorse su bypass , la tcmd ha presentato rispettivamente una sensibilit del 94 , 4% , una specificit del 98 , 4% ed unaccuratezza diagnostica del 96 , 9% . 
in one case ( 1% ) , cca demonstrated an occlusion at the distal anastomosis that was not visualised at mdct due to beam hardening artefacts caused by a metal clip ( false negative )  . 
therefore , with regard to arterial graft occlusions , the sensitivity was 83.3% , specificity 100% and accuracy 98.9% , bypass arteriosi dei 97 bypass arteriosi , 84 ( 86 , 6% ) sono stati anastomizzati con la da , 12 con la da e il ramo diagonale ( 12 , 4% ) ed 1 con la da e la cx ( 1% )  . 
in 1 caso ( 1% ) , la acc ha messo in evidenza unocclusione a livello dellanastomosi distale non evidenziata alla tc per la presenza di artefatti da indurimento del fascio da clip metallica ( falso negativo )  . 
le ricostruzioni mpr curved 2d ( b , c ) e vr ( d ) confermano lassenza di significative riduzioni di calibro dei vasi esaminati ( vero negativo )  . 1174 radiol med ( 2010 ) 115 : 11671178 fig . 
the evaluation included a total of 226 coronary segments ( 213 + 13 sequential ) , of which 20 ( 8.8% ) were considered of poor diagnostic quality due to the presence of motion artefacts and vessel wall calcifications . 
in the remaining four cases ( 2.2% ) , mdct classified as significant , stenoses that were < 50% at cca ( false positives )  . with regard to significant stenoses , 39 of 42 ( 92.8% ) were correctly identified at mdct . 
in one case ( 2.4% ) , mdct classified an lad stenosis as an occlusion that instead was subocclusive at cca ( false positive ) ; this was due to cardiac motion artefacts . 
given the economic costs and the greater risk compared with noninvasive procedures , it would appear desirable to reserve cca only for patients with an elevated risk of disease in the grafts or native vessels distal to the surgical anastomoses . 
a number of noninvasive imaging techniques can be used in the followup of patients with cabg , especially in those , as stated above , where the risk of disease in the grafts or native vessels is low to intermediate . 
quindi , considerando i bypass arteriosi occlusi , la sensibilit stata dell83 , 3% , la specificit del 100% e laccuratezza diagnostica del 98 , 9% , mentre nelle stenosi dei bypass arteriosi , la sensibilit stata del 100% , la specificit del 97 , 7% e laccuratezza diagnostica del 98% . arterie coronarie native tutti i segmenti coronarici nativi distali allanastomosi chirurgica visualizzati con la acc sono stati confrontati con i corrispondenti segmenti esaminati alla tc . 
la valutazione ha compreso in tutto 226 segmenti coronarici ( 213 + 13 sequenziali ) , di cui 20 ( 8 , 8% ) considerati di scarsa qualit diagnostica alla tc per la presenza di artefatti da movimento e di calcificazioni delle pareti vasali . 
in questo gruppo di pazienti la acc ha identificato 184 segmenti coronarici ( 81 , 4% ) esenti da stenosi significative , e 42 segmenti ( 18 , 6% ) sede di stenosi significative . 
per quanto riguarda le stenosi significative , 39 su 42 ( 92 , 8% ) sono state correttamente identificate alla tc , 2 ( 4 , 8% ) sono state sottostimate ( riduzione del lume vasale < 50% ) rispetto a quanto documentato alla acc ( falsi negativi )  . 
in 1 caso ( 2 , 4% ) , la tcmd ha definito come occlusione una stenosi della da che risultata subocclusiva alla acc ( falso positivo ) a causa degli artefatti da movimento cardiaco . 
nella valutazione della progressione di malattia , quindi , la sensibilit stata del 95 , 4% , la specificit del 97 , 3% e laccuratezza diagnostica del 97% . discussione la acc tuttoggi considerata il gold standard per la valutazione dei cabg [ 14 , 15 ] , nonostante la indiscutibile invasivit della procedura e la necessit di alcuni giorni di ospedalizzazione i cui costi non sono indifferenti per il servizio sanitario nazionale ( ssn )  . 
considerando laspetto economico ed i rischi maggiori per il paziente rispetto ad indagini non invasive sarebbe corretto riservare lindagine angiografica solo a pazienti con rischio elevato di patologia dello shunt o del circolo nativo post - anastomosi . 
ad oggi alcune tecniche di imaging non invasive possono essere impiegate nel follow - up dei pazienti con shunt coronarici in particolare , come gi affermato sopra , in quel gruppo di pazienti dove il rischio di malattia coronarica o dello shunt e bassa - intermedia . 
la angiografia con rm ( angio - rm ) si e dimostrata tecnica estremamente valida nella valutazione della perviet dei bypass con valori di sensibilit pari al 95 , 2% e specificit pari al 96 , 8% [ 16 ]  . 
ciononostante questa tecnica attualmente 1176 radiol med ( 2010 ) 115 : 11671178 addition , mr can be extremely dependent on the optimal cooperation of the patient , and the technique requires longer and more elaborate acquisition and postprocessing times . a large number of studies done with mdct for evaluating cabg have shown that 16 - slice mdct systems make it possible to correctly analyse arterial and venous bypass grafts [ 1719 ]  . 
despite the increased performance of 16 - slice mdct scanners over the older systems in terms of temporal and spatial resolution , evaluating native vessels in cabg patients remains a significant diagnostic problem [ 20 , 21 ]  . 
the new generations of 64 - slice mdct offer increased spatial and temporal resolution and allow the entire cardiac volume to be acquired in less than 9 s with an isotropic voxel resolution of 0.4 mm3 [ 2226 ]  . therefore , high - resolution images can be obtained with optimal timing of the contrast agent both in the entire length of the grafts and in the native coronary circulation distal to the anastomosis . 
 the aim of our study was to determine the accuracy of 64 - slice mdct and to test its potential in evaluating the patency of cabg and in the progression of cad in the native coronary arteries . 
mdct systems with 64 detectors have unquestionable advantages over their predecessors in terms of acquisition speed ( 610 s ) , which enables the cardiac volume to be acquired more rapidly and therefore with a marked reduction in motion artefacts due to respiration and hr variability in the initial and final phase of the acquisition . 
this shows that the examination is more feasible than the study performed with 16slice mdct , which is affected by a drastic restriction in the number of nonassessable patients and coronary segments . 
in addition , the increase in acquisition speed offers the advantage of enabling acquisition in a selective phase of arterial enhancement , thus increasing the contrast resolution in relation to the adjacent structures and avoiding visualisation of overlying venous structures . in particular , this is an unquestionable advantage in evaluating small - diameter vessels , such as those distal to the anastomoses , as it improves their visualisation and the reliability in identifying stenoses . our findings confirm that the technique is highly reliable in evaluating venous and arterial bypass grafts , both at the site of the proximal and distal anastomoses , with sensitivity , specificity and accuracy values close to those obtained with cca . 
it should be noted that similar results limitata da una bassa risoluzione spaziale , e da artefatti generati dalle clips metalliche , che rendono difficoltosa la valutazione dei bypass di piccolo calibro come quelli confezionati tra mammaria interna sinistra e da distale . 
inoltre lesame rm appare estremamente dipendente dalla ottimale collaborazione del paziente e peraltro richiede tempi di acquisizione e post - processing pi lunghi ed elaborati . un gran numero di studi effettuati con tcmd per la valutazione dei cabg , ha dimostrato che la tc a 16 strati permette una corretta analisi dei bypass arteriosi e venosi [ 1719 ]  . 
nonostante le aumentate performance della tcmd a 16 strati in termini di risoluzione temporale e spaziale rispetto agli scanner di vecchia generazione , la valutazione dei vasi nativi nei pazienti sottoposti a cabg resta ancora un importante problema diagnostico [ 20 , 21 ]  . 
le nuove generazioni di tcmd a 64 strati offrono unaumentata risoluzione spaziale e temporale e permettono di acquisire lintero volume cardiaco in meno di 9 secondi con una risoluzione di voxel isotropico di 0 , 4 mm3 [ 2226 ]  . 
ci consente di poter ottenere immagini ad elevata risoluzione e con un ottimale timing del mdc sia degli shunt dalla loro origine che del circolo coronarico nativo distale alla anastomosi . 
 lo scopo del nostro studio stato quello di determinare laccuratezza diagnostica della tcmd a 64 strati e di testarne le sue potenzialit nella valutazione di perviet dei cabg e della progressione di malattia nelle arterie coronarie native . 
le generazioni di tc a 64detettori sono indubbiamente portatrici di importanti vantaggi rispetto alle generazioni precedenti , quali la velocit di acquisizione ( 610 s ) , consentendo di acquisire pi rapidamente il volume , riducendo sensibilmente lincidenza di artefatti da respiro e di artefatti dovuti alla variabilit della frequenza cardiaca nella fase iniziale e finale dellacquisizione . 
un solo paziente ( 1 , 3% ) stato escluso per aritmia insorta durante lacquisizione , mentre solo due shunt venosi ( 1 , 7% ) sono stati giudicati non valutabili . 
inoltre lincremento della velocit di acquisizione offre il vantaggio di poter acquisire lo studio in una selettiva fase di enhancement arterioso , incrementando la risoluzione di contrasto in rapporto alle strutture adiacenti ed evitando nello stesso tempo la sovrapposizione delle strutture venose . 
in particolare nella valutazione di vasi di piccolo calibro come quelli distali alle anastomosi ci costituisce un indubbio vantaggio e migliora la loro visualizzazione e laffidabilit nellindividuare stenosi . i nostri risultati confermano come lindagine sia estremamente affidabile nella valutazione del bypass venoso e arterioso , sia in sede di anastomosi prossimale , sia in sede di anastomosi distale , con valori di sensibilit , specificit e accuratezza diagnostica prossimi a quelli ottenuti con lesame angiografico . 
da sottolineare come risultati simili radiol med ( 2010 ) 115 : 11671178 1177 can be obtained with 16 - slice scanners , as reported by several studies in the literature [ 812 ]  . 
the advantage of using a 64 - slice system , however , is not only limited to an increase in sensitivity , specificity and accuracy , but also includes a marked broadening of the patient base and a significant reduction in the number of nonassessable segments due to motion artefacts caused by respiration or arrhythmias . 
it should also be noted that in the study of arterial grafts , the entire length of the internal mammary artery is evaluated , from its origin to the distal anastomosis , in contrast to the procedure with 16 - slice scanners . the relatively low sensitivity ( 83.3% ) obtained in identifying occlusions in arterial grafts can be explained by the low prevalence of occlusions in our patient population . 
in fact , only five patients out of 97 were found to have occlusions at cca . a word needs to be said with regard to the native coronary arteries distal to the surgical anastomosis . 
these are small - diameter vessels in which the cad , and as a consequence calcification , is more advanced than found in the coronary arteries of patients who have not undergone surgical revascularisation . 
data obtained could be confirmed with the organisation of multicentre trials and enrolment of a greater number of patients . siano ottenibili anche con apparecchiature a 16 detettori , come riportato da differenti esperienze in letteratura [ 812 ]  . 
il vantaggio di impiegare unapparecchiatura a 64 detettori non si limita al solo incremento della sensibilit , specificit e accuratezza diagnostica , quanto nellampliare sensibilmente il gruppo di pazienti investigabili e nel ridurre in maniera significativa i segmenti scartati sia per la presenza di artefatti da respiro sia per irregolarit del ritmo . 
 inoltre da sottolineare come nello studio degli shunt arteriosi larteria mammaria interna venga valutata nella sua interezza a partire dallorigine fino allanastomosi distale , a differenza di quanto avveniva con tomografi a 16 detettori . 
la relativa bassa sensibilit ( 83 , 3% ) ottenuta nellidentificare le occlusioni nei bypass arteriosi spiegabile con la bassa prevalenza di occlusioni nel nostro gruppo di pazienti , infatti solo 5 di essi sul gruppo totale di 97 sono risultati occlusi allesame coronarografico . una considerazione a parte merita il circolo nativo distale alle anastomosi chirurgiche . 
si tratta di shunt di vasi di piccolo calibro nei quali la malattia aterosclerotica , e di conseguenza le calcificazioni , sono pi avanzate rispetto a quanto documentabile nelle coronarie di pazienti non sottoposti a rivascolarizzazione chirurgica . 
come dimostrato dai risultati ottenuti nel nostro gruppo di pazienti , la correttezza delle informazioni fornite dalla tcmd si avvicina a quelle fornite dallacc nella valutazione della progressione della malattia . 
pertanto riteniamo che valori di sensibilit , specificit e di accuratezza diagnostica ( 95 , 4% , 97 , 3% e 97% ) , come quelli ottenuti nel nostro gruppo su coronarie native distali allanastomosi , consentano realmente una completa valutazione del circolo chirurgico e nativo nel paziente sottoposto a bypass . 
lesame risulta essere completamente affidabile nellescludere o confermare la presenza di patologia vasale nei follow - up post - operatori . il limite attuale dello studio costituito dallesiguit della popolazione presa in esame . 
mammographic lesion type , lesion size , breast imaging reporting and data system ( birads ) category , number of specimens per lesion and presence of atypia were retrospectively analysed . 
cancer at surgery was more frequent among cases of isolated microcalcifications ( p = 0.645 ) , cases with high radiological suspicion ( p = 0.040 ) and those with riassunto obiettivo . 
identificare i parametri che consentano di distinguere nellambito del variegato gruppo di lesioni b3 diagnosticate tramite vacuum assisted breast biopsy ( vabb ) , lesioni che per il loro ridotto rischio di malignit possano essere indirizzate al follow - up piuttosto che allintervento cos da contenere il numero di procedure chirurgiche non necessarie . 
nella serie consecutiva di 608 pazienti con alterazioni mammografiche , non palpabili , non evidenziabili con ecografia e con vario grado di sospetto avviate al vabb , sono stati inclusi nello studio i 102 casi con diagnosi vabb di lesione b3 . 
laspetto radiologico pi frequente delle b3 rappresentato da microcalcificazioni isolate ( 82 , 3% ) , il diametro risultato inferiore a 10 mm ( 80 , 4% ) , il livello di sospetto radiologico stato lieve ( 64 , 7% ) e si sono prelevati pi di 11 frustoli / procedura ( 94 , 1% )  . 
on the basis of our experience , the presence or absence of atypia in our series proved to be the reliable criterion to prompt or avoid surgery in cases with a vab finding of b3 lesion . 
 parole chiave neoplasia mammaria biopsia mammaria vab proliferazione atipica lesioni b3 introduction introduzione the growing diffusion of core biopsy ( cb ) in the study of the female breast is accompanied by an increasingly frequent detection of borderline microhistological findings ( b3 lesions = lesions of uncertain malignant potential ) [ 1 , 2 ]  . 
the b3 category includes extremely heterogeneous lesions in terms of both pathological and prognostic features , all having a common denominator , namely , an increased risk of breast cancer [ 36 ]  . 
many authors agree that a microhistological finding of b3 lesion should prompt surgical excision aimed at obtaining the most reliable histological confirmation on the remaining breast tissue [ 711 ]  . 
such an overcautious approach could , however , lead to an excess of unnecessary surgical procedures , given that the positive predictive value ( ppv ) of malignancy for b3 lesions is in the order of 30% [ 1215 ]  . 
in fact , in the presence of cells with atypia [ atypical ductal hyperplasia ( adh ) or lobular carcinoma in situ ( lcis ) ] , ppv rises to 50%60% , whereas it falls to 20% in lesions without atypia ( papillary lesions , phyllodes tumour , radial scar , mucocele - like lesions ) [ 1521 ]  . lesions , columnar - cell to verify whether b3 lesions without atypia may be associated with a low ppv for malignancy and call into question the use of surgery in these selected cases , we examined a consecutive series of b3 findings diagnosed over a period of 5 years by stereotactic vacuum - assisted core biopsy ( vab )  . la crescente diffusione di prelievi con ago grosso ( core biopsy , cb ) nello studio della mammella femminile si accompagna al sempre pi frequente riscontro di reperti microistologici borderline ( lesioni b3 = lesioni di incerto potenziale maligno ) [ 1 , 2 ]  . 
la categoria b3 composta da lesioni estremamente eterogenee sia per caratteristiche patologiche che per caratteristiche prognostiche , ma con comune denominatore laumentato rischio di carcinoma mammario [ 36 ]  . 
opinione condivisa da molti autori che al riscontro microistologico di lesione b3 debba far seguito lapprofondimento chirurgico , allo scopo di ottenere la pi affidabile conferma istologica sul tessuto mammario residuo [ 711 ]  . 
la soverchia prudenza espressa da tale atteggiamento rischia tuttavia di esporre ad un eccesso di interventi chirurgici che potrebbero risultare non necessari , dal momento che il valore predittivo positivo ( vpp ) di malignit per i b3 si situa nel range del 30% [ 1215 ]  . 
in presenza di cellule con atipie infatti ( iperplasia duttale atipica , adh , o neoplasia lobulare in situ , lin ) il vpp raggiunge il 50%60% mentre si riduce sensibilmente ( fino al 20% ) per le lesioni senza cellule atipiche ( lesioni papillari , tumore filloide , cicatrice radiale , mucocele - like lesions , alterazioni a cellule colonnari ) [ 1521 ]  . con lintento di verificare se le lesioni b3 senza atipie si possano associare ad un basso vpp per malignit e mettendo in discussione il pronto ricorso allintervento chirurgico in questi casi selezionati , stata considerata una serie consecutiva di reperti b3 , diagnosticati in un periodo di 5 anni mediante prelievo microistologico ottenuto con centratura stereotassica e sistema di retro - aspirazione ( vacuum - assisted breast biopsy , vabb )  . materials and methods materiali e metodi between february 2002 and february 2007 , 608 consecutive nel periodo compreso tra febbraio 2002 e febbraio 2007 , 1248 radiol med ( 2010 ) 115 : 12461257 patients were referred for vab . 
eligibility was determined by the results of first - line imaging performed at the same breast - care centre ( 80% of cases ) or at other diagnostic departments ( 20% of cases )  . 
the procedures were performed by an experienced radiologist ( mt ) using stereotactic digital mammography with the patient in the prone position ( mammotest , fischer imaging , denver , co , usa ) and 11 - gauge needles ( mammotome , ethicon endo - surgery , cincinnati , oh , usa )  . 
the overall accuracy of vab procedures has been analysed in a previous report [ 22 ]  . of the 608 cases scheduled for vab ( during the study period ) , the procedure was completed in 530 patients ( 87.2% ) , whereas in the remaining 78 patients ( 12.8% ) , it was attempted but not completed owing to either an inability to visualise the tiny foci of microcalcifications at the fischer workstation or to the limited thickness of the compressed breast that made sampling technically impossible . 
laffluenza delle pazienti al vabb stata regolata da indagini di primo livello espletate nella stessa unit di senologia ( nell80% dei casi ) o inviate da altri servizi di diagnosi ( nel restante 20% dei casi )  . 
le procedure sono state eseguite da un radiologo esperto ( mt ) , con tecnica radiologica digitale in modalit stereotassica , con paziente in decubito prono ( mammotest , fischer imaging , denver , colorado ) e con ago da 11 gauge ( mammotome , ethicon endo - surgery , cincinnati , ohio )  . 
 nei 608 casi avviati al vabb il prelievo stato espletato in 530 pazienti ( 87 , 2% ) mentre nelle rimanenti 78 pazienti ( 12 , 8% ) la procedura stata tentata , ma non effettuata vuoi per la impossibilit di visualizzare minuscoli focolai di microcalcificazioni alla workstation del tavolo di fischer vuoi per il ridotto spessore della mammella compressa che non ha tecnicamente reso possibile il campionamento . 
con lobbiettivo di individuare nella serie in esame possibili indicatori di probabilit di carcinoma correlati al reperto b3 , le lesioni sono state classificate secondo i seguenti parametri : et ; aspetto mammografico : microcalcificazioni isolate , opacit con o senza microcalcificazioni , distorsione con o senza micro calcificazioni ; dimensioni : in rapporto al loro maggior asse , le lesioni sono state distribuite in quattro gruppi < 5 mm , 510 mm , 1120 mm , > 20 mm ; giudizio radiologico di sospetto : ciascuna lesione stata definita in base al grado di sospetto radiologico come lieve ( r3 , equivalenti alla classificazione breast imaging reporting and data system ( bi - rads ) - r4a ) , moderato ( r4 , equivalente a bi - rads - r4b ) ed elevato ( r5 , equivalenti a bi - rads r4c / r5 ) [ 23 ] ; numero di frustoli : risultato variabile ; in particolare , nei casi di microcalcificazioni il numero di prelievi dipeso dalla verifica delle calcificazioni nel radiogramma dei frustoli ottenuto in corso di procedura . 
in rapporto alla quantit di materiale prelevato per ciascuna procedura si sono identificati tre gruppi : < 11 frustoli / procedura , 1120 frustoli / procedura , > 20 frustoli / procedura ; presenza di atipie : le lesioni b3 sono state suddivise in due distinte categorie di rischio , vale a dire lesioni b3 con atipia ( ad esempio , adh e lin o altre sottocategorie con radiol med ( 2010 ) 115 : 12461257 1249 and / or architectural atypia mentioned in our study ) , and b3 lesions without atypia . the likelihood of breast cancer was verified for all variables mentioned above . 
in fact , in agreement with our protocol , surgical excision was mostly recommended for b3 lesions with atypia , whereas in the case of b3 lesions without atypia , surgery ( rather than follow - up ) was only suggested in cases with high radiological suspicion or in response to the referring physicians or patients request [ 2426 ]  . 
most b3 lesions without atypia and raising low radiological suspicion underwent imaging follow - up rather than surgery . conversely , imaging follow - up was also performed for a minority of b3 lesions with atypia : in the case of extremely small abnormalities , which appeared to have been completely removed by needle biopsy or at the request of the referring physician or the patient . 
the absence of suspicious changes on follow - up was considered to indicate an absence of residual disease . the differences observed were analysed by univariate statistical analysis ( chi - square test )  . 
overall , the most frequent radiological appearance was represented by isolated microcalcifications ( 82.3% ) , lesion diameter was < 10 mm in 80.4% of cases , level of radiological suspicion was low in 64.7% and more than 11 cores / procedure were collected in 94.1%. 
we were thus able to assume complete removal of microcalcifications ( when the foci or opacities with microcalcifications were very small ) whenever calcifications were seen on radiography of cores from the innermost rotation and absent in peripheral cores . 
this that postbiopsy assumption was a necessity given haematoma precluded reliable assessment of any persisting small microcalcifications and the decision to proceed to surgical excision could not be delayed until after resorption of the haematoma . 
non stato sempre possibile riferire il giudizio finale allistologia del pezzo operatorio ci a dire il gold standard non stato il risultato chirurgico per tutti i casi della serie oggetto di studio . 
infatti , in accordo con il protocollo in uso , lescissione chirurgica stata raccomandata prevalentemente per le lesioni b3 con atipia , mentre per le lesioni b3 senza atipia lintervento chirurgico ( piuttosto che il follow - up ) stato consigliato solo nei casi con elevato sospetto radiologico o in relazione alle esigenze del curante o della paziente [ 2426 ]  . 
 per contro , in una minoranza di casi , stato riservato il follow - up anche a lesioni b3 con atipia : in quei casi con alterazioni di minime dimensioni , ove la lesione sembrava essere stata completamente rimossa dalla sola manovra ago - bioptica o per assecondare la volont del curante e / o della paziente . 
il follow - up ( con cadenza annuale ) stato condotto con visita senologica , ecografia e mammografia in due proiezioni , i cui risultati erano disponibili per tutte le pazienti considerate in questo studio . 
nella serie globale , laspetto radiologico pi frequente stato rappresentato da microcalcificazioni isolate ( 82 , 3% ) , il diametro risultato inferiore a 10 mm ( 80 , 4% ) , il livello di sospetto radiologico stato lieve ( 64 , 7% ) e si sono prelevati pi di 11 frustoli / procedura ( 94 , 1% )  . 
si rilevata la presenza di atipie cito - architetturali in 60 su 102 casi ( 58 , 8% )  . nella maggioranza dei casi i prelievi vabb sono stati espletati tramite multipli giri coassiali . 
stato quindi possibile ipotizzare la completa rimozione delle microcalcificazioni ( qualora i focolai o le opacit con microcalcificazioni fossero di minime dimensioni ) ogni qual volta le calcificazioni risultavano presenti nei radiogrammi dei frustoli del giro pi interno e assenti nei giri periferici . 
questo assunto si rivelato necessario in quanto lematoma post - biopsia non consentiva laffidabile valutazione della persistenza nella mammella di tenui microcalcificazioni e la decisione di ricorrere o meno allallargamento chirurgico non poteva essere procrastinata fino al riassorbimento dellematoma . 
la presenza di microcalcificazioni nei radiogrammi dei frustoli stata dimostrata in 87 dei 91 casi ( 95 , 6% ) in cui le 1250 radiol med ( 2010 ) 115 : 12461257 being studied . 
in six of these 87 cases ( 5.5% ) , the abnormality was considered to have been completely removed by vab alone on the basis of the criteria mentioned above . fifty - three patients with b3 abnormality underwent surgery ; 45 had b3 lesions with atypia at vab , and eight had b3 lesions without atypia at vab . 
in the eight cases with a vab diagnosis of b3 without atypia , the decision to proceed to surgery was justified by either the absence of calcifications in the cores ( n = 4 ) or persisting radiological suspicion ( n = 4 )  . 
in the 45 cases of b3 lesions with atypia , histology confirmed the vab diagnosis in 27 and detected no residual lesion in 13 ; in the remaining five cases ( three of lcis and two of flat epithelial hyperplasia ) , vab diagnosis was changed , revealing the presence of malignancy ( intraductal carcinoma in two , invasive ductal carcinoma in two and invasive ductal and lobular carcinoma in one )  . in these five b3 cases upgraded to malignancy after surgical excision , radiological suspicion was low in one , moderate in three and high in the remaining one . 
negli 8 casi con diagnosi vabb di b3 senza atipie la decisione di ricorrere allallargamento chirurgico stata motivata vuoi dallassenza di calcificazioni nei frustoli ( in 4 pazienti ) vuoi dal persistere del sospetto radiologico ( nei rimanenti 4 pazienti )  . 
nel gruppo delle 45 lesioni b3 con atipia , lesame istologico ha confermato la diagnosi microistologica vabb in 27 casi , non ha mostrato alcuna lesione residua in 13 casi , mentre ha cambiato la diagnosi vabb nei rimanenti 5 casi ( rispettivamente 3 casi di lin e 2 casi di iperplasia epiteliale piatta ) rilevando la presenza di tumore maligno ( neoplasia intraduttale in 2 casi , carcinoma duttale invasivo in 2 casi e carcinoma duttale e lobulare invasivo nel rimanente caso )  . 
after surgical excision , patients were followed up by clinical and imaging studies , which showed no further change . in 49 patients of our series , the definitive diagnosis was inferred from lesion stability over time and was hence based on follow - up alone . 
of the 49 patients who underwent follow - up , 31 had a vab diagnosis of b3 lesion without atypia , and 18 patients had b3 lesion with atypia . mean follow - up was 39 months . 
the minimum follow - up was 14 months for patients with b3 lesions without atypia and 26 months for patients with b3 lesions with atypia ( overall range 1484 months )  . 
nei 13 casi in cui alla biopsia chirurgica non si rilevato residuo di malattia con atipie , le dimensioni della lesione erano inferiori a 10 mm ( inferiori a 5 mm in 7 / 13 casi ) e il numero dei frustoli per ciascuna procedura vabb era superiore a 11 frustoli / paziente ( tra 11 e 20 )  . 
 in 49 pazienti della serie esaminata il giudizio finale stato desunto dalla stabilit della lesione monitorata nel tempo , quindi stato basato esclusivamente sul follow - up . delle 49 pazienti avviate al follow - up , in 31 casi la diagnosi vabb stata di lesione b3 senza atipia e in 18 casi di lesione b3 con atipia . 
la durata minima del follow - up stata di 14 mesi per le lesioni b3 senza atipia e di 26 mesi per le lesioni b3 con atipia ( range nella casistica complessiva : 1484 mesi )  . 
of cases carcinoma ( % ) p value radiol med ( 2010 ) 115 : 12461257 1252 age : 5059 > 60 morphology : isolated microcalcifications mass with calcifications mass without calcifications distortion without calcifications cluster size : < 5 mm 510 mm 1120 mm > 20 mm level of suspicion : mild r3 ( 3 ) moderate r4 ( 4a ) high r5 ( 4b5 ) no . 
the inability to visualise subtle microcalcifications on the fischer workstation was the most frequent cause of biopsy failure and is related to the reduced resolution power of the system , which , at the beginning of our experience , used a firstgeneration charged - coupled device ( ccd ) sensor . 
this limitation was overcome with the introduction of a newer version , which substantially reduced the number of failed procedures ( quantification of this improvement is under way )  . the purpose of our study was to analyse our personal series of patients with consecutive b3 lesion diagnoses at vab with the aim of identifying parameters that could help select , among this diverse group of lesions , patients to be referred for surgery and those the low risk of carcinoma to be referred for follow - up care . 
 had we been operating in an ideal situation , the variables analysed to discern patients for whom surgery could be avoided without risk should have been inferred from the histological diagnosis on the surgical specimen . however , in our series , the gold standard was histology in about half of the cases only , with follow - up albeit over a long time period constituting the reference standard in the remaining cases . 
although volumetric stability of a lesion without atypia over at least 14 months and of a lesion with atypia over at least 26 months has previously been used as a reliable criterion for the absence of malignancy [ 29 ] , we cannot confidently rule out that there may tale periodo , non si sono rilevate modificazioni dei reperti clinico - strumentali . 
nei 18 casi con atipia , la scelta del follow - up stata determinata , in 6 casi dallapparentemente completa rimozione dellintero focolaio e / o dalle ridotte dimensioni dellalterazione radiologica ( < 10 mm ) , nei restanti 12 casi per richiesta del curante o della paziente . la tabella 2 riassume la correlazione tra le variabili analizzate e la probabilit di carcinoma alla biopsia chirurgica dei casi con diagnosi b3 al vabb . 
la presenza di lesione maligna allescissione chirurgica risultata pi frequente nelle pazienti con et superiore a 50 anni ( significativo , p = 0 , 036 ) , in caso di microcalcificazioni isolate ( non significativo , p = 0 , 645 ) , in presenza di alterazione con giudizio radiologico altamente sospetto ( significativo , p = 0 , 040 ) , nei casi con pi ridotto campionamento ( borderline significativo , p = 0 , 064 ) e nei casi di lesione con atipia ( non significativo , p = 0 , 146 ) mentre nessuna correlazione stata riscontrata con le dimensioni della lesione . discussione il nostro studio fa riferimento ad una ampia serie di lesioni consecutive , senza che si siano rilevati sostanziali biases di selezione della casistica . 
la proporzione di procedure tentate ma non espletate risulta piuttosto elevata ( 12 , 8% ) tuttavia in linea con i dati della letteratura [ 27 , 28 ]  . 
limpossibilit di visualizzare sul monitor della workstation fisher le pi fini microcalcificazioni , rappresenta la causa pi frequente del mancato prelievo ed da ascrivere al ridotto potere di risoluzione del sistema che allinizio della nostra esperienza impiegava un rivelatore a ccd di prima generazione . 
tale limite stato superato grazie allintroduzione di una versione pi aggiornata che ha consentito di ridurre notevolmente il numero di indagini non espletabili ( la quantificazione di tale dato in corso )  . 
 scopo di questo lavoro stato quello di analizzare la serie personale di diagnosi consecutive b3 al vabb con lintento di identificare dei parametri che consentissero di distinguere nellambito di tale variegato gruppo di lesioni quelle da avviare ad intervento chirurgico da quelle con basso rischio di carcinoma da indirizzare al semplice follow - up , risultando in tali casi superfluo il ricorso al trattamento chirurgico . se fosse stato possibile riferirsi ad una situazione ideale le variabili analizzate con lintento di individuare i casi in cui lintervento chirurgico poteva essere evitato senza rischi avrebbero dovuto essere dedotte facendo riferimento alla diagnosi istologica sul pezzo operatorio . 
nella serie in esame , tuttavia , il risultato di riferimento ( gold standard ) rappresentato dallesame istologico chirurgico solo in circa la met dei casi , essendo nei rimanenti casi rappresentato dal follow - up , seppur esteso in ampio intervallo temporale . la stabilit volumetrica di una lesione senza atipie per almeno 14 mesi e di una lesione con atipie per almeno 26 mesi stata utilizzata anche da altri autori come criterio affidabile per lassenza di tumore [ 29 ] , peraltro dobbiamo 1254 radiol med ( 2010 ) 115 : 12461257 have been cases of underestimation in our study . 
the rate of cancer underestimation in our series is fairly low ( 5 / 102 b3 lesions ; 4.9% ) in comparison with published reports in which the ppv for carcinoma was approximately 30% [ 15 ]  . 
on the other hand , a low rate of underestimation is also evident in the subgroup of patients undergoing surgery ( 5 / 53 ; 9.4% ) , which may be additional evidence of the difficulty in evaluating the final outcome on the basis of follow - up rather than surgical histology . another possible area for discussion is the relatively high frequency ( 19.2% ) of b3 lesions observed in a consecutive series of apparently unselected cases . 
this discrepancy may be in part ascribed to a better selection of cases eligible for vab , which excluded cases of low radiological suspicion ( a high probability of a microhistological diagnosis of b2 )  . 
if this were true , in the overall series of 530 vab procedures , we should expect a higher frequency of tumours compared with the published data , whereas the cases of cancer in the series were 30.0% ( 159 / 530 ) ( 154 5 in b3 = 159 ) , in line with the expected results [ 27 ]  . 
another explanation for the high frequency of b3 lesions in our series could be our pathologists inclination to classify as b3 lesions those that other pathologists might regard as b2 . 
an excess of b3 diagnoses could also be explained by the absence of atypical lesions observed at surgery in approximately one third of cases ( the pathologist who analysed the surgical specimen was not the same one who examined the vab results in all cases )  . 
in addition , an excess of b3 diagnoses could be accounted for by the low rate of underestimation in the overall series , in the subgroup undergoing surgery and , finally , in the cases of b3 with atypia . 
a precise validation of this hypothesis could only be obtained by reviewing the preparations , a solution that could not be pursued in this study . assessment of complete b3 lesion removal by vab is not easy . 
in the majority of cases , b3 lesions appear in the form of microcalcifications , even though the spatial extension of the lesion and the microcalcifications do not always coincide . 
therefore , verification of the removal of all microcalcifications at core needle biopsy ( possible in cases of small foci ) does not completely exclude the persistence of the b3 lesion . 
even verification of complete removal of microcalcifications by vab is not totally reliable , as postbiopsy haematoma may obscure small residual ammettere che non si pu escludere con certezza che nel presente studio non si siano verificati casi di sottostima . 
in realt il tasso di sottostima di carcinoma nella serie in esame risulta piuttosto basso ( 5 sottostime in 102 lesioni b3 , pari al 4 , 9% ) rispetto a dati della letteratura che riportano un vpp per carcinoma pari a circa il 30% [ 15 ]  . 
per contro , un basso tasso di sottostima evidente anche nel sottogruppo di casi sottoposti ad intervento chirurgico ( 5 di 53 , o 9 , 4% ) , il che pu rappresentare unulteriore prova delle difficolt di valutazione del risultato finale basato sul follow - up piuttosto che sul pezzo operatorio . 
tale discrepanza potrebbe essere ascrivibile , almeno in parte , alla migliore selezione dei casi eligibili al vabb , da cui siano stati esclusi quelli con basso sospetto radiologico cio con alta probabilit di diagnosi microistologica b2 . 
se questa ipotesi fosse valida , nella serie complessiva di 530 procedure vabb ci si dovrebbe aspettare una frequenza di tumori pi elevata rispetto ai dati della letteratura , per contro le lesioni maligne nellintera serie sono stati il 30 , 0% ( 159 / 530 ) ( 154 + 5 in b3 = 159 ) , pertanto in linea con i risultati attesi [ 27 ]  . 
altra giustificazione allelevata frequenza dei b3 nella presente serie potrebbe ricercarsi nella tendenza del patologo a classificare nella categoria b3 lesioni che per altri patologi potrebbero rientrare nel gruppo b2 . 
un eccesso di diagnosi b3 potrebbe anche essere supportata dallassenza di lesione atipica allintervento chirurgico rilevata in circa un terzo dei casi ( il patologo che ha analizzato il pezzo operatorio non sempre stato lo stesso che ha esaminato il vabb ) , peraltro tale dato pu anche essere spiegato con la completa rimozione della lesione . leccesso di diagnosi b3 potrebbe anche essere ipotizzato sulla scorta del basso tasso di sottostima nella serie globale , nel sottogruppo di casi sottoposti a intervento chirurgico e infine , nei casi in b3 con atipia . 
pertanto la verifica della asportazione di tutte le microcalcificazioni ( possibile nel caso di focolai di piccole dimensioni ) durante la procedura agobioptica non consente di escludere con certezza la persistenza di lesione b3 . 
in addition , the reliability of the radiographic ascertainment of the number of microcalcifications inside the cores may also be called into question . conversely , the system we used to define the spatial extension of a lesion with vab based on the presence of microcalcifications in cores from the innermost rotation and their absence in the periphery ( more external ) may be more reliable . 
in these cases , surgery can clearly be delayed with less anxiety and , in effect , no malignancy was identified during prolonged follow - up . it has been frequently emphasised that the amount of tissue available for pathological examination is a decisive factor in determining the accuracy of a histological diagnosis [ 2931 ]  . 
as a result , the number of underestimated cancers among b3 lesions should decrease with larger tissue samples , as the pathologist would be able to recognise even extremely small tumour areas . 
in our series , the relatively small mean diameter of lesions and the large number of cores obtained might , on the one hand , have contributed to the high accuracy of the procedure and , on the other hand , account for the low rate of underestimation and the poor correlation between target volume and incidence of underestimation . in our experience , the degree of radiological suspicion related to the likelihood of carcinoma does not appear to provide any additional advantage to diagnostic accuracy given that no malignancy was detected among b3 lesions without atypia treated with surgery because of high radiological suspicion . 
on the basis of our study , the presence or absence of atypia was the only criterion for considering or ruling out surgery in patients with a vab diagnosis of b3 lesion . 
this criterion was used as a discriminant to refer patients for surgical excision in current practice . nonetheless , five cases of carcinoma versus 60 cases of b3 lesion with atypia and 0 cases of cancer versus 42 cases of b3 without atypia do not provide statistical significance owing to the small size of our sample of b3 lesions . we are aware that the findings of our study could be challenged with regard to certain aspects : prevalence of b3 lesions , criteria for determining the degree of radiological suspicion , intrinsic reproducibility and ppv of a b3 finding , mean lesion size and number of cores obtained . published data are not always stratified on the basis of these variables , and it is extremely difficult to standardise the parameters that may help to identify which b3 lesions require excision . 
for all these reasons , we believe it is unlikely that our criteria can be recommended in settings other than ours . laffidabilit della verifica radiografica del numero delle microcalcificazioni contenute nei frustoli pu essere messa in discussione . 
per contro , il sistema da noi utilizzato nel tentativo di definire con il vabb lestensione spaziale della lesione basato sulla presenza di microcalcificazioni nei frustoli ottenuti nel corso del giro di prelievi pi interno e sulla loro assenza nei frustoli dei giri pi periferici pu risultare pi affidabile . 
in questi casi , ovviamente , la chirurgia pu essere differita con minori preoccupazioni e , in effetti , nella nostra esperienza non si manifestata fino ad oggi linsorgenza di patologia maligna durante il prolungato follow - up . stato pi volte affermato che la quantit di tessuto prelevato disponibile per lesame patologico uno dei fattori determinanti laccuratezza della diagnosi istologica [ 2931 ]  . la quota di tumori sottostimati nelle lesioni b3 dovrebbe pertanto diminuire con laumentare della quantit di tessuto prelevato , cos da favorire la probabilit che i patologi riconoscano minime zone di tumore . 
nella presente serie il relativamente piccolo diametro medio delle lesioni e lelevato numero di frustoli prelevati potrebbero da un lato , aver contribuito a determinare la elevata accuratezza e consentirebbero dallaltro di giustificare il basso tasso di sottostima e la rilevata scarsa correlazione tra dimensioni del bersaglio ed incidenza della sottostima . 
 il grado di sospetto radiologico che peraltro correlato con la probabilit di carcinoma nella presente esperienza non sembra offrire alla correttezza diagnostica alcun vantaggio aggiuntivo , in quanto , nei casi b3 senza atipia sottoposti a biopsia chirurgica a causa di un elevato sospetto radiologico non stata trovata nessuna lesione maligna . sulla base di questa esperienza , la presenza o la assenza di atipie nella serie esaminata stato lunico criterio per prospettare o , rispettivamente , evitare lintervento chirurgico nei casi di diagnosi vabb b3 . 
comunque , 5 casi di carcinomi versus 60 casi di b3 con atipia e 0 casi versus 42 casi di b3 senza atipia non consentono di ottenere una reale significativit statistica , presumibilmente in relazione alle contenute dimensioni del campione di lesioni b3 . abbiamo consapevolezza che i risultati sin qui esposti possono essere messi in discussione per quanto riguarda alcuni aspetti : la prevalenza di lesioni b3 , i criteri per il giudizio di sospetto radiologico , la riproducibilit intrinseca e il valore predittivo positivo del reperto b3 , le dimensioni medie delle lesioni e il numero di frustoli prelevati . 
peraltro i dati della letteratura non sempre sono stratificati in base a queste variabili ed molto difficile standardizzare i parametri che consentano di identificare i casi b3 candidati allescissione . per tutti questi motivi riteniamo che sia difficile proporre limpiego dei criteri indicati in contesti diversi dal nostro . 1256 radiol med ( 2010 ) 115 : 12461257 nevertheless , we believe the systematic use of surgical biopsy in the presence of a microhistological diagnosis of b3 currently the standard recommended procedure to be an excessively aggressive approach . 
breast - care centres should undertake a retrospective analysis of their series of b3 lesions in an attempt to identify reliable indicators to be used in selecting patients for surgical biopsy and that are capable of increasing the ppv for malignancy to values higher than those achieved to date . nondimeno , reputiamo il ricorso sistematico alla biopsia chirurgica in presenza di una diagnosi microistologica di b3 , che sinora costituisce la procedura standard consigliata , politica eccessivamente aggressiva . 
scuro 10 , 37134 verona , italy correspondence to : v girardi , tel . : + 39 - 045 - 582445 , fax : + 39 - 045 - 8124657 , e - mail : giravero@yahoo.it received : 21 september 2009 / accepted : 6 november 2009 / published online : 23 june 2010 springer - verlag 2010 abstract purpose . 
from among 655 consecutive breast mri studies , 62 lesions ( mri visible , nonpalpable , occult at first - look us and mammography ) were recommended for second - look us . 
forty - two lesions ( 68% ) were 10 mm ; only three lesions ( 5% ) were > 20 mof all lesions , the breast imaging reporting and data system ( bi - rads ) mri category was highly suggestive of malignancy in six cases ( 10% ) , suspicious abnormality in 33 ( 53% ) and probably benign in 23 ( 37% )  . 
the detection rate at second - look us was higher for mass - like mri lesions ( 75% ) than nonmass - like lesions ( 0% ) , for lesion size > 10mm ( 90% ) and for bi - rads 4 lesions ( 88% )  . 
il numero di lesioni identificate con il second - look stato superiore in caso di impregnazione di tipo massa ( 75% ) , lesioni con dimensioni > 10 mm ( 90% ) e con bi - rads 4 ( 88% )  . dodici / 44 ( 27% ) lesioni identificate dal second look ecografico erano maligne e 5 / 18 ( 27% ) lesioni prive di traduzione ecografica erano maligne . 
il second look ecografico una valida metodica nel management delle lesioni identificate incidentalmente dalla rm mammaria in quanto consente lidentificazione e la caratterizzazione della maggioranza di esse e laccurata selezione di quelle da avviare a procedure rm - guidate . parole chiave mammella rm mammella lesioni rm indicentali second look ecografico ecografia rm guidata introduction introduzione magnetic resonance imaging ( mri ) of the breast is a diagnostic examination that can identify breast lesions that appear occult on other imaging techniques [ 14 ]  . 
due to its high sensitivity in the diagnosis of invasive breast tumours [ 57 ] , the most relevant indication for breast mri is considered to be the monitoring of women at high risk of breast cancer [ 8 ]  . 
however , the main limitations to the technique are the high number of false positive findings [ 9 ] and the difficult management of incidental findings at mri [ 10 , 11 ]  . 
in a recent meta - analysis on the role of breast mri in the preoperative evaluation of malignant disease , mri proved to be superior to mammography and ultrasound ( us ) in identifying additional neoplastic foci in 6%34% of women affected by breast tumours [ 1215 ] , but only 66% of the suspicious mri findings turned out to be malignant at histology [ 16 ]  . 
the problem of false positive results therefore appears to be numerically important , and in addition to being a source of anxiety for the patient , it generates additional costs and delays in definitive treatment as well as unnecessarily extensive surgical procedures [ 17 ]  . in this complex setting , there is need for a simple and inexpensive method for identifying and characterising incidental lesions identified on mri . 
re - evaluation with a us study performed after mri and targeted at the site where mri identified the new lesion second - look us or targeted us is the first diagnostic investigation performed in the case of a lesion identified on mri . 
the aim of second - look us is to characterise a new malignant lesion or demonstrate a false positive finding at mri to conclude the diagnostic workup in as many cases as possible and select patients to be scheduled for more complex and costly procedures , such as biopsy or lesion localisation under mri guidance . the aim of this study was therefore to verify the utility of second - look us in evaluating incidental lesions detected on breast mri by analysing its detection rate and diagnostic sensitivity . la risonanza magnetica ( rm ) della mammella unindagine diagnostica capace di identificare neoplasie mammarie occulte alle altre tecniche di imaging [ 14 ]  . 
in ragione della elevata sensibilit nella diagnosi dei tumori mammari invasivi [ 57 ] , lindicazione ad oggi pi rilevante per la rm mammaria considerata la sorveglianza delle donne ad alto rischio di tumore al seno [ 8 ]  . 
daltra parte , il limite maggiore della metodica il numero di falsi positivi [ 9 ] e la difficile gestione dei reperti incidentalmente rilevati dalla rm [ 10 , 11 ]  . 
in una recente meta - analisi riguardante il ruolo della rm mammaria nella valutazione preoperatoria della patologia maligna , la rm si dimostrata superiore rispetto a mammografia ed ecografia ( us ) nella identificazione di focolai neoplastici aggiuntivi nel 6%34% delle donne affette da neoplasia mammaria [ 1215 ] , ma solo il 66% dei reperti rm sospetti sono risultati maligni al controllo istologico [ 16 ]  . 
il problema dei falsi positivi appare quindi numericamente importante e oltre ad essere motivo di ansia per la paziente , genera costi addizionali e ritardi nel trattamento definitivo della paziente nonch interventi allargati non necessari [ 17 ]  . 
la rivalutazione mediante indagine ecografica espletata dopo la rm e mirata nella sede dove lesame rm identifica la nuova lesione , il cosidetto second look ecografico o targeted ultrasound , rappresenta il primo approfondimento diagnostico in caso di lesione individuata dalla rm . 
lintento del second look ecografico quello di caratterizzare una nuova lesione maligna o di smascherare un eventuale falso positivo della rm in modo da concludere liter diagnostico nel maggior numero possibile di casi e di selezionare il gruppo di pazienti candidate a procedure pi complesse e costose , quali la biopsia o il centraggio del reperto rm sotto guida rm . 
 con tali premesse , questo studio si propone di verificare lutilit del second look ecografico nella valutazione delle lesioni identificate incidentalmente dalla rm mammaria , 1236 materials and methods between september 2006 and december 2008 , 655 breast mri examinations were performed . 
the analysis included cases in which mri identified nonpalpable lesions that were occult on mammography and for which findings of the subsequent diagnostic investigations or follow - up for a period of 24 months were available . 
the study population therefore consisted of 61 patients ( mean age 52 years , range 2278 ) , with 62 lesions identified on mri . after undergoing mammography and us at the same centre , or in other breast imaging centres in a minority of cases , patients with the following indications were referred for mri : preoperative evaluation of known tumour in 39 cases ( 63% ) , further diagnostic investigation of a mammographic finding in five cases ( 8% ) , study of surgical scar in eight cases ( 13% ) , screening for family risk in eight cases ( 13% ) and study of breast implants in two cases ( 3% )  . lesions were grouped by both mri appearance and size and in relation to the degree of suspicion on mri according to the american college of radiology breast imaging reporting and data system ( bi - rads ) lexicon [ 18 , 19 ]  . mri appearance of lesions studied with mri - guided us was a mass - like enhancement in 59 / 62 cases ( 95% ) and a non - mass - like enhancement in three ( 5% )  . 
in line with the birads classification , mri assessment was highly suggestive of malignancy ( bi - rads 5 ) in six cases ( 10% ) , suspicious for malignancy ( bi - rads 4 ) in 33 ( 53% ) and probably benign in 23 ( 37% )  . 
 us findings were analysed by evaluating the number of lesions identified by second - look us in relation to mri appearance , lesion size and level of suspicion and by calculating sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) of second - look us . 
sono stati inclusi nellanalisi i casi in cui la rm ha identificato lesioni non palpabili e non visibili allindagine senologica convenzionale e in cui fosse disponibile il risultato del successivo iter diagnostico o del follow - up per un periodo di almeno 24 mesi . 
il numero incidentali rilevati con rm complessivo di reperti mammaria nel periodo in studio stato di 69 rilievi rm per i quali stato suggerito il proseguimento diagnostico con ecografia mammaria mirata nella sede del reperto . 
 dopo aver espletato mammografia ed ecografia nella stessa sede o , in una minor parte dei casi , in altri centri di diagnosi senologica , le pazienti afferivano allindagine rm con le seguenti indicazioni : valutazione preoperatoria di neoplasia nota in 39 casi ( 63% ) , approfondimento di reperto mammografico in 5 casi ( 8% ) , studio di cicatrice in 8 casi ( 13% ) , screening per rischio familiare in 8 casi ( 13% ) e studio di protesi in 2 casi ( 3% )  . 
le lesioni sono state raggruppate sia per aspetto rm , sia per dimensione e distribuite in rapporto al giudizio di sospetto rm secondo il lessico dellamerican college of radiology ( acr ) secondo la classificazione breast imaging reporting and data system ( bi - rads ) [ 18 , 19 ]  . 
laspetto rm delle lesioni sottoposte ad ecografia rm - guidata stato di impregnazione mass - like in 59 / 62 casi ( 95% ) e di impregnazione non mass - like in 3 casi ( 5% )  . 
le dimensioni della lesioni rm erano inferiori o uguali a 10 mm in 42 casi ( 68% ) , comprese fra 10 e 20 mm in 17 casi ( 27% ) o superiori a 20 mm in 3 casi ( 5% )  . utilizzando la classificazione bi - rads il giudizio radiologico rm stato altamente sospetto di malignit ( birads 5 ) in 6 casi ( 10% ) , sospetto di malignit ( birads 4 ) in 33 casi ( 53% ) , e probabilmente benigno in 23 casi ( 37% )  . i risultati dellecografia sono stati analizzati valutando il numero di lesioni identificate dal second look ecografico in relazione allaspetto rm , alle dimensioni della lesione e al grado di sospetto radiologico e calcolando i valori di sensibilit , specificit , valore predittivo positivo e valore radiol med ( 2010 ) 115 : 12341245 1237 without temporal limitations in postmenopausal women ( 25 cases )  . 
images were acquired with a dedicated bilateral breast surface coil with the patient in the prone position . the dynamic study was performed with a three - dimensional gradient recalled echo ( 3d - gre ) sequence in the coronal plane ( tr / te 12 / 5.65 ms ; flip angle 25 ; matrix 254320 pixels ; fov 38075 ; thickness 1.24 mm ; acquisition time 60 s ) acquired prior to contrast administration and repeated six times after the intravenous injection of 0.1 mmol / kg of gadoterate meglumine ( dotarem , guebert co . ) at an injection rate of 2.5 ml / s followed by 20 ml of saline solution . images were processed with subtraction of precontrast images from postcontrast images and analysed according to the parameters of mass - like and non - mass - like enhancement [ 19 ]  . 
mri lesions with no definite correlate at first - look mammography and us were recommended for second - look us . targeted us ( second - look us ) and lesion management us study targeted at the site of the lesion identified at mri was carried out in the 2 weeks following the mri examination either by the same or a different operator . 
to identify the site of the incidental mri finding , the nipple and axial and sagittal planes passing through it and dividing the breast into quadrants were taken as reference points . 
in cases in which the mri lesion had a us correlate , the diagnostic workup proceeded according to the degree of us suspicion and , if necessary , with us - guided biopsy . 
in the cases in which the mri find had no us correlate , the finding was monitored with mri after 6 months for bi - rads 3 lesions or with histopathological examination for bi - rads 4 and 5 lesions . 
the reference standard was 24 - month follow - up and histopathology examination , respectively . results second - look us identified 44 of the 62 incidental lesions detected on breast mri ( 71% )  . 
i risultati sono stati analizzati con il test statistico di fisher ( significativit : p < 0 , 05 )  . esame rm lo studio rm stato effettuato con un magnete da 1 , 5 t ( symphony , siemens medical system , erlagen , germania ) nel periodo compreso fra 714 giorno del ciclo mestruale ( 37 casi ) e senza limitazioni temporali nelle donne in menopausa ( 25 casi )  . 
lo studio dinamico stato eseguito con una sequenza gradient echo ( gre ) 3d sul piano coronale ( tempo di ripetizione [ tr ] / tempo di eco [ te ] : 12 / 5 , 65 ms ; flip angle 25 ; matrice 254320 pixel ; campo di vista [ fov ] 38075 ; spessore 1 , 24 mm ; tempo di acquisizione 60 secondi ) acquisita prima della somministrazione di mezzo di contrasto ( mdc ) e ripetuta per sei volte dopo liniezione endovenosa di 0 , 1 mmol / kg di gadoterate meglumina ( dotarem , guerbet co . , villepinte , francia ) alla velocit di 2 , 5 ml al secondo e di 20 ml di soluzione fisiologica . 
 le immagini sono state elaborate mediante sottrazione delle acquisizioni pre - contrasto da quelle post - contrasto e analizzate secondo i parametri di impregnazione mass - like e non masss - like [ 19 ]  . 
posizionando una regione dinteresse ( roi , estesa 59 pixels ) sulle aree di impregnazione di mdc visualizzate nella seconda acquisizione dopo somministrazione di mdc sono state costruite curve delle variazioni di intensit di segnale / tempo . 
sono state avviate al second look ecografico le lesioni rm mancanti di sicuro corrispettivo con i reperti evidenziati al first look mammografico ed ecografico . indagine ecografica mirata ( second look ecografico ) e gestione delle lesioni lecografia mirata nella sede della lesione individuata dalla rm stata eseguita nelle 2 settimane successive alla rm sia dallo stesso operatore che ha espletato la rm che da operatori diversi . 
the remaining seven cases were subjected to mri - guided microhistological biopsy in three cases and histological examination during surgery for the primary tumour in the remaining four ( quadrantectomy in three and mastectomy in one )  . 
second - look us identified 44 / 59 ( 75% ) mri lesions with mass - like enhancement and 0 / 3 with non - mass - like enhancement ( table 1 )  . 
with regard to lesion size , secondlook us identified a correlate to the mri finding in 26 / 42 ( 62% ) lesions 10 mm ( p = 0.03 ) , in 15 / 17 ( 88% ) mri lesions between 10 and 20 mm ( p = 0.0004 ) and in all three ( 100% ) mri lesions with a long axis > 20 mm ( p = 0.55 ) precedenti che le immagini dellindagine rm . 
per la individuazione della sede della lesione incidentale alla rm mammaria , sono stati presi come punti di riferimento il capezzolo e i piani assiale e sagittale passanti per esso in modo da suddividere la mammella in quadranti . 
nei casi in cui il reperto rm non avesse corrispettivo ecografico , il reperto stato seguito con controllo rm dopo 6 mesi in caso di lesione bi - rads 3 o con approfondimento patologico nei casi di bi - rads 4 e 5 . 
il gold standard stato rispettivamente il follow - up a 24 mesi e lesame patologico . risultati lecografia mirata nella sede della lesione evidenziata dalla rm ha identificato 44 su 62 lesioni incidentali alla rm mammaria ( 71% )  . 
2a - c donna di 49 anni con addensamento nel versante esterno della mammella destra , fisso alla cute ( diagnosi microistologica ; carcinoma duttale infiltrante ) ( immagine assiale in proiezione di massima intensit [ mip ] t1 gre con sottrazione , a )  . 
lesame rm dopo somministrazione di mdc , evidenzia in regione parareolare della mammella contro laterale , formazione ovalare di 7 mm , con impregnazione mass - like ( piano coronale t1 gre con sottrazione , b )  . 
il reperto ha caratteri macroscopici di benignit ed stato avviato a controllo dopo 6 mesi . sono state sottoposte a prelievo sotto guida ecografica per esame patologico ( citologico in 19 casi e microistologico in 11 casi )  . 
i rimanenti 7 / 18 casi sono stati sottoposti a prelievo microistologico sotto guida rm in 3 casi e ad esame istologico nel corso dellintervento chirurgico per la patologia primitiva nei rimanenti 4 casi ( quadrantectomia in 3 casi e mastectomia in 1 caso )  . 
il second look ecografico ha evidenziato 44 / 59 ( 75% ) lesioni rm con enhancement di tipo mass - like e 0 / 3 lesioni rm con enhancement di tipo non mass - like ( tabella 1 )  . 
la presenza di un reperto ecografico correlato stato pi frequente nelle lesioni con impregnazioni mass - like rispetto a quelle non mass - like ( p = 0 , 02 )  . 
 rispetto al risultato patologico , il second look ecografico ha identificato 32 / 45 ( 71% ) lesioni benigne e 12 / 17 ( 71% ) lesioni maligne ( p = 0 , 38 ) ( tabella 4 )  . 
il risultato istologico delle 12 / 44 lesioni maligne riconosciute dal second look ecografico stato di carcinoma infiltrante in 9 casi ( rispettivamente duttale in 6 casi e lobulare in 3 casi ) e di carcinomi in situ nei rimanenti 3 casi . 
il risultato istologico delle 5 / 18 lesioni maligne incidentali alla rm mammaria stato di carcinoma infiltrante in tutti i casi ( duttale in 4 casi e lobulare in 1 caso )  . 
dodici / 44 ( 27% ) lesioni identificate dal second look ecografico erano maligne e 5 / 18 ( 27% ) lesioni prive di corrispettivo ecografico erano maligne ( p = 0 , 2 )  . 
 nel complesso , il second look ecografico mirato nella sede della lesione identificata dalla rm con prelievo ecoguidato ha dimostrato sensibilit del 71% , specificit del 1240 radiol med ( 2010 ) 115 : 12341245 fig . 
targeted sonogram shows normal lymph node ( b ) corresponding to the enhancing node near the vessel and an oval , ill - defined hypoechoic solid mass ( c ) corresponding to the deeper enhancing node . 
lesame rm con mdc mostra oltre al reperto noto due formazioni pi piccole , con impregnazione mass - like ( immagine sagittale mip t1 gre con sottrazione , a )  . 
histological diagnosis of the 12 / 44 malignant lesions identified by second - look us was infiltrating carcinoma in nine ( ductal in six and lobular in three ) and carcinoma in situ in the remaining three . 
histological diagnosis of the 5 / 18 malignant lesions identified incidentally at breast mri was infiltrating carcinoma in all cases ( ductal in four and lobular in one )  . 
nel caso in cui lindagine rm identifichi un nuova lesione , sospetta , non palpabile e priva di corrispettivo mammografico ed ecografico , la lesione mammaria in questione dovrebbe essere sottoposta a biopsia o a centraggio sotto guida rm [ 20 ]  . 
nonostante i sistemi di biopsia rm guidata si stiano diffondendo in diversi centri , i costi piuttosto proibitivi rappresentano lostacolo principale alla larga diffusione alla popolazione generale , sia nel panorama nazionale che in quello internazionale . 
bi - rads breast imaging reporting and data systems table 1 second - look ultrasound ( us ) correlate versus magnetic resonance imaging ( mri ) lesion type in 62 lesions mri enhancement pattern no . 
of lesions without second - look us correlate mass - like non - mass - like 44 / 59 ( 75% ) 0 / 3 ( 0% ) 15 / 59 ( 25% ) 3 / 3 ( 100% ) tabella 1 identificazione della lesione con second look ecografico versus tipo di lesione alla risonanza magnetica ( rm ) caratteri rm della lesione numero lesioni identificate con second look ecografico numero lesioni non identificate con second look ecografico impregnazione mass - like impregnazione non mass - like 44 / 59 ( 75% ) 0 / 3 ( 0% ) 15 / 59 ( 25% ) 3 / 3 ( 100% ) table 2 second - look ultrasound ( us ) correlate versus magnetic resonance imaging ( mri ) lesion size in 62 lesions mri lesion size no . 
in the event the mri study identifies a new , suspicious and nonpalpable lesion with no mammography and us correlate , the breast lesion should be subjected to mri - guided biopsy or localisation [ 20 ]  . 
although mri - guided biopsy systems are becoming increasingly available in numerous centres , the rather prohibitive costs constitute the main barrier to their widespread diffusion both in italy and abroad . 
the costs of mri - guided localisation procedures would be more limited if the economic costs could be divorced from the psychological costs of a subsequent surgical biopsy for lesion characterisation . second - look us is a fast , simple and inexpensive technique widely available in breast diagnostic centres and is a psicologici , di una successiva biopsia chirurgica per la tipizzazione della lesione . il second look ecografico un approfondimento veloce , semplice , poco costoso e largamente diffuso tra i centri di diagnosi senologica e rappresenta lindagine di primo livello nella valutazione delle lesioni individuate dalla rm . 
quando evidenzia un reperto di sicuro corrispondente a quello rm , il second look ecografico ne consente la tipizzazione estemporanea mediante prelievo sotto guida ecografica eludendo la necessit di procedure rmguidate . per valutare lutilit del second look ecografico nella individuazione e tipizzazione delle lesioni incidentali alla rm mammaria , stata analizzata una serie di 62 reperti identificati dalla rm , occulti alle precedenti mammografia ed ecografia quindi avviati al second look - ecografico . laspetto rm delle lesioni sottoposte ad second look ecografico stato nella maggior parte di impregnazione mass - like ( 59 casi ; 95% )  . 
when it identifies a lesion that is a definite correlate for the mri finding , second - look us is able to extemporaneously characterise the lesion by us - guided biopsy , thus avoiding the need for an mri - guided procedure . to evaluate the utility of second - look us in identifying and characterising incidental lesions found at breast mri , we analysed a series of 62 mri findings that were occult on the earlier mammographic and sonographic studies and therefore sent for second - look us . 
the dimensions were limited 10 mm in 42 cases ( 68% ) and the level of suspicion was in most cases bi - rads 4 ( 33 cases , 53% )  . targeted us after mri identified most lesions detected on mri ( 71% )  . 
the result is in agreement with other studies in which the rate of incidental mri findings detected by second - look us was reported to vary between 23% and 89% according to patient selection and breast - imaging expertise [ 2125 ]  . with regard to frequency of malignancy , 27% of lesions with a us correlate were malignant . 
unlike other studies in which the risk of malignancy was greater in mri lesions with a us correlate [ 21 , 25 ] , and in agreement with other observations [ 24 ] , our series did not demonstrate a correlation between second - look us and a diagnosis of malignancy . 
therefore , the absence of a us correlate is not a sufficient condition for ruling out the presence of a tumour ; nor does it lower the risk that the mri - detected lesion is malignant . 
in these cases , the diagnostic workup is not concluded and must proceed according to the level of mri suspicion and the clinical findings and patient history [ 25 ]  . although the main limitation of our study was the small number of lesions , findings are comparable with those of a recent study by demartini et al . 
unlike their study , however , the small number of cases in our study could in part be responsible for the failure to reach statistical significance regarding the increased risk of malignancy for lesions with a us correlate with respect to those with no us correlate . inferiori o uguali a 10 mm in 42 casi ( 68% ) , e il giudizio di sospetto stato nella maggior parte dei casi bi - rads 4 ( 33 casi ; 53% )  . lecografia mirata dopo rm ha permesso di riconoscere la maggior parte delle lesioni identificate dalla rm ovvero il 71% . 
il risultato in accordo con quello osservato in altre esperienze nelle quali , la percentuale di reperti incidentali alla rm identificati dal second look riportata con valori variabili a seconda degli autori , della selezione dei pazienti e della cultura senologica tra il 23% e l89% [ 2125 ]  . per quanto riguarda la frequenza di malignit , il 27% delle lesioni che avevano un corrispettivo ecografico sono risultate maligne . 
a differenza di altri studi in cui il rischio di lesione maligna era maggiore nelle lesioni rm con corrispettivo ecografico [ 21 , 25 ] , e in accordo con altre osservazioni [ 24 ] , nella presente serie non stata dimostrata associazione tra il second look ecografico e la diagnosi di malignit . 
in particolare , il 27% delle lesioni identificate dalla rm sono risultate maligne sia in presenza di un reperto corrispondente al second look ecografico sia in assenza di reperti al second look ecografico . 
in questi casi , liter diagnostico non concluso e deve proseguire secondo il livello di sospetto rm , nonch secondo i dati clinici e anamnestici della paziente [ 25 ]  . 
a differenza di questultima per , lesiguit dei casi potrebbe rendere ragione del mancato raggiungimento della significativit statistica per quanto riguarda il maggior rischio di malignit per le lesioni con corrispettivo ecografico rispetto a quelle senza corrispettivo ecografico . 
 in conclusione , il second look ecografico una strategia 1244 radiol med ( 2010 ) 115 : 12341245 in conclusion , second - look us is a valid strategy in the management of lesions identified on breast mri , enabling detection in most cases and characterisation in 71% of malignant lesions . 
however , mri sensitivity should not be underestimated , and in cases of mri suspicion with no us correlate and in the setting of appropriate clinical findings and history , performing mri - guided biopsy or localisation is recommended . valida nel management delle lesioni rilevate dalla rm mammaria , consentendone la identificazione nella maggioranza dei casi e la tipizzazione nel 71% delle lesioni maligne . 
daltra parte non deve essere sottovalutata la sensibilit della rm e nei casi rm sospetti , privi di corrispettivo ecografico e nellappropriato contesto clinicoanamnestico opportuno procedere a biopsia o centraggio sotto guida rm . 
in an 18 - month period , we treated 18 patients ( 13 men , five women , age range 3981 years ) with the silverhawk directional atherectomy device . inclusion criteria were symptomatic femoropopliteal stenosis / insufficiency , nonresponsiveness to medical therapy , and rutherford categories 35 . 
exclusion criteria were based on the preliminary colour doppler ultrasound ( us ) assessment and were plaque with a calcified component > 50% and inadequate upstream and / or downstream vascular bed . 
i criteri di esclusione , basati sulleco color doppler preliminare , erano : placca con componente calcifica > 50% e letto vascolare a monte e / o a valle inadeguato . 
il follow - up a 2 e 12 mesi ha evidenziato un caso di reocclusione distale , trattato con successiva amputazione , e due casi di restenosi ( perviet primaria del 79% ) : questi due pazienti sono stati successivamente trattati con successo mediante ripetizione della procedura ( perviet secondaria del 96% )  . radiol med ( 2010 ) 115 : 12081218 1209 conclusions . 
the silverhawk directional atherectomy device proved to be an effective and safe tool in all our patients treated for femoropopliteal stenosis / occlusion , with a significant improvement in both imaging findings and clinical signs and symptoms . 
laterotomo direzionale silverhawk si dimostrato efficace e privo di complicanze di rilievo in tutti i pazienti con steno - occlusione femoro - poplitea trattati , con un miglioramento considerevole sia del quadro strumentale che clinico - sintomatologico . 
 keywords chronic obstructive arteriopathy stenosis directional atherectomy device femoropopliteal artery parole chiave arteriopatia cronica ostruttiva stenosi aterotomo direzionale arteria femoro - poplitea introduction introduzione treatment approaches to obliterative arterial disease of the femoral arteries have dramatically changed in the last decade . 
until a few years ago , stenting was restricted to cases in which angioplasty had failed [ 1 , 2 ] , and as recently as 2005 , the american college of cardiology still did not acknowledge any major role for femoral stenting in the treatment of ischaemia of the lower extremities [ 3 ]  . 
in the meantime , new tools are being added to the therapeutic armamentariu among them , the silverhawk directional atherectomy device is attracting the most interest among investigators because of its ability to effect plaque removal through endovascular atherectomy [ 6 ]  . 
a small cutting assembly is located at the distal end of the catheter : it is made up of an internal rotating blade housed in a tubular casing and connected with a chamber where the excised material is collected . 
the proximal end of the catheter is designed to be inserted into a single - use battery - operated driver unit . the purpose of our study was to evaluate the feasibility , immediate effectiveness and vascular patency at 2and 12month follow - up of endovascular silverhawk directional atherectomy in patients with stenosis / occlusion of the femoral artery . materials and methods from january 2007 to june 2008 , 18 patients ( 13 men , five women ; age range 3981 years ) affected by stenosis / occlusion of the femoropopliteal segment were treated with the silverhawk directional ( ev3 , plymouth , nj , usa )  . 
the lesion was located immediately upstream of the bifurcation of the common femoral artery in atherectomy device la modalit di trattamento dellarteriopatia obliterante delle arterie femorali ha subito nellultimo decennio un vero e proprio capovolgimento : sino a poco tempo fa il ruolo dello stent era riservato ai casi di fallimento dellangioplastica [ 1 , 2 ] ; ancora nel 2005 lamerican college of cardiology non riconosceva allo stenting femorale un ruolo preminente nel trattamento delle ischemie degli arti inferiori [ 3 ]  . 
nel frattempo larmamentario terapeutico si arricchisce di nuovi strumenti . tra questi lutilizzo dellaterotomo direzionale silverhawk sta destando i maggiori interessi nella comunit scientifica per le sue possibilit di determinare una rimozione della placca mediante aterectomia endovascolare [ 6 ]  . 
il catetere , del calibro di 7 french , composto di un corpo flessibile progettato per scorrere su una guida da 0 , 014 pollici . sullestremit distale del catetere situato un piccolo gruppo di taglio costituito da una lama rotante interna contenuta in un alloggiamento tubolare , in collegamento con una camera in cui viene raccolto il materiale asportato dalloperazione di recisione . 
lestremit prossimale del catetere stata studiata per essere inserita in un azionatore a batteria monouso che consente lattivazione della lama . lobiettivo del nostro studio rappresentato dalla valutazione della fattibilit e dellefficacia immediata e della perviet vascolare al follow - up a 2 e 12 mesi dellaterotomia endovascolare direzionale silverhawk in pazienti affetti da steno - occlusione dellarteria femorale . materiali e metodi da gennaio 2007 a giugno 2008 sono stati trattati 18 pazienti , affetti da steno - occlusione del tratto femoropopliteo , utilizzando laterotomo direzionale silverhawk ( ev3 , plymouth , usa )  . 
dei 18 pazienti , 13 erano di sesso 1210 radiol med ( 2010 ) 115 : 12081218 one case , whereas in the remaining 17 cases , it was in the distal third of the superficial femoral artery and / or at the level of the popliteal artery . 
la lesione era localizzata in un caso immediatamente a monte della biforcazione dellarteria femorale comune , mentre nei restanti 17 essa era localizzata in corrispondenza del terzo distale dellarteria femorale superficiale e / o in corrispondenza dellarteria poplitea ( non veniva fatta distinzione a livello di tale tratto femoro - popliteo , il cui limite non sempre ben definibile e che spesso interessato diffusamente )  . 
patient 14 showed patency of the treated segment at the 2 - month follow - up but also a severe occlusion of the vascular axis below , and consequently underwent foot amputation number - sex age rutherford tasc diabetes arterial obesity category class hypertension hypercholeprimary patency . 
the unsubtracted images ( b , c ) show distension of the angioplasty balloon ( arrows in b ) and the directional atherectomy device in place ( arrows in c )  . 
le immagini non sottratte ( b , c ) evidenziano la distensione del pallone per angioplastica ( frecce in b ) e laterotomo direzionale in sede ( frecce in c )  . 
langiografia post - trattamento ( d ) dimostra la perviet vasale . the patients treated , five had a previously implanted femoral stent that showed clinical and colour doppler ultrasound ( us ) evidence of stenosis / occlusion . 
dei pazienti trattati , 5 erano portatori di stent femorale precedentemente posizionato con segni clinici ed ecocolor - doppler di 1212 radiol med ( 2010 ) 115 : 12081218 patients were initially identified with a clinical examination ( with identification of any skin lesions ) , evaluation of the windsor ankle - brachial index ( abi ) and walking exercise ( where possible )  . 
imaging assessment included preliminary colour doppler us with identification of the stenosis / occlusion , its site , extent ( in centimetres ) , characteristics ( either central or eccentric ) and type , with quantification of the atherosclerotic tissue ( fibrofatty , calcified )  . 
exclusion criteria were the presence of a plaque showing > 50% calcified component at preliminary doppler evaluation ( for which another system was preferred ) and the presence of an inadequate vascular bed upstream and / or downstream of the lesion at colour doppler imaging . 
the contralateral femoral artery was punctured percutaneously , and a 5 - f , 10 - cm endovascular introducer ( cook , usa ) was positioned with the seldinger technique . 
the abdominal aorta was catheterised with a 5 - f pigtail catheter ( cook ) , and the aortoiliac region and lower extremities were studied with digital subtraction angiography using 370 mgi / ml nonionic contrast material infused as multiple rapid boluses to obtain preprocedural evaluation . 
the procedure proper was then started with either crossover access from the contralateral iliac artery ( n = 12 ) or direct antegrade puncture of the ipsilateral femoral artery ( n = 6 )  . 
for the contralateral crossover approach , a 7 - f , 45or 55 - cm - long flexor check flo introducer ( cook ) was advanced through the artery , whereas for the ipsilateral approach , a 7 - f , short , 10 - cm introducer ( cook ) was used . 
the directional atherectomy device was then inserted and advanced . whenever this step proved difficult ( as occurred in six procedures ) , the stenosis was first dilated by using a percutaneous transluminal angioplasty catheter measuring 48 cm in length and 68 mm in diameter ( evercross , ev3 , usa , or wanda , boston scientific , usa ) with a low - pressure balloon ( maximum 2 atmospheres )  . 
 inizialmente individuati mediante visita clinica ( con definizione di eventuali lesioni cutanee ) , valutazione dellindice caviglia - brachiale di windsor e analisi degli esercizi di durata del cammino ( quando possibile )  . 
dal punto di vista strumentale i pazienti venivano invece studiati con eco color doppler preliminare con identificazione della steno - occlusione , della sua sede , della sua estensione ( classificata in centimetri ) , delle sue caratteristiche ( centrale o eccentrica ) e della tipologia con quantificazione di tessuto aterosclerotico ( fibrolipidico , calcifico )  . 
venivano nel frattempo misurati e registrati i parametri di stenosi e dellocclusione , quali le velocit del picco sistolico , le caratteristiche dellonda doppler pree post - stenotica con relativa morfologia . 
i criteri di esclusione erano rappresentati dalla presenza di placca che alla valutazione doppler preliminare mostrava una componente calcifica eccedente il 50% ( in questo caso si preferiva usare altro sistema ) e dalla presenza di un letto vascolare a monte e / o a valle ritenuto inadeguato al color doppler . 
 previa ratifica del consenso informato , il paziente veniva sottoposto alla procedura percutanea previa puntura percutanea dellarteria femorale controlaterale e posizionamento di introduttore endovascolare da 5 f da 10 cm ( cook , usa ) con tecnica di seldinger ; previo cateterismo dellaorta addominale con catetere pig - tail da 5 f ( cook ) si procedeva ad angiografia digitale aorto - iliaca e degli arti inferiori con mdc non ionico alla concentrazione di 370 mgi / ml , previa infusione con boli rapidi ripetuti per ottenere il quadro angiografico preprocedurale . 
successivamente si dava inizio alla procedura vera e propria previo cross - over delliliaca contro laterale ( 12 casi ) oppure mediante puntura diretta secondo corrente dellarteria femorale del lato da trattare ( 6 casi ) ; la scelta della tipologia dellapproccio era legata alla sede e alla tipologia della stenosi cercando di privilegiare in ogni caso , quando possibile , lapproccio contro laterale con cross over . 
nel caso dellapproccio contro laterale in ogni caso , dopo cross - over , si proceduto allavanzamento di un introduttore lungo da 7 f di 45 o 55 mm di lunghezza del tipo flexor check flow ( cook ) ; in caso di approccio omolaterale si invece proceduto ad avanzare introduttore corto da 10 cm ( cook ) sempre da 7 f . 
successivamente si procedeva quindi al valicamento della steno - occlusione mediante guida idrofila 0 , 0140 , 035 pollici e cateterismo distale con catetere idrofilo 4 o 5 f ( terumo , giappone )  . 
si provvedeva quindi allavanzamento dellaterotomo direzionale : quando questo passaggio risultava difficoltoso ( nel nostro studio ci avveniva in 6 procedure ) , si provvedeva a preventiva dilatazione della stenosi con catetere per pta con lunghezza che radiol med ( 2010 ) 115 : 12081218 1213 variava dai 4 agli 8 cm e con diametro di 6 - 8 mm evercross ( ev3 , usa ) o wanda ( boston scient , usa ) con distensione del palloncino a bassa pressione , non eccedente le 2 atmosfere ; a questo punto veniva somministrato un bolo di eparina endovena ( ev ) da 5000 unit internazionali . 
i passaggi per aterectomia variavano dai 5 ai 12 , fino a quando il risultato della perviet del lume e del rimodellamento parietale non veniva considerato soddisfacente ; ogni qualvolta si avvertiva loccupazione della camera di compattamento del materiale estratto , questa veniva vuotata e il materiale analizzato qualitativamente e quantitativamente . 
mediante pompa peristaltica ; al terzo giorno veniva iniziata una terapia con doppio antiaggregante ( clopidrogel + cardioaspirina ) , continuata per 3 mesi dopo la procedura . la valutazione clinica del risultato veniva effettuata subito al termine della procedura e nei giorni successivi , con misurazione dellindice caviglia - brachiale e valutazione con eco color doppler per lanalisi delle variazioni , rispetto ai precedenti pre - procedurali , in termini morfologici , flussimetrici e colorimetrici . 
i pazienti venivano valutati per il costante monitoraggio clinico , strumentale , laboratoristico da eseguire a 1 , 2 , 12 mesi e venivano controllati con valutazione clinica , mediante misurazione del tratto di cammino , dellindice caviglia - brachiale e assegnazione dello stadio di rutherford , e con eco color doppler con ridefinizione di tutti i parametri di stenosi confrontati con i medesimi ricavati nelle precedenti valutazioni . 
pretreatment angiography ( a ) shows multiple stenoses along the arterial stent ( arrows ) , whereas posttreatment angiography ( b ) depicts sufficient wall remodelling along the stent fig . 
langiografia post - trattamento ( b ) dimostra un sufficiente rimodellamento parietale lungo lo stent . was considered full of harvested plaque material , it was emptied , and the quantity and quality of the material was analysed . 
on day 3 , double antiaggregant therapy ( clopidogrel + low - dose aspirin ) was commenced and continued for 3 months after the procedure . the clinical evaluation of outcome was performed immediately after the procedure and over the following days , with measurement of anklebrachial index and colour doppler us examination to analyse any variations in morphology , flowmetry and colourimetry with respect to the preprocedural findings . 
patients were assessed for continuous clinical , imaging and laboratory monitoring performed at 1 , 2 and 12 months and were followed up with clinical assessment , walking distance test , anklebrachial index and 1214 radiol med ( 2010 ) 115 : 12081218 rutherford stage , as well colour doppler us with redefinition of all stenosis parameters compared with those obtained in the previous assessments . 
at imaging and clinical assessment immediately after the procedure , all patients showed improved angiographic and colour doppler us findings ( in terms of primary patency , reduced extent of stenosis , reduced systolic peak , change in doppler waveform due to downstream revascularisation )  . 
at the same time , improvements in the clinical symptoms and signs were observed and quantified in each patient as a shift of at least one stage in the rutherford classification . 
n allo studio angiografico di fine procedura e n al monitoraggio clinico venivano riportati segni riferibili ad embolizzazione o dislocazione frammentaria a valle della sede delle lesioni trattate ( tabella 1 )  . 
inoltre per la sua invasivit poco gradito ai pazienti e difficile da eseguire in numerose condizioni di comorbidit importanti determina percentuali di morbilit e mortalit non trascurabili ; anche nei casi pi favorevoli poi si registra un tempo di recupero per le radiol med ( 2010 ) 115 : 12081218 discussion treatments for femoral stenoses / occlusions have seen dramatic changes over the last 10 years . 
where grafting is required , and in other , more complex , anatomical situations , primary patency of the bypass graft decreases substantially [ 810 ]  . in addition , bypass grafting is an invasive procedure that is not well tolerated by the patient and is difficult to perform in the presence of significant comorbidity , leading to nonnegligible morbidity and mortality rates . 
the efficacy of endovascular treatment was definitively demonstrated by the bypass versus angioplasty in severe ischaemia of the leg ( basil ) experience [ 13 ] , a randomised controlled trial carried out in the uk that demonstrated a comparable rate of amputations for the two patient groups but with significantly longer hospital stays and more complications in the patients treated with surgery . it appears clear that endovascular treatment is particularly appreciated by patients and represents the sole treatment option for all patients with significant comorbidities who are not candidates for surgery [ 11 ]  . the most widespread and consolidated percutaneous endovascular treatment of atheromatous disease is angioplasty and / or stenting : neither removes the plaque , they only press against it , flattening it along the vessel walls with constant barotrauma on the walls . 
 have all been suggested [ 15 , 16 ] , as well as the use of a cutting balloon a noncompliant balloon catheter with longitudinal microtomes on its surface [ 18 ]  . 
in the femoropopliteal area , the broader problem of stent patency and stent endothelisation in the various body regions is compounded by the peculiarities of this anatomical area , including the length of the vessel and the stress it undergoes as it runs through canals of strong muscle groups . 
appare comunque evidente che il trattamento endovascolare particolarmente gradito dal paziente e rappresenta una prospettiva terapeutica priva di alternativa in tutti quei pazienti che presentano comorbidit importanti , non eleggibili al trattamento chirurgico [ 11 ]  . il trattamento endovascolare percutaneo della malattia ateromasica pi diffuso e consolidato rappresentato dallangioplastica e / o stenting : entrambi non provvedono a rimuovere la placca , ma si limitano a spalmarla lungo le pareti con meccanismo di schiacciamento , con un effetto costante di barotrauma a carico delle pareti ; con lo stenting si ottiene successivamente un rimodellamento delle pareti del vaso [ 14 ]  . 
alla problematica pi generale della perviet degli stent nei vari distretti corporei connessa alla endotelizzazione dello stent , si associa infatti , per il distretto femoro - popliteo , quella connessa alla particolarit del distretto anatomico in questione , rappresentata dalla lunghezza del vaso e dalle sollecitazioni che riceve in rapporto allattraversamento di canali di poderosi gruppi muscolari . 
 i primi dati circa limpiego del silverhawk per il trattamento delle steno - occlusioni dei vasi degli arti sono stati 1216 radiol med ( 2010 ) 115 : 12081218 and stent reocclusion rates that are impossible to reduce [ 17 ]  . 
 the first data on the use of silverhawk in the treatment of stenoses / occlusions of lower - limb vessels have been collected in the treating peripherals with silverhawk : outcomes collection ( talon ) registry involving 19 hospitals in the usa . 
the study reports excellent shortto mid - term results in 601 treated patients , with a 6 - month patency rate of 97% ; the 12 - month patency rate is slightly lower ( 61% vs 67% compared with stenting ) [ 20 ]  . 
in our opinion , directional atherectomy can be proposed as the treatment of choice , especially for restenosis or stent occlusion , as an additional treatment option before referring the patient for bypass surgery . 
the stenoses / occlusions observed at 2 and 12 months in our series referred to patients with complicated , severe , lower extremity vascular disease , with high tasc category and rutherford stage . 
we decided not to start the double antiaggregant before the procedure ( it is normally administered 3 days in advance ) and to rely heavily on heparin both during the procedure and , above all , in the 2 days following it . 
un dato interessante quello che emerge dal confronto del ricorso allamputazione nei pazienti trattati , che secondo la casistica di mckinsey [ 6 ] del 7 , 6% a 18 mesi ( rispetto al 16% del dato del basil per le terapie chirurgiche ed endovascolare con angioplastica e stent ) ; dato che fa affermare allautore di ritenere che attualmente laterotomia direzionale collocabile in prima linea quale scelta terapeutica endovascolare : infatti garantisce perviet simili a quelle dello stent nel breve e medio periodo , senza tuttavia gravare con la presenza di materiale eterologo ( stent ) allinterno dellorganismo . 
laterotomia direzione si propone inoltre , a nostro avviso , soprattutto per il trattamento di scelta della restenosi o occlusione dello stent , come ulteriore prospettiva terapeutica prima di indirizzare il paziente al by - pass . 
al valido risultato potrebbe aver contribuito la gestione farmacologica del paziente , diversa rispetto alla pratica corrente : abbiamo infatti preferito non iniziare il doppio antiaggregante prima del trattamento ( di solito lo si inizia tre giorni prima ) e basarci molto sullimpiego di eparina sia durante che soprattutto nei due giorni successivi alla procedura . 
the more severe and advanced forms of lower - extremity vascular disease are faced with poor therapeutic prospects due to the extreme difficulty of any surgical approach in these patients . 
therefore , at present , screening and monitoring of lower - extremity vascular disease should be intensified to treat patients at the initial stages of disease , when optimal and lasting results can be achieved . 
 catheter directional in conclusion , in our experience , the use of the silverhawk treat atherectomy femoropopliteal stenoses / occlusions was effective and free of significant complications in all patients treated . 
questo dato negativo tuttavia comune anche alle altre tecniche endovascolari quali angioplastica e stent : le forme gravi ed avanzate di vasculopatia degli arti inferiori soffrono dunque di prospettive terapeutiche non soddisfacenti , in considerazione della estrema difficolt dellapproccio chirurgico in questi pazienti . 
allo stato quindi occorre intensificare lo screening e il monitoraggio delle vasculopatie degli arti inferiori per trattare i pazienti allo stadio pi basso della malattia , unico che garantisce ottimi risultati nel tempo . 
 in conclusione , nella nostra esperienza , limpiego dellaterotomo direzionale silverhawk in corso di steno - occlusione femoro - poplitea si dimostrato efficace e privo di complicanze degne di nota in tutti i pazienti trattati . 
sezione di diagnostica per immagini , policlinico universitario , piazza giulio cesare 11 , 70124 bari , italy 2dipartimento di anatomia patologica sezione di ematologia , 3dipartimento di anatomia patologica sezione di anatomia patologica , policlinico universitario , bari , italy correspondence to : p . 
other malignant neoplasms were found in 13 / 67 , lymphoma without subtype specification was diagnosed in 7 / 67 , whereas no conclusive diagnosis could be established in 6 / 67 cases . 
percutaneous ct - guided cnb is a safe , effective and reliable tool in the management of lymphomas in patients without superficial lymphadenopathy and can be considered an alternative approach to surgical sampling . 
nel periodo compreso fra maggio 2005 e dicembre 2008 sono state eseguite 67 cb tcguidate , di lesioni non superficiali , in 64 pazienti con sospetto linfoma ; 19 / 64 ( 29 , 7% ) con sospetto di recidiva di malattia . 
in 41 / 67 casi stata posta diagnosi di linfoma con sottotipizzazione in accordo con la classificazione world health organization ( who ) , in 13 / 67 di altra neoplasia maligna , in 7 / 67 casi di linfoma senza sottotipo ed in 6 / 67 il materiale prelevato non ha permesso una diagnosi conclusiva . 
lutilizzo della tecnica coassiale modificata proponibile poich consente di ottenere una buona accuratezza diagnostica ed una ridotta incidenza di complicanze . radiol med ( 2010 ) 115 : 12921303 1293 keywords lymphoma ct - guided biopsy coaxial core biopsy computed tomography parole chiave linfoma biopsia tc - guidata tecnica coassiale tomografia computerizzata introductiont introduzione percutaneous computed tomography ( ct ) - guided fineneedle aspiration biopsy ( fnab ) is a widely used procedure in the diagnosis and follow - up of neoplasms , having high accuracy values ranging from 80% to 93% and a low complication rate [ 13 ]  . 
correct diagnosis of lymphoma requires , in addition to a morphological study , immunohistochemical and molecular analyses to define the exact histological type and , on this basis , establish the best therapeutic approach and prognostic significance [ 7 ]  . 
in patients with a clinical suspicion of lymphoma , in the absence of superficial lesions , the diagnosis may prove difficult , and additional mediastinoscopy or laparoscopy may be needed , which are occasionally associated with morbidity and , less frequently , with mortality . 
the aim of our study was to verify the effectiveness of ct - guided cnb performed with a modified coaxial technique in a group of patients with suspected lymphoproliferative disease . materials and methods between may 2005 and december 2008 , 64 patients ( 38 women and 26 men , age range 2185 years , mean 61 ) with a clinical suspicion of lymphoma ( 45 at first presentation and 19 with suspected recurrence ) underwent ct - guided cnb of deep - seated lesions . 
before the biopsy , signed , written informed consent was obtained from all patients . prothrombin time ( pt ) , partial thromboplastin time ( ptt ) and platelet count ( plt ) were measured . 
the contrastenhanced ct scans were preliminarily assessed to determine site , presence of necrotic areas and anatomical tramite lagobiopsia percutanea guidata tomografia computerizzata ( tc ) una procedura ampiamente utilizzata nella diagnosi e nel follow - up delle neoplasie , con valori elevati di accuratezza compresi tra l80% ed il 93% e con scarsa incidenza di complicanze [ 13 ]  . 
per una corretta diagnosi di linfoma necessario eseguire oltre ad esami morfologici , anche indagini immunoistochimiche e molecolari che permettano di differenziare istotipi diversi , con differenti fattori prognostici e consentano di scegliere il miglior approccio terapeutico [ 7 ]  . 
nei pazienti con sospetto clinico di linfoma , in assenza di lesioni superficiali , la diagnosi pu risultare difficile e pu essere necessario il ricorso a mediastinoscopia o a laparoscopia , occasionalmente associate a morbilit e pi raramente a mortalit . 
sono state eseguite complessivamente 67 cb poich tre soggetti sono andati incontro alla ripetizione , a distanza di tempo , della procedura bioptica in conseguenza di un primo prelievo non idoneo . 
prima di eseguire lesame bioptico , da tutti i pazienti stato ottenuto consenso informato scritto e sono stati esaminati il tempo di protrombina ( pt ) , il tempo parziale di tromboplastina 1294 radiol med ( 2010 ) 115 : 12921303 relationships between lesions so as to select lesions to be sampled , best patient position , access site and safest needle path . 
immediately before the biopsy , scans were obtained of the area of interest , with anatomical landmarks placed on the skin surface using an mdct scanner ( mx 8000 , philips medical systems , eindhoven , the netherlands ) to determine the distance and angle of the needle in relation to the target . 
we used semiautomatic guillotine - type cutting needles , ranging from 20 to 18 gauge in diameter and 100 to 200 mm in length ( precisa , hs hospital service , aprilia , italy ) , depending on lesion location and size and the patients habitus . 
to facilitate multiple sampling , a modified coaxial technique was used that involves the introduction of a cutting needle sheathed in a 6 - cm plastic cannula after administration of locoregional anaesthesia [ 10 ml lidocaine hydrochloric acid ( hcl ) 2% ]  . 
specimens were fixed in formaldehyde ( 40 g / l ) , embedded in paraffin and stained with haematoxylineosin . immunohistochemical studies were performed using antibodies directed against common leukocyte antigen , cytokeratin and viment histological subtyping was obtained using monoclonal antibodies against the following antigens : cd3 , cd4 , cd5 , cd8 , cd10 , cd15 , cd20 , cd23 , cd30 , cd45 , cd56 , cd68 , cd79a , alk , bcl2 , bcl6 , ki67 and cyclin d1 . 
in agreement with other authors , we considered complete success as all cases in which the biopsy provided adequate material to establish a diagnosis of lymphoma , with specification of histological subtyping or a diagnosis of other disease ; partial success if the material obtained enabled a diagnosis of malignant lymphoma without specification of a definite histological type ; and failure if the material sampled was nondiagnostic [ 7 , 9 ]  . 
to measure diagnostic accuracy , we considered the cases of complete success in relation to the total number of cnb performed . results sixty - four patients with a clinical suspicion or recurrence of lymphoma in the absence of superficial localisations ( ptt ) e la conta piastrinica ( plt )  . 
preliminarmente stato valutato lesame tc con mezzo di contrasto ( mdc ) per determinare la sede , la eventuale presenza di aree necrotiche ed i rapporti anatomici delle lesioni al fine di scegliere quali lesioni bioptizzare , il decubito ottimale del paziente , il sito di accesso ed il percorso pi sicuro dellago . 
immediatamente prima della biopsia , utilizzando unapparecchiatura tc multidetettore ( tcmd ) ( mx 8000 , philips medical systems , eindhoven , olanda ) sono state eseguite scansioni dellarea di interesse , con repere sulla superficie cutanea , per determinare distanza e angolazione dellago rispetto al bersaglio . 
sono stati utilizzati aghi trancianti semiautomatici a ghigliottina , di calibro compreso tra 20 e 18 gauge , della lunghezza da 100 a 200 mm ( precisa , hs hospital service , aprilia , italia ) a seconda della sede , delle dimensioni delle lesioni e dellhabitus dei pazienti . 
per facilitare prelievi multipli , stata adottata una tecnica coassiale modificata che prevede , dopo anestesia locoregionale ( 10 ml di lidocaina hcl 2% ) , lintroduzione dellago tranciante inguainato in una cannula di plastica della lunghezza di 6 cdopo aver verificato il corretto posizionamento della punta dellago mediante scansioni tc seriate ( thickness : 3 mm , increment : 3 mm , pitch : 1 , 25 , rotation time : 0 , 5 s , kvp : 120 , mas : 250 ) , la cannula di plastica stata spinta il pi possibile in profondit e lasciata in tale sede dopo il primo prelievo bioptico , per essere utilizzata come guida per le biopsie successive , al fine di ottenere almeno tre frustoli integri della lunghezza minima di 1 cin tutti i casi la procedura stata portata a termine correttamente ( durata media 25 min )  . 
immediatamente dopo i prelievi bioptici , un controllo tc stato eseguito al fine di valutare le possibili complicanze e tutti i pazienti sono stati sottoposti a monitoraggio clinico per un periodo minimo di 24 ore . 
la sottotipizzazione istologica dei linfomi stata ottenuta utilizzando anticorpi monoclonali verso gli antigeni : cd3 , cd4 , cd5 , cd8 , cd10 , cd15 , cd20 , cd23 , cd30 , cd45 , cd56 , cd68 , cd79a , alk , bcl2 , bcl6 , ki67 , ciclica d1 . 
in patients with a definite diagnosis of non - hodgkins lymphoma ( nhl ) , diagnostic accuracy reached 80.4% , whereas in those with a diagnosis of hodgkins lymphoma ( hl ) , it was 50% . 
five cases underwent subsequent intraoperative biopsy , whereas two cases underwent repeat cnb ( with complete success in one case and failed biopsy in another , which was followed by laparoscopy with definite diagnosis ) ( table 3 )  . 
in 6 / 67 cnb ( 9% ) , the material sampled from retroperitoneal lymph nodes ( three cases ) , mesenteric lymph nodes ( two cases ) and liver parenchyma ( one case ) did not yield a conclusive diagnosis ( biopsy failure ) ( table 4 )  . 
nei pazienti con diagnosi definitiva di linfoma non hodgkin ( lnh ) laccuratezza diagnostica stata dell80 , 4% mentre in quelli con diagnosi di linfoma hodgkin ( lh ) stata del 50% . 
in 5 casi stata successivamente eseguita biopsia intraoperatoria ; mentre in due la cb stata ripetuta ( in un caso con successo completo , nellaltro con insuccesso e successiva laparoscopia con diagnosi definitiva ) ( tabella 3 )  . 
in 6 / 67 cb ( 9% ) il materiale prelevato da linfonodi retroperitoneali ( 3 casi ) , linfonodi mesenterici ( 2 casi ) e parenchima epatico ( 1 caso ) non ha consentito di ottenere una diagnosi conclusiva ( insuccesso ) ( tabella 4 )  . 
dei tre pazienti con linfoadenopatie retroperitoneali , uno ha ripetuto la cb con successo parziale ( sospetto lh ) e diagnosi definitiva di lh scleronodulare , ottenuta dopo laparoscopia ; un altro stato sottoposto a laparotomia con diagnosi definitiva di metastasi da seminoma ; mentre un paziente con pregressa diagnosi di lnh follicolare , ha rifiutato ogni ulteriore procedura bioptica ed stato trattato sulla base della pregressa diagnosi con remissione completa di malattia . dei due pazienti con linfoadenopatie mesenteriche , in entrambi i casi stata effettuata laparoscopia con diagnosi definitiva di lnh diffuso a grandi cellule b e di lnh linfoplasmocitico . 
biopsy failure was recorded in one case only ( 5.3% ) ( table 5 )  . discussion lymphomas are malignancies characterised by the clonal expansion of lymphoid cells in different stages of differentiation . 
in the diagnosis of lymphoma , distinct disease entities with distinct morphological , clinical , phenotypic and molecular features diciannove pazienti della nostra serie si presentavano gi con una pregressa diagnosi di linfoma e sospetto di recidiva . 
nella diagnosi di linfoma necessario riconoscere distinte entit patologiche con caratteri morfologici , clinici , fenotipici e molecolari tali da permettere la scelta terapeutica pi adeguata e una previsione prognostica [ 10 ]  . 
la scelta terapeutica infatti pu variare dalla semplice osservazione nei lnh a basso grado di malignit fino alle chemioterapie ad alte dosi con la reinfusione delle cellule staminali emopoietiche nei lnh ad alto grado [ 11 ]  . 
b laparoscopia lnh follicolare lnh mantellare sospetto linfoma laparotomia lh scleronodulare cb , core biopsy ; lnh , linfoma non hodgkin ; lh , linfoma hodgkin undergo histological re - evaluation to assess response to therapy , histological progression or the presence of concurrent disease [ 12 ]  . 
in caso di assenza di linfoadenopatie superficiali , in alternativa allintervento chirurgico pu essere utilizzata lago - biopsia tc guidata , caratterizzata da minore invasivit , minimo rischio anestesiologico , ridotti tempi di ospedalizzazione , costi inferiori , minore incidenza di complicanze e mortalit [ 14 , 15 ]  . la cito - aspirazione con ago sottile ( fnac ) , una procedura veloce , poco invasiva ed economica ; tuttavia il suo ruolo nellidentificazione di malattie linfoproliferative resta controverso [ 16 ]  . 
previous studies have widely demonstrated the superiority of cnb compared with fnab [ 1719 ] , with reported diagnostic accuracy values for cnb in the diagnosis of lymphomas ranging from 72% to 89% [ 7 , 9 , 13 , 2025 ] , and these findings have , in part , led to a change in the diagnostic approach to these diseases . cnb performed with 14to 20 - gauge cutting needles a modificare liter diagnostico di tali patologie . 
 infatti la cb , con aghi trancianti da 1420 g , consente di prelevare una quantit di tessuto sufficiente per eseguire tutte le indagini immunoistochimiche necessarie per unadeguata diagnosi di linfoma [ 15 ]  . 
lo svantaggio di tale tecnica rappresentato dalla presenza di una cannula esterna che radiol med ( 2010 ) 115 : 12921303 1301 yields enough sampling tissue to perform all immunohistochemical studies necessary for accurate diagnosis of lymphoma [ 15 ]  . 
the disadvantage of this technique is the presence of an external cannula that increases the total diameter of the biopsy system , leading to a higher risk of complications [ 26 , 27 ]  . 
in our series , especially in patients with access points that were difficult to reach and / or in close proximity to vascular structures , the modified coaxial technique allowed us to easily obtain multiple specimens . 
another advantage is the ease with which small changes can be made in the angle of the introducing cannula to obtain a larger sampling area . cnb performed with this technique was well tolerated by most patients and was completed according to the established protocol in all cases . in our study , a small number of biopsies was performed and , independent of size , lesins were all deep - seated . 
this value , which needs to be confirmed on a larger patient population , is in line with the values reported in other series , some of which , however , also included biopsies of superficial lesions [ 7 , 9 , 13 , 2025 ]  . after extrapolating from our series the cases with a final diagnosis of lymphoma , the diagnostic accuracy of cnb in these patients was 75.9% and , in particular , in patients with a definite diagnosis of nhl , it was 80.4%. 
this latter result is probably related to the peculiar histological features of hl , which has a reactive lymphocyte population sometimes associated with sclerotic tissue ( scleronodular type )  . 
in these cases , larger tissue samples are needed to establish the histological diagnosis . however , the limited number of hl patients in our series reduces the reliability of this finding , which requires further validation . in the group of patients with a previous diagnosis of malignant lymphoma and suspected disease recurrence , the previous diagnosis was confirmed in 42.1% , cnb failed to yield a definite histological diagnosis due to colliquative material in 5.3% , histological progression of lymphoma was documented in 31.6% and a different disease was diagnosed in 21% . 
in two patients with partial success , cnb was repeated , leading to a diagnosis of follicular nhl in one case only . aumenta il diametro globale del sistema bioptico con incremento del rischio di complicanze [ 26 , 27 ]  . 
nel nostro caso , soprattutto nei pazienti che prevedevano sedi di biopsia di difficile accesso e / o in stretto rapporto con strutture vascolari , la tecnica coassiale modificata , ha permesso di ottenere agevolmente multipli prelievi . 
la cb eseguita con tale tecnica stata ben tollerata dalla maggior parte dei pazienti e comunque in tutti i casi stata portata a termine secondo il protocollo stabilito . nel nostro studio costituito da un limitato numero di biopsie , indipendentemente dalle dimensioni delle lesioni , tutte localizzate in sedi profonde , utilizzando la tecnica coassiale modificata , laccuratezza diagnostica risultata dell80 , 1% . 
tale valore , che necessita di conferma su un campione pi ampio di pazienti , in media con quelli riportati da altri autori , alcuni dei quali tuttavia hanno incluso nelle loro casistiche anche biopsie di lesioni localizzate in sede superficiale [ 7 , 9 , 13 , 2025 ]  . estrapolando dalla nostra serie i casi con diagnosi finale di linfoma , laccuratezza diagnostica della cb in questi pazienti stata del 75 , 9% ed in particolare nei pazienti con diagnosi definitiva di lnh risultata pari all80 , 4% mentre in quelli con diagnosi di lh stata del 50% . 
questultimo risultato probabilmente da mettere in relazione alle particolari caratteristiche istologiche del lh che presenta una popolazione linfocitaria reattiva associata a volte a tessuto sclerotico ( variante sclero - nodulare ) , con necessit di pi abbondante materiale per la diagnosi istologica ; tuttavia lo scarso numero dei pazienti con lh della nostra casistica riduce lattendibilit di questo dato che necessita di ulteriori conferme . 
 nel gruppo dei pazienti con pregressa diagnosi di linfoma maligno e sospetta recidiva di malattia , nel 42 , 1% stata confermata la precedente diagnosi , nel 5 , 3% la cb non ha consentito di giungere ad una diagnosi istologica definitiva per presenza di materiale colliquato mentre nel 31 , 6% dei casi stata documentata una progressione istologica del linfoma e nel 21% dei casi stata formulata diagnosi di una nuova patologia . 
questi ultimi due valori confermano quanto gi dimostrato in letteratura circa la necessit di effettuare una rivalutazione istologica in particolari condizioni cliniche nel decorso delle malattie linfoproliferative [ 7 ]  . nel 10 , 4% dei casi si ottenuto un successo parziale con diagnosi di sospetta sindrome linfoproliferativa a cellule b ( 57% ) , di sospetta sindrome linfoproliferativa a cellule t ( 28 , 6% ) e di sospetto linfoma ( 14 , 3% )  . 
it should be emphasized that the inability to diagnose malignant lymphomas with specification of subtype according to the who classification is probably not to be ascribed to the biopsy technique , but rather to the typical features of pathological lymphatic tissue itself ; in fact , in some cases , a great variety of neoplastic tissues coexist with reactive cells , whereas in other cases , the entire lymph node architecture needs to be studied to reach a diagnosis . 
 although cnb is less accurate than excisional biopsy of the entire lymph node , especially when using a modified coaxial technique , it is undoubtedly less invasive and much less expensive than intraoperative biopsy , which requires general anaesthesia and several days in hospital [ 14 , 20 , 21 ]  . cnb may therefore be considered a valuable alternative to surgical intervention , above all in patients in poor clinical condition at high anaesthetic risk [ 25 ]  . pazienti la diagnosi definitiva stata ottenuta mediante biopsia intraoperatoria . 
da sottolineare che limpossibilit di diagnosticare i linfomi maligni , con sottotipizzazione in accordo con la classificazione who , non probabilmente da attribuire alla tecnica bioptica utilizzata , ma piuttosto alle caratteristiche proprie del tessuto patologico di origine linfatica infatti , in alcuni casi coesiste una grande variet di tessuto neoplastico associato alla presenza di cellule reattive , mentre in altri necessario studiare tutta larchitettura linfonodale per giungere alla diagnosi . 
nel 9% dei casi si ottenuto un insuccesso perch il materiale prelevato risultato insufficiente o colliquato e le diagnosi definitive sono state ottenute mediante biopsia intraoperatoria . sebbene la cb sia meno accurata della biopsia escissionale dellintero linfonodo , soprattutto utilizzando una tecnica coassiale modificata , innegabile che sia meno invasiva , molto pi economica di una biopsia intraoperatoria che necessita di anestesia generale e alcuni giorni di ricovero ospedaliero [ 14 , 20 , 21 ] e quindi pu essere considerata valida alternativa allintervento chirurgico , specialmente nei pazienti in condizioni cliniche non ottimali e con elevato rischio anestesiologico [ 25 ]  . 
in assenza di linfoadenopatie superficiali costituisce una valida alternativa allintervento chirurgico come primo step diagnostico nei pazienti con sospetto linfoma . tale metodica utile anche nella gestione dei pazienti con pregressa diagnosi di linfoma e sospetta progressione di malattia o con lesioni profonde sospette per differenti patologie . 
morgagni 85 , 50134 florence , italy 2radiology unit , institute for cancer research and treatment , strada provinciale 142 km 3 , 95 , 10060 candiolo , turin , italy 3cancer prevention and research institute ( ispo ) , via cosimo il vecchio 2 , 50139 florence , italy correspondence to : l . 
sali , tel : + 39 - 055 - 4377673 , fax : + 39 - 055 - 431970 , e - mail : lapo.sali@unifi.it received : 23 september 2009 / accepted : 6 november 2009 / published online : 2 august 2010 springer - verlag 2010 abstract purpose . 
settantanove soggetti fobt positivi del programma di screening della regione toscana sono stati invitati ad eseguire nello stesso giorno la ctc e la co dopo preparazione intestinale standard ( polietilenglicole )  . 
nel contesto di un programma di screening basato sul fobt , la ctc ha mostrato elevata sensibilit ma bassi valori di specificit e valore predittivo positivo . probabilmente utilizzare la ctc come test di secondo livello nei soggetti fobt positivi non una strategia costo - efficace . 1268 radiol med ( 2010 ) 115 : 12671278 keywords computed tomography colonography faecal occult blood test colorectal cancer screening parole chiave colongrafia tc test del sangue occulto fecale screening del cancro colorettale introduction introduzione randomized clinical trials have demonstrated that screening with faecal occult blood test ( fobt ) reduces mortality for colorectal cancer ( crc ) [ 1 ]  . 
accordingly , population - based screening with fobt is currently recommended by european community health associations and has been applied in many countries , including italy [ 2 ]  . 
this means that a proportion of subjects at risk of having significant colonic lesions is potentially precluded from prompt diagnosis and treatment . in this setting computed tomography colonography ( ctc ) could be employed before endoscopy in order to enhance attendance to a pan - colonic examination . 
hence about half of the faecal tests are false positive , leading to unnecessary colonoscopies in asymptomatic subjects . we report a preliminary evaluation of the performance of ctc systematically obtained before optical colonoscopy ( oc ) in subjects with positive fobt in the context of a population - based screening programme for crc . 
subjects were selected from a list of individuals with positive fobt who were scheduled for studi clinici randomizzati hanno dimostrato che lo screening con il test del sangue occulto fecale ( fobt ) riduce la mortalit per il cancro colo - rettale ( crc ) [ 1 ]  . 
i programmi di screening di popolazione basati sul fobt sono attualmente raccomandati dalle principali associazioni sanitarie della comunit europea e vengono applicati in diversi paesi , inclusa litalia [ 2 ]  . 
in questo contesto la colongrafia tc ( ctc ) potrebbe essere impiegata nei soggetti fobt positivi , prima della colonscopia ottica ( co ) , al fine di incrementare il tasso di adesione ad un esame panesplorante del colon . daltra parte il valore predittivo positivo del fobt immunochimico per ladenoma avanzato ed il cancro varia in differenti contesti dal 38 , 9% al 51 , 8% [ 3 , 4 ]  . 
ne consegue che circa la met dei test del sangue occulto fecale sono falsi positivi , il che comporta lesecuzione di colonscopie non necessarie in soggetti asintomatici . scopo dello studio una valutazione preliminare della performance della ctc effettuata sistematicamente prima della colonscopia convenzionale in soggetti con fobt positivo nel contesto di un programma di screening di popolazione per il cancro colo - rettale . 
esso rivolto a tutti i residenti con et compresa tra i 50 e i 70 anni che vengono invitati ogni due anni , tramite lettera postale , a sottoporsi al fobt immunochimico . 
coloro che risultano negativi vengono invitati , sempre tramite posta , a ripetere il test di screening dopo radiol med ( 2010 ) 115 : 12671278 1269 colonoscopy from march 2008 to march 2009 . 
subjects with the following conditions had previously been excluded by matching with the screening programme archive : personal history of crc or adenoma ; a total colonoscopy performed in the previous 5 years ; diagnosis of inflammatory bowel disease . 
from the list of subjects with positive fobt waiting for endoscopy 79 consecutive individuals ( 44 males , 35 females ) were contacted telephonically by a radiology resident and were asked to perform same day ctc and oc . 
bowel preparation was obtained with 4 l of a polyethyleneglycole solution ( isocolan , giuliani , milan , italy ) administered the day before the procedure and a low residue diet for 3 days . ct colonography all subjects , except those with contraindications , received intravenously 30 mg of scopolamine butylbromid ( buscopan ; boehringer ingelheim , florence , italy ) before colonic insufflation . 
the subjects were placed on ct table on the right lateral decubitus and a 24 fr rubber catheter , foley type , with a small retention balloon ( 10 ml ) was inserted into the rectu after catheter positioning the subject was turned in supine position and colonic distension was obtained with manual insufflation of room air performed by a radiology resident . 
colonic distension was evaluated with an anteriorposterior ct scout view in both supine and prone position , and additional air was inflated using a manual bulb if distension was unsatisfactory . 
 ctc was performed with a 16 - mdct scanner ( sensation 16 ; siemens , erlangen , germany ) using a detector configuration of 160.75 mm , 120 kvp , 50 effective mas , tube rotation time of 500 ms and a pitch of 1.25. 
data were reconstructed using a slice thickness of 1 mm with a reconstruction increment of 1 meffective dose was estimated . for each acquisition ctdivol was 4.15 mgy with a calculated effective dose of 3.5 msv for females and 2.7 msv for males ( ct patient dosimetry calculator , impact ; measures executed on montecarlo phantom )  . 
i soggetti con fobt positivo sono invece invitati a sottoporsi alla colonscopia [ 5 ]  . il nostro studio si svolto nel comune di firenze , nellambito del programma regionale per lo screening del tumore del colon - retto . 
erano stati precedentemente esclusi , in base ai registri del programma di screening , i soggetti che presentavano le seguenti condizioni : storia personale di crc o adenoma ; pancolonscopia effettuata nei 5 anni precedenti ; diagnosi di malattia infiammatoria cronica intestinale . 
dalla lista dei soggetti fobt positivi in attesa della colonscopia , 79 individui consecutivi ( 44 maschi e 35 femmine ) sono stati contattati telefonicamente da uno specializzando in radiodiagnostica , spiegando loro il motivo dello studio , e chiedendo se erano disposti ad effettuare la ctc lo stesso giorno della colonscopia . 
i pazienti sono stati informati che il risultato della ctc non avrebbe influito sulla successiva esecuzione o meno della colonscopia . tutti i pazienti che hanno aderito allo studio si sono sottoposti nella stessa giornata alla ctc ed alla co . 
la preparazione intestinale stata ottenuta mediante somministrazione di 4 l di una soluzione di polietilenglicole ( isocolan ; giuliani , milano ) il giorno prima dellesame associata ad una dieta a basso contenuto di scorie nei 3 giorni precedenti . colongrafia tc prima di effettuare lo pneumocolon ad ogni paziente sono stati somministrati per via endovenosa 30 mg di butilbromuro di scopolamina ( buscopan ; boehringer ingelheim , firenze , italia ) , salvo controindicazioni . 
i soggetti sono stati posizionati sul tavolo tc in decubito laterale destro ed stato inserito nel retto un catetere tipo foley 24 fr . successivamente i soggetti sono stai posti in decubito supino ed stato effettuato lo pneumocolon mediante insufflazione manuale di aria ambiente eseguita da uno specialiazzando . 
prima di effettuare ciascuna scansione , sono state acquisite immagini di scout view antero - posteriore nei due decubiti per valutare il grado di distensione del colon e , qualora questo non fosse soddisfacente , ulteriore aria stata insufflata manualmente . 
non stato usato mezzo di contrasto per via endovenosa . 1270 radiol med ( 2010 ) 115 : 12671278 workstation ( cad - colon ; im3d , turin , italy )  . 
he was assisted by one of two radiology residents who annotated the ctc findings and then followed subject to the endoscopy roothe computer aided detection ( cad ) system embedded in the workstation software was not used for this study . 
the colon was divided into six segments : caecum , ascending , transverse , descending , sigmoid and rectum ( the different segments were evaluated both in supine and prone acquisitions )  . 
 ctcs were evaluated with a primary 2 - dimensional approach , using 3 - dimensional images for problem solving . all lesions detected at ctc were localized according to their segmental location in the colon . 
each lesion was measured taking into account of its maximum diameter on 2 - dimensional images viewed with a bone window ( level 400 hu , width 2000 hu )  . 
after the endoscopist had completed the evaluation of each segment of the colon , he was provided the ctc results for that segment by the radiology resident before beginning the evaluation of the next colonic segment . 
 one hour after colonoscopy a radiology resident administered a questionnaire to all subjects that investigated tolerance for ctc , colonoscopy and bowel preparation which was assessed using a visual analogue scale ( vas ) ( 0 = no discomfort , 10 = extreme discomfort )  . 
subjects were also asked to state their preferred screening examination ( colonoscopy every 10 years , ctc every 5 years or fobt every 2 years )  . tutti gli esami sono stati eseguiti con tc multistrato a 16 corone di detettori ( siemens sensation 16 , erlangen , germania ) utilizzanodo una collimazione di 160 , 75 mm , 120 kvp , 50 eff . 
mas , pitch 1 , 25 e tempo di rotazione 0 , 5 s . sono state ricostruite sezioni di 1 mm con intervallo di ricostruzione di 1 mla dose equivalente per singola acquisizione risultata di 2 , 7 msv per i maschi e di 3 , 5 msv per le femmine con un ctdivol di 4 , 15 mgy ( ct patient dosimetry calculator , impact ; misure effettuate su fantoccio montecarlo )  . le immagini di ogni paziente sono state trasferite su una workstation con software dedicato ( cad - colon ; im3d , torino )  . 
tutti gli esami sono stati interpretati da un unico radiologo ( l.s. ) con precedente esperienza di lettura di almeno 100 ctc , con lassistenza di uno specializzando che annotava i risultati e successivamente seguiva il soggetto nella sala endoscopica . 
la funzione cad ( computer aided detection ) che permette un rilevamento automatico delle lesioni polipoidi , integrata nel software , non stata usata per questo studio . preliminarmente stata valutata sulle immagini assiali la percentuale di mucosa visibile del colon . 
la percentuale di superficie mucosa visibile stata valutata tramite un sistema a quattro categorie ( pi dell80% di mucosa visibile , 5080% , 2050% , meno del 20% ) , e per ogni esame , in caso di incompleta visualizzazione , stata riportata la causa ( residui fecali , residui liquidi , spasmo colico )  . per linterpretazione degli esami stato utilizzato un approccio primary 2 - dimensional , utilizzando le immagini tridimensionali per il problem solving . 
ogni lesione rilevata alla ctc stata classificata in base alla sede ( seguendo la divisione del colon in segmenti ) ed alle dimensioni , misurandone il diametro massimo nelle immagini bidimensionali con finestra per osso ( livello 400 uh , ampiezza 2000 uh )  . 
 colonoscopia a distanza di 24 ore dalla ctc i soggetti sono stati sottoposti alla colonscopia ottica , eseguita con o senza sedazione , da uno di due gastroenterologi con particolare esperienza nello screening del tumore colo - rettale ( agb e gc )  . stato utilizzato il metodo del segmental unblinding . 
advanced adenoma was defined as any adenoma measuring at least 10 mm in diameter or having a villous component of at least 25% , or demonstrating high - grade dysplasia . 
a patient was considered positive at reference standard if unblinded colonoscopy depicted at least one cancer or one adenoma measuring 6 m when a patient had more lesions , the one with the worst histology was considered as index lesion . 
on the other hand , ctc was regarded as a false positive if it detected a lesion of at least 6 mm and reference standard was negative . sensitivity , specificity , npv and ppv were calculated with a 95% confidence interval . results forty - nine of 79 subjects ( 62% ) with positive fobt accepted to participate to the study . 
incomplete visualization was mainly due to liquid residues ( liquid residues n = 31 , faecal residues n = 4 , spasm n = 5 )  . distribution , histological type , and size of the lesions found on colonoscopy are listed in table 1 . 
the classification of patients 1271 dopo che lendoscopista aveva completato la valutazione di un segmento , prima di procedere con il successivo , veniva informato dei risultati della ctc per quel segmento . 
 stato anche chiesto ai pazienti di esprimere una preferenza riguardo allesame di screening ( colonscopia ottica ogni 10 anni , ctc ogni 5 anni , fobt ogni 2 anni )  . analisi statistica il risultato finale della colonscopia eseguita con la tecnica del segmental unblinding e listologia delle lesioni rimosse hanno costituito lo standard di riferimento per la valutazione della performance della ctc . 
le lesioni di interesse dello studio sono state carcinomi e polipi adenomatosi con diametro massimo di almeno 6 m stato definito adenoma avanzato ogni lesione adenomatosa che presentasse almeno una delle seguenti caratteristiche : diametro massimo di 10 mm e oltre ; presenza allesame istologico di almeno il 25% di componente villosa ; presenza di aree di displasia di alto grado . stata effettuata unanalisi per - paziente per - adenoma . i pazienti sono stati considerati positivi allo standard di riferimento quando la colonscopia unblinded ha rilevato la presenza di almeno una lesione cancerigna o adenomatosa con diametro di 6 mm ed oltre . 
sono stati considerati negativi quei pazienti in cui la colonscopia non ha rilevato alcuna lesione e quelli in cui sono stati rinvenute lesioni polipoidi non adenomatose o con diametro massimo inferiore ai 6 m la ctc stata considerata positiva quando ha rilevato almeno una lesione con diametro di 6 mm ed oltre , e negativa quando non ha riscontrato alcuna lesione di almeno 6 m di conseguenza , il risultato della ctc stato classificato come vero positivo quando la ctc era positiva e la lesione indice era un adenoma di almeno 6 mm , mentre stato classificato come falso positivo quando la ctc aveva identificato una lesione di almeno 6 mm ma lo standard di riferimento era negativo . 
sono stati calcolati sensibilit , specificit , valore predittivo negativo e valore predittivo positivo , con un intervallo di confidenza del 95% . 1272 radiol med ( 2010 ) 115 : 12671278 table 1 histology , location and size of lesions detected on optical colonoscopy according to location location and histology size < 6 mm ( n = 17 ) 69 mm ( n = 19 ) 10 mm ( n = 19 ) total ( n = 55 ) rectum hyperplastic polyp adenoma advanced adenoma cancer sigmoid colon hyperplastic polyp adenoma advanced adenoma cancer descending colon hyperplastic polyp adenoma advanced adenoma transverse colon hyperplastic polyp adenoma advanced adenoma ascending colon adenoma advanced adenoma not retrieved caecum adenoma other total hyperplastic polyp adenoma advanced adenoma cancer other not retrieved according to the index lesion is reported in table 2 . 
moreover among these 22 patients 14 had at least an advanced adenoma . ct performance in detecting cancer or adenoma of at least 6 mm on a patient basis is reported in table 3 . 
sensitivity stratified according to index lesion size was 91.7% ( 95% ci : 61.5%99.8% ) for adenomas of at least 10 mm and 100% ( 95% ci : 68.8%100% ) for adenomas of 69 manalysis of false positive results is showed in table 4 . 
three adenomas measuring 10 mm or more were missed on ctc . two were pedunculated polyps of the sigmoid colon completely submerged under air - fluid levels in both supine risultati quarantanove soggetti dei 79 contattati con fobt positivo ( 62% ) hanno accettato di partecipare allo studio . 
il 95 , 5% dei partecipanti non aveva alcun altro fattore di rischio per il tumore del colon - retto allinfuori dellet ; due soggetti ( 4 , 5% ) presentavano una storia familiare di tumore del colon - retto in un parente di primo grado . 
tutti i partecipanti hanno completato sia la ctc che la colonscopia ottica . alla ctc la visibilit della mucosa colica risultata ottimale ( > 80% in tutti i segmenti colici ) in 9 soggetti e buona ma sub - ottimale ( almeno un segmento con percentuale di mucosa visibile compresa tra il 50% e 80% ) in 36 soggetti . tre soggetti avevano almeno un segmento con visibilit compresa tra il 20% ed il 50 % ed uno almeno un segmento radiol med ( 2010 ) 115 : 12671278 1273 tabella 1 istologia , dimensione e sede delle lesioni identificate alla colonscopia < 6 mm ( n = 17 ) 69 mm ( n = 19 ) 10 mm ( n = 19 ) totale ( n = 55 ) dimensione sede e istologia retto polipo iperplastico adenoma adenoma avanzato cancro colon sigmoideo polipo iperplastico adenoma adenoma avanzato cancro colon discendente polipo iperplastico adenoma adenoma avanzato colon trasverso polipo iperplastico adenoma adenoma avanzato colon ascendente adenoma adenoma avanzato non recuperato cieco adenoma altro totale polipo iperplastico adenoma adenoma avanzato cancro altro non recuperato 10 and prone ctc acquisitions . 
ctc depicted one advanced adenoma of the distal rectum ( 11 mm ) that was missed on oc before unblinding . all subjects but one reported complete adherence to bowel preparation . 
overall , subjects reported greater discomfort due to bowel preparation ( average vas score = 6.022.80 ) than that experienced during ctc ( average vas score = 2.942.13 ) or colonoscopy ( average vas score = 3.272.65 ) , which were similarly tolerated . 
lincompleta visualizzazione stata determinata principalmente da residui liquidi ( residui liquidi n = 31 , residui fecali n = 4 , spasmo colico n = 5 )  . la sede , listologia e le dimensioni delle lesioni rilevate alla colonscopia sono elencate nella tabella 1 . 
inoltre 14 pazienti tra questi 22 presentavano almeno un adenoma avanzato . la performance della ctc per - paziente nel rilievo di cancri o adenomi di almeno 6 mm riportata nella tabella 3 . 
supine ( a ) and prone ( b ) ct axial images show a small protruding lesion ( box ) of the distal rectu ( c ) endoluminal 3 - dimensional reconstruction from ctc depicts a slightly elevated lesion of the rectal wall . 
la sensibilit in base alle dimensioni della lesione indice stata del 91 , 7% ( ic 95% : 61 , 5%99 , 8% ) per adenomi di almeno 10 mm e del 100% ( ic 95% : 68 , 8%100% ) per adenomi di 6 - 9 mlanalisi dei falsi positivi viene mostrata nella tabella 4 . 
la ctc ha rilevato un adenoma avanzato del retto distale di 11 mm che non era radiol med ( 2010 ) 115 : 12671278 1275 table 2 classification of individuals according to index lesion stato identificato alla co prima dellunblinding . index lesion subjects n = 49 subjects n = 49 cancer advanced adenoma 10 mm advanced adenoma 69 mm adenoma 69 mm hyperplastic polyp 10 mm hyperplastic polyp 69 mm no lesions 6 mm tabella 2 classificazione dei soggetti in base alla lesione indice lesione indice soggetti ( n = 49 ) soggetti ( n = 49 ) cancro adenoma avanzato 10 mm adenoma avanzato 69 mm adenoma 69 mm polipo iperplastico 10 mm polipo iperplastico 69 mm nessuna lesione 6 mm 12 2 1 tutti i soggetti eccetto uno hanno dichiarato di avere assunto in modo completo la preparazione intestinale . 
i soggetti hanno riferito maggiore discomfort nei confronti della preparazione intestinale ( punteggio vas medio : 6 , 022 , 80 ) , piuttosto che nella effettuazione degli esami di ctc ( vas medio : 2 , 942 , 13 ) o di colonscopia ottica ( vas medio : 3 , 27 2 , 65 ) , i quali sono stati tollerati in modo simile . 
per quanto riguarda il test di screening preferito , la maggior parte dei soggetti ha espresso la propria preferenza per il fobt ogni 2 anni ( 38 , 8% ) e per la ctc ogni 5 anni ( 36 , 7% ) , piuttosto che per la colonscopia ottica ogni 10 anni ( 24 , 5% )  . discussione implied a lower performance of ctc [ 6 ] , but permitted to maintain our usual schedule for colonoscopy . study participation was quite high ( 62% )  . 
third , the telephone conversation with a radiology resident explaining the aim of questo studio preliminare valuta limpiego della ctc come test di secondo livello in soggetti con fobt positivo nel contesto del programma di screening per il tumore colorettale della regione toscana . 
per non modificare il protocollo di screening prestabilito , il campione di individui per questo studio stato selezionato tra soggetti fobt positivi che avevano gi acconsentito di sottoporsi allesame endoscopico . 
almost half of the subjects composing our sample ( 44.9% ) had a cancer or an adenoma of at least 6 m in particular 14 patients had at least an advanced adenoma . 
 in our study per - patient sensitivity of ctc for cancer and adenoma of at least 6 mm was higher , while specificity and ppv were lower with respect to those reported in multicentric trials on asymptomatic subjects [ 7 ] and meta - analyses [ 810 ] studies . 
although all but one subjects reported complete assumption of cathartic solution , colonic wall visualization was sub - optimal in the majority of the cases ( n = 40 )  . 
moreover , an expected high prevalence of disease in fobt positive subjects might have biased the radiologist towards false - positive reporting [ 11 ]  . in accordance with previous studies [ 12 ] , most of our patients reported discomfort for bowel preparation . 
questo probabilmente ha determinato uno scadimento della performance della ctc [ 6 ] , ma ha permesso di mantenere la programmazione abituale degli appuntamenti per lesame endoscopico . la partecipazione allo studio stata relativamente alta ( 62% ) , e questo pu essere attribuito a diverse ragioni . 
in primo luogo possibile che per i pazienti fobt positivi , e quindi con elevato rischio di essere portatori di neoplasia colo - rettale , sia stata pi rassicurante la possibilit di eseguire due esami specifici piuttosto che uno solo . 
inoltre la ctc e la colonscopia venivano eseguite nella stessa giornata a distanza di 24 ore , e ci evitava la necessit di dover ripetere la preparazione intestinale una seconda volta . 
infine , il colloquio telefonico con lo specializzando che spiegava lo scopo di questo studio potrebbe aver motivato ladesione dei soggetti . i nostri risultati hanno mostrato unalta prevalenza di lesioni adenomatose in soggetti positivi al fobt , dato in linea con la letteratura [ 3 , 4 ]  . 
quasi la met ( 44 , 9% ) dei pazienti del nostro campione aveva un cancro o un adenoma di almeno 6 m in particolare 14 pazienti avevano almeno un adenoma avanzato . nel nostro studio la sensibilit per - paziente della ctc nella detezione di cancri o adenomi di almeno 6 mm risultata superiore a quella riportata in trials multicentrici su soggetti asintomatici [ 7 ] o nelle meta - analisi [ 810 ]  . 
la specificit ed il valore predittivo positivo sono invece risultati inferiori . lanalisi dei falsi positivi ha evidenziato che la nostra specificit relativamente bassa stata determinata soprattutto dallerronea interpretazione di piccoli residui fecali come lesioni polipoidi . 
sebbene tutti i pazienti , ad eccezione di uno , abbiano riferito lassunzione completa della soluzione catartica , la visualizzazione delle mucosa colica risultata sub - ottimale nella maggior parte di casi ( n = 40 )  . 
inoltre , lalta prevalenza di malattia attesa nei soggetti fobt positivi , potrebbe aver influenzato il radiologo inducendolo a segnalare un numero maggiore di polipi [ 11 ]  . in accordo con studi precedenti [ 12 ] , la maggior parte dei soggetti ha riferito scarsa tollerabilit alla preparazione intestinale , ed il discomfort da essa provocato stato maggiore rispetto a quello percepito durante la ctc o la colonscopia . quindi probabile che , per molti soggetti , la preparazione intestinale catartica possa rappresentare il principale motivo di rifiuto a sottoporsi allo screening del cancro colo - rettale . per risolvere questo problema dovrebbe essere valutato limpiego della ctc con preparazione intestinale ridotta . 
nel nostro gruppo di pazienti la tollerabilit della colonscopia ottica stata simile a quella della ctc , e questo probabilmente dovuto al fatto che la maggior parte delle colonscopie sono state eseguite in sedazione . 
infine , i questionari hanno mostrato percentuali simili di preferenza come test di radiol med ( 2010 ) 115 : 12671278 1277 discomfort for ctc and colonoscopy were quite similar . these could be due to the fact that most of colonoscopies were performed under sedation . 
this result is encouraging for the implementation of ctc as a screening test . the principal limitation of this preliminary study is the use of standard bowel preparation without faecal tagging . the use of faecal tagging reduces the number of false positive results , enabling a better distinction between polyps and faecal residues [ 13 ]  . 
conversely , another study on ctc performed without faecal tagging in fobt positive subjects showed a low specificity ( 59% for polyps > 6 mm ) [ 14 ]  . 
in this setting ctc without faecal tagging has a high sensitivity and npv for cancers and adenomas of at least 6 mm , but its specificity and positive predictive value are relatively low . 
these elements militate against use of ctc as a routine second line test after a positive fobt , due to the high prevalence of colonic neoplastic lesions in these subjects and low ppv of ctc . 
conversely , the high sensitivity and negative predictive value of ctc for adenoma and cancer in our study support its potential use in fobt positive subjects who refuse colonoscopy or in subjects with incomplete colonoscopy [ 15 ]  . screening per la ctc e per il fobt , piuttosto che per la colonscopia , dato incoraggiante per limplementazione della ctc nei programmi di screening . 
in un recente trial multicentrico , la ctc con marcatura fecale ha mostrato una specificit pi elevata ( 76 , 4% ) in una coorte di soggetti con fobt positivo [ 11 ]  . 
viceversa un altro studio sullimpiego della ctc senza marcatura fecale in soggetti fobt positivi ha dimostrato una bassa specificit ( 59% per i polipi > 6 mm ) [ 14 ]  . 
 conclusioni in conclusione , la nostra esperienza preliminare ha confermato che i soggetti con fobt positivo , nellambito di un programma di screening regionale , presentano unalta prevalenza di lesioni adenomatose . 
in questo contesto , la ctc senza marcatura fecale ha mostrato alta sensibilit ed alto valore predittivo negativo nel rilievo di cancri e adenomi di almeno 6 mm , ma specificit e valore predittivo positivo relativamente bassi . 
questi elementi non supportano limpiego di routine della ctc come test di secondo livello nei soggetti fobt positivi , data lelevata prevalenza di lesioni neoplastiche del colon in questi pazienti ed il basso valore predittivo positivo della ctc . 
owing both to the intrinsic difficulty of common radiographic and endoscopic methods in visualising the entire small bowel and the lack of typical physical findings , a delay in diagnosis is common . 
recently , magnetic resonance ( mr ) imaging has become a widely accepted imaging modality in the study of suspected small - bowel neoplasms due to its ability to depict , without exposure to ionising radiation and with excellent soft - tissue contrast , intraluminal disorders in conjunction with mural , extraparietal and regional abnormalities . 
queste neoplasie tendono ad essere diagnosticate tardivamente sia per le intrinseche difficolt delle comuni tecniche radiologiche ed endoscopiche a visualizzare lintero intestino tenue sia per la mancanza di sintomi e segni clinici specifici . 
tra le tecniche radiologiche recenti , la risonanza magnetica ( rm ) si imposta come modalit di scelta nello studio dei pazienti con sospetta patologia neoplastica di tenue e questo grazie alla capacit intrinseca di studio , senza far ricorso alluso di radiazioni ionizzanti e con ottimo contrasto tissutale , non solo della patologia luminale ma anche delle anormalit intramurali , extraparietali , locoregionali extra - intestinali . 
scopo del seguente articolo illustrare gli aspetti in rm delle principali neoplasie maligne del tenue . parole chiave intestino tenue tumori risonanza magnetica introduction introduzione small - bowel tumours are very rare , accounting for only 2% of all gastrointestinal neoplasms and less than 0.4% of all cancers [ 1 , 2 ]  . 
the most common histological types of malignant tumours of the small bowel registered by the surveillance , epidemiology and end results ( seer ) programme of the national cancer institute were adenocarcinoma ( 45% ) , carcinoid ( 29% ) , lymphoma ( 16% ) and i tumori dellintestino tenue sono estremamente rari , responsabili di appena il 2% delle neoplasie gastrointestinali e di meno dello 0 , 4% di tutti i tipi di neoplasie [ 1 , 2 ]  . nel registro del programma surveillance , epidemiology and end results ( seer ) del national cancer institute statunitense , listotipo pi frequente risultato ladenocarcinoma ( 45% ) , seguito dal carcinoide ( 29% ) , dal 1280 radiol med ( 2010 ) 115 : 12791291 sarcoma ( 10% ) [ 3 ]  . 
clinical manifestations of these neoplasms may be characterised by abdominal pain , bleeding , nausea and / or vomiting , weight loss and diarrhoea , obstruction or intussusception , palpable mass . 
owing both to the rarity of these lesions and the lack of typical physical findings , a delay in diagnosis is common , with a mean period of 68 months from first symptoms [ 4 ]  . 
however , it is not always very accurate in identifying the precise site of bleeding and is contraindicated in suspected bowel stricture due to the risk of capsule retention [ 57 ]  . 
push enteroscopy and double - balloon enteroscopy allow partial exploration of the small bowel and permit one to obtain tissue samples . however , they are invasive , time consuming and technically challenging methods . 
enteroclysis and enterographic techniques in conjunction with computed tomography ( ct ) or magnetic resonance ( mr ) scanning have increasing impact on the diagnostic approach to small - bowel disease , thanks to the ability to depict with high spatial resolution both the wall ( allowing evaluation of intraluminal disorders and structural characteristics ) and extraintestinal structures ( mesentery , adjacent fibrofatty tissue , lymph nodes , peritoneal spaces ) [ 810 ]  . 
in particular , small - bowel mr imaging , with its multiplanar capabilities and excellent soft - tissue contrast without exposure to ionising radiation , is able to supply anatomical and functional information about the bowel loops through the use of standard and fluoroscopic sequences , respectively , the latter to discriminate simple contractions from fixed strictures [ 1113 ]  . 
 the aim of this pictorial review is to illustrate , on the basis of our experience between june 2007 and may 2009 , the mr appearance of malignant small - bowel neoplasms . 
tali neoplasie possono manifestarsi clinicamente con dolore addominale , con sanguinamento gastrointestinale , con nausea e / o vomito , con calo ponderale , diarrea , con i segni dellostruzione o dellinvaginazione intestinale , come masse palpabili ; tuttavia i segni e i sintomi della neoplasia risultano aspecifici nella maggior parte dei casi . 
in virt di questultima considerazione e a causa della rarit delle lesioni , la diagnosi viene posta in genere tardivamente ( in media 68 mesi dopo lesordio dei primi sintomi ) [ 4 ]  . 
la videocapsula ( vce ) la metodica di scelta nella visualizzazione delle anomalie della mucosa nei pazienti con sanguinamento oscuro nei quali gastroscopia e colonscopia abbiano dato risultati negativi , tuttavia tale metodica non sempre riesce ad identificare lorigine del sanguinamento e risulta controindicata nei casi di sospetta steno - ostruzione , a causa del rischio di ritenzione [ 57 ]  . 
lenteroscopia con singolo o doppio pallone tecnica che permette una visualizzazione parziale del tenue e che consente lesecuzione di prelievi bioptici , tuttavia linvasivit , la tempistica dellesame , la difficolt tecnica dellesame stesso , non sono trascurabili . il tenue baritato per os e il clisma del tenue sono in grado di diagnosticare anormalit della mucosa , masse e / o invaginazioni , forniscono informazioni solo indirette sulla parete intestinale e sulle strutture extraintestinali adiacenti , sono spesso non utili ai fini della diagnosi . 
le tecniche di enteroclisi ed enterografia con tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) hanno unimportanza crescente nello studio del tenue poich consentono , con elevata risoluzione spaziale , una visualizzazione diretta sia della parete ( valutandone eventuali anomalie luminali e caratteristiche strutturali ) sia delle strutture extraviscerali adiacenti ( mesentere , tessuto adiposo limitrofo , linfonodi , spazi peritoneali ) [ 810 ]  . 
in particolare la rm , con un imaging multiplanare ad eccellente risoluzione di contrasto e senza radiazioni ionizzanti , in grado di fornire informazioni sia anatomiche sia funzionali riguardo lo stato delle anse , previa utilizzazione di sequenze rispettivamente standard e fluoroscopiche , capaci queste ultime di discriminare stenosi fisse da semplici contrazioni peristaltiche [ 1113 ]  . scopo del seguente articolo illustrare , utilizzando la casistica afferente al nostro reparto nel periodo giugno 2007maggio 2009 , gli aspetti in rm delle principali neoplasie maligne del tenue . gli esami rm sono stati eseguiti utilizzando tecnica mr technique mr examinations were performed using a superconductive 1.5 - t magnet ( excelart vantage , toshiba medical systems , japan ) and 1 , 0001 , 500 ml of polyethylene glycol ( peg ) solution administered orally to obtain adequate small - bowel distension . 
 adenocarcinoma adenocarcinomas represent 25%50% of small - bowel cancers , and the incidence is highest in the duodenum , with 65% of all neoplasms located in the periampullary region [ 14 ]  . 
in patients with crohns disease , the primary site of the neoplasm is the ileum ; the development of adenocarcinoma should be suspected in those with long - standing disease who develop a change in their clinical status , such as obstruction that fails to resolve with the usual medical treatments [ 15 ]  . 
on mr , enterografica e magnete superconduttivo da 1 , 5 t ( excelart vantage , toshiba medical systems , giappone ; 10001500 ml di polietilenglicole per os con lo scopo di ottenere unadeguata distensione delle anse intestinali )  . nel protocollo di studio sono state incluse sequenze t2weighted half - fourier single - shot fast advanced spin echo ( ssfase ) e true fast imaging in the steady - state free precession ( ssfp ) seguite da sequenze fat - suppressed spoiled 3d volume interpolated breath - hold examination ( vibe ) con acquisizione dinamica in fase arteriosa e venosa , dopo somministrazione ev di gadopentetato dimeglumina ( gd - dtpa ) ( 0 , 1 mmol / kg )  . adenocarcinoma ladenocarcinoma il tumore maligno pi frequente ( 25%50% dei casi )  . 
sono considerati fattori di rischio correlati allinsorgenza della neoplasia un morbo di crohn , la presenza di unileostomia , un bypass intestinale , una duplicazione intestinale congenita , la sindrome di peutz - jeghers . 
in presenza di morbo di crohn la complicanza correlata allinsorgenza di un adenocarcinoma va sospettata nei pazienti con malattia di lunga durata nei quali si instauri una modificazione inspiegata dello status clinico , ad esempio unocclusione intestinale non rispondente a terapia medica [ 15 ] ; in questi casi inoltre la neoplasia si localizza prevalentemente nellileo . 
nellimmagine ssfse ( haste ) t2w , presenza di lesione anulare isointensa al muscolo ( freccia bianca ) , ad estrinsecazione endoluminale , stenotizzante e determinante ectasia gastrica a monte . il linfoma intestinale primitivo si caratterizza per lassenza di linfoadenopatie superficiali palpabili , per una conta leucocitaria normale , per il mancato coinvolgimento di fegato e milza , per i reperti radiografici toracici radiol med ( 2010 ) 115 : 12791291 1282 fig . 
a livello dellileo preterminale evidenza di massa bulky ( freccia bianca ) con ostruzione luminale e secondaria dilatazione a monte , con segnale eterogeneo ed iso - ipointenso in fat sat gre t1w ( a ) , iperintenso in fse t2w ( b ) , con enhancement moderato ed irregolare nella sequenza fast spoiled gre 3d t1w acquisita su piano sagittale dopo somministrazione di mdc paramagnetico ( c )  . 
 lymphoma the findings of primary small - bowel lymphoma include no palpable superficial lymph nodes , no involvement of the liver and spleen , a normal white blood cell count , a normal chest radiograph without mediastinal or hilar adenopathy and normali ( non adenopatie mediastiniche o ilari ) , per il prevalente coinvolgimento del tratto gastrointestinale [ 18 ]  . 
pazienti a rischio neoplastico sono quelli affetti da sindrome da immunodeficienza , da malattia celiaca di lunga data , da malattia infiammatoria cronica intestinale , da patologia autoimmunitaria ( per esempio , lupus eritematoso sistemico [ les ] ) , da uno stato di immunodepressione post - trapianto [ 19 ]  . 
le forme neoplastiche tenuali sono rappresentate da linfomi non - hodgkin primitivi ( sia a cellule b , pi frequenti nellileo distale , sia a cellule t , pi frequenti nel digiuno ) , da linfomi di burkitt , da linfomi tipo muocosal associated lymphoid tumor ( malt ) , raramente da linfomi di hodgkin [ 20 , 21 ]  . 
axial ( a ) and coronal ( b ) t2 - weighted ssfse ( haste ) images show ileal segmental infiltrating lesion , isointense to muscle , with smooth regular contours and aneurysmal dilatation of the involved segment with displacement of adjacent left colon ( white arrow )  . 
le immagini assiali ( a ) e coronali ( b ) ssfse ( haste ) t2w dimostrano una lesione segmentale infiltrante dellileo ( freccia bianca ) , isointensa al muscolo , a margini regolari , con dilatazione aneurismatica del segmento coinvolto e dislocazione di anse adiacenti del colon sinistro . 
risk factors in the pathogenesis of gastrointestinal lymphoma include immunodeficiency syndrome , longstanding celiac disease , inflammatory bowel disease , autoimmune disorders such as systemic lupus erythematosus and immunosuppression after solid - organ transplantation [ 19 ]  . types of lymphoma that may involve the small intestine include primary non - hodgkins lymphoma ( both b cell and t cell ) , burkitts lymphoma , mucosa - associated lymphoid tissue ( malt ) - type lymphoma and , rarely , hodgkins lymphoma [ 20 ]  . 
whereas the distal ileum is the most common site of small - bowel b - cell lymphoma , peripheral tcell lymphoma is most frequently seen in the jejunum [ 21 ]  . 
approximately 70% of tumours are larger than 5 cm in diameter at presentation [ 23 ]  . in the setting of the more common segmental infiltrating lesions , mr can depict a typical aneurysmal dilatation of the bowel walls due to replacement of the muscularis propria and destruction of the nerve plexus by the tumour . 
nelle forme segmentali infiltranti , le pi frequenti , a causa della denervazione e della distruzione della tonaca muscolare indotta dalla crescita tumorale , tipica una dilatazione aneurismatica del tratto coinvolto . 
le linfoadenopatie retroperitoneali tendenti alla conglobazione e la dilatazione aneurismatica del tratto coinvolto rappresentano gli elementi distintivi di diagnosi differenziale rispetto agli adenocarcinomi . tumori stromali gastrointestinali i tumori stromali gastrointestinali ( gists ) sono neoplasie mesenchimali definite sul piano cellulare dallespressione del recettore per il fattore di crescita della tirosina - chinasi ( kit , molecola cd 117 )  . 
lo stomaco la localizzazione 1284 radiol med ( 2010 ) 115 : 12791291 table 1 mr findings of common histological types of malignant tumours tumour type growth pattern margins secondary intestinal findings type of lymphatic mr findings and mesenteric spread adenocarcinoma irregular margins short annular lesion with intraluminal growth , predominantly in duodenum stenotic lesion with proximal obstruction locoregional metastases lymphoma long segmental infiltrating lesion ( focal polypoid mass or large exophytic tumour ) smooth regular contours with preservation of perivisceral fat plane aneurysmal dilatation without obstruction bulky retroperitoneal metastases gists intramural submucosal mass with extraserosal extension smooth lobulated contours aneurysmal dilatation , stenosis or obstruction almost absent peritoneal metastatic nodules , adenopathy rare carcinoid irregular margins ; focal asymmetric , predominantly in ileum mesenteric stranding ( submucosal or intraluminal small nodules ) and kinking of the involved segment intermittent obstruction possible mesenteric proximally to kinked loop hypervascular isointense to muscle on t1w , heterogeneous metastases with spiculated margins hyperintense on and local adenopathy t2w , hypervas with calcification metastases wall thickening or focal polypoid mass irregular or regular localisation on aneurysmal antimesenteric dilatation almost absent , stenosis or border in case of obstruction possible peritoneal seeding gist , gastrointestinal stromal tumour ; gd , gadolinium isointense to muscle on t1w , heterogeneous signal on t2w , hypovascular lesion after gd isointense to muscle on t1w , heterogeneous signal on t2w , moderate enhancement after gd inhomogeneous lesions isointense on t1w , mildly hyperintense on t2w , peripheral enhancement in large lesions cular lesion after signal intensity reflects that of primary neoplasm lymphoma is usually accompanied by bulky retroperitoneal adenopathy and aneurysmal dilatation of affected small bowel . gastrointestinal stromal tumours gastrointestinal stromal tumours ( gists ) are mesenchymal neoplasms of the gastrointestinal tract defined by the expression of kit ( cd 117 ) , a tyrosine kinase growth factor receptor . 
gists most frequently occur in the stomach ( 70% of cases ) , followed by the small intestine ( 2030% ) , anorectum ( 7% ) , colon and oesophagus [ 24 ]  . 
gists range in size from several millimetres to greater than 30 cm , commonly originate from the muscularis propria of the prevalente ( 70% dei casi ) , seguita dal piccolo intestino ( 20%30% ) , dalla regione ano - rettale ( 7% ) , dal colon e dallesofago [ 24 ]  . 
le neoplasie originano dalla muscolare propria della parete intestinale , si estrinsecano in forma di massa ben circoscritta di dimensioni variabili ( da pochi mm a 30 cm ed oltre ) in sede intramurale sottomucosa , presentano pattern di crescita tipicamente esofitico [ 25 ]  . la crescita intramurale sottomucosa determina la distensione della mucosa del tratto coinvolto e favorisce lulcerazione della stessa , reperto riscontrabile in circa il 50% dei casi . 
nei tumori di dimensioni maggiori non sono rare la degenerazione cistico - emorragica . la necrosi e laspetto rm tipico quello della massa intramurale sottomucosa a margini lisci e lobulati con crescita esofitica extraparietale e secondaria dislocazione delle anse radiol med ( 2010 ) 115 : 12791291 tabella 1 caratteristiche rm dei principali istotipi neoplastici tipo di neoplasia pattern di crescita margini segni secondari semeiologia rm tipo di diffusione linfatica e mesenterica adenocarcinoma irregolari lesione breve , anulare , crescita endoluminale , prevalente nel duodeno stenosi ed ostruzione metastasi prossimale locoregionali linfoma lesione segmentale infiltrante ( massa polipoide focale o neoplasia di grandi dimensioni ) regolari , lisci , preservazione del tessuto adiposo periviscerale dilatazione aneurismatica senza ostruzione metastasi bulky retroperitoneali gist regolari e lobulati massa intramurale sottomucosa , estensione extrasierosa dilatazione aneurismatica , stenosi ed ostruzione quasi sempre assenti noduli metastatici peritoneali , linfoadenopatie rare 1285 segnale isointenso al muscolo in t1w , eterogeneo in t2w , ipovasco larizzazione dopo somministrazione di gadolinio ev segnale isointenso al muscolo in t1w , segnale eterogeneo in t2w , enhancement moderato dopo somministrazione di gadolinio lesione eterogenea , iso - ipointensa in t1w , moderatamente iperintensa in t2w , enhancement periferico nelle lesioni di dimensioni maggiori carcinoide massa focale , asimmetrica , prevalente nellileo , localizzazione sottomucosa ( piccoli noduli endoluminali ) irregolari ; stranding ostruzione mesenteriale , angolazione del segmento coinvolto intermittente possibile cranialmente allansa angolata metastasi ispessimento parietale o massa polipoide focale irregolari o regolari metastasi mesenteriche ipervascolari a margini irregolari , n t2w , linfoadenopatie locoregionali , calcificazioni segnale isointenso al muscolo in t1w , segnale eterogeneo iipervascolarizza zione dopo somministrazione di gadolinio vedi segnale neoplasia primitiva dilatazione aneurismatica quasi sempre assente , stenosi ed ostruzione possibili localizzazione sul versante antimesenterico dellansa nel caso di disseminazione peritoneale gist , tumore stromale gastrointestinale intestinal wall and are typically well - circumscribed masses with intramural submucosal location and exophytic growth [ 25 ]  . 
un aspetto meno tipico quello della massa focale polipoide a crescita intraluminale . nelle neoplasie di dimensioni significative la semeiologia del segnale dipende dalleventuale presenza di necrosi ( segnale ipointenso in t1w - iperintenso in t2w ) o emorragia ( segnale iso - iperintenso in t1w - t2w in base alla datazione del sanguinamento )  . 
after intravenous administration of gadolinium , the mass appears heterogeneously hypervascular , with peripheral progressive enhancement from the arterial ( b ) to the venous ( c ) and equilibrium ( d ) phase . 
dopo somministrazione di mdc paramagnetico si evidenzia ipervascolarizzazione disomogenea con enhancement progressivo e centripeto dalla fase arteriosa ( b ) alle fasi venosa ( c ) e tardiva ( d )  . 
in large tumours , mr features depend on the degree of necrosis and haemorrhage , with areas of necrosis being low signal intensity on t1weighted images and high signal intensity on t2 - weighted images and areas of haemorrhage from high to low signal intensity on both t1 - weighted and t2 - weighted images depending on the age of the haemorrhage . 
le metastasi da gists si distribuiscono per via ematogena prevalentemente nel fegato , nellomento , nel peritoneo ; a differenza di quanto avviene per gli adenocarcinomi e per i linfomi la distribuzione metastatica per va linfatica risulta estremamente rara . carcinoide i carcinoidi sono neoplasie ben differenziate ad origine radiol med ( 2010 ) 115 : 12791291 1287 fig . 
axial ( a ) and coronal ( b ) t2 - weighted ssfse ( haste ) images show giant cystic peritoneal mass in the left hypochondrium , with peripheral solid component mildly hyperintense and large necrotic central portion clearly hyperintense to muscle . 
nelle immagini ssfse ( haste ) t2w su piano assale ( a ) e coronale ( b ) si dimostra ampia massa cistica in ipocondrio sinistro con componente periferica solida moderatamente iperintensa e core centrale necrotico nettamente iperintenso . 
dopo somministrazione di mdc paramagnetico , nella sequenza coronale fast spoiled gre 3d t1w ( c ) , si rileva enhancement periferico e disomogeneo segnatamente della parte neoplastica solida . present with metastases to the liver , omentum and peritoneum ; unlike adenocarcinoma and lymphoma , lymphatic spread does not usually occur , so adenopathy is rare . carcinoid carcinoids are well - differentiated neoplasms arising from the endocrine system outside the pancreas and thyroid . 
queste forme in virt delle piccole dimensioni sono difficilmente visualizzabili in tc e rm . nellileo , sede di insorgenza del 90% dei casi , i carcinoidi si manifestano in forma di ispessimento parietale focale ed asimmetrico ove lispessimento murale il risultato della reazione desmoplastica infiltrativa sottomucosa indotta dal tumore . 
la fibrosi transmurale stessa pu determinare 1288 radiol med ( 2010 ) 115 : 12791291 mural periampullary nodules with arterial enhancement . because of their small dimensions , these tumours may be extremely difficult to visualise with mr or ct imaging . ninety percent of carcinoids arise in the ileuat this site , the tumour may manifest as asymmetric focal bowel - wall thickening , with mural thickening representing a secondary finding to the infiltrating lesion and desmoplastic submucosal fibrosis . 
metastases from carcinoids are generally hypervascular and best detected during arterial - phase imaging . metastases a small - bowel mass in a patient with a known cancer is likely to be a metastasis . 
al momento della diagnosi il 58%64% dei pazienti hanno una malattia avanzata con metastasi , classicamente ipervascolari , ai linfonodi locoregionali o al fegato [ 29 ]  . metastasi in un paziente oncologico una massa a localizzazione tenuale rappresenta verosimilmente una metastasi . 
on coronal fast imaging with steady - state free precession ( true fisp ) sequence ( a ) , the tumour ( white arrow ) appears as an irregular mesenteric mass , with adjacent desmoplastic reaction and subtle kinking of the lower intestinal loop . 
massa stessa ad elevato enhancement post - contrastografico dopo somministrazione di mdc paramagnetico nella sequenze fast spoiled gre 3d t1w su piano assiale ( b )  . radiol med ( 2010 ) 115 : 12791291 1289 fig . 
coronal t2 - weighted ssfse ( haste ) ( a ) and axial fast imaging with steady - state free precession ( true fisp ) sequences ( b ) depict a round mass with low signal intensity both in t1and t2 - weighted images ( white arrow )  . 
haematogenous metastases from lung or breast cancer produce round polypoid masses that can cause intussusception . conclusions in patients with suspected small - bowel disease , after negative upper and lower endoscopy , mr provides anatomical and functional information about the small bowel without exposure to ionising radiation and with excellent soft - tissue contrast . 
moreover , thanks to its ability to depict intraluminal disorders in conjunction with mural , extraparietal and regional abnormalities , it could be an optimal imaging procedure complementary to capsule endoscopy for detecting small - bowel tumours . 
 conclusioni nei pazienti con endoscopia superiore ed inferiore negative e con sospetta patologia di tenue , la rm metodica in grado di fornire informazioni sia anatomiche sia funzionali riguardo lo stato delle anse intestinali , senza far ricorso allutilizzo di radiazioni ionizzanti e con eccellente risoluzione di contrasto . 
grazie allabilit intrinseca della metodica nellevidenziazione non solo delle anormalit intestinali endoluminali ma anche delleventuale coinvolgimento murale , extraparietale e locoregionale , la rm risulta particolarmente utile ( e complementare alla videocapsula ) nellidentificazione delle neoplasie del tenue . 
la sequenza ssfse ( haste ) t2w su piano assiale ( a ) e coronale ( b ) mostra una lesione ileale intraluminale solida moderatamente iperintensa ( freccia bianca ) che si dimostra essere , dopo chirurgia e valutazione anatomo - patologica , una metastasi da neoplasia del colon . 
 small - bowel tumours , although generally nonspecific , may sometimes guide the diagnosis towards the different histological subtypes ( table 1 )  . semeiologia rm delle neoplasie maligne , sebbene generalmente aspecifica , consente talvolta di orientare la diagnosi verso i differenti istotipi neoplastici ( tabella 1 )  . 
between january 2005 and march 2007 , 33 fetuses with a mean gestational age of 28.9 weeks ( range 1737 ) and mild ventriculomegaly diagnosed at prenatal sonography were included in this prospective study . 
all fetuses underwent mr imaging according to the following protocol : half - fourier t2 - weighted images along the three orthogonal plane according to the longitudinal axis of the mother , and subsequently three orthogonal planes were acquired according to the fetal brain . quantitative image analysis included the size of the transverse diameter of the lateral ventricles , in the axial plane , and the thickness of the adjacent cerebral cortex . qualitative image analysis included morphology of the lateral ventricles ( normal , parallel pattern colpocephaly ) , signal intensity changes of the fetal brain , interruption of the germinative matrix , agenesis of the corpus callosum ( complete / partial ) and associated malformations . 
mean axial diameter of the lateral ventricle was 11.6 mm ( range 1015 mm ) , and mean thickness of the adjacent cerebral cortex was 2.1 mm ( range 1.83 mm ) ; 23 / 33 fetuses ( 70% ) showed normal morphology of the lateral ventricles , and 8 / 33 ( 24% ) showed abnormal morphology ( parallel pattern , colpocephaly )  . 
tra gennaio 2005 e marzo 2007 , 33 feti con et gestazionale media di 28 , 9 settimane ( range 1737 ) e ventricolomegalia lieve allecografia , sono stati inclusi in questo studio prospettico . 
lanalisi qualitativa ha compreso : morfologia dei ventricoli laterali , alterazioni dellintensit di segnale , focali o diffuse , del tessuto nervoso encefalico , soluzioni di continuo della matrice germinativa , agenesia del corpo calloso ( completa / parziale ) e malformazioni associate . 
il diametro trasversale medio ventricolare stato di 11 , 6 mm ( range 1015 mm ) con spessore corticale adiacente di 2 , 1 mm ( range 1 , 83 mm )  . 
il corpo calloso stato completamente visualizzato in 20 / 33 ( 60% ) feti ; in 8 / 33 ( 25% ) feti vi era agenesia totale mentre in 5 / 33 ( 15% ) unipogenesia . 
mr imaging may prove to be a useful secondline imaging modality in the prenatal diagnosis of corpus callosum agenesis in fetuses with mild ventriculomegaly . feti su 13 ( 46% ) mostravano agenesie isolate . 
la rm pu rappresentare una metodica di secondo livello nellidentificazione pre - natale delle forme di agenesia del corpo calloso associata a ventricolomegalia lieve . parole chiave corpo calloso imaging fetale rm ostetricia keywords corpus callosum fetal imaging mr imaging obstetric introduction introduzione agenesis of the corpus callosum is the most frequent commissural malformation of the central nervous system ( cns )  . 
prevalence of the condition is 0.3% in the general population [ 3 ] and 2%3% in subjects with delayed development [ 4 ] , with an extremely variable clinical presentation ranging from asymptomatic to severe mental retardation [ 5 ]  . early diagnosis of corpus callosum agenesis and possible associated malformations is therefore crucial for prenatal consultation and consequent pregnancy management . however , prenatal ultrasonography ( us ) performed during the second trimester of pregnancy ( < 22 weeks ) may not visualise the corpus callosum [ 68 ]  . 
therefore , diagnostic suspicion is based on indirect signs , such as the absence of the cavum septum pellucidum and / or an abnormal configuration of the lateral ventricles ( parallel course of the frontal horns of the lateral ventricles or colpocephaly ) [ 7 , 9 ]  . 
with a transverse diameter at the level of the atrium of 1015 mm [ 7 , 10 , 11 ] , which accounts for some 15%20% of fetal ventriculomegaly , the risk of isolated agenesis of the corpus callosum is 10% [ 11 ] , and those fetuses generally have a favourable prognosis in 85% of cases [ 12 ]  . 
however , 3% of cases of mild ventriculomegaly are associated with corpus callosum agenesis and / or cns or extra - cns malformations , with a less favourable prognosis [ 11 ]  . unlike us , mr constantly visualises the fetal corpus callosum , which makes possible a direct diagnosis of agenesis . 
the aim of this study was to evaluate the role of fetal mr in diagnosing corpus callosum agenesis , either isolated or lagenesia del corpo calloso la pi frequente malformazione commissurale del sistema nervoso centrale . 
la sua prevalenza dello 0 , 3% nella popolazione generale [ 3 ] e del 2%3% nei soggetti con ritardo dello sviluppo [ 4 ] con una presentazione clinica estremamente variabile : da pazienti asintomatici , fino a soggetti con grave ritardo mentale [ 5 ]  . 
tuttavia lecografia pre - natale , eseguita durante il secondo trimestre di gravidanza ( < 22 settimane ) , pu non visualizzare direttamente il corpo calloso [ 68 ] ; per cui il sospetto diagnostico si fonda su segni indiretti : quali lassenza del cavo del setto pellucido , e / o unanomala configurazione dei ventricoli laterali ( decorso parallelo dei corni frontali dei ventricoli laterali o colpocefalia ) [ 7 , 9 ]  . anche il rilievo di una ventricolomegalia cerebrale deve far sospettare unagenesia del corpo calloso . 
tuttavia quando la ventricolomegalia lieve , vale a dire con diametro trasversale a livello dellatrio di 1015 mm [ 7 , 10 , 11 ] , che rappresentano il 15%20% delle ventricolomegalie fetali , il rischio di agenesia del corpo calloso isolata del 10% [ 11 ] e tali feti presentano generalmente prognosi favorevole nell85% dei casi [ 12 ] ; il 3% dei casi di ventricolomegalia lieve si pu per associare ad agenesia del corpo calloso e / o ad altre malformazioni del sistema nervoso centrale ( snc ) o extra - snc , con prognosi peggiore [ 11 ]  . al contrario dellecografia , la risonanza magnetica ( rm ) permette costantemente di visualizzare il corpo calloso fetale , consentendo una diagnosi diretta in caso di agenesia . 
lobiettivo di questo lavoro stato quello di valutare il ruolo della rm fetale nella diagnosi di agenesia del corpo calloso , isolata od associate ad altre radiol med ( 2010 ) 115 : 301312 associated with other abnormalities , in the presence of us findings of mild ventriculomegaly . anomalie , in presenza di riscontro ecografico di ventricolomegalia lieve . materials and methods patient population materiali e metodi popolazione dei pazienti between january 2005 and march 2007 , we studied with mr 46 fetuses in 42 women ( four twin pregnancies ) with a us diagnosis of cerebral ventriculomegaly . 
our prospective study included 33 / 46 fetuses with a mean gestational age of 28.9 weeks ( range 1737 weeks ) selected on the basis of the following criteria : us finding of either unilateral or bilateral mild ventriculomegaly ( transverse diameter at the atrial level between 10 and 15 mm ) [ 7 , 10 ] with a diagnosis or suspected diagnosis of corpus callosum agenesis at us and gestational age > 14 weeks . 
the gestational age > 14 weeks was adopted as an inclusion criterion for two reasons : the stability of the size of the atrium of the lateral ventricles in the second and third trimester [ 7 ] and to avoid performing mr examinations in the first trimester of pregnancy , as indicated by the recommendations of the safety committee of the international society of magnetic resonance [ 13 , 14 ]  . 
ventriculomegaly was considered unilateral when the diameter of the lateral ventricular atrium of a single ventricle was > 10 mm , with the contralateral ventricle within the normal range of values , and bilateral when the diameter of both atria of the lateral ventricles was between 10 and 15 mm ( mild ventriculomegaly )  . exclusion criteria were us diagnosis of moderate ventriculomegaly ( transverse atrial diameter > 15 mm , with thickness of the adjacent cerebral cortex > 2 mm ) in ten patients , and severe ( ventricular diameter > 15 mm , with cortical thickness > 2 mm ) in seven patients , as well as general contraindications to mr of the mother , claustrophobia and gestational age < 14 weeks . 
in one case , maternal infection by treponema pallidum was diagnosed . of the 33 fetuses included n the study , 30 ( 91% ) were brought to term , with 17 / 30 fetuses ( 57% ) being born with natural birth , 13 / 30 with caesarean section and 3 / 33 pregnancies ( 7% ) being voluntarily terminated due to crouzon syndrome , myelocele and heart malformation associated with maternal infection by t . 
at birth , all neonates underwent a neonatal trasversale a tra gennaio 2005 e marzo 2007 , 46 feti in 42 donne ( 4 gravidanze gemellari ) , con diagnosi ecografica di ventricolomegalia cerebrale , sono stati sottoposti a rm , presso il nostro istituto . 
un consenso informato scritto , stato ottenuto da ogni donna , prima dellesecuzione dellindagine . dei 46 feti , 33 , con et gestazionale media di 28 , 9 settimane ( range 1737 settimane ) , sono stati inclusi in questo studio prospettico in base ai seguenti criteri : riscontro ecografico di ventricolomegalia lieve , sia monolaterale che bilaterale ( diametro livello dellatrio compreso tra 10 e 15 mm ) [ 7 , 10 ] con diagnosi o sospetto diagnostico di agenesia del corpo calloso allesame ecografico , ed et gestazionale > 14 settimane . 
let gestazionale superiore a 14 settimane stata adottata come criterio di inclusione per un duplice motivo : la stabilit delle dimensioni dellatrio dei ventricoli laterali , nel secondo e terzo trimestre di gravidanza [ 7 ] , e per evitare di eseguire degli esami di rm durante il primo trimestre di gravidanza , come indicato dalle raccomandazioni del comitato per la sicurezza della societ internazionale di risonanza magnetica [ 13 , 14 ]  . 
la ventricolomegalia stata considerata monolaterale quando il diametro dellatrio ventricolare laterale di un solo ventricolo risultato maggiore di 10 mm , mentre il controlaterale era compreso nellintervallo di valori normali ; bilaterale quando il diametro di entrambi gli atri dei ventricoli laterali era compreso tra 10 e 15 mm ( ventricolomegalia lieve )  . criteri di esclusione sono stati rappresentati da : diagnosi ecografica di ventricolomegalia di grado moderato ( diametro trasversale a livello dellatrio > 15 mm , con spessore della corteccia cerebrale adiacente > 2 mm ) in 10 pazienti , e severo ( diametro ventricolare > 15 mm , con spessore corticale < 2 mm ) in 7 pazienti ; nonch controindicazioni generali alla rm della madre , claustrofobia , ed et gestazionale < 14 settimane . 
lintervallo di tempo medio intercorso tra lesame ecografico e quello di risonanza magnetica stato di 3 , 1 settimane ( range 532 giorni )  . ventuno / 33 ( 64% ) avevano eseguito anche lanalisi del cariotipo ; in uno caso stata diagnosticata infezione materna da treponema pallidum . trenta / 33 ( 91% ) gravidanze sono state portate a termine : 17 / 30 ( 57% ) feti sono nati mediante parto spontaneo , 13 / 30 ( 43% ) tramite taglio cesareo , eseguito con altre indicazioni ; 3 / 33 ( 7% ) gravidanze sono state interrotte volontariamente rispettivamente per sindrome di crouzon , mielocele e malformazione cardiaca associata ad infezione materna da treponema pallidu lepoca gestazionale 304 radiol med ( 2010 ) 115 : 301312 physical examination : 28 / 30 ( 93% ) were live births and 2 / 30 ( 7% ) were still births with associated malformations ( bilateral renal agenesis and lissencephaly )  . postnatal diagnosis the 28 / 33 live births ( 85% ) underwent a us study , whereas 5 / 33 ( 15% ) underwent postmortem examination . 
neonatal physical examination , postnatal diagnostic imaging and surgery constituted the reference standard in the 28 / 33 live births ( 85% ) , whereas the postmortem examination was the reference in the remaining 5 / 33 still births ( 15% )  . 
pallidum , respectively , in one case each . magnetic resonance technique the mr examination was performed with a 1.5 - tesla system ( magnetom symphony , siemens , erlangen , germany ) using a multichannel phased - array surface coil . after emptying the bladder , the women were placed in the supine ( 28 ) or lateral ( 5 ) position according to patient build or the most comfortable position . 
to reduce intestinal peristalsis , all women received an intramuscular injection of butylscopolamine ( buscopan , schering , germany ) 10 min prior to the beginning of the examination . the examination protocol involved the acquisition of t2weighted half - fourier rapid acquisition with relaxation enhancement ( rare ) images along the three planes orthogonal to the maternal longitudinal axis : axial , sagittal and coronal . 
t2 - weighted half - fourier rare images were then obtained of the fetal brain in the axial , coronal and sagittal planes with the following parameters : tr / te ( cid : 2 ) / 95 ms , slice thickness 3 mm , matrix 256256 and 3335 cm fov , with each sequence used as spatial reference for the subsequent sequence . 
in no cases was maternal or fetal sedation used , nor were intravenous gadolinium chelates administered . image analysis images were independently analysed by two mediana al parto stata la 37a settimana ( range 2342 )  . ventuno / 33 ( 63% ) neonati erano di sesso maschile e 12 / 33 ( 37% ) di sesso femminile ; la mediana del peso alla nascita era di 2950 grammi ( range 14204260 grammi )  . 
alla nascita , tutti i neonati sono stati sottoposti ad esame obiettivo neonatologico : 28 / 30 ( 93% ) neonati vitali , 2 / 30 ( 7% ) deceduti per malformazioni associate ( agenesia renale bilaterale e lissencefalia )  . diagnostica post - natale i 28 / 33 ( 85% ) neonati vivi sono stati sottoposti ad esame ecografico , mentre 5 / 33 ( 15% ) ad esame autoptico . 
lesame obiettivo neonatologico , la diagnostica per immagini post - natale e la chirurgia hanno costituito il gold standard di riferimento nei 28 / 33 ( 85% ) neonati vivi , mentre lesame autoptico nei restanti 5 / 33 ( 15% ) neonati deceduti . 
lesame autoptico ha dimostrato le seguenti malformazioni associate alla ventricolomegalia : mielocele , lissencefalia , agenesia renale bilaterale , sindrome di crouzon e malformazione cardiaca associata ad infezione materna da treponema pallidum , ognuna in un caso . tecnica di risonanza magnetica la rm stata effettuata con un magnete a 1 , 5 tesla ( magnetom symphony , siemens , erlangen , germania ) con limpiego di una bobina di superficie multicanale ( phasedarray )  . 
dopo svuotamento vescicale , le donne sono state posizionate in decubito supino ( 28 ) o laterale ( 5 ) a seconda del habitus della paziente o della posizione pi confortevole ; il decubito laterale stato preferito soprattutto nelle pazienti con epoca gestazionale pi avanzata . per ridurre la peristalsi intestinale , tutte le donne hanno ricevuto uniniezione intramuscolo di butilscopolamina ( buscopan , schering , germania ) 10 minuti prima dellinizio dellesame . il protocollo desame prevedeva immagini t2 - dipendenti half - fourier rapid acquisition with relaxation enhancement ( rare ) lungo i tre piani ortogonali allasse longitudinale materno : assiale , sagittale e coronale . 
successivamente , sono state ottenute immagini t2 - dipendenti half - fourier rare sullencefalo fetale lungo i piani assiale , coronale e sagittale , mediante i seguenti parametri : tr / te ( cid : 2 ) / 95 ms , 3 mm di spessore di scansione , matrice 256256 e 3335 cm di fov ; con ogni sequenza usata come riferimento spaziale per la sequenza successiva . 
quantitative image analysis was performed at a workstation on axial images by a radiologist ( at ) not involved in the qualitative analysis and included measuring the transverse diameter of the lateral cerebral ventricles at the level of the atrium and the thickness of the adjacent cerebral cortex . 
qualitative analysis included lateral ventricle morphology , focal or diffuse alterations in signal intensity of the brain tissue ( present / absent ) , interruption of the germinal matrices , presence of corpus callosum agenesis and other associated brain malformations . ventricular morphology was classified in the following manner : normal configuration of the lateral ventricles , the occipital horns with or without dilatation of colpocephaly ( defined as a disproportional enlargement of the occipital horns of the lateral ventricles with respect to the frontal horns ) and abnormal orientation of the frontal horns ( parallel orientation or fused frontal horns ) [ 7 ]  . 
the findings of the analysis of the mr images were compared with those of the diagnostic reference standard . results quantitative analysis at mr , ventriculomegaly was bilateral in 28 / 33 fetuses ( 85% ) and unilateral in 5 / 33 fetuses ( 15% ) ( four cases of ventriculomegaly of the right lateral ventricle and one of the left ventricle )  . 
in one case , a focal area of altered signal intensity of brain tissue was present at the level of the left basal nuclei , and in another case , an interruption of the germinal matrix was observed . 
in 6 / 13 fetuses ( 46% ) , agenesis of the corpus callosum was isolated : one sedazione materna , o curarizzazione fetale n somministrazione e.v di chelati del gadolinio . analisi delle immagini le immagini di rm sono state analizzate da due radiologi ( rm , cb ) con esperienza di rm ostetrica ( 5 anni ) , in maniera indipendente ; in caso di discrepanza di interpretazione , la decisione finale stata presa per consenso . lanalisi quantitativa delle immagini stata eseguita su workstation da un radiologo ( at ) non coinvolto nellanalisi qualitativa , sulle scansioni assiali , ed ha compreso : la misura del diametro trasversale dei ventricolari cerebrali laterali , a livello dellatrio , e lo spessore della corteccia cerebrale adiacente . 
lanalisi qualitativa ha compreso : la morfologia dei ventricoli laterali , alterazioni dellintensit di segnale , focali o diffuse , del tessuto nervoso encefalico ( presenti / assenti ) , soluzione di continuo delle matrici germinative , la presenza di agenesia del corpo calloso ed eventuali altre malformazioni encefaliche associate . 
 la morfologia ventricolare stata classificata nella seguente maniera : configurazione normale dei ventricoli laterali , dilatazione dei corni occipitali , con o senza colpocefalia ( definita come uno sproporzionato ingrandimento dei corni occipitali dei ventricoli laterali rispetto ai corni frontali ) ed orientamento anomalo dei corni frontali ( orientamento parallelo o corni frontali fusi ) [ 7 ]  . 
i risultati dellanalisi delle immagini di rm sono stati confrontati con il gold standard diagnostico di riferimento . risultati analisi quantitativa alla rm la ventricolomegalia risultata bilaterale in 28 / 33 ( 85% ) feti e monolaterale in 5 / 33 ( 15% ) feti ( 4 ventricolomegalie del ventricolo laterale destro e una del ventricolo sinistro )  . 
lo spessore medio della corteccia cerebrale adiacente era di 2 , 1 mm ( range 1 , 83 , 0 mm )  . analisi qualitativa ventitre / 33 ( 70% ) feti hanno dimostrato una normale configurazione dei ventricoli laterali . 
in un caso era presente unarea focale di alterato segnale del tessuto nervoso encefalico a livello dei nuclei della base di sinistra ed in un caso si osservata una soluzione di continuo della matrice germinativa . 
a axial t2 - weighted half - fourier rare ( tr / ( cid : 2 ) / 95 ms ) image shows mild dilatation of the lateral ventricles ( 11 mm )  . 
a limmagine assiale t2 - dipendenti half - fourier rapid acquisition with relaxation enhancement ( haste ) ( tr / te ( cid : 2 ) / 95 ms ) dimostra lieve dilatazione dei ventricoli cerebrali laterali ( 11 mm )  . 
il corpo calloso si visualizza in tutta la sua lunghezza , come dimostrato sia dalle immagini sagittali ( freccia in b ) e coronali ( freccia in c ) t2 - dipendenti haste ( tr / te ( cid : 2 ) / 95 ms )  . case of hypogenesis and five cases of total agenesis . 
comparate alla diagnostica post - natale , la risonanza magnetica fetale ha erroneamente interpretato 2 ipogenesie del corpo calloso : abbiamo avuto un falso positivo , in un feto in cui coesisteva una malformazione di dandy - walker , ed un falso negativo , in un feto con ipogenesia isolata . 
a axial t2 - weighted half - fourier rare ( tr / te ( cid : 2 ) / 95 ms ) image shows mild dilatation of the lateral ventricles ( 15 mm ) with parallel configuration of the frontal horns ( arrows ) and colpocephaly , defined as disproportionate enlargement of the occipital horns of the lateral ventricles when compared with the frontal horns ( arrowheads )  . 
a limmagine assiale t2 - dipendente haste ( tr / te ( cid : 2 ) / 95 ms ) dimostra lieve dilatazione simmetrica dei ventricoli cerebrali laterali ( 15 mm ) , con decorso parallelo dellasse longitudinale dei corni frontali ( frecce )  . 
a sagittal t2weighted half - fourier rare ( tr / te ( cid : 2 ) / 95 ms ) image shows total agenesis of the corpus callosum ( arrowheads )  . 
on coronal t2 - weighted half - fourier rare ( tr / te ( cid : 2 ) / 95 ms ) image ( b ) , the interhemispheric scissure is deeper and is separated from the third ventricle by the chorioid tela . 
a limmagine assiale t2 - dipendente haste ( tr / te ( cid : 2 ) / 95 ms ) dimostra agenesia totale del corpo calloso ( teste di freccia )  . 
b nellimmagine coronale t2 - dipendente haste ( tr / te ( cid : 2 ) / 95 ms ) si osserva un maggiore approfondimento della scissura interemisferica , che viene separata dal terzo ventricolo solamente dalla tela corioidea . 
c limmagine assiale t2 - dipendente haste ( tr / te ( cid : 2 ) / 95 ms ) dimostra un decorso parallelo dei ventricoli cerebrali laterali con una morfologia colpocefalica . 
coronal t2 - weighted half - fourier rare ( tr / te ( cid : 2 ) / 95 ms ) images confirm the normal development of the rostrum and the genu of the corpus callosum ( arrow in b ) , whereas in a more dorsal plane , the corpus callosum is not visualised ( arrow in c )  . 
a limmagine sagittale t2dipendente haste ( tr / te ( cid : 2 ) / 95 ms ) dimostra il rostro , il ginocchio e la porzione ventrale del corpo calloso ( freccia in a ) mentre non si visualizza la parte distale del corpo e lo splenio . 
le immagini t2 - dipendenti haste ( tr / te ( cid : 2 ) / 95 ms ) acquisite lungo il piano sagittale ( a ) ed assiale ( b ) dimostrano unagenesia completa del corpo calloso ( teste di freccia in a ) , con malformazione di dandy - walker , come indicato dallinserzione pi craniale del tintorio ( freccia in a ) , dallagenesia del verme cerebellare ( asterisco in b ) , e dalla dilatazione cistica del iv ventricolo ( frecce in b )  . radiol med ( 2010 ) 115 : 301312 the human braits development originates between week 8 and week 20 of gestation . 
abnormalities of the corpus callosum have been classified by dobyns [ 3 ] in four forms two primary and two secondary on the basis of the pathogenetic mechanism at play . 
numerous studies in the literature are in agreement that the severity of the clinical presentation is more closely correlated with the presence of associated malformations than with corpus callosum agenesis itself . 
one of the most frequently associated malformations is aicardi syndrome ( total or partial agenesis of the corpus callosum associated with other cerebral malformationsgyration disorders , periventricular heterotopy , cystic masses ) , and it can be potentially suspected with mr [ 8 , 1518 ]  . identification of isolated forms is therefore crucial . indeed , in the case of isolated agenesis , the prognosis is relatively good in 85% of cases [ 19 ]  . 
the main difficulty in expressing a judgement regarding long - term prognosis lies in the fact that often , the deficits that may arise from isolated agenesis of the corpus callosum cannot be identified until school age is reached , when they manifest as learning disorders . 
the presence of epileptic seizures , however , was above normal . prenatal diagnosis of this abnormality and possible associated abnormalities is therefore vital for providing correct information to parents regarding the neurological development of their child and pregnancy management . 
for this reason , evaluation of the size of the lateral ventricles should be an integral part of the us examination in the second and third trimester , in agreement with the antepartum obstetrical ultrasound examination guidelines [ 20 ]  . however , the us evaluation of the fetal cns may be limited by objective difficulties such as maternal build , unfavourable fetal position and severe oligohydramnios . these difficulties tend to increase with advancing pregnancy due to the progressive calcification of fetal cranial bone [ 6 , 21 ]  . identifying the normal corpus callosum at us is only possible with median sagittal scans or in coronal planes of the fetal braus sensitivity in identifying agenesis of the corpus callosum is highly variable in the literature : 28% discussione il corpo calloso la pi grande struttura commissurale interemisferica ; il suo sviluppo origina tra la ottava e la ventesima settimana di gestazione . 
in letteratura , numerosi autori concordano nellaffermare che la severit del quadro clinico maggiormente correlata alla presenza di malformazioni associate , pi che allagenesia del corpo calloso di per s . 
tra le malformazioni associate , la sindrome di aicardi ( agenesia , parziale o totale del corpo calloso , associata ad altre malformazioni cerebrali disturbi della girazione , eterotopie periventricolari , formazioni cistiche ) , rappresenta una di quelle pi frequentemente associate e potenzialmente sospettabili con la rm [ 8 , 1518 ]  . lidentificazione delle forme isolate dunque fondamentale ; in caso di agenesia isolata infatti la prognosi piuttosto buona nell85% dei casi [ 19 ]  . 
la difficolt maggiore nellesprimere un giudizio prognostico a lungo termine sta purtroppo nel fatto che spesso i deficit che possono derivare dallagenesia isolata del corpo calloso non sono evidenziabili fino allet scolare dove si manifestano come disturbi dellapprendimento . 
 [ 12 ] in una serie di 21 bambini con follow - up neurologico condotto per i primi 6 anni di vita hanno dimostrato come in corso di agenesia del corpo calloso isolata lo sviluppo motorio fosse normale ; l81% dei pazienti dimostrava inoltre un quoziente intellettivo nella norma senza differenze tra agenesie di tipo parziale o totale . 
 la diagnosi prenatale di questa anomalia e di eventuali anomalie associate dunque di fondamentale importanza per una corretta informazione ai genitori sulle prospettive di sviluppo neurologico del nascituro e per la gestione di gravidanza . 
per questo motivo , la valutazione delle dimensioni dei ventricoli laterali deve essere parte integrante degli esami ecografici del secondo e terzo trimestre , in accordo con la antepartum obstetrical ultrasound examination guidelines [ 20 ]  . 
two large series of patients examined with mr [ 7 , 25 ] have shown a correlation between the size of the lateral ventricles and ventricular morphology , on the one hand , and the presence of underlying cns abnormalities , on the other . 
in particular , the presence of colpocephaly or the parallel appearance of the frontal horns was in general associated with total or partial agenesis of the corpus callosum [ 7 ]  . in our series , 10 / 13 fetuses ( 77% ) with agenesis or hypogenesis of the corpus callosum showed alteration of ventricular morphology . 
in 7 / 13 fetuses ( 54% ) , agenesis was associated with other abnormalities , in agreement with the data in the literature , according to which the association between corpus callosum agenesis and other cns malformations is described as varying from 50% to 85% of cases [ 18 , 19 ]  . 
one particular feature of our findings was the fact that 4 / 5 ( 80% ) cases of hypogenesis were associated with other malformations against the 3 / 8 ( 37% ) cases of total agenesis ( table 1 )  . 
in our series , mr was able to identify 100% of cases of total isolated agenesis ( 5 / 8 cases ) , of which 3 / 8 cases were suspected at us . 
in addition , in two cases , mr visualised the corpus callosum in its entire extension , thus making possible the diagnosis of mild isolated ventriculomegaly and not confirming the us suspicion of agenesis . dellecografia nellidentificazione dellagenesia del corpo calloso assai variabile in letteratura : dal 28% di dercole et al . 
in letteratura , due grandi serie di pazienti esaminati mediante rm [ 7 , 25 ] hanno dimostrato correlazione tra dimensione dei ventricoli laterali e morfologia ventricolare con la presenza di anomalie sottostanti a carico del snc . 
in particolare , la presenza di colpocefalia o di aspetto parallelo delle corna frontali era in genere associata ad agenesia totale o parziale del corpo calloso [ 7 ]  . nella nostra casistica 10 / 13 feti ( 77% ) , con agenesia od ipogenesia del corpo calloso , dimostravano unalterazione della morfologia ventricolare ; in 3 / 13 ( 23% ) casi , tutti di agenesia parziale , la morfologia risultava invece conservata a fronte di una dilatazione ventricolare isolata . 
in 7 / 13 feti ( 54% ) la agenesia risultata associata ad altre anomalie , in accordo con i dati della letteratura secondo i quali lassociazione tra agenesia del corpo calloso ed altre malformazioni dellencefalo descritta in una percentuale variabile tra il 50% e l85% dei casi [ 18 , 19 ]  . 
un aspetto particolare dei nostri risultati stato rappresentato dal fatto che 4 / 5 ( 80% ) delle ipogenesie si associavano ad altre malformazioni contro i 3 / 8 ( 37% ) casi di agenesia totale ( tabella 1 )  . 
nella nostra casistica la rm stata in grado di identificare il 100% delle agenesie totali isolate ( 5 / 8 casi ) , di questi 3 casi erano stati sospettati allecografia . 
in 2 casi inoltre la rm ha visualizzato il corpo calloso in tutta la sua estensione ponendo diagnosi di ventricolomegalia lieve isolata e non confermando il sospetto ecografico di agenesia . table 1 mild cerebral ventriculomegaly and agenesis of the corpus callosum ( n = 13 ) isolated associated with other malformations complete agenesis of corpus callosum partial agenesis of corpus callosum dandy - walker syndrome ( n = 2 ) lissencephaly ( n = 1 ) dandy - walker syndrome ( n = 1 ) lissencephaly ( n = 1 ) myelomeningocele ( n = 1 ) myelomeningocele , cerebellar hernia in trisomy 21 ( n = 1 ) sindrome di dandy - walker ( n = 2 ) lissencefalia ( n = 1 ) sindrome di dandy - walker ( n = 1 ) lissencefalia ( n = 1 ) mielomeningocele ( n = 1 ) mielomeningocele , ernia cerebellare in trisomia 21 ( n = 1 ) tabella 1 ventricolomegalia cerebrale lieve ed agenesia del corpo calloso ( n = 13 ) isolata associata con altre malformazioni agenesia completa del corpo calloso agenesia parziale del corpo calloso total totale radiol med ( 2010 ) 115 : 301312 one limitation of our study was the presence of a systematic error ( bias ) regarding selection of the patient population in that the fetuses enrolled already had a diagnosis or suspected diagnosis of corpus callosum agenesis at us . 
this explains the elevated prevalence of corpus callosum agenesis found in our study population ( 39% ) , which is higher than reported in the literature [ 9 , 19 , 26 ]  . in conclusion , ventricle size does not reflect the severity of the neurological condition , given that 54% of fetuses had severe associated abnormalities in the presence of a mild ventricular dilatation , thus emphasising the importance of a thorough study of fetuses that present even mild ventriculomegaly , in agreement with rickard et al [ 27 ]  . our study also demonstrated that the alteration in ventricular morphology is a reliable tool for diagnosing corpus callosum agenesis . 
this diagnosis is crucial for prenatal consultation in that these forms are characterised by neurological development within the norm . uno dei limiti del nostro studio rappresentato dalla presenza di un errore sistematico ( bias ) di selezione della popolazione dei pazienti : in quanto sono stati arruolati feti che avevano una diagnosi o un sospetto diagnostico di agenesia del corpo calloso allesame ecografico . 
questo rende ragione dellelevata prevalenza di agenesie di corpo calloso ritrovate nella nostra popolazione di pazienti ( 39% ) , che superiore a quelle riportate in letteratura [ 9 , 19 , 26 ]  . in conclusione , le dimensioni ventricolari non rispecchiano la gravit del quadro neurologico dato che il 54% dei feti presentavano gravi anomalie associate a fronte di una dilatazione ventricolare di grado lieve , sottolineando limportanza di un attento studio dei feti che presentano ventricolomegalia anche di modesta entit , in accordo con rickard et al . 
n. , istituto di ricerca diagnostica e nucleare , via pansini 5 , 80131 napoli , italy 2dipartimento di scienze biomorfologiche e funzionali , institute of bio - structure and bio - imaging , via posillipo 196 , 80123 napoli , italy 3dipartimento di chirurgia generale , geriatrica , oncologica e tecnologie avanzate , universit degli studi di napoli federico ii , napoli , italy correspondence to : m . 
both examinations were evaluated qualitatively and semiquantitatively with calculation of the mean percentage variation of the standard uptake values ( % suv max ) between pet - 1 and pet - 2 . 
tutte le lesioni che mostravano un suvmax2 , 5 alla pet - 1 o un incremento nei valori di suv , tra pet - 1 e pet - 2 , sono state considerate maligne . 
viceversa , le lesioni che mostravano un suvmax < 2 , 5 alla pet - 1 o una diminuzione dei valori di suv tra pet - 1 e pet - 2 , sono state considerate benigne . 
queste variazioni di captazione di fdg tra pet - 1 e pet - 2 , rappresentano un parametro affidabile , che pu essere utilizzato nella differenziazione tra lesioni benigne e maligne della mammella . parole chiave carcinoma mammella 18f - fdg - pet - ct acquisizione in doppia fase identificazione di lesione introduction introduzione breast carcinoma is the most common malignant tumour and the second cause of cancer death among women in western countries [ 1 ]  . 
currently , the main strategy for reducing mortality due to breast cancer is early diagnosis . conventional mammography and ultrasonography ( us ) are the most widely used techniques for early diagnosis of breast cancer . 
a number of studies have demonstrated that fdg uptake continues to increase for several hours after the injection of the radiotracer in various il carcinoma della mammella il tumore maligno pi comune e la seconda causa di morte per cancro tra le donne nei paesi occidentali [ 1 ]  . 
tuttavia , queste tecniche hanno una limitata sensibilit e specificit , in particolare nelle pazienti con parenchima mammario denso o con protesi mammarie e nella valutazione delle cicatrici post - chirurgiche . 
la tomografia ad emissione di positroni con 18ffluorodesossiglucosio ( 18f - fdg - pet - ct ) stata recentemente proposta nella diagnosi e nella stadiazione delle pazienti con carcinoma della mammella . 
tuttavia , il ruolo della pet , per la valutazione iniziale del tumore della mammella alquanto incerto , per la variabilit dei valori di sensibilit e specificit , riportati in letteratura . 
malignant tumours were classified according to the world health organisation ( who ) nomenclature and were staged using the tumour - node - metastasis ( tnm ) system . mammography two bilateral mammograms ( alpha rt , instrumentarium , finland ) were performed at our centre , with craniocaudal and mediolateral view , targeted compression and acquisition of additional views where indicated . 
the [ 18f ] - fdg ( 5.2 mbq / kg body weight ) was intravenously administered through a catheter in an antecubital vein of the arm contralateral to the suspicious lesion . 
diversi studi hanno dimostrato che la captazione di fdg continua ad incrementare per diverse ore dopo liniezione del tracciante in diversi tumori maligni [ 4 ] e studi preliminari hanno dimostrato i vantaggi di una seconda acquisizione tardiva nelle pazienti con tumore mammario primario [ 5 , 6 ]  . 
 scopo di questo studio stato quello di valutare laccuratezza diagnostica della 18fdg - pet - ct , eseguita in posizione prona e con doppia tecnica di acquisizione , nelle pazienti con sospetta neoplasia mammaria rispetto alla tecnica 18f - fdg - pet - ct convenzionale eseguita con singolo tempo di acquisizione . materiali e metodi pazienti sono state studiate quarantotto pazienti ( et media 5412 anni ) con una sospetta lesione della mammella , rilevata allesame clinico , alla mammografia e / o allesame ecografico . 
non sono state incluse nello studio , le pazienti che erano in stato di gravidanza , in allattamento , di et inferiore ai 18 anni , o che avevano in anamnesi una storia personale di cancro al seno ipsilaterale o controlaterale o che erano state sottoposte ad esame citologico prima della 18f - fdg - pet - ct . 
i dettagli dello studio sono stati spiegati da un medico e il consenso informato stato ottenuto da tutte le pazienti . tutte le pazienti sono state sottoposte a intervento chirurgico entro 10 giorni dallesame 18f - fdg - pet - ct . 
i tumori maligni sono stati classificati secondo la nomenclatura dellorganizzazione mondiale per la sanit ( oms ) e sono stati stadiati utilizzando il sistema tumore - nodulo - metastasi ( tnm )  . mammografia due mammografie bilaterali ( alpha rt , instrumentarium , finlandia ) sono state eseguite presso il nostro istituto , con proiezioni in cranio - caudale e medio - laterale obliqua , con la compressione mirata e con lacquisizione di altre proiezioni , laddove indicato . 
i risultati della mammografia sono stati riportati da un esperto di diagnostica per immagini senologica ( ar con 20 anni di esperienza nellimaging del seno ) utilizzando lamerican college of radiology breast imaging reporting and data system ( bi - rads ) categories [ 7 ]  . 18f - fdg - pet - ct tutte le pazienti sono rimaste a digiuno per almeno 68 ore prima dellesecuzione dellesame pet , e hanno avuto , al 218 radiol med ( 2010 ) 115 : 215224 pet scanner ( discovery bs , ge medical systems , milwaukee , wi , usa , advance nxi )  . 
the pet / ct study included an initial full - body acquisition in the supine position and in axial planes from the head to the pelvis with a 16 - slice spiral ct scanner using the following acquisition parameters : 140 kv , 80 mas , 0.8 s gantry rotation time , pitch 6 : 1 and slice thickness 4.25 mthe pet acquisition was then performed in the same axial planes with 4 - min acquisitions per patient table position . 
ct data were used for attenuation correction , and images were reconstructed using a conventional interactive algorithm . pet - ct data analysis data were analysed at a workstation with image fusion techniques ( xeleris , ge medical systems ) in the coronal , sagittal and axial planes as well as three - dimensional views [ maximum intensity projection ( mip ) ]  . 
a semiquantitative analysis was performed by an expert in nuclear medicine ( mgc ) with 10 years of experience , and an evaluation of all the series of images acquired was included . 
slice thickness and reconstruction increment were 4 m the standard uptake value ( suv ) in the roi was then calculated using the following formula : mean activity of the roi [ mbq / g ] / ( dose injected ) [ mbq ] / body weight ( g ) , where g = grams . 
the maximum suv ( suvmax ) was measured from the roi , which was placed over the suspicious breast lesion and showed the greatest fdg uptake in both pet - 1 ( suvmax - 1 ) and pet - 2 ( suvmax - 2 )  . 
il 18f - fdg ( 5 , 2 mbq / kg di peso corporeo ) stato somministrato per via endovenosa , attraverso un catetere a permanenza inserito in una vena antecubitale e controlaterale al sito della sospetta lesione . 
lo studio pet - ct ha incluso una prima acquisizione di tutto il corpo , in posizione supina e secondo piani assiali , dalla testa al bacino , con una tomografia computerizzata ( tc ) spirale a 16 strati utilizzando i seguenti parametri di acquisizione : 140 kv , 80 mas , 0 , 8 s per ogni rotazione , pitch 6 : 1 e spessore di fetta di 4 , 25 millimetri . 
subito dopo la scansione dellintero corpo , stata acquisita una seconda serie di immagini della mammella , in posizione prona ( pet - 1 ) ; il tempo di acquisizione per lo studio pet di emissione , stato di 5 minuti per campo di vista , entrambe le braccia sono state posizionate al di sopra della testa delle pazienti per garantire il libero penzolare delle mammelle , evitando in tal modo la compressione e la deformazione delle stesse . dopo 3 ore , stata effettuata una seconda acquisizione pet , in posizione prona ( pet - 2 )  . 
i dati tc sono stati utilizzati per la correzione dellattenuazione e le immagini sono state ricostruite utilizzando un algoritmo convenzionale interattivo . pet - ct e analisi dei dati i dati sono stati analizzati su una stazione di lavoro con tecnica di fusione delle immagini ( xeleris , ge medical systems , milwaukee , usa ) secondo piani coronali , sagittali e assiali , nonch proiezioni tridimensionali ( maximum intensity projection , mip )  . 
unanalisi semi - quantitativa stata eseguita da un esperto di medicina nucleare ( mgc con 10 anni di esperienza in medicina nucleare ) ed stata inclusa una valutazione di tutte le serie di immagini acquisite . 
sia lo spessore , che lintervallo di ricostruzione della fetta sono stati entrambi di 4 m da queste roi , il corrispondente valore di captazione standard ( suv ) stato calcolato applicando la seguente formula : attivit media della roi [ mbq / g ] / ( dose iniettata ) [ mbq ] / peso corpo ( g ) , dove g = grammi . 
il valore massimo di suv ( suvmax ) stato misurato dalla roi , che era posizionata in corrispondenza della radiol med ( 2010 ) 115 : 215224 value were calculated using standard criteria [ 8 ]  . 
tumour size ranged from 7 to 30 mm , with a mean of 167 ma total of 37 lesions were > 10 mm , and the remaining 22 lesions were 10 m of the 11 benign lesions , seven were areas of adenosis and / or fibrocystic disease and four were fibroadenomas . 
for lesions > 10 mm ( n = 37 ) , the dual - time - point acquisition showed values of accuracy , sensitivity and specificity of 89% , 88% and 100% against the 76% , 74% ( both p < 0.001 ) and 100% ( p = n.s. ) of the single - time - point acquisition ( table 2 )  . 
for lesions 10 mm ( n = 22 ) , dual - time - point imaging showed values of accuracy , sensitivity and specificity of 77% , 64% and 100% against the 59% , 36% ( both p < 0.001 ) and 100% ( p = n.s. ) of single - time - point imaging ( table 3 )  . 
tutte le lesioni che mostravano un suvmax2 , 5 alla pet - 1 o un incremento nei valori di suv tra pet - 1 e pet - 2 , sono state considerate maligne . 
viceversa , le lesioni che mostravano un suvmax < 2 , 5 alla pet - 1 o una diminuzione dei valori di suv tra pet - 1 e pet - 2 , sono state considerate benigne . analisi statistica i risultati delle acquisizioni [ 18f ] - fdg - pet - ct in fase precoce e tardiva , sono stati classificati sulla base dei risultati finali isto - patologici come vero positivo , vero negativo , falso positivo o falso negativo per neoplasia . 
la dimensione dei tumori era compresa tra 7 e 30 mm , con una dimensione media di 167 mtrentasette lesioni risultavano > 10 mm , le restanti 22 lesioni , erano 10 mdelle 11 lesioni benigne , 7 sono risultate aree di adenosi e / o malattia fibrocistica e 4 fibroadenomi . 
well - differentiated carcinoma and lobular carcinoma , show low levels of [ 18f ] - fdg uptake [ 9 ] , especially when the study technique involves a single pet - ct acquisition in the early phase [ 3 ]  . 
various studies have demonstrated the utility of suv measurements for the semiquantitative diagnostica dell85% , per le lesioni con un suvmax2 , 5 e / o con % suv max positivo , con valori di sensibilit e specificit dell81% e 100% , rispettivamente , rispetto al 69% , 63% ( entrambe p < 0 , 001 ) e 100% ( p = non stimabile ) della singola acquisizione ( tabella 1 )  . 
per lesioni > 10 mm ( n = 37 ) , laccuratezza diagnostica , la sensibilit e la specificit della 18f - fdg - pet - ct eseguita con doppia tecnica di acquisizione , sono risultate pari a 89% , 88% e 100% verso 76% , 74% ( entrambe p < 0 , 001 ) e 100% ( p = non stimabile ) della singola acquisizione ( tabella 2 )  . 
per lesioni 10 mm ( n = 22 ) , la doppia tecnica di acquisizione ha mostrato valori di accuratezza diagnostica , di sensibilit e di specificit del 77% , 64% e 100% verso 59% , 36% ( entrambe p < 0 , 001 ) e 100% ( p = non stimabile ) della singola acquisizione ( tabella 3 )  . 
limmagine di fusione pet - tc ottenuta secondo il piano assiale ed in posizione prona , mostra unarea focale di patologica captazione di fdg , in corrispondenza del quadrante superiore esterno ( qse ) della mammella sinistra , che mostra valori di suvmax pari a 2 , 4 alla pet - 1 ( a ) e 3 , 6 alla pet - 2 ( b )  . evaluation of the degree of [ 18f ] - fdg uptake in various tumours . 
this semiquantitative parameter enables the differentiation between benign and malignant nodules in some tumours [ 10 ] , and most studies conclude that a threshold value of 2.5 is ideal for obtaining elevated sensitivity while at the same time maintaining good specificity [ 11 ]  . 
 benigne non hanno mostrato nessun cambiamento , o una diminuzione dei valori di suvmax tra pet - 1 e pet - 2 , con % suvmax di 217 ( p < 0 , 001 )  . 
uno dei motivi principali di questa limitazione , stato che alcuni tipi di cancro al seno , come ad esempio i carcinomi ben differenziati e i carcinomi lobulari della mammella , mostrano bassi livelli di captazione di 18f - fdg [ 9 ] in particolare utilizzando una tecnica di studio che prevede una singola acquisizione pet - tc in fase precoce [ 3 ]  . 
tale parametro semiquantitativo , permette di differenziare i noduli benigni e maligni , in alcuni tipi di neoplasie [ 10 ] e la maggior parte delle pubblicazioni conclude che un valore soglia di 2 , 5 ideale per ottenere unelevata sensibilit , mantenendo allo stesso tempo , una buona specificit [ 11 ]  . 
 [ 13 ] hanno effettuato scansioni con doppia acquisizione su 21 pazienti , con 18 tumori maligni della testa e del collo , e 9 lesioni infiammatorie o infettive . gli autori hanno osservato , che i tumori maligni mostravano un incremento medio dei valori di suv del 12% , tra la prima e la seconda acquisizione , mentre le lesioni infiammatorie e le strutture con fisiologica captazione di 18f - fdg ( lingua , laringe ) , mostravano una captazione sostanzialmente stabile nel tempo o un leggero calo nei valori di suv . in uno studio condotto su 36 pazienti con sospette lesioni polmonari , matthies et al . 
 [ 4 ] hanno ottenuto risultati simili ; in questo studio il valore di suv delle lesioni mostrava un incremento nelle acquisizioni tardive rispetto alle precoci ( 4 , 42 , 4 vs 3 , 71 , 9 )  . 
this , in fact , seems to be the best tradeoff between extraction of the radiotracer by tumour cells and the effective half - life of the tracer , which is 110 mhowever , a number of different acquisition protocols have been proposed . 
the authors observed that the malignant tumours displayed a mean increase in suv of 12% between the first and second acquisition , whereas inflammatory lesions and structures with a physiological uptake of [ 18f ] - fdg ( tongue , larynx ) showed a substantially stable uptake over time or a slight fall in suv . 
 [ 14 ] studied 15 patients with hepatic malignancies ( 11 with hepatocellular carcinoma and four with colorectal liver metastasis ) with dual - time - point pet ( 1 and 2 h after fdg administration ) and concluded that the delayed images provided no advantages in patients with hepatocellular carcinoma . 
 [ 16 ] used a protocol involving early and delayed imaging ( 1 and 2 h after fdg administration ) in a group of 86 patients with suspected pancreatic cancer . in this study , the mean suv of neoplastic lesions in delayed acquisitions showed a highly significant increase , and delayed images identified new foci of liver metastases that were not visible in early acquisitions . in our study , we tackled the problem of the low sensitivity of pet examination in identifying pathological uptake in the breast and evaluated whether the acquisition of delayed images could be a realistic solution . 
various studies support this hypothesis , and in fact , most breast cancers display a gradual increase in suv over time after the injection of [ 18f ] - fdg [ 5 , 6 ]  . 
in agreement with these studies , we found that malignant studiato 15 pazienti con neoplasie a livello epatico ( 11 con epatocarcinoma e 4 con metastasi epatiche da carcinoma del retto ) con acquisizione dellesame pet in due fasi ( 1 e 2 ore dopo la somministrazione di fdg ) , concludendo che le immagini tardive , nei pazienti con epatocarcinoma , non portano nessun beneficio ; questo risultato va probabilmente imputato al fatto che il metabolismo tumorale nellepatocarcinoma ben differenziato simile a quello del tessuto epatico sano [ 15 ] ; mentre le acquisizioni tardive miglioravano la visualizzazione delle metastasi epatiche nei pazienti con carcinoma del retto [ 14 ]  . 
 [ 16 ] hanno utilizzato un protocollo che prevedeva lacquisizione precoce e tardiva ( 1 e 2 ore dopo la somministrazione del radiofarmaco ) in un gruppo di 86 pazienti con lesioni pancreatiche di sospetta natura neoplastica . 
in questo studio , il valore di suv medio delle lesioni neoplastiche nelle acquisizioni tardive mostrava un aumento molto significativo e le immagini tardive evidenziavano localizzazioni epatiche di natura ripetitiva , non visibili nelle acquisizioni precoci . 
 nel presente lavoro stato affrontato il problema della bassa sensibilit dellesame pet nella identificazione di accumuli patologici a livello mammario ed stato valutato se la riacquisizione di immagini tardive possa rappresentare una realistica soluzione . 
questo comporta una migliore identificazione degli accumuli patologici di fdg e quindi aumenta la sensibilit dellesame pet . questi risultati sono indipendenti dalla localizzazione del tumore primitivo e dal suo istotipo . 
diversi studi in letteratura sostengono tale ipotesi , infatti la maggioranza delle neoplasie della mammella mostra un graduale incremento dei valori di suv nel tempo , dopo liniezione di 18f - fdg [ 5 , 6 ]  . 
queste variazioni dei valori di suv nel tempo rappresentano un parametro affidabile , che pu essere utilizzato per differenziare le lesioni benigne della mammella da quelle maligne . in particolare , per le lesioni che mostrano un suvmax2 , 5 e / o un % suvmax positivo , la doppia acquisizione della 18f - fdg - pet - ct in posizione prona , mostra una maggiore accuratezza diagnostica rispetto alla singola acquisizione ( 85% vs 69% )  . 
la capacit della pet di identificare il cancro al seno , dipende molto anche dalle dimensioni del tumore ; nel nostro studio , la sensibilit complessiva della doppia acquisizione 18f - fdg - pet - ct , per lesioni > 10 mm ( n = 37 ) , stata dell88% vs 74% della singola acquisizione . radiol med ( 2010 ) 115 : 215224 lesions showed a significant increase in [ 18f ] - fdg over time compared with benign lesions . 
 sebbene la doppia acquisizione 18f - fdg - pet - ct risolva in parte i problemi legati alla localizzazione della lesione , la limitata risoluzione spaziale della metodica ed i costi elevati , ne scoraggiano lapplicazione clinica di routine in fase di screening e nella diagnosi del tumore della mammella primitivo , in particolar modo per le lesioni < 1 cm [ 18 , 19 ]  . 
la recente introduzione di apparecchiature pet dedicate per la mammella , positron emission mammography ( fdg - pem ) consente di studiare con elevatissima risoluzione spaziale lesioni con dimensioni < 1 , 5 mm , conservando una elevata risoluzione di contrasto che risulta superiore alle apparecchiature pet convenzionali [ 20 , 21 ]  . 
 un recente studio multi - centrico ha dimostrato lutilit e la elevata accuratezza diagnostica della fdg - pem nella identificazione di focolai di carcinoma in situ della mammella , confermando lutilit di tale apparecchiatura dedicata ed aprendo nuove prospettive nellimaging non invasivo del tumore primitivo della mammella [ 22 ]  . 
in particolare , nel tumore mammario primitivo si apprezza un progressivo incremento della captazione di fdg nel corso del tempo , viceversa , le lesioni benigne mostrano una diminuzione della captazione di fdg . 
 lesame 18f - fdg - pet - ct con acquisizione tardiva effettuato in posizione prona va preferito allesame 18ffdg - pet - ct con singola acquisizione , e raccomandato quando si studiano pazienti con sospetto tumore maligno della mammella . 
bassiano , bassano del grappa ( vi ) , via dei lotti 40 , 36061 bassano del grappa ( vi ) , italy 3uo radiologia diagnostica ed interventistica , azienda ospedaliera santa maria , terni , italy 4strutture complessa di radiologia , ospedale bellaria , bologna , italy 5istituto di radiologia , ospedale ss annunziata , chieti , italy correspondence to : r . 
we retrospectively reviewed hrct scans of 29 patients ( 9 men , 18 women ; mean age 63 years , range 3888 years ) with positive culture from bronchial wash . 
sono stati rivalutati retrospettivamente gli esami hrct di 27 pazienti ( 9 maschi e 18 femmine ; et media 63 anni , range 3888 anni ) con diagnosi microbiologica ( esame colturale del broncoaspirato ) di infezione da ntm . 
in tutti i pazienti era presente il m . avium complex ( mac ) , tranne in uno in cui il ntm rimasto indefinito ; in 6 pazienti vi era associazione di mac con m . 
the presence of bronchiectasis , cavitary nodules with feeding bronchus sign and tree - in - bud nodules in the middle lobe and lingula are suggestive of ntm infection , thus assisting the physician in the diagnostic workup of these patients . keywords mycobacteria pulmonary infections bronchiectasis hrct tree - in - bud hrct ( 7 / 8 , 87 , 5% ) , vetro smerigliato ( 3 , 11 , 1% ) , quadro reticolare / reticolo - nodulare ( 6 , 22 , 2% ) , bronchiettasie ( 25 , 92 , 5% ) , noduli centrolobulari ( albero con gemme ) ( 24 , 88 , 8% ) , air trapping ( 8 , 29 , 6% ) , linfonodi con diametro > 1 cm ed eventuali calcificazioni ( 13 , 3 con calcificazioni , 48 , 1% ) , versamento pleurico ( 2 , 7 , 4% )  . 
in 3 dei 7 pazienti con noduli maggiori di 1 cm e con cavitazione stato individuato il feedings bronchus sign , cio la presenza di un bronco dilatato con pareti ispessite , a contatto con il nodulo escavato . 
la presenza di bronchiettasie , di noduli escavati con il feedings bronchus sign e di noduli centrolobulari ad albero con gemme , con distribuzione prevalente nel lobo medio e nella lingula devono suggerire la possibilit di infezione da nmt , e orientare cos il clinico verso la ricerca del germe responsabile . parole chiave infezione polmonare da micobatteri non tubercolari bronchiettasie hrct albero con gemme hrct introduction introduzione ( hiv ) infection immunodeficiency virus the frequency of nontuberculous mycobacteria ( ntm ) pulmonary infection in immunocompetent patients without human constantly increasing [ 1 ]  . 
in physiological conditions these organisms are ubiquitous saprophytes and can be isolated from the respiratory tract in healthy individuals without evidence of tissue invasion or real infection ( so - called colonisation )  . 
however , in certain groups of individuals ( especially the elderly , patients with severe chronic bronchopneumonia or achalasia , or even without predisposing factors ) , a real pulmonary infection develops , although characterised by vague clinical symptoms [ 2 , 3 ]  . when this type of infection strikes female individuals , it is known as lady windermere syndrome and characterised radiologically by the presence of bronchiectasis in the middle lobe and the lingula [ 46 ]  . it should be noted that on the basis of the chest x - ray alone , ntm infections are indistinguishable from m . 
 [ 7 ] identify ntm infections in patients without previous la frequenza delle infezione polmonari da micobatteri non tubercolari o atipici ( ntm ) in pazienti non immunodepressi per infezione da virus dellimmunodeficienza acquisita umano ( hiv ) in continuo aumento [ 1 ]  . 
in condizioni fisiologiche questi organismi sono saprofiti ubiquitari e possono essere isolati dallalbero respiratorio di individui sani senza evidenza di invasione tissutale o di vera infezione ( cosiddetta colonizzazione )  . 
ma in alcuni gruppi di persone ( in particolare soggetti anziani , pazienti con grave broncopneumopatia cronica o con acalasia , o anche senza fattori predisponenti ) si sviluppa una vera e propria infezione polmonare , caratterizzata per da scarsa sintomatologia clinica [ 2 , 3 ]  . questo tipo di infezione , quando colpisce pazienti di sesso femminile , nota anche come sindrome di lady windermere ed caratterizzata radiologicamente dalla presenza di bronchiettasie localizzate nel lobo medio e nella lingula [ 46 ]  . 
 da sottolineare che le infezioni causate da ntm sono indistinguibili con il solo radiogramma del torace da quelle radiol med ( 2010 ) 115 : 191204 pulmonary abnormalities , with pulmonary nodules as the predominant radiological sign . 
as a result , the clinical diagnosis is often difficult to arrive at without the support of invasive examinations such as bronchoscopy , even though radiological findings may be suggestive of this type of infection in the appropriate clinical setting . it follows that a specific clinical diagnosis is in general difficult to make without performing pulmonary biopsy , although there are several radiological signs that , when correlated with clinical and laboratory findings , are suggestive of this type of infection . 
although numerous studies , one very recent [ 8 ] , have described the contribution of high - resolution computed tomography ( hrct ) in the evaluation of this disease in non - hiv - positive patients , in daily practice , it may still prove difficult to link the radiological findings - mainly bronchiectasis - to ntm infection and thus allow an early diagnosis of the infection and appropriate and timely treatment . therefore , since there is a reasonable gap between evidence and experience , we reviewed the hrct signs reported in the literature and compared them with those seen in patients with this disease , with the aim of demonstrating that ntm infection is not so uncommon and that the diagnosis may be suggestive to the clinician and microbiologist on the basis of the radiological pattern alone . materials and methods we included in our retrospective study 27 consecutive patients examined in four different centres ( 9 men and 18 women , mean age 636 ) between 1 january 2002 and 28 february 2008 who satisfied the inclusion criteria : positive microbiological culture ; radiological findings compatible with ntm infection ( chest x - ray and hrct ) ; with or without respiratory symptoms ( dyspnoea , cough , haemoptysis ) and systemic symptoms ( fever , weight loss , fatigue )  . exclusion criteria were hiv - positive status , positive microbiological culture with radiological findings incompatible with ntm infection and negative microbiological test with radiological findings compatible with infection . 
 [ 7 ] riconobbero per primi linfezione da ntm in pazienti senza precedenti alterazioni polmonari , con un quadro radiologico in cui il segno dominante era rappresentato da noduli polmonari . 
di conseguenza la diagnosi clinica spesso difficile da raggiungere senza il supporto di indagini invasive quali la broncoscopia , anche se gli aspetti radiologici possono essere suggestivi di questo tipo di infezione in un adeguato contesto clinico . 
ne consegue che una diagnosi clinica specifica generalmente difficile da formulare senza ricorrere alla biopsia polmonare ; esistono tuttavia alcuni aspetti radiologici che , opportunamente correlati ai dati clinico - laboratoristici , possono essere suggestivi di questo tipo di infezione . 
 anche se molti lavori , lultimo dei quali molto recente [ 8 ] , hanno gi descritto lapporto della tomografia computerizzata ( tc ) ad alta risoluzione ( hrct ) nella valutazione di questa malattia in pazienti non hiv positivi , nella pratica quotidiana pu risultare ancora difficile collegare quadri radiologici caratterizzati prevalentemente da bronchiettasie allinfezione da ntm consentendo una diagnosi precoce di infezione al fine di mettere in atto una terapia adeguata e tempestiva . quindi , esistendo ancora un discreto divario tra evidenza ed esperienza , sono stati rivalutati i segni hrct riportati in letteratura , confrontandoli con quelli presenti nei pazienti con questa malattia da noi valutati , allo scopo di dimostrare come linfezione da ntm non sia cos infrequente e come sia possibile suggerirla al clinico e al microbiologo , a volte solo sulla base del pattern radiologico . materiali e metodi dal 1 gennaio 2002 al 28 febbraio 2008 abbiamo incluso nel nostro studio retrospettivo 27 pazienti consecutivi provenienti da quattro centri differenti ( 9 maschi e 18 femmine , et media 636 ) e che soddisfacevano i seguenti criteri di inclusione : esame microbiologico colturale positivo ; quadro radiologico compatibile con infezione da ntm ( radiografia del torace e hrct ) ; con o senza sintomi respiratori ( dispnea , tosse , emoftoe ) e sistemici ( febbre , calo ponderale , astenia )  . 
sono stati esclusi dallo studio i pazienti hiv + , quelli con esame microbiologico positivo per ntm ma quadro radiologico non compatibile con infezione da ntm e quelli con esame microbiologico negativo ma quadro radiologico compatibile con infezione . 
 in tutti i pazienti stata valutata la presenza di eventuali fattori di rischio come fumo di sigaretta , abuso di alcol , 194 radiol med ( 2010 ) 115 : 191204 microbiological diagnosis was made in all patients with culture of the bronchial aspirate according to criteria recommended by the american thoracic society in 2007 and reported in table 1 [ 9 ]  . 
the examinations were performed with both the traditional technique ( slice thickness 1 mm , interval 10 mm , bone reconstruction algorithm ) and the volumetric technique , with subsequent reconstruction of adjacent sections with a thickness between 0.6 and 1 mm and a bone reconstruction algorith all hrct examinations were performed without contrast material administration with breath - hold acquisition from the lung apices to the lung bases and were completed with a scan at end - expiration acquired with the traditional hrct technique . 
transbronchial or other lung biopsy with mycobacterial features ( granulomatous inflammation or acid - fast bacillus ) and positive for ntm mycobacteria or biopsy showing mycobacterial histopathological features ( granulomatous inflammation or acid - fast bacillus ) and one or more sputum or bronchial washings that are culture positive for ntm apatients suspected of having ntm lung disease but do not meet the diagnostic criteria should be followed up until the diagnosis is firmly established or excluded hrct , high resolution computed tomography tabella 1 criteri diagnostici dellamerican thoracic society nellinfezione polmonare da micobatteri non tubercolari ( ntm ) a criteri clinici 1 . 
the radiologists reviewed patients hrct signs ( each for the group imaged at their own centre ) independently of the previous report to evaluate whether the findings justified a radiological suspicion of ntm infection and to list the most significant signs of this disease . 
tutti gli esami hrct sono stati effettuati senza somministrazione di mezzo di contrasto , dagli apici alle basi polmonari , in apnea inspiratoria e sono stati sempre completati da successivo esame in espirio condotto con tecnica hrct tradizionale , mediante scansioni ad intervalli di 3 cm dallarco aortico alle basi polmonari , per la valutazione di eventuale intrappolamento aereo . 
i radiologi hanno revisionato i segni hrct dei pazienti ( ognuno per il gruppo appartenente al proprio centro ) , indipendentemente dal referto precedente , per valutare se possibile porre il sospetto radiologico di infezione da ntm e quali siano i segni pi indicativi di questo tipo di patologia . 
i segni presi in considerazione nelle immagini hrct [ 10 ] sono riportati nella tabella 2 . si intende per esiti cicatriziali la presenza di strie e distorsione cicatriziale in corrispondenza degli apici polmonari ; per addensamento parenchimale laumento omogeneo della densit del parenchima polmonare , che nasconde i vasi e le pareti dei bronchi , associato o meno a broncogramma aereo ; per nodulo solitario / multipli ( diametro > 1 cm ) la presenza di opacit rotondeggianti abbastanza ben marginate , a distribuzione random , omogenee o con cavitazione dei noduli ; per vetro smerigliato laumento omogeneo della densit del parenchima polmonare con conservato riconoscimento dei vasi e dei bronchi sottostanti ; per quadro reticolare / reticolo - nodulare lispessimento regolare , liscio o nodulare , dei setti interlobulari e del connettivo peribroncovascolare ; per bronchiettasie la dilatazione irreversibile dei bronchi lungo tutto il loro decorso anatomico , associato ad ispessimento delle loro pareti ; per noduli centrolobulari ( albero con gemme ) presenza di micronoduli ( < 1 cm ) in sede centrolobulare rispetto al lobulo polmonare secondario , alcuni in rapporto con immagini lineari , per dilatazione del bronchiolo centrolobulare ripieno di essudato ; per air trapping la ridotta densit del parenchima polmonare con ridotta vascolarizzazione , pi evidente nelle scansioni hrct eseguite in espirio , determinata dallostruzione delle vie aeree distali . 
 stata valutata anche la presenza di linfonodi mediastinici ( diametro > 1 cm ) , con eventuali calcificazioni , e di versamento pleurico . tutti i pazienti sono stati trattati con terapia specifica secondo le linee guida dellamerican thoracic society [ 8 ]  . lesame microbiologico colturale su broncoaspirato , consensualmente al quadro clinico hanno documentato leradicazione dellinfezione da ntm . 
in tutti i soggetti al 196 radiol med ( 2010 ) 115 : 191204 walls , either with or without the air bronchogram sign . single or multiple nodules ( diameter > 1 cm ) are defined as the presence of relatively well - defined rounded opacities , with patchy or diffuse distribution or with cavitary nodules . ground glass appearance indicates homogeneous increase in pulmonary parenchyma density , with preserved recognition of vessels and bronchi . 
bronchiectasis indicates irreversible dilatation of the bronchi along their entire anatomical course , associated with bronchial wall thickening . centrilobular nodules ( tree in bud ) are described by the presence of micronodules ( < 1 cm ) in the centre of secondary pulmonary lobules , often connected to linear opacities , and caused by dilation of the centrilobular bronchiole filled with exudate . 
air trapping is defined as reduced pulmonary parenchyma density , with reduced vascularity ( tending to be more pronounced in hrct scans performed at end expiration ) caused by obstruction of the distal airways . 
we also evaluated the presence of mediastinal lymphadenopathy ( diameter > 1 cm ) with possible calcification , and pleural effusion . all patients received specific treatment in accordance with the guidelines of the american thoracic society [ 8 ]  . the microbiological culture on the bronchial aspirate , together with the clinical findings , indicated eradication of the ntm infection . 
nessun paziente ha avuto emoftoe . tutti i soggetti erano di nazionalit italiana , senza storia di abuso di alcolici e 9 ( 33 , 3% ) ( 3 maschi , 6 femmine ) con con storia di fumo ( 10 pack / years )  . 
pregressa infezione tubercolare era anamnesticamente e radiologicamente presente in 5 pazienti ( 18 , 5% ; 3 maschi , 2 femmine ) [ 11 , 12 ]  . nel gruppo 11 pazienti ( 40 , 8% ) presentavano fattori di rischio predisponenti rappresentati da pneumopatie di tipo ostruttivo ( bpco in 4 maschi e 5 femmine e fibrosi cistica in 1 maschio e 1 femmina ) e 12 ( 44 , 4% ) da malattie sistemiche , anche in associazione tra loro ( malattie cardiovascolari in 5 maschi , epatite da virus dellepatite c [ hcv + ] in una femmina , acalasia in 1 femmina , esofagite in una femmina , diabete in 1 maschio e 1 femmina , uso di steroidi in artrite reumatoide e sclerosi multipla in 2 femmine )  . 
le lesioni erano localizzate nei lobi superiori in 23 ( 85 , 1% ) , nel lobo medio / lingula in 25 ( 92 , 5% ) e nei lobi inferiori in 18 ( 66 , 6% ) , con diffusione uniforme in 13 ( 48 , 1% ) e a carta geografica in 17 ( 62 , 9% )  . discussione la diagnosi di infezione da ntm non semplice perch spesso le secrezioni bronchiali di questi pazienti sono contaminate dai micobatteri atipici senza per esitare in infezione clinica manifesta . 
nella maggior parte dei casi i soggetti manifestano sintomi di bronchite cronica o episodi di bronchite acuta ricorrente , altri possono presentare espettorazione produttiva , dispnea , emottisi e dolore toracico . 
infatti a volte difficile capire se i sintomi siano secondari ad una infezione da ntm o siano dovuti alla patologia cronica sottostante che aumenta la suscettibilit allinfezione [ 8 ]  . 
sono anche presenti aree di oligoemia a mosaico con distribuzione a carta geografica in rapporto ad intrappolamento aereo ( asterischi )  . radiol med ( 2010 ) 115 : 191204 fig . 
 discussion the diagnosis of ntm infection is not simple , because often , the bronchial secretions of these patients are contaminated by atypical mycobacteria without clinical evidence of infection . therefore , the presence of suggestive signs and symptoms is essential for making a diagnosis . 
in most cases , patients manifest chronic bronchial symptoms or recurrent episodes of acute bronchitis , whereas others may have productive cough , dyspnoea , haemoptysis and chest pa systemic symptoms such as low - grade fever , weight loss and fatigue are instead particularly present in the advanced forms of infection . 
indeed , it may be difficult to recognise whether the symptoms are secondary to an ntm infection or the result of an underlying chronic disease that increases susceptibility to infection [ 8 ]  . 
patients included in presentano caratteristiche pressoch consistenti con la letteratura con maggior prevalenza dei sintomi respiratori sui sintomi sistemici verosimilmente per la presenza di 11 soggetti su 27 con patologia cronica respiratoria ( bpco e fibrosi cistica )  . in assenza di caratteristiche cliniche e radiologiche suggestive di infezione , la diagnosi va posta sulla scorta di esami microbiologici . 
un unico campione di espettorato positivo per ntm non rappresenta la prova di una infezione attiva , specie quando non si osservano bacilli acido - alcool resistenti ( afb ) allesame microscopico e la coltura evidenzia pochi bacilli . 
la distinzione tra colonizzazione , contaminazione e vera infezione non spesso cos chiara . nel 2007 , lamerican thoracic society ha rivisto i criteri diagnostici ( tabella 2 ) dando molta importanza a colture multiple dei campioni analizzati e alla raccolta di almeno tre campioni di espettorato . 
hrct scan ( b , c ) : centrilobular nodules , tree in bud ( arrow ) , bronchiectasis in the middle lobe and lingua and small consolidations , recognisable also in the coronal multiplanar reconstruction ( d )  . 
lhrct ( b , c ) mette in evidenza sia noduli centrolobulari anche con aspetto di albero con gemme ( freccia ) , sia bronchiettasie del lobo medio e della lingula , con piccoli noduli e consolidazioni , ben evidenti anche dalle mpr nel piano coronale ( d )  . 
una scansione eseguita in espirio ( e ) dimostra intrappolamento aereo nei lobi inferiori per ostruzione anche delle vie aeree distali . radiol med ( 2010 ) 115 : 191204 our study presented characteristics to a large extent in line with those reported in the literature , with a greater prevalence of respiratory symptoms over systemic symptoms probably due to the presence of 11 / 27 patients with chronic respiratory disease ( copd and cystic fibrosis )  . in the absence of clinical and radiological findings suggestive of infection , diagnosis is made on the basis of microbiological tests . 
a single sputum sample positive for ntm is not proof of active infection , especially when no acid - fast bacilli are seen at microscopy and the culture reveals few bacilli . 
distinction between colonisation , contamination and full - blown infection is often unclear . in 2007 , the american thoracic society reviewed the diagnostic criteria ( table 2 ) , emphasising the importance of multiple cultures of the samples tested and collection of at least three sputum samples . 
they also recommended bronchoscopy for the collection of bronchial aspirate , especially in cases of doubtful contamination and in subjects without cavitary lesions . conventional chest x - ray is of little use in that it shows signs that are completely nonspecific , with scarring in the lung apices and occasionally small areas of parenchymal consolidation that , in some cases , disappear with antibiotic therapy and that can be incorrectly interpreted as slowresolving pneumonia . 
the diagnosis of ntm infection of course is more readily suggested in patients without previous respiratory symptoms or prior lung disease in whom the clinical pattern of nonspecific insidious pulmonary infection appears . 
indeed , in agreement with the literature , most of our patients were women ( 18 / 27 , 67% ) , who were not particularly elderly ( mean age 63 ) and were in good clinical condition . 
only in six patients ( 33% ) were chronic pulmonary diseases present , with the finding of the prevalently cavitary pattern in only one of the in the remaining nine male patients , two ( without pulmonary risk factors ) had the bronchiectasis - nodular hrct pattern , whereas remaining patients showed the cavitary pattern . 
in the bronchiectasis - nodular pattern , the middle lobe and lingula were the primary lesion locations ( 92.5% ) , with relative sparing of the lower lobes , whereas the upper lobes were caso di dubbia contaminazione e specialmente in soggetti senza lesioni cavitarie . 
 il radiogramma standard del torace di scarsa utilit in quanto mostra segni del tutto aspecifici , con esiti cicatriziali agli apici e con presenza , a volte , di piccole consolidazioni parenchimali che difficilmente scompaiono dopo terapia antibiotica e che vengono erroneamente interpretate come polmonite a lenta risoluzione . 
sicuramente pi facile ipotizzare la diagnosi di infezione polmonare da ntm in quei pazienti senza precedente sintomatologia respiratoria o pregresse malattie polmonari in cui compaia il quadro clinico di subdola infezione polmonare aspecifica . 
solo in 6 ( 33% ) pazienti erano presenti malattie polmonari croniche , con riscontro della forma prevalentemente cavitaria soltanto in una di esse . dei restanti 9 pazienti maschi , 2 ( senza fattori di rischio polmonare ) presentavano i segni hrct della forma bronchiettasica - nodulare , mentre i restanti mostravano il quadro della forma cavitaria . 
nella forma bronchiectasica - nodulare il lobo medio e la lingula sono risultate le sedi polmonari pi coinvolte ( 92 , 5% ) , con un relativo risparmio dei lobi inferiori , mentre i lobi superiori sono risultati coinvolti prevalentemente nella forma cavitaria ( 85 , 1% )  . 
 molti autori [ 10 , 1720 ] hanno descritto i segni hrct dellinfezione polmonare da ntm in pazienti non hiv + , sia in presenza che in assenza di pregresse malattie polmonari . nel recentissimo lavoro di kuroishi et al . 
 [ 8 ] , micronoduli ( 100% ) , bronchiettasie ( 76% ) , lesioni escavate ( 37% ) , addensamenti parenchimali ( 37% ) e ispessimenti pleurici ( 27% ) sono i segni di pi frequente riscontro nei pazienti senza altra patologia polmonare . 
 [ 8 ] micronodules ( 100% ) , bronchiectasis ( 76% ) , cavitary lesions ( 37% ) , parenchymal consolidation ( 37% ) and pleural thickening ( 27% ) were the most frequent signs in patients without associated lung disease . 
our findings are in agreement with the literature ( tree - in - bud centrilobular nodules in 88.8% of cases ; bronchiectasis in 92.5% ; nodules in 29.6% , of which 87.5% were cavitary ; parenchymal consolidation in 59.2% and no cases of pleural thickening but pleural effusion in 7.4% ) , even though the different percentages of the signs encountered may be due to the presence of patients with underlying lung disease and hrct signs consisting prevalently of a reticular pattern with scarring at the lung apices . in agreement with other authors [ 9 , 1618 ] , we report the predominant sign in the nodular pattern to be centrilobular nodules with the tree - in - bud appearance , which histologically corresponds to ntm granulomas and caseous material in the respiratory and terminal bronchioles , similar to those encountered in classic tuberculous infection . 
large nodules ( diameter > 1 cm ) and parenchymal consolidation histologically correspond to the association of caseous granulomas , nonspecific peripheral inflammation and lymphocyte infiltration , which completely fill the alveoli . 
as the disease progresses , the bronchiectasis extends and new airways are affected , thus confirming the hypothesis that bronchiectasis not only predisposes the patient to infection but is , in turn , caused by ntm infection [ 2123 ]  . as described by kim et al . 
in particular , the sign was identified in patients who had undergone hrct study with volumetric scanners and in whom the anatomical continuity of ct scans enabled visualisation of the bronchus in its entire extension and better evaluation of the relations with nodular lesions . 
 [ 24 ] : the infection at first causes bronchial wall thickening and lumen narrowing , with subsequent development of nodules with peribronchial distribution and consequent formation of cystic bronchiectasis with inflammation that at hrct appears as cavitary consolidation , with destruction of bronchial walls and their cartilage . in this situation , the bronchus drains the necrotic debris within the lesion , thus forming a cavity and causing bronchogenic spread of the infection . tuale diversa dei segni riscontrati pu essere determinata dalla presenza anche di soggetti con patologia polmonare preesistente e segni hrct rappresentati prevalentemente da quadro reticolare con esiti cicatriziali agli apici polmonari . nel nostro lavori , come in quelli di altri autori [ 9 , 1618 ] vengono riportati , come segno predominante nella forma nodulare , i noduli centrolobulari con aspetto di albero con gemme , che corrispondono istologicamente a granulomi da ntm e materiale caseoso nei bronchioli terminali e respiratori , simili a quelli dellinfezione tubercolare classica . 
i grossi noduli ( diametro maggiore di 1 cm ) e gli addensamenti parenchimali corrispondono istologicamente alla associazione di granulomi caseosi , flogosi aspecifica periferica e infiltrati linfocitari che riempiono completamente gli alveoli . 
nellevolversi dellinfezione le bronchiettasie aumentano in estensione e se ne formano di nuove , confermando lipotesi che non solo esse predispongono allinfezione , ma che sono a loro volta causate dalla infezione da ntm [ 2123 ]  . come descritto da kim et al . 
 [ 24 ] , lhrct in grado di dimostrare , in caso di nodi escavati , la presenza di feedings bronchus sign , cio di un bronco dilatato con pareti ispessite , a contatto con il nodulo escavato ; tali autori hanno riscontrato questo segno nel 75% dei 24 pazienti della loro casistica  . 
in particolare esso stato identificato nei pazienti in cui gli esami hrct sono stati effettuati con macchine volumetriche , e nei quali la continuit anatomica delle scansioni tc permette di visualizzare il bronco in tutta la sua estensione e di valutarne meglio i rapporti con le lesioni nodulari . 
 [ 24 ] : linfezione determina allinizio ispessimento delle pareti bronchiali e restringimento del lume , con successivo sviluppo di noduli a distribuzione peribronchiali e conseguente formazione di bronchiettasie cistiche con flogosi che allhrct si manifestano come consolidazioni escavate , con distruzione delle pareti bronchiali e delle loro cartilagini . 
in questa situazione il bronco drena i detriti necrotici allinterno della lesione formando una cavit e determinando la diffusione broncogena dellinfezione . nonostante lestensione importante delle lesioni , segni di intrappolamento aereo sono stati riconosciuti in circa il 30% dei casi e prevalentemente nei pazienti con noduli centrolobulari . 
 [ 25 ] in cui vengono descritte le caratteristiche istopatologiche delle biopsie transbronchiali dei pazienti con infezione da ntm : sono presenti bronchiolettasie con flogosi bronchiale e radiol med ( 2010 ) 115 : 191204 despite the significant extension of the lesions , signs of air trapping were found in only 30% of cases and most often in patients with centrilobular nodules . 
it can be surmised that in the form without granuloma formation , lumen narrowing occurs but distal airways obstruction is still incomplete , which remains patent and therefore without air trapping in the endexpiration scans , at least in the early stages of the disease . our study has a number of limitations . 
the first is due to the fact that examinations were evaluated by a single radiologist who was aware of the final diagnosis , without any diagnostic ( and therefore statistical ) comparison with other studies . 
the series was relatively large in that an additional 14 patients were excluded who had typical hrct signs but were without microbiological evidence of ntm infection , which could have been confirmed if repeated excretion examinations had been performed or if the patients had undergone bronchoscopy . 
lastly , we did not evaluate the differences in hrct pattern on the basis of the different types of ntm infection , which several studies [ 10 , 14 , 26 ] comparedwithout , however , finding any significant differences . 
hrct is instrumental in the recognition and diagnosis of pulmonary infection and , above all , in suggesting a possible ntm infection on the basis of two different imaging patterns . 
in the nodular form , the presence of bronchiectasis , cavitary nodules with the feeding bronchus sign and centrilobular nodules with the tree - in - bud appearance , with a distribution prevalently in the middle lobe and lingula , should lead the radiologist to formulate a tentative diagnosis of ntm infection [ 5 , 14 ] and the clinician to search for the germ responsible [ 26 , 27 ]  . 
in addition , as the incidence of this infection is not so rare , the presence of a nodular pattern on conventional chest x - ray in a patient with a history of repeated pulmonary infections should suggest the need for hrct study . peribronchiale con o senza formazione di granulomi . 
 ipotizzabile che nella forma senza granulomi non vi sia ancora lostruzione completa delle vie aeree distali , ma solo restringimento del lume , che resta comunque pervio e quindi senza air trapping nelle scansioni in espirio , almeno nella prima fase della malattia . il nostro lavoro ha delle limitazioni . 
la prima dovuta al fatto che gli esami sono stati valutati ciascuno da un singolo radiologo , a conoscenza della diagnosi finale , senza alcun confronto diagnostico ( e quindi statistico ) con gli altri autori . 
la casistica relativamente ampia in quanto non sono stati ammessi altri 14 pazienti con segni hrct tipici , ma senza evidenza microbiologica di infezione da ntm , che poteva essere confermata se si fossero ottenuti ripetuti esami dellescreato o se fossero stati sottoposti ad esame broncoscopico . 
infine non stata valutata la diversit del quadro hrct in base al diverso tipo di ntm riscontrato , che alcuni lavori [ 10 , 14 , 26 ] hanno messo a confronto , senza comunque riscontrare differenze significative . 
 in conclusione , si pu affermare che lincidenza dellinfezione polmonare da ntm in aumento nei pazienti non hiv + , ma la diagnosi di questa patologia resta ancora difficile , soprattutto perch la sintomatologia insidiosa e , spesso , subdola in quanto molti di questi pazienti hanno una lunga storia di malattie polmonari croniche , compresa una pregressa infezione tubercolare . lhrct una metodica fondamentale nel riconoscimento e nella diagnosi di infezione polmonare e , soprattutto , nel suggerire la possibile infezione da ntm in base ai 2 diversi pattern di presentazione . 
nella forma nodulare , la presenza di bronchiettasie , di noduli escavati con il feedings bronchus sign e i noduli centrolobulari con aspetto ad albero con gemme , distribuiti prevalentemente nel lobo medio e nella lingula , devono indurre il radiologo ad ipotizzare la diagnosi di infezione da nmt [ 5 , 14 ] , suggerendo al clinico la ricerca del germe responsabile [ 26 , 27 ]  . 
la diagnosi di trombosi venosa cerebrale ( tvc ) , patologia relativamente rara che predilige i giovani , causa dell1%2% degli stroke delladulto e che ha esordio clinico subdolo , spesso difficile . 
la conoscenza dei segni tc , rm e angio - rm di tvc essenziale per la diagnosi precoce della malattia e consente di formulare la diagnosi nella grande maggioranza dei casi , permettendo di intraprendere con tempestivit il trattamento con farmaci anticoagulanti . 
il ricorso alla dsa va riservato solo ai casi dubbi . keywords venous cerebral thrombosis dural sinuses magnetic resonance imaging magnetic resonance angiography parole chiave trombosi venosa cerebrale seni durali risonanza magnetica angio - rm 314 introduction the first description of cerebral venous thrombosis ( cvt ) dates back to 1825 , when ribes described a 45 - year - old man who died after a 6 - month history of headache , epilepsy and delirium and was found to have thromboses of the superior and transverse sagittal sinuses and of a cortical vein on postmortem examination [ 1 , 2 ]  . 
cvt can also manifest in otherwise healthy subjects , the most frequently implicated risk factors in such subjects being inherited or acquired thrombophilia , oral contraceptive use , pregnancy and puerperium [ 1 , 4 , 7 , 8 ]  . this explains the slight predilection for women . 
presenting symptoms include intense and persistent headache , often the only sign of disease [ 9 ] , and seizures , followed by focal neurological deficits and altered consciousness including coma [ 1 , 5 , 10 ]  . 
the diagnosis relies on computed tomography ( ct ) , magnetic resonance imaging ( mri ) and digital subtraction angiography ( dsa ) [ 1 , 5 , 10 ]  . this paper retrospectively reviews a series of 40 patients with cvt examined in the emergency department over a period of 10 years , with the aim of evaluating the role of ct and mri in emergency clinical practice . 
we discuss clinical presentation , risk factors , ct and mri findings , progression and follow - up of the disease . materials and methods patients we reviewed the clinical records ( electronic clinical record , outpatient summaries ) of 40 patients with cvt who presented to the emergency department between june 1996 and may 2006 . 
all patients had undergone conventional mri within 24 h of ct , and all but one ( case 34 ) had undergone mr venogradiol med ( 2010 ) 115 : 313325 introduzione descritta per la prima volta nel 1825 da ribes , in un uomo di 45 anni , deceduto dopo 6 mesi dallinsorgenza di un quadro clinico di cefalea , epilessia e delirio , con dimostrazione autoptica di trombosi dei seni sagittale superiore e trasversi e delle vene corticali [ 1 , 2 ] , la trombosi venosa cerebrale ( tvc ) un evento poco frequente che in circa il 50% dei casi determina un infarto venoso cerebrale [ 3 ]  . lesordio spesso subdolo , i segni clinici variabili e polimorfi ; la malattia pu anche essere paucisintomatica e in tali casi restare misconosciuta [ 4 ]  . 
non nota la reale incidenza della patologia [ 1 , 2 ] , la cui frequenza viene stimata in 27 casi / 1000000 per anno [ 5 ] ; la tvc viene riportata come causa di infarto nell1%2% dei giovani adulti [ 6 ]  . leziopatogenesi della tvc polimorfa : le cause possono essere distinte in locali e sistemiche , settiche e asettiche [ 1 ]  . le patologie locali che pi frequentemente si complicano con tvc sono le infezioni cerebrali e del massiccio facciale , i tumori cerebrali e i traumi cranici [ 1 ]  . 
la tvc pi frequentemente insorge in soggetti in pieno benessere ; in questi casi i fattori predisponenti maggiormente implicati sono le trombofilie congenite o acquisite , lassunzione di farmaci estroprogestinici ( ep ) , la gravidanza e il puerperio [ 1 , 4 , 7 , 8 ] ; questo spiega la lieve predominanza di incidenza nel sesso femminile . 
lesordio clinico rappresentato nella maggior parte dei casi dalla cefalea , spesso unico segno [ 9 ] , intensa e persistente , e dalle crisi comiziali , seguono i deficit neurologici focali e i disturbi della coscienza , sino al coma [ 1 , 5 , 10 ]  . 
la prognosi spesso favorevole a patto che si instauri precocemente il trattamento anticoagulante ; la diagnosi si avvale dellimaging tramite tomografia computerizzata ( tc ) , risonanza magnetica ( rm ) e dellangiografia digitale [ 1 , 5 , 10 ]  . in questo lavoro viene proposta lanalisi retrospettiva della nostra casistica , che consta di 40 pazienti con tvc giunti alla nostra osservazione , in pronto soccorso , in un periodo di 10 anni , allo scopo di valutare il ruolo della tc e della rm nella pratica clinica , in emergenza . 
vengono considerati la presentazione clinica , i fattori di rischio , i reperti tc ed rm , levoluzione ed il follow - up . materiali e metodi pazienti stata riesaminata la documentazione clinica ( cartella clinica computerizzata , schede ambulatoriali ) di 40 pazienti con tvc , giunti alla nostra osservazione , in pronto soccorso ( ps ) , nel periodo compreso tra giugno 1996 e maggio 2006 , prendendo in considerazione lesordio clinico , i fattori di rischio , la terapia , lesito e il follow - up . radiol med ( 2010 ) 115 : 313325 raphy . 
the diagnosis of cvt was based on the detection of two of the following criteria : ( 1 ) clinical history and presentation suggestive of or consistent with cvt ; ( 2 ) depiction of findings suggestive of intraluminal thrombus in the veins and / or venous sinuses on conventional mri ; ( 3 ) presence of a complete or partial venous occlusion on mr venography or dsa . all ct examinations were performed with unenhanced acquisitions between 1 and 6 h after admission to the emergency department . 
examinations between 1996 and 2002 were performed using a nonspiral ct scanner , with axial 5 - mm scans on the posterior fossa and 7 - mm scans up to the vertex . 
in a few cases , additional oblique scans and / or scans with the tutti i pazienti erano stati sottoposti a tc basale dellencefalo , completata in 8 casi con acquisizioni effettuate dopo somministrazione di mezzo di contrasto ( mdc )  . 
tutti i pazienti avevano eseguito una rm convenzionale entro le 24 ore dalla tc ed in tutti i casi , ad eccezione di uno ( caso 34 ) era stata effettuata unacquisizione con angiografia rm ( mra ) venosa . 
gli esami eseguiti dal 1996 al 2002 sono stati ottenuti con una tc non elicoidale , con scansioni assiali di 5 mm sulla fossa posteriore e di 7 mm sino al vertice . 
all data were entered into a database from which tables 14 were derived . data analysis results our series included 40 patients ( 26 women and 14 men , age range 1876 years , median age 43 )  . 
saltuariamente lesame stato completato con acquisizioni t2 * gradient echo ( gre ) e / o con somministrazione del mdc paramagnetico . lmra venosa stata ottenuta con impiego di tecnica 2dtempo di volo ( tof ) ( tr / te 24 / 5 , 1 mm / s , flip angle [ fa ] 60 , spessore 1 , 4 mm , fov 22 cm , matrice 256128 , tempo di esecuzione 56 m ) con successive ricostruzioni maximum intensity projection ( mip ) ; le slices sono state orientate sul piano coronale e sono state estese a comprendere tutto lencefalo . 
in casi isolati , per un migliore precisazione diagnostica , sono state eseguite acquisizioni supplementari con scansioni oblique e / o con impiego della tecnica phase contrast 2d ( tr 27 mm / s , fa 20 , venc 10 spessore 20 mm )  . analisi dei dati le immagini delle tc e delle rm sono state riesaminate da due differenti radiologi ( rl , gcs )  . 
patients ( % ) table 1 clinical manifestations and risk factors headache seizures altered consciousness focal neurological signs papillo - oedema nausea and vomiting visual disturbances 24 ( 60 ) 15 ( 37.5 ) 9 ( 22.5 ) 8 ( 20 ) 5 ( 12.5 ) 4 ( 10 ) 2 ( 5 ) tabella 1 quadro clinico / fattori di rischio 24 ( 60 ) cefalea crisi comiziali 15 ( 37 , 5 ) alterazione stato di coscienza 9 ( 22 , 5 ) segni neurologici focali papilledema nausea e vomito disturbi visivi 8 ( 20 ) 5 ( 12 , 5 ) 4 ( 10 ) 2 ( 5 ) inherited thrombophilia oral contraceptive use puerperium systemic malignancies local causes other 16 ( 40 ) 11 ( 27.5 ) 2 ( 5 ) 5 ( 12.5 ) 7 ( 17.5 ) 4 ( 10 ) trombofilia congenita assunzione estroprogestinici puerperio tumori sistemici cause locali altro 16 ( 40 ) 11 ( 27 , 5 ) 2 ( 5 ) 5 ( 12 , 5 ) 7 ( 17 , 5 ) 4 ( 10 ) sintomo desordio numero pazienti ( % ) fattori di rischio numero pazienti ( % ) radiol med ( 2010 ) 115 : 313325 fig . 
1a - c right transverse ( a ) and straight ( b ) sinus thrombosis : homogeneous hyperdensity on unenhanced computed tomography ( ct ) ( cord sign )  . 
c altro caso , trombosi del seno longitudinale superiore , segno del delta alla tc eseguita dopo somministrazione del mdc iodato . table 2 computed tomography ( ct ) findings tabella 2 reperti alla tomografia computerizzata ( tc ) no . 
patients ( % ) numero pazienti ( % ) ischaemia parenchymal haemorrhage subarachnoid haemorrhage ( sah ) cord sign and / or dense triangle sign empty delta sign cortical swelling no abnormal finding no focal parenchymal lesions 11 ( 25.5 ) 10 ( 25 ) 5 ( 12.5 ) 7 ( 17.5 ) 4 ( 10 ) 4 ( 10 ) 5 ( 12.5 ) 19 ( 47.5 ) ischemia emorragia parenchimale emorragia subaracnoidea ( esa ) segno della corda e / o triangolo denso segno delta rigonfiamento corticale nessun reperto patologico assenza di lesioni parenchimali focali 11 ( 25 , 5 ) 10 ( 25 ) 5 ( 12 , 5 ) 7 ( 17 , 5 ) 4 ( 10 ) 4 ( 10 ) 5 ( 12 , 5 ) 19 ( 47 , 5 ) sinus thromboses , as well as depicting one case of sss occlusion not detectable on conventional mri . 
in two cases without direct signs of thrombosis , it demonstrated small transverse sinuses in one case and aroused suspicion of dural fistula in the other by failing to depict the left transverse sinus . 
the most frequently involved sinuses were the sss ( 25 / 40 cases , six with isolated involvement ) and the transverse sinuses ( ts ) , with a prevalence of the left transverse sinus ( 14 / 40 )  . five of 40 patients died within 1 month of the diagnosis of cvt . 
of the remaining patients , five suffered residual disability ( mild to severe ) , whereas 30 made a full recovery . of the 35 subjects who survived , 24 ( 68.5% ) underwent at least one mri follow - up examination 26 months after presentation , which demonstrated partial or total recanalisation of the involved vessels in 79% of cases ( 19 / 24 )  . 
sono stati inoltre rilevati 5 casi di esa , 2 malformazioni artero - venose ( mav ) e 1 meningite ( tabella 3 )  . langio - rm ha confermato tutte le trombosi dei seni venosi 318 table 3 magnetic resonance imaging ( mri ) findings no . 
i seni pi frequentemente coinvolti sono stati il sss in 25 / 40 casi , con coinvolgimento isolato in 6 , e i trasversi ( st ) con prevalenza del sinistro ( 14 / 40 )  . cinque / 40 pazienti sono deceduti entro un mese dalla diagnosi di tvc , dei rimanenti , 5 sono sono andati incontro a esiti ( da lievi a gravi ) , mentre in 30 soggetti non vi sono stati reliquati  . 
dei 35 soggetti non deceduti in 24 ( 68 , 5% ) stato effettuato almeno un controllo con rm da 2 a 6 mesi dallesordio che ha dimostrato ricanalizzazione , parziale o totale , dei vasi interessati nel 79% dei casi ( 19 / 24 )  . 
nel caso della trombosi delle vene e dei seni venosi cerebrali la lenta progressione del trombo e linstaurarsi di circoli collaterali di deflusso spiega la lenta e progressiva insorgenza dei sintomi [ 4 ]  . 
la persistenza della trombosi causa un aumento della pressione venulare e capillare ed una riduzione della pressione arteriosa per cui si determina la morte cellulare ( edema citotossico ) ; laumentata pressione venulare e capillare pu determinare un infarcimento ematico e talora un sanguinamento subaracnoideo e / o subdurale [ 1 , 5 , 11 , 14 ]  . 
nella nostra casistica erano evidenziabili lesioni focali parenchimali in 24 / 40 soggetti ( 60% ) con una modesta prevalenza delle forme ischemiche ( 35% ) su quelle emorragiche ( 25% ) ; si sono verificati anche 5 casi di esa radiol med ( 2010 ) 115 : 313325 fig . 
d scansione assiale t2 , in fase acuta il trombo appare ipointenso con cercine periferico iperintenso . appropriate treatment to prevent , where possible , brain damage or worsening of the clinical picture and help the resolution of lesions [ 1 , 5 , 11 , 12 ]  . 
in contrast to arterial stroke , which is readily diagnosed clinically in most cases , cvt presents with subtle and diverse clinical signs , making the use of neuroimaging essential for the diagnosis [ 11 , 13 ]  . pathophysiologically , venous thrombosis is a dynamic process in which the balance of prothrombotic and thrombolytic processes is disrupted , leading to progression of the thrombus over time . 
in the case of thrombosis of the cerebral veins and venous sinuses , this slow growth of the thrombus and the development of collateral blood drainage explain the ( 12 , 5% ) , due dei quali in assenza di lesioni focali parenchimali . 
 clinicamente lesordio della tvc pu essere subacuto ( da 2 giorni a 1 mese ) in circa il 50% dei casi , acuto ( meno di 2 giorni ) nel 30% dei casi e cronico ( pi di 1 mese ) nel 20% [ 13 ]  . 
la cefalea rappresenta il sintomo desordio pi frequente ( 75%95% ) ed in genere rapidamente progressiva , severa , persistente , unilaterale [ 1 , 46 , 9 , 11 ]  . 
altri sintomi desordio sono rappresentati da segni neurologici focali ( afasia , emiplegia , amnesia , emianopsia , ecc . ) che radiol med ( 2010 ) 115 : 313325 fig . 
persistence of the thrombus causes increased venular and capillary pressure and reduced arterial pressure , leading to cell death ( cytotoxic oedema )  . the increased venular and capillary pressure may lead to subarachnoid and / or subdural haematoma or effusion or at times haemorrhage [ 1 , 5 , 11 , 14 ]  . 
in our series , focal parenchymal lesions were depicted in 24 / 40 subjects ( 60% ) , with a slight prevalence of ischaemic ( 35% ) over haemorrhagic ( 25% ) forms . there were also five cases of sah ( 12.5% ) , two of them without focal parenchymal lesions . the clinical manifestation of cvt is subacute ( from 2 days to 1 month ) in approximately 50% of cases , acute ( < 2 days ) in 30% of cases and chronic ( > 1 month ) in 20% [ 13 ]  . headache is the most common presenting symptom ( 75%95% ) and is generally rapidly progressive , severe , persistent and unilateral [ 1 , 46 , 9 , 11 ]  . 
other presenting symptoms include focal neurological signs ( aphasia , hemiplegia , amnesia , hemianopia , etc . ) in 27%80% of cases [ 11 , 13 , 15 , 16 ] and seizures in 1540% [ 1 ]  . 
in our series , focal neurological signs were present in 20% of patients , seizures in 37.5% and altered consciouscompaiono nelle varie casistiche dal 27% all80% [ 11 , 13 , 15 , 16 ] e dalle crisi comiziali nel 15%40% [ 1 ]  . 
in questa casistica sono stati riscontrati segni neurologici focali nel 20% dei soggetti , mentre nel 37 , 5% dei casi allesordio erano presenti crisi epilettiche e nel 22 , 5% alterazioni dello stato di coscienza . 
lassociazione della cefalea , intensa , gravativa e persistente con deficit focali e / o crisi epilettiche rappresenta un elemento clinico di forte sospetto di tvc [ 13 ]  . molteplici sono le condizioni che predispongono allinsorgenza della tvc ; in letteratura vengono descritte pi di 100 cause [ 4 , 5 ]  . 
i primi sono per lo pi rappresentati da infezioni , tumori e traumi ; le infezioni sono chiamate in causa raramente nelladulto , mentre sono responsabili di tvc in un discreto numero di pazienti di et pediatrica [ 7 , 17 ]  . 
le cause sistemiche includono deficit dei fattori della coagulazione ( proteina c , proteina s ) , lassunzione di farmaci ep , il puerperio , stati di ipercoagulabilit secondari a tumori maligni [ 5 ]  . 
i fattori predisponenti , se accuratamente ricercati , vengono identificati in una elevata percentuale di pazienti ( 75% , 80% , 88% ) [ 5 , 6 , 17 , 18 ] ; nella nostra casistica solo in un caso non stato trovato alcun fattore predisponente . radiol med ( 2010 ) 115 : 313325 fig . 
flair ( a ) and diffusion ( b ) images show hyperintense signal of the thalamus bilaterally ; the signal is hypointense on the t1 - weighted image ( c )  . 
the association of severe , persistent and worsening headache with focal deficits and / or seizures is a clinical sign that is strongly suggestive of cvt [ 13 ]  . many conditions can predispose to the development of cvt , and more than 100 causes have been described in the literature [ 4 , 5 ]  . 
systemic causes include deficiency of coagulation factors ( protein c , protein s ) , oral contraceptive use , puerperium and hypercoagulable states secondary to malignancy [ 5 ]  . 
in our series , we were unable to identify any risk factor in one case only . one of the main risk factors in women is the use of oral contraceptives . 
this explains the predominance of this condition among women [ 1 , 15 ]  . in our series , the female - to - male ratio was almost 2 : 1 ( 26 / 14 ) , and among the 26 women , 11 ( 42% ) used oral contraceptives . 
 ct and mri are capable of demonstrating both the direct signs ( evidence of a thrombus inside the affected veins ) and indirect signs ( parenchymal changes ) of thrombosis , whereas ct and mr venography provide a vascular map and enable identification of occluded venous sinuses [ 5 ]  . ct , the first - line examination in the emergency setting , is negative in 10%30% of cases , depending on the series [ 4 , 15 , 21 ]  . 
on unenhanced ct , the typical direct sign is thrombus hyperdensity , especially during the first 2 weeks , which appears as a cordlike hyperdensity ( cord sign ) or , if inside the sss , as a dense triangle ( dense triangle sign )  . after the first 2 weeks , the thrombus is only visible after contrast administration and appears as a sinus - filling defect surrounded by a hyperdense rim due to enhancement of the vasa vasorum and dura ( empty delta sign ) [ 1 , 13 , 22 ]  . 
in sss thrombosis , the lesions may be bilateral , whereas in lesions of the deep venous system , bilateral thalamus involvement is common [ 6 , 11 , 13 , 22 ]  . is heterogeneous , located at frequently mri combined with mr venography is the modality of nelle donne uno dei principali fattori di rischio rappresentato dallassunzione di farmaci ep ; da uno studio effettuato da de bruijn et al . 
 [ 19 ] risulta che le donne che assumono ep hanno un rischio di 13 volte superiore di sviluppare una tvc ; lincidenza aumenta se coesiste una trombofilia ereditaria [ 4 , 12 , 19 , 20 ]  . 
nella nostra serie il rapporto femmina / maschio stato di quasi 2 : 1 ( 26 / 14 ) ; tra le 26 femmine 11 ( 42% ) assumevano ep . 
 tc e rm sono in grado di dimostrare sia i segni diretti ( evidenza del trombo allinterno delle strutture venose coinvolte ) sia quelli indiretti ( alterazioni parenchimali ) della trombosi ; mentre angio - tc e angio - rm permettono la dimostrazione della mappa vascolare e lidentificazione dei seni venosi occlusi [ 5 ]  . 
la tc , primo esame di norma eseguito in emergenza , pu risultare negativa in una percentuale di casi che varia dal 10% al 30% a seconda delle casistiche [ 4 , 15 , 21 ]  . 
nella tc basale il segno diretto della trombosi rappresentato dalla iperdensit del trombo visibile , soprattutto nelle prime due settimane , come lineare area di iperdensit ( segno della corda ) o , se allinterno del sss , come immagine triangolare densa ( segno del triangolo denso )  . 
dopo le prime settimane il trombo pu essere riconosciuto solo dopo somministrazione del mdc come un difetto di riempimento del seno , circondato da un orletto di iperdensit dovuto allenhancement dei vasa vasorum e della dura ( segno delta ) [ 1 , 13 , 22 ]  . 
la percentuale di dimostrazione diretta del trombo varia a seconda delle casistiche dal 20% al 55% . i segni indiretti sono invece aspecifici e sono rappresentati da infarti cerebrali che non rispettano un territorio vascolare arterioso . 
lemorragia parenchimale cerebrale , riportata con una frequenza del 30%50% , disomogenea , ha margini irregolari ed situata pi frequentemente in sede parietale e parieto - occipitale al passaggio corticosottocorticale . 
nelle trombosi del sss le lesioni possono essere bilaterali , mentre nelle trombosi del sistema venoso profondo frequente il coinvolgimento bilaterale del talamo [ 6 , 11 , 13 , 22 ]  . la rm in associazione allangio - rm venosa attualmente la modalit di scelta per la diagnosi e il follow - up della tvc [ 1 , 6 , 22 , 23 ]  . 
il segnale , che dipende dallo stato di ossigenazione dei globuli rossi intrappolati nel trombo e dalle fasi di degradazione dellemoglobina , isointenso in t1 e dp nei primi 35 giorni e diventa iperintenso in tutte le sequenze dopo la prima settimana , permanendo iperintenso per circa 1 mese . nella fase cronica della trombosi i segni diretti non sono pi visualizzabili [ 6 , 13 , 22 , 23 ]  . 
nella nostra serie il segno diretto della trombosi stato rilevato in 37 / 40 pazienti ( 92 , 5% ) con le sequenze t1 e dp pesate , mentre nelle radiol med ( 2010 ) 115 : 313325 choice for cvt diagnosis and follow - up [ 1 , 6 , 22 , 23 ]  . direct visualisation of the thrombus is achieved in a large proportion of cases . 
the signal , which depends on the level of oxygenation of the red blood cells trapped in the thrombus and the phases of haemoglobin degradation , is isointense in t1 and pd during the first 35 days . 
in our series , direct signs were seen in 37 / 40 patients ( 92.5% ) in t1 and pd sequences but in only 31 / 40 on t2 and flair images . 
compared with ct , mri appears to have greater sensitivity for detecting nonhaemorrhagic parenchymal lesions . the role of diffusion - weighted ( dwi ) and susceptibilityweighted ( swi ) echoplanar ( epi ) sequences in the diagnosis of cvt is still controversial [ 24 , 25 ]  . 
some authors have attempted to correlate the signal from the thrombus with sinus recanalisation , finding that if the thrombus is hyperintense on dwi , recanalisation appears to be less frequent [ 14 ]  . 
in subjects with parenchymal lesions , dwi sequences enable the differentiation of vasogenic oedema and cytotoxic oedema with the possibility of predicting the degree of reversibility of the lesions [ 12 , 14 ]  . 
 the angiographic techniques most commonly employed to confirm the diagnosis of cvt and assess the extent of thrombosis are mr and ct venography , whereas dsa is only reserved for equivocal cases , partial thromboses and suspected vascular malformations [ 1 , 5 , 6 , 13 , 17 ]  . 
at our institution , we normally use mr venography with 2d - tof , which is the most widely used technique in diagnosing venous thrombosis owing to it high sensitivity for slow flows and relative insensitivity to signal - loss artefacts caused by spin saturation compared with the 3d - tof technique [ 3 , 5 , 11 ]  . 
as the technique is most sensitive to flow that is perpendicular to the acquisition plane , whenever there is any doubt of a pseudo - occlusion caused by saturation effects , another acquisition in an orthogonal plane should be obtained [ 5 ]  . 
the phase - contrast ( pc ) technique is less often used owing to the difficulty in setting the correct velocity - encoding parameters [ 5 , 6 ]  . 
rispetto alla tc lesame rm appare pi sensibile nel riconoscere le lesioni parenchimali non emorragiche . il ruolo delle sequenze echo planari ( epi ) , diffusion weighted ( dwi ) e susceptibility - weighted ( swi ) nella diagnosi della tvc ancora controverso [ 24 , 25 ]  . 
alcuni autori hanno cercato di correlare il segnale del trombo con la ricanalizzazione del seno ; dal loro lavoro emerge che se il trombo iperintenso in dwi la ricanalizzazione sembra essere meno frequente [ 14 ]  . 
le sequenze dwi in ogni caso offrono la possibilit di discriminare , nei soggetti con lesioni parenchimali , ledema vasogenico dalledema citotossico con possibilit di predire il grado di reversibilit delle lesioni [ 12 , 14 ] , mentre limpiego delle sequenze gre potrebbe facilitare il riconoscimento della trombosi delle vene corticali in fase acuta evidenziandole come lineari strie di ipointensit di segnale [ 26 ]  . 
 per confermare la diagnosi di tvc e fare un bilancio dellestensione della trombosi le tecniche angiografiche attualmente pi utilizzate sono langio - rm e langio - tc , mentre la dsa viene ormai riservata ai casi dubbi , nei casi di trombosi parziali e nel sospetto di malformazioni vascolari [ 1 , 5 , 6 , 13 , 17 ]  . 
nel nostro istituto viene abitualmente eseguita langio - rm venosa con tecnica 2d - tof , che peraltro rappresenta la tecnica pi comunemente usata per la diagnosi di trombosi venosa in quanto mostra unelevata sensibilit per i flussi lenti ed meno frequentemente inficiata da artefatti da perdita di segnale da saturazione degli spin al confronto con la tecnica 3d - tof [ 3 , 5 , 11 ]  . 
dal momento che la tecnica molto sensibile al flusso quando questo perpendicolare al piano di acquisizione , qualora esista il dubbio di una pseudo occlusione legata ad effetti di saturazione conveniente ripetere unaltra acquisizione su un piano ortogonale [ 5 ]  . 
meno utilizzata routinariamente la tecnica phase contrast ( pc ) per la difficolt di impostare i corretti valori di venc ( velocity encoding ) [ 5 , 6 ]  . recentemente alcuni studi hanno proposto limpiego della tecnica angio - rm con mdc per la valutazione dei seni venosi ; la tecnica consente , in un tempo molto breve , di ottenere la mappa vascolare venosa di tutto lencefalo , permettendo una migliore valutazione delle trombosi parziali [ 27 ] , ma il reale valore di questa tecnica ancora controverso [ 26 ]  . 
secondo alcuni autori potrebbe avere un ruolo nella diagnosi della tvc in fase cronica [ 5 ]  . langio - tc , soprattutto con lintroduzione delle tc multidetettore , ha dimostrato una sensibilit analoga a quella dellangio - rm nel riconoscimento della tvc e viene comunemente impiegata in alcuni centri [ 6 , 28 ] e , secondo alcuni autori , dopo lintroduzione di software di ricostruzione che permettono lesclusione dellosso , langio - tc 324 radiol med ( 2010 ) 115 : 313325 ct venography , especially with the advent of multidetector ct , has similar sensitivity to mr venography in detecting cvt and is commonly used in several centres [ 6 , 28 ]  . 
according to some authors , the introduction of reconstruction software allowing removal of bone from the images has enabled ct venography to provide mip images that are superior to those of mr venography [ 29 ]  . 
in our opinion , however , the use of conventional mri combined with mr venography permits direct visualisation of the thrombus , provides a map of the venous vasculature , gives indications as to the time of onset and more accurately depicts any associated parenchymal lesions . dsa , originally the gold standard for cvt diagnosis , has now come to play a more marginal role and is used in equivocal cases only to assess possible associated vascular disorders and provide an indication for endovascular treatment [ 5 , 6 , 11 , 13 , 17 ]  . 
besides the direct sign of nonopacification of the affected veins and sinuses , angiography provides a series of indirect signs that are sometimes crucial for the diagnosis ( dilatation of collateral veins , venous filling defects , collateral circulation )  . 
however , no significant difference in neurological recovery was noted between subjects with recanalisation and those with persisting thrombosis . conclusions cvt is an uncommon pathological condition with an often favourable outcome that is strongly dependent on the correct treatment strategy . 
it is therefore important to be familiar with the direct and indirect ct and mri signs and recognise the clinical manifestations that most frequently accompany cvt in order to implement the correct diagnostic workup in the emergency department . 
when possible , mri combined with mr venography should be the preferred modality because it does not expose the patient to ionising radiation or iodinated contrast material , has greater sensitivity in detecting cerebral lesions and allows identification of acute ischaemic lesions , direct recognition of the thrombus and performance of an angiographic study . 
however , where mri is unavailable in the emergency setting , ct combined with ct venogvenosa fornisce delle immagini mip di qualit superiore a quelle dellangio - rm [ 29 ]  . 
tuttavia , a nostro parere , lesecuzione dellesame rm completato da angio - rm permette la dimostrazione diretta del trombo e la visualizzazione della mappa vascolare venosa , fornisce indicazioni sul tempo di insorgenza e permette di evidenziare , con una maggiore accuratezza , tutte le eventuali lesioni parenchimali associate . langiografia digitale , che allinizio rappresentava il gold standard per la diagnosi di tvc , ha ora un ruolo pi marginale e viene utilizzata nei casi dubbi , per valutare eventuali patologie vascolari associate , dando eventualmente lindicazione al trattamento endovascolare [ 5 , 6 , 11 , 13 , 17 ]  . 
langiografia fornisce , accanto al segno diretto rappresentato dalla mancata opacizzazione delle vene e dei seni interessati , segni indiretti che a volte sono cruciali per la diagnosi ( dilatazione delle vene collaterali , ritardo di riempimento delle vene , circoli collaterali ) ; allinterno delle vene corticali trombizzate vi una persistenza di opacizzazione nella fase venosa tardiva [ 11 , 17 ]  . 
in questa casistica la ricanalizzazione dei vasi trombizzati , che avviene nei primi mesi dallevento trombotico , stata documentata in 19 / 24 soggetti ; non stata tuttavia evidenziata una significativa variazione nel recupero neurologico tra soggetti con ricanalizzazione rispetto a quelli con persistenza di trombosi . conclusioni la tvc una condizione morbosa non comune in cui la prognosi , spesso favorevole , fortemente condizionata dalla corretta impostazione terapeutica . 
 quindi importante conoscere i segni tc e rm , diretti ed indiretti , e soprattutto fondamentale saper riconoscere i quadri clinici che pi spesso si accompagnano a tvc ed impostare il corretto iter diagnostico gi in pronto soccorso . 
la risonanza magnetica completata da angio - rm venosa la metodica da preferire , quando possibile , perch permette di evitare lirradiazione dei pazienti e la somministrazione del mdc iodato , ha una maggiore sensibilit nel riconoscimento delle lesioni cerebrali , consente di identificare le lesioni ischemiche in fase acuta , di riconoscere limmagine diretta del trombo e di eseguire uno studio angiografico . 
sutera , via francesco maria alias 6 , 90145 palermo , italy , tel . : + 39 - 091 - 9295946 , fax : + 39 - 091 - 6552337 , e - mail : raffaello.sutera@alice.it received : 11 may 2009 / accepted : 17 september 2009 / published online : 3 march 2010 springer - verlag 2010 abstract purpose . 
between january and march 2009 , 20 patients with clinical evidence of plantar fasciitis ( group a ) and a similar number of healthy volunteers ( group b ) underwent mr imaging of the ankle / hind foot in the upright weight - bearing and conventional supine position . 
in group a , mr imaging confirmed the diagnosis in 15 / 20 cases ; in 4 / 15 cases , a partial tear of the plantar fascia was identified in the upright weight - bearing position alone . 
nel periodo compreso tra gennaio e marzo 2009 , 20 pazienti con diagnosi clinica di fascite plantare ( gruppo a ) ed altrettanti volontari sani ( gruppo b ) , sono stati sottoposti ad esame rm del retropiede / caviglia sia in ortostatismo che in clinostatismo . 
per le indagini stata utilizzata una apparecchiatura rm dedicata da 0 , 25 tesla ( g - scan , esaote spa , genova , italia ) con bobina di ricezione dedicata per retropiede / caviglia . 
nel gruppo a , la rm ha confermato la diagnosi in 15 / 20 casi ; in 4 / 15 casi stata evidenziata una rottura parziale della fascia plantare visualizzata solo nella posizione ortostatica . 
a causa della maggiore tensione della fascia plantare in tutti i casi , gruppo a e b , lo spessore del tratto peri - inserzionale sotto radiol med ( 2010 ) 115 : 246260 conclusions . 
limaging del retropiede / caviglia nella posizione ortostatica con rm dedicata e bobina dedicata potrebbe consentire di dimostrare le rotture parziali della fascia plantare che possono rimanere misconosciute in clinostatismo . 
 parole chiave fascia plantare rm sotto carico introduction introduzione the plantar fascia is the thick , central portion of the plantar aponeurosis that arises from the medial calcaneal tuberosity [ 1 ] and inserts distally into the plantar plates of the metatarsal - phalangeal joints . 
thanks to its combined static and dynamic role in supporting the longitudinal arch of the foot and its weight - bearing capabilities in the upright position , it is often subject to acute partial or complete tear or traction microtrauma due to functional overload ( plantar fasciitis ) [ 2 ]  . 
in the setting of diagnostic imaging , both ultrasonography ( us ) and magnetic resonance ( mr ) imaging have high levels of accuracy in identifying alterations to the plantar fascia [ 511 ]  . 
the intrinsic technical and methodological characteristics of mr imaging ( multiplanar acquisitions , highcontrast resolution , absence of bone artefacts ) generally allow optimisation of the scans in relation to the topography and morphology of the plantar fascia , such that the technique provides invaluable information . 
in addition , technological development of mr imaging in recent years has seen the introduction of systems with increasingly higher magnetic fields ( 1.5 and 3 tesla ) and of dedicated devices able to study joints even with the patient in the upright , weight - bearing position . 
this has opened up new diagnostic possibilities , including the study of the plantar fascia under physiological load , for which no studies are available in the literature . our aim was to evaluate information provided by mr study with a dedicated system on the plantar fascia during weight bearing in patients with a clinical diagnosis of plantar fasciitis and in healthy volunteers . la fascia plantare la porzione centrale , pi spessa , dellaponeurosi plantare , ed origina dalla tuberosit calcaneare mediale [ 1 ] e si inserisce distalmente sulle placche plantari delle articolazioni metatarso - falangee . 
grazie al suo ruolo combinato sia statico che dinamico nel supporto dellarco longitudinale del piede ed alla capacit di permettere il carico sul piede in ortostatismo , sono frequentemente riscontrabili patologie secondarie a microtraumatismi trazionali che derivano dal sovraccarico funzionale ( fascite plantare ) o a rottura acuta parziale o completa [ 2 ]  . 
la fascite plantare la causa pi comune di dolore al retropiede negli atleti dediti alle marce prolungate ed insorge in modo graduale , aumentando durante lattivit sportiva e regredendo con il riposo ; essa consiste in un processo flogistico che coinvolge sia le fibre fasciali che le strutture perifasciali . 
nellambito delle tecniche di diagnostica per immagini , sia lecografia ( us ) che la risonanza magnetica ( rm ) sono accreditate di elevata accuratezza diagnostica nellidentificazione delle alterazioni della fascia plantare [ 511 ]  . 
le caratteristiche tecnico - metodologiche intrinseche della rm ( acquisizione multiplanare , elevata risoluzione di contrasto , assenza di artefatti ossei ) , permettono , in genere , di ottimizzare le scansioni in rapporto alla topografia ed alla morfologia della fascia plantare , rendendo insostituibile lapporto informativo offerto da tale tecnica . 
lo sviluppo tecnologico in rm , inoltre , ha portato negli ultimi anni , da un lato , alla messa in commercio di macchine ad intensit di campo sempre pi elevato ( 1 , 5 e 3 tesla ) e dallaltro , di macchine dedicate con possibilit di studiare le articolazioni anche in ortostatismo , sotto carico gravitazionale , aprendo nuove possibilit diagnostiche , tra cui lo studio della fascia plantare sotto carico fisiologico , di cui non esiste , a tuttoggi , nessun riferimento nella letteratura scientifica . 
 lo scopo del nostro lavoro quello di valutare le informazioni fornite sulla fascia plantare dalla valutazione rm 248 materials and methods between january and march 2009 , two groups of 20 individuals underwent mr imaging with a dedicated system to evaluate the role of acquisitions performed in the upright weight - bearing position . 
in addition , patients ( group a ) had undergone no minimally invasive locoregional procedures , such as shockwave therapy or cortisone injections , but only conservative treatment with oral nonsteroid anti - inflammatory drugs . 
the mean age in group a ( 16 men and four women ) was 36 ( range 2445 ) years , and in group b ( 14 men and 6 women ) it was 33 ( range 2041 ) years . all individuals underwent an mr study with a dedicated 0.25 - t system ( g - scan , esaote spa , genoa , italy ) in the conventional supine or supine position and in the upright weight - bearing position . 
the study in the latter position was done with the gantry rotated to approximately 82 rather than 90 to allow evaluations under almost complete weight - bearing without inducing a sensation of instability . a dedicated platform - shaped receiver coil was used ( fig . 1 ) , and the foot was securely strapped to the platform to minimise differences in position , thus obtaining practically the same scout image in both the upright and supine positions and therefore approximately equivalent planes . 
the study was first performed in the weight - bearing position and then completed with the same sequences in the supine position to minimise patient discomfort and avoid onset of orthostatic hypotension and possible motion artefacts . 
the following sequences were acquired : t1 - weighted spin echo ( se ) ( tr / te 800 / 26 ms ) , t2 - weighted turbo spin echo ( tse ) ( tr / te 2 , 860 / 90 ms ) , short - tau inversion recovery ( stir ) ( tr / te / ti 4 , 140 / 30 / 80 ms ) and t1 - weighted 3d steady - state free precession ( ssfp ) ( tr / te 30 / 15 ms )  . characteristics of the t1 - weighted se sequence were a tr 800 ms , which in musculoskeletal mr imaging guarantees optimal contrast ( with respect to a particularly short tr ) between the tissues involved in the study . 
with the exception of the volumetric t1 - weighted 3d - ssfp sequences ( for which an acquisition matrix of 224224 was used ) , all sequences were characterised in acquisition by a number of samples in the read direction and a number of phase encodings in the phase - encoding directions > 256 . radiol med ( 2010 ) 115 : 246260 sotto carico eseguita con apparecchiatura dedicata nei pazienti con diagnosi clinica di fascite plantare e nei volontari sani . materiali e metodi nel periodo compreso tra gennaio e marzo 2009 , al fine di valutare il ruolo delle acquisizioni sotto carico effettuate con apparecchiatura rm dedicata , sono stati sottoposti a valutazione due gruppi di 20 soggetti , il primo composto da pazienti con diagnosi clinica di fascite plantare ( a ) , laltro da volontari sani ( b )  . 
in entrambi i gruppi nessuno dei soggetti riferiva in anamnesi patologie degenerative , traumatiche , neoplastiche ed infettive del piede , n patologie sistemiche ( spondiliti sieronegative , gotta , artrite reumatoide , artrite psoriasica , sindrome di reiter , ecc . ) ; inoltre , i pazienti ( gruppo a ) non erano stati sottoposti a terapie mini - invasive locoregionali , come le onde durto o le infiltrazioni di cortisonici , ma solo a terapia conservativa con anti - infiammatori non steroidei per os . 
 tutti i soggetti sono stati sottoposti ad esame rm con macchina dedicata da 0 , 25 tesla ( g - scan , esaote spa , genova , italia ) , sia in posizione convenzionale , supina o in clinostatismo , che sotto carico fisiologico , in ortostatismo . 
lo studio in questultima posizione stato eseguito utilizzando il sistema lettino / magnete basculato di circa 82 ; la rotazione non stata di 90 per consentire di eseguire le valutazioni in carico gravitazionale quasi completo non ingenerando la possibile sensazione di instabilit . 
lindagine stata condotta prima sotto carico e poi completata con le stesse sequenze in clinostatismo per ridurre al massimo il disagio dei pazienti , considerando anche la possibile insorgenza di ipotensione ortostatica , e gli eventuali artefatti da movimento . 
sono state acquisite sequenze spin echo ( se ) t1pesata ( tempo di ripetizione [ tr ] / tempo di eco [ te ] 800 / 26 ms ) , turbo - spin echo ( tse ) t2 - pesata ( tr / te 2860 / 90 ms ) , short tau inversion recovery ( stir ) ( tr / te / ti 4140 / 30 / 80 ms ) , e 3d - single - shot fast ( ssf ) t1 - pesata ( tr / te 30 / 15 ms )  . la sequenza se - t1 pesata impiegata nello studio caratterizzata da un tr pari a 800 ms che , nellesame rm dellapparato muscoloscheletrico , garantisce un contrasto ottimale ( rispetto a tr particolarmente brevi ) fra i tessuti coinvolti nellindagine . 
in tutti i casi , sul piano sagittale sono state radiol med ( 2010 ) 115 : 246260 acquisite tutte le sequenze , mentre sul piano coronale sono state acquisite solo le sequenze tse t2 - pesata e stir . 
tutte le sequenze , fatta eccezione quella volumetrica 3d - ssf t1 - pesata ( per la quale stata utilizzata una matrice di acquisizione di 224224 ) , sono caratterizzate , in acquisizione , da un numero di campionamenti nella direzione della lettura ed un numero di codifiche di fase nella direzione della codifica di fase maggiori di 256 ; la ricostruzione dellimmagine avviene quindi su una matrice di 512512 pixel , definita ad alta risoluzione . 
lo spessore di strato e lintervallo di ricostruzione usati erano di 4 mm e 0 , 4 mm in tutte le sequenze , fatta eccezione per la volumetrica 3d - ssf t1 - pesata , in cui stato utilizzato uno spessore di strato di 1 , 4 m tutte le indagini sono state eseguite senza la somministrazione endovenosa di mezzo di contrasto paramagnetico contenente gadolinio . 
 le immagini ottenute sono state inviate via local area network ( lan ) al sistema radiology information system ( ris ) / picture archiving and communication system ( pacs ) ( sistema medris elefante\impax , agfa healthcare system ) del nostro istituto per avere la possibilit di un confronto diretto tra le immagini ottenute in clinostatismo e quelle in ortostatismo su workstation con doppio monitor . 
la valutazione delle immagini stata effettuata in consenso da tre radiologi in cieco sullappartenenza dei soggetti ai differenti gruppi , e quindi sulla loro anamnesi e lobiettivit clinica , ma non sulla distinzione tra la posizione di acquisizione delle sequenze , ortostatismo e clinostatismo . 
si pu associare ledema dei tessuti molli limitrofi superficiali e profondi , caratterizzato da aree scarsamente circoscritte ad alta intensit di segnale , che secondo alcuni autori da solo un valido criterio diagnostico di fascite plantare [ 2 ]  . 
altro reperto che frequentemente si associa ledema dellosso subcondrale della tuberosit calcaneare mediale [ 1 , 2 , 10 , 11 ] , nella maggior parte dei casi ad estensione limitata , che isolatamente non costituisce un criterio diagnostico della patologia . nel nostro studio stata posta la diagnosi di fascite plantare in presenza di edema perifasciale o di entrambi i su esposti criteri . 
slice thickness and reconstruction intervals were 4 mm and 0.4 mm in all sequences except for the volumetric t1 - weighted 3d - ssfp sequence , in which a 1.4 - mm slice thickness was used . 
all examinations were performed without intravenous administration of gadolinium - based paramagnetic contrast material . images were sent via the local area network to the radiology information system / picture archiving and communication system ( ris / pacs ) ( medris elefante impax , agfa healthcare system ) to enable direct comparison of images obtained in the inclined and upright positions on a workstation with a double monitor . 
image evaluation was performed in consensus by three radiologists blinded to the group allocation of each individual and therefore to their history and clinical findings but not to the distinction between upright or inclined acquisition . 
mr characteristics of plantar fasciitis include : ( 1 ) fascia thickening , often with fusiform appearance , typically involving the proximal portion and extending to the calcaneal insertion ; ( 2 ) abnormal signal intensity , which appears intermediate on t1or proton250 radiol med ( 2010 ) 115 : 246260 density ( pd ) - weighted images and high in t2 - weighted or stir images [ 1 , 2 , 10 , 11 ]  . 
oedema of the surrounding superficial and deep soft tissues may be associated , characterised by poorly circumscribed areas of high signal intensity , which according to other authors is in itself a reliable diagnostic criterion for plantar fasciitis [ 2 ]  . 
another commonly associated finding is marrow oedema of the medial calcaneal tuberosity [ 1 , 2 , 10 , 11 ] , with limited extension in most cases , which on its own is not a diagnostic criterion for the disease in our study the diagnosis of plantar fasciitis was made in the presence of perifascial oedema or both of the abovementioned criteria . 
tears are defined by the following criteria : ( 1 ) thickening at the tear site ; ( 2 ) absence ( complete tear ) or partial loss ( partial tear ) of normal signal intensity , which appears as an area of intermediate signal intensity on t1or pd - weighted images and markedly hyperintense on t2 - weighted or stir images ; and ( 3 ) hyperintensity on t2weighted and stir images of the perifascial soft tissues due to oedema / haemorrhage [ 1 , 2 , 11 ]  . 
images obtained in the upright and supine positions were used to evaluate changes in : ( 1 ) morphodimensional features ( thickness , morphology , margins ) ; and ( 2 ) signal intensity of the plantar fascia and the surrounding perifascial structures , including the heel fat pad and the subchondral bone of the ankle . 
accessory findings in the ankle and foot were also evaluated and reported , such as intra - articular effusion or tendon abnormalities . plantar fascia thickness was measured using ris / pacs system callipers in sagittal scans in the proximal , middle and distal segments at around 5 , 20 and 40 mm , respectively , from the calcaneal insertion . 
calcaneal marrow oedema and fascial lesion dimensions were quantified , and the extent of oedema was evaluated with a percentage estimate of its relative involvement with respect to plantar fascia thickness . 
lo spessore della fascia plantare stato misurato , utilizzando i calipers del sistema ris / pacs , nelle scansioni sagittali nei tratti peri - inserzionale , medio e distale , rispettivamente a circa 5 , 20 e 40 mm dallinserzione calcaneare . per la definizione dellispessimento stato scelto uno spessore della fascia plantare > 5 mm in considerazione del riscontro effettuato da tsai et al . 
 [ 6 ] in us , i quali hanno osservato nel piede asintomatico di pazienti con fascite plantare monolaterale uno spessore della fascia plantare di 3 , 830 , 72 m le valutazioni delle alterazioni morfologiche e dellintensit di segnale sono state eseguite in modo soggettivo , comparando i rilievi anomali con quelli normali e tenendo conto dei criteri patologici prima definiti , sono state quantizzate le dimensioni dellalterazione edematosa dellosso subcondrale calcaneare e delle lesioni della fascia plantare ; stata valutata , inoltre , lentit di questa stimando in percentuale il coinvolgimento relativo rispetto allo spessore della fascia plantare . 
 risultati valutazione dellanamnesi e dellobiettivit clinica dei pazienti tutti i soggetti ( 100% ) del gruppo a , riferivano una sintomatologia tipica , insorta da 12 , 314 , 98 settimane ( range 524 settimane ) , caratterizzata da dolore al tallone con i primi passi dopo il riposo o insorgente al mattino ; questo , inoltre , si acuiva durante lattivit motoria in modo esponenziale alla durata della stessa . 
tutti i soggetti ( 100% ) del gruppo b , volontari , non riferivano sintomatologia algica degli arti inferiori e le manovre di dolorabilit non scatenavano alcuna sintomatologia algica . radiol med ( 2010 ) 115 : 246260 symptoms , with onset 12.314.98 weeks ( range 524 weeks ) earlier and characterised by heel pain with the first few steps after rest or after rising in the morning . 
all individuals ( 100% ) in group b reported no pain in the lower limb , and the abovementioned manoeuvres produced no pain . finding of plantar fasciitis mr in both the inclined and upright positions enabled identification of plantar fasciitis , based on the defined criteria , in 15 / 20 cases ( 75% ) in group a . 
in the remaining 5 / 20 cases ( 25% ) , the plantar fascia and perifascial soft tissues had normal appearance , although several associated abnormalities or accessory findings were observed ( see below )  . 
mr imaging in both the inclined and upright positions revealed no abnormality referable to plantar fasciitis or any other type of pathological process in any of the 20 healthy volunteers in group b . measurement of the thickness of the plantar fascia plantar fascia thicknesses are reported in table 1 . 
in individuals with plantar fasciitis in group a , mean thickness in the proximal segment ( the most common site of the condition ) was 8.520.39 mm in the supine position and 8.10.43 mm in the upright position , with a statistically significant ( p < 0.0001 ) reduction in thickness during weight - bearing . fascial thickness in the proximal segment in patients without plantar fasciitis was 4.640.09 mm in the supine position and 4.30.12 mm in the upright position , with a statistically significant ( p < 0.0001 ) reduction in thickness . 
in nessuno dei 20 volontari del gruppo controllo ( b ) , nelle acquisizioni rm in entrambe le posizioni , sono state evidenziate alterazioni riferibili alla fascite plantare o ad altro tipo di patologia . misurazione dello spessore della fascia plantare gli spessori della fascia plantare sono riportati in tabella 1 . nei casi con fascite plantare del gruppo a , lo spessore medio della fascia plantare nel tratto peri - inserzionale , sede elettiva della patologia , era di 8 , 520 , 39 mm in clinostatismo e 8 , 10 , 43 mm in ortostatismo , con evidenza statisticamente significativa ( p < 0 , 0001 ) della riduzione dello spessore sotto carico ; lo spessore in sede peri - inserzionale nei pazienti senza fascite plantare era 4 , 640 , 09 mm in clinostatismo e 4 , 30 , 12 mm in ortostatismo , con riduzione statisticamente significativa ( p < 0 , 0001 ) dello spessore . 
nel gruppo b , in clinostatismo , lo spessore medio della fascia plantare era di 3 , 70 , 24 mm nel tratto peri - inserzionale con significative riduzioni dei valori ( p < 0 , 0001 ) , in ortostatismo . 
nei restanti 11 / 15 pazienti del gruppo a con diagnosi di fascite plantare , nei 5 / 20 pazienti senza diagnosi di fascite plantare e nei volontari sani non sono state rilevate alterazioni riferibili a interruzioni focali della continuit delle fibre fasciali sia in clinostatismo che in ortostatismo . alterazioni associate del calcagno e dei tessuti molli perifasciali , e reperti accessori in tabella 2 sono riportate le incidenze dei reperti nei radiol med ( 2010 ) 115 : 246260 fig . 
2a - d sagittal t2 - weighted turbo spin echo ( a ) and t1 - weighted spin echo ( b ) images in the supine position and corresponding images ( c , d ) in the weight - bearing position of the same individual with plantar fasciitis ( group a )  . 
2a - d scansioni sagittali tse t2 - pesata ( a ) e se t1 - pesata ( b ) in clinostatismo , e rispettive sequenze in ortostatismo ( c , d ) di uno stesso soggetto con fascite plantare ( gruppo a )  . 
 changes associated with the ankle and perifascial soft tissues , and accessory findings table 2 reports the incidence of findings in individuals with and without plantar fasciitis and in healthy volunteers . calcaneal marrow oedema was found in 5 / 15 patients ( 33.33% ) with plantar fasciitis and in 2 / 5 ( 40% ) with no evidence of plantar fasciitis . 
moreover , in the five cases with plantar fasciitis , marrow oedema thickness was 11.4317.12 mm ( range 250 mm ) , with an extension of 10.2811.07 mm ( range 435 mm )  . 
in the other two cases without plantar fasciitis , the thickness was 31.4 mm ( range 24 mm ) with an extension of 3.50.7 mm ( range 34 mm )  . in group a , a heel spur was present in 7 / 15 ( 46.67% ) patients with plantar fasciitis , and in 2 / 7 of these ( 28.57% ) , there was associated marrow oedema . 
all associated pazienti con e senza fascite plantare e nei volontari sani . ledema dellosso subcondrale calcaneare stato evidenziato in 5 / 15 ( 33 , 33% ) casi tra i pazienti con fascite plantare ed in 2 / 5 ( 40% ) casi tra i pazienti senza evidenza di fascite plantare ; inoltre , lo spessore delledema osseo era , nei 5 casi con fascite plantare , di 11 , 4317 , 12 mm ( range 250 mm ) con unestensione 10 , 2811 , 07 mm ( range 435 mm ) , mentre , negli altri 2 casi senza fascite plantare , lo spessore era di 31 , 4 mm ( range 24 mm ) con unestensione di 3 , 50 , 7 mm ( range 34 mm )  . 
nel gruppo dei pazienti ( a ) era presente uno sperone calcaneare in 7 / 15 ( 46 , 67% ) casi tra i pazienti con fascite plantare , in 2 / 7 ( 28 , 57% ) dei quali questo si associava alledema osseo subcondrale . 
4a - d sagittal t2 - weighted turbo spin echo ( a ) and short - tau inversion recovery ( b ) images in the supine position and corresponding images ( c , d ) in the weight - bearing position of the same patient with plantar fasciitis ( group a )  . 
4a - d scansioni sagittali tse t2 - pesata ( a ) e stir ( b ) in clinostatismo e rispettive sequenze in ortostatismo ( c , d ) di uno stesso soggetto con fascite plantare ( gruppo a )  . 
in ortostatismo maggiormente evidente la rottura fasciale sul versante profondo ( frecce ) , probabilmente per la maggiore tensione esercitata sulle fibre fasciali , e ledema osseo calcaneare . radiol med ( 2010 ) 115 : 246260 fig . 
this process may be caused by a number of factors that , in general , can be classified according to three broad categories : mechanical , degenerative and systemic [ 2 , 3 , 11 ]  . an important cause of plantar fasciitis is clearly excessive motion in the foot during gait and the tension forces that the plantar fascia undergoes in some endurance sports ( long - distance walking , running ) or jumping sports ( basketball , dancing , volleyball ) [ 1 , 11 ]  . 
indeed , some authors [ 9 , 12 ] have emphasised the fundamental role of the plantar fascia in absorbing shock during the first phase of gait , whereas in the second phase , it acts as a cord . 
in addition , in these two positions , the plantar system is under tension and therefore contributes to protecting the foot . la fascite plantare la causa pi frequente di dolore del retropiede e consiste in un processo infiammatorio che coinvolte laponeurosi plantare senza o con associato coinvolgimento delle strutture perifasciali . 
tale processo pu risultare da un certo numero di cause , che , in generale , vengono riassunte in tre grandi categorie : meccaniche , degenerative e sistemiche [ 2 , 3 , 11 ]  . un ruolo importante nella determinazione di tale patologia dato chiaramente dallesasperato dinamismo del movimento del passo e dalle forze vettoriali alle quali sottoposta la fascia plantare in alcuni sport di durata ( marcia , fondo ) o che richiedono continui salti ( pallacanestro , danza , pallavolo ) [ 1 , 11 ]  . 
infatti , secondo alcuni autori [ 9 , 12 ] , la fascia plantare ha un ruolo fondamentale nellassorbire lo shock durante la prima parte del passo , laddove nella seconda parte agisce come una corda ; inoltre , in queste due posizioni , il sistema muscolo - aponeurotico plantare sotto tensione , e contribuisce , pertanto , alla protezione del piede . 
 lus una metodica molto valida per lo studio della fascite plantare , grazie alla sua eccellente risoluzione spaziale , tuttavia non ha la stessa sensibilit della rm , una tecnica fortemente operatore dipendente e non permette radiol med ( 2010 ) 115 : 246260 ultrasound is a highly valid technique for studying plantar fasciitis , thanks to its excellent spatial resolution . however , it does not have the same sensitivity as mr imaging , it is highly operator - dependent and is unable to identify associated changes such as calcaneal marrow oedema [ 57 ]  . 
in the diagnostic phase , mr imaging has the undeniable advantage of providing an overall structural and morphological evaluation , with the possibility of evaluating the course , thickness , margins and signal intensity of the plantar fascia , as well as distinguishing between the different types of abnormalities [ 13 , 811 ]  . effusion intra - articular all patients in group a had the typical symptoms , with onset 12.314.98 weeks earlier , therefore tending towards a chronic condition , which is defined as being present for a lengthy period , typically longer than 6 months [ 13 ]  . 
an mr diagnosis of plantar fasciitis was formulated based on the imaging features described above ( focal increase in fascial thickness and abnormal intrafascial and / or perifascial signal ) in only 15 / 20 cases ( 75% )  . 
in the remaining 5 / 20 patients ( 25% ) , associated changes only were identified ( marrow oedema and heel spur ) or accessory findings and achilles ( tibiotarsal tendinopathy )  . 
the difference was statistically significant ( p < 0.0001 ) and is most likely attributable to a functional adaptation , which produces a change in size in the absence of signal intensity changes . 
a significant reduction ( p < 0.0001 ) was observed in fascial thickness between scans acquired in the supine position and those in the weight - bearing position in the proximal and middle portions but not in the distal portion ( p = 0.0078 ) both in groups . 
a possible explanation is the different architectural and arrangement of the fascial fibres , which are more malleable in the proximal and middle portions and theredi riscontrare alterazioni associate come ledema dellosso subcondrale calcaneare [ 57 ]  . 
in fase diagnostica , la rm presenta lindubbio vantaggio di permettere la valutazione morfologica e strutturale globale , con possibilit di valutare il decorso , lo spessore , i margini , e lintensit di segnale della fascia plantare , nonch di distinguere i differenti tipi di alterazioni [ 13 , 811 ]  . tutti i pazienti del gruppo a presentavano una sintomatologia tipica insorta da 12 , 314 , 98 settimane , inquadrabile quindi come una forma tendente alla cronicizzazione , considerato che vengono definite tali quelle insorte da lungo tempo , tipicamente da pi di 6 mesi [ 13 ]  . 
la diagnosi rm di fascite plantare stata formulata , in considerazione dei criteri semeiologici descritti ( aumento focale dello spessore fasciale e unalterazione del segnale intrafasciale e / o perifasciale ) , solo in 15 / 20 casi ( 75% ) ; nei restanti 5 / 20 pazienti ( 25% ) sono state osservate solo alterazioni associate ( edema osseo e spina calcaneare ) o reperti accessori ( versamento endoarticolare tibio - tarsico e tendinopatia achillea )  . 
in tutti i casi con diagnosi rm di fascite plantare ( 100% ) abbiamo osservato un incremento dello spessore della fascia plantare nel tratto peri - inserzionale , sede elettiva della patologia , sia in clinostatismo che in ortostatismo rispettivamente di 8 , 520 , 39 mm e 8 , 10 , 43 mm ; altri autori hanno rilevato unincidenza del reperto al massimo nel 58% dei casi [ 1 , 2 ]  . 
lo spessore della fascia plantare nel tratto peri - inserzionale nei volontari e nei 5 pazienti rimanenti del gruppo a era nei limiti della norma sia in clinostatismo , 3 , 70 , 23 mm e 4 , 640 , 09 mm , che in ortostatismo , 3 , 50 , 2 mm e 4 , 30 , 12 mm , rispettivamente ; abbiamo osservato uno spessore maggiore nei pazienti rispetto ai volontari , ma laspetto non stato approfondito non rientrando tra gli scopi dello studio . 
nei pazienti con fascite plantare stato rilevato anche un ispessimento relativo del tratto medio della fascia plantare rispetto a quelli senza ; la differenza risultata statisticamente significativa ( p < 0 , 0001 ) ed da ascrivere verosimilmente a un adattamento funzionale che esita in unalterazione dimensionale in assenza di alterazioni dellintensit di segnale . 
sia nel gruppo a che nel gruppo b abbiamo rilevato una significativa riduzione ( p < 0 , 0001 ) dello spessore della fascia plantare tra le acquisizioni in clinostatismo e quelle sotto carico solo nei tratti peri - inserzionale e medio ma non nel tratto distale ( p = 0 , 0078 )  . 
una probabile spiegazione potrebbe risiedere nella differente architettura e disposizione delle fibre della fascia plantare , pi malleabili in corrispondenza di tratti peri - inserzionale e medio , che pertanto risentirebbero maggiormente della tensione a cui sono sottoposte sotto carico . 
 in tutti i casi con diagnosi rm di fascite plantare ( 100% ) 258 radiol med ( 2010 ) 115 : 246260 fore probably more heavily affected by the tension they undergo during weight - bearing . in all cases with an mr diagnosis of plantar fasciitis ( 100% ) , there was an absence of homogenous low signal intensity of the fascia and the presence of areas of signal heterogeneity , which was intermediate in the t1 - weighted se sequence and high in the stir and t2 - weighted sequences . 
a fascial tear , whether complete or partial , is an uncommon diagnosis in that not only does it occur infrequently but it is often overlooked [ 13 , 8 , 14 ]  . in most cases , the condition affects runners who subject the plantar fascia to considerable force during acceleration , or it can be the result of a repetitive trauma in amateur athletes engaging in sports involving running and jumping . 
in other cases , however , a spontaneous tear of the plantar fascia is possible in patients with prior plantar fasciitis , especially in those treated with local injections of corticosteroids ( 10% of treated cases according to some studies ) [ 13 , 8 , 14 ]  . 
in 4 / 15 cases ( 26.67% ) with an mr diagnosis of plantar fasciitis , an area of marked t2 hyperintensity was identified in the fascial fibres only in the upright position in the absence of a clear interruption of the fascial margins . the area of the lesion visible in both the sagittal and coronal planes had a width of 1.90.47 mm and a thickness of 2.750.65 mm , with lesion extent relative to plantar fascia thickness of 35.24%6.33%. 
a possible explanation for visualisation of these lesions only in the upright weightbearing position is that the tension of the fascial fibrils subjected to traction during weight bearing extends the microlesions , which are of limited extent and contained within the fascia and thus latent in the supine position . 
in the other patients in group a and in the healthy volunteers , no abnormalities attributable to focal interruptions of the fascial fibres were identified in either the inclined or upright position . 
in patients with an mr diagnosis of plantar fasciitis , perifascial oedema was identified in only 40% of cases and always associated with changes in fascial dimensions and signal intensity , in contrast to previous reports according to which this is one of the most frequent findings ( 70%100% of cases ) and in many cases the sole finding [ 1 , 2 , 8 ]  . 
in cases stata riscontrata , in entrambe le posizioni , lassenza dellomogenea ipointensit di segnale della fascia plantare con presenza di area di disomogeneit , intermedia nella sequenza se t1 - pesata ed alta nelle sequenze stir e t2pesata ; altri autori riportavano unincidenza di tale reperto al massimo nel 52% dei casi [ 1 , 2 ]  . 
la rottura della fascia plantare , sia completa che parziale , una diagnosi poco comune , dal momento che oltre ad essere poco frequente , spesso non viene riconosciuta [ 13 , 8 , 14 ]  . 
nella maggior parte dei casi colpisce atleti agonisti che sottopongono la fascia plantare a notevoli forze durante la fase di accelerazione della corsa , oppure pu essere la risultante di un trauma ripetitivo negli atleti amatoriali che praticano corsa e salto . 
in altri casi , , comunque , possibile una rottura spontanea della fascia plantare nei pazienti con sovrapposta fascite plantare , specialmente in quelli trattati con iniezioni locali di corticosteroidi ( 10% dei casi trattati secondo alcuni studi ) [ 13 , 8 , 14 ]  . 
in 4 / 15 casi ( 26 , 67% ) con diagnosi rm di fascite plantare stata identificata , solo in ortostatismo , nel contesto delle fibre fasciali , unarea di netta iperintensit di segnale in t2 , in assenza di netta interruzione dei margini della fascia . 
 larea di lesione visibile sia sul piano sagittale che su quello coronale aveva unampiezza di 1 , 90 , 47 mm e uno spessore di 2 , 750 , 65 mm con unentit della lesione rispetto allo spessore della fascia plantare del 35 , 24%6 , 33% . 
possibile ipotesi che giustifichi levidenza di queste lesioni solo in ortostatismo potrebbe essere che la tensione delle fibrille fasciali sottoposte a trazione sotto carico amplierebbe le microlesioni , poco estese e contenute nello spessore fasciale , latenti in clinostatismo . 
negli altri pazienti del gruppo a e nei volontari sani non sono state rilevate alterazioni riferibili a interruzioni focali della continuit delle fibre fasciali sia in clinostatismo che in ortostatismo . 
nei pazienti con diagnosi rm di fascite plantare ledema perifasciale stato evidenziato soltanto nel 40% dei casi e sempre associato ad alterazioni dimensionali e dellintensit di segnale della fascia , contrariamente a quanto riscontrato da altri autori , secondo cui questo uno dei reperti pi frequentemente osservati ( tra il 70% ed il 100% dei casi ) ed in molti casi viene riscontrato in modo isolato [ 1 , 2 , 8 ] ; tale reperto non stato osservato nei 5 / 20 casi senza evidenza di fascite plantare n nei soggetti del gruppo b . 
 ledema dellosso subcondrale calcaneare stato evidenziato nei pazienti con fascite plantare nel 33 , 33% dei casi , in accordo con lincidenza riportata in letteratura ( tra il 17% e il 56% dei casi ) [ 1 , 2 ] , con spessore ed estensione di 11 , 4317 , 12 mm e 10 , 2811 , 07 mm ; in uno dei casi stato osservato un edema osseo di notevole estensione ( diametro massimo 4 cm ) , non limitato alla sede peri - inserzionale come comunemente riportato in letteratura [ 1 , 2 , 10 , 11 ]  . 
nei casi senza evidenza di fascite plantare ledema osseo stato radiol med ( 2010 ) 115 : 246260 without evidence of plantar fasciitis , marrow oedema was identified in 40% of cases ( 2 / 5 ) , with limited dimensions ( maximum diameter 4 mm ) , and was probably the consequence of microtraumas due to overloading . the accessory finding of a heel spur was identified in 46.67% of cases with plantar fasciitis , but as other authors have noted , the correlation of this finding is random and is of no relevance [ 1 , 3 , 911 , 13 ]  . 
associated and accessory findings were identified in an equal amount , without significant differences in the scans acquired in both the inclined and upright positions . the increase in thickness and presence of fascial signal abnormalities are a highly sensitive parameter in that they are indicative of a pathological process . 
however , in our experience , they are nonspecific , as they were present both in patients with plantar fasciitis and in those with a partial tear 4 / 15 cases ( 27% ) in our study . the partial tear in patients with plantar fasciitis was only demonstrated in images obtained in the upright position . there are no published studies evaluating the role of mr scans acquired during weight bearing in healthy individuals or patients with plantar fasciitis . 
therefore , there are no reference standards to support the hypothesis that the areas of greater signal hyperintensity identified in plantar fasciitis during weight bearing are latent partial tears rendered visible by tension of the plantar fascia . 
we believe that evaluation in the weight - bearing position is important in terms of treatment approach , as it may be able to differentiate a partial tear from a simple plantar fasciitis and therefore change the type of treatment . there are a number of limitations to our study , including : ( 1 ) the absence of a reference standard , which could be constituted by the intraoperative findings , the only incontrovertible evidence ; and ( 2 ) the limited number of cases with a clinical diagnosis of plantar fasciitis and consequently the limited number of patients with assumed evidence of a fascial tear ( only four cases ) , which only allow for the formulation of a hypothesis and not an affirmation supported by statistical evidence . 
in consideration of these limitations , we believe that further studies conducted on larger patient populations and with objective validation can confirm our hypothesis . riscontrato nel 40% dei casi ( 2 / 5 ) , era di dimensioni limitate ( diametro massimo 4 mm ) e verosimilmente dovuto ad alterazioni microtraumatiche da sovraccarico . 
 il reperto accessorio sperone calcaneare stato rilevato nel 46 , 67% dei casi con fascite plantare , ma come evidenziato da altri autori la correlazione casuale e non riveste alcuna rilevanza [ 1 , 3 , 911 , 13 ]  . 
i reperti associati e quelli accessori sono stati rilevati in egual misura senza significative differenze sia nelle acquisizioni in clinostatismo che in quelle sotto carico . laumento dello spessore e la presenza di alterazioni del segnale della fascia risultano un parametro altamente sensibile in quanto indice di patologia , ma nella nostra esperienza aspecifico , poich presente sia in corso di fascite plantare che di lesione parziale , come evidenziato nel nostro studio in 4 / 15 casi ( 27% )  . 
pertanto , non esistono degli standard di riferimento che supportino lipotesi che le aree di maggiore iperintensit di segnale rilevate nel contesto della fascite plantare sotto carico siano lesioni parziali slatentizzate dalla tensione della fascia plantare . 
riteniamo che lapplicazione della valutazione in ortostatismo sia importante , in termini di approccio terapeutico , in quanto potrebbe , in alcuni casi , differenziare una lesione parziale da una semplice fascite plantare e cambiare il tipo di trattamento . 
l - fgs in a dominant ts , partial l - fgs in the distal part or o - fg in the medial part of any ts , a left - right mean diameter < 3 mm and absence of flow even in tof images perpendicular to the direction of blood flow should raise the suspicion of sinus pathology . keywords time - of - flight mr venography flow artefacts transverse sinuses anatomical variants venous sinus thrombosis riassunto obiettivo . 
il diametro del st destro risultato significativamente pi grande del controlaterale ( 6 , 5 mm1 , 84 vs 5 , 1 mm1 , 72 ) ; il diametro medio dei st destro - sinistro risultato di 5 , 77 mil st risultato di calibro dominante a destra nel 61% ed a sinistra nel 17% dei casi . 
dei 204 st studiati , 44 presentavano dl e 42 do . la parte distale dei st non ha mai presentato dl parziali ( meno di 2 / 3 del st )  . 
si dovrebbe sospettare una patologia a carico dei seni trasversi ogniqualvolta si riscontri : dl in un st dominante ; dl parziali nella parte distale del st ; do nella parte mediale del st ; diametro medio dei st inferiore a 3 mm ; assenza di flusso ematico anche nelle sequenze 2d - tof perpendicolari alla direzione di flusso . 
 radiol med ( 2010 ) 115 : 326338 parole chiave venografia rm in tempo di volo 2d ( 2d - tof ) artefatti del flusso semi trasversi varianti anatomiche trombosi dei seni venosi introduction introduzione the neuroradiological diagnosis of venous sinus thrombosis is challenging because of the high frequency of dural sinus anatomical variants . 
moreover , two - dimensional time - of - flight ( 2d tof ) magnetic resonance ( mr ) venography is affected by a progressive signal loss caused by slow - flowing protons and / or by the flow of protons that can be parallel rather than perpendicular to the imaging plane . 
we focused on the frequency of anatomical variants of posterior fossa dural sinuses in a nonselected population in order to define some measurable parameters that could help in detecting the presence of sinus pathology . 
moreover , we analysed the length , position and incidence of flow gaps ( fg ) and the efficacy of short lasting additional sequences in discriminating artefacts from thrombosis . materials and methods we prospectively examined 102 patient ( 59 male and 43 female ; mean age 43 years ; age range 20 days to 85 years ) who underwent cerebral mr examination for reasons other than venous thrombosis or idiopathic intracranial hypertension . 
all mr venograms were performed on a 1.0 - t scanner ( marconi picker polaris ) using a 2d tof mr angiographic technique without contrast medium ( cm ) administration . 
coronal plane images were obtained with a section thickness of 1.5 mm ( 30 / 8.9 / 40 , tr / te / flip angle ) , fov 200 mm and matrix 256128 . 
inoltre , langiografia venosa con tecnica 2d in tempo di volo ( 2d - tof ) risente di una progressiva perdita di segnale determinata da un lento flusso dei protoni e / o da un flusso parallelo , piuttosto che perpendicolare , al piano di acquisizione . 
in una popolazione non selezionata , abbiamo valutato la frequenza di varianti anatomiche dei seni venosi durali della fossa cranica posteriore al fine di definire parametri semplici in grado di facilitare il riconoscimento di trombosi dei st . abbiamo , inoltre , analizzato estensione , posizione ed incidenza dei difetti di flusso , nonch lefficacia di sequenze addizionali nel discriminare la trombosi dagli artefatti . 
 materiali e metodi sono stati studiati , in modo prospettico , 102 pazienti ( 59 maschi ; et media 43 anni , range det da 20 giorni a 85 anni ) che hanno eseguito una risonanza magnetica ( rm ) cerebrale per indicazioni cliniche non sospette per trombosi venosa od ipertensione intracranica idiopatica . prima dellesame stato ottenuto il consenso informato dai pazienti o dai genitori dei minori . 
tutti le venografie rm sono state eseguite mediante uno scanner da 1 , 0 t ( marconi picker , polaris ) con tecnica 2d - tof senza mezzo di contrasto ( mdc )  . 
le acquisizioni sono state eseguite in un piano coronale con spessore pari a 1 , 5 mm ( 30 / 8 , 9 / 40 , tempo di ripetizione [ tr ] / tempo di eco [ te ] / flip angle ) , campo di vista ( fov ) 200 mm , matrice 256128 . 
il tempo di acquisizione stato di 4 minuti e 12 secondi ( la porzione anteriore del sistema venoso non stata analizzata al fine di ridurre i tempi di acquisizione )  . stata applicata una banda di saturazione alla base del collo per eliminare il segnale delle strutture arteriose . 
 three - dimensional mr reconstructed angiograms were la ricostruzioni agiografiche 3d sono state ottenute 328 radiol med ( 2010 ) 115 : 326338 generated using a maximum intensity projection algorithm ( mip , 12 projections with intervals of 13 )  . 
whenever a flow gap was detected , we applied several slices of the same 2d tof sequence perpendicularly to the direction of blood flow . this was done to limit in - plane saturation and check actual absence of flow within the fg . 
ts calibre was measured on mip 3d reconstructions by a neuroradiologist at the distal two thirds to avoid most filling defects ; ts calibre of a subgroup of patients ( 21 ) was independently measured by a second neuroradiologist to evaluate interobserver agreement . 
queste immagini supplementari sono state effettuate per ridurre la saturazione degli spin e verificare leffettiva assenza di flusso allinterno del difetto di riempimento ; lacquisizione supplementare ha richiesto 2535 secondi in relazione al numero di immagini . 
il diametro del st stato misurato da un neuroradiologo sulle ricostruzioni mip 3d nei due terzi distali , per evitare la maggior parte dei difetti di riempimento ; il calibro del st di un sottogruppo di 21 soggetti stato misurato indipendentemente da un secondo neuroradiologo per valutare la variabilit inter - osservatore delle misure . 
stato usato il test del chiquadrato di pearson per valutare la correlazione fra difetti lineari ( dl ) e dominanza / non - dominanza dei st . risultati nel nostro campione il st destro ha presentato un diametro medio significativamente pi grande del sinistro ( 6 , 5 mm1 , 84 vs 5 , 1 mm1 , 72 , range 210 mm , p < 0 , 0001 , test t di student per dati appaiati )  . 
nel 78% dei soggetti si sono trovate asimmetrie a carico dei st ( una dominanza destra e sinistra stata osservata rispettivamente nel 61% e 17 % dei casi )  . 
short linear defects were usually in the medial or , less frequently , central part of the ts ( 14 and 11 , respectively ) , whereas they were never found in the lateral part . 
in all but two l - fgs , sagittal tof images showed a roughly triangular hyperintensity at the inferiorposterior border of the tentorium , proving the presence of blood flow within the sinus defect and therefore sinus patency . 
st dominanti non hanno mai presentato dl ; questo tipo di difetto stato riscontrato pi frequentemente nei st non - dominanti ( 34 / 80 , indipendentemente dal lato ) rispetto ai co - dominanti ( 10 / 44 ) ( p = 0 , 03 , test del chi - quadrato di pearson )  . secondo un altro punto di vista , il 44% dei st non dominanti e il 23% dei st co - dominanti hanno presentato un dl . il dl appariva di dimensioni piccole ( < 1 / 3 della lunghezza del st ) , medie ( < 2 / 3 ) o completo ( > 2 / 3 ) in 25 , 9 e 10 casi rispettivamente . 
dl piccoli erano solitamente localizzati nella porzione prossimale mediale o , meno frequentemente , nella porzione intermedia dei st ( 14 ed 11 casi rispettivamente ) , mentre non sono mai stati riscontrati nella porzione laterale distale . 
fatta eccezione per due casi , in tutti i dl le immagini 2d - tof sagittali supplementari hanno evidenziato uniperintensit triangolariforme in 330 these were located in the central and lateral part of the ts in three and 39 cases , respectively . 
fifteen , 14 and 13 were harboured in dominant , nondominant and codominant ts , respectively , without any difference according to sinus size . seventeen o - fgs were on the right and 25 on the leof these , only three ( 9% ) were in the central part of a ts . 
all l - fg were close to a labb ve oblique tof images , obtained perpendicularly to the blood flow direction within this type of sinus defect , showed the persistence of an radiol med ( 2010 ) 115 : 326338 fig . 
c calibro medio dei seni trasversi destro e sinistro , il calibro dei st di destra e sinistra ( a , b ) presenta una distribuzione ampia che si riduce notevolmente quando si consideri il valore medio ( c )  . corrispondenza del margine infero - posteriore del tentorio compatibile con la presenza di flusso ematico allinterno del dl , dimostrando quindi la perviet del st . 
 quarantadue soggetti ( 41% ) presentavano difetti di flusso di forma ovalare ( do ) , localizzati nella porzione centrale e laterale dei st in 3 e 39 casi rispettivamente . 
lo studio agiografico convenzionale mediante cateterismo ( dsa ) stato considerato a lungo il gold standard nella valutazione dei seni venosi radiol med ( 2010 ) 115 : 326338 fig 3a , c three - dimensional maximum intensity projection reconstructions of 2d tof venography acquired with coronal images . 
b parasagittal tof image on the flow gap clearly depicts the superficial cerebellar veins ( arrowheads ) and a small triangular - shaped transverse sinus along the inferior - posterior border of the cerebellar tentorium ( open arrow ) , thus demonstrating the patency of the transverse sinus ( hypoplastic transverse sinus )  . 
recently , further interest has been raised by the observation that sinus abnormalities may be anche se spesso non fornisce una visione panoramica delle strutture venose intracraniche , invasivo , necessita di somministrazione di mdc ed espone a radiazioni ionizzanti . risultati similari possono essere ottenuti con esami tc , soprattutto se si usa un sistema multi - detettore , durante somministrazione in bolo di mdc con lausilio di tecniche pi o meno sofisticate di ricostruzione 3d ( ad es . , ricostruzioni multi - planari , di sottrazione delle strutture ossee , ecc ) [ 4 ]  . 
sebbene queste tecniche si siano dimostrate diagnostiche e meno invasive della dsa , anche lesame tc richiede somministrazione di mdc ed esposizione ai raggi x e pu essere inficiato dalla presenza di clip metalliche 332 radiol med ( 2010 ) 115 : 326338 fig . 
4a - c three - dimensional maximum intensity projection reconstructions of 2d tof venography acquired with coronal images in normal anatomical variants ; d contiguous 2d tof images perpendicular to the blood flow direction within the oval flow gap ( shown in c )  . 
a roughly anteroposterior view of the intracranial venous system shows an oval flow gap ( * ) in the lateral part of the right transverse sinus , close to the termination of a labb vein ( arrows )  . 
4a - c ricostruzioni 3d mip di venografie 2d - tof acquisite in piani coronali , in varianti anatomiche normali ; d immagini 2d - tof contigue , perpendicolari alla direzione di flusso ematico del difetto ovale mostrato in c . 
a visione anteroposteriore obliqua del sistema venoso intracranico evidenzia un difetto ovale di flusso ( * ) nella porzione laterale del seno trasverso destro , in prossimit della confluenza della vena di labb ( frecce )  . 
digital subtraction angiography ( dsa ) has long been considered the gold standard , even though it often does not depict the venous structures as a whole and is invasive , requiring cm administration and x - ray exposure . 
la venografia rm ha sostituito le precedenti metodiche ed divenuta la tecnica preferenziale per lo studio del sistema venoso intracranico . progressi recenti come lintroduzione di differenti schemi di acquisizione del k spazio e di tecniche di acquisizione parallela , specialmente con macchine a 3 t , hanno migliorato significativamente lo studio delle vene e dei seni intracranici [ 5 ] , ma richiedono comunque la somministrazione di mdc e la disponibilit di scanner recenti e ad elevato campo magnetico . 
b parasagittal tof image on the flow gap reveals the lack of a triangular - shaped transverse sinus along the inferior posterior border of the cerebellar tentorium , thus demonstrating transverse sinus thrombosis ( open arrow )  . 
5a , c ricostruzioni 3d mip di venografie 2d - tof acquisite in piani coronali ; b , d immagini 2d - tof perpendicolari alla direzione del flusso ematico allinterno del difetto di flusso : a visione dallalto del sistema venoso intracranico evidenzia lassenza del seno trasverso di sinistra ( frecce )  . 
b limmagine parasagittale tof di un difetto di flusso evidenzia la mancanza del seno trasverso di forma triangolare ( frecce aperte ) lungo il bordo inferoposteriore del tentorio cerebellare suggerendo la trombosi del st ( freccia aperta )  . 
although these images have proved to be diagnostic and less invasive than dsa , ct still requires cm administration and x - ray exposure and may be limited by the presence of highly enhancing tumours or metallic vascular clips . 
mr angiography has replaced previous techniques and has become the favourite method of imaging the intracranial venous syste recent advances such as the introduction of different k - space acquisition schemes and parallel acquisition techniques , especially with 3 - t scanners , have substantially improved the depiction of intracranial veins and sinuses [ 5 ] but still require cm and modern high - field scanners . 
this limitation is persiste anche quando il sistema venoso valutato con sequenze per parenchima ( come la magnetization - prepared rapid acquisition with gradient echo [ mprage ] ) soprattutto in fase subacuta [ 7 ]  . 
questo aspetto di particolare rilievo nelle urgenze , quando pu essere difficile stabilire la presenza di insufficienza renale o di pregresse reazioni avverse in pazienti confusi o privi di coscienza e sono pertanto preferibili sequenze senza mdc . 
b lateral view of the right transverse sinus after removal of the contralateral transverse and sigmoid sinuses in order to avoid superimposition of the vessels ; the shape and the position of the oval gap ( arrow ) suggest the coexistence of a pacchionian granulation . 
b visione laterale del seno trasverso di destra dopo la rimozione dei seni venosi trasverso e sigmoideo controlaterali eseguita per evitare una sovrapposizione di strutture venose ; la forma e la posizione del difetto ovale ( freccia ) suggerisce la compresenza di una granulazione di pacchioni . 
c visione laterale obliqua visualizza un difetto di flusso ( freccia ) nella porzione distale del seno trasverso di sinistra ; nei soggetti normali in questa porzione del seno trasverso non si riscontrano difetti lineari di flusso . 
 present also when the venous system is evaluated with parenchymal sequences [ such as magnetisation - prepared rapid acquisition gradient echo ( mp - rage ) ] , particularly during the subacute phase of the thrombus [ 7 ]  . 
conversely , contrast - enhanced venography with fast t1 sequence and central fourier space acquisition may be less affected . nevertheless , the use of cm has recently been debated , as the number of reports on nephrogenic systemic fibrosis has recently increased . 
to manage these uncommon but not rare cases , it may be crucial to gain experience and confidence with nonenhanced sequences and with their most frequent artefacts . phase - contrast mr venography may be limited by gradient imperfections , eddy currents and difficulties in accurate selection of velocity encoding , whereas tof mr venography suffers from progressive signal loss caused by slowflowing protons and the flow of protons parallel rather than perpendicular to the imaging plane . 
nevertheless , with this acquisition , nella quale controindicata la somministrazione di mdc . per gestire queste situazioni , poco comuni , ma non rare , cruciale acquisire esperienza e confidenza con le sequenze senza mdc e con i loro pi frequenti artefatti . 
 langio - rm con contrasto di fase pu essere limitata da imperfezioni dei gradienti , da correnti di eddy e da difficolt nel selezionare una adeguata velocit di codifica mentre langio - rm 2d - tof pu essere inficiata da una progressiva perdita di segnale dei protoni con flusso lento o parallelo , piuttosto che perpendicolare al piano dellimmagine . 
lacquisizione coronale sembra essere la pi sensibile per la visualizzazione dellintero sistema venoso , per la predominate direzione antero - posteriore del flusso ematico nei seni durali [ 8 ]  . 
 sfortunatamente questi seni sono pure caratterizzati da una notevole variabilit anatomica e da un frequente coinvolgimento nelle trombosi venose , nellipertensione idiopatica intracranica e nei tumori della fossa cranica posteriore . 
per questo motivo ci siamo concentrati sulla visualizzazione di st nelle ricostruzioni mip delle immagini 2dtof , valutando diametro ed asimmetria dei st e la presenza di difetti di flusso ematico in soggetti normali . 
queste misure non vanno considerate come diametri radiol med ( 2010 ) 115 : 326338 artefacts are particularly frequent within the posterior part of the intracranial sinuses close to the torcular herophili . unfortunately , these sinuses are also characterised by a challenging anatomical variability and frequent involvement in venous thrombosis , idiopathic intracranial hypertension and posterior fossa tumours . 
for this reason , we focused on the ts appearance in 2d - tof - derived 3d mip reconstructions , evaluating sinus diameter , asymmetry and fgs in normal individuals . 
these measurements are not intended as being the true anatomical diameter of the sinuses , as they represent the blood flow inside the vessels and not the vessel walls themselves . 
therefore , although these data are not to be used as anatomical references , they may be useful in a clinical setting when dealing with suspected thrombosis or anatomical variants . in our sample , the side - to - side diameter difference was shown to be slightly more pronounced than that found by baikov et al . 
the difference may be due either to the age of our sample , which was greater on average , or to the different scanner and sequence parameters used , as we know that the measurements refer to the visualised flow and not directly to the sinus calibre . 
these findings are comparable with the results of several papers [ 1014 ] on venous mr angiography and dsa and are compatible with the observations by rhoton on the anatomy of the jugular foramen [ 15 ] , whose dominance proved to be on the right in 68% and on the left in 20% of cases . 
even though we found no correlation between age and ts asymmetry or agerelated differences in venous anatomy , the small number of children in our sample does not allow us to apply these results in a paediatric setting , and specific studies are needed before drawing final conclusions . in our sample the diameter of both sinuses varied greatly , and therefore , it seems that direct measurement of the diameter itself is of little help in defining the presence of pathology . 
interestingly , the mean value of the rightleft ts diameter showed less variability , as a narrow ts is usually associated with a compensatory wide contralateral ts in normal indivituals . 
in our cohort , no one had a rightleft mean diameter < 3 mfor this reason , we believe that a ts thrombosis or stenosis should be suspected whenever a mean right - left ts diameter approaches this value . the small calibre of a ts determines other important consequences . 
in one large study on normal individuals , 2d mr venography revealed ts atresia in about anatomici dei seni dal momento che esse rappresentano il flusso ematico e non la parete dei vasi . 
ciononostante , pur non essendo utilizzabili come valori di riferimento da un punto di vista anatomico , possono essere utili dal punto di vista clinico quando si debba dirimere fra la presenza di trombosi venosa o di una variante anatomica . nel nostro campione , la differenza di diametro tra i due lati risultato leggermente maggiore di quanto riscontrato da baicov et al . 
la differenza dei risultati , rispetto al nostro studio , pu essere imputabile sia allet dei soggetti , in media maggiore nel nostro campione , sia allutilizzo di macchine e sequenze diverse , essendo le misurazioni relative al flusso ematico e non al calibro del seno . la maggior parte dei nostri pazienti presentava una asimmetria dei st con una frequente dominanza del st destro . 
questi risultati sono simili a quanto riscontrato in numerosi articoli [ 1014 ] sulla venografia rm e sulla dsa e sono paragonabili alle osservazioni di rhoton a proposito dellanatomia del forame giugulare [ 15 ] , la cui dominanza nel 68% dei casi a destra e nel 20% a sinistra . 
anche se non abbiamo riscontrato alcuna correlazione fra et ed asimmetria dei st , n differenze di anatomia dei seni venosi in relazione allet , lesiguo numero di bambini esaminati non permette di estendere le nostre osservazioni alla popolazione pediatrica , rendendo necessari studi mirati . 
da sottolineare invece che il valore medio dei diametri dei st destro e sinistro ha dimostrato minore variabilit , dal momento che un piccolo st generalmente associato ad un st controlaterale ampio di significato compensatorio . 
nella nostro campione nessun soggetto aveva un diametro medio dei st inferiore ai 3 mm . per questo motivo si dovrebbe sospettare una trombosi o stenosi di un st qualora la media dei diametri fra st di destra e sinistra si avvicini a questo valore . 
in un ampio studio di soggetti sani , questa tecnica ha evidenziato una atresia del st di destra nel 20% dei casi e di sinistra nel 4% [ 10 ] , in contraddizione con studi di angiografia , in cui la prevalenza cumulativa stata del 2 , 63% ( 2 , 1% e 0 , 53% , rispettivamente ) [ 13 ]  . 
 [ 11 ] reported that 31% of their patients had fgs within the ts potentially undistinguishable from thrombosis , 90% of which were in the nondominant sinus and 10% in codominant sinus . 
this emphasises the frequent difficulty in clinical practice of discriminating an anatomical variant from a ts thrombosis . on the other hand , l - fgs were not observed in dominant ts in our study , so we can assume that the finding of a linear gap within a dominant ts should be interpreted as partial thrombosis or stenosis . 
as these fgs represent a real challenge when scanning a patient with a clinical phenotype , suggesting sinus thrombosis or idiopathic intracranial hypertension , we direct the acquisition plane perpendicular to the long axis of the ts to overcome artefactual signal loss resulting from in - plane vascular flow . 
 in two cases , the added sagittal sequence did not show intravascular blood flow and , consequently , a ts aplasia was supposed ( a prevalence of 2% of aplasia in our cohort is comparable with that reported in the abovementioned angiographic study )  . 
our frequency was significantly lower compared with that found with parenchymal ct or mr studies [ 7 , 17 ] , probably due to intrinsic limits of the tof sequence , particularly when mip reconstructions were used . 
these defects are usually located in the lateral part of the ts in correspondence with a labb vein and may be suspicious when found in the medial part of a ts . 
in these cases , a contrast - enhanced thin mp - rage sequence or a high - resolution ct examination may show the presence of a vein entering the filling defect , a feature that characterises arachnoid granulations . we emphasise that all data obtained in our cohort refer to patients whose brain mr scan was judged normal . 
in some of them , the indication was headache , a clinical condition which may be caused by an undiagnosed cerebral venous difficolt , nella pratica clinica , di differenziare varianti anatomiche da trombosi del st . 
dal momento che il riscontro di un difetto di flusso ematico venoso in un paziente con un quadro clinico suggestivo di trombosi o di ipertensione endocranica idiopatica , rappresenta un reale problema diagnostico , abbiamo effettuato alcune sezioni 2d - tof perpendicolari allasse maggiore del st , per minimizzare lartefattuale perdita di segnale di flussi ematici lenti che permangano allinterno del piano di sezione . 
 in due soli casi la sequenza sagittale supplementare non ha evidenziato flusso ematico in corrispondenza del st , suggerendo una aplasia del seno stesso ( la prevalenza di aplasia del 2% nella nostra casistica in accordo con quanto riportato nello studio angiografico sopra menzionato )  . 
in tutti gli altri casi questa sequenza stata in grado di evidenziare la perviet del seno , dimostrando di essere un potente strumento in grado di discriminare gli artefatti di flusso ematico dalla trombosi del st . 
abbiamo riscontrato una frequenza significativamente pi bassa di quella riscontrata con tomografia computerizzata ( tc ) o rm per parenchima [ 7 , 17 ] probabilmente in relazione a minor sensibilit della sequenza tof , in particolare quando vengano utilizzate ricostruzioni mip . 
in questi casi , una sequenza mprage a strato sottile con mdc o un esame tc ad elevata risoluzione possono mostrare una vena che entra nel difetto di riempimento , una caratteristica che distingue le granulazioni aracnoidali . 
moreover , due to the numerous collateral circulations , some cases of venous thrombosis may also be asymptomatic ( many patients affected by thrombosis become asymptomatic before complete recanalisation of the sinuses )  . 
as sinus thrombosis is relatively rare in the general population and our cohort was relatively large , we believe that these data , even with some caveats , may reflect the normal anatomy of the posterior portion of the intracranial venous sinuses and can therefore be confidently used as a reference when dealing with suspected sinus pathology . 
 conclusions evaluation of the posterior part of the intracranial venous sinuses remains challenging , but a few tips may help identify anatomical variants and artefacts due to the technique employed . 
poich la trombosi dei seni una condizione relativamente rara nella popolazione generale e la popolazione considerata nel nostro studio relativamente ampia , riteniamo che questi dati , pur con qualche cautela , possano essere rappresentativi della anatomia normale dei seni venosi della fossa cranica posteriore e possono pertanto rappresentare un valido riferimento quando si debba diagnosticare una loro patologia . 
 conclusioni la valutazione dei seni venosi della fossa cranica posteriore problematica , ma alcuni aspetti semeiologici possono essere di aiuto nel discriminare le varianti anatomiche dagli artefatti dovuti alla tecnica utilizzata . 
francone1 , 3 1department of radiology , gasthuisberg university hospital , uz leuven , herestraat 49 , b - 3000 leuven , belgium 2department of radiology , apss of trento ospedale s . 
the aim of this pictorial review is to provide a stepwise approach to assessing the heart on routine nonelectrocordiographic - gated ( non - ecg - gated ) chest ct and describing common and less frequent cardiac abnormalities . 
 keywords chest computed tomography myocardial morphology atrial and ventricular septum cardiac chambers cardiac valves pericardium introduction with the introduction of computed tomography ( ct ) in the late 1970s , noninvasive visualisation of the human body became a reality . 
however , with the introduction of multislice ct systems using fast rotating tubes almost 10 years ago , cardiac ct imaging revived and gained riassunto il referto radiologico di una tc del torace si focalizza soprattutto sulla rilevazione delle alterazioni del parenchima polmonare e del mediastino , mentre la valutazione del cuore viene trascurata . 
tuttavia , spesso si riscontrano e vengono misinterpretate anomalie cardiache incidentali , che potrebbero avere un significativo impatto clinico e terapeutico sul paziente o che necessiterebbero di ulteriori approfondimenti diagnostici . 
 scopo di questa rassegna iconografica fornire gli strumenti per un approccio ragionato al cuore negli esami tc del torace di routine , non cardiosincronizzati , descrivendo sia le anomalie cardiache pi comuni sia quelle meno frequenti . parole chiave tomografia computerizzata del torace morfologia miocardica setto interatriale ed interventricolare camere cardiache valvole cardiache pericardio widespread interest in the radiological and cardiological community [ 1 ]  . 
 176 radiol med ( 2010 ) 115 : 175190 in this paper we show a selection of cardiac abnormalities that can be encountered in daily routine chest ct practice . cardiac position and orientation in the majority of patients , the heart is ventromedially positioned in the chest , with the apex levocaudally oriented . body constitution , age and inspiratory depth influence the degree of orientation , tending to be more vertical in younger or slender individuals and more horizontal in obese patients . abnormalities in cardiac position , orientation and configuration may be the result of congenital or acquired cardiac pathology or the consequence of mediastinal , pleural , pulmonary , diaphragmatic or chest - wall pathology , which may be influencing the cardiac position or configuration ( table 1 )  . 
an abnormal cardiac orientation and / or shape may be the first sign of an underlying congenital anomaly and should urge the radiologist to carefully analyse the different cardiac components . 
in case of extracardiac pathology , one should carefully assess for compression of cardiac structures that may impede cardiac filling . cardiac chambers morphological cardiac analysis morphological analysis of the heart should be stepwise , assessing the characteristics of the different cardiac chambers as well as the connection pattern between atria and ventricles and between ventricles and great arteries . 
the atria are always posteriorly located in the heart , whereby the pulmonary veins drain in the left atrium and the caval veins and coronary sinus in the right atriuboth have an appendage , which are short and broadbased on the right and long , and narrow - based on the left . the right atrium has a typical muscle ridge , the crista terminalis , which separates the smooth - walled posterior portion from the muscular anterior region . 
 the morphological left ventricle ( lv ) always bears the mitral valve and the right ventricle ( rv ) the tricuspid valve , whereby the tricuspid valve is more apically implanted than the mitral valve . 
accurate assessment of atrioventricular valve position , however , necessitates a four - chamber cardiac view , which may not coincide with the axial ct radiol med ( 2010 ) 115 : 175190 fig . 
the morphological left side of the heart is positioned towards the right and the right side of the heart towards the le normal atrioventricular and ventriculoarterial concordance ; presence of a right aortic arch . 
a fine muscular structure connecting the apical half of the ventricular septum to the rv lateral ( or free ) wall , which was initially thought to prevent overdistension of the ventricle ( moderator function ) and more recently considered as part of the hearts electrical conduction system ; presence of a muscular infundibulum , which separates the tricuspid from the ventriculoarterial valve ; septal leaflet of the tricuspid valve , which arises from the ventricular septum , and coarse trabeculations in the rv apex on the other hand , lateral wall location and thickness are no reliable features in defining the morphological rv . 
structural cardiac analysis is not complete without concomitant assessment of the course , shape and morphology of the great vessels . changes in chamber dimensions whereas imaging techniques such as echocardiography , magnetic resonance imaging ( mri ) and ecg - triggered cardiac ct use either geometric assumption or volumetric approaches to quantify chamber dimensions , cardiac chamber dimensions on chest ct images are usually 178 radiol med ( 2010 ) 115 : 175190 fig . 
it bears typical features of an rv , such as the presence of a moderator band ( asterisk ) , rough apical trabeculations and complete muscular infundibuluthe rv serves as the systemic ventricle and is markedly dilated . 
notare la posizione pi apicale della valvola tricuspide ( frecce ) , rispetto alla valvola mitralica ( punte di freccia ) , altro utile indizio nella differenziazione della morfologia ventricolare . 
this can be achieved by comparing sizes of the different chambers or , in the case of global cardiac enlargement , assessing the relation of the heart to the chest . 
contrast - enhanced computed tomography ( ct ) ( window level 50 hu , window width 500 hu )  . right ventricle ( rv ) enlargement is visible on caudal views ( a ) as an rv extension below the inferior left ventricle ( lv ) level . 
la dilatazione del ventricolo destro ( rv ) osservabile nel piano pi caudale ( a ) come prolungamento del rv al di sotto delle porzioni pi inferiori del ventricolo sinistro ( lv )  . 
due to altered flow characteristics ( slow or stagnant flow ; turbulent flow ) , dilated chambers are at risk for thrombus formation , stressing the need for careful analysis of the enlarged chambers for filling defects on contrast - enhanced ct . 
thus , correct interpretation of morphological cardiac abnormalities necessitates knowledge of cardiac pathophysiology . moreover , in patients with cardiac chamber enlargement , vascular structures , lung parenchyma and pleural space are also often affected . 
important dilation of the right ventricle ( rv ) with inversion of the ventricular septum ( b , arrow ) , reflecting an important rise in pulmonary artery and rv pressure . 
significativa dilatazione del ventricolo destro ( rv ) , con inversione della curvatura del setto interventricolare ( b , freccia ) , per limportante aumento pressorio nellarteria polmonare e nel rv . 
il paziente ha avuto un collasso subito dopo lo studio tc ed deceduto , nonostante lintervento chirurgico cardiopolmonare effettuato in urgenza . of ( an ) other chamber ( s )  . 
 atrial and ventricular septum the atrial septum consists of interatrial and atrioventricular sections , whereas the ventricular septum can be divided into a muscular septum and a short membranous portion at the base . 
clinically significant atrial and ventricular septal defects are usually diagnosed and treated in childhood . adult patients with untreated tetralogy of fallot with large subaortic septal defects , overriding aorta , rv dilation , hypoplasia or agenesis of the rv outflow tract and pulmonary valve and extensive collateral flow can be encountered on chest ct ; for example , during the clinical workup of a pre - heartlung transplant . 
chest ct in patients with dyspnea and signs of enlargement of the right side of the heart may occasionally reveal a partial abnormal pulmonary venous return with a sinus venosus atrial septal defect . 
rarely , deep muscular clefts in the ventricular septum can be found , most likely reflecting closed muscular ventricular septal defects [ 13 ]  . fat deposition in the atrial septum , a disease entity called lipomatous hypertrophy of the atrial septum , is a frequent finding on chest ct in the elderly population and more frequently in obese patients [ 14 ]  . 
in patients with pulmonary emboli , the position of the ventricular septum is increased short - term mortality [ 11 ]  . a predictor of decreased pulmonary arterial pressures , for instance after pulmonary endarterectomy in patients with chronic pulmonary thromboembolism , is associated with a normaliradiol med ( 2010 ) 115 : 175190 fig . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) shows thickened , hypodense appearance ( mean density 87 hu ) of the atrial septum ( asterisks ) , typically sparing the oval fossa ( b , arrow )  . 
lesame tc con mdc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) mostra un setto ( asterischi ) ispessito ed ipodenso ( densit media 87 hu ) , con tipico risparmio della fossa ovale ( b , freccia )  . 
contrast - enhanced chest computed tomography ( ct ) ( a , window level 50 hu , window width 500 hu ) shows thickened appearance of the atrial septum extending to the right atrial wall ( asterisk )  . 
lesame tc con mdc del torace ( a , centro della finestra 50 hu , ampiezza 500 hu ) mostra ispessimento del setto interatriale , che si estende alla parete dellatrio destro ( asterisco )  . 
rispetto allipertofia lipomatosa , il setto mostra elevata densit ( densit media 92 hu ) e viene evidenziata come unarea di ipercaptazione del f - 18 - fluoro desossiglucosio alla tomografia ad emissione di positroni ( b , frecce )  . sation of the ventricular septal shape and position [ 15 ]  . atrial septum bulging can be found in mitral or tricuspid valve pathology , as well as cardiac conditions characterised by increased filling pressures . 
contrast - enhanced computed tomography ( ct ) ( a , window level 50 hu , window width 500 hu ) shows severe concentric left ventricular ( lv ) wall thickening and bilaterally a small pleural effusion . 
contrast - enhanced inversion - recovery gradient - echo magnetic resonance imaging ( mri ) acquired in midventricular short - axis scan ( b ) shows strong enhancement of the thickened myocardium ( maximal end - diastolic wall thickness , 26 mm )  . 
lesame tc con mdc del torace ( a , centro della finestra 50 hu , ampiezza 500 hu ) mostra severa ipertrofia concentrica del ventricolo sinistro ( lv ) , con versamento pleurico bilaterale di lieve entit . nello studio con risonanza magnetica ( rm ) , le sequenze inversion recovery , acquisite in asse corto a livello medio - ventricolare dopo somministrazione di mezzo di contrasto ( b ) , mostrano marcato enhancement del miocardio che appare diffusamente ispessito ( massimo spessore di parete in telediastole 26 mm )  . 
follow - up contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) shows homogeneous isodense thickening of the apical one third of the septal and lateral left ventricular ( lv ) wall ( maximal end - diastolic wall thickness 14 mm ; asterisks )  . 
il follow - up tc con mdc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) mostra un ispessimento , omogeneamente isodenso al miocardio , del terzo apicale del setto e della parete laterale del ventricolo sinistro ( lv ) ( massimo spessore di parete , misurato in fase telediastolica 14 mm ; asterischi )  . 
 radiol med ( 2010 ) 115 : 175190 non - ecg - triggered , one should be cautious to interpret myocardial wall thickness , as images can be diastolically or systolically acquired . 
 the lv myocardium is thickest towards the base ( 612 mm ) and thinnest towards the apex ( 12 mm ) ; the myocardium of the rv free wall ranges between 1 and 3 mabnormal myocardial wall thickening can be global or focal , unior bi - ventricular . 
hypertrophy of the rv wall occurs when this chamber functions as a systemic ventricle in cases of transposition of the great arteries or when exposed to other causes of increased afterload , such as pulmonary valve stenosis or pulmonary arterial hypertension . 
in contrast , focal lv wall thinning is most often the consequence of previous myocardial infarction with fibrotic replacement of the necrotic myocardiuthis may be associated with wall bulging , aneurysm formation , lipomatous metaplasia and compensatory thickening of the fig . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) shows thinning of the left ventricular ( lv ) apex ( white arrows ) and of the laterobasal lv wall ( black arrows ) , with bulging of the thinned areas . 
11 cardiomiopatia ischemica con infarto miocardico cronico inferiore e anteriore in un uomo di 67 anni con diagnosi di dissezione aortica . lesame tc con mdc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) mostra lassottigliamento dellapice ( frecce bianche ) e della parete postero - basale ( frecce nere ) del ventricolo sinistro ( lv ) con bulging delle aree assottigliate . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) shows marked dilation of the lv and thinning of the compacta , with prominent appearance of the trabeculations of the lateral lv wall ( arrowheads )  . 
chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) shows heavily calcified left ventricular ( lv ) apical aneurysm ( arrowheads )  . 
lesame tc con mdc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) mostra una marcata dilatazione del lv e assottigliamento della parte compatta della parete , con evidente accentuazione della trabeculatura della parete laterale ( punte di freccia )  . 
13 aneurisma apicale calcifico in un uomo di 67 anni con cardiomiopatia ischemica e storia di infarto miocardico acuto 15 anni prima . lesame tc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) mostra un aneurisma apicale del ventricolo sinistro ( lv ) molto calcifico ( punte di freccia )  . 
non stato somministrato il mezzo di contrasto a causa di insufficienza renale cronica . remote , noninfarcted myocardiu infarcts are typically located in specific locations of the lv ( according to the occluded coronary artery ) , which may facilitate diagnosis on chest ct . 
not infrequently , mural thrombi are found in the area of the infarcted myocardiunoncompaction cardiomyopathy of the lv is a disease entity that involves predominantly the lateral lv wall and apex and presents as prominent trabeculations with a thin compacta . 
characterisation of calcification in terms of its distribution and appearance is helpful for determining which structures are calcified , thus differentiating pathologic from nonpathologic processes . pathologic calcification in the myocardium occurs by two basic mechanisms : metabolic and dystrophic . 
the first occurs when there is a derangement of the calcium / phosphate metabolism , such as chronic renal failure and hyperparathyroidism , whereas dystrophic calcifications occur in dead or degenerative tissue in the presence of normal calcium / phosphate balance , such as in previous myocardial infarctions , ventricular aneurysm , endomyocardial fibrosis , myocarditis , tuberculosis , irradiation and rare cardiac tumours [ 2224 ]  . 
in a retrospective study by zafar et al . , lipomatous metaplasia was found on ct in 51% of patients , making its presentation on ct appealing to depict silent myocardial infarctions [ 31 ]  . 
fat depositions may be found in other locations , such as midwall or subepicardium . as it was recently recognised on contrast - enhanced cardiac mri that these locations are fairly specific for myocarditis , one can hypothesise that the fat - attenuation lesions reflect healed myocarditis [ 3234 ]  . cardiac cavities opacification of the cardiac cavities on contrast - enhanced ct provides an excellent means to depict abnormal intracavitary structures , such as thrombi or tumour masses , presenting as filling defects [ 35 ]  . 
as discussed above , knowledge of normal cardiac anatomy is ubiquitous to differentiate normal from abnormal cardiac structures . moreover , in some conditions , adequate visualisation of intracavity structures may be hampered . 
15 lipomatous metaplasia of chronic infarction in the left ventricular ( lv ) lateral wall in a 57 - year - old man with a history of lung cancer . contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu )  . 
e bene riconoscibile la sostituzione degli strati di miocardio subendocardico da parte di tessuto con densit adiposa , che si presenta come una struttura curvilinea , omogenea ( frecce bianche )  . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) with reconstructed image in the coronal plane shows extensive calcifications in the left ventricular ( lv ) walls . 
la ricostruzione sul piano coronale dellesame tc con mdc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) mostra estese calcificazioni a carico delle pareti del ventricolo sinistro ( lv )  . 
non stata trovata nessuna causa che giustificasse le grossolane calcificazioni del miocardio . near the posterior mitral leaflet may be depicted , a condition called caseous calcification of the mitral valve , or liquefaction necrosis [ 25 , 26 ]  . 
though fatty myocardial replacement of the rv wall is a well - known feature of arrhythmogenic rv dysplasia / cardiomyopathy [ 20 ] , it was recently reported to be frequently present in an ( asymptomatic ) ageing population , suggesting a benign , degenerative process of the myocardium [ 27 , 28 ]  . 
thus , other criteria are needed to diagnose arrhythmogenic rv dysplasia , such as focal bulging or aneurysm formation , rv enlargement , etc . arrhythmogenic rv dysplasia may affect the lv but usually occurs only in patients with pre - existing rv involvement . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) shows sessile , sharply defined , homogeneous mass attached to the oval fossa of the interatrial septum ( arrowhead )  . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) shows obliquely running membrane ( arrow ) in left atriuthe connection between the dorsal and ventral chambers can be appreciated on the axial image ( asterisk )  . 
lesame tc con mdc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) mostra una massa vegetante , a margini netti e struttura omogenea , attaccata alla fossa ovale del setto interatriale ( testa di freccia )  . 
sullimmagine assiale si pu apprezzare la connessione tra la camera dorsale e quella ventrale ( asterisco )  . mixing of contrast in the right atrium often impedes adequate interpretation of the right atrium cavity . 
pericardial sinuses and recesses are visible as well - defined fluid - filled structures and may be mistaken as enlarged lymph nodes , oesophageal or thymic processes or vascular abnormalities . 
pericardial abnormalities on chest ct include absence of pericardium , fluid accumulation , pericardial thickening and calcification [ 38 , 39 ]  . congenital partial or complete absence of the pericardium is extremely rare . 
their detection and diagnosis are usually simple [ 39 , 40 ]  . the presence of a pericardial effusion is usually wellradiol med ( 2010 ) 115 : 175190 fig . 
18a , b haemopericardium in a 70 - year - old man with inferior left ventricular ( lv ) wall aneuryscontrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) in the axial ( a ) and coronal ( b ) planes shows moderate pericardial effusion with high density ( 55 hu ) ( asterisks )  . 
lesame tc con mdc del torace ( centro della finestra 50 hu , ampiezza 500 hu ) nei piani assiale ( a ) e coronale ( b ) mostra un modesto versamento pericardico con elevata densit ( 55 hu ) ( asterischi )  . 
ben apprezzabile la presenza di aneurisma post - ischemico della parete inferiore del lv , con significativo assottigliamento parietale ( frecce )  . diagnosi provvisoria di rottura di aneurisma con emopericardio . 
lecocardiografia per - operatoria ha rivelato un ispessimento della parete dellaorta ascendente , suggestiva di emorragia intramiocardica , con sanguinamento nel sacco pericardico . depicted on chest ct [ 39 , 40 ]  . 
 patients with inflammatory pericarditis often present with atypical , often respiratory - related , chest pain , and they are often referred for chest ct to rule out pulmonary emboli . 
in cases where a pericardial effusion is absent , ct abnormalities may not be impressive , yielding a mild , diffusely thickened pericardium enhancing after intravenous lateral lv administration of contrast material . 
19 encapsulated pericardial effusion massively compressing the right atrium in a 61 - year - old man 2 days after aortic valve replacement . contrast - enhanced computed tomography ( ct ) ( window level 253 hu , window width 1143 hu ) shows a biconvex pericardial effusion over the right atrium ( arrows ) incompletely compressing the right atrial cavity ( asterisks )  . 
lesame tc con mdc del torace ( centro della finestra 253 hu , ampiezza della finestra 1143 hu ) mostra un versamento pericardico a morfologia biconvessa al di sopra dellatrio destro ( frecce ) che comprime non completamente la cavit cardiaca ( asterischi )  . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 500 hu ) initial ( a ) and follow - up examination ( b )  . 
al follow - up , sono comparse pi calcificazioni ( frecce ) , situate soprattutto nel pericardio ma che si estendono anche al subepicardio e miocardio ( parte latero - basale del ventricolo sinistro )  . myocardial wall may appear thickened , but the inflamed pericardium has a lower density than myocardium , and pericardial abnormalities extend over the left atrioventricular groove . acute and subacute forms of inflammatory pericarditis may evolve towards a chronic fibrotic state with or without associated pericardial calcifications . 
it should be emphasised that a considerable percentage ( up to 20% ) of patients with surgically proven constrictive pericarditis present only a normal or minimally thickened pericardium , challenging the current morphologic criteria for diagnosing constrictive pericarditis [ 42 ]  . 
 pneumopericardium is an uncommon cardiac disorder caused by either the presence of communication between the pericardial sac and an adjacent air - containing organ , usually the lungs , or by infection of the pericardium by gas - forming microorganisms [ 43 ]  . 
chest ct , using the pulmonary window setting is possibly the most appropriate technique to detect even small quantities of air in the pericardial sac . cardiac valves non - ecg - triggered chest ct provides limited information on cardiac valve morphology or functionality , but it may reveal sequelae of valvular heart disease [ 44 ]  . 
this abnormality can be recognised by the apically positioned tricuspid valve ( mainly the implantation of the septal leaflet ) , causing atrialization of the rv [ 46 ]  . conclusion cardiac diseases often have distinct features on chest ct imaging . 
contrast - enhanced chest computed tomography ( ct ) ( window level 50 hu , window width 350 hu ) shows thickened tricuspid valve leaflets with moderate right atrial enlargement ( a , arrows )  . 
lesame tc con mdc del torace ( centro della finestra 50 hu , ampiezza 350 hu ) mostra ispessimento dei lembi della valvola tricuspide con modesta dilatazione dellatrio destro ( a , frecce )  . 
presenza di una modesta falda di versamento pleurico a destra . a stepwise approach to assessing the gross cardiac anatomy as well as the presentation of different cardiac elements enables morphological evaluation of cardiac status and thus allowing frequent observation of previously unknown cardiac pathologies , some of which may be of clinical importance or necessitate further investigation . 
moglioni ( eds ) cic edizioni internazionali , 2009 isbn : 978 - 88 - 7141 - 832 - 2 published online : 22 february 2010 springer - verlag 2010 it was with great pleasure that i accepted the invitation to introduce this book , not only because i know the authors personally and regard them highly , but also because diagnostic imaging in the field of dentistry is often overlooked by specialty schools of radiology . 
many young colleagues incorrectly believe that due to the increasing amount of knowledge that needs to be acquired during the years of postgraduate training , they can skip over oral and maxillofacial radiology , which appears to be a borderland between radiologists and dentists , a field where the latter move with the utmost familiarity . 
however , we are well aware that radiologists can only aspire to performing in a qualified and competent professional manner and be a real support to modern medical practice if they base their practice on a nonsuperficial knowledge of the various clinical features and the needs arising from careful treatment planning . this book , which focuses exclusively on oral implantology , is in part a response to this awareness . 
the volume , in fact , not only broadly covers the technical problems related to correctly performing a computed tomography examination of the dental arches or the appropriate interpretation of pathological findings , it deals with surgical problems of prosthesis placement and some of the aspects regarding material biomechanics and boneimplant interaction . 
in addition , the volume has the merit of filling a gap in the italian literature where publications concentrating on prosthetic implant diagnostics are sorely lacking . the book is aimed mainly at the reader undergoing specialist training in radiology or dentistry but may also be a useful aid for medical students or trainee radiographers who wish to broaden their knowledge in the instrumental diagnostics of oral implantology . as is now a common practice , the chapters have been written by various authors , but careful editing has avoided repetition or apparent contradiction , thus providing the volume with a highly appreciated consistency and clarity . in conclusion , this is a useful manual , which will be of ho accolto con grande piacere linvito a redigere la presentazione di questo volume , sia perch conosco personalmente gli autori , e nutro dei sentimenti di stima e di considerazione nei loro confronti , sia perch la parte di diagnostica radiologica dedicata allodontoiatria viene spesso trascurata nellattivit didattica delle scuole di specializzazione in radiologia . molti giovani colleghi ritengono , erroneamente , che , a causa della consistente quantit di conoscenze da acquisire durante gli anni di formazione specialistica , si possa tranquillamente sorvolare sulla radiologia odontostomatologica , la quale , peraltro , appare come un territorio di confine tra i radiologi e gli odontoiatri , territorio dove questi ultimi si muovono con estrema familiarit . 
sappiamo bene , per , che il radiologo pu aspirare alla realizzazione di un lavoro professionale qualificato e competente , che sia di reale supporto ad una moderna pratica medica , solo partendo da una conoscenza non superficiale dei diversi aspetti clinici e delle necessit che si originano da una attenta pianificazione terapeutica . il presente lavoro editoriale , dedicato esclusivamente al settore dellimplantologia orale , nasce anche per queste ultime ragioni . 
infatti , in esso si riserva adeguato spazio non soltanto ai problemi tecnici legati alla corretta esecuzione di un esame di tomografia computerizzata delle arcate dentarie o a quelli connessi alla idonea interpretazione dei quadri patologici , ma anche alla trattazione dei problemi chirurgici propri del posizionamento delle protesi , non disdegnando di presentare alcuni aspetti relativi alla biomeccanica dei materiali utilizzati e alla interazione impianto - osso . 
 il testo rivolto principalmente a coloro che si accostano allargomento nellambito della formazione specialistica , radiologica o odontoiatrica , ma pu essere di utile supporto sia agli studenti del corso di laurea in medicina e chirurgia che a quelli del corso di laurea in tecniche di diagnostica per immagini , desiderosi di approfondire le loro conoscenze nella diagnostica strumentale dellimplantologia orale . 
 i capitoli sono stati redatti , come ormai consuetudine , da diversi autori , ma la revisione generale effettuata ha evitato sovrapposizioni o punti di apparente contraddizione , conferendo alla trattazione una coerenza ed una chiarezza estremamente apprezzabili . 340 radiol med ( 2010 ) 115 : 339340 benefit to all those wishing to master the diagnostic imaging of oral implants . 
to verify if a two step school - based scoliosis screening procedure could reduce childhood radiation exposure and , if so , to estimate the subsequent reduction in radiogenic cancer fatalities and in socio - economic burden . 
children in program a ( 5 , 731 children ) were screened using a twostep procedure in which school physicians performed the first clinical examination and uncertain cases were referred to an orthopaedist . 
children in program b ( 3 , 264 children ) were screened using a one - step procedure in which the initial clinical examination was performed directly by an orthopedist . 
the economic cost of the performed x - ray examination was calculated assuming the current national health services reimbursement to hospitals of euro 35 per x - ray exathe statistic significance of the difference in these estimates between the two programs was assessed using the proportions z - test . 
i medici scolastici , dopo essere stati istruiti da ortopedici sulla semeiotica clinica elementare , hanno effettuato la prima valutazione clinica ed hanno inviato allo specialista tutti i casi dubbi . 
in entrambi i programmi , soltanto lortopedico ha richiesto gli esami radiografici . per valutare il successivo rischio di mortalit per cancro , sono state seguite le linee guida della pubblicazione 60 della commissione internazionale sulla protezione radiologica . 
a screening of the same number of children using a two - step procedure would result in 150 x - ray exams ( 1.5% ) , with a savings of euro 4 , 935 for the national health care system , a reduction of 0.283 sv of collective dose , and an estimated 50% reduction in the number of radiogenic malignant tumours . 
using a two - step scoliosis screening procedure provides reasonable sensitivity and specificity while reducing costs and radiation exposure to children . dallortopedico , comporterebbe 291 esami radiografici ( 2 , 91% )  . 
a large body of literature has been established during this time describing the beneficial results of spinal screening [ 16 ] , most notably , a reduced need for spinal fusion [ 711 ]  . 
however , epidemiologists and public policy - makers have focused their attention on scoliosis screenings concerned with the increasing difficulty of public health services to cope with the cost of the associated x - ray examinations [ 4 , 5 ]  . 
the most important international radiological protection bodies nowadays agree that the incidence of radiogenic malignant tumours is two or three times more elevated in the child than in the adult [ 1215 ]  . 
therefore , we examined the collected data of two previously used types of scoliosis screening programmes to determine whether there was a significant difference in the total collective radiation dose between the two programmes . we then considered the health ( in terms of estimated radiogenic fatal cancers ) and cost implications of using one or the other programme . 
in the first screening programme , children were examined for scoliosis directly by an orthopaedic specialist , whereas in the other two - step method children were first screened by a specially trained school physician and then referred to a specialist only if scoliosis was suspected or if the school physician was uncertain both programmes , it was only the orthopaedist who requested x - ray examinations . 
sono quasi 50 anni che questi programmi vengono applicati negli stati uniti ed in tutto il mondo e molti articoli della letteratura hanno dimostrato i loro effetti benefici [ 16 ] , in primo luogo , la riduzione del numero di stabilizzazioni vertebrali [ 711 ]  . 
tuttavia , alcuni epidemiologi ed amministratori pubblici hanno puntato la loro attenzione sulla crescente difficolt , da parte del servizio sanitario nazionale , ad affrontare i costi degli esami radiografici previsti da questi programmi di screening [ 4 , 5 ]  . 
inoltre , bisogna considerare la particolare radio - sensibilit dei bambini al danno da radiazioni : oggi , i pi importanti enti internazionali di radioprotezione concordano sul fatto che lincidenza dei tumori maligni radio - indotti nei bambini sia due o tre volte superiore a quella degli adulti [ 1215 ]  . 
per questo motivo , abbiamo analizzato tutti i dati raccolti in due differenti programmi di screening scolastico gi effettuati , al fine di stabilire se tra i due programmi ci sia stata una differenza significativa nella dose di radiazione totale collettiva . inoltre , abbiamo considerato la salute ( in termini di stima di tumori maligni radio - indotti ) e le implicazioni economiche derivanti dallutilizzo di uno o dellaltro programma di screening . 
nel primo programma , lo screening stato effettuato direttamente da un ortopedico ; mentre nel secondo programma , che definiremo a due tappe , i bambini sono stati esaminati in prima battuta da un medico scolastico gi istruito sulla semeiotica clinica della scoliosi e quindi , in caso di dubbi o di sospetta 240 radiol med ( 2010 ) 115 : 238245 scoliosi , inviati allortopedico . 
 materiali e metodi negli anni 20062007 , abbiamo analizzato i risultati di uno screening per scoliosi idiopatica effettuato su 8995 bambini ( 4202 ragazzi , 4793 ragazze ; range det , 914 anni ; et media , 12 , 4 anni ) che frequentavano le scuole del xix municipio di roma ( 190864 abitanti )  . 
nei bambini del gruppo a ( 5731 bambini ) , la prima valutazione clinica stata effettuata dal medico scolastico istruito in precedenza da un ortopedico su come riconoscere alcuni segni fondamentali di scoliosi . 
in particolare , il questionario presentava due schemi , rispettivamente in visione postero - anteriore e latero - laterale , per riportare anomalie di curvatura del rachide ed un terzo schema che riguardava il test di antero - flessione di adams . 
durante il test , il bambino si flette in avanti a piedi uniti , ginocchia estese e braccia pendenti ; qualunque asimmetria della gabbia toracica o altre deformit lungo il rachide possono essere segno di scoliosi . 
lo screening sui bambini del gruppo b ( 3264 bambini ) stato effettuato direttamente da un ortopedico . per entrambi i gruppi , lortopedico ha accertato la reale esistenza di scoliosi con lesecuzione di un esame radiografico ed ha rinviato ad un controllo a sei mesi i casi ancora dubbi . 
dei 5731 bambini visitati dal medico scolastico , 5433 sono stati considerati esenti da scoliosi e 298 sono stati inviati allortopedico ; questultimo ha richiesto lesame radiografico per 86 di essi ed un ulteriore screening a sei mesi per i restanti 212 . 
 tutti gli esami radiografici sono stati eseguiti in ortostatismo , nelle proiezioni antero - posteriore ( ap ) e latero - laterale ( ll ) , il campo di esposizione ha compreso lintera fig . 
i primi due schemi , rispettivamente in visione posteroanteriore e laterale , sono stati utilizzati per individuare curvature rachidee abnormi ; il terzo schema si riferisce al test di adams di flessione in avanti . material and methods the results of screening for idiopathic scoliosis on 8 , 995 children ( 4 , 202 boys , 4 , 793 girls ; age range 914 ; mean age 12.4 ) attending the schools of the xix district of rome ( 190 , 864 inhabitants ) between the years 2006 and 2007 were examined . 
children in group a ( 5 , 731 ) had received a first clinical examination by a local school physician previously instructed by an orthopaedist on how to correctly observe some simple fundamental signs . 
in radiol med ( 2010 ) 115 : 238245 particular , this questionnaire included two diagrams in posteroanterior and lateral view , respectively , to depict spinal curvatures abnormalities , and one diagram regarding the adams forward bend test . 
the forward bend test is used most often in schools and doctors offices to screen for scoliosis . during the test , the child bends forward with the feet together and knees straight while dangling the arms . 
it should be noted that this is a simple screening test that can detect potential problems but cannot determine accurately the exact severity of the deformity . suspected or doubtful cases were referred by the physician to the orthopaedist . 
for both the first and second groups , the orthopaedist ascertained by x - ray examination the suspected scoliosis and deferred the still doubtful cases to a 6 - month screening . 
out of 5 , 731 children of group a examined by school physicians , 5 , 433 were considered negative for scoliosis and 298 referred to the orthopaedist , who requested x - ray ascertainment for 86 of them and a 6 - month screening for the remaining 212 . 
2. all x - ray examinations were performed in anteriorposterior ( ap ) and lateral views in standing position , the field of exposure encompassed the whole spine and the focus - film distance was 200 cm using linear , nonmovable antiscatter grids ( 60 lines for centimetre , ratio 10 : 1 )  . 
the dose to the patient is usually reported as entrance surface dose ( esd ) in radiology , but for the assessment of stochastic risk , the effective dose ( ed ) is needed . 
in case of 10 year old children , the risk has to be multiplied by 2.5 for boys and 3.2 for girls according to annex c of the icrp report [ 12 ]  . to calculate the economic burden to the national health care system of the x - rays performed , we assumed the current reimbursement to hospitals by the national health service , which is 35 euro for each x - ray examination . statistical significance of the differences was assessed by the z - test for proportions . colonna vertebrale , la distanza fuoco - film stata di 200 cm e sono state utilizzate griglie anti - diffusione , fisse , lineari ( 60 linee per centimetro , rapporto 10 : 1 )  . 
 [ 16 ] hanno recentemente calcolato la dose e per due diverse procedure radiografiche : la teleradiografia con griglia e la radiografia digitale con tecnica air gap . per i nostri calcoli , ci siamo rifatti ai valori che questi autori hanno fornito per una et di 713 anni ; per esempio , per una teleradiografia con griglia in proiezione ap : dose e = 0 , 65 msv ( ragazzi ) e dose e = 1 , 21 msv ( ragazze ) ; per la proiezione ll : dose e = 0 , 98 msv ( ragazzi ) e dose e = 1 , 2 msv ( ragazze )  . per definire lattribuibile rischio di mortalit per cancro abbiamo seguito la pubblicazione 60 della commissione internazionale di radioprotezione ( icrp 60 ) [ 12 ] che , negli adulti , indica un coefficiente di probabilit medio nominale di 510 - 2 sv - 1 ( cio , 50 per milioni per 1 msv , 1 : 20000 )  . 
nel caso di bambini di 10 anni det , il rischio deve essere moltiplicato per 2 , 5 se ragazzi e per 3 , 2 se ragazze , in accordo con lallegato c del rapporto icrp [ 12 ]  . 
 infine , per calcolare il peso economico , per il servizio sanitario nazionale , relativo agli esami radiografici eseguiti , ci siamo riferiti al rimborso che gli ospedali ricevono dal servizio sanitario nazionale che di euro 35 per ogni esame radiografico . 
per la significativit statistica delle variabili stato utilizzato lo z test per le proporzioni . risultati nel gruppo a ( il gruppo esaminato con programma a due tappe medico scolastico - ortopedico ) , sono stati eseguiti 86 esami radiografici su 5731 bambini ( 1 , 5% ) , mentre nel gruppo b ( il gruppo esaminato direttamente da un ortopedico ) , ne sono stati eseguiti 95 su 3266 bambini ( 2 , 91% )  . 
la differenza altamente significativa ( z = 4 , 452 , p < 0 , 001 )  . pertanto , il programma a due tappe , utilizzato per esaminare i bambini del gruppo a , ha portato ad una sensibile riduzione dellesposizione a radiazioni . 
il rischio doppio per le ragazze , essendo di 7 , 712 ( 2 , 413 , 2 ) / 20000 ( cio , 1 / 2600 ) ; circa quattro morti ogni 10000 ragazze esaminate . 
 estrapolando questi dati ad uno screening su 10000 bambini , usando il programma ad una tappa ( lortopedico esamina direttamente i bambini ) , verrebbero richiesti 291 esami programma a due tappe , per lo stesso numero di bambini ( 2 , 91% ) , mentre utilizzando radiografici 242 radiol med ( 2010 ) 115 : 238245 fig . 
therefore , the two - step procedure used in examining the children of group a leads to a remarkable verrebbero richiesti soltanto 150 esami radiografici ( 1 , 5% )  . questo comporterebbe una dose collettiva di 0 , 283 sv e , per il servizio sanitario nazionale , un risparmio in costi per esami radiografici di euro 35141euro = 4935 euro . 
 dal momento che il programma a due tappe comporta lesecuzione di un numero di esami radiografici che circa la met di quello che comporta il programma ad una tappa ( 141 vs 291 ) , anche il numero stimato di corrispondenti tumori radio - indotti sarebbe dimezzato . 
this would constitute a 0.283 sv of collective dose and a saving in xray costs to the national health care system of 35141 euro = 4 , 935 euro . as the two - step procedure results in essentially half the number of x - ray exams when compared with the one - step procedure ( 141 compared with 291 ) , the estimated number of related malignant radiogenic tumours would also be halved . 
 discussion scoliosis is a disease that affects the three - dimensional shape of the spine , which may occur at any stage of life but generally arises by age ten . 
although consensus recommendations for population screening , evaluation , and treatment of this disorder by medical organisations vary widely , schoolbased scoliosis screening programmes remain well established [ 3 , 4 , 17 ]  . 
 our results show that the two - step school - based scoliosis screening procedure not only has practical advantages and is less expensive , but also halves the exposure to ionising radiation . 
however , a question arises about diagnostic efficiency : would diagnostic efficiency be improved if all children were directly examined by an orthopaedic specialist ? based on our data , it appears that the first - step filtering of cases by school physicians does not impair specificity . 
as it is known , specificity is the most important characteristic for a screening test when the prevalence of the disease is low . however , an impairment of sensitivity is likely . 
it can thus be suspected that the probability of a false negative result is higher and therefore the sensitivity lower , for discussione la scoliosi una condizione patologica che altera la conformazione tridimensionale del rachide ; generalmente , insorge entro i primi dieci anni di vita anche se pu comparire a qualunque et . 
il suo riconoscimento dovrebbe spettare a tutti coloro che hanno in custodia gli alunni ( pediatri ed insegnanti , in particolare , quelli di educazione fisica )  . sebbene siano molto variabili le raccomandazioni alla popolazione , relative allo screening , diagnosi e trattamento di questa affezione , da parte delle diverse organizzazioni sanitarie , esiste invece un consenso unanime sulla necessit dello screening scolastico della scoliosi [ 3 , 4 , 17 ]  . 
nonostante ci , ci si pu porre la seguente domanda : lefficienza diagnostica migliorerebbe se tutti i bambini fossero esaminati direttamente dallortopedico ? dai nostri dati risulta che la prima tappa dello screening , il filtro effettuato dal medico scolastico , non riduce la specificit . 
dei 181 bambini ai quali stato richiesto un esame radiografico , per via di un sospetto clinico di scoliosi , soltanto 4 sono risultati falsi positivi ; pertanto , la specificit stata del 97 , 8% . 
 i medici scolastici hanno dichiarato negativo il 94% dei bambini esaminati , gli ortopedici l86% : la differenza altamente significativa ( p = 0 , 001 ) considerando lentit del nostro campione . 
pertanto , per i bambini visitati dal medico scolastico piuttosto che dallortopedico si pu sospettare che la probabilit di un risultato falso negativo sia pi alta e quindi , la sensibilit pi bassa . 
se assumiamo che lesperienza dellortopedico porti ad una corretta esclusione della scoliosi , ne deriva che il medico scolastico perde circa l8% dei casi di scoliosi ( probabilmente forme iniziali o lievi ) che meriterebbero un controllo radiografico o per lo meno un successivo ulteriore screening . 
questo un problema persistente di cui dobbiamo sempre tener conto quando consideriamo gli altri vantaggi dello screening scolastico a due tappe . tuttavia , noi siamo dellidea che i risultati falsi negativi potrebbero essere ridotti con una migliore istruzione dei medici scolastici e con lintroduzione di uno screening clinico annuale . 
if we assume that the experience of the specialist leads to the correct exclusion of scoliosis , it follows that the school physician misses about 8% of cases ( probably mild or initial scoliosis ) that would deserve radiography or at least further screening . 
the risk estimates given here are in keeping not only with icrp 60 , but also with the recent biological effects of ionizing radiation ( beir ) vii report [ 13 ] ( see tables in annex 12d of the report [ 13 ] )  . 
a large body of recent radiobiological research emphasises the possibility of previously unknown dangerous effects that could enhance the damage induced by low - dose ionising radiation [ 1821 ]  . 
morgan [ 18 , 19 ] summarised the evidence for nontargeted and delayed effects of exposure to ionising radiation in vivo , such as the so - called bystander effect , genomic instability , radiation hypersensitivity , clastogenic factors and transgenerational effects . 
the icrp 1991 report estimated as 85 the number of excess cases of fatal lung tumours in 100 , 000 individuals ( all ages ) exposed to 0.1 sv ( 100 msv )  . 
similarly , estimates of excess cases of breast cancer due to equivalent radiation exposures have grown from 20 in the icrp 60 report [ 12 ] to 43 cases in the unscear report of 2000 [ 15 ]  . 
 all this emphasises the particular importance of radiation safety in the screening of scoliosis : the exposure of children during such screening should be reduced as much as possible . the two - step school - based scoliosis screening procedure could be a collective mean to do so . 
un dogma delle scienze radio - biologiche che lenergia da radiazioni debba depositarsi nel nucleo cellulare per esercitare un effetto biologico [ 21 ] ; ebbene , stato descritto un certo numero di effetti tardivi e non targeted delle radiazioni ionizzanti che andrebbero contro questo dogma [ 18 , 19 ]  . morgan [ 18 , 19 ] ha riassunto tutte le prove esistenti circa gli effetti tardivi e non targeted dellesposizione in vivo a radiazioni effetto come bystander , linstabilit genomica , lipersensibilit alle radiazioni , i fattori clastogenici e gli effetti trans - generazionali . 
leffetto bystander , osservato in diversi laboratori internazionali in colture in vitro di cellule o tessuti , consiste nella capacit delle cellule irraggiate di trasmettere segnali tali da indurre effetti anche in cellule non direttamente esposte a radiazioni ionizzanti . 
il rapporto icrp del 1991 ha calcolato in 85 il numero di tumori polmonari maligni su 100000 individui ( di tutte le et ) esposti a 0 , 1 sv ( 100 msv )  . 
allo stesso modo , le stime dei casi di cancro mammario dovuti ad una esposizione equivalente di radiazioni sono cresciute da 20 , nel rapporto 60 dellicrp [ 12 ] , a 43 casi nel rapporto del 2000 del unscear [ 15 ]  . 
therefore , we recommend girls in particular to be carefully examined and , in case of doubt , further controlled 6 months or 1 year later . in conclusion the comparison of the two methodologies indicates that the two - step procedure , while significantly saving on orthopaedic specialists visits , is easily performed and diagnostically reliable , on the condition that the school physicians performing the initial screening are sufficiently trained . 
if performed at adequate intervals , the two - step method can both reduce initial screening costs to the national health system and the net social economic burden , but its main advantage is that it reduces radiation exposure , which is particularly important in children . media di sette per ogni paziente , come riportato da hansen et al . 
pertanto , raccomandiamo di esaminare con particolare attenzione le ragazze e , in caso di dubbio , riesaminarle dopo 6 mesi o 1 anno . in conclusione , la valutazione comparativa dei due programmi indica che la procedura a due tappe , oltre a ridurre notevolmente il numero di visite specialistiche ortopediche , facile da eseguire ed affidabile dal punto di vista diagnostico , a condizione che i medici scolastici che effettuano il primo screening acquisiscano una competenza sufficiente . 
gandini istituto di radiologia diagnostica ed interventistica , universit di torino , aso san giovanni battista di torino , sede molinette , via genova 3 , 10126 torino correspondence to : a . 
this study was conducted to evaluate the diagnostic accuracy of axillary ultrasound ( us ) alone or in combination with fine - needle - aspiration cytology ( fnac ) in patients with breast carcinoma , in comparison with the final histological examination ( sentinel node biopsy and / or axillary dissection )  . 
lecografia del cavo ascellare associata alla fnac nel 48 , 3% dei casi ha permesso di evitare la biopsia del linfonodo sentinella , orientando il trattamento chirurgico verso una dissezione ascellare immediata , con sensibile riduzione dei costi e del tempo di ospedalizzazione . 
 parole chiave carcinoma mammario cavo ascellare linfonodi ecografia 226 introduction breast cancer prognosis is heavily dependent on the presence or absence of lymph node metastases at presentation [ 1 ]  . 
the study of axillary lymph nodes is aimed at detecting metastases and avoiding two - step axillary surgery by guiding treatment towards immediate axillary dissection that is , not preceded by sentinel node biopsy in the case of positive findings . in recent years , numerous studies have assessed the role of us in the study of the axilla in an attempt to establish pathognomonic morphostructural criteria that could distinguish metastatic nodes from reactive ones ( reactive hyperplasia , inflammation ) [ 126 ]  . 
to correctly stage axillary lymph nodes , us has been combined with us - guided fineneedle - aspiration cytology ( fnac ) [ 1 , 2 , 14 , 1623 ] or core biopsy , although the latter , which is more invasive than fnac , is not widely used [ 7 , 8 , 15 , 2426 ]  . the purpose of this study was to evaluate the diagnostic accuracy of axillary us and the adjunctive role of nodal fnac in the diagnostic workup of patients with breast carcinoma in comparison with final histology of axillary lymph nodes ( sentinel node biopsy and / or axillary dissection )  . materials and methods between january 2005 and june 2008 , 427 patients with breast carcinoma scheduled for surgical excision of a primary cancer and axillary surgery ( sentinel node biopsy and / or axillary dissection ) were studied with axillary us . us scans were carried out with dedicated equipment ( technos 700 c or my lab 25 cv , esaote , genoa , italy ) and a 7.5to 12mhz probe ; all us studies were supplemented by colour and power doppler imaging . 
us findings were classified on the basis of commonly reported criteria [ 19 ] : hilar and cortical morphology , ratio between longitudinal ( l ) and transverse ( t ) diameter and ratio between hilar ( h ) and l diameter of lymph nodes . 
fnac results were classiradiol med ( 2010 ) 115 : 225237 introduzione la prognosi , in pazienti affette da carcinoma mammario , fortemente condizionata dalla presenza o meno di metastasi linfonodali al momento della diagnosi [ 1 ]  . 
lo studio ecografico del cavo ascellare , metodica non invasiva , pu contribuire ad una corretta stadiazione pre - operatoria e quindi ad una migliore pianificazione terapeutica , assicurando una migliore compliance della paziente e una riduzione dei tempi e dei costi di gestione . 
infatti , lobiettivo dello studio linfonodale la ricerca delleventuale presenza di metastasi , al fine di evitare la chirurgia del cavo ascellare in due tempi , orientando , in caso di riscontro di positivit , verso una dissezione ascellare immediata , cio non preceduta da biopsia del linfonodo sentinella ( ls )  . negli ultimi anni , numerosi lavori hanno valutato il ruolo dellecografia nello studio del cavo ascellare , cercando di stabilire dei criteri morfostrutturali patognomonici di compromissione metastatica dei linfonodi , al fine di differenziarli da quelli reattivi ( iperplasia reattiva , flogosi ) [ 126 ]  . 
per la corretta stadiazione dei linfonodi ascellari , sono stati inoltre associati allesame ecografico lutilizzo dellagoaspirato linfonodale ecoguidato con ago sottile ( fnac ) [ 1 , 2 , 14 , 1623 ] o la core biopsy . questultima metodica , pi invasiva rispetto alla fnac , non ancora utilizzata su larga scala [ 7 , 8 , 15 , 2426 ]  . scopo del presente lavoro stato quello di valutare , in pazienti affette da neoplasia mammaria , sia laccuratezza diagnostica dellecografia del cavo ascellare , sia il ruolo aggiuntivo che il prelievo linfonodale mediante fnac svolge nel percorso diagnostico , assumendo come parametro di confronto lesame istologico definitivo dei linfonodi ascellari ( biopsia del linfonodo sentinella e / o dissezione ascellare )  . materiali e metodi nel periodo tra gennaio 2005 e giugno 2008 stato eseguito lo studio ecografico del cavo ascellare in 427 pazienti affette da neoplasia mammaria e candidate ad intervento chirurgico di exeresi della neoplasia primitiva e a chirurgia del cavo ascellare ( biopsia del linfonodo sentinella e / o dissezione ascellare )  . 
lesame ultrasonografico stato eseguito in tutte le pazienti con apparecchiatura dedicata ( technos 700 c oppure my lab 25 cv , esaote , genova , italia ) con sonda da 7 , 512 mhz e completato con studio color / power doppler . 
per la classificazione dei reperti ecografici sono stati utilizzati i parametri pi frequentemente riportati in letteratura [ 19 ] : la morfologia dellilo e della corticale , il rapporto tra diametro longitudinale ( l ) e trasversale ( t ) e il rapporto tra il diametro della regione ilare ( h ) e l del linfonodo . 
sono stati considerati radiol med ( 2010 ) 115 : 225237 table 1 ultrasound ( us ) classification of axillary lymph nodes us parameters normal probably benign suspicious for malignancy probably malignant l / t ratio h / l ratio cortical thickness ( mm ) morphology hilum 50% oval shape clearly visible 50% oval shape clearly visible < 50% rounder shape not completely visible < 2 < 50% > 2 globular shape absent l / t , longitudinal and transverse ratio ; h / l , hilar and longitudinal ratio tabella 1 classificazione ecografica dei linfonodi parametri ecografici normale verosimilmente benigno sospetto per malignit verosimilmente maligno rapporto l / t rapporto h / l spessore corticale ( mm ) morfologia 50% ovalare ben visibile 50% ovalare ben visibile < 50% rotondeggiante poco visibile < 50% globosa assente l / t , diametro linfonodale longitudinale e trasversale ; h / l , diametro della regione ilare longitudinale linfonodale fied in accordance with the european guidelines [ 27 ] into five categories : c1 = inadequate , c2 = negative , c3 = equivocal probably benign , c4 = suspicious of malignancy , c5 = malignant . 
all patients with a breast mass > 3 cm or with positive lymph node cytology proceeded directly to axillary dissection ; patients with a mass 3 cm with negative or equivocal cytology were referred for sentinel node biopsy after localisation with radioactive tracer ( tc - 99 - m sestamibi ) or vital dye ( patent blue in harmless doses ) injection into the peritumoural area . 
 diagnostic accuracy , sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) of axillary us and us - guided fnac in assessing the presence of nodal metastases were established comparing the results with final histology of sentinel node biopsy and / or axillary dissection . 
all normali valori di l / t2 , di h / l50% e di spessore della corticale 2 msulla base di questi parametri , abbiamo classificato i reperti in quattro categorie : linfonodo normale , verosimilmente benigno ( indeterminato ) , sospetto per malignit o verosimilmente maligno ( tabella 1 )  . 
lesame citologico su agoaspirato stato classificato in 5 categorie : c1 = inadeguato , c2 = negativo , c3 = dubbio ( lesione probabilmente benigna ) , c4 = sospetto di malignit , c5 = positivo , in accordo con le linee guida europee [ 27 ]  . 
il materiale prelevato per lesame citologico stato sottoposto ad osservazione estemporanea ( striscio su vetrino , fissazione in metanolo e colorazione con ematossilina - eosina ) da parte dellanatomo - patologo per valutarne lidoneit . 
tutte le pazienti con neoplasia mammaria > 3 cm o con citologia linfonodale positiva sono state sottoposte direttamente a dissezione ascellare ; le pazienti con neoplasia3 cm con citologia negativa o dubbia sono state inviate a biopsia del linfonodo sentinella previa localizzazione mediante iniezione nella zona peri - tumorale di un tracciante radioattivo ( tc - 99 - m sestamibi ) o di un colorante vitale ( patent blue in dosi assolutamente prive di qualsiasi effetto nocivo )  . laccuratezza diagnostica , la sensibilit , la specificit , il valore predittivo positivo ( vpp ) e il valore predittivo negativo ( vpn ) della valutazione ultrasonografica dei linfonodi ascellari e della fnac ecoguidata per la presenza di metastasi linfonodali sono stati confrontati con i reperti istologici definitivi della biopsia del linfonodo sentinella e / o della 228 radiol med ( 2010 ) 115 : 225237 patients underwent surgery : 63.7% of cancers ( 272 / 427 ) were t1 ( t1a in nine patients ; t1b in 74 ; t1c in 189 ) , and 27.9% ( 119 / 427 ) were t2 , whereas only a small number of patients had t3t4 ( 2.3% , 10 / 427 ) cancers at final histology . the most common histological type of invasive tumour was invasive ductal carcinoma ( idc ) [ 71.3% ( 286 / 401 ) ] , followed by invasive lobular carcinoma ( ilc ) in 10.5% of cases ( 42 / 401 ) , mixed ductal - lobular carcinoma in 4.5% ( 18 / 401 ) and other histological types ( apocrine , tubular , mucinous , cribriform , inverted micropapillary , neuroendocrine , medullar carcinoma ) in the remaining 13.7% ( 55 / 401 )  . 
histological nuclear grading of infiltrating tumours according to elston and ellis [ 28 ] was low ( g1 ) in 24.2% , intermediate ( g2 ) in 42.8% and high ( g3 ) in 33% of cases . 
 concordance of us , us - guided fnac and final histological result preoperative axillary node us was negative for nodal abnormalities in 203 / 427 cases and positive for one or more us criteria in 224 / 427 cases ( table 2 )  . 
in 203 / 427 patients with normal us findings ( l / t 2 and cortical thickness 2 mm ) , fnac was not performed , and final histology ( sentinel node biopsy and / or axillary dissection ) confirmed the negative us findings in 87.2% of cases ( 177 / 203 )  . 
le valutazioni statistiche relative allaccuratezza della fnac sono state eseguite escludendo dai calcoli i campioni inadeguati ( c1 ) e considerando gli esami citologici su agoaspirato c2 - c3 come negativi e c4c5 come positivi . risultati caratteristiche istologiche delle neoplasie mammarie delle 427 pazienti ( et media 60 , 9 anni , range 2681 anni ) , 401 ( 93 , 9% ) erano affette da carcinoma mammario infiltrante con un diametro medio di 1 , 88 cm ( deviazione standard [ sd ] = 1 , 2 cm ) , mentre 26 ( 6 , 1% ) da carcinoma in situ ( tis ) [ diametro medio di 2 , 77 cm ( sd = 1 , 28 cm ) ]  . 
tutte le pazienti sono state sottoposte ad intervento chirurgico e allistologico definitivo il 63 , 7% delle neoplasie ( 272 / 427 ) risultato t1 ( t1a in 9 pazienti ; t1b in 74 ; t1c in 189 ) , il 27 , 9% ( 119 / 427 ) t2 e solo un numero ristretto t3 - t4 ( 2 , 3% , 10 / 427 )  . 
 listotipo prevalente nei casi di neoplasia infiltrante stato il carcinoma duttale infiltrante ( cdi ) ( 71 , 3% , 286 / 401 ) , seguito da quello lobulare ( cli ) nel 10 , 5% dei casi ( 42 / 401 ) , dalla forma mista duttale e lobulare nel 4 , 5% ( 18 / 401 ) e nel restante 13 , 7% ( 55 / 401 ) da altri tipi istologici ( apocrino , tubulare , mucinoso , cribriforme , micropapillare invertito , neuroendocrino , midollare )  . 
il grading nucleare istologico dei tumori infiltranti secondo elstonellis [ 28 ] risultato : basso - g1 nel 24 , 2% , intermedio - g2 nel 42 , 8% e alto - g3 nel 33% . 
tra i carcinomi in situ listotipo prevalente risultato essere il carcinoma duttale in situ ( cdis ) in 21 casi , comedonico in 3 casi , un cribriforme e un papillare . 
among 55 / 84 lymph nodes studied with fnac , 39 were c2 , one was c3 and three were c5 , resulting in 88.4% concordance with definitive histology ( 38 / 43 )  . 
in 140 / 224 cases in which lymph nodes exhibited echostructural alterations classified as suspicious for malignancy ( l / t < 2 , cortical thickening > 2mm , a more rounded shape , partially visible hilum ) or probably malignant ( l / t < 2 , cortical thickening > 2mm , globular shape , invisible hilum ) , the definitive histological examination confirmed the presence of nodal metastases in 87.9% of cases ( figs 2 , 3a , b )  . 
fnac was performed on 92 / 140 nodes ( 18 c2 , one c4 , 67 c5 ) , with a concordance between cytology and final histology of 95.3% ( 82 / 86 )  . 
in six cases , cytology was not diagnostic ( c1 ) owing to inadequate sampling ( tables 2 and 3 )  . with regard to the correlation between l / t ratio of the lymph node and final histology , out of the 287 / 427 lymph nodes with l / t2 ( index of probably benign node ) , 240 concordanza tra ecografia , fnac ecoguidata e risultato istologico definitivo lesame ecografico del cavo ascellare eseguito prima dellintervento chirurgico risultato negativo per alterazioni linfonodali in 203 / 427 casi e positivo per alterazioni di uno o pi parametri ecografici in 224 / 427 casi ( tabella 2 )  . 
nelle 203 / 427 pazienti con reperto ecografico normale ( con rapporto l / t2 e spessore della corticale2 mm ) non stata eseguita fnac : lesame istologico definitivo ( ls e / o dissezione ascellare ) ha confermato la negativit ecografica nell87 , 2% dei casi ( 177 / 203 )  . 
3a lymph node with irregular echostructure : l = 1.3 cm , t = 1.2 cm , rounded shape ( l / t = 1 ) , and no clearly visible hiluprobably malignant . b axillary us - fnac : tumour cells ( c5 )  . 
b us - fnac linfonodale con ago da 22 g : cellule tumorali ( c5 )  . istologico definitivo : presenza di metastasi linfonodali di carcinoma duttale infiltrante ( diametro = 2 , 6 cm ) ( dissezione ascellare : 4 / 18 , n + )  . were found to be free of metastasis on axillary surgery , with a specificity of 83.6% ( 240 / 287 )  . 
nei 55 / 84 casi in cui stata eseguita fnac si sono ottenuti 39 c2 , 1 c3 , 3 c5 , con una concordanza con listologia definitiva pari all88 , 4% ( 38 / 43 )  . 
tra questi , 92 / 140 sono stati sottoposti a fnac ( di cui 18 c2 , 1 c4 e 67 c5 ) con una concordanza tra citologia e istologia definitiva del 95 , 3% ( 82 / 86 )  . 
in 6 casi la citologia risultata non diagnostica ( c1 ) per lesiguit del materiale prelevato ( tabelle 2 e 3 )  . considerando la correlazione tra il rapporto l / t del linfonodo e lesame istologico definitivo , dei 287 / 427 linfonodi esaminati con un rapporto l / t2 ( indice di probabile benignit linfonodale ) 240 sono risultati indenni da metastasi alla chirurgia del cavo ascellare , con una specificit dell83 , 6% ( 240 / 287 )  . 
dei 140 / 427 linfonodi con un rapporto l / t < 2 ( indice di probabile malignit linfonodale ) listologico definitivo ha confermato la presenza di metastasi in 123 / 140 casi con una sensibilit dell87 , 9% ( tabelle 4 e 5 )  . laccuratezza complessiva tra esame ultrasonografico del cavo ascellare e istologico definitivo risultata pari all85% ( 363 / 427 ) , la sensibilit del 72 , 3% ( con il 27 , 7% di falsi negativi ecografici ) e la specificit del 93 , 4% . 
laccuratezza diagnostica tra fnac del cavo ascellare e istologico definitivo risultata del 93% ( 120 / 129 ) , la sensibilit dell88 , 8% e la specificit del 100% ( valori calcolati escludendo i c1 ) ( tabella 6 )  . 
complessivamente lecografia associata alla fnac ha modificato lorientamento chirurgico del cavo ascellare in 71 / 147 donne ( 70 c5 e 1 c4 , 48 , 3% ) , che sono state sottoposte direttamente a dissezione del cavo ascellare evitando la biopsia del linfonodo sentinella . i campioni inadeguati ( c1 ) sono risultati 18 sul totale delle 147 pazienti sottoposte a fnac ( 12 , 2% )  . 
nella maggior parte ( 12 / 18 ) lagoaspirato stato eseguito su linfonodi a basso sospetto ( verosimilmente benigni ) ; lesame istologico definitivo ha confermato la benignit in 8 / 12 casi , mentre i restanti 4 sono risultati positivi per metastatizzazione . 
in questottica , limpiego ormai consolidato , soprattutto per le lesioni infracliniche , di sistemi bioptici mini - invasivi , quali la vacuum assisted core biopsy ( vacb ) , sia con guida stereotassica [ 2931 ] e , sebbene pi limitatamente , con guida rm [ 32 , 33 ] , stanno consentendo una pi corretta pianificazione chirurgico - terapeutica , ampliando le possibilit in fase pre - operatoria dellimaging senologico . 
in most cases ( 12 / 18 ) fnac was performed on probably benign lymph nodes ; the final histological examination confirmed benignity in 8 / 12 cases , whereas the remaining four were positive for metastasis . 
in most of these cases ( 4 / 6 ) , final histology confirmed the malignancy suspected at us , whereas only two were found to be free of metastases . discussion optimisation of the diagnostic workup in locoregional staging of breast carcinoma is an important goal of breast diagnostics . 
in this context , the consolidated use especially in subclinical lesions of minimally invasive biopsy systems such as vacuum - assisted core biopsy ( vacb ) , whether stereotactically guided [ 2931 ] or , more rarely , magnetic resonance imaging ( mri ) guided [ 32 , 33 ] , are improving treatment planning by extending the possibilities of preoperative breast imaging . 
correct preoperative staging of breast carcinoma , however , requires evaluation of axillary lymph node metastasis , as spread to the axillary nodes heavily impacts the prognosis of breast cancer patients . in the us study of the axilla , the most significant criteria for detecting the presence of lymph node metastases are alteration of the ratio between longitudinal and transverse diameter , asymmetrical or focal cortical thickening and poor hilar visibility , as reported by numerous studies [ 126 ]  . 
other criteria , such as changes in size , are not sufficiently specific to distinguish between presence and absence of malignancy , given that lymph nodes may also be enlarged as a result of trasversale , lispessimento asimmetrico o focale della corticale e la mancata riconoscibilit della regione ilare , come gi evidenziato in un significativo numero di lavori [ 126 ]  . altri parametri , quali le variazioni di dimensioni , non rappresentano invece un criterio specifico per la differenziazione fra la presenza o meno di patologia maligna . infatti , i linfonodi possono essere ingranditi anche a seguito di processi infiammatori o di malattie sistemiche e , per contro , talvolta i linfonodi metastatici possono avere dimensioni inferiori al centimetro . 
i linfonodi di tipo reattivo , di frequente riscontro nel cavo ascellare , dal punto di vista ultrasonografico si presentano come strutture ovalari o reniformi di dimensioni generalmente superiori al centimetro ( anche fino a 2 , 5 cm ) , con ilo iperecogeno ben evidente . 
infatti , un prolungato stimolo patogeno pu determinare un aumento numerico dei sinusoidi dei vasi linfatici del seno linfonodale , accentuando levidenza dellilo iperecogeno [ 2 , 3 ]  . a differenza di quanto accade nei linfonodi reattivi , nei linfonodi metastatici il processo interessa prevalentemente la sede sub - corticale e corticale in toto ; perci la corticale , invasa dal tessuto neoplastico , si ipertrofizza in modo non omogeneo , deformando o cancellando liperecogenicit dellilo e pertanto i sinusoidi linfatici [ 3 ]  . 
lispessimento della corticale oltre i 2 mm ( diffuso , focale o eccentrico ) , la progressiva alterazione ecostrutturale del linfonodo fino allipoecogenicit e lilo poco o per nulla visibile sono importanti criteri per la diagnosi di metastasi linfonodali . il rapporto fra diametro l e t del linfonodo tendente allunit , definito roundness index da sakai et al . 
in accordo con quanto riportato in letteratura , anche nella nostra esperienza il rapporto l / t ( usando come soglia 2 ) ha dimostrato un elevato valore radiol med ( 2010 ) 115 : 225237 inflammatory processes or systemic disease , and metastatic lymph nodes may also be smaller than 1 cm in size . 
reactive lymph nodes , a frequent finding in the axilla , appear on us as either oval or reniform structures usually larger than 1 cm ( up to 2.5 cm ) and with a clearly visible hyperechoic hiluin fact , a prolonged pathogenic process may lead to an increased number of lymphatic sinusoids , heightening the conspicuity of the hyperechoic hilum [ 2 , 3 ]  . conversely , in metastatic lymph nodes , the process mainly involves the entire subcortical or cortical region , which , being invaded by the neoplastic tissue becomes inhomogeneously hypertrophic , deforming or cancelling the hyperechogenicity of the hilum and the lymphatic sinusoids [ 3 ]  . 
cortical thickening > 2 mm ( diffuse , focal , eccentric ) , progressive echostructural changes in the lymph node up to hypoechogenicity and poorly visible or invisible hilum are all important criteria for the diagnosis of lymph node metastases . 
in agreement with the literature , we found the l / t ratio ( considering a value of 2 as the threshold ) to have high npv ( 93.4% ) and a lower ppv ( 72.3% ) , probably because , as emphasised by feu et al . [ 6 ] and balu - maestro et al . 
on the other hand , metastatic lymph nodes > 2 cm may maintain an oval shape . in most published studies , lymph nodes are classified based on the above criteria into two categories only : normal or suspicious [ 2 , 726 ]  . 
considering all of the morphostructural alterations of axillary lymph nodes , in assessing the accuracy of us alone we proposed a classification of sonographic findings into four categories ( normal , probably benign , suspicious for malignancy , probably malignant ) in line with the breast imaging reporting and data system ( bi - rads ) classification . 
overall diagnostic accuracy of us was 85% and specificity was 93.4 % , whereas sensitivity was 72.3% , in keeping with the literature that reports high specificity values ( 80.4%95.2% ) and more variable sensitivity values ( 64.3%92.3% ) [ 8 , 1016 ] ( table 7 )  . 
in fact , in 27.7% of cases ( 47 / 170 false negative cases ) , negative axillary us findings were associated with positive axillary lymph nodes on final histology . 
per contro , linfonodi metastatici maggiori di 2 cm , possono mantenere una forma tendenzialmente ovale . nella maggior parte degli studi presenti in letteratura , i linfonodi sono classificati in base ai criteri precedentemente descritti in due sole categorie : normali oppure sospetti [ 2 , 726 ]  . 
considerando nellinsieme le alterazioni morfostrutturali dei linfonodi ascellari , abbiamo proposto nel nostro studio una classificazione dei reperti ecografici in quattro categorie ( linfonodo normale , verosimilmente benigno , sospetto per malignit o verosimilmente maligno ) in analogia con la classificazione breast imaging reporting and data system ( bi - rads ) , al fine di valutare laccuratezza della sola ecografia . 
complessivamente , nella nostra esperienza laccuratezza diagnostica dellecografia risultata pari all85% , la specificit 93 , 4% e la sensibilit 72 , 3% , in accordo con la letteratura , che riporta elevati valori di specificit ( 80 , 4%95 , 2% ) e pi variabili valori di sensibilit ( 64 , 3%92 , 3% ) ( tabella 7 ) [ 8 , 1016 ]  . 
infatti nel 27 , 7% ( 47 / 170 casi di cosiddetti falsi negativi ) alla negativit del quadro ultrasonografico dei cavi si associata la positivit dei linfonodi ascellari allistologico definitivo . 
 [ 7 , 8 ] , i falsi negativi allesame ecografico ( rispettivamente 27 , 3% e 22 , 8% ) risultavano nel complesso sovrapponibili a quelli del nostro studio . nella nostra esperienza , limpiego della fnac ha incrementato in tutte le categorie la concordanza tra istologia definitiva e sospetto ecografico , in particolare nella categoria intermedia ( aspetto del linfonodo verosimilmente benigno ) rispettivamente dal 75% all88 , 4% . 
sono stati esaminati i risultati della fnac sotto guida ecografica della nostra casistica e confrontati con quelli pi significativi della letteratura ( tabella 8 ) [ 1 , 2 , 14 , 1623 ]  . 
nella nostra esperienza , relativa a 147 fnac , la specificit stata del 100% , poich non ci sono stati falsi positivi . la sensibilit complessiva documentata nella nostra serie stata dell88 , 8% ( valore calcolato escludendo i c1 dallo studio ) ed risultata molto soddisfacente in rapporto ai valori riportati in letteratura ( variabili dal 57% al 94 , 9% ) , essendo inferiore solo a quella riportata in due 234 radiol med ( 2010 ) 115 : 225237 table 7 sensitivity and specificity of axillary ultrasound ( us ) : comparison with the literature data study ( year ) sensitivity ( 95% ci ) specificity ( 95% ci ) vaidya et al . 
in our experience with 147 fnac , specificity reached 100% , with no false positive cases . overall sensitivity in our series was 88.8% ( a value calculated excluding c1 cases from the analysis )  . 
 [ 1 , 17 ] , who performed significantly fewer fnac procedures ( 83 and 69 , respectively ) , it was higher than reported in nine other papers [ 2 , 14 , 16 , 1823 ]  . 
 [ 19 ] , who analysed 81 and 183 patients subjected to fnac , sensitivity was significantly lower ( 63% and 57% , respectively ) , as the authors considered subclinical lymph nodes only . the major limitation of fnac is , however , the number of inadequate or nondiagnostic samples . 
more specifically , the majority of altre casistiche [ 1 , 17 ] , con un numero di agoaspirati linfonodali decisamente inferiore ( rispettivamente 69 e 83 ) , mentre parsa pi elevata rispetto agli altri 9 lavori esaminati [ 1 , 2 , 14 , 1623 ]  . 
 [ 19 ] , relative a 81 e 183 pazienti sottoposte a fnac , la sensibilit risultata decisamente pi bassa ( rispettivamente del 63% e 57% ) poich sono stati considerati unicamente i linfonodi infraclinici . tuttavia , il maggior limite della fnac costituito dal numero di campioni inadeguati o non diagnostici , che in questo lavoro sono risultati pari al 12 , 2% ; in letteratura tale percentuale risulta compresa tra l8 , 2% e il 30% [ 16 , 22 , 23 ]  . 
in particolare , abbiamo osservato che il maggior numero di campioni inadeguati stato riscontrato nei prelievi su linfonodi ad aspetto verosimilmente benigno ( indeterminato ) ( 12 / 18 )  . 
per ovviare a questo limite , in alcuni recenti lavori stato proposto lutilizzo della core biopsy : con questa metodica stato riportato un incremento della sensibilit sino al 94% [ 7 , 8 , 15 , 2426 ]  . 
tuttavia , tale procedura non viene utilizzata su larga scala per la stadiazione dei linfonodi ascellari soprattutto perch pi invasiva rispetto allagoaspirato linfonodale ; la difficolt principale nellesecuzione della core biopsy consiste nel riuscire ad evitare di danneggiare i vasi sanguigni o i nervi , poich i linfonodi sono spesso localizzati in prossimit di queste strutture [ 25 , 26 ]  . 
pur con le limitazioni sia della metodica radiol med ( 2010 ) 115 : 225237 table 8 sensitivity and specificity of combined axillary ultrasound ( us ) and fine - needle - aspiration cytology ( fnac ) : comparison with the literature data study ( year ) sensitivity ( 95% ci ) specificity ( 95% ci ) no . 
to overcome this limitation , recent studies have proposed the use of core biopsy , a method that been shown to increase sensitivity to 94% [ 7 , 8 , 15 , 2426 ]  . 
the main difficulty in performing core biopsy lies in avoiding damage to blood vessels or nerves , given that lymph nodes are often located in the vicinity of these structures [ 25 , 26 ]  . 
despite the limitations of both us and needle biopsy , combined us and fnac in our study allowed sentinel node biopsy to be avoided in almost half of the patients ( 71 / 147 ; 48.3% ) , who were thus referred for immediate axillary dissection . our results suggest that in women with proven breast carcinoma , it may be appropriate to characterise lymph nodes with fnac whenever nodal abnormalities are detected on us , even those with probably benign appearance . 
this is because the goal of lymph node characterisation is not to rule out metastatic involvement but rather to search for signs of secondary disease to avoid two - step axillary surgery . ecografica , sia della metodica agobioptica , nel nostro studio lecografia associata a fnac ha infatti permesso di evitare la biopsia del linfonodo sentinella in quasi la met delle pazienti ( 71 / 147 , 48 , 3% ) orientando il trattamento chirurgico verso una dissezione ascellare immediata . questi risultati suggeriscono che nelle donne con diagnosi accertata di neoplasia mammaria , sembrerebbe opportuno ricorrere alla caratterizzazione dei linfonodi mediante fnac ogni qual volta si riscontrino alterazioni linfonodali , anche se pi verosimilmente orientate verso la benignit ecostrutturale . 
infatti , lobiettivo dello studio linfonodale non lesclusione dellinteressamento metastatico , bens la ricerca delleventuale positivit per secondariet , al fine di evitare la chirurgia del cavo ascellare in due tempi . conclusioni lecografia dei linfonodi del cavo ascellare un esame rapido , non invasivo , per cui dovrebbe essere eseguita di routine nelle pazienti affette da neoplasia mammaria , potendo svolgere un importante ruolo nella valutazione 236 conclusions axillary us is a fast , noninvasive examination that should be performed routinely in patients with breast carcinoma , as it can play a major role in the preoperative evaluation of metastatic spread . 
the main limitation of axillary us is its high false negative rate resulting from the presence of micrometastases in normal - appearing nodes and the failure to visualise all lymph nodes . on the basis of our experience , the preoperative staging of breast cancer patients scheduled for surgery can be improved by combining the us study of suspicious axillary nodes and us - guided fnac . 
in our series , axillary us combined with fnac led to a preoperative diagnosis of nodal metastasis in almost half of the patients ( 48.3% ) , who proceeded to immediate axillary dissection with a substantial reduction of costs , length of hospital stay and patients psychological distress . radiol med ( 2010 ) 115 : 225237 pre - operatoria nelleventualit di un coinvolgimento metastatico . 
bazzocchi1 1istituto di radiologia , universit degli studi di udine , via colugna 50 , 33100 udine , italy 2clinica ematologica , universit degli studi di udine , piazza santa maria della misericordia , 33100 udine , italy correspondence to : l . 
sixty - four cxrs of immunocompromised patients with clinically suspected pneumonia were retrospectively and independently evaluated by two radiologists to assess the presence of radiological signs of pneumonia , before ( first reading ) and after ( second reading ) the knowledge of clinical data . 
the sensitivity of cxr is too low to consider it a stand - alone technique for the evaluation of immunocompromised patients after hsct with suspected pneumonia , even if the radiologist knows detailed clinical riassunto obiettivo . 
due medici radiologi hanno valutato retrospettivamente 64 radiografie del torace di pazienti immunocompromessi con sospetto clinico di polmonite per leventuale presenza di reperti compatibili con polmonite , senza conoscere ( prima lettura ) e conoscendone ( seconda lettura ) la storia clinica . 
la sensibilit dei due radiologi stata rispettivamente del 39% e del 58 , 5% nella prima lettura e del 43 , 9% e del 41 , 5% nella seconda lettura . confrontando i dati ottenuti nella prima e nella seconda lettura emerso come , per entrambi i lettori , la differenza non fosse statisticamente significativa ( test di mcnemar , p > 0 , 05 )  . 
anche alla luce di dettagliate informazioni cliniche , la sensibilit della radiografia del torace rimane troppo bassa per considerare tale indagine sufficiente 206 radiol med ( 2010 ) 115 : 205214 data . 
for these patients , an early chest ct evaluation is therefore recommended . keywords chest radiography immunocompromised patient pneumonia hematopoietic stem cell transplantation nella valutazione dei pazienti immunocompromessi , in seguito a trapianto di cellule staminali emopoietiche , con sospetta polmonite . 
in tali pazienti , dunque consigliabile un precoce utilizzo della tc torace . parole chiave radiografia del torace paziente immunocompromesso polmonite trapianto di cellule staminali emopoietiche introduction introduzione the term immunocompromised patients refers to people affected by a congenital or acquired immune system dysfunction , with increased risk for life - threatening infections compared with the general population [ 1 ]  . 
the number of immunocompromised patients has greatly increased during the past few decades because of the spread of diseases such as acquired immunodeficiency syndrome ( aids ) and the wider use of immunosuppressive therapies for the treatment of many pathological entities , especially haematological in orig pneumonia represents the most frequent complication in these patients , affecting up to 60% of them [ 28 ]  . 
in the last few years , the early execution of a computed tomography ( ct ) examination on the basis of a clinical suspicion of pneumonia has become more widespread . 
thanks to information provided by ct , clinicians can narrow the spectrum of differential diagnosis , leading to more timely and proper therapy , with good probabilities of recovery for the patient [ 9 ]  . 
a diagnostic delay is associated with high mortality rates ( almost 30% ) in the population of immunocompromised patients after hematopoietic stem cell transplantation ( hsct ) [ 7 ]  . nevertheless , in clinical practice , chest radiography ( cxr ) still represents the first - line examination for immunocompromised patients with suspected pulmonary infection . 
the main drawback of cxr is a limited sensitivity in the detection of early infection in these patients , whose immune reactivity is poorer and delayed compared with immunocompetent ones [ 1014 ]  . 
to our knowledge , few authors have investigated the role of the knowledge of clinical and laboratory data in cxr evaluation of patients with suspected pulmonary infection , with discordant results [ 1517 ]  . 
 our purpose was to assess whether the knowledge of clinical data improves the diagnostic sensitivity of cxr in the setting of immunocompromised patients after hematopoietic stem cell transplantation . con il termine paziente immunocompromesso o immunodepresso ci si riferisce ad una popolazione di soggetti affetti da una disfunzione del sistema immunitario , congenita o acquisita , e per questo esposti ad un pi elevato rischio , rispetto alla popolazione generale , di contrarre infezioni potenzialmente letali [ 1 ]  . 
il numero dei pazienti immunodepressi notevolmente aumentato nelle ultime decadi , in ragione della diffusione di patologie quali la sindrome da immunodeficienza acquisita ( aids ) e di terapie immunosoppressive per la cura di numerosi stati morbosi , in particolar modo neoplasie ematologiche . 
grazie alle informazioni fornite dalla tc , il clinico pu restringere lo spettro della diagnosi differenziale e impostare in tal modo unadeguata terapia in tempi brevi , quando ancora vi sono buone probabilit di guarigione per il paziente [ 9 ]  . 
nella popolazione dei soggetti immunocompromessi in seguito a trapianto di cellule staminali emopoietiche , un ritardo diagnostico si associa ad un elevato rischio di mortalit ( prossimo al 30% ) [ 7 ]  . 
in tali pazienti , la cui reattivit al processo infettivo ridotta e ritardata rispetto ai soggetti immunocompetenti , il principale limite della radiografia del torace la limitata sensibilit nellidentificazione precoce di reperti patologici [ 1014 ]  . 
a nostra conoscenza , pochi autori hanno indagato il ruolo della conoscenza delle condizioni cliniche e dei dati laboratoristici di questi pazienti nellinterpretazione della radiografia del torace eseguita nel sospetto di polmonite , con risultati peraltro discordanti [ 1517 ]  . 
 scopo di questo studio stato stabilire se la conoscenza dei dati clinici migliori la sensibilit diagnostica della radiol med ( 2010 ) 115 : 205214 materials and methods patient population and imaging technique through a systematic review of the electronic ct database of our institution over a 3 - year period ( january 2006 december 2008 ) , we retrospectively identified 60 immunocompromised patients after hsct who underwent a chest ct examination for the clinical suspicion of pneumonia . among them , we selected those patients who had a cxr within 3 days before the ct examination , which represented the standard of reference of the study . 
a total of 44 patients ( 24 women and 20 men ; age range 2172 years ; mean age 49 years ) formed the final study population . thirty - one patients had undergone allogeneic transplant , nine autologous transplant and four both allogeneic and autologous transplant at different times . 
cxrs were all digital ( computed radiography system , cr 75.0 , agfa - gevaert , mortsel , belgium ) and consisted of 55 anteroposterior single - projection radiographys acquired in supine position at the patients bedside and 9 double - projection ( posteroanterior and lateral ) radiographys . 
 image interpretation two readers [ reader a ( gc ) and reader b ( rg ) , each with at least 5 years of experience in conventional x - ray imaging ] independently reviewed the cxrs in random order on a dedicated workstation ( impax el , agfagevaert )  . 
these data were obtained from the patients files stored in the archive of our division of haematology and included underlying disease , signs and symptoms at the time of the cxr ( fever , cough , thoracic pain , abnormalities at chest physical examination ) , time between the transplant procedure and clinical onset ( classified as less than 30 days , between 30 and 100 days , or more than 100 days ) , immune system status ( with special regard to the degree of neutropenia ) , any microbiological data available at the time of cxr and presence of a concomitant acute or chronic graft - versus - host disease ( gvhd )  . cxrs were assessed for the presence , appearance and location of parenchymal abnormalities , and the information was recorded on a standard data sheet . 
 materiali e metodi popolazione dei pazienti e tecniche di imaging mediante una revisione sistematica del database elettronico delle tc eseguite presso il nostro istituto in un periodo di tre anni ( gennaio 2006dicembre 2008 ) , abbiamo retrospettivamente identificato 60 pazienti immunocompromessi dopo trapianto di cellule staminali emopoietiche che hanno eseguito una tc del torace per sospetta polmonite . 
la popolazione finale dello studio stata formata quindi da un totale di 44 pazienti ( 24 femmine e 20 maschi ; range det , 2172 anni ; et media , 49 anni )  . 
per 14 di essi lassociazione rx torace / tc torace stata presa in considerazione pi di una volta ( per eventi tra loro non correlati ) , consentendoci cos di rivalutare in totale 64 rx del torace . tutti i radiogrammi sono stati acquisiti con tecnica digitale ( sistema computed radiography , cr 75.0 , agfa - gevaert , mortsel , belgio ) ed in particolare 55 in ununica proiezione antero - posteriore in posizione supina al letto del paziente e 9 in doppia proiezione ( postero - anteriore e laterale )  . 
 interpretazione delle immagini due lettori ( lettore a , gc , e lettore b , rg , ciascuno con almeno 5 anni di esperienza in radiologia convenzionale ) hanno valutato le radiografie del torace in maniera indipendente e con un ordine casuale , utilizzando unapposita workstation ( impax el , agfa - gevaert )  . 
tali dati , ottenuti dalle cartelle cliniche dei pazienti della nostra clinica ematologica , riguardavano : la patologia di base , i sintomi e i segni manifestati dal paziente al momento dellesecuzione del radiogramma ( febbre , tosse , dolore toracico , eventuali reperti patologici allesame obiettivo del torace ) , il periodo intercorso tra la data del trapianto e lesordio clinico ( specificando se questo fosse inferiore a 30 giorni , compreso tra 30 e 100 giorni , o superiore a 100 giorni ) , lo stato immunitario del paziente ( in particolare lentit della neutropenia ) , eventuali dati microbiologici a disposizione al momento dellesecuzione del radiogramma , la presenza di una concomitante malattia da trapianto 208 radiol med ( 2010 ) 115 : 205214 cxr findings using a four - grade scale ( grade i : noninfectious ; grade ii : probably noninfectious ; grade iii : possibly infectious ; grade iv : probably infectious )  . 
ct scans were performed on a single - slice toshiba asteion ct scanner ( toshiba medical systems , tokyo , japan ) in 45 cases and on a 4 - slice toshiba aquilion ct scanner in 19 cases . 
the scans were obtained at end - inspiration in a caudocranial direction by using a pitch factor of 1.4 and 3 - mm collimation ( aquilion scanner ) or 5 - mm collimation ( asteion scanner )  . data analysis sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and overall accuracy after the first and second readings were calculated for both radiologists . 
in a per - patient analysis , cxr was considered positive when the presence of at least one grade iii or grade iv parenchymal finding was assessed . the significance of differences in sensitivity , chosen as primary endpoint , was tested by using mcnemars test . 
sensitivity , specificity , ppv , npv and overall accuracy were 39% ( 16 / 41 ) , 95.7% ( 22 / 23 ) , 94.1% ( 16 / 17 ) , 46.8% ( 22 / 47 ) and 59.4% ( 38 / 64 ) , respectively . reader b detected 24 abnormalities out of 41 , corresponding to 17 false negative and 5 false positive cases . sensitivity , specificity , ppv , npv and overall accuracy were 58.5% ( 24 / 41 ) , 78.3% ( 18 / 23 ) , 82.8% ( 24 / 29 ) , 51.4% ( 18 / 35 ) and 65.6% ( 42 / 64 ) , respectively . 
 ogni radiogramma stato valutato in termini di presenza , aspetto e sede di alterazioni del parenchima polmonare ; le informazioni ottenute sono state registrate su un modello standard di raccolta dati . 
per ogni radiografia esaminata , i lettori dovevano esprimere il loro grado di sospetto per unalterazione di tipo infettivo utilizzando una scala semiquantitativa composta da 4 gradini ( grado i : reperto non infettivo ; grado ii : reperto molto probabilmente non infettivo ; grado iii : reperto possibilmente infettivo ; grado iv : reperto molto probabilmente infettivo )  . 
la tc stata eseguita in 45 casi con apparecchiatura tc spirale a singolo strato ( asteion , toshiba medical systems , tokyo , giappone ) ed in 19 casi con apparecchiatura tc multistrato a 4 strati ( aquilion , toshiba medical systems )  . 
le scansioni sono state eseguite con paziente in apnea inspiratoria , direzione caudo - craniale , pitch factor di 1 , 4 e collimazione pari a 3 mm ( apparecchiatura aquilion ) o 5 mm ( apparecchiatura asteion )  . 
 analisi dei dati con i dati ottenuti , sono stati calcolati sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) ed accuratezza di entrambi i radiologi nella prima e nella seconda lettura . 
un valore di k di 0 , 010 , 20 stato classificato concordanza scarsa ; 0 , 210 , 40 concordanza modesta ; 0 , 410 , 60 concordanza moderata ; 0 , 610 , 80 concordanza sostanziale ; 0 , 811 , 00 concordanza quasi perfetta . durante la lettura eseguita senza avere notizie cliniche del paziente , il lettore a ha riconosciuto correttamente 16 alterazioni parenchimali polmonari rispetto alle 41 rilevate alla radiol med ( 2010 ) 115 : 205214 fig . 
1a - d immagini relative ad una paziente femmina di 60 anni , 10 giorni dopo trapianto allogenico di cellule staminali emopoietiche , febbrile ( tmax = 38c ) ; esame obiettivo : crepitii in sede basale destra ; conta dei globuli bianchi : 0 , 91000 / mm3 . 
la tomografia computerizzata del torace eseguita due giorni dopo ( b - d ) ha delineato , a carico di entrambi i lobi superiori specie in regione subpleurica , la presenza di multipli addensamenti mal definiti con distribuzione a chiazze e di aree di opacit a vetro smerigliato . 
2a - d immagini relative ad un paziente maschio di 45 anni , pi di 100 giorni dopo trapianto allogenico di cellule staminali emopoietiche , febbrile ( tmax = 38c ) ; esame obiettivo : tosse secca e crepitii alla base polmonare sinistra ; conta dei globuli bianchi : 1 , 41000 / mm3 . 
la radiografia del torace in singola proiezione antero - posteriore ( a ) non ha evidenziato la presenza di alterazioni parenchimali polmonari . la tomografia computerizzata del torace ( b - d ) ha delineato la presenza di sfumati addensamenti parenchimali con qualche area di franco consolidamento a livello dei segmenti basale laterale e posteriore del lobo inferiore sinistro e , in misura minore , destro . 
sensitivity for singleand double - projection cxr was 39.4% ( 13 / 33 ) and 62.5% ( 5 / 8 ) for reader a and 36.4% ( 12 / 33 ) and 62.5% ( 5 / 8 ) for reader b , respectively . 
 seconda lettura nella valutazione effettuata alla luce delle notizie clinicolaboratoristiche , il lettore a ha identificato correttamente 18 alterazioni parenchimali polmonari su 41 , con 23 casi falsi negativi e nessun caso falso positivo . 
sensibilit , specificit , vpp , vpn ed accuratezza sono risultati rispettivamente pari a 41 , 5% radiol med ( 2010 ) 115 : 205214 table 1 identification of pulmonary abnormalities on chest radiography . 
values are percentages , with corresponding counts in parenthesis a nonsignificant ( p > 0.05 ) difference between these data and those obtained in the first reading ppv , positive predictive value ; npv , negative predictive value tabella 1 identificazione di alterazioni parenchimali polmonari alla radiografia del torace . 
values are percentages with corresponding counts in parenthesis single - projection cxr double - projection reader a reader b 39.4 ( 13 / 33 ) 36.4 ( 12 / 33 ) 62.5 ( 5 / 8 ) 62.5 ( 5 / 8 ) tabella 2 identificazione di alterazioni parenchimali polmonari alla radiografia del torace in singola e doppia proiezione . 
i valori sono riportati in percentuale con i corrispondenti numeri assoluti tra parentesi radiografia singola proiezione radiografia doppia proiezione discussione lettore a lettore b 39 , 4 ( 13 / 33 ) 36 , 4 ( 12 / 33 ) 62 , 5 ( 5 / 8 ) 62 , 5 ( 5 / 8 ) results of both radiologists after the two readings are reported in tables 1 and 2 . discussion the decision to focus on cxr sensitivity as a primary ( 17 / 41 ) , 87% ( 20 / 23 ) , 85% ( 17 / 20 ) , 45 , 5% ( 20 / 44 ) e 57 , 8% ( 37 / 64 )  . 
applicando il test di mc nemar , la differenza in termini di sensibilit dei lettori a e b tra la prima e la seconda lettura non risultata essere statisticamente significativa ( p > 0 , 05 )  . 
i risultati di entrambi i radiologi , con riferimento alle due letture , sono esposti nelle tabelle 1 e 2 . la decisione di considerare la sensibilit della radiografia del torace come end - point primario del nostro studio derivata dal fatto che questa il parametro diagnostico pi critico . 
infatti , dalla letteratura emerge come la radiografia del torace abbia una bassa sensibilit nellidentificazione di reperti patologici a livello polmonare nei pazienti immunodepressi dopo trapianto di cellule staminali emopoietiche con sospetta polmonite [ 18 , 19 ]  . 
 [ 20 ] , prendendo in considerazione 61 pazienti sottoposti a trapianto autologo di cellule staminali emopoietiche , hanno dimostrato come la 212 radiol med ( 2010 ) 115 : 205214 endpoint in our study derived from evidence that it represents the most critical diagnostic parameter . 
in fact , the reported sensitivity of cxr for the identification of pulmonary abnormalities in the immunocompromised patients after hsct with suspected pneumonia has been shown to be low [ 18 , 19 ]  . 
found that only 40% showed abnormalities , without influence on the current therapy [ 20 ]  . ct scan proved superior to cxr in a study by graham et al . on 18 patients who underwent allogeneic hsct , demonstrating alterations in 57% of those who had negative cxr [ 12 ]  . 
the purpose of this study was to investigate whether a detailed knowledge of the clinical data may improve the sensitivity of cxr in these patients , particularly those who underwent hsct . our results agree with previous studies , confirming the low sensitivity of cxr for early detection of pulmonary infiltrations . 
at a second independent reading before which radiologists were provided with detailed clinical information about the patients , sensitivity failed to improve significantly ; on the contrary , for reader b it worsened , although without statistical significance . 
indeed , cxr findings of aspergillus and cytomegalovirus infection , two of the most frequent pathogens in this setting , include ill - defined nodules and ground - glass changes and can be potentially very difficult to detect [ 2 ]  . 
the effective importance of the knowledge of the clinical picture and radiological signs in these patients is therefore not clear . our retrospective study has several limitations , first of all , the small number of patients and of double - projection radiografia del torace risultasse positiva soltanto nel 40% dei casi , senza peraltro portare a variazioni della terapia . 
la superiorit dellesame tc del torace rispetto alla radiografia stata dimostrata dal gruppo di graham [ 12 ] , in uno studio riguardante 18 pazienti sottoposti a trapianto allogenico di cellule staminali emopoietiche , in cui la tc ha mostrato alterazioni polmonari nel 57% dei pazienti con radiogramma negativo . 
 [ 13 ] su 94 pazienti in fase tardiva post trapianto di cellule staminali ( > 100 giorni ) , risultata essere solo del 58% , valore tale da portare alla raccomandazione dellesecuzione precoce di un esame tc [ 13 ]  . il valore della conoscenza del quadro clinico nellinterpretazione delle radiografie del torace in pazienti con sospetta patologia polmonare stato ampiamente indagato , e nella maggior parte degli studi presenti in letteratura si conferma lipotesi di una sua influenza positiva [ 16 , 17 , 2124 ]  . 
lo scopo di questo studio stato valutare se la conoscenza di dettagliate informazioni cliniche potesse migliorare la sensibilit della radiografia del torace in tali pazienti , in particolare in quelli la cui immunodepressione legata al trapianto di cellule staminali emopoietiche . i risultati emersi dal nostro studio sono in accordo con quelli presenti in letteratura , confermando la bassa sensibilit della radiografia del torace nellindividuare precocemente reperti patologici polmonari . 
nella seconda lettura delle radiografie , alla luce delle informazioni clinico - laboratoristiche , non si verificato un miglioramento statisticamente significativo della sensibilit ; al contrario , per il lettore b questa si ridotta , seppur in misura non significativa . 
i reperti radiografici delle infezioni da aspergillus e da cytomegalovirus , due dei patogeni pi frequenti in questo contesto clinico , comprendono la presenza di noduli mal definiti e di opacit tipo vetro smerigliato , potenzialmente molto difficili da individuare [ 2 ]  . 
in tali pazienti , non dunque del tutto chiara leffettiva importanza della conoscenza del quadro clinico e dei segni radiologici . il nostro studio retrospettivo presenta diversi limiti , legati soprattutto al basso numero sia di pazienti sia di radiografie ottenute con doppia proiezione . 
un secondo e forse pi importante limite consiste nellaver selezionato esclusivamente pazienti che , dopo la radiografia , sono stati sottoposti allesecuzione di una tc del torace , il nostro standard di radiol med ( 2010 ) 115 : 205214 cxrs obtained . 
 in conclusion , cxr sensitivity is still too low to consider it a stand - alone technique for the evaluation of immunocompromised patients after hsct with suspected pneumonia , even if the radiologist works in the best possible conditions , i.e. 
abbiamo quindi escluso tutti quei pazienti per i quali la radiografia era stata considerata esaustiva dal clinico , limitando la nostra analisi a soggetti con caratteristiche cliniche o radiologiche di difficile interpretazione . in conclusione , la sensibilit della radiografia del torace troppo bassa per considerare tale tecnica sufficiente nella valutazione di pazienti immunocompromessi dopo trapianto di cellule staminali emopoietiche con sospetta polmonite , anche nel caso in cui il medico radiologo operi nelle migliori condizioni possibili , ovvero avendo a disposizione una completa descrizione del quadro clinico dei pazienti stessi . 
universit di torino , asou san giovanni battista di torino , sede molinette , via genova 3 , 10126 torino , italy 2istituto di nefrologia dialisi e trapianti , universit di torino , asou san giovanni battista di torino , sede molinette , corso bramante 88 , 10126 torino , italy correspondence to : m.c. 
mri showed signal abnormalities suggestive of apn in 125 / 244 ( 51.2% ) patients with native kidneys . except for two examinations performed without paramagnetic contrast material , the inflammatory foci appeared as areas of nonenhancement : single in 39 / 123 cases , multiple in 84 / 123 , unilateral in 60 / 84 and bilateral in 24 / 84 . 
during follow - up , we observed complete normalisation of mri signs in 86 / 103 patients ; 17 / 103 ( 16.5% ) cases evolved into fibrosis and scarring . 
renal mri is an effective tool for the diagnosis and follow - up of apn both in patients not at risk and those at higher risk , such as those with a transplanted kidney . 
stata effettuata unanalisi retrospettiva di 442 esami consecutivi ( 279 in fase diagnostica e 163 di follow - up ) in 285 pazienti ( et media 42 , 17 anni ) di cui 35 portatori di trapianto renale con sospetto clinico per pna . 
eccetto in due casi , in cui gli esami sono stati eseguiti senza mezzo di contrasto ( mdc ) paramagnetico , i focolai flogistici apparivano come lacune di enhancement : singole in 39 / 123 casi , multiple in 84 / 123 , monolaterali in 60 / 84 e bilaterali in 24 / 84 . 
durante il follow - up si dimostrata una regressione completa dei segni rm in 86 / 103 pazienti ; 17 / 103 casi ( 16 , 5% ) sono andati incontro ad evoluzione fibrotico - cicatriziale . 
nella nostra esperienza la rm risultata uno strumento efficace nella diagnosi e nel follow - up della pna sia nei soggetti non a rischio , sia nei soggetti a rischio ( trapianto renale )  . 
gli elevati costi della metodica sono stati bilanciati dal corretto orientamento del trattamento clinico e dalla tempestiva individuazione delle complicanze . parole chiave risonanza magnetica pielonefrite acuta trapianto renale 288 introduction acute pyelonephritis ( apn ) is a nonspecific , suppurative ascending or blood - borne infection frequently associated with urinary tract infection ( uti ) and which simultaneously affects the renal calyces , pelvis , papillary interstitium and medullary pyramids [ 1 ]  . 
causative organisms are mainly escherichia coli ( 80% ) and , to a lesser extent , klebsiella , proteus , pseudomonas , staphylococcus and streptococcus [ 2 ]  . apn is defined as uncomplicated when it is caused by a typical pathogen in an immunocompetent patient with normal urinary tract anatomy and renal function and as complicated when it affects high - risk subjects , including diabetics ; subjects who are elderly , debilitated or affected by malformations that promote stasis or vesicoureteral reflux ; patients with urinary tract obstruction , indwelling vesical or nephrostomy catheters ; and immunocompromised subjects such as transplant recipients [ 3 ]  . the high incidence of apn 250 , 000 cases annually in the united states [ 4 ] with predominance among sexually active females younger than 50 years of age [ 5 ] and the relatively common occurrence of severe complications justify frequent hospitalisations and protracted antibiotic therapy despite the unavoidable increase in costs . 
if not adequately treated , apn may lead to sepsis and scarring , with loss of functioning parenchyma , which is a potential cause of renal failure and nephrogenic hypertension . 
abscess formation even beyond the renal parenchyma , and chronic kidney disease , are also possible complications [ 6 , 7 ]  . the diagnosis of apn is normally clinical , with medical history , clinical signs and symptoms and laboratory findings enabling differentiation between apn and uti and obviating the need for diagnostic imaging in the majority of cases [ 8 ]  . 
conversely , in cases of complicated apn and in subjects at risk or not responding to treatment , imaging is instrumental in detecting renal lesions , identifying associated conditions or conditions favouring inflammation and complications , defining extent of disease and severity of damage , and enabling a correct differential diagnosis and complete follow - up [ 9 ]  . 
in cases of uncomplicated apn in low - risk subjects , the systematic use of second - line imaging modalities computed tomography ( ct ) and magnetic resonance imaging ( mri ) , remains controversial . 
antibiotic treatment within 72 h will invariably justify further radiological investigation [ 10 , 11 ]  . the absence of ionising radiation or iodinated contrast agents , coupled with technological advances , have contributed to the increasing acceptance of mri as an alternative to ct in the study of uti , especially in pregnant women or women of childbearing age and patients with contraindications to iodinated contrast agents [ 9 , 12 ]  . 
as radiol med ( 2010 ) 115 : 287300 introduzione la pielonefrite acuta ( pna ) un processo flogistico aspecifico , a carattere suppurativo , secondario a diffusione batterica per via ascendente o ematogena , frequentemente associato a infezione delle basse vie urinarie ( ivu ) , che coinvolge contemporaneamente i calici , la pelvi e linterstizio della papilla e della piramide midollare del rene [ 1 ]  . 
i germi patogeni responsabili sono rappresentati nella maggior parte dei casi da escherichia coli ( 80% ) e in una minor parte da klebsiella , proteus , pseudomonas , stafilococco e streptococco [ 2 ]  . la pna definita non complicata quando sostenuta da un agente patogeno tipico e si sviluppa in soggetti immunocompetenti con anatomia dellapparato urinario e funzionalit renale normali . 
al contrario considerata complicata quando colpisce individui a rischio : diabetici , pazienti anziani , debilitati o affetti da malformazioni che favoriscano la stasi o il reflusso vescico - ureterale , soggetti con ostruzione delle vie urinarie o portatori di cateteri vescicali , nefrostomici o in stato di immunodepressione , come i trapiantati [ 3 ]  . lelevata incidenza della pna negli stati uniti si contano 250000 casi / anno [ 4 ] con predominanza nel sesso femminile , in particolare durante il periodo di attivit sessuale e al di sotto dei 50 anni [ 5 ] e la non infrequente insorgenza di complicanze anche gravi giustificano la frequente ospedalizzazione di questi pazienti e trattamenti antibiotici prolungati , ma comportano un inevitabile aggravio dei costi . 
la pna , se non adeguatamente trattata , pu esitare in sepsi o in un processo cicatriziale con perdita di parenchima funzionante , potenzialmente causa di insufficienza renale e di ipertensione nefrogenica . 
si pu inoltre complicare con formazione di lesioni ascessuali a estensione anche extraparenchimale o cronicizzarsi [ 6 , 7 ]  . in generale la diagnosi di pna di pertinenza clinica : anamnesi , sintomatologia e alterazioni dei valori di laboratorio consentono , nella maggior parte dei casi , di differenziare la pna dalle infezioni delle basse vie , evitando in questi casi il ricorso allimaging [ 8 ]  . 
al contrario nelle forme di pna complicata e nei soggetti a rischio o che non rispondono alla terapia , il contributo della diagnostica per immagini indispensabile per identificare le lesioni renali , per individuare patologie associate o favorenti la flogosi e le eventuali complicanze , per la definizione del bilancio di estensione della malattia e della severit del danno , per formulare una corretta diagnosi differenziale e per il follow - up [ 9 ]  . 
nei casi di pna non complicata in soggetti non a rischio limpiego sistematico delle tecniche di imaging cosiddette di secondo livello , tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) , rimane a tuttoggi controverso : tuttavia la presentazione atipica e la mancata risposta alla terapia antibiotica endovenosa entro 72 ore giustificano comunque un approfondimento diagnostico radiologico [ 10 , 11 ]  . lassenza di radiazioni ionizzanti e dellimpiego di radiol med ( 2010 ) 115 : 287300 with ct , dynamic mri with gadolinium chelates [ gadolinium diethylenetriamine pentaacetic acid ( gddtpa ) ] allows for morphological and functional evaluation of inflammatory renal disease and its potential complications [ 13 ]  . 
the rationale for the systematic use of ct and mri in apn lies in the fact that early diagnosis and monitoring of inflammation significantly influences both medical treatment and the duration and cost of hospitalisation . to assess the contribution of dynamic mri to the diagnosis , clinical staging and surveillance of apn , we retrospectively reviewed the results ( typical mri signs , impact on clinical treatment , follow - up ) obtained with mri in 285 patients with a clinical - laboratory suspicion of apn . materials and methods between august 2004 and june 2008 ( 46 months ) , abdominal mri was performed on 285 patients with a clinical suspicion of apn , 35 of whom were renal transplant recipients and therefore at increased risk of infection compared with the general population . 
all 285 patients reported symptoms including dysuria , pollakiuria , low back pain and usually fever , at times accompanied by chills on the day of the examination or on the immediately preceding days . 
suspicion for apn had been raised by clinical and laboratory findings [ creatinine , complete blood count , erythrocyte sedimentation rate ( esr ) , c - reactive protein ( crp ) , fibrinogen , procalcitonin , urinalysis ]  . 
additionally , in agreement with the department of nephrology and dialysis of the university of turin ( which had referred all of the patients in this study ) , our institute has adopted a diagnostic protocol for apn , which involves using mri both for diagnosis and follow - up to plan the most appropriate treatment and document its effectiveness . based on the integration of the clinical and imaging data , cases with positive imaging signs for apn but limited clinical manifestations received parenteral antibiotic treatment , with hospitalisation of the patient . 
conversely , cases with negative imaging signs for apn but with clinical findings either suspicious or positive for uti received oral antibiotic therapy and laboratory monitoring , generally without hospitalisation ( table 1 )  . altogether , we performed 442 mri examinations . 
la rm dinamica con chelati del gadolinio ( gd - dtpa ) consente infatti , al pari della tc , la valutazione morfologica e funzionale della compromissione flogistica renale e delle sue potenziali complicanze [ 13 ]  . 
il razionale ad un impiego sistematico di tc e rm nella valutazione della pna risiede nella dimostrazione che la diagnosi precoce e il monitoraggio dellevoluzione del processo flogistico influenzano significativamente sia il trattamento medico , sia i tempi e i costi di ospedalizzazione . lobiettivo di questo studio retrospettivo condotto su 285 pazienti con sospetto clinico - laboratoristico di patologia flogistica acuta renale stato quello di valutare , attraverso lanalisi dei risultati evidenza dei segni rm tipici , impatto sul trattamento clinico , follow - up il reale contributo della rm dinamica nel raggiungimento della diagnosi , nellinquadramento clinico e nella sorveglianza della malattia , presupposti indispensabili per evitare terapie inadeguate e ricoveri ingiustificati . materiali e metodi nel periodo compreso fra agosto 2004 e giugno 2008 ( 46 mesi ) presso il nostro istituto sono stati sottoposti ad esame rm delladdome 285 pazienti con sospetto clinico di pielonefrite acuta di cui 35 sottoposti in precedenza a trapianto renale e , come tali , con aumentati fattori di rischio a contrarre infezioni rispetto alla popolazione generale . 
dei 285 pazienti esaminati 228 ( 80% ) erano femmine e 57 ( 20% ) maschi con et media complessiva di 47 , 17 anni ( intervallo 1490 anni ) ; let media delle femmine era 39 , 34 anni quella dei maschie 55 , 53 mentre dei 35 portatori di trapianto renale ( 19 femmine e 16 maschi ) let media era di 52 , 14 anni ( intervallo 2870 anni )  . 
tutti i 285 pazienti presentavano al momento dellesame , o avevano presentato nei giorni immediatamente precedenti , una sintomatologia caratterizzata da disuria , pollachiuria , dolore lombare e febbre , solitamente elevata e , in alcuni casi , accompagnata da brivido . 
il sospetto di pna era stato formulato sulla base dei dati clinici e dei rilievi laboratoristici ( creatinina , emocromo , velocit di eritrosedimentazione [ ves ] , proteina c reattiva [ pcr ] , fibrinogeno , procalcitonina , esame urine )  . 
the first follow - up study was performed on average 30 days after diagnostic mri ( range 1090 days ) , and each patient underwent one to four follow - up mri studies . 
contrast was administered at a flow rate of 2 ml / s and dose of 0.10.2 mmol / kg depending on the product used [ gd - dtpa magnevist bayer - schering pharma ; gd - do3a - butriol , gadovist , bayer - schering pharma ag ; gd - tetraazacyclododecane tetraacetic acid ( dota ) , dotarem guerbet ] , followed by a 20 - ml bolus of saline solution delayed acquisitions in the axial and coronal planes with t1 - weighted gre sequences obtained 510 min after the beginning of contrast infusion the signs evaluated on diagnostic mri to confirm or rule out the clinical suspicion of apn were : change in renal volume ( typically increased in the presence of inflammatory oedema ) preservation , decrease or loss of the corticomedullary gradient focal or diffuse signal alterations on baseline scans areas of nonenhancement after contrast administration ( single , multiple , unilateral or bilateral ) phase of the examination during which nonenhancement site ( s ) of the signal alterations ( upper renal pole , middle was evident third , lower pole ) presence of abscess foci extrarenal spread of the inflammatory process ( perirenal and / or pararenal ) urinary tract dilatation ( unilateral or bilateral ) results patients with native kidneys diagnostico per la pna che ha previsto lutilizzo della rm sia in fase diagnostica , sia nel follow - up al fine di impostare il trattamento medico pi idoneo e documentarne i risultati . sulla base dellintegrazione del quadro clinico con la diagnostica per immagini , anche in presenza di manifestazioni cliniche scarsamente rilevanti , ma con segni di imaging suggestivi per pna , si proceduto al trattamento antibiotico parenterale con ospedalizzazione del paziente . viceversa nei casi con imaging negativo per pna , ma in presenza di un quadro clinico sospetto o positivo per ivu si invece optato per la terapia per via orale e monitoraggio laboratoristico , generalmente senza necessit di ricovero ospedaliero ( tabella 1 )  . 
 complessivamente abbiamo eseguito 442 esami rm : 279 in fase diagnostica e 163 durante il follow - up ( 153 nei pazienti con reni nativi e 10 nei pazienti con reni trapiantati ) , per monitorare levoluzione dei focolai flogistici e la risposta alla terapia antibiotica . 
signal alterations suggestive of apn were already seen at baseline , mainly as areas of t1 isohypointensity and t2 hyperintensity in 25 / 125 ( 20% ) cases ( table 2 )  . 
in 2 / 125 patients , the dynamic contrastenhanced examination could not be performed due to a technical reason in one case and pregnancy in the other . nonetheless , the presence of typical signal alterations on baseline acquisitions coupled with the clinical - laboratory sede / i delle alterazioni di segnale ( polo superiore , terzo medio , polo inferiore del / i rene / i ) ; presenza di focolai di ascessualizzazione ; estensione extrarenale del processo flogistico ( spazi peri e / o pararenali ) ; dilatazione delle vie escretrici ( mono o bilaterale )  . risultati pazienti con reni nativi la rm ha evidenziato alterazioni di segnale suggestive per pna ( riassunte nella tabella 2 ) in 125 / 244 ( 51 , 22% ) pazienti table 2 signal alterations in the 125 cases with magnetic resonance imaging ( mri ) findings suggestive for acute pyelonephritis ( apn ) finding no . 
 characteristics unilateral ( n = 26 ) ; bilateral ( n = 8 ) decreased / absent t1 - w isohypointense / t2 - w hyperintense t1 - w and t2 - w hypointense t1 - w and t2 - w hyperintense areas of nonenhancement on t1 - wa arterial / venous / delayed arterial / venous arterial only delayed only atypical ( venous - phase enhancement and delayed - phase nonenhancement ) bilateral ( 24 ) ; unilateral ( 60 ) unilateral atwo patients studied without contrast agent were excluded ( see text ) tabella 2 alterazioni di segnale nei 125 casi con segni rm suggestivi per pna reperto caratteristiche increased renal volume corticomedullary differentiation baseline abnormalities ( signal intensity ) dynamic abnormalities ( dynamic phases ) multiple lesions single lesions abscesses perirenal fluid collections volume renale aumentato gradiente cortico - midollare alterazioni in condizioni basali ( intensit di segnale ) alterazioni dinamiche ( fasi dinamiche ) focolai multipli focolai singoli focolai ascessuali falde / raccolte liquide perirenali aesclusi 2 pazienti nei quali lesame stato condotto senza mdc ( motivazioni nel testo ) monolateralmente : 26 ; bilateralmente : 8 ridotto / assente iso - / ipointenso in t1 / iperintenso in t2 ipointenso in t1 e t2 iperintenso in t1 e t2 lacune di enhancement in t1 - wa arteriosa / venosa / tardiva arteriosa / venosa solo arteriosa solo tardiva atipica ( impregnazione venosa e lacuna tardiva ) bilaterali : 24 ; monolaterali : 60 monolaterali radiol med ( 2010 ) 115 : 287300 findings allowed the diagnosis of apn to be established . 
1a - h a 39 - year - old woman with unilateral acute pyelonephritis ( apn )  . the left kidney is enlarged , and in the arterial phase of the dynamic study , three extensive areas of nonenhancement ( maximum diameter in the coronal plane 4 cm ) are recognizable at the upper pole , at the middle third ( a ) and at the lower pole ( b ) persisting also in the delayed phase ( c )  . 
1a - h giovane donna di 39 anni con pna monolaterale : il rene sinistro aumentato di volume e si riconoscono nella fase arteriosa dello studio dinamico tre estese lacune di enhancement ( diametro massimo nel piano coronale 4 cm ) localizzate al polo superiore , al terzo medio ( a ) e al polo inferiore ( b ) fase che permangono anche nella tardiva ( c )  . 
dopo 20 giorni di terapia antibiotica parenterale si osserva un netto miglioramento : le lacune sono ancora visibili nella fase arteriosa ( d ) , ma sono pressoch scomparse nella fase venosa ( e )  . 
dopo altri 2 mesi si osserva la completa guarigione con scomparsa delle alterazioni di segnale nello studio dinamico ( f - h )  . 294 radiol med ( 2010 ) 115 : 287300 ( table 2 )  . 
among the findings associated with apn , there was dilatation of the upper urinary tract in 21 / 125 patients , though none of our patients showed signs of hydropyonephrosis . 
the remaining 119 / 244 ( 48.7% ) patients with native kidneys showed no signal alteration typical of apn . of the 125 / 244 patients with native kidneys positive for apn , 103 / 125 underwent a total of 153 follow - up mri studies ; 22 / 125 did not undergo follow - up mri . 
alterazioni di segnale sospette per pna evidenti gi in condizioni basali sono state osservate in 25 / 125 ( 20% ) casi per lo pi come aree di iso - / ipointensit in t1 e iperintensit in t2 ( tabella 2 )  . 
in 2 / 125 pazienti non stato possibile eseguire lo studio dinamico con mdc ev , in un caso per cause tecniche e nellaltro per gravidanza ; la presenza nelle acquisizioni basali di alterazioni di segnale tipiche , integrate dai dati clinico - laboratoristici hanno comunque consentito di formulare la diagnosi di pna . 
in 29 / 125 pazienti si sono riscontrate aree cicatriziali correlabili a pregressi episodi di pielonefrite acuta , caratterizzate da assottigliamento e retrazione parenchimale . tra i reperti associati a pna si evidenziata una dilatazione delle vie escretrici superiori in 21 / 125 pazienti , ma in nessun paziente si sono rilevati segni di idropionefrosi . 
quali reperti collaterali , sono stati osservati un caso di colecistite acuta ed un caso di ispessimento della parete colecistica senza altri segni di flogosi in atto ( tabella 3 )  . 
 per quanto riguarda i 125 / 244 pazienti con reni nativi positivi per pna , in 103 / 125 abbiamo eseguito complessivamente 153 esami rm di follow - up mentre 22 / 125 non hanno effettuato la rm di controllo . 
 discussion the role of diagnostic imaging in confirming a clinical suspicion of apn and its impact on treatment decisions has in 15 / 35 ( 42 , 8% ) pazienti con rene trapiantato sono stati pazienti con rene trapiantato radiol med ( 2010 ) 115 : 287300 fig . 
2a - l a 50 - year - old man with a history of previous acute pyelonephritis ( apn ) episodes , who underwent magnetic resonance imaging ( mri ) for worsening clinical symptoms . 
an area of hypointensity , better depicted by t2 - weighted than t1weighted acquisitions , can be seen at the upper pole of the right kidney ( a , b )  . 
the dynamic study confirms the presence of a large area of nonenhancement involving most of the upper pole of the kidney in the arterial phase ( c ) and in the venous phase ( d )  . 
sixty days later ( corresponding to the second follow - up examination ) , healing of the infectious focus results in a scar that is hypointense in t1 and t2 and causes retraction of the renal margin ( f , g )  . 
the arterial ( h ) and venous ( i ) dynamic phases show almost complete revascularisation of the renal parenchyma surrounding the scar but also a corticalisation of the corresponding calyx . 
dopo 60 giorni ( corrispondenti al secondo controllo di follow - up ) si osserva la guarigione del focolaio che esita in una cicatrice retraente il profilo renale , ipointesa in t1 e t2 ( f , g )  . le fasi dinamiche arteriosa ( h ) e venosa ( i ) dimostrano una pressoch completa rivascolarizzazione del parenchima pericicatriziale , ma anche la corticalizzazione del calice corrispondente . 
nella fase tardiva ( l ) la lesione ascessuale completamente regredita . 296 radiol med ( 2010 ) 115 : 287300 table 3 associated findings in the 125 patients affected by apn description fibrous scars upper urinary tract dilatation renal cysts urinary tract lithiasis pyeloureteral junction defect renal malrotation acute cholecystitis thickened gallbladder wall 19 mild / moderate 2 marked tabella 3 reperti associati nei 125 pazienti affetti da pna reperto esiti flogistici cicatriziali dilatazione vie escretrici cisti renali calcolosi vie urinarie difetto del giunto pieloureterale malrotazione renale colecistite acuta ispessimento pareti della colecisti 19 lieve / moderata 2 marcata been reported by several studies [ 4 , 14 , 15 ]  . 
 [ 4 ] emphasised that imaging is indispensable not only for identifying cases of severe disease but also for confirming treatment effectiveness during the follow - up . despite the well - established mri semeiotics , relatively few studies have emphasised the value of gadolinium - enhanced dynamic mri in the diagnosis and follow - up of apn , and no data are available on the diagnostic accuracy of the technique in adults . 
in animal studies [ 16 ] , dynamic mri has a reported sensitivity and specificity of 91% and 93% , respectively , in the diagnosis of experimentally induced apn . studies comparing 99mtcdimercaptosuccinic acid ( dmsa ) scintigraphy and mri in apn in children report equivalent sensitivity ( 90.9% ) and specificity ( 88.8% ) values for gadolinium - enhanced mri with inversion recovery sequences but emphasise its superiority in differentiating scars from pyelonephritic foci in the early stages of disease [ 17 , 18 ]  . in consideration of these data , we used mri in the study of apn both as an initial diagnostic investigation in place of ultrasound followed by ct , as was done in the past and as a follow - up investigation to monitor the evolution of inflammatory foci and the effects of therapy . 
per documentare la regressione dei focolai flogistici in 8 / 15 pazienti stato sufficiente un unico esame di follow - up , mentre in un solo paziente si sono resi necessari due controlli successivi . 
dei restanti 20 pazienti portatori di trapianto in 18 non si sono evidenziati segni rm di pielonefrite acuta e negli altri 2 casi i reperti erano suggestivi per condizioni patologiche differenti dalla pna . discussione il ruolo della diagnostica per immagini nella conferma dellipotesi clinica di pna ed i risvolti nellimpostazione terapeutica sono gi stati sottolineati in una serie di studi [ 4 , 14 , 15 ]  . 
 [ 4 ] sottolineano come limaging sia indispensabile non solo per individuare i casi con caratteristiche di gravit , ma anche durante la fase di follow - up per confermare lefficacia della terapia . attualmente , in letteratura , a fronte di una semiotica rm ormai codificata , sono relativamente poco numerosi gli studi che enfatizzano il ruolo della rm dinamica con gadolinio nella diagnosi e soprattutto nel follow - up della pna e non sono disponibili dati relativi allaccuratezza diagnostica dellindagine in soggetti adulti . 
in studi su animali [ 16 ] sono riportate una sensibilit e una specificit della rm dinamica nella diagnosi di pna indotta sperimentalmente , rispettivamente pari al 91% ed al 93% , confermate istologicamente . 
studi condotti nei bambini comparando la scintigrafia 99mtc - dmsa ( acido dimercaptosuccinico ) riferiscono una sensibilit ( 90 , 9% ) e specificit ( 88 , 8% ) della rm con gadolinio utilizzando sequenze inversion recovery , sovrapponibile a quella della scintigrafia nella diagnosi di pna , ma ne sottolineano la superiorit nel differenziare le cicatrici dai focolai pielionefritici nelle fasi precoci di malattia [ 17 , 18 ]  . alla luce di questi dati abbiamo utilizzato lesame rm nello studio delle pna sia in prima istanza in fase diagnostica , diversamente dalliter utilizzato in passato che prevedeva limpiego dellecografia e successivamente della tc , sia durante il follow - up per monitorare levoluzione dei focolai flogistici e gli effetti della terapia . 
le ragioni che ci hanno indotto ad utilizzare la rm dinamica , soprattutto per il follow - up delle pna sono state motivate anche dal confronto in letteratura con le altre metodiche di imaging . lecografia , indagine operatore dipendente e non oggettiva , ha bassi valori di sensibilit ( 56 , 7% ) e specificit ( 74 , 3% ) e non consente , per le sue caratteristiche intrinseche di ridotta risoluzione spaziale , di formulare un corretto bilancio di estensione della malattia [ 9 ]  . 
la tc multidetettore , ritenuta da molti autori lindagine gold standard nella valutazione dei pazienti con pna per gli elevati valori di sensibilit e specificit ( 86 , 8% e 87 , 5% rispettivamente ) e per il vantaggio di consentire , in un unico esame e in tempi ormai radiol med ( 2010 ) 115 : 287300 of apn , were also justified by comparisons with other imaging techniques reported in the literature . 
ultrasonography , an operator - dependent , nonobjective method , has low sensitivity ( 56.7% ) and specificity ( 74.3% ) and , due to its intrinsic limited spatial resolution , does not permit a correct definition of disease extent [ 9 ]  . 
among male subjects , mean age was higher ( 55.33 years ) , presumably coinciding with the onset of prostatic hyperplasia , a cause of urinary stasis and possible risk factor for the pyelonephritic process [ 9 ]  . 
in fact , our series confirms that t1 and t2 baseline acquisitions have low sensitivity in identifying inflammatory foci , as only 21.36% of patients showed the typical signs of t1 hypointensity and t2 hyperintensity in relation to the distribution of parenchymal oedema . 
the decrease or loss of corticomedullary gradient was only observed in 7.2% of cases ( associated in 6 / 9 cases with severe apn complicated by signs of abscess formation ) , in bearing with the variability of this finding , which is not pathognomonic of apn [ 6 ]  . the dynamic contrast - enhanced study consistently enabled identification of inflammatory foci , increasing diagnostic confidence in cases suspected at baseline and , above all , demonstrating foci that were not detected at baseline . during the dynamic study , the inflammatory foci appeared as more - or - less extensive areas of nonenhancement , with a streaked appearance in the nephrographic phase ( the most sensitive phase in identifying nonenhancing areas during acute infection ) , in agreement with previous reports [ 4 , 9 ]  . brevissimi , la valutazione del parenchima , delle vie escretrici e dei vasi [ 9 ]  . 
a fronte di una elevata accuratezza ha tuttavia il limite dellutilizzo di mdc organoiodato e dellimpiego di elevate dosi di radiazioni , problema questo non trascurabile considerando la maggiore incidenza della malattia in pazienti giovani e di sesso femminile e la necessit di controlli ripetuti nel tempo per valutare levoluzione dei focolai flogistici e lefficacia della terapia . 
 nella nostra esperienza , analogamente ai dati della letteratura [ 9 , 19 ] la maggioranza ( 95 , 76% ) dei pazienti con sospetto clinico e positivit rm per pna sono state giovani donne ( et media di 39 , 41 anni )  . 
nella popolazione maschile let media risultata superiore ( 55 , 33 anni ) , coincidendo pi verosimilmente con linsorgenza di iperplasia prostatica che , causando stasi urinaria , considerata un fattore favorente il processo pielonefritico [ 9 ]  . 
non di meno , anche in un episodio di pna insorta durante la gravidanza , lrm senza mezzo di contrasto [ 9 , 20 ] rappresenta un ulteriore strumento diagnostico oltre allecografia : nel caso da noi valutato le sole alterazioni di segnale evidenziate nelle acquisizioni basali sono state sufficienti per confermare il sospetto clinico ed ecografico sebbene lo studio basale non sia stato sempre accurato . 
soltanto nel 21 , 36% dei pazienti , le lesioni mostravano una semeiotica tipica di ipointensit di segnale nelle sequenze t1 e iperintensit nelle t2 , in rapporto alla distribuzione delledema parenchimale . 
la rm ci ha consentito di valutare con precisione le alterazioni morfologiche quando presenti : lincremento volumetrico renale , correlato alledema , stato riscontrato in circa un terzo ( 27 , 2% ) dei pazienti con pna . 
la riduzione o scomparsa del gradiente cortico - midollare stata osservata solo nel 7 , 2% dei casi ( per lo pi associata 6 / 9 casi a quadri di pna pi severi , complicati con segni di ascessualizzazione ) , in accordo con il dato che si tratta comunque di reperti incostanti , non patognomonici della malattia [ 6 ]  . 
 al contrario lo studio dinamico con mezzo di contrasto paramagnetico ha sempre consentito il riconoscimento dei focolai flogistici incrementando la confidenza diagnostica nei casi gi sospetti in condizioni basali e , soprattutto , rilevando la presenza di focolai non visualizzabili o misconosciuti nelle sole condizioni basali . 
durante lo studio dinamico i focolai flogistici apparivano come aree pi o meno estese di mancata impregnazione contrastografica , con aspetto striato nella fase nefrografica ( risultata la pi sensibile per lindividuazione delle lacune di enhancement in corso di infezione acuta ) , analogamente a quanto gi descritto da altri autori [ 4 , 9 ]  . 
la fase tardiva invece risultata indispensabile per individuare e caratterizzare i focolai ascessualizzati , presenti in circa un terzo dei pazienti ( 32% ) : il loro aspetto tipico sottoforma di lacune ipointense con cercine periferico iperintenso ha consentito infatti di differenziarli agevolmente sia dai focolai non 298 radiol med ( 2010 ) 115 : 287300 on the other hand , the delayed phase was instrumental in identifying and characterising the abscess foci , present in approximately one third of patients ( 32% )  . 
in fact , their typical appearance as areas of hypointensity with hyperintense peripheral rim enabled easy differentiation from nonabscessed foci and infarction scars . regarding collateral findings , a significant finding was cholecystic involvement ( one acute cholecystitis and one case of thickened gallbladder wall ) in patients with large inflammatory foci in the upper pole of the right kidney . such association with renal infection has been reported as a frequent occurrence , albeit with uncertain aetiopathogenesis [ 2123 ]  . on the basis of our experience , we believe that dynamic mri , a noninvasive and repeatable technique , may be particularly valuable during the follow - up of apn as , unlike clinicallaboratory investigations , it is able to demonstrate directly the disappearance of inflammatory foci , thereby providing evidence of complete healing . 
 in effect , serial follow - up studies demonstrated a decrease in the number and extension of foci and a change from bilateral to unilateral involvement and ultimately the disappearance of the areas of nonenhancement , all of which are considered predictors of positive outcome and indicators of treatment effectiveness [ 14 ]  . 
follow - up with dynamic mri allowed differentiation between active foci of apn and scar tissue , seen in 16.5% of positive cases , predominantly in subjects with more extensive and severe infection at diagnosis due to the presence of abscesses . 
renal scars are characterised by parenchymal retraction , more - or - less marked deformation of the renal contour and constant signal hypointensity both at baseline and on delayed postcontrast scans [ 6 , 9 , 14 ]  . 
this finding , while not unexpected [ 1 ] , provided additional confirmation that imaging is instrumental in assessing the real severity of renal damage . although this approach involving more than one mri follow - up study in some cases ( up to four per patient ) may be questionable in terms of cost effectiveness , it nonetheless represents the rationale for the use of mri . 
in the presence of a definitive diagnosis of apn , the detailed morphological study obtained with the first mri study formed the basis for selecting and tailoring the antibiotic therapy , with cases of more severe parenchymal impairment being treated with a combination of either a penicillin ( with a beta - lactamase inhibitor ) or a carbapenemic antibiotic with an aminoglycoside , the latter taken for > 710 days in the case of abscess formation . 
during the follow - up , in addition to the clinical data and laboratory monitoring of inflammation markers , mri documented the evolution of the inflammatory focus , allowing us to customise treatment ascessualizzati sia dalle lesioni infartuali . 
 riguardo al riscontro di reperti collaterali nel corso dellesame , ci parso significativo ricordare il coinvolgimento colecistico ( 1 colecistite acuta e 1 caso di inspessimento delle pareti ) in pazienti con esteso focolaio flogistico del polo superiore del rene destro , poich la sua associazione con processi infettivi renali stata descritta da alcuni autori in letteratura come reperto non infrequente anche se ad eziopatogenesi ancora incerta [ 2123 ]  . 
 sulla base alla nostra esperienza riteniamo che la rm dinamica , in quanto indagine non invasiva e ripetibile , possa essere vantaggiosamente impiegata soprattutto nel follow - up se si considera che , a differenza dei rilievi clinico - laboratoristici , soltanto la dimostrazione della scomparsa dei focolai flogistici pu garantire lavvenuta guarigione . 
 i controlli seriati hanno infatti consentito di evidenziare la riduzione del numero , dellestensione delle localizzazioni e del coinvolgimento da bia monolaterale dei focolai fino alla scomparsa delle lacune di enhancement , considerati fattori prognostici positivi ed indici di efficacia terapeutica [ 14 ] , avvalorando , seppure a posteriori , in assenza di riscontri istologici , laccuratezza dei segni rm di pielonefrite acuta evidenziati in fase diagnostica . 
nondimeno il follow - up con rm dinamica ha consentito di differenziare focolai di pielonefrite attiva da esiti evolutivi cicatriziali , riscontrati nel 16 , 5% dei casi positivi , prevalentemente nei soggetti che alla diagnosi presentavano una maggior estensione e gravit del processo flogistico per la presenza di lesioni ascessuali . 
gli esiti cicatriziali risultano caratterizzati da retrazione parenchimale e deformazione pi o meno marcata del profili renali e segnale costantemente ipointenso , sia nelle acquisizioni basali , sia in quelle tardive dopo infusione di mdc [ 6 , 9 , 14 ]  . 
ci , se da un lato ha costituito un dato non inatteso [ 1 ] , dallaltro ha ulteriormente confermato come limaging sia indispensabile per stimare la reale gravit del danno renale . tale atteggiamento che ha comportato la necessit di eseguire in alcuni casi pi di un controllo rm al follow - up ( fino ad un massimo di 4 per paziente ) pu essere criticabile in termini economici , ma al tempo stesso costituisce il razionale per limpiego della rm . 
in presenza di una diagnosi confermata di pna , lanalisi morfologica approfondita consentita dalla rm al primo controllo , ha rappresentato la base per la scelta e la conduzione del trattamento antibiotico , riservando alle situazioni di maggiore compromissione del parenchima lassociazione di una penicillina ( associata ad un inibitore delle beta - lattamasi ) o di un carbapenemico con un aminoglicoside , questultimo protratto per un periodo superiore ai 710 giorni in caso di evoluzione ascessuale . 
nel follow - up accanto ai dati clinici ed al monitoraggio degli indici di flogosi , le caratteristiche evolutive del focolaio flogistico documentate con la rm hanno consentito di modulare in modo personalizzato limpostazione terapeutica con lobiettivo di ottenere una guarigione completa della lesione del parenchima garantendo inoltre il massimo contenimento delle molecole suscettibili di radiol med ( 2010 ) 115 : 287300 to achieve complete healing of the lesions while limiting as much as possible exposure to nephrotoxic molecules and overall duration of treatment , to be continued at home where necessary . in the evaluation of renal transplant patients , mri allowed us to differentiate all signal alterations that are not typical of inflammation and that may be ascribed to other posttransplant pathological conditions ( acute tubular necrosis , cyclosporin toxicity , acute and chronic rejection )  . in these patients , the use of mri is justified by the increased risk of developing infectious complications and renal scarring [ 14 ] or rejection in the immediate postoperative period , and by the possibility that the infection is poorly symptomatic , which could lead to delays in diagnosis and treatment [ 9 , 24 ]  . limitations to the use of mri in the diagnosis and follow - up of apn are its known contraindications , its high costs , the limited availability of adequate equipment compared with ct and the possible side effects of gadolinium - based agents [ 25 ]  . 
such sequences are currently under investigation as concerns both the differentiation of healthy from neoplastic parenchyma [ 26 , 27 ] and the diagnosis of inflammatory processes [ 28 ]  . although our study suffers the limitation of not having a gold standard to evaluate the accuracy of dynamic mri in apn compared with other techniques , our aim was to justify and emphasise the value of the technique not only in the diagnosis but especially in the follow - up of the main categories of patients affected by apn , namely , young women of childbearing age and renal transplant recipients . conclusions in our experience , contrast - enhanced mri of the renal parenchyma in clinically suspected apn proved to be accurate for confirming the disease , identifying and quantifying inflammatory foci and monitoring changes during the follow - up . 
in fact , negative mri findings or the detection of more - or - less extensive foci allowed us to institute targeted and timely treatments , which translated into different costs and different degrees of patient inconvenience . 
based on the fundamental role played by mri in treatment planning and disease monitoring in our series , we suggest that mri should be used as an alternative to ct for the diagnosis , especially in patients at high risk of nefrotossicit , della durata complessiva della terapia , eventualmente proseguita , se necessario , a domicilio . nella valutazione dei pazienti con rene trapiantato la rm ci ha permesso di differenziare le alterazioni di segnale non tipiche della flogosi e imputabili ad altre condizioni patologiche del periodo post - trapianto ( necrosi tubulare acuta , tossicit da ciclosporina , rigetto acuto e cronico )  . 
in questi pazienti limpiego della rm giustificato per la maggiore suscettibilit a sviluppare complicanze di tipo sia infettivo sia evolutivo cicatriziale [ 14 ] , ma anche di altra natura , quale il rigetto , soprattutto nellimmediato post - operatorio , oltrech dalla possibilit che linfezione si associ ad un quadro clinico oligosintomatico che potrebbe , al contrario , comportare ritardi diagnostici e terapeutici [ 9 , 24 ]  . i limiti allimpiego della rm per la diagnosi ed il followup della pna sono rappresentati dalle comuni controindicazioni della metodica , dagli elevati costi , dalla minore disponibilit di apparecchiature adeguate , nei confronti delle tc , e dai possibili effetti collaterali dei mdc a base di gadolinio [ 25 ]  . 
non escluso che , in questi casi , possano essere utilizzate sequenze in diffusione per lo studio funzionale renale che non necessitano di mdc e che sono attualmente in fase di studio sperimentale sia per la differenziazione del parenchima sano da quello neoplastico [ 26 , 27 ] , sia per la diagnosi dei processi flogistici [ 28 ]  . se da un lato il nostro studio risente del limite di non disporre di una metodica gold standard di riferimento per valutare laccuratezza della rm dinamica nelle pna nei confronti delle altre indagini , dallaltro il nostro obiettivo era piuttosto quello di motivarne e sottolinearne limpiego non soltanto nella diagnosi , ma soprattutto nel follow - up dei pazienti maggiormente colpiti quali le donne giovani in et fertile e quelli sottoposti a trapianto renale . conclusioni nella nostra esperienza , lo studio rm con mdc del parenchima renale , nel sospetto clinico di pna , si rivelato unindagine accurata ai fini della conferma della patologia , dellidentificazione e quantificazione dei focolai e nel follow - up . 
la negativit del quadro rm o , al contrario , la dimostrazione di focolai pi o meno estesi hanno infatti consentito lattuazione di terapie mirate e tempestive , traducendosi oltre che in costi diversi anche in un diverso comfort per il paziente . la persistenza di alterazioni di segnale nel follow - up ha condizionato la durata del trattamento ed eventualmente lindicazione a ulteriori indagini . 
soprattutto per il ruolo che nella nostra casistica la rm ha rivestito nellinquadramento terapeutico e nella sorveglianza della malattia riteniamo opportuno proporla in fase diagnostica , in alternativa alla tc , soprattutto nei pazienti a maggior rischio di 300 radiol med ( 2010 ) 115 : 287300 infection and in whom quantification of disease extent is particularly important , whereas its use during the follow - up is recommended for all patients . infezione ed in cui sia particolarmente importante quantificare lestensione della patologia , mentre il suo utilizzo nel follow - up sicuramente consigliabile in tutti i pazienti . 
carbognin , universit of verona , verona , italy , tel . : + 39 - 045 - 8124657 , fax : + 39 - 045 - 8277808 , e - mail : giovanni.carbognin@azosp.vr.it received : 22 january 2009 / accepted : 2 march 2009 / published online : 7 august 2009 springer - verlag 2009 abstract purpose . 
eleven patients ( 9 women and 2 men ; mean age 68 years ; age range 5882 ) with painful osteolytic vertebral body metastases unresponsive to conservative treatments underwent rf combined with kp under general anaesthesia . 
primary neoplasms were kidney carcinoma ( n = 1 ) , breast carcinoma ( n = 1 ) , thyroid carcinoma ( n = 2 ) and multiple myeloma ( n = 7 )  . 
undici pazienti ( 9 donne e 2 uomini ) , con et media di 68 anni ( range 5882 ) , affetti da metastasi osteolitiche del soma vertebrale associate a dolore resistente ai trattamenti conservativi standard , sono stati sottoposti allutilizzo combinato di rf e cp in anestesia generale . 
il dolore significativamente diminuito dopo il trattamento : il valore medio era di 8 ( range 710 ) prima del trattamento , passando a 1 , 8 ( range 03 ) 72 ore dopo il trattamento e quindi a 1 , 9 ( range 13 ) a 6 settimane dalla procedura . 
la procedura si dimostra sicura , permettendo di ottenere una significativa riduzione del dolore , un effetto di stabilizzazione del corpo vertebrale ed un miglioramento della qualit di vita . parole chiave metastasi vertebrali cifoplastica radiofrequenza introduction introduzione painful spinal metastases usually occur in malignant neoplastic disease . 
until now , treatments for bone metastases have been mainly conservative , such as high doses of analgaesics , radiotherapy , chemotherapy , hormone therapy , and bisphosphonates ; however , results are sometimes transient and ineffective . surgery could be indicated only in the presence of neurological involvement [ 59 ]  . 
recently , percutaneous procedures such as radiofrequency ( rf ) , vertebroplasty ( vp ) and kyphoplasty ( kp ) have been introduced as palliative techniques to treat painful vertebral metastasis [ 1027 ]  . 
rf , initially performed as an effective method for treating malignant and benign tumours in several organs , has been also applied recently alone or in association with vp [ 2327 ]  . 
the aim of performing rf before cementoplasty in spinal metastasis is to destroy tumour tissue by favouring central necrosis and vessel thrombosis and thereby minimising procedure - related complications [ 24 , 26 , 27 ]  . recently , kp has been introduced as an alternative to vp . the creation of a cavity inside the vertebral body allows a low - pressure injection of high - viscosity cement and reduces the risk of cement leakage [ 3 ]  . 
 rf with thermal tumour ablation and vessel thrombosis [ 26 , 27 ] and kp with low - pressure injection in a preformed cavity [ 3 , 22 ] could both reduce the risk of leakage . 
 the aim of our study was to assess the safety and efficacy of combined rf and kp in managing painful osteolytic le metastasi vertebrali dolorose sono solitamente un aspetto altamente debilitante della patologia neoplastica maligna e rappresentano un problema estremamente complesso da affrontare . 
sino ad ora trattamenti per le metastasi ossee , quali alti dosi di analgesici , radioterapia , chemioterapia , ormonoterapia , bifosfonati , sono stati principalmente conservativi e talvolta transitori ed inefficaci , limitando il ricorso alla chirurgia solo in presenza di un coinvolgimento neurologico [ 59 ]  . 
recentemente si assistito allintroduzione di nuove tecniche mini - invasive , quali la radiofrequenza ( rf ) , la vertebroplatica ( vp ) e la cifoplastica ( cp ) , come tecniche palliative percutanee di trattamento del dolore nelle metastasi vertebrali [ 1027 ]  . 
la rf , inizialmente utilizzata come efficace metodo di trattamento di lesioni tumorali in vari distretti anatomici , stata successivamente applicata nel trattamento del dolore da metastasi vertebrali da sola o in associazione alla vp [ 2327 ]  . 
lo scopo dellutilizzo della rf nella vertebra patologica prima della fase di cementoplastica di realizzare la distruzione del tessuto tumorale attraverso la necrosi centrale della lesione e la trombizzazione dei vasi permettendo pertanto una riduzione delle possibili complicanze correlate alla procedura [ 24 , 26 , 27 ]  . 
la creazione di una cavit allinterno del soma vertebrale permette liniezione di cemento a maggior viscosit e a pi bassa pressione , riducendo il rischio di stravaso di cemento [ 3 ]  . 
 la rf con lablazione termica del tumore e la trombosi vascolare [ 26 , 27 ] associata alla cp con la possibilit di iniezione di cemento ad alta viscosit e a bassa pressione [ 3 , 22 ] potrebbero ridurre il rischio di stravaso di cemento . questo rappresenta un aspetto importante in presenza di un difetto della parete e quando la lesione tumorale localizzata a stretto contatto con le principali strutture vascolari e nervose . 
in letteratura non sono radiol med ( 2010 ) 115 : 261271 vertebral body metastases unresponsive to conservative treatments . materials and methods this study was approved by our investigator review board , and informed consent was obtained in all cases . 
in the last 3 years , 11 patients ( 9 women and 2 men ) , with a mean age of 68 years ( range 5882 ) and painful osteolytic vertebral body metastases were treated with combined rf with kp . 
we used a mini - open anterolateral cervicotomy at the cervical level and a posterior percutaneous approach at the thoracic and lumbar levels ( extrapedicular approach at thoracic levels above t10 and transpedicular approach below t10 )  . 
the kyphoplasty balloon was then deflated and removed to allow injection of the cement into riportate esperienze cliniche riguardanti lutilizzo combinato della rf con cp per il trattamento del dolore correlato alle metastasi vertebrali . scopo di questo studio valutare sicurezza ed efficacia dellutilizzo combinato di rf e cp nel trattamento del dolore correlato a lesioni osteolitiche metastatiche del soma vertebrale resistente ai trattamenti conservativi . materiali e metodi questo studio stato approvato dal comitato etico ed il consenso informato stato ottenuto in tutti i casi . 
negli ultimi tre anni , 11 pazienti ( 9 donne e 2 uomini ) , con et media di 68 anni ( range 5882 ) , affetti da lesioni osteolitiche metastatiche dolorose del corpo vertebrale , sono stati trattati associando la rf alla cf . criteri di inclusione erano la presenza di lesioni osteolitiche del corpo vertebrale determinanti un dolore resistente ai comuni trattamenti conservativi ed un indice di karnofsky superiore a 30 [ 28 ]  . 
criteri di esclusione sono stati la presenza di metastasi con invasione del canale vertebrale o linfiltrazione di strutture anatomiche importanti ( vasi , nervi , ecc . ) , levidenza di un coinvolgimento neurologico , infezione e coaugolopatie non correggibili . 
abbiamo utilizzato la risonanza magnetica ( rm ) e la tomografia computerizzata ( tc ) al fine di ottenere una migliore definizione morfologica della lesione . le procedure sono state effettuate in anestesia generale e con monitoraggio neurofisiologico intraoperatorio . 
la temperatura emessa dagli elettrodi stata progressivamente innalzata fino al raggiungimento di una temperatura ottimale compresa fra 80c e 100c per un tempo di ablazione dipendente dalle dimensioni della lesione . 
il palloncino stato progressivamente insufflato fino al table 1 demographic and clinical data case age ( years ) primary neoplasm vertebral level time rf + kp ( min ) cement volume ( ml ) leakage vas : pre 72 h 6 weeks radiol med ( 2010 ) 115 : 261271 kidney multiple myeloma breast multiple myeloma thyroid multiple myeloma multiple myeloma multiple myeloma multiple myeloma thyroid multiple myeloma rf , radiofrequency ; kp , kyphoplasty ; vas , visual analogue scale ; m , male ; f , female the cavity . 
patients were asked to rate their average pain during the past week ( 0 no pain ; 10 the worst imagined ) and then 72 h and 6 weeks after treatment . 
le varie fasi di iniezione del cemento sono state effettuate con lausilio dellamplificatore di brillanza visualizzando la vertebra da trattare sia in proiezione latero - laterale che antero - posteriore . 
in tali pazienti abbiamo utilizzato diversi tipi di cemento : kyphx ( kyphon , usa ) o cemex ( tecres spa , verona , italia )  . il dolore stato valutato utilizzando una scala analogica di dolore ( vas score , 010 )  . 
i pazienti sono stati intervistati per valutare il valore medio del dolore durante la settimana precedente la procedura ( 0 , assenza di dolore ; 10 dolore insopportabile ) , e nel post - operatorio a 72 ore ed a 6 settimane . 
the time interval between symptom onset and surgical treatment ranged from 1 to 4 ( mean 3 ) months . combined rf and kp were well - tolerated by all patients . 
mean procedure time was 53 ( range 4565 ) m the average injected cement undici vertebre con osteolisi metastatiche dolorose del corpo vertebrale sono state trattate con lutilizzo combinato di rf e cp ( tabella 1 )  . 
le neoplasie primitive erano di origine renale ( 1 caso ) , mammaria ( 1 caso ) , tiroidea ( 2 casi ) , mielomatosa ( 7 casi )  . 
lintervallo intercorso tra linizio dei sintomi e lintervento chirurgico era compreso tra 1 e 4 mesi ( media 3 mesi )  . la procedura combinata di rf e cp stata ben tollerata da tutti i pazienti . 
allindagine tc eseguita nel post - operatorio abbiamo evidenziato in 1 caso uno stravaso di cemento allinterno dello spazio intervertebrale ( tabella 1 , caso 6 )  . il follow - up medio stato di 12 mesi ( range 418 )  . 
il volume medio di cemento iniettato per vertebra era di 6 , 7 ml ( range 39 ) ( tabella 1 )  . il livello del dolore significativamente diminuito dopo il trattamento : il valore medio era di 8 ( range 710 ) prima del trattamento , passando a 1 , 8 ( range 03 ) 72 ore dopo il trattamento e quindi a 1 , 9 ( range 13 ) a 6 settimane dalla procedura . 
abbiamo documentato una significativa riduzione nellassunzione di farmaci analgesici in tutti i pazienti . al momento dellanalisi finale dei dati , 5 pazienti sono deceduti per problemi non correlati alla nostra procedura . discussion discussione combination therapy with rf ablation and kf is a new treatment for painful bone metastases . 
rf is used successfully in many organs affected by cancer and is also receiving an increasing interest in neoplastic musculoskeletal diseases , its use being widened to treat osteoid osteomas , and as palliative sintomatologia dolorosa correlata alle metastasi vertebrali spesso uno degli aspetti pi debilitanti della patologia neoplastica maligna . 
i trattamenti conservativi standard del dolore vertebrale includono luso di farmaci analgesici , la chemioterapia , la radioterapia , il riposo , limmobilizzazione con busto , limitando la decompressione e la stabilizzazione chirurgica solamente in presenza di un coinvolgimento neurologico [ 59 ]  . 
la radioterapia rimane il trattamento palliativo standard per le metastasi vertebrali dolorose . attualmente la rf viene utilizzata con successo in molti organi colpiti da neoplasie e sta ricevendo un interesse crescente anche nellambito della patologia neoplastica muscolo - scheletrica avendo allargato il suo utilizzo al 268 radiol med ( 2010 ) 115 : 261271 fig . 
necrosis of the metastatic lesion and destruction of sensory nerve fibers in the periosteum and bone cortex induced by the elevated temperature represent the mechanisms through which the analgaesic effect is achieved [ 2327 ]  . 
la necrosi della lesione tumorale e la distruzione delle fibre nervose sensitive periostali e della corticale ossea indotte dallelevata temperatura , rappresentano i meccanismi attraverso i quali si esplica leffetto analgesico [ 2327 ]  . 
 [ 23 ] , su un totale di 45 pazienti con metastasi ossee trattati con rf , riportano una significativa riduzione del dolore e relativo decremento nellassunzione giornaliera di analgesici . 
 [ 25 ] , su un totale di 10 pazienti trattati con rf , riportano una riduzione del dolore del 74% ad un follow - up medio di 6 mesi , con completa risoluzione del dolore in 3 casi radiol med ( 2010 ) 115 : 261271 fig . 
espansione dellago nellemisoma ( a , b ) e iniezione di cemento nel corpo vertebrale ( c , d )  . complications related to the procedure [ 25 ]  . 
however , in the presence of an impending fracture or a pathological compression fracture , cement augmentation is necessary . vp allows rapid and lasting analgesic effect [ 10 , 13 , 14 ] , probably by means of mechanical and chemical effects . cement augmentation seems to promote mechanical stability of the pathological vertebral body by reducing micromovements responsible for pain and the progression of vertebral collapse . 
other hypotheses for the effect of vp are destruction of nerve endings by the exothermic reaction during the phase of polymerisation [ 11 , 14 , 16 , 18 ]  . 
vp demonstrated effective pain relief but has the potential drawback of cement leakage , which might occur during the injection in up to 70%75% of patients ; however , the vast majority of these leaks are asymptomatic . 
tuttavia , in presenza di un elevato rischio di frattura o di un evento fratturativo del corpo vertebrale , si rende indispensabile offrire sostegno al soma vertebrale con lutilizzo del cemento . 
leffetto di sostegno indotto dal cemento sembra promuovere il ripristino di una stabilit meccanica del corpo vertebrale patologico riducendone i micro - movimenti responsabili del dolore e del progressivo collasso vertebrale . 
altre ipotesi relative alleffetto analgesico indotto dalla vp includono la distruzione delle fibre terminali nocicettive indotte dalla reazione termica del cemento durante la fase di polimerizzazione [ 11 , 14 , 16 , 18 ]  . 
la vp si dimostrata efficace nel ridurre il dolore , a scapito per di un potenziale rischio di stravaso di cemento al momento delliniezione che si realizza dal 70% al 75% dei casi ; tuttavia , la maggior parte di questi stravasi sono asintomatici . 
lo stravaso venoso , particolarmente se si realizza allinterno della vena cava inferiore , stato riportato come causa di embolia 270 radiol med ( 2010 ) 115 : 261271 neuroforaminal veins or extravasation into the foramina may lead to radiculopathy , which is the major risk of this procedure [ 10 , 1622 ]  . 
the creation of a cavity inside the vertebral body allows the injection of cement at low pressure and higher viscosity and offers the advantage of reducing the risk of cement leakage [ 3 ]  . 
asymptomatic cement leakage occurred in seven patients : in five cases , the leakage was into the venous plexus and in two into the spinal canal through a posterior wall defect [ 26 ]  . in our experience , the procedures were safe and provided pain relief with bone augmentation and improved quality of life . 
the combination of rf , with thermal ablation and vessel thrombosis , and kp , with low - pressure injection of high - viscosity cement in a preformed cavity , reduced the risk of leakage . 
lo spandimento del cemento allinterno dei plessi venosi epidurali o neuroforaminali , o lo stravaso allinterno dei forami , possono determinare linsorgenza di radiculopatie , che rappresentano il maggior rischio connesso alla procedura [ 10 , 1622 ]  . 
la creazione di una cavit allinterno del corpo vertebrale permette liniezione di cemento a pi bassa pressione ed a maggior viscosit , riducendo il rischio di stravaso di cemento [ 3 ]  . 
 [ 3 ] hanno utilizzato la cp in 52 pazienti con mieloma multiplo in 242 vertebre ; stravasi di cemento , sempre asintomatici , si sono verificati nel 5% delle vertebre trattate . 
 [ 22 ] hanno utilizzato la cp in 18 pazienti affetti da mieloma multiplo per un totale di 55 vertebre trattate ; stravasi di cemento , sempre asintomatici , si sono verificati nel 4% dei casi . 
 [ 26 ] hanno riportato una casistica di 12 pazienti affetti da dolore da metastasi vertebrale con difetto osseo del muro posteriore trattati con lutilizzo combinato di rf e vp . le procedure sono state eseguite con successo in tutti i pazienti senza relative complicanze correlate . 
in 5 casi lo stravaso avvenuto allinterno dei plessi venosi e in 2 casi allinterno del canale vertebrale attraverso il difetto osseo del muro posteriore [ 26 ]  . nella nostra pratica clinica la procedura si dimostrata sicura , permettendo di ottenere una significativa riduzione del dolore , un effetto di sostegno del corpo vertebrale ed un miglioramento della qualit di vita . 
la rf , con lablazione termica del tessuto tumorale e la trombosi vascolare , e la cf , attraverso liniezione di cemento a bassa pressione allinterno di una cavit neoformata , hanno ridotto il rischio di stravaso del cemento . 
il ricorso allo studio preoperatorio con tc si ritiene necessario nei casi in cui lanatomia ossea sia sospetta per una frattura o per un difetto corticale del muro posteriore . conclusions conclusioni rf combined with kp represents a potential alternative method for palliation of painful osteolytic vertebral body metastases in selected patients . 
le procedure sono sicure ed in grado di ottenere la riduzione del dolore , il ripristino del volume osseo e di conseguenza il miglioramento della qualit di vita del paziente . 
tali metodiche devono essere prese in considerazione come trattamento palliativo a seguito dellinsuccesso della terapia convenzionale , ma tuttavia con indicazioni radiol med ( 2010 ) 115 : 261271 selection for the procedure , evaluating carefully site , and pain intensity . 
la dimostrazione radiologica della morfologia della lesione e dellinvasione dei tessuti molli ad essa adiacenti indispensabile : deve infatti essere tenuto in considerazione che tali procedure , bench minimamente invasive , non sono esenti da complicanze potenzialmente temibili . 
pavlica1 1uo di radiologia , dipartimento emergenza / urgenza , chirurgia generale e dei trapianti , azienda ospedaliero - universitaria di bologna , bologna , italy 2uo di radiologia urgenza ed emergenza , dipartimento ad attivit integrata di diagnostica per immagini , azienda ospedalierouniversitaria careggi di firenze , firenze , italy correspondence to : l . 
barozzi , uo di radiologia , policlinico s.orsola - malpighi , via massarenti 9 , 40138 bologna , italy , tel . : + 39 - 051 - 6364433 , e - mail : libero.barozzi@aosp.bo.it received : 11 march 2009 / accepted : 27 march 2009 / published online : 15 january 2010 springer - verlag 2010 abstract a key problem in clinical practice and research regards effective communication and comparison of results . 
we therefore tried to adapt the document on the standardisation of terminology of lower urinary tract function prepared by the international continence society for radiologists who need to acquire some basic clinical experience in the interpretation of the symptoms and signs encountered during simple urodynamic studies in order to increase the effectiveness of imaging studies of the lower urinary tract in men and women . keywords lower urinary tract clinical uroradiology riassunto uno dei maggiori problemi presenti nella pratica clinica e nella ricerca scientifica rappresentato da una efficace comunicazione dei risultati e del loro confronto . 
ci particolarmente difficile nei pazienti con disfunzione delle basse vie urinarie nei quali necessario il confronto tra specialit diverse che usano definizioni e termini differenti . noi abbiamo quindi cercato di adattare il documento sulla standardizzazione della terminologia del basso apparato urinario preparato dalla societ internazionale della continenza ad uso dei radiologi che devono acquisire la minima esperienza clinica per poter interpretare i sintomi e i segni presenti nelle indagini urodinamiche al fine di migliorare lefficienza delle loro indagini in questo campo . parole chiave vie urinarie inferiori radiourologia clinica introduction premessa the ageing of the population has led to a significant increase in lower urinary tract dysfunction ( lutd ) both in men and women . 
clinical research and new diagnostic and therapeutic procedures have prompted numerous studies investigating the association between linvecchiamento della popolazione ha comportato un aumento significativo dei disturbi a carico del basso apparato urinario sia nel sesso maschile che femminile . 
le ricerche cliniche e le nuove procedure diagnostiche e terapeutiche hanno dato origine a numerosi radiol med ( 2010 ) 115 : 272286 signs and symptoms and evaluating the effectiveness of various treatments . 
to be in a position to evaluate diagnostic utility and therapeutic results in different centres and countries , the international continence society published a report titled standardisation of terminology of lower urinary tract function [ 1 ]  . 
we believe that at least a partial and concise publication of this report can be useful to the radiologist whose task it is to examine patients who complain of lutd , in that it can provide diagnostic guidance , help in better understanding the clinical query made by the urologist and therefore guide the radiologist to search even for those minor signs that often go undetected or are underestimated by radiologists without the appropriate clinical grounding . 
the information in question is generally not found in radiology textbooks , whereas it can be found in almost all studies published in urology journals . the aim of this paper is to open up clinically oriented discussion , which is often overlooked by the radiologist involved in heavy technology . 
such an approach in clinical practice should take on increasing importance if we wish to acquire greater visibility with the patient , improve the doctorpatient relationship , relate on a par with other specialists and not simply remain seated in front of the monitor in the reporting room . the definitions used in the report are in compliance with the publication of the international classification of functioning , disability and health of the world health organization ( who ) ( 2001 ) [ 2 ] and the international classification of diseases ( icd 10 )  . report studi , nei quali stata indagata lassociazione tra segni e sintomi e valutata lefficacia dei diversi trattamenti . 
per poter valutare lutilit diagnostica ed i risultati terapeutici in diversi centri e paesi , la societ internazionale della continenza ha ritenuto necessario pubblicare un documento sulla standardizzazione della terminologia utilizzata per definire e studiare le funzioni del basso apparato urinario [ 1 ]  . 
riteniamo che la pubblicazione , almeno parziale e sintetica di questo documento possa essere utile al radiologo che deve indagare pazienti che riferiscono disturbi del basso apparato urinario , per un orientamento diagnostico , per capire meglio il quesito clinico postogli dallurologo e quindi indirizzare le sue indagini e ricercare anche quei segni minori che spesso sfuggono o vengono sottovalutati dal radiologo che non possiede basi cliniche adeguate . 
si tratta di informazioni che in genere non vengono riportate sui libri di radiologia , mentre si trovano in quasi tutti i lavori pubblicati su riviste di urologia . lo scopo di questo lavoro quello di iniziare un discorso di tipo clinico che spesso viene trascurato dai radiologi impegnati nelle tecnologie pesanti . 
tale approccio nella pratica clinica assume sempre maggiore importanza se vogliamo acquisire una visibilit nei confronti del paziente , migliorare il rapporto medico - paziente , confrontarci professionalmente con gli altri specialisti e non rimanere seduti davanti ai monitor nelle sale di refertazione . le definizioni usate nel documento sono conformi con la pubblicazione dellinternational classification of functioning , disability and health dellorganizzazione mondiale della sanit ( oms ) ( 2001 ) [ 2 ] e la international classification of disease ( icd 10 )  . the report is divided into five parts ( only some will be dealt with extensively ) : documento lower urinary tract symptoms ( luts ) symptoms are defined as the subjective indicator of a disease or change in a condition as perceived by the patient , carer or partner , and may lead him / her to seek help from health care professionals . 
in most cases , luts cannot be used to reach a definitive diagnosis , and it should be borne in mind that the same symptoms may be indicative of conditions not attributable to lutd . signs suggestive of lutd signs are defined as being observed by the physician including simple means , to verify symptoms and quantify il documento costituito da 5 aree tematiche ( saranno riportate in extenso solo alcune ) e sono le seguenti : sintomi a carico del basso apparato urinario ( lower urinary tract symptoms o luts )  . i sintomi sono indicatori soggettivi di malattia o di un cambiamento dello stato di salute percepito dal paziente o riferito dal partner o da qualcuno che si prende cura del paziente ( badante ) , per cui il soggetto si presenta o viene accompagnato dal medico . 
the incontinence should be further defined with regard to frequency , severity , precipitating factors , social impact , effect on hygiene and quality of life and should be distinguished from sweating or vaginal discharge stress urinary incontinence : complaint of involuntary leakage on effort or exertion , or on sneezing or coughing urge urinary incontinence : involuntary leakage of urine associated with the compelling desire to urinate i segni sono rilevati dal medico durante la visita e a volte possono essere quantificati . 
sintomi a carico del basso apparato urinario ( luts ) sono i disturbi riferiti dal paziente o da chi si prende cura di lui , che hanno portato ad interpellare il medico . 
essa non deve essere confusa con perdite vaginali o sudorazione . incontinenza urinaria da stress , il sintomo che si riferisce alla perdita involontaria di urina che compare in corso di sforzi fisici , starnuti o tosse . incontinenza urinaria da minzione imperiosa ( urge urinary incontinence ) , riguarda la perdita involontaria di urina preceduta o associata allo stimolo impellente di urinare . incontinenza urinaria di tipo misto , riguarda quel disturbo caratterizzato sia dalla perdita di urina in seguito a sforzo o tosse sia dalla comparsa di stimolo minzionale impellente associato alla perdita di urina . enuresi : definisce qualsiasi perdita involontaria di urina ( diurna o notturna ) ed sinonimo anche di incontinenza urinaria . enuresi notturna , si riferisce solo ai casi di perdita c . 
reduced : when the individual is aware of bladder involontaria di urina durante il sonno . filling but does not feel a definite desire to void incontinenza urinaria continua , il disturbo caratterizd . 
in women , a vaginal examination may be done to evaluate elements such as situation of the perineal plane , degree of pelvic - organ prolapse or to characterise masses of the lower abdomen . 
the utility of the physical examination increases with the experience of the operator , so it is therefore desirable that it be performed on a routine basis by all radiologists who are intent on specialising in clinical genitourinary radiology . 
segni indicativi di una disfunzione del basso apparato urinario ( lutd ) 2.1 misurazione di frequenza , entit ed impatto clinico dei sintomi del basso apparato urinario . si tratta di sintomi di solito raccolti dal paziente per alcuni giorni e riportati in una specie di diario clinico , che si riferiscono essenzialmente al processo minzionale . 
essi comprendono : diario orario delle minzioni , vengono segnati gli orari delle minzioni per almeno 24 ore . diario del volume minzionale , vengono misurati i volumi e gli orari delle singole minzioni per almeno 24 ore . diario vescicale , si registrano gli orari ed i volumi minzionali , gli episodi di incontinenza , il consumo dei pannolini e la quantit di liquidi assunti , lentit dellurgenza e il grado di incontinenza per almeno 24 ore . da questi diari raccolti dal paziente o da altre persone si possono ottenere le seguenti misurazioni : frequenza minzionale diurna : numero delle minzioni durante il periodo di veglia . nicturia : numero di minzioni durante il sonno notturno . frequenza minzionale nelle 24 ore . volume urinario nelle 24 ore . poliuria : si intende quando la produzione di urina superiore a 2 , 8 litri nelle 24 ore nelladulto . volume urinario notturno : quantit di urina prodotta durante il sonno . 
esclusa lultima minzione quando si va a dormire , ma inclusa la minzione di quando ci si alza . poliuria notturna , quando la quantit di urina prodotta nelle 8 ore di sonno superiore ad 1 / 3 della quantit di urina prodotta nelle 24 ore . volume massimo minzionale : indica il volume massimo che viene raccolto in una singola minzione . 278 radiol med ( 2010 ) 115 : 272286 and can be quantified using the oxford grading scale from 1 to 5 . 
urodynamic observations and conditions urodynamic studies have become an essential part of the physical examination in patients with lutd and serve to demonstrate certain clinical signs and symptoms or to detect others . 
it indicates the pressure exerted by the abdominal organs on the bladder detrusor pressure : the component of intravesical pressure exerted by passive and active forces of the detrusor muscle . 
sono in genere di competenza urologica e raramente il radiologo ne coinvolto se non nella esplorazione rettale prima dellecografia o della inserzione della bobina endorettale in risonanza magnetica ( rm )  . 
lutilit di una valutazione clinica aumenta con lesperienza delloperatore , per cui auspicabile venga eseguita di routine da parte di tutti i radiologi che intendano cimentarsi con la radiologia urogenitale clinica . 
dati e situazioni urodinamiche gli studi urodinamici fanno ormai parte integrante dellesame obiettivo nei pazienti con disturbi a carico del basso apparto urinario e servono per oggettivare certi segni o sintomi clinici o per evidenziane altri . 
primo stimolo minzionale : quel sintomo rilevato dal paziente durante la cistometria di riempimento , quando avverte il desiderio di mingere ma la minzione pu essere rimandata o inibita ; c . 
intenso stimolo alla minzione : esprime un intenso e persistente stimolo alla minzione , ma non associato alla sensazione di perdere lurina . aumentata sensibilit vescicale , viene definita come una fig . 
i parametri valutati sono : a pressione addominale ( pad ) che viene misurata con una sonda endorettale e registra le modificazioni della pressione endoaddominale dovute ad incrementi pressori nelladdome ( ponzamento , tosse ) ; b pressione vescicole ( pv ) registra la pressione allinterno della vescica mediante sonda endovescicale ; c pressione detrusoriale ( pdet ) esprime la reale pressione endovescicale e si ottiene sottraendo alla pressione endovescicale la pressione endoaddominale ; d tracciato del flusso urinario ( q ) ; e pressione di apertura ( pa ) : valore di pressione endovescicale registrata allinizio del flusso ; f pressione detrusoriale o intravescicale massima ( pim ) : definisce la massima pressione detrusoriale durante il processo menzionale ; g flusso urinario massimo ( qmax ) il flusso massimo registrato durante la minzione ( pfm ) ; h tempo di apertura ( ta ) esprime il tempo e le variazioni di pressione endovescicali durante la contrazione isovolumetrica prima dellinizio del flusso . 280 radiol med ( 2010 ) 115 : 272286 of bladder distension b . 
first desire to void : the feeling , during filling cystometry , that would lead the patient to pass urine at the next convenient moment , but voiding can be delayed if necessary c . 
this moment is clearly indicated on the urodynamic trace , and all other detrusor activity recorded prior to it is defined as involuntary detrusor activity . normal detrusor function : allows progressive bladder filling without or with minimal increase in intravesical pressure . 
idiopathic detrusor overactivity ( overactive bladder ) : indicates where the cause cannot be identified and replaces the term detrusor instability 3.2.3 bladder compliance during filling cystometry bladder compliance : the relationship between change in bladder volume and change in detrusor pressure . 
questo momento viene chiaramente indicato sul tracciato cistometrico e tutte le attivit detrusoriali registrate in precedenza vengono definite come attivit detrusoriali involontarie . funzionalit detrusoriale normale : consente una progressiva distensione della vescica senza o con minimo aumento della pressione endovescicale . 
cystometric capacity is the volume voided together with any residual urine maximum cystometric capacity : measures bladder volume when the individual feels a strong desire to void , whereby micturition cannot be delayed maximum anaesthetic bladder capacity 3.2.5 urethral function during filling cystometry . during bladder filling , variations in the mechanism of urethral closure occur : normal urethral closure mechanism : positive urethral closure pressure is maintained during bladder filling , even in the presence of increased abdominal pressure incompetent urethral closure mechanism : one which allows leakage of urine in the absence of a detrusor contraction urethral relaxation incontinence : leakage due to urethral relaxation in the absence of raised abdominal pressure or detrusor overactivity urodynamic stress incontinence : the involuntary fig . 
la massima pressione di chiusura uretrale ( mucp ) data dalla differenza tra pressione uretrale massima ( 120 cmh2o ) e pressione vescicole ( 20 cmh2o )  . leakage of urine during increased abdominal pressure , in the absence of a detrusor contraction . 
urethral pressure profile : a graph indicating the intraluminal pressure along the length of the urethra c urethral closure pressure profile : obtained by subtracting the intravesical pressure from the urethral pressure d . 
quando la minzione continua questo tempo equivale al tempo di flusso . tempo di flusso , il tempo durante il quale si misura il flusso continuo . radiol med ( 2010 ) 115 : 272286 3.3.1. 
il valore della pressione misurata funzione delle resistenze che lurina incontra durante la minzione . closing pressure : pressure measured at the end of the attivit detrusoriale anomala , viene distinta in : measured flow measurable flow minimum voiding pressure : lowest pressure during flow delay : time elapsed between the variations in bladder pressure and the corresponding variations in flow rate 3.3.3 detrusor function during voiding . normal detrusor function : normal voiding is obtained by voluntary detrusor contraction , which leads to complete bladder emptying in a normal time and in the absence of obstruction . 
postvoid residual : the volume of urine left in the bladder at the end of micturition ( this can be easily quantified radiologically or sonographically ) 3.3.4 urethral function during voiding . normal urethral function : a urethra that opens , and is continuously relaxed to allow the bladder to be emptied at a normal pressure abnormal urethral function : may be due to a number of causes , such as urethral overactivity or a urethra that cannot open due to an anatomical abnormality a . 
condizioni cliniche ritenzione acuta di urina , viene definita una vescica distesa , dolente e palpabile , per incapacit del paziente a vuotarla . ritenzione urinaria cronica , condizione clinica con vescica distesa , palpabile , ma non dolorosa . 
trattamenti conclusioni le definizioni si trovano nel 7 ics report [ 3 ] sulle tecniche di riabilitazione del basso apparato urinario e non verranno prese in considerazione in questa sede . la necessit della standardizzazione della terminologia utilizzata per definire , diagnosticare e trattare i disturbi a fig . 
conditions acute retention of urine : a painful , palpable or percussible bladder , when the patient is unable to pass urine chronic retention of urine : a nonpainful bladder , which remains palpable or percussible after the patient has passed urine . 
6a , b ostruzione sottovescicale in bambina da dis - sinergia detrusorestriato per contrazione involontaria della muscolatura striata periuretrale . cistouretrografia minzionale ( a ) e radiogramma dopo minzione ( b )  . 
micturition appears altered and lacks formation of the normal or cone - shaped orifice due to failed relaxation of the neck , which protrudes in the shape of a cleft lip from the posterior profile of the bladder neck ( arrow )  . 
la minzione appare alterata con mancata formazione del cono minzionale per mancato rilasciamento del collo che protrude sotto forma di labbro ( cleft ) da profilo posteriore del collo vescicale ( freccia )  . 
luretra prostatica risulta solo parzialmente distesa dallurina che fluisce lentamente . 286 conclusions the need for standardisation of terminology to define , diagnose and treat lutd reveals the complexity of a physiological phenomenon that is poorly understood by radiologists in that the study of physiology and pathophysiology are generally lacking in undergraduate and specialisation courses . 
the limited knowledge of urodynamic studies in particular is the reason for the difficulties encountered when interpreting the disturbances described by patients and in correctly correlating the morphological and functional features that may be observed during diagnostic imaging studies of the lower urinary tract . retrograde cystography and voiding cystourethrography are the examinations best able to study certain static or functional parameters , such as bladder volume , onset of involuntary contractions , behaviour of the bladder neck , length of detrusor contraction and site and nature of a bladder outlet obstruction that the urodynamic study is able to quantify but not localise . 
ultrasonography can also readily identify an atonic bladder in a patient with diabetes or a neurological condition . we believe that the first steps towards a clinical radiology are the most difficult , because there needs to be a change in mindset in terms of approach to the patient by seeking to not fall into the trap of superficiality mistakes . radiol med ( 2010 ) 115 : 272286 carico del basso apparato urinario , dimostra la complessit di un fenomeno fisiologico poco conosciuto dai radiologi in quanto gli studi di fisiologia e fisiopatologia sono in genere carenti sia nel corso di laurea che durante la specializzazione . 
sono soprattutto le scarse conoscenze degli studi urodinamici il motivo delle difficolt che si incontrano nellinterpretare i disturbi riferiti dai pazienti e nel correlare correttamente gli aspetti morfologici e funzionali che si possono osservare durante le indagini di diagnostica per immagini del basso apparato urinario . la cistografia retrograda e la cistouretrografia minzionale sono le indagini che meglio possono studiare certi comportamenti statici o funzionali quali la capacit vescicale , la comparsa di contrazioni involontarie , il comportamento del collo vescicale , la durata della contrazione vescicale e la sede e la natura di una condizione ostruttiva sottovescicale che lurodinamica riesce a quantificare , ma non a localizzare . 
bergman5 1department of radiology , ziekenhuizen oost - limburg , schiepse bos 6 , 3600 genk , belgium 2department of orthopedic surgery , hospital for special surgery , new york , ny 10021 , usa 3department of radiology , brigham and womens hospital , harvard medical school , boston , ma 02115 , massachusetts , usa 4department of radiology , lucas mrs / i center , stanford , ca 94305 , usa 5franklin & seidelmann radiologists , 4240 marble ridge road , el dorado hills , ca 95762 , usa correspondence to : j . 
unrestricted physiologic joint motion results in multidirectional displacement of the anatomic structures . when performing real - time magnetic resonance ( mr ) imaging of such a joint motion , continuous adjustment of the scan plane position may be required . 
the location of a small tracker device ( dedicated hardware ) placed on the patients skin overlying a joint was determined by an ultrashort mr sequence and used to automatically adjust the scan plane position prior to each dynamic - motion mr image . 
using a vertically open mr unit , this mr tracking system was applied in ten dynamic - motion mr examinations to evaluate flexion / extension manoeuvres in the weightbearing knee joint , and in ten dynamic - motion mr examinations of the shoulder joint to evaluate manoeuvres such as internal / external rotation of the humerus , stress testing of the glenohumeral joint and abduction / adduction manoeuvres . 
quando viene effettuato uno studio di risonanza magnetica ( rm ) in tempo reale di una articolazione in movimento , si pu rendere necessario un aggiustamento continuo del piano di scansione . 
la localizzazione di un piccolo sistema di posizionamento ( con hardware dedicato ) posizionato sulla cute del paziente stata determinata mediante una sequenza rm ultrarapida ; la sequenza viene utilizzata per riposizionare automaticamente il piano di scansione prima di ogni acquisizione rm dinamica . 
mediante un apparecchio rm aperto con campo magnetico verticale sono state effettuate 10 acquisizioni dinamiche in movimento di flesso - estensione sullarticolazione del ginocchio sottocarico e 10 acquisizioni dinamiche dellarticolazione della spalla per valutare le manovre di rotazione interna / esterna dellomero , le prove di stress dellarticolazione glenoomerale e le manovre di abduzione / adduzione . 
the mr tracking system to guide the slice position for each consecutive dynamic - motion mr image of the freely but slowly moving shoulder or knee joint was feasible for clinical use , providing a high percentage of useful images for each manoeuvre within a clinically acceptable time frame . keywords magnetic resonance imaging kinematic musculoskeletal imaging patellofemoral joint imaging glenohumeral joint imaging mr tracking introduction real - time dynamic - motion magnetic resonance ( mr ) imaging refers to acquiring images of an anatomic region of interest ( roi ) within a joint that is in motion . 
it is distinct from a video display of a series of mr images acquired while the joint is held static in different positions [ 14 ]  . open - configuration mr units provide the opportunity to image joints in motion : patients may move joints in an unrestricted physiologic way within the wide gantry space . 
moreover , vertically open mr units providing the option to place the patient in upright ( standing ) position have the added value of evaluating the spine and the joints of the lower limb in physiologically weight - bearing conditions [ 7 , 8 ]  . the unrestricted multidirectional motion of a joint , limb or entire body during mr imaging results in a technical challenge : how to continually adjust the position of the scan plane for imaging the moving anatomy of interest . 
the purpose of our study was to evaluate the clinical feasibility of this mr tracking system to maintain the scan plane position at a constant anatomic location within a joint or limb that is freely moving in a slow fashion . materials and methods mr tracking system the mr tracking system was developed from a real - time risultati . 
il sistema rm di guida della posizione dello strato per ogni immagine rm dinamica delle articolazioni della spalla e del ginocchio in movimento libero e lento applicabile per uso clinico consentendo di ottenere una percentuale elevata di immagini utili per ogni manovra in un periodo di tempo clinicamente accettabile . parole chiave : risonanza magnetica imaging muscoloscheletrico cinematico imaging dell ' articolazione rotuleo - femorale imaging dell ' articolazione glenoomerale mr tracking position - monitoring system used for localising the tip of invasive devices within patients bodies , such as mrcompatible intravascular catheters [ 10 ]  . 
relevant hardware components and function are explained hereafter . the mr tracking system or mr position - monitoring system uses a configuration of four hardware parts : a miniature radiofrequency coil immersed in a reservoir of dilute gadolinium diethylenetriamine pentaacetic acid ( dtpa ) ( cordis corporation , europe n.v. , waterloo , belgium ) , a signal amplifier with isolation circuit , the magnets computing system and a sun workstation ( sun microsystems , mountain view , ca , usa )  . 
 the position of the tracking coil is determined prior to the acquisition of dynamic - motion mr images by applying an ultrashort tracking mr pulse sequence ( containing a nonselective radiofrequency pulse and a readout magnetic field gradient pulse for determining the location of an mr signal source , to be repeated for each x , y and z axis ) that uses a hadamard multiplexing scheme ( reducing the acquisition of positional information to four instead of six excitations ) [ 10 ]  . 
this information is radiol med ( 2010 ) 115 : 133140 communicated to the magnets computing system , and the position of the scan plane is updated prior to the acquisition of the next dynamic - motion mr image . 
prior to entering the mr unit , all patients completed a screening form for mr contraindications , and informed consent was obtained . approval for this study was waived by the institutional review board . 
patient in upright weight - bearing position for flexion and extension study of the knee with large crown receive / transmit imaging coil ( white arrow ) around the knee , supported by pads and a strap . 
deep to the imaging coil ( white arrow ) , the tracker coil ( black arrow ) is attached to the skin over the proximal third of the patella ( inset )  . 
paziente in posizione eretta , sotto carico per lo studio in flessione e estensione del ginocchio con bobina ricevente / trasmittente ( freccia bianca ) attorno al ginocchio , supportata da cuscinetti e una cinghia . 
sotto la bobina di acquisizione delle immagini ( freccia bianca ) , la bobina del sistema di posizionamento ( freccia nera ) attaccata alla cute sopra il terzo prossimale della rotula . 
la bobina del sistema di posizionamento contenuta in un piccolo contenitore riempito con una soluzione acquosa contenente un chelato di gadolinio . 136 radiol med ( 2010 ) 115 : 133140 during active , slow flexion / extension of the knee between 0 and 45 of flexion . 
care was taken that the physiologic movement of the patients knee was not restricted by any device , and patients were allowed to move not only the knee , but also , for example , hip and body . for dynamic - motion mr imaging of the shoulder , patients were examined in the upright , sitting position . 
alternatively , the tracking coil could simply be held at the finger tips of the physician performing the dynamic shoulder exam to interactively guide the scan plane position to the desired anatomy . 
transverse mr images were obtained during internal and external rotation manoeuvres of the humerus and during anterior and posterior stress testing by a physician both in adducted arm position and in abduction and exorotation ( aber ) position ( apprehension test )  . 
unrestricted motion of the arm , shoulder and upper body in all directions was allowed within the imaging fov of the mr unit to achieve physiologic joint motion . the clinical feasibility of the mr tracker system was evaluated by analysing the number of manoeuvres performed , the number of mr images per manoeuvre obtained and the percentage of useful mr images per manoeuvre . 
a manoeuvre was considered completely imaged if at least four useful images were acquired ( equally spread over the range of motion for each phase of that manoeuvre )  . 
 discussion imaging osteoarticular relationships during joint motion may be used to study the normal biomechanics of a joint but also to help the clinician visualise abnormal joint biomechanics when clinical examination is abnormal or equivocal . real - time mr imaging of moving joints , i.e. 
to evaluate the relative change in position of bony structures , mr images should be acquired at a constant anatomic level through one of the bony structures of the joint . 
however , physiologic joint motion with or without weight - bearing conditions involves motion not only of the joint itself , but also of the limb , adjacent joints and often the entire body of the patient . 
consequently , if one aims to image a truly physiologically moving joint , the position of the scan plane needs to be adjusted continuously . mr tracking systems were initially developed to determine the position of devices inside or outside the patient in order to update pulse sequence parameters and slice position in real time [ 11 , 12 ]  . 
applications for mr tracking include tracking the tip of intravascular catheters , tracking devices for mr - guided biopsy and tracking of mr - guided nasogastric tube placement [ 13 , 14 ]  . 
the technical challenge to track the freely moving joint within the mr unit and guide the imaging scan plane to a constant anatomic position within the joint has been overcome using an external mr tracker coil with an internal spin source [ 9 , 15 ]  . 
imaging planes perpendicular to the main direction of joint motion ( through - plane motion ) required a higher repetition of manoeuvres and resulted in lower percentage of useful mr images compared with imaging planes parallel to the main direction of joint motion ( in - plane motion )  . 
2a - c axial dynamic - motion mr images of the knee ( patellofemoral joint ) during flexion with and without use of the mr tracking system in a 26 - year old woman . 
therefore , the position of the initial scan plane ( solid line ) through the extended knee joint does not coincide with the optimal scan plane position ( dashed line ) through the same anatomic area of the patella in higher degrees of flexion . 
b if mr imaging of the knee is performed without adjusting the scan plane , the patella ( p ) readily disappears from the image when the patient flexes the knee , and therefore , patellofemoral relationships cannot be visualised during flexion . 
c using the external mr tracker , the scan plane position is continuously adjusted and a consistent visualisation of the patella ( p ) at the same anatomic level is obtained during knee flexion . 
2ac immagini rm assiali in movimento dinamico del ginocchio ( articolazione femoro - rotulea ) in flessione con e senza impiego del sistema di posizionamento in una paziente di 26 anni . 
pertanto , la posizione del piano di scansione iniziale ( linea continua ) attraverso il ginocchio in estensione non coincide con il piano di scansione ottimale ( linea tratteggiata ) attraverso la stessa area anatomica della rotula in un grado maggiore di flessione . 
b se lesame rm viene effettuato senza correggere il piano di scansione , la rotula ( p ) scompare dallimmagine quando il paziente flette il ginocchio e di conseguenza , i rapporti femoro - rotulei non possono essere visualizzati in flessione . 
c utilizzando il sistema di posizionamento esterno la posizione del piano di scansione corretta di continuo per cui possibile ottenere una buona visualizzazione della rotula ( p ) allo stesso livello anatomico . 
la piccola bobina del sistema di posizionamento ( freccia bianca ) visibile allinterno dellalta intensit di segnale del contenitore posizionato sulla cute , al terzo medio della rotula . 138 table 1 results tabella 1 risultati radiol med ( 2010 ) 115 : 133140 type of manoeuvre scan plane manoeuvre repetition times number of images per manoeuvre useful images ( % ) imaging timea knee joint flexion / extension flexion / extension shoulder joint endo / exorotation ap and pa stress abduction / adduction abduction / adduction sagittal transverse transverse transverse transverse coronal 1.6 ( 12 ) 5.8 ( 57 ) 2.1 ( 13 ) 3.2 ( 24 ) 5.6 ( 47 ) 4.3 ( 36 ) 12 ( 520 ) 15 ( 825 ) 8 ( 614 ) 7 ( 512 ) 18 ( 1030 ) 16 ( 1230 ) 1 min 10 s 4 min 51 s 1 min 25 s 2 min 14 s 4 min 33 s 3 min 07 s numbers are averages and ranges are shown in parentheses ap , anteroposterior ; pa , posteroanterior ; stress testing was performed both in neutral and in the abduction and exorotation ( aber ) position ( apprehension test ) aimaging time refers to total imaging time including all manoeuvres performed in this scan plane manoeuvres of the knee imaged in the transverse plane ( mainly the same through - plane motion ) , whereas manoeuvre imaged in the sagittal plane often required no repetition and yielded a high percentage of useful images ( mainly in - plane motion )  . 
in our experience , flexing the knee joint too quickly resulted in a fast downward translation of the patella out of the transverse imaging plane but not out of the sagittal imaging plane , as there is only a slight medial or lateral deviation during knee flexion . 
in a preclinical study , adequate tracking of the area of interest has been demonstrated up to speeds of 1.5 cm per second using a phantom [ 9 ]  . 
 as an alternative method to set the scan plane for mr imaging during free joint motion , others have developed an interactive scan control method : based on viewing of fluoroscopic mr images , the position of the scan plane is interactively adjusted throughout the whole kinematic mr examination [ 17 ]  . 
however , these continuous adjustments are performed manually , whereas our method is fully automated : no interaction is required to adjust the scan plane position using the mr tracking system . some limitations of the external mr tracker system need to be mentioned . 
for example , when imaging in the sagittal plane , the slice position was adjusted in a medial or lateral direction ( parallel to the original scan plane )  . however , the position of the fov within this imaging plane was not adjusted in anteroposterior or superoinferior direction . 
therefore , a fov large enough to include the joint in the mr image during the full range of motion of the performed manoeuvre needed to be chosen from the start . 
mr images of better quality to evaluate joints under stress can be obtained using static mr imaging with spin - echo t1 - weighted sequences and nonmagnetic devices applying stress to joints [ 18 ]  . 
using multiple tracker coils , not only scan plane position but also scan plane direction ( including oblique imaging planes ) probably could be adjusted , but this technique was not used [ 19 ]  . in this study , true physiologic motion of the shoulder and knee joints could be performed regarding body and limb movement in space , but motion was not physiologic regarding speed . 
the slow motion needed for real - time mr image acquisition may have some influence on joint biomechanics and could therefore obscure or overestimate abnormal joint biomechanics in some cases . other applications using the mr tracker can be developed , and other mr units can be used . 
this may include the anterior and posterior drawer tests in the knee and ankle , joint motion studies of the hip joint and the elbow joint , neer and hawkins positions of the shoulder joint , and lumbar spine motion [ 20 ]  . in conclusion , the mr tracking system to guide the slice position for each consecutive transverse , coronal or sagittal radiol med ( 2010 ) 115 : 133140 fig . 
3a - c axial dynamic - motion mr images of shoulder abduction ( glenohumeral joint ) with and without use of the mr tracking system in a 24 - year old woman . 
in the sitting position , the patient is allowed to freely move torso , shoulder and arm within the imaging field of the mr unit , which represents true physiologic motion . 
therefore , the initial position of the scan plane ( solid line ) through the glenoid in the adducted upper extremity does not coincide with the optimal scan plane position ( dashed line ) through the glenoid when the arm is abducted . 
b if the mr position of the scan plane is not adjusted , dynamic - motion mr imaging in the axial plane during abduction fails to depict the glenohumeral joint at a consistent level during the full range of motion , and the axilla rather than the glenoid ( g ) and humeral head ( h ) is imaged when the arm is abducted > 45 . 
3a - c immagini rm assiali in movimento dinamico della abduzione della spalla ( articoclazione gleno - omerale ) con e senza luso del sistema di posizionamento in una paziente di 24 anni . 
in posizione seduta , viene consentito al paziente di muovere liberamente il dorso , la spalla e il braccio allinterno del campo di immagine della apparecchiatura rm , in modo da rappresentare il vero movimento fisiologico . 
si nota che la glenoide ruota e si disloca cranialmente quando il braccio abdotto ( in relazione al normale ritmo scapolo - omerale comprendente la rotazione scapolare nei confronti della parete toracica )  . 
pertanto la posizione iniziale del piano di scansione ( linea continua ) attraverso la glenoide dellestremit superiore addotta non coincide con la posizione ottimale del piano di scansione ( linea tratteggiata ) attraverso la glenoide quando il braccio abdotto . 
b se il piano di scansione non viene corretto , le immagini rm in movimento dinamico sul piano assiale in abduzione non riescono a cogliere larticolazione gleno - omerale durante tutto larco del movimento e si visualizza lascella piuttosto che la glenoide ( g ) e la testa omerale ( h ) quando il braccio abdotto per pi di 45 . 
c utilizzando il sistema di posizionamento e applicando la bobina piccola ( freccia bianca ) alla cute che ricopre la glenoide ( g ) posteriormente , possibile aggiornare e correggere la posizione del piano di scansione in modo continuo . 
in questo modo i rapporti gleno - omerali sono evidenziati in tutto larco del movimento di abduzione . 140 radiol med ( 2010 ) 115 : 133140 mr image of the freely moving shoulder or knee joint was feasible for clinical use provided joint motion was slow enough to accommodate for the acquisition of dynamicmotion mr images . 
dose surplus due to slope - up and slope - down of prospective tube current modulation in a phantom model riduzione della dose in angiografia coronarica con tc spirale con apparecchiatura a doppia sorgente . 
cademartiri1 , 2 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands correspondence to : f . 
cademartiri , dipartimento di radiologia e diagnostica per immagine , c / o piastra tecnica , piano 0 , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703756 , fax : + 39 - 052 - 1704838 , e - mail : filippocademartiri@hotmail.com received : 13 november 2008 / accepted : 7 january 2009 / published online : 7 january 2010 springer - verlag 2010 abstract purpose . 
we used four tube current modulation algorithms : narrow pulsing window , with tube current reduction to 20% ( a ) and 4% ( b ) of peak current ; and wide pulsing window , with tube current reduction to 20% ( c ) and 4% ( d )  . 
noise was measured at each r - r step in order to identify low noise ( 100% dose ) , medium noise ( slopeup / down ) and high noise ( 4 / 20% dose )  . 
sono stati valutati 4 protocolli ecggated retrospettivo dsct - ca , acquisiti con electrocardiographic ( ecg ) - controlled tube current modulation ed ecg - pulsing heart rate - adattativo : nei due diversi protocolli , a e b , la corrente stata ridotta al 20% del massimo amperaggio al di fuori di una finestra di pulsing stretta ( a ) ed ampia ( b ) ; nei protocolli c e d , la corrente stata ridotta al 4% del massimo amperaggio al di fuori di una finestra di pulsing stretta ( c ) e ampia ( d )  . sono state calcolate le finestre di modulazione della corrente : 100% ma ( finestra di acquisizione dati ) , 4% / 20% ma ( finestra di riduzione della corrente ) , dal 4% / 20% al 100% ma , e viceversa ( slope - up / down ; finestre di transizione della corrente )  . 
for c and d , instead , the slope - up increased with progressively higher hr ( 10%25% of the r - r interval , except for 90 bpm , 10% ) , whereas the slope - down remained constant at 5% ( except for 120 bpm ; 10% )  . 
la transizione della corrente relativa alla modulazione della corrente del tubo rappresenta una costante sorgente di dose surplus nellordine del 14%34% della dose totale , con valori maggiori nei protocolli acquisiti con finestra di pulsazione stretta e modulazione al 4% del massimo amperaggio . 
 parole chiave angiografica coronarica tomografia computerizzata a doppia sorgente ( dsct ) ecg - pulsing ecg - controlled tube current modulation dose di radiazione introduction introduzione multidetector - row computed tomography ( mdct ) has become an important noninvasive diagnostic tool for coronary artery and heart disease thanks to the high diagnostic accuracy of the technique [ 13 ]  . 
as a result , algorithms have been developed that are able to modulate the radiation exposure without significantly deteriorating image quality at mdct coronary angiography ( mdctca ) [ 710 ]  . 
 a recent appearance on the market is dual - source ct ( dsct ) , which offers high temporal resolution ( 83 ms ) regardless of heart rate ( hr ) and the possibility of simultaneous evaluation of left ventricular volumes [ 1013 ]  . 
 with dsct scanners , reduced radiation exposure is achieved with two ecg - triggered systems : the first ecg pulsing varies the width of the window of maximum milliampere , whereas the second ecg - controlled tube current modulation reduces the current outside the window . 
 the aim of this study was to evaluate the impact of surplus dose derived from the transition window in dsctca acquired with two different reductions in milliampere and two different pulsing windows at different hr . la tomografia computerizzata multistrato ( msct ) diventata un importante strumento diagnostico non invasivo in corso di patologia coronarica e cardiaca [ 13 ]  . 
tuttavia , lo sviluppo di apparecchiature sempre pi performanti ( ad esempio , 64 - msct ) , comporta di regola un incremento della dose di esposizione alle radiazioni ionizzanti [ 46 ]  . questo dato rappresenta una potenziale limitazione allimpiego clinico . 
sono stati pertanto sviluppati degli algoritmi capaci di modulare lesposizione alle radiazioni senza deteriorare significativamente la qualit dellimmagine mediante angiografia coronarica msct ( msct - ca ) [ 710 ]  . la tomografia computerizzata a doppia sorgente ( dsct ) di recente implementazione permette di ottenere una risoluzione temporale costante di 83 ms indipendente dalla frequenza cardiaca e la possibilit di eseguire una simultanea valutazione dei volumi del ventricolo sinistro [ 1013 ]  . nella angiografia coronarica dsct ( dsct - ca ) , la dose desposizione modulata mediante la combinazione di due sistemi cardio - sincronizzati dellemissione del tubo radiogeno : ( ecg ) - pulsing , permette di variare la larghezza della finestra di applicazione di massimo amperaggio ; il secondo , ecg - controlled tube current modulation , permette di ridurre la corrente al di fuori della medesima finestra . 
un ulteriore e significativa riduzione di dose ottenuta dalladattamento automatico del pitch allaumentare della frequenza cardiaca [ 1320 ]  . il primo , electrocardiographic lo scopo di questo studio di valutare limpatto di dose materials and methods for this study performed on a phantom , we used a firstgeneration dsct system ( siemens medical solutions , forchheim , germany )  . dsct technology the dsct system we evaluated was equipped with two xray tubes and two detectors mounted on a rotating gantry with an angular offset of 90 . 
with both tubes operating , they provide a power of 80 kw / tube ( straton , siemens medical solution ) , whereas if only tube a is in operation , the system is comparable with a single - source 64 - slice mdct systeconventional ct dose indices can also be applied to dsct , because the doses regarding each tube are combined using a linear function . 
in fact , tube current value is calculated as the current - time product per gantry rotation ( milliampere / rotation ) with the sum of the milliampere of both x - ray tubes . 
with the use of ecg - controlled tubecurrent modulation , radiation exposure is proportional to the mean value of the current applied during the entire scan [ 1320 ]  . exposure reduction systems heart - rate - adaptive pitch the pitch increases proportionally with increasing hr . 
the pitch is determined by the lowest hr observed during prescanning monitoring . cardiac bow - tie filter radiol med ( 2010 ) 115 : 3650 relativa alla transizione della corrente in dsct - ca , acquisita con due diverse riduzioni di amperaggio e due diverse finestre di pulsing , per diversi valori di frequenza cardiaca . 
 materiali e metodi per questo studio su fantoccio stato utilizzato il sistema dsct ( siemens medical solutions , forchheim , germania ) di prima generazione . tecnologia dsct il sistema dsct valutato dotato di due tubi radiogeni e due detettori montati sulla pista di rotazione del gantry ad una compensazione angolare di 90 . 
i due tubi contemporaneamente energizzati forniscono una potenza di 80 kw / tubo ( straton , siemens medical solution ) , mentre se in funzione solo il tubo a , la performance del sistema paragonabile a quella di una 64 - msct a singola sorgente . 
infatti , il valore della corrente del tubo viene calcolato come il prodotto della corrente al secondo per il tempo di rotazione del gantry ( mas / rot ) sommando i milliamperes di entrambi i tubi quando contemporaneamente attivi . 
con lutilizzo dellalgoritmo ecg - controlled tube current modulation , la dose di radiazione proporzionale al valore medio della corrente applicata durante lintera scansione [ 1320 ]  . sistemi di risparmio della dose utilizzati pitch heart rate - adattativo il pitch aumenta parallelamente allaumento della frequenza cardiaca . 
 in cardiac imaging , the collimation system is constituted by an additional filter defined as cardiac , because it limits the field of view ( fov ) to the cardiac region . cardiac bow - tie filter ecg synchronisation ecg pulsing was introduced in mdct - ca to reduce radiation exposure by around 50% [ 1416 ]  . 
the width of the image acquisition window ( pulsing window = window with maximum tube current intensity , or 100% of milliampere ) can be manually selected before the scan on the basis of the in cardio - imaging , il sistema di collimazione costituito da un filtro addizionale definto cardiac , poich limita il campo visivo ( fov ) alla regione cardiaca . 
 modulazione cardio - sincronizzata della corrente del tubo la modulazione cardio - sincronizzata dellemissione del tubo radiogeno , o ecg - pulsing , stata introdotta in msctradiol med ( 2010 ) 115 : 3650 cardiac cycle phase where cardiac motion is at a minimum . ecg - controlled tube - current modulation can reduce the current to 20% ( analysis of left ventricular function , or functional imaging ) or to 4% ( mindose ) of the nominal value outside the pulsing window , thus at the same time reducing total radiation exposure . 
transition times from minimum to maximum milliampere ( slopeup ) and vice versa ( slope - down ) are determined by the generator power ( thermionic effect ) and by the cathode cooling system , as well as r - r interval duration . 
the aim of this study was to evaluate the component of radiation exposure derived from current transition times , surplus dose / total dose and with and without a morphofunctional evaluation of the left ventricle , with different acquisition windows and different hr . dsct and ecg - pulsing scan protocols the study was performed on an anthropomorphic cardiac ct phantom ( cardio ; qrm , mhrendorf , germany )  . 
the ecg signal was provided by an ecg simulator incorporated in the syste the common scan parameters were two x - ray tubes , 380 mas / rot with 120 kv , collimation slice 640.6 mm ( z - axis flying - focal spot ) , and gantry rotation time 330 ms . 
the pitch varied between 0.2 ( low hr ; 45 bpm ) and 0.5 ( high hr ; 120 bpm ) and was automatically adapted by the scanner to the hr used : 45 , 60 , 75 , 90 and 120 bpthe craniocaudal range of the scan was 90 mm . table 1 shows the dose modulation algorithms used . 
we performed two functional imaging protocols ( reduction to 20% of maximum milliampere outside the pulsing window ; protocols a and b ) and two mindose protocols ( reduction to 4% of maximum milliampere outside the pulsing window ; protocols c and d )  . 
la larghezza della finestra di acquisizione delle immagini ( finestra di pulsing , o pulsing window , finestra di erogazione alla massima intensit di corrente del tubo , o 100% dellamperaggio ) pu essere selezionata manualmente , prima della scansione , in corrispondenza della miglior fase dimmobilit del cuore . 
lalgoritmo ecg - controlled tube current modulation permette di ridurre la corrente al 20% ( analisi della funzionalit ventricolare , o functional imaging ) o al 4% ( mindose ) del valore nominale , al di fuori della finestra di pulsing , riducendo parallelamente lesposizione totale alle radiazioni . 
la qualit delle immagini acquisite in functional imaging permette un simultaneo studio morfo - funzione del ventricolo sinistro , mentre la modulazione al 4% permette la minima esposizione alle radiazioni [ 1320 ]  . 
i tempi di transito dal minimo al massimo valore di ma ( slope - up ) , e viceversa ( slope - down ) , sono determinati dalla potenza del generatore ( effetto termoionico ) e dal sistema di raffreddamento del catodo , nonch dalla durata dellintervallo r - r . 
lo scopo di questo studio di valutare la componente di dose relativa ai tempi di transizione della corrente , dose surplus / dose totale , con e senza valutazione morfo - funzionale del ventricolo sinistro , per diverse finestra di acquisizione e diversi valori di frequenza cardiaca . 
 protocolli di scansione dsct ed ecg - pulsing lo studio stato eseguito su un fantoccio da tomografia computerizzata ( ct ) cardiaco antropomorfico ( cardio , qrm , mhrendorf , germania )  . 
i parametri di scansione comuni sono : due sorgenti a raggi x ; 380 mas / rot ad una tensione del tubo di 120 kv , collimazione - slice 640 , 6 mm ( z - axis flying focal spot ) ; tempo di rotazione del gantry 330 ms . 
il pitch variava tra 0 , 2 ( basse frequenze ; 45 bpm ) e 0 , 5 ( alte frequenze ; 120 bpm ) , adattato automaticamente dalla macchina alle frequenze cardiache utilizzate : 45 , 60 , 75 , 90 e 120 bp il range cranio - caudale di scansione era 90 m la tabella 1 riporta gli algoritmi di modulazione della dose utilizzati . 
using the coefficient of conversion for the chest , we calculated the effective dose ( dpl0.017 , mgycmcoefficient of conversion for the chest ) ( table 2 )  . evaluation of the transition window surplus dose for each hr , we reconstructed four series of data , from 0% to 95% of the r - r interval with 5% increments , for a total of 20 data sets . 
we calculated current modulation time windows ( ms ) : data acquisition window ( 100% ma = max dose ) , current reduction window ( 4%20% ma = mindose ) , current transition windows ( slope - up and slope - down , from 4 / 20% to 100% of ma and vice versa )  . 
noise was evaluated as the sd measured within a region of interest ( roi ) , positioned at the centre of the phantom and classified as low ( 100% ma = max dose ) , medium ( slope - up / slope - down ) and cardiache ( 45 , 60 , 75 bpm ) e in telesistole ad alte frequenze cardiache ( 90 , 120 bpm )  . 
sono stati valutati il ct dose index volume ( ctdivol ) espresso in mgy , dove [ j ] [ kg - 1 ] = [ gy ] , ed il doselenght product ( dlp ) espresso in mgy / cm , quali parametri di dose assorbita durante lacquisizione delle immagini gated - retrospettive . 
utilizzando il coefficiente di conversione per il torace , stata calcolata la dose efficace ( dlp0 , 017 , mgycmcoefficiente di conversione per il torace ) ( tabella 2 )  . valutazione dose surplus relativa alla transizione della corrente per ogni valore di frequenza cardiaca sono state ricostruite 4 serie di dati , da 0% al 95% dellintervallo r - r con passo del 5% , per un totale di 20 data set . 
correlations were evaluated with tpearsons r coefficient . statistics results radiol med ( 2010 ) 115 : 3650 di riduzione della corrente ( 4%20% ma = dose minima [ min dose ] ) , finestre di transizione della corrente ( slope - up e slope - down : dal 4% / 20% al 100% di ma e viceversa )  . 
il confronto tra i valori di dose surplus e dose totale stato effettuato mediante test t di student per dati appaiati , ed una p < 0 , 05 stata considerata significativa . 
the width of the slopeup / slope - down windows is dependent on the duration of the r - r interval ( hr ) , the width of the pulsing window and the tube current modulation ( functional imaging or mindose )  . risultati evaluation of total dose table 2 shows the calculated ctdivol and dlp dose indices . 
la larghezza delle finestre di slopeup / slope - down in relazione alla durata dellintervallo r - r ( fc ) , alla larghezza della finestra di pulsazione e alla modulazione della corrente del tubo ( functional imaging o mindose )  . valutazione dose totale la tabella 2 mostra gli indici di dose ctdivol e dlp calcolati . 
in base agli studi iniziali eseguiti su apparecchiature dsct [ 2123 ] , lottimale finestra di pulsing ( vale a dire narrow pulsing window ) a bassa ed alta frequenza cardiaca permette di ridurre la dose del 29%42% ( < 65 bpm ) e del 15%34% ( 80 bpm ) , con e senza valutazione dei volumi e della massa del ventricolo sinistro , rispettivamente . 
invece , a frequenze cardiache intermedie , lottimizzazione del data set dimmagine ( mediante wide pulsing window ) corrisponde ad un aumento di dose del 23%32% . radiol med ( 2010 ) 115 : 3650 radiol med ( 2010 ) 115 : 3650 radiol med ( 2010 ) 115 : 3650 a slope up a slope down b slope up b slope down fig . 
r - r , intervallo r - r ; bpm , battiti per minuto ; slope - up , finestra di transizione della corrente dal minimo al massimo valore di ma ; slope - down , finestra di transizione della corrente dal massimo al minimo valore di ma ; fi , functional imaging ; a , narrow pulsing window functional imaging ; b , wide pulsing window functional imaging . c slope up c slope down d slope up d slope down fig . 
r - r , intervallo r - r ; bpm , battiti / minuto ; slope - up , finestra di transizione della corrente dal minimo al massimo valore di ma ; slope - down , finestra di transizione della corrente dal massimo al minimo valore di ma ; md , mindose ; c , narrow pulsing window mindose ; d , wide pulsing window mindose . evaluation of total dose valutazione della dose surplus table 3 shows the slope - up / slope - down times expressed in relative ( ms ) and absolute ( % ) terms of the r - r interval for hr of 45 , 60 , 75 , 90 and 120 bpm . dependence on duration of current modulation la tabella 3 mostra la durata dei tempi di slope - up e slopedown , espressi in valore relativo ( ms ) e assoluto ( % ) dellintervallo r - r , per le frequenze cardiache di 45 , 60 , 75 , 90 e 120 bp complessivamente , la dose surplus aumenta parallelamente allaumentare della frequenza cardiaca in base alla dose totale di esposizione . in the functional imaging protocols ( a and b ) , the transition current ( slope - up / slope - down ) had the same relative value : 10% + 10% for hr 75 bpm and 15% + 15% for hr dipendenza dalla durata della modulazione della corrente nei protocolli functional imaging ( a e b ) , la transizione della radiol med ( 2010 ) 115 : 3650 surplus dose / total dose fig . 
bpm , battiti per minuto ; a , narrow pulsing window functional imaging ; b , wide pulsing window functional imaging ; c , narrow pulsing window mindose ; d , wide pulsing window mindose . 
at higher hr ( 120 bpm ) , the slope - up / slopedown showed a different value of 25% + 15% , respectively , in relation to the shorter duration of the cardiac cycle ( 500 ms ) vs . 
 discussion dsct devices are equipped with tube current modulation tube current systems ( ecg pulsing / ecg - controlled discussione le apparecchiature dsct sono dotate di sistemi cardiosincronizzati di modulazione della corrente del tubo ( ecgpulsing / ecg - controlled tube current modulation ) [ 13 , 1720 ] heart rate - adattativi atti a ridurre al minimo radiol med ( 2010 ) 115 : 3650 modulation ) [ 1317 , 2123 ] , which are hr adaptive to minimise radiation exposure during noninvasive cardiac imaging . 
however , in pulsing acquisitions , the current transition from minimum to maximum milliampere ( slope - up ) and vice versa ( slope - down ) was not instantaneous [ 13 ]  . 
the current slope produced an additional dose of radiation ( surplus dose ) , which could be reduced by increasing the capacity of the gantrys internal circuits ( i.e. cooling system and generatorcathode circuit )  . 
to evaluate the efficiency of the ecg - controlled tube current modulation system , we acquired two different pulsing windows narrow and wide at two different current modulations ( 20% of max ma functional imaging ; 4% of max ma mindose )  . dependence on current modulation the surplus dose increased alongside increasing hr , from 45 bpm to 120 bpm , in terms of total dose . 
the surplus dose , in contrast , increased with increasing hr , from 45 to 120 bpin protocols of tube current modulation to 20% of milliampere ( a and b ) , the transition current ( slopeup / slope - down ) produced a reduction in surplus dose up to hr 75 bpm and then increased at higher hr ( i.e. 25% / 15% , 120 bpm ; b )  . 
tuttavia nelle acquisizioni pulsate , la transizione della corrente dal minimo al massimo valore di ma ( slopeup ) , e viceversa ( slope - down ) , non istantanea [ 13 ]  . 
la pendenza della corrente sottende una dose di radiazione aggiuntiva ( dose surplus ) che potrebbe essere ridotta potenziando le capacit dei circuiti interni al gantry ( vale a dire , il sistema di raffreddamento e il circuito generatorecatodo )  . 
 per valutare lefficienza del sistema ecgcontrolled tube current modulation , sono state acquisite due diverse finestre di pulsazione , narrow e wide pulsing window , a due diverse modulazioni di corrente ( 20% di max ma per il functional imaging ; 4% di max ma per il mindose )  . dipendenza dalla modulazione della corrente la dose surplus aumenta parallelamente allaumento della frequenza cardiaca , da 45 a 120 bpm , rispetto alla dose totale . 
in particolare , nei protocolli modulati al 20% al di fuori della finestra di pulsing ( a e c ) , la transizione della corrente ( slope - up / slope - down ) ha lo stesso valore relativo ( 10% + 10% ) per fc90 bpm ( a / c ) , per poi aumentare alle frequenze cardiache pi elevate ( vale a dire , 25% + 15% , 120 bpm ; b )  . 
nei protocolli di modulazione della corrente al 4% di ma al di fuori della finestra di pulsing ( b e d ) , il tempo di slope - up aumenta parallelamente allaumentare della frequenza cardiaca ( 10%25% da 45120 bpm ) , eccetto a 90 bpm ( pitch = 0 , 43 vs 0 , 40 ) ; mentre la caduta di erogazione raggi ( slope - down ) ha una durata costante ( 5% ) , eccetto a 120 bpm . dipendenza dallintervallo r - r la dose totale diminuisce allaumentare della frequenza cardiaca ( 45120 bpm )  . 
la dose surplus , invece , aumenta parallelamente allaumento della frequenza cardiaca , da 45 a 120 bpnei protocolli di modulazione della corrente al 20% di ma ( a / c ) , la transizione della corrente ( slope - up / slope - down ) determina una riduzione di dose surplus fino a fc75 bpm , per poi aumentare alle frequenze cardiache pi elevate ( vale a dire 25% + 15% , 120 bpm ; b )  . 
nei protocolli di modulazione della corrente al 4% di ma ( b e d ) , laumento della pendenza della corrente ( 10%25% da 45120 bpm ) determina un significativo aumento di dose surplus da basse ad elevate frequenze cardiache ( 45120 bpm ) , eccetto a 90 bpm ( pitch = 0 , 43 vs 0 , 40 )  . 
this reduction is maximised in narrow pulsing window protocols , especially with mindose modulation . nonetheless , the use of dose optimisation algorithms entails a significant component of surplus dose ( nondiagnostic dose ) with increasing hr in terms of r - r interval duration and the information to be extrapolated . 
questa riduzione massima nei protocolli narrow pulsing window , in particolare con modulazione mindose . tuttavia , lutilizzo degli algoritmi di ottimizzazione della dose mostra una pesante componente di dose surplus ( dose non diagnostica ) , allaumento della frequenza cardiaca , in relazione alla durata dellintervallo r - r e alle informazioni da estrapolare . 
msv , dose efficace ; bpm , battiti per minuto ; slope - up , finestra di transizione della corrente dal minimo al massimo valore di ma ; slope - down , finestra di transizione della corrente dal massimo al minimo valore di ma ; dose surplus , dose sottesa dalla finestra di transizione della corrente del tubo , durante lalgoritmo di modulazione ; narrow fi , narrow pulsing window functional imaging , protocollo a ; wide fi , wide pulsing window functional imagin , protocollo b ; narrow md , narrow pulsing window mindose , protocollo c ; wide md , wide pulsing window mindose , protocollo d . dependence on modulation algorithm dipendenza dallalgoritmo di modulazione at low and high hr , the use of the narrow pulsing window protocol significantly reduced total radiation exposure , with and without evaluation of left ventricular volumes . at intermediate hr , the use of the optimal acquisition window ( wide ) produced an increase in radiation exposure both with functional imaging and mindose ( ~2 msv )  . 
in patients with suspected coronary artery disease , the radiation exposure derived from a dsct - ca acquisition without a morphofunctional study of a bassa ed elevata frequenza cardiaca , lutilizzo del protocollo narrow pulsing window permette di ridurre significativamente la dose totale di radiazione , con e senza valutazione dei volumi del ventricolo sinistro . 
a frequenze cardiache intermedie , lutilizzo dellottimale finestra di acquisizione ( ampia ) risulta in un aumento di dose sia in functional imaging che in mindose ( ~2 msv )  . 
 in base ai dati ottenuti e agli studi iniziali eseguiti su apparecchiature dsct di prima generazione , appare indispensabile lutilizzo dellottimale finestra ecg - pulsing per ridurre significativamente lesposizione complessiva alle radiazione nelle indagini dsct - ca . 
the results obtained suggest that : the hr - adaptive pitch reduces total radiation exposure with increasing hr against surplus dose ; at low and high hr , the use of the optimal pulsing window produces the highest values of radiation exposure during current transition ; modulation of tube current to 4% of maximum milliampere outside the acquisition window is advisable for evaluating the coronary arteries without a morphofunctional study of the left ventricle . 
in these cases , reduction in total dose proportional to increase in hr is characterised by a component of around 37% deriving from the transition current . currently , there are no studies that evaluate the capacity and efficiency of the generator and the cooling system of dsct devices . 
however , the impact of dose of the modulation systems described cannot be overlooked and deserves further study . dsct - ca senza studio morfo - funzionale del ventricolo sinistro ( mindose ) potrebbe essere ridotta di un fattore di 5 . 
dai risultati ottenuti possibile dedurre che : il pitch heart rate - adattativo determina una riduzione di dose totale desposizione allaumentare della frequenza cardiaca , rispetto alla dose surplus ; a basse ed alte frequenze cardiache , lutilizzo dellottimale finestra pulsata mostra i pi alti valori di dose erogata durante la transizione della corrente ; una modulazione della corrente del tubo al 4% del valore nominale di ma al di fuori della finestra di acquisizione dati raccomandabile per una valutazione delle arterie coronarie senza studio morfo - funzionale del ventricolo sinistro ; in questi casi , la riduzione di dose totale proporzionale allaumento della frequenza cardiaca , mostra una componente di circa il 37% di dose relativa la transizione della corrente . non esistono al momento studi che valutino la potenzialit e lefficienza del generatore e del sistema di raffreddamento dellapparecchiatura dsct . 
 limitations limitazioni evaluation of the impact of the surplus dose delivered during the dsct - ca study was based solely on calculations performed on a phantom and on the basis of algorithms developed for this study . 
all dose - reduction algorithms available with technique were not evaluated , such as the reduction and / or increase in x - ray tube voltage , use of double kilovoltage , b26 convolution kernel , the care dose 4d system and ecg editing . this la valutazione dellimpatto di dose aggiuntiva erogata durante indagine dsct - ca basata solo su calcoli eseguiti su fantoccio e in base agli algoritmi elaborati per questo studio . 
non sono stati valutati tutti gli algoritmi di risparmio della dose disponibili con questa metodica , quali : la riduzione e / o laumento del voltaggio del tubo radiogeno , lutilizzo del doppio voltaggio , il kernel di convoluzione b26 , il sistema care dose 4d ed ecg - editing . 
ragionevole stimare che unulteriore ottimizzazione della dose sarebbe stata ottenuta applicando il care dose 4d . conclusions conclusioni using the dose - reduction algorithms available on dsct systems can keep effective dose below 10 msv in most cases . 
current transition is a constant source of surplus dose in the order of 14%34% of total dose , with greater values in protocols acquired with the narrow pulsing window and mindose modulation ( foregoing the possibility of performing an evaluation of left ventricular volumes )  . 
surplus dose increases with increasing hr . gli algoritmi di riduzione della dose disponibili su apparecchiatura dsct consentono di mantenere la dose efficacie al di sotto dei 10 msv nella maggior parte dei casi . valori di dose inferiori potrebbero essere raggiunti aumentando la pendenza della transizione della corrente nelle acquisizioni di modulazione cardio - sincronizzata . 
la transizione della corrente rappresenta una costante sorgente di dose surplus dellordine del 14%34% della dose totale , con valori maggiori nei protocolli acquisiti con finestra di pulsazione stretta e modulazione mindose ( rinunciando alla possibilit di effettuare valutazione sui volumi del ventricolo sinistro )  . 
di diagnostica per immagini e radiologia interventistica , azienda usl di ferrara , ospedale del delta , via valle oppio 2 , 44023 lagosanto , ferrara , italy 2clinical application specialist ct , philips healtcare correspondence to : s . 
the aim of this study was to assess the radiation dose of dose - reduced unenhanced abdominal multidetector computed tomography ( mdct ) scan protocols for suspected renal colic in patients within normal weight range and overweight - obese patients and to record the cumulative dose of repeated examinations . 
over a 2 - year period , we performed 1 , 026 unenhanced ct examinations for urolithiasis ; among these , 675 were performed on 636 patients referred from the emergency department . 
patients were divided into two groups on the basis of body mass index ( bmi ) : normal weight ( bmi < 25 kg / m2 group 1 ) ; overweight and obese ( bmi > 25 kg / m2 group 2 )  . 
although radiation dose is nearly double in overweight - obese patients undergoing mdct , it remains lower than that delivered by a standard - dose protocol . patients with flank pain , who are often young , are at increased risk for serial ct examinations . 
scopo dello studio misurare la dose efficace della tc addominale diretta con protocolli a bassa dose dedicati per pazienti di corporatura normale e pazienti obesi con sospetta urolitiasi , registrando inoltre lesposizione derivante da indagini tc ripetute . 
durante un periodo di due anni abbiamo eseguito 1026 indagini tc per urolitiasi ; tra queste , 675 tc sono state eseguite in 636 pazienti provenienti dal pronto soccorso ( ps )  . 
per ogni paziente stato calcolato lindice di massa corporea ( bmi ) dividendo i pazienti in due gruppi : pazienti di taglia normale ( bmi < 25 kg / m2 , gruppo 1 ) e sovrappeso - obesi ( bmi > 25 kg / m2 , gruppo 2 )  . 
la dlp media e la dose efficace media sono risultate di 177 e 345 mgycm e 2 , 4 e 4 , 8 msv rispettivamente per il gruppo 1 ed il gruppo 2 . 
the superiority of ct compared with intravenous urography ( ivu ) and ultrasonography ( us ) has been demonstrated by many clinical trials [ 47 ] in which ct had sensitivities of 96%100% , specificities of 95.5%100% and accuracies of 96%98% . 
 moreover , several previous studies [ 6 , 8 , 9 ] have shown that 10%45% of patients presenting with flank pain are affected by extraurinary conditions ( the most common disease entities that can mimic renal colic are [ 10 ] diverticulitis , adnexal masses and appendicitis )  . 
 the limit of ct is the dose of radiation delivered to the patient , which is of particular concern because many patients are young and undergo repeated examinations [ 11 , 12 ]  . 
however , ed can vary considerably , mainly as a result of body mass , but also because of the number of images taken at ivu [ 13 ]  . 
 [ 13 ] also reported that overweight and obese individuals in whom seven or more ivu images are taken are exposed to a risk comparable with that of a standard - dose ct study . 
different low - dose protocols have been proposed for ct evaluation of renal colic [ 1620 ] , with estimated ed as low as 1.5 msv or lower [ 21 ] , maintaining sensitivities and specificities close to those of standard - dose ct . 
however , one limitation of previous low - dose studies was that the protocols were not suited for large or obese sin dalla sua introduzione nel 1995 [ 1 ] la tc addominale senza somministrazione di mezzo di contrasto ( mdc ) ( unenhanced helical computed tomography , uhct ) risultata la tecnica di imaging pi precisa ed accurata nel paziente con sospetta urolitiasi [ 2 , 3 ] divenendo quindi la metodica gold standard nella valutazione di tali pazienti . la superiorit della uhct nei confronti di urografia endovenosa ( ivu ) ed ecografia ( us ) stata dimostrata da molteplici studi clinici [ 47 ] , che hanno evidenziato per la tc valori di sensibilit tra 96%100% , di specificit tra 95 , 5%100% e accuratezza tra 96%98% . 
precedenti studi [ 6 , 8 , 9 ] hanno inoltre dimostrato che nel 10%45% dei pazienti con dolore al fianco la tc identifica facilmente le patologie extraurinarie ( le affezioni che pi frequentemente mimano il dolore della colica renale [ 10 ] sono : diverticolite , masse annessiali ed appendicite )  . il limite della tc rappresentato dalla dose erogata al paziente , specialmente in pazienti con colica renale , spesso giovani e con alta probabilit di andare incontro a ripetute indagini [ 11 , 12 ]  . 
recentemente alcuni autori hanno valutato limpatto dosimetrico di ripetute indagini tc con protocollo standard - dose , riportando una dose media efficace per un singolo studio di 6 , 5 msv con tc a singolo detettore e 8 , 5 msv con tc multistrato ( tcmd ) ; gli stessi autori hanno evidenziato una dose efficace compresa tra 19 , 5153 , 7 msv nei pazienti sottoposti a indagini multiple . rispetto alla ivu la dose media efficace della tcmd con protocollo standard - dose stata misurata circa doppia [ 1315 ]  . 
tuttavia la dose efficace pu variare considerevolmente , principalmente a causa della massa corporea , ma anche in relazione al numero di esposizioni effettuate durante ivu [ 13 ]  . 
 [ 13 ] nel loro studio hanno calcolato che individui sovrappeso - obesi sottoposti a 7 o pi esposizioni in corso di ivu sono esposti ad una dose comparabile a quella di una tc standard - dose . lutilizzo di un protocollo tc a bassa dose consente una significativa riduzione della radioesposizione . 
del resto parecchi lavori in letteratura , in campi di applicazione diversi dalla nefrolitiasi , hanno dimostrato che indagini tc di qualit diagnostica possono essere ottenute con una riduzione significativa dei mas . 
per la valutazione tc della colica renale sono stati proposti vari protocolli a bassa dose [ 1620 ] , con una dose efficace di 1 , 5 msv o anche inferiore [ 21 ] , pur mantenendo sensibilit e specificit radiol med ( 2010 ) 115 : 105114 individuals . 
we also evaluated the number of ct examinations performed for suspected renal colic and the cumulative radiation dose delivered . materials and methods patient population during a 2 - year period , 1 , 026 mdct examinations for urinary tract calculi were performed . 
among these , 675 low - dose unenhanced mdct examinations were performed on 636 consecutive patients with flank pain referred from the emergency department [ mean age 52.114.4 standard deviation ( sd ) years , range 2086 years ]  . 
patients within a normal weight range ( bmi < 25 kg / m2 ) were included in group 1 and overweight and obese patients ( bmi > 25 kg / m2 ) in group 2 . 
each patients age , sex and number of unenhanced ct examinations performed for suspected renal colic were then determined . dose - modulation systems our scanner has three systems for dose modulation and automatic current selection : automatic current selection ( acs ) : this system allows one to automatically manage milliampere per second / slice to maintain a constant signal - to - noise ratio ( snr ) in patients imaged with the same protocol . 
this system can be managed in two ways : automatic where acs refers to a database of normality already present in the syste during the scanogram , the system detects the point of greater absorption and determines the value of milliampere per second / slice appropriate to maintain the snr ( expressed by the sd value of water ) constant . simili a quelle della tc standard - dose . 
alcuni studi in letteratura riguardanti limpiego di tc bassa dose nel sospetto di nefrolitiasi , hanno evidenziato dei limiti della metodica negli individui obesi ; tali ricercatori [ 18 , 20 , 22 ] hanno suggerito , per una adeguata valutazione del paziente obeso limpiego di un protocollo tc a dose standard al fine di ottenere una migliore qualit delle immagini . 
lo scopo del nostro studio la misurazione della dose efficace della tcmd con doppio protocollo a bassa dose , per il paziente di corporatura normale e per il paziente soprappeso - obeso . 
abbiamo inoltre registrato il numero di tcmd effettuate dai pazienti con colica renale e la dose cumulativa di radiazioni erogata . materiale e metodi pazienti osservati durante un periodo di 2 anni sono state eseguite 1026 tcmd per la valutazione di litiasi delle vie urinarie . 
tra queste , sono state eseguite 675 indagini tc dirette a bassa dose su un totale di 636 pazienti consecutivi provenienti da ps con dolore al fianco ( et media 52 , 114 , 4 ( sd ) , range 2086 anni )  . 
i criteri di esclusione dei pazienti sono stati : gravidanza , et inferiore ai 18 anni , segni di infezione con febbre o precedente tc per calcoli urinari nei 6 mesi antecedenti . 
i pazienti nel range di peso considerato normale ( bmi < 25 kg / m2 ) sono stati inclusi nel gruppo 1 e i pazienti sovrappeso ed obesi ( bmi > 25 kg / m2 ) nel gruppo 2 . 
sono inoltre stati considerati per ogni paziente et , sesso e numero di indagini tc dirette eseguite per sospetta colica renale nel periodo di osservazione . sistemi di modulazione della dose il nostro scanner ha 3 sistemi di modulazione di dose e di correzione automatica dei mas utilizzabili : acs ( automatic current selection ) tale sistema consente di automatizzare la gestione dei mas / slice per mantenere costante il rapporto segnale rumore nei pazienti eseguiti con lo stesso protocollo , tale sistema pu essere gestito in due modi automatico e manuale : automatico : lacs fa riferimento ad un database di normalit gi presente nel sistema . 
al momento dellesecuzione dello scanogramma , il sistema rileva il punto di maggior assorbimento e determina il 108 radiol med ( 2010 ) 115 : 105114 manual this differs from the previous method only in the definition of the value of snr to be maintained . in this case , the examination is performed with the qualitative data decided by the operator . 
at the end of data acquisition , the sd values obtained will be repeated for the following patients . dose - modulation system ( d - dom ) works on the x - axis : the ct controller is able to assess the exposure of each reading , correcting the value of milliampere per second / slice in the next one . 
the typical example is at the level of the shoulders , where the system delivers a greater dose in laterolateral readings ( greater patient thickness ) than in anteroposterior readings . dose - modulation system on the z - axis ( z - dom ) : it acquires the scout view and determines a scale of beam attenuation on the basis of which the dose ( milliampere per second / slice ) is modulated . 
z - axis modulation adjusts the tube current in the scanning direction and results in a substantial reduction in mean radiation dose [ 23 ] compared with fixed tube current scanning [ 24 ]  . technical imaging parameters ct scans were performed from the top of the kidneys to the base of the bladder with the patient in the supine position and without the use of iv contrast material using a 64mdct scanner ( philips brilliance 64 , philips medical systems , best , the netherlands )  . 
in all patients , low - dose mdct scans were obtained with a 2 - mm nominal slice width , 1 - mm slice increment and voltage at 120 kv . 
exposure was reduced by selecting a maximum milliampere per second value for group 1 and group 2 , respectively , at 70 mas and 150 mas while keeping the other parameters constant . 
we decided not to use acs because this system changes the milliampere per second values based on patient size , so in the case of obese patients it can increase the set milliampere per second values and the dose to the patient . effective dose calculation the dose - length product ( dlp ) is the product of the weighted ct dose index ( ctdiw ) and the length of the imaged object ( in centimeters )  . 
to calculate the radiation dose delivered with a single low - dose valore di mas / slice idoneo per mantenere il rapporto segnale - rumore ( espresso dal valore di deviazione standard dellacqua ) costante . 
in questo caso si deve eseguire un esame con dei dati qualitativi decisi dalloperatore ; al termine dellacquisizione si dovr impostare il sistema in modo che la deviazione standard ottenuta sia quella da replicare nei pazienti successivi . d - dom un sistema di modulazione di dose che lavora sullasse x . 
lesempio tipico si ha a livello delle spalle dove il sistema eroga maggior dose nelle letture latero - laterali ( per maggior spessore del corpo del paziente ) rispetto a quelle anteroposteriori e postero - anteriori . z - dom un sistema di modulazione della dose sullasse z . 
la modulazione automatica di corrente lungo lasse z in grado di ridurre in maniera sostanziale la dose media di radiazioni [ 23 ] , rispetto alla scansione a corrente fissa [ 24 ]  . parametri tecnici di imaging le scansioni tc sono state eseguite dal polo superiore dei reni al pavimento vescicale con paziente in posizione supina , senza utilizzo di mdc endovenoso , utilizzando uno scanner multidetettore a 64 strati ( philips brilliance 64 , philips medical systems , best , olanda )  . 
lesposizione stata ridotta selezionando un valore massimo di milliampere / s rispettivamente di 70 mas e 150 mas per i gruppi 1 e 2 , mantenendo costanti i restanti parametri . 
nei pazienti del gruppo 1 sono stati utilizzati 70 mas senza modulatori di dose , mentre nel gruppo 2 abbiamo impostato 150 mas con modulazione di dose sullasse z ( z - dom )  . 
abbiamo deciso di non utilizzare il sistema acs poich tale sistema , che modifica i valori di mas in base alla corporatura del paziente , in caso di corporature obese potrebbe determinare un incremento del valore dei mas impostati e quindi ad un aumento della dose . calcolo della dose efficace il dlp il prodotto del ctdivol ( computer tomography dose index , dove ctdivol = ctdiw / pitch ) e la lunghezza delloggetto scansionato ( in centimetri )  . 
i fattori di radiol med ( 2010 ) 115 : 105114 unenhanced ct examination for flank pain , the estimated dlp for every ct examination was recorded from the scanner console . 
the conversion factor was taken [ 12 ] as the average ( 0.014 msv / mgy / cm ) of the abdominal and pelvic [ 25 ] conversion factors ( the conversion factor for abdominal ct is 0.012 msv / mgy / cm , and the conversion factor for pelvic ct is 0.016 msv / mgy / cm )  . 
a total of 25 patients ( 3.7% ) underwent two or more low - dose ct examinations for urolithiasis ; one patient in group 2 underwent four ct examinations during the study period . 
per calcolare la dose efficace normalizzata erogata dai protocolli tcmd a bassa dose abbiamo utilizzato i valori di dlp registrati dalla console dellapparecchio per ciascun paziente , ottenendo poi la dlp media per il gruppo 1 e 2 dalla somma delle singole dlp . 
il fattore di conversione stato calcolato [ 12 ] come la media ( 0 , 014 msv / mgy / cm ) tra il fattore di conversione addominale e pelvico ( il fattore di conversione per la ct addominale 0 , 012 msv / mgy / cm e il fattore di conversione per la ct pelvica 0 , 016 msv / mgy / cm )  . 
venticinque pazienti ( 3 , 7% ) sono stati sottoposti a 2 o pi indagini tc a bassa dose ( range 24 ) per urolitiasi ; un paziente del gruppo 2 , fig . 
1a axial image obtained in a 68 - year - old man ( body mass index 25 kg / m2 ) with low - dose protocol ( 70 mas , 120 kv ) shows a tiny calcification at the left ureterovesical junction . 
1a immagine assiale di una paziente di sesso femminile di 68 anni ottenuta con protocollo bassa dose ( 70 mas , 120 kv ) : sfumata calcificazione alla giunzione uretero - vescicale sinistra . 
posteriormente ad essa bene riconoscibile piccolo flebolita di 2 mb , la puntiforme immagine litiasica alla giunzione uretero - vescicale meglio identificabile nella immagine assiale acquisita con protocollo standard ( 300 mas , 120 kv ) al medesimo livello di a . 
after ct scan 52 / 636 patients ( 8.1% ) underwent at least one us examination within the next 6 months . mean dlp for a single examination for flank pain was estimated to be 177 and 345 mgy / cm for group 1 and group 2 , respectively . 
using these estimated ed for a single low - dose ct examination for suspected renal colic , the estimated ed delivered to the majority of patients was low , and most of these patients ( 96.3% ) underwent only one ct examination . 
however , the diagnostic value of discussione durante il periodo di studio , stato sottoposto a 4 esami tc . tutti i pazienti sottoposti a 2 o pi indagini tc avevano anamnesi positiva per calcoli delle vie urinarie . 
in 40 su 636 casi ( 6% ) i risultati della tc hanno richiesto approfondimento diagnostico , immediato o dilazionato di pochi giorni , mediante ulteriori scansioni tc con somministrazione e.v. 
dopo la tc , 52 / 636 pazienti ( 8 , 1% ) sono stati sottoposti ad almeno una indagine ecografica nei sei mesi successivi . la dlp media di una singola indagine tcmd diretta a bassa dose per il gruppo 1 ed il gruppo 2 sono state calcolate rispettivamente in 177 e 345 mgy cm ; pertanto la dose efficace media risultata di 2 , 4 msv nel paziente normotipo e 4 , 8 msv per pazienti sovappeso - obesi . 
sommando la esposizione cumulativa nei pazienti ( 3 , 7% ) sottoposti a 2 o pi indagini tc a bassa dose , risultata una dose efficace complessiva compresa nel range 4 , 819 , 2 msv . la tc attualmente la metodica gold standard nellimaging dei pazienti con sospetta colica renale , per molteplici motivi : velocit di esecuzione , elevata sensibilit nella individuazione del calcolo , panesplorabilit e diagnosi di patologie associate , utilit nella successiva gestione del paziente . 
poich i pazienti portatori di nefrolitiasi sono spesso giovani e possono incontro a ripetute indagini anche a breve distanza di tempo , luso sistematico della tc con conseguente radioesposizione ogniqualvolta si presentano con quadro clinico di colica renale costituisce per il radiologo motivo di riflessione etica [ 6 , 11 , 12 , 20 ]  . 
nellintento di contenere la dose entro valori accettabili , diversi protocolli tc a bassa dose sono stati di volta in volta proposti da vari autori , riportando risultati del tutto simili a quelli della tc standard dose ( persino un protocollo ultra - low dose a 6 , 9 mas , con esposizione simile a quella della diretta addome per ricerca calcoli , ha dimostrato migliori risultati della us nella valutazione della urolitiasi ) [ 21 ]  . 
 [ 19 ] , mediante impiego di corrente ridotta a 100 mas , hanno osservato una riduzione allincirca del 25%42% della dose al paziente rispetto allimpiego di un protocollo tc standard dose , senza significativo decremento nellaccuratezza [ 19 ]  . 
 [ 16 ] mediante impiego di corrente ridotta a 50 mas riportano una riduzione del 81% della dose nei confronti di un protocollo tc standard dose a 260 mas [ 16 ]  . 
la tc bassa dose ( 70 mas , 120 kv ) mostra ispessimento parietale del colon discendente , disomogeneit ed aspetti flogistici del grasso pericolico con minuscole micro - bolle aeree ( diverticolite con perforazione saccata )  . 
 radiol med ( 2010 ) 115 : 105114 ct comes at the expense of substantial radiation exposure . because many patients are young and undergo repeated examinations during their lifetime , the systematic use of ct at a patients admission represents an ethical concern [ 6 , 11 , 12 , 20 ]  . 
in order to decrease radiation dose , different lowdose protocols have been proposed with performance similar to that of standard - dose ct ( even an ultra - low - dose protocol 6.9 mas , with a radiation dose equivalent to that of plain abdominal x - ray ( or kub , kidney urinary bladder film ) has shown better results than us in evaluating urolithiasis ) [ 21 ]  . 
the study by kalra et al . [ 23 ] well documented the linear correlation between patient size and image quality and the need for an adequate scanning protocol for larger patients . 
 all ct equipment manufacturers have made available software that adjusts the milliampere per second continuously , depending on the thickness of the patient being penetrated by the beams at that point in time . 
these software programmes can also be used in conjunction with generalised reductions in milliampere per second levels when appropriate by setting maximum milliampere per second thresholds for the particular examination . 
in comparison with fixed tube current , automatic tube current modulation ( z - axis modulation ) results in a significant reduction of radiation , from 51% to 77% [ 23 , 27 ]  . 
 [ 20 ] compared a low - dose ct scan with a standard - dose ct scan in the same study population , showing equivalent performance for detecting stones 3 mm in the ureter of patients with a bmi < 30 kg / m2 , but some limitations in the detection of stones < 3 mm and in the determination of the exact stone size . 
 [ 17 ] hanno eseguito scansioni supplementari soltanto in caso di dubbio di calcoli o di aree con rapporto s / n estremamente sfavorevole , osservando alta accuratezza ed eccellente concordanza inter - operatore con dose efficace media di 1 , 2 msv per i maschi e 1 , 9 msv per le femmine . infatti possibile ridurre i mas nel pazienti di corporatura normale senza sacrificare la qualit dellimmagine , cosa che invece accade nei pazienti di corporatura robusta o soprattutto obesi ; in altre parole , il rumore nelle immagini tc cresce parallelamente allaumento della corporatura ( o , meglio , del diametro ) del paziente ( a parit degli altri fattori che contribuiscono allimmagine )  . 
 [ 23 ] dimostra una correlazione lineare tra la taglia del paziente e la qualit dellimmagine , suggerendo la necessit di un adeguato protocollo di studio nei pazienti di taglia robusta . 
 attualmente tutti gli apparecchi tc in commercio dispongono di software che modulano il livello di mas aggiustandolo in modo continuo , a seconda dello spessore del paziente che viene penetrato dal fascio radiogeno . 
nei confronti dei protocolli tc con corrente costante al tubo radiogeno , la modulazione automatica di corrente lungo lasse z ( z - axis modulation ) consente una significativa diminuzione della dose radiogena , dal 51% al 77% [ 23 , 27 ]  . parecchi investigatori hanno documentato problemi nellimpiego dei protocolli a bassa dose in pazienti obesi a causa di un rapporto s / n sfavorevole , con conseguente scarsa qualit diagnostica dellimmagine , suggerendo pertanto la necessit di una esposizione adeguata . 
 [ 23 ] hanno evidenziato che calcoli di dimensioni < 5 mm possono essere misconosciuti in caso di incremento notevole del rumore dellimmagine . altri autori avevano raccomandato in precedenti studi [ 18 , 28 ] limpiego di protocollo tc standard dose in pazienti obesi con bmi > 30 kg / m2 , con conseguente maggior esposizione , ai fini di ottenere una adeguata qualit dellimmagine . 
 [ 22 ] hanno messo in discussione lappropriatezza del protocollo bassa dose a 30 mas nei pazienti obesi , esprimendo dubbi riguardo alle diagnosi alternative / addizionali che potrebbero essere misconosciute in caso di eccessiva diminuzione dei mas . 
a differenza di altri autori [ 18 , 28 ] che suggeriscono limpiego di protocollo standard dose , anche nel paziente sovrappeso / obeso 112 radiol med ( 2010 ) 115 : 105114 missed at a higher noise index because of a greater image noise . 
previous studies recommended the use of standarddose ct with higher radiation exposure in obese patients ( bmi < 30 kg / m2 ) [ 18 , 28 ] to achieve adequate image quality . 
 [ 22 ] discussed the appropriateness of a low - dose protocol at 30 mas in obese individuals , expressing concern regarding the additional diagnoses that could be missed if the dose is lowered too much . unlike other authors [ 18 , 28 ] , in patients with a bmi > 25 kg / m2 , instead of a standard - dose ct protocol , we prefer to use a low - dose protocol suited for overweightobese patients , as this can reduce ed by half . 
 the mean ed delivered to overweight - obese patients of our study population ( 36% ) was nearly double that delivered to normal - weight patients ( 4.8 msv ) but lower than that of standard dose mdct [ 12 ]  . 
by setting exposure at 70 mas with automated z - axis tube current modulation , we obtained a mean ed of 2.4 msv , slightly higher than that reported by other authors with exposure at 30 mas [ 17 , 20 ] and 50 mas [ 16 ]  . 
to limit cumulative radiation exposure , in agreethe 6 - months ment with emergency physicians , following a ct scan , patients returning to the emergency department for retained stones or new episodes of colic are followed up with us . 
 our strategy of using us to follow - up patients with a former ct examination in the prior 6 months could be an explanation for the very low incidence ( 3.7% ) of repeat ct scans in our institution during a 2 - year study period . conversely , broder et al . 
 [ 11 ] reported 2.5 ct examinations per patient in emergency patients ( 49% during an observation period of 10 months had two ct scans and 10% had five or more )  . 
these authors [ 12 ] suggest that a combination of plain abdominal x - ray ( kub film ) and us could be used as a first imaging study in evaluating acute flank pain in patients who have a high pretest probability for symptomatic nephrolithiasis and who are likely to undergo serial ct . the limitations of this study include its retrospective noi preferiamo utilizzare un protocollo tc a bassa dose dedicato . la dose efficace media erogata al paziente sovrappesoobeso ( 36% dei pazienti della nostra casitica ) , pur risultando doppia ( 4 , 8 msv ) rispetto a quella del paziente normotipo , rimane comunque assai inferiore rispetto a quella di 8 , 5 msv erogata da un protocollo mdtc standard - dose [ 12 ]  . 
la maggior parte delle nostre indagini ( 64% ) sono state eseguite in pazienti di taglia normale . impostando la corrente del tubo a 70 mas , unitamente alla modulazione automatica di corrente lungo lasse z , la dose efficace media al paziente da noi registrata stata di 2 , 4 msv , leggermente pi elevata rispetto a quella riscontrata da altri autori che tuttavia hanno impostato valori minori di corrente , a 30 mas [ 17 , 20 ] o a 50 mas [ 16 ]  . la nefrolitiasi una patologia che frequentemente affligge il paziente adulto di giovane et , con una percentuale di recidiva di almeno il 50% [ 20 ] ; inoltre parecchi pazienti possono essere sottoposti a multiple esposizioni in caso di studi eseguiti durante il follow - up della malattia . 
in accordo con i colleghi del pronto soccorso , per limitare la esposizione cumulativa derivante da esami tc ripetuti , abbiamo scelto di utilizzare la us nel follow - up dei pazienti che si ripresentano al pronto soccorso nei 6 mesi successivi ad un esame tc ( per calcolo non ancora espulso o nuovi episodi di colica )  . 
in effetti nel follow - up dei pazienti con calcolo non espulso , la us la metodica pi semplice ed efficace per escludere la ostruzione subacuta o cronica delle vie urinarie . 
 la nostra scelta di effettuare il follow - up mediante us dei pazienti sottoposti nei 6 mesi precedenti ad un esame tc potrebbe essere una spiegazione della bassa incidenza ( 3 , 7% ) di ulteriori esami tc da noi riscontrata durante il periodo biennale di osservazione . 
al contrario broder et al . [ 11 ] hanno riportato in pazienti di ps una media di 2 , 5 esami tc per paziente ( 49% dei pazienti durante un periodo di osservazione di 10 mesi sono stati sottoposti a 2 indagini tc , mentre il 10% stato sottoposto a 5 o pi esami tc )  . 
gli stessi autori [ 12 ] suggeriscono che lindagine di prima istanza nello studio di pazienti con alta probabilit di nefrolitiasi sintomatica e alta probabilit di essere sottoposti a numerose indagini tc potrebbe essere la combinazione di us ed addome diretto . 
 i limiti del nostro studio includono la natura retrospettiva ed il calcolo della dose efficace partendo da valori di dlp forniti dal software dellapparecchio ; secondo alcuni autori radiol med ( 2010 ) 115 : 105114 nature and the use of estimates , rather than direct measurements , for dlp and ed . 
this may generate relevant differences in reported ed values . con tale metodologia la dose viene sottostimata nei confronti della misurazione sperimentale tramite dosimetri a termoluminescenza ( tld ) posti su un fantoccio antropomorfico [ 29 ]  . peraltro in letteratura sono usati differenti fattori di conversione specifici per la tc addominale per ottenere la dose efficace , con valori assai variabili , da 0 , 011 [ 20 ] a 0 , 0150 , 019 [ 26 ]  . 
ci pu essere causa di rilevanti differenze dei valori di dose efficace riportate dai diversi autori . conclusioni conclusions the systematic use of unenhanced ct in patients with suspected renal colic raises an ethical concern with regard to delivered radiation dose . 
a shared clinical strategy is needed to limit the number of repeat examinations in patients with renal colic . luso sistematico di tc addominale diretta nei pazienti con sospetta colica renale rappresenta un problema etico per il radiologo . 
limpiego di un protocollo tc a bassa dose pertanto obbligatorio nello studio della litiasi renale in pazienti , spesso giovani , che hanno alta probabilit di essere sottoposti a tc in altre successive occasioni . 
nel paziente soprappeso / obeso la dose efficace media erogata con il nostro protocollo dedicato pur essendo doppia rispetto al paziente di taglia normale , rimane assai inferiore rispetto alla dose erogata con protocollo standard . 
skin thickening was identified in eight patients ( 58% ) , oedema in nine ( 64% ) , nipple retraction in two ( 14% ) , architectural distortion in eight ( 58% ) , mass - like enhancement in five ( 36% ) , non - mass - like enhancement in nine ( 64% ) with washout enhancement curve in 12 ( 86% ) and plateau curve in two ( 14% ) , axillary lymphadenopathy in 12 ( 86% ) and internal mammary artery lymphadenopathy in two ( 14% ) , and pectoral muscle enhancement in one ( 7% )  . 
the most characteristic mr findings of ibc are skin thickening , oedema , architectural distortion , masslike enhancement with washout curve and axillary lymphadenopathy ; less frequent ones are nipple retraction , mass - like enhancement and internal mammary lymphadenopathy . 
ispessimento cutaneo era presente in 8 pazienti ( 58% ) , edema cutaneo in 9 ( 64% ) , retrazione del capezzolo in 2 ( 14% ) , distorsione architetturale in 8 ( 58% ) , impregnazione parenchimale tipo massa in 5 ( 36% ) , e tipo non massa in 9 ( 64% ) con curva dinamica di impregnazione persistente in 2 ( 14% ) e con wash - out in 12 ( 86% ) , impregnazione cutanea in 2 ( 14% ) , adenomegalia ascellare in 12 ( 86% ) e mammaria interna in 2 ( 14% ) , impregnazione pettorale in 1 ( 7% )  . 
nel carcinoma infiammatorio , i segni rm pi caratteristici sono ispessimento , edema cutaneo , distorsione architetturale , impregnazione estesa tipo non massa con andamento wash - out e linfoadenopatia ascellare ; meno frequenti , retrazione del capezzolo , impregnazione tipo massa e adenomegalia mammaria interna . 
la presenza di liquido pre - pettorale frequente e non ne comporta infiltrazione . keywords breast inflammatory breast cancer mr imaging parole chiave mammella carcinoma infiammatorio risonanza magnetica radiol med ( 2010 ) 115 : 7082 introduction inflammatory breast carcinoma ( ibc ) , also known as carcinomatous mastitis , is the most aggressive form of locally advanced breast cancer . 
its name refers to a clinical pattern of extensive involvement of dermal lymphatic vessels and swollen and reddened appearance of the breast rather than to any specific histological type . the clinical manifestations of ibc include discolouration with diffuse or mottled reddening of the skin extending to at least one third of the breast , dimpled peau dorange skin , a ridge at the borders of the affected area , breast mass or tenderness associated with pain and increase in volume and temperature of the entire breast . 
the breast therefore shows the typical signs and symptoms of acute inflammation , in particular , oedema and reddening , of less than 23 months duration [ 1 ]  . 
 pathology of a specimen of breast tissue reveals the presence of carcinoma , commonly poorly differentiated infiltrating ductal carcinoma , even though any histological type of breast cancer may be associated with ibc . 
the breast parenchyma is distorted by the cancer cells , with oedema and inflammatory infiltrates ; the vascular structures are invaded by tumour emboli . ibc is rare , accounting for 1%6% of all breast cancers . it has an incidence is 0.7 cases per 100 , 000 persons per year , with a mean age at onset of 58 years [ 25 ]  . 
survival is approximately 1236 months [ 1 ]  . typical or common ibc ( 50% of cases ) is characterised by all the clinical signs and symptoms of inflammatory carcinoma described above . 
finally , clinical ibc or pseudo - ibc ( 40% of cases ) shows all the inflammatory signs and symptoms and often manifests as a palpable mass without evidence of subdermal lymphatic invasion [ 28 ]  . magnetic resonance ( mr ) imaging of the breast was introduced by fischer in 1999 [ 9 ] , and since then numerous , authors have endeavoured to identify the indications and potential of the examination [ 10 ]  . 
widely accepted indications introduzione il carcinoma infiammatorio della mammella ( inflammatory breast carcinoma , ibc ) o mastite carcinomatosa la forma pi aggressiva di tumore mammario localmente avanzato la cui denominazione si riferisce alla presentazione clinica con esteso coinvolgimento dei vasi linfatici dermici e aspetto tumefatto ed eritematoso della mammella e non ad un tipo istologico specifico . le manifestazioni cliniche dellibc comprendono una discolorazione rossa o a chiazze della cute , estesa ad almeno 1 / 3 della superficie della mammella , pelle con aspetto a buccia darancia , uno scalino ai margini della zona infiammata , una massa o fragilit dei tessuti mammari associati a dolore e un aumento del volume e della temperatura dellintera mammella . 
 lesame anatomo - patologico di un frammento di ghiandola mammaria evidenzia la presenza di carcinoma mammario , pi frequentemente di carcinoma duttale infiltrante scarsamente differenziato , anche se un qualsiasi tipo istologico di tumore mammario pu associarsi a ibc . 
il parenchima ghiandolare risulta alterato dalle cellule tumorali presenti , con edema e infiltrati infiammatori ; le strutture vascolari in esso comprese sono invase da emboli neoplastici . il carcinoma infiammatorio della mammella raro , rappresentando l1%6% di tutti i tumori mammari . 
secondo il sistema di stadiazione tnm , il carcinoma infiammatorio classificato come t4d [ 6 ] ; alla diagnosi nella maggior parte dei casi vi un interessamento clinico dei linfonodi e nel 20% metastasi a distanza . 
la sopravvivenza si aggira intorno ai 1236 mesi [ 1 ]  . libc tipico o comune ( 50% dei casi di ibc ) caratterizzato dalla presenza di tutti i segni e sintomi clinici del carcinoma infiammatorio , precedentemente descritti , localizzati a una mammella in associazione a un reperto istologico positivo per emboli tumorali nei vasi linfatici subdermici e del parenchima mammario . 
infine libc clinico o pseudo - ibc ( 40% dei casi ) presenta tutti i sintomi infiammatori e spesso si manifesta con una massa palpabile senza riscontro di invasione linfatica subdermica [ 28 ]  . lo studio della mammella con risonanza magnetica radiol med ( 2010 ) 115 : 7082 for breast mr imaging are the detection of breast cancer in young women at high genetic risk , in patients with cancer of unknown primary ( cup ) syndrome and in those with breast implants , the characterisation of doubtful mammographic and sonographic findings , the staging of histologically proven cancers , the evaluation of locally advanced cancers before or after neoadjuvant chemotherapy and postsurgical follow - up [ 11 , 12 ]  . 
 numerous papers have reported the mr imaging patterns of the most common breast carcinomas infiltrating ductal and lobular carcinoma whereas the features of the rarer breast malignancies are less well known . 
 the aim of this study was to describe the mr imaging features of ibc on the basis of a review of the literature and our personal experience . materials and methods patients as the study was based on a retrospective review of mr examinations , the patients informed consent was not required . 
during a search of the radiology and pathology archives of our institution to identify all patients studied by breast mr and all histological examinations of needlebiopsy or surgical specimens carried out between january 2005 and march 2008 , we identified 25 patients with a pathological or clinical diagnosis of ibc . 
 the study included patients with breast carcinoma associated with clinical signs of inflammation and those with a histological diagnosis of massive neoplastic invasion of the subdermal lymph vessels who underwent mr imaging before surgery or chemotherapy . 
patients were excluded if they had clinical evidence of ibc without a histological diagnosis ( n = 2 ) , those studied by mr imaging after undergoing chemotherapy ( n = 3 ) or surgery ( n = 1 ) and those with a pathological diagnosis of ibc not studied by mr imaging ( n = 5 )  . our final study population therefore comprised 14 patients , with a mean age of 48 ( range 3181 ) years . 
eleven patients had clinical evidence of ibc ( typical ibc ) ; the remaining three had no clinical signs but only histological evidence of lymphatic vessel infiltration ( occult ibc )  . 
with regard to hormone status , nine patients were premenopausal and five were postmenopausal ; nine had had pregnancies with a mean number of two children , and in one case the clinical picture arose during the puerperiu a positive family ( rm ) stato introdotto nel 1999 da fischer [ 9 ] e da allora molti autori si sono adoperati per individuarne le indicazioni e le possibilit [ 10 ]  . 
le applicazioni riconosciute con largo consenso sono lidentificazione di neoplasie mammarie in giovani donne ad alto rischio genetico , in pazienti con cancer of unknown primary ( cup ) syndrome e con protesi mammarie , la caratterizzazione di reperti mammografici ed ecografici di incerto significato diagnostico , il bilancio di estensione di neoplasie gi istologicamente diagnosticate o nella valutazione pree postchemioterapia neoadiuvante in caso di tumori localmente avanzate e il follow - up post chirurgico [ 11 , 12 ]  . 
 un crescente numero di lavori ha descritto gli aspetti relativi alla semeiotica rm delle neoplasie mammarie pi frequenti carcinoma duttale e lobulare infiltrante mentre sono meno conosciute le caratteristiche delle neoplasie maligne rare della mammella . 
 scopo di questo studio quello di descrivere gli aspetti semeiotici nellindagine rm del carcinoma infiammatorio della mammella basandoci sullanalisi dei dati della letteratura e di quelli ottenuti nellesperienza personale . materiali e metodi pazienti lo studio stato condotto con la valutazione retrospettiva degli esami rm e quindi senza il consenso informato della paziente . 
dalla ricerca nellarchivio radiologico delle pazienti sottoposte a indagine rm mammaria e nellarchivio patologico di tutti gli esami istologici su frustoli agobioptici o pezzi chirurgici , nel periodo compreso fra gennaio 2005 e marzo 2008 sono state individuate 25 pazienti con diagnosi patologica o clinica di carcinoma infiammatorio . 
 sono state incluse nello studio le pazienti con neoplasia mammaria accompagnata da segni clinici di infiammazione e quelle con diagnosi istologica di massiva infiltrazione neoplastica dei vasi linfatici subdermici sottoposte a indagine rm prima dellintervento chirurgico e della chemioterapia . 
sono state escluse le pazienti con rilievi clinici di carcinoma infiammatorio senza diagnosi istologica ( 2 casi ) e quelle sottoposte a rm dopo linizio della chemioterapia ( 3 casi ) o lintervento chirurgico ( 1 caso ) e quelle con diagnosi patologica di carcinoma infiammatorio non sottoposte a indagine rm ( 5 casi )  . 
pertanto la popolazione in studio costituita da 14 pazienti con et media di 48 anni e radiol med ( 2010 ) 115 : 7082 history , with at least one relative with previous breast cancer , was present in six cases . mr imaging imaging was performed with a 1.5 - t magnet ( symphony , siemens medical system , erlangen , germany ) without time limitations in all women . 
 image analysis image postprocessing involved subtraction of the precontrast images from the postcontrast images and generation of multiplanar reconstructions ( mpr ) and maximum intensity projections ( mip )  . 
regions of interest ( roi size 59 pixels ) were placed over the areas of contrast enhancement seen on the second acquisition after contrast administration to generate time - intensity curves . two radiologists ( gc , vg ) with 7 and 3 years experience with breast mr imaging , independently reviewed all images on the workstation . 
the baseline t2 - weighted sequences were assessed for breast enlargement , nipple retraction , skin thickening , skin oedema , architectural distortion , axially and internal mammary lymphadenopathy and presence of prepectoral fluid filthe dynamic studies were assessed for areas of increased parenchymal enhancement , cutaneous enhancement , pectoral muscle enhancement and hypertrophic internal mammary artery . 
 the areas of increased enhancement were classified as showing mass - like or non - mass - like enhancement ; areas of mass - like enhancement were analysed according to the morphological and dynamic parameters described by fischer [ 9 ] ; areas of non - mass - like enhancement were interpreted according to the breast imaging reporting and data system ( bi - rads ) lexicon with regard to morphological compresa fra 31 e 81 . 
undici pazienti presentavano un quadro clinico di carcinoma infiammatorio , configurando il gruppo ibc tipico ; nelle rimanenti 3 pazienti la clinica era muta , ma il reperto patologico era positivo per infiltrazione dei vasi linfatici , configurando il gruppo i ibc occulto . 
per quanto riguarda lo stato ormonale , 9 erano in et fertile e 5 in climaterio ; 9 avevano avuto gravidanze con numero medio di 2 figli e in un caso la clinica insorta nel puerperio . 
familiarit positiva , con almeno un parente colpito da tumore della mammella , era presente in 6 casi . indagine rm lo studio rm stato effettuato con un magnete da 1 , 5 t ( symphony , siemens medical system , erlagen , germania ) senza limitazioni temporali in tutte le donne . 
lo studio basale comprendeva una sequenza short - tau inversion - recovery ( stir ) con acquisizione trasversale ( utilizzando i seguenti parametri : tr / te : 5960 / 70 ms ; matrice 254320 pixel ; fov 350100 ; spessore 3 , 00 mm ) , una sequenza stir con acquisizione coronale ( con i seguenti parametri : tr / te : 4840 / 68 ms ; matrice 254320 pixel ; fov 350100 ; spessore 3 , 00 mm ) e una sequenza turbo spin - echo ( tse ) con acquisizione sagittale ( con parametri : tr / te : 3910 / 95 ms ; matrice 254320 pixel ; fov 320100 ; spessore 3 , 80 mm )  . 
lo studio dinamico stato eseguito con una sequenza gradient recalled echo ( gre ) 3d sul piano coronale ( utilizzando i seguenti parametri : tr / te : 12 / 5 , 65 ms ; flip angle 25 ; matrice 254320 pixel ; fov 38075 ; spessore 1 , 24 mm ; tempo di acquisizione 88 secondi ) acquisita prima della somministrazione di mdc e ripetuta per sei volte dopo liniezione endovenosa di 0 , 1 mmol di gd - dtpa / kg di peso corporeo alla velocit di 2 , 5 ml al secondo e di 20 ml di soluzione fisiologica . 
 analisi delle immagini le immagini sono state elaborate mediante sottrazione delle acquisizioni pre - contrasto da quelle post - contrasto e ricostruzioni multiplanari ( mpr ) e proiezioni a massima intensit ( mip )  . 
posizionando una regione dinteresse ( roi , estesa 59 pixels ) sulle aree di impregnazione di mdc visualizzate nella seconda acquisizione dopo mdc sono state costruite curve delle variazioni di intensit di segnale nel tempo . 
areas of non - mass - like enhancement were analysed in terms of distribution ( focal , linear , ductal , regional , multiregional , diffuse ) , internal characteristics ( homogeneous , heterogeneous , stippled / punctate , clumped , reticular - dendritic ) , asymmetry . kinetic curves were assessed for increased signal intensity during the first 2 min after contrast administration and curve pattern over the following minutes , with three possible time intensity - curves : progressive steady enhancement ( type i ) , rapid wash - in followed by a plateau ( type ii ) and rapid wash - in followed by wash - out ( type iii )  . pathological analysis the diagnosis of breast cancer was established by percutaneous biopsy with ultrasound - guided microhistological sampling in seven cases ( 14 - gauge needle and automated or semiautomated sampling devices ) or by ultrasound - guided cytological sampling ( 21 - gauge needle ) in seven cases . massive neoplastic infiltration of the subdermal lymphatic vessels was identified in the microhistological sample in seven cases and in the surgical biopsy in the remaining seven . 
patients with a microhistological diagnosis of ibc were immediately referred for neoadjuvant chemotherapy . the remaining seven patients with a pathological diagnosis of ibc were referred for chemotherapy after surgical biopsy . 
 pathological diagnoses were formulated by two pathologists with more than 10 years experience in breast diseases . histological analysis of the core biopsies and surgical specimens included histological tumour type according to the world health organisation ( who ) classification , tumour grade ( g1 , g2 , g3 ) according to the elston - ellis easton system [ 14 ] and infiltration of the axillary lymph nodes ( negative / positive )  . statistical analysis interobserver variability in determining the type of enhancement and the morphological and dynamic parameters ( such as shape , margins , enhancement pattern and distribution ) was evaluated with the k statistic . 
the degree of concordance was classified as follows : 0.010.20 slight agreement , 0.210.40 fair agreement , 0.410.60 moderate agreement , 0.610.80 good agreement and 0.811.0 , almost perfect agreement . 
i rilievi analizzati nelle sequenze basali t2 - dipendenti senza mezzo di contrasto sono stati : aumento del volume mammario , retrazione del capezzolo , ispessimento cutaneo , edema cutaneo , distorsione architetturale , adenomegalia ascellare e mammaria interna , presenza di film liquido prepettorale . 
 le aree di aumentata impregnazione sono state classificate come tipo massa e tipo non - massa ; i reperti tipo massa sono stati analizzati secondo gli aspetti morfologici e dinamici descritti dai parametri di fischer [ 9 ] ; i reperti tipo non - massa sono stati interpretati secondo il lessico birads per quanto riguarda gli aspetti morfologici [ 13 ] e secondo i parametri di fischer per quanto riguarda gli aspetti dinamici [ 9 ]  . 
 le impregnazioni tipo massa sono state analizzate considerando : forma della lesione ( rotondeggiante ; ovalare ; spiculata ; irregolare ) , margini ( ben definiti ; mal definiti ) e pattern di enhancement ( omogeneo ; disomogeneo ; con setti ; ad anello , ed eventuale riempimento tardivo della porzione pi centrale )  . 
le impregnazioni tipo non - massa sono state analizzate considerando : distribuzione ( area focale , lineare , duttale , regionale , multi - regionale , diffusa ) , caratteristiche interne ( omogeneo , disomogeneo , punteggiato , raggruppato a macchia , reticolare - dendritico ) , asimmetria . i parametri cinetici valutati sono stati lincremento dellintensit di segnale nei primi due minuti dopo la somministrazione di mezzo di contrasto e il suo decorso nei successivi minuti configurando tre possibili curve intensittempo : incremento progressivo e graduale , tipo i ; rapido wash - in e successivo plateau , tipo ii ; rapido washin e wash - out , tipo iii . analisi patologica la diagnosi di neoplasia mammaria stata posta mediante biopsia percutanea con prelievo microistologico ecoguidato in 7 casi ( ago da 14 g , dispositivi di prelievo automatici o semi - automatici ) e mediante prelievo citologico ecoguidato ( ago da 21 g ) in 7 casi . 
il rilievo di massiva infiltrazione neoplastica dei vasi linfatici subdermici stato rilevato nel prelievo microistologico nei 7 casi in cui stato eseguito e alla biopsia chirurgica nei rimanenti 7 casi . 
le pazienti con diagnosi microistologica di carcinoma infiammatorio sono state immediatamente avviate a chemioterapia neoadiuvante ; le rimanenti 7 pazienti con diagnosi patologica di carcinoma infiammatorio sono state avviate a chemioterapia dopo biopsia chirurgica . 
on the dynamic study , mass - like enhancement was seen in five cases ( 36% ) and non - mass - like enhancement in nine ( 64% ) ( table 1 )  . 
in these cases , the histological diagnosis was infiltrating carcinoma not otherwise specified ( nas ) in five ( 36% ) , ductal carcinoma in situ in one ( 7% ) and lobular carcinoma in situ ( 7% ) in the remaining cases . 
 statistical concordance the degree of interobserver concordance was excellent as regards shape ( k = 0.82 ) and enhancement pattern ( k = 0.86 ) , la diagnosi patologica stata formulata da due anatomopatologici con pi di 10 anni di esperienza in patologia mammaria . 
i fattori istologici valutati sui frustoli dei prelievi microistologici e sulle sezioni dei pezzi operatori sono stati : istotipo tumorale definito secondo la classificazione who , grado tumorale ( g1 , g2 , g3 ) secondo elstonellis easton system [ 14 ] e infiltrazione dei linfonodi ascellari ( negativi / positivi )  . analisi statistica la variabilit interosservatore nel determinare tipo di impregnazione , parametri morfologici e dinamici ( quali forma , margini , pattern di enhancement e distribuzione ) nellambito dellanalisi delle immagini stata valutato con k statistico . 
la forza di concordanza stato valutato come segue : valori inferiori o pari a 0 , 20 indicativo di debole accordo ; 0 , 210 , 40 , accordo equo ; 0 , 410 , 60 , abbastanza accordo ; 0 , 610 , 80 , buon accordo , e 0 , 811 , 0 , ottimo accordo . 
allo studio dinamico , impregnazione parenchimale tipo massa si evidenziata in 5 casi ( 36% ) , e tipo non massa in 9 ( 64% ) ( tabella 1 )  . 
patients radiol med ( 2010 ) 115 : 7082 finding increased breast volume nipple retraction skin thickening oedema architectural distortion axillary adenopathy internal mammary adenopathy prepectoral fluid mass - like enhancement ring enhancement heterogeneous non - mass - like enhancement regional multiregional diffuse curves type i type ii type iii skin enhancement pectoral enhancement hypertrophic internal mammary artery aumento del volume mammario retrazione del capezzolo ispessimento cutaneo edema cutaneo distorsione architetturale adenomegalia ascellare adenomegalia mammaria interna film liquido pre - pettorale enhancement tipo massa ad anello disomogeneo enhancement tipo non massa regionale multiregionale diffuso curva tipo 1 tipo 2 tipo 3 impregnazione cutanea impregnazione del pettorale ipertrofia dellarteria mammaria interna 14.86 14 , 86 tabella 1 rilievi rm della mastite carcinomatosa in 14 pazienti rilievi numero delle pazienti percentuale radiol med ( 2010 ) 115 : 7082 fig . 
distortion is better depicted by the axial short - tau inversion recovery sequence ( arrowhead in b ) , which also shows diffuse periareolar hyperintensity due to oedema ( arrow in b )  . 
il sovvertimento architetturale meglio evidente nellacquisizione trasversale stir ( testa di freccia in b ) ove si rileva anche il diffuso aumento dellintensit di segnale della cute periareolare da imbibizione edematosa ( freccia in b )  . 
clinically , it presents with the typical signs of acute inflammation that progress rapidly within weeks or months . in 50% of cases , a palpable mass is detected [ 1 ]  . the diagnosis of ibc relies on the finding of neoplastic invasion of the dermal lymphatic vessels , which is more commonly related to a poorly differentiated ductal infiltrating carcinoma , although any histological type of breast carcinoma may be associated with ibc . 
in the present series , the diagnosis of neoplastic invasion of the lymphatic vessels was made in 7 / 14 ( 50% ) cases on microhistological samples and in the remaining 7 / 14 ( 50% ) cases on surgical biopsies . 
among the seven cases of ibc diagnosed on microhistological material , the underlying breast cancer was il rilievo di infiltrazione dei vasi linfatici subdermici stato rilevato nel prelievo microisto logico in 7 casi ; la diagnosi microistologica in questi casi stata di carcinoma infiltrante nas in 5 casi ( 36% ) , carcinoma duttale in situ in 1 caso ( 7% ) e neoplasia lobulare in situ ( 7% ) nel rimanente caso . 
il rilievo di infiltrazione dei vasi linfatici subdermici stato rilevato alla biopsia chirurgica negli altri 7 casi ; la diagnosi patologica in questi casi stata di carcinoma infiltrante non altrimenti specificato ( nas ) in 6 casi ( 43% ) , di carcinoma metaplastico in 1 caso ( 7% )  . 
 concordanza statistica la forza di concordanza di giudizio fra i due radiologi risultata ottima per forma ( k = 0 , 82 ) e pattern di enhancement ( k = 0 , 86 ) , buona per margini ( k = 0 , 78 ) , moderata per la valutazione della distribuzione ( k = 0 , 46 )  . radiol med ( 2010 ) 115 : 7082 fig . 
2a - d axial short - tau inversion recovery t2 - weighted sequence ( a ) : diffusely increased signal intensity in the left breast caused by cutaneous and parenchymal oedema ( large arrow in a ) and a prepectoral focal linear hyperintensity due to prepectoral fluid ( small arrow in a )  . 
maximum intensity projection reconstruction ( b ) shows a diffuse non - mass - like enhancement of the dendritic type extending to the entire left breast with a large supplying vessel ( arrow in b )  . 
2a - d nella sequenza stir nel piano trasversale ( a ) , si evidenzia un diffuso aumento del segnale del corpo mammario sinistro rispetto al controlaterale , della cute e dei tessuti sottocutanei per imbibizione edematosa ( freccia grande in a ) e un focale e lineare aumento del segnale in sede pre - pettorale riferibile a sottile falda liquida ( freccia piccola in a )  . 
dopo mezzo di contrasto , nella ricostruzione mip ( b ) , si apprezza diffusa impregnazione di tipo non - massa , con aspetto dendritico , che interessa la quasi totalit del corpo ghiandolare sinistro con robusto vaso afferente ( freccia in b )  . 
la curva di impregnazione intensit / tempo , misurata in pi punti ( c ) , mostra un rapido incremento seguito veloce wash - out ( curva di tipo 3 , d )  . ductal carcinoma in situ in one case and lobular carcinoma in situ in another case . 
 [ 2 ] , in a certain number of cases , despite a finding of dermal lymphatic invasion , it may be impossible to identify the exact point where the process became invasive and crossed the basal membrane . 
this occurs more frequently when the histological material is scarce , as in microbiopsies . conventional breast imaging has proved to be limited for the diagnosis of ibc owing to difficulties in identifying specific signs of malignancy in dense and swollen breasts [ 2 ]  . 
on mammography and ultrasound , space - occupying lesions and microcalcifications are rare manifestations of this disease , and the only findings suggestive of an underlying carcinoma are isolated inflammatory findings ( skin thickening , diffuse increase in density , trabecular thickening , axillary lymphadenopathy ) and a lack of response to discussione il carcinoma infiammatorio della mammella un raro tipo di tumore della mammella ( 1%6% di tutti i tumori mammari ) altamente aggressivo e con prognosi sfavorevole rappresentante il 24%40% dei tumori mammari localmente avanzati . 
clinicamente si presenta con i tipici segni infiammatori acuti che progrediscono rapidamente in qualche settimana o pochi mesi ; nel 50% dei casi concomitante il reperto di massa palpabile [ 1 ]  . la diagnosi di carcinoma infiammatorio richiede il rilievo di invasione neoplastica dei linfatici dermici pi frequentemente sostenuta da un carcinoma duttale infiltrante scarsamente differenziato , anche se un qualsiasi tipo istologico di tumore mammario pu associarsi a ibc . 
3a - d sequenza stir trasversale ( a ) : la mammella destra mostra diffuso aumento dellintensit di segnale coinvolgente posteriormente anche il muscolo pettorale ( freccia in a ) ; il fascio muscolare ispessito e disomogeneo anche nelle scansioni sagittali ( freccia in b )  . 
come reperto accessorio , multiple lesioni nodulari , ipercaptanti dopo mdc , a livello del corpo sternale ( testa di freccia in d )  . antibiotic treatment [ 4 , 1517 ]  . 
 mr imaging has taken on an increasingly important role in the management of breast cancer , and its indications now include initial diagnosis , staging of known cancer , monitoring the effects of neoadjuvant chemotherapy and the diagnosis of disease recurrence . 
in ibc it is used to determine the size of the tumour prior to chemotherapy , to exclude pectoral muscle involvement and to monitor response to treatment [ 2 , 17 ]  . 
recently , researchers have also investigated the value of vascular maps of the breasts , demonstrating increased vascularity of the breast ipsilateral to the tumour [ 1820 ]  . in our series , the most frequent mr signs of ibc were skin thickening and oedema , architectural distortion , extensive non - mass - like enhancement with wash - out timeintensity curve and axillary lymphadenopathy . 
the finding of architectural distortion is less frequent in series studied with mr imaging compared with mammography and ultrasound , where it is seen in 85% 95% of cases [ 2 , 4 ]  . axillary lymphadenopathy was present in 86% of cases , linfatici stata formulata in 7 / 14 ( 50% ) casi su materiale microistologico e nei rimanenti 7 / 14 ( 50% ) casi su biopsia chirurgica . 
tra i 7 casi con diagnosi di carcinoma infiammatorio su materiale microistologico , la sottostante eteroplasia mammaria risultata essere carcinoma duttale in situ in 1 caso e neoplasia lobulare in situ in un altro caso . come riportato nella casistica radiologica di yang et al . [ 2 ] in un certo numero di casi possibile che nonostante il reperto di invasione linfatica dermica , non si riesca ad evidenziare il punto in cui il processo diventato invasivo ed ha superato la membrana basale . 
questo accade pi frequentemente quando il materiale ridotto come nel caso delle microbiopsie . limaging senologico convenzionale si dimostrato limitato nella diagnosi del carcinoma infiammatorio per la difficolt ad individuare reperti semeiologici specifici di malignit in mammelle dense e tumefatte [ 2 ]  . 
allindagine mammografcia ed ecografica , lesioni espansive e microcalcificazioni sono rare manifestazioni di questa patologia e gli unici aspetti suggestivi di un sottostante carcinoma sono rappresentati dalla presenza di isolati reperti infiammatori ( ispessimento cutaneo , diffuso incremento della densit , ispessimento della trabecolatura stromale , linfoadenopatia ascellare ) e dalla mancata risposta alla terapia antibiotica [ 4 , 1517 ]  . 
 lindagine rm ha assunto un ruolo sempre pi importante nel management dei tumori della mammella , trovando indicazioni per la diagnosi iniziale , per la stadiazione di una radiol med ( 2010 ) 115 : 7082 table 2 pathological characteristics of inflammatory breast cancer in 14 patients finding no . 
patients % patients pathological diagnosis infiltrating ductal carcinoma metaplastic carcinoma ductal carcinoma in situ lobular carcinoma in situ lymph node metastasis positive negative grading isotipo carcinoma duttale infiltrante carcinoma metaplastico carcinoma duttale in situ carcinoma lobulare in situ stato linfonodale positivi negativi grado di differenziazione tabella 2 rilievi anatomo - patologici della mastite carcinomatosa in 14 pazienti rilievi numero di pazienti pazienti ( % ) a percentage similar to that reported by yang et al . 
nodal metastases were in 83% ( 10 / 12 cases ) of confirmed by histology lymphadenopathy suspected on mr imaging , a percentage higher than that reported by yang et al . 
our series was therefore characterised by locally , very advanced disease , as also confirmed by the type of enhancement , which was non - mass - like in the majority of cases ( 64% )  . 
 [ 2 ] , where 70% of ibc cases showed mass - like enhancement with multiple nodules and heterogeneous pattern , whereas it is similar to that reported by chow et al . 
nel carcinoma infiammatorio viene utilizzata per la documentazione delle dimensioni tumorali prima dellinizio del trattamento chemioterapico , per escludere linteressamento del muscolo pettorale e per il monitoraggio della risposta terapeutica [ 2 , 17 ]  . 
in sede tumorale , a causa degli attivi processi angiogenetici neoplastici si apprezza un accumulo di mezzo di contrasto le cui caratteristiche cinetiche rispecchiano gli aspetti fisiopatologici della crescita tumorale . 
di recente , stato indagato anche il valore delle mappe vascolari dellintero organo ed stato dimostrato un incremento della vascolarizzazione mammaria omolaterale alla sede tumorale [ 1820 ]  . nella serie personale , i segni rm pi frequenti di carcinoma infiammatorio sono ispessimento ed edema cutaneo , distorsione architetturale , impregnazione estesa tipo non massa con andamento della curva intensit - tempo a washout e linfoadenopatia ascellare . 
nelle casistiche analizzate con indagine rm il rilievo di distorsione architetturale meno frequente rispetto a quelle esaminate con mammografia ed ecografia dove si appalesa nel 85%95% dei casi [ 2 , 4 ]  . adenomegalia ascellare si apprezza nel 86% dei casi ; tale dato concorde con quello del 88% riportato nel recente lavoro di yang et al . 
metastasi linfonodali sono state istologicamente confermate nel 83% ( 10 / 12 casi ) delle adenopatie sospette alla rm ; la percentuale maggiore rispetto a quella del 44% riportata da yang et al . 
si tratta pertanto di una casistica di patologia localmente molto estesa come confermato anche dal tipo di impregnazione che nella maggioranza dei casi , il 64% , risultato essere di tipo nonmassa . 
 dalla disamina della letteratura emerge che non esiste un pattern interno di impregnazione patognomonico di carcinoma infiammatorio ; in genere vi cospicuo interessamento della ghiandola mammaria , con impregnazione regionale o a noduli multipli . 
the finding of hypertrophy of the internal mammary artery is fairly common : it is seen in 21% of all cases and in 27% of inflammatory carcinomas with invasive histological type . internal mammary artery hypertrophy is always associated with a pattern of intense diffuse enhancement related to a large invasive tumour . 
this observation is consistent with a previous report [ 20 ] according to which increased breast vascularity is dependent on the size of the tumour and is more pronounced in invasive disease . with regard to the remaining mr imaging findings , nipple retraction and internal mammary lymphadenopathy were less frequent . 
nipple retraction was seen in 14% of cases , and in the literature , it is reported to occur in percentages varying from 16% to 100% [ 2 , 4 , 21 , 22 ]  . 
although volume increase , together with rubor , calor , dolor ( redness , warmth , pain ) , is one of the pathognomonic signs of acute inflammation , it is a uncommon finding in ibc , and in atypical presentations , there is a narrowing of the breast with simultaneous nipple retraction . 
focal skin enhancement not directly in continuity with the tumour mass has been described as a usual finding ( up to 94% of cases in yang et al . ) [ 2 ] , but this was not the case in our series where it was present in 14% of cases only . there are some limitations to our study . 
secondly , performance of the mr study without assessing hormonal status in the nine premenopausal women in our series may have limited enhancement assessment ; however , the fact that enhancement was observed unilaterally allowed us to exclude a functional cause . 
tale osservazione in accordo con quella espressa in letteratura [ 20 ] secondo cui laumento della vascolarizzazione mammaria dipendente dalle dimensioni tumorali e pi evidente nel caso di patologia invasiva . per quanto riguarda i rimanenti rilievi rm , retrazione del capezzolo e adenomegalia mammaria interna risultano meno frequenti . 
la retrazione del capezzolo documentabile nel 14% dei casi e in letteratura ricorre con percentuali variabili dal 16% al 100% [ 2 , 4 , 21 , 22 ]  . 
la mammella interessata dal processo neoplastico appare aumentata di volume nel 14% dei casi ; sebbene lincremento volumetrico rappresenti assieme a rubor , calor , dolor un dei segni patognomonici di flogosi acuta , il suo riscontro poco frequente e nella presentazione atipica del carcinoma infiammatorio si assiste alla coartazione della mammella con contemporanea retrazione del capezzolo . 
lesecuzione dellindagine rm senza valutazione della fase ormonale nelle 9 donne di questa serie in et fertile potrebbe essere un limite per la valutazione dellimpregnazione ; tuttavia , la monolateralit dellenhancement osservato consente di escludere lorigine funzionale dellimpregnazione . 
inoltre , la complessit del lessico bi - rads - mri richiede un adeguato addestramento per la corretta interpretazione e per il confronto con le altre esperienze . conclusions conclusioni radiol med ( 2010 ) 115 : 7082 mr signs predictive of ibc are skin thickening and oedema , architectural distortion , extensive non - mass - like enhancement with type - iii time - intensity curve and axillary lymphadenopathy ; less frequent findings are nipple retracinternal mammary tion , mass - like enhancement and lymphadenopathy . 
the presence of fluid coating the pectoral muscle is common but does not imply muscle invasion . mr imaging identifies the presence of a spaceoccupying lesion with irregular margins or diffuse , heterogeneous , unilateral enhancement of the reticular - dendritic type . 
this enhancement pattern associated with skin thickening and skin enhancement is highly suggestive for ibc . i segni rm predittivi di carcinoma infiammatorio sono ispessimento ed edema cutaneo , distorsione architetturale , estesa impregnazione tipo non - massa con curva intensit - tempo tipo iii e linfoadenopatia ascellare ; meno frequenti risultano retrazione del capezzolo , impregnazione tipo massa e adenomegalia mammaria interna . 
la presenza di liquido che lambisce il pettorale frequente e non ne comporta infiltrazione . lindagine rm individua la presenza di una lesione espansiva con margini irregolari o un aumento unilaterale dellimpregnazione , disomogeneo e diffuso , di tipo reticolare - dendritico . 
sezione di diagnostica per immagini , policlinico universitario , piazza giulio cesare 11 , 70124 bari , italy 2 ospedale san paolo bari dipartimento di radiologia , via caposcardicchio 10 , 70100 bari , italy correspondence to : a.a. 
the following parameters were considered : presence , location , and wall thickness of the appendix ; wall enhancement ; distension ; periappendiceal fat attenuation ; presence of appendicolith ; and free air and / or periappendiceal fluid collections . 
quarantacinque pazienti con quadro clinico dubbio per appendicite acuta sono stati esaminati con tomografia computerizzata multidetettore ( tcmd ) a 16 strati , prima e dopo iniezione di mezzo di contrasto . 
due radiologi in cieco e con 2 e 9 anni di esperienza in tomografia computerizzata ( tc ) hanno valutato le immagini assiali e , a distanza di due mesi , le ricostruzioni vr e vrc . 
sono stati esaminati : presenza , sede e spessore parietale dellappendice , enhancement parietale e distensione del lume , morfologia del grasso periappendicolare , presenza di appendicolita , aria libera e / o raccolte fluide periappendicolari . 
nei pazienti con appendicite atipica le ricostruzioni vr e vrc migliorano laccuratezza della tcmd in relazione allesperienza delloperatore e riducono il numero di falsi negativi . radiol med ( 2010 ) 115 : 93104 keywords acute appendicitis atypical appendicitis multidetector ct ( mdct ) parole chiave appendicite acuta appendicite atipica tc multidetettore ( tcmd ) introduction introduzione acute appendicitis accounts for more than 50% of all causes of acute abdomen and requires prompt diagnosis and surgical treatment [ 1 ]  . 
in 70% of patients with acute appendicitis , the diagnosis is essentially based on the patients history , clinical examination and evaluation of blood chemistry tests [ 2 ]  . 
in those cases , acute appendicitis is classified as atypical and the diagnosis is more difficult , with a risk of complications exceeding 20% [ 1 , 3 , 4 ]  . 
atypical appendicitis is more frequent in the elderly , in children , in pregnant women , in subjects with other diseases ( diabetes , crohns disease , ovarian and tubal disorders ) and especially in patients with anatomical variants of the location of the appendix [ 5 ]  . diagnostic imaging plays an important role in this group of subjects , reducing the number of laparotomies and the risk of complications [ 68 ]  . ultrasonography ( us ) is the first - line investigation , which allows recognition , when the appendix is in normal position , of the inflammatory process or exclusion of other causes of acute abdomen , with a reported diagnostic accuracy of 75%95% in the different series [ 9 , 10 ]  . 
false negative results , which may approach 25% , are related to the difficult identification of the inflamed appendix in cases of atypical anatomy , especially with appendix in pelvic or retrocecal position [ 7 ]  . 
in these cases , computed tomography ( ct ) is the most widely used technique , and singleor multislice spiral ct can reach diagnostic accuracy levels between 94% and 100% in determining the site and course of the inflamed appendix and possible complications [ 11 , 12 ]  . 
multidetector ct ( mdct ) , capable of acquiring images with submillimetre slice thickness and the same spatial resolution along the z - axis and x - y axial plane , provides coronal and sagittal reconstructions of the same quality and anatomical detail as the axial scans . multiplanar reconstructions can therefore be useful in identifying the course of the appendix and anatomical relationship with adjacent structures , even in patients with a low amount of intra - abdominal fat [ 11 , 13 , 14 ]  . 
the purpose of this study was to evaluate the diagnostic potential of volume - rendering , in particular volume - rendered ( vr ) and curved vr ( cvr ) reconstructions obtained from isotropic data in the diagnosis of atypical acute appendicitis with a 16 - slice mdct scanner . lappendicite acuta rappresenta oltre il 50% di tutte le cause di addome acuto e richiede una diagnosi e un trattamento chirurgico tempestivo [ 1 ]  . 
nel 20%30% dei casi , il quadro clinico di presentazione pu essere caratterizzato da una variet di segni e sintomi che possono simulare altre patologie addomino - pelviche [ 3 ]  . 
in tal caso , le appendiciti acute vengono classificate come atipiche e rendono la diagnosi difficoltosa , con rischio di complicanze superiore al 20% [ 1 , 3 , 4 ]  . le appendiciti atipiche sono pi frequenti negli anziani , in et pediatrica , nelle donne in gravidanza , nei soggetti affetti da altre patologie ( diabete , morbo di crohn , patologia ovarica e tubarica ) e soprattutto nei pazienti con varianti anatomiche di sede dellappendice [ 5 ]  . 
in questo gruppo di soggetti , la diagnostica per immagini svolge un ruolo importante , riducendo il numero di laparotomie ed il rischio di complicanze [ 68 ]  . lecografia ( us ) rappresenta lindagine di prima istanza che consente , nei casi in cui lappendice sia in sede anatomica tipica , di riconoscere il processo infiammatorio o di escludere altre cause di addome acuto , raggiungendo unaccuratezza diagnostica compresa tra il 75% ed il 95% , basandosi sui dati riportati in letteratura [ 9 , 10 ]  . 
i falsi negativi , che possono raggiungere valori del 25% , si spiegano con la difficolt di individuare lappendice infiammata nelle forme con topografia anatomica atipica , specie se localizzata in sede pelvica o retrocecale [ 7 ]  . 
in tali casi la tomografia computerizzata ( tc ) la tecnica di studio pi utilizzata e con le apparecchiature spirali a singolo e multistrato pu raggiungere valori di accuratezza diagnostica compresi tra il 94% e il 100% , consentendo di determinare la sede , il decorso dellappendice infiammata e le eventuali complicanze [ 11 , 12 ]  . 
le apparecchiature tc multidetettore ( tcmd ) , in grado di acquisire immagini con spessori di strato al di sotto di 1 mm e con la medesima risoluzione spaziale lungo lasse z e nel piano assiale x - y , consentono di ottenere ricostruzioni su un piano coronale e sagittale della stessa qualit e dettaglio anatomico delle scansioni assiali . 
 pertanto , le ricostruzioni multiplanari possono essere utili per identificare il decorso dellappendice ed i rapporti anatomici con le strutture contigue , anche in pazienti con scarsa rappresentazione del tessuto adiposo endoaddominale [ 11 , 13 , 14 ]  . 
scopo del presente lavoro valutare le radiol med ( 2010 ) 115 : 93104 materials and methods luteum we retrospectively evaluated 45 patients ( 27 women and 18 men ) aged 2075 ( mean age 47 ) years who had come to our attention between march 2007 and september 2008 and had been examined with ct for abdominal pain , with a clinical and us suspicion of acute appendicitis . 
twelve patients were excluded from the study because they received a different diagnosis : terminal ileitis ( n = 2 ) , diverticulitis ( n = 2 ) , intestinal ischaemia ( n = 2 ) , colitis ( n = 1 ) , epiploic ( n = 1 ) , haemorrhagic corpus appendagitis ( n = 1 ) , ureteral lithiasis ( n = 1 ) , salpingitis ( n = 1 ) and cholecystitis ( n = 1 )  . 
in three cases , it was mild appendicitis ( two with normal position , one with retrocecal location ) and in 30 it was complicated appendicitis ( 17 with normal position , 13 with abnormal position )  . 
we also selected as the control group ten patients ( six women and four men , mean age 52 years ) with a negative ct examination and a favourable clinical course . 
in six cases , the appendix had normal position whereas in four the position was abnormal ( three medial and one retrocecal )  . all patients were examined using an mdct scanner ( tsx - 101a - aquilion 16 , toshiba medical system , tokyo , japan ) with the following scan parameters : slice thickness 1 mm ; pitch 1.75 ; increment 1 mm ; tube rotation time 0.5 s ; kv / mas 120 / 250 . 
the scans were performed with the patient supine from the diaphragmatic domes to the pubic symphysis before and after injection of intravenous nonionic , uroangiographic contrast material ( iomeron 400 ; bracco , milan , italy ) into the cubital vein with a 16to 18gauge needle connected to an automatic injector ( mk - iv , medrad , pittsburgh , pa , usa )  . 
the duration of postprocessing was approximately 10 m the axial and reconstructed images of our 43 patients ( 33 with acute appendicitis and ten in the control group ) were read by two blinded radiologists with more than 6 months experience in potenzialit diagnostiche delle ricostruzioni volumetriche , in particolare volume rendering ( vr ) e vr curve ( vrc ) , ottenute da dati isotropici , nella diagnosi di appendicite acuta atipica , utilizzando una apparecchiatura tcmd a 16 strati . materiali e metodi sono stati valutati retrospettivamente 45 pazienti ( 27 donne e 18 uomini ) , di et compresa tra i 20 e i 75 anni ( et media 47 anni ) , pervenuti alla nostra osservazione tra marzo 2007 e settembre 2008 e sottoposti ad esame tc per algie addominali , con quadro clinico ed ecografico dubbio per appendicite acuta . 
dodici pazienti sono stati esclusi dallo studio in quanto stata effettuata diagnosi di altra patologia : ileite terminale ( n = 2 ) , diverticolite ( n = 2 ) , ischemia intestinale ( n = 2 ) , colite ( n = 1 ) , corpo luteo emorragico ( n = 1 ) , appendicite epiploica ( n = 1 ) , calcolosi ureterale ( n = 1 ) , salpingite ( n = 1 ) e colecistite ( n = 1 )  . 
in 3 casi si trattava di mild appendicitis ( 2 a sede tipica ed 1 retrocecale ) e in 30 di complicated appendicitis ( 17 a sede tipica e 13 a sede atipica )  . 
sono stati inoltre selezionati 10 pazienti ( 6 donne e 4 uomini , et media 52 anni ) con quadro tc negativo e decorso clinico favorevole , che hanno rappresentato il gruppo controllo . 
in 6 casi , lappendice era normosituata , mentre in 4 aveva sede atipica ( 3 mediale ed 1 retrocecale )  . tutti i pazienti sono stati esaminati con una apparecchiatura tcmd tipo tsx - 101a ( aquilion 16 , toshiba medical system , tokio , giappone ) utilizzando i seguenti parametri di acquisizione : spessore di strato 1 mm ; pitch 1 , 75 ; increment 1 mm ; tempo di rotazione del tubo 0 , 5 s ; kv / mas 120 / 250 . 
le scansioni sono state condotte con paziente in decubito supino , dalle cupole diaframmatiche alla sinfisi pubica , prima e dopo iniezione endovenosa di mezzo di contrasto ( mdc ) uroangiografico non ionico ( iomeron 400 , bracco , milano , italia ) , iniettato nella vena cubitale attraverso un ago da 1618 gauge con iniettore automatico ( mk - iv , medrad , pittsburgh , pennsylvania , us ) e con i seguenti parametri : volume 1 , 5 ml / kg di peso corporeo ( valore massimo di 110 ml ) e velocit di iniezione 3 ml / s . 
le immagini sono state acquisite durante la fase porto - venosa ed il ritardo di inizio delle scansioni stato determinato automaticamente attraverso un bolus radiol med ( 2010 ) 115 : 93104 the use of the reconstruction software . 
both readers initially assessed the axial images and 2 months later the vr and cvr images , for the following parameters : presence and location of the appendix wall thickness , considered pathological when > 3 mm wall enhancement , considered altered when increased compared with adjacent loops luminal distension , graded mild ( 57 mm ) or marked ( > 10 mm ) periappendiceal fat morphology , considered heterogeneous in the presence of dense streaks presence or absence of appendicolith presence of free air and / or periappendiceal intraand retroperitoneal collections in both the axial scans and vr images , the identification of normal wall thickness , with mildly dilated appendiceal lumen and homogeneous periappendiceal fat , allowed distinction of mild from complicated appendicitis , as reported in the literature [ 1 , 1419 ]  . statistical analysis the results were entered into a database ( excel for office 2000 ; microsoft , redmond , wa , usa ) and analysed to calculate the inter - reader concordance by using cohens kappa statistic : poor concordance ( < 0.01 ) ; low concordance ( = 0.010.20 ) ; moderate concordance ( = 0.210.40 ) ; good concordance ( = 0.410.60 ) ; substantial concordance ( = 0.610.80 ) ; almost perfect concordance ( = 0.811.00 ) [ 20 ]  . 
le immagini assiali e quelle ricostruite dei 43 pazienti ( 33 con appendicite acuta e 10 del gruppo controllo ) sono state valutate in cieco da due radiologi con esperienza di utilizzo del software di ricostruzione superiore a 6 mesi . 
entrambi gli esaminatori hanno valutato inizialmente le immagini assiali e a distanza di 2 mesi le immagini vr e vrc , considerando i seguenti parametri : presenza e sede dellappendice ; spessore di parete , considerato patologico quando > 3 enhancement parietale , considerato alterato quando aumentato rispetto alla anse adiacenti ; distensione del lume , con aumento di grado lieve ( 57 mm ) o marcato ( > 10 mm ) ; morfologia del tessuto adiposo periappendicolare , considerato disomogeneo in presenza di strie dense ; presenza o assenza di appendicolita ; presenza di aria libera e / o raccolte periappendicolari intrae retroperitoneali . sia nelle scansioni assiali che nelle immagini in vr , il riconoscimento di uno spessore di parete normale , con lieve dilatazione del lume appendicolare ed omogeneit del tessuto adiposo periappendicolare , ha permesso di distinguere le forme di appendicite lieve da quelle di appendicite complicata , come riportato da alcuni autori in letteratura [ 1 , 1419 ]  . analisi statistica tables 1 and 2 show the ct alterations detected in the 43 patients , as assessed by both radiologists on the axial images and vr images . 
complicated appendicitis was diagnosed in 26 / 28 cases : the appendix had a normal position in 15 cases and i risultati ottenuti sono stati raccolti in un database ( excel per office 2000 ; microsoft corporation ; redmond , washington ) ed analizzati per calcolare la concordanza tra i due lettori mediante test statistico di kappa di cohen : ( < 0 , 01 ) , bassa concordanza scarsa concordanza ( = 0 , 010 , 20 ) , discreta concordanza ( = 0 , 210 , 40 ) , buona concordanza ( = 0 , 410 , 60 ) , sostanziale concordanza ( = 0 , 610 , 80 ) , concordanza quasi perfetta ( = 0 , 811 , 00 ) [ 20 ]  . 
in 9 / 43 casi ( 21% ) stata esclusa una diagnosi di appendicopatia sia con le immagini assiali che con quelle ricostruite ; si trattava di pazienti appartenenti al gruppo controllo , correttamente considerati esenti da appendicite . il radiologo pi esperto ha riconosciuto unappendicopatia in 31 / 43 casi ( 72% ) valutando le sole immagini assiali ; in 3 / 31 si trattava di appendicite lieve con appendice a disposizione tipica in 2 casi e retrocecale in 1 caso ed in 28 / 31 stata diagnosticata una appendicite complicata con appendice : 15 in sede tipica , 10 in sede atipica ( 3 pelviche , 2 retrocecali , 2 laterali , 2 mediali ed 1 sottoepatica ) , 2 in sede tipica e parzialmente riconoscibili e 1 non riconoscibile . 
il ricorso alle immagini ricostruite ha confermato la diagnosi di appendicopatia in tutti i 31 casi . in 2 / 43 ( 5% ) casi sulla base delle sole immagini assiali non stata riconosciuta lappendicopatia . 
le ricostruzioni in vrc sul piano sagittale ( c ) e coronale ( d ) consentono una migliore valutazione della sede e dellestensione dellappendice a decorso mediale ( frecce )  . not be made on either the axial or reconstructed images . these were two complicated forms in which only the intraperitoneal effusion was identified . 
these patients belonged to the control group and were correctly considered free from appendicitis . the experienced radiologist recognised an appendiceal disease in 31 / 43 cases ( 72% ) by evaluating the axial images only . 
in 3 / 31 cases , it was mild appendicitis , with the appendix in normal location in two cases and retrocecal in one case , whereas in 28 / 31 cases , it was complicated appendicitis , with the appendix in normal location in 15 cases , atypical location in ten cases ( three pelvic , two retrocecal , two lateral , two medial and one infrahepatic ) , in a typical and partially recognisable location in two cases and not recognisable in one case . 
in one case , vr reconstructions helped in the diagnosis of a complicated form of appendicitis , with an unrecognisable appendix due to heterogeneous periappendiceal fat , free coprolith in the pelvic cavity and stercoral peritonitis . 
these ricostruzioni in vr hanno agevolato la diagnosi di una forma complicata con appendice non riconoscibile per la presenza di disomogeneit del grasso periappendicolare , coprolita libero nello scavo pelvico e peritonite stercoracea ; nellaltro caso , le ricostruzioni non hanno invece consentito di porre la diagnosi poich erano solo presenti versamento e raccolte endoaddominali . 
in 10 / 43 casi ( 23% ) stata esclusa una appendicopatia sia con le immagini assiali che con quelle ricostruite ; si trattava dei pazienti appartenenti al gruppo controllo , correttamente considerati esenti da appendicite . 
 nella tabella 3 sono riportati per ogni radiologo i valori di sensibilit , specificit , accuratezza diagnostica , vpp e vpn nella diagnosi di appendicite acuta atipica , ottenuti valutando le immagini assiali e ricostruite . 
dal confronto tra le immagini assiali e quelle in vr , laccuratezza diagnostica nella valutazione delle appendiciti acute atipiche stata per il radiologo meno esperto del 84% per le immagini assiali e 93% per quelle in vr , mentre per il radiologo pi esperto rispettivamente del 95% e 98% . 
il grado di concordanza tra i due radiologi nella diagnosi di appendicite acuta atipica stata nelle immagini assiali di = 0 , 73 mentre in quelle ricostruite di = 0 , 87 . discussione laccuratezza nella diagnosi di appendicite acuta varia in radiol med ( 2010 ) 115 : 93104 fig . 
il tessuto adiposo periappendicolare disomogeneo ( testa di freccia ) e si associa modica quota di versamento ( asterisco )  . le ricostruzioni vrc sagittale ( c ) e coronale ( d ) consentono di riconoscere il decorso dellappendice a sede pelvica e preileale ( frecce )  . patients belonged to the control group and were rightly considered free of appendicitis . table 3 shows the sensitivity , specificity , diagnostic accuracy , ppv , and npv values in the diagnosis of atypical acute appendicitis obtained by assessing axial and reconstructed images . 
comparison between the axial and vr images yielded a diagnostic accuracy in the evaluation of atypical acute appendicitis by the less experienced radiologist of 84% for the axial images and of 93% for the vr images , whereas the values were 95% and 98% , respectively , for the more experienced reader . 
the concordance between the two radiologists in the diagnosis of atypical acute appendicitis was = 0.73 for the axial images and = 0.87 for the reconstructed images . discussion accuracy of the diagnosis of acute appendicitis varies according to age and gender , with a range of 78%92% in men and 58%85% in women . 
in these cases , an incorrect or delayed diagnosis is not only related to the atypical clinicallaboratory presentation , but also to anatomical variation in funzione dellet e del sesso , con un range pari al 78%92% negli uomini e 58%85% nelle donne . 
queste differenze riflettono le difficolt diagnostiche nei pazienti anziani , nelle giovani donne e nei bambini , in cui il quadro clinico pu essere atipico e simulare altre patologie [ 1 ]  . 
in questi casi , la diagnosi errata o tardiva legata non solo alla presentazione clinico - laboratoristica atipica , ma anche alle varianti anatomiche di sede dellappendice [ 21 ]  . pertanto , in tali forme , il ricorso a metodiche di imaging come lus e la tc consente una maggiore percentuale di diagnosi corrette e riduce il tasso di mortalit [ 4 , 6 , 7 , 12 , 22 ]  . 
tali studi sono stati effettuati con apparecchiature tc spirale a singolo detettore che , sebbene consentano una visualizzazione panoramica delle strutture addomino - pelviche , spesso non permettono di visualizzare lorigine ed il decorso dellappendice o di individuare piccoli appendicoliti per i limiti legati al rapporto tra volume da analizzare e risoluzione spaziale lungo lasse z [ 24 , 25 ]  . 
la recente introduzione delle apparecchiature multidetettore ha consentito di superare questi limiti , incrementando notevolmente la velocit di acquisizione di volumi sempre pi ampi , con riduzione degli artefatti da movimento e maggiore qualit delle ricostruzioni multiplanari ( mpr ) e vr per effetto dei voxel isotropici [ 26 ]  . 
3a - d mild appendicitis : axial scans ( a , b )  . mildly thickened and enhancing appendiceal walls ; the diameter of the appendiceal lumen does not exceed 7 mm ( arrows )  . 
le ricostruzioni vrc sagittale ( c ) e coronale ( d ) consentono una migliore valutazione della sede retrocecale dellappendice ( teste di freccia )  . the location of the appendix [ 21 ]  . 
in such cases , the use of imaging methods such as us and ct provides a higher rate of correct diagnoses and reduces mortality rates [ 4 , 6 , 7 , 12 , 22 ]  . 
comparative studies of ct and us have highlighted the higher sensitivity and diagnostic accuracy of ct [ 12 , 16 , 23 ]  . these studies were performed with single - detector spiral ct scanners that , although providing a panoramic view of the abdominal / pelvic structures , often fail to visualise the origin and course of the appendix or small appendicolith because of limitations related to the relationship between the volume to be analysed and z - axis resolution [ 24 , 25 ]  . 
the recent introduction of multidetector devices has overcome these limitations , significantly improving the acquisition rate of increasingly extensive volumes , reducing motion artefacts and improving the quality of multiplanar reconstructions ( mpr ) and vr by using isotropic voxels [ 26 ]  . 
some papers in the literature report experiences with mdct and mpr reconstructions in the identification of normal appendices and in the diagnosis of appendiceal diseases [ 11 , 13 , 2729 ]  . nevertheless , although mpr reconstructions are widely used in clinical practice , they are 2d images that only allow evaluation of structures within the reconstruction plane . 
furthermore , the quality of the reconstructed image is often reduced by the noise generated by thin - slice acquisitions , similar to those obtained when using devices with more than 16 deteclavori presenti in letteratura hanno riportato esperienze eseguite con tc multidetettore e ricostruzioni mpr nel riconoscimento di appendici normali e nella diagnosi di appendicopatia [ 11 , 13 , 27 29 ]  . 
tuttavia , anche se le ricostruzioni mpr sono quelle pi utilizzate nella pratica clinica , sono immagini bidimensionali che consentono solo la valutazione di strutture comprese nel piano di ricostruzione . 
per garantire una migliore qualit dellimmagine possibile utilizzare ricostruzioni in vr e vrc che comprendono lintero volume dei dati acquisiti e forniscono una migliore definizione dei contorni e del decorso delle strutture anatomiche in relazione alla variazione dei valori di opacit ( da 0% a 100% ) ed alla posizione rispetto al punto di vista [ 30 ]  . 
pertanto , le ricostruzioni di volume possono essere impiegate per valutare i rapporti spaziali dellappendice normale o patologica rispetto alle strutture adiacenti . in questo studio si cercato di confrontare i risultati ottenuti nella diagnosi di appendicite acuta atipica da due radiologi con diversa esperienza , che hanno valutato inizialmente le singole immagini assiali e successivamente , dopo 2 mesi , le ricostruzioni in vr . 
coronal ( b ) and sagittal ( c ) vr reconstructions and the sagittal ( d ) cvr reconstruction shows appendix in normal location ( arrowheads ) with thickened and enhancing walls and its relationship with the abscess collection . 
le ricostruzioni vr coronale ( b ) , sagittale ( c ) e vrc sagittale ( d ) mostrano unappendice in sede tipica con pareti ispessite , iperemiche ( teste di frecce ) ed i rapporti con la raccolta ascessuale . 
to ensure a higher image quality , vr and cvr reconstructions can be used that comprise the entire volume of the acquired data and provide improved definition of the outlines and course of anatomical structures in relation to variation in opacity values ( between 0% and 100% ) and to the relative position to the point of view [ 30 ]  . 
thus , vr reconstructions can be used to evaluate the spatial relationships of a normal or pathological appendix with adjacent structures . in this study we attempted to compare the results obtained in the diagnosis of atypical acute appendicitis by two radiologists with different levels of experience who initially assessed the single axial images and then , after 2 months , the vr reconstructions . 
the sensitivity and specificity obtained with the axial images in the identification of disease were between 82% and 94% and between 91% and 100% , respectively , whereas the values obtained with the reconstructed images were between 94%97% and 91%100% , respectively . 
these results are similar to those described in previous studies and confirm the usefulness of vr reconstati selezionati un gruppo di pazienti , tutti affetti da appendicite con quadro clinico di presentazione atipico , ed un gruppo di pazienti considerato come controllo , al fine di non inficiare la validit statistica dei risultati . 
i valori di sensibilit e di specificit ottenuti con le immagini assiali nel riconoscimento di malattia sono stati rispettivamente compresi tra l82% ed il 94% e tra il 91% ed il 100% ; mentre per le immagini ricostruite i valori ottenuti sono stati 94%97% ed 91%100% . 
tali risultati sono paragonabili a quelli riscontrati in precedenti studi ed avvalorano lutilit delle ricostruzioni in vr , ottenute con tcmd nello studio dei pazienti con sospetto clinico di appendicite [ 11 ]  . considerando tuttavia il numero di casi in cui la patologia stata riconosciuta con le sole immagini assiali e successivamente con quelle ricostruite , i risultati ottenuti sono stati differenti per i due lettori , soprattutto in relazione ai diversi anni di esperienza . 
dei 33 casi di appendicite atipica , il radiologo meno esperto ne ha diagnosticate soltanto 27 nelle immagini assiali e 31 nelle immagini ricostruite . pertanto le immagini assiali hanno mostrato una minore accuratezza diagnostica rispetto alle immagini ricostruite ( 84% vs 93% )  . 
lutilizzo delle ricostruzioni in vr ha fornito 102 radiol med ( 2010 ) 115 : 93104 table 3 atypical appendicitis : sensitivity ( sens ) , specificity ( spec ) , accuracy ( acc ) , positive predictive value ( ppv ) and negative predictive value ( npv ) in evaluating axial and reconstructed images obtained by the less and more experienced radiologists axial images sens spec reconstructed images spec sens less experienced radiologist more experienced radiologist 100% 95% 100% 100% 100% tabella 3 appendicite atipica : valori di sensibilit ( sens ) , specificit ( spec ) , accuratezza ( acc ) , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) nella valutazione delle immagini assiali e ricostruite per il radiologo meno esperto e per quello con maggiore esperienza immagini assiali sens spec immagini ricostriute sens spec radiologo meno esperto radiologo pi esperto 100% 95% 100% 100% 100% structions obtained with mdct in the study of patients with a clinical suspicion of appendicitis [ 11 ]  . 
however , considering the number of cases in which the disease was recognised with axial images only , and later with the reconstructed images , the results obtained were different for the two readers , especially in relation to the different years of experience . 
vr reconstructions provided better results , as they enabled identification of signs of appendiceal diseases such as the presence of obstructing appendicolith , evaluation of the relationship of the appendix with adjacent structures , visualisation of its course and location . 
indeed , vr reconstructions only proved useful in one case of complicated appendicitis with stercoral peritonitis in which , although the appendix was not recognisable due to widespread necrosis , the diagnosis was guided by the presence of a free appendicolith in the pelvic cavity . 
by contrast , in another case of complicated appendicitis associated with stercoral peritonitis in which the cause of luminal obstruction was unrelated to an appendicolith , the diagnosis of appendicitis could not be established owing to the absence of other signs . analysis of our results indicates that the two methods of image visualisation have different degrees of accuracy in identifying atypical acute appendicitis . 
indeed , given the panoramic capabilities of vr reconstructions , these proved very accurate in evaluating the extent of complicated appendicitis , with accuracy values of 93% and 98% for the less risultati migliori in quanto ha permesso di evidenziare alcuni segni di appendicopatia come la presenza di appendicoliti ostruenti , di valutare i rapporti dellappendice con le strutture adiacenti , di seguirne il decorso e riconoscerne la sede . 
infatti le ricostruzioni in vr si sono rivelate utili solo in un caso di appendicite complicata con peritonite stercoracea , in cui anche se lappendice non era riconoscibile per la necrosi estesa , la presenza di un appendicolita libero nello scavo pelvico ha permesso di indirizzare la diagnosi . al contrario , in un altro caso di appendicite complicata associata a peritonite stercoracea , in cui la causa dellostruzione del lume non era legata ad appendicoliti , non stato possibile ipotizzare la diagnosi di appendicite per la mancanza di altri segni . 
infatti per la loro panoramicit , le ricostruzioni in vr si sono rivelate molto accurate nel bilancio di estensione delle appendicite complicata con valori di accuratezza pari a 93% e 98% rispettivamente per il radiologo meno esperto e per quello pi esperto . 
nei casi di appendicite lieve , le vr sono state di aiuto solo per il radiologo con minore esperienza , in quanto hanno permesso di riconoscere la sede ed i segni di appendicopatia di grado lieve , rimasti misconosciuti nelle immagini assiali . 
 nellanalisi quantitativa , la concordanza raggiunta tra i due lettori nella diagnosi di appendicite atipica stata maggiore per le ricostruzioni in vr ( = 0 , 87 ) che per le radiol med ( 2010 ) 115 : 93104 and the more experienced radiologist , respectively . 
in the cases of mild appendicitis , vr images were only helpful for the less experienced radiologist in that they allowed correct recognition of the location and signs of mild appendiceal disease , unlike the axial images . 
 in the quantitative analysis , inter - reader concordance in diagnosing atypical appendicitis was greater in vr reconstructions ( = 0.87 ) than in axial images ( = 0.73 ) ; hence , despite the different levels of experience , the reconstructions provided almost identical results in the recognition of appendiceal diseases . 
 some of these considerations also emerge from the results of previous studies that underline the value of mpr associated with axial images in diagnosing appendicitis , with sensitivity and specificity values of 92%96% and 93%95% , respectively [ 11 , 27 ]  . 
reconstructed images were evaluated 2 months after axial images ; hence , the two readers , when evaluating reconstructed images , were not influenced by any immediately preceding analysis of axial images . 
this aspect further corroborates the results obtained with the vr technique , which provides improved spatial and contrast resolution in identifying location , relationships with adjacent organs and extremely tortuous course of the inflamed appendix compared with mpr . 
our results show that vr reconstructions were particularly useful to the less experienced radiologist , whereas they helped the more experienced reader in a few selected cases only . one limitation of our study is the two radiologists different experience in the use of reconstruction software , especially in changing the preset opacity curves , which can produce high - quality images [ 31 ]  . 
nonetheless , we believe that this limitation did not greatly affect the diagnosis of appendiceal diseases . immagini assiali ( = 0 , 73 ) ; pertanto nonostante i diversi anni di esperienza , le ricostruzioni hanno permesso di ottenere risultati pressoch sovrapponibili nel riconoscimento dellappendicopatia . alcune di tali considerazioni emergono anche dai risultati di studi riportati in letteratura in cui viene sottolineato il valore delle ricostruzioni multiplanari associate alle immagini assiali nella diagnosi di appendicite , con valori di sensibilit e specificit rispettivamente del 92%96% e del 93%95% [ 11 , 27 ]  . 
infatti le immagini ricostruite sono state valutate dopo 2 mesi dallanalisi delle immagini assiali ed i due lettori non sono stati pertanto influenzati nella valutazione delle ricostruzioni dallanalisi ravvicinata delle immagini assiali . 
questo aspetto avvalora maggiormente i risultati ottenuti con tecnica vr che fornisce una migliore risoluzione spaziale e di contrasto nellevidenziare la sede , i rapporti con gli organi adiacenti ed il decorso molto tortuoso di appendici infiammate rispetto alle ricostruzioni multiplanari . 
in base ai risultati ottenuti nel nostro lavoro , le ricostruzioni in vr si sono dimostrate particolarmente utili per il radiologo con minor esperienza , mentre nel radiologo pi esperto sono state di aiuto solo in casi selezionati . un limite del nostro studio rappresentato dal diverso grado di esperienza nellutilizzo del software di ricostruzione da parte dei due radiologi , soprattutto nel variare le curve di opacit preimpostate , che consentono di ottenere immagini di elevata qualit [ 31 ]  . 
our experience suggests that the use of vr reconstructions obtained with 16 - slice ct allows better evaluation of location , course and relationships with adjacent organs of the appendix , both in mild and in complicated appendicitis . 
however , given the small number of patients enrolled in our retrospective study , further studies conducted on a larger sample of patients are needed to establish the real diagnostic value and impact of reconstructions in diagnosing atypical appendicitis in relation to the readers experience . le immagini assiali ottenute con tcmd forniscono una diagnosi accurata di appendicopatia atipica . 
la nostra esperienza suggerisce che lutilizzo delle ricostruzioni in vr ottenute con apparecchiatura tc a 16 detettori consente una migliore valutazione della sede , del decorso e dei rapporti con gli organi adiacenti sia nelle lievi che nelle appendicite complicata . 
sono stati inclusi nel nostro studio 86 pazienti con lesione sospetta della mammella inviate allesecuzione di risonanza magnetica ( rm ) mammaria presso il nostro dipartimento da settembre 2005 a settembre 2007 . 
il diametro medio delle lesioni stato di 26 , 02 mm ( range : 490 mm ) , di cui 52 con diametro 15 mladc medio del tessuto ghiandolare normale stato di 1 , 55103 mm2 / s . 
il valore di adc sembra un parametro aggiuntivo promettente nella distinzione tra lesioni maligne e benigne della mammella . parole chiave coefficiente di diffusione apparente mammella diffusione lesioni risonanza magnetica introduction since the introduction of dimeglumine contrast agent , magnetic resonance imaging ( mri ) of the breast has undergone major technological and clinical developments , becoming a valuable diagnostic tool in breast evaluation [ 16 ]  . 
in the literature , mri is associated with a 95%99% sensitivity for invasive cancer detection , 80% for in situ cancer detection and 100% negative predictive value ( npv ) for invasive forms . 
the main limit of breast mri is its specificity , on average 80% , even though a large mismatch is reported , ranging from 37% to 97% [ 3 , 4 , 714 ]  . in recent years , different parameters have been evaluated to increase the specificity and accuracy of breast mri [ 7 , 8 ]  . morphological and dynamic study of the lesion [ 9 , 12 ] , use of high spatialtemporal resolution sequences [ 13 , 14 ] , use of alternative contrast agents ( gadobenate dimeglumine vs . gadopentate dimeglumine ) [ 15 ] and clinical application of 3 - tesla mr units [ 16 , 17 ] have been analysed . 
an important scientific application of mri concerns the use of functional sequences such as spectroscopy [ 1821 ] , diffusion that , and perfusion neuroimaging [ 2022 ] , now have an important diagnostic role in the other body systems [ 2326 ]  . initially employed imaging diffusion - weighted imaging ( dwi ) examines the random thermal motion ( brownian motion ) of water molecules , depending on their kinetic energy [ 2327 ]  . 
dwi preserves an intrinsic t1 , dp ( protonic density ) and especially t2weighed components and provides quantitative and qualitative information about water molecule diffusion in a tissue ( high or low diffusion )  . 
the adc value quantifies the limited and less randomised water diffusion in a tissue [ 27 ]  . in a biological tissue , water molecule diffusion includes brownian motion ( incoherent motion ) and capillary blood circulation ( coherent motion )  . 
dwi was acquired using echo - planar sequences where intensity and temporisation of diffusion - sensitive gradients are modified by varying the diffusion - sensitising factor ( b - value ) ; generally b - value ranged from 500 to 1 , 500 s / mm2 . 
the use of high b - value ( at least 1 , 000 s / mm2 ) reduces perfusion effects in adc measurements [ 27 ]  . the water diffusion in a tissue depends on fluid viscosity and membrane permeability between the intraand extracellular component , active transport and direction of structures that impede or enhance mobility . 
the study of water molecule diffusion could offer information about tissue characteristics and behaviour [ 28 ]  . radiol med ( 2010 ) 115 : 5169 introduzione dallintroduzione del mezzo di contrasto , la risonanza magnetica ( rm ) della mammella ha avuto notevoli sviluppi tecnologici e clinici diventando una accurata metodica nella diagnosi della patologia mammaria [ 16 ]  . 
diversi articoli in letteratura riportano valori di sensibilit del 95%99% per il carcinoma infiltrante , dell80% per il carcinoma duttale in situ ( cdis ) e un valore predittivo negativo del 100% per il carcinoma infiltrante . 
il principale limite della rm mammaria la sua specificit che , allo stato attuale , circa 80% , con un range che varia tra 37% e 97% [ 3 , 4 , 714 ]  . nei recenti anni sono stati studiati diversi parametri nel tentativo di incrementare la specificit e laccuratezza della rm mammaria [ 7 , 8 ]  . 
sono state analizzate le caratteristiche morfologiche e dinamiche delle lesioni [ 9 , 12 ] , luso di sequenze ad alta risoluzione spazio - temporale [ 13 , 14 ] , luso di mezzi di contrasto alternativi ( gadobenato dimeglumina vs gadopentato dimeglumina ) [ 15 ] , lapplicazione clinica di apparecchiature da 3 tesla [ 16 , 17 ]  . unimportante applicazione scientifica della rm riguarda luso di sequenze funzionali quali la spettroscopia [ 1821 ] , la perfusione , limaging di diffusione , che , inizialmente usato in neuroradiologia [ 2022 ] ha assunto ultimamente un importante ruolo diagnostico in altri distretti corporei [ 2326 ]  . limaging pesato in diffusione ( dwi ) esamina il movimento casuale ( moto browniano ) delle molecole dacqua , che dipende dalla loro energia cinetica [ 23 , 27 ]  . 
le immagini di diffusione conservano unintrinseca componente di pesatura in t1 , dp e soprattutto t2 , e forniscono informazioni di tipo quantitativo e qualitativo sul grado di diffusivit delle molecole dacqua in un dato tessuto ( alta o bassa diffusivit )  . 
il valore di adc quantifica la diffusione pi limitata e meno casuale delle molecole dacqua in un tessuto [ 27 ]  . nei tessuti biologici , la diffusivit delle molecole dacqua include il movimento browniano ( movimento incoerente ) e la circolazione sanguigna nei capillari ( movimento coerente )  . 
la dwi viene acquisita usando una sequenza echo - planare dove lintensit e la temporizzazione dei gradienti di diffusione sono modificate variando il fattore di sensibilizzazione alla diffusione ( valore di b ) ; generalmente il valore - b varia da 500 a 1500 s / mm2 . 
luso di alti valori di b ( almeno 1000 s / mm2 ) riduce gli effetti della perfusione nella misura delladc [ 27 ]  . la diffusivit dellacqua nei tessuti dipende dalla viscosit dei fluidi e dalla permeabilit delle membrane tra le componenti intraed extra - cellulare , dal trasporto attivo e dalla direzione delle strutture che impediscono o accentuano la mobilit . 
lo studio della diffusivit delle molecole dacqua potrebbe offrire importanti informazioni sulle caratteristiche tissutali [ 28 ]  . radiol med ( 2010 ) 115 : 5169 recent papers have demonstrated the possibility of performing adc measurements in breast tissue and the presence of an important difference between adc of normal and pathological breast tissue [ 2836 ]  . the purpose of this study was to investigate the ability of dwi and the adc in detecting and characterising breast lesions . 
secondly , we analysed the adc value of benign and malignant lesions and normal breast tissue and compared the adc value of different lesions with the pathological diagnosis . materials and methods from september 2005 to september 2007 , all patients with a breast lesion detected at mammography and / or ultrasound who underwent breast mri in our department were studied with the same mri protocol , including dwi sequence . 
as a specific negative result , we considered cytological samples with no atypical characteristics and compatible with complicated cysts , fibroadenoma , galactocele , liponecrosis , inflammation such as granuloma , and fibrocystic modifications such as apocrine metaplasia . 
in cases in which the results of fine - needle aspiration were positive for malignancy or not definitive , fnab or surgical excision and subsequent histological examination were performed , as in our usual protocol . 
patients with incomplete mri , pathological diagnosis obtained elsewhere , or who underwent mri during / after neoadjuvant chemotherapy were excluded from this study . mri protocol mri was performed using a 1.5 - t unit with 23 mt / m gradient intensity ( signa excite ; ge medical system , mi , usa ) , with the women in the prone position using a dedicated breast coil . 
in all patients , the following sequences were acquired : short - tau inversion recovery ( stir ) axial sequence : repetition time ( tr ) = 5 , 900 , echo time ( te ) = 68 , echo train length ( etl ) = 17 , bandwidth 4167 , matrix = 320288 , studi recenti hanno dimostrato la possibilit di effettuare misure di adc nel tessuto mammario e la presenza di unimportante differenza tra il valore adc del tessuto mammario normale e patologico [ 2836 ]  . lo scopo di questo lavoro stato quello di valutare lutilit della dwi e delladc nella individuazione e caratterizzazione delle lesioni mammarie . 
obiettivo secondario dello studio stato quello di analizzare il valore delladc delle lesioni mammarie benigne e maligne rispetto al parenchima normale , e confrontare i valori adc delle differenti lesioni con la diagnosi isto - patologica . materiali e metodi da settembre 2005 a settembre 2007 , tutti i pazienti con lesione sospetta della mammella inviati allesecuzione di rm mammaria presso il nostro dipartimento , hanno eseguito uno stesso protocollo di studio che includeva una sequenza di diffusione . 
i risultati dellagoaspirato sono stati accettati come diagnosi definitiva solo in casi di diagnosi specifica di lesione benigna o maligna ; sono stati considerati non definitivi in caso di discordanza tra imaging e risultato citologico o in caso di materiale insufficiente o presenza di cellule epiteliali normali . 
stato considerato negativo un risultato citologico senza evidenza di atipie e compatibile con cisti complicata , fibroadenoma , galattocele , liponecrosi , infiammazioni quali i granulomi e modificazioni fibrocistiche quali la metaplasia apocrina . 
 protocollo rm tutti gli esami sono stati eseguiti su una apparecchiatura da 1 , 5 t e gradiente di campo magnetico 23 mt / m ( signa advantage ; ge medical system , milwakee usa ) , con paziente in posizione prona e mammelle alloggiate in una bobina di superficie bilaterale dedicata . 
sono state utilizzate le seguenti sequenze : assiale short - tau inversion recovery ( stir ) [ repetition time ( tr ) = 5900 , echo time ( te ) = 68 , echo train lenght ( etl ) = 17 , bandwidth 4167 , matrice 320288 , spessore 4 mm , intervallo 0 , field of view ( fov ) 3234 , number of excitations ( nex ) 12 ] ; assiale dwi ( tr = 5150 , te = min , matrice 9696 , spessore 4 mm , intervallo 0 , fov 3234 , nex 4 )  . 
before analysing the dwi sequences , we localised and classified every lesion detected in the conventional sequences using the breast imaging reporting and data system ( bi - rads ) [ 9 ]  . subtracted images , maximum intensity projection ( mip ) and multiplanar reconstruction ( mpr ) functions were obtained from dynamic sequences and studied in cine loop . with postprocessing software that showed signal intensity changes in a given point of space in time ( functool programme ) , the region of interest ( roi ) was selected and a dynamic curve was obtained . 
the relative signal intensity changes in time ( percent signal intensity ) were calculated using the following formula : rsis = 100 ( sipostsipre ) / sipre ( where sipost is postcontrast signal intensity and sipre is precontrast signal intensity ) directly applied by the programme . 
then the dwi sequence was evaluated , and each hyperintensity area was studied and compared with all sequenza dwi stata ottenuta prima dellacquisizione delle sequenze dinamiche con una sequenza spin echo ( epi ) lungo il piano assiale . 
i gradienti di sensibilizzazione alla diffusione sono stati applicati nelle direzioni x , y , e z con valori b di 0 e 1000 secondi / mm2 ; coronali fast spoiled gradient echo ( fspgr ) 3d ( tr < 30 , te < 5 , fa = 15 , matrice 320320 , spessore 23 mm , intervallo 0 , fov 3438 , nex 0 , 5 ) , per un numero totale di 6 acquisizioni , una in condizioni di base , cinque dopo somministrazione ev di 0 , 1 mmol / kg di mdc ( gadobenato dimeglumina , bopta ) al flusso di 2 ml / s seguito dalliniezione di 20 ml di soluzione salina ; sagittale fspgr 3d ( tr < 30 , te < 5 , fa = 15 , matrice 288288 , spessore 23 mm , intervallo 0 , fov 2226 , nex 2 ) ; assiale fspgr 3d ( tr < 30 , te < 5 , fa = 15 , matrice 512256 , spessore 23 mm , intervallo 0 , fov 3438 , nex 2 ) ; per un tempo totale di esecuzione dellesame di circa 20 minuti . post - processing ed analisi dei dati le immagini rm sono state analizzate in consenso , da due radiologi con 10 ( autore mc ) e 20 ( autore pb ) anni di esperienza in imaging senologico , in cieco rispetto ai risultati istologici . 
prima dellanalisi della sequenza dwi abbiamo localizzato e classificato ogni lesione evidenziata nelle sequenze dinamiche usando il sistema breast imaging reporting and data system ( birads ) [ 9 ]  . 
sono state valutate le caratteristiche dinamiche di ogni singola lesione mediante luso di un software di processazione delle immagini ( functool ) in grado di valutare le modificazioni dellintensit di segnale di un determinato punto dello spazio in funzione del tempo . 
le modificazioni relative dellintensit di segnale nel tempo ( espressa in percentuale ) stata calcolata utilizzando la seguente formula : rsis = 100 ( sipostsipre ) / sipre dove sipost lintensit di segnale post - contrasto , sipre lintensit di segnale pre - contrasto , direttamente applicata dal programma . 
sono state successivamente analizzate le sequenze di diffusione e ogni area di iperintensit stata valutata a confronto con le immagini dello studio dinamico . le sequenze di diffusione sono state rielaborate ed stata visualizzata una mappa colore relativa alla distribuzione dei valori adc ; la mappa colore varia dal colore blu al rosso , con valori di adc da 0 , 000101 a 0 , 00250 , ove il colore blu rappresenta una scarsa diffusione delle molecole dacqua , ossia un valore di adc basso , e con colore rosso un ampio movimento delle molecole dacqua nei tessuti , ossia un valore di adc alto . 
the adc values of breast lesions and glandular tissue were calculated by using the following formula : adc = ( lns0lns ) / b ( where s0 is signal intensity obtained at b = 0 and s is signal intensity obtained at b = 1000 ) , directly applied by the programme . data and statistical analysis to evaluate the ability of dwi to detect breast lesions , we compared the number and the site of lesions shown on dynamic sequences with the hyperintense areas visualised on the dwi sequence . 
diagnostic sensitivity , specificity , accuracy , positive and negative predictive value ( ppv and npv ) of adc value in differentiating benign from malignant breast lesions were also calculated . results eighty - six patients ( 85 women and one man ; mean age 49.8 years , range 2384 years ) for a total of 126 breast lesions were considered in our study . 
lesions were classified using the bi - rads lexicon as follows : 95 in class v , 17 in class iv , 11 in class iii and 3 in class ii . 
malignant lesions included 13 in situ carcinomas , 12 lobular and 68 ductal invasive carcinomas , four poorly differentiated carcinomas , one malignant phyllodes , one papillary carcinoma and one mucinous carcinoma . 
benign lesions included nine fibroadenomas , three complicated cysts , four simple cysts , one benign phyllodes , one benign radial scar , three atypical ductal hyperplasia , one tubular adenoma , one intraductal papilloma , one nel parenchima ghiandolare normale controlaterale per ottenere il valore adc della ghiandola mammaria . 
le dimensioni delle roi utilizzate sono state inferiori a 100 pixel a seconda delle dimensioni della lesione , in modo tale da non comprendere aree cistiche e / o necrotiche . 
il valore adc stato calcolato usando la seguente formula : adc = ( lns0lns ) / b ( dove s0 lintensit di segnale ottenuta a b = 0 e s lintensit di segnale ottenuta a b = 1.000 ) , direttamente applicata dal programma . analisi statistica dei dati per valutare la capacit della dwi nella individuazione delle lesioni mammarie abbiamo confrontato il numero e la sede delle lesioni evidenziate nelle sequenza dinamiche con le aree di iperintensit visualizzate nella sequenza dwi . 
sono stati inoltre calcolati sensibilit , specificit , accuratezza , valore predittivo positivo e negativo del valore adc nel differenziare le lesioni benigne da quelle maligne . risultati sono stati inclusi nel nostro studio 86 pazienti ( 85 femmine e 1 maschio ; et media : 49 , 8 anni , range : 2384 anni ) per un totale di 126 lesioni mammarie . 
le lesioni sono state classificate secondo i criteri bi - rads come segue : 95 in classe v , 17 in classe iv , 11 in classe iii e 3 in classe ii . 
in particolare dei 100 tumori 13 erano carcinomi in situ , 80 carcinomi invasivi ( 68 duttali e 12 lobulari ) , 4 carcinomi scarsamente differenziati , 1 tumore filloide maligno , 1 carcinoma papillare e 1 carcinoma mucinoso . 
le 26 lesioni benigne comprendevano 9 fibroadenomi , 3 cisti complicate , 4 cisti semplici , 1 tumore filloide benigno , 1 radial scar , 3 iperplasie duttali atipiche , 1 adenoma tubulare , 1 papilloma intraduttale , 1 ginecomastia , 1 angioma gigante , 1 ascesso . il diametro medio delle lesioni stato di 26 , 02 mm ( range : 490 mm , deviazione standard : 20 , 04 mm , mediana : 17 , 5 mm ) , di cui 52 lesioni avevano diametro minore o uguale a 15 m delle 52 lesioni di diametro minore o uguale a 15 mm , 35 si sono dimostrate lesioni maligne e 17 benigne . 
le lesioni benigne comprendevano 8 fibroadenomi , 2 cisti semplici , 2 cisti complicate , 1 adenoma tubulare , 1 iperplasia duttale tipica , 1 tumore filloide benigno , 1 radial scar e 1 papilloma intraduttale . 
il diametro medio delle roi utilizzate per la misura del valore adc stato di radiol med ( 2010 ) 115 : 5169 gynaecomastia , one giant angioma and one abscess . 
conventional mri was negative in one case . in this case , dwi showed the presence of a small diffusion area with an adc value of 1.180.10103 mm2 / s , corresponding to a cluster of microcalcifications ( 8 mm in size ) detected at mammography . 
 31 , 7614 , 74 pixel ( range : 1290 ) , corrispondente a 50 , 4224 , 10 mm2 ( range : 18147 )  . la capacit di individuazione della dwi stata di 124 / 126 ( sensibilit 98 , 4% )  . 
questo valore stato ottenuto usando la stessa roi usata per la misura delle lesioni ( media : 31 , 7614 , 74 pixel che corrisponde ad unarea di 51 , 07 mm2 )  . 
a total of 124 measurements ( one for each contralateral lesion measurement ) of normal glandular tissue were obtained . the nonparametric mann - whitney u test showed a significant statistical difference between adc values of glandular tissue and lesions , with a p value < 0.0001. 
le lesioni maligne hanno mostrato valori adc pi bassi rispetto alle lesioni benigne con un differenza statisticamente significativa ( p < 0 , 0001 ) secondo il test non parametrico di mann - withney u . 
la tabella 2 riassume i valori medi di adc del tessuto ghiandolare normale e delle principali lesioni benigne e maligne della mammella . la capacit delle sequenza dwi nella individuazione delle lesioni di diametro minore o uguale a 15 mm stata del 100% e il valore di adc differenzia bene le lesioni benigne da quelle maligne . 
in questo sottogruppo di lesioni il valore adc delle lesioni benigne ( valore medio di 1 , 59103 mm2 / s e range di 2 , 090 , 41103 ) stato significativamente ( p < 0 , 001 ) pi alto di quello delle lesioni radiol med ( 2010 ) 115 : 5169 fig . 
table 2 summarises the mean adc values of normal glandular tissue and the main benign and malignant breast lesions . the detection rate of the dwi sequence in lesions 15 mm was 100% . 
grazie allimpiego del mezzo di contrasto e al suo potere di risoluzione spaziale la rm ha dimostrato unelevata sensibilit nella individuazione e nella caratterizzazione del carcinoma della mammella [ 26 ]  . 
esistono tuttavia ancora delle difficolt nel differenziare alcune lesioni benigne ( quali le modificazioni iperplastiche , la metaplasia apocrina , e alcuni tipi di fibroadenoma ) da quelle maligne , sia usando lapproccio morfologico che dinamico , a causa di una sovrapposizione di patterns tra la proliferazione iperplastica di tipo benigno e il processo proliferativo maligno [ 714 ]  . 
le sequenze convenzionali non sono in grado di dare informazioni sullambiente cellulare ( quantit e architettura cellulare ) tralasciando un parametro di non poca importanza quale il grado di proliferazione cellulare . limaging di diffusione potrebbe rappresentare un potenziale metodo per ottenere informazioni sulla struttura tissutale attraverso la misura della diffusivit delle molecole dacqua . 
conventional mri sequences do not provide information about the cellular environment ( cellular amount and arrangement ) , thus lacking an important index of tumour grade . dwi represents a potential method to obtain tissue structure information from the measurement of water molecule diffusion . 
several studies have demonstrated that cystic lesions show high adc values due to loss of restriction of water molecules , whereas malignant lesions show lower adc values due to altered tissue architecture [ 26 , 29 , 33 ]  . probably , the presence of a large number of packed cells and a reduced extracellular volume in malignant lesions inhibit water motion [ 26 , 33 ]  . 
these same studies report a progressive decrease in adc value in benign lesions , noninvasive carcinoma ( pure or predominant ) and invasive carcinoma [ 26 , 29 , 31 , 33 ]  . 
 our study confirms the ability of the dwi sequence to detect lesions within normal breast tissue ; an excellent correspondence between the hyperintense areas in dwi and breast lesions was shown in 124 / 126 cases . 
in all these cistiche mostrano elevati valori di adc a causa della perdita di restrizione delle molecole dacqua mentre le lesioni maligne mostrano valori di adc pi bassi a causa di una alterata architettura tissutale [ 26 , 29 , 33 ]  . 
gli stessi studi riportano un progressivo decremento del valore adc tra lesioni benigne , carcinomi non invasivi e carcinomi invasivi [ 26 , 29 , 31 , 33 ]  . 
 il nostro studio conferma innanzitutto la capacit della sequenza di diffusione di evidenziare la presenza di lesioni nel contesto del normale tessuto ghiandolare mammario ; in 124 / 126 casi stata dimostrata unottima corrispondenza tra le aree di iperintensit evidenziate in dwi e le lesioni identificate nelle sequenze convenzionali . 
la sequenza dwi non ha identificato correttamente due lesioni , nonostante sia stata in grado di evidenziare una piccola lesione maligna , che risultava invisibile nelle sequenze convenzionali ( un piccolo carcinoma duttale senza enhancement )  . 
la sequenza di diffusione ( c ) identifica correttamente la lesione e la mappa adc ( d ) mostra un valore di 1 , 13103 mm2 / s nella regione di interesse . cases , the difference between breast lesions and surrounding normal glandular tissue was clear . 
the dwi sequence missed the lesion in two cases only ; on the other hand , it was the only sequence able to detect a lesion that was invisible on the dynamic sequence ( a small invasive ductal carcinoma without enhancement )  . 
a significant difference between the adc values of glandular tissue and malignant lesions ( 1.55103 mm2 / s vs 0.97103 mm2 / s ) confirms the few data reported in the literature [ 2634 ]  . 
the different cellular architecture between normal gland and cancer , especially in cellular density and extracellular fraction volume , could explain this difference in statisticamente significativa tra il valore adc delle lesioni maligne e il parenchima ghiandolare normale , e tra le lesioni benigne e quelle maligne . 
il nostro lavoro dimostra una significativa differenza tra il valore adc del tessuto ghiandolare e quello delle lesioni maligne ( 1 , 55103 mm2 / s vs 0 , 97103 mm2 / s ) confermando i pochi dati riportati in letteratura [ 2634 ]  . 
la differente architettura cellulare tra ghiandola normale e cancro , soprattutto in densit cellulare e in volume extra - cellulare , potrebbe spiegare la differenza dei relativi coefficienti di diffusione [ 31 ]  . 
alcuni autori hanno mostrato alcune differenze statisticamente significative tra il valore adc dei carcinomi in situ e dei carcinomi invasivi , probabilmente a causa della differenza in densit cellulare , inferiore nelle forme in situ [ 29 , 30 ]  . 
la sequenza sagittale t1 post - contrasto ( a ) mostra una piccola area di enhancement allinterno di un dotto dilatato con curva dinamica di tipo plateau ( b )  . 
la sequenza dwi ( c ) visualizza la piccola massa e la mappa adc ( d ) mostra un valore di 1 , 55103 mm2 / s . diffusion coefficient [ 31 ]  . 
in our study , the mean adc value of malignant lesions was 0.97103 mm2 / s , similar to that reported in the other studies ( table 3 )  . 
a few authors showed some significant difference between the adc values of in situ carcinomas and invasive carcinomas , probably caused by different cellular density that is lower in the in situ forms [ 29 , 30 ]  . 
missed detection of some cases of malignant lesions has also been reported evidenziato tutte le lesioni maligne eccetto un caso di carcinoma lobulare invasivo di 30 mm a distribuzione sparsa . 
in their series ( 76 and 190 patients ) , they found a mean adc value for normal glandular tissue > 2103 mm2 / s ( using a 0750 s / mm2 b value and a 10mm roi diameter ) [ 30 , 31 ] , and they proposed a threshold value of 1.6103 mm2 / s to discriminate normal tissue from malignant lesions . 
il valore adc medio del tessuto ghiandolare normale ottenuto nel nostro studio pi basso rispetto a quello riportato negli studi di woodhams [ 32 , 33 ] ( 1 , 55 vs 2 , 0 ) , probabilmente in rapporto al diverso protocollo di studio e / o alla differente popolazione in esame . utilizzando il valore di threshold proposto da woodhams et al . 
 [ 32 , 33 ] ( 1 , 6103 mm2 / s ) nella nostra casistica , la dwi in grado in grado di caratterizzare correttamente 95 / 99 lesioni maligne e 14 / 25 lesioni benigne con un valore di sensibilit del 97% , di specificit del 56% , di accuratezza del 89% , e con valore predittivo positivo ( vpp ) e negativo radiol med ( 2010 ) 115 : 5169 fig . 
mip axial reconstruction ( a ) and coronal dynamic sequence ( b ) show a diffuse area of inhomogeneous abnormal enhancement in the right breast with progressive curve ( c )  . 
ricostruzione mip assiale ( a ) e sequenza coronale dinamica ( b ) che mostrano , nella mammella destra , una diffusa area di alterato e disomogeneo enhancement con curve dinamiche di tipo graduale ( c )  . 
la sequenza dwi ( d ) e la mappa adc ( e ) mostrano un valore molto basso nella regione di interesse ( 0 , 69103 mm2 / s )  . study protocols or / and different study populations . applying the threshold value proposed by woodhams et al . 
 [ 32 , 33 ] ( 1.6103 mm2 / s ) to distinguish normal from pathological tissue in our series , dwi was able to correctly characterise 95 / 99 malignant lesions and 14 / 25 benign ( vpn ) rispettivamente del 90% e del 18% . 
usando in alternativa un valore soglia di 1 , 4103 mm2 / s , la dwi si dimostra in grado di caratterizzare correttamente 93 / 99 lesioni maligne e 18 / 25 lesioni benigne : si riduce il numero di falsi positivi e i valori di sensibilit , specificit ed accuratezza radiol med ( 2010 ) 115 : 5169 fig . 
la sequenza dwi ( c ) mostra unarea diffusa di disomogenea iperintensit e la mappa adc ( d ) mostra un valore di 1 , 08103 mm2 / s nella regione di interesse . lesions with 97% sensitivity , 56% specificity , 89% accuracy , 90% ppv and 18% npv . 
in small lesions , we observed an increase in specificity but a decrease in sensitivity and accuracy . in our series , mean adc value of benign lesions ( 1.66103 mm2 / s vs 1.55103 mm2 / s ) were shown to be higher than those measured in normal glandular tissue . 
the mean adc values of fibroadenomas ( 1.64103 mm2 / s ) and cystic lesions ( 1.98103 mm2 / s ) were similar to those diventano rispettivamente del 94% , 72% e 90% . 
per le lesioni con diametro inferiore ai 15 mm i valori di sensibilit , specificit ed accuratezza sono del 65% , 92% e 83% , aumenta quindi la specificit ma diminuiscono sensibilit e accuratezza . nella nostra casistica il valore adc medio delle lesioni benigne ( 1 , 66103 mm2 / s vs 1 , 55103 mm2 / s ) stato pi elevato rispetto a quello misurato nel tessuto ghiandolare normale . 
il valore medio adc dei fibroadenomi ( 1 , 64103 mm2 / s ) e delle lesioni cistiche ( 1 , 98103 mm2 / s ) simile a quello riportato da guo et al . 
 [ 29 ] usando un valore b di 01000 il valore adc medio dei fibroadenomi e delle cisti stato rispettivamente di 1 , 57103 mm2 / s e 2 , 35103 mm2 / s . 
la sequenza dwi ( c ) identifica la massa e la mappa adc ( d ) mostra un valore adc di 1 , 63103 mm2 / s nella regione di interesse . reported by guo et al . 
in guos study [ 29 ] , which used a 01 , 000 b value , the mean adc value for fibroadenomas and cysts was 1.57103 mm2 / s and 2.35103 mm2 / s , respectively . 
the mean adc value for these benign lesions was 1.67103 mm2 / s , but the mean adc value for the 2 fibroadenomas was 1.1103 mm2 / s , significantly lower than that measured in our series [ 31 ]  . high adc values ( high diffusion ) in fibroadenomas could be due to stromal myxoid change and consequent higher water mobility [ 28 ]  . 
sebbene la media dei valori di adc per lesioni benigne stata 1 , 67103 mm2 / s , i 2 fibroadenomi avevano valori di 1 , 1103 mm2 / s , decisamente pi bassi delle restanti lesioni e anche pi bassi rispetto ai valori da noi riscontrati . 
gli alti valori di adc e quindi lelevata diffusivit delle molecole di acqua nei fibroadenomi possono dipendere dalle modificazioni mixoidi dello stroma che determinano una minore restrizione della mobilit dellacqua [ 28 ]  . 
anche in altri tipi di patologia benigna sostenuti prevalentemente da modificazioni infiammatorie si possono riscontrare valori adc piuttosto bassi e questo a causa dellelevata cellularit , della presenza di radiol med ( 2010 ) 115 : 5169 table 1 pathology results in relation to the bi - rads classes ( ii , iii , iv , v ) and to adc values ( 103 mm2 / s ) lesion adc mean median 90 / 91 sd , standard deviation ; adh , atypical ductal hyperplasia ; dcis , ductal carcinoma in situ ; idc , invasive ductal carcinoma ; ilc , invasive lobular carcinoma tabella 1 reperti istologici in relazione alle classi bi - rads ( ii , iii , iv , v ) e al valore adc ( 103 mm2 / s ) lesione adc media mediana fibroadenomas simple cysts complex cysts tubular adenoma benign phyllodes radial scar papilloma angioma abscess gynaecomastia total benign lesions dcis poorly diff . 
low adc value measured in complicated cysts and in the only abscess lesion observed in our series could be explained by granulomatous inflammatory elements , fibrous components and hemosiderin catabolites . leucociti e di fibrosi [ 30 ]  . 
further studies , with larger and more homogeneous case series and new technological developments , are necessary to assess the role of diffusion imaging in breast diagnosis . strutturali del tessuto mammario normale e patologico . lanalisi qualitativa dellimaging di diffusione sembra rappresentare un nuovo metodo nella individuazione e caratterizzazione delle lesioni mammarie . 
il nostro studio , che si allinea ai preliminari risultati presenti in letteratura , ha dimostrato come il valore adc possa essere usato come ulteriore parametro nella diagnosi differenziale tra lesioni benigne e maligne della mammella . 
ricci2 1divisione di abdominal imaging and intervention , dipartimento di radiologia , brigham & womens hospital , harvard medical school , 75 francis street , boston , ma 02115 , usa 2dipartimento di scienze radiologiche , policlinico umberto i , universit la sapienza , v.le regina elena 324 , 00167 roma , italy 3dipartimento di dermatologia , policlinico umberto i , universit la sapienza , roma , italy 4dipartimento di scienze radiologiche , campus biomedico , roma , italy 5department of radiology , universit degli studi di verona , verona , italy 6dipartimento di radiologia , clinica las condes , lo fontecilla 441 , las condes , santiago , chile correspondence to : v . 
between 2002 and 2005 , ten women with fascioliasis were admitted to the brigham and womens hospital , harvard medical school ( bwh ) , with abdominal pain and mild fever . 
in all patients ( 10 / 10 , 100% ) , us showed parenchymal heterogeneity characterised by multiple subcapsular and peribiliary hypoechoic nodular lesions that were ill - defined and coalesced into tubular or tortuous structures . 
in six patients ( 6 / 10 , 60% ) , the lesions appeared hypoechoic , whereas in four patients ( 4 / 10 , 40% ) , there was an alternation of hyperechoic and hypoechoic nodules . on ct , all patients ( 10 / 10 , 100% ) showed hypodense patchy lesions in subcapsular , peribiliary or periportal locations , which coalesced to form tubular structures and were more evident during the portal phase . 
lesion diameter ranged from 2 cm to 7 ccapsular enhancement was seen in four cases on ct ( 4 / 10 , 40% ) and in one also at mr imaging . 
la nostra casistica comprende 10 pazienti di sesso femminile , ricoverate presso il brigham and womens hospital harvard medical school ( bwh ) , tra il 2002 ed il 2005 , con dolori addominali e febbricola , studiate retrospettivamente nel 2007 . 
in tutte le pazienti lecografia evidenziava ecostruttura epatica marcatamene disomogenea , caratterizzata dalla presenza di aree nodulari ipoecogene confluenti in cordoni tubulariformi , scarsamente definite , localizzate prevalentemente in sede sub - capsulare e peribiliare . 
la tc confermava in tutti i pazienti la presenza di numerose aree ipodense sub - capsulari , peri - portali o peribiliari , confluenti in cordoni tubulariformi , caratterizzate da contorni irregolari , ipodense , pi cospicue durante la fase portale . 
alla rm , disponibile in due soli pazienti , sono state confermate le aree di disomogeneit parenchimale con reperto di iperintensit nelle immagini t2 - pesate e da lieve e periferico enhancement dopo somministrazione di gadolinio . 
la fascioliasi epato - biliare , seppur rara , dovrebbe essere messa in diagnosi differenziale , in presenza del corretto scenario clinico , soprattutto in pazienti provenienti da aree ad alta endemia . 
some cases have also occurred in europe ( france , united kingdom , spain , portugal ) as a result of the consumption of raw vegetables grown on irrigated or flooded land ( watercress )  . fascioliasis mainly affects the hepatobiliary system , where it manifests in two stages : the hepatic ( acute and invasive ) stage , and the biliary ( chronic and obstructive ) stage [ 1 , 2 ]  . 
the acute stage , which appears 24 months after infection , is characterised by nonspecific symptoms . during the hepatic acute phase , the flukes cross the smallbowel mucosa into the peritoneal cavity and spread within the liver . 
because of the nonspecific manifestations and symptoms abdominal pain and fever fascioliasis may be confused with a wide spectrum of hepatobiliary conditions , resulting in delayed treatment [ 2 , 3 ]  . 
although the definitive diagnosis relies on serological tests or detection of fluke eggs in the stool or in material obtained via endoscopy , percutaneous la fascioliasi uninfezione da parassita causata dalla fasciola epatica . 
occasionalmente si hanno piccole epidemie di fascioliasi umana soprattutto in bolivia , ecuador , per , cuba , egitto ; alcune stime parlano di 2 milioni di individui infestati nel mondo . 
si hanno casi anche in europa ( francia , regno unito , spagna , portogallo ) , causate dal consumo di ortaggi crudi cresciuti in terreni irrigati o allagati ( crescione )  . 
 questa infestazione colpisce principalmente il sistema epatobiliare e si manifesta in due stadi : lo stadio epatico ( acuto ed invasivo ) e lo stadio biliare ( cronico ed ostruttivo ) [ 1 , 2 ]  . 
lo stadio acuto , che si presenta da due a quattro mesi dopo linfezione , caratterizzato da sintomi non specifici . durante questa fase le fasciole attraversano la mucosa dellintestino tenue fino alla cavit peritoneale e si diffondono nel fegato . 
data la non specificit delle manifestazioni e dei sintomi , come il dolore addominale e la febbre , la fascioliasi pu essere confusa con un ampio spettro di malattie epatobiliari e , per questo motivo , il suo trattamento viene spesso iniziato tardivamente [ 2 , 3 ]  . 
sebbene lanalisi sierologica o lidentificazione delle uova nelle feci , per via endoscopica o con aspirazione della bile per via percutanea , o con prelievo citologico , sia necessaria per una diagnosi radiol med ( 2010 ) 115 : 8392 bile drainage or cytological sampling [ 4 , 5 ] , imaging also plays a key role in the study of fascioliasis , as it is capable of providing an accurate early provisional diagnosis [ 2 , 6 , 7 ]  . we present the ultrasound ( us ) , computed tomography ( ct ) , magnetic resonance ( mr ) imaging and endoscopic retrograde cholangiopancreatography ( ercp ) findings of ten cases of hepatobiliary fascioliasis and discuss the role and pitfalls of each technique in the diagnosis . materials and methods our study population included ten women ( age range 3258 years ; mean age 45 ) admitted to the brigham and womens hospital , harvard medical school ( bwh ) for abdominal pain and low - grade fever between 2002 and 2005 and whose records were retrospectively reviewed in 2007 . 
liver function tests demonstrated slightly elevated alkaline phosphatase ( 400500 u / l ) , gamma - gt ( 70100 u / l ) , c - reactive protein ( 4065 mg / l ) and erythrocyte sedimentation rate ( 80110 mm after the first hour ) in six patients and normal values in the remaining four patients . all patients underwent us and ct before and after administration of iodinated contrast material ; two were also studied by mr imaging and mr cholangiopancreatography ( mrcp ) ( after ct ) and one by ercp . 
two patients subsequently underwent liver biopsy . abdominal us was performed with digital scanners ( esaote technos mpx , genoa , italy ; toshiba aplio , osaka , japan ) equipped with a high - resolution convex - array broadband probe . 
abdominal ct was performed with spiral multidetector row scanners ( volume zoom or sensation 16 , siemens medical solutions , erlangen , germany ) before and 6070 s after intravenous administration of 100 ml of iopromide 300 mgi / ml ( ultravist - 300 , berlex lab , madison , wi , usa ) at a 3.0 ml / s flow rate . 
 sono di seguito riportati i reperti ecografici , tc , rm e ercp di dieci casi di fascioliasi epatobiliare e discusso il ruolo e i limiti delle singole metodiche nella sua diagnosi . materiali e metodi la nostra casistica comprende 10 pazienti di sesso femminile di et compresa tra 32 e 58 anni ( et media : 45 anni ) , ricoverate presso il brigham and womens hospital harvard medical school ( bwh ) , tra il 2002 ed il 2005 , con dolori addominali e febbricola , studiate retrospettivamente nel 2007 . 
otto hanno riferito di aver ingerito acqua o crescione contaminato . tutte le pazienti sono state sottoposte ad analisi di laboratorio , come il test elisa igg , emoagglutinazione di fissazione del complemento diretto e la reazione intradermica per la fasciola . 
i test di funzionalit epatica evidenziavano un lieve incremento della fosfatasi alcalina ( 400500 u / l ) , ggt ( 70100 u / l ) , della proteina c reattiva ( 4065 mg / l ) , e della ves ( 80110 mm dopo la prima ora ) in sei pazienti , mentre sono risultate nei limiti della norma nelle restanti quattro pazienti . 
tutte le pazienti sono state sottoposte a esame ecografico e tc prima e dopo somministrazione di mdc iodato , due anche ad esame rm e cprm ( dopo lesame tc ) e una anche a cpre . 
due di esse sono state sottoposte successivamente a biopsia epatica . lesame ecografico addominale stato eseguito con apparecchiature digitali ( esaote technos mpx , genova , italia ; toshiba aplio , osaka , giappone ) dotate di sonda convex ad ampia banda ad alta risoluzione . 
lesame tc delladdome stato eseguito con apparecchiature spirale multidetettore ( volume zoom or sensation 16 , siemens medical solutions , erlangen , germania ) prima e dopo 6070 s dalla somministrazione di mdc iv di 100 ml di 300 mg i / ml di iopromide ( ultravist - 300 , berlex lab , madison , wi , usa ) , a una velocit di flusso di 3 , 0 ml / s . 
stata usato spessore di sezione di 5 mm e un intervallo di 5 m lesame rm stato eseguito con apparecchiatura da 1 , 5 t ( magnetom vision plus ; siemens medical solutions , erlangen , germania ) provvista di bobina phased - array . 
il protocollo di esame prevedeva sequenze t2 - pesate ( tr / te infinito / 90 ; flip angle 150 ; tempo di acquisizione 25 s ; spessore di fetta 6 mm ; gap 0.25% ; matrice 256160 ; fov radiol med ( 2010 ) 115 : 8392 erlangen , germany ) equipped with a phased - array coil . 
in four patients ( 4 / 10 ; 40% ) , us identified the presence of parasites , which appeared as elongated , mildly hyperechoic , mobile and floating structures ranging in size from 6 mm to 22 min four patients ( 4 / 10 ; 40% ) , us demonstrated moderate biliary dilatation associated with thickening of the gallbladder wall . at ct , the lesions appeared hypodense and without significant contrast enhancement during the portal phase in all patients ( 10 / 10 ; 100% )  . 
in two patients ( 2 / 10 ; 20% ) periportal oedema , hilar lymphadenopathy and mild splenomegaly were also seen . two patients were also studied with mr imaging and mrcp . 
in quattro pazienti ( 4 / 10 ; 40% ) lecografia identificava la presenza dei parassiti , che apparivano come immagini di forma allungata , debolmente iperecogene , mobili e flottanti , con dimensioni comprese fra 6 e 22 m inoltre , in quattro pazienti ( 4 / 10 ; 40% ) stata rilevata allecografia modesta dilatazione delle vie biliari associata con ispessimento della parete colecistica . 
1a - f le immagini ecografiche rivelano ( a , b ) ecostruttura disomogenea del fegato , con noduli ipoecogeni scarsamente definiti , localizzati prevalentemente in zona sub - capsulare . 
la rm rivela masse sub - capsulari sparse , di aspetto iperintenso nelle sequenze t2 pesata ( c ) con enhancement periferico e della capsula glissoniana dopo somministrazione di gadolinio ( d )  . 
a distanza di una settimana le immagini della tc rivelano la presenza di estese aree ipodense a partire dalla capsula glissoniana in direzione della vena porta , senza interessamento n invasione diretta della vena porta n delle sovraepatiche ( e , f )  . radiol med ( 2010 ) 115 : 8392 fig . 
le immagini ecografiche mostrano disomogeneit del parenchima epatico ( d , e ) con presenza di molteplici noduli ipoecogeni , a margini mal definiti , alternati a molteplici noduli iperecogeni . 
allecografia ( c , d ) , si rende visibile il parenchima epatico disomogeneo con presenza di aree iperecogene sub - capsulari associate a molteplici piccoli noduli ipoecogeni . alla cpre ( e ) si osservano piccoli difetti curvilinei di riempimento nel dotto biliare dilatato ( freccia ) , compatibili con parassiti endobiliari . 
all patients were successfully treated with triclabendazole . discussione discussion fascioliasis is a rare zoonotic disease caused by fasciola , a flat , leaf - like trematode that typically infects humans following the ingestion of water or water plants containing larvae [ 8 , 9 ]  . 
owing to the lack of specific clinical symptoms , human fascioliasis needs to be differentiated from other hepatic and biliary diseases , including acute hepatitis , neoplasms , visceral toxoplasmosis , biliary amoebiasis or other larval infections of the liver such as schistosomiasis [ 8 , 9 ]  . 
in the majority of cases , the diagnosis is difficult and is thus delayed both in the acute and chronic phases , as more common infections such as pyogenic liver abscesses and metastases are not easily distinguished from fascioliasis [ 10 ]  . 
the diagnosis can be confirmed by the finding of eggs or larvae in the stool and by the detection of antilarval antibodies on the elisa test , the sensitivity and specificity of which is approximately 90% . 
in any case , the antibodies only appear 24 weeks after infection [ 11 ]  . among the various imaging modalities , us has limited use during the acute phase , whereas ct angiography and mr imaging may be very helpful [ 6 ]  . 
us is also particularly useful for identifying the presence of parasites in the gallbladder and for studying the effects of medical treatment during the follow - up . ct helps to identify multiple or isolated hypodense nodular areas , tunnel - like branching or peripheral hypodensities with tortuous appearance as a result of parasite migration through the liver . 
involvement of the glisson capsule leads to capsular hyperintensity on t2 - weighted images at mr imaging [ 14 ] or capsular enhancement at ct angiography [ 15 ] or mr angiography . in one of our cases , multiple hyperintense lesions with peripheral contrast enhancement were seen on t2 - weighted sequences . 
ct , mr imaging and us may be valuable tools for evaluating response to treatla fascioliasi una rara malattia zoonotica , causata dal parassita trematode fasciola , dallaspetto simile ad una foglia di forma piatta , che colpisce tipicamente lessere umano a seguito di ingestione di acqua e di piante acquatiche che contengono le larve [ 8 , 9 ]  . 
a causa dellassenza di specificit dei sintomi clinici , la fascioliasi umana deve essere distinta da altre malattie epatiche e biliari , come lepatite acuta , le neoplasie , la toxoplasmosi viscerale , lamebiasi del tratto biliare o altre infezioni epatiche da larva quali la schistosomiasi [ 8 , 9 ]  . 
infatti , nella grande maggioranza dei casi , la diagnosi difficile e viene ritardata sia nella fase acuta che cronica , dato che affezioni pi comuni come gli ascessi piogenici del fegato e le metastasi non sono facilmente distinguibili dalla fascioliasi [ 10 ]  . 
la diagnosi pu essere confermata dal rilevamento di uova o larve nelle feci e dal rinvenimento di anticorpi anti - larva nel siero attraverso il test elisa , al quale si devono riconoscere sensibilit e specificit attorno al 90% . 
 tra i diversi metodi di diagnosi per immagini , gli ultrasuoni hanno scarsa utilit durante la fase acuta mentre angio - tc e rm possono esser molto utili per la diagnosi [ 6 ]  . 
luso dellecografia durante la fase avanzata di malattia pu aiutare a rilevare lesioni ipoecogene sparse nel parenchima , come riferito da kabaalioglu e andersen [ 12 , 13 ] e confermato in sei dei casi da noi esaminati , oppure ecogenicit variabile come riportata da han et al . 
lecografia anche particolarmente utile perch consente di identificare la presenza di parassiti allinterno della cistifellea e nel follow - up , per valutare gli effetti della terapia medica . lesame tc consente di identificare aree nodulari ipodense multiple o isolate , diramazioni cunicolari oppure ipodensit periferiche con aspetto tortuoso come risultato della migrazione dei parassiti attraverso il fegato : la presenza di questultimo segno una manifestazione evidente della malattia . 
si pu osservare , in particolare , che la maggioranza delle larve spargendosi , rimangono intrappolate nel parenchima sub - capsulare del fegato , dove muoiono producendo cavit replete di residui necrotici . linteressamento della capsula glissoniana determina liperintensit capsulare nelle immagini t2 - pesate in rm [ 14 ] , o lenhancement della capsula allangio - tc [ 15 ] o allangio - rm . 
ercp is also very useful in this phase on account of its accuracy in depicting curvilinear filling defects , which reveal the presence of flukes in the dilated biliary ducts , as seen in one of our cases [ 7 , 17 ]  . differentiation from other parasitic diseases may prove challenging on the basis of imaging studies alone , although the different parasitic diseases do have some specific features that allow for a diagnosis of exclusion . 
for example , the liver manifestations of chronic schistosomiasis include periportal thickening , which is depicted by us , and hypodense lesions with strong contrast enhancement , a finding that is not typically observed in fascioliasis . 
at ct , the main pathognomonic feature of schistosomiasis is the presence of calcified septations , which are usually perpendicular to the liver capsule ( hence the description of tortoise shell , or turtle back ) [ 18 ]  . 
other ct signs include capsular calcifications , junctional indentations or depressions , irregular liver margins and infiltration of periportal fat into the liver as a consequence of fibrosis and parenchymal retraction . 
mr imaging is unable to adequately depict these typical calcifications , although the fibrous septa do have abnormal signal intensity and appear hyperintense or hypointense on t1and t2 - weighted images , respectively [ 19 ]  . 
significant wall calcifications are present in 50% of cases [ 20 ] , and daughter cysts may be identified in approximately 75% of patients [ 20 ] , unlike what is seen in fascioliasis . 
furthermore , the presence of subcapsular branching tunnel - like areas is useful for distinguishing fascioliasis from ascariasis , which in such areas are usually absent . in conclusion , although rare , hepatobiliary fascioliasis should be considered in the differential diagnosis in the appropriate clinical scenario , especially in patients from highly endemic areas . 
diagnostic imaging in patients presenting with the typical features of the disease may help to formulate the correct diagnosis . strumento diagnostico molto utile in questa fase per laccuratezza nella identificazione di difetti curvilinei di riempimento , che rivelano la presenza di fasciole nei dotti biliari dilatati , come riportato in uno dei nostri casi [ 7 , 17 ]  . 
 la diagnosi differenziale rispetto ad altre parassitosi pu risultare difficoltosa con le sole indagini radiologiche , per quanto le diverse parassitosi abbiano alcuni peculiari aspetti , che consentono la diagnosi per esclusione . 
ad esempio le manifestazioni epatiche della schistosomiasi cronica includono lispessimento peri - portale , rilevabile con lecografia , e le lesioni ipodense , che dopo somministrazione di mdc presentano significativo enhancement , reperto che invece non si osserva tipicamente nella fascioliasi . 
alla tc , laspetto pi patognomonico della schistosomiasi la presenza di setti calcificati , solitamente allineati in modo perpendicolare rispetto alla capsula epatica ( da cui deriva la denominazione a tartaruga , oppure a schiena di tartaruga ) [ 18 ]  . 
altri segni individuati dalla tc comprendono calcificazioni della capsula , dentellature giunzionali o depressioni , profili epatici irregolari , estensione nel fegato del grasso peri - portale come conseguenza della fibrosi e della retrazione parenchimale . 
la rm non riesce a rivelare , con sufficiente accuratezza , queste calcificazioni caratteristiche , sebbene i setti fibrosi presentino anomale intensit di segnale , risultando iperintense od ipointense alle immagini t1 e t2 - pesate , rispettivamente [ 19 ]  . 
significative calcificazioni delle pareti sono presenti nel 50% dei casi [ 20 ] e cisti figlie sono individuabili in circa il 75% dei pazienti [ 20 ] , al contrario di quanto dato osservare nella fascioliasi . 
la presenza di aree ramificate con aspetto di tunnel sub - capsulare sono , inoltre , utili a distinguere la fascioliasi dall ascaridosi , che ne , invece , solitamente priva . in conclusione , la fascioliasi epato - biliare , seppur rara , dovrebbe essere messa in diagnosi differenziale , se in presenza del corretto scenario clinico , soprattutto in pazienti provenienti da aree ad alta endemia . 
gli aspetti imaging tipici della fascioliasi epatobiliare sono costituti da alterazioni nodulari disomogenee e confluenti in cordoni tubulariformi nel parenchima epatico , peri - porto - biliare o sub - capsulari con decorso tortuoso o serpiginoso . 
invasive thymomas were more likely to be greater in size ( p < 0.01 ) , with lobulated or irregular contours ( p < 0.02 ) , a necrotic or cystic component ( p < 0.04 ) , foci of calcification ( p < 0.05 ) and heterogeneous contrast enhancement ( p < 0.01 ) than were noninvasive thymomas . 
nel gruppo invasivo si sono riscontrati , con maggior frequenza , dimensioni maggiori ( p < 0 , 01 ) , margini lobulati o irregolari ( p < 0 , 02 ) , componente cistica o necrotica ( p < 0 , 04 ) , calcificazioni ( p < 0 , 05 ) ed enhancement disomogeneo ( p < 0 , 01 )  . 
la tc utile nel differenziare i timomi invasivi dalle forme non - invasive e riveste ruolo fondamentale nella corretta gestione terapeutica dei pazienti da indirizzare ai trattamenti neoadiuvanti lescissione chirurgica . 
inoltre la tc fornisce elementi predittivi di recidiva a distanza . radiol med ( 2010 ) 115 : 121 keywords computed tomography ( ct ) thymus thymoma tumour stage prognostic factors parole chiave tomografia computerizzata ( tc ) timo timoma stadio tumorale fattori prognostici introduction introduzione epithelial tumours of the thymus are the most common tumour in the anterior mediastinum , accounting for 30% of all masses in this anatomical region in adults and 20% of all mediastinal masses regardless of compartmental location [ 1 , 2 ]  . 
nonetheless , despite the benign histological appearance and the common finding of a complete and intact capsule at surgical excision , 30%60% of these tumours ( invasive thymomas ) are characterised by invasion of the capsule and the adjacent anatomical structures , multiple pleural or pericardial implants or , more rarely , by involvement of the retroperitoneum or lymph node and / or systemic spread [ 35 ]  . 
in 1981 , which subdivides thymomas into invasive and noninvasive [ 6 ]  . whenever possible , complete surgical resection is considered the treatment of choice , associated with adjuvant therapeutic protocols ( chemotherapy and / or radiotherapy ) in all cases classified as invasive after surgical resection [ 7 ]  . 
in recent years , multimodal treatment with the integration of neoadjuvant chemotherapy protocols has been proposed for the invasive forms to improve survival and reduce the risk of recurrence [ 813 ]  . 
in addition , preoperative induction chemotherapy and / or radiotherapy have been proposed to make possible radical surgery by downstaging the tumour and making resectable those cases initially not indicated for surgical treatment [ 14 ]  . 
as the masaoka classification is by definition postsurgical , computed tomography ( ct ) and magnetic resonance ( mr ) imaging ( for frankly invasive cases ) or the various cytohistological classifications proposed in recent decades are fundamental for the correct enrolment of patients to refer to neoadjuvant treatment regimens [ 1518 ]  . 
this classification distinguishes thymomas on the basis of the prevalence of the cellular subpopulation present ( cortical or medullary ) [ 19 , 20 ] and was subsequently revised by jeong et al . , who grouped thymomas into two subgroups ( lowand high - risk thymomas ) on the basis of the probability of invasive behaviour and tumour recurrence [ 21 ]  . 
these classification systems , however , possess no absolute prognostic value [ 2224 ] , as there is no unequivocal correlation le neoplasie epiteliali del timo rappresentano i tumori di pi frequente riscontro in mediastino anteriore , costituendo il 30% di tutte le masse di tale distretto anatomico in et adulta ed il 20% di tutti i tumori mediastinici indipendentemente dalla loro localizzazione compartimentale [ 1 , 2 ]  . 
tuttavia , nonostante laspetto citologico benigno ed il frequente riscontro di una capsula completa ed indenne allescissione chirurgica , il 30%60% di tali tumori ( timomi invasivi ) caratterizzato da invasione della capsula e delle strutture anatomiche contigue , da insemenzamento dei foglietti sierosi pleuro - pericardici o infine , evenienza comunque rara , da interessamento del retroperitoneo o da diffusione linfonodale e / o sistemica [ 35 ]  . 
la prognosi ed il rischio di recidiva a distanza correlano con linvasione extracapsulare , definita dalla classificazione anatomochirurgica proposta da masaoka nel 1981 , che suddivide i timomi in invasivi e non invasivi [ 6 ]  . 
una resezione chirurgica completa , ogni qual volta sia possibile , considerata il trattamento di scelta , associata a protocolli terapeutici adiuvanti ( chemioe / o radioterapici ) in tutti i casi classificati quali invasivi dopo resezione chirurgica [ 7 ]  . negli ultimi anni sono stati proposti per le forme invasive , al fine di migliorare la sopravvivenza e ridurre il rischio di recidiva a distanza , trattamenti multimodali con lintegrazione di protocolli chemioterapici neoadiuvanti [ 813 ]  . 
in aggiunta , trattamenti radioe / o chemioterapici prechirurgici di induzione sono stati proposti al fine di implementare le possibilit di radicalit chirurgica , sottostadiando la malattia , e di rendere resecabili casi inizialmente non candidabili allintervento chirurgico [ 14 ]  . 
essendo per definizione la classificazione di masaoka post - chirurgica , per il corretto arruolamento dei pazienti da indirizzare a regimi terapeutici neoadiuvanti sono fondamentali limaging mediante tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) , per i casi francamente invasivi , o le diverse classificazioni citoistologiche proposte negli ultimi decenni [ 1518 ]  . 
in particolare , allo stato dellarte , la pi utilizzata la classificazione proposta dallorganizzazione mondiale della sanit ( who ) nel 1999 e revisionata nel 2004 , che distingue i timomi in base alla prevalenza della sottopopolazione cellulare presente ( corticale o midollare ) [ 19 , 20 ] , successivamente semplificata dalla classificazione di jeong che raggruppa i timomi in due sottogruppi ( timomi a basso ed alto rischio ) in base alla probabilit di atteggiamento invasivo e di recidiva a distanza [ 21 ]  . 
i timomi ad radiol med ( 2010 ) 115 : 121 between the who classification and masaoka stage [ 21 , 2527 ] : 30% of low - risk thymomas and 60% of high - risk thymomas are found to be invasive after surgical resection [ 27 ]  . 
therefore , the preoperative distinction between invasive and noninvasive forms has important implications for the correct therapeutic strategy [ 28 ]  . various studies in the literature have described the ct characteristics of thymoma with reference to the who classification [ 21 , 2527 ]  . 
the aims of our study were : ( 1 ) to evaluate the efficacy of ct in distinguishing between invasive and noninvasive thymomas according to the masaoka classification ; and ( 2 ) to determine the existence at diagnosis of ct characteristics predictive of recurrence following thymectomy . alto rischio vengono selezionati per i trattamenti neoadiuvanti . 
questi sistemi di classificazione non possiedono comunque assoluto valore prognostico [ 2224 ] , dal momento che non esiste univoca correlazione tra classificazione who e stadio di masaoka [ 21 , 2527 ] : il 30% dei timomi a basso rischio ed il 60% di quelli ad alto rischio risultano invasivi dopo resezione chirurgica [ 27 ]  . 
quindi la distinzione preoperatoria tra forme invasive e non invasive ha importanti implicazioni ai fini della corretta strategia terapeutica [ 28 ]  . in letteratura esistono diversi studi che hanno descritto le caratteristiche tc dei timomi relazionandole alla classificazione who [ 21 , 2527 ]  . 
al contrario , sono estremamente limitate le informazioni disponibili riguardo la possibilit di distinguere , in base allimaging tc , i timomi non invasivi dalle forme invasive [ 28 ]  . 
all patients enrolled in the study satisfied the following inclusion criteria : ( 1 ) histopathological diagnosis of thymoma ; ( 2 ) ct examination performed within 4 weeks of surgical resection ; ( 3 ) absence of neoadjuvant treatment regimens prior to surgical resection ; and ( 4 ) surgical resection of the tumour . 
of the remaining 29 subjects , 22% reported chest pain ( 13 / 58 ) , 19% had signs and symptoms of myasthenia gravis ( mg , 11 / 58 ) and 7% suffered from symptoms due to compression of the mediastinal structures . the preoperative diagnosis was obtained by biopsy in popolazione di studio , criteri di eligibilit , presentazione clinica e valutazione istopatologica in un intervallo temporale di quasi 6 anni , compreso tra gennaio 2002 e settembre 2007 , 75 pazienti consecutivi con diagnosi bioptica di neoplasia epiteliale timica sono stati sottoposti a resezione chirurgica . 
la popolazione ha pertanto incluso complessivamente 58 soggetti , 28 di sesso maschile e 30 femminile , con unet media di 53 , 2 anni ( mediana 51 anni ; deviazione standard [ ds ] 17 , 0 anni con indice di confidenza [ ic ] 95% ; intervallo 2579 anni ; 25o - 75o percentile 3769 anni )  . il 52% dei soggetti ( 30 / 58 pazienti ) risultato asintomatico alla diagnosi ed il riscontro del tumore timico stato casuale , evidenziato da un esame radiografico convenzionale o di tomografia computerizzata eseguito per altre radiol med ( 2010 ) 115 : 121 90% of subjects ( 52 / 58 ) , with a percutaneous approach under ct guidance in 57% ( 33 / 58 ) and with surgical biopsy in 33% of cases [ mediastinoscopy 12 / 58 , video - assisted thoracoscopic surgery ( vats ) 5 / 58 , incisional biopsy 2 / 58 ]  . 
the remaining cases were referred directly to surgical excision without bioptic diagnosis given the high clinical suspicion of thymic tumour ( patients affected by mg with documented expansive mass in the anterior mediastinum at ct , which was considered surgically resectable given its small size and the presence of an intact fat plane separating the mass from the adjacent anatomical structures )  . 
in most cases ( 53 / 58 , 91% ) , radical surgical excision was possible with complete enucleation of the tumour , whereas in five patients , only partial resection was possible due to advanced invasion of the adjacent mediastinal structures and / or the thoracic wall or due to the presence of pleural implants . patient history , preand postoperative histopathological findings and ct findings were analysed for all cases in the study . 
 [ 6 ] , which is based on the presence and extension of extracapsular invasion in the adjacent mediastinal structures at the time of surgery , with subsequent confirmation at microscopic examination ( table 1 )  . 
adjuvant treatment following surgical resection in the form of radiotherapy and / or chemotherapy was administered to all patients with stage iiiiv disease ( 22 / 58 patients )  . 
dei restanti 29 soggetti , il 22% ha presentato dolore toracico ( 13 / 58 ) , il 19% segni e sintomi di miastenia gravis ( mg , 11 / 58 ) ed il 7% sintomi da compressione delle strutture mediastiniche . la diagnosi prechirurgica stata ottenuta attraverso prelievo bioptico nel 90% dei soggetti ( 52 / 58 ) : per via percutanea sotto guida tc nel 57% ( 33 / 58 ) ed attraverso biopsia chirurgica nel 33% ( mediastinoscopia 12 / 58 , video - assisted thoracoscopic surgery [ vats ] 5 / 58 , biopsia incisionale 2 / 58 ) ; i restanti casi sono andati direttamente allescissione chirurgica , in assenza di una diagnosi bioptica , in considerazione dellalto sospetto clinico di tumore timico ( pazienti affetti da miastenia gravis con documentata formazione espansiva del mediastino anteriore allindagine tc , ritenuta chirurgicamente enucleabile in considerazione delle piccole dimensioni e dellevidenza di un costante piano di clivaggio adiposo con le strutture anatomiche contigue )  . 
nella maggior parte dei soggetti ( 53 / 58 , 91% ) stata eseguita unescissione chirurgica radicale , con completa enucleazione della neoplasia , mentre in 5 pazienti stato possibile effettuare una resezione solo parziale a causa dellavanzata invasione delle strutture mediastiniche adiacenti e / o della parete toracica , o per la presenza di insemenzamento pleurico . le cartelle cliniche , i risultati istopatologici pree postintervento ed i dati radiologici tc sono stati analizzati per tutti i casi in studio . 
ogni tumore stato classificato secondo il sistema di stadiazione clinico - patologico proposto da masaoka [ 6 ] , sistema che si basa sulla presenza ed estensione dellinvasione extra - capsulare nelle strutture mediastiniche viciniore quale riscontro table 1 masaoka staging systema stage definition macroscopically encapsulated tumour , without microscopically detectable capsular invasion macroscopic invasion into surrounding mediastinal fatty tissue or mediastinal pleura microscopic invasion into the capsule macroscopic invasion into neighbouring organs , ( pericardium , great vessels , lung ) pleural or pericardial dissemination through direct extension or drop metastasis lymphogenous or haematogenous metastases stage i : noninvasive thymoma , stages iiiv : invasive thymoma afrom masaoka et al . 
 [ 6 ] , modified tabella 1 classificazione anatomo - chirurgica di masaokaa stadio definizione tumore macroscopicamente capsulato , senza evidenza microscopica di invasione della capsula invasione macroscopica nel tessuto adiposo circostante o a livello della pleura mediastinica invasione microscopica della capsula invasione macroscopica negli organi adiacenti ( pericardio , grossi vasi , polmone ) disseminazione pleurica o pericardica metastasi linfatiche od ematogene stadio i : timoma non invasivo ; stadio iiiv : timoma invasivo ada masaoka et al . 
 [ 6 ] , modificata radiol med ( 2010 ) 115 : 121 table 2 world health organization ( who ) histological classification of thymic epithelial tumours ( 2004 ) a type definition an organotypic thymic epithelial neoplasm composed of bland spindle / oval epithelial tumour cells with few or no lymphocytes an organotypic thymic epithelial neoplasm composed of a mixture of a lymphocyte - poor type a thymoma component and a more lymphocyte - rich type b - like component . 
both components are present in most sections a tumour of thymic epithelial cells with a histological appearance practically indistinguishable from the normal thymus composed predominantly of areas resembling cortex with epithelial cells scattered in a prominent population of immature lymphocytes and areas of medullary differentiation with or without hassalls corpuscles , similar to normal thymic medulla . some epithelial tumour cells present large nuclei of pale chromatin and small nucleoli an organotypic thymic epithelial neoplasm composed of large , polygonal tumour cells that are arranged in a loose network and exhibit large vascular nuclei with prominent large nucleoli , closely resembling the predominant epithelial cells of the normal thymic cortex . 
lymphocytes are less abundant than in type b1 an organotypic thymic epithelial neoplasm predominantly composed of medium - sized round or polygonal cells with slight nuclear atypia and some prominent nucleoli . 
the epithelial cells are mixed with a minor component of intraepithelial lymphocytes , resulting in a sheet - like growth of epithelial cells thymic carcinoma ( type c in 1999 who classification ) not included in the study . 
 [ 20 ] , modified tabella 2 classificazione istologica who delle neoplasie epiteliali del timo ( 2004 ) a tipo definizione tumore epiteliale timico composto da cellule epiteliali a morfologia ovalare affusolata con pochi o privi di linfociti tumore epiteliale timico composto da popolazioni cellulari del tipo - a ( variante povera di linfociti ) e del tipo - b , queste ultime caratterizzate da un maggior numero di linfociti . 
entrambe le componenti si riscontrano nella maggior parte delle sezioni istologiche . neoplasia composta da cellule epiteliali timiche con aspetto istologico indistinguibile dal normale tessuto timico e caratterizzata da aree simili alla corteccia , con cellule epiteliali sparse nel contesto di numerosi linfociti immaturi , ed aree di differenziazione midollare ( in presenza o meno di corpuscoli di hassall ) , simili alla normale midollare timica . 
in alcuni casi sono presenti cellule caratterizzate da voluminosi nuclei con aspetto a palizzata e piccoli nucleoli tumore epiteliale timico composto da voluminose cellule poligonali disposte in una rete a larghe maglie , caratterizzate da grandi nuclei e nucleoli , simili alle cellule epiteliali della normale corteccia timica . 
la componente linfocitaria meno rappresentata rispetto al tipo b1 tumore epiteliale timico composto prevalentemente da cellule rotondeggianti o poligonali di media taglia , con modeste atipie nucleari e qualche voluminoso nucleolo . 
tipo a , ab , b1 : timomi a basso rischio ; tipo b2 , b3 : timomi ad alto rischio ada mller - hermelink [ 20 ] , modificata of epithelial cells and the lymphocyte / epithelial cell ratio , recognises five different subtypes of thymoma ( a , ab , b1 , b2 , b3 ) and is summarised in table 2 . 
trattamenti terapeutici adiuvanti allescissione chirurgica , in diverse associazioni radioe / o chemioterapiche , sono stati somministrati a tutti i pazienti con stadio di malattia iiiiv ( 22 / 58 soggetti )  . 
la classificazione who [ 20 ] , basata sulla morfologia delle cellule epiteliali e sul rapporto linfociti / cellule epiteliali , riconosce cinque diversi sottotipi di timoma ( a , ab , b1 , b2 , b3 ) ed riassunta in tabella 2 . 
images were assessed at a dedicated workstation and analysed with both a mediastinal window ( width 400450 hu , centre 2050 hu ) and a lung window ( width 1 , 0001 , 500 hu , centre 650 / 750 hu )  . 
the definitive result regarding ct characteristics was then reached in consensus after a joint review of the images . the evaluation took into consideration numerous variables indicating the lesion with regard to site , size ( long axis and short axis measured on axial ct scans , along the plane in which the tumour presented its maximum axial diameter ) , morphology , margins , homogeneity , attenuation ( compared with the density of the thoracic wall muscles ) and enhancement . 
analysis also included evidence of peripheral capsule , calcifications , cystic or necrotic component , invasion of mediastinal fat , obliteration of fat planes adjacent to the lesions , pleural and / or pericardial implants , pleural and / pericardial effusion , vascular infiltration or invasion of the adjacent anatomical structures , mediastinal lymph nodes with pathological size ( length of short axis in the axial plane > 10 mm ) , metastases and retroperitoneal spread . 
in addition , contrast enhancement hounsfield units , was objectively determined by the difference in lesion attenuation values obtained after contrast material administration and in baseline conditions , with sampling of the same intralesional area and avoiding necrotic - cystic components . intensity , measured the presence of a capsule was documented by evidence of a thin peripheral ring with increased or decreased attenuation . 
the presence of tumour necrosis or cystic components timomi ad alto rischio ( b2 , b3 ) , secondo la classificazione semplificata di jeong [ 21 ]  . acquisizione ed analisi delle immagini ( definizione e selezione delle variabili ) lesame tc stato effettuato utilizzando tre diversi tomografi ( elschint ct - twin 2 strati , helicat ii ; philips brillance mx8000idt 6 e 64 strati , philips medical system ) mediante acquisizione spirale volumetrica in condizioni basali , limitatamente allespanso timico , ed in corso di somministrazione endovenosa di mezzo di contrasto ( mdc ) organo - iodato ( flusso di 23 ml / s ) , dagli apici polmonari sino a comprendere entrambi gli emuntori renali ( spessore di strato 14 mm ; 120 kvp , 170200 ma )  . 
le immagini ottenute sono state valutate su workstation dedicata ed analizzate sia attraverso finestra mediastinica ( larghezza 400450 hu , livello 2050 hu ) , sia attraverso finestra per parenchima polmonare ( larghezza 10001500 hu , livello 650 / 700 hu )  . 
sono state inoltre considerate levidenza di : capsula periferica , calcificazioni , componente cistica o necrotica , infiltrazione del tessuto adiposo mediastinico , obliterazione dei piani di clivaggio adiposo adiacenti la lesione , insemenzamento pleurico e / o pericardico , versamento pleurico e / o pericardico , infiltrazione vascolare o invasione delle strutture anatomiche viciniore , linfonodi mediastinici di dimensioni patologiche ( dimensioni dellasse corto sul piano assiale superiori a 10 mm ) , localizzazioni metastatiche e diffusione retroperitoneale . 
la forma stata classificata quale rotondeggiante se il rapporto asse lungo / asse corto risultava inferiore o pari ad 1 , 5 , ovalare se tale rapporto era compreso tra 1 , 5 e 3 , 0 , a placca se tale parametro era superiore a 3 , 0 . 
lattenuazione della lesione in condizioni basali e stata classificata quale radiol med ( 2010 ) 115 : 121 was surmised on the basis of the presence of intralesional focal areas of reduced attenuation in baseline conditions and without contrast enhancement after administration of contrast material . 
infiltration of the great vessels was surmised when the lesion was related extensively with vascular structures in the absence of fat planes and altered their profile , or in the presence of stenosis of the opacified lumen or intravascular thrombosis . ct examinations for restaging were available for all patients . 
the mean follow - up was 32 ( range 1281 ) months . analysis included the presence of locoregional recurrence , pleural / pericardial implants , supraor subdiaphragmatic metastases and retroperitoneal spread of disease . statistical analysis statistical analysis was performed with the statistica 6.1 software package ( statsoft software , for windows )  . 
comparisons were then made between the two groups in terms of ct characteristics of the tumour being studied , with either discrete dichotomous ( ct characteristic present or absent ) or continuous ( numerical ) variables . 
lenhancement stato considerato omogeneo o disomogeneo . inoltre lintensit di impregnazione constrastografica , misurata in hu , risultata oggettivamente dalla differenza dei valori densitometrici di attenuazione della lesione ottenuti dopo la somministrazione del mdc ed in condizioni basali , campionando il medesimo territorio intra - lesionale ed evitando componenti necroticocistiche . la presenza di una capsula stata documentata dallevidenza di un sottile cercine periferico ad incrementata o ridotta attenuazione . 
si supposta la presenza di necrosi tumorale o di componente cistica in caso di riscontro di aree focali intralesionali a ridotta attenuazione in condizioni basali , prive di impregnazione contrastografica dopo somministrazione del mdc . 
si supposta infiltrazione dei grossi vasi nei casi in cui la lesione presentava ampio rapporto di contiguit con le strutture vascolari in assenza di piani di clivaggio adiposo , alterandone il loro profilo , o si evidenziava stenosi del lume opacizzato o trombosi endovasale . esami tc di ristadiazione sono risultati disponibili per tutti i pazienti . 
stata valutata leventuale presenza di recidiva loco - regionale , di insemenzamento pleuro / pericardico , di localizzazioni metastatiche sovrao sotto - diaframmatiche e di diffusione retroperitoneale di malattia . results analisi statistica the study included 26 patients with noninvasive ( stage i ) and 32 patients with invasive ( stages ii , iii , iva / b ) thymoma . 
with regard to the latter group , ten patients had stage ii tumours , 19 had stage iii , two had stage iva ( with pleural implants ) and one had stage ivb ( lymphatic metastasis )  . 
with regard to the who histological classification simplified by jeong , the patient population included 30 lowrisk thymomas ( eight type a tumours , 12 type b1 and ten type ab ) and 28 high - risk thymomas ( 19 type b2 tumours , nine type b3 )  . 
thirty - three percent of low - risk tumours ( 10 / 30 ) were invasive , of which 10% ( 3 / 30 ) were in stage iii with surgical evidence of macroscopic invasion of the adjacent lanalisi statistica stata condotta con lutilizzo del programma statistica 6.1 ( statsoft software , per windows )  . i pazienti sono stati , in ogni sessione analitica , suddivisi in due gruppi ( timoma non invasivo / timoma invasivo ) in accordo con la classificazione di masaoka dopo resezione chirurgica . 
si sono quindi effettuati tra i due gruppi confronti per variabili , queste ultime in relazione alle caratteristiche tc della neoplasia in studio , di tipo discreto a soluzione dicotomica ( caratteristica tc presente o assente ) o continuo ( variabili numeriche )  . 
le differenze tra i due gruppi , nella prevalenza di ciascuna variabile a carattere discreto , sono state analizzate con il test chi - quadro di pearson o , per i piccoli campioni , con il test di fisher . 
le differenze tra variabili numeriche nei due gruppi sono state analizzate utilizzando il test non parametrico mannradiol med ( 2010 ) 115 : 121 table 3 relation between masaoka clinical stage and world health organization ( who ) histological classification simplified who classification masaoka stage no . 
of cases incidence of invasive tumours ( % ) low - risk thymomas high - risk thymomas total timomi a basso rischio timomi ad alto rischio totale tabella 3 correlazione tra classificazione clinica di masaoka e classificazione istologica who classificazione semplificata who stadio di masaoka numero di casi incidenza di tumori invasivi ( % ) anatomical structures . 
in contrast , 79% of high - risk tumours ( 22 / 28 ) were found to be invasive , with six b2 tumours classified in stage i at surgical excision . 
the tumours were situated on the left side in 25 / 57 cases ( 44% ) , the right side in 21 / 57 cases ( 37% ) or symmetrically on the midline in 11 / 57 cases ( 19% )  . 
in tutti i casi stato considerato significativo un valore di p < 0 , 05 . risultati lo studio ha incluso 26 pazienti con timoma non invasivo ( stadio i ) e 32 soggetti con timoma invasivo ( stadi ii - iiiiva / b ) : in particolare , considerando questultimo gruppo , dopo resezione chirurgica si sono osservati 10 pazienti con stadio ii , 19 pazienti con stadio iii , 2 pazienti con stadio iva ( per insemenzamento della pleura parietale ) ed 1 paziente con stadio ivb ( per metastatizzazione linfatica )  . considerando la classificazione istologica who semplificata da jeong , si sono riscontrati 30 timomi a basso rischio ( 8 tumori tipo a , 12 tipo b1 e 10 tipo ab ) e 28 timomi ad alto rischio ( 19 tumori tipo b2 , 9 tipo b3 )  . 
il 33% dei timomi a basso rischio ( 10 / 30 ) sono risultati invasivi , dei quali il 10% ( 3 / 30 ) in stadio iii per levidenza chirurgica di invasione macroscopica delle strutture anatomiche contigue . 
i 5 tumori solo parzialmente resecati ( 3 tumori stadio iii e 2 tumori stadio iva , questi ultimi per presenza di insemenzamento pleurico ) hanno incluso 1 timoma a basso rischio ( 4% ) e 4 timomi ad alto rischio ( 12 , 5% )  . 
tutti i tumori , ad eccezione di uno , si sono riscontrati nella porzione superiore del mediastino anteriore , sede usuale del timo : a prevalente sviluppo sul lato sinistro ( 25 / 57 , 44% ) , sul lato destro ( 21 / 57 , 37% ) o simmetrici sulla linea mediana ( 11 / 57 , 19% )  . 
le percentuali sono calcolate sul totale delle lesioni ; n.s. , non significativo ; acalcolato dalla differenza dei valori densitometrici di attenuazione ottenuti dopo somministrazione del mezzo di contrasto ed in condizioni basali ; * valori p calcolati attraverso il test chiquadro o il test di fisher per variabili categoriche ; * * valori p calcolati attraverso il test u di mann - whitney per variabili continue radiol med ( 2010 ) 115 : 121 fig . 
1a masaoka stage i thymoma , who type ab : unenhanced ct scan obtained at the level of the aortic arch shows an anterior mediastinal mass with round shape , smooth contours , complete capsule appearing as a high - attenuation thin rim and preservation of mediastinal fat planes . 
c masaoka stage iii thymoma , who type b2 : enhanced ct - scan obtained at the level of the azygos arch shows an oval anterior mediastinal mass with mild heterogeneous enhancement and irregular margins , suggesting invasion into surrounding mediastinal fatty tissue . 
la tc in condizioni basali dimostra una formazione espansiva del mediastino anteriore caratterizzata da morfologia rotondeggiante , margini lisci , preservazione dei piani di clivaggio adiposo e presenza di una capsula completa , documentata da un sottile cercine periferico iperdenso . 
lanalisi del pezzo operatorio , dopo escissione chirurgica , evidenzia la natura di timoma non invasivo con componente cistica a contenuto mucinoso ; b timoma stadio iii di masaoka , tipo b1 who . 
alle riformattazioni assiali e sagittali , la lesione risulta indissociabile dal foglietto sieroso pericardico , in assenza di piani di clivaggio adiposo tra le due strutture , rilievo suggestivo per infiltrazione pericardica ; c timoma stadio iii di masaoka , tipo b2 who . 
la tc con mdc mostra una formazione solida del mediastino anteriore caratterizzata da enhancement tenuemente disomogeneo e margini irregolari , grossolanamente spiculati , in relazione ad infiltrazione del contiguo tessuto adiposo mediastinico . 
no significant differences were encountered between the groups in terms of attenuation , compared with the musculature of the anterior thoracic wall , and contrast enhancement . evidence of capsule and obliteration of fat planes did not prove useful for distinguishing between invasive and noninvasive forms . 
 le dimensioni della lesione , misurate rispettivamente quali diametro maggiore e minore sulle scansioni assiali tc ( mediads ) , sono risultate : nel gruppo timoma invasivo 58 , 318 , 1 mm e 39 , 211 , 2 mm ; nel gruppo timoma non invasivo 44 , 418 , 9 mm e 32 , 715 , 3 mgli assi lungo e corto del gruppo invasivo sono risultati significativamente maggiori rispetto al gruppo non invasivo ( p rispettivamente < 0 , 01 e < 0 , 05 )  . 
inoltre si riscontrata una differenza in dimensioni statisticamente significativa tra il gruppo di pazienti con evidenza di miastenia gravis ed i restanti soggetti : le dimensioni della lesione sono risultate significativamente inferiori nel primo gruppo ( mediads asse lungo rispettivamente di 40 , 513 , 1 mm e 55 , 019 , 8 mm , con p = 0 , 041 calcolato con il test u di mann - whitney )  . 
i timomi invasivi hanno presentato , con maggior frequenza rispetto ai tumori non invasivi , morfologia ovalare , in assenza di significativit statistica tra i due gruppi ( 10 / 26 , 39% gruppo non invasivo vs 17 / 32 , 53% gruppo invasivo ; p > 0 , 05 )  . 
a le immagini tc basali mostrano una formazione solida del mediastino anteriore , caratterizzata da morfologia ovalare e margini netti , con aree a ridotta attenuazione e calcificazioni nel suo contesto , ed evidenza di una sottile capsula parzialmente calcifica . 
gli ispessimenti pleurici dellemitorace destro sono associati a modesta componente di versamento pleurico declive . effusion , lymphadenopathies and invasion of the great vessels was encountered in low percentages and only in the invasive thymoma group ( 3% 1 / 32 cases , 6% 2 / 32 cases , 9% 3 / 32 cases , respectively ) , with no statistical significance between the two groups . 
no cases of retroperitoneal spread of disease were encountered . during the study period , 15% of patients ( 9 / 58 , five subjects who underwent radical surgical resection and four incomplete resections ; none of the 11 patients affected by mg at diagnosis ) suffered locoregional recurrence or metastasis . 
at diagnosis , these tumours were two low - risk and seven high - risk thymomas ( 2 b2 and 5 b3 ) according to the jeong classification and one stage ii and 8 stage iiiiv tumours according to the masaoka classification . 
at ct follow - up most of these patients ( 8 / 9 ) displayed pleural implants with or without further associated sites of disease : lymphatic ( 3 / 9 ) , pericardial ( 2 / 9 ) , pulmonary ( 1 / 9 ) and intralesionale si riscontrata prevalentemente nel gruppo invasivo ( 13 / 32 , 41% vs 4 / 26 , 15% ; p < 0 , 05 ) , al pari delle calcificazioni ( 14 / 32 , 44% vs 5 / 26 , 19% ; p < 0 , 05 ) , nonostante non vi siano state differenze significative tra i due gruppi in relazione alla distribuzione di queste ultime ( focale / multifocale , centrale / periferica )  . 
lobliterazione parziale o completa del piano di clivaggio adiposo si riscontrata con maggior frequenza nel gruppo invasivo ( 26 / 32 casi , 81% versus 19 / 26 casi , 73% ) , al pari del versamento pleurico ( 6 / 32 casi , 18% versus 1 / 26 casi , 4% ) , differenze statisticamente non significative . infine la presenza di insemenzamento pleurico , versamento pericardico , linfoadenopatie ed invasione dei grossi vasi si riscontrata in basse percentuali unicamente nel gruppo timoma invasivo ( rispettivamente 3% 1 / 32 casi , 6% 2 / 32 casi , 9% 3 / 32 casi ) , in assenza comunque di significativit statistica tra i due gruppi in studio . 
in nessun caso si evidenziata diffusione retroperitoneale di malattia . nellintervallo di studio il 15% dei pazienti ( 9 / 58 , 5 soggetti sottoposti a resezione chirurgica radicale e 4 incompleta ; nessuno degli 11 pazienti affetti da miastenia gravis alla diagnosi ) andato incontro a recidiva locoregionale o diffusione metastatica . 
tali tumori sono risultati alla diagnosi : 2 timomi a basso rischio e 7 ad alto rischio ( due b2 e cinque b3 ) secondo la classificazione di jeong ; 1 stadio ii ed 8 stadi iii - iv secondo la classificazione di masaoka . 
nel restante paziente si riscontrato tessuto solido in mediastino anteriore , suggestivo per recidiva loco - regionale . nellanalisi statistica relativa agli aspetti tc predittivi di recidiva a distanza stato considerato il solo gruppo dei timomi invasivi , dal momento che nessuna recidiva stata osservata nel gruppo non invasivo . 
in the remaining patient , solid tumoral tissue was found in the anterior mediastinum , suggestive of locoregional recurrence . statistical analysis regarding ct signs predictive of disease recurrence took into consideration only the group of invasive thymomas , as no recurrence was observed in the noninvasive group . 
tumours at diagnosis characterised by large size , lobulated or irregular margins , complete absence of a fat plane , invasion of the vascular structures and pleural implants displayed a greater frequency of recurrence ( table 5 )  . lastly , a strong correlation was found between the preoperative who classification , obtained with percutaneous or surgical biopsy , and the postoperative classification , obtained with analysis of the surgical specimen . 
in 96% of cases in which a biopsy diagnosis was available ( 50 / 52 subjects ) , the who classification obtained coincided with the histological analysis of the biopsy sample and the surgical specimen . 
the two cases of disagreement , classified as b2 after ct - guided percutaneous biopsy after surgical resection , were found to be b2 tumours with focal atypical cellular transformation ( atypical thymomas ) and were therefore classified as b3 . discussion epithelial malignancies arising from thymic precursors , which include thymoma and thymic carcinoma , are the most frequent tumours found in the adult anterior mediastinum ( 30% ) , followed by lymphomas ( 20%25% ) , germ - cell tumours ( 10%15% ) and carcinomas [ 1 , 2 ]  . 
thymomas include a broad range of epithelial malignancies characterised by a different histological appearance and biological behaviour [ 26 ] and are divided into invasive and noninvasive thymomas according to the anatomicalsurgical classification proposed by masaoka [ 6 ]  . 
noninvasive malignancies consist of completely capsulated tumours , with no microscopic evidence of capsule invasion , whereas invasive thymomas are characterised by invasion of the capsule and implants or adjacent anatomical structures , pleural metastatic spread [ 35 ]  . 
ct is the technique of choice in the study of the anterior mediastinum for visualisation and precise presurgical characterisation of thymic tumours , and it may be integrated with mr and nuclear medicine [ 2 , 25 , 27 , 29 ]  . 
diagnosis prior to resection is made on the basis of histological analysis on a sample obtained with needlepuncture ct - guided percutaneous biopsy or surgical biopsy [ 2 , 4 , 9 , 29 , 30 ]  . 
histological findings are crucial for correct treatment planning , both in defining the differential diagnosis ( primarily between lymphoma and thymoma ) and evaluating the utility of possible neoadjuvant therapy to un piano di clivaggio adiposo , invasione delle strutture vascolari ed insemenzamento pleurico hanno mostrato una maggior frequenza di recidiva a distanza ( tabella 5 )  . si infine riscontrata elevata correlazione tra classificazione who pre - escissionale , ottenuta attraverso aggressione bioptica percutanea o chirurgica , e postchirurgica , ottenuta attraverso lanalisi del pezzo operatorio . 
nel 96% dei casi nei quali risultata disponibile una diagnosi bioptica ( 50 / 52 soggetti ) , lo stadio who ottenuto ha coinciso allanalisi istologica del pezzo bioptico ed operatorio . 
i 2 casi discordanti , classificati quali b2 dopo biopsia percutanea sotto guida tc , sono poi risultati , dopo intervento chirurgico resettivo , tumori b2 con focolai di trasformazione cellulare atipica ( timomi atipici ) , e quindi considerati b3 . discussione le neoplasie epiteliali con origine da precursori timici , che includono il timoma ed il carcinoma timico , costituiscono nelladulto i tumori di pi frequente riscontro in mediastino anteriore ( 30% ) , seguiti dai linfomi ( 20%25% ) , dai tumori a cellule germinali ( 10%15% ) e dai carcinomi [ 1 , 2 ]  . 
i timomi comprendono un ampio spettro di neoplasie epiteliali , caratterizzate da un diverso aspetto istologico e comportamento biologico [ 26 ] , e vengono suddivisi in timomi invasivi e non - invasivi in accordo con la classificazione anatomo - chirurgica proposta da masaoka [ 6 ] : i tumori non - invasivi rappresentano neoplasie completamente capsulate , senza evidenza microscopica di invasione della capsula ; i timomi invasivi sono caratterizzati da infiltrazione della capsula , delle strutture anatomiche viciniore , da insemenzamento delle sierose o da diffusione metastatica [ 35 ]  . la tc rappresenta la metodica di scelta nello studio del mediastino anteriore , al fine della documentazione e della precisa caratterizzazione pre - chirurgica delle neoplasie timiche , eventualmente integrata da indagini di risonanza magnetica e medicina nucleare [ 2 , 25 , 27 , 29 ]  . 
la diagnosi pre - escissionale posta in base al rilievo istologico ottenuto attraverso biopsia percutanea con ago tranciante sotto guida tc o biopsia chirurgica [ 2 , 4 , 9 , 29 , 30 ]  . 
il risultato istologico rilevante al fine della corretta pianificazione terapeutica , sia nella definizione della diagnosi differenziale ( in prima istanza tra linfoma e timoma ) , sia nella valutazione sullutilit di eventuali trattamenti neoadiuvanti lescissione chirurgica del timoma . 
recenti studi hanno dimostrato come trattamenti multimodali , costituiti dallassociazione di chemioterapia neoadiuvante , resezione chirurgica e trattamenti chemioradioterapici adiuvanti , migliorino la sopravvivenza delle neoplasie timiche localmente avanzate ( stadi iii - iva di masaoka ) [ 713 ]  . 
percentages are calculated considering all lesions ; ns , not significant ; * p values were calculated using the chi - square test or the fisher exact test for categorical variables ; * * p values were calculated using the mann - whitney u test for continuous variables tabella 5 caratteristiche dei pazienti ed aspetti alla tomografia computerizzata ( tc ) alla diagnosi nei timomi invasivi recidivati caratteristiche dei pazienti ed aspetti tc della lesione recidiva si ( n = 9 ) no ( n = 23 ) i numeri in parentesi costituiscono percentuali . 
le percentuali sono calcolate sul totale delle lesioni ; n.s. , non significativo ; * valori p calcolati attraverso il test chi - quadro o il test di fisher per variabili categoriche ; * * valori p calcolati attraverso il test u di mann - whitney per variabili continue surgical excision of the thymoma . 
recent studies have shown that multimodal treatments , consisting of the association of neoadjuvant chemotherapy , surgical resection and adjuvant chemotherapy and radiotherapy , improve the survival of patients with locally advanced thymic malignancies ( masaoka stage iiiiva ) [ 713 ]  . 
in addition , neoadjuvant treatments are able to augment the possibility of radical valenza prognostica , con incremento dei tassi di radicalit chirurgica dal 46 , 5% al 65 , 1% negli stadi iii e dallo 0% al 20% negli stadi iva [ 5 , 10 , 14 ]  . 
essendo la classificazione di masaoka post - chirurgica , tali trattamenti vengono attualmente riservati ai timomi ad alto rischio definiti in base alla classificazione istologica di jeong [ 21 ]  . 
as the masaoka classification is postsurgical , these treatment options are reserved for high - risk thymomas defined on the basis of the jeong histological classification [ 21 ]  . 
over the decades , a number of histological classifications of thymic malignancies have been proposed [ 9 , 1518 , 31 ] from the bernatz system in 1996 that recognised four different subtypes on the basis of the prevalence of the cell population [ 31 ] , up until the who classification in 2004 [ 19 , 20 ] , which was subsequently simplified by jeong [ 21 ]  . 
nonetheless , numerous studies have shown the limited prognostic significance of these histological classifications and demonstrated how histological type is not an independent predictor of survival at multivariate analysis [ 8 , 9 , 2224 ]  . 
the prognosis is in fact correctly defined by the study of the disease according to the masaoka classification following surgical resection of the tumour [ 8 , 9 , 22 ]  . 
these malignancies , which were incorrectly excluded from neoadjuvant treatment according to the histological stage , presented ct characteristics suggestive of invasiveness ( two characterised by lobulated margins , considerable dimensions and a cystic component ; one characterised by a cystic component and heterogeneous enhancement )  . 
in contrast , 32% of high - risk tumours ( 9 / 28 , stage b2 ) with indication for neoadjuvant treatment based on histological stage were classified after surgical resection as stage i ( 6 / 28 ) or stage ii ( 3 / 28 )  . 
of these , 67% ( 6 / 9 ) showed no ct sign that was significantly predictive of invasiveness , thus suggesting neoadjuvant treatment as inappropriate . in our study , a statistically significant correlation was found between the presence of irregular / lobulated margins , cystic / necrotic component , calcifications , heterogeneous enhancement and large dimensions and the invasive thymoma group . 
these data confirm the results of the tomiyama series , with the only exception being the dimensions of the lesion , a parameter , which was not included by the author among the study variables [ 28 ]  . 
previous studies the who classification presented that focused on neoplasie timiche [ 9 , 1518 , 31 ] , dal sistema di bernatz del 1966 che riconosceva quattro diversi sottotipi in base alla prevalenza della popolazione cellulare [ 31 ] , sino alla classificazione who del 2004 [ 19 , 20 ] , successivamente semplificata da jeong [ 21 ]  . 
tuttavia , numerosi studi hanno dimostrato lo scarso significato prognostico di tali classificazioni istologiche e come il tipo istologico non rappresenti un fattore predittivo indipendente di sopravvivenza allanalisi multivariata [ 8 , 9 , 2224 ]  . 
la differente valenza prognostica delle diverse classificazioni viene confermata dalla non perfetta correlazione tra classificazione di jeong e stadio di masaoka : tomiyama ha rilevato percentuali di invasivit , dopo resezione chirurgica , del 41% per i timomi a basso rischio e del 78% nelle neoplasie ad alto rischio [ 25 ]  . successivamente , jeong e sadohara hanno riscontrato rispettivamente percentuali del 30% e 22% per i timomi a basso rischio , e del 61% e 78% per i timomi ad alto rischio [ 21 , 27 ]  . 
tali neoplasie , escluse erroneamente da trattamenti neoadiuvanti secondo lo stadio istologico , presentavano caratteristiche tc suggestive per invasivit ( due caratterizzate da margini lobulati , dimensioni rilevanti e componente cistica ; una da componente cistica ed enhancement disomogeneo )  . 
al contrario , il 32% delle neoplasie ad alto rischio ( 9 / 28 , stadio b2 ) , con indicazione a terapia neoadiuvante in relazione allo stadio istologico , poi stato classificato , dopo resezione chirurgica , in stadio i ( 6 / 28 ) o ii ( 3 / 28 )  . 
il 67% di queste ( 6 / 9 ) non presentava alcun elemento tc significativamente predittivo per invasivit , suggerendo quindi linopportunit di trattamenti neoadiuvanti . nel nostro studio la presenza di contorni irregolari / lobulati , componente cistica / necrotica , calcificazioni , enhancement eterogeneo e dimensioni elevate risultata maggiormente associata , con significativit statistica , al gruppo timoma invasivo . 
studi precedenti , focalizzati sulla classificazione who , presentano risultati contrastanti in rapporto al parametro dimensioni : jung ha dimostrato come i carcinomi timici ( stadio c ) presentino dimensioni maggiori rispetto ai timomi atipici ( stadio b3 ) , mentre tomiyama ha riscontrato dimensioni maggiori nei carcinomi timici al confronto con i timomi in stadio a e b2 [ 25 , 32 ]  . 
infine , la casistica di sadohara non ha evidenziato differenze significative tra le diverse neoplasie del timo per tutti gli stadi who , in relazione al parametro dimensioni [ 27 ]  . 
si osservano risultati radiol med ( 2010 ) 115 : 121 contrasting results in relation to lesion dimensions : jeong showed how thymic carcinomas ( stage c ) tend to have larger dimensions than atypical thymomas ( stage b3 ) , whereas tomiyama found larger dimensions in thymic carcinomas than in stage a and stage b2 thymomas [ 25 , 32 ]  . 
the findings in various studies correlating who stages and ct characteristics of the tumours are discordant also with regard to other variables , with the conclusion that ct is of limited value in distinguishing between lowand high - grade thymomas , whereas it can be useful in the differential diagnosis between thymic carcinoma and thymoma [ 21 , 2527 , 32 ]  . more specifically , some studies have shown that smooth margins and rounded morphology are more frequently found , with statistical significance , in who classification type a lesions , whereas calcifications and pleural implants are more typical of type b malignancies ( b1 , b2 , b3 ) [ 25 , 26 ]  . 
the remaining ct characteristics provide no useful information for predicting the who stage on the basis of imaging alone , such that distinguishing between ab , b1 ( low - risk thymomas ) and b2 , b3 ( high - risk thymomas ) is not possible . 
these findings do not allow correct treatment planning to be established in terms of possible neoadjuvant treatment , as they are not typical of all the low - risk or high - risk forms , with lobulated margins being the only exception . 
in contrast , a distinction based on ct imaging between type c malignancies ( thymic carcinomas ) and the remaining histological types of thymic derivation does appear to be feasible , given that irregular margins , a cystic or necrotic component , heterogeneous enhancement , lymphadenopathies , obliteration of the fat planes and infiltration of the vascular structures are the most significant ct findings in thymic carcinomas with respect to thymomas ( at low and high risk ) [ 21 , 2527 , 32 ]  . 
this latter distinction is clinically significant with regard to correct neoadjuvant treatment management , given that the presurgical differential diagnosis between thymic carcinoma and thymoma can be achieved with lesion biopsy . 
this is why a preexcision predictive diagnosis of invasiveness is so important , rather than a distinction of the who stage on the basis of the ct lesion characteristics . in our study , 62% of noninvasive tumours presented smooth margins , whereas 72% of invasive tumours had lobulated or irregular margins , which compares with the 52% and 81% reported by tomiyama [ 28 ]  . 
areas of reduced attenuation , indicative of an intralesional cystic or necrotic component , were found in 30% of cases , with significantly greater frequency ( 41% ) in the invasive forms . 
these findings are similar to the proportions obtained in the series by controversi nei diversi studi di correlazione tra stadio who e caratteristiche tc della neoplasia anche per le altre variabili in studio , con la conclusione che la tc risulta tecnica di limitato valore nella distinzione tra timomi a basso ed alto rischio , mentre assume rilevanza nella diagnosi differenziale tra carcinoma timico e timoma [ 21 , 2527 , 32 ]  . 
nello specifico , alcuni studi hanno dimostrato come margini lisci e morfologia rotondeggiante si riscontrino con maggior frequenza , statisticamente significativa , nelle neoplasie tipo a secondo la classificazione who , mentre le calcificazioni e linsemenzamento pleurico contraddistinguono maggiormente le forme b ( b1 , b2 , b3 ) [ 25 , 26 ]  . 
le restanti caratteristiche tc della lesione non consentono di predire lo stadio who sulla sola base dellimaging , risultando non possibile la distinzione tra forme ab , b1 ( timomi a basso rischio ) , b2 e b3 ( timomi ad alto rischio )  . 
tali evidenze non permettono di impostare una corretta pianificazione terapeutica in relazione a possibili trattamenti neoadiuvanti , dal momento che non risultano peculiari di tutte le forme istologiche a basso o ad alto rischio , con la sola eccezione dei margini lobulati . 
 al contrario proponibile una distinzione basata sullimaging tc tra neoplasie tipo c ( carcinomi timici ) ed i restanti tipi istologici di derivazione timica , dal momento che margini irregolari , componente cistica o necrotica , enhancement disomogeneo , linfoadenopatie , obliterazione dei piani di clivaggio adiposo ed infiltrazione delle strutture vascolari risultano elementi tc di maggior significativo riscontro nei carcinomi timici rispetto ai timomi ( a basso ed alto rischio ) [ 21 , 2527 , 32 ]  . questa ultima distinzione riveste relativa importanza clinica al fine della corretta gestione terapeutica neoadiuvante dei pazienti , dal momento che la diagnosi differenziale prechirurgica tra carcinoma timico e timoma pu essere ricavata attraverso biopsia della lesione . 
per questa ragione fondamentale una diagnosi predittiva pre - escissionale di invasivit , piuttosto che una distinzione dello stadio who sulla base delle caratteristiche tc della lesione . nel presente studio , il 62% dei timomi non invasivi ha presentato margini lisci , mentre il 72% dei tumori invasivi margini lobulati o irregolari , a confronto con rispettivamente il 52% e l81% riportato da tomiyama [ 28 ]  . 
aree a ridotta attenuazione , in relazione a componente cistica o necrotica intra - lesionale , si sono riscontrate nel 30% dei casi , con significativa maggior frequenza ( 41% ) nelle forme invasive . 
le calcificazioni rappresentano un altro elemento di maggior riscontro nelle forme invasive , come precedentemente dimostrato da tomiyama [ 28 ] : nella nostra casistica il 33% dei timomi ha presentato calcificazioni , con frequenza rispettivamente del 44% e 20% per le forme invasive e non invasive . 
the prevalence of calcifications reported in the literature ranges from 10% to 40% and is proportional to progressive technological improvements in the technique in terms of the possibility of obtaining increasingly thinner collimations [ 28 ]  . 
the focal or multifocal distribution of calcifications appears similar between the two groups , in contrast to tomiyamas findings in which a statistically significant association was found between invasive thymomas and multifocal calcifications [ 28 ]  . ct does not appear to be an appropriate technique for evaluating the tumour capsule , which was visualised in only 31% of thymomas . 
indeed , in a study comparing ct and mr , this author reports the frequency of visualising the tumour capsule by the two imaging modalities to be 20% and 80% , respectively [ 27 ]  . evaluation of fat planes with the adjacent anatomical structures is not useful for the purposes of distinguishing between invasive and noninvasive forms , as only 27% of noninvasive tumours showed complete preservation of the adipose fat planes , whereas 65% of cases showed its partial obliteration . 
these values are those reported by nonetheless notably higher tomiyama , whose series covered a time - frame from 1990 to 1999 , with percentages of 9% and 54% , respectively . 
this difference is in this case justified by the technological progress of ct , which has made it possible to visualise fine details with the use of increasingly thin collimations [ 28 ]  . than the prognosis and risk of recurrence correlate proportionally with the masaoka stage , i.e. , with the degree of extracapsular invasion , with 5 - year recurrence rates after radical surgical resection between 8% and 29% in different series . 
in 81% of cases , disease recurrence is thoracic , in 9% extrathoracic and in 10% both the supraand subdiaphragmatic regions are involved [ 21 , 34 , 35 ]  . 
the most commonly affected sites are the pleura and the lung ( frequently documented by the finding of peripheral nodules ) in 58% of cases , the pericardium or the mediastinum in 41% , bone in 10% and the liver in 8% [ 5 , 3436 ]  . 
in our study , the frequency of recurrence in the study period was 9% ( 5 / 53 patients ) of cases of radical surgical resection and 15% ( 9 / 58 patients ) with the inclusion of nonradical procedures , which showed no signs of residual disease at the follow - up ct examination performed after adjuvant therapy . 
the most frequent site was the pleura ( 89% of cases , 8 / 9 subjects ) , followed by the pericardium ( 22% , 2 / 9 ) , the lung ( 11% , 1 / 9 ) , in letteratura variabile tra il 10% ed il 40% , e risulta proporzionale alla progressiva implementazione tecnologica della metodica in rapporto alla possibilit di ottenere collimazioni sempre pi fini [ 28 ]  . 
la distribuzione focale o multifocale delle calcificazioni risultata analoga tra i due gruppi , al contrario di quanto riportato da tomiyama nel cui studio i timomi invasivi sono risultati associati , con significativit statistica , a calcificazioni multifocali [ 28 ]  . la tc non risultata metodica idonea alla valutazione della capsula tumorale , documentata solo nel 31% dei timomi . 
lautore infatti , in uno studio di comparazione tc - rm , riporta frequenze di riscontro di capsula tumorale per le due metodiche rispettivamente del 20% ed 80% [ 27 ]  . 
la valutazione dei piani di clivaggio adiposo con le strutture anatomiche contigue non risultata utile al fine della distinzione tra forme invasive e non invasive , poich solo nel 27% dei tumori non invasivi stato possibile documentare completa preservazione dei piani adiposi , mentre nel 65% dei casi si osservata parziale obliterazione . 
questi valori risultano comunque sensibilmente maggiori rispetto a quanto riportato da tomiyama , la cui casistica ricopre un intervallo di studio compreso tra il 1990 ed il 1999 , con percentuali rispettivamente del 9% e 54% . 
tale differenza anche in questo caso giustificabile dal progresso tecnologico della tc , che permette di documentare particolari fini con lutilizzo di collimazioni sempre pi sottili [ 28 ]  . la prognosi ed il rischio di recidiva a distanza correlano proporzionalmente con lo stadio di masaoka , ovvero con il grado di invasione extra - capsulare , con tassi di recidiva a 5 anni , dopo resezione chirurgica radicale , compresi tra l8% ed il 29% a seconda delle diverse casistiche : nell81% dei casi la ripresa di malattia toracica , nel 9% extra - toracica e nel 10% interessa entrambi i distretti sovrae sotto - diaframmatico [ 21 , 34 , 35 ]  . 
le sedi maggiormente coinvolte sono la pleura ed il polmone ( frequentemente documentata dal riscontro di noduli mantellari ) nel 58% dei casi , il pericardio o il mediastino nel 41% , losso nel 10% ed il fegato nell8% [ 5 , 3436 ]  . 
nel nostro studio , nellintervallo temporale analizzato , la frequenza di recidiva stata del 9% ( 5 / 53 pazienti ) considerando le resezioni chirurgiche radicali , e del 15% ( 9 / 58 soggetti ) includendo gli interventi non radicali , privi di residuo di malattia allindagine tc di follow - up dopo terapia adiuvante . 
la frequenza di recidiva aumenta con lo stadio di masaoka con tassi medi a 5 anni del 4% , 14% , 26% e 46% rispettivamente dallo stadio i al iva [ 9 ]  . 
nella nostra casistica , dopo un follow - up medio di 32 mesi , le percentuali sono risultate rispettivamente dello 0% radiol med ( 2010 ) 115 : 121 the mediastinum ( 11% , 1 / 9 ) and the liver ( 11% , 1 / 9 )  . 
the frequency of recurrence increased with the masaoka stage , with mean 5 - year rates of 4% , 14% , 26% and 46% for stages iiva , respectively [ 9 ]  . 
according to the who classification simplified by jeong , 78% of cases of recurrence ( 7 / 9 patients ) were high - risk disease , with prevalence of stage b3 ( 56% , 5 / 9 )  . 
this finding reflects the results of jeongs series , in which 75% of recurrent high - risk thymomas ( 6 / 8 ) were stage b3 , thus confirming how a slight degree of cellular atypia seen in this stage is a negative prognostic factor , i.e. , these forms are closer to the aggressive biological behaviour of thymic carcinomas rather than are thymomas [ 9 , 21 ]  . numerous studies have demonstrated the importance of a number of variables as predictive factors of recurrence and overall survival . 
these include clinical features ( age , presence of mg , etc . ) , masaoka stage , who histological type , tumour size and presence of invasion of the mediastinum and / or great vessels 21 , 3436 ]  . 
as negative prognostic factors from the histological analysis of resected tumours , suster and rosai noted irregular margins of tumour growth , mitotic count exceeding 10 / 10 high - power fields , absence of lobular growth and high - grade histology [ 37 ]  . 
jeong found in his study ( which included thymic carcinomas ) a greater frequency of recurrence or metastasis in malignancies , which at ct examination performed prior to diagnosis presented oval - shaped , lobulated or irregular margins ; invasion of the mediastinum or the great vessels ; and pleural implants [ 21 ]  . 
this disagreement might be justified by the inclusion of thymic carcinomas in jeongs study and the high proportion ( 100% , 7 / 7 cases ) of recurrent thymic carcinomas with oval shape . the role of mg as a positive prognostic factor is controversial and hotly debated . 
around 35% of patients with thymomas usually present signs and symptoms of mg , whereas 15% of subjects affected with mg are found to have thymomas [ 1 , 2 , 8 ]  . 
in contrast , several studies have demonstrated higher rates of recurrence in patients not affected by mg and better survival in patients with mg [ 5 , 8 , 9 ]  . 
this more favourable prognosis attributable to mg and confirmed by our series none of the 11 subjects affected by mg developed disease ( 0 / 26 casi ) , 10% ( 1 / 10 ) , 31% ( 6 / 19 ) e 66% ( 2 / 3 )  . 
nel nostro studio , secondo la classificazione who semplificata di jeong , il 78% dei casi recidivati ( 7 / 9 pazienti ) risultato patologia ad alto rischio , con prevalenza degli stadi b3 ( 56% , 5 / 9 )  . 
questo dato riflette i risultati della casistica di jeong , in cui il 75% dei timomi ad alto rischio recidivati ( 6 / 8 ) sono risultati stadi b3 , e permette di confermare come la modesta atipia cellulare evidenziata in questo stadio rappresenti un elemento prognostico negativo , ovvero come queste forme si avvicinino pi al comportamento biologico aggressivo dei carcinomi timici piuttosto che dei timomi [ 9 , 21 ]  . 
 numerosi studi hanno dimostrato limportanza , quali fattori predittivi di recidiva e di sopravvivenza globale , di alcune variabili quali : aspetti clinici ( et , presenza di miastenia gravis , ecc . ) , stadio di masaoka , tipo istologico who , dimensioni del tumore e presenza di infiltrazione del mediastino e / o dei grossi vasi [ 21 , 3436 ]  . 
suster e rosai hanno evidenziato , quali fattori prognostici negativi dallanalisi istologica delle neoplasie resecate , margini di crescita tumorale irregolari , conta mitotica maggiore a 10 in almeno 10 campi microscopici esaminati , assenza di crescita lobulare ed istologia di alto grado [ 37 ]  . 
jeong ha riscontrato nel suo studio ( che include anche i carcinomi timici ) una maggior frequenza di recidiva o metastasi in neoplasie che presentano , allindagine tc di prima diagnosi , forma ovalare , margini lobulati o irregolari , infiltrazione del mediastino o dei grossi vasi , e insemenzamento pleurico [ 21 ]  . 
la discordanza potrebbe essere giustificata dallinclusione dei carcinomi timici nello studio di jeong e dallelevata proporzione ( 100% , 7 / 7 casi ) di carcinomi timici recidivati a forma ovalare . controverso e dibattuto il ruolo della mg quale fattore prognostico positivo . 
circa il 35% dei pazienti con timoma presenta usualmente segni e sintomi di mg , mentre nel 15% dei soggetti affetti da mg si riscontra un timoma [ 1 , 2 , 8 ]  . 
la presenza di mg incrementa il rischio chirurgico , dal momento che la maggior parte dei decessi intra - operatori viene attribuita a crisi miasteniche subentranti [ 5 ]  . 
al contrario alcuni studi dimostrano tassi di recidiva maggiori in pazienti non affetti da mg e pi elevata sopravvivenza in presenza di mg [ 5 , 8 , 9 ]  . 
questo vantaggio prognostico attribuibile alla mg e confermato dalla nostra casistica , dal momento che nessuno degli 11 soggetti affetti da mg alla diagnosi ha sviluppato recidiva di malattia nellintervallo di studio , a nostro avviso rappresentato dallanticipazione diagnostica in radiol med ( 2010 ) 115 : 121 recurrence during the study period is in our opinion due to the fact that the diagnosis in these patients is reached earlier than in asymptomatic subjects or patients with compression symptoms . 
the use of different multidetectorrow ct scanners ( 2 , 6 and 64 slices ) , as well as variable collimations , and the time interval between ct examination and surgical resection ( 14 weeks ) may have influenced the evaluation of some features of the tumour , such as invasion of the adjacent structures , visualisation of a capsule or calcifications ; and lastly , potential variations of the lesion during the period between the ct diagnosis and the evaluation of the surgical specimen . 
in addition , the series included five patients who underwent partial resection in consideration of the locally advanced stage of disease incomplete surgical resection influences the rate of disease recurrence . conclusions in conclusion , our study shows the utility of ct in differentiating noninvasive from invasive forms of thymomas , the latter of which are characterised by greater frequency and size , lobulated / irregular margins , cystic / necrotic component , calcifications and heterogeneous enhancement . 
integration between the preoperative who classification , obtained with lesion biopsy , and ct imaging suggestive of invasive disease plays an important role in the correct treatment management prior to surgical excision . 
in addition , ct supplies predictive indicators of recurrence , as recurrence is more commonly found in tumours characterised at diagnosis by larger size , lobulated / irregular margins , complete absence of fat planes , invasion of the vascular structures and pleural implants . 
therefore , in the diagnosis of thymic masses , the radiologist should pay close attention to ct features useful for distinguishing between invasive and noninvasive tumours and predictive of disease recurrence . questi pazienti , rispetto ai soggetti asintomatici o con sintomi da compressione . 
infatti il gruppo mg ha presentato dimensioni tumorali significativamente inferiori ai restanti soggetti ( 40 , 5 mm vs 55 , 0 mm ) , e dimensioni minori rappresentano fattore prognostico positivo [ 21 , 3436 ]  . il nostro studio presenta una serie di limiti : innanzitutto la natura retrospettiva con raccolta dei dati a posteriori non consente criteri di uniformit nelliter diagnostico - terapeutico seguito dai pazienti . 
lutilizzo di diverse apparecchiature tc multidetettore ( 2 , 6 e 64 strati ) , oltre che di collimazioni variabili , e lintervallo temporale intercorso tra lesame tc e lescissione chirurgica ( 14 settimane ) pu aver influenzato la valutazione di alcuni aspetti della neoplasia quali linfiltrazione delle strutture adiacenti , levidenza di capsula o calcificazioni ed infine potenziali variazioni della lesione intercorse tra la diagnosi tc e la valutazione del pezzo operatorio . 
inoltre la casistica include 5 pazienti sottoposti a resezione parziale in considerazione dello stadio localmente avanzato di malattia ; la resezione chirurgica incompleta influenza i dati di recidiva a distanza . conclusioni in conclusione , il nostro studio dimostra lutilit della tc nel differenziare le forme non - invasive dai tumori invasivi , questi ultimi caratterizzati con maggior frequenza da dimensioni maggiori , margini lobulati / irregolari , componente cistica / necrotica , calcificazioni ed enhancement disomogeneo . 
lintegrazione tra classificazione who preoperatoria , ottenuta attraverso aggressione bioptica della lesione , ed imaging tc suggestivo per patologia invasiva , ricopre ruolo fondamentale nella corretta gestione terapeutica neoadiuvante allescissione chirurgica . 
inoltre la tc fornisce elementi predittivi di recidiva a distanza , dal momento che questa si riscontra con maggior frequenza in tumori caratterizzati alla diagnosi da dimensioni maggiori , margini lobulati / irregolari , completa assenza di piani di clivaggio adiposo , infiltrazione delle strutture vascolari ed insemenzamento pleurico . 
sartor springer - verlag , berlin heidelberg , 2009 isbn 978 - 3 - 540 - 00281 - 9 published online : 29 january 2010 springer - verlag 2010 the title of the book summarises well the goals that the editors and their team of experts from both sides of the atlantic wanted to reach . 
acute , traumatic and chronic diseases of the pancreas and their complications are discussed in 20 chapters and 390 pages plus a well structured subject index . according to the introduction , the untimely death of carlo procacci caused a delay in the planning , layout and preparation of the book , which is now dedicated to his memory . thirteen of the 20 chapters are written by experts from the verona teams , where procacci devoted much of his research to pancreatic diseases , thus making this one of the foremost schools in the world . 
this amount of work and universally renowned research is appreciated and easily recognised by perusing the references of each chapter . pancreatic diseases in all their multifaceted , various aspects often mysterious and difficult to diagnose are described and discussed to familiarise the reader with clinical evaluation , proper imaging and treatment . 
diagnostic imaging tools such as ultrasonography ( us ) , endoscopic us , computed tomography ( ct ) and multidetector ct ( mdct ) ( a revolutionary diagnostic tool in the field ) , magnetic resonance imaging ( mri ) , endoscopic retrograde cholangiopancreatography ( ercp ) and minimally invasive methods are described in depth for both diagnosis and treatment . 
use of gadolinium - enhanced mri is amply described and debated : a few words are dedicated to the possible nephrogenic systemic fibrosis ( nsf ) complication , which may occur in patients in critical condition or on dialysis . according to the preface , the reader will notice several unavoidable overlapping opinions reflecting different points of view , distinct idiosyncratic experiences and various conflicting bibliographic references . 
le malattie del pancreas , siano esse acute , croniche o traumatiche e le loro complicanze sono discusse in 20 capitoli e 390 pagine , corredate anche da un ben strutturato e completo indice analitico . secondo quanto segnalato nella prefazione , la prematura morte del prof . 
carlo procacci ha provocato un considerevole ritardo nella pianificazione , preparazione e stesura del volume , che ora dedicato a lui . tredici dei 20 capitoli sono scritti da esperti dei vari gruppo di studio di verona , dove il prof . 
il frutto di tale mole di lavoro e di ricerca , universalmente riconosciuta nel suo valore , apprezzabile e facilmente riconoscibile scorrendo le voci bibliografiche dei singoli capitoli . le malattie del pancreas in tutti i loro aspetti variegati , spesso misteriosi e di difficile diagnosi , sono ben descritte e discusse in modo tale da rendere il lettore familiare con la loro valutazione clinica , il corretto studio per immagini e la loro terapia . 
 vengono descritti in profondit e nei loro dettagli utili per la diagnosi e la terapia , strumenti per immagini quali ultrasuoni , endoscopia con ultrasuoni , tc e tc multi - detettore ( mdct , strumento rivoluzionario in questo campo ) , rm , ercp e metodi minimamente invasivi . 
luso della rm con gadolinio ampiamente descritto e dibattuto : viene brevemente fatto cenno alla possibile complicanza della nsf in pazienti in condizioni particolarmente critiche o in dialisi . secondo quanto riportato nella prefazione il lettore trover , several unavoidable overlapping opinions reflecting different points of view , distinct idiosyncratic experiences and various conflicting bibliographic references . 
 il lettore apprezzer la bellezza delle immagini sia in radiol med ( 2010 ) 115 : 170171 the reader will appreciate the beauty of the images ( a few in colour as well ) , their perfect reproduction , and their prolific use to illustrate the topic they address and render it as understandable as possible . in summary , this book will be of great help to all those who have to deal with problematic and difficult cases and care for patients affected by acute or chronic pancreatitis who will benefit most from cooperative , expert , multidisciplined teams . bianco e nero che a colori , la loro perfetta riproduzione ed il loro uso in abbondanza in modo tale da illustrare al meglio largomento cui fanno riferimento e renderlo quanto pi comprensibile possibile . 
the shield effects on the ct image were evaluated by measuring the signal - to - noise ratio in a phantom and in vivo , and by verifying the presence of artefacts on patients images . 
use of bismuth shields significantly decreases both organ and effective radiation dose , with a consequent reduction in health risk for the patient , quantified in 1.4 fewer cases of radiation - induced tumours every 5 years in our centre ( 12 , 100 exams / year ) , in agreement with the risk factors proposed by publication 60 of the international commission on radiological riassunto obiettivo . 
la differenza fra il rapporto segnale rumore per immagini con schermi e senza schermi statisticamente significativa , ma allinterno dei limiti richiesti per lassicurazione di qualit ; i risultati sono in accordo con la percezione dei radiologi sulla qualit dellimmagine . 
lutilizzo degli schermi in bismuto consente di ottenere una riduzione sia della dose agli organi che della dose efficace con una conseguente riduzione del rischio per i pazienti , quantificata in 1 , 4 casi in meno di radiol med ( 2010 ) 115 : 152169 protection ( icrp )  . 
the relative inexpensiveness of these protections , their easy application and their substantial lack of influence on image quality suggest their massive introduction into routine clinical practice . keywords bismuth shields computed tomography patient dose radiation effects tumori radio - indotti ogni 5 anni nel nostro centro ( 12100 esami / anno ) in accordo con i fattori di rischio proposti dallinternational commission on radiological protection ( icrp ) pubblicazione 60 . 
il relativo basso costo di queste protezioni , la facilit di utilizzo e la sostanziale ininfluenza sulla qualit dellimmagine ne suggeriscono lintroduzione estensiva nella routine clinica . parole chiave protezioni di bismuto tomografia computerizzata dose effetti delle radiazioni introduction introduzione the recent advent of multislice spiral computed tomography ct has led to a significant increase in the use of ct imaging in medical practice , which now provides more than 30% of all medical x - rays . 
indeed , in countries with the highest levels of health care classified by the united nations scientific committee on the effects of atomic radiation ( unscear ) [ 1 ] as level i countries the contribution of ct procedures to the collective dose from medical examinations has risen from 18% in the 1980s to 41% in 1990s ( 34% worldwide )  . 
 due to the lack of overlying tissues , the radiation dose delivered to superficial radiosensitive organs often incidentally included in the scan area , such as the eyes , the thyroid and the breast , may be very significant and approaches , or even exceeds , the dose level for the induction of radiogenic effects . 
furthermore , when a multislice ct scanner is used in the helical mode , regions adjacent to the scan volume may lie within the imaged volume [ 4 ]  . 
therefore , this potentially high radiation exposure makes it increasingly important to develop optimisation strategies capable of keeping the ct patient dose as low as possible whilst allowing for diagnostic images addressing the clinical question . 
although some authors [ 5 , 6 ] support the use of such shields , one paper [ 7 ] states that the application of shields for the eyes , the thyroid and the breasts is unnecessary : with regard to the eye , because the dose to the eye lens is low compared with the 5 - sv threshold dose for radio - induced cataract ( although they do not consider that lens opacity may be induced by doses as low as 0.5 sv [ 8 ] ) ; as regard to the thyroid , because the reduction of total energy imparted is only modest ; with lavvento della tomografia computerizzata ( tc ) multibanco , ha determinato un significativo aumento dellutilizzo clinico della tc che ora rappresenta pi del 30% di tutte le indagini mediche che utilizzano raggi x . 
nelle regioni con i pi alti livelli di assistenza sanitaria ( classificate dallunited nations scientific committee on the effects of atomic radiation [ unscear ] [ 1 ] come paesi di livello 1 ) , il contributo delle procedure tc alla dose collettiva derivante da esposizioni mediche passato dal 18% nel 1980 al 41% nel 1990 ( per un totale del 34% in tutto il mondo )  . 
 a causa dellassenza di tessuti sovrastanti , la dose impartita agli organi radiosensibili superficiali che rientrano , spesso accidentalmente , nella zona di indagine , come il cristallino , la tiroide o la mammella , pu essere significativa e raggiungere e in qualche caso superare i livelli di dose per linduzione di effetti radiogeni . 
questa potenziale esposizione ad alte dosi rende necessario sviluppare strategie di ottimizzazione al fine di mantenere la dose al paziente ai livelli pi bassi possibili senza diminuire , allo stesso tempo , la qualit diagnostica delle immagini . diversi metodi possono essere implementati per ridurre la dose al paziente . 
sebbene tale startegia sia sostenuta da alcuni autori [ 5 , 6 ] , un lavoro [ 7 ] sostiene che , per diverse ragioni , non sia necessario utilizzare queste protezioni : nel caso del cristallino , perch la dose risulta bassa rispetto alla dose soglia per linduzione di cataratta , pari 5 sv ( viene tuttavia trascurato il fatto che lopacit del cristallino pu insorgere a dosi inferiori a 0 , 5 sv [ 8 ] ) ; per la tiroide , a causa della bassa riduzione di dose che si pu ottenere , infine , per la mammella poich si pu raggiungere 154 radiol med ( 2010 ) 115 : 152169 regard to the breast , because the same dose reduction can be achieved by reducing the milliampere with the same level of image quality . 
 la stessa riduzione di dose diminuendo i ma , mantenendo inalterata la qualit dellimmagine . essendo il dibattito sullefficacia di tali schermature nel ridurre la dose al paziente ancora aperto , si ritiene che ulteriori approfondimenti possano contribuire a chiarire la questione . 
scopo di questo lavoro valutare la dose equivalente agli organi superficiali radiosensibili ( tiroide , cristallino , mammella ) e stimare la riduzione di dose ottenuta utilizzando schermature al bismuto sul paziente durante gli esami tc . 
inoltre lo studio si prefigge di valutare limpatto di queste protezioni sulla qualit dellimmagine diagnostica e confrontare la stessa con quella ottenuta riducendo i ma . materials and methods the study was conducted on two ct scanners installed in our radiology department : a 64 - slice ge lightspeed vct scanner , and an eight - slice ge lightspeed pro16 scanner ( 16 detector rows and eight channels )  . 
the number of examinations rose steeply over the first 5 years of the twenty - first century from 9 , 425 examinations in 2001 to 14 , 600 in 2006 . 
our hospital serves a population of 125 , 000 people , and considering the number of ct examinations per 1 , 000 inhabitants , these amounted to 117 in the year 2006 , making ct examinations the major source of increased collective radiation dose . 
the eye lens shield is 14 cm4 cm and was positioned over protective plastic glasses of the kind normally used to prevent biological risks . materiali e metodi lo studio stato condotto sulle due apparecchiature tc installate presso il dipartimento di diagnostica per immagini dellospedale di aosta : ge light speed vct 64 banchi e ge light speed 16 pro 8 slice ( 16 banchi e 8 canali di lettura )  . 
landamento del numero di prestazioni presso la nostra radiologia ha seguito il trend riportato dallunscear per i paesi di livello 1 con un rapido incremento fra il 2000 e il 2006 , che ha registrato il passaggio da 9425 esami nel 2001 a 14600 esami nel 2006 . 
considerato il bacino di utenza dellospedale pari a 125000 abitanti , il numero di esami tc per 1000 abitanti nel 2006 risulta pari a 117 con un aumento significativo , rispetto agli anni precedenti , del numero di prestazioni tc e della corrispondente dose collettiva . riduzione della dose per ridurre la dose agli organi radiosensibili superficiali durante gli esami tc sono state utilizzate le schermature attenurad ( f&l medical products , vandergrift , pa , usa )  . ogni schermatura costituita da 4 strati di bismuto di 0 , 0085 g / cm2 pari a 0 , 015 mm di pb ( attenuazione del 14% a energie di 120 kv , spessore emivalente [ hvl ] 5 , 6 mmal )  . questi tipi di protezioni sono disponibili sul mercato in tre diverse forme adatte per essere posizionate rispettivamente sulla mammella , sul cristallino e sulla tiroide . 
la protezione per la mammella si compone di due schermi che misurano 2025 cm tenuti insieme dal velcro e appoggiate su uno strato di gomma piuma di 0 , 7 cm ; lo schermo per la tiroide misura 126 cm ed posizionato su uno strato di gomma piuma spesso 1 , 5 cm ; le schermature per il cristallino di 144 cm sono appoggiate su un paio di radiol med ( 2010 ) 115 : 152169 occhiali simili a quelli utilizzati per la protezione dal rischio biologico . 
 valutazioni di dose la dose agli organi radiosensibili superficiali stata misurata con dosimetri termoluminescenti lif : mg , ti ( tld - 100 )  . tld provenienti dallo stesso lotto sono stati calibrati in termini di dose assorbita in aria e in acqua utilizzando unapparecchiatura radiologica tradizionale . 
per valutare la riduzione di dose ottenuta utilizzando le schermature , sono stati esposti ai principali protocolli tc set di 3 tld posizionati su un fantoccio antropomorfo con e senza schermature . 
to assess the effect of shielding on dose reduction , sets of three tlds were exposed to different standard ct examination protocols performed on an anthropomorphic phantom both with and without the protective shields . 
the average attenuation value from the different ct protocols was considered to be the organ - dose reduction factor offered by the shield and was used to assess the impact of the shield on the effective dose to the patient . 
the same method was used to evaluate the attenuation factors in vivo by applying bismuth shielding to patients undergoing the same ct procedures . tld calibration the tlds were calibrated by performing in air measurements at 120 kv and variable milliampere ( ge prestilix device , maximum kvp 150 , maximum ma 800 , hvl 2.9 mmal ) exposing three tlds simultaneously with an ionising chamber model m23331 ( ptw , freiburg , germany ) connected to a ptw unidose electrometer . 
linfluenza dellindurimento del fascio sulla risposta dei tld stata valutata esponendo una serie di tld a varie profondit in un fantoccio acqua equivalente con procedure analoghe a quelle seguite per la calibrazione in aria . valutazioni di dose in un fantoccio antropomorfo la riduzione di dose per i protocolli tc pi utilizzati che comprendono nella zona dinteresse mammella , cristallino e tiroide ( tabella 1 e 2 ) ( torace standard , cervicale , cranio standard e cranio alta risoluzione sulla ge light speed 16 pro ; torace standard , poligono di willis , supercranio , cranio helical per ge light speed vct - 64 ) stata valutata utilizzando un fantoccio antropomorfo alderson rando . 
per misurare la dose allorgano , i tld sono stati posizionati negli alloggiamenti allinterno della mammella a 2 cm di profondit e negli alloggiamenti predisposti per la tiroide a 2 , 5 cm 156 radiol med ( 2010 ) 115 : 152169 precision of the ionisation chamber measurements was assumed to be equal to 5% , as reported on the calibration certificate , whereas the precision of the tld measurements was evaluated by exposing 20 tlds . 
the influence of beam hardening on the tld reading was evaluated by a series of measurements taken at different depths in a water - equivalent phantom slab following the same procedure as used with in - air calibration . dose evaluation in the anthropomorphic phantom the dose reduction obtained in the breasts , the eye lenses and the thyroid during the most commonly used protocols ( tables 1 and 2 ) ( standard chest , cervical , standard head and high - resolution head for the ge lightspeed pro16 unit ; standard chest , willis circle , standard head , fast head , helical head for the ge lightspeed vct - 64 unit ) was measured using the alderson rando anthropomorphic phantothe tlds were placed both in the holes inside the breast ( 2 - cm deep ) and at the thyroid level ( 2.5 - cm deep ) to measure the dose to the organ and on the phantom surface , and over the breast , the eye and the thyroid to evaluate the entrance surface dose and verify the consistency of measurements on the phantom and in vivo . each ct examination was repeated twice , with and without the bismuth shields , to measure the attenuation factor and verify the efficacy of the shields in reducing organ dose . 
in all cases , the bismuth shields were placed over the phantom after the scout acquisition to avoid variations in the irradiation parameters due to the automatic exposure syste in fact , the presence of bismuth protections during scout scans causes an increase in the radiation attenuation of the phantom as well as in the milliampere selected by the automatic exposure system . in vivo measurements the number of protocols tested for each ct unit , the characteristics of which are reported in tables 1 and 2 , was determined by the availability of the machines . 
per valutare la dose ingresso pelle e verificare la consistenza dei risultati delle misure in vivo e su fantoccio , i tld sono stati posizionati sulla superficie del fantoccio in corrispondenza di mammella , cristallino e tiroide . per misurare il fattore di attenuazione e verificare lefficacia delle schermature nella riduzione della dose agli organi ogni esame tc stato ripetuto due volte , con e senza schermi . 
infatti la presenza delle protezioni in bismuto durante lo scout causa un aumento dellattenuazione del fantoccio e , di conseguenza , un aumento nel valore dei ma selezionati dallesposimetro automatico . misure in vivo il numero di protocolli valutati per ognuna delle due apparecchiature tc , le cui caratteristiche sono riportate in tabella 1 e 2 , stato determinato in base alla disponibilit delle apparecchiature . 
si sono posizionati 3 tld sotto la schermatura e 3 sul lato non protetto per misurare il fattore di attenuazione . gli schermi per la mammella sono stati utilizzati su 14 pazienti negli esami torace , addome , colonscopia virtuale , uro - tc e renale trifasica ; gli schermi per il cristallino sono stati utilizzati su 3 pazienti per due protocolli helical dedicati al cranio e allorecchio ; per la tiroide gli schermi sono stati testati su 6 pazienti per protocolli : cranio , collo e carotide - poligono di willis riduzione della dose efficace i parametri desame ( tensione , ma , tempo di rotazione e collimazione ) impostati per pazienti di corporatura standard sono stati utilizzati per calcolare la dose efficace e la dose equivalente agli organi con il software sviluppato dal national radiological protection board ( nrpb ) adattato dal gruppo imaging performance assessment of ct scanners ( impact ) [ 9 ]  . 
organ dosereduction factors , obtained by phantom and in vivo measurements , were applied to the organ dose equivalent values to assess the effects of the protective shields on effective dose to the patient . 
 image quality assessment quality evaluation in phantom the effects of the shields on the ct image were quantitatively evaluated and compared with the quality of the image obtained when reducing the milliampere , which were reduced to obtain administration of the same dose to the superficial radiosensitive organs as that obtained with the use of shields . 
la qualit dellimmagine stata valutata analizzando i principali parametri come il contrasto ( risoluzione ad alto e basso contrasto ) e il rumore , che rappresentano i parametri chiave per la sua valutazione secondo i protocolli internazionali [ 3 , 10 ]  . 
 un fantoccio ge dedicato , costituito da una sezione uniforme e da una con dettagli ad alto e basso contrasto , stato esposto in tre diverse modalit : con parametri standard ( 120 kv , 200 ma , 1 s di rotazione , 5 mm di spessore ) , introducendo le schermature e diminuendo i ma ( 115 ma ) fino ad ottenere lo stesso valore di dose ottenuto utilizzando le protezioni in bismuto e misurata utilizzando una pencil camera alloggiata in un fantoccio cilindrico , 1 cm sotto la superficie . 
a uniform cylindrical phantom and a pencil chamber , positioned in a slot 1 cm under the surface of the phantom , were used to define the amount of milliampere reduction . 
this procedure was used to confirm the linear correlation between dose and milliampere and that the milliampere needed to be decreased to the same percentage as that of the dose reduction . con schermature e riducendo i ma . 
i ma sono stati ridotti di una percentuale pari alla percentuale di riduzione di dose alla mammella ottenuta utilizzando le schermature . per ognuna delle tre acquisizioni stata selezionata la stessa slice . 
le slices sono state suddivise in regioni di interesse ( roi ) quadrate di 2020 pixel e il rumore , definito come la deviazione standard della roi , stato valutato in tutte le ragioni contenenti solo acqua . 
 per tutti i fantocci il rumore a tutte le profondit stato calcolato con imagej 1 , 35p ( national institutes of health , usa ) [ 11 ] e i risultati sono stati confrontati utilizzando il test t di student . valutazione della qualit in vivo noise was evaluated by using an elliptical water phantom simulating a thorax . 
the phantom is subdivided into four linfluenza delle schermature di bismuto sulla qualit dellimmagine stata valutata in base alla presenza di radiol med ( 2010 ) 115 : 152169 artefatti . 
the slice was then divided into 20 - 20 - pixel square regions , and the noise , defined as the region standard deviation , was evaluated in all regions that contained only water . 
data obtained were compared using students t test . in vivo quality evaluation the influence of bismuth shields on ct image quality was assessed on the basis of the presence of artefacts . 
the tld measurement overall error was evaluated to be 9% . organ dose evaluation in the anthropomorphic phantom the results obtained for each protocol for different acquisition parameters are reported in table 3 in terms of dose to the organs and dose reduction . 
the average values for shield efficacy were 30%10% for the thyroid shield , 41%15% for the breast shield and 48%17% for the eye - lens shield . effective dose reduction table 4 reports both equivalent dose ( ht ) and effective risultati valutazione di dose calibrazione dei tld la precisione delle misure dei tld stata stimata pari al 7% . 
lerrore totale delle misure con tld stata valutata essere pari al 9% . valutazione della dose agli organi nel fantoccio antropomorfo i risultati ottenuti per ogni protocollo nelle diverse condizioni di esposizione sono riportati in tabella 3 in termini di dose agli organi e di riduzione di dose . 
 riduzione della dose effettiva la tabella 4 riporta la dose equivalente ( ht ) e la dose efficace ( htwt ) per i diversi organi a rischio ( oars )  . questi valori sono stati calcolati per la mammella e la tiroide utilizzando , come gi riportato , il software impact . 
il contributo del cristallino alla dose efficace in accordo con linternational commission on radiological protection pubblicazione 60 ( icrp60 ) [ 12 ] , pu essere considerato trascurabile e quindi non compare nellanalisi . 
in tabella 4 sono riportati i valori di dose stimati nel caso in cui vengano utilizzate le protezioni in bismuto , considerando i fattori di attenuazione valutati sperimentalmente in vivo ed in fantoccio , come riportato in tabella 3 . 
la tabella 4 mostra che la dose efficace per ogni scansione pari a 3 , 9 , 7 , 7 , 3 , 3 e 6 , 6 msv rispettivamente per esami torace , addome , collo e cervicale . 
luso delle protezioni comporta una riduzione della dose efficace , la cui entit dipende dal tipo di esame : 0 , 4 , 0 , 2 , 1 , 2 e 2 , 5 msv rispettivamente per torace , addome , collo e cervicale . 160 radiol med ( 2010 ) 115 : 152169 fig . 
table 4 also contains the dose values evaluated when the shields were used , taking into account the attenuation factors experimentally assessed in the phantom and in vivo , as reported in table 3 . 
lincremento del rumore ottenuto riducendo i mas superiore in modo statisticamente significativo a quello ottenuto utilizzando gli schermi ( p < 0 , 01 )  . valutazione in vivo image quality assessment quality evaluation in the anthropomorphic phantom the results obtained for highand low\ - contrast resolution lanalisi delle risposte dei radiologi al questionario per la valutazione della qualit dellimmagine riportata in figura 7 . 
la qualit dellimmagine risulta sufficiente nel 20% dei casi e buona nel restante 80% dei casi . 162 radiol med ( 2010 ) 115 : 152169 table 3 phantom and in vivo studies : unshielded and shielded dose for each protocol . 
the number of sequences for each exam is indicated by sequence number ct model protocol unshielded ( mgy ) shielded ( mgy ) phantom study ct 8 slices phantom study ct 64 slices in vivo study ct 8 slices in vivo study ct 64 slices chest neck cervical head , high resolution head , standard carotids he 1.25 chest head , 2.5 / 5 cta carotid willis head , helical head , fast axial cervical , helical kidney , three - phase chest + abdomen seq . 
image quality was considered adequate in 20% of cases and good in the remaining 80% . anche se ulteriori approfondimenti possono essere utili per confermare i nostri risultati , lo studio ha dimostrato che luso di schermature individuali , come quelle in bismuto da noi utilizzate , pu rappresentare unottima strategia per ridurre la dose al paziente senza inficiare la qualit dellimmagine diagnostica . 
utilizzando i supporti in gomma piuma per le protezioni per la mammella e la tiroide o gli occhiali in plastica per la protezione per il cristallino , gli artefatti risultano essere trascurabili . 
 [ numero ] modello ct protocollo organi a rischio non schermati ( mgy ) schermati ( mgy ) studio con fantoccio ct 8 slices studio con fantoccio ct 64 slices studio in vivo ct 8 slices studio in vivo ct 64 slices torace collo cervicale cranio alta risoluzione cranio standard carotide he 1 , 25 torace cranio 2 , 5 / 5 cta carotide willis cranio helical cranio hast axial cervicale helical rene tre fasi torace + addome , seq . 
2 uro - ct cranio cranio orecchio helical torace cranio + cta carotide willis mammella tiroide tiroide tiroide cristallino tiroide cristallino cristallino tiroide tiroide tiroide cristallino cristallino tiroide cristallino cristallino cristallino tiroide mammella mammella mammella mammella mammella tiroide mammella mammella mammella mammella mammella mammella mammella cristallino cristallino cristallino tiroide tiroide 19 , 9 44 , 5 34 , 6 23 , 8 20 , 7 1 , 85 54 , 9 33 , 5 88 , 1 20 , 3 11 , 5 115 , 4 37 , 8 15 , 0 14 , 8 28 , 1 138 , 8 25 , 7 10 , 4 29 , 9 56 , 4 65 , 3 26 , 7 46 , 0 24 , 1 74 , 9 17 , 6 15 , 3 35 , 3 24 , 2 54 , 4 66 , 5 12 , 5 59 , 8 24 , 8 12 , 2 80 , 5 14 , 9 16 , 6 33 , 5 41 , 7 32 , 6 aec , sistema automatico di modulazione dei ma ; ct , tomografia computerizzata ; cta , angiografia con tomografia computerizzata ; he , elicoidale discussion although further studies are needed to confirm our findings , our study shows that the use of individual devices for patient protection , such as the thin overlying bismuth radioprotective shield , may represent an effective optimisation strategy able to reduce patient dose without compromising the quality of the diagnostic images . 
image quality , in terms of high - contrast resolution , low - contrast resolution and noise , was better when bismuth shields were di risoluzione ad alto e basso contrasto e rumore , migliore sulle immagini ottenute utilizzando le schermature rispetto a quelle ottenute riducendo i ma . 
the in vivo tests show that the use of breast shielding does not affect the correct diagnostic evaluation of the area of interest and causes no appreciable deterioration in the images in the lung fields or the mediastinuthough minimal and acceptable , some deterioration was observed in the depiction of the front wall structures , which are , however , rarely of interest statisticamente inferiore a quello ottenuto riducendo i ma . le immagini del cranio valutate con la finestra per il parenchima e per losso non hanno evidenziato alterazioni significative . sulla base dei risultati ottenuti in questo studio le schermature in bismuto sembrano rappresentare un utile strumento per ridurre la dose al paziente . 
images of the head were evaluated with both a brain parenchyma window and a bone window ; in either case , no lack of information or reduction in diagnostic power was recorded . 
the eye shield provided a significant dose reduction without loss of clinical image quality ; the thyroid shield offered a strong reduction in organ and effective dose ; the breast shield allowed for a high dose reduction with an acceptable deterioration of image quality ( undetected by the radiologists ) , which was at any rate lower than that observed with reduced milliampere . 
 the dose values measured for the breast , the thyroid and the eye lens ( table 3 ) and the effective dose calculated by using impact software ( table 4 ) are comparable with those reported by the icrp [ 2 ] and other publications [ 6 , 13 ]  . 
the measured doses to the thyroid in chest ct were higher than those reported in the literature [ 4 , 6 , 7 ] and may be related to the use of multidetector row ct scanners ( eight and 64 slices ) in spiral configuration , in which the radiation beam extends beyond the reconstructed region . 
however , the published data refer to measurements performed with single - , twoor four - slice ct scanners , as the first eightslice scanner was introduced in 2000 [ 14 ]  . 
 the high dose values measured for the eye lens can be explained by considering that multislice ct does not allow for complete avoidance of orbits even when using gantry angulation [ 15 ]  . 
the use of the shield reduced the organ dose by 48% ( see table 3 ) and consequently halved the risk of lens opacity . application of the effective dose data reported in table 4 to the different scans considered and the average number of ct scans per year ( 5 , 000 chest , 6 , 000 abdomen , 500 cervical and 900 neck ) yielded a total collective effective dose of 72 sv , allowing for a crude estimate of the corresponding lifetime risk for radiation - induced fatal cancer . 
it is important to note that although the icrp 60 risk factors are generally accepted by the international community as a radiation protection policy , their use cristallino consentono un elevato risparmio di dose senza perdita di qualit dellimmagine ; le protezioni per la tiroide garantiscono un elevata riduzione della dose equivalente allorgano e della dose efficace ; la protezione per la mammella permette di ottenere unelevata riduzione della dose allorgano con una modesta perdita di qualit dellimmagine , non rilevata dai radiologi , e comunque inferiore al deterioramento determinato dalla riduzione dei ma . i valori di dose misurati per mammella , tiroide e cristallino ( riportati in tabella 3 ) e la dose efficace calcolata usando il software impact ( tabella 4 ) sono confrontabili con quelli riportati dallicrp [ 2 ] e da altre pubblicazioni [ 6 , 13 ]  . 
la maggiore dose alla tiroide valutata per gli esami del torace rispetto a quella riportata in letteratura [ 4 , 6 , 7 ] pu essere giustificata dalluso di tc multibanco ( 8 e 64 banchi ) in modalit spirale . 
in questa modalit , a causa delle modalit di ricostruzione dellimmagine , il fascio di radiazione investe direttamente anche le zone limitrofe ai volumi effettivamente ricostruiti sullimmagine , mentre inizialmente solo la prima corona di detettori contribuisce allimmagine ; procedendo con lacquisizione , il numero delle corone interessate aumenta fino a raggiungere la totalit . 
in ogni caso i dati di letteratura si riferiscono ad esposizioni con tc a 1 , 2 o 4 banchi , in quanto le tc a 8 banchi sono state introdotte nel 2000 [ 14 ]  . i valori elevati di dose misurati per il cristallino sono giustificabili considerando che nellacquisizione con tc multibanco non possibile escludere completamente le orbite anche inclinando il gantry [ 15 ]  . 
di conseguenza la dose soglia per lopacit del cristallino ( 0 , 52 gy ) pu essere superata usando i protocolli ad alta risoluzione ( ad esempio supercranio in ge 8 banchi o encephalon helical in ge 64 banchi )  . 
 utilizzando i valori di dose efficace riportata in tabella 4 e considerando il numero medio di esami per anno ( 5000 toraci , 6000 addomi , 500 cervicali e 900 colli ) si ottiene una dose efficace collettiva pari a 72 sv , che permette una stima del rischio di tumori radio - indotti associati . 
in accordo con i dati dellicrp60 il rischio di induzione di tumori mortali pari al 5% per sv per la popolazione ( che corrisponde ad 1 decesso ogni 20000 persone per 1 msv ) [ 12 ]  . 
importante sottolineare che anche se i fattori di rischio stimati dallicrp60 [ 12 ] sono accettati dalla comunit scientifica nelle applicazioni radio - protezionistiche , il loro uso resta controverso in quanto derivati dagli studi relativi alla popolazione giapponese dopo lesposizione alle bombe 168 radiol med ( 2010 ) 115 : 152169 remains controversial , as they have been derived from studies of japanese citizens exposed in the hiroshima and nagasaki atomic bomb attacks [ 16 , 17 ]  . 
as stressed in a recent statement issued by the american association of physicists in medicine [ 18 ] , japanese citizens were exposed head to toe to a mixture of x - rays and particulate radiations , whereas ct examinations involve only x - rays over a small fraction of the patients body . 
in addition , the majority of atom - bomb survivors received radiation doses many times higher than those of modern ct , and the mathematical extrapolations used for scaling the very high radiation exposure levels down to the much lower exposure levels typical of partial - body ct examinations remain very controversial . the use of bismuth shielding has led to an effective dose reduction of 5.5 sv , corresponding to a lifetime risk reduction of 1.4 deaths over a 5 - year period [ 12 ]  . 
the cost of one set of shields is approximately 150 , and each set can be used for at least 1 , 000 patients ; consequently , the relative additional cost for each examination is less than 0.15. 
in fact , the presence of the bismuth protection during the scout scan will increase both the radiation attenuation of the patient and the milliampere selected by the automatic exposure system or other automatic dose - reduction systems . 
positioning of the shields after the scout acquisition will maximise the dose saving already provided by the automatic exposure syste in conclusion , our study shows that the use of bismuth protection to shield the lens of the eye , the breast and the thyroid can lead to a significant decrease in both organ and effective dose , with a consequent appreciable reduction in the health risk for the patient . 
high cost - effectiveness , ease of use and absence of any substantial deterioration of image quality suggest that bismuth shields could be introduced on a large scale into clinical routine as a first step towards the optimisation of patient exposure . 
come infatti ricordato in una recente pubblicazione dellamerican association of physicist in medicine [ 18 ] , i cittadini giapponesi hanno subito unesposizione al corpo intero da parte di campi misti di particelle e raggi x , mentre negli esami tc lesposizione relativa ai soli raggi x e ad una porzione limitata del corpo . 
inoltre , i sopravvissuti alla bomba atomica sono stati esposti a dosi molto superiori rispetto a quelle della tc e luso delle regressioni matematiche per estrapolare il rischio alle basse dosi tipiche della tc rimane controverso . lutilizzo delle protezioni in bismuto ha prodotto una riduzione di dose efficace di 5 , 5 sv corrispondente a una riduzione del rischio pari a 1 , 5 decessi in 5 anni [ 12 ]  . 
gli schermi sono utilizzati nel nostro dipartimento da oltre un anno e non hanno influenzato il numero di esami giornalieri . per ottimizzare lefficacia delle protezioni opportuno posizionarle dopo lesecuzione della scansione scout , in quanto la presenza dello schermo aumenterebbe lattenuazione e di conseguenza i mas selezionati dallesposimetro automatico o da altri sistemi di riduzione della dose . il posizionamento della schermatura dopo lesecuzione della scansione scout aumenta ulteriormente il risparmio di dose ottenuto tramite lutilizzo dellesposimetro automatico . concludendo , il presente lavoro dimostra che luso delle protezioni di bismuto per schermare il cristallino , la tiroide e la mammella determina un significativo risparmio sia della dose agli organi che della dose efficace con una conseguente sensibile riduzione del rischio per il paziente . 
skin thickening was identified in eight patients ( 58% ) , oedema in nine ( 64% ) , nipple retraction in two ( 14% ) , architectural distortion in eight ( 58% ) , mass - like enhancement in five ( 36% ) , non - mass - like enhancement in nine ( 64% ) with washout enhancement curve in 12 ( 86% ) and plateau curve in two ( 14% ) , axillary lymphadenopathy in 12 ( 86% ) and internal mammary artery lymphadenopathy in two ( 14% ) , and pectoral muscle enhancement in one ( 7% )  . 
the most characteristic mr findings of ibc are skin thickening , oedema , architectural distortion , masslike enhancement with washout curve and axillary lymphadenopathy ; less frequent ones are nipple retraction , mass - like enhancement and internal mammary lymphadenopathy . 
ispessimento cutaneo era presente in 8 pazienti ( 58% ) , edema cutaneo in 9 ( 64% ) , retrazione del capezzolo in 2 ( 14% ) , distorsione architetturale in 8 ( 58% ) , impregnazione parenchimale tipo massa in 5 ( 36% ) , e tipo non massa in 9 ( 64% ) con curva dinamica di impregnazione persistente in 2 ( 14% ) e con wash - out in 12 ( 86% ) , impregnazione cutanea in 2 ( 14% ) , adenomegalia ascellare in 12 ( 86% ) e mammaria interna in 2 ( 14% ) , impregnazione pettorale in 1 ( 7% )  . 
nel carcinoma infiammatorio , i segni rm pi caratteristici sono ispessimento , edema cutaneo , distorsione architetturale , impregnazione estesa tipo non massa con andamento wash - out e linfoadenopatia ascellare ; meno frequenti , retrazione del capezzolo , impregnazione tipo massa e adenomegalia mammaria interna . 
la presenza di liquido pre - pettorale frequente e non ne comporta infiltrazione . keywords breast inflammatory breast cancer mr imaging parole chiave mammella carcinoma infiammatorio risonanza magnetica radiol med ( 2010 ) 115 : 7082 introduction inflammatory breast carcinoma ( ibc ) , also known as carcinomatous mastitis , is the most aggressive form of locally advanced breast cancer . 
its name refers to a clinical pattern of extensive involvement of dermal lymphatic vessels and swollen and reddened appearance of the breast rather than to any specific histological type . the clinical manifestations of ibc include discolouration with diffuse or mottled reddening of the skin extending to at least one third of the breast , dimpled peau dorange skin , a ridge at the borders of the affected area , breast mass or tenderness associated with pain and increase in volume and temperature of the entire breast . 
the breast therefore shows the typical signs and symptoms of acute inflammation , in particular , oedema and reddening , of less than 23 months duration [ 1 ]  . 
 pathology of a specimen of breast tissue reveals the presence of carcinoma , commonly poorly differentiated infiltrating ductal carcinoma , even though any histological type of breast cancer may be associated with ibc . 
the breast parenchyma is distorted by the cancer cells , with oedema and inflammatory infiltrates ; the vascular structures are invaded by tumour emboli . ibc is rare , accounting for 1%6% of all breast cancers . it has an incidence is 0.7 cases per 100 , 000 persons per year , with a mean age at onset of 58 years [ 25 ]  . 
survival is approximately 1236 months [ 1 ]  . typical or common ibc ( 50% of cases ) is characterised by all the clinical signs and symptoms of inflammatory carcinoma described above . 
finally , clinical ibc or pseudo - ibc ( 40% of cases ) shows all the inflammatory signs and symptoms and often manifests as a palpable mass without evidence of subdermal lymphatic invasion [ 28 ]  . magnetic resonance ( mr ) imaging of the breast was introduced by fischer in 1999 [ 9 ] , and since then numerous , authors have endeavoured to identify the indications and potential of the examination [ 10 ]  . 
widely accepted indications introduzione il carcinoma infiammatorio della mammella ( inflammatory breast carcinoma , ibc ) o mastite carcinomatosa la forma pi aggressiva di tumore mammario localmente avanzato la cui denominazione si riferisce alla presentazione clinica con esteso coinvolgimento dei vasi linfatici dermici e aspetto tumefatto ed eritematoso della mammella e non ad un tipo istologico specifico . le manifestazioni cliniche dellibc comprendono una discolorazione rossa o a chiazze della cute , estesa ad almeno 1 / 3 della superficie della mammella , pelle con aspetto a buccia darancia , uno scalino ai margini della zona infiammata , una massa o fragilit dei tessuti mammari associati a dolore e un aumento del volume e della temperatura dellintera mammella . 
 lesame anatomo - patologico di un frammento di ghiandola mammaria evidenzia la presenza di carcinoma mammario , pi frequentemente di carcinoma duttale infiltrante scarsamente differenziato , anche se un qualsiasi tipo istologico di tumore mammario pu associarsi a ibc . 
il parenchima ghiandolare risulta alterato dalle cellule tumorali presenti , con edema e infiltrati infiammatori ; le strutture vascolari in esso comprese sono invase da emboli neoplastici . il carcinoma infiammatorio della mammella raro , rappresentando l1%6% di tutti i tumori mammari . 
secondo il sistema di stadiazione tnm , il carcinoma infiammatorio classificato come t4d [ 6 ] ; alla diagnosi nella maggior parte dei casi vi un interessamento clinico dei linfonodi e nel 20% metastasi a distanza . 
la sopravvivenza si aggira intorno ai 1236 mesi [ 1 ]  . libc tipico o comune ( 50% dei casi di ibc ) caratterizzato dalla presenza di tutti i segni e sintomi clinici del carcinoma infiammatorio , precedentemente descritti , localizzati a una mammella in associazione a un reperto istologico positivo per emboli tumorali nei vasi linfatici subdermici e del parenchima mammario . 
infine libc clinico o pseudo - ibc ( 40% dei casi ) presenta tutti i sintomi infiammatori e spesso si manifesta con una massa palpabile senza riscontro di invasione linfatica subdermica [ 28 ]  . lo studio della mammella con risonanza magnetica radiol med ( 2010 ) 115 : 7082 for breast mr imaging are the detection of breast cancer in young women at high genetic risk , in patients with cancer of unknown primary ( cup ) syndrome and in those with breast implants , the characterisation of doubtful mammographic and sonographic findings , the staging of histologically proven cancers , the evaluation of locally advanced cancers before or after neoadjuvant chemotherapy and postsurgical follow - up [ 11 , 12 ]  . 
 numerous papers have reported the mr imaging patterns of the most common breast carcinomas infiltrating ductal and lobular carcinoma whereas the features of the rarer breast malignancies are less well known . 
 the aim of this study was to describe the mr imaging features of ibc on the basis of a review of the literature and our personal experience . materials and methods patients as the study was based on a retrospective review of mr examinations , the patients informed consent was not required . 
during a search of the radiology and pathology archives of our institution to identify all patients studied by breast mr and all histological examinations of needlebiopsy or surgical specimens carried out between january 2005 and march 2008 , we identified 25 patients with a pathological or clinical diagnosis of ibc . 
 the study included patients with breast carcinoma associated with clinical signs of inflammation and those with a histological diagnosis of massive neoplastic invasion of the subdermal lymph vessels who underwent mr imaging before surgery or chemotherapy . 
patients were excluded if they had clinical evidence of ibc without a histological diagnosis ( n = 2 ) , those studied by mr imaging after undergoing chemotherapy ( n = 3 ) or surgery ( n = 1 ) and those with a pathological diagnosis of ibc not studied by mr imaging ( n = 5 )  . our final study population therefore comprised 14 patients , with a mean age of 48 ( range 3181 ) years . 
eleven patients had clinical evidence of ibc ( typical ibc ) ; the remaining three had no clinical signs but only histological evidence of lymphatic vessel infiltration ( occult ibc )  . 
with regard to hormone status , nine patients were premenopausal and five were postmenopausal ; nine had had pregnancies with a mean number of two children , and in one case the clinical picture arose during the puerperiu a positive family ( rm ) stato introdotto nel 1999 da fischer [ 9 ] e da allora molti autori si sono adoperati per individuarne le indicazioni e le possibilit [ 10 ]  . 
le applicazioni riconosciute con largo consenso sono lidentificazione di neoplasie mammarie in giovani donne ad alto rischio genetico , in pazienti con cancer of unknown primary ( cup ) syndrome e con protesi mammarie , la caratterizzazione di reperti mammografici ed ecografici di incerto significato diagnostico , il bilancio di estensione di neoplasie gi istologicamente diagnosticate o nella valutazione pree postchemioterapia neoadiuvante in caso di tumori localmente avanzate e il follow - up post chirurgico [ 11 , 12 ]  . 
 un crescente numero di lavori ha descritto gli aspetti relativi alla semeiotica rm delle neoplasie mammarie pi frequenti carcinoma duttale e lobulare infiltrante mentre sono meno conosciute le caratteristiche delle neoplasie maligne rare della mammella . 
 scopo di questo studio quello di descrivere gli aspetti semeiotici nellindagine rm del carcinoma infiammatorio della mammella basandoci sullanalisi dei dati della letteratura e di quelli ottenuti nellesperienza personale . materiali e metodi pazienti lo studio stato condotto con la valutazione retrospettiva degli esami rm e quindi senza il consenso informato della paziente . 
dalla ricerca nellarchivio radiologico delle pazienti sottoposte a indagine rm mammaria e nellarchivio patologico di tutti gli esami istologici su frustoli agobioptici o pezzi chirurgici , nel periodo compreso fra gennaio 2005 e marzo 2008 sono state individuate 25 pazienti con diagnosi patologica o clinica di carcinoma infiammatorio . 
 sono state incluse nello studio le pazienti con neoplasia mammaria accompagnata da segni clinici di infiammazione e quelle con diagnosi istologica di massiva infiltrazione neoplastica dei vasi linfatici subdermici sottoposte a indagine rm prima dellintervento chirurgico e della chemioterapia . 
sono state escluse le pazienti con rilievi clinici di carcinoma infiammatorio senza diagnosi istologica ( 2 casi ) e quelle sottoposte a rm dopo linizio della chemioterapia ( 3 casi ) o lintervento chirurgico ( 1 caso ) e quelle con diagnosi patologica di carcinoma infiammatorio non sottoposte a indagine rm ( 5 casi )  . 
pertanto la popolazione in studio costituita da 14 pazienti con et media di 48 anni e radiol med ( 2010 ) 115 : 7082 history , with at least one relative with previous breast cancer , was present in six cases . mr imaging imaging was performed with a 1.5 - t magnet ( symphony , siemens medical system , erlangen , germany ) without time limitations in all women . 
 image analysis image postprocessing involved subtraction of the precontrast images from the postcontrast images and generation of multiplanar reconstructions ( mpr ) and maximum intensity projections ( mip )  . 
regions of interest ( roi size 59 pixels ) were placed over the areas of contrast enhancement seen on the second acquisition after contrast administration to generate time - intensity curves . two radiologists ( gc , vg ) with 7 and 3 years experience with breast mr imaging , independently reviewed all images on the workstation . 
the baseline t2 - weighted sequences were assessed for breast enlargement , nipple retraction , skin thickening , skin oedema , architectural distortion , axially and internal mammary lymphadenopathy and presence of prepectoral fluid filthe dynamic studies were assessed for areas of increased parenchymal enhancement , cutaneous enhancement , pectoral muscle enhancement and hypertrophic internal mammary artery . 
 the areas of increased enhancement were classified as showing mass - like or non - mass - like enhancement ; areas of mass - like enhancement were analysed according to the morphological and dynamic parameters described by fischer [ 9 ] ; areas of non - mass - like enhancement were interpreted according to the breast imaging reporting and data system ( bi - rads ) lexicon with regard to morphological compresa fra 31 e 81 . 
undici pazienti presentavano un quadro clinico di carcinoma infiammatorio , configurando il gruppo ibc tipico ; nelle rimanenti 3 pazienti la clinica era muta , ma il reperto patologico era positivo per infiltrazione dei vasi linfatici , configurando il gruppo i ibc occulto . 
per quanto riguarda lo stato ormonale , 9 erano in et fertile e 5 in climaterio ; 9 avevano avuto gravidanze con numero medio di 2 figli e in un caso la clinica insorta nel puerperio . 
familiarit positiva , con almeno un parente colpito da tumore della mammella , era presente in 6 casi . indagine rm lo studio rm stato effettuato con un magnete da 1 , 5 t ( symphony , siemens medical system , erlagen , germania ) senza limitazioni temporali in tutte le donne . 
lo studio basale comprendeva una sequenza short - tau inversion - recovery ( stir ) con acquisizione trasversale ( utilizzando i seguenti parametri : tr / te : 5960 / 70 ms ; matrice 254320 pixel ; fov 350100 ; spessore 3 , 00 mm ) , una sequenza stir con acquisizione coronale ( con i seguenti parametri : tr / te : 4840 / 68 ms ; matrice 254320 pixel ; fov 350100 ; spessore 3 , 00 mm ) e una sequenza turbo spin - echo ( tse ) con acquisizione sagittale ( con parametri : tr / te : 3910 / 95 ms ; matrice 254320 pixel ; fov 320100 ; spessore 3 , 80 mm )  . 
lo studio dinamico stato eseguito con una sequenza gradient recalled echo ( gre ) 3d sul piano coronale ( utilizzando i seguenti parametri : tr / te : 12 / 5 , 65 ms ; flip angle 25 ; matrice 254320 pixel ; fov 38075 ; spessore 1 , 24 mm ; tempo di acquisizione 88 secondi ) acquisita prima della somministrazione di mdc e ripetuta per sei volte dopo liniezione endovenosa di 0 , 1 mmol di gd - dtpa / kg di peso corporeo alla velocit di 2 , 5 ml al secondo e di 20 ml di soluzione fisiologica . 
 analisi delle immagini le immagini sono state elaborate mediante sottrazione delle acquisizioni pre - contrasto da quelle post - contrasto e ricostruzioni multiplanari ( mpr ) e proiezioni a massima intensit ( mip )  . 
posizionando una regione dinteresse ( roi , estesa 59 pixels ) sulle aree di impregnazione di mdc visualizzate nella seconda acquisizione dopo mdc sono state costruite curve delle variazioni di intensit di segnale nel tempo . 
areas of non - mass - like enhancement were analysed in terms of distribution ( focal , linear , ductal , regional , multiregional , diffuse ) , internal characteristics ( homogeneous , heterogeneous , stippled / punctate , clumped , reticular - dendritic ) , asymmetry . kinetic curves were assessed for increased signal intensity during the first 2 min after contrast administration and curve pattern over the following minutes , with three possible time intensity - curves : progressive steady enhancement ( type i ) , rapid wash - in followed by a plateau ( type ii ) and rapid wash - in followed by wash - out ( type iii )  . pathological analysis the diagnosis of breast cancer was established by percutaneous biopsy with ultrasound - guided microhistological sampling in seven cases ( 14 - gauge needle and automated or semiautomated sampling devices ) or by ultrasound - guided cytological sampling ( 21 - gauge needle ) in seven cases . massive neoplastic infiltration of the subdermal lymphatic vessels was identified in the microhistological sample in seven cases and in the surgical biopsy in the remaining seven . 
patients with a microhistological diagnosis of ibc were immediately referred for neoadjuvant chemotherapy . the remaining seven patients with a pathological diagnosis of ibc were referred for chemotherapy after surgical biopsy . 
 pathological diagnoses were formulated by two pathologists with more than 10 years experience in breast diseases . histological analysis of the core biopsies and surgical specimens included histological tumour type according to the world health organisation ( who ) classification , tumour grade ( g1 , g2 , g3 ) according to the elston - ellis easton system [ 14 ] and infiltration of the axillary lymph nodes ( negative / positive )  . statistical analysis interobserver variability in determining the type of enhancement and the morphological and dynamic parameters ( such as shape , margins , enhancement pattern and distribution ) was evaluated with the k statistic . 
the degree of concordance was classified as follows : 0.010.20 slight agreement , 0.210.40 fair agreement , 0.410.60 moderate agreement , 0.610.80 good agreement and 0.811.0 , almost perfect agreement . 
i rilievi analizzati nelle sequenze basali t2 - dipendenti senza mezzo di contrasto sono stati : aumento del volume mammario , retrazione del capezzolo , ispessimento cutaneo , edema cutaneo , distorsione architetturale , adenomegalia ascellare e mammaria interna , presenza di film liquido prepettorale . 
 le aree di aumentata impregnazione sono state classificate come tipo massa e tipo non - massa ; i reperti tipo massa sono stati analizzati secondo gli aspetti morfologici e dinamici descritti dai parametri di fischer [ 9 ] ; i reperti tipo non - massa sono stati interpretati secondo il lessico birads per quanto riguarda gli aspetti morfologici [ 13 ] e secondo i parametri di fischer per quanto riguarda gli aspetti dinamici [ 9 ]  . 
 le impregnazioni tipo massa sono state analizzate considerando : forma della lesione ( rotondeggiante ; ovalare ; spiculata ; irregolare ) , margini ( ben definiti ; mal definiti ) e pattern di enhancement ( omogeneo ; disomogeneo ; con setti ; ad anello , ed eventuale riempimento tardivo della porzione pi centrale )  . 
le impregnazioni tipo non - massa sono state analizzate considerando : distribuzione ( area focale , lineare , duttale , regionale , multi - regionale , diffusa ) , caratteristiche interne ( omogeneo , disomogeneo , punteggiato , raggruppato a macchia , reticolare - dendritico ) , asimmetria . i parametri cinetici valutati sono stati lincremento dellintensit di segnale nei primi due minuti dopo la somministrazione di mezzo di contrasto e il suo decorso nei successivi minuti configurando tre possibili curve intensittempo : incremento progressivo e graduale , tipo i ; rapido wash - in e successivo plateau , tipo ii ; rapido washin e wash - out , tipo iii . analisi patologica la diagnosi di neoplasia mammaria stata posta mediante biopsia percutanea con prelievo microistologico ecoguidato in 7 casi ( ago da 14 g , dispositivi di prelievo automatici o semi - automatici ) e mediante prelievo citologico ecoguidato ( ago da 21 g ) in 7 casi . 
il rilievo di massiva infiltrazione neoplastica dei vasi linfatici subdermici stato rilevato nel prelievo microistologico nei 7 casi in cui stato eseguito e alla biopsia chirurgica nei rimanenti 7 casi . 
le pazienti con diagnosi microistologica di carcinoma infiammatorio sono state immediatamente avviate a chemioterapia neoadiuvante ; le rimanenti 7 pazienti con diagnosi patologica di carcinoma infiammatorio sono state avviate a chemioterapia dopo biopsia chirurgica . 
on the dynamic study , mass - like enhancement was seen in five cases ( 36% ) and non - mass - like enhancement in nine ( 64% ) ( table 1 )  . 
in these cases , the histological diagnosis was infiltrating carcinoma not otherwise specified ( nas ) in five ( 36% ) , ductal carcinoma in situ in one ( 7% ) and lobular carcinoma in situ ( 7% ) in the remaining cases . 
 statistical concordance the degree of interobserver concordance was excellent as regards shape ( k = 0.82 ) and enhancement pattern ( k = 0.86 ) , la diagnosi patologica stata formulata da due anatomopatologici con pi di 10 anni di esperienza in patologia mammaria . 
i fattori istologici valutati sui frustoli dei prelievi microistologici e sulle sezioni dei pezzi operatori sono stati : istotipo tumorale definito secondo la classificazione who , grado tumorale ( g1 , g2 , g3 ) secondo elstonellis easton system [ 14 ] e infiltrazione dei linfonodi ascellari ( negativi / positivi )  . analisi statistica la variabilit interosservatore nel determinare tipo di impregnazione , parametri morfologici e dinamici ( quali forma , margini , pattern di enhancement e distribuzione ) nellambito dellanalisi delle immagini stata valutato con k statistico . 
la forza di concordanza stato valutato come segue : valori inferiori o pari a 0 , 20 indicativo di debole accordo ; 0 , 210 , 40 , accordo equo ; 0 , 410 , 60 , abbastanza accordo ; 0 , 610 , 80 , buon accordo , e 0 , 811 , 0 , ottimo accordo . 
allo studio dinamico , impregnazione parenchimale tipo massa si evidenziata in 5 casi ( 36% ) , e tipo non massa in 9 ( 64% ) ( tabella 1 )  . 
patients radiol med ( 2010 ) 115 : 7082 finding increased breast volume nipple retraction skin thickening oedema architectural distortion axillary adenopathy internal mammary adenopathy prepectoral fluid mass - like enhancement ring enhancement heterogeneous non - mass - like enhancement regional multiregional diffuse curves type i type ii type iii skin enhancement pectoral enhancement hypertrophic internal mammary artery aumento del volume mammario retrazione del capezzolo ispessimento cutaneo edema cutaneo distorsione architetturale adenomegalia ascellare adenomegalia mammaria interna film liquido pre - pettorale enhancement tipo massa ad anello disomogeneo enhancement tipo non massa regionale multiregionale diffuso curva tipo 1 tipo 2 tipo 3 impregnazione cutanea impregnazione del pettorale ipertrofia dellarteria mammaria interna 14.86 14 , 86 tabella 1 rilievi rm della mastite carcinomatosa in 14 pazienti rilievi numero delle pazienti percentuale radiol med ( 2010 ) 115 : 7082 fig . 
distortion is better depicted by the axial short - tau inversion recovery sequence ( arrowhead in b ) , which also shows diffuse periareolar hyperintensity due to oedema ( arrow in b )  . 
il sovvertimento architetturale meglio evidente nellacquisizione trasversale stir ( testa di freccia in b ) ove si rileva anche il diffuso aumento dellintensit di segnale della cute periareolare da imbibizione edematosa ( freccia in b )  . 
clinically , it presents with the typical signs of acute inflammation that progress rapidly within weeks or months . in 50% of cases , a palpable mass is detected [ 1 ]  . the diagnosis of ibc relies on the finding of neoplastic invasion of the dermal lymphatic vessels , which is more commonly related to a poorly differentiated ductal infiltrating carcinoma , although any histological type of breast carcinoma may be associated with ibc . 
in the present series , the diagnosis of neoplastic invasion of the lymphatic vessels was made in 7 / 14 ( 50% ) cases on microhistological samples and in the remaining 7 / 14 ( 50% ) cases on surgical biopsies . 
among the seven cases of ibc diagnosed on microhistological material , the underlying breast cancer was il rilievo di infiltrazione dei vasi linfatici subdermici stato rilevato nel prelievo microisto logico in 7 casi ; la diagnosi microistologica in questi casi stata di carcinoma infiltrante nas in 5 casi ( 36% ) , carcinoma duttale in situ in 1 caso ( 7% ) e neoplasia lobulare in situ ( 7% ) nel rimanente caso . 
il rilievo di infiltrazione dei vasi linfatici subdermici stato rilevato alla biopsia chirurgica negli altri 7 casi ; la diagnosi patologica in questi casi stata di carcinoma infiltrante non altrimenti specificato ( nas ) in 6 casi ( 43% ) , di carcinoma metaplastico in 1 caso ( 7% )  . 
 concordanza statistica la forza di concordanza di giudizio fra i due radiologi risultata ottima per forma ( k = 0 , 82 ) e pattern di enhancement ( k = 0 , 86 ) , buona per margini ( k = 0 , 78 ) , moderata per la valutazione della distribuzione ( k = 0 , 46 )  . radiol med ( 2010 ) 115 : 7082 fig . 
2a - d axial short - tau inversion recovery t2 - weighted sequence ( a ) : diffusely increased signal intensity in the left breast caused by cutaneous and parenchymal oedema ( large arrow in a ) and a prepectoral focal linear hyperintensity due to prepectoral fluid ( small arrow in a )  . 
maximum intensity projection reconstruction ( b ) shows a diffuse non - mass - like enhancement of the dendritic type extending to the entire left breast with a large supplying vessel ( arrow in b )  . 
2a - d nella sequenza stir nel piano trasversale ( a ) , si evidenzia un diffuso aumento del segnale del corpo mammario sinistro rispetto al controlaterale , della cute e dei tessuti sottocutanei per imbibizione edematosa ( freccia grande in a ) e un focale e lineare aumento del segnale in sede pre - pettorale riferibile a sottile falda liquida ( freccia piccola in a )  . 
dopo mezzo di contrasto , nella ricostruzione mip ( b ) , si apprezza diffusa impregnazione di tipo non - massa , con aspetto dendritico , che interessa la quasi totalit del corpo ghiandolare sinistro con robusto vaso afferente ( freccia in b )  . 
la curva di impregnazione intensit / tempo , misurata in pi punti ( c ) , mostra un rapido incremento seguito veloce wash - out ( curva di tipo 3 , d )  . ductal carcinoma in situ in one case and lobular carcinoma in situ in another case . 
 [ 2 ] , in a certain number of cases , despite a finding of dermal lymphatic invasion , it may be impossible to identify the exact point where the process became invasive and crossed the basal membrane . 
this occurs more frequently when the histological material is scarce , as in microbiopsies . conventional breast imaging has proved to be limited for the diagnosis of ibc owing to difficulties in identifying specific signs of malignancy in dense and swollen breasts [ 2 ]  . 
on mammography and ultrasound , space - occupying lesions and microcalcifications are rare manifestations of this disease , and the only findings suggestive of an underlying carcinoma are isolated inflammatory findings ( skin thickening , diffuse increase in density , trabecular thickening , axillary lymphadenopathy ) and a lack of response to discussione il carcinoma infiammatorio della mammella un raro tipo di tumore della mammella ( 1%6% di tutti i tumori mammari ) altamente aggressivo e con prognosi sfavorevole rappresentante il 24%40% dei tumori mammari localmente avanzati . 
clinicamente si presenta con i tipici segni infiammatori acuti che progrediscono rapidamente in qualche settimana o pochi mesi ; nel 50% dei casi concomitante il reperto di massa palpabile [ 1 ]  . la diagnosi di carcinoma infiammatorio richiede il rilievo di invasione neoplastica dei linfatici dermici pi frequentemente sostenuta da un carcinoma duttale infiltrante scarsamente differenziato , anche se un qualsiasi tipo istologico di tumore mammario pu associarsi a ibc . 
3a - d sequenza stir trasversale ( a ) : la mammella destra mostra diffuso aumento dellintensit di segnale coinvolgente posteriormente anche il muscolo pettorale ( freccia in a ) ; il fascio muscolare ispessito e disomogeneo anche nelle scansioni sagittali ( freccia in b )  . 
come reperto accessorio , multiple lesioni nodulari , ipercaptanti dopo mdc , a livello del corpo sternale ( testa di freccia in d )  . antibiotic treatment [ 4 , 1517 ]  . 
 mr imaging has taken on an increasingly important role in the management of breast cancer , and its indications now include initial diagnosis , staging of known cancer , monitoring the effects of neoadjuvant chemotherapy and the diagnosis of disease recurrence . 
in ibc it is used to determine the size of the tumour prior to chemotherapy , to exclude pectoral muscle involvement and to monitor response to treatment [ 2 , 17 ]  . 
recently , researchers have also investigated the value of vascular maps of the breasts , demonstrating increased vascularity of the breast ipsilateral to the tumour [ 1820 ]  . in our series , the most frequent mr signs of ibc were skin thickening and oedema , architectural distortion , extensive non - mass - like enhancement with wash - out timeintensity curve and axillary lymphadenopathy . 
the finding of architectural distortion is less frequent in series studied with mr imaging compared with mammography and ultrasound , where it is seen in 85% 95% of cases [ 2 , 4 ]  . axillary lymphadenopathy was present in 86% of cases , linfatici stata formulata in 7 / 14 ( 50% ) casi su materiale microistologico e nei rimanenti 7 / 14 ( 50% ) casi su biopsia chirurgica . 
tra i 7 casi con diagnosi di carcinoma infiammatorio su materiale microistologico , la sottostante eteroplasia mammaria risultata essere carcinoma duttale in situ in 1 caso e neoplasia lobulare in situ in un altro caso . come riportato nella casistica radiologica di yang et al . [ 2 ] in un certo numero di casi possibile che nonostante il reperto di invasione linfatica dermica , non si riesca ad evidenziare il punto in cui il processo diventato invasivo ed ha superato la membrana basale . 
questo accade pi frequentemente quando il materiale ridotto come nel caso delle microbiopsie . limaging senologico convenzionale si dimostrato limitato nella diagnosi del carcinoma infiammatorio per la difficolt ad individuare reperti semeiologici specifici di malignit in mammelle dense e tumefatte [ 2 ]  . 
allindagine mammografcia ed ecografica , lesioni espansive e microcalcificazioni sono rare manifestazioni di questa patologia e gli unici aspetti suggestivi di un sottostante carcinoma sono rappresentati dalla presenza di isolati reperti infiammatori ( ispessimento cutaneo , diffuso incremento della densit , ispessimento della trabecolatura stromale , linfoadenopatia ascellare ) e dalla mancata risposta alla terapia antibiotica [ 4 , 1517 ]  . 
 lindagine rm ha assunto un ruolo sempre pi importante nel management dei tumori della mammella , trovando indicazioni per la diagnosi iniziale , per la stadiazione di una radiol med ( 2010 ) 115 : 7082 table 2 pathological characteristics of inflammatory breast cancer in 14 patients finding no . 
patients % patients pathological diagnosis infiltrating ductal carcinoma metaplastic carcinoma ductal carcinoma in situ lobular carcinoma in situ lymph node metastasis positive negative grading isotipo carcinoma duttale infiltrante carcinoma metaplastico carcinoma duttale in situ carcinoma lobulare in situ stato linfonodale positivi negativi grado di differenziazione tabella 2 rilievi anatomo - patologici della mastite carcinomatosa in 14 pazienti rilievi numero di pazienti pazienti ( % ) a percentage similar to that reported by yang et al . 
nodal metastases were in 83% ( 10 / 12 cases ) of confirmed by histology lymphadenopathy suspected on mr imaging , a percentage higher than that reported by yang et al . 
our series was therefore characterised by locally , very advanced disease , as also confirmed by the type of enhancement , which was non - mass - like in the majority of cases ( 64% )  . 
 [ 2 ] , where 70% of ibc cases showed mass - like enhancement with multiple nodules and heterogeneous pattern , whereas it is similar to that reported by chow et al . 
nel carcinoma infiammatorio viene utilizzata per la documentazione delle dimensioni tumorali prima dellinizio del trattamento chemioterapico , per escludere linteressamento del muscolo pettorale e per il monitoraggio della risposta terapeutica [ 2 , 17 ]  . 
in sede tumorale , a causa degli attivi processi angiogenetici neoplastici si apprezza un accumulo di mezzo di contrasto le cui caratteristiche cinetiche rispecchiano gli aspetti fisiopatologici della crescita tumorale . 
di recente , stato indagato anche il valore delle mappe vascolari dellintero organo ed stato dimostrato un incremento della vascolarizzazione mammaria omolaterale alla sede tumorale [ 1820 ]  . nella serie personale , i segni rm pi frequenti di carcinoma infiammatorio sono ispessimento ed edema cutaneo , distorsione architetturale , impregnazione estesa tipo non massa con andamento della curva intensit - tempo a washout e linfoadenopatia ascellare . 
nelle casistiche analizzate con indagine rm il rilievo di distorsione architetturale meno frequente rispetto a quelle esaminate con mammografia ed ecografia dove si appalesa nel 85%95% dei casi [ 2 , 4 ]  . adenomegalia ascellare si apprezza nel 86% dei casi ; tale dato concorde con quello del 88% riportato nel recente lavoro di yang et al . 
metastasi linfonodali sono state istologicamente confermate nel 83% ( 10 / 12 casi ) delle adenopatie sospette alla rm ; la percentuale maggiore rispetto a quella del 44% riportata da yang et al . 
si tratta pertanto di una casistica di patologia localmente molto estesa come confermato anche dal tipo di impregnazione che nella maggioranza dei casi , il 64% , risultato essere di tipo nonmassa . 
 dalla disamina della letteratura emerge che non esiste un pattern interno di impregnazione patognomonico di carcinoma infiammatorio ; in genere vi cospicuo interessamento della ghiandola mammaria , con impregnazione regionale o a noduli multipli . 
the finding of hypertrophy of the internal mammary artery is fairly common : it is seen in 21% of all cases and in 27% of inflammatory carcinomas with invasive histological type . internal mammary artery hypertrophy is always associated with a pattern of intense diffuse enhancement related to a large invasive tumour . 
this observation is consistent with a previous report [ 20 ] according to which increased breast vascularity is dependent on the size of the tumour and is more pronounced in invasive disease . with regard to the remaining mr imaging findings , nipple retraction and internal mammary lymphadenopathy were less frequent . 
nipple retraction was seen in 14% of cases , and in the literature , it is reported to occur in percentages varying from 16% to 100% [ 2 , 4 , 21 , 22 ]  . 
although volume increase , together with rubor , calor , dolor ( redness , warmth , pain ) , is one of the pathognomonic signs of acute inflammation , it is a uncommon finding in ibc , and in atypical presentations , there is a narrowing of the breast with simultaneous nipple retraction . 
focal skin enhancement not directly in continuity with the tumour mass has been described as a usual finding ( up to 94% of cases in yang et al . ) [ 2 ] , but this was not the case in our series where it was present in 14% of cases only . there are some limitations to our study . 
secondly , performance of the mr study without assessing hormonal status in the nine premenopausal women in our series may have limited enhancement assessment ; however , the fact that enhancement was observed unilaterally allowed us to exclude a functional cause . 
tale osservazione in accordo con quella espressa in letteratura [ 20 ] secondo cui laumento della vascolarizzazione mammaria dipendente dalle dimensioni tumorali e pi evidente nel caso di patologia invasiva . per quanto riguarda i rimanenti rilievi rm , retrazione del capezzolo e adenomegalia mammaria interna risultano meno frequenti . 
la retrazione del capezzolo documentabile nel 14% dei casi e in letteratura ricorre con percentuali variabili dal 16% al 100% [ 2 , 4 , 21 , 22 ]  . 
la mammella interessata dal processo neoplastico appare aumentata di volume nel 14% dei casi ; sebbene lincremento volumetrico rappresenti assieme a rubor , calor , dolor un dei segni patognomonici di flogosi acuta , il suo riscontro poco frequente e nella presentazione atipica del carcinoma infiammatorio si assiste alla coartazione della mammella con contemporanea retrazione del capezzolo . 
lesecuzione dellindagine rm senza valutazione della fase ormonale nelle 9 donne di questa serie in et fertile potrebbe essere un limite per la valutazione dellimpregnazione ; tuttavia , la monolateralit dellenhancement osservato consente di escludere lorigine funzionale dellimpregnazione . 
inoltre , la complessit del lessico bi - rads - mri richiede un adeguato addestramento per la corretta interpretazione e per il confronto con le altre esperienze . conclusions conclusioni radiol med ( 2010 ) 115 : 7082 mr signs predictive of ibc are skin thickening and oedema , architectural distortion , extensive non - mass - like enhancement with type - iii time - intensity curve and axillary lymphadenopathy ; less frequent findings are nipple retracinternal mammary tion , mass - like enhancement and lymphadenopathy . 
the presence of fluid coating the pectoral muscle is common but does not imply muscle invasion . mr imaging identifies the presence of a spaceoccupying lesion with irregular margins or diffuse , heterogeneous , unilateral enhancement of the reticular - dendritic type . 
this enhancement pattern associated with skin thickening and skin enhancement is highly suggestive for ibc . i segni rm predittivi di carcinoma infiammatorio sono ispessimento ed edema cutaneo , distorsione architetturale , estesa impregnazione tipo non - massa con curva intensit - tempo tipo iii e linfoadenopatia ascellare ; meno frequenti risultano retrazione del capezzolo , impregnazione tipo massa e adenomegalia mammaria interna . 
la presenza di liquido che lambisce il pettorale frequente e non ne comporta infiltrazione . lindagine rm individua la presenza di una lesione espansiva con margini irregolari o un aumento unilaterale dellimpregnazione , disomogeneo e diffuso , di tipo reticolare - dendritico . 
dose surplus due to slope - up and slope - down of prospective tube current modulation in a phantom model riduzione della dose in angiografia coronarica con tc spirale con apparecchiatura a doppia sorgente . 
cademartiri1 , 2 1dipartimento di radiologia e cardiologia , azienda ospedaliero - universitaria , parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands correspondence to : f . 
cademartiri , dipartimento di radiologia e diagnostica per immagine , c / o piastra tecnica , piano 0 , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy , tel . : + 39 - 052 - 1703756 , fax : + 39 - 052 - 1704838 , e - mail : filippocademartiri@hotmail.com received : 13 november 2008 / accepted : 7 january 2009 / published online : 7 january 2010 springer - verlag 2010 abstract purpose . 
we used four tube current modulation algorithms : narrow pulsing window , with tube current reduction to 20% ( a ) and 4% ( b ) of peak current ; and wide pulsing window , with tube current reduction to 20% ( c ) and 4% ( d )  . 
noise was measured at each r - r step in order to identify low noise ( 100% dose ) , medium noise ( slopeup / down ) and high noise ( 4 / 20% dose )  . 
sono stati valutati 4 protocolli ecggated retrospettivo dsct - ca , acquisiti con electrocardiographic ( ecg ) - controlled tube current modulation ed ecg - pulsing heart rate - adattativo : nei due diversi protocolli , a e b , la corrente stata ridotta al 20% del massimo amperaggio al di fuori di una finestra di pulsing stretta ( a ) ed ampia ( b ) ; nei protocolli c e d , la corrente stata ridotta al 4% del massimo amperaggio al di fuori di una finestra di pulsing stretta ( c ) e ampia ( d )  . sono state calcolate le finestre di modulazione della corrente : 100% ma ( finestra di acquisizione dati ) , 4% / 20% ma ( finestra di riduzione della corrente ) , dal 4% / 20% al 100% ma , e viceversa ( slope - up / down ; finestre di transizione della corrente )  . 
for c and d , instead , the slope - up increased with progressively higher hr ( 10%25% of the r - r interval , except for 90 bpm , 10% ) , whereas the slope - down remained constant at 5% ( except for 120 bpm ; 10% )  . 
la transizione della corrente relativa alla modulazione della corrente del tubo rappresenta una costante sorgente di dose surplus nellordine del 14%34% della dose totale , con valori maggiori nei protocolli acquisiti con finestra di pulsazione stretta e modulazione al 4% del massimo amperaggio . 
 parole chiave angiografica coronarica tomografia computerizzata a doppia sorgente ( dsct ) ecg - pulsing ecg - controlled tube current modulation dose di radiazione introduction introduzione multidetector - row computed tomography ( mdct ) has become an important noninvasive diagnostic tool for coronary artery and heart disease thanks to the high diagnostic accuracy of the technique [ 13 ]  . 
as a result , algorithms have been developed that are able to modulate the radiation exposure without significantly deteriorating image quality at mdct coronary angiography ( mdctca ) [ 710 ]  . 
 a recent appearance on the market is dual - source ct ( dsct ) , which offers high temporal resolution ( 83 ms ) regardless of heart rate ( hr ) and the possibility of simultaneous evaluation of left ventricular volumes [ 1013 ]  . 
 with dsct scanners , reduced radiation exposure is achieved with two ecg - triggered systems : the first ecg pulsing varies the width of the window of maximum milliampere , whereas the second ecg - controlled tube current modulation reduces the current outside the window . 
 the aim of this study was to evaluate the impact of surplus dose derived from the transition window in dsctca acquired with two different reductions in milliampere and two different pulsing windows at different hr . la tomografia computerizzata multistrato ( msct ) diventata un importante strumento diagnostico non invasivo in corso di patologia coronarica e cardiaca [ 13 ]  . 
tuttavia , lo sviluppo di apparecchiature sempre pi performanti ( ad esempio , 64 - msct ) , comporta di regola un incremento della dose di esposizione alle radiazioni ionizzanti [ 46 ]  . questo dato rappresenta una potenziale limitazione allimpiego clinico . 
sono stati pertanto sviluppati degli algoritmi capaci di modulare lesposizione alle radiazioni senza deteriorare significativamente la qualit dellimmagine mediante angiografia coronarica msct ( msct - ca ) [ 710 ]  . la tomografia computerizzata a doppia sorgente ( dsct ) di recente implementazione permette di ottenere una risoluzione temporale costante di 83 ms indipendente dalla frequenza cardiaca e la possibilit di eseguire una simultanea valutazione dei volumi del ventricolo sinistro [ 1013 ]  . nella angiografia coronarica dsct ( dsct - ca ) , la dose desposizione modulata mediante la combinazione di due sistemi cardio - sincronizzati dellemissione del tubo radiogeno : ( ecg ) - pulsing , permette di variare la larghezza della finestra di applicazione di massimo amperaggio ; il secondo , ecg - controlled tube current modulation , permette di ridurre la corrente al di fuori della medesima finestra . 
un ulteriore e significativa riduzione di dose ottenuta dalladattamento automatico del pitch allaumentare della frequenza cardiaca [ 1320 ]  . il primo , electrocardiographic lo scopo di questo studio di valutare limpatto di dose materials and methods for this study performed on a phantom , we used a firstgeneration dsct system ( siemens medical solutions , forchheim , germany )  . dsct technology the dsct system we evaluated was equipped with two xray tubes and two detectors mounted on a rotating gantry with an angular offset of 90 . 
with both tubes operating , they provide a power of 80 kw / tube ( straton , siemens medical solution ) , whereas if only tube a is in operation , the system is comparable with a single - source 64 - slice mdct systeconventional ct dose indices can also be applied to dsct , because the doses regarding each tube are combined using a linear function . 
in fact , tube current value is calculated as the current - time product per gantry rotation ( milliampere / rotation ) with the sum of the milliampere of both x - ray tubes . 
with the use of ecg - controlled tubecurrent modulation , radiation exposure is proportional to the mean value of the current applied during the entire scan [ 1320 ]  . exposure reduction systems heart - rate - adaptive pitch the pitch increases proportionally with increasing hr . 
the pitch is determined by the lowest hr observed during prescanning monitoring . cardiac bow - tie filter radiol med ( 2010 ) 115 : 3650 relativa alla transizione della corrente in dsct - ca , acquisita con due diverse riduzioni di amperaggio e due diverse finestre di pulsing , per diversi valori di frequenza cardiaca . 
 materiali e metodi per questo studio su fantoccio stato utilizzato il sistema dsct ( siemens medical solutions , forchheim , germania ) di prima generazione . tecnologia dsct il sistema dsct valutato dotato di due tubi radiogeni e due detettori montati sulla pista di rotazione del gantry ad una compensazione angolare di 90 . 
i due tubi contemporaneamente energizzati forniscono una potenza di 80 kw / tubo ( straton , siemens medical solution ) , mentre se in funzione solo il tubo a , la performance del sistema paragonabile a quella di una 64 - msct a singola sorgente . 
infatti , il valore della corrente del tubo viene calcolato come il prodotto della corrente al secondo per il tempo di rotazione del gantry ( mas / rot ) sommando i milliamperes di entrambi i tubi quando contemporaneamente attivi . 
con lutilizzo dellalgoritmo ecg - controlled tube current modulation , la dose di radiazione proporzionale al valore medio della corrente applicata durante lintera scansione [ 1320 ]  . sistemi di risparmio della dose utilizzati pitch heart rate - adattativo il pitch aumenta parallelamente allaumento della frequenza cardiaca . 
 in cardiac imaging , the collimation system is constituted by an additional filter defined as cardiac , because it limits the field of view ( fov ) to the cardiac region . cardiac bow - tie filter ecg synchronisation ecg pulsing was introduced in mdct - ca to reduce radiation exposure by around 50% [ 1416 ]  . 
the width of the image acquisition window ( pulsing window = window with maximum tube current intensity , or 100% of milliampere ) can be manually selected before the scan on the basis of the in cardio - imaging , il sistema di collimazione costituito da un filtro addizionale definto cardiac , poich limita il campo visivo ( fov ) alla regione cardiaca . 
 modulazione cardio - sincronizzata della corrente del tubo la modulazione cardio - sincronizzata dellemissione del tubo radiogeno , o ecg - pulsing , stata introdotta in msctradiol med ( 2010 ) 115 : 3650 cardiac cycle phase where cardiac motion is at a minimum . ecg - controlled tube - current modulation can reduce the current to 20% ( analysis of left ventricular function , or functional imaging ) or to 4% ( mindose ) of the nominal value outside the pulsing window , thus at the same time reducing total radiation exposure . 
transition times from minimum to maximum milliampere ( slopeup ) and vice versa ( slope - down ) are determined by the generator power ( thermionic effect ) and by the cathode cooling system , as well as r - r interval duration . 
the aim of this study was to evaluate the component of radiation exposure derived from current transition times , surplus dose / total dose and with and without a morphofunctional evaluation of the left ventricle , with different acquisition windows and different hr . dsct and ecg - pulsing scan protocols the study was performed on an anthropomorphic cardiac ct phantom ( cardio ; qrm , mhrendorf , germany )  . 
the ecg signal was provided by an ecg simulator incorporated in the syste the common scan parameters were two x - ray tubes , 380 mas / rot with 120 kv , collimation slice 640.6 mm ( z - axis flying - focal spot ) , and gantry rotation time 330 ms . 
the pitch varied between 0.2 ( low hr ; 45 bpm ) and 0.5 ( high hr ; 120 bpm ) and was automatically adapted by the scanner to the hr used : 45 , 60 , 75 , 90 and 120 bpthe craniocaudal range of the scan was 90 mm . table 1 shows the dose modulation algorithms used . 
we performed two functional imaging protocols ( reduction to 20% of maximum milliampere outside the pulsing window ; protocols a and b ) and two mindose protocols ( reduction to 4% of maximum milliampere outside the pulsing window ; protocols c and d )  . 
la larghezza della finestra di acquisizione delle immagini ( finestra di pulsing , o pulsing window , finestra di erogazione alla massima intensit di corrente del tubo , o 100% dellamperaggio ) pu essere selezionata manualmente , prima della scansione , in corrispondenza della miglior fase dimmobilit del cuore . 
lalgoritmo ecg - controlled tube current modulation permette di ridurre la corrente al 20% ( analisi della funzionalit ventricolare , o functional imaging ) o al 4% ( mindose ) del valore nominale , al di fuori della finestra di pulsing , riducendo parallelamente lesposizione totale alle radiazioni . 
la qualit delle immagini acquisite in functional imaging permette un simultaneo studio morfo - funzione del ventricolo sinistro , mentre la modulazione al 4% permette la minima esposizione alle radiazioni [ 1320 ]  . 
i tempi di transito dal minimo al massimo valore di ma ( slope - up ) , e viceversa ( slope - down ) , sono determinati dalla potenza del generatore ( effetto termoionico ) e dal sistema di raffreddamento del catodo , nonch dalla durata dellintervallo r - r . 
lo scopo di questo studio di valutare la componente di dose relativa ai tempi di transizione della corrente , dose surplus / dose totale , con e senza valutazione morfo - funzionale del ventricolo sinistro , per diverse finestra di acquisizione e diversi valori di frequenza cardiaca . 
 protocolli di scansione dsct ed ecg - pulsing lo studio stato eseguito su un fantoccio da tomografia computerizzata ( ct ) cardiaco antropomorfico ( cardio , qrm , mhrendorf , germania )  . 
i parametri di scansione comuni sono : due sorgenti a raggi x ; 380 mas / rot ad una tensione del tubo di 120 kv , collimazione - slice 640 , 6 mm ( z - axis flying focal spot ) ; tempo di rotazione del gantry 330 ms . 
il pitch variava tra 0 , 2 ( basse frequenze ; 45 bpm ) e 0 , 5 ( alte frequenze ; 120 bpm ) , adattato automaticamente dalla macchina alle frequenze cardiache utilizzate : 45 , 60 , 75 , 90 e 120 bp il range cranio - caudale di scansione era 90 m la tabella 1 riporta gli algoritmi di modulazione della dose utilizzati . 
using the coefficient of conversion for the chest , we calculated the effective dose ( dpl0.017 , mgycmcoefficient of conversion for the chest ) ( table 2 )  . evaluation of the transition window surplus dose for each hr , we reconstructed four series of data , from 0% to 95% of the r - r interval with 5% increments , for a total of 20 data sets . 
we calculated current modulation time windows ( ms ) : data acquisition window ( 100% ma = max dose ) , current reduction window ( 4%20% ma = mindose ) , current transition windows ( slope - up and slope - down , from 4 / 20% to 100% of ma and vice versa )  . 
noise was evaluated as the sd measured within a region of interest ( roi ) , positioned at the centre of the phantom and classified as low ( 100% ma = max dose ) , medium ( slope - up / slope - down ) and cardiache ( 45 , 60 , 75 bpm ) e in telesistole ad alte frequenze cardiache ( 90 , 120 bpm )  . 
sono stati valutati il ct dose index volume ( ctdivol ) espresso in mgy , dove [ j ] [ kg - 1 ] = [ gy ] , ed il doselenght product ( dlp ) espresso in mgy / cm , quali parametri di dose assorbita durante lacquisizione delle immagini gated - retrospettive . 
utilizzando il coefficiente di conversione per il torace , stata calcolata la dose efficace ( dlp0 , 017 , mgycmcoefficiente di conversione per il torace ) ( tabella 2 )  . valutazione dose surplus relativa alla transizione della corrente per ogni valore di frequenza cardiaca sono state ricostruite 4 serie di dati , da 0% al 95% dellintervallo r - r con passo del 5% , per un totale di 20 data set . 
correlations were evaluated with tpearsons r coefficient . statistics results radiol med ( 2010 ) 115 : 3650 di riduzione della corrente ( 4%20% ma = dose minima [ min dose ] ) , finestre di transizione della corrente ( slope - up e slope - down : dal 4% / 20% al 100% di ma e viceversa )  . 
il confronto tra i valori di dose surplus e dose totale stato effettuato mediante test t di student per dati appaiati , ed una p < 0 , 05 stata considerata significativa . 
the width of the slopeup / slope - down windows is dependent on the duration of the r - r interval ( hr ) , the width of the pulsing window and the tube current modulation ( functional imaging or mindose )  . risultati evaluation of total dose table 2 shows the calculated ctdivol and dlp dose indices . 
la larghezza delle finestre di slopeup / slope - down in relazione alla durata dellintervallo r - r ( fc ) , alla larghezza della finestra di pulsazione e alla modulazione della corrente del tubo ( functional imaging o mindose )  . valutazione dose totale la tabella 2 mostra gli indici di dose ctdivol e dlp calcolati . 
in base agli studi iniziali eseguiti su apparecchiature dsct [ 2123 ] , lottimale finestra di pulsing ( vale a dire narrow pulsing window ) a bassa ed alta frequenza cardiaca permette di ridurre la dose del 29%42% ( < 65 bpm ) e del 15%34% ( 80 bpm ) , con e senza valutazione dei volumi e della massa del ventricolo sinistro , rispettivamente . 
invece , a frequenze cardiache intermedie , lottimizzazione del data set dimmagine ( mediante wide pulsing window ) corrisponde ad un aumento di dose del 23%32% . radiol med ( 2010 ) 115 : 3650 radiol med ( 2010 ) 115 : 3650 radiol med ( 2010 ) 115 : 3650 a slope up a slope down b slope up b slope down fig . 
r - r , intervallo r - r ; bpm , battiti per minuto ; slope - up , finestra di transizione della corrente dal minimo al massimo valore di ma ; slope - down , finestra di transizione della corrente dal massimo al minimo valore di ma ; fi , functional imaging ; a , narrow pulsing window functional imaging ; b , wide pulsing window functional imaging . c slope up c slope down d slope up d slope down fig . 
r - r , intervallo r - r ; bpm , battiti / minuto ; slope - up , finestra di transizione della corrente dal minimo al massimo valore di ma ; slope - down , finestra di transizione della corrente dal massimo al minimo valore di ma ; md , mindose ; c , narrow pulsing window mindose ; d , wide pulsing window mindose . evaluation of total dose valutazione della dose surplus table 3 shows the slope - up / slope - down times expressed in relative ( ms ) and absolute ( % ) terms of the r - r interval for hr of 45 , 60 , 75 , 90 and 120 bpm . dependence on duration of current modulation la tabella 3 mostra la durata dei tempi di slope - up e slopedown , espressi in valore relativo ( ms ) e assoluto ( % ) dellintervallo r - r , per le frequenze cardiache di 45 , 60 , 75 , 90 e 120 bp complessivamente , la dose surplus aumenta parallelamente allaumentare della frequenza cardiaca in base alla dose totale di esposizione . in the functional imaging protocols ( a and b ) , the transition current ( slope - up / slope - down ) had the same relative value : 10% + 10% for hr 75 bpm and 15% + 15% for hr dipendenza dalla durata della modulazione della corrente nei protocolli functional imaging ( a e b ) , la transizione della radiol med ( 2010 ) 115 : 3650 surplus dose / total dose fig . 
bpm , battiti per minuto ; a , narrow pulsing window functional imaging ; b , wide pulsing window functional imaging ; c , narrow pulsing window mindose ; d , wide pulsing window mindose . 
at higher hr ( 120 bpm ) , the slope - up / slopedown showed a different value of 25% + 15% , respectively , in relation to the shorter duration of the cardiac cycle ( 500 ms ) vs . 
 discussion dsct devices are equipped with tube current modulation tube current systems ( ecg pulsing / ecg - controlled discussione le apparecchiature dsct sono dotate di sistemi cardiosincronizzati di modulazione della corrente del tubo ( ecgpulsing / ecg - controlled tube current modulation ) [ 13 , 1720 ] heart rate - adattativi atti a ridurre al minimo radiol med ( 2010 ) 115 : 3650 modulation ) [ 1317 , 2123 ] , which are hr adaptive to minimise radiation exposure during noninvasive cardiac imaging . 
however , in pulsing acquisitions , the current transition from minimum to maximum milliampere ( slope - up ) and vice versa ( slope - down ) was not instantaneous [ 13 ]  . 
the current slope produced an additional dose of radiation ( surplus dose ) , which could be reduced by increasing the capacity of the gantrys internal circuits ( i.e. cooling system and generatorcathode circuit )  . 
to evaluate the efficiency of the ecg - controlled tube current modulation system , we acquired two different pulsing windows narrow and wide at two different current modulations ( 20% of max ma functional imaging ; 4% of max ma mindose )  . dependence on current modulation the surplus dose increased alongside increasing hr , from 45 bpm to 120 bpm , in terms of total dose . 
the surplus dose , in contrast , increased with increasing hr , from 45 to 120 bpin protocols of tube current modulation to 20% of milliampere ( a and b ) , the transition current ( slopeup / slope - down ) produced a reduction in surplus dose up to hr 75 bpm and then increased at higher hr ( i.e. 25% / 15% , 120 bpm ; b )  . 
tuttavia nelle acquisizioni pulsate , la transizione della corrente dal minimo al massimo valore di ma ( slopeup ) , e viceversa ( slope - down ) , non istantanea [ 13 ]  . 
la pendenza della corrente sottende una dose di radiazione aggiuntiva ( dose surplus ) che potrebbe essere ridotta potenziando le capacit dei circuiti interni al gantry ( vale a dire , il sistema di raffreddamento e il circuito generatorecatodo )  . 
 per valutare lefficienza del sistema ecgcontrolled tube current modulation , sono state acquisite due diverse finestre di pulsazione , narrow e wide pulsing window , a due diverse modulazioni di corrente ( 20% di max ma per il functional imaging ; 4% di max ma per il mindose )  . dipendenza dalla modulazione della corrente la dose surplus aumenta parallelamente allaumento della frequenza cardiaca , da 45 a 120 bpm , rispetto alla dose totale . 
in particolare , nei protocolli modulati al 20% al di fuori della finestra di pulsing ( a e c ) , la transizione della corrente ( slope - up / slope - down ) ha lo stesso valore relativo ( 10% + 10% ) per fc90 bpm ( a / c ) , per poi aumentare alle frequenze cardiache pi elevate ( vale a dire , 25% + 15% , 120 bpm ; b )  . 
nei protocolli di modulazione della corrente al 4% di ma al di fuori della finestra di pulsing ( b e d ) , il tempo di slope - up aumenta parallelamente allaumentare della frequenza cardiaca ( 10%25% da 45120 bpm ) , eccetto a 90 bpm ( pitch = 0 , 43 vs 0 , 40 ) ; mentre la caduta di erogazione raggi ( slope - down ) ha una durata costante ( 5% ) , eccetto a 120 bpm . dipendenza dallintervallo r - r la dose totale diminuisce allaumentare della frequenza cardiaca ( 45120 bpm )  . 
la dose surplus , invece , aumenta parallelamente allaumento della frequenza cardiaca , da 45 a 120 bpnei protocolli di modulazione della corrente al 20% di ma ( a / c ) , la transizione della corrente ( slope - up / slope - down ) determina una riduzione di dose surplus fino a fc75 bpm , per poi aumentare alle frequenze cardiache pi elevate ( vale a dire 25% + 15% , 120 bpm ; b )  . 
nei protocolli di modulazione della corrente al 4% di ma ( b e d ) , laumento della pendenza della corrente ( 10%25% da 45120 bpm ) determina un significativo aumento di dose surplus da basse ad elevate frequenze cardiache ( 45120 bpm ) , eccetto a 90 bpm ( pitch = 0 , 43 vs 0 , 40 )  . 
this reduction is maximised in narrow pulsing window protocols , especially with mindose modulation . nonetheless , the use of dose optimisation algorithms entails a significant component of surplus dose ( nondiagnostic dose ) with increasing hr in terms of r - r interval duration and the information to be extrapolated . 
questa riduzione massima nei protocolli narrow pulsing window , in particolare con modulazione mindose . tuttavia , lutilizzo degli algoritmi di ottimizzazione della dose mostra una pesante componente di dose surplus ( dose non diagnostica ) , allaumento della frequenza cardiaca , in relazione alla durata dellintervallo r - r e alle informazioni da estrapolare . 
msv , dose efficace ; bpm , battiti per minuto ; slope - up , finestra di transizione della corrente dal minimo al massimo valore di ma ; slope - down , finestra di transizione della corrente dal massimo al minimo valore di ma ; dose surplus , dose sottesa dalla finestra di transizione della corrente del tubo , durante lalgoritmo di modulazione ; narrow fi , narrow pulsing window functional imaging , protocollo a ; wide fi , wide pulsing window functional imagin , protocollo b ; narrow md , narrow pulsing window mindose , protocollo c ; wide md , wide pulsing window mindose , protocollo d . dependence on modulation algorithm dipendenza dallalgoritmo di modulazione at low and high hr , the use of the narrow pulsing window protocol significantly reduced total radiation exposure , with and without evaluation of left ventricular volumes . at intermediate hr , the use of the optimal acquisition window ( wide ) produced an increase in radiation exposure both with functional imaging and mindose ( ~2 msv )  . 
in patients with suspected coronary artery disease , the radiation exposure derived from a dsct - ca acquisition without a morphofunctional study of a bassa ed elevata frequenza cardiaca , lutilizzo del protocollo narrow pulsing window permette di ridurre significativamente la dose totale di radiazione , con e senza valutazione dei volumi del ventricolo sinistro . 
a frequenze cardiache intermedie , lutilizzo dellottimale finestra di acquisizione ( ampia ) risulta in un aumento di dose sia in functional imaging che in mindose ( ~2 msv )  . 
 in base ai dati ottenuti e agli studi iniziali eseguiti su apparecchiature dsct di prima generazione , appare indispensabile lutilizzo dellottimale finestra ecg - pulsing per ridurre significativamente lesposizione complessiva alle radiazione nelle indagini dsct - ca . 
the results obtained suggest that : the hr - adaptive pitch reduces total radiation exposure with increasing hr against surplus dose ; at low and high hr , the use of the optimal pulsing window produces the highest values of radiation exposure during current transition ; modulation of tube current to 4% of maximum milliampere outside the acquisition window is advisable for evaluating the coronary arteries without a morphofunctional study of the left ventricle . 
in these cases , reduction in total dose proportional to increase in hr is characterised by a component of around 37% deriving from the transition current . currently , there are no studies that evaluate the capacity and efficiency of the generator and the cooling system of dsct devices . 
however , the impact of dose of the modulation systems described cannot be overlooked and deserves further study . dsct - ca senza studio morfo - funzionale del ventricolo sinistro ( mindose ) potrebbe essere ridotta di un fattore di 5 . 
dai risultati ottenuti possibile dedurre che : il pitch heart rate - adattativo determina una riduzione di dose totale desposizione allaumentare della frequenza cardiaca , rispetto alla dose surplus ; a basse ed alte frequenze cardiache , lutilizzo dellottimale finestra pulsata mostra i pi alti valori di dose erogata durante la transizione della corrente ; una modulazione della corrente del tubo al 4% del valore nominale di ma al di fuori della finestra di acquisizione dati raccomandabile per una valutazione delle arterie coronarie senza studio morfo - funzionale del ventricolo sinistro ; in questi casi , la riduzione di dose totale proporzionale allaumento della frequenza cardiaca , mostra una componente di circa il 37% di dose relativa la transizione della corrente . non esistono al momento studi che valutino la potenzialit e lefficienza del generatore e del sistema di raffreddamento dellapparecchiatura dsct . 
 limitations limitazioni evaluation of the impact of the surplus dose delivered during the dsct - ca study was based solely on calculations performed on a phantom and on the basis of algorithms developed for this study . 
all dose - reduction algorithms available with technique were not evaluated , such as the reduction and / or increase in x - ray tube voltage , use of double kilovoltage , b26 convolution kernel , the care dose 4d system and ecg editing . this la valutazione dellimpatto di dose aggiuntiva erogata durante indagine dsct - ca basata solo su calcoli eseguiti su fantoccio e in base agli algoritmi elaborati per questo studio . 
non sono stati valutati tutti gli algoritmi di risparmio della dose disponibili con questa metodica , quali : la riduzione e / o laumento del voltaggio del tubo radiogeno , lutilizzo del doppio voltaggio , il kernel di convoluzione b26 , il sistema care dose 4d ed ecg - editing . 
ragionevole stimare che unulteriore ottimizzazione della dose sarebbe stata ottenuta applicando il care dose 4d . conclusions conclusioni using the dose - reduction algorithms available on dsct systems can keep effective dose below 10 msv in most cases . 
current transition is a constant source of surplus dose in the order of 14%34% of total dose , with greater values in protocols acquired with the narrow pulsing window and mindose modulation ( foregoing the possibility of performing an evaluation of left ventricular volumes )  . 
surplus dose increases with increasing hr . gli algoritmi di riduzione della dose disponibili su apparecchiatura dsct consentono di mantenere la dose efficacie al di sotto dei 10 msv nella maggior parte dei casi . valori di dose inferiori potrebbero essere raggiunti aumentando la pendenza della transizione della corrente nelle acquisizioni di modulazione cardio - sincronizzata . 
la transizione della corrente rappresenta una costante sorgente di dose surplus dellordine del 14%34% della dose totale , con valori maggiori nei protocolli acquisiti con finestra di pulsazione stretta e modulazione mindose ( rinunciando alla possibilit di effettuare valutazione sui volumi del ventricolo sinistro )  . 
bergman5 1department of radiology , ziekenhuizen oost - limburg , schiepse bos 6 , 3600 genk , belgium 2department of orthopedic surgery , hospital for special surgery , new york , ny 10021 , usa 3department of radiology , brigham and womens hospital , harvard medical school , boston , ma 02115 , massachusetts , usa 4department of radiology , lucas mrs / i center , stanford , ca 94305 , usa 5franklin & seidelmann radiologists , 4240 marble ridge road , el dorado hills , ca 95762 , usa correspondence to : j . 
unrestricted physiologic joint motion results in multidirectional displacement of the anatomic structures . when performing real - time magnetic resonance ( mr ) imaging of such a joint motion , continuous adjustment of the scan plane position may be required . 
the location of a small tracker device ( dedicated hardware ) placed on the patients skin overlying a joint was determined by an ultrashort mr sequence and used to automatically adjust the scan plane position prior to each dynamic - motion mr image . 
using a vertically open mr unit , this mr tracking system was applied in ten dynamic - motion mr examinations to evaluate flexion / extension manoeuvres in the weightbearing knee joint , and in ten dynamic - motion mr examinations of the shoulder joint to evaluate manoeuvres such as internal / external rotation of the humerus , stress testing of the glenohumeral joint and abduction / adduction manoeuvres . 
quando viene effettuato uno studio di risonanza magnetica ( rm ) in tempo reale di una articolazione in movimento , si pu rendere necessario un aggiustamento continuo del piano di scansione . 
la localizzazione di un piccolo sistema di posizionamento ( con hardware dedicato ) posizionato sulla cute del paziente stata determinata mediante una sequenza rm ultrarapida ; la sequenza viene utilizzata per riposizionare automaticamente il piano di scansione prima di ogni acquisizione rm dinamica . 
mediante un apparecchio rm aperto con campo magnetico verticale sono state effettuate 10 acquisizioni dinamiche in movimento di flesso - estensione sullarticolazione del ginocchio sottocarico e 10 acquisizioni dinamiche dellarticolazione della spalla per valutare le manovre di rotazione interna / esterna dellomero , le prove di stress dellarticolazione glenoomerale e le manovre di abduzione / adduzione . 
the mr tracking system to guide the slice position for each consecutive dynamic - motion mr image of the freely but slowly moving shoulder or knee joint was feasible for clinical use , providing a high percentage of useful images for each manoeuvre within a clinically acceptable time frame . keywords magnetic resonance imaging kinematic musculoskeletal imaging patellofemoral joint imaging glenohumeral joint imaging mr tracking introduction real - time dynamic - motion magnetic resonance ( mr ) imaging refers to acquiring images of an anatomic region of interest ( roi ) within a joint that is in motion . 
it is distinct from a video display of a series of mr images acquired while the joint is held static in different positions [ 14 ]  . open - configuration mr units provide the opportunity to image joints in motion : patients may move joints in an unrestricted physiologic way within the wide gantry space . 
moreover , vertically open mr units providing the option to place the patient in upright ( standing ) position have the added value of evaluating the spine and the joints of the lower limb in physiologically weight - bearing conditions [ 7 , 8 ]  . the unrestricted multidirectional motion of a joint , limb or entire body during mr imaging results in a technical challenge : how to continually adjust the position of the scan plane for imaging the moving anatomy of interest . 
the purpose of our study was to evaluate the clinical feasibility of this mr tracking system to maintain the scan plane position at a constant anatomic location within a joint or limb that is freely moving in a slow fashion . materials and methods mr tracking system the mr tracking system was developed from a real - time risultati . 
il sistema rm di guida della posizione dello strato per ogni immagine rm dinamica delle articolazioni della spalla e del ginocchio in movimento libero e lento applicabile per uso clinico consentendo di ottenere una percentuale elevata di immagini utili per ogni manovra in un periodo di tempo clinicamente accettabile . parole chiave : risonanza magnetica imaging muscoloscheletrico cinematico imaging dell ' articolazione rotuleo - femorale imaging dell ' articolazione glenoomerale mr tracking position - monitoring system used for localising the tip of invasive devices within patients bodies , such as mrcompatible intravascular catheters [ 10 ]  . 
relevant hardware components and function are explained hereafter . the mr tracking system or mr position - monitoring system uses a configuration of four hardware parts : a miniature radiofrequency coil immersed in a reservoir of dilute gadolinium diethylenetriamine pentaacetic acid ( dtpa ) ( cordis corporation , europe n.v. , waterloo , belgium ) , a signal amplifier with isolation circuit , the magnets computing system and a sun workstation ( sun microsystems , mountain view , ca , usa )  . 
 the position of the tracking coil is determined prior to the acquisition of dynamic - motion mr images by applying an ultrashort tracking mr pulse sequence ( containing a nonselective radiofrequency pulse and a readout magnetic field gradient pulse for determining the location of an mr signal source , to be repeated for each x , y and z axis ) that uses a hadamard multiplexing scheme ( reducing the acquisition of positional information to four instead of six excitations ) [ 10 ]  . 
this information is radiol med ( 2010 ) 115 : 133140 communicated to the magnets computing system , and the position of the scan plane is updated prior to the acquisition of the next dynamic - motion mr image . 
prior to entering the mr unit , all patients completed a screening form for mr contraindications , and informed consent was obtained . approval for this study was waived by the institutional review board . 
patient in upright weight - bearing position for flexion and extension study of the knee with large crown receive / transmit imaging coil ( white arrow ) around the knee , supported by pads and a strap . 
deep to the imaging coil ( white arrow ) , the tracker coil ( black arrow ) is attached to the skin over the proximal third of the patella ( inset )  . 
paziente in posizione eretta , sotto carico per lo studio in flessione e estensione del ginocchio con bobina ricevente / trasmittente ( freccia bianca ) attorno al ginocchio , supportata da cuscinetti e una cinghia . 
sotto la bobina di acquisizione delle immagini ( freccia bianca ) , la bobina del sistema di posizionamento ( freccia nera ) attaccata alla cute sopra il terzo prossimale della rotula . 
la bobina del sistema di posizionamento contenuta in un piccolo contenitore riempito con una soluzione acquosa contenente un chelato di gadolinio . 136 radiol med ( 2010 ) 115 : 133140 during active , slow flexion / extension of the knee between 0 and 45 of flexion . 
care was taken that the physiologic movement of the patients knee was not restricted by any device , and patients were allowed to move not only the knee , but also , for example , hip and body . for dynamic - motion mr imaging of the shoulder , patients were examined in the upright , sitting position . 
alternatively , the tracking coil could simply be held at the finger tips of the physician performing the dynamic shoulder exam to interactively guide the scan plane position to the desired anatomy . 
transverse mr images were obtained during internal and external rotation manoeuvres of the humerus and during anterior and posterior stress testing by a physician both in adducted arm position and in abduction and exorotation ( aber ) position ( apprehension test )  . 
unrestricted motion of the arm , shoulder and upper body in all directions was allowed within the imaging fov of the mr unit to achieve physiologic joint motion . the clinical feasibility of the mr tracker system was evaluated by analysing the number of manoeuvres performed , the number of mr images per manoeuvre obtained and the percentage of useful mr images per manoeuvre . 
a manoeuvre was considered completely imaged if at least four useful images were acquired ( equally spread over the range of motion for each phase of that manoeuvre )  . 
 discussion imaging osteoarticular relationships during joint motion may be used to study the normal biomechanics of a joint but also to help the clinician visualise abnormal joint biomechanics when clinical examination is abnormal or equivocal . real - time mr imaging of moving joints , i.e. 
to evaluate the relative change in position of bony structures , mr images should be acquired at a constant anatomic level through one of the bony structures of the joint . 
however , physiologic joint motion with or without weight - bearing conditions involves motion not only of the joint itself , but also of the limb , adjacent joints and often the entire body of the patient . 
consequently , if one aims to image a truly physiologically moving joint , the position of the scan plane needs to be adjusted continuously . mr tracking systems were initially developed to determine the position of devices inside or outside the patient in order to update pulse sequence parameters and slice position in real time [ 11 , 12 ]  . 
applications for mr tracking include tracking the tip of intravascular catheters , tracking devices for mr - guided biopsy and tracking of mr - guided nasogastric tube placement [ 13 , 14 ]  . 
the technical challenge to track the freely moving joint within the mr unit and guide the imaging scan plane to a constant anatomic position within the joint has been overcome using an external mr tracker coil with an internal spin source [ 9 , 15 ]  . 
imaging planes perpendicular to the main direction of joint motion ( through - plane motion ) required a higher repetition of manoeuvres and resulted in lower percentage of useful mr images compared with imaging planes parallel to the main direction of joint motion ( in - plane motion )  . 
2a - c axial dynamic - motion mr images of the knee ( patellofemoral joint ) during flexion with and without use of the mr tracking system in a 26 - year old woman . 
therefore , the position of the initial scan plane ( solid line ) through the extended knee joint does not coincide with the optimal scan plane position ( dashed line ) through the same anatomic area of the patella in higher degrees of flexion . 
b if mr imaging of the knee is performed without adjusting the scan plane , the patella ( p ) readily disappears from the image when the patient flexes the knee , and therefore , patellofemoral relationships cannot be visualised during flexion . 
c using the external mr tracker , the scan plane position is continuously adjusted and a consistent visualisation of the patella ( p ) at the same anatomic level is obtained during knee flexion . 
2ac immagini rm assiali in movimento dinamico del ginocchio ( articolazione femoro - rotulea ) in flessione con e senza impiego del sistema di posizionamento in una paziente di 26 anni . 
pertanto , la posizione del piano di scansione iniziale ( linea continua ) attraverso il ginocchio in estensione non coincide con il piano di scansione ottimale ( linea tratteggiata ) attraverso la stessa area anatomica della rotula in un grado maggiore di flessione . 
b se lesame rm viene effettuato senza correggere il piano di scansione , la rotula ( p ) scompare dallimmagine quando il paziente flette il ginocchio e di conseguenza , i rapporti femoro - rotulei non possono essere visualizzati in flessione . 
c utilizzando il sistema di posizionamento esterno la posizione del piano di scansione corretta di continuo per cui possibile ottenere una buona visualizzazione della rotula ( p ) allo stesso livello anatomico . 
la piccola bobina del sistema di posizionamento ( freccia bianca ) visibile allinterno dellalta intensit di segnale del contenitore posizionato sulla cute , al terzo medio della rotula . 138 table 1 results tabella 1 risultati radiol med ( 2010 ) 115 : 133140 type of manoeuvre scan plane manoeuvre repetition times number of images per manoeuvre useful images ( % ) imaging timea knee joint flexion / extension flexion / extension shoulder joint endo / exorotation ap and pa stress abduction / adduction abduction / adduction sagittal transverse transverse transverse transverse coronal 1.6 ( 12 ) 5.8 ( 57 ) 2.1 ( 13 ) 3.2 ( 24 ) 5.6 ( 47 ) 4.3 ( 36 ) 12 ( 520 ) 15 ( 825 ) 8 ( 614 ) 7 ( 512 ) 18 ( 1030 ) 16 ( 1230 ) 1 min 10 s 4 min 51 s 1 min 25 s 2 min 14 s 4 min 33 s 3 min 07 s numbers are averages and ranges are shown in parentheses ap , anteroposterior ; pa , posteroanterior ; stress testing was performed both in neutral and in the abduction and exorotation ( aber ) position ( apprehension test ) aimaging time refers to total imaging time including all manoeuvres performed in this scan plane manoeuvres of the knee imaged in the transverse plane ( mainly the same through - plane motion ) , whereas manoeuvre imaged in the sagittal plane often required no repetition and yielded a high percentage of useful images ( mainly in - plane motion )  . 
in our experience , flexing the knee joint too quickly resulted in a fast downward translation of the patella out of the transverse imaging plane but not out of the sagittal imaging plane , as there is only a slight medial or lateral deviation during knee flexion . 
in a preclinical study , adequate tracking of the area of interest has been demonstrated up to speeds of 1.5 cm per second using a phantom [ 9 ]  . 
 as an alternative method to set the scan plane for mr imaging during free joint motion , others have developed an interactive scan control method : based on viewing of fluoroscopic mr images , the position of the scan plane is interactively adjusted throughout the whole kinematic mr examination [ 17 ]  . 
however , these continuous adjustments are performed manually , whereas our method is fully automated : no interaction is required to adjust the scan plane position using the mr tracking system . some limitations of the external mr tracker system need to be mentioned . 
for example , when imaging in the sagittal plane , the slice position was adjusted in a medial or lateral direction ( parallel to the original scan plane )  . however , the position of the fov within this imaging plane was not adjusted in anteroposterior or superoinferior direction . 
therefore , a fov large enough to include the joint in the mr image during the full range of motion of the performed manoeuvre needed to be chosen from the start . 
mr images of better quality to evaluate joints under stress can be obtained using static mr imaging with spin - echo t1 - weighted sequences and nonmagnetic devices applying stress to joints [ 18 ]  . 
using multiple tracker coils , not only scan plane position but also scan plane direction ( including oblique imaging planes ) probably could be adjusted , but this technique was not used [ 19 ]  . in this study , true physiologic motion of the shoulder and knee joints could be performed regarding body and limb movement in space , but motion was not physiologic regarding speed . 
the slow motion needed for real - time mr image acquisition may have some influence on joint biomechanics and could therefore obscure or overestimate abnormal joint biomechanics in some cases . other applications using the mr tracker can be developed , and other mr units can be used . 
this may include the anterior and posterior drawer tests in the knee and ankle , joint motion studies of the hip joint and the elbow joint , neer and hawkins positions of the shoulder joint , and lumbar spine motion [ 20 ]  . in conclusion , the mr tracking system to guide the slice position for each consecutive transverse , coronal or sagittal radiol med ( 2010 ) 115 : 133140 fig . 
3a - c axial dynamic - motion mr images of shoulder abduction ( glenohumeral joint ) with and without use of the mr tracking system in a 24 - year old woman . 
in the sitting position , the patient is allowed to freely move torso , shoulder and arm within the imaging field of the mr unit , which represents true physiologic motion . 
therefore , the initial position of the scan plane ( solid line ) through the glenoid in the adducted upper extremity does not coincide with the optimal scan plane position ( dashed line ) through the glenoid when the arm is abducted . 
b if the mr position of the scan plane is not adjusted , dynamic - motion mr imaging in the axial plane during abduction fails to depict the glenohumeral joint at a consistent level during the full range of motion , and the axilla rather than the glenoid ( g ) and humeral head ( h ) is imaged when the arm is abducted > 45 . 
3a - c immagini rm assiali in movimento dinamico della abduzione della spalla ( articoclazione gleno - omerale ) con e senza luso del sistema di posizionamento in una paziente di 24 anni . 
in posizione seduta , viene consentito al paziente di muovere liberamente il dorso , la spalla e il braccio allinterno del campo di immagine della apparecchiatura rm , in modo da rappresentare il vero movimento fisiologico . 
si nota che la glenoide ruota e si disloca cranialmente quando il braccio abdotto ( in relazione al normale ritmo scapolo - omerale comprendente la rotazione scapolare nei confronti della parete toracica )  . 
pertanto la posizione iniziale del piano di scansione ( linea continua ) attraverso la glenoide dellestremit superiore addotta non coincide con la posizione ottimale del piano di scansione ( linea tratteggiata ) attraverso la glenoide quando il braccio abdotto . 
b se il piano di scansione non viene corretto , le immagini rm in movimento dinamico sul piano assiale in abduzione non riescono a cogliere larticolazione gleno - omerale durante tutto larco del movimento e si visualizza lascella piuttosto che la glenoide ( g ) e la testa omerale ( h ) quando il braccio abdotto per pi di 45 . 
c utilizzando il sistema di posizionamento e applicando la bobina piccola ( freccia bianca ) alla cute che ricopre la glenoide ( g ) posteriormente , possibile aggiornare e correggere la posizione del piano di scansione in modo continuo . 
in questo modo i rapporti gleno - omerali sono evidenziati in tutto larco del movimento di abduzione . 140 radiol med ( 2010 ) 115 : 133140 mr image of the freely moving shoulder or knee joint was feasible for clinical use provided joint motion was slow enough to accommodate for the acquisition of dynamicmotion mr images . 
di diagnostica per immagini e radiologia interventistica , azienda usl di ferrara , ospedale del delta , via valle oppio 2 , 44023 lagosanto , ferrara , italy 2clinical application specialist ct , philips healtcare correspondence to : s . 
the aim of this study was to assess the radiation dose of dose - reduced unenhanced abdominal multidetector computed tomography ( mdct ) scan protocols for suspected renal colic in patients within normal weight range and overweight - obese patients and to record the cumulative dose of repeated examinations . 
over a 2 - year period , we performed 1 , 026 unenhanced ct examinations for urolithiasis ; among these , 675 were performed on 636 patients referred from the emergency department . 
patients were divided into two groups on the basis of body mass index ( bmi ) : normal weight ( bmi < 25 kg / m2 group 1 ) ; overweight and obese ( bmi > 25 kg / m2 group 2 )  . 
although radiation dose is nearly double in overweight - obese patients undergoing mdct , it remains lower than that delivered by a standard - dose protocol . patients with flank pain , who are often young , are at increased risk for serial ct examinations . 
scopo dello studio misurare la dose efficace della tc addominale diretta con protocolli a bassa dose dedicati per pazienti di corporatura normale e pazienti obesi con sospetta urolitiasi , registrando inoltre lesposizione derivante da indagini tc ripetute . 
durante un periodo di due anni abbiamo eseguito 1026 indagini tc per urolitiasi ; tra queste , 675 tc sono state eseguite in 636 pazienti provenienti dal pronto soccorso ( ps )  . 
per ogni paziente stato calcolato lindice di massa corporea ( bmi ) dividendo i pazienti in due gruppi : pazienti di taglia normale ( bmi < 25 kg / m2 , gruppo 1 ) e sovrappeso - obesi ( bmi > 25 kg / m2 , gruppo 2 )  . 
la dlp media e la dose efficace media sono risultate di 177 e 345 mgycm e 2 , 4 e 4 , 8 msv rispettivamente per il gruppo 1 ed il gruppo 2 . 
the superiority of ct compared with intravenous urography ( ivu ) and ultrasonography ( us ) has been demonstrated by many clinical trials [ 47 ] in which ct had sensitivities of 96%100% , specificities of 95.5%100% and accuracies of 96%98% . 
 moreover , several previous studies [ 6 , 8 , 9 ] have shown that 10%45% of patients presenting with flank pain are affected by extraurinary conditions ( the most common disease entities that can mimic renal colic are [ 10 ] diverticulitis , adnexal masses and appendicitis )  . 
 the limit of ct is the dose of radiation delivered to the patient , which is of particular concern because many patients are young and undergo repeated examinations [ 11 , 12 ]  . 
however , ed can vary considerably , mainly as a result of body mass , but also because of the number of images taken at ivu [ 13 ]  . 
 [ 13 ] also reported that overweight and obese individuals in whom seven or more ivu images are taken are exposed to a risk comparable with that of a standard - dose ct study . 
different low - dose protocols have been proposed for ct evaluation of renal colic [ 1620 ] , with estimated ed as low as 1.5 msv or lower [ 21 ] , maintaining sensitivities and specificities close to those of standard - dose ct . 
however , one limitation of previous low - dose studies was that the protocols were not suited for large or obese sin dalla sua introduzione nel 1995 [ 1 ] la tc addominale senza somministrazione di mezzo di contrasto ( mdc ) ( unenhanced helical computed tomography , uhct ) risultata la tecnica di imaging pi precisa ed accurata nel paziente con sospetta urolitiasi [ 2 , 3 ] divenendo quindi la metodica gold standard nella valutazione di tali pazienti . la superiorit della uhct nei confronti di urografia endovenosa ( ivu ) ed ecografia ( us ) stata dimostrata da molteplici studi clinici [ 47 ] , che hanno evidenziato per la tc valori di sensibilit tra 96%100% , di specificit tra 95 , 5%100% e accuratezza tra 96%98% . 
precedenti studi [ 6 , 8 , 9 ] hanno inoltre dimostrato che nel 10%45% dei pazienti con dolore al fianco la tc identifica facilmente le patologie extraurinarie ( le affezioni che pi frequentemente mimano il dolore della colica renale [ 10 ] sono : diverticolite , masse annessiali ed appendicite )  . il limite della tc rappresentato dalla dose erogata al paziente , specialmente in pazienti con colica renale , spesso giovani e con alta probabilit di andare incontro a ripetute indagini [ 11 , 12 ]  . 
recentemente alcuni autori hanno valutato limpatto dosimetrico di ripetute indagini tc con protocollo standard - dose , riportando una dose media efficace per un singolo studio di 6 , 5 msv con tc a singolo detettore e 8 , 5 msv con tc multistrato ( tcmd ) ; gli stessi autori hanno evidenziato una dose efficace compresa tra 19 , 5153 , 7 msv nei pazienti sottoposti a indagini multiple . rispetto alla ivu la dose media efficace della tcmd con protocollo standard - dose stata misurata circa doppia [ 1315 ]  . 
tuttavia la dose efficace pu variare considerevolmente , principalmente a causa della massa corporea , ma anche in relazione al numero di esposizioni effettuate durante ivu [ 13 ]  . 
 [ 13 ] nel loro studio hanno calcolato che individui sovrappeso - obesi sottoposti a 7 o pi esposizioni in corso di ivu sono esposti ad una dose comparabile a quella di una tc standard - dose . lutilizzo di un protocollo tc a bassa dose consente una significativa riduzione della radioesposizione . 
del resto parecchi lavori in letteratura , in campi di applicazione diversi dalla nefrolitiasi , hanno dimostrato che indagini tc di qualit diagnostica possono essere ottenute con una riduzione significativa dei mas . 
per la valutazione tc della colica renale sono stati proposti vari protocolli a bassa dose [ 1620 ] , con una dose efficace di 1 , 5 msv o anche inferiore [ 21 ] , pur mantenendo sensibilit e specificit radiol med ( 2010 ) 115 : 105114 individuals . 
we also evaluated the number of ct examinations performed for suspected renal colic and the cumulative radiation dose delivered . materials and methods patient population during a 2 - year period , 1 , 026 mdct examinations for urinary tract calculi were performed . 
among these , 675 low - dose unenhanced mdct examinations were performed on 636 consecutive patients with flank pain referred from the emergency department [ mean age 52.114.4 standard deviation ( sd ) years , range 2086 years ]  . 
patients within a normal weight range ( bmi < 25 kg / m2 ) were included in group 1 and overweight and obese patients ( bmi > 25 kg / m2 ) in group 2 . 
each patients age , sex and number of unenhanced ct examinations performed for suspected renal colic were then determined . dose - modulation systems our scanner has three systems for dose modulation and automatic current selection : automatic current selection ( acs ) : this system allows one to automatically manage milliampere per second / slice to maintain a constant signal - to - noise ratio ( snr ) in patients imaged with the same protocol . 
this system can be managed in two ways : automatic where acs refers to a database of normality already present in the syste during the scanogram , the system detects the point of greater absorption and determines the value of milliampere per second / slice appropriate to maintain the snr ( expressed by the sd value of water ) constant . simili a quelle della tc standard - dose . 
alcuni studi in letteratura riguardanti limpiego di tc bassa dose nel sospetto di nefrolitiasi , hanno evidenziato dei limiti della metodica negli individui obesi ; tali ricercatori [ 18 , 20 , 22 ] hanno suggerito , per una adeguata valutazione del paziente obeso limpiego di un protocollo tc a dose standard al fine di ottenere una migliore qualit delle immagini . 
lo scopo del nostro studio la misurazione della dose efficace della tcmd con doppio protocollo a bassa dose , per il paziente di corporatura normale e per il paziente soprappeso - obeso . 
abbiamo inoltre registrato il numero di tcmd effettuate dai pazienti con colica renale e la dose cumulativa di radiazioni erogata . materiale e metodi pazienti osservati durante un periodo di 2 anni sono state eseguite 1026 tcmd per la valutazione di litiasi delle vie urinarie . 
tra queste , sono state eseguite 675 indagini tc dirette a bassa dose su un totale di 636 pazienti consecutivi provenienti da ps con dolore al fianco ( et media 52 , 114 , 4 ( sd ) , range 2086 anni )  . 
i criteri di esclusione dei pazienti sono stati : gravidanza , et inferiore ai 18 anni , segni di infezione con febbre o precedente tc per calcoli urinari nei 6 mesi antecedenti . 
i pazienti nel range di peso considerato normale ( bmi < 25 kg / m2 ) sono stati inclusi nel gruppo 1 e i pazienti sovrappeso ed obesi ( bmi > 25 kg / m2 ) nel gruppo 2 . 
sono inoltre stati considerati per ogni paziente et , sesso e numero di indagini tc dirette eseguite per sospetta colica renale nel periodo di osservazione . sistemi di modulazione della dose il nostro scanner ha 3 sistemi di modulazione di dose e di correzione automatica dei mas utilizzabili : acs ( automatic current selection ) tale sistema consente di automatizzare la gestione dei mas / slice per mantenere costante il rapporto segnale rumore nei pazienti eseguiti con lo stesso protocollo , tale sistema pu essere gestito in due modi automatico e manuale : automatico : lacs fa riferimento ad un database di normalit gi presente nel sistema . 
al momento dellesecuzione dello scanogramma , il sistema rileva il punto di maggior assorbimento e determina il 108 radiol med ( 2010 ) 115 : 105114 manual this differs from the previous method only in the definition of the value of snr to be maintained . in this case , the examination is performed with the qualitative data decided by the operator . 
at the end of data acquisition , the sd values obtained will be repeated for the following patients . dose - modulation system ( d - dom ) works on the x - axis : the ct controller is able to assess the exposure of each reading , correcting the value of milliampere per second / slice in the next one . 
the typical example is at the level of the shoulders , where the system delivers a greater dose in laterolateral readings ( greater patient thickness ) than in anteroposterior readings . dose - modulation system on the z - axis ( z - dom ) : it acquires the scout view and determines a scale of beam attenuation on the basis of which the dose ( milliampere per second / slice ) is modulated . 
z - axis modulation adjusts the tube current in the scanning direction and results in a substantial reduction in mean radiation dose [ 23 ] compared with fixed tube current scanning [ 24 ]  . technical imaging parameters ct scans were performed from the top of the kidneys to the base of the bladder with the patient in the supine position and without the use of iv contrast material using a 64mdct scanner ( philips brilliance 64 , philips medical systems , best , the netherlands )  . 
in all patients , low - dose mdct scans were obtained with a 2 - mm nominal slice width , 1 - mm slice increment and voltage at 120 kv . 
exposure was reduced by selecting a maximum milliampere per second value for group 1 and group 2 , respectively , at 70 mas and 150 mas while keeping the other parameters constant . 
we decided not to use acs because this system changes the milliampere per second values based on patient size , so in the case of obese patients it can increase the set milliampere per second values and the dose to the patient . effective dose calculation the dose - length product ( dlp ) is the product of the weighted ct dose index ( ctdiw ) and the length of the imaged object ( in centimeters )  . 
to calculate the radiation dose delivered with a single low - dose valore di mas / slice idoneo per mantenere il rapporto segnale - rumore ( espresso dal valore di deviazione standard dellacqua ) costante . 
in questo caso si deve eseguire un esame con dei dati qualitativi decisi dalloperatore ; al termine dellacquisizione si dovr impostare il sistema in modo che la deviazione standard ottenuta sia quella da replicare nei pazienti successivi . d - dom un sistema di modulazione di dose che lavora sullasse x . 
lesempio tipico si ha a livello delle spalle dove il sistema eroga maggior dose nelle letture latero - laterali ( per maggior spessore del corpo del paziente ) rispetto a quelle anteroposteriori e postero - anteriori . z - dom un sistema di modulazione della dose sullasse z . 
la modulazione automatica di corrente lungo lasse z in grado di ridurre in maniera sostanziale la dose media di radiazioni [ 23 ] , rispetto alla scansione a corrente fissa [ 24 ]  . parametri tecnici di imaging le scansioni tc sono state eseguite dal polo superiore dei reni al pavimento vescicale con paziente in posizione supina , senza utilizzo di mdc endovenoso , utilizzando uno scanner multidetettore a 64 strati ( philips brilliance 64 , philips medical systems , best , olanda )  . 
lesposizione stata ridotta selezionando un valore massimo di milliampere / s rispettivamente di 70 mas e 150 mas per i gruppi 1 e 2 , mantenendo costanti i restanti parametri . 
nei pazienti del gruppo 1 sono stati utilizzati 70 mas senza modulatori di dose , mentre nel gruppo 2 abbiamo impostato 150 mas con modulazione di dose sullasse z ( z - dom )  . 
abbiamo deciso di non utilizzare il sistema acs poich tale sistema , che modifica i valori di mas in base alla corporatura del paziente , in caso di corporature obese potrebbe determinare un incremento del valore dei mas impostati e quindi ad un aumento della dose . calcolo della dose efficace il dlp il prodotto del ctdivol ( computer tomography dose index , dove ctdivol = ctdiw / pitch ) e la lunghezza delloggetto scansionato ( in centimetri )  . 
i fattori di radiol med ( 2010 ) 115 : 105114 unenhanced ct examination for flank pain , the estimated dlp for every ct examination was recorded from the scanner console . 
the conversion factor was taken [ 12 ] as the average ( 0.014 msv / mgy / cm ) of the abdominal and pelvic [ 25 ] conversion factors ( the conversion factor for abdominal ct is 0.012 msv / mgy / cm , and the conversion factor for pelvic ct is 0.016 msv / mgy / cm )  . 
a total of 25 patients ( 3.7% ) underwent two or more low - dose ct examinations for urolithiasis ; one patient in group 2 underwent four ct examinations during the study period . 
per calcolare la dose efficace normalizzata erogata dai protocolli tcmd a bassa dose abbiamo utilizzato i valori di dlp registrati dalla console dellapparecchio per ciascun paziente , ottenendo poi la dlp media per il gruppo 1 e 2 dalla somma delle singole dlp . 
il fattore di conversione stato calcolato [ 12 ] come la media ( 0 , 014 msv / mgy / cm ) tra il fattore di conversione addominale e pelvico ( il fattore di conversione per la ct addominale 0 , 012 msv / mgy / cm e il fattore di conversione per la ct pelvica 0 , 016 msv / mgy / cm )  . 
venticinque pazienti ( 3 , 7% ) sono stati sottoposti a 2 o pi indagini tc a bassa dose ( range 24 ) per urolitiasi ; un paziente del gruppo 2 , fig . 
1a axial image obtained in a 68 - year - old man ( body mass index 25 kg / m2 ) with low - dose protocol ( 70 mas , 120 kv ) shows a tiny calcification at the left ureterovesical junction . 
1a immagine assiale di una paziente di sesso femminile di 68 anni ottenuta con protocollo bassa dose ( 70 mas , 120 kv ) : sfumata calcificazione alla giunzione uretero - vescicale sinistra . 
posteriormente ad essa bene riconoscibile piccolo flebolita di 2 mb , la puntiforme immagine litiasica alla giunzione uretero - vescicale meglio identificabile nella immagine assiale acquisita con protocollo standard ( 300 mas , 120 kv ) al medesimo livello di a . 
after ct scan 52 / 636 patients ( 8.1% ) underwent at least one us examination within the next 6 months . mean dlp for a single examination for flank pain was estimated to be 177 and 345 mgy / cm for group 1 and group 2 , respectively . 
using these estimated ed for a single low - dose ct examination for suspected renal colic , the estimated ed delivered to the majority of patients was low , and most of these patients ( 96.3% ) underwent only one ct examination . 
however , the diagnostic value of discussione durante il periodo di studio , stato sottoposto a 4 esami tc . tutti i pazienti sottoposti a 2 o pi indagini tc avevano anamnesi positiva per calcoli delle vie urinarie . 
in 40 su 636 casi ( 6% ) i risultati della tc hanno richiesto approfondimento diagnostico , immediato o dilazionato di pochi giorni , mediante ulteriori scansioni tc con somministrazione e.v. 
dopo la tc , 52 / 636 pazienti ( 8 , 1% ) sono stati sottoposti ad almeno una indagine ecografica nei sei mesi successivi . la dlp media di una singola indagine tcmd diretta a bassa dose per il gruppo 1 ed il gruppo 2 sono state calcolate rispettivamente in 177 e 345 mgy cm ; pertanto la dose efficace media risultata di 2 , 4 msv nel paziente normotipo e 4 , 8 msv per pazienti sovappeso - obesi . 
sommando la esposizione cumulativa nei pazienti ( 3 , 7% ) sottoposti a 2 o pi indagini tc a bassa dose , risultata una dose efficace complessiva compresa nel range 4 , 819 , 2 msv . la tc attualmente la metodica gold standard nellimaging dei pazienti con sospetta colica renale , per molteplici motivi : velocit di esecuzione , elevata sensibilit nella individuazione del calcolo , panesplorabilit e diagnosi di patologie associate , utilit nella successiva gestione del paziente . 
poich i pazienti portatori di nefrolitiasi sono spesso giovani e possono incontro a ripetute indagini anche a breve distanza di tempo , luso sistematico della tc con conseguente radioesposizione ogniqualvolta si presentano con quadro clinico di colica renale costituisce per il radiologo motivo di riflessione etica [ 6 , 11 , 12 , 20 ]  . 
nellintento di contenere la dose entro valori accettabili , diversi protocolli tc a bassa dose sono stati di volta in volta proposti da vari autori , riportando risultati del tutto simili a quelli della tc standard dose ( persino un protocollo ultra - low dose a 6 , 9 mas , con esposizione simile a quella della diretta addome per ricerca calcoli , ha dimostrato migliori risultati della us nella valutazione della urolitiasi ) [ 21 ]  . 
 [ 19 ] , mediante impiego di corrente ridotta a 100 mas , hanno osservato una riduzione allincirca del 25%42% della dose al paziente rispetto allimpiego di un protocollo tc standard dose , senza significativo decremento nellaccuratezza [ 19 ]  . 
 [ 16 ] mediante impiego di corrente ridotta a 50 mas riportano una riduzione del 81% della dose nei confronti di un protocollo tc standard dose a 260 mas [ 16 ]  . 
la tc bassa dose ( 70 mas , 120 kv ) mostra ispessimento parietale del colon discendente , disomogeneit ed aspetti flogistici del grasso pericolico con minuscole micro - bolle aeree ( diverticolite con perforazione saccata )  . 
 radiol med ( 2010 ) 115 : 105114 ct comes at the expense of substantial radiation exposure . because many patients are young and undergo repeated examinations during their lifetime , the systematic use of ct at a patients admission represents an ethical concern [ 6 , 11 , 12 , 20 ]  . 
in order to decrease radiation dose , different lowdose protocols have been proposed with performance similar to that of standard - dose ct ( even an ultra - low - dose protocol 6.9 mas , with a radiation dose equivalent to that of plain abdominal x - ray ( or kub , kidney urinary bladder film ) has shown better results than us in evaluating urolithiasis ) [ 21 ]  . 
the study by kalra et al . [ 23 ] well documented the linear correlation between patient size and image quality and the need for an adequate scanning protocol for larger patients . 
 all ct equipment manufacturers have made available software that adjusts the milliampere per second continuously , depending on the thickness of the patient being penetrated by the beams at that point in time . 
these software programmes can also be used in conjunction with generalised reductions in milliampere per second levels when appropriate by setting maximum milliampere per second thresholds for the particular examination . 
in comparison with fixed tube current , automatic tube current modulation ( z - axis modulation ) results in a significant reduction of radiation , from 51% to 77% [ 23 , 27 ]  . 
 [ 20 ] compared a low - dose ct scan with a standard - dose ct scan in the same study population , showing equivalent performance for detecting stones 3 mm in the ureter of patients with a bmi < 30 kg / m2 , but some limitations in the detection of stones < 3 mm and in the determination of the exact stone size . 
 [ 17 ] hanno eseguito scansioni supplementari soltanto in caso di dubbio di calcoli o di aree con rapporto s / n estremamente sfavorevole , osservando alta accuratezza ed eccellente concordanza inter - operatore con dose efficace media di 1 , 2 msv per i maschi e 1 , 9 msv per le femmine . infatti possibile ridurre i mas nel pazienti di corporatura normale senza sacrificare la qualit dellimmagine , cosa che invece accade nei pazienti di corporatura robusta o soprattutto obesi ; in altre parole , il rumore nelle immagini tc cresce parallelamente allaumento della corporatura ( o , meglio , del diametro ) del paziente ( a parit degli altri fattori che contribuiscono allimmagine )  . 
 [ 23 ] dimostra una correlazione lineare tra la taglia del paziente e la qualit dellimmagine , suggerendo la necessit di un adeguato protocollo di studio nei pazienti di taglia robusta . 
 attualmente tutti gli apparecchi tc in commercio dispongono di software che modulano il livello di mas aggiustandolo in modo continuo , a seconda dello spessore del paziente che viene penetrato dal fascio radiogeno . 
nei confronti dei protocolli tc con corrente costante al tubo radiogeno , la modulazione automatica di corrente lungo lasse z ( z - axis modulation ) consente una significativa diminuzione della dose radiogena , dal 51% al 77% [ 23 , 27 ]  . parecchi investigatori hanno documentato problemi nellimpiego dei protocolli a bassa dose in pazienti obesi a causa di un rapporto s / n sfavorevole , con conseguente scarsa qualit diagnostica dellimmagine , suggerendo pertanto la necessit di una esposizione adeguata . 
 [ 23 ] hanno evidenziato che calcoli di dimensioni < 5 mm possono essere misconosciuti in caso di incremento notevole del rumore dellimmagine . altri autori avevano raccomandato in precedenti studi [ 18 , 28 ] limpiego di protocollo tc standard dose in pazienti obesi con bmi > 30 kg / m2 , con conseguente maggior esposizione , ai fini di ottenere una adeguata qualit dellimmagine . 
 [ 22 ] hanno messo in discussione lappropriatezza del protocollo bassa dose a 30 mas nei pazienti obesi , esprimendo dubbi riguardo alle diagnosi alternative / addizionali che potrebbero essere misconosciute in caso di eccessiva diminuzione dei mas . 
a differenza di altri autori [ 18 , 28 ] che suggeriscono limpiego di protocollo standard dose , anche nel paziente sovrappeso / obeso 112 radiol med ( 2010 ) 115 : 105114 missed at a higher noise index because of a greater image noise . 
previous studies recommended the use of standarddose ct with higher radiation exposure in obese patients ( bmi < 30 kg / m2 ) [ 18 , 28 ] to achieve adequate image quality . 
 [ 22 ] discussed the appropriateness of a low - dose protocol at 30 mas in obese individuals , expressing concern regarding the additional diagnoses that could be missed if the dose is lowered too much . unlike other authors [ 18 , 28 ] , in patients with a bmi > 25 kg / m2 , instead of a standard - dose ct protocol , we prefer to use a low - dose protocol suited for overweightobese patients , as this can reduce ed by half . 
 the mean ed delivered to overweight - obese patients of our study population ( 36% ) was nearly double that delivered to normal - weight patients ( 4.8 msv ) but lower than that of standard dose mdct [ 12 ]  . 
by setting exposure at 70 mas with automated z - axis tube current modulation , we obtained a mean ed of 2.4 msv , slightly higher than that reported by other authors with exposure at 30 mas [ 17 , 20 ] and 50 mas [ 16 ]  . 
to limit cumulative radiation exposure , in agreethe 6 - months ment with emergency physicians , following a ct scan , patients returning to the emergency department for retained stones or new episodes of colic are followed up with us . 
 our strategy of using us to follow - up patients with a former ct examination in the prior 6 months could be an explanation for the very low incidence ( 3.7% ) of repeat ct scans in our institution during a 2 - year study period . conversely , broder et al . 
 [ 11 ] reported 2.5 ct examinations per patient in emergency patients ( 49% during an observation period of 10 months had two ct scans and 10% had five or more )  . 
these authors [ 12 ] suggest that a combination of plain abdominal x - ray ( kub film ) and us could be used as a first imaging study in evaluating acute flank pain in patients who have a high pretest probability for symptomatic nephrolithiasis and who are likely to undergo serial ct . the limitations of this study include its retrospective noi preferiamo utilizzare un protocollo tc a bassa dose dedicato . la dose efficace media erogata al paziente sovrappesoobeso ( 36% dei pazienti della nostra casitica ) , pur risultando doppia ( 4 , 8 msv ) rispetto a quella del paziente normotipo , rimane comunque assai inferiore rispetto a quella di 8 , 5 msv erogata da un protocollo mdtc standard - dose [ 12 ]  . 
la maggior parte delle nostre indagini ( 64% ) sono state eseguite in pazienti di taglia normale . impostando la corrente del tubo a 70 mas , unitamente alla modulazione automatica di corrente lungo lasse z , la dose efficace media al paziente da noi registrata stata di 2 , 4 msv , leggermente pi elevata rispetto a quella riscontrata da altri autori che tuttavia hanno impostato valori minori di corrente , a 30 mas [ 17 , 20 ] o a 50 mas [ 16 ]  . la nefrolitiasi una patologia che frequentemente affligge il paziente adulto di giovane et , con una percentuale di recidiva di almeno il 50% [ 20 ] ; inoltre parecchi pazienti possono essere sottoposti a multiple esposizioni in caso di studi eseguiti durante il follow - up della malattia . 
in accordo con i colleghi del pronto soccorso , per limitare la esposizione cumulativa derivante da esami tc ripetuti , abbiamo scelto di utilizzare la us nel follow - up dei pazienti che si ripresentano al pronto soccorso nei 6 mesi successivi ad un esame tc ( per calcolo non ancora espulso o nuovi episodi di colica )  . 
in effetti nel follow - up dei pazienti con calcolo non espulso , la us la metodica pi semplice ed efficace per escludere la ostruzione subacuta o cronica delle vie urinarie . 
 la nostra scelta di effettuare il follow - up mediante us dei pazienti sottoposti nei 6 mesi precedenti ad un esame tc potrebbe essere una spiegazione della bassa incidenza ( 3 , 7% ) di ulteriori esami tc da noi riscontrata durante il periodo biennale di osservazione . 
al contrario broder et al . [ 11 ] hanno riportato in pazienti di ps una media di 2 , 5 esami tc per paziente ( 49% dei pazienti durante un periodo di osservazione di 10 mesi sono stati sottoposti a 2 indagini tc , mentre il 10% stato sottoposto a 5 o pi esami tc )  . 
gli stessi autori [ 12 ] suggeriscono che lindagine di prima istanza nello studio di pazienti con alta probabilit di nefrolitiasi sintomatica e alta probabilit di essere sottoposti a numerose indagini tc potrebbe essere la combinazione di us ed addome diretto . 
 i limiti del nostro studio includono la natura retrospettiva ed il calcolo della dose efficace partendo da valori di dlp forniti dal software dellapparecchio ; secondo alcuni autori radiol med ( 2010 ) 115 : 105114 nature and the use of estimates , rather than direct measurements , for dlp and ed . 
this may generate relevant differences in reported ed values . con tale metodologia la dose viene sottostimata nei confronti della misurazione sperimentale tramite dosimetri a termoluminescenza ( tld ) posti su un fantoccio antropomorfico [ 29 ]  . peraltro in letteratura sono usati differenti fattori di conversione specifici per la tc addominale per ottenere la dose efficace , con valori assai variabili , da 0 , 011 [ 20 ] a 0 , 0150 , 019 [ 26 ]  . 
ci pu essere causa di rilevanti differenze dei valori di dose efficace riportate dai diversi autori . conclusioni conclusions the systematic use of unenhanced ct in patients with suspected renal colic raises an ethical concern with regard to delivered radiation dose . 
a shared clinical strategy is needed to limit the number of repeat examinations in patients with renal colic . luso sistematico di tc addominale diretta nei pazienti con sospetta colica renale rappresenta un problema etico per il radiologo . 
limpiego di un protocollo tc a bassa dose pertanto obbligatorio nello studio della litiasi renale in pazienti , spesso giovani , che hanno alta probabilit di essere sottoposti a tc in altre successive occasioni . 
nel paziente soprappeso / obeso la dose efficace media erogata con il nostro protocollo dedicato pur essendo doppia rispetto al paziente di taglia normale , rimane assai inferiore rispetto alla dose erogata con protocollo standard . 
sabatini1 1department of radiology , 2department of neurology , irccs fondazione santa lucia , via ardeatina 306 , 00100 rome , italy 3interdisciplinary center for biomedical research , department of radiology , universit campus bio - medico di roma , rome , italy correspondence to : c.c. 
quattrocchi , via gravina di puglia 48 , 00133 rome , italy , tel . : + 39 - 06 - 51501346 , e - mail : c.quattrocchi@unicampus.it received : 17 september 2008 / accepted : 5 november 2008 / published online : 16 december 2009 springer - verlag 2009 abstract purpose . 
acquired images imported as digital imaging and communication in medicine ( dicom ) files , and the region of interest ( roi ) files were converted to neuroimaging informatics technology initiative ( nifti ) format and normalised to the montreal neurological institute ( mni ) standard template . 
lesame neurologico prevedeva lexpanded disability status scale ( edss ) con i sistemi funzionali , il barthel index ( bi ) e il rivermead mobility index ( rmi )  . 
le immagini , importate come file tipo digital imaging and communications in medicine ( dicom ) e file tipo regions of interest ( roi ) , sono state convertite in formato neuroimaging informatics technology initiative ( nifti ) e normalizzate rispetto al modello standard del montreal neurological institute ( mni )  . 
il metodo descritto , attraverso la attribuzione anatomica delle lesioni di sm , ha permesso di ottenere significativi coefficienti di correlazione tra la funzione sensoriale e il volume lesionale sotto - tentoriale misurato in rm in pazienti con sm . parole chiave sclerosi multipla risonanza magnetica volume lesionale correlazione clinica introduction introduzione magnetic resonance imaging ( mri ) provides the highest spatial resolution in detecting tissue alterations and plays a fundamental role in the diagnostic workup of patients with multiple sclerosis ( ms ) [ 1 ]  . 
mri has been used to characterise the real extent of tissue damage , especially in normalappearing white ( nawm ) and gray matter ( nagm ) [ 2 ] , to predict disease evolution [ 35 ] , as well as to monitor disease progression [ 68 ] and response to both established and experimental treatments [ 9 ]  . determining the amount and distribution of tissue damage by mri is crucial to understand disease pathogenesis and correctly monitor disease progression . 
this weak correlation has been ascribed to the limited sensitivity of conventional mri in detecting tissue damage in early stages , as highlighted by evidence of signal alterations in normal - appearing brain tissue using advanced mri techniques [ 2 ]  . 
the analysis of signal parameters and lesion distribution may help to overcome the discrepancy between clinical deficit and lesions detected by mri , as it has previously been reported [ 10 ]  . nevertheless the lack of total correspondence between clinical functional systems and anatomical locations and the adaptative functional changes that compensate for tissue damage may lead to underestimation of the clinical impact of lesion volume . 
in this regard , it would be interesting to analyse lesion distribution in ms patients to detect which location is correlated most closely to clinical disability and to identify sites for monitoring progression when widespread tissue involvement is observed . infratentorial locations , such as the brainstem and cerebellum , have been considered as clinically eloquent sites that may have major impact on clinical disability in ms limaging con risonanza magnetica ( rm ) permette di identificare , con la massima risoluzione spaziale possibile , alterazioni tissutali in pazienti con sclerosi multipla ( sm ) , giocando un ruolo fondamentale nella fase diagnostica di questa patologia [ 1 ]  . 
la rm stata utilizzata per caratterizzare la reale estensione del danno tissutale , soprattutto nella sostanza bianca ( nawm ) e nella sostanza grigia ( nagm ) apparentemente normale [ 2 ] , permettendo di predire levoluzione di malattia [ 35 ] , di seguirne la progressione [ 68 ] e la risposta a trattamenti sia stabiliti che sperimentali [ 9 ]  . determinare la quantit e la distribuzione del danno tissutale in rm cruciale per la comprensione della patogenesi di malattia e per seguirne correttamente la progressione . 
negli studi cross - sectional stata documentata una scarsa correlazione tra il volume lesionale totale , misurato nelle immagini t2 pesate , e la disabilit clinica [ 1012 ]  . 
la debole correlazione osservata stata riferita alla limitata sensibilit delle immagini convenzionali nella identificazione del danno tissutale negli stadi precoci di malattia , come dimostrato dalla evidenza di alterazioni della intensit di segnale a livello di tessuto cerebrale apparentemente normale , utilizzando tecniche avanzate di rm [ 2 ]  . 
lanalisi dei parametri del segnale rm e la distribuzione delle lesioni potrebbe aiutare a ridurre la incongruenza tra deficit clinico e lesioni visualizzate con rm , come gi documentato in letteratura [ 10 ] , sebbene la mancanza di totale corrispondenza tra sistemi funzionali clinici e sedi anatomiche e le modificazioni adattative , compensatorie del danno tissutale , possono determinare sottostima del reale impatto clinico del volume lesionale osservato . 
inoltre stata osservata una relazione tendente al plateau tra il volume lesionale totale misurato con sequenze a doppio eco e la disabilit a partire da valori dellexpanded disability status scale ( edss ) di 4 , 5 [ 13 ]  . 
a questo riguardo , potrebbe essere interessante analizzare la distribuzione del volume lesionale in pazienti con sm per capire quale sede anatomica correla con la disabilit clinica e per identificare siti radiol med ( 2010 ) 115 : 115124 patients [ 14 ]  . 
in this regard , the clinical impact of the infratentorial location of ms lesions may be of greater interest in advanced patients than in patients in the early stage of the disease . the proportional increment of signal - to - noise ratio provided by high field strengths ( 3.0 t ) has shown an increased sensitivity in detecting white - matter lesions [ 1820 ] and contrast - enhancing lesions [ 19 , 20 ] when compared with lower field strengths . 
the inclusion criteria were : ( a ) clinically defined ms according to the mcdonaldpolman criteria [ 22 ] , and ( b ) complete neurological examination performed by two experienced neurologists with at least 15 years experience in ms management . 
exclusion criteria were history of vascular , malignant or immunological diseases of the central nervous system ; severe systemic or psychiatric disorders ; and absolute contraindications to mri . clinical examination the neurological examination included the expanded disability status scale ( edss ) and its functional systems , i.e. 
in addition , the barthel index ( bi ) [ 23 , 24 ] and the rivermead mobility index ( rmi ) [ 25 ] were evaluated to provide more information on functional daily abilities . di monitoraggio della progressione di malattia , soprattutto quando presente ampio coinvolgimento tissutale , cio nelle fasi avanzate di malattia . le sedi sotto - tentoriali come il tronco - encefalo ed il cervelletto sono state considerate siti eloquenti che possono avere un impatto importante sulla disabilit clinica in pazienti con sm [ 14 ]  . 
a questo riguardo , limpatto clinico delle lesioni sotto - tentoriali nella sm pu essere maggiore in pazienti in fase avanzata rispetto a quelli in fase precoce di malattia . laumento proporzionale del rapporto segnale - rumore offerto dai campi magnetici ad elevate intensit di campo ( 3 , 0 t ) ha mostrato una maggiore sensibilit nella individuazione di lesioni della sostanza bianca [ 1820 ] e di lesioni con potenziamento dopo somministrazione endovenosa di gadolinio [ 19 , 20 ] , a confronto con campi magnetici di intensit inferiore . 
a 3 , 0 tesla , lidentificazione di 1 lesione sotto - tentoriale ha permesso di aggiungere un criterio di barkhof in pi nel 10% dei pazienti con sindrome clinicamente isolata [ 21 ]  . lo scopo dello studio di correlare il volume lesionale in sede sotto - tentoriale , usando immagini pesate in densit protonica ottenute a 3 , 0 tesla , con scale di disabilit e sistemi funzionali in pazienti con sm . materiali e metodi pazienti abbiamo studiato 20 pazienti consecutivi ( 13 donne e 7 uomini ) con una et mediana di 47 anni ( intervallo compreso tra 26 e 70 anni ) , affetti da sm clinicamente definita , seguite nella nostra unit operativa . 
i criteri di esclusione sono stati : anamnesi positiva per patologie cerebrali vascolari , neoplastiche e immunologiche , per gravi disordini sistemici o psichiatrici e controindicazioni assolute alla rm . 118 mri examination mri scans were performed by means of a whole - body mri system operating at 3.0 t ( allegra , siemens , erlangen , germany ) equipped with a maximum slew rate gradient of 400 t / m / s and a maximum strength of 69 mt / a quadrature birdcage head coil was used . 
the scanning protocol included contiguous interleaved axial sections ( slice thickness = 3 mm with no gap ) of dual - echo turbo spin - echo ( tse ) ( tr = 6 , 020 ms , te = 12 ms for pd weighting , te = 133 ms for t2 weighting , echo train length = 4 , slices = 48 ) , t1weighted tse ( tr = 838 ms , te = 7.5 ms , echo train length = 4 ) before and 5 min after i.v. 
identical field of view ( fov ) and matrix sizes were used for all pulse sequences , according to the guidelines of the consortium of ms centers [ 26 ]  . 
in addition , a 3d magnetisation - prepared gradient - echo ( mprage ) t1 - weighted sequence with isotropic resolution ( 1 mm3 ) ( tr = 2 , 500 ms , te = 4.38 ms , fa = 8 , fov 230 mm , matrix size = 256256 mm , slice thickness = 1 mm , a total of 176 sagittal images ) was performed . image analysis focal and confluent lesions were segmented by a trained radiologist on the pd - weighted images on a separate workstation using d - image software ( dilogix , rome , italy )  . 
for each region of interest ( roi ) , the area was measured to estimate volume according to the 3 - mm slice thickness . acquired images imported as digital imaging and communication in medicine ( dicom ) files and the roi files were converted to neuroimaging informatics technology initiative ( nifti ) format and normalised to the montreal neurological institute ( mni ) standard template . 
in the study , no distinction was made between the right and left sides . statistical analysis statistical differences in the lesion - wise analysis were assessed using the wilcoxon signed - rank test . 
univariate correlations between mri measures and disability scores radiol med ( 2010 ) 115 : 115124 esame clinico lesame neurologico ha previsto ledss e i sistemi funzionali piramidale , cerebellare , tronco - encefalo , sensoriale , sfinteriale , visivo e mentale . 
inoltre il barthel index ( bi ) [ 23 , 24 ] e il rivermead mobility index ( rmi ) [ 25 ] sono stati valutati per ottenere maggiori informazioni rispetto alle capacit funzionali quotidiane . esame rm gli esami di rm sono stati eseguiti utilizzando un magnete a 3 , 0 tesla ( allegra , siemens , erlangen , germania ) , con gradienti massimali di 400 t / m / s ed una forza massima di 69 mt / stata utilizzata una bobina di quadratura per lencefalo . 
il protocollo di scansione ha previsto una acquisizione con strati assiali contigui interfacciati ( spessore di strato = 3 mm senza gap ) utilizzando sequenza turbo spinecho ( tse ) a doppio eco ( time to repeat [ tr ] = 6020 ms , time of echo [ te ] = 12 ms per pesatura in densit protonica [ dp ] , te = 133 ms per pesatura in t2 , lunghezza del treno di echi = 4 , strati = 48 ) , t1 - pesata ( tr = 838 ms , te = 7 , 5 ms , lunghezza del treno di echi = 4 ) , prima e 5 minuti dopo somministrazione endovenosa di chelato del gadolinio , il gadolinio acido dietilentriamino penta - acetico ( gd - dtpa ) ( 0 , 1 mmol / kg di peso corporeo )  . 
sono stati usati campi di vista ( fov ) e matrici delle stesse dimensioni per tutte le sequenze di impulso , in accordo con le linee guida del consortium of ms centers [ 26 ]  . 
inoltre stata ottenuta una sequenza t1 - pesata 3d ( magnetization prepared gradient isotropica ( 1 mm3 ) echo , mprage ) a risoluzione ( tr = 2500 ms , te = 4 , 38 ms , flip angle [ fa ] = 8 , fov 230 mm , matrice = 256256 mm , spessore di strato = 1 mm , 176 immagini sagittali )  . analisi delle immagini lesioni focali e confluenti sono state segmentate da un radiologo esperto su immagini pesate in dp su una consolle separata usando il software d - image ( dilogix , roma , italia )  . 
per ciascuna regione di interesse ( roi ) , larea stata misurata per stimare il volume in accordo con uno spessore di strato di 3 mle immagini acquisite importate come file digital imaging and communications in medicine ( dicom ) e i file roi con le lesioni segmentate sono state convertite in formato tipo nifti e normalizzate rispetto al modello di riferimento standard del montreal neurological institute ( mni )  . 
la co - registrazione delle lesioni e delle immagini t1 pesate magnetization - prepared rapid acquisition with gradient echo ( mprage ) normalizzate di ogni paziente stata eseguita mediante il functional magnetic resonance radiol med ( 2010 ) 115 : 115124 fig . 
la segmentazione automatica ha incluso aree sopra - tentoriali ( lobo frontale , lobo parietale , lobo temporale , lobo occipitale , diencefalo ) e sotto - tentoriali ( cervelletto , troncoencefalo )  . 
nello studio non si considerata la distinzione tra lato destro e sinistro . analisi statistica le differenze statistiche nella analisi delle lesioni sono state valutate usando il wilcoxon - signed rank test . 
the enhancing lesions ( n = 18 ) , which were predominantly located at the periventricular level , were distributed as follows : frontal lobe ( 10 / 18 ) , parietal lobe ( 2 / 18 ) , temporal lobe ( 3 / 18 ) , occipital lobe ( 1 / 18 ) , diencephalon ( 1 / 18 ) and brainstem ( 1 / 18 )  . era statisticamente edss era di 7 , 1 per i casi di sm secondaria progressiva ( sp ) e 4 , 0 per i casi di sm recidivante - remittente ( rr ) ; significativa questa differenza ( p < 0 , 005 )  . 
non si sono osservate correlazioni significative tra rmi e bi con i sistemi funzionali sensoriale ( rho = 0 , 065 , p = 0 , 806 per rmi ; rho = - 0 , 059 , p = 0 , 823 per bi ) e visivo ( rho = - 0 , 115 , p = 0 , 661 ; rho = - 0 , 060 , p = 0 , 820 )  . stato osservato coinvolgimento diffuso della sostanza bianca periventricolare e sottocorticale , e alcune millimetriche aree focali di alterato segnale sono state individuate nella sostanza grigia corticale . 
il volume lesionale in dp era localizzato prevalentemente a livello sopra - tentoriale ( 93 , 1% ) a confronto con le aree sotto - tentoriali ( 6 , 9% )  . 
a livello sopra - tentoriale , il volume lesionale coinvolgeva prevalentemente i lobi frontali e parietali ( rispettivamente 31 , 7% e 30 , 2% del volume lesionale totale )  . 
in questo gruppo di pazienti sono state individuate un numero massimo di 4 lesioni sub - centimetriche , con un volume lesionale mediano con potenziamento di 1 , 37 cm3 ( intervallo compreso tra 0 , 62 e 13 , 2 cm3 )  . 
le lesioni con potenziamento ( n = 18 ) , prevalentemente localizzate a livello periventricolare , erano distribuite come segue : lobo frontale ( 10 / 18 ) , lobo parietale ( 2 / 18 ) , lobo temporale ( 3 / 18 ) , lobo occipitale ( 1 / 18 ) , diencefalo ( 1 / 18 ) , troncoencefalo ( 1 / 18 )  . correlazione tra scale cliniche e volume lesionale il volume lesionale misurato in dp a livello di tutto lencefalo ( tabella 2 ) non ha rivelato correlazioni significative con alcuna delle scale cliniche esaminate , anche dopo segmentazione automatica delle lesioni periventricolari ed iuxta - corticali o dopo segmentazione automatica delle lesioni a livello dei lobi frontali , parietali , temporali od occipitali . 
questo risultato stato confermato da una radiol med ( 2010 ) 115 : 115124 clinicalmri lesion - volume correlation the pd lesion volume in the whole brain analysis ( table 2 ) did not reveal significant correlation with any of the clinical measures examined ; after automatic segmentation of periventricular and juxtacortical lesions ; or after automatic segmentation of frontal , parietal , temporal and occipital lobes . 
this finding was confirmed by a significant correlation between lesion volume in the segmented brainstem ( rho = 0.701 , p = 0.005 ) and cerebellum ( rho = 0.784 , p = 0.001 ) and sensory function . no significant correlation was found between supratentorial lesion volume and edss , rmi and bi scores ( table 2 )  . discussion in this study , we observed a significant correlation between the measure of ms lesion volume in specific areas , such as the brainstem and cerebellum , and sensory functional system scores in patients with defined ms . 
previous studies have reported a significantly lower infratentorial brain volume in ms patients than in healthy subjects [ 27 ] , as well as a significant volume reduction in follow - up studies [ 28 ]  . a significant correlation between infratentorial brain volume and edss and infratentorial functional score has also been observed [ 29 ]  . 
thus , the presence of ms lesions on a shrunken infratentorial brain in ms patients may be correlazione significativa tra il volume lesionale nel troncoencefalo ( rho = 0 , 701 , p = 0 , 005 ) e nel cervelletto ( rho = 0 , 784 , p = 0 , 001 ) e il sistema funzionale sensoriale . non si sono trovate correlazioni significative tra il volume lesionale sopra - tentoriale ed edss , rmi e bi ( tabella 2 )  . discussione in questo studio abbiamo osservato una correlazione significativa tra la misura del volume lesionale in specifiche aree anatomiche , come troncoencefalo e cervelletto , e il punteggio ottenuto al sistema funzionale sensoriale in pazienti affetti da sm definita . 
studi precedenti hanno osservato un volume tissutale sotto - tentoriale significativamente ridotto in pazienti con sm rispetto a soggetti sani [ 27 ] , cos come una significativa riduzione del volume tissutale in studi di follow - up [ 28 ]  . 
stata osservata inoltre una significativa correlazione tra volume cerebrale sotto - tentoriale ed edss e sistema funzionale sotto - tentoriale [ 29 ]  . dunque , la presenza di lesioni sm in un volume cerebrale sotto - tentoriale ridotto pu essere critico per la progressione clinica di malattia in pazienti in fase avanzata di malattia . 
another explanation may be found in the specific architecture of the brainstem , where high neural fibre density and marked compartmentalisation may reduce its ability to functionally buffer the ms structural damage in eloquent sites . the correlation between the cerebellum and sensory function may be explained by a net predominance of the effect of tissue damage on functions such as proprioceptive sensory function , computation of sensory inputs and sensory - motor integration [ 30 , 31 ]  . 
 the impact of gadolinium - enhancing lesions has no significance in our study , as only one lesion enhanced at the spiegazione pu essere legata alla caratteristica architettura del troncoencefalo , dove lelevata densit di fibre e la marcata compartimentalizzazione possono ridurre la capacit di tamponare funzionalmente il danno strutturale della sm in siti eloquenti . la correlazione tra le lesioni a livello cerebellare e il sistema funzionale sensoriale pu essere spiegato da una netta prevalenza delleffetto del danno tissutale su funzioni come quella sensoriale propriocettiva e la capacit di elaborare input sensoriali ed integrare informazioni sensoriali e motorie [ 30 , 31 ]  . 
la correlazione che abbiamo osservato in questo studio tra i dati clinici e la rm potrebbe essere influenzata dalle piccole dimensioni del campione e dal fatto che il volume lesionale non ha incluso il danno della nawm e nagm , non visualizzabile nelle immagini in dp a 3 , 0 tesla . 
inoltre il coinvolgimento o lestensione del danno a livello del midollo spinale non sono stati considerati , sebbene il volume lesionale in t2 [ 32 ] , i tempi di rilassamento t1 [ 33 ] e le alterazioni metaboliche tissutali [ 34 ] a livello cervicale sono stati associati a disabilit motoria piuttosto che a disfunzioni sensoriali . limpatto di lesioni con potenziamento dopo gadolinio non significativo dal momento che soltanto una lesione mostrava potenziamento a livello sotto - tentoriale , e che il volume lesionale con potenziamento era trascurabile rispetto al volume lesionale totale misurato nelle immagini pesate in dp . 
a a 36 - year - old woman , relapsing / remitting multiple sclerosis ( rrms ) , edss = 1 , sensory functional system score = 1 ( not included in the statistical analysis )  . 
multiple lesioni iperintense a livello del compartimento posteriore del bulbo . radiol med ( 2010 ) 115 : 115124 infratentorial level , and the total volume of enhancing lesions was negligible in respect of the total lesion volume measured on pd - weighted images . 
the correlation between total t2 lesion volume and edss score is weak in cross - sectional studies [ 10 , 12 , 3537 ] in which patients with lower edss values have been evaluated . 
the plateauing relationship that has been reported between t2 lesion volume and disability for edss scores > 4.5 [ 13 ] may explain the lack of correlation in our sample . 
in this regard , the distribution of edss scores in our group of patients , whose median edss score was 6.5 , may have taken advantage of our method to correlate lesion volume with clinical disability . 
 the method that we describe allows ms lesions to be anatomically defined , thereby improving correlation indices between clinical and mri findings in patients with advanced ms and offering the possibility of monitoring disease progression more effectively . 
moreover , our approach may help reduce intercentre levels of variability in multicentre clinical trials on ms . la scala edss si dimostrata debole in studi crosssectional [ 10 , 12 , 3537 ] , in cui pazienti con edss pi bassi sono stati valutati . 
la relazione tendente al plateau tra volume lesionale in t2 e disabilit per edss superiori a 4 , 5 [ 13 ] potrebbe spiegare la mancanza di correlazione nel nostro campione . 
a questo riguardo la distribuzione dei punteggi edss nel nostro gruppo di pazienti , con valore mediano di 6 , 5 , pu essere derivata dal metodo che abbiamo utilizzato . 
noi abbiamo testato la correlazione con un approccio basato sulla sede anatomica delle lesioni , in maniera simile a come riportato da charil et al . [ 10 ] , sebbene utilizzando un differente algoritmo di analisi . nel nostro gruppo di pazienti , noi abbiamo provato ad ottenere una maggiore sensibilit nella identificazione di lesioni sm , sfruttando il maggiore rapporto segnalerumore consentito dallalto campo rispetto a campi di intensit inferiore . 
inoltre la procedura di normalizzazione dello spazio cerebrale dei nostri pazienti rispetto al modello mni e la segmentazione automatica delle aree anatomiche pu avere aumentato la consistenza della nostra analisi . recentemente nuove sequenze di impulso del tipo double inversion recovery sono state valutate ad 1 , 5 t e a 3 , 0 t , con possibilit di aumentare la sensibilit per il volume lesionale specialmente a livello di fossa posteriore [ 38 , 39 ] , sebbene noi abbiamo utilizzato sequenze standard in dp per la segmentazione delle lesioni . il metodo che descriviamo permette di definire anatomicamente in maniera automatica le lesioni di sm , permettendo di ottenere indici di correlazione pi elevati tra clinica e reperti rm in pazienti con sm in stadio avanzato , offrendo la possibilit di seguire la progressione di malattia con maggiore efficacia . 
reni , 01400 latina , italy 3university la sapienza , rome , italy 4oncology department , policlinico umberto i , university la sapienza , rome , italy correspondence to : c . 
from february 2005 to january 2008 , we treated 110 patients affected by liver metastatic disease from colorectal , breast , gastric , pancreatic , pulmonary , oesophageal and pharyngeal cancers and from cholangiocarcinoma and melanoma . 
according to our 3 - year experience , y - 90 radioembolisation ( sir - spheres ) is a feasible and safe method to treat liver metastases with an acceptable level of complications and a good response rate . keywords radioembolization liver metastases hepatic malignancy transcatheter therapy riassunto obiettivo . 
da febbraio 2005 a gennaio 2008 , sono stati trattati 110 pazienti affetti da malattia metastatica del fegato determinata da differenti tipi di tumore primitivo ( colorettale , mammario , gastrico , pancreatico , polmonare , esofageo , faringeo , melanoma e colangiocarcinoma )  . 
la risposta stata valutata come completa / parziale in 45 pazienti , come malattia stabile in 42 pazienti e come malattia in progressione in 23 pazienti . in 90 casi , stato ottenuto un decremento dei livelli sierici dei markers tumorali specifici . 
le complicanze sono rappresentate da 1 caso di insufficienza epatica di grado 4 , da 6 casi di gastrite di grado 2 e da 3 casi di colecistite di grado 2 . 
sulla base della nostra esperienza di tre anni 620 radiol med ( 2010 ) 115 : 619633 la radioembolizzazione con y - 90 rappresenta una metodica sicura ed efficace nel trattamento delle metastasi epatiche con un accettabile livello di complicanze ed una buona percentuale di risposta . parole chiave radioembolizzazione metastasi epatiche tumori epatici terapia transcatetere introduction introduzione liver metastases are among the most common tumoural manifestations worldwide . 
postmortem studies have revealed that the liver is involved in 50%70% of metastases from melanoma and lymphoma , and from the most common neoplastic diseases originating in the breast , lung and gastrointestinal tract , including colorectal carcinoma [ 2 ]  . the only curative treatment considered for liver metastases is surgical resection [ 1 ]  . 
however , this treatment is unfortunately restricted to a limited number of patients , as it depends on the size , number and site of liver tumour . the liver represents the main target for metastases so that effective control of metastatic hepatic involvement can favourably influence the progression of the disease . 
some therapeutic options are available in clinical practice for palliative care , including cryotherapy , radiofrequency and laser ablation , which have gained importance in recent years [ 3 , 4 ]  . 
however , these methods can only be used in patients with a limited number of hepatic lesions , whereas at diagnosis , most patients present with already widely disseminated metastases [ 5 ]  . chemotherapy in the form of doxorubicin has been used as the sole treatment for liver metastases for many decades and has produced modest results and survival rates . 
the introduction of taxane and herceptin now offers a significant improvement in the treatment of breast cancer [ 68 ]  . however , despite these important therapeutic advances , metastatic breast cancer is almost always fatal , with up to 60% of patients dying from hepatic insufficiency caused by the localised effects of the neoplas data from surveillance , epidemiology , and end results ( seer ) reveal that once a breast tumour has metastasised , patients have an average survival rate of 18.5 months compared with 7.5 months from colorectal tumour and 24.5 months from prostate cancer [ 9 ]  . radiotherapy can be administered with extreme accuracy through the use of linear accelerators . 
secondo studi autoptici stato dimostrato che il fegato risulta coinvolto nel 50%70% delle metastasi da melanoma , linfoma e dalle pi comuni patologie neoplastiche che originano dalla mammella , dal polmone e dal tratto gastrointestinale , tra cui il carcinoma colorettale [ 2 ]  . lunico trattamento ritenuto curativo nella patologia neoplastica metastatica confinata al fegato rappresentato dalla resezione chirurgica [ 1 ]  . 
tale trattamento purtroppo destinato ad un ristretto numero di pazienti visto che le dimensioni , il numero e la sede delle localizzazioni ne esclude la maggior parte . il fegato rappresenta dunque un organo bersaglio della malattia metastatica ed un controllo effettivo del tumore epatico pu condizionare favorevolmente la progressione complessiva della malattia . 
queste metodiche , comunque , risultano applicabili solamente in pazienti con un numero limitato di lesioni mentre , al momento della diagnosi , numerosi pazienti presentano unestesa disseminazione epatica della malattia [ 5 ]  . la chemioterapia come unico trattamento per la malattia metastatica del fegato , limitata per decenni alla doxorubicina , ha prodotto risposte e percentuali di sopravvivenza modeste . 
tuttavia , nonostante questi importanti perfezionamenti terapeutici , il tumore metastatico della mammella quasi sempre fatale : fino al 60% dei pazienti decedono per insufficienza epatica indotta dagli effetti locali della neoplasia . 
i dati del surveillance , epidemiology and end results ( seer ) rivelano che , una volta metastatizzato il tumore mammario , i pazienti hanno una sopravvivenza media di 18 , 5 mesi contro i 7 , 5 mesi del tumore colorettale e i 24 , 5 mesi del cancro alla prostata [ 9 ]  . la terapia radiante pu essere somministrata attualmente radiol med ( 2010 ) 115 : 619633 with systemic chemotherapy has become the therapeutic standard , as radiotherapy is considered to be one of the most efficacious weapons in the treatment of tumours . 
with this in mind , if the vessel supplying the tumour is catheterised using percutaneous techniques , administration of radiation , provided by radioactive - isotope - loaded microspheres , shows a significant improvement in delivering the radiation selectively to the tumour tissue [ 10 ]  . liver neoplasms receive their principal vascular supply from the hepatic artery [ 11 ] , and based on this , several cytotoxic agents have been developed that , through selective arterial catheterisation , can be administered directly inside the tumour . 
the therapy requires that 94% of radiation be administered in 11 days [ 13 ]  . the aim of our study was to evaluate the effectiveness of selective interventional radioembolisation therapy ( sirt ) in patients with liver metastases not responsive to the standard chemotherapy protocols . materials and methods consent of the hospital ethics committee was obtained before the beginning of the procedure and the retrospective collection of all data . inclusion / exclusion criteria patients with a histological diagnosis of the disease and hepatic involvement confirmed by computed tomography ( ct ) were considered for inclusion for this treatment . 
la combinazione di terapie palliative con chemioterapie sistemiche quindi diventata lo standard terapeutico dal momento che la terapia radiante considerata una delle armi pi efficaci nel trattamento dei tumori . tuttavia esistono limitazioni significative nellutilizzo di alte dosi radianti su alcuni segmenti corporei . 
in considerazione di ci , se il vaso che fornisce tale apporto al tumore viene cateterizzato tramite tecniche percutanee , la radiazione somministrata per via intra - arteriosa attraverso microsfere caricate con isotopi radioattivi si caratterizza per unelevata selettivit per il tessuto neoplastico [ 10 ]  . le neoplasie epatiche ricevono il loro principale apporto vascolare dallarteria epatica [ 11 ] e , sulla base di questo principio , sono stati sviluppati diversi agenti citotossici che , attraverso il cateterismo selettivo arterioso , vengono somministrati direttamente alla neoplasia . 
littrio 90 ( y90 ) un isotopo beta emittente con un emivita di 64 ore ed una profondit media di penetrazione di 2 , 4 mm [ 12 ]  . 
nella formulazione terapeutica il 94% della radiazione viene somministrata in 11 giorni [ 13 ]  . lo scopo del nostro studio quello di valutare lefficacia della terapia selettiva radioemobolizzate ( sirt ) nei pazienti con malattia metastatica del fegato non responsivi ai protocolli standard di chemioterapia . 
 materiali e metodi prima di intraprendere le procedure e di collezionare retrospettivamente tutti i dati stata ottenuta lapprovazione da parte del comitato etico aziendale . criteri di inclusione ed esclusione sono stati ritenuti candidabili i pazienti con diagnosi istologica di malattia e coinvolgimento epatico stimato tramite esame di tomografia computerizzata ( tc )  . 
specific tumour marker levels [ carcinoembryonic antigen ( cea ) , carbohydrate antigen 19 - 9 ( ca 199 ) , gastrointestinal - cancer - associated antigen ( gica ) ] were also measured in all patients prior to the procedure . 
 exclusion criteria were determined by bilirubin levels > 1.8 mg / dl and a hepatic - pulmonary shunt < 20% . patient selection from february 2005 to july 2008 , we treated 110 patients at the interventional radiology department , s.m goretti hospital , latina , italy , who were affected by liver metastases . 
among these , 47 cases were caused by colorectal neoplasms , 32 from breast cancer , six from gastric tumours , five from pancreatic tumours , three from oesophageal cancers , one from melanoma and one from pharyngeal cancer . 
fifteen patients had undergone prior radiofrequency treatment ( three of whom had three sessions ) ; three patients had undergone percutaneous ethanol injection ( pei ) and eight transarterial chemoembolisation ( tace )  . 
patient selection was based on the inclusion of patients who had already undergone a first - line chemotherapy such as folinic acid , second - line fluorouracil , oxaliplatin chemotherapy such as folinic acid , fluorouracil ( 5 - fu ) , irinotecan ( folfiri ) and a third line of chemotherapy , all of which had been ineffective in treating the primary tumour . 
i livelli dei marker tumorali specifici ( cea , ca 19 - 9 , gica ) al momento del trattamento sono stati misurati in tutti i pazienti . i criteri di esclusione sono stati determinati da livelli di bilirubina superiori a 1 , 8 mg / dl ed a shunt epato - polmonari > 20% . selezione dei pazienti da febbraio 2005 a luglio 2008 , nella sezione di radiologia interventistica , sono stati trattati 110 pazienti affetti da malattia metastatica del fegato . 
tra questi 47 erano causati da neoplasia colorettale , 32 da tumore della mammella , 6 da tumore gastrico , 5 da tumore del pancreas , 5 da tumore polmonare , 3 da tumore esofageo , 1 da melanoma e 1 da tumore faringeo . 
i pazienti , 65 maschi e 45 femmine presentavano unet media di 57 , 4 anni e , in tutti i casi , erano stati sottoposti a diverse linee di chemioterapia che erano risultate inefficaci . 
queste opzioni , tuttavia , erano gi state sperimentate visto che 15 pazienti erano gi stati sottoposti a radiofrequenza ( 3 dei quali per 3 volte ) , 3 pazienti ad alcolizzazione e 8 pazienti a transarterial chemioemobolization ( tace )  . 
al momento dello studio preliminare i pazienti si sono presentati con uno score eastern cooperative oncology group ( ecog ) medio di 0 , 7 [ 14 ]  . prima di essere sottoposti al trattamento tutti i pazienti hanno ricevuto le informazioni riguardo la procedura ed i rischi connessi ad essa , inclusi gli effetti collaterali , e hanno firmato un consenso informato che ci ha consentito di effettuare il trattamento . 
la selezione stata basata sullinclusione di pazienti che erano gi stati sottoposti a una prima linea di chemioterapia tra cui il folfox ( acido folinico , fluorouracile , oxaliplatino ) , una seconda linea tra cui il folfiri ( acido folinico , fluorouracile , irinotecan ) e da una terza linea di chemioterapia che erano risultate inefficaci per il trattamento della neoplasia primitiva . 
 la tc e la fdg - pet consentono di utilizzare il metodo di ct and fdg - pet imaging allow utilisation of the dose calculation method based on body surface area ( bsa ) , which indicates the required activity for treatment and provides a map of the tumour spread in the liver segments . the typical activity during infusion is around 50 bq / microsphere . 
on the day of the treatment , the patient , without sedadosimetria radiol med ( 2010 ) 115 : 619633 tion , was administered the dose of microspheres by a slow , manually controlled injection lasting on average 20 min , through selective catheterisation of the hepatic artery performed with a 3 - fr progreat ( terumo ) microcatheter . treatment planning patients selected for treatment underwent celiac - selective angiography with a transbrachial approach and 4 - fr sheath ( terumo ) to enable discharge within hours of the procedure . selective angiography was useful for evaluating the vascular anatomy of the liver . 
during selective catheterisation , branches of the hepatic artery , such as the gastroduodenal artery and the right gastric artery , were embolised by using 210 - mm and 220 - mm microcoils ( target vascular boston scientific ) to prevent reflux of y - 90 at the gastric and duodenal levels . 
after the procedure , a dose of 150 mbq of tc - 99m macroaggregated albumin ( maa ) was administered through the catheter to evaluate the arteriovenous shunt of the hepatic arterial system to that of the pulmonary arterial system and / or gastrointestinal venous system [ later verified by single - photon - emission computed tomography ( spect ) study performed in the nuclear medicine department ]  . 
this study permits evaluation of possible undesired directions of the y - 90 microspheres , which have approximately the same dimensions as the marked albumin particles . in consideration of lesion number , site and size , we performed a whole - liver treatment ( generally performed in the early phase of our experience in patients with multiple , extensive bilobar lesions > 5 cm in size ) , a lobar treatment ( in the case of single - lobe involvement ) or attempted a treatment of one lobe ( generally the right lobe ) followed by treatment of the other lobe 10 weeks later ( sequential treatment , performed in the most recent phase of our experience in patients with liver involvement < 25% )  . in the event of retreatment , the study procedure was repeated in all patients to assess possible changes in hepatic vascularisation due to the radioembolisation treatment . criteria for retreatment were based on evaluation of imaging at 8 weeks , and in cases of disease progression , partial response or stable disease stage , retreatment was performed . tumour response tumour response was evaluated both by alterations in tumour marker levels and by ct imaging and were defined according to the response evaluation criteria in solid tumours ( recist ) , as follows : complete response ( cr ) : disappearance / remission of disease ; confirmed at 4 weeks partial response ( pr ) : reduction of tumour by 30% ; confirmed at 4 weeks calcolo della dose tramite la formula body surface area ( bsa ) che indica lattivit richiesta per il trattamento e fornisce una mappa della diffusione tumorale nei segmenti da trattare . 
il giorno del trattamento , senza alcuna sedazione , la dose di microsfere stata somministrata mediante iniezione lenta eseguita manualmente con una durata media di circa 20 minuti attraverso cateterismo selettivo dellarteria epatica effettuato mediante microcatetere progreat 3 fr ( terumo )  . 
 pianificazione del trattamento i pazienti selezionati sono stati sottoposti ad unangiografia selettiva del tripode celiaco , mediante accesso transbrachiale , utilizzando introduttori da 4 french ( terumo ) al fine di ottenere la dimissione a poche ore dalla procedura . 
durante il cateterismo selettivo , branche dellarteria epatica come larteria gastroduodenale e larteria gastrica destra sono state embolizzate mediante microspirali 210 mm e 220 mm ( target vascular , boston scientific ) per prevenire leventuale reflusso di y - 90 a livello gastrico e duodenale . 
alla fine della procedura , attraverso il catetere posizionato selettivamente in arteria epatica comune , veniva somministrata una dose di 150 mbq di tecnezio ( tc ) - 99 in maniera da ottenere , tramite uno studio di tomografia computerizzata a emissione di fotoni singoli ( spect ) , eseguito successivamente nel reparto di medicina nucleare , il valore dello shunt artero - venoso dal sistema arterioso epatico a quello polmonare o a quello venoso gastrointestinale . 
questo studio permette di valutare possibili indesiderate direzioni delle microsfere di y - 90 dal momento che esse presentano approssimativamente le stesse dimensioni delle particelle di albumina marcata . in considerazione del numero , della sede e delle dimensioni delle lesioni il trattamento veniva mirato su tutto il fegato ( trattamento whole liver , generalmente eseguito nella prima fase della nostra esperienza in pazienti con multiple lesioni di dimensioni > 5 cm a distribuzione bilobare plurisegmentaria ) , su un solo lobo ( trattamento lobare , in caso di coinvolgimento di un singolo lobo epatico ) o si procedeva a trattare un lobo epatico ( generalmente il destro ) e , dopo 10 settimane , si ripeteva la procedura sullaltro lobo epatico ( trattamento sequenziale , adottato nella fase pi recente della nostra esperienza in pazienti con coinvolgimento epatico < 25% )  . 
 nei casi in cui il trattamento stato ripetuto , la procedura di studio preliminare stata eseguita nuovamente in tutti i pazienti al fine di valutare eventuali cambiamenti indotti nella vascolarizzazione epatica da parte del trattamento radioembolizzante . 
 624 radiol med ( 2010 ) 115 : 619633 stable disease ( sd ) : no aspects of pr or pd progressive disease ( pd ) : 20% increase in tumour ; absence of cr , pr and sd documented before disease progression follow - up was programmed at 8 and 12 weeks with ct risposta tumorale and pet imaging . statistical analyses average survival rates and rates of disease progression were evaluated according to the kaplanmeier analysis model . the same model was also used for comparative analysis between the largest groups , i.e. 
technical success and efficacy at 3 months were also assessed . complications and adverse effects were recorded and evaluated according to the common terminology criteria for adverse events ( ctcae )  . results on the day of treatment , patients underwent selective radioembolisation with a whole - liver ( 49 patients ) , lobar ( 15 patients ) or sequential ( 45 patients ) infusion . 
attivit media emessa , 1 , 65 trattamento totale la risposta tumorale stata valutata sia dalle modificazioni nei livelli dei markers tumorali che dallimaging tc e definita secondo i criteri response evaluation criteria in solid tumors ( recist ) sul seguente modello : riposta completa ( cr ) : scomparsa di malattia ; conferrisposta parziale ( pr ) : diminuzione del 30% ; confermata mata a 4 settimane ; a 4 settimane ; malattia stabile ( sd ) : non criteri di pr n di pd ; malattia progressiva ( pd ) : aumento del 20% ; assenza di cr , pr o sd documentate prima della progressione della malattia . il follow - up stato programmato a 8 e 12 settimane tramite controlli tc e pet . metodologia statistica sono state valutate le percentuali di sopravvivenza medie e la progressione libera da malattia dei nostri pazienti secondo lanalisi kaplan - meier . 
stata effettuata , tramite la medesima metodica di analisi , una comparazione tra i due gruppi pi rappresentati , ovvero i pazienti affetti da tumore colo - rettale e da tumore mammario . 
le complicanze e gli effetti collaterali sono stati determinati e valutati secondo i criteri common terminology criteria for adverse events ( ctcae )  . risultati dose radiante la dose media somministrata stata di 1 , 64 gbq ( tabella 1 )  . 
come riassunto dalla tabella 1 , in 25 pazienti stato eseguito un trattamento selettivo lobare , 65 un trattamento mirato su tutto il fegato e 20 pazienti un trattamento sequenziale del lobo destro seguito dal trattamento del lobo sinistro , eseguito a distanza di 10 settimane per ridurre il rischio di indurre una condizione di tossicit epatica acuta . i trattamenti whole liver sono stati eseguiti prevalentemente nella prima fase della nostra esperienza in pazienti affetti da metastasi bilobari , mentre recentemente la procedura preferenziale risultata linfusione sequenziale al fine di somministrare dosi di impianto lobare pi elevate riducendo la possibilit di indurre un danno epatico radioindotto sul restante parenchima . coinvolgimento epatico il coinvolgimento epatico stimato , calcolato sulla base della pet e della tc risultato inferiore al 25% in 61 pazienti , tra il 25% ed il 50% in 38 pazienti e maggiore del 50% in 11 pazienti . 
in 18 pazienti la tc mostrava una diffusione radiol med ( 2010 ) 115 : 619633 treatment , and 65 patients underwent whole - liver treatment . twenty patients were subjected to a sequential treatment of the right lobe , followed by treatment of the left lobe 10 weeks later to reduce the risk of acute hepatic toxicity . whole - liver treatments were performed prevalently in patients affected by bilobar metastases during the first stage of our experience . 
however , more recently , the preferred procedure has been sequential infusion , which enables administration of higher lobar doses while reducing the possibility of radioinduced hepatic damage on surrounding parenchyma . hepatic involvement the estimated hepatic involvement , calculated using pet and ct imaging , was < 25% in 61 patients , between 25%50% in 38 patients and > 50% in 11 patients . 
in particolare nei pazienti affetti da tumore colorettale in 25 pazienti i livelli di cea risultavano < 2 , 5 g / l ed in 16 inferiori a 2 , 0 g / l . 
il valore medio del livello di cea nei nostri pazienti corrispondeva a circa 4 , 2 g / l prima del trattamento ed a 2 , 1 g / l dopo il trattamento . nei pazienti che hanno eseguito un trattamento sequenziale durante la procedura selettiva sul lobo sinistro stato possibile valutare la captazione contrastografica del lobo destro trattato . 
the median cea level among our patient cohort was 4.2 g / l before treatment and 2.1 g / l after treatment . contrast uptake of the treated right lobe was evaluated in patients who had undergone sequential treatment during the selective procedure of the left lobe . 
i pazienti sono deceduti per progressione della malattia e , in 15 casi , sono state documentate diffusioni extraepatiche della malattia , in particolare a livello polmonare ( 8 pazienti ) e cerebrale ( 7 pazienti )  . 
langiografia eseguita prima del trattamento a destra mostra la presenza di multiple metastasi ipervascolarizzate ( a ) mentre langiografia eseguita prima del trattamento del lobo sinistro mostra lassenza di captazione contrastografica delle lesioni ( b )  . radiol med ( 2010 ) 115 : 619633 fig . 
the survival rate at 241 days in patients affected by colorectal cancer was 87% . at 350 and 400 days , it was 55% and 17% , respectively . breast cancer survival at 241 days was 96% . 
the estimated technical efficacy at 3 months was 83.6% , considering that in 18 subjects , the disease did not benefit from the treatment . complications complications and adverse effects were assessed according to ctcae : immediate complications : moderate abdominal pain and nausea were observed in 78 patients 12 h after the procedure . 
these symptoms were treated with medical therapy . early complications : grade 2 cholecystitis was observed in three patients 25 days after the procedure and was treated by medical therapy . late complications : six patients developed grade 2 gastritis 47 weeks after the procedure and were all treated with medical therapy . one patient treated in the initial stage of our experience developed hepatic failure 40 days after treatment , probably caused by radioinduced hepatitis . 
there were no complications related to the transbrachial examination procedure . discussion clinical experience demonstrates that secondary hepatic lesions evolve much more rapidly than neoplastic lesions in other sites , and for this reason , they play a fundamental role in determining the prognosis of patients affected by metastatic liver disease [ 5 ]  . 
the first study concerning the treatment of hepatic metastases with y - 90 microspheres in patients affected by colorectal neoplasms was published in 1967 by ariel [ 15 ]  . 
the average dose administered in these studies corresponded to 3.7 gbq and was well tolerated by the liver [ 16 ]  . over the following decades , several authors published their experiences with both glass and resin microspheres [ 1726 ]  . 
 un paziente trattato nella prima fase della nostra esperienza ha sviluppato uninsufficienza epatica a 40 giorni dal trattamento probabilmente determinata da un epatite radioindotta . complessivamente dunque sono state osservate una complicanza maggiore legata allinsufficienza epatica e 9 complicanze minori dovute a 6 gastriti di grado 2 ed a 3 colecistiti di grado 2 . 
non sono state osservate complicanze in seguito alla procedura di studio trans - brachiale . discussione lesperienza clinica dimostra che le lesioni secondarie epatiche progrediscono molto pi rapidamente rispetto ad altre localizzazioni di malattia neoplastica e , per questa ragione , ricoprono un ruolo fondamentale nel determinare la prognosi dei pazienti affetti da malattia metastatica del fegato [ 5 ]  . 
uno dei primi studi relativi al trattamento delle metastasi epatiche mediante y - 90 - microsfere in pazienti affetti da neoplasia colorettale stato pubblicato nel 1967 da ariel [ 15 ]  . 
lo sviluppo delle theraspheres ( vetro ) e delle sirspheres ( resina ) alla fine degli anni 80 ha contribuito a risvegliare linteresse per questo trattamento . i miglioramenti delle metodiche di imaging e della programmazione pre - trattamento mediante albumina marcata con tecnezio si sono rivelati di estrema utilit nella gestione di eventuali complicanze ed hanno fatto incrementare lutilizzo sia delle microsfere di resina che delle radiol med ( 2010 ) 115 : 619633 avoid this therapeutic option . 
among patients with primary colon cancer ( 47 cases ) , cr / pr was achieved in 46% , which is in contrast with the results of two recent studies by kennedy et al . 
however , the average survival rate of patients affected by primary colon cancer was 304 days in our experience , in line with the 315 days reported by jackobs et al . this apparently contradictory fact is explained by the heterogeneity of our cohort , which was composed of patients with advanced disease with hepatic involvement > 50% treated early on in our experience and patients treated later on with disease involvement < 25% . 
a future prospective study based on the exclusion of patients with hepatic involvement of > 25% could help clarify this point . similar considerations emerge from the analysis of patients with primary breast cancer . 
however , as noted for patients with primary colon cancer , the limited homogeneity of our cohort produced higher rates of pd compared with these two previous studies as a result of the advanced stage of hepatic disease at the time of treatment in patients who underwent radioembolisation in the initial phase of our experience . 
in microsfere di vetro nella pratica clinica producendo dei risultati incoraggianti . nella nostra esperienza una percentuale significativa di pazienti ( 40 , 9% ) ha mostrato una cr / pr secondo i criteri recist . 
nei pazienti con tumore primitivo del colon ( 47 casi ) la percentuale dei pazienti con cr / pr stata del 46% un dato che si discosta da quelli pubblicati in due recenti studi di kennedy et al . 
fatta eccezione per i primi casi infatti , nei quali la terapia stata effettuata in regime di salvage setting , i pazienti sono giunti alla nostra osservazione con un coinvolgimento epatico < 25% . 
tuttavia la sopravvivenza media dei pazienti affetti da tumore primitivo del colon riscontrata nella nostra esperienza ( 304 giorni ) non si discosta con quella pubblicata da jackobs et al . 
tale dato , apparentemente contradditorio , spiegabile con una scarsa eterogeneit del nostro campione , essendo esso composto da pazienti con malattia avanzata e coinvolgimento epatico talvolta > 50% trattati nella prima fase della nostra esperienza e da pazienti trattati successivamente con una compromissione , come gi descritto , < 25% . 
ci spiegherebbe anche la percentuale di pazienti con sd ( 34% ) , nettamente inferiore a quelle descritte in recenti studi [ 2729 ]  . sarebbe opportuno a tal fine condurre prospetticamente uno studio basato sul criterio di esclusione dal trattamento per pazienti con coinvolgimento > 25% . analoghe considerazioni emergono dallanalisi dei dati relativi alle pazienti affette da tumore della mammella . 
le nostre percentuali di cr / pr , sd e pd , rispettivamente del 44% , 34% e 22% , appaiono differenti se confrontate con quelle pubblicate da coldwell et al . 
la scarsa eterogeneit del campione ha prodotto percentuali pi elevate di pd rispetto ai due studi citati , in virt dello stadio avanzato della malattia epatica presente al momento del trattamento delle pazienti sottoposte a radioembolizzazione nelle primissime fasi della nostra esperienza . 
tuttavia , in accordo con la strategia terapeutica descritta per i pazienti affetti da tumore primitivo del colon , le pazienti che 630 radiol med ( 2010 ) 115 : 619633 agreement with the therapeutic strategy adopted in patients with primary colon cancer , currently treated patients usually have hepatic involvement < 25% . 
improved sensitivity may be achieved by using fdg - pet or functional magnetic resonance imaging ( fmri ) with diffusion - weighted sequences as a part of the protocol to evaluate tumour response [ 11 , 35 , 36 ]  . 
in their experience , patients with an ecog score of 0 showed an average survival rate of 731 days against 137 days of patients with an ecog score > 0 . this trend appears transversal and independent of primary tumour type and appears statistically significant to the point of considering the ecog score > 0 as a negative prognostic factor . 
 [ 37 ] , reductions of cea levels > 30% compared with the initial value are correlated to a significant increase in the survival rate , in particular when the radioembolisation is followed by intraarterial chemotherapy [ 37 ]  . 
 [ 28 ] provide analogous data that state that the average survival rate of patients with a cea reduction was 19.1 months against the 12.3 months of average survival of patients treated , even though some of these patients presented extrahepatic spread of disease [ 29 ]  . the most frequent complications observed were related vengono attualmente trattate mostrano un grado di coinvolgimento epatico solitamente < 25% . 
 significativo a tal proposito evidenziare il caso di una paziente con tumore mammario primitivo e coinvolgimento epatico del 15% circa , trattata mediante radioembolizzazione epatica come prima linea terapeutica congiuntamente alla linea di chemioterapia ed attualmente in follow - up . per contro , sato et al . 
ci si verifica in virt di svariate modificazioni peri ed intratumorali indotte dalla radioembolizzazione mediante y - 90 quali ledema peritumorale , lemorragia ed il potenziamento contrastografico periferico che impediscono di osservare una oggettiva riduzione dimensionale delle lesioni [ 34 ]  . 
al fine di incrementare la sensibilit nella valutazione della risposta tumorale dunque particolarmente raccomandato che la fdg - pet o la risonanza magnetica nucleare ( rmn ) funzionale ( tramite sequenze pesate in diffusione ) vengano eseguite nel contesto di un protocollo di valutazione della risposta [ 11 , 35 , 36 ]  . ai fini di una valutazione prognostica dei pazienti trattati necessario considerare due fondamentali parametri : il performance status e le variazioni dei livelli dei markers tumorali . 
 [ 32 ] i pazienti con uno score ecog di 0 mostrano una sopravvivenza media di 731 giorni contro i 137 giorni dei pazienti con uno score ecog > 0 . 
questa tendenza appare trasversale ed indipendente da tipo di tumore primitivo ed appare statisticamente significativa a tal punto da far ritenere uno score ecog > 0 come un fattore prognostico negativo . 
laltro fondamentale parametro il cui monitoraggio fornisce rilevanti informazioni prognostiche rappresentato dai markers tumorali . nei pazienti affetti da tumore primitivo del colon i livelli di cea appaiono molto indicativi della risposta della malattia . 
 [ 37 ] riduzioni dei livelli del cea > 30% rispetto al valore iniziale sono correlati a significativi incrementi della sopravvivenza , in particolare quando la radioembolizzazione viene seguita dalla chemioterapia intraarteriosa [ 37 ]  . 
 [ 28 ] forniscono dati analoghi stimando che la sopravvivenza media dei pazienti con diminuzioni del cea , sebbene alcuni di questi radiol med ( 2010 ) 115 : 619633 to microsphere damage to the gastrointestinal tract . 
approximately two thirds of patients developed a precise clinical condition known as postembolic syndrome ( pes ) , which is frequently seen in patients who undergo embolisation with resin microspheres ( as opposed to glass microspheres , which have a lesser embolic effect )  . 
pes is characterised by asthenia , nausea , fever , epigastric pain and pain in the right hypochondrium and is sometimes associated with vomiting . all of these symptoms are temporary and can be treated effectively with medical therapy , even after discharge from hospital [ 3840 ]  . regarding outpatient management of patients who have undergone y - 90 embolisation , it is important to consider the possible exposure to radioactivity of family members or caregivers who interact with the patient . 
in a recent study , gulec and siegel noted that individuals who interact at approximately 1 m from a patient who has been administered 3 gbq of radioactivity will receive a dose of approx . 
the doses cited appear to be insignificant in the majority of cases [ 41 ]  . considering , therefore , the promising results obtained using radioembolisation with y - 90 , there are several experimental clinical trials in progress aimed at evaluating the results of a possible combination of this new therapy with different chemotherapy protocols . 
sirt can thus no longer be considered as a salvage - setting treatment option but as a first - line treatment in combination with chemotherapy . results of a meta - analysis by vente et al . 
 [ 43 ] based on 792 patients from 19 studies showed the response to radioembolisation with y - 90 [ defined as ar ( any response ) and including cr , pr , and sd ] in patients affected by primary colon cancer to be 79% in patients treated in a salvage setting as against 91% in patients also treated with combination first - line chemotherapy [ 175 patients treated with 5 - fu / leucovorin ( lv ) or floxuridine and 20 treated with folfox ] [ 43 ]  . 
 in conclusion , the results of our study confirm the effectiveness of radioembolisation with y - 90 microspheres on secondary hepatic lesions , particularly in patients with hepatic involvement < 25% . 
an ecog score of 0 and a slight reduction of tumour markers during the follow - up may be sensitive parameters for higher survival expectancy . the therapy appears to be generally well tolerated , with an acceptable rate of complications . 
further phase iii clinical trials should clearly determine the real and effective impact presentassero una diffusione extraepatica della malattia , stata di 19 , 1 mesi contro i 12 , 3 mesi di sopravvivenza media della totalit dei pazienti trattati [ 29 ]  . le complicanze legate alla radioembolizzazione con y90 di pi frequente osservazione sono determinate dagli insulti provocati dalle microsfere sullapparato gastrointestinale . 
circa due terzi dei pazienti trattati nel nostro centro ha lamentato la cosiddetta sindrome post - embolica ( pes ) , di frequente riscontro in seguito ad embolizzazione mediante microsfere in resina al contrario di quanto avviene con quelle in vetro il cui effetto embolizzante inferiore . 
 riguardo alla gestione domiciliare del paziente in un recente studio di gulec e siegel [ 41 ] si stabilisce che individui che interagiscono a circa 1 metro da un paziente a cui sono stati somministrati 3 gbq riceveranno una dose di circa 0 , 011 msv dalle prime 6 ore fino al decadimento totale . 
le dosi citate pertanto risultano insignificanti nella maggioranza dei casi [ 41 ]  . considerati dunque i risultati promettenti della radioembolizzazione con y - 90 , sono attualmente in corso diversi trials clinici sperimentali mirati a valutare i risultati dellassociazione di tale terapia con i diversi schemi di chemioterapia sistemica . 
ci significa che la sirt si propone come opzione terapeutica non pi in un salvage setting ma , in combinazione con gli schemi chemioterapici , come prima linea di trattamento . 
 [ 43 ] , la risposta al trattamento radioemblizzante con y90 , catalogata come ar ( any response ) includendo cr , pr e sd , dei pazienti affetti da tumore primitivo del colon , si attesta su una percentuale del 79% nei pazienti trattati in salvage setting contro il 91% dei pazienti trattati in prima linea combinata con la chemioterapia ( 175 pazienti trattati con 5 - fu / lv o fluxoridina e 20 pazienti con folfox ) [ 43 ]  . in conclusione , i risultati del nostro studio confermano lefficacia del trattamento radioembolizzante con y - 90 sulle lesioni secondarie epatiche , pi evidente in pazienti con coinvolgimento < 25% . 
in questi pazienti le percentuali di sopravvivenza appaiono essere significativamente maggiori . uno score ecog di 0 e da una diminuzione sensibile dei markers tumorali in corso di follow - up rappresentato parametri sensibili per unaspettativa di sopravvivenza maggiore . 
andrea delle fratte , 06156 perugia , italy 2department of radiology , radiotherapy and nuclear medicine , magrassi lanzara ii university of naples , school of medicine , 80100 naples , italy 3department of radiology and laboratory , s . 
andrea delle fratte , 06156 perugia , italy 4department of surgical , radiologic and odontostomatologic sciences , section of oncologic surgery , 5section of thoracic surgery , university of perugia , s . 
andrea delle fratte , 06156 perugia , italy 6 department of radiology , bentivoglio hospital , via marconi 35 , asl bologna , 40010 bentivoglio , bologna , italy 7department of radiology , university of molise c.da tappino , 86100 campobasso , italy 8department of radiology , budrio hospital , via benni 44 , asl bologna , 40054 budrio , bologna , italy correspondence to : m . 
scialpi , tel : + 39 - 075 - 5783507 , fax : + 39 - 075 - 5729407 , e - mail : michelescialpi@libero.it received : 4 march 2009 / accepted : 3 april 2009 / published online : 7 january 2010 springer - verlag 2010 abstract purpose . 
we retrospectively reviewed the ct scans in three institutions from august 1996 to december 2008 , of nine patients ( six men , three women ; mean age 48.6 years ; range 2675 years ) who had histological diagnosis of pulmonary cystic disease after surgery . 
abbiamo analizzato retrospettivamente gli esami tc di tre centri , da agosto 1996 a dicembre 2008 , relativi a nove pazienti ( sei maschi e tre femmine , et media 48 , 6 anni , range compreso tra 2675 anni ) trattati chirurgicamente per patologia cistica polmonare , in cui lesame istologico del pezzo operatorio ha consentito di ottenere la diagnosi definitiva : in sei pazienti cisti broncogena intrapolmonare ( cbi ) e in tre malformazione adenomatoide cistica ( mac ) di tipo i , associata in un caso a sequestro polmonare intralobare ( spi )  . 
tre pazienti erano sintomatici e sei asintomatici . allesame tc le cbi si presentavano : in due casi come lesioni completamente liquide , in due casi con livello idroaereo contestuale , in un caso come formazione completamente ripiena di aria e in un caso come formazione omogenea rispetto alla densit dei tessuti molli . 
le mac di tipo i nella forma solitaria , si presentavano luna come lesione cistica uniloculata , con livello fluido , laltra a contenuto aereo ed entrambe erano delimitate da una parete sottile con parenchima adiacente normale . 
nelladulto sempre raccomandabile la resezione chirurgica di tutte le lesioni intrapolmonari cistiche poich la mac di tipo i un precursore del carcinoma mucinoso bronchiolo - alveolare . parole chiave cisti broncogena intrapolmonare malformazione adenomatoide - cistica sequestro polmonare intralobare tomografia computerizzata introduction introduzione congenital malformations of the lower respiratory tract are usually diagnosed prenatally , in the newborn period , in infancy or in childhood . 
in the latter cases , late complications such as recurrent localized pneumonia , abscess formation and haemoptysis , or the incidental discovery on a chest x - ray may lead to a diagnosis in adolescence or adulthood . in adults , congenital cystic pulmonary malformations include intrapulmonary bronchogenic cysts ( ibc ) , cystic adenomatoid malformation ( cam ) and pulmonary sequestration . 
an accurate diagnosis is thus essential for treatment planning . published reports on the computed tomography ( ct ) findings of intrapulmonary congenital cystic lesions in adults have been limited to case reports and small series [ 24 ] , and none has compared the radiological features of ibc with those of type - i cam . the aim of this study was to correlate the pathological findings and ct features of solitary ibc in adults to establish whether ct imaging can help identify the nature la diagnosi di una malformazione congenita dellalbero respiratorio inferiore generalmente viene posta prima della nascita , nel periodo neonatale , nellinfanzia o in et giovanile . 
solo raramente laccertamento di tali anomalie avviene in et pi avanzata , nelladolescenza o in et adulta , per sopraggiunte complicanze , come polmoniti ricorrenti , ascessi ed emottisi , o per il rilievo di un reperto occasionale in corso di esami radiografici del torace o tc eseguiti per altri motivi . 
 le malformazioni cistiche congenite polmonari nelladulto comprendono la cisti broncogena intrapolmonare ( cbi ) , la malformazione adenomatoide cistica ( mac ) ed il sequestro polmonare ( sp )  . 
recentemente , la dimostrazione della mac di tipo i quale precursore del carcinoma bronchiolo - alveolare ( cba ) di tipo mucinoso , ha completamente modificato lapproccio terapeutico alle lesioni cistiche polmonari negli adulti , individuando nella resezione chirurgica il trattamento di scelta . 
three patients were symptomatic with cough and dyspnoea ( n = 1 ) , cough , dyspnoea and persistent haemoptysis ( n = 1 ) and dyspnoea , chest pain and pneumothorax ( n = 1 )  . 
 ct technique chest ct scans were obtained using a single - detector - row scanner ( advantage ave 1 , philips medical systems , best , the netherlands ) in two patients , a 4 - detector - row scanner ( lightspeed qx / i - plus , ge medical systems , milwaukee , wi , usa ; asteion , toshiba medical systems , tokyo , japan ) in five and a 8 - detector - row scanner ( lightspeed ultra , ge medical systems , milwaukee , wi , usa ) in one . 
ct scans were obtained before and after intravenous injection of an average of 120140 ml of contrast medium ( iopamiro 300 , bracco , milan , italy ) ( iopromide ultravist 320 , schering ag , berlin , germany ) at a rate of 3 ml / seconds , after a delay of 6070 s , into an antecubital vein by using an 1820 gauge needle using a power injector ( endovision ct injector , medrad , italy )  . 
singledetector - row ct scan parameters were as follows : slice thickness : 3 - mm , reconstruction interval : 1 , 5 - mm , pitch : 1 : 1 , 120 kvp and 200250 ma . 
eight - detector - row ct scan parameters were as follows : slice thickness : 2.5 - mm , reconstruction interval : 1.25 - mm , 120 kvp and 300 ma reconstruction interval : using multi - detector - row ct , table feed and collimation were adjusted to obtain a beam pitch of approximatively 1 . coronal and sagittal multiplanar ( mpr ) and maximum lo scopo del presente studio consiste nel correlare le caratteristiche isto - patologiche delle lesioni solitarie intrapolmonari cistiche congenite nelladulto con i reperti della tc , per verificare se sia possibile ottenere una corretta diagnosi preoperatoria delle diverse malattie , in riferimento alle implicazioni cliniche del potenziale carcinogenetico della mac di tipo i . 
 materiali e metodi abbiamo rivalutato retrospettivamente gli esami tc del torace eseguiti in tre diversi centri nel periodo compreso fra agosto 1996 e dicembre 2008 , relativi a nove pazienti ( sei maschi e tre femmine , et media 47 , 6 anni , range compreso tra 2675 anni ) , con diagnosi istologica formulata su pezzo operatorio di : cbi ( n = 6 ) e mac tipo i ( n = 3 ) , associata a sequestro polmonare intralobare ( spi ) in un caso . 
tre pazienti erano sintomatici con tosse e dispnea ( n = 1 ) , tosse , dispnea ed emottisi persistente ( n = 1 ) e dispnea , dolore toracico e pneumotorace ( n = 1 )  . 
in tutti i pazienti il decorso postoperatorio stato regolare . tecnica tc gli esami tc del torace sono stati ottenuti in 3 pazienti con un tomografo a singolo strato ( advantage ave 1 , philips medical system , best , olanda ) , in 5 pazienti con un tomografo a 4 slice / rotazione ( lightspeed qx / i - plus , ge medical systems , milwaukee , usa ; asteion , toshiba medical system , tokyo , giappone ) e in 1 paziente con un tomografo a 8 slice / rotazione ( lightspeed ultra , ge medical systems , milwaukee , wi , usa )  . 
in 8 pazienti gli esami sono stati eseguiti senza e dopo somministrazione endovenosa di 120150 ml di mezzo di contrasto ( mdc ) ( iopamiro 300 , bracco , milano , italia ; iopromide ultravist 320 , schering ag , berlino , germania ) , ad una velocit di flusso di 3 ml / secondo , con tempo di ritardo dallinizio delliniezione del mdc di 6070 secondi , attraverso una vena antecubitale con ago da 1820 gauge ed un iniettore automatico ( endovision ct injector , medrad , italia )  . 
parametri di acquisizione della tc a singolo strato : spessore di strato : 3 - mm , indice di ricostruzione : 1 , 5 - mm , rapporto tavolo - pitch : 1 : 1 , 120 kvp e 200250 ma . 
parametri di acquisizione della tc a 8 slice / rotazione : spessore di strato : 2 , 5 - mm , 542 radiol med ( 2010 ) 115 : 539550 intensity projection ( mip ) reconstructions to determine a better location of the cystic lesion and its relationship with adjacent vessels were performed in two cases . 
ct scans were evaluated for shape , margin characteristics ( smooth , lobulated , irregular ) , wall ( presence or absence ) , location , attenuation with respect to muscle ( lower , intermediate similar to the muscle and higher ) , homogeneity , calcifications and pattern of enhancement after intravenous administration of iodinated contrast material [ attenuation values were expressed in hounsfield units ( hu ) on both unenhanced and enhanced ct scans ] and features of the pulmonary tissue adjacent to the lesion . 
 results ct appearance intervallo di ricostruzione : 1 , 25 - mm , 120 kvp e 300 ma . con la tc multistrato , la velocit di traslazione del tavolo e la collimazione sono stati ottimizzati al fine di ottenere un beam pitch quanto pi possibile vicino a 1 . ricostruzioni multiplanari ( mpr ) e maximum intensity projection ( mip ) sagittali e coronali sono state utilizzate in due casi per meglio determinare la sede della lesione e i rapporti con strutture vascolari intraparenchimali . 
in un paziente stata impiegata la tecnica ad alta risoluzione del torace con spessore di strato di 1 - mm ed intervallo di ricostruzione di 5 - m correlazioni radiologiche - patologiche le immagini sono state analizzate utilizzando sia la finestra per parenchima polmonare che per mediastino . 
per ogni lesione sulle immagini tc sono state valutate la forma , le caratteristiche dei contorni ( lisci , lobulati , irregolari ) , la parete ( presenza o assenza ) , la localizzazione , la densit rispetto alle strutture muscolari ( ipo - , isoo iperdensa ) , lomogeneit , la presenza di calcificazioni , il comportamento dopo somministrazione endovenosa del mdc [ i valori di attenuazione sono stati espressi in unit hounsfield ( uh ) sia sulle immagini preche post - contrastografiche ] ed infine laspetto del parenchima polmonare adiacente la lesione . 
allesame istologico , nella diagnosi differenziale tra cbi e mac di tipo i , la presenza di cartilagine nella parete della cisti stato considerato il criterio diagnostico conclusivo di cbi . 
associated findings included areas of band - like linear attenuation in three cases , atelectasia in two cases and a mucocele - like area surrounded by normal lung tissue in one . 
come reperti associati alle cbi sono state evidenziate bande fibrotiche lineari in tre casi , zone di atelettasia in due casi ed una formazione simile a mucocele circondata da parenchima polmonare normale in un caso . 
lesame tc dopo somministrazione di mezzo di contrasto per vena mostra una lesione cistica adiacente il bronco principale di destra nel segmento dorsale del lobo polmonare superiore omolaterale ( a )  . 
ct shows a unilocular oval ( 3 cm in maximum diameter ) cystic lesion in the apical segment of the lower lobe and in the dorsal segment of the upper lobe of the right lung . 
5 congenital type - i cystic adenomatoid malformation in a 62 - year - old man with a history of severe emphysema and presenting dyspnoea , chest pain and pneumothorax . 
high - resolution ct of the chest shows a large , oval ( 5 cm in maximum diameter ) , air - filled lesion ( arrows ) with thin wall indistinguishable from emphysematous bullae . 
la tc ad alta risoluzione mostra una voluminosa lesione ovalare ( 5 cm di diametro massimo ) ripiena daria ( frecce ) , con pareti sottili , indistinguibile da una bolla di enfisema nel lobo polmonare superiore sinistro . 
6a - c type - i cystic adenomatoid malformation ( cam ) associated with intralobar pulmonary sequestration in a 75 - year - old man with a history of dyspnoea . 
la tc del torace mostra la mac come una formazione espansiva tondeggiante a contenuto liquido ( 4 , 5 cm di diametro ) nel lobo polmonare inferiore destro ( a )  . 
le ricostruzioni multiplanari curvilineee mostrano unarteria afferente ad origine dallaorta toracica discendente e una vena efferente in corrispondenza della lesione ( b , c )  . thick elastic laminae , confirming systemic artery configuration . 
 on preoperative ct , the lesions were interpreted as cysts ( n = 6 ) , emphysematous bulla ( n = 1 ) , solid pulmonary lesion ( n = 1 ) and ils associated with a cystic lesion ( n = 1 )  . 
 allesame tc preoperatorio , le lesioni polmonari sono state interpretate come cisti ( n = 6 ) , bolla enfisematosa ( n = 1 ) , nodulo solitario ( n = 1 ) e spi associato con lesione cistica ( n = 1 )  . 
allesame istologico dopo la completa resezione chirurgica delle lesioni , sei erano cbi e tre mac di tipo i di cui una associata a spi . 546 radiol med ( 2010 ) 115 : 539550 discussione la malattia polmonare cistica congenita per definizione indica genericamente ogni lesione polmonare cistica ritenuta essere presente alla nascita [ 5 ]  . 
 nel nato morto , nel neonato e nellinfanzia , latresia bronchiale pu essere associata a sequestro polmonare ( sp ) e , con elevata frequenza , a mac di tipo i [ 7 , 8 ]  . nelladulto queste anomalie polmonari congenite sono rare e comprendono la cbi e la mac che possono associarsi a sp . 
tale malformazione , classificata sulla base delle dimensioni delle cisti evidenti allesame macroscopico e dei reperti istologici in tre tipi [ 10 ] , viene diagnosticata frequentemente nel periodo neonatale e nel 90% dei casi entro i primi 2 anni di vita [ 10 , 11 ]  . 
 [ 1 ] hanno dimostrato che nella mac tipo i la proliferazione mucinosa localizzata in sede intrao extracistica contiene lo stesso profilo di differenziazione del carcinoma bronchiolo - alveolare ( cba ) mucinoso . la mac di tipo i pu quindi essere considerata un precursore pre - neoplastico ed pi frequentemente associata a cba nellet adulta [ 1 , 1217 ] rispetto allinfanzia [ 1821 ]  . 
 stata riportata anche lassociazione tra cba e cbi [ 22 ] , ma , poich il profilo di differenziazione corrispondente al cba mucinoso non stato descritto , la cbi non considerata un precursore pre - neoplastico . 
la broncografia non aggiunge ulteriori informazioni ai reperti tc [ 23 ]  . in letteratura i criteri tc per la diagnosi di cbi sono i seguenti : lesione con coefficiente di attenuazione di tipo liquido con parete sottile liscia e ben definita , lesione di aspetto omogeneo con coefficiente di attenuazione dei tessuti molli ed infine , lesione che non si modifica dopo somministrazione del mezzo di contrasto ( mdc ) [ 2 , 3 ]  . 
7 listologia della parete di una cisti rivela le caratteristiche tipiche di una cisti broncogena con pareti rivestite da epitelio ciliato , contenenti cartilagine e ghiandole siero - mucose bronchiali ( ingrandimento , 100 ; colorazione con ematossilina - eosina )  . 
 into the following categories : ( a ) those assumed to be congenital [ intrapulmonary broncogenic cyst ( ibc ) , cystic adenomatoid malformation ( cam ) , bronchial atresia , lobar emphysema and ( ils ) and extralobar sequestration ( els ) ] and ( b ) those assumed to be acquired ( bronchiolitis obliterans with air trapping , bronchiectasis and abscess ) [ 6 ]  . 
 intralobar sequestration in the stillborn , the newborn and in childhood , bronchial atresia may be associated with pulmonary sequestrations and cam in a higher frequency [ 7 , 8 ]  . 
these malformations probably share a common embryogenesis due to aberrant genes , despite a different morphology [ 9 ]  . the stocker classification [ 10 ] categorizes cam by the size of the cysts on gross examination and by histological findings into three types . 
cam is most commonly found in the neonatal period , and up to 90% of cases are reported within the first 2 years of life [ 10 , 11 ]  . 
 the reported ct criteria for the diagnosis of ibc are the following : water attenuation with a well - defined , thin , smooth wall , or homogeneous soft - tissue attenuation that does not enhance following administration of contrast material [ 2 , 3 ]  . 
in solitary ibc cases , histological examination revealed fibrosis in the adjacent lung tissue ( corresponding to radiological band - like linear opacities ) in three cases , atelectasia in two cases and atelectasia associated with a mucocele - like area in one case . 
there may be areas of enhancement after intravenous contrast injection , corresponding to the wall of smaller cystic lesions [ 2527 ]  . in our study , ct was unable to distinguish ibc from type - i cam . 
8 lesame istologico della parete di una malformazione adenomatoide - cistica di tipo i mostra epitelio ciliato pluristratificato , bronchioli ectasici ed infiltrato linfocitario ( ingrandimento originale , 100 ; colorazione con ematossilina - eosina )  . attenuazione ed aree di attenuazione lineare nastriforme nel contesto del parenchima polmonare adiacente . 
associata alla cbi , lesame istologico rilevava nel tessuto polmonare adiacente in tre casi la presenza di fibrosi , in due di atelettasia ed in un caso di aree similmucocele circondate da tessuto polmonare . in nessun caso sono stati rinvenuti aggregati di cellule mucinose . 
allesame tc , le mac di tipo i si presentano come formazioni cistiche con pareti sottili , unio multiloculari , del diametro maggiore di 2 cm , che possono essere ripiene di aria , di liquido , o mostrare livelli idro - aerei . possono osservarsi zone di enhancement dopo somministrazione endovenosa di mdc , che corrispondono alla parete di lesioni cistiche pi piccole [ 2527 ]  . nel nostro studio , le cbi sono risultate indistinguibili dalle mac di tipo i , e in un caso , una cbi con densit dei tessuti molli alla tc stata interpretata come nodulo . 
tale reperto , espressione del muco e dei detriti proteinacei allinterno della cisti , pu essere agevolmente diagnosticato 548 radiol med ( 2010 ) 115 : 539550 lesion was erroneously interpreted as a solid lesion on ct . this finding suggests mucus and proteinaceous debris within the cyst and can be confidently diagnosed by magnetic resonance imaging [ 3 , 28 ]  . 
ils may be associated with ibc , and this association implies that ils is a congenital malformation and not an acquired lesion resulting from recurrent infections [ 30 , 31 ]  . ct is the method of choice for evaluating parenchymal abnormalities in bronchopulmonary sequestration [ 3235 ]  . this most commonly appears as a homogeneous or inhomogeneous solid mass with or without definable cystic changes . 
an aggregate of multiple small cystic lesions with air or fluid content , a well - defined cystic mass or a large cavitary lesion with airfluid levels may also be present . 
in our case , the ct diagnosis of cystic ils was made on the basis of the demonstration of arterial supply from the descending thoracic aorta and venous drainage via the pulmonary veins in correspondence with the cystic lesion in right lower lobe . 
in fact , an imaging diagnosis of ils associated with a unilocular cystic lesion is possible , but the origin of the cyst can only be established with the histological examination . the limitation of our study is the small number of cases , but in the adult , solitary pulmonary cystic malformations are very rare , and histological documentation was not always available for the reviewed studies . 
consequently the histological and radiological correlations of the lesions should be well understood , even with small series , to better understand the oncogenetic potential of intrapulmonary congenital cystic disease in the adult . the similarity in ct and histopathology findings across the spectrum of non - neoplastic congenital cystic lung mediante risonanza magnetica [ 3 , 28 ]  . 
la possibile associazione con cbi o , pi raramente , con mac , ne conferma la natura congenita , escludendo quella acquisita , dovuta ad infezioni ricorrenti [ 30 , 31 ]  . la tc rappresenta la metodica di scelta nella dimostrazione delle anomalie parenchimali del spi [ 3235 ] , che si presenta pi frequentemente come una massa solida omogenea o non omogenea , con o senza evidenti modificazioni cistiche . 
in questultimo caso , pu evidenziarsi come una massa cistica ben definita o come ampia lesione cavitaria con livello idro - aereo o , pi raramente , come un aggregato , talora voluminoso , di piccole lesioni cistiche ( voluminosa massa multicistica ) con contenuto aereo o fluido [ 36 ]  . 
nel nostro caso , la tc ha permesso la diagnosi di spi cistico mediante la dimostrazione dellarteria e della vena in corrispondenza di una lesione cistica localizzata nel lobo polmonare inferiore destro . 
la tc non consente di stabilire la natura di una lesione cistica presente in un spi e pertanto in questi casi , nella diagnosi differenziale , devono essere considerati i vari aspetti delle malattie cistiche polmonari congenite nelladulto ( cbi e mac di tipo i )  . 
 sino ad oggi nella letteratura anglosassone sono stati riportati 41 casi di sp associata a mac a localizzazione prevalentemente nei lobi inferiori [ 10 , 3751 ] , come pure aspetti rari di spi rappresentati da una voluminosa massa multicistica [ 36 ]  . 
in realt la diagnosi radiologica di spi associato a lesione cistica uniloculare possibile , ma lorigine delle cisti pu essere stabilita solo con lesame istologico . il limite del presente studio costituito dal numero esiguo dei casi . 
di conseguenza le correlazioni istologiche e radiologiche di queste lesioni dovrebbero essere ben conosciute , con riferimento anche a casistiche esigue , al fine di comprendere il potenziale oncogenetico della malattia intrapolmonare cistica congenita nelladulto . 
to assess the reproducibility of total volume ( v ) , volume of emphysema ( ve ) and emphysema index ( ei ) , intraand interobserver differences of those measurements were assessed . 
la riproducibilit del volume totale ( v ) , denfisema ( ve ) e dellindice denfisema ( ei ) stata valutata calcolando le differenze intraed inter - osservatore tra le misurazioni . 
sui singoli lobi , lanalisi volumetrica presenta maggiore variabilit . ai fini dellapplicazione clinica , limpiego di software per radiol med ( 2010 ) 115 : 516525 keywords computed tomography density quantitative evaluation pulmonary emphysema reproducibility la segmentazione automatica potr fornire valori di riproducibilit migliori per la volumetria mdtc quantitativa lobare . 
in patients with lung cancer , postoperative lung function can be estimated by quantifying the ratio between the volume of parenchyma to be resected and residual lung volume [ 1 , 2 ]  . 
similarly , in advanced pulmonary emphysema , postoperative lung function can be predicted by estimating the volume of parenchyma to be treated with lung volume reduction surgery [ 37 ]  . 
with the recent introduction of bronchoscopic lung volume reduction techniques using endobronchial valves [ 8 , 9 ] , pulmonary volumetry has been also proposed for defining the lobe to treated and quantifying the effects of treatment [ 10 , 11 ]  . 
the percentage distribution of the densities of selected voxels can be represented on a histogram and a density range of 1024 / 950 hu can be used to estimate the relative fraction of emphysema . 
a number of factors such as the type of ct scanner , technical parameters used for imaging , depth of breath - hold , skill and experience of the operator performing the analysis and software used for numerical evaluations , are potentially involved in the variability of q - mdct volume estimations . 
nei pazienti con tumore polmonare , la funzionalit respiratoria post - operatoria pu essere stimata quantificando il rapporto tra il volume del parenchima da resecare con la lesione ed il volume del parenchima residuo [ 1 , 2 ]  . 
analogamente , nel trattamento dellenfisema polmonare avanzato la stima del volume parenchimale da sottoporre a chirurgia riduttiva pu essere utile per predire la funzione post - operatoria [ 37 ]  . 
con la recente introduzione delle tecniche di riduzione volumetrica broncoscopica attraverso luso di valvole endobronchiali [ 8 , 9 ] , la volumetria polmonare stata anche proposta per definire il lobo da trattare e quantificare gli effetti della terapia [ 10 , 11 ]  . 
la volumetria polmonare pu essere ottenuta impiegando metodiche radiologiche quali la tomografia computerizzata multidetettore ( mdtc )  . dallacquisizione volumetrica ottenibile con gli apparecchi mdtc , applicando soglie densitometriche predefinite , si possono isolare i voxel che rappresentano il parenchima polmonare [ 12 ]  . 
listogramma della distribuzione percentuale delle densit dei voxel selezionati consente di stimare la percentuale relativa di enfisema , restringendo la misurazione al range di densit di 1024 / 950 unit hounsfield ( hu )  . 
rispetto ai test funzionali , tuttavia , la q - mdtc ha il vantaggio potenziale di poter fornire stime volumetriche regionali [ 14 ]  . ai fini di una applicazione clinica , la dimostrazione della riproducibilit dei risultati di una metodica diagnostica fondamentale [ 1921 ]  . 
di fatto , lapparecchio utilizzato , i parametri tecnici di studio , il grado di apnea del paziente , la manualit e lesperienza delloperatore che esegue le analisi nonch il software impiegato per le valutazioni numeriche comportano una variabilit nelle stime volumetriche q - mdtc . 
tuttavia , nel monitoraggio degli effetti di un 518 radiol med ( 2010 ) 115 : 516525 the effects of therapies that are increasingly targeted to single diseased pulmonary lobes , one needs to know to what extent the differences between initial and follow - up assessments are effectively due to treatment or intrinsically related imaging modality . 
the aim of this study was therefore to quantify interand intraobserver variability of q - mdct numerical estimates of global and lobar total and emphysematous parenchyma . lung volumes of trattamento sempre pi mirato alla patologia dei singoli lobi polmonari , rilevante sapere quanto le differenze tra una valutazione precedente ed una di follow - up sono effettivamente dipendenti dalla terapia e quanto sono intrinsecamente legate alla metodica . 
ad oggi , non sembrano riportati studi in letteratura che valutino la riproducibilit della q - mdtc nella volumetria lobare . abbiamo ipotizzato che una valutazione della riproducibilit delle stime q - mdtc dei volumi lobari potesse essere utile per definire meglio le potenzialit cliniche di questa metodica radiologica quantitativa . 
obiettivo dello studio stato quindi quello di quantificare la variabilit inter ed intra - osservatore delle stime numeriche q - mdtc dei volumi polmonari complessivi e lobari del parenchima totale ed enfisematoso . materials and methods materiali e metodi from the database of our institution we selected 23 mdct chest scans performed for clinical purposes and showing signs of pulmonary emphysema ( 23 patients : 16 men , 7 women ; mean age 62.7 years , range 2786 )  . 
prior to volumetric analysis , the mdct examinations were reviewed by a chest radiologist ( fm ) who identified type of emphysema ( centrilobular = 17 ; panlobular = 8 ; paraseptal = 6 ; coalescing into bullae = 8 ) , extent of lung involvement ( mild = 9 ; moderate = 5 ; severe = 9 ) , disease extent by lobe ( one lobe 6 ; two lobes 5 ; three lobes 5 ; four lobes 1 ; five lobes 6 ) and possible presence of accessory or incomplete fissures ( n = 0 )  . 
 all ct examinations were obtained from lung apices to bases using a spiral technique performed during a single breath - hold on a 16 - slice mdct scanner ( lightspeed pro 16 , ge healthcare , milwaukee , wi , usa )  . 
scanning parameters were : detector configuration 161.25 mm ; table feed 13.75 mm / s ; pitch 1.375 : 1 ; kvp 120 ; variable ma ( current modulation ) ; rotation time 0.5 s ; fov 4044 cm ; matrix 512512 pixels . 
 all examinations were transferred to a workstation ( adw 4.2 ; ge healthcare , milwaukee , wi , usa ) and a commercial clinical software was used for segmentation and quantitative analysis ( signa , ge healthcare , milwaukee , wi , usa )  . 
image analysis was performed separately by two operators ( a and m ) during two sessions held 3 months apart ( a1 , a2 ; m1 , m2 )  . 
the trachea , main bronchi , dal database del nostro istituto abbiamo selezionato 23 esami mdtc del torace eseguiti per scopi clinici ed evidenzianti segni di enfisema polmonare ( 23 pazienti : 16 uomini , 7 donne ; et media = 62 , 7 , range = 2786 )  . 
gli esami sono stati rivalutati prima della volumetria da un radiologo toracico ( fm ) , identificando il tipo di enfisema ( centrolobulare = 17 ; panlobulare = 8 ; parasettale = 6 ; con confluenza in bolle = 8 ) , il grado di coinvolgimento parenchimale ( lieve = 9 ; moderato = 5 ; severo = 9 ) , lestensione per lobi ( 1 lobo = 6 ; 2 lobi = 5 ; 3 lobi = 5 ; 4 lobi = 1 ; 5 lobi = 6 ) e leventuale presenza di scissure accessorie o incomplete ( n = 0 )  . tutti gli esami tc sono stati acquisiti con tecnica spirale dagli apici alle basi polmonari in apnea inspiratoria su apparecchio multidetettore a 16 strati ( lightspeed pro 16 , ge healthcare , milwaukee , wi , usa )  . 
i parametri di acquisizione sono stati : configurazione dei detettori = 161 , 25 mm ; velocit di spostamento = 13 , 75 mm / s ; pitch = 1 , 375 : 1 ; kvp = 120 ; ma variabile ( modulazione dellamperaggio ) ; tempo di rotazione = 0 , 5 secondi ; campo di vista ( fov ) = 4044 cm ; matrice di acquisizione = 512512 pixel . i parametri di ricostruzione sono stati : spessore di strato / intervallo = 1 , 25 / 1 , 25 mm ; algoritmo di ricostruzione ( kernel ) = bone + ( ge healthcare )  . gli esami sono stati trasferiti su una workstation ( adw 4.2 , ge healthcare , milwaukee , wi , usa )  . 
lanalisi delle immagini stata condotta separatamente da due operatori ( a e m ) in due sessioni a distanza di tre mesi luna dallaltra ( a1 , a2 ; m1 , m2 )  . 
la trachea , radiol med ( 2010 ) 115 : 516525 colon , esophagus , and ct table were manually deleted by using the graphic tools of the software ( region - growing and curved - line delimitation )  . 
the left lung was manually excluded from the global volume to obtain parameters for the right lung and vice versa ( vr , ver , eir ; vl , vel , eil )  . 
following the course of the fissures in the sagittal plane from periphery to hilum , virtual cutting planes were applied at a depth of 5 mat intervals of 5 mm , the operators modified the cutting plane manually to progressively exclude voxels outside the identified lobe . this procedure was used to calculate the parameters for each lobe ( right upper lobe : vrul , verul , eirul ; right middle lobe : vrml , verml , eirml ; right lower lobe : vrll , verll , eirll ; left upper lobe : vlul , velul , eilul ; left lower lobe : vlll , velll , eilll )  . 
numerical data of repeated measurement were considered in pairs . for each parameter ( v , ve , ei ) obtained from the two lungs , each lung and single lobes , the percentage differences over the means of the two measurements were calculated , according to the bland - altman method ( % = [ measurement 1 measurement 2 ] / [ mean of the two measurements ] 100 ) [ 19 ]  . 
accuracy of repeated measurements intra - tot ; ci inter - 2 , ci intra - m , ci intra - a , ci inter - 1 ; intra - a ; le diramazioni bronchiali principali , il colon , lesofago , ed il lettino dellapparecchio sono stati cancellati manualmente utilizzando gli strumenti grafici del software ( region growing e delimitazione con linea curva )  . 
dal volume globale stato escluso manualmente il polmone di sinistra per ottenere i parametri dal polmone destro e viceversa ( vr , ver , eir ; vl , vel , eil )  . 
seguendo sul piano sagittale il decorso delle scissure dalla periferia verso lilo sono stati applicati piani di taglio con profondit di 5 mad intervalli di 5 mm , gli operatori hanno modificato il piano di taglio manualmente in modo da escludere progressivamente i voxel esterni al lobo identificato . 
utilizzando questa procedura sono stati quindi calcolati i parametri per ciascun lobo ( lobo superiore destro : vrul , verul , eirul ; lobo medio : vrml , verml , eirml ; lobo inferiore destro : vrll , verll , eirll ; lobo superiore sinistro : vlul , velul , eilul ; lobo inferiore sinistro : vlll , velll , eilll ) , impiegando complessivamente , per lintera analisi , 60 minuti per esame . i dati ottenuti sono stati tabulati su foglio elettronico ( excel 2003 , microsoft corp . , redmond , wa , usa ) ed i dati numerici delle misurazioni ripetute sono stati considerati in coppie . 
la precisione dellanalisi qmdct nei confronti inter ed intra - osservatore stata iden ( per tificata nei rispettivi valori ( ) di ciinter - tot e ciintra - tot ci molto piccoli , massima precisione , alta riproducibilit )  . results figure 1 shows an example of the comparison between lobar measurements obtained in the first and second session of analysis by the two operators in a patient with coalescing panlobular emphysema in the upper lobes . 
 results of interand intraobserver analyses are shown in nella figura 1 viene riportato un esempio del confronto tra le misurazioni effettuate sui lobi nella prima e seconda sessione di analisi dai due operatori in un paziente con enfisema panlobulare confluente nei lobi superiori . 
la maggiore discrepanza per lindice di enfisema tra i due operatori ( confronto interosservatore ) si verificata sul lobo medio . i risultati delle analisi intered intra - osservatore sono riportati nella tabella 1 . 
le misurazioni dei volumi polmonari complessivi ( v ) sono risultate molto accurate e precise ( intra - tot = 0 , 23 , 4% ) : relativamente meno accurate e precise sono inter - tot = 0 , 23 , 4% ; intra - totci inter - totci the two fig . 
rul , lobo superiore di destra ; rml , lobo medio ; rll , lobo inferiore di destra ; lul , lobo superiore di sinistra ; lll , lobo inferiore di sinistra ; a , m , i due operatori ; a1 , a2 , analisi effettuate a distanza di tre mesi dal primo operatore ; m1 , m2 , analisi effettuate a distanza di tre mesi dal secondo operatore ; ve , volume in cm3 dei voxel compresi nel range densitometrico 1024 / 950 hu ( volume di enfisema ) ; v , volume in cm3 dei voxel compresi nel range densitometrico 1024 / - 200 hu ; ei = ve / v100 . radiol med ( 2010 ) 115 : 516525 table 1 overall interobserver ( a ) and intraobserver ( b ) variability numerical values represent v , total volume ; ve , volume of emphysema ; ei , emphysema index ; global , both lungs ; rl , right lung ; ll , left lung ; rul , right upper lobe ; rml , right middle lobe ; rll , right lower lobe ; lul , left upper lobe ; lll , left lower lobe . 
see the text for details inter - tot in ( a ) and inter - totci intra - totci tabella 1 variabilit inter - osservatore ( a ) ed intra - osservatore ( b ) globali . 
nellanalisi inter - osservatore dei lobi laccuratezza risultata pi bassa di quella dei polmoni ( per i lobi , valore minimo / massimo , v : inter - tot = 2 , 7 / 12% ; ve : inter - tot = 17 , 6 / 1 , 4% ; ei : inter - tot = 17 , 1 / 5 , 2% ) e la precisione risultata nettamente inferiore ( per i lobi , valore minimo / massimo , v : ci intertot = 11 / 137 , 6% ; ei : range lobi ci inter - tot = 28 , 9 / 96 , 4% )  . complessivamente , i pi alti intervalli di confidenza lobo medio ( v : sono stati ottenuti dallanalisi del intra = 29 , 9% ; v : ci lobi , valore minimo / massimo , v : ci intra - tot = 17 , 3 / 32 , 9% ; ei : ci intra = 10 , 6% ; ve : ci inter = 98 , 3% ; inter - tot = 13 , 3 / 98 , 3% ; ve : ci intra = 32 , 9% ; ei : ci inter = 137 , 6% ; inter = 81 , 8% )  . ve : ci intradiscussion discussione this study quantified interand intraobserver variability of numerical q - mdct estimations of global and lobar volumes of total and emphysematous lung parenchyma . whether the two lungs were considered together or separately , repeated measurements of v were accurate and precise , whereas measurements of ve and ei were relatively less accurate and precise . 
this modality has already shown a potential utility in preoperative assessment of patients with lung cancer and advanced emphysema ( surgical or bronchoscopic lung reduction with endobronchial valves )  . 
compared with commonly used lung - function tests , q - mdct offers the advantage of allowing volumetry to be applied to selected parenchymal in questo studio stata quantificata la variabilit intered intra - osservatore delle stime numeriche q - mdtc dei volumi polmonari complessivi e lobari del parenchima totale ed enfisematoso . 
considerando i due polmoni insieme o separatamente , le misurazioni volumetriche ripetute su tutto il parenchima polmonare sono risultate accurate e precise , mentre quelle sul volume e sullindice di enfisema sono risultate relativamente meno accurate e precise . laccuratezza della stime volumetriche lobari ( v e ve ) e dellindice di enfisema nellanalisi intra - osservatore risultata simile a quella delle stime condotte su tutto il polmone , mentre la precisione stata inferiore . 
nellanalisi interosservatore laccuratezza delle valutazioni lobari risultata inferiore e la precisione nettamente inferiore . lapplicabilit clinica di una metodica diagnostica dipende dalla possibilit di ottenere risultati riproducibili prescindendo dellinfluenza di fattori esterni ( per esempio , terapie ) [ 1921 ]  . 
questa metodica ha gi dimostrato infatti una potenziale utilit nella valutazione preoperatoria dei pazienti con tumore polmonare e con enfisema polmonare avanzato ( riduzione volumetrica chirurgica o con valvole endobronchiali )  . 
once the density thresholds are applied to exclude soft tissues , the trachea is easy to eliminate from the study volume , as it is separate from the two lungs . 
evaluation of volume fraction attributed to emphysema defined by the density threshold of 950 hu [ 14 ] and of the ei expressed as a percentage of v yielded a slightly lower level of accuracy and precision , even though these parameters were not influenced by any manual procedure . 
this result is explained considering that the two lungs are already separated and that elimination of one lung from the study volume does not affect the number of pulmonary voxels . 
 in analysis of lobar volume , after manual segmentation along the fissures , the accuracy of measurements repeated by the same operator ( intraobserver analysis ) was virtually identical to that of the analysis conducted on the lungs ( global or separate )  . 
considering the time interval between the two analysis sessions , compatible with a clinical follow - up setting , it is likely that the operators skill actually influenced the accuracy of the analysis . 
given that the procedure had been agreed upon in every detail prior to the analysis , manual segmentation of the lobes may have affected v and ve measurements , especially in the interoperator evaluation . 
part of this variability may be explained by the fact that for reasons of practicability and clinical applicability , segmentation was conducted on 5 - mm slices in a sagittal reconstruction plane with a thickness of 1 mm , influencing precision of the cut along the fissure . there were no segmentation difficulties due to the presence of incomplete fissures . 
moreover , compared with the lung , the smaller volume and number of voxels in each clinico , la q - mdtc offre il vantaggio di poter applicare la volumetria ad aree parenchimali selezionate . 
tuttavia , il numero di voxel coinvolti in questa procedura manuale relativamente piccolo rispetto al numero complessivo dei voxel rappresentato dai due polmoni , ed in tal senso linfluenza delloperatore sulla volumetria polmonare globale trascurabile . 
dalla valutazione della frazione di volume attribuita allenfisema definita dal valore densitometrico soglia di 950 hu [ 14 ] , ed il relativo indice percentualizzato rispetto al volume totale risultata unaccuratezza ed una precisione lievemente inferiore , pur non essendo tali parametri influenzati da alcuna procedura manuale . 
essendo i due polmoni gi separati , e considerando che la cancellazione di uno dei due polmoni dal volume di studio non interferisce con il numero di voxel polmonari , tale risultato comprensibile . dallanalisi volumetrica lobare , dopo segmentazione manuale condotta lungo le scissure , laccuratezza delle misurazioni ripetute dallo stesso operatore ( analisi intraosservatore ) stata praticamente sovrapponibile a quella dellanalisi condotta sui polmoni ( globali o separati )  . considerando il tempo intercorso tra le due sessioni di analisi , compatibile con una realt clinica di follow - up , probabile che la manualit delloperatore abbia effettivamente influito sullaccuratezza dellanalisi . 
considerato che la procedura stata concordata nel dettaglio prima dellanalisi , la segmentazione manuale dei lobi pu avere influito sulla variabilit delle misurazioni volumetriche totali e della frazione di enfisema , specie nella valutazione interoperatore . 
una parte di questa variabilit probabilmente spiegabile tendendo presente che la segmentazione , per praticit ed applicabilit clinica della procedura di analisi , stata condotta utilizzando piani di taglio di 5 mm su un piano di ricostruzione sagittale dello spessore di 1 mm , influenzando la precisione del taglio lungo la scissura . 
in other words , relatively small variations in manual segmentation of the lobes had major effects because they reflected on a similarly small volume , compared to global lung volume . 
the greatest variability between repeated measurements was noted in the middle lobe , which has a smaller volume than the other lobes . these findings seem to point to the need for a more precise segmentation technique when applying q - mdct to lobar volumes . 
inoltre , rispetto ai polmoni , il minore volume e numero dei voxel rappresentati in ogni lobo ha probabilmente amplificato le imprecisioni millimetriche della segmentazione , in quanto variazioni relativamente piccole del taglio manuale si riflettevano su un volume altrettanto piccolo rispetto al volume globale . 
elena 324 , 00161 rome , italy correspondence to : michele anzidei , tel . : + 39 - 06 - 4455602 , fax : + 39 - 06 - 490243 , e - mail : michele.anzidei@gmail.com received : 26 february 2009 / accepted : 23 april 2009 / published online : 22 february 2010 springer - verlag 2010 abstract purpose . 
for stenosis grading , accuracy , sensitivity , specificity , ppv and npv were 90% , 89% , 90% , 89% and 90% , respectively , at fp ; 95% , 95% , 95% , 95% and 95% , respectively , at ss ; and 97.5% , 95% , 100% , 100% and 95% , respectively , at cta . 
lo scopo di questo studio stato acquisire unesperienza preliminare sullutilizzo dellangiografia con risonanza magnetica ( angio - rm ) con mezzo di contrasto ( mdc ) blood pool nella valutazione del grado di stenosi e della morfologia della placca carotidea , confrontando le performance diagnostiche delle acquisizioni di primo passaggio ( pp ) ed allo stato stazionario ( ss ) con langio - tomografia computerizzata ( tc ) 64 strati e utilizzando langiografia con sottrazione digitale ( dsa ) come metodica di riferimento . 
accuratezza , sensibilit , specificit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) sono stati calcolati per le pp , ss e angio - tc . 
sono state esaminate 40 biforcazioni carotidee . per il grado di stenosi , accuratezza sensibilit , specificit , vpp e vpn sono risultati 90% , 89% , 90% , 89% e 90% al pp ; 95% , 95% , 95% , 95% e 95% allo ss ; 97 , 5% , 95% , 100% , 100% e 95% allangio - tc . 
ss e angio - tc sono radiol med ( 2010 ) 115 : 634647 evaluating plaque morphology , accuracy , sensitivity , specificity , ppv and npv were 87.5% , 89% , 86% , 85% and 90% , respectively , at fp ; 97.5% , 100% , 95% , 95% and 100% , respectively , at ss ; and 100% , 100% , 100% , 100% and 100% , respectively , at cta . 
blood - pool contrast - enhanced mra with ss sequences allow improved diagnostic evaluation of the degree of carotid stenosis and plaque morphology compared with fp and is substantially equal to cta and dsa . keywords atherosclerosis arteries stroke carotid risultati superiori al pp nella valutazione della stenosi ( p < 0 , 05 )  . 
langio - rm con mdc blood pool e sequenze ss consente uninterpretazione migliore del grado di stenosi e della morfologia della placca rispetto al pp e sovrapponibile a quella dellangio - tc e della dsa . 
 parole chiave aterosclerosi arterie stroke carotide introduction introduzione digital subtraction angiography ( dsa ) is still the reference standard in evaluating extracranial carotid artery disease to quantify the degree of carotid artery stenosis . 
with respect to cta , the routine clinical use of mra with interstitial contrast material requires a technical compromise between high spatial resolution that is vital for correct visualisation of the vessel and a rapid acquisition during the first - pass ( fp ) arterial phase [ 4 ]  . 
recent studies have shown a sensitivity of the technique ranging from 90% to 95.6% , with lower specificity levels around 75%90.3% in quantifying stenosis [ 58 ] , making improvements in accuracy necessary . 
the development of contrast media with bloodpool properties with reversible but prolonged binding to albumin could lead to a clinically relevant revolution of the conventional mra technique : intravascular permanence of these substances in the equilibrium phase of the circulation , known as steady state ( ss ) [ 9 , 10 ] , allows the scan protocol to be modified virtually without temporal limitations , thus exploiting a smaller field of view ( fov ) , increased planar resolution and providing ultrathin 3d partitions [ 11 , 12 ]  . the diagnostic performance of mra with blood - pool agents in evaluating obstructive disease of the epiaortic vessels was recently evaluated in a small patient population [ 13 ]  . 
 the aim of our study was to acquire preliminary clinical experience in applying mra with blood - pool contrast material in evaluating the degree of carotid stenosis and langiografia con sottrazione digitale ( dsa ) rappresenta ancora ad oggi il gold standard di riferimento nella valutazione della malattia carotidea extra - cranica per la quantificazione del grado di stenosi . 
lutilizzo di tecniche non invasive quali angiografia con tomografica computerizzata ( angio - tc ) ed angio - risonanza magnetica ( rm ) consente di bypassare la diagnosi mediante dsa [ 13 ]  . 
rispetto allangio - tc , lutilizzo in routine clinica dellangio - rm con mezzi di contrasto ( mdc ) interstiziali necessita di un compromesso tecnico tra lalta risoluzione spaziale indispensabile alla corretta visualizzazione del vaso ed una rapida acquisizione durante la fase arteriosa di primo passaggio ( pp ) [ 4 ]  . recenti studi dimostrano una sensibilit della metodica pari al 90%95 , 6% , con livelli di specificit relativamente ridotti , circa 75%90 , 3% , nella quantificazione della stenosi [ 58 ] , rendendo necessario un miglioramento dellaccuratezza diagnostica . 
lo sviluppo di mdc con propriet blood pool , ovvero di legame reversibile , ma prolungato , allalbumina plasmatica , potrebbe rivoluzionare in modo clinicamente rilevante le tecniche di angiorm convenzionali : la permanenza intravascolare di tali composti nella fase di equilibrio del circolo , nota come steady - state ( ss ) [ 9 , 10 ] , permette di modificare i protocolli di scansione virtualmente senza limite temporale sfruttando campi di vista ( fov ) pi piccoli , unaumentata risoluzione planare e partizioni 3d ultrasottili [ 11 , 12 ]  . 
la performance diagnostica dellangio - rm con mdc blood pool nella valutazione della patologia steno - ostruttiva dei vasi epiaortici stata recentemente valutata in una piccola popolazione di pazienti [ 13 ] ; attualmente non sono ancora disponibili dati su campioni pi vasti che permettano una 636 radiol med ( 2010 ) 115 : 634647 carotid plaque morphology and to compare the diagnostic performance with cta using dsa as the reference standard . materials and methods patient population and informed consent between november and december 2008 , we enrolled 20 patients referred from the department of vascular surgery with indications for carotid endarterectomy ( tea ) or carotid stenting . 
all patients had had one or more cerebrovascular episodes [ transient ischaemic attack ( tia ) , minor tia or stroke ] in the previous 6 months . exclusion criteria were contraindications to mra , cta or dsa ( clinical evidence of renal and / or heart failure , history of hypersensitivity to iodinated contrast media ) or previous tea or carotid artery stenting . 
all patients provided informed consent for the diagnostic procedures . contrast - enhanced mra : technology , contrast agent administration and imaging protocol all examinations were performed with a 1.5 - t system ( magnetom avanto , siemens medical system , erlangen , germany ) characterised by a gradient intensity up to 45 mt / m , a slew rate of 200 t / m / s , with total imaging matrix ( tim ) coil technology and integrated parallel acquisition technique ( ipat )  . 
the precontrast mask images were acquired in coronal planes with a 3d spoiled gradient - echo sequence optimised for high spatial resolution and short acquisition time ( time to repeat [ tr ] 3.5 ms , time to echo [ te ] 1.2 ms , flip angle [ fa ] 30 , acquisition time [ ta ] 14 s , thickness 0.7 mm , matrix 384384 , native voxel 1 mm 1 mm 0.7 mm , ipat 2 )  . 
the same sequence was repeated for fp imaging after administration of 0.03 mmol / kg of gadofosveset trisodium ( vasovist , schering , berlin , germany ) injected with an automatic injector at a rate of 1 ml / s through an 18gauge cannula placed in an antecubital vein of the right arm , followed by 15 ml of saline solution . 
 lo scopo del nostro studio stato quello di acquisire unesperienza clinica preliminare sullapplicazione dellangio - rm con mdc blood pool nella valutazione del grado di stenosi e della morfologia della placca carotidea , confrontando le performance diagnostiche con quelle dellangio - tc , utilizzando la dsa come metodica standard di riferimento . 
 materiali e metodi popolazione e consenso informato tra novembre e dicembre 2008 sono stati arruolati nel nostro studio 20 pazienti inviati dal dipartimento di chirurgia vascolare con indicazione ad intervento di endoarterectomia ( tea ) o stenting carotideo . 
i soggetti sono stati arruolati sulla base di un esame eco - color doppler preliminare che mostrava stenosi 50% dellarteria carotide interna ; tutti i pazienti avevano riferito uno o pi episodi cerebrovascolari ( attacco ischemico transitorio [ tia ] , minor tia o stroke ) nei 6 mesi precedenti . 
i criteri di esclusione sono stati : controindicazioni allangio - rm , allangio - tc o alla dsa ( evidenza clinica di insufficienza renale e / o cardiaca , storia di ipersensibilit nei confronti di mezzi di contrasto iodati ) , oppure anamnesi positiva per tea o stenting carotideo . 
tutti i pazienti hanno fornito il proprio consenso informato alle procedure diagnostiche . angio - rm con mezzo di contrasto : tecnologia , somministrazione del mdc e protocollo di imaging tutti gli esami sono stati effettuati con unapparecchiatura ad 1 , 5 t ( magnetom avanto , siemens medical system , erlangen , germania ) ( intensit dei gradienti = 45 mt / m maximum , slew rate = 200 t / m / s , con tecnologia total imaging matrix tim coil e tecnica di acquisizione integrata parallela [ ipat ] )  . 
i pazienti sono stati studiati in posizione supina con doppia bobina ( configurazione neurovascolare testa - collo : 12 + 4 elementi di ricezione )  . lo scout stato acquisito con sequenze truefast imaging with steady state precession ( fisp )  . 
le immagini maschera pre - contrasto sono state acquisite su piani coronali con una sequenza spoiled gradient - echo 3d , ottimizzata per unalta risoluzione spaziale e un breve tempo di acquisizione ( time to repeat [ tr ] 3 , 5 ms , time of echo [ te ] 1 , 2 ms , flip angle [ fa ] 30 , tempo di acquisizione [ ta ] 14 s , spessore 0 , 7 mm , matrice 384384 , voxel nativo 1 mm1 mm0 , 7 mm , ipat 2 )  . 
the scan was performed with prior placement of an 18 - gauge venous access in an antecubital vein of the right arm and after administration of 50 ml of nonionic iodinated contrast material ( iomeprol 400 mgi / ml , iomeron 400 , bracco , milan , italy ) , followed by the injection of 30 ml of saline solution at a rate of 4 ml / s with the use of a dual - head injector ( stellant d , medrad , warrendale , pa , usa )  . 
optimal delay between contrast material administration and scan initiation was evaluated with the bolus - tracking technique , with a region of interest ( roi ) placement at the level of the aortic arch and automatic triggering at 150 hu . 
a volume of 8 ml of contrast material ( iomeprol 300 , iomeron 300 , 300 mgi / ml ; bracco ) was administered at an injection rate of 6 ml / s for each carotid artery view . 
 angio - tc : tecnologia e procedura in tutti i pazienti langio - tc stata effettuata con un apparecchiatura multidetettore 64 strati ( sensation cardiac 64 , siemens medical system , erlangen , germania )  . 
la scansione stata effettuata previo posizionamento di un accesso venoso ( 18 g ) a livello della vena antecubitale del braccio destro e dopo infusione di 50 ml di mezzo di contrato iodato non ionico ( iomeprolo 400 mgl / ml , iomeron 400 , bracco , milano , italia ) seguiti da iniezione di 30 ml di soluzione salina ad un flusso di 4 ml / s per mezzo di iniettore a doppia testata ( stellant d , medrad , warrendale , pennsylvania state , usa )  . 
il ritardo ottimale tra la somministrazione del mdc e linizio della scansione stato valutato mediante tecnica di bolus - tracking con posizionamento di una regione di interesse ( roi ) a livello dellarco aortico e triggering automatico a 150 unit hounsfield ( hu )  . 
le immagini sono state acquisite con il seguente protocollo : 120 kv , 180 mas , pitch : 0 , 8 , spessore di strato : 0 , 7 mm , reconstruction increment : 0 , 5 mm , matrice 512512 , scan time : 68 secondi , kernel : b30f smooth . 
il volume di mezzo di contrasto utilizzato ( iomeprol 300 , iomeron 300 , 300 mgi / ml , bracco imaging spa , milano , italia ) stato di 8 ml somministrato alla velocit 6 ml / s per ogni proiezione carotidea . 
il campo di vista utilizzato stato di 33 / 40 cm con una matrice di 10241024 ed una risoluzione spaziale media di 0 , 320 , 32 mm . analisi delle immagini gli esami angio - rm ed angio - tc sono stati valutati da due 638 radiol med ( 2010 ) 115 : 634647 degree of stenosis and characterise vessel wall alteration morphology . 
the degree of stenosis was evaluated with the north american symptomatic carotid endarterectomy trial ( nascet ) technique [ 14 ] : i ( 1%29% ) mild stenosis , ii ( 30%49% ) and iii ( 50%69% ) moderate stenosis ; iv ( 70%99% ) severe stenosis ; v occlusion . 
plaque appearance was evaluated at the interface with the vessel lumen and was defined as irregular in the presence of small superficial irregularities and ulcerated when a deep ulcer niche with clear profiles was identified . 
dsa images were evaluated independently by a vascular radiologist , unaware of mra and cta findings , on a workstation with 2megapixel monitors ( barco n.v. , kortrijk , belgium ) equipped with a millimetric digital measurement system . data analysis findings of the image evaluation sessions were entered into a database ( excel for office 2004 , microsoft corporation , redmond , wa , usa )  . 
sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy were calculated for each of the three imaging modalities in evaluating degree of stenosis , morphology , length of the plaque and presence of ulcers and tandem lesions . 
agreement was judged to be poor for values 0.210.40 , moderate for values 0.410.60 , substantial for values 0.610.80 and excellent for values 0.811.00. results all mra , cta and dsa examinations were performed with success . 
nessuna ricostruzione , piano o proiezione sono stati ottenuti in maniera predefinita dai tecnici : le immagini sono state valutate attraverso un software client dedicato alle applicazioni cardiovascolari ( aquarius thin client , terarecon , san matteo , california , usa )  . 
non sono stati ottenuti dei piani o delle angolazioni prestabilite preliminari alle sessioni di refertazione per valutare la stenosi : i lettori hanno interagito in tempo reale con i set di dati usando ricostruzioni a massima intensit proiettiva ( mip ) per identificare il sito di stenosi ed una ricostruzione multiplanare semplice e centroluminale ( mpr e c - mpr ) al fine di quantificare il grado e la morfologia delle alterazioni parietali . 
la valutazione del grado di stenosi stata eseguita mediante misurazioni secondo north american symptomatic carotid endarterectomy trial ( nascet ) [ 14 ] : i ( 1%29% ) stenosi lieve , ii ( 30%49% ) e iii ( 50%69% ) stenosi moderata ; iv ( 70%99% ) stenosi severa , v occlusione . 
i vasi in cui sono stati identificati i criteri per diagnosticare una pseudo - occlusione sono stati esclusi dallanalisi comparativi per evitare errori da sovrastadiazione della stenosi . laspetto della placca stato valutato allinterfaccia con il lume vasale : la placca stata definita irregolare in presenza di piccole irregolarit superficiali e ulcerata quando si evidenziata una profonda ulcera a nicchia con profili netti . 
le immagini delle dsa sono state valutate indipendentemente da un radiologo vascolare non a conoscenza dei risultati dellangio - rm e dellangio - tc su workstation con schermi da 2 mega - pixel ( barco n.v. , kortrijk , belgio ) equipaggiate con misurazione digitale millimetrica . 
 analisi dei dati i risultati delle sessioni di valutazione delle immagini sono state inserite in un database ( excel for office 2004 , microsoft corporation ; redmond , washington )  . 
i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) ed accuratezza sono stati calcolati per ognuna delle tre modalit di lettura nella valutazione del grado di stenosi , radiol med ( 2010 ) 115 : 634647 reactions to contrast material during the examinations . mean duration of the examination was 212 min for mra , 152 min for cta and 406 min for dsa . 
a slight tendency to overestimation was noted in the fp reading in the 3069% range ( grades ii and iii ) , with three cases of grade ii classified as grades iii and iv and one of grade iii classified as grade iv . 
in two cases , irregularities and ulcerations were not identified della morfologia , della lunghezza della placca e per la presenza di ulcere e lesioni tandeil test di wilcoxon per ranghi stato applicato per determinare differenze significative ( p < 0 , 05 ) della performance diagnostica in relazione a grading stenotico e lunghezza delle placche tra le varie modalit , le differenze relative alla presenza di ulcerazioni , di lesioni tandem ed alla morfologia delle placche sono state invece studiate con il test di mcnemar ( p < 0 , 05 )  . 
la concordanza tra i due lettori per grading delle stenosi , valutazione della morfologia di placca , presenza di ulcere , lunghezza della placca e presenza di lesioni tandem stata stimata tramite il calcolo del coefficiente di cohen . 
lagreement stato giudicato scarso per valori di 0 , 210 , 40 , moderato per valori di 0 , 410 , 60 , buono per valori di 0 , 610 , 80 ed eccellente per valori di 0 , 811 , 00 . 
 risultati tutti gli esami angio - rm , angio - tc e dsa sono stati effettuati con successo ; non si sono verificate complicazioni o reazioni avverse al mdc durante le procedure desame . 
stato esaminato un totale di 40 biforcazioni carotidee : il tempo medio di valutazione stato di 62 minuti per il pp , di 81 minuti per lo ss , 53 minuti per langio - tc e 42 per la dsa . table 1 accuracy , sensitivity , specificity , positive predictive value and negative predictive value of magnetic resonance angiography first - pass and steadystate ( mra - fp , mra - ss ) and computed tomography angiography ( cta ) in evaluating stenosis , morphology , ulcerations , length and tandem lesions . 
le immagini dimostrano una buona correlazione tra le ricostruzioni mip a spessore sottile ottenute dai datasets di pp ( a ) , ss ( b ) e angio - tc ( c ) e la dsa ( d )  . 
3a - d fp images ( a ) show a 60% stenosisnascet grade iii ( arrows ) of the left internal carotid artery . both mra - ss ( b ) and cta ( c ) images show a 70% stenosis ( nascet grade iv ) and a small but definite ulceration ( arrowheads ) not visible at mra - fp . 
tali reperti sono stati confermati alla dsa ( d )  . radiol med ( 2010 ) 115 : 634647 table 2 evaluation of stenosis degree for digital subtraction angiography ( dsa ) vs . 
4a - d missed plaque irregularities at mra - fp ( a )  . mra - ss ( b ) and cta ( c ) images demonstrate a 40% stenosis ( nascet grade ii ) of the left bulb , not well depicted even though correctly measured on mrafp . 
sono evidenti alcune irregolarit di placca maggiormente marcate in sede prossimale al bulbo ( frecce ) e pi fini in sede distale ( punte di freccia ) , confermate alla dsa ( d )  . 
analysis of the individual cases , however , revealed that ss produced a better evaluation of stenosis degree and plaque morphology in some cases in wich the diagnostic accuracy of the fp images was reduced due to motion artefacts ( two cases ) or to incorrect synchronisation between contrast material administration and acquisition initiation ( one case )  . 
in evaluating plaque the wilcoxon test revealed no differences between the three imaging length , sensibilit , specificit , accuratezza diagnostica , vpp e vpn relativi alla valutazione della stenosi sono riportati nella tabella 1 . 
una lieve tendenza alla sovrastima stata evidenziata alla lettura pp nel range 30%69% ( gradi ii e iii ) , con 3 casi di grado ii segnalati come grado iii e iv , ed 1 caso di grado iii segnalato come iv . 
le immagini dimostrano una buona correlazione tra le ricostruzioni mip a spessore sottile ottenute dai datasets di pp ( a ) , ss ( b ) e angio - tc ( c ) e la dsa ( d )  . 
 table 3 evaluation of plaque morphology and ulcers with magnetic resonance angiography first - pass and steady - state ( mra - fp , mra - ss ) sequences and computed tomography angiography ( cta )  . 
values are expressed as number of cases fp / ss / cta morphology regular irregular regular 18 / 20 / 21 3 / 1 / 0 ulcers ulcerated not ulcerated irregular 2 / 0 / 0 17 / 19 / 19 3 / 1 / 0 29 / 31 / 32 ulcerated not ulcerated 6 / 8 / 8 2 / 0 / 0 dsa , digital subtraction angiography tabella 3 valutazione della morfologia di placca e della presenza di ulcerazioni tramite angio - rm - pp , angio - rm - ss e angio - tc . 
langio - tc e lo ss sostanzialmente si sono dimostrati sovrapponibili tra loro ( p = 0 , 564 ) e superiori al pp per la valutazione del grado di stenosi ed il test di wilcoxon ha escluso lipotesi di uneguaglianza globale ( ss vs pp p = 0 , 454 ; pp vs cta p = 0 , 305 )  . 
sensibilit , specificit , accuratezza diagnostica , vpp e vpn per la valutazione della morfologia di placca , della lunghezza della stenosi e delle lesioni tandem sono espressi nella tabella 1 . 
relativamente alla valutazione della morfologia di placca e delle ulcere , angio - tc e ss sono risultati equivalenti tra loro e leggermente superiori al pp ma con differenze non sufficienti ad evidenziare una significativit statistica al test di mcnemar ( p > 0 , 05 ) nella popolazione da noi studiata . analizzando i singoli casi per , lo ss ha permesso una miglior valutazione del grado di stenosi e della morfologia delle placche in alcuni casi in cui la qualit diagnostica delle immagini acquisite in pp risultata ridotta per la presenza di artefatti da movimento ( 2 casi ) o per una errata sincronizzazione tra somministrazione di mdc ed inizio dellacquisizione ( 1 caso )  . 
treatment with stenting or tea reduces the risk of ipsilateral ischaemic events in patients with 70%99% stenosis [ 16 ] and in selected cases with 50%69% stenosis [ 17 ]  . 
the degree of stenosis , however , is not the only parameter that needs to be evaluated for planning appropriate treatment : structural alterations of the plaque , surface irregularities and ulcerations are , in fact , considered independent factors to be used for improving risk stratification and treatment strategy [ 18 ]  . 
the accuracy of mra in evaluating extracranial carotid artery disease has been positively evaluated in various studies [ 1 , 19 , 20 ]  . however , despite the recent technical developments and the implementation of parallel imaging protocols , there is still a compromise between high temporal resolution and optimal spatial resolution . 
previous comparative studies with cta have emphasised that limitations of mra in fp acquisitions lead to reduced spatial resolution and that acquisitions with nonisotropic voxels and a low matrix value can cause partial volume effects significant enough to compromise evaluating stenosis degree and plaque morphology [ 21 , 22 ]  . 
in addition , even with modern bolus - tracking incorrect synchronisation between bolus injection and acquisition can occur , with techniques , ogni anno gli eventi ischemici cerebrovascolari causano 20 milioni di casi di disabilit permanenti e nel 25% di questi la stenosi carotidea extra - cranica pu essere identificata quale causa dellictus [ 15 ]  . 
il trattamento con stenting o tea riduce il rischio di evento ischemico ipsilaterale in pazienti con il 70%99% [ 16 ] di stenosi ed in casi selezionati con il 50%69% di stenosi [ 17 ]  . 
il grado di stenosi non per lunico parametro che deve essere valutato per la pianificazione di un corretto trattamento : le alterazioni strutturali della placca , lirregolarit di superficie e le ulcerazioni vengono infatti considerati fattori indipendenti da prendere in considerazione al fine di migliorare la stratificazione del rischio e la strategia terapeutica [ 18 ]  . 
tuttavia nonostante i recenti sviluppi tecnici e limplementazione di protocolli di imaging parallelo , permane la necessit di un compromesso tra alta risoluzione temporale ed ottimale risoluzione spaziale : precedenti studi comparativi con langio - tc mostrano che i vincoli dellangio - rm allacquisizione di primo passaggio determinano una ridotta risoluzione spaziale e che acquisizioni con voxel non isotropico e basso valore di matrice possono causare effetti di volume parziale tali da compromettere la valutazione del grado di stenosi e della morfologia di placca [ 21 , 22 ]  . 
inoltre , anche con le moderne tecniche di bolus tracking , pu verificarsi unerrata sincronizzazione tra liniezione del bolo e lacquisizione , con conseguente scarso enhancement arterioso o sovrapposizione venosa . 
recenti studi [ 23 , 24 ] hanno mostrato promettenti performance dellangio - rm delle arterie carotidi con mdc blood pool : lelevata relassivit permette 644 radiol med ( 2010 ) 115 : 634647 consequent poor arterial enhancement and venous superimposition . 
this latter approach appears to be the key to overcoming the techniques intrinsic conflict between temporal and spatial resolution . scan protocol acquisition strategies used in fp imaging are substantially similar to those applied in mra with conventional contrast material . 
with ss imaging , the scan is adapted for a submillimetre isotropic acquisition ( 0.343 mm3 ) with lower values than previously reported [ 13 ] and substantially similar to those achieved with cta . 
by exploiting the pharmacokinetics of the contrast material in combination with the ipat technique and the use of multichannel coils , this spatial resolution was achieved with no reduction in the signal - tonoise ratio ( snr )  . 
in addition , the ss protocol enabled recovery of indispensable diagnostic information in cases in which fp images had poor quality , with only a moderate increase in scan duration . degree of stenosis the findings of evaluating vascular stenosis in the fp data sets were substantially in line with data reported in previous studies . 
in these cases , the reduced concentration of contrast material in the distal lumen can cause signal loss and overestimation of stenosis or the diagnosis of false pseudo - occlusions and occlusions [ 13 , 22 , 25 ]  . 
there were no similar cases in our study population , even in examinations with suboptimal quality . however , a moderate trend to overestimation of stenosis degree was noted , particularly in the presence of long and tortuous plaques in which coaxial mpr images were unable to supply reliable measurements . 
underestimation of stenoses on fp images evaluated as severe at cta has been described [ 21 , 22 ] and could be linked to partial volume effects caused by excessive slice thickness . 
 protocollo di scansione le strategie di acquisizione usate nellimaging di pp sono state sostanzialmente sovrapponibili a quelle applicate nellangio - rm con mdc convenzionale ; una qualit ottimale delle immagini stata tuttavia raggiunta nella maggior parte dei casi con met del dosaggio e da 1 / 2 ad 1 / 3 del flusso . 
per limaging allo ss il protocollo di scansione stato adattato per unacquisizione isotropica submillimetrica ( 0 , 343 mm3 ) con valori inferiori a quanto precedentemente riportato [ 13 ] e sostanzialmente assimilabili a quelli ottenuti allangio - tc . 
sfruttando la farmacocinetica del mezzo di contrasto in combinazione con la tecnica ipat e lutilizzo di bobine multi - canale , tale risoluzione spaziale stata ottenuta senza riduzione del rapporto segnale - rumore . 
inoltre , il protocollo ss servito a recuperare informazioni diagnostiche indispensabili nei casi in cui le immagini del pp avevano una scarsa qualit , con un modesto aumento della durata del tempo di scansione . 
 grado di stenosi i risultati della valutazione delle stenosi vascolari nei datasets di pp risultato sostanzialmente in linea con quanto esposto in precedenti studi ; stenosi ed occlusioni clinicamente rilevanti sono state correttamente identificate con buona sensibilit e specificit . 
effetti di signal - void sono stati precedentemente descritti in presenza di stenosi severe : in tali casi la ridotta concentrazione di mdc nel lume distale pu causare una perdita di segnale e una sovrastima della stenosi o la diagnosi di false pseudo - occlusioni ed occlusioni [ 13 , 22 , 25 ]  . nella nostra popolazione tuttavia non si sono verificati simili casi , anche in esami con qualit sub - ottimale ; stato comunque evidenziato un moderato trend alla sovrastima del grado di stenosi , soprattutto in presenza di placche lunghe e tortuose nelle quali le immagini mpr coassiali non hanno permesso misurazioni affidabili . 
la sottostima sulle immagini di pp di stenosi valutate come severe allangio - tc stata descritta [ 21 , 22 ] e potrebbe essere legata ad artefatti di volume parziale da eccessivo spessore di sezione . 
la valutazione dello ss offre un significativo miglioramento in termini di performance diagnostica , come effetto diretto dellaumento in termini di risoluzione spaziale dellacquisizione isotropica che radiol med ( 2010 ) 115 : 634647 significant improvement in terms of diagnostic performance as a result of the direct effect of the increase in spatial resolution of the isotropic acquisition , which enables more reliable measurement of the stenosis degree on both thin - slice mip and mpr images . 
this could be explained with the simultaneous visualisation of familiar and immediate images ( fp ) and images with very high spatial resolution ( ss ) , thus enabling at the same time a rapid and panoramic identification of vascular damage and its accurate characterisation . 
lastly , it should be noted that state - of - the - art the use of visualisation / reconstruction software package , image evaluation used when reporting findings made optimal demonstration of the residual lumen possible at the level of the stenosis , not only for mra but especially for cta . indeed , it is known that the presence of extensively calcified plaques can negatively influence the ability of cta to correctly estimate stenosis degree due to calcium blooming artefacts . 
there were no cases of stenosis overestimation at cta in the presence of extensively calcified plaques . thanks plaque morphology , length and tandem lesions in the past , sensitivity and specificity of mra with interstitial contrast material have been valid but still not optimal in evaluating irregularities and ulcerations of the vessel wall [ 21 , 22 ]  . 
even though the finding was not statistically significant ( p > 0.05 ) in our patient population due to the low number enrolled , values reported in the statistical analysis are well above 90% for all parameters assessed , and they demonstrate an evident superiority of ss over fp in evaluating carotid artery plaque morphology and almost equivalent to cta performance . 
this result is vital when considering that the failure to correctly evaluate these findings can lead to incorrect treatment of moderate stenosis when fp is the only acquisition phase . permette misurazioni del grado di stenosi pi affidabili sia su immagini mpr che mip a strato sottile . 
a tale proposito la lettura delle immagini in forma combinata ( pp e ss ) potrebbe offrire un aumento di accuratezza diagnostica rispetto alle due modalit prese singolarmente e tale effetto potrebbe essere spiegato con la visualizzazione simultanea di immagini familiari ed immediate , quali quelle del pp , e di dati ad elevatissima risoluzione ottenuti nello ss , permettendo allo stesso tempo una veloce e panoramica identificazione del danno vasale e la sua accurata caratterizzazione . 
infine da notare come la modalit di valutazione delle immagini utilizzata in sede di refertazione abbia permesso , tramite limpiego di un software di visualizzazione / ricostruzione allo stato dellarte , unottimale dimostrazione del lume residuo a livello della stenosi , non soltanto per langio - rm ma soprattutto per langio - tc : infatti noto come la presenza di placche estesamente calcifiche possa influenzare negativamente la capacit dellangio - tc di stimare correttamente il grado di stenosi a causa di artefatti da blooming del calcio . 
nel nostro studio tale limitazione stata superata soprattutto grazie allimpiego degli algoritmi semiautomatici di c - mpr con integrata visualizzazione delle sezioni coassiali : in nessun caso si verificata sovrastima della stenosi allangio - tc in presenza di placche estesamente calcificate . 
 morfologia di placca , lunghezza e lesioni in tandem in passato la sensibilit e la specificit dellangio - rm con mdc interstiziale sono risultate valide , ma non ancora ottimali per la valutazione delle irregolarit e delle ulcere della parete vasale [ 21 , 22 ]  . 
alcuni studi hanno dimostrato un aumento della performance diagnostica utilizzando matrici elevate e voxel di dimensione ridotta [ 25 , 26 ] ; tuttavia , utilizzando mdc convenzionali , limaging a risoluzione sub - millimetrica determina uninevitabile riduzione del rapporto segnale - rumore ed un aumento dei tempi di acquisizione con diffusa sovrapposizione venosa . 
langio - rm con mdc blood pool con acquisizioni allo ss supera tali limitazioni : in alcuni casi ulcere e persino sottili irregolarit della superficie di placca non evidenziate nel solo esame in pp sono state correttamente identificate allo ss in ottima correlazione con langio - tc . 
anche se nella nostra popolazione il dato non risultato statisticamente significativo ( p > 0 , 05 ) , fondamentalmente per lesiguo numero di soggetti arruolati , i valori riportati nellanalisi statistica sono ben oltre il 90% per tutti i parametri valutati e descrivono unevidente superiorit dello ss sul pp nella valutazione della morfologia delle placche carotidee , pressoch equivalente alla performance dellangio - tc . tale risultato di fondamentale importanza se si considera che la mancata valutazione di tali reperti pu condurre ad un errato trattamento di stenosi moderate , considerando pp come unica fase di acquisizione . 
 646 conclusions conclusioni radiol med ( 2010 ) 115 : 634647 preliminary results obtained in our study indicate that mra with blood - pool contrast agents enables accurate evaluation of carotid artery stenosis and plaque morphology . 
nonetheless , further studies in larger patient populations are required to evaluate the potential development and future applications of the technique . i risultati preliminari ottenuti nel nostro studio indicano che langio - rm con mdc blood pool consente una valutazione accurata della stenosi carotidea e della morfologia della placca . 
radiologia muscoloscheletrica , irccs ospedale casa sollievo della sofferenza , viale cappuccini 1 , 71013 san giovanni rotondo ( fg ) , italy 3arches , castellana grotte ( ba ) , italy correspondence to : g . 
guglielmi , cattedra di radiologia , universit degli studi di foggia , foggia , italy , tel / fax : + 39 - 0881 - 733866 , e - mail : g.guglielmi@unifg.it received : 29 july 2008 / accepted : 6 october 2008 / published online : 22 february 2010 springer - verlag 2010 abstract the increasing distribution of high - field ( 3 t ) magnetic resonance ( mr ) systems for clinical use has been accompanied by the need to fully understand the advantages and disadvantages that the increase in signal quality confers . 
continuous development of the coils is required to fully express the potential of these systems , especially given the synergy between parallel imaging and the recent multichannel phased - array coils , which are able to improve image quality , spatial resolution and diagnostic accuracy in musculoskeletal imaging . 
the increase in signal offered by the high field makes possible improved visualisation of bone , cartilage , tendons and ligaments . this advantage , together with increased spatial resolution , is particularly useful when studying joints or some of their components , the evaluation of which has produced suboptimal results in non arthrographic examinations such as the glenoid labrum of the shoulder and the articular cartilage of the knee . 
thanks to the greater signal - to - noise ratio and improved spatial resolution , mr imaging at 3 t is able to notably increase diagnostic performance in the musculoskeletal setting , with a consequent improvement in patient treatment and management . keywords high field mr high resolution mr quantitative mr musculoskeletal system riassunto ad una maggiore diffusione di apparecchiature ad alto campo ( 3 t ) ad utilizzo clinico si accompagna la necessit di comprendere appieno i vantaggi e gli svantaggi apportati dallincremento della quantit di segnale . 
un continuo sviluppo delle bobine necessario per esprimere il potenziale di tali apparecchiature , specialmente in considerazione della sinergia esistente tra imaging parallelo e le recenti bobine multicanale phased array , in grado di migliorare qualit dellimmagine , risoluzione spaziale ed accuratezza diagnostica in ambito muscoloscheletrico . 
lincremento del segnale offerto dallalto campo consente una migliore visualizzazione delle strutture ossee , tendinee , cartilaginee e legamentose . tale vantaggio , unito ad una maggiore risoluzione spaziale , risulta particolarmente utile nello studio delle articolazioni o di alcune loro componenti fino ad oggi valutabili in maniera subottimale con esami non artrografici , quali il labbro glenoideo della spalla e la cartilagine articolare del ginocchio . 
grazie al maggiore rapporto segnale / rumore ed alla maggiore risoluzione spaziale , limaging in risonanza magnetica ( rm ) a 3 t in grado di incrementare notevolmente la capacit diagnostica in campo muscolo - scheletrico , con conseguente miglioramento della cura e della gestione del paziente . parole chiave rm ad alto campo rm ad elevata risoluzione rm quantitativa apparato muscoloscheletrico 572 introduction the evolution of imaging systems used in clinical practice has undergone marked acceleration in recent years . 
systems operating at 3 t are present in a number of centres , and many studies have been done to determine their benefits and drawbacks , with particular attention being paid to the central nervous system [ 13 ]  . 
the increase in signal - tonoise ratio ( snr ) offered by mr devices a 3 t can be broadly applied in the musculoskeletal setting , with promise being shown in evaluating tendons , cartilage , bone and ligaments . 
by holding constant the voxel size and number of rf pulses applied , a significant increase in snr is achieved with a consequent improvement in reconstructed image quality , 2 . 
with the same snr as a 1.5 - t system , voxel size and / or number of pulses applied can be reduced to obtain greater spatial resolution and / or shorter sequence duration along with the increase in the amount of signal issuing from a single voxel is a corresponding increase of the same amount in the specific absorption rate ( sar ) , i.e. 
turbo spin echo ( tse ) and turbo field echo ( tfe ) ] , even though the increase in tr in all sequences as will be explained below partially compensates the radiol med ( 2010 ) 115 : 571584 introduzione levoluzione delle apparecchiature utilizzate nellimaging clinico ha conosciuto negli ultimi anni unimportante accelerazione . 
per quanto riguarda la risonanza magnetica , lattenzione si concentrata sulla realizzazione di tomografi ad elevato campo magnetico statico ; apparecchi da 3 t sono presenti in diversi centri e sono ormai numerosi gli studi volti a comprendere i benefici e le problematiche da questi derivanti sui diversi apparati , con particolare attenzione rivolta al sistema nervoso centrale [ 13 ]  . 
laumento del rapporto segnale - rumore , garantito dagli apparecchi di risonanza magnetica ( rm ) da 3 t , trova vaste applicazioni in ambito muscolo - scheletrico con interessanti potenzialit per quanto concerne la valutazione di tendini , cartilagine , osso e legamenti . 
limaging rm a 1 , 5 t ha ottenuto grossi successi , tuttavia alcune strutture articolari ancora non ben valutate rappresentano un vasto campo di applicazione per i sistemi da 3 t . 
accanto allindagine clinica della rm a 3 t nello studio delle patologie muscolo - scheletriche , un settore molto promettente per limpiego di sistemi ad alto campo quello relativo allindagine dellosteoporosi e di altre malattie metaboliche dellosso . lo scopo di questo lavoro quello di illustrare le caratteristiche peculiari della risonanza magnetica a 3 t dellapparato muscolo - scheletrico , con relativi vantaggi e svantaggi rispetto a sistemi rm a pi basso campo , e di evidenziare le sue principali applicazioni cliniche . 
 aspetti tecnici rapporto segnale - rumore il rapporto segnale - rumore ( snr ) dipende da : intensit del campo magnetico statico , dimensione del voxel , numero e durata degli impulsi di radio - frequenza ( rf ) ed efficienza del sistema di ricezione del segnale [ 4 ]  . 
lincremento dintensit del campo magnetico determina pertanto un aumento della quantit di segnale proveniente dal singolo voxel ( pari a quattro volte nel passaggio da 1 , 5 t a 3 t ) ; ci significa che : 1 . 
mantenendo costante la dimensione dei voxel ed il numero dimpulsi applicati , si ottiene un importante aumento del rapporto segnale - rumore con conseguente miglioramento della qualit delle immagini ricostruite ; 2 . 
inoltre , a parit di rapporto segnale - rumore rispetto ad apparecchiature da 1 , 5 t , possiamo ridurre la dimensione del voxel e / o il numero di impulsi applicati , in modo da ottenere una maggiore risoluzione spaziale e / o una minore durata delle sequenze . allaumento della quantit di segnale proveniente dal singolo voxel corrisponde per anche un incremento radiol med ( 2010 ) 115 : 571584 dellidentica misura dello specific absorption rate ( sar ) , ossia la quantit di energia assorbita per chilogrammo di peso . 
ci ha determinato delle limitazioni nellapplicazione di sequenze a tempo di ripetizione ( tr ) breve o con impulsi di rifocalizzazione del segnale ( ad esempio turbospin echo [ tse ] e turbo field echo [ tfe ] ) , anche se lincremento del tr in tutte le sequenze come verr spiegato in seguito ha parzialmente compensato il fenomeno . 
in ogni caso , le maggiori aziende del settore hanno gi approntato delle strategie volte a ridurre il sar , quali il ricorso ad iperechi oppure ad impulsi di rifocalizzazione a ridotto angolo di flip . 
la disponibilit di una maggior quantit di segnale ha importanti conseguenze anche sulle bobine , ma questo argomento sar trattato nella relativa sezione . contrasto tissutale e soppressione del grasso laumento del campo magnetico statico determina un netto incremento del t1 , un pressoch impercettibile decremento del t2 ed un lieve decremento del t2 * dei protoni eccitabili . ci accade perch il pi elevato campo magnetico statico provoca laumento della frequenza di precessione dei protoni con conseguente riduzione della cessione di energia al reticolo ( ed allungamento del t1 ) , si accompagna ad un lieve aumento della disomogeneit di campo ( con decremento del t2 * ) , ma non ha alcun influsso sul defasamento dei protoni successivo alla loro eccitazione ( cio sul t2 ) [ 5 ]  . 
per le immagini pesate in t1 , al fine di evitare la saturazione dei protoni eccitabili si incrementato il tr di circa il 20% , pur essendo ormai noto che possibile ottenere immagini pesate in t1 con una gamma di valori di tr piuttosto ampia , e si dovuto abbreviare il tempo di eco ( te ) per via del pi rapido decadimento del segnale ; 2 . 
per le immagini pesate in t2 e t2 * si abbreviato il te per la ragione appena descritta , e si dovuto incrementare il tr per evitare la pesatura in t1 delle immagini . 
 il caso di sottolineare il fatto che , sebbene a 3 t leffetto sulla riduzione del t2 del fluido sinoviale sia decisamente maggiore rispetto alla cartilagine articolare , il valore effettivo di t2 del fluido sinoviale rimane sufficientemente elevato rispetto ai valori di te impiegati per la pesatura delle immagini in t2 . 
la conservazione di un elevato segnale per il liquido sinoviale , unita alla riduzione del segnale della cartilagine articolare , comporta un maggior contrasto tra questi tessuti e teoricamente migliora lidentificazione delle lesioni superficiali della cartilagine [ 5 ] ; 3 . 
1 immagine t1 pesata fast spin echo ( tr = 600 ms , te = 9 , 9 ms ) sul piano coronale del polso di un giovane adulto , ottenuta con unapparecchiatura a 3 tesla ( ge medical systems , milwaukee , wi ) e bobina in quadratura standard per lencefalo . 
the availability of a greater amount of signal has important consequences for the coils also ; this is dealt with in the relevant section below . tissue contrast and fat suppression the increase in the static magnetic field produces a marked increase in t1 , an almost imperceptible decrease in t2 and a slight decrease in t2 * of the excitable protons . 
these phenomena have created the need for adaptations to the sequences to obtain a correct weighting of the images : 574 radiol med ( 2010 ) 115 : 571584 delle immagini e ridurre il te per contrastare il pi rapido decadimento del segnale . in generale , dunque , si pu notare come vi sia un aumento della durata delle singole sequenze . 
possiamo ovviare a questo problema attraverso la riduzione del numero di scansioni ( nsa ) , anche se al prezzo di una non trascurabile riduzione del snr ( al dimezzamento del nsa corrisponde una riduzione del snr del 30% ) , oppure sfruttando al meglio le possibilit offerte dallimaging parallelo , di cui parleremo pi avanti . sebbene i tempi di rilassamento dei tessuti ed i parametri dacquisizione siano i maggiori responsabili del contrasto tra tessuto e fluido , la soppressione del grasso ampiamente utilizzata in campo muscolo - scheletrico per aumentare il contrasto tra i tessuti a contenuto lipidico e quelli privi di grasso . 
nel primo caso , laumento del chemical shift tra grasso ed acqua ha reso possibile lapplicazione di preimpulsi di pi breve durata ; nel secondo caso , lallungamento del t1 ha determinato un allungamento del tempo di inversione ( ti )  . da non sottovalutare inoltre la possibilit di implementare in maniera pi ampia sequenze ad eccitazione selettiva spettro - spaziale , grazie alla minore durata della combinazione dei preimpulsi . artefatti artefatti da suscettibilit magnetica come abbiamo gi detto , la maggiore intensit del campo magnetico statico determina una riduzione del t2 ma soprattutto del t2 * , con il conseguente incremento degli artefatti da suscettibilit magnetica di cui sono tipicamente responsabili le protesi in materiale metallico . per limitare questo fenomeno possiamo adottare diverse strategie : 1 . 
for t2and t2 * - weighted images , te should be shortened for the reason just described , and tr has to be increased to avoid t1 weighting of the images . 
it should be noted that although at 3 t the effect on the reduction of t2 of synovial fluid is decidedly greater than articular cartilage , the effective t2 value of synovial fluid is sufficiently higher than the te values used for weighting images in t2 . 
maintaining a high signal for synovial fluid , together with reduction in signal of articular cartilage , produces greater contrast between these tissues and in theory improves identification of lesions of the cartilage surface [ 5 ]  . 
for sequences weighted in proton density ( pd ) , tr should be increased to avoid weighting in t1 of the images , and te has to be reduced to contrast the more rapid signal decay . in general , therefore , there is an increased duration of individual sequences . 
these problems can be avoided through a reduced number of signal averages ( nsa ) , even at the price of a non negligible reduction in snr ( halving nsa corresponds to a 30% reduction in snr ) , or by exploiting the possibilities offered by parallel imaging , which is discussed below . although tissue relaxation times and acquisition parameters are the most preponderant factors affecting the contrast between tissue and fluid , fat suppression is widely used in musculoskeletal imaging to increase contrast between fat - containing tissue and tissue without fat . 
in the first case , the increase in chemical shift between fat and water enables application of quick prepulse sequences , whereas in the second , the lengthening of t1 produces lengthening of the inversion time ( ti )  . 
another useful technique is the broader implementation of selective spectral - spatial excitation sequences , thanks to the shorter duration of prepulses . artefacts magnetic susceptibility artefacts as stated above , the higher static magnetic field intensity produces a reduction in t2 , but most of all in t2 * , with a consequent increase in magnetic susceptibility artefacts most often caused by metallic prostheses . 
shortening the t2 of the sequences , bearing in mind that in fast spin - echo ( fse ) sequences , the optimal te must take into account the echo time length ( etl ) and that in the case of t2 - weighted images , an excessive shortening of te would negatively influence image contrast - tonoise ratio ( cnr ) 3 . 
in fat - suppression sequences , substituting spir with stir sequences , as the latter provide a more homogeneous suppression , albeit to the detriment of snr chemical shift at 3 t the chemical shift between fat and water protons is twice that at 1.5 t ( 448 hz against 224 hz ) [ 6 ]  . 
infine , per le sequenze a soppressione del grasso , sostituire le spir con le stir ; questultime conferiranno una soppressione pi omogenea , anche se a discapito del snr . chemical shift a 3 t il chemical shift tra i protoni del grasso e quelli dellacqua il doppio di quello a 1 , 5 t ( 448 hz rispetto a 224 hz ) [ 6 ] ; ci implica che nella rm a 3 t gli artefatti da chemical shift lungo il gradiente di lettura sono pi accentuati . in questo caso possiamo : 1 . 
altrimenti ridurre la dimensione del voxel in modo da limitare lo shift intravoxel alla base dellartefatto ; anche in questo caso avremo una riduzione del snr . artefatti da flusso lincremento dintensit del campo magnetico statico determina unaccentuazione degli artefatti da flusso [ 7 ]  . questo fenomeno pu essere attenuato attraverso lapplicazione di bande di saturazione per i flussi arteriosi e venosi , oppure attraverso unoculata scelta della direzione della codifica di fase . 
ad esempio , in immagini sagittali del ginocchio , una codifica di fase diretta dallalto verso il basso assicura una propagazione degli artefatti posteriormente ai vasi , con conseguente risparmio delle strutture interne dellarticolazione . 
 inoltre possibile ricorrere a gradienti di compensazione di flusso , ma ci determina un allungamento del te , che pu costituire un problema nellottenimento di immagini pesate in t1 o densit - protonica ( dp )  . artefatti da troncamento ad elevati valori di campo magnetico statico , per via dellincremento del snr , si verifica anche unaccentuazione della differenza dintensit di segnale a livello delle interfacce liquido / osso ; ci determina una maggiore predisposizione a sviluppare artefatti da troncamento a tale livello . 
il fenomeno pu essere limitato aumentando la risoluzione spaziale delle immagini , ricorrendo a matrici di ricostruzione di maggiori dimensioni o a campo di vista ( fov ) pi piccoli . le bobine the increase in static magnetic field intensity causes an increase in flow artefacts [ 7 ]  . 
la differenza sta nel fatto che le prime sono generalmente bobine a quadratura di fase e 576 radiol med ( 2010 ) 115 : 571584 attenuated by applying saturation bands for arterial and venous flow or by carefully selecting the phase - encoding direction . 
for example , in sagittal images of the knee , phase encoding directed downwards guarantees propagation of artefacts posterior to the vessels , with a consequent sparing of internal structures of the joint . 
another approach is to use flow compensation gradients , although this produces te lengthening , which can create difficulties in obtaining t1or proton - density ( pd ) - weighted images . truncation artefacts increased snr at higher static magnetic field levels also produces accentuation in the different signal intensities at fluid / bone interfaces . 
the phenomenon can be limited by increasing the spatial resolution of the images with the use of larger reconstruction matrices or a smaller field of view ( fov )  . coils coils can be classified into two categories : receiver / transmitter and receiver coils . 
the difference lies in the fact that the former are generally quadrature coils , which also function as a source of rf pulses , producing reduced body volume subject to the rf and a consequent reduction in sar . 
these features are highly useful in high - field mr . a special type of coil uses phased - array technology [ 8 ]  . these coils use a series of highly specialised elements to obtain the signal individually . 
at any rate , a comparison between a quadrature coil and a phased - array coil for the knee has revealed that despite the better cnr of the latter , there are no substantial differences in terms of sensitivity towards alterations of the meniscus [ 9 ]  . parallel imaging parallel imaging uses spatial data obtained from various elements of a phased - array coil to construct portions of the k - space . 
parallel imaging techniques can be classified into two broad categories : simultaneous acquisition of spatial harmonics ( smash ) [ 10 ] and sensitivity encoding ( sense ) [ 11 , 12 ]  . 
in the first case , several parallel - operating coils are able to capture different harmonics according to their distance from the column of protons of which the phase is being encoded with the application of an fungono anche da sorgente degli impulsi rf , cosa che determina la riduzione del volume corporeo investito dalle rf con conseguente riduzione del sar , dote molto utile in ambito di rm ad alto campo . un tipo speciale di bobine utilizza la tecnologia phasedarray [ 8 ] ; tali bobine impiegano una serie di elementi altamente specializzati per ottenere il segnale individualmente . queste bobine migliorano il snr in confronto ad altri tipi di bobine , e sono necessarie per limpiego dellimaging parallelo . 
la maggior parte delle bobine phased - array sono del tipo ricevente , cosa che a 3 t le rende meno vantaggiose in termini di sar rispetto alle bobine a quadratura di fase . 
in ogni modo , dal confronto tra una bobina a quadratura di fase ed una phased - array per il ginocchio , nonostante il maggior rapporto contrasto - rumore ( cnr ) di questultima non sono emerse differenze sostanziali in termini di sensibilit verso le alterazioni meniscali [ 9 ]  . imaging parallelo limaging parallelo una tecnica che utilizza i dati spaziali ottenuti dai vari elementi di una bobina phased - array per costruire porzioni dello spazio - k . 
questo comporta una riduzione del tempo di scansione e del sar , grazie alla riduzione del numero di impulsi rf necessari per ottenere le immagini . possiamo classificare le tecniche di imaging parallelo essenzialmente in due grandi categorie : lacquisizione simultanea di armoniche spaziali ( simultaneous acquisition of spatial harmonics , smash ) [ 10 ] ed il sensitivity encoding ( sense ) [ 11 , 12 ]  . 
nel primo caso abbiamo pi bobine operanti in parallelo , in grado di captare armoniche diverse a seconda della loro distanza rispetto alla colonna di protoni di cui si sta codificando la fase con lapplicazione di un apposito gradiente . 
ci consente la codifica di fase di un certo numero di colonne adiacenti dambo i lati , e permette quindi di ridurre il numero di impulsi da applicare per la codifica di fase . 
nel secondo caso ogni bobina attiva partecipa alla codifica di uno stesso , ridotto spazio - k ; limmagine finale a fov pieno deriva dalla discriminazione dei dati acquisiti da ogni singola bobina e allapplicazione di un singolo gradiente di codifica di fase corrisponde la codifica di tanti punti dello spazio - k quante sono le bobine operanti in parallelo ( a cui corrisponde il fattore di riduzione )  . entrambe queste tecniche consentono di abbreviare la durata delle singole sequenze e degli interi esami e di ridurre gli artefatti da movimento , anche se al prezzo di una riduzione del snr . 
in ambito muscolo - scheletrico , limaging parallelo si rivelato particolarmente utile nello studio delle cartilagini articolari attraverso la valutazione quantitativa del t2 ( di cui si dir successivamente ) ; tale tecnologia si infatti dimostrata in grado di produrre misurazioni accurate seppur in un tempo ben pi breve rispetto alle sequenze standard . radiol med ( 2010 ) 115 : 571584 appropriate gradient . 
the final image at full fov is derived from discrimination of acquired data from each individual coil , and application of a single phase - encoding gradient corresponds with encoding of as many points in the k - space as there are coils operating in parallel ( which corresponds to the reduction factor )  . both these techniques shorten individual sequence duration and therefore the entire examination as well as reducing motion artefacts , although at the cost of reduced snr . 
in the musculoskeletal setting , parallel imaging has proven to be particularly useful in studying articular cartilage with quantitative evaluation of the t2 ( which is discussed below )  . 
the technique has demonstrated its ability to produce accurate measurements , even in a much shorter time than in standard sequences . clinical applications in the musculoskeletal setting , attention is rapidly turning to mr imaging at 3 t . 
at 3 t a complete evaluation of the joint can be obtained in the three conventional planes in a little under 15 mwith regard to rotator cuffs , 1.5 - t systems demonstrate high accuracy in cases of complete tears ( up to 97% ) , such that application of a high field in theory presents little margin for improvement . 
il reale impatto clinico di questa tecnologia rimane tuttavia incerto per la mancanza di trial clinici controllati che valutino limpatto dell imaging rm a 3 t sul risultato diagnostico [ 13 ]  . tuttavia limaging rm a 1 , 5 t ha ottenuto grossi successi in ambito muscolo - scheletrico , laumento del rapporto segnale - rumore , garantito dagli apparecchi rm da 3 t , sembra presentare interessanti potenzialit per quanto concerne la valutazione di tendini , cartilagine , osso e legamenti . 
al contrario , molto promettente appare lutilizzo di apparecchi da 3 t o superiori nella valutazione delle rotture parziali , dove il miglioramento della risoluzione spaziale e del snr potrebbe determinare un minor ricorso allapprofondimento diagnostico mediante artro - rm ( che mantiene comunque il suo ruolo di esame gold standard su tale patologia ) , o comunque una pi elevata qualit delle immagini artrografiche [ 1619 ]  . 
limaging rm a 3 t della spalla risultato particolarmente utile nel delineare le rotture complete e parziali del sovraspinoso con unaccuratezza diagnostica significativamente migliore di quella ottenuta con i sistemi da 1 , 5 t . 
per quanto riguarda il labbro glenoideo , i sistemi da 1 , 5 t hanno dimostrato bassa sensibilit e specificit verso le lesioni ed il segnale patologico , con conseguente frequente ricorso allapprofondimento 578 radiol med ( 2010 ) 115 : 571584 the use of 3 t or higher systems appears to be promising in evaluating partial tears , where the gain in spatial resolution and snr could lead to a reduction in further diagnostic investigation with mr arthroscopy ( which nonetheless maintains its role as reference standard for this condition ) or at least higher quality of arthrographic images [ 1619 ]  . 
with regard to the glenoid labrum , 1.5 - t systems demonstrate low sensitivity and specificity in identifying lesions and the pathological signal , with consequent frequent recourse to diagnostic investigation with mr arthroscopy . 
in conclusion , mr imaging of the shoulder at 3 t is highly sensitive , specific and accurate in diagnosing injury and can reduce , although not completely replace , the need for arthrographic procedures . coxofemoral joint injury of the coxofemoral joint has been successfully studied with mr imaging . 
at the coxofemoral level , the major contribution of high - field mr systems is in studying the acetabular labrum , where increased snr may allow noninvasive imaging to equal if not surpass the diagnostic contribution made by mr arthroscopy , which is the reference standard at 1.5 t [ 23 ]  . 
 with regard to articular cartilage , many studies have shown the high level of mr imaging reliability at 1.5 t , with excellent correlation between radiological staging and degree of cartilage disease with mr imaging and surgical findings . 
the findings showed that the mr protocol at 3 t had a higher sensitivity than mr arthroscopy at a lower field , together with a better evaluation of the articular cartilage . 
the information acquired to date is encouraging , and in the future , the use of intra - articular contrast material could be supplanted by the availability of high - field mr . diagnostico con artro - rm . 
la disponibilit di apparecchiature rm da 3 t ha consentito una valutazione molto pi dettagliata che con i sistemi a pi basso campo [ 20 ] ; in particolare , magee e williams [ 21 ] hanno evidenziato come , dal confronto con le procedure artroscopiche , lrm a 3 t senza contrasto intra - articolare sia altamente sensibile e specifica nella valutazione di slap . 
in conclusione , limaging rm a 3 t della spalla risulta essere altamente sensibile , specifico ed accurato nella diagnosi di patologia e riduce , pur non sostituendo del tutto , il ricorso a procedure artrografiche . 
a livello coxo - femorale , il maggiore apporto dei sistemi rm ad elevata intensit di campo riscontrato nello studio del labbro acetabolare , dove laumento del snr potrebbe consentire allimaging non - invasivo di eguagliare o superare lapporto diagnostico dellartro - rm , esame di riferimento a 1 , 5 t [ 23 ]  . 
 per quanto riguarda la cartilagine articolare , molti studi hanno dimostrato lelevata attendibilit dellimaging rm gi a 1 , 5 t , con uneccellente correlazione tra la stadiazione radiologica del grado di patologia cartilaginea mediante imaging rm e riscontro chirurgico . 
 [ 20 ] hanno condotto uno studio prospettico volto a comparare limaging del labbro acetabolare ottenuto con rm a 3 t e con artro - rm a 1 , 5 t . 
ne risultato che il protocollo rm a 3 t ha dimostrato una sensibilit superiore allartro - rm a pi basso campo , unitamente ad una migliore valutazione delle cartilagini articolari . 
le informazioni acquisite finora sono incoraggianti ed in futuro il ricorso alliniezione di mdc intra - articolare potrebbe essere soppiantato dalla disponibilit di imaging rm ad elevata intensit di campo . ginocchio limaging rm a 3 t pu aumentare laccuratezza nella diagnosi di patologie meniscali , o quanto meno migliorare la confidenza diagnostica , oltre a fornire al chirurgo ortopedico una valutazione preoperatoria pi dettagliata [ 24 ]  . uno studio retrospettivo ha valutato la sensibilit e la radiol med ( 2010 ) 115 : 571584 specificit della rm a 3 t nellapproccio alla patologia meniscale rispetto allimaging con apparecchi da 1 , 5 t , con successivo riscontro artroscopico [ 25 ]  . 
per quanto riguarda i legamenti crociati , le cui lesioni complete sono gi valutabili con ottimi risultati con apparecchiature rm da 1 , 5 t , la rm a 3 t potrebbe giocare un ruolo fondamentale nellindividuazione delle lesioni legamentose parziali , verso le quali la confidenza diagnostica dei sistemi a pi basso campo nettamente inferiore . 
studi recenti [ 5 , 26 ] hanno inoltre dimostrato a 3 t un aumento del cnr tra liquido articolare e cartilagine , che potrebbe ulteriormente agevolare la valutazione di questultima [ 2 ]  . 
la migliorata risoluzione spaziale delle apparecchiature da 3 t ha importanti ripercussioni sulle piccole strutture del ginocchio come gli angoli postero - laterale e postero - mediale , complessi anatomici a funzione stabilizzatrice la cui corretta valutazione fondamentale per evitare il fallimento di interventi ricostruttivi sui legamenti [ 28 , 29 ]  . 
 polso la rm in grado di valutare con accuratezza le strutture articolari del polso , tuttavia alcuni chirurghi ortopedici permangono nella convinzione di dover ricorrere ad un esame artrografico per una valutazione ottimale dei legamenti [ 30 , 31 ]  . 
per quanto riguarda la cartilagine triangolare , nonostante le gi eccellenti prestazioni delle apparecchiature a pi basso campo , alcuni studi hanno dimostrato un aumento nella qualit delle immagini rm a 3 t rispetto a quelle ottenute a 1 , 5 t a parit di dimensione del voxel , con una migliore visibilit della fibrocartilagine triangolare ed un snr di muscolo , osso e cartilagine quasi raddoppiato [ 3234 ]  . similmente , gli studi condotti da lenk et al . 
 [ 33 ] hanno dimostrato la superiorit dellimaging rm a 3 t rispetto a quello a 1 , 5 t anche nella valutazione dei legamenti carpali , documentando un netto miglioramento nella diagnosi di patologia . 
3 immagine sagittale del ginocchio pesata in densit protonica , ottenuta con sequenza fast spin echo ( tr = 2100 ms , te = 21 , 5 ms ) , che mostra anchessa con buon dettaglio la cartilagine articolare . knee mr imaging at 3 t can increase diagnostic accuracy of meniscal injury , or at least increase diagnostic confidence , as well as provide the orthopaedic surgeon with a more detailed preoperative evaluation [ 24 ]  . 
a retrospective study assessed sensitivity and specificity of mr at 3 t in meniscal injury and compared them with findings obtained with 1.5 - t systems , with subsequent arthroscopic confirmation [ 25 ]  . 
recent studies [ 5 , 26 ] demonstrated an increase in cnr at 3 t between articular fluid and cartilage , which could further facilitate evaluation of the latter [ 2 ]  . 
improved spatial resolution of 3 t systems has important implications for the small structures of the knee , such as the posterolateral and posteromedial corners , which are complex anatomical stabilisers , the correct evaluation of which is crucial for avoiding failure of reconstructive procedures on ligaments [ 28 , 29 ]  . grado di sostituire del tutto lesame artrografico , essa sicuramente ridurr il numero di pazienti da sottoporre ad artro - rm . radiol med ( 2010 ) 115 : 571584 wrist mr is able to accurately evaluate articular structures of the remain wrist , although some orthopaedic surgeons convinced of the need for an arthrographic examination for optimal evaluation of the ligaments [ 30 , 31 ]  . 
high - field mr improves the diagnostic accuracy of noninvasive imaging and should reduce the need for arthrographic procedures . with regard to the triangular cartilage , despite the excellent performance of lower - field systems , several studies demonstrated increased quality of mr images at 3 t with respect to images obtained at 1.5 t with the same voxel size : visualisation of the triangular fibrocartilage complex improved and snr of the muscle , bone and cartilage almost doubled [ 3234 ]  . 
 [ 33 ] also demonstrated the superiority of mr imaging at 3 t over 1.5 t in evaluating carpal ligaments , with the finding of a clear improvement in disease diagnosis . 
similarly to the shoulder , although mr at 3 t does not seem to be in a position to completely replace the arthrographic examination , it can undeniably decrease the number of patients having to undergo an mr arthroscopy . vertebral column disadvantages associated with the increasing intensity of the static magnetic field place particular limitations on the study of the vertebral column , where the use of very broad fovs and the consequent larger voxel size produce a marked increase in sar and more noticeable chemical shift artefacts . flow artefacts are effectively limited by the application of special saturation bands . 
in these cases , some authors suggest orienting the readout gradient along the main axis of the metallic prosthesis [ 35 ] and limiting or avoiding completely the use of gradient recalled echo ( gre ) sequences [ 36 ]  . 
as a consequence of the notable signal production , in t1 - weighted images , cerebrospinal fluid assumes a grey level , which reduces the contrast with the other adjacent structures ( bone marrow , medullary cone , and cauda equina ) and creates difficulties in the identification of disease affecting the subarachnoid space . 
administration of contrast material undoubtedly facilitates detection of paraspinal tumours , and shapiro demonstrated the efficacy of fluid attenuation inversion recovery ( flair ) sequences in restoring the classic , high contrast between cerebrospinal fluid and adjacent tissues [ 35 ]  . colonna vertebrale abbiamo gi spiegato quali siano gli inconvenienti legati allincremento dintensit del campo magnetico statico ; tali fenomeni sono particolarmente limitanti nello studio della colonna vertebrale , dove luso di fov molto ampi e la conseguente maggiore dimensione dei voxel determinano un notevole incremento del sar e pi accentuati artefatti da chemical shift ; gli artefatti da flusso vengono efficacemente limitati attraverso lapplicazione di apposite bande di saturazione . 
in questi casi , alcuni autori suggeriscono di orientare il gradiente di lettura lungo lasse maggiore della protesi metallica in questione [ 35 ] , e di limitare o evitare del tutto luso di sequenze gradient echo ( gre ) [ 36 ]  . 
lapplicazione dellalto campo ha inoltre particolari ripercussioni sul contrasto tissutale ; in seguito alla sensibile produzione di segnale , nelle immagini pesate in t1 il liquor acquisisce infatti una gradazione di grigio che riduce il contrasto rispetto alle strutture adiacenti ( midollo spinale , cono midollare e cauda equina ) e rende di difficile dimostrazione patologie a carico dello spazio subaracnoideo ; la somministrazione di mezzo di contrasto facilita senza dubbio la rilevazione di localizzazioni neoplastiche paraspinali , mentre shapiro ha dimostrato lefficacia delle sequenze fast fluid - attenuated inversion - recovery ( flair ) nel ripristinare il classico , elevato contrasto tra il liquor ed i tessuti limitrofi [ 35 ]  . rm quantitativa dellosso trabecolare accanto allindagine clinica della rm a 3 t nello studio delle patologie della cartilagine , un settore molto promettente per limpiego di sistemi ad alto campo quello relativo allindagine dellosteoporosi e di altre malattie metaboliche dellosso . 
anche se losso non valutabile con la maggior parte delle tecniche rm attualmente disponibili in quanto non genera alcun segnale , nuovi approcci rm di tipo quantitativo sono utilizzati per studiare sia la densit che la struttura dellosso trabecolare [ 37 , 38 ]  . 
nel caso delle sequenze gradient - echo , le disomogeneit del campo magnetico radiol med ( 2010 ) 115 : 571584 quantitative mr of trabecular bone alongside the clinical examination with mr at 3 t in studying cartilage injury , a very promising area for highfield systems is studying osteoporosis and other metabolic bone diseases . 
even though bone cannot be evaluated with most of the available mr techniques in that they are unable to generate sufficient signal , new quantitative mr approaches are used to study trabecular bone density and structure [ 37 , 38 ]  . 
indeed , the presence of the trabecular matrix influences signal intensity of bone marrow , an effect that is particularly pronounced with certain mr sequences . in the case of gre sequences , the heterogeneity of the static magnetic field produced by the different susceptibility between trabecular bone and adjacent marrow causes a more rapid mr signal decay , which can be quantified by measuring the transverse relaxation time t2 *  . 
pioneering studies have shown that t2 * is correlated with trabecular bone density [ 39 , 40 ] , and therefore , the effective t2 * is shorter in normal trabecular bone than in the less dense trabecular structures of osteoporotic bone tissue . 
these characteristics make mr a fundamental technique in evaluating the quality of spongy bone and increase the ability of the technique not only in identifying occult fractures but also in making possible a more accurate prediction of fracture risk . the preferred site for quantitative mr studies is the heel bone in that it is mostly composed of spongy bone ( 95% )  . therefore quantitative mr of the calcaneus is extremely sensitive in identifying changes in bone quality that are not revealed by bone mineral densitometry ( bmd )  . 
the authors of this study also demonstrated that the r2 * ( 1 / t2 * ) is sensitive to changes in bone quality that were not identified with bmd . in a similar study done at 3 t on a group of 80 women , guglielmi et al . 
 [ 44 ] indicated the calcaneus tuberosity as the region most sensitive to deterioration of bone quality in patients with osteoporotic vertebral fractures . the use of high - field mr systems ( > 1.5 t ) can certainly promote the application of quantitative mr in the diagnosis of osteoporosis . 
 [ 45 ] demonstrated the possibility of ultrafast t2 * statico prodotte dalla differente suscettibilit tra losso trabecolare ed il midollo confinante causano un decadimento pi rapido del segnale rm , che pu essere quantificato misurando il tempo di rilassamento trasversale t2 *  . studi pionieristici hanno dimostrato che il t2 * correlato alla densit delle trabecole ossee [ 39 , 40 ] e quindi il tempo effettivo di rilassamento trasversale ( t2 * ) risulta essere pi breve nellosso trabecolare normale che nelle strutture trabecolari meno dense del tessuto osseo osteoporotico . 
queste caratteristiche rendono la rm un mezzo fondamentale nella valutazione della qualit dellosso spongioso , aumentando le capacit della metodica non solo nel riconoscimento di fratture occulte ma anche permettendo la predizione del rischio di fratture in modo pi accurato . 
 sito delezione per gli studi di risonanza magnetica quantitativa il calcagno , in quanto costituito in gran parte da osso spongioso ( 95% ) ; pertanto la rm quantitativa del calcagno pu essere in grado di evidenziare con estrema sensibilit alterazioni della qualit ossea non rilevate dalla densitometria ossea . 
 [ 43 ] hanno dimostrato che tra le varie zone del calcagno esaminate , la regione sottotalare quella in grado di discriminare meglio i pazienti con frattura da quelli senza frattura . 
 [ 44 ] hanno invece indicato la tuberosit calcaneare come la regione del calcagno pi sensibile al deterioramento della qualit dellosso nelle pazienti con fratture vertebrali da osteoporosi . limpiego di sistemi rm ad alto campo ( > 1 , 5 t ) pu certamente promuovere lapplicazione della rm quantitativa nella diagnosi dellosteoporosi . 
per ottenere una stima accurata del t2 * a 3 t , pu essere necessario applicare a livello di post - processing una procedura di correzione per minimizzare le variazioni di campo locali ( db0 ) responsabili della perdita di segnale e conseguente sovrastima del tasso di rilassamento r2 * ( 1 / t2 * )  . 
nel metodo proposto da dahnke e schaeffter [ 46 ] , la disomogeneit di campo magnetico principale ricavata dai dati t2 * calcolati su pi sezioni ed utilizzata come valore iniziale per una ottimizzazione interattiva , tramite la quale il segnale 582 radiol med ( 2010 ) 115 : 571584 fig . 
4a - c sagittal t1 - weighted fast spin - echo image of the calcaneus ( tr = 500 ms , te = 9.6 ms ) shows microarchitecture of the trabecular bone ( a )  . 
4a - c immagine fse t1 pesata in sagittale del calcagno ( tr = 500 ms , te = 9 , 6 ms ) in cui sono evidenti i diversi fasci trabecolari , tensivi e compressivi ( a )  . 
to obtain an accurate estimate of t2 * at 3 t , corrective measures may be required during postprocessing to minimise local field variations ( b0 ) responsible for signal loss and consequent overestimation of the r2 * relaxation rate ( 1 / t2 * )  . 
in the method proposed by dahnke and schaeffter [ 46 ] , the main field heterogeneity is derived from t2 * calculated on more than one section and is used as an initial value for interactive optimisation , with which the relaxation signal is corrected for each voxel . alongside t2 * evaluation , high - field quantitative mr can be successfully applied to obtain high - resolution images . 
adequate spatial resolution is in fact required for this type of study , as the mean diameter of the trabeculae is in the order of 100150 figure 4 shows some images of the calcaneus of a healthy individual obtained at 3 t with an in - plane resolution of 195 m , in which the structure of the trabeculae is well visualised . previous studies with quantitative mr of the microarchitecture of trabecular bone used both conventional spin - echo and gradient - echo sequences [ 47 ]  . 
recently , with the development of gradient technology , gradient - echo sequences denominated fully balanced steady - state free precession ( bssfp ) and the three - dimensional fast imaging employing steady - state acquisition ( fiesta ) sequences , true fast imaging with steady - state precession ( truefisp ) and balanced fast field echo ( bffe ) , which use very short tr , have become popular due to their efficiency in terms of snr [ 48 , 49 ]  . 
a recent study showed that bssfp sequences are particularly suitable for mr study of trabecular bone microarchitecture , but due to high - field intensity ( 3 t ) , multiple acquisitions are required to avoid artefacts deriving from heterogeneity of the magnetic field and local di rilassamento corretto per ogni voxel . accanto alla valutazione del t2 * , la rm quantitativa ad alto campo pu essere applicata con successo nellindagine della microarchitettura dellosso spugnoso , puntando soprattutto sulla possibilit di ottenere immagini ad alta risoluzione . 
una sufficiente risoluzione spaziale infatti richiesta per questo tipo di indagine , essendo il diametro medio delle trabecole nellordine dei 100150 in figura 4 sono riportate alcune immagini del calcagno di un soggetto sano ottenute a 3 t con una risoluzione nel piano di 195 m in cui ben evidenziata lorganizzazione delle trabecole ossee . studi precedenti riguardanti la rm quantitativa della microarchitettura dellosso trabecolare hanno impiegato sia sequenze spin - echo che gradient - echo [ 47 ] di tipo convenzionale . 
recentemente , con lo sviluppo della tecnologia dei gradienti , sequenze gradient - echo denominate fully balanced steady - state free - precession ( bssfp ) quali le sequenze tridimensionali fast imaging employing steadystate acquisition ( fiesta ) , true fast imaging with steadystate precession ( truefisp ) e balanced fast field echo ( bffe ) , che impiegano tempi di ripetizione molto brevi , sono diventate popolari per via della loro efficienza in termini di rapporto segnale - rumore [ 48 , 49 ]  . 
in uno studio recente , stato dimostrato che le sequenze gradient - echo del tipo bssfp sono particolarmente adatte allindagine rm della microarchitettura dellosso trabecolare , ma per intensit di campo magnetico elevato ( 3 t ) , unacquisizione multipla richiesta per evitare gli artefatti dovuti alle disomogeneit di campo magnetico e cos gli effetti off - resonance intrinseci allinterfaccia osso - midollo [ 50 ]  . 
daltro canto , noto che le sequenze locali , sono che radiol med ( 2010 ) 115 : 571584 off - resonance effects , which are intrinsic to the marrowbone interface [ 50 ]  . 
on the other hand , it is known that spin - echo sequences are less subject to off - resonance effects , which derive from differences in magnetic susceptibility between bone and marrow . 
therefore , a recently published report showed that fully balanced steady - state spin - echo sequence ( bssse ) could produce the best snr at 3 t and guarantee more accurate measurements of the microarchitecture of trabecular bone [ 51 ]  . in light of the above , high - field quantitative mr ( 3 t ) is of growing importance in evaluating the quality of trabecular bone and could contribute to predicting fracture risk and evaluating treatment in osteoporotic patients . spin - echo sono meno soggette agli effetti off - resonance , che derivano dalle differenze di suscettibilit magnetica tra losso ed il midollo . 
pertanto , una sequenza fully balanced steady - state spin - echo sequence ( bssse ) pubblicata recentemente si dimostrata produrre il miglior snr a 3 t e garantire cos misure pi accurate della microarchitettura dellosso trabecolare [ 51 ]  . alla luce di quanto riportato sopra , chiaro che la rm quantitativa ad alto campo ( 3 t ) di crescente importanza nella valutazione della qualit dellosso trasecolare e potrebbe contribuire alla predizione del rischio di frattura e alla valutazione degli interventi terapeutici nei pazienti osteoporotici . 
romano1 1unit operativa a struttura complessa di radiologia generale e di pronto soccorso , 2unit operativa a struttura complessa di radiologia vascolare , dipartimento di diagnostica per immagini , azienda ospedaliera di rilievo nazionale , a . 
pinto , via posillipo 168 / d , 80123 napoli , italy , tel : + 39 - 335 - 6762755 , fax : + 39 - 081 - 2466150 , e - mail : antopin1968@libero.it received : 2 december 2008 / accepted : 19 march 2009 / published online : 15 january 2010 springer - verlag 2010 abstract purpose . 
from january 2003 to december 2007 , 28 patients ( 19 men and nine women , age range 1680 years ) with acute symptoms from blunt pelvic trauma and a drop in haematocrit underwent mdct and angiography . 
mdct images were transferred to a workstation to assess pelvic fracture , site of haematoma and active extravasation of contrast material , visibility of possible vascular injuries and associated traumatic lesions . 
scopo del nostro lavoro stato valutare il ruolo della tomografia computerizzata multidetettore ( tcmd ) nellidentificazione di sanguinamento attivo e della sua origine in pazienti politraumatizzati con trauma vascolare della pelvi associato o non associato a fratture dellanello pelvico . 
tra gennaio 2003 e dicembre 2007 , sono stati sottoposti ad esame tcmd e successivamente ad esame angiografico 28 pazienti politraumatizzati ( 19 maschi e 9 femmine , con et compresa tra 16 e 80 anni ) affetti da specifico trauma della pelvi con calo dellematocrito . 
lesame tcmd stato condotto in 15 pazienti con apparecchiatura a quattro strati e nei rimanenti 13 pazienti con apparecchiatura a 16 strati ed ha previsto in tutti i pazienti uno studio total body per lidentificazione di lesioni traumatiche dellencefalo , della colonna vertebrale , del bacino , del torace , delladdome e della pelvi . 
stata eseguita una fase precontrastografica seguita da uno studio contrastografico trifasico con somministrazione con iniettore automatico di un volume pari a 120150 ml di mezzo di contrasto ( mdc ) con velocit di flusso di 45 radiol med ( 2010 ) 115 : 648667 pelvic aortogram was obtained in all cases before selective catheterisation of the internal iliac arteries and superselective catheterisation of their branches for embolisation purposes . 
mdct provides diagnostic information regarding the presence of small pelvic fractures and , thanks to the contrast - enhanced angiographic technique , it is capable of identifying pelvic bleeding , with the demonstration in some cases of it source . 
urgent angiography and subsequent transcatheter embolisation are the most effective methods for controlling ongoing arterial bleeding in pelvic injuries . keywords pelvis trauma active haemorrhage vessels multidetector - row ct ml / s , seguito da 40 ml di soluzione fisiologica con flusso pari a 2 ml / s . 
le immagini tcmd acquisite sono state trasferite ad una stazione di lavoro per le ricostruzioni necessarie alle differenti valutazioni : tipologia della frattura del bacino quando presente , sede dellematoma e dello stravaso di mdc , eventuale visibilit del vaso lacerato nello scavo pelvico ed eventuali ulteriori lesioni traumatiche associate dello stesso scavo pelvico o di altri distretti anatomici . 
il successivo studio angiografico stata condotto effettuando prima un angiogramma panoramico della regione aortoiliaca , seguito da uno studio selettivo della regione di interesse mediante cateterismo delle arterie ipogastriche e cateterismo superselettivo delle branche di divisione delle stesse arterie ipogastriche ai fini dellembolizzazione . 
lesame tcmd ha consentito di evidenziare la presenza di sanguinamento attivo in 21 / 28 casi ( 75% ) e la fase di studio postcontrastografico in cui pi frequentemente stato rilevato il sanguinamento attivo risultata la fase tardiva ( 13 / 21 casi , 61 , 9% )  . 
nellambito dei 21 pazienti in cui lesame tcmd ha mostrato la presenza di sanguinamento attivo , il vaso leso stato identificato in 12 / 21 casi ( 57% )  . 
le arterie pi frequentemente lese sono risultate lotturatoria ( 9 casi ) , lipogastrica ( 6 casi ) , la pudenda interna ( 6 casi ) e la glutea superiore ( 5 casi )  . 
in 8 / 28 pazienti ( 28 , 6% ) sono state osservate lesioni a carico di pi vasi arteriosi . nellambito dei 12 pazienti in cui lesame tcmd ha consentito lidentificazione del vaso leso , in 10 casi stata riscontrata una concordanza tra esame tcmd ed esame angiografico , in un caso lesame angiografico ha confermato la sede della lesione indicata allindagine tcmd mostrando anche una seconda arteria lesa , ed in un caso si verificata una discordanza tra indagine tcmd ed indagine angiografica . 
la tcmd permette di identificare anche piccole rime di frattura a carico del bacino e grazie allutilizzo del mdc ev ed alla tecnica di studio di angiografia - tcmd consente di riconoscere la presenza del sanguinamento attivo con possibilit , in alcuni casi , di definire anche la sede della perdita ematica . 
infatti la presenza di stravaso attivo di mdc ev rappresenta un indicatore della lesione che coinvolge unarteria specifica localizzata nella regione dello scavo pelvico ove lo stravaso visualizzato 650 radiol med ( 2010 ) 115 : 648667 allesame tcmd . 
langiografia eseguita in emergenza con embolizzazione della fonte emorragica il trattamento pi efficace delle emorragie di vasi arteriosi determinate da traumi pelvici . parole chiave pelvi traumi emorragia attiva vasi tc multidetettore introduction introduzione pelvic trauma is correlated with a significant level of morbidity and mortality and constitutes an important diagnostic problem in that damage to vascular structures is often more clinically significant than skeletal damage [ 1 ]  . because bone fractures are generally associated with a laceration of muscles or small - calibre veins , the resulting haematomas are self - limiting , characterised by low flow and containment within the muscular or retroperitoneal fascia , rarely require specific therapeutic intervention procedures and are therefore be treated conservatively . 
in contrast , lacerations to arterial vessels or large - calibre veins ( common iliac veins ) produce active bleeding , which is not self - limiting and which requires early diagnosis and prompt treatment , as this may rapidly lead to hypovolaemic shock and death [ 2 ]  . 
the findings reported in the literature in fact indicate that traumatic vascular lesions of the pelvis are a highly feared clinical condition , with mortality due to hypovolaemic shock > 25% [ 3 , 4 ] within 24 h of the trauma . 
death occurring after 24 h is more frequently due to multiple organ failure secondary to progressive hypovolaemia with slower onset , which can nonetheless lead to severe tissue hypoxia of vital organs . survival therefore essentially depends on duration and course of the haemorrhage and on prompt treatment and strategies undertaken in patients suffering from severe blood loss [ 5 ]  . in evaluating patients with major trauma , the use of whole - body multidetector - row computed tomography ( mdct ) is more than justified [ 6 ]  . 
this modality is in fact useful for identifying vertebral and pelvic fractures that may be missed on plain - film radiography ; for identifying associated traumatic lesions to the brain , chest or abdomen ; but above all for locating the sources of bleeding and thus enabling screening of patients with vascular lesions , which should have priority of treatment over skeletal lesions and often even over parenchymal lesions [ 711 ]  . the aim of this study was to evaluate the role of mdct in identifying the presence of active bleeding and its source in a population of polytrauma patients with known pelvic injuries and a drop in haematocrit who subsequently underwent angiography . i traumi della pelvi sono correlati ad una significativa morbilit e mortalit e rappresentano un importante problema diagnostico poich il danno alle strutture vascolari assume frequentemente un significato clinico maggiore rispetto al danno scheletrico [ 1 ]  . 
infatti la frattura di componenti ossee , in genere associata alla lacerazione di muscoli o di vasi venosi di modesto calibro , comporta la formazione di ematomi che si autolimitano , essendo a basso flusso e contenuti dalle fasce muscolari o retroperitoneali , raramente necessitano di un intervento terapeutico specifico e vengono pertanto trattati conservativamente . viceversa , la lacerazione di vasi arteriosi o di grossi collettori venosi ( vene iliache comuni ) causa di emorragia attiva che non si autolimita , e che necessita di una diagnosi precoce ed un tempestivo trattamento terapeutico , poich pu condurre rapidamente a morte il paziente per shock ipovolemico [ 2 ]  . 
i dati riportati in letteratura indicano , infatti , che le lesioni traumatiche vascolari del bacino rappresentano unevenienza clinica altamente temibile , con un tasso di mortalit per shock ipovolemico superiore al 25% [ 3 , 4 ] entro le ventiquattro ore dal trauma . lexitus che sopraggiunge oltre le ventiquattro ore pi frequentemente dovuto ad una insufficienza multipla dorgano ( mof ) secondaria ad una ipovolemia progressiva di pi lenta instaurazione che pu comunque condurre ad una grave ipossia degli organi vitali . 
 nella valutazione diagnostica dei pazienti con trauma maggiore ampiamente giustificato lutilizzo della tomografia computerizzata multidetettore ( tcmd ) total body [ 6 ] : tale metodica , infatti , particolarmente utile per la individuazione di rime di frattura della colonna vertebrale e del bacino ( che possono anche essere misconosciute allesame radiologico diretto ) , per identificare lesioni traumatiche associate dellencefalo e delle componenti anatomiche toraco - addominali , ma soprattutto per localizzare topograficamente le fonti di sanguinamento , permettendo di selezionare i casi con lesioni vascolari per i quali prioritario il trattamento rispetto a quello delle lesioni scheletriche e spesso anche delle stesse lesioni parenchimali [ 711 ]  . 
given its retrospective nature , informed consent was not required . population the patient population included 28 patients affected by major polytrauma ( age range 1680 years , mean age 43 years ; 19 men and nine women ) admitted to our emergency department between january 2003 and december 2007 with acute symptoms of pelvic trauma and low haematocrit and who underwent whole - body mdct and subsequently angiography . 
the following data were recorded for all patients : mechanism of trauma , age , sex , some vital signs recorded on admission ( haemoglobin , arterial pressure , heart rate ) , any blood transfusions performed before or after embolisation , injury severity score ( iss ) [ 4 ] , length of hospital stay , presence of pelvic fracture ( classified according to tile [ 12 ] ) , fracture treatment ( when present ) and death ( when present )  . 
time of arrival at the emergency department , as well as the time mdct scan and angiographic study were performed , were also recorded . image acquisition whole - body mdct was performed with a four - slice system in 15 patients ( lightspeed qx / i ge medical systems , milwaukee , wi , usa ) and a 16 - slice system in the remaining 13 patients ( aquilion 16 , toshiba , tokyo , japan )  . 
before entering the ct suite , each patient was assessed for vital signs , pharmacologically stabilised , sedated and provided with mechanical ventilation if spontaneous breathing was judged to be insufficient . 
a bladder catheter and a nasogastric tube were inserted ; peripheral venous access with a needle cannula at least 18 gauge was performed to allow administration of intravenous contrast material . acquisition parameters of the mdct study according to the system used are reported in table 1 . 
the study protocol involved a baseline unenhanced study followed by a triphasic study after administration of 120150 ml of contrast material at a concentration of 400 mgi / ml ( iomeron 400 , bracco , milan , italy ) with an automatic injector at a flow rate of 45 ml / s , followed by 40 ml of saline solution at a flow rate of 2 ml / s . 
the triphasic study involved an arterial phase , with the scan delay calculated with the bolus tracking technique , a portal phase obtained with a delay of 40 s after the arterial phase to evaluate parenchymal lesions and a late phase obtained with a delay of 180 s after the arterial phase to evaluate venous lesions and active bleeding . scopo del presente contributo quello di valutare il ruolo della tcmd nellidentificazione della presenza di sanguinamento attivo e della relativa fonte emorragica in pazienti politraumatizzati , con accertata compromissione della pelvi , calo dellematocrito , sottoposti a successivo esame angiografico . materiali e metodi lo studio stato approvato dal comitato etico ; data la sua natura retrospettiva non stato richiesto alcun consenso informato . popolazione sono stati esaminati 28 pazienti affetti da politrauma maggiore ( di et compresa tra 16 e 80 anni , et media 43 anni ; 19 maschi e 9 femmine ) ricoverati presso il nostro dipartimento emergenza - accettazione ( dea ) da gennaio 2003 a dicembre 2007 , con sintomatologia acuta da trauma della pelvi e calo dellematocrito , sottoposti ad esame di tcmd total body e successivamente ad esame angiografico . 
di ciascun paziente sono stati rilevati : il meccanismo del trauma , let , il sesso , alcuni parametri vitali registrati al momento del ricovero ( emoglobina , pressione arteriosa e frequenza cardiaca ) , le eventuali trasfusioni di sangue eseguite prima e / o dopo lembolizzazione , linjury severity score ( iss ) [ 4 ] , la durata dellospedalizzazione , la presenza di fratture di bacino ( distinte secondo la classificazione di tile [ 12 ] ) , il conseguente trattamento della frattura ( quando presente ) e leventuale exitus . 
di ciascun paziente stato anche rilevato lorario di arrivo presso il nostro pronto soccorso , lorario di esecuzione dellesame tc e quello dellesame angiografico . acquisizione delle immagini lesame tcmd total body stato condotto in 15 pazienti con apparecchiatura a quattro strati ( lightspeed qx / i , ge medical systems , milwaukee , wi , usa ) e nei rimanenti 13 pazienti con unapparecchiatura a 16 strati ( aquilion 16 , toshiba , tokyo , giappone )  . 
prima dellingresso in sala tomografica , ciascun paziente stato sottoposto a valutazione dei parametri vitali , stato farmacologicamente stabilizzato , sedato , e sottoposto a ventilazione meccanica se il respiro spontaneo stato giudicato insufficiente . 
 stato introdotto un catetere vescicale ed un sondino nasogastrico ; laccesso venoso periferico stato praticato con agocannula di almeno 18 g per consentire flussi adeguati di mezzo di contrasto endovena ( mdc ev )  . 
il protocollo di studio ha previsto uno studio di 652 radiol med ( 2010 ) 115 : 648667 table 1 computed tomography ( ct ) examination : acquisition parameters parameters 4 - slice mdct scanner 16 - slice mdct scanner scout patient position scan range scan direction kilovolt milliampere gantry rotation time ( s ) pitch anteroposterior supine total - body scan * craniocaudal 1.5 anteroposterior supine total - body scana craniocaudal 0.9375 ( pitch factor ) mdct , multidetector - row computed tomography afrom the top of the skull to the symphysis pubis tabella 1 esame di tomografia computerizzata multidetettore ( tcmd ) : parametri di acquisizione parametri tcmd 4 strati tcmd 16 strati scout posizione del paziente estensione della scansione direzione di scansione voltaggio del tubo ( kv ) amperaggio del tubo ( ma ) tempo di rotazione del gantry ( s ) pitch tcmc , tc multidetettore adal vertice del cranio alla sinfisi pubica antero - posteriore supina scannogramma total - body * cranio - caudale 140 220 0 , 8 1 , 5 antero - posteriore supina scannogramma total - bodya cranio - caudale 0 , 9375 ( fattore pitch ) the angiographic examination was performed with an integris v 5000 device ( philips )  . 
an initial panoramic angiogram was obtained of the aortoiliac region with a pigtail catheter and administration of contrast material ( iomeron 400 , bracco , milan , italy ) at a flow rate of 2025 ml / s for a total of approximately 2530 ml . 
image acquisition was performed at a rate of three frames per second in the arterial phase , two frames per second in the capillaryvenous phase and one frame per second in the late venous phase . 
the panoramic examination was followed by the selective study of a region of interest ( roi ) , with catheterisation of the internal iliac arteries using a cobra , multipurpose angiographic and in some cases a ruc ( cook ) catheter with the injection of a total of around 1215 ml of contrast material at a flow rate of 34 ml / s . after embolisation , superselective catheterisation was performed of internal iliac artery divisions using 2.7 - f hydrophilic progreat ( terumo , tm ) , 3 - f renegade ( boston ) or tracker ( boston ) coaxial catheters . 
the choice of embolising material was determined by the anatomical and physiological conditions of the patient ( regional vascular anatomy , presence of arterial spasms , impossibility of complete selectivity )  . base ( fase pre - contrastografica ) seguito da uno studio trifasico dopo somministrazione con iniettore automatico , di mdc ev alla concentrazione di 400 mgi / ml ( iomeron 400 , bracco , milano , italia ) con volume pari a 120150 ml , velocit di flusso di 45 ml / s , seguito da 40 ml di soluzione fisiologica con flusso pari a 2 ml / s . 
lo studio trifasico ha previsto una fase arteriosa con ritardo calcolato con il bolus tracking , una fase portale ottenuta con ritardo di 40 s rispetto alla precedente per la valutazione delle lesioni parenchimali ed una fase tardiva ottenuta con ritardo di 180 s rispetto alla fase arteriosa per la valutazione delle lesioni venose e dellemorragia attiva . 
langiografia stata condotta in tutti i casi per via percutanea transfemorale comune ( generalmente destra ) , mediante il posizionamento di un introduttore vascolare 5 f , effettuando prima un angiogramma panoramico della regione aorto - iliaca con catetere pigtail e somministrazione di mdc ( iomeron 400 , bracco , milano , italia ) ad un flusso di 2025 ml / s per un totale di 2530 ml circa . 
lesame panoramico stato seguito da quello selettivo per lo studio della regione di interesse mediante cateterismo delle arterie ipogastriche con catetere cobra , mpa , in alcuni casi ruc ( della ditta cook ) iniettando ad un flusso di 34 ml / s una radiol med ( 2010 ) 115 : 648667 data analysis the examinations were reassessed all mdct studies were evaluated by two radiologists with expertise in emergency imaging and who were unaware of the angiographic examination fndngs . 
images acquired were transferred to a workstation ( vitrea 3.5 , plymouth , minnesota , usa ) for 2d , multiplanar ( mpr ) , 3d , maximum intensity projection ( mip ) and volume rendering ( vr ) reconstructions in relation to the components to be examined ( parenchymal , vascular , bone )  . the analysis involved the presence of pelvic fractures ( classified according to tile ) , haematoma site and active extravasation of contrast material and the possible visibility of the injured vessel . 
associated traumatic lesions were sought in the pelvis and other anatomical districts in each mdct examination . angiographic images were retrospectively evaluated on digital support or film by two interventional radiologists who were unaware of the mdct findings . 
in cases of disagreement , consensus was later reached by the two interventional radiologists . quantit totale di circa 1215 ml di mdc . al fine dellembolizzazione stato successivamente eseguito il cateterismo superselettivo delle branche di divisione delle arterie ipogastriche utilizzando cateteri coassiali 2 , 7 f , idrofilici progreat ( terumo , tm ) , 3 f renegade ( boston ) o tracker ( boston )  . 
la scelta del materiale embolizzante stata subordinata alle condizioni anatomo - fisiologiche dei pazienti ( anatomia vasale regionale , eventuali spasmi arteriosi , impossibilit di completa selettivit )  . analisi dei dati tutti gli esami tc sono stati valutati da due radiologi esperti nellimaging dellurgenza che non conoscevano lesito dellesame angiografico : gli esami in cui si avuta una valutazione discordante sono stati rivalutati in maniera congiunta . 
le immagini acquisite sono state trasferite su una stazione di lavoro ( vitrea 3.5 , plymouth , minnesota , usa ) per le ricostruzioni 2d , multiplanari ( mpr ) , 3d , maximum intensity projection ( mip ) e volume rendering ( vr ) in relazione alle varie componenti da esaminare ( parenchimali , vascolari , ossee )  . 
sono stati analizzati : la presenza di fratture del bacino ( definite seguendo la classificazione di tile ) , la sede dellematoma e dello stravaso attivo di mdc e leventuale visibilit del vaso lacerato . 
sono stati ricercati in ciascun esame tc le lesioni traumatiche associate nel distretto pelvico ed in altri distretti anatomici . le immagini angiografiche sono state retrospettivamente valutate su supporto digitale o su pellicola da due radiologi interventisti che non conoscevano i risultati della tcmd . sono stati ricercati : lo stravaso di mezzo di contrasto , la presenza di pseudoaneurismi , lirregolarit del lume vasale , gli spasmi arteriosi e la trombosi . 
1 scansione in tomografia computerizzata ( tc ) dello scavo pelvico . lo scavo pelvico stato suddiviso in sei settori per la valutazione del sanguinamento : a ( regione dei muscoli retti delladdome ) , b ( regione glutea destra ) , c ( regione glutea sinistra ) , d ( regione iliaco - otturatoria destra ) , e ( regione iliaco - otturatoria sinistra ) , f ( spazio presacrale )  . let , il sesso , i parametri vitali alla presentazione ( emoglobina , pressione arteriosa e frequenza cardiaca ) , liss , la durata dellospedalizzazione e leventuale exitus di ciascun paziente sono indicati nella tabella 2 . 
il meccanismo del trauma risultato di tipo decelerativo in 12 / 28 casi ( 42 , 8% ) , diretto in 8 / 28 ( 28 , 6% ) , caduta dallalto in 654 statistical analysis the results regarding identification of the lacerated vessel were compared with angiographic findings to evaluate sensitivity and positive predictive value ( ppv ) of mdct . results age , sex , vital signs at presentation ( haemoglobin , arterial pressure , heart rate ) , iss , length of hospital stay and death when present are reported in table 2 . 
the mechanism of trauma was deceleration injury in 12 / 28 cases ( 42.8% ) , blunt trauma in 8 / 28 ( 28.6% ) , fall from a height in 4 / 28 ( 14.3% ) , compressive injury in 3 / 28 ( 10.7% ) and penetrating injury in one case only ( 3.6% ) ( table 3 )  . 
 lesame tcmd ha consentito di evidenziare la presenza di sanguinamento attivo in 21 / 28 casi ( 75% ) e la fase di studio post - contrastografico in cui pi frequentemente stato rilevato il sanguinamento attivo risultata la fase tardiva ( 13 / 21 casi , 61 , 9% )  . 
le lesioni traumatiche identificate toraco - addominali associate sono state allesame tcmd in 24 / 28 pazienti ( 85 , 7% ) ( tabella 5 )  . lintervallo di tempo intercorso tra il ricovero dei pazienti presso il nostro dea e lesecuzione dellesame tcmd risultato compreso tra 30 minuti e oltre 7 ore . 
in the 21 patients in whom mdct detected active bleeding , the lacerated vessel ( figs . 25 ) was identified in 12 / 21 cases ( 57% , table 4 )  . 
the time interval between patient admission to the emergency department and mdct examination was from 30 min to more than 7 h . patients who underwent mdct after > 60 min showed a late drop in haematocrit in the absence of pelvic fractures or with radiographically ascertained stable fractures . 
in 14 / 28 cases ( 50% ) , resorbable material was used ( contour emboli ) ; in the remaining 14 patients , nonresorbable material was used ( acrylic glue or coils )  . 
in 14 / 28 casi ( 50% ) stato adoperato materiale riassorbibile ( emboli di contour ) ; nei rimanenti 14 stato utilizzato materiale non riassorbibile ( colla acrilica oppure spirali )  . 
 nellambito dei 12 pazienti in cui lesame tcmd ha consentito lidentificazione del vaso leso ( sensibilit : 42 , 85% , valore predittivo positivo : 100% ) , in 10 casi stata riscontrata una concordanza tra esame tcmd ed esame 656 table 3 trauma characteristics radiol med ( 2010 ) 115 : 648667 mechanism of trauma pelvic fracture tile classification blunt injury deceleration injury compression injury compression injury deceleration injury fall from a height deceleration injury blunt injury fall from a height deceleration injury deceleration injury compression injury fall from a height deceleration injury blunt injury deceleration injury deceleration injury deceleration injury deceleration injury blunt injury deceleration injury blunt injury blunt injury blunt injury fall from a height blunt injury deceleration injury penetrating injury trauma diretto trauma decelerativo trauma compressivo trauma compressivo trauma decelerativo caduta dallalto trauma decelerativo trauma diretto caduta dallalto trauma decelerativo trauma decelerativo trauma compressivo caduta dallalto trauma decelerativo trauma diretto trauma decelerativo trauma decelerativo trauma decelerativo trauma decelerativo trauma diretto trauma decelerativo trauma diretto trauma diretto trauma diretto caduta dallalto trauma diretto trauma decelerativo trauma penetrante multiple multiple multiple multiple multiple multiple multiple multiple multiple multiple multiple multiple multiple singola nessuna multiple singola nessuna multiple nessuna multiple multiple singola multiple multiple multiple multiple nessuna nessuna nessuna multiple multiple multiple nessuna nessuna singola nessuna multiple nessuna multiple singola tabella 3 caratteristiche dellevento traumatico meccanismo del trauma frattura di bacino classificazione secondo tile radiol med ( 2010 ) 115 : 648667 fig . 
a ricostruzione tcmd 3d del bacino : frattura instabile con ampia diastasi della sinfisi pubica e dellarticolazione sacro - iliaca destra ; la scansione tcmd assiale b mostra uno stravaso di mdc nel territorio dellarteria otturatoria destra . 
a mdct 3d reconstruction shows an unstable pelvic fracture with a large symphysis pubis diastasis , b axial ct scan shows a large amount of active bleeding from the right pelvic sidewall . 
3a - e paziente traumatizzato con lacerazione dellarteria ipogastrica destra : a la ricostruzione tcmd 3d del bacino mostra una frattura instabile con ampia diastasi della sinfisi pubica e la scansione tcmd della pelvi b evidenzia un ampio stravaso di mdc nel territorio di distribuzione dellarteria ipogastrica destra . 
a ricostruzione tcmd 3d del bacino : frattura instabile con diastasi della sinfisi e dellarticolazione sacro - iliaca destra ; le scansioni tcmd assiali mostrano b sanguinamento attivo nel territorio di distribuzione distale dellarteria pudenda interna sinistra e c sanguinamento attivo in sede perineale sinistra . 
b axial ct scan shows active extravasation at the level of the right iliac muscle and of the left gluteal region with a large haematoma of the left flank , and c active bleeding in the left gluteal region . 
5a - e paziente traumatizzato con lacerazione dellarteria glutea sinistra ; a ricostruzione tcmd 3d del bacino : frattura instabile con diastasi della sinfisi pubica e dellarticolazione sacro - iliaca . 
scansioni assiali mdct : b stravaso attivo di mdc nel muscolo iliaco destro e gluteo sinistro , con ampio ematoma della parete del fianco sinistro , e , c , stravaso attivo di mdc nel territorio di distribuzione dellarteria glutea sinistra . 
 discussione la struttura portante dellanello pelvico il cosiddetto complesso sacro - iliaco posteriore costituito dai legamenti inter - ossei sacro - iliaci , dalle porzioni posteriori del sacro , dalle articolazioni sacro - iliache e dagli ilei . 
il riconoscimento di una frattura pubica sta comunque ad indicare la necessit di studiare il complesso sacro - iliaco posteriore , giacch la configurazione ad anello della pelvi comporta che ad ogni lesione ossea ne corrisponde unaltra ( ossea , legamentosa e / o vascolare ) sul versante opposto [ 12 , 13 ]  . 
le fratture pelviche invece , sono caratterizzate dallinterruzione dellanello pelvico in due o pi punti : quelle pi gravi possono causare shock ipovolemico , talora mortale , per grave sanguinamento da concomitanti lesioni vascolari [ 7 ]  . 
nella nostra serie di 28 pazienti con trauma della pelvi , il meccanismo del trauma risultato di tipo decelerativo in 42 , 8% dei casi , diretto ( 28 , 6% ) , caduta dallalto ( 14 , 3% ) , di tipo compressivo ( 10 , 7% ) e di tipo penetrante ( 3 , 6% ) : lesioni di tipo fratturativo del bacino sono state identificate allesame tcmd nel 64 , 3% dei casi . le fratture dellanello pelvico sono frequentemente associate ad altre lesioni traumatiche a carico del cranio , del torace , delladdome ( nella nostra casistica lesioni traumatiche toraco - addominali associate sono state identificate allesame tcmd nell85 , 7% dei casi ) e particolarmente delle diramazioni vascolari della pelvi : questultime soprattutto in caso di coinvolgimento di vasi arteriosi , possono causare lexitus del paziente [ 13 ]  . 
si tratta soprattutto di lesioni di tipo arterioso , giacch quelle venose , tranne in rari casi di interessamento dei rami iliaci comuni , provocano sanguinamenti a basso flusso che si autolimitano e vanno incontro generalmente a tamponamento spontaneo ; radiol med ( 2010 ) 115 : 648667 involvement , can lead to death [ 13 ]  . 
these are for the most part arterial lesions , as venous lesions tend to cause lowflow bleeding that tends to be self - limiting and generally undergoes spontaneous compression , except in rare cases involving the common iliac branches . 
nonetheless , the incidence of venous trauma , as with arterial trauma , should not be underestimated , as it is probably higher than reported in the literature [ 1618 ]  . 
in patients with unstable pelvic fractures and a drop in haematocrit , an mdct examination is mandatory , as it is able to detect even minimal hairline fractures as well as localise the source of bleeding , thus enabling identification of the more severe cases of pelvic trauma , for which treatment of the vascular injury with embolisation or surgery is a priority compared with treatment of skeletal lesions [ 19 ]  . 
the presence of active indispensabile tuttavia lincidenza di traumi venosi , analogamente a quelli arteriosi , non deve essere sottostimata poich probabilmente pi alta di quella riportata in letteratura [ 1618 ]  . nei pazienti con fratture pelviche di tipo instabile e calo del valore dellematocrito lesecuzione dellindagine tcmd che consente non solo di individuare anche minime rime di frattura , ma soprattutto di localizzare topograficamente la fonte di sanguinamento , permettendo di selezionare i casi con trauma pelvico pi grave per i quali prioritario il trattamento delle lesioni vascolari ( mediante embolizzazione oppure mediante intervento chirurgico ) rispetto al trattamento delle lesioni scheletriche [ 19 ]  . 
infatti allesame tcmd la presenza di stravaso attivo di mdc ev altamente predittiva di lesione di un vaso arterioso che richiede un trattamento angiografico di tipo embolizzante con valori di sensibilit pari a 66%90% , di table 5 associated traumatic lesions detected at multidetector - row computed tomography ( mdct ) no . 
the internal iliac artery and its branches in fact run in close contact with the pelvic structures and can frequently be damaged after pelvic trauma with or without associated fractures . 
in our series of 28 patients , the most frequently lacerated arteries identified at angiography were the obturator ( n = 9 ) , the internal iliac specificit pari a 85%98% e di accuratezza pari a 87%98% [ 6 , 2023 ]  . 
nella nostra casistica lesame tcmd ha consentito di evidenziare la presenza di sanguinamento attivo nel 75% dei casi e la fase di studio postcontrastografico in cui pi frequentemente stato rilevato il sanguinamento attivo risultata la fase tardiva ( 61 , 9% )  . in pazienti con trauma del bacino , le strutture arteriose pi frequentemente interessate da lacerazioni traumatiche sono le diramazioni dellarteria iliaca interna ( o ipogastrica ) , meno spesso dellarteria iliaca esterna . 
larteria iliaca interna con i suoi rami decorre , infatti , a stretto contatto con le strutture del bacino e frequentemente pu essere danneggiata dopo traumi pelvici associati o meno a fratture ossee . 
nella nostra casistica relativa a ventotto pazienti , le arterie pi frequentemente lese sono risultate , allesame angiografico , larteria otturatoria ( 9 casi ) , larteria iliaca interna ( 6 casi ) , larteria pudenda interna ( 6 casi ) e larteria glutea superiore ( 5 casi )  . 
in our series , the most frequent associated pelvic lesions were muscular . mdct is the diagnostic imaging modality of choice in major trauma thanks to its short examination time , high diagnostic power especially in the early identification of active bleeding possibility of multiplanar and 3dreconstructions and the possibility of evaluating local lesions and / or lesions to other anatomical districts [ 10 ] associated with the pelvic vascular and bone lesions . in polytrauma patients with pelvic vascular lesions , angiography is essentially used for therapeutic purposes , even though it includes a diagnostic phase with the visualisation of both external and internal common iliac arteries , which in the field of view encompasses the bony structures of the pelvis , including the coxofemoral joints . 
however , this causes a reduction in the natural compression exerted by the retroperitoneal fascia and by the haematoma on the source of bleeding , with an elevated risk of a sudden and significant increase in haemorrhage , which can lead to the death of the patient on the operating table [ 27 , 28 ]  . conclusions in polytrauma patients , mdct provides a complete study of bone , visceral and especially vascular lesions . 
thanks to the use of intravenous contrast material and the mdct angiography study technique , this modality is able to identify the presence of active bleeding with the possibility in some cases of defining the source of the blood loss . 
high - quality 2d and 3d multiplanar reconstructions also provide a reliable vascular map of the anatomical structures , which can guide the interventional radiologist in rapidly identifying the injured vessel and subsequently embolising it . 
the lesioni viscerali ( lesioni muscolari , dei mesi , dellintestino , della vescica e dellapparato genitale ) e neurologiche ( lesioni del nervo sciatico , ad esempio ) [ 2426 ]  . 
 la tcmd rappresenta lindagine diagnostica di scelta nel trauma maggiore per lelevata rapidit di esecuzione , lelevato potere diagnostico in particolare nellidentificazione precoce dei segni di sanguinamento attivo , la possibilit di ricostruzioni multiplanari e tridimensionali e la possibilit di valutazione delle lesioni locali e / o dei restanti distretti anatomici [ 10 ] associate a quelle vascolari ed ossee della pelvi . 
 nei pazienti politraumatizzati con trauma vascolare della pelvi , langiografia ha oggi una finalit essenzialmente terapeutica , anche se prevede comunque una fase di studio anche di tipo diagnostico con la visualizzazione di entrambi gli assi arteriosi iliaci comuni , esterni ed interni che comprende nel campo di vista le strutture ossee della pelvi , incluse le articolazioni coxo - femorali . 
nei casi gravi di trauma con paziente in stato di shock ipovolemico , lembolizzazione della fonte emorragica spesso non selettiva e prevede la tempestiva occlusione del vaso principale alla sua origine ( ad esempio larteria ipogastrica ) ed in alcuni casi , per fermare completamente il sanguinamento anche dei rami collaterali , si procede allocclusione di entrambe le arterie ipogastriche come procedura salvavita per il paziente . limportanza del trattamento embolizzante come procedura esclusiva delle lesioni traumatiche arteriose deriva anche dalle difficolt di arrestare lemorragia mediante trattamento chirurgico laparotomico convenzionale . 
infatti lintervento chirurgico prevede lapertura del retroperitoneo per lisolamento dei vasi lesi : questa manovra , determina una riduzione delleffetto di tamponamento naturale esercitato dalle fasce retroperitoneali e dallematoma sulla fonte emorragica con elevato rischio di un imponente improvviso incremento dellemorragia che pu condurre a morte il paziente sul tavolo operatorio [ 27 , 28 ]  . 
grazie allutilizzo del mdc ev ed alla tecnica di studio di angiografia - tcmd essa permette di riconoscere la presenza del sanguinamento attivo con possibilit , in alcuni casi , di definire anche la sede della perdita ematica . 
le ricostruzioni multiplanari 2d e 3d di elevata qualit forniscono anche una mappa vascolare fedele alla realt anatomica che costituisce unutile guida al radiologo interventista per la rapida individuazione del vaso leso ed il successivo trattamento embolizzante . 
among 534 patients with s - oiv , according to the us centers for disease control and prevention case definition , seen between june and november 2009 , 121 underwent chest x - ray and 40 ( median age 44 years , range 1679 ) had pneumonia . 
however , s - oiv can cause severe illness requiring admission to the intensive care unit for advanced mechanical ventilation and extracorporeal life support , including adult respiratory distress syndrome ( ards ) and death . 
nel periodo compreso tra giugno e novembre 2009 abbiamo identificato , mediante radiografia del torace , 40 polmoniti in pazienti con influenza a ( h1n1 ) , ( et mediana 44 anni , range 1679 anni )  . 
i radiogrammi relativi allesame del torace effettuato al momento del ricovero e la tomografia computerizzata , eseguita in due casi , sono stati valutati relativamente al quadro di presentazione , alla distribuzione e allestensione delle anormalit identificate . 
nella nostra casistica , i pazienti hanno presentato prevalentemente un quadro clinico di media gravit e la polmonite ha complicato linfluenza in 40 di essi ( 40 / 121 [ 33% ] pazienti con radiografia del torace e 40 / 534 [ 7 , 5% ] pazienti con influenza a )  . 
in questi casi pu rendersi necessario il ricovero presso reparti di rianimazione , poich linfluenza pu provocare complicazioni gravi fino alla acute respiratory distress syndrome ( ards ) e alla morte . 
il quadro di presentazione radiologica pi frequentemente osservato stato limpegno interstiziale ( 60% ) , con ( 22% ) o senza consolidamenti multifocali a vetro smerigliato , bilaterali ( 70% ) e localizzati nei campi polmonari inferiori ( 70% )  . 
alterazioni parenchimali diffuse sono state identificate nel 37 , 5% dei casi ( 15 / 40 ) e la ards si manifestata in tre pazienti ( 7 , 5% ) , tutti con comorbilit . 
in our series , the most frequent pneumonia patterns observed during s - oiv ( h1n1 ) virus were interstitial changes and patchy ground - glass appearance , mostly bilateral , and located in the lower lung zones . 
la tomografia computerizzata , effettuata nei pazienti in condizioni cliniche gravi , ha confermato la ards , gi identificata mediante la radiografia del torace , definendone meglio lestensione e le caratteristiche semeiologiche . 
 parole chiave influenza a ( h1n1 ) polmoniti virali radiografia del torace tc introduction introduzione swine - origin influenza a virus ( s - oiv ) ( h1n1 ) was first reported in mexico in late march 2009 , and rapidly spread throughout the world . 
epidemiological data suggest that the newly emerged h1n1 virus had relatively low virulence [ 1 ]  . it is believed that the mechanism of transmission of s - oiv is predominantly by droplet secretions [ 2 ]  . 
the clinical manifestations mostly consist of mild illness [ 3 ] , even though , as in the case of seasonal influenza [ 4 , 5 ] , s - oiv can cause severe illness and death , above all in persons with underlying medical conditions . 
in this paper , we review the chest radiographic and computed tomography ( ct ) findings observed in 40 individuals with pneumonia and s - oiv h1n1 infections . linfluenza suina a h1n1 ( s - oiv ) stata identificata per la prima volta in messico , nel marzo 2009 , e si successivamente diffusa in tutto il mondo con caratteristiche di una pandemia . 
s - oiv si manifesta come malattia di media severit [ 3 ] , in persone con comorbilit pu per decorrere in forma grave , anche mortale , analogamente a quanto avviene per linfluenza stagionale [ 4 , 5 ]  . il ruolo della diagnostica per immagini quello di rilevare la comparsa di complicazioni polmonari , identificando precocemente quelle con evoluzione sfavorevole . 
scopo del presente lavoro stato valutare i quadri radiologici rilevati in 40 soggetti con polmonite da influenza suina . materials and methods between june and november 2009 , 534 patients fulfilling the us centers for disease control and prevention ( cdc ) clinical criteria for the diagnosis of s - oiv [ 6 ] were observed in our institution . 
s - oiv was subsequently confirmed by polymerase chain reaction ( pcr ) in all these individuals . the study population included 24 men , median age 44 years ( range 1679 years )  . 
all patients had temperature > 38c and one or more clinical findings of respiratory illness . seventeen patients ( 42% 17 / 40 ) had one or more underlying medical conditions [ obesity , hiv infection , chronic obstructive pulmonary disease ( copd ) , bronchial asthma , fibrosis or diabetes ]  . chest radiographs were obtained on admission using conventional radiography in the two standard projections or performed at the bedside in the anteroposterior projection . materiali e metodi presso listituto l . 
spallanzani di roma , nel periodo compreso tra giugno e novembre 2009 , linfluenza suina stata accertata in 534 pazienti , aderendo ai criteri dei centers for disease control and prevention ( cdc ) [ 6 ]  . 
la nostra casistica si compone pertanto di 24 uomini e 16 donne con et mediana di 44 anni ( range , 1679 anni ) ; in tutti i casi s - oiv stata confermata con lidentificazione del virus mediante polymerase chain reaction ( pcr ) dedicata . 
in 17 soggetti coesistevano una o pi condizioni di comorbilit ( obesit , infezione da virus per limmunodeficienza umana [ hiv ] , chronic obstructive pulmonary disease [ copd ] , asma bronchiale , fibrosi , diabete )  . gli esami radiografici del torace eseguiti al momento del ricovero sono stati effettuati nelle 2 proiezioni standard , radiol med ( 2010 ) 115 : 507515 the admission chest radiographs in the standard posteroanterior and lateral views were obtained with opera g 650 rad - rt20 radiographic equipment ( general medical merate , seriate , italy ) at 110140 kv , 12 mas and 200cm film - focus distance . 
the anteroposterior bedside radiographic examinations were performed with portable equipment tmxr plus ( general electric medical system , milwaukee , wi , usa ) using 90 kv , 5 mas and 150 - cm film - focus distance . 
images were evaluated on high - resolution monitors ( 2 , 0482 , 560 pixels , display gradation 1 , 021 ( 10 - bit ) , maximum brightness 750 cd / m2 , lcd display device 54 cm ) of the picture archiving and communications system ( pacs 5.1 , kodak carestream , rochester , ny , usa )  . 
ct scans were displayed on monitors with window setting appropriate for lung parenchyma and mediastinum ( 2 , 0482 , 560 pixels , display gradation 1 , 021 , 10 - bit ) , maximum brightness ( 750 cd / m2 , lcd display device 54 cm ) of the pacs syste three experienced , board - certified radiologists ( lr , ebr , vs ) independently reviewed the radiographs obtained on admission , and consensus was reached in all cases . the chest radiographs and ct scan were assessed for the presence and distribution of the following findings : ( 1 ) reticular opacities , ( 2 ) ground - glass opacities , ( 3 ) nodular opacities , ( 4 ) parenchymal consolidation , ( 5 ) pleural effusion , and ( 6 ) adenopathies . 
in accordance with the fleischner society glossary [ 7 , 8 ] , reticular opacities were defined as linear opacities forming a mesh - like pattern , which may be thin or thick and coarse . 
nodular opacities were defined as focal round opacities , with a diameter no greater than 7 mconsolidation was an opacification of the parenchyma with obscuration of the underlying anatomical structures . 
the predominant distribution was also assessed as being in the upper ( above the level of the anterior end of the third rib ) , middle ( between the third and fifth anterior ribs ) or lower ( below the level of the anterior end of the fifth rib ) lung zones . 
 con apparecchio opera g 650rad - rt20 ( general medical merate , seriate , italia ) parametri di esposizione 110140 kv e 12 mas , distanza fuoco - film 200 c i radiogrammi ottenuti al letto del paziente , in proiezione antero - posteriore , sono stati effettuati con apparecchio portatile tmxr plus ( general electric medical system , milwaukee , usa ) , 90 kv , 5 mas , distanza fuoco - film 150 cla valutazione delle immagini stata effettuata alla workstation del picture archiving and communication system ( pacs ) 5.1 ( kodak carestream , rochester , ny , usa ) con schermi ad alta definizione ( pixel 20482560 , display gradation 1021 ( 10 - bit ) , maximum brightness 750 cd / m2 , lcd display device 54 cm )  . 
 in tre casi lo studio radiografico stato integrato con tomografia computerizzata ( tc ) , effettuata con tecnica volumetrica senza somministrazione di mezzo di contrasto , mediante scanner multidetettore ( hispeed scanner , general electric medical system , milwaukee , usa ) , ( 15 mm / s , 5 mm collimazione , 5 mm intervallo di ricostruzione , 120 kv , 140 ma )  . 
le immagini sono state interpretate ( pacs 5.1 kodak carestream , rochester , ny , usa ) con finestre appropriate per il parenchima e per il mediastino ( pixel 20482560 , display gradation 1021 , 10 - bit , 750 cd / m2 , lcd display device 54 cm )  . 
in accordo con il glossario della fleischner society [ 7 , 8 ] , reticolari sono state definite le opacit lineari disposte a formare un reticolo , con setti interlobulari sottili o spessi ; a vetro smerigliato stata definita lopacit nel cui contesto stato possibile valutare i vasi , i bronchi sottostanti e le coste regionali sovrapposte ; opacit nodulari sono state definite quelle focali rotondeggianti , con diametro non eccedente i 7 mm ; consolidamento stato definito lopacit parenchimale densa , con cancellazione delle strutture anatomiche sottostanti / locoregionali . 
la distribuzione predominante stata inoltre valutata relativamente alla sede polmonare coinvolta , come superiore ( sotto il bordo anteriore della 3a costa ) , media ( tra il bordo anteriore della 3a e della 5a costa ) e inferiore ( al di sotto del bordo anteriore della 5a costa )  . 510 results risultati radiol med ( 2010 ) 115 : 507515 all chest radiographs obtained on admission were interpreted prospectively and retrospectively as abnormal . 
patients = 40 percent interstitial changes ground - glass opacities ( ggo ) centrilobular nodules consolidation dystelectasis ggo + consolidation ggo + interstitial changes mixed pattern acute respiratory distress syndrome distribution unilateral involvement bilateral involvement extent on initial imaging focal patchy diffuse ( 3 or more involved zones ) predominance upper zones middle zones lower zones pleural effusion impegno interstiziale opacit a vetro smerigliato ( vs ) noduli centrolobulari consolidamenti distelectasie consolidamenti + vs impegno interstiziale + vs quadri misti acute respiratory distress syndrome distribuzione unilaterale bilaterale estensione nel primo esame radiografico focale multifocale diffusa ( 3 o pi zone ) predominanza campi polmonari superiori campi polmonari medi campi polmonari inferiori versamento pleurico tabella 1 segni radiografici e di tc in pazienti con polmonite e influenza suina quadri radiologici numero pazienti = 40 percentuale radiol med ( 2010 ) 115 : 507515 fig . 
 two patients with severe illness and ards identified on chest radiography were also studied with ct , which confirmed the ards pattern , better depicting the features and extent of lung abnormalities . 
in 4 pazienti abbiamo identificato un versamento pleurico di modesta entit . due pazienti con malattia clinicamente grave e ards identificato con la radiografia del torace , sono stati studiati anche con tc , che ha meglio rilevato la presenza e lestensione delle anormalit polmonari gi rilevate . 
la tc conferma la presenza di ards , gi rilevata mediante la radiografia del torace , meglio rappresentandone lestensione e gli aspetti semeiologici . radiol med ( 2010 ) 115 : 507515 discussion influenza virus belongs to the orthomyxovirus family of rna viruses , and human disease is predominantly caused by type a , the most virulent , which can easily mutate [ 9 ]  . 
the 2009 h1n1 virus contained a unique combination of gene segments that had not previously been identified in humans or animals [ 10 , 11 ]  . whereas the elderly and young children are at high risk for seasonal influenza , h1n1 - related illness predominantly affects young individuals . 
the possible explanation for this phenomenon includes the fact that the young have a greater susceptibility to the virus , as proven on the basis of serological studies [ 12 , 13 ]  . 
however , it is also possible that there is a case - ascertainment bias because more young people are tested as part of outbreak investigations in schools [ 15 ] the majority of s - oiv infections reported has been mild illness . 
one contributing factor for death during h1n1 infection may be delayed admission and / or delayed initiation of therapy [ 16 , 19 ]  . concurrent bacterial infection does not appear to be a contributing factor to the severity of illness , and lung damage was mostly due to the primary effect of infection with influenza virus [ 1619 ]  . 
esistono una grande quantit di sottotipi del virus a , identificati per la presenza di glicoproteine , emoagglutinine ( h ) e neuraminidasi ( n ) , sulla membrana di superficie . 
i dati statistici potrebbero comunque essere inquinati per un errore di campionamento , che viene effettuato prevalentemente nei giovani , in corrispondenza dellinsorgenza di epidemie scolastiche [ 15 ]  . la maggior parte delle influenze suine segnalate hanno presentato un decorso clinico di media gravit , ma il virus h1n1 in grado di provocare malattia grave con polmonite e ards [ 1619 ]  . 
i fattori di rischio correlati allinsorgenza di malattia grave sono : lobesit , le malattie cardiache , neurologiche e polmonari pre - esistenti , limmunosopressione , la gravidanza [ 1619 ]  . un ritardo nel ricovero e / o nellinizio della terapia rappresentano un fattore prognostico negativo fino al decesso [ 16 , 19 ]  . 
i possibili meccanismi di danno includono infatti lazione del virus sullepitelio respiratorio , diretta e indiretta per la successiva liberazione di citochine nellambito di complessi meccanismi flogistici [ 22 ]  . i segni radiologici della polmonite virale consistono di alterazioni interstiziali , opacit a vetro smerigliato , noduli centrolobulari , consolidamenti , variamente rappresentati , e riflettono la presenza e lestensione dei fenomeni istopatologici sottostanti [ 23 ]  . 
necrosi e desquamazione dellepitelio nel lume bronchiale , in concomitanza con lessudazione endoluminale , 514 radiol med ( 2010 ) 115 : 507515 interstitial thickening may produce reticular or linear opacities . 
variable extension and amount of exudate occur . imaging findings are ground - glass opacities or dense consolidations . rapidly progressive pneumonia may be seen , particularly in patients with underlying medical conditions ; in these cases , the lung histologically shows diffuse alveolar damage , comprising interstitial lymphocyte infiltration , airspace haemorrhage , oedema and hyaline membrane formation [ 26 , 27 ]  . 
in our series , the major radiological abnormalities were interstitial changes , with or without patchy ground - glass opacities and centrilobular nodules , mostly bilateral and located in the lower lung zones . 
these data differ considerably from the literature data [ 1619 ] in which the most prevalent pattern is patchy ground - glass opacities , more frequently bilateral and located in lower zones . 
 in our series , extensive lung abnormalities with involvement of three or more lung zones were observed in 37.5% of patients , and ards was observed in three patients , all with underlying medical conditions . 
ct was performed only three times in our series , as it is known that it does not add information in patients with evident radiographic abnormalities , leading to only a modest increase in diagnostic accuracy [ 29 , 30 ]  . 
on the contrary , incipient and / or overt ards should be further investigated with ct , which is more sensitive and specific than radiography for detecting thoracic abnormalities and may be useful for guiding treatment decisions in critical patients , providing a more accurate evaluation of the extent and distribution of the disease . in conclusion , s - oiv - related pneumonia does not differ in radiographic presentation from the other viral pneumonias , and it may evolve into ards . 
chest radiograph is an effective and adequate tool for identifying s - oiv - related pneumonia , whereas ct is helpful in individuals with severe illness to depict incipient ards and to orient prompt therapeutic management . 
 nei soggetti con comorbilit levoluzione della polmonite pu essere rapidamente ingravescente per la comparsa di un danno alveolare con aspetti anche emorragici , formazione di membrane ialine e concomitante impegno interstiziale [ 26 , 27 ]  . 
il versamento pleurico non frequente . i dati desumibili dalla letteratura [ 1619 ] mostrano che anche nella polmonite correlata allinfluenza suina , la presentazione radiologica quella aspecifica delle polmoniti virali , ma mentre nella nostra casistica le alterazioni identificate con maggiore frequenza sono state quelle interstiziali , pi spesso bilaterali e con prevalente impegno dei campi polmonari inferiori , il quadro di presentazione pi frequentemente rilevato dalla letteratura [ 1619 ] , stato il consolidamento multifocale a vetro smerigliato , pi spesso bilaterale e localizzato nei campi polmonari inferiori . nel 37 , 5% dei nostri casi la malattia stata diffusa , coinvolgendo 3 o pi campi polmonari e in 3 pazienti la polmonite si complicata per la comparsa di ards . 
noto che la tc , nei casi in cui la presenza di patologia polmonare sia gi stata rilevata mediante radiografia del torace , non aggiunge un significativo incremento di accuratezza diagnostica [ 29 , 30 ]  . 
nella nostra esperienza la tc stata effettuata solo 3 volte , in 2 soggetti con clinica rapidamente ingravescente , per i quali la precoce identificazione del tipo e dellentit delle alterazioni polmonari ha comportato una modificazione nelle scelte terapeutiche . in conclusione , la presentazione radiologica della polmonite da virus dellinfluenza suina non differisce dalle altre polmoniti virali e lards pu rappresentarne la temibile evoluzione . 
rubaltelli1 1dipartimento di scienze medico diagnostiche e terapie speciali universit degli studi di padova , via giustiniani 2 , padova , italy 2dipartimento di ingegneria clinica , 3unit valutazione technology assessment , azienda ospedaliera di padova , padova , italy correspondence to : r . 
surface transducers showed worse performance in terms of image uniformity , with 7 / 55 ( 13% ) transducers rated poor , and depth of penetration , with 24 / 55 ( 44% ) transducers , rated sufficient or poor . 
sono state testate 116 sonde ecografiche tramite lutilizzo di un fantoccio ; il controllo avvenuto su parametri relativi ad immagini acquisite in b - mode e i risultati ottenuti sono stati suddivisi in 3 classi , assegnando per ciascun parametro il giudizio buono , accettabile o scarso . 
le sonde superficiali hanno dimostrato una performance peggiore nelluniformit con 7 / 55 ( 13% ) sonde scarse e nella profondit di penetrazione con 24 / 55 ( 44% ) sonde accettabili o scarse . 
le sonde da 3 , 5 mhz hanno dimostrato una performance peggiore nella risoluzione laterale , con 18 / 48 ( 38% ) sonde scarse e ancor pi nella focalizzazione con 40 / 48 ( 83% ) sonde scarse ; inoltre le sonde da 3 , 5 mhz si sono dimostrate meno accurate nella misurazione delle distanze in direzione verticale , con 31 / 48 ( 64% ) sonde accettabili , piuttosto che in direzione orizzontale . 
lo scopo principale di un controllo di qualit in ecografia caratterizzare specifici parametri che valutino la performance delle apparecchiature e , nel caso radiol med ( 2010 ) 115 : 668677 keywords ultrasound technology assessment quality control in cui le valutazioni discostino dai livelli di tolleranza proposti , porre lindicazione ad azioni correttive . parole chiave ecografia technology assessment controllo di qualit introduction introduzione recommendations for implementing quality control in ultrasound have been made by the major international scientific bodies , including the american institute of ultrasound in medicine ( aium ) , the american association of physicists in medicine ( aapm ) and the international electrotechnical commission ( iec ) [ 1 ]  . 
the need for planning these programmes is justified by the physical deterioration that unavoidably occurs to the equipment over the years and that inevitably leads to loss in image quality . 
by performing quality control tests , the number of repeat examinations can be reduced , and just as importantly , diagnosis can be made more accurately [ 25 ]  . 
in this setting , it should be noted that deterioration in image quality is generally not perceived by the operator constantly working with the same ultrasound systewith the use of technical assessment instruments ( phantoms ) , which are built to obtain a predetermined image with constant reference features , objective assessment parameters can be analysed , and reproducible measurements can be provided [ 3 , 68 ]  . 
technical assessment parameters , with regard to b - mode imaging , refer to criteria formulated by the aapm [ 1 , 3 , 7 , 9 ] and are recognised by the aium as a standard of reference . 
it should be borne in mind that tolerance values proposed for various parameters only constitute a general guideline [ 3 ]  . the aim of our study was to develop a quality control protocol by defining objective assessment criteria and valid methods for possible monitoring over time , as well as to evaluate specific parameters to ascertain functional efficiency of ultrasound systems and transducers . ( aapm ) e le raccomandazioni allo svolgimento di controlli di qualit in ecografia provengono dalle maggiori societ scientifiche internazionali , tra cui lamerican institute of ultrasound in medicine ( aium ) , lamerican association of physicist in linternational eletrotechnical medicine commission ( iec ) [ 1 ]  . 
la necessit di pianificare tali programmi giustificata dal deterioramento fisico a cui , necessariamente , vanno incontro negli anni le apparecchiature , e che , inevitabilmente , porta ad un peggioramento della qualit dellimmagine : lattuazione di un controllo di qualit pu , in questo senso , ridurre il numero di indagini ripetute e , nondimeno , rendere pi accurata la diagnosi [ 25 ]  . 
a tal proposito va ricordato che il degrado della qualit dellimmagine non viene in genere percepito da un operatore che lavora sempre con la stessa apparecchiatura ; attraverso lutilizzo di strumenti tecnici di valutazione , i fantocci , costruiti in modo da ottenere unimmagine predeterminata con elementi di riferimento costanti , vengono analizzati parametri oggettivi di valutazione e fornite misurazioni riproducibili [ 3 , 68 ]  . 
i parametri tecnici di valutazione , relativi allimmagine b - mode , fanno riferimento a criteri espressi dallamerican association of physics [ 1 , 3 , 7 , 9 ] e sono riconosciuti dallaium come standard di riferimento ; da tener presente che i valori di tolleranza proposti per i vari parametri costituiscono solo unindicazione di massima [ 3 ]  . scopo del nostro studio stato quello di definire un protocollo di controllo di qualit stabilendo criteri oggettivi di valutazione e modalit valide per un eventuale monitoraggio nel tempo ; constatare , inoltre , attraverso la valutazione di specifici parametri , quali fossero le prestazioni funzionali degli ecografi e delle sonde . materials and methods in agreement with the clinical engineering service , quality control tests were performed in 2008 on ultrasound equipment within a single hospital . 
overall , the assessment materiali e metodi in accordo con il servizio di ingegneria clinica nel 2008 stato espletato un controllo di qualit delle apparecchiature ecografiche presenti allinterno di un unica azienda ospedaliera . 
la verifica avvenuta su un totale di 56 apparecchi , ed in tutto sono state testate 116 sonde ecografiche di vari tipi , modelli e frequenze : sono state incluse sonde convex ( frequenza centrale da 3 , 5 mhz ) , superficiali lineari ( frequenza centrale da 7 , 5 mhz e da 13 , 5mhz ) ed endocavitarie ( frequenza centrale da 6 , 5 mhz ) ; sono state escluse le sonde settoriali . 
sono state complessivamente testate 48 670 radiol med ( 2010 ) 115 : 668677 involved 48 transducers with a frequency of 3.5 mhz ( 41% ) , 44 with a frequency of 7.5 mhz ( 38% ) , 11 with a frequency of 13.5 mhz ( 9% ) and 13 with a frequency of 6.5 mhz ( 11% )  . all tests were performed by the same operator with the use of computerized imaging reference systems ( cirs ) model 054 phantom constructed from zerdine , which mimics the acoustic properties of hepatic tissue and contains the fundamental target groups , i.e. 
il protocollo si limitato al controllo dei parametri relativi ad immagini statiche tradizionali , acquisite in bmode ; in particolare la valutazione avvenuta su : uniformit , massima profondit di penetrazione , zona morta , accuratezza dei calibri orizzontali , accuratezza dei calibri verticali , risoluzione assiale , risoluzione laterale , focalizzazione , fig . 
1a the model 054 phantom , produced by cirs , is constructed from zerdine , which simulates the acoustic properties of hepatic tissue and is housed in rugged abs plastic . 
1a il fantoccio modello 054 , prodotto da cirs , costituito da zerdine che simula le propriet acustiche di un tessuto epatico ed contenuto allinterno di una robusta scatola di plastica . 
b rappresentazione schematica dei target groups contenuti allinterno del fantoccio : target verticale , target orizzontale , target di risoluzione assiale , target della zona morta , lesione solida e lesione cistica . 
c immagine ecografica , ottenuta con una sonda da 3 , 5 mhz , che mostra i target groups contenuti nel materiale simil - epatico . radiol med ( 2010 ) 115 : 668677 vertical distance accuracy , axial resolution , lateral resolution , focusing , and analysis of an anechoic and a hyperechoic target . valutazione dei parametri analisi di pseudo - cisti , analisi di inserto iperecogeno . parameter evaluation evaluation of image uniformity was subjective . 
the parameter was rated good if echoes of the same size and depth showed equal luminosity on the monitor , and poor if there was discontinuity in the area of interest . 
the depth of penetration corresponded to the point at which the last visible echo appeared within the phanto penetration depth was rated good if it was > 16 cm for transducers with a central frequency of 2.5 mhz , > 13 cm for frequencies between 2.5 and 5 mhz , > 6 cm for frequencies between 5 and 8 mhz and > 4 cm for frequencies between 8 and 12 mhz . 
a rating of sufficient was given if values were < 1 cm lower than the above values , and poor if they were > 1cm lower than the above values . 
the following assessments were made : good if = 1 mm , and poor if > 1 min addition , transducers that demonstrated reverberation artefacts within the dead zone were counted . with regard to horizontal distance accuracy , which was only assessed for the 3.5 - mhz transducers , each distance between adjacent points on a horizontal target was measured . 
an assessment of good was given for 3.5 - mhz and 6.5 - mhz transducers with an axial resolution of 1 mm and for 7.5 - mhz transducers with an axial resolution of 0.5 man assessment of poor was given if the transducers had an axial resolution greater than the above values . 
an assessment of good was given for 3.5 - mhz and 6.5 - mhz transducers with a lateral resolution 3 mm and for 7.5 - mhz and 13.5 - mhz transducers with a lateral resolution of 1.5 m an per quanto riguarda luniformit la valutazione stata soggettiva ; veniva assegnato il giudizio : buono se gli echi della stessa grandezza e profondit mostravano uguale luminosit sul monitor ; scarso se si evidenziavano discontinuit nella zona di interesse . 
la massima profondit di penetrazione corrispondeva al punto in cui allinterno del fantoccio si visualizzava lultimo eco visibile ; venivano assegnati i seguenti giudizi : buono se > 16 cm per trasduttori con frequenza centrale di 2 , 5 mhz , se > 13 cm per frequenz tra 2 , 5 e 5 mhz , se > 6 cm per frequenze tra 5 e 8 mhz , se > 4 cm per frequenze tra 8 e 12 mhz ; accettabile se i valori erano inferiori di meno di un centimetro rispetto a quelli sopra riportati ; scarso se i valori specificati erano inferiori di pi di un centimetro rispetto a quelli sopra indicati . 
nella valutazione della zona morta veniva registrata la distanza dalla superficie del trasduttore alleco identificabile pi vicino ; venivano espressi i seguenti giudizi : buono se = 1 mm ; scarso se > 1 minoltre sono state contate le sonde che mostravano fenomeni di riverbero allinterno della zona morta . per quanto riguarda laccuratezza dei calibri orizzontali , analizzata solo sulle sonde da 3 , 5 mhz , veniva misurata , sul target orizzontale , ogni distanza tra due punti contigui e tenendo conto che la distanza tra un pin e laltro era di 20 mm veniva espresso il giudizio : buono se ogni distanza risultava 18 e 22 mm ( errore accettato = 10% , cio 2 mm ) ; accettabile se una distanza aveva un errore > 10% ; scarso se pi di una distanza aveva un errore > 10% . 
laccuratezza dei calibri verticali veniva analizzata sul target verticale ; tenendo conto che la distanza tra un pin e laltro era di 20 mm veniva espresso il giudizio : buono se ogni distanza risultava 18 , 5 e 21 , 5 mm ( errore accettato = 7 , 5% , cio 1 , 5 mm ) ; accettabile se una distanza aveva un errore > 7 , 5% ; scarso se pi di una distanza aveva un errore > 7 , 5% . 
la risoluzione assiale corrispondeva allultimo paio di punti percepiti come due entit separate nel relativo target e veniva espresso il giudizio : buono per le sonde con frequenza da 3 , 5 e 6 , 5 mhz che avevano una risoluzione assiale di 1 mm e per le sonde con frequenza da 7 , 5 e 13 , 5 mhz che avevano una risoluzione assiale di 0 , 5 mm ; scarso se le sonde avevano una risoluzione assiale maggiore rispetto ai valori sopra indicati . 
venivano assegnati i seguenti giudizi : buono per le sonde con frequenza da 3 , 5 e 6 , 5 mhz che avevano una risoluzione laterale 3 mm e per le sonde con frequenza da 7 , 5 e 13 , 5 mhz che avevano una risoluzione laterale 1 , 5 mm ; scarso : se le sonde avevano una risoluzione laterale maggiore rispetto ai valori sopraindicati . 672 radiol med ( 2010 ) 115 : 668677 assessment of poor was given if the transducer had a lateral resolution greater than the above values . quality control of focusing was performed on a vertical target with acquisition of a series of images and variation of focal zone position in correspondence with the various reflectors . 
an assessment of good was given if the focused reflector had a width less than or equal to those not focused . analysis of a pseudocystic and solid mass , carried out on an anechoic and hyperechoic target with a diameter of 8 mm situated 4 cm deep took into account whether the mass was visible or not and whether the margins were regular or irregular . 
mean horizontal diameter and standard deviation of the pseudocyst and solid mass were also calculated for each frequency type . results with regard to image uniformity , 5 / 44 ( 11% ) 7.5 - mhz transducers and 2 / 11 ( 18% ) 13.5 - mhz transducers were rated poor . 
reverberation artefacts in the dead zone il controllo della focalizzazione avveniva sul target verticale e si acquisivano una serie di immagini variando la posizione del fuoco in corrispondenza dei vari riflettori ; venivano assegnati i seguenti giudizi : buono se il riflettore messo a fuoco aveva larghezza minore o uguale rispetto a quelli non a fuoco ; scarso se il riflettore messo a fuoco aveva larghezza maggiore rispetto a quelli non a fuoco . nellanalisi di pseudo - cisti e di una massa iperecogena , tenendo conto che gli inserti erano posti ad una profondit di 4 cm ed avevano diametro di 8 mm , si valutava se la massa fosse visibile o meno , se i margini fossero regolari o irregolari , ed infine veniva calcolato il rapporto altezzalarghezza , sul quale veniva espresso il giudizio : buono se era > 0 , 8 ; accettabile se era compreso tra 0 , 6 e 0 , 8 ; scarso se era < 0 , 6 . 
inoltre , stato calcolato il diametro orizzontale medio e la deviazione standard della psuedocisti e della massa iperecogena per ogni tipo di frequenza . risultati per quanto riguarda luniformit 5 / 44 ( 11% ) sonde da 7 , 5 mhz e 2 / 11 ( 18% ) da 13 , 5 mhz sono state giudicate scarse . 
laccuratezza dei calibri orizzontali stata valutata solo per le sonde da good sufficient poor frequency 3 , 5 mhz frequency 7 , 5 mhz frequency 13 , 5 mhz frequency 6 , 5 mhz fig . 
risultati dei controlli effettuati suddivisi in base alla frequenza centrale delle sonde esaminate . frequency 3 , 5 mhz frequency 7 , 5 mhz frequency 13 , 5 mhz frequency 6 , 5 mhz fig . 
risultati dei controlli effettuati suddivisi in base alla frequenza centrale delle sonde esaminate . frequency 3 , 5 mhz frequency 7 , 5 mhz frequency 13 , 5 mhz frequency 6 , 5 mhz transducers , 2 / 44 ( 4% ) 7.5 - mhz transducers , 2 / 11 ( 18% ) 13.5 - mhz transducers and 2 / 13 ( 15% ) 6.5 - mhz transducers were rated sufficient in evaluating the heightwidth ratio of the anechoic lesion ; 8 / 48 ( 16% ) 3.5 - mhz transducers , 3 / 44 ( 7% ) 7.5 - mhz transducers , 2 / 11 ( 18% ) 13.5mhz transducers and 4 / 13 ( 30% ) 6.5 - mhz transducers were classified as sufficient in evaluating the heightwidth ratio of the hyperechoic lesion . 
findings also revealed that 4 / 116 ( 3% ) transducers two 7.5 - mhz , one 13.5 - mhz and one 6.5 - mhz were unable to visualise the targets . 
in addition , 1 / 48 3.5 - mhz transducer , 7 / 44 ( 16% ) 7.5 - mhz transducers , 4 / 11 ( 36% ) 13.5 - mhz transducers and 1 / 13 6.5 - mhz transducers visualised solid lesion margins as irregular , whereas fluid - filled lesion margins were visualised as regular by all transducers . 
it was therefore possible to identify not only the vertical black bands ( indicative of broken piezoelectric crystals ) that are frequently encountered and readily appreciable , but also the less noticeable horizontal bands that may indicate a focusing defect [ 3 , 8 ]  . valutazione del rapporto altezza - larghezza della lesione iperecogena . 
il diametro orizzontale medio della lesione solida era pari a 8 , 09 cm ( 0 , 29 ) per le frequenze da 3 , 5 mhz , a 7 , 92 cm ( 0 , 18 ) per le frequenze da 7 , 5 mhz , a 7 , 86 cm ( 0 , 32 ) per le frequenze da 13 , 5 mhz e a 7 , 89 cm ( 0 , 19 ) per le frequenze da 6 , 5 mhz . discussione la valutazione delluniformit un test di indubbia rilevanza clinica , le non - uniformit dellimmagine infatti possono aumentare il rischio di falsi negativi [ 7 ] ; nel nostro studio i difetti di uniformit sono stati riscontrati nel 13% delle sonde lineari superficiali complessivamente presenti ed esclusivamente a carico di queste ultime . 
stato dunque possibile individuare non solo le bande nere verticali ( espressione di rottura di cristalli piezoelettrici ) , che risultano di pi frequente riscontro e pi facilmente apprezzabili , ma anche le meno intuibili bande nere orizzontali , che possono indicare difetti di focalizzazione [ 3 , 8 ]  . 
 nella valutazione della massima profondit di penetrazione come previsto i trasduttori a bassa frequenza hanno mostrato una maggiore profondit di penetrazione [ 10 , 11 ] ; diminuzioni nella potenza di emissione del fascio ultrasonoro o ogni incremento nel rumore elettronico , cause di subdola degradazione dellimmagine spesso difficile da radiol med ( 2010 ) 115 : 668677 in evaluating maximum penetration depth , lowfrequency transducers exhibited , as anticipated , a greater penetration depth [ 10 , 11 ]  . 
even though from a clinical perspective the few millimetres of exploration proximal to the transducer surface are not relevant , a greater extension of the dead zone is indicative of the possible presence of defects , such as a long duration ultrasound impulse , incorrect functioning of attenuation materials or rupture of a lens . 
more numerous , however , were transducers displaying reverberation artefacts within the dead zone ( 12% of transducers examined ) , which indicated the existence of fluctuations in the transmission power of the ultrasound beam [ 7 , 8 ]  . in evaluating vertical and horizontal distance accuracy , in contrast to our expectations , transducers with a central frequency of 3.5 mhz proved to be less accurate in the vertical direction than in the horizontal direction . 
errors in vertical distance measurement are especially due to inefficiencies of the internal circuit [ 7 ]  . as expected , axial and lateral resolution proved to be greater in high - frequency transducers [ 10 ]  . 
lateral resolution proved to be worse than axial resolution , especially in 3.5 - mhz transducers , thus indicating the possible presence of various defects , most of all with regard to ultrasound beam focusing [ 8 , 11 , 1316 ]  . 
 the anechoic target mimicking a fluid - filled structure was visualised with regular margins , whereas the hyperechoic target mimicking an angioma - like lesion was visualised with margins defined as irregular in 20% of the surface transducers tested . 
no significant geometrical distortions of targets were found , thus attesting that there were no significant defects in image display on the rilevare [ 3 , 12 ] sono state riscontrati principalmente a carico delle sonde lineari superficiali , in particolare per i trasduttori con frequenza centrale da 7 , 5 mhz : il 50% di questi , infatti , stato giudicato come accettabile o scarso . 
 solo il 6% delle sonde complessivamente presenti ha mostrato aumentate dimensioni della zona morta ; anche se dal punto di vista clinico i pochi millimetri di esplorazione prossimali alla superficie della sonda non sono rilevanti , una maggiore estensione della zona morta testimonia la possibile presenza di vari tipi di difetti come un impulso ultrasonoro di lunga durata , un non corretto funzionamento di materiali smorzanti o la rottura di una lente ; pi numerose , invece , sono state le sonde che a livello della zona morta hanno mostrato artefatti da riverbero ( il 12% delle sonde presenti ) , a testimonianza dellesistenza di fluttuazioni di potenza dellemissione del fascio ultrasonoro [ 7 , 8 ]  . nella valutazione dei calibri verticali ed orizzontali , a differenza di quanto ci saremmo aspettati , le sonde con frequenza centrale da 3 , 5 mhz si sono dimostrate meno accurate nella misurazione delle distanze in direzione verticale piuttosto che in direzione orizzontale : infatti il 35% delle sonde da 3 , 5 mhz stato giudicato accettabile nella valutazione dei calibri verticali . 
errori della distanza verticale sono soprattutto dovuti ad inefficienze del circuito interno [ 7 ]  . come atteso la risoluzione assiale e la risoluzione laterale si sono dimostrate superiori nelle sonde ad alta frequenza [ 10 ] , la risoluzione laterale si confermata peggiore rispetto a quella assiale , in particolare per i trasduttori da 3 , 5 mhz , a testimonianza della possibile esistenza di vari deficit , primo fra tutti deficit riguardanti la focalizzazione del fascio ultrasonoro [ 8 , 11 , 1316 ]  . 
 stata dimostrata la tendenza degli ultrasuoni ad una peggiore focalizzazione del fascio mano a mano che aumenta la profondit [ 11 ] , particolarmente evidente per le sonde da 3 , 5 mhz . 
per le sonde lineari superficiali , invece , sono stati riscontrati in generale migliori sistemi di focalizzazione . complessivamente quattro sonde non sono state in grado di visualizzare i due inserti : in due casi si deve addurre che la mancata visualizzazione fosse legata ad una scarsa profondit di penetrazione . 
le strutture liquide sono state tutte visualizzate con margini regolari ; le lesioni similangiomatose , invece , hanno mostrato margini definiti come irregolari nel 20% delle sonde superficiali complessivamente presenti : anche in questo caso una scarsa risoluzione di contrasto pu esserne allorigine . 
non sono state rilevate significative distorsioni geometriche degli inserti , a testimonianza del fatto che non ci sono significativi deficit nella rappresentazione dellimmagine sul monitor [ 7 , 8 ]  . confermiamo la tendenza delle apparecchiature ecografiche a rappresentare le strutture liquide pi piccole di 676 monitor [ 7 , 8 ]  . we confirm the tendency of the ultrasound systems to depict fluid - filled structures smaller than they really are when the measurement is made in a plane horizontal to that of the propagation of the ultrasound beam , with an underestimation of around 1.34 cm , equivalent to around 17% of the real dimensions . 
solid structures , in contrast , are substantially depicted with their real dimensions . many variables can produce a decrease in equipment efficiency , but their analysis goes beyond the scope of this study . 
 a quality control programme can be used to : evaluate the level of efficiency of the ultrasound system and , as proposed by the leading scientific associations , monitor changes in efficiency over time through annual controls check that parameters guaranteed by the manufacturer correspond with the effective parameters measured during the test run of a new scanner compare different systems , with the advantage of being able to foresee the trend in performance of the equipment over time identify degradation in image quality before it impacts patient diagnosis , thus preserving the diagnostic power of the technique our study has been useful in providing a snapshot of the functional state of transducers at our centre . 
in particular , it allowed us to identify one group of transducers indicated as sufficient in some parameters and another , in our opinion , where greater attention must be paid . 
it is in this latter group that corrective measures need to be taken to avoid deterioration of imaging conditions . radiol med ( 2010 ) 115 : 668677 quello che sono in realt quando la misurazione avviene secondo un piano orizzontale a quello di propagazione del fascio ultrasonoro , con sottostima di circa 1 , 34 mm , che equivale al 17% circa delle reali dimensioni ; le strutture solide , invece , vengono sostanzialmente rappresentate con le loro reali dimensioni . le variabili che possono portare ad una diminuzione della efficienza delle apparecchiature sono molteplici e la loro analisi va al di l dello scopo di questo studio ; in ogni caso , una delle variabile che sicuramente pu influenzare lo stato delle sonde quella legata allanno di collaudo dellecografo : a titolo esemplificativo sulle 32 sonde che complessivamente sono state giudicate come accettabili o scarse per quanto riguarda la massima profondit di penetrazione , 27 sono state collaudate prima del 2003 . 
regione emilia - romagna , bologna , italy 8dipartimento di radiologia ospedale san raffaele , milano , italy 9programma aziendale screening , ausl 2 umbria , perugia , italy 10centro di senologia , presidio ospedaliero maggiore ausl , bologna , italy correspondence to : s . 
 keywords breast cancer mammography diagnosis computer aided diagnosis riassunto esiste consistente evidenza scientifica che la computer aided diagnosis ( cad ) , aggiunta alla lettura singola , consenta un aumento della sensibilit di circa il 10% , con un aumento del tasso di richiamo di circa il 12% : luso corrente di cad nella pratica clinica pertanto raccomandabile . 
confronti tra studi non controllati suggeriscono consistentemente che cad sia comparabile alla doppia lettura quanto a tasso diagnostico incrementale di carcinoma ( cad + 10 , 6% , doppia lettura + 9 , 1% ) e possibilmente superiore quanto a tasso di richiamo ( cad + 12 , 5% , doppia lettura + 28 , 8% )  . 
al contrario , un numero limitato di studi controllati che confrontano la singola lettura + cad con la doppia lettura non mostra risultati consistenti e in media riporta per cad un minor tasso diagnostico incrementale di cancro ( 5 , 1% ) e un minor tasso di richiamo ( 9 , 8% )  . levidenza scientifica disponibile non sufficiente per raccomandare la lettura singola + cad come alternativa corrente alla doppia lettura convenzionale . parole chiave carcinoma della mammella mammografia diagnosi diagnosi computer assistita 564 radiol med ( 2010 ) 115 : 563570 computer - aided diagnosis ( cad ) has been in use as an aid to mammography reading for at least two decades . 
overall evidence consistently demonstrates that adding cad to single conventional reading allows for 10% relative incremental cancer detection rate ( table 1 ) at the cost of 12% incremental relative recall rate ( table 2 )  . 
double reading involves two radiologists with different individual diagnostic criteria and often with a different level of attention for specific morphological features ( masses , parenchymal distortions , microcalcifications )  . 
such differences in perception allow one reader to detect cancers missed by another reader and , at the same time , increase the recall rate of lesions with a specific morphological pattern . 
nella doppia lettura i due lettori hanno ovviamente criteri diagnostici diversi e , in genere , una diversa attenzione per lesioni di morfologia diversa ( opacit di massa , distorsioni , calcificazioni ) : proprio questa diversit di percezione consente da un lato ad un lettore di identificare alcune neoplasie che laltro ha sottovalutato , dallaltro di richiamare preferenzialmente determinate morfologie , diverse dai richiami dellaltro lettore . 
questo potenziamento del tasso di richiamo tra due lettori maggiore di quello legato a cad , perch in questo caso le varie entit morfologiche vengono rivalutate dallo stesso lettore , in sostanza con gli stessi criteri diagnostici . 
in altre parole un lettore che tende a dare poco importanza alle piccole opacit regolari , assumendole come benigne , continuer a considerarle tali anche se cad le evidenzia , mentre se gli associamo un altro lettore che invece d importanza a quel tipo di alterazioni , il caso ha una maggiore probabilit di essere richiamato . se levidenza da studi non controllati suggerisce che la lettura singola integrata da cad potrebbe essere una valida alternativa alla doppia lettura convenzionale , indubbio che le caratteristiche degli studi in questione ( selezione delle casistiche , contesti , protocolli , operatori diversi ) comportino una scarsa confrontabilit , perch non concordano per una serie di fattori confondenti . 
per questo motivo da tempo si auspica la conduzione di studi controllati che confrontino , a parit di casistica e di operatori , la lettura singola + cad e la doppia lettura convenzionale . 
gli studi finora disponibili in questo ambito sono riassunti nella tabella 5 . i risultati di questi studi sono a prima vista piuttosto difformi quanto a incremento del tasso diagnostico di carcinomi e di richiami . 
in other words , a reader discounting small regular opacities , assumed as benign , will insist in discounting them , even if marked by cad , whereas another reader with a special concern for missing cancers depicted as regular opacities is more likely to recall them , and possibly detect additional cancers . although the evidence from uncontrolled studies suggests single reading combined with cad as a valid alternative to conventional double reading , no doubt these studies are hardly comparable due to differences in design ( case selection , setting , diagnostic protocol , different operators ) , implying possible confounders . 
for this reason , controlled studies ( same series , same readers ) have been advocated for a long time to accurately compare single reading + cad and double reading . 
 mente discutibile , trattandosi di studi del tutto diversi come disegno , scenario , numerosit di casistica e operatori , ma , con questa limitazione , sembra indicare che le due modalit non differiscano di molto , in media con una minore sensibilit ( 5 , 1% ) per la lettura singola + cad , e differiscano maggiormente , ma questa volta a favore della lettura singola + cad , quanto a tasso di richiamo ( 9 , 8% )  . la discrepanza dei risultati tra il confronto degli studi non controllati di lettura singola + cad e doppia lettura e gli studi controllati pu spiegarsi con il fatto che tutti questi studi riguardano casistiche , lettori e disegni di studio diversi : tutte queste variabili possono influenzare in modo importante i risultati . 
anche gli studi controllati presentano le stesse variabili : una menzione speciale merita il recente studio computed - aided detection evaluation trial ( cadet ) [ 25 ] , che ha probabilmente il disegno di studio pi robusto e affidabile , che riporta una sostanziale equivalenza della doppia lettura e della lettura singola + cad , e in radiol med ( 2010 ) 115 : 563570 results are inhomogeneous at first glance , both for incremental detection and recall rate . 
a simple estimate of average results may be criticised for the intrinsic differences among studies ; however , with such a limitation , it suggests no major differences between the two modalities ( 5.1% in detection rate and 9.8% in recall rate for single reading + cad )  . 
 the discrepancy between the evidence provided by uncontrolled comparison of single reading + cad and double reading may be explained by the fact that the comparative studies dealt with different series , different readers and different study designs , and all these variables are likely to heavily influence incremental detection rates . controlled studies may also be affected by the same biases . the recently published computer - aided detection evaluation trial ( cadet ) deserves special mention [ 25 ] as the study with probably the most robust unbiased design , which reports a substantial equivalence of single reading + cad and conventional double reading as to cancer detection rate , thus confirming the results of uncontrolled comparisons . 
however , it is evident that further controlled studies are needed before a final word may be said on this topic . considering that several cad algorithms are presently marketed without proper validation of their efficacy or a careful analysis of their advantages and disadvantages , the latter being not immediately perceived in current use , the joint study group of the gruppo italiano di studio per lo screening mammografico ( gisma ) and societ italiana di radiologia medica ( sirm ) senology study section thought it worthwhile to publish these considerations and recommendations on the use of cad in current mammography practice . 
validation should be ideally based on the assessment of incremental cancer detection rate and recall rate to diagnostic assessment , obtained through double - blind reading of current mammography activity or of a ad hoc predefined case series [ 14 , 25 ]  . 
comparative studies of different cad algorithms tested on the same series [ 1 , 26 ] show that algorithms may differ to a substantial questo sembra confermare quanto suggerito dal confronto di studi non controllati . 
peraltro evidente che sono necessari altri studi controllati per dire una parola definitive sullargomento . in considerazione del fatto che diversi algoritmi cad vengono attualmente commercializzati senza una rigorosa verifica di efficacia e / o una attenta disamina dei pro e dei contro della metodica , tenuto conto che la corretta comprensione di questi ultimi non sempre immediata , il gruppo di studio congiunto gruppo italiano di studio per lo screening mammografico ( gisma ) e sezione di senologia della societ italiana di radiologia medica ( sirm ) ha ritenuto opportuno riportare queste considerazioni , precisazioni e raccomandazioni rispetto al possibile uso di cad nella pratica clinica , ad oggi . 
tali raccomandazioni e osservazioni sono rivolte sia ai radiologi che vogliano prendere in considerazione luso di cad , sia agli amministratori sanitari interessati ai possibili vantaggi della metodica . complessivamente levidenza disponibile sulluso di cad in mammografia consente di fare alcune considerazioni , precisazioni e raccomandazioni : 1 . 
la verifica in genere si basa sulla determinazione del tasso incrementale diagnostico di carcinoma e di richiamo ad approfondimento , verificata con metodica cieca su casistica corrente o su set di validazione approntati ad hoc [ 14 , 25 ]  . 
il radiologo quindi tenuto necessariamente , per evitare un intollerabile eccesso di approfondimenti diagnostici , a trascurare , come non rilevanti la maggioranza delle roi , concentrandosi su una minoranza di esse . 
caveat for cad use modality : cad systems with known performance rates usually have a low specificity . an excess of regions of interest ( roi ) is identified and proposed for review ( at least one roi per view )  . 
studies of cad performance [ 14 , 27 , 28 ] demonstrated that even well - trained radiologists with considerable experience may react in different ways to cad use , the magnitude of cad influence on diagnosis being quite variable . 
for this reason , it is of paramount importance that radiologists do not automatically assume the same average advantages of cad use reported in the literature : each reader should test his or her own cad - related incremental detection and recall rate . 
in the event that cad shows poor local performance ( too few extra cancers detected with an excess of extra recalls ) , it should not be used in current practice , being of no benefit for the patients 5 caveat for cad use by unexperienced radiologists : as discounting most cad - generated rois is unavoidable , this may be difficult for radiologists of limited experience in mammography reading , who tend to adopt a low baseline threshold for suspicion and a high recall rate , as they feel less confident with the methodology . 
medicolegal caveat relative to roi discounting : let us suppose that one radiologist is sued for diagnostic delay nonostante la mammografia clinica non sia normata come lo screening , devono evitare leccesso di falsi positivi e di accertamenti ( anche invasivi ) inutili . 
gli studi che hanno verificato leffetto di cad sulla diagnosi [ 14 , 27 , 28 ] riportano correntemente come anche radiologi esperti reagiscano diversamente a cad , facendosi influenzare da esso in diversa misura . 
per questo motivo opportuno che il radiologo che usa cad non assuma che ne avr il vantaggio medio riportato in letteratura , ma verifichi , dopo una determinato periodo duso , il reale impatto di cad sul tasso diagnostico di carcinoma e di approfondimenti diagnostici nella propria esperienza individuale . tali considerazioni non sono valide solo sul piano individuale ma anche di struttura . 
definito come inevitabile questo processo di selezione delle roi generate da cad , evidente che un radiologo di limitata esperienza in mammografia ( e per questo gi tendente ad eccedere negli approfondimenti per la minore confidenza con il metodo ) potrebbe risentire negativamente delluso di cad , che lo porterebbe facilmente ad un tasso di falsi positivi , e relativi approfondimenti inutili , eccessivo . 
se una lesione di cui si sostiene la mancata identificazione per imperizia era stata identificata come roi , questo pu essere una aggravante dellerrore del radiologo in un contenzioso medico - legale ? come indicato al punto 3 , il radiologo che usa cad ha lobbligo della censura della grande maggioranza delle roi per garantire una buona pratica diagnostica . 
quindi il fatto che abbia trascurato una roi non pu essere preso come aggravante di un supposto errore diagnostico , ma leventuale omissione verr valutata in base alla revisione del radiogramma incriminato , possibilmente con modalit cieca [ 29 ] , radiol med ( 2010 ) 115 : 563570 due to misperception of a mammographic abnormality , which had been selected as an roi by cad . 
should roi discounting be assumed as an indicator of diagnostic error ? as discussed caveat 3 , cad use involves the obligation for the radiologist to discount most rois to avoid unacceptable recall rates . 
thus , roi discounting cannot be assumed per se as a proof of diagnostic error : diagnostic error will be evaluated only on review of the mammogram , possibly using a blind review methodology [ 29 ] , and without cad use . 
caveat for the health service managers : when combined with single reading currently used for clinical mammography , cad is expected to increase cancer detection rate with a similar relative increase in recall rates . 
in other words , clinical diagnosis , with the use of cad , is more complex and costly and requires a greater workload , although this is counterbalanced by earlier diagnosis of a limited number of cancers . 
it is more reasonable to say that in the absence of sound scientific evidence that single reading + cad is as effective as conventional double reading , cad use is not recommended as an alternative to double reading . 
in ogni caso , lalgoritmo cad nella indicazione delle roi non necessariamente riproducibile nelle nuove versioni dello stesso prodotto commerciale . gli algoritmi cad , infatti , sono spesso soggetti a modifiche migliorative della performance ( in genere della specificit ) e possono , pertanto , differire da un anno allaltro . 
se combinato alla lettura singola , di comune uso in pratica clinica , cad dovrebbe aumentare il tasso diagnostico di carcinoma al costo di un aumento comparabile di approfondimenti diagnostici . 
sul piano dei costi di esercizio , pertanto , luso di cad comporta un aumento dei costi , legato ai costi intrinseci di cad ( licenza ) e al costo degli approfondimenti diagnostici aggiuntivi generati da cad . 
in altre parole , la diagnostica senologica clinica , con luso di cad , diviene pi complessa e costosa e richiede pi tempo / lavoro , anche se questo compensato da un aumento della precocit diagnostica in un limitato numero di carcinomi . 
una simile scelta porterebbe indubbiamente al risparmio di un radiologo lettore , apparentemente con una riduzione dei richiami , ma al prezzo di una riduzione della sensibilit con perdita di un 5% di carcinomi . 
 pi ragionevole affermare che , al momento , in mancanza di evidenza scientifica di una reale equivalenza tra lettura singola + cad e doppia lettura , luso di cad in alternativa alla doppia lettura non raccomandato . 
ove lo si usasse a tal fine , eventuali errori diagnostici sarebbero aggravati dal fatto di non aver adottato quei presidi ( appunto la doppia lettura ) raccomandati per garantire lefficacia dello screening . 
gandini istituto di radiologia diagnostica ed interventistica , universit di torino , aso san giovanni battista di torino , sede molinette , via genova 3 , 10126 torino , italy correspondence to : e . 
a total of 120 nodular lesions diagnosed on mammography and / or ultrasonography in 110 women ( mean age 51.27 years ) were evaluated with sonoelastography and classified according to elasticity score ( s1s5 )  . 
all nodules with an elasticity score of 5 were malignant , and those with a score 3 were benign , with the exception of four cases of invasive carcinoma with atypical elasticity ( two lobular and two ductal with liquefaction necrosis )  . 
the use of sonoelastography to complement mammography and ultrasonography could help in the differential diagnosis of nodular breast lesions , especially in breast imaging reporting data system ( bi - rads ) 3 lesions with marked elasticity ( s3 )  . 
tutti i noduli s5 sono risultati maligni mentre quelli con s3 sono tutti risultati benigni , eccetto quattro casi di carcinomi infiltranti con elasticit atipica ( 2 lobulari e 2 duttali con necrosi colliquativa )  . 
le 22 lesioni s4 sono risultate : 17 maligne , 2 dubbie ( iperplasia a cellule colonnari e lesione sclerosante complessa ) , 3 benigne ( fibroadenomi sclerotici )  . 
lelastosonografia utilizzata come metodica complementare alla mammografia ed allecografia consente unaccurata diagnosi differenziale dei noduli mammari , specialmente nelle lesioni breast imaging reporting data system ( bi - rads ) 3 dotate di elevata elasticit ( s3 )  . 
lalta concordanza tra le caratteristiche elastiche ed il riscontro anatomopatologico di benignit 552 radiol med ( 2010 ) 115 : 551562 number of needle biopsies and guide women at low radiological risk towards follow - up . potrebbe evitare il prelievo agobioptico indirizzando verso il follow - up nei casi con basso rischio radiologico . 
 keywords breast ultrasonography sonoelastography parole chiave mammella ecografia elastosonografia introduction introduzione first introduced in 1991 , sonoelastography is an ultrasound technique that evaluates the elastic properties of tissue by analysing the radiofrequency pulses generated by a structure in response to external compression [ 1 , 2 ]  . 
through a complex algorithm called combined autocorrelation method ( cam ) , the software provides an elastogram , which is essentially a colour - coded map of the degree of elasticity of tissue being examined [ 58 ]  . the most widely used elastographic technique is realtime freehand sonoelastography . 
with this technique , the image is obtained through gradual manual compression of the tissue with a linear - array transducer that allows real - time display of the elastogram as a colour image superimposed on the b - mode image [ 2 ]  . 
by exploiting these tissue changes , sonoelastography has secured a place in breast imaging . the purpose of this study was to evaluate the role and accuracy of sonoelastography in the characterising breast nodules and differentiating between malignant and benign lesions . 
to this end , we considered the following factors : correlation between mammographic , sonographic and sonoelastographic features ; sensitivity and specificity of sonoelastography , with cytological / microhistological or final histological diagnosis taken as the gold standard ; ability of sonoelastography to provide additional information on tissue elasticity in the event of equivocal mammographic and / or sonographic findings in order to guide the diagnostic workup towards biopsy or follow - up . materials and methods between july 2006 and july 2007 , sonoelastography was performed on a selection of 120 nodular breast lesions , of which 110 were detected with mammography and ultralelastosonografia una tecnica ultrasonografica che , introdotta per la prima volta nel 1991 , valuta le propriet elastiche dei tessuti analizzando gli impulsi di radiofrequenza provenienti da una struttura , in risposta ad una compressione esterna [ 1 , 2 ]  . 
tramite un complesso algoritmo definito combined autocorrelation method ( cam ) si ottiene un elastogramma , il quale non altro che unimmagine a colori ove ogni sfumatura correlata con il grado di elasticit del tessuto [ 58 ]  . la metodica elastografica attualmente pi utilizzata la freehand ultrasound elastography in real time . 
limmagine si ottiene mediante una compressione manuale graduale sul tessuto da analizzare , impiegando un trasduttore ecografico lineare che consente unimmediata visualizzazione dellelastogramma come unimmagine a colori sovrapposta a quella in b - mode [ 2 ]  . 
sfruttando tali modificazioni tissutali , lelastosonografia entrata a far parte delle tecniche di imaging nella diagnostica senologica . lo scopo di questo studio stato di valutare il ruolo e laccuratezza dellelastosonografia nella caratterizzazione dei noduli mammari e nella differenziazione delle lesioni maligne da quelle benigne . 
in questa ottica sono state prese in considerazione : la correlazione tra le caratteristiche mammografiche ed ecografiche con quelle elastosonografiche ; la sensibilit e la specificit dellelastosonografia assumendo come gold - standard la diagnosi cito - microistologica o istologica definitiva ; la capacit dellelastosonografia di apportare in caso di dubbio diagnostico mammografico e / o ecografico informazioni aggiuntive sullelasticit tissutale , al fine di orientare liter diagnostico verso lapprofondimento bioptico o verso il follow - up . radiol med ( 2010 ) 115 : 551562 sonography ( in 101 women aged > 35 years ) and ten were identified with ultrasonography alone ( in nine women aged < 35 years )  . 
patients had a mean age of 51.27 ( range 2285 ) years and were referred by the screening centre and the breast clinic . mammography was performed with senographe dmr v2 ( ge medical systems , milwaukee , wi , usa ) analogical units in the two standard views : craniocaudal ( 0 ) and mediolateral oblique ( 45 )  . 
to clarify diagnostic doubts in specific cases , we obtained additional lateral projections ( 90 ) , radiograms targeted at the area of interest and / or radiograms with direct magnification and , where necessary , rotated craniocaudal projections to inspect the axillary cavity or the intermammary clemammographic findings were coded using the breast imaging reporting data system ( bi - rads ) classification of the american college of radiology ( acr ) [ 13 ]  . 
uniform manual compression was applied , with the transducer being moved perpendicularly to the region under examination and taking care to avoid any lateral displacement that might alter the reception of radiofrequency pulses . correct performance of the sonoelastographic study was monitored by referring to the numerical indicator of data quality displayed on the monitor : image quality was only considered acceptable for values > 2 ( range 16 )  . sonoelastography was used to study both the nodular formation and the surrounding breast tissue in all cases to compare elasticity of different breast regions and average tissue deformation . 
in particular , in each lesion , we evaluated maximum diameter and depth from the skin surface . lesions were rated according to an elasticity score ( es ) from 1 to 5 based on the sonoelastographic classification of the italian multicentre study group ( table 1 ) [ 14 , 15 ]  . 
le pazienti incluse in questo studio avevano unet media di 51 , 27 anni ( range 2285 anni ) e provenivano dal centro di screening e dalla diagnostica clinica senologica . gli esami mammografici sono stati eseguiti con mammografi analogici senographe dmr v2 ( ge medical systems , milwaukee , wi , usa ) , nelle due proiezioni standard cranio - caudale ( 0 ) e medio - laterale obliqua ( 45 )  . in casi specifici per risolvere il dubbio diagnostico sono state effettuate proiezioni aggiuntive laterali ( 90 ) , radiogrammi mirati sullarea interessata e / o radiogrammi con ingrandimento diretto ed eventualmente proiezioni craniocaudali ruotate , proiezioni per evidenziare il cavo ascellare o il solco intermammario . 
i reperti mammografici sono stati codificati utilizzando la classificazione breast imaging reporting data system ( bi - rads ) , proposta dallamerican college of radiology ( acr ) [ 13 ]  . 
in corso di elastosonografia la paziente ha mantenuto la medesima posizione adottata per lindagine ecografica b - mode prolungando lesame convenzionale non pi di 23 minuti . per ottenere immagini adeguate stata applicata una compressione manuale uniforme eseguendo con la sonda dei movimenti perpendicolari alla regione in esame ed evitando tutte quelle dislocazioni laterali che avrebbero potuto alterare la ricezione delle radiofrequenze . 
la corretta esecuzione della valutazione elastosonografica stata monitorata tramite lapposito indicatore numerico luminoso presente sul monitor : la qualit dellimmagine ottenuta durante lindagine stata considerata accettabile solo per valori superiori a 2 ( range da 1 a 6 )  . con lelastosonografia sono sempre stati studiati sia la formazione nodulare sospetta sia il tessuto mammario circostante , in modo da confrontare lelasticit delle diverse regioni della mammella in esame e la deformazione media del tessuto . 
le lesioni sono state codificate mediante score elastico ( s ) con un punteggio da 1 a 5 , secondo la classificazione elastosonografica del gruppo di studio multicentrico italiano ( tabella 1 ) [ 14 , 15 ]  . 
 all biopsies were performed under sonographic guidance using 21to 23 - gauge needles for cytological samples [ fineneedle aspiration cytology ( fnac ) ] and 14to 18 - gauge needles for microhistological samples [ core biopsy ( cb ) ]  . fnac / cb results were classified according to the forza sul carcinoma mammario operativa nazionale ( foncam ) european guidelines [ 16 ]  . 
all lesions with an fnac / cb result classified as nondiagnostic ( 1 c1 ) , equivocal ( a lesion with isolated ductal epithelial laminae and focal atypia classified as c3 and a papillary lesion with high cellularity and atypia classified as c4 ) or malignant ( c / b5 ) were referred for surgical evaluation . 
lo score 5 indica una totale assenza di elasticit sia nella lesione , sia nelle strutture disposte nei piani ad essa circostanti ; lelastogramma si presenta quindi completamente blu con un alone azzurro periferico . 
 tutti i prelievi sono stati eseguiti sotto guida ecografia mediante aghi da 2123 g per lesame citologico ( fine needle aspiration cytology , fnac ) e con aghi da 1418 g per lesame microistologico ( core biopsy , cb )  . 
tutte le lesioni aventi esito cito - microistologico non diagnostico ( 1 c1 ) o dubbio ( una lesione con sporadiche lamine di epitelio duttale con focali atipie classificata c3 e una lesione papillare ad elevata cellularit con atipie classificata c4 ) oppure maligno ( c / b5 ) sono state inviate alla verifica chirurgica . 
all nodules rated s5 at sonoelastography ( n = 14 ) were malignant , with 12 c / b5 ( confirmed at surgery to be nine invasive ductal carcinomas , two invasive lobular carcinomas , one sarcoma ) and two lymphomas . 
of the 22 lesions with sonoelastography score of s4 , 17 were malignant ( c5 ) , two had equivocal fnac results and three were benign ( c2 )  . 
si assunto come veri positivi ( vp ) quelle lesioni aventi score 4 o 5 ed una verifica citologica e / o istologica di malignit e come veri negativi ( vn ) le lesioni con score 1 , 2 o 3 e risultate benigne al prelievo cito - microistologico . 
sono stati considerate come falsi positivi ( fp ) le lesioni con score 4 o 5 e verificate come formazioni benigne e come falsi negativi ( fn ) quelle con score 1 , 2 o 3 con diagnosi di malignit definitiva . risultati il diametro medio delle 120 lesioni studiate stato di 1 , 550 , 16 cm ( intervallo di confidenza [ ic ] 95% , con dimensione minima di 0 , 5 cm e massima di 5 cm ) , la profondit media stata di 1 , 700 , 11 cm ( ic 95% con profondit minima di 0 , 7 cm e massima di 3 , 87 cm )  . 
quattro pazienti con lesioni classificate r3 e con score u e s 2 hanno rifiutato di sottoporsi ad accertamento anatomopatologico optando per un monitoraggio strumentale ( tabella 2 )  . 
a sinistra : lelastosonografia evidenzia uno score 2 ( prevalenza di verde con alcuni punti blu nella compagine )  . prelievo citologico : frammenti di tessuto mixoide e sporadiche cellule epitaliali tipiche e mioepiteliali . 
quadro compatibile con fibroadenoma ( c2 )  . evaluation of the 17 malignant lesions revealed a predominance of invasive histological types ( 15 cases : 10 invasive ductal carcinomas , 3 invasive lobular carcinomas and 2 infiltrating mucinous carcinomas ) relative to in situ carcinomas ( 2 cases of ductal carcinoma in situ ) ; on the other hand , the two lesions with a score of s4 and nondiagnostic or equivocal cytology were one columnar cell hyperplasia ( cch ) and one complex sclerosing lesion . 
tutti i noduli s5 ( 14 lesioni ) sono risultati maligni : 12 c / b5 ( confermati alla verifica chirurgica essere rispettivamente : 9 cdi , 2 cli , 1 sarcoma ) e 2 linfomi . 
delle 22 lesioni con punteggio elastosonografico s4 : 17 sono risultate lesioni maligne ( c5 ) , 2 hanno avuto esito citologico dubbio e 3 sono risultate benigne ( c2 )  . 
la valutazione istologica delle 17 lesioni maligne ha evidenziato la prevalente natura infiltrante degli istotipi ( 15 casi : 10 cdi , 3 cli e 2 carcinomi mucinosi infitranti ) rispetto agli in situ ( 2 casi di carcinoma duttale in situn [ cdis ] ) , mentre le 2 lesioni s4 con esito citologico non diagnostico o dubbio sono risultate essere rispettivamente uniperplasia a cellule colonnari ( icc ) ed una lesione sclerosante complessa . 
overall , sonoelastography had a sensitivity and specificity of 88.5% ( 95% ci : 82.594.5 ) and of 92.7% ( 95% ci : 87.797.7 ) , respectively , with a diagnostic accuracy of 91.3% ( 95% ci : 85.996.7 ) ( table 4 )  . we retrospectively analysed whether the diagnostic accuracy of sonoelastography changed depending on lesion size and depth . 
sensitivity and specificity in relation to nodule diameter were calculated by dividing the 104 lesions studied with sonoelastography and cytology / microhistology into two groups : lesions up to 2 cm in diameter ( n = 76 ) and lesions > 2 cm ( n = 28 ) ( table 5 )  . 
in the first group ( 2 cm ) , sonoelastography provided 20 tp , 52 tn , two fp and two fn results , with sensitivity of 96.2% ( 95% ci : 91.9100 ) radiol med ( 2010 ) 115 : 551562 sclerotica . 
nella nostra casistica lo score medio attribuito alle lesioni benigne stato di 2 , 730 , 17 ( ic 95% : 2 , 532 , 87 ) , mentre quello delle formazioni risultate essere maligne stato di 4 , 190 , 26 ( ic 95% : 3 , 974 , 46 )  . complessivamente lelastosonografia ha avuto una sensibilit ed una specificit rispettivamente del 88 , 5% ( ic 95% : 82 , 594 , 5 ) e del 92 , 7% ( ic 95% : 87 , 797 , 7 ) , con unaccuratezza diagnostica del 91 , 3% ( ic 95% : 85 , 996 , 7 ) ( tabella 4 )  . nel corso dello studio stata fatta unanalisi retrospettiva sulleventuale modificazione della capacit diagnostica dellelastosonografia in base alle dimensioni e alla profondit delle lesioni . 
la sensibilit e la specificit della metodica in relazione al diametro dei noduli sono state calcolate suddividendo le 104 formazioni sottoposte ad elastosonografia ed accertamento cito - microistologico in due gruppi aventi uno dimensioni pari o inferiori ai due centimetri ( 76 casi ) e laltro con diametro superiore ( 28 casi ) ( tabella 5 )  . 
allo stesso modo stata eseguita una valutazione suddividendo i 104 casi in due sezioni sulla base della profondit della lesione rispetto alla cute ( tabella 6 ) : da un lato quelli posti ad una distanza inferiore ai 2 cm ( 75 casi ) e dellaltro quelli a distanza superiore ( 29 casi )  . 
in particular , sonoelastography appears especially useful in lesions classified as bi - rads 3 at mammography and ultrasonography , in which it can confirm the diagnosis of benignity [ 17 , 18 ]  . in our study , the higher average score ( 2.730.17 ) obtained in histologically benign nodules compared with other case series [ 8 , 11 ] is due to the fact needle biopsy was not performed on lesions classified as r1 or r2 with an ultrasonographic risk of u2 , those classified as r3 and / or u3 lesions and with a sonoelastography score of s1 , or on patients who opted for follow - up rather than cytological / microhistological evaluation . 
the concordance between sonoelastography scores and pathological findings was discussione confrontando i dati in nostro possesso con quelli della letteratura possiamo notare come in tutte le casistiche vi siano unelevata concordanza tra reperti elastosonografici , mammografici ed ecografici , ed una buona correlazione tra punteggio elastosonografico e risultati anatomo - patologici . in particolare , emerge limportanza di utilizzare lelastosonografia soprattutto per le lesioni classificate mammograficamente ed ecograficamente con bi - rads 3 con lo scopo di rafforzare la diagnosi di benignit [ 17 , 18 ]  . nel nostro studio lelevato score medio ( 2 , 730 , 17 ) registrato nei noduli istologicamente benigni rispetto ad altre casistiche [ 8 , 11 ] dovuto allesclusione dallindagine agobioptica delle lesioni classificate r1 o r2 con rischio ecografico u2 , di quelle r3 e / o u3 aventi punteggio elastosonografico s1 e delle pazienti che hanno preferito il follow - up al controllo cito - microistologico . 
la concordanza tra score elastosonografico e riscontro anatomopatologico stata generalmente elevata : le lesioni con maggiore rigidit ( s5 ) erano tutte di natura maligna , mentre quelle pi elastiche ( s2 - s3 ) corrispondevano per lo pi a formazioni benigne . tuttavia in alcuni casi si sono osservate discordanze tra propriet elastiche e natura del nodulo : in quattro casi di carcinomi infiltranti ( due di tipo duttale e due di tipo lobulare ) lelasticit risultata maggiore di quella attesa , con pattern simile a lesioni di natura benigna . 
 [ 2 ] hanno ipotizzato un importante ruolo dellistotipo : le forme duttali potrebbero avere diversi comportamenti elastici in relazione alla componente fibroialina prodotta dalla neoplasia e allo stadio evolutivo ( neoplasie duttali di piccole dimensioni tenderebbero ad avere una minore componente fibrosa ) mentre nelle forme lobulari lelasticit sarebbe verosimilmente influenzata caratteristiche anatomo - patologiche dalle peculiari 560 radiol med ( 2010 ) 115 : 551562 generally high : the stiffer lesions ( s5 ) were all malignant , whereas most of the more elastic lesions ( s2 - s3 ) were benign . there were , nonetheless , a few cases of discordance between the elasticity and the nature of the nodule : in four cases of infiltrating carcinoma ( two ductal and two lobular ) , elasticity was higher than expected , with a pattern similar to that of benign lesions . 
 [ 2 ] suggested that histological type plays an important role in elasticity : ductal forms might have different elasticity patterns due to the fibrohyaline component and stage of the neoplasm ( small ductal neoplasms tend to have a smaller fibrous component ) , whereas the elasticity of lobular forms is affected by their peculiar pathological characteristics , i.e. 
the four discordant malignant cases in our series all < 2 cm revealed moderate liquefaction necrosis that , given the small size of lesions , would in itself be sufficient to affect elasticity [ 2 ]  . 
conversely , although the elastography scores of several fibroadenomas characterised by a large fibrotic component and poor cellularity were suspicious ( s4 ) , they were in all cases lower than those of invasive malignant forms , and none reached a score of s5 . 
the deep location of nodules makes it difficult to correctly compress the lesion with perpendicular movements of the transducer , and the elastogram is marred by the presence of artefacts due to lateral displacements of the transducer . 
 overall sensitivity and specificity of sonoelastography in our series were high , in line with the literature ( table 7 ) [ 2 , 8 , 2025 ] , which confirms the high reliability of this method . 
if confirmed by larger case series , these results suggest that the true potential of sonoelastography is to confirm the radiological hypothesis of rappresentate da scarsa coesione tra le cellule , minima componente di fibrosi ialina e modesta reazione desmoplastica , in particolare per lesioni di piccole dimensioni . 
nei nostri quattro casi maligni discordanti , tutti con dimensioni uguali o superiori a due centimetri , abbiamo riscontrato una discreta componente necrotica a carattere colliquativo che , in relazione alle dimensioni , costituirebbe di per se un fattore alterante le propriet elastiche [ 2 ]  . 
viceversa alcuni fibroadenomi , caratterizzati da elevata componente fibrotica e scarsa cellularit sono stati associati a pattern elastografici sospetti ( s4 ) , ma pur sempre inferiori alle forme maligne infiltranti , non raggiungendo in nessun caso lo score massimo ( s5 )  . 
in considerazione di questi risultati e di quelli gi riportati in letteratura le caratteristiche elastografiche delle lesioni nodulari mammarie devono sempre essere attentamente valutate e criticamente correlate alle caratteristiche mammografiche ed ecografiche [ 19 ]  . altri fattori che possono aver influenzato il risultato dello score elastico sono stati le dimensioni e la profondit delle lesioni in esame : similmente ad altri studi abbiamo riscontrato una maggiore sensibilit e specificit nelle lesioni con diametro inferiore ai due centimetri ( rispettivamente 96 , 2% e 90 , 9% ) rispetto a quelle con estensione superiore ( rispettivamente 84 , 6% e 80% )  . 
questa discrepanza verosimilmente dovuta alla non infrequente maggiore disomogeneit strutturale dei noduli pi voluminosi ( comprendenti aree colliquate miste a zone fibroticocalcifiche ) , che determinano alterazioni atipiche del coefficiente elastico . 
 paragonando le lesioni superficiali con quelle poste ad una profondit maggiore di due centimetri , ma comunque a una profondit non inferiore a 5 mm dalla cute , i valori di sensibilit e specificit calcolati sono stati del 95 , 2% versus 75% e del 96% versus 76 , 9% . 
la localizzazione profonda della formazione nodulare ha reso difficoltosa la corretta compressione della lesione mediante movimenti perpendicolari della sonda : lelestogramma risulta quindi alterato dalla presenza di artefatti dovuti alle dislocazioni laterali del trasduttore . 
 complessivamente la sensibilit e la specificit dellelastosonografia riscontrate nella nostra casistica sono risultate elevate , in linea con i dati gi riportati in letteratura ( tabella 7 ) [ 2 , 8 , 2025 ] che evidenziano lalta affidabilit della metodica . 
infatti tutte le lesioni a basso rischio mammografico ed ecografico ( bi - rads non superiore a 3 ) con score inferiore o uguale a 3 sono risultate benigne . questi risultati suggeriscono , se saranno confermati da casistiche pi numerose , come la vera potenzialit dellelastosonografia sia di rafforzare lipotesi radiologica di benignit , con un conseguente minor ricorso al prelievo agobioptico . 
in our series , we could have avoided fnac / cb in 78 cases , that is , half of the needle biopsies could have been avoided . sonoelastography is not , however , free of limitations . these include the need for a high level of manual dexterity , subjective interpretation of elastograms and sensitivity to slight changes in patient position . 
 conclusions in our case series , sonoelastography helped to correctly assess nodules < 2 cm in size and depth and to support the tentative diagnosis suggested by mammography and ultrasonography in both benign and malignant disease . 
in particular , in low - risk lesions at mammography and ultrasonography ( bi - rads 3 ) , sonoelastography allowed accurate characterisation and showed a high concordance with pathology . 
if our findings are confirmed by larger case series , sonoelastography may be adopted as a complement to mammography and ultrasonography . tuttavia occorre ricordare i principali limiti dellelastosonografia rappresentati dalla necessit di una ottima manualit delloperatore , dalla valutazione soggettiva dellimmagine e dalla dipendenza dai leggeri cambiamenti di posizione della paziente . 
 conclusioni nella nostra casistica lelastosonografia ha contribuito ad una corretta valutazione dei noduli di dimensioni e profondit inferiore ai 2 cm ed a rafforzare lorientamento diagnostico mammografico ed ecografico , sia nella patologia benigna che in quella maligna . 
in particolare nelle lesioni classificate mammograficamente ed ecograficamente a basso rischio ( bi - rads inferiore o uguale a 3 ) , lelastosonografia ha consentito una precisa caratterizzazione dei noduli mostrando un elevato accordo con il dato anatomo - patologico . 
zompatori4 1dipartimento di scienze cliniche , sezione di diagnostica per immagini , universit degli studi di parma , parma , italy 2dottorato di scienze pneumo - cardio - toraciche di interesse medico e chirurgico , universit di bologna , bologna , italy 3u.o. 
sverzellati , padiglione barbieri , sezione di diagnostica per immagini , azienda ospedaliero - universitaria di parma , 43100 parma , italy , tel . : + 39 - 052 - 1703647 , fax : + 39 - 052 - 1986352 , e mail : nicolasve@tiscali.it received : 11 march 2009 / accepted : 4 may 2009 / published online : 15 january 2010 springer - verlag 2010 abstract idiopathic pulmonary fibrosis ( ipf ) is the most common interstitial lung disease and is associated with a fatal prognosis . 
familiarity with the typical appearances of ipf on high - resolution computed tomography ( hrct ) is important , as in the appropriate clinical setting , it is often sufficient for establishing a confident diagnosis of ipf without the need for surgical biopsy . 
the purpose of this paper is to review the progress made towards a better understanding of the hrct patterns of ipf . keywords idiopathic pulmonary fibrosis usual interstitial pneumonia high - resolution computed tomography complications riassunto la fibrosi polmonare idiopatica ( idiopathic pulmonary fibrosis , ipf ) la pi comune interstiziopatia ed associata ad una prognosi infausta . 
importante avere famigliarit con le tipiche alterazioni della ipf alla tomografia computerizzata ad alta risoluzione ( highresolution computer tomography , hrct ) , poich queste , in combinazione con un profilo clinico compatibile , sono spesso sufficienti per ottenere la diagnosi di ipf senza il bisogno di ricorrere alla biopsia chirurgica . 
lobiettivo di questo articolo quello di riassumere i recenti progressi fatti verso una migliore comprensione degli aspetti sopra - riportati della ipf . parole chiave fibrosi polmonare idiopatica polmonite interstiziale usuale tomografia computerizzata ad alta risoluzione complicanze introduction introduzione pulmonary fibrosis is a nonspecific pathological condition that may result from granulomatous disorders , certain la fibrosi polmonare uno stato patologico non specifico che pu essere conseguenza di malattie granulomatose , di radiol med ( 2010 ) 115 : 526538 pharmacological treatments , repeated exposure to organic or inorganic antigens and collagen vascular diseases . 
idiopathic pulmonary fibrosis ( ipf ) is a very severe progressive disease , with survival after diagnosis between 2 and 4 years [ 1 ] , that is , worse than that of many cancers and , more importantly , significantly worse than that of other types of fibrosis [ 2 ]  . 
ipf is the most common diffuse infiltrative lung disease and , when associated with compatible clinical findings , can be diagnosed with high - resolution computed tomography ( hrct ) without the need for biopsy [ 3 ]  . 
distinguishing between ipf and the other entities included in the classification of idiopathic interstitial pneumonias is therefore crucial for correct stratification of patients for prognostic purposes [ 3 ]  . 
ipf is associated with the histopathological finding of usual interstitial pneumonia ( uip ) , a chronic fibrosing lung disease characterised by a heterogeneous picture of fibrosis , inflammatory infiltrate and honeycombing [ 7 ]  . 
however , the histological pattern of uip is not only observed in ipf but can also be associated with other disorders , such as chronic hypersensitivity pneumonitis , asbestosis and connective tissue diseases [ 3 ]  . 
compared with patients with other types of fibrosis , those with ipf are more prone to acute exacerbations of the disease , the pathological substrate of which is diffuse alveolar damage ( dad ) , certe terapie farmacologiche , di esposizioni ripetute verso antigeni organici o inorganici e di malattie collagenovascolari . 
la fibrosi polmonare idiopatica ( idiopathic pulmonary fibrosis , ipf ) una malattia progressiva molto grave , con sopravvivenza dopo la diagnosi compresa tra i 2 e i 4 anni [ 1 ] , cio peggiore di quella di molte neoplasie e , soprattutto , significativamente peggiore di quella degli altri tipi di fibrosi [ 2 ]  . 
la ipf la malattia infiltrativa diffusa polmonare pi comune e pu essere diagnosticata con la tomografia computerizzata ad alta risoluzione ( high - resolution computed tomography , hrct ) , quando associata ad un profilo clinico compatibile , senza la necessit di ottenere una conferma bioptica [ 3 ]  . 
lo scopo di questa review principalmente quello di riassumere i valori ed i limiti dellhrct nella diagnosi e nella valutazione evolutiva della ipf . definizione , eziologia , prevalenza ed aspetti clinici della ipf la prevalenza e lincidenza della ipf sono stimate rispettivamente intorno ai 1442 , 7 / 100000 e 6 , 36 , 8 / 100000 persone , sebbene la precisione di questi dati risulti attualmente ancora incerta [ 4 ]  . 
la ipf si riscontra tipicamente in soggetti di et media o avanzata , spesso fumatori [ 3 , 5 ]  . raramente la ipf colpisce clusters famigliari [ 6 ]  . 
la distinzione tra la ipf e le altre entit incluse nellattuale classificazione delle polmoniti interstiziali idiopatiche pertanto il fattore pi importante per la corretta stratificazione dei pazienti ai fini prognostici [ 3 ]  . la ipf associata al reperto istopatologico della polmonite interstiziale usuale ( usual interstitial pneumonia , uip ) , pneumopatia fibrosante cronica caratterizzata da un quadro eterogeneo di fibrosi , infiltrato infiammatorio e honeycombing [ 7 ]  . 
tuttavia , il pattern istologico uip non si osserva esclusivamente nella ipf , ma pu essere associato anche ad altre malattie come la 528 radiol med ( 2010 ) 115 : 526538 organising pneumonia or a combination of both [ 10 ]  . mortality for each episode of acute exacerbation varies between 20% and 86% , with death often occurring within 2 weeks of onset [ 11 ]  . 
i soggetti con ipf sono pi predisposti di quelli affetti da altri tipi di fibrosi a sviluppare delle riacutizzazioni gravi della malattia , il cui substrato anatomopatologico il danno alveolare diffuso ( dad ) , oppure la polmonite organizzativa , o un insieme dei due [ 10 ]  . 
importante tener presente che la biopsia chirurgica pu di per s scatenare un episodio di riacutizzazione [ 12 ]  . circa il 20% de pazienti muore invece per complicanze cardio - vascolari . 
a limmagine trasversale hrct dimostra a livello delle basi polmonari la presenza di honeycombing in sede subpleurica , associato a bronchiectasie da trazione ( frecce curve ) ed opacit reticolari . 
la ricostruzione sul piano coronale ( b ) e sagittale ( c ) mostrano la distribuzione delle alterazioni , che dalle basi tendono a risalire lungo le zone periferiche fino a raggiungere gli apici polmonari . radiol med ( 2010 ) 115 : 526538 the upper lung subpleural zones . 
areas of honeycombing are frequently interspersed with normal parenchyma , a reflection of the spatial heterogeneity of the histopathological picture , whereas the alternation of honeycombing with reticular and ground - glass opacities suggests the temporal heterogeneity of the disease . 
le aree di honeycombing sono frequentemente inframezzate da zone di parenchima normale , riflettendo leterogeneit spaziale del sopracitato quadro istopatologico , mentre lalternanza dellhoneycombing ad opacit reticolari e ground - glass suggerisce leterogeneit temporale della malattia . 
non sempre infatti lhoneycombing costituito da areole di iperdiafania assoluta ( cisti ) , cio veri e propri buchi neri disposti su pi strati concentrici e separati da pareti spesse . 
la combinazione dellenfisema nelle zone polmonari superiori con la fibrosi nelle regioni basali ritenuta da alcuni autori indicativa per unentit clinica distinta [ 19 ] , anche se ulteriori studi sono necessari per esplorarne il significato . 
la diagnosi differenziale tra il quadro tipico della uip e quello della polmonite interstiziale non specifica ( nonspecific interstitial pneumonia , nsip ) seconda per prevalenza tra gli istotipi di fibrosi polmonare abbastanza semplice , essendo la nsip il pi delle volte caratterizzata dalla prevalenza di opacit ground - glass a distribuzione 530 radiol med ( 2010 ) 115 : 526538 emphysema is found in approximately one third of patients with ipf , as these are often smokers [ 18 ]  . 
the combination of emphysema in the upper lung zones with fibrosis in the basal regions is regarded by some authors as indicative of a distinct clinical entity [ 19 ] , although further studies are needed to clarify its meaning . 
sebbene esistano in alcuni casi dei reperti che possono rifinire la diagnosi differenziale tra un quadro di uip idiopatico ( ipf ) ed uno associato alle suddette malattie ( tabella 1 ) , la diagnosi definitiva di ipf deve sempre essere corroborata dai dati clinici che escludano possibili eziologie . 
le aree di oligoemia indicative di intrappolamento aereo che in genere favoriscono la diagnosi di polmonite da ipersensibilit cronica , possono essere osservate anche nel pattern tipico della ipf [ 22 ]  . 
limmagine hrct mostra opacit ground - glass periferiche che tendono a risparmiare le regioni subpleuriche ed unarea di consolidazione ( che rappresenta probabilmente unarea focale di polmonite organizzativa ) ( freccia )  . sebbene non siano mai state impiegate in questo contesto , potrebbero migliorare la diagnosi differenziale . questa diagnosi differenziale importante alla luce del dati che dimostrano come la uip associata alle altre malattie sia meno letale della forma idiopatica [ 23 ] , forse perch nelle altre patologie la uip rappresenta uno stadio terminale di un processo di rimaneggiamento strutturale fibrosante , mentre nella ipf rappresenterebbe un substrato patologico primitivo fortemente progressivo . 
la ragione per cui questi pazienti non dimostrano le classiche caratteristiche hrct della uip non chiara , anche se stato ipotizzato che queste siano forme di malattia ancora ad uno stadio iniziale o espressione della coesistenza di parti di polmone interessato da uip e parti da nsip . 
although in some cases certain findings valore prognostico dellhrct il decorso clinico variabile della ipf , caratterizzato dallalternarsi di lunghi periodi di stabilit a fasi di graduale declino ed accelerazioni della malattia , sottolinea la necessit di identificare dei fattori che definiscano meglio la prognosi dei pazienti al momento della diagnosi [ 26 ]  . 
 [ 24 ] dimostrarono che i casi di ipf istologicamente confermati con una hrct tipica per uip avevano una sopravvivenza media significativamente inferiore ( 21 mesi ) di quelli con un quadro hrct indeterminato o suggestivo di nsip ( 69 mesi ) [ 24 ]  . 
questo dato non ha trovato conferma nel lavoro recente di sumikawa et al . 532 radiol med ( 2010 ) 115 : 526538 may refine the differential diagnosis between idiopathic uip ( ipf ) and the above diseases ( table 1 ) , the final diagnosis of ipf requires additional clinical information to exclude potential aetiologies . 
areas of decreased attenuation indicative of air trapping and generally supporting a diagnosis of chronic hypersensitivity pneumonitis may also be observed in the typical pattern of ipf [ 22 ]  . 
the nature of such areas interspersed with fibrosis has not yet been defined in ipf , and expiratory scans , although never used in this context , might help to improve the differential diagnosis . this differentiation is important in view of the evidence that uip associated with other diseases is less lethal than the idiopathic form [ 23 ] , perhaps because in the other diseases uip is the end stage of a process of fibrosing structural remodelling , whereas in ipf , it would represent a heavily progressive primary pathological substrate . 
the reason these patients fail to show the classic hrct appearances of uip is unclear , although it thought that these are forms of initial disease or the expression of the coexistence of uip and nsip in different parts of the lung . 
1 , 6 , 7 [ 25 ]  . prognostic value of hrct the variable clinical course of ipf , characterised by the alternation of long periods of stability with phases of gradual decline and disease acceleration emphasises the need to identify factors capable of better predicting patient prognosis [ 26 ]  . 
 [ 25 ] che , classificando secondo lo schema riportato in tabella 2 le hrct di 98 pazienti con ipf confermata mediante esame istologico , non hanno osservato differenze statisticamente significative in termini di sopravvivenza tra i gruppi di pazienti con aspetto hrct diverso . 
i reperti sono pi suggestivi di polmonite da ipersensibilit che di ipf . proven cases of ipf with an hrct pattern typical of uip had a significantly shorter survival rate ( 21 months ) than those with hrct findings that were indeterminate or suggestive of nsip ( 69 months ) [ 24 ]  . 
 [ 25 ] who , after classifying hrct scans of 98 patients with histologically confirmed ipf according to the scheme in table 2 , failed to find any statistically significant differences in survival rates between the groups of patients with different hrct patterns . 
the same study showed that the degree of fibrosis ( obtained by evaluating ground - glass opacities , reticular patterns and honeycombing ) and the extent of traction bronchiectasis were the only significant predictors of mortality in ipf [ 25 ]  . 
recent studies confirmed that the severity of fibrosis ( reflecting the extent of reticulation and honeycombing ) assessed by visual score at hrct upon diagnosis , along with reduced diffusing capacity of lung for carbon monoxide ( dlco ) , would prove more useful than a typical uip pattern ( assessed , for example , according to the criteria in table 2 ) in predicting outcome in ipf [ 26 , 27 ]  . 
 moreover , emphysema detection on hrct in patients with ipf appears to be another important prognostic indicator , especially considering that patients with ipf and emphysema are more likely to develop pulmonary hypertension , an independent strong predictor of mortality in ipf [ 18 ]  . 
altri recenti studi hanno confermato che la severit della fibrosi ( espressione dellestensione delle reticolazioni e dellhoneycombing ) valutata mediante score visivo allhrct al momento della diagnosi , insieme alla riduzione della capacit di diffusione del monossido di carbonio ( diffusing capacity of lung for carbon monoxide , dlco ) , risulterebbero essere pi importanti della tipicit del pattern uip ( valutata , ad esempio , secondo i criteri riportati in tabella 2 ) nel predire loutcome dei pazienti con ipf [ 26 , 27 ]  . 
 inoltre , lidentificazione dellenfisema allhrct nei pazienti con ipf sembra fornire un altro importante indice prognostico , soprattutto in considerazione del fatto che i pazienti con ipf ed enfisema tendono a sviluppare maggiormente la ipertensione polmonare che un fattore indipendente fortemente predittivo della mortalit nella ipf [ 18 ]  . 
 vi una pletora di esempi in letteratura di studi correlativi che dimostrano una buona concordanza tra lestensione globale della malattia alla tomografia computerizzata ( tc ) e i parametri funzionali nella ipf [ 2830 ]  . 
mentre il grado di ventilazione variabile che si osserva nella uip , composta di spazi aerei cistici ( che possono intrappolare laria o meno ) e marcata fibrosi , probabilmente indebolisce le correlazioni tra estensione di malattia e gli indici volumetrici delle prove di funzionalit respiratoria , per una data estensione di polmone fibrotico la dlco ridotta , riflettendo una mancanza di perfusione ( indipendentemente se il polmone affetto sia ventilato o meno ) [ 31 , 32 ]  . 
therefore , repeat ct scans for the follow - up of patients with stable ipf are not recommended , as changes in respiratory function indices provide a sufficiently accurate reflection of the disease status on hrct . 
ct scans are , however , often repeated in ipf patients , mainly when severe complications are clinically suspected , when new opacities emerge on chest x - ray or prior to transplantation . evaluation of complications with hrct the suspicion of acute exacerbation ( or acceleration ) of the disease raised by superimposed patterns of dad and / or organising pneumonia is a common reason for repeat hrct scans in patients with a known diagnosis of ipf . 
per questo motivo non indicato ripetere lesame tc nel follow - up dei pazienti con ipf in condizioni cliniche stabili , in quanto il trend degli indici di funzionalit respiratoria nel tempo riflette in modo sufficientemente accurato lo status della malattia alla hrct . 
tuttavia , lesame tc viene ripetuto spesso nei pazienti con ipf , principalmente nel sospetto clinico di gravi complicanze , in caso di comparsa di nuove opacit allesame radiografico del torace o in fase pre - trapianto . valutazione delle complicanze con la hrct il sospetto della riacutizzazione ( o accelerazione ) della malattia causato dal sovrapporsi di un quadro di danno alveolare diffuso e / o polmonite organizzativa , motivo frequente di ripetizione di un controllo hrct nei pazienti con ipf gi diagnosticata . 
however , the diagnosis of acute exacerbation is largely based on clinical criteria , and hrct can only confirm the presence of findings compatible with the clinical diagnosis [ 34 ]  . 
the finding of enlarged mediastinal lymph nodes should not be regarded as a sign suggesting or demonstrating the presence of lung cancer , as these tend to be reactive processes in up to 70% of patients with ipf [ 36 ]  . 
a final diagnosis of cancer is made by assessing the behaviour of nodules over time , by fineneedle - aspiration biology or by positron emission tomography ( pet )  . 
in such cases the differential diagnosis includes tuberculosis ( relatively common in patients with interstitial fibrosis and responill - defined sible for atypical presentations such as basal opacities ) , postembolic infarction or plain fibrotic masses . 
la presenza di linfonodi mediastinici ingranditi non deve essere considerata come un segno indicativo o probante di neoplasia polmonare , poich questi si osservano normalmente su base reattiva fino nel 70% dei pazienti affetti da ipf [ 36 ]  . 
la diagnosi definitiva di neoplasia si ottiene valutando il comportamento delle nodularit nel tempo , o mediante agoaspirato o esame di tomografia computerizzata ad emissione di positroni ( pet )  . 
in questi casi la diagnosi differenziale comprende : tubercolosi ( relativamente comune nei pazienti con fibrosi interstiziale e responsabile anche di presentazioni atipiche , come opacit irregolari basali ) , infarti post - embolici o semplici agglomerati fibrotici . 
una massa irregolare ( freccia curva ) apprezzabile allinterno delle aree fibrotiche nel polmone di destra . la diagnosi di adenocarcinoma polmonare stata confermata con la biopsia . patients with ipf and is an indicator of poor outcome [ 18 , 38 , 39 ]  . 
although a correlation exists between diameter of the pulmonary artery main trunk as measured on ct and pulmonary artery pressure as assessed through catheterisation of the right side of the heart , this is not maintained in patients with pulmonary fibrosis [ 38 ]  . 
the increase in ratio between pulmonary artery diameter and ascending aorta diameter appears to be a more reliable ct indicator of pulmonary hypertension in ipf [ 38 ]  . [ 18 , 38 , 39 ]  . 
sebbene esista una correlazione tra il diametro del tronco principale dellarteria polmonare misurato alla tc ed il grado di pressione dellarteria polmonare valutata mediante cateterismo del cuore destro , questa non viene mantenuta nei pazienti con fibrosi polmonare [ 38 ]  . laumento del rapporto tra il diametro dellarteria polmonare e quello dellaorta ascendente sembra essere un indice tc pi accurato per la valutazione della presenza della ipertensione polmonare nella ipf [ 38 ]  . conclusions conclusioni in light of the latest published evidence , ipf appears to evolve according to different clinical phenotypes . 
for a more appropriate diagnostic approach to these patients , further studies are required to define the role of hrct in combination with clinical data and respiratory function tests , possibly based on criteria accounting for the evolution of the disease . 
per ottenere un approccio diagnostico pi appropriato verso questi pazienti , sono necessari ulteriori studi per definire il ruolo della hrct in combinazione con i dati clinici e i test di funzionalit respiratoria , probabilmente basati su criteri evolutivi della malattia . 
bellomi1 , 2 1divisione di radiologia , istituto europeo di oncologia , via ripamonti 435 , 20141 milano , italy 2facolt di medicina e chirurgia , universit degli studi di milano , 20100 milano , italy correspondence to : c . 
thyroid nodules are commonly encountered in clinical practice , and ultrasound ( us ) - guided fine - needle aspiration biopsy ( fnab ) is the gold standard in diagnosing the pathological nature of undetermined thyroid nodules . 
the same freehand technique and capillary - action technique with 22or 25 - gauge needles was used for all nodules , all specimens were prepared and fixed without the cytologist on site and were subsequently analysed by two expert cytologists . 
the rate of nondiagnostic procedures for each group was 32% in group 1 , 13% in group 2 , 17% in group 3 , 11% in group 4 , 10% in group 5 , 5% in group 6 and 8% in group 7 . 
i noduli tiroidei costituiscono un riscontro comune nella pratica clinica e la biopsia con ago sottile ( fnab ) - ecoguidata rappresenta il gold standard diagnostico nella valutazione di pazienti con noduli indeterminati . 
sono state valutate retrospettivamente 700 fnab - ecoguidate consecutive eseguite da un singolo radiologo dal 2000 al 2007 , effettuate con tecnica a mano libera per capillarit con aghi da 22 g o 25 g , preparati ed allestiti senza citologo . 
le procedure non diagnostiche di ogni singolo gruppo sono : 32% nel gruppo 1 , 13% nel gruppo 2 , 17% nel gruppo 3 , 11% nel gruppo 4 , 10% nel gruppo 5 , 5% nel gruppo 6 e 8% nel gruppo 7 . 
abbiamo stimato che siano necessarie almeno 200 procedure prima di raggiungere valori di accuratezza diagnostica riportati in letteratura . suggeriamo pertanto uno specifico training delloperatore prima di intraprendere questa procedura nella pratica clinica . radiol med ( 2010 ) 115 : 612618 keywords fine needle aspiration thyroid nodule ultrasound learning curve parole chiave biopsia con ago stottile nodulo tiroideo ultrasuoni curva di apprendimento introduction introduzione thyroid nodules are a common finding in clinical practice , with a prevalence of 10%67% among adults at ultrasonography ( us ) and 50% at autopsy [ 14 ]  . 
fineneedle aspiration biopsy ( fnab ) of the thyroid is the gold standard for evaluating patients with undetermined thyroid nodules , even though the international guidelines do not agree on the size and features of the nodules to be considered as indications for the procedure [ 1 , 5 , 6 ]  . 
small solid portions may be selected inside complex nodules [ 7 , 8 ] , thus increasing diagnostic accuracy of the procedure , especially in small nodules [ 9 , 10 ]  . 
as occurs in any operatordependent procedure , the radiologists role in us - guided biopsies is fundamental and depends both on the skill acquired with us experience and the ability to adequately prepare the biopsy specimen when the cytologist is not present . the aim of this retrospective study was to determine the learning curve for a single radiologist intent on performing and preparing us - guided thyroid fnab by measuring the rate of diagnostic adequacy and the number of complications observed . materials and methods we retrospectively evaluated 700 consecutive us - guided fnab of thyroid nodules performed by a single radiologist on 602 patients ( 496 males , 106 females ; mean age 53 years , range 1186 years ) between january 2000 and december 2007 . 
the procedures were performed on an outpatient basis on patients referred to us for us - guided cytological sampling of an undetermined , palpable or nonpalpable thyroid nodule following blood - clotting tests . all nodules were > 10 mm , and no exclusion criteria were adopted concerning nodule morphology such that all nodules with a solid , mixed and colloid - cystic echostructure were included . 
the procedures were classified as diagnostic or nondiagnostic on the basis of pathological findings ; i noduli tiroidei costituiscono un riscontro comune nella pratica clinica , con una prevalenza ecografia nella popolazione adulta del 10%67% ed un riscontro autoptico nel 50% dei casi [ 14 ]  . 
lagoaspirato ( fnab , fine needle aspiration biopsy ) della tiroide rappresenta il gold standard diagnostico nella valutazione di pazienti con noduli tiroidei indeterminati , nonostante le linee guida internazionali non siano concordi nel definire le dimensioni e le caratteristiche dei noduli che pongono indicazione alla procedura [ 1 , 5 , 6 ]  . 
lutilizzo della fnab ecoguidata consente di effettuare prelievi di noduli tiroidei non palpabili , valutando in real - time la progressione e la precisa posizione della punta dellago per il campionamento , consentendo anche di sceglire piccole porzioni solide nel contesto di noduli complessi [ 7 , 8 ] implementando cos laccuratezza diagnostica della procedura soprattutto in noduli di piccole dimensioni [ 9 , 10 ]  . 
la percentuale di campioni non diagnostici varia sensibilmente tra i diversi studi , anche in funzione , tra le altre variabili , dellesperienza delloperatore e della valutazione di adeguatezza in sede da parte di un citopatologo [ 11 ]  . 
come per ogni procedura operatore - dipendente , il ruolo del radiologo nella procedura ecoguidata di primaria importanza e dipende sia dallabilit acquisita con lesperienza ecografica sia dalla capacit di allestire adeguatamente il campione prelevato qualora non sia presente il citologo . lobbiettivo di questo studio retrospettivo pertanto stabilire la curva di apprendimento del singolo radiologo nellesecuzione ed allestimento di fnab - ecoguidate tiroidee , valutando la percentuale di adeguatezza diagnostica ed il numero di complicanze riscontrate . materiali e metodi in questo studio sono state valutate retrospettivamente 700 fnab - ecoguidate consecutive di noduli tiroidei eseguite in 602 pazienti ( 496 maschi , 106 femmine ; et media 53 anni , range 1186 anni ) da un singolo radiologo tra gennaio 2000 e dicembre 2007 . 
le procedure sono state effettuate , in regime ambulatoriale , in pazienti giunti con una richiesta di prelievo citologico eco - guidato di nodulo tiroideo indeterminato , sia esso palpabile o non palpabile , previa valutazione dei valori di coagulazione ematica . 
samples were defined as nondiagnostic if at least one of the following conditions was present : acellular sample , heavily blood - stained sample , exclusively colloid material or incorrect slide fixation . to evaluate the operators diagnostic accuracy over time , the procedures were chronologically subdivided into seven consecutive groups of 100 procedures each ; observation periods for each group were 18 months , 16 months , 14 months , 15 months , 12 months , 10 months , and 11 months , respectively . 
for each group , we recorded the number of diagnostic procedures , the number of nondiagnostic procedures and complications . ultrasonographic and cytological technique linear us scans were acquired with a sequoia 512 scanner ( siemens ag , erlangen , germany ) equipped with a multifrequency 15l9w transducer ( siemens ag , erlangen , germany ) by a single radiologist with 2 years experience in us , who started to perform biopsies in january 2000 . 
the biopsy was performed with a free - hand technique using 22 ( n = 112 ) or 25 - gauge ( n = 588 ) needles ( biopsybell , mirandola , italy ) and two consecutive passes . 
the material was sent to the department of pathology where two expert cytologists ( 8 and 10 years experience , respectively ) performed the cytological examination . results among the 700 fnab considered , 86.3% ( n = 604 ) were diagnostic and 13.7% ( n = 96 ) were nondiagnostic . 
nondiagnostic rates for each group were 32% in group 1 , 13% in group 2 , 17% in group 3 , 11% in group 4 , 10% in group 5 , della procedura , sulla scorta del referto anatomo - patologico , stato classificato come diagnostico o non diagnostico , includendo in questultima categoria sia gli esiti inadeguati che insufficienti per diagnosi . 
il campione stato definito non diagnostico se si verificava almeno una delle seguenti condizioni : campione acellulato , campione ampiamente ematico , materiale costituito esclusivamente da colloide o erronea fissazione dei vetrini . al fine di valutare laccuratezza diagnostica delloperatore nel tempo , le procedure sono state stratificate cronologicamente in sette gruppi consecutivi da 100 procedure ciascuno ; i periodi di osservazione per ogni gruppo erano rispettivamente : 18 mesi , 16 mesi , 14 mesi , 15 mesi , 12 mesi , 10 mesi , 11 mesi . 
per ogni gruppo stato successivamente calcolato : il numero di procedure diagnostiche , il numero di procedure non diagnostiche e le complicanze . tecnica ecografica e citologica gli esami ecografici sono stati eseguiti con apparecchiatura sequoia 512 ( siemens ag , erlangen , germania ) equipaggiata con sonda lineare multifrequenza 15l9w ( siemens ag , erlangen , germania ) , da un singolo radiologo con 2 anni di esperienza diagnostica ecografica , che ha iniziato nel gennaio 2000 a eseguire procedure bioptiche . 
la procedura consiste in una preliminare valutazione ecografica per individuare il reperto da sottoporre a prelievo citologico e scegliere lapproccio ottimale per il prelievo , previa dettagliata spiegazione al paziente la procedura , chiedendogli di non deglutire durante il prelievo . 
la procedura bioptica stata eseguita con tecnica a mano libera utilizzando aghi da 22g ( n = 112 ) o 25g ( n = 588 ) ( biopsybell , mirandola , italia ) con due prelievi consecutivi . 
il materiale prelevato stato inviato in anatomia patologica per valutazione citologica eseguita da due citologi esperti ( 8 e 10 anni di esperienza )  . risultati nelle 700 fnab valutate il materiale prelevato risultato diagnostico nell86.3% ( n = 604 ) , con una percentuale di procedure non diagnostiche del 13.7% ( n = 96 )  . 
le percentuali non diagnostiche di ogni singolo gruppo sono risultate : 32% nel gruppo 1 , 13% nel gruppo 2 , 17% nel gruppo 3 , 11% nel gruppo 4 , 10% nel gruppo 5 , 5% nel gruppo 6 e 8% nel gruppo 7 ; i valori sono rappresentati radiol med ( 2010 ) 115 : 612618 groups fig . 
there were two episodes of presyncope in group 1 and three cases of moderate bleeding at the biopsy site in groups 1 , 2 , and 5 , all of which resolved spontaneously . 
non sono state riportate complicanze maggiori nelle 700 procedure ; abbiamo osservato 2 episodi lipotimici nel gruppo 1 e tre modesti episodi emorragici nella sede del prelievo , uno nel gruppo 1 , uno nel gruppo 2 ed uno nel gruppo 5 , tutti risoltisi spontaneamente . 
 discussion discussione because the diagnostic accuracy of us , whether alone or combined with colour doppler imaging , in characterising laccuratezza diagnostica della sola ecografia , anche con lausilio del color - doppler , nella caratterizzazione di noduli tiroidei indeterminati risultata inadeguata [ 12 ] , pertanto la table 1 summary of study results subdivided into seven groups group 1 group 2 group 3 group 4 group 5 group 6 group 7 tabella 1 risultati dello studio , suddivisi nei sette gruppi mean age ( years ) range nondiagnostic ( % ) complications 2486 et media ( anni ) range non diagnostici ( % ) complicanze 2486 1875 1875 1880 1880 1175 1175 1284 1680 2588 1284 1680 2588 gruppo 1 gruppo 2 gruppo 3 gruppo 4 gruppo 5 gruppo 6 gruppo 7 616 radiol med ( 2010 ) 115 : 612618 undetermined thyroid nodules is inadequate [ 12 ] , fnab has progressively asserted itself as the diagnostic gold standard . 
although easy to perform , us - guided thyroid fnab is characterised by a varying rate of nondiagnostic samples related to different variables , including limited experience , and this could be a confounding factor in the interpretation of several studies . as reported by ljung et al . 
because the training of young radiologists is key to the success of the procedure , the biopsy should be done under the supervision of an expert radiologist . training should consist of an initial observation period to learn to evaluate the importance of the indication and procedures technical feasibility and to refine patient management and communication skills . 
moreover , continuity in the practice of biopsy procedures should be guaranteed to ensure a constant rate of diagnostic adequacy over time . to our knowledge , there are no published data have indicated a minimum number of procedures to be done to achieve the reported inadequacy rates of 4%16% [ 9 , 15 , 16 ]  . 
in this study , an inexperienced radiologist had a high rate of nondiagnostic fnab in the first 100 procedures ( 32% ) ; that is , an excess of nondiagnostic fnab , which leads to higher costs due to repeat procedures and greater patient discomfort . 
groups 47 , hence after 300 procedures , were characterised by excellent results , with inadequacy rates ranging from 5% to 11% . because the radiologist was the only operator in this study , rates reflect the overall experience with the procedure that is , related to skills acquired in us imaging , manual dexterity in correctly positioning the needle inside fnab si imposta come il gold standard diagnostico . 
le fnabecoguidate della tiroide pur costituendo una procedura di semplice esecuzione sono gravate da percentuali variabili di campioni non diagnostici , legate a diverse cause , tra le quali linesperienza delloperatore , che potrebbe inoltre costituire un fattore confondente nellinterpretazione dei risultati di diversi studi . 
 [ 13 ] , la percentuale non - diagnostica in 314 fnab mammarie eseguite da medici senza uno specifico training era del 36 , 9% rispetto al 2 , 2% in 729 fnab dei medici formati con adeguato training . 
costituendo pertanto il training del giovane radiologo un aspetto fondamentale della procedura , esso deve essere condotto sotto la supervisione di un radiologo esperto e dovrebbe constare inizialmente di un periodo di esclusiva osservazione per valutare limportanza dellindicazione e della fattibilit dellesame e non ultimo per affinare la capacit nella gestione e nella comunicazione con il paziente . 
solo successivamente iniziare ad allestire il materiale sui vetrini ed infine eseguire la procedura ; entrambe queste fasi dovrebbero comunque essere condivise con il radiologo esperto , eseguendo nello specifico , per ogni nodulo , un prelievo a testa nei primi pazienti . 
 in base alle nostre conoscenze , in letteratura non sono riportati dati che suggeriscano il numero minimo di procedure da eseguire per raggiungere le percentuali di inadeguatezza riportate in letteratura , che oscillano tra il 4% ed il 16% [ 9 , 15 , 16 ]  . 
in questo studio , un radiologo non esperto ha fornito unelevata percentuale di fnab nondiagnostiche nelle prime 100 procedure ( 32% ) , valori eccessivi che comportano maggiori costi per la ripetizione della procedura e disagio per il paziente . 
come atteso , lesperienza acquisita ha ridotto la percentuale di fnab non - diagnostiche nel gruppo 2 ( 13% ) : sulla scorta della nostra esperienza personale , sono pertanto state necessarie almeno 200 procedure per garantire risultati in linea con quelli riportati in letteratura . 
nel gruppo 3 , la percentuale di inadeguati inaspettatamente aumentata ( 17% ) rispetto al gruppo 2 ; questo dato potrebbe essere spiegato dalleccessiva confidenza acquisita dalloperatore , guidandolo a eseguire fnab su noduli tecnicamente di difficile esecuzione . 
come previsto i gruppi 47 , pertanto dopo 300 procedure , mostrano invece ottimi risultati con inadeguati variabili tra l5% e l11% . in questo studio , essendo il radiologo lunico operatore , le percentuali ottenute riflettono lesperienza complessiva della procedura , legata sia allabilit acquisita in campo ecografico , sia alla manualit per il corretto radiol med ( 2010 ) 115 : 612618 the nodule and technical skill in adequately preparing the slides in the absence of a on - site cytologist [ 17 ]  . 
the first is related to our failure to determine the diameter ( in any case , all > 10 mm ) and morphological features of the nodules , which would have allowed us to further stratify the nondiagnostic rate in relation to sampling complexity . furthermore , results refer to the personal experience of a single radiologist and thus may vary substantially among operators with different manual and us skills . to conclude , the rate of nondiagnostic us - guided fnab in our series was heavily dependent on operator experience , with at least 200 procedures being necessary to achieve the recommended levels of diagnostic accuracy [ 9 , 15 , 16 ]  . 
we therefore suggest that operators receive specific training before embarking on this procedure in clinical practice . posizionamento dellago nel nodulo , sia alle competenze tecniche per allestire adeguatamente i vetrini senza citologo on - site [ 17 ]  . 
tecnicamente i prelievi sono stati eseguiti per capillarit rispetto alla tecnica in aspirazione : questa modalit pi semplice e garantisce risultati sovrapponibili allaspirazione , come mostrato da tublin et al . 
il primo legato alla mancanza della valutazione del diametro dei noduli ( tutti comunque 10 mm ) e le definizioni delle caratteristiche morfologiche , che avrebbe permesso di stratificare ulteriormente la percentuale non diagnostica in relazione alla difficolt del prelievo . 
i risultati esposti sono inoltre frutto dellesperienza personale di un singolo radiologo : pertanto , essi potrebbero variare sostanzialmente tra diversi operatori con manualit e abilit ecografiche differenti . concludendo , nella nostra casistica personale la percentuale non - diagnostica di fnab - ecoguidate tiroidee fortemente dipendente dallesperienza delloperatore , rendendo necessarie almeno 200 procedure prima di raggiungere valori diagnostici in linea a quanto raccomandato in letteratura [ 9 , 15 , 16 ]  . 
feltrin1 1department of medical diagnostic sciences and special therapies , 2department of neurosciences , university of padova , via giustiniani 2 , 35128 padova , italy 3department of environmental medicine and public health , university of padova , via loredan 18 , 35131 padova , italy corresponding to : r . 
a systematic clinical evaluation based on the medical research council scale and mri was completed in ten patients with calpainopathy [ limb - girdle muscular dystrophy ( lgmd ) - 2a ] , 16 with dysferlinopathy ( lgmd - 2b ) , ten with hyaline body myopathy ( hbm ) , six with myotonic dystrophy ( md ) types 1 and 5 with md type 2 . 
la valutazione clinica , basata sulla scala del medical research council , e la rm sono state eseguite su 10 pazienti con calpainopatia ( lgmd2a ) , 16 con disferlinopatia ( lgmd2b ) , 10 con miopatia a corpi ialini ( hbm ) , 6 con distrofia miotonica di tipo 1 ( md1 ) e 5 con il tipo 2 ( md2 )  . 
la rm rappresenta unimportante tecnica diagnostica utile nella diagnosi differenziali grazie ai diversi pattern di interessamento muscolare . keywords muscle mri dystrophies myopathies parole chiave muscolo rm distrofie miopatie introduction introduzione magnetic resonance imaging ( mri ) is becoming the method of choice among the various imaging instruments used to assess dystrophic muscular diseases . 
comparative studies on ct and mri techniques have also shown that mri is more sensitive than ct in identifying early fatty replacement in muscles [ 2 , 3 ] , as well as providing better anatomical details . 
as with other investigators , we recently conducted several studies using this approach in various neuromuscular disorders . nowadays , mri can be used to establish the entity and mode of evolution of the processes characterising such diseases , i.e. 
the continual discovery of new subcategories of neuromuscular diseases deriving from various genetic disorders demands even more accurate imaging analyses with a view to finding specific patterns of muscle involvement amidst overlapping phenotypes . 
 limb girdle muscular dystrophy lim - girdle muscular dystrophy ( lgmd ) - 2a ( calpainopathy ) and lgmd - 2b ( dysferlinopathy ) are characterised by weakness and atrophy of the proximal muscles of the pelvic and scapular girdles , with no facial muscle involvement . 
lgmd - 2a and 2b account for about 30% and 20% , respectively , of all cases of lgmd [ 5 , 6 ]  . hyaline body myopathy la risonanza magnetica ( rm ) sta diventando il metodo di scelta tra i vari strumenti di imaging nella valutazione delle distrofie muscolari . 
la rm venuta a sostituire quasi completamente luso della tomografia computerizzata ( tc )  . i principali vantaggi della rm sulla tc sono lassenza di radiazioni ionizzanti e la possibilit di eseguire scansioni multiplanari [ 1 ]  . 
studi comparativi sulle tecniche di tc e rm hanno inoltre dimostrato che la rm pi sensibile della tc nellidentificazione precoce della sostituzione adiposa nei muscoli [ 2 , 3 ] , oltre a fornire migliori dettagli anatomici . 
oggi , la rm pu essere usata per stabilire lentit e le modalit di evoluzione dei processi che caratterizzano questo tipo di malattie , vale a dire linfiltrazione fibro - adiposa muscolare e ledema intramuscolare . la continua scoperta di nuove sottocategorie di malattie neuromuscolari , derivanti da diverse alterazioni genetiche , richiede unanalisi ancora pi accurata delle immagini al fine di trovare modelli di coinvolgimento muscolare differenti per patologie fenotipicamente in parte sovrapponibili . distrofie muscolari le distrofie muscolari dei cingoli , calpainopatia ( lgmd2a ) e disferlinopatia ( lgmd2b ) , sono caratterizzate da debolezza ed atrofia dei muscoli prossimali del cingolo pelvico e scapolare , senza coinvolgimento dei muscoli facciali . 
il decorso clinico varia notevolmente [ 4 ]  . nella lgdm2a , la scapola alata di solito compare gi nelle fasi iniziali mentre la postura a gambe divaricate dovuta a una sorprendente conservazione degli adduttori dellanca . la lgdm2b mostra il tempestivo coinvolgimento del muscolo gastrocnemio , mentre linteressamento scapolare minimo e non appare allesordio . 
lgmd2a e 2b rappresentano rispettivamente circa il 30% e il 20% di tutti i casi di lgmd [ 5 , 6 ]  . hyaline body myopathy ( hbm ) patients typically have muscle weakness , and eosinophil hyaline bodies are found inside the type 1 muscular fibres [ 7 , 8 ]  . 
the fibular - scapular and the girdle miopatia a corpi ialini la miopatia a corpi ialini ( hbm ) si caratterizza per debolezza muscolare e per la presenza di corpi ialini eosinofili radiol med ( 2010 ) 115 : 585599 phenotypes . 
the latter features minor loss of strength in the muscles of the superior girdle , bilateral scapular winging , weakness of the proximal rather than distal lower limbs , weakness of the superficial extensor muscle of the toes , calf muscle hypertrophy and hypotrophy of the deep muscles in the hand [ 7 ]  . nelle fibre muscolari di tipo 1 [ 7 , 8 ]  . 
sono stati distinti due fenotipi : il fenotipo scapolo - peroneale caratterizzato da scapola alata , debolezza dei muscoli della spalla , postura iperlordotica e debolezza marcata dei muscoli estensori del piede e dellalluce . 
il fenotipo dei cingoli mostra un deficit di forza minore nei muscoli del cingolo superiore , scapola alata bilaterale , debolezza prossimale ( pi che distale ) degli arti inferiori , debolezza del muscolo estensore superficiale delle dita , ipertrofia dei muscoli del polpaccio ed ipotrofia dei muscoli intrinseci della mano [ 7 ]  . myotonic dystrophy myotonic dystrophy ( md ) is characterised by myotonia , weakness and atrophy [ 9 ]  . 
md - 1 is due to a ctg expansion in the 3 untranslated region of the dmpk gene [ 10 , 11 ] and typically involves the distal muscles and those of the face , neck and fingers . 
in md - 2 , due to a cctg expansion in the first intron of the zfn9 gene [ 12 , 13 ] , the proximal muscles are more often involved at onset , particularly in the pelvic girdle [ 3 ]  . 
as the disease progresses , the pattern of muscle involvement tends to overlap in the two forms of md , with weakness also becoming proximal in md - 1 and distal in md2 [ 14 ]  . 
symptoms of md seem to result from the alternative splicing of proteins due to amplified rna filaments [ 15 ]  . here , we report on a 4 - year experience using muscularskeletal mri in three types of muscular disease , i.e. 
skeletal muscles measured were as follows : deltoid , biceps brachii , distrofia miotonica la distrofia miotonica ( md ) caratterizzata da miotonia , debolezza muscolare ed atrofia [ 9 ]  . 
la md1 dovuta ad una espansione della tripletta ctg presente nella regione non tradotta al 3 del gene dmpk [ 10 , 11 ] ed in genere coinvolge i muscoli distali e quelli del viso , del collo e delle dita . 
la md2 , dovuta allespansione della sequenza cctg nel gene della proteina zfn9 [ 12 , 13 ] coinvolge allesordio pi spesso i muscoli prossimali , in particolare del cingolo pelvico [ 3 ]  . 
al progredire della malattia , il pattern di coinvolgimento muscolare tende a sovrapporsi nelle due forme di md : la debolezza diventa prossimale nella md1 e distale nella md2 [ 14 ]  . 
la sintomatologia della md sembra essere il risultato del sequestro di specifiche proteine da parte di filamenti di rna amplificato [ 15 ]  . riportiamo lesperienza di quattro anni di utilizzo della rm nello studio di tre tipi di malattia muscolare , cio distrofia muscolare dei cingoli ( lgmd2a e lgmd2b ) , hbm , e md1 md2 . 
la diagnosi molecolare 588 radiol med ( 2010 ) 115 : 585599 triceps brachii , iliopsoas , gluteus maximus , thigh flexors ( quadriceps , rectus femoris , sartorius ) , thigh extensors ( semimembranosus , semitendinosus , biceps femoris ) , thigh adductors ( magnus , brevis , longus ) , thigh abductors ( glutei medium et minimus , tensor fasciae latae ) , foot extensors ( triceps surae , fibularis longus ) and tibialis anterior . 
acquisition parameters were : 8 mm axial slice thickness ; flip angle 150 shoulderarm t1 scans ( tr 474 ms ; te 8.7 ms ) ; tirm scans ( tr 3030 ms ; te 38 ms ) limb - girdle t1 scans ( tr 478 ms ; te 8.8 ms ) ; tirm scans ( tr 4 , 160 ms ; te 72 ms ) thighleg t1 scans ( tr 596 ms ; te 8.7 ms ) ; tirm scans ( tr 4 , 160 ms ; te 72 ms ) images were assessed separately by four radiologists with intrareader and interreader comparison in quantifying mri muscle changes . each test took about 45 m patients had scans of the scapular and forearm girdle of the right hemisoma ( for technical convenience ) and of the skeletal muscles of both lower limbs . 
i muscoli scheletrici sono stati analizzati come di seguito : deltoide , bicipite brachiale , tricipite brachiale , ileo - psoas , grande gluteo , flessori della coscia ( quadricipite , retto femorale , sartorio ) , estensori della coscia ( semimembranoso , semitendinoso , bicipite femorale ) , adduttori della coscia ( grande , lungo , breve ) , abduttori della coscia ( glutei medio e piccolo , tensore della fascia lata ) , estensori del piede ( tricipite surale , peronieri ) e tibiale anteriore . 
il caratteristico coinvolgimento dellavambraccio nei pazienti con md1 e hbm ha richiesto di analizzare anche il flessore del carpo , il flessore delle dita , gli estensori del carpo e gli estensori delle dita . 
singoli muscoli che sembravano particolarmente interessati sono stati analizzati in maniera pi approfondita ( ad esempio , il tibiale posteriore in pazienti con lgmd )  . apparecchiatura rm stata utilizzata unapparecchiatura rm da 1 , 5 t ( avanto , siemens , erlangen , germania ) per studiare i segmenti corporei con scansioni assiali t1 - pesate e sequenze turbo inversion recovery magnitude ( tirm ) presso listituto di radiologia delluniversit degli studi di padova . 
i pazienti sono stati sottoposti a scansioni del cingolo scapolare e dellavambraccio del solo emisoma destro ( per convenienza tecnica ) e dei muscoli scheletrici di entrambi gli arti inferiori . 
nei pazienti mci e dm1 stata aggiunta lacquisizione delle immagini dellavambraccio destro allo scopo di valutare i muscoli estensori e flessori dellavambraccio che appaiono generalmente compromessi da un punto di vista clinico . 
 short - tau inversion recovery ( stir ) or tirm sequences can help highlight disease in muscles that appear normal on t1 images or to clarify the nature of abnormal signals in various muscle disorders due to different genetic and protein defects . 
as the highest values on the mrc scale coincided with a normal function , whereas the highest score on the fibroadipose replacement and oedema - like changes scale corresponded with the worst signs , mrc scores were reversed so that the absence of movement scored 5 and a normal function scored 0 . statistical analysis consistency between the inverted mrc scale and the modified mercuri scale was assessed using the bland - altman method [ 19 ] and lins coefficient of concordance and correlation [ 20 ]  . 
la distribuzione delledema stata anche registrata come interfascicolare ( fluido nello spazio interfascicolare ) o intrafascicolare ( fluido nello spazio tra le singole miofibre )  . ledema stata definito come segmentato se interessa meno della met delle sezioni acquisite del muscolo , o come globale se interessa pi della met delle acquisizioni assiali . stato adottato un apposito score delledema : 0 , assente ( punteggio 0 ) ; 1 , lieve , interfascicolare ( punteggio 1 ) ; 2a , lieve , intrafascicolare , segmentato ( punteggio 2 ) ; 2b , lieve , intrafascicolare , globale ( punteggio 3 ) ; 3a , moderato , intrafascicolare , segmentato ( punteggio 4 ) ; 3b , moderato , intrafascicolare , globale ( punteggio 5 )  . 
poich i pi alti valori sulla scala mrc coincidono con una normale funzione muscolare , mentre i punteggi pi alti per la sostituzione fibro - adiposa e ledema corrispondono a danno maggiore , la scala mrc stata invertita in modo che la paralisi totale corrisponda a 5 e una forza muscolare normale corrisponda a 0 . analisi statistica laccordo tra la scala mrc inversa e la mercuri modificata stato valutato attraverso il metodo di bland e altman [ 19 ] ed il coefficiente di concordanza correlazione ( ccc ) di lin et al . 
il metodo di bland e altman prevede di calcolare i limiti di accordo per la media delle differenza tra le valutazioni ottenute con le due scale e di rappresentare graficamente i valori relativi alla media ed alla differenza delle due scale per ciascuna valutazione , la media delle differenze ed relativi i limiti di accordo . fibroadipose replacement particularly affected the biceps brachii in the scapular girdle , thigh abductors in the pelvic girdle , adductor muscles at thigh level and semitendinosus , semimembranosus and biceps femoris . 
 md - 1 patients fibroadipose muscle replacement affected all segments examined to some degree , the most affected being the flexoris and extensoris digitorum muscles ( forearm ) , quadriceps , fibularis , and especially triceps surae . 
la sostituzione fibroadiposa colpisce i muscoli gluteo medio e tensore della fascia lata ( cingolo pelvico ) , e gli adduttori , ma soprattutto i muscoli semitendinoso , semimembranoso , bicipite femorale ( zona posteriore della coscia ) e quelli del compartimento anteriore e posteriore della gamba . 
lanalisi statistica ha dimostrato che la scala mrc inversa ( valutazione clinica ) sottostima sistematicamente il deterioramento della malattia rispetto alla scala mercuri ( imaging ) ( tabella 1 )  . 
statistics showed that the inverse mrc score ( clinical evaluation ) systematically underestimates deterioration in the disease by comparison with the mercuri scale ( mri ) ( table 1 )  . 
for each muscular pathology are reported the number of patients analysed , the number of muscle groups studied and the number of total evaluations ( resulting from the number of patients by the number of muscle groups analysed )  . 
for vengono riportati il numero di pazienti analizzati , il numero di gruppi muscolari studiati ed il numero di valutazioni complessive ( risultanti dal numero di pazienti per il numero di gruppi muscolari analizzati )  . 
per ogni patologia , la media e la differenza tra gli score clinici ( mrc ) e di imaging ( mercuri ) ottenuti per singolo gruppo muscolare di ogni paziente , permettono di calcolare il coefficiente di lin di concordanza tra clinica ed imaging : i dati ottenuti dimostrano una buona concordanza solo nei pazienti con md2 . inoltre in tutte le patologie studiate , la media delle differenze tra score clinico e di imaging ha sempre valore negativo : questo indica che la valutazione clinica tende a sottostimare linteressamento muscolare . 
per quanto riguarda laccordo , i limiti sono ampi per le prime quattro patologie ed il coefficiente di lin indica uno scarso grado di accordo , mentre per il md2 i limiti risultano vicini con un conseguente buon grado di accordo . 
i nostri risultati confermano i dati in letteratura , cio che i muscoli del compartimento anteriore della coscia sono interessati pi tardivamente , e che gracile e sartorio tendono ad essere risparmiati fino alla fase pi avanzate della malattia [ 2123 ]  . nella nostra esperienza , il muscolo gracile sembra pi risparmiato rispetto al sartorio nei pazienti lgmd2b , e viceversa in caso di lgmd2a . 
questi due muscoli hanno mostrato un segnale normale e una lieve ipertrofia ( probabilmente a causa della loro funzione vicariante ) fino a fasi avanzate della malattia e la tendenza a subire sostituzione fibro - adiposa completa , quando sopraggiunge la perdita della deambulazione . 
la considerazione che alcuni segmenti del muscolo siano maggiormente sottoposti a stress meccanico e che questo potrebbe influenzare in modo negativo lequilibrio tra danneggiamento e riparazione dei miociti ha portato ad 594 radiol med ( 2010 ) 115 : 585599 fig . 
the x - axis shows the average of the two scales , and the y - axis shows the differences between the two scales for each muscle or muscle group . 
come si visto nella tabella , la valutazione clinica ( mrc ) sottostima il coinvolgimento muscolare rispetto alla valutazione con limaging ( mercuri )  . mean ( inversemrc , mercuri ) replacement . 
our compartments of the thigh were the most affected by fibroadipose findings confirmed previous data that the adductor muscles and anterior thigh compartment become involved later on , and the sartorius and gracilis tend to be preserved until the final stage of the disease [ 2123 ]  . 
these two muscles showed a normal signal and a slight hypertrophy ( probably because of their vicarious function ) up until the final stages and tended to undergo complete fibroadipose replacement , which is when the loss of ambulation occurs . indagare in quale modo avvenisse la degenerazione in due grossi muscoli biarticolari della coscia ( un flessore : bicipite femorale ; un estensore : vasto laterale ) e del tricipite della sura nella gamba . 
il coinvolgimento apparso omogeneo ( ossia il muscolo era coinvolto in tutta la sua estensione ) nel 40% dei casi , non omogeneo ( ossia il muscolo era coinvolto parzialmente alle estremit ) nel 60% , mentre in nessun caso ( 0% ) vi era una manifestazione a chiazze ( il muscolo mostra focus isolati di degenerazione lungo la sua estensione ) : questa valutazione attribuisce peso allipotesi che il processo involutivo abbia origine laddove si sviluppi il maggior carico tensivo e che poi progredisca prossimalmente o distalmente . 
nei radiol med ( 2010 ) 115 : 585599 muscles come under mechanical stress of different intensity towards their segments , and this might negatively influence the balance between myocyte damage and repair . this was the hypothesis behind our investigation on the model of degeneration in two large bi - articular thigh muscles ( flexor : biceps femoris ; extensor : vastus lateralis ) and in the triceps surae . 
it was selectively spared in lgmd - 2a ( the mercuri score for the tibialis posterior was 0 or 1 in all patients ) , even in severe cases , whereas in lgmd - 2b , it underwent severe fibroadipose replacement ( only 15% of muscles scored 0 or 1 )  . hbm patients generally had lower fibroadipose muscle replacement scores than in cases of lgmd - 2a / 2b , with correspondingly less invalidating symptoms . 
in all body parts examined , md cases showed less severe muscle involvement than in lgmd or hbm , particularly in t1 - weighted sequences , consistent with slower progression of the disease ( so oedema - like changes and fibroadipose replacement become concentrated in the same districts )  . 
the fibroadipose replacement pattern in four bi - articular muscles ( vastus lateralis , soleus and medial and lateral heads of the gastrocnemius ) was also investigated and found homogeneous in most cases ( 74% of muscles )  . 
this was particularly true of md - 1 cases , in pazienti lgmd , un altro muscolo coinvolto nella sostituzione fibro - adiposa stato il tibiale posteriore : esso selettivamente risparmiato nei pazienti lgmd2a ( il grading secondo la scala mercuri per il tibiale posteriore 0 o 1 in tutti i pazienti ) , anche in casi gravi , mentre in lgmd2b subisce una grave sostituzione fibro - adiposa ( solo nel 15% dei casi lo score era equivalente a 0 o 1 )  . 
in ogni muscolo della coscia la degenerazione adiposa ha riguardato principalmente la parte distale del ventre muscolare ; questa ultima constatazione non stato riscontrata a livello di gamba n di arto superiore . 
in tutti i distretti muscolari in esame , emerso nei casi di md un coinvolgimento dei muscoli meno grave rispetto ai pazienti con hbm ed lgmd , in particolare nelle sequenze t1 - pesate , coerente con una pi lenta progressione della malattia ( edema e sostituzione fibro - adiposa si concentrano parallelamente negli stessi distretti )  . 
 stato analizzato anche il pattern di degenerazione fibroadiposa in quattro muscoli bi - articolari ( il vasto laterale , soleo , e capi mediale e laterale del gastrocnemio ) ed stato trovato omogeneo nella maggior parte dei casi ( 74% )  . 
nelle cosce dei pazienti con md1 le sequenze t1w hanno mostrato un caratteristico aspetto di iperintensit di segnale a forma di mezzaluna profonda antero - femorale , legato alla sostituzione fibroadiposa del vasto intermedio e vasto mediale , ma non nel vasto laterale ( pi superficiale ) , retto femorale e sartorio . questa reperto descritto in alcuni studi analoghi [ 2426 ] , era presente nel 50% dei nostri pazienti con md1 e potrebbe 596 radiol med ( 2010 ) 115 : 585599 fig . 
schema riassuntivo dei livelli di sostituzione fibro - adiposa e di edema nella coscia e nella gamba che dimostra differenze di coinvolgimento muscolare nelle patologie analizzate . which distal involvement is typical , but was also seen in one md - 2 patient with severe muscle degeneration . 
t1 - weighted sequences disclosed a characteristic crescent - shaped , deep , anterofemoral , hyperintense signal in the thighs of md - 1 patients due to fibroadipose replacement in the vastus intermedius and vastus medialis but not in the more superficial vastus lateralis , rectus femoris and sartorius muscles . this finding has been described in some , but not all [ 2426 ] , other similar studies . 
nei pazienti con md2 , i muscoli della coscia sono stati i pi colpiti dalla degenerazione fibro - adiposa , che appare pi prossimale rispetto ai pazienti con md1 . nelle patologie muscolari degenerative , ledema rappresenta il primo step di un danno muscolare che evolve in sostituzione fibro - adiposa ed atrofia muscolare . 
in maniera analoga a tutte le patologie studiate il segnale delledema presente in maniera lieve nelle fasi iniziali e in quelle tardive e permane in genere elevato soprattutto dove il processo attivo . 
contrariamente alle aspettative , ledema non correlabile con il radiol med ( 2010 ) 115 : 585599 in these degenerative muscle diseases , oedema - like change is the first observable step in muscle damage , which then develops into fibroadipose replacement and muscle atrophy . 
in all the diseases examined here , there were signs of oedema - like changes , which were mild in the early and late phases and moderate in the intermediate phase . 
 the mercuri score proved useful , but it is more important to compare muscles and the overall gestalt of the pattern of degeneration rather than its severity in individual muscles . identifying a specific pattern in patients with the same form of neuromuscular disorder can be hindered by the fact that patients may have different degrees of clinical and functional impairment and consequently of muscle involvement on mri . 
these patterns are more obvious in patients with mild phenotypes , whose individual muscles are selectively involved , but they can also be seen in patients with more severe phenotypes , whose same muscles are clearly more affected [ 26 ]  . when we compared the progression of adipose replacement ( mercuri score ) with changes in clinical neurological values ( mrc scale ) [ 2729 ] , we found inconsistencies between the two sets of values in a large number of cases : inverse mrc score ( clinical evaluation ) systematically underestimates deterioration in the disease by comparison with the mercuri scale ( mri ) in all the diseases we studied . this may be due to compensatory mechanisms in individual muscle . 
 indeed , the advantage of mri compared with clinical evaluation is due to its ability to assess each individual muscle . the lin coefficient showed little concordance for lgmd - 2a / 2b , hbm and md - 1 , whereas it was better for md - 2 . 
viceversa , i pazienti con md hanno percentuali pi basse di sostituzione fibro - adiposa rispetto allimbibizione edematosa per ciascun gruppo muscolare : infatti un lento processo lascia unampia finestra temporale di persistenza delledema cui corrisponde un andamento pi favorevole e meno progressivo . la scala mercuri si rivelata utile , ma pi importante confrontare i gruppi muscolari e il tipo di pattern di degenerazione , piuttosto che valutare la severit di involuzione dei singoli muscoli . 
lindividuazione di un modello specifico in pazienti con la stessa forma di malattia neuromuscolare pu essere ostacolata dal fatto che i pazienti possono avere diversi gradi di deterioramento clinico e funzionale e , di conseguenza , di coinvolgimento muscolare alla rm . 
di solito possibile , tuttavia , riconoscere un gradiente di degenerazione ed individuare i muscoli pi o meno colpiti . questi modelli sono pi evidenti nei pazienti con fenotipo meno aggressivo , nei quali singoli muscoli sono selettivamente coinvolti , ma pu essere riconosciuto anche in pazienti con fenotipi pi gravi , nei quali gli stessi muscoli sono chiaramente pi colpiti [ 26 ]  . confrontando la progressione della sostituzione adiposa ( mercuri score ) con i cambiamenti della funzionalit neurologica ( scala mrc ) [ 2729 ] , si sono riscontrate incongruenze tra le due serie di valori in un gran numero di casi : sistematicamente la scala mrc - inversa ( valutazione clinica ) sottostima il deterioramento muscolare rispetto alla scala mercuri ( mri ) in tutte le patologie studiate . 
talvolta landamento clinico era in contraddizione con i reperti di imaging , ad esempio , nonostante le evidenze cliniche di un peggioramento della malattia , la risonanza magnetica ha evidenziato muscoli ben conservati con un normale trofismo , o viceversa . 
infatti il vantaggio della rm rispetto alla valutazione clinica dovuta alla sua capacit di valutare ogni singolo muscolo . il coefficiente di concordanza di lin ha dimostrato uno scarso grado di accordo per lgmd2a / 2b , hbm e md1 , mentre per il md2 i limiti risultano vicini con un conseguente buon grado di accordo . 
i pazienti md2 presentano generalmente un grado di interessamento muscolare molto meno marcato rispetto alle altre patologie : si pu ipotizzare quindi che laccordo tra valutazione neurologico - clinica e 598 radiol med ( 2010 ) 115 : 585599 muscle involvement than patients with the other disorders , so the concordance between clinicalneurological and imaging findings is probably lower the greater the disease severity . 
based on our hypothesis , a deep fibroadipose replacement in selectively involved muscle districts does not implicate a proportional decline in muscle strength , and whereas clinical evaluation strictly concerns muscle groups , mri can investigate every single fibre . 
finally , in patients with generalised complete muscle replacement , mri findings were consistent with the mrc scores . figure 6 shows the different distribution of muscle damage in the disorders considered here , indicating that mri can help pinpoint asymptomatic patients ( typically with md ) [ 28 ] and in staging and follow - up . 
given the peculiar horseshoe and anterofemoral crescent patterns identified and the differences between imaging findings in cases of md , lgmd and hbm , it seems appropriate to give mri a role in the differential diagnosis of these myopathies . radiologica vada diminuendo allaggravarsi della patologia . in base alla nostra ipotesi , una grave sostituzione fibroadiposa in distretti muscolari selettivamente interessati non implica una proporzionale diminuzione della forza muscolare : a differenza dalla valutazione clinica che valuta selettivamente gruppi muscolari , la rm pu analizzare ogni singolo muscolo . 
infine , in pazienti con una sostituzione completa del muscolo , la risonanza magnetica fornisce risultati coerenti con il punteggio mrc . la figura 6 riassume la diversa distribuzione di danno muscolare nelle 5 malattie studiate , evidenziando come la rm possa aiutare ad individuare i pazienti asintomatici ( in genere con md ) [ 30 ] come nella stadiazione e il follow - up . inoltre la sua precisa valutazione del danno muscolare la rende utile guida di prelievi bioptici . 
fugazzola1 1department of radiology , 2department of medical physics , 3department of stomatology , university of insubria , viale borri 57 , 21100 varese , italy correspondence to : m . 
effective dose and dose to the main organs of the head and neck were evaluated by means of thermoluminescent dosimeters ( tlds ) placed in an alderson rando anthropomorphic phantom and using a standard cbct protocol and an optimised msct protocol . five patients with occlusal plane ranging from 54 cm to 59 cm who needed close follow - up ( range 13 months ) underwent both examinations . 
effective dose and dose to the main organs of the head and neck were higher for msct than for cbct . image quality of cbct was judged to be equivalent to that of msct for visualising teeth and bone but inferior for visualising soft tissues . 
si provveduto alla misurazione della dose alle strutture di capo e collo e della dose efficace con dosimetri a termoluminescenza ( tld ) posti in un fantoccio antropomorfo alderson rando utilizzando un protocollo tcfc ed uno tcmd ottimizzato . 
lo studio delle strutture ossee pu essere effettuato , se la radiografia ortopanoramica non sufficiente , mediante tcfc , che fornisce informazioni sovrapponibili a quelle della tcmd con notevole radiol med ( 2010 ) 115 : 600611 keywords cone - beam computed tomography radiation dose jaw image quality risparmio di dose ; la tcmd indicata qualora sia necessario valutare anche i tessuti molli . parole chiave tomografia computerizzata a fascio conico arcata dentaria dose di radiazione qualit dellimmagine introduction introduzione conventional radiology is often quite adequate for studying the maxillofacial region in that it provides sufficient information to answer clinical questions while exposing the patient to low radiation doses [ 1 ]  . 
in recent years , cone - beam computed tomography ( cbct ) equipment has been developed to minimise radiation exposure , in view of the fact that dental imaging is often performed on children or young adults [ 5 , 6 ]  . 
the aim of this study was to measure radiation dose to the main organs of the head and neck region and the effective dose delivered by 64 - slice msct and by cbct , by means of thermoluminescent dosimeters in an anthropomorphic phanto additionally , we evaluated image quality in a selected sample of patients imaged with the two ct techniques . ( tlds ) placed materials and methods dose absorbed by the organs of the head and neck region and whole - body effective dose were measured using an alderson rando anthropomorphic phantom ( alderson research laboratories , inc . , new york , ny , usa )  . phantom sections 010 ( section thickness 2.5 cm ) were used for the measurements . 
forty tlds ( harshaw , lif tld - 100 , rods , 116 mm3 ) were inserted into slots in correspondence with the main organs ; two tlds were placed in correspondence with the eyelids to measure the dose to the crystalline lens . 
dose delivered to the red bone marrow was estimated by evaluating its distribution throughout the body , as described by the international commission on radiological protection ( icrp ) publication no . 
finally , the effective dose was calculated by considering the organs and their respective weighting la radiologia convenzionale spesso adeguata per lo studio del distretto maxillofaciale , in quanto in grado di fornire , erogando basse dosi , informazioni sufficienti per dare risposta ai quesiti clinici [ 1 ]  . 
peraltro , attualmente la tomografia computerizzata multidetettore ( tcmd ) , garantendo un imaging tridimensionale ed unaccuratezza diagnostica superiore , considerata il gold standard in ambito odontostomatologico [ 24 ]  . 
nella pratica clinica , lutilizzo di questa metodica limitato dai costi , dalla disponibilit delle macchine e da motivi radioprotezionistici ; negli ultimi anni sono state realizzate apparecchiature di tomografia computerizzata a fascio conico ( tcfc ) , allo scopo di contenere quanto pi possibile lesposizione radiante , considerando che spesso i soggetti che si sottopongono a tali indagini sono bambini o giovani adulti [ 5 , 6 ]  . 
lobiettivo di questo studio la misurazione della dose impartita dalla tcmd a 64 strati e dalla tcfc ad alcuni siti anatomici della testa e del collo e della dose efficace mediante dosimetri a termoluminescenza ( tld ) posti in un fantoccio antropomorfo ; stata inoltre valutata , in un campione selezionato di pazienti , la qualit delle immagini ottenute mediante le due tecniche di imaging tc . materiali e metodi la misurazione della dose assorbita dalle diverse strutture anatomiche del capo e del collo e della dose efficace al corpo intero stata effettuata utilizzando un fantoccio antropomorfo alderson rando ( alderson research laboratories , inc , new york , usa )  . 
quaranta dosimetri a termoluminescenza ( harshaw , lif tld - 100 , rods , 116 mm3 ) sono stati inseriti in fori praticati nel fantoccio in corrispondenza dei principali organi ; due tld sono stati posti in corrispondenza delle palpebre per valutare la dose al cristallino . 
la dose agli organi di piccole dimensioni stata stimata direttamente dalla dose ricevuta dal corrispettivo tld ; la dose agli organi di dimensioni maggiori stata valutata come media pesata delle dosi ricevute dai tld corrispondenti [ 7 ]  . 
la dose al midollo emopoietico stata stimata valutando la sua distribuzione nellintero organismo , come 602 radiol med ( 2010 ) 115 : 600611 factors , as suggested by icrp publication no . 
relevant organs in this respect are red bone marrow , thyroid , oesophagus , and brain . during exposure , the phantom was positioned in the manner of a normal patient with the help of medical and technical personnel . 
for the purposes of our study , we considered the most widely used clinical protocol : the 20 - s full - height scan ( voltage 120 kv , tube load 23.87 mas , 306 frames )  . the width of the craniocaudal scan was 13.2 cm , with coverage of anatomical structures located between the frontal sinuses anteriorly and the mandibular margin inferiorly . 
dose measurements alto took into account the initial scout view . the second device was a 64 - slice msct scanner ( aquilion 64 , toshiba , tokyo , japan )  . 
scans extended from the mandibular condyles to include the entire lower jaw , with a total craniocaudal length of approximately 9 c dose measurements also took into account the two scout views of the head ( anteroposterior and laterolateral )  . images were obtained by performing curved multiplanar ( panorex ) and parasagittal oblique reconstructions with both techniques ( cbct and msct ) and were then analysed by two radiologists who classified quality as excellent , good , fair , sufficient and insufficient to select the protocol providing an image quality comparable with that obtained with the i - cat 20 - s full - height scan . 
image size was 2513 cm . subsequently , five patients with a circumference at the occlusal plane within a given range ( 5459 cm ) and requiring close follow - up examinations ( 13 months ) were examined with both ct techniques . 
a tal fine , gli organi rilevanti sono : midollo emopoietico , tiroide , esofago e cervello . durante le esposizioni , il fantoccio stato posizionato in modo quanto pi simile possibile ad un paziente reale , con lausilio di personale medico e tecnico . 
la prima una tcfc per applicazioni dentali i - cat ( xoran technologies , ann arbor , mich . , and imaging science international , hatfield , usa ) con rivelatore al silicio amorfo ( 23 , 8 cm19 , 2 cm ; pixel isotropico di 0 , 4 mm )  . 
il fascio conico collimato in modo da incidere completamente sulla superficie del rivelatore ( larghezza 23 , 8 cm e altezza da 5 cm a 19 , 2 cm )  . 
per lo studio in esame stato considerato il protocollo di pi ampio impiego clinico : full height 20 s ( tensione 120 kv , carico al tubo 23 , 87 ma , 306 frames )  . lampiezza cranio - caudale delle scansioni di 13 , 2 cm , con visualizzazione delle strutture anatomiche comprese tra i seni frontali superiormente e il margine della mandibola inferiormente . 
per la valutazione della dose stato considerato anche il contributo dello scanogramma iniziale . la seconda apparecchiatura una tcmd a 64 strati ( aquilion 64 , toshiba , tokyo , giappone )  . 
per la scelta del protocollo desame sono state effettuate pi scansioni del fantoccio alderson rando , variando corrente e pitch a partire dal protocollo toshiba dentalscan standard [ tensione 120 kv , corrente 400 ma , tempo di rotazione 0 , 5 s , pitch 0 , 641 , collimazione 32 mm ( 0 , 564 mm ) ]  . 
le scansioni si estendono dai condili mandibolari fino a comprendere lintera mandibola , per una lunghezza cranio - caudale pari a circa 9 cper la valutazione della dose stato considerato anche il contributo dei due scanogrammi dellintera testa ( antero - posteriore , ap , e latero - laterale , ll )  . le immagini diagnostiche sono state ottenute effettuando ricostruzioni multiplanari curve ( panorex ) e parasagittali oblique con entrambe le metodiche ( tcfc e tcmd )  . 
le immagini sono poi state sottoposte alla visione di due medici radiologi , che le hanno valutate in base alla scala di giudizio : ottimo buono discreto sufficiente insufficiente , allo scopo di selezionare il protocollo di acquisizione che consente di ottenere immagini di qualit diagnostica paragonabile a quella ottenibile con il protocollo i - cat full height 20 s . 
comparison between cbct and msct images was performed with reference to a subjective 5 - point scale : score 1 : cbct image markedly inferior to the msct score 2 : cbct image slightly inferior to the msct score 3 : cbct image equivalent to the msct image score 4 : cbct image slightly superior to the msct score 5 : cbct image markedly superior to the msct image image image image . results current and pitch values used when selecting the best msct protocol for the comparative dose evaluation and the clinical study are shown in table 1 . 
three variations of the standard toshiba dentalscan protocol were also used , which involve current modulation along the z axis ( standard modulation and low modulation : the numbers in parentheses indicate the minimum current value )  . 
 ( 70 ) 0 , 641 0 , 641 0 , 828 0 , 641 0 , 828 0 , 828 0 , 828 0 , 828 ottima buona buona insufficiente buona discreta sufficiente insufficiente kv , corrente 15 ma , tempo di rotazione 14 , 1 s . 
le dimensioni dellimmagine acquisita sono pari a 25 cm13 cm . successivamente sono stati esaminati con entrambi i sistemi tc 5 pazienti , che presentavano una circonferenza al piano occlusale entro un range prestabilito ( 5459 cm ) e avevano la necessit di effettuare controlli ravvicinati nel tempo ( range 13 mesi )  . 
sono stati analizzati losso spongioso , i denti ( smalto , dentina , cavit pulpare ) e le strutture circostanti ( spazio periodontale , lamina dura ) ; inoltre sono stati valutati i tessuti molli . 
il confronto tra le immagini tcfc e tcmd stato eseguito utilizzando una scala con 5 livelli di giudizio soggettivo : punteggio 1 : limmagine tcfc nettamente inferiore in qualit rispetto allimmagine tcmd . punteggio 2 : limmagine tcfc lievemente inferiore in qualit rispetto allimmagine tcmd . punteggio 3 : limmagine tcfc uguale in qualit rispetto allimmagine tcmd . punteggio 4 : limmagine tcfc lievemente superiore in qualit rispetto allimmagine tcmd . punteggio 5 : limmagine tcfc nettamente superiore in qualit rispetto allimmagine tcmd . risultati i valori della corrente e del pitch utilizzati per le acquisizioni sul fantoccio mediante tcmd finalizzate a definire il protocollo da utilizzare negli studi comparativi dosimetrico e clinico sono mostrati in tabella 1 . 
sono state utilizzate anche tre varianti del protocollo toshiba dentalscan standard che prevedono la modulazione della corrente lungo lasse z ( standard modulation e low modulation : i numeri tra parentesi indicano il minimo valore che pu essere assunto dalla corrente )  . 
la tcmd con protocollo ottimizzato la tecnica che eroga le dosi pi elevate per quanto riguarda sia la dose ai vari organi che la dose efficace al corpo intero ( 0 , 99 msv )  . 
lopt la tecnica che eroga la minore dose efficace ( 0 , 05 msv ) e la minor dose agli organi esaminati , fatta eccezione per le ghiandole salivari . le dosi da tcfc sono sensibilmente inferiori a quelle da tcmd ; rispetto allopt la dose efficace circa due volte superiore ( 0 , 11 msv ) ; le dosi agli organi sono tutte superiori ad eccezione per lesofago ( valore di 0 , 01 mgy ) e le ghiandole salivari ( range compreso tra 1 , 35 e 1 , 78 mgy ) ; la dose pi elevata allopt range compreso tra 2 , 01 e 2 , 57 mgy dovuta al fatto che le ghiandole salivari sono comprese nel fascio primario . i risultati della valutazione clinica comparativa della qualit delle immagini sono riportati in tabella 3 . 
2a - d immagini comparative di pazienti studiati con tcfc e tcmd con protocollo ottimizzato : elemento dentale ( a , b ) , strutture circostanti ( c , d )  . 
le immagini delle componenti dentarie ( smalto , dentina , camera pulpare ) sono sovrapponibili in tcfc ( a ) e in tcmd ( b ) ; le immagini del legamento periodontale e della lamina dura sono sovrapponibili in tcfc ( c ) e tcmd ( d )  . 
3a - d comparative images of patients studied with cbct and msct with optimised protocol : cancellous bone ( a , b ) and soft tissues ( c , d )  . 
3a - d immagini comparative di pazienti studiati con tcfc e tcmd con protocollo ottimizzato : osso spugnoso ( a , b ) e dei tessuti molli ( c , d )  . 
however , opt gives a two - dimensional rendering of three - dimensional anatomical structures and hence may not be adequate for diagnosis in clinical situations that are quella che impartisce la pi bassa dose efficace ; anche i valori di dose agli organi sono modesti [ 1 , 10 , 11 ]  . 
tuttavia lopt , fornendo una rappresentazione bidimensionale di strutture anatomiche tridimensionali , pu non essere sufficiente ai fini diagnostici in talune evenienze cliniche che traggono vantaggio dallimpiego delle tecniche di tc [ 24 ]  . 
le dosi erogate dalle apparecchiature tc , sia spirale che a multiple file di detettori [ 1214 ] , sono pi elevate per quanto concerne sia la dose efficace al corpo intero , sia le dosi ai singoli organi ; in particolare , sono elevate anche le dosi a organi , come gli occhi e in particolare il cristallino , che non giacciono entro il fascio primario 608 radiol med ( 2010 ) 115 : 600611 fig . 
4a - d comparative images of patients studied with cbct and msct with optimised protocol : artefacts due to dental - care materials ( coronal and axial images , a , b ) and dental implants ( crosssectional images , c , d )  . 
4a - d immagini comparative di pazienti studiati con tcfc e tcmd con protocollo ottimizzato : artefatti da indurimento del fascio dovuti a materiale medicamentoso ( immagini coronali e assiali , a , b ) e protesico ( immagini parasagittali , c , d )  . 
spiral or multidetector ct doses [ 1214 ] are higher in terms of whole - body effective dose and organ dose ; in particular , high doses are delivered to the eyes and especially the crystalline lens , neither of which lies within the primary beam and the irradiation of which is due to scattered radiation only . e la cui irradiazione dovuta alla sola radiazione diffusa . 
 uno degli obiettivi di questo studio la misurazione della dose impartita dalla tcmd a 64 strati e dalla tcfc ad alcuni siti anatomici della testa e del collo e della dose efficace mediante tld posti in un fantoccio antropomorfo . dovendo confrontare due apparecchiature diverse fra loro si pu scegliere di lavorare a parit di dose e valutare le radiol med ( 2010 ) 115 : 600611 one of the aims of this study was to measure the dose to organs and tissues of the head and neck region and the effective dose delivered by 64 - slice msct and cbct by using tlds placed in an anthropomorphic phantom . because the comparison involved two different types of equipment , we could choose either to work with identical doses and evaluate differences in image quality or work with identical image quality and evaluate differences in the dose delivered . 
 on the other hand , the effective dose delivered by cbct is higher than that delivered by opt , whereas the dose to the salivary glands , which lie within the primary beam at opt , is lower for cbct [ 12 ]  . 
moreover , compared with opt , the difference between doses to the different organs is less marked with cbct as a result of the larger spatial extension of the cone beam and the large amounts of scattered radiation generated by objects lying within its range . in addition , our study included a comparison of image quality obtained with the two ct techniques , as suggested by previous authors [ 1923 ]  . 
cbct images provided inferior quality regarding visualisation of soft tissues , whereas there was no significant difference regarding bone structures ( vertebral bodies ) and cartilages ( larynx )  . 
in our study , cbct images were judged to be equivalent to msct images for studying teeth , lamina dura , periodontal space differenze in termini di qualit diagnostica delle immagini , oppure lavorare a parit di qualit diagnostica e valutare le differenze in termini di dose ; essendo impossibile ridurre le dosi impartite dallapparecchiatura tc toshiba al livello delle dosi della tc icat , si scelta la seconda possibilit . in letteratura , i protocolli utilizzati al fine di ridurre la dose assorbita sono caratterizzati dalla riduzione della corrente con incremento del pitch [ 15 ] o , meno frequentemente , dalla riduzione della tensione [ 16 ] : anche in questo studio stato scelto un protocollo ottimizzato caratterizzato da riduzione della corrente ( da 400 a 200 ma ) con aumento del pitch ( da 0 , 641 a 0 , 828 ) , che ha permesso una notevole riduzione della dose efficace ( da 2 , 37 a 0 , 99 msv ) senza peraltro una riduzione di qualit delle immagini che potesse comportare una significativa perdita di informazione . le dosi erogate dalla tcfc sono molto inferiori a quelle dei sistemi tcmd , in quanto tali apparecchiature presentano peculiarit tecniche ( rappresentate dalla geometria del fascio conico , dai bassi valori di corrente e dalle propriet del rivelatore ) che giustificano tali risultati ; i nostri dati ( dose efficace 0 , 11 msv ) trovano conferma nelle esperienze riportate in letteratura riguardanti i fantocci antropomorfi [ 1214 , 17 , 18 ]  . 
la dose efficace impartita dal sistema tcfc peraltro pi alta di quella dovuta alla opt ; comunque la dose alle ghiandole salivari , che in opt giacciono entro il fascio primario , risulta inferiore in tcfc [ 12 ]  . 
inoltre , rispetto allopt , nel caso della tcfc la differenza fra le dosi ai vari organi meno marcata , a causa della maggiore estensione spaziale del fascio conico e della elevata percentuale di radiazione diffusa dagli oggetti che si trovano entro esso . il nostro studio ha previsto inoltre un confronto della qualit delle immagini ottenute con i due sistemi tc , come proposto in passato da altri autori [ 1923 ]  . 
 [ 21 ] , prendendo in esame fantoccio antropomorfo , osso mascellare secco e pazienti , hanno ottenuto immagini di qualit superiore mediante tcfc su lamina dura e spazio periodontale e mediante tcmd su gengiva e corticale ossea . 
nel nostro studio limmagine tcfc stata giudicata sovrapponibile allimmagine tcmd nella valutazione dei denti , della lamina dura , dello spazio periodontale e dellosso spongioso ; viceversa la qualit dellimmagine dei tessuti molli risultata inferiore , in quanto la notevole quota di radiazione diffusa che incide in modo casuale sul rivelatore del dispositivo tcfc e la bassa corrente hanno come conseguenza una diminuzione del 610 radiol med ( 2010 ) 115 : 600611 and spongy bone . 
in contrast , visualisation of soft tissues was worse due to the large amount of scattered radiation which hits the cbct detector randomly and the low current produce a lower contrast . 
 [ 23 ] , we found the beam - hardening artefacts ( due the dental - care materials and implants ) to be less disturbing with cbct than with msct [ 24 ]  . conclusions in conclusion , cbct supplies essentially identical information as that of msct regarding teeth , surrounding structures and spongy bone , but it has the advantage of ensuring markedly lower effective and organ doses . 
 [ 23 ] , gli artefatti da indurimento del fascio ( dovuti alla presenza di materiale medicamentoso e protesico ) sono risultati meno disturbanti in tcfc rispetto alla tcmd [ 24 ]  . 
 conclusioni in conclusione , il contenuto informativo delle immagini ottenute con tcfc sostanzialmente sovrapponibile per quanto concerne denti , strutture circostanti e osso spongioso a quello delle immagini fornite dalla tcmd , con il vantaggio di garantire una dose efficace ed ai singoli organi notevolmente inferiore ; inoltre gli artefatti causati dalla presenza di materiale medicamentoso e protesico a livello dentale degradano maggiormente la qualit delle immagini ottenute con tcmd . 
in varie evenienze di patologia odontostomatologica non pertanto necessario il ricorso alla tcmd , che comunque superiore nella valutazione dei tessuti molli . conflict of interest statement the authors declare that they have no conflict of interest to the publication of this article . clinical mri of the abdomen . 
 this 727 pages book , encompassing 12 parts divided into 31 chapters and quite a large index , aims to offer the reader a thorough overview of mri capabilities , focusing on the strengths and limitations in the field of abdominal diagnosis , as indicated in the title . following the first two parts ( one chapter each ) on technical considerations and mri contrast agents use , the text discusses in detail the liver and biliary tract , pancreas , spleen , adrenals , kidneys , gut , pelvis , paediatric abdomen , mri advances in patients with cancer and abdominal mri at 3 tesla . the chapter lay - out opens with a dedicated abstract , followed by the topic presentation and its in - depth discussion , enriched by tables on technical details and highlighted by key - point boxes and ends with a summary and a fairly updated reference list . the book includes a quite useful and unusual addition namely : the closing of each part by one more or more less long chapter which is devoted to the pearls of wisdom and pitfalls related to the treated topics . however , if one is not familiar with the described mri sequence details , peculiarities , tricks , results and related images it will often give the reader an headache , even after just a few text pages . 
i say this since a list of acronyms is lacking , thus i was forced to fill in three a4 pages with abbreviations in two columns with small case handwriting , just to keep abreast with what i was trying to understand and learn from the text and the images . 
 there are indeed plenty of well - reproduced images : however , the author / s who are familiar with them often forget that on the contrary , the reader is not : thus , the use of more arrows etc . 
would have been very beneficial , parla risonanza magnetica ( rm ) a causa dei suoi continui progressi tecnici e conseguenti impieghi in grado di fornire al radiologo ed al clinico sempre migliori informazioni in vari ed affascinanti scenari clinici . questo volume di 727 pagine , nelle sue 12 parti , suddivise in 31 capitoli , corredate da un ampio indice analitico , offre al lettore una precisa carrellata sulle possibilit della rm , mettendone a fuoco i punti di forza e di debolezza nel campo della diagnostica delladdome , come ben indicato dal titolo . dopo le prime due parti ( un capitolo ciascuna ) su considerazioni tecniche ed uso dei mezzi di contrasto , il testo discute in dettaglio fegato e vie bilari , pancreas , milza , ghiandole surrenali , reni , intestino , pelvi , addome pediatrico , progressi della rm nei pazienti oncologici , per terminare con limpiego della rm a 3 tesla in campo addominale . il singolo capitolo impostato su di un estratto puntuale di apertura , seguito dal testo , ben presentato e discusso , arricchito da tabelle con i dettagli tecnici e da caselle che raccolgono i punti chiave , per terminare con un sommario ed un elenco aggiornato di voci bibliografiche . il volume presenta poi una particolarit , utile e non di frequente riscontro : al termine di ogni parte si trova un capitolo , pi o meno lungo , dedicato alle perle ed ai trabocchetti rilevabili negli argomenti in essa trattati . 
 tuttavia , se chi legge non ha famigliarit con i dettagli , le caratteristiche , i trucchi , i risultati e le immagini delle sequenze rm descritte , ci gli provocher un bel mal di testa , anche solo dopo la lettura di poche pagine . 
dico questo perch il volume non corredato da una lista degli acronimi e perch personalmente sono stato costretto a riempire tre pagine , formato a4 in doppia colonna e scrittura minuta per riuscire a tenermi aggiornato su cosa cercavo di capire ed imparare dal testo e dalle immagini . 
 vi una gran quantit di immagini ben riprodotte : tuttavia gli autori che le conoscono e hanno gran famigliari t nella loro lettura si dimenticano che il lettore spesso non al loro livello : cos un maggior uso di frecce ecc . 
 sarebbe stato pi che giovevole , particolarmente in alcu radiol med ( 2012 ) 117 : 896897 ticularly in some of the chapters related to the liver and adrenals . it is unusual that no reference is made to the stomach . 
i would also point out that most of the images of the fistulain - ano chapter are the same as those published on this topic in the mri of the gastrointestinal tract a book edited by j . 
 stoker in 2010 [ 1 ] , which should be kept on hand for comparison and discussion with the present book for the thirsty reader who will take full advantage of them both . under the supervision of prof . 
gourtsoyiannis , the authors , the majority from european centres ( this is really the european radiology mri abdominal book ) , all well - known authorities in their field ( among them , to be remembered for their fine and clear contributions , are italian radiologists ) have provided a truly state - of - the art text . 
 this book presents and discusses in depth the why , how and when in abdominal mri : a book that will be appreciated by radiologists ( working in the field and mastering it or at least willing to approach it ) and clinicians who will benefit in their daily research and work from the diagnostic opportunities offered by mri of the abdomen . 
those clinicians who will ultimately provide benefit for their patients . ni dei capitoli dedicati al fegato ed alle surrenali . strano che nel volume non venga fatto alcun riferimento allo stomaco . 
vorrei anche far notare che la maggior parte delle immagini del capitolo sulle fistole ano - rettali siano le stesse di quelle pubblicate sullo stesso argomento nel volume mri of the gastrointestinal tract pubblicato nel 2010 a cura di j . 
stoker [ 1 ] , volume che dovrebbe essere a disposizione , per confronto e discussione con quello ora in recensione , del lettore assetato che trarr beneficio da entrambi . sotto la supervisione del prof . 
gourtsoyiannis , gli autori , per la maggior parte operanti in centri europei ( in effetti questo il volume della radiologia europea sulla rm delladdome ) e ben rispettate figure nel loro campo ( tra di loro radiologi italiani , da ricordare per i loro contributi eleganti e precisi ) hanno fornito un testo veramente davanguardia . questo volume presenta e discute infatti in profondit il perch , il come ed il quando dello studio per immagini della rm delladdome : volume che sar apprezzato dai radiologi ( sia che prestino la loro attivit in questo campo , avendone piena competenza , sia per coloro che invece desiderino iniziarne la conoscenza ) e dai clinici che troveranno vantaggio nella loro ricerca e nel lavoro giornaliero da parte delle opportunit offerte dalla rm delladdome : clinici che cos beneficeranno i loro pazienti . radiol med ( 2012 ) 117 : 855864 doi 10.1007 / s11547 - 011 - 0767 - 5 neuroradiology neuroradiologia prevalence study of chronic cerebrospinal venous insufficiency in patients with multiple sclerosis : preliminary data studio di prevalenza della insufficienza venosa cerebrospinale cronica nei pazienti affetti da sclerosi multipla : dati preliminari r . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , roma , italy 2dipartimento di neuroscienze , fondazione policlinico di tor vergata , roma , italy correspondence to : c . 
del giudice , viale oxford 81 , 00133 roma , italy , tel . : + 39 - 06 - 20902400 , fax + 39 - 06 - 20902404 , e - mail : costantino.delgiudice@yahoo.it received : 2 january 2011 / accepted : 25 may 2011 / published online : 7 january 2012 springer - verlag 2012 abstract purpose . 
in our experience , a slight difference exists in the prevalence of ccsvi between ms and healthy controls , but it is not as yet clear which parameters may be most significant . 
it did , however , reveal a tendency that requires a larger number of patients to achieve statistically significant results . keywords multiple sclerosis venous insufficiency colour - doppler ultrasonography riassunto obiettivo . 
da novembre 2009 a febbraio 2010 , 74 soggetti ( 40 affetti da sm e 34 casi controllo ) sono stati arruolati in uno studio prospettico randomizzato a singolo cieco . 
esiste una lieve differenza di prevalenza di ccsvi tra i soggetti affetti da sm e quelli sani nella nostra valutazione , ma ad oggi non sono stati individuati quali tra i numerosi parametri siano i pi significativi . 
 parole chiave sclerosi multipla insufficienza venosa eco - color doppler 856 introduction multiple sclerosis ( ms ) is a degenerative , inflammatory and demyelinating disease of the central nervous syste the aetiopathogenesis is still unknown [ 1 ]  . 
 [ 4 ] described an abnormality of blood flow in which , owing to malformations causing narrowing of the main veins draining the brain and spinal cord , the venous system loses the ability to effectively drain blood to the heart . 
this observation attracted considerable interest within the scientific community , particularly after the same group investigating percutaneous transluminal angioplasty ( pta ) in ccsvi that demonstrated an improvement in symptoms in ms patients [ 5 ]  . 
the results were conflicting , but the studies had significant methodological differences that may have influenced their findings [ 6 ]  . we conducted this preliminary single - blind prospective study to investigate the existence of a correlation between ccsvi and ms . 
 [ 4 ] was applied to a cohort of patients affected by ms and to a group of healthy controls studied with colour - doppler ultrasound ( cdus )  . materials and methods study population from november 2009 to february 2010 , 74 participants enrolled in this prospective study at tor vergata university hospital , rome : 40 patients with ms , and 34 ageand sexmatched healthy controls . 
patients with a history of cerebral venous thrombosis , jugular vein thrombosis , deep vein thrombosis , central venous catheters , head and neck surgery , transient global amnesia , vasculitis , cerebrovascular malformations or congenital vascular malformations were excluded , as were those who had suffered disease relapse in the previous 30 days . 
le placche demielinizzanti , descritte per la prima volta da charcot , sono la lesione istologica caratteristica [ 2 ] , coinvolgente sia la sostanza bianca che la sostanza grigia cerebrale . 
tali evidenze suggeriscono che lassociazione topografica fra le lesioni focali demielinizzanti ed il sistema venoso insorga dalla distruzione del barriera ematoencefalica da parte di una risposta immune alla base della malattia . 
 [ 4 ] ha descritto unanomalia del flusso di sangue in cui il sistema venoso a causa di malformazioni che determinano un restringimento delle principali vene che drenano il sangue dal cervello e midollo spinale , non sarebbe in grado di drenare efficacemente il sangue verso il cuore , definita linsufficienza venosa cerebrovascolare cronica ( ccsvi )  . 
tale osservazione ha suscitato un grosso interesse da parte della comunit scientifica , soprattutto perch un successivo studio dello stesso gruppo , effettuato mediante il trattamento con angioplastica percutanea ( pta ) della ccsvi , dimostrava un miglioramento dei sintomi dei pazienti affetti da sm [ 5 ]  . 
 successivamente altri gruppi hanno effettuato degli studi diagnostici al fine di valutare la correlazione fra queste due patologie , confermando o meno i risultati ottenuti dal gruppo di zamboni [ 4 ]  . 
tuttavia tali studi presentano differenze metodologiche significative che potrebbero influire sulla diversit dei risultati ottenuti [ 6 ]  . il presente studio preliminare prospettico a singolo cieco ha lo scopo di investigare lesistenza di una correlazione fra ccsvi e sm . 
 [ 4 ] , stata applicata ad una coorte di pazienti affetti da sm e a controlli sani . materiali e metodi popolazione di studio da novembre 2009 a febbraio 2010 , 74 pazienti sono stati arruolati in questo studio prospettico presso il policlinico di tor vergata : 40 pazienti affetti da sm e 34 soggetti sani di sesso ed et comparabili . 
il gruppo di pazienti con sm presentavano una malattia remittente - recidivante ( 73% ) , secondariamente progressiva ( 13 , 5% ) o primariamente radiol med ( 2012 ) 117 : 855864 proved by the local ethics committee , and informed consent was obtained from all participants enrolled . cdus evaluation all participants were studied with extracranial cdus of the neck veins and transcranial cdus to assess flow at the level of the internal cerebral vein , vein of rosenthal and vein of galen to establish a diagnosis of ccsvi . 
no increase in the diameter of the internal jugular vein when changing from an upright to a supine position ( lack of - )  . progressiva ( 13 , 5% )  . 
pazienti con una storia di trombosi venosa cerebrale , trombosi delle vene giugulari , trombosi venosa profonda , cateteri venosi centrali , chirurgia della testa e del collo , amnesia transitoria globale , vasculiti , malformazioni cerebrovascolari e malformazioni vascolari congenite sono stati esclusi . 
lo studio stato approvato dal comitato etico del policlinico universitario di tor vergata , roma , ed un consenso informato stato ottenuto da tutti i soggetti arruolati nello studio . valutazione eco - color doppler tutti i soggetti arruolati sono stati sottoposti ad uno studio eco - color doppler extracranico dei vasi venosi del collo e transcranico per la valutazione del flusso a livello della vena cerebrale interna , della vena di rosenthal e della vena di galeno al fine di porre diagnosi di ccsvi . 
mancato incremento del diametro della vena giugulare interna nel passaggio dalla posizione di orto alla posizione di clinostasi ( assenza di - )  . tutti gli esami sono stati effettuati da due operatori . 
1 vena vertebrale sinistra valutata in ortostasi con evidente presenza di circolo rachidiano con flusso invertito . lesordio di malattia stato definito come primo episodio di disfunzione focale neurologica indicativo di sm . 
al momento della diagnosi di sm remittente - recidivante tutti i pazienti hanno iniziato una terapia modificata [ ogni giorno glatiramer acetato o da 1a 44 g sottocutaneo ( s.c. ) di interferone beta tre volte a settimana o interferone beta 1b , 250 mg ogni giorno ]  . 
ledss , valutato lo stesso giorno dellesame eco - color doppler , stato utilizzato in combinazione con la durata della malattia per calcolare due misure di severit della malattia : lindice di progressione ( pi ) e multiple sclerosis severity score ( msss )  . 
5a , b movimento anomalo di una valvola venosa a livello giugulare interna destro visualizzata allesame eco - color doppler alla valutazione b - mode in un paziente affetto da ccsvi . nosis , all patients were started on a disease - modifying treatment ( glatiramer acetate daily or 44 mcg interferon - beta 1a subcutaneously three times / week or 250 mg interferon - beta 1b daily )  . 
mitoxantrone ( 12 mg / m2 intravenously every 3 months with a cumulative lifetime dose of 140 mg / m2 ) and natalizumab ( 300 mg intravenously every 4 weeks ) were considered second - line treatments for patients who had exeseguita mediante test t di student per campioni parametrici o mediante test di mann - whitney per quelli non parametrici . 
il test di fisher a due code stato eseguito per la comparazione dei criteri ccsvi in pazienti malati e casi controllo e per valutare la proporzione fra pazienti ccsvi positivi e la presenza di altre variabili cliniche . 
un valore di p < 0 , 05 stato considerato significativo . 860 radiol med ( 2012 ) 117 : 855864 perienced at least two relapses during 1 year of treatment , with other approved immunomodulators . 
 the edss rating , assessed on the same day as the cdus examination , was combined with disease duration to calculate two measures of disease severity : the progression index ( pi ) and the ms severity score ( msss )  . 
the two - tailed fisher test was used to compare ccsvi criteria in patients and controls and to evaluate the proportion of ccsvi - positive patients and the presence of other clinical variables . 
the proportion of participants affected by ccsvi was , indeed , higher in the ms group , but the difference did not reach statistical significance [ 22 ccsvi - positive patients in the ms group ( 55% ) versus 12 ccsvi - positive individuals in the control group ; p = 0.09 ; fig 6 ]  . 
table 2 shows the ccsvi criteria detected at transcranial and extracranial cdus . discussion this study aimed to clarify the existence of a correlation between ccsvi , as described by zamboni et al . 
inoltre la proporzione di soggetti completamente negativi ( gruppo sm : 12 pazienti ; gruppo controllo : 14 pazienti ccsvi positivi ; p = 0 , 3 ) non era differente fra i due gruppi . 
la tabella 2 riporta i criteri di ccsvi rilevati allesame eco - color doppler transcranico ed extracranico . discussione il presente studio stato eseguito allo scopo di chiarire lesistenza di una relazione fra la ccsvi , come stata descritta da zamboni et al . 
in 55% dei pazienti con sclerosi multipla stato possibile porre diagnosi di ccsvi , mentre 35% dei pazienti nella coorte di controllo hanno presentato anomalie venose cerebrali croniche , con una differenza non significativa . 
lo stesso gruppo ha successivamente confermato tali risultati con uno studio pilota [ 5 ] che ha analizzato lefficacia del trattamento endovascolare mediante pta di stenosi / malformazioni a carico delle vene giugulari interne e della vena azygos in 65 soggetti affetti da ccsvi , dei quali 35 affetti da sm remittente - recidivante ( rr ) , 20 da sm secondariamente progressiva ( sp ) e 10 da sm primariamente progressiva ( pp )  . 
in questi pazienti stato dimostrato un significativo miglioramento in termini di pressione emodinamica venosa , outcome clinico , carico lesionale e nuove lesioni che prendono contrasto dopo somministrazione di mezzo di contrasto ( mdc ) in risonanza magnetica ( rm ) , in un follow - up esteso a 18 mesi , a fronte tuttavia di un non trascurabile tasso di re - stenosi del 47% . un successivo studio eseguito da zamboni in collaborazione con zivadinov et al . 
 [ 7 ] , ha fornito dei dati sulla radiol med ( 2012 ) 117 : 855864 table 1 demographic characteristics of the population studied variables ms group ( n = 40 ) control group ( n = 34 ) tabella 1 caratteristiche demografiche della popolazione di studio variabili gruppo sm ( n = 40 ) gruppo c ( n = 34 ) age ( years ) male gender , n ( % ) type of multiple sclerosis , n ( % ) remittingrelapsing secondary progressive primary progressive ms , multiple sclerosis ; ns , not significant et ( anni ) sesso maschile , n ( % ) tipo di sclerosi multipla , n ( % ) recidivante remittente secondariamente progressiva primariamente progressiva sm , sclerosi multipla ; c , controllo ; ns , non significativo 40.510.7 13 ( 33 ) 29 ( 73 ) 5 ( 13.5 ) 5 ( 13.5 ) 40 , 510 , 7 13 ( 33 ) 29 ( 73 ) 5 ( 13 , 5 ) 5 ( 13 , 5 ) 41.310.2 11 ( 32 ) 41 , 310 , 2 11 ( 32 ) venous abnormalities in ms pathogenesis . 
these findings are at variance with those of zamboni et al . , who reported a close correlation between these two conditions , with a sensitivity and specificity of 100% [ 4 ]  . 
the same research group subsequently confirmed their initial results in a pilot study [ 5 ] investigating the effectiveness of pta for stenosis / malformations of the internal jugular and azygos vein in 65 individuals affected by ccsvi , 35 of whom had rr , 20 sp and ten pp disease . 
over an 18 - month follow - up , patients achieved a significant improvement in venous pressure , clinical outcome , lesion burden and new enhancing lesions on contrastenhanced magnetic resonance imaging ( mri ) , even though prevalenza della ccsvi nella sm valutata mediante studio con eco - color doppler . 
i risultati forniti confermano una incrementata prevalenza nel pazienti di sm , ma con valori sensibilmente pi bassi rispetto a quelli forniti nel primo studio , con una sensibilit del 62 , 5% , specificit del 74 , 5% , con valori predittivi positivi del 81 , 4% ma soprattutto valori predittivi negativi del 52 , 7% , riportando una percentuale di prevalenza del 25 , 5% nei soggetti sanicontrollo , e del 42 , 3% nei soggetti affetti da altre patologie neurologiche . successivamente altri gruppi hanno effettuato degli studi analoghi ottenendo risultati molto differenti . 
furthermore , there was no difference in venous blood volume in the internal jugular and vertebral veins between the supine and upright position , and the decrease in blood volume on turning to the upright position was less pronounced in ms patients . 
 inoltre non vi erano differenze nel volume ematico venoso nelle vene giugulari interne e nelle vertebrali tra la posizione in clino - / ortostatismo , e vi era un minor decremento del volume ematico al ritorno nella posizione di ortostasi nei soggetti affetti da sm rispetto a quelli di controllo , concludendo quindi che nessun soggetto esaminato aveva > 1 parametro zamboni per ccsvi . 
il nostro studio presenta il vantaggio di aver seguito un protocollo di studio identico a quello utilizzato dal gruppo di zamboni e di essere stato eseguito da radiologi esperti in esami eco - color doppler . 
 [ 6 ] , neck veins do not have a tubular anatomy but are structures with a varying diameter , with a dilated proximal and distal portion and a narrowed central portion corresponding to the valves . 
this structure changes in relation to breathing and the patients position , showing extreme variability that cannot be described using the cross - sectional area only [ 8 ]  . 
all this leads to an assessment that is not always reproducible and findings that are difficult to assign to definite classes of disease and / or normality . we experienced difficulties in evaluating changes in diameter ( ) when passing from the upright to supine position , as it is not easy to take the measurements in exactly the same place in the two positions . 
however , it should be mentioned that the presence of a septum is almost invariably associated with reflux , and therefore , its presence would in itself be significant for ccsvi ( two criteria )  . 
additionally , in zamboni et al.s original study [ 4 ] , the proposed acoustic window in the transcranial doppler evaluation ( subcondylar ) is completely different from the window normally used in neurological us ( infratemporal )  . 
however , we believe the problem to be more complex in that the evaluation of ccsvi should be considered as a nonvalvular , multicompartmental , closed system , the equilibrium and flow of which are dependent on numerous parameters ( pressure , respiration , heart rate ) that may in various ways influence its alterations . doppler findings cannot be interpreted as percentages of stenosis but only as reflecting a flow obstruction that is re , ma sono strutture che presentano un diametro variabile , con una porzione prossimale e distale di diametro maggiore ed una porzione centrale in corrispondenza delle strutture valvolari in cui il calibro della vena si riduce . 
tutto ci determina una valutazione non sempre riproducibile e difficilmente inquadrabile allinterno di classi definite di patologia e / o normalit . nella nostra esperienza abbiamo avuto difficolt nella valutazione della variazione di diametro ( ) nel passaggio dalla posizione ortoalla clinostatica , in quanto non sempre facile effettuare la misurazione esattamente nello stesso punto nelle due posizioni . 
 nello studio del reflusso ci siamo trovati spesso davanti a setti ipomobili che presentavano caratteristiche emodinamiche tali da determinare alterazioni di flusso a suddetto livello con evidenza alla valutazione di una inversione dello stesso nei tempi > 0 , 8 secondi . 
tuttavia , si dovrebbe dire che quasi sempre la presenza di un setto associata ad un reflusso e che quindi sarebbe di per s gi correlata alla presenza di ccsvi ( 2 criteri )  . 
ci nonostante questi setti sono stati rilevati sia nei soggetti affetti da sm che nei casi controllo e non hanno pertanto inficiato il risultato del lavoro . restano inoltre dubbi sulla adeguatezza della valutazione eco - color doppler transcranica venosa , in cui la corretta visualizzazione del pattern venoso risulta di non facile valutazione . 
va inoltre considerato che nello studio originale di zamboni , la finestra acustica proposta nella valutazione del doppler transcranico ( sub - condilare ) risulta del tutto differente da quella normalmente utilizzata in neuro - sonologia ( infra - temporale )  . 
riteniamo tuttavia che il problema sia pi complesso in quanto la valutazione della ccsvi deve essere considerata come un sistema chiuso pluricompartimentale avalvolare il cui equilibrio e flusso si basano su molti parametri ( pressione , respiro , frequenza cardiaca ) che possono in vario modo influire sulle modificazioni dello stesso . il risultato del doppler non pu essere catalogato allinterno di percentuali di stenosi , ma solo nella considerazioni di un ostacolo al flusso di tipo cronico e pertanto caratterizzato da un processo che non si manifesta nellarco di giorni , ma di 2030 anni . 
trovare il modo per individuarlo non facile . 864 radiol med ( 2012 ) 117 : 855864 chronic and therefore characterised by a process that does not manifest within days but over 2030 years . 
finding a way to identify it is not easy . conclusioni conclusions it appears reasonable to investigate the prevalence of ccsvi in ms on a larger population sample while trying to adapt the cdus study to make it more reproducible and correlating data with phlebography . 
once a significant prevalence of ccsvi amongst ms patients has been demonstrated on a large scale , and after having performed complementary correlation studies with mri , the next step could be to start randomised controlled trials on the efficacy of pta treatment . sicuramente concludendo appare ragionevole eseguire uno studio su campione pi ampio di popolazione al fine di valutare la prevalenza della ccsvi nella sm , per ottenere dei dati su un grosso campione di soggetti , cercando anche in corso di opera di adattare lo studio eco - color doppler affinch sia pi facilmente riproducibile e correlare i dati con quelli della flebografia . 
inoltre potrebbe essere presa in considerazione la possibilit di correlare i dati ottenuti all eco - color doppler con la risonanza magnetica , non tanto in termini di correlazione morfologica delle alterazioni riscontrate , quanto nella valutazione di alcuni parametri funzionali , di emodinamica cerebrale attraverso studi di perfusione rm . 
lanzara , sezione di radiodiagnostica , seconda universit degli studi di napoli , p.zza miraglia 2 , 80138 napoli , italy 2dipartimento di scienze della salute , universit degli studi del molise , campobasso , italy correspondence to : y . 
a retrospective study was performed of 85 patients , 33 men and 52 women , previously examined with 3d anal ultrasound ( us ) for clinically suspected anorectal disease but found to be negative . 
the examinations were performed with a bruel and kjaer us system with a 2050 transducer , scanning from the anorectal junction to the subcutaneous portion of the external anal sphincter ( eas )  . 
a good knowledge of anal - canal anatomy is essential to detect sphincter abnormalities when assessing pelvic floor dysfunction . keywords 3d anal endosonography anal sphincter anal canal anatomy riassunto obiettivo . 
in uno studio retrospettivo sono stati selezionati 85 soggetti , di cui 33 maschi e 52 femmine , sottoposti precedentemente ad us endoanale 3d per sospetto clinico di patologia dellano - retto distale ma risultati essere tutti negativi allesame ultrasonografico . 
 gli esami sono stati eseguiti con apparecchio dedicato bruel e kjaer , con trasduttore tipo 2050 e scansioni dalla giunzione ano - rettale alla porzione pi superficiale dello sfintere anale esterno ( sae )  . 
nellimmediato postprocessing sono stati stimati la lunghezza degli sfinteri nei piani anteriore e posteriore e lo spessore anteriore , laterale e posteriore dello sfintere anale interno ( sai ) e del sae . 
la distribuzione della muscolatura del canale anale risulta asimmetrica in entrambi i sessi : la lunghezza di sai e sae significativamente pi breve nelle donne , specie lungo il piano longitudinale mediano anteriore ( p = 0 , 005 e p < 0 , 001 , rispettivamente )  . 
inoltre , lo spessore di entrambi gli sfinteri presenta una tendenza allaccrescimento proporzionale allet del paziente , soprattutto nella porzione laterale per il sai ( r2 = 0 , 37 , p < 0 , 001 ) e posteriore per il sae ( r2 = 0 , 29 , p = 0 , 01 )  . 
la conoscenza precisa delle componenti anatomiche muscolo - legamentose del canale anale alla 760 radiol med ( 2012 ) 117 : 759771 base della identificazione delle alterazioni sfinteriali utili alla comprensione dei disturbi del pavimento pelvico . parole chiave ultrasonografia endoanale 3d sfintere anale anatomia del canale anale introduction introduzione the anal canal is an anatomical region that is easy to explore clinically but difficult to evaluate with diagnostic imaging techniques . 
marks hospital in london , and especially application of the more recent 3d reconstruction software , has enabled accurate morphological visualisation of the anal canal with an examination that is easy to perform , well tolerated by patients and readily repeatable [ 911 ]  . 
on 2d images , the different echogenicity and numerous interfaces of the structures forming the anal canal account for faithful anatomical depiction of the region and the ability to recognise the single muscular layers composing it [ 25 , 1217 ]  . 
data acquired from a series of parallel 2d images are combined to obtain a cube - shaped volume that can be freely rotated and analysed from all angles to gain as much information as possible without time constraints , as this single - volume acquisition can be re - examined at any time . 
 immediately after acquiring the volume , it is possible to obtain coronal anteroposterior ( ap ) or posteroanterior ( pa ) and sagittal right - to - left or left - to - right multiplanar reconstructions ( mpr ) and to measure distances , areas and angles [ 1619 ]  . 
 there is quite a large body of data on the depiction of sphincter anatomy with 2d us [ 28 ] , which allows measurement of the thickness but not the length of the anal - canal muscles . 
between 1999 and 2008 , six research groups described the use of the 3d technique for estimating variability in depicting the anal musculature [ 10 , 11 , 2023 ]  . 
however , to date , it has not been possible to establish normal ranges within the populations studied owing to heterogeneity of the samples and methodological approaches and the small amount of data available . 
 the aim of our work was to provide a broader estimation , using 3d anal eus , of both the thickness and length of the ias and eas in the different planes and to identify possible paraphysiological findings related to gender and age . il canale anale rappresenta una regione anatomica di agevole esplorazione clinica , ma difficilmente valutabile con le metodiche di diagnostica per immagini . 
mark hospital di londra , e soprattutto lapplicazione del software di ricostruzione 3d , maggiormente diffuso nellultimo decennio , ne ha consentito la corretta rappresentazione morfologica attraverso un esame di facile esecuzione , ben tollerato dal paziente ed agevolmente ripetibile [ 911 ]  . 
nelle immagini bidimensionali la differente ecogenicit delle strutture che formano il canale anale e le numerose interfacce presenti sono alla base della fedele rappresentazione anatomica di questa regione , nonch del riconoscimento dei singoli strati muscolari che la costituiscono [ 25 , 1217 ]  . 
i dati acquisiti da una serie di immagini parallele in 2d sono combinati per ottenere un volume rappresentato sotto forma di un parallelepipedo , liberamente ruotabile ed analizzabile nei diversi piani dello spazio , in modo da ottenere il maggior numero di informazioni possibile , indipendentemente dal tempo desecuzione dellesame , poich questunica acquisizione volumetrica pu essere riesaminata in ogni momento . 
dopo lacquisizione del volume immediatamente possibile ottenere ricostruzioni multiplanari coronali , in senso antero - posteriore ( ap ) e viceversa ( pa ) , e sagittali , in direzione destra - sinistra e viceversa , oltre ad effettuare misurazioni di distanza , area ed angolazioni [ 1619 ]  . esiste una discreta documentazione bibliografica sulla descrizione anatomica sfinteriale con us 2d [ 28 ] che consente di misurare lo spessore , ma non la lunghezza delle strutture muscolari del canale anale . 
sei gruppi di autori , dal 1999 al 2008 , hanno descritto la tecnica 3d per la stima della variabilit nella rappresentazione della muscolatura sfinteriale [ 10 , 11 , 2023 ]  . 
tuttavia non stato ancora possibile fissare valori di normalit nellambito delle popolazioni esaminate sia per la eterogeneit di radiol med ( 2012 ) 117 : 759771 materials and methods we selected 85 patients ( 33 men and 52 women ; age range 1877 years ; mean age 47.5 years ) who had previously undergone 3d anal eus for a clinical suspicion of distal anorectal disease but who were all found to be negative on sonographic examination . 
 the examination was performed with a bruel and kjaer profocus system ultra view - 2202 with a model 2050 transducer equipped with a double multifrequency crystal ( range 616 mhz ) , with 360 mechanical rotation at a speed of 1.92.8 rotations / s , focus range up to 45 mm , dimensions 5502704017 mm , automatic extraction and field depth up to 10 c all patients were examined in the lateral decubitus position without any prior bowel preparation . 
the transducer was covered with a condom and , after adequate lubrication , placed inside the anal canal and first advanced as far as the rectal ampulla before continuing with more caudal scans ; it was then automatically withdrawn to the superficial perianal plane . 
the images were visualised in planes perpendicular to the transducer , which was kept with the same orientation so that the anterior wall was always visualised at the 12 oclock position , the left wall at 3 oclock , the posterior wall at 6 oclock and the right wall at 9 oclock . 
thickness was determined for both 2d images in the anterior ( 12 oclock ) , posterior ( 6 oclock ) and lateral ( 3 and 9 oclock ) regions , and mean values were calculated . 
longitudinal measurements of the eas were obtained in a median sagittal plane and ranged from : anteriorcampione e / o di approccio metodologico che per la esiguit dei dati disponibili . il nostro contributo si propone di fornire una pi ampia stima , con tecnica us 3d , sia dello spessore che della lunghezza degli sfinteri anali interno ( sai ) ed esterno ( sae ) nei diversi piani dello spazio e di identificare eventuali reperti parafisiologici in correlazione a sesso ed et . materiali e metodi sono stati selezionati 85 soggetti , di cui 33 di sesso maschile e 52 di sesso femminile , con et compresa tra 18 e 77 anni ( et media 47 , 5 anni ) , sottoposti precedentemente ad us endoanale 3d per sospetto clinico di patologia dellanoretto distale , ma risultati essere tutti negativi allesame ultrasonografico . 
i pazienti di sesso maschile avevano et compresa tra 21 e 47 anni ( et media 34 anni ) e quelli di sesso femminile tra 18 e 77 ( et media 47 , 5 anni )  . 
gli esami strumentali sono stati condotti in accordo con gli standard etici espressi nella dichiarazione di helsinki del 1964 . lesame ecografico stato eseguito con apparecchio bruel e kjaer profocus ultra view - 2202 con trasduttore tipo 2050 , dotato di doppio cristallo multifrequenza ( range 616 mhz ) , movimento meccanico circolare a 360 della velocit di 1 , 92 , 8 giri / secondo , focus range fino a 45 mm , dimensioni di 5502704017 mm , estrazione automatica e profondit di campo fino a 10 cm . tutti i soggetti sono stati esaminati in decubito laterale senza necessit di alcuna preparazione preventiva . 
al di sopra del trasduttore stato posto un condom e , dopo lubrificazione di questultimo , la sonda stata posizionata allinterno del canale anale , introdotta dapprima fino allampolla rettale per poi proseguire nelle scansioni pi caudali , ritirando automaticamente la sonda fino al piano perianale superficiale . 
le immagini sono state visualizzate su piani perpendicolari al trasduttore orientando la sonda sempre allo stesso modo , cos che la parete anteriore fosse rappresentata alle ore 12 , quella sinistra alle ore 3 , la posteriore alle ore 6 e quella laterale destra alle ore 9 . 
3 piano di scansione superficiale : maggiormente rappresentata la porzione pi superficiale del sae . ly , the proximal extremity of the muscular fascia at the point where they form a complete ring , up to the distal subcutaneous portion , and posteriorly , from the puborectalis sling to the distal subcutaneous portion ; the ias was also measured both anteriorly and posteriorly in a median sagittal plane , fig . 
lo spessore era calcolato , per entrambi nelle immagini 2d , nelle regioni anteriore ( ore 12 ) , posteriore ( ore 6 ) e laterale ( alle ore 3 e 9 ) , di cui sono stati ricavati i valori corrispondenti in media . 
le misurazioni longitudinali del sae sono state ottenute in un piano sagittale mediano e comprese , anteriormente , tra lestremit prossimale dei fasci muscolari dove formano un anello completo fino alla porzione distale sottocutanea ; posteriormente a partire dalla fionda puborettale fino alla porzione distale sottocutanea ; il sai stato misurato , anchesso in un piano sagittale mediano , sia anteriormente che posteriormente , laddove si osservano i fasci muscolari ipoecogeni , da un livello di scansione basso ad un livello medio - alto fino alla sua estensione prossimale . 
 obiettivo del lavoro di stabilire attraverso lus endoanale 3d i range di misurazione nella norma delle strutture muscolari sfinteriali del canale anale , analizzandone le variazioni in base allet e al sesso . radiol med ( 2012 ) 117 : 759771 where the hypoechoic muscular fascia are visualised , from a low to a mediumhigh scan level up to its proximal extension . 
the length of the anal canal was identified with the extension of the eas along the posterior longitudinal plane . the aim of our study was to establish , through the use of 3d anal eus , the range of normal measurements of the anal canal sphincter muscles and analyse their variations in relation to age and gender . 
statistical significance was set at p < 0.05. results anatomical measurements on 3d anal eus three - dimensional anal eus allowed optimal depiction of anal - canal anatomy in all spatial planes in all patients . 
the different echogenicity of the tissues , associated with the presence of numerous interfaces between the various wall layers , allowed easy distinction between the submucosal layer , muscular structures and tendons and ligaments , even on 2d images , and thus allowed easy measurement of thickness , whereas immediate 3d analysis allowed longitudinal extension to be measured . 
la lunghezza di sai e sae lungo il margine anteriore e posteriore stata inoltre confrontata tra i due sessi mediante lunpaired students t test e il mann - whitney u test . 
 la significativit statistica stata considerata per valori di p < 0 , 05 . risultati misurazioni anatomiche us endoanale - 3d in tutti i soggetti lus endoanale 3d ha consentito la rappresentazione ottimale dellanatomia del canale anale nei diversi piani dello spazio . 
la differente ecogenicit dei tessuti costituenti , associata alla presenza di numerose interfacce tra i vari strati parietali , ha permesso , gi nelle immagini 2d , di distinguere agevolmente lo strato sottomucoso dalle strutture muscolari e da quelle tendineo - legamentose , ricavandone la misura dello spessore , mentre lanalisi immediata in 3d ha consentito di esaminarne lestensione in longitudinale . 
i risultati sono riportati nelle tabelle 1 e 2 . nellambito della popolazione esaminata sono state incluse sia donne nullipare che pluripare e tra di esse non stata riscontrata alcuna differenza significativa . 
la lunghezza degli sfinteri anali , interno ed esterno , risulta pi breve nelle donne , specie nel piano longitudinale anteriore , rispetto a quella misurata nei soggetti di sesso maschile . 
la lunghezza del sai misurata lungo il suo piano longitudinale mediano anteriore era rispettivamente di 2 , 4 cm in media ( range 1 , 4 2 , 8 cm ) nei soggetti di sesso femminile rispetto ai 2 , 62 cm ( range 1 , 83 , 4 cm ) per quelli di sesso maschile ( p = 0 , 005 )  . 
a differenza del sai , le tre porzioni analizzate , anteriore ( r2 = 0 , 27 , p = 0 , 02 ) , laterale ( r2 = 0 , 23 , p = 0 , 05 ) e posteriore ( r2 = 0 , 29 , p = 0 , 01 ) , mostravano un significativo ispessimento con lavanzare dellet del soggetto . in letteratura , nellultimo decennio , apparso un numero discreto di pubblicazioni scientifiche sullimpiego dellus endoanale , sia 2d [ 17 ] che 3d [ 10 , 11 , 2125 ] , per lo studio anatomico del canale anale , da cui tuttavia emersa una eterogeneit di approccio metodologico , che non consente di poter confrontare i dati forniti dai diversi gruppi , n di determinare valori di normalit nella stima delle componenti muscolari del canale anale . 
dalle pi recenti pubblicazioni scientifiche risultata una maggiore accuratezza della tecnica 3d per la rappresentazione anatomica normale del canale anale [ 14 , 17 , 23 , 2630 ]  . 
in particolare un gruppo di autori ha comparato le misurazioni ottenute con le variabili et e sesso [ 23 ] , mentre un altro esclusivamente al sesso [ 22 ]  . 
7a three - dimensional anal endosonography of the external and internal anal sphincter in the longitudinal anterior ( a , b ) and posterior ( c , d ) planes ; distance from the external anal sphincter to the vagina and the gap in women . 
 a relatively large number of reports on the use of anal eus , in 2d [ 17 ] and 3d [ 10 , 11 , 2125 ] , for anatomical study fig . 
 these studies are , however , methodologically heterogeneous , precluding any comparison of the data reported or the definition of normal values in the measurement of muscular components of the anal canal . 
in particular , one research group compared measurements obtained with the variables age and sex [ 23 ] , whereas another group focused on sex alone [ 22 ]  . 
despite the small study populations , both of these studies identified a sex - related variability in the length of the anal sphincters in the anterior longitudinal plane independent of age [ 22 , 23 ]  . 
both sphincters appear to be shorter anteriorly in women . more conflicting are data on the thickness of the structures of the two sphincters : according to some authors [ 23 ] the thickness of both sphincters increases linearly with age , in both men and women ; according to others [ 22 ] , ias thickness increases with age , whereas eas shows no significant change related to any of the variables . 
entrambi appaiono pi brevi anteriormente nei soggetti di sesso femminile . pi discordanti sono apparsi i dati circa lo spessore delle strutture sfinteriali : secondo alcuni autori [ 23 ] risultano aumentare entrambi proporzionalmente con let , sia in soggetti maschili che femminili ; secondo altri [ 22 ] , mentre lo spessore del sai si accresce con let , il sae non mostra significative differenze con nessuna delle variabili . 
questultimo discrepante riscontro sarebbe da attribuire ai diversi criteri di inclusione ( solo donne nullipare ) o al differente approccio metodologico ( misurazione dello spessore esclusivamente alle ore 3 , esclusione del muscolo longitudinale dalla misurazione del sae , posizione prona durante lesecuzione dellesame ) [ 20 , 23 ]  . 
non agevole , infatti , ottenere una precisa comparazione dei dati presenti in letteratura , sia per i diversi metodi di misurazione adoperati , us 2d vs 3d , sia per il decubito differente assunto dai soggetti , laterale piuttosto che prono , che per la popolazione eteroge768 radiol med ( 2012 ) 117 : 759771 even found a significant negative correlation between eas thickness and age [ 7 ]  . 
the latter discrepant finding is to be ascribed to the different inclusion criteria ( only nulliparous women ) or the different methodological approach ( measurements taken at 3 oclock position only , exclusion of the longitudinal eas muscle measurements , prone position during the examination ) [ 20 , 23 ]  . 
3d us , the different position of the subjects ( lateral or prone ) and the heterogeneous study population given that some studies include only nulliparous women [ 7 ] and other pluriparous women , as well [ 23 ]  . 
 our study analysed both the length and thickness of the eas and ias in 85 patients using 3d anal eus examinations negative for distal anorectal disease , and the results were evaluated according to patients age and sex . 
as reported by others [ 5 , 7 , 10 , 11 , 23 ] , thickness increases with age , but this increase is more significant in those older than 5060 years . 
in our study population , we found mean thickness values of 0.21 cm ( range 0.050.4 cm ) in those younger than 50 and of 0.26 cm ( range 0.180.6 cm ) in those older than 50 . 
 although our results revealed a trend to increased length of the lateral segment of the ias , the anterior region in the two women with the highest values showed the greatest diameter . 
this finding supports the view of some previous authors [ 31 ] , but it contrasts with that of others [ 23 ] who describe a trend to increased length in men . 
 the greater thickness of the anterior ias is apparently justified by the fact that in women , there is a compensatory mechanism for the oblique anterior angulation of the sphincter muscles [ 31 ]  . 
 eas thickness also showed a trend to increase proportionately with age , consistent with some [ 23 ] , but in disagreement with other [ 20 , 22 ] authors who describe an absence of a significant increase and even a reduction in thickness with age [ 7 ]  . 
in four women aged 5777 years , it reached a maximum value of approximately 0.9 cthe population examined shows increased thickness of the anal sphincters in both sexes , and the finding supports the hypothesis whereby nea presa in esame , dal momento che alcuni studi includono solo donne nullipare [ 7 ] , altri anche pluripare [ 23 ]  . nel nostro studio sono stati analizzati sia la lunghezza che lo spessore di sae e sai in 85 soggetti con esame us - 3d negativo per patologia dellano - retto distale ed i risultati sono stati esaminati in relazione ad et e sesso . 
quello interno era compreso , in assoluto , tra 0 , 05 cm e 0 , 6 cm ( in media 0 , 3 cm ) e non significativamente differente nei due sessi . 
come gi riportato da altri gruppi [ 5 , 7 , 10 , 11 , 23 ] , lo spessore aumenta con let , ma questo incremento pi significativo in soggetti con et superiore a 5060 anni . 
nel nostro gruppo abbiamo riscontrato valori dello spessore medio pari a 0 , 21 cm ( spessore minimo 0 , 05 cm ; spessore massimo 0 , 4 cm ) nei soggetti con et inferiore a 50 anni , e pari a 0 , 26 cm ( spessore minimo 0 , 18 cm ; spessore massimo 0 , 6 cm ) nei soggetti con et superiore ai 50 anni . 
 in particolare i valori pi elevati sono stati riscontrati in due donne rispettivamente di 55 ( 0 , 5 cm ) e 59 ( 0 , 6 cm ) anni . sebbene i nostri risultati abbiano rivelato una tendenza allaccrescimento maggiormente significativa per il segmento laterale del sai , la regione anteriore delle due donne , con valori massimi registrati , mostrava il maggior diametro ; tale riscontro a favore della tesi di alcuni [ 31 ] , ma si contrappone ad altri [ 23 ] che descrivono invece una tendenza al maggiore sviluppo negli uomini . lo spessore pi ampio nella porzione anteriore del sai sarebbe giustificato dal fatto che , nei soggetti di sesso femminile , esiste un meccanismo di compenso allandamento obliquo anteriore di questa struttura muscolare [ 31 ]  . 
lo spessore del sae ha mostrato anchesso una tendenza allaumento proporzionale con let , in accordo con alcuni [ 23 ] , ma in disaccordo con altri [ 20 , 22 ] che descrivevano assenza di variazioni significative o viceversa una riduzione di spessore proporzionalmente allincremento dellet [ 7 ]  . 
in quattro donne con et compresa tra i 57 ed i 77 anni ha raggiunto un valore massimo di circa 0 , 9 cla popolazione esaminata presenta un accrescimento in termini di spessore degli sfinteri anali , in entrambi i sessi , ed il riscontro a favore della tesi secondo cui entrambe le strutture tendono ad ispessirsi con let [ 23 ]  . sebbene non esistano valori assoluti di normalit , sono descritti , per il sai , valori in media di 0 , 20 , 3 cm e si ritengono patologici , indipendentemente dallet , valori superiori a 0 , 4 cm , mentre per il sae sono riportati valori in media da 0 , 6 a 0 , 8 cm [ 16 , 17 ]  . 
la conoscenza di questi range di normalit appare essenziale per la diagnosi di atrofia e / o radiol med ( 2012 ) 117 : 759771 both structures tend to thicken with age [ 23 ]  . 
 although there are no absolute values of normality , the reported average ias values are 0.20.3 cm , with values > 0.4 cm being considered pathological , regardless of age ; reported average eas values 0.60.8 cm [ 16 , 17 ]  . 
knowledge of the ranges of normality is essential for diagnosing atrophy and / or the presence of sphincter defects or interruptions , as might occur after certain surgical procedures or traumatic events , which may lead to disorders such as faecal incontinence . 
moreover , knowledge of normal thickness values of the various muscular structures might be helpful for distinguishing between pathological muscular thickening and paraphysiological age - related thickening [ 1416 , 32 , 36 , 37 ]  . 
it enables distinction between cases of faecal incontinence associated with intact sphincters from other conditions related to muscular lesions , such as defects , adhesions , reduced or increased thickness or atrophy . 
furthermore , it makes possible measurements of the extension , thickness and area of the sphincter defect in the coronal and sagittal planes and volumetric reconstructions of the lesion [ 1417 ]  . 
the anatomical gap produced by this asymmetrical configuration would explain , on the basis of a lower resistance of the anterior rectal wall , the greater incidence of functional female pelvic floor disorders , such as faecal incontinence , anterior rectocele and rectorectal intussusception [ 1217 , 22 , 23 , 2630 , 3840 ]  . 
this morphological finding could also allow us to better correlate the clinical picture and sonographic findings , especially in women , in whom anatomical differences may correspond to differences in function . limitations of our study are firstly the retrospective nature of the analysis and the size of the sample which , while being the largest in the literature , is not insufficient to be able to establish an absolute range of normality . 
for example , measurements of sphincter thickness were taken in a single scan plane ( intermediate for the ias and superficial for the eas ) , and no attempt was made to calculate the distance between the eas and the anorectal junction ( defined as gap )  . 
 presenza di difetti o interruzioni sfinteriali , come potrebbe avvenire , per esempio , dopo alcuni interventi chirurgici o in seguito ad alterazioni traumatiche , che possono condurre a disturbi quali lincontinenza fecale . 
la conoscenza dei valori normali dello spessore delle varie strutture muscolari , inoltre , pu essere di ausilio nella distinzione tra un ispessimento muscolare patologico e quello para - fisiologico etcorrelato [ 1416 , 32 , 3237 ]  . lecografia endoanale 3d divenuta nel tempo la tecnica gold standard per la valutazione morfologica del canale anale . 
permette di distinguere casi di incontinenza fecale associati a strutture sfinteriali integre da altre condizioni legate a lesioni muscolari , quali difetti , aderenze cicatriziali , riduzione o incremento di spessore e atrofia . 
inoltre , permette di ottenere le misurazioni in estensione , spessore , area del difetto sfinterico nei piani coronale e sagittale e volume del danno lesionale [ 1417 ]  . 
lestensione di entrambi gli sfinteri risultata , in accordo con la letteratura [ 22 , 23 ] , meno sviluppata anteriormente nelle donne ( valori in media rispettivamente di 2 , 4 e 1 , 4 cm nelle donne vs 2 , 6 e 2 , 1 cm negli uomini )  . 
infine la lunghezza del canale anale , corrispondente a quella del sae nel piano longitudinale posteriore , si mostrata sensibilmente maggiore nel sesso maschile ( in media 3 , 5 cm vs 3 , 05 cm ) in accordo con diversi contributi scientifici [ 311 , 1820 , 22 , 23 , 31 , 3537 ]  . 
il gap anatomico determinato da tale configurazione asimmetrica del canale anale spiegherebbe , a causa di una minore resistenza della parete anteriore del retto , la maggiore incidenza di disturbi funzionali del pavimento pelvico femminile , quali incontinenza fecale , rettocele anteriore ed intussuscezione retto - rettale [ 1217 , 22 , 23 , 2630 , 3840 ]  . 
tale riscontro morfologico potrebbe consentire anche di correlare meglio linquadramento clinico con i reperti ecografici soprattutto nei soggetti di sesso femminile , nei quali alle differenze anatomiche possono corrispondere funzionalit diverse . i limiti del nostro studio sono rappresentati anzitutto dal tipo di analisi dei dati di tipo retrospettivo e dalla numerosit campionaria , che per quanto rappresenti la pi estesa in letteratura , non assurge ad un livello tale da permettere di poter stabilire range di normalit in assoluto . 
inoltre alcune misurazioni potrebbero esser considerate incomplete dal momento che per lo spessore sfinteriale esse siano state condotte in un singolo piano di scansione ( intermedio per il sai e superficiale per il sae ) e che non sia stata calcolata la distanza tra sae e giunzione ano - rettale , definita gap . conclusioni lus endoanale si rivelata una metodica di facile esecuzione ed estremamente affidabile nel riconoscimento di tutte 770 conclusions anal eus proved to be easy to perform and extremely reliable in depicting all structures making up the anal canal . 
 application of 3d imaging provides the added value of easy manipulation of the data set , which is obtained as a vector volume from different angles , to define the precise location and extension of the structures being considered . 
in relation to sex , the anal canal has an asymmetric configuration : anal sphincters are shorter anteriorly in women , as is the extension of the entire anal canal . 
in relation to age , however , there is an increase in ias and eas muscular thickness , which tends to be more significant among individuals older than 5060 years . 
the possibility of adequately correlating anatomical sphincter structures to age and sex , aided by the correct use of 3d us imaging and the knowledge of the normal range for structures being examined , may help identify and correctly interpret the small paraphysiological changes related to age and sex , distinguishing them from pathological anatomical disorders due to pelvic - floor dysfunction . 
lapplicazione dellimaging 3d offre un valore aggiunto , rappresentato dalla possibilit di poter facilmente manipolare da differenti angolazioni la serie di dati ottenuti sotto forma di un vector volume , definendo lesatta localizzazione ed estensione delle strutture esaminate . 
il canale anale , in relazione al sesso , presenta una configurazione asimmetrica : gli sfinteri anali anteriormente sono pi brevi in quello femminile , cos come appare in estensione il canale anale in toto . 
in relazione allet , invece , si assiste ad un incremento dello spessore muscolare di sai e sae tendenzialmente pi significativo in una fascia di et superiore ai 5060 anni . 
blickman georg thieme verlag stuttgart , new york , 2011 isbn : 978 - 3 - 13 - 143711 - 2 published online : 7 january 2012 springer - verlag 2012 since 1999 , when dr . 
 all these innovations [ digital imaging , workflow optimization , electronic patient records , internet exchange of patient data and consultations , ultrasounds ( us ) , computed tomography ( ct ) , magnetic resonance imaging ( mri ) , nuclear medicine , etc . ] are well presented and discussed by the authors , who also highlight , in their preface , the image gently campaign to reduce possible radiation risks in children . having on hand the previous edition of the book one will immediately realize how previous statements are reflected in text and image choice . the structure of the book is based on more or less long introductions to the addressed topic , followed by long lists of light - blue coloured tables ( the backbone of the book ! ) , which are divided into three parts : diagnosis , findings , and comments . 
these are enriched by images depicting some of the most relevant radiological problems . in the diagnosis section of each table , references to previous pages and / or figures dedicated to the same topic or problem are very often presented , making one flip backward and forward through the pages . 
the findings section of the tables , offer the most important diagnostic radiologic information while the comments section give the reader hints about what could be further done to improve the diagnosis . this 678 page book is divided into six chapters : five list the daily organ - based workflow of a paediatric radiology department ( thorax , mediastinum , heart and great vessels ; abdomen and gastrointestinal tract ; urogenital tract ; skull , intracranial space and vertebral column ; skeleton and soft tissues ) , the last chapter provides normal values , so important in the evaluation of a growing child . 
ebel e collaboratori diedero alle stampe ledizione inglese del volume differential diagnosis in pediatric radiology , questa branca della radiologia andata incontro a cambiamenti e miglioramenti epocali . tutte queste innovazioni [ radiologia digitale , organizzazione del flusso del lavoro , registrazione elettronica dei dati del paziente , possibilit di trasmissione via internet degli stessi e di consultazioni a distanza , ultrasuoni , tomografia assiale computerizzata ( tac ) , risonanza magnetica ( rm ) , medicina nucleare , ecc . ] sono ora presentate e discusse in modo ottimale dagli autori , che mettono anche ben in evidenza , nella loro prefazione , la attuale campagna di image gently ( immagini riprese con dolcezza ) allo scopo di ridurre i possibili rischi da radiazioni nei bambini . chi ha a disposizione la precedente edizione del volume si render immediatamente conto di come , quanto detto sopra , si trovi poi riflesso nel testo e nelle immagini . il volume strutturato su introduzioni pi o meno brevi allargomento da trattare , seguite da lunghi elenchi di tabelle ( lossatura del volume ! ) dal leggero colore blu di fondo , divise in tre parti : diagnosi , riscontri radiologici , commenti ; il tutto arricchito da immagini che illustrano alcuni dei pi importanti problemi radiologici . nella parte di ogni tabella dedicata alla diagnosi vengono fatti spesso riferimenti a pagine e / o figure dedicate allo stesso argomento o problema , con la conseguenza di un andare avanti ed indietro nelle pagine . 
 il volume , nelle sue 678 pagine , diviso in sei capitoli : cinque sono dedicati al flusso giornaliero diagnostico di un reparto di radiologia pediatrica su base di organo ( torace , mediastino , cuore e grandi vasi ; addome ed apparato gastrointestinale ; apparato urogenitale ; cranio , suo contenuto e colonna vertebrale ; scheletro e tessuti molli ) , mentre lultimo fornisce i valori normali , cos importanti nella valutazione di un soggetto in via di crescita . 
una lunga lista di abbreviazioni e lindice arricchiscono poi il testo . the two authors and their large team of contributors from i due autori , coadiuvati da un folto gruppo di collaboradiol med ( 2012 ) 117 : 894895 all over the world have collected a great number of images to implement and update those from the previous edition . 
 i found the hospital jargon and sometimes colloquial quotations from the literature improperly used ( how many non - english readers will , for example , know what a lincoln log vertebral body is and what it looks like or what the tam oshanker appearance of a skull x - ray means ? )  . being also pernickety i found misprints , some incorrect figure quotations and references to not existent tables . 
the literature references are listed without numbers and in alphabetical order cited , not cited in the text in four chapters ; numbered , cited in the text and not in alphabetical order in two . those who buy the book will also benefit from 12 months of free access to 250 radcases on line , to further implement their knowledge . just like the previous edition , this book should be part of any paediatric radiology department library , most of all it should be made available to younger staff members , as well as surgeons and paediatricians . 
la maggior parte delle immagini ( ma non tutte , alcune addirittura deludenti ) sono ben riprodotte . ho riscontrato che gergo ospedaliero e talora citazioni colloquiali dalla letteratura sono usati in modo improprio : per esempio chi dei lettori non di lingua inglese sa cosa sia un lincoln log ( capanna a tronchi dalbero ) riferito allaspetto di un corpo vertebrale o cosa aspettarsi da un radiogramma del cranio con laspetto tipo tam oshanker ( tipico berretto scozzese , che sporge dalla fronte ) ? pignolino , ho anche riscontrato errori di stampa , alcune citazioni improprie di figure ed anche riferimenti a tabelle inesistenti . 
le voci bibliografiche sono elencate senza numerazione , in ordine alfabetico e non citate nel testo in quattro capitoli ; numerate , citate nel testo e non in ordine alfabetico in due . quanti compreranno il volume , avranno anche diritto a 12 mesi di accesso gratuito , in rete , a 250 radcases , onde incrementare la proprie conoscenze . 
 come il volume della precedente edizione anche lattuale dovrebbe far parte della biblioteca di ogni reparto di radiologia pediatrica , per essere a disposizione soprattutto dei componenti pi giovani dello stesso , ed anche di chirurghi e pediatri . 
esso servir quale fonte importante di conoscenza e discussione quando ci si trover di fronte ad un dubbio diagnostico , ricordando sempre il vecchio adagio : maxima debetur puero reverentia . 
lagalla1 1department of radiology , university of palermo , via del carabiniere 32 , 90127 palermo , italy 2department of oncology , division of general and oncological surgery , university of palermo , via del vespro 129 , 90127 palermo , italy correspondence to : t.v. 
bartolotta , tel : + 39 - 091 - 6552330 , fax + 39 - 091 - 6552337 , e - mail : tv.bartolotta@unipa.it received : 26 february 2011 / accepted : 31 march 2011 / published online : 18 november 2011 springer - verlag 2011 abstract purpose . 
the authors sought to assess the incidence of new foci of hepatocellular carcinoma ( hcc ) using multidetector computed tomography ( mdct ) in patients treated with radiofrequency ablation ( rfa )  . 
two readers retrospectively reviewed by consensus the follow - up mdct studies of 125 patients ( 88 men and 37 women ; mean age 68 years ) with 141 hccs ( size 15.2 cm ; mean 2.2 cm ) treated with rfa . 
due radiologi hanno valutato retrospettivamente e in consenso gli studi tcmd relativi al follow - up di 125 pazienti ( 88 uomini e 37 donne ; et media : 68 anni ) affetti da 141 hcc ( dimensioni : 15 , 2 cm ; media : 2 , 2 cm ) trattati con rfta . 
 sono stati osservati 132 / 141 ( 93 , 6% ) casi di trattamento completo e 29 / 141 ( 20 , 6% ) casi di progressione locale del tumore . 740 radiol med ( 2012 ) 117 : 739748 multiple and located in a liver segment different from that of the previously treated nodules . keywords radiofrequency ablation ( rfa ) liver ct liver neoplasms conclusioni . 
in pazienti sottoposti a rfta , la tcmd rivela unelevata incidenza di nuovi foci di hcc , gi entro un anno , solitamente multipli e in segmenti diversi rispetto al nodulo trattato . parole chiave termoablazione con radiofrequenza ( rfta ) fegato tc neoplasie epatiche introduction introduzione radiofrequency ablation ( rfa ) is increasingly being used as the percutaneous treatment of choice for patients with early - stage hepatocellular carcinoma ( hcc ) in whom surgical resection or liver transplantation are not feasible or available , as it guarantees excellent local control with acceptable morbidity and mortality rates [ 13 ]  . 
an accurate assessment of response to treatment is essential considering that , although complete treatment significantly increases patient survival , evidence of viable tumour tissue typically represents a precise indication for repeated treatment [ 4 ]  . 
 however , regardless of the treatment strategy , hcc has a high rate of intrahepatic distant recurrence , which is associated with a significant increase in mortality rates [ 5 , 6 ]  . 
 as a consequence , early detection of new hcc nodules at follow - up is crucial to improve clinical management and , ultimately , patient survival [ 7 ]  . 
for this purpose , diagnostic imaging , and multidetector computed tomography ( mdct ) in particular , plays a key role in clinical practice [ 8 , 9 ]  . 
the purpose of this study was to assess the incidence of new hcc foci at mdct in patients who underwent rfa . materials and methods patients and lesions after obtaining approval from the local ethics committee , we retrospectively studied 125 cirrhotic patients ( 88 men and 37 women ; age range 4684 years ; mean age 67.96.95 ) who had undergone rfa treatment of 141 hcc nodules ( size 15.2 cm ; mean , 2.20.83 cm ) between february 1999 and march 2010 . 
 rfa technique all treatments were performed using the ultrasound ( us ) la termoablazione mediante radiofrequenza ( rfta ) sempre pi frequentemente impiegata come trattamento percutaneo di scelta per quei pazienti affetti da epatocarcinoma ( hcc ) in stadio precoce , allorquando la resezione chirurgica o il trapianto di fegato sono opzioni non praticabili o non disponibili , garantendo un eccellente controllo locale di malattia a fronte di accettabili tassi di morbilit e mortalit [ 13 ]  . 
unaccurata valutazione della risposta terapeutica di cruciale importanza , considerato che , mentre un trattamento completo migliora significativamente la sopravvivenza dei pazienti , lidentificazione di tessuto tumorale vitale pone , di norma , la precisa indicazione ad un nuovo trattamento [ 4 ]  . 
tuttavia , indipendentemente dalla modalit di trattamento , lepatocarcinoma presenta un elevato tasso di recidiva intraepatica a distanza , questultimo associato ad un significativo incremento della mortalit [ 5 , 6 ]  . 
di conseguenza , la precoce individuazione di nuovi noduli di hcc durante il follow - up risulta fondamentale al fine di migliorare la gestione clinica del paziente e , in ultima analisi , la sopravvivenza [ 7 ]  . 
a tale scopo , nella pratica clinica , le tecniche di diagnostica per immagini , e tra queste la tomografia computerizzata multidetettore ( tcmd ) , giocano un ruolo chiave [ 8 , 9 ]  . 
scopo del presente lavoro stato quello di valutare lincidenza di nuovi foci di hcc alla tcmd in pazienti sottoposti a trattamento di rfta di epatocarcinoma . materiali e metodi pazienti e lesioni ottenuta lapprovazione da parte del comitato etico istituzionale , sono stati retrospettivamente valutati 125 pazienti ( 88 uomini ; 37 donne ) di et compresa fra 46 e 84 anni ( et media : 67 , 96 , 95 anni ) affetti da cirrosi epatica e complessivamente sottoposti a trattamento di rfta di 141 noduli di hcc ( dimensioni : 15 , 2 cm ; media 2 , 20 , 83 cm ) dal febbraio 1999 al marzo 2010 . 
in particolare , i criteri radiol med ( 2012 ) 117 : 739748 di inclusione nello studio sono stati : ( 1 ) presenza di almeno un nodulo di hcc sottoposto a rfta ; ( 2 ) disponibilit di almeno uno studio tcmd multifasico post - rfta reperito nel nostro pacs istituzionale ( impax , agfa - gevaert , milano , italia )  . 
 tecnica rfta tutti i trattamenti sono stati effettuati con tecnica percutanea ( n = 97 ) , laparoscopica ( n = 7 ) o chirurgica open ( n = 37 ) mediante guida ecografica ed impiegando gli aghi e i generatori indicati in tabella 3 . 
 dopo la termoablazione , lago stato estratto mantenendo lestremit calda al fine di prevenire , mediante termocoagulazione , eventuali fenomeni emorragici o un accidentale insemenzamento neoplastico lungo il percorso dellago . 
 tecnica desame tc e follow - up i pazienti sono stati sottoposti ad esame tc dopo un mese dal trattamento e , qualora negativo , a distanza di 3 e poi 612 mesi , salvo diversa indicazione clinica o esigenze relative al paziente . 
lo studio tc stato eseguito utilizzando unapparecchiatura multidetettore a 64 strati philips brilliance ( royal philips electronics , andover ma , usa ) acquisendo immagini in condizioni di base e dopo somministrazione di 1 , 5 ml / kg di iomeprolo ( 400 mgi / ml ; iomeron bracco , milano , italia ) ad una velocit di 4 ml / s mediante un iniettore automatico . 
una volta raggiunta questultima sono state effettuate tre scansioni impostando un ritardo , rispettivamente , di 2025 s ( fase arteriosa ) , 50 s ( fase portale - venosa ) e 180300 s ( fase allequilibrio )  . per la valutazione delle immagini tcmd , stato impiegato il sistema picture archiving and communications system ( pacs ) in dotazione alla nostra istituzione ( impax , agfagevaert , milano , italia )  . 
due radiologi con pi di dieci anni di esperienza in radiologia addominale , non coinvolti nellesecuzione degli esami e non a conoscenza della storia clinica dei pazienti n della diagnosi finale , hanno esaminato in consenso off - line le immagini ottenute . 
 ct examination and follow - up patients underwent ct examination 1 month after treatment and , if results were negative , at 3 and then 612 months , unless there were specific clinical indications or patient requirement . 
images were acquired at baseline and after administration of 1.5 ml / kg of iomeprol ( 400 mgi / ml ) ( iomeron , bracco , milan , italy ) delivered at a flow rate of 4 ml / s using an automatic injector . 
scans were performed using the multable 3 radiofrequency ablation technique nodules treated total 2 ( p ) 3 ( o ) 5 p , percutaneous ; o , open surgery ; l , laparoscopy tabella 3 tecnica rfta noduli trattati totale 2 ( p ) 3 ( o ) p , percutanea ; o , open ; l , laparoscopica 10 ( p ) 7 ( o ) 10 ( p ) 7 ( o ) 1 . 
linsorgenza di nuovi foci di hcc , definiti come noduli ipervascolari in fase arteriosa e con wash - out in fase portale e / o allequilibrio insorgenti in altro segmento rispetto al nodulo trattato con rfta o nello stesso segmento , ma ad una distanza superiore a 2 cm dal nodulo trattato [ 10 ] ; 2 . 
la presenza di foci di ipervascolarit nodulare ad una distanza inferiore a 2 cm dal nodulo inizialmente trattato stata considerata : ( a ) tumore residuo non ablato ( persistenza di malattia ) se rilevata al primo controllo tc post - rfta ( 1 mese dopo il trattamento ) ; ( b ) progressione locale del tumore ( ripresa di malattia ) se rilevata ad un successivo controllo tc ( in questi casi nel controllo ad 1 mese era assente tessuto tumorale residuo )  . 
a region of interest ( roi ) was positioned near the abdominal aorta , at the level of the celiac tripod , and an enhancement threshold of 150 hu was selected . 
once the threshold was reached , three scans were obtained with a delay of 2025 s ( arterial phase ) , 50 s ( portalvenous phase ) and 180300 s ( equilibrium phase )  . image analysis image analysis was conducted on our institutions pacs system ( impax , agfa - gevaert , milan , italy )  . 
two radiologists with > 10 years of experience in abdominal radiology , not involved in the scanning phase and blinded to patients clinical history and final diagnoses reviewed the images in consensus working off - line . 
the development of new hcc foci , defined as hypervascular nodules in the arterial phase and with washout in the portal and / or equilibrium phase , arising in either a different segment from that of the rfa - treated nodule or in the same segment but at a distance > 2 cm from the treated nodule [ 10 ] ; 2 . 
the presence of foci of nodular hypervascularity < 2 cm from the nodule treated initially was considered : ( a ) residual , nonablated tumour ( disease persistence ) if detected at the first follow - up ct after rfa ( 1 month after treatment ) , and ( b ) local tumour progression ( disease relapse ) if detected at subsequent follow - up ct scans ( in these cases , no residual neoplastic tissue was evident at 1 - month follow - up )  . 
 analisi statistica relativamente alla comparsa di nuovi noduli di hcc dopo rfta sono stati valutati i seguenti potenziali fattori di rischio : ( a ) grado avanzato della sottostante malattia epa tica ( classe child - pugh c ) ; ( b ) diametro massimo del tu more trattato superiore a 2 cm ; ( c ) pregresso trattamento interventistico o chirurgico ; ( d ) tumore multiplo al mo mento della rfta ; ( e ) contatto del tumore trattato con i vasi epatici maggiori ; ( f ) contatto del tumore trattato con la capsula epatica ; ( g ) inadeguatezza dei margini di re sezione . lanalisi statistica stata effettuata mediante un programma commerciale ( intercooled stata , versione 9.2 per windows , statecorp , tx , usa ) , mediante il test del chiquadrato , o il test esatto di fisher quando appropriato , con livello di significativit statistica fissato a p inferiore a 0 , 05 . 
ottantasei nuovi noduli di hcc su 113 ( 76 , 1% ) erano multipli , mentre i rimanenti 27 / 113 ( 23 , 9% ) nuovi noduli erano singoli ( p < 0 , 0001 )  . 
in particolare , 7 pazienti hanno sviluppato 2 noduli , 10 pazienti 3 noduli , 4 pazienti 4 noduli e i rimanenti 4 pazienti 5 , 6 , 7 e 8 noduli ciascuno . lintervallo libero da malattia stato in media di 16 , 116 , 31 mesi ( intervallo : 152 mesi )  . 
per quanto attiene la sede dei nuo vi noduli rispetto al primitivo nodulo trattato mediante rfta , 21 / 113 ( 18 , 6% ) hcc sono insorti nello stesso segmento mentre la maggioranza dei nuovi foci di hcc ( 92 / 113 ; 81 , 4% ) si sviluppata in altri segmenti epatici ( p < 0 , 0001 ) , prevalentemente nel lobo destro ( 70 / 113 ; statecorp , tx , usa ) using the chi - square test , or the fisher exact test when appropriate , with statistical significance set at p < 0.05. 
in particular , seven patients developed two nodules , ten three nodules , four four nodules and the remaining four five , six , seven and eight nodules each . mean disease - free interval was 16.116.31 ( range 152 ) months . 
regarding the site of the new hcc relative to the treated nodule , 21 / 113 ( 18.6% ) occurred in the same segment , whereas the majority of new hcc foci ( 92 / 113 ; 81.4% ) occurred in other hepatic segments ( p < 0.0001 ) , more frequently in the right ( 70 / 113 ; 62% ) than in the left ( 43 / 113 ; 38% ) lobe ( p = 0.0003 ) ( table 4 )  . 
questi pazienti sono stati monitorati in media 15 , 6419 , 25 mesi ( intervallo : 189 mesi ) , periodo mediamente inferiore in maniera statisticamente significativa rispetto ai 69 pazienti con nuovi noduli di hcc ( 30 , 3819 , 14 mesi ) ( p < 0 , 001 )  . 
lunico fattore di rischio che ha presentato una correlazione statisticamente significativa con linsorgenza di nuovi noduli di hcc risultato essere la vicinanza alla capsula epatica ( p < 0 , 018 ) ( tabella 5 )  . persistenza di malattia e / o progressione locale complessivamente , sono stati osservati 9 / 141 ( 6 , 4% ) casi di trattamento incompleto a fronte di una necrosi completa nei rimanenti 132 / 141 ( 93 , 6% ) noduli trattati ( p < 0 , 0001 )  . 
la progressione locale del tumore stata osservata in 29 / 141 ( 20 , 6% ) casi , dopo un intervallo di tempo pari a 248 mesi ( media : 13 , 2 mesi )  . 
nessuna recidiva locale stata osservata dopo 48 mesi e lintervallo libero da recidiva risultato in media di 15 , 6419 , 25 mesi ( intervallo : 238 mesi )  . discussione nella nostra serie di pazienti , trattati mediante rfta e controllati con tcmd in media per circa due anni , nuovi noduli di hcc sono stati riscontrati in poco pi della met dei casi ( 55 , 2% )  . 
a alla tc effettuata 18 mesi dopo rfta , in corrispondenza del vivii segmento , si apprezza una formazione ovalare iperdensa in fase arteriosa del diametro di 2 , 1 cm ( freccia )  . 
in fact , similar recurrence rates may be observed in cirrhotic patients with hcc treated with any type of percutaneous technique or even after surgical resection [ 12 ]  . 
although in our experience new hcc nodules were detected in significant percentages of cases as late as 2 and 3 years after treatment ( in 35% and 20% of cases , respectively ) , most patients ( 45% approximately ) developed new hcc foci within 1 year from treatment . 
concerning a more rapid growth rate of new hcc nodules in patients treated with rfa compared with nontreated hcc , suggesting the need for shorter follow - up intervals in the first group compared with the second [ 13 ]  . 
however , it should be noted that the group of patients who did not develop new hcc nodules in our series had a substantially shorter follow - up period , espressione dellintrinseca natura multicentrica dellhcc insorgente nel fegato cirrotico e , dunque , non rappresenta un inconveniente dellrfta . 
un analogo tasso di recidiva si pu riscontrare , infatti , in pazienti cirrotici con hcc che sono trattati con qualsiasi tipo di terapia percutanea o , anche , dopo resezione chirurgica [ 12 ]  . 
sebbene nella nostra esperienza nuovi noduli di hcc siano stati riscontrati in percentuali significative anche dopo due e tre anni dal trattamento rispettivamente nel 35% e nel 20% dei casi la maggioranza dei pazienti trattati ha sviluppato nuovi foci di hcc nellarco del primo anno di controlli , con una percentuale di circa il 45% . 
 [ 13 ] di un pi rapido tasso di crescita di nuovi noduli di epatocarcinoma in pazienti trattati con rfta rispetto agli epatocarcinomi non trattati , suggerendo nei primi leffettuazione di controlli pi ravvicinati nel tempo rispetto ai secondi [ 13 ]  . 
tuttavia , opportuno sottolineare come , nella nostra serie , il gruppo dei pazienti che non ha sviluppato nuovi hcc sia stato monitorato per un tempo nettamente inferiore , pari a circa la met , rispetto al primo . 
 [ 12 ] al prolungarsi del follow - up , pari a ben l81% a cinque anni , che il perdurare dellosservazione avrebbe potuto condurre alla scoperta di nuovi noduli anche in questo gruppo di pazienti [ 12 ]  . i nuovi foci di hcc da noi osservati si sono manifestati in maniera statisticamente significativa prevalentemente in forma multipla ( 86 / 113 ; 76 , 1% ) ed in segmenti epatici diversi ( 92 / 113 ; 81 , 4% ) rispetto alla sede del primitivo nodulo di hcc trattato mediante rfta . 
in particolare , sebbene nella nostra casistica i segmenti maggiormente coinvolti dallinsorgenza di nuovi noduli siano stati quelli di destra rispettivamente lviii , seguito dal vii e dal vi nessun segmento stato tuttavia risparmiato . 
tali rilievi sono sostanzialmente in accordo con i dati di letteratura che indicano un elevato tasso di recidiva intraepatica dellhcc in siti diversi rispetto a dove avvenuto il trattamento termoablativo , con percentuali variabili dal 40 , 6% al 53% [ 2 , 6 , 14 , 15 ]  . 
 over longer follow - up periods ( as high as 81% at 5 years ) , a longer follow - up period might have led to detection of new nodules in this group of patients [ 12 ]  . there was a statistically significant predominance of new hcc foci that were multiple ( 86 / 113 ; 76.1% ) and occurring in different segments ( 92 / 113 ; 81.4% ) relative to the site of the primary hcc nodule treated with rfa . 
these findings are consistent with the literature , which indicates a high rate of intrahepatic hcc recurrence at sites other than that of the rfa , with percentages ranging from 40.6% to 53% [ 2 , 6 , 14 , 15 ]  . 
in this respect , there is evidence that recurrence in a different hepatic segment , associated with the presence of distant metastases , has a significant negative influence on overall survival ; hence , constant monitoring and aggressive treatment may be indicated in patients with intrahepatic recurrence in a different segment in order to optimise the benefits of rfa [ 6 , 7 ]  . 
 therefore , all the above confirms the advantage of following up patients treated with rfa with an imaging modality , such as mdct , which is able to visualise the entire hepatic parenchyma . 
other modalities , such as contrast - enhanced us , may be useful for assessing treatment effectiveness verso segmento epatico , insieme alla presenza di metastasi a distanza , influenzano negativamente e significativamente la sopravvivenza globale , per cui una sorveglianza regolare e un trattamento aggressivo possono risultare indicati in pazienti con recidiva intraepatica in un segmento differente per ottimizzare i benefici dellrfta [ 6 , 7 ]  . 
quanto sopra riportato conferma , quindi , tutta limportanza ed il vantaggio di impiegare ai fini del monitoraggio dei pazienti sottoposti a rfta una tecnica , quale la tcmd , in grado di valutare lintero parenchima epatico . 
infatti altre tecniche , quali ad esempio lecografia con mezzo di contrasto , possono essere sicuramente utili per valutare lefficacia del trattamento , soprattutto durante la procedura interventistica stessa , ma risultano poco o affatto indicate nella individuazione di nuovi foci di epatocarcinoma nei successivi controlli [ 16 , 17 ]  . meno univoci sono i dati riportati in letteratura riguardo i fattori di rischio della recidiva intraepatica a distanza dellhcc . 
 [ 15 ] si giunti alla conclusione che i pazienti che hanno pi noduli di hcc , bassi livelli sierici di piastrine o di albumina , associati ad infezione da virus dellepatite c dovrebbero essere seguiti attentamente a causa dellelevata incidenza di nuove lesioni di hcc nel resto del fegato , anche dopo necrosi coagulativa radiol med ( 2012 ) 117 : 739748 especially during the interventional procedure but they have few or no indications for detecting new hcc foci during the follow - up [ 16 , 17 ]  . data regarding risk factors for intrahepatic distant recurrence of hcc are more equivocal . 
reached the conclusion that patients with a greater number of hcc nodules , low serum platelet or albumin levels and associated c virus infection should undergo close monitoring because of the high incidence of new hcc lesions in the rest of the liver , even after complete post - rfa coagulative necrosis [ 15 ]  . 
in our experience , the only risk factor that correlated significantly with the development of new hcc nodules although difficult to ascribe to a precise pathogenetic mechanism was proximity to the hepatic capsule . 
further studies are needed to provide accurate evaluation of this statistical result . the percentage of complete tumour ablation , assessed at mdct , was 93.6% of the nodules ( 132 of 141 treated nodules )  . 
this finding is in line with previously reported values , which confirms the effectiveness of rfa in well - selected patients and suggests its use as a first - line strategy to treat patients with early - stage hcc [ 2 , 6 , 19 ]  . 
first , the reference standard was not liver biopsy in all cases but mdct and / or mr imaging criteria , which are , however , well established in the literature and commonly used in clinical practice . 
rfa was not always performed with the same equipment owing to technological improvements over the years ; this , however , might have influenced failure or progression rates but not the number of new hcc nodules . 
another limitation is that the readers analysed the images in consensus , so we were unable to assess the degree of agreement between independent readers . in conclusion , in our experience , patients with hcc treated with rfa very frequently develop new nodules , even during the first year after treatment . 
therefore , the use of mdct is not only indicated for assessing treatment effectiveness in terms of disease persistence and / or recurrence but , also and above all , for detecting possible new hcc foci and allowing appropriate early treatment . conflict of interest none completa post - rfta [ 15 ]  . 
 [ 14 ] , invece , solo laumento nei livelli sierici di alfa - fetoproteina ( afp ) risultato essere un fattore di rischio per la recidiva intraepatica [ 14 ]  . 
nella nostra esperienza , lunico fattore di rischio correlato in maniera statisticamente significativa allinsorgenza di nuovi noduli di hcc , anche se difficilmente riconducibile ad un preciso meccanismo patogenetico , risultato essere la vicinanza alla capsula epatica . 
ulteriori studi si rendono necessari per valutare correttamente tale dato statistico . di contro , la percentuale di ablazione tumorale completa , individuata sulla base dellesame tcmd , stata del 93 , 6% dei noduli ( 132 noduli su 141 trattati )  . 
questo dato sostanzialmente in linea con i valori riportati in letteratura , confermando lefficacia dellrfta proprio in pazienti adeguatamente selezionati e suggerendone limpiego come tecnica di prima linea nel trattamento dei pazienti con hcc in stadio precoce [ 2 , 6 , 19 ]  . 
durante il follow - up , stata osservata la progressione locale del tumore in 29 casi ( 23 , 2% di tutti i pazienti trattati ) , con un intervallo di tempo compreso tra 2 e 48 mesi , in media 13 , 2 mesi . 
in primo luogo lo standard di riferimento non stato , in tutti i casi , la biopsia epatica , bens i criteri semeiologici alla tcmd e / o alla rm , ancorch noti in letteratura e comunemente impiegati nella pratica clinica . 
la tecnica rfta non stata eseguita con le stesse apparecchiature a causa dei miglioramenti tecnologici apportati nel tempo , ma ci potrebbe avere avuto influenza sul tasso di insuccesso o di progressione , non di nuovi noduli di hcc . 
inoltre , da parte dei lettori stata effettuata una valutazione in consenso e , pertanto , non stato possibile valutare il grado di correlazione tra lettori indipendenti . in conclusione , nella nostra esperienza , i pazienti con epatocarcinomi trattati mediante rfta sviluppano con elevata frequenza nuovi noduli di epatocarcinoma , anche durante il primo anno post - trattamento , solitamente multipli ed in segmenti differenti rispetto al nodulo trattato . 
mci patients showed decreased alff in the right hippocampus and parahippocampal cortex , left lateral temporal cortex and right ventral medial prefrontal cortex and increased alff in the left temporalparietal joint ( tpj ) and inferior parietal lobule . 
the alff value in the right hippocampus and parahippocampal cortex was positively correlated with the scores of mini - mental state exareduced medial temporal lobe activity may implicate the underlying memory impairment mechanisms in mci . 
these findings suggest that alff analysis could provide a useful tool in the fmri study of mci . keywords mild cognitive impairment resting - state functional mri amplitude of low - frequency fluctuation medial temporal lobe compensation riassunto le fluttuazioni spontanee a bassa frequenza dellimaging a risonanza magnetica funzionale ( fmri ) , ottenuto tramite segnale dipendente dal grado di ossigenazione del sangue ( bold ) , hanno dimostrato di rispecchiare lattivit nervosa spontanea . 
lo scopo dello studio stato quello di indagare i cambiamenti funzionali del cervello , in pazienti affetti da deterioramento cognitivo lieve ( mild cognitive impairment , mci ) , attraverso la misurazione dellampiezza dei segnali bold . 
i pazienti con mci hanno presentato una riduzione dellafbf nellippocampo di destra , nella corteccia para - ippocampale , nella corteccia temporale laterale di sinistra e nella corteccia pre - frontale ventro - mediale di destra ; lafbf era aumentata nella giunzione temporoparietale di sinistra ( gtp ) e nel lobo parietale inferiore . 
queste evidenze suggeriscono che lanalisi delle afbf potrebbe 866 radiol med ( 2012 ) 117 : 865871 essere uno strumento molto utile nello studio fmri dei pazienti con mci . parole chiave deterioramento cognitivo lieve rm funzionale resting - state ampiezza delle fluttuazioni a bassa frequenza lobo temporale mediale compensazione introduction mild cognitive impairment ( mci ) is a syndrome with cognitive decline greater than expected for an individuals age and educational level but not interfering notably with activities of daily living [ 1 ]  . 
the amnestic subtype of mci ( amci ) has a high risk of progression to alzheimers disease ( ad ) , constituting a prodromal stage of ad [ 2 ]  . 
therefore , early detection and treatment of amci have become very important at present . structural mri has been primarily used to differentiate between ad and healthy elderly individuals and to predict conversion from mci to ad , relying on volume measurements of the hippocampus and surrounding structures [ 4 ] that are closely related to cognitive decline . 
however , most patients with structural mri abnormalities often have irreversible pathological damage in the bragiven that functional alterations might precede structural abnormalities , blood - oxygenation - level - dependent functional mri ( fmri ) may be a promising technique for studying mci [ 57 ]  . 
studies have reported decreased activity of the mtl in mci [ 10 , 11 ] , or increased activity [ 12 ] or even no significant change [ 13 ]  . 
an alternative way of measuring regional brain activity during resting state is to examine the amplitude of low - frequency fluctuation ( alff ) of the bold signal [ 14 ]  . 
 [ 15 ] reported that the reduced low - frequency fluctuation in white matter relative to grey matter by approximately 60% suggests that alff is associated with field - potential activity in local brain region . 
 in this case , the alff are considered to be the reflection of regional spontaneous neuronal activity [ 16 ] and physiological states of the brain [ 17 ]  . 
 the purpose of this study was to explore the possibility of the altered resting state of brain activity in mci patients using alff analysis and examine possible clinical correlates of alff measurements . materials and methods eighteen amci patients and 20 healthy elderly controls participated in the study . 
 prior to resting - state fmri scanning , examination of each participant included medical history , neurological examination , informant interview , neuropsychological assessment [ including mini - mental state exam ( mmse ) , activity of daily living scale , hachinski ischaemic scale , and hamilton rating scale for depression ] , and structural mri . 
there were no significant differences ( p > 0.05 ) in age ( years ) , sex and education ( years ) between groups amci , deterioramento cognitivo lieve in anamnesi ; mmse , punteggio questionario mini mental state ; cdr , scala clinical dementia rating . * i valori sono rappresentati come mediadeviazione standard : p < 0 , 01 . 
et ( anni ) , sesso ed educazione ( anni ) non erano differenti in modo significativo ( p > 0 , 05 ) tra i due gruppi . from initiating goal - directed , attention - demanding activity . 
 a t2 * - weighted , gradient - recalled echo - planar imaging ( fpi ) sequence was obtained for functional images : echo time , 40 ms ; repetition time , 2 , 000 ms ; slice thickness , 6 mm ; gap , 1 mm ; flip angle , 90 ; field of view , 24 cm ; resolution , 6464 matrix . 
for each participant , functional images were realigned using least - squares minimisation without higher - order corrections for spin history and normalised to the montreal neurological institute ( mni ) template . 
images were resampled to 333 mm3 and smoothed with a 4 - mm full width at half maximum . rest package ( rest , sourceforge . net ) was used to calculate the alff with a voxel - based approach . 
the time courses were first converted to the frequency domain using fast fourier transform ( fft ) , and the power spectrum was obtained by square - rooted fft and averaged across 0.010.08 hz at each voxel . 
to reduce global effects of variability across participants , the alff of each voxel was divided by the global mean alff value within the whole - brain mask obtained previously . 
the global mean alff was calculated only within the brain , with the background and other tissues outside the brain removed . two - sample students t tests were used to assess differences in age , years of education and mmse scores between the two groups using spss 13.0. 
 two statistical results were set : one was a higher alff value ( cluster size > 458 mm3 , p < 0.01 , corrected ) in mci patients compared with healthy controls ; another was a lower alff value ( cluster size > 525 mm3 , p < 0.01 , corrected ) in mci patients compared with healthy controls . 
linear correlations were calculated between mmse scores and mean alff values across all voxels in the abnormal areas in mci patients . results the demographics of mci patients and healthy elderly controls , including age , sex and education years , were matched . 
compared with healthy controls , mci patients showed significantly decreased alff in the right hippocampus ( hc ) , parahippocampal cortex ( phc ) , left lateral temporal cortex ( ltc ) and right ventral medial prefrontal cortex ( vmpfc ) , and increased alff in the left inferior parietal lobule ( ipl ) and left tpj . 
no significant correlations between alff values and mmse scores were found in other above - mentioned brain regions . discussion using resting - state fmri based on alff analysis , we found abnormal spontaneous functional activity during the resting state in mci patients , who showed decreased alff compared with controls in the medial temporal lobe , specifically in hc and phc , and ltc and vmpfc , indicating functional deficiency ; and increased alff compared with controls in the tpj and ipl , suggesting functional compensation . 
mtl , including the hc , phc and entorhinal cortex ( ec ) , is critical for memory function [ 9 ] , which plays an important role in the process of information storage and retrieval , especially for episodic memory retrieval [ 20 ]  . 
significant bilateral hc and underlying ec coactivation was found in both healthy young and elderly people , as well as unilateral mtl coactivation in the mild ad group [ 6 ]  . 
the results in our study are consistent with some ica findings : compared with healthy elderly participants , reduced mtl activity was observed in mci patients with an mmse score 24.773.84. 
our correlation analysis linked alff values in the hc and phc to mmse scores , such that lower alff values in the hc and phc were found in mci fig . 
1 regions showing decreased amplitude lowfrequency fluctuations ( alff ) in mild cognitive impairment ( mci ) patients : a right hippocampus ( hc ) and parahippocampal cortex ( phc ) ; b leftlateral temporal cortex ( ltc ) ; c right ventral medial prefrontal cortex ( vmpfc )  . 
a ippocampo di destra ( hc ) e corteccia para - ippocampale ( phc ) ; b corteccia temporale laterale di sinistra ( ltc ) ; c corteccia pre - frontale ventro - mediale di destra ( vmpfc )  . 
2 regions showing increased amplitude of low - frequency fluctuations ( alff ) in mild cognitive impairment ( mci ) patients : d left temporalparietal joint ( tpj ) ; e left inferior parietal lobule ( ipl )  . 
these findings suggest that altered mtl activation may be associated with levels of memory impairment seen in mci patients , and decreased mtl activity could be an imaging - based biomarker to depict mci . in our study , there was also decreased alff in ltc and vmpfc . 
the vmpfc is assumed to play a general role in emotional processing , such as attention to emotion , identification or regulation of emotion [ 23 ] , and guides motivational behaviour by modulating or appraising autonomic emotional responses [ 24 ]  . 
mci patients showed decreased alff in multiple brain areas , indicating that there might be many other memory - related brain areas with abnormal activities in the resting state . in addition to reduced spontaneous activity , increased activity in the left tpj and ipl was found in mci patients . 
ipl are evoked in working memory and are involved in short - term storage and retrieval of phonology - coded language materials [ 25 ] and are obligatorily or unintentionally engaged in the recall of episodic memory information [ 24 ]  . 
 a previous fmri study indicated that increased activity in the left prefrontal cortex ( pfc ) and ipl is found in amci patients on the basis of ica analysis of resting - state fmri [ 10 ]  . 
increased functional connectivity between prefrontal regions and other brain regions during memory tasks [ 28 ] , as well as between the left hc and right dorsolateral prefrontal cortex during resting states [ 29 ] , was thought to function as compensatory neuronal activity due to cognitive deficits in ad patients . 
therefore , the obviously increased activity might suggest that mci patients could recruit network resources , primarily from tpj and ipl , to maintain memory functions following reduced mtl activity . 
future studies should record simultaneous cardiac rate to deal with this potential confound . in conclusion , the abnormal spontaneous brain activity that is closely related to the episodic memory was found in mci patients . 
although rather simple , alff analysis may provide a useful tool in fmri study of mci . acknowledgements this work was supported by the national natural foundation of china ( grant 30970818 ) and the national high - tech research and development program of china ( 863 program no : 2008aa02z302 )  . 
williams4 1uoc radiodiagnostica e radiologia interventistica , irccs azienda ospedaliera universitaria san martino - ist , monoblocco 1 - f , largo rosanna benzi 10 , 16132 genova , italy 2unit cardio - vascolare radiologica , ospedale giovanni xxiii , via giovanni xxiii 7 , 31050 monastier di treviso ( tv ) , italy 3department of radiology , division of cardiothoracic radiology , university of michigan medical center , 1500 east medical center drive , ann arbor , mi 48109 - 0326 , usa 4department of radiology , division of vascular and interventional radiology , university of michigan medical center , 1500 east medical center drive , ann arbor , mi 48109 - 0326 , usa correspondence to : s . 
in the majority of patients ( 5 / 6 , 83% ) the pseudoaneurysms were multiple and involved the branches of the descending thoracic aorta ( 14 / 22 , 64% ) , mainly the intercostal arteries ( 11 / 22 , 50% )  . 
aortic branch artery pseudoaneurysms associated with imh may be considered a benign disease , as the majority of cases resolved or did not change in size , with haematoma resorption . 
abbiamo incluso 14 pazienti ( 9 maschi ; et media : 64 , 69 , 6 , range : 4275 anni ) con diagnosi in fase acuta di eia di tipo b senza evidenza di lacerazione intimale . 
nella maggior parte dei pazienti ( n = 5 / 6 , 83% ) gli ps erano multipli ed interessavano le branche dellaorta toracica discendente ( n = 14 / 22 , 64% ) , soprattutto le arterie intercostali ( n = 11 / 22 , 50% )  . 
gli ps delle branche arteriose aortiche associati alleia possono essere considerati una patologia benigna , in quanto , nella maggior parte dei casi , vanno incontro a risoluzione o stabilit dimensionale parallelamente al riassorbimento dellematoma . 
tuttavia , abbiamo osservato frequentemente unevoluzione dinamica degli ps nella fase acuta e sub - acuta , per cui si rende 790 radiol med ( 2012 ) 117 : 789803 keywords aortic intramural haematoma acute aortic syndromes aortic disease pseudoaneurysm multidetector computed tomography necessario uno stretto follow - up clinico e mediante imaging . parole chiave ematoma intramurale dellaorta sindromi aortiche acute patologia aortica pseudoaneurisma tomografia computerizzata multidetettore introduction introduzione aortic intramural haematoma ( imh ) is classified among acute aortic syndromes ( aas ) , together with aortic dissection ( ad ) and penetrating atherosclerotic ulcer ( pau )  . 
 imh is classically defined as a haematoma in the aortic wall that is distinguished from classic aortic dissection and haematoma secondary to pau by the absence at imaging of any evident intimal tear [ 14 ]  . 
although the precise aetiology is still uncertain , the most common theory of pathogenesis reported in the literature is spontaneous rupture of the vasa vasorum in the media and intramural haemorrhage formation [ 1 , 2 ]  . 
 [ 7 , 8 ] recorded the presence of small collections of contrast material within the imh in several patients , which can mimic pau but which differ according to anatomical details and pathophysiological characteristics . 
 these collections of contrast material are the sequelae of damage caused by propagation of the haematoma across the origin of aortic branch arteries and , having no wall of their own , they are defined pseudoaneurysms [ 7 , 8 ]  . the aim of this study was to describe according to multidetector computed tomography ( mdct ) imaging the morphological characteristics of aortic branch artery pseudoaneurysms associated with imh and their possible evolution in order to bring this still little known condition to the attention of the radiologist . lematoma intramurale dellaorta ( eia ) rientra nellambito delle sindromi aortiche acute che comprendono anche la dissezione aortica ( da ) e lulcera penetrante aterosclerotica ( upa )  . 
leia stato classicamente definito come un ematoma nel contesto della parete aortica che si distingue dalla dissezione aortica classica e dallematoma secondario allupa per lassenza allimaging di una evidente lacerazione intimale [ 14 ]  . 
sebbene lesatta eziologia sia ancora incerta , lipotesi eziopatogenica pi comunemente riportata in letteratura la rottura spontanea dei vasa vasorum allinterno della tonaca media dellaorta con formazione di unemorragia intramurale [ 1 , 2 ]  . 
 [ 7 , 8 ] hanno documentato la presenza in alcuni pazienti con eia di piccole raccolte di mezzo di contrasto allinterno delleia , le quali possono simulare le upa , ma dalle quali differiscono per dettagli anatomici e caratteristiche fisiopatologiche [ 7 , 8 ]  . 
queste raccolte di mezzo di contrasto rappresentano la sequela del danno dellorigine delle branche aortiche interessate dalla propagazione dellematoma e , non avendo dal punto di vista anatomopatologico una parete propria , vengono definiti pseudoaneurismi ( ps ) [ 7 , 8 ]  . scopo di questo lavoro descrivere le caratteristiche morfologiche alla tomografia computerizzata multidetettore ( tcmd ) degli ps delle branche aortiche associati alleia e la loro possibile evoluzione , al fine di portare , quindi , allattenzione del medico radiologo queste entit ad oggi ancora poco conosciute . materials and methods patients materiali e metodi pazienti between january 2007 and august 2010 , 41 patients with clinical suspicion of aas were diagnosed at mdct with imh . 
of these , 14 patients were retrospectively enrolled nel periodo compreso fra gennaio 2007 e agosto 2010 stata fatta diagnosi alla tcmd di eia in 41 pazienti con sospetto clinico di sindrome aortica acuta . 
all patients underwent mdct and clinical follow - up , including systolic blood pressure control to a target of 110 mmhg and evaluation for the presence of pain or other clinical complications . scan protocol and other diagnostic criteria stati retrospettivamente arruolati 14 pazienti con i seguenti criteri : ( a ) pazienti senza storia pregressa di sindrome aortica acuta ; ( b ) presenza di eia di tipo b secondo stanford o di tipo iii secondo de - bakey ; ( c ) pazienti sottoposti a tcmd ( 16 o 64 strati ) eseguita entro 48 ore dallinizio dei sintomi ; ( d ) presenza di almeno due tcmd per paziente e di un follow - up > 1 mese . 
tutti i pazienti sono stati sottoposti a follow - up mediante tcmd e a follow - up clinico che includeva il controllo della pressione sistolica a valori 110 mmhg e la valutazione della presenza di dolore o altre complicanze cliniche . all mdct examinations were performed with a 16 - slice ( lightspeed 16 ; ge healthcare , milwaukee , wi , usa ) or a 64 - slice ( somatom sensation 64 , siemens , forchheim , germany ) systescans were performed prior to contrast material administration and in the arterial and late phases in the craniocaudal direction from the submandibular region protocollo di scansione e criteri diagnostici tutti gli esami tc sono stati eseguiti con apparecchiature tcmd a 16 - strati ( lightspeed 16 , ge healthcare , milwaukee , wisconsin , usa ) o 64 strati ( somatom sensation 64 , siemens , forcheim , germania )  . 
all patients received 100 ml of iodinated contrast material at a rate of 45 ml / s ( iomeron 400 , bracco , milan , italy ) , followed by a 50 - ml bolus of saline solution at the same injection speed via an antecubital vein in the arscan synchronisation with contrast material passage was achieved with the bolus - tracking technique . 
scan parameters for the 64 - slice mdct system were : detector width 0.6 mm ; gantry rotation time 330 ms ; effective temporal resolution 165 ms ; feed 3.8 mm / rotation ; tube voltage 120 kvp ; tube current 750 mas . 
scan parameters for the 16 - slice system were : detector width 1.25 mm ; gantry rotation time 500 ms ; effective temporal resolution 250 ms ; feed 27.5 mm / rotation ; tube voltage 120 kvp ; tube current 20 - 400 mas . data sets were reconstructed immediately after the scans . 
 axial data were then transferred to a dedicated workstation ( leonardo , siemens , forchheim , germany or advantage windows 4.1 , ge healthcare , milwaukee , wisconsin , usa ) for postprocessing and subsequent evaluation . at the initial mdct performed in the acute phase , the diagnosis of imh was made according to the following criteria [ 24 ] : ( 1 ) presence of a semilunar or circumferential hyperdense area with thickness > 5 mm in the aortic wall with attenuation values ( hu ) greater than those of the aortic lumen in the nonenhanced scan ; ( 2 ) absence of contrast enhancement of the intramural hyperdense area in the contrast - enhanced scan ; ( 3 ) absence of intimal tear with ulcerlike projection ( ulp ) [ 9 ] or direct communication between the true and the false lumen , with formation of a doublebarrelled aorta in the contrast - enhanced scan ; ( 4 ) possible visualisation of the dislocation of subintimal calcification caused by the imh . diagnostic criteria for the presence of pseudoaneurysm in the contrast - enhanced scans were the following [ 7 , 8 ] : ( 1 ) presence of a collection of contrast material in the imh located at the origin of the aortic branch arteries ; ( 2 ) communication between the collection and the affected aortic branch artery ; ( 3 ) possible visualisation of the communication of the collection with the aortic lumen . 
in addition , maximum haematoma thickness and axial diameter of the pseudoaneurysm at initial mdct and at follow - up were measured in all patients using multiplanar reconstructions ( mpr ) perpendicular to the long axis of the aorta . 
the ethics committee approved the study , and all patients provided written informed consent . fase arteriosa e in fase tardiva in senso cranio - caudale dalla regione sottomandibolare fino alla regione inguinale . 
sono stati somministrati 100 ml di mezzo di contrasto iodato alla velocit di 45 ml / s ( iomeron 400 , bracco , milano , italia ) seguiti da un bolo di soluzione fisiologica di 50 ml alla stessa velocit di iniezione attraverso una vena antecubitale del braccio . 
i parametri di scansione sono stati per la tcms a 64 strati : larghezza del rilevatore 0 , 6 mm , periodo di rotazione del tubo 330 ms , risoluzione temporale effettiva 165 ms , avanzamento 3 , 8 mm / rotazione , tensione del tubo kvp 120 , corrente 750 mas ; per la tcms a 16 strati : larghezza del rilevatore 1 , 25 mm , periodo di rotazione del tubo 500 ms , risoluzione temporale effettiva 250 ms , avanzamento 27 , 5 mm / rotazione , tensione del tubo kvp 120 , corrente 20400 ma . i set di dati sono stati ricostruiti immediatamente dopo la scansione . 
i dati assiali venivano poi trasferiti a una stazione di lavoro dedicata ( leonardo , siemens , forchheim , germania o advantage windows 4.1 , ge healthcare , milwaukee , wisconsin , usa ) per il post - processing e per la conseguente valutazione . alla tcmd iniziale in fase acuta la diagnosi delleia stata fatta utilizzando i seguenti criteri [ 24 ] : ( 1 ) presenza di unarea iperdensa semilunare o circonferenziale con spessore > 5 mm nel contesto della parete aortica con valori di attenuazione ( uh ) superiori a quelli del lume aortico nella scansione pre - contrastografica ; ( 2 ) assenza di presa di contrasto dellarea iperdensa intramurale aortica nella scansione contrastografica ; ( 3 ) assenza di lacerazione intimale con estroflessione ulcera - simile del lume ( nella letteratura anglosassone : ulcer - like projection , ulp [ 9 ] ) o di comunicazione diretta fra il vero e il falso lume con formazione di un doppio canale nella scansione contrastografica ; ( 4 ) possibile visualizzazione della dislocazione di calcificazioni subintimali da parte dellematoma allinterno del lume aortico . i criteri diagnostici per la presenza di ps nella scansione contrastografica sono stati i seguenti [ 7 , 8 ] : ( 1 ) presenza di una raccolta di contrasto allinterno delleia localizzata allorigine delle branche aortiche ; ( 2 ) comunicazione della raccolta con la branca aortica interessata ; ( 3 ) possibile visualizzazione della comunicazione della raccolta con il lume aortico . 
inoltre , in tutti i pazienti stato misurato lo spessore massimo dellematoma ed il diametro assiale massimo dello ps alla tcmd iniziale e al follow - up utilizzando ricostruzioni multiplanari ( mpr ) perpendicolari allasse maggiore dellaorta . 
lo studio stato approvato dal comitato etico locale e tutti i pazienti hanno fornito per iscritto il loro consenso informato . statistical analysis analisi statistica categorical variables were described as number and percentage and compared with the chi - squared test , or fishers le variabili categoriche sono state descritte come numero e percentuale e comparate con il test del quadrato o il radiol med ( 2012 ) 117 : 789803 exact test where appropriate . 
considering the progression of mdct findings and the persistence of intermittent chest pain despite optimal medical therapy , both patients underwent endovascular treatment with the deployment of a thoracic endoprosthesis and coverage of the ulp and thoracic pseudoaneurysms . at the last mdct follow - up ( mean 10.6 months ; range 224 months ) , resolution of the imh was observed in all patients ( including the two who underwent endovascular treatment )  . 
abbiamo riscontrato la presen za alla tcmd di 22 ps in 6 pazienti , risultando in una prevalenza del 43% ( n = 6 / 14 ) ; di questi 4 pazienti ( 67% ) avevano eia toraco - addominale e 2 pazienti ( 33% ) aveva no eia toracico . 
complessivamente , il range del diametro assiale massimo degli ps alla tcmd iniziale era di 214 mm , con diametro medio di 5 , 7 mm . al follow - up ravvicinato ( 15 giorni ) mediante tcmd , considerando solo i pazienti con evidenza di ps ( n = 6 ) , abbiamo osservato riduzione dimensionale delleia in 4 pazienti ( n = 4 / 6 , 67% ) e un aumento dimensionale delleia nei restanti 2 pazienti ( n = 2 / 6 , 33% )  . 
complessivamente , 6 ps sono scomparsi , 1 ps rimasto stabile , 3 ps sono andati incontro a riduzione dimensionale , 11 ps sono andati incontro ad un aumento dimensionale ed infine 1 ps comparso al follow - up . 
nei 2 pazienti con aumento delleia ( caso 3 e 5 ) , stata dimostrata inoltre al follow - up ravvicinato , rispettivamente a 3 e a 15 giorni , la presenza a livello dellistmo aortico di una lacerazione focale dellintima ( ulcer - like projection , ulp )  . 
inoltre , in entrambi i pazienti abbiamo osservato lincremento dimensionale degli ps presenti alla tcmd iniziale e in un paziente ( caso 5 ) anche la comparsa di un nuovo ps di un vaso aortico viscerale al follow - up a 15 giorni ( tabella 2 )  . 
considerata la progressione del quadro tcmd e la persistenza di dolore toracico intermittente nonostante la terapia medica ottimale , entrambi i pazienti sono stati sottoposti a trattamento endovascolare mediante posizionamento di endoprotesi toracica con copertura della ulp e degli ps toracici . allultimo follow - up mediante tcmd ( media : 10 , 6 mesi ; range 224 mesi ) , in tutti i pazienti si osservata una risoluzione delleia ( compresi i 2 pazienti trattati per via endovascolare )  . 
inoltre , in un paziente con risoluzione delleia al follow - up a 2 , 5 mesi ( caso 4 ) , stata dimostrata la comparsa di una piccola ulp a livello della794 radiol med ( 2012 ) 117 : 789803 radiol med ( 2012 ) 117 : 789803 796 radiol med ( 2012 ) 117 : 789803 fig . 
a unenhanced mdct axial image shows dislocation of an intimal calcification due to the presence of hyperattenuating intramural fluid collection with circumferential extension into the descending thoracic aorta ( arrow )  . 
b contrast - enhanced mdct axial image at the same level shows the absence of contrast enhancement of the hyperattenuating intramural fluid collection in the descending thoracic aorta ( arrow )  . 
c mdct axial maximum intensity projection ( mip ) reconstruction of a pseudoaneurysm at the right intercostal artery origin at the d9 level ( arrow ) in the context of the thoracoabdominal imh . 
a tcmd assiale senza mezzo di contrasto che dimostra dislocazione di una calcificazione intimale e la presenza di una iperdensit di tipo ematico a livello intramurale dellaorta toracica discendente con estensione circonferenziale ( freccia )  . 
b tcmd assiale con mezzo di contrasto allo stesso livello che evidenzia lassenza di presa di contrasto delliperdensit di tipo ematico a livello intramurale dellaorta toracica discendente ( freccia )  . 
c tcmd con ricostruzione maximum intensity projection ( mip ) assiale di un pseudoaneurisma allorigine dellarteria intercostale destra a livello di d9 ( freccia ) nel contesto delleia toraco - addominale . 
d tcmd con ricostruzione mip coronale che mette in evidenza la presenza di quattro pseudoaneurismi alle origini delle arterie intercostali di destra a livello di d5 , d9 , d10 e d11 , e un altro pseudoaneurisma allorigine dellarteria lombare sinistra a livello di l2 ( frecce ) , nel contesto delleia toraco - addominale . absence of clinical symptoms and the good response to medical therapy , the patient was referred for close follow - up . with regard to the remaining eight patients with imh and no sign of pseudoaneurysm at initial mdct , mean maximum imh thickness was 9.51 mat mean follow - up of 16.97.4 ( range 628 ) months , we observed complete imh orta toracica discendente prossimale e laumento dimensionale dello ps toracico ; considerata lassenza di sintomatologia clinica e la buona complicanza alla terapia medica , il paziente stato rinviato a stretto follow - up . considerando i restanti 8 pazienti con eia senza evidenza di ps alla tcmd iniziale , lo spessore massimo medio delleia risultato essere 9 , 51 mal follow - up medio radiol med ( 2012 ) 117 : 789803 fig . 
b contrastenhanced mdct axial image shows the presence of two pseudoaneurysms of the right and left lumbar artery origins at the l3 level ( arrows ) in the context of the thoracoabdominal imh . 
c contrast - enhanced mdct axial image at 1 month follow - up showing increasing volume of the of two pseudoaneurysms of lumbar artery origins at the l3 level , with confluence of these ( arrows )  . 
b tcmd assiale con mezzo di contrasto che evidenzia la presenza di due pseudoaneurismi , rispettivamente allorigine dellarteria lombare di destra e di sinistra a livello di l3 ( frecce ) nel contesto delleia toracoaddominale . 
c tcmd assiale con mezzo di contrasto a 1 mese che dimostra aumento dimensionale dei due pseudoaneurismi alle origini delle due arterie lombari a livello di l3 con confluenza degli stessi ( frecce )  . 
d tcmd con ricostruzione volume rendering technique ( vrt ) sagittale sinistra che mette in evidenzia gli pseudoaneurismi confluenti allorigine delle arterie lombari a livello di l3 ( freccia )  . resolution in six patients ( 6 / 8 , 75% ) and segmental spindleshaped ectasia of the thoracic aorta in two ( 2 / 8 , 25% )  . di 16 , 97 , 4 ( range 628 mesi ) abbiamo osservato la risoluzione completa delleia in 6 pazienti ( n = 6 / 8 , 75% ) ed ectasia fusiforme segmentale dellaorta toracica in 2 pazienti ( n = 2 / 8 , 25% )  . discussion in the aas setting , imh , ad and pau make up a spectrum of dynamic disorders that may have similar clinical manifestations and at follow - up show a possibly rapid morphological progression from one to the other . 
however , they may have a common pathogenetic mechanism , such as inflammation , susceptibility to ischaemia , expression of matrix metalloproteinase [ 11 ] or medial proliferation with transition of the smooth - muscle cells from the contractile to the synthetic type [ 12 ]  . 
by definition , imh is distinguished from classic ad by the absence of direct communication between discussione nellambito delle sindrome aortiche acute , leia , la da e lupa rappresentano uno spettro di patologie dinamiche che possono avere manifestazioni cliniche simili e mostrare al follow - up unevoluzione morfologica , anche rapida , di unentit verso laltra ; inoltre in uno stesso paziente si possono riscontrare due diverse lesioni contemporaneamente [ 10 ]  . 
la relazione patogenetica tra queste entit a tuttoggi ancora non chiara ; tuttavia , possono avere come meccanismo patogenetico comune linfiammazione , la suscettibilit allischemia , lespressione di metalloproteinasi della matrice [ 11 ] , o fenomeni di proliferazione della tonaca media con trasformazione del fenotipo delle fibrocellule muscolari lisce da quello contrattile a quello sintetizzante 798 radiol med ( 2012 ) 117 : 789803 fig . 
3a multidetector computed tomography ( mdct ) contrast - enhanced axial image of the abdominal aorta ( a ) showing a pseudoaneurysm ( * ) at the inferior mesenteric artery origin ( arrow )  . 
c mdct contrast - enhanced axial image of the abdominal aorta ( a ) at the 3 - month follow - up shows resolution of the pseudoaneurysm at the inferior mesenteric artery origin ( arrow )  . 
d tcmd con ricostruzione vrt coronale che conferma lassenza dello pseudoaneurisma allorigine dellarteria mesenterica inferiore ( freccia )  . true and false lumina with creation of a communicating double - barrel aorta [ 24 ]  . 
pathogenesis has still not been confirmed , although it is widely accepted that the condition arises from spontaneous rupture of the vasa vasorum , which seem to play an important pathogenetic role in all three aas types [ 10 ]  . the presence of aortic branch artery pseudoaneurysms associated with imh has recently been described both in terms of imaging ( mdct and angiography ) and pathology [ 7 , 8 , 13 ]  . 
per definizione , leia si distingue dalla dissezione aortica classica per lassenza di comunicazione diretta tra il vero e il falso lume dellaorta con formazione di un doppio canale comunicante [ 24 ]  . 
leziopatogenesi ad oggi ancora non confermata , ma largamente accettata , la rottura spontanea dei vasa vasorum , i quali sembrano giocare un ruolo patogenetico importante in tutte e tre le sindromi aortiche acute [ 10 ]  . recentemente stata descritta , sia dal punto di vista dellimaging ( tcmd e angiografia ) che anatomo - patologico , la presenza di ps delle branche aortiche nel contesto delleia [ 7 , 8 , 13 ]  . 
as a result , blood flow at the level of the aortic branch proceeds from the true lumen , through the interrupted origin of the aortic branch , within the intramural blood collection and , lastly , within the aortic branch itself . 
this intramural blood collection is defined as a pseudoaneurysm , which by definition is not bounded by the elements of the arterial wall itself but simply confined within the haematoma of the false lumen bounded by the media [ 7 ]  . 
given that the small communication in the intimal - medial flap between the true and false lumen of the imh is only 12 mm in diameter , it may not be visible with 2.5to 5 - mm mdct scans . 
however , with the latest generation mdct systems and the use of thin collimations ( 0.61.2 mm ) , which enables isotropic spatial resolution up to 0.3 mm , in our experience , the small communication in the imh flap can be visualised in most cases . 
the same can be said for small pseudoaneurysms ( < 5 mm ) , which may not be clearly identifiable using a slice thickness > 2.5 mm , with the result that small pseudoaneurysms can be confused with ulp or vice versa [ 5 , 8 ]  . being confined within the imh and not having a wall of their own , aortic branch artery pseudoaneurysms may extend along the circumference of the imh , and they generally tend to have an elongated morphology in axial scans , with a greater width than depth . 
di conseguenza , il flusso ematico a livello della branca aortica procede dal vero lume , attraverso lorigine interrotta della branca aortica , allinterno della raccolta ematica intramurale ed , infine , allinterno della branca aortica stessa . 
questa raccolta ematica intramurale viene definita ps , che , per definizione , non delimitato da elementi propri della parete arteriosa , ma semplicemente confinato allinterno dellematoma del falso lume delimitato dalla tonaca media [ 7 ]  . 
considerato che la piccola comunicazione nel lembo intimo - mediale tra il vero lume e il falso lume delleia di soli 12 mm di diametro , essa pu non essere apprezzabile con scansioni tcmd di 2 , 55 mtuttavia , con le tcmd di ultima generazione e limpiego di collimazioni sottili ( 0 , 61 , 2 mm ) che consentono una risoluzione spaziale isotropica fino a 0 , 3 mm , in molti casi , secondo la nostra esperienza , possibile visualizzare la piccola comunicazione nel lembo delleia . 
lo stesso vale per gli ps di piccole dimensioni ( < 5 mm ) , che possono non essere chiaramente identificati utilizzando spessori di strato > 2 , 5 mm , con il risultato che piccoli ps possono essere confusi con ulps o viceversa [ 5 , 8 ]  . gli ps delle branche aortiche , essendo confinati nelleia e non essendo dotati di parete propria , si possono estendere lungo la circonferenza delleia e , generalmente , tendono ad assumere nelle scansioni assiali una morfolo gia allungata con larghezza maggiore della profondit . 
5a - f cross - sectional images through a normal aorta ( a , adventitia ; m , media ; i , intima ) , b aortic intramural haematoma ( imh ) , c re - entry tear of intramural haematoma ( imh ) tear , d penetrating atherosclerotic ulcer ( pau ) , e branch - artery pseudoaneurysm with complete interruption of artery origin , f branch - artery pseudoaneurysm with partially interrupted artery origgenerally , the pseudoaneurysm has a small orifice on the intimomedial flap , whereas the re - entry tear and the pau has a gaping communication between the aortic true lumen and the collection of contrast media within the haematoma of the medial layer . 
5a - f disegni schematici raffiguranti immagini assiali di a unaorta normale ( a , avventizia ; m , tonaca media ; i , intima ) , b un ematoma intramurale dellaorta ( eia ) , c un sito di rientro delleia , d unulcera penetrante aterosclerotica ( upa ) , e uno pseudoaneurisma di una branca aortica con interruzione completa della sua origine , f uno pseudoaneurisma di una branca aortica con interruzione parziale della sua origine . 
lo pseudoaneurisma ha generalmente un piccolo orifizio nel flap intimo - mediale mentre il sito di rientro delleia e lupa hanno una comunicazione evidente fra il vero lume dellaorta e la raccolta di mezzo di contrasto allinterno dellematoma della tonaca media . 
sebbene la presenza di aterosclerosi avanzata con calcificazioni sub - intimali sia patognomonica per lupa , non possibile stabilire una distinzione basata sullimaging fra sito di rientro dellematoma ed ulcera in quanto non esistono studi di correlazione radiologico - anatomopatologica . tres up to several centimetres , with a possible confluence of pseudoaneurysms arising from aortic branch arteries adjacent to each other . previous studies have documented pseudoaneurysms of intercostal arteries ( even multiple ) , a bronchial artery and a right renal artery [ 7 , 8 , 13 ]  . 
in our series , only eight pseudoaneurysms ( 8 / 22 , 36% ) involved abdominal aortic branch arteries , and of these , only two involved visceral vessels ( 2 / 28 , 25% ; one right renal artery ; one inferior mesenteric artery )  . 
this may be due to the small diameter and wall thickness of the small intercostal , bronchial and lumbar arteries compared with visceral vessels , which makes them more vulnerable to wall damage during imh propagation . 
a recent histopathological study showed that intercostal arteries have a very thin layer of intima and media ( mean values 5438 m and 20538 m , respectively ) and that in most cases the latter is also characterised by multiple elastic lamellae at the origin [ 14 ]  . caudale , da pochi millimetri fino anche a centimetri , con possibile confluenza di ps di branche aortiche adiacenti luno nellaltro . nei precedenti lavori sono stati documentati ps di arterie intercostali ( anche multipli ) , di unarteria bronchiale e di unarteria renale destra [ 7 , 8 , 13 ]  . 
nella nostra casistica , solo 8 ps ( n = 8 / 22 , 36% ) interessavano le branche aortiche addominali e , di questi , solo 2 interessavano i vasi viscerali ( n = 2 / 8 , 25% : n = 1 arteria renale destra ; n = 1 arteria mesenterica inferiore )  . 
 ci pu essere dovuto al minor calibro e spessore parietale delle piccole arterie intercostali , bronchiali e lombari rispetto ai vasi viscerali , che li rende maggiormente vulnerabili al danno parietale durante la propagazione delleia . 
 di interesse un recente lavoro istopatologico che dimostra come le arterie intercostali abbiano uno spessore sottile dellintima e della tonaca media ( valori medi rispettivamente di 5438 microns e di 20538 microns ) , questultima caratterizzata inoltre , nella maggior parte dei casi , da multiple lamelle elastiche allorigine [ 14 ]  . at mean follow - up of 10.68.7 months , we observed inoltre , al follow - up medio di 10 , 68 , 7 mesi abbiamo radiol med ( 2012 ) 117 : 789803 the resolution of both the imh and the pseudoaneurysms in 59% of cases ( 13 / 22 )  . 
in the remaining cases , eight pseudoaneurysms ( 8 / 22 , 36% ) either decreased in size or remained stable despite imh resolution , and one ( 1 / 22 , 5% ) , in an asymptomatic patient , increased in size despite complete imh regression . 
re - entry sites of imh , as with pseudoaneurysms , are secondary to imh and generally located in regions of the aortic wall characterised by high longitudinal stress and not involved by atherosclerotic plaque . 
in the light of these findings , the persistence of intermittent symptoms despite optimal medical therapy and recent guidelines on the treatment of thoracic aortic disease [ 1921 ] , 2 / 3 patients osservato la risoluzione di entrambi leia e gli ps nel 59% dei casi ( n = 13 / 22 )  . 
nei restanti casi , 8 ps ( n = 8 / 22 , 36% ) sono andati incontro a riduzione dimensionale o sono rimasti stabili nonostante la risoluzione delleia , e 1 ps ( n = 1 / 22 , 5% ) andato incontro ad aumento dimensionale nonostante la regressione completa delleia , con paziente asintomatico . 
infatti , curioso , anche se di comune osservazione clinica , che i pazienti con eia o da spesso mostrino una minima aterosclerosi sistemica a confronto dei pazienti che sviluppano lupa , i quali , generalmente di et pi avanzata , sono caratterizzati da una parete aortica spessa e diffusamente fibro - calcifica [ 15 , 16 ]  . 
tuttavia , non possibile una distinzione certa fra i siti di rientro dellematoma e le upa sulla base dellimaging , in quanto non esistono studi di correlazione radiologicoistopatologica [ 8 ]  . nella nostra casistica , al follow - up mediante tcmd , abbiamo riscontrato la presenza di ulps in 3 pazienti con una prevalenza complessiva del 21% ( n = 3 / 14 ) , che comparabile alla prevalenza compresa fra il 15%28% riportata in letteratura nellambito degli eia di tipo - b [ 9 , 16 , 17 ]  . 
 inoltre , abbiamo riscontrato la comparsa della ulp dopo un intervallo medio dallevento acuto di 31 giorni ( range : 3 giorni2 , 5 mesi ) , che sovrapponibile ai valori medi riportati in letteratura ( range valori medi : 17 , 8 giorni2 , 4 mesi ) [ 9 , 16 ]  . 
la storia naturale delle ulps ancora incerta , tuttavia , studi precedenti hanno riportato una progressione di queste lesioni nel contesto delleia di tipo - b in una percentuale di casi non trascurabile , compresa fra il 31% e il 43% : verso la dissezione aortica classica , verso la rottura o verso la dilatazione aneurismatica , anche rapida , dellaorta toracica con necessit di trattamento chirurgico [ 9 , 16 , 17 ]  . 
inoltre , uno studio prognostico condotto in unampia coorte di pazienti con eia di tipo b ( n = 170 ) ha recentemente dimostrato che i pazienti che sviluppano una ulp al follow - up hanno un outcome significativamente sfavorevole rispetto ai pazienti senza evidenza di ulp [ 18 ]  . 
sulla base di queste evidenze , della persistenza di sintomatologia intermittente nonostante la terapia medica ottimale e delle recenti linee guida sul trattamento della patologia dellaorta toracica [ 1921 ] , 2 / 3 pazienti con eia e ulp della with imh and ulp in our series were treated with a thoracic endoprosthesis . nostra casistica sono stati trattati mediante posizionamento di endoprotesi toracica . radiol med ( 2012 ) 117 : 789803 802 limitations limiti our study has several limitations . 
in addition , the absence of a histopathological correlation of the identified aortic lesions ( pseudoaneurysms and ulps ) , especially in the acute phase , is an intrinsic limitation to the study design . 
however , one advantage of our study was the use of a dedicated mdct acquisition protocol with suband paramillimetric collimation , which may have improved sensitivity and specificity in identifying these lesions . il nostro studio presenta alcuni limiti : primo fra tutti , la natura retrospettiva che pu avere portato alla mancata inclusione di alcuni pazienti . 
la diagnosi di eia stata eseguita sulla base dellimaging utilizzando come criterio di esclusione la presenza di lacerazione intimale ( ulp ) , tuttavia , come gi riportato da casistiche chirurgiche , microlacerazioni intimali possono non essere identificate allimaging [ 22 ] ; inoltre , lassenza di correlazione istopatologica delle lesioni aortiche identificate ( ps e ulps ) , specialmente nella fase acuta , una limitazione intrinseca al disegno di questo studio . 
 di conseguenza , si rendono necessari ulteriori studi prospettici pi ampi e a lungo termine che consentano di trarre delle conclusioni sul ruolo degli ps nelle sindromi aortiche acute e sulla storia naturale di queste lesioni . 
tuttavia , uno dei vantaggi del nostro studio stato lutilizzo di protocolli tcmd di acquisizione dedicati con collimazione sube para - millimetrica che pu avere migliorato la sensibilit e la specificit nellidentificazione di queste lesioni . conclusions conclusioni in conclusion , we observed that aortic branch artery pseudoaneurysms associated with imh can be considered a benign condition in that in most cases , they resolve or their size stabilises alongside imh resolution . 
nonetheless , we frequently observed a dynamic evolution of pseudoaneurysms in the acute and subacute phases , thus emphasising the need for close clinical and radiological follow - up . in conclusione , abbiamo osservato che gli ps delle branche aortiche associati alleia possono essere considerati una patologia benigna , in quanto , nella maggior parte dei casi , vanno incontro a risoluzione o stabilit dimensionale parallelamente alla risoluzione delleia . 
tuttavia , abbiamo osservato frequentemente unevoluzione dinamica degli ps nella fase acuta e sub - acuta , per cui si rende necessario uno stretto follow - up clinico e mediante imaging . conflict of interest none radiol med ( 2012 ) 117 : 872884 doi 10.1007 / s11547 - 011 - 0772 - 8 neuroradiology neuroradiologia imaging in congenital deformities of the spinal cord imaging delle malformazioni congenite del midollo spinale g . 
pinto 1 , 71100 foggia , italy 2department of radiology , scientific institute casa sollievo della sofferenza hospital , viale cappuccini 1 , 71013 san giovanni rotondo , foggia , italy 3department of radiology , airlanga university , surabaya , indonesia correspondence to : g . 
pinto 1 , 71100 foggia , italy , tel . / fax : + 39 - 0881 - 733866 , e - mail address : g.guglielmi@unifg.it received : 20 april 2011 / accepted : 10 june 2011 / published online : 7 january 2012 springer - verlag 2012 guarantor of integrity of entire study , g . 
guglielmi study concept , data acquisition , data analysis , manuscript drafting , manuscript editing , manuscript final version approval and literature research , all authors . abstract vertebromedullary malformations are a heterogeneous group of anomalies of mesenchymal and neuroectodermal tissue differentiation or closure in the midline of the back . 
 on the basis of an embryological analysis , the authors describe the more common malformations , placing them at different times of onset and describing the pathological features and radiological findings based on the use of the most appropriate imaging techniques . 
conversely , during the postnatal period , when the patients clinical conditions do not warrant emergency surgical treatment , the disorder can be better defined with a detailed mri scan of the brain and spinal cord . 
in less complex dysraphisms , although mri is the imaging modality of choice , it may be useful to integrate the study with plain radiography ( x - ray ) and multidetector computed tomography ( mdct ) for a better assessment of the skeletal components . 
seguendo un iter di studio condotto sulla guida di una precisa analisi embriologica , gli autori descrivono i quadri malformativi meno rari collocandoli nelle diverse epoche di insorgenza ed associando alla descrizione anatomopatologica una descrizione radiologica attraverso limpiego delle metodiche di studio pi appropriate . 
in epoca postnatale , invece , quando le condizioni cliniche non impongono un trattamento chirurgico in urgenza , il quadro pu essere meglio definito con una rm di dettaglio dellencefalo e del midollo spinale . 
nei disrafismi meno complessi , sebbene la rm rappresenti la metodica di imaging di scelta , si pu utilmente integrare lo studio con la radiologia a raggi x ( rx ) e con la tomografia computerizzata ( tc ) multidetettore per una migliore valutazione delle componenti ossee . 
during the third week of gestation , a process takes place known as gastrulation , during which three germ layers ( ectoderm , mesoderm and endoderm ) arise that will later form all organs and tissues of the human being . 
towards the end of the third week , the lateral margins of the neural plate rise to form the neural folds , and the central region of the neural plate depress to form a groove known as the neural groove . 
 this structure will give rise to the central nervous syste primary neurulation is completed with full closure of the neural tube , which occurs on the 27th day of gestation [ 3 ]  . 
nel corso della terza settimana di gestazione ha luogo un processo noto come gastrulazione , durante il quale originano i tre foglietti germinali ( ectoderma , mesoderma e endoderma ) , da cui successivamente si formeranno tutti gli organi e i tessuti dellessere umano . 
verso la fine della 3a settimana i margini laterali della placca neurale si sollevano a formare le pieghe neurali , mentre la regione centrale si introflette a formare un solco , noto come solco neurale . 
la neurulazione secondaria si concretizza allestremit caudale del tubo neurale primario , come risultato di un processo di differenziazione retrograda , che porta alla formazione delle porzioni caudali del midollo spinale ( cono midollare e filum terminale ) [ 4 ]  . 
la formazione del midollo spinale attribuibile , quindi , in gran parte alla neurulazione primaria mentre solo piccole porzioni del tubo neurale e del sacro - coccige si sviluppano dalla neurulazione secondaria . 
successivamente , la met inferiore di unemivertebra ( emisclerotomo ) si fonde con la met superiore di quella sottostante realizzando il corpo vertebrale . there are different classifications of spinal malformations . 
among dysraphic disorders are open spinal dysraphisms , in which the nervous tissue is exposed to the external environment , and closed spinal dysraphisms , in which there is an intact layer of skin that covers the nervous tissue . 
il termine disrafismo in passato era riservato solo ai difetti di chiusura del tubo neurale , ma con luso nel corso del tempo diventato sinonimo di malformazione vertebro - midollare . 
in questambito si distinguono i disrafismi spinali aperti , in cui 874 radiol med ( 2012 ) 117 : 872884 table 1 our classification divides spinal anomalies into dysraphic and nondysraphic malformations . 
because of different embryogenesis , vertebral - body anomalies are classified as a distinct group dysraphic spinal malformations nondysraphic spinal malformations tabella 1 la nostra classificazione divide le anomalie spinali in : malformazioni spinali disrafiche e malformazioni spinali non disrafiche . 
a causa della differente embriogenesi , le anomalie dei corpi vertebrali saranno collocate in un gruppo a parte spina bifida aperta myelocele myelomeningocele myelomeningocystocele spina bifida occulta meningocele spinal lipoma lipomyelomeningocele fibromatosis of the filum terminale tethered cord diastematomyelia dorsal dermal sinus malformazioni spinali disrafiche spina bifida aperta mielocele mielomeningocele mielomeningocistocele spina bifida occulta meningocele lipoma spinale lipomielomeningocele fibromatosi del filum terminale midollo ancorato diastematomielia seno dermico dorsale partial / complete agenesis of sacrum congenital tumours spinal cysts arnold chiari malformation syringomyelia congenital stenosis of the spinal canal vertebral body abnormalities failure of formation anterior central defect incarcerated hemivertebra free hemivertebra wedge vertebra multiple hemivertebrae failure of segmentation unilateral unsegmented bar block vertebra malformazioni spinali non disrafiche parziale / totale agenesia del sacro tumori congeniti cisti spinali malformazione di arnold chiari siringomielia stenosi congenita del canale spinale anomalie dei corpi vertebrali difetto di formazione difetto centrale anteriore emivertebra incarcerata emivertebra libera vertebra a cuneo emivertebre multiple difetto di segmentazione barra non segmentata unilaterale vertebre a blocco myelocele and myelomeningocele , which are not described in this article . dysraphic spinal malformations : closed spinal dysraphisms meningocele the classic posterior meningocele is a condition characterised by herniation of dura and arachnoid meninges through a cleft of the posterior vertebral arches . 
i disrafismi spinali aperti pi frequenti sono il mielocele ed il mielomeningocele che non saranno presi in considerazione in questo articolo . malformazioni spinali disrafiche : disrafismi spinali occulti meningocele il classico meningocele posteriore una patologia caratterizzata da unerniazione delle meningi , dura madre e radiol med ( 2012 ) 117 : 872884 fig . 
the thin wall of this diverticulum consists of an outer layer of dura mater and an inner layer of arachnoid and is in communication with the intraspinal thecal sac [ 6 ]  . imaging ultrasound is sufficient to evaluate the anechoic and typically fluid content of meningocele . 
on magnetic resonance imaging ( mri ) , meningocele appears hypointense in fluidattenuated inversion recovery ( flair ) and spin - echo ( se ) or fast spin - echo ( fse ) t1 - weighted images and hyperintense in fse t2 - weighted images . 
sometimes there may be roots in the wall of meningocele , a highly important finding surgical planning . in anterior sacral meningocele , the imaging modality of choice is mri : it recognises a unior multilocular fluid collection in the pelvis , which is isoechoic on ultrasound ( us )  . 
 also in this case , for surgical planning , it is essential to detect the possible presence of roots in the wall through axial aracnoide , che protrude attraverso una schisi degli archi posteriori vertebrali . 
la sottile parete di tale diverticolo composta da uno strato esterno rappresentato dalla dura madre e da uno interno rappresentato dallaracnoide ed in comunicazione con il sacco tecale intraspinale [ 6 ]  . 
in risonanza magnetica ( rm ) il meningocele si presenta ipointenso nelle immagini spin echo ( se ) o fast spin echo ( fse ) t1 dipendenti e fluid attenuated inversion recovery ( flair ) e iperintenso nelle fse t2 . 
evaluation with the patient in the prone position allows assessment of possible adhesions or spinal cord anchorage . lipomas these are benign tumours composed of a distinct collection of fat and connective tissue , at least partially encapsulated , with a definite connection with the spinal cord . 
the sites most affected by this type of abnormality are cervical , dorsal and the terminal filu meningocele il cui rilievo molto importante per il plaining operatorio . nel meningocele sacrale anteriore la metodica di scelta la rm : in essa si riconosce una raccolta fluida in sede pelvica , unio multiloculata , isointensa allecografia . 
per la valutazione di anomalie ossee in alcuni casi pu essere indicato uno studio con tomografia computerizzata ( tc )  . nella valutazione della fase postoperatoria , lo studio diagnostico di scelta la rm per valutare eventuali aderenze con ancoraggio midollare in ricorso a sequenze in posizione prona . lipomi sono tumori benigni costituiti da una raccolta distinta di grasso e tessuto connettivo , almeno parzialmente capsulata , con una ben definita connessione con il midollo spinale . 
large expansile mass with signal hyperintensity in t2 - weighted images , and homogeneously hypointense in sequences with fat suppression , adhering to the dorsal surface of the spinal cord , on which it exerts a mass effect . 
 voluminosa neoformazione espansiva iperintensa nelle sequenze t2 - pesate ed omogeneamente ipointensa nelle sequenze con soppressione del grasso , adesa alla superficie dorsale del midollo spinale su cui esercita un effetto massa . 
luso di sequenze di soppressione del grasso consente di riconoscere i lipomi come focolai di assenza di segnale ; tali sequenze appaiono utili anche nella definizione del placode allinterfaccia con il lipoma . 
nella forma totale , il midollo spinale formato da due o pi parti simmetriche o asimmetriche , ciascuna contenente uno strato interno ependimale , un corno posteriore con una radice dorsale e un corno anteriore con una radice ventrale . 
nella regione toracica inferiore , evidente un disrafismo complesso caratterizzato da un ampia breccia ossea con erniazione dorsale di parte del sacco durale con liquor e meningi cui si associa presenza di emicorde . imaging the imaging modality of choice is mri . 
the use of fat suppression allows lipomas to be recognised as an area of no signal ; these sequences appear to be useful in defining placode at its interface with lipoma . 
in total diastematomyelia , the spinal cord is formed of two or more symmetrical or asymmetrical portions , each containing an inner ependymal layer , a posterior horn with a dorsal root and an anterior horn with a ventral root . 
in the partial form , only the front or back half of the spinal cord is affected ; such cases are often associated with total diastematomyelia in the segment imlo studio radiografico convenzionale pu essere utile per valutare lallargamento del diametro trasverso del canale vertebrale , le anomalie di segmentazione vertebrale , la fusione delle lamine ai due livelli adiacenti e lo sperone osseo al centro del canale . 
la rm consente di valutare la sede e lestensione della diatematomielia , il carattere unio multifocale , se appartiene al tipo i o al tipo ii , la posizione del cono terminale e delle radici della cauda equina in rapporto alla diatematomielia e leventuale coemediately above or below . 
classification is based on this distinction . 878 imaging conventional radiography may be useful for evaluating enlargement of the transverse diameter of the spinal canal , abnormalities of vertebral segmentation , fusion of laminae at two adjacent levels and the bony spur in the middle of the canal . 
mri allows evaluation of diastematomyelia location and extent , its unior multifocal character , whether it is type i or type ii , position of the terminal cone and roots of the cauda equina in relation to diastematomyelia and the possible coexistence of other malformations or complications ( scoliosis , spinal cord suffering , intramedullary cavity )  . 
to demonstrate the fibrocartilaginous septum ( for which ct is the gold standard ) , fse t2 - weighted and gradient echo ( ge ) t2 * sequences and myelographic acquisitions ( myelo - mri ) both in single partitions and in maximum intensity projection ( mip ) [ 12 ] are useful . 
in the case of anchoring an evaluation of cerebrospinal fluid , flow dynamics may be helpful ( cine mri )  . dorsal dermal sinus if the superficial ectoderm fails to separate from the neural ectoderm , a focal segmental adhesion arises . 
a lumbar dorsal dermal sinus is frequently associated with tethered cord , dermoid or epidermoid tumours or lipoma . imaging x - ray study is useful to exclude associated bony malformations . 
this should be performed with conventional technique and short tau inversion recovery ( stir ) sequence to highlight the intramural dermal sinus , dermoid tumours and lipomas [ 14 ]  . 
the use of contrast material is helpful when there is suspicion of associated infections . radiol med ( 2012 ) 117 : 872884 sistenza di malformazioni associate o di altre complicazioni ( scoliosi , sofferenza midollare , cavit intramidollari )  . 
per la dimostrazione del setto fibro - cartilagineo ( gold standard la tc ) , sono utili le sequenze fse t2 - pesata e ge t2 * e le acquisizioni mielografiche ( mielo - rm ) sia nelle singole partizioni sia nelle ricostruzioni in proiezione di massima intensit ( mip ) [ 12 ]  . 
in caso di ancoraggio pu essere utile una valutazione della dinamica del flusso liquorale ( cine - rm )  . seno dermico dorsale se lectoderma superficiale non riesce a separarsi da quello neurale , si crea unadesione focale segmentale . 
la breccia cutanea del seno dermico si apre al di sopra della linea interglutea e di solito circondata da un nevo angiomatoso o da radi e sottili peli [ 13 ]  . 
la metodica di scelta la rm da eseguire con tecnica convenzionale e sequenza short - tau inversion recovery ( stir ) per evidenziare il seno dermico intramurale , tumori dermoidi e lipomi [ 14 ]  . 
il tipo i comprende le cisti extradurali senza le radici nervose spinali , il tipo ii comprende le cisti extradurali con le radici nervose spinali , mentre il radiol med ( 2012 ) 117 : 872884 tipo iii rappresentato dalle cisti intramurali [ 15 ]  . 
per tale motivo , possibile visualizzare solo quelli di maggiori dimensioni per leffetto massa che esercitano sul canale e sul midollo spinale . tumori congeniti sono tumori mesenchimali o tumor - like lesions . 
presence of a fibrous adhesion with craniocaudal oblique course that ends on the skin at the level of l3l4 and heads anteriorly to the spinal canal , where it connects with the thickened filum terminale . 
presenza di tragitto fibroso a decorso obliquo cranio - caudale , con estremit cutanea a livello di l3 - l4 , che si dirige anteriormente fino al canale rachideo , ove si connette con il filum terminale ispessito . 
generally , these cysts are observed as occasional incidental findings in the form of multiple lesions , but sometimes they are associated with radiculopathy or incontinence [ 16 ]  . 
these cysts are lined by a single layer of normal arachnoid cells containing cerebrospinal fluid . 880 imaging cysts have a similar mri signal intensity to that of cerebrospinal fluid , so only large cysts can be visualised because of their mass effect on the spinal canal and spinal cord . congenital tumours congenital tumours are spinal mesenchymal tumours or tumour - like lesions , most likely formed in the early weeks of foetal life , even though the symptoms appear only after several decades of life . 
in group 2 , spinal dysgenesis is less severe , with tapered spinal cord that ends lower , below l1 [ 14 ]  . radiol med ( 2012 ) 117 : 872884 fig . 
nel gruppo 1 , la disgenesia caudale pi grave e il midollo spinale assume la conformazione di una clava che termina in posizione cefalica rispetto alla limitante inferiore di l1 . 
nel gruppo 2 , la disgenesia spinale meno grave e si presenta con midollo spinale affusolato che termina pi in basso , al di sotto di l1 [ 14 ]  . imaging le radiografie convenzionali documentano lentit del deficit osseo . 
 mdct and us are useful for establishing the extent of soft tissue involvement [ 20 ]  . anomalies of vertebral bodies congenital absence of vertebrae is a malformation that has an extreme severity and high variability . 
agenesis usually affects the lower spinal segments ( sacrum and coccyx ) ; more rarely , there may be involvement of the higher segments with lumbo - sacro - coccygeal agenesis and exceptionally dorso - lumbo - sacro - coccygeal agenesis [ 21 ]  . 
there are different types of hemivertebra : segmented ( nonincarcerated ) , t1 e t2 - pesate evidenziano lestensione del difetto lombosacrale , la morfologia del midollo spinale distale e la presenza di ancoramento . 
metodiche come tc ed ecografia sono utili per spiegare lestensione del coinvolgimento dei tessuti molli [ 20 ]  . anomalie dei corpi vertebrali lassenza congenita delle vertebre una malformazione che riveste carattere di estrema gravit e di grande variabilit . 
lagenesia interessa abitualmente i segmenti vertebrali inferiori ( sacro e coccige ) ; assai pi raramente possono essere colpiti anche i segmenti superiori con agenesia lombo - sacro - coccigea ed eccezionalmente dorso - lombo - sacro - coccigea [ 21 ]  . 
il difetto di formazione causa dellipoplasia di una o pi vertebre , della vertebra trapezoidale o dellemivertebra a forma di cuneo , della vertebra con difetto centrale anteriore , dellemivertebra incarcerata , dellemivertebra libera e delle emivertebre multiple . 
rarely , there may be an irregular distribution , with affected vertebrae interposed between normal ones . imaging lanomalia pi comune e severa rappresentata dallemivertebra segmentata , in cui gli spazi discali superiore ed inferiore sono sviluppati normalmente . 
raramente , pu essere presente una distribuzione irregolare , con vertebre affette intercalate a vertebre normali . conventional radiography is useful for documenting bony anomalies , but in our experience , mdct with multiplanar reconstructions ( mpr ) , 3d volume rendering and bony window represents the modality of choice for evaluating structural anomalies . 
mri can be helpful to assess possible involvement of the spinal cord and soft tissues . imaging le radiografie convenzionali sono utili per documentare le anomalie ossee , ma la metodica di scelta , nella nostra esperienza , la tc multidetettore con ricostruzioni multiplanaradiol med ( 2012 ) 117 : 872884 fig . 
la rm pu essere utile per valutare leventuale coinvolgimento del midollo spinale e dei tessuti molli . conclusioni conclusions congenital spinal abnormalities arise during embryogenesis and include dysraphic and nondysraphic spinal malformations and deformity of the vertebral body . 
plain radiography , mdct and mri can demonstrate these malformations , but as each technique has its own peculiarity , an integrated imaging approach is recommended to evaluate the different aspects of these disorders . le anomalie congenite spinali si verificano durante lembriogenesi e comprendono le malformazioni disrafiche , non disrafiche e le anomalie dei corpi vertebrali . 
knauth springer - verlag berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 540 - 85380 - 0 e - isbn : 978 - 3 - 540 - 85381 - 7 published online : 21 october 2011 springer - verlag 2011 this book follows a previous one in the same series dedicated to acute and chronic diseases of the pancreas and their complications , targeting the more severe and devastating pancreatic adenocarcinoma . once again , italian researchers and the group of international researchers / clinicians ( all well known and respected experts ) under the wise supervision of the editor , prof . 
 the main target of the book is to provide the reader with updated data and knowledge on the latest advances not only in the therapeutic but also in the diagnostic field , when you have to deal with this life - threatening and insidious disease , which remains associated with a very poor prognosis for the patient ( about 80% of pancreatic adenocarcinomas are inoperable at the time of diagnosis ! )  . questo volume fa seguito ad uno precedente , nella stessa serie , dedicato alle malattie acute e croniche del pancreas ed alle loro complicanze , avendo come oggetto il pi grave e devastante adenocarcinoma pancreatico . come nel precedente , anche in questo volume sono da lodare per i loro contributi i ricercatori italiani ed il gruppo di esperti internazionali , autorit ben riconosciute ed apprezzate in questo campo , sotto la saggia supervisione del coordinatore , prof . 
laghi. obiettivo principale del volume quello di fornire al lettore dati ed elementi cognitivi quanto pi aggiornati possibile sui pi recenti progressi , non solo nel campo terapeutico , ma anche in quello diagnostico , quando ci si debba confrontare con questa malattia insidiosa e minacciosa per la vita , associata ad una prognosi molto povera per il paziente ( circa l80% infatti degli adenocarcinomi pancreatici sono inoperabili al momento della diagnosi ! )  . 
 il volume strutturato in 13 capitoli divisi in 3 parti per the book is structured into 13 chapters divided into 3 un totale di 173 pagine , cui si aggiunge lindice . parts for a total of 173 pages , plus the index . the first part offers new insights on epidemiology , risk factors , clinical aspects and pathology , plus information on the genetics of the disease . 
the second part deals with detailed advances in the diagnostic tools and how to choose the most appropriate one to properly diagnose the disease : ultrasound , multidetector - row computed tomography , magnetic resonance imaging ( mri ) , endoscopic ultrasonography , positron emission tomography ( pet ) / computed tomography ( ct ) ending with a cost decision analysis for diagnosing and staging . 
the third and last part is devoted to therapy : when to recommend surgery , how to manage locally advanced nonmetastatic or apply systemic therapy in metastatic cancer , which is the role of interventional enla prima parte offre informazioni sullepidemiologia , i fattori di rischio , gli aspetti clinici e patologici , nonch informazioni sulla genetica della malattia . 
la seconda parte dedicata alla descrizione dettagliata sui progressi della diagnostica strumentale e sul modo di scegliere con appropriatezza il pi indicato di questi strumenti per porre la diagnosi corretta : ecografia , tomografia computerizzata ( tc ) multidetettore , risonanza magnetica ( rm ) , ecografia endoscopica , tomografia ad emissione di positroni ( pet ) / tomo grafia computerizzata ( tc ) per terminare con unanalisi sulla decisione sui costi della diagnosi e della stadiazione . 
 la terza ed ultima parte dedicata alla terapia : come e quando raccomandare lintervento chirurgico , come trattare la malattia in fase avanzata , ma non metastatizzata , o come utilizzare terapie sistemiche nel cancro metastatizzato ; quale sia il ruolo dellendoscopia interventistica , descriradiol med ( 2012 ) 117 : 892893 doscopy and it describes local ablative techniques in the treatment of locally advanced cancer . 
 as it is the case for patients affected by acute or chronic pancreatitis , those affected by pancreatic adenocarcinoma will benefit most from cooperative multi - expert teams and a multi - faceted approach is widely described and stressed all throughout the book . 
anyway , the reader has the uncomfortable feeling that despite continuous efforts and the subsequent diagnostic and therapeutic improvements , the final result for the patient is unfortunately not optimistic . the images are well chosen and reproduced , with the exception of some of the mri images . 
it should be a useful , complementary companion to the previous one on acute and chronic pancreatic disease . vendo le tecniche di ablazione nel trattamento del tumore localmente avanzato . come gi sottolineato per i pazienti affetti da pacreatite acuta o cronica , anche quelli portatori di un adenocarcinoma trarranno migliore beneficio se trattati in collaborazione da gruppi di molteplici esperti cos come un approccio pluri - specialistico viene ampiamente discusso ed evidenziato in tutto il volume . 
il lettore ha per la spiacevole sensazione che , malgrado i continui sforzi diagnostici e terapeutici ed i conseguenti miglioramenti , il risultato finale per il paziente sia sfortunatamente non ottimistico . 
cademartiri1 , 2 1unit cardio - vascolare radiologica , ospedale giovanni xxiii , monastier di treviso ( tv ) , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia , universit di torino , italy 4dipartimento di radiologia , universit di genova , italy 5dipartimento di radiologia , universit di ferrara , italy 6dipartimento di radiologia , universit di palermo , italy 7dipartimento di radiologia , universit di messina , italy 8dipartimento di radiologia , fondazione sdn - irccs , napoli , italy 9dipartimento di cardiologia , azienda ospedaliero - universitaria di parma , italy correspondence to : f . 
cademartiri , unit cardio - vascolare radiologica , ospedale giovanni xxiii , via giovanni xxiii 1 , 31050 monastier di treviso ( tv ) , italy , tel . : + 39 - 0422 - 8961 , fax : + 39 - 0422 - 898051 , e - mail : filippocademartiri@gmail.com received : 19 march 2011 / accepted : 6 june 2011 / published online : 18 november 2011 springer - verlag 2011 abstract purpose . 
the authors evaluated the diagnostic accuracy of second - generation dual - source ( dsct ) computed tomography coronary angiography ( ctca ) with iterative reconstructions for detecting obstructive coronary artery disease ( cad )  . 
for the ctca scan ( definition flash , siemens ) , we use prospective tube current modulation and 70100 ml of iodinated contrast material ( iomeprol 400 mgi / ml , bracco )  . 
scopo del presente lavoro stato valutare laccuratezza diagnostica dellangiografia coronarica non invasiva con tomografia computerizzata ( ctca ) a doppia sorgente ( dsct ) di seconda generazione ( 6422 strati ) con ricostruzioni iterative , nellindividuazione della malattia coronarica ( cad ) ostruttiva . 
tra giugno 2010 e febbraio 2011 sono stati arruolati nello studio 160 pazienti ( 85 maschi , et media 61 , 211 , 6 anni ) con sospetta malattia coronarica . 
 the excellent negative predictive value and likelihood ratio make ctca a first - line noninvasive method for diagnosing obstructive cad . keywords computed tomography coronary angiography iterative reconstructions diagnostic accuracy dualsource computed tomography conventional coronary angiography coronary artery disease clinical value di malattia dimostrata alla cag era del 30% ( 48 / 160 )  . 
 sensibilit , specificit , valore predittivo positivo e negativo della ctca nella determinazione delle stenosi significative sono risultate del 90 , 1% , 93 , 3% , 53 , 2% , 99 , 1% ( per segmento ) ; 97 , 5% , 91 , 2% , 61 , 4% , 99 , 6% ( per vaso ) ; e 100% , 83% , 71 , 6% , 100% ( per paziente )  . 
i valori ottimali di valore predittivo negativo ed i likelihood ratio collocano la ctca tra le metodiche non invasive di prima istanza per la diagnosi di cad ostruttiva . parole chiave angiografia coronarica mediante tomografia computerizzata ricostruzioni iterative accuratezza diagnostica tomografia computerizzata a doppia sorgente malattia coronarica valore clinico introduction introduzione computed tomography coronary angiography ( ctca ) has become a part of clinical practice for diagnosing obstructive coronary artery disease ( cad ) [ 18 ]  . 
guidelines and international panels recommend using ctca in patient populations at low to intermediate risk , where stress tests are inconclusive or cannot be performed [ 8 , 2022 ]  . the introduction of new technologies with improved temporal , spatial and contrast resolution , such as the second - generation dual - source computed tomography ( dsct ) , offers the possibility of making the technique more reliable and robust . 
gli studi che fino ad ora hanno dimostrato laccuratezza diagnostica della ctca a 64 strati hanno utilizzato in prevalenza metodologie di validazione ( ossia con la coronarografia convenzionale , cag , come standard di riferimento ed in popolazione a rischio elevato ) [ 37 , 918 ]  . 
le correnti linee guida ed i panel internazionali raccomandano lutilizzo della ctca in popolazioni di pazienti a rischio basso - intermedio con test provocativi dubbi o non eseguibili [ 8 , 2022 ]  . lintroduzione di nuove tecnologie con migliore riso luzione temporale , spaziale e di contrasto , come ad esempio la seconda generazione di apparecchiature a doppia sorgente ( dsct ) , consente di rendere pi affidabile e robusta la metodica . 
inoltre , la recente introduzione di algoritmi di ricostruzione iterativa consente un miglio ramento della qualit di immagine che consiste nelle significativa riduzione del rumore dellimmagine [ 19 ]  . 
only patients with sinus rhythm who had never undergone percutaneous angioplasty or coronary artery bypass graft surgery and were able to maintain a breath - hold for at least 5 s were included . 
patients with acute coronary syndrome , with absolute contraindications to intravenous administration of iodinated contrast material ( e.g. , known allergy , kidney failure or thyroid disorders ) were excluded . 
the ethics committee approved the study , and all patients provided informed consent . patient preparation patients with a heart rate ( hr ) > 60 bpm and without specific contraindications received a 5 - mg intravenous dose of betablockers ( atenolol , tenormin , astrazeneca )  . 
 ctca scan protocol and image reconstruction the study was performed with a dsct system with 128 ( 6422 ) slices ( definition flash , siemens , forchheim , germany ) [ 4 , 5 ]  . 
images were reconstructed with the following parameters : effective slice thickness 3 mm ; reconstruction increment 1.5 mm ; field of view ( fov ) 150160 mm ; convolution kernel for calcium score ( b35f )  . 
solo i pazienti con ritmo sinusale , mai sottoposti ad angioplastica percutanea o ad intervento chirurgico per il posizionamento di by - pass e capaci di trattenere il respiro per almeno 5 secondi , sono stati inclusi nello studio . 
i pazienti con sindrome coronarica acuta , quelli nei quali esistevano delle controindicazioni assolute alla somministrazione endovenosa di mezzo di contrasto iodato ( per esempio , allergia nota , insufficienza renale o disordini tiroidei ) sono stati esclusi dallo studio . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . preparazione del paziente ai pazienti con una frequenza cardiaca ( fc ) superiore a 60 battiti per minuto ( bpm ) e senza specifiche controindicazioni stata somministrata per via endovenosa una fiala di beta - bloccante ( atenololo , tenormin , astrazeneca , italia ) da 5 mg . 
inoltre , in assenza di contro - indicazioni , pochi minuti prima della scansione stato somministrato del nitrato sublinguale ( isosorbide dinitrato , carvasin 5 mg , wyeth lederle , usa )  . 
 protocollo di scansione ctca e ricostruzione delle immagini per lo studio mediante tomografia computerizzata ( tc ) stato utilizzato uno scanner a doppia sorgente con 128 ( 6422 ) strati ( definition flash , siemens , forchheim , germania ) [ 4 , 5 ]  . 
le immagini sono state ricostruite con i seguenti parametri : spessore di strato effettivo 3mm , incremento di ricostruzione 1 , 5 mm , campo di vista ( fov ) 150160 mm , filtro di convoluzione dedicato per il calcium score ( b35f ) ; 728 radiol med ( 2012 ) 117 : 725738 fig . 
mean dose - length product was 517153 , which corresponds to an effective dose ( conversion factor 0.014 msvmgy - 1cm - 1 for the chest ) of 7.22.1 msv [ 7 ]  . 
 between 70 ml and 100 ml of iodinated contrast material ( iomeprol , iomeron 400 , bracco , milan , italy ) was administered at an injection rate of 56 ml / s using an automatic injector ( stellant , medrad , pittsburgh , pa , usa ) attached to an 18to 20 - gauge needle cannula positioned in an antecubital vein [ 5 ]  . coronary artery enhancement was optimised by using the bolus - tracking technique ( care bolus , siemens , forchheim , germany ) to synchronise contrast material arrival in coronary arteries with the beginning of the scan [ 5 , 23 ]  . 
 retrospective reconstructions based on the ecg signal were done on the angiography scans to obtain images free from motion artefacts in the maximum - dose time window ( 6580% of the rr interval )  . 
il dose length product ( dlp ) medio delle scansioni stato di 517153 corrispondente ad una dose efficace ( fattore di conversione 0 , 014 msvmgy - 1cm - 1 per il torace ) di 7 , 22 , 1 msv [ 7 ]  . 
sono stati somministrati 70100 ml di mezzo di contrasto iodato ( iomeprol , iomeron 400 , bracco , milano ) alla velocit di 56 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unago - cannula da 1820 gauge preventivamente posizionata in una vena antecubitale [ 5 ]  . allo scopo di ottimizzare lopacizzazione dei vasi arteriosi coronarici , stata utilizzata la tecnica del bolus - tracking ( care bolus , siemens , forchheim , germania ) per sincronizzare larrivo del mezzo di contrasto nelle arterie radiol med ( 2012 ) 117 : 725738 field and who were unaware of cca findings . 
all conventional visualisation techniques were used by the operator ( axial images , multiplanar images , curved multiplanar images , maximum intensity projection , volume rendering ) on a dedicated workstation with a cardiology software platform ( syngovia , siemens , germany )  . 
segments were classified as being without significant stenosis ( normal or with wall irregularities or stenosis < 50% ) or with significant stenosis ( stenosis 50% ) using the commonly applied classifications [ 3 , 6 , 7 ]  . conventional coronary angiography cca was performed within 2 weeks of the ctca examination using a conventional technique . 
the operator was aware of data from the ctca report and images and identified coronary artery segments using the modified american heart association ( aha ) 17 - segment classification [ 24 ]  . 
segments were classified as being without significant stenosis ( normal or with wall irregularities or noncritical stenosis < 70% ) or with significant stenosis ( critical stenosis 70% ; in the left main coronary artery 50% ) using the conventional classifications and guidelines . 
accuracy was then calculated as sensitivity , specificity and positive and negative predictive values ( ppv and npv ) , with 95% confidence intervals ( ci ) calculated with binomial expansion . 
sulla scansione angiografica sono state effettuate delle ricostruzioni retrospettive basate sul segnale elettrocardiografico ( ecg ) per ottenere una qualit dellimmagine priva di artefatti da movimento nella finestra temporale di dose massima ( 65%80% dellintervallo rr )  . 
quando ritenuto necessario ( per esempio , in caso di persistente movimento cardiaco residuo che riduce la qualit diagnostica dellimmagine ) sono state analizzate altre ricostruzioni in differenti finestre temporali di ricostruzioni del ciclo cardiaco . 
 valutazione dellimmagine di ctca tutte le scansioni ctca sono state analizzate da due osservatori in consenso con 10 e 5 anni di esperienza nel settore , non a conoscenza dei risultati della cag . 
tutte le modalit convenzionali di visualizzazione sono state utilizzate dalloperatore ( assiali , multiplanari , curvate multiplanari [ mip ] , volume rendering [ vr ] ) su una workstation dedicata con piattaforma software cardiologica ( syngovia , siemens , germania )  . 
i segmenti sono stati classificati come senza stenosi significative ( normali o con irregolarit della parete o con stenosi < 50% ) o con stenosi significativa ( stenosi 50% ) , utilizzando le classificazioni comunemente applicate [ 3 , 6 , 7 ]  . coronarografia convenzionale ( cag ) la cag stata eseguita entro 2 settimane dalla ctca con tecnica convenzionale . 
i segmenti sono stati classificati come senza stenosi significative ( normali o con irregolarit della parete o con stenosi non critica < 70% ) o con stenosi significative ( stenosi critica 70% ; nel caso del tronco comune 50% ) , utilizzando le classificazioni convenzionali e linee guida . 
cad and caa disetable 1 description of the study population radiol med ( 2012 ) 117 : 725738 analisi statistica la performance diagnostica della ctca stata valutata confrontando i referti archiviati nel sistema informatico dellospedale per la ctca e per la cag , rispettivamente . 
per la ctca il tempo medio di refertazione stato di 10 min mentre per la cag stato di 8 min . le lesioni sono state considerate significative se 50% per la ctca e se 70% per la cag . 
sono stati inoltre calcolati la prevalenza di malattia , ed i likelihood ratio positivo e negativo ( lr + e lr - , rispettivamente ) con intervalli di confidenza del 95% . 
circa un decimo dei pazienti aveva malattia monovasale ( 9 , 4% ; 15 / 160 ) , e uno su venticinque aveva malattia trivasale ( 3 , 8% ; 6 / 160 )  . 
il calcium score coronarico secondo agatston risultato intermedio con ampia variabilit ( mediadeviazione standard [ ds ] = 178 , 6346 , 1 ; mediana = 17 ; range = 02123 ) , rispecchiando una popolazione eterogenea ed con prevalenza di malattia coronarica medio - bassa . 
approximately one tenth of patients had single - vessel disease ( 9.4% , 15 / 160 ) , and one in 25 had three - vessel disease ( 3.8% , 6 / 160 )  . 
the best accuracy values were recorded in the left main coronary artery and the left anterior descending coronary artery ( sensitivity 100% )  . per - patient evaluation a total of 160 patients were included in the comparison with cca . 
accuracy values were excellent , with a sensitivity and npv of 100% . discussion validation studies conducted to date focused on patient populations with a high pretest probability of cad ( range 5090% ) who were already candidates for cca [ 37 , 918 ]  . 
recommendations for the clinical use of ctca suggest that it i appropriate to use the technique in cases in which the patient is at low to intermediate risk and stress tests are doubtful , inconclusive or cannot be performed [ 8 , 20 , 22 ]  . 
findings of our study show accuracy values in the type of disease no or non significant disease , n ( % ) single - vessel disease , n ( % ) two - vessel disease , n ( % ) three - vessel disease , n ( % ) total , n tipo di malattia assenza di malattia o malattia non significativa , n ( % ) malattia mono - vasale , n ( % ) malattia bi - vasale , n ( % ) malattia tri - vasale , n ( % ) totale , n tabella 2 prevalenza di malattia coronarica mediante cag prevalence 112 ( 70 ) 15 ( 9.4 ) 13 ( 8.1 ) 6 ( 3.8 ) prevalenza 112 ( 70 ) 15 ( 9 , 4 ) 13 ( 8 , 1 ) 6 ( 3 , 8 ) valutazione per vaso sono stati inclusi nella valutazione 637 vasi coronarici . 
dei 4 vasi valutati il tronco comune sinistro e la discendente anteriore hanno mostrato i migliori valori di accuratezza diagnostica ( sensibilit 100% )  . valutazione per paziente sono stati inclusi per il confronto con la cag 160 pazienti . 
i valori di accuratezza sono risultati ottimali con una sensibilit ed un valore predittivo negativo pari al 100% . discussione gli studi di validazione condotti fino a questo momento si sono focalizzati su popolazioni di pazienti ad elevata probabilit pre - test di malattia coronarica ( range 50%90% circa ) gi candidati alla cag [ 37 , 918 ]  . 
le attuali raccomandazioni di utilizzo clinico della ctca suggeriscono che un utilizzo congruo della metodica sarebbe nei casi in cui il paziente sia a rischio basso - intermedio ed i test provocativi siano dubbi , non fattibili o inconclusivi [ 8 , 20 , 21 ]  . 
in our study , fluctuations in accuracy values can be seen , with a high npv ( > 99% in all cases ) , in the three levels of analysis , along with a progressive increase , from per - segment to pervessel and per - patient analyses , in sensitivity ( 90% , 98% , 100% , respectively ) and ppv ( 53% , 61% , 71% , respectively )  . 
in some patients with obstructive disease , there may be more than one lesion , and it is more likely that at least one of the lesions is correctly interpreted if they are multiple in the individual patient . 
 the lr + describes the extent to which the likelihood of disease increases when the test is positive , whereas the lrdescribes the extent to which the likelihood of disease 16 , 18 ]  . 
nel nostro studio si osservano delle fluttuazioni nei valori di accuratezza diagnostica con un valore predittivo negativo conservato ( sempre > 99% ) nei tre livelli di analisi ed un progressivo incremento , passando dallanalisi per segmento , a quella per vaso , e a quella per paziente , della sensibilit ( 90% , 98% , 100% , rispettivamente ) e del valore predittivo positivo ( 53% , 61% , 71% , rispettivamente )  . 
un ottimo test di inclusione ( sensibilit ) dovrebbe fornire valori di lr + > 10 , mentre un ottimo test di esclu734 radiol med ( 2012 ) 117 : 725738 fig . 
for this and clinical reasons , the patient with stenosis > 50% , both in ctca and cca , should undergo stress imaging to precisely define the presione ( valore predittivo negativo ) dovrebbe fornire valori di lr - < 0 , 10 . 
deve essere specificato che lutilizzo della ctca come metodica di prima istanza ( prima dei test provocativi ) non esclude leffettuazione dei test di inducibilit ma la riserva ai casi in cui la malattia coronarica sia sub - critica / critica . 
per questo motivo e per motivi clinici il paziente con stenosi > 50% , sia in ctca che in cag , dovrebbe effettuare uno stress imaging per definire presenza , sede ed entit dellischemia inducibile . nel nostro studio un valore aggiuntivo hanno avuto le radiol med ( 2012 ) 117 : 725738 fig . 
ctca ( a - e ) shows coronary arteries with no significant stenoses both in the volume - rendered images ( a , b ) and the curved multiplanar images ( c : right coronary artery ; d : left anterior descending coronary artery ; e : circumflex coronary artery )  . 
la ctca ( a - e ) mostra coronarie esenti da stenosi significative sia nelle immagini con volume rendering ( a , b ) sia nelle immagini multiplanari curvate ( c coronaria destra ; d coronaria discendente anteriore ; e coronaria circonflessa )  . 
lesame stato condotto ad una frequenza cardiaca di 58 bpm con una dose di radiazioni di 8 , 9 msv . sence , site and extent of inducible ischaemia . in our study , an additional advantage was provided by using first - generation iterative reconstructions ( iris , siemens , germany ) that enable image noise to be significantly reduced without adjusting any other variables . 
lastly , the radiation dose ricostruzioni iterative di prima generazione ( iris , siemens , germania ) che consentono di ridurre significativamente il rumore dellimmagine a parit di altri parametri . 
infine , la dose di radiazioni utilizzata nel presente studio legata allutilizzo di un protocollo con gating ecg retrospettivo e modulazio736 radiol med ( 2012 ) 117 : 725738 fig . 
this 54 - year - old , hypertense man ( body mass index 26 ) with a family history of cardiovascular disease presented with atypical chest pain and abnormal electrocardiogram suggestive of ischaemia . 
ctca ( a - c ) shows a left anterior descending coronary artery without significant stenosis ( b ) and a circumflex coronary artery with stenosis > 50% in the context of a very irregular section of the wall ( arrowhead , c )  . 
la ctca ( a - c ) mostra una coronaria discendente anteriore senza stenosi significative ( b ) ed una coronaria circonflessa con una stenosi > 50% nel contesto di un tratto di parete molto irregolare ( testa di freccia , c )  . 
lesame stato condotto ad una frequenza cardiaca di 55 bpm con una dose di radiazioni di 5 , 9 msv . used in this study is based on a protocol with retrospective ecg gating and prospective dose modulation . 
questa tecnica consente di scendere al di sotto di 1 msv in condizioni ottimali che consistono di frequenza cardiaca regolare e < 60 bpm associata ad una corporatura minuta del paziente ( bmi < 25 ) [ 25 , 28 ]  . 
in ogni caso , la riduzione della dose deve essere uno degli obiettivi essenziali nella pratica della ctca , senza che questo condizioni radiol med ( 2012 ) 117 : 725738 affect the accuracy of the technique and , in particular , the npv . in alcun modo laccuratezza diagnostica ed in particolare il valore predittivo negativo . limitations limitazioni ctca and cca reports can be interpreted as a limitation with respect to the more rigorous and semiquantitative / quantitative evaluations performed in validation studies . 
however , in the phases outside the maximum dose window ( from 80% to 65% of the rr interval in our case ) , the dose is 4% with the protocol used ( mindose , siemens , germany ) , which enables evaluation of the ejection fraction and left ventricular wall motion ( which otherwise cannot be performed )  . lutilizzo dei referti della ctca e della cag pu essere interpretato come un limite rispetto alle valutazioni pi rigorose e semi - quantitative / quantitative effettuate negli studi di validazione . 
 la dose di radiazioni stimata durante la ctca ( 7 , 22 , 1 msv ) paragonabile a quella di una cag diagnostica anche nella nostra casistica [ 2934 ]  . 
tuttavia , nelle fasi al di fuori della finestra di dose massima ( dall80% al 65% dellintervallo rr nel nostro caso ) la dose del 4% con il protocollo utilizzato ( mindose , siemens , germania ) e consente la valutazione della frazione di eiezione e della cinetica del ventricolo sinistro ( altrimenti non effettuabile )  . conclusions conclusioni the accuracy of ctca with a second - generation dsct system and using iterative reconstructions enables the technique to be used as a noninvasive anatomical reference test for the diagnosis and exclusion of obstructive cad . 
 laccuratezza diagnostica della ctca con apparecchiature dsct di seconda generazione con ricostruzioni iterative consente di utilizzare la metodica come test anatomico non invasivo di riferimento per la diagnosi e lesclusione di malattia coronarica ostruttiva . 
favrel1 1dpartement de radiothrapie oncologie , centre hospitalier lyon sud , chemin du grand - revoyet , 69310 pierre - bnite , et ea3738 , universit claude - bernard , lyon , france 2service de biostatistique , universit lyon - sud , chemin du grand - revoyet , 69495 pierre bnite cedex , france correspondence to : b . 
other clinical and / or anthropometrical features should be prospectively evaluated in order to assess the need for re - planning . keywords adaptive radiotherapy head and neck cancers imrt setup margins weight loss riassunto obiettivo . 
gli errori di setup dei pazienti h&n trattati con imrt dal 01 / 2010 al 06 / 2010 sono stati analizzati in maniera prospettica e correlati statisticamente alla perdita di peso . 
altri criteri clinici e / o antropomorfici devono essere valutati in maniera prospettica per stabilire la necessit di un replanning . parole chiave radioterapia adattativa tumori della testa e del collo imrt margini di setup perdita di peso 886 introduction radiotherapy plays a critical role in the management and the cure of many patients with head and neck ( h&n ) cancer . 
at the same time , significant anatomical changes , which may be related to multiple factors ( shrinkage of the tumour and / or nodal masses , weight loss , resolution of postoperative changes ) , could often occur during the treatment [ 1 , 2 ]  . 
four - dimensional conformal radiotherapy ( 4d - crt ) has been described as the explicit inclusion of the temporal changes in anatomy during the imaging , planning , and delivery of radiotherapy [ 3 ]  . 
intrafraction changes may occur during sessions of radiotherapy as a result of processes such as breathing , swallowing , cardiac motion or patient movements due to discomfort . because of these changes , it could be argued that the planned dose distributions to target volumes and organs at risk ( oars ) based on computed tomography ( ct ) images obtained before treatment may significantly differ from those actually delivered during the course of fractionated radiotherapy [ 4 , 5 ]  . 
moreover , the advent of intensity - modulated radiation therapy ( imrt ) leads to highly conformal treatment designed to maximise tumour coverage and spare normal tissues , particularly the spinal cord and parotid glands [ 610 ]  . 
the sharp dose gradients between boundaries of planned target volumes ( ptv ) and critical normal tissues that occur in the setting of imrt make attention to margins around the clinical target volume ( ctv ) crucial because of the higher risk of dosimetric changes that may be even more drastic than in conventional treatments [ 5 ] , with consequent underdosage of tumour volumes and / or overdosage of critical normal structures . 
if the internal target volume ( itv ) is not a major issue in h&n cancers , setup margins ( sm ) should be strictly considered in the definition of treatment volumes of these tumours . 
moreover , if the impact of anatomical changes on dosimetry has already been shown , little evidence exists about the possibility to predict when it is better to replan patients showing major anatomical modifications in order to improve their setup . 
in particular , radiation oncologists would like to have a simple parameter to use during their daily practice in order to establish the correct time to repeat simulation ct scans during the course of treatment and recalculate optimised imrt treatment plans ( tps ) for patients with locally advanced h&n cancer . 
weight could radiol med ( 2012 ) 117 : 885891 be a good candidate ; however , to our knowledge , it is not known whether there is a relationship between weight loss and setup errors . 
in this prospective study , we verified whether a statistical relationship could be found between weight loss and setup errors in order to assess the predictive value of weight loss on setup errors of patients treated for h&n cancers . materials and methods patients this prospective analysis of patients treated in our radiation oncology department between january and june 2010 includes setup data of patients with locally advanced ( ct34n0 - 3m0 ) h&n cancer who were treated with imrt with and without concomitant chemotherapy ( or cetuximab )  . 
 treatment and imaging before treatment , all patients underwent a 2.5 - mm slicespacing ct scan simulation in the supine position and were stabilised using a thermoplastic mask , h&n board , neckshaped support ( medtec orange city , ia , usa ) , and standard knee fix during rt according to standard quality assurance procedures of our radiation oncology department . 
 reference lines were marked on the immobilisation device during simulation defined by laser beams , and equivalent alignment was performed at treatment . target volumes and all oars were manually contoured on axial slices of the planning ct scan by an experienced radiation oncologist . 
following international commission on radiation units and measurements ( icru ) 62 indications [ 11 ] , gross tumour volume ( gtv ) represented visible tumour and / or enlarged or suspicious lymph nodes identified either clinically or radiographically by magnetic resonance ( mr ) imaging , ct scan and / or positron emission tomography ( pet )  . 
ctv1 and 2 represented tissue believed to harbour risk of microscopic disease and included lymph - node regions and a 0.5to 2 - cm margin on the gtv ( depending on the presence or absence of anatomical boundaries to microscopic spread and / or proximity to critical normal structures )  . 
in this analysis , we only considered volumes treated with the imrt technique . results patient characteristics analysis of setup errors our standard departmental rt protocol incorporated weekly 2d orthogonal electronic portal images ( epi ; gantry position 0 and 90 )  . 
analysis of these images was performed by outlining the regional anatomical bony structures ( including vertebrae , intervertebral spaces , mandible and skull ) on each fields reference image , which was their ct - derived digitally reconstructed radiography ( drr )  . 
manual offline matching was done of bony anatomy using the as - 500 or as - 1000 portal imager ( varian ) to compare reference drrs to those acquired weekly during treatment . 
errors > 5mm were recorded for the analysis , but they were corrected before treatment . evaluation of setup margins the systematic constituent of setup errors ( ) from the isocentre is the displacement that persists during the entire treatment course , whereas the random constituent ( ) is the day - to - day variations during the course of treatment . 
as previously reported , the mean and standard deviation ( sd ) of weekly measurements for each axis of each patient were derived to assess and [ 14 ]  . 
resultant values were incorporated into the formulas proposed by the icru [ 11 ] , by stroom and heijmen [ 14 ] and by van herk [ 15 ] , in order to derive ctv - toptv margins in the rl , si and ap planes . 
these formulas are derived to estimate that 95% of the dose is delivered to the ctv for 90% of patients . evaluation of relationship between weight loss and setup errors from january to june 2010 , 22 consecutive patients with locally advanced , nonmetastatic stage iiiiva h&n cancer were treated by imrt . 
all had a diagnosis of squamouscell carcinoma , except two patients receiving post - ct radiotherapy for a lymphoma of the nasopharynx ( patient 3 in table 1 ) and adjuvant radiotherapy for a melanoma presenting close surgical margins at the specimens ( patient 4 in table 1 )  . 
analysis of the impact of weight loss ( absolute value ) and of the percent of weight loss showed no statistical relation with setup precision in patient in the three directions ( table 3 )  . looking at table 1 , it is interesting to note that the ranges of setup errors seemed not to be different when comparing patients with limited weight loss and those with more substantial weight loss . 
we found the same probability of having large setup errors ( > 5 mm ) in patients with a relatively low weight loss ( < 3kg , patients 2 , 3 , 4 and 6 ) and in those with a greater weight loss value ( > 7kg , patients 10 , 11 , 14 , 21 )  . 
similarly , we found the same probability of having small setup errors ( < 5 mm ) in patients with a relatively low weight loss ( < 3kg , patients 5 and 9 ) and in those with a higher weight loss value ( > 7 kg , patients 8 , 15 , 17 , 19 and 22 )  . 
weight loss ( absolute value ) and percent of weight loss were studied to assess the impact of these parameters on setup precision of patients in the rl , si and ap planes . 
at the same time , significant anatomical changes , which may be related to multiple factors such as shrinkage of the tumour and / or nodal masses , weight loss and resolution of postoperative changes , could often occur during treatment and should strictly be considered because of their impact on the real delivered dose [ 4 , 5 ]  . 
only two articles and one abstracts exist in the literature , and their results are contrasting [ 1820 ]  . there are some limitations to our study , such as its retrospective design and population heterogeneity . 
the advent of imrt leads to highly conformal treatments designed to maximise tumour coverage and spare normal tissues , particularly the spinal cord and parotid glands [ 610 ] , and increases the importance of taking into account inter and intrafraction variations [ 7 , 21 ]  . 
although it has already reported that replanning is useful to account for anatomical and tumoural changes and to decrease dose to normal tissues around the tumour [ 22 ] , the effect of weight loss on setup margins has never been extensively studied . 
in our opinion , the first method can expose the analysis to two selection biases : the first is the choice of group determinants ; the second is the risk of performing different statistical analyses with different ad hoc groups in order to finally obtain a statistically significant result . 
for this reason , it was not considered to be a confounding factor in our analysis . as stated above , only two papers report the impact of weight loss on setup errors . 
the aim of their study was to quantify setup errors of patient positioning during image890 radiol med ( 2012 ) 117 : 885891 guided radiation therapy ( igrt ) and correlate setup errors to patient - specific factors such as weight , height , body mass index ( bmi ) and weight loss . 
setup errors were studied on a cone - beam ct system on which acquisitions were obtained according to a standardised action - limit protocol and compared with pretreatment ct images . 
the average 3d deviation from three initial cone - beam ct scans was compared with deviations at the 10th and 20th treatment session and correlated by linear regression analysis to height , weight and bmi and in h&n to weight loss as expressed by the relative weight change over time . 
with h&n and lung cancer analysed separately , no statistically significant correlation was observed between setup errors and height , weight , bmi or weight change during treatment , irrespective of whether 3d deviations from the initial three cone - beam scans or scans from the 10th or 20th treatment sessions were used . 
 the authors concluded that this igrt study did not support the hypothesis that setup errors during radiotherapy are correlated to patient height , weight , bmi or weight loss [ 18 ]  . different results were reported in an abstract presented by wang et al . 
high weight loss values , even though we did not perform a statistical analysis because of our decision to consider weight as a continuous variable . the effect of an intensive nutritional programme delivered by percutaneous endoscopic gastrostomy ( peg ) on daily setup variations of h&n cancer patients was also evaluated by mercuri et al . 
 [ 20 ] , who verified that there was a significant difference in weight loss experienced between peg ( ten patients ) and non - peg ( ten patients , p = 0.04 ) groups , with the non - peg group losing an average of 2.6 kg more than the peg group over the course of rt . 
the authors concluded that intensive enteral support maintained weight stability in h&n patients considered at risk of weight loss during rt , and this was associated with reduced setup variation . 
that it is important to prevent weight loss during rt , as maintaining weight can reduce toxicity and morbidity , we cannot conclude that weight loss has an impact on setup errors of patients treated for an h&n cancer . 
 it should be also noted that the optimal method for providing en to patients with h&n cancer is still unclear : at our institution , the decision to deliver en is based on a reactive policy , which consists of placing a nasogastric ( ng ) feeding tube only when required by the patients nutritional status , as recently reported by clavel et al . 
we statistically demonstrated that weight loss does not have a significant impact on setup errors and the trend of weight loss cannot help clinicians decide on the correct timing of replanning . 
the next step of this study will be to verify whether new technological possibilities can help radiation oncologists find other simple methods to identify when to replan a patient who loses weight . 
the role of conebeam ct and deformable image registration as a method for studying dosimetric consequences of anatomical changes in adaptive imrt of h&n cancer has already been investigated [ 24 ]  . 
ji3 1department of radiology , zhongshan hospital of fudan university and department of medical image , shanghai medical college of fudan university , shanghai , china 2global applied science laboratory , ge healthcare , shanghai , china 3department of pathology , zhongshan hospital of fudan university , shanghai , china correspondence to : mengsu zeng , department of radiology , zhongshan hospital of fudan university , no138 , fenglin road , xuhui district , shanghai , 200032 china , tel . : + 86 - 021 - 64041990 - 2130 , fax : + 86 - 021 - 64439906 , e - mail : zengmengsu@gmail.com foundation item : scientific research foundation for new teachers of fudan university ( jjf152005 ) received : 11 april 2011 / accepted : 4 may 2011 / published online : 18 november 2011 springer - verlag 2011 abstract purpose . 
per la rilevazione dei metaboliti nel pancreas normale e nel tessuto neoplastico stata utilizzata la spettroscopia rm con gating respiratorio ; i dati spettroscopici sono stati elaborati con il software sage . 
compared with normal pancreas , pancreatic carcinoma has a higher ratio of fatty acids ( ch = ch ) to lipids and lower ratios of lipids to unsuppressed water and choline to unsuppressed water at 3t . keywords pancreas carcinoma magnetic resonance spectroscopy 3t pancreas normale risultato significativamente maggiore del medesimo rapporto nel carcinoma pancreatico ( p = 0 , 004 )  . 
it ranks ninth in the incidence of solid cancers and fourth for cancer - related deaths , with an overall median survival of around 46 months [ 1 ]  . 
 owing to the lack of specific symptoms and insufficient diagnostic tools , most pancreatic cancers are diagnosed at a late stage and cannot be visualised as easily and early as cancer of hollow organs of the gastrointestinal tract . 
although diagnostic pancreatic imaging modalities , such as ultrasound ( us ) , computed tomography ( ct ) and magnetic resonance imaging ( mri ) , have evolved markedly in recent years , most patients still present with a progressive and incurable state of the disease at diagnosis , with the only option being palliative chemotherapy [ 2 ]  . 
furthermore , preoperative imaging diagnosis is often challenging because of some masslike lesions , such as inflammatory mass , focal lipomatosis , pancreatic abscess or other benign abnormalities [ 3 ]  . in vivo mr spectroscopy , a noninvasive technique , has been successfully used to provide a preoperative diagnosis of malignancies , particularly in several organs , including the brain , breast and prostate [ 49 ]  . 
the elevation of total choline - containing compounds detected by in vivo mr spectroscopy has also been recognised and confirmed as the phenotype of metabolisms in these malignant neoplasms [ 1018 ]  . 
although in vivo 1h - mr spectroscopy of chronic focal pancreatitis showed less lipids than did the spectra of pancreatic carcinoma at 1.5 tesla , the specific metabolic markers in pancreatic carcinoma were not detected [ 19 ]  . with the availability of ultra - high - field magnets for wholebody clinical scanning and the increased signal - to - noise ratio ( snr ) , there is improvement in both imaging and spectral resolution . 
reported that the ratios of concentrations of taurine , lactate and creatine to phosphocreatine in pancreatic tumours were significantly different from those of normal pancreases at a bruker am - 360 wb spectrometer [ 20 ]  . 
however , to the best of our knowledge , evaluation of pancreatic cancer with in vivo proton mr spectroscopy with a 3 - t scanner has not yet been reported . in this manuscript , we present our initial experience of using 1h - mr spectroscopy at 3 t in evaluating pancreatic cancer , providing a comparison with normal pancreas , which might be helpful to further investigate early diagnosis , differentiation and treatment monitoring of pancreatic cancer . 
 materials and methods the study was approved by our institutional review board ; written informed consent was obtained from all participants . patient population between may 2008 and january 2011 , 40 patients ( 24 men and 16 women ; mean age 55.8 years ; age range 3866 years ) with pancreatic cancer ( range of the smallest diameter 2.24.3 cm ; mean diameter 3.3 cm ) in the head of pancreas proved by histopathology after surgery and 40 healthy volunteers ( 25 men and 15 women ; mean age 55.6 years ; age range 4065 years ) , who had no previous medical history or current morbidity , were included in this prospective study . 
thirty - seven healthy volunteers with a small pancreatic head ( unsuitable for positioning the single voxel of 782 radiol med ( 2012 ) 117 : 780788 mr spectroscopy ) .were excluded twenty - five patients who had lesions with necrotic area ( n = 8 ) or no histopathological confirmation ( n = 17 ) were also excluded . 
patients and volunteers fasted for 6 h prior to mri examination . mri technique mri and proton mr spectroscopy were performed using a whole - body 3 - t scanner ( signa hdx , ge healthcare , milwaukee , wi , usa ) with an eight - element phased - array surface coil . 
respiration - triggered single - voxel point - resolved spectroscopy sequence ( press ) 1h mr spectra were acquired on all participants with te = 35 ms , tr = 2 , 5003 , 500 ms , 128 averages , eight phase cycles and 16 additional unsuppressed water reference lines . 
b spectrum with water suppression showed five main peaks in the head of normal pancreas : unsaturated fatty acids ( ch2ch = ch ) at 5.4 ppm ; residual water signal at 4.7 ppm ; choline metabolites at 3.2 ppm ; unsaturated fatty acids ( ch2ch = ch ) at about 2.0 ppm ; lipids at 1.3 ppthe ratios of choline to unsuppressed water and fatty acids ( ch2ch = ch ) to lipids were 6.13710 - 3 and 35.79310 - 3 , respectively . 
b lo spettro con la soppressione del segnale dellacqua nella testa del pancreas normale composto da 5 picchi principali : acidi grassi insaturi ( ch2 ch = ch ) a 5 , 4 ppm ; acqua residua a 4 , 7 ppm ; metaboliti della colina a 3 , 2 ppm ; acidi grassi insaturi ( ch2ch = ch ) a 2 , 0 ppm e lipidi a 1 , 3 pp il rapporto colina / acqua non soppressa ed acidi grassi insaturi ( ch2ch = ch ) / lipidi di 6 , 13710 - 3 e 35 , 79310 - 3 rispettivamente . 
c lo spettro senza la soppressione del segnale dellacqua dimostra il picco dellacqua a 4 , 7 ppm e quello dei lipidi a 1 , 3 ppil rapporto lipidi / acqua 9 , 00710 - 3 . radiol med ( 2012 ) 117 : 780788 fig . 
b lo spettro con la soppressione del segnale dellacqua nella testa del pancreas normale composto da 5 picchi principali : acidi grassi insaturi ( ch2ch = ch ) a 5 , 4 ppm ; acqua residua a 4 , 7 ppm ; metaboliti della colina a 3 , 2 ppm ; una combinazione di n - acetilaspartato ( naa ) , n - acetil - aspartil - glutammato ( naag ) , glutammina , glutammato e acidi grassi insaturi ( ch2ch = ch ) a 2 , 0 ppm e lipidi a 1 , 3 ppm . of three chemical - shift - selective pulses with predefined flip angles to leave a significant amount of residual water in the spectrum to enable line - by - line phase correction . 
all participants were instructed to breathe in a regular rhythm in the supine position so that localisation images for the single - voxel mr spectroscopy and press method spectra were acquired at the same respiratory level . 
acquisition time for mr spectroscopy was 8 m mr spectra with analysable quality were defined as having a water suppression rate > 90% combined with a line width < 10 hz after auto - prescanning . 
 mr image and spectral analysis mr spectral data were analysed using commercially available software ( sage 7.2 , ge healthcare ) by a single mr physicist experienced in mr spectral analysis . 
c spectrum with water suppression shows five main peaks in pancreatic cancer : unsaturated fatty acids ( ch2ch = ch ) at 5.4 ppm ; residual water signal at 4.7 ppm ; choline metabolites at 3.2 ppm ; unsaturated fatty acids ( ch2ch = ch ) at about 2.0 ppm ; lipids at 1.3 ppratios of choline to unsuppressed water and fatty acids ( ch2ch = ch ) to lipids were 1.57210 - 3 and 103.37710 - 3 , respectively . 
a la scansione assiale ottenuta dopo somministrazione di mezzo di contrasto tramite sequenza volumetrica t1 - dipendente con saturazione del grasso ( lava ) mostra la lesione alla testa pancreatica . 
c lo spettro con la soppressione del segnale dellacqua nel carcinoma pancreatico composto da 5 picchi principali : acidi grassi insaturi ( ch2ch = ch ) a 5 , 4 ppm ; acqua residua a 4 , 7 ppm ; metaboliti della colina a 3 , 2 ppm ; grassi insaturi ( ch2ch = ch ) a 2 , 0 ppm e lipidi a 1 , 3 ppil rapporto colina / acqua non soppressa ed acidi grassi insaturi ( ch2ch = ch ) / lipidi 1.57210 - 3 e 103.37710 - 3 , rispettivamente . 
d lo spettro senza la soppressione del segnale dellacqua dimostra il picco dellacqua a 4 , 7 ppm e quello dei lipidi a 1 , 3 ppil rapporto lipidi / acqua 2 , 93210 - 3 . radiol med ( 2012 ) 117 : 780788 ppm , with line width < 15 hz and snr > 3 . 
some spectra that revealed no significant choline resonance or fatty acids but met criteria for analysable quality were included . statistical analysis all data were processed using a statistical software package ( spss for windows , version 16.0 ; spss inc , chicago , il , usa )  . 
ratio of lipids to unsuppressed water and ratios of the peak areas of fatty acids and choline to that of unsuppressed water were analysed between normal pancreas and pancreatic cancer , respectively . 
ratios of the peak area at 5.4 ppm to unsuppressed water and the peak area at 3.2 ppm to that at 1.3 ppm showed no statistical differences between normal pancreas and pancreatic cancer . 
in this study , all pancreatic heads in 40 healthy volunteers were large enough to posit the adapted voxel of mr spectroscopy , and those healthy volunteers with a small pancreatic head were excluded . 
the possible interference of adjacent tissue for metabolic acquisition using in vivo 1h - mr spectroscopy was mainly from peripancreatic fat , vessels , duodenum , gastrointestinal tract and its contents . 
in order to diminish noise from physiologic movement , all participants were instructed to breathe in a regular rhythm to make sure that the time of signal acquisition of images of localisation and spectra data could fall approximately into the end of expiration at the same level of respiratory baseline . 
furthermore , the small range of movement of the pancreas during respiration seemed to help diminish noise due to its retroperitoneal positioning [ 19 ]  . determining metabolite concentrations is relative rather than absolute and requires acquisition of a reference signal . 
the unsuppressed water at 4.7 ppm was used as internal reference in this study . in vivo 1h - mr spectroscopy of pancreatic carcinoma did not detect the specific metabolic markers in pancreatic carcinoma at 1.5 t [ 19 ]  . 
according to previously published in vitro 1h - mr spectroscopy studies using ultra - high - field magnets , decreases in phosphocholine and glycerophosphocholine levels and increases in leucine , isoleucine , valine , lactate and alanine levels were observed in pancreatic cancer [ 20 , 21 ]  . 
in addition , due to the higher signal and reduced measurement time for acquiring specific data , in vivo acquisition of mr spectroscopy may be particularly advantageous for 3 t [ 24 ]  . 
previously , the presence of the signal at 3.2 ppm ( attributed to choline metabolites ) was found to be a marker of malignancies in the breast , prostate and brain , because choline kinase overexpression and activity have increased in these malignant cells . 
the choline transporter - like proteins of the ctl family are composed of the five genes , ctl1 ctl5 , with ctl1 being the main member of the family [ 26 ]  . 
 hctl1 protein is expressed as two major polypeptides of 50 and 23 kda each in a variety of tissues , including brain , heart , small intestine , kidney , liver , lung , skeletal muscle , pancreas , spleen , ovary and testis [ 27 ]  . 
for most mammals , prolonged ( weeks to months ) ingestion of a diet deficient in choline ( and adequate though limited in methionine and folate content ) has consequences that include pancreatic disorders [ 28 ]  . 
the peak of choline metabolites can be detected by in vivo 1h - mr spectroscopy in some normal organs , such as brain , liver , kidney and skeletal muscle , because high concentrations of those metabolites are indispensable for maintaining normal function of these cells . 
pancreatic acinar cells can produce rich and various digestive enzymes , which highly correlate with exocytosis in all types of membranes , and their integrity is related to choline phospholipid metabolis furthermore , pancreatic islets are densely innervated by postganglionic cholinergic nerve fibres emanating from nerve - cell bodies in the pancreatic ganglia that are innervated by the vagus nerves [ 29 , 30 ]  . 
cholinergic receptors have been observed in close association with insulin - secreting cells within pancreatic islets , whereas choline increased the acetylcholine content of the pancreas and enhanced acetylcholine release from minced pancreas [ 31 ] , which suggests that high concentrations of choline aids to enhance the function of insulin secretion in the normal pancreas . 
although the high proliferation of cancer cells can cause high concentrations of choline metabolites , the concentration of these free molecules in the normal pancreas might be higher than that in pancreatic cancer owing to pancreatic hypermetabolism . fatty deposition in the pancreas usually occurs with aging and is sometimes combined with pancreatic atrophy . 
despite having higher content of choline metabolites and lipids , normal pancreas did not reach a statistically significant difference from pancreatic cancer in terms of ratio of choline metabolites to lipids . more endogenous fatty acids are produced within cancerous microenvironment owing to anoxia [ 32 ]  . 
the resonance of fatty acids at 5.4 ppm is attributed to cholesterol and unsaturated olefinic regions of fatty acids , which might afford important metabolic information in mr spectroscopy of pancreatic cancer due to its poorer blood supply and severer anoxia . 
accordingly , a higher content of lipids within the voxel of mr spectroscopy resulted in the lower ratio of fatty acids to lipids in normal pancreas compared with that in pancreatic cancer , whereas the ratio of fatty acids to unsuppressed water did not reach statistical difference between these two groups . 
however , initial results were that mr spectroscopy equipped with a 3 - t clinical mr imager proved to have enough spectral resolution and sensitivity to quantify metabolic changes in normal pancreas and pancreatic cancer . 
another limitation was that no other pancreatic abnormalities were compared with normal pancreas and pancreatic cancer in the analysis of mr spectral data , which should be performed in the future based on the mr spectra of normal pancreas and pancreatic cancer . 
the third limitation was the application of this technique in depicting small pancreatic cancers , especially those < 1 cm , which was mainly due to the low spectral resolution from the small voxel of mr spectroscopy . in conclusion , our study demonstrated that in vivo proton mr spectroscopy at 3 t was technically feasible for evaluating normal pancreas and pancreatic cancer . 
based on our preliminary study , pancreatic cancer tends to have lower ratios of lipids and choline to unsuppressed water , whereas a higher ratio of fatty acids ( ch2ch = ch ) to lipids existed in pancreatic cancer . 
fugazzola1 1department of radiology , universit dellinsubria , viale borri 57 , 21100 varese , italy 2department of surgery , universit dellinsubria , viale borri 57 , 21100 varese , italy correspondence to : g . 
in the last 3 years , pc was performed on 30 elderly and critically ill patients ( 17 men , 13 women ; mean age 78.6 , range 57 - 97 years ) with acute cholecystitis and comorbid diseases . 
clinical effectiveness was 30 / 30 ( 100% ) , with statistically significant reductions in while blood cell ( wbc ) count , c - reactive protein ( crp ) and fever . 
lefficacia clinica si avuta in 30 casi su 30 ( 100% ) con una riduzione statisticamente significativa della leucocitosi ( wbc ) , proteina c reattiva ( cpr ) e febbre . 
il valore medio dei globuli bianchi al ricovero ( 19 , 87101 , 6110 / l ) , della febbre ( 38 , 20 , 11c ) e della crp ( 248 , 74 , 76 mg / l ) si sono significativamente ridotti nelle 72 ore successive al trattamento di colecistostomia percutanea [ 12 , 9101 , 0510 / l ( p0 , 0001 ) , 370 , 04c ( p0 , 0001 ) , 113 , 53 mg / l ( p0 , 0001 ) , rispettivamente ]  . 
in conclusione si dimostra che la colecistostomia percutanea , nonostante il numero limitato di pazienti del nostro campione , un metodo di trattamento veloce , semplice ed efficace per la cura della colecistite acuta nei malati critici e nei pazienti anziani . 
 la morbilit relativa alla procedura e la mortalit sono radiol med ( 2012 ) 117 : 772779 cholecystostomy critically ill and elderly patients ultrasonographic guidance molto basse se comparate alla chirurgia tradizionale . 
 il trattamento conservativo per i pazienti per i quali controindicato il trattamento chirurgico ben tollerato . parole chiave colecistite acuta colecistostomia percutanea pazienti critici e anziani guida ecografica introduction introduzione cholecystectomy is the most appropriate treatment for acute calculous and acalculous cholecystitis , with a mortality rate of 00.8% [ 1 , 2 ]  . 
for these patients , over the last two decades , image - guided percutaneous cholecystostomy ( pc ) for tube placement has become a useful therapeutic intervention [ 5 , 6 ]  . 
the aims of the study were to investigate the efficacy and clinical outcome of pc in treating acute cholecystitis in critically ill and elderly patients . materials and methods over the last of 3 years , pc was performed on 30 elderly and critically ill patients ( 17 men , 13 women ; mean age 78.6 , range 5797 years ) with acute cholecystitis and comorbid diseases . 
according to results of the bile culture . risk classification la colecistectomia il trattamento pi appropriato nella colecistite acuta litiasica o alitiasica , con un tasso di mortalit compreso tra lo 0% e lo 0 , 8% [ 1 , 2 ]  . 
 lobbiettivo del nostro studio quello di dimostrare lefficacia della colecistostomia percutanea nel trattamento della colecistite acuta nei malati critici e nei pazienti anziani e il loro outcome clinico . materiali e metodi negli ultimi tre anni , la colecistostomia percutanea stata eseguita su 30 pazienti , malati critici e pazienti anziani , ( 17 uomini , 13 donne , et media 78 anni , range 5797 anni ) con colecistite acuta e associate comorbilit . 
la diagnosi di colecistite acuta si basa sullesame obiettivo ( dolore in ipocondrio destro e febbre ) , sullalterazione degli indici di laboratorio ( leucocitosi e proteina c reattiva > 5 mg / l ) e su reperti radiologici ed ecografici come la distensione della colecisti , la calcolosi colecistica , lispessimento delle pareti del viscere ( > 3 mm ) , versamento pericolecistico e il segno di murphy ecografico [ 7 ]  . 
diagnosticata la colecistite acuta , sono stati somministrati antibiotici endovena in accordo con i risultati dellesame colturale effettuato sui campioni di bile dei pazienti . all patients were graded for risk of cholecystectomy according to the american society of anesthesiologists ( asa ) classification system ( table 1 ) , and all ware classified as asa iii . 
moreover , pre - procedura il rischio operatorio della colecistectomia per tutti i pazienti stato classificato adottando i criteri dellamerican society of anesthesiologists ( asa ) ( tabella 1 ) , nel nostro studio tutti i pazienti sono stati classificati come asa iii . la colecistostomia percutanea stata eseguita in asepsi e con 774 radiol med ( 2012 ) 117 : 772779 table 1 society of interventional radiology classification system for complications by outcome complications classification minor complications 1 . 
decesso conscious sedation was used according to the principles of monitored anaesthesia care ( a combination of propofol , midazolam and fentanyl was administered in adequate doses according to patient weight and procedure duration )  . 
 procedure the procedure was carried out under ultrasonographic ( us ) guidance ( atl 5000 and iu22 philips , best , the netherlands ) in the interventional unit of the radiology department in 26 patients and at the patients bedside in four cases . 
inoltre , stata utilizzata una blanda sedazione in accordo con i principi della monitored anaesthesia care ( mac ) ( stata utilizzata una combinazione di propofol , midazolam e fentanyl con dosaggio variabile in base al peso del paziente e alla durata della procedura )  . 
 la saturazione dellossigeno , la pressione arteriosa e il ritmo cardiaco sono stati monitorati in tutti i pazienti . procedura la procedura stata eseguita sotto guida ecografica ( atl 5000 e iu22 philips , best , the netherlands ) , 26 pazienti sono stati trattati nellunit di radiologia interventistica del reparto di radiologia e 4 nei rispettivi reparti , al letto del paziente . 
il colecistogramma stato eseguito iniettando manualmente 10 ml di contrasto opportunamente diluito con soluzione fisiologica sotto guida fluoroscopica ( half contrast media : iopamiro , bracco , milano , italia ; half saline solution )  . 
le complicanze relative alla procedura sono state differenziate in maggiori e minori in accordo con i criteri della societ di radiologia interventistica ( sir ) ( tabella 1 )  . analisi statistica i dati demografici sono stati espressi come mediana ( range ) , radiol med ( 2012 ) 117 : 772779 mentre gli altri dati sono stati espressi come mediaerrore standard ( se )  . 
i dati sono stati analizzati utilizzando un software statistico ( excel , microsoft ; spss per windows , spss )  . risultati il successo tecnico stato del 100% ( 30 / 30 )  . 
let media dei pazienti era 78 anni ( range 5797 ) , il rapporto maschi / femmine era 1 , 31 / 1 ( 17 / 13 ) , la maggior parte dei pazienti ( 93 , 3% , n = 28 / 30 ) aveva dolore alla palpazione in ipocondrio destro . 
escherichia coli stato il solo batterio trovato nella bile di 16 / 26 ( 61 , 5% ) pazienti , mentre nei rimanenti 7 / 26 ( 26 , 9% ) pazienti stato trovato in associazione con enterobacter . 
il tempo medio di ospedalizzazione stato di 8 giorni ( 420 giorni ) e il periodo medio di cateterizzazione stato di 23 giorni ( 1434 giorni ) , in tutti i pazienti stato rimosso il catetere dopo questo periodo . non ci sono state complicanze maggiori o decessi relativi alla procedura . 
procedure - related complications were recorded and differentiated into major and minor according to the criteria of the society of interventional radiology ( table 1 )  . statistical analysis demographic data are given as medians ( range ) , whereas other data are expressed as meansstandard error ( se )  . 
data were analysed using statistical software ( excel , microsoft ; spss for windows , spss )  . results discussione technical success was 30 / 30 ( 100% )  . 
the mean wbc on admission ( 19.87101.6110 / l ) , axilla colecistostomia percutanea stata proposta come trattamento alternativo alla chirurgia ( colecistectomia ) in tutti quei pazienti con colecistite acuta anziani , con alti fattori di rischio e / o critici con associate importanti comorbilit . 
 median hospitalisation time was 8 days ( 420 days ) , and median catheterisation period was 23 days ( 1434 days ) , the catheter being removed in all patients after this period . there were no major complications or procedure - related death . 
2 puntura effettuata mediante ago 18 g . discussion in critically ill or elderly patients at high risk , pc can be proposed as an alternative to surgery ( cholecystectomy ) for treating acute cholecystitis . 
although cholecystectomy remains the definitive operation for acute cholecystitis , its mortality rates in patients with septic shock or multisystem organ failure is unacceptably high [ 3 , 9 ]  . in our study , pc was technically successful in 100% of [ 8 ]  . 
sebbene la colecistectomia rimane lintervento di prima scelta nella colecistite acuta , la mortalit di questo intervento nei pazienti che hanno uno shock settico o uninsufficienza multiorgano ( mof ) inaccettabilmente alta [ 3 , 9 ]  . nel nostro studio la colecistostomia percutanea ha avuto un successo tecnico del 100% , confermando gli ottimi risultati pubblicati in letteratura [ 1012 ]  . 
4 posizionamento di catetere di drenaggio calibro 8 f con apice a pigtail nel lume colecistico . patients , confirming the good results recently published in the literature [ 1012 ]  . 
probably , the absence of bile leakage and colonic injury in our series is due to the transhepatic approach to the gallbladder , an approach that offers the additional benefit of promoting fibrin - sheath formation and facilitating earlier catheter removal [ 20 ]  . 
although this approach carries a potential risk of pneumothorax , intrahepatic bleeding or haemobiliary fistula [ 18 , 20 ] , none of these complications were seen in our series . 
probabilmente lassenza delle complicanze descritte nella nostra casistica dovuta allapproccio transepatico della colecisti , unaltro beneficio di questo approccio quello di promuovere la formazione del tappo di fibrina , pertanto una precoce rimozione del catetere [ 20 ]  . 
 di contro questo tipo di approccio ha un rischio potenzialmente alto di pneumotorace , di sanguinamento intraepatico o di fistola emato - biliare [ 18 , 20 ] ; nei nostri casi nessuna di queste complicanze si per verificata . 
solitamente i pazienti che sono stati trattati in acuto mediante colecistostomia percutanea sono eleggibili per una colecistectomia laparoscopica in elezione , tuttavia per i pazienti con alto rischio chirurgico / anestesiologico lapproccio percutaneo rimane lunico trattamento possibile . nel nostro studio , in accordo con quanto riportato da welschbillig - meunier et al . 
 [ 22 ] il 90% dei pazienti trattati mediante approccio percutaneo hanno avuto un miglioramento clinico entro 4 giorni , ci conferma lefficacia del trattamento in acuto della colecistite , tuttavia stato ripor778 radiol med ( 2012 ) 117 : 772779 laparoscopic cholecystectomy was therefore performed in patients able to safely undergo surgery , even though the recurrence rate of acute calculous cholecystitis has been reported to be approximately 25% [ 20 ]  . managing patients after the acute cholecystitis period is controversial . 
 elective surgery has a lower mortality rate ( 12% ) than emergency surgery ( 646% ) for aged patients with acute cholecystitis [ 24 , 25 ] in elderly patients who are inappropriate surgical candidates because of severe concomitant systemic diseases or terminal malignancies , less invasive treatments , such as percutaneous cholecystolithotomy [ 26 ] and long - term gallbladder drainage [ 18 ] may prevent recurrence . 
 expectant conservative management may be justified , as pc is an excellent option for treating recurrent cholecystitis . tato un tasso di recidiva di colecistite acuta litiasica pari al 25% [ 20 ]  . 
 la chirurgia in elezione del paziente anziano con colecistite acuta ha mostrato un tasso minore di mortalit ( 1% 2% ) rispetto al trattamento chirurgico eseguito in urgenza ( 6%46% ) [ 24 , 25 ]  . 
nei pazienti anziani con gravi malattie sistemiche associate o con patologia neoplastica terminale , dove non effettuabile un intervento chirurgico , i trattamenti meno invasivi come la litotomia colecistica percutanea [ 26 ] o il drenaggio a lungo termine [ 18 ] rimangono i trattamenti di scelta per prevenire le recidive . 
 conclusioni conclusions although our patient series was small , we conclude that pc is a fast , easy and effective treatment method for the acute phase of cholecystitis in elderly and critically ill patients . 
conservative treatment for patients who are not suitable for surgery is acceptable . in conclusione la colecistostomia percutanea , nonostante il numero limitato di pazienti del nostro campione , un metodo di trattamento veloce , semplice ed efficace per la cura della colecistite acuta nei malati critici e nei pazienti anziani . 
la morbilit relativa alla procedura e la mortalit sono molto basse se comparate alla chirurgia tradizionale , inoltre il trattamento percutaneo , nei pazienti con controindicazioni alla chirurgia , ben tollerato . 
the transition point was identified in 89 patients ( 94% ) ; morphology in relation to the proximal loop was concave in 64 cases ( 68% ) , linear in five ( 5% ) and convex in 20 ( 21% )  . 
concave transition - point morphology was indicative of a nonneoplastic condition , with sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy values of 89% , 100% , 100% , 74% and 92% , respectively . 
il punto di transizione era evidente in 89 pazienti ( 94% ) e la sua morfologia rispetto allansa a monte era concava in 64 pazienti ( 68% ) ; lineare in 5 ( 5% ) ; convessa in 20 ( 21% )  . 
una morfologia concava del punto di transizione risultata indicativa di una condizione non neoplastica , con valori di sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) ed accuratezza diagnostica rispettivamente di 89% , 100% , 100% , 74% e 92% . 
 750 radiol med ( 2012 ) 117 : 749758 parole chiave occlusione intestinale tcmd punto di transizione introduction introduzione bowel obstruction is a frequent cause of acute abdomen , accounting for approximately 2025% of cases [ 1 ]  . 
obstruction of the normal bowel lumen is located within the small bowel in 60% of cases and often consists of postoperative adhesions , which account for 5080% of cases ; hernias are responsible for 10% , and crohns disease , neoplasms and other causes are less frequent [ 1 , 2 ]  . 
large - bowel obstruction is less common and has different aetiology ( mostly neoplastic ) , pathophysiology , treatment and prognosis , with a mortality rate of around 20% [ 3 ]  . 
when bowel obstruction is suspected , plain abdominal radiography is often the imaging method of choice as it can detect obstruction in 5084% of cases , is doubtful in 2030% and normal , nonspecific or incorrect in 1020% [ 411 ]  . 
given its diagnostic potential , this method is conclusive in some cases but is often inadequate for defining the nature of an obstruction and detecting possible ischaemic complications [ 12 ]  . 
 multidetector computed tomography ( mdct ) is considered a fundamental modality in the study of patients with suspected bowel obstruction , thanks to its accuracy in demonstrating site , level and cause of obstruction and ruling out possible ischaemic complications [ 13 , 14 ]  . 
a recent report highlighted the diagnostic value of a new ct sign , dubbed protruding lips sign , and based on the morphology of neoplastic tissue that protrudes into the dilated bowel loop upstream of the stenosis , ct can define the neoplastic nature of a bowel obstruction [ 15 ]  . the purpose of our work was to verify the different transition - point appearances and consider their possible diagnostic contribution in defining the nature of bowel obstruction . materials and methods we retrospectively reviewed ct scans of 95 patients ( 33 men , 62 women ; age range 4376 years ; mean age 61 years ) affected by surgically controlled bowel obstruction and studied between january 2010 and december 2010 . 
ct scans had been acquired on an emergency basis owing to development of acute abdomen caused by probable obstruction after plain abdominal radiography in 68 cases and as a first - line examination in 27 . 
patients were identified by searching our electronic radiology relocclusione intestinale una causa frequente di addome acuto e ne determina la comparsa in circa il 20%25% dei casi [ 1 ]  . 
lostacolo alla canalizzazione intestinale localizzato in corrispondenza del tenue nel 60% dei casi ed pi spesso determinato da aderenze post - operatorie che incidono nel 50%80% dei casi , ernie in circa il 10% e meno frequentemente da morbo di crohn , patologia neoplastica ed altro [ 1 , 2 ]  . 
lostruzione del colon meno frequente e differisce per eziologia , nella gran parte dei casi di origine neoplastica , fisiopatologia , terapia e prognosi , con un tasso di mortalit di circa il 20% [ 3 ]  . 
nel sospetto di occlusione intestinale lesame radiografico ( rx ) diretto delladdome , spesso , la prima indagine che viene eseguita ed in grado di riconoscere la presenza di unocclusione nel 50%84% , risulta dubbia nel 20%30% , normale , non specifica o erronea nel 10%20% dei casi [ 411 ]  . 
tale indagine , pertanto , per le sue potenzialit diagnostiche , in alcuni casi risolutiva , ma spesso inadeguata per definire la natura di unocclusione e per ricercare eventuali complicanze ischemiche [ 12 ]  . la tomografia computerizzata multidetettore ( tcmd ) ormai considerata una metodica fondamentale nella valutazione del paziente con sospetta occlusione intestinale , per la sua accuratezza nel dimostrare la sede , il livello e la causa dellostruzione e per escludere eventuali complicanze ischemiche associate [ 13 , 14 ]  . 
recentemente , nella definizione della natura neoplastica di unostruzione intestinale , stato sottolineato il valore diagnostico di un nuovo segno tc , definito labbra sporgenti , che si basa sulla caratteristica morfologia del tessuto neoplastico che protrude nellansa intestinale dilatata a monte della stenosi [ 15 ]  . scopo del presente lavoro valutare la differente morfologia del punto di transizione e considerare leventuale contributo diagnostico nella definizione della natura di unocclusione intestinale . materiali e metodi sono stati valutati retrospettivamente gli esami tc di 95 pazienti ( 33 uomini , 62 donne ) , di et compresa tra 43 e 76 anni ( et media 61 anni ) , studiati tra gennaio 2010 e dicembre 2010 , affetti da occlusione intestinale , controllata chirurgicamente . 
lesame tc stato eseguito in regime di urgenza per la comparsa di addome acuto da probabile occlusione , dopo un esame rx radiol med ( 2012 ) 117 : 749758 cords using key words such as surgically treated bowel obstruction ct . in the 71 patients with small - bowel obstruction , the obstruction was secondary to nonneoplastic disease in 66 ( 42 due to adhesions , eight to hernia , seven to crohns disease , two to endometriosis , six to volvulus , one to invagination ) and to malignancy in five cases ( one carcinoma , one metastasis from melanoma , three extrinsic neoplastic infiltrations )  . 
among the 24 patients with large - bowel obstruction , six cases were of nonneoplastic origin ( two due to volvulus , two to adhesions , two to diverticulitis ) and 18 cases were of malignant origin ( 17 adenocarcinomas , one extrinsic neoplastic infiltration )  . 
scans were always acquired before and after intravenous administration of a contrast agent ( 120140 ml injected at a rate of 33.5 ml / s ) , with image acquisition during the arterial phase with scan delay from 30 to 40 s from the beginning contrast - agent administration and during the venous phase with scan delay from 60 to 70 s from beginning of contrast - agent administration . 
axial and reconstructed images were blindly analysed by two independent experienced radiologists who assessed the images for the following parameters : evidence of signs of bowel obstruction [ 5 ] ; identification of the site of obstruction ; morphology of the transition point ( identified as concave , linear or convex with respect to the dilated loop upstream of the stenosis )  . any disagreement was resolved in consensus . statistical analysis diretta delladdome in 68 casi e come prima indagine in 27 . 
 i pazienti sono stati identificati ricercando nel nostro archivio radiologico computerizzato alcune parole chiave come occlusione intestinale trattata chirurgicamente tc . nei 71 pazienti con unocclusione del piccolo intestino , lostacolo era secondario a patologia non neoplastica in 66 casi ( 42 briglie aderenziali , 8 ernie , 7 morbo di crohn , 2 endometriosi , 6 volvoli , 1 invaginazione ) ed a patologia neoplastica maligna in 5 casi ( 1 carcinoma , 1 metastasi da melanoma , 3 infiltrazioni neoplastiche ab - estrinseco )  . 
nei 24 pazienti con unocclusione del grosso intestino si trattava in 6 casi di patologia non neoplastica ( 2 volvoli , 2 briglie aderenziali , 2 diverticoliti ) ed in 18 casi di patologia neoplastica maligna ( 17 adenocarcinomi , 1 infiltrazione neoplastica ab estrinseco )  . 
complessivamente , quindi , la casistica esaminata comprendeva 23 occlusioni da patologia neoplastica maligna e 72 occlusioni da patologia non neoplastica . gli esami tc sono stati eseguiti con apparecchiature tcmd a 320 strati ( aquilion one , toshiba medical system , tokio , giappone ) , tcmd a 16 strati ( tsx - 101aaquilion 16 , toshiba medical system , tokio , giappone ) , utilizzando , rispettivamente , i seguenti parametri di acquisizione : spessore di strato 0 , 5 e 1 ; incremento 0 , 5 e 0 , 8 mm ; tempo di rotazione del tubo 0 , 5 s ; kv / mas 120 / 250 ; matrice 512512 . 
 in tutti i casi sono state eseguite scansioni prima e dopo iniezione endovenosa di mezzo di contrasto ( 120140 ml iniettati alla velocit di 33 , 5 ml / s ) , con acquisizione delle immagini in fase arteriosa , con ritardo compreso tra 3040 s dallinizio della somministrazione del mezzo di contrasto , ed in fase venosa , con ritardo compreso tra 6070 s dallinizio della somministrazione del mezzo di contrasto . 
le immagini assiali e quelle ricostruite sono state analizzate in cieco da due radiologi esperti indipendenti , considerando i seguenti parametri : evidenza dei segni di occlusione intestinale [ 5 ] ; definizione della sede della ostruzione ; morfologia del punto di transizione della stenosi ( differenziata , rispetto allansa dilatata a monte della stenosi , in concava , lineare , o convessa )  . eventuali differenze di valutazione sono state risolte in the series was first analysed with descriptive statistics by considering age , gender , disease aetiology ( neoplastic or nonneoplastic ) and calculating their percentage values . 
 subsequently , in order to verify the value of transition - point consenso . 752 radiol med ( 2012 ) 117 : 749758 morphology , we calculated sensitivity , specificity , diagnostic accuracy and positive ( ppv ) and negative ( npv ) predictive values in the study population . 
statistical analysis was done with ncss 2007 software . results obstruction site was identified in 89 patients and was not recognised in six ( 6% ) ; in these six cases , transition - point morphology was considered undetermined . 
a analisi statistica lanalisi del nostro campione stata eseguita dapprima mediante statistica descrittiva , esaminando et , sesso , eziologia della patologia ( neoplastica o non neoplastica ) e calcolando i relativi valori percentuali . 
successivamente , al fine di verificare la validit della morfologia del punto di transizione , nei gruppi di pazienti esaminati , sono stati valutati i valori di sensibilit , specificit , accuratezza diagnostica ( ad ) , valore predittivo positivo ( ppv ) e valore predittivo negativo ( npv )  . 
 il grado di concordanza tra i due lettori stata valutato mediante test statistico di kappa di cohen : scarsa concordanza ( k < 0 , 01 ) , bassa concordanza ( k = 0 , 010 , 20 ) , discreta concordanza ( k = 0 , 210 , 40 ) , buona concordanza ( k = 0 , 41 0 , 60 ) , sostanziale concordanza ( k = 0 , 610 , 80 ) , concordanza quasi perfetta ( k = 0 , 811 , 00 )  . 
per lanalisi statistica stato utilizzato il software ncss 2007 . risultati la sede dellocclusione stata definita in 89 pazienti ed risultata non riconoscibile in 6 ( 6% ) ; in tali casi , la morfologia del punto di transizione stata considerata indeterminata . 
considerando la morfologia del punto di transizione , stato riscontrato un aspetto concavo in 64 pazienti ( 68% ) ; una morfologia lineare in 5 casi ( 5% ) ; un aspetto convesso in 20 casi ( 21% )  . 
dallanalisi statistica dei dati ottenuti , pertanto , una morfologia del punto di transizione di tipo concavo si dimostrata indicativa di una condizione non neoplastica , con valori di sensibilit del 89% , specificit del 100% , valore predittivo positivo del 100% , valore predittivo negativo del 74% ed accuratezza diagnostica del 92% . 
infine , un punto di passaggio convesso risultato correlato a patologia neoplastica , con valori di sensibilit , specificit , valore predittivo positivo , valore predittivo negativo ed accuratezza diagnostica rispettivamente pari a fig . 
a , b transverse scans : carcinoma of the pancreatic tail ( arrows ) ; c coronal reconstruction ; d sagittal reconstruction ; colonic loops are considerably dilated ( * )  . 
lastly , in the six cases with indeterminate transition point , the cause was always nonneoplastic ( six adhesions ) , and the failure to define transition - point 87% , 100% , 100% , 96% e 97% . 
nei 6 pazienti in cui la morfologia del punto di passaggio risultata indeterminata si trattava sempre di occlusioni non neoplastiche del tenue , generate da briglie aderenziali e la mancata definizione della morfologia del punto di transizione era determinata dalla presenza di anse dilatate conglomerate tra loro . radiol med ( 2012 ) 117 : 749758 il grado di concordanza tra i due radiologi risultato morphology was due to the presence of a conglomerate of dilated loops . 
statistical analysis therefore indicates that a concave transition point implies a nonneoplastic condition , with 89% sensitivity , 100% specificity , 100% ppv , 74% npv and 92% diagnostic accuracy . 
a convex shape correlated with malignancy , with sensitivity , specificity , ppv , npv and accuracy values of 87% , 100% , 100% , 96% and 97% , respectively . 
a comparative study [ 1 ] of ct , ultrasound ( us ) and plain abdominal radiography in detecting bowel obstruction reported sensitivity and specificity values of 93% and 100% , respectively , for ct ; 83% and 100% for us ; and 77% and 50% for radiography . 
finally , accuracy in defining the nature of obstruction was 87% for ct , 23% for us and 7% for abdominal radiography . ct detection of obstruction is based on identifying dilated proximal loops and collapsed distal loops [ 5 , 6 , 16 ] ; definition of obstruction site requires establishing where there is a change in bowel - loop calibre ; that is , locating the transition point [ 5 ]  . 
mpr allows visualisation of the obstruction site in different planes and consequently provides optimal depiction of the transition point [ 3 , 1921 ] , with accuracy values of 9093% [ 21 ]  . 
in our experience , transition - point morphology was evaluated in 94% of cases with the axial images and mpr reconstructions . another change to be assessed in order to define obstruction site is represented by the faeces sign [ 22 ] , produced by the possible presence of particulate matter inside a dilated small - bowel loop immediately above the transition point [ 23 , 24 ]  . 
this sign , however , has a low prevalence ( 78% approximately ) and may also be present in patients with no obstruction at all . once the obstruction has been detected and located , its nature needs to be defined . 
the causes of an obstruction may be classified as extrinsic , intraluminal or intrinsic , and multidetector ct has a 9395% diagnostic accuracy in deliter diagnostico di unocclusione intestinale si basa inizialmente sulla valutazione clinica del paziente , ma fondamentale il contributo della diagnostica per immagini per stabilirne la presenza , definire la sede e la natura dellostruzione e ricercare eventuali complicanze . 
in uno studio comparativo [ 1 ] tra le possibilit della tc , ecografia ( us ) e rx diretta delladdome nel riconoscimento di occlusione intestinale , i valori di sensibilit e specificit riportati sono stati rispettivamente di 93% e 100% per la tc , 83% e 100% per lus , 77% e 50% la rx diretta delladdome . 
 la diagnosi tc di occlusione si basa sullidentificazione di anse prossimali dilatate e di anse distali collabite [ 5 , 6 , 16 ] , mentre per definirne la sede fondamentale stabilire il punto ove si determina la variazione di calibro delle anse intestinali , cio la zona di transizione [ 5 ]  . 
le ricostruzioni mpr consentono di valutare la sede dellostruzione secondo differenti piani e , pertanto , facilitano la visualizzazione della zona di transizione [ 3 , 1921 ] , con valori di accuratezza compresi tra 90% e 93% [ 21 ]  . 
nella nostra esperienza , il riconoscimento della morfologia del punto di transizione stato ottenuto complessivamente nel 94% dei casi , utilizzando le immagini assiali e le ricostruzioni mpr . unaltra alterazione da valutare per ricercare la sede dellostruzione rappresentata dal segno delle feci [ 22 ] , determinato dalla possibile presenza di materiale strutturato allinterno di unansa del tenue dilatata , subito a monte della zona di transizione [ 23 , 24 ]  . 
tale segno , tuttavia , ha una bassa prevalenza ( circa 7%8% ) e pu essere presente anche in pazienti senza occlusione . dopo aver diagnosticato la presenza dellocclusione e localizzato la sede , occorre necessariamente stabilire la natura dellostacolo . 
le cause di unocclusione possono essere distinte in estrinseche , intraluminali ed intrinseche , e nella loro definizione la tcmd presenta unaccuratezza diagnostica del 93%95% [ 15 , 25 , 26 ]  . 
le occlusioni da patologia intraluminale in rapporto a calcoli biliari , fitobezoari e fecalomi sono facili da riconoscere e non rientrano tra le situazioni in cui indicata la valutazione del punto di transizione . 
le occlusioni da patologia intrinseca od estrinseca sono molto varie e talora la loro precisa identificazione pu essere 756 radiol med ( 2012 ) 117 : 749758 fining the cause [ 15 , 25 , 26 ]  . 
in particular , small - bowel obstruction of intrinsic origin may be caused by adenocarcinoma , crohns disease , radiation - induced enteropathy and , rarely , by intramural haematoma and eosinophilic gastroenteritis [ 5 ] ; large - bowel obstruction is most often caused by adenocarcinoma and , less frequently , diverticulitis , crohns disease and other chronic inflammatory diseases [ 3 ]  . 
in obstructions of intrinsic origin , a circumscribed wall thickening is seen in the transition zone [ 6 , 26 ] , which is stratified in nonneoplastic obstructions [ 19 ] and sharply defined and irregular in neoplastic obstructions [ 27 ]  . 
however , in the case of intrinsic stenosis , the differential diagnosis between neoplastic and inflammatory stenosis may sometimes be complex [ 3 , 7 ] , even though it is decisive for a correct therapeutic approach . 
in extrinsic obstructions , diagnosis is usually straightforward when extrinsic neoplastic infiltrations or hernias are present , whereas it may be difficult in the presence of adhesions , which are only diagnosed when there are no evident wall alterations at the site of the stenosis . 
 in order to define the nature of an obstruction , studying the transition point ( classified as concave , linear or convex ) has been proposed , in addition to the known signs and symptoms . 
this morphological evaluation is very easy to perform and was possible in 94% of our patients ; that is , in all patients in whom the transition zone was recognisable . 
 our results indicate that a concave transition point is always associated with nonneoplastic disease ( adhesions , hernias , crohns disease , endometriosis , volvulus ) , with 100% ppv , 100% specificity , 89% sensitivity and 92% diagnostic accuracy . 
a convex transition point , also called protruding lips sign [ 15 ] , is strongly indicative of a malignant lesion [ 28 , 29 ] , with 100% specificity and ppv , and sensitivity , npv and diagnostic accuracy values of 87% , 96% and 97% , respectively . 
in particolare , le occlusioni intestinali da causa intrinseca possono essere determinate a livello del tenue da adenocarcinoma , morbo di crohn , enteropatia da radiazioni e raramente da ematoma intramurale e gastroenterite eosinofila [ 5 ] ; a livello del colon , sono pi spesso causate da adenocarcinoma e , pi raramente , da diverticolite , morbo di crohn ed altre malattie infiammatorie croniche [ 3 ]  . 
nelle occlusioni da patologia intrinseca , nella zona di transizione compare un circoscritto ispessimento parietale [ 6 , 26 ] , stratificato nelle occlusioni non neoplastiche [ 19 ] , brusco ed irregolare in quelle neoplastiche [ 27 ]  . 
talora , comunque , nelle stenosi intrinseche , la diagnosi differenziale tra stenosi neoplastiche e stenosi infiammatorie pu essere complicata [ 3 , 7 ] , anche se determinante per un corretto approccio terapeutico . 
nelle occlusioni da cause estrinseche , la diagnosi generalmente agevole in presenza di infiltrazioni neoplastiche ab estrinseco o di ernie , mentre pu essere difficile quando in rapporto a briglie aderenziali , diagnosticate soltanto in assenza di evidenti alterazioni parietali nella sede della stenosi . 
dai risultati ottenuti , emerge che la morfologia concava della parete intestinale nel punto di passaggio si associa , in tutti i casi , ad una patologia non neoplastica ( briglie aderenziali , ernie , morbo di crohn , endometriosi , volvolo ) con valore predittivo positivo del 100% , specificit del 100% , sensibilit del 89% ed accuratezza diagnostica del 92% . 
lassenza di tale segno , tuttavia , non esclude la presenza di una occlusione non neoplastica , come deducibile dal valore predittivo negativo ottenuto nel campione , pari al 74% . 
il punto di transizione di aspetto lineare non discriminante tra eziologia neoplastica ( 60% ) e non neoplastica ( 40% ) , poich presenta unincidenza pressoch sovrapponibile nelle due forme . 
laspetto convesso del punto di transizione , altres denominato segno delle labbra sporgenti [ 15 ] , fortemente indicativo di una lesione eterologa maligna [ 28 , 29 ] , con specificit e valore predittivo positivo del 100% , sensibilit , valore predittivo negativo ed accuratezza diagnostica rispettivamente del 87% , 96% e 97% . 
infine , una morfologia del punto di passaggio di tipo indeterminato , causata dalla presenza di anse dilatate conglomerate tra loro , si associata sempre ad occlusione da briglie aderenziali , ma tale reperto stato riconosciuto in un numero troppo esiguo di paziente ed pertanto meritevole di ulteriori approfondimenti . la nostra ricerca avvalora il contributo diagnostico radiol med ( 2012 ) 117 : 749758 although our study was limited by its retrospective nature and the fact that only high - grade stenoses requiring surgical treatment were included , it confirms the diagnostic contribution of transition - point analysis . dellanalisi del punto di transizione , ma presenta alcuni limiti , rappresentati dallessere retrospettiva e dallavere considerato soltanto stenosi di alto grado , meritevoli di un trattamento chirurgico . conclusions conclusioni ct is an accurate technique for identifying the nature of bowel obstructions . 
in particolare , una morfologia concava indica , con elevato grado di probabilit , una condizione non neoplastica , mentre una morfologia convessa fortemente indicativa di una patologia di tipo neoplastico . 
knauth springer - verlag berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 0978 - 3 - 540 - 73270 - 9 e - isbn 978 - 3 - 540 - 73271 - 6 published online : 7 january 2012 springer - verlag 2012 this 518 page , 28 chapter book is dedicated to the ever increasing importance of magnetic resonance imaging ( mri ) in fetal imaging . 
 sia nelle introduzioni che nella prefazione viene puntulizzato come la rm fetale sia divenuta uno strumento pratico e molto importante nella diagnosi fetale a seguito dellintroduzione di sequenze di acquisione rapida delle immagini [ half - fourier single - shot sequences ( haste ) , single shot fast spin echo ( ssfse ) ] cui sono da aggiungere le tecniche eco - planari e le immagini pesate in diffusione . quattro capitoli sono cos dedicati alla presentazione , discussione e modalit di impiego delle differenti tecniche di rm che permettono la corretta visualizzazione dello sviluppo fetale e della maturazione cerebrale senza dimenticare le condizioni psicologiche della gestante . a questa introduzione tecnica segue un capitolo molto lungo ( quasi un piccolo volumetto nel volume con le sue 65 pagine , 21 delle quali dedicate alla bibliografia ! ) dedicato allo sviluppo prenatale del telencefalo fetale . 
infatti , senza una ben precisa e completa informazione e conoscenza dello sviluppo cerebrale , sar impossibile valutare correttamente immagini riprese in tempi diversi della gestazione e di conseguenza porre una diagnosi corretta da offrire ai pazienti ed ai curanti . il fatto che i movimenti embrionali e fetali giochino un ruolo molto importante nello sviluppo armonico e corretto dei sistemi musculo - scheletrico e neurale viene discusso nei dettagli in un capitolo apposito : senza una motilit fetale adeguata non v sviluppo fetale corretto . i due capitoli successivi sono dedicati alla discussione radiol med ( 2012 ) 117 : 898899 the following two chapters are dedicated to the discussion of ultrasound ( us , always the first diagnostic step in pregnancy evaluation ) or mri in fetal neuroimaging , and to the multidisciplinary approach to the fetal neurologic clinic , which provides the best end - results for fetal well - being . eleven ensuing chapters are dedicated to single organ presentation and discussion , from normal fetal lung to fetal heart mri , from mri of fetal endocrine glands to facial clefts , cerebral malformations , acquired brain pathology , congenital diaphragmatic hernia and its related lung problems and proper treatment ( fetal endoscopic tracheal occlusion in order to increase lung volume ) , to mri of the pathologic fetal thorax and abdomen . due to the fact that the placenta plays an important role in fetal well - being , quite a long chapter ( enriched by beautiful full size and pathological specimen images ) is devoted to its development and pathology . the last chapters deal with the problems of multiple pregnancies , fetal / perinatal autopsy and mri , post - mortem mri of the fetus , genetics of fetal disease and close with maternal disease and its possible impact on pregnancy . under the supervision of prof . 
prayer , a well - known authority in the field , all chapters are written by experts , reporting not only on the experience of medical groups from vienna but also by other european teams . 
to properly point to and highlight the addressed problem ( being pernickety : why are black arrows and asterisks used to pin - point problems on black t1 - weighted images ? )  . 
 hints are given all throughout the book on how to properly deal with mothers and parents who , after an us , are sent to the mri suite in order to further delineate and study a suspected fetal malformation , a situation of severe parental distress to be properly addressed by the medical mri tea in conclusion , this is a bench - book for all those who are devoted to fetal mri , a state - of - the art tool for radiologists , obstetricians , gynecologists and paediatricians . sullimpiego dellecografia ( sempre la prima tappa nella valutazione della gravidanza ) o della rm nello studio delle neuroimmagini fetali ed allapproccio multidisciplinare alla clinica neurologica fetale che fornisce i migliori risultati per il benessere del feto . 
 undici capitoli sono poi dedicati alla presentazione e discussione del quadro rm di un singolo organo , dal polmone al cuore fetale , dalle ghiandole endocrine alle fissurazioni facciali , alle malformazioni cerebrali , alla patologia encefalica acquisita , allernia diaframmatica [ con i relativi problemi polmonari ed il loro trattamento ( occlusione tracheale fetale endoscopica onde aumentare il volume polmonare ) ] , al torace ed alladdome patologico fetale . dal momento poi che la placenta riveste un ruolo molto importante per il benessere fetale , un capitolo piuttosto lungo , arricchito da bellissime immagini a tutto campo della stessa e da salienti quadri anatomo - patologici , viene dedicato al suo sviluppo e patologia . gli ultimi capitoli trattano i problemi riguardanti luso della rm nelle gravidanze multiple , nellautopsia fetale / perinatale , nello studio post - mortem del feto , nonch le malattie genetiche fetali , per chiudere con le malattie materne che possono avere un qualche impatto sulla gravidanza . 
 sotto la supervisione della prof.ssa prayer , ben nota autorit nel campo , tutti i capitoli sono scritti da esperti , che descrivono non solo lesperienza dei gruppi medici di vienna ma anche di altri gruppi europei . largomento in esame non facile n semplice da studiare e digerire , soprattutto per chi non abbia uninfarinatura dello stesso . 
with growing experience , however , the spectrum of midand long - term complications has broadened to include potentially disastrous events , other than paraplegia or stroke , that require diligent surveillance . 
three - dimensional data sets acquired quickly by multidetector computed tomography ( mdct ) allow multiplanar reformations and 3d viewing , as well as quantitative assessment of vessel lumens , walls and surroundings . 
accordingly , the goal of this report is to summarise our experience with the presentation , diagnostic approach , management and outcomes of these unusual , but potentially catastrophic , postendovascular aortic repair complications to highlight their significance and increase familiarity with them among the imaging community . 
increasing awareness of these complications may facilitate rapid diagnosis and / or triage and treatment . riassunto il posizionamento di protesi endovascolari una tecnica ampiamente accettata ed utilizzata in alternativa alla chirurgica tradizionale nel trattamento della patologia aortica e sta divenendo , soprattutto in determinate patologie , la modalit terapeutica di scelta . 
con la crescente esperienza , tuttavia , lo spettro delle complicanze a medio e lungo termine si ampliato fino ad includere eventi potenzialmente disastrosi , diversi dalla paraplegia o dallictus , che richiedono unattenta sorveglianza . 
i set di dati tridimensionali acquisiti rapidamente dalla tomografia computerizzata multidetettore consentono ricostruzioni multiplanari e la visualizzazione 3d delle protesi , cos come la valutazione quali - / quantitativa dei lumi , delle pareti vasali e del tessuto periaortico . 
however , it was not until a decade later that the us food and drug administration ( fda ) approved the first commercial endograft for use in the thoracic aorta [ 3 ]  . with the development of minimally invasive surgical techniques , endovascular stent - graft placement has become an accepted and widely used alternative to the traditional surgical repair of aortic disease and is gaining acceptance as the treatment of choice in some diseases [ 412 ]  . 
common thoracic aortic pathologic conditions amenable to stent placement include degenerative and posttraumatic aortic aneurysm , aortic rupture , pseudoaneurysm , traumatic transections , penetrating atherosclerotic ulcer ( pau ) , intramural haematoma ( imh ) , congenital abnormalities and dissection [ 1319 ]  . 
many studies show that endovascular stent - graft therapy is safe and effective [ 415 ] , with satisfactory short and midterm ( up to 5 years ) results [ 20 , 21 ] , although complications related to this treatment are also recognised [ 22 33 ]  . 
potential and more common complications of endovascular stent placement include endoleaks , stent migration , pseudoaneurysms , aortic perforation , kinking , thrombosis , coverage of vital branch vessels with left upper - extremity ischaemia , distal embolisation , stroke and intestinal and spinal cord ischaemia [ 2232 ]  . 
accurate detection and classification of endoleaks is essential for its proper management [ 14 , 22 , 30 ] ; type i endoleaks are the most common in tevar [ 7 , 11 , 14 , 15 ]  . 
cross - sectional radiological imaging plays a crucial role in evaluating a patients candidacy for planning the intervention and assessing postprocedural results and complications of tevar [ 3436 ]  . 
three - dimensional ( 3d ) high - resolution data sets acquired quickly by mdct allow multiplanar reformations ( mprs ) and 3d viewing , as well as quantitative assessment il trattamento endovascolare dellaneurisma dellaorta addominale ( evar ) stato descritto per la prima volta da parodi et al . 
tuttavia , fu solo un decennio pi tardi che la food and drug administration ( fda ) approv la prima endoprotesi commerciale da utilizzare nel tratto toracico del vaso [ 3 ]  . 
 con lo sviluppo di tecniche chirurgiche mini - invasive , limpianto di protesi endovasali una alternativa ampiamente utilizzata alla classica chirurgia aortica open ed ora si sta affermando come trattamento di elezione in alcune condizioni morbose del vaso [ 412 ]  . 
patologie dellaorta toracica suscettibili di terapia con stent endovasale comprendono gli aneurismi degenerativi e post - traumatici , la rottura aortica , lo pseudoaneurisma , le transezioni traumatiche , lulcera aterosclerotica penetrante ( pau ) , lematoma intramurale ( imh ) , le anomalie congenite e la dissezione [ 13 19 ]  . 
molti lavori dimostrano che la terapia endoprotesica sicura ed efficace [ 415 ] , con risultati soddisfacenti [ 20 , 21 ] a breve e medio termine ( fino a 5 anni ) , sebbene siano riconosciute anche complicanze legate a questo trattamento [ 2233 ]  . 
gli eventi avversi potenziali e pi comuni della tevar comprendono gli endoleaks , la migrazione protesica , gli pseudoaneurismi , la perforazione aortica , il kinking , la trombosi , la copertura di branche collaterali vitali ad esempio con ischemia dellarto superiore sinistro , embolizzazione distale , stroke , ischemia enterica e spinale [ 2232 ]  . 
la diagnosi ( e la classificazione ) accurata degli endoleaks essenziale per il loro corretto trattamento [ 14 , 22 , 30 ] ; gli endoleaks di tipo i sono i pi comuni nella tevar [ 7 , 11 , 14 , 15 ]  . 
limaging gioca un ruolo cruciale nella valutazione del paziente candidato al posizionamento dello stent , sia nella pianificazione pre - procedurale che nella valutazione dei risultati della tevar e delle sue complicanze [ 3436 ]  . 
i set di dati tridimensionali ( 3d ) ad elevata risoluzione permettono ricostruzioni multiplanari e la valutazione 3d , cos come diagnosi quali - / quantitative dei lumi vasali , delle pareti e del tessuto perivasale . 
sebbene la gran parte dei radiologi non sia coinvolta direttamente nellimpianto delle endoprotesi , molti si confrontano quotidianamente con linterpretazione degli sturadiol med ( 2012 ) 117 : 831854 of vessel lumens , walls , and surroundings . 
accordingly , the goal of this report is to summarise our experience with risk factors , presentation , diagnostic approach , management and outcomes of some unusual , but sometimes severe or lifethreatening , post - evar adverse events or complications and to increase familiarity with them among the imaging community . 
increasing awareness of these complications may facilitate rapid diagnosis and / or triage and treatment . mdct protocol of study and technical notes our experience ( from 2001 to 2011 ) refers to patients who underwent retrograde transfemoral / transiliac tevar at our institution , a level - ii cardiovascular emergency hospital , and patients transferred from other institutions because of complications or adverse events after stent - graft placement . 
images were obtained with a single - slice toshiba xpress gx ( toshiba medical systems , tokyo , japan ) from 2001 to 2004 , then with 16 - mdct ( brilliance ct 16 - slice philips , healthcare philips medical systems , best , the netherlands ) and 64 - mdct ( lightspeed vct 64 - slice ge , ge medical system , milwaukee , wi , usa )  . 
the study plan covered from the lung apices to the grono contrast agent was administered orally unless there were air findings in endovascular or perivascular soft tissue or in the case of clinical suspicion of bronchial / oesophagealvascular fistula . 
each ct study started with an unenhanced scan of the thorax to evaluate details of stent lumen , geometry , orientation and strut thickness , spontaneous aortic hyperdensity and / or periaortic soft - tissue abnormality . 
when feasible , in selected cases valve plane , aortic root and proximal ascending aorta contrast - enhanced thoracic acquisition was obtained with retrospective electrocardiographic ( ecg ) - gating [ 3638 , 41 , 44 ]  . 
nonionic contrast material ( total volume 60130 ml of low - osmolar contrast medium ) was injected at a rate of 36 ml / s through a 18to 20 - gauge cannula in the right arm , if possible , with a dualdi di follow - up post - impianto . 
pertanto , lobiettivo del presente contributo quello di illustrare la nostra esperienza sui fattori di rischio , sulla presentazione clinica , sullapproccio diagnostico e la gestione di alcuni eventi avversi o complicanze insolite ma talora potenzialmente fatali della terapia endoprotesica dellaorta toracica , al fine di aumentarne la conoscenza nella comunit dellimaging . 
la crescente consapevolezza degli eventi avversi possibili pu facilitarne la pronta diagnosi ed il trattamento . protocollo di studio tcmd e note tecniche la nostra esperienza ( dal 2001 al 2011 ) si riferisce sia a pazienti sottoposti a tevar per via transfemorale / transiliaca presso la nostra azienda ospedaliera , dotata di un centro di emergenza / urgenza cardio - vascolare di ii livello , sia a pazienti trasferiti da altre istituzioni per sopraggiunte complicanze o eventi avversi dopo il posizionamento di endoprotesi aortiche . 
le immagini sono state ottenute con apparecchiature tc single - slice toshiba xpress gx ( toshiba medical systems , tokyo , giappone ) dal 2001 al 2004 , successivamente con una macchina tcmd 16 strati ( brilliance ct 16 - slice philips , healthcare philips medical systems , best , paesi bassi ) e 64 strati ( lightspeed vct 64 - slice ge , ge medical system , milwaukee , wi , usa )  . 
il protocollo di studio costituito da una tipica angiografia tc trifasica : una fase pre - contrastografica , una arteriosa ed una fase tardiva [ 40 , 41 ]  . 
non stato somministrato mezzo di contrasto ( mdc ) per os a meno che non fosse presente aria libera endovasale o nellambito delle parti molli perivasali o nel sospetto clinico di fistola aorto - bronchiale / esofagea . 
ogni esame tc cominciato con una fase pre - contrastografica del torace per valutare i dettagli della protesi , la sua geometria , lorientamento , lo spessore del supporto protesico , qualsiasi spontanea iperdensit aortica e / o anomalie delle parti molli periaortiche . 
la configurazione dei detettori stata di 161 , 5 mm e di 640 , 625 mm con reconstruction index rispettivamente di 1 e 0 , 625 mquesta configurazione tcmd ha prodotto dati volumetrici di alta qualit , con risoluzione isotropica in qualsiasi piano , consentendo ricostruzioni multiplanari e immagini 3d di buona qualit . 
quando possibile lacquisizione contrastografica del piano valvolare , della radice aortica e della porzione prossimale dellaorta ascendente stata ottenuta con sincronizzazione elettrocardiografica ( ecg ) [ 3638 , 41 , 44 ]  . 
il bolo di mdc ( volume totale di 60130 ml di mdc non ionico a bassa osmolarit alla concentrazione di 370 o 400 mgi / ml ) stato iniettato ad una velocit di 36 ml / s attraverso un ago - cannula 1820 g , inserita , se possibile , nel braccio destro , attraverso iniettore a due vie ( stellant sct 211 , medrad , indianola , ia , usa ) , con la tecnica del bolus triggering con unica regione di interesse ( roi ) posizionata nellaorta ascendente o nellarco aortico [ 4548 ] ; il bolo 834 radiol med ( 2012 ) 117 : 831854 barrel power injector ( stellant sct 211 , medrad , indianola , ia , usa )  . 
we used a bolus - triggering technique with a single region of interest ( roi ) positioned in the ascending aorta or in the aortic arch [ 4548 ]  . 
 ct findings of normal endovascular stent most endovascular stents have an inner metallic skeleton made of nitinol , with a characteristic zigzag appearance causing only mild streak artefacts , surrounded by a covering of plastic ( polytetrafluoroethylene ) or polyester graft membrane [ 4 , 6 , 7 , 35 ]  . 
at mdct scans , the metallic framework is easily visualised as a metal - density tubular device surrounded by the diseased aorta and adherent to the wall of normal aorta at both ends of the stent . 
additional postprocessing techniques using a wide window width ( > 500 wl ) , mip and volume - rendered ( vr ) images improve visualisation of the detail of metallic stents [ 38 ]  . when the stent graft is correctly positioned , the diseased portion of the aorta is covered and excluded from the systemic circulation ; at follow - up ct angiography , the endograft should be unchanged in position from that at postoperative angiography and should exclude the entire aortic di contrasto iodato stato seguito di routine dalla soluzione fisiologica ( 2040 ml )  . 
sono create di routine ricostruzioni curvilinee ( cpr ) , post - processing di superficie , proiezioni di massima intensit ( mip ) , immagini bidimensionali oblique e 3d volumetriche . 
 segni tc dellendoprotesi ben posizionata la gran parte delle endoprotesi ha uno scheletro metallico costituito da nitinolo con una caratteristica morfologia a zig - zag causa di solo modesti artefatti a striscia , circondato da una membrana protesica di plastica ( politetrafluoroetilene ) o di poliestere [ 4 , 6 , 7 , 35 ]  . 
tecniche di post - processing aggiuntive utilizzano unampia larghezza di finestra ( > 500 wl ) , la mip ed il volume rendering ( vr ) per migliorare il dettaglio degli stent metallici [ 38 ]  . 
 se la protesi correttamente posizionata la parte patologica dellaorta esclusa dal circolo sistemico ; alla tc di follow - up lendoprotesi non varier di posizione rispetto al controllo post - operatorio e dovrebbe escludere lintera aorta patologica . 
il lume protesico deve essere pervio e senza brusche angolazioni , con stent ben aderente alla parete senza spazio apprezzabile tra esso e lintima vasale per tutto il decorso protesico , particolarmente agli estremi prossimale e distale . 
le zone di ancoraggio dello stent - graft ( landing zones ) , piatte , diritte , lunghe e cilindriche , sono critiche per uno stabile posizionamento protesico [ 36 ]  . 
 landing zones vicine o prossimali allorigine dellarteria succlavia sinistra sono associate ad alto rischio di formazione dellendoleak e la difficolt ad ottenere una buona tenuta radiol med ( 2012 ) 117 : 831854 disease . 
landing zones located near or proximal to the origin of the left subclavian artery are associated with a high risk of endoleak formation , and failure to achieve a proximal seal in the aortic arch resulting in a proximal type i endoleak remains an achilles heel of the tevar procedure [ 5053 ]  . 
 to treat aortic dissection , it is essential to cover the entry tear ( proximal split in the intimal flap ) , which not only will provide protection from aortic rupture and promote thrombosis of the false lumen but will also reduce the risk of dynamic true lumen collapse and the resulting malperfusion to distal branch vessels . 
in these patients , there should be no flow into the false lumen ; with time , this lumen may become imperceptible in cases of acute dissection [ 54 ]  . 
 immediately after tevar , mdct may show aortic wall thickening , low - density periaortic fluid , and / or pleural effusions , which are more common on the left , as well as lowerlobe atelectasis . 
these findings commonly resolve within 8 weeks , and periaortic fluid and aortic - wall thickening should not be mistaken for intramural haematoma or aortic rupture , which are of higher attenuation ( > 40 hu ) [ 38 ] .the overall size of the aorta after stent graft should be similar to or smaller than the original diseased aorta [ 14 ]  . 
perceived aortic enlargement on axial images compared with preoperative mdct images may occur because of stent rigidity , stent altering the position and angulation of the aorta [ 37 , 38 ]  . 
 per il trattamento della dissezione essenziale coprire la breccia di ingresso tra i lumi , il che non protegger solo dalla rottura aortica promuovendo la trombosi del falso lume , ma ridurr anche il rischio del collasso dinamico del vero lume e le conseguenti sindromi da malperfusione . 
in questi pazienti non dovr essere apprezzabile flusso nel falso lume ; nel caso di dissezione acuta questo lume , con il tempo , pu diventare impercettibile [ 54 ]  . 
 immediatamente dopo tevar , la tcmd pu mostrare lispessimento della parete vasale , il fluido periaortico a bassa densit e / o il versamento pleurico , in genere pi comune a sinistra ed associato a parziale atelettasia del lobo inferiore . 
 questi segni generalmente scompaiono entro 8 settimane ; lispessimento di parete ed il fluido periaortico non devono essere confusi con lematoma intramurale o la rottura aortica , che presentano maggiore densit ( > 40 uh ) [ 38 ]  . 
nelle immagini assiali dopo procedura si pu avere la percezione di un incremento dei diametri del vaso rispetto allesame pre - impianto , perch la rigidit dello stent pu alterare la posizione e langolazione dellaorta [ 37 , 38 ]  . 
1a - c volume - rendering sagittal reconstruction ( a ) shows normal appearance of the endograft ( talent endovascular stent graft ; medtronic vascular , santa rosa , ca , usa ) , which is tightly apposed to the aorta ; axial ( b ) and coronal ( c ) maximum intensity projection ( mip ) reconstructions show perfusion of the aneurysmal sac caused by poor apposition of the distal landing zone with the aortic wall , consistent with type 1b endoleak ( arrows )  . 
1a - c la ricostruzione sagittale in volume rendering ( a ) mostra la normale morfologia dellendoprotesi ( talent endovascular stent graft ; medtronic vascular , santa rosa , ca ) , che strettamente aderente alla parete aortica ; le ricostruzioni mip assiale ( b ) e coronale ( c ) mostrano la perfusione del sacco aneurismatico causata da incompleta apposizione della zona di attacco distale dellendoprotesi alla parete aortica , da endoleak di tipo ib ( frecce )  . extravascular structures of the thorax should be routinely assessed to look for possible postprocedural complications , including pneumonia and pulmonary embolus . 
esso sarebbe attribuibile a cause miste , tra cui la fragilit della parete aortica e la progressione naturale della malattia , anche se il background anatomo - patologico ed elementi correlati allendoprotesi , come il ripiegamento o il collasso protesico , possono essere un aspetto causale importante . 
fattori di rischio per linfolding o il collasso dello stent sono un lume aortico ridotto , un piccolo raggio di curvatura dellarco aortico ( pazienti giovani ) , cos come leccessivo sovradimensionamento ( oversizing ) protesico , che un importante fattore di rischio ed descritto per differenti tipi di endoprotesi ( gore tag e cook zenith ) [ 38 ]  . 
la gran parte dei pazienti con collasso protesico non ha sintomi legati ad insuccesso della terapia ; in radiol med ( 2012 ) 117 : 831854 risk factors for stent - graft infolding or collapse are a small aortic lumen and a small radius of the aortic arch curvature ( young patients ) , as well as oversizing , which is an important risk factor and is described for different types of endografts and prostheses ( gore tag and cook zenith ) [ 38 ]  . 
most patients with endograft collapse do not have symptoms related to the endograft failure ; in these patients , abnormality is detected during standard follow - up imaging , supporting the importance of continued surveillance after tevar . 
endovascular stent collapse management is dictated by the extent and location of the collapse ; if it involves only the proximal segment , it may be possible to insert another endograft to stabilize the proximal portion of the collapsed endoprosthesis [ 59 ]  . 
if there is only a focal area of collapse , it may be possible to balloon the endograft and maintain patency by inserting a palmaz stent ( johnson & johnson , cordis , miami lakes , fl , usa ) [ 59 ]  . 
distal endograft collapse can possibly be treated conservatively under close follow - up [ 60 ]  . fracture of the connecting bar of a stent graft ( after tevar for chronic posttraumatic pseudoaneurysm ) stent - graft rupture has been described as a possible cause of graft fatigue . 
to better understand the underlying mechanisms of a graft rupture , an analysis on explanted stent fragments was conducted by scanning electron microscopy ( sem ) and energy dispersive radiograph ( edx )  . 
the analysis revealed surface abnormalities in most grafts as a result of , presumably , a cell - mediated corrosive process of the nitinol wire that , in conjunction with circulatory stress , may lead to stent cracks and eventually fractures [ 61 , 62 ]  . questi pazienti lanomalia viene rilevata durante il normale imaging di follow - up , sottolineando limportanza dello stretto monitoraggio dopo tevar . 
la sua gestione dettata dal grado e dalla sede del collasso ; se coinvolto il solo segmento prossimale , pu essere possibile impiantare unaltra endoprotesi per stabilizzare la porzione prossimale dello stent [ 59 ]  . 
se c solo unarea focale di collasso , pu essere possibile balloonare lendoprotesi e mantenerne la perviet inserendo un catetere di palmaz ( johnson&johnson , cordis , miami lakes , fl , usa ) [ 59 ]  . 
la dilatazione della porzione collassata spesso non sufficiente ; in tali casi , nei pazienti con un collasso protesico prossimale , necessario limpianto di una seconda protesi o lintervento chirurgico . 
il collasso del segmento protesico distale pu essere eventualmente trattato in modo conservativo sotto stretto follow - up [ 60 ]  . frattura della barra di connessione di unendoprotesi ( dopo tevar per pseudoaneurisma post - traumatico cronico ) la rottura della protesi gi stata descritta come una possibile causa di fallimento del trattamento ; per capirne meglio i meccanismi sono state effettuate analisi di microscopia elettronica a scansione e tecniche radiografiche a dispersione di energia su frammenti di stent espiantati . 
i dati presenti in letteratura aggiungono la tevar alla lista delle procedure che possono dar luogo alla dissezione iatrogena [ 14 , 15 , 27 , 29 , 31 , 34 , 6365 , 68 , 69 ]  . 
la dissezione iatrogena pu inoltre derivare da un aggressivo oversizing , da fissazione della protesi ad una parete aortica patologica , da unipertensione scarsamente controllata o da sfavorevoli condizioni anatomo - patologiche , quali leccessiva angolazione del colletto o la presenza di ematoma intramurale nelle zone di fissazione [ 64 ]  . 
axial oblique craniocaudal mip reconstruction ( a ) and oblique coronal three - dimensional volume - rendered image ( b ) show descending aorta stent graft with the infolding of two proximal rings ( arrow ) ; note the flap extended to common iliac arteries . 
la ricostruzione mip assiale obliqua cranio - caudale ( a ) , il volume rendering in coronale obliqua ( b ) ed il dettaglio in volume rendering ( c ) mostrano lendoprotesi in aorta discendente con linfolding di due anelli prossimali ( freccia ) ; si noti il lembo di dissezione esteso alle iliache comuni . 
le scansioni tcmd in fase pre - contrastografica ( c , e ) mostrano lematoma intramurale dellarco e dellaorta ascendente ( freccia ) ; le scansioni mdtc in fase contrastografica ( d , f ) confermano la presenza dellimh retrogrado di tipo a associato a versamento pleurico bilaterale . radiol med ( 2012 ) 117 : 831854 fig . 
images obtained in a 66 - year - old man before , at discharge and at routine follow - up 3 months after tevar for distal - arch - pau associated with imh . 
mdct scan before tevar in axial mip reconstruction ( a ) shows a pau as a focal contrastmaterial - filled pouch ( arrow ) associated with imh ( star )  . 
at discharge mdct , axial mip reconstruction ( b ) shows the stent apposed to the aortic wall , with no appreciable space between it and the aortic intima along its entire circumference . 
la tcmd contrastografica precedente alla tevar con ricostruzione mip assiale ( a ) mostra unestroflessione focale di mezzo di contrasto , simil - ulcerosa , da pau ( freccia ) con ematoma intramurale associato ( stella )  . 
la mdtc di follow - up a 3 mesi con ricostruzioni mip coronale ( c ) e sagittale ( d ) mostra il lembo di dissezione immediatamente distale alla protesi ( freccia )  . 
literature data add tevar to the list of the procedures resulting in iatrogenic dissection [ 14 , 15 , 27 , 29 , 31 , 34 , 6365 , 68 , 69 ]  . 
iatrogenic dissection may further result from aggressive oversizing , fixation in the diseased portion of the aorta , poorly controlled hypertension or definite anatomical / pathological conditions such as excessive neck angulation or intramural haematoma in the landing areas [ 64 ]  . avoiding aortic - arch stent grafting in patients with marfan syndrome , preferably selecting the endograft without the bare spring for patients with a kinked aortic arch or with marfan syndrome ( if endografting is used ) , improving device design and standardising endovascular manipulation might lessen the occurrence of retrograde or anterograde dissection [ 7173 ]  . 
 simultaneous thoracoabdominal retrograde dissection and stent - graft thrombosis / occlusion ( after evar for abdominal aortic aneurysm ) acute retrograde dissection , extending to the thoracic aorta , is surely the result of abnormal manoeuvres during evar [ 74 ]  . 
we performed an emergency mdct scan on the first day after placement of an anaconda stent graft for unstable abdominal aortic aneurysm in a 72 - year - old man with recurrent renal cancer and ubiquitous metastases . 
the unstable infrarenal abdominal aneurysm for which the stent was implanted became a dissecting aneurysm , with deviation of much aortic flow in the intra - aneurysmal false lumen due to endoleak type iii ( from inadequate sealing at the junction of the stent grafts main body and left limb )  . 
stenosis of the iliac graft limb is reported in a series of bifurcated grafts not fully supported by stents [ 82 ] , but graft occlusion is a relatively rare event after stent - graft implantation [ 83 , 84 ]  . 
percutaneous local thrombolysis or open surgical conversion depends on the severity of the vascular occlusion . dissezione retrograde toraco - addominale simultanea e trombosi / occlusione protesica ( dopo evar per aneurisma dellaorta addominale ) la dissezione acuta retrograda , estesa allaorta toracica , sicuramente il risultato di manovre anomale effettuate durante evar [ 74 ]  . 
laneurisma aterosclerotico sottorenale instabile per il quale venne impiantata lendoprotesi si trasform , dopo limpianto , in un aneurisma dissecante , con deviazione di gran parte del flusso aortico nel falso lume intra - aneurismatico a causa di un endoleak di tipo iii ( da difetto di coesione alla giunzione tra il corpo ed il gambo iliaco di sinistra della protesi ) ; dopo pochi giorni si svilupp una trombosi completa della protesi , con paraparesi di grado avanzato . 
la stenosi della branca iliaca della protesi segnalata in una casistica comprendente protesi biforcate non completamente supportate da stent [ 82 ] , ma locclusione protesica un evento relativamente raro dopo limpianto di endoprotesi [ 83 , 84 ]  . 
la trombolisi locale percutanea o la conversione chirurgica dipendono dal grado dellocclusione vasale . fistola aortobronchiale in due tempi ( dopo tevar per aneurisma dellaorta discendente ) le fistole aortobronchiali ( fab ) , rare e fatali se non trattate , rappresentano una connessione anatomica patologica tra laorta ed il bronco . 
la loro eziopatogenesi comprende la tubercolosi polmonare , la polmonite da stafilococco , il carcinoma broncogeno , laortite , la dissezione , gli aneurismi aortici e le protesi vascolari dopo chirurgia dellaorta toracica [ 85 ] ; gli aneurismi ne costituiscono leziologia pi comune , responsabili di almeno il 50%60% delle fab riportate in letteratura [ 8688 ]  . 
nel caso sia presente un aneurisma od uno pseudoaneurisma aortico , dovrebbero essere considerate : la possibilit dellerosione da parte della pressione radiol med ( 2012 ) 117 : 831854 fig . 
images obtained in a 72 - year - old man with recurrent renal cancer and ubiquitous metastases who underwent evar for unstable atherosclerotic abdominal aortic aneurysoblique coronal mip reconstruction ( a ) shows postsurgical mdct control of anacondatm stent grathe proximal part of the main body consists of two nitinol rings at a variable distance from each other according to the vascular diameter ; the distal one is unsupported by other stents or longitudinal bars and is largely radiolucent ( arrow )  . 
emergency mdct scans in the first day post - evar in oblique coronal mip reconstruction ( b ) shows retrograde thoracoabdominal iatrogenic dissection , with entry tear located at the proximal part of the stent grafts main body ( arrow )  . 
in axial mip reconstruction ( c ) , a lumbar artery that feeds a hypervascular metastasis to the left psoas muscle simulates a type ii endoleak ( arrow ) ; indeed , its density is lower than that of the false lumen . 
mdct scans ( axial and coronal mip reconstructions ) show complete thrombosis of the prosthesis due to poor outflow , appreciated either at aortic component ( d ) or at iliac limbs ( e )  . 
la porzione prossimale del corpo della protesi comprende due anelli di nitinolo a distanza variabile sulla base del diametro vasale , mentre quella distale non supportata da altri stent o barre longitudinali di fissazione e risulta in gran parte radiotrasparente ( freccia )  . 
la tcmd in prima giornata dalla procedura in ricostruzione mip coronale obliqua ( b ) mostra una dissezione retrograda toraco - addominale iatrogena con breccia di ingresso localizzata allestremo prossimale della protesi ( freccia )  . 
in ricostruzione mip assiale ( c ) unarteria lombare diretta ad una metastasi localizzata al muscolo psoas sinistro simula un endoleak di tipo ii ( freccia ) , ma la sua densit inferiore rispetto a quella del falso lume . 
 842 radiol med ( 2012 ) 117 : 831854 two - stage aortobronchopulmonary fistula ( after tevar for descending thoracic aorta aneurysm ) aortobronchial fistulae ( abfs ) are an anatomical connection between aorta and bronchus , which are rare , and fatal if untreated . 
the left lung is much more involved than the right one , which may be explained by the short distance from the left bronchus to the descending thoracic aorta ( dta ) [ 92 ]  . 
dyspnoea and cough , chest or back pain , pulmonary rales , hypoxaemia , dysphonia , hoarseness , tachypnoea , fever , sepsis or respiratory alkalosis have been reported [ 86 ]  . 
standard chest x - rays may be completely normal , may show infiltrates in the adjacent lung parenchyma or a new enlarging mass , or may suggest an enlarged dta [ 93 ]  . 
occasionally , intragraft or perigraft air surrounding the aneurysm and stent graft is the presenting feature of an abf , whereas a fistula between bronchus and graft almost never can be seen [ 9396 ]  . 
as in our case , shrinkage of the aneurysmal sac ( first stage ) in a very tortuous aorta may expose the nitinol mesh to a more direct contact and finally to direct erosion ( second stage ) into the airways . 
la fistola solitamente di piccole dimensioni ed facilmente chiusa dai coaguli ; pu restare chiusa per settimane o mesi , ma per linstabilit dei coaguli , la comunicazione potrebbe riaprirsi con una conseguente nuova emorragia [ 86 , 91 , 92 ]  . 
il polmone sinistro pi spesso interessato del destro , il che spiegabile per la minore distanza tra il bronco principale sinistro e laorta discendente ( atd ) [ 92 ]  . 
sono stati segnalati : dispnea e tosse , dolore toracico o al dorso , rantoli , ipossiemia , disfonia , raucedine , tachipnea , febbre , sepsi o alcalosi respiratoria [ 86 ]  . 
la radiografia standard del torace pu essere completamente normale , pu mostrare addensamenti nel parenchima polmonare adiacente allaorta , evidenziare una massa di nuova comparsa ed in progressione in controlli successivi od unaorta discendente ingrandita [ 93 ]  . 
raramente pu essere apprezzato lo stravaso arterioso attivo di mdc dallaorta nel parenchima polmonare o nelle vie aeree ; di rado le bollicine gassose intrao periprotesiche o perianeurismatiche sono il segno tc di presentazione di una fab , mentre la fistola tra il bronco e la protesi non quasi mai visibile [ 9396 ]  . 
nel nostro caso , la riduzione volumetrica del sacco aneurismatico ( primo tempo ) , un evento auspicabile dopo tevar , in unaorta notevolmente tortuosa , pu esporre le maglie di nitinolo ad un pi diretto contatto con le vie aeree ed infine allerosione franca ( secondo tempo ) nelle stesse . 
nonostante sia il trattamento chirurgico che quello endoprotesico delle fab sia associato ad unelevata mortalit , la terapia conservativa non sembra essere unopzione valida [ 90 ]  . fistola aorto - esofagea associata a tevar ( per aneurisma dellaorta discendente ) la fistola aorto - esofagea ( fae ) una rara causa di sanguiradiol med ( 2012 ) 117 : 831854 fig . 
images obtained in a 76 - year - old man with a medical history of hypertension , noninsulin - dependent diabetes mellitus , peripheral vascular disease and biliary neoplasm who underwent tevar for descending thoracic aorta inflammatory aneurysmdct before discharge : mip axial ( a ) and coronal ( b ) reconstructions show two endovascular stent grafts obliterate the large , thick - walled aneurysm in the severely tortuos descending thoracic aorta , which is elongated , kinked and angulated in the right vertebral direction in the mediodistal tract . 
the 6 - month follow - up mdct coronal volume - rendered image ( c ) shows shrinkage of the aneurysmal sac but also marked increase in right - angle convexity of the stent graft , with its severe oblique positioning and constriction in the longitudinal axis . 
mip axial ( d ) and coronal ( e ) reconstruction ( parenchymal lung window ) images disclose the proximal end of the stent graft in close proximity to the right lowerlobe bronchus and a large amount of air surrounding the aneurysm and stent graft ; neither endoleak nor extravasation of contrast medium into the perigraft space is noted . 
maschio di 76 anni con storia di ipertensione , diabete mellito non insulino - dipendente , malattia vascolare periferica e neoplasia biliare venne trattato con tevar per aneurisma infiammatorio dellaorta discendente . 
tcmd prima della dimissione : la ricostruzione mip sul piano assiale ( a ) e coronale ( b ) mostra due stent posizionati per un grossolano aneurisma a pareti spesse dellaorta discendente che si presenta notevolmente tortuosa , allungata e con modesta angolazione paravertebrale destra nel tratto medio - distale . 
la tcmd di follow - up al sesto mese in volume rendering ( c ) mostra una significativa riduzione delle dimensioni dellaneurisma ma anche un marcato incremento dellangolazione destro - convessa e dellobliquit dellendoprotesi . 
la ricostruzione mip assiale ( d ) e coronale ( e ) ( finestra parenchimale ) mostra lestremo prossimale dellendoprotesi a stretto contatto del bronco del lobo inferiore destro , circondata da una grande quantit di aria ; non c spandimento di mdc nello spazio periprotesico n endoleak . 
la ricostruzione in proiezione di minima intensit ( minip ) coronale obliqua ( f ) dimostra multiple ampie comunicazioni tra i rami della piramide basale ed il trombo periprotesico . 844 radiol med ( 2012 ) 117 : 831854 ity in 100% of patients , but even successful surgery for abf carries considerable mortality and morbidity risks . 
 tevar - associated aortooesophageal fistula ( for dta aneurysm ) aortooesophageal fistula ( aof ) is a rare cause of upper gastrointestinal bleeding , with aetiologies including foreignbody ingestion , malignancy and postoperative trauma , but it is often described in the cardiovascular literature as being associated with penetrating or ruptured taas [ 101 ]  . 
secondary aof is well recognised as a complication of thoracic aortic surgery and has catastrophic consequences without treatment [ 102 ]  . aof as an unusual , life - threatening complication of lessinvasive tevar occurs in less than 1% of endovascular repair procedures and is thus probably not widely known within the medical community . 
it is often an early to midterm complication , encountered within 116 months after tevar , presenting either as haematemesis or new - onset fever accompanied by elevated inflammation markers , and may herald the onset of imminent rupture of the aorta into the oesophagus , followed by sepsis . 
thus , not only haematemesis but new - onset fever in patients with prior tevar should alert the physician to this potentially life - threatening complication [ 106 , 108 , 109 ]  . 
ct is particularly helpful as an initial imaging modality because evidence of a relatively characteristic new heterogeneous mass between the descending thoracic aorta and oesophagus with or without air entrapment in the arterial wall give an early clue to the diagnosis . 
early evidence of new - onset fever after tevar and ct finding of a new mass between the aorta and oesophagus provides an early clue that could then further be confirmed by prompt oesophagogastroduodenoscopy ( ogd )  . 
aof may be directly visualised by ogd as a large oesophageal defect with a clear view onto the stent graft or as only a mild erosive lesion [ 111 ]  . 
early diagnosis is probably life saving namento a partenza dal tratto gastroenterico superiore , con eziologie che comprendono lingestione di corpi estranei , le neoplasie , i traumi post - operatori , ma spesso descritta nella letteratura cardiovascolare poich associata ad aneurismi dellaorta toracica in rottura contenuta o franca [ 101 ]  . 
 la fae secondaria una complicanza nota della chirurgia dellaorta toracica ed ha conseguenze catastrofiche se non trattata [ 102 ]  . essa inoltre una complicanza inusuale , ma potenzialmente letale della tevar , avviene in meno dell1% delle procedure di impianto endoprotesico ed unevenienza probabilmente poco conosciuta nella comunit medica . 
spesso una complicanza precoce o a medio termine , riscontrata tra 1 e 16 mesi dalla procedura , pu esordire con ematemesi o febbre di nuova comparsa accompagnata ad incremento dei markers dellinfiammazione , potendo tali sintomi essere i prodromi della rottura imminente dellaorta in esofago e della sepsi generalizzata . 
cos , non solo lematemesi , ma anche la febbre di nuova insorgenza in pazienti sottoposti a tevar deve allertare il clinico nei confronti di questa complicanza potenzialmente pericolosa per la vita [ 106 , 108 , 109 ]  . 
la tc particolarmente utile come modalit diagnostica iniziale , perch la comparsa di una massa a densit disomogenea in una sede relativamente caratteristica tra laorta discendente e lesofago , con o senza intrappolamento di bollicine gassose nella parete vasale , fornisce un elemento prezioso per la diagnosi precoce . 
lassociazione precoce tra la febbre di nuova insorgenza ( dopo tevar ) ed il segno tc di una massa tra laorta e lesofago fornisce un primo indizio che poi pu essere ulteriormente confermato da una esofagogastroduodenoscopia ( egd ) urgente . 
 allegd la fae pu essere visualizzata direttamente come un ampio difetto esofageo che permette di avere una chiara visione dellendoprotesi attraverso lottica o solo come una piccola lesione erosiva [ 111 ]  . 
i lavori pubblicati hanno confermato che un management di tipo conservativo per controllare il risanguinamento e prevenire la mediastinite ha quasi invariabilmente una prognosi fatale , giustificando potenzialmente la pi aggressiva strategia chirurgica che implica la resezione esofagea , una revisione ed efficace toilette del mediastino e linterposizione di una ( omo ) protesi [ 114 ]  . 
unenhanced ( a ) and enhanced axial ( b ) and sagittal ( c ) mip reconstructions show new nonhomogenous mass ( star ) between the aorta and oesophagus , with entrapment of small air bubbles in the aortic wall ( arrow ) within the thrombosed aneurysmal sac and a tubular contrast - medium extravasation due to type iii endoleak ( white triangle )  . 
unenhanced axial , sagittal and coronal mpr after ingestion of contrast medium ( d ) shows a partially calcified pseudoaneurysm wall ( arrow ) with thrombus extensively communicating with the oesophageal lumen through a solution of continuity of subcarinal oesophagus . 
le ricostruzioni mip assiali in fase pre - contrastografica ( a ) e post - contrastografica assiale ( b ) e sagittale ( c ) mostrano una nuova massa non omogenea ( stella ) tra laorta e lesofago con intrappolamento di piccole bolle gassose ( freccia ) nellaneurisma trombosato ed uno stravaso di mdc da endoleak di tipo iii ( triangolo bianco )  . 
le ricostruzioni pre - contrastografiche mpr assiale , sagittale e coronale dopo ingestione di mezzo di contrasto per os ( d ) mostrano uno pseudoaneurisma a pareti in parte calcifiche ( freccia ) con trombo ampiamente comunicante con il lume esofageo attraverso una soluzione di continuo dellesofago sottocarenale . 
published reports have confirmed that conservative management to control rebleeding and prevent mediastinitis has almost invariably a fatal outcome , potentially justifying a more aggressive surgical il posizionamento di unendoprotesi per curare la fae secondaria a chirurgia open [ 114 , 115 ]  . una seconda tevar ( re - tevar ) in un ambiente potenzialmente contaminato o infetto rimane del tutto discutibile . 
most strategies remain far from optimal for managing this condition , emphasising the need for further research in this area , not only for identifying patients at risk but for evaluating strategies for better management . 
 thoracic endograft infection and mediastinitis ( after tevar for pseudoaneurysm ) thoracic endograft infections ( teis ) are rare but are associated with significant morbidity and mortality [ 117119 ]  . 
ct findings suggestive of teis after tevar are expected to be similar to those after placement of abdominal prosthetic grafts and include aortic - wall thickening , perigraft soft tissue or fluid collection , pseudoaneurysm , perigraft air or an increasing amount of air on serial imaging studies , adjacent soft - tissue stranding or abscess formation and graft thrombosis or expansion [ 120 , 121 ]  . 
 in the thoracic aorta , > 5 mm of perigraft soft tissue between an adjacent organ or vessel and the graft is abnormal and may suggest infection . endograft infection can be difficult to diagnose , especially early after treatment owing to after tevar periaortic changes . 
when a tei is established , treatment is demanding and includes several medical therapies associated with protesi intatta , rendendo alquanto improbabile il sanguinamento diretto dallaorta [ 103107 , 116 ]  . 
la maggior parte delle strategie rimangono tuttaltro che ottimali per la gestione di questa complicanza , evidenziando la necessit di ulteriori ricerche in questo settore , non solo per identificare i pazienti a rischio , ma anche per lo studio di migliori modalit di gestione di questa patologia . infezione dellendoprotesi toracica ( iet ) e mediastinite ( dopo tevar per pseudoaneurisma ) linfezione dellendoprotesi toracica ( iet ) rara , ma associata a morbilit e mortalit significative [ 117119 ]  . 
i segni tc suggestivi di iet dopo tevar sono simili a quelli attesi dopo posizionamento di endoprotesi addominale e rappresentati da ispessimento di parete aortica , raccolte periprotesiche a densit fluida o delle parti molli , pseudoaneurismi , aria periprotesica o quota gassosa in incremento nei controlli seriati , da stranding delle parti molli adiacenti o formazione di un ascesso , trombosi protesica o espansione dellaneurisma [ 120 , 121 ]  . 
nellaorta toracica uno spessore di tessuto della densit delle parti molli maggiore di 5 mm , tra un organo adiacente o il vaso e la protesi , patologico e deve suggerire uninfezione . 
i pazienti di solito sono gravemente compromessi dalla sepsi e nella maggior parte dei casi non sono considerati candidati allintervento chirurgico per le condizioni cliniche generali o per cause locali [ 117122 ]  . 
mdct obtained before tevar at discharge and 3 - month follow - up for isthmic pseudoaneurysm in a 67 - year - old cirrhotic woman with persistent fever of unknown origin and left hemithorax paaxial ( a ) mip reconstruction and volume - rendered ( b ) image before tevar show an aortic isthmus pseudoaneurysm ( arrow )  . 
tcmd effettuate prima della tevar , alla dimissione ed al follow - up a 3 mesi per pseudoaneurisma istmico in una donna di 67 anni con cirrosi epatica , febbre persistente di origine sconosciuta e dolore allemitorace sinistro . 
la 18f - fdg - pet ( f ) ( da sinistra a destra : scansioni assiali , sagittali e coronali ) mostra elevata attivit metabolica a livello della protesi e del tessuto periprotesico . 848 radiol med ( 2012 ) 117 : 831854 various surgical options . 
patients are usually severely compromised by sepsis , and in most cases , they are considered unfit for surgery due to general clinical conditions or local concerns [ 117 , 122 ]  . 
the effect of prophylactic antibiotic use during subsequent invasive procedures must be solidified . arch aneurysm ( after tevar for type b dissection ) stent - graft designs are relatively stiff , with long segments , and they are unable to conform to highly angulated or curved arches ; however , future devices in development address this issue by using more conformable and flexible designs [ 123 , 124 ]  . 
due to asymmetric pressure of the stent graft on the aortic wall , in the case of a straight stent graft placed in the aortic arch or due to stent - graft oversizing , stress on the vessel wall becomes high and consequently remodelling of the aortic wall will take place . 
this nonmatching geometry may give rise to high ( peak ) stress levels in the arterial wall in the ascending and descending part of the aortic arch , leading , as in our case , to aneurysm formation proximal to the prosthesis . 
similar to a type i endoleak is bird - beaking of the proximal stent , defined as the lack of apposition of the proximal stent graft to the aortic wall , with a wedge - shaped gap between the undersurface of the stent graft and the aortic wall along the lesser curvature of the aortic arch [ 126 ]  . 
bird - beak length refers to the longitudinal segment of the unapposed stent graft ; it is shortest in patients who do not develop endoleaks ( 6.78.8 mm ) and longest in patients who formed complex endoleaks ( 22.65.1 mm ) [ 126 , 127 ]  . 
therefore , patients with bird - beak configuration need to undergo follow - up at closer intervals than prescribed by the routine postprocedural protocol to assess progression to a true type i endoleak , stent - graft collapse or aneurysm formation . 
 aneurisma dellarco aortico ( dopo tevar per dissezione di tipo b ) la struttura delle endoprotesi attualmente disponibili relativamente rigida con segmenti protesici lunghi , scarsamente capaci di adattarsi ad archi aortici fortemente angolati o ricurvi , ma i dispositivi protesici in sviluppo mirano alla risoluzione di questo problema attraverso una geometria pi adeguata ed una configurazione maggiormente flessibile [ 123 , 124 ]  . 
a causa dellasimmetrica pressione della protesi sulla parete aortica , sia nel caso di uno stent rettilineo inserito nellarco , sia per eccessivo oversizing , lo stress sulle pareti vasali diverr elevato ed avr luogo un conseguente rimodellamento di parete . 
tale disaccoppiamento geometrico pu dar luogo ad elevati livelli di stress parietale sulle porzioni ascendente e discendente dellarco , portando , come nel nostro caso , alla formazione di un aneurisma prossimale alla protesi . 
simile ad un endoleak di tipo i la configurazione a becco duccello ( bird - beak ) dellestremo prossimale protesico , definita come la mancata apposizione della porzione prossimale dellendoprotesi alla parete aortica , con un divario cuneiforme tra la superficie inferiore della protesi e la parete aortica lungo la piccola curvatura dellarco [ 126 ]  . 
la lunghezza del bird - beak la lunghezza del segmento protesico non aderente alla parete ed minore nei pazienti che non sviluppano endoleaks ( 22 , 65 , 1 mm ) [ 126 , 127 ]  . 
 pertanto , i pazienti con endoprotesi con configurazione a becco duccello necessitano di follow - up ad intervalli pi ravvicinati di quanto prescritto dal protocollo di routine post tevar , per valutare la presenza o la progressione di un endoleak di tipo i , di un collasso protesico o la formazione di un aneurisma . dissezione endoprotesica ( dopo tevar per lesione aortica traumatica ) in - stent - graft dissection ( after tevar for aortic blunt trauma ) monitoring neointima formation within the stent graft incorporated onto the aortic wall is not yet available by ct / mr imaging . 
it is possible that following blunt trauma in a young patient already subject to tevar , in - stent - graft dissection il monitoraggio della formazione della neointima sul profilo interno dellendoprotesi impiantata non attualmente possibile con tc / risonanza magnetica ( rm )  . 
invece probabile che in seguito ad un trauma chiuso in un paziente giovane gi sottoposto a tevar , si possa avere una dissezione endoprotesica , con riduzione conseguente del flusso ematico a valle [ 128 ]  . 
mdct images obtained in 67 - year - old man before tevar ( a ) and at 6 - month follow - up after tevar ( b , c ) for type b aortic dissection complicated by distal arch imh and worsening hypertension . 
mip sagittal reconstruction ( b ) 6 months after tevar shows new appearance of an arch aneurysm upstream of the stent graft and a bird - beak configuration ; bird - beak angle ( between arrows )  . 
tcmd in un maschio di 67 anni prima della tevar ( a ) ed al follow - up a 6 mesi dopo tevar ( b , c ) per una dissezione aortica di tipo b complicata da imh dellarco ed ipertensione farmaco - resistente . 
 la ricostruzione mip sagittale ( b ) nella tc di follow - up a 6 mesi dopo tevar mostra la nuova comparsa di un aneurisma dellarco a monte dellendoprotesi ed una configurazione bird - beak della stessa ; angolo del bird - beak ( tra le frecce )  . 
la ricostruzione sagittale in volume rendering ( c ) mostra chiaramente laneurisma dellarco a monte dellendoprotesi . may occur , resulting in a reduction in flow downstream [ 128 ]  . 
the patient may successfully be treated with further stent - graft implantation by the percutaneous approach . conclusions as tevar use grows , physicians and general radiologists should be aware of usual and uncommon potential adverse events or complications as one of the differential diagnoses in tevar patients . 
specific for the trauma population , a variety of grafts that are shorter , precurved and smaller are vrebbe essere tenuto presente nel follow - up , specialmente in soggetti giovani , dediti ad attivit fisica , che possono essere trattati con successo grazie allimpianto di una seconda endoprotesi per via percutanea . conclusioni con laumentata diffusione della tevar , sia i clinici che i radiologi generali devono essere consci delle potenziali complicanze della procedura : di quelle pi frequenti , di quelle insolite , cos come delle possibilit diagnostico differenziali . 
sono in fase di sviluppo stent specifici per i traumatizzati , pi brevi , pre - curvati e di piccole dimensioni che permetteranno un rilascio protesico pi preciso e ridur850 radiol med ( 2012 ) 117 : 831854 being developed , which will allow more precise deployment and potentially reduce complication rates . 
gli interventisti devono avere almeno due piani di riserva tra cui la conversione in chirurgia open con bypass atrio - femorale con o senza arresto circolatorio ipotermico ; infine , i pazienti devono essere strettamente monitorizzati nel postoperatorio . 
axial pulsatility measurements were taken at three levels : 2 cm above the highest renal artery ; immediately below the lowest renal artery ; 1 cm below the lowest renal artery . 
le misurazioni della pulsatilit aortica sono state effettuate da tre lettori indipendenti : 2 cm sopra larteria renale pi craniale ; immediatamente al di sotto dellarteria renale pi caudale ; 1 cm al di sotto dellarteria renale pi caudale . 
sono state misurate le pressioni arteriose brachiali sistolica e diastolica al fine di valutare il grado di distensibilit della parete aortica , espresso come modulo pressorio di deformazione elastica ( ep )  . 
 lidentificazione di pazienti con maggior distensibilit dellaorta sottorenale potrebbe modificare la scelta del calibro dellendoprotesi . radiol med ( 2012 ) 117 : 804814 keywords ct angiography evar dynamic imaging abdominal aorta endovascular treatment parole chiave angio - tc stent - graft imaging dinamico aorta addominale trattamento endovascolare introduction introduzione stent - graft migration is a late complication of endovascular abdominal aortic aneurysm ( aaa ) repair ( evar ) and is characterised by downward slippage of the endograft , leading to a type i endoleak with enlargement of the aneurysmal sac diameter and consequently increased risk of aneurysm rupture [ 14 ]  . 
multiple factors have been postulated to predict endovascular - graft migration ; however , migration aetiology seems to be principally inherent to problems with endograft fixation , although aortic - neck dilation may also play a critical role in that it seems to be a marker of , and possibly a risk factor for , migration . 
in detail , late aneurysmal neck dilation was associated with graft migration in up to 35.3% of patients in one series and was identified as an independent predictor of type i endoleaks and need for secondary intervention [ 5 , 6 ]  . based on a recent report , a possible contributor to aortic - neck dilation ( and ) after evar is the radial force of endograft oversizing , which might induce or accelerate aortic - wall degeneration and dilation [ 2 ]  . 
it has been hypothesised that compliance , which relates directly to aortic - wall behaviour and composition and is strictly related to pulsatility , might provide such information [ 7 ]  . 
 dynamic computed tomography angiography ( cta ) , in which acquisition is synchronised to the patients ecg , provides information on aortic pulsatility and changes in aortic conformation that occur during the cardiac cycle [ 812 ]  . 
the purpose of our study was to evaluate whether dynamic ct imaging can provide functional vessel information to predict the likely outcomes of the aortic neck in patients undergoing evar . materials and methods study design a prospective , single - centre study was carried out on 40 patients > 75 years in order to reduce potential consequences una delle complicanze a lungo termine pi frequenti del trattamento endovascolare ( evar ) degli aneurismi dellaorta addominale ( aaa ) rappresentata dalla migrazione dellendoprotesi , responsabile di endoleak di tipo i con conseguente aumento del diametro e del rischio di rottura della sacca aneurismatica [ 14 ]  . 
sono state analizzate differenti teorie per predire la migrazione dello stent graft ; leziologia della migrazione sembra essere correlata principalmente a problemi di ancoraggio del gra tuttavia anche la dilatazione del colletto prossimale sembra svolgere un ruolo cruciale , rappresentando un marker ed un possibile fattore di rischio per la migrazione . 
in particolare , la dilatazione tardiva del colletto aneurismatico si associa alla migrazione dello stent graft nel 35 , 3% circa dei pazienti ed stato identificato come fattore predittivo indipendente degli endoleak di tipo i che necessita di un re - intervento [ 5 , 6 ]  . da recenti dati della letteratura , un possibile contributo alla dilatazione del colletto pu essere fornito dalloversizing dellendoprotesi che , aumentando la forza radiale della protesi sulla parete aortica , pu indurre o accelerare la degenerazione della parete aortica e la sua dilatazione [ 2 ]  . 
sulla base di tali considerazioni , potrebbe risultare utile validare un metodo in grado di identificare i pazienti con elevata distensibilit aortica , in modo tale da predire una potenziale dilatazione del colletto prossimale dellaneurisma nel follow - up a lungo termine post - evar . 
stato ipotizzato che la compliance , strettamente legata al comportamento e alla composizione della parete aortica e alla pulsatilit , possa fornire alcune informazioni utili [ 7 ]  . studi recenti hanno dimostrato che langio - tomografia computerizzata ( tc ) dinamica , eseguita con gating cardiaco , permette di ottenere informazioni sulla pulsatilit aortica e sulle modificazioni di conformazione che avvengono durante il ciclo cardiaco [ 812 ]  . 
basandoci su tali considerazioni , lobiettivo del nostro studio stato quello di valutare se langio - tc dinamica possa realmente fornire informazioni vascolari di tipo funzionale in grado di predire loutcome del colletto aortico in pazienti sottoposti ad evar . 806 radiol med ( 2012 ) 117 : 804814 of increased exposure to radiation . 
patients were divided into two groups : group a was composed of 20 consecutive patients with aaa detected on ultrasonography ( us ) who had been referred to our institution to undergo routine preoperative cta ; group b was composed of 20 consecutive patients who had been referred for standard abdominal ct for oncological follow - up . 
all patients underwent standard cta ( group a ) or ct ( group b ) examination , as clinically requested , as well as dynamic ecg - gated cta performed with double ct acquisition and double contrast - medium injection . 
 dynamic ecg - gated mdcta examinations dynamic ecg - gated data sets were acquired with a lowdose acquisition protocol ( 100 kv ) extending from the origin of celiac trunk to the aortic bifurcation using a 0.625 - mm slice collimation and a 0.625 - mm reconstruction increment during intravenous injection of 40 ml iodinated nonionic contrast medium ( iomeprol 400 mgi / ml , iomeron400 ; bracco diagnostics , inc ; milan , italy ) at a flow rate of 4 ml / s , followed by a 40 - ml saline flush injected at the same rate , using a power injector . 
scan delay was individualised per patient using bolus - tracking software ( smartprep ; ge medical systems , milwaukee , wi , usa ) , with a region of interest ( roi ) placed in the abdominal aorta at the level of the celiac trunk , with a threshold of 150 hu to trigger scanning and ensure correct peak enhancement , with a diagnostic delay of 3 s . the scanner acquired data in a nonstop helical mode while an independent electrocardiographic ( ecg ) trace was simultaneously generated . 
images were thus acquired both during systole and diastole , followed by standardised incremental 10% reconstructions performed from 5% to 95% of the cardiac cycle , at ten equidistant time points during the r - r cardiac cycle . 
data materiali e metodi design dello studio stato condotto uno studio prospettico unicentrico , arruolando 40 pazienti di et superiore a 75 anni al fine di ridurre le potenziali conseguenze correlate allesposizione a radiazioni ionizzanti . 
in particolare , i pazienti sono stati divisi in due gruppi : nel gruppo a sono stati inclusi 20 pazienti consecutivi con aaa diagnosticato allesame ecografico e che afferivano al nostro istituto per eseguire unindagine angiotc pre - trattamento , mentre nel gruppo b sono stati inclusi 20 pazienti consecutivi che afferivano al nostro istituto per eseguire un esame tc addome standard per follow - up oncologico . 
tutti i pazienti sono stati sottoposti ad esame tc con doppia acquisizione e doppia iniezione di mezzo di contrasto ( mdc ) , ovvero ad uno studio statico angio - tc ( gruppo a ) o tc addome standard ( gruppo b ) , come da richiesta clinica , e ad uno studio dinamico con gating cardiaco ; al fine di ridurre le potenziali conseguenze correlate allesposizione a radiazioni ionizzanti sono stati esclusi dallo studio pazienti con et inferiore a 75 anni . 
sono stati inoltre esclusi dallo studio pazienti con storia di cardiopatia congestizia , infarto del miocardio e aritmie severe , cos come pazienti con compromissione renale moderata o severa ( creatininemia > 1 , 5 mg / dl o clearance della creatinina < 60 ml / min / 1 , 73 m )  . 
 esame angio - tc dinamico con gating cardiaco i dati dellangio - tc dinamica sono stati ottenuti con un protocollo di acquisizione a bassa dose ( 100 kv ) , esteso dallorigine del tripode celiaco fino alla biforcazione aortica , con collimazione di 0 , 625 mm e con incremento di ricostruzione di 0 , 625 mm , durante linfusione a bolo di 40 ml di mdc iodato non ionico ( iomeprol 400 mgi / ml , iomeron - 400 ; bracco diagnostics , inc ; milano , italia ) a 4 ml / s di flusso , seguiti da 40 ml di soluzione fisiologica , utilizzando un iniettore a doppia testata . 
il ritardo di scansione ( scan delay ) stato individuato per ogni paziente usando un software semiautomatico ( smartprep ; ge medical systems , milwaukee , wi , usa ) posizionando una regione di interesse ( roi ) in aorta addominale a livello del tripode celiaco con una soglia di 150 uh per sincronizzare la scansione ed avere una corretta opacizzazione arteriosa , e con un ritardo diagnostico di 3 secondi . per lo studio dinamico , lo scanner ha acquisito i dati in maniera elicoidale continua , mentre contemporaneamente veniva registrato un tracciato elettrocardiografico ( ecg ) indipendente . 
le immagini sono state acquisite sia in sistole che in diastole e i dati ottenuti sono stati ricostruiti retrospettivamente in tutte le fasi del ciclo cardiaco , dal 5% al 95% , a dieci punti equidistanti dellintervallo r - r , con un incremento del 10% . 
al fine di annullare leffetto di sommaradiol med ( 2012 ) 117 : 804814 sets of each patient were loaded into a dedicated 3d workstation and processed using the cardiac review programme function . 
to measure aortic diameter , avoid measurement errors related to its morphology ( angulated , conical or tapered neck ) or luminal irregularity , reformatted cross - sectional images perpendicular to the long axis of the aorta were obtained to create a modified axial plane . 
to match the level of measurement , the study coordinator ( ri , with 10 years of experience in vascular imaging and interventional radiology ) , who was not involved in image evaluation , selected the images to be evaluated by the readers ; for each patient , the coordinator selected three images located : ( a ) 2 cm above the highest renal artery ( suprarenal level ) , ( b ) immediately below the lowest renal artery ( juxtarenal level ) and ( c ) 1 cm below the lowest renal artery ( infrarenal level )  . aortic distensibility dynamic reconstructed scans were reviewed twice by three independent experienced readers in random order . 
minimum and maximum diameters during the cardiac cycle were determined to evaluate aortic distension during the cycle and identify a diastolic ( minimum ) and systolic ( maximum ) diameter , respectively . 
 the term pulsatility was defined as radial displacement of the aorta lumen during a single cardiac cycle and was calculated as the largest difference between maximum ( systolic ) and minimum ( diastolic ) diameters obtained on dynamic images . 
strain ( fractional diameter change ) was defined as : pulsatility ( systolic diameter diastolic diameter ) / diastolic diameter arterial - wall distensibility was expressed as pressure strain elastic modulus ( ep ) , where : ep = k ( systolic pressure diastolic pressure ) / strain the constant k = 133.3 allows ep to be converted from millimetres of mercury to newton ( n / m2 )  . 
a nessun paziente stata somministrata una quantit di mezzo di contrasto superiore a 140 ml . valutazione delle immagini per lo scopo dello studio , sono state valutate solo le immagini acquisite con angio - tc dinamica . 
al fine di eliminare eventuali condizionamenti nella valutazione da parte dei lettori , i dati di tutti i pazienti sono stati resi anonimi e sono stati resi ignoti i parametri di imaging . 
le immagini da valutare sono state selezionate in ordine random da un altro autore ( rd , con 3 anni di esperienza in tc body ) che non ha partecipato allanalisi . 
per la misura del diametro aortico , al fine di evitare errori relativi alla morfologia aortica ( colletto angolato , conico o conico inverso ) o alla irregolarit del lume , sono state ricostruite immagini perpendicolari allasse lungo dellaorta , in modo tale da creare un piano assiale modificato . 
per stabilire il livello da misurare , il coordinatore dello studio ( ri , con 10 anni di esperienza in radiologia interventistica ed imaging vascolare ) , non coinvolto nella valutazione delle immagini , ha selezionato le immagini da far valutare ai lettori ; in particolare , per ciascun paziente , il coordinatore ha selezionato tre livelli : ( a ) 2 cm sopra larteria renale pi craniale ( livello soprarenale ) ; ( b ) immediatamente al di sotto dellarteria renale pi caudale ( livello iuxtarenale ) ; ( c ) 1 cm al di sotto dellarteria renale pi caudale ( livello infrarenale )  . distensibilit aortica le immagini dinamiche ricostruite sono state valutate da tre lettori indipendenti in ordine randoi lettori hanno eseguito le misurazioni manuali sulle immagini assiali modificate ai tre livelli selezionati . 
la pulsatilit aortica stata definita come lo spostamento radiale del lume aortico durante il ciclo cardiaco e calcolato come la differenza maggiore tra il diametro massimo ( sistolico ) e minimo ( diastolico ) ottenuto sulle immagini dinamiche . 
statistical analyses were carried out using sas release 9.2. results study population twenty consecutive adult patients older than 75 years referred for preoperative mdcta of the abdominal aorta ( group a : 16 men , four women ; mean age 79.3 years ; range 7589 years ) and 20 consecutive adult patients older than 75 years referred for standard abdominal ct study for oncological follow - up ( group b : 14 men , six women ; mean age 80.2 years ; range 7587 years ) were prospectively enrolled . 
 patients mean height and weight were 168.33.4 cm ( range 161178 cm ) and 786.5 kg ( range 6598 kg ) , respectively , for group a , and 165.55.3 cm ( range 160175 cm ) and 805.4 kg ( range 6396 kg ) , respectively , for group b . 
mean systolic and diastolic blood pressures were 128.29.1 mmhg ( range 110145 mmhg ) and 83.76.5 ( range 70100 mmhg ) ( difference between systolic and diastolic values : 48.48.1 mmhg , range 3560 mmhg ) for group a and 126.86.8 mmhg ( range 100140 mmhg ) and 79.87.8 ( range 6095 mmhg ) ( difference between systolic and diastolic values : 46.36.2 mmhg , range 3565 mmhg ) for group b . 
 in group a , statistically higher systolic and diastolic diameters were obtained in all three levels considered ( table 1 )  . aortic pulsatility / distensibility interobserver repeatability coefficient was 0.9 , with no la costante k = 133 , 3 permette la conversione della deformazione elastica da mmhg a newton ( n / m2 )  . 
si inoltre stabilito che in caso di differenza statisticamente significativa in termini di modulo pressorio di deformazione elastica ( ep ) in uno o pi livelli aortici , sulla base della distribuzione nella popolazione , si sarebbe cercato di individuare un valore cut - off in grado di identificare , nel gruppo degli aneurismatici , un sottogruppo con maggiore distensibilit aortica ( a1 : sottogruppo con regolare distensibilit ; a2 : sottogruppo con elevata distensibilit )  . 
 la pressione arteriosa sistolica e diastolica stata misurata con uno sfigmomanometro a livello dellarteria brachiale . analisi statistica i diametri ottenuti sono stati riportati come mediadeviazione standard ( sd ) per variabili continue , mentre i dati categorici e ordinali sono stati riportati come frequenze e percentuali . 
lanalisi statistica della distensibilit della parete aortica , espressa come valore di ep stata eseguita usando il test t di student , con un valore significativo per p < 0 , 05 . 
lanalisi statistica stata eseguita usando il software sas release 9.2. risultati popolazione dello studio nello studio sono stati arruolati un totale di 20 pazienti consecutivi con et superiore a 75 anni che dovevano eseguire un esame angio - tc pre - trattamento per aneurisma dellaorta addominale ( gruppo a : 16 maschi , 4 femmine ; et media : 79 , 3 anni ; range : 7589 anni ) e 20 pazienti consecutivi di et superiore a 75 anni sottoposti ad esame tc delladdome per follow - up oncologico ( gruppo b : 14 maschi , 6 femmine , et media : 80 , 2 anni ; range : 7587 anni )  . 
la frequenza cardiaca basale media ottenuta stata 71 , 3 battiti per minuto ( bpm ) ( range : 5685 ) per il gruppo a e 75 , 7 bpm ( range : 5881 ) per il gruppo b . 
il valore medio di pressione sanguigna sistolica e diastolica ottenuto stato rispettivamente di 128 , 29 , 1 mmhg ( range : 110145 mmhg ) e 83 , 76 , 5 mmhg ( range : 70100 mmhg ) ( differenza tra valore sistolico e diastolico : 48 , 48 , 1 mmhg , range : 3560 mmhg ) per il gruppo a e di 126 , 86 , 8 mmhg ( range : 100140 mmhg ) e 79 , 87 , 8 mmhg ( range : 6095 mmhg ) ( differenza tra valore sistolico e diastolico : 46 , 36 , 2 mmhg , range : 3565 mmhg ) per il gruppo b . 
nel gruppo a , i diametri sistolici e diastolici sono risultati maggiori in tutti e tre i livelli considerati in maniera statisticamente significativa ( tabella 1 )  . pulsatilit aortica / distensibilit il coefficiente di ripetibilit interosservatore stato 0 , 9 , in assenza differenze significative tra i diversi osservatori ; i dati provenienti dai tre lettori sono stati pertanto riuniti al fine di ottenere un valore medio finale del diametro aortico a ogni livello per ciascun paziente . 
1a - f immagini assiali dinamiche ricostruite nel gruppo a ( gruppo aneurismatico ) a livello soprarenale ( a , b ) , iuxtarenale ( c , d ) e infrarenale ( e , f ) ( immagini diastoliche : a , c , e ; immagini sistoliche : b , d , f )  . terms of aortic pulsatility registered at the three aortic levels ( p > 0.05 ) ( table 1 )  . when comparing groups in terms of ep , no statistically significant differences were found in the suprarenal and juxtarenal level ( p > 0.05 ) , whereas a significantly higher value ( p = 0.04 ) was obtained in the infrarenal level for group a ( 103 , 45443 , 467 n / m2 ) versus group b ( 83 , 56425 , 539 n / m2 )  . 
on the basis of distribution of ep values in the infrarenal aortic level , a cutoff value of 100 , 000 n / m2 was identified : in group a , in the infrarenal level , 11 patients ( 55% , subgroup a1 ) obtained an ep value < 100 , 000 n / m2 , whereas nine patients ( 45% , subgroup a2 ) obtained an ep value > 100 , 000 n / m2 . 
2a - f immagini assiali dinamiche ricostruite nel gruppo b ( gruppo non aneurismatico ) a livello soprarenale ( a , b ) , iuxtarenale ( c , d ) e infrarenale ( e , f ) ( immagini diastoliche : a , c , e ; immagini sistoliche : b , d , f )  . also on preventing procedure - related complications . 
one of the most clinically relevant procedure - related complications is stent - graft migration , which is a late - term complication of evar evidenced by downward slippage of the endograas an end result , migration can lead to repressurisation of the aneurysmal sac , type i endoleak , aneurysm growth and even rupture [ 13 ]  . 
multiple factors have been postulated to predict and affect endovascular graft migration : knowledge of the pathophysiology and forces that lead to migration is central to its prevention , diagnosis and treatment . 
recent reports support the hypothesis that aneurysmal progression could play a key role in the aetiology of and , which is a marker of and a possible risk factor for migration [ 14 ]  . 
 to the best of our knowledge , there are no published studies on the attempt to predict post - evar proximal and in the long - term follow - up on the basis of physical characteristics . 
it is well known that development of aneurysmal disease is a complex and multifactorial process that may involve an imbalance between synthesis and degradation of elastin and collagen , together with autoimmune , inflammatory and haemodynamic responses . 
una delle complicanze a lungo termine del trattamento endovascolare clinicamente pi rilevante rappresentata dalla migrazione dellendoprotesi che pu portare alla riperfusione della sacca aneurismatica , con conseguente endoleak di tipo i , crescita dellaneurisma e spesso rottura [ 13 ]  . 
sono stati 812 radiol med ( 2012 ) 117 : 804814 considerati multipli fattori in grado di predire ed influenzare la migrazione dellendograft : la conoscenza della fisiopatologia e delle forze che agiscono sullendograft determinandone la migrazione , essenziale nella sua prevenzione , diagnosi e trattamento . 
recenti studi suggeriscono lipotesi che la progressiva dilatazione aneurismatica possa giocare un ruolo chiave nella eziologia della dilatazione del colletto , possibile marker e fattore di rischio per la migrazione [ 14 ]  . non ci sono a tuttoggi studi pubblicati che suggeriscono , sulla base delle caratteristiche fisiche , come prevenire la dilatazione del colletto prossimale post - evar nel follow - up a lungo termine . 
ormai noto come alla base dello sviluppo della dilatazione aneurismatica vi sia un complesso processo multifattoriale che coinvolge da un lato unalterazione dellequilibro tra sintesi e degradazione di elastina e collagene e dallaltro fattori autoimmunitari , infiammatori ed emodinamici . 
in particolare , la degenerazione della parete aortica potrebbe essere correlata ad una significativa riduzione della sintesi di elastina e di cellule muscolari lisce ed ad un incremento di collagene e matrice extracellulare , con conseguente perdita della compliance e minore distensibilit della parete aortica [ 7 , 15 , 16 ]  . 
nel nostro studio stato utilizzato uno scanner 64 strati , rapido e con elevata risoluzione spaziale e temporale unito allimpiego di un mezzo di contrasto ad elevata concentrazione di iodio per minimizzare lattenuazione intrarteriosa [ 17 , 18 ]  . 
i nostri dati confermano che esiste una variabilit significativa in termini di pulsatilit aortica allinterno del colletto dellaneurisma durante il ciclo cardiaco sia nel gruppo dei pazienti aneurismatici che nei non aneurismatici ; in particolare , durante il ciclo cardiaco , stata ottenuta una pulsatilit media di 8 , 41%2 , 91% e 8 , 44%2 , 51% rispettivamente nel gruppo a e b , in assenza di una differenza statisticamente significativa . 
nessuna differenza statisticamente significativa di pulsatilit aortica stata rilevata ai tre livelli allinterno del colletto ( soprarenale vs iuxtarenale vs infrarenale p > 0 , 05 )  . i risultati pi interessanti del nostro studio sono rappresentati dal fatto che confrontando i due gruppi ( gruppo a e gruppo b ) in termini di modulo pressorio di ep , non si sono documentate differenze statisticamente significative a livello soprarenale e iuxtarenale , mentre esiste una differenza statisticamente significativa nel tratto infrarenale , nel gruppo a ( pazienti aneurismatici )  . 
in detail , aortic - wall degeneration could be related to a significant decrease in elastin and smooth - muscle content and increase in collagen and ground substance , with a consequent loss of compliance and less distensibility of the aortic wall [ 7 , 15 , 16 ]  . 
we used a 64 - slice scanner capable of rapid , high - resolution image acquisition , together with a high - iodine - concentration contrast medium to maximise intra - arterial attenuation [ 17 , 18 ]  . 
furthermore , no statistically significant differences were found between groups in terms of aortic pulsatility registered at the three aortic levels ( suprarenal , juxtarenal , infrarenal )  . the principal findings of our study are that when comparing the two groups in terms of ep , no statistically significant differences were found in the suprarenal and juxtarenal level , whereas a significantly higher value was obtained for group a in the infrarenal level . 
this seems to indicate that in patients with abdominal aortic disease , the infrarenal aortic neck is also involved by aneurysmal progression , even if the size is not increased . 
furthermore , in group a , based on ep distribution in the infrarenal aortic level , a cutoff value of 100 , 000 n / m2 was identified , allowing recognition of patients ( 45% ) with significantly higher aortic - wall degeneration , potentially predicting post - evar proximal and in long - term follow - up on the basis of physical characteristics . the main limitation of our study was the relatively small number of patients examined ; further investigations with a large series of patients is needed to confirm our findings and recognise a defined cutoff for ep . 
it would be interesting to demonstrate in such a follow - up the eventual dilation of the infrarenal aortic neck in patients with higher aortic - wall degeneration ; however , this investigation falls beyond the scope of this pilot study and remains a goal for future studies . in conclusion , our study seems to demonstrate that dynamic ct imaging could provide insight into the pathophysiology of the abdominal aorta . 
it seems to demonstrate that in patients with abdominal aortic disease , the infrarenal aortic neck is also affected by aneurysmal progression , even if the size is not increased . 
furthermore , identifying patients with higher infrarenal distensibility , potentially predicting post - evar proximal and in the long - term follow - up , could change stent - graft selection to ensure improved fixation . 
inoltre , nel gruppo dei pazienti aneurismatici , sulla base della distribuzione di ep al livello infrarenale , stato identificato un valore cut - off di 100.000 n / m2 , che permette di riconoscere pazienti con una degenerazione della parete aortica significativa ( 45% ) , potenzialmente predittiva di dilatazione del colletto prossimale post - evar nel follow - up a lungo termine sulla base delle caratteristiche fisiche . il principale limite del nostro studio costituito dal numero relativamente basso di pazienti esaminati ; per confermare quanto detto e definire un cut - off preciso di modulo pressorio di deformazione elastica , necessario estendere lo studio ad un gruppo pi ampio di pazienti . 
tuttavia tale approfondimento esula dallobiettivo del nostro studio e costituisce un obiettivo per studi futuri . in conclusione , il nostro studio sembra dimostrare che limaging tc dinamico sia in grado di fornire unanalisi della fisiopatologia dellaorta addominale : sembra infatti dimostrare che il colletto infrarenale dei pazienti con aneurisma dellaorta addominale sia coinvolto dalla progressione aneurismatica , anche in assenza di effettivo incremento dimensionale . 
inoltre , lidentificazione di pazienti con elevata distensibilit infrarenale , che pu potenzialmente predire una dilatazione del colletto prossimale post - evar nel follow - up a lungo termine , pu modificare la scelta dello stent - graft da impiantare , garantendo un miglior ancoraggio . 
tale dato potrebbe spiegare alcune delle complicanze post - trattamento correlate allo stent - graft , come la migrazione dellendoprotesi o lendoleak di tipo i , in grado di peggiorare loutcome dei pazienti . 
of these , 26 / 31 were treated with metal coils , 3 / 31 with cardiatis multilayer stent , 1 / 31 with a coated stent and 1 / 31 with coils and amplatzer plug . 
da gennaio 2002 a settembre 2009 sono stati trattati con terapia endovascolare 30 pazienti ( 22 maschi , 8 femmine ) portatori di aneurismi ( n = 18 ) o pseudoaneurismi ( n = 13 ) originanti dallarteria splenica ( n = 11 ) , epatica ( n = 6 ) , renale ( n = 5 ) , pancreaticoduodenale ( n = 3 ) , gastrica sinistra ( n = 2 ) , gastroduodenale ( n = 1 ) , rettale ( n = 1 ) , colica media ( n = 1 ) e dal tripode celiaco ( n = 1 )  . 
ventisei / 31 sono stati trattati con spirali metalliche , 3 / 31 con stent multimaglia cardiatis , 1 / 31 con spirali e amplatzer plug , 1 / 31 con stent ricoperto . 
 some 60% of splanchnic aneurysms originate from the splenic artery , 20% from the hepatic arteries , 5.5% the coeliac axis , 4% the superior mesenteric artery , 4% the gastric and gastroepiploic arteries , 3% the intestinal arteries , 2% the pancreaticoduodenal arteries , 1.5% the gastroduodenal artery and < 1% the inferior mesenteric artery [ 5 ]  . most vaa are asymptomatic and are often diagnosed incidentally . 
whereas the aetiology of vaa is prevalently the result of atheromatous disease , the causes of vapa are atherosclerosis , trauma , iatrogenic injury , inflammation or infection [ 4 ]  . 
vap diagnosis , generally made as an incidental finding , can be made with colour - doppler ultrasound ( cdus ) sonography , which in some cases shows the flow within the vessels and visualises the origin of the sac , its size and presence of a thrombus . 
nonetheless , the technique of choice for accurately evaluating the vascular anatomy and the presence of an aneurysmal neck , as well as measuring vessel diameters , is computed tomography angiography ( cta ) [ 5 ]  . 
whereas treatment of bleeding vap cannot be delayed , there are no indications in the literature regarding treatment timing for nonbleeding vap ; in general , treatment is suggested when they exceed 2 cm in diameter [ 4 , 6 , 7 ]  . 
today , interventional radiology has proven to be highly suited to this type of condition , thanks to reduced invasiveness , high success rate and lower risk of complications [ 4 , 8 , 9 ]  . 
indeed , vap can be treated with percutaneous techniques such as transcatheter embolisation , injection of thrombin and deployment of coated or multilayer stents , alone or in combination [ 1013 ]  . the aim of our study was to evaluate the feasibility , efficacy and safety of endovascular treatment of vap . materials and methods a retrospective study was performed by reviewing patients gli aneurismi ( vaa ) e gli pseudoaneurismi ( vapa ) viscerali ( aneurismi + pseudoaneurismi = vap ) rappresentano unentit patologica relativamente rara con unincidenza variabile dallo 0 , 01% allo 0 , 2% [ 14 ]  . 
gli aneurismi renali hanno incidenza molto bassa ( 0 , 01%0 , 09% ) , mentre per quelli splancnici risulta relativamente maggiore ( 0 , 1% 0 , 2% )  . 
nel gruppo degli aneurismi splancnici il 60% origina dallarteria splenica seguita dalle arterie epatiche ( 20% ) , dal tronco celiaco ( 5 , 5% ) , dallarteria mesenterica superiore ( 4% ) , dalle arterie gastrica e gastroepiploica ( 4% ) , dalle arterie intestinali ( 3% ) , dalle arterie pancreaticoduodenali ( 2% ) , dallarteria gastroduodenale ( 1 , 5% ) e dallarteria mesenterica inferiore ( < 1% ) [ 5 ]  . la maggior parte dei vaa sono asintomatici e spesso vengono diagnosticati incidentalmente . 
la diagnosi di vap , generalmente accidentale o come reperto occasionale , pu essere effettuata con leco - color doppler ( ecd ) , che in grado , in alcuni casi , di dimostrare il flusso allinterno dei vasi , visualizzare lorigine della sacca , le sue dimensione e leventuale presenza di apposizione trombotica . 
tuttavia , al fine di valutare pi precisamente lanatomia vascolare , la presenza di eventuali colletti e le misure dei calibri vascolari , langiotomografia computerizzata ( atc ) rappresenta la metodica di scelta [ 5 ]  . 
sebbene il trattamento di vap sanguinanti sia indifferibile , non esistono in letteratura indicazioni condivise circa il trattamento dei vap non sanguinanti , e in generale si ritiene necessario un trattamento quando questi superano i 2 cm di diametro [ 4 , 6 , 7 ]  . 
attualmente le tecniche di radiologia interventistica bene si adattano a questo tipo di patologia per la minore invasivit , lalto successo tecnico e il minor rischio di complicanze [ 4 , 8 , 9 ]  . 
1a , b distribuzione degli aneurisnmi ( vaa ) e degli pseudoaneurismi ( vapa ) ; b eziologia degli pseudoaneurismi . with vap who underwent endovascular treatment between january 2002 and september 2009 . materiali e metodi patients thirty - one vap were treated in 30 patients ( 22 men , eight women ) , aged between 24 and 85 ( mean age 59.8 ) years ; one patient was found to have two splenic aneurysms . 
all patients who were symptomatic or asymptomatic with a vap of the coeliac axis , the superior mesenteric artery , the inferior mesenteric artery , the renal artery and of their respective branches were included in the study . 
in 20 patients , the procedure was performed with anaesthesia : conscious sedation in 17 / 20 cases ; general anaesthesia in 3 / 20 cases . diagnosis stato eseguito uno studio retrospettivo analizzando i pazienti con vap sottoposti a trattamento endovascolare da gennaio 2002 a settembre 2009 . pazienti sono stati complessivamente trattati 31 vap in 30 pazienti ( 22 maschi e 8 femmine ) , con et compresa tra 24 e 85 anni ( et media 59 , 8 anni ) ; una paziente risultava portatrice di due aneurismi splenici . 
sono stati inclusi nello studio tutti i pazienti , sintomatici o asintomatici , portatori di vap del tripode celiaco , dellarteria mesenterica superiore , della mesenterica inferiore , della renale e delle loro rispettive branche . 
in 20 pazienti la procedura stata eseguita con assistenza anestesiologica ; in particolare 17 / 20 sono stati sottoposti a sedazione , mentre per gli altri 3 / 20 si resa necessaria lanestesia generale . the diagnosis of vap was made with a cta system ( brilliance ct - 64 , philips , eindhoven , the netherlands ) or doppler ultrasound system ( acuson s2000 , siemens , erlangen , germany ) , except in three haemodynamically unstable patients who required an emergent angiography study ( integris , philips , eindhoven , the netherlands )  . 
anatomical distribution of vap was as follows : 11 / 31 arising from the splenic artery ( 35.5% ) , six the hepatic artery ( 19.5% ) , five the renal artery ( 16% ) , three the pancreaticoduodenal artery ( 9.5% ) , two the left gastric artery ( 6.5% ) and in the remaining 4 / 31 ( 13% ) , one each from the gastroduodenal artery , rectal artery , colic artery and coeliac axis . vaa aetiopathogenesis was atherosclerotic in 15 / 18 patients . 
la distribuzione anatomica dei vap trattati includeva : 11 / 31 originanti dallarteria splenica ( 35 , 5% ) , 6 dallepatica ( 19 , 5% ) , 5 dalla renale ( 16% ) , 3 dalla pancreatico - duodenale ( 9 , 5% ) , 2 dalla gastrica sinistra ( 6 , 5% ) , ed i restanti 4 / 31 ( 13% ) rispettivamente 1 dalla gastroduodenale , 1 dalla rettale , 1 dalla colica media , 1 dal tripode celiaco . leziopatogenesi dei vaa era aterosclerotica in 15 / 18 pazienti . 
the remaining 20 symptomatic patients ( 66.7% ) presented with signs and / or symptoms of anaemia : four had haematemesis , three haematuria , one rectorrhagia and the remaining 12 showed ct signs of abdominal or retroperitoneal bleeding . 
in three patients , endovascular intervention was performed as an emergent procedure following active bleeding and haemodynamic instability defined as arterial pressure < 90 mmhg or infusion of at least 6u of whole blood in the previous 24 h . 
all vapa were symptomatic at presentation . dieci pazienti erano asintomatici ( 33 , 3% ) e la diagnosi di vap stata occasionale durante esecuzione di esami tc o ecografici per altri motivi . 
i restanti 20 pazienti ( 66 , 7% ) sintomatici si erano presentati con segni e / o sintomi dellanemizzazione ; in particolare 4 presentavano ematemesi , 3 ematuria , 1 rettorragia e i rimanenti 12 pazienti presentavano allesame tc un sanguinamento addominale o retroperitoneale . 
in 3 pazienti la procedura endovascolare stata eseguita in regime durgenza in seguito a sanguinamento attivo e instabilit emodinamica definita come pressione arteriosa < 90 mmhg o come infusione di almeno 6 sacche di sangue intero nelle ultime 24 ore . 
sette / 18 vaa ( 38 , 8% ) erano sintomatici ; i restanti 11 erano asintomatici , identificati incidentalmente e trattati sulla base di criteri esclusivamente dimensionali ( > 20 mm )  . 
differentemente dai vaa , tutti i vapa erano sintomatici alla presentazione . technique tecnica the endovascular procedure was performed in an angiography suite with a digital angiograph ( integris allura , philips , eindhoven , the netherlands )  . 
the preferential percutaneous access site was the right femoral artery in all except one case of pseudoaneurysm of the coeliac axis , in which access via the left axillary artery was preferred . 
a 5 - f vascular introducer ( terumo , tokyo , japan ) was used in all except three cases in which a 6 - f introducer was used and one in which a 9 - f introducer was used . 
a triaxial system was used with telescopic technique and a microcatheter ( fastracker , boston scientific ; or renegade , progreat , terumo , tokyo , japan ) in 19 / 30 patients whose vascular anatomy was particularly tortuous . 
the microcatheter also proved useful in cases of selective embolisation of the aneurysmal sac , enabling preservation of flow in the main vessel . all patients received 2 , 500 u of heparin , except those who were haemodynamically unstable . 
technical success was defined as the correct release of the device with no further angiographic evidence of the aneurysmal sac or extraluminal leakage of contrast material . la procedura endovascolare stata eseguita in sala angiografica mediante angiografo digitale ( integris allura , philips , eindhoven , olanda )  . 
 stato sempre utilizzato un introduttore vascolare di 5 f ( terumo , tokyo , giappone ) di calibro , fatta eccezione per i trattamenti in cui si sono impiegati introduttori da 6 f in 3 casi e da 9 f in un caso . 
stata utilizzata guida idrofilica 0 , 035 inch ( terumo , tokyo , giappone ) e catetere shepper hook ( boston scientific , natick , usa ) o cobra idrofilico ( terumo , tokyo , giappone ) per cateterizzare il vaso viscerale . 
 stato utilizzato un sistema triassiale con tecnica telescopica e impiego di microcatetere ( fastracker o renegade , boston scientific , natick , usa o progreat , terumo , tokyo , giappone ) in 19 / 30 pazienti nei casi in cui lanatomia vascolare era particolarmente tortuosa . 
il microcatetere risultato utile anche nei casi di selettiva embolizzazione della sacca aneurismatica permettendo di preservare il flusso nel vaso principale . a tutti pazienti stata somministrata eparina ( 2500 unit ) tranne in quelli emodinamicamente instabili . 
il successo tecnico stato definito come il corretto rilascio del device senza pi dimostrazione angiografica della sacca aneurismatica o di spandimento extraluminale di mezzo di contrasto . 820 follow - up periprocedural complications and morbidity and mortality rates within 30 days of treatment were recorded . 
the correct exclusion of the aneurysm was documented both as cessation of bleeding and absence of flow within the aneurysmal sac at cta or cdus performed at 1 , 6 and 12 months . 
in cases of vaa in which a metallic stent was used , size reduction of the aneurysmal sac was also evaluated at 1 , 6 and 12 months . results in most patients ( 26 / 30 ) , vap was treated with the release of nonmagnetic metal coils covered with dacron fibres ( vortex , boston scientific ; or reye , cook , bloomington , usa ) , platinum coils ( balt , monmorency , france ) or microcoils ( vortex , boston scientific )  . 
cases in which vapa was secondary to interventional procedures ( one postpyelostomy and one after biliary drainage ) , coil embolisation was done after temporary retraction of the drainage catheter from the parenchyma with the assistance of a guidewire . 
in patients who showed no symptoms or signs of active bleeding , the size criteria was used , with treatment being considered necessary in aneurysms 20 mm in diameter . radiol med ( 2012 ) 117 : 815830 follow - up sono state raccolte le complicanze periprocedurali , la morbilit e la mortalit entro 30 giorni dal trattamento . 
 la corretta esclusione dellaneurisma stata documentata sia come cessazione del sanguinamento sia come assenza di flusso allinterno della sacca allesame atc o eco - color doppler a 1 , 6 e 12 mesi . 
nei casi di vaa in cui stato impiegato uno stent metallico si inoltre valutata la riduzione delle dimensioni della sacca aneurismatica a 1 , 6 e 12 mesi . risultati nella maggioranza dei pazienti ( 26 / 30 ) il vap stato trattato mediante rilascio di spirali metalliche amagnetiche e rivestite con fibre in dacron ( vortex , boston scientific , natick , usa o reye , cook , bloomington , usa ) oppure spirali in platino ( balt , montmorency , francia ) o microspirali ( vortex , boston scientific , natick , usa )  . 
i casi in cui i vapa erano secondari a procedure interventistiche ( 1 postpielostomia e 1 dopo drenaggio biliare ) lembolizzazione con spirali metalliche stata eseguita previa temporanea retrazione del catetere di drenaggio dal parenchima con lausilio di filo guida . 
3a - d dsa : pseudoaneurisma dellarteria epatica propria ( * ) ( a ) ; cateterizzazione selettiva del ramo efferente laneurisma con microcatetere angiografico ( b ) ; esclusione dellaneurisma con microspirali metalliche a monte e a valle della lesione mediante isolation - tecnique ( c ) ; controllo angiografico finale con esclusione dellaneurisma ( d )  . a total of 26 / 31 ( 84% ) vap were embolised with metal coils , 3 / 31 ( 9.5% ) with cardiatis multilayer stents and the remaining 2 / 31 ( 6.5% ) with coils and amplatzer plug or fluency - coated stent . 
one patient with a pseudoaneurysm of the coeliac axis died 10 days after treatment as a result of renewed haemorrhage , producing a 30 - day mortality of 3% . follow - up was performed both clinically ( cessation of bleeding ) and at 1 , 6 and 12 months with cdus or cta . 
follow - up was done with cta in 20 / 30 patients , with cdus in 2 / 30 patients and in the remaining 8 / 30 patients ( six symptomatic and with signs of active bleeding ) invece il criterio stato volumetrico , ed stato considerato necessario il trattamento in caso di aneurisma di diametro superiore ai 20 mm . ventisei / 31 ( 84% ) vap sono stati embolizzati con spirali metalliche , 3 / 31 ( 9 , 5% ) con stent multimaglia cardiatis , e i restanti 2 ( 6 , 5% ) rispettivamente con spirali ed amplatzer plug oppure con stent ricoperto fluency . 
 un paziente portatore di pseudoaneurisma del tripode celiaco deceduto dopo 10 giorni dal trattamento in seguito a nuovo sanguinamento , con una mortalit a 30 giorni del 3% . il follow - up stato eseguito sia clinicamente ( cessazione del sanguinamento ) sia a 1 , 6 e 12 mesi mediante eco - color 822 radiol med ( 2012 ) 117 : 815830 fig . 
4a - d digital subtraction angiography in a patient with posttraumatic pseudoaneurysm ( * ) of the inferior polar artery of the right kidney ( a , b )  . 
4a - d dsa in paziente portatore di pseudoaneurima post - traumatico ( * ) , dellarteria polare inferiore del rene destro ( a , b ) ; embolizzazione con microcatetere angiografico e spirali metalliche ( c ) ; controllo finale con esclusione dello pseudoaneurisma ( d )  . the good outcome of the procedure was verified by the cessation of bleeding . 
in particular , in two cases the significant amount of metal made it impossible to verify the exclusion of the aneurysmal sac such that these patients underwent cdus study . during follow - up all , vaa remained excluded , and no new endovascular procedure was required in any patient . 
in 5 / 10 patients ( 50% ) with splenic vap ( four vaa , one vapa ) , ischaemia of the parenchyma occurred ( with cta evaluation of the ischaemic tissue varying from 10% to 90% )  . 
il follow - up con esame tc stato effettuato in 20 / 30 pazienti , in 2 / 30 pazienti con eco - color doppler ; nei rimanenti 8 pazienti ( 6 sintomatici e con segni di sanguinamento attivo ) il buon esito della procedura stato attestato dalla cessazione del sanguinamento . 
 in particolare in 2 casi la presenza di abbondante materiale metallico non ha permesso di stabilire la reale esclusione della sacca aneurismatica e pertanto questi pz sono stati sottoposti a controllo con eco - color doppler . 
5a - d dsa con dimostrazione di aneurisma dellarteria splenica ( * ) ( a ) ; rilascio di un primo stent ricoperto con incompleta esclusione della sacca ( # ) ( b ) ; embricatura di un secondo stent ricoperto ( c ) ; controllo finale con corretta esclusione della sacca aneurismatica ( d )  . the percentage of ischaemic tissue varying from 10% to 25% . 
non si sono registrati casi di infarto epatico o intestinale . dei 4 pazienti in cui si impiantato uno stent metallico si valutata oltre alla perviet dello stent anche la riduzione delle dimensioni della sacca aneurismatica . 
6a - d dsa : presenza di aneurisma dellarteria splenica ( * ) ( a ) ; cateterizzazione del tratto distale dellarteria splenica con rilascio di amplatzer plug 4 da 8 mm di diametro ( # ) ( b ) ; embolizzazione della sacca con spirali metalliche ( c ) e rilascio di unulteriore plug da 8 mm a monte dellaneurisma ( c ) ; controllo finale con esclusione della sacca e rivascolarizzazione del parenchima splenico grazie al compenso dei rami gastrici brevi ( d )  . discussion vap is a rare but potentially lethal pathological condition . 
recent years have seen an increase in the detection of these lesions due to an increase in both the number and resolution of diagnostic techniques ( ct ) and an increase in percutaneous , endoscopic and laparoscopic procedures on the biliary and urinary systems [ 4 ]  . traditional surgical treatment of these aneurysms is considered the reference standard [ 6 , 9 ]  . 
7a - d digital subtraction angiography of the coeliac axis shows an aneurysm of the hepatic artery ( * ) ( a ) treated with deployment of the cardiatis multilayer stent ( b , c )  . 
in addition , the literature [ 1416 ] shows that endovascular treatment is preferable in vap in the following circumstances : lesions secondary to acute pancreatitis ; lesions of the mesenteric artery secondary to iatrogenic injury or sepsis ; intrahepatic iatrogenic or traumatic lesions ; in haemodynamically unstable patients . 
in these situations , open surgery is difficult to perform due to the technical difficulty and patients clinical conditions ( haemodynamic instability ) and comorbidities ( pancreatitis , hepatobiliary disease )  . most published studies on the surgical treatment of vap are limited to small patient series or case reports . 
 [ 6 ] , mero e della risoluzione delle tecniche diagnostiche ( tc ) sia allaumento degli interventi percutanei , endoscopici e laparoscopici su vie biliari e urinarie [ 4 ]  . 
dalla letteratura [ 1416 ] si evince inoltre che il trattamento endovascolare da preferire nei vap : secondari a pancreatite acuta ; dellarteria mesenterica iatrogeni o secondari a sepsi ; iatrogeni o traumatici intraepatici ; in pazienti emodinamicamente instabili . 
in queste situazioni la chirurgia a cielo aperto di difficile attuazione sia per le difficolt tecniche sia per le condizioni cliniche ( instabilit emodinamica ) e di comorbilit ( pancreatite , patologia epatobiliare ) dei pazienti . 
8a - d axial ( a , b ) , coronal and sagittal ( c , d ) computed tomography angiography scans show results of coil embolisation ( # ) of the postpancreatic pseudoaneurysm of the splenic artery . 
8a - d atc : scansioni assiali ( a , b ) coronali e sagittali ( c , d ) in cui si apprezzano gli esiti dellembolizzazione con spirali metalliche ( # ) di pseudoaneurimsa post - pancreatitico dellarteria splenica : si apprezzi la voluminosa necrosi del parenchima splenico ( * ) con sovrainfezione associata testimoniata dalla presenza di bolle aeree nel contesto . 
the perioperative mortality rate is probably even higher in cases of ruptured aneurysms of the hepatic artery , the mesenteric region and the renal artery . endovascular treatment can provide benefits in terms of survival not only in elective interventions but also in emergent procedures in patients with aneurysm rupture . 
 indeed , in our study the technical success was 100% , with immediate exclusion of the aneurysmal sac , no evidence of periprocedural complications and a 30 - day mortality rate of 3% . 
la mortalit perioperatoria probabilmente ancora pi alta in caso di rottura di aneurismi epatici , del distretto mesenterico e dellarteria renale . il trattamento endovascolare pu fornire un beneficio in termini di sopravvivenza non solo negli interventi elettivi , ma anche nelle procedure eseguite durgenza in pz con rottura di aneurisma viscerale . 
in this case , embolisation was technically impossible due to the absence of a suitable aneurysmal neck and consequent high risk of coil migration or occlusion of the entire coeliac axis . 
in addition , the hostile anatomical situation , with a markedly sharp origin of the coeliac axis , did not allow catheterisation of the vessel with an 8 - f introducer ( indispensible for deploying the coated stent )  . 
the choice was therefore made to treat the aneurysm with a new - generation multilayer stent via axillary access , which allowed the use of a smaller diameter introducer ( 6 - f )  . 
the stent , which should reduce flow inside the sac within 30 days , was unable to interrupt the haemorrhage in the following days , which suggests that this device should not be used in bleeding vapa . in our study , most vapa involved the splenic region ( 33% ) , which is in agreement with data reported in the literature [ 4 , 10 ]  . 
half of our patients with a splenic artery aneurysm were affected by infarction of the splenic parenchyma , with the percentage of ischaemic tissue varmediata della sacca aneurismatica senza evidenza di complicanze periprocedurali e con una mortalit a 30 giorni dal trattamento del 3% . 
tale paziente , affetto da pancreatite necrotico - emorragica , era portatore di vapa del tripode ; in questo caso lembolizzazione era tecnicamente impossibile per assenza di adeguato colletto con elevato rischio di migrazione di spirali o di occlusione di tutto il tripode . 
 inoltre la situazione anatomica ostile , con origine del tripode assai angolata , non permetteva cateterismo del vaso con introduttore di 8 f di calibro ( indispensabile per il rilascio di stent ricoperto )  . 
si optato quindi per il trattamento con stent multimaglia di nuova generazione con accesso ascellare , che ha consentito di utilizzare un introduttore di calibro relativamente ridotto ( 6 f )  . 
tale stent , che dovrebbe ridurre il flusso allinterno della sacca entro 30 giorni , non ha tuttavia consentito di interrompere lemorragia nei giorni seguenti , dato che suggerirebbe che tale device non dovrebbe essere utilizzato nei vapa sanguinanti . nel nostro studio la maggior parte dei vapa interessava il distretto splenico ( 33% ) come del resto ampiamente riportato in letteratura [ 4 , 10 ]  . 
when embolisation involved the vessel in the immediate vicinity of the origin of bleeding , or when the presence of a suitable neck allowed embolisation of the aneurysmal sac alone , splenic infarction was not identified due to the compensatory flow from the short gastric branches or the guaranteed patency of the splenic artery . the endovascular technique , reported to notably reduce splenic infarction and receiving increasing intention [ 12 ] , involves deployment of coated stents . 
in these situations , bringing a large - diameter introducer ( 89 f ) in proximity of the lesion is a particularly complex task . ischaemic phenomena were also recorded in three of the four patients with renal artery vapa , with the percentage of ischaemic tissue varying from 10% to 25% . 
the only case in which parenchymal ischaemia was not observed involved a vaa with a neck in which coil embolisation of the aneurysmal sac alone could not be performed . another interesting feature of our series was the two cases of aneurysms of the pancreaticduodenal arch associated with chronic obstruction of the coeliac axis . 
 [ 19 ] report , obstruction of the coeliac axis and the consequent compensatory hypertrophy of the pancreaticduodenal circulation causes haemodynamic alterations that favour the development of pancreaticduodenal arch aneurysms . 
in these situations , embolisation proves particularly difficult due to tortuosity of the vascular segments involved , thus obliging the operator to use angiographic microcatheters . special attention should also be drawn to the two patients with hepatic artery aneurysms treated with deployment of a cardiatis multilayer stent . 
this stent , which has only been available since may 2009 , is a coated stent consisting of a double layer of cobalt mesh that reduces flow in the aneurysmal sac up to complete thrombosis within 30 days . 
in addition , it has a lower profile than similarly sized coated stents and is theretori di aneurisma splenico si verificato un infarto del parenchima splenico con percentuale di tessuto ischemico variabile dal 10% al 90% . 
tale reperto si dimostrato privo di sequele cliniche in 4 pazienti , mentre in una sola paziente si verificata sovrainfezione con sindrome peritoneale che ha obbligato allintervento chirurgico di splenectomia . 
quando lembolizzazione ha interessato il vaso nel sanguinamento a ridosso dellorigine o nei quali la presenza di un adeguato colletto ha permesso lembolizzazione della sola sacca aneurismatica linfarto della milza non stato documentato in accordo sia con il compenso sostenuto dai rami gastrici brevi sia con la garantita perviet dellasse splenico . 
 [ 19 ] infatti lostruzione cronica del tripode celiaco e la conseguente ipertrofia compensatoria dei circoli pancreatico - duodenali determina alterazioni emodinamiche che favoriscono lo sviluppo di aneurismi dellarcata pancreatico - duodenale . 
in tali situazioni lembolizzazione risulta particolarmente difficoltosa a causa delle notevoli tortuosit dei segmenti vascolari coinvolti e obbliga loperatore allutilizzo di microcateteri angiografici . un discorso a parte meritano i due pazienti portatori di aneurismi dellarteria epatica trattati con il posizionamento di stent multimaglia cardiatis . 
tale stent , disponibile solo dal maggio 2009 , uno stent ricoperto a doppia maglia di cobalto che consente di ridurre il flusso nella sacca aneurismatica sino alla sua completa trombizzazione nellarco di 30 giorni . 
these characteristics make the stent particularly useful in treating visceral artery aneurysms , which are often tortuous and in which preserving collateral vessel patency is extremely important and the aneurysmal neck is either unsuitable or absent . 
queste caratteristiche rendono intuitiva lutilit di tale stent nel trattamento di aneurismi del distretto viscerale spesso tortuosi e dove estremamente importante conservare la perviet dei vasi collaterali e dove spesso i colletti sono corti o non presenti . 
il controllo tc a 1 , 6 e 12 mesi ha confermato in entrambi i casi lesclusione completa dei vaa con mantenuta perviet dei vasi collaterali e con iniziale riduzione di volume della sacca aneurismatica . il nostro studio presenta per alcuni limiti : ( 1 ) sono stati considerati tutti i risultati dei vap senza distinguere tra vaa e vapa ; ( 2 ) non stata fatta una distinzione circa il distretto anatomico interessato , includendo nello studio sia aneurismi del tripode , dellarteria mesenterica superiore , dellarteria mesenterica inferiore e dei loro rami , sia aneurismi dellarteria renale ; ( 3 ) nei casi di vapa sanguinanti spesso il follow - up stato clinico e non mediante tc , inoltre nei casi in cui si effettuato il follow - up tc gli artefatti derivanti dallutilizzo di spirali metalliche hanno in parte reso difficoltosa linterpretazione dellesame . 
 we implanted three fiducial markers ( gold seeds ) within the prostatic gland in order to quantify daily target displacements and to generate specific margins around the clinical target volume ( ctv ) to create an appropriate planned target volume ( ptv )  . 
after manual localisation , comparison between the position of the gold seeds on the portal and reference images was carried out , and a set of extrapolated laterallateral ( ll ) , anterior - posterior ( ap ) and cranialcaudal ( cc ) shift riassunto obiettivo . 
la moderna radioterapia ha raggiunto traguardi considerevoli in termini di controllo tumorale e riduzione dei tassi di tossicit associati al trattamento , con la possibilit di erogare dosi importanti al volume bersaglio , risparmiando contemporaneamente i tessuti sani . 
tra aprile e dicembre 2009 , 10 pazienti affetti da adenocarcinoma prostatico organo - confinato sono stati sottoposti ad impianto trans - rettale sotto guida ecografica di 3 reperi fiduciali radio - opachi . 
ogni paziente stato sottoposto a tomografia computerizzata ( ct ) di pianificazione con una adeguata preparazione vescicale e rettale ; ad ogni seduta di trattamento , sono state acquisite 2 immagini ortogonali e poi confrontate con immagini radiografiche a ricostruzione digitale . 
systematic and random errors for each direction were calculated either as measured according to displacement of the gold seeds prior to any couch movement and after couch position correction according to the radio - opaque markers . 
a scatter plot generated on all measurements after couch repositioning according to gold - seed displacement suggested a confidence range of shift distributions within 5 mm for ll , 8 mm for cc , and 7 mm for ap . 
 keywords image - guided radiotherapy prostate cancer fiducial markers gold seeds treatment margins una localizzazione manuale confrontando la posizione dei reperi fiduciali nelle immagini portali con quella nelle immagini di riferimento . 
sono stati calcolati lerrore standard e sistematico per ogni direzione , misurando gli scostamenti dei semi doro prima del movimento del lettino di trattamento e dopo aver applicato gli spostamenti secondo i reperi fiduciali . 
per i reperi cutanei , lerrore sistematico e casuale medio sono stati 0 , 122 , 94 mm per la direzione ll , 1 , 043 , 37 mm per la direzione ap e 1 , 142 , 71 mm per la direzione cc ; per i reperi fiduciali , lerrore sistematico e casuale medio sono stati 0 , 61 , 5 mm per la direzione ll , 0 , 512 , 45 mm per la direzione ap e 0 , 252 , 51 mm per la direzione cc . 
stato creato un diagramma di distribuzione di tutte le misure ottenute dopo il riposizionamento del lettino in funzione degli scostamenti registrati mediante i reperi fiduciali ; lambito di confidenza della distribuzione degli spostamenti si trova entro i 5 mm per la direzione ll , entro i 6 mm per la direzione cc ed entro i 7 mm per la direzione ap . 
lerrore sistematico e lerrore casuale totale sono stati utilizzati per generare margini per ottenere il ptv nei pazienti trattati convenzionalmente ( 7 mm per la direzione ll ; 9 mm sia per la direzione ap che per la direzione cc )  . 
il monitoraggio della posizione della prostata mediante reperi fiduciali ed immagini portali in grado di ridurre la dispersione degli scostamenti rispetto allatteso , contribuendo in maniera significativa al miglioramento della precisione balistica della radioterapia . parole chiave radioterapia guidata dalle immagini tumore della prostata reperi fiduciali semi doro margini di trattamento introduction introduzione modern radiotherapy techniques , with the implementation of three - dimensional conformal radiotherapy ( 3d - crt ) and / or intensity - modulated radiation therapy ( imrt ) , have achieved a substantial improvement in tumour control rates by allowing escalation of the total dose to the target volume while sparing surrounding normal tissues [ 1 ]  . 
in this context , it becomes crucial to obtain a reliable correspondence between the planned dose distribution and the in vivo dose le moderne tecniche radioterapiche , con limplementazione della radioterapia conformazionale 3d ( 3dcrt ) e della radioterapia ad intensit modulata ( imrt ) , hanno garantito un miglioramento sostanziale dei tassi di controllo tumorale mediante la possibilit di erogare dosi pi alte al volume bersaglio , risparmiando allo stesso tempo i tessuti sani circostanti [ 1 ]  . 
in questo senso , diventa cruciale ottenere una corrispondenza precisa tra la distribuzione di dose prevista radiol med ( 2012 ) 117 : 10571070 1059 delivery [ 2 ]  . 
hence , as correct targeting of a tumoural lesion might be affected by changes in patient position and target - volume shape , as well as by internal - organ motion , it is necessary to precisely track tumour position in order to minimise these geometrical uncertainties [ 3 ]  . 
it is known that prostate gland position might be affected by interfraction displacements relative to pelvic bone anatomy due to rectal and bladder filling status and repositioning errors [ 4 , 5 ]  . 
in order to achieve the highest ballistic precision during prostate irradiation , several image - guided radiation therapy ( igrt ) techniques have been employed , such as implanted intraprostatic fiducial markers visualised by either megavoltage or kilovoltage computed tomography ( ct ) systems , transabdominal ultrasound ( us ) , several types of accelerators ( cone - beam ct in conjunction with conventional accelerators ; megavoltage ct with tomotherapy ) and electromagnetic markers used as implanted transponders [ 1 ]  . 
using three fiducial markers ( gold seeds ) implanted within the prostatic gland , we conducted this prospective evaluation of prostate cancer patients treated with image - guided 3d - crt at our institution to quantify daily target displacements and to generate specific margins around the clinical target volume ( ctv ) to create an appropriate planned target volume ( ptv )  . 
 materials and methods patient cohort and marker implantation between april and december 2009 , ten patients affected with histologically confirmed localised prostate cancer were transrectally implanted with three radio - opaque markers ( specifically , cylindrical gold seeds 1.2 mm diameter and 3 mm long ) using a 17 - gauge needle ( northwest medical physics equipment , lynnwood , wa , unites states )  . 
we included intermediate - risk patients [ american joint committee on cancer and union for international cancer control ( ajcc - uicc ) , ct2b - ct2cn0m0 ; gleason score , 7 ; initial prostate - specific antigen ( psa ) , 1020 ng / ml ] according to the damico classification [ 6 ]  . ct acquisition each patient underwent a ct scan for planning purposes between 1 and 2 weeks after gold - seed implantation to allow any prostatic or periprostatic swelling to settle ; moreover , to e quella erogata in vivo [ 2 ]  . 
pertanto , in considerazione del fatto che la corretta individuazione di una lesione tumorale pu dipendere dalle variazioni del posizionamento del paziente e della forma della lesione bersaglio e dal movimento dorgano , risulta necessario valutare in maniera precisa lesatta collocazione del tumore per minimizzare le incertezze geometriche [ 3 ]  . 
noto che la posizione della ghiandola prostatica pu essere influenzata da scostamenti inter - frazione rispetto alle strutture ossee pelviche , in seguito al riempimento rettale , a quello vescicale ed agli errori di riposizionamento [ 4 , 5 ]  . 
per poter ottenere unalta precisione balistica durante la radioterapia prostatica , diverse modalit di radioterapia guidata dalle immagini ( igrt ) sono state implementate in anni recenti : tra queste i reperi fiduciali intraprostatici visualizzati sia con tomografia computerizzata ( tc ) in megavoltaggio che in chilovoltaggio , sistemi ecografici per via trans - addominale , alcuni sistemi di igrt associati agli acceleratori ( cone - beam tc associata ad acceleratori tradizionali ; mvct associata alla tomoterapia ) , reperi elettromagnetici utilizzati come trasduttori impiantati [ 1 ]  . 
abbiamo intrapreso una valutazione prospettica di pazienti affetti da carcinoma prostatico trattati con 3dcrt e monitorati con igrt presso listituto di radioterapia delluniversit di torino , mediante limpianto di 3 reperi fiduciali intraprostatici , allo scopo di quantificare gli scostamenti giornalieri del volume bersaglio e di generare margini specifici attorno al volume bersaglio clinico ( ctv ) per creare un volume bersaglio di pianificazione ( ptv ) appropriato . materiali e metodi coorte dei pazienti ed impianto dei reperi fiduciali tra aprile e dicembre 2009 , 10 pazienti con diagnosi istologica di carcinoma prostatico sono stati sottoposti ad impianto per via trans - rettale di tre reperi radio - opachi ( semi doro cilindrici con diametro di 1 , 2 mm e lunghezza di 3 mm ) mediante un ago di 17 gauge ( northwest medical physics equipment , lynnwood , wa , usa )  . 
ogni repere stato inserito dallo specialista urologo sotto anestesia locale , utilizzando un approccio trans - rettale sotto guida ecografica , rispettivamente alla base , al centro ed a livello dellapice della prostata . 
patients were placed in supine position with both an index - shaped knee rest and ankle support ( civco medical solutions , kalona , ia , usa ) to prevent hip rotation . 
ctv comprised the entire prostate gland and proximal one third of the seminal vesicles , whereas ptv was generated by adding a 5 - mm isotropic margin to the ctv . 
3.0 software ; two orthogonal digitally reconstructed radiographs ( drrs ) were subsequently generated from the anterior and lateral beams - eye view and considered as a reference for comparison with portal images produced at each treatment session . 
 the nominal dose prescribed at the isocentre was 70.2 gy given in 26 fractions ( daily fraction 2.7 gy ) that , assuming an / ratio for prostate cancer ranging between 1.5 gy and 3 gy , might correspond to a biologically equivalent dose in 2 gy fractions ( eqd2 ) between 80 gy and 84 gy , according to the formalism of the linear quadratic model [ 7 ]  . image - guidance procedures all patients were placed on the treatment couch with the same immobilisation devices used during the planning ct scan . 
the gold seeds were manually localised by a radiation oncologist on both the drrs and the epis , generating a so - called centre of mass , which was used as a surrogate for prostate position . 
subsequently , comparison between the position of the gold seeds on epis and reference images was carried out , and a set of tc di centratura tutti i pazienti sono stati sottoposti a tc di centratura tra 1 e 2 settimane dallimpianto dei semi doro per permettere il riassorbimento delledema post - procedura . 
al fine di garantire la riproducibilit quotidiana delle condizioni del retto , della vescica e del volume bersaglio , i pazienti sono stati istruiti ad introdurre 500 ml di acqua 1 ora prima della tc di centratura ( come prima di ogni frazione di trattamento ) e ad effettuare un clistere associato a dieta priva di scorie a partire da 3 giorni prima della centratura . 
i pazienti sono stati posizionati supini su di un presidio di immobilizzazione per le ginocchia e le caviglie ( civco , medical solutions , kalona , ia , usa ) , al fine di prevenire la rotazione del bacino . 
3.0 ( nucletron , veendhal , paesi bassi ) a livello della ghiandola prostatica e sono state tatuate le sue proiezioni sulla cute dei pazienti sotto guida laser . volumi di trattamento e frazionamento il contornamento stato effettuato mediante il programma oncentra masterplan v . 
3.0 ; il ctv comprendeva lintera ghiandola prostatica ed il terzo prossimale delle vescichette seminali ; il ptv stato successivamente creato mediante laggiunta di un margine isotropico di 5 mm attorno al ctv . 
 stato creato un piano di trattamento per ogni paziente mediante 5 campi co - planari ( angoli di trattamento : 0 , 90 , 45 , 270 , 315 ) utilizzando il programma oncentra masterplan v . 
3.0 ; 2 radiografie ortogonali digitalmente ricostruite ( drrs ) sono state ottenute secondo angolo anteriore e laterale per fungere da confronto con le immagini portali generate ad ogni sessione di trattamento . 
la dose nominale di prescrizione allisocentro stata di 70 , 2 gy in 26 frazioni ( dose giornaliera : 2 , 7 gy ) che , assumendo un valore del rapporto / per il tumore della prostata compreso tra 1 , 5 gy e 3 gy , corrisponde ad un equivalente biologico di dose in frazioni da 2 gy ( eqd2 ) compreso tra 80 e 84 gy , in accordo con il formalismo del modello lineare quadratico [ 7 ]  . procedure di igrt tutti i pazienti sono stati immobilizzati sul lettino di trattamento con gli stessi presidi di immobilizzazione utilizzati duradiol med ( 2012 ) 117 : 10571070 1061 rante la tc di centratura . 
i semi doro sono stati individuati manualmente da un radioterapista oncologo sia sulle drrs che sulle immagini portali , generando , in tal modo un cosiddetto centro di massa che stato utilizzato come surrogato della posizione della prostata . 
in seguito , prima di ogni seduta , un confronto tra la posizione dei semi doro sulle immagini portali e quella sulle immagini di riferimento stato effettuato con la successiva estrapolazione di spostamenti generati e relative correzioni nelle direzioni latero - laterale ( ll ) , antero - posteriore ( ap ) e cranio - caudale ( cc )  . 
si , poi , provveduto a delineare le strutture scheletriche pelviche , come il margine superiore delle ossa pubiche , la cresta iliaca ed ischiatica e la sinfisi pubica sulle drrs con una successiva co - registrazione con le immagini portali ; gli scostamenti delle strutture ossee sono stati misurati utilizzando il programma dcm - view v.1.19.8 ( tecnologie avanzate , torino , italia )  . 
il posizionamento giornaliero basato sui reperi cutanei stato registrato , ottenendo 260 scostamenti per le direzioni ll , ap e cc ; successivamente , 120 misure sono state registrate dopo lo spostamento del lettino di trattamento , ove il valore soglia di 3 mm fosse stato raggiunto in almeno 1 delle 3 direzioni dello spazio . 
 calcolo dei margini per il ptv e valutazione dosimetrica gli errori sistematico e casuale sono stati calcolati utilizzando gli scostamenti registrati prima ( basandosi sui reperi cutanei ) e dopo i movimenti ( basandosi sui reperi fiduciali ) del lettino di trattamento , in accordo con il metodo descritto da van herk et al [ 8 ]  . 
nessuna dose aggiuntiva stata erogata al paziente durante tale procedura , in quanto la singola esposizione necessaria per la visualizzazione stata ottenuta direttamente dal campo di trattamento . extrapolated lateral - lateral ( ll ) , anterior - posterior ( ap ) and cranial - caudal ( cc ) shift corrections was calculated and recorded before each treatment session . 
a 3 - mm threshold was considered in repositioning the patient by changing the couch coordinates , with shifts taking place only for displacements > 3 mat the end of the repositioning procedures , another two orthogonal images were acquired to verify the accuracy of the couch movements . 
hence , pelvic skeletal segments such as the superior border of the pubic bones , the ilialischiatic line and the pubic symphysis were identified on drrs and then coregistered with epis ; bone displacement was measured using dcm - view v . 
conversely , 120 measurements were recorded after the couch had been moved if the action level of 3 mm was reached in at least one of the three directions . 1062 radiol med ( 2012 ) 117 : 10571070 calculation of ptv margins and dosimetric evaluation systematic and random errors were calculated using the shift data obtained before ( based on skin marks ) and after ( based on fiducial markers ) couch movements , according to the method described by van herk et al . 
for each patient , systematic error was calculated as the mean of the displacement distribution , whereas random error is the standard deviation ( sd ) of the shift distribution . 
the total systematic error ( ) is calculated as the sd of all individual systematic errors , whereas overall random error ( ) is represented by the quadratic average of all random errors . 
oars considered for dose constraints were bladder , rectum ( d30 and d50 ) and femoral heads ( mean dose )  . written informed consent was obtained from each patient for the implantation of seeds and for the fractionation schedule . 
the study was approved by the institutional review board . results considering all igrt procedures of the ten study patients , 260 daily measurements were obtained and analysed ( table 1 )  . 
the systematic and random errors for each direction were calculated both as measured according to gold - seed displacement before any couch movement ( based on skin marks ) and after correction of couch position , as suggested by radio - opaque markers ( based on fiducial markers )  . 
moreover , results of a paired students t test between values obtained before and after couch correction revealed a statistically significant difference between the considered parameters in each direcquadratica di tutti gli errori causali ; i margini per il ptv corrispondenti sono stati calcolati in accordo con la formula seguente [ 8 ] : 2 , 5 + 0 , 73 mm sono stati derivati margini per 2 specifiche situazioni cliniche , ovvero sia per trattamenti standard senza procedure igrt basandosi sui reperi cutanei che per trattamenti con localizzazione igrt mediante immagini portali basandosi sui reperi fiduciali intraprostatici . 
ogni piano di trattamento a schedula ipofrazionata ( 2 , 7 gy giornalieri ) generato con margini isotropici di 5 mm per lespansione del ptv stato confrontato con un relativo piano di cura ottenuto su ptv generati con margini di espansione standard , precedentemente utilizzati presso il nostro istituto ( 10 mm per la direzione ll ; 12 mm per la direzione cc ; 10 mm per la direzione anteriore ed 8 mm per quella posteriore ) e con il frazionamento convenzionale . 
lo studio stato approvato dal comitato etico aziendale . risultati utilizzando tutte le procedure igrt ottenute dalla coorte di 10 pazienti , sono stati generati ed analizzati 260 spostamenti ( tabella 1 )  . 
lerrore sistematico e casuale sono stati calcolati sia in accordo con gli scostamenti misurati tramite i semi doro prima di qualsiasi spostamento del lettino di trattamento ( basandosi sui reperi cutanei ) sia dopo gli spostamenti effettuati in accordo con quanto indicato dai reperi fiduciali ( basandosi sugli stessi )  . 
per i reperi cutanei , lerrore sistematico e casuale medio sono stati 0 , 122 , 94 mm per la direzione ll , 1 , 043 , 37 mm per la direzione ap , - 1 , 142 , 71 mm per la direzione cc . 
al contrario , per i reperi fiduciali , lerrore sistematico e casuale medio sono stati 0 , 61 , 5 mm per la direzione ll , 0 , 512 , 45 mm per la direzione ap e - 0 , 252 , 51 per la direzione cc . 
inoltre , i risultati del confronto effettuato con il test t di student tra i valori ottenuti prima e dopo leffettuazione della correzione della posizione del lettino di trattamento hanno rivelato una differenza statisticamente significativa tra i parametri considerati in ogni direzione dello spazio ( p < 0 , 01 per ll , ap e cc )  . 
stato generato un diagramma di dispersione radiol med ( 2012 ) 117 : 10571070 1063 table 1 mean value and standard deviation of the distribution of displacements of each patient , along the three considered directions before and after on - line correction patient no . 
 shift distribution obtained after comparison with drrs was represented by plotting the ap direction with the cc direction ( sagittal plane ) , the ll direction with the cc direction ( coronal plane ) and the ll direction with the ap direction ( axial plane )  . 
as shown in figure 2 , the confidence range of shift distributions lies within 5 mm for the ll direction and 7 mm for the ap direction , whereas the cc direction stands roughly in the middle . 
 la distribuzione degli spostamenti ottenuti dopo confronto con le drrs rappresentata in un diagramma utilizzando come variabili le direzioni ap e cc ( piano sagittale ) , quelle ll e cc ( piano coronale ) e quelle ll ed ap ( piano assiale )  . 
come mostrato nella figura 2 , lintervallo di confidenza della distribuzione degli spostamenti rimane entro i 5 mm per la direzione ll , entro i 7 mm per la direzione ap , mentre la direzione cc si posiziona circa a met . 
in particolare , lerrore sistematico totale ( ) stato calcolato per il posizionamento risultando in 2 , 4 mm per la direzione ll , 2 , 08 mm per la direzione ap e 1 , 7 mm per la direzione cc ; per il movimento dorgano , ( ) risultato essere 1 , 35 radiol med ( 2012 ) 117 : 10571070 1064 table 2 systematic ( ) and random ( ) components for setup and organ motion derived from analysis of the sample of considered patients setup ( mm ) setup ( mm ) organ m . 
in particular , calculated for the setup was 2.40 mm for the ll direction , 2.08 mm for the ap direction and 1.7 mm for the cc direction ; for organ motion , it was 1.35 mm for the ll direction , 1.92 mm for the ap direction and 2.25 mm for the cc direction . 
in addition , calculated for both setup and organ motion was 3.00 mm for the ll direction , 2.07 mm for the ap direction and 1.79 mm for the cc direction ; for organ motion , it was 1.13 mm for the ll direction , 2.68 mm for the ap direction and 3.63 mm for the cc direction . 
systematic and random components obtained were subsequently used to calculate ( according to van herk [ 8 ] ) appropriate margins around the contoured ctv to guarantee a ptv with consistently adequate target coverage for patients receiving conventional treatment ( no igrt procedures )  . 
another issue addressed in data analysis was comparison between biologically equivalent doses received by critical structures around the target volume , both with standard margins and conventional fractionation and with reduced ( based on the gold seeds ) margins and hypofractionation ; in particular , dosimetric parameters were extrapolated from dose volume histograms ( dvhs ) regarding dose to the rectum ( 50% and 30% of the entire volume ; i.e. , d30 and d50 ) , bladder ( 30% of the volume ; d30 ) and femoral heads ( mean dose )  . 
 the original values of dose received by oars in the hypofractionated scheme were corrected for / ratio to be compared with values obtained for standard fractionation ( 2 gy per fraction ) ; results are shown in table 3 for each patient . 
values obtained for the hypofractionated scheme ( 2.7 gy / fraction ) using 5 - mm expansion from ctv to ptv were compared with values obtained with the conventional schedule using traditional margins with no igrt procedure . 
inoltre , lerrore casuale totale ( ) stato calcolato sia per il posizionamento che per il movimento dorgano risultando in 3 , 00 mm per la direzione ll , 2 , 07 mm per la direzione ap , 1 , 79 mm per la direzione cc ( posizionamento ) e 1 , 13 mm per la direzione ll , 2 , 68 mm per la direzione ap e 3 , 63 mm per la direzione cc ( movimento dorgano )  . 
pertanto , le componenti cos ottenute sistematiche e casuali sono state utilizzate per calcolare ( in accordo con van herk ) margini appropriati attorno al ctv per ottenere un ptv che garantisse un adeguata copertura del volume bersaglio per i trattamenti standard ( senza procedure di igrt )  . 
un altro aspetto indagato dalla presente analisi stato il confronto tra gli equivalenti biologici di dose ricevuti dagli oars attorno al volume bersaglio sia con margini standard e frazionamento convenzionale che con margini ridotti ( basati sui reperi fiduciali ) ed una schedula ipofrazionata ; in particolare , i parametri dosimetrici sono stati estrapolati dagli istogrammi dose - volume ( dvhs ) a riguardo del retto ( 50% e 30% del volume rettale ovvero d30 e d50 ) , della vescica ( 30% del volume vescicale ovvero d30 ) e delle teste femorali ( dose media )  . 
i valori nominali delle dosi ricevute dagli oars tramite la schedula ipofrazionata sono stati corretti in funzione del rapporto / per essere confrontati con quelli del frazionamento convenzionale ( 2 gy per frazione ) ; i risultati sono evidenziati nella tabella 3 . 
i valori ottenuti per la schedula ipofrazionata ( 2 , 7 gy per frazione ) con margine isotropico di espansione di 5 mm tra ctv e ptv sono confrontati con i valori ottenuti con una schedula convenzionale e margini tradizionali senza procedure di igrt . 
il valore 0 , ovvero il punto dove il valore della dose ottenuta si sovrappone con quello del vincolo dosimetrico per uno radiol med ( 2012 ) 117 : 10571070 1065 table 3 comparison of conventional fractionation of 2 gy / fraction using standard margins and hypofractionated radiotherapy schedule with 2.7 gy / fraction and 5 - mm margins ( eqd2gy ) in terms of dose to critical structures . 
in particular , we analysed dose to 30% of the volume of both rectum and bladder , as well as 50% of the volume of the rectum and mean dose to femoral heads patient no . 
confronto tra un frazionamento convenzionale ( 2 gy / die ) con margini standard ed una schedula ipofrazionata ( eqd , 2 , 7 gy / die ) con margini di 5 mm in termini di dose ricevuta dagli organi a rischio . 
in particolare stata analizzata la dose ricevuta dal 30% del volume rettale e vescicale , quella ricevuta dal 50% del volume rettale e la dose media alle teste femorali paziente no . 
a mean value of about 5% with a consistent number of negative points is shown by the distribution of conventional fractionation values . specifico organo , rappresenta la massima deviazione pianificata accettabile . 
la distribuzione della soluzione di classe in termini di eqd2 mostra soltanto un valore negativo ed un valore medio di una differenza percentuale del 38% in termini positivi tra i valori considerati del dvh ed i vincoli dosimetrici . 
 discussione discussion recent years have been significantly stimulating in the field of radiation oncology , with substantial improvements in cancer treatment results in terms of both tumour control and avoidance of radiation - induced toxicity to normal tissue . 
specifically , new developments in target definition , treatment planning and radiation delivery have resulted in high dose gradients between the target volume and the surgli ultimi anni sono stati significativamente stimolanti nel campo della radioterapia oncologica , con miglioramenti sostanziali nei risultati dei trattamenti oncologici sia in termini di controllo tumorale che di riduzione della tossicit attinica . 
 nello specifico , nuovi sviluppi nella definizione del volume bersaglio , nella pianificazione e nell erogazione del trattamento radiante sono stati in grado di offrire lopportunit di generare elevati gradienti di dose tra il volume bersaglio e 1066 radiol med ( 2012 ) 117 : 10571070 fig . 
ci particolarmente evidente nel contesto del carcinoma prostatico dove una sostanziale riduzione delle dimensione dei volumi di trattamento stata ottenuta attraverso le nuove tecnologie , con la necessit susseguente di caratterizzare precisamente la posizione e la forma della ghiandola prostatica e degli organi a rischio [ 9 ]  . 
 [ 10 ] applicano un modello adattativo per determinare le variazioni ed i margini specifici per ogni paziente ed eliminare le differenze sistematiche in termini di posizione [ 10 ]  . 
in tempi recenti , si giunti ad un accordo generale sul fatto che le variazioni posizionali della ghiandola prostatica possono essere sostanziali , raggruppando insieme sia le incertezze dovute alle variazioni della forma dellorgano che quelle dovute al suo movimento , gli errori di posizionamento e la geometria dei fasci di irradiazione [ 11 , 12 ]  . 
 [ 11 ] hanno esplorato approfonditamente questa problematica , analizzando un intero pacchetto di dati derivanti dalle immagini portali quotidiane , da sessioni ripetute di simulazione , e da scansioni tc effettuate durante il trattamento [ 11 ]  . 
nello specifico , la deviazione standard ( sd ) dellerrore di posizionamento ( la componente casuale che tiene conto delle deviazioni tra le differenti frazioni nel corso di un trattamento ) varia tra 1 e 4 mm ; ci sostanzialmente in accordo con i nostri dati come mostrato nella tabella 1 . 
this is particularly evident in the setting of prostate cancer , where a substantial downsizing of radiation fields has been obtained thanks to new technology , leading to a need for consistent characterisation of both location and shape of the prostate gland and oars [ 9 ]  . 
there is now general agreement regarding the fact that positional variations of the prostate gland can be substantial , combinradiol med ( 2012 ) 117 : 10571070 1067 ing uncertainties deriving from changes in organ shape and motion , setup errors and beam geometry [ 11 , 12 ]  . 
as far as setup uncertainties are concerned , this issue has been extensively explored by hurkmans et al . , who analysed a complete data set obtained from daily portal images , repeated simulation sessions and ct scans during radiation [ 11 ]  . 
specifically , the sd for setup error ( random component describing deviations between different fractions over a treatment course ) ranges between 1 mm and 4 mm ; this is substantially in accordance with our results , as shown in table 1 . 
this is mainly confirmed by our data , as shown in table 1 , and by the comparison of margins calculated by deriving the total systematic and random errors according to the method proposed by van herk et al . 
 [ 8 ] , as shown in table 2 ( for conventional treatments with no image - guidance ) and the scatter plot of displacement obtained after repositioning based on the gold seeds in the three spatial planes ( sagittal , coronal and axial ) , as described in figure 2 . 
as several investigators have shown that breathing effects are negligible for patients in the supine position , we might assume that prostate displacements in our study were mainly due to rectum activity , bladder filling , prostatic bed motion and clenching of pelvic floor muscles [ 15 , 16 ]  . 
it has been suggested that patients should be treated with empty bladder to eliminate uncertainty in prostate position caused by variation in bladder filling ; however , there is an obvious advantage of using a full bladder to reduce normal tissue toxicity by displacing the anterior bladder wall and small bowel from the high - dose regions . 
observed that bladder distension displaced the back border of the prostate up to 8 mm ( median 2 mm ) posthis fact is explained by the contraction of pelvic teriorly ; floor musculature due to full bladder [ 16 ]  . 
demonstrated that rectal distension ( obtained with 60 cc of contrast material ) shifted the prostate by a mean of 5 mm ( range 020 mm ) in the ap direction [ 17 ]  . 
ci confermato dai nostri dati , come mostrato nella tabella 1 e come si evince dal confronto con i margini calcolati derivando lerrore sistematico totale e casuale secondo il metodo proposto da van herk et al . 
 [ 8 ] , come si pu osservare nella tabella 2 ( per i trattamenti standard senza procedure di igrt ) e dal diagramma di dispersione degli scostamenti sui tre piani dello spazio ( sagittale , coronale , assiale ) , ottenuti dopo il riposizionamento basato sui reperi fiduciali , come descritto nella figura 2 [ 8 ]  . 
poich alcuni studi hanno dimostrato che gli effetti del respiro sono trascurabili per i pazienti trattati in posizione supina per il tumore della prostata , possibile ipotizzare che gli scostamenti della ghiandola nel nostro studio siano principalmente dovuti all attivit del retto , al grado di replezione della vescica , al movimento della loggia prostatica dovuto allo stato di contrazione dei muscoli del pavimento pelvico [ 15 , 16 ]  . 
pertanto , tutti i pazienti inclusi nel nostro studio hanno effettuato una preparazione atta ad avere una vescica ripiena durante la tc di centratura e durante tute le frazioni della radioterapia . 
alcuni autori hanno suggerito di trattare i pazienti a vescica vuota per eliminare le incertezze della posizione della prostata dovute alla variabilit del grado di riempimento vescicale ; tuttavia , esiste un vantaggio palese nellirradiazione a vescica ripiena in termini di riduzione della tossicit dei tessuti sani tramite lallontanamento della parete vescicale anteriore e del piccolo intestino dalle regioni ad alta dose . 
 [ 16 ] hanno osservato che la distensione vescicale sposta il margine posteriore della prostata stessa anche di 8 mm ( in media 2 mm ) in direzione posteriore , in seguito alla contrazione dei muscoli del pavimento pelvico [ 16 ]  . 
 [ 17 ] hanno osservato che la distensione rettale ( ottenuta con 60 cc di liquido di contrasto ) sposta la ghiandola prostatica in direzione ap in media di 5 mm ( intervallo 020 mm ) [ 17 ]  . 
stato evidenziato un movimento dorgano maggiore ( mediamente 4 , 5 mm ; intervallo 016 mm ) in direzione ap , apparentemente correlato con il grado di riempimento rettale e vescicale . 
nello specifico della nostra coorte di pazienti , suggeriamo una spiegazione per la quale ci pu essere dovuto alla contrazione del pavimen1068 radiol med ( 2012 ) 117 : 10571070 et al . 
if a margin ranging between 7 and 9 mm , depending on the chosen axis , is mandatory to ensure a 95% probability that a point within the ctv might be enclosed by the ptv , this margin decreases to 57 mm if gold - seed repositioning is employed . 
as it has been demonstrated that the use of a 15 - mm margin around the ctv might cause significant rectal bleeding if doses > 74 gy are delivered , it is necessary to shrink irradiated volumes by reducing the margins in order to spare normal tissues [ 21 , 22 ]  . 
this is evident in table 3 , which compares doses received by oars with conventional fractionation with no image - guidance protocols and the dose received with hypofractionation and gold - seed tracking . 
our data may suggest that the margins currently used in our institute to create a specific ptv might be considered generous ; margins of 7 mm , 9 mm and 9 mm in ll , ap and cc , respectively , may be used if no daily localisation is employed . 
margin reduction might also help minimise the volume of rectal wall and penile bulb included in the high - dose regions , as there is evidence that , by restricting these volumes , one could have beneficial effects on late rectal toxicity and erectile function [ 24 , 25 ]  . 
estimated that a margin reduction from 1 cm to 0.5 cm without daily localisation would result in a significant increase in the deviation of treatment dose from the planned dose and could result in a reduction of the prescribed dose of approximately 10 gy [ 26 ]  . 
the most recent radiation therapy oncology group ( rtog ) protocols for prostate cancer radiation therapy define the ptv as the ctv with an expansion margin of 510 mthus , our data seems to be in agreement with that to pelvico a seguito della scomodit di effettuare il trattamento a vescica piena . 
se un margine compreso tra 7 e 9 mm , a seconda della direzione in esame , necessario per assicurare il 95% di probabilit che un punto incluso nel ctv sia compreso nel ptv , tale margine scende a 57 mm con limpiego dei reperi fiduciali . 
poich noto che un margine di 15 mm attorno al volume bersaglio clinico pu causare sanguinamenti rettali significativi , per dosi superiori a 74 gy , risulta evidente limportanza di ridurre i volumi di trattamento , diminuendo i margini , al fine di risparmiare i tessuti sani [ 21 , 22 ]  . 
ci evidente nella tabella 3 , dove possibile osservare un confronto tra la dose ricevuta dagli organi a rischio con un frazionamento convenzionale , senza lutilizzo di procedure di igrt e la dose ricevuta dagli stessi organi con una schedula ipofrazionata e lutilizzo dei semi doro . 
i dati di questo studio suggeriscono che i margini comunemente utilizzati presso il nostro istituto per generare il ptv sono generosi ; probabilmente margini di 7 mm ( ll ) e 9 mm ( ap e cc ) sarebbero sufficienti per i trattamento senza igrt . 
 [ 23 ] raccomandano margini corrispondenti a 1 , 5sd per coprire il ctv con il 93% della dose di prescrizione , risultando in margini di 6 , 6 mm , 6 , 5 mm e 8 , 7 mm rispettivamente [ 23 ]  . 
altri studi , utilizzanti varie tecniche di igrt , raccomandano margini compresi tra 5 , 39 , 2 mm , 7 , 014 , 6 mm e 9 , 211 , 0 mm nelle direzioni ll , cc ed ap rispettivamente [ 12 ]  . 
la riduzione dei margini pu , altres , essere di aiuto per ridurre la porzione di parete rettale e di bulbo penieno inclusa nelle regioni ad alta dose , riducendo in tal modo la tossicit tardiva a carico di queste strutture [ 24 , 25 ]  . 
 [ 26 ] hanno stimato che una riduzione dei margini compresa tra 0 , 5 e 1 cm senza conseguente utilizzo di procedure di igrt quotidiane pu risultare in un significativo aumento della deviazione dalla dose pianificata di circa 10 gy [ 26 ]  . 
 monitorare la variabilit della posizione della ghiandola prostatica mediante reperi fiduciali intra - prostatici ed immagini portali una metodica fattibile ed efficace che in grado di aumentare la precisione balistica della radioteraradiol med ( 2012 ) 117 : 10571070 1069 definition , as our derived margins result in 7 mm in ll and 9 mm in ap and cc directions . tracking prostate position variability with intraprostatic fiducial markers and electronic portal imaging seems to be feasible and effective , with the possibility of increasing the ballistic precision of radiation therapy in terms of target coverage and normal tissue sparing . 
as the entire procedure is time consuming , we suggest reserving it for specific clinical settings in which igrt is employed and there is a need to precisely locate the target volume , given the high dose gradients generated . 
with the implementation of new - generation linear accelerators and the possibility of using on - board imaging ( cone - beam ct , megavoltage ct , us , for example ) , simpler and less invasive methods for igrt in prostate cancer are available . 
nel nostro istituto non utilizziamo come standard terapeutico questa modalit di igrt ; poich lintera procedura pu risultare dispendiosa in termini di tempo , suggeriamo di riservare tale approccio a contesti clinici selezionati in cui viene utilizzata la imrt che , generando alti gradienti di dose , necessita di una precisa localizzazione della ghiandola prostatica . 
con limplementazione degli acceleratori di nuova generazione e la possibilit di utilizzare sistemi di igrt associati allo stesso acceleratore ( tc cone beam , mvtc , ultrasuoni , per esempio ) , metodiche pi semplici e meno invasive di monitoraggio del volume bersaglio sono ora disponibili . 
thus , daily localisation with implanted fiducial markers is useful for margin shrinkage , but long - term follow - up and a more robust sample size are needed to evaluate the clinical impact of this approach on radiation - induced toxicity and clinical outcome . mediante lutilizzo di reperi fiduciali intra - prostatici , stato possibile migliorare la localizzazione della ghiandola prostatica durante il trattamento radiante . 
infine , la localizzazione giornaliera del volume bersaglio mediante semi doro utile per la riduzione dei margini del ptv ; tuttavia , valutazioni cliniche a lungo termine ed un campione di pazienti allargato sono ancora necessari per valutare limpatto clinico di tale approccio sugli effetti attinici tardivi e sul risultato clinico . 
rossi1 1sezione di diagnostica per immagini , dipartimento di scienze cliniche , padiglione barbieri , azienda ospedaliero - universitaria di parma , universit degli studi di parma , via gramsci 14 , 43100 parma , italy 2sezione di malattie dellapparato respiratorio , dipartimento di scienze cliniche , azienda ospedaliero - universitaria di parma , universit degli studi di parma , parma , italy 3dipartimento di diagnostica per immagini , azienda ospedaliero - universitaria di parma , parma , italy 4sezione di lungodegenza critica , dipartimento di scienze cliniche , azienda ospedaliero - universitaria di parma , universit degli studi di parma , parma , italy 5dipartimento clinico di scienze radiologiche ed istocitopatologiche , radiologia cardiotoracovascolare , policlinico s . 
sverzellati , e - mail : nicola.sverzellati@unipr.it received : 3 february 2011 / accepted : 7 april 2011 / published online : 14 may 2012 springer - verlag 2012 abstract purpose . 
each follow - up hrct examination was assessed as stable , improved ( when the extent of hrct findings was reduced compared with baseline ) and worsened ( when the extent of hrct findings was increased and / or when hrct pattern had become fibrotic compared with baseline )  . 
la malattia stata valutata come : stabile , migliorata ( per riduzione in estensione delle alterazioni ) e peggiorata ( per aumento in estensione delle alterazioni e / o evoluzione verso un pattern fibrotico )  . 
allesame hrct di follow - up ( mediana 33 mesi , intervallo 1563 mesi ) , la malattia apparsa peggiorata in 8 / 14 pazienti ( 57% ) , mentre migliorata in 3 / 14 ( 21% ) ed invariata in 3 / 14 ( 21% )  . 
 parole chiave sarcoidosi follow - up hrct capacit vitale forzata introduction introduzione sarcoidosis is a systemic disease characterised by the development of noncaseating granulomatous inflammatory infiltrations that may affect any organ , with involvement of the lung and intrathoracic lymph nodes in 90% of cases . 
in the lung , the disease infiltrates into the perilymphatic interstitium and is detected at high - resolution computed tomography ( hrct ) , with different morphological patterns that may develop into fibrosis in 2025% of cases . 
the development of pulmonary fibrosis is generally associated with a restrictive functional defect and increased morbidity and mortality rates [ 1 , 2 ]  . pulmonary function testing ( pft ) has always represented the standard of reference for monitoring the course of disease over time [ 35 ] , even though it is unable to provide specific information about morphological changes developing in the sarcoidotic lung . 
according to the international guidelines , only chest radiography has a role in diagnosing and staging sarcoidosis and may be usefully combined with pft in monitoring the course of the disease [ 2 ]  . 
studies demonstrate that serial chest radiography and pft has a sensitivity comparable with that of bronchoalveolar lavage lymphocyte counts , serum angiotensin - converting enzyme measurement and gallium scan in monitoring sarcoidosis activity [ 6 ]  . 
however , hrct provides a new diagnostic standard : in fact , it has been demonstrated that , compared with radiography , it has higher sensitivity and specificity in characterising lesion pattern and extent , both at baseline and at follow - up [ 3 , 711 ]  . 
a livello polmonare , la malattia infiltra linterstizio perilinfatico manifestando si alla tomografia computerizzata ad alta risoluzione ( high - resolution computed tomography , hrct ) con diversi pattern morfologici che nel 20%25 % dei casi possono evolvere in fibrosi . 
la comparsa di fibrosi polmonare generalmente associata ad unalterazione funzionale di tipo restrittivo ed aumento della morbilit e della mortalit [ 1 , 2 ]  . le prove di funzionalit respiratoria ( pulmonary function test , pft ) rappresentano da sempre lesame di riferimento per monitorare la malattia nel tempo [ 35 ] , senza per fornire informazioni specifiche sulle modificazioni morfologiche a cui la sarcoidosi pu andare incontro . 
secondo le linee guida internazionali , solo lesame radiografico del torace ha un ruolo nella diagnosi e nella stadiazione della sarcoidosi e pu essere utilmente associato alle pft nel monitorare il decorso della malattia [ 2 ]  . 
studi precedenti hanno dimostrato che luso seriale dellesame radiografico del torace e delle pft ha un livello di sensibilit comparabile a quello del conteggio dei linfociti su lavaggio broncoalveolare , dei livelli dellenzima convertitore dellangiotensina nel siero e dei risultati della scintigrafia con gallio nel monitorare lattivit della sarcoidosi [ 6 ]  . 
tuttavia la hrct ha permesso il raggiungimento di nuovi standard diagnostici : infatti ormai dimostrato come presenti , rispetto alla radiografia , maggior sensibilit e specificit nel caratterizzare il pattern e lestensione delle lesioni sia alla presentazione che nellevoluzione della malattia [ 3 , 711 ]  . 
lo scopo del nostro studio stato quello di valutare lutilit clinica della hrct nel monitorare levoluzione della sarcoidosi , mettendo a confronto i cambiamenti della malattia alla hrct con quelli alle pft . 970 radiol med ( 2012 ) 117 : 968978 cases of sarcoidosis studied from january 1998 to december 2010 by using two or more hrct examinations performed at intervals of at least 15 months , combined with pft within 2 months from hrct . 
 materiali e metodi popolazione di studio hrct technique and image assessment hrct scans were acquired using a 64 - slice ( sensation siemens , forcheim , germany ) or a six - slice ct scanner ( somatom emotion siemens )  . 
all scans were performed with the high - resolution volumetric technique : thin collimation ( 0.60.75 mm ) and breath - hold acquisition from the lung apices to below the costophrenic angles with the patient in supine position . 
 in eight cases , the baseline ct was only available on hardcopy film . the first phase of image assessment consisted of analysing the findings and overall pattern of disease at baseline hrct . 
hrct patterns were visually classified according to akira et al.s modified model [ 10 ] : nodular pattern : prevalence of nodules of variable diameter , with well - defined margins and perilymphatic distribution ( in subpleural , fissural and perivascular regions and in interlobular septa ) ; ground - glass pattern : prevalence of subsolid heterogeneous opacities with visible small bronchi and vessels ; consolidation : prevalence of increased parenchymal attenuation obscuring bronchi and vessels and without architectural distortion ; reticular pattern : prevalence of thickened interlobular septa ( < 4 mm ) , either smooth or nodular ; fibrotic pattern : prevalence of ground - glass opacities with bronchiectasis , irregular reticulation ( > 4 mm in thickness ) associated with traction bronchiectasis and / or hilarperihilar consolidation at the upper and middle third of the lung fields associated with signs of architectural distortion and / or honeycombing . subsequently , a visual comparison was made between baseline and follow - up hrct scans . 
 tecnica e valutazione delle immagini hrct gli esami hrct sono stati eseguiti mediante apparecchiatura ct a 64 strati ( sensation siemens , forcheim , germania ) o a 6 strati ( somatom emotion siemens , forcheim , germania )  . 
tutte le scansioni sono state eseguite con tecnica volumetrica ad alta risoluzione utilizzando una collimazione sottile ( 0 , 60 , 75 mm ) , a paziente supino , dagli apici del polmone fino agli angoli costo - frenici , con il paziente in apnea dopo uninspirazione massimale . 
 gli esami hrct sono stati valutati da un medico radiologo con 7 anni di esperienza nella valutazione delle malattie infiltrative diffuse alla hrct , su una postazione di lavoro dedicata ( leonardo , siemens , germania )  . 
gli esami iniziali di 8 pazienti sono stati invece valutati su pellicola . la prima fase della valutazione radiologica consistita nellanalisi dei reperti e del pattern globale della malattia agli esami hrct iniziali . 
 [ 10 ] : pattern nodulare : predominanza di noduli di diametro variabile , a margini netti , a distribuzione peri - linfatica ( in sede sub - pleurica , scissurale , nei setti interlobulari e peri - vasale ) ; pattern a vetro smerigliato : predominanza di opacit sub - solide disomogenee con piccoli bronchi e vasi visibili nel contesto ; pattern consolidativo : predominanza di addensamenti parenchimali senza distorsione della architettura polmonare ; pattern reticolare : predominanza di setti interlobulari ispessiti ( < 4 mm ) , lisci o con noduli ; pattern fibrosante : predominanza di opacit a vetro smerigliato con bronchi ectasie nel loro contesto , reticolaradiol med ( 2012 ) 117 : 968978 level . 
analysis was based on the overall qualitative visual assessment of changes in disease extent ( no change , decreased , increased ) and pattern ( no change , changed with or without signs of fibrosis )  . 
the above data were used to formulate a final assessment regarding disease evolution at hrct , which was classified as follows : no change : no change in extent or pattern ; improved : decrease in extent ; worsened : increase in extent and / or change into a fibrotic pattern . pulmonary function testing pft was performed with a pneumotachograph and plethysmograph connected to a computer ( vmax 6200 , sensormedics , yorba linda , usa ) and included spirometry , measurement of lung volumes and diffusion lung capacity ( dlco )  . 
recorded parameters , expressed as percentage of theoretical values , were total lung capacity ( tlc ) , forced vital capacity ( fvc ) , slow vital capacity ( svc ) , ratio of forced expiratory volume at 1 s to fvc ( fev1 / fvc ) and dlco . 
 zioni ( > 4 mm di spessore ) irregolari associate e bronchiettasie da trazione , e / o consolidazioni ilo - perilari al terzo superiore e medio dei campi polmonari associati a segni di distorsione dellarchitettura parenchimale , e / o honeycombing . successivamente stata effettuata una valutazione visiva comparativa tra gli esami hrct iniziali e quelli al followup . 
lanalisi si basata sulla valutazione visiva globale - qualitativa dei cambiamenti in estensione ( invariata , diminuita , aumentata ) e del pattern ( invariato , mutato con o senza segni di fibrosi ) della malattia . 
dalle suddette valutazioni stato estrapolato il dato finale circa levoluzione della malattia alla hrct secondo il seguente schema : invariata : non cambiamenti in estensione e del pattern ; migliorata : riduzione in estensione ; peggiorata : aumento in estensione e / o evoluzione verso un pattern fibrotico . prove di funzionalit respiratoria le pft sono state eseguite con pneumotacografo e cabina pletismografica connessi a computer ( vmax 6200 , sensormedics , yorba linda , usa ) e comprendevano la spirometria , la misura pletismografica dei volumi polmonari e la misura della capacit di diffusione del polmone ( dlco )  . 
i parametri registrati , espressi come percento del teorico , sono stati la capacit polmonare totale ( tlc , total lung capacity ) , la capacit vitale forzata ( fvc , forced vital capacity ) , la capacit vitale lenta ( svc , slow vital capacity ) , il rapporto tra il volume espiratorio forzato al 1 secondo ( fev1 , forced expiratory volume at 1st second ) e la fvc ( fev1 / fvc ) e la dlco . 
tutte le pft sono state effettuate entro due mesi dallesame hrct . results analisi statistica fourteen patients with sarcoidosis were selected for the final analysis ( ten men , mean age 52.6 years , range 3468 , and four women , mean age 62.2 years , range 3679 ) who had undergone pft and follow - up hrct after a median of 33 ( range 1563 ) months . 
the diagnosis of sarcoidosis was confirmed by 11 / 14 ( 78.6% ) transbronchial biopsies , 2 / 14 ( 14.3% ) surgical lung biopsies and 1 / 14 ( 7.1% ) surgical lymph node biopsy . 
 972 table 1 baseline high - resolution computed tomography ( hrct ) findings and patterns baseline hrct findings predominant pattern on baseline hrct nodular ( 5 patients ) ground - glass ( 3 patients ) reticular ( 2 patients ) fibrotic ( 4 patients ) radiol med ( 2012 ) 117 : 968978 micronodules , n macronodules ( 0.53 cm ) , n consolidation ( > 3 cm ) , n ground - glass opacity , n interlobular septal thickening , n irregular reticulation and / or honeycombing , n traction bronchiectasis , n micronoduli macronoduli ( 0 , 53 cm ) consolidazioni ( > 3 cm ) opacit a vetro smerigliato setti interlobulari ispessiti reticolazioni irregolari e / o honeycombing bronchiettasie da trazione tabella 1 frequenza dei singoli reperti polmonari stratificata per i pattern predominanti hrct reperti iniziali pattern predominante iniziale nodulare ( 5 pazienti ) vetro smerigliato ( 3 pazienti ) reticolare ( 2 pazienti ) fibrosante ( 4 pazienti ) ten ( 71.4% ) had been treated with steroid therapy , and two ( 14.3% ) had taken no drugs . hrct findings and patterns are summarised in table 1 . 
the two cases of worsening included one of increased extent of ground - glass opacities with development of bronchiectasis and one of evolution towards fibrosis with development of irregular consolidations associated with traction bronchiectasis . 
in the two patients with reticular pattern ( 2 / 14 , 14.3% ) , follow - up revealed one case of improvement with decreased disease extent and one of stable disease . 
in the four patients risultati sono stati selezionati per lanalisi finale 14 pazienti con sarcoidosi ( 10 maschi , et media di 52 , 6 anni , range 34 68 anni , e 4 femmine , et media 62 , 2 anni , range 3679 anni ) che avevano eseguito le pft ed il controllo hrct di follow - up ad una mediana di 33 mesi ( 1563 mesi )  . 
la diagnosi di sarcoidosi stata corroborata da 11 / 14 ( 78 , 6% ) ago - biopsie trans - bronchiali , 2 / 14 ( 14 , 3% ) biopsie polmonari chirurgiche , 1 / 14 ( 7 , 1% ) biopsia linfonodale chirurgica . 
lanamnesi farmacologica era disponibile in 12 pazienti : 10 ( 71 , 4% ) erano stati sottoposti a terapia steroidea , mentre 2 ( 14 , 3% ) non assumevano alcun farmaco . i reperti e i pattern hrct sono schematizzati nella tabella 1 . 
sono stati riscontrati 4 pattern predominanti : nodulare ( 5 pazienti ) , vetro smerigliato ( 3 pazienti ) , reticolare ( 2 pazienti ) e fibrosante ( 4 pazienti )  . 
i noduli ( 11 / 14 , 78 , 6% ) e le bronchiettasie da trazione ( 8 / 14 , 57 , 1% ) sono risultati i reperti di maggior riscontro . 
among patients with disease worsening , 5 / 14 ( 35.7% ) showed increased extent of disease and 3 / 14 ( 21.4% ) evolution towards fibrosis . there was no significant difference in mean pulmonary function parameter values and body mass index ( bmi ) as measured at baseline and at follow - up ( table 2 )  . 
in questultimi abbiamo riscontrato in un caso un aumento in estensione delle aree a vetro smerigliato con comparsa di alcune bronchiectasie , mentre nellaltro unevoluzione in fibrosi con la comparsa di consolidazioni irregolari associate a bronchiettasie da trazione . 
nei due pazienti con pattern reticolare ( 2 / 14 , 14 , 3% ) , al follow - up abbiamo osservato un miglioramento , con riduzione in estensione della patologia , ed un quadro invariato . 
nei quattro pazienti con pattern fibrosante ( 4 / 14 , 28 , 6% ) , al follow - up abbiamo rilevato un quadro staziona974 radiol med ( 2012 ) 117 : 968978 fig . 
tra quelli peggiorati , in 5 / 14 ( 35 , 7% ) si osservato un aumento in estensione dei reperti , mentre in 3 / 14 ( 21 , 4% ) unevoluzione fibrosante del pattern . non stata osservata alcuna differenza significativa tra i valori medi dei parametri funzionali respiratori di base , cos come dellindice di massa corporea ( bmi ) e quelli corrispondenti misurati al follow - up ( tabella 2 )  . 
una correlazione significativa stata trovata tra la variazione media della fvc e della vc ( r = 0 , 82 , p < 0 , 01 )  . la comparazione tra i dati hrct e le pft nella valutazione dellevoluzione della malattia riassunta nella tabella 3 . 
in the four patients with reduced fvc , hrct revealed fibrotic evolution in one case of nodular pattern at baseline hrct and increased extent in the remaining cases ( one ground - glass opacity and two fibrotic patterns at baseline hrct )  . 
in 5 / 14 patients , hrct and fvc were discordant at follow - up : one patient had estensione nei restanti casi ( 1 a vetro smerigliato , 2 fibrosante alla hrct baseline )  . 
in 5 / 14 pazienti invece emersa una discordanza tra hrct e fvc al follow - up : un paziente presentava fvc aumentata , ma quadro hrct peggiorato ( pattern fibrosante al baseline ) ; quattro mostravano fvc invariate , mentre lesame hrct era in un caso migliorato ( pattern reticolare al baseline ) ed in tre peggiorato ( pattern nodulare o a vetro smerigliato al baseline )  . 
 discussione il decorso della sarcoidosi molto variabile e nessun indice 976 radiol med ( 2012 ) 117 : 968978 improved fvc but a worse hrct pattern ( fibrotic pattern at baseline ) ; four had unchanged fvc associated with improved hrct in one case ( reticular pattern at baseline ) and worsened hrct in three ( nodular or ground - glass pattern at baseline )  . 
several studies using hrt have assessed the evolution of sarcoidosis over time , but information regarding the clinical usefulness of the technique in this setting is only limited and indirect [ 8 , 10 ]  . 
there was discordance in 5 / 14 cases : 4 / 4 showed worsening of the hrct pattern at follow - up ( increased extent of lesions in three patients and development of fibrotic changes in one ) with no change in fvc in three cases and improvement in one . 
consequently , whether treatment decisions can be based on hrct changes not accompanied by changes in pft is still a matter of debate . to our knowledge , no other study has addressed this topic directly . 
nonostante non risulti previsto dalle linee guida internazionali , i clinici ricorrono sempre pi spesso alluso della hrct del torace ( al posto o dopo lesame radiografico ) associato alle pft per valutare il decorso della sarcoidosi . 
diversi studi hanno valutato levoluzione della sarcoidosi nel tempo con limpiego della hrct , ma esistono scarse nonch indirette informazioni riguardo allutilit clinica di questultima in questo ambito [ 8 , 10 ]  . 
 in questo studio , in assenza di un numero sufficiente di misurazioni della dlco , la fvc stata considerata il parametro funzionale di riferimento per monitorare il decorso della malattia . 
le discordanze sono state riscontrate in 5 / 14 casi , di cui 4 / 14 dimostravano un peggioramento del pattern hrct al follow - up ( causato da aumento in estensione delle lesioni in tre pazienti e sviluppo di alterazioni fibrotiche nellaltro ) a fronte di una stabilit della fvc in tre casi e di un miglioramento in un caso . 
rimane quindi oggetto di dibattito e di riflessione se le modificazioni hrct non accompagnate da consensuali modificazioni delle pft , rappresenti un dato su cui basarsi per rifinire le strategie terapeutiche . non sono di nostra conoscenza altri studi che hanno esplorato in modo mirato questa tematica . 
 losservazione che 3 / 5 casi con pattern nodulare allesame hrct iniziale hanno dimostrato un peggioramento al follow - up , costituito in 2 / 3 casi da unevoluzione fibrotica della malattia , rappresenta il dato che maggiormente si discosta dalle conoscenze finora disponibili . 
infatti , negli studi precedenti il pattern nodulare andava incontro a miradiol med ( 2012 ) 117 : 968978 nodular pattern at baseline hrct worsened at follow - up , in 2 / 3 cases with fibrotic change , is the most divergent finding from currently available data . 
in fact , in previous studies , the nodular pattern either improved or completely regressed over time in most cases , thus representing a favourable prognostic sign on baseline hrct examinations [ 8 , 10 ]  . 
in our study , in 2 / 5 cases of nodular pattern at baseline hrct , the signs of disease progression were not paralleled by changes in fvc , which may therefore not be a good index for monitoring this type of hrct pattern . as reported in previous studies , our data confirm that a reticular pattern tends not to worsen at hrct or pft , whereas the fibrotic pattern does , with good levels of agreement ( 3 / 4 cases ) between hrct and fvc [ 3 , 8 ]  . 
however , unlike the case with idiopathic pulmonary fibrosis or emphysema , it is difficult to visually estimate the extent of parenchymal involvement by lung nodules or other scarcely profuse lesions . 
therefore , in order to evaluate the agreement between hrct and pft in assessing disease course , we considered it sufficient and correct to provide an overall qualitative assessment on the evolution of hrct findings , similar to the type of assessment given by radiologists in clinical practice ( that is , determining whether the disease is stable , has progressed or regressed by directly comparing baseline and follow - up hrct images )  . 
a double - blind study would have allowed determination of interobserver variability , helping us to understand the usefulness and reliability of the diagnostic investigation . although fvc is an accurate index for assessing lung volume changes caused by inflammatoryfibrotic infiltrates in sarcoidosis , a combined analysis with dlco would have been more accurate for assessing disease evolution . 
in our study , the majority of patients with disease progression at hrct were nonsmokers and patients who were not receiving steroid therapy , which suggests a weak relationship between these factors and progression . 
 these findings need to be confirmed on a larger patient population than considered in our study , which does not allow for any definitive conclusions on the role of hrct in assessing disease course in relation to the different patterns of presentation . 
nel nostro studio , in 2 / 5 casi con pattern nodulare alla hrct iniziale , i segni di progressione della malattia non sono stati evidenziati dallandamento della fvc che potrebbe quindi non essere un buon indice per monitorare questo tipo di pattern hrct . analogamente agli studi precedenti , anche i nostri dati confermano che il pattern reticolare tende a non peggiorare sia alla hrct che alle pft , mentre il pattern fibrotico tende a progredire nel tempo con una buona concordanza ( 3 / 4 casi ) tra hrct e fvc [ 3 , 8 ]  . 
tuttavia , al contrario di quanto avviene per la fibrosi polmonare idiopatica o dellenfisema , risulta difficile stimare visivamente lestensione dellinteressamento parenchimale da parte dei noduli polmonari o di altre alterazioni scarsamente profuse . 
pertanto , al fine di valutare la concordanza con le pft circa levoluzione della malattia , abbiamo ritenuto sufficiente e corretto basarci su un giudizio qualitativo - globale sullevoluzione delle alterazioni hrct analogo a quello che viene richiesto ai radiologi nella pratica clinica ( ovvero se la malattia stabile , progredita o regredita mettendo a confronto diretto le hrtc iniziali con quelle al follow - up )  . 
 le immagini hrct sono state valutate da un solo radiologo esperto , mentre una valutazione in doppio cieco avrebbe permesso di stimare il grado di variabilit interosservatore necessario per comprendere meglio lutilit e laffidabilit della valutazione diagnostica in questi casi . sebbene la fvc sia un indice accurato nel valutare la variazione dei volumi polmonari causato dagli infiltrati infiammatori - fibrotici della sarcoidosi , la valutazione combinata con la dlco sarebbe stata maggiormente accurata per valutare le modificazioni della malattia nel tempo . 
nel nostro studio la maggioranza dei pazienti con progressione di malattia alla tc era costituita da non fumatori e soggetti non sottoposti a terapia steroidea , suggerendo una scarso legame tra tali fattori e la progressione della sarcoidosi . 
questi dati devono essere confermati su un numero di casi maggiore di quello del nostro studio che non consente di trarre conclusioni definitive riguardo il ruolo della hrct nella valutazione dellevoluzione della patologia , specie in relazione ai vari pattern con cui essa si pu notoriamente manifestare . 
for each patient the pretest probability of cad was obtained by using the morise score as well as the diagnostic performance of the exercise test and of mdct - ca , considering conventional coronary angiography ( cca ) as the gold standard . 
based on these results , we calculated the posttest likelihood of cad after stress testing , comparing the incremental diagnostic value for each category of cardiovascular risk with data obtained with mdct - ca . 
the diagnostic performance of the exercise test for identifying patients with significant lesions had a sensitivity and specificity of 20% and 88% , respectively , with positive ( ppv ) and negative ( npv ) predictive value of 41% and 72% , respectively . 
taking ca as the gold standard , mdctca had 93% sensitivity , 89% specificity , 88% ppv and 93% npv compared with cca in evaluating significant stenoses in the per - patient analysis . 
per ogni paziente stato calcolata la probabilit pre - test di cad mediante morise score e la performance diagnostica del cicloergometro e della actcms considerando lac come standard di riferimento ; sulla base dei risultati stata calcolata la probabilit post - test di cad dopo stress test , confrontandone il valore diagnostico incrementale per ogni categoria di rischio cardiovascolare con i dati ottenuti dalla ac - tcms . 
la performance diagnostica dello stress test nella individuazione dei pazienti con lesioni significative ha dimostrato una sensibilit e specificit del 20% e 88% con valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) di 41% e 72% . 
considerando come standard di riferimento la ac il confronto tra ac e actcms nella valutazione di stenosi significative mediante analisi per paziente ha rilevato una sensibilit pari a 93% , una specificit pari a 89% , un vpp e vpn pari a 88 % e 93% . 
 the use of diagnostic protocols based on mdct - ca ensures improved diagnostic performance compared with those involving conventional exercise electrocardiograms . keywords mdct - ca coronary angiography cad exercise test diagnostic protocol cardiovascular risk risultata essere pari a 91% . 
lutilizzazione del protocollo diagnostico che prevede lutilizzo dellac - tcms garantisce una migliore perfomance diagnostica rispetto al protocollo tradizionale . parole chiave ac - tcms angiografia coronarica cad cicloergometro protocollo diagnostico rischio cardiovascolare introduction introduzione coronary angiography with multidetector computed tomography ( mdct - ca ) is gradually entering clinical practice to exclude obstructive coronary artery disease ( cad ) [ 18 ]  . 
 the majority of studies demonstrating the diagnostic accuracy of 64 - slice mdct - ca have used methods suitable for validating the technique in comparison with conventional coronary angiography ( cca ) [ 710 ] ; however , to date , none has reported on its real effectiveness in a clinical setting [ 11 ]  . while allowing adequate validation of the modality , the approach does not allow the results to be completely extrapolated to the clinical setting . 
the current international guidelines and panels recommend the use of mdct - ca in populations with a low to intermediate risk of cad and equivocal or unfeasible stress tests [ 8 , 12 , 13 ]  . 
however , before extending the clinical use of mdct - ca to these populations , the modality should be validated in different clinical settings from those featured in traditional studies . 
although exercise testing is widely accepted as a cardiological screening tool in patients at low to intermediate risk of cad , its diagnostic performance is significantly lower than that of mdct - ca [ 14 ] , with a high number of false positive and false negative findings , resulting in diagnostic delay . 
in the standard diagnostic workup , cca is used when the exercise test is positive , but it proves to be the only examination capable of excluding with certainty obstructive cad in the presence of persisting pain adla coronarografia mediante tomografia computerizzata multistrato ( ac - tcms ) sta progressivamente entrando nella pratica clinica per la esclusione di malattia coronarica ostruttiva [ 18 ]  . 
la maggior parte degli studi che fino ad ora hanno dimostrato laccuratezza diagnostica della actcms a 64 strati hanno utilizzato metodologie atte alla validazione della stessa nei confronti dellangiografia coronarica [ 710 ] , tuttavia non esistono a tuttoggi studi pubblicati nella letteratura nei quali venga riportata la reale efficacia in ambito clinico [ 11 ]  . 
le attuali linee guida ed i panel internazionali raccomandano lutilizzo della ac - tcms in popolazioni di pazienti a rischio basso - intermedio con test provocativi dubbi o non eseguibili [ 8 , 12 , 13 ]  . 
nella pratica clinica , infatti , la actcms si confronta con difficolt maggiori per unaumentata variabilit dei profili dei pazienti dal punto di vista della sintomatologia e del profilo di rischio . 
nonostante lutilizzo del test da sforzo sia ampiamente usato come screening cardiologico nella categoria di pazienti a basso - medio rischio cardiovascolare la sua performance diagnostica decisamente minore rispetto a quella fornita dalla ac - tcms [ 14 ] , con un elevato numero di falsi positivi ma soprattutto di falsi negativi , con un conseguente ritardo diagnostico . 
nelliter radiol med ( 2012 ) 117 : 939952 dition , it is the gold standard for detecting coronary artery stenoses . diagnostico standard lac utilizzata quando la prova da sforzo risulta positiva , ma si rivela lunico esame in grado di escludere con certezza la coronaropatia ostruttiva se la sintomatologia dolorosa perdura , ed essa rappresenta oggi il gold standard per lidentificazione delle stenosi coronariche . 
 materials and methods between april 2008 and august 2010 , 531 consecutive patients ( mean age 6511.51 years ; 344 men ) undergoing mdct - ca with a 64 - detector ct device ( brilliance 64 , philips , the netherlands ) were considered . materiali e metodi inclusion criteria all patients underwent mdct - ca if they had a heart rate ( hr ) 65 bpm , whether spontaneous or induced by i.v. 
another inclusion criterion was the presence of sinus rhythm ; however , patients with chronic atrial fibrillation and relatively slow ventricular response , which could be induced to < 65 bpm , were also enrolled . 
all patients provided written informed consent . exclusion criteria symptomatic patients with acute chest pain , electrocardiogram ( ecg ) positive for ischaemia , heart rate > 65 bpm , known allergy to iodinated contrast material , pregnancy , respiratory failure , unstable clinical condition or severe cardiac decompensation were excluded from the study . 
patients with irregular heart rhythm and unable to hold their breath for at least 810 s were also excluded . preand post - test assessment of cardiovascular risk for each patient , we recorded the indication for the examination and drew up a pretest risk profile for atherosclerotic heart disease using the morise score calculated on the basis of cardiovascular history alone . 
 criteri di inclusione tutti i pazienti dello studio sono stati sottoposti allindagine ac - tcms se la frequenza cardiaca era 65 battiti per minuto ( bpm ) spontanea o indotta dalla somministrazione endovenosa di - bloccante ( metoprololo , tenormin ) con dosaggio da 2 , 5 a 5 mg , e se la capacit di mantenere unapnea era sufficiente per il periodo di acquisizione del volume toracico ( 1012 s )  . 
un altro criterio di inclusione stato costituito dalla presenza di ritmo cardiaco sinusale ; tuttavia , sono stati accettati nello studio anche i pazienti con fibrillazione atriale cronica con risposta ventricolare medio bassa , inducibile a < 65 bp tutti i pazienti hanno fornito consenso scritto allindagine . criteri di esclusione i pazienti sintomatici con dolore toracico acuto e elettrocardiogramma ( ecg ) positivo per ischemia , con frequenza cardiaca > 65 bpm , allergia nota al mezzo di contrasto iodato , gravidanza , insufficienza respiratoria , stato clinico instabile e scompenso cardiaco di grado severo sono stati esclusi dallo studio . 
 valutazione pree post - test del rischio cardiovascolare per ciascun paziente stata registrata lindicazione allesame ed stato tracciato un profilo di rischio di cardiopatia aterosclerotica pre - test da sforzo utilizzando il morise score calcolato sulla base della sola anamnesi cardiovascolare . 
il morise score pre - test stato calcolato mediante la seguente formula [ 15 , 16 ] : - 3 , 6 + ( 0 , 08et ) ( 1 , 3sesso ) + ( 0 , 6sintomi ) + ( 0 , 7dia bete ) + ( 0 , 3fumo ) ( 1 , 5superficie corporea ) + ( 0 , 50 estrogeni ) + ( 0 , 3numero di fattori di rischio ) ( 0 , 40ecg a riposo ) 942 patient preparation each patient studied by mdct - ca underwent preliminary ecg at our cardiology service in order to rule out any contraindications to - blockers . 
their heart rate was then measured immediately before the examination and further reduced if necessary . examination technique scan protocol a dose of 80100 ml of iodinated nonionic contrast medium ( iomeprol 400 mgi / ml , iomeron , bracco , milan , italy ) was administered intravenously at a flow rate of 5 ml / s , followed by 40 ml of saline at the same rate . 
the contrast material was introduced using a dual - head automatic injector ( stellant , medrad , pittsburgh , pa , usa ) connected to an antecubital vein via a 16 - gauge needle cannula . 
 to limit the radiation dose as far as possible , the acquisition protocol was tailored on the basis of each patients heart rate and body mass index ( bmi )  . 
the mdct - ca radiation dose delivered to the patients was obtained from data supplied by the equipment manufacturer and compared with that of cca and expressed in msv . data processing image analysis image reconstruction was performed using retrospective ecg gating [ 20 , 21 ] in the mid - / end - diastolic phase ; if image quality proved inadequate , additional reconstructions were obtained in the end - systolic phase . images were evaluated by a radiologist with 5 years experience in mdct - ca . 
for each lesion , stenosis was estimated visually according international criteria [ 7 , 8 ] ; 020% 2050% 5070% 70100% severe occlusive or subocclusive stenosis . absence of stenosis or wall irregularities ; nonsignificant stenosis ; significant stenosis ; radiol med ( 2012 ) 117 : 939952 per i pazienti sottoposti al cicloergometro stato calcolato il rischio cardiovascolare post - test da sforzo calcolato mediante il morise score posttest [ 15 , 16 ] : - 0 , 12 + ( 4 , 5morise pre - test ) + ( 0 , 37depressione st in mm ) + ( 1slivellamento st ) ( 0 , 4sottoslivellamento st ) ( 0 , 016 frequenza cardiaca massima raggiunta durante lo sforzo ) preparazione del paziente ogni paziente sottoposto ad ac - tcms aveva eseguito un ecg preliminare presso il nostro servizio di cardiologia , per escludere la presenza di controindicazioni alluso del - bloccante . 
al momento dellesame stata controllata le frequenza cardiaca e se necessario ulteriormente abbassata . esecuzione dellesame protocollo di scansione sono stati somministrati per via endovenosa 80100 ml di mezzo di contrasto non ionico iodato ( iomeprol 400 mgl / ml , iomeron , bracco , milano , italia ) con un flusso di 5 ml / s , seguito da 40 ml di soluzione salina allo stesso flusso . 
il mezzo di contrasto stato introdotto tramite un iniettore automatico a doppia pompa ( stellant , medrad , pittsburgh , pa , usa ) connesso a una vena antecubitale con un agocannula da 16 g . 
sulla base dei valori di frequenza cardiaca e delle caratteristiche antropometriche del paziente ( indice di massa corporea , bmi ) stato scelto per ciascun paziente il protocollo di acquisizione ottimale al fine di ottenere il maggior risparmio di dose possibile . 
stata registrata dai dati forniti dallapparecchiatura la dose radiogena somministrata ai pazienti con lac - tcms , confrontandola con quella dellac ed espressa in msv . elaborazione dei dati per la ricostruzione delle immagini stata utilizzata una tecnica retrospettica ecg - gated [ 20 , 21 ] in fase meso - / telediastolica , e in caso di qualit delle immagini non sufficiente sono state eseguite ricostruzioni aggiuntive in fase tele - sistolica . 
 analisi delle immagini la valutazione delle immagini stata effettuata da un radiologo con 5 anni di esperienza continuativa in ac - tcms e , radiol med ( 2012 ) 117 : 939952 table 1 sixty - four - slice computed tomography ( ct ) parameters tabella 1 parametri di scansione di tc - 64 slice angiografia coronarica convenzionale ( ac ) scan detectors collimation ( mm ) kilovolts milliamperes / s rotation time ( ms ) table feed ( mm / rotation ) detector pitch conical pitch time for a 30 - cm scan ( s ) reconstruction effective slice thickness ( mm ) reconstruction index ( mm ) field of view ( mm ) convolution kernel window ( width / centre ) 0.625 120 / 80 1201 , 000 19.2 250300 medium ( xcc ) 600 / 200 scansione detettori collimazione ( mm ) voltaggio ( kv ) milliampere / s tempo di rotazione ( ms ) avanzamento ( mm / rot ) pitch del detettore pitch conico tempo per una scansione di 30 cm ( s ) ricostruzione spessore effettivo dello strato ( mm ) indice di ricostruzione ( mm ) campo di vista ( mm ) filtro di convoluzione finestra ( ampiezza / centro ) 0 , 625 120 / 80 1201000 19 , 2 250300 medio ( xcc ) 600 / 200 based on the per - segment analysis , identifying a vessel with stenosis > 50% stenosis led to an indication for cca . conventional coronary angiography ( cca ) angiography was carried out with a dedicated single - plane angiography system ( coroskop siemens , erlangen , germany )  . 
segments were classified as nonsignificantly stenotic ( normal or with wall irregularities or with noncritical stenosis < 70% ) or significantly stenotic ( critical stenosis > 70% ) , in agreement with the conventional classifications and guidelines [ 8 ]  . 
 la valutazione delle arterie coronarie ha previsto uno studio dei singoli segmenti effettuato seguendo una classificazione dellalbero coronarico a 17 segmenti secondo lamerican heart association ( aha ) [ 22 ]  . 
per ogni lesione stata effettuata una stima di stenosi visuale distinta secondo i criteri internazionali [ 7 , 8 ] : 0%20% 20%50% 50%70% 0%100% assenza di stenosi o irregolarit parietali ; stenosi non significativa ; stenosi significativa ; stenosi severa occludente o sub occludente . sulla base dellanalisi per segmenti la identificazione di un vaso con stenosi > 50% ha portato allindicazione ad eseguire allo studio coronarografico ( ac )  . le procedure angiografiche sono state effettuate mediante un angiografo monoplanare dedicato ( coroskop siemens , erlangen , germania )  . 
i segmenti sono stati classificati come non significativamente stenotici ( normali o con irregolarit della parete o con stenosi non critica < 70% ) o significativamente stenotici ( stenosi critica > 70% ) , utilizzando le classificazioni convenzionali e le linee guida [ 8 ]  . 
lintervallo di tempo tra lac - tcms e la ac stato compreso tra 24 ore e 15 giorni . test da sforzo mediante cicloergometro ciascun paziente stato posizionato su un ciclo in posizione seduta . 
il tracciato elettrocardiografico stato registrato in tutte le fasi dellindagine , partendo da una fase di riposo fino ad arrivare a energie negative incrementali di 25 w ogni 2 minuti , fino al raggiungimento della soglia massima teorica . 
 il test risultato positivo quando stato riconosciuto un sotto slivellamento st rettilineo maggiore o uguale a 1 mm , o discendente o ascendente maggiore o uguale a 1 , 5 mm in due derivazioni contigue , o quando il paziente ha accusato sintomatologia anginosa . 
il test risultato dubbio per patologia significativa in caso vi fosse un sotto slivellamento st minore dei parametri indicati con persistenza del pattern al recupero , in presenza di sintomatologia tipica , o se presente angina tipica anche in assenza di alterazioni elettrocardiografiche . 
in tutti gli altri casi lesame risultato essere negativo . 944 radiol med ( 2012 ) 117 : 939952 exercise testing with cycle ergometer percorsi diagnostici / terapeutici each patient was seated on a cycle ergometer . 
ecg tracing was recorded in all phases of the study , starting with a rest phase , followed by 25 - w increments every 2 min up to maximum theoretical threshold . 
the test was positive when a horizontal st - segment depression of at least 1 mm or a downsloping or upsloping st depression of at least 1.5 mm was identified in two contiguous derivations , or when the patient reported angina - like symptoms . 
the test was equivocal for significant disease if the st - segment depression was lower than the parameters indicated above with the pattern persisting on recovery , in the presence of typical symptoms or if typical angina was present even without ecg abnormalities . 
 stata valutata la correlazione tra la stenosi coronarica misurata tramite actcms ed il semplice profilo di rischio cardiovascolare , rappresentato dal morise score pre - test , e con laggiunta del cicloergometro , rappresentato dal morise score post - test . 
 the diagnostic protocols taken into consideration were assessed on the basis of these comparisons between the two methods . results mdct - ca the patients studied with mdct - ca were predominantly those with low to intermediate risk of cad and discrepancy between symptoms and clinical laboratory findings ( table 2 )  . 
history findings allowed us to distinguish a low - risk profile for the presence of one or two risk factors and an intermediate risk profile for the presence of two or more risk factors ( table 2 )  . 
mdct - ca study quality , based on qualitative criteria , i pazienti sottoposti ad indagine ac - tcms erano in prevalenza soggetti con basso - medio rischio di malattia coronarica ( cad ) con discrepanza tra sintomatologia e dati clinico - laboratoristici ( tabella 2 )  . 
i rilievi anamnestici hanno permesso di distinguere un profilo di rischio basso per la presenza di uno o due fattori di rischio e intermedio per la presenza di due o pi fattori di rischio ( tabella 2 )  . 
la qualit delle indagini ac - tcms , basata su un criterio qualitativo stata definita in 468 / 550 ( 85% ) casi buona , in 72 / 550 ( 13% ) casi discreta , in 11 / 550 ( 2% ) casi insufficiente per artefatti da movimento respiratorio del paziente durante la scansione angiografica . 
 la frequenza cardiaca media dei pazienti prima della preparazione era di 67 bpm ; la frequenza cardiaca media durante lacquisizione ( dopo eventuale somministrazione di cronotropi negativi ) risultata essere di 63 bp trecentonovantatr casi su 550 ( 71% ) casi non presentano lesioni significative , di questi 122 / 393 ( 31% ) erano cadfree , cio totalmente privi di lesioni coronariche ; nei rimanenti 157 / 550 ( 29% ) pazienti sono state riconosciute lesioni significative ad almeno un segmento coronarico . 
dei 157 pazienti , risultati positivi allac - tcms , 128 ( 23% ) sono stati sottoposti ad ac , che ha confermato in 116 pazienti ( 91% ) i dati rilevati allac - tcms , nei rimanenti 12 casi lac non ha confermato la positivit dellac - tcms . 
patients average heart rate prior to preparation was 67 bpm ; mean heart rate during acquisition ( after administration of - blockers , if necessary ) was 63 bpm . a total of 393 of 550 ( 71% ) cases showed no significant lesions ; of these , 122 / 393 ( 31% ) were cad free . 
significant lesions in at least one coronary segment were recognised in the remaining 157 / 550 ( 29% ) patients , of the 157 patients with positive mdct - ca , 128 ( 23% ) underwent cca , which confirmed the mdct - ca findings in 116 patients ( 91% ) , and did not confirm them in the remaining 12 cases . 
taking coronary cca as the reference standard , direct comparison between cca and mdct - ca in assessing significant stenoses on a per - patient basis provided the results shown in table 3 : cycle ergometer on the basis of the risk profiles and clinical history data previous to mdct - ca , 214 / 550 ( 39% ) patients underwent hanno completato liter diagnostico - terapeutico presso la nostra struttura per rifiuto del paziente . 
considerando come standard di riferimento lac il confronto diretto tra ac e ac - tcms nella valutazione di stenosi significative mediante analisi per paziente ha fornito i dati presentati in tabella 3 . cicloergometro sulla base dei profili di rischio e dei dati clinico anamnestici precedentemente allac - tcms sono stati sottoposti a cicloergometro 214 / 550 ( 39% ) pazienti di cui solo il 15% risultato positivo mentre l85% dubbio o negativo . 
considerando come riferimento la ac - tcms la performance diagnostica espressa dalla prova da sforzo mediante cicloergometro nella determinazione di pazienti con lesioni significative ha dimostrato i dati riportati in tabella 4 . il confronto tra grado di stenosi coronarica misurata tramite ac - tcms e morise score pre - test ha dimostrato come , allaumentare del grado di stenosi , ci sia un progressivo aumento del grado di rischio cardiovascolare calcolato su dati esclusivamente anamnestico - laboratoristici , e che questo dato sia pi specifico in caso stenosi coronarica severa , rispetto ai pazienti privi di stenosi , nei quali il rischio rimane comunque di circa il 50% . i dati riguardanti la valutazione pre - test del rischio di cad mediante morise score con i soli dati anamnestiradiol med ( 2012 ) 117 : 939952 table 3 diagnostic accuracy of multidetector computed tomography coronary angiography ( mdct - ca ) versus conventional coronary angiography ( cca ) tabella 3 accuratezza diagnostica dellangiografia coronarica mediante tomografia assiale multistrato ( ac - tcms ) vs . 
cca true positives false positives false negatives true negatives positive predictive value negative predictive value sensitivity specificity likelihood ratio ( t + ) likelihood ratio ( t ) accuracy exercise test vs . 
taking mdct - ca as a reference , the diagnostic performance of bicycle exercise testing in identifying patients with significant lesions yielded the data presented in table 4 . comparison between severity of coronary stenosis as measured by mdct - ca and the pretest morise score showed that with increasing degree of stenosis there is a steady increase in cardiovascular risk as calculated on historylaboratory data alone and that this correlation is more specific in the event of severe coronary stenosis compared with patients without stenosis , in whom the risk remains around 50% results of the pretest evaluation of cad risk using the morise score based on patient history alone , in the various degrees of coronary stenosis obtained on mdct - ca , are presented in fig . 
the incremental value of the exercise test showed a trend similar to that of patient history alone : the cycle ergometer became more sensitive with increasing ci , nei diversi gradi di stenosi coronarica ottenuti tramite ac - tcms sono riportati in figura 3 . 
il valore incrementale del test da sforzo mostra un trend simile a quello della semplice anamnesi : il cicloergometro diventa pi sensibile allaumentare della stenosi coronarica mentre d uno scarso valore aggiunto in caso di pazienti con coronarie sane . 
i dati riguardanti la valutazione post test del rischio di cad mediante morise score con i dati anamnestici sommati al risultato del cicloergometro , nei diversi gradi di stenosi coronarica ottenuti tramite ac - tcms sono riportati in figura 4 . nel nostro studio la maggior parte dei pazienti stata sottoposta ad un protocollo a risparmio di dose : il protocollo retrospettivo cardiac dose right in 248 / 550 pazienti ( 45% dei casi ) , con valori attorno ai 10 msv di dose effettiva erogata , ed il protocollo prospettico steep and shoot in 77 / 550 pazienti ( 14% dei casi ) , con valori di circa 1 , 2 mssv di dose effettiva . 
nel rimanente 40% dei pazienti non stato possibile utilizzare un protocollo a risparmio di dose a causa della frequenza cardiaca elevata , di aritmie , della costituzione del paziente e della scarsa collaborazione dello stesso , in questo 948 radiol med ( 2012 ) 117 : 939952 fig . 
 la freccia trasversale che attraversa orizzontalmente le diverse categorie di stenosi rappresenta linterpolazione lineare dei singoli rilievi e indica come allaumentare del grado di stenosi vi sia un incremento del rischio pre - test di malattia . 
the results of the post - test evaluation of cad risk using the morise score with patient history data added to the cycle ergometer results in the various degrees of coronary stenosis obtained on mdct - ca are shown in figure 4 . most patients in our study were imaged with a dose - saving protocol : the retrospective cardiac dose right protocol in 248 / 550 patients ( 45% ) , with values around 10 msv of effective delivered dose , and the prospective step and shoot protocol in 77 / 550 patients ( 14% ) , with values around 1.2 msv of effective dose . 
gli studi di validazione condotti fino ad oggi si sono focalizzati su popolazioni di pazienti ad elevata probabilit pre - test di malattia coronarica ( range 50%80% circa ) [ 1 , 4 , 2426 ]  . 
recentemente stanno emergendo risultati discrepanti rispetto alle evidenze della letteratura , espresse sia nelle recenti linee guida della societ europea di cardiologia [ 8 ] , sia in un recente documento di consenso sullappropriatezza delle indicazioni della cardio - tc e cardio - risonanza magnetica ( rm ) [ 27 ]  . 
da questi studi viene suggerito che un utilizzo della metodica in un contesto clinico sarebbe congruo nei casi in cui il paziente a rischio basso - intermedio con test provocativi dubbi , non eseguibili o inconclusivi , in virt dellelevato valore predittivo negativo dellac - tcms , in grado di escludere con accuratezza vicina al 100% la presenza di cad . radiol med ( 2012 ) 117 : 939952 fig . 
results at a variance with the literature have recently emerged and are expressed both in the new guidelines of the european society of cardiology [ 8 ] and in a consensus paper on the appropriateness of indications for cardiac ct and cardiac magnetic resonance imaging ( mri ) [ 27 ]  . 
these studies suggest that the clinical application of this modality would be appropriate in patients with low to intermediate risk of cad and with equivocal , unfeasible or inconclusive stress tests because of the high npv of mdct - ca , which can exclude cad with accuracy close to 100% . however , no study to date has described the real diagnostic accuracy of mdct - ca in a real - world clinical setting , in which the cardiologist and clinician in general can use the information provided to direct patients to the most appropriate diagnostictherapeutic protocol . 
in particular , allo stato attuale nessuno studio riporta per la reale accuratezza diagnostica estrapolata dalla realt clinica , che consiste nella effettiva performance della metodica sul campo dove il cardiologo ed il clinico in generale possono utilizzare le informazioni ottenute da questa metodica per indirizzare con maggior accuratezza il paziente al percorso diagnostico terapeutico pi ottimale . 
in particolare si pu notare come laccuratezza diagnostica dallactcms si avvicini al 100% contro solo il 68% della prova da sforzo . dai nostri dati la performance diagnostica espressa dalla prova da sforzo nella determinazione di pazienti con lesioni significative ha dimostrato una sensibilit e specificit pari a 2% e 88% rispettivamente con un vpp e vpn di 41% e 72% rispettivamente , con unaccuratezza diagnostica media di solo 68% , in linea con studi precedenti su questo argomento [ 14 , 28 ]  . 
la discrepanza tra la clinica e lo stress test ha posto indicazione alla tc che ha dimostrato una placca fibrolipidica significativa nel tratto prossimale dellarteria discendente anteriore ( in basso , immagini di volume rendering e multiplanari )  . the diagnostic accuracy of mdct - ca is close to 100% , as against 68% for exercise testing . according to our data , the diagnostic performance of exercise testing in identifying patients with significant lesions had 2% sensitivity and 88% specificity , with 41% ppv and 72% npv and a mean diagnostic accuracy of 68% , consistent with previous studies [ 14 , 28 ]  . 
accuracy changes with increasing degree of stenosis , that is , the cycle ergometer is poorly effective in low - risk patients , whereas it achieves good accuracy levels in patients with moderate to severe stenoses . 
an example of the discrepancy between anginalike symptoms and negative ecg and stress test is shown in figure 5 . these findings have an impact on the conventional diagnostic workup , as exercise testing is the first - line investigation to be performed on patients at low to intermediate risk , in whom the diagnostic performance of the exercise test is limited . 
according to our experience , the diagnostic algorithm should be changed by including mdct - ca , to be performed initially on the basis of cardiovascular history alone in order to discriminate cad - free individuals from those with cad . 
as mdct - ca has a high sensitivity for excluding disease , only patients with significant disease will have to undergo functional testing to obtain information on the reduction of coronary flow reserve related to lesions depicted by ct and , if necessary , direct the patients to invasive revascularisation procedures . stenosi del paziente , rendendo il cicloergometro scarsamente efficace nei pazienti a basso rischio mentre ritrova valori di accuratezza piuttosto buoni nel sottogruppo di pazienti con stenosi medio severe . 
un esempio di discrepanza tra sintomatologia anginosa ed ecg e cicolergometro negativi esemplificato in figura 5 . limpatto di tali osservazioni si ripercuote quindi sulliter diagnostico tradizionale che vede il test da sforzo come primo esame da sottoporre ai pazienti con rischio basso e intermedio . 
secondo la nostra esperienza sarebbe opportuno modificare dellalgoritmo diagnostico mediante lutilizzo dellac - tcms che dovr essere effettuata inizialmente sulla base sella sola anamnesi cardiovascolare per stratificare i pazienti indenni da patologia coronarica da quelli con arterie coronariche malate . 
essendo la ac - tcms metodica valida ed accurata nellesclusione di malattia con elevata sensibilit , solo i pazienti portatori di patologia significativa dovranno effettuare test funzionali in grado di dare informazioni utili sulla riduzione di riserva coronarica causata dalle lesioni evidenziate anatomicamente dalla tc , ed eventualmente indirizzare tali pazienti a procedure invasive di rivascolarizzazione . una problematica che resta da affrontare riguarda la dose radiante a cui il paziente si sottopone durante lesame tc . 
tali valori rimangono mediamente superiori a quelli dellac puramente diagnostica , ma questultima essendo metodica invasiva gravata da un 2% di complicanze peri - procedurali maggiori assenti invece nella ac - tcms . 
dose values are , on average , higher than those of purely diagnostic cca , even though cca is invasive and burdened with a 2% rate of major complications , which are absent in mdct - ca . 
recent technological progress has led to further dose savings and faster examinations , and the new generation of ct devices , according to the literature , allow the mean dose to be brought below the levels of diagnostic cca [ 19 ]  . our study has a few limitations : first , the comparison between mdct - ca and cca and between mdct - ca and exercise testing was performed on subgroups and not on the entire patient population . 
as with the entire study population , the subgroups had heterogeneous clinical indications and orig however , these limitations are justified by the clinical setting of the study , which aimed to verify the literature data in a real - world setting and assess the implications for patient management . conclusions sixty - four - slice mdct - ca has good diagnostic accuracy , even in a purely clinical setting . 
in view of the poor overall diagnostic accuracy of exercise testing with the cycle ergometer , mdct - ca may be used as a gateway to coronary angiography in patients with low to moderate cardiovascular disease risk , give that exercise testing does not provide any effective incremental value compared with cardiovascular history alone in this class of patients . il miglioramento tecnologico costante degli ultimi anni ha permesso per di ottenere ulteriori risparmi di dose e una maggiore rapidit dellesame , e con la nuova generazione di apparecchiature tc i dati in letteratura dimostrano la possibilit di abbassare la dose media erogata sotto i livelli dellac diagnostica [ 19 ]  . 
 il nostro studio presenta alcuni limiti : in primo luogo il confronto tra ac - tcms ed ac , e tra ac - tcms e cicloergometro stato eseguito su sottogruppi e non sullintera popolazione . 
queste limitazioni sono tuttavia giustificate dal contesto clinico dello studio , che non voleva essere unulteriore analisi di validazione della metodica , bens una verifica dei dati riportati in letteratura su di un contesto reale , e sulle conseguenti implicazioni a livello del managment del paziente . conclusioni la ac - tcms mediante apparecchiature a 64 strati mantiene una buona accuratezza diagnostica anche in contesto puramente clinico . 
morrone2 1radiotherapy department , azienda ospedaliera san camillo - forlanini , rome , italy 2chief executive officer , azienda ospedaliera san camillo - forlanini , rome , italy correspondence to : v . 
camillo - forlanini , circonvallazione gianicolense 87 , 00152 roma , italy , tel . : + 39 - 06 - 58704431 , fax : + 39 - 06 - 58704673 ; e - mail : vdonato@scamilloforlanini.rm.it received : 6 june 2011 / accepted : 30 august 2011 / published online : 14 may 2012 springer - verlag 2012 abstract purpose . 
twelve weeks after rt , a reduction in pain level compared with baseline ( t0 ) was recorded , which was classified as 1 in 36 patients ( 45% ) and 2 in 44 patients ( 55% )  . 
pain interference with daily activities was also recorded , with significantly reduced scores with respect to t0 : 1 in eight patients ( 10% ) , 2 in 28 patients ( 35% ) and 3 in 44 patients ( 55% ) ; quality of life scores also improved with respect to t0 : 2 in 28 patients ( 35% ) , 3 in 23 patients ( 29% ) , 4 in 22 patients ( 27% ) and 5 in seven patients ( 9% )  . 
the proposal for treating patients with painful bone metastases with a single 8 - gy fraction of rt , with all the procedures being performed on the same day , offers many advantages in terms of pain relief , quality of life and clinical management . 
ad ogni paziente stato distribuito leuropean organization for research and treatment of cancer ( eortc ) quality of life questionnaire ( qlq ) - c30 allinizio del trattamento e ad intervalli successivi . 
a 12 settimane dalla radioterapia si registrata una riduzione dellintensit del dolore rispetto al t0 , che stato classificato come 1 e 2 da 36 ( 45% ) e 44 pazienti ( 55% ) , rispettivamente . 
rispetto al t0 , si registrata anche una riduzione dellinterferenza del dolore con le attivit quotidiane , che stata classificata come 1 , 2 e 3 da 8 ( 10% ) , 28 ( 35% ) e 44 ( 55% ) pazienti , rispettivamente . 
rispetto al t0 c stato un miglioramento della qualit di vita , classificata come 2 , 3 , 4 e 5 da 28 ( 35% ) , 23 ( 29% ) , 22 ( 27% ) e 7 pazienti ( 8% ) , rispettivamente . 1072 radiol med ( 2012 ) 117 : 10711078 keywords bone metastases palliative radiotherapy single fraction quality of life conclusioni . 
la proposta di trattare con una frazione singola di 8 gy i pazienti con metastasi ossee dolenti , effettuando tutte le procedure nello stesso giorno , offre molti vantaggi in termini di riduzione del dolore , miglioramento della qualit di vita e di gestione clinica del paziente . parole chiave metastasi osee radioterapia palliativa frazione singola qualit della vita introduction introduzione about 25% of all patients with cancer develop bone metastases in the course of their illness , especially when the disease becomes incurable ; at that moment , symptom management and preservation of quality of life ( qol ) become the main priorities . 
however , this treatment option is often underutilised because the traditional and current approach consists of a multifractionated external - beam ( eb ) rt regimen [ 13 ]  . since the 1980s , randomised clinical trials have shown that single - fraction rt may provide pain relief equal to that gained from multiple - fraction regimens in bone metastases treatment [ 4 ]  . 
no dose - response relationship was noticed when comparing data from single and multifraction trials , but the role of re - irradiation and the impact of rt on other treatment endpoints , such as qol , should be considered . 
the single - fraction regimens have the additional advantage of being more convenient for both patient and care department in terms of cost effectiveness [ 5 ]  . several retrospective and prospective randomised trials comparing outcomes of various fractionated regimens versus single - fraction regimens showed unequivocally that single - fraction regimens ( mostly 8 gy ) were at least equal to various fractionated regimens in terms of pain relief [ 4 , 610 ]  . 
the latter approach , performed all in a single day , may help facilitate access to the rt unit for oncological patients and allow them to complete the planning phase and treatment delivery . 
despite the high level of evidence in the literature , the use of single - fraction rt in managing painful bone metastases is not widely adopted , as evidenced in several practice surveys [ 15 ]  . 
the aim of this study was to highlight the advantages of rapid access to a palliative rt unit adopting a multidisciplinary approach to symptom management . circa il 25% di tutti i pazienti oncologici sviluppa metastasi ossee nel corso della malattia , specialmente quando questa diventa incurabile ; in quel momento , la gestione del sintomo e la preservazione della qualit di vita diventano le priorit principali . 
sfortunatamente , questa opzione terapeutica spesso viene poco utilizzata , perch lattuale e tradizionale approccio consiste in un regime di radioterapia esterna frazionata [ 13 ]  . fin dagli anni 80 , studi clinici randomizzati hanno mostrato che la singola frazione di radioterapia consente una riduzione del dolore simile a quanto si ottiene con un regime di multifrazionamento nel trattamento delle metastasi ossee [ 4 ]  . 
nessuna correlazione dose - risposta stata notata confrontando i dati tra studi di monofrazionamento e frazionamento multiplo , ma si dovrebbe considerare il ruolo della re - irradiazione e limpatto della radioterapia su altri obiettivi del trattamento come la qualit di vita . 
i monofrazionamenti hanno lulteriore vantaggio di essere pi convenienti sia per il paziente che per il dipartimento in termini di costo - efficacia [ 5 ]  . diversi studi randomizzati retrospettivi e prospettici che hanno valutato i risultati di vari regimi di frazionamento versus regimi monofrazionati , hanno mostrato in maniera inequivocabile che la monofrazione ( soprattutto 8 gy ) almeno equivalente ai regimi frazionati in termini di riduzione del dolore [ 4 , 610 ]  . 
questultimo approccio , tutto nello stesso giorno , pu essere utile nel facilitare ai pazienti laccesso alla unit di radioterapia e nel permettere loro di completare le fase di pianificazione e il trattamento radiante . 
nonostante lalto livello di evidenza in letteratura , limpiego della radioteraradiol med ( 2012 ) 117 : 10711078 materials and methods from january 2007 to december 2008 , 142 consecutive patients affected by painful bone metastases were treated in the rt department , each with a total dose of 8 gy delivered in a single fraction . 
inclusion criteria were painful bone metastases ; any primary solid tumour except for renal cell carcinoma and melanoma ; any site with the exception of the cervical spine , as verified by bone x - ray , bone scan , computed tomography ( ct ) or magnetic resonance imaging ( mri ) ; karnofsky performance status ( kps ) > 40 ; and life expectancy > 3 months as estimated by the treating physician . 
 saturdays were dedicated to procedures related to singlefraction rt treatment of patients affected by bone metastases , which included consultation visit with a full history and a physical examination , simulation , treatment planning and rt delivery . 
fields were planned to include detected skeletal lesions with an additional 2to 3 - cm margin ; for spinal lesions , the field included at least one vertebral body above and below the painful vertebrae . 
after rt , all patients received a discharge letter and an appointment for subsequent follow - up evaluation . during treatment planning , age , sex , kps , date of histopathological diagnosis of the primary tumour , primary tumour site , treatment site , presence of other bone metastases and / or visceral metastases , concomitant systemic treatments and analgesic use were recorded . 
 1073 pia in frazione singola nella gestione delle metastasi ossee non viene ancora adottato su larga scala a livello mondiale , come evidenziato in molti studi [ 15 ]  . 
lo scopo di questo studio stato quello di evidenziare i vantaggi di un accesso rapido ad una unit di radioterapia palliativa , adottando un approccio multidisciplinare alla gestione del sintomo . materiali e metodi da gennaio 2007 a dicembre 2008 , 142 pazienti consecutivi affetti da metastasi ossee dolenti sono stati trattati nel dipartimento di radioterapia con una dose totale di 8 gy somministrata in frazione singola . 
i criteri di inclusione erano : metastasi ossee dolenti ; qualsiasi tumore primitivo solido eccetto il carcinoma renale e il melanoma ; qualsiasi sito anatomico studiato con radiografia , scintigrafia ossea , tomografia computerizzata ( tc ) o risonanza magnetica ( rm ) ad eccezione della colonna cervicale ; karnofsky performance status ( kps ) superiore a 40 ; , aspettativa di vita superiore a 3 mesi secondo la valutazione del medico di riferimento . ogni settimana i medici hanno stilato la lista dei pazienti da trattare con la singola dose di 8 gy , sulla base delle condizioni cliniche e dei reperti radiologici . 
dopo aver acquisito il consenso informato al trattamento , il paziente stato visitato ed il medico ha somministrato una copia delleuropean organization for research and treatment of cancer ( eortc ) quality of life questionnaire ( qlq ) - c30 [ 16 ]  . 
il sabato veniva riservato per le procedute correlate al trattamento di radioterapia in frazione singola dei pazienti affetti da metastasi ossee : la visita con una anamnesi completa e un esame clinico , la simulazione , il piano di trattamento ed il trattamento vero e proprio . 
i campi sono stati pianificati in modo da comprendere le lesioni scheletriche con margini di 23 cm ; per le lesioni vertebrali i campi includevano un corpo vertebrale al di sopra e al di sotto delle vertebre dolenti . 
il sistema di pianificazione di trattamento pinnacle stato usato per realizzare il trattamento e stabilire le unit monitor , sulla base delle dimensioni dei campi definiti in fase di simulazione . 
al termine della radioterapia i pazienti 1074 results of the 142 patients , 96 agreed to fill in the eortc qlqc30 ; 80 actually completed it at t4 and t12 . 
all clinical data regarding patient population are summarised in table 1 . scores for pain symptom were as follows : 3 and 4 reported by 44 ( 55% ) and 36 patients ( 45% ) , respectively , at t0 ; 1 , 2 and 3 by four ( 5% ) , 56 ( 70% ) and 20 patients ( 25% ) , respectively , at t4 ; 1 and 2 by 36 ( 45% ) and 44 patients ( 55% ) , respectively , at t12 . 
scores for pain interference with daily activities were as follows : 3 and 4 reported by 72 ( 90% ) and eight patients ( 10% ) , respectively , at t0 ; 2 and 3 by 32 ( 40% ) and 48 patients ( 60% ) , respectively , at t4 ; 1 , 2 and 3 by eight ( 10% ) , 28 ( 35% ) and 44 patients ( 55% ) , respectively , at t12 . 
in particular , the rate of patients not taking any analgesic at t0 , t4 and t12 were 6% , 35% and 40% , respectively ; only in four cases did analgesic use remained unvaried . discussion despite strong evidence of the advantages of single - fraction rt in treating bone metastases , multifractionated regimens are preferred in current clinical practice . 
the primary goal of this study was to evaluate the advantages of accelerating access to rt by providing for consultation , treatment planning and treatment delivery on the same day , thus minimising inconvenience to patients and their families . 
this approach , which is highly innovative in italy , was multidisciplinary in consideration of the fact that if a patient needs palliative rt , we can be fairly radiol med ( 2012 ) 117 : 10711078 hanno ricevuto una lettera di dimissione con la data stabilita per le visite di controllo successive . 
 durante la fase di pianificazione sono stati registrati i dati relativi ad et , sesso , kps , data della diagnosi istologica del tumore primitivo , localizzazione del tumore primitivo , sito di trattamento , presenza di altre metastasi e / o metastasi viscerali , trattamenti sistemici concomitanti , assunzione di analgesici . 
lobiettivo primario stato quello di studiare la riduzione del dolore sulla base della scala di valutazione presente nelleortc qlq - c30 , mentre le altre domande sono state considerate obiettivi secondari ; in particolare q9 ( ha avuto dolore ? ) stata considerata lo strumento principale per valutare lintensit del dolore e le sue variazioni in base a quattro differenti punteggi . 
inoltre , durante lintero periodo di osservazione stata registrata lassunzione di farmaci analgesici . risultati dei 142 pazienti , 96 hanno accettato di compilare leortc qlq - c30 e 80 lhanno completato a t4 e t12 . 
il distretto anatomico pi frequentemente irradiato stata la pelvi ( n = 31 , 38 , 8% ) , seguita dagli arti superiori e inferiori ( n = 24 , 30% ) , dalla colonna vertebrale ( n = 17 , 21 , 3% ) e da altri distretti ossei ( n = 8 , 10% )  . 
mentre tutti i pazienti hanno presentato dolore di grado severo a t0 , c stato un progressivo miglioramento fino a t12 , quando quasi la met dei pazienti non provava pi alcun dolore . 
stato ottenuto un miglioramento significativo in termini di controllo del doloradiol med ( 2012 ) 117 : 10711078 table 1 patient baseline characteristics variable tabella 1 caratteristiche di base dei pazienti caratteristica total patients median age ( range ) gender male female karnofsky performance status 5070 80100 diagnosis prostate breast lung other metastatic site spine pelvis upper / lower extremities other number of lesions solitary multiple pazienti et media ( range ) genere maschi femmine kps 5070 80100 diagnosi prostata seno polmone altro sito metastatico colonna vetebrale pelvi arti superiori / inferiori altro numero di lesioni singola multipla kps , karnofsky performance status 142 67 ( 3585 ) 111 142 67 ( 3585 ) 111 sure that rt is not all the patient needs [ 17 ]  . 
the focus on single - fraction palliative rt is an evidence - based strategy to offer greater convenience for patients , use fewer rt resources and therefore ensure greater accessibility for all patients , especially those living far away from the rt unit . 
 by concentrating all procedures in a single day , patients can 1075 re che ha consentito un miglioramento della qualit di vita ; infatti a partire da t4 nessun paziente ha avuto una qualit di vita valutata come pessima . 
i dati relativi le domande sul dolore e sulla qualit di vita delleortc qlq - c30 riferiti a t0 , t4 e t12 , sono riportati nella tabella 2 . complessivamente stata notata una progressiva riduzione dellassunzione di analgesici . 
in particolare , le percentuali di pazienti che non hanno assunto alcun analgesico a t0 , t4 e t12 sono state rispettivamente pari a 6% , 35% e 40% ; solo in 4 casi non c stata alcuna variazione nellassunzione di analgesici . discussione nonostante la forte evidenza dei vantaggi della radioterapia in frazione singola , nella pratica clinica per il trattamento delle metastasi ossee si preferisce utilizzare il regime in frazioni multiple . 
tutto questo ha significative implicazioni per la qualit di vita , il carico di lavoro del dipartimento di radioterapia , i costi per il sistema sanitario e una certa convenienza per il paziente [ 1 , 5 , 8 , 11 ]  . 
lobiettivo primario del presente studio stato quello di valutare i vantaggi della velocizzazione di un processo di somministrazione della radioterapia ad un paziente : consulto , pianificazione del trattamento e completamento della radioterapia , tutto in un solo giorno , riducendo i disagi per i pazienti e per i loro familiari . 
questo approccio , che molto innovativo in italia , ha avuto carattere multidisciplinare , considerando che se un paziente ha bisogno di una radioterapia palliativa , possiamo essere abbastanza sicuri che la radioterapia non tutto quello di cui il paziente ha bisogno [ 17 ]  . 
il punto focale della radioterapia palliativa in frazione singola si fonda sul fatto di offrire una maggiore convenienza ai pazienti , usare minori risorse di radioterapia e quindi assicurare una maggiore accessibilit a tutti i pazienti , specialmente quelli che vivono lontano dalla unit di radioterapia . 
 [ 18 ] hanno valutato , in uno studio clinico randomizzato , il risultato clinico e la tossicit di due diversi regimi di ipofrazionamento in pazienti che presentavano compressione metastatica del midollo spinale : 8 gy2 giorni vs . 
with regard to e tossicit , ma sono stati sottolineati i vantaggi di un regime short - course in termini di convenienza per il paziente e tempo macchina . per quanto riguarda la palliazione delle metastasi ossee radiol med ( 2012 ) 117 : 10711078 1077 treatment - machine time , decrease of the time for consultation and for rt delivery allows treatment of a greater number of patients without further burdening waiting lists [ 1 ]  . 
 [ 20 ] were 75% , 15% and 60% in the singlefraction arm and 86% , 13% and 73% , respectively , in the multifraction arm . analysis of our data shows that single - fraction ( 8 - gy ) rt has a major impact on pain relief and qol improvement up to 12 weeks after treatment . 
patients and their families were very satisfied with the possibility of completing all procedures and radiotherapy on the same day ; in fact , this therapeutic strategy was logistically much easier . 
this important aspect related to managing bone metastases was confirmed by the high level of satisfaction reported by our patients and their relatives , although this issue was not formally investigated . 
 single - fraction rt provides valid palliation and improved qol , with lower medical and societal costs in comparison with fractionated rt ; therefore , it should be considered the palliative treatment of choice for patients with painful bone metastases [ 21 , 22 ]  . 
nevertheless , there is still reluctance to adopt single - fraction rt as standard practice , mainly due to the need for changes in the organisation of services [ 23 ]  . 
in consideration of the relatively limited number of rt centres and their workload in italy , adoption of this rt treatment could allow a large number of patients with bone metastases to benefit from rt . 
 dolenti , i pi recenti studi clinici randomizzati di radioterapia shortversus long - course , basati sul confronto fra il braccio 8 gy ed il braccio 30 gy , hanno confermato una sostanziale equivalenza in termini di risposta ( riduzione del dolore e dellassunzione di narcotici )  . 
 [ 9 ] hanno ottenuto simili riduzione del dolore , fatigue e qualit di vita globale in entrambi i gruppi per tutto il periodo di osservazione , focalizzando la propria attenzione soprattutto sulle domande q9 e q19 delleortc qlq - c30 . 
 [ 20 ] sono stati rispettivamente 75% , 15% e 60% nel braccio della frazione singola e 86% , 13% e 73% nel braccio delle frazioni multiple . lanalisi dei dati attuali mostrano che la radioterapia in frazione singola ( 8 gy ) ha un grande impatto sulla riduzione del dolore ed il miglioramento della qualit di vita , fino a 12 settimane dal trattamento . 
i pazienti e i loro familiari hanno mostrato una forte gradimento perch hanno avuto lopportunit di sottoporsi a tutte le procedure e al trattamento stesso nello stesso giorno ; infatti , questa strategia terapeutica risultata molto pi semplice dal punto di vista logistico . 
questo importante aspetto correlato alla gestione delle metastasi ossee stato confermato dallalto livello di soddisfazione manifestato dai pazienti e dai loro familiari , anche se questo punto non stato analizzato in maniera formale . 
sulla base di questi risultati positivi , si potrebbe incentivare un tale approccio in maniera da ottimizzare le risorse umane ed economiche e migliorare la qualit di cura e il confort dei pazienti . la radioterapia in singola frazione permette una valida palliazione e un miglioramento della qualit di vita con costi medici e sociali pi bassi di quelli necessari per una radioterapia frazionata ; pertanto , dovrebbe essere considerato il trattamento di scelta per i pazienti con metastasi ossee [ 21 , 22 ]  . 
tuttavia , c ancora una certa riluttanza ad utilizzarla come una pratica standard , soprattutto a causa della necessit di dover operare cambiamenti nellorganizzazione dei servizi [ 23 ]  . 
considerato il numero relativamente limitato dei centri di radioterapia in italia e il loro carico di lavoro , ladozione di questo trattamento di radioterapia potrebbe permettere ad un maggior numero di pazienti con metastasi ossee di beneficiare del trattamento radiante . conclusioni conclusions the proposal to treat patients with painful bone metastases la proposta di trattare i pazienti con metastasi ossee dolenti con una frazione singola di 8 gy , realizzando tutte le procedure nello stesso giorno , offre molti vantaggi in termini 1078 radiol med ( 2012 ) 117 : 10711078 with single - fraction rt ( 8 gy ) , with all the procedures being performed on the same day , offers many advantages in terms of pain relief , qol and clinical management . 
this multidisciplinary character of treatment delivery and its holistic approach to symptom management in such a brief time was appreciated by both patients and their families , as was the convenience of having all the rt - related procedures in 1 day . 
 questo aspetto multidisciplinare del trattamento ed il suo approccio olistico alla gestione del sintomo in un tempo cos breve stato apprezzato sia dai pazienti che dai loro familiari , considerata la convenienza nel realizzare tutte le operativit in un solo giorno . 
i dati ottenuti dimostrano , in accordo con la letteratura , una corrispondenza tra i segni dellimaging e i reperti chirurgici , confermando il ruolo di gold standard della rm nello studio delle protesi mammarie . parole chiave impianti protesici rottura dellimpianto siliconi risonanza magnetica introduction introduzione breast implants can be used for cosmetic or reconstructive purposes . 
the first group includes bilateral breast augmentation in the absence of organic defects as well as unior il ricorso al posizionamento di impianti protesici mammari pu dipendere da motivi estetici o ricostruttivi . 
 to accommodate the different needs of cosmetic or reconstructive procedures , plastic surgeons can now choose from > 240 models of implants that differ in shape ( anatomical , rounded , horn - shaped ) , size , structure ( number of lumina ) , surface of the elastomer silicone shell ( smooth or textured ) and filler material ( silicone fluid or gel , saline solution , vegetable oils ) [ 1 ]  . 
in most cases , implant rupture is asymptomatic , with the free silicone remaining within the fibrous capsule surrounding the implant ; in this case , the rupture is discovered as an incidental finding at routine breast examination . 
very often , clinical changes in the affected breast will raise suspicion of implant coarctation or rupture , and sometimes , even in the absence of clear imaging signs of rupture , patients are referred for surgery . 
to verify a mammographic , sonographic or clinical ( generally self - reported by the patient ) suspicion of implant rupture or to assess the state of breast implants that have been in place for at least 10 years , a targeted study of the implants can be provided by magnetic resonance ( mr ) imaging , a modality considered far superior to mammography and ultrasound owing to its high diagnostic sensitivity and specificity in this setting [ 24 ]  . 
however , very often , the mr study fails to provide unequivocal signs of rupture , allowing for suspicion only . the purpose of our study was to assess the prevalence and significance of the different signs of implant rupture identified at mr imaging ( diagnostic accuracy of the modality ) by verifying in co - operation with the plastic surgeons the state of explanted prostheses after capsule enucleation and opening . materials and methods we retrospectively reviewed 253 cases of women who had undergone mr examination of breast implants over a 6 - year period ( 1 january 2004 to 31 december 2010 ) out of a total of 2 , 243 breast mr scans . 
subsequently , all patients with suspected implant rupture on the basis of clinical assessment or a level - one imaging examination ( mammography and / or ultrasound ) were referred for breast mr imaging , as were those with implants in place for 10 years . 
all patients with positive mr imaging associated with suspected bilaterale in assenza di difetti organici , cos come interventi di protesizzazione monoo bilaterale a causa di ipoplasia mammaria o di asimmetria volumetrica tra i due lati . 
 attualmente si ricorre al posizionamento di protesi mammarie per ragioni estetiche nel 70%80% dei casi ; nel 20%30% dei casi , invece , lintervento chirurgico di tipo ricostruttivo dopo trattamento terapeutico [ 1 ]  . 
per rispondere alle diverse esigenze estetiche o ricostruttive , ad oggi sono a disposizione del chirurgo plastico oltre 240 modelli diversi di protesi mammarie sulla base della forma ( anatomica , rotonda , a cornetto ) , delle dimensioni , della struttura ( ovvero al numero delle camere che le costituiscono ) , della superficie dellelastomero di silicone ( liscia o testurizzata ) e dei materiali interni ( silicone fluido o gel , soluzione salina , oli vegetali ) [ 1 ]  . 
talora le protesi possono andare incontro ad usura , a spostamenti o a vere e proprie rotture che rappresentano la principale indicazione alla loro rimozione chirurgica definitiva o alla loro sostituzione . 
il pi delle volte le rotture protesiche possono rimanere asintomatiche , in quanto il silicone libero rimane allinterno della capsula fibrosa che circonda la protesi ; in tal caso vengono diagnosticate occasionalmente nel corso di esami senologici di routine . 
oggi molto spesso la variazione clinica della mammella protesizzata che d il sospetto di coartazione o rottura della protesi e a volte , anche in assenza di chiari segni strumentali di rottura protesica , la paziente viene avviata allintervento . 
in caso di sospetto mammo - ecografico di rottura o qualora esista un sospetto clinico rilevato generalmente in maniera autonoma dalla paziente o , infine , nella valutazione dello stato di protesi mammarie impiantate da almeno 10 anni , fondamentale ricorrere alla rm per lo studio mirato delle protesi , metodica ritenuta di gran lunga superiore alla mammografia ( mx ) ed ecografia ( us ) in ragione dellalta sensibilit e specificit diagnostica in questo campo [ 24 ]  . 
molto spesso , per , in corso di esame rm non si hanno segni certi di rottura , bens di sospetto . lo scopo e la novit di questo studio , pertanto , stato quello di valutare la prevalenza e significativit dei vari segni di rottura protesica rilevabili con la rm ( pertanto laccuratezza diagnostica di tale metodica ) , verificando , in collaborazione con i chirurghi plastici , lo stato delle protesi espiantate , dopo enucleazione con capsula ed apertura della stessa . materiali e metodi sono stati rivalutati in maniera retrospettiva 253 casi di donne sottoposte a studio rm per protesi mammaria 1006 radiol med ( 2012 ) 117 : 10041018 or positive clinical and / or sonographic diagnosis of rupture were referred for surgery . 
all patients provided informed consent to undergo mr imaging and surgery and to be included in the study . breast mr imaging was performed using two 1.5 - t devices : ( a ) siemens mr imager ( magnetom symphony maestro class , siemens , forcheim , germany ) , with a dedicated coil for prone breast imaging ; ( b ) philips mr unit ( aurora imaging technology , paramed medical system , philips healthcare , the netherlands ) specially designed for breast imaging . 
with selective suppression of the silicone signal ( resonance frequency slightly lower than used for fat suppression )  . sequences acquired with the philips scanner were as follows : 1 . 
t1 rotating delivery of excitation off - resonance ( rodeo ) axial hires silicone suppressed : 128 slices ; matrix 30028096 ; fov 280280140 mm3 ( small ) , 320320150 mm3 ( medium ) , 360360180 mm3 ( large ) ; tr 11.0 ms ; te 4.8 ms ; time , 5 min ; 3 . 
t1 rodeo axial hires saline spoiled : 128 slices ; matrix 30028096 ; fov 280280 40 mm3 ( small ) , 320320150 mm3 ( medium ) , 360360180 mm3 ( large ) ; tr 11.0 ms ; te 4.8 ms ; time 5 min . on the basis of the breast mr findings , three groups were identified ( table 1 ) : 1 . 
patients with implants with clear signs of rupture , which were further subdivided into : eseguite nellarco di tempo di 6 anni , compreso tra il 01 / 01 / 2004 e il 31 / 12 / 2010 , su un totale di 2243 rm mammarie . 
successivamente , sono state inviate allo studio con rm mammaria tutte quelle pazienti che erano risultate sospette per rottura di protesi allindagine clinica o ad unindagine strumentale di primo livello ( mx e / o us ) e tutte coloro che avevano impiantato le protesi da oltre 10 anni . 
non sono stati presi in considerazione gli esami clinico - strumentali ed rm risultati positivi per rottura protesica , per i quali le pazienti hanno eseguito lintervento di espianto presso un altro ospedale . 
t2 short tau inversion recovery ( stir ) overview [ strati 5 ; spessore di strato 7 mm ; matrice 256256 ; capo di vista ( fov ) 320320 mm2 ; tempo di ripetizione ( tr ) 1540 ms ; tempo di eco ( te ) 68 ms ; numero di eccitazioni ( nex ) 1 ; tempo 0 min 22 s ] ; 2 . 
con soppressione selettiva del segnale del silicone ( frequenza di risonanza di poco inferiore a quella del grasso )  . per laurora , invece , si sono usate le seguenti sequenze : 1 . 
t1 gradiente echo ( ge ) ( 80 ) axial hires ( a - p ) : strati 64 ; matrice 285296 ; fov 280280140 mm3 ( piccolo ) , 320320150 mm3 ( medio ) , 360360180 mm3 ( grande ) ; tr 12 , 9 ms ; te 5 , 3 ms ; tempo 4 min 04 s ; radiol med ( 2012 ) 117 : 10041018 table 1 magnetic resonance imaging findings group mr imaging findings ( 157 implants ) group 1 group 2 group 3 extracapsular rupture ( n = 18 ) negative isolated fibrosis isolated coarctation intracapsular rupture isolated extracapsular rupture intra - / extracapsular rupture siliconomas seromas tabella 1 reperti riscontrati allesame rm gruppo gruppo 1 gruppo 2 gruppo 3 rottura extracapsulare ( n = 18 ) risultato rm ( 157 protesi ) negativo fibrosi isolata coartazione isolata rottura intracapsulare rottura extracapsulare isolata rottura intra - / extracapsulare siliconomi sieromi 1007 mr , magnetic resonance ; group 1 , normal implants ; group 2 , implants with alterations caused by wear and tear without clear signs of rupture ; group 3 , implants with obvious intracapsular and / or extracapsular rupture ; extracapsular rupture , siliconomas or seromas rm , risonanza magnetica ; gruppo 1 , impianti normali ; gruppo 2 , impianti con alterazioni da usura senza chiari segni di rottura ; gruppo 3 , impianti protesici con chiari segni di rottura intracapsulare e / o extracapsulare . 
extracapsular ruptures , if the silicone had leaked outside the capsule . the signs of intracapsular rupture considered at mr imaging were : the linguine sign ( including subcapsular lines ) , the droplet sign , the teardrop and noose ( or keyhole ) sign , and the salad - oil sign . 
patients with clear mr imaging signs of intraor extracapsular rupture were referred for surgery , as were those with implants in place for 10 years and signs of implant wear and tear . 
t1 rodeo axial hires silicone suppressed : strati 128 ; matrice 30028096 ; fov 280280140 mm3 ( piccolo ) , 320320150 mm3 ( medio ) , 360360180 mm3 ( grande ) ; tr 11 , 0 ms ; te 4 , 8 ms ; tempo 5 min ; 3 . 
t1 rodeo axial hires saline spoiled : strati 128 ; matrice 30028096 ; fov 280280140 mm3 ( piccolo ) , 320320150 mm3 ( medio ) , 360360180 mm3 ( grande ) ; tr 11 , 0 ms ; te 4 , 8 ms ; tempo 5 min . dallanalisi delle rm mammarie eseguite , sono stati individuati tre gruppi ( tabella 1 ) : 1 . 
rotture extracapsulari , se il silicone era fuoriuscito dalla capsula . i segni di rottura protesica intracapsulare , in corso di esame rm , presi in considerazione sono i seguenti : linguine sign ( incluse le linee subcapsulari ) , droplet sign , interval ( ci ) was considered ]  . 
of these , 167 ( 66% ) had negative results and 86 ( 34% ) had results that were either positive or suggestive for implant rupture , leading to an indication for surgery . 
 the 86 patients with positive or suggestive findings for uni or bilateral rupture had in 82.6% of cases ( n = 71 ) a bilateral implant , and in 17.4% ( n = 15 ) a unilateral implant ; therefore , the total number of studied and explanted prostheses was 157 . 
it should be noted that in patients with bilateral implants , bilateral explantation and replacement was always performed on aesthetic grounds , even if only one implant was suspected of rupture . mr findings are reported in table 1 . 
sulla base dei reperti rm sono state inviate al chirurgo plastico quelle pazienti cui erano stati rilevati segni franchi di rottura intrao extracapsulare , ma anche molte di quelle pazienti cui fossero stati presenti segni di usura legati al posizionamento dellimpianto protesico pi di 10 anni prima . 
rotture protesiche sia intrache extracapsulari . analisi statistica i dati raccolti , relativi ai reperti rm e quelli riguardanti lanalisi delle protesi , a seguito dellintervento chirurgico , sono stati sottoposti ad analisi statistica con il test esatto di fisher e il test del chi - quadro ( 2 ) corretto di yates al fine di determinare la significativit di ciascun aspetto rm nella diagnosi di rottura protesica ( stato considerato un livello di intervallo di confidenza pari a 0 , 05 )  . 
le 86 pazienti con protesi risultate positive o sospette di rottura mono o bilaterale , presentavano nell82 , 6% ( n = 71 ) un impianto protesico bilaterale e nel 17 , 4% ( n = 15 ) un impianto monolaterale ; ne deriva un numero totale di protesi studiate ed espiantate pari a 157 . 
as the noose sign was combined with other highly significant signs of rupture in 28 / 35 cases , the chi - square test with yates correction was applied to assess the actual importance of this sign in the diagnosis . 
the test showed that , in relation to the total number of noose signs detected , the combination of noose sign with other signs is statistically significant ( 2 = 16.90 , with p = 0 at 0.05 confidence interval ) , whereas the level of significance decreases ( 2 = 0.45 , with p = 0.50 ) for the noose sign seen in isolation . discussion the use of mr in the study of suspected implant rupture was introduced at the beginning of the 1990s as a complement to clinical , mammographic and sonographic assessment . 
 among all the possible complications of breast implants , tra i 18 casi di rottura extracapsulare , 7 mostravano raccolte fluide pericapsulari ( sieromi ) e 11 raccolte in regione periprotesica e / o ascellare ( siliconomi )  . 
i risultati ottenuti dallo studio degli impianti protesici con rm sono i seguenti : sensibilit pari al 96% , specificit pari al 77% e valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) e accuratezza diagnostica pari al 90% ciascuna . 
dallanalisi dei singoli segni di rottura protesica intracapsulare deriva che il segno delle linguine sia quello maggiormente osservato , in particolare 1010 radiol med ( 2012 ) 117 : 10041018 fig.2a , b axial t2 short - tau inversion recovery water - suppressed ( a ) and silicone - suppressed ( b ) sequences . 
nel lume della stessa protesi concomita il droplet sign che , associato al precedente reperto , aumenta la significativit dellesame rm nella diagnosi di rottura protesica intracapsulare . those that occur most frequently are microleakage , leakage and rupture . 
establishing a preoperative diagnosis of implant rupture on a clinical basis alone is often very difficult , because the signs and symptoms may be nonspecific , especially when the rupture is confined within the fibrous capsule [ 57 ]  . 
il segno delle linguine , sulla base del test esatto di fisher , appare uno dei segni statisticamente significativi di rottura protesica intracapsulare ( p = 0 con livello di intervallo di confidenza pari a 0 , 05 )  . 
poich il segno del nodo scorsoio in 28 / 35 casi era associato ad altri segni di rottura protesica altamente significativi , stato applicato anche il test del chi - quadro con correzione di yates per valutare la reale importanza di tale segno nella diagnosi . 
raccolta capsulata iperintensa lungo il margine posteriore della protesi sinistra ( sieroma capsulato ) , senza evidenza di chiari segni di interruzione lungo il decorso della membrana e / o capsula . 
la protesi di destra mostra contemporaneamente linguine , droplet e noose sign ; nella protesi di sinistra lunico segno di rottura intracapsulare il linguine sign , ben evidente sottoforma di segno dello stepladder allesame ecografico ( b ) effettuato ancor prima dellesame rm . in a single - lumen implant or in one or both membranes of a double - lumen implant , with leakage of silicone gel within the periprosthetic fibrous capsule , the diagnosis is intracapsular rupture . 
an extracapsular rupture , conversely , is characterised as interruption of the fibrous capsule with consequent migration of silicone and / or saline solution into the surrounding tissues . mammography , ultrasound and mr imaging are all capable of evaluating implant integrity . 
each technique has some advantages and limitations , which must be adapted to the che , in riferimento al numero totale di noose sign presenti , tale aspetto statisticamente significativo ( 2 = 16 , 90 con p = 0 al livello di intervallo di confidenza di 0 , 05 ) , mentre in caso di noose sign in assenza di altre alterazioni , la significativit viene meno ( 2 = 0 , 45 con p = 0 , 50 )  . discussione limpiego della rm nello studio degli impianti protesici 1012 radiol med ( 2012 ) 117 : 10041018 fig . 
left intraand extracapsular implant rupture evident as multiple and multidirectional hypointense folded wavy lines ( linguine sign ) together with hyperintense siliconomas along the front and medial ( retrosternal ) edge of the implant . 
a sinistra , rottura protesica intraed extracapsulare caratterizzata da multiple linee ipointense ondulate e multidirezionali ( linguine signs ) associate a raccolta di materiale iperintenso ( siliconoma ) lungo il margine anteriore e mediale ( retrosternale ) della protesi stessa . 
mammography is , in fact , able to depict extracapsular ruptures , but the signs are nonspecific , and the reported sensitivity and specificity values are relatively low ( 68% and 81% , respectively ) [ 2 ]  . 
 the main limitations of ultrasound are its complex interpretation and consequent reliance on the radiologists experience ; ultrasound has a reported sensitivity of 77% , which is con sospetta rottura stato introdotto agli inizi degli anni 90 , come completamento delliter diagnostico clinico , mx ed us . 
tra tutte le possibili complicanze , legate al posizionamento di protesi mammarie , un grosso capitolo per motivi di incidenza rappresentato da filtrazioni , stravasi e rotture , legati alla permeabilit relativa e allusura meccanica della protesi stessa , che possono causare modificazione di volume o di forma del seno . 
tali situazioni possono essere accompagnate da dolore , eritema e altre possibili anomalie segnalate in primo luogo dalla paziente radiol med ( 2012 ) 117 : 10041018 1013 table 2 number of cases for each magnetic resonance ( mr ) sign of intracapsular rupture sign of intracapsular rupture cases , n linguine sign isolated with droplet with noose with salad - oil with droplet + noose with noose + salad - oil with coarctation total droplet sign isolated with linguine with noose with linguine + noose total noose sign isolated with linguine with droplet with salad - oil with linguine + droplet with linguine + salad - oil total salad - oil sign isolated with linguine with noose with linguine + noose total coarctation isolated with linguine total 40 ( 4 ) a 7 ( 2 ) a 4 ( 3 ) a 7 ( 2 ) a 7 ( 1 ) a anumber of false positive cases at surgery halfway between mammography and mr imaging , but its specificity is the lowest of the three modalities ( 69% ) [ 2 ]  . mr imaging has higher diagnostic accuracy in assessing implant integrity , with the major advantage that specific sequences can be used to distinguish silicone from the surrounding breast tissue . 
we observed 11 false positive cases ( table 3 ) , that is , cases of implants found to be intact after surgery but characterised by equivocal findings ( n = 1 ) or clear intracapsular rupture ( n = 10 ) at mr imaging . 
the single equivocal case was coarctation of an implant , which did not show any loss of capsular continuity at surgery but only reduction in volume , accounting for changes and irregularities in contour mimicking a possible rupture at mr imaging . 
molto spesso difficile fare diagnosi preoperatoria di rottura protesica con il solo esame clinico , poich pu accadere che segni e sintomi siano aspecifici , specialmente quando la rottura confinata allinterno della capsula fibrosa [ 57 ]  . 
la prima rappresentata da un involucro costituito da silicone allo stato solido , che contiene al suo interno gel di silicone o soluzione salina o altri costituenti della camera protesica . 
la seconda espressione della reazione istopatologia ed immunitaria dellorganismo ospite allimpianto di un corpo estraneo e in rm appare come una linea ipointensa in tutte le sequenze , non distinguibile dallinvolucro protesico , anche se tra loro esiste uno spazio virtuale . 
quando c perdita di continuit della membrana protesica nella protesi monocamera o di una o entrambe nella bicamera , con successivo stravaso di gel di silicone non oltre la capsula fibrosa periprotesica , viene denominata rottura intracapsulare . 
al contrario , nelle rotture extracapsulari si verifica anche linterruzione della capsula fibrosa con associata migrazione del silicone e / o soluzione salina nei tessuti limitrofi . mx , us e rm sono tutte tecniche in grado di valutare lintegrit protesica . 
nelle pazienti con ricostruzione mammaria , il vantaggio diagnostico delle tecniche convenzionali limitato , sia in riferimento alla valutazione delle complicanze protesiche , sia alla diagnosi di eventuale patologia in sede perie / o retro - protesica . 
lus trova il suo limite in una se meiotica spesso complessa e quindi nellesperienza del radiologo e presenta in letteratura una sensibilit pari al 77% , valore intermedio tra mx e rm , ma la pi bas sa specificit tra le 3 tecniche diagnostiche , ovvero del 69% [ 2 ]  . lo studio rm possiede , invece , una maggiore accuratezza diagnostica nella valutazione dellintegrit degli impianti protesici , con il grande vantaggio di poter utilizzare sequenze specifiche per la differenzazione del silicone dal circostante tessuto ghiandolare . 
dai dati riportati in letteratura , infatti , la rm viene generalmente considerata la tecnica di scelta per la valutazione dellintegrit delle protesi mammarie , avendo una sensibilit del 72%94% e specificit dell85%100% [ 24 ]  . 
sempre riferendoci al nostro lavoro , abbiamo osservato 11 casi di 1014 radiol med ( 2012 ) 117 : 10041018 tabella 2 numero di casi per ciascun segno rm di rottura protesica intracapsulare : linguine sign ; droplet sign ; noose sign ; salad - oil sign ; coartazione segno di rottura protesica linguine sign isolato con droplet con noose con salad - oil con droplet + noose con noose + salad - oil con coartazione totale droplet sign isolato con linguine con noose con linguine + noose totale noose sign isolato con linguine con droplet con salad - oil con linguine + droplet con linguine + salad - oil totale salad - oil sign isolato con linguine con noose con linguine + noose totale coartazione isolato con linguine totale casi , n 40 ( 4 ) a 7 ( 2 ) a 4 ( 3 ) a 7 ( 2 ) a 7 ( 1 ) a anumero di casi risultati falsi positivi al riscontro post - operatorio the inflatable expanders used in the initial phases of breast reconstruction after radical mastectomy . 
the remaining false positive cases ( n = 10 ) showed isolated linguine sign ( n = 4 ) , isolated noose / teardrop sign ( n = 1 ) , isolated droplet sign ( n = 3 ) and droplet + linguine signs ( n = 2 )  . 
single signs of implant rupture and the possible reasons for diagnostic error are now described : the linguine sign and its early variant , known as subcapsular lines [ 811 ] are defined as hypointense wavy lines within the silicone gel , folded over themselves and often lying more or less parallel to the fibrous capsule [ 12 ]  . 
 [ 13 ] reported 76% sensitivity and 97% falsi positivi ( tabella 3 ) , ovvero casi di protesi dichiarate integre dopo intervento chirurgico e caratterizzate , invece , alla rm da reperti di dubbio significato ( n = 1 ) o di evidente rottura protesica intracapsulare ( n = 10 )  . 
lunico caso refertato come dubbio era quello della coartazione protesica , che al momento dellespianto non presentava difetti di continuit della capsula , ma semplicemente riduzione del volume del contenuto interno che ha determinato modifiche e irregolarit dei profili protesici allesame rm , simulando una possibile rottura . 
in realt tale protesi presentava soluzione salina come unica componente interna , come si osserva negli espansori gonfiabili utilizzati nelle fasi iniziali di ricostruzione mammaria dopo un intervento di mastectomia demolitiva . 
di seguito verranno descritti i singoli segni di rottura protesica ed il possibile motivo dellerrore diagnostico . il segno delle linguine e la sua variante precoce rappresentata dalle linee subcapsulari [ 811 ] sono definite come linee ipointense ondulate allinterno del gel di silicone , ripiegate su se stesse e spesso disposte in maniera pi o meno parallela alla capsula fibrosa [ 12 ]  . 
nei 4 casi falsi positivi alla rm in cui abbiano descritto il linguine sign , questo era dato dalla presenza di pliche radia li complesse o atipiche che mimavano la rottura dellelastomero di silicone , cos come accaduto in altri studi riportati in letteratura [ 2 , 5 ]  . 
le pliche radiali sono linee ipointense continue , caratterizzate da un doppio strato , e si estendono dalla superficie dellimpianto verso linterno con andamento piuttosto perpendicolare , terminando a fondo cieco nel lume e rappresentano un reperto di comune riscontro nelle protesi integre [ 12 ]  . 
le pliche radiali complesse si differenziano dalle precedenti per la loro maggiore lunghezza e per landamento spesso multidirezionale e rappresentano un reperto di normalit ma non escludono la possibilit di rottura protesica precoce , specie se associate ad altri segni [ 12 ]  . 
inoltre va specificato che in alcuni casi gli artefatti sulla codifica di fase dovuti a movimenti della paziente possono produrradiol med ( 2012 ) 117 : 10041018 1015 table 3 comparison between magnetic resonance ( mr ) imaging data and findings at explantation mr imaging data findings at explantation ( n ) total ( n ) mr positive mr negative ( or fibrosis ) total rupture 104 ( tp ) 4 ( fn ) 108 tp , true positive ; fp , false positive ; fn , false negative ; tn , true negative positivi negativi ( o fibrosi ) totale rottura 104 ( vp ) 4 ( fn ) 108 vp , veri positivi ; fp , falsi positivi ; fn , falsi negativi ; vn , veri negativi no rupture 11 ( fp ) 38 ( tn ) non rottura 11 ( fp ) 38 ( vn ) tabella 3 confronto tra dati dellimaging in risonanza magnetica ( rm ) e reperti riscontrati in sala operatoria dopo la rimozione protesica reperti rm reperti chirurgici ( n ) totale ( n ) specificity for this sign [ 14 ]  . 
in the four mr false positive cases in our study in which the linguine sign was detected , the sign was produced by the presence of complex or atypical radial folds mimicking rupture of the elastomer silicone shell , as reported in previous studies [ 2 , 5 ]  . 
it should be recalled that artefacts due to patient motion may in some cases produce curvilinear hypointense lines within the implant , mimicking the subcapsular lines seen in implant rupture [ 11 ]  . 
among the false positive results , there was one case ( n = 1 ) characterised by the presence of a teardrop sign and a noose ( or keyhole ) sign . 
these two very similar signs are indicative of possible intracapsular rupture and represent a focal area of shell invagination towards the centre of the implant , with escaped gel being trapped on the outer surface of the implant between the two shell sheets , which may remain separate ( noose or keyhole sign ) or adhere proximally to the capsule ( like a droplet ) [ 9 , 1113 , 15 ]  . 
it was not significant in all cases in which it was the only appreciable sign , re linee ipointense ricurve allinterno dellimpianto che possono essere confuse con le linee subcapsulari tipiche di rottura protesica [ 11 ]  . 
tra i falsi positivi del nostro studio abbiamo individuato un caso ( n = 1 ) caratterizzato dalla presenza di teardrop sign e noose sign ( questultimo denominato anche key - hole sign )  . 
questi due segni molto simili sono indicativi di una possibile rottura intracapsulare e rappresentano unarea focale di invaginazione della membrana verso il centro dellimpianto e il gel fuoriuscito rimane intrappolato allesterno tra i due foglietti della membrana che possono rimanere staccati ( nodo scorsoio o buco della serratura ) o essere accollati prossimalmente alla capsula ( goccia ) [ 9 , 1113 , 15 ]  . 
 it may , however , act as a warning sign when looking for subtle evidence of intracapsular rupture , often represented by the linguine sign [ 2 , 16 , 17 ]  . 
the droplet sign may be interpreted as microleakage , through shell defects , of serum / water droplets , which do not mix with silicone [ 12 , 14 ]  . 
 furthermore , it is also seen when saline solution , steroids or antibiotics are injected directly into the silicone chamber during the perioperative period [ 12 ] or as treatment for capsular contracture [ 2 ]  . 
the negative mr results are explained by the fact that the ruptured surface elastomer adhered to the fibrous capsule without giving rise to the linguine sign and maintaining a homogeneous high signal intensity within the ( ruptured ) implant [ 2 , 5 ]  . 
silicone , which more than 30 years ago was thought to be biologically inert [ 19 ] , is a nonbiodegradable material composed of dimethylsiloxane polymers , which elicits small local inflammatory reactions in most individuals owing to its limited ability to elicit immune reactions [ 1923 ]  . 
as described in the literature , silicone has been associated with several complications , including local and systemic granulomatous inflammatory reactions affecting breast tissue , lymph nodes , joint capsules , heart , liver and kidneys . 
il droplet sign pu essere interpretato come microfiltrazione , attraverso difetti della membrana , di goccioline di siero / acqua , che non si mescolano con il silicone [ 12 , 14 ] ; si osserva inoltre qualora vengano iniettati , direttamente nella camera di silicone , soluzione salina , steroidi o antibiotici in fase perioperatoria [ 12 ] o come terapia della contrattura capsulare [ 2 ]  . 
la negativit dellesame rm si spiega poich la rottura dellelastomero di superficie , aderiva alla capsula fibrosa senza creare il linguine sign e mantenendo omogenea liperintensit di segnale allinterno della protesi ( rotta ) [ 2 , 5 ]  . 
il silicone , che oltre 30 anni fa stato considerato come una sostanza biologicamente inerte [ 19 ] , invece un materiale protesico non biodegradabile , costituito da polimeri di dimetilxilossano , che determina linsorgenza di piccole infiammazioni locali nella maggior parte delle persone a causa della sua bassa capacit di attivare reazioni immunologiche tissutali [ 1923 ]  . 
al contrario , come descritto in letteratura , esistono complicanze associate alla presenza di silicone e che includono reazioni infiammatorie locali e sistemiche di tipo granulomatoso che coinvolgono la ghiandola mammaria , i linfonodi , le capsule articolari , il cuore , il fegato e i reni ; si pu osservare inoltre insorgenza di sindrome da distress respiratorio acuto ( ards ) , malattie autoimmuni e del tessuto connettivo in base a meccanismi ancora incerti [ 19 , 21 , 24 , 25 ]  . 
infine , nonostante non sia stata ancora accertata la reale cancerogenicit del silicone , si osservato uno sviluppo di lesioni maligne in soggetti portatori di protesi , quali il linfoma , il cancro della mammella e del polmone [ 19 ]  . nel nostro studio , tutti i 18 casi di risonanza magneradiol med ( 2012 ) 117 : 10041018 1017 autoimmune and connective tissue diseases as a result of mechanisms still to be clarified [ 19 , 21 , 24 , 25 ]  . 
tale fenomeno , definito gel - bleed o leakage stato descritto ampiamente in letteratura come trasudazione ovvero diffusione di microscopiche quantit di silicone allesterno della protesi attraverso una superficie intatta [ 5 , 1921 , 23 , 24 , 26 ]  . limite del nostro studio stata la natura retrospettiva dello stesso , che non ha consentito il recupero di tutti i dati anamnestici relativi al tipo di impianto protesico ( per quelle pi vecchie ) e alleventuale iniezione di cortisone o acqua intraprotesica che possono essere stati la causa di falsi positivi allesame rm . 
 conclusioni conclusions consistent with published data , the evaluation of implant integrity starts with a clinical and imaging assessment that includes breast examination , ultrasound and mammography according to patient age , for all symptomatic and asymptomatic patients . 
women with breast implants in place for 10 years should always undergo mr imaging , even when no clinical and / or imaging signs of rupture are present . breast mr imaging is the most sensitive technique for studying breast implant rupture , not only because of the statistical significance of some of the signs of intracapsular rupture but also because it permits investigation of equivocal abnormalities seen at mammography and ultrasound , thus representing the gold standard in diagnostic imaging . in accordo con i dati presenti in letteratura , per la valutazione dellintegrit degli impianti protesici si proceder ad una prima valutazione clinico strumentale di routine con visita senologica , us e mx in base allet , a cui saranno sottoposte tutte le pazienti sintomatiche e asintomatiche . 
nelle donne portatrici di protesi mammarie impiantate da oltre 10 anni , consigliabile comunque il ricorso alla rm anche in assenza di segni clinici e / o strumentali sospetti di rottura . la rm mammaria ad oggi risulta essere la tecnica pi sensibile per lo studio delle rotture protesiche , specialmente per la significativit statistica di alcuni segni di rottura intracapsulare , ma anche per lapprofondimento di alterazioni dubbie alle indagini strumentali mammoecografiche , rappresentando quindi il gold standard della diagnostica strumentale . 
miotto1 1sezione radiologia , dipartimento di scienze medico - diagnostiche e terapie speciali , universit di padova , via giustiniani 2 , 35128 padova , italy 2dipartimento di radiologia , azienda universit - ospedale di padova , via giustiniani 2 , 35128 padova , italy 3unit di chirurgia pediatrica e cardiopatie congenite , dipartimento di chirurgia cardiovascolare , universit di padova , via giustiniani 2 , 35128 padova , italy 4u.o. 
antonio , via facciolati 71 , 35127 padova , italy 5dipartimento di scienze oncologiche e chirurgiche , universit di padova , via giustiniani 2 , 35128 padova , italy correspondence to : r . 
contrast - enhanced ultrasonography ( ceus ) is an appealing alternative to computed tomography angiography ( cta ) for the follow - up of patients who underwent endovascular abdominal aortic aneurysm repair ( evar )  . 
lecografia con mezzo di contrasto ( ceus ) rappresenta una valida alternativa allangio - tomografia computerizzata ( cta ) nel follow - up dei pazienti sottoposti a trattamento endovascolare di aneurisma aortico addominale ( evar )  . 
ceus non apparsa superiore a cta nellidentificazione degli endoleak , probabilmente grazie al protocollo mirato comprendente la fase tardiva ( 180 s ) , che permette di 1080 radiol med ( 2012 ) 117 : 10791092 following ceus and cta results . 
attualmente cta non pu essere completamente sostituita , ma importanti limiti impongono di ridefinire il follow - up strumentale post - evar : proponiamo un algoritmo che alterni ceus e cta . parole chiave ecografia con mezzo di contrasto ( ceus ) angio - ct ( cta ) endoleaks evar aneurisma aortico addominale introduction introduzione endovascular aortic aneurysm repair ( evar ) , introduced by parodi et al . 
evar was designed to prevent aneurysm expansion and rupture by placing a covered stent - graft inside the aorta as a blood - flow conduit through the aneurysm sac [ 1 , 2 ]  . 
evar has low perioperative mortality and morbidity rates compared with oar , but it carries the need for close life - long surveillance due to a relevant incidence of long - term complications , such as endoleak , aneurysm enlargement , structural graft failure , graft migration / distortion / thrombosis , limb outflow impairment , aortic branch occlusion and graft infection [ 1 , 35 ]  . 
the overall complication rate for evar has been reported to be as high as 3040% [ 1 ] ; however , complications requiring a secondary intervention are lower ( 2.110% ) [ 4 , 6 ] , and the majority are addressed with the endovascular approach . 
catastrophic complications after evar , such as aneurysm rupture , are more frequently observed in patients with poor compliance at follow - up [ 3 , 7 , 8 ] ; 33% of patients are reportedly lost to follow - up [ 1 , 9 ]  . according to the guidelines of the society of interventional radiology [ 10 ] , post - evar imaging surveillance should evaluate three major parameters : ( 1 ) aneurysm diameter , ( 2 ) detection and classification of endoleaks and ( 3 ) detection of peculiar stent - graft morphology . 
computed tomography angiography ( cta ) remains the gold standard imaging technique to evaluate all these complications [ 1 ] , even though some alarmist studies in recent years have demonstrated an increased risk of radiation - induced cancer after repeated exposure to ct scans [ 11 , 12 ]  . 
recently , however , different dose - reduction strategies have been developed in the latest - generation scanners , such as automatic exposure - control systems and promising methods based upon iterative reconstruction , resulting in dose reduction by up to 60% [ 13 ] , or the prospecil trattamento endovascolare degli aneurismi dellaorta addominale ( evar ) , introdotto da parodi et al . 
la tecnica evar concepita per prevenire lespansione e la rottura dellaneurisma mediante il posizionamento di uno stent - graft ricoperto allinterno dellaorta , che funge da condotto per il flusso ematico attraverso la sacca aneurismatica [ 1 , 2 ]  . 
per quanto tale tecnica abbia dimostrato mortalit e morbilit perioperatorie ridotte rispetto a oar , tuttavia essa comporta la necessit di un attento monitoraggio per tutta la vita del paziente , legato alla rilevante incidenza di complicanze anche a lungo termine come gli endoleak , la crescita dellaneurisma , difetti strutturali dello scheletro protesico , migrazione del graft , trombosi con compromissione del flusso ematico , occlusione di diramazioni aortiche e infezione dellendoprotesi [ 1 , 35 ]  . 
 lincidenza complessiva delle complicanze post - evar riportata fino al 30%40% [ 1 ] , tuttavia con necessit di reintervento pi limitata ( 2 , 1%10% ) [ 4 , 6 ] e , per lo pi , possibile con approccio endovascolare . 
complicanze catastrofiche , come la rottura dellaneurisma , sono spesso correlate a scarsa compliance al follow - up [ 3 , 7 , 8 ] ; si stima che fino al 33% di pazienti vengano completamente persi al follow - up [ 1 , 9 ]  . in base alle linee guida della societ di radiologia interventistica [ 10 ] , il monitoraggio strumentale post - evar deve mirare a valutare tre parametri principali : ( 1 ) diametro aneurismatico , ( 2 ) rilevazione e classificazione degli endoleak , ( 3 ) morfologia e caratteristiche strutturali del gra devono inoltre poter essere rilevate altre evenienze come locclusione o linfezione dellendoprotesi [ 4 ]  . 
 langio - tomografia computerizzata ( cta ) rimane il goldstandard per valutare complessivamente queste complicanze [ 1 ] , sebbene negli ultimi anni alcuni studi allarmistici abbiano segnalato un aumentato rischio di carcinogenesi radio - indotta legata a ripetuti esami in tomografia computerizzata ( tc ) [ 11 , 12 ]  . 
recentemente , tuttavia , sono staradiol med ( 2012 ) 117 : 10791092 1081 tive echocardiographic ( ecg ) - gating technique in coronary ct , which is able to reduce the radiation dose by up to 90% compared with retrospective triggering [ 13 , 14 ]  . 
moreover , these radiation effects are less relevant in patients undergoing evar because patients are older ; on the other hand , their advanced age may enhance the nephrotoxic effects of iodinated contrast media [ 15 ]  . 
in light of this fact , many investigators have proposed replacing cta with other imaging modalities in post - evar surveillance , including colour doppler us ( cdu ) , contrast - enhanced us ( ceus ) or magnetic resonance imaging ( mri ) [ 16 , 17 ]  . 
cdu is a relatively inexpensive and appealing alternative for postoperative surveillance , and it is also a noninvasive modality with widespread availability [ 6 , 18 , 19 ]  . 
the introduction of ceus with second - generation us contrast agents , which increase the us sensitivity in endoleak detection , has enhanced interest in the potential of us for replacing cta in post - evar surveillance [ 16 ]  . 
the aim of this study was to evaluate monitoring of patients treated with evar by comparing ceus and cta performed with a tailored protocol and a 64 - row multidetector ct ( mdct ) scanner . materials and methods patients and study design the population in this prospective single - centre study comprised 88 consecutive patients who underwent cta between january 2008 and december 2010 : 87 during their routine follow - up after evar ( 1 and 6 months after the procedure , and then once a year ) and one patient in emergency . 
within a few hours , all patients underwent both cta ( 64 - mdct somatom sensation , siemens healthcare , erlangen , germany ) and ceus ( esatune and mylab25 , esaote biomedica , genoa , italy ) , yielding 142 paired examinations . 
 the study had three main goals : ( 1 ) identification and characterisation of endoleaks according to the classification of standard guidelines [ 2527 ] , ( 2 ) evaluation of graft patency and ( 3 ) measurement of aneurysm maximum diameter . 
inoltre , tali effetti risultano meno rilevanti nella popolazione sottoposta a evar data let mediamente avanzata , la quale peraltro pu accentuare gli effetti nefrotossici del contrasto iodato [ 15 ]  . 
alla luce di questi fatti , molti ricercatori hanno proposto di sostituire la cta con altre modalit di imaging nel follow - up post - evar , come lecografia color doppler ( cdu ) , lecografia con mezzo di contrasto ( ceus ) o la risonanza magnetica ( rm ) [ 16 , 17 ]  . 
 la cdu , relativamente economica , non - invasiva e ampiamente disponibile [ 6 , 18 , 19 ] , ha dimostrato risultati modesti nella rilevazione degli endoleak [ 2022 ] ; lintroduzione di ceus con mezzi di contrasto di seconda generazione , che aumenta in particolare la sensibilit nella rilevazione degli endoleak [ 16 , 17 ] , ha invece rinvigorito linteresse verso lecografia e il suo potenziale in questo campo [ 16 ]  . 
 fino ad oggi , pochi studi hanno comparato laccuratezza di ceus e cta nella classificazione degli endoleak [ 20 , 23 , 24 ] ; il nostro obiettivo quello di valutare il monitoraggio dei pazienti sottoposti ad evar confrontando ceus e cta , questultima eseguita con apparecchio multistrato ( 64 mdct ) e adottando un protocollo mirato . materiali e metodi popolazione e disegno dello studio in questo studio prospettico e monocentrico , tra gennaio 2008 e dicembre 2010 sono stati reclutati 88 pazienti consecutivi che si sottoponevano a cta , 87 nel corso del consueto follow - up dopo evar ( due volte nel primo anno , a 1 e 6 mesi dopo la procedura , e successivamente una volta allanno ) e uno in urgenza . 
tutti i pazienti sono stati sottoposti entro poche ore sia a cta ( 64mdct somatom sensation , siemens healthcare , erlangen , germania ) che a ceus ( esatune e mylab25 , esaote biomedica , genova , italia ) , ottenendo in totale 142 esami abbinati . 
 i tre principali obiettivi valutati in questo studio sono stati : ( 1 ) lidentificazione degli endoleaks e la loro caratterizzazione secondo la classificazione delle linee guida standard [ 2527 ] ; ( 2 ) la perviet del graft ; ( 3 ) la misura del diametro massimo dellaneurisma . 
the acquisition parameters used for the arterial phase were : collimation 640.6 mm , rotation time 0.5 s , automatic exposure modulation ( care - dose , siemens healthcare )  . 
as the measurements derived from transverse ct images may not be representative of true aneurysm dimensions , especially in tortuous vessels , we measured the maximum sac diameter in sections perpendicular to the centreline as defined by semiautomated software that determines the vessel centre line ( vessel analysis , syngo siemens )  . 
all diameters were measured from outer wall to outer wall on cta and ceus . endoleak cta classification characteristics included : ( 1 ) location and relation to the graft , ( 2 ) density on delayed images , ( 3 ) patency of the inferior mesenteric or lumbar arteries and ( 4 ) appearance of endograft junctions [ 7 , 18 , 23 , 28 , 29 ]  . 
cta examinations were performed by two senior radiologists ( dm and rm with 30 and 10 years of experience , respectively , in vascular radiology and each with 10 years of experience in ct angiography ) , in consensus reading and blinded to ceus results . ceus protocol and evaluation ceus examinations and evaluations were performed by two other senior radiologists ( lr and rs , each with 10 years of experience in the use of us contrast material ) in consensus reading , masked to cta findings , with an esatune ( 26 patients ) or a mylab25 ( 62 patients ) , with continuous low - mechanical - index ( mi 0.060.08 ) tissue harmonic imaging ( contrast - tuned imaging , esaote ) , a nonlinear imaging technique specific for second - generation echo - contrast agents . 
il ritardo della fase arteriosa stato ottimizzato con la tecnica del bolus - tracking ( carebolus , siemens healthcare ) , mentre quello della fase tardiva stato fissato a 180 secondi dalliniezione del contrasto . 
 i parametri di acquisizione della fase arteriosa prevedevano : collimazione 640 , 6 mm , tempo di rotazione 0 , 5 s , modulazione automatica dellesposizione ( care - dose , siemens healthcare )  . 
le scansioni pre - contrastografica e tardiva sono invece state condotte con collimazione pi spessa ( 241 , 2 mm ) , allo scopo di ridurre la dose di radiazioni . 
 poich le misurazioni ottenute sulle immagini assiali native possono non rappresentare le reali dimensioni dellaneurisma soprattutto in caso di vasi tortuosi , abbiamo misurato i diametri della sacca nelle sezioni perpendicolari rispetto al center - line , mediante un software semiautomatico che identifica la linea centrale del lume vasale ( vessel analysis , syngo siemens )  . 
il mezzo di contrasto tipo blood - pool di 2a generazione ( microbolle stabilizzate di esafluoruro di zolfo , sonovue , bracco , milano , italia ) , stato somministrato in una vena antecubitale in bolo da 2 , 4 ml , seguito da un flush di 10 ml di soluzione salina ( 0 , 9% nacl ) ; nei casi dubbi , stato somministrato un secondo bolo di contrasto , in particolare per potenziare la visualizzazione di tenui enhancement contrastografici . 
sometimes , microbubbles were instantly destroyed with the destructionreperfusion technique by using a brief pulse of high - intensity ( high - mi ) to detect or exclude the presence of subtle endoleaks [ 16 , 17 ]  . 
 comparisons of the cta and ceus maximum diameter of the aneurysm sac were performed with the bland - altman plot , the pearson correlation coefficient and a paired t test to assess differences in their means . 
talvolta le microbolle sono state istantaneamente distrutte con breve impulso ad alta intesit ( high - mi ) secondo la tecnica destructionreperfusion , al fine di identificare o escludere la presenza di esili endoleak [ 16 , 17 ]  . 
sono stati applicati i medesimi criteri di classificazione degli endoleaks utilizzati con la cta , implementati dalle valutazioni emodinamiche dei leak possibili durante il monitoraggio ceus [ 16 , 23 , 2830 ]  . 
le misure di diametro massimo ottenute con le due metodiche di imaging sono state comparate mediante il bland - altman plot , calcolando il coefficiente di correlazione di pearson e stimando il paired test t di student per valutare le differenze nelle loro medie . 
il limit of agreement ( loa ) clinicamente accettabile era fissato tra - 0 , 5 e 0 , 5 cm , valori tra i quali il 95% delle differenze tra i due metodi di misura sono attesi ricadere . 
questo significa che nel 95% dei casi ci sarebbe una possibilit inferiore al 5% che le differenze eccedano tale limite di 0 , 5 cm . during the study period , 95 patients were initially recruited . 
the median number of follow - up evaluations was one , with a maximum of four , over a period ranging from 1 month to 10 years after evar . risultati pazienti durante il periodo di studio , inizialmente erano stati arruolati 95 pazienti , sette dei quali poi esclusi per severa allergia al mezzo di contrasto iodato ( n = 2 ) o per grave insufficienza renale ( n = 5 )  . 
non sono state riscontrate complicanze durante gli esami , n effetti collaterali dovuti alliniezione ravvicinata dei due mezzi di contrasto endovenosi , somministrati entro 23 ore . let media dei pazienti era di 75 anni ( range 5595 anni ) ; 86 erano uomini ( 97 , 7% )  . 
scansioni assiali della cta in fase arteriosa ( a ) e tardiva ( b ) al medesimo livello : nessun leak si riconosce in fase arteriosa , mentre un leak posteriore si visualizza facilmente alla periferia della sacca nella fase tardiva a 3 minuti , ben riconoscibile anche durante il monitoraggio ceus circa 100 secondi dopo liniezione del contrasto ( in scansioni longitudinale , c , e assiale , d ) , alimentato da unarteria lombare . endoleak detection and classification both cta and ceus excluded the presence of endoleaks in 105 examinations . 
the three endoleaks missed by ceus ( all of them occurred in the first year of our study ) were described as type 2 by cta ( one from the inferior mesenteric artery and two from the lumbar artery )  . 
in one case , ceus was able to detect a type - 1 proximal endoleak only , missing the associated type - 2 endoleak , which was visualised by cta ( involving the inferior mesenteric and lumbar arteries )  . 
 appaiati per paziente variato tra 1 e 4 con mediana di 1 , in un periodo di tempo compreso tra 1 mese e 10 anni dal trattamento evar . identificazione e classificazione degli endoleak in 105 esami appaiati su 142 , sia ceus sia cta hanno escluso la presenza di endoleak , invece evidenziati in 37 esami con cta ( 26 , 05% ) e in 34 esami con ceus ( 23 , 94% )  . 
i tre endoleak non riconosciuti con ceus ( tutti durante il primo anno dello studio ) , alla cta risultavano appartenere al tipo 2 ( uno alimentato dallarteria mesenterica inferiore e due dalle lombari )  . 
in un terzo caso di tipo misto , ceus dimostrava solamente lendoleak tipo 1 prossimale e non il tipo 2 associato , coinvolgente le radiol med ( 2012 ) 117 : 10791092 1085 fig . 
2a - f volume - rendering ( vr ) 3d reconstruction of cta ( a ) shows distal dislocation of the left graft limb , corresponding to a type - 3 endoleak ( white arrow ) ; the exact correspondence between cta and ceus imaging is seen in axial ( b , white arrow ) and longitudinal ( c , black arrow ) ceus views as well as in the depiction of the collateral finding of a left hypogastric artery aneurysm ( d )  . 
preprocedure digital subtraction angiography ( e ) confirms extravasation of contrast material outside the graft from the overlapping between the main body and the contralateral limb , depicting a type - 3 endoleak . 
2a - f la ricostruzione 3d vrt di cta ( a ) mostra la migrazione distale della branca iliaca di sinistra , con endoleak di tipo 3 ( freccia bianca ) ; si noti lottima corrispondenza con le immagini ceus , in assiale ( b , freccia bianca ) e longitudinale ( c , freccia nera ) , anche nel caso di aneurisma ipogastrico , reperto collaterale ( d )  . 
la cta post - procedurale ( ricostruzione vrt , f ) documenta lesclusione dellendoleak mediante posizionamento endovascolare di stent ricoperto ed embolizzazione con spirali dellaneurisma ipogastrico . graft patency evaluation we documented one total limb graft occlusion shortly after evar , which was caused by defective graft expansion and thrombotic deposits . 
both cta and ceus depicted a kinking and infolding of graft limb skeleton with in situ occlusive thrombosis , which was treated by percutaneous revascularisation with catheter - directed in situ thrombolysis and self - expanding stenting . in 134 paired examinations , both techniques visualised complete graft patency ( n = 117 ) or the presence of endograft partial thrombosis ( n = 17 )  . 
in merito al riconoscimento degli endoleak , la sensibilit e la specificit di ceus rispetto a cta sono state rispettivamente 91 , 89% e 100% , con valore predittivo positivo e negativo rispettivamente di 100% e 97 , 22% . 
 valutazione della perviet dellendoprotesi si riscontrato un solo caso di occlusione completa di una branca protesica poco dopo lintervento , causata da difettosa espansione del graft associata a depositi trombotici . 
sia ceus sia cta hanno dimostrato la stenosi del graft con trombosi occlusiva , successivamente trattata con rivascolarizzazione endovascolare mediante trombolisi in situ e dilatazione con stent autoespandibile . in 134 esami abbinati su 142 , entrambe le metodiche hanno analogamente dimostrato la completa perviet del graft ( n = 117 ) o la presenza di parziale trombosi ( n = 17 )  . 
 in merito alla valutazione della perviet dellendoprotesi , la sensibilit e la specificit di ceus rispetto a cta sono state rispettivamente 72% e 100% , con valore predittivo positivo e negativo rispettivamente di 100% e 94 , 35% . 
selected images from the contrast - enhanced ultrasound examination at the level of the main body ( b ) and iliac branches ( c ) show complex leaks : type 3 , from the overlapping between a proximal cuff and the main body ( white arrow ) , and type 2 from the mesenteric artery ( white arrow ) act as inflow vessels , whereas the lumbar arteries act as outflow vessels . 
immagini ceus selezionate a livello del corpo principale ( b ) e delle branche iliache ( c ) descrivono un leak complesso , con afflussi provenienti sia dallembricazione tra corpo principale e cuffia prossimale ( tipo 3 , freccia bianca ) , sia dalla ima ( tipo 2 , freccia bianca ) , mentre le arterie lombari costituivano tutte vie di efflusso . 
limits of agreement were + 4.61 mm and - 4.27 mm : this indicates that in 95% of cases , the difference in cta and ceus measurement is expected to lie between these values , which are within the clinically acceptable limits of agreement ( no more than 0.5 cm ) [ 25 ]  . discussion endoleak is the most common complication after evar , with a reported incidence up to 50% [ 7 , 18 , 23 , 29 ]  . 
4 correlazione tra le misure cta e ceus del diametro massimo aneurismatico , con coefficiente di correlazione di pearson 0 , 98 ( p < 0 , 0001 )  . radiol med ( 2012 ) 117 : 10791092 1087 misurazione del diametro della sacca aneurismatica il diametro medio della sacca aneurismatica stato calcolato rispettivamente 47 , 32 mm [ deviazione standard ( sd ) = 11 , 48 mm ] con cta e 47 , 15 mm ( sd = 11 , 27 mm ) con ceus . 
 gli endoleak di tipo 2 vengono riscontrati subito dopo la procedura fino al 30% dei casi , ma la maggior parte si risolve spontaneamente ; la loro persistenza oltre i 6 mesi appare pi spesso correlata a risultati peggiori , legati alla crescita della sacca aneurismatica [ 19 ]  . 
la diagnosi degli endoleak cruciale per la prognosi del paziente e pertanto svariate tecniche di imaging sono state testate nel follow - up dopo evar . molti autori hanno comparato cdu con cta , questultima considerata il gold - standard nella diagnosi di endoleak , ottenendo risultati in parte discordanti , con sensibilit variabile tra 12% e 100% e specificit tra 74% e 99% [ 2023 , 27 , 28 , 3133 ]  . 
inoltre , la cdu presenta alcuni limiti ben noti come loperatore - dipendenza , la suscettibilit ad artefatti da meteorismo , obesit , estese calcificazioni vascolari o a elementi metallici delle protesi , oltre alla scarsa sensibilit per i leak a basso flusso [ 18 , 23 , 28 ]  . 
lintroduzione dei mezzi di contrasto di 2a generazione e dei software specifici correlati , ha eliminato i problemi legati agli artefatti e ridotto la dipendenza dalloperatore , nonch linfluenza dellobesit e del gas intestinale [ 8 , 16 , 18 , 23 ]  . 
alcuni studi hanno recentemente affermato la superiorit di ceus rispetto alla cta nella diagnosi degli endoleak [ 7 , 20 , 23 , 24 , 29 ] , grazie alla risoluzione di contrasto , alla valutazione angiodinamica del flusso , alla durata dellenhancement ( fino a 5 minuti ) , alla sensibilit nei confronti dei leak tardivi e a basso flusso ( pi di 100150 secondi dopo liniezione del contrasto )  . 
type - 1 and type - 3 endoleaks , which are relatively uncommon , are significantly related to a higher risk of aneurysm rupture and should be treated immediately when discovered . 
detection and classification of endoleaks is crucial for the patients prognosis , so many different imaging techniques have been considered for evar surveillance . many authors have compared cdu to cta the gold standard in endoleak detection with partly conflicting results , with sensitivity varying from 12% to 100% and specificity from 74% to 99% [ 2023 , 27 , 28 , 3133 ]  . 
moreover , cdu presents some well - known limitations , such as operator dependence , susceptibility to meteorism , obesity , extended endovascular calcifications , echo reflection by metallic graft components and lack of sensitivity for small lowflow leaks [ 18 , 23 , 28 ]  . 
the introduction of second - generation contrast agents with low - mi tissue harmonic imaging , in addition to the improvement of imaging technologies ( such as contrast - imaging software ) have eliminated artefact - related problems and reduced operator dependency as well as sus1088 radiol med ( 2012 ) 117 : 10791092 ceptibility to obesity or bowel gas [ 8 , 16 , 18 , 23 ]  . 
recent studies have stated that ceus is superior to cta in endoleak diagnosis [ 7 , 20 , 23 , 24 , 29 ] due to high - contrast resolution , angiodynamic evaluation , longer duration of enhancement ( up to 5 min ) , better sensitivity to late and low - flow endoleak ( more than 100150 s after contrast injection )  . 
according to this finding , we believe that ceus could be used along with cta when the latter reveals the presence of endoleak to better characterise it in view of either a second intervention [ 22 ] or monitoring . 
our results confirm that the routine use of a too short delay would explain the undetectability of slow - flow endoleaks on cta images [ 16 , 17 , 24 , 29 , 30 , 40 ]  . 
moreover , the substantial variability of the reported cta performance could be the effect of the different equipment used , mostly earlier - generation scanners ( single , 4 and 16 slices ) , compared with the device used in our study ( 64 - slice mdct )  . 
mdct high - resolution data sets now allow precise multiplanar reformatted images and 3d reconstructions , which are useful for obtaining a better definition of endoleaks , with higher sensitivity even than in conventional angiography [ 2 , 27 ]  . 
 on the other hand , in our experience ceus missed three type - 2 endoleaks and failed to demonstrate completely a mixed endoleak , showing only a type - 1 proximal endoleak and missing the other fillings , involving the mesenteric and lumbar arteries ( type - 2 endoleak ) , which were correctly detected by cta . 
nevertheless , patient management would not have changed with the use of ceus only , because the type - 1 endoleak was correctly depicted by recenti suggeriscono che ceus sia in grado di correggere valutazioni errate della cta , anche modificando sostanzialmente la gestione del paziente [ 2 , 20 ]  . 
 tale metodica appare pertanto molto utile se affiancata alla cta in caso di endoleak , poich ne perfeziona la caratterizzazione , cruciale sia nella pianificazione di un eventuale reintervento [ 22 ] , sia nel monitoraggio . 
dalla letteratura che ha confrontato ceus o cdu alla cta , emerge invece che la fase tardiva della cta , sebbene considerata indispensabile , viene eseguita con ritardi molto variabili dalliniezione del contrasto , compresi tra 6070 secondi [ 17 , 24 , 31 , 3335 ] , 80120 secondi [ 2 , 18 , 20 , 23 , 27 , 29 , 30 , 32 , 3638 ] , o qualche volta non specificati [ 3 , 4 , 8 , 19 , 39 ]  . 
luso di routine di una fase tardiva troppo precoce pu effettivamente giustificare la mancata diagnosi con cta dei leak a basso flusso nelle precedenti esperienze , come gi ipotizzato da altri [ 16 , 17 , 24 , 29 , 30 , 40 ]  . 
anche la grande variabilit di performance della cta apprezzabile in questi studi pu dipendere dalle differenti apparecchiature impiegate , che risultano per lo pi appartenere a generazioni precedenti ( singolo strato , 4 e 16 strati ) , rispetto a quella da noi utilizzata ( 64 strati )  . 
i dataset ad alta risoluzione attualmente forniti dalle mdct permettono precise ricostruzioni multiplanari e 3d , molto utili nella diagnosi di endoleak anche , secondo alcuni , con sensibilit maggiore rispetto allangiografia [ 2 , 27 ]  . 
 invece , nella nostra esperienza , 3 endoleak di tipo 2 non sono stati riconosciuti da ceus ed un endoleak misto stato incompletamente dimostrato , identificando la componente di tipo 1 prossimale ma ignorando altri inflow provenienti dalle arterie lombari e mesenterica ( tipo 2 ) ; in proposito , riteniamo che lalto flusso del leak di tipo 1 abbia mascherato il basso flusso del secondo leak . 
abbiamo osservato comunque che anche in questi casi la gestione del paziente non sarebbe cambiata anche utilizzando la sola ceus , perch il leak di tipo 1 era stato correttamente identificato e perch il comportamento attuale nei confronti dei leak di tipo 2 generalmente conservativo , con interventi selezionati nei casi di significativo ingrandimento della sacca [ 7 , 26 , 41 ] : come affermano schmieder et al . 
 [ 31 ] , alla fine sono le dimensioni della sacca il principale marcatore nella radiol med ( 2012 ) 117 : 10791092 1089 ceus and because the most recent treatment strategy for type - 2 endoleaks is conservative , with selected intervention in the case of significant sac increase [ 7 , 26 , 41 ] : as reported by schmieder et al . 
 [ 31 ] , aneurysm size is ultimately the main marker for evar surveillance , so it is not necessary to detect all type - 2 endoleaks . thrombosis is the second most common indication for reintervention ( reported between 1.4% and 7% ) , and kinking seems to be its most frequent predictor [ 7 , 34 , 42 ]  . 
both ceus and ct were able demonstrate the graft limb occlusion in the only two cases of acute ischaemia in our study due to distortion and infolding of the metallic skeleton . 
in our protocol , we paid particular attention to measurement accuracy , using curved multiplanar reformation and 3d reconstructions [ 25 ] , in order to reduce overestimation of size even in the presence of tortuosity [ 44 ]  . 
according to our results , reformatted cta measurements exceeded us diameter by a mean of 0.2 mm only , showing a very high correlation between cta and us better than in other experiences [ 8 , 32 , 44 ]  . 
based on that , ceus seems to be able to predict the maximum diameter of the aneurysmal sac as precisely as cta and could be reliably used to determine the therapeutic strategy based on the expanding sac [ 36 ]  . concerns regarding radiation dose have led some investigators to consider the possibility , in the follow - up protocols , of reducing ct radiation exposure by using low - dose protocols [ 45 ] , including other imaging modalities such as magnetic resonance imaging ( mri ) or us [ 7 , 15 , 20 , 27 , 28 , 46 ] or eliminating portions of multiphasic cta . 
although some authors have advocated eliminating precontrast scanning [ 2 , 27 ] , the arterial phase [ 37 , 38 ] or the delayed phase [ 35 ] , we believe that the typical triphasic cta may offer better results . 
in fact , precontrast and delayed imaging are critical for endoleak detection , whereas the arterial phase is effective in exactly planning percutaneous treatment of endoleaks [ 4 , 27 ]  . 
 [ 16 , 28 ] , who suggested both cta and ceus for the follow - up after evar , we are currently performing paired cta and ceus monitoring at 1 month , followed by ceus at 6 months and cta at 1 year in the case of absence of endoleaks . 
on the contrary , a closer folsorveglianza post - evar , perci non serve identificare tutti i leak di tipo 2 . la trombosi la seconda pi frequente causa di reintervento ( incidenza riportata tra 1 , 4% e 7% ) , per lo pi associata a kinking del graft [ 7 , 34 , 42 ]  . 
ovviamente , le ricostruzioni 3d elaborate dalla cta ci hanno permesso di delineare al meglio la morfologia del grale sette trombosi endoprotesiche parziali che non sono state diagnosticate con ceus erano rappresentate da apposizioni assai sottili , che non richiedono alcun intervento ; infatti , nei graft di seconda generazione , i depositi parietali non - occlusivi sembrano essere benigni e da non trattare [ 7 , 42 , 43 ]  . in merito alla misurazione del diametro della sacca aneurismatica , un coefficiente di correlazione peason statisticamente significativo ha indicato che ceus e cta producono risultati paragonabili ( r = 0 , 97 , p < 0 , 0001 )  . 
nel nostro protocollo cta abbiamo prestato particolare attenzione allaccuratezza delle misurazioni , avvalendoci delle riformattazioni su piano curvo e delle ricostruzioni 3d [ 25 ] , al fine di ridurre la sovrastima del diametro specie in caso di tortuosit [ 44 ]  . 
secondo i nostri risultati , le misurazioni del diametro massimo in cta superavano quelle ecografiche in media solo di 0 , 2 mm , dimostrando elevata correlazione tra le due metodiche , migliore rispetto ad altri studi [ 8 , 32 , 44 ]  . 
ceus quindi appare in grado di determinare il diametro massimo della sacca tanto precisamente quanto la cta ed attendibile nel definire la strategia terapeutica sulla base dellingrandimento dellaneurisma [ 36 ]  . preoccupazioni legate allesposizione alle radiazioni ionizzanti nei protocolli di follow - up hanno portato alcuni ricercatori a considerare lopportunit di adottare protocolli cta a bassa dose [ 45 ] , di includere altre modalit di imaging come rm o us [ 7 , 15 , 20 , 27 , 28 , 46 ] o di eliminare scansioni della cta multifasica : sebbene alcuni autori suggeriscano di eliminare la scansione precontrastografica [ 2 , 27 ] , la fase arteriosa [ 37 , 38 ] , o quella tardiva [ 35 ] , noi crediamo che la classica cta trifasica garantisca i risultati migliori . 
infatti , le scansioni diretta e tardiva sono cruciali per riconoscere gli endoleak , mentre la fase arteriosa fondamentale nella pianificazione delleventuale reintervento , specie se endovascolare [ 4 , 27 ]  . 
 [ 16 ] , che raccomandano un follow - up post - evar composto sia da ceus che da cta , noi proponiamo un monitoraggio con cta e ceus appaiate al primo mese post - evar , seguito da ceus a 6 mesi e cta ad 1 anno in assenza di complicanze , o al contrario un controllo pi stretto con ceus in presenza di endoleak di tipo 2 ; il riconoscimento di endoleak di tipo 1 o 3 , cos come lingrandimento della sacca , 1090 radiol med ( 2012 ) 117 : 10791092 fig . 
 as have other authors [ 3 , 32 ] , we suggest ceus surveillance as the primary imaging modality , in patients with collapsed sac ( < 4 cm ) , significant shrinkage ( 5 mm ) , or severe renal dysfunction ( cr > 2.0 mg / dl ) , if necessary , associated with ct scan in the case of expanding sac , suboptimal or uncertain ceus results , endograft position assessment and device integrity and to confirm aneurysm morphology and size . 
 in conclusion , we believe that in patients suitable for us , ceus provides the same results in terms of patient management as three - phase cta performed with a 64 - slice mdct and a tailored protocol with bolus tracking for the arterial phase and a delayed phase of at least 3 m on the other hand , we agree with many authors that cta cannot be completely replaced by other diagnostic modalities in the surveillance of patients after evar , as it provides a more precise evaluation of changes in aneurysm morphology with volumetric analysis [ 47 ] and of graft anchorage and structural integrity [ 7 , 16 , 20 , 23 , 29 , 32 ] , which are early markers of critical events , such as graft migration or sealing defects . 
 come altri autori [ 3 , 32 ] , anche noi suggeriamo ceus come principale metodica di follow - up nei pazienti con collasso ( < 4 cm ) o significativo shrinkage ( 5 mm ) della sacca , nonch nei pazienti con severa insufficienza renale ( cr > 2 , 0 mg / dl ) , valutando lopportunit di procedere a ct ( diretta nel caso di insufficienza renale ) in caso di dubbio o di aumento della sacca , per controllare la posizione e lintegrit del graft e per confermare la morfologia e le dimensioni dellaneurisma . in conclusione noi riteniamo che , nei pazienti anatomicamente adatti , ceus fornisca gli stessi risultati in termini di gestione del paziente rispetto alla cta trifasica eseguita con un apparecchio a 64 strati secondo un protocollo mirato , con timing della fase tardiva ad almeno 3 minuti . 
concordiamo peraltro con molti autori che la cta non possa in questo momento essere del tutto sostituita dalle altre modalit diagnostiche nel monitoraggio dei pazienti trattati con evar , in quanto permette una pi precisa valutazione delle variazioni morfologiche dellaneurisma anche con analisi volumetriche [ 47 ] , degli ancoraggi e dellintegrit strutturale del graft [ 7 , 16 , 20 , 23 , 29 , 32 ] , precoci indicatori di eventi critici come migrazione e difetti di sealing della protesi . 
nieder springer - verlag berlin heidelberg , 2011 issn 0942 - 5373 isbn 978 - 3 - 642 - 16332 - 6 e - isbn 978 - 3 - 642 - 16333 - 3 doi 10.1007 / 978 - 3 - 642 - 16333 - 3 published online : 14 may 2012 springer - verlag 2012 the book decision making in radiation oncology is divided into a two volume set . 
volume one ( not available for review ) addresses in its i - v sections , 17 chapters and 511 pages , palliative treatment , head and neck cancer , breast cancer , tumors of the thorax , cancer of the gastrointestinal tract . 
the second volume in review addresses in its vi - xi sections , 23 chapters and 573 pages , tumors of the genitourinary system , gynecological cancers , lymphomas , tumors of the central nervous system , skin cancer and soft tissue sarcoma , pediatric tumors . the two volumes aim to offer oncologists and radiotherapists updated knowledge on all types of tumours and related conditions , knowledge based on disease management and sound results of properly run clinical trials and research . 
 at the opening of each chapter one will find a very well structured key point list summarizing the most relevant information on what is to be found in the following pages , while the text is kept to a minimum , tables and figures take the lions share . tables and figures are displayed and highlighted in different colours , accordingly throughout the text , offering the reader all possible information on epidemiology , risk factors , histology , diagnosis , staging and prognosis , imaging , spread and recurrence , metastasis , tnm or american joint commission on cancer or other international study group classifications , and treatment ( surgery , radiotherapy , chemotherapy , radio - chemotherapy )  . one peculiarity is the fact that references ( here referred to as sources ) are found in extenso and italics in the text following each relevant item and in smaller case italics , at the tables bottom , here usually listed without single breaks , one after the other , making them difficult to appreciate . 
il primo volume ( non disponibile per la recensione ) tratta nelle sue sezioni i - v , 17 capitoli e 511 pagine : trattamenti palliativi , cancro della testa e del collo , cancro della mammella , tumori del torace e cancro del tratto gastro - enterico . 
il secondo volume , qui recensito , tratta nelle sue sezioni vi - xi , 23 capitoli e 573 pagine : tumori del sistema genito - urinario , tumori ginecologici , linfomi , tumori del sistema nervoso centrale , cancri della pelle e sarcomi delle parti molli e tumori pediatrici . scopo del volume di offrire agli oncologi ed ai radioterapisti informazioni aggiornate su tutti i tipi di tumori e condizioni affini , informazioni e conoscenze basate sul trattamento della malattia e su solidi risultati di ricerca e sperimentazioni cliniche correttamente condotte . 
cademartiri17 1dipartimento di medicina sperimentale , universit di laquila , italy 2dipartimento di scienze radiologiche , oncologiche e anatomo - patologiche , universit sapienza di roma , roma , italy 3istituto di radiologia , diagnostica ed interventistica , universit a . 
avogadro , novara , italy 4dipartimento di radiodiagnostica , apss di trento , trento , italy 5department of radiology and experimental imaging center , san raffaele hospital and vita - salute san raffaele university , milano , italy 6dipartimento di radiologia , ospedale san gennaro , asl napoli 1 centro , napoli , italy 7u.o.c. 
orsola , bologna , italy 10dipartimento di radiologia , universit degli studi di ancona , ancona , italy 11sezione di scienze radiologiche , dipartimento di biopatologia e biotecnologie mediche e forensi , a.o.u.p. 
paolo giaccone , universit degli studi di palermo , italy 12radiologia 1 dai servizi diagnostici e per immagine azienda ospedaliero - universitaria , policlinico di modena , italy 13department of bioimaging and radiological sciences , institute of radiology , a . 
gemelli hospital , catholic university , rome , italy 14catholic university of sacred heart , centro oncologico fiorentino , mri dept . , sesto fiorentino , italy 15dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e terapia radiante della fondazione policlinico universitario tor vergata , roma , italy 16universit degli studi di milano , dipartimento di scienze medico - chirurgiche , servizio di radiologia , irccs policlinico san donato , san donato milanese milano , italy 17imaging cardiovascolare , ospedale giovanni xxiii , monastier di treviso , treviso , italy correspondence to : f . 
min ( department of cardiac imaging , cedars - sinai medical center , los angeles , ca , usa ) received : 6 september 2011 / accepted : 14 september 2011 / published online : 28 june 2012 springer - verlag 2012 abstract cardiac computed tomography ( cct ) has grown as a useful means in different clinical contexts . 
lo sviluppo della tecnologia ha portato ad una progressiva espansione delle indicazioni con una concomitante riduzione della dose di radiazioni 902 radiol med ( 2012 ) 117 : 901938 international scientific societies describing the proper use and clinical indications of cct ; in particular , there are no complete guidelines . 
ancora oggi sono pochi i documenti delle maggiori societ scientifiche internazionali che si esprimono sulle effettive modalit di utilizzo e sulle indicazioni cliniche della cct ; in particolare mancano delle linee guida complete . 
questo documento rispecchia la visione del gruppo di lavoro della sezione di cardio - radiologia della societ italiana di radiologia medica in merito alle indicazioni correnti della cct . parole chiave cct angiografia coronarica a tomografia computerizzata linee guida consenso indicazioni cliniche introduction introduzione computed tomography ( ct ) of the heart and coronary arteries [ i.e. 
the first experiences with this technique go back to 1999 , when a four - slice ct scanner was used ; current technology can exploit devices with as many as 320 slices [ 4 ]  . 
ct equipment that can be used to carry out cardiac investigations is now widely spread throughout the country , whereas scientific evidence regarding this technique has been taking shape in the last few years only [ 1 ]  . 
 the aim of this document is to collate and update stateof - the - art knowledge regarding cct in order to formulate guidelines on the appropriate clinical use of this technique . 
the appropriateness of the use of cct in specific clinical settings is summarised according to the following classification ( table 1 , modified from [ 11 ] ) : class i : provides diagnostic information of clinical relevance and is appropriate ; may be used as the imaging modality of choice ; class ii : provides diagnostic information of clinical relevance ; other imaging modalities may provide similar information ; class iii : provides diagnostic information but is infrequently used because information from other imaging techniques is usually adequate ; class inv : potentially useful , but still investigational . this classification is neither an equivalent nor a replacement of other classifications used in documents or guidelines form the american heart association ( aha ) , amerila tomografia computerizzata del cuore e delle coronarie ( cct ) una delle metodiche di indagine non invasiva del cuore e delle coronarie di pi recente introduzione [ 13 ]  . 
 le prime esperienze risalgono al 1999 con apparecchiature di tomografia computerizzata ( tc ) a 4 strati mentre la tecnologia corrente pu sfruttare apparecchiature fino a 320 strati [ 4 ]  . 
attualmente non esistono delle vere e proprie linee guida per lutilizzo clinico della cct ma piuttosto documenti di appropriatezza , raccomandazioni di utilizzo e documenti condivisi [ 510 ]  . 
 lo scopo del presente documento quello di recepire ed aggiornare lo stato dellarte delle conoscenze in ambito di cct al fine di formulare delle linee di indirizzo per lutilizzo clinico appropriato della metodica . 
the combination of fast rotation of the tube - detector complex and multislice acquisition is the starting point for cardiac applications [ 1 , 3 , 12 , 13 ]  . 
more specifically , hardware requirements for cct imaging are ( table 2 ) : high temporal resolution and synchronisation with phases of the cardiac cycle ; the fact that the heart beats means that the method must be able to acquire images in a sufficiently short time to minimise or avoid all movement artefacts completely . 
furthermore , in order to avoid these artefacts , image scanning and reconstruction must be synchronised with the best phase of the cardiac cycle ; that is , the one with the least residual movement . high spatial resolution : the structures under investigation , in particular , the coronary arteries , have a small diameter ( < 5 mm )  . 
the questa classificazione non sostitutiva o analoga ad altre utilizzate nei documenti di appropriatezza o nelle linee guida dellamerica heart association ( aha ) / american college of cardiology ( acc ) / european society of cardiology ( esc ) / society of cardiovascular computed tomography ( scct )  . tecnica e requisiti hardware le componenti pi importanti di unapparecchiatura tc sono il tubo radiogeno ed il sistema dei detettori . 
la combinazione di un tempo di rotazione veloce del complesso tubo detettore e lacquisizione multistrato il punto di partenza per le applicazioni cardiologiche [ 1 , 3 , 12 , 13 ]  . 
in particolare , i requisiti hardware della tc per limaging cardiologico sono ( tabella 2 ) : elevata risoluzione temporale e sincronizzazione con le fasi del ciclo cardiaco : il battito cardiaco richiede che la metodica sia in grado di acquisire le immagini in un tempo sufficiente per limitare al minimo o evitare del tutto gli artefatti da movimento . 
inoltre , per poter evitare tali artefatti la scansione / ricostruzione delle immagini dovr essere sincronizzata con la fase del ciclo cardiaco ideale , ossia quella caratterizzata dal minor movimento residuo ; elevata risoluzione spaziale : le strutture oggetto di indagine ed in particolar modo le coronarie sono caratterizzate da calibro ridotto ( < 5 mm )  . 
 slowing the heart rate produces a longer diastolic interval , which translates into a longer duration of end - diastole , the period in which the heart and coronary arteries are almost motionless . 
although cct can provide diagnostic information when performed at higher heart rates , movement artefacts progressively reduce the number of segments that can be visualised correctly [ 14 ]  . 
the second criterion is applied elevata risoluzione di contrasto : la distinzione tra le strutture oggetto di studio ( per es . , lume vascolare , cavit ventricolari , muscolo cardiaco , tessuti molli adiacenti ) richiede una risoluzione di contrasto adeguata alla distinzione delle strutture stesse ed alla loro misurazione ; elevata velocit di scansione : la velocit di scansione diviene importante per il fatto che il movimento respiratorio determina artefatti da movimento . 
 inappropriate breathing during scanning reduces the quality and quantity of the information acquired . exclusion criteria concern technical aspects related to heart rate , ionising radiation exposure issues and contrast agent administration . 
la bradicardizzazione permette di ottenere un intervallo diastolico pi lungo , che si traduce con un aumento della durata della tele - diastole , momento in cui il cuore e le arterie coronarie risultano quasi prive di movimento . 
anche se la cct pu essere diagnostica a frequenze cardiache pi elevate , gli artefatti da movimento riducono progressivamente il numero di segmenti che possono essere visualizzati correttamente [ 14 ]  . 
la respirazione non adeguata del paziente durante la scansione riduce la qualit e la quantit delle informazioni acquisite . i criteri di esclusione riguardano gli aspetti tecnici inerenti la frequenza cardiaca , gli aspetti radio - protezionistici e gli aspetti relativi alla somministrazione del mezzo di contrasto . 
i pazienti con frequenza cardiaca ( fc ) 65 bpm , allergia nota al mezzo di contrasto iodato , insufficienza renale 906 radiol med ( 2012 ) 117 : 901938 tial resolution ( thin collimation ) , high temporal resolution ( fast gantry rotation ) and the least possible exposure to ionising radiation [ prospective modulation of tube current synchronised to the electrocardiogram ( ecg ) , etc . ] compatible with a good signal - to - noise ratio ( snr )  . 
technical details of the scanning parameters are described in the specific literature [ 1 , 3 , 12 , 13 ]  . ( creatinina sierica > 140 mmol / l ) , gravidanza , insufficienza respiratoria , stato clinico instabile e scompenso cardiaco di grado severo vengono normalmente esclusi dallo studio mediante cct [ 8 ]  . 
per la valutazione del calcio coronarico i criteri di esclusione relativi alla frequenza cardiaca ed al mezzo di contrasto non si applicano . synchronisation with the cardiac cycle and image reconstruction image acquisition in cct scanning must be synchronised to the heart beat and , ideally , to the phase of the cardiac cycle with the least residual movement [ 1 ]  . 
in the former case , scanning is continuous low pitch ( 0.150.4 ) spiral scanning , and data can be reconstructed in any phase of the cardiac cycle , shifting the initial point of the image reconstruction relative to the r wave . 
retrospective cardiac gating is more flexible and enables optimisation of the reconstruction time windows at the cost of an averagely higher radiation dose ; prospective cardiac triggering is less flexible but allows radiation dose to be reduced significantly . phases of the cardiac cycle in which images are usually acquired / reconstructed are end - diastole ( 6080% of the rr interval ; - 300 / - 400 ms before the next r wave ) and end - systole , when available ( 2040% of the rr interval ; + 175 / + 325 ms after the preceding r wave )  . 
the field of view should be as small as possible while including the entire heart in order to fully exploit the image matrix , which is constant ( 512512 pixels )  . 
when the coronary arteries are highly calcified or contain stents , higher convolution filters , even though they increase image noise , improve vessel wall , stent structure , and internal lumen visualisation . image evaluation a standardised technique to evaluate images collected during a cct study is lacking . 
evalscansione cct il protocollo ideale per la cct quello che permette unelevata risoluzione spaziale ( collimazione pi sottile ) , unelevata risoluzione temporale ( pi veloce rotazione del sistema tubo - detettore ) , la minore esposizione a radiazioni ionizzanti ( modulazione prospettica della corrente del tubo sincronizzata allelettrocardiogramma , ecc . ) compatibilmente con un buon rapporto segnale / rumore . 
per i dettagli tecnici sui parametri di scansione si rimanda alla letteratura specifica [ 1 , 3 , 12 , 13 ]  . sincronizzazione con il ciclo cardiaco e ricostruzione delle immagini lacquisizione delle immagini nella scansione di cct deve essere sincronizzata al battito cardiaco e possibilmente alla fase del ciclo cardiaco caratterizzata dal minor movimento residuo [ 1 ]  . 
nel primo caso la scansione spirale continua a basso pitch ( 0 , 150 , 4 ) ed i dati possono essere ricostruiti in qualunque fase del ciclo cardiaco , spostando il punto dinizio della ricostruzione delle immagini relativamente allonda r . 
 il gating cardiaco retrospettivo pi flessibile e consente di ottimizzare meglio le finestre temporali di ricostruzione a prezzo di una dose di radiazioni mediamente superiore ; il triggering cardiaco prospettico meno flessibile ma consente di ridurre in modo significativo la dose di radiazioni . generalmente , le fasi del ciclo cardiaco nelle quali vengono acquisite / ricostruite le immagini sono la fase telediastolica ( 60%80% dellintervallo rr ; - 300 / - 400 ms prima della successiva onda r ) e la fase tele - sistolica quando disponibile ( 20%40% dellintervallo rr ; + 175 / + 325 ms dopo la precedente onda r )  . 
in particolare , lo spessore di strato effettivo pu essere pari o lievemente pi ampio della minima collimazione possibile in modo tale da migliorare il rapporto segnale / rumore dellimmagine . 
images are evaluated on an axial data set and then reconstructed by multiplanar reconstruction ( mpr ) , maximum intensity projection ( mip ) and volume rendering ( vr )  . 
with 64 - slice equipment , the average effective dose is about 12 ( range 818 ) msv in a period in which the prospective technique had already been introduced [ 16 ]  . 
other techniques and acquisition modes associated with improvements in the reconstruction phase have enabled progressive dose decreases ( table 3 ) [ 17 , 18 ]  . campo di vista dovrebbe essere quanto pi piccolo possibile includendovi lintero cuore , in modo tale da sfruttare pienamente la matrice dellimmagine che costante ( 512512 pixel )  . 
quando le arterie coronarie sono molto calcifiche o sono presenti degli stent , i filtri di convoluzione pi alti , anche se aumentano il rumore dellimmagine , migliorano la visualizzazione della parete del vaso o della struttura dello stent e del lume al suo interno . valutazione dellimmagine la valutazione delle immagini di unindagine cct non ancora effettuata mediante una tecnica standardizzata . 
le immagini vengono valutate sul dataset assiale , quindi ricostruite mediante ricostruzioni multiplanari ( mpr ) , maximum intensity projections ( mip ) e volume rendering ( vr )  . 
numerous studies considered particular subpopulations with different risk profiles , different symptoms and different clinical characteristics [ 1824 ]  . validation of the prognostic value of cct also began recently [ 2527 ]  . 
various studies show that risk stratification of all - cause mortality and cardiovascular - disease mortality based on cct findings is independent from conventional risk stratification based on cardiovascular risk factors , coronary calcium score ( cs ) and results of stress tests [ 2833 ]  . radiol med ( 2012 ) 117 : 901938 nale , sia manualmente che in modo semi - automatico ( mpr curvate ) [ 15 ]  . strategie di riduzione della dose di radiazioni la tecnica di riferimento per lesecuzione della cct quella spirale a basso pitch ( 0 , 20 , 35 )  . 
con le apparecchiature a 64 strati la dose efficace media di circa 12 msv ( range 818 msv ) in una fase nella quale la tecnica prospettica gi stata introdotta [ 16 ]  . 
 altre tecniche e modalit di acquisizione associate a miglioramenti in fase di ricostruzione hanno consentito una progressiva riduzione della dose ( tabella 3 ) [ 17 , 18 ]  . congenital heart diseases valore diagnostico e prognostico the role of cct in diagnosing congenital heart diseases ( chd ) is currently being defined , particularly considering the important roles of ecg and magnetic resonance imaging ( mri ) in this field ( table 4 )  . 
furthermore , cct provides only limited functional information ( none concerning assessment and quantification of blood flow across valves or through prosthetic conduits , or arterial blood flow for the calculation of shunts )  . 
in contrast , left ventricular function can be studied , albeit at the cost of higher radiation doses ( techniques to reduce the dose do not facilitate precise quantification of cardiac volumes )  . 
new ct technology ( in particular , dualsource ct ) enables the use of paediatric scan protocols at 80 kv and 10 mas / kg , which employ significantly lower doses ( < 1 msv ) and yet provide excellent diagnostic images and reconstructions [ 3436 ]  . 
 on the basis of the foregoing , it is reasonable to consider the use of cct in the morphological study of chd , particularly in childhood and in patients in an intensive care unit , in whom the need to use anaesthesia and , more generally , the unfavourable logistics of mri limit the feasibility of this latter imaging technique . 
 cct has various advantages over other imaging techniques when applied to chd : it is fast and can be used to investigate paediatric patients with only mild sedation ( as for perinatal echocardiography ) ; in generale , la cct caratterizzata da una elevata sensibilit e da un elevato valore predittivo negativo nella rilevazione delle stenosi coronariche significative ( per esempio , riduzione del calibro del lume 50% ) nei pazienti con sospetta malattia coronarica ( cad )  . 
molteplici studi hanno preso in considerazione sotto - popolazioni particolari di pazienti caratterizzate da differenti profili di rischio , differenti sintomi , differenti caratteristiche cliniche [ 1824 ]  . di recente iniziata anche la validazione del valore prognostico della cct [ 2527 ]  . 
molteplici studi hanno evidenziato come la stratificazione del rischio di morte per tutte le cause e per eventi cardiovascolari basata sui reperti ottenuti alla cct sia indipendente rispetto alla stratificazione convenzionale basata sui fattori di rischio cardiovascolari , al calcium score coronarico ( cs ) ed ai test provocativi [ 2833 ]  . cardiopatie congenite il ruolo della cct nella diagnostica delle cardiopatie congenite ( cc ) in fase di definizione , soprattutto considerando il ruolo importante dellecocardiografia e della risonanza magnetica ( rm ) ( tabella 4 )  . 
inoltre la cct , analogamente al cateterismo cardiaco , limitata dallimpiego di radiazioni ionizzanti in una popolazione pediatrica o di giovani adulti che necessitano di ripetute indagini di follow - up e sono maggiormente suscettibili al danno da radiazioni . 
lo studio della funzione ventricolare invece possibile , a prezzo di una maggiore dose di radiazioni ( le tecniche di riduzione della dose non favoriscono una precisa quantificazione dei volumi cardiaci )  . 
le nuove tecnologie tc ( in particolare la tc a doppia sorgente ) consentono lapplicazione di protocolli pediatrici di scansione con protocolli a 80 kv e 10 mas / kg caratterizzati da significativa riduzione della dose ed immagini e ricostruzioni esaustive dal punto di vista diagnostico ( < 1 msv ) [ 3436 ]  . 
 su queste basi ragionevole considerare lutilizzo della cct nello studio morfologico delle cc , soprattutto nellet infantile e nei pazienti in terapia intensiva , dove la necessit dellanestesia e pi in generale la logistica pi sfavorevole della rm , ne limitano la disponibilit . 
 in clinical practice , the use of cct should be reserved to cases in which the ecg is not conclusive and mri cannot be used due to an absolute contraindication or is unavailable . 
 one specific indication in this context is the study of right ventricular systemic function in patients with a pacemaker , as the morphology renders it poorly evaluable by ecg and otherwise evaluable only by haemodynamic investigations [ 38 , 39 ]  . 
 coronary vessel anomalies coronary vessel anomalies are rare ( 0.35.6% at coronarography and 0.30.5% in postmortem series ) and usually asymptomatic , with the exception of some malignant variants [ 4042 ]  . 
the course and anatomical relations of the coronary vessels are also important to define prior to possible repair surgery or interventional procedures , such as percutaneous implantation of pulmonary valves or pulmonary stents [ 44 ]  . congenital anomalies of the aorta congenital anomalies of the heart can be well evaluated with ct without cardiosynchronisation , given the high scanning speed , the possibility of reducing the dose in small patients and the potential for studying the trachea , bronchi , oesophagus and relationships of these organs with extracardiac vascular structures . 
the main indication for cct in the postoperative follow - up of coarctation surgery is to evaluate aortic stents ( stent fracture , correct placement , in - stent restenosis ) [ 45 , 46 ]  . 
cct also allows excellent visualisation of the systemic - pulmonary collateral vessels , which are important to identify in the preoperative study of many chd [ 47 ]  . anomalous venous return cct , even without cardiac synchronisation , can be used to evaluate the presence , diameter and course of pulmonary veins . 
the presence of partial anomalous venous return of the right superior pulmonary vein into the superior vena cava can change a patients diagnosis , also in relation to alle cc ha alcuni vantaggi rispetto alle altre tecniche di imaging : veloce e permette di effettuare indagini su pazienti pediatrici con una blanda sedazione ( analogamente allecocardiografia perinatale ) ; ha una elevata risoluzione spaziale che la rende adatta alla valutazione delle diramazioni periferiche delle arterie polmonari o delle arterie coronarie , con possibilit di ricostruzioni multiplanari bie tri - dimensionali ; permette una valutazione panoramica del torace che consente di valutare eventuali anomalie associate ( non solo cardiovascolari ma anche parenchimali polmonari , tracheo - bronchiali ed esofagee ) ; meno influenzata ( se non per gli artefatti regionali ) dalla presenza di protesi e device metallici - elettronici ( stimolatori , pace - maker , defibrillatori impiantabili , stent , clips e spirali metalliche ) ; meno limitata dalla claustrofobia o pi in generale dalla scarsa compliance dei pazienti . 
 la cct unindagine ottimale per lo studio morfologico pre - operatorio e post - operatorio delle cc , in particolare delle anomalie complesse e per la valutazione delle anomalie vascolari extracardiache [ 37 ]  . 
 limpiego nella pratica clinica della cct andrebbe riservato ai casi in cui lecocardiogramma non ha unadeguata finestra acustica e la rm non utilizzabile ( pazienti claustrofobici , portatori di pace - maker o defibrillatore ) o logisticamente non disponibile . 
unindicazione specifica importante in tal senso lo studio della funzione del ventricolo destro sistemico nei portatori di pace - maker , po co valutabile dallecocardiografia ed altrimenti studia bile solo con esame emodinamico [ 38 , 39 ]  . 
 anomalie coronariche le anomalie coronariche sono rare ( 0 , 3%5 , 6% alla coronarografia e 0 , 3%0 , 5% in serie autoptiche ) e generalmente asintomatiche , ad eccezione di alcune varianti maligne [ 4042 ]  . 
la prevalenza di anomalie delle coronarie maggiore nelle cardiopatie congenite ( tetralogia di fallot , trasposizione dei grossi vasi ) e rappresenta un possibile fattore di rischio quoad valetudinem o quoad vitam [ 43 ]  . 
anche il decorso ed i rapporti anatomici delle coronarie con alcune strutture cardiache sono importanti da definire in previsione di atti chirurgici riparativi o procedure interventistiche come il posizionamento di valvole polmonari percutanee o di stent polmonari [ 44 ]  . radiol med ( 2012 ) 117 : 901938 identifying any associated abnormalities , such as venous sinus defects . 
in scimitar syndrome and in total anomalous pulmonary venous return , cct allows correct evaluation of the outlets ( above or below the diaphragm ) and any involvement of the portal syste primary prevention coronary calcium score cs is widely used in north america and asia to stratify cardiovascular risk ( table 5 )  . 
the presence of calcifications represents a stage in the evolution of an atherosclerotic plaque and enables an estimate to be made of coronary artery atherosclerosis and the risk of stenosis and cardiovascular events [ 48 ]  . 
the risk ratio or relative risk ( rr ) for cardiovascular events or myocardial infarction in the following 35 years in asymptomatic patients is proportional to the score obtained ( cs 0100 , rr 1.9 ; cs 100400 , rr 4.3 ; cs 4001 , 000 , rr 7.2 ; cs > 1 , 000 , rr 10.8 ) [ 50 ]  . 
this group of patients , who represent 40% of the population , can be partly reclassified as high anomalie congenite dellaorta le anomalie congenite dellaorta sono ben valutabili mediante tc ( senza cardiosincronizzazione ) in relazione alla elevata velocit di scansione , alla possibilit di riduzione della dose nei pazienti pi piccoli e alla possibilit di studiare le strutture tracheo - bronchiali , lesofago ed i rapporti tra queste e le strutture vascolari extracardiache . 
lindicazione principale della cct nel follow - up post - operatorio delle coartazioni la valutazione degli stent aortici ( fratture dello stent , corretto posizionamento , stenosi intra - stent ) [ 45 , 46 ]  . 
la cct consente anche unottimale visualizzazione delle collaterali sistemico - polmonari , importanti da segnalare nello studio pre - operatorio di molte cc [ 47 ]  . ritorni venosi anomali la cct , anche senza cardiosincronizzazione , permette di valutare presenza , calibro , decorso delle vene polmonari . 
 la presenza di un ritorno venoso anomalo parziale della vena polmonare superiore destra in cava superiore pu modificare lindirizzo diagnostico del paziente anche in relazione alla identificazione di eventuali anomalie associate quali i difetti del seno venoso . 
 table 5 cardiac computed tomography in primary prevention calcium score prevenzione primaria indication risk stratification in asymptomatic patients without known cad low risk intermediate risk high risk monitoring pharmacological treatments cad , coronary artery disease tabella 5 la tomografia computerizzata del cuore nella prevenzione primaria . 
calcium score indicazione stratificazione del rischio in pazienti asintomatici senza cad nota rischio basso rischio intermedio rischio alto monitoraggio terapie farmacologiche cad , malattia coronarica class classe calcium score coronarico il cs coronarico un test ampiamente utilizzato in nord america ed in asia per la stratificazione del rischio cardiovascolare ( tabella 5 )  . 
il risk ratio ( rr ) di eventi cardiovascolari o infarti miocardici nei 35 anni successivi in pazienti asintomatici proporzionale al punteggio ottenuto ( cs 0100 , rr 1 , 9 ; cs 100400 , rr 4 , 3 ; cs 4001000 , rr 7 , 2 ; cs > 1000 , rr 10 , 8 ) [ 50 ]  . 
there is no evidence that the value of the cs changes the risk class significantly in asymptomatic individuals with a high probability of disease ( > 20% ) : according to the current guidelines , these patients are candidates for pharmacological treatment in any case . 
there are insufficient data on whether it is possible to modify the progression of coronary calcification through medical treatment and whether this would improve the patients outcome [ 50 ]  . cardiac computed tomography il 40% della popolazione , pu essere in parte riclassificato nel gruppo ad elevato rischio , con conseguente modificazione della gestione terapeutica [ 51 ]  . 
non ci sono evidenze che i valori di cs modifichino in maniera significativa la classe di rischio in soggetti asintomatici con alta probabilit di malattia ( > 20% ) , poich secondo le attuali linee guida questi individui sono , comunque , candidati a terapia farmacologica . 
cct can be used to assess some characteristics of the vulnerability of plaques , such as positive remodelling , eccentricity and noncalcified components , which are associated with a higher risk of cardiovascular events [ 29 , 52 ]  . 
 qualitative and quantitative evaluation of the atherosclerotic burden of coronary vessels is an interesting application in the context of noninvasive estimation of cardiovascular risk and its changes during pharmacological treatment , although it should still be considered an experimental approach [ 51 , 53 , 54 ]  . 
in fact , there is only limited information on the la cct consente di evidenziare il calcio coronarico e le componenti non calcifiche della placca aterosclerotica coronarica ( tabella 6 )  . 
la cct permette lidentificazione di alcune caratteristiche di vulnerabilit , quali il rimodellamento positivo , leccentricit e le componenti non calcifiche , che si associano maggiormente ad eventi cardiovascolari [ 29 , 52 ]  . 
la valutazione qualitativa e quantitativa del carico aterosclerotico coronarico unapplicazione interessante per lapproccio non invasivo alla stima del rischio cardiovascolare ed alle modificazioni in corso di table 6 cardiac computed tomography ( cct ) and primary prevention indication risk stratification in asymptomatic patients without known cad imaging of atherosclerotic plaques ( evaluation and monitoring ) follow - up of patients who have received a heart transplant cct following cs estimation in patients with agatston > 400 preoperative evaluation of coronary vessels in patients to undergo noncoronary cardiac surgery preoperative risk evaluation in patients without cardiac symptoms undergoing noncardiac surgery cad , coronary artery disease ; cs , calcium score tabella 6 la tomografia computerizzata e la prevenzione primaria indicazione class classe stratificazione del rischio in pazienti asintomatici senza malattia coronarica nota imaging placca aterosclerotica ( valutazione e monitoraggio ) follow - up in pazienti sottoposti a trapianto cardiaco cct successiva allesecuzione di calcium score in pazienti con agatston > 400 valutazione preoperatoria delle coronarie in previsione di chirurgia cardiaca non coronarica valutazione del rischio preoperatorio in pazienti da sottoporre a chirurgia non cardiaca senza sintomatologia cardiaca cct , tomografia computerizzata del cuore radiol med ( 2012 ) 117 : 901938 role of cct in risk evaluation in asymptomatic individuals and the possible prognostic implications [ 5557 ]  . 
it seems reasonable to foresee the use of cct in asymptomatic subgroups at high risk ( in patients with a family history of premature death due to cad , hypercholesterolaemia or multiple risk factors and in diabetics > 40 years ) in the setting of primary prevention programmes in order to diagnose coronary atherosclerosis early [ 51 , 58 , 59 ]  . 
cct provides a more complete evaluation of coronary atherosclerosis than that afforded by the cs , but there are as yet no data on the usefulness of integrating the cs ( especially when > 400 ) with cct in asymptomatic patients . cct has recently been proposed as a noninvasive test to exclude cad in specific classes of asymptomatic patients at high risk who must selectively undergo conventional angiography , such as patients being followed up after heart transplantation or who are candidates for elective noncoronary cardiac surgery ( valve replacements , aortic aneurysms , tumours , percutaneous closure of defects of the interatrial or interventricular septum ) or vascular surgery . 
these uses are more appropriate in patients with an intermediate pretest probability [ 8 , 6062 ]  . suspected coronary artery disease the main use of cct is the diagnosis / exclusion of obstructive cad [ 1 , 8 ] , for which it has a high sensitivity ( > 90% ) and a high npv ( > 98% ) ( table 7 ) [ 1 , 8 ]  . 
there are now some documents from the esc and american cardiology societies , aha and acc that define the main fields of cct application in suspected cad [ 510 ]  . 
when the result of an exercise test is unclear , it is appropriate to terapia farmacologica , ma deve essere considerata ancora in fase sperimentale [ 51 , 53 , 54 ]  . 
appare ragionevole prospettare limpiego della cct in sottogruppi asintomatici ad elevato rischio ( in pazienti con storia familiare di morte prematura per malattia coronarica , ipercolesterolemia o fattori di rischio multipli e nei diabetici con et superiore ai 40 anni ) nellambito di programmi di prevenzione primaria per la diagnosi precoce dellaterosclerosi coronarica [ 51 , 58 , 59 ]  . 
 la cct fornisce una valutazione dellaterosclerosi coronarica pi completa del cs , ma non esistono ancora dati in letteratura circa lopportunit di integrare il cs ( specie se > 400 ) con la cct nei pazienti asintomatici . recentemente la cct stata proposta anche come test non invasivo per escludere la malattia coronarica in specifiche classi di pazienti asintomatici ad alto rischio , che selettivamente debbano eseguire uno studio angiografico convenzionale , quali i pazienti in follow - up dopo trapianto cardiaco o da sottoporre in elezione ad interventi cardiochirugici non coronarici ( sostituzioni valvolari , aneurismi aortici , tumori , chiusura percutanea dei difetti del setto inter - atriale o interventricolare ) o di chirurgia vascolare . 
 tali applicazioni risultano pi appropriate nei pazienti con probabilit pre - test intermedia [ 8 , 6062 ]  . malattia coronarica sospetta la principale applicazione della cct consiste nella diagnosi / esclusione di coronaropatia ostruttiva [ 1 , 8 ]  . 
la cct caratterizzata da una elevata sensibilit ( > 90% ) ed un elevato valore predittivo negativo ( > 98% ) ( tabella 7 ) [ 1 , 8 ]  . 
 la cct pu quindi rappresentare uno strumento elettivo per lesclusione di malattia coronarica ( cad ) ed caratterizzata da molti vantaggi ed alcuni svantaggi rispetto alle metodiche non invasive basate sullinducibilit dellischemia e rispetto alla cag [ 1 ]  . 
sono ormai disponibili alcuni documenti della societ europea di cardiologia ( european society of cardiology , esc ) , delle societ americane di cardiologia ( america heart association , aha , ed american college of cardiology , acc ) che definiscono i campi di applicazione principali della cct nella cad sospetta [ 510 ]  . 
in generale , le situazioni cliniche nelle quali si ritiene opportuno o appropriato effettuare una cct per sospetta malattia coronarica consistono in quelle situazioni nelle quali il paziente a rischio intermedio abbia eseguito test provocativi dubbi o non diagnostici ( per esempio , stress ecg non massimale ) o quelle nelle quali i test provocativi non siano fattibili [ 1 , 8 ]  . 
this becomes all the more appropriate when the patient is in the intermediate category of cardiovascular risk [ 1 , 8 , 24 ]  . other clinical situations in which cct can be considered appropriate are : the symptomatic patient at intermediate risk who has or has not undergone a stress test previously ; the symptomatic patient at intermediate risk who has undergone two stress tests with discordant results ; the symptomatic patient who continues to have symptoms after a negative stress test [ 1 , 8 ]  . however , for clinical purposes , information concerning obstructive disease detected by cct must always be integrated with data on inducible ischaemia [ 1 , 8 , 24 ]  . broadening the indications for cct derives from growing evidence on the diagnostic potential of this method , together with the fact that there are now techniques to reduce the radiation dose [ 1 , 8 , 63 ]  . 
cct can be used in this context to rule out the presence of obstructive cad . acute chest pain patients with acute chest pain account for 510% of patients who present to emergency departments ; of these patients , 70 - 80% are classified as having nonanginal pain , 78% as having acute coronary syndrome and up to 78% as having non - selevation myocardial infarction ( nstemi ) and / or unstable angina ( ua ) [ 64 , 65 ]  . 
conventional strategies are based on a clinical assessment ( including stratification of patient cardiovascular risk ) , evaluation of the ecg and levels of biohumoural markers [ 6466 ]  . 
la prassi indica il test da sforzo ( vale a dire , ecg da sforzo ) come primo test provocativo dopo lelettrocardiogramma di base ed eventualmente lecocardiografia [ 1 , 8 ]  . 
questa evenienza diviene tanto pi appropriata quanto pi il rischio cardiovascolare del paziente si trovi allinterno della categoria intermedia [ 1 , 8 , 24 ]  . altre situazioni cliniche nelle quali la cct pu essere considerata appropriata sono : il paziente sintomatico a rischio intermedio con o senza un test provocativo effettuato in precedenza ; il paziente sintomatico a rischio intermedio che abbia effettuato due test provocativi dal risultato discordante ; il paziente sintomatico che continua ad avere sintomi dopo un test provocativo negativo [ 1 , 8 ]  . linformazione relativa alla malattia ostruttiva rilevata mediante cct deve sempre e comunque essere integrata ai fini clinici dal dato sullischemia inducibile [ 1 , 8 , 24 ]  . lallargamento delle indicazioni della cct deriva dalla crescente evidenza sulle potenzialit diagnostiche abbinata allimplementazione di tecniche di riduzione della dose di radiazioni [ 1 , 8 , 63 ]  . 
la cct in questo contesto pu essere utilizzata per escludere leffettiva presenza di cad ostruttiva . dolore toracico acuto il dolore toracico acuto rappresenta il 5%10% dei pazienti che accedono al pronto soccorso ; di questi il 70%80% vengono classificati come dolore non anginoso , il 7%8% sono classificati come sindrome coronarica acuta e fino al 7%8% vengono classificati come infarto miocardico senza sopra - elevazione del tratto st ( nstemi ) e / o angina insta916 radiol med ( 2012 ) 117 : 901938 they are simple , quick , reliable and capable of detecting or excluding significant cad and other major cardiothoracic causes of chest paa test with these characteristics would reduce costs , decrease errors / responsibilities and could also increase patient satisfaction [ 6466 ]  . 
the optimal prognostic value of cct for excluding significant disease and events gives this method an excellent safety profile [ 67 ]  . in the setting of acute chest pain , cct can be considered one of the diagnostic options when ecg and biohumoural findings are equivocal [ 68 ]  . 
in the case of negative ecg and biohumoural results , cct could be used to reach a diagnosis more quickly and thereby lead to earlier discharge from hospital , with a consequent reduction in costs . known coronary disease indications and evaluation of patients with known cad are presented in table 8 . after percutaneous transluminal angioplasty / stenting it is more difficult to evaluate coronary stents by cct than it is to evaluate normal coronary segments in the absence of stents , independently from the scanner generation , because of at least three types of artefacts : movement , beam hardening and partial volume effect [ 6975 ]  . 
when evaluating a patient with a coronary stent with a diameter 3 mm , the clinical presentation of which suggests a low to intermediate probability of restenosis , cct could be a reasonable alternative to invasive coronary angiography to exclude the presence of significant disease . 
in particular , cct reevaluation of stents of the common trunk is a valid alternative to coronary angiography . after coronary artery bypass grafting there are fewer problems with cct of coronary vein bypasses than with the native coronary circulation because of the larger calibre of these veins ( 34 mm ) , their lesser mobility and the lower prevalence of vessel wall calcification . 
 the evaluation of arterial bypasses can be more complex , both because of their smaller calibre ( 12 mm ) and because of the surgical clips along the graft pathway . 
moreover , adequate analysis of the distal anastomosis of the bypass is more difficult and complex than assessing both patency and stenoses of the bypass body bebile ( ua ) [ 64 , 65 ]  . 
nel contesto della sindrome coronarica con sopra - elevazione del tratto st la cct non ha un ruolo significativo . la distinzione clinica tra dolore toracico non anginoso e nstemi / ua non sempre chiara , e questa una popolazione nella quale le strategie di esclusione ( rule - out ) possono risultare pi efficaci . 
i requisiti per ulteriori test sono : semplice e veloce , affidabile , capacit di rilevare e / o escludere cad significativa e altre cause cardio - toraciche maggiori di dolore toracico . 
il valore prognostico ottimale della metodica per lesclusione di malattia significativa e di eventi conferisce alla metodica un ottimo profilo di sicurezza [ 67 ]  . la cct nel contesto del dolore toracico acuto pu essere considerata tra le opzioni diagnostiche quando i reperti elettrocardiografici e bioumorali risultino equivoci [ 68 ]  . 
 nel caso di reperti elettrocardiografici e bioumorali negativi la cct potrebbe essere utilizzata per accelerare la fase diagnostica e portare ad una pi precoce dimissione con conseguente riduzione dei costi . malattia coronarica nota indicazioni terapeutiche e valutazioni sul paziente con malattia coronarica nota sono presentate nella tabella 8 . post - angioplastica percutanea / stent la valutazione degli stent coronarici mediante cct risulta pi difficoltosa della valutazione dei normali segmenti coronarici in assenza di stent , indipendentemente dalla generazione degli scanner , per leffetto di almeno tre differenti tipologie di artefatti : da movimento , da indurimento del fascio e di volume parziale [ 6975 ]  . 
 it is essential that four main aspects are considered during noninvasive cct evaluation of coronary bypasses : bypass patency and the smoothness of its walls ; presence of stenoses along the bypass body ; patency and appearance of the proximal anastomosis ( origin ) and of the distal anastomosis or anastomoses ; presence of significant stenoses in the native coronary circulation , both distal to the bypass anastomoses and in coronary vessels that have not been bypassed . 
in particolare , la rivalutazione degli stent sul tronco comune costituisce una alternativa valida alla coronarografia convenzionale . post - bypass coronarico la cct nei bypass coronarici venosi pone minori problematiche rispetto allo studio del circolo coronarico nativo , sia per il loro maggior calibro ( 34 mm ) e la minore mobilit rispetto alle coronarie native , che per la minor prevalenza di calcificazioni parietali . 
la valutazione dei bypass arteriosi pu invece risultare pi complessa , sia per il minor calibro ( 12 mm ) che per la presenza di clip chirurgiche lungo il decorso del gra 918 radiol med ( 2012 ) 117 : 901938 occlusion [ 7682 ]  . 
if severe stenoses are considered together with occlusions , sensitivity is 98% , specificity 97% , positive likelihood ratio is > 10 and negative likelihood ratio is 0.02 , indicating that cct is a powerful test for confirming or ruling out with a high degree of confidence the presence of bypass disease in patients with an intermediate pretest probability of disease [ 7682 ]  . 
native coronary circulation evaluation is more difficult because of the smaller vessel diameter and higher prevalence of calcifications in these vessels than in bypasses , with the overall diagnostic accuracy being lower than that in patients without bypasses . 
 after myocardial infarction some preclinical and clinical studies demonstrate that cct can be used to evaluate myocardial viability through a delayed enhancement technique , as with mri [ 8389 ]  . 
 perfusion defects in chronic , subacute and acute myocardial infarction can be observed during the first passage of the contrast bolus ( early diffusion defect ) and can also be shown with greater precision in a later phase ( 515 min after contrast administration )  . 
as cct can be used to study the coronary circulation and subsequently evaluate , through delayed enhancement , the myocardium , it could also be used as a single - shot imaging method to determine whether there is an underlying ischaemic aetiology of any left ventricular dysfunction , in the manner in which mri can integrate conventional coronary angiography studies [ 87 ]  . 
although clinical trials carried out in small samples of patients show promising results , mri remains the noninvasive reference method for evaluating the extent of postischaemic , nonviable myocardiupatients with absolute contraindication to mri could selectively undergo cct . laccuratezza diagnostica della cct riportata in letteratura nella valutazione delle stenosi dei bypass coronarici leggermente inferiore a quella della valutazione delle occlusioni , mentre ladeguata analisi dellanastomosi distale del bypass risulta essere pi difficoltosa e complessa della valutazione sia della perviet che delle stenosi del corpo del bypass a causa della frequente presenza di clip e / o calcificazioni a tale livello e per la maggior mobilit del tratto distale del bypass , prossimo in tale sede al miocardio [ 7682 ]  . 
 la valutazione non invasiva dei bypass coronarici con cct deve obbligatoriamente comprendere lanalisi di 4 principali differenti aspetti : la perviet e la regolarit parietale del bypass , la presenza di stenosi lungo il corpo del bypass ; la perviet e laspetto dellanastomosi prossimale ; origine della / e anastomosi distale / i del bypass ; la presenza di stenosi significative nel circolo coronarico nativo , sia distalmente alle anastomosi dei bypass che nei vasi coronarici non bypassati . 
considerando unitamente invece stenosi severe ed occlusioni , la sensibilit risulta del 98% , la specificit del 97% con una positive likelihood - ratio superiore a 10 ed una negative likelihoodratio di 0 , 02 , indicando la cct come metodica diagnostica utile per confermare od escludere la presenza di malattia dei bypass con un elevato grado di confidenza nei pazienti con una probabilit pre - test intermedia di malattia [ 7682 ]  . 
 la valutazione del circolo coronarico nativo risulta pi complessa per il minor calibro e per la maggior incidenza di calcificazioni rispetto ai bypass , con unaccuratezza diagnostica complessiva inferiore rispetto a quella ottenuta in pazienti non bypassati . 
 chronic total occlusion and computed - tomography - guided revascularisation post - infarto miocardico chronic total occlusion of the coronary vessels can occur in patients with coronary atherosclerosis , and it causes considerable management problems , both with regards to interventions and therapy . 
whereas new technical approaches , guides and devices have been developed and refined for use in chronic total occlusion , the problems of coronary angiography in accurately visualising the occluded vessels make angioplastic interventions and stenting particularly complex and difficult to perform in this setting . 
unlike coronary angiography , cct provides a precise assessment of the length and characteristics of the atherosclerosis ( calcified or not calcified ) of the occluded alcuni studi pre - clinici e clinici hanno dimostrato che la cct consente lo studio della vitalit miocardica attraverso la tecnica del delayed enhancement similmente alla rm [ 8389 ]  . 
in quadri di infarto miocardico acuto ( ami ) , subacuto e cronico , i difetti di perfusione possono essere osservati nella fase di primo passaggio del bolo di contrasto ( difetto di perfusione precoce ) , ma possono essere evidenziati con maggiore precisione in una fase successiva ( 515 minuti dopo la somministrazione del contrasto )  . 
la cct , permettendo lo studio del circolo coronarico e la successiva valutazione mediante delayed enhancement del miocardio , potrebbe consentire anche lidentificazione con una singola metodica di imaging delleziologia ischemica sottostante quadri di disfunzione ventricolare sinistra , similmente allintegrazione degli studi angiografici convenzionali con radiol med ( 2012 ) 117 : 901938 segments , factors that are predictors of intervention success and duration [ 9094 ]  . 
furthermore , lesions of vessel bifurcations can be studied ( angulation , extension , plaque composition ) by cct with more accuracy than with coronary angiography . biventricular functional assessment , heart valves and cardiomyopathies la rm [ 87 ]  . 
sebbene queste sperimentazioni cliniche condotte in gruppi numericamente ridotti di pazienti risultino promettenti , la rm resta attualmente la metodica non invasiva di riferimento per valutare lestensione delle aree non vitali post - ischemiche . 
i pazienti portatori di pace - maker o defibrillatori cardiaci automatici , con controindicazione allindagine rm , potrebbero essere , invece , selettivamente sottoposti a cct . occlusioni totali croniche e rivascolarizzazione tc - guidata indications for assessing biventricular function , heart valves and cardiomyopathies are presented in table 9 . le occlusioni totali croniche ( cto ) delle coronarie coinvolgono un gruppo di pazienti con aterosclerosi coronarica con notevoli problematiche di gestione , sia interventistica table 9 biventricular functional assessment , heart valves and cardiomyopathies indication biventricular function evaluation of left ventricular function evaluation of right ventricular function evaluation of left ventricular function ( in coronary studies ; retrospective gating ) valve disorders valve morphology ( mitral and aortic valves ) valve calcification ( mitral and aortic valves ) valve stenosis ( area ) valve regurgitation ( area ) prosthetic valve complication cardiomyopathies arrhythmogenic right ventricular cardiomyopathy dilated cardiomyopathy ( myocardial evaluation ) dilated cardiomyopathy ( coronary evaluation ) hypertrophic cardiomyopathy myocarditis tabella 9 funzione biventricolare , valvole e cardiomiopatie indicazione funzione biventricolare valutazione funzione ventricolare sinistra valutazione funzione ventricolare destra valutazione funzione ventricolare sinistra ( in studio coronarico ; gating retrospettivo ) valvulopatie morfologia valvolare ( valvola mitrale ed aortica ) calcificazioni valvolari ( valvola mitrale ed aortica ) stenosi valvolare ( area ) rigurgito valvolare ( area ) complicanze su protesi valvolari cardiomiopatie cardiomiopatia aritmogena del ventricolo destro cardiomiopatia dilatativa ( valutazione miocardio ) cardiomiopatia dilatativa ( valutazione coronarie ) cardiomiopatia ipertrofica miocardite class classe 920 biventricular functional assessment functional parameters , such as end - diastolic and end - systolic volumes , stroke volume , ejection fraction and myocardial mass can be calculated for both left and right ventricles using the cct data set [ 95 ]  . 
as regards functional assessment of the left ventricle , various studies show that cct has a good to excellent correlation with mri and echocardiography ( r > 0.85 for 16 - slice instruments and r = 0.870.96 for 64 - slice instruments ) [ 96100 ]  . 
functional cct evaluation of the right ventricle has also been validated through comparative studies with mri and echocardiography , showing an excellent correlation ( r = 0.830.99 ) [ 101103 ]  . although cct allows precise evaluation of biventricular contractile function , in most cases , cct is not performed for this purpose ; other methods , such as echocardiography and mri , are preferred . 
cct evaluation of biventricular function is , however , indicated in various situations in which mri is not feasible , in the presence of an inadequate echocardiographic window or in conditions such as pulmonary hypertension , pulmonary embolism , heart failure , infarction , congenital heart diseases and pretransplantation evaluation . 
nevertheless , mri and cct can have a complementary role when the echocardiographic acoustic window is inadequate and when transoesophageal echocardiography ( tee ) or catheterisation is not tolerated / desired . 
regarding aortic valve regurgitation , cct has an excellent diagnostic accuracy compared with tee ( sensitivity = 95% , specificity = 96100% ) [ 109 ]  . the mitral valve can also be studied by cct : the correlation between cct and tee is very good for stenosis ( r = 0.88 ) , and regurgitation can also be estimated correctly [ 110 ]  . 
valves of the right side of the heart ( tricuspid and pulmonary ) are usually evaluated by cct in an indirect manner by observing signs of right - side overload ( increased size of the right atrium and ventricle , regurgitation of suprahepatic veins , dilatation of the vena cava )  . 
 finally , prosthetic valves can be evaluated well by cct , and not only from a morphological point of view : in fact , radiol med ( 2012 ) 117 : 901938 che terapeutica . 
mentre nuovi approcci tecnici , guide e dispositivi sono stati sviluppati e perfezionati per lutilizzo nelle cto , le difficolt della cag nel visualizzare adeguatamente le coronarie occluse rendono gli interventi di angioplastica e stenting particolarmente complessi e di difficile esecuzione . 
a differenza della cag , la cct fornisce una valutazione accurata della lunghezza e delle caratteristiche dellaterosclerosi ( calcifica e non calcifica ) dei segmenti occlusi , che sono predittori di successo e durata della procedura [ 9094 ]  . 
anche le lesioni di biforcazione possono essere studiate dalla cct ( angolazione , estensione , composizione di placca ) , con pi accuratezza della cag . funzione contrattile biventricolare , valvole e cardiomiopatie le indicazioni per diagnosticare funzione contrattile biventricolare , valvole cardiache e cardiomiopatie sono presentate nella tabella 9 . funzione contrattile biventricolare i parametri funzionali come volume telediastolico e telesistolico , stroke volume , frazione di eiezione e massa possono essere calcolati sia per il ventricolo sinistro che per il destro utilizzando il dataset della cct [ 95 ]  . 
per quanto riguarda lo studio funzionale del ventricolo sinistro , diversi studi hanno dimostrato come sia gli scanner tc a 16 strati ( r > 0 , 85 ) che , soprattutto , a 64 o pi strati ( r = 0 , 870 , 96 ) si abbia una buona - ottima correlazione con rm ed ecocardiografia [ 96100 ]  . 
anche la valutazione funzionale tc del ventricolo destro stata validata attraverso studi comparativi con rm ed ecocardiografia , dimostrando unottima correlazione ( r = 0 , 830 , 99 ) [ 101103 ]  . sebbene la cct consenta unaccurata valutazione della funzione contrattile biventricolare , nella maggior parte dei casi lesame cct non viene eseguito per tale scopo ; in tali situazioni sono da preferirsi altre metodiche come ecocardiografia ed rm . 
la valutazione cct della funzione biventricolare trova comunque indicazione in diverse situazioni in cui la rm non risulti fattibile ( pazienti claustrofobici o portatori di pace - maker ) , in presenza di una inadeguata finestra acustica ecocardiografica , o ancora in condizioni quali ipertensione polmonare , malattia embolica polmonare , scompenso , infarto , nelle cardiopatie congenite e nella valutazione pre - trapianto . 
 radiol med ( 2012 ) 117 : 901938 postoperative complications such as dehiscence of anastomoses , abscesses , pseudoaneurysms , endocardial vegetations and thrombi can be detected by cct [ 111 ]  . valvole cardiache cardiomyopathies cardiomyopathies comprise a variety of disorders in which the primary pathological process directly involves the myocardiuthe main noninvasive methods used to study these conditions are echocardiography and mri . 
only in the last few years has cct begun to find space as a complementary or alternative method in the event that the first - choice method provides poor - quality results or cannot be performed . 
as far as concerns dilated cardiomyopathy , cct can be used to suggest or rule out a possible ischaemia cause by determining whether cad is present or absent , respectively [ 113 ] , and is also able to evaluate biventricular contractile function accurately . 
finally , cct can be used to study hypertrophic cardiomyopathy to exclude the concomitant presence of more or less significant cad or in cases in which mri is not feasible and / or diagnostic : morphology , function and myocardial perfusion can be evaluated [ 114 ]  . 
cct is of limited use in assessing acute myocarditis and restrictive cardiomyopathy . thoracic aorta and pre - tavi assessment indications for cct use in pre - transcatheter aortic valve implantation ( tavi ) and thoracic aorta assessment are presented in table 10 . disorders of the thoracic aorta the main acquired acute or chronic disorders of the thoracic aorta are aneurysms , dissection , intramural haematoma , penetrating atherosclerotic ulcer and trauma ; ct is considered the diagnostic reference standard for these disorders , having a sensitivity and specificity of 100% [ 115 ]  . aneurysms : ct affords adequate assessment of the presence and extent of aneurysmal dilatation as well as any involvement of branches originating from the aorta . dissection : the main characteristic feature of aortic dissection visualised by ct is the presence of two aortic lumens and an intima media flap that separates the true lumen from the false one ; ct defines entry and exit tears . 
sometimes , the presence of intimal calcifications on the dissected flap allows prompt diagnosis even on noncontrast ct scans [ 115 ]  . intramural haematoma : noncontrast - enhanced ct shows a crescent - shaped hyperdense area within the wall il basso costo , la facile accessibilit e modalit di utilizzo rendono lecocardiografia transtoracica ( tte ) lindagine di prima scelta nella valutazione delle patologie valvolari cardiache . 
la valutazione cct della stenosi valvolare aortica pu essere effettuata misurando larea valvolare , con unottima correlazione ( r = 0 , 99 ) con tee [ 106108 ]  . 
 per quanto riguarda invece linsufficienza valvolare aortica , la cct in grado di valutarla con unottima accuratezza diagnostica se paragonata alla tee ( sensibilit = 95% , specificit = 96%100% ) [ 109 ]  . anche la valvola mitrale pu essere adeguatamente studiata mediante cct : per la stenosi vi unottima correlazione fra cct e tee ( r = 0 , 88 ) , ed anche il rigurgito risulta correttamente stimabile [ 110 ]  . 
le valvole cardiache delle sezioni di destra ( tricuspide e polmonare ) mediante cct si valutano prevalentemente in maniera indiretta , osservando la presenza di segni di sovraccarico destro ( aumentate dimensioni di atrio e ventricolo , rigurgito vene sovraepatiche , dilatazione della vena cava )  . 
 anche le protesi valvolari risultano ben valutabili con la cct , e non solo da un punto di vista morfologico : infatti possibile valutare anche le complicanze post - operatorie quali deiscenze anastomotiche , ascessi , pseud - aneurismi , vegetazioni endocardiche e trombi [ 111 ]  . cardiomiopatie le cardiomiopatie racchiudono una variet di patologie in cui il processo patologico primario coinvolge direttamente il miocardio . 
solo negli ultimi anni la cct ha iniziato a trovare il suo spazio come metodica complementare o alternativa in caso di scarsa qualit o impossibilit ad eseguire i suddetti esami di prima scelta . 
per quanto riguarda la cardiomiopatia dilatativa , la cct trova spazio nellescluderne uneventuale causa ischemica valutando la presenza di malattia coronaria [ 113 ] , ed inoltre in grado di valutare accuratamente la funzione contrattile bi - ventricolare . 
la cct pu essere 922 indication table 10 thoracic aorta and pre - percutaneous aortic valve implantation ( tavi ) assessment thoracic aorta aneurysm ( diagnosis , morphology , dimensions and follow - up ) aortic dissection ( diagnosis and follow - up ) intramural haematoma ( diagnosis and follow - up ) penetrating ulcer ( diagnosis and follow - up ) aortic trauma ( diagnosis and follow - up ) planning surgery / endovascular procedures postoperative follow - up of surgery to the thoracic aorta arteritis / aortitis monitoring atherosclerotic plaques in the aorta pre - tavi morphology and dimensions of the aortic annulus morphology and dimensions of valsalva sinuses and the s - t junction morphology of coronary arteries ( distance of coronary ostia / aortic valve plane ) morphology and dimensions of the femoral / subclavian access s - t , sino - tubular aortic junction tabella 10 aorta toracica e valutazione pre - impianto valvolare aortico percutaneo ( tavi ) indicazione aorta toracica aneurisma ( diagnosi , morfologia , dimensioni e follow - up ) dissezione aortica ( diagnosi e follow - up ) ematoma intramurale ( diagnosi e follow - up ) ulcera penetrante ( diagnosi e follow - up ) lesione aortica traumatica ( diagnosi e follow - up ) pianificazione intervento chirurgico / endovascolare follow - up post intervento chirurgico su aorta toracica arteriti / aortiti monitoraggio placche ateromasiche aortiche pre - tavi morfologia e dimensioni dellannulus aortico morfologia e dimensioni dei seni di valsalva e della giunzione s - t morfologia delle coronarie ( distanza ostii coronarici / piano valvolare aortico ) morfologia e dimensioni dellaccesso femorale / succlavio s - t , giunzione sino - tubulare aortica radiol med ( 2012 ) 117 : 901938 class classe of the aorta or circumferential thickening of the aortic wall [ 116 ]  . 
following contrast agent administration , the abovementioned crescent - shaped / circumferential area appears not to be perfused and does not have intimal lacerations . penetrating atherosclerotic ulcer : when examined by ct , the ulcer presents as a void of filling by contrast agent , with a neck , and strongly resembles the appearance of a peptic ulcer [ 117 ]  . aortic trauma : ct has a sensitivity and specificity close to 100% . 
 ct also plays a fundamental role in planning the management of acute and chronic aortic pathologies , whether usata anche nello studio della cardiomiopatia ipertrofica per escludere la contemporanea presenza di malattia coronarica pi o meno significativa o nei casi in cui la rm non risulti fattibile e / o diagnostica : con la cct possibile valutare morfologia , funzione e perfusione miocardica [ 114 ]  . 
 la cct trova scarsa applicabilit nella valutazione della miocardite acuta e della cardiomiopatia restrittiva . aorta toracica e valutazione pre - impianto trans - catetere di valvola aortica le indicazioni per valutare laorta toracica e il pre - impianto trans - catetere di valvola aortica sono presentate nella tabella 10 . radiol med ( 2012 ) 117 : 901938 by conventional surgery or endovascular procedures , and in their follow - up [ 119 ]  . 
ecg synchronisation is usually recommended for aortic studies , particularly when the root of the aorta and / or the ascending tract is involved [ 8 ]  . preoperative assessment prior to percutaneous transapical aortic valve implantation tavi has emerged as a less invasive therapeutic option for patients who cannot undergo conventional surgery or who are at high risk [ 120 ]  . 
characteristics that must be evaluated prior to a tavi procedure are coronary vessel anatomy ( in particular , the position and distance of the coronary ostia from the valve leaflets ) , dimensions of the aortic annulus , valsalva sinuses and sinotubular junction , and last but not least , diameter , tortuosity and calcification of peripheral accesses , such as the femoral or subclavian arteries [ 120 ]  . 
 it was recently reported that ct can , in a single - shot examination , be used to assess the anatomy of the thoracic aortic root - aorta and of the aortoiliac vasculature [ 121 ]  . 
in patients who are candidates for tavi , cct is also able accurately assess the presence of cad , contractile function of the left ventricle and the presence of atrial or ventricular thrombi . pericardial diseases and cardiac masses pericardial diseases and cardiac masses are usually assessed first by echocardiography . 
cct may have a role in some situations , such as when the pericardial pathology is concomitant with or incidental to the investigation requested or when mri studies are not possible ( table 11 ) [ 122127 ]  . pericardial diseases cct provides accurate anatomical definition and characterisation of the main pathologies of the pericardiu in fact , cct can , in a single - shot examination , determine the thickness of pericardial membranes , fluid levels and any congenital anomalies of the pericardium itself [ 122 , 125 ]  . 
for example , a pericardial effusion with a density significantly greater than that of water is suggestive of haemopericardium or purulent exudate . acute pericarditis , when not accompanied by pericardial patologia dellaorta toracica le principali patologie acquisite che interessano laorta toracica ( acute o croniche ) , sono gli aneurismi , la dissezione , lematoma intramurale , lulcera penetrante aterosclerotica e la patologia traumatica ; la tc considerata lo standard di riferimento diagnostico per queste patologie , con una sensibilit ed una specificit del 100% [ 115 ]  . per quanto riguarda gli aneurismi , la tc consente di valutare adeguatamente presenza ed estensione di una dilatazione aneurismatica , nonch leventuale coinvolgimento dei rami ad origine aortica . nella dissezione aortica la principale e peculiare caratteristica visualizzabile con la tc la presenza di due lumi aortici e della lacerazione intimale che separa il vero lume dal falso [ 115 ]  . nellematoma intramurale la scansione basale tc mostra la presenza di unarea di iperdensit di aspetto falciforme allinterno della parete aortica , oppure un ispessimento circonferenziale della stessa [ 116 ]  . 
dopo somministrazione di mezzo dicontrasto ( mdc ) la suddetta area falciforme / circonferenziale non viene perfusa e non si evidenziano lacerazioni intimali . lulcera penetrante in tc si presenta come un plus di riempimento di mdc con colletto , del tutto simile a quanto si osserva in unulcera peptica [ 117 ]  . anche nella patologia aortica traumatica la tc ha una sensibilit ed una specificit prossime al 100% . 
la lesione traumatica si pu manifestare con un evidente stravaso di mdc , ematoma periaortico o mediastinico , anomalie del profilo aortico , pseudoaneurismi o lacerazioni intimali [ 118 ]  . 
 nella patologia aortica acuta e cronica la tc gioca un ruolo fondamentale anche nella pianificazione di un possibile trattamento , sia esso chirurgico convenzionale oppure endovascolare , e nel follow - up [ 119 ]  . 
in generale si raccomanda lutilizzo della sincronizzazione con il segnale ecg per lo studio della patologia aortica , in particolare quando sono coinvolti la radice aortica e / o il tratto ascendente [ 8 ]  . valutazione pre - operatoria per impianto percutaneo / transapicale di valvole aortiche limpianto trans - catetere di valvola aortica ( tavi ) emerso come opzione terapeutica meno invasiva per i pazienti inoperabili per via convenzionale o per i pazienti ad alto rischio [ 120 ]  . 
le caratteristiche da valutare in funzione di una procedura tavi sono lanatomia delle coclass table 11 pericardial diseases and cardiac masses 924 indication pericardial effusion acute pericarditis constrictive pericarditis detection and characterisation of cardiac masses detection and characterisation of pericardial masses tabella 11 patologia pericardica e masse cardiache indicazione classe versamento pericardico pericardite acuta pericardite costrittiva rilevazione e caratterizzazione di neoformazioni cardiache rilevazione e caratterizzazione di neoformazioni pericardiche effusion , can be visualised by cct as a result of the early uptake of contrast medium in the thickened pericardial areas ; however , mri is much more accurate in this setting . 
 chronic pericarditis is shown by fusion of the pericardial membranes , which are thickened , and sometimes by the presence of calcifications [ 122 ]  . constrictive pericarditis can be diagnosed by cct on the basis of morphological criteria , such as an abnormal outline of a notably thickened pericardium , conical deformation of the ventricles and right atrial dilatation . 
however , a pericardium with a width of < 4 mm excludes the diagnosis of constrictive pericarditis , even in patients with clear symptoms , suggesting instead a possible diagnosis of restrictive cardiomyopathy [ 126 ]  . the most common mass lesion of the pericardium is a cyst . 
 recentemente stata riportata in letteratura la capacit della tc di valutare , con un unico esame , lanatomia della radice aortica - aorta toracica e lanatomia vascolare aortoiliaca [ 121 ]  . 
nei pazienti candidati a tavi , la cct anche in grado di valutare accuratamente la presenza di malattia coronarica , la funzione contrattile ventricolare sinistra e la presenza di trombi atriali o ventricolari . patologia pericardica e masse cardiache le patologia del pericardio e le masse cardiache vengono normalmente valutate in prima istanza mediante ecocardiografia . 
la cct pu assumere un ruolo in alcune situazioni come ad esempio quando la patologia del pericardio sia concomitante o incidentale rispetto allindagine richiesta o quando lapprofondimento mediante rm non sia possibile ( tabella 11 ) [ 122127 ]  . patologia pericardica la cct permette unaccurata definizione dellanatomia e unottimale caratterizzazione delle principali patologie del pericardio . 
la cct pu identificare , infatti , in un unico esame , lo spessore dei foglietti pericardici , le falde di versamento ed eventuali anomalie congenite del pericardio stesso [ 122 , 125 ]  . 
una densit sovra - idrica suggerisce ad esempio la presenza di un emopericardio o di essudati purulenti . la pericardite acuta , quando non associata a versamento pericardico , pu essere visualizzata in cct per una precoce impregnazione di contrasto dei tratti pericardici ispessiti ( la rm consente una accuratezza diagnostica superiore )  . 
la pericardite cronica , si evidenzia per la fusione dei foglietti pericardici , che presentano contorni ispessiti e , talvolta , per la presenza di calcificazioni [ 122 ]  . la pericardite costrittiva pu essere valutata mediante cct sulla base di criteri morfologici quali lanomalia del profilo del pericardio ( notevolmente ispessito ) ; le deformazioni coniche dei ventricoli e la dilatazione atriale destra . 
benign neoplasms are more common than malignant ones , but even the former are associated with a high rate of morbidity and mortality because of their capacity to induce syncope and arrhythmias and to facilitate emboli formation [ 124 ]  . 
the main role of imaging is to differentiate primary and secondary tumours from thrombi , which are definitively more common , and from pseudotumours , such as tuberculoma and hydatid cysts . 
cct can be performed in cases in which mri is not available or not feasible or to evaluate the mass and metastatic spread of the malignancy in a single examination . electrophysiological applications table 12 describes indications for electrophysiological applications . left atrium - pulmonary vein complex following the discovery in 1998 of the fine mechanisms triggering atrial fibrillation , electrophysiological procedures of transcatheter ablation to disconnect pulmonary veins from the left atrium were rapidly developed and spread widely , particularly for patients refractory to pharmacological treatment [ 128130 ]  . 
 thanks to epicardial and endocardial three - dimensional vr reconstructions , which are added to the native axial images and to the mpr / mip , cct enables identification of numerous variants of confluence of the pulmonary veins into the left atrium [ 137 ]  . 
furthermore , cct can be used to define vein branches , assess ostia morphology , calculate atrial volumes and detect the presence of any thrombi in the lumen of the left auricle a condition that is an absolute contraindication to the performance of ablation procedures . 
it is now possible to integrate the images acquired by cct with electroanatomical maps derived from the navigation systems used by electrophysiologists during the ablation procedures diagnosi di cardiomiopatia restrittiva [ 126 ]  . la massa pi comune del pericardio la cisti . 
la cct pu essere utilizzata per la caratterizzazione , per la definizione della sede e per identificare i rapporti della cisti con le strutture circostanti , in particolare per un eventuale valutazione pre - chirurgica . 
la cct pu essere utilizzata per la diagnosi quando la rm non sia disponibile [ 122 , 126 ]  . masse cardiache le neoplasie cardiache primitive sono molto rare ( prevalenza 0 , 001%0 , 03% )  . 
le neoplasie benigne sono pi comuni di quelle maligne , ma hanno comunque un elevato indice di morbilit e mortalit a causa della loro capacit di indurre aritmie e di favorire la formazione di emboli [ 124 ]  . 
il ruolo principale dellimaging quello di differenziare le lesioni tumorali cardiache primitive e secondarie dai trombi sicuramente pi frequenti e dalle lesioni pseudotumorali quali il tubercoloma e la cisti idatidea . lecocardiografia transtoracica la tecnica di prima linea per lidentificazione delle masse cardiache . 
la cct pu essere utilizzata in caso di indisponibilit o non fattibilit della rm o per valutare in un unico esame la massa e la diffusione metastatica del tumore . applicazioni elettrofisiologiche la tabella 12 riporta le indicazioni per le appliocazioni elettrofisiologiche . 
 complesso atrio sinistro - vene polmonari dopo la scoperta nel 1998 dei fini meccanismi di attivazione della fibrillazione atriale le procedure elettrofisiologiche di ablazione transcatetere per deconnettere le vene polmonari ( vp ) dallatrio sinistro ( as ) si sono rapidamente table 12 electrophysiological applications 926 indication overall evaluation of the la - pv anatomic complex ( preablation road map ) assessment of postprocedure complications ( stenosis , atrial - oesophageal fistulae , etc . ) identification of thrombi in the left atrium or auricle integration with electroanatomic maps evaluation of the cardiac venous system la - pv , left atrium pulmonary veins tabella 12 applicazioni elettrofisiologiche valutazione complessiva del complesso anatomico as - vp ( road - map pre - ablazione ) valutazione delle complicanze post - procedura ( stenosi , fistole atrio - esofagee , ecc . ) identificazione di trombi nellatrio o nellauricola sinistra integrazione con mappe elettro - anatomiche valutazione apparato venoso cardiaco as - vp , atrio sinistro e vene polmonari class indicazione classe [ 138 , 139 ]  . 
this integration enables navigation of the real anatomy of the left atriumpulmonary vein complex , further optimising the intervention , also in terms of reducing radiation dose given the shortening of fluoroscopy times . 
furthermore , cct is fundamental for the follow - up of patients who have undergone ablation procedures : an examination performed after 3 months readily shows any narrowing of the vessel lumen , which usually occurs in the preostial part of the vein , causing an hourglass - shaped deformity of the vessel [ 132 , 134 ]  . 
 cardiac veins the growing interest in cardiac ( coronary ) veins is due to the increase in interventions involving these vessels ( electrophysiological studies with placement of catheters in the coronary sinus ; ablation of accessory electrical circuits ; retrograde coronary perfusion in high - risk or complicated angioplasty )  . 
furthermore , knowledge of the exact anatomy of the cardiac veins , characterised by a certain variability [ 140 , 141 ] , is highly important in cardiac resynchronisation interventions ( biventricular pacing or cardiac resynchronisation ) in some patients with heart failure [ 142 , 143 ]  . 
the main factor responsible for the success of these procedures is prior knowledge of cardiac vein anatomy : retrograde venography is diagnostic in only 67% of patients because of the impossiradiol med ( 2012 ) 117 : 901938 sviluppate e diffuse , soprattutto per i pazienti refrattari alla terapia farmacologica [ 128130 ]  . 
grazie alle ricostruzioni in volume rendering 3d epicardico ed endocardico , che si aggiungono alle immagini assiali native e alle mpr / mip , la cct garantisce la identificazione delle numerose varianti di confluenza delle vp nellas [ 137 ]  . 
inoltre la cct consente di riconoscere sia il branching di confluenza delle vene , sia la morfologia degli osti , di calcolare i volumi atriali e di rilevare la presenza di eventuali trombi nel lume dellauricola sinistra , condizione che controindica in maniera assoluta la procedura di ablazione . 
recentemente diventato possibile integrare le immagini realizzate con cct con le mappe elettroanatomiche derivate dai sistemi di navigazione utilizzate dagli elettrofisiologi durante le procedure di ablazione [ 138 , 139 ]  . 
questa integrazione consente di navigare nellanatomia reale del complesso as - vp , ottimizzando ulteriormente le procedure interventistiche , anche in termini di riduzione di dose radiante , stante la contrazione dei tempi di fluoroscopia . 
inoltre , la cct fondamentale per il follow - up dei pazienti sottoposti alla procedura di ablazione : lesame eseguito dopo 3 mesi permette di riconoscere agevolmente eventuali restringimenti del lume venoso che solitamente si realizzano in sede pre - ostiale , determinando una deformazione a clessidra del vaso [ 132 , 134 ]  . vene cardiache il crescente interesse per le vene cardiache ( vene coronariche ) dovuto allaumento di procedure interventistiche che utilizzano questi vasi ( studi elettrofisiologici con posizionamento di cateteri nel seno coronarico ; procedure di ablazione di circuiti elettrici accessori ; retroperfusione coronarica in angioplastiche ad elevato rischio o complicate )  . 
 inoltre , lesatta conoscenza anatomica delle vene cardiache , caratterizzata da una discreta variabilit [ 140 , 141 ] , di grande importanza negli interventi di resincronizzazione cardiaca ( pacing biventricolare o crt ) in alcuni pazienti affetti da scompenso cardiaco [ 142 , 143 ]  . 
il principale fattore responsabile del successo di tale procedura rappresentato dalla conoscenza preliminare dellanatomia delle vene cardiache : la venografia retrograda risulta diagnostica solo nel 67% dei pazienti a causa dellimpossibilit di radiol med ( 2012 ) 117 : 901938 bility of cannulating the coronary sinus or inadequate vessel occlusion by the balloon , which should prevent backwash of the contrast medium injected against the blood flow to render the cardiac veins opaque [ 140 ]  . 
cct , on the other hand , enables excellent visualisation of the entire cardiac venous system and thanks to the three - dimensional vr reconstruction and mpr / mip identification of a vessel suitable for housing the stimulatory electrode and performance of qualitative - quantitative evaluations ( diameter , tortuosity , distance between coronary sinus ostium and confluence of the left posterolateral vein , angulation of this confluence ) that are indispensable to make the biventricular pacing more effective and efficient [ 144148 ]  . incannulare il seno coronarico o dellinadeguata occlusione vasale da parte del palloncino che impedisce il lavaggio ( backwash ) del mezzo di contrasto iniettato controcorrente per lopacizzazione delle vc [ 140 ]  . 
kyriakides contrast - enhanced ultrasound should be used more frequently for aortic endograft surveillance barts and the london nhs trust , barts and the london school of medicine and dentistry , circulatory sciences clinical academic unit , vascular and endovascular surgical services , the royal london hospital , whitechapel , london e1 1bb , uk correspondence to : s . 
for their work [ 1 ] and were delighted to read their report regarding redefining follow - up protocols after endovascular abdominal aortic aneurysm repair in their prospectively enrolled 88 consecutive patients . 
we were delighted to see their comparison of the two endovascular aortic aneurysm repair ( evar ) surveillance modalities demonstrating that contrast - enhanced ultrasound scanning ( ceus ) of their patients was comparable with the gold standard of computed tomography angiography ( cta )  . 
questions we have regarding their work concern data regarding the cost of these two modalities and the prospective savings that could be made by introducing ceus in their evar surveillance programme . 
also , we would appreciate any information regarding radiation exposure to patients in preoperative evar planning , during the actual evar procedure itself and during cumulative evar surveillance using triple - phase computed tomographic angiography ( cta )  . 
we do not use triphasic cta for our surveillance programme ; instead , we use a reduced biphasic protocol that decreases radiation exposure to our patients . in summary , we found motta et al.s study extremely helpful , and it will no doubt help us in our pursuits to implement routine ceus not only in our practice but in protocols of others in the uk . 
calabrese2 1department of experimental medicine dimes , institute of anatomy , universit di genova , largo rosanna benzi 8 , 16132 genova , italy 2irccs azienda ospedaliera san martino - ist , genova , italy 3department of radiology , university of genova , genova , italy correspondence to : a . 
affinch i valori derivanti dallo studio con dti siano clinicamente utili , in particolare per la prognosi o il monitoraggio degli effetti della terapia , devono essere affidabili e attendibili . 
 lo scopo di questo studio quello di valutare la riproducibilit intrae inter - osservartore dellanisotropia frazionaria derivante dalla dti e il coefficiente di diffusione apparente ( adc ) utilizzando un apparecchio di risonanza magnetica da 3 , 0 t . 
 sessanta mammelle normali controlaterali , rispetto a quelle malate , di 60 pazienti ( 2885 anni di et , mediana di 67 anni ) sono state analizzate con una sequenza dti seguendo il protocollo standard per rm della mammella . 
gli stessi autori , senza conoscere i dati radiol med ( 2012 ) 117 : 9921003 interobserver agreement of the four radiologists for adc and fa were good ( acceptable )  . 
i valori di adc e fa ottenuti con la tecnica dti sono riproducibili , e possono essere considerati validi e attendibili . parole chiave mammella rm imaging con tensore di diffusione accuratezza reproducibilit introduction introduzione up - to - date magnetic resonance imaging ( mri ) of the breast is the most sensitive method for detecting breast cancer [ 1 , 2 ]  . 
for this reason , analysis of enhancement patterns in breast mri is sometimes not sufficiently specific as a standalone method for differential diagnosis ; therefore , the mri breast imaging - reporting and data system ( bi - rads ) lexicon recommends a combination of dynamic and morphological criteria for differential diagnosis of breast lesions [ 4 ]  . 
standard dwi , based on diffusion encoding in three orthogonal directions , is limited to quanal momento la risonanza magnetica ( rm ) la tecnica di imaging pi sensibile per la valutazione del cancro della mammella [ 1 , 2 ]  . 
per questa ragione lanalisi di un pattern di enhancement nella rm della mammella non sufficientemente specifica come unico criterio per la diagnosi differenziale ; pertanto il breast imagingreporting and data system ( bi - rads ) raccomanda la valutazione di criteri combinati sia dinamici che morfologici per la diagnosi differenziale delle lesioni [ 4 ]  . 
stato dimostrato che il dwi associato ad una normalizzazione del coefficiente di diffusione apparente ( adc ) migliora significativamente la performance diagnostica dalla rm della mammella convenzionale comprendendo come parametri di valutazione lacquisizione sia di criteri morfologici che di una curva di dati acquisiti durante se994 radiol med ( 2012 ) 117 : 9921003 tifying only the adc . 
diffusion tensor imaging ( dti ) represents an extension of standard dwi , with diffusion encoding in at least six directions , to measure the full diffusion tensor and characterise the motion of water in more detail . 
dti can provide valuable information on tissue microstructure and pathophysiology that cannot be obtained by other imaging techniques [ 17 ] and has been extensively used on the brahowever , with recent advancements in mri technology , dti has also enabled unique microstructural characterisation of normal and abnormal abdominal tissue [ 1822 ]  . 
the study comprised 60 women who underwent breast mri for unclear or suspicious findings on x - ray mammography or breast ultrasound ( us ) following european society of breast cancer specialists ( eusoma ) indications and recommendations [ 25 ]  . 
breast dti was added to the standard breast mri protocol and was performed on the lesion - free breast , assessed with mammography , us and dynamic mri in the same session . 
larea sottesa alla curva receiver operating characteristic ( roc ) migliorata passando da 0 , 89 a 0 , 98 e il tasso di falsi positivi diminuito utilizzando un apparecchio da 3 , 0 t [ 16 ]  . 
limaging con tensore di diffusione ( dti ) rappresenta unestensione della tecnica standard dwi , rendendo possibile la codifica del segnale in almeno sei direzioni e misurando il tensore di diffusione completo , e caratterizza molto pi dettagliatamente il movimento delle molecole dacqua . 
per quel che riguarda il valore adc , la dti non in grado di calcolare il grado di diffusione anisotropa ( o la direzionalit ) e la principale direzione della diffusione associata ad essa , in ogni singolo voxel . 
la dti ha trovato ampio ruolo nello studio dellencefalo , tuttavia recenti progressi tecnologici dellimaging in rm hanno reso la dti utile per la caratterizzazione microstrutturale dei tessuti sia normali e che patologici anche a livello delladdome [ 1822 ]  . 
i promettenti risultati ottenuti in questo campo con un 3.0 t , utilizzando la dwi , ci hanno suggerito la possibilit di esaminare la mammella con la dti con apparecchiature di questo tipo . 
in merito a ci una sfida per incrementare la diffusione dellapplicazione della dti nello studio della mammella rappresentata dalla standardizzazione e dalla ripetibilit dei risultati quantitativi ottenuti [ 17 ]  . 
al momento , in letteratura , mancano studi in proposito che prevedano lutilizzo di un apparecchio da 3 , 0 t ; pertanto il nostro studio ha lo scopo di valutare la riproducibilit intrae inter - osservatore dellanisotropia frazionaria e del coefficiente di diffusione apparente ottenuti con la dti applicata a un sistema da 3 , 0 t . materiali e metodi pazienti questo studio prospettico stato approvato dal comitato etico del nostro istituto e le pazienti coinvolte hanno firmato il consenso informato . 
lo studio ha incluso 60 donne che hanno eseguito un esame rm a causa di reperti dubbi o sospetti evidenziati in seguito a una mammografia o a unecografia mirata , come indicano le linee guida della societ europea di mastologia ( eusoma ) in questi casi [ 25 ]  . 
non sono state osservate differenze tra il lato destro e quello sinistro adc , coefficiente di diffusione apparente ; fa , anisotropia frazionaria using a dedicated eight - channel bilateral breast coil ( general electric medical systems , milwaukee , wi , usa ) with the patient in the prone position . 
the t1 - weighted sequence was acquired with a 3d fast spoiled - gradient - recalled echo sequence with parallel imaging [ volume imaging for breast assessment ( vibrant ) ] , repetition time ( tr ) = 6.2 ms , echo time ( te ) = 3 ms ; flip angle = 10 ; 350350 matrix , and 90 - s scan time . dti was performed using dw echo - planar imaging ( epi )  . 
image acquisition parameters were as follows : te = minimum , tr = 16 , 675.0 ms , phase encoding r / l , frequency = 96 , phase = 128 , fov 26 cm , slice thickness = 2 mm , gap = 0 , slice number = 49 . 
before performing tensor estimation , a ge correction procedure was applied to the dti data set ( 1 , 617 images ) to correct distortions related to eddy currents induced by the large diffusion - sensitising gradients . 
four authors ( 6 , 5 , 4 , 4 years of experience in breast mri research , respectively ) performed all image postprocessing and analysis independently and in different dti pazienti sono state esaminate tra il 5 e il 15 giorno del ciclo mestruale . 
sono state escluse dallo studio : le donne sottoposte a precedente chirurgia , radioterapia o chemioterapia per il trattamento del cancro della mammella , in terapia ormonale sostitutiva e quelle pazienti il cui esame risultato incompleto o ha fornito immagini scarsamente diagnostiche a causa di artefatti . 
 limaging con diffusione di tensore stato eseguito per le mammelle prive di lesioni , valutate come tali , nella stessa seduta da un esame mammografico , ecografico mirato e da sequenze dinamiche di rm . 
let dei soggetti era compresa tra i 28 e gli 85 anni di et , presentando una mediana di 57 anni ( body mass index : 23 , 53 , 2 ) e su ogni paziente esaminata sono state eseguite delle acquisizioni dti durante lesame rm standard . protocollo rm tutti gli esami rm sono stati eseguiti , con paziente in posizione prona , con un apparecchio general electric 3 , 0 t hdx signa , utilizzando una bobina a 8 canali per lo studio bilaterale della mammella . 
la sequenza t1 pesata stata acquisita con 3d fast spoiled gradient , nota come sequenza echo , con imaging parallelo ( volume imaging for breast assessment , vibrant ) ; tempo di ripetizione ( tr ) = 6 , 2 ms , tempo di eco ( te ) = 3 ms ; flip angle = 10 ; 350350 matrice e tempo di scansione = 90 s . limaging con tensore di diffusione stato eseguito utiradiol med ( 2012 ) 117 : 9921003 996 fig . 
unilateral rois defined in the anterior , central and posterior regions of the breast were defined on the t2 - weighted b = 0 s / mm2 image ( a )  . 
le roi ottenute sono state tipicamente di 30 mm e sono state posizionate nelle aree di tessuto fibro - ghiandolare in ogni regione , escludendo con attenzione il tessuto adiposo . 
the t1 - weighted image and b = 0 image was used as an anatomical reference in each case , and rois were drawn to include only fibroglandular tissue and exclude regions of adipose tissue or cyst . 
breasts were visually divided into three regions , representing the anterior , central and posterior thirds of the breast , and rois were positioned on the b = 0 s / mm2 image near the level of the nipple , as illustrated in figure 1 . 
 sono stati inoltre utilizzati i dati di studio precedente in cui la diffusione era stata misurata in 32 direzioni ( tabella 1 ) con valori di b di 0 e di 1000 s / mm2 . 
blandaltmann and kappa statistics were used to asses precision and repeatability of measurements and intraand interobserver agreement between the four radiologists in evaluating quantitative parameters , as previously reported [ 2629 ]  . 
concordance correlation coefficient ( icc ) , 95% confidence interval ( ci ) , pearson ( precision ) and bias correction factor for accuracy were calculated [ 2629 ]  . 
data were first assessed to verify that there was no relationship between measurement error and magnitude of parameter values ( by kendalls ) and that there were no statistically significant differences between repeated examinations [ 17 ]  . 
statistical analysis was performed by one author using statistical software ( spss , version 12.0.1 , spss , excel 2007 , microsoft and medcalc , version 11.4 medcalc software , broekstraat 52 , 9030 mariakerke , belgium )  . results dti parameters , including adc and fa , were measured unilaterally in the breasts of 60 women in this study . 
quattro radiologi ( rispettivamente con 6 , 5 , 4 e 4 anni di esperienza nel campo della rm mammaria ) hanno attuato il post - processing e lanalisi delle immagini indipendentemente luno dallaltro e in diverse sessioni . 
gli stessi esperti , ignari dei risultati iniziali , hanno ripetuto il post - processing e lanalisi 4 settimane dopo la prima seduta . sono stati poi calcolati ladc e lanisotropia frazionaria ( fa ) nelle sequenze dti ottenute . 
stata utilizzata unimmagine t1 - pesata con un valore di b = 0 s / mm2 , come riferimento anatomico in ogni singolo caso e la roi stata delineata esclusivamente su tessuto fibroghiandolare escludendo la componente adiposa ed eventuali cisti . 
le mammelle sono state divise visivamente in tre regioni rappresentate rispettivamente dal terzo anteriore , dal terzo centrale e dal terzo posteriore e le roi sono state posizionate con un valore di b = 0 s / mm2 vicino al capezzolo come illustrato in figura 1 . 
le roi sono state posizionate anteriormente ( vicino al capezzolo ) , centralmente ( tra la zona anteriore / posteriore e la zone laterale / mediale ) e nelle regioni laterali e posteriori della ghiandola . 
in figura 1 illustrata le tipica dimensione e collocazione della roi . analisi statistica i valori normali sono stati calcolati per ogni parametro dti come medio e deviazione standard ( ds ) di tutti i soggetti . 
i dati di adc ed fa sono stati analizzati con ripetute misure di analisi della varianza ( anova ) per escludere che la posizione anatomica della roi avesse una significativa influenza sui dati . 
i test di bland - altmann e il test sono stati utilizzati per definire la precisione e la ripetibilit dei valori ottenuti e definire altres laccordo intraed inter - osservatore tra i quattro radiologi nella valutazione dei parametri quantitativi , come precedentemente accennato [ 2629 ]  . 
sono stati calcolati inoltre il coefficiente di correlazione della concordanza , lintervallo di confidenza al 95% , pearson ( precisione ) e il fattore di correzione dellerrore statistico per laccuratezza . 
i dati sono stati innanzitutto esaminati per verificare se esisteva o meno correlazione tra lerrore delle misurazioni e il valore dei parametri ( con il test di kendall ) , e per assicurare che non ci fossero differenze significative tra le ripetute misurazioni [ 17 ]  . 
sono stati usati un livello di errore ( intervallo di confidenza ) del 5% e un livello di errore ( potere statistico : 1 ) di 80% , considerati parametri accettabili per lo scopo dello studio . 
mean adc for dti sequences was 1.920.30 , and this finding is consistent with previously published data at 1.5 t on normal breasts [ 17 , 30 , 31 ]  . 
concerning regional differences , no significant differences were observed in breast adc and fa , in contrast to a recently published paper in which adc was higher in the central region and fa was generally higher in the outer posterior region [ 17 ]  . 
in our study , we chose a b value of 1 , 000 because dti at higher b values may be more sensitive to slower diffusing water compartments , such as intracellular water , and may better reflect reduced water diffusion associated with breast tumours [ 32 ]  . 
le indagini eseguite , precedentemente alla dti , tramite mammografia , ecografia mirata ed rm hanno avuto lo scopo di includere nel nostro studio solo mammelle sane prive di reperti patologici . 
 on breast dti measurements , we found less error for adc than for fa : the within - patient coefficient of variation was 15% for adc and 30% for fa . 
prior studies demonstrated that on 1.5 - t systems , adcs have the potential to help differentiate benign from malignant lesions [ 615 ] and that using a 3.0 - t system dwi with normalisation of adcs significantly improves diagnostic performance of conventional breast mri [ 16 ]  . 
moreover , in oncological imaging , prior studies demonstrated adc to be a sensitive biomarker for treatment response [ 34 ] , and in patients with breast cancer , it is proposed that adcs identify patients who did and did not respond to neoadjuvant chemotherapy [ 35 ]  . 
 our study had several limitations : the same 3.0 - t system laccordo intraed inter - osservatore tra i quattro radiologi per adc e fa valutati nelle immagini in dti , sono riportati nelle tabelle 2 e 3 . 
i valori medi nelle sequenze dti per ciascuna mammella sono stati ripetuti e confrontati in ciascun soggetto ( tabella 5 )  . discussione questo lavoro stato il primo studio in letteratura che abbia utilizzato la dti per la valutazione di adc ed fa nel tessuti normali , con un apparecchio da 3 t . 
le differenze regionali dei valori di adc e di fa non sono state considerate significative , contrariamente a recenti lavori scientifici pubblicati , in cui il coefficiente di diffusione apparente risultava pi elevato nelle regioni centrali e lanisotropia frazionaria risultava generalmente pi alta nelle regioni posteriori [ 17 ]  . 
una possibile spiegazione a questo sta nel fatto che il volume parziale considerato potesse comprendere al suo interno anche una parte di componente adiposa , daltra parte nel nostro studio lo spessore delle sezioni era nettamente minore che negli studi precedenti [ 17 ]  . 
i valori tipici di adc riportati , di 1 , 6 a 2 , 010 - 3 mm2 / s per la ghiandola mammaria normale corrispondono a un ottimale pesatura in diffusione con un valore approssimativo di b = 600 s / mm2 . 
nel nostro studio abbiamo scelto un valore di b di 1000 in quanto la sequenza dti ad un maggiore valore di b , pi sensibile ai compartimenti con una pi lenta diffusione dellacqua , come ad esempio gli spazi intracellulari , e pu meglio riflettere la diffusione delle molecole dacqua associata ai tumori mammari [ 32 ]  . 
aumentando il valore di b pu decrescere lintensit totale del segnale , tuttavia il contrasto tra i vari tessuti con diversi adc migliora aumentando i valori di b [ 33 ]  . 
questo processo solitamente limitato dal signal - noise ratio ( snr ) disponibile , quindi un sistema 3 , 0 t pu essere pi adeguato a fronte di un snr aumentato . 
lo studio in dti della mammella che ha fornito un errore di misura minore per adc piuttosto che per fa : la varianza intra - osservatore stata del 15% per adc e del 30% per fa . 
number of b values , field strength , and analysis software affect the measured adc , so it is possible that they also affect measurement reproducibility [ 36 ]  . 
this possible limitation concerning roi positioning is a current research topic , as it has been demonstrated that roi size and positioning have a considerable influence on tumour adc values and interobserver variability [ 38 ]  . 
studi precedenti hanno dimostrato che utilizzando dei sistemi da 1 , 5 t , i valori adc costituiscono un potenziale aiuto discriminativo nella differenziazione tra tumori benigni e maligni [ 615 ] e che lutilizzo di sistemi da 3 , 0 t unitamente a sequenze di dwi con normalizzazione del adc , migliora significativamente la performance dellimaging rm mammario [ 16 ]  . 
per di pi nellimaging oncologico , studi precedenti hanno dimostrato che adc adatto come biomarker nella valutazione della risposta terapeutica [ 34 ] e nelle pazienti con cancro della mammella il adc stato proposto come parametro di identificazione delle pazienti che rispondono o meno alla chemioterapia neoadiuvante [ 35 ]  . 
i nostri risultati suggeriscono che fa meno sensibile nel controllo degli effetti terapeutici nei soggetti per via della maggiore variabilit delle misure , dunque adc misurato in sequenze dti il parametro pi affidabile . 
nonostante il relativamente alto numero di osservatori , laccordo intrae inter - osservatore stato buono , tuttavia questi dati sono stati migliori per i valori adc misurati in dti , confermando , in conclusione , adc come il parametro pi affidabile . 
il numero dei valori di b , il campo di forza , e il programma di elaborazione dati hanno influenzato i valori di adc misurati , dunque possibile che abbiano altres influenzato la riproducibilit delle rilevazioni [ 36 ]  . 
questa potenziale limitazione relativa al posizionamento della roi comunque un argomento di ricerca attuale , considerando che stato dimostrato che la grandezza e il posizionamento della roi hanno uninfluenza considerevole sui valori di adc e sulla variabilit inter - osservatore [ 38 ]  . un aspetto positivo del nostro studio che il calcolo dellaccordo intrae inter - osservatore si basato sullosservazione di quattro radiologi . 
questo studio contribuisce alla valutazione delle potenzialit dellutilizzo dei 1002 radiol med ( 2012 ) 117 : 9921003 of diffusion - related values in breast tissue studies [ 39 ]  . 
the potential value of adc obtained with dti instead of that obtained with the usual dwi sequences may be that technical differences in these sequences may result in more precise and reproducible data for dti - derived measurements , as demonstrated in a preliminary study [ 40 ]  . 
in dti - derived sequences , the use of more directions ( 32 directions in this study ) , for example , may have helped to achieve more precise measurements . 
coefficient of variation was 15 % for adc on dti sequences , whereas on dwi sequences , the within - patient coefficient of variation for adc was 26 % [ fisci et al . 
 in conclusion , our results provide evidence that adc values obtained with dti are more reproducible than fa and that adc assessment on 3.0 - t systems may be valid , reliable , sensitive to change and feasible for lesion characterisation and therapy monitoring . valori ottenuti dalle sequenze pesate in diffusione nello studio del tessuto mammario [ 39 ]  . 
il vantaggio di utilizzare valori di adc ottenuti dalle sequenze dti , invece che dwi , potrebbe essere dovuto al fatto che le differenze tecniche in queste sequenze forniscano dati pi precisi e riproducibili con la dti . 
zompatori1 1cardio - thoracic - vascular department of radiology , santorsola - malpighi hospital , university of bologna , via massarenti 9 , bologna , italy 2library of general surgery and organ transplant l . 
section of centralized clinical library , santorsola - malpighi hospital , university of bologna , via massarenti 9 , bologna , italy 3institute of cardiology , santorsola - malpighi hospital , university of bologna , via massarenti 9 , bologna , italy correspondence to : f . 
from january 2006 to october 2009 , we measured the baseline and postcontrast attenuation values of acute pulmonary thrombi emboli on ct angiograms of 86 patients with acute pulmonary embolism ( pe ) and those of chronic thrombi in 29 patients with pulmonary hypertension of various origins . 
da gennaio 2006 a ottobre 2009 sono stati calcolati i valori densitometrici basali e postcontrastografici dei trombi acuti ricavati dalle angiotomografie computerizzate ( tc ) di 86 pazienti con embolia polmonare acuta e dei trombi cronici di 29 pazienti con ipertensione polmonare di diversa eziologia . 
only chronic thrombi exhibit ce , and ce is significantly associated with the development of collateral circulation , which may be involved in the process of thrombotic recanalisation . keywords pulmonary embolism intrathrombotic contrast enhancement pulmonary hypertension hypertrophic bronchial artery pulmonary angio - ct il ce si associa significativamente allo sviluppo di circoli collaterali che potrebbero essere implicati nel processo di ricanalizzazione trombotica . parole chiave embolia polmonare enhancement intratrombotico ipertensione polmonare arteria bronchiale ipertrofica angio - tomografia computerizzata polmonare introduction introduzione pulmonary embolism ( pe ) , the third most common cardiopulmonary disease after myocardial infarction and stroke , is responsible for hundreds of deaths every year , as it frequently goes undiagnosed [ 1 , 2 ]  . 
the natural course of acute pe shows that , in most cases , after migration of thrombotic material and endogenous thrombolysis , vascular patency is completely restored without haemodynamic consequences [ 3 ]  . 
chronic pulmonary hypertension may also develop following a nonembolic thrombotic process , with local extension ; this thrombosis in situ is typical of idiopathic pulmonary hypertension and hypertension associated with cyanogenic congenital heart diseases ( eisenmengers syndrome )  . 
acute pe , chronic thromboembolic pulmonary hypertension and idiopathic chronic pulmonary hypertension and pulmonary hypertension associated with congenital heart disease represent , among the thromboembolic pulmonary diseases , a broad and multiform spectrum , in particular , in terms of therapeutic approach and prognostic assessment . computed tomography angiography ( cta ) is the gold standard for diagnosing pulmonary thromboembolism , as it directly demonstrates the presence of intraluminal filling defects and allows other indirect signs to be identified [ 5 , 6 ]  . 
in particular , pe has never been studied both before and after contrast material administration [ 711 ]  . in this study , we measured the density of acute and chronic thromboembolic filling defects of pulmonary arteries before and after contrast agent administration and correlated attenuation values of acute emboli with those of blood circulating in the common pulmonary trunk , as well as the values of chronic thrombi with the presence of hypertrophic systemic - pulmonary vessels , such as bronchial arteries . lembolia polmonare la terza malattia cardio - polmonare dopo linfarto miocardio e lo stroke ed gravata da centinaia di morti ogni anno , poich spesso rimane misconosciuta [ 1 , 2 ]  . 
la storia naturale dellembolia polmonare acuta prevede che nella maggior parte dei casi , dopo la migrazione del trombo e la trombolisi endogena , venga ripristinata la totale perviet vascolare , senza alcuna ripercussione sullemodinamica polmonare [ 3 ]  . 
peraltro , se residuano difetti di riempimento endoluminali , le resistenze vascolari del circolo polmonare possono aumentare fino allistaurarsi di un quadro di ipertensione polmonare cronica [ 4 ]  . 
inoltre , lipertensione polmonare cronica pu instaurarsi in seguito ad un processo trombotico di natura non embolica , che si sviluppa localmente ; questa trombosi in situ caratterizza le forme di ipertensione polmonare idiopatica e quella associata alle cardiopatie congenite cianogene ( sindrome di eisenmenger )  . 
lembolia polmonare acuta , lipertensione polmonare cronica posttromboembolica e le forme di ipertensione polmonare cronica idiopatica e associata a cardiopatie congenite costituiscono pertanto , nellambito della malattia tromboembolica polmonare , un panorama ampio e diversificato , soprattutto in termini di scelte terapeutiche e categorie prognostiche . la tomografia computerizzata ( tc ) con studio angiografico attualmente il gold standard per la diagnosi di trombo - embolia polmonare , poich mostra direttamente la presenza dei difetti di riempimento endoluminali e permette di identificare altri segni indiretti [ 5 , 6 ]  . 
le caratteristiche morfologiche dei difetti di riempimento acuti e cronici , di natura embolica o trombotica locale che possibile individuare con tc non sono mai state valutate in modo sistematico in letteratura . 
in particolare i trombi polmonari non sono mai stati considerati nella fase sia preche post - contrastografica [ 711 ]  . alla luce di queste considerazioni , nel nostro lavoro abbiamo misurato la densit dei difetti di riempimento trombo - embolici acuti e cronici delle arterie polmonari sia prima che dopo somministrazione di mezzo di contrasto ; abbiamo correlato i valori densitometrici degli emboli acuti con quelli del sangue circolante nel tronco polmonare coradiol med ( 2012 ) 117 : 979991 materials and methods we consecutively reviewed cta scans performed between january 2006 and october 2009 , identified through a search of the picture archiving and communication system ( pacs ) , of 324 patients with pulmonary artery thromboembolisscans were considered if the patients fulfilled clinical criteria for suspected acute pe : presence of dyspnoea / tachypnoea , tachycardia , chest pain , cough , blood - tinged sputum with positive d - dimer test or signs of acute / subacute deep venous thrombosis . 
furthermore , we considered scans of patients with a haemodynamic diagnosis of pulmonary hypertension ( pulmonary artery pressure > 25 mmhg measured at rest by right heart catheterisation ) of three possible origins : pulmonary hypertension associated with chronic thromboembolic pulmonary hypertension ( cteph ) , associated with eisenmengers syndrome ( eis ) and idiopathic pulmonary arterial hypertension ( ipah ) [ 12 ]  . 
thromboembolic pulmonary hypertension was defined as a history of previous venous thromboses and / or pe in which the acute episode was excluded on clinical grounds ( absence of current vein thrombosis or of a verified emboligenic factor )  . 
other forms of pulmonary hypertension associated with pulmonary diseases , leftsided heart failure , pulmonary veno - occlusive disease and haematological , oncological , metabolic and systemic diseases ( sarcoidosis , angioleiomyoma , histiocytosis x ) were not taken into consideration . radiological criteria used to define acute emboli were complete or partial filling defects at the level of the pulmonary arteries , and , if partial , central or peripheral defects forming acute angles with the vascular wall . 
radiological criteria used to define chronic thrombi were preocclusive or partial parietal filling defects , forming obtuse angles with the vascular wall , often with intramural calcifications . we excluded 209 cases for the following reasons : 185 thromboemboli for dimensional reasons ( those located distally from the lobar branches or with thickness precluding adequate densitometric assessment ) ; ten filling defects of ascertained / suspected neoplastic origin ( two verified cases of pulmonary artery sarcoma and eight of suspected neoplastic emboli ) and one of parasitic origin ( one case of verified echinococcosis ) ; three studies degraded by motion artefacts ( respiratory , cardiac ) and ten by beam - hardening artefacts ( due to flow in the superior vena cava or adjacent intrathrombotic calcifications )  . 
thus the study finally assessed 115 patients who were subdivided into two groups on mune e quelli dei trombi cronici con la presenza di circoli sistemico - polmonari ipertrofici , come le arterie bronchiali . materiali e metodi questo studio ha esaminato , mediante ricerca su picture archiving and communication system ( pacs ) , in modo consecutivo , le indagini angio - tc di 324 pazienti con tromboembolia dellarteria polmonare in un periodo compreso da gennaio 2006 ad ottobre 2009 . 
sono state valutate le angiotc di pazienti che rispondevano ai criteri clinici compatibili con il sospetto di embolia polmonare acuta : presenza di sintomi quali dispnea / tachipnea , tachicardia , dolore toracico , tosse , emoftoe con d - dimero positivo , segni di trombosi venosa profonda acuta / subacuta . 
inoltre abbiamo valutato le angio - tc di pazienti con diagnosi emodinamica di ipertensione polmonare ( pressione arteriosa polmonare > 25 mmhg misurata a riposo mediante cateterismo cardiaco destro ) di tre eziologie : ipertensione polmonare associata a malattia tromboembolica polmonare cronica ( cteph ) , associata a sindrome di eisenmenger ( eis ) e forma idiopatica ( ipah ) [ 12 ]  . 
in particolare la forma di ipertensione polmonare post - tromboembolica stata definita da storia di pregressi eventi di trombosi venosa e / o embolia polmonare , nei quali per lepisodio acuto fosse clinicamente escluso ( assenza di trombosi venosa in atto o fonte emboligena accertata )  . 
non sono state considerate le altre forme di ipertensione polmonare associate a malattie polmonari , a scompenso cardiaco sinistro , a malattia polmonare veno - occlusiva , a malattie ematologiche , tumorali , metaboliche e sistemiche ( sarcoidosi , leiomiangiomatosi , istiocitosi x )  . i criteri radiologici per definire lembolo acuto sono stati : difetto di riempimento a livello delle arterie polmonari di tipo completo o parziale , questultimo centrale o periferico con angoli acuti rispetto alla parete del vaso . 
scans were acquired in the caudocranial direction from lung apices to bases during a single breath - hold , without electrocardiographic ( ecg ) gating , using the following parameters : slice thickness 1.25 mm , reconstruction increment 0.8 mm , 120 kv , 110 mas . patients in group b underwent pulmonary artery cta using a multislice somatom cardiac 16 ct scanner ( siemens )  . 
scans were acquired in the caudocranial direction from lung apices to bases during a single breath - hold , without ecg gating , using the following parameters : slice thickness 0.75 mm , reconstruction increment 0.5 mm , 120 kv , 120 mas . all scans were acquired before and after intravenous administration of approximately 100150 ml nonionic iodinated contrast material ( iomeron 350 ; bracco spa , milan , italy ) by automatic injector at a flow rate of 3 ml / s , followed by a 40 - ml bolus of saline solution . 
the scan delay was automatically determined by the bolus - tracking system , with a region of interest ( roi ) placed over the bifurcation of the common pulmonary trunk , with acquisition beginning at a threshold level of + 70 hu . 
precontrast acquisitions were always obtained to assess the pulmonary parenchyma , rule out other diseases ( aortic dissection , pneumonia , pneumothorax , lung cancer , etc . ) and select the roi for bolus tracking . 
we only assessed thromboemboli that could be seen on at least three consecutive axial scans and inside which at least three distinct rois could be traced , with a standard area of 20 mm2 ( 1 mm2 ) at a distance of at least 2 mm from the vascular wall . 
ne risultato un gruppo finale di 115 pazienti suddivisi in base alla diagnosi clinico - radiologica in due gruppi finali : gruppo a con diagnosi di embolia acuta , composto da 86 pazienti , di cui 32 maschi e 54 femmine , con et compresa da 41 a 96 anni ( et media di 74 , 4 anni ) ; gruppo b con diagnosi di trombosi cronica , composto da 29 pazienti , di cui 21 maschi e 8 femmine , con et compresa da 26 a 88 anni ( et media 61 anni ) , di cui 18 con ipertensione polmonare post - tromboembolica , 10 con ipertensione polmonare associata alla sindrome di eisenmenger ed 1 con la forma idiopatica . 
per i pazienti del gruppo a stato preso in esame il valore di ematocrito ( ht ) , valutato nella stessa giornata dellindagine tc . i pazienti del gruppo a sono stati sottoposti ad indagine angio - tc delle arterie polmonari utilizzando tomografo computerizzato multistrato somaton emotion 6 ( siemens , forcheim , germania )  . 
gli esami sono stati acquisiti in senso caudo - craniale , dagli apici alle basi polmonari , in singola apnea , senza sincronizzazione elettrocardiografica ( ecg ) , utilizzando i seguenti parametri : spessore di strato 1 , 25 mm , incremento di ricostruzione di 0 , 8 mm , 120 kv , 110 mas . i pazienti del gruppo b hanno eseguito indagine angiotc delle arterie polmonari utilizzando tomografo computerizzato multistrato somatom cardiac 16 ( siemens , forcheim , germania )  . 
gli esami sono stati acquisiti in senso caudo - craniale , dagli apici alle basi polmonari , in singola apnea , senza sincronizzazione ecg , utilizzando i seguenti parametri : spessore di strato di 0 , 75 mm , incremento di ricostruzione 0 , 5 mm , 120 kv , 120 mas . le acquisizioni sono state eseguite prima e dopo somministrazione di circa 100150 ml di mezzo di contrasto iodato non ionico ( iomeron 350 ; bracco spa , milano , italia ) endovena , al flusso di 3 ml / s , introdotto mediante iniettore automatico , seguito da un bolo di 40 ml di soluzione fisiologica . 
il ritardo di scansione stato determinato automaticamente mediante software di bolus tracking , con regione di interesse ( roi ) posizionata alla biforcazione del tronco polmonare comune ed inizio della scansione al raggiungimento della soglia prestabilita ( + 70 uh )  . 
la fase precontrastografica sempre eseguita per la valutazione del parenchima polmonare , al fine di escludere altre patologie ( dissezione aortica , polmoniti , pneumotorace , tumore polmonare , ecc . ) ed il posizionamento della roi del bolus tracking . 
we measured the difference in roi density after and before ce , setting a difference in density > 15 hu seen in at least one roi on three measurements as an arbitrary threshold value for significant ce . when studying chronic thrombi , we calculated mean attenuation values of the three precontrast measurements and mean ce values . 
in both groups , we calculated the difference in attenuation of thromboemboli compared with that of the pulmonary trunk during the precontrast phase ; to define a hyperattenuating or hypoattenuating thrombus , we used arbitrary threshold values of + 15 hu and 15 hu , respectively . 
as regards , in particular , acute emboli , occlusion was considered partial in the presence of partial vascular opacification and total when the filling defect completely occupied the lumen . 
in chronic thrombi , occlusion was defined as marked or mild depending on whether the thrombus occupied more or less than half of the lumen . statistical analysis to compare baseline attenuation levels of acute emboli with mean baseline levels of chronic thrombi , the nonparametric mannwhitney test was used . 
linear regression analysis was used to correlate ht levels with baseline attenuation measured at the level of the common pulmonary trunk and to correlate ht level with baseline attenuation values of acute emboli . 
fishers exact test was used to study possible associations ; in particular , we considered the association between the disease underlying pulmonary hypertension and the presence of intrathrombotic ce > 15 hu , the association between the underlying disease and the presence of hypertrophic bronchial arteries and the association between the presence of intrathrombotic ce > 15 hu and the presence of hypertrophic bronchial arteries . 
we also considered the association between degree of thrombotic occlusion and the presence of hypertrophic bronchial arteries and between degree of chronic thrombotic occlusion and intrathrombotic ce > 15 hu . 
sono stati valutati solo tromboemboli che fossero visualizzabili almeno in tre scansioni assiali consecutive ed allinterno dei quali si potessero tracciare almeno tre distinte roi con area standard di 20 mm2 ( 1 mm2 ) a distanza di almeno 2 mm dalla parete del vaso . 
per questo motivo sono stati valutati solo difetti di riempimento centrali , cio localizzati nei rami polmonari principali o allorigine delle diramazioni lobari . stato preliminarmente stabilito il punto in cui posizionare le aree , poi le valutazioni densitometriche sono state effettuate separatamente da due radiologi con diversi anni di esperienza in radiologia toracica ( fdl 5 anni e mz 30 anni ) , ottenendo risultati sovrapponibili . 
abbiamo calcolato la differenza densitometrica delle roi nelle due fasi di acquisizione , dopo e prima somministrazione di mezzo di contrasto ( mdc ) , stabilendo come cut off arbitrario per un ce significativo una differenza densitometrica > 15 uh , riscontrabile in almeno una roi su tre misurazioni . per i trombi cronici sono stati calcolati i valori medi di densit sulle tre misurazioni pre - contrastografiche ed i valori medi di contrast enhancement . 
in entrambi i gruppi stata calcolata la differenza di densit del trombo rispetto a quella del tronco polmonare in fase pre - contrastografica ; per definire un trombo iperdenso o ipodenso abbiamo stabilito arbitrariamente un cut off rispettivamente di + 15 uh e - 15 uh . 
 nei pazienti del gruppo b si valutata anche la presenza di circoli sistemico - polmonari locali come le arterie bronchiali ( ib )  . stata valutato qualitativamente il grado di occlusione vascolare . 
in particolare per gli emboli acuti , locclusione stata definita parziale quando era riscontrabile una parziale opacizzazione del vaso o totale quando il difetto di riempimento occupava completamente il lume . 
per i trombi cronici locclusione stata definita marcata o lieve a seconda che il trombo occupasse pi o meno della met del lume . analisi statistica per confrontare i valori densitometrici basali degli emboli acuti con quelli basali medi dei trombi cronici stato utilizzato il test di confronto non parametrico di mann - whitney . 
 abbiamo utilizzato un test di regressione lineare per correlare i valori di ematocrito con il valore densitometrico basale misurato a livello del tronco polmonare comune e 984 radiol med ( 2012 ) 117 : 979991 fig . 
a statistically significant correlation ( p = 0.000 ; r = 0.425 ) was found between ht and attenuation values of the common pulmonary trunk , whereas no correlation was found between baseline attenuation of acute emboli and ht levels . 
seventy - seven percent ( 27 / 35 ) of chronic thrombi had an attenuation difference < 15 hu compared with the common pulmonary trunk ; in 23% ( 8 / 35 ) of cases , the common pulmonary trunk had fig . 
2 dopo la somministrazione di mdc , il medesimo embolo acuto presentato in figura 1 non mostra significativo contrast enhancement . per correlare lematocrito con i valori densitometrici basali degli emboli acuti . 
il test esatto di fisher stato utilizzato per valutare le diverse associazioni ; in particolare abbiamo considerato lassociazione tra la patologia alla base del quadro di ipertensione polmonare e la presenza di un contrast enhancement intratrombotico > 15 uh , lassociazione tra la patologia di base e la presenza di arterie bronchiali ipertrofiche , lassociazione tra la presenza di contrast enhancement intratrombotico > 15 uh e la presenza di arterie bronchiali ipertrofiche . 
 stata inoltre considerata lassociazione tra grado di occlusione trombotica e presenza di arterie bronchiali ipertrofiche e tra grado di occlusione del trombo cronico e contrast enhancement intratrombotico > 15 uh . 
valori di p minori o uguali a 0 , 05 sono stati considerati significativi . risultati il valore medio di densit pre - contrastografica dei trombi acuti stato di 54 , 9 uh [ 11 , 4 deviazione standard ( ds ) ]  . 
il 47% ( 40 / 86 ) degli emboli acuti con valori densitometrici medi di 47 , 1 uh ( 9 , 1 ds ) ha mostrato una differenza densitometrica < 15 uh ( 4 uh ) riradiol med ( 2012 ) 117 : 979991 fig . 
3 valori densitometrici in fase pre - contrastografica degli emboli acuti ( valore medio 54 , 9 uh ) e dei trombi cronici ( valore medio 33 , 8 uh )  . spetto al tronco polmonare comune , che presentava valori densitometrici medi di 43 , 1 uh ( 6 , 7 ds )  . 
il 45% ( 39 / 86 ) dei pazienti aveva un ematocrito sotto i valori di riferimento , in particolare 21 erano femmine ( ematocrito medio di 34 , 12 , 0 ds ) e 18 maschi ( ematocrito medio 36 , 80 , 5 )  . 
esiste una correlazione statisticamente significativa ( p = 0 , 000 ; r = 0 , 425 ) tra valori di ematocrito ed i valori densitometrici del tronco polmonare comune ; non stata rilevata invece alcuna correlazione tra la densit basale degli emboli acuti e lematocrito . 
il valore densitometrico medio degli emboli acuti dopo contrasto risultato 55 , 1 uh ( 11 , 4 ds ) ; la differenza tra valori densitometrici in fase poste pre - contrastografica degli emboli acuti risultata 0 , 2 uh . i trombi cronici hanno mostrato una densit basale media di 33 , 8 uh ( 7 , 7 ds ) , mentre il tronco polmonare comune di 43 , 3 uh ( 6 , 8 ds )  . 
il 77% ( 27 / 35 ) dei trombi cronici ha mostrato una differenza densitometica < 15 uh rispetto al tronco polmonare comune ; nel 23% ( 8 / 35 ) dei casi il tronco polmonare comune ha mostrato valore densitometrico basale > 15 uh rispetto ai valori densitometrici basali medi dei trombi cronici . 
di questi 19 casi , 2 trombi hanno mostrato un incremento densitometrico > 15 uh in ununica misurazione delle tre calcolate ; 13 su 19 lhanno mostrato in due su tre misurazioni ed i restanti 4 in tutte e tre le aree calcolate . 
i trombi con contrast enhancement superiore alla soglia stabilita sono stati rilevati in 12 dei 18 pazienti con diagnosi di ipertensione polmonare post - tromboembolica cronica ( 66% ) , in 4 dei 10 pazienti con ipertensione polmonare associata a sindrome di eisenmenger ( 40% ) e nellunico paziente con ipertensione polmonare idiopatica . 
 visto il meccanismo patogenetico comune di queste ultime due forme di ipertensione arteriosa polmonare ( associate a cardiopatie congenite e forma idiopatica ) abbiamo considerato i pazienti con trombosi in situ come una unica categoria patologica rispetto alla malattia post - tromboembolica . 
anche in questo caso non stata rilevata unassociazione significativa ( p = 0 , 72 ) tra presenza di arterie bronchiali ipertrofiche ( ib ) e la patologia di base . dai nostri dati emersa una significativa correlazione fig . 
7 il medesimo trombo presentato in figura 6 mostra significativo ed omogeneo contrast enhancement . in only one of the three measurements ; 13 of 19 showed an increase in two of three measurements and the remaining four in all three rois . 
thrombi with ce exceeding the defined threshold were identified in 12 of 18 patients with a diagnosis of cteph ( 66% ) , in four of the ten with pulmonary hypertension associated with eis ( 40% ) and in the only patient with idiopathic pulmonary hypertension . 
 on the basis of the common pathogenetic mechanism of the two latter forms of pulmonary arterial hypertension ( associated with congenital heart diseases and idiopathic forms ) , we considered patients with thrombosis in situ to form a single pathological category compared with thromboembolic disease . 
in 13 of 17 patients with bronchial artery hypertrophy , intrathrombotic ce > 15 hu coexisted : in nine patients with thromboembolic pulmonary hypertension , in three with pulmonary hypertension associated with eis and in the only patient with idiopathic pulmonary hypertension . 
the degree of vascular occlusion did not correlate significantly either with the presence of thrombotic ce higher than the established threshold ( p = 0.711 ) or with tra la presenza di arterie bronchiali ipertrofiche e contrast enhancement intra - trombotico ( p = 0 , 026 ) : in 13 su 17 pazienti con ipertrofia delle arterie bronchiali era presente anche contrast enhancement intratrombotico > 15 uh ed in particolare in 9 pazienti con ipertensione polmonare posttromboembolica , in 3 pazienti con ipertensione polmonare associata a sindrome di eisenmenger e nellunico paziente con ipertensione polmonare idiopatica . 
il grado di occlusione vascolare non risultato significativamente correlato n alla presenza di contrast enhancement trombotico maggiore della soglia stabilita ( p = 0 , 711 ) n alla presenza di arterie bronchiali ipertrofiche ( p = 0 , 999 )  . discussione dallanalisi dei nostri dati emerso che gli emboli acuti mostrano in pi della met dei casi valori densitometrici basali maggiori di 15 uh rispetto al tronco polmonare comune . 
la significativa correlazione che abbiamo riscontrato tra valori dellematocrito ed i valori densitometrici calcolati a livello del tronco polmonare comune evidenzia laccuratezza delle tc attuali nella determinazione delle densit , come gi dimostrato in precedenti studi [ 13 , 14 ]  . 
 la mancata correlazione tra la densit basale degli emboli acuti e lematocrito indica che le caratteristiche tomodensitometriche dellembolo acuto dipendono prevalentemente dalla sua struttura intrinseca piuttosto che dalle caratteristiche reologiche del circolo . 
the significant correlation found between ht levels and attenuation values measured at the common pulmonary trunk is proof of the accuracy of modern ct systems in determining attenuation , as reported in previous studies [ 13 , 14 ]  . 
the lack of correlation between baseline attenuation of acute emboli and ht indicates that densitometric features of acute emboli largely depend on their intrinsic structure rather than on the rheological characteristics of circulating blood . 
this finding can be explained by considering the mechanisms at play in the early stages of an acute thrombus : the thrombus retracts and loses its water content , which leads to an increase in concentration of haemoglobin and , consequently , to a higher attenuation compared with the blood circulating through the pulmonary vasculature [ 15 ]  . 
none of the acute emboli in our series showed significant ce ; this is easily understood if we consider that acute thrombi are composed of fibrin and erythrocytes , platelets and necrotic blood cells . 
when occlusive or preocclusive emboli are identified in the central pulmonary vessels , and we assume from clinical data that they have an acute origin even when time of onset is unknown we can suppose that they still have this inert structure and that the organisation mechanisms have not yet been triggered . chronic thrombi were found to be mainly isoattenuating to the common pulmonary trunk on precontrast scans . 
the difference between baseline attenuation of acute emboli and mean attenuation of chronic thrombi was statistically significant ; in particular , it emerged that acute emboli have higher baseline attenuation values compared with chronic thrombi . the only published study to have measured the density of chronic thrombi was conducted by wittram et al . 
the additional strength of our study compared with the existing literature radiol med ( 2012 ) 117 : 979991 liperdensit basale dei trombi acuti gi stata riscontrata in letteratura [ 7 , 8 , 10 ]  . 
questo dato potrebbe essere spiegato considerando i meccanismi che si innescano precocemente a carico del trombo acuto : il trombo si retrae , perde il suo contenuto idrico con conseguente aumento della concentrazione di emoglobina , che si traduce in una maggior attenuazione rispetto al sangue circolante nel circolo polmonare [ 15 ]  . 
la totalit degli emboli acuti della nostra casistica non ha mostrato una significativa captazione di mezzo di contrasto ; questo risultato facilmente comprensibile se si considera che il trombo acuto costituito da fibrina e aggregati di eritrociti , piastrine e cellule ematiche necrotiche . 
quando identifichiamo emboli occludenti o suboccludenti a carico dei vasi polmonari centrali , assumendo dai dati clinici che siano di origine acuta , pur non conoscendone let dinsorgenza , possiamo supporre che siano ancora costituiti da questa struttura inerte sulla quale non si sono ancora innescati meccanismi di organizzazione . i trombi polmonari cronici sono risultati , in fase precontrastografica , prevalentemente isodensi rispetto al tronco polmonare comune . 
la differenza di densit basale di emboli acuti rispetto a quella media dei trombi cronici risultata statisticamente significativa ; in particolare dai nostri dati emerso che gli emboli acuti hanno valori densitometrici basali maggiori dei trombi cronici . in letteratura lunico studio che aveva gi valutato la densit dei trombi cronici stato quello di wittram et al . 
uno studio istologico condotto su circa 200 campioni di pezzi chirurgici post - endoarteriectomia polmonare mostra che nella maggior parte dei casi i trombi cronici post - embolici sono costituiti da solo materiale in fase di avanzata radiol med ( 2012 ) 117 : 979991 lies in the evaluation of intrathrombotic ce . 
this degree of ce may be explained by considering the organisation processes occurring in chronic thromboemboli and in thrombi of local origa histological study conducted on approximately 200 surgical specimens after pulmonary endarterectomy showed that in most cases , chronic postembolic thrombi are only composed of material at an advanced stage of organisation or are associated with fibradditionally , inflammatory cell infiltrates were observed around the newly developed vessels [ 16 ]  . 
 according to some experimental models , this process takes place though the formation of new intrathrombotic vessels , supported by the cooperation of monocytes / macrophages ( mcs / mph ) and endothelial progenitor cells ( epcs ) not circulating within the occluded vessel but infiltrating into the thrombotic region through collateral vessels [ 17 ]  . 
 it is known that in pulmonary vascular obstruction , the bronchial arteries , which normally supply the bronchovascular structures , take on the vicarious function of the pulmonary circulation through the formation of systemicpulmonary anastomoses . 
several experimental studies have demonstrated that in acute pulmonary embolism , bronchial artery flow is reduced [ 18 , 19 ] , whereas other studies suggest that bronchial artery hypertrophy is a peculiar feature of chronic thromboembolism [ 20 ]  . 
in particular , analysis of patients with eis revealed that all those who had posttricuspid defects ( two with an interventricular defect and one with a single ventricle ) had systemicpulmonary shunts , whereas these findings were present in only half of patients with pretricuspid defects ( that is , with interatrial defects such as ostium secundum or sinus venosus defects )  . 
 however , the small number of patients studied does not allow for definite conclusions . several authors attempted to demonstrate an association between bronchial artery hypertrophy and other parenchymal signs of thromboembolic pulmonary hypertension . 
secondo alcuni modelli sperimentali questo processo avviene attraverso la neoformazione di vasi intra - trombotici sostenuta dalla cooperazione di cellule monocitarie / macrofagiche ( mcs / mph ) e cellule progenitrici della linea endoteliale ( epcs ) non circolanti nel vaso sede dellocclusione ma infiltrate nella sede trombotica attraverso vasi collaterali [ 17 ]  . 
 noto che le arterie bronchiali , normalmente deputate al nutrimento delle strutture broncovasali , in caso di ostruzione vascolare polmonare , assumono funzione vicariante del circolo polmonare , attraverso la formazione di anastomosi sistemico - polmonari . 
alcuni studi sperimentali hanno dimostrato che nelle embolie polmonari acute il flusso delle arterie bronchiali si riduce [ 18 , 19 ] , mentre altri lavori sostengono che lipertrofia delle arteria bronchiali sia una caratteristica peculiare delle forme tromboemboliche croniche [ 20 ]  . 
analizzando in particolare il gruppo di pazienti con sindrome di eisenmenger si osserva che tutti quelli con difetto di tipo post - tricuspidalico ( 2 pazienti con difetto interventricolare ed 1 con ventricolo unico ) presentano circoli sistemico - polmonari , mentre li presentano solo la met dei pazienti con difetto pre - tricuspidalico ( cio difetti interatriali tipo ostium secundum o tipo seno venoso )  . 
questo dato pu trovare spiegazione nelle differenze emodinamiche tra le due categorie di cardiopatie ; peraltro lesiguit della popolazione studiata non consente di trarre conclusioni definitive . in letteratura si cercato pi volte di dimostrare lassociazione tra lipertrofia delle arterie bronchiali ed altri segni parenchimali dellipertensione polmonare post - tromboembolica , ma in nessun altro lavoro come nel nostro si dimostrata una cos stretta relazione come quella trovata con lenhancement trombotico ( p = 0 , 026 ) : nel 76 , 5% dei casi i due reperti sono concomitanti . se riconduciamo il contrast enhancement trombotico ai fenomeni di neovascolarizzazione intra - trombotici , dobbiamo ricordare che inizialmente lapporto delle cellule implicate nella neoangiogenesi avviene attraverso circoli collaterali che circondano il vaso ostruito [ 17 ]  . 
alla luce di queste considerazioni e dei nostri risultati possiamo ragionevolmente ipotizzare che il ruolo di circoli collaterali deputati alla ricanalizzazione del trombo cronico sia rivestito proprio dalle arterie bronchiali . il riscontro di un enhancement intra - trombotico , infine , ci pone inevitabilmente di fronte ad un gravoso problema 990 radiol med ( 2012 ) 117 : 979991 sonably hypothesise that the role of collateral circulations involved in recanalisation of the chronic thrombus could be played by the bronchial arteries . finally , the finding of intrathrombotic contrast enhancement raises a serious problem of differential diagnosis with pulmonary artery angiosarcoma . 
 furthermore , the coexistence of thromboembolic events in oncological patients is not a rare occurrence ; a tumour provides excellent ground for embolus development , facilitating its establishment and further complicating diagnosis of the nature of the filling defects . 
 the limitations of our study are a lack of histological correlates defining the exact structure of acute and chronic thrombi and the actual vascularity of the chronic thrombus by bronchial arteries . 
the number of patients with chronic thrombi is still too limited to allow any confident statement of the fact that chronic thrombi are specifically characterised by significant contrast enhancement ; in particular , idiopathic pulmonary hypertension was diagnosed in one patient only . conclusions our study proved that in the precontrast phase , most acute pulmonary emboli have a higher attenuation than the common pulmonary trunk . 
we suggest paying particular attention to the search for filling defects occluding the pulmonary arteries on unenhanced cta scans , particularly in emergency settings and patient instability , even when there is no clinical suspicion of pulmonary embolism . postembolic or local chronic thrombi showed increased attenuation during the postcontrast phase in more than half of cases . 
in particular , thrombotic ce was significantly associated with the presence of hypertrophic bronchial arteries , which indicates that the local systemicpulmonary circulation may play a role in intrathrombotic vascularity . 
 larger series and an accurate assessment of thrombus attenuation and systemicpulmonary circulation could expand current knowledge of the pathophysiological and adaptive mechanisms leading to the development of persistent pulmonary artery hypertension , with major repercussion for identifying patients at risk and for treatment decisions . di diagnosi differenziale rispetto allangiosarcoma dellarteria polmonare . 
in pazienti oncologici inoltre non raro il concomitare di eventi tromboembolici ; gli emboli trovano nel focus tumorale un ottimo terreno di accrescimento che ne facilita la cronicizzazione e complica ulteriormente la diagnosi di natura del difetto di riempimento stesso . 
 i limiti del nostro studio risiedono nella mancanza di riscontri istologici che accertino la reale struttura dei trombi sia acuti che cronici e leffettiva vascolarizzazione del trombo cronico da parte delle arterie bronchiali . 
la popolazione di pazienti con trombi cronici ancora poco numerosa per poter asserire con certezza che questi siano specificatamente caratterizzati da un significativo contrast enhancement ; in particolare la forma idiopatica di ipertensione polmonare rappresentata da un unico caso . conclusioni il nostro studio ha mostrato che la maggior parte degli emboli polmonari acuti in fase pre - contrastografica avevano una densit maggiore rispetto al tronco polmonare comune . 
possiamo suggerire di porre particolare attenzione nella ricerca di difetti di riempimento occlusivi delle arterie polmonari anche nelle tc eseguite senza mezzo di contrasto , soprattutto in condizioni di emergenza ed instabilit del paziente , anche senza il sospetto clinico di embolia polmonare . i trombi cronici , di origine post - embolica o locale , hanno mostrano in pi della met dei casi un incremento densitometrico in fase post - contrastografica . 
 un ampliamento numerico della casistica ed unaccurata valutazione della densit trombotica e dei circoli sistemico - polmonari potrebbero incrementare le conoscenze dei meccanismi fisiopatologici ed adattativi che contribuiscono allo sviluppo dellipertensione arteriosa polmonare persistente , con importanti ripercussioni nellidentificazione di categorie di pazienti a rischio e nelle scelte terapeutiche . conflict of interest none 1 . 
gemelli 8 , 00168 roma , italy 2laboratorio di fisica medica e sistemi esperti , istituto nazionale tumori regina elena , roma , italy 3istituto di radiodiagnostica , ospedale pediatrico bambino ges , roma , italy 4radiologia e diagnostica per immagini , istituto nazionale tumori regina elena , roma , italy correspondence to : a.r. 
this study compared the sensitivity of two commercial computer - aided detection ( cad ) systems in identifying noncalcified pulmonary nodules on low - dose multidetector computed tomography ( mdct ) scans by using a double reference standard . 
three chest low - dose mdct scans of patients who had undergone lung cancer screening were retrospectively analysed using two distinct commercial cad systems : lungcad vc10a , siemens medical solutions ( cad1 ) and lungvcar , ge healthcare ( cad2 )  . 
two panels of experienced thoracic radiologists from two different institutions independently established two reference standards ( rs1 , rs2 ) by identifying the true positive findings with spatial coordinates without using cad . 
tre esami tcmd a bassa dose del torace di pazienti sottoposti a screening del tumore polmonare sono stati retrospettivamente analizzati mediante due diversi sistemi cad disponibili in commercio ( lungcad vc10a , siemens medical solutions ; cad1 ) ( lungvcar , ge healthcare ; cad2 )  . 
la posizione esatta secondo le coordinate spaziali ( x , y , z ) di ogni reperto identificato automaticamente da ciascuno dei due sistemi stata registrata da un lettore indipendente . 
due gruppi di radiologi toracici esperti , appartenenti a due diverse istituzioni , hanno stabilito in modo indipendente i due rispettivi standard di riferimento ( sr1 , sr2 ) , identificando i reperti veri positivi mediante coordinate spaziali , senza luso del cad . 
il numero totale 954 radiol med ( 2012 ) 117 : 953967 correctly identified 11 / 34 nodules ( sensitivity 35% ) for rs1 and 13 / 54 ( sensitivity 23% ) for rs2 . 
il cad1 ha identificato correttamente 13 / 34 noduli ( sensibilit 38% ) indicati da sr1 e 17 / 54 ( sensibilit 30% ) indicati da sr2 , mentre il cad2 ha identificato 11 / 34 noduli ( sensibilit 35% ) indicati da sr1 e 13 / 54 ( sensibilit 23% ) indicati da sr2 . 
 parole chiave cad noduli polmonari tomografia computerizzata multidetettore bassa dose introduction introduzione lung cancer is a potentially curable disease when detected at an early stage [ 1 , 2 ]  . 
this has led to the development of numerous low - dose spiral computed tomography ( ct ) screening programmes , over the past 10 years , as ct is a reliable technique for detecting smaller and earlier lung cancers compared with standard chest radiography [ 36 ]  . 
the introduction of multidetector ct ( mdct ) has further improved the spatial resolution and sensitivity of the technique in identifying pulmonary nodules , particularly when small [ 7 ]  . 
as a result , since the late 1990s , there has been a considerable development in automated systems for detecting pulmonary nodules , which are known as computer - aided detection ( cad ) systems [ 8 , 9 ]  . 
 [ 10 ] demonstrated that 84% of lung cancers missed in a screening programme were correctly identified by an automated system . cad performance is usually tested by measuring the systems sensitivity , that corresponds to the number of true pulmonary nodules identified , and the number of false positive results it produces . 
when testing the performance of a cad system or comparing the performance of several such systems , choosing the strategy for defining the truth , or the reference standard against which to evaluate cad reil tumore polmonare potenzialmente curabile quando identificato in stadio iniziale [ 1 , 2 ]  . 
ci ha indotto negli ultimi dieci anni lo sviluppo di numerosi programmi di screening del tumore polmonare con tomografia computerizzata ( tc ) spirale a bassa dose , in quanto metodica in grado di identificare tumori polmonari di pi piccole dimensioni e in stadio pi precoce rispetto allesame radiografico del torace [ 36 ]  . 
 lintroduzione della tc multidetettore ( tcmd ) ha ulteriormente migliorato la risoluzione spaziale e la sensibilit della metodica nella identificazione dei noduli polmonari , in particolare di piccole dimensioni [ 7 ]  . 
 [ 6 ] riporta che nel 26% dei pazienti sottoposti al primo controllo tc annuale sono stati identificati retrospettivamente noduli polmonari non documentati allesame tc di base [ 6 ]  . 
sulla base di questi presupposti , a partire dalla fine degli anni 90 , si avuto un notevole sviluppo dei sistemi automatici per lidentificazione dei noduli polmonari , denominati computer - aided detection ( cad ) [ 8 , 9 ]  . 
 la performance di un cad viene solitamente testata valutando la sensibilit del sistema , ovvero il numero dei noduli polmonari veri identificati , e il numero dei falsi positivi che esso produce . 
quando si vuole testare la performance di un cad o confrontare la performance di pi sistemi , di fondamentale importanza la scelta della strategia utilizzata per stabilire la verit o standard di riferimento rispetto al quale confrontare i risultati del cad [ 12 , 13 ]  . 
all of these studies used a single reference standard consisting of a panel of experienced thoracic radiologists who reviewed the images in consensus or independently , with an additional reader being asked to settle any disagreement , and established which cad findings were real nodules ( true positives )  . 
 [ 12 ] , however , demonstrated a substantial interreader variability in detecting pulmonary nodules and showed that the performance of experienced chest radiologists in establishing the reference standard may not be the best when compared with that of other experienced thoracic radiologists . 
the purpose of our study was therefore to compare the sensitivity of two different commercial cad systems in detecting noncalcified pulmonary nodules on lowdose mdct examinations for lung cancer screening by using two independent reference standards . materials and methods study population and ct technique our study was approved by the ethics committee of regina elena national cancer institute in rome . 
three chest low - dose mdct scans of participating patients ( two men , one woman ; mean age 58.7 years ; age range 5564 years ) were retrospectively identified . 
the criterion for selecting the scans was a finding of numerous pulmonary nodules for each patient in order to limit the sample size while ensuring adequate statistical power to conduct a lesion - level analysis rather than a patient - level analysis [ 20 ]  . all ct scans were performed with a 4 - slice mdct scanner ( somatom sensation 4 ; siemens medical solutions , forchheim , germany )  . 
acquisition parameters were as follows : detector configuration 41.25 mm ; kvp 120 ; mas 40 ; rotation time 0.5 s ; field of view ( fov ) 4044 studi in letteratura hanno testato la performance dei cad e dimostrato limpatto positivo di questi software nella identificazione dei noduli polmonari da parte del radiologo [ 1419 ]  . 
in tutti questi lavori stato utilizzato uno standard di riferimento unico rappresentato da pi radiologi toracici esperti che , per consenso o in modo indipendente e con lintervento di un ulteriore lettore per risolvere il disaccordo , hanno revisionato le immagini e stabilito quali reperti erano noduli veri ( veri positivi )  . 
 [ 12 ] , stata osservata , tuttavia , una sostanziale variabilit tra radiologi diversi nella identificazione dei noduli polmonari ed stato dimostrato che la performance di radiologi toracici esperti nel determinare lo standard di riferimento pu non essere la migliore , quando confrontata con quella di altri radiologi toracici esperti . 
 al meglio delle nostre conoscenze , a tuttoggi , non esistono in letteratura lavori che abbiano testato la sensibilit dei sistemi automatici di identificazione dei noduli polmonari utilizzando pi di uno standard di riferimento . 
obiettivo del nostro lavoro stato , pertanto , quello di confrontare la sensibilit di due diversi sistemi cad commerciali nella identificazione dei noduli polmonari non calcifici negli esami tcmd a bassa dose di screening del tumore polmonare , utilizzando due standard di riferimento indipendenti . materiali e metodi popolazione di studio e tecnica tc il lavoro stato approvato dal comitato etico dellistituzione in cui si svolge il programma di screening del tumore polmonare , ancora in corso ( istituto nazionale tumori regina elena di roma )  . 
sono stati identificati retrospettivamente 3 esami tcmd del torace a bassa dose di 3 pazienti sottoposti a screening del tumore polmonare ( 2 uomini , 1 donna ; et media : 58 , 7 anni ; range di et : 5564 anni )  . 
il criterio di selezione degli esami stato il riscontro di numerosi noduli polmonari per ciascun paziente , al fine di ridurre la numerosit campionaria da esaminare mantenendo un sufficiente potere statistico per lo svolgimento di unanalisi per lesione piuttosto che per paziente [ 20 ]  . tutti gli esami tc sono stati acquisiti dagli apici alle basi polmonari , in apnea inspiratoria , mediante limpiego di un apparecchio tc multidetettore a 4 strati ( somatom sensation 4 , siemens medical solutions , forchheim , germania ) , secondo un protocollo per screening del tumore polmonare a bassa dose . 
i parametri di acquisizione sono stati : configurazione dei detettori = 41 , 25 mm ; kvp = 120 ; mas = 40 ; tempo di rotazione = 0 , 5 secondi ; field of view ( fov ) = 4044 cm ; matrice di acquisizione = 512512 pixel . 
ct images were transferred to two separate workstations for image analysis : siemens medical solutions ( ws1 ) and advantage ge healthcare ( ws2 )  . struzione sono stati : spessore di strato = 1 mm ; intervallo = 1 mm ; algoritmo di ricostruzione ( kernel ) = b50f ( siemens medical solutions )  . 
le immagini tc sono state trasferite su due workstation distinte ( ws1 , siemens medical solutions ; ws2 , advantage ge healthcare ) per lanalisi delle immagini . image analysis and reference standards one reader ( a radiologist with 8 years of experience in thoracic imaging ) analysed , retrospectively and blinded to the reference standards , the three mdct scans using two different commercially available cad systems : lungcad vc10a , siemens medical solutions , forchheim , germany ( cad1 ) and lungvcar , ge healthcare , milwaukee , wi , usa ( cad2 )  . 
the reader recorded the ct image number ( z ) , the x and y coordinates in the axial plane and the size of all outputs generated by each of the two cad systems , without applying any dimensional threshold and without formulating any diagnostic judgement ( true nodule / false nodule ) ( cad used as a stand - alone system ) or knowing the reference standards results . 
the spatial coordinates for each finding were generated considering the lower left corner of the 512512 matrix as point zero of the x and y axes of each axial reference image . 
 this allowed us to precisely locate the tridimensional ( 3d ) position of each output provided by the two software programmes on each exam . in order to test the sensitivity of the two cad systems , defined for each nodular lesion ( lesion - level analysis ) , we used two independent reference standards reference standard 1 ( rs1 ) and 2 ( rs2 ) represented by two panels of three experienced thoracic radiologists ( average group experience 10 years ) from two different institutions . 
each rs independently analysed the images , blinded to the other group and at different times ( rs1 first and then rs2 ; the radiologists of rs2 were aware that their assessments would be compared with those of rs1 ) , without using the cad system ; they identified in consensus all true noncalcified pulmonary nodules , regarded as true positives ( tp ) , without expressing any probability judgement on the remaining findings . 
solid ( s ) , nonsolid ( ns ) and partly solid ( ps ) nodules , that is , those consisting of a solid and a nonsolid component were considered . 
focal thickening of the bronchial walls and all nonrounded opacities were analisi delle immagini e standard di riferimento un lettore ( radiologo con esperienza di 8 anni nellimaging toracico ) ha analizzato , retrospettivamente ed in cieco rispetto agli standard di riferimento , i tre esami tcmd , utilizzando due diversi sistemi cad disponibili in commercio ( cad1 , lungcad vc10a , siemens medical solutions , forchheim , germany ; cad2 , lungvcar , ge healthcare , milwaukee , wi , usa )  . 
il lettore ha registrato il numero dellimmagine tc ( z ) , le coordinate x , y sul piano assiale e le dimensioni di ciascuno dei reperti generati da ciascuno dei due sistemi cad , senza applicare alcuna soglia dimensionale e senza esprimere alcun giudizio diagnostico ( nodulo vero / nodulo falso ) ( metodo di utilizzo del cad da solo o stand - alone ) n conoscere i risultati dello standard di riferimento . 
le coordinate spaziali di ciascun reperto sono state generate considerando come punto 0 dellasse x e dellasse y langolo inferiore sinistro della matrice 512512 , relativa a ciascuna immagine assiale di riferimento . 
le misurazioni della distanza di ciascun reperto polmonare , rispetto allasse x ed y , sono state effettuate con metodo manuale mediante calibro elettronico sulla ws2 e con metodo semiautomatico sulla ws1 . 
questo ha consentito di identificare spazialmente lesatta posizione tridimensionale ( 3d ) di ciascun reperto identificato dai due software in ciascun esame . per testare la sensibilit dei due sistemi cad , definita per lesione nodulare ( analisi per lesione ) , abbiamo utilizzato due standard di riferimento indipendenti , lo standard di riferimento 1 ( sr1 ) e lo standard di riferimento 2 ( sr2 ) , costituiti da due gruppi di tre radiologi toracici esperti ( esperienza media simile di 10 anni / gruppo ) appartenenti a due istituzioni differenti . 
ciascuno dei due sr ha analizzato le immagini in modo indipendente e blindato dallaltro , in tempi differenti ( prima sr1 e poi sr2 ; sr2 era a conoscenza che le sue valutazioni sarebbero state confrontate con quelle di sr1 ) , senza lausilio del cad , identificando per consenso tutti i noduli polmonari non calcifici certi , ritenuti veri positivi ( vp ) , senza esprimere alcun giudizio di probabilit sui restanti reperti . 
 sono stati considerati noduli a densit solida ( s ) , non solida ( ns ) e parzialmente solida ( ps ) , ovvero costituiti da una componente solida e da una non solida . 
il nodulo identificato mediante un cerchio rosso dal cad1 ( b ) e mediante un punto rosso dal cad2 ( c )  . excluded , as were diffusely calcified pulmonary nodules , given that diffuse calcifications are highly suggestive of benign lesions ( granuloma , hemartoma ) and have no clinical significance . 
for each true nodule , we recorded the number of the ct image in which it was detected ( z ) ; its spatial location in the axial plane according to the x and y coordinates , calculated with the method reported above ; and its morphological and densitometric features ( diameter ; regular or irregular margins ; solid , part solid or nonsolid density )  . 
 all findings reported by each cad system were compared with the true pulmonary nodules identified by each rs in order to measure the sensitivity of each cad systethe outputs of the two cad systems whose location did not correspond with that of the findings identified by each rs were indicated as cad false positives ( fp ) , and no confidence score was assigned . 
all fp outputs provided by each cad system were later re - evaluated by another independent reader ( a radiologist with 5 years experience in thoracic radiology ) who used spatial coordinates indicated by the first reader to identify the output and report its morphological features . statistical analysis all data obtained were entered into an electronic spreadsheet ( excel 2003 , microsoft corp . , redmond , wa , usa )  . 
the sensitivity of each cad system , as measured using lesionlevel analysis , was tested by calculating the ratio between the number ( overall and per patient ) of outputs provided by ca altamente probativo di benignit ( granuloma , amartoma ) e non rivestono interesse clinico . 
per ciascun nodulo certo sono stati registrati il numero dellimmagine assiale in cui era identificabile ( z ) , la localizzazione spaziale sul piano assiale secondo le coordinate cartesiane ( x e y ) , calcolate con lo stesso metodo sopra riportato , e le caratteristiche morfodensitometriche ( diametro , margini regolari o irregolari , densit solida , parzialmente solida o non solida )  . 
 tutti i reperti segnalati da ciascuno dei due sistemi cad sono stati confrontati con i noduli polmonari certi ( vp ) identificati dai due standard di riferimento , allo scopo di valutare la sensibilit di ciascun sistema cad . 
i reperti segnalati dai due sistemi cad la cui localizzazione non coincideva con quella dei reperti identificati dai due standard di riferimento sono stati indicati come falsi positivi ( fp ) del cad , senza assegnare loro uno score di confidenza . 
tutti i reperti fp segnalati da ciascun sistema cad sono stati rivalutati , in un tempo successivo , da un ulteriore lettore indipendente ( radiologo con esperienza di 5 anni in radiologia toracica ) che ha utilizzato le coordinate spaziali indicate dal primo lettore per identificare ciascun reperto e riportarne le caratteristiche morfologiche . analisi statistica tutti i dati ottenuti sono stati tabulati su foglio elettronico ( excel 2003 , microsoft corp . , redmond , wa , usa )  . 
la sensibilit di ciascun sistema cad , valutata con metodo di analisi per lesione , stata testata calcolando il rapporto tra il numero ( globale e per singolo paziente ) dei reperti identificati dal cad e il numero ( globale e per singolo paziente ) dei reperti identificati da ognuno dei due standard di rife958 radiol med ( 2012 ) 117 : 953967 the cad system and the number ( overall and per patient ) of findings identified by each rs . 
comparison between diameter of the findings identified by the cad systems and between sensitivity values and number of fp of each cad system was performed using the student t test , with = 0.05 ( p < 0.05 indicative of statistically significant difference between systems )  . 
il confronto tra il diametro dei reperti identificati dai due sistemi cad , cos come il confronto tra i valori di sensibilit e tra il numero dei falsi positivi di ciascun cad stato effettuato mediante il test t di student , con di 0 , 05 ( p < 0 , 05 indicativo di differenza statisticamente significativa tra i due sistemi )  . 
 risultati results standard di riferimento e caratteristiche dei noduli reference standards and nodule features rs1 identified 34 noncalcified pulmonary nodules , considered to be real nodules and therefore tp findings . 
seventeen of the 88 nodules were identified by both rs ( 34 for rs1 , 54 for rs2 ) ( 20% ) ( mean diameter 3.2 mm ; range 28.8 mm ) , 15 of which were s , and 2 were interpreted as ps by rs1 and as ns by rs2 . 
reference standards with respect to rs1 , cad1 correctly identified 13 of the lo standard di riferimento 1 ( sr1 ) ha individuato 34 noduli polmonari non calcifici , considerati come noduli certi e quindi reperti veri positivi ( vp ) , di cui 29 s ( 85% ) e 5 ps ( 15% ) , 23 con margini regolari ( 68% ) e 11 irregolari ( 32% ) e con diametro medio di 4 , 2 mm ( range 28 , 8 mm )  . 
sono stati riconosciuti da entrambi gli standard di riferimento 17 noduli sugli 88 totali ( 34 per sr1 , 54 per sr2 ) ( 20% ) ( diametro medio 3 , 2 mm ; range 28 , 8 mm ) , di cui 15 s e 2 interpretati come ps da sr1 e come ns da sr2 . 
standard di riferimento in rapporto allo standard di riferimento 1 ( sr1 ) , il cad1 ha identificato correttamente 13 dei 34 reperti veri positivi ( vp ) , con un valore di sensibilit complessiva del 38% , mentre il cad2 ne ha identificati correttamente 11 , con una sensibilit complessiva del 35% ( tabella 3 )  . 
for each patient , number , dimension and densitometric and morphological features of the nodules are reported tabella 1 numero e caratteristiche dei noduli identificati dallo standard di riferimento 1 ( sr1 )  . 
for each patient , dimension and densitometric and morphological features of the nodules are reported rs2 patient 2 patient 3 patient 1 total tabella 2 numero e caratteristiche dei noduli identificati dallo standard di riferimento 2 ( sr2 )  . 
nella tabella sono riportati il numero , le dimensioni e le caratteristiche densitometriche e morfologiche dei noduli , suddivisi per ciascun paziente sr2 paziente 1 paziente 2 paziente 3 34 tp findings , with an overall sensitivity of 38% , whereas cad2 correctly identified 11 nodules , with an overall sensitivity of 35% ( table 3 )  . 
in rapporto allo standard di riferimento 2 ( sr2 ) , il cad1 ha identificato correttamente 17 dei 54 reperti vp , con un valore di sensibilit complessiva del 30% , mentre il paziente 1 paziente 2 paziente 3 radiol med ( 2012 ) 117 : 953967 960 fig . 
2a - f nella figura sono rappresentati i reperti identificati dal cad1 ( a , c , e ) e dal cad2 ( b , d , f ) in ciascun esame tc dei tre pazienti selezionati . 
si noti il maggior numero di reperti segnalati dal cad 2 in ciascun esame / paziente , in particolare nel paziente 1 . and three ps ( 3 / 5 , 60% )  . 
in relation to rs2 , cad1 correctly identified 17 of the 54 tp findings , with an overall sensitivity of 30% , whereas cad2 correctly identified 13 , with an overall sensitivity of 23% ( table 4 )  . 
 the comparison of true positives , based on the topographic location of findings , shows that the two cad systems identified different findings as tp ( only 13% in common relative to rs1 , and 27% relative to rs2 )  . 
il risultato di questo confronto dei vp , basato sulla localizzazione topografica dei reperti , sottolinea che i due cad testati hanno identificato come vp reperti diversi ( solo il 13% in comune rispetto a sr1 e il 27% rispetto a sr2 )  . 
number of nodules detected by rs1 and the number of true positives ( tp ) and sensitivity values of cad1 and cad2 are reported for each patient and in total . 
 comparison between cad systems , performed by students t test , showed no statistically significant difference ( p > 0.05 ) nodules ( n ) cad1 cad2 students t test rs1 patient 1 patient 2 patient 3 total tp ( n ) sensitivity ( % ) tp ( n ) sensitivity ( % ) 0.42 tabella 3 confronto tra la sensibilit dei due sistemi cad nellidentificazione dei noduli polmonari in rapporto allo standard di riferimento 1 ( sr1 )  . 
 nella tabella sono riportati , per ciascun paziente e nel totale , i noduli identificati da sr1 e i reperti veri positivi ( vp ) con i valori di sensibilit del cad1 e del cad2 . 
il confronto tra i due sistemi cad , effettuato mediante test t di student , non ha documentato una differenza statisticamente significativa ( p > 0 , 05 ) sr1 paziente 1 paziente 2 paziente 3 totale sensibilit ( % ) test t di student sensibilit ( % ) noduli ( n ) vp ( n ) vp ( n ) cad2 cad1 0 , 42 in relation to rs1 , cad1 suggested 46 fp findings ( 17 in patient 1 , 17 in patient 2 , 12 in patient 3 ) , with an average of 15.3 fp per scan / patient ; the number of fp findings suggested by cad2 was 614 ( 277 in patient 1 , 194 in patient 2 , 141 in patient 3 ) , with an average of 204.7 fp per scan / patient . 
 with respect to rs2 , cad1 suggested 42 fp findings ( 17 in patient 1 , 14 in patient 2 , 11 in patient 3 ) , with an average of 14 fp per scan / patient ; the number of fp findings suggested by cad2 was 612 ( 275 in patient 1 , 193 in patient 2 , 144 in patient 3 ) , with an average of 204 fp per scan / patient . 
in rapporto a sr2 , il numero dei reperti fp proposti dal cad1 stato di 42 ( 17 nel paziente 1 , 14 nel paziente 2 , 11 nel paziente 3 ) , con una media di 14 fp per esame / paziente ; il numero dei reperti fp proposti dal cad2 stato di 612 ( 275 nel paziente 1 , 193 nel paziente 2 , 144 nel paziente 3 ) , con una media di 204 fp per esame / paziente . 
pur presentando un numero notevolmente inferiore di reperti fp , anche per il cad1 i falsi positivi pi frequentemente riscontrati sono state le interfacce con le strutture bronchiali , vascolari e le superfici pleuriche , sia in rapporto a sr1 ( 37 / 46 , 80% ) che a sr2 ( 35 / 46 , 83% ) , mentre gli incroci vascolari sono risultati meno numerosi ( in rapporto a sr1 : 9 / 46 , 19% ; in rapporto a sr2 : 7 / 42 , 17% )  . confronto dei cad il confronto della perfomance dei due software cad in termini di sensibilit non ha dimostrato una differenza statisticamente significativa ( p > 0 , 05 ) , sia in rapporto a sr1 ( p = 0 , 42 ) che in rapporto a sr2 ( p = 0 , 33 ) , con valori di sensibilit del cad1 solo di poco superiori a quelli del cad2 . 
number of nodules detected by rs2 and the number of true positives ( tp ) and sensitivity values of cad1 and cad2 are reported for each patient and in total . 
 comparison between cad systems , performed by students t test , showed no statistically significant difference ( p > 0.05 ) nodules ( n ) cad1 cad2 students t test tp ( n ) sensitivity ( % ) tp ( n ) sensitivity ( % ) radiol med ( 2012 ) 117 : 953967 tabella 4 confronto tra la sensibilit dei due sistemi cad nellidentificazione dei noduli polmonari in rapporto allo standard di riferimento 2 ( sr2 )  . 
 nella tabella sono riportati , per ciascun paziente e nel totale , i noduli identificati da sr2 e i reperti veri positivi ( vp ) con i valori di sensibilit del cad1 e del cad2 . 
il confronto tra i due sistemi cad , effettuato mediante test t di student , non ha documentato una differenza statisticamente significativa ( p > 0 , 05 ) noduli ( n ) cad1 cad2 test t di student vp ( n ) sensibilit ( % ) vp ( n ) sensibilit ( % ) 0.33 0 , 33 962 rs2 patient 1 patient 2 patient 3 total sr2 paziente 1 paziente 2 paziente 3 totale fig . 
3 bidimensional topographic location ( x , y ) of each of the 24 true positive lung nodules detected by cad1 and cad2 , in relation to reference standard 1 ( rs1 )  . 
3 nel grafico riportata la distribuzione topografica bidimensionale ( x , y ) di ciascuno dei 24 noduli polmonari veri positivi identificati dal cad1 e cad2 , in rapporto allo standard di riferimento 1 ( sr1 )  . 
i tre simboli evidenziati dai cerchi rossi tratteggiati hanno la medesima localizzazione spaziale e rappresentano , pertanto , i tre noduli identificati da entrambi i cad . relation to both rs1 ( p = 0.42 ) and rs2 ( p = 0.33 ) , with only slightly higher sensitivity values for cad1 . 
 discussione negli studi che hanno testato la performance dei sistemi cad impiegati come singolo lettore ( cad da solo , senza losservatore umano ; metodo stand - alone ) si riportano varadiol med ( 2012 ) 117 : 953967 fig . 
4 bidimensional topographic location ( x , y ) of each of the 30 true positive lung nodules detected by cad1 and cad2 , in relation to reference standard 2 ( rs2 )  . 
4 nel grafico riportata la distribuzione topografica bidimensionale ( x , y ) di ciascuno dei 30 noduli polmonari veri positivi identificati dal cad1 e cad2 , in rapporto allo standard di riferimento 2 ( sr2 )  . 
i sei simboli evidenziati dai cerchi rossi tratteggiati e i due simboli indicati dalle frecce rosse tratteggiate hanno la medesima localizzazione spaziale e rappresentano , pertanto , gli otto noduli identificati da entrambi i cad . discussion studies testing the performance of stand - alone cad systems ( cad used as a single reader without human readers ) report variable sensitivity values between 38% and 86% [ 10 , 11 , 14 , 15 , 18 , 22 - 24 ]  . 
 among technical factors , it is known that ct scans acquired with thin slices and standard dose tend to result in higher cad sensitivity compared with thick - slice scans obtained at lower dose [ 11 ]  . 
 [ 25 ] showed that the sensitivity of a cad system applied to low - dose mdct is identical to that observed at standard - dose imaging and that these systems may therefore be used in screening programmes . 
 sensitivity of a cad system may also be influenced by nodule size and location ; in particular , it tends to increase with increasing nodule size and in centrally located nodules as a result of the 3d analysis , which allows cad to easily differentiate nodules from central vessels [ 11 ]  . 
 when designing studies of this type , the rs method against which to test cad performance should also be taken into careful consideration given the lack of pathological correlation to confirm identified lesions and the difficulty in establishing which finding is a true lesion and which is not . 
although the radiologists interpretation can surely be considered closest to the truth , this approximation should always be acknowledged and accounted for in exlori di sensibilit piuttosto variabili , compresi tra il 38% e l86% [ 10 , 11 , 14 , 15 , 18 , 2224 ]  . 
tra i fattori tecnici , ad esempio , noto che le scansioni tc acquisite con spessore di strato sottile e dose di radiazione standard tendono a determinare valori pi elevati di sensibilit dei cad rispetto allutilizzo di scansioni a strato pi elevato e a bassa dose [ 11 ]  . 
 [ 25 ] ha dimostrato che la sensibilit di un sistema cad applicato agli esami tcmd a bassa dose sovrapponibile a quella osservata a dose standard e che , quindi , questi sistemi possono essere applicati negli studi di screening . 
la sensibilit di un cad pu essere influenzata anche dalle dimensioni e dalla sede dei noduli ; in particolare , tende ad essere maggiore con laumentare delle dimensioni dei noduli e per noduli localizzati in sede centrale , in rapporto alla modalit di analisi tridimensionale che consente al cad di distinguerli agevolmente dai vasi centrali [ 11 ]  . 
 anche il metodo utilizzato per costituire lo standard di riferimento ( sr ) , rispetto al quale testare la performance di un cad , dovrebbe essere attentamente considerato quando si impostano studi di questo tipo , data la mancanza di conferma anatomo - patologica delle lesioni identificate e il difficile compito di stabilire quale reperto rappresenti una vera lesione e quale no . 
 [ 12 ] hanno , infatti , dimostrato in un interessante lavoro che esiste una sostanziale variabilit nella determinazione della 964 radiol med ( 2012 ) 117 : 953967 fig . 
5a - c example of false positive outputs detected by cad2 on ct axial images at the level of interfaces with pleural surface ( a ) and with bronchovascular structures ( b ) and in correspondence with pulmonary vascular junctions ( c )  . 
5a - c esempio di reperti falsi positivi identificati dal cad2 sulle immagini assiali tc , in corrispondenza delle interfacce con la superficie pleurica ( a ) , con le strutture bronco - vascolari ( b ) e con un incrocio vascolare ( c )  . 
 [ 12 ] : the two rs recognised different nodules in both quantitative ( number ) and qualitative ( densitometry and dimensions ) terms , and only 20% of nodules were identified by both rs . 
psychological factors may also be involved ; radiologists of rs2 , who identified the highest number of nodules , were aware that their assessments would be compared with those of other experienced thoracic radiologists , and this might have positively affected their performance , as previously suggested by armato et al . 
a recent study [ 20 ] demonstrated that to accurately assess cad performance , a lesion - level analysis that takes into account the exact spatial location of each lesion should be preferred to a patient - level analysis , which introduces an overestimation bias , as several lesions may be present in each patient . 
the fact that the highest cad sensitivity values ( 8086% ) have been reported by studies that failed to adopt a rigorous method of analysis taking into account the topographic location of each finding [ 10 , 15 , 24 ] , supports the trend of overestimating cad sensitivity reported in literature . verit o sr tra radiologi toracici esperti diversi nella identificazione dei noduli polmonari . 
infatti , i due sr hanno riconosciuto noduli diversi , non solo dal punto di vista quantitativo , ovvero in termini numerici , ma anche qualitativo , ovvero in termini di caratteristiche densitometriche e dimensionali , e soltanto il 20% dei noduli sono stati identificati da entrambi gli standard di riferimento . 
i fattori che potrebbero aver determinato tale diversit possono essere di ordine pratico , ovvero errori di ricerca o di interpretazione dei reperti osservati sulle scansioni tc , anche in relazione alle piccole dimensioni dei noduli identificati nel nostro lavoro . 
anche fattori di ordine psicologico possono essere chiamati in causa ; il gruppo di radiologi sr2 , che ha identificato il maggior numero di noduli , era a conoscenza del fatto che le sue valutazioni sarebbero state confrontate con quelle di altri radiologi toracici esperti , e questo potrebbe aver indotto nei lettori una maggiore attenzione nella valutazione delle immagini , come peraltro ipotizzato anche nello studio di armato et al . 
in uno studio recente [ 20 ] , stato dimostrato che per unaccurata valutazione della performance di un cad si dovrebbe preferire un metodo di analisi finalizzato alla valutazione delle singole lesioni ( analisi per lesione ) che tenga conto della esatta localizzazione spaziale di ciascuna di esse , invece del metodo di analisi per paziente che introduce un bias di sovrastima della sensibilit , dal momento che possono essere presenti pi lesioni per paziente . 
losservazione che i valori di sensibilit pi elevati del cad ( 80%86% ) sono stati riportati in quegli studi in cui non stato utilizzato un rigoroso metodo di analisi che tenesse conto della localizzazione topografica radiol med ( 2012 ) 117 : 953967 the use of a 3d spatial localisation method for every cad output and for every true nodule identified by the rs , as done in our study , enables cad sensitivity to be accurately estimated by comparing the spatial coordinates of each finding . 
however , it must be remembered that the truth or falsehood of the findings of each cad system is only valid in the context of what the rs consider or do not consider to be noncalcified pulmonary nodules . 
 as expected , by using this accurate method of analysis , we obtained lower sensitivity values with the two cad systems with respect to both rs1 ( cad1 38% , cad2 35% ) and rs2 ( cad1 30% , cad2 23% ) compared with data reported in most published studies . 
 [ 23 ] , who used a lesion - level analysis with spatial localisation of the findings , reported a sensitivity value of 38% for stand - alone cad , which is a similar result to that found in our study . 
cad is proposed as a complementary system and , in particular , as a second or concurrent reader , depending on whether there is a need to improve the radiologists performance or to reduce reading time [ 14 19 , 22 ]  . 
 in our study , statistical comparison between the two commercial systems showed very similar sensitivity in detecting noncalcified pulmonary nodules , although cad1 had slightly higher sensitivity than cad2 , with respect to both rs1 and rs2 . 
this demonstrates that although the two cad systems are produced by different companies , and although they recognised different true positive nodules , their sensitivity is virtually identical as a result of accuracy of the method used . 
 [ 26 ] also failed to find any significant difference in sensitivity between two different systems that besides used different mathematical algorithms for pulmonary nodule detection , being one a cad and the other a nodule enhanced viewing ( nev ) syste in addition , with regards to what we hypothesised in the introduction and already reported by armato et al . 
 [ 12 ] , our results prove that the sensitivity of the cad systems tested does not appear to be influenced by the use of two rs , even though they recognised different tp nodules . 
 however , it should be noted that the mean diameter of findings detected by cad2 was significantly smaller than that identified by cad1 , which probably indicates that the two systems work with different mathematical segmentation algorithms . 
it is interesting also to note that the disproportion in the fp number between the two systems did di ciascun reperto identificato [ 10 , 15 , 24 ] , avvalora lipotesi di una tendenza alla sovrastima della sensibilit di tali sistemi riportata in letteratura . lutilizzo di un metodo di localizzazione spaziale 3d di ogni reperto identificato dal cad e di ogni nodulo certo indicato dallo standard di riferimento , come nel nostro studio , consente una stima accurata della sensibilit del cad , mediante il confronto delle coordinate spaziali di ciascun reperto . 
tuttavia da ritenersi che la verit o falsit dei reperti di ciascun cad sia valida soltanto nel contesto di ci che gli sr hanno ritenuto , o non ritenuto , noduli polmonari non calcifici . 
come atteso , utilizzando questo metodo accurato di analisi abbiamo ottenuto valori di sensibilit bassi con entrambi i sistemi cad , sia in riferimento a sr1 ( cad1 38% , cad2 35% ) che a sr2 ( cad1 30% , cad2 23% ) , rispetto a quanto stato riportato nella maggior parte dei lavori della letteratura . 
 [ 23 ] , che ha utilizzato un metodo di analisi per lesione con localizzazione spaziale dei reperti , si riporta un valore di sensibilit del cad impiegato da solo del 38% , simile ai nostri risultati . 
il cad viene proposto come sistema complementare , in qualit di secondo lettore o come lettore concorrente , a seconda della necessit rispettivamente di migliorare la performance del radiologo nella identificazione dei noduli polmonari o di preferire la rapidit di analisi delle immagini tc [ 1419 , 22 ]  . 
 nel nostro studio , il confronto statistico tra i due sistemi commerciali impiegati ha dimostrato una sensibilit sovrapponibile nellidentificazione dei noduli polmonari non calcifici , nonostante il cad1 abbia riportato una sensibilit di poco superiore al cad2 , sia in rapporto a sr1 che a sr2 . 
 questo dato dimostra come , nonostante i due cad siano prodotti da aziende diverse e abbiano riconosciuto noduli veri positivi diversi , si possa ritenere la loro sensibilit oggettivamente sovrapponibile , in rapporto allaccurata metodologia impiegata . 
 [ 26 ] non hanno riportato differenze significative della sensibilit di due software automatici diversi che , peraltro , impiegavano algoritmi matematici differenti nella identificazione dei noduli polmonari , essendo uno un sistema cad e laltro un sistema nodule enhanced viewing ( nev )  . 
 [ 12 ] , i nostri risultati documentano che la sensibilit dei sistemi cad testati non sembra essere stata influenzata dallimpiego di due standard di riferimento diversi , pur avendo questi riconosciuto noduli veri positivi differenti . 
per quanto riguarda la performance dei due cad in termini di falsi positivi , abbiamo riscontrato una percentuale di gran lunga pi elevata di reperti fp per il cad2 rispetto al cad1 . 
bisogna , tuttavia , notare che il diametro medio dei reperti segnalati dal cad2 risultato significativamente inferiore a quello dei reperti identificati dal cad1 , ad indicare probabilmente che i due sistemi lavorano con algoritmi matematici di segmentazione differenti . 
moreover , in our study , no size threshold was applied for automatic detection of findings , and this accounts for the large number of fp , particularly with cad2 . 
both cad systems allow the operator to set a size threshold above which the system should report findings , and clearly , the number of fp results indicated by cad systems can be decreased by setting progressively higher size thresholds . 
although the number of patients / scans analysed was only three , it should be noted that analysis was performed on lesions and not on patients and therefore there was no loss in statistical power associated with a patient - level analysis [ 20 ]  . 
another limitation is that our study is to be considered a laboratory trial in which the human observer does not take part in the decision - making process ( except for the rs ) ; although sufficient for assessing sensitivity , it cannot be considered a clinical study . 
a clinical study should analyse the potential improvement in radiologist performance by the use of cad systems ; it would require larger samples and more sophisticated methods , such as receiver operating characteristic ( roc ) [ 27 ] and free - response roc ( froc ) analysis [ 28 , 29 ]  . 
these methods assess performance in terms of indexes that are independent from decision thresholds that affect a parameter such as sensitivity ( defining whether a nodule is present or absent is always a decision dependent on a criterion or decision threshold )  . 
furthermore , as the radiologists did not read the images with the aid of the cad system , we were unable to assess the effect of the different number of fp of the two cad systems in terms of either overall reader performance or image reading times . 
 even though it is reasonable to believe that a high number of fp results identified by cad could lead to longer reading times , it has been shown that the radiologist is scarcely influenced by the total number of fp outputs , as he or she is able to decide quickly , on the basis of previous experience , which are true and which are false nodules [ 11 , 16 ]  . 
 however , this issue remains to be resolved and is still a subject of debate . in conclusion , the two cad systems showed similar sensitivity in detecting noncalcified pulmonary nodules when compared with two different and independent rs . 
the use of an accurate method for spatial localisation of findings showed that the sensitivity values of the cad systems only interessante osservare che nonostante la sproporzione del numero dei falsi positivi tra i due sistemi , questo non abbia in alcun modo influenzato la sensibilit che risultata simile tra i due cad . 
inoltre , nel nostro studio non stata applicata alcuna soglia dimensionale nella identificazione automatica dei reperti e questo giustifica il grande numero di falsi positivi riscontrati , in particolare con il cad2 . 
entrambi i cad consentono di stabilire a priori un livello soglia dimensionale , al di sopra del quale identificare i reperti , ed evidente che settando il software su valori soglia progressivamente pi elevati si assista ad una consensuale riduzione del numero dei falsi positivi proposti dal cad . 
anche se il numero di pazienti / esami analizzati stato soltanto di tre , da sottolineare che lanalisi stata effettuata sulle lesioni e non sui pazienti e , pertanto , non si avuta perdita di potere statistico associata ad unanalisi di tipo patient - level [ 20 ]  . 
altro limite del nostro studio che da ritenersi un test di laboratorio , in cui losservatore umano non fa parte del processo decisionale ( eccetto che per gli sr ) , sufficiente per stimare la sensibilit , ma non per essere considerato un test clinico . 
il test clinico dovrebbe analizzare il potenziale miglioramento della performance del radiologo con limpiego dei sistemi cad mediante studi su larga scala ed utilizzo di metriche pi sofisticate , quali le analisi receiver operating characteristic ( roc ) [ 27 ] e free - response roc ( froc ) [ 28 , 29 ]  . 
tali analisi permettono di valutare la performance in termini di indici indipendenti dalle soglie decisionali a cui soggetto un parametro come la sensibilit ( stabilire se il nodulo presente o non presente sempre una decisione soggetta ad un criterio o soglia decisionale )  . 
inoltre , non essendo stata effettuata la lettura delle immagini da parte di un radiologo utilizzando il cad , non stato possibile stimare leffetto del diverso numero dei falsi positivi riportato dai due cad , sia in termini di performance complessiva del lettore che in termini di tempi di lettura delle immagini . 
anche se ragionevole ritenere che un numero elevato di falsi positivi identificati dal cad possa determinare un aumento dei tempi di lettura degli esami tc , in letteratura stato dimostrato che il radiologo poco influenzato dal numero complessivo dei reperti falsi positivi , essendo in grado di decidere rapidamente , sulla base dellesperienza , quali siano i veri noduli e quali i falsi noduli [ 11 , 16 ]  . 
questo problema , tuttavia , rimane ancora aperto ed oggetto di discussione . in conclusione , i due sistemi cad testati hanno dimostrato una sensibilit sovrapponibile nella identificazione dei noduli polmonari non calcifici , quando analizzata a confronto con due standard di riferimento diversi ed indipendenti . 
vite2 1dipartimento di medicina sperimentale , universit degli studi dellinsubria , varese , italy 2unit operativa di fisica sanitaria , azienda ospedaliera - universitaria ospedale di circolo e fondazione macchi , varese , italy correspondence to : l . 
a new calibration method for an amorphoussilicon ( a - si ) electronic portal imaging device ( epid ) used for dose measurements in pretreatment verification ( fieldrelated ) of intensity - modulated radiation therapy ( imrt ) with sliding - window technique . 
for fluence - modulated fields , different dose / reading calibration factors are associated with each pixel of the image acquired by calculating equivalent areas representing the exact ratio between primary and scatter components . 
il lavoro finalizzato allimplementazione di un nuovo metodo di calibrazione di un dispositivo portale al silicio amorfo ( epid ) impiegato per misure di dose nelle verifiche pre - trattamento ( field - related ) con tecnica di radioterapia ad intensit modulata ( imrt ) sliding window . 
per campi a fluenza modulata si associano ai pixel dellimmagine diversi fattori di calibrazione dose / lettura calcolando delle aree equivalenti rappresentative del rapporto puntuale tra le componenti primaria e diffusa . 
ciascun fattore di calibrazione viene confrontato con quello calcolato considerando separatamente i contributi di radiazione primaria e secondaria ottenuti con metodo di convoluzione di un kernel analitico per mezzi omogenei . 
 keywords imrt dosimetry pretreatment epid parole chiave imrt dosimetria pre - trattamento epid radiol med ( 2012 ) 117 : 10441056 1045 introduction introduzione intensity - modulated radiotherapy ( imrt ) techniques help to improve the quality of radiation therapy treatments , as they make it possible to increase tumour control probability ( tcp ) and decrease normal tissue complication probability ( ntcp ) compared with conventional techniques . 
verification results derived from portal images in terms of dose to the patient , to the phantom and to the epid are compared with the dose to the patient , to the phantom or to the epid calculated by the treatment planning system ( tps )  . epids based on amorphous silicon technology ( a - si epid ) offer the advantage of being highly sensitive and having adequate spatial resolution [ 2 ]  . 
however , they are indirect detection systems , and some of their features pose problems in converting the signal to dose , particularly with regard to the energy dependence of the response [ 35 ]  . a number of methods have been devised for field - related pretreatment verification using a - si epids . 
these methods are based on portal images acquired with a beam directly incident on the epid surface , with or without depths of tissue - equivalent material placed on the surface of the device . 
other pretreatment epid - based verification methods are based on the calculation of either the 2d or 3d distribution of the energy fluence or of the dose to the patient or phantom [ 1326 ]  . 
distributions of the energy fluence or of the dose obtained at the level of the epid , patient or phantom are compared with the values provided by the tps or other calculation procedures unrelated to the tps . this paper describes a dose calibration method of an a - si epid for pretreatment verification of imrt with slidingwindow technique . 
the portal image is calibrated using a simple procedure entirely based on experimental data contained in the image itself . materials and methods epid calibration le tecniche di radioterapia a intensit modulata ( imrt ) permettono di migliorare la qualit dei trattamenti radioterapici poich rendono possibile aumentare la tumor control probabiliy ( tcp ) e ridurre la normal tissue complication probability ( ntcp ) rispetto alle tecniche tradizionali . 
numerosi sono gli studi effettuati allo scopo di mettere a punto modalit di verifica con epid per garantire la correttezza dei piani di trattamento imrt e della loro esecuzione [ 1 ]  . 
 i risultati di tali verifiche , ottenuti a partire dalle immagini portali in termini di dose al paziente , di dose a un fantoccio o di dose a livello dellepid , vengono messi a confronto con le dosi al paziente , al fantoccio o a livello dellepid , calcolate dal sistema di calcolo dei piani di trattamento ( tps )  . 
 i dispositivi epid basati sulla tecnologia del silicio amorfo ( a - si epid ) hanno il vantaggio di una elevata sensibilit e di una risoluzione spaziale adeguata [ 2 ]  . 
tuttavia , essendo sistemi di rivelazione indiretti , presentano alcune caratteristiche che pongono dei problemi nella conversione del segnale in dose , in particolare per quanto riguarda la dipendenza energetica della risposta [ 35 ]  . 
 per verifiche pre - trattamento di tipo field related mediante a - si epid sono stati messi a punto negli ultimi anni diversi metodi che si basano su immagini portali acquisite con fascio direttamente incidente sulla superficie dellepid , con o senza spessori di materiale tessuto - equivalente posizionati sulla superficie del dispositivo . 
 altri metodi di verifica pre - trattamento con epid si basano sul calcolo della distribuzione 2d o 3d della fluenza di energia o della dose nel paziente o in un fantoccio [ 1326 ]  . 
 le distribuzioni della fluenza di energia o della dose ottenute a livello dellepid oppure nel paziente o in fantoccio vengono confrontate con i valori previsti dal calcolo del tps o da altre procedure di calcolo indipendenti dal tps . questo articolo descrive un metodo di calibrazione dosimetrica di un a - si epid per verifiche pre - trattamento dei piani imrt con tecnica sliding window . 
limmagine portale viene calibrata con un semplice procedimento interamente basato su dati sperimentali contenuti nellimmagine stessa . the as500 epid device consists of an a - si matrix of 512384 pixels ( pixel size 0.7840.784 mm2 , total sensitive area 4030 cm2 )  . 
a layer of copper ( depth 1 mm ) and a layer of scintillator material ( gd2o2s : tb ) overlie the silicon materiali e metodi calibrazione dellepid il dispositivo epid as500 costituito da una matrice di 1046 radiol med ( 2012 ) 117 : 10441056 fig . 
modulated fluences are obtained using the sliding - window technique , with 6 mv photon beams generated by two linear accelerators ( varian clinac dhx ) equipped with a multileaf collimator with 120 leaves ( millennium mlc - 120 ) and a clinical dose rate of 300 monitor units / min ( mu / min )  . 
for pretreatment verification with the epid , we chose to deliver the fluence corresponding to each treatment field , maintaining gantry orientation to 0 and placing the detector at a tissue - equivalent depth of 5 cthus , portal images are acquired by placing a 4.2 - cm polystyrene phantom on the surface of the epid coating in addition to the copper - equivalent depth . 
 a correction matrix corresponding to a large - size open field is applied to the acquired images in order to reproduce the real 2d pattern of the field . figure 1a illustrates the epid - based method for acquiring images of square fields measuring 33 , 55 , 66 , 77 , 88 , 99 , 1010 , 1212 , 1414 , 1616 , 1818 , 2020 , 2222 cm2 at their isocentres . 
figure 1b shows the method for measuring dose on the beam axis using a 0.6cc farmer ptw 30001 ionisation chamber for square fields having the same size as the epid acquisition fields . 
in this case , we verified the dependence of the measured dose on the area of the square field , at equal mu . silicio amorfo ( a - si ) di 512384 pixel ( dimensione del pixel 0 , 7840 , 784 mm2 , area sensibile totale 4030 cm2 )  . 
le fluenze modulate sono ottenute , mediante tecnica sliding window , con fasci di fotoni da 6 mv prodotti da due acceleratori lineari varian modello clinac dhx dotati di collimatore multilamellare a 120 lamelle ( millenium mlc - 120 ) , con dose - rate clinico di 300 unit monitor / minuto ( um / min )  . 
 per le verifiche pre - trattamento mediante epid si scelto di erogare la fluenza corrispondente a ciascun campo di trattamento mantenendo lorientazione del gantry a 0 e ponendo il rivelatore a 5 cm di profondit tessuto - equivalente . 
 per questo motivo , le immagini portali sono acquisite ponendo 4 , 2 cm di fantoccio a strati di polistirene sulla superficie del rivestimento dellepid in aggiunta allo spessore equivalente del rame . 
 la figura 1a illustra la modalit di acquisizione mediante epid delle immagini di campi quadrati aventi le dimensioni di 33 , 55 , 66 , 77 , 88 , 99 , 1010 , 1212 , 1414 , 1616 , 1818 , 2020 , 2222 cm2 allisocentro . 
 radiol med ( 2012 ) 117 : 10441056 1047 as the field area grows , there is an increase in the contribution of scatter radiation , the energy of which is lower than that of the primary bea with the increasing field area , the epid response shows a function that grows faster than that representing the dose measured with the ionisation chamber . 
for all selected fields , the measured dose was compared with epid response : the dose / response ratio for each field is the calibration factor that allows the detector response to be converted to dose . in the event of imrt treatments , the ratio between scattered and primary dose at epid level changes from pixel to pixel such that a different calibration factor has to be associated with each pixel . 
la figura 1b illustra la modalit di misura mediante camera a ionizzazione farmer ptw 30001 da 0 , 6 cc della dose sullasse del fascio per campi quadrati aventi le stesse dimensioni dei campi di acquisizione con epid . 
in questo caso stata verificata , a parit di unit monitor , la dipendenza della dose misurata in funzione dellarea del campo quadrato . al crescere dellarea del campo aumenta il contributo della radiazione diffusa la cui energia inferiore rispetto allenergia del fascio primario . 
per tutti i campi selezionati la dose misurata stata messa a confronto con la risposta dellepid : il rapporto dose / risposta per ciascun campo il fattore di calibrazio ne che consente di convertire in dose la risposta del rivelatore . nel caso di trattamenti con tecnica imrt il rapporto tra scattering e dose primaria a livello dellepid varia da pixel a pixel e perci a ciascun pixel va associato un diverso fattore di calibrazione . 
2 radiazione diffusa incidente su un singolo pixel ( area ds ) della matrice attiva dellepid . ciascuno degli elementi ds equivale ad un incre1048 radiol med ( 2012 ) 117 : 10441056 di , p = primary beam dose in pixel ik ; dk , p = primary beam dose in pixel k ; n = number of thin beams contributing to scatter in the pixel to be calibrated k ; ds = area corresponding to the size of one pixel . 
 each of the elements of ds is equivalent to an increase in the area ds of weighted pixel k for the ratio between the primary dose components di , p dk , p di , p dk , p the summation is extended to the number n of pixels contained in an roi centred on the pixel k to be calibrated . 
 inside the roi , the contribution of scatter radiation in pixel k from the beams included in the roi is assumed to be independent of the distance from pixel k . di , p dk , p the ratio can be replaced with the ratio between ri , p rk , p the epid responses and the primary radiation since the calibration factor for the primary dose can be considered constant in every pixel . 
 di , p dk , p pu essere sostituito dal rapporto tra le risposte dellepid alla radiazione primaria ch il fattore di calibrazione per la dose primaria pu essere considerato costante in ogni pixel . 
1 and 2 , there will be an overestimation of the equivalent area when there is a greater contribution of scatter radiation in pixel i than in pixel k ( case 2 ) and an underestimation in the reverse situation ( case 3 )  . 
the suggested algorithm allows for an approximate calculation of the area of the equivalent field to be attributed to each pixel based on the signal generated in the surrounding pixels . in the section titled epid calibration above , each square field was assigned a calibration factor defined as the relationship between dose and epid response . 
for modulated fluences , the calibration factor of the single pixel , which allows pixel response to be converted to dose , corresponds to the calibration factor of the regular field covering an area equal to that of the equivalent field . 
hence an equivalent calibration is obtained , which is given by the relation factor neq = ship between the dose in the middle of the equivalent field and the pixels response . the pixels surrounding the one to be calibrated are included in an roi of the size of an open 1010 cm2 field centred on the pixel to be calibrated . 
this choice is justified because in the middle of an open field , under the measurement conditions described here , the contribution of scattered radiation increases rapidly up to a size of 10 10 cm2 , whereas it increases very little for larger fields . 
the pixels contained in areas belonging to the field delimited by the jaws , which throughout the delivery are only , however , exposed to the radiation transmitted through the leaves , are associated with a constant equivalent field value . 
the size of this field corresponds to the calibration factor of the portal device relative to transmitted radiation only , measured with completely closed leaves and comparing the dose measured with the ionisation chamber with the image ac1049 se a > b , se a < b , ak > ds + ak < ds + siri , p rk , p siri , p rk , p ds ( caso 2 ) ds ( caso 3 ) rispetto alle stime dellarea di cui alle relazioni ( 1 ) e ( 2 ) si avr una sovrastima dellarea equivalente quando nei pixel i si ha mediamente un contributo di radiazione diffusa maggiore di quello presente nel pixel k ( caso 2 ) e si avr una sottostima quando avviene il contrario ( caso 3 )  . lalgoritmo proposto consente un calcolo approssimato dellarea del campo equivalente da attribuire a ciascun pixel sulla base del segnale prodotto nei pixel circostanti . 
 per fluenze modulate il fattore di calibrazione del singolo pixel che consente di convertire in dose la risposta del pixel , corrisponde al fattore di calibrazione del campo regolare di area uguale a quella del campo equivalente . 
si ha dunque un fattore di calibrazione equivalente neq = dal rapporto tra la dose al centro del campo equivalente e la risposta del pixel considerato . che dato i pixel circostanti a quello da calibrare sono contenuti in una roi che ha le dimensioni di un campo aperto di 1010 cm2 centrata sul pixel da calibrare . 
questa scelta giustificata dal fatto che al centro di un campo aperto , nelle condizioni di misura descritte , il contributo della radiazione diffusa aumenta rapidamente fino a dimensioni di 1010 cm2 mentre aumenta di poco per campi di dimensioni superiori . 
ai pixel che si trovano in regioni appartenenti al campo definito dai jaws , che per sono esposti per tutta la durata dellerogazione solo a radiazione trasmessa attraverso le lamelle , si associa un valore di campo equivalente costante . 
the function depends on scattering angle , on the between the point of interaction s and the point distance d of dose calculation r , as well as on the energy spectrum of the incident radiation . 
 il fattore di calibrazione np / s pu essere espresso dalla relazione : radiol med ( 2012 ) 117 : 10441056 the calibration factor neq , obtained using the equivalentfield method , with calibration factor np / s , which was calculated by separating the primary and scattered dose components . 
the calibration factor for the primary beam component ( np ) can be obtained by extrapolation from a smallsized field in which the incident radiation is assumed to be only primary . 
the response to scattered ra primary radiation rp = diation is calculated by subtracting the primary dose component from the total response ( rs = r rp ) , whereas the calibration factor is obtained from the scattered radiation  . 
the calibration factor is expressed as the relationship between the dose ( gy ) and the response of the epid along the axis of the radiation beait should be noted that the function obtained , considering the negative sign of the response , shows that as the field area grows , the dose / response relationship decreases in absolute value . 
the function in figure 3 allows the area of each equivalent field obtained as described in the section above titled equivalent area calculation method to be associated with a calibranp ns essendo rp = e rs = le risposte alla dose primaria dp e alla dose da scattering ds e np e ns i fattori di calibrazione parziali per ciascuna delle due componenti . 
 il fattore di calibrazione relativo alla sola componente primaria del fascio ( np ) pu essere ottenuto per estrapolazione in corrispondenza di un campo di piccole dimensioni in cui si assume che la radiazione incidente sia solo primaria  . 
per diverse dimensioni del campo aperto stato ricavato il valore di lettura portale atteso sullasse del fascio in risposta alla sola radiazione primaria rp = diffusa si ottiene sottraendo alla risposta totale la componente primaria ( rs = r rp ) e da questa il fattore di calibra . 
si nota come la funzione ottenuta , tenuto conto del segno negativo della risposta , dimostri come al crescere dellarea del campo il rapporto dose / risposta diminuisca in valore assoluto . 
la funzione in figura 3 consente di associare allarea di ciascun campo equivalente , ottenuta con il metodo descritto nei materiali e metodi nel paragrafo metodo di calcolo dellarea equivalente , un fattore di calibrazione per la conversione in dose della risposta dellepid in tutti i pixel dellimmagine acquisita . 
 risultati ottenuti con lanalisi gamma nei casi clinici da settembre 2007 ad oggi nel nostro centro sono stati trattati con tecnica imrt 196 pazienti con patologie della regione 1052 radiol med ( 2012 ) 117 : 10441056 fig . 
3 fattore di calibrazione dose / lettura dellepid in funzione dellarea del campo . tion factor for converting to dose the response of epid in all pixels of the image acquired . results obtained with - analysis in clinical cases since september 2007 , 196 patients with pelvic diseases and 100 with head and neck diseases and breast or pancreas diseases were treated with imrt at our centre . 
for each field , we know the expected dose distribution in the detector plane , as calculated by the tps eclipse , and the dose distribution obtained with the epid detector , through calibration of the acquired portal image . 
the results of - analysis were examined for all points included in the area defined by the jaws for 854 clinical fields ( 444 relating to the head and neck region , 368 to the pelvic region , and 42 to other regions )  . 
for all these fields , the confidence index and the average value obtained in the - analysis were regarded as validation indices of the comparison between expected and measured doses . pelvica , 100 pazienti con patologie del distretto capo - collo e 8 pazienti con patologie relative a mammella o pancreas . 
il confronto tra la distribuzione della dose attesa e quella misurata stato fatto mediante analisi ( criteri del dose difference pari al 3% e del distance to agreement pari a 3 mm )  . 
 sono stati esaminati i risultati dellanalisieffettuata su tutti i punti compresi nellarea definita dai jaws , per 854 campi clinici di cui 444 relativi al distretto capo - collo , 368 riferiti al distretto pelvico , 42 riferiti ad altri distretti corporei . 
 dallanalisi sono stati considerati , per tutti i campi , come indici di validazione del confronto tra dose prevista e dose misurata , lintervallo di confidenza ( ic ) e il valore medio . la figura 4 riporta listogramma delle frequenze dei valori dellindice di confidenza per tutti i campi analizzati . 
4 istogramma delle frequenze dellintervallo di confidenza ( ic% ) calcolato per tutti i campi nellarea delimitata dal collimatore principale . radiol med ( 2012 ) 117 : 10441056 1053 figure 4 shows the histogram of frequency of the confidence index values for all fields considered . 
 comparison between epid calibration factors obtained with empirical algorithm and with calculation of primary and scatter components the algorithm for separate calculation of primary and scatter doses allowed us to calculate the calibration factors for both components . 
 as with static square fields , for some clinical fields , factor ns , which is used to calibrate the contents of the dose image , was calculated for each pixel . 
therefore , it was assumed that ns = - 2.4107 gy / reading , a value dellindice gamma per tutti i campi analizzati di 0 , 39 con una deviazione standard di 0 , 06 . 
 confronto tra i fattori di calibrazione dellepid con algoritmo empirico e con calcolo delle componenti primaria e diffusa lalgoritmo per il calcolo separato di dose primaria e diffusa ha consentito di calcolare i fattori di calibrazione per le due componenti . 
 analogamente al caso dei campi quadrati statici , per alcuni campi clinici , stato calcolato in corrispondenza di ciascun pixel , il fattore ns utilizzato per calibrare il contenuto dellimmagine in dose . 
5 fattori di calibrazione dose / lettura dellepid per la radiazione primaria ( np ) e diffusa ( ns ) in funzione dellarea del campo . 1054 radiol med ( 2012 ) 117 : 10441056 fig . 
6 istogramma delle frequenze degli scarti percentuali tra il fattore di calibrazione np / s , ottenuto dalle componenti primaria e diffusa , e il fattore neq ottenuto dallarea equivalente . corresponding to the static open field of 160 cm2 . 
this result shows that the two independent calculation methods agree and provides further validation to the empirical method , supported by the results of - analysis . portale , ottenuto mediante la relazione ( eq.10 ) , stato confrontato con il fattore calcolato mediante lalgoritmo empirico di calibrazione neq delle immagini portali . 
 discussion and conclusions the proposed method allows pretreatment verification to be performed using a portal imaging device as a detector for dose measurement that is completely independent of the tps and system - controlling leaf motion in the multileaf collimator . 
the contents of each pixel belonging to the epid - sensitive area is converted to dose by means of a calibration factor , taking into account the relationship between primary and scatter components of the radiation beam at the point being considered . 
the approximations introduced are acceptable , as demonstrated by the results of - analysis conducted on a large number of fields , and by the separate calculation of the calibration factors of the primary and scatter beam components . 
 this entails an error in the estimation of the calibration factor under 1% . discussione e conclusioni il metodo proposto permette di effettuare verifiche pre - trattamento utilizzando il dispositivo per immagini portali come un rivelatore per misure dosimetriche del tutto indipendente dal sistema di calcolo del tps e dalle modalit di funzionamento del sistema di controllo dei movimenti delle lamelle del collimatore multilamellare . 
il contenuto di ciascuno dei pixel appartenenti allarea sensibile dellepid viene convertito in dose mediante un fattore di calibrazione che tiene conto del rapporto tra componente primaria e diffusa del fascio radiante nel punto considerato . 
le approssimazioni introdotte risultano accettabili come dimostrato dai risultati dellanalisi gamma effettuata su un numero elevato di campi e dal calcolo separato dei fattori di calibrazione delle componenti primaria e diffusa del fascio . 
questo comporta un errore nella stima del fattore di calibrazione inferiore all1% . the time needed to calculate the calibration factors i tempi di calcolo dei fattori di calibrazione dei pixel radiol med ( 2012 ) 117 : 10441056 1055 of the pixels of the entire matrix is in the order of 1 m this allows pretreatment verification to be carried out routinely and to be repeated several times . 
however , acquisition of the experimental data explained earlier is still needed . as the empirical algorithm for calculating the equivalent area can be applied under different conditions from those described here , it can be also be tested for verification in the course of treatment , as of the in vivo acquisition of portal images . 
comunque necessaria lacquisizione dei dati sperimentali in precedenza descritti . poich lalgoritmo empirico per il calcolo dellarea equivalente applicabile in condizioni diverse da quelle descritte esso pu essere sperimentato anche per verifiche in corso di trattamento a partire dalla acquisizione in vivo di immagini portali . 
magnavita4 1istituto di medicina del lavoro , universit cattolica del sacro cuore , largo gemelli 8 , 00168 roma , italy 2istituto nazionale di riposo e cura dellanziano ( inrca ) , roma , italy 3istituto oncologico veneto irccs dipartimento di scienze oncologiche e chirurgiche delluniversit degli studi di padova , padova , italy 4cnr presso ministero dellambiente , roma , italy correspondence to : n . 
the immediate consequences of violence in the workplace are emotions such as anger , disappointment , humiliation , anxiety , fear , distress , a feeling of helplessness and isolation , occasionally a feeling of guilt or of having riassunto obiettivo . 
le conseguenze immediate della violenza sono emozioni come rabbia , delusione , 1020 radiol med ( 2012 ) 117 : 10191033 done wrong and a desire to take revenge , change behaviour or change workplace . 
 keywords violence workplace radiologist occupational aggression umiliazione , ansia , paura , angoscia , sensazione di essere indifeso e isolato , a volte senso di colpa o di avere sbagliato , impulso a vendicarsi , a cambiare modo di agire , a cambiare posto di lavoro . 
 parole chiave violenza luogo di lavoro radiologo occupazionale aggressione introduction introduzione violence in the workplace , intended as violent incidents , includes physical abuse , threats or harassment and is an important occupational risk [ 1 , 2 ]  . 
numerous studies have emphasised that violence is particularly common in certain healthcare settings , such a psychiatric services [ 4 , 5 ] and emergency departments [ 6 , 7 ]  . 
 studies conducted in various countries with widely varying methods suggest a very broad range in the annual frequency of acts of physical abuse in the various healthcare professions and the different types of activity , from 3% to 70% [ 5 , 817 ]  . 
even higher is the frequency of nonphysical violence , which affects more than one third of all workers [ 8 , 9 , 11 , 12 , 1519 ]  . 
a very small percentage of those violent acts are formally reported , which is due to the tendency of healthcare workers to consider them a part of the work environment or to the belief that making such a report would be useless [ 20 , 21 ]  . violence in the workplace has a significant cost and can lead to deterioration of the workers health and quality of patient care . 
a systematic review of the literature suggests that despite the differences in nationality , culture and methodology of the studies and the type of healthcare activities , healthcare workers respond to violence in the same way . 
immediate reactions include frustration , fear , anger or anxiety and distress [ 11 , 22 ] , which may be lasting and lead to addictive behaviour [ 23 ] , psychiatric disorders such as burnout [ 24 ] and posttraumatic stress disorder [ 25 ] ; a sense of guilt , shame , self - condemnation [ 25 ] ; right up to the intent to change jobs or institutions [ 13 ]  . 
such reactions may last for months or years after the violent incident , particularly if the la violenza sul luogo di lavoro , intesa come atti violenti , comprendenti aggressioni fisiche , minacce o molestie , un rilevante rischio professionale [ 1 , 2 ]  . 
i lavoratori della sanit sono particolarmente esposti alle aggressioni , che derivano principalmente da pazienti , loro parenti o accompagnatori , ma possono anche originare allinterno dello staff medico , da parte di colleghi ( violenza laterale o orizzontale ) o superiori ( violenza verticale ) [ 3 ]  . 
una copiosa letteratura ha messo in evidenza come la violenza sia particolarmente frequente in alcuni ambienti sanitari , come i servizi psichiatrici [ 4 , 5 ] , o i dipartimenti di emergenza e urgenza [ 6 , 7 ]  . 
 le indagini , condotte in diversi paesi e con metodi molto differenti , stimano in un intervallo molto ampio , dal 3% al 70% annuo , la frequenza delle aggressioni fisiche nelle diverse professioni sanitarie e nei diversi tipi di attivit [ 5 , 817 ]  . 
ancora pi elevata la frequenza delle aggressioni non fisiche , che riguardano da oltre un terzo alla quasi totalit dei lavoratori [ 8 , 9 , 11 , 12 , 1519 ]  . 
una quota molto bassa di tali atti di violenza d origine ad una formale denuncia , per la tendenza degli operatori della sanit a ritenerli come parte del lavoro , o per un insieme di considerazioni circa linutilit della segnalazione stessa [ 20 , 21 ]  . il costo della violenza sul luogo di lavoro rilevante e si pu tradurre in un deterioramento della salute dei lavoratori e in un abbassamento della qualit dellassistenza . 
una revisione sistematica della letteratura indica che nonostante le differenze di nazionalit , cultura , metodologia degli studi e tipo delle attivit sanitarie , i lavoratori della sanit rispondono alle aggressioni nello stesso modo , con reazioni immediate come delusione , paura , rabbia o ansia e angoscia [ 11 , 22 ] , che possono protrarsi e sfociare in comportamenti addittivi [ 23 ] , disturbi psichiatrici come il burnout [ 24 ] ed il disturbo di stress post - traumatico [ 25 ] , senso di colpa , vergogna , auto - condanna [ 25 ] , fino allintento di lasciare lattivit o di cambiare luogo di lavoro [ 13 ]  . 
productivity can also be compromised , with an increase in errors , a decline in performance [ 15 , 26 , 27 ] and reduced organisational commitment [ 28 ]  . in 2007 , the italian ministry of health issued a recommendation [ 29 ] calling on the healthcare authorities to monitor the problem and to implement appropriate preventive measures . 
this appeal for the most part went unheard , and there are few data available regarding the incidence and prevalence of violence in the italian healthcare system [ 15 , 30 ]  . 
whereas studies in the international literature regarding the risk of violence in radiological activity are extremely rare [ 3133 ] , they are completely absent with regard to italian diagnostic imaging . 
 this study is the first investigation aimed at evaluating the prevalence of physical and verbal abuse against italian radiologists and identifying its origins and understanding the consequences for victims health . 
in a subsequent study , the relationship between violence in the workplace and psychosocial problems ( mental well - being , stress , social support , sense of justice , job satisfaction ) will be studied . materials and methods italian radiologists who took part in the national congress were called on to fill in an anonymous questionnaire that asked whether in the previous 12 months or during their working life they had experienced physical abuse , threats or harassment in the workplace . 
 those who reported being victims of such behaviour were then asked to describe the episode of physical abuse and , separately , nonphysical abuse using the violent incident form ( vif ) , a questionnaire drawn up by arnetz for reporting violent incidents in the healthcare setting [ 34 ] and applied in the italian setting in previous studies [ 3538 ]  . 
 the vif describes a specific incident of direct violence or harassment against a healthcare worker and includes questions on the perpetrator of the violence ( sex , age , status ) , the type of abuse and the consequences of the incident . 
anche la produttivit pu risultare compromessa , con un aumento degli errori e un peggioramento delle performances professionali [ 15 , 26 , 27 ] ed un ridotto coinvolgimento del lavoratore nellorganizzazione del lavoro [ 28 ]  . il ministero della salute italiano ha emanato nel 2007 una raccomandazione [ 29 ] , invitando le aziende sanitarie a monitorare il fenomeno e a mettere in atto le opportune misure preventive . 
tale invito rimasto in larga misura inascoltato , e ci sono al momento pochi dati sullincidenza e la prevalenza della violenza nelle aziende sanitarie italiane [ 15 , 30 ]  . 
se gli studi sul rischio di violenza nelle attivit radiologiche sono molto rari nella letteratura mondiale [ 3133 ] , essi sono del tutto assenti per ci che riguarda le attivit di diagnostica per immagini italiane . 
 questo lavoro la prima indagine che mira a valutare la prevalenza delle aggressioni fisiche e verbali contro i radiologi italiani , ad individuarne lorigine e a conoscere le possibili conseguenze per la salute delle vittime . 
in una successiva pubblicazione sar studiata la relazione tra violenza sul lavoro e fenomeni psicosociali ( benessere mentale , stress , sostegno sociale , senso di giustizia , soddisfazione dal lavoro )  . materiali e metodi i radiologi italiani convenuti per il loro congresso nazionale sono stati invitati a compilare un questionario anonimo , nel quale si chiedeva se ciascuno di loro avesse subito , negli ultimi 12 mesi o nel corso della vita lavorativa , una aggressione fisica , una minaccia o una molestia sul lavoro . 
veniva anche richiesto se sul luogo di lavoro avessero mai subito una molestia assillante ( stalking ) , cio un comportamento caratterizzato da richieste insistenti , messaggi , telefonate e altri contatti non richiesti , tali da indurre fastidio , preoccupazione o paura . 
 coloro che rispondevano in maniera affermativa alle precedenti domande , venivano invitati a descrivere un episodio di violenza fisica e , separatamente , non fisica , utilizzando il violent incident form ( vif ) , un questionario proposto da arnetz per la registrazione degli eventi violenti negli ambienti sanitari [ 34 ] e gi applicato nella versione italiana in precedenti studi [ 3538 ]  . 
 il vif descrive uno specifico incidente di violenza o molestia diretto contro un operatore sanitario , comprende domande sullautore della violenza ( sesso , et , stato ) , il tipo di assalto e le conseguenze dellincidente . 
analysis of this part of the questionnaire is the subject of a subsequent study [ 39 ]  . research was authorised by the ethics committee of the rome campus of the universit cattolica del sacro cuore . 
distribution of respondents is representative of the italian society of medical radiology ( sirm ) membership , which in 2009 comprised 9 , 158 , of whom 61.7% were men and 38.2% women , with a greater prevalence in the younger age groups and an absolute predominance of men in the older age groups . 
the characteristics of our sample are reported in table 1 . in the 12 months prior to the study , 59 radiologists ( 5.9% of the entire population ) had suffered physical abuse , whereas 298 ( 30.0% ) reported having been victim of at least one act of physical violence during their working lives . 
the prevalence of verbal abuse was much higher : 162 ( 16.3% ) received threats in the previous year , whereas 484 ( 48.8% ) received threats of physical violence at least once in their working lives . 
in the previous year , 274 ( 27.6% ) experienced other forms of harassment , and 55 ( 5.5% ) reported being the target of violent behaviour at the time of the questionnaire . 
overall , 647 ( 65.2% ) described at least one episode of harassment during their working lives ( table 2 )  . physical violence all violent incidents reported in the previous year occurred in public hospitals or clinics . 
female radiologists in public hospitals and clinics reported having been victim of at least one act una precedente ricerca [ 3 ] mediante il test di ripetizione di spearman - brown ad un mese di distanza ( the one - month test - retest spearman - brown split - half coefficient ) era pari a 0 , 91 ( molto elevata )  . 
il questionario comprendeva quindi una serie di domande relative al benessere psicologico , alla soddisfazione da lavoro , al sostegno sociale , allo stress da lavoro ed alla percezione di giustizia organizzativa . 
lanalisi di questa parte del questionario sar oggetto di un successivo lavoro [ 39 ]  . la ricerca stata autorizzata dal comitato etico delluniversit cattolica del sacro cuore di roma . 
si fatto uso del software pasw / spss 15.0. risultati hanno risposto al questionario 992 radiologi , 610 dei quali ( 61 , 5% ) di genere maschile , 382 ( 38 , 5% ) di genere femminile . 
la distribuzione del campione di rispondenti rispecchia quella degli iscritti alla societ italiana di radiologia medica ( sirm ) , che nel 2009 erano 9158 , per il 61 , 7% maschi e per il 38 , 2% femmine , con una maggiore prevalenza delle colleghe nelle fasce di et inferiori ed una assoluta predominanza dei maschi in quelle di et pi avanzata . 
le caratteristiche del nostro campione sono riportate in tabella 1 . nei 12 mesi precedenti lindagine , 59 radiologi ( 5 , 9% dellintera popolazione ) sono stati fisicamente aggrediti , 298 ( 30 , 0% ) riportano di avere subito almeno una aggressione fisica nel corso delle vita lavorativa . 
162 radiologi ( 16 , 3% ) hanno subito nellultimo anno minacce , 484 ( 48 , 8% ) hanno subito minacce di lesioni fisiche almeno una volta nel corso delle vita di lavoro . 
nellultimo anno , 274 soggetti ( 27 , 6% ) hanno subito altre forme di molestie , e 55 ( 5 , 5% ) dichiarano di essere tuttora sottoposti al comportamento violento al momento dellindagine . 
complessivamente , 647 ( 65 , 2% ) dei soggetti intervistati ricordano e descrivono un episodio di molestia ( tabella 2 )  . violenza fisica tutte le aggressioni fisiche segnalate nellultimo anno si sono verificate nelle strutture pubbliche . 
the frequency of incidents of physical abuse in the previous year was highest among radiologists in the age range 3640 years ( 19.4% ) , which progressively decreased with age to become zero in the older age ranges . 
the level of responsibility of the respondent within the healthcare facility also influences the distribution of violent incidents : the percentage of acts of physical abuse was highest among respondents with a low level of responsibility ( 8.2% ) , lower among respondents with an intermediate level of responsibility and zero among healthcare directors , none of whom were the target of violent behaviour in the previous year . 
la frequenza delle aggressioni fisiche subite nellultimo anno massima per i radiologi nella classe di et tra i 36 e i 40 anni ( frequenza 19 , 4% ) e decresce progressivamente con let , fino ad azzerarsi nelle et pi avanzate . 
anche il ruolo nella struttura sanitaria influenza la distribuzione degli eventi violenti : il tasso di aggressioni fisiche massimo nei dirigenti ( 8 , 2% ) , decresce nei responsabili di struttura semplice e si azzera nei direttori , nessuno dei quali stato fatto oggetto di aggressioni nellultimo anno . 
le aggressioni in prevalenza sono state rappresentate da spinte o afferramento degli abiti accompagnate da grida e minacce ; in un ridotto numero di casi vi sono stati anche pugni ( 9 , 1% ) , schiaffi ( 6 , 4% ) , calci ( 6 , 0% ) , sputi ( 4 , 0% )  . 
molti radiologi hanno anche avvertito ansia ( 22 , 1% ) , umiliazione ( 20 , 1% ) delusione ( 17 , 1% ) , paura ( 15 , 8% ) , angoscia ( 13 , 4% ) e , soprattutto , sensazione di essere indifeso ( 25 , 8% )  . 
i radiologi di genere femminile riportano una pi frequente esperienza di stalking sul lavoro ( 90 casi pari al 23 , 6% contro 115 , 18 , 9% nei maschi ) , ma la differenza non raggiunge significativit statistica ( p < 0 , 08 )  . 
il molestatore prevalentemente maschio ( 477 ; 75 , 1% )  . il tipo di comportamento molesto pi frequentemente descritto consiste nellalzare la voce ( 30 , 1% ) per insultare ( 47 , 3% ) e criticare ( 39 , 3% ) o ridicolizzare ( 9 , 4% ) , spesso aggiungendo minacce di provocare un danno fisico ( 10 , 8% ) o altri tipi di danno ( 17 , 5% )  . 
nonphysical violence , however , was equally present in the public and private sectors and affected 65% of radiologists , with a prevalence of violent behaviour ( frequency in a certain period of time ) of 5.5%. 
the lower number of cases in the under - 35 age group is due to the national health service having frozen recruitment , which has led to a lengthening of the time that young radiologists spend working in the public sector with shortterm contracts , which do not allow them access to jobs in emergency services . 
the prevalence of violent incidents , which we calculated to be 6.8% annually for all radiologists operating in the public sector , is in fact much higher around 20% annually for young radiologists working in emergency services . 
although the physical harm associated with these violent incidents is moderate in most cases , the emotional consequences are much more significant and prompt the desire to change jobs in one third of victims . 
 this begs questions regarding the effects these violent behaviours may have on the psychophysical well - being of radiologists , on their levels of stress and job satisfaction , on their clinical and diagnostic capabilities and on their degree of commitment to their job . 
we will seek to respond to these queries in a subsequent study . ste nellignorare volutamente ( 7 , 9% ) o nel fare riferimenti di natura sessuale ( 4 , 2% ) o inviare messaggi lettere e sms non richiesti ( 8 , 7% )  . 
 le conseguenze immediate degli atti di violenza non fisica sono analoghe a quelle della violenza fisica : rabbia ( 55 , 8% ) , delusione ( 29 , 5% ) , ansia ( 21 , 9% ) , sensazione di essere indifeso ( 18 , 5% ) e umiliazione ( 14 , 5% )  . 
con percentuale minore , i radiologi aggrediti avvertono anche angoscia ( 13 , 6% ) , paura ( 5 , 9% ) , senso di colpa ( 4 , 6% )  . 
gli atti di violenza fisica hanno una prevalenza del 6 , 8% annuo e riguardano esclusivamente gli operatori delle strutture pubbliche e , tra questi , soprattutto coloro che lavorano nei servizi di pronto soccorso ed emergenza . 
la violenza non fisica , viceversa , egualmente presente nelle strutture private ed in quelle pubbliche e riguarda circa il 65% dei radiologi , con una prevalenza puntuale dei comportamenti violenti ( frequenza in un determinato momento temporale ) pari al 5 , 5% . 
 lapparente effetto protettivo nella fascia di et pi giovane , al di sotto dei 35 anni , dovuto al blocco delle assunzioni nel servizio sanitario nazionale e al conseguente allungamento dei tempi che i giovani radiologi trascorrono lavorando nei servizi pubblici con rapporti di lavoro precario o a progetto , che non consentono loro di accedere ai servizi di pronto soccorso ed emergenza . 
la prevalenza degli atti di violenza fisica , che abbiamo calcolato pari al 6 , 8% annuo per tutti i radiologi operanti nelle strutture pubbliche , in realt molto pi alta , circa il 20% annuo , per i giovani radiologi impegnati nei servizi di emergenza ed urgenza . 
 bench i danni fisici associati a queste aggressioni siano nella maggior parte dei casi modesti , le conseguenze emotive sono assai rilevanti e determinano , in circa un terzo delle vittime , limpulso ad abbandonare il posto di lavoro . 
c da chiedersi quali siano i danni che tali aggressioni possono comportare sullo stato di equilibrio psicofisico dei radiologi , sul loro livello di stress e soddisfazione da lavoro , sulle radiol med ( 2012 ) 117 : 10191033 1029 even though the perpetrator of the violence is prevalently a patient or a patients companion , a significant finding is the fact that a quarter of all cases of physical violence and almost half of the cases of verbal abuse were perpetrated by a colleague or a superior . 
the aggressor is in most cases a man and most often the patient or the companion of the patient , although a significant number of violent acts were perpetrated by nurses , doctors or other radiologists . 
several factors relating to the victim were also identified , such as the radiologist working alone or working in close contact with the patient , whereas others were related to the aggressor , such as alcohol and drug use / abuse . our study has the limitation of being based exclusively on survey data and is therefore subject to recall bias . 
nonetheless , compared with other studies in the literature , ours has the advantage of being based on a relatively large series that , precisely because of its size , is representative of italian radiologists in terms of sex and age distribution . 
the agreement between our results and those reported in the literature gives us the confidence to propose effective measures for prevenient the risk of violence in the radiological workplace . we believe that in order to identify the most appropriate preventive measures , external violence i.e. 
the first form , which is most commonly characterised by physical aggression , has been studied in capacit clinico - diagnostiche e sul grado di coinvolgimento nella propria attivit lavorativa ; a questo quesito ci proponiamo di risponder in un successivo lavoro . anche se laggressore prevalentemente un paziente o un accompagnatore , non va sottovalutato il dato secondo cui in circa un quarto dei casi di violenza fisica e in quasi la met delle aggressioni verbali laggressore un collega o un superiore . 
laggressore nella gran maggioranza dei casi un maschio , per lo pi un paziente o un parente o accompagnatore del paziente , ma una quota significativa delle aggressioni portata da infermieri , medici o altri radiologi . 
gli autori indicano come possibili cause della violenza contro i radiologi alcuni problemi strutturali , come i lunghi tempi di attesa , le carenze di organico ed i problemi di comunicazione . 
sono altres identificati alcuni fattori inerenti alla vittima , come il fatto di lavorare da solo , o di dover agire a stretto contatto con il paziente , o legati allaggressore , come labuso di alcool e luso di droghe . il nostro lavoro presenta la limitazione di essere basato esclusivamente su dati anamnestici ed pertanto soggetto allerrore sistematico di richiamo ( recall bias )  . 
inoltre la risposta volontaria nel corso di un congresso pu avere introdotto un errore di selezione ( selection bias ) la cui esistenza , intensit e direzione non sono determinabili . 
tuttavia , rispetto ai lavori presenti in letteratura , esso ha il vantaggio di aver raccolto una casistica ragguardevole e che , proprio per le dimensioni , corrisponde alla distribuzione dei radiologi italiani per genere e classi di et . 
la corrispondenza dei risultati da noi raccolti con quelli della letteratura , ci rende confidenti di poter proporre misure efficaci per la prevenzione del rischio di violenza sul lavoro in ambito radiologico . secondo la nostra opinione , per identificare le pi opportune misure preventive necessario considerare separatamente la violenza esterna , cio iniziata da pazienti , loro accompagnatori e parenti o soggetti estranei allospedale , e quella interna , che portata da colleghi o superiori . 
administering treatment , particularly if invasive , explaining to patients what they can and cannot do and performing procedures in close contact with patients can expose healthcare workers to acts of physical aggression , especially if the patients are demented , disturbed or under the effects of medication or drugs [ 3 ]  . 
it has been observed that the risk of physical violence is seven to nine times higher in workers who perform these kinds of activities in close contact with patients than in those who have little contact with them [ 40 ]  . 
 [ 33 ] , it is clear that the radiologist is also exposed to this type of aggression when having to work alone , which often occurs in outlying emergency services . 
 the obvious solution is to have the patient accompanied by appropriate personnel when they need to undergo diagnostic imaging . a different mechanism underlies the physical and verbal violence from the patients relatives , friends and companions . 
 however , the real factor that should be considered is the anxiety these people experiencing while waiting for their loved ones to undergo the prescribed tests , their limited knowledge of the workings of a hospital or a casualty ward and the lack of communication between the hospital and those waiting for its services . 
anyone who is unaware of the way triage works will find it difficult to understand how their loved ones can have to wait their turn while patients arriving after them are treated or why they might have to wait many hours in anxiety and discomfort without receiving any news regarding the decisions being made on their account . 
in these potentially explosive situations , the radiologist may be the first physician to come into contact with the patients companion , and he or she may not necessarily be prepared to manage the communication between hospital and patients . 
preventing these incidents requires a set of measures that involve reorganisation of the layout of emergency services in a manner more favourable to patients , reduction in waiting times and a proactive role adopted by the healthcare personnel in providing information regarding diagnostic procedures on admission . 
in this setting , implementing training programmes to improve communication skills of the radiologist would be useful . the fact that most cases of physical abuse involve young radiologists operating in public clinics and hospitals emphasises the need for appropriate training for these operators on how to manage violent incidents . 
la somministrazione di trattamenti , specie se invasivi , lindicazione di obblighi o divieti e lesecuzione di manovre a stretto contatto con i pazienti possono esporre ad aggressioni fisiche , specie se i pazienti sono dementi , agitati o sotto leffetto di farmaci o droghe [ 3 ]  . 
 stato osservato che il rischio di violenza fisica da 7 a 9 volte pi alto nei lavoratori che svolgono queste attivit a diretto contatto con il paziente , rispetto a coloro che hanno pochi contatti con essi [ 40 ]  . 
 [ 33 ] , si osserva che anche il radiologo esposto a questo tipo di aggressione quando si trova a lavorare da solo , cosa che avviene soprattutto nei servizi periferici di emergenza e urgenza . 
la pi ovvia soluzione che il paziente sia accompagnato da personale appropriato quando deve sottoporsi a diagnostica per immagini . un meccanismo diverso allorigine delle aggressioni fisiche e verbali da parte di parenti , amici e accompagnatori di pazienti . 
i fattori pi spesso allorigine di queste aggressioni sono i tempi , spesso eccessivamente lunghi , di attesa ; ma il vero fattore , a ben considerare , lo stato di ansia nel quale si trovano queste persone nellattesa che il loro caro esegua gli accertamenti prescritti , la loro scarsa conoscenza dei meccanismi di un ospedale o di un pronto soccorso , lassenza di comunicazioni tra la struttura ospedaliera e coloro che sono in attesa per accedervi . 
chi non a conoscenza dei meccanismi del triage avr difficolt a capire perch il proprio caro sia stato scavalcato nellordine di servizio da altri pazienti arrivati dopo di lui o perch sia necessario trascorrere alcune ore , spesso non poche , in uno stato di sofferenza e scomodit , senza avere notizia delle decisioni che qualcun altro sta prendendo sul nostro conto . 
in queste situazioni potenzialmente esplosive , a volte il radiologo il primo medico che entra in contatto con gli accompagnatori e non necessariamente egli preparato a gestire la comunicazione tra lospedale ed i pazienti . 
la prevenzione di questi incidenti richiede un complesso di misure , che comportino la riorganizzazione del layout dei servizi di pronto soccorso in senso pi favorevole ai pazienti , con la riduzione dei tempi di attesa e con un intervento proattivo da parte del personale sanitario nella trasmissione delle informazioni sulle procedure diagnostiche di ammissione , al fine di stemperare lansia di pazienti e visitatori e al tempo stesso chiarire e delimitare i compiti del servizio sanitario . 
in questo quadro sarebbe utile migliorare le capacit di comunicazione del radiologo , mediante idonee esperienze formative . la constatazione che la maggior frequenza di aggressioni fisiche si verifica contro giovani radiologi che operano nelle strutture pubbliche induce a ritenere che tali categorie debbano essere opportunamente istruite sulle modalit di gestione degli incidenti violenti . 
the programmes should also include methods for calming aggression and controlling violent situations . our study shows that a significant percentage of violent incidents , especially nonphysical incidents , is perpetrated by colleagues or superiors . 
first , the healthcare authority should lay down a policy of zero tolerance of violence in all its forms and therefore provide for actions aimed at counteracting bullying [ 41 ] and mobbing [ 42 ] , which are the most common forms of violence in the workplace , but also other forms of violence , such as stalking [ 43 ] and sexual harassment [ 44 ]  . 
the role of this third party would be to listen to the victims and set in motion support services and counselling , as well as measures for verifying the reported incidents , which could be used as the basis for enacting the disciplinary measures laid down in the authoritys policy . 
 sabilit della prevenzione del rischio , della predisposizione delle misure di sicurezza e della formazione e informazione dei lavoratori al datore di lavoro ( quindi al direttore generale nelle aziende sanitarie locali )  . 
lo stesso principio di responsabilit , pur nella differenziazione dei compiti , grava sul dirigente ( il direttore della struttura ) e sul preposto ( il dirigente medico )  . 
sarebbe opportuno che anche listruzione universitaria contribuisse alla formazione di una cultura condivisa , introducendo nei programmi una formazione specifica sulla violenza , sui suoi determinanti e sui fattori precipitanti , nonch sulle modalit per stemperare laggressivit e controllare le situazioni di violenza . nella nostra indagine si osserva che una quota non trascurabile delle aggressioni , specie di natura non fisica , provocata da altri colleghi o superiori . 
in primo luogo , opportuno che lazienda sanitaria esprima una politica aziendale ( policy ) di tolleranza zero verso la violenza in tutte le sue forme , e quindi preveda azioni di contrasto del bullying [ 41 ] e del mobbing [ 42 ] che sono le pi comuni forme di violenza tra lavoratori , ma anche delle altre forme di violenza , come lo stalking [ 43 ] e la molestia sessuale [ 44 ]  . 
il lavoratore deve essere incoraggiato a segnalare tutte le forme di molestia , tramite listituzione di una figura terza non appartenente alla struttura aziendale , con funzione di ascolto e con la possibilit di attivare sia interventi di sostegno e counseling della vittima , sia procedure di accertamento dei fatti segnalati , dalle quali potranno scaturire i provvedimenti disciplinari previsti dalla policy aziendale . 
in italy , even failure to consider violence amongst occupational risks and the lack of a prevention plan could lead to criminal sanctions , regardless of whether acts of aggression have occurred against workers or not . 
we therefore trust that this study will help raise awareness among radiologists about the problem of violence in the workplace and prompt implementation of effective preventative strategies . conclusioni in conclusione , la violenza contro i radiologi un fenomeno di rilevante importanza , ma sostanzialmente misconosciuto . 
 non ci pare possibile ignorare il fatto che mediamente ogni anno un giovane radiologo su cinque viene aggredito fisicamente , e che anche in questo momento un radiologo su venti sottoposto sul lavoro a violenza verbale . 
la realizzazione di strategie per la tempestiva eradicazione della violenza dai luoghi di lavoro , leliminazione dei fattori predisponenti o scatenanti e lassistenza ai lavoratori colpiti rientrano tra gli obblighi del datore di lavoro . 
in italia anche lomessa considerazione della violenza tra i rischi professionali e la mancanza di un piano di prevenzione potrebbero comportare sanzioni penali , indipendentemente dal verificarsi di aggressioni e di danni per i lavoratori . 
fileni2 1istituto di medicina del lavoro , universit cattolica del sacro cuore , largo gemelli 8 , 00168 roma , italy 2istituto nazionale di riposo e cura dellanziano ( inrca ) , roma , italy correspondence to : n . 
physical violence experienced in the previous 12 - month period was associated with the radiologists poor mental health [ odds ratio ( or ) 1.11 ] and overcommitment to work ( or 1.06 ) , whereas radiologists in good physical health ( or 0.64 ) , with job satisfaction ( or 0.96 ) and with overall happiness ( or 0.67 ) were less exposed . 
un intervento preventivo sulla violenza nei luoghi di lavoro deve migliorare lorganizzazione del lavoro e i rapporti interpersonali tra i lavoratori . parole chiave violenza radiologo giustizia felicit soddisfazione introduction introduzione violence in the workplace is a relevant risk for healthcare workers [ 15 ]  . 
in a previous paper we evaluated the prevalence of the phenomenon in la violenza sul lavoro un rischio rilevante per i lavoratori della sanit [ 15 ] ; i radiologi , soprattutto quelli impegnati nei servizi di emergenza e pronto soccorso , sono anchessi esposti a tale rischio [ 68 ]  . 
 in particular , we aimed to evaluate the association between radiologists , in its broadest definition of psychosocial and social wellbeing , and physical or verbal abuse experienced in the workplace . biamo valutato la prevalenza del fenomeno in italia , le sue caratteristiche e le principali conseguenze immediate degli atti violenti [ 9 ]  . 
il 6 , 8% dei radiologi nelle strutture pubbliche ha subito negli ultimi 12 mesi una aggressione fisica , soprattutto da parte di pazienti o loro accompagnatori , ed il 5 , 5% ha dichiarato di essere tuttora sottoposto a comportamenti violenti di natura non fisica al momento dellindagine . 
in particolare , intendiamo valutare lassociazione tra la salute dei radiologi , nella sua accezione pi ampia di benessere psicofisico e sociale , e la violenza fisica o verbale subita sul lavoro . materials and methods materiali e metodi italian radiologists who attended the annual national congress were invited to fill in an anonymous questionnaire containing questions on physical violence experienced in the workplace . 
the questionnaire investigated the main variables potentially linked with violence : physical and mental well - being , job strain , satisfaction and happiness , social support and perception of organisational justice : 1 . 
physical health was self - assessed with a single question : how would you judge your overall health ? respondents were required to give a graded response from 1 ( major problems ) to 5 ( very good )  . 
in the original version , the warr scale consists of 15 questions each with responses on a 7 - point likert scale ranging from 1 = extremely unsatisfied to 7 = extremely satisfied . 
 in research studies on physicians [ 1216 ] , the scale has been used in a reduced 10 - question version , the last question of which asks for an overall assessment ( from 1 to 7 ) on job satisfaction . 
with this question we were able to divide the healthcare workers into two groups : those who were satisfied with their jobs ( response from 5 = moderately satisfied to 7 = extremely satisfied ) and those who were unsatisfied ( responses from 1 = extremely unsatisfied to 3 = moderately unsatisfied )  . 
in the original study the i radiologi italiani convenuti per il loro congresso nazionale sono stati invitati a compilare un questionario ano nimo , contenente domande sulla violenza fisica subita sul lavoro . 
la scala di warr nella versione originale consta di 15 domande , a ciascuna delle quali si pu rispondere , secondo una scala likert in 7 punti , che va da estremamente insoddisfatto ( 1 punto ) a estremamente soddisfatto ( 7 punti )  . 
nelle ricerche sui medici [ 1216 ] tale scala stata usata in una versione ridotta in 10 domande , lultima delle quali chiede di esprimere un giudizio complessivo , sempre espresso da 1 a 7 , sulla soddisfazione professionale . 
questa domanda consente di dividere i lavoratori in due gruppi : quelli soddisfatti del lavoro ( risposte da 5 , moderatamente soddisfatto a 7 estremamente soddisfatto ) e quelli insoddisfatti ( risposte da 1 estremamente insoddisfatto a 3 moderatamente insoddisfatto )  . 
in our study we reduced the questions on the r scale to 10 , because the first question ( my superiors treat me with due respect ) was not applicable to the freelance radiologists or those at the top of the hierarchy . 
the response was graded with a 5 - point likert scale ranging from 1 = disagree , does not apply to 5 = i fully agree , does apply and very strained . 
the eri effort scale was homogeneous ( 65.68% single factor ) , as was the overcommitment scale ( 66.43% single factor ) , whereas the reward scale , as in the original version , contains three components ( overall variance 69.9% ) , with high correlation of all the items with the first factor ( 47% )  . 
il questionario , tradotto e validato in italiano [ 22 ] composto di 22 domande , 5 relative allimpegno lavorativo ( scala e , effort ; es : sono sempre sotto pressione per il carico di lavoro ) , 11 alle ricompense ( scala r , reward ; es . : sono trattato ingiustamente sul lavoro ) , e 6 alleccessivo impegno ( scala o , overcommitment ; es . : sono facilmente sopraffatto dal ritmo eccessivo di lavoro )  . 
in questo studio abbiamo ridotto a 10 le domande della scala r , perch la prima domanda ( i superiori mi trattano con il dovuto rispetto ) non era applicabile ai radiologi liberi professionisti n agli apicali . 
la risposta graduata mediante scale likert in 5 punti , da 1 = non sono daccordo , non si applica a 5 = sono del tutto daccordo , ci mi stressa molto . 
la consistenza interna del questionario , cio la percentuale di varianza che ciascuna scala spiega rispetto allipotetica varianza reale delluniverso , misurata mediante il coefficiente alfa di cronbach , risultata buona , cio superiore all80% , per tutte le tre scale delleri ( rispettivamente : effort = 0 , 89 ; reward = 0 , 88 ; overcommitment = 0 , 89 )  . 
 la scala effort delleri risulta omogenea ( 65 , 68% unico fattore ) e cos la scala overcommitment ( 66 , 43% un solo fattore ) , mentre la scala reward contiene , come nella versione originale , tre componenti ( varianza complessiva 69 , 9% ) , con elevata correlazione di tutti gli item con il primo fattore ( 47% )  . 
la scala support composta da 6 domande ( es . : nel posto di lavoro c unatmosfera calma e piacevole ) la cui risposta graduata tra 1 = non mai cos a 4 = proprio cos . 
 laffidabilit del questionario molto elevata , con un alfa di cronbach pari a 0 , 92 per lintero questionario , e con alfa rispettivamente pari a 0 , 94 per la sub - scala radiol med ( 2012 ) 117 : 10341043 1037 ethics committee of the rome campus of the universit cattolica del sacro cuore . 
lastly , a stepwise backwards selection method was used to evaluate which of the psychosocial variables significantly associated with the violent events had the greatest weight in a multiple logistic regression model . results sample characteristics are reported in table 1 . 
the binary logistic regression analysis was performed by associating the value 0 with participants who had not and the value 1 with participants who had experienced physical abuse in the previous 12 months . 
a positive state of physical health is significantly correlated in a protective sense with events of physical abuse ( or 0.64 ) , as is job satisfaction ( or 0.96 ) and happiness ( or 0.64 ) , whereas poor psychological well - being ( or 1.11 ) and job strain or overcommitment ( or 1.06 ) increase the risk of physical aggression . similarly , with regard to verbal abuse occurring at the time of the study , logistic regression analysis was performed that indicated a significant protective association with health ( or 0.54 ) , job satisfaction ( or 0.96 ) , happiness ( or 0.81 ) , perception of organisational justice ( or 0.94 ) and social support ( or 0.80 ) , and a negative association with poor psychological well - being ( or 1.10 ) and job strain ( or 1.14 ) ( table 3 )  . we then evaluated which variable was most closely associated with events of physical violence . 
we used a multivariate logistic regression model with backwards stepwise selection in which we inserted all psychosocial variables that were found to be associated in the previous univariate model ( health , psychological well - being , job satisfaction , happiness , job strain ) , as well as sex , role and age . 
the results show that the variables most associated with events of physrelazionale , 0 , 88 per la giustizia distributiva , 0 , 79 e 0 , 63 per le altre due scale di giustizia procedurale . 
stata quindi applicata la regressione logistica binaria per studiare la relazione tra ciascuna variabile e lesperienza di eventi violenti , calcolando il rischio relativo ( odds ratio , or ) ed i relativi intervalli di confidenza al 95% . 
il rischio relativo cos ottenuto stato quindi corretto introducendo nel modello di regressione logistica il sesso , let , il ruolo ed il tipo di struttura ( pubblica o privata )  . 
infine , mediante selezione retrograda condizionale ( stepwise backward ) , si valutato quale delle variabili psicosociali significativamente associate alle aggressioni , avesse maggiore peso in un modello di regressione logistica multipla . risultati le caratteristiche del campione sono riportate nella tabella 1 . 
lanalisi della regressione logistica binaria , effettuata ponendo con valore 0 i soggetti che non avevano subito una aggressione fisica negli ultimi 12 mesi , e con valore 1 coloro che invece lavevano subita , ha indicato che numerose variabili psicosociali risultano significativamente associate con lesperienza di aggressioni nellultimo anno . 
this study shows that physical abuse , which exclusively affects healthcare workers in the casualty wards and emergency services of public hospitals , for the most part involves individuals with physical or psychological health problems and who are excessively committed to their work , whereas healthcare workers who experience job satisfaction and are happier are relatively protected . 
even verbal abuse and harassment , of which radiologists were victims at the time of the study , is associated with poor physical and psychological health , dissatisfaction and unhappiness , as well as with a low level of social support and perception of organisational justice . 
il risultato indica che le variabili maggiormente associate alle aggressioni fisiche , oltre al lavoro nella struttura pubblica , sono il ruolo gerarchico ( sono protetti i livelli apicali ) , lo stato di salute fisica ( sono protetti i sani ) , il malessere psicologico ( sono pi colpiti i soggetti con disturbi ) , la felicit ( sono protetti i soggetti pi felici ) ( tabella 4 )  . 
da questo studio emerge che le aggressioni fisiche , che riguardano esclusivamente gli addetti a servizi di pronto soccorso ed emergenza nelle aziende pubbliche , colpiscono soprattutto soggetti con problemi di salute fisica o mentale ed eccessivo attaccamento al lavoro , mentre i lavoratori pi soddisfatti dal lavoro e pi felici sono relativamente protetti . 
it is likely that the person experiencing the violent event feels little social support and perceives the occupational organisation as unjust and has a low level of job satisfaction , happiness and physical and psychological health . 
that an unsatisfied and unhappy individual who is relatively isolated and suffering problems of physical and psychological health is more exposed to violent events . in the literature , individuals who report mistreatment generally express low levels of social support and a sense of isolation , psychological distress and low levels of overall happiness . 
happiness has been associated with various positive effects on health for two reasons : it is associated with favourable lifestyles and favourable biological responses to job strain [ 27 ]  . 
studies conducted in the elderly indicate that those with limited psychological fisica e mentale , linsoddisfazione e linfelicit , e con un basso livello di sostegno sociale e di giustizia organizzativa percepita . 
i fattori pi strettamente associati alle aggressioni fisiche , oltre al fatto di lavorare in un pronto soccorso pubblico , sono il basso ruolo gerarchico , il malessere fisico e mentale , linfelicit . 
 verosimile che chi oggetto di violenza avverta poco sostegno sociale e percepisca lorganizzazione lavorativa come ingiusta , abbia un basso livello di soddisfazione e felicit e di salute fisica e mentale . 
plausibile per anche la relazione inversa , e cio che un soggetto insoddisfatto e infelice , relativamente isolato e con problemi fisici e mentali sia maggiormente esposto alle aggressioni . nella letteratura , i soggetti che riportano maltrattamento esprimono generalmente bassi livelli di sostegno sociale e senso di isolamento , bassi livelli di felicit globale e distress psicologico . 
la felicit stata associata con vari effetti positivi per la salute per due motivi : essa si associa con risposte biologiche favorevoli allo stress e con stili di vita favorevoli [ 27 ]  . 
odds ratio ( or ) e intervalli di confidenza ( ic ) al 95% calcolati mediante modelli univariati di regressione logistica , non corretti e corretti per et , sesso , ruolo , tipo di struttura pubblica o privata variabile violenza fisica , un anno molestia attuale or ( ic 95% ) non corretto or ( ic 95% ) corretto or ( ic 95% ) non corretto or ( ic 95% ) corretto stato di salute malessere psicologico soddisfazione felicit stress da lavoro stress intrinseco giustizia organ . 
positive emotions , such as calmness , peace , happiness and ability to combat strain are , on the other hand , associated with improvement in health which ensues from health - promotion programmes in the workplace [ 29 ]  . 
on the other hand , the ability to combat strain should not be confused with expending high levels of physical effort to the point of ignoring ones own physiological needs , which is known as john henryism among us psychologists [ 30 ] , nor with phenomena of karoshi ( death from overwork ) and karojisatsu ( suicide from overwork ) , described several years ago by japanese physicians [ 31 ]  . 
these dramatic consequences of job strain follow from overcommitment , which was measured in our study . physicians , and more in general those in the caring professions , often have a behavioural profile of this type , tending to react to environmental tensions by increasing work commitment and overlooking their own needs , which they replace with achieving results in their job [ 32 ]  . 
in the nursing profession , overcommitment is associated with the onsugli anziani indicano che i soggetti con scarse risorse psicologiche o con deficit psicologici sono pi vulnerabili al maltrattamento , e il maltrattamento risulta particolarmente nocivo per queste persone [ 28 ]  . 
le emozioni positive , come calma , pace , felicit e capacit di opporsi allo stress , risultano daltro canto associate al miglioramento di salute che consegue ai programmi di promozione della salute nei luoghi di lavoro [ 29 ]  . 
daltro canto , la capacit di opporsi allo stress non va confusa con limpegno strenuo fino al punto di ignorare le proprie esigenze fisiche , detto henryismo dagli psicologi americani [ 30 ] , n coi fenomeni del karoshi o morte da superlavoro , e del karojisatsu , suicidio da superlavoro , descritti qualche anno fa nei medici giapponesi [ 31 ]  . 
queste drammatiche conseguenze dello stress conseguono difatti ad un impegno eccessivo , che viene anche indicato come overcommitment , e che stato misurato nella nostra indagine . i medici , e pi in generale coloro che scelgono professioni di aiuto , hanno spesso un profilo comportamentale di questo tipo , reagiscono alle tensioni ambientali aumentando limpegno nel lavoro e trascurano le proprie esigenze , alle quali antepongono il raggiungimento del risultato lavorativo [ 32 ]  . 
the tendency to overcommitment is negatively associated with happiness , especially among men , and this is considered a relevant element to bear in mind when developing public health programmes [ 30 ]  . 
even in our study , many radiologists who were victims of physical or verbal abuse expressed the intention of changing their way of operating or changing their job [ 9 ]  . few studies have taken into consideration the workplace environment in relation to conflicts that occur there , and the published studies take into account only a part of the psychosocial factors and the consequences for the wellbeing of healthcare workers . 
among nurses who work in conditions of staff shortages , a high level of perceived justice is associated with a normalisation of the levels of satisfaction and commitment [ 37 ]  . 
clearly , therefore , a programme aimed at reducing violence in the workplace must include a commitment to improve the levels of procedural and distributive justice in the work organisation and the relationships between workers in order to avoid conflicts and increase the well - being , health and productivity of healthcare workers . in conclusion , our study shows that the phenomenon of parsa di disturbi depressivi [ 33 ]  . 
la propensione allimpegno eccessivo associata negativamente alla felicit , soprattutto tra i maschi , e ci considerato un rilevante elemento del quale tenere conto nella predisposizione dei programmi di salute pubblica [ 30 ]  . 
anche nella nostra indagine , molti dei radiologi che erano stati oggetto di aggressioni fisiche o verbali hanno manifestato lintenzione di cambiare modo di fare , o di cambiare posto di lavoro [ 9 ]  . pochi studi hanno preso in considerazione lambiente di lavoro in relazione ai conflitti che vi avvengono , e quelli pubblicati tengono in conto solo in parte dei fattori psicosociali e delle conseguenze per la salute dei lavoratori . 
un recentissimo studio svedese indica tra i fattori che riducono la probabilit di conflitti la giustizia procedurale ( correttezza delle decisioni ) ed il sostegno sociale [ 35 ]  . 
nelle infermiere che lavorano in condizioni di carenza di personale , un alto livello di giustizia percepita si associa con una normalizzazione dei livelli di soddisfazione e di impegno [ 37 ]  . 
evidente quindi che un programma mirante a ridurre la violenza nei luoghi di lavoro deve prevedere un impegno per migliorare i livelli di giustizia procedurale e distributiva nellorganizzazione del lavoro e le relazioni tra i lavoratori , al fine di evitare i conflitti ed aumentare il benessere , la salute e la produttivit dei lavoratori . in conclusione , il nostro studio dimostra che il fenomeno della violenza nei radiologi che ne fanno esperienza si 1042 radiol med ( 2012 ) 117 : 10341043 radiologists experiencing violence in the workplace is associated with those with poor physical and psychological health and possibly with negative behaviour , such as overcommitment and social isolation , the perception of an unjust work environment , professional job dissatisfaction and overall unhappiness . 
violence in the workplace is therefore a much more severe problem than the modest levels of physical harm reported or the low number of reports by victims would lead us to believe . 
this observation strengthens the need to counter violence in the workplace and promote continuous improvement in working conditions . associa con un cattivo stato di salute fisica e mentale e con talune attitudini negative , come leccessivo impegno sul lavoro e lisolamento sociale , la percezione dellambiente di lavoro come ingiusto , linsoddisfazione professionale e linfelicit nella vita . 
la violenza sul lavoro quindi un fenomeno molto pi grave di quanto potrebbero far intendere la modestia dei danni fisici riportati , o il ridottissimo numero di denunce da parte delle vittime . 
sartor springer - verlag berlin heidelberg , 2009 isbn : 978 - 3 - 540 - 77982 - 7 eisbn : 978 - 3 - 540 - 77984 - 1 doi 10.1007 / 978 - 3 - 540 - 77984 - 1 published online : 7 january 2012 springer - verlag 2012 six - hundred and eigthy - six plus 6 subject index pages are to be found in the 39 chapters of this book . 
at first sight the topic is one that makes your heart skip a beat : however going through the text the reader realises how well thorough it has been planned and organized in order to provide a full and precise insight into the subject . the book starts with an introductory chapter on bone tumour epidemiology , classification and pathology ; then five chapters deal with diagnostic tools stressing the importance of magnetic resonance imaging ( mri ) , computed tomography ( ct ) , ultrasound ( us ) , nuclear medicine and positron emission tomography ( pet ) without forgetting the role of simple , yet so important , standard plain x - ray films . 
 the following six chapters highlight the role of the above diagnostic tools in the clinical setting regarding prognosis , surgical staging , and response to available therapies . then comes the bulk of the book : eighteen chapters discussing all types of tumours including radiation - induced or reactive metabolic or tumour - like lesions and seven chapters devoted to tumours that can be found in peculiar locations ( ribs and clavicles or scapula , for example )  . 
 the last two chapters deal with compartmental anatomy important in diagnosis and therapy results and the last one with more or less long biographies of those names that are linked and synonymous with bone tumours . each chapter not only is exhaustive in its presentation , lay - out and content but also enriched by the excellent choice of reproduced images , helping the reader become acquainted with the type of lesion presented . perusing the literature referred to within the text one realizes how important the contribution of italian scholars questo volume composto da 39 capitoli , 686 pagine totali , cui aggiungere le 6 dellindice . 
a prima vista , il soggetto tale da mettere in crisi il lettore : tuttavia leggendo e scorrendo il testo ci si rende conto di quanto bene sia stata pianificata ed organizzata la materia , in modo tale da renderne quanto pi completa , precisa ed approfondita la sua conoscenza . il volume inizia con un capitolo introduttivo sullepidemiologia , classificazione ed aspetti anatomo - patologici dei tumori dello scheletro ; i successivi cinque di questa prima parte trattano gli strumenti diagnostici , mettendo in opportuna luce limportanza di risonanza magnetica ( rm ) , tomografia computerizzata ( tc ) , ecografia , medicina nucleare e tomografia ad emissione di positroni ( pet ) , senza tuttavia dimenticare il ruolo del semplice , ma sempre importante , esame radiologico tradizionale . 
 i seguenti sei capitoli mettono in evidenza il ruolo e limportanza degli strumenti diagnostici di cui sopra dal punto di vista clinico nei riguardi della prognosi , stadiazione chirurgica e risposta alle terapie disponibili . 
 a questi capitoli fa seguito il nocciolo duro dellopera : diciotto capitoli che discutono tutti i tipi di tumori scheletrici compresi quelli radio - indotti ed anche le lesioni reattive metaboliche e simil - tumorali , nonch sette capitoli dedicati ai tumori che possono essere trovati in sedi particolari ( coste e clavicole oppure la scapola , per esempio )  . gli ultimi due capitoli si occupano dellanatomia topografico - compartimentale assai importante sia nella diagnosi che nei risultati della terapia e di biografie pi o meno lunghe di coloro i cui nomi sono legati o sinonimo di un tumore osseo . ciascun capitolo non solo completo ed esaustivo nella sua presentazione , impostazione grafica e contenuto , ma anche arricchito da una eccellente scelta delle immagini , che aiutano il lettore a familiarizzare al meglio con il tipo di lesione in studio . 
 nel passare in rassegna e leggendo con attenzione le voci bibliografiche citate nei vari capitoli ci si rende conto dellimportante contributo degli studiosi italiani alla materadiol med ( 2012 ) 117 : 12701271 1271 to the field has been following prof . 
campanaccis and his schools footsteps . the editors and their international team of experts in the field have produced an important and impressive book giving the radiologist ( expert or in training ) as well orthopaedic surgeons and oncologists a reference text to be used in daily practice in order to obtain the best results in patient care , a text i am sure will shortly become a must in radiology departments and clinics . ria , nella scia della la strada indicata dal prof . 
colosimo1 1istituto di radiologia , universit cattolica del sacro cuore , roma , italy 2istituto di igiene , universit cattolica del sacro cuore , roma , italy correspondence to : r . 
gemelli 8 , 00168 roma , italy , tel . : + 39 - 06 - 30154494 , fax : + 39 - 06 - 35501928 , e - mail : rosellinarusso@gmail.com received : 16 may 2011 / accepted : 14 july 2011 / published online : 28 june 2012 springer - verlag 2012 abstract purpose . 
we evaluated size , signal intensity and contrast enhancement and calculated apparent diffusion coefficient ( adc ) , relative cerebral blood volume ( rcbv ) , percentage of signal intensity recovery ( psr ) and maximum values of n - acetylaspartate ( naa ) , choline ( cho ) , creatine ( cr ) , lipids ( lip ) , naa / cr and cho / cr . 
 abbiamo valutato dimensioni , caratteristiche di segnale e contrast enhancement ( ce ) , calcolato coefficiente di diffusione apparente ( adc ) , volume cerebrale ematico relativo ( rcbv ) , percentuale di recupero della curva ( rc ) , valori massimi di n - acetil - aspartato ( naa ) , colina ( cho ) , creatina ( cr ) , lipidi ( lip ) , naa / cr , cho / cr . 
rispetto alla sostanza bianca normale il rcbv nelle lesioni era superiore ( 3 , 301 , 59 ) e nelledema perilesionale inferiore ( 0 , 420 , 15 )  . 
the incidence of brain metastases is rising , not only as a result of the use of advanced combination therapies against the primary tumour and the decrease in mortality rates but also as a result of the new neuroradiology techniques [ 2 , 3 ]  . 
the tumours with the greatest tendency to metastasise to the intracranial region are , in decreasing order , lung cancers , breast cancers , melanoma , colorectal cancers and urogenital cancers [ 57 ]  . 
at diagnosis , 50% of brain metastases are solitary and arise at the following sites : brain hemisphere ( 60% ) , cerebellum ( 30% ) and brain stem ( 10% ) [ 10 ]  . 
when solitary and in the absence of a known primary , brain metastases enter the differential diagnosis with a wide range of conditions , most commonly with high - grade gliomas , brain lymphomas and abscesses and , least commonly , with inflammatory / demyelinating lesions and ischaemic lesions . 
thanks to its multiparametric and multiplanar capabilities , high - contrast resolution , limited invasiveness and use of nonionising energy , magnetic resonance ( mr ) imaging is the modality of choice in the study of expansile brain lesions in general and of metastases in particular . 
to increase mr imaging specificity , nonmorphological techniques , such as diffusion - weighted ( dwi ) and perfusion - weighted ( pwi ) imaging and mr spectroscopy have emerged that provide cytostructural , haemodynamic and metabolic information [ 1115 ] to assist in the differential diagnosis . 
on the basis of our data and the most recent literature , we defined the most significant findings of morphological and nonmorphological mr imaging of solitary metastases le metastasi cerebrali sono i tumori intracranici pi comuni nelladulto , con pi di 100.000 nuovi casi lanno diagnosticati negli stati uniti [ 1 ]  . 
lincidenza delle metastasi cerebrali inoltre in continuo aumento , non solo grazie alladozione di terapie combinate allavanguardia contro il tumore primitivo ed al decremento della mortalit , ma anche in rapporto alle nuove ed avanzate tecniche di neuroradiologia [ 2 , 3 ]  . 
le neoplasie con maggiore tendenza alla localizzazione a distanza nel compartimento endocranico sono , in ordine decrescente , i carcinomi del polmone , i carcinomi della mammella , il melanoma , i carcinomi del colon - retto e quelli del tratto urogenitale [ 57 ]  . 
alla diagnosi , il 50% delle metastasi cerebrali sono uniche e le localizzazioni sono in ordine decrescente : emisferica cerebrale ( 60% ) , cerebellare ( 30% ) e troncoencefalica ( 10% ) [ 10 ]  . 
 quando uniche ed in assenza di un tumore primitivo noto , le metastasi cerebrali entrano in diagnosi differenziale con un ampio ventaglio di patologie , pi frequentemente con gliomi di alto grado , linfomi cerebrali ed ascessi , meno frequentemente con lesioni infiammatorie / demielinizzanti e lesioni ischemiche . 
grazie alla sua multiparametricit , multiplanariet , allelevata risoluzione di contrasto , alla scarsa invasivit ed allutilizzo di energia non - ionizzante , la risonanza magnetica ( rm ) la metodica di elezione nello studio delle lesioni espansive encefaliche in generale e nello specifico delle metastasi . 
per incrementare la specificit della rm si sono affermate sequenze non morfologiche , quali la diffusione ( dwi ) , la perfusione ( pwi ) e la spettroscopia ( mrs ) , che fornendo informazioni cito - strutturali , emodinamiche e metaboliche [ 1115 ] sono di supporto alla diagnosi differenziale . 
questo lavoro , basato su una casistica personale di 59 metastasi solitarie istologicamente provate , ha lo scopo di illustrare le caratteristiche rm morfologiche e non morfologiche delle metastasi solitarie . 
in questo ambito abbiamo verificato lutilit dei parametri suggeriti dalla radiol med ( 2012 ) 117 : 12251241 1227 to the brain this context , we verified the usefulness of the parameters reported in the literature for the differential diagnosis of solitary brain neoplasms by comparing them with those seen in our series in order to suggest which nonmorphological technique and findings can best support the criteria of conventional semiotics . 
 letteratura per la diagnosi differenziale delle neoplasie cerebrali solitarie , confrontandoli con quelli provenienti dal nostro campione per arrivare a proporre quale metodica non morfologica e quali reperti siano di maggior supporto ai criteri della semeiotica tradizionale . materials and methods between march 2005 and october 2010 , 153 patients ( age range 1292 years ) with a definitive diagnosis of brain metastasis underwent mr imaging at our hospital . 
of these , we selected 59 patients ( age range 1287 years ; male 31 , female 28 ) on the basis of the following criteria : histologically proven diagnosis of brain metastasis ( biopsy , surgery or autopsy ) , evidence on all mr studies of a single intraaxial brain lesion and no previous treatment with radiotherapy , chemotherapy or surgery of either the brain metastasis or the primary tumour . 
 fifty - one patients also underwent a dwi study , 31 a pwi study and 22 mr spectroscopy ; 35 patients were also imaged with noncontrast - enhanced computed tomography ( ct )  . 
 study protocol all mr studies were carried out on 1.5 - t scanners ( signa excite 2 echospeed general electric medical systems ) with an 8 - channel dedicated coil . 
in all cases , the acquisition protocol included t2and t1 - weighted multiplanar fast spinecho ( fse ) , fluid - attenuated inversion recovery ( flair ) and gradient - echo ( gre ) sequences ( slice thickness 34 mm ; gap , 0.30.4 mm ) , followed by three t1 - weighted multiplanar fse sequences after administration of a single bolus of paramagnetic contrast mediuin some cases , suppression of the fat signal in the t2and / or t1 - weighted sequence was applied ; additional sequences were obtained in specific cases . 
sulla base dei seguenti criteri di inclusione abbiamo selezionato 59 pazienti ( et compresa tra 12 e 87 anni , maschi 31 e femmine 28 ) : diagnosi istologicamente provata ( bioptica , escissionale o autoptica ) di metastasi cerebrale , evidenza in tutti gli esami rm di ununica lesione cerebrale intrassiale , assenza di pregressi trattamenti con radioterapia , chemioterapia o chirurgia della lesione encefalica e del tumore primitivo . 
in 51 casi stato eseguito uno studio di diffusione , in 31 di perfusione ed in 22 di spettroscopia ; in 35 casi stato inoltre eseguito uno studio in tomografia computerizzata ( tc ) senza somministrazione di mezzo di contrasto . 
 protocollo di studio tutti gli esami rm sono stati eseguiti su apparecchi da 1 , 5 t ( signa excite 2 echospeed general electric medical systems ) con bobina dedicata ad 8 canali . 
in tutti gli esami il protocollo di acquisizione includeva sequenze multiplanari ( spessore 34 mm ; gap 0 , 30 , 4 mm ) fast spin echo ( fse ) t2e t1 - dipendenti , fast fluid - attenuated inversionrecovery ( flair ) e gradient echo ( gre ) , e dopo somministrazione endovenosa di singola dose di mezzo di contrasto paramagnetico 3 sequenze multiplanari fse t1 - dipendenti . 
 in alcuni casi stata applicata la saturazione del segnale proveniente dal tessuto adiposo nelle sequenze t2 e / o t1 - dipendenti ; sequenze aggiuntive sono state eseguite in casi specifici . 
per lo studio di diffusione stata utilizzata una sequenza echo - planar imaging ( epi ) gre acquisita sul piano assiale , tempo di ripetizione ( tr ) / tempo di eco ( te ) 8600 / 80 , 2 ms , campo di vista ( fov ) 28 cm , matrice 128128 , spessore di strato 4 mm , gap 0 , 4 mm , b value 0 / 1000 mm2 / s . 
in all cases , a few minutes before the dynamic phase , patients received a prebolus of 0.05 mmol / kg gadolinium to attenuate the t1 effects of bloodbrain barrier ( bbb ) disruption . 
the spectroscopy study consisted of sequences with an intermediate te of 144 , single - voxel technique , performed with pointresolved spectroscopy ( press ) probe - p sequence , tr / te 1 , 500 / 144 , 8 nex , fov 24 and voxel thickness 20 m evaluation of morphological sequences two authors in consensus ( sg , vl ) measured the maximum diameter of each lesion , assessed the presence of perilesional oedema and rated signal intensity and contrast enhancement ( ce )  . 
on the basis of these maps and the corresponding morphological images ( t2 - weighted and postcontrast t1 - weighted ) , three rois were positioned over the solid portion of each lesion showing reduced diffusivity , taking care not to include cystic , necrotic or haemorrhagic areas . 
the mean adc value of the lesion was normalised to the mean adc value in three same - sized rois placed over the contralateral normal - appearing white matter ( nawm )  . 
dwi signal intensity was assessed on the solid component showing contrast enhancement and classified as hypointense , isointense or hyperintense ( compared with the contralateral white matter )  . from the perfusion sequences , colour maps of the cerebral blood volume ( cbv ) were generated . 
on the basis of the simultaneous evaluation of the maps and corresponding morphological images ( t2 - weighted and postcontrast t1weighted ) , the solid areas of lesions showing higher cbv values were sampled with three rois , taking care not to include vascular structures ( arterial or venous ) or choroid lizzando unagocannula 18 g . 
in tutti i casi la fase dinamica stata preceduta di pochi minuti dalla somministrazione di un prebolo di 0 , 05 mmol / kg di gadolinio per attenuare gli effetti t1 da alterazione della barriera ematoencefalica . 
lo studio di spettroscopia consisteva in sequenze con te intermedio di 144 , singolo voxel , effettuato con sequenza press probe - p , tr / te 1500 / 144 , 8 numero di eccitazioni ( nex ) , fov 24 , voxel thickness 20 m valutazione delle sequenze morfologiche due autori in consensus ( sg , vl ) hanno misurato il diametro massimo di ogni lesione , valutato la presenza di edema perilesionale e classificato lintensit di segnale ed il contrast enhancement ( ce )  . 
per gli studi di diffusione e perfusione sono state utilizzate regioni di interesse ( roi ) ovalari di 3070 mm2 , tranne nel caso della lesione di pi piccole dimensioni ( diametro massimo 5 mm ) per la quale si utilizzata una roi di 20 mm2 ( diametro massimo 4 , 8 mm ) disegnata a mano . dalle sequenze dwi sono state generate mappe colorimetriche del coefficiente di diffusione apparente ( adc )  . 
 sulla base di tali mappe e delle corrispettive immagini morfologiche ( t2 - dipendenti e t1 - dipendenti dopo contrasto ) sono state posizionate tre roi nella porzione solida di ogni lesione che mostrava minore diffusivit , evitando accuratamente di includere aree cistiche , necrotiche o emorragiche . 
 il valore di adc medio della lesione stato normalizzato con il valore adc medio proveniente da tre roi di analoghe dimensioni posizionate nella sostanza bianca controlaterale apparentemente normale ( sban )  . 
lintensit del segnale dwi stata valutata sulla componente solida che mostrava impregnazione dopo mdc e classificata come ipointensa , isointensa ed iperintensa ( rispetto alla sostanza bianca controlaterale )  . per le sequenze di perfusione sono state prodotte mappe colorimetriche del cerebral blood volume ( cbv )  . 
sulla base della valutazione contemporanea delle mappe e delle corrispettive immagini morfologiche ( t2 - dipendenti e t1 - dipendenti dopo contrasto ) , sono state campionate con tre roi le aree solide delle lesioni che mostravano i valori maggiori di cbv , facendo attenzione a non includere strutture vascolari ( arteriose o venose ) e plessi corioidei . 
the values of relative cbv ( rcbv ) of the lesion and perilesional oedema were obtained by normalising the mean of the cbv values ( of the lesion and of the vasogenic oedema ) with those of the contralateral nawm . 
to normalise adc and cbv values of subtentorial lesions , the rois were placed over the nawm of the contralateral middle cerebellar pedicle for cerebellar metastases and over the nawm of the pons for pontine metastases . 
 the voxel of interest for the spectroscopic study was placed on the solid component of the lesion , taking care to avoid haemorrhagic areas , although it was not always possible to avoid the vasogenic oedema . 
data from the spectroscopy study were visualised as spectra , and the peak values of the following metabolites were calculated : n - acetylaspartate ( naa ) , choline ( cho ) , creatine ( cr ) , lipids ( lip ) and naa / cr and cho / cr ratios normalised to the contralateral normal parenchyma . 
no exclusive samplings of the perilesional oedema were carried out . statistical analysis for quantitative variables , we calculated the mean , standard deviation ( sd ) and minimum and maximum values ; for qualitative variables , we calculated absolute and relative frequencies . 
lesions were subdivided according to tumour of origin ( five groups : lung , gastrointestinal , breast , genitourinary , other ) , and histological type ( two groups : metastasis from adenocarcinoma and from nonadenocarcinoma )  . 
differences between quantitative variables were tested with the students t test for unpaired data in the case of comparisons of two groups and with analysis of variance ( anova ) when the comparison involved more than two groups . 
the most common histological type was adenocarcinoma , with 33 lesions , originating from the lung ( n = 17 ) , breast ( n = 8 ) , colon and ovary ( n = 3 )  . 
per normalizzare i valori di adc e di cbv delle lesioni sottotentoriali le roi sono state posizionate sulla sban del peduncolo cerebellare medio controlaterale e sulla sban pontina , rispettivamente per le metastasi cerebellari e per lunica metastasi pontina . 
 il voxel per lo studio spettroscopico stato posizionato sulla componente solida della lesione , evitando principalmente le aree emorragiche , ma non stato sempre possibile evitare di includere ledema vasogenico . 
i dati degli studi di spettroscopia sono stati visualizzati sotto forma di spettri , e sono stati calcolati i valori dei picchi dei seguenti metaboliti : n - acetil - aspartato ( naa ) , colina ( cho ) , creatina ( cr ) , lipidi ( lip ) ed i rapporti tra naa / cr , cho / cr , normalizzati con il controlato . 
non sono stati effettuati campionamenti esclusivi sulledema perilesionale . analisi statistica per le variabili quantitative sono state calcolate le medie , le deviazioni standard ( ds ) ed i valori di minimo e massimo ; per le variabili qualitative le frequenze , assolute e relative . 
abbiamo suddiviso le lesioni in base al tumore di origine ( 5 gruppi : polmone , gastrointestinale , mammella , genito - urinario , altro ) , ed in base allistotipo ( due gruppi : metastasi da adenocarcinoma e da non adenocarcinoma )  . 
le differenze tra le variabili quantitative sono state testate tramite il test t di student per dati non appaiati , ove fossero confrontati 2 gruppi , tramite il test di anova ove i gruppi da paragonare fossero pi di 2 . 
i tumori meno frequenti ( 1 solo caso per ciascuno ) : prostatico , gastrico , esofageo , endometriale , della ghiandola parotide , melanoma , delle vie biliari e neuroblastoma . 
listotipo pi frequente risultato ladenocarcinoma con 33 lesioni , di cui le pi frequenti ad origine dal tumore del polmone ( 17 ) , della mammella ( 8 ) , del colon e dellovaio ( 3 )  . 
delle 26 metastasi con istotipo non adenocarcinoma 17 sono risultate ad origine da tumore del polmone ( 8 da carcinoma a piccole cellule , 5 da carcinoma squamocellulare , 2 da carcinoma a grandi cellule e 2 da carcinoide )  . rm morfologica delle 59 lesioni 48 erano sovratentoriali e 11 sottotentoriali , con le seguenti localizzazioni in ordine decrescente : 1230 radiol med ( 2012 ) 117 : 12251241 other than adenocarcinoma , 17 originated from lung cancers ( eight from small cell carcinoma , five from squamous cell carcinoma , two from large cell carcinoma and two from carcinoid tumour )  . morphological mr imaging of the 59 lesions , 48 were supratentorial and 11 were subtentorial . 
lesions ranged in size from 5 mm to 65 mtwenty - two metastases were completely solid , 37 had fluid a component ( cystic or necrotic ) and 19 had blood in various stages of degradation ( from extracellular methaemoglobin to haemosiderin )  . 
most metastases appeared isohypointense on t1 - weighted images ( 36 / 59 ) , whereas greater variability of appearance was seen on t2 - weighted images : hypointense in 20 , hyperintense in 19 , mixed in 12 and isointense in eight . 
after administration of contrast material , all lesions showed contrast enhancement , although with different enhancement patterns : prevalently marginal ( n = 23 ) , heterogeneous but evident ( n = 20 ) , nodular ( n = 15 ) and poor ( n = 1 )  . 
 perfusion - weighted imaging all lesions exhibited greater perfusion than the contralateral nel lobo frontale ( 21 ) , nel lobo parietale ( 12 ) , nel cervelletto ( 10 , di cui 9 emisferiche ed una vermiana ) , nel lobo occipitale ( 9 ) , nel lobo temporale ( 6 ) e nel ponte ( 1 )  . 
le lesioni avevano dimensioni comprese tra 5 e 65 mventidue metastasi erano completamente solide , 37 presentavano componenti fluide ( cistiche o necrotiche ) e 19 materia le ematico in diversi stadi ( da metaemoglobina extra - cellulare ad emosiderina )  . 
la maggior parte delle metastasi apparsa iso - ipointensa nelle immagini t1 - dipendenti ( 36 / 59 ) , mentre pi variabile risultato il segnale t2 : ipointenso in 20 lesioni , iperintenso in 19 , misto in 12 ed isointenso in 8 . 
dopo la somministrazione del mdc tutte le lesioni hanno dimostrato contrast enhancement ma con diversi pattern : prevalentemente marginale ( 23 lesioni ) , disomogeneo ma evidente ( 20 lesioni ) , nodulare ( 15 lesioni ) , scarso ( 1 lesione )  . 
le metastasi da adenocarcinoma hanno presentato valori di adc pi bassi rispetto a quelle da altri istotipi tumorali ( rispettivamente 1 , 030 , 410 - 3 e 1 , 100 , 210 - 3 )  . 
le metastasi che pi frequentemente hanno dimostrato valori di diffusivit ristretti erano tutte a partenza dal tumore del polmone ( adc min 0 , 000587 mm2 / s ; mediads 0 , 000980 , 00032 mm2 / s )  . 
 rm di perfusione tutte le lesioni hanno dimostrato maggiore perfusione rispetto alla sostanza bianca controlaterale con valori di rcbv , analizzati per tipologia tumorale , compresi tra 1 , 59 e 8 , 68 , con un valore medio di 3 , 301 , 59 . 
1a - f solitary metastatic disease in the right parietal lobe ( lung adenocarcinoma ) : t2 - weighted images demonstrate a small solid mass surrounded by conspicuous perilesional oedema in the right parietal lobe ( a )  . 
the shape of the pathological curve ( * ) demonstrates lower values at the end of the first passage ( large arrow ) of contrast medium compared with those at baseline ( small arrow ) ; the shape of the curve of the normal white matter ( ) appears regular . 
le immagini t2 - dipendenti mostrano una lesione solida ipointensa , circondata da cospicuo edema perilesionale , localizzata nel lobo parietale di destra ( a ) , caratterizzata da enhancement nodulare / omogeneo nelle immagini t1 - dipendenti dopo somministrazione di mdc ( b , c )  . 
landamento della curva patologica ( * ) mostra che i valori al termine del primo passaggio ( freccia grande ) sono nettamente inferiori rispetto alla baseline iniziale ( freccia piccola ) ; regolare il recupero della curva della sostanza bianca controlaterale ( )  . 
moreover , metastases from pulmonary microcytoma showed strongly fluctuating rcbv values , from extremely low ( 1.71 ) to high polmonare hanno dimostrato valori di rcbv oscillanti tra estremamente bassi ( 1 , 71 ) ed elevati ( 7 , 88 )  . 
in tutte le lesioni i valori di rcbv calcolati nelledema perilesionale ( parenchima alterato esterno al margine di impregnazione ) sono risultati inferiori a quelli della sostanza bianca controlaterale apparentemente normale ( valore medio 0 , 420 , 15 )  . 
2a - f solitary metastatic disease in the left cerebellar hemisphere ( lung adenocarcinoma ) : t2 - weighted ( a ) and t1 - weighted images after contrast administration ( b ) show a necrotic mass with enhancing rim in the left cerebellar hemisphere . 
the solid components appear isointense on dwi ( c ) , with increased adc values ( d ) ; pwi demonstrates high rcbv values ( e ) with incomplete recovery of the dynamic curve ( f )  . 
le immagini t2 - dipendenti ( a ) e t1 - dipendenti dopo somministrazione di mdc ( b ) mostrano nellemisfero cerebellare di sinistra una lesione eterogenea con componente necrotica ed enhancement marginale . 
 le componenti solide appaiono isointense in dwi ( c ) con valori di coefficiente di diffusione apparente ( adc ) superiori alla sostanza bianca controlaterale ( d ) e mostrano elevati livelli di rcbv ( e ) e scarso recupero della curva ( f ) allo studio perfusionale . radiol med ( 2012 ) 117 : 12251241 1233 fig . 
il grafico a dispersione mostra una distribuzione omogenea dei valori di adc nei pazienti con tumori primitivi , ad eccezione dei valori outlier di 3 pazienti , che si osservano nel grafico al di sopra del valore adc = 1 , 510 - 3 . 
5 comparison of mean percentage of signal intensity recovery among the different types of primary cancer : the scatter plot shows that almost 90% of the values are below the cutoff value of 75% . 
il grafico a dispersione mostra che in quasi il 90% dei casi la percentuale di recupero della curva media si assestata al di sotto del valore di cut - off prestabilito del 75% . 
supratentorial metastases had mean signal recovery values ranging from 0.30 ( metastases from lung adenocarcinoma ) to 0.79 ( metastases from unknown primary ) ; minimum values ranged from 0.13 ( metastases from poorly differentiated carcinoma of unknown origin ) to 0.60 ( metastases from poorly differentiated lung cancer )  . 
in subtentorial metastases , mean signal recovery values ranged from 0.28 ( metastasis from lung adenocarcinoma ) to 0.74 ( metastasis from lung adenocarcinoma ) ; minimum signal recovery values varied between 0.26 ( metastasis from lung adenocarcinoma ) and 0.70 ( metastasis from lung adenocarcinoma )  . 
 il pi alto valore medio di recupero ( 78 , 2% , ds 0 , 012 ) risultato in due metastasi da carcinoma del polmone scarsamente differenziato ed in una da carcinoma di origine ignota ; il campionamento con roi singole di queste lesioni ha individuato aree con percentuali di recupero nettamente minori ( 66 , 8% , ds 0 , 03 )  . 
nellambito delle metastasi sovratentoriali i valori medi di rc sono risultati variabili da 0 , 30 ( metastasi da adenocarcinoma polmonare ) a 0 , 79 ( metastasi da tumore ignoto ) ; quelli minimi da 0 , 13 ( metastasi da carcinoma scarsamente differenziato di origine ignota ) a 0 , 60 ( metastasi da carcinoma scarsamente differenziato di origine polmonare )  . 
nelle metastasi sottotentoriali i valori medi di rc sono risultati variabili da 0 , 28 ( metastasi da adenocarcinoma polmonare ) a 0 , 74 ( metastasi da adenocarcinoma polmonare ) ; il recupero minimo presentava valori variabili da 0 , 26 ( metastasi da adenocarcinoma polmonare ) a 0 , 70 ( metastasi da adenocarcinoma polmonare )  . 
 si possono presentare in diversi stadi del tumore primitivo , anche come prima manifestazione sintomatologica e di imaging o addirittura possono rappresentare lunica manifestazione della presenza di una neoplasia occulta [ 17 ]  . 
6a - c solitary metastatic lesion in the left occipital lobe ( breast adenocarcinoma ) : the left occipital lesion exhibits inhomogeneous hypointensity on t2weighted imaging ( a ) owing to a prominent haemorrhagic component . 
la lesione occipitale sinistra presenta segnale disomogeneo nelle immagini t2 - dipendenti ( a ) a causa della vasta componente emorragica ipointensa nelle immagini t2 * ( b ) che determina artefatti nello studio di perfusione ( area nera in c ) e non permette il corretto campionamento . 
they may present at different stages of the primary tumour , including as a first clinical or imaging manifestation or even as the only manifestation of an occult primary tumour [ 17 ]  . 
 metastases elude precise characterisation with mr imaging because of the wide variety of microand macroscopic features connected to the histological characteristics of the primary tumour , speed of growth and previous treatments . 
the most challenging situation is when a single expansile brain lesion is found , which enters the differential diagnosis with primary brain tumours ( high - grade gliomas ) , lymphomas ; less frequently with abscesses , cavernomas and inflammatory / demyelinating lesions ; and , rarely , with ischaemic lesions . 
evaluation of a solitary intra - axial lesion requires a semiological analysis that must take into account the characteristics of the signal in each sequence ( t2 , t1 , t2 * ) , contrast enhancement and the interrelation of these data . 
the findings in our series confirm the many possible mr presentations of solitary metastases and revealed no specific signal and enhancement features predictive of the metastatic nature of the lesion . 
as reported by previous authors and consistent with the mr presentation of brain tumours in general [ 18 ] , the low signal intensity of metastases in t2 - weighted images may be related to the presence of paramagnetic material such caratteristiche microe macroscopiche , che derivano dalle caratteristiche istologiche del tumore primitivo , dalla rapidit di crescita e dai trattamenti precedenti . 
in assenza di queste condizioni tipiche aumenta il grado di difficolt della diagnosi , che diviene massimo in presenza di una singola lesione espansiva encefalica , che entra in diagnosi differenziale principalmente con i tumori primitivi encefalici ( gliomi di alto grado ) , con i linfomi , meno frequentemente con lesioni ascessuali , cavernomi e lesioni infiammatorie / demielinizzanti e pi raramente con le lesioni ischemiche . 
la valutazione di una lesione intrassiale necessita di unanalisi semeiologica che deve considerare le caratteristiche di segnale in ogni sequenza ( t2 , t1 , t2 * ) , limpregnazione dopo somministrazione del mdc , e lintegrazione tra loro di questi dati . 
nella nostra casistica si sono confermate le molteplici possibilit di presentazione rm delle metastasi solitarie e non si sono individuate caratteristiche di segnale e di impregnazione contrastografica specifiche ed indicative della natura secondaria . 
come gi riportato in letteratura , ed in accordo con le modalit di presentazione rm dei tumori endocranici in generale [ 18 ] , il basso segnale delle metastasi nelle immagini t2 - dipendenti pu essere determinato da materiale paramagnetico come la melanina , mucina o metaemoglobina intracellulare [ 18 , 19 ]  . 
una relativa iperintensit di segnale nelle immagini t1 - dipendenti sostenuta da quelle componenti che determinano accorciamento del t1 , quali la melanina , la mucina , la metaemoglobina intrao extracellulare e lelevato contenuto di proteine e calcio . 
il basso segnale nelle immagini t2 * pi spesso il 1236 radiol med ( 2012 ) 117 : 12251241 as melanin , mucin or intracellular methaemoglobin [ 18 , 19 ]  . 
 the relatively high signal intensity in t1 - weighted images is related to components responsible for t1 shortening , such as melanin , mucin , intraor extracellular methaemoglobin and high protein and calcium content . 
a low signal intensity in t2 * images is more often a reflection of paramagnetic substances such as haemosiderin or calcium , the definition of which can only be provided by ct . 
 this lack of typical morphological features means that mr imaging is not specific in the diagnosis of solitary metastases and that morphological sequences ( preand postcontrast ) in general cannot be considered sufficient for complete characterisation of brain lesions . 
some authors have provokingly gone as far as to define as obsolete any mr study of brain lesions that does not include nonmorphological sequences , such as dwi and pwi and spectroscopy , with a qualitative , semiquantitative and quantitative approach [ 20 ]  . 
there is no doubt that dwi , pwi and spectroscopy have become part of the routine protocols for studying brain lesions , but their real diagnostic contribution is obtained when the sequences are state of the art , the parameters are correctly sampled and the values interpreted in the light of data reported in the literature . dwi is based on the mobility of water molecules in the extracellular space . 
in our series , mean adc values were extremely variable , without any statistically significant differences between metastases from the different organs / systems or between the two main histological types ( adenocarcinoma and nonadenocarcinoma )  . 
however , we can speculate that adc values of the solid component of metastases correlate with cellularity [ 21 ] and that the lower adc values of adenocarcinomas compared with nonadenocarcinomas are due to the greater differentiation of adenocarcinomas . 
even though some authors claim that diffusion is useful in the differential diagnosis between metastasis and high - grade glioma [ 23 ] , the majority of investigators have not reported a significant and reproducible cutoff value . 
anche limpregnazione contrastografica non ha dimostrato pattern specifici per le metastasi , n sono state trovate correlazioni tra il tumore primitivo ed il tipo di enhancement della lesione secondaria encefalica . 
 non essendoci dunque caratteristiche morfologiche tipiche la rm non pu considerarsi specifica nella diagnosi delle metastasi solitarie , ed in generale le sequenze morfologiche ( prima e dopo somministrazione di mdc ) non sono pi ritenute sufficienti per la completa caratterizzazione delle lesioni encefaliche . 
recentemente alcuni autori si sono spinti , in senso provocatorio , a definire obsoleto uno studio rm mirato alla valutazione di neoformazioni encefaliche che non sia integrato da sequenze non morfologiche quali la diffusione , la perfusione e la spettroscopia , utilizzando un approccio qualitativo , semi - quantitativo e quantitativo [ 20 ]  . 
indubbio che le sequenze di diffusione , perfusione e spettroscopia siano entrate a far parte dei protocolli di studio delle lesioni cerebrali nella pratica quotidiana , ma il loro reale apporto diagnostico si ottiene quando le sequenze vengono acquisite allo stato dellarte , i parametri campionati correttamente ed i valori interpretati in rapporto ai dati provenienti dalla letteratura . la diffusione si basa sulla mobilit delle molecole di acqua nello spazio extra - cellulare . 
stato dimostrato che la diffusivit inversamente proporzionale alla cellularit dei tumori encefalici , e nel caso specifico delle metastasi diversi autori hanno cercato di correlare i valori di adc con il tumore di origine e con listotipo della metastasi [ 21 ]  . 
nella nostra casistica i valori medi di adc sono risultati estremamente variabili , senza differenze statisticamente significative tra le metastasi ad origine dai diversi organi / apparati , n tra i due istotipi principali ( adenocarcinoma e non - adenocarcinoma )  . 
tuttavia possiamo speculare che i valori di adc della componente solida delle metastasi siano correlati con la cellularit [ 21 ] , e che i valori di adc , pi bassi nel gruppo degli adenocarcinomi rispetto al gruppo degli altri istotipi , siano dovuti al maggior grado di differenziazione del gruppo adenocarcinomi . 
per quanto alcuni autori sostengano che la diffusione sia utile nella diagnosi differenziale tra metastasi e tumore gliale di alto grado [ 23 ] , la maggior parte degli autori non riporta un cut - off significativo e riproducibile , ed in accordo con rizzo et al . 
 [ 24 ] anche i dati della nostra casistica si sovrappongono a quelli riportati dalla letteratura , confermando che da sola la diffusione non permette una differenziazione tra tumore primitivo cerebrale e lesione secondaria . 
i linfomi cerebrali primitivi dimostrano una diffusivit ridotta rispetto ai tumori gliali di alto grado , ma non sono mai stati definiti valori soglia di adc per la differenziazione tra linfomi e metastasi . 
la dwi trova la sua utilit maggiore nella radiol med ( 2012 ) 117 : 12251241 1237 brain lymphomas exhibit reduced diffusivity compared with high - grade gliomas , but to date , no threshold adc values have been defined that allow discrimination between lymphomas and metastases . 
dwi is most useful in the differential diagnosis with brain abscesses , in which adc values are markedly and significantly reduced ( 0.380.7710 - 3 mm / s ) compared with gliomas and metastases [ 25 ]  . 
 pwi with the dsc technique analyses the first pass of a bolus of a nondiffusible contrast agent ( gadolinium ) through the cerebral vascular bed to which gadolinium remains confined , as it does not cross the bbb by acquiring a repeated series of axial images . 
mathematical algorithms are used to generate different colour - coded maps ( cbv , cerebral blood flow , mean transit time ) required for quantitative and panoramic evaluation of lesion and brain perfusion . 
 the maps must then be used to guide lesion sampling by means of multiple , geometric or freehand - drawn rois , such that some authors call them road maps [ 26 ]  . 
in pwi with dsc , cbv that is , the quantity of blood ( millilitres ) passing through a given tissue volume ( ml / 100 g ) is indicated as the most important parameter for demonstrating / measuring tumour neoangiogenesis , which occurs both in metastases and in high - grade gliomas . 
more controversial is the application of the parameter of lesion permeability , which is more reliably determined with dynamic contrast - enhanced ( dce ) perfusion imaging , and was thus not considered in our work . 
 neoangiogenesis is characterised by an abnormal proliferation of new vessels within the tumour vascular bed , reflected in a corresponding increase in cbv , with the newly formed vessels lacking the bbb and thus leading to increased microvascular permeability . 
the actual value of rcbv could be altered by the presence of a disrupted / absent bbb , allowing leakage of contrast material into the extravascular space , where the t1 , t2 and t2 * effect will be simultaneously present . 
to overcome this problem , which always occurs when the bbb is absent , we administered a predose of contrast medium ( 0.05 mmol / kg ) approximately 5 min before the perfusion study [ 2729 ]  . 
on the basis of the most recent evidence , we used as perfusion parameters the rcbv and the percentage of signal recovery ( psr ) , with sampling not only of the lesion but also of the perilesional areas of abnormal signal beyond the margins of contrast enhancement . 
the rcbv and psr values in our series are in line with those reported in the literature and confirm the reproducibility of pwi with the dsc technique when performed with accurate acquisition and processing / sampling methods . 
the ( nonsignificant ) differences in rcbv and psr between supraand subtentorial lesions diagnosi differenziale con gli ascessi cerebrali , che mostrano valori di adc marcatamente e significativamente ridotti ( 0 , 380 , 7710 - 3 mm / s ) rispetto a quelli dei tumori gliali e delle metastasi [ 25 ]  . 
 la perfusione con tecnica dsc analizza il primo passaggio di un bolo di un mdc non diffusibile ( gadolinio ) attraverso il letto vascolare cerebrale , dove il gadolinio rimane confinato poich non attraversa la barriera emato - encefalica ( bee ) , mediante lacquisizione di una serie ripetuta di immagini assiali . 
mediante algoritmi matematici si generano diverse mappe parametriche colorimetriche ( volume ematico cerebrale , flusso ematico cerebrale , tempo medio di transito ) , necessarie alla valutazione qualitativa e panoramica della perfusione della lesione e dellencefalo . 
le mappe devono essere utilizzate per guidare il successivo campionamento della lesione con roi multiple geometriche o disegnate a mano libera , tanto che alcuni autori le chiamano road map [ 26 ]  . 
nella perfusione con tecnica dsc il volume ematico cerebrale , ovvero la quantit di sangue ( ml ) che attraversa un certo volume di tessuto ( ml / 100 gr ) , viene indicato come il parametro perfusionale pi importante per dimostrare / misurare la neoangiogenesi tumorale , che si verifica sia nelle metastasi che nei gliomi ad alto grado . 
pi discussa lapplicazione del parametro permeabilit della lesione , la cui misurazione risulta pi attendibile con la metodica perfusionale dynamic contrastenhanced ( dce ) , e che non stata quindi inclusa in questo lavoro . 
la neoangiogenesi caratterizzata da abnorme proliferazione di nuovi vasi allinterno del letto vascolare della neoplasia , che si traduce in un corrispettivo aumento del cbv , e da vasi neoformati con bee disfunzionante , che comporta un aumento della permeabilit microvascolare . 
il reale valore del rcbv potrebbe risultare alterato in presenza di una bee danneggiata / assente che consenta lo stravaso di mdc nello spazio extravascolare , dove risulteranno quindi simultaneamente presenti leffetto t1 , t2 e t2 *  . 
 per ovviare a tale problematica , sempre presente in caso di metastasi dove la bee assente , abbiamo somministrato una pre - dose di mdc ( 0 , 05 mmol / kg ) circa 5 minuti prima dellacquisizione perfusionale [ 2729 ]  . 
sulla base della pi recente letteratura abbiamo utilizzato come parametri perfusionali il rcbv e la percentuale di rc , campionando non solo la lesione ma anche le aree di alterato segnale perilesionali , oltre i margini dellimpregnazione . 
i valori di rcbv e di rc del nostro campione rispecchiano quelli riportati in letteratura e confermano la riproducibilit della perfusione dsc quando viene applicata una corretta metodologia di acquisizione e rielaborazione / campionamento . 
tutte le metastasi hanno dimostrato valori di rcbv elevati e bassa percentuale di recupero della curva , ma non sono state riscontrate differenze statisticamente significative dei valori di rcbv e di rc tra i differenti tumori primitivi e tra il gruppo di adenocarcinomi ed il gruppo di non adenocarcinomi . 
 le differenze ( non statisticamente significative ) del rcbv e della percentuale di recupero della curva tra lesioni sovra e sottotentoriali sono probabilmente dovute alla diversa perfusione dei due compartimenti , sostenuta dallasse caro1238 radiol med ( 2012 ) 117 : 12251241 are probably due to the different perfusion of the two compartments , the anterior and middle circulation being supplied by the carotid axis and the posterior circulation by the vertebrobasilar axis ; however , these findings require further investigation on larger and more heterogeneous samples . 
metastases therefore have high rcbv , enabling differentiation from poorly perfused lesions such as abscesses ( mean rcbv 0.450.11 ) [ 30 ] , multiple sclerosis plaques ( mean rcbv 0.880.46 ) and low - grade gliomas ( mean rcbv 1.860.77 ) [ 31 ]  . 
in the differential diagnosis with more highly perfused lesions , such as high - grade gliomas and particularly with glioblastoma multiforme , rcbv values identified are not reported to be significant , being similar in metastases and high - grade gliomas . 
likewise , rcbv values detected in our sample ( mean values 3.301.59 ) confirm these data by showing a wide range of overlap with those previously reported for high - grade gliomas [ 32 , 33 ]  . 
 the psr was defined by those authors as the percentage of signal intensity that is recovered at the end of the first pass of contrast medium compared with baseline signal intensity . 
 [ 31 ] psr = 100% ( s1smin ) / ( s0smin ) where s1 is the signal intensity at the end of the first pass , s0 the baseline signal intensity and smin the minimum signal intensity reached during the first pass of contrast material . 
according to mangla et al . , when measuring the psr , a single sampling of the lesion is insufficient ; instead , one should calculate the minimum , mean and maximum psr to ensure a more reliable differential diagnosis between metastases , gliomas and cerebral lymphomas [ 34 ]  . 
the maximum psr appears to provide the highest sensitivity and specificity ( 82% and 93% , respectively ) in differentiating lymphomas from metastases and from gliomas ( cutoff > 114 ) , whereas the mean and minimum psr were found to be more useful for differentiating metastases from lymphomas and gliomas . 
cutoff values for mean psr of < 75% and < 67% showed high sensitivity ( 100% and 95% ) and specificity ( 83% and 85% ) ; a slight increase in specificity ( 89% ) was obtained with a minimum psr cutoff value of < 51% . 
in two lesions , in which mean psr values were > 75% , the minimum psr values were found to be markedly lower ( 66.8% ) ; this finding seems to imply that minimum psr has a greater diagnostic value than mean psr , but the observation is based on two cases only . 
 tideo per il circolo anteriore e medio , e da quello vertebrobasilare per il circolo posteriore , ma tali reperti necessitano di ulteriori studi con campioni pi ampi ed eterogenei . 
le metastasi hanno dunque valori di rcbv elevati che ne permettono la diagnosi differenziale con lesioni poco perfuse quali gli ascessi ( rcbv medio 0 , 450 , 11 ) [ 30 ] , le placche di sclerosi multipla ( rcbv medio 0 , 880 , 46 ) , ed i gliomi di basso grado ( rcbv medio 1 , 860 , 77 ) [ 31 ]  . 
nella diagnosi differenziale con lesioni maggiormente perfuse come i gliomi di alto grado , ed in particolar modo con il glioblastoma multiforme , i valori isolati di rcbv non sono riportati come significativi , poich simili nelle metastasi e nei gliomi di alto grado . 
anche i valori di rcbv provenienti dal nostro campione ( valore medio di 3 , 301 , 59 ) riproducono questo dato , evidenziando un ampio range di sovrapposizione con quelli riportati da diversi autori per i gliomi di alto grado [ 32 , 33 ]  . 
 [ 34 ] hanno dimostrato che la percentuale di recupero della curva della lesione un parametro perfusionale pi affidabile per differenziare i gliomi di alto grado , le metastasi ed linfomi cerebrali primitivi . 
 [ 31 ] come la percentuale dellintensit di segnale che viene riacquistata alla fine del primo passaggio del mdc rispetto allintensit di segnale prima dellarrivo del bolo di mdc ( baseline ) [ 31 , 34 ]  . 
 [ 31 ] : psr = 100% ( s1 - smin ) / ( s0 - smin ) dove per s1 si intende lintensit di segnale al termine del primo passaggio , s0 lintensit di segnale prima dellarrivo del bolo , smin lintensit di segnale minima a cui arriva la curva durante il primo passaggio . 
nel misurare il rc non bisogna fermarsi ad un singolo campionamento della lesione , ma si deve calcolare la percentuale di rc minima , media e massima per una pi affidabile diagnosi differenziale tra metastasi , gliomi e linfomi cerebrali . 
la percentuale di rc massima sembra infatti offrire la maggiore sensibilit e specificit ( rispettivamente 82% e 93% ) nel differenziare i linfomi dalle metastasi e dai gliomi ( cut - off > 114 ) , mentre le percentuali di rc media e minima sono risultate pi utili nel differenziare le metastasi dai linfomi e dai gliomi . 
cut - off della percentuale di rc media < 75% e < 67% dimostrano elevata sensibilit ( 100% e 95% ) e specificit ( 83% e 85% ) ; un lieve incremento della specificit ( 89% ) si ottiene con un cut - off della percentuale di rc minima < 51% . 
in due lesioni , in cui i valori medi di rc erano superiori al 75% , la valutazione dei valori minimi di rc risultata nettamente inferiore ( 66 , 8% ) ; questo dato sembrerebbe attribuire alla percentuale di recupero minimo un valore diagnostico maggiore rispetto alla percentuale di recupero medio , ma rimane unosservazione basata su due soli casi . 
 un apporto significativo nella differenziazione tra metaradiol med ( 2012 ) 117 : 12251241 1239 a significant contribution to the differentiation of metastases and high - grade gliomas may come from evaluating the rcbv of abnormal tissue surrounding the enhancing margins of the lesion . 
according to the majority of recent papers , perilesional rcbv values are lower in metastases than in the contralateral nawm ( reflecting simple oedema ) , but they are higher in high - grade gliomas ( due to margin invasion properties of gliomas )  . 
similarly , we found perilesional rcbv values that were lower than those of the contralateral nawm , consistent with the presence of plain vasogenic oedema due to increased permeability of the newly formed capillaries . 
the effect of vasogenic oedema on perfusion has been widely demonstrated , even by studies on preand postoperative meningiomas , in which the low rcbv values in vasogenic oedema returned to normal ( approximately 1 : 1 ratio with the contralateral nawm ) after tumour resection [ 36 ]  . 
we believe that the evaluation of perfusion should always include measurement of rcbv values in the parenchyma surrounding the enhancing area in addition to sampling the lesions rcbv . mr spectroscopy is a noninvasive technique that enables in vivo assessment of the relative concentration of certain metabolites , providing useful information for tissue characterisation . 
in order to increase the specificity of mr spectroscopy , above all in the differential diagnosis of neoplastic and nonneoplastic lesions , it is necessary to compare lesion values with those of the contralateral healthy tissue [ 20 ] and sample the abnormal perilesional area as well . 
despite the limitations deriving from the use of single - voxel spectroscopy and the small study population , the high cho / cr ratio ( 2.92.4 ) , the low naa / cr ratio ( 1.21.3 ) and the increase in lipids detected in our sample are consistent with the values commonly reported in the literature , both for metastases and for high - grade gliomas and lymphomas [ 15 ] , and are therefore not decisive for the differential diagnosis . 
numerous studies show statistically significant differences between cho / cr values in the brain parenchyma adjacent to the enhancing lesion margins , with significantly higher cho / cr ratios in glioblastoma multiforme than in metastases [ 39 ]  . 
a multivoxel stasi e gliomi di alto grado pu derivare dalla valutazione del rcbv del tessuto cerebrale alterato che circonda i margini di impregnazione della lesione ; i valori del rcbv perilesionale , secondo la maggior parte dei pi recenti contributi , sono inferiori alla sostanza bianca sana controlaterale nelle metastasi ( semplice edema ) mentre nei gliomi di alto grado risultano aumentati ( per linfiltrazione marginale caratteristica dei gliomi )  . 
anche i nostri dati mostrano nelle metastasi valori di rcbv perilesionale inferiori a quelli della sb normale controlaterale , in accordo con la presenza di semplice edema vasogenico da aumentata permeabilit dei capillari neoformati . 
leffetto delledema vasogenico sulla perfusione stato ampiamente dimostrato anche da studi su meningiomi pree post - operatori , dove i bassi valori del rcbv in corrispondenza delledema vasogenico tornavano verso la normalit ( ratio 1 : 1 circa con la sostanza bianca controlaterale ) dopo rimozione del tumore [ 36 ]  . 
nostra opinione che nella valutazione della perfusione si debba sempre andare al di l del semplice campionamento del rcbv della lesione e si debbano sempre valutare i valori di rcbv del parenchima adiacente limpregnazione contrastografica . 
i metaboliti considerati sono generalmente : naa , cho , cr , lip e lac , visualizzati sotto forma di spettro di frequenza , e dei quali vengono considerati sia il valore assoluto della concentrazione che il rapporto principalmente con la cr . 
per incrementare la specificit della mrs , soprattutto nella diagnosi differenziale tra lesioni neoplastiche e non - neoplastiche , necessario confrontare i valori della lesione con quelli del controllo sano [ 20 ] e campionare anche le alterazioni perilesionali . 
nonostante i limiti dellutilizzo della spettroscopia single voxel e dellesiguit del campione , lelevato rapporto cho / cr ( 2 , 92 , 4 ) , il ridotto rapporto naa / cr ( 1 , 21 , 3 ) e lincremento dei lipidi rilevati nel nostro campione rispecchiano i valori comunemente riportati dalla letteratura sia per le metastasi che per i gliomi di alto grado ed i linfomi [ 15 ] , e non risultano quindi dirimenti per la diagnosi differenziale . 
un numero crescente di lavori riporta differenze statisticamente significative tra i valori cho / cr nel parenchima encefalico adiacente i margini di enhancement delle lesioni , con rapporti cho / cr significativamente superiori nel glioblastoma multiforme rispetto alle metastasi [ 39 ]  . 
 anche con la spettroscopia risulta quindi sempre necessario il campionamento di pi aree intralesionali e peritumorali , ed pertanto consigliato uno studio multivoxel 1240 radiol med ( 2012 ) 117 : 12251241 study is thus recommended that , by allowing normalisation of values to the healthy contralateral parenchyma , could further increase the specificity of the method . a few important considerations should be made concerning the measurement methods . 
the greatest sampling problems in our series , for all nonmorphological imaging techniques , were related to the presence of haemorrhage ( in different stages of evolution ) and the resulting disturbance to the magnetic field , to which epi sequences are especially sensitive . 
in diffusion and perfusion studies , roi placement must be accurate and based on the maps ( colour - coded or grey - scale ) to ensure sampling of areas with reduced diffusivity and higher cbv values . 
it is also necessary to evaluate simultaneously the morphological images ( or their coregistration ) to make sure exclusively solid areas are sampled , with the exclusion of vascular structures , haemorrhagic or cystic areas that may affect measurement reliability . 
 che , consentendo anche la normalizzazione dei valori con il controlato sano , potrebbe incrementare ulteriormente la specificit della metodica . poche ma importanti considerazioni vanno fatte sulle modalit di misurazione . 
nella nostra casistica i maggiori problemi di campionamento , per tutte le metodiche non morfologiche , sono risultati dalla presenza di emorragia ( in diverse fasi di evoluzione ) e dalle conseguenti perturbazioni del campo magnetico a cui sono particolarmente sensibili le sequenze epi . 
nella valutazione della diffusione e della perfusione , il posizionamento delle roi deve essere accurato e si deve basare sulle mappe ( colorimetriche o in gradazioni di grigio ) affinch siano campionate le aree con diffusivit ridotta e con valori di cbv pi elevati . 
inoltre necessaria la contemporanea valutazione delle immagini morfologiche ( o la loro co - registrazione ) per campionare esclusivamente le aree solide ed escludere strutture vascolari , aree emorragiche o cistiche che possono rendere non attendibili le misurazioni . 
 conclusions in patients with a known primary tumour and / or multiple brain lesions , the mr diagnosis of brain metastasis is straightforward ; when the primary tumour is unknown and the brain lesion is solitary , diagnostic accuracy is lower due to the lack of a typical mr finding or pattern . 
although nonmorphological techniques allow a cytoarchitectural , haemodynamic and metabolic evaluation of metastases , the patterns and values of the various diffusion , perfusion and spectroscopy parameters are not decisive for a firm diagnosis . 
on pwi , a low psr in the lesion and a lower rcbv in the peritumoural area than in the nawm proved to be the most consistent findings in our sample of solitary metastases , with less overlap than reported in the literature for other brain lesions commonly considered in the differential diagnosis ( high - grade glioma and primary lymphoma )  . 
pwi with the dsc technique therefore appears to be the nonmorphological mr technique that offers the most significant contribution to the diagnosis of brain metastases . conclusioni in pazienti con tumore primitivo noto e / o con lesioni encefaliche multiple , la diagnosi di metastasi cerebrali con la rm agevole ; in assenza di un tumore primitivo noto e di fronte ad una lesione unica , invece , laccuratezza diagnostica inferiore , per la mancanza di un aspetto / reperto rm tipico . 
sebbene le metodiche non morfologiche permettano la valutazione citoarchitetturale , emodinamica e metabolica delle metastasi , il comportamento ed i valori dei diversi parametri di diffusione , perfusione e spettroscopia non risultano dirimenti . 
nello studio perfusionale una bassa percentuale di recupero della curva nella lesione ed un volume ematico cerebrale relativo dellarea peritumorale inferiore a quello della sostanza bianca non alterata , sono risultati i parametri pi costanti nella nostra popolazione di metastasi solitarie , con valori meno sovrapponibili a quelli riportati in letteratura per le altre lesioni encefaliche che pi frequentemente entrano in diagnosi differenziale ( glioma di alto grado e linfoma cerebrale primitivo )  . 
racca3 1istituto di radiologia , universit di torino , facolt san luigi gonzaga , regione gonzole 10 , 10043 orbassano torino , italy 2istituto di radiologia diagnostica e interventistica , universit di torino , via genova 3 , 10126 torino , italy 3sscvd colo - rectal cancer unit , medical oncology 1 , aou san giovanni battista , c.so bramante 88 , 10126 torino , italy correspondence to : a . 
the following predictors were analysed in the remaining 248 : synchronous / metachronous metastases , single / multiple metastases , diameter of largest metastasis and absence / presence of extrahepatic metastases . 
in light of our long - term results obtained with commonly used equipment , small lesion size ( diameter of largest lesion 3 or 2.5 cm ) proved to be the most favourable prognostic factor for survival in patients riassunto obiettivo . 
quattordici sono stati persi al follow - up ; in 248 sono stati analizzati i seguenti predittori : metastasi sincrone / metacrone , metastasi unica / multiple , diametro della metastasi principale , assenza / presenza di metastasi extraepatiche . 
alla luce dei nostri risultati a lungo termine , ottenuti con le apparecchiature comunemente utilizzate negli ultimi anni , le piccole dimensioni ( diametro della lesione principale 3 o 2 , 5 cm ) si confermano il fattore prognostico pi favorevole per la sopravvivenza dei pazienti con metastasi epatiche da crc sottoposti a rfa . 
in the presence of extrahepatic metastases , rfa has less impact on survival , even though it is potentially useful in patients at a higher risk of death due to hepatic rather than extrahepatic metastases . questa conclusione molto probabilmente riconducibile alla possibilit di unablazione radicale e induce a prospettare lutilit di apparecchiature in grado di aumentare il volume di ablazione . 
la rfa in presenza di metastasi extraepatiche meno efficace in termini di sopravvivenza , ma potenzialmente utile nei pazienti a minor rischio di decesso per le metastasi extra - epatiche rispetto a quelle epatiche . keywords colorectal cancer liver metastases radiofrequency thermal ablation survival interventional oncology parole chiave carcinoma colorettale metastasi epatiche termoablazione con radiofrequenze sopravvivenza oncologia interventistica introduction introduzione worldwide , at least one million new cases of colorectal cancer ( crc ) are diagnosed each year , leading to > 500 , 000 deaths [ 1 ]  . 
the disease is the third cause of cancer - related death in the united states ( around 150 , 000 new cases and > 52 , 000 deaths yearly ) [ 2 ] and uk , and the fourth cause of death at a global level [ 1 ]  . 
according to the staging criteria of the american joint committee on cancer ( ajcc ) , the presence of hepatic metastases determines a stage iv disease , which is associated with a highly unfavourable prognosis and a mean survival of 612 months if untreated [ 3 ]  . 
 in fact , several studies on the natural course of metastases ( when not completely ablated ) report 5 - year survival rates of 02.5% , whereas radical ablation has been shown to be effective in the treatment of liver metastases from crc [ 4 , 5 ]  . 
therefore , metastases remain the leading cause of death from crc [ 6 ] , and surgery is the gold standard treatment . at the time of initial diagnosis , only a minority of patients fulfil the criteria for radical surgery in terms of resectability , hepatic functional reserve , and performance status [ 3 ]  . 
this has led to the development of minimally invasive techniques , in particular , imaging - guided percutaneous approaches , as a valuable therapeutic alternative for the multimodal treatment of liver metastases in all settings in which radical surgery is precluded . 
rfa is now a common option for treating liver metastases from crc and is increasingly used as an adjunct to liver resection or as an alternative to it when surgery is not feasible . 
since its introduction , rfa has proven to be a highly versatile technique [ 8 ] that rapidly became popular for treating extrahepatic cancer as well [ 9 ] , thanks to its minimal invasiveness and well - proven safety . 
this paper presents our experience with rfa of liver metastases from crc and highlights the safety and benefits of the technique in terms of increased survival . ogni anno vengono diagnosticati almeno 1 milione di nuovi casi di cancro del colon - retto nel mondo , che causano oltre 500000 morti [ 1 ] ; tale neoplasia la terza causa di morte cancro - correlata negli stati uniti ( circa 150000 nuovi casi per anno e pi di 52000 decessi ) [ 2 ] e nel regno unito , e la quarta a livello mondiale [ 1 ]  . 
secondo i criteri di stadiazione del cancro dellamerican joint committee , la presenza di metastasi epatiche comporta la classificazione della malattia in stadio iv , che associato a una prognosi molto sfavorevole , con un tempo medio di sopravvivenza di 612 mesi senza trattamento [ 3 ]  . 
infatti , diversi studi sulla storia naturale delle metastasi ( quando non completamente asportate ) riportano tassi di sopravvivenza a 5 anni tra lo 0% e il 2 , 5% , mentre lo stesso presupposto rende lablazione radicale efficace nella cura delle metastasi epatiche da cancro del colon - retto [ 4 , 5 ]  . 
pertanto lo sviluppo di metastasi rimane la principale causa di morte per carcinoma del colon - retto [ 6 ] e la chirurgia il gold standard nel trattamento delle metastasi stesse . purtroppo , al momento della diagnosi iniziale solo una minoranza di pazienti soddisfa i criteri necessari per essere sottoposta a un intervento chirurgico radicale , sia in termini di resecabilit e di riserva epatica , sia riguardo il performance status del paziente [ 3 ]  . 
per questo motivo , sono state sviluppate tecniche minimamente invasive , in particolare con approccio percutaneo guidato dallimaging , come valida alternativa terapeutica nei trattamenti multimodali delle metastasi epatiche in tutte quelle situazioni in cui non sia possibile una chirurgia radicale ; queste terapie includono lablazione termica con radiofrequenze ( rfa ) [ 7 ]  . 
lrfa oggigiorno unopzione di trattamento delle metastasi epatiche da cancro del colon - retto diffusa in tutto il mondo , utilizzata con sempre maggiore frequenza come procedura complementare alla resezione epatica o come alternativa a essa nei casi in cui la chirurgia non sia possibile . 
dalla sua introduzione , lrfa ha dimostrato di essere una tecnica molto versatile [ 8 ] e il suo uso si diffuso rapidamente , anche per il trattamento del cancro a radiol med ( 2012 ) 117 : 11391151 materials and methods from march 1996 to january 2009 , we performed rfa of liver metastases from crc on 262 patients , for a total of 458 lesions treated . 
consistent with the literature , all metastases treated with rfa had been judged to be unresectable for reasons relating to patient or lesion characteristics : contraindications to general anaesthesia ( deterioration of general condition and / or cardiorespiratory disease ) , insufficient hepatic functional reserve , presence of extrahepatic metastases , recurrence after hepatectomy , progression of liver disease during systemic chemotherapy or location of hepatic lesions at sites deemed unresectable by the surgeon [ 3 , 12 , 13 ]  . preoperative assessment included abdominal contrastenhanced computed tomography ( ct ) and liver ultrasound ( us ) in all cases . 
all patients underwent us - guided percutaneous or laparotomic rfa , except one case of ct - guided percutaneous rfa ; in almost all cases , the decision to opt for a laparotomic approach was dictated by the need to resect the primary tumour and / or other metastases simultaneously . 
contrast - enhanced us was sometimes used to better depict isoechoic lesions during the procedure . the results of rfa were assessed by contrast - enhanced ct at 1 , 6 and 12 months to depict any remaining tumoural tissue at the margins of the ablation zone ; additional us , ct and positron - emission tomography - ct ( pet - ct ) studies were acquired to diagnose subsequent tumour progression . 
 outcomes were calculated on the basis of patient survival at the most recent follow - up visit or at death due to disease progression or other causes . each patient provided informed consent before the procedure . 
the study was conducted according to the guidelines for retrospective reviews established by the institutional review board of our hospital . patients and lesions analysis of the data extracted from our institutes database allowed us to identify the following variables for each of the patients treated : gender and age ; time of onset of metastases ( synchronous or metachronous ) ; number ( single or multiple ) , location and size ( largest diameter in mm ) of liver metastases ; presence of other metastases prior to treatment ( including nodal metastases ) ; complications during or after the procedure ; any other therapy , including systemic secondor third - line chemotherapy , in most cases following the 5 - fluorouracil , leucovorin and oxaliplatin ( folfox ) or 5 - fluorouracil , leucovorin , and irinotecan ( folfiri ) regimen with 1141 livello extraepatico [ 9 ] , grazie alla sua minima invasivit e ben dimostrata sicurezza . 
in questo lavoro intendiamo presentare lesperienza maturata a partire dal 1996 nel nostro istituto nel trattamento con rfa delle metastasi epatiche da carcinoma del colon - retto , cercando di evidenziare la sicurezza di questa tecnica e i benefici in termini di aumento della sopravvivenza che essa pu apportare . materiali e metodi tra marzo 1996 e gennaio 2009 , 262 pazienti sono stati sottoposti , presso il nostro istituto , a rfa per metastasi epatiche da carcinoma del colon - retto , per un totale di 458 lesioni trattate . 
in accordo con la letteratura , tutte le metastasi trattate con rfa erano state giudicate non passibili di intervento chirurgico per motivi legati al paziente o alle lesioni : controindicazioni allanestesia generale ( compromissione generale e / o problemi cardio - respiratori ) , insufficiente riserva epatica , presenza di metastasi extraepatiche , recidiva dopo epatectomia , progressione della malattia epatica in corso di chemioterapia sistemica , localizzazione delle lesioni epatiche in siti giudicati non resecabili dal chirurgo [ 3 , 12 , 13 ]  . nella valutazione pre - procedurale sono sempre state effettuate una tomografia computerizzata ( tc ) con mezzo di contrasto ( mdc ) delladdome e unecografia epatica . 
tutti i pazienti sono stati sottoposti a rfa ecoguidata con approccio percutaneo o laparotomico , tranne un caso di rfa percutanea tc - guidata ; la decisione di preferire un approccio laparotomico stata quasi sempre dettata dalla necessit di resecare contemporaneamente il tumore primitivo e / o altre metastasi . 
lecocontrastografia stata talvolta utilizzata per visualizzare meglio le lesioni isoecogene nel corso della procedura . il risultato della rfa stato valutato mediante tc con mdc a 1 , 6 e 12 mesi dalla procedura per evidenziare eventuale tessuto tumorale residuo alla periferia della zona di ablazione ; ulteriori controlli ecografici , tc e tomografia ad emissione di positroni ( pet ) - tc sono stati eseguiti nel tempo al fine di diagnosticare successive progressioni tumorali . 
loutcome della malattia stato calcolato in base alla sopravvivenza del paziente alla data dellultimo controllo o alla morte a causa della progressione della malattia o per altre cause . ogni paziente ha sottoscritto il consenso informato prima della procedura . 
among the former , 71 had solitary lesions ( 53.4% ) and 62 multiple lesions ( 46.6% ) ; among the latter , 83 had solitary lesions ( 64.3% ) and 46 multiple lesions ( 35.7% ) , for a total of 154 patients with solitary metastases ( 58.8% ) and 108 with multiple lesions ( 41.2% ) at the time of rfa . 
it was the first metastasis in 107 patients , whereas 102 had already developed liver metastases ( though not extrahepatic ) treated by means other than rfa . extrahepatic metastases were detected before rfa treatment in 51 patients ( 19.5% ) , occasionally at more than one site : 27 pulmonary , 14 peritoneal , 4 nodal at the hepatic hilum , 3 osseous , 1 cerebral , 1 retroperitoneal , 1 right adrenal , 1 peritoneal in the right iliac fossa , 1 diaphragmatic and 1 uterine . 
one patient was also affected by multiple myeloma and another by urothelial neoplasm of the bladder . prior to rfa , all patients had undergone the standard treatment protocols in use at the time : whenever possible , they had undergone partial hepatectomy . 
regarding the systemic chemotherapy protocols , until 2000 , patients had mainly been treated with 5 - fluoruracil alone , from 2001 with folfox / folfiri combinations and from 2004 with additional target therapies as well . 
a total of 458 lesions received at least one rfa session ; of these , 36 were retreated in a second session ( 7.9% ) owing to persistence of residual tumour . 
of the 36 lesions retreated because of residual tumour , 33 were treated percutaneously and 3 during laparotomy . equipment rfa was performed with cool - tip electrodes in the first 14 treatments ( radionics , burlington , ma , usa ) and with multitined rita starburst ( rita medical systems , inc . , mountain view , ca , usa ) and leveen ( boston scientific , waltham , ma , usa ) electrodes in the following 249 and 195 lesions , respectively . 
the ablation algorithm is based on delivered energy for the radionics system , temperature for the rita system and tissue impedance for the boston pazienti e lesioni analizzando i dati estratti dal database del nostro istituto , per ogni paziente trattato sono state identificate le seguenti variabili : il sesso e let ; il tempo di esordio delle metastasi ( sincrone o metacrone ) ; il numero ( unica o multiple ) , la localizzazione e la dimensione ( diametro massimo in mm ) delle metastasi epatiche ; la presenza di altre metastasi pretrattamento ( comprese le metastasi linfonodali ) ; le complicanze durante o dopo la procedura ; altre eventuali terapie ( incluse chemioterapie sistemiche di seconda o terza linea , nella maggior parte dei casi con schema folfox / firi abbinato o meno a target therapies ) ; la data del decesso o la data di fine di osservazione . dei 262 pazienti trattati , 155 erano maschi ( 59 , 2% ) con unet media di 66 , 2 anni ( mediana 67 , 6 anni ) e 107 femmine ( 40 , 8% ) con unet media di 66 , 1 anni ( mediana , 67 , 8 anni )  . 
al momento della prima rfa let media generale era di 66 anni ( mediana , 67anni , range 3089 anni )  . in 133 pazienti , le metastasi erano sincrone ( 50 , 8% ) e in 129 metacrone ( 49 , 2% )  . 
tra i primi , 71 avevano lesioni solitarie ( 53 , 4% ) e 62 lesioni multiple ( 46 , 6% ) , mentre tra i secondi sono state diagnosticate 83 lesioni solitarie ( 64 , 3% ) e 46 multiple ( 35 , 7% ) , per un totale di 154 pazienti con metastasi solitarie ( 58 , 8% ) e 108 con lesioni multiple al momento del trattamento ( 41 , 2% )  . 
 in 51 pazienti ( 19 , 5% ) erano state invece rilevate anche lesioni metastatiche extraepatiche prima del trattamento con rfa , a volte in pi di una sede : 27 polmonari , 14 peritoneali , 4 linfonodali allilo epatico , 3 ossee , 1 cerebrale , 1 retroperitoneale , 1 surrenalica destra , 1 peritoneale in fossa iliaca destra , 1 diaframmatica e 1 uterina . 
un paziente era affetto anche da mieloma multiplo e un altro da neoplasia uroteliale vescicale . tutti i pazienti avevano ricevuto come trattamenti antecedenti lrfa i protocolli di terapia standard relativi al proprio periodo : quando possibile erano stati sottoposti a epatectomie parziali e , per quanto riguarda i protocolli di chemioterapia sistemica , fino al 2000 erano stati trattati prevalentemente col solo 5 - fluoruracile , dal 2001 con associazioni folfox / firi e dal 2004 anche con combinazioni con target therapies . 
quattrocentocinquantotto lesioni hanno subito almeno una sessione di rfa ; tra queste , 36 sono state trattate nuovamente in una seconda sessione ( 7 , 9% ) a causa della persistenza di tessuto tumorale residuo . 
in particolare , 321 metastasi ( 70 , 1% ) avevano diametro inferiore o uguale a 3 cm e 137 ( 29 , 9% ) diametro superiore a 3 cogni paziente stato associato al diametro della sua metastasi principale al momento della rfa . 
delle 36 lesioni sottoposte a nuovo trattamento a causa della perradiol med ( 2012 ) 117 : 11391151 1143 scientific syste depending on the generators available ( with maximum power rising from 50 to 200 w over the years ) , ablation time ranged from 7 to 20 mthe choice of equipment was related to availability rather than to other variables . before the procedure , all patients underwent routine laboratory tests , with particular attention being paid to coagulation , which was corrected in the few cases of thrombocytopaenia , antiplatelet therapy or increased inr . 
a local anaesthetic was administered at the needle entry point and under conscious sedation ; patients treated during laparotomy necessarily required general anaesthesia . adverse events complications were considered both in terms of absolute number and of percentage , subdivided according to the society of interventional radiology ( sir ) classification into minor and major ( requiring surgical intervention or radiological manoeuvres , blood transfusion , significant medical therapies or longer hospital stay ) , and stratified on the basis of the technique used ( percutaneous or intraoperative )  . survival survival , expressed in months , was calculated for each patient from the date of diagnosis of liver metastases and rfa treatment ( often significantly delayed relative to the diagnosis of metastasis because of the use of other treatments ) until death or the end of our observation period . 
in both cases , we calculated overall survival curves and stratified them according to the possible prognostic factors represented by patient and lesion variables . statistical analysis all variables were entered into a microsoft excel spreadsheet ( microsoft , inc . , redmond , wa , usa ) for processing by dedicated statistical analysis software ( sas version 8 ; sas institute , inc . , cary , nc , usa )  . 
the statistical analysis did not consider 14 patients ( with a total of 18 lesions ) who were lost to follow - up after rfa ( due to refusal to participate or inability to locate )  . 
multivariate analysis was not performed , as the covariates available were too few and sistenza di tessuto tumorale residuo , 33 sono state trattate con tecnica percutanea e 3 durante laparotomia . apparecchiature per eseguire lrfa sono stati usati ago - elettrodi cool - tip nei primi 14 trattamenti ( allora radionics , burlington , ma , usa ) ed elettrodi multitined rita starburst ( rita medical systems , inc . , mountain view , ca , usa ) e leveen ( boston scientific , waltham , ma , usa ) nelle successive 249 e 195 lesioni , rispettivamente . 
anche a seconda dei generatori a disposizione ( con potenza massima cresciuta , nel corso degli anni , da 50 a 200 w ) , il tempo per ogni ablazione variato da 7 a 20 mla scelta delle apparecchiature utilizzate stata legata alla loro disponibilit piuttosto che ad altre variabili . prima di eseguire la procedura , per tutti i pazienti sono stati effettuati esami laboratoristici di routine , con particolare attenzione alla coagulazione , che stata corretta nei rari casi di piastrinopenia , terapia antiaggregante o aumentato international normalized ratio ( inr )  . 
tutte le rfa percutanee sono state eseguite sotto guida ecografica ( salvo il caso tc - guidato sopra citato ) , con il paziente monitorato , in ambiente sterile , effettuando lanestesia locale nel sito di infissione dellago - elettrodo e in sedazione cosciente ; i casi eseguiti durante laparotomia , ovviamente , hanno comportato lanestesia generale . eventi avversi le complicanze sono state considerate sia nel numero assoluto sia in percentuale , suddivise in accordo con la classificazione della society of interventional radiology ( sir ) in minori e maggiori ( ovvero che hanno reso necessari interventi chirurgici o manovre radiologiche , trasfusioni di sangue , significative terapie mediche o una pi lunga ospedalizzazione ) , e stratificate in base alla tecnica utilizzata ( percutanee o intraoperatorie )  . sopravvivenza la sopravvivenza , espressa in mesi , stata valutata per ogni paziente sia dalla data della diagnosi delle metastasi epatiche , sia dalla data del trattamento con rfa ( spesso eseguito a significativa distanza dalla diagnosi di metastasi per il precedente impiego di altre terapie ) , fino al decesso o alla fine della nostra osservazione . 
in entrambi i casi sono state calcolate le curve di sopravvivenza , totali e stratificate per i possibili fattori prognostici costituiti dalle caratteristiche dei pazienti e delle lesioni sopra elencate . analisi statistica tutte le variabili sono state inserite in un foglio di calcolo 1144 radiol med ( 2012 ) 117 : 11391151 unequally distributed among groups to allow for stable modelling . 
only three patients developed major complications ( 1.2% ) : one infected biloma that was drained percutaneously ; one segmental biliary dilatation followed by cholangitis and biliobronchial fistula that was treated with biliary drainage ; and one haemoperitoneum that required transarterial embolisation and blood transfusion . 
in the 36 cases of retreatment due to residual tumour or local relapse , 4 complications occurred ( 11.1% ) , two of which were major : one surgical haemoperitoneum with iatrogenic seeding of neoplastic tissue at the level of the abdominal wall , and one abdominal wall phlegmon caused by a perforation concealed by the adjacent colon . survival overall survival at 1 , 2 , 3 and 5 years was 93% , 78% , 62% and 35% from the time of metastasis diagnosis and 84% , 59% , 43% and 23% from the time of rfa treatment . 
 median survival was 46 months from metastases diagnomicrosoft excel ( microsoft , inc . , redmond , wa , usa ) per essere utilizzate dal software sas dedicato allanalisi statistica ( sas versione 8 ; sas institute , inc . , cary , nc , usa )  . 
 per quanto riguarda lanalisi statistica dei risultati della procedura , 14 pazienti sono stati esclusi ( per un totale di 18 lesioni ) in quanto persi al follow - up dopo la rfa ( per irraggiungibilit o rifiuto di ulteriori esami )  . 
stato applicato un cut - point per le variabili di tipo continuo , per esempio il diametro della lesione principale in ogni paziente , per convertirle in una scala dimensionale corrispondente alle categorie utilizzate in letteratura o creare sottogruppi . 
il tempo di follow - up medio dallablazione ( fino alla morte o alla fine dellosservazione ) stato di 26 , 4 mesi ( mediana 19 , 2 mesi , range 2 , 4129 , 6 mesi )  . eventi avversi dopo la prima rfa sono stati osservati eventi avversi direttamente o indirettamente legati alla procedura nel 7 , 3% dei pazienti ( 18 / 248 ) e nel 5 , 2% delle lesioni ( 23 / 440 )  . 
solo 3 pazienti hanno sviluppato complicanze maggiori ( 1 , 2% ) : un biloma infetto , drenato per via percutanea , una dilatazione biliare segmentaria seguita da colangite e fistola bilio - bronchiale , curata con drenaggio biliare , e un emoperitoneo che ha richiesto lembolizzazione transarteriosa e una trasfusione di sangue . 
i rimanenti 15 pazienti hanno presentato una o pi complicazioni minori che non hanno richiesto alcun tipo di intervento : 3 casi di emoperitoneo di scarsa entit ( senza necessit di trasfusione ) , 4 dilatazioni biliari prive di significato clinico , 4 casi di dolore persistente , 3 ipertermie per alcuni giorni e un accumulo di fluido subcapsulare a risoluzione spontanea . nessuna delle variabili sopra descritte , relative ai pazienti , alle lesioni o alla procedura , risultata predittiva per lo sviluppo di complicanze ; in particolare , neppure la dimensione media delle lesioni con eventi avversi post - procedurali risultata differente rispetto a quella delle lesioni radiol med ( 2012 ) 117 : 11391151 1145 fig . 
2 curva di sopravvivenza degli stessi pazienti di figura 1 dalla data della rfa . sis to death [ 95% confidence interval ( ci ) , 39 - 53 ] and 32 months from rfa treatment to death ( 95% ci , 2540 )  . 
a total of 131 / 248 patients died during the follow - up : 7 deaths ( 5.3% ) were caused by unrelated conditions ( cardiovascular disease ) , whereas the other 124 were due to disease progression . 
nei 36 casi di trattamento ripetuto per residuo tumorale o recidiva locale si sono verificate 4 complicanze ( 11 , 1% ) , di cui 2 maggiori : un emoperitoneo chirurgico con insemenzamento iatrogeno di tessuto neoplastico a livello della parete addominale e un flemmone della parete addominale dovuto a una perforazione coperta del colon adiacente . sopravvivenza la sopravvivenza globale a 1 , 2 , 3 , e 5 anni stata del 93% , 78% , 62% e 35% dal momento della diagnosi di metastasi , e dell84% , 59% , 43% e 23% dalla data del trattamento con rfa . 
la sopravvivenza mediana stata di 46 mesi datando le curve dal momento della diagnosi di metastasi [ 95% intervallo di confidenza ( ic ) : 3953 ] e di 32 mesi datando 1146 predictors table 1 univariate analysis of main predictors for survival synchronous vs . 
conversely , significant differences in survival were seen in relation to the presence or absence of extrahepatic disease at the time of treatment and especially in relation to the size of the main metastasis at the time of rfa ( table 1 )  . 
centotrentuno ( di 248 ) pazienti sono morti durante il follow - up : 7 decessi ( 5 , 3% ) sono stati causati da malattie non correlate ( patologie cardio - vascolari ) , mentre gli altri 124 si sono verificati per progressione di malattia . 
per quanto riguarda la sicurezza della tecnica , il tasso complessivo di complicanze risultato basso , con mortalit 0% ed eventi avversi nel 7 , 3% dei pazienti e nel 5 , 2% delle lesioni trattate . 
these results are in line with those published in other large multicentre studies , which report rates of major complications ranging from 1% to 3% , and of minor complications from 5% to 8.9% [ 1 , 1418 ]  . 
this finding could be related to greater aggressiveness of the treatment ( multiple insertions , longer ablation time , etc . ) , justified by the fear that the lesion may be resistant . the true challenge for rfa is to increase survival . 
the methodological question underlying this estimate is that in all retrospective studies , > 80% of patients are treated with rfa after undergoing other therapies for the same metastatic disease , and more than two thirds of them experience local or metastatic progression . 
questo risultato potrebbe essere legato a una maggior aggressivit del trattamento ( inserzioni multiple , maggior tempo di erogazione , ecc . ) , motivata dal timore di una resistenza della lesione al trattamento stesso . la vera sfida per la rfa laumento della sopravvivenza . 
il problema metodologico alla base di questa stima che in tutti gli studi retrospettivi oltre l80% dei pazienti giunge alla rfa dopo aver gi ricevuto altre terapie per la medesima malattia metastatica e pi di due terzi va incontro a progressione locale o eterofocale , per cui pi di tre quarti dei pazienti vengono sottoposti a ulteriori terapie successive alla rfa , che possono consolidarne ma anche mistificarne lefficacia . nel nostro studio la sopravvivenza globale a 1 , 2 , 3 , e 5 1148 radiol med ( 2012 ) 117 : 11391151 fig . 
4 curve di sopravvivenza in base alla presenza ( y - ) o meno ( n - ) di metastasi extraepatiche al momento del trattamento . than three fourths of patients undergo other therapies following rfa , which may either enhance or hinder its effectiveness . in our study , overall survival at 1 , 2 , 3 and 5 years was 93% , 78% , 62% and 35% from the time of diagnosis of metastasis , and 84% , 59% , 43% and 23% from the time of treatment ; median survival was 46 months from diagnosis and 32 months from rfa . 
these data are consistent with those reported in the literature : all studies report better midterm survival curves for unresectable metastases compared with the natural course of the disease ( median survival of patients with liver metastases who do not receive treatment is not longer than 9 months [ 19 ] ) ; survival following rfa at 1 year was high in all studies ( 8393% ) ; survival at 3 years was 3641% , nearing those of surgical patients [ 20 ]  . 
 [ 21 ] report a median survival period of 38 months from the diagnosis of liver metastasis , with 99% survival rate at 1 year , 58% at 3 years and 30% at 5 years , whereas from the first rfa treatment , the values were 31 months and 91% , 28% and 25% , respectively . 
 [ 24 ] , who report a mean survival period and survival rates at 3 years from rfa of 67 months and 66% in patients with small solitary lesions with diameter < 3 coverall , these results ( including those of other studies [ 13 , 2023 ] ) are better than those obtained with chemotherapy , even when associated with a target therapy ( median > 20 months , but survival at 5 years close to 0 [ 2429 ] ) , providing indirect evidence that rfa improves survival in patients with metastatic liver disease ; however , no randomised controlled anni stata 93% , 78% , 62% e 35% dal momento della diagnosi di metastasi , e 84% , 59% , 43% e 23% dal trattamento ; la sopravvivenza mediana stata 46 mesi nel primo caso e 32 mesi nel secondo . 
questi dati sono in linea con quelli della letteratura : tutti gli studi riportano curve di sopravvivenza a medio termine per metastasi non resecabili migliori rispetto alla storia naturale della malattia ( la mediana di sopravvivenza di pazienti con metastasi epatiche che non ricevono nessun trattamento non superiore a 9 mesi [ 19 ] ) ; la sopravvivenza a 1 anno elevata in tutti gli studi ( tra l83% e il 93% ) ; i tassi di sopravvivenza a 3 anni risultano tra il 36% e il 41% , molto vicini a quelli dei pazienti chirurgici [ 20 ]  . 
 [ 21 ] riportano una sopravvivenza mediana di 38 mesi dalla diagnosi di metastasi epatiche , con sopravvivenze 99% a 1 anno , 58% a 3 anni e 30% a 5 anni , mentre dalla prima rfa gli stessi valori sono 31 mesi e 91% , 28% , e 25% , rispettivamente . 
 [ 24 ] , che riportano sopravvivenza media e tasso di sopravvivenza a 3 anni dalla rfa 67 mesi e 66% nei pazienti con lesioni solitarie piccole , cio di diametro < 3 cnel complesso questi risultati ( inclusi quelli degli altri studi [ 13 , 2023 ] ) risultano migliori di quelli ottenuti con la chemioterapia , anche abbinata a target therapy ( mediana superiore ai 20 mesi , ma sopravvivenza a 5 anni prossima a 0 [ 2429 ] ) , fornendo elementi di prova indiretta che la rfa migliora la sopravvivenza nei pazienti con malattia metastatica epatica ; a supporto di questa tesi , per , non stato finora possibile condurre a termine trial randomizzati controllati in grado di confrontare adeguatamente la sola chemioterapia rispetto alla stessa chemioterapia in combinazione con lrfa . sebbene non sia possibile paragonare gli studi sulla reradiol med ( 2012 ) 117 : 11391151 1149 trials adequately comparing chemotherapy alone with chemotherapy combined with rfa have been conducted to support this view . although it is not possible to compare studies on liver resection used as first - line treatment with a radical intent with studies on rfa that include patients who have already undergone conventional treatments , if we compare survival at 5 years between surgically treated patients ( 2540% ) and those treated with rfa at our centre ( 35% from the diagnosis of metastasis ) , the results are very similar and should no doubt be considered promising [ 30 , 31 ]  . 
in our series , the diagnosis of synchronous or metachronous metastases or the presence of single or multiple lesions at the time of rfa did not influence survival ; in particular , as concerns multifocal disease , its greater dangerousness is probably lessened by the capability that rfa has , just like surgery , of treating several lesions at the same time . the evidence that a main lesion diameter < 3 cm and - even more - < 2.5 cm has a significant impact on survival further demonstrates the importance of achieving radical ablation , whether with rfa or surgery . 
in fact , in the case of small hepatic lesions , published data report comparable results between rfa and surgery , even in terms of survival [ 20 ]  . 
therefore , if rfa is today still a second - line choice when surgery is feasible , in the future , it may become the first - line choice , especially when the test of time approach suggested by livraghi in 2003 is applied ( that is , the use of rfa to reduce the number of unnecessary surgical resections ) [ 33 ]  . as concerns the presence of extrahepatic disease at the time of rfa , in contrast to our findings in an earlier , smaller series , this review seems to suggest a significantly shorter survival period compared with the group with disease confined to the liver . 
on this sezione epatica , utilizzata in prima istanza con intento radicale , con quelli sulla rfa , che includono pazienti in cui spesso le opzioni terapeutiche convenzionali sono gi state impiegate , se si confronta la sopravvivenza a 5 anni dei pazienti trattati chirurgicamente , che va dal 25% al 40% , con quella dei pazienti trattati con rfa nel nostro centro ( 35% dalla diagnosi di metastasi ) , si evidenzia come tali risultati siano molto simili e da considerarsi certamente promettenti [ 30 , 31 ]  . 
nella nostra casistica , la diagnosi delle metastasi sincrona o metacrona , o la presenza di lesioni uniche o multiple al momento della rfa non sono risultate influenti sulla sopravvivenza ; in particolare , per quanto riguarda la multifocalit , la sua maggior pericolosit probabilmente stemperata dalla capacit della rfa , al pari della chirurgia , di trattare pi lesioni contemporaneamente . levidenza che il diametro della lesione principale inferiore a 3 cm e , ancor pi , a 2 , 5 cm incide significativamente sulla sopravvivenza unulteriore riprova dellimportanza di ottenere la radicalit con la rfa , cos come con la chirurgia . 
infatti , in caso di lesioni epatiche piccole , in letteratura sono stati riportati risultati uguali tra rfa e chirurgia anche in termini di sopravvivenza [ 20 ] ; quindi , se oggi il ruolo della rfa ancora di seconda scelta quando possibile lopzione chirurgica , in futuro lindicazione alla rfa potrebbe diventare di prima scelta , soprattutto applicando il concetto di test - of - time gi proposto da livraghi et al . 
nel 2003 ( ossia luso della rfa per ridurre il numero di resezioni chirurgiche inutili ) [ 33 ]  . per quanto riguarda la presenza di malattia extraepatica al momento della rfa , a differenza di una nostra precedente valutazione su casistica pi limitata , questa nostra ultima revisione sembra dimostrare una sopravvivenza significativamente inferiore rispetto al gruppo con malattia esclusivamente localizzata al fegato ; ci comprensibile se si tiene conto del fatto che in questi casi lrfa pu non essere radicale e i pazienti possono decedere a causa della malattia extraepatica , ma non esclude lutilit della rfa rispetto a pazienti con malattia extraepatica non trattati . 
 [ 13 ] non hanno evidenziato differenze di sopravvivenza in presenza di malattia extraepatica ; invece 1150 radiol med ( 2012 ) 117 : 11391151 subject , the literature reports conflicting results : siperstein et al . 
knauth springer - verlag berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 540 - 87596 - 3 e - isbn : 978 - 3 - 540 - 87597 - 0 doi 10.1007 / 978 - 3 - 540 - 87597 - 0 published online : 7 january 2012 springer - verlag 2012 more than a book , this is an encyclopaedia on kidney radiological imaging . 
it is a voluminous text - book presenting the reader in its 896 pages plus index , all possible pathological and clinical problems affecting the kidney . the reader will find 36 chapters divided into five parts : embryology and anatomy ; imaging and interventional modalities ; non - tumoral pathology ; tumor pathology ; special topics . quaia is not only the editor of the book , but also the author of 6 chapters and co - author of 6 additional chapters . 
 a very impressive one - man effort . all the other chapters are the product of contributions from a team of well - known experts from italian , european and north - american hospitals . 
he is also presented with the different and continuously improving diagnostic tools [ basic radiology , ultrasound ( us ) , computed tomography ( ct ) , primarily multidetector ct , magnetic resonance imaging ( mri ) , angiography and vascular interventional radiology procedures as well as nonvascular interventional procedures , nuclear medicine , renal biopsy , molecular imaging ] , and what is now considered out of date intravenous urography . 
 all of the above diagnostic tools are relevant to the text , documenting all possible kidney affections and diseases from infection ( with detailed information on the latest discussion on the topic ) to malformation , tumour staging [ recently up - dated world health organization ( who ) classification ] , transplantation , imaging of dialysis , postoperative kidney , etc . , not to mention the use of contrast media and possible drawbacks ( nephrogenic systemic fibrosis ) , functional imaging of the kidney and future trends in renal imaging . 
 pi che un semplice volume , questo libro da considerare unenciclopedia sullo studio per immagini del rene : un testo vouluminoso che nelle sue 896 pagine , pi quelle dellindice , presenta al lettore una disanima di tutti i possibili problemi clinici e patologici che possono interessare il rene . 
 il lettore trover la materia trattata in 36 capitoli , divisi in cinque sezioni : embriologia ed anatomia ; studio per immagini e tecniche interventistiche ; patologia non tumorale ; patologia tumorale ; argomenti speciali . 
 tutti gli altri capitoli sono il risultato dei contributi di un gruppo di ben riconosciuti esperti che prestano la loro opera in ospedali italiani , europei e nord - americani . il lettore viene condotto dallembriologia e sviluppo del rene , alla anatomia radiologica ed alla sua fisiologia : viene poi anche messo a conoscenza ed a fronte dei vari strumenti diagnostici in continua evoluzione [ radiologia tradizionale , ecografia ( us ) , tomografia computerizzata ( tc ) , in particolare tc multidetettore , risonanza magnetica ( rm ) , angiografia , procedure di radiologia interventistica vascolare e di interventitisca non - vascolare , medicina nucleare , biopsie renali , imaging molecolare ] , nonch di quellurografia endovenosa attualmente considerata obsoleta . tutti gli strumenti diagnostici di cui sopra sono ben pertinenti accompagnatori del testo , documentando tutte le possibili affezioni e malattie renali , dallinfezione ( con informazioni dettagliate sulle ultime discussioni sullargomento ) alle malformazioni , dalla stadiazione dei tumori ( riportando la classificazione recentemente aggiornata della world health organization ) ai trapianti , dallo studio per immagini nella dialisi , al rene post - operatorio , ecc . , senza dimenticare luso dei mezzi di contrasto e le loro possibili complicanze ( fibrosi nefrogenica sistemica ) , allo studio per immagini funzionali ed ai futuri sviluppi nello studio per immagini del rene . 
 radiol med ( 2012 ) 117 : 12681269 1269 the ever increasing importance of us in all its possible aspects , doppler , colour and power doppler , contrast - enhanced us as a first - step diagnostic instrument is stressed all throughout the book . 
emphasis is also given to ct , which is able to detect , when performed for the diagnosis of other abdominal problems , unsuspected tumours in an early stage , with its ability to provide high spatial resolution of the kidney and renal arteries . 
 as a paediatric radiologist , i greatly appreciated the two chapters on congenital development disorders of the kidney and the other on the paediatric kidney ( however , there were too many self - citations in this last one ! )  . 
in some of the chapters there is also the strange habit of not presenting the images in consecutive order ( for instance image b not necessarily be next to image a , etc . ) , which often is confusing for the reader . i would have liked to have had a list of the acronyms that are used all throughout the book . 
acronyms are sometimes a nightmare for the reader , especially when he / she is not an expert on the topics and their hidden secrets . the reference list in each chapter is quite extensive and up - to - date , some citations are even from 2010 . 
the index is quite large , yet not always complete . in summary , this is a book that will be greatly appreciated by radiologists , urologists , nephrologists and clinicians , a book which will surely mark a point of arrival in the diagnosis and understanding of kidney diseases and the ensuing correct treatment of patients , one more example of the high - standards in italian , european and north american radiology . lungo tutto il testo viene messa in evidenza la sempre maggior importanza dellecografia in tutti i suoi possibili aspetti ( doppler , doppler a colori e power doppler , ecografia con contrasto ) , quale strumento diagnostico di primo livello . 
viene poi enfatizzato luso della tc che in grado , quando utilizzata per lo studio di altri problemi addominali , di mettere in evidenza ( data la sua capacit di fornire unalta risoluzione spaziale del rene e delle arterie renali ) , tumori renali del tutto insospettati , asintomatici ed in uno stadio molto precoce . da radiologo pediatrico ho molto apprezzato i due capitoli sulle malformazioni dello sviluppo congenito e sul rene pediatrico ( con troppe auto - citazioni in questultimo ! )  . 
in alcuni dei capitoli vi poi lo strano vezzo di non presentare le immagini in ordine consecutivo ( per esempio limmagine b non necessariamente vicino alla a ecc . ) , con conseguente confusione per chi legge . mi sarebbe piaciuta la presenza di un elenco degli acronimi usati nel testo . 
gli acronimi rappresentano spesso un incubo per il lettore , soprattutto se questi non un esperto degli argomenti trattati e dei loro nascosti segreti . lelenco delle voci bibliografiche in ciascun capitolo piuttosto ampio e ben aggiornato , con riferimenti anche al 2010 . 
volterrani1 1uoc di radiologia universitaria , istituto toscano tumori , azienda ospedaliera universitaria senese , universit degli studi di siena , viale bracci , 53100 siena , italy 2radioterapia , istituto toscano tumori , azienda ospedaliera universitaria senese , universit degli studi di siena , viale bracci , 53100 siena , italy 3anatomia patologica , istituto toscano tumori , azienda ospedaliera universitaria senese , universit degli studi di siena , viale bracci , 53100 siena , italy 4chirurgia ii , istituto toscano tumori , azienda ospedaliera universitaria senese , universit degli studi di siena , viale bracci , 53100 siena , italy correspondence to : s.f. 
a diffusion - weighted ( dw ) sequence was acquired [ spin - echo diffusion - weighted echo - planar imaging ( sedw - epi ) ] with a b - value of 800 s / mm2 and volume ( vdwi ) was calculated by semiautomatic segmentation of tumour hyperintensity . 
due osservatori hanno estrapolato indipendentemente il vc dalle immagini t2 - pesate e il vdwi dallacquisizione spin echo ( se ) - echo - planar imaging ( epi ) - diffusion - weighted ( dw ) ( b - value 800 s / mm ) mediante segmentazione semiautomatica delliperintensit patologica . 
la vdwi sembra essere promettente per valutare la risposta alla chrt nelle neoplasie rettali , tuttavia sono necessari ulteriori studi su casistiche pi ampie al fine di migliorare la qualit di tale metodo e per valutarne il reale valore predittivo . 
 parole chiave risonanza magnetica diffusione neoplasia rettale volumetria neoplasia terapia adiuvante introduction preoperative management of patients affected by locoregionally advanced rectal cancer relies on concurrent chemoradiotherapy ( chrt ) [ 1 ]  . 
this approach achieves tumour regression in many cases , and an improved prognosis after surgery in responding patients is reported by many authors in terms of both decreased local failure rate and improved metastasisfree and overall survival [ 1 , 2 ]  . 
 however , volumetric decrease and downstaging , also if available , are not suitable markers of a favourable response , neither does a residual mass always imply a defective tumour response [ 4 , 5 ]  . 
a correlation between tumour response to chrt and a favourable clinical course after surgery could be demonstrated by identifying suitable reproducible pathological parameters , such as tumour regression grade ( trg ) [ 4 , 6 ]  . 
 many methods have been investigated by which to assess presurgical tumour response to chrt using imaging , and magnetic resonance imaging ( mri ) for volumetric evaluation seems to be a promising tool . 
the accuracy of mri in volume quantification has been the subject of previous reports [ 8 , 9 ] , but the significant tissue changes outlined above decrease its reliability in assessing actual tumour regression [ 10 ]  . 
diffusion - weighted mri ( dw - mri ) might be useful to show viable neoplastic tissue because of its reliability in detecting the restricted proton diffusion in hypercellular tissues introduzione il trattamento pre - operatorio dei pazienti affetti da cancro del retto localmente avanzato attualmente basato sulla chemio - radioterapia ( chrt ) concomitante [ 1 ]  . 
questa impostazione ottiene la regressione del tumore in molti casi ; un miglioramento prognostico viene riportato da diversi autori , in termini sia di riduzione del rischio di recidiva locale , sia di sopravvivenza globale e libera da metastasi a distanza [ 1 , 2 ]  . 
tuttavia la riduzione dimensionale del tumore ed il downstaging , per quanto utilizzabili nella pratica clinica , non sono di per s marker affidabili di risposta favorevole n una massa residua implica sempre una mancata risposta della malattia [ 4 , 5 ]  . 
una correlazione tra risposta del tumore alla chemio - radioterapia e decorso clinico favorevole dopo chirurgia potrebbe essere dimostrata attraverso lidentificazione di parametri anatomo - patologici idonei e riproducibili come il cosiddetto tumor regression grade ( trg ) [ 4 , 6 ]  . 
questo metodo prende in considerazione un ampio spettro di modificazioni rilevabili dopo chrt : quantit di cellule neoplastiche residue , modificazioni a livello cellulare ( picnosi del nucleo , necrosi ed eosinofilia ) e stromale ( fibrosi densa o edematosa , infiltrato infiammatorio , granulomatosi giganto - cellulare intorno alle ghost cells e presenza di cheratina ) [ 4 ]  . 
 ad oggi molti metodi di imaging sono stati utilizzati per valutare la risposta neoplastica alla chrt prima della chirurgia e , in tale ambito , la misurazione del volume neoplastico con rm sembra uno strumento promettente , essendo gi stata dimostrata una generica correlazione tra volume del tumore valutato con rm e volume patologico [ 7 ]  . 
 laccuratezza in tale quantificazione volumetrica stata argomento di precedenti pubblicazioni [ 8 , 9 ] , ma le notevoli modificazioni tissutali post - chrt diminuiscono laffidabilit di questo parametro nella valutazione della reale 1114 radiol med ( 2012 ) 117 : 11121124 with high nucleocytoplasmic ratio [ 12 ]  . 
therefore , a 3d measurement of the signal directly expressing the presence of neoplastic tissue can be obtained in the attempt to generate functional volumetry . the aim of this study was to evaluate the feasibility in terms of reproducibility ( interobserver agreement ) of dwmri volumetry in rectal cancer treated by chrt and to establish a comparison with conventional mr volumetry , in respect to trg , in order to assess the potentially better prediction of tumour response of the former method . 
furthermore , the reproducibility of dw - mri was assessed by analysis of concordance of results obtained independently by two separate observers . materials and methods patients fourteen patients ( age range 5574 years ; mean 65.6 years ) with endoscopic and bioptic diagnosis of rectal carcinoma were retrospectively included in this study . 
after a clinical and imaging workup [ based on abdominal mri , chest x - ray or computed tomography ( ct ) and liver ultrasound ( us ) in all cases , and transrectal endoscopy in 12 cases ] patients were staged as follows : dukes stage a in three cases , stage b in one case and stage c in ten cases . 
in relation to the tnm system , they were all ct3t4 , n0 / + , m0 and were therefore included in a preoperative chrt protocol , as follows : radiotherapy : a radiation dose of 45 gy was delivered to the rectum , perirectal tissues and draining lymph nodes , with 15 - mev photons and 3d conformal irradiation ( crt ) in 5 weekly sessions of 180 cgy for 5 weeks ; a further boost dose of 9 gy in five sessions and the same fraction size was delivered the following week , coned down to the rectum and to the mesorectal region , with 6 - mev photons and a 3d - crt dynamic technique based on a micromultileaf collimator . chemotherapy : oxaliplatin ( 60 mg / m2 , i.v. ) was delivered concurrently to radiotherapy on days 1 , 15 and 29 ; capecitabine ( 825 mg / m2 , per os ) was delivered daily throughout the radiotherapy course . all patients completed the scheduled chrt , and surgery was performed 48 weeks later . 
 [ 6 ] , as follows : grade 1 , complete regression with absence of residual cancer and fibrosis extending throughout the wall ; grade 2 , presence of residual cancer cells scattered among the fibrosis ; grade 3 , a higher number of residual cancer cells embedded in a inregressione neoplastica [ 10 ]  . 
la risonanza magnetica pesata in diffusione ( dw - rm ) potrebbe essere utile nel mostrare il tessuto neoplastico vitale , poich in grado di rilevare la restrizione della diffusibilit protonica presente nei tessuti ipercellulari con elevato rapporto nucleo - citoplasma [ 12 ]  . 
 quindi plausibile tentare una misurazione del volume relativo alliperintensit in dw - rm , diretta espressione del tessuto patologico , quale metodo per ottenere una volumetria funzionale . lobiettivo di questo studio quello di valutare la fattibilit in termini di riproducibilit ( accordo inter - osservatore ) della volumetria rm sia convenzionale ( vc ) , sia calcolata con dw - rm ( vdwi ) nel cancro del retto trattato con chemioradioterapia , nonch di comparare i due metodi . 
inoltre , stata valutata in via preliminare la correlazione di entrambe le volumetrie con il trg , al fine di valutare leventuale miglior grado di predittivit nella risposta tumorale . materiali e metodi pazienti quattordici pazienti ( et compresa tra 55 e 74 anni ; mediana 65 , 6 anni ) con diagnosi endoscopica e bioptica di neoplasia del retto sono stati inclusi retrospettivamente in questo studio . 
la stadiazione clinica e strumentale si basata su rm delladdome , radiografia ( rx ) o tomografia computerizzata ( tc ) del torace ed ecografia epatica in tutti i casi , e ecografia trans - rettale con trasduttore radiale in 12 : 3 pazienti sono stati inquadrati in stadio a di dukes , 1 in stadio b , 10 in stadio c . 
in base alla stadiazione tumorenodulo - metastasi ( tnm ) tutti i pazienti rientravano nelle categorie ct3 - t4n0 / + m0 e sono stati quindi sottoposti al seguente protocollo chemio - radioterapico pre - operatorio : radioterapia ( rt ) : stata somministrata la dose totale di 45 gy su retto , tessuto perirettale e linfonodi di drenaggio con fotoni da 15 mev e tecnica 3d conformazionale , con frazionamento di 1 , 8 gy per 5 sedute settimanali per un totale di 5 settimane . 
nella settimana successiva stato erogato un ulteriore boost con dose di 9 gy in 5 sedute , con lo stesso frazionamento , su retto e regione mesorettale con fotoni da 6 mev e tecnica 3d conformazionale cinetica con collimatore micromultilamellare ; chemioterapia : stato somministrato , in concomitanza alla rt , oxaliplatino ( 60 mg / m endovena ) nei giorni 1 , 15 e 29 e capecitabina ( 825 mg / m per os ) tutti i giorni , per tutta la durata della rt . 
 tutti i pazienti inclusi in questo studio hanno concluso il radiol med ( 2012 ) 117 : 11121124 1115 tensely fibrotic stroma ; grade 4 , large groups of cancer cells outgrowing fibrosis ; grade 5 , absence of regressive changes . patients with trg 12 were considered optimal responders and those with trg 35 nonoptimal responders . 
the overall pathological tumour volume was not analysed because it includes fibrotic and necrotic areas other than the viable tissue that was the subject of our evaluation . all patients gave written informed consent to the mri examination and analysis of imaging and pathological data . 
 for this retrospective observational study , a notification to the local ethics committee was performed in accordance with national laws . imaging all patients underwent mri evaluation before and 4515 days after the end of chrt ; the second mr examination was performed 1816 days before surgery . 
mr studies were performed using a 1.5 - t system ( signa excite hd , ge healthcare , milwaukee , wi , usa ) with an eight - channel phased - array coil . 
the imaging protocol consisted of highresolution t2 - weighted fast spin echo ( fse ) sequences in the sagittal plane , followed by the same sequence in the axial and coronaloblique planes oriented perpendicularly and parallel to the axial extension of the tumour in the rectal lumen , as previously described by other authors [ 13 ]  . 
 sequence parameters were time to repetition ( tr ) / time to echo ( te ) 4 , 600 / 105.6 ms ; matrix 288256 ; field of view ( fov ) 2424 cm ; thickness / gap 34 / 0 mm ; number of signal averages ( nsa ) 6 . 
other parameters were tr / te 3 , 675 / 119 ms , fov 4332 cm , slice thickness 4 mm without gap , matrix 128128 , six signal averages . 
se - dw - epi sequences were acquired in the axial plane by application in three orthogonal directions of a b - factor of 0 ( or reference images ) and 800 s / mm2 ( dw images ) in all patients . 
 two readers with different experience in mri ( a radiologist with 10 years experience in body imaging , and a resident ) independently evaluated lesion volume with the following methodology : tumour volume on conventional t2weighted images ( vc ) was calculated using commercially available software ( advantage windows , release 4.3 , ge healthcare , usa ) by manual segmentation of the lesion on each axial image in which it was visualised as rectal parietal protocollo e sono stati avviati alla chirurgia dopo 48 settimane . 
tutti i preparati istologici sono stati analizzati da un solo patologo che ha assegnato il trg secondo la classificazione di mandard [ 6 ] : grado 1 , completa regressione con assenza di residuo neoplastico e fibrosi largamente estesa ; grado 2 , presenza di cellule cancerogene residue sparse nel contesto fibroso ; grado 3 , maggior numero di cellule neoplastiche nel contesto di uno stroma intensamente fibrotico ; grado 4 , vasti agglomerati di cellule cancerogene predominanti sulla fibrosi ; grado 5 , assenza di regressione di malattia . 
 tutti i pazienti hanno firmato il consenso allesame rm ed al trattamento dei loro dati di imaging e anatomo - patologici ; inoltre per tali valutazioni retrospettive stata eseguita una notifica al comitato etico locale in accordo con le leggi nazionali . imaging tutti i pazienti sono stati sottoposti a valutazione con rm prima e dopo 4515 giorni dalla fine della chrt ; il secondo esame di rm stato effettuato 1816 giorni prima della chirurgia . 
tutti gli esami di rm sono stati effettuati usando un sistema ad alto campo da 1 , 5 t ( signa excite hd , ge healthcare , milwaukee , usa ) con bobina phased - array a 8 canali . 
il protocollo di imaging consisteva in una acquisizione t2 - fast spin echo ( fse ) sul piano sagittale seguita da acquisizioni t2 - fse sui piani assiale e coronale - obliquo orientati rispettivamente in maniera perpendicolare e parallela allestensione assiale del tumore nel lume del retto , come precedentemente descritto da altri autori [ 13 ] ; i parametri delle sequenze sono stati : tempo di ripetizione ( tr ) / tempo di eco ( te ) ( ms ) 4600 / 105 , 6 ; matrice 288256 ; campo di vista ( fov ) ( cm ) 2424 ; spessore / gap ( mm ) 34 / 0 ; numero di scansioni ( nsa ) 6 ; dimensione del pixel 0 , 80 , 9 m per la dwi stata utilizzata una sequenza spin echo ( se ) echo - planar imaging ( epi ) con applicazione di impulsi di radiofrequenza in serie di 90 e 180 con read - out eco - planare . 
1a - c segmentazione manuale della neoplasia nelle immagini t2 - pesate ( a , linea bianca ) , con successivo cutting ( b ) ripetuto per ciascuna immagine e estrapolazione automatica del volume ( c ) , come descritto nel testo . thickening isointense to nearby muscles . 
the extrapolation of volume from dw images ( vdwi ) was performed using a semiautomatic segmentation of each lesion defined as hyperintense relative to the background on the dw data set . 
 the same commercially available software was used by the two observers to manually cut out the lesion and segment the hyperintense tumour tissue using a subjective visual threshold ; the isolation process excluded lymph nodes from the volumetric analysis . 
in an attempt to avoid including inappropriate volume ( post - chrt hyperintensity of rectal wall , signal heterogeneity of prostatic adenomyoma ) , this step was performed using the t2 - weighted conventional imaging as a visual reference . 
 due osservatori con differente esperienza in rm ( un radiologo con dieci anni di esperienza in imaging body ed un medico in formazione ) hanno valutato indipendentemente il volume della lesione con la metodologia descritta di seguito . 
il volume tumorale sulle immagini t2 pesate convenzionali ( vc ) stato calcolato usando un software ( advantage windows , release 4.3 , ge healthcare , usa ) attraverso una segmentazione manuale della lesione su ogni immagine assiale in cui la neoplasia stata visualizzata come ispessimento parietale della parete rettale isointenso rispetto ai muscoli vicini . 
lo stesso software stato usato dai due osservatori per ritagliare manualmente la lesione e segmentare il tessuto tumorale iperintenso adoperando una soglia visiradiol med ( 2012 ) 117 : 11121124 1117 fig . 
 the application of a threshold using the axial dwi image as a reference allows for the segmentation of hyperintense tumour tissue and the next automatic tumoural segmentation , thanks to high - contrast resolution between tumour signal intensity and background . 
lapplicazione di una soglia utilizzando , come riferimento , una singola immagine assiale dw visualizzante la lesione consente la segmentazione del tessuto tumorale iperintenso e la successiva estrapolazione automatica del volume sulla mip , applicando un metodo di segmentazione di pixel - contiguity . 
the icc was also used to evaluate agreement between the two methods , and spearmans rank test was used to assess linear correlation between vc and vdwi with trg ; nonparametric tests ( signed - rank wilcoxon test and mannwhitney u test ) were used to compare vc and vdwi in the preand posttreatment setting because of the small number of patients , both in optimal and nonoptimal responders ( r ) , as well as to compare their volume changes ( rvc and rvdwi ) , respectively . 
for statistical evaluation , the statistical package for the social sciences ( spss 15.0 , chicago , il , usa ) was used . results table 1 summarises imaging and pathological staging and volumetry for the 14 patients . 
finally , posttreatment vc showed an rho = 0.597 ( p < 0.05 ) concordance with trg , whereas a more signifiva soggettiva ; il taglio escludeva dallanalisi volumetrica i linfonodi . 
inoltre , al fine di evitare inclusioni di volume non congruo ( iperintensit post - attinica della parete rettale , disomogeneit di segnale del lobo medio della prostata in caso di ipertrofia ) , tale operazione di taglio stata effettuata utilizzando come riferimento visivo limaging t2 - pesato . 
lo stesso test stato utilizzato anche per valutare laccordo fra i due metodi e lo spearman rank test stato adoperato per valutare la correlazione lineare tra vc e vdwi con il trg . 
per confrontare vc , vdwi e le loro modificazioni relative rvc e rvdwi pree post - chrt sono stati usati test non parametrici ( signed - rank wilcoxon test e test di mannwhitney ) , visto lesiguo numero di pazienti . 
per i calcoli statistici stato usato il software commerciale statistical package for social sciences ( spss 15.0 , chicago , ill )  . risultati la stadiazione mediante imaging , nonch quella anatomopatologica e le volumetrie sono riportate nella tabella 1 . 
many reports in the literature suggest that a pathological downstaging , in particular , is related to improved local control and disease - free and overall survival [ 2 ]  . 
however , one pitfall in establishing downstaging is the spurious comparison laccordo inter - osservatore per vc e vdwi stato rispettivamente di 0 , 977 [ 95% intervallo di confidenza ( ci ) 0 , 954 0 , 989 ] e 0 , 956 ( 95% ci 0 , 9050 , 980 )  . 
laccordo tra vc e vdwi nelle indagini pre - chrt e post - chrt stato di 0 , 964 ( 95% ci 0 , 8960 , 988 ) e 0 , 271 ( 95% ci - 0 , 2670 , 686 )  . una significativa riduzione del volume tumorale stata rilevata con entrambi i metodi ( tabella 2 )  . 
in particolare , la letteratura ha dimostrato che un downstaging patologico correla con il controllo della malattia locale e la sopravvivenza libera da malattia e complessiva [ 2 ]  . 
lefficacia della chrt potrebbe essere meglio valutata con la medesima tecnica di imaging eseguita nei due tempi , posto che i dati post - chrt abbiano una stretta correlazione con i rilievi anatomo - patologici . 
indispensabile , inoltre , una elevata riproducibilit della metodica . nella pratica clinica corrente il sistema per valutare la risposta alla chrt rimane ancora losservazione delle modificazioni del parametro t e del parametro n . 
 la valutazione quantitativa del volume neoplastico considerata pi accurata rispetto agli altri metodi di valutazione del parametro t , nello stabilire la risposta alla terapia neo - adiuvante [ 15 , 16 ]  . 
molti autori , anche tenendo conto dellimportanza del trattamento radiante nella terapia integrata di questi tumori , hanno utilizzato la rm per il calcolo del volume neoplastico nei tumori del retto , usando differenti approcci come la segmentazione manuale della lesione o semplicemente moltiplicando le dimensioni dei tre maggiori assi lesionali . 
la riduzione della massa in percentuale stata indagata quale possibile marker di risposta alla chrt [ 11 , 15 ] tanto nel carcinoma rettale quanto nelle neoplasie ginecologiche e nei tumori del distretto testa - collo [ 17 ]  . 
alcuni autori hanno cos documentato che il volume neoplastico evidenziato dalla rm dopo chrt era quasi sempre maggiore di quanto poi accertato sul pezzo anatomico [ 7 ]  . dimostrato che il trg correla significativamente con il controllo locale e sistemico della malattia [ 2 ] : questo parametro interessante , quindi , per una correlazione con una metodica di imaging che consenta di discriminare tra tessuto vitale e fibrosi . 
la vc ( tondi bianchi ) non correla con lo score di regressione tumorale ( linea tratteggiata ) , mentre la vdwi ( quadratini neri ) correla significativamente con il trg ( linea nera continua )  . between clinical and imaging - based staging before chrt and pathological evaluation of the surgical specimen after chrt . 
the effectiveness of chrt might be best evaluated with the same imaging technique performed in both settings , provided that post - chrt data show a strong correlation with pathological staging . 
thanks to its multiplanar capabilities , mri allows reliable outlining of a target volume for radiotherapy . a quantitative determination of tumour volume by mri is considered more accurate than t staging for assessing treatment response [ 15 , 16 ]  . 
many investigators demonstrated that ypt ( pathological t parameter in patients undergoing chrt ) does not correlate with prognosis after neoadjuvant therapy in rectal cancer [ 17 ] , whereas trg seems to be an important prognostic factor [ 6 ]  . 
a higher concordance can be expected vante pre - chirurgica , lo ypt ( ovvero lo stadio patologico t nei casi trattati con chrt ) non correli con la prognosi [ 17 ] , mentre il trg sembra essere un importante fattore prognostico [ 6 ]  . 
di conseguenza , in questo studio abbiamo tentato di identificare un parametro radiologico che possa correlare con il trg , utilizzando una acquisizione funzionale in rm al fine di calcolare il volume tumorale . 
in tale acquisizione il segnale espressione della cellularit tissutale , essendo la dw - rm capace di evidenziare il tessuto neoplastico vitale [ 18 ] : lelevata cellularit determina una restrizione della diffusibilit protonica e produce unarea di iperintensit rispetto alla diffusa ipointensit del background . 
in precedenza , il dato volumetrico era stato riportato sempre come valore ottenuto in consenso fra due osservatori [ 11 , 15 , 19 ] e una valutazione della riproducibilit del parametro quantitativo mediante accordo interosservatore non mai stata riferita in letteratura . 
una elevata concordanza per il vc in realt era attesa , data la semplicit della metodologia di segmentazione manuale immagine - per - immagine del tessuto neoplastico , con i margini tracciati cos come evidenti sulle immagini t2 - dipendenti . 
daltro canto , lestrapolazione del vdwi prevedeva alcuni passaggi , come la scelta della soglia e leliminazione preliminare , mediante cutting , dei tessuti extra - rettali , sostanzialmente osservatore - dipendenti . 
 on the other hand , we assessed vdwi semiautomatically , and some steps , such as choice of threshold and preliminary cutting of extrarectal tissue , are observer dependent in this case . 
the certainty that the hyperintensity visualised in dw images and used to extrapolate the volume corresponded to the tumour site was inferred by using the t2 - weighted images as a visual reference in the cutting step . 
in particular , the relatively lower rvdwi to rvc can be explained with the presence of hyperintensity due to t2 shine - through artefacts of necrotic tumour areas , mostly in treated lesions . 
inoltre , gli artefatti dal t2 - shine - through e suscettibilit magnetica sullinterfaccia aria - parete rettale potevano , comportare rispettivamente problemi di sovra e sottostima dei volumi neoplastici . 
in particolare , il valore pi basso di rvdwi rispetto a quello di rvc pu esser spiegato con la presenza di iperintensit dovute allartefatto da t2 - shine - through delle aree di colliquazione tumorale , specie dopo trattamento chrt ; infatti , la presenza di iperintensit non correlabile a restrizione della diffusione ma a persistenza del segnale t2 ( lartefatto da t2 - shinethrough , appunto ) poteva determinare una sovrastima del vdwi post - chrt con conseguente sottostima delle modificazioni prodotte dalla terapia adiuvante su tale parametro . nondimeno , abbiamo ottenuto nel presente studio una elevata riproducibilit del vdwi , probabilmente a causa dellelevata risoluzione di contrasto tra liperintensit del tessuto neoplastico vitale ed il background nelle immagini dw . 
i problemi tecnici in precedenza citati potrebbero essere ovviati confrontando le immagini dw con le corrispondenti mappe dellapparent diffusion coefficient ( adc ) , al radiol med ( 2012 ) 117 : 11121124 1122 fig . 
t2 - weighted magnetic resonance image ( a ) shows pathological hypointense tissue ( black arrow ) that involves the left portion of the mesorectal fascia , whereas in diffusion - weighted imaging , only a focal hyperintensity ( white arrow ) is detected at the same site ( b )  . 
limmagine t2 - pesata ( a ) mostra tessuto ipointenso patologico ( freccia nera ) che raggiunge la porzione sinistra della fascia mesorettale , mentre nella immagine in dwi si rileva soltanto una focale iperintensit ( freccia bianca ) nella medesima sede ( b ) ; il reperto anatomo - patologico ( c ) dimostra la presenza di tessuto fibroso con alcuni gruppi neoplastici isolati nel suo contesto ( trg = 3 )  . nevertheless , we obtained a higher reproducibility of vdwi , probably due to the high contrast resolution between the hyperintensity of viable tumour tissue and the background in dw images . 
the technical problems addressed above could be overcome by matching dw images with the corresponding apparent diffusion coefficient maps to manually rule out pseudohyperintensities , and by changing patient position in the bore in order to move residual air to the opposite position . 
 the high level of reproducibility prompted us to use the semiautomatically extrapolated volume by dwi data set in the same way as the volumes obtained with conventional methods from the t2 - weighted sequences [ 7 , 15 ]  . 
in prechrt evaluations , we found no significant differences between conventional and dwi - based volumes for such lesions , whereas after therapy , vc was always higher than vdwi . 
these results might be due to the changes occurring in neoplastic tissue after chrt , with the increase in fibrotic fine di escludere manualmente le false iperintensit ovvero cambiando il posizionamento dei pazienti nel bore al fine di ottenere una dislocazione dellaria rettale residua in sede opposta a quella della lesione da studiare . lelevata riproducibilit ottenuta ci ha consentito di utilizzare lestrapolazione semi - automatica dei volumi dai data - set dw allo stesso modo dei volumi calcolati con metodo convenzionale sulla base delle immagini t2 - dipendenti [ 7 , 15 ]  . 
nelle valutazioni eseguite nei casi pre - chrt non stata riscontrata alcuna differenza tra vc e vdwi , mentre nelle lesioni valutate dopo chrt , vc stato sempre pi elevato di vdwi . 
dopo chrt , quindi , vc potrebbe sovrastimare il volume tumorale , a causa dellimpossibilit nelle immagini t2 - dipendenti di distinguere la fibrosi dal tessuto vitale radiol med ( 2012 ) 117 : 11121124 1123 component that sustains lesion volume , whereas the cellular component shrinks or disappears . 
 despite the lack of correlation between vc and trg , postchrt vc seems to discriminate optimal from nonoptimal responders , as does vdwi ( p < 0.05 for both the methods ) ( table 3 ) , as previously assessed by kim et al . 
however , trg is currently considered more important than other staging parameters for predicting patient outcomes [ 2 ] , and the significant correlation demonstrated in our study between vdwi and trg appears promising in the attempt to find a useful presurgical imaging marker of response to chrt . finally , we are aware of some limitations of our study , such as the small number of patients , which could lead to overestimation of interobserver agreement of dwi , and the lack of any survival end - point , which does not allow assessment of the predictive value of dwi volume determination in terms of prognosis . 
mr volumetry could be one of these biomarkers ; in particular , vdwi could represent a further step towards an imaging technique in which morphological / morphometric parameters can be combined with functional parameters . 
 however , further studies are needed to verify the correlation between parameters obtained with the methodology described in this paper and biological and pathological findings , as well as to correlate mr volumetry , especially vdwi , with patient outcome . 
al contrario , il tessuto vitale iperintenso nelle immagini pesate in diffusione , mentre la fibrosi non mostra un segnale significativo , di conseguenza il vdwi potrebbe essere pi simile al reale volume tumorale vitale . 
nonostante la mancanza di correlazione tra vc e trg , il vc post - chrt sembra discriminare gli optimal dai non - optimal responder tanto quanto vdwi ( p < 0 , 05 per entrambi i metodi ) ( tabella 3 ) , come gi evidenziato da altri autori [ 15 ]  . 
nessuna correlazione , inoltre , era stata dimostrata fra la volumetria dopo trattamento e la risposta tumorale : ci risultava confermato da un altro studio recente [ 11 ]  . 
al contrario , il trg attualmente considerato un importante parametro predittivo di outcome dei pazienti trattati con chrt [ 2 ] , e la significativa relazione evidenziata in questo lavoro tra vdwi e trg da considerare molto promettente , nella prospettiva di selezionare un utile indicatore pre - chirurgico di risposta nel trattamento neo - adiuvante . infine , siamo consapevoli di alcune limitazioni del nostro studio , come il basso numero di pazienti esaminati , che potrebbe determinare una sovrastima dellaccordo interosservatore , nonch della mancanza di una valutazione in termini di sopravvivenza , che ovviamente non consente deduzioni circa il significato prognostico del vdwi . in conclusione , il valore dei predittori di risposta alla chrt rappresenta ad oggi una sfida . 
la volumetria con rm si inserisce tra questi biomarcatori ed in particolare il vdwi potrebbe rappresentare un ulteriore passo verso un imaging nel quale elementi di valutazione morfologici / morfometrici possano essere associati a parametri di tipo funzionale ; tali valutazioni nel complesso potrebbero migliorare sia il planning chirurgico che il successivo management di questi pazienti . 
ulteriori studi quindi sono auspicabili al fine di verificare il legame tra i parametri ottenuti con la metodologia descritta nel presente lavoro e quelli biologici e anatomo - patologici , nonch per correlare la volumetria in particolare con vdwi alla prognosi di questi pazienti . 
chen , tel : + 86 - 21 - 64370045 - 665728 , fax : + 86 - 21 - 64661351 , e - mail : chenkeminrj@yahoo.cn received : 23 september 2011 / accepted : 26 october 2011 / published online : 28 june 2012 springer - verlag 2012 abstract purpose . 
the purpose of our study was to retrospectively assess imaging features of computed tomography ( ct ) and clinical characteristics of children with solid pseudopapillary tumours ( spts ) of the pancreas in comparison with those of spts in adults . 
 spt diagnosis should always be considered when a large pancreatic mass with typical imaging is found in a child , especially in adolescent girls . keywords solid pseudopapillary tumour pancreas computed tomography paediatrics riassunto obiettivo . 
18 pazienti sono stati classificati come bambini ( et 18 anni ) , e 68 pazienti sono stati classificati come adulti ( et > 18 anni ) secondo let alla diagnosi . 
la diagnosi di spt dovrebbe essere considerata quando viene ritrovata una massa pancreatica di grandi dimensioni con le tipiche caratteristiche di immagine , specialmente in adolescenti femmine . parole chiave tumore solido pseudopapillare pancreas tomografia computerizzata pediatria radiol med ( 2012 ) 117 : 12421249 1243 introduction ct technique solid pseudopapillary tumour ( spt ) of the pancreas was first reported in 1933 [ 1 ] , well described by frantz in 1959 [ 2 ] , and finally widely accepted as an entity by the world health organization ( who ) in 1996 . 
imaging features and clinical characteristics of spt in children are discussed to help radiologists provide a more confident diagnosis . materials and methods patient selection the authors institutional review board approved this retrospective study , and the requirement for informed consent was waived . 
there were 18 children in the paediatric age group ( mean age , 15.1 years ; range , 1118 years ) and 68 in the adult age group ( mean age , 36.2 years ; range , 1967 years )  . 
there were 14 male patients with a mean age of 39.4 ( range , 1567 ) years and 72 female patients with a mean age of 30.3 ( range , 1158 ) years . available clinical manifestations , as well as surgical and pathology reports , were reviewed for each patient . 
 twelve patients underwent 4 - slice , 40 16 - slice , and 34 64 - slice mdct scan ( lightspeed 4 , 16 , 64 ; ge medical systems , milwaukee , wi , usa )  . 
after fasting for at least 4 h , patients were administered 500800 ml of water 30 min prior to the study and an additional 250300 ml of water immediately prior to the study to achieve adequate distension of the stomach and duodenuall patients were given nonionic iodinated contrast material ( omnipaque 300 mg i / ml , ge healthcare ) administered with a power injector ( ulrich medical , germany ) at a rate of 2.53.5 ml / s through an 18 - gauge catheter placed in an antecubital vethe volume of contrast material delivered was 1.52 ml / kg body weight . 
thirty - two patients underwent triple - phase ct during the unenhanced , arterial , pancreatic and hepatic venous phases , whereas 54 patients underwent dual - phase ct during the unenhanced , pancreatic and hepatic venous phases . 
items included in the image analysis were location ( head , neck , body or tail ) , shape ( round , oval or lobulated ) , encapsulation ( present or absent ) , calcifications ( present or absent ) , existence of solid and cystic components and fraction of tumour composed of solid versus cystic material ( greater than or less than 50% solid )  . 
internal attenuation characteristics of the tumour were compared with those of the surrounding pancreas and were described as follows : hypo - , isoor hyperattenuation on unenhanced pancreatic - phase images ; enhancement pattern ( peripheral or complete ) ; dilatation of the pancreatic duct ; atrophy of pancreatic parenchyma . 
in the paediatric age group , three were boys , with a male - to - female ratio of 1 : 5 , and mean age at diagnosis was 15.1 ( range , 1118 ) years . 
conservative surgery in the paediatric age group was employed in seven patients , including a spleen - preserving distal pancreatectomy in four , a segment radiol med ( 2012 ) 117 : 12421249 pancreatectomy in one and local tumour resection in two . 
 radical surgery was performed in 11 paediatric patients , including distal pancreatectomy without splenic preservation in four , whipples operation in four and concurrent resection of other organs in three . 
all 18 paediatric patients were alive with no evidence of disease recurrence or distant metastasis during follow - up . imaging features ct features observed in paediatric and adult spts are summarised in table 2 . 
no significant differences in imaging features were observed between age groups with respect to location , shape , encapsulation , composition , attenuation , calcifications and enhancement grade and pattern . 
calcification was noted in 17 adult patients ( 17 / 68 , 25% )  . according to mdct images , tumours were divided into three types by density , namely , cystic , solid or solidcystic component ( mixed )  . 
seventeen cases manifested early peripheral heterogeneous enhancement with progressive fill - in on dynamic examination after contrast material administration , 16 with a lower attenuation but one isoattenuation compared with the density of adjacent normal pancreas during the pancreatic phase . 
although there were no marked differences in the prevalence of parenchymal atrophy or pancreatic ductal dilatation between the two groups , all spts showed low prevalence of associated parenchymal atrophy ( 9% ) and pancreatic duct dilatation ( 10% )  . 
spt invasion to adjacent organs or tissues , including the spleen ( n = 4 ) , duodenum ( n = 3 ) , kidney ( n = 1 ) , vessel encasement or invasion ( n = 8 ) and liver metastasis ( n = 1 ) was revealed . 
furthermore , to the authors knowledge , there is no prior report comparing imaging features in adults and children . pancreatic tumours are quite rare in children , with < 0.2% of malignant paediatric deaths [ 10 ]  . 
 [ 15 ] suggested that the female preponderance may be less in paediatric patients , which does not agree with other reports [ 4 , 9 , 16 ] and the fact that 15 / 18 paediatric patients in our study were girls . 
however , some authors reported that in children , the body and tail of the pancreas are more frequently affected ( 64% ) than the head [ 5 ]  . 
a unenhanced ct scan shows an oval , mixed , neoplas b scan obtained during the pancreatic phase shows early , moderate , peripheral , heterogeneous enhancement of the solid component . 
d limmagine coronale , ottenuta in fase pancreatica , mostra dilatazione del dotto pancreatico ( freccia ) ed atrofia parenchimale a monte della massa localizzata nel corpo del pancreas . capsulated mass with varying solid and cystic components , often with peripheral contrast enhancement corresponding to the fibrous pseudocapsule . 
these cases and other reports [ 7 , 9 ] in the literature suggest that imaging findings of spt in children are highly similar to those in the larger published series , which described mostly adult patients [ 18 , 19 ]  . 
 familiarity with the characteristic ct appearances and clinical characteristics of spts in children will help radiologists make a more confident diagnosis . the criterion for malignant spt has not yet been firmly established . 
limited data show spt to have the best prognosis among the paediatric pancreatic malignancies , and several studies show excellent survival and high cure rates with complete surgical resection [ 5 , 16 , 17 ]  . 
although our study is one of the largest clinical and pathological studies to date , consistent with prior reports [ 23 ] , the malignancy potential of spt cannot be predicted before surgery by age , sex and tumour size . 
there are no well - known tumour markers for aggressive behaviour . the low - grade malignancy of this tumour and the fact that the mass is usually surrounded by a dense fibrous capsule led some surgeons to perform simple enucleation of the neoplasm , especially in children [ 12 , 14 ]  . 
given the limited number and indolent course of these tumours , little is known about the natural radiol med ( 2012 ) 117 : 12421249 1249 course of the disease or the risk factors for recurrence . 
from october 2006 to november 2009 , 48 patients with non - insulin - dependent diabetes mellitus ( dm ) and an indication for percutaneous revascularisation of the femoropopliteal arteries were randomly assigned to treatment with angioplasty or cryoplasty . 
da ottobre 2006 a novembre 2009 , 48 pazienti affetti da diabete mellito con indicazione ad intervento di rivascolarizzazione percutanea dellasse femoro - popliteo sono stati assegnati in maniera randomizzata al trattamento mediante crioplastica ed angioplastica . 
langioplastica convenzionale risulta pi efficace della crioplastica nel trattamento delle lesioni steno - ostruttive del distretto femoro - popliteo in pazienti diabetici , con migliori risultati immediati ed a medio e lungo termine . radiol med ( 2012 ) 117 : 11761189 1177 keywords cryoplasty angioplasty diabetes mellitus angiography parole chiave crioplastica angioplastica diabete mellito angiografia introduction introduzione diabetes mellitus ( dm ) is a metabolic disease in which alterations appear on the walls of vessels at various levels , and especially small vessels such as the coronaries and arteries of the lower limbs [ 1 ]  . 
in consideration of the higher prevalence of diabetic foot ulcers and critical limb ischaemia ( cli ) , diabetic patients have a five - fold higher risk of amputation and a ten - fold higher mortality rate compared with normoglycaemic patients [ 2 ]  . 
of note , dm has been identified as an independent risk factor for recurrent occlusive disease , with reduced patency and higher rates of restenosis after percutaneous or surgical revascularisation procedures on the infrainguinal arteries [ 4 , 5 ]  . 
despite the safety and versatility of such techniques , results of endovascular treatments for percutaneous angioplasty ( pta ) of atherosclerotic lesions of the femoropopliteal arteries remain mediocre , with patency rates at 12 months ranging from 40% to 60% [ 68 ]  . 
 the low long - term primary patency rate and the high rate of repeat interventions , mainly due to restenosis caused by intimal hyperplasia , has prompted a search for alternative techniques such as laser - assisted angioplasty , covered stentgrafts , brachytherapy and cryoplasty [ 912 ]  . 
huge interest has developed in particular around cryoplasty owing to its potential to combine mechanical plaque destruction through balloon inflation with freezing of the vessel wall to reduce local inflammation and induce cell apoptosis [ 1315 ]  . 
to date , few studies have evaluated the efficacy of cryoplasty for treating stenoticocclusive lesions of the femoropopliteal arteries [ 1618 ] , in particular , in comparison with conventional angioplasty [ 1921 ]  . 
in considerazione dellalta prevalenza nel piede diabetico di ulcere e ischemia critica degli arti ( cli ) , i pazienti diabetici presentano un rischio 5 volte pi elevato di amputazione e 10 volte pi alto di mortalit rispetto ai pazienti normoglicemici [ 2 ]  . 
 interessante notare che il dm stato identificato come un fattore di rischio indipendente di patologia occlusiva ricorrente con una diminuzione della perviet vascolare e tassi pi alti di restenosi dopo le procedure di rivascolarizzazione percutanea o chirurgica delle arterie infrainguinali [ 4 , 5 ]  . 
nonostante la loro sicurezza e versatilit , i risultati dei trattamenti endovascolari di angioplasti ca percutanea di lesioni aterosclerotiche del distretto femoro - popliteo restano mediocri , con tassi di perviet a 12 mesi compresi tra il 40% e il 60% [ 68 ]  . 
la bassa perviet primaria a lungo termine e lalto tasso di ritrattamento , principalmente a causa di restenosi da iperplasia intimale , ha spinto alla ricerca di tecniche alternative , quali angioplastica laser assistita , impiego di stent ricoperti , brachiterapia e crioplastica [ 912 ]  . 
enorme interesse si sviluppato particolarmente attorno alla crioplastica , per la sua potenzialit di associare leffetto meccanico di distruzione della placca , mediante il gonfiaggio del palloncino , al congelamento della parete vasale , in grado di ridurre i fenomeni di flogosi locale ed indurre apoptosi cellulare [ 1315 ]  . 
attualmente sono pochi gli studi che hanno valutato lefficacia della crioplastica nel trattamento delle lesioni steno - ostruttive del distretto femoro - popliteo [ 1618 ] in particolare a confronto con langioplastica convenzionale [ 1921 ]  . 
 scopo del nostro lavoro confrontare la crioplastica e langioplastica nel trattamento di lesioni steno - ostruttive del distretto femoro - popliteo in pazienti diabetici , valutando la perviet ed il run - off distale immediati e a medio e lungo termine . 
 the study protocol was evaluated and approved by the ethics committee ; patients enrolled were informed of their random allocation to either treatment group and of the risks and possible complications of the procedures and signed a valid informed consent for most patients had metabolic syndrome with associated dm ( n = 48 ) , hypertension ( n = 39 ) and dyslipidaemia ( n = 27 ) ; 16 patients were smokers , two were receiving dialytic treatment for chronic renal insufficiency and five had a history of myocardial infarction . 
inclusion criteria were dm and peripheral atherosclerotic disease with severe claudication or cli ( rutherford stages 2 - 6 ) ; haemodynamically significant stenosis ( 70% ) or occlusion of the superficial femoral artery ( sfa ) and / or popliteal artery ( pa ) as assessed by preliminary colour doppler ultrasound ( cdus )  . 
we excluded patients with a history of severe allergy or hypersensitivity to contrast material , intolerance to aspirin and / or clopidogrel , coagulation disorders , acute ischaemia of the lower limbs , buergers disease , deep vein thrombosis , loss of infected tissue and absence of outflow . the purpose of the study was to evaluate the effectiveness of cryoplasty for treating stenotic - occlusive lesions of the femoropopliteal arteries by comparing it with the standard treatment ( pta ) in terms of the following parameters : technical success and postprocedural distal run - off , degree of restenosis and distal run - off at 6 and 12 months . 
clinically , patients were subdivided according to the leriche - fontaine classification : 10 / 24 in the cryo group 11 / 24 in the pta group were stage iib ( claudication distance < 200 m ) ; 10 / 24 in the cryo group and 10 / 24 in the pta group were stage iii ( rest pain ) and 4 / 24 in the cryo group and 3 / 24 in the pta group were stage iv ( trophic lesions )  . 
most treatments were performed for stage a and b lesions according to the transatlantic inter - society consensus ( tasc ) classification , with preoperative stenosis between 60% and 90% . 
lesions were generally concentric , with moderate - to - severe calcifications . endovascular procedures all patients were premedicated with aspirin ( 100 mg / daily ) materiali e metodi nel periodo compreso tra ottobre 2006 e novembre 2009 un totale di 48 pazienti affetti da dm ( 27 maschi e 21 femmine ) con et media di 7010 anni che hanno avuto indicazione ad intervento di rivascolarizzazione percutanea dellasse femoro - popliteo per arteriopatia ostruttiva cronica periferica ( aocp ) sono stati assegnati in maniera randomizzata al trattamento mediante crioplastica ( gruppo cryo : 24 pazienti ) o angioplastica ( gruppo pta : 24 pazienti )  . 
 il protocollo di studio stato valutato ed approvato dal comitato etico ; i pazienti arruolati sono stati informati dellassegnazione casuale degli stessi ad una delle due tipologie di trattamento , dei rischi e possibili complicanze associate ed hanno firmato un valido consenso informato . 
 la maggior parte dei pazienti presentava sindrome metabolica con associazione di dm ( 48 pazienti ) , ipertensione ( 39 pazienti ) e dislipidemia ( 27 pazienti ) ; 16 pazienti erano fumatori , 2 erano in trattamento dialitico per insufficienza renale cronica , 5 pazienti avevano avuto un pregresso infarto miocardico . 
i criteri di inclusione erano : dm e malattia aterosclerotica delle arterie periferiche con un quadro di grave claudicatio o cli ( stadi rutherford da 2 a 6 ) ; stenosi emodinamicamente significativa ( 70% ) o occlusione dellarteria femorale superficiale ( afs ) e / o dellarteria poplitea ( ap ) , come documentata da un esame diagnostico preliminare ( eco - color doppler )  . 
 sono stati esclusi dallarruolamento pazienti con una storia di grave allergia o ipersensibilit al mezzo di contrasto , intolleranza allaspirina e / o clopidogrel , disturbi della coagulazione , ischemia acuta degli arti inferiori , malattia di buerger , trombosi venosa profonda , perdita di tessuto infetto e assenza di out flow . lobiettivo dello studio era valutare lefficacia della crioplastica nel trattamento delle lesioni steno - ostruttive del distretto femoro - popliteo mediante confronto col trattamento standard , langioplastica convenzionale , analizzando i seguenti parametri : successo tecnico e run - off distale post - procedurale , grado di restenosi e run - off distale a 6 e 12 mesi . 
clinicamente i pazienti sono stati ripartiti secondo la classificazione di leriche - fontaine : 10 / 24 pazienti nel gruppo cryo e 11 / 24 nel gruppo pta erano in stadio iib ( claudicatio alla marcia con autonomia < 200 m ) ; 10 / 24 pazienti nel gruppo cryo 10 / 24 nel gruppo pta erano in stadio iii ( dolore a riposo ) e 4 / 24 pazienti nel gruppo cryo 3 / 24 nel gruppo pta erano in stadio iv ( lesioni trofiche )  . 
a polarcath ( polarcath peripheral dilatation system , boston scientific , natick , ma , usa ) balloon was positioned at the stenosis to perform cryoplasty ( b )  . 
il controllo angiografico finale documenta la buona riuscita della procedura con ripristino di un buon calibro vasale ( c )  . and clopidogrel ( 75 mg / daily ) for at least 3 days before the procedure . 
patients who were taking metformin as an antidiabetic agent were adequately hydrated and advised by the specialist to momentarily modify their therapy ( with insulin or sulfonylurea ) , as recommended by guidelines of the european society of urogenital radiology ( esur ) [ 22 ]  . 
after local anaesthesia , an antegrade approach was used in 20 / 24 patients , a retrograde approach with crossover technique in 3 / 24 and a left humeral approach in 1 / 24 . 
two polarcath balloons of varying size ( from 3.4 mm in diameter 40 mm in length to 7 mm in diameter 60 mm in length ) were used depending on the diameter of the vessel of origin menti sono stati eseguiti per lesioni di stadio a e b secondo la classificazione tasc con stenosi pre - operatoria variabile tra il 60% ed il 90% . 
le lesioni erano generalmente concentriche con presenza di calcificazioni di grado variabile da moderato a severo . procedure endovascolari tutti i pazienti sono stati premedicati con aspirina ( 100 mg / die ) e clopidogrel ( 75 mg / die ) per almeno 3 giorni prima della procedura . 
i pazienti che stavano assumendo metformina come trattamento per il diabete sono stati adeguatamente idratati ed stata momentaneamente modificata dallo specialista la terapia ( con insulina o sulfanilurea ) , come determinato dalle linee guida della societ europea di radiologia urogenitale ( esur ) [ 22 ]  . 
previa anestesia locale in 20 / 24 pazienti stato effettuato approccio anterogrado , in 3 / 24 approccio retrogrado con tecnica di cross - over e in 1 / 24 accesso per via omerale sinistra . 
in 3 casi stato impiegato introduttore 7 1180 radiol med ( 2012 ) 117 : 11761189 and lesion extension , with an average of two inflations per lesion . polarcath is a peripheral dilatation system , which comprises an over - the - wire device , with a double - lumen balloon catheter made of pebax ( atochem inc , pa , usa ) and an inflation system consisting of a microprocessor unit and nitrous oxide cartridge . 
the cryoplasty catheter is made up of three layers ( inner , middle and outer ) and its fluoroscopic visibility is ensured by the presence of radiopaque marker in the middle layer . 
balloon inflation is attained by a specially designed device releasing liquid nitrogen from a high - pressure cartridge through the catheter lumen and into a lowpressure balloon chamber , where the liquid changes state to gas and expands in volume . 
 rapid expansion of the gas volume inflates the balloon and produces a rapid drop in temperature , thereby effectively cooling the balloon surface and the adjacent vessel wall to - 10c , and the inflation pressure gradually reaches 8 at the cooling period between active inflation and passive deflation ranges from 26 to 30 s . 
the technique aims at improving the immediate and long - term results by cooling the atherosclerotic plaque and its elastic components and obtaining more uniform and less traumatic vessel dilatation , which results in better plaque remodelling and fewer wall dissections [ 15 , 23 ]  . 
 several studies have shown that temperatures of 10c create a dehydration effect through a change in the osmotic forces acting in the area around the catheter [ 24 , 25 ]  . 
the procedure is thought to induce cell apoptosis ( programmed cell death ) rather than necrosis of the remaining endothelium and smooth muscle cells of the vessel media and may therefore result in less infiltration of inflammatory cells , less intimal hyperplasia and consequently less restenosis [ 24 , 25 ]  . 
patients were hospitalised overnight and discharged the following day with a prescription for dual antiplatelet therapy ( 75 mg / daily clopidogrel and 100 mg / daily aspirin ) for 6 weeks , and only aspirin or clopidogrel indefinitely thereafter . angioplasty treatment all pta were performed in the angiography room with constant arterial pressure and electrocardiographic monitoring . 
superata la lesione steno - ostruttiva mediante guida idrofilica 0 , 035 o guida in acciaio 0 , 014 stato posizionato il sistema polarcath ( polarcath peripheral dilatation system , boston scientific , natick , ma , usa ) in corrispondenza della sede da trattare . 
 sono stati impiegati palloni polarcath di varie dimensioni ( da 3 , 4 mm di diametro40 mm di lunghezza a 7 mm di diametro60 mm di lunghezza ) a seconda del diametro del vaso di origine e dellestensione della lesione , con una media di due gonfiaggi per sede trattata . il polarcath consiste in un sistema di dilatazione periferica , che comprende un device over - the - wire , con catetere a palloncino a doppio lume in pebax ( atochem inc , pa , usa ) e un sistema di gonfiaggio costituito da un microprocessore ed una cartuccia di protossido di azoto . 
il catetere da crioplastica formato da tre strati ( interno , medio ed esterno ) e la sua visibilit fluoroscopia resa possibile grazie alla presenza di marker radiopachi nello strato intermedio . 
il gonfiaggio del palloncino realizzato da un apposito apparecchio che libera il protossido di azoto liquido , attraverso una cartuccia ad alta pressione , nel lume del catetere e quindi nella camera del pallone a bassa pressione , dove il liquido cambia di stato , da liquido a gassoso , ed espande il suo volume . 
la rapida espansione del volume di gas gonfia il palloncino e produce una rapida diminuzione temperatura , cos si realizza efficacemente il raffreddamento della superficie del pallone e della parete del vaso adiacente a - 10c , mentre la pressione di gonfiaggio raggiunge gradualmente 8 at il periodo di raffreddamento tra gonfiaggio attivo e sgonfiaggio passivo varia da 26 a 30 s . 
la tecnica mira ad ottenere migliori risultati immediati ed a lungo termine grazie al processo di raffreddamento del placca aterosclerotica e delle sue componenti elastiche e cerca di ottenere una pi uniforme e meno traumatica dilatazione del vaso , con conseguente migliore rimodellamento della placca e riduzione della quota di dissezioni parietali [ 15 , 23 ]  . 
 diversi studi hanno dimostrato che a temperature di 10c si crea una disidratazione mediante un cambiamento nelle forze osmotiche che intervengono nel campo intorno al catetere [ 24 , 25 ]  . 
la procedura sembra indurre lapoptosi cellulare ( morte cellulare programmata ) , piuttosto che la necrosi dellendotelio rimanente e delle cellule muscolari lisce della media e potrebbe quindi comportare un minor richiamo di cellule dellinfiammazione , minore risposta di iperplasia neo - intimale e , di conseguenza , riduzione della comparsa di restenosi vascolare [ 24 , 25 ]  . 
poich il periodo di tempo e la pressione del catetere da crioplastica non pu essere regolata da parte delloperatore , per ottenere buoni risultati si prevedono almeno due sessioni di inflazione lo stesso pallone , soprattutto quando le lesioni siano particolarmente resistenti . al termine della procedura , lemostasi stata ottenuta radiol med ( 2012 ) 117 : 11761189 1181 cases , 6 f in five and 5 f in 16 . 
patients were hospitalised overnight and discharged the following day with a prescription for dual antiplatelet therapy ( 75 mg / daily clopidogrel and 100 mg / daily aspirin ) for 6 weeks and only aspirin or clopidogrel indefinitely thereafter . definitions immediate technical success was defined as residual stenosis not exceeding 30% of vessel diameter . 
lesions requiring additional conventional balloon angioplasty owing to a suboptimal result or requiring stent placement due to vessel dissection were classified as failures and were not considered in the follow - up . 
haemodynamic success was defined as the presence of stenosis < 30% at cdus with a finding , at the target site , of a peak systolic velocity ( psv ) < 150 cm / s and ratio ( psv at the stenosis / pvs above the stenosis ) < 1.5 : 1 ; haemodynamic failure was defined as stenosis 3070% ( psv 200400 cm / s , ratio 2 : 1 / 4 : 1 ) and / or stenosis > 70% ( psv > 400 cm / s , ratio > 4 : 1 )  . 
distal run - off was considered improved or worsened on the basis of the presence or absence , respectively , of the physiological triphasic flow in the leg vessels ; it was considered unchanged if the velocity values showed no change in morphology and systolic / diastolic peak . 
postprocedural angiograms and follow - up studies were evaluated by two independent radiologists with experience in vascular and interventional radiology ( rf and gg , both 12 years in angiography )  . 
i pazienti sono stati ricoverati in ospedale per una notte e dimessi il giorno successivo con una prescrizione di duplice terapia antiaggregante piastrinica ( 75 mg / die clopidogrel e 100 mg / die di aspirina ) per 6 settimane e successivamente solo aspirina o clopidogrel a tempo indeterminato . trattamento con angioplastica tutte le procedure di angioplastica sono state eseguite in sala angiografica con monitoraggio della pressione arteriosa e dellattivit elettrica cardiaca ( ecg )  . 
superata la lesione steno - ostruttiva mediante guida idrofilica 0 , 035 o guida in acciaio 0 , 014 stato posizionato catetere a palloncino da angioplastica in corrispondenza delle sedi da trattare . 
i pazienti sono stati ricoverati in ospedale per una notte e dimessi il giorno successivo con una prescrizione di duplice terapia antiaggregante piastrinica ( 75 mg / die clopidogrel e 100 mg / die di aspirina ) per 6 settimane e successivamente solo aspirina o clopidogrel a tempo indeterminato . definizioni il successo tecnico immediato della procedura stato definito quello in cui la stenosi residua non superava morfologicamente il 30% del diametro vasale . 
le lesioni che hanno richiesto un ulteriore trattamento con angioplastica con palloncino convenzionale a causa di un risultato non ottimale delle procedure o che hanno richiesto il posizionamento di stent a causa di dissezione vasale non sono state classificate come risultati positivi e non sono state considerate nel follow - up . 
il run - off distale stato giudicato migliorato o peggiorato in base rispettivamente alla presenza / assenza di flusso trifasico fisiologico nei vasi di gamba ; immodificato nel caso di riscontro di valori di velocit invariati per morfologia e picco sisto - / diastolico . 
locclusione vascolare stata definita come assenza di flusso o flusso filiforme . results follow - up angiograms were obtained immediately after the procedure to evaluate outcomes on vessels and distal run - off . 
in one patient in the cryo group , the procedure had to be discontinued because of intense pain : this case was considered a technical failure and was excluded from the follow - up . 
le immagini angiografiche post - procedurali ed i controlli del follow - up sono stati esaminati da due radiologi indipendenti esperti in radiologia vascolare ed interventistica ( r.f. , 12 anni di esperienza in angiografia ; g.g. , 12 anni di esperienza in angiografia )  . 
once the severe stenosis was crossed , cryoplasty was performed with a polarcath balloon ( polarcath peripheral dilatation system , boston scientific , natick , ma , usa ) ( b )  . 
il controllo angiografico finale documenta la buona riuscita della procedura con ripristino di un buon calibro vasale ( c )  . radiol med ( 2012 ) 117 : 11761189 1183 fig . 
il controllo angiografico finale documenta la buona riuscita della procedura con ripristino di un buon calibro vasale ( c )  . remaining three cases , there was residual stenosis between 30% and 50% . 
cryoplasty was more painful than angioplasty , with 5 / 24 patients reporting mild pain , 3 / 24 moderate pain and only one patient unbearable pain that preventing completion of the procedure ; angioplasty was associated with minor discomfort only , which never required interruption of the procedure . 
 all patients underwent 6 - month follow - up with cdus , which yielded the following results : in the cryo group , 18 treated lesions were patent , nine had varying degrees of residual stenosis and one had preocclusive stenosis ( the patient who did not tolerate the procedure was excluded from the follow - up ) ; distal run - off was unchanged at four sites , had worsened in five and improved in 19 . 
in the pta group 28 treated sites were patent and only three had residual stenosis ( two between 30% and 70% and one > 70% ) , without any occlusions ; distal run - off had improved in 30 cases and worsened in one . 
there was a statistically significant reduction in restenosis rate ( p = 0.02 ) and a significant imanalisi statistica mediante test u di mann - whitney stato confrontato , tra il gruppo cryo e pta , il successo tecnico , la riduzione di stenosi ed il run - off distale al termine della procedura , la percentuale di restenosi ed il run - off distale a 6 e 12 mesi , considerando significativa una differenza di p < 0 , 05 . risultati al termine della procedura sono stati eseguiti controlli angiografici per valutare il risultato dellintervento sui vasi trattati e sul run - off distale . 
nel gruppo cryo in un caso non stato possibile completare lintervento a causa dellintenso dolore accusato dal paziente : questo caso stato considerato come insuccesso tecnico ed stato escluso dal follow - up . 
in the cryo group , 1 - year follow - up was carried out with cdus in 23 / 29 treated sites and dsa in 4 / 29 sites ( 1 / 24 patients died due to comorbidity ; 1 / 24 experienced a procedural technical failure ) ; the radiol med ( 2012 ) 117 : 11761189 tra il 30%50% . 
risultata pi dolorosa la crioplastica dellangioplastica , con 5 / 24 pazienti che hanno accusato dolore lieve , 3 / 24 di media entit e solo un paziente ha accusato dolore intollerabile che ha impedito il completamento della procedura ; il trattamento con angioplastica stato associato solo a lievi fastidi , mai di entit tale da far sospendere lintervento . 
 tutti i pazienti sono stati sottoposti a follow - up a 6 mesi mediante ecd che ha dato i seguenti risultati : nel gruppo cryo 18 sedi trattate erano pervie , 9 presentavano stenosi residua di vario grado ed una presentava stenosi preocclusiva ( il paziente che non ha tollerato il trattamento stato escluso dal follow - up ) ; il run - off distale era in 4 sedi immodificato , in 5 peggiorato ed in 19 migliorato . 
 nel gruppo pta 28 sedi trattate erano pervie e solo tre presentavano stenosi residua ( 2 comprese tra 30%70% ed 1 > 70% ) , senza nessuna occlusione ; il run - off distale stato in 30 casi migliorato ed in uno peggiorato . 
ad 1 anno nel gruppo cryo , delle 29 sedi trattate , 23 sono state controllate mediante ecd e 4 con angiografia ( 1 decesso / 24 pazienti per co - morbili t ; 1 paziente / 24 : insuccesso tecnico intra - procedurale ) ; nel gruppo pta delle 31 sedi trattate , 29 sono state controllate mediante ecd ed 1 con angiografia ( 1 decesso / 24 pazienti per co - morbilit )  . 
un paziente trattato con crioplastica , che al momento dellarruolamento era gi in terapia dialitica per nefropatia diabetica causante insufficienza renale cronica , deceduto allundicesimo mese post - intervento ; anche nel gruppo trattato con angioplastica un paziente con grave co - morbilit deceduto prima del follow - up a 12 mesi . 
il follow - up a 12 mesi stato eseguito nel gruppo cryo in 23 sedi precedentemente trattate con ecd e in 4 mediante dsa ; nel gruppo pta una sede trattata stata valutata mediante dsa , le restanti 29 mediante ecd . nel gruppo cryo i risultati a 12 mesi sono stati : 4 occlusioni , 5 stenosi > 70% , 4 comprese tra il 30% ed 70% , 6 stenosi del 30% ; 8 erano ancora completamente pervie . 
nel gruppo pta i risultati a 12 mesi sono stati : una occlusione , 4 stenosi > 70% , 4 comprese tra il 30% ed il 70% , 6 del 30% ; 15 erano ancora pervie . 
group 1 shows a greater dispersion of restenosis values ( a ) and distal run - off ( b ) with respect to group 2 , reflecting the significant difference in results at 6 months . 
nel gruppo trattato con crioplastica si ottenuta una maggior dispersione dei valori di restenosi ( a ) e di run - off distale ( b ) rispetto al gruppo trattato con angioplastica , a testimonianza della differenza significativa di risultati ottenuti a 6 mesi . 
mediante test u mann - whitney si ottenuta una riduzione statisticamente significativa del grado di restenosi ( p = 0 , 021 ; z - score = 2 , 29 ; somma dei ranghi = 787 ) ed un incremento statisticamente significativo del runoff distale ( p = 0 , 005 ; z - score = - 2 , 75 ; somma dei ranghi = 1018 , 5 ) a favore del gruppo trattato con angioplastica . pta group was followed up with cdus in 29 / 31 treated sites and with dsa in one ( 1 / 24 patients died due to comorbidity )  . 
one patient cryo receiving dialysis for diabetic nephropathy and chronic renal failure at enrolment died 11 months after the procedure ; even in the pta group , one patient with severe comorbidity died before the 12 - month follow - up . 
 in the cryo group , 12 - month outcomes were four occlusions ; five stenoses > 70% , four between 30% and 70% and six equal to 30% ; eight sites remained completely patent . 
in the pta group , 12 - month outcomes were one occlusion ; four stenoses > 70% , four between 30% and 70% and six equal to 30% ; 15 sites remained patent . 
the correlation between dm and chronic poad is so strong that it has been estimated that the risk of poad increases by 26% at each discussione lassociazione tra diabete mellito ed arteriopatia obliterante cronica periferica ( aocp ) ormai nota con una incidenza di cli circa doppia nella popolazione diabetica rispetto a quella non - diabetica . 
 recenti studi documentano che il principale fattore di rischio per lo sviluppo di aocp linsulino - resistenza : in soggetti non - diabetici ma insulino - resistenti si ha un incremento del rischio di aocp del 40%50% [ 27 ]  . 
larteriopatia periferica nei pazienti diabetici pi aggressiva rispetto ai non - diabetici , con rapido sviluppo di macroangiopatia associata a neuropatia simmetrica distale che favorisce levoluzione negativa della patologia , con necessit di unamputazione maggiore aumentata da 5 a 10 volte nei diabetici rispetto ai non diabetici , legata alla neuropatia sensoriale ed alla ridotta resistenza alle infezioni [ 28 ]  . 
linteresse della comunit scientifica si concentrato pertanto nella ricerca di nuove terapie di rivascolarizzazione percutanea , che associano i vantaggi di una ridotta invasivit e di breve decorso post - operatorio a una buona risoluzione della sintomatologia clinica e delle lesioni trofiche stesse [ 913 , 30 ]  . 
lalta incidenza di restenosi dopo angioplastica e / o stenting del distretto femoro - popliteo in pazienti diabetici [ 68 ] ha spinto a studiare il potenziale beneficio di terapie alternative , quali la crioplastica [ 912 ]  . 1186 radiol med ( 2012 ) 117 : 11761189 fig . 
a similar dispersion of restenosis values ( a ) was found in the two groups , whereas a greater dispersion of distal run - off values ( b ) was found in group 1 . 
nei due gruppi di trattamento si riscontrata una analoga dispersione dei valori di restenosi ( a ) , a fronte di una maggior dispersione dei valori di run - off distale ( b ) nel gruppo cryo che documenta la maggior efficacia dellangioplastica convenzionale a lungo termine . 
mediante test u mann - whitney si ottenuto un incremento statisticamente significativo del run - off distale ( p = 0 , 018 ; z - score = - 2 , 35 ; somma dei ranghi = 961 ) a favore del gruppo trattato con angioplastica , a fronte di una sovrapponibile riduzione del grado di restenosi ( p = 0 , 12 ; z - score = 1 , 54 ; somma dei ranghi = 748 )  . 1% increase in haemoglobin ( hb ) a1c [ 26 ]  . 
studies have demonstrated that the main risk factor for poad is insulin resistance : nondiabetic insulin - resistant individuals have a 4050% increased risk of poad [ 27 ] , which in diabetic patients is more aggressive than in nondiabetics . 
there is faster progression to macroangiopathy associated with symmetric distal neuropathy , which promotes the negative progression of the disease , with a fiveto ten - times higher rate of major amputations among diabetics compared with nondiabetics , a result of sensory neuropathy and reduced resistance to infection [ 28 ]  . 
 the interest of the scientific community has focused on the search for new percutaneous revascularisation procedures , which combine reduced invasiveness , short postoperative recovery and resolution of the clinical symptoms as well as of the trophic lesions themselves [ 913 , 30 ]  . 
the high incidence of restenosis after angioplasty and / or stenting of the femoropopliteal arteries in diabetic patients [ 6 - 8 ] has prompted researchers to investigate the potential benefits of alternative treatments , such as cryoplasty [ 912 ]  . we conducted a prospective , randomised , controlled study comparing cryoplasty and standard angioplasty for treating stenotic - occlusive lesions of the femoropopliteal arteries by evaluating the patency and distal run - off in the immediate , mid and long terthe initial hypothesis was that cryoplasty was a more uniform and less traumatic procedure , which - associated with the induction of cell apoptosiswould translate into less intimal hyperplasia and therefore abbiamo condotto uno studio prospettico , randomizzato e controllato di confronto tra crioplastica ed angioplastica standard nel trattamento di lesioni steno - ostruttive del distretto femoro - popliteo , valutando la perviet ed il runoff distale immediati e a medio e lungo termine . 
liniziale ipotesi era che la crioplastica fosse una procedura pi uniforme e meno traumatica che , associata allinduzione delleffetto apoptotico , si traducesse in minor iperplasia neointimale e , di conseguenza , a migliori risultati immediati ed a medio e lungo termine [ 15 , 16 ]  . 
 da una ricerca effettuata relativa alla letteratura pi recente abbiamo evidenziato che pochi sono gli studi che hanno valutato la reale efficacia della crioplastica in termini di successo tecnico immediato e a medio e lungo termine [ 1721 ]  . 
 [ 20 ] hanno dimostrato che la crioplastica non fornisce sostanziali benefici rispetto allangioplastica in termini di successo tecnico immediato e perviet vasale a lungo termine e ci , associato allalto grado di restenosi seguite da nuove procedure di rivascolarizzazione e allalto costo del device polarcath , rende langioplastica convenzionale il trattamento pi indicato nel trattamento dellaocp in pazienti diabetici . 
 a search of the recent literature showed that , indeed , few researchers have evaluated the real efficacy of cryoplasty in terms of immediate technical success and midand longterm outcomes [ 1721 ]  . 
 [ 20 ] demonstrated that cryoplasty does not provide substantial benefits compared with pta in terms of immediate technical success and long - term patency , which , coupled with the high rate of restenosis followed by repeat revascularisation procedures and the high cost of the polarcath system , makes conventional pta the most indicated treatment for poad in diabetic patients . 
the initial technical success was 68% for native vessels and 71% for in - stent procedures and 1 - year patency 17% and 28% , respectively , with freedom from disease at 1 year of 32% and 21% ; the authors therefore concluded that cryoplasty is not an advantageous endovascular treatment for poad . even the most enthusiastic supporters of cryoplasty effectiveness have reconsidered their initial results for treating stenotic - occlusive lesions of the femoropopliteal arteries and no longer routinely use this procedure [ 31 , 32 ]  . 
it is important to note that to make the sample more homogeneous , we excluded patients treated with stent placement because of vessel dissection . mid - term results ( 6 months ) demonstrate the definite superiority of pta compared with cryoplasty : we found a significant reduction in restenosis rate ( p = 0.02 ) and significant der et al . 
il successo tecnico iniziale era del 68% per i vasi nativi e del 71% per le procedure intrastent , la perviet ad 1 anno era rispettivamente del 17% e 28% con intervallo libero da malattia rispettivamente del 32% e 21% , concludendo pertanto che la crioplastica rappresenta un approccio endovascolare non vantaggioso nel trattamento della arteriopatia ostruttiva degli arti inferiori . anche i pi entusiasti sostenitori dellefficacia della crioplastica hanno revisionato i loro iniziali risultati nel trattamento delle lesioni steno - ostruttive del distretto femoropopliteo , abbandonando luso routinario di tale procedura [ 31 , 32 ]  . 
il nostro studio , in linea con i pi recenti lavori , dimostra che la crioplastica fornisce risultati di perviet primaria e run - off distale immediato e a medio e lungo termine inferiori rispetto allangioplastica convenzionale e pertanto ha un ruolo secondario nel trattamento dellaocp in pazienti diabetici . nella nostra esperienza la crioplastica assicura un adeguato successo tecnico procedurale bench langioplastica convenzionale sia associata ad un incremento statisticamente significativo di perviet primaria ( p = 0 , 048 )  . 
nel nostro lavoro importante sottolineare , rispetto a quelli citati , che per rendere pi omogeneo il campione , sono stati esclusi pazienti che , in seguito a dissezioni , hanno posizionato uno stent . i risultati a medio termine ( 6 mesi ) dimostrano una importante superiorit dellangioplastica rispetto alla crioplastica : abbiamo riscontrato una riduzione significativa della percentuale di restenosi ( p = 0 , 02 ) ed un significativo miglioramento del run - off distale ( p = 0 , 005 ) nel gruppo trattato con angioplastica rispetto a quello trattato con crioplastica . 
 i risultati a lungo termine ( 12 mesi ) evidenziano che , a fronte di una percentuale di restenosi sovrapponibile tra i due gruppi di trattamento ( p = 0 , 122 ) , il run - off distale significativamente maggiore per il gruppo trattato con angioplastica rispetto a quello trattato con crioplastica ( p = 0 , 018 )  . 
 [ 21 ] che ha ottenuto un grado di restenosi a 9 mesi nel gruppo trattato con crioplastica maggiore rispetto 1188 radiol med ( 2012 ) 117 : 11761189 improvement in distal run - off ( p = 0.005 ) in the group treated with pta . 
no stents were placed in patients in either study group . limitations of our study are the small number of patients allocated to each treatment group and the selection of patients themselves : indeed , we even allocated patients with advanced , highly calcified lesions to both groups , for which the effectiveness of cryoplasty is known to be reduced [ 13 , 14 ]  . 
this was done to ensure adequate representation of the diabetic population in both groups and to evaluate the real effectiveness of this innovative procedure in relation to pta for treating diabetic poad . the hypothesis that cryoplasty , by inducing cell apoptosis , is associated with less intimal hyperplasia with longerlasting midand long - term results does not appear to be validated by our results . 
cryoplasty provides adequate technical success but is associated with a higher rate of restenosis at 6 months , with less distal run - off at 6 and 12 months compared with pta . 
in evaluating the degree of restenosis at 12 months , we found statistical equivalence between the two procedures despite a higher degree of occlusion ( 4 : 1 ) and a lower degree of patency ( 1 : 2 ) in the cryo group than om the pta group . 
another aspect to be considered is the different cost of the two techniques , with pta materials being less expensive than cryoplasty material . consistent with recent studies [ 1821 , 32 ] , we believe angioplasty to be more effective for treating poad in diabetic patients , as it ensures better primary technical success , a lower degree of restenosis and a greater distal run - off in the short and long term compared with cryoplasty . to conclude , in our experience , cryoplasty is a safe and useful procedure for treating stenotic - occlusive lesions of the femoropopliteal region in diabetic patients . 
however , pta remains the most effective treatment , guaranteeing the best immediate , midand long - term results . a quello trattato con angioplastica ( 79 , 3% vs 66 , 7% rispettivamente ) , in assenza tuttavia di significativit statistica , a differenza di quello di spiliopoulos et al . 
 [ 20 ] che ha invece ottenuto un tasso di perviet primaria a 12 mesi sovrapponibile con le due metodiche di trattamento ( 67 , 6% con crioplastica e 66 , 6% con angioplastica )  . le procedure di rivascolarizzazione mediante crioplastica sono risultate pi dolorose rispetto alle procedure di angioplastica , in assenza tuttavia di complicanze maggiori . 
 il trattamento con crioplastica ha richiesto dei tempi tecnici di preparazione leggermente maggiori dellangioplastica ( durata media crioplastica : 1 ora ; durata media angioplastica : 40 minuti )  . 
nei due gruppi inclusi nello studio non sono stati posizionati stent . i limiti del nostro studio sono rappresentati dal basso numero di pazienti assegnati a ciascun gruppo di trattamento e dalla selezione dei pazienti stessi : sono stati infatti assegnati ai due gruppi di trattamento lesioni anche di grado avanzato e fortemente calcifiche per le quali lefficacia della crioplastica ridotta [ 13 , 14 ]  . 
questa selezione stata effettuata al fine di assicurare una adeguata rappresentazione della popolazione diabetica nei due gruppi di trattamento e confrontare pertanto la reale efficacia di questa innovativa procedura , rispetto allangioplastica standard , nel trattamento dellaocp diabetica . lipotesi che la crioplastica , mediante linduzione dellapoptosi cellulare , si associasse a minore iperplasia intimale con risultati pi duraturi a medio e lungo termine non sembra pertanto validata dal nostro studio . 
la crioplastica determina un adeguato successo tecnico procedurale ma si associa ad un maggior grado di restenosi a 6 mesi con minor run - off distale a 6 e 12 mesi rispetto a quello ottenuto con angioplastica standard . 
nella valutazione del grado di restenosi a 12 mesi abbiamo riscontrato una sovrapponibilit statistica tra le due procedure , a fronte comunque di un maggior grado di occlusione ( 4 : 1 ) ed un minor grado di perviet ( 1 : 2 ) nel gruppo cryo rispetto al gruppo pta . 
simonetti dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , policlinico universitario tor vergata , via oxford 81 , 00133 roma , italy correspondence to : a . 
interim pet - mdct was negative in 104 / 132 patients ( 79% ) , and their final pet - mdct showed complete remission in 102 / 104 ( 98% ) of cases , with disease recurrence / persistence in two ( 2% )  . 
in the remaining 28 ( 21% ) patients , interim pet - mdct revealed an early response in 68% of cases and chemoresistance with disease progression in 32% of cases ; in these 28 patients , final pet - mdct showed a lack of response to treatment in 43% of cases ( 43% ) and complete remission in 57% of cases . 
interim pet - mdct has a reliable prognostic role in diagnosis and treatment of patients with hl , as it helps predict which patients are more likely to achieve a riassunto obiettivo . 
sono stati studiati retrospettivamente 132 pazienti affetti da lh con pet - tcms alla stadiazione della malattia e prima della terapia , dopo 2 cicli di chemioterapia ( cht ) abvd [ doxorubicina ( adriblastina ) , bleomicina , vinblastina e dacarbazina ] ( pet - tcms in itinere ) , almeno dopo 30 giorni dallultimo ciclo di cht e / o dopo tre mesi dal termine della radioterapia , quando prevista ( pet - tcms finale )  . 
104 ( 79% ) , dei 132 pazienti studiati , hanno presentato la pet - tcms in itinere negativa ; la pettcms finale in tali pazienti ha mostrato la remissione completa in 102 pazienti ( 98% ) ed una recidiva / persistenza di malattia in 2 ( 2% )  . 
in 28 pazienti ( 21% ) abbiamo riscontrato alla pet - tcms in itinere , una risposta precoce parziale nel 68% e una chemioresistenza con progressione di malattia nel 32% ; in tali pazienti la pet - tcms finale ha mostrato una mancata risposta al trattamento in 12 casi ( 43% ) e una remissione completa in 16 ( 57% )  . 
dallanalisi statistica di questi dati emerso che la pet - tcms in itinere possiede un valore predittivo negativo ( vpn ) del 98% ed un valore predittivo positivo ( vpp ) del 42% con valori del 85 , 7% , 86 , 4% ed 86 , 4% rispettivamente di sensibilit , la specificit e di accuratezza diagnostica [ intervallo di confidenza ( ic ) 95 ]  . 
la pet - tcms in itinere pu avere un importante significato prognostico durante il percorso diagnostico - terapeutico dei pazienti affetti da lh , radiol med ( 2012 ) 117 : 12501263 1251 complete response at the end of treatment . 
pet / mdct may also lead to a change in treatment , with reduced treatment - related toxic effects and significantly reduced total costs . keywords hodgkins lymphoma diagnosis prognosis pet / mdct permettendo di identificare precocemente il numero di pazienti con elevata probabilit di risposta completa della malattia al termine della terapia . 
pu anche essere utile nelle scelte terapeutiche con riduzione degli effetti tossici correlati e dei costi complessivi . parole chiave linfoma hodgkin , diagnosi linfoma hodgkin , prognosi linfoma hodgkin , pet - tc introduction introduzione hodgkins lymphoma ( lh ) is most common among young adults and appears to be associated with a high likelihood of remission , with mean 5 - year survival rates of > 80% , thanks to the combination of new chemotherapy and radiotherapy treatments [ 1 , 2 ]  . 
the rigid application of treatment protocols and the close follow - up of these patients are often responsible for the onset of midand long - term side effects , such as myelosuppression , leukaemias , neuropathy , pulmonary fibrosis , cardiocirculatory disorders and secondary neoplasms , including thyroid and breast cancer [ 3 ]  . 
study of the cancers gene expression profile , individual drug metabolism , serum cytokine profiles and the increasingly rational use of positron emission tomography / multidetector computed tomography ( pet / mdct ) could help identify , early on in the course of treatment , patients at increased risk of side effects and adoption of more appropriate treatments as a first - line approach . 
in this context , the major difficulty in restaging patients ( that is , reassessing them 2 months after the beginning of chemotherapy ) lies in the need to differentiate between disease persistence and remission , even in the presence of lymphomatous tissue , which may persist up to 3 years after treatment in > 64% of patients in clinical remission [ 4 , 5 ]  . 
 the role of pet in defining the extent of disease and the metabolic activity of the cellular components of hl for assessing treatment response and the follow - up of hl patients is generally accepted . 
when early on in the course of treatment the patient is considered nonresponsive to chemotherapy - radiotherapy , it is necessary to change to a higher - dose treatment regimen or perform bone marrow transplantation . 
 il linfoma di hodgkin ( lh ) costituisce una delle patologie pi frequenti tra i giovani adulti e , soprattutto grazie alla combinazione dei nuovi trattamenti chemioterapici ( cht ) e radioterapici ( rt ) , appare caratterizzato da unelevata possibilit di remissione della malattia con una sopravvivenza media a 5 anni in oltre l80% dei casi [ 1 , 2 ]  . 
la rigorosa applicazione di protocolli terapeutici e lo stretto follow - up cui vengono sottoposti tali pazienti , sono spesso causa dinsorgenza di effetti collaterali a medio e lungo termine , quali ad esempio linduzione della mielosoppressione , linsorgenza di forme leucemiche , di neuropatie , di fibrosi polmonare , di danni cardio - circolatori e di neoplasie secondarie , tra cui soprattutto il carcinoma tiroideo e quello mammario [ 3 ]  . 
 linsorgenza degli effetti collaterali riportati sopra , impongono la necessit di identificare quanto prima possibile lo schema terapeutico pi idoneo per ciascun paziente , in relazione alla dose e alla combinazione dei diversi agenti chemioterapici e del trattamento radioterapico . 
lo studio del profilo dellespressione genica della neoplasia , del metabolismo individuale dei farmaci , dei profili delle citochine sieriche e luso sempre pi razionale della tomografia ad emissione di positroni ( pet ) / tomografia computerizzata ( tc ) potrebbero permettere , di individuare precocemente i pazienti pi a rischio e di utilizzare , gi in prima istanza , terapie pi idonee . 
in tale contesto , la maggior difficolt della ristadiazione del paziente ( ovvero la rivalutazione effettuata a due mesi dallinizio della chemioterapia ) consiste nel dover discriminare tra la persistenza di malattia linfoproliferativa in fase attiva e la sua remissione , pur in presenza di tessuto linfomatoso che tende a persistere in oltre il 64% dei pazienti in remissione clinica fino ad oltre 3 anni dal termine della terapia [ 4 , 5 ]  . 
 limportanza della pet nella definizione dellestensione della malattia e del metabolismo delle componenti cellulari del lh oggi riconosciuta nella valutazione della risposta al trattamento e nel follow - up di pazienti affetti da linfoma . 
 si deduce pertanto che qualora in fase iniziale il paziente sia considerato non responsivo al trattamento chemio - / radioterapico in atto , necessariamente risulti indispensabile utilizzare uno schema terapeutico a pi alte dosi ovvero ricorrere al trapianto di midollo osseo . 
to ensure a homogeneous study population , we included only 132 / 210 patients ( 72 men , 60 women ; mean age 34 years ; range 1674 ) who met the following criteria : a diagnosis based on biochemical tests and bone marrow biopsy ; a pet - mdct staging examination performed at diagnosis before the start of treatment , at 15 days after two cycles of chemoradiotherapy ( interim petmdct ) and at 30 days after the end of chemotherapy , or 3 months after the end of radiotherapy if delivered ( final pet - mdct )  . 
the remaining 78 / 210 patients were excluded from the study . for each patient , we reviewed medical history ( age , sex , clinical stage i - iv ) , presence or absence of associated symptoms , bulky involvement ( mass with maximum diameter > 5 cm or > 1 / 3 of thoracic diameter ) , histological subtype and laboratory data ( albumin , erythrocyte sedimentation rate , haemoglobin , full blood count )  . 
according to the world health organisation ( who ) classification [ 6 ] , the 132 patients included in the study were distributed as follows : 91 with nodular sclerosis histology , 25 with mixed cellularity , 16 with lymphocytic predominance and none with lymphocytic depletion ( table 1 )  . radiol med ( 2012 ) 117 : 12501263 il nostro studio si pone lobiettivo di valutare quale sia il ruolo prognostico della 18f - fluorodeossiglucosio ( fdg ) pet / tc multi strato ( ms ) nellindividuare i pazienti affetti da linfoma di hodgkin responsivi o meno al trattamento chemio - terapico iniziale e di modulare i successivi protocolli chemio - / radioterapici meno tossici qualora possibile . 
 materiali e metodi pazienti abbiamo valutato retrospettivamente le indagini pet / tcms effettuate nel periodo compreso tra gennaio 2005 e giugno 2010 presso il nostro dipartimento , in 210 pazienti con diagnosi di linfoma di hodgkper rendere omogeneo il campione in esame sono stati inclusi nello studio unicamente 132 / 210 pazienti , 72 maschi e 60 femmine con et media 34 anni ( range 1674 ) , la cui diagnosi fosse stata ottenuta mediante esami biochimici e biopsia osteomidollare , e la cui rivalutazione pet / tcms fosse stata effettuata allesordio per la stadiazione di malattia prima dellinizio del trattamento , 15 giorni dopo 2 cicli di chemio - radioterapia ( pet / tcms in itinere ) e 30 giorni al termine della stessa o 3 mesi se sottoposti anche a radioterapia ( pet / tcms finale )  . 
prior to the examination , patients were administered an intravenous infusion of radiopharmaceutical equivalent to 5 mbq / kg as a single bolus over the course of 4560 min , followed by 250500 ml saline and 500 cc diluted water - soluble oral contrast agent ( gastrografin , bayer schering , berlin ) to obtain optimal bowel opacification . 
 with the patient in supine position , a low - dose ( 50 ma ) unenhanced ct scan was obtained for attenuation correction of pet data ; pet images were subsequently acquired over six to seven bed positions of 4 - 5 min in a caudocranial direction , from pelvis to head . 
the mdct scan was then performed with a multiphase technique after administration of an intravenous bolus of 120150 ml of nonionic iodinated contrast material ( 300370 mgi / ml ) at a rate of 2.53 ml / s , with a scan delay of approximately 30 s for the arterial phase , 70 s for the venous phase and 180 s for the urographic phase , if necessary . 
mean examination time was approximately 35 m the fused pet / mdct images were made available to the radiologist and nuclear medicine specialist on a postprocessing workstation ( advantage - windows 4.4 , general electric , medical system )  . 
in all cases , qualitative interpretation of pet images was confirmed by semiquantitative analysis whereby a region of interest ( roi ) was placed over the areas of pathological radiotracer uptake and the actual extent of uptake was calculated and compared with that seen in the images obtained before , during and after treatment . 
in view of the correlation between uptake and variables , such as baseline serum glucose , body surface area , body weight and time elapsed between intravenous administration of radiotracer and pet acquisition , all follow - up pet / mdct examinations were performed under completely identical conditions to ensure comparability of uptake data . treatment regimen and follow - up all patients received [ doxorubicin ( adriblastin ) , bleomycin , vinblastine and dacarbazine ( abvd ) ] chemotherapy in standard doses every 2 weeks . 
the regimen was decided upon on the basis of clinical stage : four chemotherapy cycles followed by radiotherapy for the early stages ( i - iia ) ; six to eight chemotherapy cycles followed by radiotherapy for more advanced stages ( iib - iv )  . 
to avoid the problem 1253 sintomi associati , interessamento bulky ( massa con diametro massimo superiore a 5 cm o pi di 1 / 3 del diametro toracico ) , sottotipo istologico e dati di laboratorio [ albumina , velocit di eritrosedimentazione ( ves ) , emoglobina , emocromo ]  . 
 secondo la classificazione della world health organization ( who ) del 2000 [ 6 ] , i 132 pazienti inclusi nello studio erano cos rappresentati : 91 con istotipo sclerosi nodulare , 25 con cellularit mista , 16 con prevalenza linfocitaria e nessun caso di deplezione linfocitaria ( tabella 1 )  . tecnica di esame pet / tcms tutte le indagini pet / tcms sono state eseguite con sistema scanner integrato pet / tcms discovery st ( ge , general electric , medical system , germania ) , che utilizza uno scanner tc modello high speed ultra con 16 file di detettori con un tomografo pet a 10080 cristalli di germanato di bismuto ( bgo ) disposti su 24 anelli . 
in fase preliminare abbiamo somministrato endovena ( e.v. ) una dose di radiofarmaco equivalente a 5 mbq / kg in bolo unico in circa 4560 minuti , seguita dallinfusione di circa 250500 ml di soluzione fisiologica e di circa 500 cc di una soluzione acquosa con mezzo di contrasto idrosolubile diluito ( gastrografin , bayer schering , berlino , germania ) per os , al fine di ottenere unottimale opacizzazione delle anse intestinali . successivamente il paziente stato posizionato in decubito supino e si proceduto ad acquisire una tc basale a basso amperaggio ( 50 ma ) necessaria per la correzione dellattenuazione dei dati pet ; sono state quindi acquisite immagini emissive pet della durata di 45 minuti per lettino con un totale di 67 lettini in direzione caudo - craniale dalla pelvi allencefalo . 
di 120150 ml di mezzo di contrasto ( mdc ) organo - iodato non ionico ( 300370 mgi / ml ) a 2 , 53 ml / s con ritardo di scansione di circa 30 secondi per la fase arteriosa , di circa 70 secondi per la fase venosa e di circa 180 secondi per la fase urografia , se necessaria . 
 le immagini fuse pet / tc sono successivamente rese disponibili per il medico radiologo ed il medico nucleare su una consolle di ricostruzione advantage - windows 4.4 ( ge , general electric , medical system )  . 
in tutti i casi analizzati linterpretazione qualitativa delle immagini pet stata confermata dallanalisi semiquantitativa mediante posizionamento di una region of interest ( roi ) in corrispondenza degli accumuli di radiofarmaco ritenuti patologici , con lintento di calcolare lintensit effettiva della captazione e poterla confrontare nelle acquisizioni eseguite prima , durante e dopo la terapia . 
al fine di poter confrontare tale parametro nei vari controlli , in relazione alla sua correlazione e dipendenza da alcune variabili quali la glicemia basale , la superficie corporea , il peso del paziente e il tempo inter1254 radiol med ( 2012 ) 117 : 12501263 of findings related to chemotherapy - induced inflammation which is reported to be particularly evident in the early days after treatment [ 710 ] pet / mdct was scheduled at the end of the second chemotherapy cycle ( 15 days after infusion of the second dose ) , 1 month after the end of treatment and 3 months after the end of radiotherapy . 
when deciding upon the timing of pet / mdct restaging , we took into account the in vitro demonstration that , following chemotherapy , tumour cells show a fluctuating uptake of [ 18f ] - fdg , with a significant decrease in uptake shortly after the beginning of therapy as a result of the stunning effect [ 11 ]  . 
 [ 14 ] : cases of uptake at sites unrelated to lymphoma that had already been identified by other imaging methods ( such as areas of inflammation ) ; sites of physiological uptake ( brain , heart , blood vessels , ureters , gastrointestinal tract , brown fat ) ; sites of marrow reactivation resulting from chemotherapy and the administration of haematopoietic factors . 
the false positive nature of these findings was then confirmed by morphological ct data or , where necessary , by the follow - up or comparison with other imaging modalities ( ultrasound )  . 
 sites of suspected active disease were defined as moderate and diffuse radiotracer uptake in correspondence with medium - sized and large nodal masses showing less intense or equal uptake to that of mediastinal vessels ( blood pool ) ; uptake in correspondence with nodular masses at least 1.5 cm in size located in the hepatic , splenic or pulmonary parenchyma even if uptake was lower than that of surrounding tissue ; and finally , diffusely increased metabolic activity at bone marrow level . 
secondary localisations were defined as new lung nodules at least 1.5 cm in size and with uptake exceedcorso tra liniezione del farmaco per via endovena e lacquisizione pet , sono state sempre rigorosamente rispettate le stesse condizioni di esecuzione dellesame pet / tcms ad ogni controllo . schema terapeutico e controlli tutti i pazienti sono stati sottoposti a trattamento polichemioterapico secondo lo schema doxorubicina ( adriblastina ) , bleomicina , vinblastina e dacarbazina ( abvd ) in dosi standard ogni 2 settimane . 
il trattamento dei pazienti stato impostato in base allo stadio clinico : da 4 cicli di cht seguiti da rt negli stadi precoci ( i - iia ) e da 68 cicli di cht + rt negli stadi avanzati ( iib - iv )  . 
al fine di evitare che i risultati ottenuti fossero dovuti a flogosi reattiva successiva alla risposta agli agenti chemioterapici che , secondo i dati riportati in letteratura , risulta particolarmente evidente nei primi giorni del trattamento [ 710 ] , la rivalutazione strumentale stata programmata rispetto alla somministrazione della chemioterapia al termine del ii ciclo ( dopo 15 giorni dallinfusione della seconda dose ) , un mese dopo la fine del trattamento e tre mesi dopo la fine della radioterapia . 
per la scelta del timing di rivalutazione strumentale si tenuto conto della dimostrazione in vitro che le cellule tumorali in seguito al trattamento chemioterapico mostrano una fluttuante captazione del 18f - fdg con significativo calo di fissazione del radiofarmaco a pochi giorni dallinizio della terapia per il cosiddetto effetto stunning [ 11 ]  . 
i pazienti hanno proseguito il trattamento programmato , anche in presenza di una risposta metabolica non completa dopo il ii ciclo , ad eccezione dei casi nei quali era dimostrata con certezza una progressione della malattia . 
secondo quanto riportato in letteratura [ 14 ] sono stati considerati falsi positivi i casi di iperaccumulo del radiofarmaco in siti di reperti non correlati alla patologia linfomatosa ed evidenziati in precedenza con altre metodiche , come per esempio aree di flogosi , ovvero siti di fisiologico uptake del radiofarmaco , quali lencefalo , il miocardio , i vasi , gli ureteri , il tratto gastrointestinale ed il grasso bruno , ed infine , anche in relazione al dato anamnestico , sedi di riattivazione midollare conseguente al trattamento chemioterapico e alla somministrazione di fattori ematopoietici ; la falsa positivit di tali riscontri stata quindi confermata dal dato morfologico dellindagine tc ovvero , qualora necessario , dal follow - up o dal confronto successivo con altre metodiche ( ecografia )  . 
 sono state definite come sospette localizzazioni di malattia in fase attiva le modeste e diffuse captazioni del radiofarmaco in corrispondenza di masse linfonodali di medie e grandi dimensioni caratterizzate da intensit di captaradiol med ( 2012 ) 117 : 12501263 1255 fig . 
alla stadiazione le immagini a 18f - fdg - pet coronale , b tcms con mdc assiale e c pet / tcms assiale mostrano laumento volumetrico bulky di linfonodi mediastinici con estensione alla parete toracica anteriore di sinistra e versamento pleurico omolaterale . 
 al controllo in itinere le immagini a 18f - fdg - pet coronale , b tcms con mdc assiale e c pet / tcms assiale mostrano la riduzione volumetrica delle tumefazioni linfonodali mediastiniche e la precoce negativizzazione dellincremento dellattivit metabolica con fissazione pari al blood pool mediastinico . 
non pi presente il versamento pleurico a sinistra . ing that of the mediastinal blood - pool structures , in agreement with the competence network malignant lymphomas [ 15 ]  . 
 zione inferiore o uguale a quella delle strutture vascolari mediastiniche ( blood - pool ) , le iperfissazioni del tracciante in corrispondenza di formazioni nodulari con dimensioni di almeno 1 , 5 cm a carico del parenchima epatico , splenico e polmonare anche se con intensit di fissazione inferiore al tessuto limitrofo ed infine gli incrementi diffusi dellat1256 radiol med ( 2012 ) 117 : 12501263 fig . 
3a - c uomo di 42 anni con stadio ivb di lh a prevalenza linfocitaria , con interessamento polmonare , epatico , splenico ed osseo come dimostrato , alla stadiazione , nelle immagini a 18f - fdg - pet in proiezione di massima intensit ( mip ) ( sopra ) e di fusione pet / tcms coronali ( in basso )  . 
b le immagini 18ffdg - pet e pet / tcms effettuate dopo i primi due cicli di terapia mostrano la parziale risposta con residuo di malattia a carico della milza ( frecce )  . 
c il controllo 18f - fdg - pet e pet / tcms al termine della terapia mostrano la completa risposta con scomparsa delle aree focali di incremento dellattivit metabolica . statistical analysis we considered sensitivity , specificity and diagnostic accuracy of the pet / mdct examination , as well as the positive ( ppv ) and negative ( npv ) predictive values . 
 results data analysis for the 132 hl patients in our study revealed that 104 cases ( 79% ) were negative at interim pet / mdct at the end of first - line therapy . 
in these patients , final pet / mdct confirmed the negative results in 102 cases ( 98% ) and revealed pathological uptake in the remaining two cases tivit metabolica a livello midollare . 
 [ 14 ] , were mainly due to physiological uptake and were noted at the level of the ureters ( 20% ) , gastrointestinal tract ( 15% ) , blood vessels ( 14% ) and brown fat ( 10% )  . 
 the results of our analysis suggest that both morphological and metabolic data are important for identifying sites of disease ; in particular , mdct helped us to define equivocal sites of uptake and to detect sites of parenchymal localisations , whereas [ 18f ] - fdg - pet enabled us to discriminate fibrotic scar tissue and to define as pathological nodal masses of normal size . 
 univariate analysis of the main patient - specific variables ( sex , age , presence of associated symptoms , histological type , stage , bulky mediastinal disease , extranodal involvement ) performed to isolate possible indicators of poor prognosis showed that disease stage at presentation , involvement of parenchymal structures and residual disease after two chemotherapy cycles are correlated with a significant risk of progression / chemoresistance . 
moreover , our results show that pet / mdct had a ppv of 42% based on the number of patients who achieved complete response at the end of treatment and who were thus still positive at the interim examination . 
sono state ritenute localizzazioni secondarie di malattia le formazioni nodulari polmonari , assenti nellesame di stadiazione , con dimensioni di almeno 1 , 5 cm e ipercaptazione del radiotracciante anche se di poco superiore a quella del blood - pool mediastinico , in accordo con quanto proposto dal competence network malignant lymphoma [ 15 ]  . 
tuttavia la comparsa di nuove formazioni nodulari in un paziente con negativizzazione metabolica post - terapeutica di tutti i siti nodali o extranodali di malattia , stata messa in relazione alla natura infettiva o infiammatoria delle stesse . 
 risultati dallanalisi finale dei dati riguardanti i 132 pazienti con linfoma di hodgkin , del nostro studio , abbiamo osservato in 104 casi ( 79% ) la negativizzazione alla pet / tcms in itinere alla fine terapia di prima istanza . 
in questi pazienti la valutazione morfo - metabolica ( pet / tcms finale ) ha confermato la negativizzazione alla pet / tc in 102 casi ( 98% ) , mentre ha mostrato una patologica captazione del radio farmaco nei restanti 2 ( 2% )  . 
nei 28 ( 21% ) rimanenti pazienti abbiamo riscontrato alla pet / tcms in itinere una parziale risposta in 19 casi ( 68% ) e una stabilit o progressione di malattia in 9 ( 32% ) ; in tali pazienti il controllo finale con pet / tcms finale ha confermato in 12 casi ( 43% ) una persistenza di malattia e in 16 ( 57% ) una rispo1258 radiol med ( 2012 ) 117 : 12501263 when subdividing the 28 patients showing only partial response at interim pet / mdct according to clinical stage at presentation , we found 68% were at a high - risk stage ( stage iib - iv ) and only 32% had localised disease ( stage i - iia )  . 
in six patients , the disease also presented with extranodal involvement ( one breast lesion , three splenic lesions , two hepatic lesions , three lung lesions , three areas of bone marrow involvement )  . 
long - term follow - up of these patients showed that one died after recurrence 3 months after autologous bone marrow transplantation ; 11 underwent bone marrow transplantation , as they did not respond to any chemotherapy regimen or second - line treatment ; two showed early negative findings followed , however , by recurrence within days after finishing therapy . 
the remaining patients were all in remission at subsequent follow - up examinations . discussion until recently , the restaging of hl patients following chemotherapy and radiotherapy was based on the assessment of morphological parameters , such as dimension and vascularity , of lymphomatous masses , enlarged nodes and parenchymal localisations , determined by clinical - laboratory tests and particularly with imaging investigations [ 16 ] , the most important of which was total - body ct . 
complete remission was considered as the complete absence of residual radiological abnormalities at previous sites of disease ; incomplete remission or partial response was assessed as persistence of a lesion > 1.5 cm in maximum diameter , with a 75% reduction in size compared to its original volume ; disease progression was defined as the appearance of a new lesion or 50% increase in the size of known lesions ; recurrence was defined as reappearance of disease after a period of remission [ 17 ]  . 
this is confirmed by the frequent occurrence of false negative results in the case of pathological nodal structures of normal size or false positive results in the presence of reactive inflammatory adenomegaly or splenomegaly related to the use of haematopoietic growth factors during chemotherapy [ 18 ]  . as a result of the inherent limitations of ct , innovative imaging modalities such as [ 18f ] - fdg - pet have been developed and increasingly introduced into clinical practice [ 1921 ]  . 
dallanalisi statistica di questi dati emerso che la pet / tcms in itinere possiede un vpn del 98% con valori del 85 , 7% di sensibilit , del 86 , 4% di specificit e del 86 , 4% di accuratezza diagnostica . 
 dalla nostra analisi emersa limportanza di entrambe i dati a nostra disposizione ( dato morfologico e dato metabolico ) nellindividuazione dei siti di patologia ; in particolare lesame tc ci ha permesso di definire siti di uptake di dubbia interpretazione e di individuare localizzazioni di patologia intraparenchimali , mentre lindagine 18f - fdgpet ci ha consentito di discriminare condizioni di fibrosi cicatriziale e di definire patologiche formazioni linfonodali regolari per dimensioni . 
 con lintento di isolare eventuali indici di prognosi infausta , la valutazione dei risultati di unanalisi univariata delle principali variabili legate a ciascun paziente ( sesso , et , presenza di sintomi associati , istotipo , stadio , localizzazione mediastinica bulky , interessamento extranodale ) ci ha permesso di attestare che lo stadio della malattia allesordio , lestensione alle strutture parenchimali e la persistenza di malattia residua dopo 2 cicli di cht si traducono in un rischio significativo di progressione / chemioresistenza . 
dallanalisi dei dati emerge inoltre che la tecnica di imaging da noi utilizzata possiede un vpp del 42% , in rapporto al numero di pazienti che sviluppano una risposta terapeutica completa a fine protocollo , persistendo quindi positivi allesame di controllo eseguito in itinere . 
 suddividendo i 28 pazienti che hanno mostrato una risposta terapeutica solo parziale nel controllo pet / tcms in itinere in base allo stadio clinico desordio della malattia , si evidenzia che il 68% appartiene ad uno stadio ad alto rischio ( stadi iib - iv ) e solo il 32% presenta malattia localizzata ( stadi i - iia )  . 
in 6 pazienti la malattia ha esordito anche con interessamento extranodale ( 1 lesione mammaria , 3 lesioni spleniche , 2 lesioni epatiche , 3 lesioni polmonari , 3 aree di interessamento midollare )  . 
allinterno di questa popolazione di soggetti positivi alla pet / tcms in itinere si sono registrati 12 casi di pazienti resistenti alla terapia , con persistenza di malattia alla valutazione strumentale pet / tcms finale . 
il follow - up a lungo termine in questi casi ha mostrato che uno di essi deceduto dopo recidiva a 3 mesi dal trapianto autologo di midollo osseo ( tmo ) ; 11 pazienti sono stati sottoposti a radiol med ( 2012 ) 117 : 12501263 1259 glucose transporters and increased hexokinase activity shown by neoplastic and actively replicating cells . 
for this reason , the most recent guidelines recommend the use and correct timing of [ 18f ] - fdg - pet for monitoring response to treatment of the various types of lymphoma . 
in fact , in vitro experiments confirm that antineoplastic treatments are 99.9% effective , even after only two treatment cycles [ 21 ]  . combining the metabolic assessment provided by [ 18f ] fdg - pet and the morphological assessment provided by mdct makes it possible to overcome the limitations of pet , especially in cases of parenchymal localisations and false positive results , thereby improving patients diagnostic and therapeutic pathway [ 2225 ]  . 
 [ 18f ] - fdg - pet is known to be burdened by a high rate of false positive results , as are seen in infection , inflammation , supraclavicular brown fat , thymic hyperplasia or marrow reactivation due to haematopoiesis - stimulating factors . 
in addition , excretion of the radiotracer through the urinary and intestinal system could mask the presence of millimetre - sized abdominal adenopathies at nearby sites or mimic a pathological focal uptake by those structures . 
in these cases , the concurrent acquisition of ct images for anatomical localisation of the functional data is fundamental for evaluating equivocal findings and reducing the number of false positive and false negative results . the results of our analysis attest to the importance of both morphological and metabolic information in identifying sites of disease ; in particular , ct scans allowed us to define sites of uptake that were difficult to interpret , as well as to identify intraparenchymal sites of disease , whereas [ 18f ] - fdg - pet helped us distinguish sites of fibrotic scarring and characterise as pathological nodal masses of regular size . 
in this retrospective study , the two techniques were used in combination to accurately stage the disease prior to treatment and , through a comparison of results , to restage it early on in the course of treatment and at the end of standard treatment . our findings are in bearing with the results reported in the literature [ 18 ] and confirm that plain unenhanced ct is sufficient to discriminate between pathological nodal masses and physiological radiotracer uptake in supradiaphragmatic - mediastinal regions . 
to his end , in the event of uptake along the internal iliac vessels or obturator chains , it was fundamental to obtain late urographic postcontrast acquisitions tmo perch non responsivi a nessuno schema chemioterapico o in terapia di seconda istanza . 
i rimanenti pazienti sono risultati , ai controlli successivi , in remissione di malattia . discussione fino a qualche anno fa la rivalutazione dello stadio di malattia alla fine del trattamento chemio - / radioterapico in pazienti con linfoma si basava sulla valutazione di parametri morfologici , quali le dimensioni e la vascolarizzazione , delle masse linfomatose , delle tumefazioni linfonodali e delle localizzazioni parenchimali , che si eseguiva mediante indagini clinico - laboratoristiche e soprattutto esami strumentali di diagnostica per immagini [ 16 ] , in particolare un ruolo preminente era affidato alla tc total - body . 
si considerava la remissione completa lassenza di anomalie radiologiche residue in siti di pregressa localizzazione di malattia ; la remissione incompleta o la parziale risposta alla terapia era valutata nel caso in cui vi era la persistenza di tessuto con dimensioni maggiori ai 1 , 5 cm di diametro massimo , ridotto per di almeno il 75% rispetto al volume originario ; la progressione di patologia era considerato il riscontro di una nuova localizzazione di malattia ovvero un incremento di oltre il 50% su pregresse lesioni ; infine era considerata recidiva qualora si assisteva alla ricomparsa della malattia dopo un periodo di remissione [ 17 ]  . 
in particolare tale considerazione si conferma dal frequente riscontro di falsa negativit in caso di formazioni linfonodali patologiche seppure di normali dimensioni o viceversa di risultati falsamente positivi in presenza di adenomegalie a carattere reattivo infiammatorio o di splenomegalia correlata alluso di fattori di crescita ematopoietici utilizzati durante la chemioterapia [ 18 ]  . considerando quindi i limiti intrinseci della metodica tc , si comprende lo sviluppo e la sempre pi frequente introduzione nella pratica clinica di innovative tecniche di imaging molecolare come lesame 18f - fdg - pet [ 1921 ] che si basa sulla valutazione dellaumentata glicolisi , dellamplificazione del numero di proteine trasportatrici di glucosio e dellincrementata attivit dellesochinasi che mostrano le cellule neoplastiche e quelle in attiva replicazione ; tali caratteristiche quindi consentono di distinguere un tessuto metabolicamente attivo da uno inerte o da una condizione di fibrosi cicatriziale . 
per questo luso della 18f - fdg - pet e il suo timing sono raccomandati nella valutazione della risposta al trattamento dei vari tipi di linfoma nelle pi recenti linee guida . 
infatti i dati riportati in letteratura hanno confermato negli esperimenti in vitro , che le terapie antiblastiche sono efficaci al 99 , 9% gi dopo soli 2 cicli [ 21 ]  . lassociazione della valutazione metabolica ottenuta 1260 radiol med ( 2012 ) 117 : 12501263 fig . 
axial mdct scan ( a ) shows focal uptake ( arrow ) in the right laterocervical area in correspondence to a nodular mass depicted on unenhanced axial mdct ( arrow ) ( b )  . 
a limmagine pet / tcms assiale mostra unarea di focale aumento dellattivit metabolica ( freccia ) in sede latero - cervicale profonda a destra in corrispondenza di formazione nodulare dimostrata alla tcms assiale senza mdc ( freccia ) ( b )  . 
c la tcms con mdc mostra che la formazione di pertinenza vascolare ( freccia ) nella scansione assiale tcms con mdc . to to correctly identify the course of the ureters and reduce the number of false positive results . 
therefore , the integration of pet and mdct allowed us to reduce the intrinsic limitations of each technique used alone , such as the low anatomical resolution of pet and the inadequate diagnostic accuracy of mdct in evaluating lymphomatous tissue following treatment . 
the result is an examination of high clinical value that reduces the number of interpretation errors by combining an anatomical and functional assessment [ 27 ]  . our study confirms the effectiveness of abvd chemotherapyradiotherapy , with complete remission being achieved in 118 / 132 patients ( 89% ) at the end of therapy . 
these findings allow us to emphasise not mediante la metodica 18f - fdg - pet , e quella morfologica della metodica tc , consente di superare i limiti della pet soprattutto nei casi di localizzazioni parenchimali e di false positivit , permettendo il miglioramento dei risultati diagnostici e delliter terapeutico [ 2225 ]  . 
noto che lindagine 18f - fdg - pet risulta gravata da un elevata percentuale di falsi positivi , riscontrabili in corso di infezione , di infiammazione , di grasso bruno sopraclaveare , di iperplasia timica o di riattivazione midollare dovuta a fattori ematopoietici stimolanti . 
inoltre leliminazione del radiofarmaco attraverso lapparato escretore urinario ed intestinale potrebbe mascherare la presenza di millimetriche adenopatie addominali presenti in sede limitrofa oppure simulare un patologico focale accumulo del radiotracciante nelle strutture stesse . 
 in questi casi , la concomitante acquisizione di immagini tc per la verifica anatomica dei dati funzionali rappresenta un fondamentale ausilio per la valutazione dei reperti non univoci , limitando il numero di falsi positivi e di falsi negativi . dalla nostra analisi emersa limportanza di entrambe i dati a nostra disposizione ( dato morfologico e dato metabolico ) nellindividuazione dei siti di patologia ; in particolare lesame tc ha permesso di definire siti di uptake di dubbia interpretazione e di individuare localizzazioni di patologia intraparenchimali , mentre lindagine 18f - fdg - pet ha consentito di discriminare condizioni di fibrosi cicatriziale e di definire patologiche formazioni linfonodali regolari per dimensioni . 
in questo studio retrospettivo , abbiamo utilizzato lassociazione delle due metodiche per una definizione precisa dellestensione della malattia prima del trattamento e , confrontandone le risposte , in fase precoce e al termine della terapia standard per il lh . radiol med ( 2012 ) 117 : 12501263 1261 fig . 
alla stadiazione ( a ) limmagine di fusione pet / tc non mostra aree di patologico incremento dellattivit metabolica in corrispondenza del polo superiore della milza , al cui livello si riconosce , invece , b alla tcms con mdc e.v unarea focale di irregolare ipodensit , c scarsamente riconoscibile alla tcms acquisita in condizioni basali per la correzione dellattenuazione . only the speed and efficacy with which modern antineoplastic agents act on hl , but also the importance of interim pet / mdct as a prognostic factor for complete remission in the long ter la nostra esperienza concorda con quanto riportato in letteratura [ 18 ] , ossia che la semplice acquisizione basale della tc risulta sufficiente nella discriminazione tra formazioni linfonodali patologiche e fisiologici accumuli del radiotracciante di metabolismo in sede sovradiaframmatica - mediastinica . 
al fine di dirimere tali perplessit , in caso di captazioni presenti lungo i vasi iliaci interni ed a livello delle catene otturatorie , stato indispensabile eseguire delle acquisizioni post - contrastografiche in fase tardiva urografica per consentire di identificare correttamente il decorso degli ureteri e ridurre il numero di risultati falsamente positivi . 
lintegrazione di pet e tc , pertanto , ci ha permesso di ridurre i limiti intrinseci di ognuna delle due tecniche utilizzate singolarmente , quali la scarsa risoluzione anatomica dellindagine pet e linsufficiente accuratezza diagnostica della tc nella valutazione del tessuto linfomatoso residuo dopo terapia . 
si ottiene in tal modo un esame di notevole ausilio clinico , riducendo il numero di errori nellinterpretazione integrando la valutazione anatomica a quella funzionale [ 27 ]  . nel nostro studio si conferma lefficacia del trattamento chemioterapico ( abvd ) radioterapia con lincidenza della remissione completa in 118 / 132 pazienti ( l89% ) al termine della terapia . 
tra questi pazienti che hanno mostrato precoce inattivazione metabolica soltanto 2 ( 2% ) hanno presentato una precoce recidiva rispettivamente a distanza di 30 e 60 giorni dallultimo ciclo di terapia . 
finally , interim pet / mdct represents , in parallel to disease stage and extranodal involvement , one of the most reliable predictors of the need to review the treatment strategy and the time interval for the follow - up [ 29 ]  . in conclusion , our results demonstrate that the early negativity of pet / mdct is a strong predictor of diseasefree survival ; in other words , the likelihood of a recurrence among patients with negative results on interim pet / mdct is extremely low . 
the results of interim pet / mdct should therefore be assessed in comparison with the conventional prognostic indicators ( age , sex , stage , extranodal involvement , bulky mediastinal disease , presence of associated symptoms ) , and their combined analysis may help to individualise medical treatment [ 30 ]  . 
moreover , in a context of diminishing health - care resources , the use of an imaging investigation able to discriminate response to chemotherapy with a high level of diagnostic accuracy would lead to a major reduction in costs by modifying the diagnostic and therapeutic pathway , with the effect of rationalising available economic resources . 
il vpp della metodica in esame stato invece del 42% rivelando come gi da altri autori riferito [ 28 ] che , specialmente in particolari presentazioni della malattia ( ad esempio , la bulky ) , questa indagine pu sottostimare la scomparsa di tessuto patologico attraverso linterferenza dellevoluzione necrotico - cicatriziale che porta alla risoluzione anatomica della malattia . 
la valutazione della pet / tcms in itinere costituisce infine , parallelamente allo stadio e allinteressamento extranodale del lh , uno dei fattori prognostici pi affidabili per la necessit di modificare in itinere la terapia e lintervallo di tempo del follow - up [ 29 ]  . in conclusione , i risultati emersi dal nostro studio dimostrano che la precoce negativizzazione della pet / tc rappresenta un criterio altamente predittivo di sopravvivenza libera da malattia ; ovvero la probabilit che si verifichi una recidiva di malattia tra coloro che sono risultati negativi al controllo precoce pet / tcms risulta estremamente bassa . 
 lesito della pet / tcms precoce deve quindi essere valutata comparativamente ai tradizionali indici di prognosi ( et , sesso , stadio , interessamento extranodale , localizzazione mediastinica bulky , presenza di sintomi associati ) e dalla loro analisi combinata pu quindi essere personalizzata la terapia medica [ 30 ]  . 
inoltre in un contesto sanitario di risorse economiche sempre pi carenti lutilizzo di unindagine strumentale che , con elevata accuratezza diagnostica , permette di discriminare la risposta al trattamento chemioterapico consentirebbe di ottenere unimportante riduzione dei costi , modulando liter diagnostico e terapeutico , razionalizzando in tal modo le risorse economiche a disposizione . 
do you remember that old print showing , in a sort of gaussian curve , mans life from birth to decrepitude ? it looks like more and more people will be pigeon - holed at the last and more unpleasant side of that print . this book is devoted to magnetic resonance imaging ( mri ) findings as the key - factor in diagnosing people affected by dementia ; a many - faceted condition . the reader is guided through a very well planned text : first , how to use this book ? ; dementia : clinical background ; toolbox ; normal ageing ; primary grey matter loss ; vascular dementia ; disorders mainly affecting white matter ; dementia with associated brain swelling . after opening the book one will find a welcome surprise : on four and some part of a fifth page there is a listing ( as yet incomplete : i added at least one more page ) of the abbreviations and acronyms to be found in the text . 
 interestingly in each section there is a history and nosology of most of the described conditions ( and information about the people behind them ) , supplemented with information on aetiology , genetics and histopathology . 
uncommon is the fact that practically no reference is cited in the text , while a list of suggested readings is to be found at the end of each section . the book explains how to study and diagnose dementia and dementia like conditions and differentiate these from physiologic ageing . 
mri is by far the most important tool in this endeavour ( due to its various capabilities and techniques ) , clearly outclassing computed tomography ( ct ) ( yet sometimes due to local situations the only diagnostic tool available ) and well supported by new diagnostic tools such as positron emission tomography ( pet )  . 
however all of the above must be coupled with a battery of laboratory demenza : un grande problema con il quale devono confrontarsi sia i clinici che i neuroradiologi a causa dellincremento nellet della popolazione . 
chi si ricorda il vecchio disegno che descrive , sotto forma di curva gaussiana , le et della vita dalla nascita alla decrepitezza ? sembra proprio che un sempre maggior numero di persone andr a far parte dellultima e meno piacevole parte del disegno . 
 questo volume dedicato alla risonanza magnetica ( rm ) quale fattore chiave nella diagnosi di coloro che sono affetti dalla demenza , una situazione dalle molte sfaccettature . il lettore viene guidato attraverso un testo ben strutturato : in primo luogo , come usare il volume ? poi dati clinici sulla demenza , gli strumenti diagnostici , linvecchiamento fisiologico , la perdita primaria della sostanza bianca , la demenza da causa vascolare , i disturbi interessanti principalmente la sostanza bianca e la demenza con associato rigonfiamento cerebrale . allapertura del volume ci si trover di fronte ad una gradita sorpresa : quattro pagine e parte di una quinta riportanti lelenco ( non completo tuttavia : vi ho aggiunto personalmente almeno unaltra pagina ) delle abbreviazioni e degli acronimi usati nel testo . interessante il trovare allapertura di ciascuna parte , la storia e la nosologia della maggior parte delle affezioni ( con informazioni su coloro che le hanno descritte per primi ) , integrate da informazioni su eziologia , genetica ed istopatologia delle stesse . 
del tutto inusuale il riscontro di quasi nessuna citazione nel testo , mentre una lista di letture consigliate presente alla fine di ogni sezione . nel libro viene spiegato come studiare e diagnosticare la demenza e gli stati simil - demenziali , differenziandoli dai quadri del fisiologico invecchiamento . 
la rm lo strumento diagnostico principe in questo campo , grazie alle sue varie possibilit e tecniche , surclassando chiaramente la tomografia computerizzata ( tc ) ( anche se talvolta , in funzione delle condizioni locali , rappresenta il primo strumento diagnostico a disposizione ) , ben sostenuta anche da nuovi strumenti diagnostici , come la tomografia ad emissione di positroni radiol med ( 2012 ) 117 : 12661267 1267 tests , most of which investigate a possible metabolic source of the condition under question . all throughout the book there is a peculiar feeling , in any case outlined by the various authors : is dementia a clear - cut physical condition or a sort of faint , unclear situation at its initial appearance ? are dementia symptoms which are often elusive and difficult to catch sufficient to formulate a diagnosis and related ( when possible ) treatment ? to take full advantage of all the wisdom poured into the text one will need to be up to date on clinical neurological signs as well as brain anatomy in order to fully appreciate the mri and pet findings beautifully illustrated in all the well - chosen images . 
in ogni caso tuttavia tutto quanto fornito dalle immagini deve essere associato ad un certo numero di esami di laboratorio , per la maggior parte dedicati alla ricerca di una possibile causa metabolica alla base dellaffezione in studio . una strana sensazione aleggia nelle varie parti del volume , sottolineata anche dai vari autori : la demenza una condizione fisica ben definita e precisa , oppure una situazione vaga , non chiara , sfumata nelle sue fasi iniziali ? i sintomi delle demenza che sono spesso elusivi e difficili da cogliere sono sufficienti per porne la diagnosi ed instaurare , se possibile , una terapia ? per trarre un beneficio completo da tutta la sapienza distillata nel testo , il lettore dovr essere ben informato sui segni neurologici clinici e sullanatomia dellencefalo , in modo tale da apprezzare in pieno i reperti rm e pet mostrati in modo superbo in tutte le immagini scelte con cura . 
bazzocchi1 1istituto di radiologia diagnostica , dipartimento di scienze mediche sperimentali e cliniche , universit di udine , via colugna 50 , 33100 udine , italy 2unit medica per i trapianti di fegato , dipartimento di scienze mediche sperimentali e cliniche , universit di udine , udine , italy correspondence to : r . 
 diameter was measured at the level of the extrahepatic bile duct ( ebd ) , right hepatic duct ( rhd ) , left hepatic duct ( lhd ) , anterior and posterior right hepatic ducts ( arhd , prhd ) and left lateral and medial ducts ( lld , lmd )  . 
in general , nonlongitudinal analysis showed minimally larger duct size after 1 year ( mean + 1.40.5 mm ) despite significant differences at most sites of measurement considering all types of strictures ( p < 0.01 ; mann - whitney u test )  . 
 il diametro dei dotti stato misurato a livello di : dotto biliare extraepatico ( dbe ) , dotto epatico destro ( ded ) , dotto epatico sinistro ( des ) , dotto epatico destro anteriore e posteriore ( deda , dedp ) , dotto epatico sinistro mediale e laterale ( desm , desl )  . 
in generale , lanalisi non longitudinale ha mostrato un calibro dei dotti solo minimamente pi ampio dopo 1 anno ( media di + 1 , 40 , 5 mm ) , nonostante una differenza significativa per la maggior parte dei siti di misurazione considerando tutte le stenosi ( p < 0 , 01 ; mann - whitney u test )  . 
la dilatazione biliare dopo trapianto di fegato lieve ed a lento sviluppo , indipendentemente dal tipo di stenosi cui associata , probabilmente in relazione a propriet del grala crm ha un ruolo potenziale come modalit di imaging di prima scelta nella valutazione della dilatazione biliare e della presenza di una stenosi . 
 parole chiave colangiografia risonanza magnetica trapianto di fegato stenosi biliare dotti biliari dilatazione introduction introduzione strictures represent the most frequent biliary complication after orthotopic liver transplantation ( olt ) , with reported frequencies up to 14% [ 1 ]  . 
diagnosis is difficult , as clinical and biochemical manifestations overlap with those of other major nonobstructive conditions , such as rejection , primary dysfunction or viral reinfection of the graft [ 24 ]  . 
however , early diagnosis is crucial to direct patients to prompt treatment , because both the site and time of onset of a stricture have significant impact on the outcome following endoscopic or percutaneous procedures [ 5 ]  . 
ultrasonography ( us ) still represents the first - line imaging modality for evaluating olt - related biliary obstruction , although its sensitivity in assessing the stricture site and degree of proximal biliary dilatation is lower than 50% [ 4 , 69 ]  . 
because of its poor accuracy in assessing the degree of bile - duct dilatation , us is also considered unreliable in monitoring the response to therapy [ 10 ]  . 
however , it has been hypothesised that , at least partially , results depend on intrinsic graft properties capable of reducing the response of donor bile ducts to obstruction [ 11 ]  . 
this information would be helpful in providing reference measurements and confirming whether bile - duct dilatation develops slowly and / or in a limited manner in the graft , irrespective of the intrinsic limitations of us imaging . 
 the purpose of this study was to investigate whether the degree of stricture - related bile - duct dilatation is correlated with the time of observation after olt and the type of underlying stricture . 
we evaluated the biliary tree using magnetic resonance cholangiography ( mrc ) , which represents the noninvasive modality of choice for imaging the biliary tree in its physiological state after olt [ 1315 ]  . le stenosi rappresentano la complicanza biliare pi frequente dopo trapianto ortotopico di fegato ( olt ) , raggiungendo una prevalenza del 14% [ 1 ]  . 
la diagnosi difficile , poich le manifestazioni cliniche e di laboratorio sono sovrapponibili a quelle di altre complicanze maggiori non ostruttive , quali il rigetto , una insufficienza primaria del graft o una sua re - infezione virale [ 24 ]  . 
in ogni caso , la diagnosi precoce essenziale al fine di indirizzare il paziente al trattamento pi appropriato , poich sia la localizzazione che il momento dellesordio di una stenosi hanno un impatto significativo sulloutcome dopo procedure endoscopiche o percutanee [ 5 ]  . 
lecografia ( us ) rappresenta ancora la metodica di imaging di prima linea nella valutazione dellostruzione biliare conseguente al trapianto , bench la sensibilit nella determinazione del sito di stenosi e del grado di dilatazione biliare sia inferiore al 50% [ 4 , 69 ]  . 
daltra parte , stato ipotizzato che almeno in parte essi dipendano da propriet intrinseche del graft in grado di ridurre la risposta dei dotti biliari del donatore allostruzione [ 11 ]  . 
 per quanto a nostra conoscenza , scarse sono le evidenze disponibili sulle variazioni della misura dei dotti biliari dopo olt , e basate sulla colangiografia [ 11 , 12 ]  . 
linformazione sul grado di dilatazione biliare in presenza di stenosi sarebbe utile sia per stabilire delle misure di riferimento , sia per confermare se la dilatazione biliare si sviluppi poco e / o lentamente nel graft ( indipendentemente dai limiti intrinseci dellimaging ecografico )  . 
 su queste basi , lo scopo del presente studio stato di investigare se il grado di dilatazione biliare legato alla presenza di una stenosi sia correlato con il tempo di osradiol med ( 2012 ) 117 : 10971111 materials and methods patient population a computerised search was performed in our institutional database to identify all liver - transplanted patients ( ltps ) with a clinical suspicion of biliary complications who underwent mrc over a 3 - year period ( march 2006 to march 2009 )  . 
of these , we included those with at least one stricture of the extrahepatic bile ducts and / or hepatic confluence , as confirmed by endoscopic retrograde cholangiography ( erc ) and / or percutaneous transhepatic cholangiography ( ptc ) performed within 1 month after the baseline mrc . 
lithiasis alone ( n = 2 ) and sphincter of oddi dysfunction alone ( n = 1 ) ; ( b ) false - positive ( n = 1 ) and false - negative ( n = 1 ) mrc diagnosis as assessed by direct cholangiography ; ( c ) cases of coexisting biliary complications ( including strictures ) in the presence of a biliary stent , which would have introduced a bias in duct size estimation because of reduced intraductal pressure ( n = 10 )  . 
biliary strictures were associated with intraand / or extrahepatic biliary sludge / lithiasis ( n = 11 ) , biliary leakage ( n = 1 ) and papillary stenosis ( n = 1 )  . 
however , the study was performed in accordance with declaration of helsinki criteria . mrc protocol mrc was performed on a 1.5 - tesla system ( magnetom avanto , siemens medical imaging , erlangen , germany ) equipped with a six - element phased - array torso coil working in conjunction with the built - in spine array to increase the signal ( total imaging matrix technology , siemens )  . 
abbiamo studiato lalbero biliare ricorrendo alla colangiografia con risonanza magnetica ( crm ) poich essa rappresenta , al momento , la tecnica di imaging elettiva e non invasiva per rappresentare lalbero biliare nel suo stato fisiologico conseguente allolt [ 1315 ]  . 
 materiali e metodi popolazione di studio allinterno del database della nostra istituzione , stata effettuata una ricerca computerizzata per identificare i pazienti trapiantati di fegato ( ptf ) che fossero stati sottoposti , nellarco di 3 anni ( marzo 2006marzo 2009 ) , ad una crm per sospetto clinico di complicanze biliari . 
di questi , abbiamo incluso coloro che presentassero almeno una stenosi a carico delle vie biliari extraepatiche e / o della confluenza biliare , come confermato da una successiva colangiografia retrograda endoscopica ( cre ) e / o colangiografia percutanea transepatica ( cpt ) effettuate entro un mese dalla crm basale . 
i criteri di esclusione includevano : ( a ) casi di diagnosi crm di ostruzione biliare senza stenosi , ossia litiasi isolata ( n = 2 ) e disfunzione dello sfintere di oddi isolata ( n = 1 ) ; ( b ) diagnosi crm false - positive ( n = 1 ) e false - negative ( n = 1 ) , come verificato ad una successiva colangiografia diretta ; ( c ) casi di complicanze biliari coesistenti ( stenosi incluse ) in presenza di stent biliare ( n = 10 ) , che avrebbe potuto determinare un bias nella stima dei diametri per la riduzione della pressione intraduttale da esso operata . 
oltre a ci , sono stati esclusi 7 pazienti con esame crm vero - negativo , come confermato da un follow - up clinico e / o di imaging di 1 anno . 
 ladesione ai criteri di inclusione stata riscontrata in quarantadue ptf con stenosi biliare ( 35 maschi e 7 femmine ; range di et 4073 anni , media di 57 , 3 )  . 
di questi 42 pazienti , 11 hanno effettuato ulteriori 15 esami successivi per il sospetto clinico di recidiva di stenosi dopo trattamento cre o cpt ( 24 crm per paziente , media di 2 , 4 esami )  . 
al momento della crm basale , i pazienti presentavano una anastomosi biliare coledoco - coledocica in 38 casi , ed una anastomosi bileo - digestiva su ansa alla roux in 4 casi . 
le stenosi biliari erano associate a sludge / calcoli biliari intrae / o extraepatici , leakage biliare e stenosi papil1100 radiol med ( 2012 ) 117 : 10971111 spin - echo ( tse ) sequences were used : ( a ) the first , available from march 2006 to december 2007 [ time to repetition ( tr ) 1 , 700 ms ; time to echo ( te ) 654 ms ; matrix 241256 ; field of view ( fov ) 250250 mm ; 60 - 80 slices ; thickness 1.5 mm ; averages 1 ; gap 0 ; nominal acquisition time 3 min 51 s ; planes of acquisition coronal and , if necessary , axial ] ; ( b ) a more recent , nearly isotropic sequence , available from january 2008 ( tr 2 , 500 ms ; te 682 ms ; matrix 357384 ; fov 380380 mm ; slices 7290 ; thickness 1 mm ; thickness in z direction 1.1 mm ; averages 1 ; gap 0 ; generalized autocalibrating partially parallel acquisition ( grappa ) imaging with an acceleration factor of 3 ; nominal acquisition time 3 min 51 s ; plane of acquisition coronal )  . 
a preliminary half - fourier acquired single - shot turbo spin - echo ( haste ) sequence to assess the anatomical coverage was performed with the following acquisition parameters : tr 1 , 000 ms ; te 88 ms ; slices 20 ; thickness 5 mm ; averages 1 ; gap 20% ; acquisition time 10 s ; planes of acquisition coronal ( matrix 192256 ; fov 178103 mm ) and axial ( matrix 146256 ; fov 262350 mm )  . image analysis two abdominal radiologists ( rg , gc ) evaluated the mrc examinations in consensus on a dedicated workstation ( vitrea , vital images inc . , minnetonka , mn , usa )  . 
reading sessions were organised separately by a third radiologist ( cm ) with the aim of displaying the images randomly and in separate sessions in the case of mrc examinations repeated on the same patient . 
they included the right hepatic duct ( rhd ) , left hepatic duct ( lhd ) , posterior right hepatic duct ( prhd ) , anterior right hepatic duct ( arhd ) , left medial duct ( lmd ) and left lateral duct ( lld )  . 
in the case of anatomical variants [ 1618 ] , measurements were performed as follows : at the level of the largest duct in the case of multiple branches for the hepatic segment iv ( lmd ) ; no measurement was performed in the case of very short or absent lld and rhd ; aberrant branches were named and measured like the normal replaced ducts ; accessory branches were not measured . 
lo studio , comunque , stato eseguito in accordo con i criteri di helsinki . protocollo di crm le crm sono state eseguite su un magnete da 1 , 5 t ( magnetom avanto , siemens medical imaging , erlangen , germania ) , equipaggiato con una bobina di superficie phasedarray a 6 elementi , funzionante insieme alle bobine spine inserite nel lettino porta - paziente , al fine di massimizzare il segnale ( tecnologia total imaging matrix , siemens medical imaging , erlangen , germania )  . 
le sessioni di lettura sono state organizzate separatamente da un terzo radiologo ( c.m. ) , con lobiettivo di presentare le immagini in ordine casuale ed in sessioni separate nel caso di crm ripetute sullo stesso paziente . 
1 sites of bile - duct size measurement : extrahepatic bile duct ( ebd ) , right hepatic duct ( rhd ) , anterior right hepatic duct ( arhd ) , posterior right hepatic duct ( prhd ) , left hepatic duct ( lhd ) , left medial duct ( lmd ; corresponding to the duct for segment iv ) , left lateral duct ( lld )  . 
1 siti di misurazione del diametro delle vie biliari : dotto biliare extraepatico ( dbe ) , dotto epatico destro ( ded ) , dotto epatico destro anteriore ( deda ) , dotto epatico destro posteriore ( dedp ) , dotto epatico sinistro ( des ) , dotto epatico sinistro mediale ( desm , corrispondente al dotto per il segmento iv ) , dotto epatico sinistro laterale ( desl )  . 
la misurazione dei calibri dei dotti biliari stata effettuata sopra il livello della stenosi . reference values for normal duct calibre were 8.0 mm for the cbd , 3 mm for the rhd and 2 mm for the lhd [ 19 ]  . 
strictures were rated as mild ( 30% of luminal involvement ) , moderate ( 31 - 70% ) and severe ( 71 - 100% )  . data analysis a nonlongitudinal analysis was performed on a per - examve . 
la misurazione stata effettuata a livello del punto pi largo dei dotti , a monte del sito di stenosi , ed espressa in mse un dotto era coinvolto in tutta la sua lunghezza , si optato per la esclusione dalla misurazione . 
esse includevano il dotto epatico destro ( ded ) , il dotto epatico sinistro ( des ) , il dotto epatico destro posteriore ( dedp ) , il dotto epatico destro anteriore ( deda ) , il dotto epatico sinistro mediale ( desm ) ed il dotto epatico sinistro laterale ( desl )  . 
qualora fossero presenti varianti anatomiche [ 1618 ] , le misurazioni sono state effettuate come di seguito : a livello del dotto di maggior calibro in caso di rami multipli per il segmento iv ( desm ) ; non stata effettuata misurazione per desm o ded moli rami aberranti sono stati nominati e misurati come i to corti od assenti ; dotti regolari sostituiti ; i rami accessori sono stati esclusi dalle misurazioni . 
la classificazione finale delle stenosi stata basata su un confronto fra le ricostruzioni maximum intensity projection ( mip ) ed il complesso dei referti e delle immagini delle cre e cpt effettuate dopo la crm . 
le stenosi , di conseguenza , sono state inquadrate come lievi ( 30% di restringimento luminale ) , moderate ( 31%70% ) e severe ( 71%100% )  . analisi dei dati stata effettuata una analisi non - longitudinale per - esame , comparando per ogni sede di misurazione i diametri dei dotti biliari di due gruppi di crm : quelle eseguite entro 1 anno dallolt vs . 
 stata eseguita anche una analisi longitudinale nei pazienti con esami ripetuti , comparando il diametro dei dotti biliari in ciascuna sede di misurazione tra le crm basali e quelle effettuate entro e dopo 1 anno da essa . 
infine , il diametro dei dotti biliari stato confrontato per ciascuna sede di misurazione tra i differenti tipi di stenosi , sia nel gruppo di esami eseguiti entro 1 anno dallolt che in quello degli esami eseguiti dopo 1 anno dallolt . 
4 paziente maschio , di 62 anni , sottoposto a ritrapianto per insufficienza del grail quadro di stenosi biliare stato classificato come misto , a causa di stenosi coinvolgenti sia la confluenza epatica che il dotto extraepatico allanastomosi bilio - digestiva . risultati distribuzione delle stenosi la tabella 1 riassume il numero e la distribuzione dei reperti nei pazienti . 
la severit delle stenosi stata classificata dai lettori radiol med ( 2012 ) 117 : 10971111 1103 ination basis by comparing at each site of measurement bile - duct diameters of two groups of mrc : those performed within 1 year from olt vs . 
 a longitudinal analysis was carried out in patients with repeated examinations by comparing bile - duct diameter at each measurement site among baseline mrc examinations and those performed within and after 1 year from baseline , respectively . 
finally , bile - duct diameter was compared at each site of measurement among different types of strictures , both in the group of examinations performed within 1 year and in the group after 1 year from olt . 
analysis was performed using commercially available software ( medcalc 9.2.0.1 , mariakerke , belgium )  . results stricture distribution the frequency and distribution of findings among patients are shown in table 1 . 
mean differences between the two groups of come lieve in 15 / 57 casi ( 26 , 3% ) , moderata in 24 / 57casi ( 41 , 1% ) e severa in 18 / 57 casi ( 31 , 6% )  . correlazione fra il calibro dei dotti biliari ed il tempo di osservazione dallolt : analisi non longitudinale i diametri medi dei dotti biliari nei ptf con stenosi biliare sono riportati in tabella 3 . 
la sola eccezione , per il riscontro di un calibro al di sotto della soglia di dilatazione stabilita , stata osservata al dbe ( indipendentemente dal tipo di stenosi )  . 
 dopo 1 anno dal trapianto , stato osservato un diametro biliare medio maggiore rispetto al periodo precedente in tutte le sedi di misurazione , fatta eccezione per il desm nei casi con stenosi anastomotica e per il desl in quelli con stenosi simil - ischemica ( + 0 , 0 mm )  . 
nel confronto fra i dotti intraepatici , la minore dilatazione rispetto al periodo precedente stata dimostrata a livello di desm e di desl ( rispettivamente + 0 , 7 e + 1 , 1 mm considerando tutti i tipi di stenosi )  . 
il des risultato il dotto intraepatico maggiormente dilatato , con un calibro di 5 , 03 , 1 entro 1 anno dallolt e di 6 , 72 , 6 mm dopo 1 anno dallolt . 
le differenze corrispondevano ad una significativit statistica ( p < 0 , 01 ) nelle sedi di ded , des , deda , dedp e desl , ma solo considerando tutti i tipi di stenosi . 
le crm sono state effettuate entro 1 anno dallolt in 5 pazienti ( per un totale di 6 esami ) e dopo 1 anno dallolt in 5 pazienti ( per un totale di 7 esami )  . 
 correlazione fra il calibro dei dotti biliari ed il tipo di stenosi stato osservato che , a qualunque tempo dallolt , i diatable 1 distribution of biliary stricture types in the study population on a per - examination and per - patient basis . 
cases of evolution ( or not ) to different pattern of stricture in patients who performed repeat 3d magnetic resonance cholangiograms ( mrcs ) are also reported mrc findings ltps at baseline mrc ( n ) mrcs ( n ) patients with repeat examinations ( n = 11 ) radiol med ( 2012 ) 117 : 10971111 ltps showing evolution to mixed - type stricture ( n ) ltps showing no stricture evolution ( n ) ltps , liver - transplanted patients aadditional examinations in these patients , who showed an anastomotic stricture at baseline mrc , are included in the number of mrcs of mixed strictures tabella 1 distribuzione per - esame e per - paziente dei tipi di stenosi biliare nelle popolazione di studio . 
sono riportati i casi di evoluzione ( o meno ) verso un pattern di stenosi differente nei pazienti sottoposti a colangiografie con risonanza magnetica ( crm ) ripetute ptf alla crm basale ( n ) crm ( n ) pazienti sottoposti ad esami ripetuti ( n = 11 ) ptf con evoluzione verso una stenosi mista ( n ) ptf senza evoluzione a stenosi ( n ) 1104 anastomotic strictures ischemic - like strictures mixed strictures total diagnosi alla crm stenosi anastomotica stenosi simil - ischemica stenosi mista totale ptf , pazienti trapiantati di fegato agli esami ripetuti in questi pazienti , che mostravano una stenosi anastomotica alla crm basale , sono inclusi nel computo del numero di colangiografierm dei casi di stenosi mista table 2 per - examination distribution of biliary stricture types in liver - transplanted patients . 
 differences showed statistical significance ( p < 0.01 ) only considering all types of stricture at the rhd , lhd , arhd , prhd and lld . correlation between bile - duct size and time of observation from olt : longitudinal analysis results of the longitudinal analysis on 11 patients are shown in table 4 . 
 correlation between bile - duct diameter and stricture types at any time from olt , mean bile - duct diameters were shown to be not significantly different at each site of measurement among cases with different types of stricture ( p > 0.01 ) ( tables 5 and 6 )  . 
 discussion in the case of biliary obstruction after olt , the degree of bile - duct dilatation poorly correlates with clinical presentation [ 20 ] and has little or no significance for establishing the diagnosis of stricture in clinical practice [ 10 ]  . 
moreover , bile - duct size is not a reliable indicator of adequate biliary drainage in the follow - up of ltps or in the assessment of response to endoscopic treatment of strictures [ 10 , 2025 ]  . 
although us remains the first - line imaging modality in evaluating ltps , it is affected by lack of panorama , difficulty in examining patients in the postoperative period and presence of biliary sludge and / or casts obscuring ductal dilatation [ 4 ]  . 
however , it has been hypothesised that irrespective of us limitations dilatation of the biliary system in transplanted livers develops slowly and to a lesser extent compared with nontransplanted livers [ 22 ]  . 
 denervation , ischaemia - reperfusion injury , or preservation injury have been proposed as causes for reduced response of the ducts to obstruction [ 20 ] , together with the development of parenchymal fibrosis as a consequence of the injury sustained in the perioperative period [ 10 ]  . 
 little is known about the size of bile ducts after olt as metri medi dei dotti biliari non mostravano differenze significative in ciascuna sede di misurazione fra casi con differenti tipi di stenosi ( p > 0 , 01 ) ( tabelle 5 e 6 )  . 
 discussione nellevenienza di ostruzione biliare dopo olt , il calibro dei dotti biliari correla scarsamente con la presentazione clinica [ 20 ] , avendo minimo o nessun significato , nella pratica clinica , nello stabilire la diagnosi di stenosi [ 10 ]  . 
 il calibro dei dotti biliari , inoltre , non indicatore affidabile di drenaggio biliare efficace nel follow - up dei ptf o nella valutazione della risposta al trattamento endoscopico delle stenosi [ 10 , 2025 ]  . 
 nonostante lus rimanga la metodica di imaging di primo livello nella valutazione dei ptf , essa limitata dalla scarsa panoramicit , dalla difficolt nellesaminare i pazienti nel periodo post - operatorio , e dalla presenza di sludge o di detriti biliari in grado di mascherare la dilatazione dei dotti [ 4 ]  . 
stato ipotizzato , tuttavia , che indipendentemente dalle limitazioni dellus la dilatazione dellalbero biliare si sviluppi lentamente nei fegati trapiantati , ed in ogni caso con una entit minore rispetto a quelli non trapiantati [ 22 ]  . 
 quali cause per la ridotta risposta dei dotti allostruzione sono stati chiamati in causa la denervazione , il danno da ischemia - riperfusione ed il danno da preservazione [ 20 ] , oltre che lo sviluppo di fibrosi parenchimale come conseguenza del danno peri - operatorio [ 10 ]  . 
 [ 11 ] hanno investigato il diametro dei dotti extraepatici di ricevente e donatore utilizzando procedure di colangiografia diretta , rispettivamente in pazienti con disfunzione dello sfintere di oddi e senza ostruzione biliare . 
per quanto a nostra conoscenza , nessun precedente studio basato sulla crm si occupato di misurare il calibro dei dotti biliari in pazienti con stenosi post - olt comprovate alla colangiografia diretta . 
inoltre , mentre le procedure di colangiografia diretta fanno uso di mezzo di contrasto per distendere i dotti , causando una potenziale sovrastima del calibro [ 11 ] , la crm li rappresenta in maniera non invasiva nello stato di fisiologica risposta alla presenza di una stenosi [ 2 ]  . 
di conseguenza , questa tecnica ideale nello stabilire il grado e levoluzione della dilatazione biliare in ptf con stenosi , e se e esse siano influenzate dal tipo di stenosi sottostante . 
 [ 12 ] investigated the calibre of extrahepatic recipient and donor bile ducts by using direct cholangiography in patients with sphincter of oddi dysfunction and without biliary obstruction , respectively . 
furthermore , whereas direct cholangiography procedures use contrast medium to distend the ducts , causing potential size overestimation [ 11 ] , mrc noninvasively displays them in the physiological state of response to the presence of a stricture [ 2 ]  . 
thus , this technique is ideal for assessing the degree and evolution of biliary dilatation in ltps with strictures and to evaluate whether they are influenced by the type of underlying stricture . 
 in our series , bile ducts were shown to be dilated within 1 year from olt ( except for the ebd ) , irrespective of the underlying type of stricture ( anastomotic , ischaemic - like , or mixed )  . 
overall , dilatation was mild , in the range of 2.9 ( at lmd and lld ) to 5.0 mm ( at lhd ) , considering all types of strictures . 
although no direct correlation was performed in this study , our findings somehow correlate with the limitations of us in diagnosing post - olt biliary obstruction [ 4 , 79 ] , suggesting that they depend only in part on technical factors . 
nonetheless , despite showing statistical significance at the rhd , lhd , arhd , prhd and lld when considering all types of stricture , the difference in size was minimal , not exceeding 1.5 mm ( in mixed strictures )  . 
in generale , la dilatazione si rivelata lieve , compresa fra 2 , 9 ( a livello di desm e desl ) e 5 , 0 mm ( a livello di des ) considerando tutti i tipi di stenosi . 
anche se non stata effettuata nessuna comparazione diretta in questo studio , i nostri risultati correlano , in generale , con i limiti dellus nella diagnosi di ostruzione biliare post - olt discussi sopra [ 4 , 79 ] , a suggerire che tali risultati dipendano solo in parte da limiti tecnici . 
probabile , piuttosto , che la denervazione od altre propriet del graft possano spiegare i nostri risultati ( per esempio , edema peribiliare o fibrosi che riducano la compliance biliare ) [ 10 , 20 ]  . 
nondimeno , nonostante fosse significativa nelle sedi del ded , des , deda , dedp e desm considerando tutti i tipi di stenosi , la differenza di calibro fra i due periodi era minima , non superiore a 1 , 5 mm ( nelle stenosi miste )  . 
 come nel caso degli esami effettuati entro 1 anno dallolt , non stata riscontrata una differenza che suggerisse relazioni tra il calibro duttale ed il tipo di stenosi sottostante ( p > 0 , 01 )  . 
 possibile che , dopo 1 anno dal trapianto , la risposta dei dotti sia ancora influenzata da propriet del graft , sebbene ad un livello minore rispetto al precedente periodo . 
la nostra ipotesi che la tendenza alla dilatazione , favorita dallaumento della pressione intraduttale , sia bilanciata da svariati fattori , alcuni transitori ( per esempio , ledema post - operatorio ) , altri persistenti e / o accentuati con il trascorrere del tempo ( per esempio , la fibrosi parenchimale )  . 
sono necessari ulteriori studi , possibilmente con correlazione patologica , allo scopo di determinare con precisione perch la dilatazione biliare si verifichi ad un grado minore di quello atteso nei pazienti trapiantati . 
la differenza pi piccola prima e dopo 1 anno dallolt stata osservata a livello di desm e desl , con variazioni minime pari a + 0 , 0 mm nei casi con stenosi anastmotiche e simil - ischemiche . 
considerato che , radiol med ( 2012 ) 117 : 10971111 1109 graft properties after 1 year from olt , but to a lesser degree compared with the previous period . 
smaller differences before and after 1 year from olt were found at the lmd and lld , with minimum values of + 0.0 mm in cases with anastomotic and ischaemia - like strictures , respectively . 
as the bile ducts of the left lobe are known to dilate earlier [ 2 ] , it is likely that their response to strictures is nearly maximal within a relatively short period of time from olt . 
 by analysing mrc examinations repeated before and after 1 year ( 15 examinations ) from the baseline study ( 11 examinations ) , a trend towards increasing duct size was shown . 
from a clinical point of view , it is arguable that such a slight degree of dilatation might be easily missed on us because of the above - mentioned limitations of us . 
in our series , dilatation of bile ducts per se even when conspicuous was an unreliable marker for the site and type of stricture based on its degree and / or anatomical distribution . 
it is arguable that a panoramic and noninvasive imaging modality such as mrc has a potential role as a first - line tool in symptomatic ltps in order to directly assess strictures ( and further biliary complications ) [ 3 ]  . 
in fact , mrc provides equivalent imaging to erc in identifying and quantifying post - olt strictures and has the capability to noninvasively identify true - negative patients who are at risk of overtreatment [ 14 ]  . as with any retrospective study , ours has some limitations . 
the lack of this estimation reflects what frequently happens in clinical practice [ 8 ] , in which the only come noto , i dotti biliari dei settori di sinistra si dilatano pi precocemente di quelli controlaterali [ 2 ] , probabile che la loro risposta alla presenza di una stenosi sia pressoch massimale entro un periodo relativamente breve dallolt . 
in particolare , stato riportato [ 10 ] che lincremento medio del calibro duttale di 1 , 9 e 1 , 8 mm durante il follow - up dei ptf con stenosi anastomotica , rispettivamente responsivi e non - responsivi al trattamento . 
da un punto di vista della ricaduta clinica , intuibile che una dilatazione cos lieve abbia maggiori probabilit di essere misconosciuta usando lus , a causa dei limiti sopra discussi . 
nella nostra casistica , la dilatazione biliare , anche quando pi cospicua , si rivelata , di per s , un marker inaffidabile della sede e del tipo di ostruzione , considerando il suo grado e / o la sua distribuzione anatomica . 
desumibile che una modalit di imaging panoramica e non invasiva quale la crm abbia un ruolo potenziale come approccio di prima linea nei ptf sintomatici , al fine di identificare e quantificare direttamente la stenosi ( oltre che ulteriori complicanze biliari ) [ 3 ]  . 
del resto , la crm si dimostrata equivalente alla cre nella identificazione e quantificazione delle stenosi post - olt , e possiede la capacit di identificare in maniera non invasiva i pazienti veri - negativi a rischio di sovratrattamento [ 14 ]  . come ogni studio retrospettivo , il nostro ha dei limiti . 
la mancanza di questa stima riflette , del resto , quello che spesso accade nella pratica clinica [ 8 ] , quando il solo riferimento affidabile per valutare levoluzione temporale di un qualunque effetto delle stenosi ( o , indirettamente , delle propriet del graft ) sullalbero biliare la data dellolt . 
the resulting potential underestimation of duct size after 1 year from olt in nonlongitudinal and longitudinal evaluations does not affect the general results of reduced bile - duct dilatation in ltps . 
 second , because of the per - examination analysis , measurements on 11 patients with a combined additional 15 mrc examinations might seem redundant , potentially affecting the nonlongitudinal analysis . 
nonetheless , it would be unreasonable to exclude these cases , as the study reflects clinical practice , in which multiple mrc studies may be performed at different times of a patients natural history , i.e. 
despite occurring in the same patient , recurrent strictures have been previously treated with erc or ptc and develop as independent events at a certain time from olt , determining proportional biliary dilation upstreathird , the differential contribution to biliary dilatation of coexisting obstructive complications ( in particular , 11 cases with lithiasis ) was impossible to determine , mainly because of the variability in stone position , i.e. 
on the other hand , our results reflect clinical practice , in which coexisting obstructive complications and their effects on the biliary tree cannot be dissociated , regardless of stricture severity [ 1 , 2 ]  . 
as the coexistence of several obstructive complications occurred in a minority of cases ( 13 of 57 examinations ) , our results were probably not affected by this potential limitation . 
based on the readers assessments ( and considering mrc equivalent to erc in quantifying strictures [ 14 ] ) , mild ( 26.3% ) , moderate ( 41.1% ) and severe strictures ( 31.6% ) were substantially well balanced , thus avoiding any bias due to the prevalence of one type . 
according to the nonlongitudinal evaluation , biliary dilation in ltps is mild , irrespective of the time of symptom onset from olt ( within or after 1 year )  . 
la conseguente , potenziale sottostima del calibro duttale dopo 1 anno dallolt nelle valutazioni non - longitudinale e longitudinale non inficia , peraltro , il risultato complessivo di una dilatazione biliare ridotta nei ptf . 
in secondo luogo , a causa dellanalisi per - esame , le misurazioni effettuate sugli 11 pazienti con 15 esami ripetuti potrebbero sembrare ridondanti , inficiando potenzialmente lanalisi non - longitudinale . 
sarebbe stato irragionevole , tuttavia , escludere questi casi , poich lo studio riflette la pratica clinica , nella quale la crm pu essere ripetuta in momenti differenti della storia naturale del paziente , vale a dire quando una stenosi recidiva od evolve ( per esempio , verso il tipo misto , come in 4 pazienti della nostra casistica )  . 
bench si verifichino nello stesso paziente , le stenosi recidive hanno ricevuto un precedente trattamento cre o cpt e si sviluppano come eventi indipendenti ad un certo tempo dallolt , determinando una dilatazione biliare proporzionale a monte . 
in terzo luogo , nello studio stato impossibile determinare il contributo relativo alla dilatazione biliare di complicanze ostruttive co - esistenti ( specialmente gli 11 casi di litiasi ) , soprattutto a causa della variabilit di sede dei calcoli , potenzialmente prossimali o distali rispetto alla stenosi o ad occupare uno specifico ramo biliare ( quindi , senza effetto combinato con la stenosi sui restanti rami )  . 
daltra parte , i nostri risultati ricalcano quanto accade nella pratica clinica , nella quale le complicanze ostruttive co - esistenti ed i loro effetti sullalbero biliare sono indistricabili , indipendentemente dalla severit della stenosi [ 1 , 2 ]  . 
poich la co - esistenza di pi complicanze ostruttive stata riscontrata in una minoranza di casi ( 13 / 57 esami ) , i nostri risultati probabilmente non sono inficiati da questo limite potenziale . 
infine , stato impossibile stabilire se la dilatazione dei dotti fosse correlata con la severit delle stenosi , a causa della assenza di una correlazione diretta fra crm e colangiografia diretta . 
sulla base della valutazione dei lettori ( e considerando la crm equivalente nella quantificazione delle stenosi [ 14 ] ) , le stenosi lievi ( 26 , 3% ) , moderate ( 41 , 1% ) e severe ( 31 , 6% ) sono risultate sostanzialmente ben bilanciate , cos da evitare che la prevalenza delluno o dellaltro tipo avesse una ricaduta effettiva sui risultati . 
una analisi non - longitudinale dei nostri risultati dimostra che la dilatazione nei ptf lieve , indipendentemente dallesordio temporale dei sintomi rispetto allolt ( entro o dopo 1 anno )  . 
il grado di dilatazione e la distribuzione anatomica non sono markers della sede e radiol med ( 2012 ) 117 : 10971111 1111 markers for the site and type of the underlying stricture . 
from a clinical point of view , further studies are required to assess whether mrc might replace us as the first - line tool to directly identify and quantify suspected biliary strictures after olt . del tipo della stenosi sottostante . 
knauth springer - verlag , berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 540 - 88589 - 4 e - isbn : 978 - 3 - 540 - 88590 - 0 doi 10.1007 / 978 - 3 - 540 - 88590 - 0 published online : 10 february 2012 springer - verlag 2012 sports in all their different facets are achieving ever increasing importance in daily life due to improved socio - economical conditions , and they mirror health and well - being in adults as well as children . 
 differences in pathological findings involve the growing skeleton and differences in the proper diagnostic tools [ front - line ultrasonography ( us ) ] to be used to properly investigate the suspected lesion , in order to reduce the radiation burden and formulate a correct diagnosis . the book edited by dr . 
it is divided into three parts : general aspects of sport injuries in youth ( classification , epidemiology , clinical examination ; normal anatomy and variants simulating injury ; incidental findings and pseudotumours in sport injuries ; current role of ultrasonography ) , injuries by anatomical location ( shoulder ; elbow ; wrist and hand ; pelvis and groin ; hip ; knee ; ankle and foot ; spine ) and common injuries in popular sports ( soccer injuries ; common injuries in mountain skiing , water sports , tennis and gymnastics )  . 
 all throughout the book the text and the very well reproduced , accurate choice of images , indicate how much gli sport , in tutte le loro diverse sfaccettature , stanno assumendo una sempre maggor importanza nella vita quotidiana a seguito del miglioramento delle condizioni socioeconomiche e rappresentano una cartina di tornasole dello stato di salute e benessere sia negli adulti che nei bambini . 
 le attivit sportive possono rappresentare una semplice attivit ricreativa per la maggior parte dei praticanti , ma diventare anche , con un allenamento sempre pi intensivo , una attivit atletica e professionistica . lattivit fisica procura certamente dei benefici , non scevra per da possibili inconvenienti , soprattutto quando si tengano in considerazione le differenze di et : i bambini e gli adolescenti sono infatti diversi dagli adulti in funzione di come i loro corpi si sviluppano e crescono . 
 differenze nei reperti patologici che comprendono sia lo scheletro in evoluzione che quelle negli strumenti diagnostici da utilizzare in modo adeguato ( ecografia in prima linea ) per studiare la sospetta lesione , in modo tale da ridurre il carico delle radiazioni e formulare una diagnosi corretta . il volume curato dal dott . 
karantanas , a capo di un gruppo internazionale di esperti , dedicato allargomento delle lesioni da sport nel giovane , coprendolo interamente ( ad eccezione delle lesioni craniche )  . 
esso diviso in tre parti : aspetti generali delle lesioni da sport nella giovinezza ( classificazione , epidemiologia , esame clinico ; anatomia normale e varianti simulanti una lesione ; reperti occasionali e pseudotumori nelle lesioni da sport ; ruolo attuale dellecografia ) , lesioni a secondo della localizzazione anatomica ( spalla ; gomito ; polso e mano ; bacino ed inguine ; anca ; ginocchio ; caviglia e piede ; rachide ) e lesioni comuni in sport popolari ( nel calcio ; lesioni comuni nello sci , sport acquatici , tennis e ginnastica )  . in tutto il volume il testo e le immagini ben riprodotte radiol med ( 2012 ) 117 : 12641265 1265 knowledge one requires in order to properly diagnose what is behind a young injured patient , most of all if he / she is a radiologist not fully aware of the different possibilities . 
stress is also given to the ever increasing role radiologists play not only in diagnosing but also in caring for the injured child in view of prognosis , therapy and recovery . 
 one also will realize how important it is to not over train children in what should be a recreational and not hard labour in order to meet parents or trainers wishes and expectations . im sure this book will be very much appreciated by radiologists , orthopaedics , paediatricians , physiotherapists and sports trainers . 
 ed accuratamente scelte , mettono in evidenza quanta conoscenza sia necessaria per diagnosticare in modo corretto ci che pu essere nascosto in un giovane paziente offeso , soprattutto se lui / lei un radiologo non ben informato delle differenti possibilit . 
 viene poi segnalata la sempre maggior importanza del ruolo giocato dal radiologo non solo nella diagnosi ma anche nella cura del bambino ferito in funzione di prognosi , terapia e recupero . 
maria delle croci , v.le randi 5 , 48100 ravenna , italy 2istituto di radiodiagnostica , universit degli studi di ferrara , corso giovecca 203 , 44100 ferrara , italy 3servizio di anatomia patologica , ospedale civile s . 
between january 2004 and january 2011 , 798 patients were examined with colour doppler ultrasound ( cdus ) for disease of the scrotu fourteen patients with cdus findings suspicious for sti were subjected to magnetic resonance imaging ( mri )  . 
lrm ha confermato la presenza di lesioni prevalentemente ipointense nelle sequenze dipendenti dal t1 e dal t2 , prive di contrast enhancement e con vascolarizzazione principalmente perilesionale in 13 pazienti . 
dalla nostra esperienza ecd , ceus e rm si sono dimostrate metodiche indispensabili per un corretto approccio clinico - terapeutico nel sospetto di ist . keywords scrotum magnetic resonance imaging colour doppler ultrasound infarction ultrasonography parole chiave testicolo rm eco - color doppler infarto ecografia 1162 introduction radiol med ( 2012 ) 117 : 11611175 introduzione segmental testicular infarction ( sti ) is a rare ischaemic process with a generally idiopathic aetiology . 
the most frequently reported presentation is acute scrotum , a nonspecific clinical setting in which imaging has a primary role in the differential diagnosis [ 1 , 2 ]  . 
the literature describes several radiological findings that can help the radiologist differentiate an sti from a hypovascular testicular tumour , thus making possible a conservative therapeutic approach [ 1 , 37 ]  . 
 we report our experience through a description of the most significant radiological findings observed in sti , evaluated with colour doppler ultrasound ( cdus ) , contrast - enhanced ultrasound ( ceus ) and magnetic resonance imaging ( mri ) at onset and during follow - up . linfarto segmentale testicolare ( ist ) un processo ischemico raro , ad eziologia solitamente idiopatica . 
la sintomatologia di esordio pi frequentemente riportata in letteratura lo scroto acuto , un quadro clinico aspecifico in cui limaging assume un ruolo di primo piano nella diagnosi differenziale [ 1 , 2 ]  . 
in letteratura sono stati descritti alcuni reperti radiologici che possono indirizzare il radiologo nella differenziazione dellist da un tumore testicolare ipovascolare , permettendo cos un approccio terapeutico conservativo [ 1 , 37 ]  . 
gli autori riportano la propria esperienza descrivendo i reperti radiologici pi rilevanti osservati nellist , valutato con eco - color doppler ( ecd ) , ecografia con mezzo di contrasto ( ceus ) e risonanza magnetica ( rm ) allesordio e nel follow - up . materials and methods patient selection materiali e metodi selezione dei pazienti the study population was selected from a database of 798 patients referred to our us division over a 7 - year period ( january 2004 to january 2011 ) for urgent or priority testicular examination for suspected acute or subacute scrotal disease . 
the diagnosis of sti was hypothesised in 14 patients ( 1.75% of our database ) examined with cdus and mri at onset and after a follow - up period varying from 20 to 200 days to evaluate progression . 
the criteria adopted for establishing a diagnosis of sti were : at us , the presence of hypoisoechoic intratesticular echostructural changes , with no microcalcification , no mass effect , and no or markedly reduced cdus signal , in the absence of signs of infiltration of parenchymal vessels , capsule and scrotal tunics ; at mri , the presence of abnormal intratesticular signal with no contrast enhancement ; at cdus and mri follow - up , the absence of progression and / or presence of a reduction in size due to lesion involution , with absent or reduced flow ; negative tumour markers for primary malignant testicular disease ( alpha fetoprotein , lactate dehydrogenase , human beta chorionic gonadotropin ) ; no history of testicular trauma and no clear sign of acute inflammation , with the exception of two cases of subacute epididymitis . five patients with suspected sti underwent ceus at onset and during follow - up in order to analyse lesion contrast enhancement patterns and document their progression . imaging techniques all patients underwent cdus performed by experienced la popolazione dello studio stata selezionata da un database di 798 pazienti , che in un periodo di 7 anni ( gennaio 2004gennaio 2011 ) sono stati inviati al nostro servizio di ecografia per un esame testicolare in regime di urgenza o prioritario ambulatoriale , nel sospetto di una patologia acuta o subacuta dello scroto . 
la diagnosi di ist stata ipotizzata in 14 pazienti ( 1 , 75% del nostro database ) esaminati con ecd e rm allesordio e dopo un intervallo di tempo variabile da 20 a 200 giorni , per documentarne levoluzione . 
i criteri adottati per fare diagnosi di ist sono stati : allesame ecografico presenza di alterazioni ecostrutturali intratesticolari ipo - isoecogene , senza microcalcificazioni , prive di effetto massa , con segnale color doppler assente o marcatamente ridotto allinterno , in assenza di segni di infiltrazione dei vasi parenchimali , capsulari e delle tuniche scrotali ; allesame rm presenza di area di alterato segnale intratesticolare priva di contrast enhancement ; agli esami ecd e rm di follow - up assenza di progressione e / o presenza di riduzione dimensionale per fenomeni involutivi della lesione con assente o ridotta vascolarizzazione ; markers tumorali per patologia testicolare maligna primitiva negativi ( alfa - fetoproteina , lattato deidrogenasi , gonadotropina corionica umana beta ) ; assenza di traumi testicolari in anamnesi e di segni conclamati di flogosi acuta in atto , ad eccezione di 2 casi con epididimite subacuta . in 5 pazienti con sospetto ist stata eseguita ceus allesordio e nel follow - up allo scopo di evidenziare le caratteristiche contrastografiche delle lesioni e documentarne levoluzione . radiol med ( 2012 ) 117 : 11611175 1163 operators who used a high - resolution transducer ( 7 - 17 mhz linear - array probe ) with b - flow ( b - mode flow ) , colour doppler and power doppler ( ge healthcare logic 7 , philips iu22 )  . 
automatic settings for testicular examination were used , and the operator modified the pulse repetition frequency ( prf ) , focal zone , gain and wall filter to obtain optimal colour doppler flow . ceus was performed using sulphur hexafluoride microbubbles ( sonovue , bracco ) , with the injection of a 2 to 2.5 - cc bolus followed by 10 cc of saline solution . 
 images were acquired in the three orthogonal planes with t2 - weighted fast spin - echo ( fse ) sequences and in the axial plane with t2 - weighted spoiled gradient echo ( gre ) sequences to detect haemoglobin breakdown products at the site of haemorrhagic infarction . 
the examination took approximately 25 - 30 min . image and data analysis us and mri were assessed for size , morphology , echogenicity , signal intensity , presence / absence of vascularity and pattern of contrast enhancement of the lesions in their various phases of progression . 
we also gathered information about patient age , clinical presentation and possible causes of testicular infarction . results tecniche di imaging tutti i pazienti sono stati esaminati con ecd da ecografisti esperti utilizzando una sonda ad alta risoluzione ( sonda lineare da 717 mhz ) con modulo color - power doppler e b flow ( ge heathcare logic 7 , philips iu22 , usa )  . 
stata utilizzata limpostazione automatica per lesame testicolare e loperatore ha modificato la pulse repetition frequency ( prf ) , la zona focale , il guadagno e il filtro di parete per ottenere un ottimale flusso color doppler . la ceus stata eseguita utilizzando microbolle di esafloruro di zolfo ( sonovue , bracco , italia ) , con iniezione di 22 , 5 cc a bolo seguita da 10 cc di soluzione fisiologica . 
stata impiegata apparecchiatura philips archieva 1 , 5 tesla con bobina di superficie circolare da 14 cm , campo di vista 1012 cm , matrice 256256 , spessore di strato di 3 msono state acquisite immagini sui tre piani ortogonali utilizzando sequenze fast spin - eco pesate in t2 e immagini assiali con sequenza spoiled gradientecho ( ge ) pesata in t2 per evidenziare i prodotti di degradazione dellemoglobina negli esiti di infarti emorragici . 
 dopo introduzione di acido dietilen - triamino - penta - acetico chelato con gadolinio ( gd - dtpa ) per via endovenosa sono state acquisite immagini assiali e coronali t1 pesate . 
la durata dellesame stata di circa 2530 min . interpretazione delle immagini e analisi dei dati sono state analizzate le immagini ecografiche ed rm studiando le dimensioni , la morfologia , lecogenicit , lintensit di segnale , la presenza / assenza di vascolarizzazione ed il pattern di contrast enhancement delle lesioni nelle diverse fasi evolutive . 
sono inoltre state raccolte informazioni sullet dei pazienti , sulla presentazione clinica e sulle possibili cause di infarto testicolare . in 14 of the 798 patients examined with cdus ( 1.75% of the total ) , the study found abnormalities suspicious for sti . 
clinical presentation in seven of these 14 patients was acute scrotum : six with testicular tenderness after a prior acute episode and one with testicular pain 25 days after varicocele embolisation . 
at presentation , all patients underwent cdus of the affected testis , which brought to light the following characteristics : the common feature among all 14 patients was single or multiple hypoechoic areas with no sign of microcalcifications , poor vascularity and no mass effect and / or signs of infiltration of vascular structures or scrotal tunics ; risultati in 14 dei 798 pazienti esaminati con ecd ( 1 , 75% del totale ) lindagine ha rilevato alterazioni sospette per ist . 
di questi 14 pazienti , 7 hanno esordito con un quadro di scroto acuto , 6 con dolenzia testicolare dopo pregresso episodio acuto ed infine 1 pazienti con algia testicolare insorta a 25 giorni da un intervento di scleroembolizzazione per varicocele . 
allesordio dei sintomi tutti i pazienti sono stati sottoposti ad esame ecd che , a livello del testicolo coinvolto , ha messo in luce i seguenti aspetti : la caratteristica che accomunava tutti i 14 pazienti stata il riscontro di singole o multiple aree ipoecogene , 1164 radiol med ( 2012 ) 117 : 11611175 fig . 
multiple aree con morfologia a cuneo , ipointense , con contrast enhancement periferico ad anello . docapsule and ill - defined margins ; these findings were defined as plurisegmental infarction , i.e. 
t1 - weighted sequences showed hyperintense lesions ( indicating haemorrhagic infarction ) in 6 dei 14 pazienti ( 43% del totale ) nel contesto del parenchima testicolare interessato si sono evidenziate multiple aree a distribuzione lobulare , ipoecogene , avascolari , prive di capsula o dotate di sottile pseudocapsula , a margini sfumati . 
in t2 - weighted sequences , lesions displayed varying signal intensity ( hyper - , isoand hypointensity ) , margins were well defined and they were often bounded by a low - signal rimorphology was oval , rounded or wedge shaped . 
these were most evident in lesions displaying hyperintense signal intensity in the t1 - weighted sequence and were most likely the result of extravasation of blood in the setting of the infarction . 
cdus follow - up showed progressive reduction in size of intratesticular lesions , which prevalently appeared inhomogeneously hypoechoic , as well as a higher definition of the lesions themselves with respect to the surrounding parenchyma . 
in 13 patients , lesions appeared isohyperintense , with a hypointense rim in the t1and t2 - weighted images , although they were better defined in the t2 - weighted sequences . 
after administration of contrast material , the lesions showed no intrinsic , but only peripheral , enhancement in 13 patients , whereas in one case , the multiple lesions showed partial contrast enhancement . 
following detailed evaluation of cdus and mri features at presentation and especially during follow - up , only one patient underwent orchiectomy , with a histologitutti i 14 pazienti , a distanza di 15 giorni dal primo riscontro allecd , sono stati esaminati con la rm . 
le sequenze pesate in t1 hanno evidenziato in 6 dei 14 pazienti ( 43% del totale ) lesioni iperintense ( espressione di infarto emorragico ) , mentre nei restanti 8 casi ( 57% del totale ) le lesioni si sono dimostrate isointense o debolmente ipointense rispetto al parenchima circostante . 
 nelle sequenze pesate in t2 le alterazioni si presentavano di intensit di segnale variabile ( iper - , iso - , ipointense ) , a contorni ben definiti , spesso delimitate da orletto di basso segnale , con morfologia ovalare , rotondeggiante o a cuneo . 
 con le sequenze ge stato possibile rilevare , nel contesto delle lesioni , segnale ipointenso riconducibile alla presenza di prodotti di degradazione dellemoglobina , maggiormente evidente nei pazienti ove le lesioni presentavano iperintensit del segnale nelle sequenze t1 pesate , espressione di possibile stravaso di sangue nel contesto dellinfarto . 
nei 6 pazienti che riferivano una dolenzia testicolare in pregresso episodio acuto stata documentata , nelle sequenze pesate in t1 , una stria di basso segnale circondata da una zona di contrast enhancement . 
in 13 dei 14 pazienti le lesioni apparivano iso - / iperintense , con cercine ipointenso nelle immagini sia t1 che t2 dipendenti , anche se certamente meglio definite nelle sequenze t2 . 
dopo somministrazione di mdc in 13 pazienti le lesioni non presentavano contrast enhancement intrinseco , ma solo un contrast enhancement periferico , mentre in 1 caso le alterazioni multiple assumevano in parte mdc . 
a 60200 giorni le lesioni note apparivano volumetricamente ridotte , prevalentemente ipo - / isointense in t1 e t2 ; in 7 casi era presente retrazione della tunica albuginea , peraltro ispessita , associata a distorsione ed ispessimento dei setti lobulari . 
4a - d multiple ischaemic lobules in the left testis examined 20 days after onset of acute left testicular paa cdus image , longitudinal view : hypoechoic avascular areas with reduction in size . 
in this case , cdus at presentation showed the coexistence of multiple hypoechoic oval - shaped lesions with no mass effect and mildly vascular appearance , which had been initially interpreted as sti . 
mri follow - up performed at 20 and 30 days proved crucial in confirming the presence of multiple areas characterised by hypointense signal with a peripheral hyperintense halo in t1 - weighted and hypointense signal in t2 - weighted sequences . 
in seguito alla dettagliata rivalutazione delle caratteristiche di ecd e di rm allesordio e soprattutto di quelle emerse nei successivi followup , solo 1 pazienti stato sottoposto ad orchiectomia , con diagnosi istologica di linfoma b cellulare . 
in questo caso lesame ecd ha documentato allesordio la coesistenza di lesioni multiple , ipoecogene , ovalari , prive di effetto massa , in parte lievemente vascolarizzate , inizialmente interpretate come ist . 
5a - e multiple ischaemic lobules in the left testis examined 100 days after onset of acute left testicular paa cdus image , longitudinal view : hypoechoic avascular areas with reduction in size . 
6a - d multiple ischaemic lobules in the left testis examined 200 days after onset of acute left testicular paa cdus image , longitudinal view : hypoechoic avascular areas with reduction in size . 
involvement of a single testicular segment ( sti ) is much more rare , with only 63 cases having been reported since the first case was described in 1909 [ 10 ]  . 
c sagittal t1 - weighted mri : low - signalintensity area with high - signal rid sagittal t2 - weighted mri : multiple inhomogeneous low - signal - intensity areas . 
contrast enhancement intrae perilesionale omogeneo . literature , most cases of sti are idiopathic , although the condition has been described in association with blood dyscrasias ( polycythaemia , sickle cell anaemia , protein s deficit ) , vasculitis ( hypersensitivity angiitis ) , fat embolism , acute epididymoorchitis , bell - clapper deformity ( the testicle is free to move and rotates in the tunica vaginalis , with a possible mechanism of torsion - detorsion , which leads to ischaemia ) , physical exertion and surgical lesions ( varicocele embolisation , surgical procedure to treat inguinal hernia ) della torsione intravaginale del funicolo spermatico [ 8 , 9 ]  . 
 il coinvolgimento di un solo segmento testicolare molto pi raro ed in letteratura , dal primo caso descritto nel 1909 ad oggi , sono stati riportati solo 63 casi [ 10 ]  . 
with regard to sti in children , the few cases described in the literature are idiopathic or related to urinary tract infections or post trauma [ 10 ]  . predisposing factors include various anomalies , which can favour sti onset , such as anomalies of the intratesticular centripetal arteries or bifurcation of the testicular artery or those linked to an inconstant anterior epididymal artery . 
in all these cases , the predisposition for an sti is particularly frequent in areas where collateral vessels are lacking , especially at the upper testicular pole where the vasculature is more precarious , as described in the literature [ 3 ]  . in two patients in our series , sti was associated with subacute epididymitis . 
although the pathogenesis of sti that follows epididymitis has not been well defined , two mechanisms have been proposed : arterial compression caused by hydrocele ; and venous obstruction due to thrombosis , most commonly at the level of the pampiniform plexus [ 19 ]  . 
in the other 11 cases , we hypothesised an idiopathic nature given that no patient had a history of aetiological and / or predisposing factors correlated with sti onset . sti symptoms are nonspecific and depend on the cause and time elapsed since the event . 
the differential diagnosis of acute scrotum requires ruling out the most common causes : torsion of the spermatic cord or testicular appendages , epididymoorchitis and , more rarely , sti [ 27 ]  . 
cdus findings of sti at onset generally include a hypoisoechoic area with no microcalcifications , little or no intralesional vasculature and no mass affect or signs of infiltration [ 4 ]  . 
some authors suggest that the predominant vascular insult in a rounded lesion could relate to venous drainage , and in such a case , the lesion may also present a mass effect linked to vascular congestion , whereas in a wedge - shaped lesion , it could be secondary to arterial compromise caused by thrombosis or microemboli [ 4 ]  . 
location in the middle to upper third of the testis and wedge - shaped morphology are typical and produced by anatomical characteristics of the testicular vasculature [ 3 ]  . 
per quanto riguarda gli infarti testicolari segmentali in et pediatrica , i pochi casi descritti in letteratura sono idiopatici o correlati a infezioni urinarie o post - traumatici [ 10 ]  . tra i fattori predisponenti sono state descritte diverse anomalie che in ambito testicolare possono favorire linstaurarsi di un ist , come anomalie delle arterie centripete intratesticolari o della biforcazione dellarteria testicolare o ancora legate ad unincostante arteria epididimale anteriore . 
in tutti questi casi la predisposizione ad un ist risulta pi frequente nelle zone dove i vasi collaterali sono deficitari , in particolare , al polo testicolare superiore , ove la vascolarizzazione pi precaria , come descritto in letteratura [ 3 ]  . nella nostra casistica in 2 pazienti list era associato a epididimite subacuta . 
sono per stati proposti due meccanismi : la compressione arteriosa da parte di un idrocele teso e lostruzione venosa da trombosi , pi spesso a livello del plesso pampiniforme [ 19 ]  . 
in tutti gli altri 11 casi abbiamo ipotizzato la natura idiopatica visto che nessun pazienti riportava in anamnesi fattori eziologici e / o predisponenti correlati allinsorgenza dellist stessa . i sintomi dellist sono aspecifici e dipendenti dalla causa e dal tempo intercorso dallesordio . 
la diagnosi differenziale in un paziente con scroto acuto impone di escludere le cause pi comuni : la torsione del funicolo spermatico o delle appendici testicolari , lorchi - epididimite e pi raramente list [ 27 ]  . 
allesordio list si presenta allecd generalmente come unarea ipo - isoecogena priva di microcalcificazioni , con ridotta o assente vascolarizzazione intralesionale , che non provoca effetto massa n segni di infiltrazione [ 4 ]  . 
secondo alcuni autori linsulto vascolare predominante in una lesione rotondeggiante potrebbe riguardare il drenaggio venoso e in questo caso la lesione pu presentare anche un effetto massa legato alla congestione vascolare , mentre in una lesione a cuneo potrebbe essere secondario a compromissione arteriosa da fenomeni trombotici o microembolia [ 4 ]  . 
la sede nel radiol med ( 2012 ) 117 : 11611175 1173 and better defined with respect to the surrounding parenchyma [ 28 ]  . in our experience , and once again in line with the data in the literature , mri proved to be highly useful in confirming the diagnosis of sti when us findings were atypical and / or suggestive of a solid lesion , and thus enabled conservative treatment [ 7 , 29 , 30 ]  . 
in addition , in some cases t2 - weighted sequences make it possible to identify the typical wedge - shaped morphology of sti , which may be difficult to visualise at cdus [ 3 ]  . 
in the sequences obtained after administration of contrast material , one of the most relevant findings in sti reported in the literature and confirmed in our series is rim enhancement in the absence of intralesional uptake of contrast material [ 5 , 6 ]  . 
in our series , rim enhancement was identified at mri examination performed 130 days after onset , whereas at the following examination performed at 80200 days , this finding was no longer significantly appreciable . 
in some cases , retraction of the tunica albuginea can be appreciated , with distortion and thickening of the lobular septa , because hyalinisation and fibrosis resulting from the ischaemic insult lead to a loss of testicular substance [ 28 ]  . 
the follow - up performed with mri enabled us to justify the persistence of testicular tenderness related to the outcome of sti in the six patients who reported a prior episode of acute scrotu indeed , in these patients , a hypointense streak with peripheral contrast enhancement was seen in t1weighted images . 
therefore follow - up with cdus and mri made it possible to document sti evolution , thus confirming the diagnostic hypothesis put forward at onset and justifying the subacute or chronic clinical presentations in our patient series . we feel that the , albeit limited , use of ceus in our study proved useful for evaluating sti and in the followup , where it may prove to be a valid alternative to mri . 
al follow - up ecografico , nella nostra casistica , cos come in letteratura , list si presenta come lesione disomogeneamente ipoecogena , ridotta di dimensioni rispetto allesordio e meglio definita rispetto al parenchima circostante [ 28 ]  . dalla nostra esperienza , concorde con i dati della letteratura , emerso che la rm appare molto utile nel confermare la diagnosi di ist quando i reperti ecografici sono atipici e / o suggestivi di una lesione solida , consentendo cos un trattamento conservativo [ 7 , 29 , 30 ]  . 
nelle sequenze ottenute dopo somministrazione di mdc uno dei reperti pi rilevanti nellist , gi segnalato in letteratura e confermato dalla nostra casistica , il contrast enhancement periferico ad anello in assenza di impregnazione intralesionale [ 5 , 6 ]  . 
nella nostra casistica il contrast enhancement periferico ad anello stato documentato nelle indagini rm eseguite a distanza di 130 giorni dallesordio , mentre nelle indagini successive a 80200 giorni il reperto non era pi significativamente apprezzabile . 
 [ 31 ] che ha valutato una serie di pazienti con ist mediante ceus ed ha ricondotto il contrast enhacement periferico ad anello alla possibile comparsa di tessuto di granulazione in risposta al fenomeno ischemico . 
in alcuni casi possibile documentare la retrazione cicatriziale della tunica albuginea con distorsione ed ispessimento dei setti lobulari , poich la ialinizzazione e la fibrosi conseguenti allinsulto ischemico portano ad una perdita di sostanza testicolare [ 28 ]  . 
il follow - up eseguito con rm ci ha permesso di giustificare , nei 6 pazienti che riferivano pregresso episodio di scroto acuto , la persistenza di dolenzia testicolare correlata agli esiti di ist . 
in questi pazienti infatti stato possibile documentare nelle sequenze pesate in t1 una stria ipointensa con contrast enhancement periferico : tale reperto stato da noi interpretato come esito cicatriziale in pregressa lesione ischemica , con presenza di circoli collaterali di compenso periferici [ 3 ]  . 
pertanto il follow - up mediante monitoraggio ecd e rm ha permesso di documentare levoluzione dellist confermando lipotesi diagnostica prospettata allesordio e permettendo di giustificare quadri clinici subacuti o cronici giunti alla nostra osservazione . a nostro parere la ceus , nella nostra limitata esperien1174 radiol med ( 2012 ) 117 : 11611175 particular , as several authors note [ 31 ] , reduction in lesion size and revascularisation of the ischaemic area seen during follow - up proved to be valuable diagnostic criteria in sti . 
this is confirmed in the subsequent follow - up examinations , which demonstrate the natural evolution of the ischaemic process . za , si rilevata utile nella valutazione dellist e valida nel follow - up ove pu risultare valida alternativa alla rm . 
in particolare , come segnalato da altri autori [ 31 ] , la riduzione volumetrica e la rivascolarizzazione dellarea ischemica nel follow - up si sono dimostrati validi criteri diagnostici nellist . 
la rm fornisce importanti elementi spesso dirimenti per la diagnosi , che viene confermata nei successivi controlli di follow - up che documentano la naturale evoluzione del processo ischemico . conclusions conclusioni our study reconfirms the indispensable role of imaging ( cdus , mri , ceus ) in characterising parenchymal abnormalities that are doubtful or suspicious for sti , thus allowing conservative treatment . 
the nature of the lesions can also be confirmed and monitored during follow - up , and ceus may be considered a valid supplement to cdus and mri in this context . la nostra esperienza riconferma il ruolo indispensabile delle metodiche di imaging ( ecd , rm , ceus ) nel caratterizzare alterazioni parenchimali dubbie o sospette per ist permettendo un approccio terapeutico conservativo . 
ventisette pazienti con il sospetto di patologia uroteliale maligna , sono stati sottoposti a biopsia per via retrograda , utilizzando il biotomo da 7 f ( cordis , miami , fl , usa )  . 
lalta accuratezza diagnostica era dovuta alla corrispondenza positiva tra esame isto - patologico eseguito sul prelievo bioptico ed i reperti patologici chirurgici o la stazionariet / riduzione dimensionale della alterazione durante il periodo di follow - up . 
considerando la sede dei prelievi , la performance della procedura risultata pi bassa per le lesioni localizzate nei calici che non per quelle localizzate in altre sedi dellapparato urinario superiore ( aus ) , con un successo tecnico , pari al 71 , 43% . 
 several studies in the literature compare the accuracy of radiographic studies , ureteroscopy , biopsy and cytology in predicting the histopathology of upper - urinary - tract transitional cell carcinoma ( tcc ) [ 2 , 3 ]  . 
however , ureteroscopic biopsy can be associated with some complications , such as perforation , spillage of tumour cells and ureteral strictures [ 5 , 6 ]  . forceps biopsy was originally designed for endomyocardial biopsies [ 7 ]  . 
the pathological grade obtained from biopsy was compared to that of the surgically resected specimens , and all patients undergoing conservative treatment were closely monitored . the aim of the study was to evaluate the feasibility , sensitivity , specificity , diagnostic accuracy and safety of urological biopsy performed using a flexible alligator forceps . nella popolazione generale , lincidenza dei tumori uroteliali dellapparato urinario superiore ( aus ) , bassa ( uno o due casi per 100000 persone allanno ) ; essa maggiore nei soggetti con precedenti tumori del tratto urinario basso , con una incidenza del 3 , 9%4 , 8% [ 1 ]  . 
in letteratura , sono presenti alcuni lavori che paragonano laccuratezza di indagini radiologiche , dellureteroscopia , della biopsia e della citologia urinaria nel predire listopatologia del carcinoma a cellule transizionali ( tcc ) dellaus [ 2 , 3 ]  . 
inoltre , il biotomo stato utilizzato per le biopsie biliari percutanee transluminali ( previo posizionamento di drenaggio biliare ) ; ed in questultimo caso risultata essere una tecnica sicura e facile da eseguire [ 8 ]  . 
inoltre , i pazienti trattati in maniera conservativa , sono stati tenuti sotto stretto follow - up . lo scopo del nostro studio quello di valutare la fattibilit , la sensibilit , la specificit , laccuratezza diagnostica e la sicurezza delle biopsie uroteliali condotte con il biotomo flessibile alligator type . 
 materials and methods patients materiali e metodi pazienti from february 2007 to september 2010 , 27 patients ( 15 men and 12 women ; mean age 71.15 years ; range 43 - 89 ) with suspected calyceal ( n = 7 ) , pelvis ( n = 5 ) , pelvic - ureteral junction ( n = 4 ) or ureteral ( n = 11 ) lesions ( four thickenings and 23 filling defects ) underwent transureteral biopsy using the 50 - cm , 7 - f flexible biopsy forceps ( cordis , miami , fl , usa ) ( table 1 )  . 
 urine cytology was obtained at least once prior to the urothelial biopsy in all patients ; in particular , in seven patients , urinary cytology identified the presence of atypical cells . 
all cases were discussed during a multidisciplinary meeting involving an interventional radiologist , a urologist , an oncologist and a pathologist , da febbraio 2007 a settembre 2010 , 27 pazienti ( 15 maschi e 12 femmine ; et media 71 , 15 anni , range 4389 ) con sospette lesioni caliceali ( n = 7 ) , pelviche ( n = 5 ) , della giunzione pelvi - ureterale ( n = 4 ) o ureterali ( n = 11 ) [ 4 ispessimenti parietali focali e 23 difetti di riempimento allesame uro - tomografia computerizzata ( tc ) ] sono stati sottoposti a biopsia trans - ureterale con biotomo flessibile , 7 f , lungo 50 cm , ( cordis , miami , florida , usa ) ( tabella 1 )  . 
tutti i pazienti hanno eseguito lesame citologico delle urine almeno una volta prima della biopsia uroteliale ; in particolare in 7 pazienti sono state identificate la presenza di cellule atipiche . 
tutti i casi sono stati discussi durante un meeting multidisciplinare tra radiologo interventista , urologo , oncologo ed anatomo - patologo che hanno concordato per 1154 radiol med ( 2012 ) 117 : 11521160 all of whom agreed to obtain a biopsy using a flexible biopsy forceps under fluoroscopic guidance . 
written informed consent was obtained from all patients . baseline imaging pretreatment imaging consisted of a urological multidetector computed tomography ( mdct ) scan ( aquilion 64 , toshiba , tokyo , japan ) without and after contrast medium administration i.v.. 
the contrast - enhanced scans were acquired after injection of 100 ml of iodinated contrast agent ( visipaque 320 , ge healthcare , princeton , nj , usa ) at an injection rate of 3 ml / s , followed by injection of 40 ml saline at a rate of 2 ml / s . 
after baseline acquisition , the contrast medium was administered and a venous ( 60 s ) and a late ( excretory phase , after 1020 m ) scan were obtained . 
ct findings were classified as thickness and filling defects on the basis of longitudinal and transverse diameters . pretreatment procedure all patients arrived in the angiography suite with a ureteral catheter previously placed by the urologist during ureteroscopy . 
administration of a combination of midazolam ( ipnovel 15 , roche , milan , italy ) ( 0.070.08 mg / kg ) , propofol ( diprivan , astrazeneca s.p.a. , caponago , italy ) ( 0.52.0 mg / kg / h ) and fentanyl ( fentanest ; pharmacia & upjohn , milan , italy ) ( 12 g / kg )  . 
 imaging pre - trattamento limaging pre - trattamento stato ottenuto mediante indagine con tc multistrato addominale ( aquilion 64 , toshiba , tokio , giappone ) , con e senza iniezione di mezzo di contrasto ( mdc )  . 
le scansioni con mdc sono state eseguite iniettando 100 ml di contrasto iodato ( visipaque 320 , ge healthcare , princeton , nj , usa ) ad una velocit di 3 ml / s seguito dalliniezione di 40 ml di soluzione salina ad una velocit di 2 ml / s . 
stata eseguita unacquisizione basale e , dopo la somministrazione intravenosa di mdc , stata ottenuta unacquisizione venosa ( 60 secondi ) e una tardiva ( fase escretoria dopo 1020 minuti )  . 
i reperti tc sono stati classificati come ispessimenti parietali focali e difetti di riempimento sulla base dei diametri longitudinale e trasverso . procedure pre - trattamento tutti i soggetti sono giunti in sala angiografia con un catetere ureterale , precedentemente posizionato dagli urologi durante lesame ureteroscopico . 
ciascun paziente stato mantenuto in regime di sedazione moderata , ottenuta mediante la somministrazione per via endovenosa di una combinazione di midazolam ( ipnovel 15 , roche , milano , italia ; 0 , 070 , 08 mg / kg ) , propofol ( diprivan , astrazeneca s.p.a. , caponago , italia ; 0 , 52 mg / kg / h ) e fentanil ( fentanest , pharmacia & upjohn , milano , italia ; 12 g / kg )  . 
the detector has a field of view of 3830 cm and an array of 2 , 4801920 tutte le procedure sono state eseguite con guida fluoroscopica ( philips allura xper fd20 , philips medical system , best , paesi bassi )  . 
through the ureteral catheter , a 0.035j - tip hydrophilic guidewire ( glidewire , terumo medical corporation , somerset , nj , usa ) was introduced in the ureteral lumen . 
the catheter was then replaced first by a 4or 5 - f vascular catheter ( cordis europe , n.v. , lj roden , the netherlands ) to perform ascending pyelography using radiopaque contrast medium ( visipaque 320 , ge healthcare ) and subsequently by a 7 - f vascular introducer ( cordis europe ) , with an appropriate length to reach the site of the biopsy , shown as a filling defect during pyelography . 
because of its flexibility and adjustability , it allowed for several histological samples to be obtained ( typically three to five passes ) , depending on the subjective quality of the material obtained as assessed by visual inspection . outcomes technical success was defined as correct positioning of the biopsy device within the lesion . 
lesions were classified on the basis of histopathological reports : group 1 , indicating an adequate sample for histopathological analysis to yield a definitive diagnosis of a benign or malignant lesion ( e.g. , tcc , normal ureteral tissue , etc ) ; group 2 , indicating that the sample was insufficient to yield a definitive diagnosis . 
biopsy results from group 1 were compared with the pathological diagnosis on the surgical specimens or with biotomo flessibile , 7 f , lungo 50 cm ( cordis , miami , florida , usa )  . 
mediante il catetere ureterale , stata introdotta nel lume ureterale una guida idrofilica , 0 , 035 inch , ( terumo medical corporation , somerset , nj , usa ) con punta a j . 
 successivamente il catetere stato sostituito con un catetere vascolare 4 o 5 f ( cordis europe , n.v. , lj roden , paesi bassi ) al fine di eseguire una pielografia utilizzando mdc radiopaco ( visipaque 320 , ge healthcare , princeton , nj , usa ) e successivamente da un introduttore vascolare da 7 f ( cordis europe , n.v. , lj roden , paesi bassi ) , della lunghezza adeguata per raggiungere il sito della biopsia , documentata come un difetto di riempimento durante la pielografia . 
 le lesioni sono state classificate sulla base dei reperti istopatologici in due gruppi : gruppo 1 , costituito dalle lesioni in cui il materiale bioptico risultato sufficiente per esami istopatologici e quindi per giungere ad una diagnosi definitiva di lesione benigna o maligna ( per esempio tcc , tessuto normale uroteliale , etc . ) ; gruppo 2 , costituito dalle lesioni in cui il materiale prelevato non stato sufficiente per giungere ad una diagnosi definitiva . 
i risultati delle biopsie del gruppo 1 sono stati confrontati con quelli ottenuti dallesame 1156 radiol med ( 2012 ) 117 : 11521160 the imaging findings during close follow - up ( of at least 12 months )  . 
lesions were defined as benign when the histological report showed a definitive diagnosis of benignity or when the lesion exhibited a decrease in size or no morphological change during imaging follow - up . 
filling defects unreachable by forceps were considered as possible malignancies and were consequently subjected to a close followup ( of at least 12 months ) , but they were not considered for our analysis . 
complications were classified as major or minor in accordance with the classification system of the society of interventional radiology [ 9 ]  . results technical success was obtained in 92.6% ( 25 / 27 ) of patients . 
all lesions sampled ( 25 / 27 , 92.6% ) had either a surgical histological correspondence ( n = 21 ) , or the close follow - up demonstrated stability or reduction in size ( n = 4 )  . 
with regard to biopsy site , the procedure proved to be less precise in the calyceal lesions than in the remaining sites , with a value of technical success of 71.43%. 
in all cases in which the biopsy was performed , the tissue sampled was sufficient for histological examination . there were no major complications related to the biopsy procedures ; some patients ( n = 20 ) had asymptomatic haematuria in the early hours ( up to 24 h ) after the procedure , and others ( n = 10 ) had mild dysuria . 
una lesione stata definita come benigna quando lesame istologico ha riportato una diagnosi definitiva di benignit o quando , nel corso del follow - up , risultata dimensionalmente ridotta o invariata . 
i difetti di riempimento non raggiungibili dal biotomo sono stati considerati come possibili maligni e di conseguenza sottoposti ad un periodo di stretto follow - up ( almeno 12 mesi ) , ma non sono stati considerati per la nostra analisi . 
le complicanze sono state classificate in maggiori e minori , in accordo con il sistema di classificazione della societ internazionale di radiologia interventistica [ 9 ]  . risultati il successo tecnico stato ottenuto nel 92 , 6% dei pazienti ( 25 dei 27 pazienti )  . 
in 2 pazienti ( 7 , 4% ) non stato possibile eseguire la biopsia perch la pielografia non ha consentito di identificare la precisa sede del difetto di riempimento documentato allesame uro - tc ; in entrambi i pazienti i difetti di riempimento avevano un diametro trasverso inferiore ad 1 cm e sono stati considerati come possibili lesioni maligne e pertanto sottoposti a stretto follow - up . 
tutte le lesioni sottoposte a biopsia ( 25 / 27 , 92 , 6% ) hanno avuto una corrispondenza istologica chirurgica ( n = 21 ) oppure il follow - up ha mostrato stabilit o riduzione delle dimensioni dellalterazione ( n = 4 )  . 
alcuni pazienti ( n = 20 ) hanno presentato ematuria asintomatica nelle prime ore successive alla procedura ( entro 24 ore ) e lieve disuria ( n = 10 ) ; nessun paziente ha necessitato di terapie specifiche . 
therefore , histological confirmation is often required for correct diagnosis , discussione luro - tc risulta essere efficace nellindividuare i tumori dellaus in pazienti con anamnesi positiva per tumori uroteliali . 
exfoliated cell cytology in combination with biopsy grade is recommended as part of the evaluation of upper urinary tract tcc selected for endoscopic management [ 12 ]  . endoscopic brush cytology is a specific method for detecting tcc of the upper urinary tract but does not appear to be successful in diagnosing dysplasia or in carcinoma in situ ( cis )  . 
 nei pazienti a basso rischio con ematuria microscopica asintomatica , la citologia urinaria rappresenta un costo aggiuntivo , senza aggiungere alcun beneficio diagnostico [ 11 ] ; oggi usata solo come fattore predittivo , in associazione con i rilievi dellimaging [ 4 ]  . 
la citologia urinaria in associazione con il grading istopatologico , raccomandata nella valutazione del carcinoma a cellule transizionali dellaus in pazienti selezionati per la procedura endoscopica [ 12 ]  . 
 this biopsy forceps was originally designed for endomyocardial biopsies [ 7 , 16 , 17 ] and consists of three parts : a three - pull ring handle , cutting jaws and a coiled sha the literature contains several reports on the use of the biopsy forceps for histological sampling of the biliary tree [ 18 ] , and jung et al . 
 [ 8 ] considered percutaneous transluminal forceps biopsy through a transhepatic biliary drainage tract safe and easy to perforadditionally , the procedure provides relatively high accuracy in the diagnosis of malignant biliary obstructions . 
 il biotomo stato originariamente progettato per le biopsie endomiocardiche [ 7 , 16 , 17 ] ed costituito da tre parti : una impugnatura a triplo anello , un sistema tagliente ed uno shaft a spirale . 
al meglio delle nostre conoscenze , radiol med ( 2012 ) 117 : 11521160 1159 ours is the first series in which the forceps biopsy device has been used in the upper urinary tract . 
the procedure can be considered safe and easy to perform . the biopsy method proposed offers two indisputable advantages : the possibility of obtaining histological samples while visualising the precise site of the lesion , and the opportunity to obtain tissue cores and consequently a histopathological grading . 
correct and diagnostic samples were obtained from the filling defects and urothelial thickenings documented on ct urography , especially if they were located in the renal pelvis , pelvic - ureteral junction and along the ureter . 
 the main limitation of our study is the small number of patients ; further research with a large patient population and longer follow - up periods will be needed to precisely evaluate diagnostic accuracy and establish a possible correlation between accuracy and lesion location . 
further comparative studies with a prospective randomised design might establish the best biopsy system for urothelial biopsies . in conclusion , our preliminary results are encouraging , and the forceps device can be proposed as an innovative approach for urothelial biopsy . la serie di pazienti da noi presentata la prima in cui il biotomo utilizzato per prelievi bioptici uroteliali dellaus . 
la procedura pu essere considerata sicura e facile da eseguire . il metodo bioptico presentato presenta due indiscutibili vantaggi : la possibilit di eseguire prelievi istologici vedendo lesatta sede della alterazione e lopportunit di ottenere frustoli di tessuto e di conseguenza un grading istopatologico . 
un campionamento bioptico corretto e diagnostico stato eseguito nei difetti di riempimento e negli ispessimenti uroteliali focali documentati allesame uro - tc , soprattutto se questi erano localizzati nella pelvi renale , a livello della giunzione pelvi - ureterale e lungo luretere . 
prendendo in considerazione la sede del prelievo , la procedura risultata essere meno precisa nelle lesioni dei calici renali rispetto a quelle delle altre sedi , con un successo tecnico del 71 , 43% . 
 il principale limite dello studio presentato il basso numero dei pazienti ; pertanto , ulteriori studi con un maggior numero di pazienti e periodi di follow up pi lunghi saranno necessari per una esatta valutazione dellaccuratezza diagnostica e per stabilire una correlazione tra questa e la localizzazione della lesione . 
following neoadjuvant chemoradiation therapy , the analysis of mr images showed 23 ( 59% ) patients with a rectal disease staged t2 and 16 ( 41% ) with a disease staged > t2 . 
cohens kappa to measure concordance between post - chemoradiation mr staging and histological response showed 83.6% concordance for disease confined to the serosa ( t3 ) : concordance was 97.22% for disease n1 and 33.33% for disease > n1 . 
mr imaging is critical for discovering t3 disease ; moreover , morphological mr imaging does not always provide the opportunity to discern small residual cancer cells hidden in fibrotic tissue that could cause involvement of circumferential resection margin ( crm ) on histology . keywords mri rectal cancer chemoradiation therapy staging of rectal cancer mri and circumferential resection margins riassunto obiettivo . 
dopo il trattamento chemio - radioterapico neoadiuvante , abbiamo osservato , dopo lanalisi delle immagini rm , 23 ( 59% ) pazienti con una neoplasia del retto con staging t2 e 16 ( 41% ) pazienti con una neoplasia del retto con staging > t2 . 
lanalisi istopatologica dello staging effettuata dopo trattamento , ha mostrato 13 pazienti con una neoplasia del retto con staging > t2 e 26 pazienti con una neoplasia del retto con staging t2 . 
il valore di concordanza tra la stadiazione rm dopo chemio - radioterapia ed il responso istologico , con una malattia confinata alla sierosa ( t3 ) era dell83 , 6% ( test della k cohen )  . 
le immagini di rm sono cruciali nellindividuazione di una malattia di grado t3 ; inoltre , con limaging morfologico di rm non abbiamo sempre la possibilit di mettere in evidenza piccole cellule 1126 radiol med ( 2012 ) 117 : 11251138 tumorali residue nascoste nel tessuto fibrotico che possono causare un coinvolgimento del margine di resezione circonferenziale ( crm ) allistologia . parole chiave rm cancro del retto trattamento chemio - radioterapico staging del cancro del retto rm e margini di resezione circonferenziali introduction introduzione colorectal carcinoma is the third most common cancer worldwide , with more than one million new cases every year [ 1 ]  . 
stage t3 tumours carry a greater risk of local recurrence , and the current t staging system does not discriminate between tumours with a wide circumferential resection margin ( crm ) and those with a close or involved crm . 
it has been repeatedly shown that the distance from the tumour to the circumferential mesorectal resection plane is a more powerful predictor of local recurrence than is the t stage [ 2 ]  . 
stage t4 tumours are defined as neoplasms extending beyond the rectal wall , with infiltration of surrounding organs or structures or perforation of the visceral peritoneualthough en bloc resection of the neoplasm and adjacent organs is performed in these patients , the local recurrence rate remains high . 
with the worldwide adoption of preoperative radiation therapy , preoperative staging is important for distinguishing between patients who need only surgery and those who will be at high risk of local disease recurrence without preoperative therapy [ 5 , 6 ]  . total mesorectal excision ( tme ) is the surgical treatment of choice ; en bloc removal of both the tumour and the mesorectal fascia gives a 10% rate of recurrence when used as a single therapeutic modality . 
the swedish rectal cancer trial [ 4 ] demonstrated a 58% reduction in local recurrence rates by applying short - course radiotherapy ( 25 gy in five fractions over 5 days ) before surgery . 
by contrast , in patients with locally advanced rectal carcinoma , it is widely recogil carcinoma del retto il terzo tumore pi comune al mondo , con pi di un milione di nuovi casi ogni anno [ 1 ]  . 
questo tipo di tumore poco comune nella popolazione al di sotto dei 40 anni di et e la sua prevalenza aumenta costantemente dopo i 50 anni di et , specialmente nei maschi . 
vi sono due fattori predittivi indipendenti : lo stadio locale del tumore ( stadio di t ) e la presenza o assenza di linfonodi metastatici ( stadio delln )  . 
i tumori con stadio t3 presentano un rischio pi alto di recidiva locale , e la presenza di un sistema di stadiazione t non permette di differenziare tra tumori con un ampio margine di resezione circonferenziale ( crm ) e quelli con un coinvolgimento pi o meno grande del crm . 
stato ripetutamente dimostrato che la distanza del tumore dal piano di resezione circonferenziale del meso - retto un fattore predittivo della possibilit di recidiva locale pi efficace rispetto al solo stadio t [ 2 ]  . 
i tumori di stadio t4 sono definiti come neoplasie che si estendono aldil della parete del retto , con infiltrazione degli organi o delle strutture circostanti o con perforazione del peritoneo viscerale . 
con ladozione a livello mondiale della terapia radiante pre - operatoria , la stadiazione pre - operatoria importante per differenziare i pazienti che necessitano soltanto del trattamento chirurgico , da quelli che sarebbero ad alto rischio per recidiva locale di malattia senza terapia pre - operatoria [ 5 , 6 ]  . 
 lescissione totale del meso - retto ( etm ) il trattamento chirurgico di scelta ; la rimozione in blocco sia del tumore che della fascia meso - rettale d un tasso di recidiva pari al 10% quando usata come singola modalit terapeutica . 
le nuove strategie sono tali che il coinvolgimento del mesoradiol med ( 2012 ) 117 : 11251138 1127 nised that preoperative long - course radiotherapy ( 4554 gy in 2530 fractions over 56 weeks ) with concomitant chemotherapy reduces tumour size resulting in downstaging [ 7 ]  . the role of imaging modalities is progressively increasing , with physicians making use of computed tomography ( ct ) , magnetic resonance ( mr ) imaging , endorectal ultrasound ( us ) and positron emission tomography ( pet ) [ 8 ]  . 
 subsequently , the introduction of endorectal coils overcame this problehowever , high costs and the inability to completely evaluate the mesorectal fascia and the surrounding tissues , together with the difficulty in positioning the coil in patients with proximal or nearly obstructing tumours , made it clear that the endorectal coil had many drawbacks . 
at the same time , the n staging obtained with mr imaging did not seem to be as precise as t staging , with an accuracy of 3995% [ 11 ]  . 
 diagnosis , staging and treatment planning are based on a multidisciplinary approach , where radiotherapy , chemotherapy , pathology and surgery are combined in order to reduce disease recurrence and improve anal sphincter - saving surgery . 
with this multimodal approach in mind , the aim of our study was to determine , by a retrospective analysis , the diagnostic accuracy of mr imaging in patients with rectal carcinoma by comparing post - chemoradiation mr findings with the pathological specimens obtained after surgery . materials and methods from january 2007 to january 2010 , we enrolled 39 patients ( 17 women ; 22 men ) aged between 41 years and 81 ( mean age 64 ) years with a proven diagnosis of locally advanced rectal cancer . 
patients were excluded from the study if the tumour was stage t4 , if they had distant metastasis or if mr imaging had been performed without contrast - enhanced sequences due to renal disease that precluded contrast - material administration i.v. 
all patients received chemoradiation therapy before surgery and underwent clinical assessment ( digital rectal exploration ) , colonoscopy , computed tomography ( ct ) and pelvic mr imaging : colonoscopy was performed to obtain histological specimens , ct for systemic staging of the disease ( n and m ) and mr imaging for accurate local disease staging ( t and n )  . 
il swedish rectal cancer trial [ 4 ] ha dimostrato un 58% di riduzione del tasso di recidiva locale tramite luso di un breve ciclo di radioterapia ( 25 gray in 5 frazionamenti per 5 giorni ) prima del trattamento chirurgico . 
 invece , nei pazienti con un carcinoma del retto con stadio avanzato , ampiamente riconosciuto che un lungo ciclo di radioterapia ( 4554 gray in 2530 frazionamenti per 56 settimane ) preoperatorio con trattamento chemioterapico concomitante , comporti la riduzione delle dimensioni del tumore ottenendo un downstaging [ 7 ]  . il ruolo delle modalit di imaging progressivamente in aumento e fra queste i medici fanno uso della tomografia computerizzata ( tc ) , della risonanza magnetica ( rm ) , della ecografia endo - rettale ( us ) e della tomografia ad emissione di positroni ( pet ) [ 8 ]  . 
tuttavia , gli alti costi e lincapacit di una completa valutazione della fascia meso - rettale e dei tessuti circostanti , insieme alla difficolt nel posizionamento della bobina nei pazienti con una ostruzione pi o meno prossimale del retto rende chiaro che la bobina endo - rettale risulta avere non pochi inconvenienti . 
allo stesso tempo , la stadiazione linfonodale ottenuta tramite limaging di rm non sembra essere cos precisa come quella del t , con un range che va dal 39% al 95% [ 11 ]  . 
 i passaggi seguenti di diagnosi e di stadiazione , la pianificazione della strategia di trattamento sono basate su un approccio multidisciplinare , dove la radioterapia , la chemioterapia , lanatomia patologica e la chirurgia sono combinate nellintento di ridurre la recidiva di malattia e migliorare la chirurgia di salvataggio dello sfintere anale . 
 con questo approccio multimodale in mente , lo scopo del nostro studio era di determinare , tramite unanalisi retrospettiva , laccuratezza diagnostica dellimaging di rm nei pazienti con carcinoma del retto mettendo a confronto limaging di rm post trattamento chemio - radioterapico con i campioni patologici ottenuti dopo chirurgia . materiali e metodi nel nostro istituto , da gennaio 2007 a gennaio 2010 , abbiamo arruolato 39 pazienti ( 17 donne ; 22 uomini ) con et compresa tra 41 e 81 anni ( let media era di 64 anni ) con una diagnosi comprovata di cancro del retto localmente avanzato . 
i pazienti venivano esclusi dallo studio se il tumore era di stadio t4 , se avevano metastasi a distanza o 1128 radiol med ( 2012 ) 117 : 11251138 a phased - array coil . 
 all patients underwent the same imaging protocol , which comprised t1and t2 - weighted spin - echo sequences in multiple planes to obtain a complete , preliminary view of the pelvic region . 
t1 - weighted spin - echo sequences were performed with the following imaging parameters : time to repetition ( tr ) / time to echo ( te ) 500 / 20 ; flip angle 90 ; echo train length 1 . 
t2 - weighted turbo spin - echo sequences were acquired according to the following protocol : tr / te 6 , 0006 , 500 / 130 ; flip angle 175 ; echo - train length 23 . 
 coronal sequences were acquired with the following imaging parameters : tr / te 4 , 5005 , 000 / 135 ; flip angle 180 ; echo - train length 23 . 
transverse t2 - weighted sequences were oriented perpendicularly to the long axis of the rectum and were acquired with the following imaging parameters : tr / te 7 , 0007 , 500 / 130 ; flip angle 180 ; echotrain length 23 ; slice thickness 3 mm ; field of view 20 cm ; matrix 318512 . mr images were analysed by a team of two expert radiologists who were unaware of the clinical and histopathological findings . 
a tumour was defined as stage t3 if it showed a broad base or nodular configuration of the lateral tumour margin , with signal intensity greater than that of muscle extending into perirectal fat . 
fibrosis has a lower signal intensity and is spiculated ; on the other hand , active tumour was predicted if there was a broad base or nodular configuration of the lateral tumour marg the number and features of pelvic lymph nodes were reviewed . 
 a node was considered enlarged if the length was > 5 mm ( mesorectal ) , 7 mm ( internal iliac ) , 10 mm ( external iliac ) or 9 mm ( common iliac )  . 
locoregional nodal involvement se lesame era stato effettuato senza lutilizzo di sequenze post - contrastografiche per via di problemi renali che precludessero la somministrazione endovenosa di mezzo di contrasto ( livello di creatinina sierica > 1 , 9 mg / dl )  . 
tutti i pazienti sono stati esaminati clinicamente ( esplorazione digito ano - rettale ) e poi tramite colonscopia , tomografia computerizzata ( tc ) e risonanza magnetica ( rm ) della pelvi ; la colonscopia stata effettuata per ottenere campioni istologici , la tc per una stadiazione sistemica della malattia ( n ed m ) , la rm per ottenere unaccurata stadiazione locale della malattia ( t ed n )  . 
successivamente , abbiamo comparato le immagini di rm dopo trattamento chemio - radioterapico con i campioni patologici . le immagini di rm sono state ottenute con un magnete di 1 , 5 t ( magnetom simphony , siemens , erlangen , germania ) e bobina phased - array . 
successivamente alla somministrazione endorettale di circa 240 ml di acqua , un farmaco antispasmodico ( iniezione intravenosa di hyoscine - n - butyl bromide 20 mg ) stato somministrato preventivamente allesame per ridurre la peristalsi intestinale ; il farmaco mio - rilassante non stato utilizzato in quei pazienti che soffrivano di glaucoma , di ipertrofia prostatica benigna e di patologie cardiache . tutti i pazienti sono stati sottoposti allo stesso protocollo di imaging , che includeva sequenze spin - echo t1 e t2 pesate su multipli piani di scansione per ottenere una visione completa , preliminare della regione pelvica . 
le sequenze spin - echo t1 pesate venivano ottenute con i seguenti parametri di imaging : tempo di ripetizione ( tr ) / tempo di eco ( te ) , 500 / 20 ; flip angle , 90 ; echo train length , 1 . 
 le sequenze turbo spin - echo t2 pesate venivano ottenute con questo protocollo : tr / te 6 , 0006 , 500 / 130 ; flip angle , 175 ; echo - train length , 23 . 
le sequenze coronali sono state ottenute con i seguenti parametri di imaging : tr / te 4 , 5005 , 000 / 135 ; flip angle , 180 ; echotrain length , 23 . 
le sequenze t2 pesate trasversali erano orientate perpendicolarmente al retto lungo lasse maggiore e sono state realizzate con i seguenti parametri di imaging : tr / te 7 , 0007 , 500 / 130 ; flip angle , 180 ; echo train length , 23 ; spessore di sezione , 3 mm ; fov , 20 cm ; matrice , 318512 . le immagini rm sono state analizzate da una quipe di 2 radiologi esperti ai quali i risultati clinici e isto - patoloradiol med ( 2012 ) 117 : 11251138 1129 fig . 
at 2 cm above the anal verge , there is hemicircumferential parietal thickening of the rectum , with anterior extension into the mesorectal fat before chemoradiation therapy ( red circle )  . 
at 10 cm above the anal verge , there is a circumferential parietal thickening of the rectum with partial retraction of the mesorectal fat before chemoradiation therapy ( red circle )  . 
nodal signal intensity was documented along with the margin , which was classified as smooth and well defined or as irregular and poorly defined . immobilising systems were used to guarantee reproducigici erano sconosciuti . 
ad essi veniva chiesto di determinare la localizzazione e la dimensione del tumore e la sua estensione fuori dal retto , definendo profondit e direzione della diffusione extramurale del tumore . 
la fibrosi ha unintensit di segnale pi bassa e chiede di essere ipotizzata ; dallaltro lato , il tumore attivo era possibile se si evidenziava unampia estensione oppure una configurazione nodulare del margine laterale del tumore . sono stati esaminati il numero e le caratteristiche dei linfonodi pelvici . 
un linfonodo veniva considerato aumentato se la lunghezza era pi di 5 mm ( a livello del meso - retto ) , 7 mm ( a livello delliliaca interna ) , 10 mm ( a livello delliliaca esterna ) , o 9 mm ( a livello delliliaca comune )  . 
lintensit di segnale dei linfonodi stata documentata lungo tutto il margine , che veniva classificato come regolare e ben definito o come irregolare e poco definito . sono stati utilizzati dei sistemi di immobilizzazione per garantire la riproducibilit del trattamento frazionato . 
i pazienti sono stati posizionati supini tramite i supporti di immobilizzazione per le ginocchia e i piedi , o proni tramite luso di una cintura ( belly - board )  . 
la posizione supina stata usata solo per i pazienti che hanno ricevuto irradiazione della lesione meso - rettale e rettale ( escludendo i linfonodi pelvici ) , mentre la posizione prona con la belly - board consentiva lirradiazione dei linfonodi pelvici mediante la dislocazione delle anse intestinali . la dose totale di radiazione somministrata stata di 50 , 4 gray con una frazione di 180 cgray / die sulla lesione e 45 gray con lo stesso frazionamento sui linfonodi di drenaggio . 
inoltre , stata utilizzata una terapia radiante ad intensit modulata ( imrt ) per modulare lintensit del fascio radiante cos che la dose poteva conformarsi pi correttamente alla forma 3 - d del tumore e in misura minore alle strutture normali circostanti . 
 circa 15 cm cranialmente al margine anale , si osserva un ispessimento circonferenziale della parete rettale , prima del trattamento chemio - radiante ( cerchio rosso )  . bility of the fractionated treatment . 
the supine position was used only for patients who received mesorectal and rectal lesion irradiation ( excluding pelvic lymph nodes ) , whereas the prone position with a belly board allowed irradiation of the pelvic lymph nodes by displacing the bowel loops . 
 total radiation dose administered was 50.4 gy , with a fraction size of 180 cgy / daily on the rectal lesion and 45 gy with the same fraction size on draining lymph nodes . 
moreover , intensitymodulated radiation therapy ( imrt ) was used so that the dose could conform more precisely to the 3d shape of the tumour and less to the surrounding normal structures . 
oxaliplatin plus a chronomodulated schedule of capecitabine , such as 1 , 300 mg / m2 daily orally ( 8.00 am , 25% of radiol med ( 2012 ) 117 : 11251138 1131 total dose ; 6 pm , 50% ; 11 pm , 50% ) was administered . 
 capecitabine was given daily until the end of radiotherapy ; on the contrary , oxaliplatin was given at 100 mg / m2 on days 1 , 19 , and 38 of radiotherapy . 
some patients ( older patients or those with a low performance status ) received a lower dose of oxaliplatin ( 80 mg / m2 ) or alternatively only two doses ( compared with the three scheduled )  . 
evaluation of oncological response was based on the response evaluation criteria in solid tumours ( recist ) criteria of the european organization for research and treatment of cancer ( eortc ) , the national cancer institute of the united states and the national cancer institute of canada . 
 the therapeutic schemes applied were as follows : 31 patients ( 79.5% ) were treated according to the capecitabine plus oxaliplatin ( xelox ) protocol ; three patients ( 7.7% ) underwent the reduced - volume protocol ( treatment of the rectal and mesorectal lesion without treatment of the pelvic lymph nodes ) ; four patients ( 10.2% ) were treated with the interact protocol ( intensification therapy achieved by combining two chemotherapeutic agents or through a concomitant boost ) and one patient ( 2.6% ) was given a daily infusion of cisplatin during radiation therapy due to comorbidities that hindered the use of fluorine and platinum at standard doses . all patients underwent the same follow - up protocol , based on clinical examination every 3 months during the first year , every 6 months in the following 2 years and annually thereafter . 
specifically , we sought to interpret the value of the concordance of t and n obtained by mr imaging or pathological specimens . collimatori multi - lamellari , che producevano bande di radiazione con una forma irregolare ed asimmetrica vicina a quella del target volume . 
stato previsto un programma di oxaliplatino pi capecitabina crono - modulata , come per esempio 1300 mg / m2 / die per os ( ore 8 : 00 il 25% ; ore 18 : 00 il 50% ; ore 23 : 00 il 50% della dose totale )  . 
la capecitabina veni va somministrata giornalmente fino alla fine della radioterapia ; al contrario loxaliplatino veniva somministrato alla dose di 100 mg / m2 nei giorni 1 , 19 e 38 della radioterapia . alcuni pazienti ( i pi anziani o quelli con un basso performance status ) ricevevano una dose pi bassa di oxaliplatino ( 80 mg / m2 ) o alternativamente ricevevano solo due dosi ( rispetto alle tre previste )  . 
 lospedalizzazione veniva presa in considerazione in quei pazienti in cui veniva registrata una tossicit urinaria o gastro - intestinale di grado 3 . gli schemi terapeutici applicati erano i seguenti : 31 pazienti ( 79 , 5% ) erano trattati in accordo con il protocollo xelox ; 3 pazienti ( 7 , 7% ) si sono sottoposti al protocollo reduced volume ( trattamento della lesione rettale e mesorettale senza trattamento dei linfonodi pelvici ) ; 4 pazienti ( 10 , 2% ) erano trattati con il protocollo interact ( intensification therapy che realizzata tramite la combinazione di due agenti chemioterapici o attraverso un concomitant boost ) e ad un paziente ( 2 , 6% ) veniva data una infusione giornaliera di cisplatino durante la terapia radiante a causa delle comorbilit che comportava luso del fluoro e del platino alle dosi standard . tutti i pazienti sono stati sottoposti allo stesso protocollo di follow - up , basato sullesame clinico ogni tre mesi durante il primo anno , ogni sei mesi nei seguenti due anni e poi annualmente . 
 in one case , radiation therapy was interrupted ( total dose received was 43.2 gy ) due to the onset of grade 3 acute gastrointestinal toxicity ( proctitis )  . 
nine ( 23% ) patients did not receive one of the three scheduled infusions of oxaliplatin because of the onset of haematological ( n = 5 , 12% ) or gastrointestinal toxicity ( n = 4 , 10% )  . 
 the mean interval between the mr examination before and after chemoradiation was 92 ( range 67134 ) days , whereas the mean interval between the end of the chemoradiation therapy and mr re - staging was 29 ( range 5119 ) days . 
the cohen kappa test of concordance between post - chemoradiation mr staging and histological response showed an agreement of 83.6% if the disease was confined to the serosa ( t3 ) ( table 4 )  . 
the same statistical analysis for concordance between histology and mr staging of nodal disease yielded an agreement of 73% ( table 5 )  . radiol med ( 2012 ) 117 : 11251138 analisi statistica abbiamo utilizzato il test della k di cohen per determinare se fosse possibile una concordanza tra limaging di rm e i campioni patologici ottenuti dopo chirurgia . 
in particolare , abbiamo provato a interpretare il valore di concordanza del t e delln tramite la rm e tramite i campioni patologici . risultati la stadiazione pre - trattamento ottenuta tramite rm era come segue : 15 ( 38 , 5% ) ha mostrato t2n0m0 ; 1 ( 2 , 6% ) t2n1m0 ; 19 ( 48 , 7% ) t3n0m0 ; 3 ( 7 , 7% ) t3n1mo e 1 ( 2 , 6% ) t3n2m0 . 
la tolleranza globale al trattamento combinato era buona , dal momento che 38 pazienti ( 97 , 4% ) su 39 hanno portato a termine il trattamento alle dosi descritte . 
in un solo caso la terapia radiante stata interrotta ( la dose totale ricevuta era di 43 , 2 gray ) a causa dellinsorgenza di una tossicit gastro - intestinale acuta ( proctite ) di grado 3 . 
nove ( 23 , 1% ) pazienti non hanno ricevuto una delle tre infusioni di oxaliplatino come da programma a causa dellinsorgenza di tossicit ematologica o gastrointestinale , rispettivamente 5 pazienti ( 12 , 8% ) e 4 pazienti ( 10 , 3% )  . 
 lintervallo medio tra la rm prima e dopo il trattamento chemio - radioterapico era di 92 giorni ( range 67134 ) , mentre lintervallo medio tra la fine della terapia chemioradiante e il re - staging con rm era di 29 giorni ( range 51 19 )  . 
la microchirurgia endoscopica trans - anale ( met ) stata utilizzata in 3 pazienti ( 7 , 7% ) e altri 3 ( 7 , 7% ) sono stati sottoposti a resezione addominoperineale . 
tutti i pazienti sono stati sottoposti ad acquisizioni di immagini di rm seguite dopo la chemio - radioterapia neoadiuvante , per permettere un confronto tra la stadiazione di rm prima e dopo trattamento chemio - radioterapico . 
4a , b t2 - weighted turbo spin - echo sequence in sagittal planes : parietal thickening of the rectum , located 2 cm above the anal verge , before ( a ) and after ( b ) chemoradiation therapy , shrinkage of the tumour , with no mesorectal anterior fat infiltration observed after therapy ( red circle )  . 
si noti lispessimento parietale del retto , localizzato 2 cm cranialmente al margine anale , prima ( a ) e dopo ( b ) trattamento chemio - radiante : si osservi in fase posttrattamento la riduzione volumetrica del tumore , in assenza di infiltrazione del tessuto adiposo mesorettale sul versante amteriore ( cerchio rosso )  . 
lesame istologico ha rivelato un down - staging da t4n2m0 ( prima della terapia ) a t3n1m0 ( dopo la terapia )  . discussion the mesorectum is the fatty anatomical space around the rectum that contains mainly lymph nodes and vessels and is surrounded by the mesorectal fascia , which represents the circumferential resection margin ( crm ) when tme is performed . 
lanalisi di stadiazione istologica posttrattamento ( tnm ) ha rivelato 13 pazienti con una malattia > t2 e 26 pazienti con una malattia del retto t2 ( tabella 3 )  . 
analizzando tutto con lutilizzo del test della k di cohen per trovare il valore di concordanza tra la stadiazione rm dopo chemio - radioterapia e il responso istologico , abbiamo trovato che con una malattia confinata alla sierosa 1134 radiol med ( 2012 ) 117 : 11251138 fig . 
5a , b t2 - weighted turbo spinecho sequence in sagittal planes : parietal thickening of the rectum , located 3.5 cm above the anal verge , before ( a ) and after ( b ) chemoradiation therapy . 
si noti lispessimento parietale del retto , localizzato 3 , 5 cm cranialmente al margine anale , prima ( a ) e dopo ( b ) trattamento chemioradiante : si osservi in fase post - trattamento la mancata riduzione volumetrica del tumore ( cerchio rosso )  . 
 lesame istologico dopo terapia ha rivelato un down - staging di malattia esclusivamente a livello linfonodale ( da t4n2m0 a t4n1m0 )  . table 2 post - treatment histological staging post - treatment histological staging ( 26 with disease t2 ) 6 ( 23% ) tis n0 m0 10 ( 38.5% ) t1 n0 m0 5 ( 19.2% ) t2 n0 m0 3 ( 11.5% ) t2 n1 m0 2 ( 7.7% ) t3 n1 m0 tabella 2 stadiazione istologica dopo il trattamento post - treatment histological staging ( 13 with disease > t2 ) 10 ( 76.9% ) t3 n0 m0 3 ( 23% ) t3 n1 m0 stadiazione istologica dopo il trattamento ( 26 pazienti con malattia t2 ) stadiazione istologica dopo il trattamento ( 13 pazienti con malattia > t2 ) 10 ( 76 , 9% ) t3 n0 m0 3 ( 23% ) t3 n1 m0 6 ( 23% ) tis n0 m0 10 ( 38 , 5% ) t1 n0 m0 5 ( 19 , 2% ) t2 n0 m0 3 ( 11 , 5% ) t2 n1 m0 2 ( 7 , 7% ) t3 n1 m0 surgery . 
although no agreement is reported , it is thought that a distance of at least 5 mm between the tumour and the fascia is enough to exclude involvement of the latter and consequently a local recurrence [ 12 ]  . 
 staging rectal tumours using mr imaging is clearly critical for discovering t3 disease , as it is considered a subset of crm involvement and accordingly requires neoadjuvant treatment [ 13 ]  . 
in view of the importance of mr imaging in staging t3 cancers , we investigated its accuracy in predicting t3 stage by comparing imaging findings with histological response ( the gold standard )  . 
infatti , per far fronte ad un tumore t3 la considerazione principale da fare la distanza tra la massa neoplastica e la fascia meso - rettale ( o crm nei campioni isto - patologici ) , poich il coinvolgimento della fascia strettamente correlata alla recidiva dopo chirurgia . 
sebbene non vi sia nessuna concordanza riportata , si suppone che una distanza di almeno 5 mm tra tumore e fascia sia sufficiente per considerare risparmiato il coinvolgimento di questultima e una eventuale conseguente recidiva di malattia [ 12 ]  . 
 ovviamente , la stadiazione dei tumori del retto tramite lutilizzo della rm cruciale nellidentificare una malattia t3 , dal momento che considerato come un sottoinsieme del coinvolgimento del crm e in accordo ad esso richiede un trattamento neoadiuvante [ 13 ]  . 
in considerazione del fatto che possa giocare un importante ruolo nella stadiazione dei tumori di stadio t3 , abbiamo voluto capire quanto accurate fossero le immagini rm nella previsione dello stadio t3 tramite la comparazione dei dati radiologici con il responso istologico ( considerandolo sempre come gold standard )  . 
however , the magnetic resonance imaging and rectal cancer european equivalence ( mercury ) study group [ 15 ] predicted clear crm after radiotherapy with a high degree of accuracy despite the inability to distinguish residual cancer cells within a fibrotic area . 
such valuable results could be explained by considering two points : firstly , the mercury study enrolled a large number of patients , and accordingly , both diagnostic and therapeutic results were more likely to be significant ; secondly , the study emphasised the importance of quality control in image assessment , surgery and pathology in order to demonstrate the value of multidisciplinary preoperative management of rectal cancer based on constant training . 
the problems in nodal staging have been reported in many other studies and seem to relate to some open dilemmas , such parameters to be used to discern whether a node is pathological or not . 
 [ 17 ] suggested that many factors other than size be considered , such as spiculated or indistinct borders ( which may be due to perinodal fat tissue infiltration ) or a mottled heterogeneous appearance ( which may be due to intranodal necrosis and mucin build up )  . 
in the future , we may regularly use a contrast medium based radiol med ( 2012 ) 117 : 11251138 neoadiuvante aggressivo spesso esita in una cicatrice che non ci consente di identificare in maniera chiara la fibrosi prodotta dal tumore stesso . 
inoltre , con la rm standard non abbiamo la possibilit di discernere se pochi residui di cellule cancerogene sono nascoste nel tessuto fibrotico e possono quindi causare un coinvolgimento del crm allistologia ; le tecniche di imaging funzionale ( dynamic contrast enhancement rm , diffusion weighted sequences ) che possono aiutare a monitorare in maniera non invasiva la risposta del tumore al trattamento , sono ampiamente accettate [ 14 ]  . 
 tuttavia il gruppo di studio mercury [ 15 ] era in grado di predire chiaramente il margine di resezione circonferenziale dopo radioterapia con un alto grado di precisione , malgrado limpossibilit di distinguere piccoli residui di cellule cancerogene dentro larea fibrotica . 
questi risultati utili potrebbero essere spiegati prendendo in considerazione due punti : primariamente , lo studio mercury ha arruolato un largo numero di pazienti e in accordo con i risultati sia diagnostici che terapeutici era pi probabile che fossero significativi ; secondariamente , essi enfatizzano limportanza del controllo di qualit nella valutazione delle immagini , nella chirurgia , e nellanatomia patologica al fine di dimostrare il valore della gestione multidisciplinare preoperatoria del cancro del retto basato sulla formazione continua . per quanto riguarda il coinvolgimento dei linfonodi , la nostra esperienza si dimostrata essere troppo piccola nella capacit di fare differenze tra le immagini di rm e listologia . 
i problemi nella stadiazione linfonodale sono stati riportati in molti studi e sembrano correlare con alcuni dilemmi aperti come per esempio quello che riguarda i parametri che devono essere usati per distinguere se un linfonodo patologico oppure no . 
 [ 17 ] hanno suggerito che molti altri fattori oltre alle dimensioni dovrebbero essere usati , come per esempio i bordi spiculati o poco distinti ( che dovrebbero essere dati dallinfiltrazione del tessuto adiposo perilinfonodale ) o un aspetto disomogeneo ( che potrebbe essere dovuto alla necrosi intra - linfonodale e alla mucina formatasi )  . 
forse in futuro , useremo regolarmente un mezzo di contrasto basato su particelle di ossido di ferro superparamagnetico per mettere in evidenza micro - metastasi linfonodali , come riportato prima da bellin et al . 
abbiamo provato a differenziare una malattia minore o uguale a n1 e una malattia pi avanzata di n1 poich abbiamo pensato che il crescente numero di linfonodi coinvolti ( minore o uguale a 3 linfonodi per n1 o pi di 3 linfonodi per una malattia pi avanzata ) potrebbe rappresentare una buona opportunit per trovare una correradiol med ( 2012 ) 117 : 11251138 1137 up on superparamagnetic iron oxide particles in order to highlight nodal micrometastasis , as previously reported by bellin et al . 
we tried to differentiate between disease of n1 or less and more advanced than n1 , as we thought that the increasing number of nodes involved ( up to three nodes for n1 disease and more than three for more advanced disease ) could provide a good opportunity to find a correlation between mr imaging and histology . 
finally , as our sample size was relatively small , a bias cannot be excluded . to summarise , mr imaging is a good tool for determining tumour stage and allowing treatment to be tailored to individual patients . 
 our experience shows that neoadjuvant therapy based upon chemoradiation is generally well tolerated ; however , the addition of chemotherapy to radiation treatment may sometimes result in reduced tolerance , which could delay the scheduled plan . 
accordingly , an acceptable balance between toxicity and tumoricidal effect should be reached in each patient and , in our opinion , this goal can be achieved only by assembling a high - quality , professional team . lazione tra immagini rm e istologia . 
la nostra esperienza ha mostrato che la terapia neoadiuvante basata sulla chemio - radioterapia generalmente ben tollerata ; tuttavia , a volte laggiunta della chemioterapia al trattamento radiante pu risultare in casi di ridotta tolleranza che potrebbe portare alla riprogrammazione del piano terapeutico . 
di radiologia , ospedale di cattinara , azienda ospedaliero - universitaria , ospedale di cattinara , strada di fiume 447 , 34149 trieste , italy 2dipartimento scienze della vita , universit di trieste , piazzale europa 1 , 34127 trieste , italy 3u.c.o di neurologia , universit di trieste , ospedale di cattinara , azienda ospedaliero - universitaria , ospedale di cattinara , strada di fiume 447 , 34149 trieste , italy 4dipartimento di fisica , i.f.n.f. 
the aims of this study were to determine fractional anisotropy ( fa ) and the fibre density index ( fdi ) in the cervical spinal cord of patients with multiple sclerosis ( ms ) by using diffusion - tensor magnetic resonance imaging ( dt - mri ) to identify possible differences between ms patients and controls . 
we studied 27 patients with ms nine with primary progressive ( ppms ) , nine with secondary progressive ( spms ) and nine with relapsing remitting ( rrms ) disease and 18 healthy individuals as controls . 
sono stati arruolati 27 pazienti affetti da sm , 9 con decorso primario progressivo ( pp ) , 9 con decorso secondario progressivo ( sp ) e 9 con decorso recidivante remittente ( rr ) e 18 soggetti sani per controllo . 
stata osservata una differenza statisticamente significativa fra i valori di fdi nei pazienti e nei controlli ; in particolare sono state riscontrare differenze fra il gruppo di pazienti pp ed sp e i controlli . 
nonostante la ridotta numerosit del campione , i risultati ottenuti suggeriscono che la valutazione congiunta dei valori di fa e dellfdi rappresenta uno strumento valido per stimare il danno a livello del midollo spinale . keywords spinal cord multiple sclerosis magnetic resonance imaging diffusion tensor imaging parole chiave midollo spinale sclerosi multipla risonanza magnetica tensori di diffusione radiol med ( 2012 ) 117 : 12151224 1216 introduction introduzione spinal cord involvement is common in patients with multiple sclerosis ( ms ) and is a frequent cause of disability [ 13 ]  . 
although magnetic resonance ( mr ) imaging plays a key role in studying the spinal cord in these patients , it has largely been demonstrated that conventional sequences tend to underestimate the true extent of damage at the level of both the brain and the spinal cord , which show areas of involvement despite appearing normal on conventional imaging . 
in particular , conventional sequences are unable to characterise pathological abnormalities such as axonal injury and irreversible demyelination , which are more closely correlated with disability [ 47 ]  . 
from a clinical and therapeutic point of view , axonal injury appears to be caused by repeated disease relapses , which suggests that currently available treatments and , in particular , aggressive neuroprotective therapies , should be initiated as early as possible to limit the damage . 
these observations led to the introduction of nonconventional imaging techniques such as diffusionweighted sequences and , more recently , diffusion - tensor imaging ( dti ) to diagnose and follow - up patients with ms [ 810 ]  . the purpose of this study was to determine fractional anisotropy ( fa ) and fibre density index ( fdi ) values [ 11 , 12 ] at the level of the spinal cord in patients with ms and in a healthy control group by using dt - mri . materials and methods forty - five participants were included in the study : 27 patients with ms [ 18 women , nine men ; mean age 42 ( range 2363 ) years ] , with a mean disease duration of 10 ( range 132 ) years and disability score of 3.7 ( range 17 ) assessed using the expanded disability status scale ( edss )  . 
 after providing informed consent , all participants underwent mr imaging on a 1.5 - t philips achieva scanner ( philips achieva version 2.1.3.4 ; philips medical systems , best , the netherlands ) , with 33 mt / m gradients and 150 t / ms slew rate . 
first , conventional sequences were acquired in the sagittal plane for the morphological study il coinvolgimento del midollo spinale nella sclerosi multipla ( sm ) un evento comune , spesso causa di disabilit [ 13 ]  . 
 nonostante limaging di risonanza magnetica ( rm ) giochi un ruolo fondamentale nello studio del midollo spinale nei pazienti affetti da sm , stato ampiamente dimostrato che le sequenze convenzionali tendono a sottostimare la reale estensione del danno , non solo a livello cerebrale ma anche a livello del midollo spinale , che risultano coinvolti anche nelle sedi che appaiono indenni allimaging convenzionale . 
 nello specifico , le sequenze convenzionali non sono in grado di caratterizzare alterazioni patologiche quali il danno assonale e la demielinizzazione irreversibile , pi strettamente correlate alla disabilit [ 47 ]  . 
da un punto di vista clinico e terapeutico , il danno assonale sembra essere determinato da ripetute ricadute della patologia , suggerendo pertanto lutilit di attuare pi precocemente possibile i trattamenti attualmente a disposizione al fine di limitare il danno stesso , in particolare di una terapia neuroprotettiva aggressiva . 
queste considerazioni hanno portato allintroduzione di tecniche di imaging non convenzionale , tra le quali le sequenze pesate in diffusione e pi recentemente limaging con tensore di diffusione ( dti ) , sia per la diagnosi che per il follow - up dei pazienti con sm [ 810 ]  . lobiettivo di questo studio stato quello di valutare , mediante dti - rm , i valori di anisotropia frazionaria ( fa ) e del fiber density index ( fdi ) [ 11 , 12 ] a livello del midollo spinale nei pazienti affetti da sm e in un gruppo di controllo . materiali e metodi nello studio sono stati inclusi 45 soggetti : 27 pazienti erano affetti da sm ( 18 donne , 9 uomini ; et media di 42 anni e range di 2363 anni ) , con una durata media della patologia pari a 10 anni ( range 132 anni ) e disabilit pari a 3 , 7 ( range 17 ) valutata con la expanded disability status scale ( edss ) ; di questi pazienti 9 presentavano un decorso recidivante - remittente ( rr ) , 9 un decorso primario progressivo ( pp ) e 9 secondario progressivo ( sp )  . 
 una volta ottenuto un consenso informato , tutti i soggetti sono stati sottoposti ad unindagine di rm con unapparecchiatura philips achieva da 1 , 5 tesla ( philips achieva versione 2.1.3.4 , philips medical systems , best , paesi bassi ) , radiol med ( 2012 ) 117 : 12151224 1217 of the spinal cord . 
a diffusion - weighted imaging ( dwi ) sequence was then obtained in the axial plane , with b values of 0 and 1000 mm2 / s and diffusion - sensitising gradients applied in 32 directions ( tr 6 , 731 ; te 91 ; flip angle 90 ; 40 slices , slice thickness 2 mm ; isotropic voxel 222 mm ; slice interval 0 ; number of averages 1 ; field of view 224224 ; acquisition time 4.02 min ; sense factor 2 ; fat suppression )  . 
no device was used to correct image registration and distortion , and no cardiac gating was used ; each series of dwis was carefully checked to exclude the presence of motion artefacts . 
in the tractography analysis , threshold values were established on the basis of white matter fa values reported in the literature : a minimum fa value of 0.25 and maximum curvature angle of 70 . 
on the basis of these maps , regardless of the presence or absence of demyelinating plaques , a region of interest ( roi ) was placed every three layers of cervical cord , starting from the first : each roi had an ovoid shape and fixed area of 80 mm2 ( 20 pixels ) and was adapted to the area of cervical cord visible in the axial plane , taking care not to include the cerebrospinal fluid . 
in each roi , mean fa values , total number of fibres contained in the region [ 12 ] and fdi were calculated , which indicates the average number of fibres present in each pixel of the roi [ 10 ]  . data were analysed using multivariate analysis [ analysis of variance ( anova ) ] to assess the heterogeneity of the groups included in the study ; students t test was used for post hoc comparison between patients with the different forms of disease and normal controls . 
the p value for statistical significance was set at 0.05. for each patient , we calculated the total lesion burden in the cervical cord segment examined ( c2c5 ) by using the mricro programme and verified whether a statistically significant correlation existed between lesion burden in each group and in all patients . 
dapprima sono state eseguite sequenze convenzionali sul piano sagittale per lo studio morfologico del midollo spinale ed in particolare sono state eseguite una sequenza turbo spin echo ( tse ) pesata in t2 [ tempo di ripetizione ( tr ) = 3500 , tempo di eco ( te ) = 120 , flip angle 90 , spessore di strato = 3 mm , intervallo fra gli strati di 0 , 30 ; tempo di scansione = 3 , 3 minuti ] e una sequenza short time inversion recovery ( stir ) [ tr = 2500 , te = 10 , inversion time ( ti ) = 170 ms , flip angle 90 , spessore di strato = 3 mm , intervallo fra gli strati di 0 , 30 ; tempo di scansione = 4 , 35 minuti ]  . 
successivamente stata eseguita una sequenza pesata in diffusione , sul piano assiale , con valori di b pari a 0 e 1000 mm2 / s e con gradienti sensibilizzati alla diffusione applicati in 32 direzioni dello spazio ( tr = 6731 , te = 91 , flip angle = 90 , 40 strati , spessore di strato = 2 mm , voxel isotropico pari a 222 mm , intervallo tra gli strati pari a 0 , medie = 1 , campo di vista = 224224 , durata dellacquisizione = 4 , 02 minuti , fattore sense = 2 , soppressione del segnale del tessuto adiposo )  . 
non sono stati utilizzati accorgimenti per la correzione della registrazione e della distorsione delle immagini n il gating cardiaco ; ogni serie di immagini pesate in diffusione stata controllata accuratamente per escludere la presenza artefatti da movimento . 
per lanalisi mediante trattografia sono stati applicati valori soglia sulla base dei valori di fa della sostanza bianca riportati in letteratura : valore minimo di fa pari a 0 , 25 ed angolo massimo di curvatura pari a 70 . 
sulla base della mappa colorimetrica , indipendentemente dalla presenza o meno di placche di demielinizzazione , stata posizionata una regione di interesse ( roi ) ogni 3 strati di midollo cervicale a partire dal primo : ogni roi aveva forma ovalare , dimensioni fisse pari a 80 mm2 ( 20 pixels ) , e veniva adattata in ogni soggetto allarea di midollo visibile sul piano assiale prestando attenzione a non includere il liquor cerebrospinale . 
per ogni roi sono stati calcolati il valore medio di fa , il numero totale di fibre in essa contenuto [ 12 ] e lfdi che esprime il numero medio di fibre contenuto in ogni pixel della roi [ 10 ]  . i dati ottenuti sono stati analizzati con lanalisi statistica multivariata anova per valutare leterogeneit dei gruppi inclusi nello studio e successivamente stato applicato per confronti post - hoc tra pazienti nelle varie forme e normali il test t di student . 
sono state valutate le differenze fra i valori di fa e dellfdi nel gruppo di pazienti e nel gruppo di controllo e le differenze di tali valori fra le tre forme cliniche di sm . 
 it was then extended to the assessment of normal - appearing white and grey matter , with results consistent with those obtained with other mr techniques , which confirms that the apparently normal white matter on conventional imaging is , in fact , already altered during the early stages of the disease radiol med ( 2012 ) 117 : 12151224 valori di fa e dellfdi ottenuti e let ed il grado di disabilit dei soggetti . 
il valore di significativit statistica p stato fissato a 0 , 05 . per ogni paziente stato inoltre calcolato il carico lesionale , mediante il programma mricro nel tratto di midollo cervicale indagato ( c2 - c5 ) ed stato verificato se esiste una correlazione statisticamente significativa tra carico lesionale per ogni singolo gruppo e per tutti i pazienti . 
il valore di significativit statistica stato fissato a p < 0 , 05 . risultati dallanalisi statistica non sono emerse differenze significative fra il valore di fa osservato nel gruppo con sm e quello osservato nel gruppo di controllo : nel gruppo con sm sono stati ottenuti valori medi di fa pari a 0 , 69 ( ds 0 , 04 ) nel gruppo con la forma pp , 0 , 60 ( ds 0 , 04 ) nel gruppo con la forma sp e 0 , 68 ( ds 0 , 04 ) in quello con forma rr . 
nel gruppo di controllo stato riscontrato un valore pari a 0 , 68 ( ds 0 , 04 )  . per quanto riguarda lfdi , stata riscontrata una differenza statisticamente significativa fra lintero gruppo di pazienti con sm ed il gruppo di controllo per valori di significativit p < 0 , 01 . 
lanalisi statistica anova dellfdi ha messo in evidenza leterogeneit sia nel gruppo di pazienti con sm che fra il gruppo di pazienti ed il gruppo di controllo : lfdi risultato pari a 10 , 4 ( ds 4 , 9 ) nei pazienti con forma pp , 11 , 4 ( ds 4 , 7 ) nei pazienti con forma sp e 13 , 6 ( ds 6 , 1 ) in quelli con forma rr . 
 il confronto fra le forme cliniche di sm ed i soggetti sani mediante test t di student risultato significativo per i pazienti con forma pp e per i pazienti con forma sp per livelli di significativit p < 0 , 05 . 
successivamente stata estesa anche alla valutazione sia della sostanza bianca che della sostanza grigia apparentemente normali con risultati coerenti con quelli ottenuti con altre tecniche di rm a conferma del fatto che la sostanza bianca apparentemente normale allimaging convenzionale in realt alterata gi nelle fasi precoci della patologia [ 3 , 68 , 13 , 14 ]  . 
in particolare stato indagato il midollo cervicale , sia perch maggiormente colpito dalla sm rispetto al midollo toracico sia perch questultimo pi sottile e difficile da studiare a causa della bassa risoluzione delle fig . 
significant correlations are observed in both groups ; moreover , the correlation lines are statistically different ( see text )  . fig 2 correlazione tra fdi e fa per i pazienti ( cerchi vuoti ) e controlli ( rombi neri )  . 
these studies investigated in particular the cervical cord because it is both more severely affected by ms than is the thoracic cord and because the latter is thinner and more difficult to visualise owing to the low resolution of dti [ 15 ]  . `several studies have found different fa values at the level of the cervical cord in the comparison between healthy individuals and ms patients , especially patients with spms and rrms . 
regarding fa values at the level of the cervical cord , regardless of the presence of plaques , our study detected no significant difference but only a trend towards significance , which is in agreement with results reported by other authors . 
this lack of significance may be ascribed to several factors , particularly to the small patient population and to the suboptimal radiol med ( 2012 ) 117 : 12151224 immagini ottenute con dti [ 15 ]  . 
 numerosi studi hanno dimostrato differenti valori di fa a livello del midollo cervicale confrontando soggetti sani e pazienti con sm , soprattutto per quanto riguarda le forme sp ed rr . 
nella maggior parte di questi studi i valori di fa sono stati determinati sia in presenza che in assenza di placche di demielinizzazione visibili con limaging convenzionale [ 5 , 9 , 1523 ]  . 
 [ 24 ] ha riscontrato differenze statisticamente significative fra i valori di fa soltanto fra il gruppo di controllo ed i pazienti con rr , mentre quello di ohgiya et al . 
 per quanto riguarda i valori di fa a livello del midollo cervicale , a prescindere dalla presenza o meno di placche , il nostro studio non ha dimostrato alcuna differenza significativa , nonostante sia stato dimostrato un trend di significativit in accordo con i risultati ottenuti da studi precedenti . 
 il nostro lavoro di ricerca aveva un orientamento clinico , motivo per il quale stata utilizzata unapparecchiatura da 1 , 5 tesla con una durata dellacquisizione dti clinicamente accettabile , pari a 4 minuti . 
 [ 26 ] hanno dimostrato che la misurazione dei valori di fa gravata da una bassa riproducibilit qualora basata sullutilizzo di una roi , anche se effettuata dallo stesso osservatore e sulla stessa serie di immagini ; a nostro avviso , i nostri risultati concordano con questa osservazione . necessario sottolineare come il confronto con i dati presenti in letteratura non sia agevole a causa della differente metodologia desame e di analisi . 
oltretutto il valo re di fa un parametro sensibile sia al rapporto segnale / rumore che al numero delle direzioni dei gradienti ; tenu to conto che a livello del midollo cervicale le immagini sono rumorose , i valori di fa di riferimento dovrebbero essere definiti in ogni struttura e per ogni protocollo clinico [ 27 ]  . 
da mettere in evidenza come tale valore , calcolato nella stessa roi in cui stato misurato il valore di fa , sia statisticamente differente nel gruppo di controllo rispetto ai sottogruppi di sm , mentre tale differenza non stata riscontrata per quanto riguarda i valori di fa . 
per quanto radiol med ( 2012 ) 117 : 12151224 quality of the images obtained . our study had a clinical orientation , which accounts for the use of a 1.5 - t device with clinically acceptable length ( 4 min ) of dti acquisitions . 
 [ 26 ] demonstrated that fa determination is limited by low reproducibility whenever it is based on the use of an roi , even when this is defined by the same observer and on the same series of images ; in our opinion , our results are consistent with this observation . it should be noted that comparison with the literature is not easy owing to the different methods used for examination and analysis . 
furthermore , fa is a parameter that depends on the signal - to - noise ratio ( snr ) and on the number of gradient directions ; considering that images are noisy at the level of the cervical cord , reference fa values should be defined in each structure and for each clinical protocol [ 27 ]  . 
it should be noted that this value , calculated in the same roi used for fa determination , was statistically different in the control group compared with the ms subgroups , whereas no difference was noted in fa values . 
with regard to fdi , heterogeneity was demonstrated in ms subgroups and the control group , and a statistically significant difference was found between the spms group and controls and between the ppms group and controls . 
these results reflect the prevalence of axonal damage in ms patients damage that is already present during the initial stages of the disease and that worsens in the progressive forms . 
although the process of remyelination may preserve axonal function , regenerated fibres are usually thin and not compact , which accounts for the low fdi values in the three subgroups . 
it is known that the number of reconstructed fibre tracts is algorithm dependent ; therefore , fdi values must be measured in each study using the same software and settings . 
in this study , we used the same software used in previous studies to analyse fdi at the brain level the dti studio programme [ 10 , 11 ]  . 
at the level of the spinal cord , qualitatively superior results could be obtained by using dedicated tractography techniques [ 30 ] and by raising the snr by increasing the number of dwis [ 27 ] or by using a high - field scanner . 
 other limitations of our study are the small number of patients and the poor dti quality , as they were acquired 1221 riguarda lfdi stata dimostrata uneterogeneit nei sottogruppi di sm e nel gruppo di controllo e una differenza statisticamente significativa fra il gruppo sp ed i controlli e fra il gruppo pp ed i controlli . 
questi risultati riflettono la prevalenza del danno assonale nei pazienti con sm , danno che si verifica gi nelle fasi iniziali della patologia e si accumula nelle forme progressive della stessa . 
noto che il numero di fibre ricostruite algoritmo - dipendente , quindi i valori dellfdi devono essere valutati in ogni studio con il medesimo software ed impostando gli stessi parametri . 
a livello del midollo spinale si potrebbero ottenere risultati qualitativamente superiori mediante tecniche trattografiche dedicate [ 30 ] e incrementando il rapporto segnale / rumore ottenibile aumentando il numero di immagini pesate in diffusione [ 27 ] o ricorrendo ad apparecchiature ad alto campo . 
qualora i nostri risultati fossero confermati su un campione numericamente maggiore , potrebbero essere sviluppate tecniche dedicate allo studio del midollo spinale in grado di consentire una rapida valutazione dei parametri fdi ed fa . 
nel nostro studio non abbiamo correlato i valori dellfdi ottenuti a livello del midollo cervicale con il carico lesionale cerebrale , in quanto questultimo condiziona la densit delle fibre nervose in virt della degenerazione walleriana , ma , come dimostrato in studi recenti [ 16 ] , il contributo di questo processo al danno assonale marginale . 
we did not correlate fdi values obtained at the level of the cervical cord with cerebral lesion burden because this influences nerve fibre density as a result of wallerian degeneration ; however , as demonstrated [ 16 ] , the contribution of this process to axonal injury is only marginal . 
conversely , we did study the correlation between fdi and cervical cord lesion burden , which was not found to be statistically significant despite a trend towards significance in spms patients . 
this may be explained in part by the small number of individuals studied but also by the fact the fdi ( which reflects axonal organisation ) might also be influenced by lesions located outside the voi . 
cervical cord atrophy was not measured ; the roi selected for tractography was positioned at the level of the residual cervical cord tissue , displayed in blue on the colour - coded map . 
 from a clinical viewpoint , no correlation was found between the fa values and edss scores in ms patients , between the fdi and edss scores or between fdi and age or fa values and age . 
the existence of a significant , although minimal , correlation between fa values and age at the spinal cord level was recently demonstrated by using a dedicated technique for studying the spinal cord based on tractography segmentation ; however , on the same series of images , no correlation was found between patient age and fa values using manual positioning of rois , even in a patient population twice as large as ours and using a threefoldlonger acquisition time [ 30 ]  . 
the lack of correlation between clinical findings and values obtained at dti could be explained by the relatively small number of patients ; furthermore , edss scores obtained from the clinical assessment of disability reflect the degree of overall patient disability , which is also related to cerebral lesions . we did not use a device to correct image registration and distortion or any cardiac gating ; motion artefacts are not common in cervical cord images of cooperative patients , as the spine is in close contact with the patient bed and only an abrupt and significant movement of the head could produce an artefact in low - resolution dwis . 
a similar approach was adopted by other authors who used a 1.5 - t device and images with the same spatial resolution [ 26 ]  . conclusions we used fdi to assess the contribution of dti when studying the spinal cord in patients with ms . 
non stata inoltre valutata latrofia del midollo spinale cervicale ; la roi per la trattografia stata posizionata a livello del midollo cervicale residuo , visualizzabile in blu nella mappa colorimetrica . 
 da un punto di vista clinico , non stata osservata alcuna correlazione fra i valori di fa ed il punteggio della scala edss nei pazienti con sm , n fra lfdi ed il punteggio edss , tantomeno fra lfdi e let e fra i valori di fa e let . 
stata recentemente dimostrata lesistenza di una significativa , seppur minima , correlazione fra i valori di fa e let a livello del midollo spinale utilizzando una tecnica dedicata allo studio del midollo spinale basata sulla trattografia mediante segmentazione ; sulla medesima serie di immagini non stata per osservata alcuna correlazione fra let ed i valori di fa utilizzando il posizionamento manuale della roi , anche in presenza di un campione numericamente doppio rispetto al nostro e con un tempo di acquisizione tre volte pi lungo [ 30 ]  . 
la mancata correlazione fra i rilievi clinici ed i valori ottenuti mediante dti potrebbe essere ricondotta principalmente alla relativa scarsa numerosit del gruppo di pazienti ; inoltre i punteggi ottenuti nella valutazione clinica della disabilit mediante edss riflettono il grado di disabilit globale dei pazienti alla quale contribuiscono anche le lesioni cerebrali . nel nostro studio non sono stati applicati accorgimenti per correggere la registrazione e la distorsione delle immagini n lacquisizione con gating cardiaco ; gli artefatti da movimento nelle immagini del midollo cervicale sono un evento raro in pazienti collaboranti in quanto il rachide si trova a stretto contatto con il lettino porta paziente e solo un brusco ed importante movimento del capo potrebbe determinarne la comparsa in immagini a bassa risoluzione quali quelle pesate in diffusione . 
lo stesso tipo di approccio stato utilizzato da altri autori che hanno a disposizione unapparecchiatura da 1 , 5 tesla ed immagini con la stessa risoluzione spaziale [ 26 ]  . conclusioni nel nostro lavoro abbiamo applicato lfdi per valutare il contributo fornito dal dti nello studio del midollo spinale in pazienti affetti da sm . 
i risultati ottenuti suggeriscono come lfdi possa rappresentare , associato alla misurazione dellfa , un parametro efficace per una valutazione del radiol med ( 2012 ) 117 : 12151224 1223 ments . 
 nevertheless , further studies using tractography dedicated to studying the spinal cord should be conducted on a larger and more representative number of ms patients to define the role of dti and its possible applications in clinical practice . danno assonale a livello del midollo spinale . 
between march 2005 and may 2010 , 13 patients ( eight men and five women ; mean age 67.08 years , range 3895 ) with rcc and rvt associated or not with ivc thrombosis underwent implantation of a retrievable suprarenal ivc filter . 
implantation of a temporary suprarenal ivc filter is an additional and feasible procedure that can prevent immediate and perioperative pe . keywords renal cell carcinoma inferior vena cava filter renal vein thrombosis riassunto obiettivo . 
tra marzo 2005 e maggio 2010 , 13 pazienti ( 8 maschi e 5 femmine ) con rcc e trombosi della vena renale associata o meno a quella della vci , sono stati sottoposti al posizionamento di un filtro cavale removibile in sede sovrarenale . 
tutti i pazienti sono stati sottoposti ad angio - tomografia computerizzata ( cta ) , indagine che ha documentato una trombosi della vena renale e talvolta la sua estensione alla vci . 
limpianto di un filtro cavale di tipo removibile in vci una procedura aggiuntiva e fattibile , che pu evitare lembolia polmonare immediata nel periodo perioperatorio . parole chiave carcinoma a cellule renali filtro cavale trombosi della vena renale introduction introduzione the incidence of renal cell carcinoma ( rcc ) is increasing worldwide [ 14 ] , possibly as a result of improvements in radiological diagnosis . 
the common use of imaging methods such as ultrasound ( us ) , computed tomography ( ct ) and magnetic resonance ( mr ) imaging as a first - line investigation for a multiplicity of indications has led to earlier detection of asymptomatic renal tumours that would have otherwise remained undetected [ 1 ]  . 
when renal tumours remain silent or are in the presence of disease progression , extension of the tumour thrombus into the renal vein and / or the inferior vena cava ( ivc ) is one of the most challenging presentations . 
this complication has been reported to occur in 410% of patients [ 5 , 6 ]  . in those cases with an aggressive surgical approach is recommended even if there is tumour invasion of the ivc . 
before the introduction of ivc filters , surgical cava ligation or plication was performed to protect patients from potentially lethal pe if these patients could not receive anticoagulants [ 10 , 11 ]  . 
implantation of a temporary suprarenal ivc filter is an additional procedure that can avoid immediate and perioperative pe [ 8 , 9 , 12 ]  . the purpose of our study was to evaluate the feasibility , safety and efficacy of suprarenal ivc filters in patients with a tumour thrombus extending into the renal vein or ivc . 
 materials and methods patients and lesions lincidenza di carcinoma a cellule renali ( rcc ) in aumento in tutto il mondo [ 14 ] ; tale dato sembra essere collegato al perfezionamento della diagnosi radiologica del carcinoma renale , ovvero lutilizzo di metodiche di imaging quali ultrasonografia ( us ) , tomografia computerizzata ( tc ) e risonanza magnetica ( mri ) , ha portato alla diagnosi precoce dei tumori renali asintomatici che altrimenti non sarebbero stati diagnosticati [ 1 ]  . 
se i tumori renali restano misconosciuti o se vi progressione della malattia , si pu osservare linvasione neoplastica della vena renale e talvolta anche della vena cava inferiore ( vci ) ; questa considerata una delle complicanze pi gravi e viene riscontrata nel 4%10% dei pazienti con rcc [ 5 , 6 ]  . 
nei pazienti che non potevano essere sottoposti a terapia anticoagulante , prima dellintroduzione dei filtri cavali , veniva eseguita la legatura chirurgica della vci per prevenire la ep , potenzialmente letale in questo gruppo di soggetti [ 10 , 11 ]  . 
il posizionamento di un filtro cavale in sede sovrarenale una procedura aggiuntiva , che previene lembolia polmonare durante lintervento di nefrectomia e nel periodo perioperatorio [ 8 , 9 , 12 ]  . lo scopo del nostro studio consiste nel valutare la fattibilit , la sicurezza e lefficacia dei filtri cavali in sede sovrarenale nei pazienti con trombosi neoplastica della vena renale ed eventualmente della vena cava inferiore . this is a retrospective study of patients with rcc and renal vein and ivc thrombosis who underwent suprarenal implantation of a removable ivc filter at our institution between march 2005 and may 2010 ( table 1 )  . 
all patients received 110130 ml of iodinated contrast material ( iomeron 350 , bracco , milan , italy ) at an injection rate of 2 ml / s , followed by 40 ml of saline solution at the same rate , using a dual - head automatic injector . 
the ct scan extended from the 12th thoracic vertebra to the middle of the femoral tuto nel periodo compreso tra marzo 2005 e maggio 2010 ( tabella 1 )  . 
1a , b computed tomography ( ct ) scan reveals right renal vein thrombosis ( a ) ; coronal view better reveals the extension of the thrombosis ( b )  . 
1a , b lesame ct evidenzia la trombosi della vena renale destra ( a ) ; la ricostruzione secondo il piano coronale meglio documenta lestensione della trombosi della vena renale destra ( b )  . 
 filter implantation technique all procedures were carried out in the angiography suite using a digital angiographic device ( allura , philips medical systems , best , the netherlands )  . 
a right internal jugular vein puncture was performed after local anaesthesia ( 10 ml of 2% carbocaine ) , and ivc phlebography was carried out to determine the level of the tumour thrombus . 
after the filter delivery sheath was placed in the suprarenal ivc , the filter was deployed according to the manufacturers guidelines ( aln implants chirurgicaux , ghisonaccia , france )  . 
following removal , ivc cavography was carried out through the retrieval sheath . dal livello della xii vertebra toracica fino al iii medio del femore , con un ritardo di 120150 secondi dallinizio della somministrazione del mezzo di contrasto . 
2 a , b una cavografia preliminare evidenzia il livello dello sbocco delle vene renali e lestensione della trombosi ( a ) ; alla fine della procedura , una nuova cavografia conferma il corretto posizionamento del filtro ( b )  . vografia inferiore per confermare la perviet della vci e lassenza di complicanze . sono stati registrati i dati clinici e di imaging di ciascun paziente . 
una angio - tc ( cta ) stata eseguita una settimana prima di rimuovere il filtro con la stessa tecnica tc descritta sopra . risultati in questo studio , sono state valutate la fattibilit , la sicurezza e lefficacia dellimpianto del filtro cavale removibile nel tratto sovrarenale della vci , in pazienti con carcinoma renale e trombosi della vena renale omolaterale e talvolta della vci , prima di essere sottoposti ad intervento chirurgico di nefrectomia . la fattibilit stata definita come il corretto posizionamento del filtro cavale . 
there was no evidence of filter migration . discussion thrombosis of the renal vein and ivc and its extension into the ivc occurs in 410% of patients with a renal tumour radiol med ( 2012 ) 117 : 11901198 1195 fig . 
non vi stato alcun caso di migrazione del filtro . discussione la presenza di una trombosi neoplastica della vena renale e lestensione della stessa nella vci si verifica nel 4%10% dei pazienti con un tumore renale [ 5 , 6 ]  . 
a scopo preventivo , pu essere eseguito il clampaggio chirurgico diretto della porzione sovrarenale della vci o quello guidato da ecocardiografia trans - esofagea [ 10 , 11 ]  . lo scopo del nostro studio di valutare lopportunit di utilizzo di una metodica meno invasiva , ossia limpianto di filtri cavali removibili , in genere collocati sotto lafferenza della vena renale in vci , anche se non vi un protocollo standard per il posizionamento di tali filtri . 
in assenza di un protocollo standard per il posizionamento del filtro cavale sovrarenale , vi sono alcuni fattori che vengono presi in considerazione dalla maggior parte degli autori , tra cui : il calibro del vaso in quanto eventuali restringimenti del lume ( ab - intrinseco o ab - estrinseco ) della vci a tale livello impediscono il pofig . 
4a , b il filtro viene catturato dal device di rimozione ( a ) e successivamente introdotto nel catetere ( b )  . 1196 table 2 literature review feng et al . 
 [ 12 ] vci , vena cava inferiore radiol med ( 2012 ) 117 : 11901198 authors patients thrombosis extension filter type removal renal vein and ivc renal vein and ivc renal vein and ivc ( 4 patients ) renal vein and ivc ( 2 patients ) tempofilter ii 1 gnther tulip ; 1 optease autori pazienti estensione della trombosi tipo di filtro rimozione vena renale e vci vena renale e vci in 4 pazienti vena renale e vci in 2 pazienti vena renale e vci tempofilter ii 1 gnther tulip ; 1 optease the aim of our study was to evaluate the use of a removable ivc filter as a less invasive treatment . 
in the absence of a standard protocol for suprarenal filter placement , some indications are followed by most authors , which include evaluation of vessel diameter , because intrinsic or extrinsic narrowing of the infrarenal ivc is a contraindication for placement of an ivc filter [ 14 ] ; the possibility of gonadal or rvt [ 1517 ] and anatomical variations of the ivc or renal veins must be considered for each patient . 
 these factors influence the choice of filter and the risk of incomplete protection [ 18 ] and may be associated with a major incidence of complications , such as filter migration [ 19 ] , perforation of the ivc [ 20 ] and device fracture [ 12 ]  . different papers have reported on the feasibility and efficacy of this technique ( table 2 )  . 
no metastases or tumour recurrences were sizionamento del filtro [ 14 ] ; la possibilit di una trombosi dei vasi gonadici e delle vene renali [ 1517 ] e le variazioni anatomiche della vena cava inferiore e delle vene renali che necessitano di essere valutate caso per caso . 
questi fattori influenzano la scelta del filtro e il rischio di incompleta protezione [ 18 ] , e possono esporre a complicanze , quali la migrazione del filtro [ 19 ] , la perforazione della vci [ 20 ] e la rottura del dispositivo [ 12 ]  . in letteratura diversi lavori hanno confermato la fattibilit e lefficacia di questa tecnica ( tabella 2 )  . 
durante il follow - up , disponibile per 61 dei 70 pazienti , 10 hanno presentato sintomi e segni di ep ( un paziente ha presentato due episodi )  . 
trenta dei 361 filtri cavali sono stati collocati in sede sovrarenale in pazienti con estesa trombosi cavale o con trombosi della vena renale che si estendeva allvci e solo 14 dei 30 pazienti avevano un tumore maligno con radiol med ( 2012 ) 117 : 11901198 1197 detected during the follow - up period ( range 218 months ) [ 8 ]  . 
of these , 30 ivc filters were placed in a suprarenal position in patients with extensive caval thrombosis or rvt extending to the ivc , and only 14 / 30 patients had a malignancy with thrombosis extending to the ivc . 
placement of a removable suprarenal ivc filter before performing radical nephrectomy for rcc with neoplastic involvement of the renal vein and / or ivc reduces or eliminates the possibility of pe , avoiding any potential complications of permanent ivc filter placement [ 9 ]  . in our experience , we performed 13 suprarenal ivc implantations . 
il posizionamento di un filtro cavale removibile sovrarenale prima della nefrectomia radicale per rcc con trombosi della vci , riduce sino ad annullare la possibilit di ep , evitando ogni potenziale complicanza tipica del filtro cavale permanente [ 9 ]  . nella nostra esperienza abbiamo eseguito 13 impianti di filtri cavali sovrarenali . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , fondazione policlinico di tor vergata , viale oxford 81 , 00133 roma , italy 2stroke unit , dipartimento di neuroscienze , fondazione policlinico di tor vergata , viale oxford 81 , 00133 roma , italy correspondence to : c . 
we retrospectively reviewed 18 consecutive patients with acute ischaemic stroke due to the occlusion of large cerebral vessels who were treated with mechanical thrombolysis at our centre between september 2009 and july 2010 . 
riportiamo retrospettivamente i risultati di 18 pazienti consecutivi affetti da ictus ischemico acuto dovuto ad occlusione di vasi cerebrali di grosso calibro trattati con trombolisi meccanica nel nostro centro tra settembre 2009 e luglio 2010 . 
tutti i pazienti hanno eseguito un esame neurologico ed uno studio in angio - risonanza magnetica ( rm ) post - procedurale a distanza di 3 e 6 mesi dal trattamento . 
our preliminary experience with the penumbra mechanical thrombolysis system confirms previously reported results showing the efficacy and safety of the device in treating acute stroke caused by the occlusion of large intracranial vessels . keywords stroke thrombolysis stent endovascular in 5 pazienti ( 27 , 8% ) una procedura di stenting stata necessaria . 
la nostra esperienza preliminare con il sistema di trombolisi meccanica penumbra conferma risultati precedentemente riportati , dimostrando la sua efficacia e sicurezza nel trattamento dello stroke acuto dovuto allocclusione di vasi endocranici di grande calibro . parole chiave stroke trombolisi stent endovascolare introduction introduzione cerebral stroke is the third leading cause of death in the western world and the main cause of disability among the elderly , with a significant social and economic impact . 
 [ 1 ] , intravenous thrombolytic treatment in this condition has a high failure rate : only 30% of patients show any improvement in symptoms [ modified rankin scale ( mrs ) 2 ]  . 
the development of intra - arterial pharmacological thrombolysis and the introduction of mechanical thrombolysis devices have extended the time window for treatment and enabled effective treatment with a low rate of complications [ 2 ]  . 
 with the catheter positioned proximal to the vascular occlusion , thrombotic tissue within the artery is aspirated and removed , minimising the risk of dissection , vascular fissures and distal embolisms [ 3 ]  . 
other studies report similar results when treating ischaemic stroke with mechanical thrombolysis alone [ 5 , 6 ] and combined with the administration of fibrinolytic agents [ 7 ]  . we report on our experience with the penumbra device to assess the potential efficacy , safety and clinical benefits of endovascular revascularisation of cerebral vascular occlusions in patients with acute cerebral stroke . 
 [ 1 ] il trattamento trombolitico endovenoso in questo tipo di patologia presenta un elevato tasso di insuccesso , infatti solo il 30% dei pazienti che presenta un miglioramento dei sintomi ( modified rankin scale , mrs2 )  . 
la trombolisi farmacologica condotta per via intrarteriosa e successivamente lintroduzione di dispositivi per la trombolisi meccanica hanno consentito di estendere la finestra temporale terapeutica ed ottenere un trattamento efficace con ridotto tasso di complicanze [ 2 ]  . in particolare il sistema penumbra un dispositivo costituito da un sistema microguida / catetere associato ad una pompa di aspirazione che consente , mantenendo il catetere prossimalmente alla sede dellostruzione vasale , di rimuovere il tessuto trombotico formatosi allinterno dellarteria minimizzando il rischio di dissezioni , fissurazioni vasali ed embolie distali [ 3 ]  . 
 [ 4 ] riportano in letteratura un successo procedurale del 100% per ictus ischemico secondario ad occlusione di grossi vasi con un significativo miglioramento clinico nel 45% dei pazienti trattati . 
altri lavori riportano analoghi risultati nel trattamento dellictus ischemico sia con trombolisi meccanica isolata [ 5 , 6 ] che in associazione alla somministrazione intraprocedurale di fibrinolitici [ 7 ]  . in questo lavoro presentiamo la nostra esperienza con il device penumbra al fine di valutare la potenziale efficacia , radiol med ( 2012 ) 117 : 11991214 materials and methods this study was retrospective and nonrandomised . 
 table 2 summarises the cardiovascular risk factors evalutable 1 study participation criteria criteria inclusion clinical signs compatible with acute cerebral stroke symptom onset within 8 h thrombosis with flow interruption in a main cerebral vessel severe neurological symptoms with an nihss score8 patients who were not candidates not responding to thrombolytic therapy with intravenous rtpa , with symptom onset within 3 h exclusion cerebral vessels that were too tortuous to be approached with this type of device ( partial ) patients with severe uncontrolled arterial hypertension ( systolic arterial pressure > 185 mmhg , or diastolic arterial pressure > 110 mmhg ) intracranial haemorrhage pregnancy nihss , national institutes of health stroke scale ; mrs , modified rankin scale ; rtpa , recombinant tissue plasminogen activator tabella 1 criteri di inclusione ed esclusione criteri inclusione segni clinici compatibili con un quadro di ictus cerebri acuto insorgenza della sintomatologia inferiore alle 8 ore trombosi con interruzione di flusso in un vaso cerebrale principale sintomatologia neurologica severa con uno nhiss8 pazienti non candidati o con mancata risposta alla terapia trombolitica endovenosa con rtpa , con insorgenza dei sintomi entro le 3 ore esclusione vasi cerebrali eccessivamente tortuosi per risultare approcciabili con questa tipologia di device ( parziale ) pazienti con ipertensione arteriosa grave non controllata : pas > 185 mm hg , o pad > 110 mm hg emorragia intracranica donne in stato di gravidanza nihss , national institutes of health stroke scale ; pas , pressione arteriosa sistolica ; pad , pressione arteriosa diastolica ; rtpa , attivatore del plasminogeno tissutale ricombinante sicurezza ed i vantaggi clinici del trattamento di rivascolarizzazione endovascolare di occlusioni vascolari cerebrali in pazienti affetti da ictus cerebri acuto . 
la tabella 2 riassume i fattori di rischio per malattia cardiovascolare valutati pre - operatoriamente , la sede di occlusione arteriosa causa dello stroke e le condizioni neurologiche pre - procedurali valutate mediante la national health institute stroke scale ( nhiss ) e mrs . 
 tutti i pazienti sono stati valutati pre - proceduralmente previo esame neurologico , con valutazione dellnhiss e mrs , e sottoposti ad esame in tomografia computerizzata ( tc ) del cranio senza somministrazione di mezzo di contrasto al fine di escludere la natura emorragica . 
quattordici pazienti sono stati sottoposti ad approfondimento diagnostico mediante uno studio di risonanza magnetica ( rm ) preprocedurale con sequenze pesate in diffusione [ echo - planar imaging ( epi ) - spin - echo ( se ) tempo di eco ( te ) , 55 ms , tempo di ripetizione ( tr ) 2079 ms , flip angle 90 , durata 30 secondi ] , fluid attenuated inversion recovery ( flair ) [ te 125 ms , tr 11000 ms , tempo di inversione ( ti ) 2800 ms , durata 3 minuti e 40 secondi ] t1 - turbo spin echo ( tse ) ( te 10 ms , tr 2000 ms , durata 4 minuti ) angio - rm [ time of flight ( tof ) te 3 , 3 ms , tr 25 ms , durata 3 minuti ] e perfusione [ epifast field echo ( ffe ) , te 40 ms , tr 2460 ms , flip angle 90 , durata 1 minuto e 45 secondi ] , questultima condotta previa somministrazione a bolo di 30 ml di mezzo di contrasto gadobenato dimeglumina ( gd - dtpa ) ad un flusso di 4 ml / s , al fine di discernere le componenti tissutali necrotiche ovvero ischemiche attraverso lanalisi del mismatch diffusione ( dwi ) / perfusione ( pwi ) e la relativa delineazione dellarea di penombra ischemica , identificata come area di parenchima encefalico caratterizzata da normale diffusivit dellh2o tra compartimento intraed extracellulare ed anormali parametri perfusivi ematici . 
il mismatch diffusione / perfusione stato valutato sulla base delle aree di alterata diffusione e le mappe di transito medio [ ( mtt ) : mtt - dwi / dwi ] * 100 come precedentemente riportato da schaefer et al . 
 in un paziente non stato eseguito lo studio rm per la gravit del quadro clinico , perch portatore di un pacemaker cardiaco , mentre in 2 pazienti i sintomi erano insorti da 6 ore ed erano quindi al limite della finestra temporale per lesecuzione della trombolisi meccanica . 
 before the procedure all patients underwent neurological examination , with assessment of the nihss and mrs , and unenhanced cranial computed tomography ( ct ) in order to exclude haemorrhagic stroke . 
per laspirazione il catetere di riperfusione usato in parallelo con il separatore in un sistema coassiale connesso una pompa di aspirazione per separare e aspirare il trombo nel vaso occluso . procedura endovascolare tutti i pazienti arruolati sono stati trattati mediante un approccio retrogrado trans - femorale , mediante puntura dellarteria femorale comune e successivo posizionamento di un introduttore da 6 fr radifocus ( terumo , giappone )  . 
 sono state somministrate 5000 ui di eparina sodica intrarteriosa seguita da infusione in bolo al fine di mantenere un tempo di attivazione piastrinica ( act ) superiore ai 250 secondi . 
 tutte le procedure sono state eseguite da personale deradiol med ( 2012 ) 117 : 11991214 1203 a flow rate of 4 ml / s in order to distinguish necrotic and ischaemic tissue by analysing the diffusion ( dwi ) / perfusion ( pwi ) - weighted imaging mismatch and delineate the area of ischaemic penumbra , identified as an area of brain parenchyma with normal water diffusion between the intra and extracellular compartments and abnormal blood perfusion . 
in addition , in two patients , the symptoms began 6 h earlier , so the patients were at the limit of the time window for mechanical thrombolysis . patients were treated with mechanical thrombolysis using the penumbra system thrombus aspiration device . 
for aspiration , the reperfusion catheter is used in parallel with the separator in a coaxial system , which is connected to an aspiration pump to separate and aspirate the thrombus from the occluded vessel . endovascular procedure all patients enrolled were treated using a transfemoral retrograde approach , with puncture of the common femoral artery and placement of a 6 - f radifocus introducer sheath ( terumo , japan )  . 
 all procedures were performed by dedicated staff in an angiography room equipped with an allura xper fd20 / 10 digital subtraction angiography ( dsa ) system ( philips healthcare , best , the netherlands )  . 
selective cannulation of epiaortic vessels was achieved with a neuron delivery catheter ( penumbra inc . , alameda , ca , usa ) , which is extremely flexible and provides stable support for nontraumatic cannulation of epiaortic and intracranial vessels . 
the reperfusion catheter , suitably sized for the calibre of the obstructed artery , was then advanced on a transend 300 neurological microguidewire ( boston scientific , natick , usa ) until the tip was close to the occlusion site . 
once the correct position was reached , the microguidewire was advanced past the thrombus , followed by the reperfusion catheter , and contrast material was injected to confirm correct placement . 
 the reperfusion catheter was then retracted , the microguidewire replaced with the separator and the latter connected to the aspiration systethe thromboaspiration procedure was carried out in a similar manner to that described in previously published studies [ 3 ]  . the angiographic result was evaluated using the thromdicato in una sala angiografica equipaggiata con un angiografo digitale a sottrazione di immagini allura xper fd20 / 10 ( philips healthcare , best , paesi bassi )  . 
la cannulazione selettiva dei vasi epiaortici stata condotta con catetere portante neuron ( penumbra inc , alameda , ca , usa ) , estremamente flessibile e che consente un supporto stabile per una cannulazione atraumatica dei vasi epiaortici ed intracranici . 
si proceduto pertanto allavanzamento , su microguida neurologica transend 300 ( boston scientific natick usa ) , del catetere riperfusore del sistema penumbra ( penumbra inc , alameda , ca , usa ) , con dimensioni adeguate al calibro dellarteria sede di ostruzione , sino in prossimit del sito di occlusione . 
una volta raggiunta la corretta posizione , la guida stata avanzata ad oltrepassare il trombo seguita dal catetere riperfusore ed uniniezione di mezzo di contrasto stata eseguita per confermare il corretto posizionamento allinterno del vaso . 
 il risultato angiografico stato valutato mediante le scale di trombolisi nellictus cerebri ( tici ) [ 9 ] e di ricanalizzazione dellarteria primaria occlusa ( aol ) [ 9 ]  . 
 il successo tecnico procedurale stato definito come score di ricanalizzazione del vaso trattato e di riperfusione del parenchima cerebrale a valle dellocclusione rispettivamente di 23 ( aol ) e 23 ( tici )  . 
in alcuni pazienti che giungevano entro le 3 ore dallinsorgenza dei sintomi , una trombolisi venosa sistemica stata effettuata con attivatore tissutale del plasminogeno ricombinante ( rt - pa ) endovena alla dose di 0 , 9 mg / kg prima della procedura di trombolisi meccanica . 
stata definita una condizione di disabilit severa il riscontro di valori mrs2 . la tc cranio di controllo stata condotta entro le 24 h dalla procedura per delineare leventuale insorgenza di 1204 radiol med ( 2012 ) 117 : 11991214 bolysis in cerebral infarction ( tici ) [ 9 ] scale and the recanalisation of the primary arterial occlusive lesion ( aol ) [ 9 ] scale . 
technical success was defined as a score for recanalisation of the treated vessel and for reperfusion of the cerebral parenchyma downstream of the occlusion of 2 / 3 ( aol ) and 2 / 3 ( tici ) , respectively . 
in a few patients presenting at our centre within 3 h of symptom onset , systemic venous thrombolysis was carried out by giving 0.9 mg / kg recombinant tissue plasminogen activator ( rtpa ) intravenously before mechanical thrombolysis . 
an mrs score 2a was defined as severe disability . cranial ct was performed within 24 h after the procedure in order to identify the possible onset of subarachnoid and / or intraparenchymal haemorrhage of iatrogenic or postreperfusional origin in affecting the ischaemic cerebral regions . 
symptomatic intracranial haemorrhage was defined as a ct finding of intraor extra - axial blood collections associated with neurological deterioration ( nihss reduction > 4 ) or causing the patients death . statistical analysis continuous variables were expressed as meanstandard deviation ( sd ) and discrete variables as absolute and percentage values . 
in order to evaluate differences in the parameters considered for the two groups , students t test was used for continuous variables and the 2 test for discrete variables . results technical success was 83% . 
a total of 26 arteries were treated : four patients presented with a tandem obstruction of emorragie subaracnoidee e / o intra - parenchimali a genesi iatrogena o post - riperfusiva nei territori encefalici sede di ischemia . 
le emorragie intracraniche sintomatiche sono state definite come riscontro tc di raccolte ematiche intrao extrassiali associate ad un deterioramento del quadro neurologico ( riduzione del nhiss superiore a 4 ) o determinanti il decesso del paziente . 
per valutare le differenze dei parametri presi in considerazione fra i due gruppi di studio sono stati utilizzati il test t di student per le variabili continue e il test del 2 per le variabili discrete . risultati il successo tecnico procedurale stato dell83% . 
in 7 pazienti ( 39% ) giunti entro le 3 ore dallinsorgenza dai sintomi una trombolisi venosa sistemica stata eseguita con insuccesso ed stata necessaria una procedura di trombolisi meccanica di salvataggio . 
 quindici pazienti ( 83 , 3% ) presentavano un deficit neurologico pre - procedurale severo ( nhiss > 20 ) ; tuttavia nessuna differenza statisticamente significativa stata rilevata fra i pazienti con un valore nhiss pre - procedurale > 20 e 20 in termini di successo tecnico procedurale e regressione della sintomatologia neurologica ( nhiss4 ) a 3 mesi di follow - up . 
tutti i 14 pazienti , in cui stato possibile effettuare uno studio rm pre - procedurale , presentavano unarea di mismatch dwi / pwi > 20% ; tuttavia non stata rilevata alcuna correlazione di entit significativa tra la dimensione delle aree di alterata diffusione , anormale mtt e di mismatch ed i tassi di successo clinico e di regressione della sintomatologia neurologica . valutando i risultati della rivascolarizzazione angiografica la popolazione di studio stata suddivisa in sottogruppi in base alla classificazione tici e aol . 
in particolare considerando il tici score , 8 pazienti ( 44 , 4% ) hanno ottenuto una riperfusione completa del tessuto cerebrale ischemico ( tici = 3 ) , 7 ( 38 , 9% ) una riperfusione parziale ( tici = 2 ) e 3 ( 16 , 7% ) una riperfusione scarsa o assente ( tici = 1 )  . 
 fifteen patients ( 83% ) had a severe preprocedural neurological deficit ( nihss > 20 ) ; nonetheless no statistically significant difference was found between patients with preoperative nihss values > 20 and 20 in terms of technical success and neurological symptom regression ( nihss4 ) at the 3 - month follow - up . 
however , no significant correlation was found between the size of the areas showing altered diffusion , abnormal mtt and mismatch and rates of clinical success and regression of neurological symptoms . 
lunica differenza statisticamente significativa si riscontrata attraverso lanalisi dei valori pre - procedurali della proteina c - reattiva ( pcr ) dosata a 24 ore dalla procedura , che risultavano pi elevati nel gruppo di pazienti che presentavano una ricanalizzazione sub - ottimale . unulteriore analisi statistica dei gruppi sopra riportati stata condotta prendendo in considerazione le condizioni cliniche dei pazienti a 3 mesi , secondo le scale nhiss e mrs . 
i pazienti in cui si riusciti a determinare una rivascolarizzazione completa , con score tici e aol uguale a 3 hanno presentato un miglioramento clinico a 3 mesi di follow - up con una regressione della sintomatologia neurologica ( nhiss < 4 )  . 
in particolare nei pazienti che hanno ottenuto una ricanalizzazione completa ( aol = 3 ) tale dato raggiunge , posto a confronto con i restanti pazienti , una rilevanza statisticamente significativa ( p = 0 , 0024 )  . 
 la valutazione della disabilit conseguente allictus cerebri , analizzata attraverso la scala di rankin modificata , ha evidenziato una correlazione significativa tra pazienti 1206 radiol med ( 2012 ) 117 : 11991214 fig . 
1a - g angiographic examination of a 61 - yearold patient presenting with an occlusion of the internal carotid artery and the anterior cerebral circulation ( a , b ) treated with mechanical thrombectomy using a penumbra device ( c - f )  . 
1a - g esame angiografico di un paziente di 61 anni che evidenzia unocclusione dellarteria carotide interna e del circolo cerebrale anteriore ( a , b ) trattato mediante trombectomia meccanica con dispositivo penumbra ( c - f )  . 
2a - d angiographic examination of a 69 - year - old patient showing an occlusion in the left posterior cerebral circulation ( a ) treated with mechanical thrombectomy using a penumbra device ( b , c )  . 
2a - d esame angiografico di un paziente di 69 anni che evidenzia un occlusione dellarteria cerebrale posteriore sinistra ( a ) trattato mediante trombectomia meccanica con dispositivo penumbra ( b , c )  . 
controllo angiografico post - procedurale evidenziante una completa rivascolarizzazione ( aol = 3 ) ( d )  . ( tici = 3 ) , seven ( 38.9% ) partial reperfusion ( tici = 2 ) and three ( 16.7% ) limited or no reperfusion ( tici = 1 )  . 
patients who achieved complete revascularisation ( tici and aol scores = 3 ) showed clinical improvement at 3 months folin cui stata ottenuta una rivascolarizzazione completa e coloro che presentavano un ripristino ottimale dellautonomia ed indipendenza nello svolgimento delle attivit quotidiane ( mrs2 ) ( p = 0 , 05 )  . 
infatti 9 pazienti ( 50% ) con un valore aol = 3 a 3 mesi di follow - up erano in grado di eseguire le attivit quotidiane senza assistenza o con una minima disabilit ( mrs2 ) , mentre nessuno dei pazienti che presentavano una rivascolarizzazione sub - ottimale ha ottenuto un significativo miglioramento . 
indeed , nine patients ( 50% ) with an aol score = 3 at the 3 - month followup were able to attend to their own activities of daily living without help or with minimal disability ( mrs2 ) ; no patient with suboptimal revascularisation showed any significant infatti mentre nessun exitus stato rilevato con aol = 3 , alcuni decessi sono stati riscontrati in pazienti con una ricanalizzazione vasale sub - ottimale e generalmente nel primo mese post - procedurale . 
suboptimal reperfusion and recanalisation are significantly correlated with the appearance of clinical deterioration in the immediate postprocedural period ( p = 0.05 based on tici score and p = 0.0024 based on aol score , respectively )  . 
in fact , whereas no death occurred among aol = 3 patients , some deaths occurred among patients with suboptimal recanalisation , generally during the first month after the procedure . 
in particular , one patient ( 5.6% ) , treated 3 h after symptom onset , who achieved complete revascularisation ( tici = 3 , aol = 2 ) , died in intensive care due to multiple organ failriperfusione . 
le emorragie intraparenchimali , evidenziate al controllo tc a 24 ore dalla procedura , sono state classificate rispettivamente come emorragia infartuale tipo ii , con multiple aree petecchiali confluenti senza effetto - massa , ed ematoma parenchimale di tipo i , con una componente ematica occupante meno del 30% dellarea infartuale con minimo effetto massa . discussione attualmente lictus cerebri acuto pu essere trattato mediante diverse opzioni terapeutiche a disposizione del clini1210 radiol med ( 2012 ) 117 : 11991214 ure ; two patients ( 11.1% ) , treated respectively at 3 and 4 h after symptom onset and who had suboptimal recanalisation ( tici = 0 and 1 , aol = 0 and 2 , respectively ) , died 15 and 20 days , respectively , after the procedure , in both cases as a result of postreperfusion intraparenchymal haemorrhage . 
 cases of intraparenchymal haemorrhage detected at 24 - h ct scan were classified as type ii infarction haemorrhage , with multiple confluent petechiae without mass effect ; and type i parenchymal haematoma , with a haematic component occupying < 30% of the infarction area , with minimal mass effect . discussion acute cerebral stroke can be treated with a variety of therapeutic options : intravenously administered pharmacological thrombolysis can be successfully used within 3 h of the onset of symptoms related to distal cerebral vessel occlusion . 
 in the event of large - vessel occlusions , local pharmacological intra - arterial therapy and the more recent mechanical thrombolysis are used , as they can be performed within 8 h [ 2 ]  . 
as reported in the literature , intravenous thrombolysis with rtpa is only administered in 12% of patients with cerebral stroke [ 12 ] ; the main cause of inadequate administration is generally the delay with which the patient arrives at the emergency department . 
 published studies emphasise that the effectiveness of pharmacological treatment is also correlated with the site of vascular occlusion : the combined lysis of thrombus in brain ischemia using transcranial ultrasound and systemic t - pa ( clotbust ) study found that in only 50 ( 44% ) of 113 patients with occlusion of the distal segment of the middle cerebral artery and 49 ( 30% ) of 163 patients with occlusion in the proximal segment was intravenous thrombolysis with rtpa effective in recanalising the occluded vessel . 
results are significantly worse in patients with occlusion of the terminal segment of the internal carotid artery ( 6% ) or a tandem lesion of the internal carotid and middle cerebral arteries ( 27% ) or of the basilar artery ( 30% ) [ 13 ]  . 
in our experience , four patients had a tandem lesion of the internal carotid artery and middle and / or anterior cerebral artery ( 22.2% ) and two patients ( 11.1% ) an occlusion of the basilar artery . 
 although in one patient with a tandem occlusion of the internal carotid and middle cerebral arteries we were unable to achieve optimal revascularisation and the patient died , our co , come per esempio la terapia trombolitica farmacologica endovenosa che pu essere utilizzata con successo entro le 3 ore dallinsorgenza dei sintomi per occlusione di vasi cerebrali distali . 
in caso di occlusione di vasi di grosso calibro vengono utilizzate la terapia intrarteriosa farmacologica locale e la pi recente trombolisi meccanica che possono essere effettuate entro le 8 ore dallinsorgenza dei sintomi [ 2 ]  . 
 come riportato in letteratura , la terapia trombolitica endovenosa con rt - pa viene somministrata in solo l1%2% dei pazienti con ictus cerebri [ 12 ] ; la principale causa di mancata somministrazione generalmente il ritardo con cui il paziente giunge in pronto soccorso . 
nella maggior parte dei casi , inoltre , le strutture vascolari cerebrali occluse sono arterie di grosso calibro che presentano un basso tasso di rivascolarizzazione con questo tipo di terapia . i lavori presenti in letteratura sottolineano come lefficacia del trattamento farmacologico sia correlata anche alla sede dellocclusione vasale : nello studio clotbust solo in 50 ( 44% ) di 113 pazienti con occlusione del tratto distale dellarteria cerebrale media ed in 49 ( 30% ) dei 163 pazienti con occlusione del tratto prossimale della medesima arteria , la trombolisi endovenosa con rt - pa risultata efficace nella ricanalizzazione del vaso occluso . 
tali risultati risultano notevolmente inferiori nei pazienti che presentano unocclusione del tratto terminale dellarteria carotide interna ( 6% ) o con una lesione in tandem dellarteria carotide interna e dellarteria cerebrale media ( 27% ) o dellarteria basilare ( 30% ) [ 13 ]  . 
nella nostra esperienza 4 pazienti presentavano una lesione in tandem dellarteria carotide interna e dellarteria cerebrale media e / o anteriore ( 22 , 2% ) e 2 pazienti ( 11 , 1% ) unocclusione dellarteria basilare . 
sebbene in uno dei pazienti con occlusione in tandem dellarteria carotide interna e dellarteria cerebrale media non sia stato possibile ottenere una rivascolarizzazione ottimale con esito infausto , tuttavia non risulta tuttavia evidenziabile nei nostri risultati una correlazione statisticamente significativa fra la sede docclusione ed il successo della procedura ( p = non significativo )  . lo studio condotto dal national health institute of neurological disorders and stroke ha evidenziato che solo il 30% dei pazienti sottoposti a terapia trombolitica presentavano una minima o assente disabilit a 3 mesi di follow - up . 
 inoltre il 6 , 4% dei pazienti sottoposti a terapia sistemica , sviluppava una emorragia cerebrale intraparenchimale , principale complicanza nei pazienti sottoposti a questo tipo di terapia , rispetto allo 0 , 6% dei pazienti del gruppo placebo [ 14 ]  . 
 [ 15 ] ha evidenziato un tasso di ricanalizzazione del 75% nel trattamento di occlusione prossimale dellarteria cerebrale media con infusione endovenosa di rt - pa a dispetto tuttaradiol med ( 2012 ) 117 : 11991214 1211 results show no statistically significant correlation between occlusion site and the success of the procedure ( p = ns )  . the study conducted by the national institute of neurological disorders and stroke showed that only 30% of patients undergoing thrombolysis had minimal or no disability at 3 months . 
showed a 75% recanalisation rate following treatment of proximal middle cerebral artery occlusions using an intravenous infusion of rtpa [ 15 ] , despite a higher risk of postprocedural haemorrhage , due to the large amount of fibrinolytic drug required to lyse the thrombus . 
 low success rates coupled with a high incidence of complications , especially haemorrhage , have led to the exploration of new endovascular techniques for mechanical thrombolysis in order to obtain better results with fewer complications . 
devices have been designed for treating cerebral stroke that extend the time window for revascularisation through mechanical thrombectomy , allowing patients to be treated in emergency departments beyond 3 h of symptom onset . 
reported results show improved vascular recanalisation rates from 48% , obtained in the mechanical embolus removal in cerebral ischemia trial [ 16 ] , to 69% , obtained in the multi mechanical embolus removal in cerebral ischemia trial [ 17 ]  . 
this device , however , is associated with a high incidence of intraparenchymal haemorrhage ( 9% symptomatic and 29.7% asymptomatic ) , most likely due to the higher risk of vessel dissection and fissuring resulting from the retrieval - type mechanism of thrombus removal . 
i prolyse in acute cerebral thromboembolism trial ( proact ) i e ii hanno cercato di stabilire se linfusione loco regionale di pro - urochinasi a livello del sito di occlusione vasale presenti caratteristiche di sicurezza ed efficacia . 
 le basse percentuali di successo associate allelevata incidenza di complicanze prevalentemente di tipo emorragico hanno portato alla ricerca di nuove tecniche endovascolari di trombolisi meccanica al fine di ottenere un miglioramento dei risultati ed una riduzione delle complicanze . 
recentemente nel trattamento dellictus cerebri sono stati ideati dei dispositivi che consentono attraverso una trombectomia di tipo meccanico di ampliare la finestra temporale per la rivascolarizzazione , rendendo possibile il trattamento di pazienti giunti in pronto soccorso oltre le 3 ore dallesordio dei sintomi . 
questi dispositivi differiscono fra loro per la modalit con cui agiscono sul trombo , dividendosi in due grossi gruppi : ( 1 ) device prossimali , comprendenti i dispositivi tromboaspiranti ed i grasper , che effettuano la trombectomia senza attraversare la porzione di vaso occluso , dei quali i pi utilizzati sono il merci ( concentric medical inc mountain view , ca , usa ) ed il penumbra ( penumbra inc . , alameda , ca , usa ) ; ( 2 ) device distali , compredenti i dispositivi a cestello , a cappio e stent retraibili come il solitarie ( ev3 plymouth , usa )  . il merci retriever system stato il primo dispositivo nato a tale scopo . 
i risultati riportati in letteratura hanno evidenziato un miglioramento nel tasso di ricanalizzazione vasale tra il 48% , ottenuto nel trial mechanical embolus removal in cerebral ischemia [ 16 ] , al 69% del multi mechanical embolus removal in cerebral ischemia trial [ 17 ]  . 
questo dispositivo tuttavia presenta un incidenza elevata di emorragie intraparenchimali ( 9% sintomatiche e 29 , 7% asintomatiche ) , verosimilmente in relazione allincrementato rischio di dissezione e fissurazione vasali legati al meccanismo di trombo - rimozione di tipo retrieval . 
 di converso la filosofia del sistema penumbra quella di attraversare e frammentare il tessuto trombotico in maniera graduale esclusivamente con lutilizzo del separatore evitando di avanzare il catetere in una struttura vascolare anatomicamente non delineabile . 
la procedura deve essere eseguita su tratti del vaso occluso rettilinei , evitando di avanzare il separatore lungo le curve del vaso al fine di ridurre il rischio di perforazione e dissezione dello stesso . 
 il sistema di aspirazione , inoltre , riduce la possibilit di provocare embolie distali nelle ramificazioni vascolari ce1212 radiol med ( 2012 ) 117 : 11991214 conversely , the concept of the penumbra system is to cross and fragment the thrombotic tissue gradually using only the separator and without advancing the catheter into a vascular structure that cannot be outlined anatomically . 
the procedure should be carried out on straight segments of the occluded vessel , with care taken not to advance the separator along curved segments , thus reducing the risk of perforation or dissection . 
our technical success rate was 83 % , probably due to the inclusion of patients with primary atherosclerosis with subsequent formation of organised thrombus . we obtained a rate of complete revascularisation with aol and tici scores of 23 in 83% of cases ; only three patients ( 17% ) failed to achieve optimal recanalisation . 
improvement of the neurological picture was directly related to the degree of vessel reperfusion and recanalisation achieved , with nine patients ( 50% ) showing complete disappearance of the disability ( mrs2 ) and 11 ( 61.1% ) showing a significant reduction in neurological symptoms ( nihss4 )  . 
on other hand , 26% of patients developed postprocedural intraparenchymal haemorrhage related to reperfusion within 1 week of the procedure , two of them ( 11.1% ) with a fatal outcome . 
the penumbra pivotal stroke study reported an 82% rate of revascularisation to thrombolysis in myocardial infarction ( timi ) grades 23 , a 33% mortality rate and a 25% rate of functional recovery [ 3 ]  . 
in the single - centre study conducted by stuffert et al . , 12 patients ( 80% ) obtained complete recanalisation of the occluded vessel , with clinical symptoms improving in 42 % [ 7 ]  . 
these data are comparable with those obtained in a study of 29 patients by grunwald et al . , who report an 86% rate of recanalization to timi 23 and no disability in 38% of cases [ 5 ]  . 
 nel nostro centro abbiamo ottenuto una percentuale di rivascolarizzazione completa con aol score e tici score 23 pari all83% , solo in 3 pazienti ( 17% ) non stato possibile ottenere una ricanalizzazione ottimale . 
il miglioramento del quadro clinico neurologico risultato essere direttamente correlato con il grado di riperfusione e ricanalizzazione vasale al termine della procedura , con rispettivamente 9 pazienti ( 50% ) che presentavano completa risoluzione della disabilit ( mrs2 ) ed 11 pazienti ( 61 , 1% ) che mostravano una significativa riduzione della sintomatologia neurologica ( nhiss4 )  . 
il 26% dei pazienti ha sviluppato un emorragia intraparenchimale post - procedurale da riperfusione entro 1 settimana dalla procedura , di cui 2 ( 11 , 1% ) ad esito infausto . 
nel penumbra pivotal stroke study l82% dei pazienti al termine della procedura avevano un timi score 2 / 3 con una mortalit del 33% e una libert da disabilit del 25% [ 3 ]  . 
infatti nei pazienti in cui la rivascolarizzazione risultata essere subottimale , con valori di aol score inferiori a 2 , i valori medi di pcr risultavano essere di 111 , 5 mg / dl , di converso nei pazienti in cui la ricana lizzazione si rivelata ottimale i valore di pcr sono risultati pari a 10 , 2 mg / dl con una differenza statisticamente significativa ( p = 0 , 05 )  . 
 the correlation between postprocedural results and preprocedural crp levels allowed us to identify a subset of patients for whom treatment is less beneficial , most likely because of a prothrombotic inflammatory state promoting and stabilising the vascular occlusion . 
although larger studies and a serial preand postprocedural crp evaluation are needed , we postulate that this parameter can be used to identify patients requiring a more aggressive treatment . the innovation of interventional radiology techniques allows many patients to be treatment who , only a few years earlier , would have been destined to die or suffer permanent disability . 
the cooperation between stroke units and interventional radiology has made it possible to carry out mechanical recanalisation , thus extending the treatment time window to 8 h , with positive results . 
this technique is no longer considered an alternative to pharmacological therapies but the first choice in patients with acute ischaemia caused by major intracranial artery occlusion . relazione tra i risultati post - procedurali ed il dosaggio di questa molecola a 24 ore dalla procedura ci ha permesso di delineare una classe di pazienti nei quali risultano potenzialmente ridotti i benefici del trattamento , probabilmente in relazione ad uno stato infiammatorio pro - trombotico favorente e stabilizzante locclusione vasale . 
sebbene siano necessari studi pi ampi ed una valutazione della pcr pre e postprocedurale seriati , si pu ipotizzare che questo parametro possa essere utilizzato per individuare una classe di pazienti in cui sia necessario condurre un trattamento pi aggressivo . 
 linnovazione delle tecniche di radiologia interventistica permette di trattare pazienti che fino a pochi anni fa erano destinati ad andare incontro a morte o invalidit permanente in unelevata percentuale dei casi . 
the aim of this paper is to illustrate imaging features of patients affected by congenital aural atresia ( caa ) before and after treatment with a vibrant soundbridge ( vsb ) device implanted on the round window . 
ten patients ( 5 males and 5 females ; mean age 22.1 years ) with caa underwent preoperative high - resolution computed tomography ( hrct ) to estimate the degree of involvement of the middleand inner - ear structures and highlight radiological landmarks useful for surgical planning . 
hrct provides accurate information about anatomy and malformations of the middle and inner ear and can thus assist the surgeon in planning the procedure . keywords ear congenital abnormalities spiral computed tomography prostheses and implants riassunto obiettivo . 
la finestra rotonda era nei limiti in tutti i soggetti , mentre in 6 orecchi ( 35 , 3% ) erano presenti anomalie di decorso e / o di calibro del nervo faciale . 
la tc ad alta risoluzione fornisce le corrette informazioni circa lanatomia e le malformazioni dellorecchio medio ed interno , utili per il chirurgo per la programmazione operatoria . parole chiave orecchio anomalie congenite tomografia computerizzata spirale protesi e impianti radiol med ( 2012 ) 117 : 488499 introduction introduzione congenital aural atresia ( caa ) is a birth defect characterized by conductive hearing loss due to the presence of varying degrees of external auditory canal ( eac ) deformity . 
 on assessing the patient for surgical repair , it is crucial to know whether the malformation involves the eac and auricle only or whether there is diffuse involvement of the temporal bone and , especially , of inner ear structures [ 1 , 2 ]  . 
 because the pathogenic insult may occur at different stages of embryological development , not all atretic ears are the same [ 3 ]  . the presence of an associated sensorineural hearing loss due to coexisting inner ear abnormalities constitutes a contraindication to conventional surgery [ 4 ]  . 
in view of the high rate of complications [ 57 ] and the need for surgical revision in approximately one third of cases of reconstructive surgery [ 810 ] there was a need for an alternative treatment , specifically designed for children , to prevent impairment of normal cognitive and verbal development . with the innovative surgical implantation of a vibrant soundbridge ( vsb , med - el , innsbruck , austria ) floating mass transducer ( fmt ) on the round window , the malformed eac and the damaged ossicular chain are bypassed , and the implant delivers its energy directly onto the cochlea [ 11 , 12 ]  . 
the excellent clinical results of this approach indicate that it may represent a viable alternative to conventional surgery [ 13 , 14 ]  . caa diagnosis and proper pre - operative assessment rely on clinical and functional examinations ( history , clinical examination , audiogram , electrophysiological tests ) and radiological investigations , such as computed tomography ( ct ) and magnetic resonance ( mr ) imaging . 
ct scan of the temporal bone is crucial to establish the indication for surgical intervention in that it provides information regarding external - , middleand inner - ear anatomy and reveals the type of bone dysplasia and associated pathologies , if present [ 2 ]  . 
post - operative radiological investigations are mandatory both within hours after surgery to exclude early complications , and at different intervals to highlight any implant malposition / displacement . the aims of this study was to identify anatomical landmarks and middle ear structures to be visualized on ct to achieve proper pre - operative assessment of patients with caa who are eligible for vsb implantation on the round window . materials and methods we evaluated ct examinations of 10 patients affected by severe caa [ 5 males and 5 females ; age range 2 months latresia congenita aurale ( aca ) una condizione malformativa congenita caratterizzata da sordit trasmissiva per la presenza di diversi gradi di anomalia del condotto uditivo esterno ( cue )  . 
nel momento in cui il paziente viene valutato per una correzione chirurgica , fondamentale sapere se la malformazione coinvolge solo il cue ed il padiglione auricolare o se presente un diffuso interessamento dellosso temporale , in particolare delle strutture dellorecchio medio [ 1 , 2 ]  . 
infatti , poich linsulto patogeno pu colpire in differenti fasi dello sviluppo embriogenetico , non tutti gli orecchi atresici sono uguali [ 3 ]  . la presenza di unassociata ipoacusia neurosensoriale per una contemporanea anomalia delle strutture dellorecchio interno rappresenta una controindicazione allintervento chirurgico tradizionale [ 4 ]  . 
nel caso in cui lorecchio interno sia integro , sono stati proposti diversi approcci chirurgici , in particolare apparecchi acustici a conduzione ossea , apparecchi acustici ancorati allosso ed infine la plastica ricostruttiva . 
a causa dellalto tasso di complicanze [ 57 ] e alla necessit di revisione dellintervento in circa 1 / 3 dei casi di chirurgia ricostruttiva [ 810 ] si sentiva il bisogno di una alternativa , soprattutto indirizzata a pazienti pediatrici , al fine di impedire compromissioni del normale sviluppo cognitivo e verbale . con linnovativo intervento chirurgico di posizionamento della massa vibrante ( mv ) del vibrant soundbridge ( vsb , med - el , innsbruck , austria ) sulla finestra rotonda il cue malformato e la catena ossiculare danneggiata vengono superati e la protesi scarica la sua energia direttamente sulla coclea [ 11 , 12 ]  . 
gli ottimi risultati clinici di questo approccio lo indicano come vera alternativa alla chirurgia tradizionale [ 13 , 14 ]  . la diagnosi di aca ed il corretto inquadramento prechirurgico si basano su esami clinici e funzionali ( anamnesi , visita clinica , audiometria e test elettrofisiologici ) e su indagini radiologiche come la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm )  . 
lesecuzione della tc dellosso temporale cruciale per lindicazione allintervento chirurgico , fornendo informazioni circa lanatomia ossea dellorecchio esterno , medio ed interno per evidenziare il tipo di displasia ossea presente ed eventuali patologie associate [ 2 ]  . 
valutazioni radiologiche post - operatorie sono obbligatorie a poche ore dallintervento per escludere complicanze chirurgiche precoci e successivamente , a differenti intervalli , per evidenziare eventuali mal posizionamenti / dislocazioni della protesi . lo scopo del lavoro stato di identificare i punti di riferimento anatomici e le strutture dellorecchio medio da descrivere per ottenere il corretto inquadramento pre - operatorio dei pazienti con aca e candidati al posizionamento di vsb alla finestra rotonda . 490 radiol med ( 2012 ) 117 : 488499 to 50 years ; mean age 22.1 years ; standard deviation ( sd ) 5.1 years ] in whom a fmt was placed on the round window between may 2005 and may 2010 . 
all images were retrospectively reviewed by two radiologists with > 5 and 10 years of experience , respectively , in ear imaging , and compared with the intra - operative findings . 
pre - operatively , all patients underwent high - resolution ct ( hrct ) to allow visualization of the external - , middleand inner - ear anatomy and to determine the degree of dysplasia . 
scans were performed with the ct units available at our centre : a ct brilliance 64 ( philips , eindhoven , the netherlands ; 140 kv ; 150 ma ; slice thickness 0.67 mm ; spiral technique ; pitch 0.32 ; matrix 512512 ) and a ct brilliance 6 ( 120 kv ; 150 ma ; slice thickness 0.8 mm ; spiral technique ; pitch 0.4 ; matrix 256256 )  . 
in addition , on the same day , the patients had undergone a brain mr scan completed with a study of the ponto - cerebellar angle to exclude malformations or disorders of inner ear structures or central auditory pathways . 
then , maximum intensity projection ( mip ) reconstructions were obtained to gain an overall view of the anterior and posterior labyrinth , and parasagittal multiplanar reconstructions ( mpr ) to visualize nerve structures of the inner ear canal . 
post - operatively , all patients underwent radiological assessment to exclude early complications and incorrect placement of the fmt ( ct protocol within 8 hours ) using ct scan of the skull and petrous bones . 
patients were then followed up from 12 to 60 months after surgery . all patients were implanted with a vsb on the round window : this is made up of an external portion consisting of an audio processor with microphone and receivertransmitter , and an internal portion consisting of the receiver connected via a wire to the fmt , a 21.5 - mm titanium - coated magnetic coil weighing 25 mg that vibrates when current runs through it . 
the patients were evaluated and classified according to the following variables : affected side , atresia type , ossicular - chain involvement , facial nerve course , oval and round window patency , mastoid pneumatization and aeration and the presence of vascular abnormalities ( table 1 )  . materiali e metodi sono state valutate le indagini tc espletate in 10 pazienti affetti da severa aca ( 5 maschi e 5 femmine , et compresa fra 2 mesi e 50 anni : media 22 , 1 anni , deviazione standard : 5 , 1 anni ) ed operati con posizionamento di mv alla finestra rotonda nel periodo compreso fra maggio 2005 e maggio 2010 . 
 in sede pre - operatoria tutti i dieci pazienti hanno eseguito lesame tc ad alta risoluzione per ottenere i dettagli anatomici dellorecchio esterno , medio ed interno e delineare il grado di displasia . 
le scansioni sono state espletate mediante le apparecchiature tc a disposizione presso il nostro istituto : tc brilliance 64 ( philips , eindhoven , olanda ; 140 kv , 150 ma , spessore dello strato 0 , 67 mm , tecnica spirale , pitch 0 , 32 , matrice 512512 ) e tc brilliance 6 ( 120 kv , 150 ma , spessore dello strato 0 , 8 mm , tecnica spirale , pitch 0 , 4 , matrice 256256 )  . 
nella stessa seduta giornaliera i dieci pazienti avevano eseguito inoltre la rm encefalo completato con studio dellangolo ponto - cerebellare per escludere malformazioni o patologie delle strutture dellorecchio interno o delle vie acustiche centrali . 
lesame rm stato eseguito mediante apparecchiatura symphony maestro da 1 , 5 t ( siemens , enlargen , germania ) con scansioni anatomi che spin echo ( se ) e turbo spin echo ( tse ) t1 e t2 - dipendenti e completato con immagini assiali constructive interference in steady state ( ciss ; 28 strati , tempo di ripetizio ne [ tr ] : 17 , 3 , tempo di eco [ te ] : 6 , 9 , spessore 0 , 65 , flip angle 70 , matrice 358512 * ( interpolazione ) , nex 2 , campo di vista [ fov ] 100100 )  . 
sono state successivamente ottenute ricostruzioni in proiezione di massima intensit ( mip ) per avere una visione globale del labirinto anteriore e posteriore e ricostruzioni multiplanari ( mpr ) para - sagittali per visualizzare le strutture nervose nel condotto uditivo interno . 
in 15 / 17 ears ( 88% ) , atresia was of the mixed type , whereas in only 2 ( 12% ) it was of the isolated membranous type . 
stapes was not recognizable in 3 / 17 ears ( 17.6% ) , a finding confirmed at surgery , whereas a poorly developed stapes was seen in 8 / 17 ears ( 47% )  . 
the mastoid appeared well pneumatized in 8 / 17 ears ( 47% ) but poorly aerated in 2 / 8 ( 25% ) , as it was occupied by hypodense inflammatory tissue . 
none of the patients had any alteration in eustachian - tube dimensions or any innerear abnormalities . post - operative findings no patient showed evidence of early post - operative complications , in particular , intracranial haemorrhage , at ct performed within 8 hours after the procedure . 
in all patients ( 100% ) , scans focusing on the temporal bone showed small gas bubbles and a moderate quantity of slightly hyperdense tissue , referable to reactive inflammatory tissue mixed with blood , occupying the site of surgery . 
la staffa non era riconoscibile in 3 / 17 orecchi ( 17 , 6% ) , quadro confermato in sede di intervento , mentre un abbozzo stapediale era riconoscibile in 8 / 17 orecchi ( 47% )  . 
la mastoide ap pariva ben pneumatizzata in 8 orecchi / 17 ( 47% ) , tutta via in 2 / 8 ( 25% ) risultava scarsamente areata poich occupata da tessuto ipodenso flogistico per fenomeni suppurativi sovrapposti . 
a - c axial and coronal highresolution computed tomography scans show membranous atresia ( triangle ) and fusion and dysplasia of the malleus ( thick arrow ) and incus ( thin arrow ) on both sides ; the stapes is present ( arrowhead ) , and the mastoid is well pneumatized ( star )  . 
a - c le immagini tc ad alta risoluzione nei piani assiali e coronali dimostrano la presenza di unatresia di tipo membranoso ( triangolo ) e la fusione e displasia del martello ( freccia spessa ) e dellincudine ( freccia sottile ) , ad ambo i lati ; la staffa presente ( testa di freccia ) e la mastoide ben pneumatizzata ed aerata ( stella )  . 
ct represents the examination of choice for its intrinsic high - contrast resolution , which well depicts environments such as the external and middle ear , which mostly consist of air and bone [ 18 ]  . 
ct can help to diagnose suspected congenital malformations as well as other causes of conductive hearing loss , such as tympanosclerosis and otosclerosis [ 19 ] , and therefore it is a necessary step in pre - operative planning [ 20 ]  . standard radiography of the skull with dedicated otological projections and conventional tomographic studies are not indicated or even useless in the diagnostic assessment of patients with caa . 
compared with ct , mr imaging is unable to provide a detailed representation of externaland reperti post - operatori nessun paziente ha mostrato la presenza di complicanze precoci post - operatorie , in particolare emorragie intracraniche , mediante tc entro 8 ore come da protocollo . 
in tutti i soggetti ( 100% ) , nelle scansioni focalizzate sullosso temporale , stato possibile riconoscere piccole bolle di gas ed una modesta quantit di tessuto leggermente iperdenso , riconducibile a materiale flogistico reattivo misto a sangue , ad occupare la sede dellintervento . 
la tc rappresenta lindagine di scelta in corso di aca per lintrinseca elevata risoluzione ad alto contrasto che esalta ambienti come lorecchio esterno e medio composti per lo pi da aria ed osso [ 18 ] : in questo modo la tc riesce ad evidenziare eventuali malformazioni congenite sospette , includendo anche altre cause di ipoacusia trasmissiva come timpanosclerosi e otosclerosi [ 19 ] , rappresentando uno step obbligatorio nel planning pre - chirurgico dellaca [ 20 ]  . le radiografie standard del cranio , nelle proiezioni dedicate per lo studio otologico e gli studi tomografici convenzionali non presentano indicazioni allespletamento n risultano utili ai fini diagnostici in pazienti con aca . 
la rm , paragonata alla tc , non in grado di dimostrare nel dettaglio le malformazioni dellorecchio esterno e medio [ 19 ] , ma riveste un ruolo fondamentale nelliter radiologico pre - chirurgico perch lunica indagine di imaging in grado di studiare nel dettaglio le strutture dellorecchio interno , il nervo cocleare e le vie acustiche centrali [ 2123 ] , la cui integrit condizione necessaria per la candidatura allimpianto vsb . una cassa timpanica poco sviluppata ed un antro mastoideo ipoplasico associati ad aca possono rendere difficoltoso lapproccio chirurgico alla finestra rotonda . 
a , b la tc ad alta risoluzione sul piano assiale mostra una massa incudo - malleolare fusa e dismorfica ( freccia spessa ) allinterno di una cavit timpanica piccola e ripiena di liquido . 
c , d nelle sezioni coronali il conglomerato ossiculare fissato al piatto atresico ( testa di freccia ) ; la mastoide non areata ( stella ) e la finestra rotonda pervia ( freccia sottile )  . middle - ear malformations [ 19 ] , but it has a fundamental role in pre - operative imaging , being the only modality capable of providing a detailed study of the inner ear , cochlear nerve and central auditory pathways [ 2123 ] , the integrity of which structures is a prerequisite for considering the patient as a candidate for prosthetic implantation . a poorly developed tympanic cavity and a hypoplastic mastoid antrum associated with caa may render surgical access to the round window difficult . 
abnormalities of the ossicular chain are frequently associated with caa and include partial or total agenesis , deformity , ectopia , malrotations and ossicular fusion [ 2 , 16 , 19 ]  . 
in our study , the most frequent findings were the presence of a rudimentary malleus and incus that were fused to each other . window abnormalities have been reported to occur in association with caa and mainly consist of agenesis , stenosis and otosclerosis [ 16 , 26 ]  . 
in our study , all patients had a normal round window with caliber > 2 mm ; abnormalities of the oval window do not , however , constitute a contraindication for the surgical procedure . 
 abnormalities of the facial - nerve course are commonly found in association with externaland middle - ear congenipneumatizzazione e le dimensioni dellorecchio medio e della mastoide sono inversamente proporzionali allo spessore del piatto atresico [ 16 ]  . 
anomalie a carico della catena ossiculare frequentemente si associano ad aca , comprendendo agenesie parziali o totali , deformit , ectopie , malrotazioni e fusioni ossiculari [ 2 , 16 , 19 ] : nel nostro studio i reperti pi frequenti sono stati la presenza di un martello e di unincudine rudimentali e fusi fra loro . lassociazione di anomalie fenestrali e aca sono riportate in letteratura e consistono principalmente in agenesia , stenosi e otosclerosi [ 16 , 26 ] : nel nostro studio tutti i pazienti presentavano una finestra rotonda regolare , con calibro superiore a 2 mm , mentre anomalie a carico della finestra ovale non rappresentavano una controindicazione . 
la condizione pi frequente la deiscenza del tratto timpanico che potrebbe rendere difficoltoso laccesso alla finestra rotonda ; sono descritte inoltre anomalie di decorso e stenosi / ipoplasia del canale osseo per il nervo faciale [ 16 ] , radiol med ( 2012 ) 117 : 488499 fig . 
a , b axial and coronal high - resolution computed tomography scans show the ossicular chain ( thick arrow ) fused with the atretic plate ( circle ) in a large and well - pneumatized tympanic cavity ( star ) and a diverticulum of the internal jugular vein ( curved arrow )  . 
a , b la tc ad alta risoluzione nel piano assiale e coronale dimostra la fusione della catena ossiculare ( freccia spessa ) con il piatto atresico ( cerchio ) nel contesto di una cavit timpanica ampia e ben pneumatizzata ( stella ) e il diverticolo della vena giugulare interna ( freccia curva )  . 
 the most frequent of these abnormalities is tympanic segment dehiscence , which might obstruct access to the round window ; additional abnormalities concern facial - nerve canal course and stenosis / hypoplasia [ 16 ] , a situation present in only one of our patients . 
one jugular diverticulum was seen in our study that , together with other vascular abnormalities , constitutes a rare but potential risk of intra - operquestultima evenienza era presente in un singolo soggetto . 
 un diverticolo giugulare stato evidenziato nel nostro studio , che insieme ad altre anomalie vascolari , rappresenta un raro ma potenziale rischio intra - operatorio di emorragia [ 2 , 16 ]  . 
non sono state evidenziate alterazioni a carico della tuba di eustachio nei pazienti con aca del nostro studio , tuttavia sono segnalate patologiche dilatazioni del suo tratto osseo [ 16 ]  . 
b - d in the coronal plane , the opacified tympanic cavity appears small , and the incus is in contact with the atretic plate ( star ) ; bony closure of the oval window is evident ( thin arrow ) , whereas the round window has a normal shape ( arrowhead )  . 
a la tc ad alta risoluzione sul piano assiale mostra un ben definito spazio articolare fra la testa del martello ed il corpo dellincudine ( articolazione normale ; freccia spessa )  . 
b - d nelle sezioni coronali la cavit timpanica opacata piccola e lincudine in contatto con il piatto atresico ( stella ) ; una chiusura ossea a livello della finestra ovale riconoscibile ( freccia sottile ) , mentre la finestra rotonda normo - conformata ( testa di freccia )  . 
caa may be associated with syndromic disorders involving cranio - facial malformations due to embryological damage to structures deriving from the first two branchial arches [ 27 , 28 ] , but no such cases were identified in our study . 
 after vsb device placement , mr imaging is contraindicated , even though some studies regarding the safety of high - field - strength mr imaging and hearing implants have been published in the literature [ 29 ]  . 
ct is therefore the only imaging technique capable of verifying the accurate position of the fmt on the round window , given that conventional radiography has already been shown inadequate for this purpose [ 30 ]  . 
relatively recently , cone - beam ct ( cbct ) has been proposed as an alternative to hrct for studying the temporal bone in cases of conductive hearing loss and for the follow - up of patients with cochlear implant condotto uditivo interno nei soggetto selezionati in questo tipo di intervento , eventualmente rilevabili con la rm [ 4 , 21 ]  . 
la aca pu associarsi a quadri sindromici di malformazioni cranio - facciali per danno embriologico delle strutture derivanti dai primi due archi branchiali [ 27 , 28 ] che tuttavia nel nostro studio non sono stati riscontrati . 
 successivamente al posizionamento della vsb lesecuzione della rm risulta controindicata , nonostante alcuni studi riguardanti la sicurezza rm ad alto campo e gli impianti acustici siano presenti in letteratura [ 29 ]  . 
la tc pertanto la tecnica a disposizione del radiologo per verificare lesatta collocazione della mv nella finestra rotonda essendo la radiografia convenzionale gi stata dimostrata inadeguata per questo scopo [ 30 ]  . 
in tempi relativamente recenti la cone beam computed tomography ( cbct ) stata proposta in letteratura come indagine alternativa alla tc ad alta risoluzione nello studio dellosso temporale in casi di ipoacusia trasmissiva e nel follow - up di pazienti con impianto cocleare o vsb alla finestra rotonda [ 3032 ]  . 
b , c axial highresolution computed tomography scans show the dysmorphic and fused malleo - incudal joint ( arrowhead ) ; the right middle ear is opacified due to the presence of acute otitis media ( asterisk ) , whereas the affected ear has a small tympanic cavity . 
b , c la tc ad alta risoluzione nei piani assiali evidenzia la dismorfica e fusa articolazione incudo - malleolare ( testa di freccia ) ; lorecchio medio di destra opacato per la presenza di unotite media acuta ( asterisco ) , mentre il lato atresico presenta una cassa timpanica piccola . 
la tc ad alta risoluzione nei piani coronale , assiale e nelle ricostruzioni mip dimostra la corretta posizione della massa vibrante nella finestra rotonda ( freccia spessa )  . 498 radiol med ( 2012 ) 117 : 488499 or vsb at the round window [ 3032 ]  . 
this technique has in common with ct the delivery of ionising radiation , good high - contrast resolution and the possibility of obtaining multiplanar and volumetric reconstructions ; cbct offers some advantages over standard ct , such as low costs , limited size and low radiation dose , but also some disadvantages , including small field of view and lower image quality [ 33 , 34 ]  . 
 lemissione di radiazioni ionizzanti , lelevata risoluzione ad alto contrasto e la possibilit di ottenere ricostruzioni secondo piani multipli e volumetriche ; la cbct presenta alcuni vantaggi rispetto alla tc standard come i bassi costi , le dimensioni ridotte e la minor dose radiante emessa , ma anche alcuni svantaggi come il piccolo campo di vista e la minor qualit dellimmagine [ 33 , 34 ]  . 
gandini2 1istituto di radiologia , universit di torino , facolt san luigi gonzaga , regione gonzole 10 , 10043 orbassano , torino , italy 2istituto di radiologia diagnostica e interventistica , universit di torino , via genova 3 , 10126 torino , italy correspondence to : a . 
microwave thermal ablation ( mwa ) opens up a new scenario in the field of image - guided tumour ablation thanks to its potential advantages over validated radiofrequency ablation ( rfa )  . 
after obtaining informed consent , we enrolled 15 inoperable patients , for a total of 19 lesions ( ten metastases , nine hepatocellular carcinoma ) with a mean diameter of 47 mm ( range 1478 mm )  . 
mwa proved to be feasible and safe in treating advanced - stage liver tumours and represented an additional therapeutic attempt to be validated in further and larger efficacy studies . keywords microwave ablation hepatocellular carcinoma liver metastases interventional oncology riassunto obiettivo . 
la termoablazione con microonde ( mwa ) prospetta un nuovo scenario nel campo delle ablazioni tumorali imaging - guidate per i potenziali vantaggi rispetto allormai validata termoablazione con radiofrequenze ( rfa )  . 
previo consenso informato , abbiamo arruolato 15 pazienti non operabili , portatori di 19 lesioni ( 10 metastasi [ mts ] , 9 carcinomi epatici [ hcc ] ) con diametro medio di 47 mm ( range 1478 mm )  . 
lablazione completa ( ac ) , ottenuta nel 68 , 4% dei casi , non ha dimostrato correlazioni statisticamente significativa n con listotipo , n con il diametro delle lesioni . 
la mwa stata fattibile e sicura nel trattamento di neoplasie epatiche avanzate , e ha costituito un tentativo terapeutico oltre i protocolli oncologici standard da sottoporre al vaglio di pi ampi studi di efficacia . parole chiave ablazione con microonde carcinoma epatocellulare metastasi epatiche oncologia interventistica radiol med ( 2012 ) 117 : 378392 introduction introduzione primary and secondary hepatic tumours are the third cause of death by cancer worldwide [ 1 ]  . 
for example , in cases of metastases ( mts ) from colorectal cancer , in the absence of extrahepatic disease , surgical resection remains the most radical treatment , with reported 5 - year survival rates ranging from 15% to 50% and a disease - free interval at 5 years of approximately 19% [ 2 ]  . 
almost 7580% of lesions are nonresectable at diagnosis owing to lesion number , size and site , limited hepatic functional reserve , presence of extrahepatic disease and / or of comorbidities . 
of all these techniques , radiofrequency ablation ( rfa ) is the most widely used in clinical practice and is considered as the treatment of choice for nonresectable hepatic lesions 3 cm [ 3 , 4 ]  . 
 microwave ablation ( mwa ) , initially used experimentally in japan at the end of the 1980s to achieve intraoperative haemostasis during hepatectomy [ 5 ] , has undergone considerable technological developments and has emerged as a new treatment option in the field of oncology [ 6 , 7 ]  . 
when applied to tissue , mw produce dielectric hysteresis or polarisation whereby the polar molecules ( mainly water molecules ) present in the tissue start to oscillate and rotate extremely rapidly in an attempt to realign with the variations in charge produced within the electromagnetic field ( emf )  . 
the frequencies used by the devices employed in europe are 915 mhz and 2.45 ghz and within a few seconds produce intratumoural temperatures ranging from 60c to 140c , causing cellular death by coagulation necrosis . 
the extent of necrotic area depends on the energy delivered and the dielectric conductivity and permittivity of the tissue irradiated , on the type of antenna and on the timetemperature profile ( which depends on power and time of application )  . 
the studies reported in the literature are mainly retrospective series of consecutive treatments carried out with nonstandard technique , and none has provided conclusive evidence as to the therapeutic role of mw in oncology [ 8 , 9 ]  . 
le opzioni terapeutiche pi comuni sono rappresentate dalla chirurgia ( resezione e trapianto epatico ) e dalle terapie loco - regionali ( ablazione tumorale ed embolizzazione / chemioembolizzazione )  . 
ad esempio , per quanto riguarda le metastasi da neoplasia colo - rettale , in assenza di malattia extraepatica , la resezione chirurgica resta il trattamento con maggiori garanzie di radicalit , con percentuali di sopravvivenza a 5 anni riportate tra il 15% e il 50% , e una percentuale di sopravvivenza libera da malattia a 5 anni di circa il 19% [ 2 ]  . 
sfortunatamente , circa il 75%80% dei pazienti non operabile alla diagnosi per il numero , le dimensioni e la sede delle lesioni , la scarsa riserva funzionale epatica , la presenza di malattia extraepatica e / o di comorbilit . 
 tra queste , la termoablazione con radiofrequenze ( rfa ) la tecnica maggiormente impiegata nella pratica clinica ed attualmente considerata il trattamento di scelta per lesioni epatiche di dimensioni inferiori o uguali a 3 cm , non operabili [ 3 , 4 ]  . 
 lablazione con microonde ( mwa ) , inizialmente sperimentata alla fine degli anni ottanta in giappone con lo scopo di ottenere lemostasi intraoperatoria in corso di epatectomia [ 5 ] , ha subito notevoli sviluppi tecnologici ed emersa come nuova opzione terapeutica in campo oncologico [ 6 , 7 ]  . 
quando applicate ad un tessuto , le mw determinano listeresi dielettrica o polarizzazione per orientamento delle molecole polari presenti ( principalmente molecole dacqua ) che compiono rapidissimi movimenti di oscillazione e rotazione su se stesse nel tentativo di riallinearsi con le variazioni di carica indotte nel campo elettromagnetico ( cem )  . 
le frequenze attualmente impiegate dalle apparecchiature commercializzate in europa sono di 915 mhz e 2 , 45 ghz e producono in pochi secondi temperature intratumorali comprese tra 60c e 140c , determinanti la morte cellulare per necrosi coagulativa . 
lestensione dellarea di necrosi dipende , oltre che dallenergia somministrata , anche dalla conducibilit dielettrica e dalla permettivit del tessuto irradiato , dal tipo di antenna utilizzato e dal profilo tempo - temperatura ( condizionato dal tempo di applicazione e dalla potenza impiegata )  . 
 gli studi presenti in letteratura , per ora principalmente di tipo retrospettivo su serie consecutive di trattamenti condotti 380 radiol med ( 2012 ) 117 : 378392 cies ( rf ) : larger ablation diameters , shorter procedure time , higher intralesional temperatures , greater efficacy on lesions with a cystic component and / or in proximity to large vessels and the possibility of simultaneously using multiple antennae [ 10 ]  . the purpose of this study was to critically review our preliminary experience with mwa on a limited number of unresectable primary and secondary hepatic neoplasms and compare results with the literature . 
we also designed comparative study protocols between rfa and mwa to verify the abovementioned potential advantage of mwa . materials and methods patients and lesions we consecutively treated 15 patients with hepatocellular carcinoma ( hcc , n = 6 ) and metastases ( mts , n = 9 , tables 1 and 2 ) , with nine primary nodules and ten secondary lesions , respectively ( eight from colorectal , one from breast and one from lung cancer )  . 
 inclusion criteria were surgical unresectability ( owing to tumour size , insufficient liver function , comorbidity or patients refusal ) and / or failure of previous treatment , including rfa . 
indications , risks and potential benefits table 1 characteristics of patients with hepatocellular carcinoma ( hcc ) patient characteristics gender ( m / f ) age in years : mean ( range ) cirrhosis aetiology ( hcv / cryptogenic ) child - pugh ( a / b ) previous treatments ( yes / no ) treated nodules / patients ( single / multiple ) diameter ( mm ) of treated lesions : range ( meansd ) ; median tabella 1 caratteristiche dei pazienti con epatocarcinoma caratteristiche paziente con tecnica non standardizzata , non sono a oggi conclusivi circa il ruolo terapeutico delle mw in oncologia [ 8 , 9 ]  . 
ci nonostante , le mw sembrerebbero offrire alcuni potenziali vantaggi rispetto alle rf : maggiori diametri di ablazione , tempi procedurali pi rapidi , maggiori temperature intralesionali , maggior efficacia su lesioni con componente cistica e / o in prossimit di grossi vasi , possibilit di utilizzare contemporaneamente multiple antenne [ 10 ]  . lo scopo di questo studio una valutazione critica della nostra esperienza preliminare di mwa di un numero limitato di neoplasie epatiche primitive e secondarie non candidabili alla chirurgia , anche mediante un confronto con la letteratura ; il fine quello di disegnare protocolli di studio comparativi tra rfa e mwa per accertare i suddetti potenziali vantaggi di questultima . materiali e metodi pazienti e lesioni presso il nostro istituto sono stati trattati consecutivamente 15 pazienti con carcinoma epatico ( hcc , 6 ) e metastasi ( mts , 9 ) ( tabella 1 e 2 ) , portatori rispettivamente di 9 noduli neoplastici primitivi e 10 lesioni secondarie ( 8 da neoplasie colo - rettali , 1 mammaria e 1 polmonare )  . 
the first threshold provided a more even distribution of lesions into two groups ( ten 4.5 cm and nine > 4.5 cm ) , whereas the second represents the true limit of the current ablation techniques . technique in our preliminary experience with mwa , we had the opportunity to use both devices available in our country , namely : evident microwave ablation system , covidien ltd ( boulder , co , usa ) , consisting of a generator producing a maximum power level of 60 w at a 915 - mhz frequency and equipped with teflon - coated 14.5 - g antennae ( with radiating section of 3.7 cm and constantly perfused by saline solution at room temperature , at a speed of 60 ml / min ) ; hs amica gen , hs hospital service s.p.a. 
 ( rome , italy ) , consisting of a generator producing a continuous power level of 140 w at 2450 mhz , connected to a 14 - g teflon - coated disposable interstitial applicator ( cooled by saline solution delivered by an automatic pump )  . sono stati la non resecabilit chirurgica ( per estensione del tumore , insufficiente funzione epatica , comorbilit o espresso rifiuto del paziente ) e / o linsuccesso di pregresse terapie , inclusa la rfa . 
la prima soglia distribuiva pi omogeneamente le nostre lesioni in due gruppi ( 10 inferiori / uguali a 4 , 5 cm e 9 superiori a 4 , 5 cm ) , mentre la seconda rappresenta il vero limite delle attuali tecniche ablative . tecnica nella nostra esperienza preliminare di mwa abbiamo potuto utilizzare entrambe le apparecchiature disponibili in commercio nel nostro paese , ossia : evidenttm microwave ablation system , covidien ltd ( boulder , colorado , usa ) , costituita da un generatore in grado di produrre una potenza massima di 60 w a una frequenza di 915 mhz , e da antenne in teflon del calibro di 14 , 5 g ( con sezione radiante di 3 , 7 cm e perfuse in continuo con soluzione fisiologica a temperatura ambiente a una velocit di 60 ml / min ) ; 382 radiol med ( 2012 ) 117 : 378392 fig . 
1 numero di lesioni in relazione ai diametri soglia ( 4 , 5 e 5 cm )  . the two devices were used on 11 ( four hcc and seven mts ) and four ( two hcc and two mts ) patients , respectively . all patients had been restaged during the month prior to mwa with multiphase computed tomography ( ct ) scans ( five with hcc ; five with mts from colorectal carcinoma ) or magnetic resonance imaging ( mri ) ( one patient with hcc ) , or positron emission tomography ( pet ) - ct ( two with mts from colorectal ; one from breast ; one from lung carcinoma )  . 
before each procedure , the liver was studied by ultrasonography ( us ) ( esaote mylab 70 , broadband convex - array probe with frequencies ranging from 3.5 to 8 mhz ) , with intercostal and subcostal scans , to verify lesion size and number and anatomical relationships with structures prone to iatrogenic thermal damage . after monitoring the patients vital parameters , treatment was performed with the patient under analgesia / sedation using the same standardised protocol adopted by our institute for rfa ; the antenna was implanted after skin disinfection and local anaesthesia with 10 ml of lidocaine hydrochloride at 2% , and the skin was incised with a no . 
lesions with maximum diameter < 3 cm ( 2 / 19 ) were treated with a single antenna ( two hcc : one with covidien ; one with hs ) , whereas those with a diameter > 3 cm ( 17 / 19 ) were treated with either multiple simultaneous antennae ( possible with the covidien device only : five hcc , eight mts ) or multiple insertions of a single antenna ( four hs : two hcc ; two mts ) to obtain a sufficient area of necrosis . 
at the end of the ablation procedure , us scans were obtained to exclude immediate complications ; patients were then monitored for 24 h at the department in which they were hospitalised . hs amica gen , hs hospital service spa ( roma , italia ) , con un generatore in grado di erogare una potenza di 140 w in onda continua a 2450 mhz , collegato a un applicatore interstiziale monouso in teflon di 14 g ( raffreddato con soluzione fisiologica da una pompa a controllo automatico )  . le due apparecchiature sopra descritte sono state utilizzate rispettivamente in 11 ( 4 hcc e 7 mts ) e 4 ( 2 hcc e 2 mts ) pazienti . tutti i pazienti erano stati ristadiati entro il mese precedente la mwa con studi multifasici in tomografia computerizzata ( tc ) ( 10 pazienti : 5 con hcc , 5 con mts da carcinoma colo - rettale ) o risonanza magnetica ( rm ) ( 1 paziente con hcc ) , o tomografia ad emissione di positroni ( pet ) - tc ( 4 pazienti : 2 con mts da carcinoma colo - rettale , 1 da carcinoma mammario , 1 polmonare )  . 
prima di ciascuna procedura il fegato stato indagato ecograficamente ( esaote mylab 70 , sonda convex a banda larga con frequenze da 3 , 5 a 8 mhz ) con scansioni intercostali e sottocostali , per valutare il numero e le dimensioni delle lesioni , nonch i loro rapporti anatomici con strutture suscettibili di danno termico iatrogeno . previo monitoraggio dei parametri vitali , il trattamento stato sempre eseguito in analgo - sedazione utilizzando le stesse modalit standardizzate impiegate presso il nostro istituto per le rfa e linfissione dellantenna stata effettuata dopo disinfezione della cute ed anestesia locale con 10 ml al 2% di lidocaina cloridrato tamponata , e incisione della cute con bisturi con punta n . 
le lesioni con diametro massimo fino a 3 cm ( 2 / 19 ) sono state trattate con singola antenna ( 2 hcc ; 1 covidien , 1 hs ) , mentre per quelle con diametro superiore a 3 cm ( 17 / 19 ) sono state effettuate linserzione sincrona di multiple antenne ( possibile solo con lapparecchiatura covidien ; 5 hcc , 8 mts ) o inserzioni multiple di una singola antenna ( 4 hs ; 2 hcc , 2 mts ) , al fine di ottenere unarea di necrosi radiol med ( 2012 ) 117 : 378392 fig . 
2a - c tempi salienti della procedura : ecografia durante la pianificazione ( a ) , linserzione delle antenne ( b ) e il monitoraggio dellablazione ( c )  . analysis of results in agreement with the standards of the society of interventional radiology ( sir ) for studies on image - guided ablation [ 6 ] , the following aspects were considered : technical success of the procedure in terms of the possibility of correctly ablating the lesion to obtain an area of transient hyperechogenicity exceeding the diameter of the neoplastic tissue ( produced by vaporisation ) , visible for some minutes ; complications suspected on the basis of clinical events and / or changed laboratory findings and confirmed by instrumental investigations ( including radiology ) ; complications were classified in terms of severity according to sir [ 11 ] ( table 3 ) and as immediate , postprocedural and late if developing 624 h , 30 days or > 30 days , respectively , from the procedure [ 6 ] ; local efficacy ; all patients underwent four - phase ct examination ( ge medical system , healthcare lightspeed pro 16 , waukessha , mn , usa ) 3045 days after the procedure to analyse the area of necrosis , and in agreement with sir standards ( based on imaging evidence during follow - up ) [ 6 ] , we identified complete ablation di dimensioni adeguate . 
al termine dellablazione stata eseguita unecografia di controllo per escludere la comparsa di complicanze immediate ; in seguito i pazienti sono stati monitorati per 24 ore presso la struttura di degenza di provenienza . 
 analisi dei risultati anche in accordo con gli standard della societ di radiologia interventistica ( sir ) per gli studi sulle ablazioni imaging - guidate [ 6 ] , sono stati valutati : il successo tecnico della procedura , in termini di possibilit di infiggere correttamente la lesione ottenendo unarea di iperecogenicit transitoria esuberante il diametro del tessuto neoplastico ( dovuta a fenomeni di evaporizzazione ) e visualizzabile per alcuni minuti ; le complicanze , sospettate in base allinsorgenza di eventi clinici e / o allalterazione di parametri di laboratorio , e supportate da esami strumentali ( inclusi quelli radiologici )  . 
queste sono state classificate per gravit secondo il sistema sir [ 11 ] ( tabella 3 ) e come immediate / post - pro384 complications minor major complicanze minori maggiori table 3 society of interventional radiology ( sir ) classification system for complications by outcome radiol med ( 2012 ) 117 : 378392 a . 
decesso ( ca ) when an area of homogeneous hypoattenuation without enhancement was present in the entire ablated zone ; partial ablation ( pa ) when residual enhancement was present ; in consideration of the arbitrary nature of this definition , the recent modified response evaluation criteria in solid tumors ( recist ) criteria were adopted for hcc only ( considering pa a decrease by at least 30% in the sum of the diameters of residual vascular tissue with respect to the initial target lesion ) [ 12 ]  . in the case of ambiguous interpretation of results at ct ( evidence of an enhancement rim at the periphery of the ablated zone ) , we considered the possibility of supplementing the diagnosis by percutaneous needle biopsy of the lesion margins . 
in the case of pa and persistent clinical indications , patients underwent a second thermal ablation ( persistent pa after the second procedure was considered tf ) ; failing these indications , patients were referred for other palliative therapies . follow - up all patients were followed up by integrated imaging ( contrast - enhanced us , ct and / or pet - ct ) and blood testing ( including tumour markers ) according to the referring physicians requests . 
tf was defined as either persistent pa or local progression ( lp ) , that is , appearance of neoplastic tissue at the ablation site or in proximity to a previously ablated lesion [ as opposed cedurali / tardive se insorte rispettivamente a 624 ore / 30 giorni / oltre 30 giorni dalla procedura [ 6 ] ; lefficacia locale della procedura . 
tutti i pazienti sono stati sottoposti a esame tc ( ge medical system , healthcare lightspeed pro 16 , waukessha , minnesota , usa ) con protocollo quadrifasico dopo 3045 giorni dalla procedura per una valutazione dellarea di necrosi . 
sempre in accordo con i suddetti standard della sir ( basati sullevidenza allimaging durante il follow - up ) [ 6 ] , stata definita : ablazione completa ( ac ) la presenza di unipodensit omogenea , senza enhancement in tutte le fasi , della zona ablata ; ablazione parziale ( ap ) la presenza di enhancement residuo ; data la nota arbitrariet di tale definizione , limitatamente allhcc , sono stati utilizzati i recenti response evaluation criteria in solid tumors ( recist ) modificati ( considerando ap un decremento di almeno il 30% della somma dei diametri del tessuto vascolarizzato residuo rispetto alla lesione target iniziale ) [ 12 ]  . nei casi di dubbia interpretazione del risultato dellablazione allesame tc ( evidenza di un rim di enhancement alla periferia della zona ablata ) , si contemplata la possibilit di un completamento diagnostico mediante agobiopsia percutanea di tale margine . 
nei casi di ablazione parziale , se ancora presenti le indicazioni cliniche , il paziente stato sottoposto a unulteriore seduta di termoablazione ( la persistenza di ablazione parziale dopo la seconda sessione stata considerata come fallimento del trattamento ) ; in caso contrario il paziente stato indirizzato ad altre terapie palliative . radiol med ( 2012 ) 117 : 378392 to distant progression ( dp ) , which refers to the appearance of one or more new lesions in the remaining hepatic parenchyma or in extrahepatic regions ]  . follow - up statistical analysis the unbalanced distribution of treatments between the two devices ( 14 coviden , five hs ) and the heterogeneous histological and dimensional distribution of lesions did not permit an acceptable stratification for comparison between the two mw systems . 
the prognostic value of the largest diameter was calculated by using the same test , considering the thresholds described above ( or > 4.5 cm ; or > 5 cm ) ; conversely , the difference between mean / median lesion diameter with ca compared with lesions with pa was analysed with the unpaired t test and the mannwhitney u test . 
as regards tf , we calculated the percentages of persistence or lp ; furthermore , outcomes were correlated with histological type and with the size of lesions treated using the statistical tests mentioned above . 
the results of statistical analyses were considered significant with p values < 0.05. results duration of follow - up , starting from the date of mwa until the end of the follow - up period , ranged between 1 and 14 ( mean 8 ) months . 
for each lesion , 1.9 insertions were performed ( range 14 ) , with procedures lasting 19 ( range 1040 ) min . two patients , both with mts from colorectal carcinoma , developed complications classified as level d and b , respectively , on the basis of the sir scoring systein the first case , the lesion , which had already been treated by rfa , was located at the border between segments iv and viii ; this lesion had recurred and become complicated by a biloma produced by stenosis / fistulisation of the left hepatic duct , in turn treated by interventional radiology . 
after bile - duct reconstruction and after 1 month approximately , bile drainage catheters were removed ; 20 days later , despite the persistence of a small nonvascular biloma and in the absence of any symptoms , the intraparenchymal drainage catheter was removed as well . 
at approximately 9 months , tutti i pazienti sono stati monitorati con imaging integrato ( ecografia con mezzo di contrasto [ ceus ] , tc e / o pettc ) e indagini siero - ematiche ( incluso il dosaggio dei marcatori tumorali ) , anche in accordo con le indicazioni dei medici invianti . 
il fallimento del trattamento ( ft ) stato decretato o , come detto , in caso di persistenza di ablazione parziale , o in base alla comparsa di progressione locale ( pl ) , cio di tessuto neoplastico nella stessa sede o in prossimit di una pregressa lesione precedentemente ablata , distinta dalla progressione a distanza ( pd ) ossia la comparsa di una o pi nuove lesioni nel restante parenchima epatico o in sede extraepatica . analisi statistica il numero sbilanciato di trattamenti tra le due diverse apparecchiature ( 14 coviden , 5 hs ) , nonch la disomogenea distribuzione anche istologica e dimensionale delle lesioni , non ha consentito una stratificazione accettabile per ten tare un confronto tra i due sistemi di produzione di mw . 
pertanto , lefficacia locale stata correlata solo con listotipo delle neoplasie e , soprattutto , con le dimensioni delle lesioni trattate , allo scopo di valutare il significato prognostico di questi due parametri . 
il significato prognostico del diametro massimo stato valutato con il medesimo test , considerando le soglie descritte in precedenza ( / > 4 , 5 cm , / > 5 cm ) ; la differenza tra il diametro medio / mediano delle lesioni con ablazione completa rispetto a quello delle lesioni con ablazione parziale stata invece analizzata con lunpaired t - test e il test di mann - whitney . 
per ci che riguarda il fallimento del trattamento , sono state calcolate le percentuali di persistenza o pl ; loutcome stato inoltre correlato con listotipo della neoplasia e con le dimensioni delle lesioni trattate , utilizzando i test statistici di cui sopra . 
i risultati delle analisi statistiche sono stati espressi come significativi per un valore p < 0 , 05 . risultati il tempo di follow - up , considerato a partire dalla data della mwa ed esteso sino al termine dellosservazione , varia tra 1 e 14 mesi ( media 8 mesi )  . 
per ogni lesione sono state condotte in media 1 , 9 infissioni ( min 1 , max 4 ) , con una durata media della procedura pari a 19 minuti ( range 1040 minuti )  . in due pazienti sono state registrate due complicanze , classificate come d e b in base alla classificazione sir , entrambe in pazienti trattati per mts da carcinoma del colonretto . 
la tc un mese dopo il trattamento mostra un cercine di tessuto ancora vitale alla periferia della zona ablata , confermato dallagobiopsia . four - phase ct depicted disease progression with evidence of a large local recurrence at the site of the previous biloma and thrombosis of the portal branch of the iv segment . 
of the four patients with hcc , three underwent transcatheter arterial chemoembolisation ( tace ) , whereas one patient was lost to follow - up . figures 4 and 5 show the overall efficacy values ( per lesion ) in relation to lesion histological type and diameter , respectively . 
 regarding correlation with lesion size , no statistically significant difference in the number of ca was identified between lesions with diameter or > 4.5 ( p = 0.35 ) or or > 5 cm ( p = 0.26 ) , but there was a higher percentage in both cases in the group with smaller diameters ( 4.5 cm 45% , > 4.5 26% ; 5 cm 58% ; > 5 cm 11% )  . 
54 mm ; passaggio tra i segmenti iv ed viii , gi sottoposta a rfa e recidivata , complicatasi con biloma da stenosi / fistolizzazione del dotto epatico sinistro , trattato mediante manovre radiologiche interventistiche . 
in entrambi i dotti biliari principali intraepatici venivano posizionati 2 drenaggi biliari esterni - interni di 8 f e nel biloma veniva inserito un drenaggio di 8 , 4 f ; dopo bilioplastica e circa 1 mese i drenaggi biliari venivano rimossi ; dopo ulteriori 20 giorni , pur persistendo un piccolo biloma non rifornito e in assenza di sintomatologia , anche il drenaggio intraparenchimale veniva retratto . 
a circa 9 mesi , la tc quadrifasica documentava progressione di malattia con evidenza di una voluminosa recidiva locale nella sede del pregresso biloma , nonch trombosi del ramo portale del iv segmento . 
nel secondo caso , in presenza di comorbilit per diabete non insulino - dipendente , si verificato un episodio febbrile con temperatura elevata , trattato con successo con antibioticoterapia domiciliare . 
dei 4 pazienti con hcc , 3 sono stati sottoposti a chemioembolizzazione arterio sa transcatetere ( tace ) , 1 caso stato perso al follow - up . radiol med ( 2012 ) 117 : 378392 45 mm vs . 
quanto alla correlazione con le dimensioni delle lesioni , non si sono evidenziate differenze statisticamente significative nel numero di ac tra le lesioni di diametro inferiore / uguale o superiore a 4 , 5 ( p = 0 , 35 ) , o a 5 cm ( p = 0 , 26 ) , ma solo una percentuale in entrambi i casi superiore nel gruppo con diametri inferiori ( 4 , 5 cm 45% , > 4 , 5 cm 26% ; 5 cm 58% ; > 5 cm 11% )  . 
analogamente il diametro medio e mediano delle ac risultato inferiore a quello delle ap ( 44 mm versus 54 mm e 45 mm versus 51 mm ) , ma tali differenze non hanno raggiunto la soglia di significativit statistica ( rispettivamente p = 0 , 16 ; p = 0 , 31 )  . nel corso del follow - up ( 2 lesioni escluse perch il follow - up era di un solo mese , altre 2 nel medesimo paziente perch il paziente stesso stato perso al follow - up ) , si constatato il fallimento del trattamento in 9 / 15 ( 60% ) lesioni per persistenza o pl della neoplasia , mentre la ac stata mantenuta in 6 / 15 lesioni ( 40% )  . 
5a - c correlation between diameter and complete ( ca ) versus partial ( pa ) ablation based on the 45 - mm ( a ) and 50 - mm ( b ) threshold . 
a per valori di diametro 45 mm , > 45 mm ; b per valori di diametro 50 mm , > 50 mm ; c differenza tra diametro ( mm ) delle lesioni con ablazione completa rispetto a quelle con ablazione parziale . 388 radiol med ( 2012 ) 117 : 378392 fig . 
7a , b correlation between lesion diameter and treatment failure ( tf ) based on the 45 - mm ( a ) and 50 - mm ( b ) thresholds . 
in our experience , complete ablation maintained over time was almost 70% for colorectal mts up to 3 cm and only 33% for larger lesions , but most of all , survival was significantly longer in patients with diameter of the main lesion 3 cm [ 4 ]  . 
until now , in view of the mentioned size limits dictated by the devices ( related to the features of needle electrodes and to the power of the generators used ) , it is not possible to successfully treat a nonnegligible percentage of patients with large lesions ineligible for surgery and / or poorly responsive or refractory to chemotherapy . 
this has prompted healthcare providers to stringently select patients and the medical device industry to develop percutaneous thermal ablation systems capable of producing larger volumes of necrosis with short procedure times . 
mwa fits into this scenario , and noteworthy experiences are already available in the literature , even though no uniformly adopted technique has yet been identified [ 17 ]  . 
 in base a diversi studi , anche ampi ma quasi esclusivamente retrospettivi , la rfa garantisce , per lesioni di diametro 3 cm in pazienti non eleggibili alla chirurgia , risultati soddisfacenti , con una sopravvivenza a 3 anni del 28%37% nelle metastasi da carcinoma colo - rettale e del 38%77% nellhcc [ 13 ] , e con una percentuale di progressione locale di malattia variabile tra il 3 , 6% e il 60% nelle mts colo - rettali [ 3 ] , e tra il 14% e il 17% nellhcc [ 14 , 15 ]  . 
nella nostra esperienza lablazione completa mantenuta nel tempo stata di quasi il 70% nelle mts colo - rettali fino a 3 cm , e solo del 33% nelle lesioni di diametro superiore , ma soprattutto la sopravvivenza risultata significativamente superiore nei pazienti con diametro della lesione principale 3 cm [ 4 ] ; in particolare , a una pi recente analisi della nostra casistica ( 248 pazienti ) , le dimensioni si sono confermate il principale fattore prognostico , con una sopravvivenza mediana dallesecuzione della rfa di 45 mesi in caso di diametro massimo fino a 2 , 5 cm , 28 mesi tra 2 , 5 e 3 , 5 cm e soli 18 mesi oltre i 3 , 5 cm [ 16 ]  . 
fino a oggi , dunque , in considerazione dei suddetti limiti dimensionali imposti dalle apparecchiature ( legati alle caratteristiche degli aghi - elettrodi e alla potenza dei generatori commercializzati ) , non possibile trattare con successo una non trascurabile percentuale di pazienti con lesioni voluminose gi escluse dalla chirurgia e / o poco responsive o refrattarie alla chemioterapia . 
 questo dato ha spinto gli operatori sanitari a selezionare in maniera restrittiva i pazienti e lindustria a sviluppare device per termoablazione percutanea in grado di ottenere volumi di necrosi pi ampi in tempi il pi possibile contenuti . 
in questo panorama si collocano le microonde , di cui sono gi disponibili in letteratura esperienze degne di rilievo , ma per le quali non sono ancora state indicate modalit di applicazione uniformemente condivise [ 17 ]  . 
discutendo gli aspetti tecnici , bisogna sottolineare che , se le modalit di infissione sono molto simili a quelle degli aghi da rfa non uncinati , lantenna da mwa richiede qualche accortezza in pi ( per esempio , una pi profonda incisione dei tessuti molli superficiali ) per la maggiore fragilit del teflon . 
in most cases , it was possible to focus all energy on the neoplasm without damaging adjacent noble structures ; in fact , the only major complication occurred on a malacic bile duct , which was damaged by a previous rfa procedure . 
finally , the limited procedure times could reduce the dose of analgesics and sedatives , which may sometimes produce dangerous cardiorespiratory alterations . in our study , statistical analysis aimed at establishing a relationship between local treatment efficacy , tumour type and lesion diameter did not produce statistically significant results . 
this may be attributed at least in part to the small size of our series and to patient selection , which was made following ethically correct inclusion criteria but which increased the variability of the lesions treated . 
this could be explained by a greater aggressiveness in our approach to metastases resulting from an awareness that a greater safety margin is needed compared with hcc , and the liver has a higher functional reserve and is less prone to haemorrhagic complications in patients not suffering from liver disease . 
lastly , we did not believe that invasive treatment of large hcc was justified because the therapeutic intervention is only palliative ( hcc nodules > 5 cm have a high likelihood of developing satellite lesions and microvascular invasion [ 19 ] ) , and possible persistent disease could still be treated with tace . 
per contenere questo fenomeno sono stati sperimentati rivestimenti isolanti sulla superficie dellantenna o sistemi di raffreddamento interni ad essa con soluzione fisiologica o gas ; la dispersione di energia lungo il cavo di connessione tra generatore e antenna ; i diametri relativamente grandi ( in media superiori agli aghi elettrodi da rfa ) e la conseguente traumaticit degli applicatori ; laspetto fusiforme dellarea di ablazione , con diametro maggiore lungo lasse dellapplicatore ( specie impiegando antenne di prima generazione )  . quanto alla sicurezza della tecnica , nella nostra del tutto preliminare esperienza , la mwa si rivelata semplice e sicura . 
nella gran parte dei casi stato possibile focalizzare lenergia sulla neoplasia senza danneggiare strutture nobili contigue ; lunica complicanza maggiore occorsaci infatti avvenuta su una via biliare malacica , gi danneggiata da una precedente rfa . 
 i ridotti tempi di procedura potrebbero infine consentire di ridurre il dosaggio di analgesici e sedativi , che talvolta possono causare pericolose alterazioni cardio - respiratorie . nel nostro studio , lanalisi statistica condotta per stabilire una relazione tra lefficacia locale del trattamento , il tipo di tumore e il diametro delle lesioni non ha prodotto risultati statisticamente significativi ; questo imputabile almeno in parte al ridotto numero del campione e alla modalit di selezione dei pazienti , dovuto ai criteri di inclusione eticamente corretti , ma che hanno aumentato la variabilit delle lesioni trattate . 
tuttavia , i nostri risultati suggeriscono una maggiore incisivit delle mw nellablazione di lesioni secondarie ; questo dato potrebbe essere spiegabile con la nostra maggiore aggressivit nellapproccio alle metastasi , suggerito dalla consapevolezza sia di dover ottenere un maggior margine di sicurezza rispetto allhcc , sia di poter aggredire nel paziente non epatopatico un fegato con maggiore riserva funzionale e meno suscettibile di complicanze emorragiche ; infine non abbiamo ritenuto giustificato trattare in modo troppo invasivo hcc di grandi dimensioni perch lintervento terapeutico in tal caso palliativo ( i nodi di hcc superiori a 5 cm hanno elevata probabilit di satellitosi e invasione microvascolare [ 19 ] ) e leventuale malattia persistente avrebbe ancora potuto essere sottoposta a tace . 
 altre cause di ablazione incompleta potrebbero essere fattori tecnici , come : il mancato ancoraggio delle antenne non uncinate in sedi soggette a movimenti fisiologici ( per esempio , cupola epatica e atti respiratori ) ; la difficolt di un corretto parallelismo in casi di infissioni multiple contemporanee ( specie se introdotte con approccio intercostale ) ; lerrata interpretazione del volume lesionale e linadeguata previsione tridimensionale . nella nostra esperienza lefficacia del trattamento nel radiol med ( 2012 ) 117 : 378392 tion of lesion volume ; and inadequate three - dimensional vision . in our experience , the efficacy of mwa treatment in local disease control was slightly worse compared with values reported in the literature [ 18 ] , with a 33% percentage of disease progression for mts and 27% for hcc . 
the only randomised prospective trial conducted on hcc nodules with diameter < 3 cm [ 20 ] reported no significant difference in terms of efficacy , disease recurrence and survival between rfa and mwa ; hence , there is no strong evidence allowing us to confirm the superiority of mwa , but only indications on the potential utility coming from larger comparative studies . conclusions any preliminary experience inevitably concludes with the hope of being able to demonstrate the superiority of a new technique ( mwa ) over the standard procedure ( rfa ) in future randomised trials . 
in fact , the use of mwa , although at present more expensive than the reference standard rfa , has shown an adequate technical success and reasonable safety in the ablation of more - advanced liver neoplasms compared with those treated with rfa in oncological treatment protocols . 
we believe that , on the one hand , there is a need for further investigation into the longterm local efficacy of mwa and , on the other , for comparative clinical studies on time to progression with regard to hcc and long - term survival of patients who may have been cured thanks to more radical ablations as regards mts . controllo locale della malattia risultata lievemente peggiore rispetto ai valori pi frequentemente riportati in letteratura [ 18 ] , con una percentuale di progressione di malattia pari al 33% nelle mts e al 27% negli hcc . 
 ci si potrebbe spiegare con la nostra learning curve e i gi citati criteri di selezione , in particolare le dimensioni cospicue delle lesioni ; anche nel nostro studio , infatti , il diametro delle lesioni si confermato un fattore prognostico significativo per la progressione locale di malattia ( p = 0 , 006 )  . confrontando i suddetti studi clinici sulla rfa con quelli sulla mwa si riscontrano risultati lievemente maggiori con sopravvivenze a 3 anni dal trattamento di lesioni metastatiche da crc e di hcc variabili tra il 43%73% [ 9 ] e una percentuale media di recidive locali del 15% ( tra 0 e 50% ) nelle mts , e di circa il 10% nella maggior parte degli studi sullhcc ( in alcuni studi anche superiore al 50% ) [ 18 ]  . 
nellunico trial prospettico randomizzato condotto su nodi di hcc con diametro < 3 cm [ 20 ] non sono per state riportate differenze significative in termini di efficacia , ricorrenza di malattia e sopravvivenza tra ablazioni ottenute con rf e con mw ; non vi sono dunque ancora sicure evidenze che consentano di affermare la superiorit della mwa , ma solo indicazioni sulla potenziale utilit di pi ampi studi comparativi . conclusioni linevitabile conclusione di ogni esperienza preliminare lauspicio di poter in futuro dimostrare con trial randomizzati la superiorit di una nuova tecnica ( la mwa ) rispetto a quella standardizzata ( la rfa )  . 
noi riteniamo che i risultati del nostro studio incoraggino a proseguire la sperimentazione di questa promettente tecnologia ; luso delle mw , seppur per ora pi costose , ha infatti dimostrato adeguato successo tecnico e sufficiente sicurezza nellablazione di neoplasie epatiche pi avanzate rispetto a quelle trattate con rf in protocolli terapeutici oncologici a oggi considerati standard . 
a total of 142 patients with suspected biliary complications after liver surgery underwent hepatobiliary mr before and after administration of gadolinium ethoxy benzylic diethylenetriamine pentaacetic acid ( gd - eob - dtpa )  . 
sono stati valutati 142 pazienti sottoposti ad intervento di chirurgia epatica con sospette complicanze biliari con colangio - pancreato - rm ( mrcp ) e sequenze post - contrasto con somministrazione di gadolinio - acido etossi - benzil - dietilen - triamino - pentaacetico ( gd - eob - dtpa )  . 
 the diagnosis of major biliary complications represented by fistulas , leakage and stenosis is crucial for an accurate choice of conservative medical , interventional or surgical treatment and is associated with improved patient outcome [ 2 , 3 ]  . 
surgical interventions by laparoscopy in the last decade have almost routinely replaced the open technique as the procedure of choice for symptomatic gallstones [ 6 ] due to multiple benefits in terms of better aesthetic result , shorter hospitalisation , early return to work [ 7 ] and reduced perioperative mortality rates [ 8 ]  . 
the pancreatic fistula is one of the most serious and feared complications after pancreaticoduodenectomy , with a high mortality rate ranging from 850% up to 80% according to the same authors [ 12 , 13 ]  . 
 biliary complications after hepatectomy are related to many factors , such as patient age , white blood cell counts before surgery , duration and kind of intervention , left versus right hepatectomy and occurrence and extent of intraoperative bleeding . 
imaging diagnosis requires the integrated use of ultrasound ( us ) , computed tomography ( ct ) , endoscopic retrograde cholangiopancreatography ( ercp ) and magnetic resonance ( mr ) imaging [ 3 , 1416 ]  . 
us can detect the presence of peritoneal fluid and biliary tract dilatation , but it is operator dependent and does not always lead to a precise diagnostic hypothesis [ 3 ]  . 
ercp is certainly endowed with a high diagnostic accuracy in evaluating the biliary tree and provides precise anatomical detail of the injury , except in the case of tight stenosis , where it is limited to the study of the distal lesion , without being able to study the portion of the biliary tree proximal to the obstruction [ 3 ] ; it also allows for therapeutic manoeuvres but is conditioned by a high level of invasiveness [ 18 , 19 ] and a high risk of complications ( biliary sepsis , bile leakage , acute pancreatitis , duodenal perforation , biliary peritonitis , endoluminal bleeding ) [ 18 ] , use of ionising radiation and iodinated contrast media , adverse la patologia biliare iatrogena unevenienza relativamente frequente negli interventi di chirurgia epatica che grava il decorso post - operatorio , con incremento del tasso di morbilit e mortalit [ 1 ] e riducendo la qualit di vita e la sopravvivenza a lungo termine [ 2 , 3 ]  . 
la diagnosi delle principali complicanze biliari rappresentate da fistole , leakage , e stenosi appare fondamentale per unaccurata scelta del trattamento conservativo , medico , interventistico o chirurgico , e si associa ad un miglior outcome per il paziente [ 2 , 3 ]  . 
gli interventi con tecnica laparoscopica nellultima decade hanno sostituito quasi di routine la tecnica aperta , come procedura di scelta nelle litiasi sintomatiche [ 6 ] per i molteplici vantaggi in termini di miglior risultato estetico , pi breve ospedalizzazione , precoce ritorno allattivit lavorativa [ 7 ] e ridotta mortalit peri - operatoria [ 8 ]  . 
lincidenza delle complicanze , in relazione al tipo di chirurgia , varia dallo 0 , 1%0 , 5% con tecnica aperta , fino al 1 , 2% in laparoscopia [ 3 ]  . 
la fistola pancreatica una delle pi gravi e temute complicanze dopo duodenocefalopancreasectomia ( dcp ) con unalta percentuale di mortalit correlata , con valori compresi tra l8% ed il 50% sino ad arrivare , secondo alcuni autori , all80% [ 12 , 13 ]  . 
 linsorgenza di complicanze biliari post - epatectomia in relazione a molti fattori quali let del paziente , la conta di globuli bianchi pre - operatoria , la durata dellintervento , se si tratta di una epatectomia sinistra e se si verifica unemorragia intraoperatoria e di che entit . 
la diagnosi strumentale prevede lutilizzo integrato di ecografia ( us ) , tomografia computerizzata ( tc ) , colangiopancreatografia retrograda endoscopica ( ercp ) e risonanza magnetica ( rm ) [ 3 , 1416 ]  . 
lus consente la valutazione della presenza di versamento addominale e di dilatazione delle vie biliari , ma operatore - dipendente e non sempre consente una precisa ipotesi diagnostica [ 3 ]  . 
la tc non permette sempre unottimale visualizzazione dellalbero biliare , anche se con limpiego della tc multidetettore ( tcmd ) questo limite stato in parte superato ; resta comunque lattuale indisponibilit di un mezzo di contrasto ( mdc ) iodato ad escrezione epatobiliare ai fini diagnostici [ 17 ]  . 
lercp sicuramente dotata di unelevata accuratezza diagnostica nella valutazione dellalbero biliare e permette un preciso dettaglio anatomico delle lesioni , tranne nel caso di stenosi serrate in cui si limita allo studio della porzione distale della lesione , senza poter studiare la porzione dellalbero biliare prossimale allostruzione [ 3 ] ; consente , inoltre , di 356 radiol med ( 2012 ) 117 : 354368 reactions to contrast medium or premedication [ 3 ] , a 310% failure rate ( due to impossible bile duct cannulation for anatomical factors and / or technical difficulties ) and heavy operator dependence [ 18 ]  . 
compared with ercp , mrcp presents the great advantages of documenting the biliary tree obstruction upstream to a lockout , locating the presence of abscesses or perihepatic fluid collections and showing the site of bile leakage ; it also allows parallel evaluation of the liver parenchyma and pancreas [ 20 ] , providing possible alternative diagnoses [ 19 ] although limited to those possible without using a contrast agent . 
in particular , gadolinium ethoxy benzylic diethylenetriamine pentaacetic acid ( gd - eob - dtpa ) is a liver - specific contrast agent that has the characteristic of being eliminated by a attuare manovre terapeutiche , ma condizionata da elevata invasivit [ 18 , 19 ] ed elevato rischio di complicanze ( sepsi biliare , leakage , pancreatite acuta , perforazione duodenale , peritonite biliare , sanguinamento endoluminale ) [ 18 ] , impiego di radiazioni ionizzanti e di mezzo di contrasto iodato , e reazioni avverse al mezzo di contrasto o alla premedicazione [ 3 ] , da un tasso del 3%10% di insuccesso ( incannulazione del dotto biliare non possibile per fattori anatomici e / o difficolt tecniche ) , e fortemente dipendente dalloperatore [ 18 ]  . 
la mrcp presenta , rispetto alla ercp , il grande vantaggio di documentare lalbero biliare a monte di una eventuale ostruzione serrata , di localizzare la presenza di ascessi o raccolte sottoepatiche , mostra la sede di leakage biliare e consente contestualmente anche fig . 
1a - c biliary leakage ( arrow ) in orthotopic liver transplantation ( olt ) : a , b magnetic resonance cholangiopancreatography ( mrcp ) , maximum intensity projection ( mip ) : the anastomotic leakage is evident . 
there are many characteristics that distinguish gd - eob - dtpa from other contrast agents : its high relaxivity , low plasma protein binding ( 10% ) and the relatively low dose of gadolinium ( 0.025 mmol / kg ) and contrast volume [ 23 ]  . 
because of the presence of the ethoxy benzylic group ( eob ) in the dtpa structure , approximately 50% of the administered dose of contrast agent is captured selectively through organic anion transporting polypeptides ( oatp ) on the basolateral membrane of healthy hepatocytes and then excreted in biliary pathways [ 24 ]  . 
gd - eob - dtpa has an extracellular phase and an accumulation phase ( liverspecific phase ) characterised by complete filling of the bile ducts , and it allows accurate and dynamic imaging , thus facilitating lesion characterisation . 
the many possible applications of ce - mrc have not yet been fully explored , and in particular , little attention has been given to the use of ce - mrc in assessing the broad spectrum of situations that may complicate the postoperative course of patients undergoing major liver surgery . 
the aim of this study was to demonstrate that , in evaluating biliary tract abnormalities that may occur in connection with major liver surgery , ce - mrc with liver - specific contrast medium can play a crucial and decisive role . una valutazione del parenchima epatico e pancreatico [ 20 ] permettendo cos possibili diagnosi alternative [ 19 ] anche se limitatamente a quelle fornite delle acquisizioni senza contrasto . 
in particolare , il gadolinio - acido etossibenzil - dietilentriamino - pentaacetico ( gd - eob - dtpa ) un mdc epato - specifico che ha la caratteristica di essere eliminato attraverso una duplice via di escrezione : 50% per via renale e 50% per via biliare [ 21 , 22 ]  . 
sono molteplici le caratteristiche che distinguono il gd - eob - dtpa dagli altri mdc : ridotto volume iniettato , alta relassivit , basso legame con le proteine plasmatiche ( 10% ) , dose relativamente ridotta di gd ( 0 , 025 mmol / kg ) [ 23 ]  . 
a causa della presenza del gruppo etossibenzilico ( eob ) nella struttura dtpa , circa il 50% della dose di gd - eob - dtpa somministrata viene captata selettivamente attraverso il trasportatore organic anion transporting polypeptides ( oatps ) presente sulla membrana cellulare degli epatociti sani e successivamente eliminata attraverso le vie biliari [ 24 ]  . 
la distribuzione epatica del gd - eob - dtpa presenta una prima fase vascolo - interstiziale extra - cellulare , ed una seconda fase di accumulo ( fase epatospecifica ) che si caratterizza per il completo riempimento dei dotti biliari e ne permette uno studio accurato , consentendo un imaging dinamico multifasico che radiol med ( 2012 ) 117 : 354368 358 fig . 
patients in whom mri was contraindicated were preliminarily excluded from the study , as were claustrophobic patients or those with a known hypersensitivity to gadoliniupatients were imaged with unenhanced mrcp and postcontrast sequences after 0.1 ml / kg gd - eob - dtpa ( 0.25 mmol / kg ) administration . 
 the 142 patients were distributed as follows : 21 ( 17 men and four women , mean age 53 years ) had undergone liver transplantation ( olt ) ; 50 patients ( 31 men and 19 women , mean age 57 years ) had undergone major liver resection ; favorisce la caratterizzazione delle lesioni . 
 da tempo ormai la mrcp , che non prevede la somministrazione di mezzo di contrasto , svolge un ruolo fondamentale nello studio delle vie biliari sia in situazioni di patologia primitiva che dopo intervento chirurgico [ 28 , 29 ]  . 
after acquisition of these sequences , 0.1 ml / kg ( 0.25 mmol / kg ) gd - eobdtpa ( primovist , bayer schering pharma ) was administered at a flow rate of 2 ml / s followed by a bolus of 20 ml of saline , and postcontrast images were obtained . 
lava 3d fat - suppressed t1 - weighted multiphase sequences were performed at 4.0 - mm slice thickness in the arterial , portal and equilibrium phases and repeated 20 min and 30 min after bolus administration ; mpr reformatted and 3d mip images were then reconstructed . 
the total duration of the examination was around 45 mtwo experienced radiologists then performed a blinded comparative assessment of the images obtained by conventional mrcp and ce - mrc with hepatocyte - specific contrast agent . 
the following parameters were considered for analysis : type of surgical intervention ; parenchymal contrast enhancement ; contrast enhancement of the biliary tract ; examination timing ; sono stati valutati 142 pazienti ( et media 52 ; 59 femmine , 83 maschi ) sottoposti ad intervento di chirurgia epatica maggiore , in follow - up clinico - laboratoristico per lo studio di possibili alterazioni delle vie biliari . 
i pazienti sono stati sottoposti ad indagine mrcp senza somministrazione di mezzo di contrasto e sequenze post - contrasto con somministrazione di gd - eob - dtpa 0 , 1 ml / kg ( 0 , 25 mmol / kg )  . 
i 142 pazienti valutati si sono cos distribuiti ( tabella 1 ) : 21 pazienti , dei quali 17 maschi e 4 femmine di et media di 53 anni , sottoposti a trapianto epatico ( olt ) ; 50 pazienti , 31 maschi e 19 femmine di et media di 57 anni , sottoposti a resezione epatica maggiore ; 63 pazienti , 35 maschi e 28 femmine di et media di 45 anni , sottoposti a colecistectomia ; ed 8 pazienti , 5 maschi e 3 femmine di et media di 66 anni , sottoposti a cefalopancreasectomia . 
dopo lacquisizione di tali sequenze , sono state ottenute immagitable 2 complications detected on magnetic resonance imaging for each surgical procedure complications , n ( % ) surgical procedure type of biliary complications radiol med ( 2012 ) 117 : 354368 360 6 ( 29 ) 5 ( 10 ) 7 ( 1.1 ) 4 ( 50 ) 6 ( 29 ) 5 ( 10 ) 7 ( 1 , 1 ) 4 ( 50 ) tabella 2 complicanze rilevate dalla rm per ogni tipo di procedura chirurgica complicanze , n ( % ) procedura chirurgica tipo di complicanze biliari orthotopic liver transplantation major liver resection cholecystectomy pancreaticoduodenectomy 3 anastomosis stenoses 2 inflammatory stenoses 1 biliary leakages 3 biliary fistulas 1 biliary leakage 1 inflammatory stenosis 5 biliary leakages 1 inflammatory stenosis 1 biliary fistula 3 biliopancreatic fistulas 1 biliary leakage olt resezione epatica maggiore colecistectomia cefalopancreasectomia 3 stenosi dellanastomosi 2 stenosi infiammatorie 1 biliary leakage 3 fistole biliari 1 biliary leakage 1 stenosi infiammatorie 5 biliary leakage 1 stenosi infiammatorie 1 fistole biliari 3 fistole biliopancreatiche 1 biliary leakage olt , trapianto ortotopico di fegato lesions of the bile ducts ( intrahepatic , hilar , extrahepatic )  . for each examination , a semiquantitative evaluation of the diagnostics possibilities provided by mrcp and ce - mrc in detecting postsurgical complications was performed , and a score was assigned : 0 = negative no alterations ; 1 = doubtful changes identified doubtfully or not fully characterised ; 2 = positive alterations identified with certainty . 
in three of these patients , the alteration was identified on both unenhanced mrcp and postcontrast images ( score 2 ) ; in two patients , the lesion was unclear and / or not completely detectable on ni post - contrasto dopo somministrazione di gd - eob - dtpa ( primovist , bayer schering pharma ) 0 , 1 ml / kg ( 0 , 25 mmol / kg ) ad un flusso pari a 2 ml / s , seguito da un bolo di 20 ml di soluzione fisiologica . 
si sono acquisite sequenze 3d lava ( slice thickness 4 , 0 mm ) in tre fasi ( arteriosa , portale , allequilibrio , a 20 min e 30 min ) e sono state ottenute ricostruzioni 3d , ricostruzione multiplanari ( mpr ) e mip . 
nei 22 dei 142 pazienti quindi sottoposti ad esame ercp , i risultati delle indagini rm sono stati retrospettivamente comparati con i dati emersi dalle indagini ercp . risultati allanalisi comparativa dei 142 pazienti , in 22 casi sono emerse complicanze post - chirurgiche ( tabella 2 ) ; questi 22 pazienti sono stati sottoposti ad ercp . 
dei 63 pazienti sottoposti a colecistectomia , 7 presentavano alterazioni delle vie biliari : 5 presentavano biliary leakage ; 1 paziente presentava stenosi infiammatorie ed 1 paziente presentava fistole biliari . 
4 contrast - enhanced magnetic resonance cholangiography ( ce - mrc ) after gadolinium ethoxy benzylic diethylenetriamine pentaacetic acid ( gd - eob - dtpa ) ( primovist ) administration in olt : maximum intensity projection ( mip ) , inflammatory stenosis ( arrow )  . 
 precontrast mrcp ( score 1 ) but was more clearly identified on ce - mrc images ( score 2 ) ; in a last patient , the alteration depicted by the postcontrast images ( score 2 ) was not visualised on unenhanced mrcp ( score 0 )  . 
 in three of these patients , the alteration was identified on both mrcp and ce - mrc sequences ( score 2 ) ; one patient showed a alteration not clearly or completely demonstrated by mrcp ( score 1 ) but that was identified on postcontrast images ( score 2 ) ; in the last patient , the alteration identified on postcontrast images ( score 2 ) had not been depicted by mrcp ( score 0 )  . 
of the 63 patients undergoing cholecystectomy , seven showed abnormalities of the biliary tract : biliary leakage ( n = 5 ) ; inflammatory stenosis ( n = 1 ) ; biliary fistulas ( n = 1 )  . 
in five of these cases , the alteration was identifiable in both the ce and non - ce sequences ( score 2 ) ; in one case , the lesion was not clearly and / or completely revealed by mrcp ( score 1 ) but was detected on postcontrast images ( score 2 ) ; in one case , the lesion was detected only on the ce - mrc images ( score 2 ) but not on the precontrast ones ( score 0 )  . of the eight patients who underwent pancreaticoduodenectomy , four had biliary lesions : biliarypancreatic fistulas ( n = 3 ) , and biliary leakage ( n = 1 )  . 
in three of these 362 radiol med ( 2012 ) 117 : 354368 denziata una lesione non chiaramente e / o completamente dimostrabile alla mrcp ( punteggio 1 ) , che stata per individuata dalle immagini post - contrasto ( punteggio 2 )  . 
la mrcp ha diagnosticato con certezza il 64% delle complicanze biliari post - chirurgiche ed ha permesso di sospettare la presenza di 5 alterazioni che sono poi state confermate dalla ercp . 
5 contrast - enhanced magnetic resonance cholangiography ( ce - mrc ) after gadolinium ethoxy benzylic diethylenetriamine pentaacetic acid ( gd - eob - dtpa ) ( primovist ) administration in hepatectomy : axial image . 
 patients , the alteration was identified both on the precontrast mrcp images and in the ce - mrc sequences ( score 2 ) ; one patient had a alteration not clearly and / or completely identified on the precontrast mrcp ( score 1 ) , which was , however , correctly identified on the ce - mrc images ( score 2 )  . 
in one case , however , the mrcp sequence showed a doubtful finding that ercp then excluded , whereas in two cases , mrcp did not reveal the lesion that was depicted by ce - mrc and confirmed by ercp ( table 3 )  . discussion mrcp is now established as a fundamental method in evaluating the biliary tract , both in primary diseases and after surgery . 
 [ 22 , 30 ] recently reported their experience with clinical applications of ce - mrc with gd - eob - dtpa , even though some preliminary studies had already appeared earlier [ 31 , 32 ]  . 
 the best diagnostic contribution is therefore provided by ce - mrc using liver - specific contrast medium , which allows accurate and dynamic study , providing functional as well as morphological information about biliary lesions [ 3 , 30 , 33 ]  . 
study of the biliary tree requires a detailed outline of each small anatomical structure , and it is thus essential to obtain high - quality imaging and high spatial resolution . 
the ce - mrc technique investigates the bile ducts by increasing the signal intensity of bile on t1 - weighted tale nella valutazione delle vie biliari , sia nelle situazioni di patologia primitiva che dopo intervento chirurgico . 
il miglior apporto diagnostico , pertanto , fornito dallattuazione di uno studio di ce - mrc , utilizzando mezzo di contrasto epatospecifico , che consente un accurato studio dinamico , in grado di fornire informazioni funzionali oltre che morfologiche delle lesioni [ 3 , 30 , 33 ]  . 
tra le complicanze biliari che gravano il decorso postoperatorio dopo intervento di trapianto epatico le pi frequenti includono le stenosi , il leakage biliare e la disfunzione dello sfintere di oddi [ 3842 ] : lincidenza risulta variabile da un 10% nel caso di donatore cadavere al 30% nel caso di donatore vivente . 
le stenosi rappresentano le complicanze tardive pi frequenti , verificandosi generalmente dopo mesi radiol med ( 2012 ) 117 : 354368 images acquired during the hepatobiliary excretion of contrast mediuthe high contrast obtained in the biliary tract after contrast administration makes mpr and mip of the biliary tree highly diagnostic . 
 as are related to technical factors such as an exceedingly tight seam , whereas the nas have a pathogenetic mechanism related to ischaemic and immunologic factors and to graft deficiency [ 39 ]  . 
this event can occur because the surgeon mistakes the common hepatic duct for the cystic duct , thus closing the former instead of the latter , or in case of incorrect assessment of abnormal course of the common hepatic duct , which is thus injured during the surgical procedure [ 36 , 37 , 43 ]  . 
this complication is often also due to a thermal injury during the surgical procedure that can lead to acute necrosis of the bile duct with bile leak or , if the injury is less severe , late fibrosis . 
with regard to complications occurring after pancreaticoduodenectomy , well described in the literature are the possible consequences of pancreatic enzyme activation when they are in contact with the enteric juice ( in the presence of pancreatic anastomosis dehiscence ) and the negative consequences in patients who develop postoperative peritonitis resulting in a pancreatic digestive fistula [ 44 ]  . 
left hepatectomy shows a higher incidence of bile leakage , but after right hepatectomy , bile leakage is frequently difficult to control due to the pumping action of the right hemidiaphragm [ 45 , 46 ]  . ce - mrc provides good representation of the nondilated bile duct segments , and this can be particularly useful in post - olt assessment . 
le as sono in relazione ad fattori tecnici come una sutura troppo stretta , mentre le nas riconoscono un meccanismo patogenetico legato a fattori immunologici , ischemici , ed insufficienza del graft [ 39 ]  . 
frequente anche lostruzione acuta del dotto epatico comune , che causa marcata dilatazione a monte ; tale evenienza si pu verificare perch il chirurgo scambia il dotto epatico comune per il dotto cistico e lo chiude , e in caso di errata valutazione di decorsi anomali del dotto epatico comune con lesione dello stesso durante la procedura chirurgica [ 36 , 37 , 43 ]  . 
tale complicanza si verifica spesso anche per una lesione termica durante la procedura chirurgica che pu portare a necrosi acuta del dotto biliare con leak biliare o , se la lesione meno severa , a fibrosi . 
per quanto concerne le complicanze post - duodenocefalopancreasectomia , sono ben descritte in letteratura sia le possibili conseguenze dellattivazione degli enzimi pancreatici quando questi vengono a contatto con il succo enterico ( in presenza di una deiscenza dellanastomosi pancreatica ) , sia le conseguenze negative nei pazienti che sviluppano una peritonite post - operatoria conseguente una fistola pancreatico - digestiva [ 44 ]  . 
 lepatectomia sinistra mostra unincidenza maggiore di leakage biliare , ma dopo epatectomia destra relativamente alta la frequenza di un leak difficilmente controllabile a causa dellazione di pompaggio dellemidiaframma destro [ 45 , 46 ]  . 
nel caso di pazienti con anastomosi bilioenterica , la ce - mrc consente di valutare la perviet dellanastomosi , evidenziare la presenza di bile leak , e dimostrare , in caso di una lesione cistica , la presenza di comunicazione tra questa e la via biliare [ 47 ]  . 
sebbene molte indicazioni allo studio delle vie biliari vengano soddisfatte dalla mrcp , ci sono delle specifiche situazioni in cui lutilizzo di ce - mrc con mezzo di contrasto epatospecifico diventa indispensabile : per esempio lo studio di leakage biliari dopo chirur366 radiol med ( 2012 ) 117 : 354368 in the case of a cystic lesion the presence of communication with the bile duct [ 47 ]  . 
although many indications to the study of the biliary tract are met by mrcp , there are specific situations in which the use of ce - mrc with liver - specific contrast becomes essential , for example , in studying bile leakage after surgery or trauma , and for functional evaluation of the sphincter of oddi [ 4750 ]  . 
mrcp is useful for highlighting the presence of biliary leakage , but it does not provide functional information ; it often shows indirect signs of the presence of leaks but cannot show them directly . 
ce - mrc , by contrast , provides both anatomical and functional information [ 17 ]  . this study showed that mrcp could detect 64% of bile duct lesions , but in 27% of cases , it led only to a suspected alteration without allowing a positive definition ( table 3 )  . 
di frequente la mrcp non consente di differenziare il biliary leakage da ascite , raccolte fluide , edema / flogosi dei tessuti molli , tutte condizioni comuni nel periodo post - operatorio . 
 da questo lavoro emerso che la mrcp stata in grado di rilevare il 64% delle lesioni delle vie biliari , ma nel 27% dei casi ha permesso di esprimere solo un sospetto di alterazione , senza consentire una definizione certa e dirimente ( tabella 3 )  . 
ce - mrc overcomes the limitations of mrcp in all cases in which the latter does not permit a definitive diagnosis and allows complete and definitive characterisation of biliary tract alterations in patients undergoing major liver surgery , without the use of more invasive tests , such as ercp , which exposes the patient to a high dose of ionising radiation and is burdened by a risk of serious complications . 
 the high concentration of gd - eob - dtpa in the bile ducts enables functional imaging of biliary excretion , assessment of segmental function , fistulas and extent of bile leakage , and differentiation of the causes of biliary obstruction . luso di mdc ad escrezione epatobiliare consente uno studio accurato e panoramico delle alterazioni delle vie biliari , specie nelle valutazioni delle complicanze postchirurgiche . 
158 , chung - der first road , taichung 406 , taiwan , tel . : + 886 - 952 - 196 - 994 ; fax : + 886 - 4 - 2201 - 9522 , e - mail : bihliuin@ms2.hinet.net received : 17 january 2011 / accepted : 15 march 2011 / published online : 21 october 2011 springer - verlag 2011 abstract purpose . 
following doppler ultrasound , patients were divided into groups based on baseline renal resistive index ( rri ) : normal rri ( 0.7 ) , group 1 ( n = 14 ) ; and abnormal rri ( > 0.7 ) , group 2 ( n = 5 ) , and were followed up with radioisotopic renography 1 or more years later . 
result of univariate generalised estimation equation ( gee ) analysis for the factors affecting the change in effective renal plasma flow ( erpf ) indicated that the high rri value ( rri > 0.7 ) correlated with the change in erpf . 
sono stati valutati 19 pazienti con et media pari a 50 anni [ scarto interquartilico ( iqr ) 3557 ] con tempo medio trascorso dal trauma di 4 , 7 anni ( iqr 1 , 39 , 2 ) , seguiti in follow - up mediante renografia radioisotopica . 
lanalisi univariata mediante equazione di stima generalizzata ( gee ) per i fattori che influenzano il flusso renale plasmatico effettivo ( fpre ) , ha indicato che un elevato irr ( > 0 , 7 ) correla con il cambiamento del fpre . 
pertanto si raccomanda lecografia doppler annuale per la stima dellirr e dellentit didronefrosi . radiol med ( 2012 ) 117 : 500506 keywords spinal cord injury doppler ultrasonography effective renal plasma flow parole chiave lesione midollo spinale ecografia doppler flusso plasmatico renale effettivo introduction after spinal cord injury , an overactive bladder with high outlet resistance may induce prolonged elevation of intravesical pressure . 
these authors found that patients with initially high rri values had poor renal function outcomes [ 12 , 13 ]  . annual urological evaluation of patients with spinal cord injury is one of the effective ways to assess renal function and detect hydronephrosis [ 14 , 15 ]  . 
traditionally , renal ultrasonography ( us ) has been used to determine the degree of hydronephrosis , and radioisotopic renography has been used to calculate effective renal plasma flow ( erpf )  . 
 our previous study [ 17 ] shows that patients with spinal cord injury and obvious hydronephrosis ( defined as at least grade 2 ) had higher rri values compared with normal patients . 
moreover , studies are often limited by the overall condition of the person with spinal cord injury and whether the person has an upper motor neuron or lower motor neuron bladder lesion [ 18 ]  . 
 reliable information on long - term consequences in these patients is needed so that physicians can assist persons with spinal cord injury in making the best possible decision concerning their optimal management . 
 therefore , the purpose of this study was to compare long - term renal function in patients with spinal cord injury using both the initial rri value and the annual change in erpf to determine whether rri has predictive value . 
 materials and methods from june 1998 to february 2000 , 51 spinal cord injury patients ( 38 men and 13 women ) underwent both doppler us and radioisotopic renography within 1 week . 
the median age was 50 ( iqr 3557 ) years , and the median time after injury was 4.7 ( iqr , 1.39.2 ) years ( table 1 )  . 
institutional review board approval was obtained prior to performing this study ; all patients gave their informed consent to participate . us scanner ( philips - envisor ; bothell , wa ) with a 2 - 5 mhz transducer was used to perform the examinations . 
colour doppler us was performed after the routine survey . colour - flow doppler imaging was used to identify intrarenal vessels , and waveforms were recorded from arteries at 502 radiol med ( 2012 ) 117 : 500506 fig . 
the annual change in erpf was defined as : ( follow - up erpf data initial erpf data ) / interval ( years )  . we defined deterioration of renal function as a decrease in erpf > 4.5 ml / min per year , in accordance with kuhlemeier et al . 
for kidney characteristics , data are represented as meanstandard deviation ( sd ) for continuous variables and n ( % ) for categorical variables by the initial rri0.7 ( group 1 ) , and > 0.7 ( group 2 ) , respectively . 
statistical analyses were performed using spss 15.0 statistics software ( spss inc , chicago , il , usa )  . results all patients underwent doppler us and radioisotopic renography from june 1998 to september 2000 and were followed up with radioisotopic renography after 1 or more years . 
as shown in table 2 , the average initial effective renal plasma flow ( erpf ) was 240.12 ml / min ( sd = 77.28 ) , and no sigradiol med ( 2012 ) 117 : 500506 fig . 
however , no significant difference was found between groups ( table 2 )  . the results of univariate generalised estimation equation ( gee ) analysis for factors related to erpf change are shown in table 3 . 
 our study showed that rri values can help predict renal function deterioration in patients with spinal cord injury : initial rri value negatively correlated with annual erpf change , and patients with initial rri > 0.7 had a more rapid annual decline in erpf change . after spinal cord injury , elevated intravesical pressure from neurogenic bladder dysfunction causes compression of the intramural ureter and ureteral efflux of urine towards the bladder ceases [ 1 ]  . 
increased renal resistance causes impairment of renal blood flow , and the consequent decrease in urine production restores the intrapelvic pressure balance to normal but with a persistent decrease in renal blood flow . 
 renal parenchymal resistance , measured by the rri , represents the global resistance to blood flow by the different parenchymal structures because of vascular or tubulointerstitial involvement [ 11 , 24 ]  . 
 [ 25 ] reported that an elevated rri ( > 0.7 ) was associated with impaired renal function , increased proteinuria at 24 h and poor outcome in patients with diabetic mellitus . 
 [ 13 ] reported that the rri correlated significantly with the rate of decline in reciprocal serum creatinine ( r = 0.52 , p = 0.02 ) in patients with chronic renal failure . 
 [ 28 ] reported a negative correlation between rri and 1 - month or 1 - year creatinine clearance ( ccr ) values ( 1 month , r = 0.564 , p < 0.05 ; 1 year , r = 0.466 , p < 0.05 ) in uncomplicated renal transplant recipients . 
when renal resistance is increased , renal blood flow declines for a given perfusion pressure , and because the decline is more prominent in diastole than in systole , it leads to an increase in rri [ 30 ]  . 
pulse pressure is a known marker of increased rigidity of the arterial vascular bed , which increases during aging as a result of stiffening of the arterial wall [ 31 , 32 ]  . 
 despite these previous reports , our study is the first to show a significant correlation between initial rri and decline in annual erpf change in patients with spinal cord injury . 
that in patients with hypertension and chronic renal failure , rri correlated significantly with erpf ( r = 0.5 , p = 0.006 ) and radiol med ( 2012 ) 117 : 500506 ccr ( r = 0.6 , p = 0.006 ) [ 3 ]  . 
in contrast , ccr measurement is an overall functional index of both kidneys and can therefore be an average of the left and right kidneys rather than a reflection of the individual kidney . 
conventional uroradiological studies are not recommended for patients who have normal renograms because these studies are more invasive and cumbersome and have more side effects , as well as higher radiation exposure . 
in a previous study , we found that radioisotope renography with tc - 99m mag3 is a safe , noninvasive , sensitive and valuable urological screening test for patients with spinal cord injury [ 14 ]  . 
in our study , we used radioisotope renography to measure erpf instead of gfr because alteration in renal tubular function probably occurs earlier than alteration in glomerular function as a result of obstruction or infection . 
 therefore , in patients with spinal cord injury , measuring erpf can probably provide earlier information regarding adverse effects of neurogenic bladder dysfunction on upper urinary tracts [ 14 ]  . 
lauro2 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e radioterapia , fondazione policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy 2unit di nefrologia , dipartimento di medicina interna , fondazione policlinico universitario tor vergata , viale oxford 81 , 00133 roma , italy correspondence to : a . 
all patients were studied by computed tomography angiography ( cta ) of the renal arteries before the procedure and underwent follow - up at 30 and 60 days with colour doppler ultrasound ( cdus ) with evaluation of resistive index , glomerular filtration rate ( gfr ) , 24 - h blood pressure and serum catecholamine concentration . 
in treated patients , mean blood pressure at baseline was 171 / 100 mmhg [ standard deviation ( sd ) 8 / 10 ] ; mean gfr was 91.6 ml / min / 1.73 m2 ( sd15 )  . 
 blood pressure after the procedure was reduced by 18 / 5 and 13 / 10 mmhg at 30 and 60 days , respectively , with a mean medication reduction of 3.6. 
stata eseguita angio - tomografia computerizzata ( tc ) delle arterie renali pre - procedurale e follow - up a 30 e 60 giorni con eco - color doppler , valutazione degli indici di resistenza , del filtrato glomerulare , monitoraggio della pressione arteriosa nelle 24 ore e misurazione della catecolaminemia . 
i valori pressori medi basali della popolazione erano 171 / 100 mmhg [ deviazione standard ( ds ) 8 / 10 ] , con filtrato glomerulare medio di 91 , 6 ml / min / 1 , 73 m2 ( ds15 )  . 
il decremento pressorio medio post - procedurale stato di 18 / 5 mmhg e 13 / 10 mmhg a 30 e 60 giorni con riduzione media di 3 , 6 farmaci . 
il sistema symplicity si dimostrato efficace nel ridurre i livelli pressori e la somministrazione dei radiol med ( 2012 ) 117 : 426444 patients affected by essential hypertension resistant to medical therapy . 
nonostante incoraggianti premesse , sar necessario validare i preliminari dati ottenuti mediante pi ampi studi prospettici randomizzati . keywords percutaneous renal denervation essential hypertension medical - therapy - resistant parole chiave simpaticectomia renale percutanea ipertensione essenziale resistenza a terapia farmacologica introduction introduzione arterial hypertension is among the leading causes of morbidity and mortality worldwide , being a major risk factor for acute myocardial infarction , stroke , heart failure and other cardiovascular and renal diseases . 
according to the american heart association ( aha ) , a 5 - mmhg reduction in systolic blood pressure ( sbp ) results in a 14% decrease in the likelihood of stroke , a 9% decrease in heart disease and a 7% decrease in the risk of death ; a 20 - mmhg decrease in systemic arterial pressure corresponds to a 50% reduction in cardiovascular mortality risk [ 1 ]  . 
central nervous system ( cns ) overactivity plays a leading role in increasing arterial blood pressure through baroreceptors located at the level of the renal afferent arterioles , which are particularly sensitive to changes in renal perfusion and to the amount of sodium that reaches the cells of the macula densa of the distal renal tubule . 
activation of the baroreceptors triggers renin secretion and thus stimulates the reninangiotensin aldosterone ( raas ) system , which represents one of the major determinants of increased arterial blood pressure . 
at present , the treatment of essential arterial hypertension is based on effective and safe pharmacological therapies that act on the raas system [ angiotensin - converting enzyme inhibitors ( acei ) , angiotensin ii receptor antagonists ] , on peripheral vascular resistance ( calcium - channel blockers , alphalytics ) , on sympathetic nervous system ( sns ) overactivity ( sympathomimetic drugs , beta - blockers ) and on blood - volume regulation ( diuretics )  . 
this reflects the inability of physicians to obtain adequate pressure control despite the use of all pharmacological therapies available and the frequent poor compliance among patients , who find it difficult to follow a lifelong drug therapy to control a disease that may be asymptomatic for a long time [ 2 , 3 ]  . 
within this setting , there is a subgroup of patients with hypertension refractory to pharmacological treatment , that is , patients who take at least three antihypertensive agents and neverthelipertensione arteriosa rappresenta una delle cause principali di morbilit e mortalit a livello mondiale risultando uno dei maggiori fattori di rischio dellinfarto acuto del miocardio , dello stroke , dello scompenso cardiaco e di altre malattie cardiovascolari e renali . 
 secondo i dati dellamerican heart association ( aha ) una riduzione di 5 mmhg della pressione sistolica determina un decremento del 14% della probabilit di stroke , del 9% di insorgenza di patologia cardiaca e del 7% del rischio di morte ; ad un decremento di 20 mmhg della pressione arteriosa sistemica corrisponde una riduzione della mortalit per cause cardio - vascolari pari al 50% [ 1 ]  . 
liperattivit del sistema nervoso centrale ( snc ) gioca un ruolo di primaria importanza nel determinare laumento della pressione arteriosa , attraverso barocettori posti a livello delle arteriole afferenti renali , sensibili alle variazioni della perfusione renale ed alla quantit di sodio che arriva a livello delle cellule della macula densa del tubulo distale renale . 
 lattivazione dei barocettori determina la secrezione di renina e quindi lattivazione del sistema renina - angiotensina - aldosterone ( raas ) che rappresenta uno dei principali fattori responsabili dellaumento dei livelli pressori arteriosi . 
attualmente il trattamento dellipertensione arteriosa essenziale si basa sullimpiego di terapie farmacologiche efficaci e sicure che agiscono sul sistema renina - angiotensina - aldosterone [ angiotensin converting enzyme ( ace ) - inibitori , antagonisti del recettore dellangiotensina ii ] , sulle resistenze vascolari periferiche ( calcio - antagonisti , alfalitici ) , sulliperattivit del tono simpatico ( simpaticomimetici , beta - bloccanti ) e sulla regolazione del volume ematico ( diuretici )  . 
in realt ad oggi stato stimato che solo il 65% circa della popolazione di pazienti trattata con terapia medica , ottiene soddisfacenti livelli pressori , dato da correlare alla impossibilit da parte dei medici di ottenere un adeguato controllo della pressione arteriosa nonostante lutilizzo di tutte le terapie farmacologiche a disposizione , nonch alla frequente scarsa compliance dei pazienti che riscontrano difficolt ad assumere per tutta la vita medicinali per la 428 radiol med ( 2012 ) 117 : 426444 less have pressure levels > 160 / 90 mmhg . 
in patients resistant to treatment in whom a secondary cause cannot be identified , high arterial blood pressure involves an increased risk of severe morbidity related to the presence of concomitant cardiovascular diseases , and in these patients , treating the hypertension is life saving [ 4 ]  . in the past , such patients were treated surgically with radical sympathectomy ( thoracic , abdominal and pelvic )  . 
 this treatment was effective in lowering arterial pressure , although it carried high perioperative morbidity and mortality rates and was often responsible for the onset of long - term complications , including bowel and bladder dysfunction , erectile dysfunction and severe postural hypotension [ 5 ]  . 
on the basis of this scientific evidence , a key role was demonstrated for the renal sns in regulating arterial pressure , a role already demonstrated in animal studies [ 6 ]  . 
 our purpose was to investigate the efficacy and safety of the ardian symplicity catheter system for percutaneous denervation in a preliminary series of five patients with essential hypertension refractory to conventional pharmacological treatment . materials and methods study population in september 2010 , five patients ( three men , two women ; mean age 50.6 years ) with arterial hypertension refractory to medical therapy were enrolled at our centre for arterial hypertension ( table 1 )  . 
the study population consisted of patients who had been unable to achieve acceptable pressure levels despite the use of three or more antihypertensive medications ( including a diuretic ) at the highest tolerated doses . 
they had a mean arterial pressure ( ap ) at baseline of 171 / 100 mmhg [ standard deviation ( sd ) 8 / 10 ] measured by 24 - h dynamic monitoring , with a mean heart rate ( hr ) of 71 bpm despite the use of an average of five antihypertensive drugs ( including the following pharmacological classes : acei , angiotensin ii receptor antagonists , beta - blockers , alpha - adrenergicblocking agents , calcium - channel blockers , direct vasodilators and diuretics )  . 
 following are the inclusion criteria : essential arterial hypertension not responding to pharmacological treatment with three or more antihypertensive cura di una patologia che per lungo tempo pu non essere sintomatica [ 2 , 3 ]  . 
in questo contesto si colloca un sottogruppo di pazienti affetti da ipertensione resistente a terapia farmacologica ovvero pazienti che assumono almeno 3 farmaci anti - ipertensivi e ci nonostante presentano valori pressori > 160 / 90 mmhg e che pertanto risultano resistenti alla terapia farmacologica . 
nei pazienti resistenti a terapia in cui non possibile trovare una causa secondaria , lelevata pressione arteriosa comporta un incrementato rischio di insorgenza di forme morbose gravi legate alla presenza di concomitanti malattie cardiovascolari in cui il trattamento dellipertensione risulta un intervento salvavita [ 4 ]  . 
essi risultavano efficaci nel ridurre la pressione arteriosa , ma gravati da elevati tassi di morbilit e mortalit nel peri - operatorio nonch spesso responsabili dellinsorgenza di complicanze a lungo - termine tra cui : disfunzioni intestinali e vescicali , disfunzioni erettili ed ipotensioni posturali severe [ 5 ]  . 
sulla base di tali evidenze scientifiche stato dimostrato un ruolo chiave del sistema nervoso simpatico renale nella regolazione della pressione arteriosa , peraltro gi dimostrato da studi su animali [ 6 ]  . 
 da ci nasce lesigenza di determinare linterruzione in modo selettivo delle fibre nervose del simpatico , attraverso tecniche interventistiche mini - invasive mediante limpiego di energia sottoforma di radiofrequenza ( rf )  . 
il nostro obiettivo stato quello di valutare lefficacia e la sicurezza del sistema ardian symplicity nel trattamento percutaneo di denervazione in una serie preliminare di 5 pazienti con ipertensione essenziale resistente alla terapia farmacologica convenzionale . materiali e metodi popolazione di studio nel mese di settembre 2010 , presso il nostro centro per lipertensione arteriosa sono stati arruolati 5 pazienti affetti da ipertensione arteriosa resistente a terapia medica . 
 la popolazione arruolata comprendeva pazienti che non erano in grado di raggiungere target pressori accettabili nonostante limpiego di 3 o pi farmaci anti - ipertensivi ( compreso un diuretico ) alle massime dosi tollerate . 
tutti i pazienti arruolati , hanno eseguito la procedura interventistica di denervazione del simpatico renale per via percutanea , presso il dipartimento di diagnostica per immagini e radiologia interventistica della nostra struttura . 
i pazienti in esame presentavano valori basali medi di pressione arradiol med ( 2012 ) 117 : 426444 drugs , including a diuretic ; sbp levels 160 mmhg ; normal renal function or with low or moderate chronic renal failure ( crf ) , according to the national kidney foundation kidney disease outcomes quality initiative ( nkf - kdoqi ) guidelines , based on glomerular filtration rate ( gfr ) measured with the cockcroftgault formula ; age > 18 years and < 75 years ; absence of renal pathology or systemic disease with possible renal involvement ; renal artery length 2 cm and minimum ostial diameter 4 mm ; no evidence of accessory renal arteries ; pathological microalbuminuria ( > 300 mg / 24 h ) ; altered fundus oculi examination ( varying degrees of hypertensive retinopathy ) and left ventricular hypertrophy at echocardiography . patients with clinical evidence of arterial hypertension secondary to renal , endocrine or pharmacological causes were excluded . 
all patients were required to accept and provide written informed consent before undergoing any of the procedures . preprocedural assessment all patients enrolled at our department of diagnostic imaging and interventional radiology underwent the following preprocedural examinations on an outpatient basis ( t0 ) : computed tomography angiography ( cta ) of the renal arteries using multiplanar ( mpr ) , volume rendering ( vr ) and maximum intensity projection ( mip ) reconstruction algorithms , as well as advanced vessel analysis ( ava ) , to obtain correct measurement of diameter and length of the renal arteries to check fulfilment of the anatomical inclusion criteria ; catecholamines and their metabolites ; proteinuria and microalbuminuria ; blood count , glycaemia , creatininaemia and cystatin c , azotaemia , uricaemia , plasma electrolytes ; lipid and coagulation profile ; colour doppler ultrasound ( cdus ) of the renal arteries to measure resistive index ( ri ) ; anaesthesiological assessment ; clinical and laboratory evaluation according to international guidelines to rule out any secondary cause for arterial hypertension . interventional procedure percutaneous renal sympathetic denervation was performed in the angiography room in the presence of an anesthesiologist and under constant invasive pressure and oximetry teriosa ( pa ) pari a 171 / 100 mmhg [ deviazione standard ( ds ) 8 / 10 ] , valutati mediante registrazione dinamica nelle 24 h , con una frequenza cardiaca ( fc ) media di 71 battiti per minuto nonostante lassunzione di una media di 5 farmaci anti - ipertensivi ( comprendenti le seguenti classi farmacologiche : ace - inibitori , antagonista del recettore dellangiotensina ii , beta - bloccanti , alfa - 1 bloccanti , calcio - antagonisti , vasodilatatori diretti e diuretici )  . 
il gruppo dei pazienti arruolati e trattati comprendeva 3 maschi e 2 femmine con unet media di 50 , 6 anni , che presentavano valori basali di pa considerati non a target nonostante la terapia plurifarmacologica assunta . 
tutti i pazienti dovevano accettare e firmare il consenso informato scritto prima dellimplementazione di qualsiasi procedura prevista . valutazione pre - procedurale i pazienti arruolati presso il dipartimento di diagnostica per immagini e radiologia interventistica della nostra struttura hanno eseguito , in regime di day - hospital , i seguenti esami pre - procedurali ( t0 ) : angio - tomografia computerizzata ( tc ) delle arterie renali mediante lausilio di algoritmi di ricostruzione , multiplanari ( mpr ) , volume rendering ( vr ) ed a massima intensit di proiezione ( mip ) , nonch limpiego 430 radiol med ( 2012 ) 117 : 426444 monitoring . 
a 5 - f pigtail catheter ( boston scientific natick , ma , usa ) was then inserted to perform a preliminary angiographic examination after administration of around 20 ml of iodinated contrast agent ( xenetix 300 , 300 mgi / ml ) to visualised all vascular anatomical structures . 
each renal artery was catheterised using a standard 180 - cm j - tip terumo guide wire ( terumo corporation , tokyo , japan ) and a 6 - f rdc1 guiding catheter ( boston scientific , tijuana , mexico ) ending in a y connector attached to a constant - pressure sodium chloride ( nacl ) bag ( 1 , 000 cc ) , which guarantees constant lavage of the catheter lumen during the procedure . 
 almost 3 , 000 iu of heparin were initially administered , followed by approximately 200 gamma of nitroglycerin selectively administered at the level of each renal artery to guarantee adequate arterial vasodilation and prevent vasospasm . the guide wire was then replaced by a symplicity catheter ( ardian inc , palo alto , usa ) , followed by a selective injection of 10 ml of iodinated contrast agent to depict renal artery anatomy . 
ablation was performed under roadmapping guidance at the level of the renal arteries , with the catheter placed at the distal third of the artery close to the lobar branches . 
the power delivered by the generator ( 58 w ) , with a maximum temperature of 52c , and the impedance of the catheter tip ( range 250350 ohm ) were constantly monitored throughout the ablation procedure . at the end of the procedure , a second angiography was performed to confirm renal artery patency and the absence of intraprocedural complications . 
vital parameters and blood count were monitored at the end of the procedure and 3 h later . patient hospitalisation lasted 2 days , with discharge on day 2 after the procedure . 
in patients with crf , this treatment was combined with oral administration of n - acetylcysteine to significantly reduce the risk of contrast nephrotoxicity . delladvanced vessel analysis ( ava ) , al fine di ottenere una corretta stima di diametro e lunghezza delle arterie renali che rientrino nei criteri anatomici di inclusione ; catecolamine e loro metaboliti ; proteinuria e microalbuminuria ; emocromo , glicemia , creatininemia e cistatina c , azotemia , uricemia , elettroliti plasmatici ; assetto lipidico e coagulativo ; eco - color doppler ( ecd ) arterie renali per la valutazione dellindice di resistenza ( ir ) ; valutazione anestesiologica ; esami clinico - laboratoristici , secondo le attuali linee guida internazionali , per escludere le cause secondarie di ipertensione arteriosa . procedura interventistica la procedura di denervazione del simpatico renale per via percutanea stata eseguita in sala angiografica , con presenza di anestesista e con monitoraggio continuo della pressione invasiva ed ossimetria . 
previo approccio trans - femorale retrogrado destro stato posizionato un introduttore 6 f ( terumo corporation , tokyo , giappone ) attraverso il quale stato inserito un catetere pigtail 5 f ( boston scientific natick , ma , usa ) , al fine di effettuare il preliminare esame angiografico con somministrazione di circa 20 ml di mezzo di contrasto ( mdc ) organo - iodato ( xenetix 300 , 300 mgi / ml ) e visualizzare le strutture anatomiche vascolari . 
si proceduto a cateterizzazione di ciascuna arteria renale mediante guida terumo j 180 standard ( terumo corporation , tokyo giappone ) e catetere guida con morfologia rdc1 6 f ( boston scientific tljuana , b.c. , messico ) collegato a rubinetto ad y valvolato connesso a sacca a pressione costante di nacl ( 1000 cc ) che garantisce un lavaggio permanente del lume del catetere nel corso della procedura ed alla somministrazione di circa 3000 ui di eparina . 
sono stati successivamente somministrati circa 200 g di nitroglicerina selettivamente in corrispondenza di ciascuna arteria renale al fine di garantire unadeguata vasodilatazione dellarteria stessa e prevenire eventuali vasospasmi . la guida stata poi sostituita con il catetere symplicity ( ardian inc , palo alto , ca , usa ) a cui ha fatto seguito una iniezione selettiva di circa 10 ml di mdc iodato per confermare lanatomia della arteria renale . 
sotto guida road mapping si proceduto alle ablazioni a livello delle arterie renali , posizionando il catetere in corrispondenza del terzo distale dellarteria stessa , in prossimit delle diramazioni lobari . 
serie di ablazioni endovascolari con intervalli di retrazione di circa 5 mm e torsione di circa 90 del catetere simplicity , dalla porzione distale inferiore pre - dicotomica dellarteria renale sino a circa 5 mm dallostio , nella porzione superiore dellarteria stessa . follow - up patients treated by percutaneous renal sympathetic denervation underwent follow - up at 30 ( t1 ) and 60 days ( t2 )  . 
 the follow - up consisted of : clinical examination ; blood chemistry tests ; 24 - h urine assay for catecholamines and their metabolites , proteinuria , microalbuminuria ; cdus of renal arteries ; 24 - h ap monitoring ; cta of renal arteries at 60 days . results the mean duration of the procedure was 32 ( range 3045 ) min , the time needed to denervate both renal arteries . 
durante lablazione , stata costantemente monitorata la potenza erogata dal generatore ( compresa tra 58 watt ) , con temperatura massima di 52 gradi centigradi , e limpedenza della punta del catetere , la quale doveva avere un valore compreso tra 250 e 350 ohm . al termine della procedura stata eseguita una ulteriore angiografia per confermare la perviet delle arterie renali e lassenza di complicanze intraprocedurali . 
sono stati monitorati i parametri vitali ed eseguiti controlli emocromocitometrici al termine della procedura ed a distanza di 3 ore . i pazienti trattati sono stati ricoverati in regime di degenza per 2 giorni , con dimissione in seconda giornata dallef432 radiol med ( 2012 ) 117 : 426444 figs . 
to induce conscious sedation , 2 mg of midazolam was administered 510 min before the procedure , followed by an additional maintenance dose of fentanyl citrate ( fentanest , 50 mg )  . 
after the procedure , only one woman of the five treated patients reported persistent visceral pain , which lasted 12 h and required analgesics : 50 mg / 2 ml tramadol i.v. 
none of the patients had abnormal blood count , which revealed stable haemoglobin and haematocrit values at 1 , 3 and 6 h from the procedure . no complications occurred either intraor periprocedurally or at the 30and 60 - day follow - up ( t1 and t2 )  . 
cdus repeated at t1 and t2 revealed no strictures at the level of the treated renal arteries in any patient , with regular ri measured at the ostium and middle third and at the level of the main intraparenchymal branches ; there were no significant variations compared with the preprocedural examifettuazione della procedura . 
nelle 12 ore precedenti e successive alla procedura , secondo la pratica clinica , i pazienti sono stati idratati per via orale o mediante la somministrazione endovenosa di liquidi ( soluzione salina 0 , 9% )  . 
nei pazienti gi affetti da irc , al fine di ridurre significativamente il rischio di nefrotossicit da mezzo di contrasto organoiodato , tale terapia stata associata allassunzione orale di fluimucil ( n - acetilcisteina )  . follow - up i pazienti trattati con procedura di denervazione del simpatico renale per via percutanea sono stati sottoposti ad un follow - up a 30 ( t1 ) e 60 giorni ( t2 )  . 
il follow - up stato articolato in : esame clinico ; esami ematochimici ; dosaggio sulle urine / 24 h di catecolamine e loro metaboliti , proteinuria , microalbuminuria ; ecd delle arterie renali ; monitoraggio pa nelle 24 h ; angio - tc delle arterie renali a 60 giorni . radiol med ( 2012 ) 117 : 426444 fig . 
no risultati la durata media della procedura stata di circa 32 min ( range 3045 min ) , tempo in cui stata effettuata la denervazione di entrambe le arterie renali . 
nel corso della procedura e durante lemissione di rf , alcuni pazienti hanno riferito linsorgenza di diffuso dolore viscerale , opportunamente controllato mediante la somministrazione di farmaci sedativi per via endovenosa . 
per linduzione della sedazione vigile sono stati somministrati 2 mg di midazolam 510 minuti prima della procedura seguiti dalla somministrazione della dose aggiuntiva di mantenimento di fentanil citrato ( fentanest ) 50 g . 
urinary catecholamines showed no significant variation and remained within the normal range in all patients ( epinephrine 020 mg / 24 h , norepinephrine 23105 mg / 24 h , normetanephrine 0390 mg / 24 h , metanephrine 0320 mg / 24 h )  . 
at t1 and t2 , no alteration was observed in microalbumin levels measured on morning urine samples , which remained within the normal range in all patients ( 30300 mg / 24 h , 020 mg / g creatinine )  . discussion chronic overactivity of the sns , in particular of renal sympathetic nerves , plays a pivotal role in the pathophysiology of arterial hypertension , heart failure , chronic renal failure , ischaemic heart disease , diabetes mellitus , obesity and metabolic syndrome [ 7 , 8 ]  . 
the kidneys are innervated mina dei 5 trattati ha riferito dolore viscerale persistente e protrattosi per 12 ore che ha richiesto la somministrazione di farmaci analgesici : tramadolo 50 mg / 2 ml per via endovenosa a 2 ml / min e paracetamolo 1 g . 
il controllo con esame ecd ripetuto a t1 e t2 dalla proce dura non ha mostrato in nessun paziente la presenza di stenosi a livello delle arterie renali trattate con regolari ir mi surati allostio , al terzo medio ed in corrispondenza delle prin cipali diramazioni intraparenchimali , non documentando va riazioni significative rispetto al controllo eseguito in sede pre - procedurale . 
afferent sns nerve fibres originating from the kidneys and heading towards the central nervous system ( cns ) produce excessive stimulation and are responsible for increased heart rate , peripheral vasoconstriction , myocardial contractility and arterial hypertension . 
 efferent nerve endings from the renal sympathetic system release norepinephrine as the main transmitter , which acts by stimulating the alpha - 1 receptors of the smooth muscle cells of the renal arteries , thus inducing contraction of the smooth muscle and consequently vasoconstriction [ 10 , 11 ]  . 
 this leads to reduced renal blood flow , tubular reabsorption of sodium , renin release and raas system activation , as well as to the release of catecholamines and other vasoactive substances all factors that lead to an increase in systemic ap [ 12 , 13 ]  . 
the afferent sensory system plays a major role in communicating changes in pressure and serum electrolytes to the cns [ 14 ]  . afferent nerve endings are chiefly located at the level of the renal pelvis and comprise two classes of receptors : durale . 
dati preliminari , ottenuti ad un iniziale controllo dei valori tensivi effettuato a 4872 ore dalla procedura mediante monitoraggio dinamico della pa nelle 24 ore , hanno mo strato una riduzione dei valori pressori registrati rispetto a t0 . 
 il primo e il secondo follow - up a t1 e t2 hanno confermato una riduzione significativa di pa , nei valori sistolici ( pas ) , diastolici ( pad ) e medi . 
il decremento dei valori di pressione arteriosa media dopo la procedura stato di - 18 / - 5 mmhg e - 13 / - 10 mmhg rispettivamente a t1 e t2 . 
i dosaggi urinari delle catecolamine non hanno mostrato variazioni significative e sono rimasti nel range della normalit in tutti i pazienti ( adrenalina 020 g / 24 h ; noradrenalina 23105 g / 24 h , normetanefrina 0390 g / 24 h , metanefrina 0320 g / 24 h )  . 
tutti i pazienti arruolati non 436 radiol med ( 2012 ) 117 : 426444 mechanosensitive receptors record any change in hydrostatic pressure within the renal arteries , renal veins and renal pelvis , whereas chemosensitive receptors are activated by renal ischaemia and changes in the chemical composition of the renal interstitium and urine produced [ 15 ]  . 
this evidence correlates with an increased risk of hypertension , vascular remodelling , left ventricular hypertrophy , ventricular arrhythmias and sudden cardiac death [ 16 ]  . on the basis of this concept , the use of effective and safe pharmacological therapies capable of reducing sympathetic overactivity has increased progressively . 
the concept of sns denervation arises from extensive surgical sympathectomy techniques dating back to 1930 , which involved the thoracic , abdominal and pelvic sns and were performed as life - saving procedures table 2 study population , follow - up presentavano variazioni della microalbuminuria dosata sul campione urinario delle 24 h . 
a t1 e t2 non sono state osservate variazioni dei valori della microalbuminuria mattutina che si sono mantenuti nel range della normalit ( 30300 mg / 24 h ; 020 mg / g creatinina ) in tutti i pazienti . discussione liperattivazione cronica del sistema nervoso simpatico ( sns ) , in particolar modo dei nervi del simpatico renale , svolge un importante contributo nella fisiopatologia dellipertensione arteriosa , dello scompenso cardiaco , dellinsufficienza renale cronica , della cardiopatia ischemica , del diabete mellito , dellobesit e della sindrome metabolica [ 7 , 8 ]  . 
il rene innervato da una rete di neuroni simpatici postgangliari provenienti dal tratto toracico e lombare ( t10 - l2 ) della colonna vertebrale localizzati nella tunica avventizia della parete delle arterie renali [ 9 ]  . 
fibre nervose afferenti al sns provenienti dai reni e dirette al snc , determinano stimolazioni eccessive e sono responsabili dellincremento della frequenza cardiaca , della vasocostrizione periferica , della bpv ( t0 ) bpv ( t1 ) gfr ( t1 ) ( ml / min ) antihypertensive therapy ( t0 ) antihypertensive therapy ( t1 ) rm 165 / 90 mmhg 170 / 100 mmhg 180 / 100 mmhg 170 / 110 mmhg 170 / 100 mmhg 145 / 80 mmhg 170 / 80 mmhg 165 / 90 mmhgg 130 / 80 mmhg 150 / 90 mmhg 100 angiotensin type 2 receptor blockade calcium channel blockers thiazide diuretics vasodilator therapy alpha 1 blockers ace inhibitor alpha 2 adrenergic agonists beta blockers calcium channel blockers thiazide diuretics angiotensin type 2 receptor blockade alpha 2 adrenergic agonists direct renin inhibitor angiotensin type 2 receptor blockade alpha 1 blockers calcium channel blockers loop diuretics beta blockers angiotensin type 2 receptor blockade thiazide diuretics alpha 2 adrenergic agonists beta blockers loop diuretics calcium channel blockers anviotensin type 2 receptor blockade alpha 1 blockers angiotensin type 2 receptor blockade calcium channel blockers thiazide diuretics vasodilator therapy alpha 1 blockers beta blockers calcium channel blockers angiotensin type 2 receptor blockade direct renin inhibitor angiotensin type 2 receptor blockade alpha 1 blockers calcium channel blockers loop diuretics beta blockers beta blockers loop diuretics calcium channel blockers angiotensin type 2 receptor blockade pt , patients ; t0 , baseline blood pressure values and pharmacological therapy during patient enrolment ; t1 , blood pressure values and pharmacological therapy at 30 - day follow - up ; bpv , blood pressure value ; gfr , glomerular filtration rate ; ace , angiotensin converting enzyme radiol med ( 2012 ) 117 : 426444 tabella 2 popolazione di studio . 
follow - up paziente vp ( t0 ) 165 / 90 mmhg 170 / 100 mmhg 180 / 100 mmhg 170 / 110 mmhg 170 / 100 mmhg ( t1 ) 145 / 80 mmhg 140 / 80 mmhg 165 / 90 mmhg 130 / 80 mmhg 150 / 90 mmhg 100 vgf ( t1 ) ( ml / min ) terapia anti - ipertensiva ( t0 ) terapia anti - ipertensiva ( t1 ) antagonista recettore angiotensina ii calcio - antagonista diuretico - tiazidico vasodilatatori diretti alfa - 1 bloccante ace - inibitore clonidina trans dermica beta - bloccante calcio - antagonista diuretico - tiazidico antagonista recettore angiotensina ii clonidina trans dermica inibitore diretto renina antagonista recettore angiotensina ii alfa - 1 bloccante calcio - antagonista diuretico dellansa beta - bloccante antagonista recettore angiotensina ii diuretico - tiazidico clonidina trans dermica beta - bloccante diuretico dellansa calcio - antagonista antagonista recettore angiotensina ii alfa - 1 bloccante antagonista recettore angiotensina ii calcio - antagonista diuretico - tiazidico vasodilatatori diretti alfa - 1 bloccante beta - bloccante calcio - antagonista antagonista recettore angiotensina ii inibitore diretto renina antagonista recettore angiotensina ii alfa - 1 bloccante calcio - antagonista diuretico dellansa beta - bloccante beta - bloccante diuretico dellansa calcio - antagonista antagonista recettore angiotensina ii t0 , valori basali pressori e terapia farmacologica al momento dellarruolamento dei pazienti ; t1 , valori pressori e terapia farmacologica a 30 giorni dalla procedura ; vp , valori pressori ; vfg : filtrato glomerulare renale ; ace , angiotensin converting enzyme on patients with malignant hypertension [ 17 ]  . 
these techniques were effective in reducing ap , although they were burdened by high perioperative morbidity and mortality rates and often led to long - term complications such as bowel and bladder dysfunction , erectile dysfunction and severe postural hypotension [ 5 ]  . 
since this nerve supply originates from t10l1 and mainly runs along the adventitia , sympathetic nerve ablation at this level can be achieved by using an rf catheter connected to a power generator [ 20 ]  . 
in fact , low - power rf allows ablation and ensuing inactivation of renal sympathetic nerves located at the adventitia level , with selective reduction of both the pathological central activation of the efferent system and the effect of afferent nerves on the hypothalamic centre of sympathetic overactivity . 
the procedure is minimally invasive , requires a short hospital stay , has relatively low hospitalisation contrattilit miocardica e quindi dellipertensione arteriosa . le terminazioni nervose efferenti del sistema simpatico renale rilasciano norepinefrina come principale trasmettitore che agisce attraverso la stimolazione dei recettori alfa1 posti sulle cellule della muscolatura liscia delle arterie renali inducendo la contrazione delle cellule muscolari lisce e quindi la vasocostrizione [ 10 , 11 ] con conseguente riduzione del flusso ematico renale , riassorbimento tubulare del sodio , rilascio di renina e conseguente attivazione del sistema ras , e il rilascio di catecolamine e di altre sostanze vasoattive , tutti meccanismi che portano ad un incremento della pa sistemica [ 12 , 13 ]  . 
il sistema afferente sensoriale gioca un ruolo di primo piano nella comunicazione delle variazioni pressorie e degli elettroliti sierici al snc [ 14 ]  . le terminazioni nervose afferenti sono prevalentemente localizzate a livello della pelvi renale e contengono due classi di recettori . 
i meccano - sensitivi , che registrano i cambiamenti della pressione idrostatica nelle arterie renali , nelle vene renali e nella pelvi urinaria e i chemio - sensibili , che vengono attivati dallischemia renale e dai cambiamenti nella composizione chimica dellinterstizio renale e dellurina prodotta [ 15 ]  . 
t2 , blood pressure values and pharmacological therapy at 60 - day follow - ups ; bpv , blood pressure values ; gfr , glomerular filtration rate tabella 3 popolazione di studio . 
follow - up paziente vp ( t1 ) ( t2 ) vgf ( t2 ) ( ml / min ) terapia anti - ipertensiva ( t1 ) terapia anti - ipertensiva ( t2 ) t1 , valori pressori e terapia farmacologica a 30 giorni dalla procedura . 
t2 , valori pressori e terapia farmacologica a 60 giorni dalla procedura ; vp , valori pressori ; vfg : filtrato glomerulare renale radiol med ( 2012 ) 117 : 426444 fig . 
6a , b paziente r.m. ; a indicazione ai tempi t0 - t1 - t2 di pressione arteriosa sistolica ( pas ) , pressione arteriosa distolica ( pad ) e valore del filtrato glomerulare ( vfg )  . 
 studies are focusing on patients who suffer from refractory hypertension , that is , those unable to achieve acceptable bp pressure levels despite the use of three or more antihypertensive medications ( including a diuretic ) at the highest tolerated doses . two major studies [ 20 , 21 ] paved the way for a new era in treating hypertension . 
7a , b paziente c.m. ; a indicazione ai tempi t0 - t1 - t2 di pressione arteriosa sistolica ( pas ) , pressione arteriosa distolica ( pad ) e valore del filtrato glomerulare ( vfg ) ; b numero di farmaci anti - ipertensivi . 
8a , b paziente r.p. ; a indicazione ai tempi t0 - t1 - t2 di pressione arteriosa sistolica ( pas ) , pressione arteriosa distolica ( pad ) e valore del filtrato glomerulare ( vfg ) ; b numero di farmaci anti - ipertensivi . 
although that study was neither prospective nor randomised , and although it included a markedly heterogeneous population of 50 patients ( five australian and european centres ) , it demonstrated a significant and longlasting decrease in pressure values of patients with uncontrolled hypertension ( sbp 20 / 25 mmhg ; dbp 10 / 15 mmhg ) , as well as a decrease in the systemic levels of un adeguato controllo della pa [ 2 ]  . 
il concetto di denervazione del sistema nervoso simpatico pone le sue radici nelle tecniche chirurgiche di simpaticectomia estesa risalente al 1930 che coinvolgeva il simpatico toracico , addominale e pelvico praticate come intervento salvavita in pazienti con ipertensione maligna [ 17 ]  . 
9a , b paziente g.m. ; a indicazione ai tempi t0 - t1 - t2 di pressione arteriosa sistolica ( pas ) , pressione arteriosa distolica ( pad ) e valore del filtrato glomerulare ( vfg ) ; b numero di farmaci anti - ipertensivi . harmful neurohormones ( norepinephrine ) , which underlie the pathophysiological mechanism leading to hypertension . 
la denervazione localizzata dei nervi del simpatico renale nelluomo , stata ottenuta per la prima volta mediante uno specifico catetere , il sistema symplicity ( ardian symplicity catheter )  . 
poich tale innervazione nasce da d10 - l1 e decorre principalmente lungo lavventizia , lablazione del simpatico a questo livello possibile mediante limpiego di un catetere a rf collegato ad un generatore di energia che ne permette la denervazione [ 20 ]  . 
la rf a bassa potenza consente infatti di ablare e quindi disattivare i nervi del simpatico renale localizzati a livello della avventizia , in modo da ridurre selettivamente sia il patologico azionamento centrale del sistema efferente , sia il contributo delle afferenze sul centro ipotalamico di iperattivit simpatica . 
attualmente lo studio stato indirizzato ai pazienti affetti da ipertensione resistente ovvero pazienti che non sono in grado di raggiungere target pressori accettabili nonostante limpiego di 3 o pi farmaci antiipertensivi ( compreso un diuretico ) alle massime dosi tollerate . 
 [ 20 ] , pone come obiettivo quello di dimostrare la sicurezza e lefficacia del sistema symplicity nel ridurre la pa mediante la denervazione simpatica renale , con un follow - up a 12 mesi . 
 pur non essendo uno studio prospettico n randomizzato e pur includendo una popolazione di 50 pazienti ( 5 centri australiani ed europei ) molto eterogenea , dimostra una significativa e duratura riduzione dei valori pressori in pazienti con ipertensione non controllata dalla terapia medica ( sistolica : - 20 / - 25 mmhg ; diastolica - 10 / - 15 mmhg ) e la diminuzione del livello di neurormoni dannosi ( noradrenalina ) , che sono alla base del meccanismo fisiopatologico dellipertensione , a livello del circolo sistemico . 
il nostro studio nasce dallesigenza di contribuire alla validazione dei preliminari dati attualmente proposti dalla letteratura riguardo la sicurezza e lefficacia della denervazione del simpatico renale mediante approccio percutaneo trans - catetere . 
i risultati clinici da noi ottenuti , sostanzialmente in accordo con i sopracitati gruppi di studio , dimostrano eccellenti effetti in termini di sicurezza procedurale ( la nostra esperienza non evidenzia alcuna complicanza intra - / peri - procedurale ) e di efficacia da parte di tale metodica , nel trattamento di pazienti affetti da ipertensione arteriosa essenziale resistente a terapia farmacologica . 
although the follow - up period was very short , we found no complications at 60 - day follow - up cdus or any stricture at the level of the treated renal arteries , with the renal vascular ri within normal ranges . 
a significant decrease in bp was obtained in all patients , as measured by holter monitoring on the day following the procedure and at t1 and t2 ; in addition , the decrease in the number and dosage requirements of antihycomplicanza , in assenza di stenosi a livello delle arterie renali trattate e con ir vascolare renale nella norma . 
 inoltre , la funzionalit renale non ha mostrato alcun deterioramento , dato confermato dalla mancata variazione del vfg ( valore medio di 91 , 6 ml / min / 173 m2 )  . 
in un solo paziente abbiamo riscontrato linsorgenza di dolore viscerale persistente che si protratto per circa 12 ore , ma che tuttavia stato agevolmente tenuto sotto controllo mediante la somministrazione di farmaci analgesici . 
lottenimento di una riduzione pressoria significativa in tutti i pazienti trattati , valutata mediante misurazione holter della pressione , eseguita il giorno successivo alla procedura ed a t1 e t2 dalla stessa , nonch la riduzione del numero e della posologia dei farmaci anti - ipertensivi somministrati , conferma lefficacia clinica della terapia di denervazione . 
un solo paziente ha mostrato al controllo t1 una iniziale riduzione dei livelli pressori ed un radiol med ( 2012 ) 117 : 426444 pertensive medications confirms the clinical effectiveness of the denervation treatment . 
despite the encouraging immediate clinical response , there is awareness , given previous experience on transplanted kidneys , that the efferent nerves of the renal sympathetic system have the ability to regenerate , which means that the procedure may have limited effectiveness over time . nevertheless , it is also true that the afferent renal sympathetic system is not able to regenerate and that it plays a key role in modulating renal sympathetic activity [ 6 ]  . 
 [ 20 ] , whereby six patients reported either a minimal or no reduction in pressure levels , in our experience , all patients exhibited a decrease in pressure levels compared with t0 . 
in our opinion , this discrepancy may be explained by the small number of patients considered and the short follow - up period , as well as by the fact that in patients not responding to percutaneous denervation , the altered activation of the afferent and efferent renal sympathetic systems may not be the pathophysiological mechanism causing hypertension , as previously reported by krum et al . 
on the other hand , it is not possible at present to reliably identify the factors predicting success of the percutaneous treatment . as reported above , the limitations of our study are the small number of patients treated and the short follow - up period ; furthermore , our study was neither randomised nor prospective . 
the results will be essential to unequivocally establish the role of the approach in treating patients with refractory hypertension and , in the future , those with heart failure and crf , both conditions that have renal sympathetic overactivity as their pathogenetic mechanism . successivo incremento degli stessi in t2 . 
nonostante questa incoraggiante immediata risposta clinica , vi la consapevolezza , data dalle trascorse esperienze sui reni trapiantati , che i nervi efferenti del simpatico renale sono capaci di rigenerarsi dopo insulto , indicando la possibilit che la procedura abbia una efficacia limitata nel tempo . ciononostante altrettanto vero che linterruzione del simpatico renale afferente non risulta in grado di rigenerarsi e che questultimo gioca un ruolo importante di modulazione dellattivit simpatica renale [ 6 ]  . 
 [ 20 ] , in cui in 6 pazienti veniva riscontrata una minima se non assente riduzione dei livelli pressori , nella nostra casistica in tutti i pazienti trattati abbiamo ottenuto una riduzione dei valori pressori rispetto a t0 . 
tale discrepanza di risultati , a nostro avviso , da ricondurre probabilmente alla nostra limitata coorte di pazienti ed al breve follow - up degli stessi nonch al fatto che nei pazienti non rispondenti al trattamento di denervazione percutanea , lalterata attivazione del simpatico renale afferente ed efferente non sia alla base del meccanismo fisiopatologico dellipertensione , come peraltro gi descritto da krum et al . 
daltronde , attualmente non possibile identificare con precisione fattori predittivi di successo del trattamento percutaneo . come gi sopraccitato , i limiti del nostro studio sono da riferire allesiguo numero di pazienti trattati ed al breve periodo di follow - up ad essi dedicato , inoltre il nostro studio non risulta randomizzato n prospettico . 
lattesa di tali risultati sar fondamentale per determinare , in maniera inequivocabile , il ruolo di tale approccio nel trattamento di pazienti con ipertensione refrattaria , ed in futuro anche per il trattamento di pazienti con scompenso cardiaco ed irc , anchesse patologie aventi come meccanismo patogenetico uniperattivit simpatica renale . conclusions conclusioni therapeutic renal denervation is an innovative , rapid , simple and safe percutaneous procedure for treating hypertension in patients who are refractory to conventional pharmacological treatment . 
clinical and procedural effectivela denervazione terapeutica del simpatico renale una procedura percutanea innovativa , rapida , semplice e sicura per il trattamento dellipertensione dei pazienti refrattari alla terapia farmacologica convenzionale . 
lefficacia clinica e 444 radiol med ( 2012 ) 117 : 426444 ness have been demonstrated by the achievement of significant and long - lasting reduction in arterial pressure and the absence of intra - , periand postprocedural complications . 
 although the results of our study are encouraging , further confirmation is required from randomised prospective studies on larger patient series and with longer - term followup periods to definitely validate this method . procedurale stata dimostrata dal raggiungimento di significative e durature riduzioni della pressione arteriosa nella popolazione di studio , in assenza di complicanze intra - / perie post - procedurali . 
vermiglio1 1environmental , health , social and industrial department , university of messina , policlinico universitario torre biologica , viale gazzi , 98125 messina , italy 2department of electronic and electrical engineering , university of bath , bath ba27ay , uk 3department of experimental medicine , university of insubria , viale borri 57 , 21100 varese , italy correspondence to : g . 
in all cases , there was no statistically significant variation between the two different procedures and the lv procedure , which can therefore be proposed as a valuable alternative to other commonly used procedures and be reliably used on any ct and mri scanner . keywords quality control computed tomography magnetic resonance slice thickness riassunto obiettivo . 
un parametro di fondamentale importanza da monitorare durante i controlli di qualit sulle apparecchiature di tomografia computerizzata ( tc ) e di risonanza magnetica ( rm ) rappresentato dallaccuratezza dello slice thickness ( st ) , per la cui verifica i protocolli standard richiedono procedure complesse e fantocci dedicati . 
pertanto , pu essere proposta come una valida alternativa alle procedure comunemente adottate ed utilizzata indifferentemente in tc ed rm . parole chiave controlli di qualit tomografia computerizzata risonanza magnetica spessore dello strato 508 introduction the main goal of a medical imaging system is to produce images that allow accurate and timely diagnoses [ 1 ]  . 
in this context , to guarantee the maintenance of consistent image quality over the lifetime of the radiological equipment and to ensure safe and accurate operation of the process as a whole , it is necessary to establish and actively maintain regular and adequate quality - assurance ( qa ) procedures . 
any qa programme should include periodic tests to identify any degradation in image quality [ 3 ] , which reduces the ability to detect and correctly interpret abnormal findings , which means a decrease in accuracy and overall diagnostic confidence . 
such tests , known as quality control tests ( qcs ) , play a key role within the qa procedure because they enable complete evaluation of system status and image quality [ 4 , 5 ]  . 
importantly , qcs permit identification of image quality degradation before it affects patient scans and of the source of possible equipment malfunction , pointing to preventive or immediate maintenance requirements . 
protocols for qcs and qa in medical imaging systems have been produced by several professional groups [ american association of physicists in medicine ( aapm ) ; national electrical manufacturer association ( nema ) ] [ 7 ]  . 
in particular , accuracy of the slice thickness represents an important parameter that should be estimated during qc procedures , not only because the signal - to - noise ratio ( snr ) varies linearly with slice thickness , but also because clinical image resolution is strongly affected by partial volume effect , thus reducing clinical image quality with increasing slice thickness [ 8 ]  . 
28 state that the slice thickness can be evaluated starting from the measure of the full width at half maximum ( fwhm ) of the response across the slice [ 9 , 10 ]  . 
devised a system providing an approximate measurement of beam width consisting of a series of small beads angled across the beam width at a distance < 1 mm from one another . 
beam width ( fwhm ) can be measradiol med ( 2012 ) 117 : 507518 introduzione lo scopo di unimportante categoria di dispositivi di diagnostica strumentale quello di produrre immagini in grado di fornire informazioni quanto pi precise e accurate [ 1 ]  . 
in particolare , la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm ) possono essere considerate tra le tecniche di imaging pi sofisticate , nonch tra le pratiche strumentali attualmente pi utilizzate nella attivit di diagnostica clinica [ 2 ]  . 
tali procedure includono la conduzione di test periodici , finalizzati allindividuazione di possibili degradazioni nella qualit dellimmagine [ 3 ] , cosa che implica una minore capacit di identificare ed interpretare correttamente reperti patologici , con conseguente riduzione dellaccuratezza e della confidenza diagnostica complessiva . 
i test indicati con il termine controlli di qualit ( cq ) , giocano un ruolo chiave allinterno delle procedure di qa , poich sono in grado di fornire una completa valutazione dello stato dellapparecchiatura e dellimmagine , che essa fornisce [ 4 , 5 ]  . 
 per tale motivo leffettuazione dei cq raccomandata sia dai costruttori delle apparecchiature che dalle organizzazioni professionali dei fisici medici ( american association of physicists in medicine , aapm ; national emergency medicine association , nema ) [ 7 ]  . infatti , nella conduzione di un qualunque studio clinico , risulta indispensabile verificare in maniera accurata le caratteristiche fisiche dei dispositivi di imaging . 
in particolare , laccuratezza dello spessore dello strato costituisce un importante parametro da valutare durante lespletamento dei cq , non solo perch il rapporto segnale - rumore direttamente proporzionale allo spessore dello strato , ma anche perch la risoluzione dellimmagine risulta fortemente influenzata dalleffetto di volume parziale : pertanto , un aumento dello spessore dello strato influisce negativamente sulla qualit dellimmagine clinica [ 8 ]  . 
i report dellaapm n 1 e n 28 evidenziano come lo spessore dello strato possa essere determinato a partire dalla misura della larghezza a met altezza del massimo ( fwhm ) della funzione di risposta dellintera fetta selezionata [ 9 , 10 ]  . 
hanno realizzato un sistema per fornire una sua valutazione approssimata che consiste in una radiol med ( 2012 ) 117 : 507518 ured directly from a beam profile plot if care is taken to ensure the aluminium piece is oriented at 45 across the width of the beam [ 9 ]  . 
another typical test object for evaluating slice thickness is the crossed high - signal ramps oriented at a fixed angle [ 10 ]  . however , most ct and mri scanners adopt specific automated procedures that require the use of dedicated phantoms , often provided with the scanners , coupled with dedicated imaging software tools that do not include the line profile tool . 
furthermore , even the newest medical imaging software packages do not allow direct measurement of slice thickness accuracy with ct and mri scanners but require a complicated procedure to be performed by the manufacturers technicians , who are authorised to access the service menu of the medical device . to simplify procedures and provide a versatile and unique qc procedure to estimate slice thickness accuracy , we propose a novel dedicated phantom and associated procedure that is easy to implement and that can be used on both ct and mri scanners . 
the phantom can be used either with already existing dedicated software or with simple labview - based tools to readily measure slice thickness in real time and / or during postprocessing . 
the reliability of this innovative technique was evaluated with respect to previously validated procedures by conducting statistical analysis , as discussed in detail in the following sections . materials and methods the method developed to determine slice - thickness accuracy using the novel phantom proposed here consists of two steps : ( 1 ) acquisition of images of the phantom using ct and mri scanners ; ( 2 ) image processing using the dedicated labview - based software . 
to test the procedure and obtain detailed information about the quality of the results , the images acquired and processed were compared with those obtained by processing the same phantom images with commercial software following validated procedures [ 11 ]  . 
to determine slice - thickness accuracy , the pmma box was filled with two different fluids water and air for assessment in a ct scanner ; for mri assessment , water was replaced with a cuso4 5h2o + h2so4 + 1ml / l antialga ( arquad ) liquid solution ( t1 = 300 ms , t2 = 280ms )  . 
a spirit level was used to serie di piccole sferette posizionate ad un angolo fissato rispetto alla direzione del fascio incidente e separate le une dalle altre di meno di 1 mtuttavia , il fantoccio realizzato risulta molto complicato da utilizzare per la misura quantitativa dello spessore della fetta irraggiata . 
la larghezza del fascio pu alternativamente essere direttamente misurabile a partire dal grafico del profilo della fetta , se si ha cura di realizzare un sistema in cui una rampa di alluminio forma un angolo di 45 gradi con la larghezza del fascio [ 9 ]  . 
unaltra tipologia di oggetto test che ad oggi viene normalmente utilizzato per la valutazione dello spessore dello strato consiste in un fantoccio che include una doppia rampa incrociata orientata ad un angolo fisso [ 10 ]  . 
 tuttavia la maggior parte degli scanner tc e rm oggigiorno si avvalgono di specifiche procedure automatizzate che richiedono limpiego di fantocci dedicati , i quali spesso vengono forniti unitamente alle apparecchiature , accoppiati con software proprietari che , fra laltro proprio di recente , hanno rimosso lo strumento per la determinazione del profilo della linea . 
ad aumentare le difficolt che si incontrano nel condurre questo tipo di operazioni , i software che ultimamente vengono forniti in dotazione alle apparecchiature non consentono una misura diretta dellaccuratezza dello spessore dello strato , ma richiedono una procedura complicata che pu essere effettuata solo da personale tecnico della casa costruttrice autorizzato ad accedere al men di service dellapparecchiatura stessa . al fine di semplificare le procedure e di fornire una metodologia che permetta la valutazione dello spessore dello strato , indifferentemente sugli scanner tc e rm , stato realizzato da parte degli autori un nuovo fantoccio dedicato , il quale pu essere utilizzato sia con i software in dotazione allapparecchiatura , sia accoppiato con il software dagli stessi appositamente realizzato in ambiente labview , in maniera tale che lo spessore dello strato possa indifferentemente essere misurato in tempo reale o in post processing . 
 la tecnica innovativa qui descritta stata successivamente confrontata con altre procedure gi validate in precedenza , ed stata anche sottoposta ad analisi di natura statistica al fine di valutare laffidabilit della tecnica stessa . materiali e metodi la metodologia sviluppata per la determinazione dellaccuratezza dello spessore dello strato , che utilizza il fantoccio di nuova realizzazione qui presentato , si sviluppa in due passi successivi : ( 1 ) acquisizione delle immagini del fantoccio ; ( 2 ) elaborazione delle immagini utilizzando lapposito software realizzato in ambiente labview ( lv )  . 
1 fantoccio ( a ) realizzato per la determinazione dellaccuratezza dello spessore dello strato completo di livella ( b ) utilizzata per la verifica della corretta planarit del fantoccio rispetto al fascio ed al lettino . check the planarity of the phantom with respect to the beam and the patient couch . 
scanning the phantom with a single slice of known thickness . the phantom images were acquired using standard head and body protocols , shown in tables 1 and 2 for ct and mri devices , respectively . 
images were then acquired , processed , analysed and transferred to a storage or printtable 1 standard protocol for testing ct medical devices scan parameters head protocol body protocol scan time ( s ) fov ( mm ) reconstruction matrix filter 120 100 230 512 none none tabella 1 protocollo utilizzato per i test su tomografi tc parametri di scansione protocollo testa protocollo corpo tempo di scansione ( s ) fov ( mm ) matrice di ricostruzione filtro 120 100 230 512 nessuno nessuno sulla bont dei risultati , i dati ottenuti dalle immagini acquisite e successivamente processate sono stati confrontati con quelli ricavati tramite lelaborazione delle medesime immagini facendo ricorso a software commerciali e procedure gi precedentemente validate [ 11 ]  . il fantoccio realizzato consiste in una scatola vuota di polimetilmetacrilate ( pmma ) avente dimensioni 14 , 0 cm7 , 5 cm7 , 0 cm , diagonalmente divisa in due sezioni da un setto sempre di pmma ( dello spessore di 2 mm ) e che forma un angolo di 26 gradi con il piano su cui ruota il fascio incidente . 
in particolare per determinare laccuratezza dello spessore dello strato , la scatola di pmma stata riempita con due differenti fluidi : acqua / aria nel caso di scanner tc , aria / soluzione liquida contenente cuso4 5h2o + h2so4 + 1 ml / l antialga ( arquad ) ( t1 = 300 ms , t2 = 280 ms ) nel caso di scanner rm . 
scansione del fantoccio impostando una singola fetta di spessore noto . le immagini del fantoccio sono state acquisite impostando i protocolli standard head e body illustrati in tabella 1 e 2 per le apparecchiature tc e rm rispettivamente . 
 radiol med ( 2012 ) 117 : 507518 table 2 standard protocol for testing magnetic resonance imaging ( mri ) medical devices scan parameters head protocol body protocol coil type scan mode scan technique slice orientation number of echoes fov ( mm ) repetition time ( ms ) scan matrix reconstruction matrix water fat shift ( pixels ) head transversal 250 1 , 000 256 256 1.3 body transversal 1 , 000 maximum se , spin echo ; ms , multislice ; fov , field of view tabella 2 protocollo utilizzato per i test su tomografi rm parametri di scansione protocollo testa protocollo corpo testa tipo di bobina modo di scansione tecnica di scansione trasversale orientamento della fetta numero di echi fov ( mm ) 250 tempo di ripetizione ( ms ) 1000 256 matrice di scansione matrice di ricostruzione 256 shift acqua - grasso ( pixels ) 1 , 3 corpo trasversale 1000 massimo se , spin echo ; ms , multistrato ; fov , field of view ing device . 
stored images were subsequently transferred to a dedicated workstation , whereas printed images were acquired by the same workstation using a vidar scanner for further processing . the method developed for data processing uses a software for slice thickness measurement purposely developed for a labview environment . 
to evaluate slice width , the fwhm of the wedge , expressed in pixels , is measured and calibrated with respect to the effective length of the pmma box , expressed in millimetres . 
for slice - thickness evaluation , the software uses the following equation in real time : st = fwhmtan ( 26 )  . successivamente le stesse immagini sono state acquisite , elaborate ed analizzate , e quindi inviate ad un dispositivo di memorizzazione e / o ad una stampante . 
le immagini su supporto fisso sono quindi state trasferite ad un elaboratore dedicato , mentre le immagini stampate sono state acquisite dalla stessa work station mediante uno scanner vidar per la successiva elaborazione . 
il software in grado di leggere immagini sia in formati standard che non ( bmp , tiff , jpeg , jpeg2000 , png , e aipd ) [ 12 ]  . 
per determinare laccuratezza dello spessore dello strato delle immagini acquisite il software dedicato fornisce in forma grafica il profilo della fetta irraggiata , che descrive la risposta del sistema ad un impulso attenuante in funzione della posizione lungo lasse z , attraverso il piano della fetta selezionata . 
 per la valutazione quantitativa dello spessore dello strato il software utilizza la seguente equazione : st = fwhmtan ( 26 ) i risultati riportati sono relativi a misure condotte , in un intervallo di tempo che va dal 2006 al 2010 , su diversi scanner tc e rm . 
per validare la procedura proposta , i risultati sono quindi stati paragonati con quelli ottenuti elaborando le stesse immagini , ma utilizzando un software commerciale , quale il software image pro plus ( ipp ) della media cybernetics [ 11 , 13 ] , mentre per supportare laccuratezza della procedura stata inoltre condotta unindagine statistica . 
 nello specifico il metodo scelto stato lanalisi delle varianza attraverso il test di fisher ( f - test ) , al fine di verificare se esiste una differenza significativa tra i set di dati ottenuti utilizzando le diverse metodologie di misura [ 14 ]  . 
il test di fisher molto utile ogni qual volta lobiettivo dello studio la valutazione di un tecnica di misurazione : infatti , lanalisi della varianza consiste nella fattorizzazione della varianza totale in un insieme di varianze parziali . 
il primo riferito ad un valore di riferimento ( rf ) dello spessore dello strato di 10 mm e sono riportate un totale di 16 misure , ottenute utilizzando le due differenti procedure , il secondo riguarda un rf di 5 mm ed interessa 14 misure in totale . 
2a - c front panel of the dedicated slice - thickness measurement labview software showing x - ray phantom section ( a ) , the detected line profile and corresponding gaussian fit ( b ) and the resulting slice thickness value ( c )  . 
sezione del software riservata alla visualizzazione dellimmagine acquisita ( a ) ; profilo della linea e corrispondente fit gaussiano ( b ) e accuratezza dello spessore dello strato cos come determinato dal software ( c )  . eral ct and mri devices in an extended study from 2006 to 2010 . 
to test the procedure , results were compared with those obtained by processing the same phantom images with the commercial software image - pro plus from media cybernetics [ 11 , 13 ]  . statistical analysis was conducted on the resulting data sets to further validate the proposed methodology . 
analysis of variance using fishers exact test ( f - test ) was used to assess whether a significant difference existed between data sets obtained following different procedures [ 14 ]  . 
the first is referred to a reference ( rf ) value of 10 mm , and 16 measurements obtained using two different procedures are reported ; the second refers to an rf value of 5 mm , with 14 measurements reported . for mri equipment , slice - thickness measurements refer to an rf value of 10 mm ; in this case , three different procedures were compared , so that 24 measurements were conducted on three different mri scanners . results results of slice - thickness measurements using the proposed si riferiscono ad un rf di 10 mm ; in questo caso , per , sono state comparate tre differenti procedure per un totale di 24 misure . in questa sezione vengono presentati i risultati relativi alle misure dellaccuratezza dello spessore dello strato condotte con lutilizzo del fantoccio di nuova realizzazione . risultati scanner tc unimmagine bidimensionale del setto presente nel fantoccio realizzato e raffigurato in figura 1 , stata acquisita utilizzando lo standard head protocol riportato in tabella 1 . 
 in questo caso lo strumento per tracciare il profilo della linea era presente e landamento dello stesso mostrato nella stessa figura . i risultati ottenuti dalla misura dellaccuratezza dello spessore dello strato mediante lutilizzo del software sviluppato in ambiente lv e del software commerciale image pro plus ( ipp ) , e riferiti al corrispondente rf , sono riportati in tabella 3 ; gli stessi sono presentati in forma grafi ca in figura 4 , dove possibile osservare il confronto tra i risultati relativi alla misura dellaccuratezza dello spessore dello strato ( ipp : tonalit chiara , lv : tonalit scura ) e lo scarto dal valore di riferimento ( ipp : quadrato , lv : cerchio ) ottenuti mediante le procedure ipp e lv , per i varadiol med ( 2012 ) 117 : 507518 methodology and statistical data analysis are presented for both ct and mri devices . ct medical devices a two - dimensional image of the wedge of the dedicated phantom in figure 1 was acquired using the standard head protocol described in table 1 . 
figure 3 shows the x - ray imlori di riferimento di 10 e 5 mm rispettivamente . nella tabella 4 vengono mostrati i valori medi e le deviazioni standard ottenuti analizzando gli insiemi dei dati con le due differenti procedure . 
daltro canto per , le due deviazioni standard sono considerevolmente differenti : in particolare , la deviazione standard calcolata per la tecnica lv risulta essere pi piccola , a significare che le misure ottenute con tale procedura sono decisamente pi accurate . dallanalisi statistica condotta sui dati mostrati nella tabella 3 emerso un valore di f calcolato ( fc ) pari a fc = 0 , 011 e fc = 0 , 332 rispettivamente per rf di 10 mm e 5 mquesti valori sono stati confrontati con quelli tabulati per un livello di confidenza p = 0 , 05 ( ft = 4 , 54 nel caso di un rf pari a 10 mm ed ft = 4 , 67 nel caso di un rf uguale a 5 mm )  . 
quindi lanalisi statistica ha confermato che , in entrambi i casi , non esiste una variazione statisticamente significativa tra le due diverse procedure adottate . scanner rm le immagini del cuneo del fantoccio realizzato sono state acquisite utilizzando lo standard head protocol riportato in tabella 2 . 
i risultati ottenuti , mediante le tecniche ipp e lv , per la valutazione dellaccuratezza dello spessore dello strato sono riportati in tabella 5 e si riferiscono tutte ad un rf di 10 min questo caso laccuratezza dello spessore dello strato stata misurata anche mediante i software proprietari in dotazione ai tomografi rm ( cs )  . 
 results obtained by measuring the slice - thickness accuracy with different ct scanners and by employing the labview , developed in - house , and the commercial image pro plus ( ipp ) software are compared , with the corresponding rf values , in table 3 and presented in graphical form in figure 4 . 
however , most importantly , the sd obtained from the two procedures is considerably different , with the labview procedure providing a narrower deviation and hence a more accurate measurement . statistical analysis conducted on the data sets shown in table 3 yielded f - values equal to fc = 0.011 and fc = 0.332 for rf values of 10 mm and 5 mm , respectively . 
these fvalues were then compared with the tabulated values for the p = 0.05 confidence level ( ft = 4.54 for the rf value of 10 mm and ft = 4.67 for the rf value of 5 mm )  . 
valori alterati dello spessore dello strato possono inoltre determinare uninterferenza tra due fette successive durante acquisizioni multi - slice , che possono condurre ad una misura non corretta del rapporto segnale / rumore . 
per quanto concerne , invece , le apparecchiature tc , la misura dellaccuratezza dello spessore dello strato rappresenta un elemento importante durante lespletamento dei cq , dal momento che da essa dipende in modo stringente lanalisi quantitativa condotta sugli scanner tc . 
pertanto , stata qui illustrata una procedura alternativa sviluppata dagli autori , che si basa sullimpiego di un fantoccio dedicato , appositamente concepito , accoppiato con un software dedicato dagli stessi realizzato in ambiente labview , concepita per risultare al contempo solida , attendibile e , soprattutto , utilizzabile indifferentemente sulle apparecchiature tc ed rm . 
il nuovo fantoccio per la determinazione dello spessore dello strato qui proposto ed in associazione al software a tal fine sviluppato , permette di ottenere una determinazione quantitativa automatizzata di tale parametro , in modo semplice ed , allo stesso tempo , accurato . 
4a - d comparison between results of slice - thickness accuracy [ lighter shading image pro plus ( ipp ) ; darker shading labview ( lv ) ] refers to a reference ( rf ) value of 10 mm ( a ) and 5 mm ( b )  . 
4a - d confronto tra i risultati ottenuti per la determinazione dellaccuratezza dello spessore dello strato determinato con la metodologia ipp ( bianco ) e con la nuova procedura lv ( grigio )  . 
confronto , riferito allo spessore di strato nominale ( rf ) pari a 10 mm ( c ) e 5 mm ( d ) , tra le deviazioni rispetto al valore di riferimento ottenute utilizzando le due differenti metodiche ( quadrato vuoto : ipp ; cerchio vuoto : lv )  . mri medical devices two - dimensional images of the wedge of the dedicated phantom were acquired using the head protocol reported in table 2 . 
the preliminary results obtained using the ipp and labview procedures applied to mri are reported in table 5 for the rf value 10 m in this case , slice - thickness accuracy measured using in - built mri software ( cs ) is also included . 
as evident utilizzato un setto dello spessore di 2 mm , tuttavia , sono in fase di realizzazione delle modifiche che intendono ridurre tale spessore , in modo da poter valutare lo spessore dello strato anche sulle apparecchiature tc elicoidali , nelle quali possono essere facilmente impostate larghezze della fetta inferiori a 2 mm . la deviazione standard ottenuta con la procedura alternativa risulta pi bassa rispetto a quella che stata ottenuta facendo ricorso ad altre metodiche di misura gi in precedenza validate ( ad esempio , mediante il software ipp )  . 
 questa nuova procedura per la valutazione dellaccuratezza dello spessore dello strato proposta in alternativa alle tecniche comunemente utilizzate , le quali fanno tipicamente uso di software e fantocci dedicati distribuiti unicamente dai costruttori per una specifica apparecchiatura di ima516 radiol med ( 2012 ) 117 : 507518 from data in table 7 , the calculated f value is significantly smaller than the tabulated value at p = 0.05 confidence level in all cases . 
moreover , slice - thickness accuracy is an important element in the qc programme for ct scanners , because quantitative ct analysis is heavily dependent on slice - thickness accuracy . 
therefore , to provide an adaptable , reliable and robust procedure to evaluate slicethickness accuracy , we developed propose a novel , dedicated phantom and corresponding labview - based procedure tabella 4 valori medi e deviazione standard ottenuti con le tecniche image pro plus ( ipp ) e labview ( lv ) per i valori di riferimento ( rf ) di 10 e 5 mm valore rf ( mm ) ipp ( mm ) lv ( mm ) 9 , 641 , 26 4 , 830 , 41 9 , 690 , 68 4 , 730 , 25 ging . 
la tecnica qui proposta utilizza un nuovo fantoccio , accoppiato con un software appositamente sviluppato in ambiente labview , e pu essere indifferentemente adottata sia su scanner tc che rm , in maniera semplice , veloce e riproducibile . la facilit e lapplicabilit della procedura illustrata stata supportata da prove quantitative , utilizzando differenti procedure testate su diversi scanner tc e rm . 
6a comparison between results of slice - thickness accuracy related to the 10 - mm reference ( rf ) value , determined directly at the equipment console and measured using the image pro plus ( ipp ) and labview ( lv ) procedures . 
6a confronto tra i risultati ottenuti per la determinazione dellaccuratezza dello spessore dello strato determinato con le due diverse metodologie : ipp ( bianco ) e lv ( grigio scuro )  . 
b confronto tra le deviazioni rispetto al valore di riferimento ottenute utilizzando le tre differenti metodiche ( quadrato vuoto : ipp ; cerchio vuoto : lv ; croce : cs )  . 
preliminary studies were conducted using the 2 - mm septum because the z - axis dimensions for rotating anode x - ray tube foci are typically less than this value . 
however , it is our intention to reduce the septum width in order to evaluate slice thickness for helicoidal ct scanners , as well , which can reach slice widths < 2 mm . the accuracy ( sd ) obtained with the proposed novel table 6 mean reference ( rf ) valuesstandard deviations obtained from data presented in table 5 for the three different procedures ( 10 - mm rf value )  . 
this new procedure for determining slice - thickness accuracy is proposed as an alternative to the commonly adopted procedures , which are typically complicated by the use of ad hoc software and phantoms distributed by manufacturers and specific to the medical equipment . 
the proposed method employs a new , universal phantom coupled with a dedicated labview - based software that can be used on any ct and mri scanner in a quick , simple and reproducible manner . the ready availability and applicability of the proposed procedure has been validated by quantitative tests using several different medical devices and procedures . 
bazzocchi doctor - patient communication in radiology : a great opportunity for future radiology la comunicazione verbale medico - paziente in radiologia : una grande opportunit nel futuro della radiologia institute of diagnostic radiology , university of udine , p.le santa maria della misericordia 15 , 33100 udine , italy correspondence to : m . 
patients , who are becoming better informed and more aware about medical issues , have a right to be given a timely diagnosis and want to receive as much information as possible from the radiologist . 
better interaction with the patient helps to build a closer , more trusting , relationship with the result that the radiologist will be more motivated in his or her work . 
it is important to emphasise the need for more specific and practical training in this respect , which is indispensable for future developments of the discipline . riassunto nel presente testo vengono discussi gli aspetti relativi alla comunicazione medico - paziente in radiologia : le origini , i vantaggi , gli aspetti etici e legali . 
viene enfatizzata la necessit di una preparazione pi specifica ed eminentemente pratica , imprescindibile negli sviluppi futuri della disciplina . keywords communication radiology physician - patient relations parole chiave comunicazione radiologia rapporto medico - paziente introduction introduzione genesis 1 ( 3 , 4 ) : and god said let there be light genesi 1 ( 3 , 4 ) : e dio disse sia la luce the first verses of the bible state that god said and that each phase of creation essentially came in to being through nei primi versi della bibbia si legge che dio disse e che alla sua parola sostanzialmente fecero seguito le diverse 340 radiol med ( 2012 ) 117 : 339353 gods word . 
i therefore like to think that speech the word is the divine element within humans . speech is therefore also a vital component of the radiologists profession , and specifically in the field of doctorpatient communication . 
and yet , most meetings on communication deal with issues concerning the written report , nowadays structured and undoubtedly evolved compared with the past partly the result of information technology but nonetheless still a written report . 
there are good reasons to believe that written communication cannot be considered sufficient and that verbal communication will become increasingly central to the development of the modern radiologist [ 13 ]  . if we look at the patients healthcare journey from the time of the request for a radiological investigation to when the report and images are delivered , we find a number of situations in which any form of communication other than verbal is insufficient . 
this survey found that despite the wealth of health information accessible through the thousands of media available today , only 22% of users consider themselves to be adequately informed [ 4 ]  . 
one of the most tangible problems of modern radiology with its dramatic technological progress lies in the radiologists loss of visibility ( increasingly faceless , having no contact with the patient ) , an aspect well captured by glazer and ruizwibbelsmann in their description of the invisible radiologist working behind the machines or even in distant offices [ 3 ]  . 
il prologo del iv vangelo ( giovanni 1 , 1 - 18 ) presenta la figura del verbo ( logos ) come colui che era in principio , che era presso dio ed era dio ( giovanni 1 , 1 )  . dunque mi piace pensare che sia proprio la parola lelemento divino che realmente caratterizza luomo . 
 eppure la gran parte dei convegni di comunicazione si preoccupano di trattare le problematiche del referto scritto , ora strutturato e indubbiamente evoluto , grazie anche allo sviluppo dellinformatica , rispetto al passato , ma pur sempre scritto . 
esistono fondati motivi per ritenere che non ci si possa accontentare della sola comunicazione scritta , ma che la comunicazione verbale vada a rivestire un ruolo determinante nello sviluppo del radiologo moderno [ 13 ]  . se analizziamo il percorso che il paziente compie dal momento in cui viene formulata la richiesta di unindagine radiologica alla consegna del referto e delle immagini relative esistono tutta una serie di situazioni nelle quali le forme di comunicazione diverse dalla parola , ovvero dalla comunicazione verbale , non sono sufficienti . 
tale disagio del paziente stato anche sottolineato da una ricerca del censis , settore ricerca biomedica , in un convegno tenutosi a roma nel 2007 , dove si evidenziato che , a fronte di una massa enorme di informazioni sanitarie che pervengono attraverso i mille veicoli mediatici oggi a disposizione , solamente il 22% degli utenti si ritiene sufficientemente informato [ 4 ]  . analizziamo i diversi punti : 1 . 
il paziente gi nella fase di prenotazione si interroga , spesso sollecitato dal medico prescrivente , se la prescrizione di indagine a lui fornita sia la migliore per il suo problema . 
raccontava il giornalista tiziano terzani che grazie ad unattenta diagnosi operata da un medico radiologo newyorchese , durante uno dei suoi tanti ricoveri per problematiche oncologiche , ne ricav un cospicuo giovamento in termini di vita sia qualitativamente che quantitativamente , ma lo stesso affermava di non aver potuto manifestare la propria riconoscenza per non aver mai avuto loccasione di incontrare e vedere il radiologo . 
una delle problematiche pi reali della radiologia moderna consiste a fronte di uno sviluppo tecnologico eccezionale in una perdita della visibilit del radiologo radiol med ( 2012 ) 117 : 339353 practices and clearly does not apply to imaging techniques performed by the radiologists themselves , such as ultrasound , breast imaging , biopsy techniques and interventional procedures . 
the written report , whether structured or otherwise , is mostly incomprehensible to patients , even though the situation has considerably improved and radiologists have stopped using purposefully cryptic and indecipherable terms . 
on the other hand , reports often refer to international classifications [ breast imaging reporting and data system ( bi - rads ) [ 5 ] , or the bosniak classification for renal masses [ 6 ] , etc . ] , which may be useful to the doctor but are no less obscure and unsettling for the patient . 
even though the shift towards an increasingly quantitative and epicritic as opposed to descriptive and qualitative radiology is a prerequisite for providing objective , measurable and comparable data , it does not help improve the patients understanding of the purely technical content . 
it requires a careful analysis , such as the one that led glazer and ruiz - wibbelsmann to advocate a patient - centred , personalised radiology and a new culture of improved healthcare , where radiology is no longer just a service [ 1 , 3 ]  . 
still , tamburrini [ 7 ] warns us of the possible dichotomy between technology ( radiologist increasingly expert and knowledgeable about technology ) and communication ( less knowledgeable but a better communicator )  . 
the issue of complexity , particularly felt in the western world due to the pressure of many stakeholders ( electromedical , pharmaceutical industry , physicians themselves , etc . ) , was well analysed and taken apart by atul gawande in his special lecture at radiological society of north america ( rsna ) 2010 in chicago titled real reform : facing the complexity of health care [ 8 ]  . 
 but who is to take on this role of gatekeeper ? is it enough to indicate it in the structured report ? often , the patient feels lost and confused , particularly when faced with a diagnosis perceived as fatal , and it becomes extremely difficult to find the way through the diagnostic and thera ( radiologo sempre pi faceless , senza faccia , senza contatto con il paziente ) , aspetto ben descritto da glazer e ruiz - wibbelsmann nel loro radiologo invisibile che opera dietro le macchine o addirittura lontano [ 3 ]  . 
il referto scritto , strutturato o meno , perlopi in larga parte incomprensibile al paziente , anche se , oggi , le cose sono decisamente migliorate rispetto al passato e si abbandonata da tempo quella terminologia scritta che era appositamente criptica per risultare indecifrabile . 
in compenso oggi molto spesso adottiamo delle classificazioni internazionali ( breast imaging reporting data system , bi - rads [ 5 ] , o quella di bosniak per le masse renali [ 6 ] , ecc . ) che risultano altrettanto oscure e inquietanti per il paziente , anche se straordinariamente utili per il medico . 
il passaggio ad una radiologia sempre pi quantitativa ed epicritica , invece che descrittiva e qualitativa , se da un lato rappresenta una necessit , al fine di fornire dati oggettivi misurabili e confrontabili nel tempo , dallaltro non riduce lincomprensione che il paziente nutre per i suoi contenuti squisitamente tecnici . 
il problema non si riduce con dei semplici atti formali , come ribadisce oscar tamburrini [ 7 ] ( consenso firmato = consenso informato ) , ma da unattenta analisi che portano gary glazer e julie ruiz - wibbelsmann a sostenere la necessit di una radiologia centrata sul paziente , personalizzata e quindi a sostenere il dovere di creare una nuova cultura che condizioni il sistema sanitario , dove la radiologia non sia mero servizio [ 1 , 3 ]  . 
 sempre tamburrini [ 7 ] ci mette in guardia sulla possibile dicotomia fra tecnologia ( radiologo sempre pi ricco di conoscenze tecnologiche e informato ) e comunicazione ( radiologo pi comunicatore , ma meno informato )  . 
tale problema , presente nel mondo occidentale spesso per la spinta di numerosi stake - holders ( industria elettromedicale , farmaceutica , gli stessi medici ecc . ) , stato ben analizzato e smontato da atul gawande nella special lecture al rsna 2010 di chicago : real reform : facing the complexity of health care [ 8 ]  . 
molto spesso , inoltre , lindagine diagnostica non conclusiva , ma da richiedere la consulenza di un determinato specialista per completare la diagnosi o per impostare la terapia pi corretta . 
as a result , the patient needs to be guided , almost taken by the hand and led in the right direction through this personal hell , just as virgil led dante through the circles of hell in the divine comedy . 
sherman [ 12 ] the ethical principle of an increasingly patient - centred medicine and heightened patient awareness that allows patients to make guided but autonomous decisions has been established by the latest versions of the 1998 italian code of ethics [ 13 ]  . 
the concept had been expressed by the remarkable intuition of mayo more than a century ago and then restated by robert sherman more than 50 years ago in relation to the radiologist being considered the doctors doctor [ 14 ] ; that is , the professional who was meant to serve another professional and report to that professional alone . 
in this scenario , the self - referred patient enters an unwritten contract with the radiologist and demands that the response be given to himself / herself or to a trusted person . in parallel , a culture of prevention has developed , which in radiology has translated into screening mammography . 
 in this case , the subject is a healthy individual in whom the test and the wait for the answer create a state of anxiety ; the subject wants to know the outcome of the test as soon as possible , even though the most likely result is negative . 
in this regard , the mammography quality standards act ( mqsa ) [ 15 ] , introduced into us law on 27 october 1992 , strongly recommended communicating as soon as possible any doubtful or suspicious result from screening mammography . 
the concern at the time perhaps had more to do with insurance problems than ethical issues , as it emerged that several malpractice lawsuits had been filed turato ? molto spesso il paziente spaesato e confuso soprattutto di fronte ad una diagnosi che venga percepita come infausta e quindi in estrema difficolt nel trovare la via per proseguire il suo iter diagnostico e terapeutico . 
quindi si intravede la reale necessit che il paziente venga guidato , quasi preso per mano , e condotto nella giusta direzione come virgilio guidava dante nella divina commedia attraverso i gironi infernali , dato che il paziente in determinate circostanze vive il suo personale inferno in quel momento . in ultima analisi sono molti gli interrogativi e le problematiche che entrano in gioco , che giustificano il perch comunicare , e richiedono che cosa e quando comunicare , come comunicare . 
sherman [ 12 ] il concetto etico di una medicina sempre pi pazientocentrica e orientata verso la consapevolezza del paziente in grado di operare scelte guidate ma autonome , sancito dallultima versione del codice etico nazionale del 1998 [ 13 ]  . 
mayo di oltre 100 anni fa , e ribadito da robert sherman oltre 50 anni fa a proposito della professione del radiologo , per lungo tempo considerato il dottore dei dottori [ 14 ] , ovvero il professionista che doveva servire un altro professionista e riferire a lui solo . 
in tal modo il paziente self - referred stipula un contratto non scritto con il radiologo e esige la risposta per se medesimo o per una persona di sua fiducia . parallelamente nata la cultura della prevenzione , che in ambito radiologico si tradotta con la mammografia di screening . 
in tal caso il soggetto un paziente sano in cui viene creato uno stato di ansiet attraverso lesecuzione di un test e lattesa della sua risposta ; il soggetto desidera conoscere quanto prima il risultato della sua indagine , anche se le aspettative pi probabili sono rappresentate dalla negativit del test . 
in relazione a questo the mammography quality standars act ( mqsa ) [ 15 ] , introdotto in una legge americana il 27 ottobre 1992 , suggeriva con forza il dovere di comunicare nel pi breve tempo possibile alle interessate levenienza di un risultato dubbio o sospetto radiol med ( 2012 ) 117 : 339353 because women claimed they had not been duly informed of a suspicious result [ 16 ]  . 
this feeling is illustrated by leonard berlin in an article with the self - explanatory title : communicating results of all radiologic examinations directly to patients : has the time come ? [ 1719 ]  . 
berlin asks whether it would be possible to reduce the patients anxiety if she were to receive the results directly from the radiologist as soon as possible [ 17 ]  . 
a survey conducted in 1993 demonstrated that 75% of referring physicians and 90% of radiologists were comfortable with radiologists communicating the test results directly to the patient , even though only 28% of clinicians and 33% of radiologists were willing to have the radiologist communicate the result if the test was positive [ 20 ]  . 
other surveys in 1995 found that 94% of patients believed that the radiologist should give them the diagnosis directly at the time of the examination [ 21 , 22 ]  . 
a 1994 study on the preferences of women undergoing mammography revealed that 90% of respondents agreed that the radiologist should give them the results directly on site [ 24 ]  . 
this desire is confirmed by a public health journal with regard to young women affected by breast cancer and their desire to be informed of their fate [ 25 ]  . 
in the same year , the concept was restated that information and a more direct involvement of the patient in decision making improved patient satisfaction as well as outcome , as it had a positive impact on functional recovery and quality of life and increased acceptance of oncological therapies [ 26 ]  . 
no less than 35% of patients preferred receiving abnormal results by phone . therefore , the demand for more , better , direct and faster communication is present throughout the western world , including in italy , where the media often highlight the poor communication skills of health professionals [ 28 ]  . 
in eastern europe , particularly in russia , the practice of informing the patient is less widespread , whereas lorch and scherer report that in germany , 48% of patients want to be informed by their radiologist and 58% by their physician ; 75% would prefer to be told of the result within 30 min of the test and therefore by the radiologist [ 29 ]  . 
la preoccupazione allora era forse motivata pi che da motivi etici da problemi assicurativi , perch emergeva che diverse cause legali erano state intraprese perch le donne affermavano di non essere state debitamente informate del risultato , quando sospetto [ 16 ]  . 
tale sensazione viene descritta con alcuni significativi esempi da leonard berlin in un articolo dal titolo esplicativo : communicating results of all radiologic examinationts directly to patients : has the time come ? [ 1719 ]  . 
berlin si domanda se vi sia la possibilit di ridurre lo stato dansia nel caso il paziente riceva direttamente dal radiologo la risposta nel pi breve tempo possibile [ 17 ]  . 
 uninchiesta effettuata nel 1993 dimostr che il 75% dei medici prescrittori e il 90% dei radiologi erano daccordo nel favorire la comunicazione diretta della diagnosi al paziente da parte del radiologo , anche se soltanto il 28% dei clinici e il 33% dei radiologi stimava che il radiologo dovesse fornire il risultato qualora fosse stato positivo [ 20 ]  . 
 altre inchieste condotte nel 1995 trovarono che il 94% dei pazienti pensavano fosse il caso che il radiologo spiegasse loro direttamente e subito la diagnosi [ 21 , 22 ]  . 
uninchiesta eseguita nel 1994 sui desideri di donne sottoposte a mammografia dimostr che pi del 90% delle intervistate era daccordo sul fatto che il radiologo dovesse fornire la diagnosi direttamente alle interessate [ 24 ]  . 
la stessa aspirazione viene sancita su di una rivista di sanit pubblica a proposito della volont di conoscere il proprio destino da parte di giovani donne affette da carcinoma mammario [ 25 ]  . 
nello stesso anno viene ribadito il concetto che gi lesperienza di molti aveva suggerito , che una migliore informazione e un pi diretto coinvolgimento della paziente nelle decisioni dimostrava avere un effetto positivo sia nella soddisfazione della donna , sia nel suo out - come , ovvero come ricaduta positiva nel recupero funzionale e sulla qualit di vita , anche per una migliore accettazione delle terapie oncologiche [ 26 ]  . 
 [ 27 ] mettono in luce che lesigenza principale del paziente quella di avere la comunicazione della risposta nel pi breve tempo possibile , anche indipendentemente dal medico che la fornisce . 
addirittura il 35% degli intervistati preferirebbe avere le risposte patologiche per telefono piuttosto che di persona . la richiesta quindi di una maggiore , migliore , pi diretta e pi rapida comunicazione presente in tutto il mondo occidentale , nella fattispecie in italia , dove i media spesso mettono in evidenza le carenze di capacit di comunicazione con il pubblico [ 28 ]  . 
nellest europeo , in particolare in russia , la pratica di informare il paziente meno diffusa , mentre in germania lorch e scherer [ 29 ] riportano che il 48% dei pazienti vorrebbe essere informato dal radiologo , il 58% preferirebbe il proprio medico , ma ben il 75% dei soggetti vorrebbe avere 344 professionals point of view the single biggest problem in communication is the illusion that it has taken place . george bernard shaw because the responsibilities of radiologists have expanded , it seems possible that radiologists may eventually be charged with directly informing patients of the results of procedures as well . leonard berlin [ 14 ] communicating is not easy and , as berlin stresses [ 14 ] , taking on new responsibilities implies knowing how to communicate directly with the patient . 
berlin recounts a paradigmatic case [ 30 ] : on 6 june 2008 the virginia supreme court [ 31 ] rendered a decision against a radiologist on the basis of negligence for not having communicated to a patient the presence of a deep vein thrombosis of the leg , or rather , the need to start anticoagulation therapy immediately to prevent pulmonary embolisa series of tragic circumstances caused the death of the woman who developed fatal pulmonary embolism 48 h later . 
over time , there has been an increase in malpractice lawsuits for faulty communication ; in the usa in only 5 years between 1985 and 1990 they have grown by 15% [ 32 ]  . 
an article by levinson reports that in 1994 , 80% of malpractice lawsuits in the usa were based on communication problems [ 33 ] ; in 2004 , fernald et al . 
this applies , as adriano fileni states [ 35 ] , both to outpatients [ 30 ] and inpatients , which means the patient must be satisfied even in terms of direct information . 
extending the professional contract to inpatients would in itself necessitate careful consideration and discussion , as communication issues may be even more complex in the case of inpatients and closely related to their state of health and ability to relate . radiol med ( 2012 ) 117 : 339353 la risposta entro 30 minuti dallindagine e quindi dal radiologo . 
nel frattempo le aziende ospedaliere hanno creato nuovi uffici di relazione con il pubblico ( urp ) che per non vanno alla radice del problema , che di squisita natura rapporto medico - paziente . il punto di vista professionale the single biggest problem in communication is the illusion that it has taken place . george bernard shaw because the responsabilities of radiologists have expanded it seems possible that radiologists may eventually be charged with directly informing patients of the results of procedures as well leonard berlin [ 14 ] non facile comunicare e , come sottolinea berlin [ 14 ] , lassunzione di nuove responsabilit implica il dovere di sapere comunicare direttamente al paziente . 
 molte cause legali , sia negli stati uniti che in italia ed in europa hanno alla loro base un difetto di comunicazione , una mancata comunicazione o una comunicazione insufficiente . 
il 6 giugno 2008 la suprema corte dello stato della virginia [ 31 ] pronunci una sentenza sfavorevole al radiologo per negligenza per non avere comunicato a una paziente la presenza di una flebotrombosi dellarto inferiore o meglio la necessit di intraprendere immediatamente un trattamento anticoagulante per evitare lembolia polmonare . 
un insieme di tragiche circostanze portarono a morte la donna che dopo 48 ore ebbe unembolia polmonare mortale : il radiologo cerc al telefono il medico curante che non rispose ( era un venerd pomeriggio ) ; invi un fax che il medico curante vide , ma non lesse , ed infine capit davvero lembolia e per giunta nel giorno festivo . 
un altro articolo di levinson riporta che , nel 1994 , l80% delle cause per malpractice negli usa si fondavano su difetti di comunicazione [ 33 ] e , nel 2004 , fernald et al . 
 daltra parte oggi la legislazione italiana vede nel rapporto medico paziente un rapporto di tipo contrattuale , che va onorato , e questo vale , come afferma adriano fileni [ 35 ] , non solo nei confronti del paziente esterno [ 30 ] , ma anche del ricoverato e questo significa che il paziente deve essere soddisfatto anche in termini di informazione diretta . 
il contratto professionale esteso ai pazienti ricoverati radiol med ( 2012 ) 117 : 339353 moreover , many patients often file lawsuits for not having been , in their opinion , informed or listened to or because they feel they have been treated in a cold and detached manner [ 36 ]  . 
the situation is worse if there is also some error that , once disclosed , is not acknowledged by the doctor . the only unforgivable sin is to conceal errors karl popper [ 37 ] it is a fact that physicians often tend to conceal their errors , whereas patients think that physicians should never make mistakes ( and the media reinforce such a conviction )  . 
antonio damasio [ 41 ] states that effective communication ( empathetic ) is the most crucial personal asset : it allows us to coordinate all our other skills , such as observing and solving problems ; it changes the quality of the relationship , preventing dysfunction , misunderstandings , errors and waste of time and resources . 
when creating an empathetic communication with the patient , the doctor is aware of the patients needs , is more concentrated and makes fewer mistakes ; at the same time , the patient appreciates the doctors difficulties . what and when to communicate da solo richiederebbe unattenta riflessione e discussione , dato che per tali pazienti le problematiche di comunicazione possono essere ancora pi complesse , fortemente legate anche allo stato di salute del paziente e alla sua capacit di interrelazione . molti pazienti inoltre spesso ricorrono legalmente verso il medico per non essere stati , a loro dire , informati n ascoltati su loro richiesta oppure perch si sono sentiti trattati in modo freddo e distaccato [ 36 ]  . 
la cosa si aggrava se c anche un errore che , diventato palese , non viene riconosciuto dal medico . lunico errore imperdonabile nascondere un errore karl popper [ 37 ] un dato di fatto che spesso i medici tendono a celare i propri errori , mentre i pazienti pensano che i medici non dovrebbero mai sbagliare ( e i media rafforzano tale convinzione )  . 
 evidente quindi che solamente con unadeguata comunicazione al paziente della potenziale possibilit di errore , possa venire recepita la fallibilit umana , nonch compresa la percentuale di incertezza insita nel metodo , e apprezzata la sincerit . 
antonio damasio [ 41 ] afferma che una comunicazione efficace ( empatica ) costituisce la pi cruciale delle risorse personali e consente di coordinare tutte le altre capacit che si possiedono , come osservare e risolvere problemi ; trasforma la qualit della relazione impedendo disfunzioni , incomprensioni , errori , spreco di tempo e di risorse . 
creando una comunicazione empatica il medico avverte le necessit del paziente , pi concentrato e fa meno errori e contestualmente il paziente comprende le difficolt del medico . you have two ears and one mouth , which means you should listen twice as much as you speak saint jerome che cosa e quando comunicare ... 
in situations of uncertainty the patients anxiety is reduced merely by talking , even if this is not conclusive . anonymous a willingness to listen to the patient is the first step towards correct verbal communication , and just uttering simple words in an understanding manner reduces anxiety and creates a proactive problem - solving atmosphere . 
smith and gunderman [ 42 ] address the issue by discussing four approaches : ( 1 ) hai due orecchie e una bocca , ci significa che devi ascoltare il doppio delle parole che pronunci san girolamo ... 
lansia del paziente viene ridotta , nelle situazioni di incertezza , dal semplice colloquio , anche se non conclusivo . anonimo la semplice disponibilit ad ascoltare il paziente rappresenta il primo passo per una corretta comunicazione verbale , e pronunciare parole semplici in tono comprensivo di per s riduce lo stato ansioso e crea un clima proattivo alla soluzione dei problemi . 
dont tell : the view of the radiologist as the doctors doctor has been widely overcome , as has that of radiologists choosing this specialty because they do not feel comfortable with having a direct relationship with patients [ 43 ]  . 
roy filly warns against providing patients with too much information [ 44 ] , stating that 10% of obstetrical sonograms contain apparent foetal abnormalities , which may even be interpreted as markers for down syndrome but which are ultimately of no consequence . 
on the other hand , who better than the radiologist understands the images and is able to explain them to the patient ? the radiologist knows the indications , limitations , risks and implications of imaging better than the clinician does [ 45 ]  . 
if the radiologist fails to seize the opportunity to interact with the patient , overall control of the patient will be lost ; today , in fact , it is not unusual for the patient not to know that the radiologist is a doctor , and they are able to distinguish radiology technicians from radiologists . 
ask to tell : some people who are reluctant to ask or are not used to asking or have limited knowledge of the language often elderly or foreign patients might fail to ask for information about their tests . 
in these cases , medical personnel should be instructed to ask the patients if the information received is exhaustive or if they would like more details on their tests and test results . 
such a proactive attitude would be extremely convenient if it translated into useful information and actions , especially in the event of findings requiring further diagnostic tests or specialist consultations , or in situations that necessitate monitoring . 
la visione del radiologo dottore dei dottori oggi ampiamente superata , cos come la posizione del medico che sceglie la specialit radiologia in quanto non desidera o non ritiene di avere la predisposizione a rapportarsi direttamente con il paziente [ 43 ]  . 
roy filly pone un caveat sul fornire eccessive informazioni alle pazienti [ 44 ] sostenendo che il 10% delle ecografie ostetriche contiene anormalit apparenti , che possono essere interpretate anche come markers di sindromi di down , ma che alla fine si rilevano inconsistenti . 
daltra parte chi pi del radiologo conosce le immagini e pu spiegarle al paziente ? il radiologo conosce le indicazioni , i limiti , nonch i rischi e le implicazioni dellimaging pi del clinico [ 45 ]  . 
se il radiologo non comprende le opportunit di interagire con il paziente in tale contesto perder il totale controllo dei pazienti ; oggi , infatti , non inusuale che il paziente non sappia neppure che il radiologo sia un medico o non in grado di distinguere il tecnico di radiologia dal medico . 
alcune persone per scarsa propensione a chiedere , oppure per scarsa abitudine o per modesta o incompleta conoscenza della lingua , quindi spesso anziani o stranieri , potrebbero non richiedere informazioni circa le indagini di proprio interesse . 
in tali casi dovrebbe essere programmata la disponibilit del personale medico a richiedere agli interessati se le informazioni ottenute sono esaustive oppure se desiderano conoscere dettagli sulle loro indagini e sugli esiti relativi . 
tale atteggiamento propositivo sarebbe estremamente conveniente se si traducesse con informazioni e atti utili alle persone soprattutto in caso di indagini positive che richiedano ulteriori accertamenti o visite specialistiche , oppure che presentino situazioni da controllare nel tempo . 
in questi casi il radiologo pu provvedere a fornire gli appuntamenti con i colleghi specialisti , se le persone condividono i suggerimenti , oppure fornire gli appuntamenti per le indagini radiol med ( 2012 ) 117 : 339353 there would be no increase in costs but , instead , savings resulting from more efficient management of healthcare by reducing idle time , as well as benefits not only for the patients , who might feel overwhelmed by the complexity of the healthcare system , but for all of society . 
 [ 23 ] report that the time spent informing the patient of normal results is on average less than 2 min the case of minor abnormalities , it is on average less than 5 min , whereas in the case of significant abnormalities , it takes more than 8 malthough we can consider delegating to nonmedical professionals the task of communicating normal results , it is necessarily the radiologist who must communicate complex abnormalities or neoplastic diagnoses . 
the existing practice in some breast imaging services of employing psychologists is deleterious , as a psychologist knows nothing or very little about the disease , the case at hand or the next steps to be taken . 
always tell : gradually , it appears clear that we might as well always tell the patient , even if from a psychological point of view patients have to be given the impression that the request for information actually came from the this would eliminate the risk of breaches in communication and any problems connected to the failure to communicate . 
after all , informing the patient is already the rule when his or her life is in immediate danger : what is the difference if the danger is deferred ? this position is in line with that of the italian society of medical radiology ( sirm ) [ 47 ] and the guidelines of the american college of radiology ( acr ) that , while not indicating this behaviour as compulsory , suggest that it is desirable . 
 in fact , in 1999 , the acr guidelines [ 48 ] introduced the concept of direct communication with the patient , and in the 2005 review , the radiologists ethical responsibility to communicate the test results directly to the selfreferred patient was added , and in any case , whenever the patients life is at risk . 
 there are three main situations in which physicians need to be prepared to communicate findings verbally to patients in a clear and not counterproductive manner : incidental findings , situations of risk and the presence of severe disease ( especially if neoplastic )  . di controllo di propria competenza . 
non si tratterebbe di un aggravio di costi , ma in realt di un risparmio per una gestione sanitaria pi efficiente senza tempi morti , e di un guadagno non solo per i pazienti che , spaesati , potrebbero perdersi nei meandri della complessit sanitaria , ma per tutta la societ . 
 possibile pensare di potere delegare anche del personale non medico per fornire informazioni sulla normalit delle indagini , ma deve essere delegato il radiologo per problematiche complesse o per riferire diagnosi neoplastiche . 
la pratica esistente in alcuni servizi di senologia di impiegare psicologi deleteria perch lo psicologo nulla sa o poco conosce sulla malattia e sul caso specifico e su quello che seguir . 
passo dopo passo si giunge alla conclusione che tanto vale dire in ogni caso , anche se , da un punto di vista psicologico , necessario dare limpressione agli interessati che la richiesta scaturisca motu proprio da loro stessi . 
in fin dei conti informare il paziente gi la regola quando la sua vita in pericolo immediato , che cosa cambia se il pericolo pi dilazionato ? tale posizione non contrasta con quella della societ italiana di radiologia medica ( sirm ) [ 47 ] , n con le linee guida dellamerican college of radiology ( acr ) che peraltro non indicano categoricamente come obbligatorio questo comportamento , ma lasciano intendere lauspicabilit . 
lacr infatti introduce nel 1999 [ 48 ] il concetto di direct communication to the patient ; nella revisione del 2005 acr introduce il concetto della responsabilit etica del radiologo nella comunicazione diretta del risultato delle indagini al paziente self referred e in ogni caso quando sia a repentaglio la vita del paziente . 
in questo ambito va rimarcato , comunque , un certo ritardo culturale delle societ scientifiche rispetto alle esigenze della societ in evoluzione . in ogni caso non affatto banale comunicare verbalmente con il paziente soprattutto in caso di comunicazione di anormalit . esistono tre situazioni principali nelle quali occorre essere preparati per comunicare verbalmente in modo chiaro e non controproducente ai pazienti : i reperti incidentali , situazioni di rischio , e la presenza di una patologia grave ( in particolare neoplastica )  . incidental findings reperti incidentali these have become increasingly common and are in most cases absolutely benign . 
despite the lack of guidelines on the subject , which we hope will be developed in the near future , it is clear that the patients need to be given the most up - to - date information so that they will ask for follow - up tests themselves in a calm and rational manner . 
pur mancando spesso le linee guida , auspicabili in un prossimo futuro , vanno fatte presenti le informazioni pi recenti su quellargomento , cos che il paziente stesso richieder il controllo in maniera serena . 
knowledge , trust in the doctor and health system , controllability and willingness are all aspects that help reduce the negative perception of risk ; in contrast , highlighting the catastrophic potential , previous negative examples and inappropriate media messages will negatively affect the awareness of risk . 
we therefore need to frame the situation positively for the patient ( the greater likelihood of not developing severe conditions or complications , the fact that monitoring the complication will help to detect it early on )  . 
 this may result in excessive alarmism , which is counterproductive and tends to drive the patient away rather than ensure adherence to all the necessary tests and investigations . situazioni di rischio un discorso analogo va fatto per il rischio . 
la conoscenza del problema da parte della persona , la fiducia verso il medico e nelle istituzioni , la controllabilit e volontariet sono aspetti che riducono la percezione negativa del rischio , mentre lesaltazione del potenziale catastrofico , di precedenti esempi negativi , lincertezza e i messaggi mediatici incongrui peggiorano la consapevolezza del rischio . 
 necessario quindi prospettare sempre laspetto positivo ( il cosiddetto framing positivo o quadro di presentazione ) per il paziente ( la migliore probabilit di non incorrere in situazioni o complicanze gravi , il fatto che essendo sotto controllo la complicazione sar colta in tempo ) , e non quello negativo . 
loperatore stesso spesso non ha ben chiaro il concetto di rischio e potrebbe creare un eccessivo allarmismo , che come nel caso precedente si rivela controproducente , e tende ad allontanare linteressato , piuttosto che farlo propendere per i controlli del caso . bad news cattive notizie communicating bad news requires special skill and sensitivity . 
the severity of bad news is directly proportional to the gap between the real situation ( objective reality ) and perceived situation ( subjective reality ) ; on the other hand , the majority of individuals want to be told [ 4951 ]  . 
the operator must be motivated and prepared , know how to start ( breaking the ice ) , inform ( giving hope ) , be able to provide psychological support and outline a plan of action capable of overcoming the patients psychological confusion , and finally be able to close the consultation stating clearly what the next steps are . 
the radiologist must know how to use simple language , not give all the information at once but leave room for questions and use euphemisms to prepare the patient and lessen the impact of the news . 
the radiologist must also inform the patient that treatment will involve a team of professionals ; in this case , it is useful to use the comunicare cattive notizie richiede unattenzione e delle capacit particolari . 
la notizia tanto pi cattiva quanto maggiore la differenza tra la situazione reale ( realt oggettiva ) e la percezione della realt ( realt soggettiva ) , daltra parte , come sopradetto , la maggior parte delle persone vuol sapere [ 4951 ]  . 
loperatore deve essere motivato e preparato , sapere iniziare ( rompere il ghiaccio ) , informare ( mantenendo viva la speranza ) , sapere fornire supporto psicologico e predisporre un piano di azione che consenta di superare la confusione psicologica dellinteressato e infine sapere concludere rendendosi disponibile per i successivi passi . 
il radiologo deve sapere usare un linguaggio semplice , non dare le notizie tutte in una volta ma lasciare spazio per le domande , impiegare eufemismi per preparare e attenuare limpatto . 
il radiologo inoltre deve fare presente che la cura del paziente coinvolge pi professionisti ; in questo caso utile utilizzare lesempio della staffetta dove il paradiol med ( 2012 ) 117 : 339353 example of the relay race in which the patient is the baton being passed from hand to hand among the race participants ( the different professionals ) and never dropped . ziente corrisponde al testimone che viene passato di mano in mano dai vari componenti la staffetta ( i diversi professionisti ) e mai lasciato cadere . how to communicate come comunicare x , i dont like what i saw... ...i would have wanted the earth to open up and swallow me ! its been two years now and my daughter is fine , and i want you to know that the fact that she was there helped to reduce my fears . 
 setting and time have already been mentioned ; verbal communication , especially of information regarding major abnormalities , cannot take place in a corridor or waiting room or take only 30 sec . 
on the other hand , effective communication is an essential component of high - quality healthcare , so hospital managers need to be aware of the additional time required to give due communication in the organisation of work and productivity . in her paper communication : the key to improve patient care [ 53 ] , peggy j . 
if there is miscommunication here , who is failing ? the patient ? the radiologist ? it is clear that even if both are failing , communication is the responsibility of the physician , who must be prepared for the task . 
communication is , in fact , a circular process , with an emitter ( the physician ) , a receiver ( the patient ) , a means ( speech and body language ) and a feedback mechanism for checking reception . 
we could discuss at length the various aspects of communication through body language , a complementary yet essential component of verbal communication a comforting hand , eye contact to convey honesty and truthfulness , but also looking at your watch when you are in a hurry or at your hand on the door handle when you signora , quello che ho visto , non mi piaciuto per niente avrei voluto che una voragine si aprisse sotto i miei piedi e sprofondarci dentro ! sono ormai passati due anni e mia figlia sta bene e io desidero dirle che il fatto che ci fosse lei con me , in quel momento mi ha fatto avere un po meno paura . 
 grazie ( lettera di una paziente ) si gi fatto cenno su alcuni aspetti pratici , ma il problema tuttaltro che semplice e il processo del tutto in evoluzione , per ortega e garca si tratta di un capitolo non ancora risolto [ 52 ]  . 
sul contesto e sul tempo si gi accennato ; la comunicazione verbale , specie per le informazioni di anormalit importanti , non pu avvenire in un corridoio o in una sala daspetto . 
oggi questo crea conflitto sia con la struttura del servizio che prevede pochi spazi tranquilli e nessuno deputato ad hoc , che dovr invece essere previsto per il futuro , sia con la produttivit . 
fritzsche scrisse in un suo lavoro communication : the key to improve patient care [ 53 ] : se i tuoi pazienti sono come i miei , tu sai che vogliono sapere il risultato dellesame . 
la comunicazione infatti un processo circolare con unemittente ( il medico ) , un ricevente ( il paziente ) , un mezzo ( la parola , ma anche il linguaggio del corpo ) , e un meccanismo di feed - back per controllo dellavvenuta ricezione . 
si potrebbe parlare a lungo degli aspetti relativi alla comunicazione attraverso il linguaggio del corpo che rappresenta una componente complementare , ma essenziale della comunicazione verbale , dalla mano che conforta e accarezza , allo sguardo diretto che conferisce veridicit e sincerit alle parole , ma anche allo sguardo allorologio che indica fret350 radiol med ( 2012 ) 117 : 339353 want to put an end to the conversation . 
these are all aspects of basic communication psychology that reinforce the conviction that the operators require adequate training . in 2006 , ortega and garca found that the majority of radiologists reported insufficient training in communication skills [ 52 ]  . 
thus , the need for training in communication skills has been felt for at least a decade in developed countries . in 2000 , the american board of medical specialties [ 55 ] defined six main competencies that should be common to all physicians , one of them being interpersonal and communication skills . 
in 2005 , the official gazette of the italian republic published the new statute of medical residency schools [ 56 ] , which for the first time feature communication as a taught subject . 
the new standards for professional accreditation in the united states are published on the internet : ( 1 ) the national board of medical examiners , steps 2 and 5 [ 57 ] ; ( 2 ) the accreditation council for graduate medical education [ 58 ] , where verbal communication is an established component . 
in the context of communication skills in diagnostic imaging , the standards provide a list of required skills : sensitivity , courtesy , compassion , appropriateness , honesty and openness . 
also acting as teachers on these programmes are patients who survived breast cancer , and awkward and delicate conversations are carried out that allow one to assess the operators communicative competence . 
sono tutti aspetti di psicologia elementare della comunicazione che ci aiutano a rafforzare il convincimento che sia necessaria una robusta formazione degli operatori . ortega e garca nel 2006 affermavano che la maggior parte dei radiologi riportava una preparazione insufficiente nellambito dei processi di comunicazione [ 52 ]  . 
quindi da almeno un decennio che nei paesi occidentali nasce la necessit di formare in comunicazione . lamerican board of medical specialties [ 55 ] nel 2000 defin 6 principali competenze comuni a tutti i medici . 
nel 2005 in italia viene pubblicata sulla gazzetta ufficiale il nuovo statuto delle scuole di specializzazione [ 56 ] , dove per la prima volta viene previsto linsegnamento della comunicazione . 
nellambito dei processi comunicativi in radiologia vengono indicate le capacit necessarie : sensibilit , cortesia , capacit di creare empatia / partecipazione emotiva , appropriatezza del comportamento , onest , disponibilit e viene enunciato il decalogo : 1 . 
per quanto riguarda la preparazione pratica si suggeriscono delle simulazioni nelle quali pazienti o ex - pazienti volontari fungono da veri e propri insegnanti e valutatori [ 61 ]  . 
in questi programmi si prestano al ruolo di insegnanti pazienti sopravvissute a neoplasie mammarie , e vengono messe in essere conversazioni difficili e scabrose , che permettano di identificare il grado di capacit comunicativa degli operatori ; gli incontri vengono registrati , rivisti e commentati . 
nella scuola di specializzazione radiol med ( 2012 ) 117 : 339353 which i am employed , radiology residents training in breast imaging observe the radiologist during verbal communication of the diagnosis to the patient , and then , once they have gained sufficient autonomy , conduct the encounter themselves in the presence of a tutor . 
these responsibilities , which are indispensable for adding clinical value to radiology , are a source of stress and often cause detachment and withdrawal from the discipline ( burnout ) , or at least from those activities requiring direct contact with the patient , and especially breast imaging [ 61 ]  . 
it is therefore clear that we need trainers prepared to devise adequate curricula to teach and assess the residents individual skills . connected to this there is also a need , as pasquale marano suggested [ 1 ] , to create a cultural background that gives the radiologist a partly humanistic education and a more holistic view of patients problems and to adopt a more practical and tutorial approach to teaching . 
this process should also involve health system administrators and politicians at a local and national level to communicate the idea that medicine is changing and becoming more personalised and targeted to the needs and dignity of the individual . 
 in radiologia della mia universit lo specializzando durante il training senologico affianca lo strutturato durante la comunicazione verbale della diagnosi , per poi condurre lui stesso in prima persona la conversazione in presenza del tutor , una volta acquisita una sufficiente autonomia . 
lassunzione di tali responsabilit , indispensabili per dare valore clinico alla radiologia , sono fonte di stress e spesso provocano il distacco dalla disciplina ( burn out ) o perlomeno da quelle attivit della disciplina che sono a pi diretto contatto con il paziente , specialmente la diagnostica senologica [ 61 ]  . linsegnamento per della comunicazione ridurrebbe lo stress e consentirebbe lassunzione di maggiori responsabilit [ 14 , 17 , 30 ]  . 
quindi evidente il bisogno di uno staff preparato per confezionare curricula adeguati proprio per insegnare ( formare per formare ) , e per valutare le capacit individuali degli specializzandi . dietro tutto questo sta anche , come ha suggerito pasquale marano [ 1 ] , avere e creare un back - ground culturale che conferisca al radiologo una preparazione anche umanistica e una visione pi olistica delle problematiche dei pazienti , nonch modificare le modalit di insegnamento verso formule pi pratiche e tutoriali . 
in tale processo vanno coinvolti anche gli amministratori del sistema nonch i politici a livello locale e nazionale per fare comprendere che la medicina sta evolvendo verso modalit pi personalizzate e ritagliate sui bisogni e sulla dignit della persona . 
fugazzola1 1interventional radiology , department of radiology , university of insubria , viale borri 57 , 21100 varese , italy 2vascular surgery , department of surgical sciences , university of insubria , varese , italy 3cardiac surgery , department of surgical sciences , university of insubria , varese , italy 4anaesthesia and palliative care , circolo university hospital , varese , italy correspondence to : g . 
in our experience , a higher mortality rate was observed for the aorto - uni - iliac configuration ; shock at admission was confirmed as the most important factor for postoperative survival . keywords ruptured abdominal aortic aneurysms endovascular repair aortic endograft riassunto obiettivo . 
nella nostra esperienza , si osservata una pi alta mortalit nel gruppo in cui stata posizionata una ep aorto - uni - iliaca ; lo shock allingresso risultato essere il fattore pi importante da correlare con la sopravvivenza post - operatoria . parole chiave aneurismi dellaorta addominale rotti trattamento endovascolare endoprotesi aortica radiol med ( 2012 ) 117 : 410425 introduction introduzione although recent meta - analyses reported a gradual decrease in mortality rate associated with ruptured abdominal aortic aneurysms ( raaa ) , it is generally accepted that in the last few decades , there has been no consistent improvement in the number of operative deaths [ 1 , 2 ]  . 
these results have raised many questions on when endovascular repair of raaas should be attempted , particularly in subsets of patients in whom the probability of a fatal outcome is high [ 36 ]  . 
recently , several centres have published their experiences with emergency endovascular repair ( eevar ) of raaa , reporting encouraging results and improvements in mortality and morbidity rates compared with surgical repair ; these results may have been biased by patient selection [ 715 ]  . 
there is no reliable evidence to support the widespread adoption of evar in an unselected population of patients who present with raaa . recent studies also identified issues surrounding the new technique , notably , aneurysm morphology , logistics and endograft ( eg ) requirements [ 1619 ]  . 
several unresolved questions remain regarding the use of eevar in raaas ; the possibility of performing eevar is related to aneurysmatic morphological factors , in particular , infrarenal neck anatomy , iliac artery patency and device configuration [ 2022 ]  . 
the aim of this study was to analyse the results of our ongoing experience with eevar for raaa and , in particular , to compare results of the modular aorto - uni - iliac ( aui ) versus the bifurcated ( bif ) configuration . materials and methods patients this was a nonrandomised , retrospective , single - centre study . 
in all cases , a vascular nonostante le recenti meta - analisi riportino dati di una graduale riduzione della mortalit , rimane come dato di fatto che nelle ultime decadi , non c stato un consistente miglioramento nel numero dei decessi intra - operatori per aneurismi dellaorta addominale in rottura ( raaa ) [ 1 , 2 ]  . 
 questi risultati hanno fatto sorgere molteplici interrogativi su quando lintervento di riparazione endovascolare dellraaa debba essere tentato , in particolare in quel sottogruppo di pazienti in cui la probabilit di esito fatale alta [ 36 ]  . 
ultimamente , molti centri hanno pubblicato la loro esperienza riguardo al trattamento di riparazione endovascolare di aneurismi in regime di emergenza ( eevar ) , riportando risultati incoraggianti ed un miglioramento sulla mortalit e sulla morbilit rispetto al trattamento chirurgico ; tali risultati possono essere stati falsati dalla selezione dei pazienti trattati [ 715 ]  . 
attualmente , non vi un livello di evidenza tale che indirizzi verso il trattamento endovascolare in maniera diffusa in una popolazione di pazienti che presenta raaa . studi recenti hanno identificato una serie di problematiche associate a questo approccio : la morfologia dellaneurisma , la logistica ed i requisiti intrinseci dellendoprotesi ( ep ) [ 1619 ]  . 
attualmente restano irrisolti diversi interrogativi riguardo leevar in raaa ; la possibilit di eseguire eevar da correlare con la morfologia dellaneurisma , in particolare il colletto sottorenale , la perviet delle arterie iliache ed alla configurazione dellep stessa [ 2022 ]  . 
lo scopo di questo studio di analizzare i risultati della nostra esperienza sulleevar nellraaa ed in particolare di confrontare i risultati tra lutilizzo di ep aorto - uni - iliaca ( aui ) versus quella biforcata ( bif )  . materiali e metodi pazienti lo studio presentato uno studio non - randomizzato , retrospettivo mono - centrico . 
quarantadue pazienti ( 62 , 7% ) sono stati trattati con eevar ; allinizio della nostra esperienza endovascolare , 7 ( 14 , 28% ) pazienti potevano essere sottoposti ad eevar , ma sono stati trattati chirurgicamente in open ; perci , in realt , i pazienti che potevano essere trattati con approccio endovascolare sarebbero stati 49 / 61 ( 80 , 3% )  . 
patients were divided into two subgroups for comparative analysis according to the configuration of the eg : aui ( group a ) and bif ( group b )  . baseline imaging all patients underwent 64 - slice multidetector computed tomography ( mdct ) ( aquilon 64 , toshiba , tokyo , japan ) to assess their clinical condition . 
scanning parameters were : collimation 0.564 ; wide field of view ( fov ) ( 320400 mm ) ; gantry rotation speed 0.400 s ; modulated mas [ standard deviation ( sd ) 12 ] ; 120 kv ; pitch factor 0.825 ; slice thickness 1.0 mm ; reconstruction interval 0.8 mthe arterial phase was acquired after administration of 120 ml of 350 mgi / ml iodinated contrast media ( iomeron 350 , bracco , milan , italy ; visipaque 320 , ge healthcare , fairfield , ct , usa ) at an injection rate of 4 ml / s , followed by 40 ml of saline solution at the same injection rate , using a doublehead automatic injector ( stellant d , medrad , usa )  . 
optimal arterial enhancement was achieved with the bolus - tracking technique by positioning a region of interest ( roi ) on the abdominal aorta ( at the suprarenal level ) , with a threshold 100 hu higher than baseline density . 
on ct angiography ( cta ) , rupture was defined as extravasation of blood surrounding the aneurys aneurysm morphology was defined according to the european collaborators sunte nella figura 1 . 
i pazienti inseriti nello studio sono stati divisi in 2 sottogruppi in relazione alla ep utilizzata per poter eseguire un analisi comparativa , in particolare : ep aorto - uni - iliaca ( gruppo a ) ed ep biforcata ( gruppo b )  . modalit di immagine tutti i pazienti sono stati sottoposti ad esame angio - tomografia computerizzata ( tc ) con apparecchio multidetettore a 64 strati ( aquilon 64 , toshiba , tokio , giappone ) in relazione alle condizioni cliniche . 
i parametri tecnici sono stati : collimazione 0 , 564 ; campo di vista ( fov ) largo ( 320400 mm ) , rotazione del gantry 0 , 400 s , modulazione mas ( standard deviation 12 ) , kv 120 , pitch factor 0 , 825 , spessore di taglio 1 mm , intervallo di ricostruzione 0 , 8 mla fase arteriosa stata acquisita dopo la somministrazione 120 ml di mezzo di contrasto iodato 350 mgi / ml ( iomeron 350 , bracco , milano , italia ; visipaque 320 , ge healthcare , usa ) con un flusso di iniezione di 4 ml / s , seguiti da un iniezione di 40 ml di soluzione fisiologica con lo stesso flusso , utilizzando una radiol med ( 2012 ) 117 : 410425 on stent - graft techniques for abdominal aortic aneurysm repair ( eurostar ) classification [ 23 ] , as shown in fig . 
exclusion criteria for eevar at our centre are based on anatomical parameters : proximal neck length < 10 mm , proximal neck diameter > 32 mm and external iliac artery diameter < 7 mm with severe bilateral iliac artery disease . pretreatment procedure the procedure is generally carried out with the patient under sedation from of 37 mg of midazolam chlorohydrate ( ipnovel 15 ; roche , milan , italy ) and 4 ml of fentanyl citrate ( fentanest ; pharmacia & upjohn , milan , italy ) or 2.5 mg / kg propofol ( diprivan , astrazeneca ) and with continuous monitoring of the cardiovascular and respiratory systems . 
each patient received a fluid protocol ( 5% mannitol , 3 l / kg / min dopamine plus 600 mg intravenously administered n - acetylcysteine ) against the ischaemic - related delivery of free radicals and renal damage due to the contrast mediuheparin ( 2 , 5005 , 000 iu intravenously ) was administered to all patients , and short - term antibiotic prophylaxis was performed . equipment imaging guidance intraoperative angiography ( bv 300 , philips , best , the netherlands ) was carried out at the time of the operative procedure . 
2 morfologia degli aneurismi aortici rotti sottoposti a trattamento di riparazione endovascolare in regime di emergenza , classificati secondo le linee guida eurostar . pompa automatica a doppio sistema di iniezione ( stellant d , medrad , usa )  . 
lenhacement arterioso ottimale stato ottenuto mediante la tecnica del bolus tracking , posizionando la regione di interesse ( roi ) nel contesto della aorta addominale ( nel tratto sovra - renale ) con una soglia di 100 uh al di sopra della densit basale . 
i criteri di esclusione nel nostro centro per eevar sono basati su rilievi anatomici : lunghezza del colletto prossimale inferiore a 10 mm , diametro del colletto prossimale maggiore di 32 mm e diametro dellarteria iliaca esterna inferiore a 7 mm con severa malattia aterosclerotica dei vasi iliaci bilateralmente . procedura pre - trattamento la procedura generalmente eseguita in sedazione mediante somministrazione endovena ( ev ) di 37 mg di midazolam cloridrato ( ipnovel 15 , roche , milano , italia ) e 4 ml di fentanil citrato ( fentanest , pharmacia & upjohn , milano , italia ) o 2 , 5 mg / kg di propofol ( diprivan , astrazeneca , milano , italia ) , sotto continuo monitoraggio delle funzioni cardiocircolatoria e respiratoria . 
ogni paziente riceve un protocollo infusionale ( mannitolo 5% , 3 l / kg / min di dopamina e 600 mg di n - acetilcisteina ) atto a prevenire il danno da radicali liberi e il danno renale da somministrazione di 414 radiol med ( 2012 ) 117 : 410425 positioning of a 5 - f introducer ( terumo , tokyo , japan )  . 
a first panoramic angiogram was obtained on the aortoiliac region with placement of 5 - f pigtail catheter and administration of iodinated contrast media ( iomeron 350 , bracco ; visipaque 320 , ge healthcare )  . 
the entire procedure was performed under fluoroscopic control . endografts and procedure we have a large number of proximal eg components ( 22 , 26 , 28 , 30 , 34 and 36 mm in diameter ) , extensions and distal eg branches ( 10 , 12 , 16 , 20 24 mm in diameter ) of different lengths , along with occluding plugs of different diameters . 
an endovascular clamp with occlusion balloon ( boston scientific , natick , ma , usa ) was used in cases of severe instability . follow - up the follow - up protocol included a cta examination at 1 and 12 months after the intervention following the same parameters of the preprocedural ct . 
all ceus examinations were performed on a philips iu22 ( philips medical system ) after a 2.5 - ml intravenous bolus of second - generation ultrasound contrast medium ( sonovue , bracco ) , followed by a 10 - ml bolus of saline solution . 
all images were stored on an ultrasound machine as three clips lasting 60 s each ; dynamic observation of the contrast - enhancement phases ( arterial , venous , late ) was possible by maintaining the same scanning frame rate as the b - mode examination . primary technical and clinical success , and safety mezzo di contrasto ( mdc ) iodato . 
ad ogni paziente vengono inoltre somministrate 25005000 ui di eparina sodica ev ed una profilassi antiobiotica a breve termine . strumentazione imaging per tutte le procedure stato utilizzato un angiografo portatile intra - operatorio ( bv 300 , philips , best , paesi bassi )  . 
 un primo angiogramma del distretto aorto - iliaco stato quindi ottenuto mediante posizionamento di un catetere pig tail 5 f e la somministrazione di un bolo di mdc ( iomeron 350 , bracco , milano , italia ; visipaque 320 , ge healthcare , fairfield , ct , usa )  . 
lintera procedura stata eseguita sotto guida fluoroscopica . endoprotesi e procedura presso il nostro centro , abbiamo a disposizione una vasta gamma di endoprotesi ( diametri di 22 , 26 , 28 , 30 , 34 e 36 mm ) , di estensioni e di branche protesiche distali ( diametri di 10 , 12 , 16 , 20 e 24 mm ) , ognuna in differenti lunghezze , oltre a dispositivi di chiusura vascolare ( plug ) di differenti diametri . 
nei casi di severa instabilit emodinamica stato utilizzato un pallone occlusore aortico ( boston scientific , natick , ma , usa )  . follow - up the outcomes of primary technical and clinical success and safety were defined as follows . 
safety was defined as the frequency of major or minor complications ( in accordance with the classification system of the society of interventional radiology [ 24 ] )  . statistical analysis clinical data were prospectively recorded and tabulated with microsoft excel ( microsoft corp , redmond , wa , usa )  . 
continuous variables were tested for normal distribution by kolmogorovsmirnov test and compared between groups with unpaired students t test for normally distributed values ; otherwise , the mannwhitney u test was employed . 
the strength of the association of variables with the development of af was estimated by calculating the odds ratio ( or ) and 95% confidence intervals ( ci )  . 
statistical analysis was computed with spss , release 13.0 for windows ( spss inc , chicago , il , usa )  . results group a thirteen patients ( 30.9% ) received an aui ( group a ) and 29 a bif ( group b ) eg . 
an endovascular clamp with occlusion balloon was used in four cases ( 9.5% ) : one in group a and three in group b . in the 13 group a patients , aneurysm diameter averaged 7.31.3 ( range 610 ) cm ; nine patients ( 69.2% ) were haemodynamically unstable . 
mean delay from admission to intervention was 80.62 ( range 35210 ) mhaemoglobin , systolic blood pressure and heart rate were 8.53.7 g / dl , 9018 mmhg and 10016 bpm , respectively . 
tutti gli esami ceus sono stati eseguiti con ecografo philips iu22 ( philips medical system , best , paesi bassi ) , dopo somministrazione ev di un bolo di 2 , 5 ml di contrasto ecografico di seconda generazione ( sonovue , bracco , milano , italia ) , seguito da 10 ml di soluzione fisiologica . 
tutte le immagini sono state registrate sullapparecchiatura come 3 clips di 60 secondi ognuna ; losservazione dinamica delle varie fasi contrastografiche ( arteriosa , venosa e tardiva ) stata ottenuta mantenendo lo stesso frame rate dellacquisizione in b - mode . successo tecnico primario , successo clinico primario e sicurezza il successo tecnico primario stato definito come corretto posizionamento dellep aui o bif con completa esclusione dellaneurisma documentata allangiografia eseguita al termine della procedura . 
la sicurezza stata definita come frequenza delle complicanze maggiori o minori ( classificate secondo il sistema della societ di radiologia interventistica [ 24 ] )  . analisi statistica i dati clinici sono stati registrati prospetticamente e tabulati con microsoft excel ( microsoft corp , redmond , wa , usa )  . 
 le variabili continue sono state testate per la distribuzione normale con il test di kolmogorov - smirnov e comparate tra i gruppi con il test t di student per i valori distribuiti normalmente ; in caso contrario stato utilizzato il test u di mann - whitney . 
3a , b type b ruptured aneurysm with right anteromedial aortic hole as shown on preoperative cta ( a1 , arrow ) and also detected during intraoperative aortography ( a , arrow ) treated in 14 min ( arrows in the right upper angles of the angiographic images ) with a transrenal aorto - uni - iliac endograft ( b )  . 
3a , b aneurisma rotto di tipo b con punto di rottura in sede anteromediale , come mostrato dalla cta pre - operatoria ( a1 , freccia ) e come evidenziato anche durante laortografia intra - operatoria ( a , freccia ) , trattato in 14 minuti ( vedi frecce negli angoli in alto a destra delle immagini angiografiche ) con unendoprotesi transrenale aorto - uniliaca ( b )  . 
the zenith eg was the only aui device used , with a mean diameter of 283 mm ; an 8 - mm dacron graft was the most frequent prosthesis used to carry out the femorofemoral bypass . 
 mean intervention duration was 11344 ( range 50180 ) min ; a mean of 4 u of packed red blood cells and 2 u of radiol med ( 2012 ) 117 : 410425 guita mediante spss , release 13.0 per windows ( spss inc , chicago , ill , usa )  . risultati tredici pazienti ( 30 , 9% ) hanno ricevuto unep aui ( gruppo a ) e 29 bif ( gruppo b )  . 
un pallone occlusore aortico stato utilizzato in 4 casi ( 9 , 5% ) , 1 nel gruppo a e 3 nel gruppo b . nei tredici pazienti del gruppo a , il diametro medio dellaneurisma risultato essere 7 , 31 , 3 cm ( range 610 ) ; 9 pazienti ( 69 , 2% ) erano emodinamicamente instabili . 
lemoglobinemia , la pressione arteriosa sistolica e la frequenza cardiaca media erano rispettivamente di 8 , 53 , 7 g / dl , 9018 mmhg e 10016 battiti / minuto . 
otto pazienti ( 61 , 5% ) hanno richiesto il ricovero in terapia intensiva . gruppo b nei 29 pazienti del gruppo b , il diametro medio dellaneurisma risultato di 7 , 51 , 6 cm ( range 3 , 711 ) ; 8 pazienti ( 27 , 6% ) erano emodinamicamente instabili . 
 la lunghezza media del colletto prossimale era di 18 , 37 mlanatomia pi frequente dellaneurisma era quella di tipo b : in 4 pazienti ( 13 , 8% ) stata necessaria la copertura di unarteria ipogastrica ( intenzionale n = 3 ) per consentire unadeguata sigillatura distale dellaneurisma , ma in nessun caso locclusione stata bilaterale ; non stato registrato alcun caso di ischemia colica . 
4a - c aneurisma rotto di tipo b in un paziente in shock : laortografia preliminare intra - operatoria ( a ) mostra un jet ( freccia ) nella porzione posterolaterale sinistra della sacca aneurismatica . 
la cta post - operatoria ( c ) conferma lesclusione della rottura ( freccia ) e lassenza di endoleak . freshfrozen plasma were infused ; eight patients ( 61.5% ) required intensive care unit ( icu ) stay . successo tecnico primario il tasso di successo tecnico primario stato del 100% . 
mean delay from admission to intervention was 11693 ( range 31340 ) mhaemoglobin , systolic blood pressure , and heart rate were 103 g / dl , 11928 mmhg and 9512 bpm , respectively . 
average length of the proximal neck was 18.37 mthe most frequent aneurysm anatomy was type b : four patients ( 13.8% ) required overstenting of a hypogastric artery ( intentional n = 3 ) to adequately seal off blood flow to the aneurysm , but none of the occlusions were bilateral ; no colonic ischaemia was encountered . 
mean intervention duration was 11958 ( range 60160 ) min ; a mean of 5 u of packed red blood cells and 2 u of freshfrozen plasma were infused ; nine patients ( 31% ) required icu stay . primary technical success primary technical success rate was 100% . additional procedures group a three patients ( 23% ) required an additional procedure : proxprocedure addizionali gruppo a tre pazienti ( 23% ) hanno richiesto una procedura addizionale : un posizionamento di una cuffia prossimale ( n = 1 ) per sigillare un endoleak prossimale , una pta preliminare per lunica arteria iliaca esterna utilizzabile ( n = 1 ) e un endoarteriectomia dellarteria femorale comune per ottimizzare lanastomosi del by - pass femoro - femorale ( n = 1 )  . gruppo b quattro pazienti hanno richiesto una procedura addizionale : un paziente presentava una morfologia sfavorevole dellaneurisma con un colletto prossimale risultato troppo corto pertanto stato necessario il posizionamento di una cuffia prossimale , con copertura di entrambi gli osti delle arterie renali , al fine di sigillare un endoleak di tipo 1 , mentre in 3 casi stata necessaria una pta preliminare di una delle arterie iliache per facilitare il posizionamento dellep . successo clinico primario il successo clinico primario stato del 95 , 3% ( 40 / 42 )  . 
complessivamente , 12 pa418 group b group a group b safety group a imal cuff ( n = 1 ) to seal a proximal endoleak , preliminary percutaneous angioplasty ( pta ) of the only viable external iliac artery ( n = 1 ) and endarterectomy of the common femoral artery to optimise the femorofemoral anastomosis ( n = 1 )  . zienti ( 28 , 5% ) sono morti entro 30 giorni : 9 pazienti sono deceduti nelle prime 48 ore ed altri 3 pazienti entro due settimane dallintervento . 
il tasso di morte durante il ricovero stato del 30 , 5% ( 13 / 42 )  . radiol med ( 2012 ) 117 : 410425 four patients ( 13.8% ) required an additional procedure : one had unfavourable aneurysm morphology with too short a neck and therefore an additional proximal cuff was placed across both renal artery ostia to seal a proximal type 1 endoleak ; in three cases , a preliminary pta of one iliac artery was performed to facilitate eg deployment . primary clinical success primary clinical success was 95.3% ( 40 / 42 )  . 
in particolare , 6 / 8 pazienti sono deceduti durante le prime 48 ore : le cause di morte sono state lo shock intrattabile ( n = 5 ) , linsufficienza multi - organo ( mof , n = 2 ) e linfarto miocardico acuto ( n = 1 )  . la mortalit complessiva in questo gruppo stata del 17 , 2% ( n = 5 )  . 
in particolare , 4 pazienti sono deceduti nelle prime 48 ore per le conseguenze di uno shock intrattabile ( n = 2 ) , la rottura di un aneurisma dellarco aortico misconosciuto ( n = 1 ) e per linsorgenza di mof ( n = 1 )  . 
one patient died 40 days after the intervention due to an acute myocardial infarction . gruppo b there were four major complications ( 30.7% ) of a total of six : acute renal insufficiency ( n = 2 ) that did not required dialysis ; intra - abdominal compartment syndrome ( n = 2 ) that did not necessitate drainage ; respiratory insufficiency ( n = 1 ) without a need for tracheostomy ; distal type 1 endoleak ( n = 1 ) ( this patient was alive at the time of writing but refused further treatment )  . 
no other patients underwent additional intervention . sono state registrate 4 complicanze maggiori ( 30 , 7% ) su un totale di 6 complicanze : insufficienza renale acuta non necessitante trattamento emodialitico ( n = 2 ) , sindrome compartimentale intra - addominale senza necessit di drenaggio ( n = 2 ) , insufficienza respiratoria senza necessit di tracheostomia ( n = 1 ) ed un endoleak distale di tipo 1 ( n = 1 ) : questultimo paziente ancora vivo , ma ha rifiutato qualsiasi ulteriore trattamento . 
 sono state riscontrate complicanze maggiori in 8 pazienti ( 27 , 6% ) , comprendenti lendoleak ( n = 3 ) , in particolare due di tipo 1 ( un caso di posizionamento di una cuffia prossimale , n = 1 , mentre laltro paziente ha rifiutato lintervento , n = 1 ) ed uno di tipo 2 ( risoluzione spontanea al follow - up a 4 mesi ) , linsufficienza renale acuta ( n = 1 ) a seguito della copertura intenzionale di entrambe le origini delle arterie renali , la sindrome compartimentale intra - addominale ( n = 1 ) trattata con evacuazione chirurgica mediante approccio extraperitoneale con laparotomia a livello della fossa iliaca sinistra , la polmonite ( n = 2 ) e uno pseudoaneurisma femorale ( n = 1 ) che ha richiesto correzione chirurgica . group b interventi secondari major complication occurred in eight patients ( 27.6% ) : encomplessivamente gli interventi secondari sono stati : un radiol med ( 2012 ) 117 : 410425 doleak ( n = 3 ) , in particular two type 1 ( additional cuff n = 1 ; refused intervention n = 1 ) and one type 2 ( spontaneously thrombosed at 4 months follow - up ) ; acute renal failure ( n = 1 ) following intentional coverage of both renal artery origins ; intra - abdominal compartment syndrome ( n = 1 ) treated with surgical evacuation through an extraperitoneal approach via a left iliac fossa cutdown ; pneumonia ( n = 2 ) ; femoral pseudoaneurysm ( n = 1 ) that required surgical correction . secondary interventions overall , secondary interventions were a femorofemoral bypass performed at 2 months to treat thrombosis of an iliac limb , and one proximal type 1 endoleak sealed with an additional cuff at 12 months follow - up . 
no further endoleaks were observed , and no further interventions were performed . by - pass femoro - femorale stato eseguito dopo due mesi dallintervento per trattare una trombosi di una branca iliaca ed un endoleak prossimale di tipo 1 stato sigillato mediante il posizionamento di una cuffia addizionale dopo 12 mesi di follow - up . 
non sono stati osservati altri endoleaks , n sono stati necessari ulteriori interventi . risultati statistici allanalisi unie multivariata , i sottogruppi sono risultati omogenei per genere , et , dimensione e morfologia dellaneurisma , tipo di diagnosi , intervallo di tempo e valori dei parametri al momento del ricovero ; la frequenza di shock risultata statisticamente pi elevata nel gruppo a . 
considerando i dati operativi , la mortalit durante la degenza risultata statisticamente pi elevata nel gruppo a ( tabella 1 ) ; il tipo di ep ed il ricovero in terapia intensiva sono risultati gli unici predittori indipendenti di mortalit ( tabella 2 )  . 
 statistical results at univariate and multivariate analyses , the subgroups were well matched for gender , age , aneurysm size and morphology , type of diagnosis , delay and parameter values at admission ; shock was statistically more frequent in group a . 
 considering the operative data , in - hospital mortality was statistically higher in group a ( table 1 ) ; eg type and icu admission were the only independent predictors of in - hospital mortality ( table 2 )  . discussion since 1997 , when the aui was first proposed for eevar , several others groups have adopted a similar eg system for raaa management [ 8 , 14 , 2527 ]  . 
the aui system could present several advantages , being particularly useful in emergency settings : simplification of operative technique and device characteristics ; rapidity of deployment also related to the fact of not having to place the contralateral gating , as in the bif system ; the shorter learning curve . 
 [ 29 ] treated half of their patients without an interventional radiologist being present in the operating room , reporting a median time to rupture exclusion of 30 min and a total 150 min to complete the intervention with the femorofemoral bypass graft ; verhoeven et al . 
 il sistema aui presenta alcuni vantaggi , particolarmente utili in emergenza : semplificazione della tecnica operativa e delle caratteristiche del device , rapidit di posizionamento ( grazie anche al fatto che non va posizionato il gating controlaterale , come per il sistema biforcato ) ed una ridotta curva di apprendimento ; questi fattori contribuiscono ad un aumento nel numero dei pazienti trattabili con eevar . 
 [ 29 ] hanno trattato la met dei loro pazienti senza la presenza di un radiologo interventista in sala operatoria , riportando un tempo medio di esclusione della rottura di 30 minuti ed un totale di 150 minuti per completare lintervento con il confezionamento del by - pass femoro - femorale ; nella casistica presentata da verhoeven et al . 
we believe there are two potential reasons to explain this observation : the much shorter time to deploy the aui device allowed a much longer time to perform the femorofemoral bypass graft ; the need in the bif group to perform secondary procedures , such as balloon clamping and / or pta of the iliac arteries . 
the first reason was mandatory to stabilise the patient , whereas the latter was not relevant for eg deployment but necessary to optimise the implantation procedures . in eevar treatment , preference for the aui system by sebbene la seconda non fosse importante per il posizionamento della ep , ma necessaria per ottimizzare la procedura di impianto . 
 nelleevar , la preferenza per il sistema aui da parte di molti autori , pu essere attribuita alla sua semplicit e rapidit di posizionamento e alla grande adattabilit anatomica ; per queste ragioni , la preferenza per questo device , supportata sia da esperienze pubblicate da singoli centri che da studi multicentrici [ 26 , 29 , 31 , 32 ]  . 
however , this preference is not supported on the whole by other studies , which collectively have a mean aui use of 46.2% , as the use of a femorofemoral prosthetic bypass is considered a disadvantage by some , carrying risks such as late occlusion or infection [ 32 , 33 ]  . 
in a european multicentre trial [ 28 ] on eevar , only one patient had a prosthetic infection , which was successfully treated by replacing the crossover bypass with a vein graft ; a literature review [ 34 ] concluded that the complication rate of femorofemoral bypasses in combination with aui devices was low and the long - term patency excellent . 
 we agree that selecting an aui system is of extraordinary importance in the setting of haemodynamic insufficiency owing to the rapidity of deployment , but we also experienced , as previously reported [ 35 ] , a still high mortality rate when an aui system was used , which could reflect the severity of the circulatory collapse [ 28 , 31 ]  . 
 [ 29 ] hanno dimostrato che laui una ep che pu essere utilizzata per la riparazione di aaa sintomatici acuti ed in rottura , con una mortalit perioperatoria che viene paragonata positivamente con i dati pubblicati per or convenzionale e con quelli riportati nel trial europeo [ 28 ] , analizzando le serie di pazienti in cui stata posizionata tale ep , occorrerebbero alcune precisazioni che riguardano : errori di selezione , presenza di differenti co - morbilit ed un piccolo numero di pazienti trattati con tecnica endovascolare . 
nella nostra esperienza , abbiamo incluso solo pazienti con documentata rottura dellaaa , ed un importante differenza in termini di mortalit stata riportata 422 radiol med ( 2012 ) 117 : 410425 presence of different comorbidities ; and a small number of patients treated endovascularly . 
in our experience , we included only patients with documented rupture , but an important difference in terms of mortality was noted between patient subgroups : haemodynamic condition strongly influenced outcomes [ 36 ]  . 
 [ 37 ] , in which patient - related predictors of outcome such as age , loss of consciousness and haemoglobin were independently associated with in - hospital mortality , in our multivariate analysis , the type of eg and icu admission were the only independent factors of mortality . 
it has been reported that the main disadvantage of the bif system is the need for a potentially difficult catheterisation in a patient who continues to bleed through the contralateral gate , although some centres have used the bif system under local anaesthesia with encouraging results , and some technical tricks may be helpful in these situations , such as the use of an occluding balloon [ 39 ]  . 
local anaesthesia carries some potential drawbacks , including patient discomfort and movement artefacts ; in fact , one disadvantages of the aui system is that guidewire placement and eg delivery could be done under local anaesthesia in the groin , but the ischaemic pain during the femorofemoral crossover is generally too great for most patients [ 30 , 40 ]  . 
 we believe that eevar for raaa could be performed under local anaesthesia in patients with stable haemodynamic condition , able to cooperate with the surgical team and have no signs of ischaemic organ failure [ 30 , 41 ]  . 
these considerations are based on the fundamental semantic concept of a raaa : in fact , if haemorrhagic shock is present at admission , the patient should be treated with resuscitation first , whereas if the aneurysm is symptomatic but intact , initial anaesthetic management could be more liberal [ 42 ]  . 
 indeed , we emphasise that in contrast to most of the reported experiences , in our series , only documented raaa were included : the decision to perform a general anaesthesia should not be considered standard procedure ; rather , it must be kept in mind that it is a complex manoeuvre , differentiable in every component depending on the patients status . 
 [ 37 ] , in cui let del paziente , la perdita di coscienza e labbassamento dei valori di emoglobina erano i fattori correlati con la mortalit intraospedaliera , nella nostra analisi multivariata , il tipo di ep e laccesso nella unit di terapia intensiva ( icu ) erano gli unici fattori correlati con la mortalit . interessante notare che , lo shock era statisticamente pi frequente nei pazienti che hanno messo la endoprotesi aui , rispecchiando le condizioni emodinamiche peggiori del paziente al suo ingresso . 
 lanestesia locale ha alcuni svantaggi , come il discomfort per il paziente e gli artefatti da movimento ; infatti , uno degli svantaggi del sistema aui che la guida ed il device possono essere posizionati in anestesia locale , ma il dolore ischemico durante il confezionamento del by - pass femoro - femorale generalmente troppo intenso per questi pazienti [ 30 , 40 ]  . 
 noi crediamo che il posizionamento endovascolare di una endoprotesi aortica pu essere eseguito in anestesia locale in pazienti con condizioni emodinamiche stabili , capaci di collaborare con il team chirurgico , ed in assenza di sintomatologia ischemica [ 30 , 41 ]  . 
queste considerazioni sono basate su un fondamentale concetto : infatti , se il paziente allingresso in shock emorragico , deve essere prima rianimato , mentre se laneurisma sintomatico ma intatto , la gestione dellanestesia pu essere pi libera [ 42 ]  . 
contrariamente a quanto riportato nella maggior parte delle esperienze citate , abbiamo incluso nel presente studio solo pazienti con aaa in rottura : la decisione di eseguire una anestesia generale non pu essere considerata una procedura standard , piuttosto deve essere tenuto presente che una manovra complessa , differenziabile in tutte le sue componenti in relazione alle condizioni del paziente . 
oggi , gli anestetici di ultima generazione permettono di eseguire una anestesia generale anche in pazienti in condizioni emodinamiche non ottimali contenendo la riduzione dei valori pressori durante la fase di induzione , prevenendo , allo stesso tempo , la stimolazione simpatica che comporterebbe picchi ipertensivi , pericolosi soprattutto in questo ambito [ 42 ]  . in uno studio che aveva un follow - up di 10 anni , la percentuale delle complicanze dopo riparazione degli aaa era doppia rispetto a quelle viste nelle riparazioni degli aaa in elezione ( 17% versus 8% ) [ 43 ]  . 
una delle complicanze pi sottostimate , e probabilmente poco riportata , quella che deriva da un errore delloperatore ; nella serie di pazienti radiol med ( 2012 ) 117 : 410425 most underestimated , and probably underreported , issues of the eevar is the complication rate as a direct result of operator error . 
 [ 29 ] , one eg was deployed too proximally , thus occluding both renal arteries , and three major complications ( two bilateral renal artery occlusions and one migration ) were encountered during retrieval of the delivery systein our experience , we encountered one case of unintentional coverage of a hypogastric artery and one case of intentional coverage of the origins of both renal arteries secondary to positioning an additional proximal cuff to seal a proximal type 1 endoleak . 
 this compares favourably with the published reports but also suggests that operator errors should not be surprising given the emergent setting in which the procedure is done and the possible adverse aneurysm morphology . 
therefore , we believe that patients with raaa may be ideal candidates for endovascular surgery provided that the aneurysm has suitable anatomy , but further analyses should focus on which patients could most benefit from the endovascular approach in order to obtain a positive final outcome despite initial clinical condition [ 44 , 45 ]  . in our experience , the rate of eevar for raaa is higher than in most previous studies ; the eg configuration was dictated by the patients haemodynamic condition at admission . 
 [ 29 ] , una ep era stata posizionata troppo prossimalmente occludendo lostio delle arterie renali , e 3 complicanze maggiori ( 2 casi di occlusione bilaterale delle arterie renali ed una migrazione ) sono state registrate durante il recupero del device . 
nella nostra esperienza , stato registrato un caso di non intenzionale copertura della arteria ipogastrica ed un altro caso di copertura intenzionale dellostio di entrambe le arterie renali durante il posizionamento di un allungamento prossimale per il trattamento di un endoleak di tipo i . 
questo in accordo con quanto pubblicato in letteratura e suggerisce che gli errori degli operatori non devono sorprendere per la condizione di emergenza della situazione in cui viene svolta la procedura e la possibile morfologia sfavorevole dellaneurisma . 
inoltre , da ricordare che lo scopo del posizionamento di una ep aortica per via percutanea in aaa in rottura quello di salvare la vita del paziente , a differenza di quanto ci si prefigge in elezione . 
ulteriori studi si sono focalizzati sulla selezione del paziente in cui sia indicato lapproccio percutaneo , cos da ottenere un buon risultato finale nonostante le condizioni allingresso non siano ottimali [ 44 , 45 ]  . nella nostra esperienza , la percentuale di pazienti sottoposti a posizionamento di ep per riparare aaa in rottura con approccio percutaneo , pi alta che negli studi precedenti ; la scelta della ep stata dettata dalle condizioni emodinamiche allingresso . 
 + 39 - 0823 - 854196 , fax + 039 - 0823 - 851941 , e - mail : mscaglione@tiscali.it received : 27 december 2010 / accepted : 11 april 2011 / published online : 18 november 2011 springer - verlag 2011 abstract nontraumatic acute thoracic aortic syndromes ( aas ) describe a spectrum of life - threatening aortic pathologies with significant implications on diagnosis , therapy and management . 
in this context , multidetector computed tomography ( mdct ) is the gold standard due to its intrinsic diagnostic value ; its performance approaches 100% sensitivity and specificity , and it is accepted as a first - line modality for suspected acute aortic disease . 
 mdct allows early recognition and characterisation of acute aortic syndromes as well as the presence of any associated complications findings that are essential for optimising treatment and improving clinical outcomes . 
we reviewed the classic and less common ct findings , correlating them with pathophysiology , timing and management options , to achieve a definite and timely diagnostic and therapeutic definition . keywords acute thoracic aortic syndromes aortic dissection intramural hematoma penetrating aortic ulcer multidetector - row ct management riassunto di recente sistematizzazione , le sindromi aortiche acute rappresentano uno spettro di condizioni patologiche assai temibili per le notevoli implicazioni diagnostiche , terapeutiche e gestionali . 
in questo contesto , la tomografia computerizzata multidetettore ( tcmd ) attualmente il gold standard per il suo intrinseco valore diagnostico , con sensibilit e specificit vicine al 100% , e costituisce la tecnica di imaging di scelta per sospetta patologia aortica acuta . 
la tcmd consente il riconoscimento precoce e la caratterizzazione delle sindromi aortiche acute , nonch la presenza di eventuali complicanze associate , con risultati essenziali per ottimizzare il trattamento e migliorare la prognosi . 
lo scopo di questo lavoro rivedere la semeiotica classica e soprattutto evidenziare gli aspetti tc meno frequenti , correlandoli alla fisiopatologia , al timing e alle opzioni gestionali al fine di raggiungere una pi precisa e tempestiva definizione diagnostica e terapeutica . parole chiave sindromi aortiche acute dissezione aortica ematoma intramurale ulcera aortica penetrante tc multidetettore gestione introduction introduzione knowledge about aortic diseases has grown considerably and continues to evolve , with ongoing research into pathophysiology , and technological advances for detecting and improvle conoscenze sulla patologia aortica sono notevolmente accresciute e continuano a progredire parallelamente alla ricerca sulla fisiopatologia del vaso , ai progressi tecnolo394 radiol med ( 2012 ) 117 : 393409 ing therapeutic options . 
acute aortic syndrome ( aas ) refers to a spectrum of emergencies , including aortic dissection ( ad ) , acute intramural haematoma ( imh ) and penetrating atherosclerotic ulcer ( pau ) [ 14 ] , causing a series of signs and symptoms , the foremost of which is chest paall these conditions may lead to aortic rupture , making timely diagnosis and treatment crucial for a favourable prognosis and patient outcome . 
in particular , it is critical to diagnose ad , the most common aortic disease , as prompt identification can significantly decrease patient mortality rates and have a favourable impact on survival rate [ 57 ]  . 
in ad , overall outcome is determined by disease type and extent and the presence of associated complications ; therefore , evaluation of the entire aorta , branch vessels and iliac and proximal femoral arteries is mandatory for tailored treatment planning . 
 contrast - enhanced cardiac - gated multidetector ct ( mdct ) is considered the gold standard in aas because of its nearly 100% sensitivity and specificity [ 79 ]  . 
most importantly , its high spatial and temporal resolutions are crucial in assisting the physician to accurately diagnose severely ill patients , independently of the patients body habitus and compliance [ 10 , 11 ]  . 
the aim of this review was to present the common and uncommon ct findings of aas , correlating ct signs with pathophysiology , timing and therapeutic options , as these aspects are critically important for establishing an accurate diagnosis and timely treatment . mdct study protocol and technical notes between may 2007 and october 2010 , 94 patients with aas were referred to our level - ii cardiovascular emergency hospital and promptly examined with an emergency mdct . 
 images were obtained with 16and 64 - mdct scanners ( brilliance ct 16 - slice philips , healthcare philips medical systems , best , the netherlands ; lightspeed vct 64 - slice ge , ge medical system , milwaukee , wi , usa )  . 
the study scanning protocol covered from the lung apices to the gro each ct study started with an unenhanced ct scan of the thorax to assess any spontaneous aortic hyperdensity and / or periaortic soft - tissue abnormality . 
le sindromi aortiche acute non traumatiche ( aas ) rappresentano uno spettro di condizioni di emergenza comprendenti la dissezione aortica ( ad ) , lematoma intramurale acuto ( imh ) e lulcera penetrante aterosclerotica ( pau ) [ 14 ] che causano una serie di segni e sintomi , primo tra i quali il dolore toracico acuto . 
in particolare nella dissezione acuta , la pi comune patologia aortica , la rapida identificazione diagnostica essenziale nel ridurne significativamente la mortalit , con un impatto favorevole sulla tasso di sopravvivenza [ 57 ]  . 
la prognosi della ad determinata dal tipo e dallentit della malattia e dalla presenza di complicanze associate ; di conseguenza , la valutazione dellintera aorta , delle collaterali , delle arterie iliache e femorali prossimali obbligatoria per la corretta pianificazione del trattamento . 
attualmente , la tomografia computerizzata multidetettore ( tcmd ) con mezzo di contrasto endovenoso ( mdc ) , cardio - sincronizzata , considerata il gold standard nella diagnosi delle aas , con valori di sensibilit e specificit prossimi al 100% [ 79 ]  . 
soprattutto lelevata risoluzione spaziale e temporale della metodica sono cruciali al fine di una diagnosi accurata in pazienti gravemente malati , indipendentemente dal loro habitus corporeo [ 10 , 11 ]  . 
scopo di questo lavoro quello di presentare i segni tc comuni e meno comuni nelle aas , correlandoli con gli aspetti fisiopatologici , i tempi e le opzioni terapeutiche , il che di importanza critica per ottenere una diagnosi accurata ed un trattamento tempestivo . protocollo di studio tcmd e note tecniche tra maggio 2007 ed ottobre 2010 , 94 pazienti con aas sono giunti al centro di emergenza / urgenza cardio - vascolare di ii livello della nostra azienda ospedaliera e sono stati tempestivamente sottoposti a tcmd . 
le immagini sono state ottenute con apparecchiature tcmd a 16 e 64 file di detettori ( brilliance ct 16 - slice philips , healthcare philips medical systems , best , paesi bassi ; lightspeed vct 64 - slice ge , ge medical system , milwaukee , wi , usa )  . 
arterial - phase imaging was planned to coincide with arterial contrast opacification of the entire lumen ; a double arterial acquisition was performed in the case of weak opacification of the false distal lumen . 
 common ct findings typical ct findings of ad are well known [ 1 , 2 , 6 , 1518 ] and include direct visualisation of media - intima entrance tear from true to false lumen as a distinct intimal flap defect , and different morphology of the true and false lumen , with the true lumen usually smaller and more intensely opacified than the false lumen in the early angiographic phase due to higher pressure and faster mixing with blood , whereas the false lumen is likely to be crescent - shaped , with acute angles ( beak sign ) between detached intima and the aortic wall [ 19 , 20 ]  . 
in some cases , media - intima separation is not complete , and cobwebs or tendrils of the media layer ( cobweb sign ) persist between the intima and media , generally over short segments of the dissection [ 21 ]  . 
further crucial findings include involvement of the collateral branches arising from the aorta and associated lesions , such as haemopericardium , haemomediastinum , renal or splenic infarctions and limb ischaemia . 
thus , when aas is suspected , it is useful to perform unenhanced ct scans because extensive atherosclerosis and imh are easily seen on unenhanced ct , whereas contrast material may obscure haemorrhage within the aortic wall . 
finally , an additional observation that helps differentiate imh from a thrombosed false lumen is that in typical ad , the former remains in a constant , circumferential relationship with the aortic wall , whereas the latter tends to spiral longitudinally around the aorta [ 23 ]  . 
differential diagnoses include all entities that may cause aortic - wall thickening , such as aortitis , intraluminal thrombosis and soft atheromatous plaque . pau is a focal atherosclerotic plaque that corrodes a variable depth through the intima into the media ; it is a frequent qualsiasi piano , consentendo ricostruzioni multiplanari e immagini in 3d di buona qualit . 
il bolo di mdc ( volume totale di 60130 ml di mdc non ionico a bassa osmolarit alla concentrazione di 370 o 400 mgi / ml ) stato iniettato ad una velocit di 35 ml / s attraverso unago - cannula 1820 g , inserita , se possibile , nel braccio destro , attraverso iniettore a due vie ( stellant sct 211 , medrad , indianola , ia , usa ) , con la tecnica del bolus triggering con unica regione di interesse ( roi ) posizionata nellaorta ascendente o nellarco aortico [ 12 14 ] ; il bolo di contrasto iodato stato seguito , di routine , dalla soluzione fisiologica . 
infine , in casi selezionati , una fase venosa tardiva stata utile per ottenere la valutazione ottimale dei parenchimi . segni tc comuni i segni tc comuni nella ad sono ben noti [ 1 , 2 , 6 , 1518 ] e comprendono la diretta visualizzazione della breccia di ingresso o lacerazione medio - intimale dal vero al falso lume come un distinto difetto o flap intimale , la diversa morfologia dei lumi : il vero lume di solito risulta pi piccolo e pi intensamente opacizzato del falso lume nella fase angiografica precoce a causa di pressioni pi elevate e di un flusso ematico ad alta velocit mentre il falso lume risulta pi ampio o semilunare con angoli acuti ( segno del becco ) tra intima scollata e parete aortica [ 19 , 20 ]  . 
 in alcuni casi , il distacco medio - intimale incompleto e brandelli di media , segno della ragnatela , o cobweb sign , persistono tra intima e media , generalmente in brevi segmenti della dissezione [ 21 ]  . 
ulteriori segni cruciali sono rappresentati dal coinvolgimento delle branche collaterali aortiche e dalle lesioni associate come emopericardio , emomediastino , infarti renali o della milza , lischemia degli arti . limh appare , nellesame precontrastografico , come un ispessimento iperdenso semilunare di parete aortica , corrispondente ad un ematoma della media vasale . 
cos , quando si sospetta una aas , utile eseguire scansioni tc preliminari senza mdc perch laterosclerosi ampia e limh sono facilmente visibili nella tc basale ( specie nel caso di sanguinamento recente ) , mentre il mdc pu , in qualche modo , mascherare lemorragia di parete 396 radiol med ( 2012 ) 117 : 393409 fig . 
b la tcmd dopo somministrazione di mdc per venam non mostra incremento densitometrico dellarea semilunare di parete aortica ( freccia ) ed appare meno evidente in fase post - contrastografica . ct finding in older patients . 
mild periaortic stranding should be mentioned if present , but it is not a definitive sign of rupture in stable / asymptomatic patients . uncommon findings at unenhanced ct hyperacute intimal flap in the early stages of acute ad , one may occasionally see a spontaneous hyperdense intimal flap , called a hyperacute flap , at unenhanced ct . 
infine , ulteriore segno che aiuta a differenziare limh dalla trombosi del falso lume tipico della ad che il primo ha un rapporto costante , circonferenziale con la parete aortica , mentre la seconda presenta andamento spiraliforme longitudinale lungo tutta laorta [ 23 ]  . 
limh va differenziato da tutte le altre patologie che causano un ispessimento della parete , come laortite , la trombosi parietale e la placca ateromasica . la pau una placca aterosclerotica focale ulcerata che supera lintima e si approfonda nella media ed un reperto tc pi frequente nella popolazione dei pazienti pi anziani . 
2a - c penetrating aortic ulcer : a unenhanced and b contrast - enhanced axial mdct image shows a focal contrast - material - filled pouch ( arrow ) that communicates with the aortic lumen but extends outward , beyond its normal circumference ; surrounding intramural haematoma ( asterisk )  . 
lindagine tcmd pre - contrastografica ( a ) e post - contrastografica ( b ) mostra unestroflessione focale di mezzo di contrasto , simil - ulcerosa ( freccia ) che comunica con il lume aortico ma si estende verso lesterno , al di l della suacirconferenza normale ; ematoma intramurale associato ( stella )  . 
c la ricostruzione in volume rendering mostra lulcera penetrante allistmo aortico ( freccia )  . pulsation artefacts are typically observed at the proximal ascending aorta , especially at the left anterior and right posterior aspects of the aortic circumference [ 32 ]  . 
location of artefacts is related to the pendular motion of the ascending aorta , which on axial scans demonstrates a position on the aortic circumference between 12 or 1 oclock and 6 or 7 oclock .they can be recognised on the basis of their characteristic location and are limited to one or two adjacent sections [ 32 ]  . 
these artefacts can be significantly reduced by shortening the scanning time or implementing electrocardiograph ( ecg ) triggering . aortic dissection with early thrombosed false lumen ad with early thrombosed false lumen can be recognised at unenhanced ct as a crescent - shaped , high - attenuation area in the aortic wall due to recent bleeding . 
some reports indicate that this kind of ad is associated with better clinical outcome [ 2 , 4 ]  . menzionato , se presente , ma non un segno conclusivo di rottura in pazienti stabili / asintomatici . segni tc meno comuni allesame non contrastografico flap intimale iperacuto nelle fasi precoci di una ad acuta si pu talora vedere nelle scansioni preliminari , pre - contrastografiche , un flap intimale spontaneamente iperdenso , da noi chiamato flap iperacuto . 
3a , b rupture of penetrating atherosclerotic ulcer : a unenhanced mdct coronal scan of the aortic arch shows a subintimal hyperdense haematoma in the aortic wall ( arrow )  . 
b lindagine tcmd post - contrastografica nella scansione coronale mostra lalesione ulcerata aortica e lo spandimento del mezzo di contrasto dal lume aortico ( freccia )  . uncommon findings at contrast - enhanced mdct disappearing or missing flap : circumferential intimal dissection with intimo - intimal intussusception in ad , the primary tear is usually > 50% of the aortic circumference , whereas full circumference is rarely involved . 
 a circumferential tear may lead to central displacement of the intimal - medial flap and intimo - intimal intussusceptions [ 3336 ] , presenting with either antegrade or retrograde intussusception . 
typically , this is a stanford type a lesion that usually originates near the coronary ostia and extends to the great vessels , being limited by attachments of the ascending aorta intima to the great vessels . 
the typical ct appearance of intimo - intimal intussusception includes visibility of a relatively short flap in the aortic root , absence of an intimal flap in the mid - ascending aorta , windsock linear or curvilinear filling defects in the livello dellaorta ascendente prossimale , specialmente sul profilo parietale anteriore sinistro e posteriore destro della circonferenza aortica [ 32 ]  . 
la sede degli artefatti legata al moto pendolare dellaorta ascendente , che nelle scansioni assiali si localizza tra le ore 12 / 13 e tra le 6 / 7 sulla circonferenza aortica . 
questi possono essere riconosciuti sulla base della loro sede caratteristica e sono limitati a uno o due scansioni adiacenti [ 32 ] ed , infine , essere significativamente ridotti limitando il tempo di scansione o attraverso la sincronizzazione ecg . dissezione aortica con trombosi acuta del falso lume la trombosi acuta del falso lume nella ad pu essere riconosciuta alla tc pre - contrastografica come semiluna iperdensa di parete aortica a causa del recente sanguinamento . 
alcuni lavori indicano che questo tipo di dissezione associato ad una prognosi migliore [ 2 , 4 ]  . segni meno comuni alla tcmd con mdc flap che scompare o perso ( dissezione circonferenziale con intussuscezione intimo - intimale ) nella dissezione la breccia di ingresso coinvolge generalmente pi del 50% della circonferenza aortica , mentre radiol med ( 2012 ) 117 : 393409 fig . 
4a - d uncommon appearance of type a aortic dissection : a 64 - year - old man with acute symptom onset with tightness in the throat and numbness in the lower limbs 2 - h earlier . 
 a , c la tcmd in fase pre - contrastografica evidenzia spontanea iperdensit del flap iperacuto ( frecce ) sullascendente e sullarco ; b , d in fase post - contrastografica si ha conferma della sede del flap mediointimale , di tipo circonferenziale sullarco . aortic arch with involvement of aortic arch vessels , and circumferential tears just above the aortic valve [ 39 , 40 ]  . 
finally , intimo - intimal intussusception is rare , and because of the possible aortic wall rupture and / or neurological events , it is more often fatal than is classic ad . aortic - arch abnormality involvement normal human aortic arch and great vessels are formed by selective regression of vascular arches that connect the embryonic ventral and dorsal aorta [ 41 , 42 ]  . 
una dissezione a piena circonferenza pu portare allo spiazzamento centrale del flap medio - intimale ed allintussuscezione intimo - intimale [ 3336 ] , che si pu presentare sia come intussuscezione anterograda o retrograda . 
in genere , si tratta di una lesione tipo a di stanford che di solito origina in contiguit degli osti delle coronarie e si estende ai grossi vasi , dove limitata dalle adesioni dellintima dellascendente ai vasi epiaortici . 
5a - e a 67 - year - old man presenting to the emergency department with intense upper back pain : mdct scans show a intimal flap at the aortic root ; b , c absence of flap at the distal ascending aorta and proximal arch and d partial dissection flap at the middle aortic arch associated with a small haemopericardiu e volume - rendered mdct scan clearly demonstrates a flap ( arrow ) propagating from the aortic root to the midaortic arch . 
la tcmd in fase post - contrastografica mostra ( a ) flap medio intimale in corrispondenza della radice aortica ( b , c ) mancata evidenza del flap nellaorta ascendente distale e nellarco prossimale , d flap da dissezione parziale sullarco medio associato ad una piccola quota di emopericardio . 
e la ricostruzione in volume rendering dimostra continuit tra il lembo dellascendente e quello dellarco medio ( freccia ) , rendendo pi sicura la diagnosi di dissezione prossimale , di tipo a . 
allintervento chirurgico , si osserva intussuscezione intimo - intimale e si effettua un intervento di ricostruzione dellaorta ascendente e di parte dellarco . gression of vascular arches [ 43 ]  . 
6a - d a 62 - year - old hypertensive man presenting with acute chest pain : acute dissection involving the double aortic arch : dominant and aneurysmal right arch , hypoplastic and patent left arch . 
a estesa breccia di ingresso tra vero e falso lume ( freccia ) nellarco destro - posto ed aneurismatico ( b ) larco sinistro ipoplasico e pervio ( freccia ) si connette distalmente allaorta discendente . 
d la ricostruzione in volume rendering mostra chiaramente la continuit dellarco sinistro ipoplasico con larco destro ( stella ) , con la carotide comune ( asterisco ) e la succlavia di sinistra ( triangolo ) che si unisce distalmente alla discendente prossimale ( freccia )  . chial or oesophageal compression or abnormal blood flow , or because they are associated with congenital cardiovascular disease [ 44 ]  . 
left aortic arch with abnormal branching , right aortic arch , double aortic arch and interrupted aortic arch are the most frequent anomalies [ 43 , 4547 ]  . vascular rings are uncommon anomalies ( < 1% of all congenital cardiac defects ) with a similar frequency in both sexes and are caused by abnormal persistence or regression of one of the six embryonic aortic arches . 
la semeiotica tipica dellintussuscezione intimo - intimale alla tc comprende la visibilit di una flap relativamente breve nella radice aortica , lassenza dello stesso nellascendente media , difetti di riempimento lineari o curvilinei a banderuola , windsock sign , nellarco aortico con il coinvolgimento dei vasi epiaortici ed una breccia circonferenziale 402 radiol med ( 2012 ) 117 : 393409 fig . 
7a - d a 52 - year - old man complaining of acute chest pain for 2 days : a , b axial and sagittal maximum intensity projection ( mip ) mdct scans show a three - channel dissection in the aneurysmal proximal descending aorta with intimomedial tear ( arrow ) entering the false lumen from the true lumen , clearly demonstrated in the sagittal mip reconstruction . 
a , b le ricostruzioni in proiezione di massima intensit ( mip ) assiale e sagittale mostrano dissezione a tre lumi nellaorta discendente prossimale aneurismatica con breccia dingresso ( freccia ) tra vero e falso lume evidente nella ricostruzione sagittale . 
patients with a lusoria artery seem to be more predisposed to abnormal blood vessel dissection , probably because its emergence is a site of least resistance . complex flap morphology and / or multichannel lumen rarely , a three - channel dissection can be seen if a secondary dissection occurs within one of the channels , with a resulting intimal flap giving rise to the mercedes - benz sign or other complex and bizarre morphologies [ 49 , 50 ]  . 
infine , lintussuscezione intimo - intimale rara e per la possibile rottura della parete aortica e / o per la comparsa acuta di accidenti neurologici , pi spesso fatale della classica ad . 
 coinvolgimento delle anomalie dellarco aortico larco aortico umano normale ed i vasi epiaortici si formano per un processo di regressione selettiva degli archi vascolari che collegano laorta ventrale e dorsale embrionarie [ 41 , 42 ]  . 
dopo 8 settimane di vita fetale larco aortico in via di sviluppo ed i vasi epiaortici pervengono alla loro configurazione definitiva attraverso la regressione selettiva degli archi vascolari [ 43 ]  . 
although these lesions may mimic penetrating ulcerations or ulcer - like projections ( ulp ) and are associated with imh , they actually represent focal mural haematoma communicating with both the native aortic lumen and side - branch ostium by a tiny orifice < 2 mm in diameter [ 54 ]  . 
shearing injury is caused by haematoma propagation across the origin of the branch vessel ; the origin of the intercostal or bronchial artery is thus interrupted , resulting in a small , high - attenuation , rounded focus , which is contiguous with the extra - aortic tubular course of the vessel [ 54 , 55 ]  . anticoagulant therapy or coagulation disorders may cause increased imh thickness periosteal focal collections of contrast medium or psa at the emergence of the bronchial and intercostal arteries . 
in accordance with williams et al . , [ 53 , 55 ] , we believe that extravasation of blood originating from intimal breakdown injuries at the emergence of an aortic branch artery , site of least resistance , can determine imh progression and increase its thickness ; however , wu et al . 
 [ 54 ] report that intramural blood pools are often associated with a relatively benign clinical course , with complete resorption or stability in most patients , as seen in our experience . 
many pathological entities enter the differential diagnosis with multiple - branch artery psa / ibp in imh , including initial progression of imh to overt dissection , ulp and pau . 
 in pau , depending on the different mechanism of injury , such extravasation does not appear along the emergence of side branches but along the pleural surface of the aorta , and the gaping communication with the aortic lumen is wider and constantly evident [ 53 , 55 , 58 ]  . 
un arco aortico sinistro con collaterali anomale , larco aortico destro , il doppio arco aortico e linterruzione dellarco sono le anomalie pi frequenti [ 43 , 4547 ]  . gli anelli vascolari sono anomalie poco comuni ( < 1% di tutti i difetti cardiaci congeniti ) con una frequenza simile in entrambi i sessi e sono causate da abnorme persistenza o regressione di uno dei sei archi aortici embrionali . 
i pazienti con arteria lusoria sembrano essere predisposti alla dissezione probabilmente perch lemergenza del vaso anomalo costituisce un locus minoris resistentiae . flap a morfologia complessa e / o lume multicanale raramente possibile trovare una morfologia a tre canali se una dissezione secondaria si verifica allinterno di uno dei canali , con i flaps intimali che danno origine al segno della mercedes - benz o ad altre morfologie complesse e bizzarre [ 49 , 50 ]  . 
lincidenza di questo tipo di dissezione maggiore in pazienti con sindrome di marfan [ 51 , 52 ]  . pseudoaneurismi o raccolte ematiche intramurali delle collaterali nellimh un meccanismo proposto per lo sviluppo della dissezione da un imh preesistente legato alla presenza di picco le raccolte focali ematiche di mdc sul decorso delle collaterali aortiche o pseudoaneurismi ( psa ) [ 53 ] o raccolte ematiche intramurali ( ibp ) [ 54 ]  . 
anche se queste lesio ni possono simulare ulcere penetranti o aggetti simil - ulcerosi ( ulp ) e sono associate allimh , esse rappresenta no in realt ematomi focali di parete che comunicano sia con il lume aortico nativo che con lostio della collaterale attraverso un piccolo orifizio del diametro inferiore ai 2 mm [ 54 ]  . 
la propagazione dellematoma allemergen za della collaterale causa lesioni da taglio ; lorigine dellarteria intercostale o bronchiale cos interrotta , dando luogo ad un piccolo focus iperdenso tondeggiante contiguo al decorso tubulare extra - aortico della collaterale [ 54 , 55 ]  . la terapia anticoagulante o disturbi della coagulazione possono causare un aumentato spessore dellimh e radiol med ( 2012 ) 117 : 393409 404 fig . 
 d two days after low - dose anticoagulant therapy , follow - up mdct scan shows thromboembolism regression and e , f small collections of contrast material within the imh at the emergence of bronchial arteries ( not shown ) and at three intercostal arteries ( t10 level shown )  . 
d al controllo tc , dopo due giorni di terapia anticoagulante a basso dosaggio , si apprezza regressione della tromboembolia ; e , f in corrispondenza dellemergenza delle arterie bronchiali ( non mostrato ) e di tre arterie intercostali ( viene mostrato il livello t10 ) , si apprezzano piccole raccolte di mezzo di contrasto nel contesto dellematoma intramurale . 
lo pseudoaneurisma dellarteria intercostale in continuit tra il lume aortico e la collaterale e si pone in diagnosi differenziale con unulcerazione focale penetrante . radiol med ( 2012 ) 117 : 393409 fig . 
9a - d le ricostruzioni mip in fase pre - contrastografica coronale ( a ) e sagittale ( b ) mostrano ematoma intramurale spontaneamente iperdenso rispettivamente sullaorta ascendente e discendente . 
d la ricostruzione in volume rendering mostra chiaramente stravaso del mezzo di contrasto nel contesto dellematoma ( freccia )  . branch - vessel involvement originating from the true lumen associated with malperfusion syndrome mdct provides optimal details concerning potential involvement of branch vessels and their origin from the true or false lumen . 
in accordo con williams [ 53 , 55 ] , noi crediamo che lo stravaso ematico originato dalla lesione dellintima della collaterale allemergenza , sede di minor resistenza , possa determinare la progressione dellematoma intramurale , un incremento del suo spessore , anche se 406 fig . 
10a , b a 68 - year - old man presenting with acute thoracoabdominal pain of 10 h ; malperfusion syndrome with acute gastroduodenal necrosis : a mdct shows dissection extension to the abdominal aorta . 
b close - up view shows that the superior mesenteric artery originates from the true lumen but is isodense to the false lumen , which shows greater opacification than the crescentic and increasingly thin true lumen crushed by the false lumen . 
b limmagine di dettaglio evidenzia che larteria celiaca origina dal lume vero , ma isodensa al falso lume , maggiormente opacizzato rispetto al vero che filiforme perch compresso dal falso lume . 
il paziente deceduto nonostante il tentativo di fenestrazione chirurgica . anisms are described by analogy to conventional atheromatous lesions that reduce arterial calibre in the form of ostial or proximal stenosis . 
 [ 54 ] riferiscono che le ibp sono spesso associate ad un decorso relativamente benigno con riassorbimento completo o stabilit nella maggior parte dei pazienti , come risulta anche dalla nostra esperienza . 
molte condizioni patologiche entrano in diagnosi differenziale con lo psa / ibp della collaterale nellimh , tra cui la fase iniziale di progressione dellimh in dissezione franca , lulp e la pau . 
 nella pau , a causa del differente meccanismo della lesione , questo stravaso non compare lungo lemergenza delle collaterali , ma sulla superficie pleurica dellaorta e la comunicazione con il lume aortico pi ampia e costantemente evidente [ 53 , 55 , 58 ]  . 
lintima contigua non mostra di solito una placca aterosclerotica , che spesso presente nellulcera aterosclerotica penetrante [ 59 ]  . il coinvolgimento di una collaterale che origina dal lume vero associato a sindrome da malperfusione la tcmd fornisce informazioni dettagliate riguardanti il potenziale coinvolgimento delle collaterali e la loro origine dal lume vero o falso . 
queste informazioni sono cruciali per la pianificazione di un trattamento di sostituzione della radice aortica , sia per il posizionamento di uno stent intravascolare o per la procedura di fenestrazione . 
lischemia degli arti , mesenterica e renale si pu verificare per ipoperfusione da estensione del lembo di dissezione nelle collaterali o attraverso lemergenza della collaterale da un vero o falso lume sede di ridotta perfusione . 
locclusione dinamica pu portare a termine ischemia - infarto dorgano quando il flap intimale risparmia la collaterale , ma prolassa ripetutamente e ne occlude in maniera intermittente il suo orifizio [ 8 , 60 ]  . 
 [ 62 ] propongono un nuovo sistema di classificazione che tiene conto della posizione del flap e della estensione radiol med ( 2012 ) 117 : 393409 namic occlusion can lead to end - organ ischaemia if the intimal flap spares the branch vessel but repetitively prolapses and intermittently occludes its orifice [ 8 , 60 ]  . 
proposed a new classification system taking into account the position of the aortic flap and the potential extension of the dissection into the visceral arteries or ostial avulsion [ 62 , 63 ]  . 
 specific information in patients with aas include lesion characterisation ( ad and its variants ) , anatomical extent , measurements of aortic diameters for stent - graft planning , identification of true and false lumen , side branches , coronary arteries , aortic valve involvement and complications . 
in the emergency setting , therefore , emergency radiologists play a vital role in formulating a timely and definitive diagnosis and establishing the most appropriate management of such life - threatening situations . 
pau , cos come la dissezione , pu portare ad aneurisma e alla formazione di pseudoaneurisma e richiederne la riparazione urgente a causa del rischio di rottura aortica [ 38 ]  . 
informazioni specifiche nei pazienti con aas comprendono la caratterizzazione della lesione ( ad e le sue varianti ) , lestensione anatomica , le misurazioni dei diametri dellaorta per la pianificazione di uno stent - graft , lidentificazione di lume vero e falso , rami laterali , arterie coronarie , coinvolgimento della valvola aortica e complicazioni . 
in pronto soccorso , dunque , i radiologi demergenza svolgono un ruolo fondamentale nella formulazione di una diagnosi tempestiva e definitiva , indirizzando la gestione pi appropriata di situazioni di pericolo . conflict of interest none 1 . 
angelelli , unit operativa radiodiagnostica universitaria , azienda ospedaliera universitaria - ospedale , policlinico consorziale , piazza giulio cesare 11 , 70124 bari , italy , tel . : + 39 - 080 - 5478840 , fax : + 39 - 080 - 5592911 , e - mail : g.angelelli@radiologia.uniba.it received : 27 december 2010 / accepted : 31 march 2011 / published online : 21 october 2011 springer - verlag 2011 abstract purpose . 
lesion size ranged between 8 and 40 mmetastases from rcc were hyperattenuating in the arterial phase , metastases from breast cancer and lung cancer were hypoattenuating and metastases from uterine leiomyosarcoma were inhomogeneous . 
sono stati esaminati retrospettivamente gli esami tc di 17 pazienti , affetti da metastasi pancreatiche , secondarie a carcinoma renale in 8 casi , a leiomiosarcoma uterino in 2 casi , a carcinoma polmonare in 4 casi e a carcinoma mammario in 3 casi . 
le lesioni pancreatiche erano singole in 7 casi e multiple in 10 casi e le loro dimensioni variavano tra 8 e 40 mle metastasi secondarie a carcinoma renale erano iperdense in fase arteriosa , quelle secondarie a carcinoma mammario e polmonare ipodense , quelle da leiomiosarcoma francamente disomogenee . 
nei restanti 5 pazienti , tutti affetti da metastasi singole da carcinoma renale , una precisa diagnosi risultata impossibile , poich le lesioni non erano differenziabili da un tumore neuroendocrino . 
 keywords multidetector computed tomography pancreatic metastases pancreas parole chiave tomografia computerizzata multidetettore metastasi pancreatiche pancreas 370 introduction pancreatic metastases account for approximately 25% of malignancies affecting this organ [ 13 ]  . 
tumours that most frequently metastasise to the pancreas are renal cell carcinomas ( rcc ) , carcinomas of the lung and breast , colorectal cancers , melanomas and some types of sarcoma ( leiomyosarcomas , myxoid liposarcoma ) [ 5 ]  . 
clinical manifestations include jaundice , abdominal pain , weight loss , gastrointestinal bleeding or signs of pancreatic insufficiency [ 8 ]  . diagnostic imaging is essential for their detection and relies on ultrasound ( us ) , magnetic resonance ( mr ) imaging and particularly computed tomography ( ct )  . 
 although us is the first - line imaging study used in the event of suspected pancreatic disease , few data are reported in the literature concerning its use in the study of secondary pancreatic involvement [ 913 ]  . 
ct is the most frequently used method for studying pancreatic cancer [ 19 ] , and a limited number of studies have also reported its use in studying metastases [ 36 , 8 ]  . the purpose of this study was to investigate the diagnostic potential of ct for characterising pancreatic metastases and to assess the clinical and radiological course of the disease over time . materials and methods ct scans of 17 patients ( 11 men and six women ; age range 5274 years ; mean age 63.8 years ) with pancreatic metastases studied from 2004 to 2010 were retrospectively reviewed . 
the final diagnosis was histologically confirmed in ten patients ( eight cases of rcc metastasis and two of metastasis from leiomyosarcoma ) ; in the other cases , histological confirmation was obtained for the primary tumour , whereas the secondary pancreatic lesions were characterised on the basis of the ct images and clinical disease course . 
 after identification of the condition , all patients underwent biannual ct follow - up examinations ; these were interrupted in the event of patient death , whereas they are radiol med ( 2012 ) 117 : 369377 introduzione le metastasi pancreatiche rappresentano circa il 2%5% dei tumori maligni a carico di tale organo [ 13 ]  . 
studi autoptici , condotti su ampie casistiche di soggetti deceduti per malattia neoplastica avanzata , ne riportano tuttavia una prevalenza variabile dall1 , 6% al 37 , 5% [ 24 ]  . 
le neoplasie che pi frequentemente metastatizzano al pancreas sono i carcinomi del rene , del polmone , della mammella , del colon - retto , i melanomi ed alcuni tipi di sarcoma ( leiomiosarcomi , liposarcoma mixoide ) [ 5 ]  . 
 la diagnostica per immagini fondamentale per la loro identificazione e si basa su ecografia , risonanza magnetica ( rm ) e , soprattutto , tomografia computerizzata ( tc )  . 
 lecografia generalmente la prima indagine utilizzata nel sospetto di una patologia pancreatica , tuttavia , in letteratura sono riportati pochi dati riguardanti il suo impiego nello studio delle localizzazioni secondarie intraghiandolari [ 9 13 ]  . 
la tc attualmente la metodica maggiormente adoperata nello studio dei tumori del pancreas [ 19 ] ed il suo impiego nello studio delle metastasi stato riportato in letteratura , anche se le esperienze sono ancora poco numerose [ 36 , 8 ]  . scopo del presente lavoro considerare le potenzialit diagnostiche della tc nella caratterizzazione delle metastasi pancreatiche e valutare levoluzione clinica e radiologica della patologia nel tempo . materiali e metodi sono stati esaminati retrospettivamente gli esami tc di 17 pazienti ( 11 uomini e 6 donne ) , di et compresa tra 52 e 74 anni ( et media : 63 , 8 anni ) , affetti da metastasi pancreatiche , studiati nel periodo compreso tra il 2004 e il 2010 . 
le metastasi erano secondarie a carcinoma renale in 8 casi , a leiomiosarcoma uterino in 2 casi , a carcinoma polmonare in 4 casi e a carcinoma mammario in 3 casi . 
 la diagnosi definitiva stata controllata istologicamente in 10 pazienti ( 8 casi di metastasi da carcinoma renale , 2 casi di metastasi da leiomiosarcoma ) , negli altri il tumore primitivo stato controllato istologicamente , mentre la caratterizzazione delle lesioni pancreatiche secondarie si basata sulle immagini tc e sullevoluzione clinica della radiol med ( 2012 ) 117 : 369377 still under way for surviving patients . 
images were acquired during the venous phase alone ( 5060 s after initiation of contrast administration ) in studies performed for tumour staging or follow - up , and with the biphasic technique ( arterial phase at 2530 s and venous phase at 5060 s after contrast administration ) in the remaining cases . 
 the images were assessed for the following : lesion number , size and location ( pancreatic head , body , lesion appearance ( nodular or infiltrative ) ; lesion enhancement ( hyperattenuating , hypoattenuating , inhomogeneous , presence of areas of intralesional colliquation ) ; presence of metastases to other organs ; time to development after diagnosis of the primary tail ) ; tumour ; clinical ( survival or death ) and radiological course ( morphological , volumetric and numerical changes in lesions ) as assessed at biannual ct follow - up examinations . results patient characteristics , time to development of metastases and abnormalities detected at ct are reported in table 1 . 
pancreatic lesions were solitary in seven cases ( 41% ) of which five were secondary to rcc and two to uterine leiomyosarcoma and multiple in ten ( 59% )  . 
 dopo avere riconosciuto la patologia tutti i pazienti sono stati sottoposti a controlli tc a cadenza semestrale ; tali controlli sono stati interrotti per alcuni pazienti deceduti e per i pazienti viventi sono ancora in corso . 
 gli esami tc sono stati eseguiti con apparecchiature tcmd a 4 strati ( mx 8000 , philips medical system , royal philips electronic , best , olanda ) e tcmd a 320 strati ( aquilion one , toshiba medical systems , tokyo , giappone ) , utilizzando , rispettivamente , i seguenti parametri di acquisizione : spessore di strato 2 , 5 e 1 mm ; pitch 1 , 25 e 0 , 8 . 
in tutti i casi sono state eseguite scansioni prima e dopo iniezione endovenosa di mezzo di contrasto ( io meron 400 bracco , milano , italia ) iniettato in quantit pari ad 1 , 5 ml pro - kg di peso corporeo , alla velocit di 3 , 5 ml al secondo . 
lacquisizione delle immagini avvenuta soltanto in fase venosa ( 5060 secondi dopo linizio della somministrazione del contrasto ) nei pazienti studiati per stadiazione o in corso di follow - up oncologico e con tecnica bifasica ( fase arteriosa 2530 s ; fase venosa 5060 s dopo la somministrazione del contrasto ) in tutti gli altri casi . 
 nel valutare le alterazioni patologiche sono stati considerati : numero , dimensioni e sede ( testa , corpo , coda ) ; aspetto ( nodulare o infiltrativo ) ; enhancement ( iperdenso , ipodenso , disomogeneo , eventuale presenza di aree di colliquazione intralesionali ) ; presenza di localizzazioni secondarie in altri organi ; tempo di comparsa rispetto al tumore primitivo ; evoluzione clinica ( sopravvivenza o decesso ) e radiologica ( variazioni morfologiche , volumetriche e numeriche delle lesioni ) della patologia valutata con controlli tc a cadenza semestrale . risultati i dati dei soggetti esaminati , il tempo di comparsa delle lesioni e le alterazioni riscontrate allesame tc sono indicati nella tabella 1 . 
in the eight patients with metastases from rcc , secondary lesions were present at the pancreatic level only ; in all of the remaining nine patients , the metastases also affected other organs as well . with regard to clinical course , among the eight patients with rcc , one died of complications following pancreatectomy and seven were still alive at the time of writing , of whom four underwent surgery and three chemotherapy . 
for these patients , survival time since the diagnosis ranged from 12 to 48 months ; at the last ct follow - up examination , none of the patients who underwent surgery showed recurrence , and the patients who underwent chemotherapy had persistin 7 casi ( 41% ) , in rapporto a carcinoma renale ( 5 casi ) e a leiomiosarcoma uterino ( 2 casi ) , e multiple in 10 casi ( 59% ) e le loro dimensioni variavano tra 8 mm e 40 mm ( media : 23 mm )  . 
of the remaining eight patients , all with metastatic involvement of several organs at diagnosis , six died within 18 months from the diagnosis and two ( metastasis from uterine leiomyosarcoma , treated with chemotherapy ) were alive at follow - up ct performed 2 years and 1 year after the diagnosis , respectively . discussion pancreatic metastases are rarely detected in vivo , most probably because they do not always cause significant clinical and laboratory findings . 
the incidence , however , is underestimated , as the prevalence rates at autopsy have been reported to range from 1.6% to 37% , depending on vamente a livello pancreatico , nei restanti 9 pazienti esistevano sempre localizzazioni secondarie anche in altri organi . 
 dal punto di vista dellevoluzione clinica della patologia , degli 8 pazienti affetti da carcinoma renale , 1 deceduto per complicanze in seguito ad intervento di pancreasectomia , 7 sopravvivono e sono stati sottoposti 4 a trattamento chirurgico e 3 a chemioterapia . 
per tali pazienti il tempo di sopravvivenza trascorso dalla diagnosi compreso tra 12 e 48 mesi ed agli ultimi controlli tc i pazienti trattati chirurgicamente risultano esenti da ripresa di malattia ; i pazienti trattati con chemioterapia mostrano una persistenza delle lesioni che comunque appaiono prive di una evidente progressione volumetrica . 
dei restanti 8 pazienti , affetti al momento della diagnosi da localizzazioni metastatiche in vari organi , 6 sono deceduti entro 18 mesi dalla diagnosi , radiol med ( 2012 ) 117 : 369377 2 ( metastasi da leiomiosarcoma dellutero ) sopravvivono dopo chemioterapia rispettivamente ai controlli effettuati a 2 e 1 anno dalla diagnosi . discussione il riscontro di metastasi pancreatiche in vivo abbastanza raro , probabilmente poich non sempre determinano una significativit clinica e laboratoristica ; la loro incidenza , tuttavia , sottostimata , infatti al controllo autoptico , come gi riportato , la prevalenza compresa tra l1 , 6% ed il 37% , a seconda che vengano esaminate casistiche oncologiche aspecifiche o casistiche selettive di soggetti deceduti per neoplasie altamente metastatizzanti [ 24 ]  . 
 come gi sottolineato la diagnostica per immagini delle metastasi pancreatiche si basa su ecografia , tc ed rm , anche se la tc , essendo lindagine pi utilizzata nei pazienti oncologici , quella che pi spesso riconosce la patologia . 
 da un punto di vista morfologico , nei nostri risultati compaiono soltanto lesioni nodulari , mentre mancano le forme infiltrative riportate in altre casistiche nel 4 , 5%35% dei casi [ 4 , 6 ]  . 
per quanto riguarda lenhancement delle lesioni , i risultati ottenuti confermano i dati gi presenti in letteratura ; le lesioni pancreatiche hanno presentato una morfologia variabile , francamente ipodense in rapporto a carcinomi polmonari e mammari , disomogenee con ampie aree di colliquazione in rapporto a leiomiosarcomi , francamente iperdense in fase arteriosa in rapporto a carcinomi renali [ 38 , 2022 ]  . 
 nonostante la variabilit dei reperti tc , nella nostra esperienza una precisa diagnosi sempre stata possibile nelle forme multifocali , anche per la contemporanea presenza di localizzazioni secondarie in altri organi , circostanza verificatasi nelle metastasi da carcinoma polmonare , mammario e leiomiosarcoma . 
 [ 3 ] la percentuale di metastasi sincrone era pari , rispettivamente , al 44% , 39% e 40% dei casi , e la percentuale di metastasi metacrone era pari al 56% , 61% e 60% . 
 as previously stated , diagnostic imaging in pancreatic metastases relies on us , ct and mr imaging , even though the disease is most often recognised on ct , the modality that is most widely used in cancer patients . 
in terms of lesion morphology , we identified only nodular lesions , with no instances of infiltrative lesion reported in 4.535% of cases in other series [ 4 , 6 ]  . 
with regard to lesion enhancement , our results confirm the literature data ; pancreatic lesions showed a variable pattern , being frankly hypoattenuating when they were secondary to lung and breast carcinomas , inhomogeneous with large areas of colliquation when secondary to leiomyosarcomas and markedly hyperattenuating in the arterial phase when secondary to rcc [ 38 , 2022 ]  . 
 despite the variability in ct findings , we found it was always possible to reach a precise diagnosis in the multifocal forms , in part thanks to the simultaneous involvement of other organs , a circumstance that occurred in metastases from lung and breast carcinoma and from leiomyosarcoma . 
 esse appaiono iperdense in fase arteriosa ( a , b ) e lenhancement si riduce in fase portale ( c , d )  . the rate of synchronous metastases was , respectively , 44% , 39% and 40% and of metachronous metastases 56% , 61% and 60% [ 3 , 4 , 6 ]  . 
this finding is also confirmed by other studies , which report the appearance of pancreatic metastases after nephrectomy , with time intervals > 5 years in 70% of cases [ 24 ] and > 10 years in 11% of cases [ 25 ]  . 
the delayed appearance of pancreatic metastases from rcc seems to be ascribable , as maintained by sellner et al . , to the high affinity of tumour cells for the pancreatic parenchyma , where they apparently find a microenvironment suitable for their growth [ 26 , 27 ]  . 
in fact , all patients who underwent surgery or chemotherapy are still alive , with the exception of one patient who died of postoperative complications . compreso tra 10 e 30 anni . 
tale riscontro trova conferma in altre esperienze , che riportano la comparsa di metastasi pancreatiche dopo nefrectomia con un intervallo di tempo rispettivamente superiore a 5 anni nel 70% dei casi [ 24 ] e superiore a 10 anni nell11% dei casi [ 25 ]  . 
these hypervascular , well - circumscribed masses usually have innocuous clinical manifestations as slowly enlarging soft - tissue lesions ; however , more rarely , they can cause cranialnerve palsy , particularly lesions arising near the skull base , or symptoms related to their secreting activity . 
 most paragangliomas are benign and their prognosis is directly related to the location of the tumour : those arising at the carotid body have the best outcome , whereas those located at the skull base have a less favourable prognosis . 
queste lesioni , ipervascolarizzate e ben delimitate , si manifestano solitamente in maniera innocua come masse dei tessuti molli a lenta crescita mentre pi raramente causano paralisi dei nervi cranici , in particolare per le lesioni che si sviluppano a livello della base cranica , o sintomi relativi alla loro attivit secernente . 
i paragangliomi sono per la maggior parte benigni e la loro prognosi direttamente correlata alla posizione del tumore : quelli che si sviluppano alla biforcazione carotidea hanno esito migliore , mentre quelli situati a livello della base cranica hanno una prognosi meno favorevole . 
epidemiological studies have shown that one of the genetically determined forms of the disease has a particularly high incidence in some valleys of the trentino region in italy [ 2 , 3 ]  . 
based on a large case series ( 77 patients ) , this paper aims to provide epidemiological and genetic background information and illustrate , through an extensive pictorial essay , the main morphological [ computed tomography ( ct ) and magnetic resonance imaging ( mri ) ] , vascular ( angiography ) and functional ( nuclear medicine ) features of paragangliomas . 
it does not take into consideration the diagnostic role of ultrasonography ( us ) , a level - one investigation limited to detecting carotid and vagal paragangliomas in the presence of lateral cervical swelling : if , on the one hand , us can help identify a suspected paraganglioma on the basis of location , relationship with neighbouring vascular structures and high vascularity at colour doppler imaging on the other , it cannot provide accurate anatomical and topographic information , which the surgeon or nuclear medicine physician needs for resection or radiometabolic treatment , respectively [ 4 , 5 ]  . genetics and pathology radiol med ( 2012 ) 117 : 471487 introduzione i paragangliomi , sporadici o familiari , sono rare neoplasie di natura neuroendocrina e rappresentano il 0 , 03% di tutti i tumori [ 1 ]  . 
la numerosa casistica ( 77 pazienti ) ha reso possibile la realizzazione di questo lavoro che , attraverso unampia rassegna iconografica , oltre a fornire nozioni di ordine epidemiologico e genetico si propone di illustrare le principali caratteristiche morfologiche alla tomografia computerizzata ( tc ) e alla risonanza magnetica ( rm ) , vascolari ( angiografiche ) e funzionali ( medicina nucleare ) dei paragangliomi . 
non verr invece preso in considerazione il ruolo diagnostico dellecografia , peraltro limitato ai soli paragangliomi carotidei e vagali come indagine di i livello in presenza di una tumefazione laterocervicale : se da un lato lecografia in grado di identificare agevolmente un sospetto paraganglioma , anche in base alla sede , ai rapporti con le strutture vascolari limitrofe e alla presenza dellelevata vascolarizzazione rilevabile al color doppler , dallaltro tale metodica non pu fornire le accurate ed indispensabili informazioni anatomo - topografiche , necessarie al chirurgo o al medico nucleare , rispettivamente per lintervento di rimozione o la terapia radiometabolica [ 4 , 5 ]  . forms the extra - adrenal neuroendocrine system , which together with the sympathetic nervous system and the adrenal medulla the sympathoadrenal neuroendocrine system , is made up of groups of specialised cells that possess unique regulatory functions [ 6 ]  . 
of neuroectodermal origin , paraganglia are classified into four categories on the basis of their anatomical location ( table 1 ) : branchiomeric , vagal , aortosympathetic and visceral [ 1 ]  . 
paraganglia of the first two categories are related to the parasympathetic nervous system ( nonchromaffin ) , have a chemoreceptorlike function and are typically nonsecreting ; those in the other two categories are functionally related to the orthosympathetic system ( chromaffin ) , have a function similar to that of the adrenal medulla and typically secrete catecholamines [ 7 ]  . 
 historically referred to by the names of glomus tumour , chemodectoma , glomangioma , sympathoblastoma , endothelioma and / or fibroangioma , tumours arising from paraganglia are named paraganglioma preceded by the anatomical location [ 8 ]  . 
the former genetica e anatomia patologica il sistema neuroendocrino extra - surrenalico , che insieme al sistema nervoso ortosimpatico e alla midollare del surrene costituisce il sistema simpatico - adrenale , composto da gruppi di cellule specializzate che hanno specifiche funzioni regolatorie [ 6 ]  . 
in rapporto alla loro distribuzione in tutto il corpo , in stretta adiacenza ai gangli nervosi , questi agglomerati cellulari sono definiti paragangli , termine coniato da kohn nel 1903 . 
embriologicamente di origine neuroectodermica , sono classificati in base alla sede anatomica in quattro categorie ( tabella 1 ) : i paragangli branchiomerici , i vagali , gli aorto - simpatici e infine , quelli localizzati in sede viscerale [ 1 ]  . 
i paragangli appartenenti alle prime due categorie sono legati al sistema nervoso parasimpatico ( non - cromaffini ) , hanno una funzione simil - chemorecettoriale e sono tipicamente non secernenti ; quelli appartenenti alle altre due categorie sono funzionalmente legati al sistema ortosimpatico ( cromaffini ) , hanno una funzione simile alla midollare del surrene e caratteristicamente secernono catecolamine [ 7 ]  . 
 storicamente indicate con i termini di tumore glomico , chemodectoma , glomangioma , simpaticoblastoma , endotelioma e / o fibroangioma , attualmente , per indicare le neoplasie che originano dai paragangli si utilizza il termine radiol med ( 2012 ) 117 : 471487 table 1 glenner classification of extra - adrenal paragangliomas ( modified from [ 1 ] ) group description associated with the great vessels of the chest and neck and with the cranial nerves ( branchiomeric origin ) : aortopulmonary , pulmonary , coronary , carotid body , subclavian , jugulotympanic , laryngeal associated with the vagal nerve associated with the aorticosympathetic chain of the thoracolumbar region , from the superior cervical ganglion to the pelvis , including the organ of zuckerkandl associated with the visceral organs : interatrial septum , liver hilum , renal hilum , bladder walls , gallbladder , duodenum tabella 1 classificazione di glenner . 
modificata da [ 1 ] categoria descrizione associati ai grandi vasi del torace e del collo e ai nervi cranici ( origine branchiomerica ) : aorto - polmonari , polmonari , coronarici , carotidei , succlavi , giugulo - timpanici , laringei associati al nervo vago associati ai gangli delle catene aorto - simpatiche della regione toraco - lombare , dal ganglio cervicale superiore alla pelvi , incluso lorgano di zuckerkandl associati agli organi viscerali ( setto interatriale , ilo epatico , ilo renale , pareti della vescica , della colecisti e del duodeno ) have polygonal morphology and neurosecretory granules , are more abundant , form fairly densely packed cell clusters ( cell nests , or zellballen ) and are encircled by the spindleshaped sustentacular cells with their long cytoplasmic processes [ 1 ]  . 
although the majority of paragangliomas are isolated and develop sporadically , approximately 10% are hereditary and can develop in patients affected by syndromes predisposing them to multiple neoplasms , such as multiple endocrine neoplasia type 2 ( men 2 ) , type 1 neurofibromatosis , von hippel lindau disease , carneys triad ( gastric leiomyosarcomas , pulmonary chondromas , paragangliomas ) or may be inherited as a pure familial pattern ( familial paragangliomas ) with no association with other tumours . 
approximately 3550% of familial cases present with multifocal lesions [ 9 ]  . paraganglioma syndrome ( pgl ) is a rare hereditary disease ( incidence 1 / 300 , 000 year ) and is due to mutations inactivating the sdhb , sdhc and / or sdhd genes encoding for subunits of the succinate - dehydrogenase enzyme ( mitochondrial enzyme complex ii ) , which plays a key role in the electron transport chain of the krebs cycle . 
the loss of succinate - dehydrogenase activity results in a build up of succinate , which activates the vascular endothelial growth factor and , by increasing oxidative stress , promotes tumour growth and abundant vascularisation [ 10 ]  . 
pgl 1 , the most frequent , is associated with mutations of the sdhd gene ( chromosome 11q23 ) and is transmitted as an autosomal dominant trait ( variable expressivity and 92% penetrance ) with maternal imprinting : that is , the mutated protein is paraganglioma seguito dalla sede anatomica [ 8 ]  . 
le prime , dalla morfologia poligonale e con granuli neurosecretori , sono pi numerose e formano aggregati cellulari ( nidi o zellballen ) piuttosto compatti , alla cui periferia si distribuiscono le seconde , fusiformi e dai lunghi processi citoplasmatici [ 1 ]  . 
bench la maggior parte dei paragangliomi siano singoli e insorgano sporadicamente , in circa il 10% dei casi sono ereditari e possono svilupparsi in pazienti con sindromi predisponenti a neoplasie multiple quali le neoplasie endocrine multiple ( men 2 ) , la neurofibromatosi di tipo 1 , la malattia di von hippel lindau , la triade di carney ( leiomiosarcomi gastrici , condromi polmonari , paragangliomi ) oppure possono essere ereditati come pattern familiare puro ( paragangliomi familiari ) privi di associazione con altre neoplasie . 
circa il 35%50% dei casi familiari presenta inoltre una multifocalit delle lesioni [ 9 ]  . la sindrome paraganglioma ( pgl ) una malattia ereditaria rara ( incidenza 1 / 300000 anno ) , dovuta a mutazioni inattivanti i geni sdhb , sdhc e / o sdhd , codificanti subunit dellenzima mitocondriale succinato - deidrogenasi ( complesso mitocondriale ii ) , che gioca un ruolo chiave nella catena di trasporto degli elettroni del ciclo di krebs . 
 la perdita dellattivit della succinato - deidrogenasi determina laccumulo di succinato che attiva il fattore di crescita dellendotelio vascolare e , aumentando lo stress ossidativo , promuove la crescita tumorale e la ricca vascolarizzazione 474 radiol med ( 2012 ) 117 : 471487 produced from the paternal allele only , with selective silencing of the maternal allele [ 11 , 12 ]  . 
 some 40 years ago , several cases of familial paraganglioma were reported in specific areas of the trentino region ( val dei mocheni , altopiano di pin , val di cembra ) , with descriptions of the difficulties encountered in surgical treatment ; in the 1980s , there was talk of an epidemic [ 13 ] , whereas the sdhd mutation was first identified in 2001 . 
 however , all mutation carriers had the same haplotype , which suggested that they descended from a common ancestor and that the mutation probably appeared in this area in 1400 ( trentino founder effect ) [ 2 , 3 ]  . 
from the initial ten index cases , the investigation has extended to 75 families , for a total of 448 individuals , 233 of whom are carriers of the mutation : of these , 33% are affected by paragangliomas , with multiple locations in more than 60% of thein addition , an epidemiological study is underway to evaluate the true frequency of the mutation , with results so far indicating 59 carriers of 4 , 020 healthy volunteers from these geographical areas . 
 pgl 1 may manifest with nonchromaffin tumours of the head and neck or with adrenal or extra - adrenal pheochromocytoma or with a combination of the two types of tumour ; lesions are generally benign and often multiple . 
 onset peaks between the ages of 20 and 40 years , with high incidence rates also in the sixth and seventh decades ; malignancy is rare ( < 10% ) and related to the presence of nodal , lung and skin metastasis . 
the distinction is based lesion location in that metastases occur at sites devoid of paraganglia tissue , whereas the primary tumour always arises from tissues containing paraganglia [ 14 ]  . paragangliomas of the head and neck head and neck paragangliomas are functionally related to the parasympathetic nervous system ( categories 1 and 2 ; table 1 )  . 
la pgl 1 , in assoluto la pi frequente , associata a mutazioni del gene sdhd ( cromosoma 11q23 ) , viene trasmessa come tratto autosomico dominante ( espressivit variabile e penetranza del 92% ) ed sottoposta ad imprinting materno , cio la proteina mutata viene prodotta solo a partire dallallele paterno con inibizione selettiva dellespressione dellallele materno [ 11 , 12 ]  . 
 quarantanni fa in alcune aree geografiche del trentino ( val dei mocheni , altopiano di pin , val di cembra ) furono segnalati alcuni casi di paragangliomi familiari e descritte le difficolt incontrate nel loro trattamento chirurgico ; negli anni 80 si parl di epidemia [ 13 ] mentre nel 2001 venne identificata per la prima volta la mutazione sdhd . 
supponendo che queste famiglie avessero un antenato comune , furono ricostruiti gli alberi genealogici fino al 1700 , senza tuttavia identificare ascendenti comuni ; peraltro , tutti i carrier di mutazione presentavano lo stesso aplotipo il che sugger la loro origine da un precursore ancestrale comune e che la mutazione fosse probabilmente comparsa in questa area nel 1400 ( effetto fondatore trentino ) [ 2 , 3 ]  . 
dai 10 casi indice iniziali si giunti alla quota attuale di 75 famiglie studiate , per un totale di 448 individui , di cui 233 sono risultati portatori della suddetta mutazione : di questi il 33% risulta affetto da paragangliomi , in pi del 60% con localizzazioni multiple . 
 inoltre in corso di realizzazione uno studio epidemiologico mirato a valutare la reale frequenza della mutazione , con identificazione , fino ad ora , di 59 portatori su 4020 soggetti ( volontari sani ) originari di queste aree geografiche . 
 la pgl 1 si pu manifestare con tumori non - cromaffini della testa e del collo oppure con feocromocitoma surrenalico o extra - surrenalico o con una combinazione dei due tipi di tumore ; si tratta generalmente di lesioni benigne e spesso multiple . 
let di insorgenza ha un picco tra i 2040 anni , con incidenze elevate anche nella vivii decade ; la malignit , rara ( < 10% ) , legata alla presenza di metastasi in sede linfonodale , polmonare e cutanea . 
the growth pattern is expansile rather than invasive , with the tumour tending to completely surround the carotid arteries without , however , narrowing their lumen ( vascular encasement )  . 
often asymptomatic , these tumours may manifest clinically either as lateral cervical pulsatile masses or with dysphagia , anisocoria , dysphonia and deafness due to compression and / or displacement of neighbouring nerve te legati al sistema nervoso parasimpatico ( categorie 1 e 2 ) ( tabella 1 )  . 
unilateral paraganglioma ( c , d ) : contrast - enhanced axial ct image ( c ) and volume - rendering image ( d ) demonstrate an intensely enhancing right carotid - space lesion that displaces the external carotid from the internal ( arrows ) ; compare with normal left side ( asterisk )  . 
nellimmagine assiale tc ( c ) e nel volume rendering ( d ) lesione ipervascolarizzata , che determina un ampliamento dello spazio tra le due carotidi di destra ( frecce ) ; a sinistra normale distanza tra i due vasi ( asterisco )  . 
allindagine spect whole body ( 111in - octreotide , radiofarmaco recettoriale ) si apprezzano due aree di intensa , disomogenea captazione in sede laterocervicale bilateralmente , corrispondenti a paragangliomi carotidei . 
the pathognomonic finding , though not frequent , is the salt - and - pepper pattern , where the salt represents the hyperintense areas due to haemorrhage or slow flow , and the pepper represents the punctate or serpentine hypointense foci , which reflect high flow in the intratumoural vessels and correspond to areas of flow void . 
rarely used , angiography provides evaluation of vascularity ( arterial inflow and venous outflow ) and the circle of willis and allows identification of synchronous lesions missed on ct and mri . 
angiography typically shows enlarged feeding arteries usually branches from the ascending pharyngeal artery and less commonly from the superior thyroid artery and / or maxillary artery as well as intense and protracted blushing of the lesion and early venous drainage . 
the role of preoperative selective embolisation is controversial : it is considered only for lesions > 3 cm and performed approximately 48 h prior to surgery [ 16 ]  . 
functional imaging cannot be divorced from preliminary humoral evaluation targeted to the type of paraganglioma ( orthosympathetic , frequently secreting catecholamines ; parasympathetic , nonsecreting ) , which will influence the type of radiopharmaceutical to be used [ 8 ]  . 
in the case of paragangliomas not secreting catecholamines , there is an indication for the use of 111in - octreotide [ 17 ] hybrid single photon emission ct and ct ( spect / ct ) and / or positron - emitting tracers such as 68ga - dotatoc with hybrid positron emission tomography and ct ( pet / ct ) [ 18 ]  . 
in those rare cases in which head and neck paragangliomas ( 12% ) [ 21 ] are associated with increased catecholamines , there is an indication for scintigraphy with 123i - mibg ( metaiodobenzylguanidine ) , a structural guanethidine analogue similar to noradrenaline , with elective uptake by cells of neuroectodermal origin [ 22 ] , an essential requirement for radiometabolic treatment with 131i - mibg . 
la crescita neoplastica , di tipo espansivo piuttosto che infiltrativo , tende a circondare completamente il lume delle carotidi senza peraltro determinarne riduzione di calibro ( encasement vascolare )  . 
spesso asintomatici , clinicamente possono manifestarsi o come masse pulsatili laterocervicali o con disfagia , anisocoria , disfonia e sordit , legate alla compressione e / o dislocazione delle strutture nervose adiacenti . 
laspetto patognomonico , seppur non frequente , rappresentato dal pattern a sale e pepe : il sale rappresentato da aree iperintense , secondarie ad emorragia o a flusso lento , mentre il pepe da foci puntiformi o serpiginosi ipointensi , che rispecchiano lelevato flusso allinterno dei vasi intratumorali e che corrispondono ad aree di vuoto di segnale ( flow void )  . 
allindagine angiografica si ricorre raramente e in genere per la valutazione dellapporto vascolare ( inflow arterioso - outflow venoso ) , per la valutazione del poligono del willis e per lindividuazione di lesioni sincrone non rilevate da tc e rm . 
langiografia mostra tipicamente vasi arteriosi afferenti dilatati di solito rami provenienti dallarteria faringea ascendente e pi raramente dalle arterie tiroidea superiore e / o mascellare , unintensa e prolungata opacizzazione della lesione ( blushing ) e un precoce drenaggio venoso . 
il ruolo dellembolizzazione selettiva preoperatoria controverso : viene preso in considerazione solo per lesioni con dimensioni superiori a 3 cm , circa 48 ore prima dellintervento chirurgico [ 16 ]  . 
limaging funzionale non pu prescindere da una preliminare valutazione bioumorale , strettamente correlata al tipo di paraganglioma ( ortosimpatico , frequentemente secernente catecolamine ; parasimpatico , non secernente ) , che conseguentemente condiziona la scelta del tipo di radiofarmaco da utilizzare [ 8 ]  . 
qualora si tratti di paragangliomi non secernenti catecolamine , vi indicazione allutilizzo di 111in - octreotide [ 17 ] con metodica dacquisizione single - photon emission computed tomography ( spect - tc ) e / o di traccianti positroni emittenti quali il 68ga - dotatoc , con metodica tomografia ad emissione di positroni ( pet - tc ) [ 18 ]  . 
however , an increasing body of evidence suggests the use of 18f - dopa ( with pet / ct ) , especially in patients with signs of a catecholaminesecreting tumour but with negative 123i - mibg [ 22 ]  . 
the differential diagnosis of carotid - body paragangliomas includes hypervascular nodal metastases ( from renal or thyroid tumours ) , vagal schwannomas and neurofibromas , carotid aneurysms and vagal paragangliomas [ 1 ]  . jugulotympanic paragangliomas the paraganglia of the temporal bone are small ovoid bodies with lobulated margins and a diameter of 0.11.5 mthey are located along the tympanic branch of the glossopharyngeal nerve ( jacobsons nerve ) and auricular branch of the vagus nerve ( arnolds nerve )  . 
paragangliomas arising from jacobsons nerve ( tympanic ) may be found anywhere along the course of the nerve , including the facial canal and inferior tympanic canaliculus , although most of them arise in the mucosa of cochlear promontory . 
 because of the close proximity between the cochlear promontory and the jugular fossa , larger lesions tend to involve both regions , and it is often impossible to make a clear - cut anatomical distinction ; for this reason , they are referred to as jugulotympanic paragangliomas . 
 tympanic paragangliomas may cause pulsatile tinnitus ( 82% ) and hearing loss ( 52% ) , and otoscopy examination generally reveals a pulsating retrotympanic mass , with bluish tympanic membrane . 
jugular paragangliomas present with extremely diverse symptoms related to impaired adjacent nervous structures : vernet syndrome ( or jugular foramen syndrome ) caused by involvement of the cranial nerves ix ( glossopharyngeal ) , x ( vagus ) and xi ( accessory ) with resulting dysphagia , loss of sensation in the posterior pharyngeal wall , loss of taste on the posterior third of the tongue and deviation of the soft palate towards the healthy side ( ix ) ; hoarseness due to vocal cord paralysis ( x ) ; weakness and atrophy of the sternocleidomastoid and trapezius muscles ( xi )  . 
nei rari casi in cui al paraganglioma del capo - collo ( 1%2% ) [ 21 ] si associ un incremento delle catecolamine vi indicazione ad eseguire la scintigrafia con 123i - meta - benzil - guanidina ( mibg ) , un analogo strutturale della guanetidina simile alla noradrenalina , elettivamente captato dalle cellule dei tessuti di derivazione neuroectodermica [ 22 ] , fondamentale premessa ad eventuale terapia radiometabolica con 131i - mibg . 
vanno comunque segnalate le sempre maggiori evidenze in letteratura sullopportunit di impiegare la 18f - dopa ( con tecnica dacquisizione pet - tc ) , specie nei pazienti con evidenza di tumore secernente catecolamine ma con 123i - mibg negativa [ 22 ]  . 
la diagnosi differenziale dei paragangliomi carotidei include le metastasi linfonodali ipervascolarizzate ( da neoplasie renali o tiroidee ) , gli schwannomi e neurofibromi vagali , gli aneurismi carotidei nonch i paragangliomi vagali [ 1 ]  . paragangliomi giugulo - timpanici i paragangli dellosso temporale sono piccoli corpiccioli ovoidali a margini lobulati del diametro compreso tra 0 , 1 e 1 , 5 mm e si localizzano lungo il decorso della branca timpanica del nervo glossofaringeo ( nervo di jacobson ) e della branca auricolare del nervo vago ( nervo di arnold )  . 
 i paragangliomi che originano dal nervo di jacobson ( timpanici ) si possono riscontrare ovunque lungo il suo decorso , incluso il canale del facciale e il canalicolo timpanico inferiore , anche se pi frequentemente insorgono sulla mucosa del promontorio cocleare . 
a causa della stretta vicinanza tra il promontorio cocleare e la fossa giugulare , le lesioni di grandi dimensioni tendono a coinvolgere entrambe le regioni e spesso non possibile effettuare una netta distinzione anatomica ; pertanto , si parla di paragangliomi giugulo - timpanici . 
 i paragangliomi timpanici possono causare tinnito pulsatile ( 82% ) e ipoacusia ( 52% ) e allesame otoscopico si rileva generalmente una massa retro - timpanica pulsante , con membrana timpanica bluastra . 
axial high - resolution ct images ( a , b ) and coronal multiplanar reconstructions ( c , d ) show soft - tissue mass located at the right cochlear promontory ( a , b arrow )  . 
a - d le immagini assiali tc ad alta risoluzione ( a , b ) e le ricostruzioni mpr coronali ( c , d ) mostrano una neoformazione solida ipodensa che si dispone a ridosso del promontorio cocleare di destra ( a , b : freccia ) , inglobando la catena ossiculare senza determinarne erosione . 
they tend to grow in a predictable manner along pathways of least resistance : through the eustachian tube into the rhinopharynx ; through the aditus into the mastoid antrum ; through the tympanic membrane into the external auditory canal . 
bone invasion is rare : if the paraganglioma is small , it does not erode the ossicular chain ; the floor of the middle ear remains intact , as does the bone of the jugular spine and carotidjugular crest . 
a left paraganglioma causes jugular foramen enlargement ( a , b arrow ) and extends into the hypotympanum ( c , d ) near the eustachian tube ( c arrow ) and partially surrounds the malleus manubrium ( e )  . 
a sinistra paraganglioma che determina ampliamento del forame giugulare ( a , b : freccia ) e va ad occupare lipotimpano ( c , d ) , in adiacenza allimbocco tubarico ( c : freccia ) e circondando parzialmente anche il manico del martello ( e )  . 
si noti lintegrit delle strutture ossee cocleari . medial border of the foramen causing irregular enlargement ; anteriorly , they may invade the tympanic cavity ( through flow erosion ) and posteriorly penetrate the posterior cranial fossa . 
they therefore have a markedly destructive nature , causing lysis of the jugular spine and carotidjugular crest in the absence of osteosclerosis ( moth - eaten appearance of the jugular foramen ) and erosion of the ossicular chain with possible involvement extending to the mastoid segment of the facial nerve . 
administration of paramagnetic contrast material allows for better evaluation of the real extent of the tumour within the skull base and middle - ear cavity , as well as its possible intraluminal extent within the internal jugular veangiography shows enlarged feeding vessels ( ascending pharyngeal artery or possible branches from the anteriorinferior cerebellar artery and / or posterior inferior cerebellar artery ) , intense and protracted opacification of the mass and early venous drainage . 
tendono a crescere in maniera prevedibile sfruttando loci di minor resistenza : attraverso la tuba di eustachio nel rinofaringe , attraverso ladito nellantro mastoideo , attraverso la membrana timpanica nel condotto uditivo esterno . 
linvasione ossea rara : se sono di piccole dimensioni non erodono la catena ossiculare ; il pavimento dellorecchio medio intatto cos come viene mantenuta lintegrit ossea della spina giugulare e della cresta carotico - giugulare . 
jugular paragangliomas should , instead , be essentially differentiated from schwannomas of cranial nerves ix , x , xi , which arise from the medial portion or pars nervosa of the jugular foramen , whereas paragangliomas tend to arise from the lateral portion or pars vascularis . 
larger lesions may extend cranially into the posterior cranial fossa through the jugular foramen , whereas inferiorly they may reach the carotid bifurcation without widening it , as happens with carotid - body paragangliomas . 
 they clinically manifest as nontender masses behind the mandible angle or with symptoms related to impairment of adjacent nerve structures , such as hoarseness or dysphagia due to vocal cord paralysis following infiltration of cranial nerve x , horners syndrome ( miosis , enophthalmos , ptosis of the eyelids ) due to infiltration into the cervical sympathetic chain , and vernets syndrome ( as occurs in jugular paragangliomas ) in paragangliomas originating from the superior ganglion [ 23 ]  . 
differential diagnosis si presentano come formazioni che originano dalla porzione laterale del forame giugulare con tipica crescita supero - laterale ; tuttavia , possono svilupparsi in ogni direzione ed estendersi sino al confine mediale del forame determinandone irregolare ampliamento ; anteriormente posso no invadere la cavit timpanica ( per erosione del pavimento ) e posteriormente penetrare nella fossa cranica posteriore . 
presentano quindi un carattere marcatamente destruente , determinando lisi della spina giugulare e della cresta carotico - giugulare in assenza di osteosclerosi ( aspetto tarlato del forame giugulare ) ed erosione della catena ossiculare con possibile interessamento anche del segmento mastoideo del nervo faciale . 
langiogra fia mostra vasi afferenti dilatati ( arteria faringea ascendente o possibili rami dallarteria cerebellare anteriore inferiore , aica , e / o dallarteria cerebellare posteriore inferiore , pica ) , intensa e prolungata opacizzazione della massa e drenaggio venoso precoce . 
per limaging funzionale valgono le considerazioni gi espresse nel paragrafo relativo ai paragangliomi carotidei ( 111in - octreotide e / o 123i - mibg ) , risultando tuttavia fondamentale eseguire lacquisizione dellindagine esclusivamente tramite apparecchiature spect - tc con limpiego di dispositivi dimmobilizzazione del capo - collo per aumentare laccuratezza nella localizzazione anatomica ed evitare artefatti da movimento [ 25 ]  . la diagnosi differenziale dei paragangliomi timpanici include : neoplasie ipervascolarizzate dellosso tempora le , presenza di unarteria carotide interna aberrante che entra allinterno della cavit timpanica attraverso un canalicolo timpanico inferiore dilatato , persistenza dellarteria stapedia e , infine , colesteatomi dellorecchio medio , che di solito sono altamente erosivi . 
i paraganglio mi giugulari vanno invece differenziati essenzialmente dagli schwannomi dei ix , x , xi nervi cranici , che per originano dalla porzione mediale o pars nervosa del fora me giugulare mentre i paragangliomi da quella laterale o pars vascularis . 
la diagnosi differenziale include anche le malformazioni artero - venose della dura madre , il tumore osseo a cellule giganti , i meningiomi del forame giugulare e , infine , la deiscenza del bulbo della giugulare [ 23 , 24 ]  . radiol med ( 2012 ) 117 : 471487 fig . 
 lindagine angiografica ( g - l ) conferma lipervascolarizzazione ( g , l : freccia ) e la normalit dello spazio intercarotideo ( g - l : asterisco )  . 
quando raggiungono dimensioni considerevoli possono estendersi cranialmente nella fossa cranica posteriore attraverso il forame giugulare mentre inferiormente possono spingersi fino alla biforcazione carotidea , senza ampliarla come avviene per i carotidei . 
clinicamente si manifestano come masse non dolenti , palpabili dietro langolo della mandibola o con sintomi correlati alla compromissione di strutture nervose adiacenti , quali raucedine o disfagia per paralisi delle corde vocali da infiltrazione del x nervo cranico , sindrome di horner ( miosi , enoftalmo , ptosi palpebrale ) da infiltrazione del plesso simpatico cervicale e sindrome di vernet ( in analogia con i paragangliomi giugulari ) per i paragangliomi che originano dal ganglio superiore [ 23 ]  . 
la diagnosi differenziale comprende gli schwannomi vagali , le metastasi linfonodali ipervascolarizzate ( neoplasie renali o tiroidee ) , i paragangliomi carotidei e quelli ad origine dal basicranio ( giugulari ) e , infine , i meningiomi dello spazio carotideo . altre localizzazioni paragangliomi del torace i paragangliomi toracici ( 1%2% ) si localizzano prevalentemente nel mediastino e si suddividono in due gruppi sulla base della sede anatomica e dellinnervazione : quelli localizzati nel compartimento medio - anteriore , associati al sistema nervoso parasimpatico ( coronarici , polmonari , succlavi e sovra - aortici ) , e quelli in sede posteriore , legati allortosimpatico e disposti lungo le catene paravertebrali [ 6 ]  . 
i primi sono piccoli corpi chemorecettoriali localizzati prevalentemente nella finestra aorto - polmonare e per que482 radiol med ( 2012 ) 117 : 471487 includes vagal schwannomas , hypervascular nodal metastases ( renal or thyroid neoplasms ) , paragangliomas of the carotid body and skull base ( jugular ) and , finally , carotidspace meningiomas . other locations paragangliomas of the chest paragangliomas of the chest ( 12% ) are mostly found in the mediastinum and are divided into two groups on the basis of anatomical location and innervation : those located in the mid - anterior compartment associated with the parasympathetic nervous system ( coronary , pulmonary , subclavian and supra - aortic paraganglia ) , and those located in the posterior compartment associated with the orthosympathetic system along the paravertebral chains [ 6 ]  . 
in some cases , especially if large , they cause symptoms due to compression of mediastinal structures ( chest pain , dyspnoea , persistent dry cough , hoarseness , dysphagia , haemoptysis and , more rarely , superior vena cava syndrome ) [ 26 ]  . 
 the latter ( orthosympathetic nervous system ) occur in younger adults ( mean age 30 years ) , and approximately half of patients present with symptoms related to the secreting activity of the tumour ( tachycardia , hypertension ) [ 15 ]  . 
 irrespective of their location , imaging features of intrathoracic paragangliomas are identical : on ct , they appear as solid expansile masses with sharp and well - defined borders and intense enhancing after contrast medium infusion . 
on mri , they generally show homogeneous intermediate signal intensity similar to that of liver in t1 sequences ; on t2 images , signal intensity increases but to levels lower than those of subcutaneous fat . 
i secondi ( sistema nervoso ortosimpatico ) insorgono in soggetti pi giovani ( et media 30 anni ) e in circa la met dei pazienti si manifestano con sintomi correlati allattivit secernente della neoplasia ( tachicardia , ipertensione ) [ 15 ]  . 
 indipendentemente dalla sede , laspetto dei paragangliomi intratoracici identico : allindagine tc appaiono come formazioni espansive solide a margini netti e ben definiti , caratterizzate da intensa impregnazione dopo somministrazione di mdc . 
allindagine rm , nelle sequenze t1 mostrano unintensit di segnale intermedia , simile a quella del parenchima epatico , generalmente omogenea ; nelle sequenze t2 si assiste ad un aumento del segnale ma comunque sempre inferiore rispetto a quello del tessuto adiposo sottocutaneo . 
 grazie alla crescente diffusione delle apparecchiature tc multidetettore , in grado di fornire mappe vascolari di ottima qualit , per la valutazione della vascolarizzazione arteriosa e del rapido drenaggio venoso si ricorre sempre pi raramente , allindagine angiografica . 
contrast - enhanced ct images in the three spatial planes ( bd ) reveal that this shift is caused by a large middle mediastinum paraganglioma , which appear heterogeneous with central areas of poor enhancement , suggesting necrosis . 
le immagini tc post - mdc nei tre piani spaziali ( b - d ) dimostrano come tale spostamento sia determinato dalla presenza di un voluminoso paraganglioma del mediastino medio , disomogeneamente iperdenso per la presenza di numerose lacune necrotiche centrali . 
nelle immagini spect whole boby ( e , ricostruzioni mip sul piano coronale in senso antero - posteriore ) la captazione dell111in - octreotide mostra la presenza di recettori per la somatostatina ( frecce )  . 
 for midanterior mediastinal paragangliomas and tumours of nervous origin and germ - cell tumours for posterior mediastinal paragangliomas . paragangliomas of the abdomen and pelvis retroperitoneal paragangliomas extra - adrenal abdominal paragangliomas arise from paraganglia located in the retroperitoneum ; these paraganglia are symmetrically distributed along the abdominal aorta and are closely related to the orthosympathetic nervous systethey are responsible for secreting catecholamines ; the largest cluster of these paraganglia is found close to the origin of the inferior mesenteric artery and is known as the organ of zuckerkandl . 
retroperitoneal paragangliomas affect adults in the fourth and fifth decades of life , and in more than half the cases , they present with symptoms related to hypersecretion of catecholamine ( hypertension , tachycardia , flushing ) [ 28 , 29 ]  . 
on ct , they appear as solid expansile masses with tra questi , il gruppo pi consistente si trova in adiacenza dellemergenza dellarteria mesenterica inferiore ed noto come organo di zuckerkandl . 
colpiscono soggetti nella ivv decade di vita ed in pi della met dei casi si accompagnano a sintomi legati allipersecrezione di catecolamine ( ipertensione , tachicardia , flushing cutaneo ) [ 28 , 29 ]  . 
la scintigrafia con mibg , marcato con 123i , diversamente da tc e rm , fornisce informazioni di carattere funzionale - metabolico e , in relazione alla sua elevata specificit ( 97% ) , pu essere utilizzata per lidentificazione di neoplasie sincrone o di metastasi , 484 radiol med ( 2012 ) 117 : 471487 fig . 
axial contrast - enhanced ct images in the arterial ( a , b ) and venous ( c , d ) phases show an expansile solid mass with well - defined borders and heterogeneous appearance located between the abdominal aorta and the inferior vena cava , which is compressed and dislocated laterally . 
le immagini assiali tc post - mdc nelle fasi arteriosa ( a , b ) e venosa ( c , d ) mostrano una formazione espansiva solida a margini netti e struttura disomogenea disposta tra laorta addominale e la vena cava inferiore , che viene compressa e dislocata lateralmente . 
unlike ct and mri , metaiodobenzylguanidine ( mibg ) scintigraphy labelled with 123i provides useful functionalmetabolic information and , in view of its high specificity ( 97% ) , can be used to detect synchronous primary tumours or metastases , as well as to support the diagnosis of paraganglioma whenever morphological imaging is inconclusive [ 15 ]  . 
peraltro la diagnosi differenziale particolarmente complessa in quanto le caratteristiche tc - rm di queste neoplasie sono sovrapponibili a quelle di altri forme tumorali retroperitoneali , quali le neoplasie che originano dalle guaine nervose ( neurofibromi e schwannomi ) , tumori di origine mesodermica ( lipomi e liposarcomi , che se altamente indifferenziati presentano scarsa componente adiposa ) e leiomiosarcomi . 
infine , un fibroma istiocitico maligno , che origini in prossimit del rene o della ghiandola surrenale potrebbe essere indistinguibile da un paraganglioma dellilo renale [ 28 ]  . paragangliomi vescicali originano da paragangli simpatici contenuti nella parete vescicale , nel contesto del muscolo detrusore ; si tratta di paragangliomi sporadici per i quali non stata descritta radiol med ( 2012 ) 117 : 471487 fig . 
contrast - enhanced axial ( a ) and sagittal ( b ) ct images show an attenuating focal thickening on the posterior wall of the bladder ( arrow )  . 
le immagini tc post - mdc assiale ( a ) e sagittale ( b ) mostrano un ispessimento iperdenso della parete vescicale posteriore ( freccia ) , morfologicamente indistinguibile da una neoformazione vescicale ( carcinoma a cellule transizionali )  . 
finally , a malignant histiocytic fibroma arising close to the kidney or adrenal gland might prove indistinguishable from a paraganglioma of the renal hilum [ 28 ]  . bladder paragangliomas these paragangliomas arise from sympathetic paraganglia contained in the detrusor muscle of the bladder wall and are sporadic forms for which no mutation and / or association with genetically determined syndromes have been reported . 
mri , with its higher contrast resolution , highlights the difference between the moderate t2 hyperintensity of the paraganglioma and the high signal intensity of urine , providing not only a more accurate depiction of the lesion but also demonstration of its submucosal origafter paramagnetic contrast administration , there is strong enhancement [ 29 , 30 ]  . 
the differential diagnosis includes other bladder tumours ( transitional cell carcinoma or adenocarcinoma ) and proves extremely complex on the basis of morphological imaging alone . treatment the treatment of choice for paragangliomas is surgical resection . 
la rm , in relazione alla maggiore risoluzione di contrasto , fa risaltare la differenza tra la moderata iperintensit in t2 del paraganglioma e lelevato segnale dellurina , permettendo cos non solo una pi precisa identificazione della lesione ma anche di dimostrarne lorigine sottomucosa . 
la diagnosi differenziale va posta innanzitutto con neoplasie vescicali ( carcinoma a cellule transizionali o adenocarcinoma ) e rimane estremamente complessa sulla base del solo imaging morfologico . trattamento la terapia di scelta dei paragangliomi rappresentata dallasportazione chirurgica , con modalit peculiari che riguardano soprattutto le lesioni del distretto capo - collo , laddove il trattamento include non solo la resezione , ma pu comprendere anche la radioterapia e lembolizzazione o eventualmente una combinazione delle tre . 
per i paragangliomi 486 radiol med ( 2012 ) 117 : 471487 ment depends on many parameters , such as tumour size and extent and the presence of multicentric lesions . 
carotid - body paragangliomas are normally classified according to shamblins classification : type i are located between the internal and external carotid arteries and may be easily resected ; type ii adhere to and partially encircle the vessels ; type iii completely surround and encase the vessels . 
the operative morbidity of vagal and jugular paragangliomas is much higher than that of carotid - body tumours , which is explained by the fact that to ensure a truly radical procedure , it is often necessary to sacrifice cranial nerve x in vagal lesions , and nerves ix , x and xi are usually infiltrated in jugular lesions . 
surgical resection is also indicated in small tumours and in cases where there is a high possibility of radical removal without high morbidity or when the tumour has already caused cranial nerve impairment . 
in fact , in patients with malignant unresectable and / or metastatic paraganglioma and in those with multiple and / or recurrent lesions , radiometabolic therapy with 177lu - dotatoc or 90y - dotatoc [ 20 ] and / or for catecholamine secreting tumours with 131i - mibg is an option that should not be overlooked [ 31 ]  . 
finally , given the slow growth rate of these tumours , adoption of a conservative expectant approach with mri follow - up ( wait and scan approach ) may be reasonable in cases of asymptomatic tumours , young patients or patients with stable multifocal disease [ 23 ]  . carotidei viene usualmente utilizzata la classificazione di shamblin : i tumori di tipo i si localizzano tra le arterie carotide interna ed esterna e possono essere facilmente resecati ; quelli di tipo ii aderiscono o circondano parzialmente i vasi ; infine , quelli di tipo iii determinano encasement completo . 
la morbilit chirurgica dei paragangliomi vagali e giugulari molto pi elevata rispetto ai carotidei ed legata al fatto che per garantire una radicalit completa nei vagali spesso necessario sacrificare il x nervo , mentre ix , x e xi sono di solito infiltrati nei giugulari . 
peraltro , la resezione indicata in presenza di neoplasie di piccole dimensioni e qualora non comporti unelevata morbilit con alta possibilit di una resezione completa o quando la neoplasia abbia gi comunque causato un deficit dei nervi cranici . 
non va infatti dimenticata la possibilit , nei pazienti con paraganglioma maligno non resecabile e / o metastatico ed in quelli con lesioni multiple e / o recidivanti , di utilizzare la terapia radiometabolica con 177lu - dotatoc o 90y - dotatoc [ 20 ] e / o se secernenti catecolamine con 131i - mibg [ 31 ]  . 
infine , essendo neoplasie a lenta crescita , in assenza di sintomi e in pazienti giovani o con malattia multifocale e stabile pu essere assunto anche un atteggiamento conservativo che preveda lattesa e un follow - up rm nel tempo ( wait and scan degli autori anglossani ) [ 23 ]  . conclusioni conclusions the precise anatomical localisation of paragangliomas is essential in planning a surgical procedure aimed at achieving full extirpation of the tumour . 
integration of the different multiplanar morphological imaging modalities ( ct and mri ) provides crucial information for diagnosing and staging paragangliomas of the head and neck , chest , abdomen and pelvis . 
 functional imaging is indicated for detecting , staging and evaluating recurrences ; it is also fundamental for identifying patients who may benefit from radiometabolic therapies . la precisa localizzazione anatomica dei paragangliomi essenziale per pianificare un intervento che miri alla radicalit chirurgica . 
lintegrazione tra le diverse metodiche di imaging morfologico multiplanare ( tc - rm ) fornisce informazioni indispensabili nella diagnosi e nel bilancio di estensione dei paragangliomi del capo - collo , torace , addome e pelvi . 
bozzao1 1nesmos department , neuroradiology faculty , sant andrea hospital , la sapienza university , via di grottarossa 1035 , 00189 rome , italy 2radiotherapy department , santandrea hospital , rome , italy 3ircss san raffaele pisana , rome , italy correspondence to : m.c. 
brain perfusion maps and calculation of perfusion parameters , such as relative cerebral blood flow ( rcbf ) , relative cerebral blood volume ( rcbv ) and mean transit time ( mtt ) allow assessment of vascularity and angiogenesis within tumours of the central nervous system ( cns ) , thus providing additional information to conventional mri sequences . 
the aim of this review was to analyse the application of perfusion mri in the study of brain tumours by summarising our personal experience and the main results reported in the literature . keywords perfusion magnetic resonance imaging neuroradiology brain tumours riassunto lutilizzo della sequenza dinamica di perfusione con mezzo di contrasto ( dsc - pwi ) in risonanza magnetica ( rm ) nello studio dei tumori cerebrali fornisce informazioni sulle caratteristiche emodinamiche del tessuto neoplastico . 
 lelaborazione delle mappe di perfusione cerebrale ed il calcolo dei parametri di perfusione , come il flusso ematico cerebrale relativo ( rcbf ) , il volume ematico cerebrale relativo ( rcbv ) ed il tempo di transito medio ( mtt ) , consentono di studiare la vascolarizzazione ed i processi angiogenetici presenti nel contesto dei tumori del sistema nervoso centrale ( cns ) , fornendo informazioni aggiuntive alle sequenze rm convenzionali . 
 lo scopo di questa revisione quello di analizzare le applicazioni della sequenza di perfusione nello studio dei tumori cerebrali riassumendo lesperienza personale ed i principali risultati emergenti dalla letteratura . parole chiave perfusione risonanza magnetica neuroradiologia tumori cerebrali 446 radiol med ( 2012 ) 117 : 445460 general principles evaluating the microvasculature of a tissue and studying neoangiogenesis provide information enabling detection and characterisation of several conditions on the basis of their intrinsic microstructural features . 
the dynamic sequence ( dynamic susceptibility contrast , dsc ) allows assessment of local changes in the magnetic field , which are related to the passage of a paramagnetic contrast agent within tissues ( magnetic susceptibility )  . 
these changes in the magnetic field are translated into changes in signal intensity over time . in clinical practice , echoplanar images ( epi ) are more widely used for dynamic acquisitions in magnetic resonance imaging ( mri ) perfusion studies that are spin - echo ( se ) and gradient - echo ( gre ) sequences . 
in the field of neoangiogenesis studies , it is well known that epi sequences are more sensitive in the case of gross neovascularity than in microvascularisation , in which se sequences are more sensitive . 
this different sensitivity is , however , counterbalanced by a lower signal - to - noise ratio of se techniques , so that epi sequences are more frequently used in clinical practice . under physiological conditions , that is , with an intact bloodbrain barrier ( bbb ) , the intravenously administered contrast material effectively remains confined to the vascular region . 
this leads a steep local magnetic field gradient slope between the blood vessel and the surrounding interstitiu as water protons diffuse freely between the two compartments , this gradient causes the local magnetic field to become heterogeneous ( with altered magnetic susceptibility ) , which accelerates their loss of phase coherence and consequently of signal . 
in areas away from major vascular structures , loss of signal is usually uniform and proportional to the blood concentration of paramagnetic contrast agent . the effect of the first passage of a gadolinium bolus through the capillary region is to modify local magnetic susceptibility . 
these events can be detected using fast sequences in order to discriminate passage of the contrast bolus through the cerebral vascular bed over time , providing an index with which to measure haemodynamic parameters . 
 indeed , to determine relative cerebral blood volume ( rcbv ) or cerebral blood flow ( rcbf ) values using this approach , changes in mri signal intensity over time need to be converted into curves of contrast agent concentration in tissue over time . 
thus , cbv maps can be obtained by converting signal - intensity time curves into intravascular contrast conprincipi generali la valutazione della micro - vascolarizzazione di un tessuto , cos come lo studio della neo - angiogenesi , fornisce informazioni che permettono di identificare e caratterizzare alcune patologie in funzione delle loro caratteristiche microstrutturali intrinseche . 
la tecnica di perfusione con mezzo di contrasto si basa sulle modificazioni dellintensit di segnale , indotte dal passaggio dello stesso , allinterno dei tessuti cerebrali in un determinato tempo . 
la sequenza dinamica ( dynamic susceptibility contrast , dsc ) permette di valutare le modificazioni locali del campo magnetico legate al passaggio nei tessuti di un mezzo di contrasto paramagnetico ( fenomeno della suscettibilit magnetica )  . 
 nella pratica clinica le sequenze eco - planari ( epi ) sono quelle pi frequentemente impiegate per le acquisizioni dinamiche negli studi di perfusione in risonanza magnetica ( rm ) rispetto a sequenze spin - echo ( se ) e gradient - echo ( gre )  . 
nellambito degli studi sulla neoangiogenesi , noto che limpiego di sequenze epi ha una maggiore sensibilit verso una pi grossolana neo - vascolarizzazione rispetto ad una micro - vascolarizzazione in cui le se si dimostrano pi sensibili . 
questa diversa sensibilit tuttavia controbilanciata da una perdita del rapporto segnale - rumore delle tecniche spin - echo per cui pi spesso , nella pratica clinica , sono maggiormente utilizzate le sequenze epi . 
 in condizioni fisiologiche , cio con una barriera ematoencefalica integra ( bee ) , il mezzo di contrasto ( mdc ) iniettato per via venosa rimane effettivamente compartimentalizzato al solo distretto vascolare . 
tale fenomeno determina la comparsa di un ripido gradiente di campo magnetico locale tra vaso sanguigno e interstizio limitrofo ; poich i protoni dellacqua diffondono liberamente tra i due compartimenti , tale gradiente causa una disomogeneit del campo magnetico locale ( cio unalterata suscettibilit magnetica ) che provoca unaccelerazione della loro perdita di coerenza di fase e quindi di segnale . 
la rilevazione di questi eventi necessita di sequenze veloci , allo scopo di discriminare nel tempo il passaggio del bolo di mdc nel letto vascolare cerebrale fornendo un indice con il quale misurare i parametri emodinamici . 
infatti , per determinare il volume ematico cerebrale ( cbv ) o il flusso ematico cerebrale ( cbf ) relativi con questo approccio , necessario convertire le modificazioni dellintensit del segnale di rm nel tempo in curve di concentrazione tissutale del contrasto radiol med ( 2012 ) 117 : 445460 centration time curves and through their numerical integration . the intravascular contrast concentration time curve can also provide a measure of the mean transit time ( mtt ) and cbf . 
time curve and is usually determined by placing a region of interest ( roi ) over a major vessel , such as the middle cerebral artery ( mca )  . 
 basic principles in the study of neoplastic disease an important factor when evaluating the malignancy of brain tumours is the lesions ability to recruit vessels and develop a capillary network through growth and proliferation . 
 the perfusion technique allows this aspect to be studied in depth , with more accurate grading and survival prediction [ 1 ]  . gliomas histology is the reference standard for evaluating primary brain tumours . 
gliomas are classified according to the prevalent cell type , whereas grading is classified according to either the presence or absence of several features , such as cellular or nuclear pleomorphism , mitotic activity , cell and endothelial proliferation ( angiogenesis ) and necrosis [ 1 , 2 ]  . 
 dynamic susceptibility contrast perfusion - weighted imaging ( dsc - pwi ) is one of the noninvasive methods used to quantify the extent of neoplasm neovascularity [ 35 ]  . 
lowgrade glial lesions account for 20% of glial neoplasms of the central nervous system ( cns ) have an indolent clinical course and in most cases evolve into more aggressive forms . 
to date , there is no significant difference in terms of survival between patients who underwent biopsy only or a subtotal / total lesion resection ; starting radiotherapy early does not affect the total survival time [ 10 ]  . low - grade astrocytomas have increased cellularity and atypia on histology , but no mitotic figures , endothelial proliferations or necrosis , and on mri they show no contrast enhancement . 
la determinazione delle mappe di cbv , quindi , possibile grazie alla conversione delle curve intensit di segnale / tempo in curve concentrazione del mdc intravasale / tempo e alla loro integrazione numerica . dalla curva concentrazione del mdc intravasale / tempo inoltre possibile ottenere la misura del tempo di transito medio ( mtt ) e del cbf . 
 principi di base nello studio della patologia tumorale un importante fattore per valutare la malignit dei tumori cerebrali rappresentato dalla capacit della lesione di reclutare vasi e di sviluppare una rete capillare attraverso fenomeni di crescita e proliferazione . 
la tecnica di perfusione consente di studiare questo fenomeno migliorando la definizione di grading della neoplasia e consentendo di definire la sopravvivenza del paziente [ 1 ]  . gliomi listologia lo standard di riferimento per la valutazione dei tumori primitivi cerebrali . 
i gliomi vengono classificati sulla base del tipo cellulare predominante , mentre il grading viene classificato in base alla presenza o meno di alcune caratteristiche , quali il pleomorfismo cellulare e nucleare , lattivit mitotica , la proliferazione cellulare ed endoteliale ( angiogenesi ) e la presenza di necrosi [ 1 , 2 ]  . 
i valori di cbv relativo ( rcbv ) correlano con lattivit replicativa , con il grado istologico e con i livelli di colina riscontrati alla spettroscopia [ 69 ]  . 
lesioni tumorali gliali di basso grado rappresentano il 20% delle neoplasie gliali del sistema nervoso centrale ( snc ) , hanno un decorso clinico indolente e nella maggior parte dei casi evolvono verso forme pi aggressive . 
ad oggi , non esiste una significativa differenza in termini di sopravvivenza tra i pazienti che hanno effettuato soltanto biopsia , la resezione subtotale o totale della lesione ed iniziare la radioterapia precocemente non incide sul tempo di sopravvivenza totale [ 10 ]  . gli astrocitomi di basso grado presentano , dal punto di 448 radiol med ( 2012 ) 117 : 445460 ( gbm ) [ 1 ]  . 
in particular , it has been shown that low - grade gliomas with rcbv > 1.5 are more likely to evolve into high - grade gliomas than those with lower rcbv values [ 7 ]  . 
furthermore , although caution should be used when adopting any threshold value , an rcbv > 1.5 was found to be predictive of progression from low grade to high grade over a period of 365 days , whereas with values < 1.5 , this evolution occurred over a period of 889 days [ 10 ]  . for these same reasons , foci of pathological perfusion detected within a glial lesion with an apparently low malignancy grade may also become the target of a more focused biopsy procedure . 
this may also apply to high - grade tumours , which often contain foci of rcbv having heterogeneous values : in these cases the focus with the highest rcbv is considered representative of tumour grade , even in terms of contrast enhancement [ 2 ]  . 
 on the basis of these results , numerous studies have demonstrated that dsc - pwi , and in particular , the evaluation of rcbv values , can also be used to establish the prognosis of patients affected by cns glial tumours [ 1216 ]  . 
found that rcbv values are directly correlated with prognosis in patients with low - grade gliomas and are also better predictors of disease progression than is histological evaluation after biopsy or partial resection , or even contrast enhancement [ 12 , 16 ]  . 
in reality , according to this study , rcbv values ( using as a threshold an rcbv of 1.75 ) strongly correlate with time to disease progression , as well as with the patients clinical and treatment outcome : with a follow - up of 4.2 years , it was demonstrated that rcbv < 1.75 was indicative of gliomas showing stability over time or resolving completely after surgery , whereas gliomas with rcbv values > 1.75 showed radiological progression and clinical deterioration proportional to the increase in rcbv values [ 16 ]  . 
this observation has obvious implications for treatment ; a glioma classified as low grade on conventional imaging but with high cbv values should be treated more aggressively than one with low rcbv values . 
a patient with a low - grade glioma and low rcbv values might undergo close monitoring over time or be treated more conservatively than a patient with the same diagnosis but with high rcbv values [ 14 ]  . 
la presenza di elevati valori di rcbv nel contesto di alcune aree di un glioma apparentemente di basso grado ( quindi in assenza di potenziamenti patologici dopo mdc ) pu essere linizio di una neoangiogenesi e quindi potenziale indice di maggiore grading o progressione di malattia [ 10 ]  . 
in particolare , stato dimostrato che gliomi di basso grado con valori di rcbv > 1 , 5 evolvono pi probabilmente in gliomi di alto grado rispetto ai tumori con valori di rcbv inferiori [ 7 ]  . 
inoltre , sebbene ladozione di un qualsiasi valore soglia debba essere considerato con la dovuta cautela , un rcbv > 1 , 5 risultato predittivo di progressione da basso ad alto grado in 365 giorni a differenza di valori < 1 , 5 in cui tale evoluzione si verificata in 889 giorni [ 10 ]  . 
 per gli stessi motivi lidentificazione di focolai di perfusione patologica nel contesto di una lesione gliale apparentemente di basso grado di malignit pu essere anche il target per una pi mirata procedura bioptica . 
ci pu essere valido anche nei tumori di alto grado che contengono spesso foci di rcbv con valori eterogenei : in questi casi , il focolaio di massimo rcbv considerato rappresentativo , anche nellambito del potenziamento , del grado tumorale [ 2 ]  . 
 [ 13 , 17 ] hanno documentato , infatti , come i valori di rcbv siano direttamente correlati con la prognosi dei pazienti affetti da gliomi di basso grado e rappresentino , inoltre , dei predittori di progressione neoplastica migliori rispetto alla valutazione istologica post - biopsia o dopo resezione parziale o rispetto al grado di potenziamento dopo mdc [ 12 , 16 ]  . 
in effetti , secondo questi studi i valori di rcbv ( utilizzando come soglia un rcbv pari a 1 , 75 ) correlano fortemente con il tempo di progressione della neoplasia e quindi con loutcome clinico e terapeutico del paziente in quanto , con un follow - up di 4 , 2 anni , stato dimostrato che un valore di rcbv < 1 , 75 era rappresentativo di gliomi stabili nel tempo o con completa risoluzione dopo terapia chirurgica a differenza di gliomi con valori di rcbv > 1 , 75 che mostravano una progressione radiologica ed un peggioramento clinico proporzionale allaumentare del rcbv stessi [ 16 ]  . 
questa osservazione ha delle ovvie implicazioni terapeutiche ; un glioma classificabile come di basso grado allimaging convenzionale , ma con un cbv alto dovrebbe essere trattato in modo pi aggressivo rispetto ad un tumore con valori di rcbv bassi . 
un paziente con radiol med ( 2012 ) 117 : 445460 oligodendrogliomas oligodendrogliomas are uncommon but distinct tumours , generally characterised by long patient survival , better treatment response and characteristic genetic alterations [ 17 ]  . 
therefore , if the finding of high rcbv values in the context of nonenhancing glial lesions is compatible with the presence of tissue undergoing histological transformation into more anaplastic forms , this concept no longer applies to oligodendrogliomas . 
this rich microvascularity may reflect the presence of powerful proangiogenic mutagens , such as vascular endothelial growth factor ( vegf ) or the hypoxia - inducible factor ( hif ) - 1 , which contribute to neovascularity and vascular hyperplasia [ 20 ]  . 
conventional mri in the follow - up of low - grade gliomas considering the literature data concerning the value of pwi information in the transformation and progression of lowgrade glial tumours , researchers have investigated whether this method is superior to conventional mri in monitoring such neoplasms and whether its use should be considered in daily clinical practice [ 21 ]  . 
assessed the role of rcbv values and tumour volume changes evaluated with fluid - attenuated inversion recovery ( flair ) sequences to predict the transformation of glial tumours from low to high grade . 
the study demonstrated that changes in tumour volun glioma di basso grado ed un rcbv basso potrebbe essere sottoposto a controlli ripetuti nel tempo o essere trattato in modo pi conservativo , rispetto ad un paziente con la stessa diagnosi , ma con rcbv alto [ 14 ]  . 
 oligodendrogliomi gli oligodendrogliomi sono forme tumorali non comuni ma ben distinte , caratterizzate generalmente da lunga sopravvivenza , migliore risposta al trattamento e caratteristiche alterazioni genetiche [ 17 ]  . 
ponendo un cut - off pari a 1 , 5 di rcbv normalmente nessun tumore di basso grado si pone al di sopra di tale limite , eccezion fatta per gli oligodendrogliomi . 
pertanto , se il riscontro di valori di rcbv alti nel contesto di lesioni gliali che non mostrano potenziamento dopo somministrazione di mdc era compatibile con la presenza di un tessuto in fase di viraggio istologico verso forme pi anaplastiche , questo concetto non pi valido considerando gli oligodendrogliomi . 
una delle ragioni di questo fenomeno potrebbe essere rappresentata dal fatto che la maggior parte degli oligodendrogliomi sono localizzati in sede corticale , regione pi ricca di vasi [ 18 ]  . 
questa ricca micro - vascolarizzazione potrebbe essere lespressione della presenza di potenti mutageni pro - angiogenici come il fattore di crescita dellendotelio vascolare ( vegf ) o fattore stimolato dallipossia ( hif ) - 1 che contribuiscono alla neovascolarizzazione e alla iperplasia vascolare [ 20 ]  . 
 gli oligodendrogliomi di basso grado con la mutazione presentano una risposta positiva in particolare al trattamento con farmaci lipofilici ( come ad esempio procarbazina , lomustina e temozolomide ) , che facilmente attraversano la barriera emato - encefalica ed hanno un prolungato tempo di sopravvivenza . 450 radiol med ( 2012 ) 117 : 445460 fig . 
conventional sequences documents similar radiological patterns in low - grade astrocytomas ( a , b ) , anaplastic astrocytomas ( d , e ) and grade ii oligodendrogliomas ( g , h )  . 
in relative cerebral blood volume ( rcbv ) maps , low - grade astrocytomas can be distinguished from the remaining two categories because of the low rcbv values ( c , f , i , arrows )  . 
limmagine mostra come le sequenze convenzionali possano documentare simili pattern radiologici negli astrocitomi di basso grado ( a , b ) , anaplastici ( d , e ) e negli oligodendrogliomi di ii grado ( g , h )  . 
nelle mappe di rcbv gli astrocitomi di basso grado si differenziano dalle restanti due categorie per ridotti valori del parametro ( c , f , i , frecce )  . 
hyperintense lesion in a flair image ( a ) in the right temporal lobe and in the insular cortex without significant increase of rcbv values on perfusion maps ( b )  . 
a mostra una lesione iperintensa nellimmagine flair a livello del lobo temporale di destra e della corteccia insulare senza significativo aumento dei valori di rcbv nelle mappe di perfusione ( b )  . 
dopo 3 anni , limmagine rm di controllo mostrano un aumento di volume della lesione nella sequenza flair ( c ) e , contestualmente , dei valori di rcbv nelle mappe di perfusione ( d )  . yet be considered superior to conventional t2 - weighted or flair sequences in predicting malignant transformation of low - grade tumours . cerebral lymphomas over the last two decades , the incidence of cerebral lymphomas has increased along with the number of immunocompromised patients ( affected by tumours , aids , or transplanted )  . 
the rcbv delle informazioni fornite dalla pwi nellambito della trasformazione e della progressione dei tumori gliali di basso grado , ci si posti il quesito se questa metodica sia superiore rispetto alle sequenze rm convenzionali nel controllo di tali neoplasie e debba pertanto essere considerata per tale scopo nella pratica clinica quotidiana [ 21 ]  . 
 [ 10 ] hanno valutato , in 34 pazienti , il ruolo predittivo dei valori di rcbv e della variazione del volume tumorale , valutato con sequenze fast fluid - attenuated inversion - recovery ( flair ) , nella trasformazione da basso ad alto grado di tumori gliali . 
pertanto , sulla base dei dati disponibili , la dsc - pwi non pu essere ancora considerata superiore alla valutazione delle sequenze t2 convenzionali o delle sequenze flair nel predire la trasformazione maligna di un tumore di basso grado . linfomi cerebrali nelle ultime due decadi lincidenza dei linfomi cerebrali 452 radiol med ( 2012 ) 117 : 445460 fig . 
3a - i primary cerebral lymphoma ( a - c ) , secondary lymphoma ( d - f ) and secondary localisation of leukaemia ( g - i )  . 
il parametro rcbv , aumentato solo nel linfoma non hodgkin ( d - f ) , differenzia questa patologia dalle altre due in cui lrcbv risulta ridotto ( c , i )  . radiol med ( 2012 ) 117 : 445460 values are apparently comparable with those of low - grade gliomas , which , however , show no contrast enhancement in conventional sequences . 
differentiating a lymphoma from a low - grade glioma is thus still possible thanks to the presence of contrast enhancement in the former . in a study by lee et al . 
the statistically significant result obtained was that the rcbv value of the perilesional oedema of malignant meningiomas was higher than in benign meningiomas , being the expression of a likely infiltration of cerebral tissue and the presence of vascular proliferation [ 27 ]  . 
this value is significantly different from those found in dural metastatic lesions ( 1.263.34 ) , making it easy to distinguish these masses from real meningiomas [ 28 ]  . 
la possibilit di differenziare un linfoma da un glioma di basso grado quindi tuttora possibile grazie alla presenza del potenziamento dopo mdc dei linfomi rispetto ai gliomi . in uno studio di lee et al . 
 [ 25 ] la maggior parte dei linfomi cerebrali primitivi mostravano valori di rcbv inferiori a 2 , 3 ( valore medio 1 , 68 ) , risultati significativamente inferiori rispetto ai valori di rcbv riscontrabili nei gliomi di alto grado ( 4 , 037 , 32 ) , metastasi ( 4 , 685 , 27 ) o meningiomi ( 8 , 0210 , 58 ) [ 25 ]  . 
potenziali applicazioni della tecnica di perfusione in questo campo sono la caratterizzazione di forme con apparente maggiore aggressivit biologica e la diagnosi differenziale con lesioni a localizzazione meningea di natura secondaria . 
 454 metastasis despite considerable advances in neuroradiological diagnosis and follow - up of brain tumours , the differential diagnosis between primary and secondary solitary brain neoplasms is often only achieved with histological characterisation . 
on the other hand , to obtain accurate staging and plan appropriate treatment , the ability to differentiate noninvasively between primary brain tumours and metastases appears useful , especially when these are solitary secondary localisations developing in patients with unknown primary and when no univocal clinical and patient history are available . 
dscpwi appears to be a highly promising tool in this field , as it provides information on the peculiar haemodynamic aspects of the pathological tissue under study . at a histological level , anaplastic gliomas can be distinguished from metastases by the different organisation of vascular structures produced by neoangiogenesis , which translate into differences in haemodynamics . 
neoangiogenesis of metastases , instead , reflects vascularity characteristics of the tissue they arise from ; as a result , the bbb is always absent , and a marked increase in capillary permeability is always observed , which accounts for the frequent early finding of extensive vasogenic oedema around the lesion . pathophysiological changes affecting areas surrounding the tumour ( peritumoral regions ; ptr ) are also varied : histologically : glioblastoma ptr show , in addition to vasogenic oedema , infiltrating glial cells and neoplastic capillaries that may be responsible for possible increases in the rcbv parameter . 
metastases ptr appear predominantly characterised by vasogenic oedema due to the passage of plasma through the part of capillaries without bbb , with compression of microcirculation structures and a resulting reduction in blood flow ( decreased rcbv parameter ) [ 2931 ]  . in addition to rcbv , which is the most reliable perfusion parameter in terms of vascular hyperplasia quantification , some studies evaluated the usefulness of two other haemodynamic perfusion variables that can be extrapolated from the time - signal intensity curves : peak height and percentage of signal recovery . 
peak height is defined as the highest drop radiol med ( 2012 ) 117 : 445460 uno con caratteristiche maligne importante sia per poter decidere lapproccio terapeutico e leventuale trattamento adiuvante che per stabilire loutcome del paziente . 
il risultato statisticamente significativo ottenuto era che il valore di rcbv in corrispondenza delledema peritumorale dei meningiomi maligni era maggiore rispetto a quello dei meningiomi benigni , espressione di una probabile infiltrazione del tessuto cerebrale e della presenza di proliferazione vascolare [ 27 ]  . 
tale valore risulta significativamente differente dai valori di rcbv nelle lesioni metastatiche durali ( 1 , 263 , 34 ) rendendo facilmente distinguibili tali neoformazioni dai veri meningiomi [ 28 ]  . 
 metastasi nonostante i notevoli progressi che si sono compiuti nellultimo decennio in ambito neuro - radiologico nella diagnosi e nel follow - up dei tumori cerebrali , una diagnosi differenziale di certezza tra neoformazioni cerebrali primitive e secondarie con singola localizzazione spesso formulabile solo tramite una caratterizzazione istologica . 
daltra parte ai fini di una corretta stadiazione e di unadeguata pianificazione del trattamento appare di grande utilit poter differenziare in maniera non invasiva i tumori cerebrali primitivi dalle metastasi soprattutto quando si tratta di localizzazioni secondarie solitarie che si sviluppano in pazienti in cui la neoplasia primitiva non nota e non sono disponibili elementi clinici e anamnestici univoci . 
 dal punto di vista istologico , i gliomi anaplastici si distinguono dalle metastasi in relazione ad una diversa organizzazione delle strutture vascolari prodotte dai fenomeni di neoangiogenesi del tessuto neoplastico che si traducono in differenze proprio sul piano emodinamico . 
anche la permeabilit capillare delle metastasi differisce da quella dei glioblastomi : nelle neoplasie primitive del snc ed in particolare nei tumori gliali sono presenti componenti vascolari displasiche eterogenee che possono simulare la vascolarizzazione del tessuto cerebrale normale per cui radiol med ( 2012 ) 117 : 445460 la barriera emato - encefalica ( bee ) spesso conservata e la permeabilit del tessuto neoplastico pu essere estremamente variabile in uno spettro compreso tra valori del tutto normali ( ovvero sovrapponibili a quelli del tessuto cerebrale normale ) e valori aumentati . 
la neoangiogenesi delle metastasi , invece , riflette le caratteristiche di vascolarizzazione del tessuto da cui esse originano per cui la bee sempre assente e di conseguenza si osserva costantemente un marcato incremento della permeabilit capillare che spiega il frequente e precoce riscontro di un esteso edema vasogenico perilesionale . anche le modificazioni fisiopatologiche cui vanno incontro le aree circostanti il tumore ( regioni peritumorali , rpt ) sono diverse : dal punto di vista istologico nelle rpt dei glioblastomi sono presenti , oltre alledema vasogenico anche cellule gliali infiltranti e capillari neoplastici che possono essere alla base di possibili aumenti del parametro rcbv . 
le rpt delle metastasi appaiono prevalentemente caratterizzate da edema vasogenico in relazione al passaggio del plasma attraverso la parte di capillari privi della bee con fenomeni compressivi a carico delle strutture del microcircolo e conseguente riduzione del flusso ematico ( riduzione del parametro rcbv ) [ 2931 ]  . oltre al rcbv , che rappresenta il pi attendibile parametro di perfusione in termini di quantificazione delliperplasia vascolare , alcuni studi hanno valutato lutilit di altre due variabili emodinamiche di perfusione estrapolabili dalle curve intensit - tempo : laltezza del picco e la percentuale di recupero del segnale . 
laltezza del picco si definisce come la massima caduta dellintensit di segnale dalla fase pre - contrastografica durante il passaggio del bolo di mdc , esprime quindi il volume capillare totale ed direttamente correlato con il cbv . 
in una popolazione di pazienti con diagnosi ( confermata istologicamente ) di glioblastoma o metastasi cerebrale il parametro di picco di caduta del segnale stato misurato sia in corrispondenza delle lesioni che a livello delle rpt [ 32 ]  . 
i valori di altezza del picco misurati nel contesto delle lesioni sono risultati sovrapponibili tra le due popolazioni mentre i valori di picco misurati nelle rpt delle metastasi sono risultati significativamente minori rispetto alle rpt dei gbm . 
in a patient with a high - grade brain glioma ( a ) a perfusion curve with regular recovery of the venous plateau ( c , box ) is evident compared with a secondary lesion ( b ) , which shows increased capillary permeability and decreased curve recovery corresponding to the venous washout phase ( d , box )  . 
nel paziente affetto da glioma cerebrale di alto grado di malignit ( a ) evidente la presenza di una curva di perfusione con regolare recupero del plateau venoso ( c , riquadro ) rispetto ad una lesione secondaria ( b ) che mostra aumento della permeabilit capillare ed un ridotto recupero della curva corrispondente alla fase di wash - out venoso ( d , riquadro )  . 
nelle immagini ( c , d ) si evidenzia la demarcazione tra il tessuto patologico ( curve di perfusione ) e la quota edemigena perilesionale . in signal intensity from the precontrast phase during the passage of contrast bolus ; as such , it expresses total capillary volume and is directly correlated to cbv . 
in a population of patients with a diagnosis of glioblastoma or brain metastasis ( confirmed histologically ) , the peak height of maximal signal drop was measured both within the lesions and in the ptr . 
the peak height values measured within the lesions were found to be comparable between the two populations , whereas the peak height values measured in the metastatic ptr were significantly lower than in glioblastoma ptr . 
 radiation necrosis one of the possible evolutions of radiotherapy ( rt ) in treating brain tumours is the presence of radiation necrosis ( rn ) , which , in most cases , develops in the site of the previous tumour . 
it is thus often difficult to determine , based on conventional semiotics , whether a lesion developing after radiotherapy at the site of the tumour is a recurrence or a radiation necrosis , because this is characterised by mass effect , contrast enhancement and perilesional oedema . 
 the possibility of differentiating radiation necrosis from tumour recurrences has enormous clinical significance , not only from a prognostic but also from a therapeutic point of view : if , however , treating a recurrence may involve repeat surgery , in the case of radiation necrosis , steroid therapy is usually indicated . 
 [ 33 ] report that within tumour recurrences ( later confirmed by biopsy or clinicalradiological criteria seen during a 9 - month follow - up ) , the ratio between cbv in diseased tissue and normal contralateral tissue ( rcbv ) exceeded 2.6 , whereas in radiation necrosis , the cbv ratio remained < 0.6. 
some authors state that an rcbv value of 0.71 constitutes a demarcation line allowing glioblastoma recurrences to be differentiated from radiation necrosis with more than 90% sensitivity and 100% specificity [ 34 ]  . 
others suggest that an rcbv value > 2.1 may be considered the optimal parameter to differentiate between recurrence and radiation necrosis , ensuring 100% sensitivity and more than 95% specificity [ 35 ]  . 
other studies confirmed the presence of lower rcbv values in the areas affected by postactinic trattamento dei tumori cerebrali la presenza di radionecrosi ( rn ) che , nella maggior parte dei casi , si sviluppa nella sede della precedente patologia tumorale . 
quindi spesso difficile determinare sulla base dei dati della semeiotica convenzionale se una lesione che si sviluppa a distanza di tempo dal trattamento con rt nella sede del tumore , possa rappresentare una recidiva o una radionecrosi essendo caratterizzata da effetto massa , potenziamento dopo mdc ed edema perilesionale . 
 daltronde la possibilit di differenziare la rn dalle recidive tumorali di enorme rilevanza clinica non solo dal punto di vista prognostico ma anche terapeutico : se da un lato il trattamento delle recidive pu prevedere il re - intervento chirurgico , in caso di rn indicata normalmente , come unico approccio , la terapia steroidea . 
allo stato attuale per una diagnosi differenziale di certezza tra recidiva e rn indispensabile la caratterizzazione istologica poich gli aspetti clinici o di imaging convenzionale non consentono di differenziare con certezza le due condizioni . 
 [ 33 ] , lautore documenta che nel contesto delle recidive tumorali ( confermate successivamente con esame bioptico o sulla base di criteri clinico - radiologici emersi in un follow - up di 9 mesi ) il rapporto tra il cbv del tessuto patologico ed il tessuto controlaterale sano ( rcbv ) risultato maggiore di 2 , 6 mentre nei casi di rn il cbv ratio si attestato su valori inferiori a 0 , 6 . 
nei casi in cui esisteva una sovrapposizione nei valori di rcbv tra i due gruppi gli autori suggeriscono la necessit di un completamento diagnostico con lesecuzione di studi pet . alcuni autori affermano che un valore di rcbv pari a 0 , 71 rappresenta una linea di confine che consente di differenziare con una sensibilit superiore al 90% ed una specificit del 100% , le recidive da glioblastoma dalla rn [ 34 ]  . 
 altri suggeriscono che un valore di rcbv maggiore di 2 , 1 possa essere considerato il parametro ottimale per la differenziazione tra recidiva e rn garantendo una sensibili t del 100% ed una specificit superiore al 95% [ 35 ]  . 
chiaro che i valori di sensibilit e specificit variano in funzione dei parametri scelti per lesistenza di una zona di confine in cui le due patologie possono coesistere e pertanto la dsc - pwi pu indirizzare prevalentemente , ma non in termini assoluti , verso una delle patogenesi . oltre al pi utilizzato parametro cbv , recentemente sono stati introdotti altri parametri emodinamici utili nella valutazione della patologia post - attinica . 
il valore relativo dellaltezza di picco ( rph ) ed la percentuale di recupero dellintensit di segnale ( psr ) sono due indici sensibili radiol med ( 2012 ) 117 : 445460 fig . 
presence of pathological tissue in the right temporal region ( a , b ) with enhancement after contrast administration in association with surrounding oedema and decreased rcbv values ( c , arrow ) , consistent with necrotic tissue after radiotherapy . 
in a , b viene documentata la presenza di un tessuto patologico in regione temporale destra che mostra potenziamento dopo mezzo di contrasto in associazione ad edema perilesionale , in presenza di ridotti valori di rcbv ( c , freccia ) compatibili con tessuto necrotico in esito di terapia radiante . 
it is clear that sensitivity and specificity values vary according to chosen parameters due to the existence of a border area in which the two diseases coexist and that dsc - pwi can prevalently guide towards one type of pathogenesis , but not in absolute terms . in addition to the more widely used cbv parameter , other useful haemodynamic parameters have been introduced to evaluate postactinic disease . 
relative peak height ( rph ) and percentage of signal intensity recovery ( psr ) are two indices sensitive to changes in magnetic susceptibility at passage of contrast material into the intracranial vascular compartments . 
 [ 36 ] hanno dimostrato lutilit di tali parametri nella valutazione del tessuto radio - necrotico e della recidiva tumorale , esistendo una significativa differenza tra i due quadri patologici . 
gli autori suggeriscono che il parametro ph rappresenti un indice quantificabile della vascolarizzazione tumorale , correlato al valore di rcbv ed espressione del volume vascolare totale allinterno di una regione di interesse . 
il psr rappresenta invece il parametro pi sensibile nel riconoscere le modificazioni strutturali del microcircolo ; valori ridotti del parametro , evidenti nelle recidive di glioblastoma , sono imputabili al danno della bee , che risulta altamente permeabile alle macromolecole del mezzo di contrasto . 
gli autori concludono sottolineando lutilit di tali parametri di perfusione 458 radiol med ( 2012 ) 117 : 445460 vascularity , which is correlated with the rcbv value and expresses total vascular volume within an roi . 
the authors conclude by emphasising the usefulness of these perfusion parameters in distinguishing radiation necrosis from tumour recurrences and the importance of completing an mri study with perfusion sequences to differentiate these pathological aspects [ 36 , 37 ]  . main limitations the first limitation of this technique is that it provides relative data . 
since this technique is susceptibility weighted , it is extremely sensitive to structures or lesions that induce strong inhomogeneity in the magnetic field , such as blood products , calcium , melanin , metals or lesions located near the brain boneair interface ( anterior and middle cranial fossa )  . 
in these cases , the t1 - relaxing effect of gadolinium in the tissue in which it has diffused ( dipoledipole interactions ) predominates and counterbalances the decreased t2 * signal intensity , giving falsely decreased rcbv values . 
in the presence of a damaged bbb , the injection of a small amount of contrast material ( 0.0250.05 mmol / kg ) 510 min before the bolus injection is recommended to saturate the areas with high vascular permeability and reduce the effect of contrast extravasation on the t2 * signal . a further limitation concerns small lesions and those located subcortically , close to arterial structures . 
this problem is particularly relevant in high - grade tumours , given the great heterogeneity of these tissues . nel distinguere la radionecrosi dalla recidiva tumorale e suggerendo limportanza di completare uno studio rm con sequenze di perfusione per differenziare tali aspetti patologici [ 36 , 37 ]  . 
poich questa tecnica pesata sulla suscettibilit , risulta estremamente sensibile alle strutture o lesioni che inducono una forte disomogeneit del campo magnetico , come i prodotti del sangue , il calcio , la melanina , i metalli o le lesioni localizzate vicino allinterfaccia tessuto cerebrale - osso - aria ( fossa cranica media e anteriore )  . 
in questi casi , leffetto t1 rilassante del gadolinio nel tessuto in cui si diffuso ( interazioni dipolo - dipolo ) , predomina e controbilancia la riduzione di intensit di segnale t2 * risultandone valori di rcbv falsamente diminuiti . 
in presenza di una bee danneggiata viene consigliata liniezione di una piccola quantit di mdc ( 0 , 0250 , 05 mmol / kg ) 510 minuti prima delliniezione del bolo , in maniera da saturare le aree ad elevata permeabilit vascolare , per ridurre leffetto dello stravaso di contrasto sul segnale t2 *  . 
bonomo1 1dipartimento di bioimmagini e scienze radiologiche , istituto di radiologia , universit cattolica del sacro cuore , largo francesco vito 1 , 00168 roma , italy 2dipartimento di diagnostica per immagini , universit degli studi di foggia , viale luigi pinto 1 , 71100 foggia , italy 3dipartimento di radiologia , ospedale irccs casa sollievo della sofferenza , viale dei cappuccini 1 , 71013 san giovanni rotondo , foggia , italy correspondence to : t . 
the aim of this paper is to demonstrate that computed tomography ( ct ) and three - dimensional ( 3d ) ct imaging techniques can be useful tools for evaluating gunshot wounds of the skull in forensic medicine . 
ct imaging techniques are excellent tools for addressing the most important questions of forensic medicine in the case of gunshot wounds of the skull , with results as good as ( or sometimes better than ) traditional autoptic methods . 
le tecniche dimaging tc sono in grado di soddisfare con performances uguali o , in alcuni casi , superiori alla metodica autoptica tradizionale , molti dei principali quesiti forensi in casi di ferite cranio - encefaliche darma da fuoco a carica singola . 462 radiol med ( 2012 ) 117 : 461470 keywords virtopsy brain gunshot injury 3d - ct reconstructions parole chiave autopsia virtuale lesioni cerebrali da arma da fuoco ricostruzioni 3d - tc introduction introduzione since their inception , radiological sciences have enjoyed a close connection with forensic medicine . 
the first radiographic documentation of gunshot wounds dates back to 1895 , the year in which x - rays were discovered , whereas the first radiographic study of a cadaver was performed in 1898 [ 1 ]  . 
in the past 30 years , the connection between radiology and forensic medicine has been revitalised by the remarkable progress of diagnostic imaging and the introduction of computed tomography ( ct ) in forensic investigations on corpses . 
in the following years , the spread of spiral ct opened the door to 3d acquisitions and postprocessing , and ct increasingly became a standardised modality for evaluating intracranial gunshot wounds , making its unique contribution to forensic science . it is now widely recognised [ 47 ] that ct scanning and 3d reconstructions can provide fast , accurate and complete demonstration of : bullet location and bullet and bone fragments within the skull ; intracranial course of the bullet ; skull fractures associated with the gunshot wound . 
 the aim of this study was to establish , on the basis of our experience with cranioencephalic gunshot wounds , whether the advances in ct and 3d imaging techniques can be transferred to the medicolegal domain to assist in three specific tasks : locating , describing and differentiating the bullet entrance and , if present , exit wound ; identifying the intracranial trajectory of the bullet through depiction of bony and parenchymal lesions ; identifying elements that may help in formulating hypotheses about the dynamics of the event . materials and methods uno stretto legame con la medicina legale ha caratterizzato le scienze radiologiche fin dai loro inizi . 
la prima documentazione radiografica di ferite da arma da fuoco , infatti , risale al 1895 , anno della scoperta dei raggi x , mentre nel 1898 fu eseguito il primo esame radiografico su cadavere [ 1 ]  . 
nellultimo trentennio , si assistito alla rivitalizzazione di questo connubio grazie agli enormi progressi della diagnostica per immagini e allintroduzione ed ottimizzazione di metodiche di imaging con tomografia computerizzata ( tc ) nelle investigazioni forensi su cadavere . 
cronologicamente si deve a wullenweber [ 3 ] nel 1977 la prima applicazione forense della tc mirata alla descrizione dei caratteri di una lesione da arma da fuoco alla testa . 
in seguito , la diffusione della tc spirale ha aperto le porte allacquisizione e al post - processing tridimensionale divenendo sempre pi un metodo standardizzato nella valutazione delle lesioni cranio - encefaliche da arma da fuoco e apportando un contributo peculiare alla scienza forense . ad oggi stato ampiamente riconosciuto [ 47 ] che lindagine tc e le ricostruzioni tridimensionali sono in grado di delineare in maniera rapida , accurata e completa : la posizione del proiettile , dei suoi frammenti e di frammenti ossei nel cranio nelle tre dimensioni ; la traiettoria intracranica del proiettile ; le fratture craniche associate alla lesione ; vicariando , quando possibile , la tecnica autoptica tradizionale . 
 lobiettivo del nostro studio appunto quello di stabilire , attraverso la nostra esperienza sulle lesioni darma da fuoco cranio - encefaliche , se il progresso nelle tecniche dimmagine tc e 3d - tc pu essere trasferito in ambito medico - legale tanto da consentire di rispondere a tre quesiti specifici : individuare e descrivere il foro dentrata e , ove presente , quello di uscita del proiettile , differenziandoli tra di loro ; individuare la traiettoria intrasomatica del proiettile attraverso lo studio delle lesioni ossee e parenchimali ; fornire elementi utili alla formulazione di ipotesi riguardanti la dinamica dellevento . our experience is based on ten cases of fatal cranioencephalic wounds caused by a single bullet . 
all cases underwent postmortem total - body ct imaging and convenmateriali e metodi la nostra esperienza si basa su 10 casi di ferite cranio - encefaliche mortali da singolo proiettile esploso da arma da radiol med ( 2012 ) 117 : 461470 tional autopsy , the findings of which were considered the gold standard . 
in 9 / 10 cases the ct study was performed within 72 h of death and prior to autopsy ; in the remaining case , it was carried out after exhumation of the body 10 years after the individuals death . 
nine of ten cases were imaged with multislice ct scanners and , specifically , with a 16 - slice scanner in four cases and a 64 - slice device in the remaining five . 
for all examinations , 3d surface reconstructions with volume - rendering technique and 2d images in multiple planes were obtained . two radiologists with specific experience in neuroimaging and postmortem imaging independently assessed the images of the head and neck region . 
the two radiologists were asked to note the number of holes detected on the skull ; distinguish the bullet entrance and , if present , exit wound ; locate in the three spatial planes the final position of the bullet and bullet and bone fragments ; describe tissue lesions so as to trace the bullets likely course within the victims body . 
results obtained by the two readers were compared with each other and with the autopsy report and circumstantial evidence . results in 8 / 10 cases , both examiners identified two wounds in the skull and distinguished the entrance wound from the exit wound . 
in these cases , the bullets intracranial course was defined in the three spatial planes by ideally joining the entrance and exit holes and considering the spatial distribution of bone fragments and lesions caused by the passage of the bullet within the bra in all cases , on entering the skull , the bullet broke up into several metallic fragments . 
the bullets intracranial course was defined in both cases by studying the final location of the largest bullet fragment , the smaller fragments , the bone fragments and the tissual signs of the bullets passage ( haemorrhage / air bubbles )  . 
the trajectory angles in the three spatial planes calculated by the two observers did not reveal significant differences in amplitude . comparison with autopsy findings did not reveal any disagreement in the number of bullet holes detected in the skull fuoco a carica singola . 
in tutti i casi , stato eseguito uno studio dimaging post - mortale total body mediante apparecchiatura tc ed un esame autoptico , i cui rilievi sono stati utilizzati come gold standard . 
in 9 / 10 casi lo studio tc stato eseguito entro le 72 ore successive al decesso e prima dellautopsia ; nel caso rimanente , a distanza di 10 anni , dopo la riesumazione del cadavere . 
in 9 / 10 casi , sono state utilizzate apparecchiature tc multistrato , rispettivamente in 4 casi con un tomografo a 16 strati , nei restanti 5 con un tomografo a 64 strati . 
per tutti gli esami sono state ottenute ricostruzioni 3d di superficie con tecnica volume rendering , nonch immagini 2d secondo piani multipli . due radiologi con specifica esperienza in neuroimaging e imaging post - mortale hanno esaminato indipendentemente fra loro le immagini del distretto cranio e collo . 
per ciascun caso , stato richiesto ai radiologi di annotare il numero di fori presenti sulla teca cranica ; di distinguere il foro di entrata , ed eventualmente quello di uscita del proiettile ; di individuare nei tre piani dello spazio la posizione finale dei proiettili , dei loro frammenti e dei frammenti ossei , di descrivere le lesioni tissutali al fine di tracciare le probabili traiettorie dei proiettili nel corpo delle vittime . 
i risultati ottenuti dai due osservatori sono stati confrontati fra loro e con i dati autoptici e circostanziali . risultati in 8 / 10 casi analizzati , gli esaminatori hanno concordemente individuato due fori nella teca cranica e distinto il foro dentrata del proiettile , da quello di uscita . 
in questi casi , la traiettoria intrasomatica stata definita nei tre piani dello spazio congiungendo idealmente il foro dentrata con quello duscita e tenendo conto della distribuzione spaziale nellencefalo dei frammenti ossei e delle lesioni tissutali causate dal passaggio del proiettile . 
la traiettoria intrasomatica stata definita in entrambi i casi attraverso lo studio della posizione finale del frammento di maggiori dimensioni del proiettile , dei frammenti pi piccoli , dei frammenti ossei e dei segni tissutali del passaggio del proiettile ( emorragie / bolle daria )  . 
ct proved to be superior to conventional autopsy for describing the entrance hole when this was located at the skull base ; 3d - ct imaging allowed the bullets intracranial course to be traced in a manner similar to autopsy but proved superior in locating the bullet and / or bone fragments and thus depicting the bullets intracranial course in the three spatial planes . 
 in one case , ct allowed the detection of a bullet wound in the musculofascial tissues of the neck also , and enabled its trajectory to be defined . discussion results of our study demonstrated that the performance of ct imaging is equivalent to , if not better than , autopsy in answering many forensic questions arising in the investigation of single - bullet gunshot wounds of the head . 
in fact , this type of forensic investigation relies not only on careful analysis of circumstantial evidence , examination of bullet fragments and chemical investigation of gunshot residues , but also on analysis and location of the bullets entrance and , if present , exit hole , description and location of the bullet and its fragments and of bone fragments and parenchymal lesions , as well as on spatial delineation of the bullets intracranial trajectory . 
 for almost a century , forensic literature has described how single - shot firearms produce injuries on the target body characterised by a bullet entrance hole , a bullet trajectory through the body and , if present , a bullet exit hole . 
in particular , differentiation between the bullet entrance and exit hole at the point of passage of the bullet through flat bone is based on the morphology both of the margins of the osseous wound and of the pattern of the fracture line [ 810 ]  . 
 when a bullet enters the skull bones , it determines a loss of substance , which appears conical or funnel shaped with bevelling of the bone surface in the direction of the exit wound . 
normally , the entrance wound has a punched out appearance , with the diameter measured on the outer table almost completely coinciding with that of the bullet ; then , in addition to the loss of substance caused directly by the bullet , there are often also small cracks or fractures radiating from the central hole . 
if the impact is oblique to the bone surface , this creates a larger wound on the outer table , on the side in which direction the bullet is travelling , conducibili al proiettile , sono stati riconosciuti anche in corrispondenza dei tessuti molli latero - cervicali . 
gli angoli di traiettoria nei tre piani dello spazio calcolati dai due esaminatori non hanno mostrato significative differenze dampiezza . il confronto con i dati autoptici non ha mostrato discrepanze nellidentificazione del numero dei fori della scatola cranica , n nella differenziazione del foro dentrata da quello duscita . 
limaging 3d - tc ha permesso di tracciare la traiettoria intracranica del proiettile in maniera simile allautopsia , ma si mostrato superiore nella definizione spaziale dei frammenti di proiettile e / o di osso e quindi pi accurato nel localizzare nei tre piani dello spazio la traiettoria intrasomatica . 
in un caso la tc ha permesso di individuare un tramite anche in corrispondenza dei tessuti muscolo - fasciali del collo e di definirne una traiettoria . discussione i risultati di questo studio dimostrano che le tecniche dimaging tc sono in grado di soddisfare con performances uguali o , in alcuni casi , superiori alla metodica autoptica tradizionale molti dei principali quesiti forensi in casi di ferite cranio - encefaliche darma da fuoco a carica singola . 
 in questo genere di investigazioni forensi , oltre allattenta analisi dei dati circostanziali allesame dei frammenti del proiettile ed allindagine chimica dei residui di sparo , fondamentale importanza rivestono infatti lo studio e lidentificazione del foro dingresso e quello duscita del proiettile , ove presente , la descrizione e la localizzazione del proiettile , dei suoi frammenti , di frammenti ossei e delle lesioni parenchimali la delineazione nello spazio della traiettoria intrasomatica del proiettile . 
 da quasi un secolo , la letteratura forense descrive come le lesioni da arma da fuoco a carica singola producano sullorganismo bersaglio delle ferite caratterizzate dal rilievo di un foro di entrata , di un tramite intrasomatico e , se obiettivabile , di un foro di uscita . 
in particolare la differenziazione del foro di entrata da quello di uscita segnatamente al passaggio di un proiettile attraverso le ossa piatte si basa sia sullo studio della morfologia dei margini della breccia ossea , sia sullandamento delle linee di frattura [ 810 ]  . 
 quando un proiettile attraversa le ossa craniche determina in queste una perdita di sostanza che assume forma conica , ad imbuto , con svasatura marginale aperta verso il lato di uscita del proiettile . 
qualora il proiettile fuoriesca , i radiol med ( 2012 ) 117 : 461470 relativi fori di entrata e di uscita assumono ampiezza diversa , con il primo di diametro inferiore al secondo . 
di norma il foro dentrata assume aspetto a stampo , con diametro misurato sulla teca esterna corrispondente quasi a quello del proiettile ; in aggiunta poi , alla perdita di sostanza causata direttamente dalla penetrazione del proiettile , si associano spesso piccole fissurazioni cos come vere e proprie fratture del cranio , a partenza dal foro centrale . 
il foro di uscita si presenta , invece , come una breccia di dimensioni pi ampie in relazione allazione contundente del proiettile che ha perso gran parte della sua forza viva . 
se limpatto avviene obliquamente sulla superficie ossea , si crea una lesione pi ampia sul tavolato esterno , in corrispondenza del lato verso cui il proiettile diretto fornendo ulteriori dati aggiuntivi sulla direzione della sua traiettoria [ 9 ]  . altro fondamentale aspetto riveste lo studio delle linee di frattura che si dipartono dai fori di passaggio del proiettile . 
 nel 1903 puppe [ 1113 ] ha introdotto il principio secondo il quale , in presenza di pi linee di frattura del cranio , possibile indicare la frattura che si prodotta per prima attraverso lo studio della loro intersecazione o convergenza verso un foro , nel caso di lesioni da arma da fuoco . 
generalmente , il tramite intrasomatico di un proiettile si ottiene congiungendo idealmente il foro dentrata con quello di uscita o in assenza di questo con il proiettile non fuoriuscito e proiettando nello spazio lasse direzionale cos ricavato . 
coerentemente con il teorema di puppe le linee di frattura pi corte e sottili che originano dal foro di uscita della vittima terminano nelle rime di frattura pi grossolane che originano dal foro dentrata posto nellemicranio controlaterale ( frecce lunghe )  . thus providing additional information on the course of the trajectory [ 9 ]  . 
in 1903 , puppe introduced the principle [ 1113 ] whereby when several fracture lines are present on the skull , it is possible to reconstruct the sequence of injuries by studying their intersection or , in the case of gunshot wounds , convergence towards the bullet hole . 
dal lato di uscita dalla scatola cranica il proiettile ha determinato una estesa perdita di sostanza comportando un fracasso osseo . entrance and exit hole or retained bullet if no exit hole is present and projecting the resulting directional axis into space . 
however , in some rare cases , the bullet may follow a nonlinear course within the skull and stop at sites totally unrelated to the original position as a result of the impact with bone or interposed tissues . 
in such cases , additional information about the direction of the trajectory can be derived by analysing the numerical and spatial distribution of sualizzazione dei frammenti di proiettile e di osso e nellanalisi del loro pattern di distribuzione , soprattutto con la finestra di visualizzazione adeguata alla densit dei metalli [ 14 , 15 ]  . 
stato gi dimostrato [ 16 ] come la possibilit di descrivere la precisa localizzazione spaziale dei vari frammenti , insieme ad opportuni calcoli fisici basati sul teorema della conservazione della quantit di moto possa essere di grande utilit nella delineazione del tramite intra - cranico , radiol med ( 2012 ) 117 : 461470 fig . 
in base allo studio della distribuzione dei frammenti ossei e di proiettile allinterno del parenchima cerebrale ( a , b ) la traiettoria intrasomatica del proiettile stata definita come diretta in senso antero - posteriore , da destra verso sinistra e dallalto in basso ( c )  . 
 several studies have confirmed the value of both 2d and 3d ct images for depicting bullet and bone fragments and helping to analyse their distribution pattern , above all when a ct viewing window adequate for the density of metal is used [ 14 , 15 ]  . 
it has already been demonstrated [ 16 ] that the possibility of describing the precise location of the various fragments , coupled with appropriate physical calculations based on the law of conservation of quantity of motion , can be very useful in outlining the intracranial trajectory , above all when the bullet is retained or fragmented . 
in addition , ct study , especially when performed shortly after death and with window settings suitable for brain tissue , enables definition of the bullets intraparenchymal course by visualising direct and indirect effects of its passage on intracranial structures . although postmortem investigation with magnetic resonance imaging [ 6 ] or contrast - enhanced ct [ 17 ] is the most accurate method for clearly depicting the areas of brain tissue involved by passage of the bullet , even unenhanced ct is able to provide adequate information by depicting intraparenchymal haemorrhage and bone or metal fragments surrounding the bullets intracranial course . a further component of trajectory assessment is the distribution of air bubbles that enter the skull along with the bullet . 
air bubble formation is due to the temporary cavity created by the transfer of energy from the bullet to the tissues surrounding the bullets intracranial course and which is normally larger in diameter than the definitive lesion ( permanent cavity ) [ 18 , 19 ]  . 
in aggiunta , lo studio tc , soprattutto se eseguito precocemente rispetto al decesso e con finestra di visualizzazione correttamente definita per la densit del tessuto nervoso cerebrale , consente di definire la traiettoria intraparenchimale del proiettile in base alla descrizione degli effetti diretti ed indiretti del passaggio dello stesso nelle strutture intracraniche . sebbene unindagine post - mortale con risonanza magnetica [ 6 ] o mediante tc con mezzo di contrasto [ 17 ] costituisca allo stato attuale la metodica pi accurata per descrivere con accuratezza le aree di tessuto cerebrale interessate dal passaggio del proiettile , anche la tc in condizioni di base in grado di fornire adeguate informazioni su di esse attraverso la documentazione di emorragie intraparenchimali , frammenti dosso e metallici lungo il percorso del proiettile nellencefalo . ulteriore componente di valutazione della traiettoria rappresentata dalla disposizione delle bolle daria penetrate con il proiettile nella scatola cranica . 
la formazione di queste dovuta alla cavit temporanea ( temporary cavity ) che si crea quando lenergia del proiettile trasmessa ai tessuti che circondano il tramite intrasomatico e che normalmente presenta diametro maggiore rispetto alla lesione definitiva ( permanent cavity ) [ 18 , 19 ]  . 
 nei casi di lesioni da arma da fuoco il tragitto del proiettile si distingue in extrasomatico , di pertinenza balistica , ed intrasomatico , di interesse squisitamente medico - legale . 
la traiettoria intrasomatica del proiettile tracciata nellimmagine ( c ) : essa presenta direzione antero - posteriore , da destra verso sinistra e dal basso verso lalto . bullet course is distinguished into an extrasomatic portion , of ballistic relevance , and an intrasomatic portion , of purely medicolegal relevance . 
however , thanks to the data mentioned above , ct volume reconstructions can also give indications as to the position of the victims head at the time of the gunshot and add information regarding the bullets extrasomatic course to support the circumstantial evidence [ 20 ]  . 
an example is the case shown in figure 5 in which the ct examination was performed on a corpse exhumed 10 years after the homicide : the bullet hit the victim in a craniocaudal direction entering through the parietal bone and exiting from the skull base , to then pass through the laterocervical muscle fascia . 
 this discrepancy could only be explained by hypothesising that the victims head at the time of the gunshot was rotated axially from right to left and tilted posteriorly and to the left , probably in a desperate gesture of self - defence . vra citati , possono fornire indicazioni relativamente alla posizione del capo della vittima al momento dello sparo e aggiungere informazioni sul percorso extrasomatico del proiettile a conferma dei dati circostanziali [ 20 ]  . 
il caso riportato in figura 5 , in cui lesame tc stato effettuato su cadavere riesumato a 10 anni dallomicidio : il proiettile ha attinto la vittima con direzione cranio - caudale entrando dallosso parietale e fuoriuscendo dalla base cranica , per dirigersi nei piani muscolo - fasciali laterocervicali ; da questi dati emersa una discrepanza tra la direzione della traiettoria intracranica del proiettile e la traiettoria prodottasi in corrispondenza dei tessuti molli del collo . 
tale incongruenza stata giustificata solo ipotizzando che il capo della vittima al momento dello sparo fosse ruotato sul piano assiale da destra verso sinistra e inclinato posteriormente e verso sinistra , in un probabile gesto di disperata autodifesa . conclusioni conclusions our limited experience with fatal cranioencephalic single bullet wounds has clearly highlighted the value of the use of ct imaging in these types of injury . 
ct and 3d reconstruction techniques should be considered extremely useful for identifying and differentiating the bullets entrance and , if present , exit holes , indicating the bullets intrasomatic course and , in some cases , suggesting hypotheses on the extrasomatic course to confirm circumstantial evidence . 
 in conclusion , in view of the noninvasiveness , rapidity and la nostra esperienza , seppur limitata , in caso di lesioni cranio - encefaliche mortali da arma da fuoco a carica singola , ha chiaramente messo in luce la validit dellimpiego di tali metodiche di imaging in questo tipo di lesivit . 
le tecniche tc e di ricostruzione volumetrica infatti devono essere ritenute estremamente utili ad identificare e differenziare il foro dentrata da quello duscita , se presente , ad indicare la traiettoria intracranica del proiettile , e , in alcuni casi , a fornire ipotesi su quella extrasomatica a conferma dei dati circostanziali . 
the bullet hit the victim in a cranial - caudal , slightly anteroposterior , direction entering through the parietal bone and exiting through the skull base , then passed through the laterocervical fascia . 
elgazzar springer - verlag berlin heidelberg , 2011 isbn 978 - 3 - 642 - 19425 - 2 e - isbn 978 - 3 - 642 - 19426 - 9 doi 10.1007 / 978 - 3 - 642 - 19426 - 9 published online : 14 may 2012 springer - verlag 2012 this 150 page text , plus 3 glossary pages are intended to give the student and professional clear , and very sound information about nuclear medicine . 
the topic is divided into 11 chapters , starting with basic considerations and ending with nuclear oncology and therapeutic applications in nuclear medicine . the authors main endeavour is to make the reader aware that nuclear medicine is an imaging modality that offers poor anatomic information in comparison with computed tomography ( ct ) or magnetic resonance imaging ( mri ) yet , on the contrary , it provides valuable and important results regarding physiologic , metabolic and molecular imaging , as well as body functions . taking into account that nuclear medicine with its reduced radiation burden , patient comfort , ease of performance , possible examination controls over time and continuous improvements in equipment and radiation tracers , it is strange how it is not , very often , the first diagnostic option offered to patients . the text is clearly written in primer style , enriched by useful images and a few tables . 
this concise book will be appreciated by all those who want an introduction to this fascinating field of up - to - date imaging modality and study of body functions . questo testo di 150 pagine pi 3 di glossario stato concepito per offrire allo studente ed al professionista chiare e ben solide informazioni sulla medicina nucleare . 
 intendimento principale dellautore di far s che il lettore si renda conto che la medicina nucleare una metodica per immagini che , rispetto alla tomografia assiale computerizzata ( tac ) ed alla risonanza magnetica ( rm ) , offre scarse informazioni anatomiche mentre , al contrario , in grado di fornire validi ed importanti contributi in merito allo studio per immagini fisiologiche , metaboliche e molecolari , nonch in merito alle funzioni corporee . 
 tenuto conto del fatto che la medicina nucleare offre un basso carico di radiazioni , comodit per il paziente , facilit di esecuzione , possibilit di controlli nel tempo , continui progressi delle attrezzature e dei traccianti radioattivi , strano come molto spesso non sia offerta come prima opzione diagnostica al paziente . il testo scritto in modo chiaro , stile bigino , arricchito da utili immagini e da qualche tabella : questo conciso volumetto verr apprezzato da tutti coloro che desiderano una introduzione a questa affascinante , moderna modalit di immagine e di studio delle funzioni corporee . 
seventeen patients ( 11 men and 6 women ; mean age 57.8 ; range 1781 ) with 17 bone lesions underwent biopsy with xperguide cbct ( philips medical system , best , the netherlands )  . 
 in 15 patients , a sample of adequate material for histopathological analysis to yield a definitive diagnosis was obtained ; in two patients , the sample was inadequate for a definitive diagnosis . 
in one of these two cases , the lesion was closely followed up for 1 year , during which it remained stable in size , and as a result , it was considered a false positive ; the other was considered a false negative . 
diciassette pazienti ( 11 maschi e 6 femmine ; et media 57 , 8 anni , range 1781 ) con 17 lesioni ossee sono stati sottoposti a biopsia percutanea con guida xperguide cbct . 
in 15 pazienti , stato ottenuto un campione di materiale adeguato per lesame isto - patologico e per giungere ad una diagnosi definitiva ; in 2 pazienti il campione risultato inadeguato per giungere ad una diagnosi . 
in uno dei 2 casi , la lesione stata seguita per un periodo di follow - up di 1 anno , durante il quale le sue dimensioni sono rimaste stabili ; pertanto questa stata considerata un falso positivo . 
la biopsia ossea sotto guida xperguide cbct pu essere considerata accurata grazie alla radiol med ( 2012 ) 117 : 13861397 1387 encouraging in terms of complication rate , diagnostic accuracy , sensitivity , specificity and reduction of ct workload . keywords percutaneous biopsy bone lesions xperguide cone - beam ct combinazione tra la possibilit di orientamento nello spazio real - time dellago e la risoluzione spaziale della fluoro - tomografia computerizzata ( tc )  . 
inoltre , i nostri risultati sono incoraggianti in termini di percentuale di complicanze , accuratezza diagnostica , sensibilit , specificit e non ultimo , riduzione del carico di lavoro del servizio tc . parole chiave biopsia percutanea lesioni ossee xperguide cone - beam ct introduction introduzione percutaneous bone biopsy is a vital step in the diagnosis of infectious and neoplastic musculoskeletal lesions . 
although open biopsy is considered the reference standard in achieving a tissue diagnosis , with a reported accuracy of 98% , it carries a risk of significant complications in up to 16% of cases , including haematoma , infection and spread of tumour cells [ 24 ]  . 
this is in contrast to percutaneous needle biopsy , which has a reported diagnostic accuracy ranging from 66% to 97% [ 1 , 2 , 5 ] and a low complication rate ( 1.1% ) [ 5 ]  . 
however , there are known drawbacks to conventional ct guidance : exposure to ionising radiation for patients and operators , the limitation of image orientation in the plane of needle insertion [ 6 ] and the lack of realtime viewing . 
the ct fluoroscopy system was developed to overcome the lack of real - time visualisation [ 7 ] , but there are several disadvantages : the significant exposure to ionising radiation for the operator ; the difficulty performing an interventional procedure within a small - size gantry ; the limited orientation of the imaging plane . 
it may therefore be difficult to choose an appropriate approach to the tissue have to be sampled . recently , a c - arm with a flat panel detector system was developed that consists of a cone - beam x - ray tube and a flat - panel detector integrated with a c - arm gantry : conebeam ct ( cbct ) ( philips medical system , best , the netherlands )  . 
this new system can be used to visualise the correct needle trajectory from the skin to the lesion under real - time fluoroscopic guidance and verify the exact location of the needle tip within the target lesion , thereby improving the diagnostic accuracy and la biopsia percutanea un passaggio essenziale nella diagnosi sia di infezioni che di lesioni neoplastiche dellosso . 
nonostante la biopsia a cielo aperto sia da considerarsi il gold standard per ottenere la diagnosi istologica , con un accuratezza riportata del 98% ; essa non del tutto scevra dal rischio di complicanze significative sino al 16% dei casi ; le complicanze comprendono : ematoma , infezione e disseminazione di cellule tumorali [ 24 ]  . 
differenti sono i dati della biopsia percutanea che ha unaccuratezza diagnostica variabile tra il 66% ed il 97% con un basso tasso di complicanze ( 1 , 1% ) [ 5 ]  . 
detto ci vi sono noti inconvenienti nellutilizzo della guida tc : lesposizione a radiazioni ionizzanti sia per il paziente che per loperatore , i limiti nella visualizzazione dellorientamento dellago nei diversi piani [ 6 ] e la mancanza di una visione in tempo reale . 
il sistema di fluoro - tc stato sviluppato nel tentativo di colmare limpossibilit di avere una visualizzazione in tempo reale [ 7 ] , ma nonostante ci vi sono ulteriori svantaggi : limportante esposizione alle radiazioni ionizzanti dell operatore , la difficolt di eseguire la procedura quando il gantry di piccole dimensioni e il limitato orientamento del piano di visualizzazione . 
pertanto pu essere difficile scegliere un approccio appropriato al tessuto su cui eseguire la biopsia . recentemente stato sviluppato un arco a c con un detettore flat panel ; esso consiste in un tubo radiogeno di tipo cone - beam con un detettore flat panel integrati con un gantry ad arco a c , cone - beam tc ( cbct ) ( philips medical system , best , paesi bassi )  . 
inoltre , il sistema cbct fornisce alloperatore sia un sistema di visua1388 radiol med ( 2012 ) 117 : 13861397 efficacy of percutaneous needle biopsies and enhancing the operators confidence during the procedure . 
furthermore , the previous limitations of ct fluoroscopy systems , such as a small gantry bore and limited gantry orientation , can easily be overcome with this cbct systeseveral studies have already demonstrated the usefulness of cbct systems during interventional procedures [ 811 ]  . 
the purpose of this study was to determine the diagnostic performance of cbct - guided percutaneous needle core biopsy in patients with bone lesions . materials and methods patients from may 2009 to september 2010 , 17 patients ( 11 men and six women ; mean age 57.8 ; range 1781 ) with 17 bone lesions underwent biopsy with xperguide cbct ( table 1 )  . 
all cases were discussed in a multidisciplinary meeting involving musculoskeletal interventional radiologists , orthopaedic surgeons , oncologists and pathologists , at which a decision was made to perform percutaneous bone biopsy in accordance with guidelines described by liu et al . 
questo nuovo sistema pu essere utilizzato al fine di visualizzare la corretta traiettoria dellago dalla cute sino allinterno della lesione , il tutto sotto guida fluoroscopica real - time ed inoltre consente di verificare la corretta posizione della punta dellago all interno della lesione con la modalit tc del sistema cbct ; ci migliora laccuratezza diagnostica e lefficacia delle biopsie percutanee ed aumenta la confidenza delloperatore durante la procedura . 
lo scopo di questo studio stato quello di determinare la performance diagnostica delle biopsie ossee percutanee eseguite con tale sistema . materiali e metodi pazienti da maggio 2009 a settembre 2010 , 17 pazienti ( 11 maschi e 6 femmine ; et media 57 , 8 anni , range 1781 anni ) con 17 lesioni ossee sono stati sottoposti a biopsia ossea percutanea con xperguide cbct ( tabella 1 )  . 
adequate antibiotic prophylaxis was used . baseline imaging pretreatment imaging consisted of an x - ray examination in five patients and a skeletal multidetector computed tomography ( mdct ) scan in all patients ( aquilion 64 , toshiba , tokyo , japan )  . 
each mdct scan was acquired with a thickness of 0.5 mm , voltage of 120 kv and tube current of 250 ma . equipment imaging guidance all procedures were performed with xperguide cbct ( philips medical system )  . 
the biopsy route was also discussed in order to avoid needle penetration and contamination of uninvolved muscle compartments , in accordance lo - scheletrica , chirurghi ortopedici , oncologi e patologi ; stata quindi presa la decisione di eseguire una biopsia ossea percutanea in accordo con le linee guida sulle biopsie delle lesioni ossee descritte da liu et al . 
nei casi in cui era in corso un trattamento anticoagulante e / o antiaggregante , questo stato sospeso 7 giorni prima della procedura e , quando necessario , stato sostituito con la somministrazione di eparina frazionata . 
una adeguata profilassi antibiotica stata effettuata in tutti i casi . imaging di base le indagini radiologiche eseguite prima della procedura sono state un rx in 5 pazienti ed una tc multistrato dei segmenti ossei coinvolti ( tcms ) in tutti i pazienti ( aquilion 64 , toshiba , tokio , giappone )  . 
ogni acquisizione tcms stata ottenuta con uno spessore di slice di 0 , 5 mm , 120 kv di voltaggio e 250 ma di amperaggio . 1390 radiol med ( 2012 ) 117 : 13861397 fig . 
2 limmagine mostra il tragitto dellago dal punto di ingresso cutaneo ( in viola ) al punto target ( in verde )  . with the biopsy guidelines for limb - sparing surgery of the extremities [ 12 ]  . equipaggiamento guida imaging biopsy equipment the biopsy needle system to be used was selected on the basis of lesion characteristics . 
 xperguide cbct examination was performed with a single - plane c - arm angiography system equipped with a flat - panel detector ( allura xper fd20 , philips healthcare )  . 
this system is equipped with software for the following three beam ct modes : 3d rotational antutte le procedure sono state eseguite con xperguide cbct ( philips medical system , best , paesi bassi )  . 
il tragitto dellago stato pianificato al fine di non attraversare o contaminare compartimenti muscolari sani , in accordo con le linee guida suddette , biopsy guidelines for limb - sparing surgery of the extremities [ 12 ]  . strumentazione per la biopsia il sistema di prelievo utilizzato per la biopsia stato scelto in relazione alle caratteristiche della lesione . 
nelle lesioni totalmente sclerotiche , in quelle con margine sclerotico o ancora in quelle con una componente extraossea molto sottile ( < 1 cm ) la biopsia stata eseguita con un sistema coassiale costituito da un ago da vertebroplastica 13 g ( optimed medizinische instrumente gmbh , ettlingen , germania ) attraverso il quale veniva introdotto un ago 16 g ( cook inc europe , bjaeverskov , danimarca )  . 
3a , b dopo il posizionamento dellago , una scansione cbct conferma lesatto posizionamento dellago allinterno della lesione ; visione assiale ( a ) e visione coronale ( b )  . giography ; xperct ( philips healthcare ) low definition , low dose ; xperct high definition , high dose . 
the differences were as follows : 3d rotational angiography , 120 projections , 4.1 - s scanning time ; xperct low definition , 300 projections , 10 - s scan time ; no - plano ad arco a c con sistema flat - panel ( allura xper fd20 , philips medical system , best , paesi bassi )  . 
il detettore ha un campo di vista di 3830 cm2 ed una matrice di 24801920 pixels ed un pixel pitch di 154 questo sistema dotato di un software con le seguenti 3 modalit beam tc : angiografia rotazionale 3d , xperct ( philips healthcare ) a bassa definizione ed a bassa dose ed infine xperct ad alta definizione e ad alta dose . 
le differenze sono le seguenti : angiografia rotazionale 3d , 120 proiezioni , tempo di acquisizione di 4 , 1 secondi ; xperct a bassa definizione , 300 proiezioni , tempo di acquisizione di 10 secondi ; xperct ad alta definizione , 600 proiezioni , tempo di acquisizione di 20 secondi . 
le acquisizioni cbct sono state ottenute in modalit rotazionale con i seguenti parametri : distanza sorgente - detettore 1200 mm ; distanza sorgente - asse rotazionale 810 mm ; distanza detettore - asse rotazionale 390 mm ; velocit di rotazione 55 / secondo ; durata della rotazione 4 , 1 secondi ; range totale di traiettoria dellarco 240 ; numero di proiezioni 120 ; misura della matrice 10241024 e controllo automatico dellesposizione . 
sono evidenziabili piccole bolle aeree nel contesto della lesione . 1392 radiol med ( 2012 ) 117 : 13861397 xperct high definition , 600 projections , 20 - s scan time . 
cbct acquisition data were acquired in the propeller mode with the following parameters : sourcedetector distance 1 , 200 mm ; sourcerotation axis distance 810 mm ; detectorrotation axis distance 390 mm ; rotation speed 55s ; rotation duration 4.1 s ; total arc trajectory range 240 ; number of projections 120 ; matrix size 1 , 0241 , 024 pixels ; automatic exposure control . 
 acquisition frames were transferred via an optical link in real time to the 3d rotational angiography workstation ( allura release 6.2 , philips healthcare ; precision 670 , dell )  . xperguide cbct bone biopsy technique the patient was placed either supine or prone depending on lesion location . 
subsequently , the systems xperguide functionality , needle planning and navigation software tool , which creates an overlay of live fluoroscopy and 3d soft - tissue images ( philips xperct ) , was used in the next phases of the procedure . 
first , the 3d volume reconstructed from the xperct images was used to plan the needle trajectory from the skin entry point to the centre of the lesion ( target location )  . 
the software also calculates the position of the x - ray tube to view the entry point of the needle on the skmoreover , it is used to automatically move the gantry and precisely align the needle to the determined path . 
the determined path was projected onto real - time fluoroscopy images together with an overlay of the xperct images to allow exact needle placement on the patients skin and constant monitoring and adjustments during needle progression . 
progression of the needle into the patient was followed in real time under fluoroscopic guidance after selecting the progression view , which rotates the gantry 90 perpendicularly to the trajectory . 
the number of needle passes depended on the subjective quality of the material obtained as assessed by visual inspection and typically ranged from two to four passes , as reported by wu et al . 
nelle diverse fasi della procedura , per la pianificazione del tragitto dellago sono state utilizzate la modalit xperguide ed il software di navigazione ; questultimo crea una sovrapposizione della fluoroscopia real time e delle immagini 3d preacquisite dei tessuti molli ( philips xperct )  . 
il tragitto determinato viene proiettato in fluoroscopia in tempo reale sovrapponendo le immagini xperct , cos da permettere lesatto posizionamento dellago sulla superficie cutanea del paziente , ed il suo continuo monitoraggio durante la progressione . 
la progressione dellago allinterno del paziente direttamente visualizzato in fluoroscopia dopo aver selezionato la finestra di avanzamento ago , la quale determina una rotazione del gantry di 90 perpendicolarmente alla traiettoria . 
il numero dei passaggi dellago dipende dalla qualit soggettiva delloperatore all ispezione visiva del materiale ottenuto , tipicamente esso varia dai 2 a 4 passaggi in accordo con quanto descritto da wu et al . 
ogni biopsia stata classificata come adeguata o inadeguata sulle base del risultato istopatologico ; adeguata quando stato ottenuto un campione di materiale sufficiente per lanalisi istopatologica , in modo da ottenere una diagnosi definitiva di lesione maligna o benigna . 
each biopsy was classified as adequate or inadequate on the basis of the histopathological report : adequate when a sample of sufficient material was obtained for histopathological analysis to yield a definitive diagnosis of a benign or malignant lesion ; inadequate when the sample was insufficient to yield a definitive diagnosis . the needle core biopsy results were correlated with histopathological diagnosis of surgical specimens in patients who underwent curettage or resection of the benign or malignant lesion . 
moreover , a lesion characterised by pathological examination revealing nonspecific findings was designated as benign when follow - up images ( for a period of 1 year at least ) showed stability or decrease in size . 
therefore , accuracy was determined on histological diagnosis on the tissue core , possibly confirmed by surgical histology , and for cases with nonspecific histological findings , with a follow - up of 1 year at least . 
 complications were classified as major or minor in accordance with the classification system of the society of interventional radiology [ 14 ]  . results a technical success of 100% was obtained , which means that correct positioning of the needle within the lesion was possible in all cases . 
 among biopsies designated as adequate , ten were malignant ( four metastasis and six primary bone tumours ) , and six were benign according to clinical , histopathological and imaging follow - up . 
diagnostic accuracy , sensitivity and specificity were 94.12% ( 16 / 17 ) , 90.91% ( 10 / 11 ) and 100% ( 6 / 6 ) , respectively . no major complications were recorded . 
quindi laccuratezza diagnostica stata determinata sulle basi del risultato dellesame istologico sul frustolo bioptico , eventualmente confermata dallesame istologico sul reperto chirurgico e per i casi con esame istologico non specifico con stabilit al follow - up per almeno un anno . 
i casi con biopsia non diagnostica o con un follow - up di durata inferiore ad un anno sono stati considerati come possibili maligni e conseguentemente definiti come falsi negativi . 
le complicanze sono state classificate come maggiori o minori in accordo con il sistema di classificazione della societ di radiologia interventistica [ 14 ]  . risultati il successo tecnico stato del 100% , il che significa che in tutti i casi stato possibile posizionare correttamente lago allinterno della lesione . 
in uno di questi due casi , il follow - up ad un anno ha dimostrato una stabilit dimensionale della lesione e pertanto questa lesione stata inclusa nel gruppo dei falsi positivi ( tabella 2 )  . 
 tra le biopsie definite come adeguate 10 erano lesioni maligne ( 4 metastasi e 6 tumori ossei primitivi ) e 6 erano lesioni benigne in accordo con la clinica , i risultati istopatologici ed il follow - up allimaging . 
laccuratezza diagnostica , la sensibilit e la specificit sono state del 94 , 12% ( 16 / 17 ) , 90 , 91% ( 10 / 11 ) e 100% ( 6 / 6 ) rispettivamente . non stata osservata nessuna complicanza maggiore ; solo in un caso ( in una lesione dellosso iliaco ) stato registrato un modico sanguinamento con successivo ematoma che si risolto in circa 15 giorni . 
recentemente la risonanza magnetica stata identificata come tecnica di imaging per lesecuzione di biopsie di lesioni difficilmente visualizzabili con le altre metodiche , in adiacenza a strutture critiche [ 17 ]  . radiol med ( 2012 ) 117 : 13861397 1395 have become the standard imaging methods used to guide musculoskeletal needle biopsies , yielding excellent results [ 15 ]  . 
recently , mri has been described as a technique for percutaneous musculoskeletal biopsies in lesions that might otherwise be difficult to visualise using other techniques or lesions adjacent to critical structures [ 17 ]  . 
 [ 20 ] reported an accuracy rate of 81% for bone lesions sampled with ct guidance . the literature contains few reports about the use of ct fluoroscopy during interventional radiological procedures . 
subsequently , others authors [ 18 ] hypothesised and / or described the application of ct fluoroscopy guidance for radiological interventional procedures , such as hepatic radiofrequency [ 19 ] , managing spinal pain [ 22 ] , during bone tumour surgery in a series of five patients [ 23 ] and in a case of plasma - mediated radiofrequency ablation followed by percutaneous cementoplasty [ 24 ]  . the use of xperguide cbct during interventional radiological procedures was described by our group [ 10 ] during microwave ablation of lung lesions and by some other authors in a few other procedures , such as vertebroplasty or needle biopsy positioning [ 8 , 9 ]  . 
xperguide cbct may be considered an alternative to reduce the workload of ct , to obtain an accurate approach of the coaxial introducer and technically successful sampling , resulting in high diagnostic accuracy . 
the 3d imaging data sets attained with cbct can also provide an advantage over the other methods , as they can be easily manipulated to allow multiplanar reconstruction through any part of the imaged object and demonstrate the trajectory angle of the approach with high spatial resolution . 
this approach also provides accurate information enabling modification of the angle and distance of the coaxial introducers approach during the procedure , resulting in a higher technical success rate and diagnostic accuracy . 
 [ 13 ] hanno riportato unaccuratezza diagnostica migliore nelle lesioni litiche rispetto alle lesioni sclerotiche , in quelle pi voluminose ed in quelle in cui si sono ottenuti frustoli di dimensioni maggiori . 
 [ 20 ] hanno dimostrato che laccuratezza diagnostica delle biopsie ossee percutanee sotto guida tc dell81% . in letteratura ci sono pochi lavori riguardo luso della fluoro - tc nelle procedure di radiologia interventistica . 
successivamente altri autori [ 18 ] hanno descritto luso della fluoro - tc in procedure di radiologia interventistica quali la radiofrequenza epatica [ 19 ] , il controllo del dolore spinale [ 22 ] , durante procedure chirurgiche di tumori ossei in un esperienza di 5 pazienti [ 23 ] e durante unablazione con radiofrequenza plasma - mediata seguita da cementoplastica percutanea in un case - report [ 24 ]  . luso dellxperguide cbct durante le procedure di radiologia interventistica stato descritto dal nostro gruppo [ 10 ] durante lablazione con microonde di lesioni polmonari e da alcuni altri autori in poche procedure come la vertebroplastica o il posizionamento dellago durante biopsia [ 8 , 9 ]  . 
 [ 11 ] hanno descritto la loro iniziale esperienza nellesecuzione di biopsie trans - toraciche di noduli polmonari utilizzando il sistema c - arm cbct . secondo le nostre conoscenze , questo il primo studio che valuta laccuratezza dellxperguide cbct durante le biopsie ossee . 
lxperguide cbct pu essere considerata una valida alternativa al fine di ridurre il carico di lavoro della tc , per ottenere un adeguato utilizzo del sistema coassiale e per ottenere prelievi bioptici validi cos da garantire una elevata accuratezza diagnostica . 
il sistema di imaging 3d ottenuto con le immagini cbct presenta un ulteriore vantaggio rispetto alle altre metodiche : le ricostruzioni multiplanari permettono di individuare la traiettoria dellago , con tutte le angolature possibili , ottenendo una elevata risoluzione spaziale . 
questo sistema permette , inoltre , modificazioni della traiettoria dellago e / o di tutto il sistema coassiale , durante la procedura stessa , garantendo un pi alto successo tecnico ed un elevata accuratezza diagnostica . 
inoltre gli operatori in tc devono manovrare lago direttamente con le mani o comunque con un porta aghi allinterno del gantry , con una conseguente elevata esposizione radiante delle mani dello1396 radiol med ( 2012 ) 117 : 13861397 tors must handle the needle manually or with the aid of a needle holder device within the limited ct gantry , resulting in considerable radiation exposure to the operators hand and unavoidable discomfort during the performance of the procedure . 
although the factors associated with an inadequate biopsy are probably not dependent on the size and number of the tissue cores , the number of procedures was too low to draw conclusions . 
we are planning a comparative study with a prospective randomised design that might be able to provide a definitive answer on which imaging guidance system is the best for the biopsy of bone lesions . 
as previously mentioned , the possibility of performing biopsies in the angiographic suite using the xperguide cbct is an important advantage in terms of reducing the workload of the ct service . peratore ed un inevitabile discomfort durante lesecuzione della procedura . 
i fattori associati con biopsia inadeguata probabilmente non dipendono dal numero e dalle dimensioni del frustolo ; il numero delle procedure per troppo basso per estrapolare delle conclusioni al riguardo . 
stiamo pianificando uno studio comparativo randomizzato prospettico che potrebbe darci una risposta definitiva su quale tecnica per immagini sia la migliore da usare come guida per le biopsie di lesioni ossee . 
quando si combinano labvs , lecografia convenzionale e la mammografia , laccuratezza diagnostica , la sensibilit e la specificit raggiungono il 96 , 4% , il 97 , 1% e il 95 , 2% , rispettivamente . 
esso ha 1288 radiol med ( 2012 ) 117 : 12871293 una sensibilit significativamente maggiore della mammografia , ma simile allecografia convenzionale e non pu essere preferibile ad un esame ecografico convenzionale . 
 parole chiave ecografia 3d lesioni mammarie bi - rads mammografia ricostruzioni multiplanari introduction in manual ultrasound ( us ) , a breast lesion has to be immediately characterised during the examination . 
by using 3d us , complex growth patterns and their margins can be better appreciated in three orthogonal planes in both benign and malignant tumours . automated breast volume scanning ( abvs ) a 3d function performed with an acuson s2000 ultrasound system and abvs attachment . 
 few studies have assessed the application of abvs to the diagnosis of breast lesions [ 6 , 7 ] , and the main purpose of these studies was to compare abvs with manual us . 
 the aim of this study was to compare the diagnostic efficiency of abvs with those of manual us and mammography in the differentiation of benign from malignant solid breast masses , with histopathologic examination as the reference standard . patients and methods from may 2010 to august 2010 , mammography , manual us and abvs were performed in 155 consecutive patients ( total 165 lesions ) scheduled to undergo us - guided core needle biopsy due to suspicious breast lesions detected during screening mammography or manual us . 
all lesions were confirmed with pathology after surgical excision ( n = 112 ) or with us - guided percutaneous core needle biopsy ( n = 53 ) within 48 h of us examination . 
surgical excision was performed in 92 lesions because of suspicious or malignant findings at a previous percutaneous core needle biopsy ( n = 76 ) and referring clinician preference on clinical grounds ( n = 16 )  . 
 mammography and manual ultrasound mammograms were taken with a senograph 2000 ( ge healthcare , waukesha , wi , usa ) in craniocaudal ( 27 kv , 85 mas , mo / mo ) and mediolateraloblique views ( 27 kv , 58 mas , mo / mo )  . 
breast density was according to birads categories and / or quantification : acr 1 , almost entirely fat ( low density , up to 25% mammary gland parenchyma ) ; acr 2 , scattered fibroglandular densities ( average density , 2650% gland parenchyma ) ; acr 3 , heterogeneously dense ( high density , 5175% gland parenchyma ) ; acr 4 , extremely dense ( very high density , > 75% gland parenchyma ) [ 10 ]  . 
 a manual us examination was performed with an acuson s2000 us system ( acuson , mountain view , ca , usa ) with a 14l - 5 linear - array probe , and iu22 us system ( philips medical systems , andover , ma < usa ) with a l12 - 5 linear - array probe by one radiologist ( zlw ) with 10 years of experience in breast us . 
with the patient supine , radiol med ( 2012 ) 117 : 12871293 1289 suspect regions were imaged in two perpendicular scanning planes ( sagittal and transverse ) , and data imaging and communications in medicine ( dicom ) images were stored on hard disks . 
after completing the reading session and receiving histopathological results , diagnostic accuracy , sensitivity , specificity and positive ( ppv ) and negative ( npv ) predictive values were calculated for each method . 
the system automatically adjusts depth , frequency , focal zone placement and overall gain . a typical examination comprises three automated 65 - s scans of each breast in the anteroposterior ( ap ) and both oblique positions . 
after the acquisition is finished , proprietary postprocessing algorithms are applied based on nipple location to maximise diagnostic information quality . after acquisition , the transverse image series is automatically sent from the acuson s2000 abvs to a dedicated breast us review workstation that presents images through multiplanar reconstruction ( mpr ) and reconstructs secondary images from the acquisition volume in any plane , such as sagittal , coronal , radial and antiradial views . 
figure 1 shows an example of the three multiplanar compounded reconstructions from abvs in comparison with the mammogra data evaluation the acquired dicom data were analysed offline at a separate workstation and evaluated by two radiologists ( lg , xn ) with 5 and 6 years , respectively in mammography . 
lesion detection rates of manual us , abvs and mammography were 95.8% ( 158 / 165 ) , 97.6% ( 161 / 165 ) and 87.8% ( 145 / 165 ) , respectively . 
 1290 radiol med ( 2012 ) 117 : 12871293 fig.1a - d three multiplanar compounded reconstructions from abvs in comparison with the mammograac three orthogonal planes ( transverse , sagittal , coronal ) of the left breast from abvs . 
c , d due esempi di fibroadenomi che presentano margini ben definiti , senza segni di infiltrazione del tessuto mammario circostante . was the same or better than manual us in terms of accuracy , sensitivity , specificity , ppv and npv . 
 value of coronal plane in 3d ultrasound as the coronal plane is unique to the 3d technique and not available for conventional manual us , it is important to emphasise the role of the coronal plane in the diagnosis . 
all eight malignant lesions missed by mammography occurred in higher - density breast tissue , and all were detected by us 1292 radiol med ( 2012 ) 117 : 12871293 and abvs . 
furthermore , three cases missed by us were found by abvs , which illustrates a key advantage of an automated us system for standardised , reproducible and bilateral whole - breast imaging . 
in our study , both us and abvs had much better diagnostic sensitivity for solid breast lesions than did mammography , which demonstrates an important role of us in lesion detection [ 14 ]  . 
in particular , abvs could provide a coronal - plane image , which does not have sound attenuation and thus allows better observation of lesion margabvs may also avoid investigator - dependent and nonstandardised documentation . 
 us findings used to characterise a solid breast mass include shape , orientation , margin , echogenicity , echotexture , posterior acoustic transmission , boundary echo and presence of calcifications [ 16 ]  . 
some studies previously assessed the value of the criteria in discriminating between benign and malignant masses and concluded that margin characteristics are associated with the highest diagnostic value [ 15 , 17 ] : 3d us can be used to evaluate these features more completely in focal breast lesion classification . 
the main limitation of this study is that benign lesions confirmed by pathology should receive a long - term follow - up to confirm stability . in summary , abvs is a promising diagnostic adjunct to mammography , and the retraction phenomenon in the coronal plane of 3d us has high diagnostic capability to differentiate between benign and malignant breast lesions . 
bazzocchi5 , 6 1department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 2department of radiology , scientific institute casa sollievo della sofferenza hospital , viale cappuccini 1 , 71013 san giovanni rotondo ( fg ) , italy 3university of crete , faculty of medicine , department of medical physics , p.o. 
box 1352 , 71110 heraklion , crete , greece 5imaging division , clinical department of radiological and histocytopathological sciences , university of bologna , santorsola , malpighi hospital , via g . 
pinto 1 , 71100 foggia , italy , tel . : + 390881 - 733866 , fax : + 39 - 0881 - 350368 , e - mail : g.guglielmi@unifg.it received : 12 july 2012 / accepted : 24 july 2012 / published online : 22 october 2012 springer - verlag 2012 abstract recent advances in the densitometric and imaging techniques involved in the management of osteoporosis are associated with increasing accuracy and precision as well as with higher exposure to ionising radiation . 
the development of effective and efficient qa programmes is mandatory to guarantee optimal image quality while reducing radiation exposure levels to the alara principle ( as low as reasonably achievable )  . 
lo sviluppo di programmi di qa efficaci ed efficienti necessario al fine di garantire una qualit dellimmagine ottimale e al contempo di ridurre i livelli di esposizione alle radiazioni secondo il principio alara ( cio al livello pi basso ragionevolmente ottenibile )  . 
this disease is widely recognised as an important public health problem because of the significant morbidity , mortality and economic and social costs 1348 radiol med ( 2012 ) 117 : 13471354 associated with its complications , i.e. , fractures at different skeletal sites [ 2 ]  . 
fractures tend to occur in those bone parts , such as the vertebral body , hip and wrist , which rely heavily on trabecular bone for their strength [ 3 , 4 ]  . 
it is estimated that every year 9 million osteoporotic fractures affect the worldwide population , and more than half of these occur in europe and in the americas [ 5 , 6 ]  . 
 osteoporotic fractures cost 36 billion euro in europe and 18 billion dollars in the us every year , and these are expected to increase twofold or more by 2050 unless treatments are pursued that have a significant impact on the global burden of fractures [ 7 , 8 ]  . quality assurance ( qa ) is by definition a programme for the systematic monitoring and evaluation of the various aspects of a service or facility to ensure that standards of quality are being met . 
qa in bone densitometry and associated methods is composed of those actions aiming to ( 1 ) maintain adequate equipment performance with the lowest possible radiation dose to patients consistent with clinical imaging requirements and ( 2 ) assure that adequate diagnostic information is provided at the lowest possible cost . 
dual - energy x - ray absorptiometry ( dxa ) is currently the most widely used method for the measurement of areal bone mineral density ( bmda ) ( g / cm2 )  . 
peripheral qct ( pqct ) , and high - resolution pqct ( hr pqct ) are ct - based techniques dedicated to the study of appendicular sites of the skeleton , with the aim of analysing both density and microarchitectural bone properties . 
vertebral fractures are usually diagnosed on spine radiographs or images of the spine acquired by dxa devices . the use of diagnostic imaging methods for the assessment of bone status has constantly and quickly increased , so that qa in bone densitometry deserves special attention [ 9 ]  . 
the purpose of this review article is to summarise the current practice of qa in bone densitometry and related techniques and to discuss the magnitude of radiation exposure from the x - ray methods used for the assessment of bone status . equipment and installation the technical features of bone densitometry and other related medical devices should satisfy clinical requirements . 
equipment packages should include not only the specific application software package but also dedicated phantoms for calibration and quality control procedures . the installation of the equipment should be followed by procedures that ensure proper functioning , satisfy all current radiation protection requirements and manufacturer specifications . 
electrical safety tests , equipment tests and staff training should be provided by the supplier of the equipment ; the employer should verify if equipment tests and staff training have been performed on the newly installed equipment [ 9 ]  . quality control an important issue in the study of bone status is the establishment of sufficient qc procedures , performed to ensure that a manufactured product meets a defined and standardised set of quality criteria . 
these procedures include monitoring of the stability and performance of the devices as well as guidelines for the handling of error sources in order to guarantee reliable quantitative information to clinicians and patients as an aid to diagnosis and management of osteo porosis . dual - energy x - ray absorptiometry dxa has a relevant and central role in the evaluation of individuals at risk of osteoporosis , in helping clinicians to assess fracture risk and in patients with osteoporosis to select pharmacological therapy and to monitor treatment or disease progression [ 10 ]  . 
this is influenced by several parameters , such as skill and training of the technician performing the scan , the site of measurement and the clinical features of patients [ 9 ]  . radiol med ( 2012 ) 117 : 13471354 1349 to determine the accuracy of a dxa densitometer , a phantom containing tissue - mimicking materials of known and different densities is scanned to ensure that measured values are truly assessed for all quantities under investigation [ 11 ]  . 
 thus , every facility should determine in vivo reproducibility for each dxa device [ 13 , 14 ]  . it is well known that dxa devices developed by different manufacturers and even by the same manufacturer provide different bmd results when used to measure the same skeletal site of a patient because of differences in scanner design , data acquisition , algorithms and method of calibration . 
although sbmd values can reduce the differences between measurements performed by systems developed by different manufacturers to less than 6% , the use of different dxa systems to longitudinally monitor the bone status of an individual is not recommended . quantitative ct precision is better for 3d multidetector qct than for singleslice 2d qct [ 17 ]  . qct is based on analysis of the trabecular bone compartment in the spine or proximal femur . 
most calibration approaches consist of a calcium hydroxyapatite - based bone mineral reference phantom that is scanned with the patient and placed underneath the lumbar spine or between the hips . 
the image analysis ( columbia , ky , usa ) standard consists of rods with varying concentrations of calcium hydroxyapatite mixed in a water - equivalent solid resin matrix [ 18 ]  . 
another approach , phantomless calibration , uses histograms of hu values placed in regions of subcutaneous fat and skeletal muscle , assuming fixed properties for each tissue types to determine a hu calibration [ 17 ]  . 
qus measurements are affected by precision errors due to patient positioning , coupling between the transducer and the skin of the patients , and the effect of soft tissue properties . 
a phantom should emulate the in vivo measurement as much as possible in terms of geometry and acoustic properties . the differences in measurements between available qus equipment are greater than those between dxa devices ; this is due to the different transducers and frequency ranges [ 21 ]  . the qa of ct systems is recognised as an important topic and scientific and professional organisations have developed guidelines for equipment specifications , equipment qc tests and radiation safety [ 17 ]  . 
radiation safety in ct is emphasised because patient radiation doses from ct are considerably higher than those from dxa . the measurement of precision is influenced by the ct scanner model , qct method , skill of the radiological technologist , patient positioning and movement . 
 radiation dosimetry a bone densitometry qa programme should involve periodic checks and measurements to maintain diagnostic image quality at the lowest possible radiation exposure . quantities and units the two most frequently used radiation quantities in diagnostic radiology are absorbed dose ( ad ) and effective dose ( ed )  . 
the ad , expressed in grays ( gy ) , is a measure of the energy per unit of mass deposited in the tissue and organs of the exposed body . 
the ed , expressed in sieverts 1350 radiol med ( 2012 ) 117 : 13471354 ( sv ) , is calculated using organ or tissue absorbed doses and the relative radiosensitivity assigned to each of these organs or tissues , defined by the international commission on radiological protection ( icrp ) [ 22 ]  . 
 the ed was introduced to allow comparison of the risk estimates from different sources of ionising radiation , for example from dxa and qct , or from imaging techniques and natural background radiation . 
the annual worldwide average ed from natural background radiation is 2.4 msv [ 9 ]  . dosimetric quantities used in ct are the ct dose index ( ctdi ) and the dose - length product ( dlp ) [ 9 ]  . 
ctdi measurements are performed at the periphery and at the centre of cylindrical phantoms representing the human head and body by using a pencil ionisation chamber with a length of 100 mfrom these measurements , a weighted ctdi ( ctdiw ) representing the average dose to a single slice is obtained . 
moreover , ctdi volume ( ctdiv ) has been introduced to take into account the effect of pitch on radiation dose , for imaging performed in the spiral mode , which is defined as ctdiw divided by pitch . 
 broad estimates of effective dose e can be derived from dlp values using conversion coefficients : e = dlpk where k is body regionspecific normalised ed factors ( msv * mgy1 * cm1 ) [ 23 ]  . patient exposure children and adult doses from dxa have been reported in several studies [ 24 - 28 ]  . 
the increased field size of fan - beam scanners ( linear - array detector ) and more recently of cone beam densitometers ( bi - dimensional detector ) , compared to pencil beam devices , has resulted in shorter scan times allowing greater patient compliance and better image quality . 
however , patient doses associated with state - of - the - art dxa scanners have also been increased [ 29 ]  . patient doses from pencil - beam dxa is 1 sv or less . 
patient doses up to 15 sv and 10 sv for spine and hip scans , respectively , have been reported for fan - beam dxa examinations performed on adult patients [ 26 ]  . 
specifically , paediatric patients will receive about two to three times higher ed than adults due to ( a ) the larger field size and ( b ) higher dose to internal organs because of less attenuation of x - rays by overlying tissue [ 26 ]  . 
when a patient is found to be pregnant after having undergone a dxa examination , communication with the woman is very important to give her an assessment of conceptus dose . 
published research shows that conceptus doses and potential radiogenic risks from dxa are negligible and , therefore , abortion due to radiation exposure is not recommended [ 22 , 32 ]  . 
an examination acquired at 80 kvp tube potential and 125 mas tube load delivers a radiation dose to a patient from 60 to approximately 300 sv , depending on protocol parameters and ct scanner model [ 25 , 33 ]  . 
on the other hand , qct of the appendicular skeleton , is associated with low patient ed ( lower than 10 sv ) [ 34 ]  . the analysis of mdct high resolution ( hr ) images provides important information about the trabecular bone network [ 36 , 37 ]  . 
however , patient doses associated with hrct ( with isotropic spatial resolution , submillimetre range ) are high , reaching about 3 msv [ 38 ]  . several factors play a role in the reduction of radiation dose to the patient . 
the use of adaptive section collimation , available in new - generation mdct scanners , allows reduction of exposure due to z - over scanning associated with helical scanning [ 39 ]  . 
nevertheless , studies are still needed to maximise the diagnostic information provided by the new technologies with the lowest radiation dose to the 1352 radiol med ( 2012 ) 117 : 13471354 patient . 
however , more accurate calculation of patient ed is possible using patient - specific monte carlo software packages for ct dosimetry [ 42 ]  . peripheral qct ( pqct ) scanners are dedicated units capable of assessing bone architecture and bmd at appendicular bones . 
the ed from pqct examinations is on the order of few sv [ 34 , 43 ]  . occupational radiation doses and shielding the scan type and mode , the workload and the relative position of the workstation to the scanning table are factors influencing exposure to the operator . 
the ministry of health service in british columbia has found that the exposure per 1000 scans to the bone densitometry operator was 56.0 mr for hologic qdr4500w , 7.0 mr for norland eclipse xe and 21.0 mr for ge prodigy lunar [ 44 ]  . 
the need for shielding mainly depends on patient workload , the size of the examination room , and the type of dxa scanner ( especially for fan - beam technology )  . 
when planning a bone densitometry facility , however , several parameters should be taken into account so that the exposure in adjoining areas is at a level acceptable for members of the public . 
moreover all resulting test results should be recorded and periodically reviewed to detect needed changes [ 9 ]  . education and staff training the performance of a bone densitometry facility is greatly influenced by the education and training of the staff delivering the services . 
they should also be acquainted with the application of all radiological techniques employed for the diagnosis of osteoporosis and familiar with the bone densitometry diagnostic activity [ 45 ]  . 
valutare prospettivamente se la presenza alla tomografia computerizzata multidetettore ( tcmd ) di calcoli pancreatici con pattern a bulls eye si correli alla pancreatite associata a mutazione genetica ( gmap ) e se vi siano altre caratteristiche tcmd suggestive nei pazienti affetti da gmap . 
il pattern a bulls eye stato rilevato in 10 / 15 pazienti ( 67% ) con gmap e in 4 / 32 ( 12% ) pazienti con pancreatite cronica non associata a mutazione genetica ( ngmap : p0 , 0001 )  . 
anche calcoli duttali con diametro 15 mm sono un segno correlato alle gmap . parole chiave pancreatite cronica mutazioni genetiche calcoli pancreatici tomografia computerizzata multidetettore pattern a bulls eye 1276 introduction chronic pancreatitis is an inflammatory disease of the pancreas characterised by destruction of the pancreatic parenchyma , fibrosis and dilatation of the main pancreatic duct , often associated with calcified duct stones [ 15 ]  . 
 several gene mutations associated with chronic pancreatitis have been identified [ 620 ] , the most frequent involving the cftr ( cystic fibrosis transmembrane regulator ) gene [ 7 , 8 , 12 , 14 ] , the spink1 ( serine protease inhibitor , kazal type 1 ) gene [ 9 , 11 , 13 , 17 , 20 ] and the prss1 ( cationic trypsinogen ) gene [ 6 , 10 , 1619 ]  . 
according to some authors [ 2 , 21 , 22 ] patients with pancreatitis associated with one of these gene mutations show onset at a younger age than those with pancreatitis related to other factors , even though the diagnosis is often late compared with the appearance of symptoms . accurate diagnosis of gene - mutation - associated pancreatitis ( gmap ) is important for careful follow - up of these patients , as the risk of developing pancreatic adenocarcinoma is higher in this group than in the normal population or in patients affected by chronic pancreatitis not associated with gene mutations [ 23 , 24 ]  . 
the presence of a particular kind of duct stones with a bulls - eye appearance , with a dense peripheral rim and a noncalcified radiolucent central core on plain abdominal x - ray , was first reported by rohrmann et al . 
as prss1 gene mutations have been reported in association with familial chronic pancreatitis [ 6 ] , we hypothesised that the presence of duct stones with bulls - eye appearance might be associated with gmap . 
 multidetector computed tomography ( mdct ) is the most commonly used imaging modality for studying patients with chronic pancreatitis due to its high sensitivity in detecting duct stones [ 2632 ]  . 
in a previous retrospective study [ 33 ] of 14 patients with gmap and pancreatic - duct stones , all of which were studied with ct , the bulls - eye pattern was found in 5 / 14 ( 36% of cases )  . 
the second purpose was to compare other mdct findings in patients affected by gmap with those of patients with chronic pancreatitis not associated with gene mutations to identify further mdct findings related to gmap . 
 radiol med ( 2012 ) 117 : 12751286 introduzione la pancreatite cronica ( pc ) una malattia infiammatoria del pancreas caratterizzata da distruzione del parenchima pancreatico , fibrosi e dilatazione del dotto pancreatico principale , spesso associata alla presenza di calcoli duttali calcifici [ 15 ]  . 
recentemente sono state rilevate alcune mutazioni genetiche in associazione alla pancreatite cronica [ 620 ] , le pi frequenti legate al gene regolatore transmembrana della fibrosi cistica ( cftr ) [ 7 , 8 , 12 , 14 ] , al gene inibitore delle proteasi seriniche kazal tipo 1 ( spink1 ) [ 9 , 11 , 13 , 17 , 20 ] e al gene tripsinogeno cationico ( prss1 ) [ 6 , 10 , 1619 ]  . 
secondo alcuni autori [ 2 , 21 , 22 ] i pazienti con pancreatite associata a una di queste mutazioni genetiche evidenziano i primi sintomi clinici in et pi giovane rispetto ai pazienti con pancreatite causata da altri fattori eziologici , sebbene la diagnosi sia spesso tardiva rispetto alla comparsa dei sintomi . 
 una corretta diagnosi di gmap importante per un attento follow - up di questo gruppo di pazienti , poich il rischio di sviluppare un adenocarcinoma pancreatico risulta maggiore in questi soggetti rispetto alla popolazione normale e a pazienti affetti da pancreatite cronica non associata a mutazione genetica [ 23 , 24 ]  . 
la presenza di un particolare tipo di calcoli duttali con morfologia a bulls eye , con un cercine periferico denso e un core centrale non calcificato , radiotrasparente , fu descritta per la prima volta da rohrmann [ 26 ] nel 1981 al radiogramma diretto delladdome e successivamente da hoshina [ 27 ] nel 1999 con colangio - pancreatografia endoscopica retrograda nella pancreatite cronica familiare . 
 poich stata riportata lassociazione tra le mutazioni del gene prss1 e la pancreatite cronica familiare [ 6 ] abbiamo ipotizzato che la presenza di calcoli duttali con morfologia a bulls eye possa essere associata con le gmap . 
 la tomografia computerizzata multidetettore ( tcmd ) la metodica di imaging pi frequentemente impiegata nello studio di pazienti con pancreatite cronica per lelevata sensibilit nellidentificazione dei calcoli duttali [ 2632 ]  . 
 in uno studio precedente retrospettivo [ 33 ] in 14 pazienti con gmap e calcoli duttali pancreatici , tutti studiati con tc , laspetto a bulls eye era presente in 5 / 14 ( 36% dei casi )  . 
in 3 / 5 di questi pazienti sono state rilevate mutazioni del gene cftr e in 2 / 5 quelle del gene spink1 . obiettivo principale di questo studio di valutare prospetticamente la presenza dei calcoli duttali con morfologia a bulls eye alla tcmd e correlarla con la presenza di pancreatite cronica e mutazioni genetiche . secondo obiettivo dello studio comparare altre caratradiol med ( 2012 ) 117 : 12751286 materials and methods patient population teristiche tcmd di pazienti affetti da gmap con quelle di pazienti con pancreatite cronica e test genetici negativi per identificare altri elementi tcmd correlati alle gmap . 
the diagnosis of chronic pancreatitis was obtained on the basis of clinical data ( abdominal pain , at least a threefold increase in serum amylase and / or lipase levels ) and laboratory tests ( faecal elastase 1 , faecal fat , fasting glycaemia > 127 mg / dl )  . 
patients who had undergone sphincterotomy , lithotripsy or surgery were excluded from the study . all patients underwent genetic testing carried out on 50 g of genomic dna extracted from 200 l of blood treated with ethylenediaminetetraacetic acid ( edta ) and using a commercial kit ( qiagen , hilden , germany )  . 
mean age of onset was 39.5 ( range , 1668 ) years in patients with gmap and 48.5 ( range 3572 ) years in those with ngmap . clinically , 35 / 47 ( 74% ) patients presented with pancreatic abdominal pain ( epigastric pain radiating to the back ) , 22 / 47 ( 47% ) with dyspepsia , 15 / 47 ( 32% ) with steatorrhea and 5 / 47 ( 11% ) with weight loss . 
the interval between disease onset and mdct imaging was 10.210.1 ( range , 152 ) months , without any statistically significant difference between the gmap and ngmap group . imaging all patients enrolled in the study between may 2006 and materiali e metodi popolazione di pazienti sono stati inclusi nello studio prospettico tutti i pazienti con pancreatite cronica calcifica , giunti consecutivamente alla nostra osservazione da maggio 2006 a luglio 2008 . 
la diagnosi di pancreatite cronica stata ottenuta sulla base di dati clinici ( dolore addominale , incremento di almeno tre volte del livello delle amilasi e / o lipasi sieriche ) , esami di laboratorio ( elastasi fecale 1 , dosaggio del grasso fecale , glicemia a digiuno superiore a 127 mg / dl )  . 
 tutti i pazienti sono stati sottoposti ai test genetici mediante unanalisi di 50 g di dna genomico , estratto da 200 l di sangue trattato con acido tetracetico diamino etilene ( edta ) , mediante kit commerciale ( qiagen , hilden , germania )  . 
tutti gli esoni 4 del gene spink 1 sono stati amplificati usando primers specifici , come descritto da pfutzer [ 10 ]  . sulla base della presenza delle mutazioni genetiche i pazienti sono stati classificati in due gruppi : pazienti affetti da pancreatite cronica associata a mutazioni genetiche ( gmap ) e pancreatite cronica non associata a mutazioni genetiche ( ngmap )  . 
allesordio clinico di malattia , let media dei pazienti con gmap era di 39 , 5 anni ( range 1668 ) e di 48 , 5 anni ( range 3572 ) in quelli ngmap . clinicamente , 35 / 47 ( 74% ) pazienti presentavano dolore addominale di tipo pancreatico ( sede epigastrica con irradiazione al dorso ) , 22 / 47 ( 47% ) dispepsia , 15 / 47 ( 32% ) steatorrea e 5 / 47 ( 11% ) perdita di peso . 
a 120 - ml bolus of nonionic iodinated contrast material ( ultravist 370 , schering , berlin , germany ) was injected intravenously with an automatic injector ( stellant d dual syringe , medrad , pittsburgh , pa , usa ) at a flow rate of 4 ml / s , followed by 50 ml of saline solution at 4 ml / s . 
 the contrast - enhanced ct scan was performed with the bolus - tracking synchronisation technique , with a region of interest ( roi ) placed over the aortic lumen , taking care to avoid the vessel walls . 
the reconstruction thickness for images acquired in the precontrast phase was 2 mm , with an interval of 1 mthe pancreatic arterial and venous phases were acquired with a collimation of 640.625 m reconstruction thickness for images acquired in the pancreatic arterial and portal phases was 1 mm , with an interval of 0.50 m curved multiplanar reconstructions were obtained at the workstation ( ebv philips , best , the netherlands ) starting from the axial images of all phases of both the mdct studies ( 6and 64 - slice scanner )  . imaging tutti i pazienti inseriti nello studio tra maggio 2006 e dicembre 2006 sono stati sottoposti a indagine tcmd a 6 strati ( brillance ct ; philips , best , the netherlands ) con tempo di rotazione di 0 , 75 secondi . 
lo studio in fase precontrastografica stato esteso dalla cupola diaframmatica al processo uncinato del pancreas con scansione a 120 kvp , 200 ma , e collimazione di 61 , 5 m stato utilizzato uno spessore di ricostruzione di 2 mm , con un intervallo di ricostruzione di 1 msono stati somministrati 120 ml di mezzo di contrasto iodato non ionico a bolo ( ultravist 370 , schering , berlin , germania ) per via endovenosa tramite iniettore automatico ( stellant d dual syringe , medrad , pittsburgh , usa ) con velocit di flusso 4 ml / s seguiti da 50 ml di soluzione salina a 4 ml / s . 
 la scansione contrastografica ha previsto luso della sincronizzazione con bolus - tracking , dopo aver posizionato la regione di interesse ( roi ) allinterno del lume aortico , prestando attenzione a evitare le pareti del vaso . 
le immagini in fase arteriosa pancreatica sono state acquisite da 1 cm sopra il tripode celiaco fino a comprendere lintera ghiandola pancreatica dopo 20 secondi dal raggiungimento del bolus tracking ( collimazione : 60 , 75 mm )  . 
le immagini in fase portale sono state acquisite dal margine superiore del diaframma fino a comprendere i reni o la pelvi dopo 60 secondi dal raggiungimento del bolus tracking ( collimazione : 60 , 75 mm ; pitch : 0 , 9 ) ; lo spessore di ricostruzione stato di 1 mm nella fase arteriosa pancreatica e portale , con un intervallo di 0 , 50 m le tc eseguite tra gennaio 2007 e luglio 2008 sono state acquisite mediante una tc multidetettore a 64 strati ( brillance ct , philips , best , paesi bassi ) con tempo di rotazione di 0 , 4 secondi . 
i parametri di scansione della fase precontrastografica sono stati i seguenti : 120 kvp , 200 ma , collimazione di 641 , 25 mlo spessore di ricostruzione per le immagini acquisite in fase precontrastografica stato di 2 mm con intervallo di 1 mm . le fasi arteriosa pancreatica e venosa sono state acquisite con una collimazione di 640 , 625 mlo spessore di ricostruzione per le immagini acquisite in fase arteriosa pancreatica e portale stato di 1 mm con intervallo di 0 , 50 m sono state successivamente ottenute su workstation ( ebv philips , best , paesi bassi ) ricostruzioni multiplanari curviliradiol med ( 2012 ) 117 : 12751286 image analysis images were independently reviewed by two radiologists ( rg , cc ) with > 10 years experience each in gastrointestinal imaging . 
 axial images of all phases were assessed at the workstation ( ebv philips ) with optimal window levels for parenchyma ( 600 / 1 , 500 hu ) and for bone ( 400 / 2 , 000 hu )  . 
the qualitative analysis assessed presence / absence of duct stones with noncalcified , hypodense central cores compared with the remaining portion of the calcified stone ( bulls - eye ) , site of the duct stones ( head / bodytail ; portions of the gland corresponding to the splenicportal confluence to the right and left of the superior mesenteric vein , respectively )  . in quantitative analysis , a third radiologist ( mca ) , not involved in the qualitative analysis , assessed the number and maximum diameter of duct stones and the maximum diameter of the main pancreatic duct ( head / bodytail )  . 
the diameter of the main pancreatic duct was measured as the distance between the anterior and posterior walls of the duct in the pancreatic head ( the portion of the gland to the right of the superior mesenteric vein at the level of the splenic portal confluence ) and bodytail ( the portion to the left of the superior mesenteric vein at the level of the splenicportal confluence )  . nee a partire dalle immagini assiali di tutte le fasi di entrambe le indagini tcmd ( 6 e 64 strati )  . 1279 analisi delle immagini le immagini sono state indipendentemente analizzate da due radiologi ( rg , cc ) con esperienza superiore a 10 anni nella radiologia del tratto gastrointestinale . 
sono state valutate le immagini assiali di tutte le fasi acquisite su workstation ( ebv philips , best , paesi bassi ) con valori di finestra ottimali per i parenchimi ( 600 / 1500 hu ) e per il tessuto osseo ( 400 / 2000 hu ) , impiegando un tempo medio non superiore a quello dedicato allanalisi delle immagini per la refertazione . 
nellanalisi qualitativa sono state valutate : la presenza / assenza di calcoli duttali con core centrale non calcifico , ipodenso rispetto alla restante porzione del calcolo calcifica ( bulls eye ) , sede dei calcoli duttali ( testa / corpo - coda del pancreas : porzione di ghiandola a livello della confluenza splenoportale a destra e a sinistra della vena mesenterica superiore , rispettivamente )  . 
 nellanalisi quantitativa un terzo radiologo ( mca ) , non coinvolto nellanalisi qualitativa , ha valutato il numero dei calcoli duttali , il loro massimo diametro , diametro massimo del dotto pancreatico principale ( testa / corpo - coda )  . 
come diametro del dotto pancreatico principale stata considerata la misura tra la parete anteriore e posteriore del dotto pancreatico principale a livello della testa pancreatica ( porzione di ghiandola a destra della vena mesenterica superiore allaltezza della confluenza splenoportale ) e del corpo - coda ( porzione a sinistra della vena mesenterica superiore allaltezza della confluenza splenoportale )  . statistical analysis analisi statistica the fisher test was used to confirm the statistical significance of differences in qualitative data and the mannwhitney u test for quantitative analysis . 
statistical significance was set at 5% . per verificare la significativit statistica della differenza dei dati qualitativi stato utilizzato il fisher test , mentre per lanalisi dei dati quantitativi stato utilizzato il mann - whitney u test . 
multidetector computed tomography ( mdct ) study : axial images ( a , b ) and multiplanar reconstructions in the precontrast phase ( c ) and in the pancreatic arterial phase ( d ) , with a liver soft - tissue window in the images in a , c , e and d and a bone window in b . 
indagine tcmd : immagini assiali ( a , b ) e ricostruzioni multiplanari in fase precontrastografica ( c ) e in fase arteriosa pancreatica ( d ) , con finestra per tessuti molli da fegato nelle immagini in a , c e d e per tessuto osseo da osso nellimmagine in b . 
 stones were ubiquitous in the two groups of patients , without significant differences between them . quantitative analysis the average number of stones in patients with gmap was 19.813.3 ( range , 552 ) and reached 20.715.3 ( range , 365 ) in patients with ngmap ( p = ns )  . 
 analisi quantitativa il numero medio di calcoli riscontrati nei pazienti con gmap stato di 19 , 813 , 3 ( range 552 ) mentre di 20 , 715 , 3 ( range 365 ) nei pazienti con ngmap ( p = ns )  . 
il valore medio del massimo diametro dei calcoli duttali ( tabella 1 ) risultato di 15 , 38 , 7 mm ( range 540 mm ) nei pazienti con gmap radiol med ( 2012 ) 117 : 12751286 1281 fig . 
significant dilatation of the main pancreatic duct ( c , d , short arrow ) , atrophy of the pancreatic parenchyma and multiple large duct stones in the head ( a , d ) and body / tail of pancreas ( c , d ) can be seen . 
sono presenti marcata dilatazione del dotto pancreatico principale ( c , d , freccia corta ) , atrofia del parenchima pancreatico e multipli calcoli duttali di grandi dimensioni a livello della testa ( a , d ) e del corpo - coda del pancreas ( c , d )  . 
in accordo con i dati della letteratura , come per altro nella precedente analisi retrospettiva nella nostra casistica , la mutazione riscontrata con maggior frequenza stata quella del gene cftr ( 52% ) , 1282 radiol med ( 2012 ) 117 : 12751286 fig . 
diffuse dilatation of the main pancreatic duct , atrophy of the pancreatic parenchyma and multiple large calcified duct stones in the head ( a , b ) and body / tail of pancreas ( c , d ) can be observed . 
indagine tcmd : immagini assiali ( a , b , d ) e ricostruzione multiplanare ( c ) in fase precontrastografica ( a , c ) e contrastogafica arteriosa pancreatica ( d ) , con finestra da tessuti molli nelle immagini in a e d e finestra da tessuto osseo nelle immagini in b e c . 
sono presenti diffusa dilatazione del dotto pancreatico principale , atrofia del parenchima pancreatico e multipli calcoli duttali calcifici di grandi dimensioni a livello della testa ( a , b ) e del corpo - coda del pancreas ( c , d )  . 
le immagini con finestra sia da tessuti molli che da tessuto osseo non mostrano aspetto a bulls eye dei calcoli . table 1 statistically significant difference between gene - mutation - associated pancreatitis ( gmap ) and non - gmap ( ngmap )  . 
stone diameter was also larger in gmap ( p < 0.04 using mann whitney u test ) gmap stones with bulls eye appearance stone maximum diameter ( average ) tabella 1 differenza statisticamente significativa tra gmap e ngmap . 
all genetic tests performed on cftr , spink1 and press1 were negative for gene mutations in both patients : no disease was found to be associated with the onset of chronic pancreatitis ( ad )  . 
axial images in the multidetector computed tomography ( mdct ) precontrast phase with a soft - tissue window ( a , c ) and bone window ( b , d )  . 
4a - d pazienti con ngmap ( tutti i test genetici eseguiti su cftr , spink 1 e press 1 sono risultati negativi per mutazioni geniche in entrambi i pazienti : a , b e c , d ; non stata trovata nessuna affezione associata allinsorgenza di pc )  . 
 i calcoli sono omogeneamente calcifici nel caso in a , b ; con finestra da osso nelle immagini assiali nel caso c , d possibile notare la presenza di piccolo core centrale non calcifico ( aspetto a bulls eye ) nei calcoli della testa pancreatica ( d , freccia )  . data and with our previous retrospective analysis , the most common mutation involves the cftr gene ( 52% ) , with a prevalence among males of 63% [ 34 ]  . recognition of the gene mutation is especially important for the prognosis of patients with chronic pancreatitis , as the risk of developing pancreatic cancer is higher in gmap than in ngmap patients [ 23 , 24 ]  . 
 previous studies [ 26 , 27 ] describe imaging findings of pancreatic - duct stones with dense peripheral margins and radiolucent , noncalcified central core ( bulls - eye pattern ) in some families of patients with chronic pancreatitis . 
in a previous retrospective study [ 33 ] , 5 / 14 patients with gmap and duct stones on ct showed a bulls - eye appearance , 3 / 5 of whom had cftr gene mutation and 2 / 5 spink1 gene mutation . in our series of 47 patients with chronic calcific pancreatitis , presence of the bulls - eye pattern of duct stones on mdct was significantly associated with gene mutations , as the difference in frequency of bulls - eye pattern con una prevalenza nel sesso maschile del 63% [ 34 ]  . il riconoscimento di mutazione genetica particolarmente importante per la prognosi dei pazienti con pancreatite cronica , poich il rischio di insorgenza di neolplasia pancreatica pi elevato nei pazienti con gmap rispetto a quelli ngmap [ 23 , 24 ]  . 
 in passato alcuni autori [ 26 , 27 ] hanno descritto con alcune tecniche di imaging la presenza di calcoli duttali pancreatici con un margine periferico denso e centro radiotrasparente in quanto non calcifico ( pattern a bulls eye ) in alcune famiglie di pazienti con pc . 
anche in un precedente studio retrospettivo [ 33 ] , 5 / 14 pazienti con gmap e calcoli duttali alla tc avevano aspetto a bulls eye , dei quali 3 / 5 presentavano mutazione del gene cftr , e 2 del gene spink 1 . 
 nella nostra serie di 47 pazienti affetti da pancreatite cronica calcifica , la presenza del pattern tcmd a bulls eye dei calcoli duttali risultata significativamente associata al riscontro di mutazione genetica , in quanto la diversa frequenza di calcoli con pattern tcmd a bulls eye stata rilevata statisticamente significativa nei due gruppi di 1284 radiol med ( 2012 ) 117 : 12751286 on mdct was statistically significant between gmap and ngmap patients ( p < 0.0001 ) ( table 1 )  . 
however , because we tested only 35 of the main mutations of the cftr gene and two of the main mutations of the prss1 gene , these patients might carry other rarer or as yet unknown mutations for which we failed to test . 
 another interesting finding was the presence of larger pancreatic - duct stones in patients with gmap than in those with ngmap ( p < 0.04 ) , consistent with rohrmann et al . , who reported stones with diameters > 15 mm in patients with gmap [ 26 ]  . 
even in our previous retrospective study [ 33 ] , the mean maximum diameter of stones on ct was 19.411.9 mm ( range , 250 mm ) in 14 / 25 patients with gmap . 
conversely , the number and location of duct stones and the maximum diameter of the main pancreatic duct did not differ significantly between groups . a correct diagnosis of gmap is extremely important for the prognosis of these patients , who face a higher risk of developing cancer compared to individuals with ngmap . 
 performing the genetic screening test is , however , complex and expensive and , given the small number of patients carrying these mutations , mdct can be used to identify large ductal stones with the bulls - eye pattern ( maximum diameter 15 mm )  . 
in young patients with a history of chronic pancreatitis and who have no risk factors for this disease , mdct may suggest a hypothetical genetic aetiology of the pancreatitis , which could subsequently be confirmed by genetic testing . the main limitation of our study was that we limited the search for gene mutations to those most often associated with chronic pancreatitis ( cftr , spink1 , and prss1 ) and , in particular , to a small number of mutations involving these genes . 
finally , the patient population was small , even though this reflects the low incidence of this condition . pazienti , gmap e ngmap ( p < 0 , 0001 , tabella 1 )  . 
poich abbiamo testato solo 35 delle principali mutazioni del gene cftr e 2 delle principali mutazioni del gene prss1 , questi pazienti della nostra casistica potrebbero essere portatori di altre mutazioni pi rare da noi non testate . 
ci potrebbe spiegare il riscontro di calcoli duttali con pattern a bulls eye in due pazienti della nostra casistica negativi ai test genetici e senza riscontro di nessuna patologia associata alla pancreatite cronica . 
 altro risultato di questo studio stata la presenza di calcoli duttali pancreatici con dimensioni maggiori nei pazienti con gmap comparati con quelli ngmap ( p < 0 , 04 ) , in accordo con rohrmann che descrisse in pazienti con pancreatite cronica e mutazioni genetiche calcoli pancreatici con diametro massimo superiore a 15 mm [ 26 ]  . 
in questo studio , la media del diametro massimo dei calcoli duttali stato di 15 , 2 mm nei pazienti con gmap e di 10 , 3 mm nei pazienti con ngmap . 
anche nel precedente lavoro retrospettivo [ 33 ] 14 / 25 pazienti con gmap alla tc presentavano una media di diametro massimo di 19 , 411 , 9 mm ( range 250 mm )  . 
diversamente , il numero dei calcoli duttali rilevati , la loro sede e il diametro massimo del dotto pancreatico principale non sono risultati significativamente differenti nei due gruppi di pazienti . 
la realizzazione di test genetici come screening peraltro complessa e costosa e , considerando anche che il numero di portatori di tali mutazioni rimane esiguo , la tcmd risulta metodica utile allidentificazione di calcoli duttali con morfologia bulls eye e di cospicue dimensioni ( diametro massimo pari o superiore a 15 mm )  . 
in pazienti giovani con storia di pancreatite cronica , in assenza di fattori di rischio per tale affezione , tale indagine pu essere daiuto nel suggerire lipotesi di uneziologia genetica della pancreatite , che deve essere successivamente confermata da test genetici . 
 il limite principale del nostro studio rappresentato dalla ricerca delle mutazioni genetiche limitata alle forme pi frequentemente associate a pancreatite cronica ( cftr , spink 1 e prss 1 ) e soprattutto a un numero ristretto delle mutazioni che colpiscono questi geni . 
altro limite costituito dalla mancanza di un riscontro istopatologico dei calcoli pancreatici con pattern a bulls eye , per cui non conosciamo le caratteristiche anatomopatologiche e strutturali del core centrale non calcifico di questi calcoli . 
 radiol med ( 2012 ) 117 : 12751286 1285 conclusions conclusioni the presence of duct stones with bulls - eye appearance on mdct correlates with gmap , as previously suggested by other authors . 
questi criteri possono quindi essere di aiuto nellidentificare i pazienti con gmap al fine di selezionare coloro che risultano a pi alto rischio di sviluppare un adenocarcinoma duttale in rapporto alla popolazione generale . 
clinical presentation and disease course are extremely variable , as there may be acute onset with acute coronary syndrome , or cardiogenic shock , or progressive heart failure or arrhythmias . 
all patients underwent b - mode echocardiography ( echo ) and tissue doppler imaging , coronarography , ventriculography , endomyocardial biopsy and contrast - enhanced mri examination , as well as clinical and echo follow - up at 6 months . 
at 6 - month follow - up , patients were divided in two groups according to values of end - systolic volume and ejection fraction : patients with negative remodelling and those with positive remodelling . 
contrast - enhanced mri is useful both in the diagnosis and as a prognostic indicator in the clinical suspicion of myocarditis . keywords myocarditis acute coronary syndrome heart failure arrhythmias magnetic resonance imaging riassunto obiettivo . 
lesatta incidenza delle miocarditi non ben conosciuta e spesso la diagnosi viene raggiunta tardivamente o non viene raggiunta affatto ; anche la presentazione ed il decorso clinico sono estremamente variabili , potendo manifestarsi con un esordio acuto come una sindrome simil - coronarica acuta o shock cardiogeno , oppure con una insufficienza cardiaca spesso progressiva , o ancora con limprovvisa comparsa di aritmie . 
scopo del nostro studio stato il tentativo di identificare eventuali fattori prognostici alla risonanza magnetica ( rm ) eseguita allesordio della sintomatologia e dopo sei mesi in pazienti con biopsia endomiocardica positiva per miocardite . 
da gennaio a dicembre 2010 sono stati studiati 56 pazienti consecutivi in base alle possibili presentazioni cliniche suddette ( 20 con sindrome similcoronarica acuta , 20 con scompenso cardiaco e 16 con aritmie ) , tutti sottoposti ad ecocardiografia b - mode e doppler tissutale , coronarografia , ventricolografia e biopsia endomiocardica e rm con mezzo di contrasto ( mdc )  . 
i pazienti al follow - up sono stati divisi in due gruppi in base alla variazione di volume telesistolico ( vts ) e frazione di eiezione ( fe ) : pazienti con rimodellamento negativo e pazienti con rimodellamento positivo . 
la rm con mdc estremamente utile non solo per la diagnosi ma anche come indicatore prognostico nel sospetto clinico di miocardite . 1310 radiol med ( 2012 ) 117 : 13091319 parole chiave miocardite sindrome coronarica acuta insufficienza cardiaca aritmie risonanza magnetica introduction introduzione myocarditis is a common cardiac condition that is found in approximately 9% of autopsy examinations [ 1 ]  . 
it appears to be a major cause of sudden cardiac death in patients under the age of 40 years [ 2 ] ; the condition may progress to chronic dilated cardiomyopathy [ 3 ]  . 
later , other viruses , such as adenoviruses , were identified in endomyocardial biopsies of patients with suspected myocarditis and with idiopathic dilated cardiomyopathy [ 5 ]  . it is important to note that the natural course of myocarditis varies , as do clinical presentation , laboratory findings and aetiology . 
although standard echocardiography ( echo ) , tissue doppler imaging ( tdi ) , troponin assays and other noninvasive cardiac imaging techniques such as magnetic resonance imaging ( mri ) play an essential role in the diagnosis and follow - up of myocarditis [ 6 ] , it is difficult to identify prognostic factors , especially in a population of patients with dilated cardiopathy due to myocarditis . the aim of this study was to evaluate the presence of different patterns of myocardial damage and identify prognostic factors capable of predicting improvement or progression to cardiac failure by correlating the different clinical presentations , mri patterns and follow - up data in a group of patients with clinically suspected myocarditis subjected to cardiac biopsy . materials and methods between january and december 2010 , we examined 116 consecutive patients with suspected myocarditis on the basis of a combination of signs and symptoms , including chest pain , dyspnoea , fatigue , electrocardiographic alterations ( conduction blocks , st - segment abnormalities ) , arrhythmias ( supraventricular tachycardia , sustained or nonsustained ventricular tachycardia ) coupled with a history compatible with inflammatory disease , such as diarrhoea , fever , malaise and elevated c - reactive protein le miocarditi sono una patologia cardiaca comune , identificata in circa il 9% degli esami autoptici [ 1 ] , che sembra essere la principale causa di morte cardiaca improvvisa in soggetti al di sotto dei quarantanni [ 2 ] ; inoltre possono progredire in cardiomiopatia dilatativa [ 3 ]  . 
attualmente i virus sono considerati la causa pi frequente di miocarditi in nord america e in europa ; inizialmente si pensava che i coxsackie virus fossero tra le cause pi comuni di miocarditi , visto lelevato titolo anticorpale che si riscontrato nei pazienti con miocardite acuta ed in fase di convalescenza . 
successivamente , altri virus , come gli adenovirus , sono stati rinvenuti nelle biopsie miocardiche di pazienti con sospetta miocardite e con cardiomiopatia dilatativa idiopatica [ 5 ]  . importante precisare che la storia naturale delle miocarditi variabile , come variabili sono la presentazione clinica , il quadro laboratoristico , oltre leziologia . 
lecocardiografia standard e tissue doppler imaging ( tdi ) , il dosaggio delle troponine , ed altre tecniche di imaging cardiaco non invasivo come la risonanza magnetica ( rm ) forniscono un notevole contributo nellinquadramento diagnostico e nel follow - up delle miocarditi [ 6 ] , tuttavia rimane difficile individuare fattori prognostici , specie in una popolazione di individui con cardiopatia dilatativa dovuta a miocardite . a tale proposito , nel nostro studio abbiamo valutato il rapporto tra la differente presentazione clinica ed il quadro di imaging rm in un gruppo di pazienti con sospetto clinico di miocardite , sottoposti a biopsia endomiocardica , correlando tali dati al follow - up , allo scopo di valutare la presenza di differenti pattern di danno miocardico e di riconoscere un fattore predittivo in grado di valutare il miglioramento oppure la progressione verso lo scompenso cardiaco . materiali e metodi nel nostro centro abbiamo esaminato 116 pazienti consecutivi , da gennaio a dicembre 2010 , con sospetto di miocardite sulla base della combinazione di sintomi e segni quali dolore toracico , dispnea , fatica , alterazioni ecg ( blocchi di conduzione , anomalie del tratto st ) , aritmie ( tachicardia sopraventricolare , tachicardia ventricolare sostenuta o non sostenuta ) in combinazione con una storia compatibile con patologia radiol med ( 2012 ) 117 : 13091319 1311 ( crp )  . 
on admission , patients with acute coronary - like syndrome were assessed with bidimensional echo , tdi , and coronarography performed as urgent procedures , and in all other cases , as elective procedures . 
 patients were followed up at 6 months with bidimensional echo and tdi . three patterns of clinical presentation were identified : ( 1 ) chest pain associated with ventricular repolarisation changes and raised indexes of myocardial necrosis ; ( 2 ) signs and symptoms of cardiac failure such as dyspnoea , dependent oedema , asthenia ; ( 3 ) onset of arrhythmias . cardiac magnetic resonance imaging mri examinations were performed with a 1.5 - t imager ( signa excite ii echospeed , general electric medical systems , buc , paris , france ) equipped with high - performance gradients ( maximum gradient strength 33 mtm / m , maximum gradient slew rate 175 t m - 1 s - 1 )  . 
images were acquired in the fourand two - chamber long - axis views with cine - mr steady - state free precession ( ssfp ) sequences and in the short axis plane with black - blood fast spin echo ( fse ) sequences , with double inversion recovery for suppression of the blood signal and an additional inversion recovery pulse for suppression of the fat signal to demonstrate the presence of possible areas of high signal intensity caused by oedema . 
 finally , late - enhancement ( le ) images were acquired 15 min after intravenous administration of paramagnetic contrast material [ gdbenzyloxy - propionic tetraacetic acid ( bopta ) , 0.1 mmol / kg ] [ 7 ] using a t1 - weighted 2d fast gradient - echo ( fgre ) sequence with an inversion recovery preparation pulse to suppress the signal of the healthy myocardium and highlight the areas of enhancement . 
the endocardial and epicardial contours were delineated in the short - axis planes of both the cine - mr iminfiammatoria come diarrea , febbre , malessere e aumento della proteina c reattiva . 
ciascun paziente stato sottoposto al momento del ricovero a valutazione ecocardiografica bidimensionale , nonch a doppler tissutale , a coronarografia , in urgenza nei casi con presentazione simil - sindrome coronarica acuta , in elezione negli altri casi , tutti sottoposti a cateterismo cardiaco con biopsia miocardica ed a risonanza magnetica cardiaca con mezzo di contrasto paramagnetico ( gadolinio )  . 
a sei mesi stata eseguita ecocardiografia bidimensionale e doppler tissutale . sono stati identificati tre pattern di identificazione : ( 1 ) presentazione con dolore toracico associato ad alterazioni della ripolarizzazione ventricolare e movimento degli indici di miocardionecrosi ; ( 2 ) presentazione clinica caratterizzata da segni e sintomi di scompenso cardiaco quali dispnea , edemi declivi , astenia ; ( 3 ) presentazione caratterizzata dalla comparsa di aritmie . risonanza magnetica cardiaca gli esami di risonanza magnetica sono state eseguiti mediante apparecchiatura da 1 , 5 t ( signa excite ii echospeed , general electric medical systems , buc , parigi , francia ) equipaggiata con sistema di gradienti ad alte prestazioni ( maximum gradient strength 33 mtm / m , maximum gradient slew rate 175 t m - 1 s - 1 )  . 
le immagini sono state acquisite in asse lungo quattro e due camere mediante sequenze cine - rm con tecnica steady state free precession ( ssfp ) , in asse corto mediante sequenze fast spin echo ( fse ) a sangue nero con tecnica double inversion recovery per la soppressione del segnale del sangue ed ulteriore impulso inversion recovery per la soppressione del segnale del tessuto adiposo , al fine di documentare la presenza di eventuali aree di iperintensit del segnale , riferibili ad edema . 
infine sono state acquisite immagini dopo somministrazione ev di mezzo di contrasto ( mdc ) paramagnetico [ gadobenato dimeglumina ( gd - bopta ) , 0 , 1 mmol / kg ] [ 7 ] 15 minuti dopo liniezione ( tecnica late enhancement , le ) , mediante una sequenza t1pesata fast gradient echo ( fgre ) 2d con impulso di preparazione inversion recovery atto a sopprimere il segnale del miocardio sano ed esaltare le aree miocardiche caratterizzate da accumulo di mdc . 
two of the three samples were frozen for molecular studies and the remaining samples fixed in formalin and paraffall invasive procedures were carried out after the patients informed consent had been obtained . 
i profili endocardici ed epicardici sono stati delineati nelle immagini asse corto sia della cine - rm , per il calcolo della funzione contrattile regionale e degli indici di funzione sistolica globale biventricolare , sia del late enhancement , per la quantificazione in grammi del tessuto patologico . 
le biopsie miocardiche ( da 3 a 4 per ogni ventricolo ) sono state ottenute in regione setto apicale ; 2 dei 3 campioni erano congelati per gli studi molecolari . 
multiple sezioni dello spessore di 5 micron sono state colorate con ematossilina / eosina , van gieson elastico di miller , tricromia di masson , ed esaminate al microscopio ottico . 
tutti i campioni sono stati sottoposti ad immunoistochimica per la caratterizzazione degli infiltrati infiammatori . molecular biology biologia molecolare two biopsy samples from each patient were analysed with polymerase chain reaction ( pcr ) and pcr with reverse transcriptase ( rt - pcr ) to identify viral nucleic acids for the main cardiotropic viruses . due campioni bioptici da ciascun paziente sono stati sottoposti a polymerase chain reaction ( pcr ) e pcr con trascrittasi inversa , al fine di individuare acidi nucleici virali per i principali virus cardiotropi . statistical analysis statistical analysis was done with the software package spss 10.0 for windows ( spss inc . , chicago , il , usa )  . 
we used nonparametric test for unpaired data ( mann - whitney u test for comparison of two groups and kruskal - wallis test for comparison of more than two )  . 
sono stati utilizzati test non parametrici per dati non appaiati ( test di mann - whitney u quando si confrontavano due gruppi diversi e quello di kruskal - wallis quando se ne confrontavano pi di due ) .nel confronto fra pi gruppi si ricorso alla correzione di bonferroni applicata al test di mann - whitney u . 
la trasformazione logaritmica stata usata per effettuare il test post - hoc per landamento liradiol med ( 2012 ) 117 : 13091319 1313 transformation was used for the post hoc test for the linear trend at univariate analysis of variance ( anova )  . 
of these , eight presented with infarction - like syndrome , five with heart failure and three with arrhythmias . patients were followed up at 6 months by clinical assessment , echo and tdi . 
they were subdivided on the basis of the delta ejection fraction ( ef ) increase in ef at follow - up compared with baseline value , cutoff 10% and delta endsystolic volume ( esv ) reduction in esv compared with baseline , cutoff 15% , with the latter intended as a reflection of positive remodelling [ 8 , 9 ]  . negative remodelling was observed in 26 patients and was distributed as follows : 4 / 20 with acute coronary - like syndrome ; 14 / 20 with heart failure ; 8 / 16 with arrhythmias ( table 1 )  . 
sixteen patients ( nine presenting with heart failure and seven with arrhythmias ) were treated with corticosteroids on the basis of the clinical picture and molecular biology findings ; at 6 - month follow - up , they all showed a 10% in tutti i pazienti lanalisi istologica ed immunoistochimica ha confermato la presenza di miocardite linfocitaria attiva . biologia molecolare di tutti i pazienti , 16 sono risultati positivi per presenza di genoma di parvovirus . 
in 8 di questi pazienti la miocardite ha esordito come sindrome simil - infartuale , in 5 come insufficienza cardiaca , in 3 come aritmia . decorso clinico i pazienti sono stati sottoposti a follow - up a sei mesi mediante valutazione clinica , ecocardiografica e doppler tissutale . 
i pazienti sono stati suddivisi sulla base del delta della frazione di eiezione ( fe ) ( aumento della fe nel follow - up rispetto al valore basale , cut - off 10% ) e sulla base del delta del volume telesistolico ( vts ) ( riduzione del vts , cut - off 15% rispetto al basale ) , inteso questultimo come espressione del rimodellamento positivo [ 8 , 9 ]  . il rimodellamento negativo stato osservato in 26 pazienti , cos distribuito : 4 / 20 nel gruppo con presentazione simil - sindrome coronarica acuta ; 14 / 20 nel gruppo con presentazione a tipo insufficienza cardiaca , 8 / 16 nel gruppo con presentazione caratterizzata da aritmie ( tabella 1 )  . 
il gruppo dei pazienti con rimodellamento positivo era costituito da 30 pazienti , cos suddivisi : 16 pazienti con esordio simil - sindrome coronarica acuta , 6 con esordio caratterizzato da scompenso cardiaco e 8 pazienti che avevano presentato aritmie allesordio . 
si evidenzia impregnazione di mdc in sede subepicardica inferiore ed infero - laterale , in paziente con miocardite e presentazione clinica a tipo sindrome coronarica acuta . radiol med ( 2012 ) 117 : 13091319 1315 fig . 
2a short - axis 2d inversion - recovery fast gradient echo postgadolinium images , from base to apex ; intramural delayed enhancement in septal wall in a patient with myocarditis and heart failure presentation ( new york heart association class ii )  . 
del gruppo che esordiva con patologia simil - sindrome coronarica acuta , 18 pazienti presentavano le ( media le 3 , 8% lv mass range 2%21 , 2% ) ; del gruppo che esordiva con scompenso cardiaco 13 pazienti presentavano le ( media le 6% lv mass range 3 , 2%9 , 8% ) ; del gruppo che esordiva con aritmie 10 pazienti presentavano le ( media 6 , 9% lv mass range 0%5 , 2% )  . 
confrontando i due pattern di distribuzione del le si evidenziava una differenza statisticamente significativa tra il gruppo con presentazione simil - sindrome coronarica acuta e il gruppo aritmia ( p < 0 , 001 ) rispetto al gruppo sindrome coronarica acuta e scompenso cardiaco ( p = 0 , 75 )  . 
confrontando invece le due sottopopolazioni di pazienti , si osservato che lespressione del le era nettamente maggiore nel gruppo delta fe < 10% e delta vts < 15% ( rispettivamente 21 / 26 , pari all88% nel gruppo con rimodellamento negativo , rispetto a 14 / 30 , pari al 46% nel gruppo con rimodellamento positivo )  . 
inoltre raggruppando tutti i pazienti , si osservata una correlazione significativa allesordio tra valore percentuale di le e volumi telediastolici , sia sinistro ( p = 0 , 038 ) , che , soprattutto , destro ( p = 0 , 015 )  . 
si apprezza enhancement settale inferiore in sede intramurale , in paziente con miocardite e presentazione con aritmie ventricolari ( tachicardia ventricolare non sostenuta )  . discussion discussione our data suggest three distinct forms of clinical presentation . 
probably , aetiological agent affects the endothelial cells but not the myocytes , causing endothelial dysfunction and diapedesis of inflammatory cells to the myocardial interstitium with consequent damage to the myocytes . 
this combination of ischaemia and inflammation may explain the ecg changes and the raised levels of circulating troponin ; in addition , focal distribution of the inflammatory process may account for the fact that lv function is not severely impaired . the other two clinical presentations are heart failure and arrhythmias . 
probabilmente in questi pazienti agisce un agente eziologico che colpisce le cellule endoteliali ma non i miociti , causando una disfunzione endoteliale , come pure linduzione della diapedesi di cellule infiammatorie nellinterstizio miocardico con successivo danno dei miociti . 
tale combinazione di ischemia e infiammazione pu spiegare le alterazioni elettrocardiografiche e laumento del livello di troponina circolante ; inoltre la distribuzione focale del processo infiammatorio pu spiegare il fatto che la funzione ventricolare sinistra non sia severamente compromessa . le altre due presentazioni cliniche sono rappresentate dallo scompenso cardiaco e dallinsorgenza di aritmie ; queste presentazioni sono ampiamente descritte in letteratura [ 1215 ]  . 
tali pazienti presentano una significativa dilatazione e disfunzione ventricolare sinistra allesordio e recuperano di meno rispetto al gruppo precedente nel radiol med ( 2012 ) 117 : 13091319 1317 cells and virus - specific immune response play a key role [ 16 ]  . 
an abnormal immune response may explain the more severe lv dysfunction seen in these patients and the slower , if not absent , clinical and functional recovery . patterns of myocardial injury on the basis of le distribution in patients with different clinical presentations , we identified two patterns of myocardial injury . 
the first , which is present in the majority of patients presenting with acute coronary - like syndrome , has subepicardial location at the level of the left lateral wall . 
unalterata risposta immunitaria pu spiegare la maggiore disfunzione ventricolare sinistra in questi pazienti e il rallentato se non assente recupero clinico e funzionale . pattern di danno miocardico in base alla distribuzione del le nei pazienti con differente presentazione clinica abbiamo rilevato due pattern di danno miocardico . 
il primo , che presente nella maggioranza dei pazienti che esordisce con sintomatologia simil - sindrome coronarica acuta , si localizza a livello della parete laterale sinistra , in sede sub - epicardica . 
il secondo , che presente in maggioranza nelle altre due popolazioni cliniche di pazienti , si localizza a livello del setto interventricolare , a sede intramurale ; questo potrebbe spiegare il fatto che questi ultimi hanno una maggiore incidenza di aritmie ventricolari , blocchi della conduzione ed una prognosi pi sfavorevole . clinical course decorso clinico our data indicate that patients presenting with myocardialinfarction - like symptoms show an improvement in ef and recover almost completely . 
it is likely that there dai nostri dati si evince che coloro che esordiscono con una sintomatologia simil - infartuale hanno un miglioramento in termini di frazione deiezione e recuperano quasi completamente . 
if a certain threshold is exceeded , dilation may become irreversible , and this may explain why lv dilation in the acute phase may be a predictor of chronic lv dysfunction and dilation . 
se viene superata una certa soglia , la dilatazione pu diventare irreversibile e questo pu spiegare perch la dilatazione ventricolare sinistra nella fase acuta possa essere un predittore di disfunzione e di dilatazione ventricolare sinistra cronica . 
tale pattern di distribuzione settale correlato a una disfunzione e dilatazione ventricolare sinistra e pu essere riscontrato anche in pazienti con cardiomiopatia dilatativa apparentemente idiopatica [ 2729 ] , ma altri studi saranno necessari per confermare le differenti ipotesi . conclusions conclusioni late enhancement identifies a myocardial injury in patients with myocarditis . 
our study has some limitations : firstly , the biopsy and the mr examination were only performed in patients who were not excluded from the study due to coronary disease at coronarography ( there is a theoretical possibility of myocarditis coexisting with significant coronary stenosis )  . 
finally , the follow - up was performed only with ecg to evaluate positive or negative remodelling and not with mri , which means there are no data on the evolution of le at follow - up . il le identifica un danno miocardico in pazienti con miocardite e la sua differente espressione e localizzazione in grado , insieme alla presentazione clinica iniziale dei pazienti , di predire landamento clinico e funzionale di questi nel tempo . 
simonetti department of diagnostic and molecular imaging , interventional radiology and radiation therapy , fondazione policlinico tor vergata , viale oxford 81 , 00133 rome , italy correspondence to : a . 
valutare la fattibilit della tomografia computerizzata ( tc ) a bassa dose con algoritmo di ricostruzione adaptive statistical iterative reconstruction ( asir ) nellesame total - body con ridotta differenza di potenziale e ridotta intensit di corrente del tubo radiogeno . 
il valore medio di dose efficace ottenuto con lutilizzo dellasir stato 15 , 65 msv versus 21 , 85 , 3 msv con il protocollo fbp ( p < 0 , 0001 )  . 
although the mean dose reaches a value that is still comparable with that of natural radiation , it is estimated that ct alone is responsible for around 2% of all tumours diagnosed in the usa [ 2 ]  . 
the cumulative risk may be even higher , especially for certain subpopulations of patients , for example those requiring multiphase imaging or undergoing serial studies or obese and paediatric patients . a number of dose - reduction strategies have been devised and implemented in order to ensure an image quality that does not undermine ct diagnostic accuracy [ 5 , 6 ]  . 
the most effective are automatic modulation of tube current ( mas ) [ 7 ] , reduction of current intensity ( ma ) [ 8 ] and beam energy ( kv ) [ 9 ] , and adequate collimation of the x - ray beahowever , a direct consequence of dose reduction is increased noise , which the currently used reconstruction system filtered back projection ( fbp ) is unable to compensate for . the adaptive statistical iterative reconstruction ( asir ) algorithm allows dose reduction systems to be applied while preserving image quality by noise correction obtained with repeated or iterative statistical calculations [ 10 ]  . 
if it is used at 100% , it tends to provide a plastic image , with an unusually homogeneous attenuation . recent studies have investigated the potential of asir in the study of the chest [ 11 , 12 ] and abdominal regions [ 13 16 ] , in cardiac imaging and in virtual colonoscopy , providing useful indications as to technical settings of diagnostic tests and their possible limitations . 
we also compared the diagnostic quality obtained with asir and fbp . materials and methods patient selection between january and april 2011 , 23 patients ( ten women and 13 men ; mean age , 59.3 years ; range , 1880 years ) unradiol med ( 2012 ) 117 : 13331346 introduzione il ricorso alla tomografia computerizzata ( tc ) ha subito un notevole incremento nel corso degli ultimi decenni grazie alle notevoli capacit diagnostiche raggiunte dai moderni tomografi e alla drammatica riduzione dei tempi di scansione ed elaborazione dei dati acquisiti . 
si stima , infatti , che la dose di radiazioni annuale derivante da procedure mediche ricevuta da ogni soggetto negli usa sia cresciuta di circa sei volte ( da 0 , 5 msv a 3 , 0 msv ) tra il 1980 e il 2006 [ 1 ]  . 
sebbene la dose media raggiunga un valore ancora simile a quello della radiazione naturale diffusa , si stima che soltanto luso della tc sia responsabile di circa il 2% di tutti i tumori diagnosticati negli usa [ 2 ]  . 
gli esami tc rappresentano il 15% degli esami radiologici effettuati ; ciononostante , la tc determina oltre due terzi della dose totale derivante dallimaging [ 3 , 4 ]  . 
il rischio cumulativo potrebbe essere anche maggiore , soprattutto in certe sottopopolazioni di pazienti , per esempio quelli che richiedono studi multifasici o controlli seriati oppure nei pazienti obesi e in quelli pediatrici . molte strategie di riduzione della dose sono state sviluppate e messe in atto con lobiettivo di mantenere una qualit dimmagine tale da non compromettere laccuratezza diagnostica dellesame tc [ 5 , 6 ]  . 
tra queste le pi efficaci sono : la modulazione automatica della corrente del tubo ( mas ) [ 7 ] , la riduzione dellintensit di corrente ( ma ) [ 8 ] e dellenergia del fascio ( kv ) [ 9 ] e unadeguata collimazione del fascio radiante . 
conseguenza diretta della riduzione di dose purtroppo un aumento del rumore e il sistema di ricostruzione attualmente in uso , la filtered back projection ( fbp ) non in grado di compensarlo . lalgoritmo di ricostruzione adaptive statistical iterative reconstruction ( asir ) consente di applicare i sistemi di riduzione della dose mantenendo una buona qualit dimmagine mediante una correzione del rumore effettuata con calcoli statistici ripetuti o iterativi [ 10 ]  . 
questo nuovo metodo viene usato in combinazione con la fbp in varie percentuali ; infatti , se utilizzato al 100% , tende a fornire unimmagine plastica , con unattenuazione insolitamente omogenea . alcuni recenti studi hanno indagato le potenzialit dellasir nello studio del distretto toracico [ 11 , 12 ] e delladdome [ 1316 ] , nellesame del cuore e nella colonscopia virtuale , fornendo utili indicazioni sullimpostazione tecnica degli esami diagnostici e sulle possibili limitazioni . 
obiettivo del nostro studio valutare la possibilit di applicare lalgoritmo di ricostruzione asir allo studio tc total - body a bassa dose con riduzione della tensione e dellintensit di corrente del tubo radiogeno . 
abbiamo inoltre confrontato la qualit diagnostica ottenuta con lutilizzo dellasir e della fbp . radiol med ( 2012 ) 117 : 13331346 1335 dergoing whole - body ct for oncological follow - up were enrolled at our department . 
all patients underwent contrastenhanced whole - body ct with a low - dose multiphase acquisition , with 40% of asir and parameters modulated according to body mass index ( bmi )  . 
patient demographic data ( sex and age ) and body habitus ( weight , height , bmi ) were collected and recorded ( table 1 )  . ct acquisition protocol with the asir algorithm all examinations were performed with a 64 - slice multidetector scanner ( lightspeed vct - 64 row asir , ge healthcare , milwaukee , wi , usa ) equipped with both the fbp and asir reconstruction algorithm , with the possibility of selecting asir percentage levels between 0% and 100% . 
in line with previous studies [ 13 , 15 ] and the manufacturers recommendations , a blend of 40% asir and 60% fbp was selected , which proved sufficient to reduce the noise of lowdose examinations to a value similar to that of abdominal ct with conventional dose and fbp . 
our initial evaluations indicated that this value is also well suited to the study of the chest . patients were divided into two groups based on their bmi , and tube parameters ( x - ray - beam energy , tube current ) were selected as follows : in patients with a bmi < 24 kg / m2 ( n = 12 ) , a peak of 100 kv was fixed and the tube current was automatically modulated by the manufacturers software ( aec , automatic exposure control , automa , ge healthcare ) ; in patients with a bmi24 kg / m2 ( n = 11 ) , a peak of 120 kv was set and the tube current was automatically modulated within a maximum threshold of 400 mas . the noise index value was also selected with the aid of the aec software , based on the percentage of dose reduction ( 40% ) , so as to select the most suitable value for the patients body habitus . 
a preliminary unenhanced ( baseline ) scan was carried out to evaluate the upper abdomen ( beam collimation , 5 mm ; gantry rotation speed , 0.5 s / rotation ; pitch , 55 mm / rotation ; 40 detectors )  . 
a thin - slice scan of the chest , abdomen and pelvis was then acquired in the portal phase ( 70to 80 - s delay ; beam collimation , 2.5 mm ; gantry rotation speed , 0.5 s / rotation ; pitch , 55 mm / rotation ; 40 detectors )  . 
in seven patients , a late phase was also acquired ( 150 s from contrast material injection ) with materiali e metodi selezione dei pazienti nel periodo compreso tra gennaio e aprile 2011 , presso il nostro dipartimento stato arruolato un totale di 23 pazienti ( 10 donne e 13 uomini , et media 59 , 3 anni , range 1880 anni ) nei quali lindicazione allesame era costituita da follow - up oncologico ( tabella 1 )  . 
tutti i pazienti hanno eseguito una tc total - body con mezzo di contrasto ( mdc ) con acquisizione multifasica a bassa dose , con 40% di asir e parametri modulati in base allindice di massa corporea ( imc ) , ovvero dividendo i pazienti in due gruppi , quelli con imc < 24 kg / m2 e quelli con imc24 kg / m2 . 
i dati demografici ( sesso ed et ) e riguardanti lhabitus dei pazienti ( peso corporeo , altezza , imc ) sono stati raccolti e registrati ( tabella 1 )  . protocollo di acquisizione tc con algoritmo asir tutti gli esami sono stati eseguiti su tomografo a 64 strati multidetettore ( lightspeed vct - 64 row asir , ge healthcare , milwaukee , wi , usa )  . 
in accordo con i risultati di precedenti studi [ 13 , 15 ] e secondo le raccomandazioni del costruttore , stata scelta una miscela con 40% di asir e 60% di fbp , che risultata idonea a ridurre il contenuto di rumore di un esame a bassa dose a un valore assimilabile a quello di uno studio tc delladdome con fbp a dose convenzionale . 
neither the study of the skull nor the late phase was included in the dosimetric evaluations . ct acquisition protocol with the fbp algorithm conventional - dose ct scans obtained with the fbp algorithm alone were performed with the same 64 - slice multidetector scanner 372 days earlier on average ( range , 159486 days )  . 
peak values of 120 kv were used , as x - ray beam energy and the tube current was automatically modulated using the same software supplied by the manufacturer . data analysis the value of the dose - length product ( dlp ) for each acquisition phase was derived from the dose report page , which is generated automatically at the end of ct scans and sent directly to the picture archiving and communication system ( pacs ) ( carestream health , rochester , ny , usa ) and was di riduzione della dose richiesta ( 40% ) , cos che fosse selezionato il valore pi idoneo allhabitus del paziente . 
stata eseguita una preliminare acquisizione senza mdc ( basale ) mirata alla valutazione delladdome superiore ( collimazione del fascio 5 mm ; velocit di rotazione del gantry 0 , 5 s / giro ; pitch 55 mm / rot ; 40 detettori )  . 
sono stati somministrati 120 cc di mdc organo - iodato ( iomeron 350 mgi / ml , bracco imaging , milano , italia ) seguiti da 40 cc di soluzione fisiologica , al flusso di 2 , 5 ml / s . 
stata quindi acquisita una scansione a strato sottile del torace , delladdome e della pelvi in fase portale ( 7080 s di ritardo ; collimazione del fascio 2 , 5 mm ; velocit di rotazione del gantry 0 , 5 s / giro ; pitch 55 mm / rot ; 40 detettori )  . 
in 7 pazienti stata acquisita una fase tardiva ( 150 s dalliniezione del mdc ) , mirata allapprofondimento di reperti individuati nelle fasi precedenti ; sono stati utilizzati gli stessi parametri di acquisizione della fase portale . 
sia lo studio del cranio che la fase tardiva non sono stati inclusi negli studi dosimetrici . protocollo di acquisizione tc con algoritmo fbp gli esami tc a dose convenzionale , ottenuti soltanto con lalgoritmo di ricostruzione fbp , erano stati eseguiti sulradiol med ( 2012 ) 117 : 13331346 1337 separately available for viewing every acquisition phase . 
 measurement accuracy performed by the scanner and displayed on the monitor was checked during quality control tests . the effective dose was calculated in millisievert from the dlp using the conversion factors approved by the american association of physicists in medicine and deriving from jessen and shrimptons studies [ 17 ] : 0.014 for the chest ; 0.012 for the abdomen ; 0.016 for the pelvis ( in msvmgy - 1 cm - 1 )  . we used the abdomen conversion factor for the precontrast phase , as well as the chest conversion factor , corresponding to the mean value of the three regions being studied , for the portal phase . 
two radiologists unaware of the scanning technique used for each image set jointly assessed image quality of low - dose and conventional - dose examinations , judging sharpness , noise level and presence of artefacts . 
 image sharpness , defined as margin definition of structures under examination , was rated on a scale from 1 to 5 ( 1 = poor ; 2 = suboptimal ; 3 = sufficient ; 4 = good ; 5 = optimal )  . 
 the presence of artefacts and their impact on image quality were quantified on a scale from 1 to 3 ( 1 = absent ; 2 = present but not affecting the diagnosis ; 3 = present and affecting diagnosis )  . 
both major ( ring , zebra , beam - hardening and motion ) and minor ( partial volume effects , spiral , streak due to cone beam ) artefacts were considered . 
image noise was also measured objectively by placing , in portalphase scans , two circular regions of interest ( roi ) of 15 mm2 , respectively , at the centre of the thoracic aorta ( in d7 ) and on the liver parenchyma ( anterior to the bifurcation of suprahepatic veins )  . 
mean density pixels sampled was measured in the roi , and the standard deviation ( sd ) in hounsfield units ( hu ) was considered an indicator of image noise . diagnostic quality was assessed on a likert scale from 1 to 3 ( 1 = poor ; 2 = sufficient ; 3 = good ) , both for lowand conventional - dose ct . 
a score of 1 was given if image quality was marred by excessive noise and major artefacts , with poor delineation of parenchymal margins , vascular structures , airways and excretory systea score of 2 was given if noise was average , without major artefacts and with sufficient delineation of margins . 
a score of 3 was assigned for good image quality with low or no noise , few or no minor lo stesso tomografo a 64 strati multidetettore mediamente 372 giorni prima ( range 159486 )  . 
 per lenergia del fascio radiante sono stati utilizzati valori di picco di 120 kv e la corrente del tubo stata modulata automaticamente utilizzando lo stesso software fornito dal produttore e descritto in precedenza . analisi dei dati il valore di dose - lenght product ( dlp ) per ogni singola fase di acquisizione stato ricavato dalla dose report page , che viene automaticamente generata alla fine dellesame tc e inviata direttamente al nostro sistema picture archiving and communication system ( pacs ) ( carestream health , rochester , ny , usa ) ed era disponibile separatamente per ogni fase di acquisizione . 
laccuratezza delle misurazioni effettuate dal tomografo tc e visualizzate sul monitor stata verificata durante i controlli di qualit . la dose effettiva in msv stata calcolata dal dlp , utilizzando i fattori di conversione approvati dallamerican association of physicists in medicine e derivanti dagli studi di jessen e shrimpton [ 17 ] : 0 , 014 per il torace ; 0 , 012 per laddome ; 0 , 016 per la pelvi ( in msvmgy - 1cm - 1 )  . per la fase pre - contrasto , stato utilizzato il fattore di conversione delladdome ; per la fase portale , stato scelto il fattore di conversione del torace , corrispondente al valore medio dei tre distretti esaminati . 
i dati sono stati registrati sia per lesame a bassa dose che per lesame a dose convenzionale e sono stati analizzati separatamente nei due gruppi di pazienti . tutti gli esami , sia quelli ottenuti con asir sia i controlli ottenuti con fbp , sono stati randomizzati , resi anonimi e visualizzati in parallelo ( precedente vs controllo ) su monitor ad alta risoluzione . 
due radiologi , che non erano a conoscenza della tecnica desame utilizzata per ogni singolo set dimmagini , hanno valutato in consensus la qualit dimmagine degli esami a bassa dose e di quelli a dose convenzionale , esaminando la nitidezza dellimmagine , il livello di rumore e la presenza di artefatti . 
la nitidezza dellimmagine , intesa come definizione dei margini delle strutture in esame , stata misurata con una scala da 1 a 5 ( 1 = scarsa ; 2 = sub - ottimale ; 3 = sufficiente ; 4 = buona ; 5 = ottima )  . 
la presenza di artefatti e il loro impatto sulla qualit dimmagine sono stati misurati con una scala da 1 a 3 ( 1 = assenti ; 2 = presenti ma senza influenza sulla diagnosi ; 3 = presenti e con influenza sulla diagnosi )  . 
the total effective dose ( msv ) and the dlp ( mgycm ) obtained by adding the contributions of each phase of ct scans obtained with the fbp and asir algorithms were compared using wilcoxons test . 
this analysis considered the total of examinations obtained with the asir protocol and the single subsets obtained with the asir protocol and tube voltages of 100 kv or 120 kv . 
we also compared mean density values and sd obtained at the level of the liver and aorta in scans obtained at voltages of 100 kv and 120 kv using the mannwhitney test . 
in examinations performed at 120 kv , the average reduction in effective dose was smaller ( 17.49% ) , although statistically significant ( p = 0.005 ) ( table 2 )  . 
analysis of variables used as indicators of image quality showed no statistically significant difference , with the exception of the noise level ( p = 0.001 ) , with significant difference in both patients subgroups ( 100 mi , artefatti striati da fascio conico )  . 
il livello di rumore soggettivamente rilevabile stato valutato con una scala da 1 a 5 ( 1 = assente ; 2 = scarso ; 3 = medio ; 4 = abbondante ; 5 = eccessivo )  . 
il rumore stato inoltre misurato in maniera oggettiva posizionando nelle scansioni in fase portale di ogni esame , due regioni di interesse ( region of interest , roi ) circolari delle dimensioni di 15 mm2 , rispettivamente al centro dellaorta toracica ( a livello di d7 ) e nel parenchima epatico ( anteriormente alla biforcazione delle vene sovraepatiche )  . 
in corrispondenza della roi stata rilevata la media della densit dei pixel campionati e la deviazione standard ( ds ) in unit hounsfield ( hu ) stata considerata indice del rumore dellimmagine . la qualit diagnostica stata infine valutata con lutilizzo di una scala di likert con punteggio da 1 a 3 ( 1 = scarsa ; 2 = sufficiente ; 3 = buona ) sia per la tc a bassa dose che per la tc a dose convenzionale . 
stato attribuito un punteggio pari a 1 se la qualit dimmagine era compromessa da eccessivo rumore e dalla presenza di artefatti maggiori , con scarsa delineazione dei margini dei parenchimi , delle strutture vascolari , delle vie aeree e delle vie escretrici . 
un punteggio pari a 3 stato infine assegnato in caso di buona qualit dimmagine con rumore scarso o assente , artefatti minori scarsi o assenti e buona delineazione dei margini delle strutture in esame . analisi statistica per lanalisi statistica dei dati stato utilizzato un software dedicato ( statistica release 7 , statsoft , tulsa , oklahoma )  . 
 i valori di dose effettiva ( msv ) e dlp ( mgycm ) totali degli esami tc , ottenuti dalla somma dei singoli contributi derivanti da ogni singola fase , eseguiti con algoritmo di ricostruzione fbp e asir sono stati posti a confronto tra loro usando il test di wilcoxon . 
inoltre , abbiamo provveduto a confrontare i valori di densit e di ds , espressi in hu , ottenuti a livello del fegato e dellaorta , tra gli esami acquisiti con algoritmo fbp e asir , usando sempre il test di wilcoxon.questo tipo di analisi stato condotto considerando sia il totale degli esami eseguiti con protocollo asir , sia considerando i singoli sottogruppi degli esami tc eseguiti con protocollo asir e differenza di potenziale del tubo pari a 100 kv e 120 kv . 
abbiamo inoltre messo a confronto le densit medie e le ds ottenute a livello del fegato e dellaorta tra gli esami eseguiti con tensione pari a 100 kv e pari a 120 kv , usando il test di mann - whitney . 
no statistically significant difference was found between density values ( average and sd ) in scans performed with the asir protocol at 100 kv and 120 kv ( table 5 )  . discussion in recent decades , ct has become widespread in all developed countries as the diagnostic technique of choice , thanks e limc usando il test di correlazione per ranghi di spearman . 
un valore di p < 0 , 05 stato considerato significativo . risultati la dose effettiva media somministrata con il protocollo asir stata di 15 , 65 msv e 21 , 85 , 3 msv con il protocollo standard fbp , con una riduzione media del 27 , 41% . 
la differenza tra i valori ottenuti con asir e fbp risultata statisticamente significativa ( p < 0 , 0001 ) , come pure la differenza del valore di dlp ( 1173380 mgycm vs 1652410 mgycm ; p < 0 , 001 ) ( tabella 2 )  . 
1a , b correlazione tra imc e dose effettiva ( espressa in msv ) somministrata negli esami eseguiti con filtered back projection ( fbp ) ( a ) e con adaptive iterative statistical reconstruction ( asir ) ( b )  . to its speed , ease of use and availability ; approximately one in five people in the usa are estimated to undergo a ct scan every year [ 18 ]  . 
its use , however , is not free from risks , and studies reveal that most patients and family doctors are not aware of them [ 18 , 19 ] , which results in an increased number of examinations with an unfavourable riskbenefit ratio and lower use of alternative , potentially less harmful , examination techniques . sottogruppi di pazienti che avevano effettuato lesame con una differenza di potenziale di 100 e 120 kv ha mostrato una maggior riduzione dei valori dosimetrici negli esami eseguiti a minor tensione , con riduzione media della dose effettiva pari al 42 , 83% ( 12 , 81 , 3 msv con asir e 22 , 84 , 7 msv con fbp , p = 0 , 008 )  . 
per gli esami eseguiti con differenza di potenziale pari a 120 kv , la riduzione media della dose effettiva stata inferiore ( 17 , 49% ) , seppur statisticamente radiol med ( 2012 ) 117 : 13331346 1341 fig . 
comparison between examination performed with filtered back projection ( fbp ) ( 120 kv , automatic mas ) ( a , b ) and adaptive iterative statistical reconstruction ( asir ) ( 100 kv , automatic mas ) ( c , d ) , with reconstructions in the axial ( a , c ) and coronal ( b , d ) planes . 
the most important are reducing scan times and extent ( use of the largest number of available detectors , higher pitch , fewer acquisition phases where clinically indicated ) and modulating x - ray - tube parameters ( beam collimation , peak voltage , current )  . 
 an innovative reconstruction algorithm known as asir has been introduced that , based on a statistical model of photon distribution and related electronic noise , corrects excessive signal fluctuations without limiting spatial resolution . 
in order to make the reconstruction process more efficient and rapid and to avoid excessive noise reduction making the image too feeble , with loss of anatomical detail , this system is used in combination with fbp . significativa ( p = 0 , 005 ) ( tabella 2 )  . 
non sono state rilevate differenze statisticamente significative tra i valori di densit ( media e ds ) ottenuti negli esami eseguiti con asir rispettivamente a 100 e 120 kv ( tabella 5 )  . reduction of the mean effective dose achieved with the use of the asir protocol used in combination with negli ultimi decenni , la tc si diffusa in tutti i paesi sviluppati come tecnica diagnostica delezione per la sua velocit , radiol med ( 2012 ) 117 : 13331346 1343 fig . 
comparison between examination obtained with filtered back projection ( fbp ) ( a , b ) and adaptive iterative statistical reconstruction ( asir ) ( 120 kv , automatic mas , maximum ma = 400 kv ) ( c , d ) , with reconstructions in the axial ( a , c ) and coronal ( b , d ) planes . 
 modulation of tube parameters ( pitch reduction , tube - intensity modulation and voltage reduction in normal - to - underweight patients ) was 27.41% on average , in line , though slightly lower , than reported by previous clinical studies on chest and abdominal ct ( range , 2544% ) [ 1113 , 15 ]  . 
this result may be explained by the small size and heterogeneity of our sample and by the great variability of the protocols applied in the studies available in the literature . 
in addition , examinations performed with fbp in our study benefited from the automatic current intensity modulation system , which resulted in a minimal dose reduction . we also confirmed a direct linear correlation between radiation dose and bmi ( r = 0.69 for examinations performed with asir and r = 0.52 for those performed with fbp ) , with a higher dose reduction ( 42.83% ) in the subset of patients with bmi < 24 kg / m2 [ 11 , 13 , 15 ]  . 
il suo utilizzo non tuttavia scevro da rischi e alcuni studi hanno rivelato che la maggior parte dei pazienti e dei medici di famiglia non ne sono consapevoli [ 18 , 19 ] , con un conseguente incremento del numero di esami con rapporto rischio / beneficio sfavorevole e un minor ricorso a tecniche desame alternative e potenzialmente meno dannose . parallelamente alle campagne di sensibilizzazione sui rischi derivanti dallincongruo utilizzo della tc , sono state proposte e applicate molteplici strategie di riduzione della dose degli esami effettuati . 
le principali sono rappresentate dalla riduzione dei tempi di scansione e della sua estensione ( utilizzo del maggior numero di detettori disponibili , aumento del pitch , riduzione delle fasi di acquisizione ove clinicamente indicato ) e dalla modulazione dei parametri relativi al tubo radiogeno ( collimazione del fascio , picco di 1344 radiol med ( 2012 ) 117 : 13331346 tensione e intensit di corrente )  . 
tutte queste soluzioni generano purtroppo un aumento del rumore delle immagini , che gli algoritmi di ricostruzione in uso e , in particolare , la fbp non sono in grado di compensare . 
 recentemente stato introdotto un innovativo algoritmo di ricostruzione delle immagini , lasir , che a partire da un modello statistico di distribuzione dei fotoni e del relativo rumore elettronico , corregge le fluttuazioni eccessive del segnale senza limitazioni della risoluzione spaziale . 
al fine di rendere pi efficiente e rapido il processo di ricostruzione , questo sistema viene utilizzato in combinazione con lfbp , anche per evitare uneccessiva riduzione del rumore che renderebbe limmagine troppo tenue con una perdita del dettaglio anatomico . nel nostro studio , infatti , il rumore risultato inferiore negli esami eseguiti con protocollo asir sia nelle valutazioni soggettive che nelle misurazioni oggettive effettuate . 
 negli esami eseguiti con protocollo asir non stata dimostrata alcuna differenza significativa tra quelli con 100 e con 120 kv e questo conforta lipotesi che la modulazione dei parametri del tubo debba essere adattata allhabitus del paziente per mantenere una qualit dimmagine sufficiente . la riduzione della dose media effettiva con lutilizzo dellasir , associato alla modulazione dei parametri del tubo ( riduzione del pitch , modulazione dellintensit del tubo e riduzione della differenza di potenziale nei pazienti normo - sottopeso ) , stata in media del 27 , 41% , in linea con i risultati di precedenti studi clinici sullesame tc del torace e delladdome [ 1113 , 15 ] , anche se di entit lievemente inferiore a questi ( range 2544% )  . 
non da ultimo , gli esami eseguiti con fbp beneficiavano , nel nostro studio , del sistema automatico di modulazione dellintensit di corrente , con una minima seppur presente riduzione della dose . abbiamo inoltre confermato una correlazione lineare diretta della dose con limc ( r = 0 , 69 per gli esami eseguiti con asir e r = 0 , 52 per gli esami eseguiti con fbp ) , con una riduzione della dose di maggiore entit ( 42 , 83% ) nel sottogruppo di soggetti con imc < 24 kg / m2 [ 11 , 13 , 15 ]  . 
 in alcuni studi la correlazione stata effettuata con il peso corporeo [ 12 , 16 ] , ma a nostro avviso tale parametro rispecchia in maniera meno precisa lhabitus dei pazienti e di conseguenza le differenti caratteristiche di attenuazione . 
la correlazione con limc risulta solo minimamente influenzata dalla diversa tecnica desame utilizzata nei pazienti , ovvero dal diverso picco di energia del tubo ( 100 vs 120 kv ) e si conferma infatti negli esami eseguiti con fbp . nonostante la differente dose somministrata nei due sottogruppi di pazienti , non si sono evidenziate differenze significative nella qualit dimmagine soggettivamente perfig.4a , b a 77 - year - old patient with a body mass index ( bmi ) of 27.5. 
 comparison between noise with adaptive iterative statistical reconstruction ( asir ) ( 120 kv , automatic mas , maximum ma = 400 kv ) ( a ) and with filtered back projection ( fbp ) ( b )  . 
confronto tra il rumore dellesame eseguito con asir ( 120 kv , mas automatici , ma massimo = 400 kv ) ( a ) e di quello eseguito con fbp ( b )  . 
 cepita , ove si eccettui una maggiore nitidezza degli esami eseguiti con asir nei pazienti che avevano eseguito lesame con picco di 120 kv , ovvero quelli con imc > 24 kg / m2 . 
bonomo2 1unit di risonanza magnetica , centro oncologico fiorentino , via attilio ragionieri 101 , 50119 sesto fiorentino , italy 2dipartimento di bioimmagini e scienze radiologiche , universit cattolica s . 
a number of noninvasive imaging modalities have been employed in viability identification , but contrast - enhanced magnetic resonance ( mr ) imaging has been shown to be extremely accurate because of its transmural resolution and precise definition of microvascular obstruction . 
at first mr examination , postcontrast images were analysed according to three patterns , based on a combination of first - pass and delayed - enhancement data : pattern 1 ( normal first pass and late hyperenhancement < 50% thickness ) identified viable myocardium , whereas pattern 2 ( late hyperenhancement > 50% thickness , with or without first - pass perfusion defect ) and pattern 3 ( perfusion defect at first pass and late hypoenhancement ) recognised nonviable myocardium , with 93% sensitivity , riassunto obiettivo . 
numerose metodiche di imaging non invasivo sono state utilizzate per lo studio della vitalit , ma tra queste la risonanza magnetica ( rm ) si dimostrata particolarmente accurata , grazie alla sua risoluzione transmurale e alla identificazione dellostruzione del microcircolo . 
quarantasei pazienti consecutivi con primo infarto acuto del miocardio e trattati con angioplastica coronarica percutanea ( ptca ) ( n = 40 ) o fibrinolisi ( n = 6 ) sono stati studiati con rm con mezzo di contrasto ( mdc ) , per definire edema , funzione , ostruzione del microcircolo e vitalit . 
considerando il pattern 1 ( iper - enhancement tardivo < 50% dello spessore , con primo passaggio normale ) come miocardio vitale , ed i pattern 2 ( iperenhancement tardivo > 50% dello spessore , con o senza difetto di perfusione al primo passaggio ) e 3 ( ipo - enhancement al primo passaggio e tardivo ) come radiol med ( 2012 ) 117 : 12941308 1295 75% specificity , 92% positive predictive value and 78% negative predictive value for identifying viable tissue . 
after acute mi , not all infarcts with transmurality > 50% can be considered nonviable ; microvascular obstruction detected at first pass can help to better stratify these cases . keywords acute myocardial infarction infarct size microvascular obstruction magnetic resonance imaging miocardio non vitale , si ottenuta una sensibilit del 92% , una specificit del 75% , un valore predittivo positivo del 93% ed un valore predittivo negativo del 78% nella identificazione della vitalit . 
negli infarti acuti , non tutti i segmenti con transmuralit maggiore del 50% mostrano mancato recupero contrattile , indice di non vitalit ; lanalisi del danno microcircolatorio al primo passaggio pu aiutare la corretta identificazione e stratificazione di questi casi . parole chiave infarto miocardico acuto infarct size ostruzione del microcircolo risonanza magnetica introduction introduzione identifying myocardial viability after acute myocardial infarction ( ami ) is a crucial point when defining prognosis and evaluating the efficacy of a revascularisation procedure . 
 it is well known that in patients with ischaemic cardiomyopathy , weakening of global contractile function is one of the main negative prognostic factors for long - term survival [ 1 , 2 ]  . 
both in acute and chronic ischaemia , it is of pivotal relevance to identify viable but functionally depressed ( stunned or hibernated ) myocardial zones that are capable of recovery after effective revascularisation therapy . 
 noninvasive modalities used to determine myocardial viability include positron - emission tomography ( pet ) , singlephoton - emission computed tomography ( spect ) , dobutamine echocardiography ( ecg ) and contrast - enhanced ( ce ) echo . 
 besides fulfilling this requisite , magnetic resonance imaging ( mri ) allows different approaches to myocardial viability [ infarct size quantification , contractile reserve definition , first - pass ( fp ) perfusion study ]  . 
 moreover , the meaning of different myocardial enhancement patterns obtained when combining fp and delayed enhancement ( de ) ( 1015 min after contrast administration ) studies is also a matter of debate . the purpose of this study was to evaluate the capability la valutazione della vitalit miocardica rappresenta un fattore cruciale nella stratificazione prognostica dopo infarto acuto del miocardio ( ami ) e nella valutazione dellefficacia delle procedure di rivascolarizzazione . 
 ben noto che nei pazienti con cardiopatia ischemica la riduzione della funzione contrattile globale uno dei principali fattori prognostici negativi per la sopravvivenza a lungo termine [ 1 , 2 ]  . 
nellischemia sia acuta che cronica di rilevanza fondamentale individuare quelle zone del miocardio che sono vitali ma funzionalmente depresse ( stordite o ibernate ) e capaci di recupero dopo una efficace terapia di rivascolarizzazione . 
 numerose sono le modalit non invasive utilizzate per determinare la vitalit miocardica : la tomografia ad emissione di positroni ( pet ) , la tomografia computerizzata ad emissione di singolo fotone ( spect ) , lecocardiografia con dobutamina , e la ecocardiografia con contrasto . 
queste modalit sono di provata utilit clinica , ma ciascuna di esse ha limiti conosciuti , che ne penalizzano laccuratezza diagnostica : il loro principale svantaggio rappresentato dalla scarsa capacit di determinare esattamente lentit transmurale del danno miocardico . oltre a soddisfare questo requisito , la risonanza magnetica ( rm ) consente la valutazione di diversi parametri correlati allinfarto e alla vitalit miocardica quali quantificazione dellinfarct size , definizione della riserva contrattile , valutazione del danno del microcircolo , quantificazione del miocardio salvabile , coinvolgimento del ventricolo destro . 
 in ogni caso , leffettivo ruolo prognostico di ciascuno degli elementi suddetti ancora discusso ; inoltre , il significato dei diversi pattern di enhancement miocardico ottenuto quando si combinano studi di primo passaggio e studi di imaging 1296 radiol med ( 2012 ) 117 : 12941308 of ce - mri to predict segmental functional recovery after ami with special focus on the role of microvascular damage ( no reflow ) and infarct transmurality . materials and methods study population forty - six patients ( mean age 658 years ) with first mi , defined with ecg criteria and twofold increase of serum creatine phosphokinase isoenzyme mb ( cpk - mb ) , were enrolled through the cardiology department of our university and underwent ce - mri 57 days after the acute event . 
patients were evaluated again with ce - mri after 46 months to assess functional recovery . mri protocol both acute and chronic mr studies were performed on a 1.5 - t scanner ( signa excite ii , ge healthcare , milwaukee , wi , usa )  . 
delayed imaging was obtained with irfgre sequences on 912 short - axis slices 15 min after a second equivalent contrast dose administered at the end of the perfusion sequence ( total dose 0.2 mmol / kg )  . 
in the former case , the optimal inversion time was chosen through a dedicated look - locker cine ir sequence ; in the latter case , ritardato ( delayed enhancement , 1015 minuti dopo la somministrazione di contrasto ) , ancora materia di dibattito . lo scopo di questo studio valutare la capacit delle sequenze contrastografiche ( ce - mri ) di predire il recupero funzionale segmentale dopo infarto miocardico acuto , con particolare attenzione al ruolo del danno del microcircolo ( no - reflow ) e della transmuralit dellinfarto . materiali e metodi popolazione dello studio attraverso il dipartimento di cardiologia del nostro policlinico abbiamo arruolato 46 pazienti ( media 658 anni ) con primo infarto miocardico acuto [ definito con criteri basati sullelettrocardiogramma ( ecg ) e aumento duplice del valore sierico della creatinfosfochinasi del muscolo cardiaco ( cpk - mb ) ] ; tali pazienti a 57 giorni dallevento acuto sono stati sottoposti ad esecuzione di ce - mri . 
39 pazienti avevano infarto acuto anteriore , 4 pazienti infarto inferiore e 3 pazienti infarto laterale ; tutti i pazienti sono stati sottoposti a terapia di rivascolarizzazione , 40 dei quali con angioplastica coronarica percutanea ( ptca ) primaria , i 6 rimanenti con trombolisi . 
i pazienti sono stati esaminati di nuovo con ce - mri dopo 46 mesi , per valutare il recupero funzionale . protocollo mri abbiamo eseguito gli studi rm sia in fase acuta che in followup su uno scanner da 1 , 5 t ( signa excite ii , ge healthcare , milwaukee , wi , usa )  . 
il protocollo di imaging includeva una sequenza t2 pesata , lo studio di primo passaggio / perfusione durante somministrazione di gadolinio - acido penata - acetico dietilenetriamine ( gd - dtpa ) endovena ( ev ) , uno studio funzionale e uno studio di delayed enhancement a 15 minuti dopo la somministrazione del contrasto . 
lo studio di perfusione stato ottenuto con sequenze saturation recovery prep - fast gradient echotrain durante somministrazione ev di 0 , 1 mmol / kg di gd - dtpa con flusso 3 ml / s , seguito da 20 ml di soluzione fisiologica : abbiamo acquisito 3 sezioni ( basale , medio ventricolare ed apicale ) in asse corto . 
lo studio di delayed enhancement stato ottenuto con sequenze ir - prep fgre acquisendo 912 sezioni in asse corto , 15 minuti dopo una seconda dose equivalente di contrasto , somministrato al termine della sequenza di perfusione ( totale dose = 0 , 2 mmol / kg )  . 
particolare cura stata prestata per fare in modo tale che ci fosse la perfetta sovrapposizione delle tre sezioni acquisite nello studio di primo passaggio con tre sezioni delle 912 sezioni dello studio di delayed enhancement . 
fp hypoenhancement was defined as absent or present in each segment ; de was visually graded in each segment with a semiquantitative score depending on its transmural extent ( 0 = normal ; 1 = 125% ; 2 = 2650% ; 3 = 5175% ; 475% )  . 
a total of 736 segments were classified according to both fp and de as : pattern 1 : normal fp , absent or < 50% de ; pattern 2a : de transmurality > 50% , without fp hypoenpattern 2b : de transmurality > 50% , with fp hypoenpattern 3 : persisting hypoenhancement even at delayed hancement ; hancement ; imaging . del tempo di ripetizione utilizzato ( ogni rr o ogni due intervalli rr ) , la scelta del tempo di inversione stata differente : nel primo caso , il tempo di inversione ottimale stato scelto attraverso una sequenza dedicata look - locker ( cine - ir ) ; nel secondo caso stato utilizzato un tempo di inversione standard ( 325 ms ) , fornendo in tutti i casi un contrasto ottimale tra miocardio infartuato e miocardio sano . analisi dei dati rm tutte le immagini ottenute sono state esaminate da due radiologi esperti in rm cardiovascolare e valutate mediante un modello a 16 - segmenti del ventricolo sinistro dellamerican heart association ( aha )  . 
la cinetica regionale stata visivamente valutata con il wall motion score index ( wmsi : 0 = normale , 1 = ipocinetico ; 2 = acinetico ; 3 = discinetico )  . 
il difetto di perfusione allo studio di primo passaggio ( fp ) stato definito come assente o presente in ogni segmento ; il delayed enhancement ( de ) stato visivamente classificato in ogni segmento con un punteggio semiquantitativo a seconda della sua estensione transmurale ( 0 = normale ; 1 = 1%25% ; 2 = 26%50% ; 3 = 51%75% ; 475% )  . 
settecentotrentasei segmenti sono stati classificati , in base sia al fp che al de come : pattern 1 : iper - enhancement tardivo assente o < 50% dello spessore , con primo passaggio normale ; 1298 radiol med ( 2012 ) 117 : 12941308 a further 828 segments from the slices not included in the fp study were evaluated only at delayed imaging and classified according only to de as : pattern 1 : normal or de transmurality < 50% ; pattern 2 : de transmurality > 50% ; pattern 3 : persisting hypoenhancement . distribution of different patterns is reported in figure 1 . patterns 2 ( including subpatterns 2a and 2b ) and 3 were defined as nonviable , whereas pattern 1 was considered as being associated with functional recovery at follow - up . 
the segmental function scores were compared to the follow - up scores , and special care was taken to make the acute and follow - up studies overlap as closely as possible . 
functional recovery was defined as wmsi improvement compared with the acute study . statistical analysis mri data were entered onto a spreadsheet ( excel 2003 , microsoft , redmond , wa , usa ) to calculate the frequency distribution of functional recovery for each pattern . 
frequency distribution for patterns and segmental recovery were analysed with 2and fisher tests with a commercial software package ( medcalc version 7.6 , medcalc software , mariakerke , belgium ) to evaluate its statistical significance . 
1 distribuzione dei segmenti vitali e non vitali nei tre pattern . pattern 2a : iper - enhancement tardivo > 50% dello spessore , senza ipo - enhancement al fp ; pattern 2b : iper - enhancement tardivo > 50% dello spessore , con ipo - enhancement al fp ; pattern 3 : persistente ipo - enhancement , anche nella immagini de . ulteriori 828 segmenti relativi alle sezioni non comprese nello studio fp sono stati valutati solo nelle immagini de e classificati , solo secondo il de , come : pattern 1 : normale o iper - enhancement tardivo < 50% ; pattern 2 : iper - enhancement tardivo > 50% ; pattern 3 : persistente ipo - enhancement . nella figura 1 riportata la distribuzione dei differenti pattern . il pattern 2 ( compresi i sub - pattern 2a e 2b ) ed il pattern 3 sono stati definiti come non vitali , mentre il pattern 1 stato considerato come associato al recupero funzionale al followup . 
gli score della funzione segmentale sono stati confrontati con gli score al follow - up e particolare attenzione stata prestata affinch lo studio in fase acuta si sovrapponesse il pi possibile a quello di follow - up . 
il recupero funzionale stato definito come miglioramento del wmsi , rispetto allo studio in fase acuta . analisi statistica i dati rm sono stati riportati su un foglio elettronico ( excel 2003 , microsoft , redmond , wa , usa ) , utilizzato per calcolare la distribuzione di frequenza del recupero funzionale per ciascun pattern ; inoltre sono stati calcolati sensibilit , specificit , valori predittivi positivi e negativi per ciascuna sequenza di ce - mri per predire il recupero funzionale segmentale . 
la distribuzione di frequenza per i vari pattern e per il recupero segmentale stata analizzata con il test del chi - quadro ed il fisher test mediante un software commerciale ( medcalc versione 7.6 , medcalc software , mariakerke , belgio ) per valutarne la significativit statistica . 
il pattern 3 stato osservato in 132 segmenti , e tra questi , solo 9 ( 6 , 82% ) hanno mostrato un minimo di recupero funzionale al follow - up . 
il pattern 2 stato osservato in 265 segmenti : 187 segmenti non erano vitali al follow - up , mentre 78 hanno mostrato recupero funzionale ( 29 , 43% )  . 
la distribuzione di frequenza tra i diversi pattern ed il recupero funzionale risultata statisticamente significativa ( 2 = 757 , 37 ; p < 0 , 0001 )  . considerando il pattern 1 come predittivo del recupero funzionale ed i pattern 2 e 3 come espressione di necrosi miocardica , lo studio ce - mri ha correttamente previsto il recupero funzionale in 1065 segmenti su 1167 segmenti ; il mancato recupero funzionale stato correttamente previsto in 310 su 397 segmenti . 
 i 736 segmenti valutati sia allo studio di perfusione che allo studio de sono stati analizzati separatamente per determinare il ruolo dellipo - enhancement nelle sequenze fp nel recupero funzionale . 
il pattern 2a ( iper - enhancement tardivo > 50% dello spessore , senza difetto di perfusione al primo passaggio ) stato riscontrato in 42 pazienti ; di tali segmenti , 23 ( 54 , 8% ) non hanno mostrato recupero funzionale . 
lipo - enhancement al primo passaggio stato associato ad un rischio relativo di 1 , 39 per mancato recupero rispetto ai segmenti con il solo iper - enhancement tardivo > 50% . 
first - pass study ( a ) shows a perfusion defect in the lateral wall of the left ventricle , with involvement of the anterior papillary muscle ( arrowhead )  . 
il primo passaggio ( a ) mostra un difetto di perfusione nella parete laterale del ventricolo sinistro , con interessamento del muscolo papillare anteriore ( testa di freccia )  . 
in five segments in four patients , delayed imaging showed persisting hypoenhancement without any appreciable alteration at perfusion study . discussion hyperenhancement after contrast - medium administration in mi is a well - known finding [ 3 , 4 ] related to the extracellular nature of traditional mr contrast agents and to their ne di frequenza dei segmenti vitali tra i sub - pattern 2a e 2b risultata statisticamente significativa ( p = 0 , 0229 ) ( tabella 3 )  . 
perfusion and delayed imaging show pattern 2b ( a first - pass defect and b delayed enhancement > 50% ) in the midventricular anterolateral wall ; pattern 2a ( delayed enhancement > 50% without first - pass defect ) is present in the inferolateral wall , with the enhanced area becoming thinner in the apical lateral wall . 
il primo passaggio ed il delayed enhancement mostrano un pattern 2b ( difetto di perfusione , a e delayed enhancement > 50% , b ) in corrispondenza della parete antero - laterale medio - ventricolare ; nella parete infero - laterale si osserva un pattern 2a ( delayed enhancement > 50% , senza difetto di perfusione al primo passaggio ) , con assottigliamento parietale in sede laterale apicale . 
i frame telediastolico ( c ) e telesistolico ( d ) mostrano disfunzione contrattile nei medesimi segmenti , con mancato recupero funzionale al follow - up nei segmenti con pattern 2b e lieve miglioramento nei segmenti con pattern 2a ( e telediastole , f telesistole )  . 
 first pass first pass + kappa coefficient discussione persistent hypo persistent hypo + 559 107 0.464 hypo - , absence of persistent hypoenhancement ; hypo + , presence of persistent hypoenhancement tabella 4 lo studio di primo passaggio pi sensibile del delayed enhancement nella identificazione delostruzione microvascolare . 
lagreement tra i due approcci solo moderato primo passaggio passaggio + primo hypo persistente hypo + persistente 559 107 0 , 464 hypo - , assenza di ipoenhancement persistente ; hypo + , presenza di ipoenhancement persistente increased distribution volume in infarcted area voxels due to ruptured cellular membranes [ 35 ]  . 
de is found even in chronic infarction due to increased contrast distribution volume between collagen fibres of scarred tissue and to reduced capillary density [ 8 , 9 ]  . 
several authors also demonstrated a close agreement between de and pathology data [ 7 , 8 , 1012 ] : even though initial reports of some overestimation of the necrotic area by ce - mri were mainly attributed to partial volume effects [ 11 , 13 , 14 ] , the hypothesis that the enhanced area could partly represent some viable myocardium is still debated [ 15 , 16 ]  . 
 discrepancies between the different imaging modalities have partly to be ascribed to methodological factors ; to the possible incomplete overlap between animal and human studies ; and to technical factors such as time elapsed between contrast administration and delayed imaging , sequence parameters , or postprocessing techniques used to quantify the enhanced area [ 6 , 12 ]  . keeping a fixed inversion time , the enhanced area tends to vary with time due to continuous contrast diffusion [ 17 ]  . 
 furthermore , the correlation between pathological necrosis and the enhanced area tends to vary depending on duration of ischaemia , possibly due to a viable border zone , with increased gd distribution volume in less prolonged ones . 
finally , a double gd - dtpa dose ( 0.2 mmol / kg ) is liper - enhancement dopo somministrazione di mezzo di contrasto ( mdc ) nellinfarto del miocardio di ben noto riscontro [ 3 , 4 ] , ed legato alla natura extra - cellulare dei tradizionali mezzi di contrasto in rm ed al loro maggiore volume di distribuzione nei voxel dellarea infartuata , a causa della rottura delle membrane cellulari [ 35 ]  . 
un altro meccanismo in questione la riduzione del wash - out del contrasto da parte della rete dei capillari e dei vasi linfatici nelle aree necrotiche [ 6 , 7 ]  . 
il delayed enhancement si osserva anche nellinfarto cronico , a causa dellaumento del volume di distribuzione del mezzo di contrasto tra le fibre collagene nel tessuto cicatriziale ed alla riduzione della densit capillare [ 8 , 9 ]  . 
diversi autori hanno poi dimostrato una stretta correlazione tra il delayed enhancement ed i dati anatomo - patologici [ 7 , 8 , 1012 ] : sebbene i dati iniziali di minima sovrastima dellarea necrotica con le sequenze ce - mri siano stati attribuiti principalmente ad effetti di volume parziale [ 11 , 13 , 14 ] , lipotesi che parte dellarea di iper - enhancement in fase acuta potrebbe in parte rappresentare miocardio vitale ancora dibattuta [ 15 , 16 ]  . le discrepanze osservate tra diverse modalit di imaging vanno in parte attribuite a fattori metodologici , alla difficile riproducibilit dei modelli sperimentali animali e degli studi sullessere umano e soprattutto a fattori tecnici , come il tempo intercorso tra la somministrazione di contrasto e lacquisizione delle sequenze de , i parametri delle sequenze o le tecniche di post - processing utilizzate per quantificare larea di iper - enhancement [ 6 , 12 ]  . mantenendo un tempo fisso di inversione , larea di iperenhancement tende a variare nel tempo a causa della continua diffusione del contrasto [ 17 ]  . 
inoltre , la correlazione tra la necrosi patologica e larea di iper - enhancement tende a variare a seconda della durata di ischemia , forse a causa di un zona di confine di tessuto vitale con maggiore volume di distribuzione di gd in caso di ischemia meno prolungata . 
infine , una doppia dose di gd - dtpa ( 0 , 2 mmol / kg ) raccomandata per permettere , tra i 6 ei 16 minuti , un miglior contrasto tra il miocardio con enhancement ed il miocardio senza enhancement [ 18 ]  . 
risultati simili sono stati ottenuti con una dose standard ( 0 , 1 mmol / kg ) di mezzo di contrasto a maggior relassivit t1 , come il gadobenato dimeglumina ( gd - bopta ) [ 19 , 20 ]  . le zone di ipo - enhancement tra le aree di enhancement possono essere riscontrate nelle sequenze de non solo negli infarti non completamente riperfusi , ma anche laddove la perviet dellarteria coinvolta stata completamente ripristinata e dimostrata angiograficamente [ 4 , 21 , 22 ] : in questultimo caso , questo dato dovuto al cosiddetto fenoradiol med ( 2012 ) 117 : 12941308 1303 fig . 
the same area is clearly dysfunctional when comparing the end - diastolic ( e ) and end - systolic ( f ) frames of the cine magnetic resonance imaging sequence . 
4a - h infarto miocardico acuto ( pattern 3 ) : difetto di perfusione persistente al primo passaggio ( a ) e al delayed enhancement ( b ) in corrispondenza del setto anteriore . 
al follow - up ( g telediastole , h telesistole ) si evidenzia netto assottigliamento antero - settale e mancato recupero contrattile . 1304 radiol med ( 2012 ) 117 : 12941308 reported to allow , between 6 and 16 min , a better image contrast between enhanced and nonenhanced myocardium [ 18 ]  . 
similar results were obtained with a standard dose ( 0.1 mmol / kg ) of a contrast agent with higher t1 relaxivity , such as gdbenzyloxy - propionic tetraacetic acid ( bopta ) [ 19 , 20 ]  . dark zones between enhanced areas can be found at delayed imaging not only in incompletely reperfused infarctions but even if the patency of the culprit artery has been angiographically proven [ 4 , 21 , 22 ]  . 
persistent capillary obstruction in the infarcted area due to several pathological mechanisms [ 23 ] ( microembolisation , cellular debris , blood - cell plugging , endothelial protrusions ) is thought to prevent arrival of the contrast agent in some parts of the infarcted area , thus determining persistently hypoenhanced zones . 
these data are confirmed by the correspondence between these areas and those of flow reduction measured with microparticles [ 7 ]  . the no - reflow phenomenon has a definite dynamic and progressive course : in canine models , its extent is reported to grow in the first 48 h and then stabilise [ 10 , 24 ]  . 
furthermore , its effective conspicuity is strictly related to the progressive diffusion of contrast agent through collateral vessels and neighbouring interstitial space : this way , the fp perfusion study seems to be the most accurate choice for evaluating the microvascular bed . 
recently introduced ultrafast sequences , with mixed gre echoplanar acquisition , make possible to combine high temporal resolution with whole - ventricle coverage in the fp study , maintaining a high correlation with microsphere - measured perfusion [ 25 ]  . 
parallel imaging and b - ssfp sequences for fp studies [ 26 ] seem to further improve signal to noise ratio and image quality and to reduce artefacts . even though lund et al . 
lostruzione capillare persistente nella zona infartuata , a causa dei diversi meccanismi patologici [ 23 ] ( microembolizzazione , detriti cellulari , aggregazione piastrinica , protrusioni endoteliali ) si pensa che possa impedire larrivo di contrasto in alcune parti della zona infartuata , determinando in questo modo levidenza di zone con persistente ipo - enhancement : questi dati sono confermati dalla corrispondenza tra queste aree e quelle con riduzione del flusso misurato con microparticelle [ 7 ]  . 
 il fenomeno del no - reflow ha un definito decorso dinamico e progressivo : nei modelli canini , si dimostrato che la sua estensione pu aumentare nelle prime 48 ore e poi si stabilizza [ 10 , 24 ]  . 
inoltre , la sua effettiva cospicuit sarebbe strettamente legata alla diffusione progressiva del contrasto attraverso i vasi collaterali ed il vicino spazio interstiziale : di conseguenza , lo studio di perfusione fp sembra essere la metodica pi accurata per valutare il letto microvascolare . 
 lintroduzione recente di sequenze ultra - fast , con acquisizione ibrida gradient - echo ed echo planare , permette di combinare lalta risoluzione temporale con la copertura dellintero ventricolo nello studio di primo passaggio , mantenendo una elevata correlazione con la perfusione valutata con le microsfere [ 25 ] ; limaging parallelo e le sequenze b - ssfp per lo studio di primo passaggio [ 26 ] sembrano migliorare ulteriormente il rapporto tra segnale e rumore ( snr ) e la qualit dimmagine riducendo gli artefatti . 
 [ 29 ] hanno riportato che lostruzione microvascolare dimostrata con la risonanza magnetica associata , a prescindere dallestensine delarea infartuale , con una pi elevata incidenza di complicanze cardiovascolari al follow - up ; in altri lavori , lostruzione microvascolare associata ad un rimodellamento ventricolare positivo e ad un recupero funzionale globale inferiore [ 29 , 32 , 33 ]  . 
possibile che le zone con grave danno microvascolare potrebbero avere una compliance ridotta in qualche modo , ad esempio determinando sia un aumento di stress sulla parete miocardica vicina , sia lo stretching delle zone infartuate [ 13 , 34 ]  . il ruolo relativo del fenomeno di no - reflow e del delayed enhancement nella previsione del recupero funzionale amradiol med ( 2012 ) 117 : 12941308 1305 is associated with unfavourable ventricular remodelling and lower global functional recovery [ 29 , 32 , 33 ]  . 
it is possible that zones with severe microvascular damage could somehow have a reduced compliance , determining both increased wall stress on neighbouring myocardium and stretching of the infarcted areas [ 13 , 34 ]  . the relative roles of the no - reflow phenomenon and de in predicting functional recovery are widely debated and controversial , mostly as a result of technical and methodological differences between series . 
 [ 15 , 16 ] , obtained in two different series of patients with first mi , suggest both a possible functional recovery in segments with de and the association between fp hypoenhancement and less frequent functional recovery . 
in different series [ 3537 ] , fp hypoenhancement reaches high specificity values for persistent dysfunction ; however , its absence has reduced sensitivity ( 19% ) , greatly underestimating nonviable myocardiu this could be possibly due to reversible no reflow or to necrotic myocardium with undamaged microvascular network , especially in patients with postprocedural grade 3 timi flow . 
moreover , considering the endoepicardial progression of the ischaemic wavefront , functional recovery is obviously more unlikely with growing infarct and de transmurality , becoming very rare when the infarcted area involves > 75% of the myocardial wall [ 35 , 3840 ]  . 
 furthermore , they found a statistically significant difference ( p < 0.001 ) between enhanced segments with transmural extent 75% ( 44% showed recovery ) and those with transmural extent > 75% ( functional improvement in only 8% )  . 
among those segments , neither fp nor dobutamine stress studies had a significant impact in identifying viable segments . in the first place , our data confirm the role of the transmural extent of de in segmental functional recovery . 
i risultati del gruppo di rogers e kramer [ 15 , 16 ] , ottenuti in due diverse serie di pazienti con primo infarto del miocardio suggeriscono che sia possibile il recupero funzionale in segmenti con delayed enhancement , cos come lassociazione tra lipo - enhancement al primo passaggio ed un minor frequente recupero funzionale . 
in diversi studi [ 3537 ] lipo - enhancement al primo passaggio raggiunge valori di alta specificit per la disfunzione persistente ; tuttavia la sua assenza ha una sensibilit ridotta ( 19% ) , pertanto sottostimando fortemente le zone di miocardio non vitale . 
ci potrebbe essere forse dovuto ad un no - reflow reversibile oppure a miocardio necrotico ma con rete microvascolare non danneggiata ( specialmente in pazienti con flusso timi 3 post - procedurale )  . 
 inoltre , considerando la progressione endo - epicardica del fronte ischemico , il recupero funzionale ovviamente molto meno probabile quanto pi aumenta linfarto e la transmuralit del de , diventando molto raro quando la zona infartuata coinvolge pi del 75% della parete miocardica [ 35 , 3840 ]  . 
 [ 40 ] , il mancato de risultato essere il parametro pi affidabile nel prevedere il recupero funzionale [ 56 segmenti su 61 ( 92% ) , p < 0 , 05 ] : inoltre , gli stessi autori hanno evidenziato una differenza statisticamente significativa ( p < 0 , 001 ) tra i segmenti con enhancement con estensione transmurale inferiore al 75% ( 44% ha mostrato di recupero ) e quelli con estensione transmurale di oltre il 75% ( miglioramento funzionale pari all8% )  . 
tuttavia , non vi era una differenza statisticamente significativa in termini di probabilit di recupero tra i segmenti con de con estensione transmurale del 1%25% , 26%50% e 51%75% : inoltre , tra questi segmenti , n lo studio first pass n lo studio con stress dobutaminico hanno comportato un impatto significativo nellidentificazione dei segmenti vitali . in primo luogo , i nostri dati confermano il ruolo dellestensione transmurale del delayed enhancement nel prevedere il recupero funzionale segmentale . 
assumendo il pattern 1 ( iper - enhancement tardivo assente o < 50% dello spessore ) come miocardio vitale ed i pattern 2 ( iper - enhancement tardivo oltre il 50% ) e 3 ( ipo - enhancement persistente ritardato ) come miocardio necrotico , la risonanza magnetica con contrasto ha raggiunto il 93% di sensibilit ed il 91 , 9% di valore predittivo positivo nella identificazione del miocardio vitale . 
this type of pattern , evaluated by a few authors only [ 15 , 16 , 30 ] , is likely due to myocardium with high - grade microvascular damage , as they are unreachable by the contrast agent even through collateral diffusion . 
the presence of myocardial oedema in early postinfarction , especially after a revascularisation procedure with ptca , could explain de even in areas that are at least partially composed of viable myocardiu in this setting , the fp perfusion study could be a valuable tool in defining segments that are most likely to recover from segments that are not . 
in our series , nonviable segments were more frequently found in subpattern 2b : perfusion defects were associated with 1.39 relative risk of failed recovery ( 39% more than segments with transmural de but without fp hypoenhancement )  . 
such data confirm that the fp perfusion study , together with delayed imaging , can play a primary role in predicting functional recovery after ami , improving the specificity and diagnostic potential of ce - mri . study limitations there are some possible limitations that have to be taken into account when evaluating the findings of this study : recupero funzionale veramente bassa . 
per le stesse ragioni , limaging tardivo sembra di solito sottostimare il danno microvascolare , mostrando solo le aree pi critiche : questa affermazione confermata dal maggior numero di segmenti con ipo - enhancement al primo passaggio e dalla bassa concordanza tra lo studio di primo passaggio e limaging tardivo . 
tuttavia , la maggiore concordanza riportata in quello studio tra fp e imaging tardivo probabilmente dovuta a fattori tecnici : la valutazione della perfusione effettuata in tali lavori era limitata ad una sola sezione e questo probabilmente ha portato ad una sottostima della cospicuit dei difetti di primo passaggio . 
anche nel nostro studio abbiamo individuato 5 segmenti con normale primo passaggio e ipo - enhancement ritardato : questo dovuto principalmente ad uno studio di perfusione sub - ottimale ; inoltre , teoricamente possibile che i piccoli difetti di perfusione subendocardici possano essere stati trascurati a causa della bassa risoluzione delle sequenze di primo passaggio . 
 ci sembra confermare la possibilit di una sovrastima del miocardio necrotico da parte dellimaging tardivo : la presenza di edema del miocardio in fase postinfartuale precoce , soprattutto dopo una procedura di rivascolarizzazione con ptca , potrebbe spiegare lenhancement tardivo anche in aree che sono almeno in parte costituite da miocardio vitale . 
in questa maniera , lo studio di primo passaggio potrebbe essere un valido strumento per definire i segmenti che hanno pi probabilit di recuperare rispetto a quelli che non la hanno . 
nel nostro studio abbiamo riscontrato pi frequentemente segmenti non vitali nel sub - pattern 2b : i difetti di perfusione sono associati ad un rischio relativo di 1 , 39 di mancato recupero funzionale ( 39% in pi segmenti con de transmurale ma senza ipo - enhancement al first pass )  . 
 [ 41 ] : questi autori hanno dimostrato che , tra i segmenti con un iper - enhancement tardivo di oltre il 50% , la presenza di un difetto di perfusione al first pass con estensione transmurale di oltre il 50% fortemente associata ad un mancato recupero funzionale ( 90 , 9% dei segmenti )  . 
tali dati confermano che la perfusione valutata mediante lo studio di primo passaggio , insieme alle sequenze di delayed enhancement , possa giocare un ruolo primario nella previsione del recupero funzionale dopo infarto miocardico acuto , migliorando la specificit e le potenzialit diagnostiche delle tecniche di ce - mri . limiti dello studio ci sono alcune possibili limitazioni che devono essere prese in considerazione quando si valutano i risultati di questo studio : in particolare , la valutazione visiva dellestensione transmurale di fp , de e del recupero funzionale potrebbero aver influenzato i nostri risultati . 
luso di sequenze b - ssfp radiol med ( 2012 ) 117 : 12941308 1307 visual evaluation of the transmural extent of fp , de and functional recovery could have affected our results . 
the use of b - ssfp sequences [ 26 ] and quantitative or semiquantitative evaluation [ 42 ] of perfusion data could contribute to further clarify the role of the fp study in evaluating functional recovery after ami . 
this improved approach could further increase the reliability of ce - mri in evaluating functional recovery . [ 26 ] e la valutazione quantitativa o semiquantitativa [ 42 ] dei dati di perfusione potrebbe contribuire a chiarire ulteriormente il ruolo dello studio di primo passaggio nella valutazione del recupero funzionale dopo infarto miocardico acuto . 
inoltre , in questo studio , lestensione dei difetti di perfusione di primo passaggio non stata presa in considerazione : questo miglior approccio potrebbe ulteriormente aumentare laffidabilit degli studi di ce - mri nella valutazione del recupero funzionale . conclusions ce - mri has a high sensitivity and good specificity in identifying viable myocardium after ami . 
fp perfusion study allows a better evaluation of the microvascular network , identifying segments that will more rarely show signs of functional recovery . conclusioni le sequenze ce - mri hanno alta sensibilit e buona specificit nellidentificazione del miocardio vitale dopo infarto miocardico acuto . 
il delayed enhancement con estensione transmurale di oltre il 50% non necessariamente indicativo di miocardio non vitale , ma a volte pu essere associato ad un miglioramento della contrattilit al follow - up . 
from january 2003 to august 2010 , 32 patients ( 24 with primary non - small - cell lung cancer and eight with metastases ) with single lung cancer were treated with rf ablation . 
follow - up was performed using computed tomography ( ct ) scans at 1 , 3 , 6 , 12 , 18 and 24 months after the procedure and annually thereafter . 
scopo del presente lavoro stato analizzare i patterns di recidiva in pazienti con tumore polmonare ( primitivo o secondario ) trattato mediante termo - ablazione con radiofrequenza ( rfa ) per via percutanea . 
da gennaio 2003 ad agosto 2010 , sono stati trattati 32 pazienti [ 24 affetti da tumore polmonare non a piccole cellule ( nsclc ) ed 8 da lesioni secondarie ] con tumore polmonare singolo . 
il followup stato eseguito con la tomografia computerizzata ( tc ) a 1 , 3 , 6 , 12 , 18 e 24 mesi dopo la procedura , e poi annualmente . 
la recidiva locale il pattern di recidiva pi frequente nella nostra serie ; probabilmente un trattamento iniziale con rfa pi aggressivo potrebbe dare dei risultati radiol med ( 2012 ) 117 : 13201332 1321 keywords single tumour lung tumour radiofrequency ablation migliori , ma in accordo con lanalisi della letteratura riportata , sono necessari un maggior numero di pazienti e di studi per confermare questa ipotesi . 
 parole chiave tumore singolo tumore polmonare ablazione con radiofrequnza introduction introduzione lung cancer is certainly one tumour that is of particular interest to the scientific community in relation to its increasing incidence and high rate of mortality worldwide [ 1 ]  . 
in the advanced stages of disease , other objectives achieved with local rf ablation are cytoreduction associated or not with radiotherapy and / or chemotherapy and palliation . the aim of our study was to evaluate the effectiveness of rf ablation , overall disease - free survival ( dfs ) after rf ablation in patients with nsclc or secondary lung lesions and factors associated with recurrences . 
 materials and methods patients and lesions between january 2003 and august 2010 , 32 patients ( 25 men and seven women ; mean age 67.8 years ; range 4984 years ) with 32 unresectable single lung lesions underwent percutaneous treatment with rf ablation ( table 1 )  . 
the remaining lesions comprised one ( 4.2% ) stage iiia and two ( 8.3% ) stage iiib ; there were le neoplasie polmonari sono neoplasie che destano particolare interesse nella comunit scientifica in relazione al continuo incremento dellincidenza ed agli elevati tassi di mortalit in tutto il mondo [ 1 ]  . 
questo ha portato alla ricerca di terapie alternative alla chirurgia , quali le tecniche ablative che consentono di ottenere un controllo locale dei tumori non operabili [ 5 , 6 ]  . 
nel corso degli anni , sono state sviluppate diverse tecniche di ablazione ; queste sono rappresentate dallablazione con etanolo , lablazione con laser , la crioablazione e la termoablazione con radiofrequenza ( rfa ) [ 7 ]  . 
i pazienti appartenenti alla serie presentata in questo lavoro , non erano candidati alla chirurgia per la presenza di co - morbilit mediche o di altre controindicazioni alla chirurgia , come la insufficienza cardio - respiratoria . 
negli stadi avanzati di malattia , altri scopi ottenibili con la termo - ablazione locale possono essere la cito - riduzione associata o meno alla radioterapia e / o alla chemioterapia e la palliazione . lo scopo di questo studio di valutare lefficacia della rfa , lintervallo libero da malattia dopo rfa in pazienti con tpnpc o tumori secondari , ricercando i fattori associati alle recidive . materiali e metodi pazienti e lesioni nel periodo compreso tra gennaio 2003 ed agosto 2010 , trentadue pazienti ( 25 uomini e 7 donne ) , et media 67 , 8 anni ( range 4984 anni ) con 32 lesioni singole polmonari non operabili , sono stati sottoposti a trattamento percutaneo di rfa ( tabella 1 )  . 
tutti i pazienti inclusi in questo studio sono stati etichettati come non - chirurgici ( sulla base delle caratteristiche della lesione , la presenza di comorbilit , etc )  . 
of the eight metastatic lesions , three ( 37.5% ) were from prostate cancer , three from colorectal cancer ( 37.5% ) , one ( 12.5% ) from osteosarcoma and one ( 12.5% ) from endometrial cancer . 
a central tumour was defined as being entirely located within the inner two thirds of the lung and as peripheral if a portion of it resided in the outer one third of the lung . 
informed consent was obtained from each patient before the procedure . baseline imaging pretreatment imaging consisted of a thoracic multidetectorrow computed tomography ( mdct ) scan extending to the erano tpnpc e 8 erano metastasi . 
diciassette ( 70 , 8% ) pazienti avevano una malattia in stadio ia e 4 ( 16 , 7% ) pazienti presentavano una malattia in stadio ib al momento del trattamento con rf . 
i restanti pazienti erano cos suddivisi : un caso ( 4 , 2% ) con stadio iiia , 2 ( 8 , 3% ) con stadio iiib mentre nessuno ( 0% ) aveva una malattia in stadio iv . 
degli 8 pazienti con metastasi , 3 ( 37 , 5% ) erano affetti da carcinoma prostatico , 3 ( 37 , 5% ) da carcinoma colon - rettale , uno ( 12 , 5% ) da osteosarcoma e uno ( 12 , 5% ) da carcinoma endometriale . 
the contrast - enhanced scans were acquired after injection of 100 ml of iodinated contrast agent ( visipaque 320 , ge healthcare , usa ) at an injection rate of 3 ml / s , followed by injection of 40 ml saline at a rate of 2 ml / s . 
one week prior to the ablation treatment , all patients underwent percutaneous pulmonary biopsy under ct guidance , with histological confirmation of nsclc or metastasis for all lesions . treatment procedures before the beginning of each procedure , local anaesthesia of the needle entrance site was achieved with subcutaneimaging di base prima della procedura , ciascun paziente stato sottoposto ad indagine tomografica computerizzata multidetettore ( tcmd ) ( aquilion 64 , toshiba , tokio , giappone ) del torace estesa anche alladdome senza e con somministrazione di mezzo di contrasto . 
lesame con mezzo di contrasto stato acquisito dopo liniezione di 100 ml di mezzo di contrasto iodato ( visipaque 320 , ge healthcare , usa ) ad una velocit di iniezione di 3 ml / s , seguito dallinfusione di 40 ml di soluzione salina ad una velocit di 2 ml / s . 
una settimana prima del trattamento ablativo , tutti i pazienti sono stati sottoposti ad ago - biopsia polmonare sotto guida tc , con successiva conferma istologica di tpnpc o metastasi per tutte le lesioni . 1324 radiol med ( 2012 ) 117 : 13201332 ous injection of a 10 - ml solution of 2% carbocaine . 
each patient was kept in a state of moderate sedation through intravenous administration of a combination of midazolam ( 0.070.08 mg / kg ) , propofol ( 0.52.0 mg / kg / h ) and fentanyl ( 12 g / kg )  . 
adequate antibiotic prophylaxis was achieved with intravenous administration of 1 g cefazolin sodium ( ancef , smithkline beecham pharmaceuticals , philadelphia , pa , usa ) given every 8 h for 24 h , beginning shortly before the procedure . equipment imaging guidance procedure di trattamento prima di iniziare ogni procedura , stata effettuata una anestesia locale a livello del punto di ingresso dellago con iniezione sottocutanea di 10 ml di carbocaina al 2% . 
ciascun paziente stato dunque portato a uno stato di sedazione moderata attraverso la somministrazione intravenosa di una combinazione di midazolam ( 0 , 070 , 08 mg / kg ) , propofol ( 0 , 52 , 0 mg / kg / h ) e fentanyl ( 12 g / kg )  . 
unadeguata profilassi antibiotica stata ottenuta mediante somministrazione endovenosa di un 1 g di cefazolina sodica ( ancef , smithkline beecham pharmaceuticals , philadelphia , usa ) ogni 8 h per 24 h , iniziata appena prima della procedura . in 22 / 32 sessions ( 22 / 32 lesions ) , the needle was placed under ct fluoroscopy guidance , whereas in the remaining sessions ( 10 / 32 lesions ) , the procedure was performed with xperguide cone - beam ct ( allura , philips medical systems , best , the netherlands )  . 
the choice of imaging guidance was made on a random basis . equipaggiamento guida imaging rf ablation technique the rf ablation delivery system consisted of an rf generator ( rf 3000 , boston scientific , natick , ma , usa ) operating at 460 khz with a maximum power of 200 w . 
 choice of electrode was at the discretion of the interventional radiologist , who also decided on the possible need for more than one application in the same session to obtain a larger area of necrosis . 
chest x - ray and a complete serum metabolic panel were used for a more comprein 22 su 32 trattamenti ( 22 / 32 lesioni ) , lago stato posizionato sotto guida fluoro - tc mentre nei restati trattamenti ( 10 / 32 lesioni ) , la procedura stata effettuata con il sistema xperguide cone beam tc ( allura , philips medical systems , best , the netherlands )  . 
la scelta della metodica di imaging utilizzata per posizionare lago stata casuale . tecnica di rfa il sistema di conduzione di rf consiste in un generatore di radiofrequenze ( rf 3000 ; boston scientific , natick , ma ) operativo a 460 khz con una potenza massima di 200 w . 
la scelta dellagoelettrodo stata a discrezione dal radiologo interventista che ha anche deciso leventuale necessit di eseguire pi di una applicazione nel corso della stessa seduta per ottenere unarea di necrosi pi grande . 
due ore dopo la procedura , ogni paziente stato sottoposto ad una radiografia del torace per valutare la presenza di eventuali complicanze immediate . radiol med ( 2012 ) 117 : 13201332 1325 fig . 
patterns of recurrence were classified as local , intrapulmonary , nodal , mixed and distant [ 9 , 10 ]  . local recurrence was defined as a recurrence within or at the margin of the ablation site . 
nodal recurrence was defined as new lymphadenopathy within the thorax , involving either the ipsilateral or contralateral hilum or mediastinua mixed pattern of recurrence referred to the presence of both local and nodal disease at the time of follow - up imaging . 
le recidive sono state classificate come locali , intrapolmonari , linfonodali , miste e a distanza [ 9 , 10 ]  . la recidiva locale stata definita come recidiva entro o ai margini della zona di ablazione . 
2a - h lesame tc documenta un tumore polmonare ( a ) ; scansione tc eseguita dopo il posizionamento dellelettrodo rf ( b ) ; scansione tc condotta al termine del trattamento che ha dimostrato la presenza di inclusi aerei nel contesto della lesione ( c ) , la soffusione emorragica peri - lesionale ed una esile falda di pneumotorace ( d ) ; lesame tc eseguito dopo 3 mesi mostra la presenza di cavitazioni intra - lesionali ( e ) e lassenza di contrast enhancement ( f ) ; lesame tc eseguito dopo 6 mesi ha mostrato la presenza di un consolidamento parenchimale ( g ) , ipodenso dopo somministrazione di mdc ev in relazione a fenomeni necrotico - colliquativi ( h )  . outcomes statistical analysis effectiveness of rf ablation , overall disease - free survival ( dfs ) after rf ablation and factors correlated with recurrence . 
 correlations between sex and age and tumour stage , size and location were correlated with overall survival ( os ) using the chi - square test . analisi statistica va linfoadenopatia allinterno del torace , che coinvolge sia lilo omolaterale o controlaterale che il mediastino . 
 la malattia metastatica a distanza stata definita come la comparsa , oltre che di nuove lesioni nello stesso lobo sede della primitivit o nel lobo controlaterale , anche di linfoadenopatie mediastiniche o iliari . 
 gli outcomes presi in considerazione sono stati lefficacia della rfa , lintervallo libero da malattia ( ilm ) dopo rfa e i fattori correlati con la recidiva . results follow - up imaging showed no evidence of residual or recurrent tumour in 17 ( 53.1% ) of 32 tumours ( table 2 )  . 
 in the remaining five ( four metastases and one nsclc ) patients without recurrence , death was determined by causes not related to the lesion treated with rf ablation ; in particular , two patients ( one with a secondary lesion and the other with nsclc ) died of cerebral haemorrhage , one in a car accident and two due to the primary cancer ( independent from the lung localisation : one due to liver metastases that appeared during the follow - up and the other due to a septic complication after partial hepatectomy )  . 
let media dei pazienti di questo gruppo era 72 , 1 anni ( range 5284 anni ) , e la dimensione media del tumore risultata di 27 , 4 mm ( range 1550 mm )  . 
4 lintervallo libero da malattia ( ilm ) dopo rfa : ilm dopo rfa era 20 mesi ( periodo massimo di follow - up 72 mesi )  . ti di questo gruppo era di 63 anni ( range 4973 anni ) e la dimensione media del tumore di 32 , 3 mm ( range 2054 mm )  . 
delle 15 recidive , in 6 ( 40% ) pazienti si verificata una recidiva locale , in 3 ( 20% ) intrapolmonare , in 3 ( 20% ) linfonodale ed in 2 casi ( 13 , 3% ) a distanza . 
gli altri parametri ( sesso , stadio , localizzazione , dimensioni ) non erano statisticamente correlati con il rischio di recidiva ( p > 0 , 05 )  . recurrence no recurrence group risultati statistici fig . 
5 i box - plots mostrano una influenza significativa dellet del paziente ( p < 0 , 05 ) sul rischio di recidiva . patient had a mixed pattern of local and nodal recurrence . 
attualmente , la terapia ablativa toracica ha un ruolo in tre scenari principali : il trattamento del tumore polmonare primitivo , il trattamento delle metastasi polmonari , e la palliazione delle masse dolorose della 1330 discussion since the first report of rf ablation of pulmonary tumours in 2000 , multiple publications have confirmed the feasibility , safety and efficacy of rf ablation of lung malignancy [ 2 , 7 , 12 ]  . 
currently , thoracic abla tive therapy has a role in three broad scenarios : treating primary lung cancer and lung metastases and palliation of painful chest - wall masses [ 15 , 16 ] , the last of which is beyond the scope of this paper . 
a prospective intention - totreat multicentre clinical trial , the radiofrequency ablation of pulmonary tumors response evaluation ( rapture ) trial [ 17 ] , showed that in 106 patients with 183 primary or secondary lung tumours < 3.5 cm treated with rf ablation , cancer - specific survival rates for patients with nsclc were 92% at 1 year and 73% at 2 years [ 17 ]  . 
 [ 7 ] reported on a series with a follow - up of 5 years and noted an overall survival rate for nsclc of 78% at 1 year and 27% at 5 years . 
for most studies , inclusion criteria were limited to those patients unfit for surgery , radiotherapy or chemotherapy , leading many authors to suggest the need for a randomised controlled trial comparing standard treatment versus rf ablation to assess the possible benefits . 
the rates of local tumour progression and survival for lesions treated with rf ablation have been linked to pretreatment tumour size ( 3 cm ) and location ( proximity to vasculature ) [ 7 , 18 ]  . the major role of rf ablation in pulmonary metastasis , as in primary lung cancer , is to treat patients for whom surgical metastasectomy would not be ideal . 
 the goal of ablation should be to include an expected ablation zone that covers the primary tumour plus at least an additional 810 mm of ablation beyond the visible tumour margin in all directions . 
 [ 19 ] suggests that the lack of a circumferential ground - glass halo at the time of treatment of pulmonary metastases may be an early predictor of treatment failure . results of our study showed recurrence in 46.9% of lung cancers after rf ablation . 
our data are consistent with those of previous studies [ 10 , 20 ]  . radiol med ( 2012 ) 117 : 13201332 parete toracica , aspetto , questultimo , che non rientra negli obiettivi di questo manoscritto [ 15 , 16 ]  . 
un recente studio clinico multicentrico prospettico , il radiofrequency ablation of pulmonary tumors response evaluation trial [ 17 ] , ha dimostrato che in 106 pazienti con 183 tumori polmonari primitivi o secondari con dimensioni inferiori a 3 , 5 cm trattati mediante rfa , i tassi di sopravvivenza cancro - specifici per i pazienti con tpnpc sono del 92% ad 1 anno e 73% a 2 anni [ 17 ]  . 
 [ 7 ] hanno riportato unesperienza con un follow - up di 5 anni e hanno notato un tasso di sopravvivenza globale per i tpnpc del 78% ad 1 anno e 27% a 5 anni . 
per la maggior parte degli studi , i criteri di inclusione sono stati limitati a quei pazienti non candidati a terapia chirurgica , a radioterapia ( rt ) o a chemioterapia , portando dunque molti autori a suggerire la necessit di uno studio randomizzato controllato confrontando il trattamento standard con la rfa per valutare i possibili vantaggi . 
la probabilit di progressione locale del tumore e la sopravvivenza per le lesioni trattate con rfa sono dipendenti dalla dimensione pre - trattamento del tumore ( 3 cm ) e dalla posizione ( vicinanza a strutture vascolari ) [ 7 , 18 ]  . attualmente , il ruolo principale della rfa nelle metastasi polmonari , peraltro non dissimile da quello per il tumore polmonare primitivo , quello di trattare quei pazienti per i quali la metastasectomia chirurgica non risulta essere lopzione terapeutica ideale . 
nei pazienti con metastasi del colon - retto , il radiofrequency ablation of pulmonary tumors response evaluation trial [ 17 ] ha dimostrato tassi di sopravvivenza cancro - specifici del 93% ad 1 anno e del 67% a 2 anni . lobiettivo della termoablazione dovrebbe prevedere una zona di ablazione che comprenda il tumore primitivo pi almeno altri 810 mm di ablazione oltre il margine del tumore visibile in tutte le direzioni . 
tale obbiettivo non sempre facile da ottenere , soprattutto nei tumori di grandi dimensioni o nei tumori che sono adiacenti a strutture critiche , come il cuore o lilo polmonare . 
 [ 19 ] suggerisce come la mancanza di un alone circonferenziale di ground glass al momento del trattamento delle metastasi polmonari possa essere un predittore precoce di fallimento del trattamento . i risultati del nostro studio hanno mostrato una recidiva nel 46 , 9% dei casi di cancro al polmone dopo rfa . 
some authors suggest that the use of rf ablation in combination with radiotherapy is safe and provides improved local survival versus conventional radiotherapy alone [ 10 , 21 ]  . 
for larger primary lung tumours , a combination of ablation and radiotherapy is generally recommended , but to date there is no evidence of this protocol providing additional benefits [ 22 ]  . 
in this study , we excluded patients undergoing concomitant external - beam radiation because they represent only a small part of the population . efficacy and safety data that have emerged for pulmonary rf ablation serve as benchmarks for performance of newer ablative technologies , such as mwa . 
 [ 25 ] suggested that mwa of primary and metastatic tumours in patients deemed to have medically inoperable disease may confer a survival benefit versus rf ablation in tumours > 3 c as rf ablation is dependent on thermal conductivity , air - filled spaces in the ventilated lung adjacent to tumours tend to limit the size of the ablation , which is a potential cause of local tumour progression at the periphery of the ablated lesion [ 26 , 27 ]  . 
 microwave propagation is thought not to be similarly hindered and may therefore be more effective in achieving a complete ablation [ 3 ]  . more studies are needed to determine how best to exploit the properties of this technology for better tumour ablation . 
a retrospective investigation about dfs after rf or mw ablation will be a further goal once we have collected a sufficient number of patients treated with mwa with a long follow - up period ( at least comparable with that presented in this study )  . local recurrence is the most common pattern of recurrence in our series . 
although a more aggressive initial rf ablation could potentially offer improvement in outcomes , on the basis of the literature , further studies involving larger patient samples are required to confirm this hypothesis . 
alcuni autori hanno suggerito che limpiego della rfa in combinazione con la rt sicura e fornisce una miglior sopravvivenza rispetto alla sola rt convenzionale [ 10 , 21 ]  . 
 per i tumori polmonari primitivi pi grandi generalmente raccomandata una combinazione di ablazione e rt , ma per tale protocollo , al momento , non esistono dimostrazioni circa benefici aggiuntivi [ 22 ]  . 
in questo studio abbiamo escluso quei pazienti sottoposti contemporaneamente a rt esterna , in quanto rappresentavano solo una piccola parte . i dati di efficacia e di sicurezza che sono emersi dalle esperienze di rfa possono servire come punto di riferimento per lo sviluppo di nuove tecnologie ablative , come lablazione mediante microonde ( mwa )  . 
 [ 25 ] ha suggerito che la mwa di tumori primari e metastatici in pazienti considerati non clinicamente operabili garantisce un beneficio di sopravvivenza rispetto alla raf nei tumori con dimensioni maggiori di 3 cdal momento che la rfa dipendente dalla conducibilit termica , gli spazi ripieni daria nel polmone ventilato adiacente alla neoplasia tendono a limitare le dimensioni dellablazione ; ci potenziale causa di progressione locale del tumore dalla periferia della lesione ablata [ 26 , 27 ]  . 
 la propagazione delle microonde si pensa non essere ostacolata in modo simile e possa quindi essere pi efficace per ottenere unablazione completa [ 3 ]  . ulteriori studi sono necessari per determinare il modo migliore per sfruttare le propriet di questa tecnologia per migliorare i risultati dellablazione di tali neoplasie . 
unindagine retrospettiva sullintervallo libero da malattia dopo rfa o mwa rappresenta un altro dei nostri obiettivi , quando saranno disponibili un numero sufficiente di pazienti trattati con mwa , con un lungo periodo di follow - up ( almeno paragonabile a quello presentato in questo studio )  . la recidiva locale il pattern di recidiva pi frequente nella nostra serie ; probabilmente un trattamento iniziale con rfa pi aggressivo potrebbe dare dei risultati migliori , ma in accordo con lanalisi della letteratura riportata , sono necessari un maggior numero di pazienti e di studi per confermare questa ipotesi . 
 in this early phase , i am working both on revamping the editorial board by appointing two deputy editors , in bearing with the societys rules , and on reorganising the advisory editorial board and the list of peer referees . the challenges awaiting the new working group are many and complex . 
the objectives are not only to maintain the current impact factor through a careful and strict selection of manuscripts , but also to progressively extend the journals international scope , consistent with the levels already reached by many italian radiologists . in agreement with what was discussed by the sirm executive board , we will soon present the new editorial project whereby two parallel journals will be issued as of the year 2014 . 
 the other , in italian , will be printed and distributed to all sirm members in the usual manner . in particular , the italian journal will contain a translation of the english on - line version , supplemented by a series of educational articles , reviews , case reports , consensus papers and reports , with the aim of providing members with a pracmi accingo a presentare il numero di dicembre de la radiologia medica come nuovo direttore editoriale , dopo il lungo e prestigioso periodo di direzione del pozzi mucelli , che ha lasciato lincarico dopo pi di dieci anni . chi mi ha preceduto , ha saputo elevare la rivista ad una dignit e valore scientifico che la pone ai primi posti , non solo in europa , fra le riviste del settore e per questa opera irripetibile lo ringrazio a nome mio e di tutta la radiologia italiana . 
 in questa prima fase sto lavorando sia al rinnovo delleditorial board , in linea con il regolamento societario , con la nomina dei due vice - direttori , che alla ristrutturazione del comitato consultivo editoriale e della lista dei peer referee . le sfide che attendono il nuovo gruppo di lavoro saranno molteplici e complesse , non solo volte a mantenere i livelli bibliometrici raggiunti attraverso una rigida e accurata selezione degli articoli , ma anche a lavorare affinch la rivista assuma sempre di pi un respiro internazionale , coerente con il livello gi raggiunto da molti radiologi italiani . in accordo con quanto discusso in seno al consiglio direttivo sirm , sar presto presentato il nuovo progetto editoriale che preveder , a partire dal 2014 , la costituzione di due riviste parallele , una in inglese solo su web , che assicuri la visibilit internazionale degli autori e la valenza scientifica con particolare riguardo allincremento del impact factor , e una in italiano , che verr stampata e distribuita con le stesse modalit attuali a tutti i soci sirm . in particolare la versione italiana conterr la versione inglese on - line tradotta , corredata e implementata da una serie di articoli educazionali , review , case report , documenti e articoli di consensus cos da essere un pratico strumento di 1274 radiol med ( 2012 ) 117 : 12731274 tical and easy - to - consult resource for work and professional development . lavoro e di aggiornamento professionale facilmente consultabile a disposizione del socio . next year sirm will be 100 years old : a major society with a long history full of prestigious achievements which has always placed its members with their needs and cultural and professional growth at the forefront , with a view to safeguarding radiology and the patients best interests . 
luigi gonzaga hospital , regione gonzole 10 , 10043 orbassano , torino , italy 2radiation oncology unit , department of medical and surgical sciences , university of torino , s . 
for a threshold 5 mm , the two systems provided corresponding setup errors along the y and z axes , whereas along the x axis , the threshold was not necessary . 
alignrt is an accurate technique for setup in 3d - crt prostate cancer patients , especially along the lateral direction . keywords surface imaging system alignrt prostate cancer conformal radiotherapy setup reproducibility riassunto obiettivo . 
il corretto set - up rappresenta un requisito fondamentale della radioterapia conformazionale ( 3d - crt ) ed i sistemi di registrazioni di immagini di superficie rappresentano una delle metodiche utilizzate per la verifica . 
per la soglia di 5 mm gli errori di set - up rilevati dal alignrt lungo gli assi y , z e x sono stati osservati nel 47 , 4% , 42 , 1% e 5 , 3% dei pazienti , rispettivamente . 
alignrt un sistema accurato per la valutazione del set - up nei pazienti sottoposti a 3d - crt , specialmente lungo la direzione laterale . parole chiave sistema di registrazione di immagini di superficie corporea alignrt tumore della prostata radioterapia conformazionale riproducibilit del set - up 1420 introduction conformal radiotherapy ( 3d - crt ) of prostate cancer has the aim of increasing the dose delivered to the clinical target volume ( ctv ) while sparing critical organs , and therefore the margins around the ctv should be maximally reduced . 
the techniques include standard megavoltage electronic digital portal images ( dpi ) [ 2 ] , kilovoltage ( kv ) x - ray localisation of implanted clips [ 3 ] , optical imaging [ 4 , 5 ] and video imaging [ 69 , 9 ]  . 
 in this study we collected , analysed and compared target registration errors , using a surface imaging system , with setup errors determined from dpi in 19 prostate cancer patients treated with 3d - crt at the radiation oncology unit , san giovanni battista hospital , university of turin , with the aim of verifying the validity of this video - based system . materials and methods patient population radiol med ( 2012 ) 117 : 14191428 introduzione lo scopo della radioterapia conformazionale ( 3d - crt ) nel tumore della prostata quello di aumentare la dose somministrata al volume bersaglio e risparmiare gli organi critici e quindi i margini intorno al clinical target volume ( ctv ) saranno minimi . 
i fattori che influenzano la riproducibilit del target durante il trattamento e tra le sedute di rt sono lo spostamento degli organi interni tra le sedute e il movimento degli organi interni durante la seduta stessa . 
dimostrato che per il paziente affetto da tumore della prostata lerrore di set - up lungo lasse laterale maggiore rispetto allerrore di set - up lungo gli altri assi [ 1 ]  . 
le tecniche includono le immagini portali ( dpi ) [ 2 ] , la localizzazione di reperi radiopachi attraverso immagini kilovoltage ( kv ) [ 3 ] , le immagine ottiche [ 4 , 5 ] e le immagini video [ 69 ]  . 
le immagini portali acquisite durante il trattamento e la loro analisi , sono dirimenti per eliminare significativamente gli errori sistematici e casuali presenti nella pratica clinica [ 1 ]  . 
 in questo studio abbiamo raccolto , analizzato e confrontato gli spostamenti del target , usando un sistema di registrazioni di immagini di superficie , con gli errori di set - up del paziente ottenuti con il dpi , in 19 pazienti affetti da tumore della prostata sottoposti a 3d - crt presso lunit di radioterapia oncologica , ospedale san giovanni battista , universit di torino con lobiettivo di verificare la validit di questo sistema basato sulle immagini from july 2009 to december 2009 , 19 patients affected by adenocarcinoma of the prostate and subjected to external radiotherapy were enrolled in this study . 
all patients underwent a planning computed tomography ( ct ) scan in the supine position with kneefix and feetfix immobilisation device ( civco , the netherlands ) , filled bladder , empty rectum and an endorectal catheter . 
ct slices materiali e metodi caratteristiche dei pazienti in questo studio sono stati arruolati , da luglio 2009 a dicembre 2009 , 19 pazienti affetti da adenocarcinoma della prostata e sottoposti a radioterapia conformazionale . 
three skin tattoos , two lateral and one anterior , were performed for setup verification by alignment to a mobile laser systethe ct images were transferred to the treatment planning system ( oncentra masterplan v 3.0 , nucleotron , the netherlands ) to define the volumes of interest . 
the planning target volume ( ptv ) was derived by automatic expansion of ctv of 12 mm in the craniocaudal direction , 10 mm in the lateral and anterior directions and 8 mm in the posterior direction . 
patients were treated with five individually shaped coplanar fields ( 0 , 45 , 90 , 270 , 315 ) delivered with 10 - mv photons produced by a clinic varian 2500 c / d in daily fractions of 2 gy . 
orthogonal portal images for treatment verification were acquired at the beginning of 3dcrt and weekly for each enrolled patient and subsequently compared with digitally reconstructed radiographs ( drrs ) generated from the planning ct scans . image acquisition system a commercially available video - based 3d surface - imaging system ( alignrt ; visionrt , london , uk ) was installed in sono stati definiti in sovrappeso e tre pazienti sono stati definiti obesi . 
per tutti i pazienti in studio stata eseguita una tomografia computerizzata ( tc ) di pianificazione in posizione supina , con la vescica piena , il retto vuoto e una sonda rettale ed stato utilizzato un sistema dedicato e personalizzato per limmobilizzazione dei pazienti ( kneefix and feetfix , civco , nl , usa )  . 
mediante un software di simulazione virtuale , durante la tc , stato identificato lisocentro a livello della ghiandola prostatica e sono stati eseguiti tre tatuaggi , allineando il sistema dei laser ( uno anteriore e due laterali ) , per la verifica del set - up . 
le immagini tc acquisite sono state trasferite al sistema per la pianificazione del trattamento ( oncentra masterplan v 3.0 , nucleotron , nl , usa ) e utilizzate per la definizione dei volumi di interesse radioterapico . 
il planning target volume ( ptv ) stato ottenuto espandendo il ctv di 12 mm a livello cranio - caudale , 10 mm anteriormente e lateralmente e 8 mm posteriormente . 
la 3d - crt stata effettuata mediante tecnica isocentrica a 5 campi co - planari ( 0 , 45 , 90 , 270 , 315 ) sagomati , utilizzando fotoni x con energia di 10 mv prodotti da un clinic varian 2500 c / d in frazioni giornaliere di 2 gy . 
alignrt is designed as a patientsetup device ( classified as a class ii device ) used to image the skin surface of a patient in 3d before and during radiotherapy treatment . 
the surface - imaging device consists of two camera pods mounted in the linear accelerator room under an oblique angle of 30 with respect to the treatment table ; each pod contains camera and flash systems that allow the capture of 3d surface information . 
this reference image is generated by either recording the surface of a patient placed in a conventional radiotherapy simulator in which the system is installed or by importing skin contours from ct volumetric data . 
if a movement from the position of the reference surface image is detected , the software calculates new coordinates to adjust the treatment couch to the original position of the patient . 
the roi consisted of the lower abdomen from the umbilical region to all sacru during the first treatment session , patients were aligned using standard lasers and skin tattoos , and two orthogonal portal images were acquired ( 090 )  . 
al fine di verificare la correttezza del trattamento , sono state acquisite , alla prima seduta e successivamente con cadenza settimanale , le immagini portali e successivamente confrontate con le radiografie digitali ricostruite ( drrs ) ricavate dal piano di cura del trattamento radioterapico . sistema di acquisizione di immagini un sistema di registrazione di immagini di superficie corporea ( alignrt ; visionrt , london , regno unito ) stato installato nella sala di trattamento presso il reparto di radioterapia oncologica , universit di torino . 
lalignrt un dispositivo per il controllo del set - up del paziente ( classificato come dispositivo di classe ii ) ed usato per acquisire un immagine in 3d della superficie corporea del paziente prima e durante il trattamento radioterapico . 
il sistema composto da due unit ottiche con telecamere stereoscopiche che sono saldamente fissate al soffitto della sala di trattamento e poste a 30 rispetto alla verticale e focalizzate entrambe verso lisocentro del linac . 
le immagini vengo registrate in un punto dellatto respiratorio sempre ripetibile.per il set - up del paziente , lalignrt genera una immagine di superficie di riferimento della posizione di trattamento ottimale determinata durante la simulazione . 
questa immagine di riferimento pu essere generata o durante la simulazione di radioterapia registrando la superficie del paziente se presente lalignrt nella sala di simulazione o importando i contorni volumetrici dalla tc . 
se viene rilevato uno spostamento dalla posizione di riferimento , il software calcola le nuove coordinate da dare al lettino per riportare il paziente alla posizione originale . protocollo di acquisizione delle immagini in questo studio limmagine di superficie di riferimento della regione di interesse ( roi ) stata generata importando i contorni volumetrici dalla tc . 
1 distribuzione degli spostamenti individuati con dpi nelle tre direzioni ( vrt , verticale ; lat , laterale ; lng , longitudinale )  . tematic and random errors were calculated and reported as mean and standard deviation ( sd )  . 
setup errors detected by dpi in the vertical ( z ) , lateral ( x ) and longitudinal ( y ) directions and the respective p values are reported in figure 1 . 
 durante la prima seduta di trattamento , i pazienti sono stati allineati secondo i laser e secondo i tatuaggi e sono state acquisite due immagini portali ortogonali ( 090 )  . 
gli errori sistematici e random sono stati calcolati e riportati come media e come deviazione standard ( ds )  . dpi > threshold threshold 3 mm 4 mm 5 mm vrt 62% 52% 41% lng 71% 56% 47% vrt , vertical ; lat , lateral ; lng , longitudinal soglia 3 mm 4 mm 5 mm dpi > soglia vrt 62% 52% 41% lng 71% 56% 47% vrt , verticale ; lat , laterale ; lng , longitudinale risultati sono state ottenute complessivamente 653 immagini alignrt ( media di 34 , 37 immagini per paziente ) e 99 immagini portali ( media di 5 , 2 immagini per paziente )  . 
la distribuzione degli errori di set - up individuati sulle immagini dpi nelle direzioni verticale ( z ) , laterale ( x ) e longitudinale ( y ) e i rispettivi valori di p sono riportati nella figura 1 . 
la maggior parte sono stati effettuati in ambito toracico e per i tumori della mammella e hanno dimostrato come i sistemi di registrazione di immagini di superficie possono migliorare la precisione del set - up e come sono affidabili nel ridurre gli effetti delle escursioni respiratorie [ 2 , 7 , 12 ]  . 
 [ 10 ] sono stati analizzati gli errori di set - up in 22 pazienti affetti da adenocarcinoma prostatico , confrontando gli spostamenti rilevati da un sistema di registrazione di immagini di superficie corporea ( axis 2100 network camera , svezia ) con quelli rilevati dalle immagini portali . 
gli autori hanno analizzato solo gli spostamenti lungo la direzione laterale rilevati dalle due metodiche e hanno osservato che la correlazione presente tra i due sistemi era maggiore che quella tra la posizione del marker e gli errori rilevati dalle immagini portali . 
gli autori hanno concluso che questo sistema un metodo accurato per determinare gli errori di set - up lungo la direzione laterale e potrebsystems detected similar setup errors , with a statistical significance for each threshold level , whereas along the vertical and longitudinal directions , the two systems showed similar shifts only for the threshold level of 5 mm . discussion in modern radiotherapy multiple approaches are used to obtain data on patient position at various treatment sites . 
4 confronto fra dpi e alignrt in funzione delle soglie ( vrt , verticale ; lat , laterale ; lng , longitudinale ) : diagramma dei valori di p . studies investigating the use of these systems [ 2 , 6 , 7 , 913 ] have been published . 
most of them were performed on patients with intrathoracic and breast cancers and showed that surface - imaging systems may improve setup precision and are reliable for reducing the effects of respiratory motion [ 2 , 7 , 12 ]  . 
ploeger and colleagues [ 10 ] analysed setup errors in 22 patients affected by prostate cancer by comparing the shifts detected by video - surface imaging ( axis 2100 network camera , sweden ) with those obtained by dpi . 
the authors analysed only errors along the lateral direction detected by portal and video - surface images ; they observed that the correlation between the two systems was higher than the correlation between the marker position and the portal images error . 
 [ 14 ] investigated the reproducibility of patient setup by using a video - surface imaging registration system ( alignrt ) in a series of 16 patients affected by prostate cancer and treated with curative 3d - crt . 
analysis of systematic and random errors ( calculated using van herks formula ) showed that the mean largest systematic error was found on the z axis and the highest sd in the x axis , similar to what was observed by ploeger et al . 
furthermore , the authors analysed the distribution of positioning errors along the three main axes detected by the alignrt syste for a threshold > 5 mm , shifts along the x axis were observed in 14% of patients , whereas along the other axes ( y and z ) , deviations occurred , respectively , in 2% and 5% of patients . 
 [ 14 ] hanno analizzato la riproducibilit del set - up del paziente utilizzando un sistema di registrazioni di immagini ( alignrt ) in 16 pazienti affetti da adenocarcinoma prostatico e sottoposti a 3d - crt con intento curativo . 
le immagini ottenute dallalignrt sono state confrontate con le immagini portali ed stata osservata una correlazione statisticamente significativa tra le due metodiche , come dimostrato dalla regressione lineare tra gli errori di posizionamento rilevati dai due sistemi che variava tra 0 , 77 e 0 , 92 , con una media di 0 , 85 e una deviazione standard di 0 , 13 . 
lanalisi degli errori sistematici e casuali ( calcolati usando la formula di van herks ) ha dimostrato che lerrore sistematico maggiore stato rilevato lungo lasse z e la deviazione standard maggiore stata rilevata per lasse x , similmente a quanto osservato da ploeger et al . 
prendendo in considerazione la soglia di 5 mm , gli spostamenti maggiori sono stati osservati lungo lasse x ( 14% ) , mentre lungo gli altri assi ( y e z ) , gli errori maggiori di 5 mm sono stati osservati rispettivamente solo nel 2% e 5% dei casi . 
gli autori hanno concluso che lalignrt un metodo affidabile e riproducibile nel ridurre quotidianamente gli errori di set - up ; tuttavia nello studio non sono stati analizzati la rotazione , il movimento intrafrazione e le escursioni respiratorie , parametri che possono influenzare il posizionamento del paziente . 
inoltre , come immagine di riferimento non stata utilizzata la tc di pianificazione del trattamento , ma radiol med ( 2012 ) 117 : 14191428 1427 profiles , mainly due to changes in content of the bowel and rectualso , for a threshold > 3 mm , shifts along the x axis were observed in 37% of patients , whereas along the other axes , deviations were observed in 14% and 28% of patients , respectively . 
the authors concluded that the alignrt system is a reliable and reproducible device to prevent daily setup errors , but they did not analyse parameters that may affect patient setup regarding rotation , intrafraction motion and breathing movements . 
moreover , they did not correlate surface images with ct images but only with dpi , and they used as a reference image the acquisition at the time of the first radiotherapy session . in this study we analysed in 19 patients the daily setup errors detected by alignrt along the three directions during every rt treatment session using ct study as reference images . 
also for the threshold of 3 mm , movements along the y and z axes were observed in the majority of patients ( 68% and 69% , respectively ) ; in the x axis , errors occurred in 10% of patients only . 
 comparing the setup errors detected by alignrt and dpi , we found a statistically significant difference in the detection of shifts along longitudinal and vertical directions , where the optical system showed an overestimation of these shifts . 
however , results obtained with the two systems were in good agreement for a smaller threshold value for the lateral shiwe supposed that the alignrt system is more reliable in the lateral direction because it is able to acquire a larger surface image . considering dpi - drr matching only , the values are significantly shifted from 0 in the y direction ; in all patients we found a shift < 3 mthis systematic error is probably due to reconstruction of the drr based on ct slices of 5 - mmthick sections . 
in fact , decreasing slice thickness ( 3 mm ) will improve the quality of the drr and should eliminate this systematic error . moreover , we investigated the possible relationship between bmi and weight changes with setup shifts detected by alignrt . 
due to the limited numbers of patients , we saw no correlation : in particular , overweight and obese patients showed no significant differences , although alignrt is a body surface imaging systein a larger series of 329 prostate cancer patients , wong and colleagues found a significantly larger shift in the lateral direction for obese patients [ 16 ]  . furthermore , for correct patient setup , rotation and reslimmagine acquisita dallalignrt il primo giorno del trattamento radioterapico . in questo studio abbiamo analizzato gli errori di setup quotidiano rilevati dallalignrt lungo le tre direzioni durante ogni seduta di rt , usando limmagine della tc di pianificazione come immagine di riferimento . 
 [ 14 ] , per una soglia > 5 mm gli spostamenti maggiori sono stati osservati lungo gli assi y e z ( rispettivamente nel 47 , 4% e 42 , 1% dei casi )  . 
anche prendendo in considerazione la soglia di 3 mm , gli spostamenti maggiori sono stati osservati lungo gli assi y e z ( 68% e 69% , rispettivamente )  . 
lungo lasse x gli errori al di sopra di questa soglia sono stati osservati nel 10% dei casi . confrontando gli spostamenti rilevati dallalignrt e dal dpi , stata osservata una significativa differenza nella rilevazione degli spostamenti lungo le direzioni longitudinale e verticale , dove il sistema ottico mostra una sovrastima degli spostamenti stessi . 
pertanto , i dati sono stati analizzati in funzione di determinate soglie di spostamento di 3 , 4 e 5 m prendendo in considerazione la soglia 5 mm , i due sistemi hanno fornito spostamenti corrispondenti lungo la direzione longitudinale e verticale , mentre lungo la direzione laterale la soglia non risultata necessaria . 
abbiamo ipotizzato che il sistema alignrt lungo la direzione laterale pi affidabile in quanto in grado di acquisire unimmagine di superficie pi ampia . considerando il confronto dpi - drrs , gli spostamenti sono significativamente deviati rispetto allo 0 solo nella direzione y ; in tutti i pazienti stato osservato uno spostamento inferiore a 3 mquesto errore sistematico probabilmente dovuto alla ricostruzione delle drrs che si basa sulla scansioni assiali tc ( 5 mm )  . 
poich la qualit delle drrs strettamente correlata allo spessore delle scansioni tc , una riduzione dello spessore da 5 mm a 3 mm potrebbe eliminare questo errore sistematico rilevato unicamente nella direzione longitudinale . inoltre , stata analizzata una possibile correlazione tra il bmi e i cambiamenti di peso con gli spostamenti di setup rilevati dallalignrt . 
in questo studio , probabilmente a causa del numero limitato di pazienti , non stata osservata nessuna correlazione : in particolare i pazienti sovrappeso ed obesi non hanno mostrato differenze significative , sebbene lalignrt sia un sistema di registrazione di immagini di superficie corporea . 
 [ 16 ] hanno trovato spostamenti maggiori nella direzione laterale nei pazienti obesi . inoltre , per un corretto set - up del paziente dovrebbe ro essere anche considerati la rotazione il movimento respiratorio . 
in our opinion , the alignrt system could be used daily in prostate cancer 3d - crt to define setup alignment , whereas portal images could be limited only to the first radiotherapy session and in case of exceeding the tolerance threshold ( > 5 mm )  . 
 i risultati di questo studio dimostrano che gli spostamenti di set - up ottenuti mediante il sistema alignrt sono in accordo con quelli rilevati tramite dpi , in particolare lungo la direzione laterale . 
quin di secondo noi , il sistema alignrt potrebbe essere utilizza to quotidianamente nella 3d - crt del carcinoma prostatico , limitando alla sola prima seduta o in caso di superamento della prestabilita soglia di tolleranza ( > 5 mm ) , le acquisizione delle immagini portali di verifica . 
bonomo3 1radiology department , bambino ges hospital , irccs , rome , italy 2research unit for multifactorial diseases , bambino ges hospital , irccs , rome , italy 3radiology department , catholic university , rome , italy 4cystic fibrosis unit ; bambino ges hospital , irccs , rome , italy correspondence to : l . 
onofrio 4 , 00165 rome , italy , tel . / fax : + 39 - 06 - 68592490 / 2394 , e - mail : lidia.monti@opbg.net received : 23 november 2011 / accepted : 10 january 2012 / published online : 17 september 2012 springer - verlag 2012 abstract purpose . 
il virtual touch tissue quantification , una applicazione quantitativa della tecnica ecografica arfi che fornisce valori numerici ( shear wave velocity , swv : velocit di propagazione dellonda ) della elasticit del parenchima epatico stato utilizzato in 75 pazienti pediatrici affetti da fibrosi cistica ( fc ) nel sospetto di cfld . 
arfi is an innovative screening technique able to help identify cfld in children . keywords acoustic radiation force impulse ( arfi ) imaging cystic fibrosis liver disease liver stiffness pazienti senza evidenza ecografica di malattia 1 , 08 m / s [ 95% intervallo di confidenza ( ci ) 1 , 021 , 14 ]  . 
larfi una tecnica innovativa di imaging in grado di aiutare nella identificazione del coinvolgimento epatico nei pazienti pediatrici affetti da fc . parole chiave acoustic radiation force impulse ( arfi ) fibrosi cistica coinvolgimento epatico rigidit epatica introduction introduzione with the increasing life expectancy of patients with cystic fibrosis , liver disease has become increasingly frequent as an early complication , which should be detected during the first decade of life [ 13 ]  . 
cystic - fibrosis - associated liver disease ( cfld ) is characterised by hepatobiliary fibrosis , which may lead to portal hypertension , growth delay and failure of liver synthetic capacity , requiring liver transplant [ 4 , 5 ]  . 
 diagnosis is based on abnormal biochemistry and clinical and ultrasound ( us ) findings of liver involvement ( hepatomegaly and / or splenomegaly ) , the detection of which may vary over time or occur late in patients with advanced cirrhosis [ 1 ]  . 
in addition , several comorbidities ( due to infection and medications ) , which frequently occur in patients with cystic fibrosis , can cloud the diagnosis , hence altering the classic noninvasive markers of liver disease . 
a recent cohort study has shown that clinical tests , serum alanine aminotransferase ( alt ) levels and us are unable to identify either liver fibrosis or the development of portal hypertension . 
on the contrary , only liver biopsy , the accuracy of which has been improved by dual passes , is able to stage liver fibrosis and predict the development of portal hypertension [ 3 ]  . 
however , liver biopsy has several drawbacks , including sampling error in that the histological lesions of cfld are unevenly distributed throughout the liver parenchyma [ 1 ] ; inaccuracy due to intraand interobserver variability of histopathological interpretation [ 6 ] ; bleeding risk ; high cost ; and healthcare resource utilisation . 
there is therecon laumento dellaspettativa di vita nei pazienti affetti da fibrosi cistica ( fc ) , il riscontro del coinvolgimento epatico ( cfld ) diventato sempre pi frequente come complicanza precoce che deve essere diagnosticata nei primi dieci anni di vita [ 13 ]  . 
la cfld istologicamente caratterizzata da fibrosi biliare responsabile dellinstaurarsi di ipertensione portale , ritardo della crescita e insufficienza di sintesi che pu comportare la necessit del trapianto di fegato [ 4 , 5 ]  . 
 studi trasversali e longitudinali hanno dimostrato una prevalenza complessiva della malattia epatica fra il 27% [ 1 ] e il 41% [ 2 ] con evidenza di cirrosi nel 7 , 8% e 9 , 6% dei casi , rispettivamente . 
il ricorso al trapianto di fegato stato necessario nello 0 , 5% e nel 2 , 1% dei casi , rispettivamente , nel momento in cui si manifesta insufficienza terminale [ 1 , 2 ]  . 
la diagnosi si basa sullalterazione degli esami di laboratorio , sui segni clinici ed ecografici di coinvolgimento epatico ( epatomegalia e / o splenomegalia ) , il cui rilievo tuttavia variabile nel tempo e comunque tardivo nei pazienti in fase avanzata di degenerazione cirrotica [ 1 ]  . 
i test diagnostici clinici , biochimici e radiologici attualmente disponibili possono sovrastimare o sottostimare la prevalenza di cfld e , soprattutto , non possono predire la gravit del danno epatico . 
infatti , un recente studio di coorte ha dimostrato che gli esami clinici , i livelli sierici di alanina aminotransferasi ( alt ) e lecografia non sono in grado di individuare n la presenza di fibrosi epatica n lo sviluppo di ipertensione portale . 
al contrario solo la biopsia , la cui accuratezza migliorata con la tecnica del doppio prelievo , stadia la fibrosi e individua lo sviluppo di ipertensione portale [ 3 ]  . 
tuttavia la biopsia epatica presenta alcuni svantaggi tra cui lerrore di campionamento in quanto le alterazioni istologiche nella cfld sono irregolarmente distribuite nel 1410 radiol med ( 2012 ) 117 : 14081418 fore a need for a diagnostic test able to identify this prevalent condition . 
acoustic radiation force impulse ( arfi ) is a new tissue - strain imaging technology that utilises sound waves by applying an acoustic push pulse to a defined region of interest ( roi )  . 
using us , we are able to measure shearwave velocity ( swv ) ( m / s ) .theoretically , the stiffer the tissue , the faster the shear wave will be propagated . 
quantitative in vivo study results have been obtained in chronic liver conditions , including viral hepatitis [ 712 ] , and nonalcoholic fatty liver disease [ 13 , 14 ]  . 
 the aim of our study was to assess the diagnostic performance of arfi with virtual touch tissue quantification technology integrated into a conventional us system in detecting signs of cfld in children ( splenomegaly , portal hypertension and oesophageal varices )  . materials and methods study population from september 2009 to october 2010 , 75 patients with cf [ 35 boys and 40 girls aged 14.40.91 years ; 95% confidence interval ( ci ) , 13.616.2 ] followed at the cystic fibrosis unit of our institution with suspected cfld were consecutively enrolled . 
the suspicion of cfld was based on one of the following criteria : alanine aminotransferase ( alt ) persistently elevated or fluctuating between normal and elevated ( > 1.5 the upper limit of alt ) , with at least two measurements of elevated alt in the 18 months prior to the study ; hepatomegaly and / or splenomegaly . 
information on genotype , history of meconium ileus and diabetes , intake of ursodeoxycholic acid ( 2030 mg / kg / day ) or use of recombinant long - acting insulin were available from the cf patients files . 
on the day of the study , serum liver function tests [ alt , aspartate parenchima [ 1 ] , linacuratezza dovuta alla variabilit intra ed interoperatore nella interpretazione istopatologica [ 6 ] , il rischio emorragico , lalto costo ed il largo impiego di risorse economiche . 
lacoustic radiation force impulse ( arfi ) una metodica nuova di imaging della rigidit di un tessuto che impiega onde meccaniche applicando un impulso acustico di breve durata in una circoscritta regione di interesse ( roi )  . 
sono gi stati effettuati studi quantitativi in vivo nelle epatopatie croniche incluse le epatiti virali [ 712 ] e nella steatosi epatica non alcolica [ 13 , 14 ]  . 
 lo scopo del nostro studio di valutare la prestazione diagnostica della tecnologia arfi con virtual touch tissue quantification integrata in un ecografo convenzionale , nel rilevare segni di cfld ( splenomegalia , ipertensione portale e varici esofagee ) nei pazienti pediatrici . 
 materiali e metodi popolazione in studio fra settembre 2009 e ottobre 2010 sono stati arruolati settantacinque pazienti affetti da fibrosi cistica e con sospetta cfld [ 35 maschi e 40 femmine con et media di 14 , 40 , 91 anni , 95% intervallo di confidenza ( ci ) 13 , 616 , 2 ] , seguiti presso lunit operativa di fibrosi cistica della nostra struttura . 
la presenza di cfld stata sospettata quando era presente uno dei seguenti criteri : livelli di aminotransferasi persistentemente elevati ( superiori a 1 , 5 il limite massimo ) o fluttuanti tra normali ed elevati in almeno 2 misurazioni nei 18 mesi precedenti allo studio ; epatomegalia e / o splenomegalia . 
i dati relativi al genotipo , alla storia di ileo da meconio e di diabete , lassunzione di acido ursodesossicolico ( 2030 mg / kg / die ) o lutilizzo di insulina ad azione prolungata erano disponibili nel database dei pazienti del reparto di fibrosi cistica . 
nesradiol med ( 2012 ) 117 : 14081418 1411 aminotransferase ( ast ) , gamma - glutamyltranspeptidase ( gt ) ] , liver synthetic function [ international normalised ratio ( inr ) and albumin ] were investigated . 
all patients were negative for hepatotropic viruses ( hepatitis a , b , c , d , e , and g ; cytomegalovirus ; and epstein - barr virus )  . 
 scheduled examinations included pulmonary function tests [ forced vital capacity ( fvc ) and forced expiratory volume in 1 s ( fev1 ) ] expressed as percentage of normal predicted values for age and sex [ 17 ] , and liver us . ultrasound protocol and arfi assessment using virtual touch tissue quantification technique us imaging was performed after a 3to 4 - h fast to obtain gallbladder distention . 
 coded variables were entered in a sonographic cfld score which ranged from 0 ( no us evidence of cfld ) to 4 ( all the parameters were present )  . 
portal hypertension ( pht ) was defined , as previously reported [ 5 ] , in the presence of one of the following criteria : a mean blood velocity < 10 cm / s at the level of the portal trunk , presence of irregular margins and nodular pattern , enlarged portal vein diameter ( measured at the porta hepatis ) , presence of portalsystemic collateral veins . 
 arfi ( acuson s2000 , virtual touch tissue quantification mode ) was performed , as follows : the right lobe of the liver was accessed through an intercostal space while the patient lay in the dorsal decubitus position with the right arm in maximum abduction . 
after the patient paused breathing , an imaging location was found that had homogeneous liver parenchyma on standard b - mode imaging , devoid of any vessels or other liver substructures . 
 swv from the liver tissue was calculated as the median value of ten successful acquisitions ( m / s ) in each patient . statistical analysis the kolmogorovsmirnov goodness - of - fit test was apsun paziente presentava storia di insufficienza epatica o di pregressa chirurgia epatobiliare . 
tutti i pazienti erano negativi per i comuni virus epatotropi ( epatite a , b , c , d , e e g , citomegalovirus e virus di epstein - barr )  . 
gli esami in programma comprendevano anche test di funzionalit polmonare , capacit vitale forzata e volume espiratorio forzato in 1 secondo ( fev1 ) , [ 17 ] ed ecografia epatica . protocollo ecografico e valutazione arfi con virtual touch tissue quantification lesame ecografico stato eseguito previo digiuno di 34 ore per ottenere la distensione della colecisti . 
le scansioni ecografiche standard b - mode ed elastosonografia con tecnica arfi associata sono state effettuate utilizzando un apparecchio s2000 siemens ( siemens medical , erlangen , germania ) dotato di trasduttori da 4 a 6 mhz . 
sono stati valutati i seguenti parametri ecografici : lepatomegalia , laumento di ecogenicit e / o la disomogeneit del parenchima , la presenza di lesioni nodulari e la regolarit dei margini epatici . 
le variabili sono state inserite in uno score ecografico di cfld compreso fra 0 ( nessuna evidenza ecografica di cfld ) e 4 ( in presenza di tutti e quattro i parametri ecografici )  . 
lipertensione portale stata definita [ 5 ] dalla presenza di uno dei seguenti reperti : velocit media del flusso a livello del tronco portale inferiore a 10 cm / s , margini epatici irregolari e pattern parenchimale nodulare , aumento di calibro della vena porta ( misurato in corrispondenza della porta hepatis ) , presenza di circoli collaterali porto - sistemici . 
lelastosonografia arfi ( acuson s2000 , virtual touch tissue quantification ) stata eseguita nella seguente modalit : il lobo destro del fegato 1412 radiol med ( 2012 ) 117 : 14081418 table 1 patient characteristics tabella 1 caratteristiche dei pazienti . 
analysis for mutation of the genes encoding for the cystic fibrosis ( cf ) transmembrane conductance regulator was performed in all patients . bmi , body mass index ; cfld , cystic fibrosis liver disease ; fev1 , forced vital capacity at 1 min ; hpt , portal hypertension ; inr , international normalised ratio ; udca , ursodeoxycholic acid i dati sono espressi come medieerrori standard della media o calcoli e percentuali . 
 bmi , indice di massa corporea ; fev1 , capacit vitale forzata a 1 min ; inr , international nomalized ratio ; udca , acido ursodeossicolico ; ast , aspartato aminotransferasi ; alt , alanina aminotransferasi ; gt , gamma - glutamil - transpeptidasi plied for determining whether sample data likely derive from a normally distributed population . 
la swv nel parenchima stata calcolata come risultato della mediana di 10 acquisizioni consecutive ( m / s ) in ogni paziente . analisi statistica previa verifica della distribuzione normale della popolazione ( test di kolmogorov - smirnov ) i dati sono stati espressi come media e intervalli di confidenza della media ( 95%ci )  . 
us abnormalities of the hepatic parenchyma were found in 63 patients ( 84% ) : 17 ( 26% ) presented at least one abnormality ; 23 ( 36% ) two of four abnormalities , 15 ( 23% ) three of four and eight ( 13% ) all us signs associated with cfld ( table 1 )  . 
alterazioni ecografiche del parenchima epatico sono state riscontrate in 63 pazienti ( 84% ) : 17 ( 26% ) presentavano almeno unanomalia , 23 ( 36% ) due delle quattro anomalie , 15 ( 23% ) tre anomalie e 8 ( 13% ) pazienti presentavano tutti i segni ecografici associati a cfld ( tabella 1 )  . 
i risultati del nostro studio suggeriscono che larfi una tecnica affidabile , non invasiva , potenzialmente utile nel follow - up clinico di questi pazienti nella detezione del coinvolgimento epatico . 
i nostri rilievi confermano i risultati di precedenti studi [ 3 ] , che hanno rilevato che lesame obiettivo e i livelli sierici di aminotransferasi , nonostante lampio utilizzo clinico , possono non essere specifici per lindividuazione di malattia epatica avanzata come invece evidente in presenza di splenomegalia e varici esofagee . 
 inoltre il rapporto tra rigidit del parenchima epatico e stadio della fibrosi stato dimostrato in studi che mettono in relazione le propriet fisiche della matrice extracellula re con lattivazione delle cellule stellate epatiche [ 19 ]  . 
2 box plots of swv in patients with no cystic fibrosis liver disease ( no cfld , n = 11 ) , portal hypertension ( pht , n = 28 ) , splenomegaly ( n = 18 ) and oesophageal varices ( n = 8 )  . 
2 box plot della swv in pazienti senza malattia epatica associata a fibrosi cistica ( no cfld , n = 11 ) , ipertensione portale ( pht , n = 28 ) , splenomegalia ( n = 18 ) e varici esofagee ( n = 8 )  . 
our results confirm previous reports [ 3 ] , which found that clinical evaluation and serum aminotransferases , despite continued widespread clinical use , may be not specific for detecting advanced liver disease , as estimated by the presence radiol med ( 2012 ) 117 : 14081418 1415 table 2 shear - wave velocity ( swv ) in patients presenting with pancreatic insufficiency and signs of liver involvement . 
p value represents the statistical significance at the mannwhitney u test or the kruskalwallis test , as appropriate swv , shear wave velocity ; cfld , cystic fibrosis liver disease tabella 2 velocit dellonda shear nei pazienti con insufficienza pancreatica e segni di coinvolgimento epatico . 
il valore di p rappresenta la significativit statistica ottenuta al test u di mann - whitney o al test di kruskal - wallis quando appropriato sign of liver involvement pancreatic insufficiency splenomegaly portal hypertension oesophageal varices ultrasound score of cfld segni di coinvolgimento epatico insufficienza pancreatica splenomegalia ipertensione portale varici esofagee score ecografico di cfld no . 
moreover , correlation between hepatic stiffness and fibrosis stage has been demonstrated in studies relating the physical properties of the extracellular matrix with activation of hepatic stellate cells [ 19 ]  . 
in patients with chronic hepatitis c , swv > 1.34 m / s was diagnostic of moderate - tosevere fibrosis ( f score between 2 and 4 ) , swv > 1.44 m / s of a stage ranging from severe fibrosis and cirrhosis , and swv > 1.80 m / s diagnostic of cirrhosis ( grade f4 ) [ 7 , 10 ]  . 
 similar results were observed in another study , which did not provide cutoff values but mean values of swv associfettivamente precedere la fibrosi come risultato sia di un incremento delledema sia dellinfiltrazione di cellule infiammatorie [ 20 ]  . 
risultati simili sono stati osservati in un altro studio , che non ha per fornito valori di cut - off , ma i valori medi di swv correlati allaumento del grado di fibrosi [ 12 ]  . 
the optimal cutoff values of swv for the diagnosis of hepatic fibrosis stages 3 and 4 were 1.77 m / s and 1.90 m / s , respectively [ 14 ]  . 
liver stiffness as a correlate of hepatic fibrosis has also been investigated with a different technique , known as transient elastography , or fibroscan [ 24 , 25 ]  . 
on the contrary , caution is warranted in interpreting us findings in patients with suspected cfld , particularly in the absence of liver nodularity and splenomegaly or in the presence of steatosis [ 3 , 26 , 27 ]  . some limitations affect this preliminary analysis . 
moreover , portal hypertension was suspected on the basis of the detection of irregular margins and a nodular pattern , not with a more reliable technique such as measurement of hepatic venous pressure gradient . 
nel loro insieme , i risultati degli studi sopra citati , sostengono con fermezza il concetto che ci sia un consistente aumento progressivo del rischio di fibrosi epatica con laumentare dei valori di swv . 
considerando i valori mediani delle stime multiple di swv per ogni lobo , vengono superati i limiti determinati dallerrore di campionamento associato alla biopsia e agli artefatti dovuti al movimento cardiaco . 
al contrario , dovrebbero essere analizzati con prudenza i risultati ecografici di pazienti con sospetta cfld , soprattutto in assenza di nodularit del fegato e splenomegalia o in presenza di steatosi [ 3 , 26 , 27 ]  . 
lipertensione portale stata sospettata sulla base della rilevazione dei margini epatici irregolari e pattern nodulare , e non attraverso una tecnica pi affidabile come la misurazione del gradiente di pressione venosa epatica . 
ulteriori studi sono necessari per migliorare la valutazione della performance della tecnica di prevedere la progressione della malattia epatica . radiol med ( 2012 ) 117 : 14081418 1417 conclusions conclusioni in conclusion , arfi with virtual touch tissue quantification is an easy , fast and noninvasive tool for the clinical follow - up of children with cf - associated liver disease . 
being a noninvasive imaging technique , arfi with swv determination may be useful for screening children with liver disease who require biopsy or upper endoscopy , sparing patients the potential complications of these procedures and reducing resource utilisation and healthcare costs . 
clinical presentation and disease course are extremely variable , as there may be acute onset with acute coronary syndrome , or cardiogenic shock , or progressive heart failure or arrhythmias . 
all patients underwent b - mode echocardiography ( echo ) and tissue doppler imaging , coronarography , ventriculography , endomyocardial biopsy and contrast - enhanced mri examination , as well as clinical and echo follow - up at 6 months . 
at 6 - month follow - up , patients were divided in two groups according to values of end - systolic volume and ejection fraction : patients with negative remodelling and those with positive remodelling . 
contrast - enhanced mri is useful both in the diagnosis and as a prognostic indicator in the clinical suspicion of myocarditis . keywords myocarditis acute coronary syndrome heart failure arrhythmias magnetic resonance imaging riassunto obiettivo . 
lesatta incidenza delle miocarditi non ben conosciuta e spesso la diagnosi viene raggiunta tardivamente o non viene raggiunta affatto ; anche la presentazione ed il decorso clinico sono estremamente variabili , potendo manifestarsi con un esordio acuto come una sindrome simil - coronarica acuta o shock cardiogeno , oppure con una insufficienza cardiaca spesso progressiva , o ancora con limprovvisa comparsa di aritmie . 
scopo del nostro studio stato il tentativo di identificare eventuali fattori prognostici alla risonanza magnetica ( rm ) eseguita allesordio della sintomatologia e dopo sei mesi in pazienti con biopsia endomiocardica positiva per miocardite . 
da gennaio a dicembre 2010 sono stati studiati 56 pazienti consecutivi in base alle possibili presentazioni cliniche suddette ( 20 con sindrome similcoronarica acuta , 20 con scompenso cardiaco e 16 con aritmie ) , tutti sottoposti ad ecocardiografia b - mode e doppler tissutale , coronarografia , ventricolografia e biopsia endomiocardica e rm con mezzo di contrasto ( mdc )  . 
i pazienti al follow - up sono stati divisi in due gruppi in base alla variazione di volume telesistolico ( vts ) e frazione di eiezione ( fe ) : pazienti con rimodellamento negativo e pazienti con rimodellamento positivo . 
la rm con mdc estremamente utile non solo per la diagnosi ma anche come indicatore prognostico nel sospetto clinico di miocardite . 1310 radiol med ( 2012 ) 117 : 13091319 parole chiave miocardite sindrome coronarica acuta insufficienza cardiaca aritmie risonanza magnetica introduction introduzione myocarditis is a common cardiac condition that is found in approximately 9% of autopsy examinations [ 1 ]  . 
it appears to be a major cause of sudden cardiac death in patients under the age of 40 years [ 2 ] ; the condition may progress to chronic dilated cardiomyopathy [ 3 ]  . 
later , other viruses , such as adenoviruses , were identified in endomyocardial biopsies of patients with suspected myocarditis and with idiopathic dilated cardiomyopathy [ 5 ]  . it is important to note that the natural course of myocarditis varies , as do clinical presentation , laboratory findings and aetiology . 
although standard echocardiography ( echo ) , tissue doppler imaging ( tdi ) , troponin assays and other noninvasive cardiac imaging techniques such as magnetic resonance imaging ( mri ) play an essential role in the diagnosis and follow - up of myocarditis [ 6 ] , it is difficult to identify prognostic factors , especially in a population of patients with dilated cardiopathy due to myocarditis . the aim of this study was to evaluate the presence of different patterns of myocardial damage and identify prognostic factors capable of predicting improvement or progression to cardiac failure by correlating the different clinical presentations , mri patterns and follow - up data in a group of patients with clinically suspected myocarditis subjected to cardiac biopsy . materials and methods between january and december 2010 , we examined 116 consecutive patients with suspected myocarditis on the basis of a combination of signs and symptoms , including chest pain , dyspnoea , fatigue , electrocardiographic alterations ( conduction blocks , st - segment abnormalities ) , arrhythmias ( supraventricular tachycardia , sustained or nonsustained ventricular tachycardia ) coupled with a history compatible with inflammatory disease , such as diarrhoea , fever , malaise and elevated c - reactive protein le miocarditi sono una patologia cardiaca comune , identificata in circa il 9% degli esami autoptici [ 1 ] , che sembra essere la principale causa di morte cardiaca improvvisa in soggetti al di sotto dei quarantanni [ 2 ] ; inoltre possono progredire in cardiomiopatia dilatativa [ 3 ]  . 
attualmente i virus sono considerati la causa pi frequente di miocarditi in nord america e in europa ; inizialmente si pensava che i coxsackie virus fossero tra le cause pi comuni di miocarditi , visto lelevato titolo anticorpale che si riscontrato nei pazienti con miocardite acuta ed in fase di convalescenza . 
successivamente , altri virus , come gli adenovirus , sono stati rinvenuti nelle biopsie miocardiche di pazienti con sospetta miocardite e con cardiomiopatia dilatativa idiopatica [ 5 ]  . importante precisare che la storia naturale delle miocarditi variabile , come variabili sono la presentazione clinica , il quadro laboratoristico , oltre leziologia . 
lecocardiografia standard e tissue doppler imaging ( tdi ) , il dosaggio delle troponine , ed altre tecniche di imaging cardiaco non invasivo come la risonanza magnetica ( rm ) forniscono un notevole contributo nellinquadramento diagnostico e nel follow - up delle miocarditi [ 6 ] , tuttavia rimane difficile individuare fattori prognostici , specie in una popolazione di individui con cardiopatia dilatativa dovuta a miocardite . a tale proposito , nel nostro studio abbiamo valutato il rapporto tra la differente presentazione clinica ed il quadro di imaging rm in un gruppo di pazienti con sospetto clinico di miocardite , sottoposti a biopsia endomiocardica , correlando tali dati al follow - up , allo scopo di valutare la presenza di differenti pattern di danno miocardico e di riconoscere un fattore predittivo in grado di valutare il miglioramento oppure la progressione verso lo scompenso cardiaco . materiali e metodi nel nostro centro abbiamo esaminato 116 pazienti consecutivi , da gennaio a dicembre 2010 , con sospetto di miocardite sulla base della combinazione di sintomi e segni quali dolore toracico , dispnea , fatica , alterazioni ecg ( blocchi di conduzione , anomalie del tratto st ) , aritmie ( tachicardia sopraventricolare , tachicardia ventricolare sostenuta o non sostenuta ) in combinazione con una storia compatibile con patologia radiol med ( 2012 ) 117 : 13091319 1311 ( crp )  . 
on admission , patients with acute coronary - like syndrome were assessed with bidimensional echo , tdi , and coronarography performed as urgent procedures , and in all other cases , as elective procedures . 
 patients were followed up at 6 months with bidimensional echo and tdi . three patterns of clinical presentation were identified : ( 1 ) chest pain associated with ventricular repolarisation changes and raised indexes of myocardial necrosis ; ( 2 ) signs and symptoms of cardiac failure such as dyspnoea , dependent oedema , asthenia ; ( 3 ) onset of arrhythmias . cardiac magnetic resonance imaging mri examinations were performed with a 1.5 - t imager ( signa excite ii echospeed , general electric medical systems , buc , paris , france ) equipped with high - performance gradients ( maximum gradient strength 33 mtm / m , maximum gradient slew rate 175 t m - 1 s - 1 )  . 
images were acquired in the fourand two - chamber long - axis views with cine - mr steady - state free precession ( ssfp ) sequences and in the short axis plane with black - blood fast spin echo ( fse ) sequences , with double inversion recovery for suppression of the blood signal and an additional inversion recovery pulse for suppression of the fat signal to demonstrate the presence of possible areas of high signal intensity caused by oedema . 
 finally , late - enhancement ( le ) images were acquired 15 min after intravenous administration of paramagnetic contrast material [ gdbenzyloxy - propionic tetraacetic acid ( bopta ) , 0.1 mmol / kg ] [ 7 ] using a t1 - weighted 2d fast gradient - echo ( fgre ) sequence with an inversion recovery preparation pulse to suppress the signal of the healthy myocardium and highlight the areas of enhancement . 
the endocardial and epicardial contours were delineated in the short - axis planes of both the cine - mr iminfiammatoria come diarrea , febbre , malessere e aumento della proteina c reattiva . 
ciascun paziente stato sottoposto al momento del ricovero a valutazione ecocardiografica bidimensionale , nonch a doppler tissutale , a coronarografia , in urgenza nei casi con presentazione simil - sindrome coronarica acuta , in elezione negli altri casi , tutti sottoposti a cateterismo cardiaco con biopsia miocardica ed a risonanza magnetica cardiaca con mezzo di contrasto paramagnetico ( gadolinio )  . 
a sei mesi stata eseguita ecocardiografia bidimensionale e doppler tissutale . sono stati identificati tre pattern di identificazione : ( 1 ) presentazione con dolore toracico associato ad alterazioni della ripolarizzazione ventricolare e movimento degli indici di miocardionecrosi ; ( 2 ) presentazione clinica caratterizzata da segni e sintomi di scompenso cardiaco quali dispnea , edemi declivi , astenia ; ( 3 ) presentazione caratterizzata dalla comparsa di aritmie . risonanza magnetica cardiaca gli esami di risonanza magnetica sono state eseguiti mediante apparecchiatura da 1 , 5 t ( signa excite ii echospeed , general electric medical systems , buc , parigi , francia ) equipaggiata con sistema di gradienti ad alte prestazioni ( maximum gradient strength 33 mtm / m , maximum gradient slew rate 175 t m - 1 s - 1 )  . 
le immagini sono state acquisite in asse lungo quattro e due camere mediante sequenze cine - rm con tecnica steady state free precession ( ssfp ) , in asse corto mediante sequenze fast spin echo ( fse ) a sangue nero con tecnica double inversion recovery per la soppressione del segnale del sangue ed ulteriore impulso inversion recovery per la soppressione del segnale del tessuto adiposo , al fine di documentare la presenza di eventuali aree di iperintensit del segnale , riferibili ad edema . 
infine sono state acquisite immagini dopo somministrazione ev di mezzo di contrasto ( mdc ) paramagnetico [ gadobenato dimeglumina ( gd - bopta ) , 0 , 1 mmol / kg ] [ 7 ] 15 minuti dopo liniezione ( tecnica late enhancement , le ) , mediante una sequenza t1pesata fast gradient echo ( fgre ) 2d con impulso di preparazione inversion recovery atto a sopprimere il segnale del miocardio sano ed esaltare le aree miocardiche caratterizzate da accumulo di mdc . 
two of the three samples were frozen for molecular studies and the remaining samples fixed in formalin and paraffall invasive procedures were carried out after the patients informed consent had been obtained . 
i profili endocardici ed epicardici sono stati delineati nelle immagini asse corto sia della cine - rm , per il calcolo della funzione contrattile regionale e degli indici di funzione sistolica globale biventricolare , sia del late enhancement , per la quantificazione in grammi del tessuto patologico . 
le biopsie miocardiche ( da 3 a 4 per ogni ventricolo ) sono state ottenute in regione setto apicale ; 2 dei 3 campioni erano congelati per gli studi molecolari . 
multiple sezioni dello spessore di 5 micron sono state colorate con ematossilina / eosina , van gieson elastico di miller , tricromia di masson , ed esaminate al microscopio ottico . 
tutti i campioni sono stati sottoposti ad immunoistochimica per la caratterizzazione degli infiltrati infiammatori . molecular biology biologia molecolare two biopsy samples from each patient were analysed with polymerase chain reaction ( pcr ) and pcr with reverse transcriptase ( rt - pcr ) to identify viral nucleic acids for the main cardiotropic viruses . due campioni bioptici da ciascun paziente sono stati sottoposti a polymerase chain reaction ( pcr ) e pcr con trascrittasi inversa , al fine di individuare acidi nucleici virali per i principali virus cardiotropi . statistical analysis statistical analysis was done with the software package spss 10.0 for windows ( spss inc . , chicago , il , usa )  . 
we used nonparametric test for unpaired data ( mann - whitney u test for comparison of two groups and kruskal - wallis test for comparison of more than two )  . 
sono stati utilizzati test non parametrici per dati non appaiati ( test di mann - whitney u quando si confrontavano due gruppi diversi e quello di kruskal - wallis quando se ne confrontavano pi di due ) .nel confronto fra pi gruppi si ricorso alla correzione di bonferroni applicata al test di mann - whitney u . 
la trasformazione logaritmica stata usata per effettuare il test post - hoc per landamento liradiol med ( 2012 ) 117 : 13091319 1313 transformation was used for the post hoc test for the linear trend at univariate analysis of variance ( anova )  . 
of these , eight presented with infarction - like syndrome , five with heart failure and three with arrhythmias . patients were followed up at 6 months by clinical assessment , echo and tdi . 
they were subdivided on the basis of the delta ejection fraction ( ef ) increase in ef at follow - up compared with baseline value , cutoff 10% and delta endsystolic volume ( esv ) reduction in esv compared with baseline , cutoff 15% , with the latter intended as a reflection of positive remodelling [ 8 , 9 ]  . negative remodelling was observed in 26 patients and was distributed as follows : 4 / 20 with acute coronary - like syndrome ; 14 / 20 with heart failure ; 8 / 16 with arrhythmias ( table 1 )  . 
sixteen patients ( nine presenting with heart failure and seven with arrhythmias ) were treated with corticosteroids on the basis of the clinical picture and molecular biology findings ; at 6 - month follow - up , they all showed a 10% in tutti i pazienti lanalisi istologica ed immunoistochimica ha confermato la presenza di miocardite linfocitaria attiva . biologia molecolare di tutti i pazienti , 16 sono risultati positivi per presenza di genoma di parvovirus . 
in 8 di questi pazienti la miocardite ha esordito come sindrome simil - infartuale , in 5 come insufficienza cardiaca , in 3 come aritmia . decorso clinico i pazienti sono stati sottoposti a follow - up a sei mesi mediante valutazione clinica , ecocardiografica e doppler tissutale . 
i pazienti sono stati suddivisi sulla base del delta della frazione di eiezione ( fe ) ( aumento della fe nel follow - up rispetto al valore basale , cut - off 10% ) e sulla base del delta del volume telesistolico ( vts ) ( riduzione del vts , cut - off 15% rispetto al basale ) , inteso questultimo come espressione del rimodellamento positivo [ 8 , 9 ]  . il rimodellamento negativo stato osservato in 26 pazienti , cos distribuito : 4 / 20 nel gruppo con presentazione simil - sindrome coronarica acuta ; 14 / 20 nel gruppo con presentazione a tipo insufficienza cardiaca , 8 / 16 nel gruppo con presentazione caratterizzata da aritmie ( tabella 1 )  . 
il gruppo dei pazienti con rimodellamento positivo era costituito da 30 pazienti , cos suddivisi : 16 pazienti con esordio simil - sindrome coronarica acuta , 6 con esordio caratterizzato da scompenso cardiaco e 8 pazienti che avevano presentato aritmie allesordio . 
si evidenzia impregnazione di mdc in sede subepicardica inferiore ed infero - laterale , in paziente con miocardite e presentazione clinica a tipo sindrome coronarica acuta . radiol med ( 2012 ) 117 : 13091319 1315 fig . 
2a short - axis 2d inversion - recovery fast gradient echo postgadolinium images , from base to apex ; intramural delayed enhancement in septal wall in a patient with myocarditis and heart failure presentation ( new york heart association class ii )  . 
del gruppo che esordiva con patologia simil - sindrome coronarica acuta , 18 pazienti presentavano le ( media le 3 , 8% lv mass range 2%21 , 2% ) ; del gruppo che esordiva con scompenso cardiaco 13 pazienti presentavano le ( media le 6% lv mass range 3 , 2%9 , 8% ) ; del gruppo che esordiva con aritmie 10 pazienti presentavano le ( media 6 , 9% lv mass range 0%5 , 2% )  . 
confrontando i due pattern di distribuzione del le si evidenziava una differenza statisticamente significativa tra il gruppo con presentazione simil - sindrome coronarica acuta e il gruppo aritmia ( p < 0 , 001 ) rispetto al gruppo sindrome coronarica acuta e scompenso cardiaco ( p = 0 , 75 )  . 
confrontando invece le due sottopopolazioni di pazienti , si osservato che lespressione del le era nettamente maggiore nel gruppo delta fe < 10% e delta vts < 15% ( rispettivamente 21 / 26 , pari all88% nel gruppo con rimodellamento negativo , rispetto a 14 / 30 , pari al 46% nel gruppo con rimodellamento positivo )  . 
inoltre raggruppando tutti i pazienti , si osservata una correlazione significativa allesordio tra valore percentuale di le e volumi telediastolici , sia sinistro ( p = 0 , 038 ) , che , soprattutto , destro ( p = 0 , 015 )  . 
si apprezza enhancement settale inferiore in sede intramurale , in paziente con miocardite e presentazione con aritmie ventricolari ( tachicardia ventricolare non sostenuta )  . discussion discussione our data suggest three distinct forms of clinical presentation . 
probably , aetiological agent affects the endothelial cells but not the myocytes , causing endothelial dysfunction and diapedesis of inflammatory cells to the myocardial interstitium with consequent damage to the myocytes . 
this combination of ischaemia and inflammation may explain the ecg changes and the raised levels of circulating troponin ; in addition , focal distribution of the inflammatory process may account for the fact that lv function is not severely impaired . the other two clinical presentations are heart failure and arrhythmias . 
probabilmente in questi pazienti agisce un agente eziologico che colpisce le cellule endoteliali ma non i miociti , causando una disfunzione endoteliale , come pure linduzione della diapedesi di cellule infiammatorie nellinterstizio miocardico con successivo danno dei miociti . 
tale combinazione di ischemia e infiammazione pu spiegare le alterazioni elettrocardiografiche e laumento del livello di troponina circolante ; inoltre la distribuzione focale del processo infiammatorio pu spiegare il fatto che la funzione ventricolare sinistra non sia severamente compromessa . le altre due presentazioni cliniche sono rappresentate dallo scompenso cardiaco e dallinsorgenza di aritmie ; queste presentazioni sono ampiamente descritte in letteratura [ 1215 ]  . 
tali pazienti presentano una significativa dilatazione e disfunzione ventricolare sinistra allesordio e recuperano di meno rispetto al gruppo precedente nel radiol med ( 2012 ) 117 : 13091319 1317 cells and virus - specific immune response play a key role [ 16 ]  . 
an abnormal immune response may explain the more severe lv dysfunction seen in these patients and the slower , if not absent , clinical and functional recovery . patterns of myocardial injury on the basis of le distribution in patients with different clinical presentations , we identified two patterns of myocardial injury . 
the first , which is present in the majority of patients presenting with acute coronary - like syndrome , has subepicardial location at the level of the left lateral wall . 
unalterata risposta immunitaria pu spiegare la maggiore disfunzione ventricolare sinistra in questi pazienti e il rallentato se non assente recupero clinico e funzionale . pattern di danno miocardico in base alla distribuzione del le nei pazienti con differente presentazione clinica abbiamo rilevato due pattern di danno miocardico . 
il primo , che presente nella maggioranza dei pazienti che esordisce con sintomatologia simil - sindrome coronarica acuta , si localizza a livello della parete laterale sinistra , in sede sub - epicardica . 
il secondo , che presente in maggioranza nelle altre due popolazioni cliniche di pazienti , si localizza a livello del setto interventricolare , a sede intramurale ; questo potrebbe spiegare il fatto che questi ultimi hanno una maggiore incidenza di aritmie ventricolari , blocchi della conduzione ed una prognosi pi sfavorevole . clinical course decorso clinico our data indicate that patients presenting with myocardialinfarction - like symptoms show an improvement in ef and recover almost completely . 
it is likely that there dai nostri dati si evince che coloro che esordiscono con una sintomatologia simil - infartuale hanno un miglioramento in termini di frazione deiezione e recuperano quasi completamente . 
if a certain threshold is exceeded , dilation may become irreversible , and this may explain why lv dilation in the acute phase may be a predictor of chronic lv dysfunction and dilation . 
se viene superata una certa soglia , la dilatazione pu diventare irreversibile e questo pu spiegare perch la dilatazione ventricolare sinistra nella fase acuta possa essere un predittore di disfunzione e di dilatazione ventricolare sinistra cronica . 
tale pattern di distribuzione settale correlato a una disfunzione e dilatazione ventricolare sinistra e pu essere riscontrato anche in pazienti con cardiomiopatia dilatativa apparentemente idiopatica [ 2729 ] , ma altri studi saranno necessari per confermare le differenti ipotesi . conclusions conclusioni late enhancement identifies a myocardial injury in patients with myocarditis . 
our study has some limitations : firstly , the biopsy and the mr examination were only performed in patients who were not excluded from the study due to coronary disease at coronarography ( there is a theoretical possibility of myocarditis coexisting with significant coronary stenosis )  . 
finally , the follow - up was performed only with ecg to evaluate positive or negative remodelling and not with mri , which means there are no data on the evolution of le at follow - up . il le identifica un danno miocardico in pazienti con miocardite e la sua differente espressione e localizzazione in grado , insieme alla presentazione clinica iniziale dei pazienti , di predire landamento clinico e funzionale di questi nel tempo . 
quando si combinano labvs , lecografia convenzionale e la mammografia , laccuratezza diagnostica , la sensibilit e la specificit raggiungono il 96 , 4% , il 97 , 1% e il 95 , 2% , rispettivamente . 
esso ha 1288 radiol med ( 2012 ) 117 : 12871293 una sensibilit significativamente maggiore della mammografia , ma simile allecografia convenzionale e non pu essere preferibile ad un esame ecografico convenzionale . 
 parole chiave ecografia 3d lesioni mammarie bi - rads mammografia ricostruzioni multiplanari introduction in manual ultrasound ( us ) , a breast lesion has to be immediately characterised during the examination . 
by using 3d us , complex growth patterns and their margins can be better appreciated in three orthogonal planes in both benign and malignant tumours . automated breast volume scanning ( abvs ) a 3d function performed with an acuson s2000 ultrasound system and abvs attachment . 
 few studies have assessed the application of abvs to the diagnosis of breast lesions [ 6 , 7 ] , and the main purpose of these studies was to compare abvs with manual us . 
 the aim of this study was to compare the diagnostic efficiency of abvs with those of manual us and mammography in the differentiation of benign from malignant solid breast masses , with histopathologic examination as the reference standard . patients and methods from may 2010 to august 2010 , mammography , manual us and abvs were performed in 155 consecutive patients ( total 165 lesions ) scheduled to undergo us - guided core needle biopsy due to suspicious breast lesions detected during screening mammography or manual us . 
all lesions were confirmed with pathology after surgical excision ( n = 112 ) or with us - guided percutaneous core needle biopsy ( n = 53 ) within 48 h of us examination . 
surgical excision was performed in 92 lesions because of suspicious or malignant findings at a previous percutaneous core needle biopsy ( n = 76 ) and referring clinician preference on clinical grounds ( n = 16 )  . 
 mammography and manual ultrasound mammograms were taken with a senograph 2000 ( ge healthcare , waukesha , wi , usa ) in craniocaudal ( 27 kv , 85 mas , mo / mo ) and mediolateraloblique views ( 27 kv , 58 mas , mo / mo )  . 
breast density was according to birads categories and / or quantification : acr 1 , almost entirely fat ( low density , up to 25% mammary gland parenchyma ) ; acr 2 , scattered fibroglandular densities ( average density , 2650% gland parenchyma ) ; acr 3 , heterogeneously dense ( high density , 5175% gland parenchyma ) ; acr 4 , extremely dense ( very high density , > 75% gland parenchyma ) [ 10 ]  . 
 a manual us examination was performed with an acuson s2000 us system ( acuson , mountain view , ca , usa ) with a 14l - 5 linear - array probe , and iu22 us system ( philips medical systems , andover , ma < usa ) with a l12 - 5 linear - array probe by one radiologist ( zlw ) with 10 years of experience in breast us . 
with the patient supine , radiol med ( 2012 ) 117 : 12871293 1289 suspect regions were imaged in two perpendicular scanning planes ( sagittal and transverse ) , and data imaging and communications in medicine ( dicom ) images were stored on hard disks . 
after completing the reading session and receiving histopathological results , diagnostic accuracy , sensitivity , specificity and positive ( ppv ) and negative ( npv ) predictive values were calculated for each method . 
the system automatically adjusts depth , frequency , focal zone placement and overall gain . a typical examination comprises three automated 65 - s scans of each breast in the anteroposterior ( ap ) and both oblique positions . 
after the acquisition is finished , proprietary postprocessing algorithms are applied based on nipple location to maximise diagnostic information quality . after acquisition , the transverse image series is automatically sent from the acuson s2000 abvs to a dedicated breast us review workstation that presents images through multiplanar reconstruction ( mpr ) and reconstructs secondary images from the acquisition volume in any plane , such as sagittal , coronal , radial and antiradial views . 
figure 1 shows an example of the three multiplanar compounded reconstructions from abvs in comparison with the mammogra data evaluation the acquired dicom data were analysed offline at a separate workstation and evaluated by two radiologists ( lg , xn ) with 5 and 6 years , respectively in mammography . 
lesion detection rates of manual us , abvs and mammography were 95.8% ( 158 / 165 ) , 97.6% ( 161 / 165 ) and 87.8% ( 145 / 165 ) , respectively . 
 1290 radiol med ( 2012 ) 117 : 12871293 fig.1a - d three multiplanar compounded reconstructions from abvs in comparison with the mammograac three orthogonal planes ( transverse , sagittal , coronal ) of the left breast from abvs . 
c , d due esempi di fibroadenomi che presentano margini ben definiti , senza segni di infiltrazione del tessuto mammario circostante . was the same or better than manual us in terms of accuracy , sensitivity , specificity , ppv and npv . 
 value of coronal plane in 3d ultrasound as the coronal plane is unique to the 3d technique and not available for conventional manual us , it is important to emphasise the role of the coronal plane in the diagnosis . 
all eight malignant lesions missed by mammography occurred in higher - density breast tissue , and all were detected by us 1292 radiol med ( 2012 ) 117 : 12871293 and abvs . 
furthermore , three cases missed by us were found by abvs , which illustrates a key advantage of an automated us system for standardised , reproducible and bilateral whole - breast imaging . 
in our study , both us and abvs had much better diagnostic sensitivity for solid breast lesions than did mammography , which demonstrates an important role of us in lesion detection [ 14 ]  . 
in particular , abvs could provide a coronal - plane image , which does not have sound attenuation and thus allows better observation of lesion margabvs may also avoid investigator - dependent and nonstandardised documentation . 
 us findings used to characterise a solid breast mass include shape , orientation , margin , echogenicity , echotexture , posterior acoustic transmission , boundary echo and presence of calcifications [ 16 ]  . 
some studies previously assessed the value of the criteria in discriminating between benign and malignant masses and concluded that margin characteristics are associated with the highest diagnostic value [ 15 , 17 ] : 3d us can be used to evaluate these features more completely in focal breast lesion classification . 
the main limitation of this study is that benign lesions confirmed by pathology should receive a long - term follow - up to confirm stability . in summary , abvs is a promising diagnostic adjunct to mammography , and the retraction phenomenon in the coronal plane of 3d us has high diagnostic capability to differentiate between benign and malignant breast lesions . 
 conflict of interest none radiol med ( 2012 ) 117 : 1443 doi 10.1007 / s11547 - 012 - 0855 - 1 erratum comparison of automated breast volume scanning to hand - held ultrasound and mammography confronto tra scansione ecografica automatica del volume mammario , ecografia convenzionale e mammografia zhi li wang jian hong xu jun lai li yan huang jie tang department of ultrasound , chinese peoples liberation army general hospital , 28 fuxing road , beijing 100853 , peoples republic of china correspondence to : zhi li wang , tel . : + 86 - 10 - 66936848 , fax : + 86 - 10 - 68161218 , e - mail : wzllg@sina.com received : 21 august 2011 / accepted : 11 october 2011 / published online : 27 july 2012 springer - verlag 2012 erratum to : la radiol med doi 10.1007 / s11547 - 012 - 0836 - 4 the original version of this article , unfortunately , contained a mistake . 
we are thus indebted to the following experts who reviewed papers which completed the peer - reviewing process within 2012 . la qualit scientifica della rivista la radiologia medica dipende dalla collaborazione qualificata e puntuale di esperti riconosciuti che hanno dedicato il loro tempo alla revisione scientifica degli articoli inviati per la pubblicazione . 
elgazzar springer - verlag berlin heidelberg , 2011 isbn 978 - 3 - 642 - 19425 - 2 e - isbn 978 - 3 - 642 - 19426 - 9 doi 10.1007 / 978 - 3 - 642 - 19426 - 9 published online : 14 may 2012 springer - verlag 2012 this 150 page text , plus 3 glossary pages are intended to give the student and professional clear , and very sound information about nuclear medicine . 
the topic is divided into 11 chapters , starting with basic considerations and ending with nuclear oncology and therapeutic applications in nuclear medicine . the authors main endeavour is to make the reader aware that nuclear medicine is an imaging modality that offers poor anatomic information in comparison with computed tomography ( ct ) or magnetic resonance imaging ( mri ) yet , on the contrary , it provides valuable and important results regarding physiologic , metabolic and molecular imaging , as well as body functions . taking into account that nuclear medicine with its reduced radiation burden , patient comfort , ease of performance , possible examination controls over time and continuous improvements in equipment and radiation tracers , it is strange how it is not , very often , the first diagnostic option offered to patients . the text is clearly written in primer style , enriched by useful images and a few tables . 
this concise book will be appreciated by all those who want an introduction to this fascinating field of up - to - date imaging modality and study of body functions . questo testo di 150 pagine pi 3 di glossario stato concepito per offrire allo studente ed al professionista chiare e ben solide informazioni sulla medicina nucleare . 
 intendimento principale dellautore di far s che il lettore si renda conto che la medicina nucleare una metodica per immagini che , rispetto alla tomografia assiale computerizzata ( tac ) ed alla risonanza magnetica ( rm ) , offre scarse informazioni anatomiche mentre , al contrario , in grado di fornire validi ed importanti contributi in merito allo studio per immagini fisiologiche , metaboliche e molecolari , nonch in merito alle funzioni corporee . 
 tenuto conto del fatto che la medicina nucleare offre un basso carico di radiazioni , comodit per il paziente , facilit di esecuzione , possibilit di controlli nel tempo , continui progressi delle attrezzature e dei traccianti radioattivi , strano come molto spesso non sia offerta come prima opzione diagnostica al paziente . il testo scritto in modo chiaro , stile bigino , arricchito da utili immagini e da qualche tabella : questo conciso volumetto verr apprezzato da tutti coloro che desiderano una introduzione a questa affascinante , moderna modalit di immagine e di studio delle funzioni corporee . 
seventeen patients ( 11 men and 6 women ; mean age 57.8 ; range 1781 ) with 17 bone lesions underwent biopsy with xperguide cbct ( philips medical system , best , the netherlands )  . 
 in 15 patients , a sample of adequate material for histopathological analysis to yield a definitive diagnosis was obtained ; in two patients , the sample was inadequate for a definitive diagnosis . 
in one of these two cases , the lesion was closely followed up for 1 year , during which it remained stable in size , and as a result , it was considered a false positive ; the other was considered a false negative . 
diciassette pazienti ( 11 maschi e 6 femmine ; et media 57 , 8 anni , range 1781 ) con 17 lesioni ossee sono stati sottoposti a biopsia percutanea con guida xperguide cbct . 
in 15 pazienti , stato ottenuto un campione di materiale adeguato per lesame isto - patologico e per giungere ad una diagnosi definitiva ; in 2 pazienti il campione risultato inadeguato per giungere ad una diagnosi . 
in uno dei 2 casi , la lesione stata seguita per un periodo di follow - up di 1 anno , durante il quale le sue dimensioni sono rimaste stabili ; pertanto questa stata considerata un falso positivo . 
la biopsia ossea sotto guida xperguide cbct pu essere considerata accurata grazie alla radiol med ( 2012 ) 117 : 13861397 1387 encouraging in terms of complication rate , diagnostic accuracy , sensitivity , specificity and reduction of ct workload . keywords percutaneous biopsy bone lesions xperguide cone - beam ct combinazione tra la possibilit di orientamento nello spazio real - time dellago e la risoluzione spaziale della fluoro - tomografia computerizzata ( tc )  . 
inoltre , i nostri risultati sono incoraggianti in termini di percentuale di complicanze , accuratezza diagnostica , sensibilit , specificit e non ultimo , riduzione del carico di lavoro del servizio tc . parole chiave biopsia percutanea lesioni ossee xperguide cone - beam ct introduction introduzione percutaneous bone biopsy is a vital step in the diagnosis of infectious and neoplastic musculoskeletal lesions . 
although open biopsy is considered the reference standard in achieving a tissue diagnosis , with a reported accuracy of 98% , it carries a risk of significant complications in up to 16% of cases , including haematoma , infection and spread of tumour cells [ 24 ]  . 
this is in contrast to percutaneous needle biopsy , which has a reported diagnostic accuracy ranging from 66% to 97% [ 1 , 2 , 5 ] and a low complication rate ( 1.1% ) [ 5 ]  . 
however , there are known drawbacks to conventional ct guidance : exposure to ionising radiation for patients and operators , the limitation of image orientation in the plane of needle insertion [ 6 ] and the lack of realtime viewing . 
the ct fluoroscopy system was developed to overcome the lack of real - time visualisation [ 7 ] , but there are several disadvantages : the significant exposure to ionising radiation for the operator ; the difficulty performing an interventional procedure within a small - size gantry ; the limited orientation of the imaging plane . 
it may therefore be difficult to choose an appropriate approach to the tissue have to be sampled . recently , a c - arm with a flat panel detector system was developed that consists of a cone - beam x - ray tube and a flat - panel detector integrated with a c - arm gantry : conebeam ct ( cbct ) ( philips medical system , best , the netherlands )  . 
this new system can be used to visualise the correct needle trajectory from the skin to the lesion under real - time fluoroscopic guidance and verify the exact location of the needle tip within the target lesion , thereby improving the diagnostic accuracy and la biopsia percutanea un passaggio essenziale nella diagnosi sia di infezioni che di lesioni neoplastiche dellosso . 
nonostante la biopsia a cielo aperto sia da considerarsi il gold standard per ottenere la diagnosi istologica , con un accuratezza riportata del 98% ; essa non del tutto scevra dal rischio di complicanze significative sino al 16% dei casi ; le complicanze comprendono : ematoma , infezione e disseminazione di cellule tumorali [ 24 ]  . 
differenti sono i dati della biopsia percutanea che ha unaccuratezza diagnostica variabile tra il 66% ed il 97% con un basso tasso di complicanze ( 1 , 1% ) [ 5 ]  . 
detto ci vi sono noti inconvenienti nellutilizzo della guida tc : lesposizione a radiazioni ionizzanti sia per il paziente che per loperatore , i limiti nella visualizzazione dellorientamento dellago nei diversi piani [ 6 ] e la mancanza di una visione in tempo reale . 
il sistema di fluoro - tc stato sviluppato nel tentativo di colmare limpossibilit di avere una visualizzazione in tempo reale [ 7 ] , ma nonostante ci vi sono ulteriori svantaggi : limportante esposizione alle radiazioni ionizzanti dell operatore , la difficolt di eseguire la procedura quando il gantry di piccole dimensioni e il limitato orientamento del piano di visualizzazione . 
pertanto pu essere difficile scegliere un approccio appropriato al tessuto su cui eseguire la biopsia . recentemente stato sviluppato un arco a c con un detettore flat panel ; esso consiste in un tubo radiogeno di tipo cone - beam con un detettore flat panel integrati con un gantry ad arco a c , cone - beam tc ( cbct ) ( philips medical system , best , paesi bassi )  . 
inoltre , il sistema cbct fornisce alloperatore sia un sistema di visua1388 radiol med ( 2012 ) 117 : 13861397 efficacy of percutaneous needle biopsies and enhancing the operators confidence during the procedure . 
furthermore , the previous limitations of ct fluoroscopy systems , such as a small gantry bore and limited gantry orientation , can easily be overcome with this cbct systeseveral studies have already demonstrated the usefulness of cbct systems during interventional procedures [ 811 ]  . 
the purpose of this study was to determine the diagnostic performance of cbct - guided percutaneous needle core biopsy in patients with bone lesions . materials and methods patients from may 2009 to september 2010 , 17 patients ( 11 men and six women ; mean age 57.8 ; range 1781 ) with 17 bone lesions underwent biopsy with xperguide cbct ( table 1 )  . 
all cases were discussed in a multidisciplinary meeting involving musculoskeletal interventional radiologists , orthopaedic surgeons , oncologists and pathologists , at which a decision was made to perform percutaneous bone biopsy in accordance with guidelines described by liu et al . 
questo nuovo sistema pu essere utilizzato al fine di visualizzare la corretta traiettoria dellago dalla cute sino allinterno della lesione , il tutto sotto guida fluoroscopica real - time ed inoltre consente di verificare la corretta posizione della punta dellago all interno della lesione con la modalit tc del sistema cbct ; ci migliora laccuratezza diagnostica e lefficacia delle biopsie percutanee ed aumenta la confidenza delloperatore durante la procedura . 
lo scopo di questo studio stato quello di determinare la performance diagnostica delle biopsie ossee percutanee eseguite con tale sistema . materiali e metodi pazienti da maggio 2009 a settembre 2010 , 17 pazienti ( 11 maschi e 6 femmine ; et media 57 , 8 anni , range 1781 anni ) con 17 lesioni ossee sono stati sottoposti a biopsia ossea percutanea con xperguide cbct ( tabella 1 )  . 
adequate antibiotic prophylaxis was used . baseline imaging pretreatment imaging consisted of an x - ray examination in five patients and a skeletal multidetector computed tomography ( mdct ) scan in all patients ( aquilion 64 , toshiba , tokyo , japan )  . 
each mdct scan was acquired with a thickness of 0.5 mm , voltage of 120 kv and tube current of 250 ma . equipment imaging guidance all procedures were performed with xperguide cbct ( philips medical system )  . 
the biopsy route was also discussed in order to avoid needle penetration and contamination of uninvolved muscle compartments , in accordance lo - scheletrica , chirurghi ortopedici , oncologi e patologi ; stata quindi presa la decisione di eseguire una biopsia ossea percutanea in accordo con le linee guida sulle biopsie delle lesioni ossee descritte da liu et al . 
nei casi in cui era in corso un trattamento anticoagulante e / o antiaggregante , questo stato sospeso 7 giorni prima della procedura e , quando necessario , stato sostituito con la somministrazione di eparina frazionata . 
una adeguata profilassi antibiotica stata effettuata in tutti i casi . imaging di base le indagini radiologiche eseguite prima della procedura sono state un rx in 5 pazienti ed una tc multistrato dei segmenti ossei coinvolti ( tcms ) in tutti i pazienti ( aquilion 64 , toshiba , tokio , giappone )  . 
ogni acquisizione tcms stata ottenuta con uno spessore di slice di 0 , 5 mm , 120 kv di voltaggio e 250 ma di amperaggio . 1390 radiol med ( 2012 ) 117 : 13861397 fig . 
2 limmagine mostra il tragitto dellago dal punto di ingresso cutaneo ( in viola ) al punto target ( in verde )  . with the biopsy guidelines for limb - sparing surgery of the extremities [ 12 ]  . equipaggiamento guida imaging biopsy equipment the biopsy needle system to be used was selected on the basis of lesion characteristics . 
 xperguide cbct examination was performed with a single - plane c - arm angiography system equipped with a flat - panel detector ( allura xper fd20 , philips healthcare )  . 
this system is equipped with software for the following three beam ct modes : 3d rotational antutte le procedure sono state eseguite con xperguide cbct ( philips medical system , best , paesi bassi )  . 
il tragitto dellago stato pianificato al fine di non attraversare o contaminare compartimenti muscolari sani , in accordo con le linee guida suddette , biopsy guidelines for limb - sparing surgery of the extremities [ 12 ]  . strumentazione per la biopsia il sistema di prelievo utilizzato per la biopsia stato scelto in relazione alle caratteristiche della lesione . 
nelle lesioni totalmente sclerotiche , in quelle con margine sclerotico o ancora in quelle con una componente extraossea molto sottile ( < 1 cm ) la biopsia stata eseguita con un sistema coassiale costituito da un ago da vertebroplastica 13 g ( optimed medizinische instrumente gmbh , ettlingen , germania ) attraverso il quale veniva introdotto un ago 16 g ( cook inc europe , bjaeverskov , danimarca )  . 
3a , b dopo il posizionamento dellago , una scansione cbct conferma lesatto posizionamento dellago allinterno della lesione ; visione assiale ( a ) e visione coronale ( b )  . giography ; xperct ( philips healthcare ) low definition , low dose ; xperct high definition , high dose . 
the differences were as follows : 3d rotational angiography , 120 projections , 4.1 - s scanning time ; xperct low definition , 300 projections , 10 - s scan time ; no - plano ad arco a c con sistema flat - panel ( allura xper fd20 , philips medical system , best , paesi bassi )  . 
il detettore ha un campo di vista di 3830 cm2 ed una matrice di 24801920 pixels ed un pixel pitch di 154 questo sistema dotato di un software con le seguenti 3 modalit beam tc : angiografia rotazionale 3d , xperct ( philips healthcare ) a bassa definizione ed a bassa dose ed infine xperct ad alta definizione e ad alta dose . 
le differenze sono le seguenti : angiografia rotazionale 3d , 120 proiezioni , tempo di acquisizione di 4 , 1 secondi ; xperct a bassa definizione , 300 proiezioni , tempo di acquisizione di 10 secondi ; xperct ad alta definizione , 600 proiezioni , tempo di acquisizione di 20 secondi . 
le acquisizioni cbct sono state ottenute in modalit rotazionale con i seguenti parametri : distanza sorgente - detettore 1200 mm ; distanza sorgente - asse rotazionale 810 mm ; distanza detettore - asse rotazionale 390 mm ; velocit di rotazione 55 / secondo ; durata della rotazione 4 , 1 secondi ; range totale di traiettoria dellarco 240 ; numero di proiezioni 120 ; misura della matrice 10241024 e controllo automatico dellesposizione . 
sono evidenziabili piccole bolle aeree nel contesto della lesione . 1392 radiol med ( 2012 ) 117 : 13861397 xperct high definition , 600 projections , 20 - s scan time . 
cbct acquisition data were acquired in the propeller mode with the following parameters : sourcedetector distance 1 , 200 mm ; sourcerotation axis distance 810 mm ; detectorrotation axis distance 390 mm ; rotation speed 55s ; rotation duration 4.1 s ; total arc trajectory range 240 ; number of projections 120 ; matrix size 1 , 0241 , 024 pixels ; automatic exposure control . 
 acquisition frames were transferred via an optical link in real time to the 3d rotational angiography workstation ( allura release 6.2 , philips healthcare ; precision 670 , dell )  . xperguide cbct bone biopsy technique the patient was placed either supine or prone depending on lesion location . 
subsequently , the systems xperguide functionality , needle planning and navigation software tool , which creates an overlay of live fluoroscopy and 3d soft - tissue images ( philips xperct ) , was used in the next phases of the procedure . 
first , the 3d volume reconstructed from the xperct images was used to plan the needle trajectory from the skin entry point to the centre of the lesion ( target location )  . 
the software also calculates the position of the x - ray tube to view the entry point of the needle on the skmoreover , it is used to automatically move the gantry and precisely align the needle to the determined path . 
the determined path was projected onto real - time fluoroscopy images together with an overlay of the xperct images to allow exact needle placement on the patients skin and constant monitoring and adjustments during needle progression . 
progression of the needle into the patient was followed in real time under fluoroscopic guidance after selecting the progression view , which rotates the gantry 90 perpendicularly to the trajectory . 
the number of needle passes depended on the subjective quality of the material obtained as assessed by visual inspection and typically ranged from two to four passes , as reported by wu et al . 
nelle diverse fasi della procedura , per la pianificazione del tragitto dellago sono state utilizzate la modalit xperguide ed il software di navigazione ; questultimo crea una sovrapposizione della fluoroscopia real time e delle immagini 3d preacquisite dei tessuti molli ( philips xperct )  . 
il tragitto determinato viene proiettato in fluoroscopia in tempo reale sovrapponendo le immagini xperct , cos da permettere lesatto posizionamento dellago sulla superficie cutanea del paziente , ed il suo continuo monitoraggio durante la progressione . 
la progressione dellago allinterno del paziente direttamente visualizzato in fluoroscopia dopo aver selezionato la finestra di avanzamento ago , la quale determina una rotazione del gantry di 90 perpendicolarmente alla traiettoria . 
il numero dei passaggi dellago dipende dalla qualit soggettiva delloperatore all ispezione visiva del materiale ottenuto , tipicamente esso varia dai 2 a 4 passaggi in accordo con quanto descritto da wu et al . 
ogni biopsia stata classificata come adeguata o inadeguata sulle base del risultato istopatologico ; adeguata quando stato ottenuto un campione di materiale sufficiente per lanalisi istopatologica , in modo da ottenere una diagnosi definitiva di lesione maligna o benigna . 
each biopsy was classified as adequate or inadequate on the basis of the histopathological report : adequate when a sample of sufficient material was obtained for histopathological analysis to yield a definitive diagnosis of a benign or malignant lesion ; inadequate when the sample was insufficient to yield a definitive diagnosis . the needle core biopsy results were correlated with histopathological diagnosis of surgical specimens in patients who underwent curettage or resection of the benign or malignant lesion . 
moreover , a lesion characterised by pathological examination revealing nonspecific findings was designated as benign when follow - up images ( for a period of 1 year at least ) showed stability or decrease in size . 
therefore , accuracy was determined on histological diagnosis on the tissue core , possibly confirmed by surgical histology , and for cases with nonspecific histological findings , with a follow - up of 1 year at least . 
 complications were classified as major or minor in accordance with the classification system of the society of interventional radiology [ 14 ]  . results a technical success of 100% was obtained , which means that correct positioning of the needle within the lesion was possible in all cases . 
 among biopsies designated as adequate , ten were malignant ( four metastasis and six primary bone tumours ) , and six were benign according to clinical , histopathological and imaging follow - up . 
diagnostic accuracy , sensitivity and specificity were 94.12% ( 16 / 17 ) , 90.91% ( 10 / 11 ) and 100% ( 6 / 6 ) , respectively . no major complications were recorded . 
quindi laccuratezza diagnostica stata determinata sulle basi del risultato dellesame istologico sul frustolo bioptico , eventualmente confermata dallesame istologico sul reperto chirurgico e per i casi con esame istologico non specifico con stabilit al follow - up per almeno un anno . 
i casi con biopsia non diagnostica o con un follow - up di durata inferiore ad un anno sono stati considerati come possibili maligni e conseguentemente definiti come falsi negativi . 
le complicanze sono state classificate come maggiori o minori in accordo con il sistema di classificazione della societ di radiologia interventistica [ 14 ]  . risultati il successo tecnico stato del 100% , il che significa che in tutti i casi stato possibile posizionare correttamente lago allinterno della lesione . 
in uno di questi due casi , il follow - up ad un anno ha dimostrato una stabilit dimensionale della lesione e pertanto questa lesione stata inclusa nel gruppo dei falsi positivi ( tabella 2 )  . 
 tra le biopsie definite come adeguate 10 erano lesioni maligne ( 4 metastasi e 6 tumori ossei primitivi ) e 6 erano lesioni benigne in accordo con la clinica , i risultati istopatologici ed il follow - up allimaging . 
laccuratezza diagnostica , la sensibilit e la specificit sono state del 94 , 12% ( 16 / 17 ) , 90 , 91% ( 10 / 11 ) e 100% ( 6 / 6 ) rispettivamente . non stata osservata nessuna complicanza maggiore ; solo in un caso ( in una lesione dellosso iliaco ) stato registrato un modico sanguinamento con successivo ematoma che si risolto in circa 15 giorni . 
recentemente la risonanza magnetica stata identificata come tecnica di imaging per lesecuzione di biopsie di lesioni difficilmente visualizzabili con le altre metodiche , in adiacenza a strutture critiche [ 17 ]  . radiol med ( 2012 ) 117 : 13861397 1395 have become the standard imaging methods used to guide musculoskeletal needle biopsies , yielding excellent results [ 15 ]  . 
recently , mri has been described as a technique for percutaneous musculoskeletal biopsies in lesions that might otherwise be difficult to visualise using other techniques or lesions adjacent to critical structures [ 17 ]  . 
 [ 20 ] reported an accuracy rate of 81% for bone lesions sampled with ct guidance . the literature contains few reports about the use of ct fluoroscopy during interventional radiological procedures . 
subsequently , others authors [ 18 ] hypothesised and / or described the application of ct fluoroscopy guidance for radiological interventional procedures , such as hepatic radiofrequency [ 19 ] , managing spinal pain [ 22 ] , during bone tumour surgery in a series of five patients [ 23 ] and in a case of plasma - mediated radiofrequency ablation followed by percutaneous cementoplasty [ 24 ]  . the use of xperguide cbct during interventional radiological procedures was described by our group [ 10 ] during microwave ablation of lung lesions and by some other authors in a few other procedures , such as vertebroplasty or needle biopsy positioning [ 8 , 9 ]  . 
xperguide cbct may be considered an alternative to reduce the workload of ct , to obtain an accurate approach of the coaxial introducer and technically successful sampling , resulting in high diagnostic accuracy . 
the 3d imaging data sets attained with cbct can also provide an advantage over the other methods , as they can be easily manipulated to allow multiplanar reconstruction through any part of the imaged object and demonstrate the trajectory angle of the approach with high spatial resolution . 
this approach also provides accurate information enabling modification of the angle and distance of the coaxial introducers approach during the procedure , resulting in a higher technical success rate and diagnostic accuracy . 
 [ 13 ] hanno riportato unaccuratezza diagnostica migliore nelle lesioni litiche rispetto alle lesioni sclerotiche , in quelle pi voluminose ed in quelle in cui si sono ottenuti frustoli di dimensioni maggiori . 
 [ 20 ] hanno dimostrato che laccuratezza diagnostica delle biopsie ossee percutanee sotto guida tc dell81% . in letteratura ci sono pochi lavori riguardo luso della fluoro - tc nelle procedure di radiologia interventistica . 
successivamente altri autori [ 18 ] hanno descritto luso della fluoro - tc in procedure di radiologia interventistica quali la radiofrequenza epatica [ 19 ] , il controllo del dolore spinale [ 22 ] , durante procedure chirurgiche di tumori ossei in un esperienza di 5 pazienti [ 23 ] e durante unablazione con radiofrequenza plasma - mediata seguita da cementoplastica percutanea in un case - report [ 24 ]  . luso dellxperguide cbct durante le procedure di radiologia interventistica stato descritto dal nostro gruppo [ 10 ] durante lablazione con microonde di lesioni polmonari e da alcuni altri autori in poche procedure come la vertebroplastica o il posizionamento dellago durante biopsia [ 8 , 9 ]  . 
 [ 11 ] hanno descritto la loro iniziale esperienza nellesecuzione di biopsie trans - toraciche di noduli polmonari utilizzando il sistema c - arm cbct . secondo le nostre conoscenze , questo il primo studio che valuta laccuratezza dellxperguide cbct durante le biopsie ossee . 
lxperguide cbct pu essere considerata una valida alternativa al fine di ridurre il carico di lavoro della tc , per ottenere un adeguato utilizzo del sistema coassiale e per ottenere prelievi bioptici validi cos da garantire una elevata accuratezza diagnostica . 
il sistema di imaging 3d ottenuto con le immagini cbct presenta un ulteriore vantaggio rispetto alle altre metodiche : le ricostruzioni multiplanari permettono di individuare la traiettoria dellago , con tutte le angolature possibili , ottenendo una elevata risoluzione spaziale . 
questo sistema permette , inoltre , modificazioni della traiettoria dellago e / o di tutto il sistema coassiale , durante la procedura stessa , garantendo un pi alto successo tecnico ed un elevata accuratezza diagnostica . 
inoltre gli operatori in tc devono manovrare lago direttamente con le mani o comunque con un porta aghi allinterno del gantry , con una conseguente elevata esposizione radiante delle mani dello1396 radiol med ( 2012 ) 117 : 13861397 tors must handle the needle manually or with the aid of a needle holder device within the limited ct gantry , resulting in considerable radiation exposure to the operators hand and unavoidable discomfort during the performance of the procedure . 
although the factors associated with an inadequate biopsy are probably not dependent on the size and number of the tissue cores , the number of procedures was too low to draw conclusions . 
we are planning a comparative study with a prospective randomised design that might be able to provide a definitive answer on which imaging guidance system is the best for the biopsy of bone lesions . 
as previously mentioned , the possibility of performing biopsies in the angiographic suite using the xperguide cbct is an important advantage in terms of reducing the workload of the ct service . peratore ed un inevitabile discomfort durante lesecuzione della procedura . 
i fattori associati con biopsia inadeguata probabilmente non dipendono dal numero e dalle dimensioni del frustolo ; il numero delle procedure per troppo basso per estrapolare delle conclusioni al riguardo . 
stiamo pianificando uno studio comparativo randomizzato prospettico che potrebbe darci una risposta definitiva su quale tecnica per immagini sia la migliore da usare come guida per le biopsie di lesioni ossee . 
luigi gonzaga hospital , regione gonzole 10 , 10043 orbassano , torino , italy 2radiation oncology unit , department of medical and surgical sciences , university of torino , s . 
for a threshold 5 mm , the two systems provided corresponding setup errors along the y and z axes , whereas along the x axis , the threshold was not necessary . 
alignrt is an accurate technique for setup in 3d - crt prostate cancer patients , especially along the lateral direction . keywords surface imaging system alignrt prostate cancer conformal radiotherapy setup reproducibility riassunto obiettivo . 
il corretto set - up rappresenta un requisito fondamentale della radioterapia conformazionale ( 3d - crt ) ed i sistemi di registrazioni di immagini di superficie rappresentano una delle metodiche utilizzate per la verifica . 
per la soglia di 5 mm gli errori di set - up rilevati dal alignrt lungo gli assi y , z e x sono stati osservati nel 47 , 4% , 42 , 1% e 5 , 3% dei pazienti , rispettivamente . 
alignrt un sistema accurato per la valutazione del set - up nei pazienti sottoposti a 3d - crt , specialmente lungo la direzione laterale . parole chiave sistema di registrazione di immagini di superficie corporea alignrt tumore della prostata radioterapia conformazionale riproducibilit del set - up 1420 introduction conformal radiotherapy ( 3d - crt ) of prostate cancer has the aim of increasing the dose delivered to the clinical target volume ( ctv ) while sparing critical organs , and therefore the margins around the ctv should be maximally reduced . 
the techniques include standard megavoltage electronic digital portal images ( dpi ) [ 2 ] , kilovoltage ( kv ) x - ray localisation of implanted clips [ 3 ] , optical imaging [ 4 , 5 ] and video imaging [ 69 , 9 ]  . 
 in this study we collected , analysed and compared target registration errors , using a surface imaging system , with setup errors determined from dpi in 19 prostate cancer patients treated with 3d - crt at the radiation oncology unit , san giovanni battista hospital , university of turin , with the aim of verifying the validity of this video - based system . materials and methods patient population radiol med ( 2012 ) 117 : 14191428 introduzione lo scopo della radioterapia conformazionale ( 3d - crt ) nel tumore della prostata quello di aumentare la dose somministrata al volume bersaglio e risparmiare gli organi critici e quindi i margini intorno al clinical target volume ( ctv ) saranno minimi . 
i fattori che influenzano la riproducibilit del target durante il trattamento e tra le sedute di rt sono lo spostamento degli organi interni tra le sedute e il movimento degli organi interni durante la seduta stessa . 
dimostrato che per il paziente affetto da tumore della prostata lerrore di set - up lungo lasse laterale maggiore rispetto allerrore di set - up lungo gli altri assi [ 1 ]  . 
le tecniche includono le immagini portali ( dpi ) [ 2 ] , la localizzazione di reperi radiopachi attraverso immagini kilovoltage ( kv ) [ 3 ] , le immagine ottiche [ 4 , 5 ] e le immagini video [ 69 ]  . 
le immagini portali acquisite durante il trattamento e la loro analisi , sono dirimenti per eliminare significativamente gli errori sistematici e casuali presenti nella pratica clinica [ 1 ]  . 
 in questo studio abbiamo raccolto , analizzato e confrontato gli spostamenti del target , usando un sistema di registrazioni di immagini di superficie , con gli errori di set - up del paziente ottenuti con il dpi , in 19 pazienti affetti da tumore della prostata sottoposti a 3d - crt presso lunit di radioterapia oncologica , ospedale san giovanni battista , universit di torino con lobiettivo di verificare la validit di questo sistema basato sulle immagini from july 2009 to december 2009 , 19 patients affected by adenocarcinoma of the prostate and subjected to external radiotherapy were enrolled in this study . 
all patients underwent a planning computed tomography ( ct ) scan in the supine position with kneefix and feetfix immobilisation device ( civco , the netherlands ) , filled bladder , empty rectum and an endorectal catheter . 
ct slices materiali e metodi caratteristiche dei pazienti in questo studio sono stati arruolati , da luglio 2009 a dicembre 2009 , 19 pazienti affetti da adenocarcinoma della prostata e sottoposti a radioterapia conformazionale . 
three skin tattoos , two lateral and one anterior , were performed for setup verification by alignment to a mobile laser systethe ct images were transferred to the treatment planning system ( oncentra masterplan v 3.0 , nucleotron , the netherlands ) to define the volumes of interest . 
the planning target volume ( ptv ) was derived by automatic expansion of ctv of 12 mm in the craniocaudal direction , 10 mm in the lateral and anterior directions and 8 mm in the posterior direction . 
patients were treated with five individually shaped coplanar fields ( 0 , 45 , 90 , 270 , 315 ) delivered with 10 - mv photons produced by a clinic varian 2500 c / d in daily fractions of 2 gy . 
orthogonal portal images for treatment verification were acquired at the beginning of 3dcrt and weekly for each enrolled patient and subsequently compared with digitally reconstructed radiographs ( drrs ) generated from the planning ct scans . image acquisition system a commercially available video - based 3d surface - imaging system ( alignrt ; visionrt , london , uk ) was installed in sono stati definiti in sovrappeso e tre pazienti sono stati definiti obesi . 
per tutti i pazienti in studio stata eseguita una tomografia computerizzata ( tc ) di pianificazione in posizione supina , con la vescica piena , il retto vuoto e una sonda rettale ed stato utilizzato un sistema dedicato e personalizzato per limmobilizzazione dei pazienti ( kneefix and feetfix , civco , nl , usa )  . 
mediante un software di simulazione virtuale , durante la tc , stato identificato lisocentro a livello della ghiandola prostatica e sono stati eseguiti tre tatuaggi , allineando il sistema dei laser ( uno anteriore e due laterali ) , per la verifica del set - up . 
le immagini tc acquisite sono state trasferite al sistema per la pianificazione del trattamento ( oncentra masterplan v 3.0 , nucleotron , nl , usa ) e utilizzate per la definizione dei volumi di interesse radioterapico . 
il planning target volume ( ptv ) stato ottenuto espandendo il ctv di 12 mm a livello cranio - caudale , 10 mm anteriormente e lateralmente e 8 mm posteriormente . 
la 3d - crt stata effettuata mediante tecnica isocentrica a 5 campi co - planari ( 0 , 45 , 90 , 270 , 315 ) sagomati , utilizzando fotoni x con energia di 10 mv prodotti da un clinic varian 2500 c / d in frazioni giornaliere di 2 gy . 
alignrt is designed as a patientsetup device ( classified as a class ii device ) used to image the skin surface of a patient in 3d before and during radiotherapy treatment . 
the surface - imaging device consists of two camera pods mounted in the linear accelerator room under an oblique angle of 30 with respect to the treatment table ; each pod contains camera and flash systems that allow the capture of 3d surface information . 
this reference image is generated by either recording the surface of a patient placed in a conventional radiotherapy simulator in which the system is installed or by importing skin contours from ct volumetric data . 
if a movement from the position of the reference surface image is detected , the software calculates new coordinates to adjust the treatment couch to the original position of the patient . 
the roi consisted of the lower abdomen from the umbilical region to all sacru during the first treatment session , patients were aligned using standard lasers and skin tattoos , and two orthogonal portal images were acquired ( 090 )  . 
al fine di verificare la correttezza del trattamento , sono state acquisite , alla prima seduta e successivamente con cadenza settimanale , le immagini portali e successivamente confrontate con le radiografie digitali ricostruite ( drrs ) ricavate dal piano di cura del trattamento radioterapico . sistema di acquisizione di immagini un sistema di registrazione di immagini di superficie corporea ( alignrt ; visionrt , london , regno unito ) stato installato nella sala di trattamento presso il reparto di radioterapia oncologica , universit di torino . 
lalignrt un dispositivo per il controllo del set - up del paziente ( classificato come dispositivo di classe ii ) ed usato per acquisire un immagine in 3d della superficie corporea del paziente prima e durante il trattamento radioterapico . 
il sistema composto da due unit ottiche con telecamere stereoscopiche che sono saldamente fissate al soffitto della sala di trattamento e poste a 30 rispetto alla verticale e focalizzate entrambe verso lisocentro del linac . 
le immagini vengo registrate in un punto dellatto respiratorio sempre ripetibile.per il set - up del paziente , lalignrt genera una immagine di superficie di riferimento della posizione di trattamento ottimale determinata durante la simulazione . 
questa immagine di riferimento pu essere generata o durante la simulazione di radioterapia registrando la superficie del paziente se presente lalignrt nella sala di simulazione o importando i contorni volumetrici dalla tc . 
se viene rilevato uno spostamento dalla posizione di riferimento , il software calcola le nuove coordinate da dare al lettino per riportare il paziente alla posizione originale . protocollo di acquisizione delle immagini in questo studio limmagine di superficie di riferimento della regione di interesse ( roi ) stata generata importando i contorni volumetrici dalla tc . 
1 distribuzione degli spostamenti individuati con dpi nelle tre direzioni ( vrt , verticale ; lat , laterale ; lng , longitudinale )  . tematic and random errors were calculated and reported as mean and standard deviation ( sd )  . 
setup errors detected by dpi in the vertical ( z ) , lateral ( x ) and longitudinal ( y ) directions and the respective p values are reported in figure 1 . 
 durante la prima seduta di trattamento , i pazienti sono stati allineati secondo i laser e secondo i tatuaggi e sono state acquisite due immagini portali ortogonali ( 090 )  . 
gli errori sistematici e random sono stati calcolati e riportati come media e come deviazione standard ( ds )  . dpi > threshold threshold 3 mm 4 mm 5 mm vrt 62% 52% 41% lng 71% 56% 47% vrt , vertical ; lat , lateral ; lng , longitudinal soglia 3 mm 4 mm 5 mm dpi > soglia vrt 62% 52% 41% lng 71% 56% 47% vrt , verticale ; lat , laterale ; lng , longitudinale risultati sono state ottenute complessivamente 653 immagini alignrt ( media di 34 , 37 immagini per paziente ) e 99 immagini portali ( media di 5 , 2 immagini per paziente )  . 
la distribuzione degli errori di set - up individuati sulle immagini dpi nelle direzioni verticale ( z ) , laterale ( x ) e longitudinale ( y ) e i rispettivi valori di p sono riportati nella figura 1 . 
la maggior parte sono stati effettuati in ambito toracico e per i tumori della mammella e hanno dimostrato come i sistemi di registrazione di immagini di superficie possono migliorare la precisione del set - up e come sono affidabili nel ridurre gli effetti delle escursioni respiratorie [ 2 , 7 , 12 ]  . 
 [ 10 ] sono stati analizzati gli errori di set - up in 22 pazienti affetti da adenocarcinoma prostatico , confrontando gli spostamenti rilevati da un sistema di registrazione di immagini di superficie corporea ( axis 2100 network camera , svezia ) con quelli rilevati dalle immagini portali . 
gli autori hanno analizzato solo gli spostamenti lungo la direzione laterale rilevati dalle due metodiche e hanno osservato che la correlazione presente tra i due sistemi era maggiore che quella tra la posizione del marker e gli errori rilevati dalle immagini portali . 
gli autori hanno concluso che questo sistema un metodo accurato per determinare gli errori di set - up lungo la direzione laterale e potrebsystems detected similar setup errors , with a statistical significance for each threshold level , whereas along the vertical and longitudinal directions , the two systems showed similar shifts only for the threshold level of 5 mm . discussion in modern radiotherapy multiple approaches are used to obtain data on patient position at various treatment sites . 
4 confronto fra dpi e alignrt in funzione delle soglie ( vrt , verticale ; lat , laterale ; lng , longitudinale ) : diagramma dei valori di p . studies investigating the use of these systems [ 2 , 6 , 7 , 913 ] have been published . 
most of them were performed on patients with intrathoracic and breast cancers and showed that surface - imaging systems may improve setup precision and are reliable for reducing the effects of respiratory motion [ 2 , 7 , 12 ]  . 
ploeger and colleagues [ 10 ] analysed setup errors in 22 patients affected by prostate cancer by comparing the shifts detected by video - surface imaging ( axis 2100 network camera , sweden ) with those obtained by dpi . 
the authors analysed only errors along the lateral direction detected by portal and video - surface images ; they observed that the correlation between the two systems was higher than the correlation between the marker position and the portal images error . 
 [ 14 ] investigated the reproducibility of patient setup by using a video - surface imaging registration system ( alignrt ) in a series of 16 patients affected by prostate cancer and treated with curative 3d - crt . 
analysis of systematic and random errors ( calculated using van herks formula ) showed that the mean largest systematic error was found on the z axis and the highest sd in the x axis , similar to what was observed by ploeger et al . 
furthermore , the authors analysed the distribution of positioning errors along the three main axes detected by the alignrt syste for a threshold > 5 mm , shifts along the x axis were observed in 14% of patients , whereas along the other axes ( y and z ) , deviations occurred , respectively , in 2% and 5% of patients . 
 [ 14 ] hanno analizzato la riproducibilit del set - up del paziente utilizzando un sistema di registrazioni di immagini ( alignrt ) in 16 pazienti affetti da adenocarcinoma prostatico e sottoposti a 3d - crt con intento curativo . 
le immagini ottenute dallalignrt sono state confrontate con le immagini portali ed stata osservata una correlazione statisticamente significativa tra le due metodiche , come dimostrato dalla regressione lineare tra gli errori di posizionamento rilevati dai due sistemi che variava tra 0 , 77 e 0 , 92 , con una media di 0 , 85 e una deviazione standard di 0 , 13 . 
lanalisi degli errori sistematici e casuali ( calcolati usando la formula di van herks ) ha dimostrato che lerrore sistematico maggiore stato rilevato lungo lasse z e la deviazione standard maggiore stata rilevata per lasse x , similmente a quanto osservato da ploeger et al . 
prendendo in considerazione la soglia di 5 mm , gli spostamenti maggiori sono stati osservati lungo lasse x ( 14% ) , mentre lungo gli altri assi ( y e z ) , gli errori maggiori di 5 mm sono stati osservati rispettivamente solo nel 2% e 5% dei casi . 
gli autori hanno concluso che lalignrt un metodo affidabile e riproducibile nel ridurre quotidianamente gli errori di set - up ; tuttavia nello studio non sono stati analizzati la rotazione , il movimento intrafrazione e le escursioni respiratorie , parametri che possono influenzare il posizionamento del paziente . 
inoltre , come immagine di riferimento non stata utilizzata la tc di pianificazione del trattamento , ma radiol med ( 2012 ) 117 : 14191428 1427 profiles , mainly due to changes in content of the bowel and rectualso , for a threshold > 3 mm , shifts along the x axis were observed in 37% of patients , whereas along the other axes , deviations were observed in 14% and 28% of patients , respectively . 
the authors concluded that the alignrt system is a reliable and reproducible device to prevent daily setup errors , but they did not analyse parameters that may affect patient setup regarding rotation , intrafraction motion and breathing movements . 
moreover , they did not correlate surface images with ct images but only with dpi , and they used as a reference image the acquisition at the time of the first radiotherapy session . in this study we analysed in 19 patients the daily setup errors detected by alignrt along the three directions during every rt treatment session using ct study as reference images . 
also for the threshold of 3 mm , movements along the y and z axes were observed in the majority of patients ( 68% and 69% , respectively ) ; in the x axis , errors occurred in 10% of patients only . 
 comparing the setup errors detected by alignrt and dpi , we found a statistically significant difference in the detection of shifts along longitudinal and vertical directions , where the optical system showed an overestimation of these shifts . 
however , results obtained with the two systems were in good agreement for a smaller threshold value for the lateral shiwe supposed that the alignrt system is more reliable in the lateral direction because it is able to acquire a larger surface image . considering dpi - drr matching only , the values are significantly shifted from 0 in the y direction ; in all patients we found a shift < 3 mthis systematic error is probably due to reconstruction of the drr based on ct slices of 5 - mmthick sections . 
in fact , decreasing slice thickness ( 3 mm ) will improve the quality of the drr and should eliminate this systematic error . moreover , we investigated the possible relationship between bmi and weight changes with setup shifts detected by alignrt . 
due to the limited numbers of patients , we saw no correlation : in particular , overweight and obese patients showed no significant differences , although alignrt is a body surface imaging systein a larger series of 329 prostate cancer patients , wong and colleagues found a significantly larger shift in the lateral direction for obese patients [ 16 ]  . furthermore , for correct patient setup , rotation and reslimmagine acquisita dallalignrt il primo giorno del trattamento radioterapico . in questo studio abbiamo analizzato gli errori di setup quotidiano rilevati dallalignrt lungo le tre direzioni durante ogni seduta di rt , usando limmagine della tc di pianificazione come immagine di riferimento . 
 [ 14 ] , per una soglia > 5 mm gli spostamenti maggiori sono stati osservati lungo gli assi y e z ( rispettivamente nel 47 , 4% e 42 , 1% dei casi )  . 
anche prendendo in considerazione la soglia di 3 mm , gli spostamenti maggiori sono stati osservati lungo gli assi y e z ( 68% e 69% , rispettivamente )  . 
lungo lasse x gli errori al di sopra di questa soglia sono stati osservati nel 10% dei casi . confrontando gli spostamenti rilevati dallalignrt e dal dpi , stata osservata una significativa differenza nella rilevazione degli spostamenti lungo le direzioni longitudinale e verticale , dove il sistema ottico mostra una sovrastima degli spostamenti stessi . 
pertanto , i dati sono stati analizzati in funzione di determinate soglie di spostamento di 3 , 4 e 5 m prendendo in considerazione la soglia 5 mm , i due sistemi hanno fornito spostamenti corrispondenti lungo la direzione longitudinale e verticale , mentre lungo la direzione laterale la soglia non risultata necessaria . 
abbiamo ipotizzato che il sistema alignrt lungo la direzione laterale pi affidabile in quanto in grado di acquisire unimmagine di superficie pi ampia . considerando il confronto dpi - drrs , gli spostamenti sono significativamente deviati rispetto allo 0 solo nella direzione y ; in tutti i pazienti stato osservato uno spostamento inferiore a 3 mquesto errore sistematico probabilmente dovuto alla ricostruzione delle drrs che si basa sulla scansioni assiali tc ( 5 mm )  . 
poich la qualit delle drrs strettamente correlata allo spessore delle scansioni tc , una riduzione dello spessore da 5 mm a 3 mm potrebbe eliminare questo errore sistematico rilevato unicamente nella direzione longitudinale . inoltre , stata analizzata una possibile correlazione tra il bmi e i cambiamenti di peso con gli spostamenti di setup rilevati dallalignrt . 
in questo studio , probabilmente a causa del numero limitato di pazienti , non stata osservata nessuna correlazione : in particolare i pazienti sovrappeso ed obesi non hanno mostrato differenze significative , sebbene lalignrt sia un sistema di registrazione di immagini di superficie corporea . 
 [ 16 ] hanno trovato spostamenti maggiori nella direzione laterale nei pazienti obesi . inoltre , per un corretto set - up del paziente dovrebbe ro essere anche considerati la rotazione il movimento respiratorio . 
in our opinion , the alignrt system could be used daily in prostate cancer 3d - crt to define setup alignment , whereas portal images could be limited only to the first radiotherapy session and in case of exceeding the tolerance threshold ( > 5 mm )  . 
 i risultati di questo studio dimostrano che gli spostamenti di set - up ottenuti mediante il sistema alignrt sono in accordo con quelli rilevati tramite dpi , in particolare lungo la direzione laterale . 
quin di secondo noi , il sistema alignrt potrebbe essere utilizza to quotidianamente nella 3d - crt del carcinoma prostatico , limitando alla sola prima seduta o in caso di superamento della prestabilita soglia di tolleranza ( > 5 mm ) , le acquisizione delle immagini portali di verifica . 
bazzocchi5 , 6 1department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 2department of radiology , scientific institute casa sollievo della sofferenza hospital , viale cappuccini 1 , 71013 san giovanni rotondo ( fg ) , italy 3university of crete , faculty of medicine , department of medical physics , p.o. 
box 1352 , 71110 heraklion , crete , greece 5imaging division , clinical department of radiological and histocytopathological sciences , university of bologna , santorsola , malpighi hospital , via g . 
pinto 1 , 71100 foggia , italy , tel . : + 390881 - 733866 , fax : + 39 - 0881 - 350368 , e - mail : g.guglielmi@unifg.it received : 12 july 2012 / accepted : 24 july 2012 / published online : 22 october 2012 springer - verlag 2012 abstract recent advances in the densitometric and imaging techniques involved in the management of osteoporosis are associated with increasing accuracy and precision as well as with higher exposure to ionising radiation . 
the development of effective and efficient qa programmes is mandatory to guarantee optimal image quality while reducing radiation exposure levels to the alara principle ( as low as reasonably achievable )  . 
lo sviluppo di programmi di qa efficaci ed efficienti necessario al fine di garantire una qualit dellimmagine ottimale e al contempo di ridurre i livelli di esposizione alle radiazioni secondo il principio alara ( cio al livello pi basso ragionevolmente ottenibile )  . 
this disease is widely recognised as an important public health problem because of the significant morbidity , mortality and economic and social costs 1348 radiol med ( 2012 ) 117 : 13471354 associated with its complications , i.e. , fractures at different skeletal sites [ 2 ]  . 
fractures tend to occur in those bone parts , such as the vertebral body , hip and wrist , which rely heavily on trabecular bone for their strength [ 3 , 4 ]  . 
it is estimated that every year 9 million osteoporotic fractures affect the worldwide population , and more than half of these occur in europe and in the americas [ 5 , 6 ]  . 
 osteoporotic fractures cost 36 billion euro in europe and 18 billion dollars in the us every year , and these are expected to increase twofold or more by 2050 unless treatments are pursued that have a significant impact on the global burden of fractures [ 7 , 8 ]  . quality assurance ( qa ) is by definition a programme for the systematic monitoring and evaluation of the various aspects of a service or facility to ensure that standards of quality are being met . 
qa in bone densitometry and associated methods is composed of those actions aiming to ( 1 ) maintain adequate equipment performance with the lowest possible radiation dose to patients consistent with clinical imaging requirements and ( 2 ) assure that adequate diagnostic information is provided at the lowest possible cost . 
dual - energy x - ray absorptiometry ( dxa ) is currently the most widely used method for the measurement of areal bone mineral density ( bmda ) ( g / cm2 )  . 
peripheral qct ( pqct ) , and high - resolution pqct ( hr pqct ) are ct - based techniques dedicated to the study of appendicular sites of the skeleton , with the aim of analysing both density and microarchitectural bone properties . 
vertebral fractures are usually diagnosed on spine radiographs or images of the spine acquired by dxa devices . the use of diagnostic imaging methods for the assessment of bone status has constantly and quickly increased , so that qa in bone densitometry deserves special attention [ 9 ]  . 
the purpose of this review article is to summarise the current practice of qa in bone densitometry and related techniques and to discuss the magnitude of radiation exposure from the x - ray methods used for the assessment of bone status . equipment and installation the technical features of bone densitometry and other related medical devices should satisfy clinical requirements . 
equipment packages should include not only the specific application software package but also dedicated phantoms for calibration and quality control procedures . the installation of the equipment should be followed by procedures that ensure proper functioning , satisfy all current radiation protection requirements and manufacturer specifications . 
electrical safety tests , equipment tests and staff training should be provided by the supplier of the equipment ; the employer should verify if equipment tests and staff training have been performed on the newly installed equipment [ 9 ]  . quality control an important issue in the study of bone status is the establishment of sufficient qc procedures , performed to ensure that a manufactured product meets a defined and standardised set of quality criteria . 
these procedures include monitoring of the stability and performance of the devices as well as guidelines for the handling of error sources in order to guarantee reliable quantitative information to clinicians and patients as an aid to diagnosis and management of osteo porosis . dual - energy x - ray absorptiometry dxa has a relevant and central role in the evaluation of individuals at risk of osteoporosis , in helping clinicians to assess fracture risk and in patients with osteoporosis to select pharmacological therapy and to monitor treatment or disease progression [ 10 ]  . 
this is influenced by several parameters , such as skill and training of the technician performing the scan , the site of measurement and the clinical features of patients [ 9 ]  . radiol med ( 2012 ) 117 : 13471354 1349 to determine the accuracy of a dxa densitometer , a phantom containing tissue - mimicking materials of known and different densities is scanned to ensure that measured values are truly assessed for all quantities under investigation [ 11 ]  . 
 thus , every facility should determine in vivo reproducibility for each dxa device [ 13 , 14 ]  . it is well known that dxa devices developed by different manufacturers and even by the same manufacturer provide different bmd results when used to measure the same skeletal site of a patient because of differences in scanner design , data acquisition , algorithms and method of calibration . 
although sbmd values can reduce the differences between measurements performed by systems developed by different manufacturers to less than 6% , the use of different dxa systems to longitudinally monitor the bone status of an individual is not recommended . quantitative ct precision is better for 3d multidetector qct than for singleslice 2d qct [ 17 ]  . qct is based on analysis of the trabecular bone compartment in the spine or proximal femur . 
most calibration approaches consist of a calcium hydroxyapatite - based bone mineral reference phantom that is scanned with the patient and placed underneath the lumbar spine or between the hips . 
the image analysis ( columbia , ky , usa ) standard consists of rods with varying concentrations of calcium hydroxyapatite mixed in a water - equivalent solid resin matrix [ 18 ]  . 
another approach , phantomless calibration , uses histograms of hu values placed in regions of subcutaneous fat and skeletal muscle , assuming fixed properties for each tissue types to determine a hu calibration [ 17 ]  . 
qus measurements are affected by precision errors due to patient positioning , coupling between the transducer and the skin of the patients , and the effect of soft tissue properties . 
a phantom should emulate the in vivo measurement as much as possible in terms of geometry and acoustic properties . the differences in measurements between available qus equipment are greater than those between dxa devices ; this is due to the different transducers and frequency ranges [ 21 ]  . the qa of ct systems is recognised as an important topic and scientific and professional organisations have developed guidelines for equipment specifications , equipment qc tests and radiation safety [ 17 ]  . 
radiation safety in ct is emphasised because patient radiation doses from ct are considerably higher than those from dxa . the measurement of precision is influenced by the ct scanner model , qct method , skill of the radiological technologist , patient positioning and movement . 
 radiation dosimetry a bone densitometry qa programme should involve periodic checks and measurements to maintain diagnostic image quality at the lowest possible radiation exposure . quantities and units the two most frequently used radiation quantities in diagnostic radiology are absorbed dose ( ad ) and effective dose ( ed )  . 
the ad , expressed in grays ( gy ) , is a measure of the energy per unit of mass deposited in the tissue and organs of the exposed body . 
the ed , expressed in sieverts 1350 radiol med ( 2012 ) 117 : 13471354 ( sv ) , is calculated using organ or tissue absorbed doses and the relative radiosensitivity assigned to each of these organs or tissues , defined by the international commission on radiological protection ( icrp ) [ 22 ]  . 
 the ed was introduced to allow comparison of the risk estimates from different sources of ionising radiation , for example from dxa and qct , or from imaging techniques and natural background radiation . 
the annual worldwide average ed from natural background radiation is 2.4 msv [ 9 ]  . dosimetric quantities used in ct are the ct dose index ( ctdi ) and the dose - length product ( dlp ) [ 9 ]  . 
ctdi measurements are performed at the periphery and at the centre of cylindrical phantoms representing the human head and body by using a pencil ionisation chamber with a length of 100 mfrom these measurements , a weighted ctdi ( ctdiw ) representing the average dose to a single slice is obtained . 
moreover , ctdi volume ( ctdiv ) has been introduced to take into account the effect of pitch on radiation dose , for imaging performed in the spiral mode , which is defined as ctdiw divided by pitch . 
 broad estimates of effective dose e can be derived from dlp values using conversion coefficients : e = dlpk where k is body regionspecific normalised ed factors ( msv * mgy1 * cm1 ) [ 23 ]  . patient exposure children and adult doses from dxa have been reported in several studies [ 24 - 28 ]  . 
the increased field size of fan - beam scanners ( linear - array detector ) and more recently of cone beam densitometers ( bi - dimensional detector ) , compared to pencil beam devices , has resulted in shorter scan times allowing greater patient compliance and better image quality . 
however , patient doses associated with state - of - the - art dxa scanners have also been increased [ 29 ]  . patient doses from pencil - beam dxa is 1 sv or less . 
patient doses up to 15 sv and 10 sv for spine and hip scans , respectively , have been reported for fan - beam dxa examinations performed on adult patients [ 26 ]  . 
specifically , paediatric patients will receive about two to three times higher ed than adults due to ( a ) the larger field size and ( b ) higher dose to internal organs because of less attenuation of x - rays by overlying tissue [ 26 ]  . 
when a patient is found to be pregnant after having undergone a dxa examination , communication with the woman is very important to give her an assessment of conceptus dose . 
published research shows that conceptus doses and potential radiogenic risks from dxa are negligible and , therefore , abortion due to radiation exposure is not recommended [ 22 , 32 ]  . 
an examination acquired at 80 kvp tube potential and 125 mas tube load delivers a radiation dose to a patient from 60 to approximately 300 sv , depending on protocol parameters and ct scanner model [ 25 , 33 ]  . 
on the other hand , qct of the appendicular skeleton , is associated with low patient ed ( lower than 10 sv ) [ 34 ]  . the analysis of mdct high resolution ( hr ) images provides important information about the trabecular bone network [ 36 , 37 ]  . 
however , patient doses associated with hrct ( with isotropic spatial resolution , submillimetre range ) are high , reaching about 3 msv [ 38 ]  . several factors play a role in the reduction of radiation dose to the patient . 
the use of adaptive section collimation , available in new - generation mdct scanners , allows reduction of exposure due to z - over scanning associated with helical scanning [ 39 ]  . 
nevertheless , studies are still needed to maximise the diagnostic information provided by the new technologies with the lowest radiation dose to the 1352 radiol med ( 2012 ) 117 : 13471354 patient . 
however , more accurate calculation of patient ed is possible using patient - specific monte carlo software packages for ct dosimetry [ 42 ]  . peripheral qct ( pqct ) scanners are dedicated units capable of assessing bone architecture and bmd at appendicular bones . 
the ed from pqct examinations is on the order of few sv [ 34 , 43 ]  . occupational radiation doses and shielding the scan type and mode , the workload and the relative position of the workstation to the scanning table are factors influencing exposure to the operator . 
the ministry of health service in british columbia has found that the exposure per 1000 scans to the bone densitometry operator was 56.0 mr for hologic qdr4500w , 7.0 mr for norland eclipse xe and 21.0 mr for ge prodigy lunar [ 44 ]  . 
the need for shielding mainly depends on patient workload , the size of the examination room , and the type of dxa scanner ( especially for fan - beam technology )  . 
when planning a bone densitometry facility , however , several parameters should be taken into account so that the exposure in adjoining areas is at a level acceptable for members of the public . 
moreover all resulting test results should be recorded and periodically reviewed to detect needed changes [ 9 ]  . education and staff training the performance of a bone densitometry facility is greatly influenced by the education and training of the staff delivering the services . 
they should also be acquainted with the application of all radiological techniques employed for the diagnosis of osteoporosis and familiar with the bone densitometry diagnostic activity [ 45 ]  . 
ospedali galliera , mura delle cappuccine 14 , 16128 genova , italy 2clinica reumatologica , dipartimento di medicina interna ( dimi ) , universit di genova , viale benedetto xv 6 , 16132 genoa , italy correspondence to : f . 
two types of iog have been described : an idiopathic form ( or type i ) , the pathogenesis of which has not been completely clarified , and a penetrating form ( or type ii ) , caused by the intrusion of juxtacortical material ( often a ganglion cyst of the dorsal soft tissue ) into the cancellous bone compartment . 
the differential diagnosis for iog is wide - ranging and complex , including lesions of posttraumatic ( posttraumatic cystlike defects ) , degenerative ( subchondral degenerative cysts ) , inflammatory [ cystic rheumatoid arthritis , chronic tophaceous gout ( ctg ) ] , neoplastic ( benign primary bone tumours and synovial proliferative lesions ) , ischaemic ( kienbcks disease or avascular osteonecrosis of the lunate ) and metabolic ( amyloidosis ) origmultimodality imaging of iogs is a useful diagnostic tool that provides complete morphological characterisation and differentiation from other intraosseous cystic abnormalities of the carpus . 
thin - slice multidetector computed tomography ( mdct ) can provide high - spatial - resolution images of the cortical and cancellous bone compartments , allowing detection of morphological findings helpful in characterising bone lesions , whereas magnetic resonance ( mr ) imaging can simultaneously visualise bone , articular surfaces , hyaline cartilage , fibrocartilage , capsules and ligaments , along with intraand periarticular soft tissues . riassunto il ganglio intraosseo ( iog ) la lesione ossea del carpo di pi frequente riscontro e spesso rappresenta un reperto occasionale in esami radiografici eseguiti per altri motivi . 
la diagnosi differenziale dei iog ampia ed articolata , includendo lesioni di origine post - traumatica ( difetti simil - cistici post - traumatici , ptcd ) , degenerativa ( cisti subcondrali degenerative , sdc ) , infiammatoria ( artrite reumatoide cistica e gotta cronica tofacea ) , neoplastica ( tumori ossei primitivi e lesioni proliferative sinoviali benigne ) , ischemica ( morbo di kienbock od osteonecrosi avascolare del semilunare ) e metabolica ( amiloidosi )  . 
la tomografia computerizzata multi - detettore ( mdct ) consente di ottenere immagini ad elevata risoluzione spaziale dei compartimenti ossei corticale e spongioso , permettendo di rilevare elementi morfologici utili ad una precisa caratterizzazione delle lesioni ossee , mentre la risonanza magnetica ( rm ) offre il vantaggio di visualizzare simultaneamente la componente ossea , le superfici articolari , gli spessori condrali , le strutture 1356 radiol med ( 2012 ) 117 : 13551373 keywords intraosseous ganglion bone cyst bone tumours of the wrist bone erosion fibrocartilaginee , capsulo - legamentose ed i tessuti molli intrae peri - articolari . parole chiave ganglio intraosseo cisti ossea tumori ossei del polso erosione ossea introduction introduzione intraosseous ganglion ( iog ) is the most frequently occurring benign osteolytic lesion of the cancellous compartment of the carpal bones and is often an incidental finding on radiographs obtained for other purposes [ 1 ]  . 
despite the high frequency of these lesions , the pathogenesis has not been completely elucidated , and the terminology used to describe them is highly heterogeneous ( intraosseous ganglion cyst , intraosseous cyst , juxtaarticular bone cyst , subchondral bone cyst , subchondral synovial cyst [ 35 ] ) , resulting in a risk of misinterpretation and misclassification . 
 [ 6 ] suggested dividing iogs into two types : one primary intraosseous ( type i , or idiopathic ) and the other resulting from penetration into bone of juxtacortical material , in most cases a carpal soft - tissue ganglion ( type ii , or penetrating )  . 
 [ 7 ] proposed a detailed histopathological description of anatomical specimens , along with radiographic and magnetic resonance ( mr ) imaging correlation . evidence of a topographical correspondence between type i iogs and the insertion of intrinsic ( scapholunate and lunotriquetral ) and extrinsic ligaments ( capsular ) of the carpus suggests a causal role for entheseal abnormalities in the pathogenesis of cystic lesions within the cancellous bone . 
according to this recent theory [ 7 ] , the chronic biomechanical stress at the insertion of the ligaments to the carpal bones causes enthesis degeneration followed by cortical damage and intrusion of synovial fluid into the cancellous bone . the recent radiological literature contains no comprehensive description of multimodality imaging and differential diagnosis of carpal iogs . 
as for type ii iogs , the only published report [ 8 ] is not supported by complete radiological images . il ganglio intraosseo ( iog ) la pi frequente alterazione osteolitica benigna del compartimento spongioso delle ossa del carpo , costituendo spesso un reperto occasionale in esami radiografici eseguiti per altri motivi [ 1 ]  . 
 dal punto di vista anatomo - patologico i iog dimostrano molte analogie con i gangli dei tessuti molli del carpo , presentando una parete costituita da tessuto fibroso , sprovvista di rivestimento sinoviale , ed un contenuto gelatinoso e denso . 
nonostante lelevata frequenza di riscontro , la patogenesi di queste alterazioni ossee carpali non stata ancora completamente chiarita e la terminologia utilizzata per descriverle risulta molto eterogenea ( cisti ganglionare intraossea , cisti intraossea , cisti ossea juxta - articolare , cisti ossea subcondrale , cisti sinoviale subcondrale [ 35 ] ) con il rischio di generare problemi interpretativi e di classificazione . 
 [ 6 ] hanno suggerito la distinzione del iog in due forme , quella primitivamente intraossea ( tipo i o idiopatica ) e quella conseguente alla penetrazione intraossea di materiale juxta - corticale ( tipo ii o penetrante ) , nella maggior parte dei casi rappresentato da un ganglio dei tessuti molli del carpo . 
 [ 7 ] hanno proposto una dettagliata descrizione istopatologica di preparati anatomici , completata da correlazione con radiografia e risonanza magnetica ( rm )  . levidenza di una corrispondenza topografica tra iog di tipo i ( idiopatici ) e linserzione dei legamenti intrinseci ( scafo - lunato e luno - piramidale ) ed estrinseci ( capsulari ) del carpo suggerisce un ruolo causale delle alterazioni entesiche nella patogenesi delle lesioni cistiche intraspongiose . 
secondo questa recente [ 7 ] teoria patogenetica lo stress biomeccanico cronico in corrispondenza delle inserzioni legamentose sulle ossa del carpo provocherebbe inizialmente la degenerazione entesica , seguita dal danneggiamento della corticale e dallintrusione di liquido sinoviale nel compartimento spongioso . nella letteratura radiologica recente non reperibile una trattazione organica riguardante limaging integrato dei iog carpali e la loro diagnosi differenziale . 
per quanto riguarda i iog penetranti ( di tipo ii ) , in particolare , il solo report disponibile [ 8 ] non corredato da uniconografia radiologica completa . radiol med ( 2012 ) 117 : 13551373 1357 the differential diagnosis of iogs should consider other intraosseous cystic lesions of the carpus and include lesions of posttraumatic ( posttraumatic cyst - like defects ) , degenerative ( subchondral degenerative cysts ) , neoplastic ( primary bone lesions and benign tumours of the synovium ) , inflammatory ( cystic rheumatoid arthritis and ctg ) , ischaemic ( kienbcks disease or avascular necrosis of the lunate ) and metabolic ( amyloidosis ) origmany mechanisms may lead to the development of osteolytic lesions in the cancellous bone of the carpus . 
often , correct diagnosis is impossible on the basis of radiography alone , and further investigations such as multidetector computed tomography ( mdct ) and mr imaging are needed , with biopsy being reserved for selected cases . thin - slice mdct produces images with a high spatial resolution of mineralised tissues ( cortical and cancellous bone compartments ) , outlining important features of the osseous lesions ( cortical penetration sites , interruption of the trabecular pattern , calcified septations , matrix calcifications )  . 
at microscopy , the iog wall does not present any synovial lining and is composed of fibrous tissue and collagen fibres with aspects of myxoid degeneration ; the cyst contains dense and gelatinous material . 
iogs usually occupy an eccentric position at the periphery of the cancellous compartment and close to the la diagnosi differenziale dei iog si pone con le altre alterazioni cistiche intraspongiose del carpo , ed include lesioni di origine post - traumatica ( difetti simil - cistici posttraumatici , ptcd ) , degenerativa ( cisti subcondrali degenerative , sdc ) , neoplastica ( lesioni ossee primitive e lesioni proliferative sinoviali benigne ) , infiammatoria ( artrite reumatoide cistica e gotta cronica tofacea ) , ischemica ( morbo di kienbock od osteonecrosi avascolare del semilunare ) e metabolica ( amiloidosi )  . 
i meccanismi di danno che possono condurre allo sviluppo di lesioni osteolitiche intraspongiose nel carpo sono molteplici ed spesso impossibile formulare una corretta diagnosi sulla scorta del solo esame radiografico , senza limpiego di ulteriori indagini radiologiche [ tomografia computerizzata multi - detettore ( mdct ) e rm ] , riservando lesame bioptico a casi selezionati . la mdct con tecnica a strato sottile consente di ottenere immagini ad elevata risoluzione spaziale dei tessuti mineralizzati ( compartimenti ossei corticale e spongioso ) , delineando importanti aspetti delle lesioni ossee ( punti di penetrazione corticale , interruzione del disegno trabecolare , sepimentazioni calcifiche interne , calcificazioni della matrice )  . 
la rm offre il vantaggio di visualizzare simultaneamente la componente ossea , le superfici articolari , gli spessori condrali , le strutture fibrocartilaginee , capsulo - legamentose ed i tessuti molli intrae peri - articolari ; essa rappresenta inoltre la sola metodica radiologica in grado di dimostrare ledema osseo midollare intraspongioso , che costituisce un utile indicatore della stabilit dimensionale o della tendenza evolutiva delle lesioni ossee . lo scopo del presente lavoro quello di descrivere laspetto dei iog nelle diverse metodiche di imaging , fornendo gli elementi per la loro caratterizzazione ed una guida immediata per orientarsi nella diagnosi differenziale tra le molteplici lesioni osteolitiche del carpo . imaging integrato del ganglio intraosseo il iog la lesione ossea pi comune del carpo [ 1 ] , ma , nonostante lelevata frequenza di riscontro , la patogenesi dei iog idiopatici ( o di tipo i ) non stata ancora chiarita in modo univoco . 
allesame microscopico la parete del iog non presenta un rivestimento sinoviale ed costituita da tessuto fibroso e fibre collagene con aspetti di degenerazione mixoide ; il contenuto cistico risulta costituito da materiale denso e gelatinoso . 
 le ossa carpali pi frequentemente colpite sono , in ordine di frequenza , il semilunare , il capitato e lo scafoide [ 1 , 7 , 9 ] ; raramente vi pu essere un interessamento multiplo o bilaterale [ 10 , 11 ]  . 
le due scansioni tc assiali contigue ( b , c ) dimostrano i margini osteosclerotici della lesione ed il sottile peduncolo trans - corticale sul versante volare dellosso ( freccia vuota in c ) , il quale risulta ben visualizzato anche nella ricostruzione tc con tecnica surface rendering ( d ) ( freccia bianca spessa )  . cortical bone [ 7 ] , away from subchondral bone and articular surfaces [ 1 , 2 ]  . 
 [ 7 ] , these lesions are mainly located on the palmar aspect of the carpal bones at the insertion of the intrinsic ( scapholunate , lunotriquetral ) or extrinsic ( capsular ) carpal ligaments . 
histological sections have revealed degenerative changes at the insertion of ligaments adjacent to the iogs , suggesting a link between biomechanical factors acting on ligament insertions and the development of these intraosseous lesions [ 7 ]  . 
 according to the first theory , an unknown stimulus causes intramedullary mesenchymal precursor cells to differentiate into fibrohistiocytic cells , with associated accumulation of hyaluronic acid in the extracellular matrix and initial formation of cyst - like chambers in the cancellous bone [ 1222 ]  . 
the necrotic material is then reabsorbed and the iog develops [ 13 , 20 , 21 ]  . on conventional radiography , iogs appear as radiolucent intraosseous lesions , with well - defined margins , circondrale e dalle superfici articolari [ 1 , 2 ]  . 
 [ 7 ] , queste alterazioni sono localizzate in prevalenza sul versante palmare delle ossa del carpo , in rapporto allinserzione dei legamenti intrinseci ( scafo - lunato , luno - piramidale ) o estrinseci ( capsulari ) del carpo . 
le sezioni istologiche dei preparati anatomici hanno rivelato alterazioni degenerative inserzionali dei legamenti contigui ai iog , suggerendo quindi lesistenza di un legame tra i fattori biomeccanici che agiscono sui punti entesici e lo sviluppo di queste lesioni intraspongiose [ 7 ]  . 
 secondo la prima teoria uno stimolo sconosciuto provocherebbe la differenziazione di precursori mesenchimali intramidollari in cellule fibroistiocitarie , con associato conseguente accumulo di acido ialuronico nella matrice extracellulare e iniziale formazione di concamerazioni pseudocistiche nella spongiosa ossea [ 1222 ]  . 
lipotesi del danno microvascolare suggerisce la combinazione di una pressione intra - articolare persistentemente elevata e di microtraumatismi ripetuti come fenomeno alla base della formazione di un focolaio di osteonecrosi . 
il materiale necrotico verrebbe quindi riassorbito , lasciando come esito il iog [ 13 , 20 , 21 ]  . il iog appare in radiografia tradizionale come unalterazione intraspongiosa radiotrasparente , a margini ben deradiol med ( 2012 ) 117 : 13551373 1359 fig . 
in the t2 - weighted fast spin - echo ( fse ) ( c ) and short tau inversion recovery ( stir ) ( d ) axial images , the content of the cyst appears hyperintense . 
nelle sequenze fast spin echo ( fse ) t2 - pesata ( c ) e short inversion - time inversion recovery ( stir ) ( d ) sul piano assiale il contenuto della cisti appare iperintenso . 
sagittal t2 - weighted fse ( b ) and coronal stir ( c ) images show a ganglion cyst in the dorsal soft tissues ( g ) that penetrates into the base of the third metacarpal bone through a discontinuity of the bone cortex ( arrows in b )  . 
dorsovolar radiograph ( a ) shows a scaphoid nonunion advanced collapse ( snac ) wrist caused by an untreated fracture of the proximal pole of the carpal scaphoid ( black arrow )  . 
sagittal t2 - weighted fse image ( b ) reveals a hyperintense ganglion cyst in the carpal dorsal soft tissues ( g ) , which penetrates into the spongiosa through a discontinuity in the bone cortex ( arrowhead )  . 
il radiogramma in proiezione dorsovolare ( a ) dimostra un quadro di scaphoid non - union advanced collapse ( snac ) , per frattura non trattata del polo prossimale dello scafoide carpale ( freccia nera )  . 
lesame radiografico in proiezione dorso - volare ( a ) dimostra una linea di frattura ( punta di freccia ) in corrispondenza del corpo dello scafoide , insorta su una voluminosa formazione osteolitica . 
la ricostruzione tc sul piano coronale ( b ) dimostra con elevato dettaglio anatomico la rima di frattura ( freccia ) ed il sottostante iog . defects ( ptcd ) , which are the late sign of an occult , untreated fracture and are considered useful indicators of delayed bone consolidation [ 26 , 27 ]  . 
i micromovimenti e gli stress biomeccanici ripetuti in corrispondenza della rima della frattura occulta possono provocare linsorgenza di una condizione di ischemia , associata a conseguente proliferazione di fibroblasti e produzione di tessuto cartilagineo , che 1362 radiol med ( 2012 ) 117 : 13551373 fig . 
le due ricostruzioni tc sagittali contigue ( a , b ) dimostrano una linea di frattura a carico del polo prossimale dello scafoide con evoluzione in pseudoartrosi ( frecce bianche ) ed alcune alterazioni cistiche intraspongiose ( punte di freccia ) in rapporto alla rima di frattura . with fibroblast proliferation and production of cartilage tissue , which on conventional radiography appears as focal cyst - like radiolucencies . 
histopathological examination of surgical specimens has revealed that these focal radiolucencies are not real fluid - containing cysts but islands of ectopic cartilage [ 27 ]  . subchondral degenerative cysts iogs should not be confused with subchondral degenerative cysts ( sdc ) , also known as geodes , which characterise carpal osteoarthritis and are considered the consequence of a high - grade chondropathy [ 7 , 9 ]  . 
subcortical intrusion of synovial fluid through small , uncontained fissures within the hyaline cartilage leads to the formation of subchondral chambers in the cancellous bone ( sdc ) that connect with the articular surface through a thin transcortical pedicle [ 9 ]  . 
histological analysis of the walls of sdcs reveals a nonspecific , flat or synovial epithelial lining , whereas the walls of iogs are covered with fibromyxoid tissue containing proteoglycans and mucopolysaccharide chains [ 7 ]  . mdct scans can depict the thin transcortical pedicle connecting the sdc with the adjacent synovial space , si presenta in radiografia tradizionale sotto forma di focali aree di radiotrasparenza con aspetto cistico . 
una condizione predisponente allo sviluppo delle sdc sembra essere la presenza di una elevata pressione di contatto focale tra le superfici articolari , come si verifica nel contesto della patologia degenerativa articolare . 
lintrusione sottocorticale di liquido sinoviale , attraverso piccole fissurazioni non contenute della cartilagine ialina articolare , conduce al progressivo sviluppo di concamerazioni intraspongiose subcondrali ( sdc ) , comunicanti con la superficie articolare mediante un sottile peduncolo trans - corticale [ 9 ]  . 
lanalisi istologica della parete delle sdc dimostra la presenza di un rivestimento epiteliale di tipo piatto aspecifico o di tipo sinoviale , mentre la parete dei iog ricoperta da tessuto fibromixoide contenente proteoglicani e catene mucopolisaccaridiche [ 7 ]  . le scansioni mdct possono dimostrare il sottile peduncolo trans - corticale che collega la sdc allo spazio sinoviale adiacente , situato classicamente in corrispondenza della superficie articolare , la quale risulta caratterizzata da una degradazione della cartilagine ialina di rivestimento . 
coronal ( a ) and sagittal ( b ) ct reconstructions with bone window indicate a scaphoid nonunion ( arrow ) with dorsal tilt of the lunate and early proximal migration of the capitate . 
two sequential axial ct images ( c , d ) reveal the presence of sdcs ( arrowheads ) in the distal epiphysis of the radius and ulna and in the trapezoid and hamate bones . 
le ricostruzioni tc sui piani coronale ( a ) e sagittale ( b ) con finestra per losso dimostrano una pseudoartrosi dello scafoide ( freccia ) con sublussazione dorsale del semilunare e iniziale migrazione prossimale del capitato . 
la due scansioni tc assiali contigue ( c , d ) dimostrano la presenza di alcune sdc ( punte di freccia ) in corrispondenza dellepifisi distale di radio e ulna , del trapezoide e delluncinato , caratterizzate da margini spongiosclerotici ben definiti ed in comunicazione con la superficie articolare . typically located in correspondence with the articular surface , which is characterised by degradation of the hyaline cartilage covering . 
 benign bone tumours aneurysmal bone cyst ( abc ) , osteoid osteoma ( oo ) and enchondroma are bone tumours that may appear lytic with regular margins , mimicking an iog on radiography [ 1 , 30 ]  . 
abcs account for around 12% of all bone tumours and usually develop in the metaphysis of long bones and in the posterior elements of vertebral bodies [ 30 ]  . 
according to one theory , primary abcs develop from existing intraosseous arteriovenous malformations that , through erosion of the trabecular meshwork , lead to the formation of a blood - filled cystic cavity [ 32 ]  . 
 tumori ossei benigni la cisti ossea aneurismatica ( aneurysmal bone cyst , abc ) , losteoma osteoide ( oo ) e lencondroma sono neoformazioni ossee che possono assumere sui radiogrammi un aspetto puramente litico con margini regolari , simulando la presenza di un iog [ 1 , 30 ]  . 
la abc rappresenta circa l1%2% di tutti i tumori ossei e solitamente si sviluppa nella metafisi delle ossa lunghe e negli elementi posteriori dei corpi vertebrali [ 30 ]  . 
secondo una teoria patogenetica la abc primitiva si sviluppa da una preesistente malformazione arterovenosa intraossea , che , mediante un processo di erosione della tela trabecolare spongiosa , pu condurre alla formazione di una cavit cistica ripiena di sangue [ 32 ]  . 
una abc si pu anche formare secondariamente ad altri tumori , in particolare in seguito allo sviluppo di alterazioni cistiche emorragiche nel tumore a cellule giganti [ 33 ]  . 
lindagine mdct dimostra la presenza di una lesione cistica intraossea con distruzione della struttura trabecolare , tipicamente associata ad assottigliamento della corticale ossea contigua , che non presenta tuttavia grossolane soluzioni di continuit . 
 1364 radiol med ( 2012 ) 117 : 13551373 sion with destruction of the trabecular structure , typically associated with thinning of the adjacent cortical bone , which does not , however , show evident interruptions . 
histopathology of surgical specimens may reveal blood - filled cystic cavities separated by fibrous septa in which fibroblasts , multinucleate osteoclasts and neoplastic bone tissue surrounded by osteoblasts may be identified [ 32 ]  . 
 oo and enchondroma are two benign tumours that may rarely arise in carpal bones , where they typically have a lytic appearance , mimicking iog on radiography [ 1 ]  . 
the internal architecture of oo and enchondromas is readily evaluated on mdct [ 1 , 34 , 35 ] , which may demonstrate the distinctive characteristics of these lesions , such as the oo nidus and the chondroid calcifications of the enchondroma matrix . 
 giant - cell tumour ( gct ) , or osteoclastoma , most often affects young adults after they have reached skeletal maturity [ 36 ] and consists histologically of multinucleated giant cells immersed in a homogeneous matrix of stromal cells [ 1 , 37 ]  . 
 gct of the carpal bones typically appears as a well - defined radiolucent area , without cortical swelling [ 39 ] , and is characterised by a less aggressive biological behaviour than gct of the distal radius . 
the first case of gct of the lunate bone reported in the literature was initially interpreted as kienbcks disease [ 1 ]  . benign tumours of intra - articular soft tissues the differential diagnosis of cystic carpal lesions should also consider benign synovial proliferative lesions . 
pigmented villonodular tenosynovitis , ( pvnts ) , also known as giant - cell tumour of tendon sheaths , is the second most frequent lesion of the carpal soft tissues after dorsal ganglion cysts [ 4042 ]  . 
loo e lencondroma sono due neoplasie benigne che possono raramente originare nelle ossa del carpo , dove tipicamente assumono un aspetto litico , simulando allesame radiografico la presenza di un iog [ 1 ]  . 
larchitettura interna delloo e dellencondroma agevolmente valutabile allindagine mdct [ 1 , 34 , 35 ] , che pu dimostrare le caratteristiche distintive di queste lesioni , come il nidus delloo e le calcificazioni condroidi della matrice dellencondroma . il tumore a cellule giganti ( giant cell tumor , gct ) , od osteoclastoma , colpisce con maggiore frequenza giovani adulti dopo il raggiungimento della maturit scheletrica [ 36 ] , e dal punto di vista istologico risulta costituito da cellule giganti multinucleate immerse in una matrice omogenea di cellule stromali [ 1 , 37 ]  . 
il radio distale rappresenta la terza sede pi comune di sviluppo del gct che , a tale livello , si presenta allesame radiografico come unarea radiotrasparente a margini ben definiti . 
il gct che insorge nelle ossa del carpo si manifesta tipicamente come unarea di radiotrasparenza ben definita , senza rigonfiamento della corticale [ 39 ] , ed caratterizzato da un comportamento biologico meno aggressivo rispetto al gct che si sviluppa nel iii distale del radio . 
il primo caso documentato in letteratura di gct dellosso semilunare era stato inizialmente interpretato come morbo di kienbock [ 1 ]  . tumori benigni dei tessuti molli intra - articolari nella diagnosi differenziale delle lesioni cistiche del carpo devono essere tenute in considerazione anche le lesioni proliferative sinoviali benigne . 
la tenosinovite villonodulare pigmentosa ( pigmented villo - nodular teno - synovitis , pvnts ) , definita anche tumore a cellule giganti delle guaine tendinee , rappresenta la seconda lesione dei tessuti molli carpali in ordine di frequenza dopo le cisti ganglionari dorsali [ 4042 ]  . 
two pseudocystic formations ( extrinsic erosions ) caused by extrinsic compression and filled with vascular solid tissue ( stars ) can be observed on the distal radial epiphysis and on the volar aspect of the capitate . 
the gadolinium - enhanced t1 - weighted turbo 3d reconstructed axial image ( c ) and the corresponding axial ct image ( d ) show the osteolytic lesion of the distal radial epiphysis , which is characterised by osteosclerotic margins ( arrowheads ) and filled with enhancing solid tissue . 
limmagine post - mezzo di contrasto rm turbo - 3d t1 - pesata ricostruita sul piano assiale ( c ) e la corrispondente scansione assiale tc ( d ) evidenziano lalterazione osteolitica dellepifisi distale del radio , occupata da tessuto attivamente impregnante il mezzo di contrasto e circoscritta da margini spongiosclerotici ( punte di freccia )  . 
il tessuto neoplastico ( t ) disloca ventralmente il tendine flessore radiale del carpo ( fcr ) e si estende distalmente lungo le guaine dei tendini del i compartimento degli estensori . 
periosteal reaction ( 8% of cases ) and intralesional calcifications ( 6% ) may also be seen [ 43 ]  . on mr imaging , pvnts has medium to low signal intensity in all sequences and is characterised by active uptake of i.v. 
 usually , the haemosiderin deposition due to intralesional bleeding is not sufficient to generate the blooming effect , which consists of areas of focal signal loss in t2 * gradientecho sequences . 
unlike pvnts , pvns rarely affects the carpus , where it manifests as a moderately paincalcificazioni nel contesto della lesione ( 6% ) [ 43 ]  . la pvnts mostra allindagine rm una intensit di segnale intermedio - bassa in tutte le sequenze ed caratterizzata da attiva captazione del mezzo di contrasto paramagnetico dopo iniezione endovenosa . 
solitamente nella pvnts la deposizione di emosiderina , per fenomeni intralesionali di sanguinamento , non risulta sufficientemente elevata da generare leffetto blooming , che consiste nella presenza di focali aree di caduta del segnale nelle sequenze gradient - echo t2 *  . 
al contrario della pvnts , la pvns pu raramente interessare il carpo , manifestandosi con una tumefazione articolare monolaterale moderatamente dolen1366 radiol med ( 2012 ) 117 : 13551373 fig . 
axial ct image with bone window ( a ) and detail ( b ) depicts gouty erosions ( arrowheads ) of the lunate ( l ) and scaphoid ( s ) bones , with sharp , osteosclerotic margins . 
in the two corresponding stir ( c ) and t1 - weighted se ( d ) axial images , tophaceous tissue shows medium to high and medium to low signal intensity , respectively . 
scansione tc assiale ( a ) con finestra dellosso e dettaglio ( b ) che dimostra la presenza di erosioni gottose ( punte di freccia ) del semilunare ( l ) e dello scafoide carpale ( s ) , caratterizzate da margini netti e spongiosclerotici . 
allinterno delle lesioni si apprezza tessuto tofaceo iperdenso ( t ) , che presenta unintensit di segnale intermedio - alta nella sequenza rm assiale stir ( c ) ed intermedio - bassa nella sequenza assiale se t1 - pesata ( d )  . 
the literature reports one case of carpal pvns , which was initially diagnosed as iog based on radiography alone [ 43 ]  . te , associata alla presenza di erosioni estrinseche allesame radiografico . 
in letteratura stato descritto un caso di pvns del carpo inizialmente diagnosticato come iog sulla scorta del solo esame radiografico [ 43 ]  . inflammatory arthropathies artropatie infiammatorie some patients with rheumatoid arthritis were found to have extensive subchondral cystic lesions of the cancellous bone with well - defined sclerotic margins , which led to the identification of a rare subtype of the disease ( cystic rheumatoid arthritis ) , which is different from the classic erosive form [ 44 ]  . 
 in this form of rheumatoid arthritis , the main mechanism for subchondral cyst formation is thought to be the subcortical intrusion of synovial fluid through small , erosive chondral lesions [ 44 , 45 ]  . 
this theory has been supported in alcuni pazienti con artrite reumatoide sono state descritte ampie lesioni cistiche intraspongiose subcondrali , a margini sclerotici ben definiti , che hanno permesso di identificare un raro sottotipo della malattia ( artrite reumatoide cistica ) , differente dalla classica forma erosiva [ 44 ]  . 
 si pensa che in questa forma di artrite reumatoide il principale meccanismo di formazione delle cisti subcondrali sia rappresentato dallintrusione sottocorticale di liquido sinoviale attraverso piccole lesioni condrali di natura erosiva [ 44 , 45 ]  . 
a supporto di questa teoria stato dimostrato , mediante limpiego combinato di rm e controlli bioptici , che le lesioni subcondrali contengono liquido sinoviale e , talvolta , radiol med ( 2012 ) 117 : 13551373 1367 by the finding , on both mr imaging and biopsy , that subchondral lesions contain synovial fluid and , sometimes , hypertrophic synovial pannus [ 44 ]  . 
 in the subgroup of patients with cystic rheumatoid arthritis , juxta - articular osteoporosis , joint - space thinning and destructive osteoarticular changes are less frequent than in the classic erosive form [ 45 ]  . 
 within the group of microcrystalline arthropathies , ctg is typically associated with well - marginated , eccentric erosions , both intra - , and extra - articular , characterised by joint - space sparing and the absence of juxta - articular osteoporosis . 
gouty erosions have a typically cystic appearance , with overhanging margins , related to reactive osteoproliferation extending beyond the theoretical border of the cortical bone to involve the contiguous soft tissues [ 46 ]  . 
tophi are characterised by a specific attenuation value of 170200 hu caused by the monosodium urate crystals [ 48 ]  . the mechanism underlying bone erosions in ctg , however , remains uncertain , and it seems unlikely that the local pressure exerted by the tophaceous mass alone is sufficient to cause bone damage . 
the most recent pathogenetic theory presupposes a combined mechanism of extrinsic compression and local production of lytic enzymes within the tophaceous tissue , which are thought to damage the osteoarticular structures [ 47 ]  . 
mr imaging may reveal perierosive bone marrow oedema [ 46 , 48 ]  . kienbcks disease and carpal amyloidosis according to the decoulx classification , later modified by lichtman , stage ii of kienbcks disease ( avascular necrosis of the lunate bone ) is radiographically characterised by small radiolucent , cyst - like inclusions within the spongiosa , surrounded by a dense osteosclerotic reaction and considered the expression of the bone remodelling stage preceding fragmentation ( stage iii ) [ 49 , 50 ]  . 
in stage ii of kienbcks disease , mr imaging shows a diffuse low signal intensity both on t1weighted se and in t2 - weighted fat - suppressed se sequences . in order to correctly diagnose kienbcks disease , mr signal alterations and osteosclerotic reaction should be anche panno sinoviale ipertrofico [ 44 ]  . 
 nel sottogruppo di pazienti con artrite reumatoide cistica losteoporosi juxta - articolare , il restringimento della rima articolare e le alterazioni distruttive osteoarticolari sono meno frequenti rispetto alla classica forma erosiva [ 45 ]  . allinterno del gruppo delle artropatie da microcristalli , la gotta cronica tofacea ( chronic tophaceous gout , ctg ) si associa tipicamente ad erosioni eccentriche , a margini ben definiti , sia intra - , sia extraarticolari , caratterizzate da risparmio dello spazio articolare e dallassenza di osteoporosi juxta - articolare . 
le erosioni gottose presentano un aspetto tipicamente cistico , con margini sovrastanti ( overhanging ) , determinati da una osteoproliferazione reattiva che si estende oltre il confine presunto della corticale ossea , spingendosi nei tessuti molli contigui [ 46 ]  . 
i tofi sono infatti caratterizzati da un valore di attenuazione specifico di 170200 uh , dovuto alla presenza di cristalli di urato monosodico al loro interno [ 48 ]  . il meccanismo alla base delle erosioni ossee nella ctg rimane tuttavia ancora incerto , e sembra poco verosimile che la sola pressione locale esercitata dalla massa tofacea sia sufficiente a determinare il danno osseo . 
la teoria patogenetica pi recente prende in considerazione un meccanismo combinato di compressione estrinseca e produzione locale di enzimi litici allinterno del tessuto tofaceo , che agirebbero danneggiando le strutture osteoarticolari [ 47 ]  . 
la rm pu dimostrare la presenza di edema osseo intraspongioso perierosivo [ 46 , 48 ]  . morbo di kienbock e amiloidosi del carpo in accordo con la classificazione di decoulx modificata da lichtman , lo stadio ii del morbo di kienbock ( necrosi avascolare dellosso semilunare ) caratterizzato , allesame radiografico tradizionale , da piccole inclusioni intraspongiose radiotrasparenti di aspetto cistico , circondate da una densa reazione osteosclerotica , considerate espressione del rimodellamento osseo che precede lo stadio della frammentazione ( stadio iii ) [ 49 , 50 ]  . 
lindagine rm dimostra nello stadio ii del morbo di kienbock una diffusa bassa intensit di segnale sia nelle sequenze se t1 - , sia nelle sequenze se t2 - pesate a soppressione del grasso . al fine di una corretta diagnosi di morbo di kienbock necessario che i cambiamenti del segnale rm e la reazione spongiosclerotica siano diffuse e coinvolgano losso semilunare nella sua interezza . 
histological examination of biopsy specimens demonstrates that these bone lesions are filled with amyloid - positive synovial minate , mediante un meccanismo di compressione estrinseca , dallaccumulo di sostanza amiloide nella membrana sinoviale . 
the radiological suspicion of intra - articular deposits of amyloid substance in the carpus must be confirmed histologically with congo red staining and an electron or polarised - light microscope [ 53 , 54 ]  . 
in carpal amyloidosis , conventional radiography shows radiolucent lesions of varying size within the spongiosa , which may carpo richiede conferma istologica mediante la colorazione con rosso congo e limpiego del microscopio elettronico o a luce polarizzata [ 53 , 54 ]  . 
le alterazioni osteolitiche carpali , in pazienti sottoposti a emodialisi da lungo tempo , non sono una caratteristica esclusiva dellamiloidosi , in quanto possono anche riflettere una condizione di iperparatiroidismo secondario allinsufficienza renale . mr imaging can accurately depict the involvement of la rm consente una accurata valutazione del coinvolgiintrusione di liquido sinoviale attraverso fissurazioni cartilaginee micromovimenti e carico in sede di frattura varie lesioni che conducono alla formazione di cisti ripiene di sangue sostituzione di trabecole di osso spongioso sostituzione di trabecole di osso spongioso sostituzione di trabecole di osso spongioso compressione estrinseca compressione estrinseca 1372 radiol med ( 2012 ) 117 : 13551373 bones , joints and soft tissues in patients with carpal amyloidosis . 
in most cases , bone lesions have low signal intensity on t1 - weighted sequences , and extremely variable signal intensity on t2 - weighted sequences , depending on hydration levels . 
synovial thickening is also well depicted both on t1and t2 - weighted sequences [ 54 ]  . mento osseo , articolare e dei tessuti molli nei pazienti con amiloidosi del carpo . 
nella maggior parte dei casi le lesioni ossee presentano una bassa intensit di segnale nelle sequenzet1 - pesate , ed unintensit di segnale molto variabile nelle sequenze t2 - pesate , in relazione allo stato di idratazione . 
lispessimento sinoviale inoltre ben visualizzabile sia nelle sequenze t1 - , sia in quelle t2 - pesate [ 54 ]  . conclusions conclusioni conventional radiology is often the first step in characterising carpal osteolytic lesions , which may be caused by a variety of pathological mechanisms . 
the use of mdct and mr imaging to supplement and complement radiography can provide useful information for establishing a correct diagnosis , with biopsy being reserved for suspected neoplastic lesions ( table 1 )  . la radiologia tradizionale rappresenta spesso il primo approccio nella caratterizzazione delle lesioni osteolitiche del carpo , che possono essere determinate da molteplici meccanismi patologici . 
orsola malpighi , azienda ospedaliero - universitaria di bologna , via massarenti 9 , 40138 bologna , italy 2servizio sanit pubblica , direzione generale sanit e politiche sociali , regione emilia - romagna , via a . 
the 20 procedures amongst cr , ct , nm and ir that in 2006 contributed the most to emilia - romagna population radiation dose are described in detail : cr , ct , nm and ir contribute to approximately 10% , 66% , 9% and 15% of the total dose , and to 70% , 21% , 3% and 6% of procedure frequency , respectively . 
si sono indicate le 20 procedure tra quelle di rc , tc , mn e ri che nel 2006 hanno fornito i pi elevati contributi di dose alla popolazione emiliano - romagnola . 
 le percentuali di rc , tc , mn e ri sono rispettivamente circa 10% , 66% , 9% e 15% per la dose e 70% , 21% , 3% e 6% per la frequenza di prestazioni . 
fondamentale che venga curata radiol med ( 2012 ) 117 : 312321 as ir operators are often not radiologists , special attention should be paid to education in radiation protection of the professionals involved . in modo approfondito la formazione radioprotezionistica degli specialisti che spesso non sono radiologi . keywords interventional radiology radiation dosimetry patient protection parole chiave radiologia interventistica dosimetria radioprotezione paziente introduction introduzione ionising radiation has been used in medicine for over a century for diagnostic and therapeutic purposes , and this use has been regulated over the years to minimise the associated risks . 
187 / 2000 [ 1 ] in italy emphasised the importance of two principles of radiation protection that should always be applied in the field of medicine : examination justification and radiological procedure optimisation . 
application of these principles has provided healthcare workers with the means and the opportunity to constantly improve their activity at whatever level they operate . in addition to fulfilling the legal obligations provided for by the abovementioned decree , in 2000 ( the year the european union ( eu ) directive 97 / 43 / euratom was transposed [ 2 ] ) , the emilia - romagna region began to perform data - collection campaigns of radiation dose and procedure frequency [ 37 ] to monitor radiation dose delivered to the regions population due to medical radiodiagnostic exposure resulting from conventional radiology ( cr ) , computed tomography ( ct ) and nuclear medicine ( nm ) procedures . 
 accuracy of the evaluations has gradually improved thanks to the diffusion of a culture of patient radiation protection among the facilities of the regional health service [ 7 ]  . 
as a result , the most recent data - collection campaign also gathered data regarding interventional radiology ( ir ) procedures performed in 2006 , thus completing the spectrum of health services that significantly contribute to the population dose from medical exposures to ionising radiation . 
indeed , only radiation therapy procedures have been excluded , but the evaluation of radiobiological risks associated with radiotherapy doses is performed differently to evaluation associated with radiological and nuclear medicine procedures and is therefore always left out in studies of this kind . the aim of this study was to supplement the analysis of data published in this journal regarding cr , ct and nm [ 5 , 7 ] with data regarding ir , with a view to illustrating the contribution of all radiological procedures to the dose delivered to the emilia - romagna population to compare with similar studies conducted in other countries and to describe a method for collecting and evaluating radiation dose data that can be applied to other situations . le radiazioni ionizzanti vengono usate in medicina da oltre un secolo sia a scopo diagnostico sia a scopo terapeutico e tale utilizzo stato regolamentato nel corso degli anni in modo da tenere sotto controllo i rischi correlati . 
187 / 2000 [ 1 ] ha sottolineato limportanza dei due principi di radioprotezione del paziente che devono sempre essere applicati in campo medico , cio la giustificazione degli esami e lottimizzazione delle procedure radiologiche , fornendo mezzi ed opportunit agli operatori sanitari , a qualunque livello essi lavorino , per adoperarsi in un miglioramento costante delle loro attivit . la regione emilia - romagna , oltre ad ottemperare agli obblighi normativi previsti da tale decreto , ha iniziato fin dal 2000 ( anno di recepimento della direttiva europea 97 / 43 / euratom [ 2 ] ) ad effettuare campagne di raccolta dati dosimetrici e di frequenza delle prestazioni [ 37 ] per monitorare la dose alla popolazione regionale dovuta ad esposizioni mediche di radiodiagnostica nelle procedure di radiologia convenzionale ( rc ) , tomografia computerizzata ( tc ) e medicina nucleare ( mn )  . 
laccuratezza nelle valutazioni effettuate progredita gradualmente grazie alla diffusione di una cultura di radioprotezione del paziente presso le strutture sanitarie del servizio sanitario regionale [ 7 ] e pertanto nellultimo monitoraggio sono stati richiesti i dati riguardanti le procedure di radiologia interventistica ( ri ) relativi allanno 2006 , completando in questo modo lo spettro di prestazioni sanitarie in grado di apportare un contributo significativo alla dose alla popolazione da esposizioni mediche dovute a radiazioni ionizzanti : infatti rimane esclusa la sola radioterapia , ma la valutazione dei rischi radiobiologici associata alle dosi somministrate per fini radioterapeutici si pone in modo differente rispetto a quella associata alle pratiche di radiologia e di medicina nucleare e quindi viene sempre tralasciata in questo tipo di studi . scopo del presente lavoro completare lanalisi dei dati gi presentati in passato su questa stessa rivista relativamente alle procedure di rc , tc e mn [ 5 , 7 ] integrandole con quelle di ri ed illustrando in tale modo il contributo di tutte le pratiche radiologiche alla dose alla popolazione della regione emilia - romagna , per confrontarla con indagini analoghe condotte in altre nazioni e mostrare una 314 materials and methods considering 2006 as the reference year , we estimated the exposure of the regions population due to ir procedures by monitoring all procedures performed in the region and specifically characterising the dose for each procedure . 
 following the data collection procedure successfully used for cr , ct and nm ( where examinations were analysed that contribute significantly to the effective collective dose in that they are the most widespread or have a significant dose impact for the individual patient ) , we considered 30 ir procedures divided into six major categories ( cardiology , general ir , neuroradiology , surgery , gastroenterology , orthopaedics ) and grouped them together in several homogeneous classes according to examination type , as shown in the first two columns of table 1 . information was then acquired regarding the frequency of these procedures in the 17 health facilities in emiliaromagna ( university hospital trusts of bologna , ferrara , modena , reggio emilia , rimini ; local health authorities of bologna , cesena , ferrara , forl , imola , modena , parma , piacenza , ravenna , reggio emilia , rimini ; rizzoli orthopaedic institutes of bologna ) , by directly requesting the number of examinations performed at each facility subdivided by typology and , where collected data were incomplete , by extrapolating results on the basis of averages and proportions performed on other healthcare facilities . with regard to radiation dose measurements , calculating e is standardised for cr , ct and nm , whereas there is still no universally accepted procedure for ir examinations . 
 indeed , the dynamic nature of ir examinations ( variable fluoroscopy times , multiple fields of view and projections , etc . ) , the use of both fluorography and fluoroscopy and the broad range of possible settings make it unfeasible to use the dosimetric units used for cr , ct and nm . 
therefore , in line with indications described in the literature [ 1014 ] , we measured the dose in this type of examination using the dosearea product ( dap ) ; from this , with the use of suitable conversion coefficients , we arrived at an estimate of the effective dose for each procedure . as dose values in ir are not subject to systematic compulsory measurements in accordance with italian legislative decree no . 
187 / 2000 - as occurs , for example , for diagnostic reference levels in cr , ct and nm - we identified a number of health facilities of the regional health service for each of the six categories reported in table 1 ( at least one per sector ) where the medical physics departments perform this type of dose measurement , in order to obtain the dap values characteristic of the various types of ir examinations . 
the seven health facilities identified cover radiol med ( 2012 ) 117 : 312321 modalit di raccolta e valutazione dei dati dosimetrici applicabile anche in altre realt . materiali e metodi stato preso in considerazione lanno di riferimento 2006 procedendo alla stima dellesposizione della popolazione regionale dovuta agli esami di radiologia interventistica monitorando le procedure effettuate in ambito regionale e , per ognuna , effettuando una caratterizzazione dosimetrica specifica . 
le grandezze dosimetriche utilizzate , in accordo con le pi recenti raccomandazioni emerse a livello internazionale , sono state la dose efficace ( e ) e la dose efficace collettiva ( s ) [ 79 ]  . 
 seguendo lo schema ormai collaudato per la raccolta dati in rc , tc e mn ( dove sono stati analizzati esami che forniscono un contributo rilevante alla dose efficace collettiva in quanto sono i pi diffusi oppure quelli che hanno un impatto dosimetrico rilevante per il singolo paziente ) sono state prese in considerazione 30 procedure interventistiche suddivise in 6 macrosettori di applicazione ( cardiologia , radiologia interventistica generale , neuroradiologia , chirurgia , gastroenterologia , ortopedia ) e raggruppate in poche classi omogenee per tipologia di indagine , come mostrato nelle prime due colonne della tabella 1 . si quindi proceduto ad acquisire informazioni relative alla frequenza di queste procedure eseguite nelle 17 aziende sanitarie ( as ) dellemilia - romagna ( aziende ospedaliero - universitarie di bologna , ferrara , modena , parma e reggio emilia ; aziende unit sanitarie locali [ usl ] di bologna , cesena , ferrara , forl , imola , modena , parma , piacenza , ravenna , reggio emilia , rimini ; istituti ortopedici rizzoli di bologna ) , richiedendo direttamente alle as il numero di esami suddiviso per tipologia e , ove i dati raccolti fossero incompleti , estrapolando i risultati in base a medie e proporzioni effettuate sulle altre as . dal punto di vista dosimetrico , il calcolo di e una metodica standardizzata negli esami diagnostici di rc , tc e mn , mentre per gli esami di ri non esiste ancora una procedura universalmente accettata : infatti nelle procedure interventistiche la natura dinamica dellesame ( tempi di scopia alquanto variabili , multipli campi di vista e proiezioni , ecc . ) , lutilizzo sia della modalit grafia sia della modalit scopia e lampio range di possibili parametri operativi che si possono impiegare rendono non significativo lutilizzo delle grandezze dosimetriche usate per la rc , tc e mn . 
after having calculated e for the various procedures , we calculated the collective effective dose ( s ) and the percapita dose ( s / number of inhabitants in emilia romagna )  . results the third and the fourth column of table 1 report , respectively , the number of procedures subdivided by type and s value for each procedure . 
figure 1 graphically depicts the subdivision of the contribution of the six categories to the collective effective dose due to ir procedures alone in poich i valori di dose in ri non sono oggetto di misura da effettuarsi obbligatoriamente in maniera sistematica ai sensi del d . 
187 / 2000 come invece avviene , ad esempio , per i livelli diagnostici di riferimento in rc , tc e mn , per ognuno dei 6 macrosettori riportati in tabella 1 sono state identificate diverse as del servizio sanitario regionale ( almeno una per settore ) , i cui servizi di fisica sanitaria effettuano questo tipo di misure dosimetriche , per ottenere dei valori di dap caratteristici delle varie tipologie di esami di ri . 
particularly noteworthy are the cardiology procedures , which account for around 48% of the dose , followed by general ir with around 43% , with the other four sectors accounting for < 5% . in order to place these data in a broader context , the analogous results obtained in the same year for cr , ct and nm and reported in a previous study [ 7 ] need to be considered . 
therefore , figure 2 shows the 20 cr , ct , nm and ir procedures that in 2006 accounted for the greatest contribution to total dose , with relative percentages , whereas the percentage contributions of the same procedures to the total number of examinations are also shown . 
data reported in le grandezze dosimetriche dose efficace collettiva , s , e dose pro - capite ( s / numero degli abitanti dellemilia - romagna )  . risultati nella terza e quarta colonna della tabella 1 sono riportate rispettivamente il numero di procedure suddiviso per tipologia ed il valore di s per ogni procedura . 
in figura 1 si illustra graficamente la suddivisione dei contributi dei 6 macrosettori alla dose efficace collettiva dovuta alle sole procedure interventive in emilia - romagna nellanno 2006 : radiol med ( 2012 ) 117 : 312321 fig . 
figure 3 graphically shows the subdivision of these contributions to the collective effective dose and the number of examinations / procedures , all the time with the aim of considering the entire spectrum of medical procesi nota che le procedure di cardiologia contribuiscono per circa il 48% a questa dose , seguite da quelle di radiologia interventistica generale con circa il 43% , mentre ognuno degli altri settori fornisce meno del 5% . se si vogliono inserire questi dati in un contesto pi ampio occorre considerare anche i risultati analoghi ottenuti relativamente allo stesso anno in rc , tc e mn e riportati in un precedente lavoro [ 7 ] : pertanto in figura 2 si riportano le 20 procedure di rc , tc , mn e ri che hanno fornito nel 2006 i pi elevati contributi alla dose della popolazione emiliano - romagnola , con le relative percentuali , e conte318 radiol med ( 2012 ) 117 : 312321 fig . 
3a , b suddivisione dei contributi delle quattro metodiche [ radiologia convenzionale ( rc ) , tomografia computerizzata ( tc ) , medicina nucleare ( mn ) e radiologia interventistica ( ri ) ] alla dose efficace collettiva ( a ) ed al numero di prestazioni ( b ) nel 2006 . dures that use ionising radiation , with the exclusion of radiation therapy . 
 lastly , nm accounts for 8.5% of s and only 3% of total examinations / procedures . discussion the first problem that arose in organising this study was lexical in nature and similar to that seen with cr and ct when the emilia - romagna region began data collection campaigns [ 5 , 15 ]  . 
the indications recently provided in the literature have clarified the issue by describing a radiological examination ( or an interventional procedure ) as one or a series of x - ray exposures of an anatomical region in which a single imaging modality is used to answer a specific clinical query or diagnostic problem during one visit to the hospital [ 16 ]  . 
this definition does not completely eliminate the possibility of ambiguity in some types of examinations , but those reported in table 1 , defined by medical specialists in the relevant discipline , facilitated and rendered uniform data collection regarding examination frequency . figure 3 shows that the different contribution of the different types of procedures using ionising radiation to the dose delivered to the population can provide useful indications regarding the sectors in which it would be best stualmente vengono indicati anche i contributi percentuali delle stesse procedure al numero totale di prestazioni . 
linsieme di tutti i contributi riportati in figura 2 rappresenta circa il 96% della dose efficace collettiva alla popolazione dellemilia - romagna dovuta alle esposizioni mediche analizzate nel presente lavoro . tenendo conto dei contributi dosimetrici delle quattro metodiche ( rc , tc , mn e ri ) si possono stimare la dose efficace collettiva e la dose pro - capite alla popolazione emiliano - romagnola nellanno 2006 , pari rispettivamente a 5237 sv - persona e a 1 , 2 msv . 
in figura 3 si illustra graficamente la suddivisione di tali contributi alla dose efficace collettiva ed al numero di prestazioni , sempre con lintento di considerare tutto lo spettro delle procedure che utilizzano radiazioni ionizzanti in campo medico , ad esclusione di quelle radioterapeutiche . 
si nota che la rc contribuisce per il 10 , 4% a s e per il 69 , 8% alla frequenza di prestazioni : invece il contributo della tc a s circa 6 volte maggiore ( 66 , 2% ) e quello alla frequenza di prestazioni circa 3 volte minore ( 20 , 8% )  . 
il peso relativo della ri simile a quello della tc : infatti , pur essendo le prestazioni soltanto il 6 , 4% del totale , il peso dosimetrico pari al 14 , 9% . 
infine , la mn contribuisce a s per l8 , 5% e soltanto per il 3% al numero di prestazioni . discussione il primo problema che si presentato nellorganizzare il presente studio in ri stato di tipo lessicale , come gi si era riscontrato nellambito della rc e della tc quando la regione emilia - romagna dette inizio alle relative campagne di raccolta dati [ 5 , 15 ]  . 
 whereas data show the well - known fact that ct delivers the highest dose , they also demonstrate the ir has a very similar trend in that the technique is used around 12 times less frequently than cr but accounts for 45% more of the collective effective dose delivered to the emilia - romagna population than cr . 
ir procedures have numerous advantages , and their use is destined to increase ( in some countries , their number doubles every 24 years [ 17 ] ) , as in some diseases , ir allows a greater number of cases to be treated with lower costs and less patient discomfort than do other more invasive techniques . 
as these procedures are often performed not by radiologists but by specialists in other disciplines , it is paramount that not only the appropriateness of the individual examination is guaranteed , but also that special attention is paid to training operators in terms of radiation protection and correct and optimal use of ionising radiation , as is recommended with increasing insistence by international bodies [ 9 , 17 ]  . although the use of effective dose and collective effective dose such as dosimetric quantities for this type of analysis was the subject of debate following the latest recommendations of the international commission on radiological protection , they are considered perfectly suitable for evaluations such as the one performed in this study [ 9 , 16 , 1820 ]  . 
we also felt it appropriate to include nm examinations ( even though similar studies do not take them into consideration ) , in part to provide a holistic approach to the topic and in part because italian legislative decree no . 
187 / 2000 defines radiodiagnostic as being related to medical diagnostic radiology and in vivo diagnostic nuclear medicine . ir data collected in this study are based on values measured in a percentage of health facilities that do not cover the entire region . 
nonetheless , the estimate performed is reliable , as it is based on values measured in the field and shows that a culture of patient radioprotection and procedure optimisation is widespread ; all operators and health facilities contacted were highly cooperative , even with regards to requests that went beyond their legal obligations . the per - capita dose makes possible practice comparisons between nations and regions that have a similar level of healthcare services [ 21 ]  . 
as table 2 shows , the percapita dose in the emilia - romagna region is in line with levels obtained in other surveys performed in countries with well - developed national health services [ 10 , 2224 ] , considering that some of these surveys did not take into account nm procedures . in letteratura hanno fatto chiarezza in merito descrivendo un esame radiologico ( o una procedura interventistica ) come una o una serie di esposizioni di una regione anatomica in cui si utilizza ununica modalit di imaging , necessaria a rispondere ad uno specifico quesito clinico o problema diagnostico durante una singola visita in ospedale [ 16 ] : tale definizione non elimina completamente possibili ambiguit nellinterpretazione di alcune tipologie di esame , ma quelle riportate in tabella 1 , definite dai medici specialisti dei vari settori , hanno facilitato e reso uniforme la raccolta dei dati relativi alle frequenze . dalla figura 3 si nota che il contributo differenziale delle diverse tipologie di procedure utilizzanti radiazioni ionizzanti alla dose alla popolazione pu fornire utili indicazioni relativamente ai settori in cui pi opportuno concentrare gli sforzi per diminuire la dose erogata oppure per ottimizzare nel modo pi efficiente ed efficace la radioprotezione del paziente . 
oltre allevidenza , gi nota , che la tc rappresenta la metodica che somministra la maggior dose si pu infatti notare che la radiologia interventistica ne sta seguendo da vicino landamento , in quanto in termini di frequenza circa 12 volte inferiore alla rc ma eroga alla popolazione dellemilia - romagna il 45% in pi di dose efficace collettiva rispetto alla rc . 
le procedure di ri presentano molti vantaggi e si andranno sempre pi diffondendo ( in alcune nazioni il loro numero raddoppia ogni 24 anni [ 17 ] ) in quanto in alcune patologie offrono lopportunit di trattare un maggior numero di casi con minori costi e minori disagi per i pazienti rispetto ad altre metodiche pi invasive : inoltre con queste tecniche si possono ridurre i giorni di degenza necessari ed i rischi , dovuti a fattori diversi dalle radiazioni ionizzanti , per il paziente . 
 poich queste procedure vengono spesso eseguite non da radiologi bens da medici specialisti in altre discipline fondamentale , oltre al garantire lappropriatezza dei singoli esami , che venga curata in modo approfondito la formazione degli operatori dal punto di vista della radioprotezione del paziente e del corretto ed ottimale utilizzo delle radiazioni ionizzanti , come del resto raccomandato sempre pi insistentemente dagli organismi internazionali [ 9 , 17 ]  . luso della dose efficace e della dose efficace collettiva come grandezze dosimetriche da usare in analisi di questo tipo stato oggetto di dibattito dopo la pubblicazione delle ultime raccomandazioni dellinternational commission on radiological protection ma attualmente lo si ritiene assolutamente adeguato per valutazioni come quella esaminata in questo lavoro [ 9 , 16 , 1820 ] , nella quale inoltre si ritenuto corretto includere anche gli esami di medicina nucleare ( nonostante in alcuni studi omologhi al presente non siano stati presi in considerazione ) , sia per fornire un approccio olistico allargomento sia perch nel d . 
 320 radiol med ( 2012 ) 117 : 312321 table 2 per - capita dose for the emilia - romagna population ( reference year , 2006 ) compared with some values reported in the literature country per - capita effective dose [ msv ] reference no . 
ir procedures are becoming increasingly frequent and widespread due to their undeniable advantages over other more invasive techniques ; however , they do involve delivering high doses of ionising radiation to the patient and should therefore receive the same attention that is paid to other high - dose techniques , such as ct . 
in addition , physicians who use these procedures often are not radiologists , so it is paramount that not only the appropriateness of the individual examination is guaranteed but also that special attention is paid to training operators in terms of patient radiation protection and the correct and optimal use of ionising radiation . 
 in analyses of this type , the dosimetric values measured in the field provide added value to the reliability of the study , and therefore , data collection campaigns of radiation dose in ir will need to be extended in the future . e alla medicina nucleare diagnostica in vivo . i dati raccolti relativamente alla ri si basano sui valori misurati in una percentuale di strutture sanitarie che non esaurisce la realt regionale , per quanto ne costituisca un riferimento affidabile : pertanto si dovranno reperire ulteriori informazioni nelle prossime campagne di raccolta dati , ma si ritiene che la stima effettuata sia comunque attendibile , in quanto basata su valori misurati sul campo , e dimostri che su tutto il territorio regionale si sia diffusa una cultura di radioprotezione del paziente e di ottimizzazione delle procedure per cui tutti gli operatori e le strutture interpellati rispondono in maniera collaborativa anche a richieste che vanno al di l del mero adempimento normativo . la dose pro - capite permette il confronto di pratiche tra nazioni e regioni che hanno un livello di cure sanitarie analogo [ 21 ] : come si pu notare in tabella 2 , il valore di dose pro - capite della regione emilia - romagna allineato con quelli ottenuti in altre campagne di raccolta dati eseguite in paesi con servizi sanitari nazionali ben sviluppati [ 10 , 2224 ] , tenendo anche presente che in alcune di queste le procedure di medicina nucleare non erano state prese in considerazione . conclusioni la stima della dose alla popolazione dovuta ad esposizioni mediche , oltre ad essere un obbligo di legge , rappresenta un validissimo strumento per monitorare nel tempo landamento delle diverse pratiche cliniche che utilizzano radiazioni ionizzanti , per ottimizzarne lutilizzo e per valutare limpatto delle pratiche di radioprotezione del paziente adottate in uno stato / regione tramite il confronto con altre realt sanitarie . 
le procedure di radiologia interventistica si vanno sempre pi diffondendo a causa dei loro innegabili vantaggi rispetto ad altre metodiche pi invasive , per comportano elevate dosi ai pazienti e pertanto necessario dedicare ad esse la stessa attenzione che si rivolge ad altri esami con elevato impatto dosimetrico , come ad esempio quelli di tomografia computerizzata . 
inoltre i medici che usano queste procedure spesso non sono radiologi e quindi fondamentale , oltre al garantire lappropriatezza dei singoli esami , che venga curata in modo approfondito la formazione degli operatori sia nel campo della radioprotezione del paziente sia in quello del corretto ed ottimale utilizzo delle radiazioni ionizzanti . 
cademartiri1 , 2 1dipartimento di radiologia e del cuore , c / o piastra tecnica piano 0 , azienda ospedaliero - universitaria di parma , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia , ospedale san martino , genova , italy 4dipartimento di radiologia , universit di messina , messina , italy 5dipartimento di cardiologia , ospedale san gennaro , napoli , italy 6dipartimento di cardiologia , universit di foggia , foggia , italy 7dipartimento di radiologia , universit di verona , verona , italy 8dipartimento di cardiologia , universit di padova , padova , italy correspondence to : f . 
from a population of 2 , 881 consecutive patients ( 1 , 842 men , mean age 6213 years ) in sinus rhythm who underwent ctca , we extracted data on patients with suspected coronary artery disease ( cad )  . 
 we selected patient outliers in the fifth and sixth decades of life with the following criteria : 3 risk factors and absence of cad , zero to one risk factors and 5 diseased coronary segments . 
scopo del nostro lavoro stato valutare i criteri di selezione , la presenza e la distribuzione dei pazienti outliers mediante angiografia coronarica non invasiva con tomografia computerizzata ( ctca ) in un ampio database istituzionale . 
da una popolazione di 2881 pazienti consecutivi ( 1842 maschi , et media 6213 anni ) in ritmo sinusale sottoposti a ctca sono stati estratti i pazienti con indicazione allo studio delle coronarie per sospetta malattia coronarica ( cad )  . 
sono stati quindi selezionati i pazienti outliers nella 5a e 6a decade : pazienti con pi di 3 fattori di rischio e assenza di cad ; pazienti con 0 - 1 fattore di rischio e cad su pi di 5 segmenti coronarici . 
di questi , 210 erano nella 5a decade e 231 nella 6a decade ( maschi 196 , femmine 245 ) , e quelli con pi di 3 fattori di rischio erano il 4 , 2% ( 102 / 2432 ; maschi 42 , femmine 60 )  . 
 this will enable dedicated trials aimed at characterising biomarkers and genomics of protective and nonprotective factors against cad and its complications . keywords ct coronary angiography coronary artery disease outliers risk factors coronarici affetti da cad erano il 28% ( 686 / 2432 ; 510 maschi , et media 6810 anni )  . 
questo consentir di effettuare studi mirati per la caratterizzazione dei biomarkers e della genetica dei fattori protettivi / anti - protettivi rispetto alla malattia coronarica ed alle sue complicanze . parole chiave angiografia coronarica con tomografia computerizzata malattia coronarica outliers fattori di rischio introduction introduzione computed tomography coronary angiography ( ctca ) is an accurate and robust modality for diagnosing and excluding coronary artery disease ( cad ) [ 18 ]  . 
the same concept can be used to select patients with characteristics that differ from the classic presentation as far as the association between risk factors and presence / severity of cad is concerned [ 24 ]  . 
these patients can be defined as outliers , and in our case they consist of individuals with healthy coronary arteries and multiple risk factors or those without risk factors but with advanced cad . 
studying and mapping these individuals using ctca as a morphological tool could facilitate focused genetic studies , with the potential for identifying further targets to prevent cad . the aim of our study was to demonstrate how ctca langiografia coronarica con tomografia computerizza ta ( ctca ) una metodica accurata e robusta per la diagno si e lesclusione della malattia coronarica [ 18 ]  . 
laterosclerosi coronarica , oltre alle stenosi , si stanno dimostrando parametri utili nella stratificazione del rischio cardiovascolare dei pazienti con sospetta malattia coronarica ( cad ) [ 17 , 22 , 23 ]  . alcune esperienze dimostrano come la stratificazione del rischio secondo i parametri convenzionali ( per esempio , framingham risk score , morise score , score , ed altri ) sia inadeguata rispetto al dato ctca [ 2433 ]  . 
 lo stesso concetto pu essere utilizzato per selezionare i pazienti che mostrano caratteristiche difformi da quelle classiche per quanto concerne lassociazione tra fattori di rischio e presenza / severit della malattia coronarica [ 24 ]  . 
 questi pazienti possono essere definiti outliers e consistono , nel nostro caso , di individui o pazienti con coronarie indenni e multipli fattori di rischio oppure di individui o pazienti senza fattori di rischio , ma con aterosclerosi coronarica avanzata . 
lo studio e la mappatura di questi individui utilizzando la ctca come 216 radiol med ( 2012 ) 117 : 214229 can be used to select from a large institutional database the population of outlier patients . materials and methods patient population from january 2005 to june 2010 , 2 , 881 consecutive patients ( 1 , 842 men , mean age 6213 years ) were studied with ctca . 
 the ethics committee approved the study , and all patients provided informed consent . patient preparation in the absence of absolute contraindications , intravenously administered beta blockers ( 100 mg atenolol , 5 mg propranolol , 5 mg metoprolol ) were administered to patients with a heart rate ( hr ) > 60 beat per minute ( bpm ) directly in the diagnostic suite under constant electrocardiographic ( ecg ) and pressure monitoring . 
immediately prior to examination , a single dose of isosorbide dinitrate ( 2 mg ) was administered sublingually . scan protocol and image reconstruction a 64 - slice ct system ( sensation 64 , siemens , forchheim , germany ) was used according to standard protocols described elsewhere [ 39 ]  . 
lo scopo dello studio di dimostrare come la ctca possa essere utilizzata per selezionare la popolazione degli outliers da un ampio database istituzionale . materiali e metodi popolazione da gennaio 2005 a giugno 2010 , sono stati studiati 2881 ( 1842 maschi , et media 6213 anni ) pazienti consecutivi mediante ctca . 
i pazienti con sindro me coronarica acuta nei quali la scansione di tomografia computerizzata ( tc ) avrebbe provocato un ritardo nellesecuzione della rivascolarizzazione o quelli nei quali esistevano delle controindicazione assolute alla somministrazio ne intravenosa di mezzo di contrasto iodato ( per esempio , allergia nota , insufficienza renale o disordini tiroidei ) so no stati esclusi dallo studio . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . preparazione del paziente in assenza di contro - indicazioni assolute , nei pazienti con una frequenza cardiaca ( fc ) superiore a 60 battiti per minuto ( bpm ) sono stati somministrati beta - bloccanti per via endovenosa ( atenololo 100 mg , propanololo 5 mg , metoprololo 5 mg ) direttamente in sala diagnostica con monitoraggio elettrocardiografico e pressorio costante . 
nei pazienti con controindicazioni assolute ai beta - bloccanti ( vale a dire , stenosi valvolare aortica severa , asma bronchiale in trattamento con steroidi , blocchi atrio - ventricolari ) , sono stati utilizzati calcio antagonisti ( diltiazem 5 mg , verapamil 5 mg ) per via endovenosa . 
nei pazienti con evidente componente ansiosa stata somministrata per via orale una dose di 1 mg di lorazepaimmediatamente prima della scansione stato somministrata una singola dose sub - linguale di isosorbide dinitrato ( 2 mg )  . radiol med ( 2012 ) 117 : 214229 scan parameters used the lowest collimation available ( 0.6 mm ) , with pitch appropriately reduced to allow oversampling ( 0.2 ) and 120 kv and 600900 mas . 
temporal windows used were the mid and end - diastolic phase ( from 300 / 450 ms before the next r - wave and / or at 6070% of the r - r interval )  . 
a dedicated software package ( windose , institute of medical physics , erlangen , germany ) was used to calculate ionising radiation dose delivered to the patient during the angiographic scans ( mean value 15.2 msv for women and 21.4 msv for men )  . 
segments were classified as normal / no significant disease ( healthy or with lumen irregularities or < 50% lumen reduction ) or significantly diseased ( 50% stenosis of the lumen )  . statistical analysis data are reported as prevalence , mean and standard deviation ( sd )  . 
diabetes mellitus protocollo di scansione e ricostruzione delle immagini per lindagine stato utilizzata una apparecchiatura tc a 64 strati ( sensation 64 , siemens , forchheim , germania ) secondo protocolli standard gi descritti [ 39 ]  . 
i parametri di scansione hanno sfruttato la minore collimazione disponibile ( 0 , 6 mm ) , il pitch ridotto adeguato al sovra campionamento delle informazioni ( 0 , 2 ) , 120 kv , 600900 mas . 
sono stati somministrati 80100 ml di mezzo di contrasto iodato ( iomeprolo , iomeron 400 mgi / ml , bracco ) alla velocit di 46 ml / s mediante iniettore automatico ( stellant , medrad , pittsburgh , usa ) collegato ad unagocannula da 1820 gauge preventivamente posizionata in una vena antecubitale . 
allo scopo di ottimizzare lopacizzazione dei vasi arteriosi coronarici stata utilizzata la tecnica del bolus - tracking per sincronizzare larrivo del mezzo di contrasto nelle arterie coronarie con linizio della scansione ed il bolo di salina di seguito al bolo di mezzo di contrasto [ 4042 ]  . le immagini sono state ricostruite con spessore di strato pari a 0 , 75 mlincremento di ricostruzione stato mantenuto al 50%60% dello spessore di strato ( 0 , 4 mm )  . 
 le finestre temporali utilizzate sono state la fase mesoe telediastolica ( da - 300 / - 450 ms prima della successiva onda r e / o dal 60%70% dellintervallo r - r )  . 
quando ritenuto necessario ( per esempio , in caso di persistente movimento cardiaco residuo che riduce la qualit diagnostica dellimmagine ) sono state analizzate altre ricostruzioni in fase telesistolica ( + 225 / + 325 ms dopo la precedente onda r e / o dal 25%40% dellintervallo r - r )  . 
utilizzando un software dedicato ( windose , istituto di fisica medica , erlangen , germania ) stata calcolata la dose di radiazioni ionizzanti alla quale i pazienti sono stati esposti durante la scansione angiografica ( valore medio 15 , 2 msv per le donne e 21 , 4 msv per gli uomini )  . 
sulle singole 218 radiol med ( 2012 ) 117 : 214229 lesioni sono state effettuate quindi ricostruzioni multiplanari longitudinali ed assiali per classificare le lesioni come significative o non - significative . 
 i segmenti sono stati classificati come normali / non significativamente malati ( indenni o con irregolarit del lume o con riduzione del diametro < 50% ) o significativamente malati ( stenosi del lume 50% )  . analisi statistica i dati sono presentati come prevalenze , medie e deviazioni standard . 
in questa popolazione il calcio coronarico era pari a 0 ( criterio di selezione ) ed i fattori di rischio pi frequenti erano nellordine lipertensione ( 45% ; 379 / 837 ) , la familiarit ( 44% ; 366 / 837 ) , e la dislipidemia ( 36% ; 302 / 837 ) ( tabella 1 )  . 
in questa popolazione il calcio coronarico era pari a 819947 e abbiamo osservato un prevalenza di malattia ostruttiva ( riduzione del lume 50% di almeno un segmento coronarico ) pari al 63% ( 430 / 686 )  . 
cdx , coronaria destra ; csx , coronaria sinistra ; tcs , tronco comune sinistro ; acx , arteria coronaria circonflessa ; ada , arteria coronaria discendente anteriore . was in all cases considered independently with respect to the other risk factors due to its particular characteristics . 
in this population , the coronary calcium score was 0 ( selection criteria ) ; the most frequent risk factors were hypertension ( 45% ; 379 / 837 ) , family history ( 44% ; 366 / 837 ) and dyslipidaemia ( 36% ; 302 / 837 ) ( table 1 )  . 
patients with more than five coronary artery segments affected by cad accounted for 28% of the total ( 686 / 2 , 432 : 510 men , mean age 68 10 years )  . 
cad , malattia coronarica ; pts , pazienti ; decade , decade di et . population , coronary calcium score was 819 947 , and we observed a prevalence of obstructive disease ( 50% lumen reduction in at least one coronary artery segment ) equal to 63% ( 430 / 686 )  . 
a total of 210 patients with healthy coronary arteries ( tables 2 and 4 ) were in the fifth decade of life , and 231 were in the sixth decade ( men 196 , women 245 )  . 
a total of 115 patients with more than five diseased coronary artery segments ( tables 3 and 4 ) were in the fifth decade , and 270 were in the sixth decade ( men 309 , women 76 )  . 
with further restriction of selection criteria , we identified a subpopulation of patients with healthy coronary arteries ( n = 22 ; 12 men ) and more than four risk factors and a subpopulation with more than five diseased coronary artery segments and zero risk factors ( n = 13 ; 12 men ) ( table 4 )  . 
as with the other subgroups , these two groups displayed coronarie indenni ( tabella 2 e 4 ) , 210 erano appartenevano alla 5a decade e 231 alla 6a decade ( maschi 196 , femmine 245 ) , e quelli con pi di 3 fattori di rischio erano il 4 , 2% ( 102 / 2432 ; maschi 42 , femmine 60 )  . 
dei pazienti con pi di 5 segmenti coronarici malati ( tabelle 3 e 4 ) , 115 erano nella 5a decade e 270 nella 6a decade ( maschi 309 , femmine 76 ) , e quelli con 0 - 1 fattori di rischio erano il 3 , 0% ( 73 / 2432 ; maschi 66 , femmine 7 )  . 
limitando ulteriormente il criterio di selezione abbiamo individuato : una popolazione di pazienti con coronarie indenni ( 22 ; 12 maschi ) e pi di 4 fattori di rischio ed una popolazione con pi di 5 segmenti coronarici malati e 0 fattori di rischio ( 13 ; 12 maschi ) ( tabella 4 )  . 
in questi due sottogruppi , come anche in quelli precedenti , si osservano significative differenze di et , distribuzione di genere , di prevalenza del dolore tipico , body mass index ( bmi ; p < 0 , 05 )  . 
the category other among the symptoms includes non - angina - like chest pain , dyspnoea , arrhythmias , high - risk asymptomatic patients population total healthy coronary arteries cad 5 segments cad , coronary artery disease ; sd , standard deviation ; acs , acute coronary syndrome ; bmi , body mass index ; hr , heart rate ; lvef , left ventricular ejection fraction ; rf , risk factors tabella 1 dati demografici . 
nei due sottogruppi con pi di 5 segmenti coronarici malati il fattore di rischio che rimane dominante risultato lipertensione ( 36% ) e la malattia coronarica risultata essere non ostruttiva nell11% ( 8 ) dei pazienti con 0 - 1 fattori di rischio e nell8% ( 1 ) dei pazienti con 0 fattori di rischio . discussione il valore prognostico della ctca stato dimostrato in alcu ni report preliminari ; in alcuni di questi si osservato co 222 radiol med ( 2012 ) 117 : 214229 residual population healthy coronary arteries cad 5 segments residual population healthy coronary arteries > 3rf cad 5 segments 0 - 1rf residual population cad 5 segments 0rf healthy coronary arteries > 4rf healthy coronary arteries cad 5 segments fig . 
in particular , the effect of stratification based on ctca morphological criteria alone ( a ) ; incremental effect of the number of risk factors on the width of the population of outliers with respect to the general reference population in their fifth and sixth decades ( b , c )  . 
in particolare , a mostra leffetto della sola stratificazione basata sul criterio morfologico ctca ; b e c mostrano leffetto incrementale del numero di fattori di rischio sullampiezza della popolazione degli outliers rispetto alla popolazione generale di riferimento nella 5a e 6a decade di et . 
la figura mostra la distribuzione relativa del genere nei due sottogruppi di outliers a coronarie indenni e con cad in pi di 5 segmenti coronarici nella 5a e 6a decade di et . 
cad , malattia coronarica ; m , maschi ; f , femmine . two subgroups with more than five diseased coronary artery segments was hypertension ( 36% ) ; cad was nonobstructive in 11% ( n = 8 ) of cases with zero to one risk factors and 8% ( n = 1 ) of patients with zero risk factors . me la tipologia prevalente di placca aterosclerotica co ronarica nel singolo paziente possa avere un valore prognostico incrementale rispetto ad altri fattori di rischio noti [ 3438 ]  . 
absolute distribution of gender in the subgroups of outliers with healthy coronary arteries and with cad 5 coronary artery segments according to the number of risk factors in the fifth and sixth decades . 
la figura mostra la distribuzione assoluta per maschi e femmine nei due sottogruppi di outliers a coronarie indenni e con cad in pi di 5 segmenti coronarici a seconda del numero di fattori di rischio nella 5a e 6a decade di et . 
some show how the prevalent typology of atherosclerotic coronary plaque in the individual patient can provide added prognostic value with respect to other known risk factors [ 3438 ]  . 
for individuals in whom the association between risk factors and the presence / severity of cad is in line with epidemiological expectations , the task of stratification is , for the most part , simplified . 
however , there is a certain portion of individuals in whom the characteristic association between risk factors and presence / severity of cad is discordant with epidemiological expectations [ 24 ]  . 
in the case of cad , these individuals are characterised by : ( 1 ) healthy coronary arteries and multiple risk factors ; ( 2 ) coronary arteries with advanced disease and no risk factors . 
the importance of these populations lies in their biological and tra fattori di rischio e presenza / severit della malattia coronarica conforme alle aspettative epidemiologiche il lavoro di stratificazione tutto sommato semplificato . 
tuttavia , esiste una quota di individui e pazienti nei quali le caratteristi che di associazione tra fattori di rischio e presenza / severit della malattia coronarica sono difformi da quelle attese su base epidemiologica [ 24 ]  . 
 lo studio e la mappatura di questi individui utilizzando 224 radiol med ( 2012 ) 117 : 214229 healthy coronary arteries m + f 50 - 59 males tot m + f 60 - 70 females tot cad 5 segments m + f 50 - 59 males tot m + f 60 - 70 females tot fig . 
la figura mostra la distribuzione relativa ( in percentuale ) degli outliers scomposti per genere , fasce di et , e numero di fdr nella 5a e 6a decade di et . 
it is in fact likely that these individuals are characterised by the presence of protective / antiprotective factors that influence the development of cad . the study and mapping of these individuals using ctca as a morphological tool could facilitate focused genetic studies , with the potential for identifying further targets for cad prevention . 
according to the width and asymmetry of the selection criteria , an outlier population of 7% ( 4% with healthy and 3% with diseased coronary arteries ) or 2% ( 1% with healthy and 1% with diseased coronary arteries ) can be identified equally distributed at the outer limits of the spectrum of cad . 
 a seconda dellampiezza e della asimmetricit dei criteri di selezione possibile evidenziare un 7% ( 4% con coronarie indenni e 3% con coronarie malate ) o un 2% ( 1% con coronarie indenni e 1% con coronarie malate ) di popolazione outliers equamente distribuite ai margini dello spettro della malattia coronarica . le due sottopopolazioni di outliers che abbiamo identificato differiscono per alcune caratteristiche macro - scopiche . 
questa osservazione pu essere spiegata con il fatto che : i primi sono mediamente pi giovani e quindi la malattia ha avuto meno radiol med ( 2012 ) 117 : 214229 table 3 patients with cad in more than five segments at ctca . 
la tabella mostra la distribuzione dei pazienti cad in pi di 5 segmenti per genere e fascia di et con la scomposizione per numero di fattori di rischio ( fdr )  . 
individuals in the second group are older and the effect of gender and age is more evident among men . as there are no other similar reports available in the literature , comparison of our study and method of analysis is difficult . 
further prospective studies targeted at implementing demographic data , morphological tempo per agire , indipendentemente dal numero di fattori di rischio ( le donne inoltre contano sulleffetto protettivo degli estrogeni fino alla menopausa ) ; i secondi invece , pi anziani , mostrano leffetto del genere e dellet pi evidente sul genere maschile . non esistono , attualmente , altri report in letteratura con i quali confrontare questa esperienza e questa modalit di analisi , ed pertanto difficoltoso dare un valore comparativo . 
ulteriori studi prospettici mirati allimplementazione del dato demografico , di quello morfologico , di quello bioumorale e genotipico , consentiranno di analizzare le differenze 226 radiol med ( 2012 ) 117 : 214229 table 4 characteristics of outlier subpopulations . 
 however , the introduction of new hardware and software able to provide adequate image quality using prospective triggering based on the ecg signal has brought dose values to < 5 msv [ 912 ]  . 
the population from which we selected our individuals is nonetheless very large , and it would not have been possible to obtain a stratification of outliers on a smaller population . 
tuttavia , lintroduzione di nuovi hardware e software in grado di fornire adeguata qualit di immagine utilizzando il triggering prospettico basato sul segnale elettrocardiografico ( ecg ) consentono di portare i valori di dose al di sotto dei 5 msv [ 912 ]  . 
further prospective studies will enable targeted evaluations of the biological state and genotype of individuals in these populations , with the aim of identifying protective / antiprotective factors with respect to cad . la ctca si dimostra uno strumento in grado di stratificare ed individuare popolazioni agli estremi dello spettro rispetto al rapporto tra presenza di malattia e numero di fattori rischio . 
our aim was to evaluate the evolution of 20 patients with h1n1 pneumonia , focusing our attention on patients with severe clinical and radiological findings who developed post - acute respiratory distress syndrome ( postards ) pulmonary fibrosis . 
twenty adult patients ( nine women and 11 men ; mean age 43.516.4 years ) with a diagnosis of h1n1 infection confirmed by pharyngeal swab came to our attention from september to november 2009 and were followed up until september 2010 . 
 twenty - five percent of patients ( 5 / 20 ) developed acute respiratory distress syndrome ( ards ) , which progressed to predominantly peripheral pulmonary fibrosis in 10% ( 2 / 20 ; one died and one had late - onset pulmonary fibrosis , documented on day 68 )  . 
venti pazienti adulti , di cui 9 donne e 11 uomini , con et media di 43 , 516 , 4 anni e con diagnosi di influenza suina h1n1 confermata mediante tampone faringeo sono giunti alla nostra osservazione tra settembre e novembre 2009 e sono stati valutati evolutivamente fino a settembre 2010 . 
tutti i pazienti , in considerazione della severit del quadro clinico , sono stati sottoposti a regime di ricovero ed hanno eseguito almeno una radiografia del torace ; 12 di essi hanno eseguito inoltre almeno una tomografia computerizzata ( tc ) del torace . 
nel restante 25% ( 5 / 20 ) , il ricovero stato gravato da complicanze respiratorie fino ad un quadro conclamato di ards , con evoluzione in interstiziopatia prevalentemente periferica in 2 pazienti , di cui uno poi deceduto ed uno con sviluppo tardivo di fibrosi polmonare documentata in 68a giornata . 
poich levoluzione in interstiziopatia 186 radiol med ( 2012 ) 117 : 185200 in these patients , fibrosis could present a different spatial distribution and a different temporal trend , with delayed late onset ; moreover , in one case , the signs of interstitial lung disease partially regressed over time . 
therefore , ct should be considered not only in the diagnostic stage , but also during the follow - up . keywords ards fibrosis ct h1n1 pneumonia polmonare dellards da h1n1 rappresenta una complicanza di non rara osservazione , il monitoraggio evolutivo dei pazienti con presentazioni cliniche particolarmente severe non pu esimersi dallimpiego dellindagine tc . 
il nostro studio ha documentato che la interstiziopatia conseguente alla polmonite virale con ards pu presentare non solo una distribuzione spaziale peculiare , ma anche un inconsueto andamento temporale , con insorgenza tardiva ; inoltre , in un singolo caso si documentata una parziale e graduale riduzione nel tempo dei segni di interstiziopatia . 
questa osservazione pu giustificare ulteriormente , limpiego della tc non solo in acuto ma soprattutto nel monitoraggio tardivo di questi pazienti . parole chiave ards fibrosi tc polmonite h1n1 introduction introduzione the influenza virus belongs to the orthomyxoviridae family and is responsible for pathological conditions that may develop following one of two patterns : endemic ( seasonal , type b influenza ) and pandemic ( occasional , type a influenza )  . 
these viruses were responsible for the major pandemics of the past century : the spanish flu ( 19181919 , the most serious , with a total of 2025 million deaths ) , the asian flu ( 19571958 ) and the hong kong flu ( 19681969 )  . 
on 11 june 2009 , the world health organization raised the pandemic level to 6 for the novel type a ( h1n1 ) influenza , also known as swine influenza virus due to its origin from the recombination of two viral strains of swine influenza circulating in eurasia and north america . 
this virus , which first appeared in mexico in april 2009 , spread rapidly throughout the world , renewing fears of a disease that had caused high mortality rates in the past [ 1 ]  . 
of note , however , was the fact that the population groups most vulnerable to infection and with the highest incidence of severe forms were children and young adults , as had happened during the 1918 pandemic . 
the low incidence of severe disease among the elderly may be explained by the presence of a sensitised immune system following exposure to the 1918 virus or related strains that circulated until 1957 [ 2 ]  . 
 complications due to either the direct action of the virus or to the development of superinfections may worsen the clinical picture , leading to acute respiratory distress syndrome ( ards ) , death , or permanent fibrotic sequelae [ 3 ]  . the purpose of this study was to evaluate the evolution of 20 patients with a definite diagnosis of h1n1 pneumonia , focusing our attention on those with a severe clinical and il virus dellinfluenza appartiene alla famiglia degli orthomyxoviridae ed responsabile di un quadro patologico che si pu estrinsecare seguendo due modelli : quello endemico ( stagionale , sostenuto dal gruppo b ) e quello pandemico ( ad incidenza occasionale , sostenuto dal gruppo a )  . 
si ricordino in proposito le grandi pandemie del secolo scorso : la spagnola ( 19181919 , la pi grave , con un numero di decessi complessivamente pari a 2025 milioni di persone ) , la asiatica ( 1957 - 1958 ) e la hong kong ( 19681969 )  . 
 l11 giugno del 2009 , lorganizzazione mondiale della sanit ha dichiarato il livello 6 di pandemia influenzale per un nuovo ceppo a , il virus h1n1 , noto anche come virus dellinfluenza suina perch nato dalla ricombinazione di due ceppi virali suini circolanti in eurasia e nel nordamerica . 
tale virus , comparso per la prima volta in messico nellaprile del 2009 , si rapidamente diffuso in tutto il mondo , risvegliando i timori per una patologia che in passato aveva determinato un alto tasso di mortalit [ 1 ]  . 
lattenzione stata per richiamata dal fatto che le categorie pi suscettibili allinfezione e in cui si registrata la maggior incidenza di forme severe siano stati bambini e giovani adulti , cos come accadde nella pandemia del 1918 . 
la bassa incidenza negli anziani pare sia da ricondurre proprio alla presenza di un sistema immunitario gi sensibilizzato in seguito allesposizione al virus nel 1918 o ai ceppi correlati circolanti fino al 1957 [ 2 ]  . 
le complicanze , dipendenti o dallazione diretta del virus o dallo sviluppo di superinfezioni , possono aggravare il radiol med ( 2012 ) 117 : 185200 radiological course progressing to interstitial disease and post - ards pulmonary fibrosis . materials and methods epidemiological data reveal that approximately 4 , 760 , 000 cases of h1n1 infection occurred in italy , just under 500 , 000 of which were in the emilia romagna region , leading to 228 deaths throughout italy [ 4 ]  . 
from september to november 2009 , 20 adult patients nine women and 11 men with a mean age of 43.516.4 years and a diagnosis of h1n1 swine flu confirmed by pharyngeal swab [ swine - flu a / h1 reverse transcriptase polymerase chain reaction ( rt - pcr ) ] , came to our observation . 
all 17 patients admitted to the ed were hospitalised , with patient outcome research team ( port ) iii - iv [ 5 ] classification ; seven required admission to the intensive care unit ( icu ) for assisted mechanical ventilation ( port class v ; tables 1 and 2 )  . 
consistent with the data reported in the literature [ 1 ] , all patients had nonspecific symptoms of influenza , namely : 88% had fever ( > 38c ) , 52% cough , 29% dyspnoea , 11% headache , 11% arthralgia and 11% gastrointestinal symptoms . 
ct scans were performed on a 6or 16 - slice siemens ct scanner ( somatom sensation cardiac 16 , forchheim , germany ) with the volumetric technique , no contrast enhancement , and thin - slice reconstructions . 
the images obtained were independently reviewed with specific window settings for the pulmonary parenchyma and mediastinum by two specialised physicians and two radiology trainers to obtain a final diagnostic interpretation . 
abnormalities of parenchymal density at baseline ( areas of ground - glass opacity , consolidation with or without air bronchogram , mixed patterns such as consolidation associated with ground - glass attenuation ) , their distribution ( unilateral , bilateral ) , location and extent ( upper lobes , lower lobes , hilar - perihilar region , subpleural region , diffuse ) ; 2 . 
presence of hilarmediastinal lymph nodes with shortaxis diameter > 1 cm ; quadro clinico fino allacute respiratory distress syndrome ( ards ) , al decesso del paziente o allo sviluppo di sequele permanenti di tipo fibrotico [ 3 ]  . 
 scopo del presente lavoro stato quello di effettuare una valutazione evolutiva in 20 pazienti con diagnosi di certezza di polmonite da h1n1 , focalizzando la nostra attenzione sui casi clinici con decorso clinico - radiologico severo , complicatosi con evoluzione in quadri di interstiziopatia e di fibrosi polmonare post - ards . 
 materiali e metodi i dati epidemiologici rilevano che in italia si sono verificati circa 4760000 di casi di infezione , delle quali poco meno di cinquecentomila in emilia - romagna , con un totale di decessi pari a 228 in tutta italia [ 4 ]  . 
i pazienti sono stati arruolati nel nostro studio in seguito ad accesso diretto tramite pronto soccorso o perch gi ricoverati per altri quadri patologici ( nello specifico : 17 afferenti dal pronto soccorso , 2 oncologici e 1 donna gravida ricoverata per il parto ) e presentavano tutti un quadro clinico - laboratoristico tale da richiedere un approfondimento con radiogramma e / o tomografia computerizzata ( tc ) polmonare . 
la totalit dei pazienti presentava , in linea con la letteratura [ 1 ] , sintomi influenzali aspecifici , in particolare : iperpiressia ( > 38 ) nel 88% , tosse nel 52% , dispnea nel 29% , cefalea 11% , artralgie 11% e disturbi gastrointestinali nel 11% . 
le indagini tc sono state invece eseguite su tc siemens 6 strati o tc siemens 16 strati ( somatom sensation cardiac 16 , forchheim , germania ) con tecnica volumetrica , senza somministrazione di mezzo di contrasto ( mdc ) e ricostruzioni a strato sottile . 
le immagini radiologiche , ottenute utilizzando specifiche finestre per il parenchima polmonare e per il mediastino , sono state quindi esaminate indipendentemente da due medici specialisti in radiodiagnostica e da due medici in formazione in radiodiagnostica , ottenendo una interpretazione diagnostica finale . 
le differenze sono state risolte per con188 radiol med ( 2012 ) 117 : 185200 table 1 patient outcome research team ( port ) : scores ; subdivision into different risk classes based on score [ 5 ] patient features score age in yrs age in yrs 10 + 10 demographic factors age men women personal care facility resident comorbid illnesses tumours liver failure congestive heart failure cerebrovascular disease renal failure physical findings altered mentation tachypnoea ( > 30 breaths / min ) systolic pressure < 90 mmhg body temperature < 35c or > 40c pulse rate > 125 beats per minute laboratory and radiographic findings blood ph ( arterial ) < 7.25 serum urea nitrogen ( bun ) > 30 mg / d sodium < 130 meq / l blood sugar > 250 mg / dl anaemia ( hematocrit < 30% ) partial pressure of oxygen in arterial blood < 60 mmhg pleural effusion fattori demografici et sesso maschile sesso femminile residente in una casa protetta comorbilit neoplasie insufficienza epatica scompenso cardiaco congestizio patologia cerebro - vascolare insufficienza renale reperti obiettivi stato mentale alterato frequenza respiratoria > 30 atti / minuto pressione sistolica < 90 mmhg temperatura < 35c o > 40c polso > 125 bpm reperti strumentali ph arterioso < 7 , 25 azotemia > 30 mg / dl na < 130 meq / l glucosio > 250 mg / dl ematocrito < 60% pao 2 < 60 mmhg versamento pleurico + 30 + 20 + 10 + 10 + 10 + 20 + 20 + 20 + 15 + 10 + 30 + 20 + 20 + 10 + 10 + 10 + 10 tabella 1 port ( patient outcome research team ) : assegnazione dei punteggi [ 5 ] caratteristiche del paziente punteggio anni di et anni di et - 10 bpm , battiti per minuto ; pao2 , pressione parziale arteriosa di ossigeno senso . 
alterazioni della densit basale parenchimale ( aree di opacit a vetro smerigliato , ground - glass ; addensamenti consolidativi con o senza broncogramma aereo ; quadri misti : consolidazioni associate a ground - glass ) , loro distribuzione ( monolaterale ; bilaterale ) , localizzazione ed estensione ( lobi superiori ; lobi inferiori , sede ilo - perilare ; mantellare , diffusa ) ; 2 . 
segni di interstiziopatia polmonare e di fibrosi ( distorsione dellarchitettura parenchimale , reticoli , ispessimenti settali ed interlobari , bronchiectasie da trazione )  . risultati nel 45% dei pazienti ( 9 / 20 ) il primo radiogramma del torace non ha mostrato lesioni pleuro - parenchimali ; nei rimanenti casi ( 65% , 11 / 20 ) , invece , il reperto pi frequente stato il riscontro di addensamenti consolidativi bilaterali ( 64% , 7 / 11 ) , prevalentemente localizzati nelle regioni polmonari basali ( 36% , 4 / 11 )  . 
reperti di pi rara osservazione sono stati : affastellamento dei reperi broncovasali in sede bibasale ( 9% , 1 / 11 ) , strie radiopache parenchimali al terzo medio del campo polmonare di destra ( 9% , 1 / 11 ) e addensamento polmonare singolo a distribuzione parailare ( 18% , 2 / 20 )  . 
signs of interstitial lung disease and fibrosis ( architectural distortion , reticular opacities , septal and interlobar thickening , traction bronchiectasis )  . in 45% of patients ( 9 / 20 ) , the first radiograph showed no pleuroparenchymal lesions ; in the remaining cases ( 65% , 11 / 20 ) , the most frequent finding was bilateral consolidation ( 64% , 7 / 11 ) , with predominant location in the basal lung areas ( 36% , 4 / 11 )  . 
less frequent findings included thickening of bronchovascular bundles at both lung bases ( 9% , 1 / 11 ) , radiopaque parenchymal striae at the middle third of the right lung field ( 9% , 1 / 11 ) and a single lung consolidation with parahilar distribution ( 18% , 2 / 20 )  . 
of the nine patients with normal radiograph , three underwent lung ct without contrast enhancement on account of their clinical condition and low oxygen saturation ; ct scans confirmed the negative radiological finding in one case only . overall , lung ct was performed in 60% of patients ( 12 / 20 ) , with the following results : bilateral and peripheral ground - glass attenuation , in particular at the time of symptom onset , in 25% of patients ( 3 / 20 ) ; concurrent areas of consolidation and ground - glass attenuation , in some cases with air bronchogram , in 25% ( 3 / 20 ) ; areas of parenchymal consolidation in 42% ( 5 / 20 ) ; mostly moderate pleural effusion in 17% ( 2 / 20 ) ; pericardial effusion in 17% ( 2 / 20 ) leading to cardiac tamponade in one case only ; hilarmediastinal lymph nodes with short - axis diameter > 1 cm in 33% ( 4 / 20 ) ; pneumothorax in 17% ( 2 / 20 )  . 
no patient showed sign of pulmonary fibrosis at onset . all patients clinical course showed regression of parenchymal symptoms and abnormalities after treatment ( osellargo spettro / guidata dallantibiogramma ) , in assenza di significativi esiti parenchimali . 
nel restante 25% ( 5 / 20 ) , il ricovero stato gravato da complicanze respiratorie , fino ad un quadro conclamato di ards , con evoluzione fibrotica in 2 / 20 , di cui un paziente deceduto . 
si segnala infine un caso ( 5% ) che present evoluzione con un quadro compatibile con fibrosi polmonare e che tuttavia , nei controlli tc a distanza , si progressivamente ridotta fino alla pressoch completa risoluzione ( tabella 3 )  . 
 riportiamo di seguito una succinta descrizione del decorso clinico dei pazienti che hanno sviluppato una fibrosi polmonare post - ards e del paziente in cui un processo apparentemente simile andato incontro ad una graduale regressione . caso 1 paziente maschio di anni 33 , senza comorbilit ad eccezione di una condizione di sovrappeso ( body mass index [ bmi ] : 29 , 5 ) e di una dislipidemia mista , si present in pronto soccorso per iperpiressia ( 39 ) ed insufficienza respiratoria acuta ( spo2 : 89% )  . 
il primo radiogramma standard e lo studio tc torace eseguiti allingresso , dimostravano la presenza di multiple consolidazioni parenchimali bilaterali , pi evidenti ai lobi inferiori , in assenza di segni di versamento pleurico o di scompenso emodinamico . 
nonostante la severit del quadro clinico , il paziente ebbe una progressiva , lenta risposta alle terapie ( antivirale ed antibiotica a largo spettro ) , con progressiva stabilizzazione dei parametri vitali fino al raggiungimento graduale della autonomia respiratoria , sia pure con prove di funzionalit indicative di severo deficit restrittivo ed un quadro parenchimale riferibile ad evoluzione fibrotica di ards . 
il paziente venne dimesso , dopo 95 giorni di degenza , con una diagnosi di sindrome ipocinetica e polineuropatia da malattia critica , in esiti di insufficienza respiratoria acuta da focolai broncopneumonici multipli da virus h1n1 . 
in the remaining 25% of cases ( 5 / 20 ) , hospital stay was characterised by respiratory complications , including full - blown ards with fibrotic evolution in 2 / 20 cases , one of which lead to the patients death . 
the first standard radiograph and chest ct performed on admission showed multiple bilateral consolidation areas , more evident at the lower lobes , with no sign of pleural effusion or haemodynamic compromise . 
despite the severity of the symptoms , the patient showed progressive , slow response to antiviral and broad - spectrum antibiotics , with gradual stabilisation of vital signs until progressive return to breathing air , even though the function tests indicated severe restrictive defects and the parenchymal pattern suggested fibrotic ards . 
the patient was discharged on day 95 with a diagnosis of hypokinetic syndrome and critical - illness polyneuropathy , with acute respiratory failure due to multiple foci of bronchopneumonia secondary to h1n1 virus . 
 case 2 a 39 - year - old man with no concomitant disease was admitted to the ed with fever ( 39.7c ) and acute respiratory failure ( spo2 = 88% ) which prompted icu admission with intubation and placement of a tracheostomy tube to provide mechanical ventilation . 
i radiogrammi standard successivi dimostravano un ulteriore incremento dimensionale delle aree consolidative , comparsa di minimo versamento pleurico bibasale , di enfisema sottocutaneo , di pneumocollo , pneumomediastino e di falde di pneumotorace bilaterali , in parte saccate , che hanno richiesto il posizionamento di tubi di drenaggio . 
nelle fasi successive del ricovero , caratterizzate da sovrainfezioni da aspergillus ed enterobacter , da persistenza dei pneumotorace bilaterale anche in presenza dei drenaggi e da comparsa di necrosi della mucosa tracheale , si constatava unassenza di risposta alle terapie con severa , rapida compromissione del quadro respiratorio . 
lassenza di controlli tc intermedi non consente di datare con certezza il viraggio dalla fase proliferativa ( radiologicamente caratterizzata da consolidazioni parenchimali ) alla fase fibrotica ( radiologicamente iniziale fibrosi parenchimale ) dellards . 
al 113 giorno infine sopraggiunto il decesso del paziente per stato settico con conferma del quadro radiologico anche allindagine autoptica che documentava la presenza di una broncopolmonite bilaterale , necrotizzante ed ad impronta emorragica , con caverne ascessuali multiple , in polmoni a struttura sovvertita per la presenza di una polmonite interstiziale fibrotica e segni di laringotracheite ulcerativo - emorragica . caso 3 paziente maschio , di anni 52 , senza comorbilit al momento del ricovero ad eccezione di una condizione di sovrappeso ( bmi non specificato in cartella clinica ) , giunse alla nostra osservazione per dispnea ed iperpiressia ( 39 , 5 ) refrattaria a terapia con levofloxacina e paracetamolo . 
si procedette quindi al ricovero nel reparto di terapia intensiva respiratoria dove il paziente venne sottoposto a ventilazione in c - pap con o2 al 100% , in considerazione della radiol med ( 2012 ) 117 : 185200 192 radiol med ( 2012 ) 117 : 185200 radiol med ( 2012 ) 117 : 185200 fig . 
a la tomografia computerizzata ad alta risoluzione ( hrct ) a 15 giorni dallesordio , evidenzia la presenza di multiple consolidazioni parenchimali , minimo versamento pleurico bibasale , pneumotorace bilaterale persistente anche dopo posizionamento di drenaggi , in assenza di segni di fibrosi parenchimale . 
b il controllo hrct a 68 giorni evidenzia la comparsa di iniziali segni di fibrosi polmonare caratterizzati da ispessimento reticolare dellinterstizio e bronchiectasie da trazione , a distribuzione tipicamente periferica . solidation , with no signs of haemodynamic compromise or pleural effusion . 
further standard radiographs showed enlargement of the consolidation areas , presence of a small bi - basal pleural effusion , subcutaneous emphysema , pneumoneck , pneumomediastinum and bilateral pneumothorax , partially saccular , which required insertion of drainage catheters . 
during the hospital stay , characterised by aspergillus and enterobacter superinfection , by persistent bilateral pneumothorax despite the drainage catheters , and by necrosis of the tracheal mucosa , the patient showed no response to treatment , with severe , rapid compromise of the respiratory pattern . 
 the absence of intermediate ct scans does not allow us to clearly date the change from the proliferative phase ( radiologically characterised by parenchymal consolidation ) to the fibrotic phase ( radiologically indicated by initial parenchymal fibrosis ) of ards . 
on day 113 , the patient died from sepsis ; autopsy findings confirmed the radiological diagnosis , showing the presence of bilateral , necrotising , haemorrhagic bronchopneumonia , with multiple abscess cavities within a subverted lung structure due to fibrotic interstitial pneumonia , as well as signs of ulcerative - haemorrhagic laryngotracheitis . grave ipossiemia evidenziata allemogas - analisi arteriosa e venne trattato con somministrazione di tazocin e terapia antivirale . 
b lhrct dopo 60 giorni mostra aree consolidative , enfisema sottocutaneo , pneumocollo e pneumotorace ; si associano diffusi segni di fibrosi polmonare , con ispessimento di tipo reticolare dellinterstizio e bronchiectasie da trazione . case 3 discussione a 52 - year - old man with no concurrent disease on admission except for being overweight ( bmi not recorded on the clinical chart ) presented with dyspnoea and fever ( 39.5c ) refractory to treatment with levofloxacin and paracetamol . 
 the patient was admitted to the respiratory icu where he received continuous positive airway pressure ( cpap ) ventilation with 100% oxygen ( o2 ) due to severe hypoxaemia detected at arterial blood gas analysis , and he was treated by tazocin ( piperacillin / tazobactam ) and antiviral therapy . 
il pi comune pattern allora descritto fu quello delle opacit a chiazze ; tuttavia molti autori convennero sulla non specificit del quadro radiologico e soprattutto sulla difficolt di differenziazione con altre patologie ad elevata incidenza , prima tra tutte , la tubercolosi [ 6 ]  . 
 fondamentale quindi per la diagnostica per immagini , oggi come in passato , non solo il corretto inquadramento diagnostico dei pazienti con influenza da h1n1 , ma anche il monitoraggio evolutivo delle possibili complicanze . 
il miglioramento tecnologico , ma soprattutto la nascita e lo sviluppo dellindagine tc , rendono ragione dellimportanza che tale metodica assume come strumento fondamentale da integrare con i parametri clinici e laboratoristici per lidentificazione , la gestione ed il follow - up dei pazienti con forme severe . 
b la hrct ripetuta a 15 giorni mostra riduzione di estensione e di densit delle consolidazioni parenchimali con comparsa di aspetti compatibili in prima ipotesi con segni di evoluzione fibrotica prevalentemente periferici , con reticoli e bronchiectasie cilindriche parzialmente ripiene di secreti . 
c il controllo a 71 giorni mostra la completa regressione delle residue aree consolidative con persistenza di ground - glass periferico bilateralmente ed aspetti reticolari esclusivamente ai lobi inferiori dorsalmente ; notevolmente ridotti gli aspetti bronchiettasici . 
d il controllo dopo 120 giorni documenta la pressoch completa risoluzione dei reticoli e delle bronchiectasie , residuando esclusivamente delle aree di ground - glass in sede basale perifericamente . discussion diagnostic imaging has contributed to the management of patients with influenza a virus infection since 1918 ; as a consequence of world war i , the american army and many community hospitals were supplied with radiological devices , and this made possible the first large - scale studies during the outbreak of the pandemic infection [ 5 ]  . 
the most common pattern described at that time was patchy lung opacities ; however , several authors agreed on the nonspecificity of the pattern and the difficulty differentiating the condition from other particularly common diseases , such as tuberculosis [ 6 ]  . 
it was only with the 1957 pandemic that the radiological findings were classified , with the identification of four different syndromic patterns : in particolare , la nostra attenzione si soffermata sulla valutazione diagnostico - evolutiva di quei pazienti che hanno presentato lo sviluppo di complicanze durante il regime di ricovero . 
la letteratura sottolinea come , tra le condizioni predisponenti allo sviluppo di complicanze , oltre ai classici fattori di rischio , comuni allinfluenza endemica ( patologie cardiovascolari , patologie polmonari , turbe neurologiche , immunodepressione , insufficienza renale o epatica cronica ) , vadano tenuti in considerazione anche obesit e gravidanza [ 2 , 8 ]  . 
i meccanismi che si associano allo sviluppo di complicanze possono essere legati allazione diretta del virus ( in genere un danno alveolare diffuso dad ) , allinsorgenza di superinfezioni batteriche / fungine o a danni iatrogeni e possono determinare un 196 chest x - ray ; 1 . 
viral and bacterial co - infection [ 7 ]  . therefore , today as in the past , the fundamental goals of diagnostic imaging are not only to provide accurate diagnostic interpretation of patients with h1n1 influenza but also to monitor the evolution of possible complications over time . 
 technological advances , and in particular , the introduction and development of ct imaging , account for the importance of ct as an essential tool to be integrated with clinical and laboratory data for detection , management and follow - up of patients with severe forms of disease . 
previous studies have reported on the need to consider obesity and pregnancy among the risk factors for complications , in addition to the typical risk factors of endemic influenza ( cardiovascular disease , lung disease , neurological disorders , immunodeficiency , chronic renal or liver failure ) [ 2 , 8 ]  . 
the mechanisms associated with the development of complications may be related to the direct action of the virus ( typically diffuse alveolar damage ; dad ) and the onset of bacterial / fungal superinfections or iatrogenic injury , which may lead to worsening clinical condition and eventually death or irreversible damage , such as post - ards fibrosis . 
the pathogenesis of membrane damage is complex and related to both the release of inflammatory cytokines [ interleukin ( il ) - 1 , tumour necrosis factor ( tnf ) , granulocyte - macrophage colony - stimulating factory ( gm - csf ) , il - 8 , leukotriene b4 ( ltb4 ) ] and the aberrant immune response mediated by the cd8 t and b lymphocytes [ 9 ]  . 
proliferative phase ( 27 days ) : in response to the noxious stimulus , connective tissue and other structural elements accumulate in the lung , which appears richly cellular at microscopy . 
 furthermore , in this phase , in cases of ards secondradiol med ( 2012 ) 117 : 185200 peggioramento clinico fino al decesso del paziente o allo sviluppo di danni irreversibili , quale la fibrosi post - ards . 
 la ards , o sindrome da distress respiratorio delladulto , si caratterizza per una grave insufficienza respiratoria , refrattaria allossigenoterapia e consegue ad edema polmonare da aumentata permeabilit della barriera alveolo - capillare . 
la patogenesi del danno di membrana complessa ed legata sia al rilascio di citochine infiammatorie ( interleuchina [ il ] 1 , tumor necrosis factor [ tnf ] , granulocytemacrophage colony stimulating factor [ gm - csf ] , il8 , leucotriene [ lt ] b4 ) , sia allaberrante risposta immunitaria mediata dai linfociti t cd8 e dai linfociti b [ 9 ] , e determina un quadro anatomopatologico - radiologico caratteristico , in cui si distinguono tre fasi ormai ben conosciute che si susseguono nel tempo [ 1015 ]  . 
fase proliferativa ( da 2 a 7 giorni ) : in risposta allo stimolo nocivo , il tessuto connettivo ed altri elementi strutturali si depositano nel polmone , che alla microscopia appare densamente cellulare . 
 inoltre , in questa fase , in caso di ards conseguente a polmonite , di frequente riscontro lenfisema polmonare interstiziale , in particolare nei pazienti con ards sottoposti a continua ventilazione a pressione positiva . 
la tc documenta raccolte di aria nellinterstizio adiacenti alle vene polmonari ed ai vasi linfatici , molto prima della radiografia del torace o cisti aeree fino a 5 mm di diametro a sede subpleurica o perilare . 
levoluzione fibrosante associata ad una prognosi peggiore e la precoce presenza di procollagene iii nel lavaggio bronco - alveolare ( bal ) associata a quadri pi severi e ad aumentato rischio di morte . 
il danno polmonare si correla ad un deficit respiratorio di tipo restrittivo e si caratterizza per radiol med ( 2012 ) 117 : 185200 ary to pneumonia , interstitial pulmonary emphysema is frequently seen , particularly in patients with ards receiving cpap . 
ct demonstrates air collections within the interstitium adjacent to the pulmonary veins and lymph vessels before these become apparent on chest radiography , or air cysts 5 mm in diameter in the subpleural or perihilar regions . 
fibrotic evolution is associated with a worse prognosis , and the early presence of procollagen iii in bronchoalveolar lavage ( bal ) fluid is associated with more severe disease and an increased risk of death . 
later abnormalities include signs of fibrosis , mainly in the anterior lung portions , which testifies to the protective effect of the parenchymal consolidations against the mechanical damage induced by ventilation . 
hypoventilated areas of subtotal atelectasia , appearing as ground - glass areas on ct , are re - ventilated more rapidly with positive - pressure mechanical ventilation compared with areas of completely atelectatic or nonventilated areas , which appear on ct as areas of consolidation . 
several studies on ards patients undergoing zeroand positive - pressure ventilation have demonstrated that alveolar re - ventilation is obtained by increasing ventilation pressure along a craniocaudal and ventrodorsal axis . 
therefore , basal and dorsal areas are ventilated last at the expense of overdistention of the ventral and cranial portions , leading to an increased risk of barotraumavolutrauma and fibrotic evolution in these areas [ 1016 ]  . despite our small patient series , analysis of our experience allows some considerations to be made . 
in the patient who died and underwent autopsy , some of the most common patterns were observed ( dad , necrotising and haemorrhagic bronchopneumonia , necrosis of the airway mucosa , pneumothorax ) ; conversely , the presence of thromboembolism and pulmonary infarction was not detected [ 2729 ]  . 
the additional information provided by our study , even though with the limitations of a small patient series , concerns the possible evolution of h1n1 infection into pulmonary fibrosis ( 10% of patients , 2 / 20 ) , characterised by signs that differ in part from those of post - ards fibrosis due to other causes . 
alterazioni pi tardive sono i segni di fibrosi prevalenti nelle porzioni anteriori del polmone , a dimostrazione delleffetto protettivo esercitato dalle consolidazioni parenchimali nei confronti del danno meccanico da ventilazione . 
 stato dimostrato che zone di atelettasia subtotale , ipoventilate , che si presentano come ground - glass alla tc , sono riventilate pi velocemente dalla ventilazione meccanica a pressioni positive rispetto a quelle di atelettasia completa o non ventilate , che alla tc sono rappresentate da aree di consolidazione . 
numerosi studi su pazienti con ards sottoposti a ventilazione a pressione zero e positiva hanno dimostrato che la riventilazione alveolare si verifica aumentando la pressione di ventilazione lungo un asse cranio - caudale e ventro - dorsale . 
pertanto , le aree basali e dorsali sono ventilate per ultime a spese della sovradistensione delle porzioni ventrali e craniali , con aumentato rischio di barotraumivolutraumi e di evoluzione in fibrosi in tali sedi [ 1016 ]  . nonostante la limitata casistica , lanalisi della nostra esperienza consente di fare alcune considerazioni . 
nel paziente deceduto ed in cui stata eseguita lindagine autoptica , si sono documentati alcuni dei pattern pi frequentemente descritti ( danno alveolare diffuso , broncopolmonite necrotizzante e ad impronta emorragica , necrosi della mucosa delle vie aeree , pneumotorace ) ; non stata invece documentata la presenza di tromboembolia e di infarto polmonare [ 2729 ]  . 
le informazioni aggiuntive fornite da questo studio , pur con i limiti legati al ridotto numero di pazienti , riguardano la possibile evoluzione in fibrosi polmonare dellinfezione da h1n1 ( nella nostra casistica , 10% dei pazienti : 2 / 20 ) , con caratteristiche in parte differenti rispetto alla fibrosi post - ards da altre cause . 
su due pazienti , almeno in un caso ( caso 1 ) , abbiamo avuto la dimostrazione che la comparsa dei segni di fibrosi stata pi tardiva e si evidenziata non prima del 68 giorno dallinsorgenza dellards . 
la consapevolezza della non occasionale evoluzione fibrotica , anche tardiva , deve indurre il radiologo ad un attento monitoraggio e giustifica limpiego della tc toracica nel follow - up , anche se la tempistica dei controlli non ben definita . 
in at least one ( case 1 ) of two cases , we confirmed that the appearance of the signs of fibrosis was delayed , with no sign being detected before day 68 after ards onset . 
 awareness of the nonoccasional , possibly delayed , fibrotic evolution must suggest careful radiological monitoring and justifies the use of follow - up chest ct , despite there being no clear definition as to the best timing of follow - up studies . 
in fact , even in the case of nonspecific interstitial pneumonia ( nsip ) , reticular opacities and bronchiectases may regress after treatment , demonstrating that in the absence of honeycombing , the ct diagnosis of interstitial fibrosis may not correspond to pathology findings . 
in these cases , it may be assumed that potentially reversible bronchiectasis could be induced by peribronchial atelectasia rather than by fibrotic traction [ 30 , 31 ]  . conclusions although h1n1 influenza has a benign clinical course in the majority of cases , a proportion of patients , particularly young individuals , may develop complications . 
in our experience , the most severe cases were complicated by superinfections , necrosis of the tracheal mucosa and bilateral pneumothorax and especially by the development of post - ards fibrosis ( 10% of cases ; 2 / 20 ) , with ventral but also posterior - segment distribution . 
a few days later , we observed the appearance of bilateral , mainly bi - basal , parenchymal consolidations , some with air bronchogram and frequently with associated pneumothorax , often bilaterally . 
in one case only could we demonstrate that the appearance of initial signs of fibrosis occurred > 2 months after hospital admission , much later than reported in the literature for the fibrotic evolution of ards / dad . 
this type of fibrosis differs from post - ards fibrosis from other causes due to its spatial and temporal distribution . we also describe a case in which signs suggestive of fibrosis on ct performed on day 15 progressively regressed glass , forse attribuibile ad un quota di fibrosi microscopica a sede prevalentemente basale e periferica . 
questa osservazione giustifica ulteriormente limpiego della tc per definire levolutivit dei quadri radiologici in pazienti con ards da h1n1 e non sorprendente , basti pensare che anche nel caso della polmonite interstiziale non specifica ( nsip ) , opacit reticolari e bronchiectasie possono regredire dopo terapia , a dimostrazione che , in assenza di honeycombing ( polmone ad alveare ) la diagnosi tc di fibrosi interstiziale pu non corrispondere alla realt anatomo - patologica . 
in questi casi si suppone che le bronchiectasie potenzialmente reversibili non siano dovute a trazione fibrotica ma ad atelettasia peribronchiale [ 30 , 31 ]  . conclusioni sebbene linfluenza da h1n1 abbia un decorso benigno nella maggior parte dei casi , esiste una percentuale di pazienti , specie in et giovanile , che possono presentare lo sviluppo di complicanze . 
qualora si sospetti questo tipo di evoluzione , la tc del torace si dimostra uno strumento fondamentale , sia nella esatta definizione dellestensione del danno parenchimale , sia nel monitoraggio evolutivo . 
nella nostra esperienza , i casi pi severi sono stati complicati da comparsa di sovrainfezioni , necrosi della mucosa tracheale e pneumotorace bilaterale ma , soprattutto , dallinstaurarsi di un quadro di fibrosi post - ards ( 10% dei casi , 2 / 20 ) , con distribuzione non solo ventrale ma anche ai segmenti polmonari posteriori . 
in questi pazienti lo studio tc ha evidenziato , nelle fasi iniziali , ground - glass localizzato ad entrambi i campi polmonari e a distribuzione prevalentemente periferica , in assenza di versamento pleurico . 
 dopo alcuni giorni , abbiamo osservato la comparsa di addensamenti consolidativi parenchimali bilaterali , specie in sede bibasale , in parte con broncogramma aereo e frequente comparsa di pneumotorace , spesso bilaterale . 
in un singolo caso abbiamo potuto documentare con certezza che lesordio degli iniziali segni di fibrosi polmonare si verificato dopo oltre 2 mesi dal ricovero , quindi molto pi tardivamente di quanto riportato nella letteratura per levoluzione fibrotica dellards / dad . 
per le sue caratteristiche di distribuzione spaziale e temporale , tale fibrosi potrebbe presentarsi con aspetti differenti rispetto alla fibrosi post - ards da altre cause . abbiamo inoltre descritto un caso in cui i segni suggestivi per fibrosi , documentati in tc al 15 giorno , sono progressivamente regrediti fino allisolato riscontro , a 4 mesi , di opacit ground - glass prevalentemente basali , a distriradiol med ( 2012 ) 117 : 185200 to the point that the only finding at 4 - months follow - up was predominantly basal ground - glass opacities with peripheral distribution . 
therefore , as the evolution of postviral ards ( in our case related to h1n1 virus ) into pulmonary fibrosis does not represent an infrequent complication , follow - up monitoring of patients with extremely severe clinical symptoms must include ct examination . 
although our patient population was limited , our study proved that this type of fibrosis may be unusual both in spatial distribution and temporal trend ( late onset )  . 
pertanto , poich levoluzione in fibrosi polmonare dellards ad eziologia virale ( nella nostra casistica , da h1n1 ) rappresenta una complicanza di non rara osservazione , il monitoraggio evolutivo dei pazienti con presentazioni cliniche particolarmente severe non pu esimersi dallimpiego dellindagine tc . 
nonostante la casistica sia limitata , il nostro studio ha dimostrato che tale fibrosi pu presentare non solo una distribuzione spaziale peculiare , ma anche un inconsueto andamento temporale con insorgenza tardiva . 
we prospectively analysed 4 , 018 outpatient requests , the appropriateness of which was assessed using an evaluation foreconomic analysis was based on costs listed in the italian national health services ( nhs ) national tariff as established by the ministerial decree of 22 july 1996 . 
scopo del nostro lavoro stato verificare lappropriatezza delle richieste di esami di diagnostica per immagini non inserite in programmi di follow - up e quanto i precedenti radiologici influiscano sulla specificit delle richieste e sullappropriatezza , valutare il loro riscontro diagnostico , registrare limpatto economico degli esami inappropriati . 
nellanalisi economica sono stati valutate le tariffe previste dal nomenclatore per il sistema sanitario nazionale ( ssn ) determinato dal decreto ministeriale ( dm ) del 22 / 07 / 1996 . 
 la presenza di precedenti indagini ha influenzato lappropriatezza delle richieste ( p < 0 , 001 ) e la conferma della diagnosi ( p < 0 , 001 )  . 
abbiamo documentato una appropriatezza prescrittiva del 56% e come una richiesta appropriata associata alla presenza di un quesito specifico comporti una percentuale significativamente elevata di conferme dellipotesi diagnostica , calcolando inoltre il rilevante impatto sul piano finanziario delle richieste inappropriate . parole chiave appropriatezza economia sanitaria studi socioeconomici radiol med ( 2012 ) 117 : 322332 introduction introduzione health care costs are steadily increasing in the western world , and many national organisations have developed measures to reduce theguidelines , diagnostic algorithms and appropriateness criteria have been established , sometimes causing confusion as far as terminology and purpose are concerned [ 1 ]  . 
in this respect , the italian national agency for regional health services produced in 2004 a text titled guidelines for diagnostic imaging in line with the guidelines applied by other member states of the european union and canada , focusing the attention on three key issues : investigation appropriateness , radiation protection and expenditure containment [ 2 ]  . 
this document states that a prescription for a radiological examination should include a diagnostic hypothesis so that the radiologist can choose the best possible technique or procedure for that particular case . 
 many studies have evaluated the applicability and effects of the guidelines on clinical practice , and numerous strategies have been suggested to improve adherence : informing the referring physicians of the costs incurred in connection with inappropriate requests [ 3 ] , sending copies of the guidelines to referring physicians [ 4 ] , setting up training courses for referring physicians [ 5 ] , obliging referring physicians to consult a radiology specialist before an examination is requested [ 6 , 7 ] and evaluating requests using a computerised pre - authorisation system [ 8 , 9 ]  . 
 the objectives of our study were to assess the appropriateness of requests and the influence of previous radiological procedures on request specificity and appropriateness , to evaluate diagnostic outcomes and to record the economic impact of inappropriate examinations . 
this decision was made because there are no definite guidelines related to radiological follow - up programmes and because requests for serial examinations should by definition be considered appropriate . materials and methods we prospectively analysed 4 , 018 consecutive outpatient requests referred to our diagnostic imaging department in 2008 . 
the requests for diagnostic imaging examinations were distributed as follows : computed tomography ( ct ) ( n = 581 ) , magnetic resonance imaging ( mri ) ( n = 577 ) and ultrasound ( us ) ( n = 2 , 860 )  . 
the appropriateness of the requests was assessed using an evaluation form to record the following information : i costi dellassistenza sanitaria nel mondo occidentale sono in continuo aumento e numerose organizzazioni nazionali hanno sviluppato accorgimenti tesi alla loro riduzione , sono state infatti redatte linee guida , algoritmi diagnostici e criteri di appropriatezza , talvolta generando confusione di terminologia e scopi [ 1 ]  . 
in questottica , lagenzia nazionale per i servizi sanitari regionali ( anssr ) ha elaborato nel 2004 un testo di linee guida in diagnostica per immagini in accordo con le linee guida dellunione europea , canadesi ed inglesi , concentrando la propria attenzione su tre aspetti fondamentali : lappropriatezza delle indagini , la radioprotezione ed il contenimento della spesa [ 2 ]  . 
in tale documento sottolineato come la richiesta di prestazione radiologica debba esplicitare lipotesi diagnostica , in modo tale che il radiologo possa scegliere la tecnica o il procedimento migliore possibile per quel caso specifico . 
molti studi hanno valutato lapplicabilit e gli effetti delle linee guida sulla pratica clinica e le strategie suggerite per migliorare laderenza alle linee guida sono state molteplici : informare i medici richiedenti sullaggravio di costi causato dalle loro richieste improprie [ 3 ] , spedire copie delle linee guida ai medici richiedenti [ 4 ] , istituire dei corsi per i medici richiedenti [ 5 ] , obbligare i medici richiedenti a un consulto radiologico prima di effettuare le richieste [ 6 , 7 ] , valutare con un sistema informatico di preautorizzazione le richieste [ 8 , 9 ]  . 
nel 2008 la regione lazio , ha avviato un progetto di monitoraggio , sensibilizzazione e formazione per migliorare lappropriatezza prescrittiva [ 10 ]  . il nostro studio , inserito in questo contesto , ha avuto come obiettivo quello di verificare lappropriatezza delle richieste e quanto i precedenti radiologici influiscano sulla specificit delle richieste e sullappropriatezza , valutare il riscontro diagnostico , ed infine di registrare limpatto economico degli esami inappropriati . 
abbiamo operato questa selezione in quanto non esistono definite linee guida sui programmi di monitoraggio , ritenendo inoltre che le richieste di controlli seriati dovrebbero essere considerate appropriate per definizione . materiali e metodi abbiamo analizzato prospetticamente 4018 richieste ambulatoriali consecutive afferite al nostro servizio nellanno 2008 , cosi suddivise : 581 tomografie computerizzate ( tc ) , 577 risonanze magnetiche ( rm ) e 2860 ecografie . 
in cases where the prescription did not provide a diagnostic hypothesis or was nonspecific , the radiologist collected the patients medical history to establish whether the examination should be considered appropriate or inappropriate . 
si tratta di indagini complesse o costose che vengono eseguite , di norma , unicamente su richiesta da parte di medici che dispongono dellesperienza clinica atta a valutare i risultati dellindagine e ad agire di conseguenza . 
gli esami di questo gruppo sono quelli nei quali manca la base logica allesecuzione dellindagine . nellanalisi economica sono stati valutate le tariffe previste dal nomenclatore per il sistema sanitario nazionale ( ssn ) determinato dal decreto ministeriale ( dm ) del 22 / 07 / 1996 [ 11 ] ; i fatturati sono stati successivamente aggregati per metodica . 
per studiare lassociazione di alcune caratteristiche delle richieste desame con la probabilit dellappropriatezza e con quella della conferma della diagnosi sono stati utilizzati modelli di regressione logistica univariata e multivariata . results risultati of the 4 , 018 prescriptions analysed , 71% ( 2 , 846 / 4 , 018 ) were issued by general practitioners and 29% ( 1 , 172 / 4 , 018 ) delle 4018 prescrizioni esaminate , i medici di medicina geradiol med ( 2012 ) 117 : 322332 by medical specialists ( 1 , 172 / 4 , 018 ) ( p < 0.001 ) ; 1 , 715 ( 43% ) requests were included in a follow - up protocol , whereas 2 , 303 ( 57% ) were not . 
in total , 63% ( 1 , 087 / 1 , 715 ) of prescriptions included in a follow - up protocol were issued by general practitioners , and 76% ( 1 , 308 / 1 , 715 ) were related to conditions previously investigated by diagnostic imaging . 
in total , 76% ( 1 , 715 / 2 , 303 ) of requests not included in a follow - up protocol were made by general practitioners , and 37% ( 863 / 2 , 303 ) presented previous diagnostic imaging examination results . 
of prescriptions not included in a follow - up protocol , the diagnostic problem was specified n 47% ( 1 , 086 / 2 , 303 ) , and 53% ( 1 , 217 / 2 , 303 ) did not specify the clinical problem [ no diagnostic hypothesis in 61% ( 741 / 1 , 217 ) and nonspecific diagnostic hypothesis in 39% ( 426 / 1 , 217 ) ]  . 
in these cases , the radiologist responsible for the investigation would collect the clinical data needed to evaluate appropriateness ( table 1 )  . of the 2 , 303 requests , 55.5% ( 1 , 280 / 2 , 303 ) were appropriate , 16% ( 375 / 2 , 303 ) were not indicated initially , 6% ( 130 / 2 , 303 ) were not indicated routinely and 22% ( 518 / 2 , 303 ) were not indicated . 
the proportion of appropriate requests was not significantly different when comparing prescriptions issued by general practitioners to those issued by medical specialists : 55% ( 963 / 1 , 759 ) and 58% ( 317 / 544 ) , respectively . 
characteristics of the 2 , 303 requests not related to a follow - up protocol are summarised in table 2 . examinations considered not indicated were not performed immediately , and in particular , ct due to the radiation protection rules and mri due to the high economic costs involved . 
in these cases , after evaluating the patients clinical presentation and medical history , the radiologist responsible for the examination would contact the referring physician directly or through the patient to obtain appropriate explanation and suggestions useful for a possible reevaluation and subsequent examination . 
millesettecentoquindici ( 43% ) erano inserite in un protocollo di follow - up , mentre 2303 richieste ( 57% ) non erano inserite in un protocollo di follow - up . 
il 63% ( 1087 / 1715 ) delle richieste in follow - up sono state effettuate dai medici di medicina generale e il 76% ( 1308 / 1715 ) avevano eseguito precedenti esami di diagnostica per immagini . 
il 76% ( 1715 / 2303 ) delle richieste non in follow - up sono state effettuate dai medici di medicina generale e il 37% ( 863 / 2303 ) delle richieste non in follow - up era accompagnato da precedenti esami di diagnostica per immagini . 
nel 53% ( 1217 / 2303 ) dei casi la richiesta non in follow - up non era corredata da inquadramenti o quesiti clinici specifici [ quesito assente 61% ( 741 / 1217 ) e quesito aspecifico 39% ( 426 / 1217 ) ] , in questi casi stato il radiologo responsabile dello studio a raccogliere i dati clinico / anamnestici indispensabili per la valutazione dellappropriatezza ( tabella 1 )  . delle 2303 richieste il 55 , 5% ( 1280 / 2303 ) sono risultate appropriate , il 16% ( 375 / 2303 ) inizialmente non indicate , il 6% ( 130 / 2303 ) non indicate di routine , il 22% ( 518 / 2303 ) non indicate . 
la proporzione di richieste appropriate non risultata significativamente differente paragonando i medici di medicina generale con i medici specialisti , rispettivamente 55% ( 963 / 1759 ) e 58% ( 317 / 544 )  . 
le caratteristiche delle 2303 richieste non in follow - up sono riassunte nella tabella 2 . gli esami considerati non indicati non sono stati immediatamente eseguiti , in particolare quelli relativi a tc , in considerazione delle norme protezionistiche , e a rm , per gli elevati costi economici . 
in questi casi il radiologo responsabile dellesame , dopo aver valutato caso per caso i dati clinico anamnestici , ha proceduto a contattare il prescrittore , direttamente o tramite il paziente , per gli opportuni chiarimenti e suggerimenti , riservandosi di rivalutare il caso per un eventuale reinserimento tra i candidati ad indagine di diagnostica per immagini . 
nel 65% ( 561 / 863 ) degli esami appropriati erano disponibili precedenti indagini di diagnostica per immagini , mentre nel 50% degli esami appropriati queste non erano disponibili ( 719 / 1440 ) ( p < 0 , 001 )  . 
la presenza di precedenti indagini ha significativamente influenzato anche quella delle richieste con conferma della diagnosi , portandola dal 40% ( 472 / 1181 ) al 63% ( 381 / 604 ) ( p < 0 , 001 )  . 
the medical doctor is viewed positively by the patient because he or she prescribes a wide range of investigations , and the nhs is ready to deliver a high volume of supposedly necessary services in order to request additional financing . 
in this context , it is understandable that medical doctors who try to introduce virtuous practices aimed at limiting inappropriate services end up being penalised compared with those who indiscriminately continue to satisfy the request for further services . discussione la richiesta di prestazioni di diagnostica per immagini , in particolare per le indagini ad alta tecnologia , in aumento esponenziale perch questultimo tipo di studi identificato , anche erroneamente , come risolutivo di un percorso diagnostico o come irrinunciabile a fini difensivistici . 
article 3 lays down the basic principle related to the justification for radiation : before exposing a person to ionising radiation , the direct benefits to his / her health should be compared with the damage that exposure might cause . 
it is the responsibility of both the referring physician and the radiologist who receives the request to avoid unnecessary radiation exposure , and the radiologist may consider alternative techniques that pursue the same diagnostic objective . 
after establishing guidelines , many studies were conducted on their applicability and effectiveness , especially in relation to the knowledge of their existence and use by the referring physicians , yielding rather conflicting results . 
 [ 14 ] reported that a low percentage of radiologists had used the criteria of appropriateness issued by the american college of radiology ( acr ) , whereas wolfe et al . 
showed that the guidelines may predispose physicians to consider changing their behaviour , but they concluded that unless incentives or disincentives are introduced , it is unlikely that the guidelines , because of their complexity , will lead to a change in clinical practice [ 16 ]  . 
in questo contesto si capisce come chi metta in atto pratiche virtuose , tese a limitare le prestazioni inappropriate , sia in realt penalizzato rispetto a chi procede indiscriminatamente ad esaudire la domanda di prestazioni . in italia , gi per il solo aspetto radioprotezionistico , il decreto legislativo 187 / 2000 , nel definire i principi generali della radioprotezione per quanto riguarda le esposizioni mediche , allart . 
3 fissa il principio basilare della giustificazione , secondo cui per esporre una persona alle radiazioni ionizzanti si deve tener conto dei benefici diretti alla salute in rapporto ai danni che lesposizione potrebbe causare . 
sia il clinico prescrivente che il radiologo , cui la richiesta di esame afferisce , hanno la responsabilit di evitare esposizioni non necessarie , il radiologo eventualmente valutando tecniche alternative che perseguano lo stesso obiettivo diagnostico . 
dopo listituzione di linee guida , molti studi sono stati condotti sulla loro applicabilit ed efficacia , soprattutto sulla loro conoscenza ed utilizzo da parte dei medici , con risultati piuttosto discordanti . 
 [ 14 ] hanno evidenziato che la percentuale di radiologi che dichiaravano di avere utilizzato i criteri dappropriatezza dellamerican college of radiology ( acr ) era bassa , mentre wolfe et al . 
 [ 15 ] hanno rilevato che la maggior parte dei medici dei famiglia americani dichiarava di avere una buona conoscenza delle linee guida e di ritenerle utili nello svolgimento delle loro attivit . 
 [ 16 ] hanno documentato che le linee guida possono predisporre i medici a pensare di modificare i loro comportamenti , ma concludono che , a meno di interventi incentivi o disincentivi , improbabile che le linee guida , a causa della loro complessit , producano un cambiamento nella pratica clinica . 
 [ 18 ] hanno documentato rispettivamente che 330 radiol med ( 2012 ) 117 : 322332 propriateness of 1 , 000 outpatient requests for conventional radiology , us , ct and mri received by a department of radiology . 
 [ 21 ] found that 73.4% of 500 radiological examinations ( ct and us ) were appropriate . other studies have evaluated the effectiveness of organisational tools aimed at improving the applicability of the guidelines but with discrepant results [ 710 , 22 ]  . 
obliging the referring physicians to consult a radiology specialist before the examination is requested [ 7 ] , and evaluating the requests using a computerised preauthorisation system [ 8 ] seems to have significantly reduced the number of inappropriate examinations . 
 centers for medicare and medicaid services ( cms ) have authorised a us $10 million dollar study to create a computer system to support requests for diagnostic imaging examinations based on acr guidelines [ 9 ]  . 
in this context , and as the first of its kind , our study analysed only the requests for examinations that were not part of a follow - up programme . 
in our study , 56% ( 1 , 280 / 2 , 303 ) of requests were considered appropriate according to the guidelines issued by the italian national agency for regional health services . 
in this group , 69% ( 711 / 1 , 023 ) of requests were provided with a specific diagnostic hypothesis . a division by diagnostic methods shows that mri reached the highest percentage of appropriateness ( 72% ) , followed by ct ( 51.5% ) and then us ( 38% )  . 
us was also , in terms of statistical significance ( p < 0.001 ) , the technique most burdened by inappropriate requests , and in 27% ( 355 / 1304 ) of cases , it was classified as not indicated according to regional guidelines . 
however , the economic analysis revealed that the cost of examinations not considered appropriate because of being classified as not indicated initially or not indicated routinely was distributed almost equally between the three methods . 
 [ 21 ] su 500 esami radiologici ( tc ed ecografia ) ha riscontrato unappropriatezza del 73 , 4% . ulteriori studi hanno valutato lefficacia di strumenti organizzativi atti a migliorare lapplicabilit delle linee guide con risultati discrepanti [ 710 , 22 ]  . 
solo obbligare i medici richiedenti ad un consulto radiologico prima di effettuare le richieste [ 7 ] e valutare con un sistema informatico di preautorizzazione le richieste [ 8 ] sembrano aver ottenuto lo scopo di ridurre sensibilmente leffettuazione desami inappropriati , anche se lefficacia della preautorizzazione informatizzata attualmente dibattuta dai maggiori esperti americani [ 22 ] e lus centers for medicare and medicaid services ( cms ) ha indetto un progetto di studio di 10 milioni di dollari per la creazione di un sistema informatico di supporto per la prescrizione degli esami radiologici basato su linee guida dellacr [ 9 ]  . 
il nostro studio , inserito in tale contesto , ha riguardato esclusivamente , primo nel suo genere , le richieste di esami eseguiti non in corso di follow - up . 
abbiamo operato questa selezione in quanto non solo non esistono definite linee guida sui programmi di monitoraggio , ma le richieste di controlli seriati dovrebbero essere considerate appropriate per definizione . 
 distinguendo tra le metodiche , la rm ha presentato la percentuale pi alta di appropriatezza ( 72% ) , seguita dalla tc ( 51 , 5% ) e dallecografia ( 38% )  . 
lecografia ha rappresentato la tecnica pi gravata , anche in termini di significativit statistica ( p < 0 , 001 ) , da richieste inappropriate e in particolare , sempre alla luce delle linee guida dellanssr , non indicate , che si sono attestate al 27% ( 355 / 1304 )  . 
comunque , dallanalisi economica emerge come i costi relativi agli esami considerabili non appropriati perch inizialmente non indicati o non indicati routine siano quasi divisi equamente tra le tre metodiche . 
 radiol med ( 2012 ) 117 : 322332 sis confirmed that the correct orientation of the clinician and the use of an appropriate method contributed to a confirmed diagnostic hypothesis . 
there was a statistically significant difference between the number of requests confirming the disease compared to the type of examination ( p < 0.001 ) , with mri reaching 72% . 
this finding confirms that the more sophisticated methods are generally used as second - line examinations , which play a role in solving a specific diagnostic problem , whereas us is often used as a screening tool . 
the overall economic analysis shows that 36.5% of fees paid by the nhs , distributed more or less equally across the three methods , were related to inappropriate tests . conclusions this study evidenced the large number of inappropriate outpatient requests ( 44% ) received by the department of radiology at our institution and the economic impact of these requests . 
it also shows that an appropriate examination and prescriptions provided with a specific indication of the condition for which the examination is being prescribed led to a significantly higher rate of diagnostic hypothesis confirmation . 
 the use of human and technological resources depends on political and managerial decisions , and it still has to be decided what could or should be the radiologists role as evaluators of prescriptions in order to ensure that diagnostic imaging departments perform only appropriate examinations . 
this would lead to significant improvements not only in terms of radiological performance but also shorter waiting lists and consequent health advantages , as appropriate examinations would run less risk of being performed too late . abbiamo inoltre valutato il riscontro diagnostico che ha concluso la performance radiologica , confermando che il corretto orientamento del clinico e lutilizzo della metodica appropriata concorrono alla conferma dellipotesi diagnostica . 
statisticamente significativa ( p < 0 , 001 ) risultata la differenza nella proporzione di richieste con conferma della patologia rispetto al tipo di esame , con la rm che raggiunge il 72% . 
tale dato conferma che le metodiche pi sofisticate sono generalmente utilizzate come metodica di seconda istanza e giocano un ruolo di problem solving , mentre lecografia spesso utilizzata come metodica di screening . 
lanalisi economica globale evidenzia come il 36 , 5% del fatturato a carico del ssn , cui contribuiscono sostanzialmente in parti eguali tutte le metodiche , sia riconducibile a esami non appropriati . 
 conclusioni il nostro lavoro ha documentato come un elevato numero di richieste ambulatoriali inappropriate ( 44% ) siano afferite al servizio di diagnostica per immagini del nostro istituto e quale stato limpatto economico che tali richieste hanno avuto sul piano finanziario . 
department of internal and public medicine , section of radiology , university of bari medical school , piazza giulio cesare 11 , 70124 bari , italy correspondence to : a.a. 
transverse images and multiplanar reconstructions ( mpr ) were retrospectively examined by two blinded expert radiologists in order to assess t and n parameters , and the results were compared with histological findings . 
il tipo di mezzo di contrasto endoluminale non sembra influenzare la definizione del parametro n . radiol med ( 2012 ) 117 : 254267 keywords colosigmoideal cancer staging mdct colonography computed tomography parole chiave carcinoma del colon - sigma stadiazione tcmd colonografia tomografia computerizzata introduction introduzione colosigmoideal cancer represents one of the leading causes of death related to cancer in industrialised countries and patients prognosis depends on the stage of the disease at the time of diagnosis [ 1 ]  . 
in the choice of therapeutic strategy , preoperative staging is essential and can be obtained by using different tools , such as ultrasound ( us ) , computed tomography ( ct ) and magnetic resonance ( mr ) imaging , which are able to evaluate t ( depth of wall invasion , peritumoural fat tissue infiltration or invasion of adjacent organs ) and m ( presence of distant metastases ) parameters with different accuracy values [ 2 ]  . 
ct is the most commonly used imaging tool for staging colosigmoideal carcinoma , with reported accuracy values varying between 48% and 84% , probably in relation to the technique used , the patients studied and the ct device [ 37 ]  . 
the aim of this study was to assess the diagnostic accuracy of multidetector - row ct ( mdct ) colonography in the preoperative local staging of colosigmoideal cancer by using water or air for colonic distension . 
 materials and methods patients between april 2006 and june 2009 , 70 consecutive patients ( 43 men and 27 women aged 4079 years , mean age 56.3 years ) with endoscopically and histologically proven colosigmoideal cancer underwent mdct examination . 
 all tumours were adenocarcinomas : well - differentiated ( n = 39 ) , moderately differentiated ( n = 14 ) and poorly differentiated ( n = 17 )  . 
fifty patients ( 25 of whom underwent water ct and 25 air ct colonography ) underwent intestinal preparation 24 h before ct examination by ingesting 4 l of water solution containing 280 g of polyethylene glycol ( selg - esse , promefarm srl , sigmar italy srl ) associated il carcinoma del colon - sigma rappresenta una delle principali cause di morte per cancro nei paesi industrializzati e la prognosi dei pazienti dipende dallo stadio di malattia al momento della diagnosi [ 1 ]  . 
i progressi della tecnica chirurgica ed in particolare lintroduzione di procedure chirurgiche mini - invasive hanno determinato un significativo miglioramento del decorso post - operatorio ed una riduzione dei rischi nei pazienti anziani . 
nella scelta della strategia terapeutica , la stadiazione pre - operatoria fondamentale e pu essere realizzata mediante differenti metodiche , come la ecografia ( us ) , la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm ) , in grado di valutare i parametri t ( profondit di invasione parietale , infiltrazione del tessuto adiposo peritumorale o invasione di organi adiacenti ) ed m ( presenza di metastasi a distanza ) con differenti valori di accuratezza [ 2 ]  . 
la tc rappresenta la modalit di imaging maggiormente utilizzata per la stadiazione del carcinoma del colon - sigma , con valori di accuratezza riportati tra 48% e 84% , probabilmente in base alla tecnica impiegata , al gruppo di pazienti esaminato ed al tipo di apparecchiatura utilizzata [ 37 ]  . 
scopo di questo studio valutare laccuratezza diagnostica della colonografia ottenuta con tc multidetettore ( tcmd ) nella stadiazione pre - operatoria locale del carcinoma del colon - sigma , utilizzando lacqua o laria per la distensione colica . 
 materiali e metodi pazienti nel periodo compreso tra aprile 2006 e giugno 2009 , 70 pazienti consecutivi ( 43 uomini e 27 donne , di et compresa tra 40 e 79 anni , et media 56 , 3 ) , con diagnosi endoscopica ed istologica accertata di carcinoma del colon - sigma , sono stati sottoposti ad esame tcmd . 
the remaining 20 patients ( ten of whom underwent water ct and ten air ct colonography ) did not undergo intestinal preparation so we could compare the accuracy of the two staging techniques when residual faecal material was present . 
patients were informed of the study design and signed an institutional review - board - approved consent form on which the procedure and study were explained . ct protocol immediately before the ct examination , a 12 - f balloontipped rectal tube was inserted in all cases . 
through this , 1 , 0001 , 500 ml of water was infused in 35 patients ( supine position ) and room air was manually and gently insufflated to maximum patient tolerance in the remaining 35 patients ( lateral position )  . 
in the group of patients who underwent air ct colonography , the rectal tube was removed 5 min after the end of the procedure in order to reduce abdominal bloating and discomfort . 
ten minutes before data acquisition , 20 mg of scopolaminen - butylbromide ( buscopan , boehringer ingelhein , tokyo , japan ) was injected intramuscularly to reduce colonic wall spas in all cases , a 16 - slice mdct device ( tsx - 101a aquilion 16 , toshiba medical system , tokyo , japan ) was used with the following parameters : slice thickness 1 mm ; increment 0.8 mm ; pitch 1.75 ; rotation time 0.5 s ; 120 / 250 kvp / mas . 
ct data were acquired from the pubic symphysis to the lung apices after intravenous injection of iodinated contrast material ( iomeron 400 , bracco , milan , italy ) into a cubital vein using a 16to 18 - gauge needle and an automatic injector ( mk - iv , medrad , pittsburgh , pa , usa ) at a dose of 1.5 ml / kg body weight and an injection rate of 3.5 ml / s , with a 50to 60 - s start delay . 
 image analysis ct transverse and mpr images were retrospectively evaluated by two independent , blinded abdominal radiologists ( ga , aasi ) with more than 10 years experience in abdominal ct and image reconstruction software . 
 cinquanta pazienti ( 25 dei quali sottoposti a colonografia tc con acqua e 25 a colonografia tc con aria ) sono stati sottoposti a preparazione intestinale 24 ore prima della esecuzione dellesame tc , mediante ingestione di 4 l di soluzione acquosa contenente 280 g di polietilene glicole ( selg - esse , promefarm srl , sigmar italia srl , italia ) ed associazione di dieta liquida . 
i restanti 20 pazienti ( 10 dei quali sottoposti a colonografia tc con acqua e 10 a colonografia tc con aria ) non hanno eseguito alcuna preparazione intestinale , al fine di confrontare laccuratezza delle due tecniche di stadiazione anche in caso di residui fecali . 
 i pazienti sono stati informati del disegno dello studio ed hanno sottoscritto un modulo di consenso scritto informato , approvato dal comitato etico locale , che riportava la descrizione della procedura e dello studio . protocollo tc immediatamente prima dellesame tc , in tutti i casi stata posizionata una sonda rettale da 12 f dotata di un palloncino alla estremit . 
in 35 pazienti , in decubito supino , sono stati introdotti 10001500 ml di acqua ; nei restanti 35 casi , in posizione laterale , si proceduto ad una insufflazione manuale e delicata di aria , fino alla massima tolleranza dei pazienti , ed stato eseguito uno scanogramma tc standard al fine di valutare il grado di distensione gassosa del colon . 
nel gruppo di pazienti sottoposti a colonografia tc con aria , la sonda rettale stata rimossa 5 minuti dopo il termine della procedura , per detendere le anse coliche e ridurre il gonfiore addominale ed il disagio dei pazienti . 
dieci minuti prima dellacquisizione dei dati , sono stati iniettati per via intramuscolare 20 mg di scopolamina - n - butilbromuro ( buscopan , boehringer ingelhein , tokyo , giappone ) , al fine di ridurre lo spasmo parietale del colon . 
in tutti i casi , stata utilizzata una apparecchiatura tcmd a 16 strati ( tsx101aaquilion 16 , toshiba medical system , tokyo , giappone ) , con i seguenti parametri : spessore di strato 1 mm ; incremento 0 , 8 mm ; pitch 1 , 75 ; tempo di rotazione 0 , 5 s ; 120 / 250 kvp / mas . 
i dati tc sono stati acquisiti dalla sinfisi pubica agli apici polmonari , dopo iniezione endovenosa di mezzo di contrasto iodato ( iomeron 400 , bracco , milano , italia ) in una vena cubitale , mediante ago da 1618 g ed iniettore automatico ( mk - iv , medrad , pittsburgh , pa ) , ad una dose di 1 , 5 ml / kg di peso corporeo e velocit di infusione di 3 , 5 ml / s , con ritardo di scansione pari a 5060 s . 
 radiol med ( 2012 ) 117 : 254267 degree of colonic wall distension by water or air , rated as insufficient ( collapsed or not sufficiently distended walls ) , good ( distended walls ) and optimal ( excellent distension with visualisation of all colonic segments ) ; degree of colonic wall enhancement after water or air distension , rated as poor , moderate or high based on tomodensitometric features ; intestinal cleansing , classified as insufficient ( evidence of residual faecal material in three or more colonic segments ) , good ( evidence of residual faecal material in only one colonic segment ) and optimal ( absence of residual faecal material ) ; presence , number and site of neoplastic lesions ( sigmoid , descending colon , transverse colon , ascending colon , caecum ) ; colosigmoideal wall thickness and density at the lesion site thickness was considered pathological when > 5 mm [ 8 ] ; peritumoural fat tissue morphology , classified as normal or pathological in the absence or presence of linear strands , respectively ; presence and location of lymphadenopathy , considered pathological regardless of diameter , number and densitometric features . mdct staging was performed following criteria described in the literature [ 9 ] and shown in table 1 . 
as reported by other authors [ 8 , 10 ] , t1 and t2 cancers were considered the same stage because they are difficult to distinguish from each other on ct imaging . 
in view of the aims of this study , the presence of distant metastases was not conanalisi delle immagini le scansioni assiali e le ricostruzioni mpr sono state valutate retrospettivamente ed in cieco da due radiologi addominali indipendenti ( ga , aasi ) , con pi di 10 anni di esperienza in campo di tc addominale e software di ricostruzione di immagini . 
i lettori sapevano che tutti i pazienti erano affetti da carcinoma del colon - sigma , ma non conoscevano i risultati endoscopici , la sede , le dimensioni e le caratteristiche morfologiche delle lesioni . 
ct staging obtained by water and air colonography was then compared with histological staging based on the tnm classification as approved by the american joint committee on cancer ( ajcc ) and the international union against cancer [ 11 , 12 ]  . statistical analysis sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and diagnostic accuracy for both ct techniques were calculated . 
differences in accuracy for t and n staging were assessed using the mcnemar test , with a two - tailed probability ( p ) value < 0.05 considered to indicate a statistically significant difference . 
lo spessore stato considerato patologico quando maggiore di 5 mm [ 8 ] ; morfologia del tessuto adiposo peritumorale , differenziato in normale o patologico , rispettivamente in assenza o in presenza di strie dense contestuali ; presenza e sede di linfoadenopatie , considerate patologiche indipendentemente da diametro , numero e caratteristiche densitometriche . la stadiazione tcmd stata eseguita sulla base dei criteri descritti in letteratura [ 9 ] e mostrati anche nella tabella 1 . 
come gi riportato da altri autori [ 8 , 10 ] , le forme t1 e t2 sono state considerate nello stesso stadio di malattia poich difficili da differenziare sulla base dellimaging tc . 
la stadiazione tc ottenuta mediante colonografia con acqua e con aria stata successivamente confrontata con la stadiazione istologica eseguita secondo la classificazione tumore - nodulometastasi ( tnm ) approvata dallamerican joint commettee on cancer ( ajcc ) e dalla international union against cancer [ 11 , 12 ]  . results water and air mdct colonography allowed the cancer to be detected in all cases . 
table 2 displays the results obtained in the radiological staging of the 70 patients studied by water and air colonography with regard to lesion site and morphodensitometric features , peritumoural fat tissue morphology , presence of lymphadenopathies , grade of colonic distension and intestinal cleansing . 
overstaging occurred in 4 / 35 ( 11.4% ) patients : ct examination detected peritumoural fat tissue invasion ( t3 ) in two cases , which was then excluded at histology ( t1 / t2 ) ; in the remaining two cases , ct detected invasion of the peritoneum and adjacent organs ( t4 ) , which was later excluded at histology ( t3 )  . 
in n parameter evaluaanalisi statistica sono stati calcolati i valori di sensibilit , specificit , valore predittivo positivo ( vpp ) , valore predittivo negativo ( vpn ) ed accuratezza diagnostica per entrambe le metodiche tc . 
 le differenze in termini di accuratezza per la stadiazione dei parametri t ed n sono state valutate utilizzando il test di mcnemar , considerando statisticamente significativo un valore di probabilit ( p ) a due code inferiore a 0 , 05 . 
al fine di valutare laccordo inter - osservatore tra i due lettori e la riproducibilit diagnostica della metodica , stato applicato il test di kappa ( k ) di cohen . 
un valore di k superiore a 0 , 81 stato considerato indicativo di accordo quasi perfetto , mentre valori di 0 , 610 , 80 e 0 , 410 , 60 hanno rappresento rispettivamente un accordo sostanziale o moderato . 
i risultati ottenuti nella stadiazione radiologica dei 70 pazienti studiati mediante colonografia con acqua e con aria , con riferimento a sede e caratteristiche morfo - densitometriche delle lesioni , morfologia del tessuto adiposo peritumorale , presenza di linfoadenopatie , grado di distensione colica e pulizia intestinale , sono riportati nella tabella 2 . 
 in fact , five n1 cancers were understaged to n0 and two n2 cancers were understaged to n1 because water mdct colonography failed to visualise small perilesional and distant lymphadenopathies , respectively . 
one n0 cancer was overstaged to n1 because small perilesional lymph nodes colonografia con acqua la stadiazione mediante colonografia tcmd con acqua risultata corretta in 24 / 35 pazienti , con accuratezza complessiva pari a 68 , 6% . 
dal confronto con la stadiazione istologica , la valutazione del parametro t risultata corretta in 31 / 35 casi , con un valore di accuratezza pari a 88 , 6% . 
over ( 11 , 4% ) pazienti , si sono verificati errori di sovrastadiazione : lesame tc ha identificato una infiltrazione del tessuto adiposo peritumorale ( t3 ) in 2 casi , successivamente esclusa al controllo istologico ( t1 / t2 ) ; nei restanti 2 casi , allesame tc stata diagnosticata una invasione peritoneale e di organi adiacenti ( t4 ) , esclusa al successivo controllo istologico ( t3 )  . 
nella valutazione del parametro n , la colonografia tcmd con acqua non ha identificato alcuna linfadenopatia peritumorale ( n0 ) in 13 / 35 pazienti ( 37 , 1% )  . 
dal confronto con i reperti istologici , la stadiazione mediante colonografia tcmd con acqua risultata corretta radiol med ( 2012 ) 117 : 254267 table 3 multidetector - row computed tomography ( mdct ) staging compared with histopathological results for water and air ct colonography mdct t1 / t2 tcmd t1 / t2 histology water ct colonography t1 / t2 istologia colonografia con acqua t1 / t2 air ct colonography t1 / t2 t1 / t2 colonografia con aria t , tumor ; n , node tabella 3 stadiazione tcmd confrontata con i reperti istopatologici per colonografia mediante acqua e aria t , tumore ; n , nodulo staging occurred in 5 / 35 ( 14.3% ) patients : ct examination detected peritumoural fat tissue invasion ( t3 ) in two cases , which was later excluded at histological examination ( t1 / t2 ) ; in the remaining three patients , ct detected invasion of adjacent organs ( t4 ) , later excluded by histological examination ( t3 )  . 
understaging occurred in 2 / 35 ( 5.71% ) cases because air ct colonography failed to detect an outer colonic surface irregularity ( t2 ) , which was found to be a t3 cancer at histological examination because of invasion of the peritumoural fat tissue . 
in fact , five n1 cancers were understaged to n0 and four n2 cancers to n1 because air mdct colonography failed to detect small perilesional and distant lymphadenopathies , respectively . 
infatti , 5 forme n1 sono state sottostadiate a n0 e 2 forme n2 a n1 , in quanto la colonografia tcmd con acqua non ha consentito il riconoscimento di piccole linfoadenopatie , rispettivamente peritumorali ed a distanza . 
una forma n0 stata sovrastadiata a n1 poich piccoli linfonodi perilesionali identificati alla colonografia tc sono risultati di tipo reattivo al controllo istologico . colonografia con aria la stadiazione mediante colonografia tcmd con aria risultata corretta in 22 / 35 pazienti , con accuratezza complessiva pari a 62 , 8% . 
in entrambi i casi , la lesione neoplastica ( frecce ) risulta limitata alla parete intestinale . sensitivity , specificity , ppv , npv and diagnostic accuracy values for water and air mdct colonography are reported in table 4 . 
 despite the significant accuracy of water colonography for studying early t stages of disease , no significant difference between the two techniques was found in the evaluation of the n parameter . 
 discussion accurate preoperative staging of colosigmoideal cancer is radiol med ( 2012 ) 117 : 254267 la valutazione del parametro t risultata corretta in 28 / 35 casi , con un valore di accuratezza pari al 80% . 
in 5 ( 14 , 3% ) pazienti si sono verificati errori di sovrastadiazione : lesame tc ha identificato una infiltrazione del tessuto adiposo peritumorale ( t3 ) in 2 casi , successivamente esclusa al controllo istologico ( t1 / t2 ) ; nei restanti 3 pazienti , allesame tc stata diagnosticata una invasione di organi adiacenti ( t4 ) , esclusa al successivo controllo istologico ( t3 )  . 
in 2 ( 5 , 71% ) casi si sono verificati errori di sottostadiazione poich la colonografia tc con aria non ha consentito la identificazione di una irregolarit della superficie esterna della parete colica ( t2 ) , risultata essere una forma t3 al controllo istologico , a causa della infiltrazione del tessuto adiposo peritumorale . 
 nella valutazione del parametro n , la colonografia tcmd con aria non ha identificato alcuna linfadenopatia peritumorale ( n0 ) in 17 / 35 ( 48 , 6% ) pazienti . 
dal confronto con i reperti istologici , la stadiazione mediante colonografia tc con aria risultata corretta in 26 / 35 pazienti , con un valore di accuratezza diagnostica pari a 74 , 3% per il parametro n . 
infatti , 5 forme n1 sono state sottostadiate a n0 e 4 forme n2 a n1 , in quanto la colonografia tcmd con aria non ha consentito il riconoscimento di piccole linfodenopatie , rispettivamente perilesionali ed a distanza . i valori di sensibilit , specificit , vpp , vpn ed accuratezza diagnostica per la colonografia tcmd con acqua e con aria sono riportati nella tabella 4 . 
il valore di accuratezza della colonografia con acqua ha mostrato un significativo incremento nella stadiazione delle forme t1 / 2 e t3 rispetto alla colonografia con aria ( p < 0 , 05 )  . 
nonostante la accuratezza significativa della colonografia con acqua per lo studio degli stadi t precoci di malattia , nella valutazione del parametro n non stata riscontrata alcuna differenza significativa tra le due tecniche tc . 
 stato riscontrato un accordo quasi perfetto tra i due lettori ( k = 0 , 83 )  . discussione una stadiazione pre - operatoria accurata del carcinoma del colon - sigma fondamentale per la pianificazione di una terapia ottimale e potrebbe influenzare il tasso di sopravvivenza e la qualit di vita [ 8 ]  . 
infatti , le neoplasie limitate alla tonaca sottomucosa potrebbero essere trattate con resezione colica per via laparoscopica , mentre in caso di tumori allo stadio t3 - t4 sono spesso necessari un approccio laparotomico e trattamenti neoadiuvanti chemioterapici e radioterapici [ 13 , 14 ]  . 
in fact , tumours limited to the submucosal layer could be treated by laparoscopic colonic resection , whereas t3 - t4 tumours often require a laparotomic approach and neoadjuvant chemoand radiotherapy [ 13 , 14 ]  . 
in t parameter evaluation , transrectal endoscopic us ( eus ) is widely used , with reported accuracy values of 6497% and sensitivity values of 5057% in detecting peritumoural lymphadenopathies la us endoscopica transrettale ( eus ) viene ampiamente impiegata nella valutazione del parametro t , con valori di accuratezza riportati tra 64% e 97% e valori di sensibilit pari a 50%57% nel riconoscimento di linfoadenopatie peritumorali [ 15 , 16 ]  . 
however , this technique is operator dependent and usually applied only for studying the colonic distal tract [ 17 ]  . diagnostic accuracy values of 81% and 65.2% have been reported for mr imaging and ct , respectively , in colorectal cancer staging [ 18 ] ; ct examination is , however , usually preferred , as it is a faster and less expensive tool , with increased diagnostic potential due to the diffusion of multidetector - row devices [ 7 , 19 ]  . 
in t - parameter evaluations , results reported in the literature are rather discordant , with accuracy values between 60% and 97% [ 38 , 10 ] , depending on the ct device and the technique used to achieve colonic distension . 
the use of endoluminal hyperdense contrast materials , such as diatrizoate meglumine water solutions , might not allow accurate evaluation of wall enhancement after intravenous injection of contrast material or the detection of small wall lesions . 
as already reported in the literature , endoluminal hypodense contrast media , such as water and air , are preferred for preoperative staging of colosigmoideal cancer because they offer an accurate evaluation of the intestinal walls and the si di metodica rapida e meno costosa , con miglior potere diagnostico dovuto alla diffusione delle apparecchiature multidetettore [ 7 , 19 ]  . 
nella valutazione del parametro t , i risultati presenti in letteratura sono piuttosto discordanti , con valori di accuratezza compresi tra 60% e 97% [ 38 , 10 ] , sulla base delle apparecchiature tc utilizzate e del tipo di tecnica eseguita per la distensione del colon . 
limpiego di mezzi di contrasto endoluminali iperdensi , come le soluzioni acquose di diatrizoato di meglumina , potrebbero impedire una accurata valutazione dellenhancement parietale dopo iniezione endovenosa di mezzo di contrasto o il riconoscimento di piccole lesioni parietali . 
come gi riportato in letteratura , preferibile limpiego di mezzi di contrasto endoluminali ipodensi , come lacqua o laria , per la stadiazione pre - operatoria del carcinoma del colonsigma , in quanto consentono una accurata valutazione delle pareti intestinali ed il riconoscimento di piccole lesioni parietali , del diametro compreso tra 3 e 5 mm [ 5 , 6 ]  . la distensione del colon mediante aria riduce il rischio di evacuazione del paziente sul tavolo tc e pu consentire navigazioni endoscopiche virtuali ; tale distensione pu essere ottenuta con insufflazione manuale di aria o radiol med ( 2012 ) 117 : 254267 detection of small wall lesions between 3 and 5 mm in diameter [ 5 , 6 ]  . air colonic distension reduces the risk of patient evacuation on the ct table and could allow virtual endoscopic studies ; it can be obtained by manual insufflation of room air or automated insufflation of carbon dioxide [ 20 ]  . 
also , the excessive difference between wall and lumen density , especially after intravenous injection of contrast material , may prevent optimal evaluation of the actual wall thickness both in normal and pathological conditions [ 21 ]  . 
besides , colonic distension by automated carbon dioxide insufflation reduces patient discomfort after the procedure because of its rapid reabsorption compared with room air , as shown by clinical studies [ 20 , 22 , 23 ] ; however , in our experience , by removing the rectal tube 5 min after the end of the examination , patients did not report particular abdominal bloating or discomfort , even though room air was insufflated for colonic distension . 
 the use of water as endoluminal hypodense contrast material has been already reported by other authors in the study of the colorectal tract and other portions of the digestive tract . 
in fact , this gastrointestinal contrast material provides a more accurate evaluation of wall thickness and enhancement , even when residual faecal material is present [ 5 , 6 ]  . to our knowledge , no study has compared water and air mdct colonography in the setting of colosigmoideal cancer or demonstrated which technique allows better evaluation of the local extension of the disease . 
comparing two groups of patients with histologically similar lesions who underwent water and air ct colonography , accuracy values for t staging were 88.6% and 80% , respectively , for water and air . 
these inhomogeneous results may be related to the different technique performed for colonic distension and the presence of artefacts that reduce image quality when air is used as hypodense contrast material . 
in fact , in our experience , the number of artefacts was higher in patients with poor intestinal cleansing who underwent air ( 25.7% ) compared with water ct colonography . 
 conversely , water mdct colonography allowed a better evaluation of t1 / t2 and t3 stages in the absence of adequate intestinal cleansing and reduced the number of underand overstaged cases , probably because of better luminal distension and optimal contrast between intestinal lumen and walls after intravenous injection of contrast mediante insufflazione automatica di anidride carbonica [ 20 ]  . 
tuttavia , indipendentemente dalla tecnica utilizzata per distendere il colon , la colonografia con aria potrebbe risultare pi dolorosa rispetto a quella con acqua , a causa della iperpressione endoluminale e la eccessiva differenza di densit tra parete e lume intestinale , specialmente dopo iniezione endovenosa di mezzo di contrasto , potrebbe impedire una ottimale valutazione del reale spessore parietale , sia in condizioni normali che patologiche [ 21 ]  . 
inoltre , la distensione del colon mediante insufflazione automatica di anidride carbonica riduce il disagio del paziente dopo la procedura , a causa del suo rapido riassorbimento rispetto allaria , come mostrato in recenti studi clinici [ 20 , 22 , 23 ] ; tuttavia , nella nostra esperienza , rimuovendo la sonda rettale 5 minuti dopo il termine della procedura , i pazienti non hanno riferito particolare gonfiore addominale o disagio , pur avendo insufflato aria per la distensione del colon . lutilizzo dellacqua come mezzo di contrasto endoluminale ipodenso stato gi riportato da altri autori nello studio del colon - retto , come anche di altri tratti del tubo digerente . 
infatti , tale mezzo di contrasto gastrointestinale consente una pi accurata valutazione dello spessore e dellenhancement parietale , anche in presenza di materiale fecale residuo [ 5 , 6 ]  . per quanto di nostra conoscenza , nessuno studio ha confrontato la colonografia con acqua e con aria con riferimento al cancro del colon - sigma o ha dimostrato quale tecnica consenta una migliore valutazione della estensione locale di malattia . 
 dal confronto dei due gruppi di pazienti , affetti da lesioni con simili caratteristiche istologiche e sottoposti a colonografia con acqua o con aria , i valori di accuratezza ottenuti dalla nostra esperienza per la stadiazione del parametro t sono stati rispettivamente pari a 88 , 6% e 80% , rispettivamente per lacqua e per laria . 
questa disomogeneit di risultati potrebbe essere determinata dalla differente tecnica eseguita per la distensione del colon e dalla presenza di artefatti che riducono la qualit delle immagini , qualora si utilizzi laria come mezzo di contrasto ipodenso . 
infatti , nella nostra esperienza , il numero di artefatti risultato maggiore nei pazienti con scarsa pulizia intestinale sottoposti a colonografia con aria ( 25 , 7% ) rispetto alla colonografia con acqua . 
 al contrario , la colonografia tcmd con acqua ha consentito una migliore valutazione dei parametri t1 / t2 e t3 , anche in assenza di una adeguata preparazione intestinale ed ha ridotto il numero dei casi di sottoo sovrastadiazione , probabilmente per una migliore distensione luminale ed un contrasto ottimale tra lume e parete intestinale dopo iniezione endovenosa di mezzo di contrasto [ 6 ]  . 
sebbene luso di differenti preparazioni intestinali per un piccolo sottogruppo di pazienti possa avere uno scarso potere statistico , tale elemento non ha rappresentato , tuttavia , un fattore con266 radiol med ( 2012 ) 117 : 254267 material [ 6 ]  . 
although the different colonic preparations for a small subgroup of patients could be of little statistical value , this element did not constitute a confounding effect in the interpretation of results and contributed to the evaluation of staging capability in the event of insufficient intestinal cleansing . 
 however , despite the increased number of errors , the accuracy rate of air colonography obtained in our study ( 80% ) for t staging is similar to values already reported by other authors with the same ct technique ( 78.7% in a group of 33 patients and 83% in another group of 41 patients ) [ 8 , 24 ]  . 
 in our experience , the low misdiagnosis rate for both techniques is also due to the technical features of the multidetector - row scanner , which reduce partial volume artefacts and provide high - quality mpr , with better evaluation of perilesional fat tissue [ 8 , 19 ]  . 
conversely , the different endoluminal contrast media do not significantly influence diagnostic accuracy of the n parameter , even though optimal distension of colorectal walls could allow detection of peritumoural lymph nodes , especially when they are closely adherent to the tumour site . 
this difference is not significant , and the values are similar to those already reported in the literature for n staging of colorectal cancer [ 8 , 10 ]  . 
however , these possibilities should be demonstrated by larger studies . fondente nella interpretazione dei risultati ed ha contribuito alla valutazione della capacit di stadiazione , anche in caso di pulizia intestinale insufficiente . 
infatti , il tasso di sovrastadiazione del parametro t risultato pari al 11 , 4% per la colonografia tc con acqua , mentre il tasso complessivo di errata diagnosi per la colonografia tc con aria risultato pari al 20% . 
tuttavia , nonostante lincremento del numero di errori , laccuratezza della colonografia con aria ottenuta nel nostro studio ( 80% ) per la stadiazione del parametro t simile ai valori gi riportati in letteratura da altri autori con la stessa tecnica tc ( 78 , 7% in un gruppo di 33 pazienti ed 83% in un altro gruppo di 41 pazienti ) [ 8 , 24 ]  . nella nostra esperienza , il basso tasso di errata diagnosi per entrambe le metodiche anche determinato dalle caratteristiche tecniche dellapparecchiatura multidetettore che riducono gli artefatti da volume parziale e forniscono ricostruzioni mpr di alta qualit , con migliore valutazione del tessuto adiposo perilesionale [ 8 , 19 ]  . 
al contrario , i differenti mezzi di contrasto endoluminali non influenzano in modo significativo laccuratezza diagnostica del parametro n , sebbene una distensione ottimale delle pareti del colonretto possa consentire il riconoscimento di linfonodi peritumorali , specie quando strettamente adesi alla sede della neoplasia . 
infatti , i valori di accuratezza riportati nel nostro studio per il parametro n sono pari al 77 , 1% e 74 , 3% , rispettivamente per la colonografia tc con acqua e con aria . 
questa differenza non risulta significativa ed i valori riportati sono simili a quelli gi descritti in letteratura per la stadiazione del parametro n del cancro del colon - retto [ 8 , 10 ]  . 
tuttavia , tali potenzialit devono essere dimostrate su pi ampie casistiche . conclusions mdct with the possibility of performing high - quality mpr represents an accurate tool for staging colosigmoideal cancer . 
in the definition of the t parameter , water colonography seems to provide more accurate information compared with air , as it enables a better evaluation of the walls in the case of poor lumen distension and insufficient intestinal cleansing , thereby allowing a better selection of patients to be treated by radical or palliative surgery . 
however , an essential limitation for both techniques remains the degree of patient cooperation and quantity of endoluminal hypodense contrast material introduced , which may influence adequate distension of the colonic segments . 
la colonografia tcmd presenta lo stesso valore di accuratezza diagnostica per la stadiazione del parametro n , indipendentemente dal mezzo di contrasto endoluminale ipodenso impiegato per la distensione del colon . 
nella definizione del parametro t , la colonografia con acqua sembra fornire informazioni pi accurate rispetto a quella con aria , a causa di una migliore valutazione parietale , anche in caso di scarsa distensione luminale ed insufficiente pulizia intestinale , consentendo una migliore selezione dei pazienti da sottoporre a trattamento chirurgico radicale o palliativo . 
tuttavia , limite fondamentale per entrambe le metodiche resta il grado di collaborazione del paziente e la quantit di mezzo di contrasto endoluminale ipodenso introdotto , in grado di influenzare una adeguata distensione dei segmenti colici . 
donofrio springer verlag , 2012 isbn - 13 : 978 - 88 - 470 - 2378 - 9 published online : 10 february 2012 springer - verlag 2012 the book ultrasonography of the pancreas represents the state of the art in this field and is the result of the contribution of a group of authors of internationally renowned authors and , primarily , of the editor . 
 ultrasonography ( us ) is , in many cases , the initial imaging modality in most institutions with which to evaluate pancreatic pathologies and clinical symptoms that may be related to pancreatic diseases . 
however , many of these limitations have been overcome by technological advances in us , which have had an extremely positive impact in studying the pancreas , as in other organs . significant advances have occurred both in conventional , harmonic and doppler imaging . 
contrast media has received growing attention in us , with special emphasis in liver studies in which contrast - enhanced us ( ceus ) is now a well - established modality . 
furthermore , in recent years , the application of and indication for interventional , endoscopic and intraoperative us have imil libro ultrasonography of the pancreas rappresenta lo stato dellarte dellecografia in questo distretto portando , grazie al contributo di autori di livello internazionale e in particolar modo delleditore , un vero avanzamento in campo diagnostico e interventistico . lecografia rappresenta spesso la prima metodica di immagine nella valutazione di una sospetta patologia pancreatica ; al tempo stesso lecografia lindagine che , proprio per il suo ampio utilizzo , spesso la prima indagine che identifica una lesione ancora asintomatica . 
ciononostante , le possibilit dellecografia nello studio del pancreas sono spesso messe in discussione da parte di molti radiologi , e non solo , sia per la diversit dei risultati sia per la sua scarsa riproducibilit . 
i principali motivi alla base di tali perplessit e del ruolo controverso che lecografia ha nello studio di questo organo , sono rappresentati dalla diversa esperienza degli operatori e da problematiche riguardanti lesplorabilit del paziente , come meteorismo ed obesit . 
peraltro vero che i progressi tecnologici hanno avuto un impatto estremamente positivo nello studio ecografico del pancreas sia per quanto concerne lecografia convenzionale , sia per le tecniche doppler e limaging armonico , permettendo oggi una valutazione precisa della patologia pancreatica . 
al tempo stesso , possibile visualizzare i vasi peri - pancreatici mediante lo studio ecografico convenzionale e doppler , fornendo elementi utili per il bilancio di estensione . il ruolo del mezzo di contrasto in ecografia ha acquistato unimportanza sempre maggiore , in particolare nello studio del fegato , in cui lecografia con mezzo di contrasto ( ceus ) rappresenta una tecnica dindagine ormai affermata . 
in ambito pancreatico , il contributo che il mezzo di contrasto offre nella caratterizzazione dei tumori , sia solidi sia cistici , esocrini ed endocrini , sta assumendo sempre maggiore importanza . 
va infine sottolineato come , negli ultimi anni , grazie agli avanzamenti tecnologici , si assistito ad un aumento delle applicazioni dellecografia in ambito interventistico , endoscopico ed intraoperatorio . 334 radiol med ( 2012 ) 117 : 333334 proved significantly due to technological advances . all these new us applications are extensively reviewed in this book , which provides the reader with an updated overview of modern pancreatic imaging . 
the book contains 14 chapters dedicated to technical issues concerning modern us imaging , image - guided biopsy , endoscopic us , interventional us - guided procedures and intraoperative us . 
an interesting chapter on normal anatomy , including variants and pseudolesions , of the pancreas appears before the chapters dedicated to pancreatic pathologies that address solid and cystic tumours , rare tumours that are discussed with emphasis on imaging and pathologic correlation . 
 tutte queste nuove applicazioni dellecografia sono descritte in maniera approfondita in questo libro , che ha lo scopo di fornire al lettore una panoramica aggiornata sul moderno studio ecografico del pancreas con essenziali correlazioni imaging ( tcms e rm ) e anatomopatologiche . 
segue poi una serie di capitoli dedicati alle principali patologie del pancreas , in particolare le pancreatiti , i tumori solidi e cistici e i tumori rari del pancreas , descritti in modo approfondito sia dal punto di vista imaging che anatomopatologico . 
colagrande1 1careggi , viale morgagni 85 , 50134 florence , italy 2section of medical physics , azienda ospedaliero - universitaria careggi , florence , italy 3cirm , university of florence , azienda ospedaliero - universitaria careggi , florence , italy 4department of diagnostic for imaging , 1st radiology , spedali civili of brescia , italy 5center for systemic manifestations of hepatitis viruses ( masve ) , department of internal medicine , university of florence , florence , italy correspondence to : s . 
the final study group of 50 patients was divided into two subgroups on the basis of clinical course : group 1 consisted of 42 patients requiring noninvasive mechanical ventilation and admitted to the utsir ; group 2 consisted of eight patients who required icu admission and extracorporeal membrane oxygenation or advanced mechanical ventilation from october 2009 to december 2009 . 
lo scopo di questo lavoro stato quello di definire il quadro radiologico ( rx ) e la semeiotica della tomografia computerizzata ( tc ) a strato sottile delle complicanze polmonari in una popolazione selezionata di 50 pazienti consecutivi affetti da influenza virale a ( h1n1 ) di origine suina ( s - oiv ) ricoverati nellunit di terapia respiratoria subintensiva ( utsir ) e nella terapia intensiva ( icu ) dellazienda ospedaliera monaldi , napoli , italia . 
quattro radiologi hanno retrospettivamente esaminato gli esami radiologici tradizionali ( rx ) e di tomografia computerizzata multidetettore ( tcmd ) di cinquanta pazienti che rispettavano i criteri della world health organization ( who ) per linfluenza a ( h1n1 ) s - oiv . 
il gruppo dei 50 pazienti in studio stato suddiviso in due sottogruppi sulla base del decorso clinico : il gruppo 1 , composto da 42 pazienti che hanno richiesto la ventilazione meccanica non invasiva e ricoverati allutsir ; il gruppo 2 , costituito da 8 pazienti sottoposti a extra corporeal membrane oxygenation ( ecmo ) o a ventilazione meccanica convenzionale protetta , ricoverati in icu da ottobre a dicembre 2009 . 
tutti i pazienti hanno eseguito esami rx e tcmd a strato sottile , di cui stato valutato il pattern di ingresso e di follow - up ( consolidazione , opacit groundglass , noduli e reticolazione interstiziale ) , la distribuzione e lestensione delle alterazioni . 
thoracic comorbidity was present in 18% of patients ; 22% of patients was obese , and in this group , the clinical course was more aggressive than in the others with the same lesion extent at imaging . 
the most common cxr and ct findings in patients with s - oiv infection were unilateral or bilateral ground - glass opacities with or without associated focal or multifocal areas of consolidation . 
on mdct , ground - glass opacities and areas of consolidation had a predominant peribronchovascular and subpleural distribution , resembling organising pneumonia ; they progressed to bilateral extensive airspace disease in severely ill patients . keywords influenza a ( h1n1 ) viral pneumonia reverse halo sign ( rhs ) radiology computed tomography in una polmonite virale in tre pazienti il segno dellalone invertito ( reversed halo sign )  . 
il 18% dei pazienti presentava una comorbidit toracica ; il 22% di essi era obeso ed in questo gruppo , pur con la stessa estensione delle lesioni allimaging rispetto ai non obesi , il decorso clinico stato pi aggressivo . 
i segni rx e tcmd pi comuni nei pazienti con influenza virale a di origine suina sono rappresentati da opacit ggo unio bilaterali con o senza aree di consolidazione focali o multifocali associate . 
alla tc le aree ggo e consolidative hanno presentato una distribuzione prevalente subpleurica e peribroncovasale , rassomigliando alla polmonite in organizzazione ; in pazienti gravemente malati esse progrediscono ad una malattia consolidativa degli spazi aerei bilaterale ed estesa . parole chiave influenza a ( h1n1 ) polmonite virale segno dellalone inverso ( rhs ) radiologia tomografia computerizzata introduction introduzione influenza viruses are common and important human pathogens that are responsible for seasonal epidemics and occasional unpredictable pandemics . 
the influenza a virus infects wide varieties of warm - blooded animals , including birds , swine , horses and humans , whereas influenza b and influenza c viruses almost exclusively infect humans and are also implicated in epidemics [ 1 ]  . 
a new subtype of influenza a virus was described from march 24 through april 24 , 2009 , in mexico city , which rapidly spread around the world [ 2 ]  . 
transmission of the 2009 influenza a ( h1n1 ) virus was declared to be a worldwide pandemic by the world health organization ( who ) on 11 june 2009 [ 3 ]  . 
clinical manifestations of influenza - like illness range from asymptomatic infection to mild upper respiratory illness , viral syndrome , diarrhoea and severe pneumonia to acute respiratory distress syndrome ( ards ) and to progression to multiorgan failure . 
the h1n1 influenza a virus may cause severe viral pneumonia in persons with underlying pulmonary abnormalities as well as in healthy i virus dellinfluenza sono comuni ed importanti patogeni umani responsabili di epidemie stagionali ed occasionalmente di imprevedibili pandemie . 
il virus influenzale infetta numerosi animali a sangue caldo , compresi gli uccelli , i maiali , i cavalli e gli esseri umani , mentre i virus influenzali b e c infettano quasi esclusivamente gli esseri umani e sono implicati nelle epidemie [ 1 ]  . 
un nuovo sottotipo di virus influenzale a ( h1n1 ) stato descritto dal 24 marzo al 24 aprile 2009 a citt del messico e si diffuso rapidamente in tutto il mondo [ 2 ]  . 
le manifestazioni cliniche della malattia possono variare da uninfezione asintomatica ad una lieve malattia delle vie respiratorie superiori , ad una sindrome virale con diarrea , ad una polmonite grave con sindrome da distress respiratorio acuto ( ards ) fino alla progressione allinsufficienza multiorgano . 
populations at increased risk for morbidity and mortality are the very young and elderly , the pregnant , those with comorbid chronic cardiopulmonary conditions such as asthma and the immunocompromised . 
the pneumonia may develop into a diffuse ards type of pulmonary involvement , and those with respiratory failure may require ventilatory support and sometimes treatment with extracorporeal membrane oxygenation . chest x - ray ( cxr ) findings described in clinical and radiological reports of viral pneumonia are bilateral patch alveolar opacities with basal lung predominance or interstitial opacities such as linear , reticular or nodular shadows [ 2 , 511 ]  . 
the purpose of our study was to retrospectively analyse cxr and thin - section ct findings of pulmonary complications in a selected population of 50 consecutive patients admitted to monaldi hospital ( naples , italy ) , a tertiary care centre for respiratory diseases , with novel swine - origin influenza a ( h1n1 ) virus ( s - oiv ) pneumonia requiring subintensive or intensive care and relate the radiological signs to patients outcomes . 
informed consent was waived because of the retrospective nature of this study ; however , patient confidentiality was maintained in accordance with the ethical standards of the world medical association . 
the definitive diagnosis of s - oiv infection , which typically takes 12 days at our hospital , was made with real - time reverse transcriptase polymerase chain reaction ( rt - pcr ) or the us food and drug administrationapproved proflu + assay and subtyping for 2009 h1n1 influenza . 
all patients had severe and non - self - limited clinical course of s - oiv infection and were transferred from other city or regional hospitals due to critical clinical conditions . the study group was divided into two subgroups on the basis of their clinical course : group 1 consisted of 42 patients with severe acute hypoxaemic respiratory failure come in soggetti sani [ 4 ]  . 
 la polmonite pu progredire ad una sindrome da distress respiratorio acuto delladulto ed i pazienti con insufficienza respiratoria possono richiedere supporti ventilatori e talvolta il trattamento con ossigenazione extracorporea a membrana ( ecmo )  . 
 i segni radiologici tradizionali ( rx ) pi spesso descritti nelle polmoniti virali sono chiazze bilaterali di addensamento alveolare a vetro smerigliato a distribuzione basale , opacit interstiziali di tipo lineare , reticolare e nodulare [ 2 , 511 ]  . 
alla tomografia computerizzata ( tc ) si apprezzano in genere noduli centrolobulari mal definiti delle piccole vie aeree , aree peribronchiali sfumate con densit a vetro smerigliato e consolidazioni segmentarie o diffuse . 
scopo del nostro studio definire il quadro radiologico ( rx ) e la semeiotica della tc multidetettore a strato sottile ( tcmd ) delle complicanze polmonari in una popolazione selezionata di 50 pazienti consecutivi affetti da influenza virale a ( h1n1 ) di origine suina ( s - oiv ) , ospedalizzati in terapia respiratoria subintensiva o intensiva , correlando la semeiotica radiologica alla prognosi . materiali e metodi il nostro comitato etico ha approvato questa revisione retrospettiva dellimaging toracico dei pazienti e delle cartelle cliniche . 
il consenso informato non stato richiesto a causa della natura retrospettiva dello studio , tuttavia , la riservatezza del paziente stata mantenuta conformemente agli standard etici della world medical association . 
abbiamo retrospettivamente esaminato gli esami rx e tcmd di cinquanta pazienti consecutivi ricoverati presso lazienda ospedaliera monaldi ( napoli , italia ) , centro di riferimento regionale per la cura delle malattie respiratorie , da ottobre a dicembre 2009 ( 28 donne , 22 maschi ; et media , 40 , 9 anni13 , 01 deviazione standard [ sd ] ; et mediana , 41 , 5 anni ; range 2176 anni ) con quadro clinico di polmonite complicata secondo i criteri oms per linfluenza a ( h1n1 ) da s - oiv . 
la diagnosi definitiva di influenza virale h1n1 di origine suina stata ottenuta con tecnica reverse transcriptase polymerase chain reaction ( rt - pcr ) o con il test proflu + approvato dalla food and drug administration con sottotipizzazione per linfluenza h1n1 2009 e ha richiesto in genere 12 giorni presso la nostra azienda . 
tutti i 50 pazienti hanno avuto una forma grave e non autolimitata 168 radiol med ( 2012 ) 117 : 165184 resistant to conventional oxygen therapy who required noninvasive mechanical ventilation ( nmv ) using continuous positive airway pressure ( cpap ) and admission to the subintensive respiratory unit ( utsir ) ; group 2 consisted of eight patients who required admission to the intensive care unit ( icu ) , where four underwent extracorporeal membrane oxygenation ( ecmo ) or advanced conventional mechanical ventilation . 
thirty - six patients who were able to stand had posteroanterior and lateral - projection initial radiographs , and the remaining 14 had bedside anteroposterior - projection initial radiographs ( direct view dr system , kodak , using a standardised technique ; 90 kv , 5 mas , 180 - cm film - focus distance for posteroanterior ; 100 kv , 5 mas , 180 - cm film - focus distance for lateral ; direct view cr 850 system , kodak , using a standardised technique ; 75kv , 6 mas , 100 - cm film - focus distance for bedside anteroposterior ; broad tube focus for all )  . 
images were assessed using a picture archiving and communication system ( pacs ) viewer with a 2 , 0482 , 048 - pixel monitor ( totoku electric , me551i2 minatoku , tokyo , japan )  . 
all patients underwent follow - up cxr ; eight patients had one follow - up ct scan , four had two follow - up ct scans and two had three followup ct scans . 
a clinical database of these patients that included sex , age , comorbidities and need for mechanical ventilation was collected for clinicalradiological comparison and to relate the radiological signs to the patients outcome . 
on initial cxr images , the reviewers first classified all chest radiographs as normal or abnormal on the basis of an assessment of the lung parenchyma , airways , pleura , hila and mediastinuabnormalities were further characterised as consolidation ( opacification obscuring the underlying vessels ) , ground - glass opacity ( ggo ; increased attenuation not obscuring the underlying vessels ) , nodules and reticulation . 
 each lung was divided into upper , middle and lower lung zones ( each comprising a third of the craniocaudal extent of the lungs on frontal radiograph ) and zone involvement dinfezione e , per le condizioni cliniche critiche , sono stati trasferiti da altri ospedali cittadini o della nostra regione . il gruppo di pazienti oggetto di studio stato suddiviso in due sottogruppi sulla base del decorso clinico . 
il gruppo 1 era costituito da 42 pazienti con grave insufficienza respiratoria ipossiemica resistente allossigenoterapia convenzionale che ha richiesto una ventilazione meccanica non invasiva con pressione continua positiva delle vie aeree ( cpap ) e ricovero in ununit di terapia respiratoria subintensiva ( utsir ) ; il gruppo 2 era composto da 8 pazienti che hanno richiesto ricovero in terapia intensiva ( icu ) , dove quattro sono stati sottoposti a ecmo e 4 a ventilazione meccanica convenzionale protetta . 
solo un paziente , gi affetto da tubercolosi fibrocavitaria , stato trasferito dallutsir allicu ( dal gruppo 1 al gruppo 2 ) per mancata risposta alla ventilazione meccanica non invasiva . 
nei 36 pazienti che potevano mantenere lortostatismo lesame stato eseguito nelle proiezioni postero - anteriore ( pa ) e latero - laterale ( ll ) , nei restanti 14 pazienti , obbligati al clinostatismo , stata eseguita la sola proiezione antero - posteriore ( ap ) a letto ( sistema kodak direct view dr con tecnica standardizzata ; 90 kv , 5 mas , distanza fuoco - film 180 cm per la proiezione postero - anteriore ; 100 kv , 5 mas , distanza fuoco - film 180 cm per la proiezione latero - laterale ; sistema kodak direct view cr 850 con tecnica standardizzata ; 75kv , 6 mas , distanza fuoco - film 100 cm per esami a letto in proiezione antero - posteriore ; fuoco non fine in tutti i casi )  . 
nella fase acuta tutti i pazienti hanno eseguito radiografie di follow - up , solo 8 pazienti hanno effettuato una tc di controllo , 4 di essi due tc , mentre 2 sono stati sottoposti a tre tc di follow - up . 
stato raccolto un database , comprendente tra laltro il sesso , let , le comorbilit , la necessit di ventilazione meccanica , per il confronto clinico - radiologico al fine di correlare il quadro radiologico alloutcome dei pazienti . 
the presence of lymph node enlargement , pleural effusions , pneumothorax and pneumomediastinum was recorded . ct studies were obtained using a 16 - slice ct scanner ( philips brilliance ; philips healthcare )  . 
images were viewed on both lung ( window width 1 , 500 hu ; level 700 hu ) and mediastinal ( window width 350 hu ; level 40 hu ) settings . 
ct scans were assessed for the presence of peribronchovascular or peripheral ( subpleural ) ggo , consolidation , nodular opacities , tree - in - bud pattern , septal lines and reticular opacities . 
a lymph node was considered enlarged when the short - axis diameter was > 1 cm at the hilum and mediastinuggo were defined as hazy areas of increased opacity or attenuation without obscuration of the underlying vessels . 
predominant distribution was also assessed as being in the upper , middle or lower lung zone and as being predominantly subpleural ( involving mainly the peripheral one third of the lung ) , random ( without predilection for subpleural or central regions ) , peribronchovascular or diffuse ( continuous involvement without respect to lung segments )  . 
attention was also paid to the presence of nodules or masses , lymphadenopathy , cyst - like lesion , bronchiolar and / or bronchial dilatation , overinflated secondary pulmonary lobules , pulmonary interstitial emphysema , logica sulla base della valutazione del parenchima polmonare , delle vie aeree , della pleura , degli ili e del mediastino . 
ogni polmone stato diviso in una zona superiore , media ed inferiore ( ciascuna comprendente un terzo dei polmoni in senso apico - basale sulla radiografia frontale ) ed stato valutato il coinvolgimento zonale . 
 gli studi tc sono stati ottenuti usando unapparecchiatura a 16 file di detettori ( philips brilliance ct 16 - slice ; healthcare philips medical systems , best , paesi bassi )  . 
il protocollo di studio utilizzato prevedeva scansioni , quando possibile , in inspirio , spessore di strato di 2 mm , intervallo di ricostruzione di 1 mm , collimazione 161 , 5 , pitch 0 , 938 , campo di vista ( fov ) di 400 mm , tempo di rotazione 0 , 5 s , kv 120 , 199 ma . 
le immagini sono state visualizzate con finestra polmonare ( larghezza della finestra , 1500 uh ; livello , - 700 uh ) e mediastinica ( larghezza della finestra , 350 uh ; livello , 40 uh )  . 
le scansioni tc sono state valutate per la presenza di ggo peribroncovasale o periferico ( subpleurico ) , consolidazioni , opacit nodulari , tree - in - bud , ispessimento dellinterstizio settale , reticolazioni . 
la distribuzione stata definita come focale , multifocale o diffusa ; focale se presente un solo focolaio patologico , multifocale 170 radiol med ( 2012 ) 117 : 165184 pneumothorax and pneumomediastinu the presence of parenchymal bands ; irregular bronchovascular , pleural or mediastinal interfaces ; and traction bronchiectasis was considered evidence of probable fibrosis [ 1316 ]  . 
the upper zone was defined as the area above the level of the carina , the middle as the area between the level of the carina and the level of infrapulmonary vein and the lower zone as the area below the level of infrapulmonary vethe extent of each abnormality was determined by visually estimating the percentage ( to the nearest 10% ) of the affected lung parenchyma in each zone . 
assessments of the four observers were averaged . the frequency of signs was indicated , and the percentage with the 95% confidence limits ( cl95% ) was reported in the assumption of a normal distribution . 
 ards was defined as acute onset of hypoxaemia with partial arterial pressure of oxygen to fraction of inspired oxygen ( pao2 / fio2 ) < 200 mmhg with characteristic rapid opacification of the entire lung and clinical absence of elevated left atrial pressure [ 17 ]  . 
twelve patients had other thoracic comorbidity : three bullous dystrophy , one amiodarone lung toxicity , five chronic obstructive pulmonary disease ( copd ) , one asthma , one recurrent bronchitis and one fibrocavitary tuberculosis with several infected cysts , blebs and bullous emphysema . 
twenty had combined extrathoracic comorbidity : five cardiac disease , seven systemic hypertension , 11 obesity ( 22% + 11 cl95% ) , two chronic hepatitis , one renal failure , one hyperthyroidism , one hereditary spherocytosis , two hyperlipidaemia , one a drug abuser one endocarditis . cxr and mdct findings are summarised in tables 1 and 2 . 
la distribuzione prevalente stata valutata come interessante la zona di polmone superiore , medio o inferiore e , sul piano assiale , come prevalentemente subpleurica ( che comprende principalmente il terzo periferico del polmone ) , random ( senza predilezione per la regione subpleurica ) , peribroncovasale , diffusa ( coinvolgimento continuo senza specificit per i segmenti polmonari )  . 
stata inoltre posta attenzione alla presenza di noduli o masse , adenomegalie , lesioni cistiche , dilatazione dei bronchi e / o dei bronchioli , di lobuli polmonari secondari sovradistesi , enfisema interstiziale , pneumotorace e pneumomediastino . 
la presenza di bande parenchimali , di interfacce irregolari broncovascolari , della pleura o del mediastino , di bronchiectasie da trazione stata considerata la prova di fibrosi probabile [ 1316 ]  . 
 lestensione delle lesioni stata valutata in modo indipendente su tre zone di ciascun polmone ( superiore , media ed inferiore ) ; la zona superiore definita come larea sovracarenale , la zona intermedia come larea posta tra la carena e le vene polmonari inferiori , la zona inferiore come larea caudale alle vene polmonari inferiori . 
stata fatta una media delle valutazioni dei quattro osservatori . stata registrata la frequenza dei segni e la loro percentuale con intervalli di confidenza al 95% ( cl95% ) nel presupposto di una distribuzione normale . 
i cl95% sono stati calcolati con la formula : 1.96 p ( 1 - p ) / n , dove p indica la percentuale ed n la grandezza della popolazione . 
non stata effettuata alcuna altra analisi statistica dal momento che non era disponibile un gruppo di controllo e non stata considerata appropriata una comparazione tra il gruppo della terapia subintensiva e quello della rianimazione . 
la ards stata definita come insorgenza acuta di ipossiemia ( pao2 / fio2 < 200 mmhg ) , la caratteristica opacizzazione rapida di tutto il polmone allimaging e lassenza clinica di elevata pressione atriale sinistra [ 17 ]  . risultati ventinove / 50 pazienti ( 58%13 cl95% ) hanno avuto comorbilit , in dodici casi sia toracica che extratoracica . 
in 18 patients , it was between 10% and pazienti avevano comorbilit solo toracica : tre presentavano distrofia bollosa , un paziente era affetto da tossicit da amiodarone , cinque da malattia polmonare cronica ostruttiva ( bpco ) , uno da asma , uno da bronchiti ricorrenti , un altro era affetto da tubercolosi fibrocavitaria con diverse cisti infette , blebs ed enfisema bolloso . 
c ricostruzione multiplanare coronale : ggo peribroncovasale con risalto apparente del lume aereo dei bronchi segmentali e subsegmentali , definito il segno del broncogramma scuro ( bronchi a contenuto aereo troppo scuri rispetto al parenchima circostante , che pieno di essudati infiammatori alveolari ed a densit ggo )  . 
2 a 57 - year - old man with clinical finding of fever ( 39 c ) , headache , cough , severe dyspnoea and hepatomegaly ( group 1 )  . 
2 uomo di 57 anni con presentazione clinica costituita da febbre ( 39 c ) , mal di testa , tosse , grave dispnea ed epatomegalia ( gruppo 1 )  . 
lobesit ( indice di massa corporea > 30 ; da 32 a 42 nei nostri casi ) e la concomitante patologia polmonare sono state associate ad un decorso pi aggressivo ; in particolare , tra gli 11 pazienti obesi , 5 ( 45% ) hanno richiesto la ventilazione assistita . 
quattro pazienti tra i 2538 anni , in terapia intensiva ( gruppo 2 ) sono morti ( 8% ) ; uno , affetto da tubercolosi fibrocavitaria e sovra - infezione con pseudomonas aeruginosa , per sepsi generalizzata ; negli altri 3 casi ( 2 adulti obesi ) la morte stata conseguenza dellards con insufficienza multiorgano ( mof )  . 
3 a 42 - year - old obese hyperlipidemic man with clinical finding of high fever ( 39.7 c ) , nonproductive cough , dyspnoea and acute respiratory failure ( group 1 )  . 
3 uomo di 42 anni obeso ed iperlipidemico con presentazione clinica costituita da febbre alta ( 39 , 7 c ) , tosse non produttiva , dispnea ed insufficienza respiratoria acuta ( gruppo i )  . 
obesity ( body mass index > 30 ; 3242 ) and concomitant pulmonary pathology were associated with a more aggressive course , in particular , in the 11 obese patients , five of whom ( 45% ) required assisted ventilation . 
four patients aged between 25 and 38 years old admitted to the icu ( group 2 ) died ( 8% ) : one due to generalised sepsis in fibrocavitary tuberculosis and superinfection with p . 
in one survivor discharged from icu after 4 weeks , a natural progression of ards was observed [ 18 , 19 ] : early or exudative stage , intermediate stage that began nel mondo . 
a differenza delle forme stagionali questo nuovo ceppo interessa le fasce di et pi giovanili probabilmente a causa della precedente esposizione dei soggetti anziani a virus con antigeni simili , cross - reattivi [ 20 , 21 ]  . 
i virus influenzali di tipo a e b sono responsabili della maggior radiol med ( 2012 ) 117 : 165184 parte delle polmoniti virali negli adulti immunocompetenti [ 5 ]  . 
le polmoniti virali comunemente si manifestano alla radiografia del torace come noduli a contorni sfumati ( noduli alveolari del diametro di 410 mm ) , chiazze di ggo peribronchiale con o senza consolidazione ed aree di reticolazione [ 5 ]  . 
alla tc si apprezzano in genere noduli centrolobulari mal definiti , aree di densit a vetro smerigliato con una distribuzione lobulare , consolidazione segmentaria o diffusa , ispessimento dei setti interlobulari [ 5 ]  . 
aree multifocali di opacit degli spazi aerei possono diventare rapidamente confluenti sulle radiografie del torace di controllo e rappresentano allimaging una combinazione di danno alveolare diffuso , di emorragia e di polmonite in organizzazione , eventualmente con sovrapposta infezione batterica secondaria nelle fasi avanzate della malattia [ 1 , 20 , 22 ]  . 
5 a 68 - year - old man , cardiopathic , affected by influenza a ( h1n1 ) pneumonia overimposed on known amiodarone toxicity with clinical finding of high fever ( 39.5 c ) , cough and marked dyspnoea ( group i )  . 
5 uomo di 68 anni , cardiopatico , affetto da polmonite influenzale a ( h1n1 ) sovrapposta ad una gi nota tossicit polmonare da amiodarone con presentazione clinica costituita da febbre alta ( 39 , 5 c ) , tosse e dispnea marcata ( gruppo i )  . 
le scansioni tcmd assiali a al iii medio e b superiore dei polmoni mostrano un coinvolgimento parenchimale bilaterale con aree tondeggianti di ggo in periferia e broncogramma aereo . 178 radiol med ( 2012 ) 117 : 165184 fig . 
 unilaterale a bilaterale , associate o meno ad aree di consolidazione focale o multifocale principalmente alle basi polmonari , con un quadro simile alla polmonite in organizzazione [ 7 ]  . 
 [ 6 ] hanno riportato i segni rx in 108 pazienti pediatrici , 22 dei quali con ospedalizzazione breve , 14 ricoverati in terapia intensiva e concludevano che discussion a new strain of influenza virus a ( h1n1 ) spread across the world in 2009 . 
unlike seasonal influenza infection , this new form of influenza tends to affect young people , probably as a result of previous exposure of older people to some similar , cross - reacting antigens [ 20 , 21 ]  . 
viral pneumonias commonly manifest on crx as poorly defined nodules ( airspace nodules of 410 mm in diameter ) and patchy areas of peribronchial ggo with or without consolidation and reticular areas of increased opacity [ 5 ]  . 
ct findings consist of poorly defined centrilobular nodules , ground - glass attenuation with a lobular distribution , segmental consolidation or diffuse ground - glass attenuation with thickened interlobular septa [ 5 ]  . 
9a , b a 37 - year - old man with influenza a ( h1n1 ) pneumonia associated to fibrocavitary tuberculosis , infected cysts with fluid level , blebs , bullous emphysema and superinfection with pseudomonas aeruginosa . 
9a , b uomo di 37 anni con polmonite influenzale a ( h1n1 ) associata a tubercolosi fibrocavitaria , cisti infette livellate , blebs , enfisema bolloso e sovra - infezione da pseudomonas aeruginosa . 
a , b scansioni tcmd assiali : consolidazioni associate ai segni della tb fibrocavitaria , cisti infette livellate , blebs ed enfisema bolloso . elderly and immunocompromised patients [ 22 ]  . 
multifocal areas of airspace opacities can rapidly become confluent on serial cxr , and these imaging findings reflect combinations of diffuse alveolar damage , haemorrhage and organising pneumonia , with possibly superimposed secondary bacterial infection in later - stage disease [ 1 , 20 , 22 ]  . 
 [ 7 ] reported radiographic and ct findings in seven patients with s - oiv infection that ranged from unilateral to bilateral predominant peribronchovascular and subpleural ggo with or without associated focal or multifocal areas of consolidation , predominantly in the basal lung zones , resembling organising pneumonia . 
reported radiographic findings in 108 paediatric patients , 22 with brief hospitalisation and 14 with icu admission , and concluded that bilateral , symmetric and multifocal areas of consolidation , often associated with ggo , were the predominant radiographic findings in paediatric patients with a more severe clinical course of s - oiv infection [ 6 ]  . 
 [ 8 ] reported that in patients in more severe stages of infection , the most frequent pattern was bilateral alveolar disease with predominance in the mid - basal lung zones . cxr and ct findings in our study are consistent with those in other series . 
the extent of disease is underestimated il pattern radiologico tradizionale nei pazienti pediatrici , con decorso clinico pi grave , era rappresentato da aree di consolidazione multifocali , bilaterali e simmetriche , spesso associate a ggo [ 6 ]  . 
 [ 8 ] hanno riferito che nei pazienti con forme pi gravi dellinfezione , il pattern pi frequente era la malattia da riempimento alveolare bilaterale , prevalente alle zone polmonari medio - basali [ 8 ]  . 
lestensione della malattia sottostimata dalla radiografia del torace ; il pattern tc prevalente ( 34 / 50 pazienti ; 68% ) era rappresentato da chiazze periferiche di ground - glass segmentario e subsegmentario , nel contesto delle quali risaltano i corrispondenti rami bronchiali , segno gi definito del bronco scuro [ 24 ]  . 
il ggo era predominante nei lobi medio - inferiori dei polmoni , con o senza consolidazione ; il ggo generalmente attribuibile alla sostituzione dellaria con riempimento parziale di spazi aerei , allispessimento dellinterstizio da fluido , sangue o cellule , al parziale collasso alveolare o allaumentato volume ematico capillare . 
 non abbiamo trovato segni di ostruzione delle piccole vie aeree con air trapping ed anomalie del flusso ematico regionale , che sono peraltro state descritte nelle polmoniti virali [ 5 ] ; in soli 2 / 50 casi ( 0 , 04% ) abbiamo avuto un pattern di tree - in - bud ; la perfusione a mosaico era nella gran arte dei casi assente . 
a la radiografia del torace a letto in proiezione antero - posteriore , eseguita alla 1a settimana dal ricovero in terapia intensiva durante la fase essudativa dell ards causata da h1n1 , mostra progressiva opacizzazione bilaterale dei polmoni . 
b alla 3a settimana la scansione tcmd assiale e c la ricostruzione mp coronale mostrano i segni della fibrosi , cio interfacce irregolari ventrali bilaterali e simmetriche , aree di ggo , consolidazioni irregolari e bronchiectasie da trazione . with cxr ; the predominant ct pattern ( 34 / 50 patients ; 68% ) was peripheral distribution of segmental and subsegmental patchy or peribronchovascular ggo with apparent prominence of segmental and subsegmental bronchi , which has been referred to as the dark bronchus sign [ 24 ]  . 
ggo was predominant in the lower and central lung lobes with or without consolidation ; ggo is generally attributable to displacement of air from partial filling of air spaces , thickening of interstitial tissues from fluid , blood or cells , partial alveolar collapse or increased capillary blood volume . we found no signs of small - airway obstruction with air trapping and regional blood flow abnormalities , which have otherwise been described in viral pneumonias [ 5 ] ; in only two cases ( 0.04% ) did we find a tree - in - bud pattern ; mosaic perfusion was conspicuously absent . 
these findings were suggestive of less airway inflammation due to the propensity of h1n1 virus to involve the alveolar epithelium more than the bronchiolar epithelium . initial lesions in h1n1 pneumonia typically appear as lung opacities that occur mostly in the middle and lower zones of the lung with peripheral and peribronchovascular minore infiammazione delle vie aeree inferiori dovuta al maggior tropismo del virus h1n1 per lepitelio alveolare rispetto a quello bronchiolare . 
nelle infezioni gravi le alterazioni anatomo - patologiche comprendono la tracheobronchite , la necrosi alveolare con emorragia , la formazione delle membrane ialine , la trombosi dei piccoli vasi con foci infartuali pleuro - parenchimali e degenerazione cistica [ 25 ]  . 
 lestensione delle lesioni a consolidazioni degli spazi aerei confluenti e bilaterali , come avvenuto nei nostri pazienti di terapia intensiva , si correla con la gravit dellipossia e con la prognosi . 
in severe infection , pathological changes of influenza pneumonia include tracheobronchitis , alveolar necrosis with haemorrhage , hyaline membrane formation and small - vessel thrombosis with foci of parenchymal and pleural infarction and cystic change [ 25 ]  . 
in ards , respiratory epithelial injury with abnormally increased permeability of the capillary endothelium initially produces patchy consolidations on ct and cxr , with evolution to confluent bilateral airspace opacity . 
injury to the lung parenchyma may be caused by infection , toxic inhalation , trauma , barotrauma or emboli and may be caused indirectly by extrapulmonary disease , such as septic shock , pancreatitis or other metabolic derangement . 
in our patients , ards was associated with a pattern of severe lung injury involving peribronchial inflammation with predominant nondependent distribution ; alveoli in the nondependent portions of the lungs , located anteriorly in the supine patient , are thus more susceptible to overinflation and rupture . 
free air can also track peripherally , towards the subpleural interstitium , and rupture through the visceral pleura , causing pneumothorax and pneumomediastinufrom the mediastinum , air can further track into the fascial layers of the neck and continue into the subcutaneous tissues of the chest and abdomen , as in three of our cases . 
it is possible that nmv , mainly intermittent positive pressure ventilation delivered via a nasal , face or mouth mask ( nippv ) has several advantages in terms of avoiding barotrauma complications of invasive mv , probably reducing the number of icu admissions [ 26 ]  . 
 a review of our selected s - oiv patients shows that highrisk patients are more likely to have severe and complicated courses and that influenza virus infection may cause viral pneumonia with secondary bacterial infection and exacerbate underlying chronic illness . 
in our population , obesity appears to be an important risk factor for developing pneumonia , as in our experience 11 / 50 patients admitted si hanno lesioni dellepitelio respiratorio associate ad un aumento anomalo della permeabilit capillare , che producono inizialmente allimaging addensamenti a chiazze , con successiva evoluzione in opacit confluenti bilaterali da occupazione degli spazi aerei . 
la lesione al parenchima polmonare pu essere causata da infezioni , inalazione di tossici , traumi , barotrauma o emboli o indirettamente da una malattia extrapolmonare , come lo shock settico , la pancreatite o lo squilibrio metabolico . 
nei nostri pazienti lards stata associata ad un pattern di danno infiammatorio polmonare grave con coinvolgimento peribronchiale a distribuzione prevalentemente antigravitazionale ; gli alveoli nelle porzioni antideclivi dei polmoni , che si trovano anteriormente nel paziente in decubito supino , sono quindi pi suscettibili alla superinflazione ed alla rottura . 
 possibile pensare che la ventilazione meccanica non invasiva ( nmv ) , principalmente la ventilazione intermittente a pressione positiva attraverso una maschera nasale , al viso o alla bocca ( nippv ) abbia diversi vantaggi nellevitare le complicanze da barotrauma presenti nella ventilazione meccanica invasiva , probabilmente riducendo il numero di ricoveri in terapia intensiva [ 26 ]  . 
 [ 30 ] hanno rilevato che i segmenti polmonari interessati sono stati prevalentemente localizzati nei lobi inferiori e che erano presenti segni comuni alle due condizioni come il ggo , talvolta associato a consolidazione . 
 i nostri casi s - oiv selezionati dimostrano che in pazienti ad alto rischio pi probabile avere un decorso grave e complicato e che linfezione influenzale virale pu causare polmonite con infezione batterica secondaria e pu esacerbare una malattia cronica pregressa . 
nella nostra popolazione lobesit sembra essere stata un importante fattore di rischio per lo sviluppo della polmonite ; nella nostra esperienza 11 / 50 pazienti ricoverati in ospedale per polmonite virale erano obesi e 5 di loro hanno richiesto la ventilazione meccanica . 
in tre casi ( 6% ) abbiamo osservato nelle scansioni tc a strato sottile il segno dellatollo o dellalone invertito o rhs , che definito come uniperdensit centrale ggo circondata da una consolidazione anulare di spessore minimo di 2 mm estesa ad almeno i tre quarti della circonferenza della lesione [ 12 ] ; prima della 182 radiol med ( 2012 ) 117 : 165184 to hospital for viral pneumonia were obese ; five of them required mv . 
in three cases ( 6% ) , we observed on thinsection ct the atoll or reversed halo sign ; this is defined as a central region of ggo surrounded by a dense ring of consolidation forming more than three fourths of a circle of at least 2 - mm thick [ 12 ] ; before the formal description of this sign [ 31 ] , the terms crescentic and ring - shaped opacities were used [ 32 ]  . 
histologically , the central ggo area corresponds to alveolar septal inflammation and cellular debris , whereas the outside ring or crescent represents granulation tissue within the alveoli and bronchioles [ 32 ]  . 
 this sign is very suggestive of organising pneumonia ( op ) and is likely quite specific for that diagnosis , although it is only seen in one fifth of patients with the disease [ 3235 ]  . 
 other lung diseases may be associated with significant components of op , and the reversed halo sign has been described in other conditions , such as pulmonary zygomycosis [ 36 , 37 ] , pulmonary small - vessel vasculitis [ 38 ] , wegeners granulomatosis [ 39 ] , lymphomatoid granulomatosis [ 40 ] , sarcoidosis [ 41 , 42 ] and pulmonary tuberculosis [ 43 , 44 ]  . 
 these findings indicate that the reversed halo sign may be seen in patients with active infection and is therefore not specific for cryptogenic op ; however , we consider its presence an indicator of components of op or of an association of viral infection and thromboembolic disease , as reported by the university of michigan series [ 8 ]  . as a limitation in our study , we encountered some technical imaging limitations due to the severity of patient illness ; in these cases , ct was performed without contrast material ( mostly owing to progressing acute renal failure ) , and we could not evaluate the association of viral infection with pulmonary embolism . descrizione formale di questo segno [ 31 ] , stato utilizzato il termine opacit semilunare e ad anello [ 32 ]  . 
istologicamente , larea centrale di vetro smerigliato corrisponde allinfiammazione setto - alveolare ed a detriti cellulari , mentre lanello esterno o semiluna rappresenta il tessuto di granulazione allinterno degli alveoli e dei bronchioli [ 32 ]  . 
questo segno molto suggestivo di polmonite in organizzazione ( po ) ed ha elevata specificit per questa diagnosi , anche se stato rilevato solo in un quinto dei pazienti con tale patologia [ 3235 ]  . 
altre malattie polmonari possono essere associate a componenti significative di po e il rhs stato recentemente descritto in altre condizioni , quali zigomicosi polmonare [ 36 , 37 ] , la vasculite dei piccoli vasi polmonari [ 38 ] , la granulomatosi di wegener [ 39 ] , la granulomatosi linfomatoide [ 40 ] , la sarcoi dosi [ 41 , 42 ] , la tubercolosi polmonare [ 43 , 44 ]  . 
 questi risultati indicano che il segno alone invertito pu essere trovato in pazienti con infezione attiva e pertanto non specifico per po criptogenetica ( cop ) , ma dobbiamo considerarlo come un indicatore di una componente di polmonite in organizzazione o come risultato dellassociazione di uninfezione virale con la malattia tromboembolica , come segnalato da un lavoro delluniversit del michigan [ 8 ]  . nella nostra casistica il maggior limite dellimaging , a causa della grave condizione clinica dei pazienti , stato il mancato utilizzo del mdc ev ( per lo pi a causa della progressione dellinsufficienza renale acuta ) e cos non si potuta valutare leventuale associazione dellinfezione con lembolia polmonare . 
 conclusioni conclusions the most common radiological findings in patients with influenza a ( h1n1 ) pneumonia are unilateral or bilateral ggo with or without associated focal or multifocal areas of consolidation . 
radiologists should be aware of cxr and ct findings of this viral infection so that the diagnosis of novel influenza a ( h1n1 ) pneumonia should be promptly considered . in conclusione , i segni radiologici pi comuni in pazienti affetti da polmonite influenzale a ( h1n1 ) sono il groundglass unilaterale o bilaterale con o senza aree focali o multifocali di consolidazione . 
knauth springer - verlag berlin heidelberg , 2011 issn : 0942 - 5373 isbn : 978 - 3 - 642 - 01739 - 1 e - isbn : 978 - 3 - 642 - 01740 - 7 published online : 21 october 2011 springer - verlag 2011 this book is entirely devoted to the impact on clinical practice induced by dual energy computed tomography ( dect ) , describing in full detail the advances in this domain offered by the introduction of the newest machines , more robust hardware and post - processing dedicated software . the book is divided into six parts : physical implementation ( 5 chapters discussing the different approaches to the physical and technical problems and solutions offered by the vendors ) ; vascular system ( 4 chapters : head and neck , aorta , peripheral arteries , plaque differentiation ) ; thoracic imaging ( 4 chapters : lung perfusion , lung ventilation , pulmonary nodule and lung cancer , myocardial perfusion ) ; neurological imaging ( 1 chapter : neurological applications ) ; abdominal imaging ( 4 chapters : liver imaging , kidney imaging , pancreas , kidney stones ) ; extremities ( 2 chapters : tendons and ligaments , gout )  . due to its ability to differentiate between spectral molecular substances , dect offers radiologists and clinicians the possibility to identify and define pathologic tissues and substances at the core of the disease . very nice examples of this ability are given , for instance , kidney stone characterization ( to avoid unnecessary interventions ) or gout diagnosis , not to mention plaque differentiation or pulmonary nodules . due also to its ability to create virtual non contrast images , dect is able to substantially reduce dose radiation to patients , most of all in those who need follow - up examinations , such as after endovascular aneurysm repair surgery . 
 this is an important book which will be of great interest to all those approaching , using and mastering dect , who will make good use of the extensive practical experquesto volume dedicato esclusivamente allimpatto sullattivit clinica prodotto dalla tomografia computerizzata a doppia sorgente ( tcds ) , descrivendo in ogni dettaglio i progressi verificatisi in tale campo con lintroduzione di attrezzature pi avanzate , dotate di pi potenti hardware e di programmi dedicati di rielaborazione delle immagini . 
 il volume diviso in sei parti : implementazione fisica ( 5 capitoli discutono i diversi approcci ai problemi fisici e tecnici e le rispettive soluzioni offerte dallindustria ) ; sistema vascolare ( 4 capitoli : capo e collo , aorta , arterie periferiche , differenziazione delle placche ) ; studio per immagini del torace ( 4 capitoli : perfusione polmonare , ventilazione polmonare , noduli e tumore del polmone , perfusione miocardica ) ; studio per immagini del sistema nervoso ( 1 capitolo : applicazioni neurologiche ) ; estremit ( 2 capitoli : tendini e legamenti , gotta )  . data la sua intrinseca capacit di differenziare tra gli spettri molecolari delle sostanze , la tcds offre , sia ai radiologi che ai clinici , la possibilit di identificare e definire i tessuti patologici che sono alla base del processo morboso . vengono forniti esempi assai significativi di questa capacit diagnostica , per esempio nella caratterizzazione dei calcoli delle vie urinarie ( potendosi cos evitare interventi chirurgici inutili ) o nella diagnosi della gotta , per non parlare della differenziazione delle placche o dei noduli polmonari . 
 valendosi poi della sua capacit di creare immagini virtuali senza contrasto , la tcds offre anche la capacit di ridurre sostanzialmente la dose radiante ai pazienti , soprattutto in quelli che necessitano di controlli periodici , come , per esempio , dopo interventi di riparazione chirurgica endovascolare degli aneurismi . 
 dunque , volume importante , che sar di grande interesse per tutti coloro che si avvicinano , usano o sono gi esperti della tcds , che faranno buon uso di tutta lesperienza pra336 radiol med ( 2012 ) 117 : 335336 tise in the text from all contributing authors . 
colagrande1 1department of clinical physiopathology , section of radiodiagnostics , university of florence , azienda ospedaliero - universitaria careggi , viale morgagni 85 , 50134 florence , italy 2section of medical physics , azienda ospedaliero - universitaria careggi , florence , italy 3 cirm , university of florence , azienda ospedaliero - universitaria careggi , florence , italy 4department of diagnostic for imaging , 1st radiology , spedali civili of brescia , italy 5center for systemic manifestations of hepatitis viruses ( masve ) , department of internal medicine , university of florence , florence , italy correspondence to : s . 
twenty - eight patients were evaluated with abdominal mr - dwi from march to november 2010 : seven healthy volunteers , seven patients with chronic liver disease f0f2 ( metavir score ) , seven f3f4 child - pugh a , and seven f4 child - pugh bc , classified as groups 14 , respectively . 
dwi acquisitions were performed during breath - holding ( b = 0150 s / mm2 and 1 , 000 ) and free breathing ( multi - b = 0200400 6008001 , 000 s / mm2 )  . 
using a double - blind control procedure , two observers estimated adc , d , and f by applying a region of interest ( roi ) in 4 / 12 sections in the middlelower portion of the right hepatic lobe . 
a reduction in the mean value of f , adc150 and , to a lesser extent , adc1 , 000 is shown to progress from healthy volunteers ( group 1 ) to cirrhosis patients ( group 4 ) , with wide overlap among groups . 
da marzo a novembre 2010 sono stati valutati con rm 28 soggetti : 7 sani , 7 epatopatici cronici f0 - f2 secondo metavir , 7 f3 - f4 child a e 7 f4 child b - c , denominati gruppi i - ii - iii - iv rispettivamente . 
sono state eseguite acquisizioni dwi a respiro sospeso ( b = 0150 e 1000 s / mm2 ) e libero ( poli - b = 02004006008001000 s / mm2 )  . 
there is therefore the need to develop methods for detection , risk stratification and prognosis and therefore techniques in which findings can be integrated or even supersede those obtained with invasive procedures such as measuring hepatic vein pressure gradient ( hvpg ) and biopsy . 
the limitations of the latter lie in the possible complications ( > 0.3% , a mortality risk of 0.018% ) [ 3 ] , poor representation ( it evaluates only 1 / 50 , 000 of the parenchyma ) and the equivocal reading in cases of intermediate fibrosis [ 46 ]  . 
several years ago , magnetic resonance diffusionweighted imaging ( mr - dwi ) was proposed as a potential noninvasive instrument for evaluating and monitoring the degree of fibrosis in chronic liver disease . 
at first , there were great expectations , given the sensitivity of the dwi technique in detecting the growing barrier to the movement of water molecules produced by progression of parenchymal fibrosis . 
this interpretation was at least in part refuted by an elegant experiment conducted by annets group on rats [ 12 ] , which demonstrated that the reduced adc found with disease progression appeared mostly linked to concomitant changes in perfusion and therefore to the microcirculation . 
on the other hand , it has been known for some time [ 19 ] and emphasised in a recent commentary [ 20 ] that dwi can discriminate between the roles played by diffusion and perfusion in a certain tissue . 
the aim of this prospective study was to evaluate whether and which of the dwi parameters adc , diffusion ( d ) or perfusion fraction ( f ) correlates with the progression of chronic liver disease and whether there may be a possible clinical application . la cirrosi epatica un crescente problema di salute pubblica mondiale , per il costante invecchiamento della popolazione e il diffondersi del virus dellepatite c , con conseguenti problemi di morbilit cronica , mortalit e spese sempre pi rilevanti per i servizi sanitari nazionali [ 1 , 2 ]  . 
per questi pazienti , si avverte quindi il bisogno di sviluppare metodi di identificazione , stratificazione del rischio e prognosi , e quindi di tecniche che permettano di superare o almeno integrare i risultati ottenuti tramite procedure invasive come la misurazione del gradiente pressorio trans - epatico ( hepatic vein pressure gradient , hvpg ) e la biopsia . 
questa mostra i suoi limiti nelle possibili complicanze ( maggiori nello 0 , 3% , con rischio di mortalit dello 0 , 018% ) [ 3 ] , la scarsa rappresentativit ( valuta solo 1 / 50000 del parenchima ) e nella lettura non univoca dei gradi intermedi di fibrosi [ 46 ]  . 
la misura del grado di fibrosi rappresenta infatti il pi importante predittore di progressione di malattia che condiziona le scelte terapeutiche , pu servire per valutare la risposta al trattamento e determina prognosi e follow - up del paziente . 
alcuni anni orsono , fu proposto lo studio con diffusione in risonanza magnetica ( rm - dwi ) quale potenziale strumento non invasivo per la valutazione ed il monitoraggio del grado di fibrosi epatica in corso di epatopatia cronica . 
in un primo momento si sono manifestate notevoli aspettative , spiegate con la sensibilit della tecnica dwi a rilevare il crescente ostacolo al movimento delle molecole di acqua determinato dalla progressione della fibrosi parenchimale . 
 annet sui ratti [ 12 ] , dove si dimostrato che la riduzione delladc evidenziata al progredire della malattia , appariva maggiormente legata alle concomitanti alterazioni perfusionali e quindi alla microcircolazione , argomento ripreso successivamente in studi condotti su volontari sani ed epatopatici cronici [ 13 , 14 ]  . 
daltra parte nota da tempo [ 19 ] e ribadita in un recente commento [ 20 ] , la possibilit di discriminare tramite dwi il contributo diffusivo da quello perfusivo in un determinato tessuto . 
 si evince pertanto che leventuale ruolo del dwi nello studio delle epatopatie diffuse ancora dibattuto : scopo di materials and methods 244 patients between march and november 2010 , mr was used to evaluate 30 consecutive patients with chronic liver disease in various stages of progression and cirrhosis . 
the patients presented at our department for their routine check - up as part of their diagnostictherapeutic workup , to evaluate liver disease progression and confirm the presence of any new - onset focal lesions suspected at screening with ultrasound ( us ) and alpha - fetoprotein ( afp )  . 
of the 21 remaining patients , seven had histologically diagnosed chronic liver disease ( with biopsy performed not more than 3 months before the mr examination ) classified according to the metavir score ( f0f4 ) [ 21 , 22 ] ; 14 had a clinical diagnosis ( in two cases also histological ) of cirrhosis , of which seven were child - pugh ( cp ) class a and seven in cp classes b and c . 
we also studied seven healthy volunteers , using mr - dwi , who were chosen from among interns and physicians working in our department there was therefore no need for local ethics committee approval of the protocol , as patients were studied as regional referrals for clinicaldiagnostic investigation according to normal clinical procedure ( patient privacy was maintained and the therapeutic pathway was not changed )  . 
 the aim and the nature of our study were explained to the patients involved , and each provided written informed consent prior to beginning the examination , in compliance with the principles of the declaration of helsinki ( edinburgh revision , 2000 )  . 
in total , therefore , the study enrolled 28 patients divided into four groups , each comprising seven individuals : group 1 , healthy volunteers ( age range 2640 years , mean 32 years ) ; group 2 , patients with chronic liver disease classified as f0f1f2 ( low - grade f , age range 4576 years , mean 55 years ) ; group 3 , patients with chronic liver disease classified as f3 and f4cp a ( high grade f and / or low cp , age range 5072 years , mean 64 years ) ; group 4 , patients classified as f4cp b and c ( high grade f and high cp , age range 4770 years , mean 54 years )  . 
healthy volunteers all had a negative history for alcohol or drug abuse , systemic diseases , hepatic viral infection and focal or diffuse hepatic lesions at the us study performed prior to mr . 
in addition , liver function blood tests were all within normal limits ( for volunteers , we used routine examinations done as part of the radiation protection medical examination )  . mr imaging mr examinations were performed using a superconducting radiol med ( 2012 ) 117 : 242253 questo studio prospettico quello di valutare se e quale fra i parametri adc , coefficiente di diffusione ( d ) e frazione di perfusione ( f ) , correli con il progredire del grado dellepatopatia cronica e se possa esistere una possibile applicazione clinica . materiali e metodi pazienti da marzo a novembre 2010 sono stati valutati con rm 30 pazienti consecutivi per epatopatia cronica in vari stadi evolutivi e cirrosi . 
i pazienti si sono presentati presso il nostro dipartimento per il routinario controllo previsto dal loro iter diagnostico - terapeutico , per la valutazione evolutiva della patologia epatica e per la conferma di eventuali lesioni focali di nuova insorgenza sospettate allo screening con ecografia e alfa - fetoproteina ( afp )  . 
non stata quindi necessaria lapprovazione del protocollo da parte del comitato etico locale , in quanto i pazienti giungevano alla nostra osservazione per un controllo clinico - diagnostico con richiesta regionale secondo la normale procedura clinica ( la privacy dei pazienti stata mantenuta e liter terapeutico non ha subito variazioni )  . 
lo scopo e la natura dello studio sono stati spiegati ai soggetti coinvolti , ognuno dei quali ha fornito il consenso scritto prima di iniziare lesame , in conformit con i principi della dichiarazione di helsinki ( revisione di edimburgo , 2000 )  . 
a four - element phased - array surface coil was used and positioned to cover the entire upper abdomen in the supine position , with arms extended above the head to reduce blood - flow artefacts . 
in addition to the standard sequences for studying the abdomen with and without contrast material ( the healthy volunteers only underwent the noncontrast and dwi study ) , which is not described here , the study protocol included three supplementary dw sequences with varying b - values as follows : 1 . 
the orientation of the diffusion gradient , defined by the option gradient overplus ( philips medical systems ) is intermediate to the orthogonal axes of the gradients . selective fat saturation was systematically used to reduce chemical - shift artefacts . 
after application of the dw sequence , a set of images corresponding to each b - value was obtained , and in the dw breath - hold sequences , an adc map calculated automatically by the scanner console was also obtained . 
to validate the accuracy of our system , as suggested [ 16 ] , a preliminary study on a phantom was done with the application at room temperature of a diffusion sequence , as described in a previous study [ 23 ]  . image analysis a radiologist and a physicist with 4 years and 3 years of liver dwi experience , respectively , and who were blinded to della rm , abuso di alcol o droghe ; inoltre gli indici ematici di funzionalit epatica risultavano nei limiti di norma ( per i nostri volontari si sfruttavano gli esami eseguiti di routine per la visita medica di radioprotezione )  . imaging rm gli esami rm sono stati effettuati utilizzando un tomografo a risonanza 1 , 5 t superconduttivo ( gyroscan nt intera release 12 , philips , eindhoven , paesi bassi ; massima intensit dei gradienti 30 mt / m )  . 
stata impiegata una bobina phasedarray di superficie a 4 elementi , posizionata a coprire tutto laddome superiore del soggetto , che giaceva in posizione supina , con le braccia estese sopra la testa per ridurre gli artefatti legati alla pulsatilit vascolare . 
il protocollo prevedeva , oltre alle normali sequenze standard per lo studio delladdome superiore senza e con mezzo di contrasto ( mdc ) ( i volontari sani sono stati sottoposti solo alla valutazione diretta e dwi ) , che pertanto non descriveremo , tre sequenze supplementari pesate in diffusione a vari valori di b , i cui parametri sono riportati di seguito : 1 . 
due acquisizioni eco - planari ( echo planar imaging , epi ) single - shot , respiro sospeso , con valori di b rispettivamente 0150 s / mm2 e 01000 s / mm2 , tempo di ripetizione [ tr ] / tempo di eco [ te ] = 1949 / 61 e 2438 / 70 ms , epi factor = 65 , spessore / numero di strati = 9 mm / 12 , gap = 1 mm , flip angle = 90 , fattore sense 2 , field of view [ fov ] = 300420 mm , numero di medie del segnale ( nsa ) = 2 , tempo di acquisizione = 20 s , half scan factor 62% , larghezza di banda 1535 hz , rectangular field fo view [ rfov ] 70% , phase scan percentage 74% , voxel di acquisizione ( mm3 ) 3 , 32 / 4 , 50 / 9 , 00 , voxel di ricostruzione ( mm3 ) 1 , 33 / 1 , 33 / 9 , 00 , matrice di acquisizione 12865 , matrice di ricostruzione 320220 ; 2 . 
una acquisizione epi single - shot , respiro libero , valori di b crescente : 0 , 200 , 400 , 600 , 800 , 1000 s / mm2 , tr / te = 2000 / 66 ms , epi factor = 65 , spessore / numero di strati = 9 mm / 12 , gap = 1 mm , flip angle = 90 , fattore sense 2 , fov = 300420 mm , nsa = 2 , tempo di acquisizione = 2 min 12 s , half scan factor 73% , larghezza di banda 1739 hz , rfov 70% , phase scan percentage 73% , voxel di acquisizione ( mm3 ) 3 , 32 / 4 , 50 / 9 , 00 , voxel di ricostruzione ( mm3 ) 1 , 33 / 1 , 33 / 9 , 00 , matrice di acquisizione 12865 , matrice di ricostruzione 320220 . considerando la gi dimostrata isotropia del fegato [ 18 ] , stata applicata una sola direzione di gradiente di diffusione in ogni acquisizione , in modo da ridurre il tempo di eco al valore minimo disponibile e di conseguenza la pesatura t2 della sequenza dw . 
lorientamento del gradiente di diffusione , definito dalla opzione gradient overplus ( philips medical systems ) , intermedio agli assi ortogonali dei gradienti . 246 radiol med ( 2012 ) 117 : 242253 the diagnosis analysed the images . 
disagreement between readers was resolved with a joint evaluation in consensus with the assistance of a third operator , the study coordinator , who has 11 years of liver dwi experience . 
liver sampling , done on both the dwi images and the relative adc maps , was conducted by placing a region of interest ( roi ) , drawn freehand , on four adjacent sections of the 12 acquisitions , in the middleinferior portion of the right lobe , where the reproducibility and repeatability of the measures are the best , as already shown [ 23 ]  . 
the size of each roi was around 1 , 500 pixels per section ( for a total of around 6 , 000 pixels ) , and each was drawn taking care to exclude artefacts and major vessels . 
image analysis was performed using the mricro software application ( 1.40 build 1 , chris rordens mricro , university of south carolina , columbia , sc , usa )  . 
mean values of the roi directly represent adc values when the adc maps were obtained with the two sequences at 150 s / mm2 and 1 , 000 s / mm2 , whereas they correspond to the dwi signal decay in the case of the multi - b sequence . calculation of the d and f parameters pseudodiffusion parameter d * was not calculated because the series of b - values was too large to obtain the parameter with acceptable uncertainty . 
as a result , given the documented influence of d * only in regimens of low diffusion weighting ( b < 150 s / mm2 ) [ 20 , 24 ] , a signal decay model was used in the interval of b - values between 200 and 1 , 000 s / mm2 , which only takes into account the diffusion d . 
the mathematical model of signal decay is monoexponential and is expressed by the equation : where both the diffusion coefficient d and the perfusion fraction f appear , whereas s and s0 represent , respectively , the signal with and without dw , and b is the sensitisation factor . 
associated with the random movement of water molecules due to thermal agitation ; f represents the fraction of water molecules present within the capillary bed ; and 1 - f represents the fraction external to the microcirculation . 
per validare laccuratezza del nostro sistema , come suggerito da un recente lavoro [ 16 ] , stato effettuato uno studio preliminare su fantoccio applicando , a temperatura ambiente una sequenza in diffusione , secondo quanto descritto in un precedente studio [ 23 ]  . analisi delle immagini lanalisi delle immagini stata effettuata in cieco rispetto alla diagnosi da un radiologo e da un fisico , entrambi con esperienza in dwi epatica rispettivamente di 4 e 3 anni . 
in caso di disaccordo fra lettori , stata ottenuta una valutazione comune in consensus con lausilio di un terzo operatore , il coordinatore dello studio , con 11 anni di esperienza in dwi epatica . 
il campionamento del fegato , effettuato sia sulle immagini dwi che sulle relative mappe adc , stato condotto posizionando una regione di interesse ( roi ) , disegnata a mano libera su quattro sezioni contigue delle 12 acquisite , nella porzione medio - inferiore del lobo di destra , dove la riproducibilit e la ripetibilit delle misure sono migliori , come dimostrato da un recente lavoro [ 23 ]  . 
 la dimensione di ciascuna roi era di circa 1500 pixel per sezione ( per un totale di circa 6000 pixel ) ed ognuna stata disegnata avendo cura di escludere artefatti e grandi vasi . 
i valori medi delle roi rappresentano direttamente i valori di adc nel caso delle mappe ottenute con le due sequenze a 150 s / mm2 e 1000 s / mm2 , mentre corrispondono al segnale di decadimento dwi nel caso della sequenza poli - b . calcolo dei parametri d ed f in questo studio lindagine non ha compreso il calcolo del parametro di pseudodiffusione d * , a causa dellutilizzo di una serie con valori multipli di b troppo grandi per poter ottenere tale parametro con incertezza accettabile . 
di conseguenza , data la documentata influenza del d * solo in regimi di bassa pesatura in diffusione ( b < 150 s / mm2 ) [ 20 , 24 ] , stato utilizzato un modello di decadimento del segnale , nellintervallo dei valori di b da 200 a 1000 s / mm2 , che tiene conto solo della diffusione d . 
il modello matematico di deradiol med ( 2012 ) 117 : 242253 statistical analysis for each group , the mean , standard deviation ( sd ) and 95% confidence intervals ( ci ) were calculated for the parameters d , f and adc ( from the maps with b 150 and 1 , 000 s / mm2 , hereinafter indicated respectively by adc150 and adc1 , 000 , considering the breath - hold sequences alone )  . 
significant differences between means of the different groups were calculated using a parametric test based on analysis of variance ( anova ) , preceded by the levene test to verify the homogeneity of variances between groups . 
the anova test showed the following statistically significant differences ( p < 0.05 ) between groups : = ( 1 f ) exp ( b d ) cadimento del segnale monoesponenziale ed espresso dallequazione : dove compaiono sia il coefficiente di diffusione d che la frazione di perfusione f , mentre s ed s0 rappresentano , rispettivamente , il segnale con e senza pesatura in diffusione , mentre b il fattore di sensibilizzazione . 
in tale equazione d rappresenta il coefficiente di diffusione , ovvero legata al movimento random delle molecole dacqua dovuto alla agitazione termica , f rappresenta la frazione di molecole dacqua presenti allinterno del letto capillare , 1 - f quella esterna al microcircolo . 
loperazione di fitting stata effettuata con il programma originlab v.8. analisi statistica per ogni gruppo sono state calcolate media , ds e limiti di concordanza al 95% dei parametri d , f e adc ( dalle mappe a b = 150 e 1000 s / mm2 , in seguito indicati rispettivamente con adc150 e adc1000 , considerando le sole acquisizioni a respiro sospeso )  . 
per determinare differenze significative tra le medie nei diversi gruppi , stato eseguito un test parametrico basato sullanalisi della varianza ( anova ) preceduto dal test di levene per la verifica della omogeneit delle varianze fra i gruppi . 
media e ds di coefficiente di diffusione apparente ( adc ) 150 , adc1000 , diffusione ( d ) ( espressi come10 - 6 mm2 / s ) e frazione di perfusione ( f ) per ciascun gruppo di pazienti iii 2483290 127091 1168108 0 , 180 , 04 2296275 1229120 1120103 0 , 170 , 04 2114268 123984 117079 0 , 130 , 05 1923153 114355 111380 0 , 120 , 02 adc150 adc1 , 000 adc150 adc1000 ds , deviazione standard ; adc apparent diffusion coefficient ; d , diffusion ; f perfusion fraction 248 radiol med ( 2012 ) 117 : 242253 fig . 
even with a large overlap among the four groups , a decrease is visible in the values of adc150 ( a ) , adc1 , 000 and f ( less prominent ) ( b , d ) with increasing degree of chronic liver disease , without correlation with d ( c )  . 
the introduction of fibroscan has significantly reduced the number of liver biopsies , such risultati i risultati delle misure di adc in fantoccio , ottenuti da serie ripetute di una sequenza poli - b ( 2001000 s / mm2 ) hanno dato una ripetibilit di circa 0 , 7% . 
stata riscontrata una riduzione del valor medio di f , delladc150 e , in misura minore , delladc1000 al progredire da i verso iv ; al contrario non stata osservata alcuna variazione statisticamente significativa di d . 
i gruppi sono risultati omogenei per le varianze e quindi nessuna correzione stata radiol med ( 2012 ) 117 : 242253 that histological findings in patients with chronic liver disease are hard to come by [ 2528 ]  . 
these include patients physical and constitutional characteristics , such as obesity and intestinal gas , which hamper the propagation of the elastic wave ; and pathological conditions concerning either the liver , such as haemochromatosis , fatty liver and intermediate degrees of fibrosis , or of other organs , such as pleural effusion or ascites . 
there is therefore a real need for noninvasive techniques that will provide useful information regarding the progression of chronic liver disease , thus avoiding the need for liver biopsy [ 16 ]  . 
 several years ago , when fibroscan did not have the validation that it does today , a number of papers were published on the clinical applications of dwi in patients with chronic liver disease [ 711 ]  . 
the authors suggest that there is a variation in adc between normal and cirrhotic individuals of no more than 300400 u ( expressed in 10 - 6 mm2 / s ) at b 01 , 000 s / mm2 [ 11 , 17 ] , with lesser differences between the various stages of disease ( around 100 u of adc at b 01 , 000 s / mm2 ) [ 11 ]  . 
the fact that this difference between healthy and cirrhotic livers is not so great should be evaluated in the light of the ample dispersion of the adc measurements [ 11 , 14 , 17 , 23 ]  . 
even under optimal conditions , the sd of the averages is in fact not less than 15% , which is around 200 u ( 10 - 6 mm2 / s ) at b 1 , 000 s / mm2 , a difference that therefore spans the adc interval between healthy and cirrhotic livers . 
it is also worth noting that the best results in stratifying the degree of fibrosis using adc are obtained with low b - values ( b 128 s / mm2 ) , as shown in the study by koinuma et al . 
the weighting on the d parameter , instead , increases with increasing b : it is significant above values of 200 s / mm2 and becomes crucial above 500 s / mm2 . 
this study showed that the reduction in adc values observed in rats with carbontetrachloride - induced cirrhosis correlates to a greater extent with a reduction in hepatic infusion rather than a restriction in free diffusion . 
in fact , the differences noted in the in vivo study are less apparent when the examination is repeated at a constant temperature immediately after the animal has been sacrificed . 
it is also known that the nodular transformation of the liver , the vascularisation of the sinusoids and the increase in fibrosis progresses , reduces portal and total apportata ai dati . 
lanova test ha evidenziato le seguenti differenze statisticamente significative ( p < 0 , 05 ) tra gruppi : adc150 : gruppi i , ii , iii verso iv , gruppo i verso ii e gruppo i verso iii ; adc1000 : gruppi i , ii , iii verso iv ; f : gruppi i , ii , verso iii , iv . discussione il diffondersi dellepatopatia sclerogena ha portato allo sviluppo di tecniche diagnostiche non invasive quale strumento di identificazione e stratificazione del grado di fibrosi , fondamentale per la prognosi e leventuale terapia . 
fra i test non invasivi disponibili , si sta sempre pi affermando la misurazione del grado di fibrosi mediante la elastometria ad impulsi ultrasonori ( fibroscan ) , tecnica che consente di valutare la risposta elastica del parenchima in kilopascal ( liver stiffness ) [ 25 , 26 ]  . 
lintroduzione del fibroscan ha ridotto notevolmente il numero di biopsie epatiche , tanto che attualmente non facile poter disporre di un riscontro istologico in pazienti con epatopatia cronica [ 2528 ]  . 
va peraltro fatto notare che tale metodica , seppur preziosa , inficiata da vari fattori , dipendenti sia dalle caratteristiche fisiche e costituzionali del paziente quali obesit e meteorismo intestinale che ostacolano il propagarsi dellonda elastica , sia inerenti condizioni patologiche epatiche quali lemocromatosi , la steatosi , i gradi intermedi di fibrosi e non epatiche come il versamento pleurico o ascitico . 
pertanto si sente forte la necessit di poter disporre di metodiche non invasive in grado di fornire informazioni utili sullo stadio evolutivo dellepatopatia cronica , senza dover ricorrere alla biopsia epatica [ 16 ]  . 
alcuni anni orsono , quando il fibroscan non aveva ancora le attuali validazioni , sono stati pubblicati vari articoli a proposito delle applicazioni cliniche del dwi nel paziente epatopatico cronico [ 711 ] , il razionale dei quali era rappresentato dallassunto che il grado di restrizione alla libera diffusione delle molecole di acqua era proporzionale al progredire della sclerosi parenchimale . 
da tali articoli si evince che esiste una variazione di adc fra pazienti normali e cirrotici di non pi di 300400 unit ( espresse come 10 - 6 mm2 / s ) a b = 01000 s / mm2 [ 11 , 17 ] con differenze naturalmente minori fra i vari stadi di malattia ( 100 unit di adc a b = 01000 s / mm2 ) [ 11 ]  . 
la ds delle medie infatti , nelle migliori condizioni , non inferiore a 15% , circa 200 unit ( 10 - 6 mm2 / s ) a b = 1000 s / mm2 , una differenza quindi sovrapponibile allintervallo di adc fra sani e cirrotici . 
di qui il limite e , a nostro avviso , la spiegazione 250 radiol med ( 2012 ) 117 : 242253 della mancata applicazione della tecnica in ambito clinico [ 11 , 14 , 17 , 22 ]  . 
 peraltro interessante ricordare che i risultati migliori nella stratificazione dei gradi di fibrosi tramite adc sono stati ottenuti a valori di b bassi ( b = 128 s / mm2 ) , come per esempio nello studio di koinuma et al . 
 [ 10 ] , mentre noto che la pesatura sul parametro d cresce con il b : significativa sopra valori di 200 s / mm2 , per essere poi determinante sopra 500 s / mm2 . 
annet [ 12 ] , dove si evince che la diminuzione dei valori di adc osservata nei ratti , nei quali era stata farmacologicamente indotta la cirrosi tramite la somministrazione di tetracloruro di carbonio , correla per lo pi con la riduzione della perfusione epatica piuttosto che con la restrizione alla libera diffusione . 
 daltra parte noto che al progredire della trasformazione nodulare del fegato , della capillarizzazione dei sinusoidi , dellincrementare della fibrosi , si osserva una riduzione del flusso portale e totale del fegato , con tentativo di compenso tramite incremento del flusso arterioso ( meccanismo definito tampone , tramite il quale il fegato tenta di mantenere lomeostasi circolatoria ) [ 3234 ]  . con studi dwi si ha la possibilit di stimare in modo almeno semi - quantititivo alcuni parametri legati alla perfusione ( f e d * ) [ 20 , 35 ]  . 
in vivo , la prima parte della curva , a bassi valori di b , influenzata dai moti ivim non diffusionali ( f e d * ) , ovvero la variazione dellintensit di segnale con b dipende in larga parte dal flusso nel microcircolo capillare , orientato in tutte le direzioni . 
la seconda parte della curva , a valori di b pi elevati , invece influenzata dai moti ivim di diffusione pura ( d )  . da questa descrizione discende uninteressante considerazione che differenzia in modo sostanziale i due parametri legati alla perfusione . 
mentre il d * , che appare pi legato alla portata , deriva dallinterpolazione dei valori raccolti a basso b , il parametro f , che esprime lentit del let to capillare , viene descritta nel modello fisiologico proposto [ 17 , 19 ] dal punto di intersezione con lasse delle ordinate della funzione monoesponenziale ottenuta tramite il fit dei soli punti a b alti ( 200 s / mm2 )  . 
pertanto , mentre il d * dipende fortemente dai bassi b ed pi esposto allerrore di misura , il parametro f , pur essendo correlato al flusso , appare maggiormente dipendente dagli alti b e fig . 
b ( s / mm2 ) compared between healthy liver parenchyma and an isotropic phantom in a multi - b acquisition [ 23 ] : bi - exponential decay of the healthy liver curve , with respect to the monoexponential decay of isotropic medium [ 19 ]  . 
b ( s / mm2 ) tra parenchima epatico sano e fantoccio isotropo a multi - b [ 23 ] : si evidenzia landamento biesponenziale della curva relativa al parenchima epatico sano , rispetto a quello monoesponenziale del mezzo isotropo [ 19 ]  . 
tale differenza da imputarsi ai moti ivim perfusionali . flow in the liver , with an attempt at compensation via increased arterial flow ( a mechanism defined buffer response , by which the liver attempts to maintain its circulatory homeostasis ) [ 3234 ]  . dwi study enables the semiquantitative estimate of several parameters associated with perfusion ( f and d * ) [ 20 , 35 ]  . 
in vivo , the first part of the curve is , at low b - values , influenced by nondiffusional intravoxel incoherent motion ( ivim ) ( f and d * ) , i.e. 
 the second part of the curve , at higher b - values , is , instead , influenced by the ivim of pure diffusion ( d )  . this description suggests a substantial underlying difference in the two parameters associated with perfusion . 
d * , which appears to be linked to flow , is derived from the interpolation of values gathered at low b - values ; the f parameter , which expresses the extent of the capillary bed , corresponds in the proposed physiological model [ 17 , 19 ] to the intersection point with the ordinate axis of the monoexponential function obtained by fitting only the high b - value points ( > 200 s / mm2 )  . 
therefore , whereas d * largely depends on radiol med ( 2012 ) 117 : 242253 low b - values and is more open to measurement error , the f parameter , despite being correlated with flow , appears to be more dependent on high b - values and therefore less open to measurement error . as there are few studies to our knowledge that deal with this issue , we compared healthy volunteers and patients with chronic liver disease ( both cirrhotic and noncirrhotic ) to verify whether the progression of fibrosis is more closely correlated with ivim diffusion or perfusion parameters . 
nonetheless , the latter reported a moderate reduction in d with disease progression , which we failed to confir this difference can be explained by considering the different acquisition techniques used . 
in our study , there was also a reduction in the mean value of adc150 with disease progression , which confirms and explains the results obtained in koinuma et al.s study [ 10 ]  . 
 the adc150 parameter is strongly influenced by the weighting in d * , so it is understandable that the differences appear more sensitive . in addition , when evaluating the robustness of our results , it worth noting the dispersion of values of the parameters calculated with dwi ( adc , d and f ) in healthy individuals , with values in the literature varying from a minimum of 870 / 960 / 15 to a maximum of 2 , 040 / 1 , 380 / 40.29 [ 11 , 13 , 14 , 17 , 23 ] , respectively , for adc / d / f ( adc and d expressed in 10 - 6 mm2 / s and f in % )  . 
in addition , analysis of our results shows that there is a great deal of overlap in values among the different groups ; therefore , this technique is not suitable for stratifying fibrosis for clinical purposes . the main limitations of our study are the small number of enrolled individuals , which nonetheless is comparable with other studies [ 9 , 11 , 13 , 17 , 37 , 38 ]  . 
the failure to estimate d * may seem to be a second limitation , but as explained above , this parameter is notoriously open to major error , and investigating it would require giving priority to low b - values and forgoing reaching b 1 , 000 s / mm2 . 
finally , the four groups were significantly different in terms of age , although this is not a limitation in that it has recently been shown that there is no correlation between adc and age [ 39 , 40 ]  . quindi meno esposto allerrore di misura . su queste basi , il nostro intento , con pochi analoghi in letteratura per quanto a noi noto , stato quello di verificare su pazienti epatopatici cronici ( cirrotici e non ) a confronto con volontari sani , se il progredire della fibrosi era maggiormente correlabile ai parametri ivim di diffusione o di perfusione . 
nel nostro studio abbiamo riscontrato una modesta ma significativa correlazione fra il progredire della malattia ed il ridursi del valore di f , mentre non stata osservata alcuna correlazione col valore di d , confermando che quanto veniva riportato nei primi lavori era da imputarsi prevalentemente a variazioni di perfusione , come poi confermato da studi pi recenti [ 17 ]  . 
 da notare che anche altri autori riportano correlazione con i parametri di perfusione [ 15 ] ; tuttavia nella loro esperienza la correlazione con il d * e quindi con un parametro legato alla portata . 
nel nostro lavoro si osserva inoltre una riduzione del valor medio delladc150 col progredire della malattia , che conferma e spiega i risultati ottenuti nel gi citato studio di koinuma et al . 
il parametro adc150 risente abbastanza della pesatura in d * e quindi si capisce perch appaiano pi sensibili le differenze . inoltre , per valutare la robustezza dei risultati qui riportati , utile sottolineare in primo luogo quanto sia grande la dispersione dei valori dei parametri calcolati con dwi ( adc , d ed f ) in soggetti sani , con valori in letteratura variabili da un minimo di 870 / 960 / 15 ad un massimo di 2040 / 1380 / 40.29 [ 11 , 13 , 14 , 17 , 23 ] rispettivamente per adc / d / f ( adc e d espressi 10 - 6 mm2 / s e f in % )  . 
inoltre lanalisi dei risultati ci fa notare lampia sovrapposizione dei valori fra i vari gruppi e quindi come questa tecnica non possa essere attualmente proponibile per una stratificazione ad uso clinico della fibrosi . le principali limitazioni del nostro studio riguardano il numero non cospicuo di soggetti arruolati , che comunque paragonabile a quello riportato in altri lavori [ 9 , 11 , 13 , 17 , 37 , 38 ] ; peraltro i nostri soggetti sono stati stratificati in 4 gruppi e non solo in due , per meglio valutare landamento dei parametri . 
la mancata stima del d * potrebbe sembrare un secondo limite del lavoro , ma abbiamo sopra spiegato che questo parametro notoriamente esposto a grande errore e per indagarlo avremmo dovuto privilegiare i pi bassi b , rinunciando a salire fino a b = 1000 s / mm2 . 
infine i 4 gruppi di soggetti arruolati differiscono significativamente per classe di et , ma questo non un limite allo studio , in quanto stato recentemente dimostrato che non esiste correlazione fra valore di adc ed et [ 39 , 40 ]  . 252 radiol med ( 2012 ) 117 : 242253 in conclusion , our study confirms that dwi does not enable the stratification of chronic liver patients for clinical purposes . 
however , in the per - group analysis , the technique demonstrates a tendency towards a reduction in perfusion - associated parameters with worsening chronic liver disease , without an associated change in diffusion parameters . concludendo , il nostro lavoro conferma che studi dwi non permettono una stratificazione ad uso clinico dei pazienti epatopatici cronici , ma mostrano una tendenza , nella valutazione per gruppi , alla riduzione dei parametri legati alla perfusione con laumentare del grado di epatopatia sclerogena , senza che questa sia evidenziabile nei parametri connessi alla diffusione . acknowledgements the present research study was performed with the contribution of the italian society of medical radiology ( sirm )  . 
cademartiri1 , 2 1cardiovascular imaging , giovanni xxiii clinic , monastier ( tv ) , italy 2department of radiology and cardiology , erasmus medical center , rotterdam , the netherlands 3sdn foundation irccs , naples , italy 4department of radiology , university of verona , verona , italy 5department of radiology , university of ferrara , ferrara , italy correspondence to : f . 
cademartiri , cardiovascular imaging , giovanni xxiii clinic , via giovanni xxiii 7 , 31050 monastier ( tv ) , italy , tel . : + 39 - 0422 - 8961 , fax : + 39 - 0422 - 898051 , e - mail : filippocademartiri@gmail.com received : 9 november 2010 / accepted : 14 april 2011 / published online : 18 november 2011 springer - verlag 2011 abstract purpose . 
using a 50 - hu threshold , 12 ( 7.2% ) plaques would be classified as lipid rich on arterial scan compared with 28 ( 17% ) on the delayed - phase scan . 
nei segmenti con aterosclerosi coronarica , stata misurata lattenuazione ( hu ) del lume coronarico , delle componenti calcifica e non calcifica delle placche aterosclerotiche e del tessuto adiposo epicardico adiacente . 
utilizzando una soglia di 50 hu , 12 ( 7 , 2% ) placche sarebbero state classificate come lipidiche nella fase arteriosa , contro 28 ( 17% ) nella fase tardiva . 
la classificazione delle placche coronariche come lipidiche o fibrose sulla base dei valori assoluti di attenuazione significativamente influenzata dallattenuazione vascolare e dalle soglie di densit utilizzate per la definizione . parole chiave angiografia coronarica con tomografia computerizzata classificazione delle placche caratterizzazione delle placche attenuazione delle placche introduction introduzione identification of rupture - prone atherosclerotic plaque to prevent adverse cardiovascular events is the topic of ongoing research [ 13 ]  . 
several studies have demonstrated an association between plaque ct attenuation ( measured in hounsfield units , hu ) and the histopathological composition or their appearance on intravascular imaging techniques [ 410 ] and have suggested that ctca may allow differentiation of potentially vulnerable lipid rich and fibrous plaques , which are assumed to be more stable . 
however , intracoronary contrast enhancement has been shown to affect measured attenuation of plaque material [ 1113 ] , which could have implications for the use of absolute attenuation values to differentiate lipid and fibrous coronary plaque . 
fibrous coronary plaque definition are under evaluation , and there is no standardised approach in the scientific community . the aim of the study was to investigate in vivo the effect of vascular attenuation and density thresholds on attenuation values of noncalcified coronary plaque components and their impact on plaque classification as lipid rich vs . 
molti studi hanno dimostrato come vi sia una associazione tra i valori di attenuazione della tomografica computerizzata ( tc ) della placca ( misurati in unit hounsfield , hu ) e la composizione istopatologica o le sue caratteristiche identificate utilizzando metodiche di indagine endo - vascolari [ 410 ] , e suggeriscono che la ctca possa essere in grado di differenziare le placche vulnerabili lipidiche da quelle fibrose , riconosciute come pi stabili . 
sia i valori di attenuazione vascolare che le soglie di densit di riferimento per la definizione della placca lipidica piuttosto che fibrotica sono oggetto di valutazione e non esiste un approccio standardizzato nella comunit scientifica . lo scopo di questo studio di valutare leffetto dellattenuazione vascolare e delle soglie di densit sui valori di attenuazione della componente di placca coronarica non calcifica e , quindi , limpatto sulla classificazione della placca lipidica piuttosto che fibrotica . 
 we prospectively enrolled 30 patients [ 25 men , mean age 598 ; mean body mass index ( bmi ) 274 ] with stable angina pectoris in a crossover study . 
only patients with stable angina , in sinus rhythm with a heart rate < 65 bpm ( spontaneous or beta - blocker induced ) , who had never materiali e metodi popolazione trenta pazienti ( maschi 25 ; et 598 anni ; indice di massa corporea [ bmi ] medio 274 ) con angina stabile sono stati 232 radiol med ( 2012 ) 117 : 230241 undergone percutaneous coronary intervention or bypass surgery and who were able to hold their breath for 12 s were included . 
our institutional review board approved the study protocol , and all patients gave written informed consent . scan protocol and image reconstruction all scans were performed with on a 64 - slice ct scanner ( sensation 64 cardiac , siemens , forchheim , germany )  . 
a 100 - ml bolus of contrast material ( iomeprol 400 mg / ml ; iomeron , bracco , italy ) was injected through an antecubital vein at 46 ml / s . 
 for the first ( standard arterial phase ) scan , a bolus - tracking technique with saline chaser was used to synchronise the arrival of contrast in the coronary arteries with scan initiation [ 15 ]  . 
reconstruction parameters for the ecg - gated images were field of view 100 mm , effective slice thickness 0.6 mm and slice increment 0.3 mconvolution kernel filtering was the same for the two scans : mediumsmooth ( b30f )  . 
solo i pazienti con ritmo sinusale ( spontaneo o indotto mediante somministrazione di beta - bloccanti ) , mai sottoposti ad angioplastica percutanea o ad intervento chirurgico per il posizionamento di by - pass e capaci di trattenere il respiro per almeno 12 s , sono stati inclusi nello studio . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . protocollo di scansione e di ricostruzione delle immagini per lo studio mediante tc stato utilizzato uno scanner a 64 strati ( somatom , siemens , forchheim , germania )  . 
i parametri di scansione utilizzati sono stati : numero di strati per rotazione 3220 , 6 mm , tempo di rotazione del gantry 330 ms , table feed 2 , 84 mm / rotazione , pitch 0 , 2 , risoluzione temporale 165 ms , voltaggio del tubo radiogeno 120 kv , potenza del tubo radiogeno 700900 mas [ 14 ]  . 
 per la prima scansione ( fase arteriosa standard ) stata utilizzata una tecnica di bolus - tracking con chaser di soluzione salina al fine di sincronizzare larrivo del contrasto nelle arterie coronarie con linizio della scansione [ 15 ]  . 
 i parametri di ricostruzione per le immagini sincronizzate con lelettrocardiogramma erano : campo di vista 100 mm , spessore effettivo dello strato 0 , 6 mm , incremento di ricostruzione 0 , 3 mil filtro / kernel di convoluzione stato il medesimo per due scansioni : medium - smooth ( b30f )  . 
i dataset sono stati ricostruiti in diverse fasi del ciclo cardiaco nella fase meso - / tele - diastolica ( 450 ms / - 300 ms ) per ottenere la migliore qualit di immagine . 
dopo aver identificato i segmenti coronarici prossimali e intermedi ( vale a dire i segmenti 1 , 2 , 5 , 6 , 7 , 11 , 12 , 16 in accordo con classificazione fornita dallamerican heart association classification [ 16 ] ) , loperatore ha identificato la presenza di placca coronarica aterosclerotica , definita come ispessimento della parete coronarica ben distinguibile dal radiol med ( 2012 ) 117 : 230241 lumen , ( 2 ) the noncalcified plaque component , ( 3 ) the calcified plaque component if present , and ( 4 ) the surrounding epicardial fat . 
to account for the impact of neighbouring calcifications , we performed a subanalysis for mixed and noncalcified plaques . each measured plaque ( both for mixed and noncalcified plaques ) was classified as fibrous when attenuation was 30 hu and lipid rich when attenuation was < 29 hu ( threshold = 30 hu )  . 
intraand interobserver variability was assessed by calculating the coefficient of variability ( equal to the sd of the difference between two measurements over the mean of the two measurements , expressed as percentage )  . results both scans were completed successfully and without complications in all patients . 
i data - set angiografici e tardivi sono stati visualizzati e valutati in parallelo mediante le modalit di visualizzazione convenzionali utilizzate dalloperatore ( window width 700 hu ; window level 140 hu )  . 
essendo pi agevole lidentificazione dei margini nella fase arteriosa , questultima stata utilizzata per prima per il posizionamento delle roi ; quindi sono state posizionate le roi nella fase tardiva . 
per tenere conto dellimpatto delle calcificazioni coronariche , abbiamo effettuato una sottoanalisi per le placche miste e per quelle non calcifiche . ogni placca ( mista o non - calcifica ) stata classificata come fibrotica se il valore di attenuazione era 30 uh , lipidica se < 29 uh ( soglia = 30 uh )  . 
lintervallo medio tra la somministrazione del mezzo di contrasto e la fase arteriosa stato di 18 , 53 , 1 s , quello con la fase tardiva stato di 48 , 15 , 5 s . 
 la prevalenza di malattia coronaria significativa ( stenosi 50% ) risultata pari al 76 , 7% ( 23 pazienti )  . 234 table 1 measured computed tomography ( ct ) attenuation values ( hounsfield units ) on arterial and delayed - phase ct scans . 
la media dei valori di attenuazione tcds in hu misurata a livello del lume coronarico , della componente di placca calcifica e non calcifica e nel tessuto epicardio circostante , stratificata per placca di composizione mista e per placca esclusivamente non calcifica scansione arteriosa scansione tardiva placche totali placca mista ( n = 167 ) ( n = 116 ) strutture lume componente non calcifica componente calcifica tessuto epicardico circostante 91 , 024 , 0 321 , 368 , 2 * 135 , 771 , 4 * 564207 327 , 471 , 3 * 148 , 373 , 1 * 564207 90 , 223 , 5 placca esclusivamente non calcifica ( n = 49 ) placche totali placca ( n = 167 ) mista ( n = 116 ) placca esclusivamente non calcifica ( n = 49 ) 307 , 058 , 6 * 106 , 257 , 9 * n / a 92 , 925 , 4 168 , 248 , 6 * 97 , 353 , 0 * 559233 99 , 931 , 0 178 , 039 , 4 * 111 , 450 , 5 * 559233 99 , 333 , 6 145 , 459 , 7 * 64 , 443 , 4 * n / a 101 , 424 , 3 * p < 0 , 05 in colonna ; p < 0 , 05 in riga n / a , non applicabile ( 12% ) , segment 12 = 24 ( 14% )  . 
higher noncalcified plaque attenuation was associated with higher luminal contrast attenuation [ r = 0.41 ; 95% confidence interval ( ci ) 0.3210.499 ; p < 0.01 : pooled data from all plaques in arterial and delayed phases ]  . 
la valutazione di placca stata eseguita su entrambe le scansioni mostrando la seguente distribuzione coronarica : segmento 1 = 24 ( 14% ) , segmento 2 = 22 ( 13% ) , segmento 5 = 16 ( 10% ) , segmento 6 = 30 ( 18% ) , segmento 7 = 30 ( 18% ) , segmento 11 = 21 ( 12% ) , segmento 12 = 24 ( 14% )  . 
 dal confronto dei dati , il lume vasale ha mostrato valori di attenuazione tc significativamente pi elevati se confrontati a quelli delle placche non calcifiche ( p < 0 , 001 ) , eccetto che per quelle calcifiche ( p > 0 , 05 )  . 
inoltre , sta ta trovata una buona correlazione tra lelevata opacizzazione del lume vasale in fase arteriosa e lelevato valore di attenuazione della placca non calcifica ( r = 0 , 41 [ 95% intervallo di confidenza , ci , 0 , 3210 , 499 ] ; p < 0 , 01 : da ti aggregati di tutte le placche nella fase arteriosa e tardiva )  . 
 la figura mostra le differenze tra lattenuazione della placca in fase arteriosa e tardiva per tutti i tipi di placca ( a ) , per placca mista ( b ) , e per placca non calcifica ( c )  . 
 reproducibility valori di attenuazione per la placche miste rispetto a quelle non calcifiche le componenti di placca non calcifica adiacenti ai depositi di calcio ( placche miste ) hanno mostrato una attenuazione significativamente pi elevata sia nella fase arteriosa che in quella tardiva rispetto alle placche esclusivamente non calcifiche ( p < 0 , 01 )  . 
la correlazione tra lattenuazione del lume coronarico e le componenti non calcifiche delle placche miste risultata scarsa sia nella fase arteriosa ( r = 0 , 19 ) che in quella tardiva ( r = 0 , 20 )  . 
utilizzando una soglia di 50 hu , 12 ( 7 , 2% ) placche sarebbero state classificate come lipidiche nella fase arteriosa contro 28 ( 17% ) placche nella fase tardiva ( p < 0 , 05 )  . 
 una soglia di 70 hu avrebbe classificato 30 ( 18% ) placche come lipidiche nella fase arteriosa contro 53 ( 32% ) placche nella fase tardiva ( p < 0 , 05 )  . 
 riproducibilit la variabilit intra - osservatore per lanalisi dellattenuazione di placca stata dell8 , 2% , mentre la variabilit inter - osservatore stata del 12 , 3% . discussione la ctca pu aiutare potenzialmente a caratterizzare le placche aterosclerotiche coronariche [ 49 ]  . 
una recente meta - analisi eseguita su 14 studi e 340 pazienti ha dimostrato una sensibilit complessiva della ctca dell81%86% nella visualizzazione della placca coronarica , con una pi elevata sensibilit nella rilevazione della placca calcifica rispetto a quella non calcifica [ 9 ]  . 
studi mediante ctca effettuati in vitro ed ex vivo hanno dimostrato che le attenuazioni misurate a livello della parete vascolare mostrano valori intravascolari pi elevati ( per la pi elevata concentrazione di iodio ) [ 1113 ]  . 
tale fenomeno , gi precedentemente descritto come pseudo - opacizzazione [ 1719 ] , determinato da una scarsa risoluzione spaziale dovuta agli artefatti da volume parziale e da indurimento del fascio [ 20 ]  . 
la media pi elevata dei valori di attenuazione delle placche ( 38 hu ) stata osservata nella fase arteriosa , durante il picco di concentrazione di mezzo di contrasto intravascolare , rispetto a quella della fase tardiva quando lattenuazione del lume coronarico inferiore . diversi gruppi di ricerca hanno valutato la relazione tra lattenuazione in tc e lecogenicit con ecografia intravascolare ( ivus ) delle placche coronariche per differenziare le placche lipidiche da quella fibrotiche . 
le placche lipidiche e quelle fibrotiche , valutate sulla base dei reperti di ecogenicit ivus , corrispondevano a valori di attenuazione di 1426 hu e 9121 hu [ 4 ] , 4922 hu e 9122 hu [ 8 ] , e 5843 hu e 12134 hu [ 10 ] , rispettivamente . 
according to a recent metaanalysis of 14 studies and 340 patients , overall sensitivity for detecting coronary plaque was 8186% , with better sensitivity for calcified compared with noncalcified plaques [ 9 ]  . 
in - vitro and ex - vivo ctca studies demonstrated that the measured attenuation values of the vascular wall are affected by high intravascular attenuation as a result of high iodine concentrations [ 1113 ] , a phenomenon previously described as pseudoenhancement [ 1719 ] , caused by insufficient spatial resolution resulting in partial voluming and beam - hardening artefacts [ 20 ]  . 
utilizzando una soglia di 70 hu , stato osservato lo spostamento di 23 placche da fibrotica in fase arteriosa a lipidica in fase tardiva fase arteriosa lipidica , n ( % ) fibrotica , n ( % ) 238 radiol med ( 2012 ) 117 : 230241 fig . 
 the average measured ct attenuation values of noncalcified plaque was 38 hu higher on arterial - phase ct images during peak contrast - medium concentration in coronary arteries compared with delayed - phase ct images when contrast concentrations in the coronary arteries are lower . 
lipid rich and fibrous plaque , as interpreted from the ivus images based on echogenicity , corresponded with plaque attenuation values of 1426 and 9121 hu [ 4 ] , 4922 and 9122 hu [ 8 ] and 5843 and 12134 hu [ 10 ] , respectively . 
we decided to apply the three different thresholds ( 30 , 50 and 70 hu ) to provide a spectrum of possible solutions that may be applied in clinical practice . 
in this study , depending on the applied threshold ( 30 , 50 or 70 hu ) the number of lipid rich plaques was 857% higher on delayed - phase scan confronto dei valori di attenuazioni delle placche lipidiche rispetto a quelle fibrotiche riportati in letteratura , difficile stabilire nella pratica clinica il cut - off dei valori di attenuazione da utilizzare per la classificazione di placca aterosclerotica . 
sulla base dei dati pubblicati in letteratura [ 4 , 8 , 10 ] , nel nostro studio le placche sono state classificate come lipidiche ( valori di attenuazione al di sotto della soglia ) o fibrose ( valori di attenuazione al di sopra della soglia ) sulla base di tre differenti soglie di densit ( 30 hu , 50 hu e 70 hu )  . 
la prevalenza di placche lipidiche valutata sulla base dei valori soglia utilizzati ( 30 hu , 50 hu o 70 hu ) stata dell8%57% , con maggior incidenza nelle scansioni tardive rispetto a quelle arteriose . 
leffetto dellattenuazione intra - vascolare stato maggiore in presenza di placche non calcifiche , probabilmente a causa dei valori medi di attenuazione inferiori ed un maggiore differenza di attenuazione tra il lume intracoronarico e la placca . 
i pi elevati valori di attenuazione misurati a livello della componente non calcifica nelle placche miste potrebbero essere spiegati dalla presenza di piccoli spot di calcio nel contesto della componente apparentemente non calcifica , cos come dallo pseudo - enhancement causato dalle adiacenti calcificazioni . 
the effect of luminal contrast enhancement was stronger for exclusively noncalcified plaques , which may be explained by the lower average plaque attenuation values and larger contrast between lumen and plaque . 
the higher measured attenuation values of noncalcified plaque material in mixed plaques could be explained by small calcium particles within the seemingly noncalcified material , as well as pseudoenhancement caused by the proximity of calcified plaque . 
 highly attenuating tissue causes a shift towards highenergy levels within the polychromatic roentgen spectru high - energy photons are less attenuated , causing shadowing behind high - attenuation structures , such as metal , calcium and contrast - enhanced coronary lumen . 
motion during data acquisition causes blurring and appears to aggravate beam - hardening artefacts , which mostly affect bordering image elements and are magnified by the small size and continuous motion of coronary arteries . 
based on our observation that plaque attenuation values strongly depend on arterial contrastenhancement levels as well as proximity of calcifications , consideration and perhaps correction of absolute measurements based on these aspects may improve classification of plaque as high ( lipid rich ) or low ( fibrous ) risk . 
i fotoni ad elevata energia subiscono una minor attenuazione , causando una velatura dietro le strutture ad elevate attenuazione , come nel caso dei metalli , del calcio , e nel lume coronarico dopo somministrazione di mezzo di contrasto . 
in tale contesto , giocano un ruolo importante gli effetti da volume parziale ( la media pesata dei valori di attenuazione dei diversi tessuti contenuti allinterno di un elemento dellimmagine ) , gli algoritmi di ricostruzione e i filtri di convoluzione utilizzati che determinano una riduzione o accentuazione dei contrasti tissutali , alterando anche i valori di attenuazione delle placche adiacenti a strutture con elevata densit . 
gli artefatti fin qui menzionati , riguardanti soprattutto i bordi degli oggetti nellimmagine , vengono ingigantiti in presenza di strutture di piccole dimensioni e dal continuo movimento delle arterie coronarie . 
in particolare , la caratterizzazione di placca mediante tc , includendo la misurazione dei bassi valori di attenuazione tc , un predittore di eventi cardiovascolari avversi [ 23 , 24 ]  . 
sulla base delle nostre osservazioni , la consapevolezza della forte dipendenza dei valori di attenuazione della placca dal grado di opacizzazione vascolare , cos come dalla vicinanza di calcificazioni , induce a relative considerazioni ed eventuali correzioni sui valori assoluti di attenuazione da utilizzare per migliorare la classificazione di placca come ad alto rischio ( lipidica ) o a basso rischio ( fibrosa )  . 
per studi futuri e per un imaging seriale il pi possibile riproducibile , la valutazione delle considerazione fatte finora potrebbe migliorare la misurazione dei valori di attenuazione , per esempio partendo da condizioni di imaging comparabili . 
infatti , paradossalmente , i valori di attenuazione della placca potrebbero essere pi realistici in assenza di agente di contrasto e se il sangue e la parete vasale avessero valori di attenuazione simile . 
 limitazioni per ottimizzare e minimizzare leffetto della dose di radiazioni , lo studio stato eseguito su una piccola coorte di pazienti ad elevato rischio cardiovascolare , limitando la 240 limitations to optimise and minimise overall radiation exposure , we performed our study is a small cohort of high risk patients and restricted our assessment to the ( clinically most relevant ) larger coronary segments , thereby avoiding excessive interference by additional artefacts . 
as the aim of our study was to evaluate the effect of differences in luminal contrast enhancement on plaque - attenuation values , with each participant acting as his or her own control , we did not perform a comparison to invasive imaging . 
finally , radiation exposure as a general limitation to cardiac ct needs to be mentioned , although contemporary equipment and scan methods allow data acquisition at significantly lower radiation doses [ 2527 ]  . 
 radiol med ( 2012 ) 117 : 230241 valutazione ai segmenti coronarici di maggiori dimensioni ( sulla base della rilevanza clinica ) , per evitare eventuali sviste dovute agli artefatti . 
il nostro studio , infatti , stato effettuato per valutare leffetto dellattenuazione vascolare sulla base dei valori di attenuazione tc della placca misurati su immagini tc e per classificare la tipologia di placca sulla base di valori soglia di densit fissati arbitrariamente . 
infine , la dose di radiazione rappresenta ancora il principale limite della ctca , sebbene le pi innovative apparecchiature e modalit di scansione permettano lacquisizione dei dati con valori di dose significativamente inferiori rispetto al passato [ 2527 ]  . 
in particolare , la classificazione della componente non calcifica della placca come materiale lipidico o fibrotico eseguita sulla base dei valori assoluti di attenuazione tc varia con i pi bassi livelli di opacizzazione vascolare . 
from january 2003 to january 2009 , 29 patients ( 36 lung lesions ) were treated with rfa ; from january 2007 to january 2009 , 16 patients ( 17 lung lesions ) were treated with mwa . 
scopo del presente studio stato analizzare retrospettivamente le complicanze registrate nel trattamento termo - ablativo con radiofrequenze ( rfa ) e con microonde ( mwa ) di tumori polmonari , confrontarli con i dati riportati in letteratura e valutare i fattori di rischio correlati alle due procedure . 
da gennaio 2003 a gennaio 2009 , 29 pazienti ( 36 lesioni polmonari ) sono stati trattati con rfa ; da gennaio 2007 a gennaio 2009 , 16 pazienti ( 17 lesioni polmonari ) sono stati trattati con mwa . 
in accordo con i dati presenti in letteratura , lo pneumotorace la complicanza pi frequente anche se la sua incidenza nella nostra casistica pi bassa ( 5 , 8% versus 4 , 3%18% in letteratura )  . 
la termo - ablazione percutanea , sia rfa che mwa , rappresenta unottima opzione terapeutica in termini di sicurezza e tolleranza . 202 radiol med ( 2012 ) 117 : 201213 parole chiave radiologia interventistica lesioni polmonari maligne termo - ablazione microonde radiofrequenza complicanze revisione introduction introduzione the surgical approach to lung malignancies represents the first therapeutic choice [ 1 ]  . 
various ablation techniques have been developed over the years , including ethanol ablation , laser ablation , cryoablation and radiofrequency ablation ( rfa ) [ 2 , 3 ]  . 
it offers all the benefits of rfa as well as some substantial advantages , such as reduced procedure times , efficacy on lesions with cystic components and / or in proximity to vascular structures , reduced heat - sink effect and less intraprocedural pain [ 4 , 5 ]  . rfa and mwa of lung lesions can also lead to some complications [ 6 , 7 ]  . 
the aim of this study was to retrospectively review the complications recorded during our experience with percutaneous rfa and mwa of lung tumours , to compare them with data reported in the literature and to assess the risk factors related with the procedures . materials and methods patients il trattamento di prima scelta per le lesioni maligne del polmone tuttora rappresentato dalla chirurgia . 
ci nonostante solo il 20% delle lesioni risulta chirurgicamente resecabile [ 1 , 2 ] ; questo ha portato allo sviluppo di tecniche alternative alla chirurgia come ad esempio i trattamenti ablativi che permettono un controllo locale di questo gruppo di lesioni [ 2 , 3 ]  . 
nel corso degli anni varie tecniche ablative sono state sviluppate e proposte , dall iniezione di etanolo , alla crioablazione , allablazione con il laser e mediante radiofrequenza ( rfa ) , questultima attualmente quella di pi largo impiego [ 2 , 3 ]  . 
 le microonde sono in grado di fornire tutti i benefici della radiofrequenza con in pi alcuni sostanziali vantaggi come tempi di ablazione pi brevi , efficacia anche in lesioni di tipo cistico od in lesioni in prossimit di grossi vasi senza essere gravate dallheat sink effect e con un minore dolore intra - procedurale per il paziente [ 4 , 5 ]  . lutilizzo della radiofrequenza e delle microonde nel trattamento di lesioni polmonari pu comunque essere associato alla comparsa di alcune complicanze . 
complicanze documentate in letteratura ma pi rare sono : enfisema sottocutaneo , lesioni del sistema nervoso periferico , tumor seeding , ascessi , polmoniti ed infezioni [ 5 , 912 ]  . 
lo scopo di questo studio retrospettivo quello di analizzare le complicanze registrate nella nostra esperienza nel trattamento di lesioni polmonari con rfa e mwa , compararle con i dati della letteratura e valutare i rischi associati a queste procedure percutanee . a retrospective study was conducted with the approval of the local ethics committee . 
in the mwa group , average age was 74.75 ( range 4084 ) years ; one patient in this group had two lesions , both treated in the same session . 
da gennaio 2003 a gennaio 2009 in 29 pazienti con 36 lesioni polmonari stata effettuata una termo - ablazione con radiofrequenza mentre in 16 pazienti con 17 lesioni polmonari stata eseguita una termo - ablazione con microonde . 
 in the rfa group , 19 / 29 patients were affected by nonsmall - cell lung carcinoma ( nsclc ) ; ten of them were defined as inoperable on the basis of disease stage ( iiia , n = 5 ; iiib , n = 5 ) ; of the remaining patients ( nine with nsclc and ten with metastases ) , eight were defined as inoperable due to advanced age , eight to comorbidities and three refused surgery . 
in the mwa group , patients were classified as inoperable for the following reasons : nine due to advanced stage ( iiib , n = 6 ; iiia , n = 3 ) , six due to comorbidities and one with metastases from advanced primary disease . 
written informed consent was obtained from all patients . baseline imaging pretreatment imaging consisted of a thoracic multidetectorrow ct ( mdct ) scan extending to the abdomen ( aquilion 64 , toshiba , japan ) with and without contrast administration . 
the contrastenhanced scans were acquired after injection of 100 ml of iodinated contrast agent ( visipaque 320 , ge healthcare , usa ) at an injection rate of 3 ml / s , followed by injection of 40 ml saline at a rate of 2 ml / s . 
 pretreatment procedure before the beginning of each procedure , local anaesthesia of the access site was achieved with a subcutaneous injection of a 10 - ml solution of 2% carbocaine . 
each patient was kept in a state of moderate sedation through intravenous administration of a combination of midazolam ( 0.070.08 mg / kg ) , propofol ( 0.52.0 mg / kg / h ) and fentanyl ( 12 g / kg )  . 
il gruppo di pazienti sottoposti a mwa presentava le seguenti caratteristiche : et media 74 , 7 anni ( range 4084 anni ) , lesioni con diametro medio di 3 , 75 cm ( range 2 , 8 4 , 7 cm )  . 
una settimana prima del trattamento , tutti i pazienti sono stati sottoposti a prelievo bioptico con guida tomografica computerizzata ( tc ) con conseguente conferma istologica di malignit per tutte le lesioni . 
le lesioni con componente cistica od in prossimit dei grossi vasi sono state trattate quasi esclusivamente con le mwa ; questo grazie al fatto di poter utilizzare simultaneamente pi antenne e / o di poter evitare il furto di calore da parte delle strutture a contenuto liquido [ 4 ]  . 
in tutti i pazienti i valori di riferimento della coagulazione sono risultati nella norma , in quei pazienti che erano in trattamento con anticoagulanti , il farmaco stato sospeso 7 giorni prima del trattamento ablativo e , laddove necessario , sostituito con eparina . 
tutti i pazienti hanno firmato un consenso informato . metodiche di imaging prima del trattamento stata eseguita una tc del torace con scansione che si estendeva alladdome ( aquilion 64 , toshiba , giappone ) sia in condizioni basali che dopo somministrazione di mezzo di contrasto . 
le sequenze con mezzo di contrasto sono state acquisite dopo liniezione di 100 ml di contrasto iodato ( visipaque 320 , ge healthcare , usa ) con un flusso di 3 ml / s , seguito da un iniezione di 40 ml di soluzione fisiologia ad un flusso di 2 ml / s . procedure pre - ablazione prima dellinizio di ogni procedura ablativa stata eseguita 204 radiol med ( 2012 ) 117 : 201213 rate , electrocardiographic trace , oxygen saturation , respiratory frequency and blood pressure were continuously monitored throughout the procedure . 
 adequate antibiotic prophylaxis was achieved with intravenous administration of 1 g of cefazolin sodium ( ancef , smithkline beecham pharmaceuticals , philadelphia , pa , usa ) given every 8 h for 24 h , beginning shortly before the procedure . treatment with rfa in 24 of 36 sessions ( 24 / 36 lesions ) , the electrode was placed under ct fluoroscopy guidance , whereas in the remaining 12 sessions ( 12 / 36 lesions ) , the procedure was performed with xperguide cbct ( philips medical system , best , the netherlands )  . 
 treatment with mwa in 8 out of 17 sessions ( 8 / 17 lesions ) , the antenna was placed under ct fluoroscopy guidance , whereas in the remaining nine sessions ( 9 / 17 lesions ) , the procedure was performed with xperguide cbct ( philips medical system , best , the netherlands )  . 
an ablation system was used comprising a microwave generator ( evident microwave ablation system , covidien ltd ) capable of producing 45 w at 915 mhz , connected by coaxial cable to a 14.5 - gauge straight microwave antenna with a 3.7 - cm radiating section . 
 lesions with a maximum diameter 3 cm were treated with a single antenna , whereas in lesions with a maximum diameter > 3 cm , two antennae were simultaneously positioned at a distance of 1 cm from each other to achieve adequate necrosis . 
 on completion of the rfa or mwa procedure , technical success and immediate complications were checked with unanestesia locale , a livello del punto di accesso , mediante liniezione di 10 ml di soluzione al 2% di carbocaina . 
in tutti pazienti stata eseguita una sedazione moderata attraverso la somministrazione endovena di una combinazione di midazolam ( 0 , 070 , 08 mg / kg ) , propofol ( 0 , 52 , 0 mg / kg / h ) e fentanyl ( 12 g / kg )  . 
frequenza cardiaca , tracciato elettrocardiografico , ossimetria , frequenza respiratoria e pressione sanguigna sono stati monitorati costantemente durante tutta la durata della procedura con la presenza e lassistenza continua di un anestesista che ha assistito tutte le procedure . 
tutti i pazienti sono stati sottoposti a terapia profilattica antibiotica , con 1 g di cefazolina sodica ( ancef , smithkline beecham pharmaceuticals , philadelphia , usa ) , ogni 8 ore per 24 ore , iniziando poco prima della procedura . trattamento con rfa in ventiquattro casi su trentasei ( 24 / 36 lesioni ) , lelettrodo stato posizionato sotto guida fluoro - tc ; negli altri dodici casi ( 12 / 36 lesioni ) , la procedura stata effettuata con xperguide cbct ( philips medical system , best , paesi bassi )  . 
in tutte le procedure stato utilizzato un ago elettrodo coassiale le veen da 14 gauge ( diametro aperto 24 cm ) collegato ad un generatore da 200 w ( rf 3000 ; boston scientific corporation , san jose , ca , usa )  . 
le lesioni con diametro superiore a 4 cm ( 4 casi ) sono state trattate con un doppio posizionamento dellago elettrodo . trattamento con mwa in otto casi su diciassette ( 8 / 17 lesioni ) , lantenna stata posizionata sotto guida fluoro - tc , mentre negli altri nove casi ( 9 / 17 lesioni ) , la procedura stata effettuata con xperguide cbct ( philips medical system , best , paesi bassi )  . 
stato utilizzato un sistema di ablazione composto da un generatore di microonde ( microonde evident ablation system , covidien ltd . ) in grado di produrre 45 w a 915 mhz , collegato tramite un cavo coassiale ad unantenna a microonde da 14 , 5 gauge con una sezione di 3 , 7 c le antenne sono state continuamente perfuse con soluzione fisiologica ( 60 ml / min ) a temperatura ambiente per evitare possibili danni termici lungo lasse prossimale dellantenna . 
secondo le linee guida specifiche dellazienda produttrice , lablazione stata eseguita inserendo lantenna allinterno della lesione e mantenendo una potenza di 45 w per un tempo di ablazione totale di 10 minuti al fine di ottenere un volume di necrosi di circa 3 , 5 cm di diametro . 
 lesioni con diametro massimo 3 cm sono state trattate con una singola antenna , mentre lesioni con diametro massimo > 3 cm con due antenne posizionate contemporaneamente ad una distanza di 1 cm luna dallaltra al fine di ottenere un adeguata area di necrosi . radiol med ( 2012 ) 117 : 201213 ct fluoroscopy or with xperguide cbct . 
at 2 h from the procedure , each patient underwent chest radiography to evaluate the presence of early complications . follow - up all patients underwent ct follow - up with and without contrast administration at 1 , 3 , 6 , 12 and 18 months , in combination with complete blood and metabolic tests ; ct was then performed annually . 
contrastenhanced scans were obtained after administration of 100 ml of iodinated contrast agent ( visipaque 320 mgi / ml , ge healthcare ) injected at a rate of 3 ml / s , followed by 40 ml of saline solution at a rate of 2 ml / s . 
total volume of the ablated area was calculated with dedicated volume analysis software ( vitrea 2 , software 3.8 , vital images inc , minnetonka , mn , usa )  . efficacy , safety and complication frequency al termine di ogni procedura , eseguita sia sotto guida fluoro - tc che xperguide , stato eseguito un controllo tc per valutare il successo tecnico e le complicanze immediate . 
ciascun paziente , 2 ore dopo la procedura , stato sottoposto ad una radiografia del torace al fine di valutare leventuale presenza di complicanze precoci . follow - up tutti i pazienti sono stati sottoposti a tc di follow - up con e senza somministrazione di mezzo di contrasto a distanza di 1 , 3 , 6 , 12 e 18 mesi e ad esami ematochimici di laboratorio ; successivamente la tc stata eseguita annualmente . 
le scansioni con mezzo di contrasto sono state eseguite iniettando 100 ml di contrasto iodato ( visipaque 320 , ge healthcare ) ad una velocit di 3 ml / s seguito dalliniezione di 40 ml di soluzione salina ad una velocit di 2 ml / s . 
 le immagini sono state valutate secondo i criteri response evaluation criteria in solid tumors ( recist ) [ 13 ] ed il volume totale della zona di ablazione ( calcolata con il software di volume di analisi , vitrea 2 , software 3.8 , vital images inc , minnesota , usa )  . 
le complicanze sono state classificate in peri - procedurali ( quando si verificavano entro 30 giorni ) table 1 complication classification of percutaneous ablation of lung lesions according to the society of interventional radiology ( sir ) [ 6 , 7 , 15 ] adverse effects minor complications major complications a . 
death tabella 1 classificazione delle complicanze della termo - ablazione polmonare percutanea della societ di radiologia interventistica ( sir ) [ 6 , 7 , 15 ]  . effetti avversi complicazioni minori a . 
morte 206 radiol med ( 2012 ) 117 : 201213 classified as periprocedural ( when occurring within 30 days ) or delayed ( when occurring > 30 days ) and divided into side effects and major and minor complications in accordance with the classification proposed by the society of interventional radiology ( sir ) [ 6 , 7 , 15 ] ( table 1 )  . 
pain reported by patients after lung ablation was classified into four levels in accordance with the common toxicity criteria of the national cancer institute [ 19 ]  . systematic literature review a systematic literature review was performed in pubmed entrez using limits for dates , species and subsets : last 3 years , humans and medline , respectively . 
on 20 november 2010 , the following topics were searched : lung tumour radiofrequency , pulmonary tumour radiofrequency ablation and complications , lung tumour microwaves and pulmonary tumour microwave ablation and complications . o tardive ( quando si verificavano a pi di 30 giorni ) e distinte in effetti collaterali , complicanze maggiori e minori , secondo la classificazione elaborata dalla society of interventional radiology ( sir ) [ 6 , 7 , 15 ] descritte nella tabella 1 . 
il dolore riferito dai pazienti dopo ablazione del polmone stato classificato in 4 livelli secondo il common toxicity criteria del national cancer institute [ 19 ]  . revisione sistematica della letteratura tramite pubmed stata eseguita una revisione sistematica della letteratura degli ultimi 3 anni , utilizzando i limiti di data , specie e subsets ( rispettivamente ultimi 3 anni , esseri umani e medline )  . 
 the patient with residual tumour was treated with a second mwa session , but the result is beyond the scope of this la percentuale di successo in termini di efficacia stata del 94 , 4% . 
le 2 lesioni in cui la necrosi era stata incompleta sono state nuovamente trattate con 2 sessioni supplementari di ablazione , il cui risultato va oltre lo scopo di questo studio . 
linclusione di bolle aeree nel sito della lesione , noto come fenomeno della cavitazione , era presente in 6 dei 36 casi , ma successivamente scomparso nel giro di 6 mesi . 
after an initial increase in maximum diameter , there was a persistent reduction in diameter of the ablated areas at subsequent examinations , with a consolidation of the pulmonary parenchyma . 
the only major periprocedural complication consisted of a large apical pneumothorax requiring chesttube placement , which was associated with subcutaneous stato il riscontro di unarea a vetro smerigliato allinterno della lesione ablata e nei tessuti circostanti . 
dopo un iniziale aumento del diametro massimo , ai successivi controlli , si osservata una persistente riduzione del diametro delle zone di ablazione , consistente nel consolidamento del parenchima polmonare . 
durante il follow - up , la presenza di cavitazione stata osservata nel 47 , 1% dei casi ( 8 / 17 lesioni )  . complicanze trattamento con rf in 43 procedure eseguite in 36 lesioni tumorali del polmone , si sono registrate complicanze in 29 casi ( 67 , 4% ) , una delle quali ( 3 , 5% ) era una complicanza maggiore e 28 ( 96 , 5% ) erano effetti collaterali . 
dei 28 casi in cui si sono registrati effetti collaterali , in 16 ( 55 , 2% ) si trattava di una sottile falda di pneumotorace , risoltosi spontaneamente nel secondo - terzo giorno , in 4 ( 13 , 8% ) di piccole falde di 208 radiol med ( 2012 ) 117 : 201213 fig . 
the 28 side effects consisted of 16 ( 55.2% ) cases of small pneumothorax , which resolved spontaneously on days 2 and 3 , respectively ; four ( 13.8% ) small pleural effusions visible on conventional radiographs ; one ( 3.4% ) case of moderate grade ii chest pain treated with nonsteroidal anti - inflammatory drugs ( nsaids ) that resolved within a few hours ; five ( 17.2% ) cases of subcutaneous emphysema ; and two ( 6.9% ) cases of pleural reaction that resolved spontaneously . 
there were two cases of postablation syndrome . systematic review of the literature table 2 summarises the studies with the highest number of versamento pleurico visibile con radiogrammi convenzionali , in uno ( 3 , 4% ) di dolore toracico di grado moderato trattato con farmaci anti - infiammatori non steroidei ( fans ) e risolto in poche ore , in 5 ( 17 , 2% ) di enfisema sottocutaneo ed in 2 ( 6 , 9% ) di reazione pleurica risoltasi spontaneamente . 
 trattamento con mw delle 17 lesioni trattate , in quattro casi ( 23 , 5% ) si verificato pneumotorace di grado i , risolto spontaneamente entro il terzo giorno ed in 2 casi si osservata sindrome post - ablazione . risultati della revisione sistematica della letteratura nella tabella 2 sono riassunti gli studi con il maggior numero di pazienti e di tumori riguardo al trattamento con rf ed alle sue complicanze . 
nella tabella 3 sono riassunti gli studi con il maggior numero di pazienti e di tumori riguardo al trattamento con mw ed alle sue complicanze . radiol med ( 2012 ) 117 : 201213 table 2 systematic review of radiofrequency ablation complications in pulmonary tumours literature patients ( tumours ) , n major complications , % minor complications , % suzuki et al . 
table 3 summarises studies with the highest number of patients and tumours treated with mwa and complications related with treatment . discussione complicanze del trattamento con rf discussion rfa complications rfa of lung lesions is characterised by good morbidity ( 210% ) and mortality ( 0.092% ) rates in nonsurgical patients [ 18 ]  . 
furthermore , there are no lablazione con rf delle lesioni del polmone caratterizzata da un basso tasso di morbilit ( 2%10% ) e di mortalit ( 0 , 09%2% ) in pazienti non chirurgici [ 18 ]  . 
la rfa pu avere diversi vantaggi rispetto alla radioterapia standard o alla chemioterapia , come una sensibile riduzione del danno ai tessuti polmonari limitrofi e di conseguenza preserva maggiormente la funzionalit polmonare . 
inoltre , vengono risparmiati gli effetti collaterali sistemici della chemioterapia ; altri vantaggi per il paziente sono rappresentati dalla rapidit del trattamento e da una ospedalizzazione generalmente pi breve [ 10 ]  . 
la rfa riservata alle neoplasie giudicate non chirurgiche , in assenza di co - morbilit , come la broncopneumopatia cronica ostruttiva di grado severo [ 9 , 10 , 35 ]  . 
lenfisema grave 210 radiol med ( 2012 ) 117 : 201213 table 3 systematic review of microwave ablation complications in pulmonary tumours literature cases minor complications major complications durick et al . 
 [ 12 ] 8 swine ( 24 ablation zones ) 3 swine ( 18 ablation zones ) 9 patients ( 10 tumours ) 50 patients ( 82 tumours ; 66 sessions ) ~ 10% tabella 3 revisione sistematica delle complicanze della termo - ablazione con mw dei tumori polmonari autori casi complicazioni minori complicazioni maggiori durick et al [ 32 ] brace et al [ 33 ] carrafiello et al [ 34 ] wolf et al [ 12 ] 8 suini ( 24 zone di ablazione ) 3 suini ( 18 zone di ablazione ) 9 pazienti ( 10 tumori ) 50 pazienti ( 82 tumouri ; 66 sessioni ) ~10% ~30% ~30% systemic side effects , as with chemotherapy , and both the short treatment time and rapid recovery may result in better patient compliance [ 10 ]  . 
 [ 9 ] evidenced a statistical correlation of pneumothorax with male sex , no previous surgical lung interventions , multiple electrode insertions , tumour location in the middle or lower lobe , length of the electrode path and procedure duration [ 9 , 29 , 36 ] ; our results are in line with these findings . 
this is probably due to two factors : the use of a coaxial system that allows for more precise positioning of the needle and the injection of saline solution and anaesthetic at the pleural junction to obtain an increased thickness of extrapulmonary tissue and therefore greater stability . 
 [ 9 ] hanno messo in evidenza una correlazione statistica tra il rischio di pneumotorace e le seguenti condizioni : il sesso maschile , nessun precedente intervento chirurgico al polmone , lutilizzo di multipli elettrodi , la localizzazione del tumore nel lobo medio o nellinferiore , la lunghezza del percorso dellelettrodo , la durata della procedura [ 9 , 29 , 36 ] ; i nostri risultati sono in accordo con questi . 
questa bassa incidenza probabilmente dovuta a due fattori : luso di un sistema coassiale che permette un posizionamento pi preciso dellago e liniezione di soluzione fisiologica e di anestetico a livello della giunzione pleurica per ottenere un maggiore spessore del tessuto extrapolmonare da attraversare e quindi una maggiore stabilit . la soffusione pleurica rappresenta la seconda complicanza pi frequente , spesso con risoluzione spontanea e qualche volta associata a dolore al petto che viene trattato con analgesici [ 9 ]  . 
una complicanza minore come riportaradiol med ( 2012 ) 117 : 201213 pleural effusion represents the second most frequent complication , with spontaneous resolution and sometimes associated with chest pain treated with analgesics [ 9 ]  . 
in our experience , using the hot withdrawal technique is an established procedure , and no case of tumour seeding was recorded [ 10 ]  . mwa complications in the largest single - centre experience published [ 12 ] , no intraprocedural deaths occurred , and the overall 30 - day postablation mortality rate was 0% . 
 [ 12 ] was 39% ; of which 69% were classified as mild [ common terminology criteria for adverse events ( ctcae ) grade 1 ] and required no treatment . 
 conclusions further studies with a larger number of patients and treatments are required to confirm the preliminary data about the advantages of mwa and compare the complication to sia in letteratura che nella nostra esperienza lenfisema sottocutaneo , che nella maggior parte casi asintomatico . 
la stimolazione vagale pu produrre dolore in regione mandibolare , ai denti , al petto o agli arti superiori simile al dolore dovuto ad ischemia miocardica [ 2 ]  . 
nella nostra esperienza luso della tecnica di ritiro a caldo una procedura consolidata e non sono stati registrati casi di seeding [ 10 ]  . complicanze del trattamento con mw nella pi grande esperienza di singolo centro ad oggi pubblicata [ 12 ] , non stato registrato nessun caso di morte intra - procedurale e la percentuale di mortalit nei 30 giorni post - ablazione stata dello 0% . 
tra i pazienti presentati nello studio di wolf [ 12 ] , solo uno ( 2% ) ha presentato la sindrome post - ablazione ( ctcae grado 1 )  . 
 conclusioni sono necessari ulteriori studi con un numero maggiore di pazienti e di trattamenti per confermare i dati preliminari circa i vantaggi della termo - ablazione con mw e per paragonare la percentuale di complicanze post - mwa e postrfa . 
la nostra esperienza preliminare di ablazione con mw del tumore al polmone [ 34 ] ha mostrato un diametro medio della necrosi maggiore ( diametro medio 3 , 5 cm ) di quello ottenuto con rfa ( 1 , 7 cm ) [ 2 , 40 ] , in accordo con i 212 radiol med ( 2012 ) 117 : 201213 rates of rfa and mwa . 
our preliminary experience with mwa [ 34 ] showed a mean necrosis diameter ( 3.5 cm ) greater than that obtained with rfa ( 1.7 cm ) [ 2 , 40 ] , in agreement with the results reported by durick et al . 
safety evaluation shows that the 30 - day mortality rate ( 0% ) after mwa is markedly lower than after rfa ( 3.9% , 6 / 153 patients ) or after surgery ( 2.0% , 1 / 66 patients ) [ 2 , 41 ]  . in conclusion , both techniques report pneumothorax as the most common complication . 
mwa appears to be safer , free from the heat - sink effect and may be useful in tumours close to airways , arteries or veins [ 5 ]  . 
la valutazione della sicurezza delle microonde mostra che lincidenza di mortalit nei 30 giorni post - mwa ( 0% ) significativamente inferiore sia della incidenza di mortalit post - rfa ( 3 , 9% , 6 / 153 pazienti ) che di quella nel post - chirurgia ( 2% , 1 / 66 pazienti ) [ 2 , 41 ]  . in conclusione , per entrambe le tecniche lo pneumotorace rappresenta la complicanza pi comune . 
di conseguenza , si pu concludere che sia la mwa che la rfa rappresentano entrambe una scelta eccellente per lesioni con un diametro massimo inferiore a 3 c le lesioni di maggiori dimensioni possono esser trattate usando mw . 
la termo - ablazione con mw sembra essere pi sicura , non accompagnata dallheat sink effect , e pu essere utile nel trattamento di tumori vicini alle vie aeree o ai vasi [ 5 ]  . 
cesare 2 , 70124 bari , italy 3radiologia diagnostica per immagini , dimimp , universit di bari , bari , italy 4oncology unit , di venere hospital , bari , italy 5radiology unit , l . 
 [ 18f ] - fdg - pet / ct remains the best whole - body technique to identify lymph - node and skeletal lesions , but its limitation is identifying tumours with low glucose metabolism as in mucinous neoplasms . 
i risultati di questo studio retrospettivo dimostrano che la rm - dwibs pu essere utilizzata per studiare le localizzazioni parenchimali e scheletriche di neoplasia , ma che essa risulta meno efficacie nella caratterizzazione delle lesioni linfonodali . 
research has focused on methods with high sensitivity and specificity that permit lesion identification , characterisation and study , particularly the m parameter , in order to optimise patient treatment . 
 whole - body magnetic resonance ( mr ) with a dedicated coil and automatically moving table permits whole - body image acquisition in a short time with highly detailed morphology in 3d display . 
water motion is quantified by the apparent diffusion coefficient ( adc ) , which shows intraand extracellular microscopic water diffusibility in relation to factors that restrict diffusion with tissue ( cell membranes , viscosity )  . the aim of the study was to assess the overall diagnostic accuracy of magnetic resonance diffusion - weighted whole - body imaging with background signal suppression ( mr - dwibs ) compared with [ 18f ] - fluorodeoxyglucose ( fdg ) - positron emission tomography ( pet ) / computed tomography ( ct ) , which is considered the reference standard of whole - body tumour imaging modalities , in a series of consecutive patients with malignant tumour . 
 patientand lesion - based analysis was performed , and adc vs standardised uptake value ( suv ) were compared . loutcome dei pazienti oncologici dipende in maniera decisiva dalla precocit diagnostica , dalla strategia terapeutica e da un appropriato follow - up . 
in questottica si rende necessario lo studio panoramico di tutti i distretti corporei in un tempo unico e con apparecchi disponibili sul territorio in considerazione dellalta incidenza della patologia neoplastica . 
la ricerca stata orientata verso metodiche ad alta sensibilit e specificit che consentano di riconoscere , caratterizzare e stadiare le lesioni , con riferimento in particolare al parametro m , per ottimizzare il percorso terapeutico del paziente . 
la tecnica whole body in risonanza magnetica ( rm ) , con bobina dedicata e movimento automatico del tavolo , permette di acquisire immagini dellintero corpo in tempi brevi , con un elevato dettaglio morfologico nei tre piani . 
la diffusivit dellacqua viene quantificata dal coefficiente di diffusione apparente ( adc ) che descrive la diffusione intraed extracellulare in relazione a fattori di costrizione dei tessuti ( membrane cellulari , viscosit )  . lo scopo di questo studio stato valutare in un campione di pazienti consecutivi con neoplasia maligna , laccuratezza diagnostica complessiva della rm - diffusion weighted whole body imaging with background signal suppression ( dwibs ) whole body comparata con la 18f - fluor - deossiglucosio ( fdg ) - tomografia a emissione di positroni ( pet ) / tomografia computerizzata ( tc ) , che considerata lo stanradiol med ( 2012 ) 117 : 293311 materials and methods thirty - eight patients ( 18 men , 20 women , mean age 60.6 years ) diagnosed with a malignant tumour over a 4 - month period and who had undergone [ 18f ] - fdg - pet / ct and mr - dwibs were enrolled in this retrospective , observational study . 
based on histological findings , 15 patients were diagnosed with breast cancer , 12 with colon cancer , two with ovarian cancer , five with lung cancer and one with mesothelioma , whereas three patients were diagnosed with mucinous tumour probably of intestinal origin , adenocarcinoma probably of pulmonary origin and adenocarcinoma probably of pancreatic origin , respectively . 
twenty - four patients had undergone [ 18f ] - fdg - pet / ct and mr - dwibs during chemotherapy ( cht ) , and 16 had previously been treated with cht with a minimum 30 - day and maximum 360 - day interval . 
our study was conducted in accordance with the guidelines established by the local ethics committee for retrospective evaluation , and patients gave their written informed consent to data analysis . [ 18f ] - fdg - pet / tc imaging protocol patients were instructed to fast , except for glucose - free oral hydration , for at least 6 h before intravenous injection of 370550 mbq ( 3.7 mbq / kg ) of [ 18f ] - fdg . 
we used a 16 slice spiral ct scanner with a dedicated full - ring pet scanner with bismuth germinate crystals ( discovery ste , general electric healthcare milwaukee , wi , usa )  . 
initially , the ldct scan was acquired starting from the orbitomeatal level and moving towards the feet using the following parameters : 80 ma , 140 kv , 0.5 s per tube rotation , slice thickness dard di riferimento nelle modalit whole body di imaging oncologico . 
stata eseguita unanalisi sui pazienti e sulle lesioni , ed stato comparato ladc con lo standardized uptake value ( suv )  . materiali e metodi nel nostro studio osservazionale retrospettivo , in un periodo di 4 mesi , sono stati inclusi 38 pazienti ( 18 maschi , 20 femmine , et media : 60 , 6 anni ) che avevano eseguito 18f - fdg - pet / tc e rm - dwibs , affetti da neoplasia maligna . 
in base alla diagnosi istologica 15 pazienti sono risultati affetti da carcinoma della mammella , 12 pazienti da carcinoma del colon retto , 2 da carcinoma dellovaio , 5 da carcinoma polmonare , 1 da mesotelioma , mentre in 3 pazienti stata fatta diagnosi rispettivamente di metastasi da carcinoma occulto mucinoso di probabile origine intestinale , adenocarcinoma di probabile origine polmonare e adenocarcinoma di probabile origine pancreatica . 
i 3 pazienti con carcinoma occulto sono stati valutati per la ricerca del tumore primitivo e per la stadiazione di malattia , gli altri 35 sono stati studiati per valutare la risposta alla terapia . 
ventiquattro pazienti sono stati sottoposti ad esame pet / tc e rm - dwibs durante la chemioterapia ( cht ) , 16 pazienti erano stati trattati precedentemente con cht con un intervallo di minimo 30 giorni e un massimo di 360 giorni ; 8 pazienti erano stati sottoposti a cht neoadiuvante ; 4 pazienti erano stati trattati con radioterapia ( rt ) associata a cht , di cui uno solo con rt e cht neoadiuvante . 
la pet whole - body e la tc sono state eseguite consecutivamente , 60 minuti 296 radiol med ( 2012 ) 117 : 293311 3.75 mm , pitch 1.35 : 1 , scan length 867 mm ( depending on patient height ) , data acquisition time 12.522.5s. 
depending on patient height , seven to eight bed positions were acquired covering the body from the hip to the head in approximately 2427 mct data were used for attenuation correction , and images were reconstructed with a matrix of 256256 using the standard 3d iterative algorithm ( vuepoint hd )  . 
the images were reviewed on the workstation xeleris ( ge healthcare ) with a software dedicated to pet / ldct , providing multiplanar reformatted ( mpr ) attenuation - corrected and noncorrected images of pet only , ldct only and fused pet / ldct with linked cursor and 3d volume rendering ( vr ) pet / ct . 
pet / ct images were reviewed by a nuclear medicine physician with 4 years of experience in reading combined pet / ldct in patients with tumours ( primary and secondary lesions ) and who had no knowledge of the results of the clinical investigations , including mr data ( imaging and dwibs )  . 
the suv body weight ( suvbw ) , expressed in grams per millilitre , was calculated using the commercially available software provided by the manufacturer , which considers pixel values in kilobecquerel per millilitre ( kbq / ml ) decay corrected , multiplied by patient weight and divided by the decaycorrected net injected activity . 
lesion size was measured on ldct images . mr - dwibs imaging protocol an achieva 1.5 - tesla ( philips , best , the netherlands , release 2.5 ) with morphologic sequences [ turbo spinecho and short - tau inversion recovery ( tse and stir ) ] and diffusion was used to evaluate all patients . 
the q body coil and mobi - track technology with five to stacks per slice and multiple b values ( b = 500 and b = 1000 ) were used . 
the dwibs protocol required an acquisition time of approximately 20 min , a mean post elaboration time of 15 min and a mean interpretation time of 18 min ( table 1 )  . 
abbiamo usato un sistema pet / tc che combina uno scanner tc spirale a 16 slice con uno scanner pet dedicato con cristalli di germanato di bismuto ( discovery ste , general electric healthcare milwaukee , wi )  . 
inizialmente , la scansione tc stata acquisita cominciando dal livello orbitomeatale e muovendosi in senso cranio - caudale usando i seguenti parametri : 80 ma , 140 kv , 0 , 5 s alla rotazione del tubo , spessore delle fette 3 , 75 mm con un pitch di 1 , 35 : 1 , lunghezza di scansione 867 mm ( dipende dallaltezza del paziente ) , tempo di acquisizione dei dati 12 , 522 , 5 s . 
immediatamente dopo la scansione tc , una scansione a emissione pet stata acquisita in 3d , con un tempo di acquisizione di 3 minuti a lettino , con un overlap di 9 slices . 
in base allaltezza del paziente sono stati acquisiti 78 lettini per esplorare il corpo dal femore alla testa in circa 2427 mi dati ct sono stati usati per la correzione dellattenuazione e le immagini sono state ricostruite con una matrice di 256256 , usando lalgoritmo interattivo 3d standard ( vuepoint hd )  . 
le immagini acquisite sono state elaborate sulla workstation xeleris , ( ge healthcare , milwaukee , wi ) con un software dedicato alla pet / tc , mostrando immagini multiplanari con correzione dellattenuazione e immagini non corrette della sola pet , della sola tc e le immagini fuse pet / tc e il 3d volume rendering . 
le immagini pet / tc sono state analizzate da un medico nucleare con 4 anni di esperienza nella lettura della pet / tc combinata nei pazienti con tumori ( lesioni primitive e secondarie ) e che non conosceva il risultato degli esiti clinici inclusi gli esiti della mr ( imaging e dwibs )  . 
il suv ( suvbw ) espresso in g / ml , stato calcolato usando il software commerciale disponibile della ditta che considera i valori del pixel in base al decadimento corretto kbq / ml , moltiplicato per il peso del paziente e diviso per il decadimento corretto della dose iniettata . 
sono state utilizzate la bobina q - body e la tecnologia mobi - track con 58 stack per piano e con multipli valori del coefficiente b ( b = 500 e b = 1000 )  . 
il protocollo dwibs ha richiesto un tempo dacquisizione di circa 20 minuti , un tempo medio di post - elaborazione di 15 minuti e un tempo di lettura medio di circa 18 minuti ( tabella 1 )  . 
 il calcolo delladc stato ottenuto mediante il posizionamento di una regione di interesse ( roi ) con diametro scelto in base alle dimensioni e alla omogeneit del segnale di costrizione di ogni lesione , ottenendo una valutazione statistica della media e della deviazione standard . 
le aree di alterata diffusivit in dwibs sono state correlate con le immagini ottenute con le sequenze morfologiche per la loro localizzazione anatomica e per il riconoscimento delle fisiologiche sedi di alterato segnale di diffusione . analisi statistica la concordanza tra i risultati pet / tc e mr - dwibs stata valutata mediante la di cohen , mentre laccordo tra le lesioni positive identificate con entrambe le metodiche stato valutato usando la percentuale positiva di accordo ( ppa )  . 
 risultati region of interest ( roi ) with a diameter based on the size and homogeneity of the signal for each lesion , performing a statistic evaluation by mean and standard deviation ( sd )  . 
 the mr - dwibs images were examined by two radiologists with 4 years of experience in these methods and who had no prior knowledge of the [ 18f ] - fdg - pet / ct results . 
 areas showing changes in diffusion in mr - dwibs were lanalisi qualitativa della mr - dwibs e della 18f - fdgpet / tc mostra che un paziente era negativo ad entrambe le tecniche . 
un accordo complessivo di 34 / 38 ( 89 , 47% ) stato trovato , ma la concordanza era bassa e non statisticamente significativa ( di cohen = 0 , 243 ; p = 0 , 164 )  . 
due dei 4 pazienti discordanti e risultati nega298 radiol med ( 2012 ) 117 : 293311 correlated with images obtained in the morphological sequences for anatomic localisation and identifying the site of restricted diffusion signal . statistical analysis concordance between [ 18f ] - fdg - pet / ct and mr - dwibs was evaluated using cohens kappa , whereas agreement among positive lesions identified by both methods was evaluated using the positive percent agreement ( ppa )  . 
 correlation between suv and adc was calculated using pearsons correlation coefficient . results qualitative analysis of mr - dwibs and [ 18f ] - fdg - pet / ct showed that one patient was negative at both techniques . 
mr - dwibs was positive in 36 patients , 34 of whom were positive and two negative at [ 18f ] - fdg - pet / ct , respectively ( table 2 )  . 
at mr - dwibs , 38 lesions were parenchymal , 74 lymph nodal and 143 bone lesions , whereas at [ 18f ] - fdg - pet / ct they were 30 , 38 and 116 , respectively . 
 nei 34 pazienti risultati positivi ad entrambe le tecniche 89 lesioni risultavano perfettamente concordanti , 81 positive alla rm - dwibs e negative alla 18f - fdg - pet / tc , 85 negative alla rm - dwibs e positive alla 18f - fdg - pet / tc . 
in 4 pazienti positivi solo alla rm - dwibs ( pazienti discordanti ) sono state riscontrate 31 lesioni . alla rm - dwibs le lesioni hanno mostrato diametro compreso tra 8 e 58 mm , alla 18f - fdg - pet / tc tra 8 , 789 , 5 m alla rm - dwibs le sedi sono state 38 parenchimali , 74 linfonodali e 143 ossee mentre alla 18f - fdg - pet / tc rispettivamente 30 , 38 e 116 . 
in tabella 4 riportato il confronto tra rm - dwibs , 18f - fdgpet / tc e i risultati del follow - up clinico a 12 mesi . se per i 4 pazienti discordanti alla rm - dwibs escludiamo le lesioni linfonodali , 2 pazienti divengono negativi in accordo con 18f - fdg - pet / tc e con i risultati del followup , e se si escludono le lesioni ossee anche un altro paziente diviene rm - dwibs negativo in accordo con la pet / tc e con i risultati del follow - up . 
lindice di correlazione tra suv e adc delle lesioni positive a entrambe le tecniche non statisticamente significativo ( r = 0 , 283 ; p = 0 , 116 )  . 
table 4 shows comparisons between mr - dwibs , [ 18f ] - fdg - pet / ct and results of clinical follow - up at 12 months . considering mr - dwibs data in the four discordant patients , if lymph - node lesions are excluded , then two patients become negative in accordance with [ 18f ] - fdgla 18f - fdg - pet / tc e con la rm - dwibs non statisticamente significativa ( t = 2 , 097 ; p = 0 , 044 )  . 
 discussione in letteratura sono apparsi studi di confronto tra 18f - fdgpet / tc e rm - dwibs ma con un limitato numero di pazienti e per alcuni istotipi di neoplasia . 
 [ 1 ] ha perfezionato la tecnica whole body mediante unefficace soppressione del segnale di fondo e lutilizzazione di specifici software di acquisizione riducendo drasticamente i tempi di esecuzione dellesame [ 2 ]  . 
 discussion comparative studies of [ 18f ] - fdg - pet / ct and mr - dwibs reported in the literature have are limited to small numbers of patients and only some neoplasm isotypes . 
 water motion is a functional and dynamic phenomenon that can vary over time due to many physiological and pathological factors , such as body temperature , oedema and cellular necrosis [ 3 , 4 ]  . 
much importance has been paid to deterdellacqua un fenomeno funzionale e dinamico che pu variare nel tempo , in risposta a numerosi fattori fisiologici e patologici quali la temperatura corporea , edema e necrosi cellulare [ 3 , 4 ]  . 
molta importanza stata posta per determinare i valori del fattore di sensibilizzazione b che esprime il peso in diffusione della sequenza per la migliore identificazione delle lesioni nei differenti organi [ 5 , 6 ]  . 
numerosi studi sono stati fatti per lottimizzazione dei valori di b , modificandoli a seconda del distretto anatomico da esaminare , nellintento di migliorare la detezione delle lesioni [ 7 , 8 ]  . 
la 18f - fdgpet / tc si dimostrata una tecnica estremamente affidabile nellidentificazione di tumori maligni sia primitivi che secondari e nella valutazione della risposta alla chemio e radioterapia [ 9 , 10 ]  . 
 [ 11 ] in uno studio preliminare hanno confrontato le due metodiche e la loro accuratezza diagnostica in un gruppo selezionato di pazienti affetti da linfoma ( hodgkin [ lh ] e non hodgkin [ lnh ] ) prima della terapia , valutando laccuratezza diagnostica della metodica dwibs rispetto alla 18f - fdg - pet / tc . 
le immagini trans - assiali della scansione ct ( a ) , pet ( b ) e la fusion ( c ) mostrano tenue captazione del radiofarmaco a livello dei linfonodi dellilo polmonare di destra ( suv max 2 , 5 )  . radiol med ( 2012 ) 117 : 293311 304 fig . 
a , b assiale t1 ; focale ipointensit a carico dellarco posteriore della iii costa destra ; c dwibs ricostruzione mip coronale in parallelo ; focale costrizione di segnale a carico della iii costa destra . mining the sensitivity factor of b values , which expresses diffusion - weighted sequence , in order to better identify lesions in different organs [ 5 , 6 ]  . 
many studies have been performed in an attempt to optimise b values , changing them according to the body area examined to improve lesion detection [ 7 , 8 ]  . 
 the aim of our study was to compare the functional parameter of water motion in mr - dwibs with the increased metabolism of [ 18f ] - fdg , a reliable metabolic reference marker for tumours . 
 [ 18f ] - fdg - pet / ct is an extremely reliable technique for identifying primary and secondary malignant tumours and evaluating response to chemotherapy and radiotherapy [ 9 , 10 ]  . 
 [ 11 ] compared both methods ( and their diagnostic accuracy ) in a selected group of patients with lymphoma ( hodgkins and non - hodgkins ) before treatment , evaluating the diagnostic accuracy of mr - dwibs compared with [ 18f ] - fdg - pet / ct . 
questo dato in accordo con la bassa sensibilit della 18f - fdg - pet / tc per le neoplasie mucinose caratterizzate da alto contenuto dacqua ma basso metabolismo glucidico [ 12 ]  . 
esiste quindi una stretta relazione tra radiofarmaco e marker metabolico della neoplasia maligna . il nostro studio senza la selezione di una specifica neoplasia ha mostrato una concordanza tra le due tecniche in 34 di 38 pazienti ( 71 , 43% ) senza selezionare un istotipo specifico tumorale . 
la rm - dwibs risultata positiva anche in 3 pazienti che non avevano evidenza di lesioni alla 18f - fdg - pet / tc anche nel successivo follow up a 12 mesi . 
 therefore , a close relationship exists between radiopharmaceuticals and the metabolic marker of malignant tumours . our study showed an overall agreement between the two techniques in 34 of 38 patients ( 71.43% ) without selecting a specific tumour histological type . 
mr - dwibs was also positive in three patients with no evidence of lesions at [ 18f ] - fdg - pet / ct , even at 12 months follow - up . 
oltre allanalisi qualitativa , hanno confrontato i valori numerici del suv ottenuti in pet con quelli delladc nella dwibs , dimostrando il limitato apporto diagnostico delladc per distinguere neoplasie maligne da lesioni benigne . in uno studio pilota , stecco et al . 
nel nostro studio le lesioni identificate alla 18f - fdg - pet / tc hanno mostrato valori di suv sempre maggiori di 2 , 5 con un massimo di 24 , 1 ( 35 lesioni su 68 con suv > 5 ) con una ampia variazione del metabolismo glicidico . 
lanalisi delladc ha mostrato valori in un range molto ristretto tra 0 , 2 e 1 , 9 come confermato in letteratura dalla mancanza di valori di cut - off delladc e / o di valori standardizzati . 
a assiale stir ; focale iperintensit a carico del soma di l5 ; b coronale t1 ; focale ipointensit di segnale a carico di l5 ; c dwibs ricostruzione mip coronale in parallelo ; focale costrizione di segnale a carico del soma di l5 . adc in distinguishing malignant from benign lesions . 
la diffusivit dellacqua non un marker biometabolico di neoplasie maligne al contrario dellaumentato metabolismo del 18f - fdg [ 8 ]  . la non specificit del segnale dwibs per le neoplasie da mettere anche in relazione alle variazioni del parametro b in base ai distretti corporei nei quali localizzata la lesione . 
anche per le lesioni ossee stata riscontrata una ampia discordanza tra le due tecniche ed anche per esse il parametro b pu aver influito per la visualizzazione di alterazioni ossee non dovute a neoplasie maligne . 
ci giustifica il riscontro di un maggior numero di lesioni alla dwibs ( 255 ) rispetto alla 18f - fdg - pet / radiol med ( 2012 ) 117 : 293311 fig . 
le immagini coronali della 18f - fdg - pet / tc , le scansioni ct ( a ) , pet ( b ) e le immagini fuse ( c ) mostrano patologico accumulo del radiofarmaco nel soma di l5 ( suv max 5 , 7 )  . the non specificity of the mr - dwibs signal for lesions is related to the variations in the b value , depending on lesion site . 
in bone lesions , an important difference between the two techniques was observed and , in this case , the b parameter may have influenced the identification of bone changes , which were unrelated to malignant neoplasms . 
this would justify the higher number of lesions observed at mr - dwibs ( 255 ) compared with [ 18f ] - fdg - pet / ct ( 184 )  . 
per i linfonodi sono state evidenziate 63 lesioni dwibs positive e 18f - fdg - pet / tc negative ( 62% ) rispetto alle 27 18f - fdg - pet / tc positive e dwibs negative , con una concordanza in sole 11 lesioni ( ppa = 28 , 57% )  . 
per lo scheletro sono state evidenziate 75 lesioni dwibs positive ( 39% ) e 18f - fdg - pet / tc negative rispetto alle 48 18f - fdg - pet / tc positive e dwibs negative , con una concordanza positiva in 67 lesioni ( ppa = 58 , 14% )  . 
 questo pu essere spiegato con la presenza di alterata diffusivit della acqua in sede midollare in risposta a modificazioni metaboliche e non alla presenza di neoplasia maligna che invade il midollo e riassorbe ed erode il tessuto osseo . 
 la performance della dwibs migliorata se dalla analisi vengono escluse sia le lesioni linfonodali che ossee con la esatta concordanza sui dati dei pazienti ( 92% ) dopo 12 mesi di follow - up . radiol med ( 2012 ) 117 : 293311 308 fig . 
a assiale thrive dopo somministrazione di mezzo di contrasto ; marcata e disomogenea impregnazione della testa omerale sinistra ; b dwibs ricostruzione mip coronale in parallelo ; focale costrizione del segnale della testa e del collo omerale sinistro . 
this may be explained by changes in water diffusion in the bone marrow site due to metabolic changes and not to the malignant bone marrow lesions , which reabsorb and destroy bone tissue . 
if lymph - node and bone lesions are excluded from the analysis , then mr - dwibs performance improves , with total agreement in patient data ( 92% ) at 12 months follow - up . the wider diameter of lesions concordant with mr - dwibs is due to changes in the content and diffusion of water bordering and surrounding the tumour . 
mr and ct imaging are fundamental in assessing total tumour size but do not distinguish the metabolically active areas from the induced changes , which often make lesions appear larger . il maggior diametro con cui appaiono le lesioni concordanti alla dwibs pu essere spiegato da alterazioni del contenuto e diffusivit dellacqua alla periferia ed intor no al tumore . 
limaging morfologico rm e tc rimane determinante per la valutazione delle dimensioni della intera neoplasia ma non distingue le porzioni metabolicamente attive dalle alterazioni indotte che spesso fanno apparire le lesioni di maggiori dimensioni . limiti i limiti dello studio oltre al ridotto numero di pazienti ed alla difformit delle patologie esaminate sono legati radiol med ( 2012 ) 117 : 293311 fig . 
18f - fdg - pet / tc con immagini coronali : tc ( a ) , pet ( b ) e le immagini fuse ( c ) mostrano accumulo patologico dellomero di sinistra , nel soma di l3 e di l5 . 
 limitations this study has several limitations related to a small sample size , pathology heterogeneity and signal constriction of normal anatomic structures , such as the waldeyers ring , salivary glands , spleen , brain and medulla , lymph nodes , intestinal content , peripheral nerves , adrenal glands , kidneys , bladder , prostate , endometrium , ovaries and testial segnale di costrizione di alcune strutture anatomiche normali quali lanello di waldeyer , ghiandole salivari , milza , encefalo e midollo , i linfonodi , il contenuto intestinale , nervi periferici , surreni , reni , vescica , prostata , endometrio , ovaie e testicoli . 
altro limite delle sequenze dwi riguarda lidentificazione di lesioni contigue al cuore , come quelle in sede mediastinica ed al lobo epatico di sinistra per la presenza di artefatti da movimento . 
le sequenze table 4 comparison between mr - dwibs , [ 18f ] - fdg - pet / ct and results of clinical follow - up at 12 months pet pos neg neg pos , positive ; neg , negative ; pts , patients dwibs pos neg pos tot pts if lymphnode lesions are excluded from dwibs data ( tot pts ) if lymphnode and bone lesions clinical follow - up at 12 months are ecluded from dwibs data ( tot pts ) diagnosis tot pts pos neg 310 radiol med ( 2012 ) 117 : 293311 tabella 4 confronto tra rm - dwibs , 18f - fdg - pet / tc e i risultati al follow - up clinico a 12 mesi se le lesioni linfonodali sono escluse dai risultati della dwibs ( pazienti , n ) dwibs ( pazienti , n ) dwibs pos neg pos pazienti ( n ) diagnosi pet pos neg neg pos , positivo ; neg , negativo cles . 
 high b - value dwi sequences determine signal suppression of anatomic structures and therefore create difficulty in placing lesions , so that a comparative assessment of morphological sequences is needed . conclusioni se le leioni linfonodali e ossee follow - up clinico a 12 mesi sono escluse dai risultati della diagnosi pos neg pazienti , n dwi con elevati valori di b determinano soppressione del segnale delle strutture anatomiche con conseguente difficolt nella localizzazione delle lesioni e ci rende indispensabile il ricorso alla valutazione comparata delle sequenze morfologiche . conclusions results of this observational , retrospective , comparative study of mr - dwibs and [ 18f ] - fdg - pet / ct show that mr - dwibs may be used to evaluate localisation of parenchymal neoplasms but is less efficacious in characterising lymph - node and skeletal lesions . 
compared with mr - dwibs , [ 18f ] - fdg - pet / ct is limited when identifying tumours with low glucose metabolism due to the high water content , as in mucinous neoplasms . 
the results of our study show that mr - dwibs evaluation must be integrated with morphological images to increase diagnostic accuracy of mr . i risultati di questo studio osservazionale retrospettivo di comparazione tra rm - dwibs e 18f - fdg - pet / tc indicano che la tecnica dwibs pu essere usata per la valutazione delle localizzazioni neoplastiche parenchimali e scheletriche risultando meno efficace nella caratterizzazione linfonodale . 
la 18f - fdgpet / tc mostra un forte limite nella identificazione dei tumori con basso metabolismo glucidico , come i carcinomi mucinosi , a differenza della dwibs , in rapporto allelevato contenuto di acqua , per le quali il radiofarmaco fdg non considerato ottimale . 
accordingly , the use of contrastenhanced us ( ceus ) has made possible an evaluation of the vascular enhancement pattern , similar to the use of magnetic resonance imaging ( mri )  . 
the parameters analysed in both techniques were the following : lesion length , wall thickness , layered wall appearance , comb sign , fibroadipose proliferation , presence of enlarged lymph nodes and stenosis . 
la presenza di attivit di malattia ( cdai ) nel morbo di crohn ( mc ) rappresenta un parametro fondamentale per stabilire la strategia medica o chirurgica nel trattamento , tuttavia una delle maggiori difficolt nel monitoraggio del mc costituito dalla non concordanza tra sintomatologia e rilievi imaging di attivit di malattia . 
 lecografia dellintestino tenue emerge come tecnica a basso costo non invasiva nella diagnosi e nel follow - up dei pazienti con mc , e inoltre lo studio mediante mezzo di contrasto ( ceus ) ha reso possibile la valutazione dellenhancement parietale similmente alla enteroclisi in risonanza magnetica ( rm )  . 
lenteroclisi - rm stata effettuata con apparecchiatura da 1 , 5 t con bobine phased - array e mezzo di contrasto ( mdc ) orale bifasico prima e dopo la somministrazione di chelati del gadolinio endovena . 
 i parametri analizzati per entrambe le metodiche sono : lunghezza della lesione , spessore parietale , aspetto striato di parete , segno del pettine , proliferazione fibroadiposa , linfoadenomegalie , stenosi . 
comparison between crohns disease activity index ( cdai ) and mri showed a low correlation , with an rho = 0.398 ; correlation between cdai - laboratory data and ceus activity was low , with rho = 0.354 ; correlation between mri activity and ceus activity was good , with rho = 0.791 ; high correlation was found between ceus and mri of the small bowel when assessing wallthickness , lymph nodes and comb sign ; good correlation was fund when assessing layered wall appearance , disease extension and fibroadipose proliferation . 
mri of the small bowel remains the most accurate method for evaluating disease activity . keyword mri enteroclysis contrast enhanced us crohns disease entrambe le metodiche in : ( 1 ) rapida impregnazione e rapida dismissione del mdc ; ( 2 ) lenta impregnazione e plateau con lenta dismissione del mdc . 
la correlazione tra cdai e rm si dimostrata scarsa con un coefficiente di correlazione spearmans ( rho ) = 0 , 398 ; la correlazione tra cdai e dati di laboratorio e attivit ceus si dimostrata scarsa con un coefficiente di correlazione spearmans ( rho ) = 0 , 354 ; la correlazione tra attivit rm e attivit ceus si dimostrata buona con un coefficiente di correlazione spearmans ( rho ) = 0 , 791 ; ottima correlazione tra ceus e enteroclisi - rm nella valutazione dello spessore parietale , dei linfonodi e segno del pettine ; buona correlazione nella valutazione dellaspetto striato della parete , dellestensione di malattia e della proliferazione fibro - adiposa . 
lenteroclisi rm rimane tuttora la metodica imaging non invasiva pi accurata per la stima di attivit di malattia . parole chiave enteroclisi rm ecografia con mdc morbo di crohn introduction introduzione crohns disease ( cd ) is a chronic inflammatory bowel disease characterised by periods of remission and exacerbation . 
the combination of clinical score [ 1 ] , laboratory investigations , endoscopy and imaging techniques [ 2 ] is therefore used to follow - up on patients affected by cd , although there is no gold standard defined . 
magnetic resonance imaging ( mri ) and ultrasound ( us ) of the small bowel easily identify location and length of affected segments of the small intestine in patients with cd [ 37 ] and provide information on possible complications , such as abscesses , fistulas and stenosis [ 711 ]  . 
mri is also a powerful tool for detecting the presence of multiple affected segments , abnormalities of the intestinal wall [ 12 , 13 ] and as extraluminal disease . bowel us has emerged as a low - cost , noninvasive technique in diagnosis and follow - up of patients with cd [ 14 , 15 ] , as it is a nonionising imaging modality that is well tolerated and accepted by patients and , overall , is relatively acil morbo di crohn ( mc ) una malattia cronica infiammatoria intestinale caratterizzata da periodi di remissione e di riacutizzazione . 
la combinazione di punteggio clinico [ 1 ] , indagini di laboratorio , endoscopia e tecniche di imaging [ 2 ] viene utilizzata per monitorare lattivit , anche se attualmente non esiste un gold standard definito . 
in pazienti con mc , lenteroclisi in risonanza magnetica ( rm ) e lecografia della parete intestinale identificano facilmente la localizzazione e la lunghezza dei segmenti affetti del piccolo intestino [ 37 ] e forniscono informazioni riguardo a possibili complicanze , come ascessi , fistole e stenosi [ 711 ]  . 
 la rm inoltre un potente mezzo per rilevare la presenza di pi segmenti affetti , di anomalie della parete intestinale [ 12 , 13 ] come pure patologie extraluminali . lecografia dellintestino emersa come metodica non invasiva e a basso costo nella diagnosi e nel follow - up dei pazienti con mc [ 14 , 15 ] ; essa rappresenta una modalit di imaging non ionizzante ben tollerata ed accettata dai pa270 radiol med ( 2012 ) 117 : 268281 curacy for determining intramural and extramural extension of the disease [ 15 ]  . zienti con buona accuratezza per la valutazione dellestensione intramurale ed extramurale della malattia [ 15 ]  . a substantial number of studies have shown a correlation between bowel - wall thickening and clinical disease activity [ 1618 ]  . 
us limitation is , however , the difficulty in evaluating the entire intestinal loops and intestinal wall vascularity ; moreover , differentiation between thickening due to active inflammation or fibrosis is another limit [ 1719 ]  . second - generation us contrast agents ( contrast - enhanced us , ceus ) has made microvascular imaging possible [ 2023 ] , allowing evaluation similar to that of mri of vascular enhancement [ 24 , 25 ]  . 
however , to the best of our knowledge , only a few comparative studies exist in the literature evaluating ceus and mri in relation to disease activity [ 26 ]  . 
the aim of this study is therefore to describe the potential role of ceus compared with mri in monitoring cd activity . un numero consistente di studi in letteratura riporta una correlazione tra lispessimento della parete intestinale e lattivit clinica di malattia [ 1618 ]  . 
il limite dellecografia tuttavia la difficolt nel valutare la vascolarizzazione della parete intestinale ; inoltre la differenziazione tra ispessimento dovuto a infiammazione attiva o a fibrosi rappresenta un limite per questa metodica [ 1719 ]  . recentemente luso di mezzi di contrasto ecografici di seconda generazione ( contrast enhanced ultrasonography , ceus ) ha reso possibile limaging microvascolare [ 2023 ] , consentendo una valutazione analogamente a quanto avviene in rm [ 24 , 25 ]  . 
 materials and methods study population materiali e metodi popolazione di studio we prospectively enrolled 31 consecutive patients ( 17 men , 14 women , mean age 41.2 years , range 1780 years ) between march and july 2009 . 
laboratory parameters were obtained , such as c - reactive protein ( crp ) , white blood cell count ( wbc ) , haematocrit , erythrocyte sedimentation rate ( esr )  . 
the time interval between mri and ceus was a maximum of 2 days . exclusion criteria we excluded patients with mri contraindications , with suspicion of acute abdomen ( suspected perforation , intestinal obstruction ) and cases with presence of multiple intestinal lesions . 
moreover , patients with a body mass index ( bmi ) > 30 were also sono stati selezionati per lo studio 31 pazienti consecutivi ( 17 maschi , 14 femmine , et media 41 , 2 anni , range 1780 anni ) arruolati in maniera prospettica nel periodo compreso fra marzo e luglio 2009 . 
il comitato etico ha approvato lo studio e tutti i pazienti hanno fornito il consenso informato per le indagini prima di essere inclusi nello studio . criteri di inclusione sono stati arruolati i pazienti con diagnosi di mc provata mediante biopsia effettuata in corso di colonscopia con una sola lesione a livello dellintestino tenue . 
per ogni paziente stato compilato un questionario clinico anamnestico al fine di calcolare lo score di attivit di malattia ( cdai , crohns disease activity index ) , e sono stati ottenuti i parametri laboratoristici per la determinazione dello stato infiammatorio della parete intestinale [ proteina c reattiva ( pcr ) , velocit di eritrosedimentazione ( ves ) , ematocrito , leucociti ]  . 
 tutti i pazienti hanno eseguito prima una enteroclisi - rm e successivamente un esame ecografico in b - mode e dopo somministrazione di mezzo di contrasto ( mdc ) ( ceus ) per studiare il tratto intestinale sede di malattia . 
lintervallo tra rm e ceus stato compreso entro 2 giorni . criteri di esclusione sono stati esclusi i pazienti con controindicazioni alleseradiol med ( 2012 ) 117 : 268281 excluded because of lack of sufficient technical accuracy in evaluating small - bowel loops with high - frequency us probe . 
laboratory tests and the cdai were considered the reference standard for monitoring disease activity . imaging mri examinations were performed with 1.5 - t magnet ( siemens symphony , germany ) and phased - array coils with patients in the supine position . 
administration of gadolinium chelates ( 0.1 mmol / kg ) ( magnevist , schering ag , germany )  . to evaluate the enhancement of the intestinal wall , vibe sequences repeated at time 0 ( pre - enhanced phase ) during cuzione dellindagine rm , con sospetto di addome acuto ( sospetta perforazione , occlusione intestinale ) e i casi con presenza di pi lesioni intestinali . 
la popolazione definitiva risultata essere pari a 30 pazienti . indagini clinico - laboratoristiche i pazienti sono stati monitorati da un punto di vista clinico laboratoristico utilizzando il cdai ed esami di laboratorio . 
i test di laboratorio e il cdai sono stati considerati standard di riferimento per monitorare lattivit di malattia nel nostro studio . imaging gli esami rm sono stati eseguiti con magnete da 1 , 5 t ( siemens simphony , germania ) con paziente in decubito supino utilizzando bobine phased - array ; tutti i pazienti hanno seguito una dieta priva di scorie nei 2 giorni precedenti lindagine , e digiuno completo nelle 8 ore antecedenti lesame . 
 per ottenere una ottimale distensione delle anse intestinali sono stati somministrati a ciascun paziente 15002000 ml di soluzione peg per via orale ( isocolan , bracco , milano , italia )  . 
in tutti i casi stato usato un agente antispastico per inibire la motilit intestinale [ 1 mg di metil scopolamina endovena ( ev ) subito prima dellesame ] al fine di annullare gli artefatti da peristalsi intestinale . 
tutti i pazienti sono stati analizzati con apparecchiatura rm da 1 , 5 t ( magnetom symphony , siemens medical solutions , erlangen , germania ) utilizzando una bobina body phased - array . 
il protocollo di scansione utilizzato in tutti i pazienti stato il seguente : sequenze coronali turbo spin echo ( tse ) t2272 radiol med ( 2012 ) 117 : 268281 fig . 
using the image subtraction technique , the signal intensity level of a circular region of interest ( roi ) placed over the examined thickened bowel loop was calculated , and contrast enhancement was evaluated . 
ceus was performed with a 7.5 - mhz linear probe using a second - generation us contrast agent ( sonovue , bracco , milan , italy ) and contrast - tuned imaging technology ( cnti , esaote genoa , italy ) , a real - time technology based on a low mechanical index and a real - time scan that ensures the continued preservation of the contrast agent . 
a low acoustic power setting was used , 4045 kpa pressure , which expresses the same mechanical index ( mi ) , 0.090.14 , of a 7.5 - mhz linear probe . 
gain setting was adjusted to obtain an anechoic wall except for hyperechoic serosal layer and hyperechoic central line arising from the intestinal lumen . dipendenti in apnea espiratoria [ tempo di ripetizione ( tr ) / tempo di eco ( te ) 4500 / 985 ms , spessore di fetta 6 cm , campo di vista ( fov ) 350350 mm , matrice 330512 ] , sequenze coronali half - fourier acquisition single - shot turbo spin - echo ( haste ) t2 - dipendenti in apnea espiratoria ( tr / te 1900 / 113 , spessore di fetta 4 mm ) , sequenze true fast imaging with steady precession ( fisp ) con saturazione del grasso sui piani coronale , sagittale e assiale dal diaframma alla pelvi . 
sequenze 3d volume interpolated breath - hold ( vibe ) ( tr / te 4 , 5 / 1 , 7 ms , spessore di fetta 2 , 5 mm , fov 400400 mm , matrice 300512 ) nelle condizioni di base e ripetute in fase arteriosa , portale e venosa tardiva dopo somministrazione ev di chelati del gadolinio ( 0 , 1 mmol / kg ) ( magnevist , schering ag , germania )  . al fine di valutare limpregnazione della parete intestinale sono state analizzate le sequenze vibe ripetute al tempo 0 ( fase precontrastografica ) e rispettivamente nella fasi arteriosa , portale e tardiva . 
individuata lansa intestinale patologica si proceduto alla somministrazione a bolo ( dose di 4 , 8 ml ) del mdc ( sonovue , bracco , milano , italia ) attraverso unagocannula posizionata su una vena antecubitale del braccio . 
la ceus stata eseguita con una sonda lineare da 7 , 5 mhz , utilizzando un mezzo di contrasto ecografico di seconda generazione sonovue ( bracco , milano , italia ) e la tecnologia contrast tuned imaging ( cnti , esaote , genova , italia ) una tecnologia real time basata su un basso indice meccanico e una scansione in tempo reale che assicura la prolungata preservazione del mezzo di contrasto . 
loscillazione non lineare delle microbolle risulta in frequenze armoniche che sono multiple della frequenza di trasmissione ; lecografo viene impostato sul segnale generato dalle microbolle in vibrazione , che pi grande in ampiezza di quello generato dai tessuti . 
stato utilizzato un basso settaggio del potere acustico , pressione 4045 kpa , che esprime lindice meccanico ( mi ) pari a 0 , 090 , 14 , con sonda lineare da 7 , 5 mhz . 
il settaggio dei guadagni stato regolato in modo da ottenere una parete intestinale anecogena eccetto per lo strato sieroso iperecogeno e la linea centrale iperecogena derivante dal lume intestinale . tramite software integrato nellapparecchio stata calcolata lintensit dellenhancement continuativamente dal tempo 0 ( ecografia di base ) alla fase venosa tardiva considerata a 120 secondi dalliniezione posizionando una roi in corrispondenza della zona interessata ( parete intestinale ispessita sul versante antimesenterico )  . 
 using device - embedded software , enhancement intensity was evaluated continuously from time 0 ( baseline us ) to late venous phase , considered to be 120 s after injection . 
a signal intenle immagini rm sono state valutate in maniera indipendente da due radiologi esperti in patologia gastrointestinale , a conoscenza della diagnosi di mc , ma non delle attuali condizioni cliniche dei pazienti . 
3a - c b - mode us scan with 7.5 - mhz linear probe showing the long axis of a small - bowel loop affected by crohns disease in the active phase . 
c time - intensity curve obtained with a roi on the bowel wall shows rapid enhancement and slow washout of the contrast agent , reflecting the presence of severe inflammation at the lesion . 
3a - c scansione ecografica in b - mode ottenuta mediante sonda lineare 7 , 5 mhz che dimostra unansa ileale seconda lasse longitudinale affetta da morbo di crohn in fase attiva . 
la curva intensit / tempo in c ottenuta mediante posizionamento di roi sulla parete intestinale dimostra un enhancement rapido e una lenta dismissione del contrasto , rispecchiando un importante impegno infiammatorio a livello della lesione . sity - time curve was obtained to determine the maximum difference between baseline us and the point of maximum lesion enhancement . image analysis mr images were assessed independently by two radiologists experienced in gastrointestinal disease who were aware of the diagnosis of crohns disease but unaware of the patients clinical condition . 
parameters analysed for both techniques were the following : lesion length , wall thickness measured on the point of maximum diameter of the diseased wall , striated wall appearance , presence of vasa recta ( comb sign ) , fibroadipose proliferation , presence of lymphadenopathy , stenosis and dilation . 
patients were considered active if wall thickness was > 3mm , with layered appearance of the wall layers , with fibroadipose proliferation , with the comb sign and intense uptake of contrast agent in the arterial phase . 
contrast - enhanced mr images were evaluated by subtracting the precontrast images from the late postcontrast ones , resulting in a timeintensity curve . estensione in lunghezza della lesione , spessore parietale misurato nel punto di massimo diametro della parete interessata , aspetto striato parietale , presenza dei vasa recta ( segno del pettine ) , proliferazione fibroadiposa , presenza di linfoadenomegalie , stenosi e dilatazioni prestenotiche . 
 sulla base dei risultati della positivit dei parametri imaging sono stati considerati attivi i pazienti con spessore parietale > 3 mm , con aspetto striato della parete , con proliferazione fibroadiposa , con segno del pettine e con intensa impregnazione di mdc in fase arteriosa . 
abbiamo classificato le curve di impregnazione parietale di mc in 2 tipi in relazione al pattern contrastografico ottenuto dalla curva intensit - tempo sia alla radiol med ( 2012 ) 117 : 268281 fig . 
4a - c b - mode us with a linear probe showing the long axis of a small - bowel loop affected by crohns disease in the inactive phase ( a )  . 
4a - c scansione ecografica in b - mode in a ottenuta mediante sonda lineare 7 , 5 mhz che dimostra unansa ileale seconda lasse longitudinale affetta da morbo di crohn in fase quiescente . 
la prima curva riflette un mc in fase attiva , seconda in fase cronica . i risultati ceus e rm sono stati messi a confronto utilizzando il test parametrico di spearman ed infine correlati ai dati clinico - laboratoristici . 
la correlazione tra rm , il cdai e il ceus stata ottenuta mediante il test di spearman utilizzando un software dedicato ( spss , version 12 , chicago , il , usa )  . ceus and mri results were compared using the parametric spearman test and finally related to clinical and laboratory data using a dedicated software package ( spss , version 12 , chicago , il , usa )  . risultati clinical evaluation allowed us to distinguish 2 / 30 patients with cdai > 150 ( active phase ) and 28 / 30 with cdai < 150 ( chronic phase )  . 
laboratory investigations showed positive la valutazione clinico anamnestica ha permesso di distinguere 2 / 30 pazienti con cdai > 150 e quindi in fase attiva mentre 28 / 30 presentavano cdai < 150 , in fase cronica . 
i risultati dei statistics results table 1 disease activity in the patient population according to the crohns disease activity index ( cdai ) and laboratory tests tabella 1 attivit di malattia secondo crohns disease activity index ( cdai ) e valori di laboratorio patient no . 
mri investigation showed the following results : average lesion length 11.9 cm ( range 4.530 cm ) , average wall thickness 5.8 mm ( range 410 mm ) , parietal striated appearance in 10 / 30 cases , comb sign in 9 / 30 , fibroadipose proliferation in 3 / 30 , stenosis in 0 / 30 and upstream dilatation in 0 / 30 and lymphadenopathy in 7 / 30 . 
ceus gave the following results : average lesion length 10.4 cm ( range 320 cm ) , average wall thickness 5.7 mm ( range 410 mm ) , parietal multilayer appearance in 14 / 30 patients , comb sign in 6 / 30 , fibroadipose proliferation in 1 / 30 , stenosis in 0 / 30 , upstream dilatation 0 / 30 and lymphadenopathy in 3 / 30 . 
allindagine rm sono stati rilevati i seguenti risultati : lestensione media in lunghezza della lesione era di 11 , 9 cm ( range 4 , 530 cm ) , lo spessore parietale medio di 5 , 8 cm ( range 410 mm ) , laspetto striato parietale era presente in 10 / 30 casi , il segno del pettine in 9 / 30 , la proliferazione fibroadiposa in 3 / 30 , stenosi in 0 / 30 casi e dilatazione a monte in 0 / 30 pazienti , linfoadenomegalie in 7 / 30 . 
la correlazione tra cdai e rm si dimostrata scarsa con un coefficiente di correlazione spearmans ( rho ) = 0 , 398 e un valore di p pari a 0 , 03 . 
 lindagine ceus ha fornito i seguenti risultati : lestensione media in lunghezza della lesione era di 10 , 4 cm ( range 320cm ) , lo spessore parietale medio di 5 , 7 mm ( range 410 mm ) , laspetto striato parietale era presente in 14 / 30 casi , il segno del pettine in 6 / 30 , la proliferazione fibroadiposa in 1 / 30 , la stenosi del tratto interessato in 0 / 30 casi e dilatazione a monte in 0 / 30 pazienti , linfoadenomegalie in 3 / 30 . 
 la correlazione tra attivit rm e attivit ceus si dimostrata buona con un coefficiente di correlazione spearmans ( rho ) = 0 , 791 con un valore di p < 0 , 0001 . 
i risultati hanno messo in evidenza una ottima correlazione ( rho = 0 , 926 ; p < 0 , 0001 ) tra ceus e enteroclisi - rm nella valutazione dello spessore parietale , dei linfonodi e dei vasa recta ; buona correlazione ( rho = 0 , 716 ; p < 0 , 0001 ) nella valutazione dellaspetto striato della parete , dellestensione di malattia e della proliferazione fibroadiposa . 
in rm le curve intensit tempo sono risultate essere attive in 12 / 30 pazienti , in ceus in 14 / 30 pazienti , con correlazione curva ceus / curva rm scarsa ( r = 0 , 167 p = 0 , 36 )  . 
tutti i valori di correlazione e la significativit dei risultati sono riportati in tabella 3 . table 3 correlation values and significance of results in comparison between clinical and laboratory tests , ceus and mri parameters correlation coefficient ceus , contrast - enhanced ultrasonography ; mri , magnetic resonance imaging ; cdai , crohns disease activity index ; lab , laboratory results ; us , ultrasound tabella 3 valori di correlazione e significativit dei risultati nel confronto tra dati clinici , valori di laboratorio , ecografia con mezzo di contrasto ( ceus ) e risonanza magnetica ( rm ) dellintestino tenue cdai vs . 
a high correlation ( rho = 0.926 ; p < 0.0001 ) was found between ceus and mri of the small bowel for assessing wall thickness , lymph nodes and vasa recta ; there was good correlation ( rho = 0.716 ; p < 0.0001 ) for assessing layered wall appearance , disease extension and fibroadipose proliferation . 
all correlation values and significance of the results are reported in table 3 . discussion one of the most common problems in managing a patient with cd is the discrepancy between reported symptoms , laboratory and clinical evaluation and imaging . 
several diagnostic techniques are commonly used to diagnose cd : conventional enteroclysis represents the standard of reference , as it is highly sensitive in detecting mucosal ulcerations and cobblestone appearance of the wall , allowing for an early diagnosis ; however , a considerable dose of ionising radiation is administered to the patient , with an average dose of 510 msv . mri of the small bowel and ceus represent new , noninvasive techniques for multiplanar imaging aimed not only at diagnosing the disease but also monitoring its activity . 
mri of the small bowel already has a well - established role in the diagnosis of cd , as it allows optimal evaluation of disease extension , activity and possible related complications ; however , it is not widely available , and the time for image acquisition is relatively long compared with that of ct of the small bowel [ 2730 ]  . 
mri of the small bowel can study in detail not only the lumen but also the intestinal wall and surrounding tissue ; these patterns , combined with high sensitivity in the diagnosis of complications ( fistulas , abscesses ) and the absence of ionising radiation , make mri one of the most widely used surveys as a baseline examination for chronic inflammatory diseases and also for the follow - up . on the other hand , ceus is a very promising technique that offers the possibility of detecting all the characteristic signs of active disease , in particular , bowel - wall enhancement , using contrast agents as a blood - pool , which better shows the increased vascular network of the affected bowel loop compared with ct and mri contrast agents , which are vascular and interstitial . 
however , this method has discussione uno dei problemi pi comuni nella gestione di un paziente affetto da mc la discrepanza fra i sintomi riferiti , la valutazione clinico laboratoristica e la malattia obiettivabile allimaging . 
numerose metodiche diagnostiche sono correntemente utilizzate per la diagnosi del morbo di crohn : lenteroclisi convenzionale rappresenta lindagine di riferimento , molto sensibile nel rilevare le ulcerazioni mucose e laspetto ad acciottolato della parete permettendo una diagnosi precoce ; tuttavia viene somministrata al paziente una dose non trascurabile di radiazioni ionizzanti mediamente pari a 510 msv . la enteroclisi rm e lecografia con mezzo di contrasto ( ceus ) , rappresentano la nuova frontiera dellimaging non invasivo multiplanare con lintento non solo di diagnosticare la malattia ma anche di monitorarne lattivit . 
la enteroclisi rm ha un ruolo consolidato nella diagnosi di mc permettendo di ottenere una valutazione ottimale del bilancio destensione , di attivit di malattia e di eventuali complicanze associate ; tuttavia non largamente disponibile sul territorio e i tempi di esecuzione dellindagine sono relativamente maggiori se paragonati alla enteroclisi tc [ 2730 ]  . 
anche se priva della sensibilit per le fini alterazioni della mucosa rilevabili con la enteroclisi convenzionale , la enteroclisi rm caratterizzata dalla maggiore panoramicit e dalla possibilit di studiare in dettaglio non solo il lume e la parete intestinale , ma anche tutto ci che sta intorno . 
queste caratteristiche , unite alla elevata sensibilit nella diagnosi delle complicanze ( fistole , ascessi ) e lassenza di radiazioni ionizzanti hanno reso la enteroclisi rm una delle indagini pi utilizzate di fronte al sospetto di patologia infiammatoria del piccolo intestino e soprattutto come indagine di riferimento per il follow - up e per il bilancio di attivit di malattia . 
 il ceus infine una tecnica di studio molto promettente che offre la possibilit di individuare tutti i segni caratteristici della malattia in fase attiva , ed in particolare lenhancement della parete intestinale grazie allutilizzo di mdc blood - pool che meglio dimostra , rispetto ai mezzi di contrasto tc ed rm , laumentata vascolarizzazione su base infiammatoria dellansa intestinale affetta . 
tuttavia tale metodica gravata da svantaggi fra i quali la stretta dipendenza dalla perizia delloperatore , labitus del paziente , il meteorismo intestinale e non ultimo la mancanza di panoramicit [ 31 ]  . 
di conseguenza il ruolo del ceus diventa quello di effettuare lo studio di particolare di una lesione diagnosticata tramite unaltra metodica imaging [ 11 , 23 ]  . la sovrapponibilit delle curve di ce delle indagini ceus e rm ha confermato la loro accuratezza nel valutare la vascolarizzazione della parete intestinale . 
come gi riradiol med ( 2012 ) 117 : 268281 disadvantages , such as operator - skill dependence , patient bmi , intestinal gas and the lack of a panoramic view [ 31 ]  . 
 therefore , we argue that ceus could serve as a diagnostic tool to better estimate a particular lesion already diagnosed by another imaging technique [ 11 , 23 ]  . time - intensity curves at ceus and mri confirmed the accuracy of the technique for assessing intestinal - wall vascularity . 
as also reported by quaia et al . , quantitative analysis of enhancement patterns allows a more precise assessment of parietal enhancement with a lower influence of subjective visual assessment related to observer experience [ 32 ]  . 
 these differences were due to two main factors : the first is the development of fibrous scar tissue , which leads to delayed enhancement in the venous phase at mri . 
the second depends on the pharmacodynamic differences of the two contrast agents used : gadolinium chelates tend , after an initial vascular period , to migrate and then to accumulate in the interstitium , including the fibrous tissue of chronic wounds , whereas us contrast agents consist of gas microbubbles that remain for the entire time inside the microcirculation and break up in the vascular systethese blood - pool contrast agents only lead to enhancement of the anatomical structures that have an effective increase in the microand / or macrovascular network , but they are not retained in fibrous tissue . 
in our study , the parameters that better correlate with disease activity are wall thickening ; homogeneous , early and intense enhancement of lesions , especially in the arterial phase ; the comb sign ; and reactive lymphadenopathy . 
in our study , we did not evaluate the type of enhancement owing to the small number of patients enrolled and the fact that our study aimed to compare wall - enhancement curves between ceus and mri . our study has some limitations : we did not consider parameters such as small wall ulcerations , fistulas and possible neoplastic degeneration ; these findings are relatively infrequent , and ceus is inaccurate in evaluating thefurthermore , these parameters are not closely related to disease activity . 
le differenze rilevate a carico delle lesioni in fase cronica , che hanno mostrato un discreto enhancement alla rm , non mostrando significativa impregnazione al ceus , sono da ricondurre a due importanti fattori : il primo rappresentato dallo sviluppo di tessuto fibroso e cicatriziale in corrispondenza di tali lesioni che le rende capaci di impregnarsi in fase contrastografica venosa / tardiva . 
il secondo dipende dalle differenze di natura farmacodinamica dei 2 mdc impiegati : mentre i chelati del gadolinio tendono , dopo un primo periodo definito vascolare , a migrare e quindi ad accumularsi nellinterstizio , ivi compreso il tessuto fibroso delle lesioni croniche , il mdc ecografico costituito da microbolle di gas che restano , per tutto il tempo compreso fra la loro immissione in circolo e la loro rottura , allinterno del sistema vascolare . 
i mezzi di contrasto blood - pool causano quindi un rinforzo delle sole strutture che presentano un aumento concreto del micro e / o del macro - circolo ma non ristagnano nel tessuto fibroso . 
 [ 26 ] , non abbiamo focalizzato la nostra attenzione solo sulla vascolarizzazione della parete intestinale , valutando anche altri parametri morfologici e cercando di effettuare una valutazione globale di attivit di malattia . 
nel nostro studio , i parametri che meglio correlano con lattivit di malattia sono lispessimento parietale , lenhancement omogeneo , precoce ed intenso delle lesioni , soprattutto se limitato alla fase arteriosa , il segno del pettine e le linfoadenopatie reattive . 
nel nostro studio non abbiamo valutato il tipo di impregnazione dato lesiguo numero di pazienti arruolati e per il fatto che il nostro studio intende paragonare le curve di impregnazione di parete tra il ceus e la rm . il nostro lavoro presenta alcuni limiti : non abbiamo considerato parametri quali le ulcerazioni parietali , le fistole , e leventuale degenerazione neoplastica : oltre ad essere reperti relativamente infrequenti , non sono sempre valutabili in corso di ceus in relazione alla sua mancanza di panoramicit . 
we selected only patients with single lesions because the diagnosis of cd is established very early , and most patients are diagnosed with only one location of inflammation . conclusions the use of ceus allows evaluation of bowel - wall vascularity in patients with cd . 
the high number of false positive results , however , associated with the limits of the time - intensity curves , makes the technique difficult to use in daily clinical practice . 
mri of the small bowel still remains the most accurate method for evaluating disease activity . nella realt clinica la maggior parte dei pazienti presenta pi anse intestinali colpite con interessamento spesso del colon . 
inoltre nel tempo spesso vi la comparsa di ulteriori lesioni rispetto al precedente controllo . conclusioni lutilizzo dellecografia con mezzo di contrasto permette una valutazione della vascolarizzazione della parete intestinale in pazienti con mc . 
 i valori di fe - 1 sono stati utilizzati per quantificare la riserva pancreatica esocrina ; successivamente i pazienti sono stati suddivisi in due gruppi a seconda di un valore soglia clinico di fe - 1 di 200 g / g . 
la cprmq risultata significativamente differente ( p = 0 , 007 ) tra il gruppo con funzione pancreatica ridotta e quello con funzione normale ; mediana e range interquartilico ( iqr ) sono stati di 150 , 7 ml ( 137 , 3205 , 5 ml ; n = 9 ) e 332 , 4 ml ( 190 , 6506 , 9 ml ; n = 26 )  . 
possibile discriminare una funzione pancreatica esocrina conservata da una ridotta per mezzo della cprmq . parole chiave cprmq pancreatite cronica riserva esocrina pancreatica risonanza magnetica quantitativa secretina introduction introduzione chronic pancreatitis is an inflammatory and sclerotic process responsible for irreversible morphological changes of the pancreatic parenchyma and ducts , with progressive loss of exocrine function probably due to ischaemic events [ 1 , 2 ]  . 
therefore , the pancreatic functional exocrine reserve may represent an index of disease evolution and thus contribute to therapeutic planning . pancreatic functional exocrine reserve can be measured through various direct and indirect methods , all affected by intrinsic limitations [ 3 , 4 ]  . 
direct techniques , despite their high sensitivity ( 7490% ) , are invasive , expensive and time consuming , as they require duodenal intubation in order to collect pancreatic juice , with potential morbidity [ 5 , 6 ]  . 
regardless , previous studies demonstrate a good correlation between the secretin cerulein test and fe - 1 , suggesting that it has a possible role in evaluating exocrine pancreatic function [ 10 , 11 ]  . dynamic magnetic resonance cholangiopancreatography ( mrcp ) during intravenous administration of secretin ( s - mrcp ) improves mrcp sensitivity in diagnosing morphological changes in chronic pancreatitis and allows a semiquantitative measurement of pancreatic exocrine reserve by monitoring duodenal filling [ 12 , 13 ]  . 
recent published series have shown the feasibility of s - mrcp in quantifying pancreatic exocrine reserve by demonstrating a linear relationship between mr signal intensity , as measured in the duodenal lumen , and fluid volume [ 1315 ]  . 
these methods , however , require a calibration procedure that lengthens imaging time . la pancreatite cronica un processo infiammatorio e sclerotico , responsabile di modificazioni morfologiche irreversibili , sia del parenchima che dei dotti pancreatici , con una progressiva perdita di funzione esocrina , probabilmente dovuta a processi ischemici [ 1 , 2 ]  . 
conseguentemente la riserva funzionale pancreatica esocrina potrebbe rappresentare un indice dellevoluzione della malattia e contribuire alle decisioni terapeutiche . la riserva funzionale pancreatica esocrina pu essere misurata attraverso vari metodi diretti ed indiretti , tutti affetti da limitazioni intrinseche [ 3 , 4 ]  . 
le tecniche dirette , nonostante la loro alta sensibilit ( 74%90% ) , sono invasive , costose e di lunga esecuzione , dal momento che necessitano dellintubazione duodenale per la raccolta del succo pancreatico , con potenziale morbilit associata [ 5 , 6 ]  . 
i test indiretti determinano la funzione pancreatica esocrina misurando i prodotti della degradazione dei substrati ad opera degli enzimi digestivi nelle feci . lelastasi fecale - 1 ( fe - 1 ) un test che valuta la funzione pancreatica esocrina in modo diretto . 
nonostante ci , alcuni studi dimostrano una buona correlazione tra il test secretina - ceruleina ed il test dellelastasi fecale , suggerendo il suo possibile ruolo nella valutazione della riserva funzionale ed esocrina pancreatica [ 10 , 11 ]  . 
 la colangiopancreatografia dinamica con risonanza magnetica durante liniezione intravenosa di secretina ( scprm ) , migliora la sensibilit della cprm nella diagnosi delle alterazioni morfologiche nel corso di pancreatite cronica , e permette una misura semi - quantitativa della riserva pancreatica esocrina tramite la valutazione del riempimento duodenale [ 12 , 13 ]  . 
dati pubblicati di recente hanno dimostrato la capacit della s - cprm nel quantificare la riserva pancreatica esocrina dimostrando una relazione lineare tra lintensit di segnale nel lume duodenale 284 radiol med ( 2012 ) 117 : 282292 the purpose of this study was to investigate whether a simplified quantification method using s - mrcp can quantitatively discriminate patients with preserved pancreatic exocrine reserve from those with impaired exocrine reserve , as determined using clinical criteria . materials and methods for the purpose of this study , patients with recurrent pancreatitis defined as at least two episodes of abdominal pain and at least a three - fold increase of serum amylases and lipases were enrolled . 
the final diagnosis of chronic pancreatitis was made on compatible morphologic changes at imaging ( dilation > 6 mm of main pancreatic duct , presence of pancreatic calcifications , glandular atrophy , side branch duct dilation )  . 
 exclusion criteria were patients with a time interval 6 months between s - mrcp and fe - 1 test ( two patients ) , who previously underwent surgery ( four patients ) and with insufficient quality of mri ( two patients )  . 
thus our study population consisted of 35 patients , 25 men and ten women , with a mean age of 53 ( range 3074 ) years . pancreatic exocrine reserve was determined in all patients using the fe - 1 test , and results were determined using sandwich enzyme - linked immunosorbent assay ( elisa ) test , with two monoclonal antibodies that exclusively bind to human elastase - 1 . 
elastase concentration was then determined by a photometric method . according to the results of the fe - 1 test , patients were divided into two groups using a threshold value of 200 g / g , as commonly employed in clinical practice : patients with preserved pancreatic exocrine reserve ( n = 26 ) and patients with impaired pancreatic exocrine reserve ( n = 9 )  . 
subsequently all patients underwent s - mrcp examination , with a mean time interval of 23.6 ( range 0164 ) days between the s - mrcp and the fe - 1 test . 
 mr technique mri was performed on a 1.5 - t scanner ( magnetom symphony , siemens , erlangen , germany ) with a 4 - channel phased - array coil . 
 the mri protocol included chemical - shift t1 - weighted gradient - echo axial images , with time of echo ( te ) both in phase and out of phase , with the following parameters : time in risonanza magnetica e il volume fluido [ 1315 ]  . 
questi metodi tuttavia necessitano una calibrazione pre - esame che allunga il tempo di studio . lo scopo di questo studio quello di investigare la possibilit di discriminare pazienti con una riserva pancreatica esocrina conservata da quelli con una riserva esocrina ridotta , cos come classificati sui dati clinici , attraverso un metodo di quantificazione s - cprm semplificato . materiali e metodi ai fini dello studio sono stati arruolati i pazienti affetti da pancreatiti ricorrenti , definite come almeno due episodi di dolore addominale ed almeno un aumento di tre volte delle amilasi e delle lipasi sieriche . 
la diagnosi finale di pancreatite cronica stata fatta sulle alterazioni morfologiche compatibili con pancreatite cronica allimaging ( dilatazione > 6 mm del dotto pancreatico principale , presenza di calcificazioni pancreatiche , atrofia del parenchima , dilatazione dei dotti secondari )  . 
i criteri di inclusione sono stati : pazienti con pancreatite cronica , con accertamento clinico della riserva pancreatica esocrina per mezzo dellfe - 1 ed esame cprm con stimolo secretinico . 
i criteri di esclusione sono stati : pazienti con un intervallo maggiore di sei mesi tra esame di risonanza magnetica ed il test clinico ( 2 pazienti ) , pazienti che erano stati precedentemente sottoposti a chirurgia ( 4 pazienti ) , pazienti con uninsufficiente qualit delle immagini di risonanza magnetica ( 2 pazienti )  . 
conseguentemente il nostro studio comprendeva una popolazione di 35 pazienti , di cui 25 maschi e 10 femmine , con unet media di 53 anni , variando dai 30 ai 74 . la riserva pancreatica esocrina stata determinata in tutti i pazienti per mezzo del test della elastasi fecale . 
i valori della fe - 1 sono stati ottenuti tramite un test sandwich enzyme - linked immunosorbent assay ( elisa ) , con due anticorpi monoclonali che si legano esclusivamente alla elastasi umana - 1 . 
la concentrazione di elastasi stata successivamente determinata con un metodo fotometrico . basandosi sui risultati del test fe - 1 , la popolazione dei pazienti stata divisa in due gruppi , usando un valore soglia di 200 g / g , cos come comunemente utilizzato nella pratica clinica . 
conseguentemente la popolazione dei pazienti stata sottodivisa in pazienti con una riserva pancreatica esocrina conservata ( n = 26 ) e pazienti con una riserva pancreatica esocrina ridotta ( n = 9 )  . 
successivamente tutti pazienti sono stati sottoposti a s - cprm , con un intervallo di tempo medio di 23 , 6 giorni ( variando da 0 a 164 giorni )  . radiol med ( 2012 ) 117 : 282292 of repetition ( tr ) / te 107160 / 2.44.8 ms , slice thickness 7 m axial fat - saturated t2 - weighted rapid acquisition with relaxation enhancement ( rare ) images were also obtained with the following parameters : tr / te 4 , 000 4950 / 91102 ms , slice thickness 7 mcoronal and axial t2 - weighted half - fourier rare [ half - fourier single - shot turbo spin - echo ( haste ) ] images were obtained with the following parameters : tr / te / 60102 ms , slice thickness 46 mm , with no slice gap . 
subsequently , this sequence was also acquired along the sagittal and coronal oblique planes according to different angulations of the longest diameter of the pancreas to optimise depiction of the pancreatic ductal syste when the most appropriate plane for investigating the biliary and pancreatic ductal systems was identified , mrcp was performed with a heavily t2 - weighted 2d haste pulse sequence , along the coronal / coronaloblique plane , during a single breathhold . 
imaging parameters were tr / te / 1 , 100 ms , field of view ( fov ) 320 mm , matrix size 348348 , slice thickness 6585 mm , to encompass the entire pancreatic duct system and the biliary tree , including papillae , duodenum and small bowel . 
after the first dynamic acquisition , a bolus of secretin was injected intravenously at a dose of 1 cu / kg body weight ( secrelux , sanochemia , neuss , germany )  . 
ten minutes after secretin administration , a coronal t2 - weighted 2d haste sequence was obtained with the following parameters : tr / te / 60102 ; echo train length 128 ; slice thickness 46 mm with no interslice gap . image analysis image analysis was performed by two radiologists ( rm , sp ) with different levels of expertise in biliary and pancreatic imaging ( 14 and 3 years , respectively ) , without knowledge of clinical and fe - 1 data . 
a semiquantitative evaluation of duodenal filling , a function of pancreatic exocrine secretion , was performed on mrcp images obtained 10 min after secretin injection and compared with mrcp images acquired before secretin administration . 
subsequently , a quantitative analysis of duodenal filling was performed by measuring the volume of fluid present within the duodenal lumen on half - fourier tecnica di risonanza magnetica limaging di risonanza magnetica ( rm ) stato eseguito su uno scanner da 1 , 5 t ( magnetom symphony , siemens , erlangen , germania ) , usando una bobina phased array a 4 canali . 
il protocollo di studio rm includeva immagini chemical shift imaging ( csi ) gradient echo t1 - dipendenti assiali , con tempo di eco ( te ) sia in fase che fuori fase , con i seguenti parametri : tempo di ripetizione ( tr ) / te 107 160 / 2 , 44 , 8 ms , slice thickness 7 mm . sono state anche ottenute immagini assiali t2 - dipendenti con saturazione del grasso di tipo rapid acquisition with relaxation enhancement ( rare ) con le seguenti parametri : tr / te 40004950 / 91102 ms , slice thickness 7 m immagini coronali ed assiali t2 - dipendenti di tipo halffourier rare ( half fourier single - shot turbo epin - echo , haste ) sono state ottenute con i seguenti parametri : tr / te / 60102 ms , slice thickness 46 mm , a strati contigui . 
 successivamente questa sequenza stata anche acquisita lungo i piani sagittale e coronale obliquo secondo la differente angolazione del diametro lungo del pancreas , in modo da ottimizzare la visualizzazione del sistema duttale . 
una volta identificato il piano pi appropriato per analizzare il sistema duttale pancreatico e biliare , la cprm stata eseguita con una sequenza pulsata bidimensionale haste pesantemente t2 - dipendente , lungo il piano coronale / coronale obliquo , durante lapnea , con i seguenti parametri : tr / te / 1100 ms , campo di vista ( fov ) 320 mm , matrix size 348348 , slice thickness 6585 mm , in modo da comprendere lintero sistema pancreatico duttale e lalbero biliare , includendo entrambe le papille , il duodeno e il piccolo intestino . 
dopo la prima acquisizione dinamica , un bolo di secretina stato iniettato endovena alla dose di 1 unit clinica per chilogrammo di peso corporeo ( secrelux , sanochemia , neuss , germania )  . 
dieci minuti dopo la somministrazione di secretina stata applicata una sequenza coronale t2 - dipendente bidimensionale haste con i seguenti parametri : tr / te / 60102 ; echo train length 128 ; slice thickness 46 mm a strati contigui . analisi delle immagini lanalisi delle immagini stata eseguita da due radiologi ( rm , sp ) con diverso livello di esperienza nellimaging pancreatico e biliare ( 14 anni e tre anni rispettivamente ) , senza conoscenza dei dati clinici e dei dati di fe - 1 . 
from the duodenal filling volume , calculated as described above , the volume of fluid present within the duodenal lumen , calculated on coronal t2 - weighted half - fourier images before secretin administration , was subtracted . 
finally , measurements of the pancreatic functional exocrine reserve were compared with the fe - 1 values . statistical analysis continuous variables are described using median value and interquartile range ( iqr ) ( 25 ; 75 percentile ) as central tendency and dispersion values , respectively , whereas categorical variables are described as numbers and percentages . 
differences between subgroups ( pancreatic functional reserve insufficient or maintained ) were evaluated using semiquantitativa del riempimento duodenale , funzione della secrezione esocrina pancreatica , sulle immagini di cprm ottenute 10 minuti dopo liniezione di secretina , a confronto con le immagini di cprm ottenute prima della somministrazione del farmaco . 
per garantire laccuratezza il software stato dapprima calibrato con le immagini di risonanza specificando la dimensione della matrice , il campo di vista , lo spessore e lintervallo di fetta . 
la superficie del riempimento duodenale stata contornata a mano libera , tuttavia lasciando che il software suggerisse in tempo reale un tragitto compatibile , sulle immagini ottenute 10 minuti dopo la iniezione di secretina . 
dal volume di riempimento duodenale , calcolato con il metodo descritto , stato sottratto il volume del fluido presente nel lume duodenale calcolato similmente sulle immagini coronali t2 - dipendenti haste prima della somministrazione di secretina . 
infine , le misure della riserva funzionale esocrina pancreatica sono state comparate tra loro e con i valori di fe - 1 . analisi statistica le variabili continue sono state descritte usando i valori mediani e il range interquartilico ( iqr ) ( 25 e 75 percentile ) come valore centrale e valore di dispersione , mentre le variabili categoriche sono state descritte con numeri e percentuali . 
le differenze tra i sottogruppi ( riserva pancreatica esocrina ridotta o conservata ) sono state analizzate tramite un test u di mann - whitney per le variabili continue dopo unappropriata trasformazione su una scala ordinale . 
le differenze tra i gruppi ( riserva pancreatica esocrina conservata o ridotta ) sono state valutate per mezzo di un test u di mann - whitney , dopo unappropriata trasformazione su una scala ordinale . 
the relationship between measurements of the pancreatic juice and fe - 1 was evaluated using pearson risultati elastasi fecale - 1 complessivamente , il valore medio di fe - 1 misurato nella popolazione dei pazienti stato di 335 , 26 g / g di feci , con una mediana di 331 g / g , variando da 0 , 6 g / g a 587 , 6 g / g . 
in the group of patients ( n = 9 ) with impaired fe - 1 values ( < 200 g / g of stool ) , mean fe - 1 value was 55.8 g / g of stool , with median 49.3 g / g and range 0.6127.3 g / g ( table 1 )  . semiquantitative image analysis ten minutes after secretin administration , 29 / 35 ( 82% ) patients showed a duodenal filling beyond the genu inferius ( grade 3 ) ; whereas 6 / 35 ( 18% ) showed a duodenal filling up to the genu inferius ( grade 2 ) [ 16 ]  . 
 analisi semi - quantitativa dieci minuti dopo la somministrazione di secretina , 29 dei 35 pazienti ( 82% ) hanno mostrato un riempimento duodenale oltre il ginocchio inferiore ( grado 3 ) ; mentre 6 dei 35 pazienti ( 18% ) hanno mostrato un riempimento duodena le che non raggiunge il ginocchio inferiore ( grado 2 ) [ 16 ]  . 
 la concordanza inter - osservatore stata del 100% ( ta bella 2 )  . il confronto tra le misurazioni semiquantitative del riempimento duodenale , misurato sulle immagini s - cprm ottenute 10 minuti dopo secretina , e lfe - 1 riportato in tabella 2 . 
da sottolineare che tutti i pazienti con riserva pancreatica esocrina ridotta ( n = 9 , fe - 1 < 200 g / g ) hanno mostrato un riempimento duodenale oltre il ginocchio inferiore ( grado 3 ) ( tabella 2 )  . analisi quantitativa delle immagini il volume di riempimento duodenale medio stato di 307 , 36 ml , con valore mediano di 308 , 55 ml , e range tra 70 , 19 ml e 696 , 44 ml . 
la differenza tra il gruppo con funzione conservata e quello con funzione ridotta , valutato tramite il test u di mann - whitney , risultata significativa , con una p = 0 , 007 ( tabella 3 )  . radiol med ( 2012 ) 117 : 282292 table 2 distribution of semiquantitative score [ 16 ] among patients with impaired or preserved pancreatic exocrine reserve s - mrcp semiquantitative assessment patients with impaired pancreatic function ( fe - 1 < 200 g / g ) patients with preserved pancreatic function ( fe - 1 > 200 g / g ) overall s - mrcp , magnetic resonance cholangiopancreatography during intravenous administration of secretin ; fe - 1 , faecal elastase - 1 tabella 2 distribuzione dei gradi semi - quantitativi [ 16 ] tra i pazienti con riserva funzionale pancreatica ridotta o conservata pazienti con funzione pancreatica ridotta ( fe - 1 < 200 g / g ) pazienti con funzione pancreatica conservata ( fe - 1 > 200 g / g ) totale limited to the duodenal bulb ( grade 1 ) up to the genu inferius ( grade 2 ) beyond the genu inferius ( grade 3 ) total s - cprm valutazione semi - quantitativa limitato al bulbo duodenale ( grado 1 ) fino al ginocchio inferiore ( grado 2 ) oltre il ginocchio inferiore ( grado 3 ) totale s - mrcp , colangiopancreatografia con risonanza magnetica durante somministrazione intravenosa di secretina ; fe - 1 , elastasi - 1 fecale comparison between semiquantitative measurement of duodenal filling , assessed on the s - mrcp images obtained 10 min following secretin administration , and fe - 1 determinations is reported in table 2 . 
mean duodenal filling volume for the group of patients with impaired fe - 1 ( < 200 g / g of stool ) was 178.87 ml , with median 150.67 ml and range 133.26311.56 ml ( table 3 )  . 
 mean duodenal filling volume for the group of patients with preserved ( > 200 g / g of stool ) fe - 1 was 342.89 ml , with median 332.43 ml and range 70.19696.44 ml ( table 3 )  . 
the difference between the preserved function group and the impaired function group , as evaluated by the mannwhitney u test , was significant , with p = 0.007 ( table 3 )  . discussion measurement of the pancreatic exocrine reserve in patients with chronic pancreatitis or recurrent acute pancreatitis is important for monitoring disease evolution and treatment planning [ 17 ]  . 
pancreatic exocrine reserve is routinely discussione la misurazione della riserva pancreatica esocrina , nei pazienti con pancreatite cronica o con pancreatite acute ricorrenti , importante nel monitorare levoluzione della malattia e pianificarne il trattamento [ 17 ]  . 
recentemente c stato un rinnovato interesse nello sviluppo e nella comprensione del potenziale ruolo della tecnica cprm dinamica durante stimolo secretinico , nello studio della fisiologia pancreatica , ed in particolar modo nella valutazione della riserva funzionale esocrina pancreatica , per mezzo di metodi semiquantitativi e quantitativi [ 18 ]  . 
dal momento che la cprm rappresenta attualmente la miglior metodica per lesplorazione dellanatomia duttale nella malattia pancreatico - biliare [ 19 ] , tale tecnica andrebbe a rendere lesame di risonanza magnetica ancora pi informativo in questi pazienti . 
 le misurazioni semiquantitative ottenute per mezzo della cprm dopo stimolo secretinico possono essere facilmente eseguite nella pratica clinica ; tuttavia questo metodo non in grado di valutare modeste riduzioni della riserva pancreatica esocrina , cos come evidenziato anche dai risultati del nostro studio . 
al fine di superare questo limite documentato della tecnica s - cprm nel valutare la riserva pancreatica esocrina , metodi quantitativi sono stati proposti ed analizzati per determinare in modo accurato la funzione pancreatica esocrina [ 1315 ]  . 
recently , there has been a renewed interest in developing and understanding the potential role of dynamic mrcp during secretin stimulation for studying pancreatic physiology , namely , for assessing exocrine pancreatic functional reserve using semiquantitative and quantitative methods [ 18 ]  . 
given that the mrcp examination is considered the best option for exploring ductal anatomy in pancreatobiliary diseases [ 19 ] , this technique would prove mri even more useful in these patients . investigated the semiquantitative measurements obtained using mrcp after secretin stimulation can be easily performed in clinical practice ; however , the technique is not able to assess mild reductions in pancreatic exocrine reserve , as also indicated by the findings of our study . 
to overcome this known limitation of s - mrcp in assessing pancreatic exocrine reserve , quantitative methods have been proposed and to accurately determine pancreatic exocrine function [ 1315 ]  . 
 to propose the use of the s - mrcp examination along with the traditional noninvasive tests , it was necessary to calculate the correlation between output volumes and fe - 1 , as the latter is considered the reference test in clinical practice . 
 per proporre lesame s - cprm insieme ai tradizionali test non invasivi , stato necessario calcolare la correlazione tra i volumi di riempimento calcolati su queste immagini , e i valori di elastasi fecale , dal momento che questultimo esame considerato il test di riferimento nella pratica clinica . 
in b si evidenzia una abbondante secrezione che riempie lintero duodeno e scorre in parte attraverso le prime anse del piccolo intestino ( grado 3 )  . and whether this could be used to discriminate impaired pancreatic output from preserved output . 
therefore , when absolute values are required , methods that include voxel calibration are more accurate . another minor limitation may be represented by the numeric discrepancy between the number of patients with preserved pancreatic exocrine reserve at fe - 1 test ( n = 26 ) and the number of patients with impaired pancreatic exocrine reserve ( n = 9 )  . 
however , this is the expression of the higher number of patients with mild chronic pancreatitis and recurrent acute pancreatitis compared with severe chronic pancreatitis in clinical practice . despite the above limitations , our study confirmed the capability of mrcp images to quantitatively evaluate the pancreatic exocrine reserve , a finding in agreement with previous studies that differ from ours in terms of patient characteristics and imaging technique . 
di conseguenza quando si necessita di misurazioni assolute accurate , i metodi che includono la calibrazione del voxel sono pi esatti . un altro limite minore potrebbe essere rappresentato dalla discrepanza numerica tra il numero dei pazienti con riserva pancreatica esocrina conservata al test fe - 1 ( n = 26 ) e il numero dei pazienti con riserva pancreatica esocrina ridotta ( n = 9 )  . 
tuttavia questa lespressione del pi alto numero di pazienti con pancreatiti croniche e pancreatiti ricorrenti lievi , a confronto con la pancreatite cronica severa nella pratica clinica . nonostante i limiti sopracitati , il nostro studio ha confermato la capacit della cprm di valutare quantitativamente la riserva pancreatica esocrina , un risultato che in accordo con studi precedenti che differiscono in termini di caratteristiche dei pazienti e di tecniche di acquisizione . 
 la tecnica in grado di restituire sia una valutazione qualitativa che una quantitativa della riserva pancreatica allo stesso tempo , e pu quindi essere suggerita per monitorare 292 radiol med ( 2012 ) 117 : 282292 fore be suggested for monitoring the pancreatic exocrine reserve of patients affected by chronic or acute recurrent pancreatitis . 
la cprm quantitativa dopo stimolo secretinico correla significativamente con i valori di fe - 1 ( p < 0 , 001 ) , e pu essere usata per discriminare i pazienti con riserva funzionale esocrina conservata da quelli con funzione ridotta ( p = 0 , 007 )  . conflict of interest none radiol med ( 2012 ) 117 : 112124 doi 10.1007 / s11547 - 011 - 0678 - 5 dental radiology radiologia odontoiatrica assessing the need for computed tomography for lower - third - molar extraction : a survey among 322 dentists verifica della necessit di prescrizione di tomografia computerizzata per lestrazione dei terzi molari inferiori : indagine tra 322 dentisti s . 
berengo1 1department of oral surgery , institute of clinical dentistry , university of padova , via venezia 90 , 35100 padova , italy 2department of statistical science , university of padova , via c . 
orthopantomograms ( opt ) are used to assess the anatomical relationship between the inferior alveolar nerves ( ian ) and the roots of third molars and the related risk of postextraction iatrogenic neurological lesions . 
a total of 2 , 713 letters were sent to italian dentists ( veneto region ) , inviting them to access an internet web site showing 20 opts and answer a questionnaire on the need for ct or periapical x - ray . 
lortopantomografia ( opt ) utilizzata per valutare la vicinanza del nervo alveolare inferiore ( nai ) alle radici del terzo molare e il rischio di una lesione neurologica iatrogena post - estrattiva . 
sono state inviate 2713 lettere a dentisti italiani ( regione veneto ) , chiedendo di accedere ad un sito internet contenente 20 opt ed un questionario riguardanti lindicazione alla tc o alla radiografia endorale . 
il motivo principale per cui non viene prescritta la tc per la mancanza di necessit ai fini dellestrazione . radiol med ( 2012 ) 117 : 112124 not recommending ct was that it was unnecessary for the purposes of the extraction . 
il nostro studio ha rivelato una certa cautela dei professionisti che tendono a sovra - prescrivere la tc . parole chiave terzo molare inferiore ortopantomografia tomografia computerizzata indagine keywords lower third molar orthopantomogram computed tomography survey introduction introduzione surgical extraction of the lower - third molars is a routine procedure in oral surgery . 
it may be associated with complications , including transient or permanent lesions of the inferior alveolar nerve ( ian ) , with related sensory disorders of variable severity [ 1 , 2 ]  . 
the main risk factors for ian lesions during lowerthird - molar extraction include the depth of the tooths impaction , its angle of inclination , the use of ostectomy or odontotomy , the patients age and the finding of particular radiographic signs [ 4 , 5 ]  . 
this last risk factor explains why it is so important to accurately assess the anatomical relationship of the root of the wisdom tooth in relation to the mandibular canal [ 610 ]  . orthopantomography ( opt ) is indispensable for this purpose , but in some situations , it may prove inadequate , in which case computed tomography ( ct ) may be warranted [ 1 , 4 , 8 , 1114 ]  . 
the advisability of prescribing ct for lower third - molar extraction is controversial , however , because the dosebenefit and costbenefit ratios might be unfavourable [ 15 , 16 ]  . 
 the aim of this study was to investigate the perceived need for ct for lower - third - molar extraction based on the assessment of a set of opts by a sample of dentists practising in the veneto region ( northeast italy )  . 
pu essere associata ad alcune complicanze come lesioni transitorie o permanenti del nervo alveolare inferiore ( nai ) con alterazioni della sensibilit di varia entit [ 1 , 2 ]  . 
i maggiori fattori di rischio per le lesioni del nai durante lestrazione del terzo molare includono : la profondit dinclusione del dente , la sua angolazione , luso di osteotomia o odontotomia , let del paziente , e losservazione di particolari segni radiografici [ 4 , 5 ]  . 
questultimo fattore di rischio dimostra limportanza di accertare il rapporto anatomico tra le radici del dente del giudizio e il canale mandibolare [ 610 ]  . a tale scopo lortopantomografia ( opt ) indispensabile , ma in alcune situazioni in cui risulta inadeguata consigliato eseguire la tomografia computerizzata ( tc ) [ 1 , 4 , 8 , 1114 ]  . 
lappropriatezza della prescrizione della tc ai fini dellestrazione del terzo molare inferiore pu essere discutibile , poich i rapporti dose / beneficio e costo / beneficio potrebbero non essere favorevoli [ 15 , 16 ]  . 
le linee guida delle principali societ scientifiche invitano al rispetto dei principi di giustificazione e ottimizzazione nella prescrizione degli esami radiologici [ 1719 ]  . lo scopo di questo studio di verificare la percezione della necessit di tc per pazienti candidati allestrazione dei terzi molari inferiori , basandosi sulla valutazione dellopt da parte di un campione di dentisti operanti nel veneto ( nord - est dellitalia )  . 
 le valutazioni dei dentisti partecipanti al sondaggio sono state confrontate con quelle degli autori basate sulla tc e poi correlate con alcune caratteristiche dei partecipanti ( per esempio , et ed esperienza professionale )  . materials and methods materiali e metodi 114 survey for the purposes of this investigation , 20 opts were selected for which corresponding cts were available , relating to 20 patients requiring extraction of impacted lower - third molars . 
respondent characteristics : year of birth ; year of graduation from university ; years of dental practice ; weekly frequency of impacted third - molar extractions ( 01 ; 23 ; > 3 ) ; percentage of ian lesions experienced in their clinical practice ; specialisation ; 2 . 
opt characteristics : the 20 opts were displayed in sequence , each associated with the questions listed in table 1 . after completing the questionnaire , respondents could access a section providing instant feedback on the answers they had given based on the comments and assessments recorded by the radiologist and surgeon who coordinated the study . letters of invitation to participate in the survey were sent to 2 , 713 dentists practising in the region , and particularly in the cities of padova ( 1 , 102 ) , verona ( 946 ) and treviso ( 665 ) ; the dentists could access the site by entering a username and password . 
the final number of respondents was 322 , corresponding to 11.9% of the dentists contacted . statistical analysis radiol med ( 2012 ) 117 : 112124 indagine per questa indagine sono state selezionate 20 ortopantomografie e corrispondenti tomografie computerizzate di 20 pazienti che dovevano sottoporsi allintervento di estrazione del terzo molare mandibolare incluso . 
le opt scelte erano varie per tipologia di paziente ( et , sesso , ecc . ) e per rapporto anatomico tra la radice del dente incluso e il canale mandibolare . 
caratteristiche opt : le 20 opt sono visualizzate in sequenza e ad ognuna di esse sono associate le domande illustrate in tabella 1 . al termine della compilazione del questionario , il rispondente disponeva di una sezione di feedback che forniva un riscontro immediato circa le risposte date , basata sui commenti e le valutazioni del radiologo e del chirurgo che hanno coordinato lo studio . sono state inviate 2713 lettere a dentisti operanti nella regione , in particolare nelle citt di padova ( 1102 ) , di verona ( 946 ) , e di treviso ( 665 ) ; i dentisti potevano accedere al sito inserendo username e password necessari . 
 il numero dei rispondenti stato 322 , corrispondente al 11 , 9% dei dentisti contattati . to assess answers provided by dentists who judged the opts , we considered the corresponding cts analysed by the authors ( ss and gdc ) , i.e. 
can you identify one or more radiographic signs of potential problems in the anatomical relationship between the third molars and the mandibular canal ? the root and mandibular canal overlap the course of the mandibular canal is diverted there are gaps in the margins of the mandibular canal narrowing of the mandibular canal narrowing of the root the root is diverted loss of definition of the contours of the mandibular canal and / or root no 2 . 
if not , why not ? no yes because it is unnecessary for the purposes of the extraction because the radiation dose / benefit ratio is unfavourable because the cost / benefit ratio is unfavourable because it is difficult for the patient to access a radiology unit 4 . 
rileva uno o pi rapporti tra terzi molari ed il canale mandibolare ? sovrapposizione della radice con il canale candibolare deviazione della direzione del canale mandibolare interruzione del bordo del canale mandibolare restringimento del canale mandibolare restringimento della radice deviazione della radice perdita di definizione del contorno del canale e / o della radice nessuna relazione 2 . 
se non indicata , perch ? non necessaria ai fini dellestrazione perch non c un rapporto dose / beneficio perch non c un buon rapporto costo / beneficio per la difficolt di accesso ad un servizio di radiologia 4 . 
suitable measures of association ( dependence between nominal variables ) and cograduation ( dependence between ordinal variables ) were used to seek any correlation and dependence between the variables considered . 
for the associations , zione del canale mandibolare in relazione al terzo molare mandibolare [ 8 , 14 , 20 , 21 ]  . analisi dei dati in primo luogo sono state analizzate le relazioni fra attivit e caratteristiche dei rispondenti . 
per verificare la sussistenza di relazioni e dipendenze tra le variabili di volta in volta considerate , si fatto ricorso ad appropriate misure di asso116 radiol med ( 2012 ) 117 : 112124 we used the chi - square statistic and the corresponding standardised measure , cramers v statistic , which ranges between 0 ( stochastic independence ) and 1 ( perfect association ) ; for both measures , the chi - square distribution with a significance level of 95% was used [ 22 ]  . 
for cograduation , we used the goodmankruskal gamma coefficient , which ranges between 1 ( a perfectly inverse relationship ) and 1 ( a perfectly direct relationship ) , where 0 represents the order independence ; the related approximated test to verify the hypothesis has a students t distribution ( here again , we set the level of significance at 95% ) [ 23 ]  . 
the propensity index ( pi ) ranged between 1 ( nonchalant , failing to recommend ct when it would be useful ) and 1 ( cautious , recommending ct even when it is unnecessary )  . 
total indices ( tai and tpi ) were obtained for all dentists . ciazione ( dipendenza tra variabili di tipo nominale ) e cograduazione ( dipendenza tra variabili di tipo ordinale )  . 
nel caso dellassociazione si sono considerati gli indici chi quadrato e la corrispondente misura standardizzata , lindice v di cramr , che varia tra 0 ( indipendenza stocastica ) e 1 ( associazione perfetta ) : per entrambe le misure viene utilizzato il test di verifica dipotesi del chi quadrato con un livello di significativit del 95% [ 22 ]  . 
nel caso della cograduazione stato utilizzato il coefficiente di goodman - kruskal che varia tra 1 ( relazione perfetta inversa ) e 1 ( relazione perfetta diretta ) , con lo 0 che rappresenta lindipendenza dordine ; il relativo test di verifica dipotesi , approssimato , ha distribuzione secondo il test t di student ( livello di significativit utilizzato pari al 95% ) [ 23 ]  . 
la seconda parte del lavoro finalizzata a valutare le risposte date dai dentisti relativamente alle 20 opt , in termini di correttezza delle valutazioni e di propensione a richiedere la tc . 
 per studiare la correttezza e la propensione sono stati creati degli appositi indici , indice di correttezza ( ic ) e indice di propensione ( ip ) , calcolati con riferimento ad ogni dentista . 
lip varia tra 1 ( massima leggerezza , non prescrizione di tc quando servirebbe ) e 1 ( massima cautela , prescrizione di tc quando non servirebbe ) ; il valore 0 indica la neutralit . 
sono stati ricavati i rispettivi indici complessivi ( ict e ipt ) , relativi a tutti i dentisti . results respondents personal and professional characteristics risultati the sample consisted of 280 men ( 87% ) and 41 women ( 13% ) , for a total of 321 ( one respondent failed to state their gender )  . 
assuming that the 20to 64 - year age distribution of the veneto population is a proxy of the age distribution of dentists in the same region , we compared age distributions of respondents and the veneto population . 
more than 60% of respondents had < 20 years of professional experience . there was a direct relationship between the mean number of lower - third - molar extractions performed per week and the reported occurrence of ian lesions , particularly when dentists performing 01 procedure a week ( who reported a 15.9% rate of ian lesions ) were compared with those caratteristiche e attivit professionale degli intervistati il campione composto da 280 ( 87 , 0% ) maschi e 41 ( 13% ) femmine per un totale di 321 rispondenti ( 1 intervistato non ha dichiarato il genere )  . 
si tratta di un tasso di risposta piuttosto basso , ma riteniamo che la popolazione indagata non sia sistematicamente distorta e si possa pertanto considerare affidabili i risultati ottenuti dallindagine . 
infatti , sulla base dellipotesi , del tutto plausibile , che la distribuzione per et fra i 25 e i 64 anni dei dentisti del veneto sia pari a quella della popolazione veneta , si proceduto con un confronto della distribuzione per et dei rispondenti allindagine con quella della popolazione veneta . 
mediante il test non parametrico di wilcoxon [ 24 ] sulle classi quinquennali det abbiamo verificato che le due distribuzioni per et non sono significativamente diverse ( p = 0 , 48 )  . 
let media dei rispondenti pari a 42 , 6 anni ( maschi 43 , 8 anni ; femmine 34 , 4 ) ; il 3 , 4% ha unet fino a 25 anni , il 28 , 0% da 26 a 35 , il 24 , 9% da 36 a 45 , il 31 , 5% da 46 a 55 e il radiol med ( 2012 ) 117 : 112124 table 2 distribution of respondents by number of impacted lower - third - molar extractions performed per week and inferior alveolar nerve lesions reported . 
 risposte mancate n = 9 ( 2 , 8% ) lesione numero interventi , n ( % ) performing these extractions more frequently ( the reported rate of ian lesions was 32.9% for dentists performing 23 procedures a week , and 29.4% for those performing more than three a week ) ( table 2 )  . 
five of the other respondents had more than two specialist qualifications and the remaining either did not say or had none . opt assessment concerning the anatomical relationship between the lowerthird molar and the mandibular canal , the situation most often reported by respondents , judging from the calculation of the weighted mean ( the mean of the number of reports from each dentist , each weighted according to the total number of opts analysed by the dentist concerned ) , was 12 , 1% pi di 56 anni . 
pi del 60% dei rispondenti ha meno di 20 anni di anzianit professionale . si constatata una relazione diretta tra numero medio settimanale di interventi di estrazione chirurgica dei terzi molari inferiori e numero di lesioni del nervo alveolare inferiore riscontrate , in particolare fra chi fa 0 o 1 intervento a settimana ( 15 , 9% di lesioni ) rispetto a chi ne fa di pi ( 32 , 9% per 23 interventi alla settimana e 29 , 4% per pi di 3 ) ( tabella 2 ) ; il coefficiente di goodman - kruskal ( 0 , 40 ) rivela una forte dipendenza positiva ( p = 0 , 005 )  . 
per contro non si rilevata una particolare significativa relazione tra gli anni di pratica clinica e il numero di procedure eseguite per settimana ( p = 0 , 067 )  . per quanto riguarda la specializzazione dei professionisti , i rispondenti devono essere suddivisi tra coloro che sono laureati in medicina ( 135 ) e quelli che sono laureati in odontoiatria ( 160 ) ; la somma superiore al numero di rispondenti che hanno valutato le opt perch alcuni non hanno concluso lintervista . 
cinque tra i rispondenti hanno pi di due specializzazioni e gli altri la possiedono o non lhanno specificato . analisi delle opt per quanto riguarda i rapporti fra terzo molare e canale mandibolare , la relazione maggiormente rilevata dagli intervistati , secondo il calcolo di una media ponderata , 118 radiol med ( 2012 ) 117 : 112124 fig . 
1 comparison between the number of radiographic signs suggesting an intimate anatomical relationship between the inferior alveolar nerves and the roots of the third molar on orthopantomograms ( opts ) and the recommendations for computed tomography ( ct ) for all 20 opts examined . 
percentuale richiesta tc = 0 , 030 ( numero relazioni ) 2 + 0 , 380 ( numero relazioni ) 0 , 026 . percentage of cts recommended 0.030 ( number of radiographic signs ) 2 + 0.380 ( number of radiographic signs ) 0.026 a root overlapping the mandibular canal . 
the third was a gap in the margins of the mandibular canal . the larger the number of radiographic signs on a given opt , the stronger the recommendation for ct , with a deterministic trend . 
the curve plotted in figure 1 ( representing the percentage of recommendations for ct as a function of the number of radiographic signs identified ) shows a nearperfect correlation between the two variables ( r2 = 0.958 ) estimated by means of a parabolic curve . 
 concordance between the dentists recommendations and the gold standard the proportion of dentists opinions in agreement with the gold standard ranged from 21.8% ( minimum concordance ) for opt no . 
on the whole , 78.9% of dentists were in agreement with the gold standard in at least 75% of opts ( based on the 215 dentists who assessed 20 opts )  . 
the appropriateness of dentists opinions was unrelated to their years of professional activity , as the goodmankruskal - coefficient amounted to 0.057 and was not significant ( p = 0.61 ) , whereas it did seem to depend slightly , though not to a statistically significant degree , on the number of procedures performed per week ( goodmankruskal = 0.231 , p = 0.062 ) ( table 4 )  . 
the total propensity index , measuring dentists tendency to be cautious or nonchalant in recommending ct , amounted to 0.116 , revealing a slight tendency to err on the side of caution . 
when ct was not recommended , the main reasons were because it is ( media del numero di relazioni di ogni dentista , ognuna pesata col numero totale di opt analizzate dal dentista ) stata la sovrapposizione della radice con il canale mandibolare ; la seconda la perdita di definizione del contorno del canale e / o della radice e la terza linterruzione del bordo del canale mandibolare . maggiore il numero di segni radiografici allopt pi forte lindicazione alla tc con un trend deterministico : la curva illustrata in figura 1 ( rappresentante la percentuale di richieste di tc in funzione del numero di relazioni rilevate ) mostra una relazione quasi perfetta fra le due variabili ( correlazione r2 = 0 , 958 ) , stimata mediante una curva parabolica . 
 concordanza fra indicazioni dei dentisti e gold standard la percentuale di giudizi concordanti con il gold standard varia tra il 21 , 8% ( minima concordanza ) della opt 6 al 93 , 0% ( massima concordanza ) della opt 14 ( tabella 3 )  . 
la correttezza dei dentisti non correlata agli anni di attivit professionale , dato che il coefficiente di goodman - kruskal 0 , 057 e non significativo ( p = 0 , 61 ) , mentre sembra dipendere lievemente , anche se non con un grado di significativit statistica rilevante , dal numero di interventi eseguiti a settimana ( di goodman - kruskal = 0 , 231 , p = 0 , 062 ) ( tabella 4 )  . 
tra i dentisti che non avrebbero raccomandato la tc , il 55% avrebbe eseguito una radiografia periapicale , mentre il restante 45% non 120 radiol med ( 2012 ) 117 : 112124 table 4 distribution of dentists by number of impacted third - molar - extraction procedures performed per week and appropriateness index . 
dati mancanti : 5 ( 1.6% ) indice di correttezza dentisti totali 0 , 0000 , 635 0 , 6361 , 000 unnecessary for the purposes of the extraction unfavourable radiation dose / benefit ratio unfavourable cost / benefit ratio difficult for patients to access a radiology unit no answer total 882 ( 41.2% ) 595 ( 27.8% ) 148 ( 6.9% ) 33 ( 1.5% ) 485 ( 22.6% ) 2 , 143 ( 100% ) tabella 5 motivazioni della mancata richiesta di tc non necessaria ai fini estrazione 882 ( 41 , 2% ) non c rapporto dose / beneficio non c rapporto difficolt accesso servizio radiologia costo / beneficio non risponde totale 595 ( 27 , 8% ) 148 ( 6 , 9% ) 33 ( 1 , 5% ) 485 ( 22 , 6% ) 2143 ( 100% ) 55% would have prescribed a periapical x - ray ; the other 45% would not . 
tra i rispondenti favorevoli alla tc , il 37 , 6% avrebbe suggerito una radiografia periapicale , mentre il 62 , 4% non lavrebbe ritenuta utile . discussione discussion impacted lower - third - molar surgery can be associated with ian lesions [ 2528 ] and , according to libersa et al . 
the prevalence of ian lesions due to third - molar surgery is estimated in the la chirurgia dei terzi molari pu essere associata a lesioni del nai [ 2528 ] e secondo libersa et al . 
no correlation emerged between the appropriateness of dentists interpretations of the opts ( nearness to the gold standard ) and their years of professional activity , whereas there was a slight positive correlation between the appropriateness of their interpretations and the number of procedures completed per week . judging from the literature [ 68 , 10 ] , the signs visible on the opt are : overlap between the dental root and the mandibular canal , a diverted course of the mandibular canal , gaps in the mandibular canal margins , narrowing of the mandibular canal , narrowing of the root , a diverted root and loss of definition of contours of the canal and / or root . in our survey , radiographic signs most often identified were , in order of frequency : overlap between dental root and mandibular canal , loss of definition of contours of the canal and / or root and gaps in the mandibular canal margins . 
 [ 9 ] recorded no episodes of paraesthesia in cases lacking any sign of problems on the opt , but they found that none of the diagnostic signs ( when present ) had the specificity and sensitivity needed to predict the risk of ian exposure . 
 [ 30 ] stated that ct is warranted in the presence of roods criteria [ 31 ] and particularly the lack of cortical bone between the mandibular canal and the third molar . 
the sensitivity of opt in this setting has been estimated at around 4275% and its specificity at 6691% , which some authors consider inadequate in situations at risk [ 4 , 11 ]  . it is often claimed that opt is fundamental in assessing the anatomical relationship between the dental root and mandibular canal but that , because it is only two - dimensional , more complex cases ( in which one of roods criteria is visible ) warrant further investigation with ct , using various data acquisition and processing methods [ 7 , 8 , 1214 ]  . 
flygare and ohman [ 32 ] claimed that opt and endoral x - ray suffice in the majority of cases , providing there is no overlap between mandibular canal and dental root . 
 based on our survey , 54.96% of dentists who would [ 25 ] e la permanenza del disturbo varia tra lo 0 , 4% e il 23% dei casi [ 29 ]  . 
non emersa alcuna relazione tra la correttezza dellinterpretazione delle opt da parte del dentista ( vicinanza al gold standard ) e gli anni di attivit professionale , mentre c una leggera correlazione tra la correttezza dellinterpretazione e il numero di interventi a settimana . dalla letteratura [ 68 , 10 ] emerge che i segni visibili allopt sono : sovrapposizione della radice con il canale mandibolare , deviazione della direzione del canale mandibolare , interruzione del bordo del canale mandibolare , restringimento del canale mandibolare , restringimento della radice , deviazione della radice , perdita di definizione del contorno del canale e / o della radice . il nostro studio ha dimostrato che i segni radiografici maggiormente rilevati sono stati i seguenti , in ordine di frequenza : sovrapposizione della radice con il canale mandibolare , perdita del contorno del canale mandibolare e / o della radice ed interruzione del bordo del canale mandibolare . 
una ricerca affine alla nostra [ 11 ] ha stimato che pi frequentemente i professionisti rilevano : radiotrasparenza della radice , interruzione del canale mandibolare e deviazione del canale mandibolare . 
 [ 9 ] hanno potuto constatare che non c stato alcun caso di parestesia in assenza di segni predittivi allopt , ma che nessuno dei segni diagnostici ( quando presente ) aveva i caratteri di specificit e sensibilit per poter predire il pericolo di esposizione del nai . 
 [ 30 ] affermano che la presenza dei criteri di rood [ 31 ] , ed in particolare la mancanza di corticale tra il canale mandibolare ed il terzo molare , sia unindicazione a prescrivere la tc . 
 [ 11 ] hanno dimostrato che le lesioni postoperatorie si sono verificate in un numero di casi maggiore rispetto a quello prospettato dai segni predittivi visibili allopt ( nel 3 , 5% dei casi )  . 
 la sensibilit dellopt stata stimata attorno al 42%75% e la specificit al 66%91% , per alcuni non sufficienti nelle situazioni a rischio [ 4 , 11 ]  . comunemente affermata lassoluta necessit dellopt per la valutazione del rapporto tra radici e canale mandibolare ma , data lassenza di tridimensionalit , nei casi pi complessi ( in cui sia visibile uno dei criteri di rood ) consigliato lapprofondimento con tomografia computerizzata con varie modalit di acquisizione ed elaborazione [ 7 , 8 , 1214 ]  . 
flygare e ohman [ 32 ] sostengono che lopt e le radiografie endorali siano sufficienti per la maggior parte dei casi in cui non c sovrapposizione fra canale mandibolare e radici . 
 122 radiol med ( 2012 ) 117 : 112124 not prescribe a ct in a given situation would recommend a periapical x - ray , whereas 62.41% of those who would prescribe a ct did not consider periapical x - ray a useful adjunct to opt . 
 [ 6 ] found that 11% of dentists answering a questionnaire on how best to establish the anatomical relationship between the third - molar root and mandibular canal preferred to combine opt with periapical x - ray , 4% preferred ct and periapical x - ray and 53% considered it best to combine ct with opt . 
among the dentists in our survey who would not recommend ct , 41.2% justified their decision by saying it was unnecessary for the purposes of the extraction , and 27.8% felt that the dose / benefit ratio was unfavourable . 
the european unions council directive and the guidelines of the international scientific societies with regard to ionising radiation recommend adopting the principles of justification , appropriateness and optimisation in prescribing radiological examinations [ 1719 ]  . 
 a comparative analysis of the effective dose to head and neck tissues demonstrated that multislice ct ( msct ) with an optimised protocol delivered a higher effective dose ( 0.99 msv ) when compared with cbct dose ( 0.11 msv ) [ 37 ]  . 
the provisional guidelines published by the european atomic energy community ( euratom ) in 2009 ( sedentexct project ) state that cbct is justified where conventional radiographs suggest a close relationship between a mandibular third molar and the inferior dental canal and when a decision to perform surgical removal has been made [ 19 ]  . 
our survey seems to show that our sample of dentists tended to comply with the directives on ionising radiation , though we identified a slight propensity to prescribe ct more than necessary ( total propensity index 0.116 ) , probably for medicolegal reasons . 
some authors [ 14 ] state that ct can change the outcome of the third - molar extraction procedure , converting a situation at high surgical risk into a low likelihood of neurological damage . 
other studies [ 6 , 13 ] found no scientific evidence of lower morbidity rates among patients who had preoperative ct , concluding that it has only a minimal effect in improving the outcome of this type of surgery . 
older dentists may have been less inclined to use the web site : in italy , the use of the internet is still very limited ( 48.5% ) among people aged 3544 years , and among 60to 64 - year - olds , it drops secondo la nostra analisi il 54 , 96% di chi non prescrive la tc ritiene utile una radiografia periapicale , mentre il 62 , 41% di chi la prescrive non la ritiene utile oltre allopt . 
 [ 6 ] ha dimostrato che l11% dei rispondenti ad un questionario circa i metodi pi idonei per definire il rapporto radice dellottavo / canale mandibolare , giudica utile la combinazione opt e radiografia periapicale , il 4% la combinazione tc e radiografia periapicale , mentre il 53% ritiene utile la combinazione tc e opt . 
i dentisti intervistati , che non hanno indicato la necessit di prescrivere la tc , hanno giustificato la scelta per il 41 , 2% perch non necessaria ai fini dellestrazione e nel 27 , 8% dei casi per la mancanza di un rapporto dose / beneficio favorevole . 
le direttive del consiglio dellunione europea e le linee guida delle societ scientifiche internazionali in materia di radiazioni ionizzanti invitano ai principi di giustificazione , appropriatezza e ottimizzazione nella prescrizione di esami radiologici [ 1719 ]  . 
 unanalisi comparativa della dose effettiva ai tessuti di testa e collo dimostra che la multislice computed tomography ( msct ) , utilizzata con un protocollo ottimizzato , comporta una dose effettiva pi alta ( 0 , 99 msv ) rispetto alla dose della cbct ( 0 , 11 msv ) [ 37 ]  . 
le linee guida pubblicate dall european atomic energy community ( euratom ) nel 2009 ( sedentexct project ) sostengono che la cbct giustificata quando la radiologia convenzionale dimostra una stretta relazione tra terzo molare mandibolare e il canale mandibolare e quando deve essere presa una decisione riguardo lestrazione chirurgica [ 19 ]  . 
da questa indagine sembra emergere che il campione esaminato tenda a rispettare le direttive in materia di radiazioni ionizzanti , sebbene si sia rilevata una lieve propensione a prescrivere la tc pi del necessario ( ipt = 0 , 116 )  . 
 stato riportato [ 1 ] che il 20% dei pazienti che ha subito una lesione iatrogena del nai dopo lestrazione del terzo molare inizia unazione legale contro il proprio dentista . alcuni autori [ 14 ] sostengono che la tc possa cambiare le sorti dellintervento , portando da una condizione di rischio operatorio alto ad una bassa probabilit di lesione neurologica . 
altri studi [ 6 , 13 ] affermano non esserci evidenza scientifica riguardo una diminuzione del grado di morbilit del paziente utilizzando una tc preoperatoria , ma che questa abbia solo un minimo effetto nel miglioramento dellintervento . 
 in questa indagine si rilevato che una percentuale consistente dei rispondenti ( 31 , 5% ) , presumibilmente superiore rispetto alla popolazione dei dentisti , aveva unet fino a 35 anni . 
i dentisti pi anziani potrebbero essere meno inclini allaccesso al web : in italia luso di internet ancora radiol med ( 2012 ) 117 : 112124 to 14.9% , whereas among people > 65 , these technologies are still only marginally used [ 40 ]  . 
we must therefore assume that older , more experienced , professionals were not adequately represented in our sample , even though our study found that the appropriateness of dentists assessments of opts did not depend on their years of professional experience . 
we nonetheless believe that we avoided the potential risk of a sample bias by ascertaining that our sample was not biased in terms of age ( in fact , different ages correlated not only with a different propensity to use the web to communicate but also with different levels of professional experience )  . 
 our findings indicate a slight tendency to prescribe ct even when it is unnecessary , although the criteria relating to the appropriateness of ct for lower - third - molar extractions were generally met . molto limitato ( 48 , 5% ) tra le persone di et compresa tra i 35 e i 44 anni , tra le persone di et 6064 anni scende al 14 , 9% , mentre per gli over - 65 lutilizzo di nuove tecnologie marginale [ 40 ]  . 
possiamo dunque dire che forse i professionisti pi anziani e con maggior esperienza non siano stati rappresentati nel campione esaminato , anche se comunque lo studio ha dimostrato che la correttezza del dentista nella valutazione dellopt non dipende dagli anni di esperienza professionale . 
ci induce a pensare che siano state presentate troppe opt e che ci abbia incrementato il rischio di perdere informazioni . il nostro sondaggio caratterizzato da un basso tasso di risposta . 
ci nonostante riteniamo di aver scongiurato il potenziale pericolo di bias , verificando che il campione non distorto per et ( let infatti correlata a differenze nella propensione a rispondere via web , ma anche a livelli differenti di esperienza )  . 
angelelli1 1section of radiology , di.m.i.m.p. , hht interdepartmental centre , university hospital , policlinico of bari , piazza giulio cesare 11 , 70124 bari , italy 2 section of internal medicine , di.m.i.m.p. 
hereditary haemorrhagic telangiectasia ( hht ) , or renduoslerweber disease , is a rare autosomal dominant disorder characterised by mucocutaneous or visceral vascular abnormalities that may be widely distributed throughout the cardiovascular systethe purpose of this study was to compare multislice computed tomography angiography ( mscta ) and 4d dynamic contrast - enhanced magnetic resonance angiography ( d - mra ) for evaluating vascular hepatic involvement in patients with hht . 
 the images from the two techniques were reviewed independently by two expert radiologists to identify the following vascular abnormalities : telangiectases or large vascular masses ; perfusion disorders [ transient hepatic attenuation differences ( thads ) ] ; hepatic arteriovenous malformations ( havms )  . 
data , as well as diameters of the common hepatic artery and portal vein , were compared with cohens kappa statistic , students t test and receiver operating characteristic ( roc ) curve analysis , as appropriate . 
la teleangiectasia emorragica ereditaria ( hht ) o malattia di rendu - osler - weber una patologia rara a trasmissione autosomica dominante caratterizzata da alterazioni vascolari mocoso - cutanee o viscerali che possono coinvolgere diversi organi e apparati . 
le immagini di entrambi gli esami sono state valutate indipendentemente da due radiologi esperti al fine di ricercare le seguenti alterazioni vascolari epatiche : teleangiectasie , disordini di perfusione ( thads ) , malformazioni artero - venose ( havms )  . 
in 36 / 52 pazienti le due metodiche hanno riscontrato la presenza di una o pi delle seguenti alterazioni vascolari epatiche ( 29 / 52 teleangiectasie , 23 / 52 thads e 25 / 52 havms )  . 
le due tecniche hanno dimostrato una buona concordanza nel determinare il tipo 30 radiol med ( 2012 ) 117 : 2945 36 / 52 cases ( telangiectases in 29 / 52 , thads in 23 / 52 and havms in 25 / 52 [ ce1 ] )  . 
d - mra has the same diagnostic accuracy as mscta and has the advantage of being less invasive due to the absence of ionising radiation . keywords mr angiography ct angiography hereditary hemorrhagic telangiectasia , hht liver shunt epatico ( = 0 , 9 )  . 
la d - mra presenta il vantaggio di una minore invasivit legata allassenza di radiazioni ionizzanti . parole chiave angio - rm angio - tc teleangiectasia emorragica ereditaria ( hht ) fegato introduction introduzione hereditary haemorrhagic telangiectasia ( hht ) , or rendu oslerweber disease , is a rare autosomal dominant disorder with an estimated incidence of 1 : 6 , 000 persons [ 13 ] and is characterised by mucocutaneous or visceral vascular abnormalities that may be widely distributed throughout the cardiovascular system [ 1 ]  . 
at present , diagnosis of this disease is based on the curaao clinical criteria [ 4 ] ( table 1 ) , even though genetic testing to identify the most frequent mutations in the gene encoding for endoglin ( eng ) [ 5 ] and activin receptor type ii - like kinase i ( alk - 1 ) [ 6 ] is available in many countries [ 7 ]  . a wide spectrum of clinical manifestations may involve the nose , skin , brain , lung , liver and gastrointestinal tract . 
 liver involvement in hht is characterised by different types of hepatic arteriovenous malformations ( havms ) , principally consisting of vascular lesions , such as telangiectases or large confluent vascular masses , and shunts between the major vessels of the liver and classified as arteriosystemic or arteriovenous ( avs ) , arterioportal ( aps ) and portosystemic ( pss ) [ 810 ]  . recent reports have demonstrated that up to 75% of hht patients have hepatic vascular or biliary abnormalities , although symptoms due to liver involvement are uncommon [ 1012 ]  . 
screening for hepatic involvement in asymptomatic patients is not mandatory [ 13 ] , but as symptoms may depend on specific vascular lesions , knowledge of imaging aspects of the liver in symptomatic patients is fundamental [ 12 , 14 , 15 ]  . 
moreover , extensive hepatic screening as part of a research protocol may well offer insights into the pathogenesis and course of the disease in patients with liver involvement [ 16 ]  . colour doppler ultrasound ( cdus ) and multislice computed tomography ( msct ) are the imaging modalities of choice to rule out hepatic vascular abnormalities . 
cdus was the first technique used to study hepatic vascular la teleangiectasia ereditaria emorragica ( hht ) o malattia di rendu - osler - weber una patologia genetica rara con trasmissione autosomica dominante , prevalenza stimata di 1 / 6000 soggetti [ 13 ] , caratterizzata da malformazioni vascolari mucoso - cutanee o viscerali che possono distribuirsi in tutto lapparato cardio - vascolare [ 1 ]  . 
attualmente la diagnosi si basa sui criteri clinici di curaao ( tabella 1 ) [ 4 ] anche se in molte nazioni sono disponibili test genetici per identificare le mutazioni pi frequenti dei geni che codificano per lendoglina ( eng ) [ 5 ] e per il recettore dellattivina tipo ii ( alk1 ) [ 6 , 7 ]  . le manifestazioni cliniche sono molto varie e possono interessare la mucosa nasale , la cute , lencefalo , il polmone , il fegato e il tratto gastroenterico . 
il coinvolgimento epatico dellhht caratterizzato da diversi tipi di malformazioni artero - venose ( havms ) , che consistono principalmente nelle teleangiectasie , nelle grandi masse vascolari confluenti e negli shunt tra le diverse strutture vascolari epatiche classificati in shunt artero - sistemici o arterovenosi ( avs ) , shunt artero - portali ( aps ) e shunt porto - sistemici ( pss ) [ 810 ]  . lavori recenti hanno dimostrato che il 75% circa dei pazienti con hht hanno anomalie epatiche o biliari anche se i pazienti sintomatici sono piuttosto rari [ 1012 ] ; pertanto la ricerca delle anomalie epatiche nei pazienti non indispensabile [ 13 ] , ma poich i sintomi possono dipendere da specifiche anomalie vascolari , la conoscenza dellimaging associato al coinvolgimento epatico indispensabile per il corretto inquadramento dei pazienti [ 12 , 14 , 15 ]  . 
lo screening epatico , inoltre , uno strumento di ricerca prezioso per la comprensione della reale prevalenza e della storia naturale di tali lesioni in corso di hht [ 16 ]  . 
due to the diffusion of the multislice imaging , which allows scanning both the thorax and the upper abdomen in a few seconds , the popularity of msct as a one - step imaging modality for screening patients for vascular visceral lesions has increased considerably [ 10 , 13 , 17 ]  . the role of magnetic resonance imaging ( mri ) in this clinical setting has been described since the late 1980s [ 8 , 17 ] ; however , extensive use of this technique has been discouraged because of the duration of the exam , the low spatial resolution and high costs . 
developments in mri technology , such as high magnetic fields , phased - array coils and high - performing gradients , have improved mri capabilities , and recently some authors have described mri and mr angiography ( mra ) as valid examinations to provide complete parenchymal , biliary and vascular screening for the liver in hht and to assess the outcome of an interven ( msct )  . 
la cdus stata la prima metodica utilizzata per la possibilit di valutare la direzione , la velocit e la pulsatilit del flusso sanguigno dellarteria epatica , della vena porta e delle vene sovra - epatiche [ 8 , 9 ]  . 
negli ultimi anni , invece , la popolarit della msct come esame di scelta nello screening del paziente con hht , cresciuta in modo considerevole per la possibilit di ottenere in pochi secondi scansioni con elevata risoluzione spaziale sia del torace , sia degli organi addominali [ 10 , 13 , 17 ]  . il ruolo della risonanza magnetica nucleare ( mri ) stato descritto sin dagli anni ottanta [ 8 , 17 ] , ma luso di routine di questa metodica stato scoraggiato in passato dalla lunga durata dellesame , dalla bassa risoluzione spaziale e dai costi elevati . 
il progresso tecnologico rappresentato dalluso di alti campi magnetici , dalle bobine di superficie e da gradienti performanti , ha notevolmente incrementato le possibilit della mri e recentemente alcuni autori hanno descritto la mri e langio - risonanza magnetica ( mra ) come un valido esame per lo studio del fegato nei pazienti con hht in grado di fornire informazioni complete a livello vascolare , parenchimale e biliare e di valutare il successo di procedure interventistiche in pazienti sintomatici [ 12 , 18 , 19 ]  . 
 per quanto di nostra conoscenza , in letteratura non esistono studi che confrontino le capacit diagnostiche dellangio - msct ( mscta ) che considerata il goldstandard non invasivo , e della mra nella valutazione del coinvolgimento vascolare epatico dei pazienti con hht . 
 scopo di questo lavoro confrontare laccuratezza diagnostica delle mscta a 16 strati e della mra dinamica - 4d ( d - mra ) in 52 pazienti consecutivi affetti da hht . materiali e metodi pazienti nel periodo compreso tra giugno 2006 e giugno 2009 sono stati arruolati , presso il centro interdipartimentale per lo studio dellhht della nostra universit , 52 pazienti consecutivi ( 27 maschi e 25 femmine ; et media 48 , 8 anni , range 1679 )  . 
la maggior parte dei pazienti lamentava epistassi ( 31 / 52 ; 60% ) , 5 / 52 ( 10% ) riferivano un precedente ascesso cerebrale secondario a voluminose fistole artero - venose polmonari ( pavms ) , un paziente lamentava 32 radiol med ( 2012 ) 117 : 2945 tional procedure in symptomatic patients [ 12 , 18 , 19 ]  . to our knowledge , no study is available comparing the capabilities of msct angiography ( mscta ) , which is considered the noninvasive diagnostic gold standard , and mra for evaluating vascular hepatic involvement in hht . 
 hence , in this study , 16 - slice mscta and dynamic 4d contrast - enhanced mra ( d - mra ) were evaluated in a cohort of 52 consecutive hht patients referring to a single institution . episodi ricorrenti di sanguinamento gastroenterico , 5 / 52 ( 10% ) pazienti erano affetti da cardiopatia congestizia , un paziente riferiva un episodio di sanguinamento da varici esofagee , mentre 11 / 52 ( 21% ) pazienti erano asintomatici . 
 lo studio stato approvato dal comitato etico locale e gli esami mscta e d - mra sono stati eseguiti entro una settimana luno dallaltro dopo aver ottenuto consenso informato scritto da tutti i pazienti in accordo con la dichiarazione di helsinki del 1990 . materials and methods patients from june 2006 to june 2009 , 52 new consecutive patients ( 27 men , 25 women ; mean age 48.8 years ; range 1679 ) were enrolled at the interdepartmental centre for the study of hht of our university hospital . 
at the time of inclusion , three curaao diagnostic criteria were already present in 31 / 52 cases , whereas only two criteria were found in 21 / 52 patients . 
most patients ( 31 / 52 ; 60% ) complained of nosebleeds , 5 / 52 ( 10% ) had a history of brain abscess due to large pulmonary arteriovenous malformations ( pavms ) , one had recurrent gastrointestinal bleeding ( 2% ) , 5 / 52 ( 10% ) had congestive heart failure , one ( 2% ) reported a history of bleeding oesophageal varices and 11 / 52 ( 21% ) were asymptomatic . 
the study was approved by the local ethics committee , and mscta and d - mra procedures were performed within 1 week of each other after obtaining written informed consent from all patients , in agreement with the 1990 declaration of helsinki . ct imaging a systematic screen for vascular visceral involvement was performed with msct using a 16 - slice scanner ( tsx - 101aaquilion , toshiba medical system , tochigi , japan ) with the following parameters : slice thickness 1 mm ; reconstruction interval 0.8 mm ; tube rotation time 0.5 s ; 120 kv and 240 mas . 
the scan delay for the early arterial phase was assessed automatically with the bolusprotocollo tc gli esami msct sono stati eseguiti per lo screening del coinvolgimento epatico con apparecchiatura a 16 detettori ( tsx - 101a - aquilion , toshiba medical system , tochigi , giappone ) usando il seguente protocollo : thickness 1 mm , intervallo di ricostruzione 0 , 8 mm , tempo di rotazione del tubo 0 , 5 secondi , 120 kv e 240 mas . 
 stato seguito un protocollo trifasico ( fase arteriosa precoce , fase arteriosa tardiva e fase venosa ) dopo iniezione di 1 , 5 ml / kg di mezzo di contrasto non ionico ( ultravist 370 , schering , berlino , germania ) attraverso un ago 16 g in una vena cubitale con lausilio di iniettore automatico alla velocit di 4 ml / s seguito da un bolo di 30 ml di soluzione fisiologica alla stessa velocit . 
lo scan delay per la fase arteriosa precoce stato stabilito automaticamente con tecnica di bolus tracking posizionando una regione di interesse ( roi ) nellaorta addominale allemergenza del tripode celiaco con un valore soglia di 150 hu . 
la scansione in fase arteriosa tardiva stata acquisita con un inter - scan delay di 10 secondi , mentre per la fase venosa stato utilizzato un inter - scan delay di 40 secondi estendendo lacquisizione al torace . 
tutte le immagini sono state inviate ad una workstation dedicata ( vitrea 4.1 , vital images , minneapolis , minnesota , us ) per ottenere ricostruzioni multiplanar rendering ( mpr ) e proiezione di massima intensit ( mip )  . protocollo mri la mri stata eseguita con magnete da 1 , 5 t ( philips achieva v1.54 ) con una bobina di superficie a 4 canali ( sense body ) posizionata sulladdome superiore . 
the late arterial phase was acquired with a interscan delay of 10 s from the previous acquisition , whereas the venous phase utilised an interscan delay of 40 s , including the thoracic scan . 
all images were transferred to a workstation ( vitrea 4.1 , vital images , minneapolis , mi , us ) to obtain multiplanar reformation ( mpr ) and maximum intensity projection ( mip ) images . mr imaging mri was performed using a 1.5 - t magnet ( philips achieva v1.54 ) with a sense body coil positioned on the upper abdomen . 
the following standard unenhanced liver imaging protocol was used in all cases : axial t1 - weighted sequence ( thickness 78 mm , time of echo [ te ] 4.6 in phase , time to repeat [ tr ] shortest , matrix 256 [ reconstruction matrix 512 ] , field of view [ fov ] 350380 , breath - hold ) , axial single - shot fast spin - echo ( ss - fse ) , t2 ss and ssfse , t2 spectral selection attenuated inversion recovery ( spair ) ( thickness 78 mm , te 100 , tr shortest , flip angle [ fa ] 90 , matrix 320 , fov 350380 , with respiratory triggering ) , coronal balanced turbo field echo ( b - tfe ) ( thickness 8 mm with 4 mm overlapping , te / tr shortest , fa 90 , fov 350400 , breath - hold )  . subsequently , eight consecutive dynamic mras were obtained in a single breath - hold after i.v. 
le immagini dinamiche 3d sono state trasferite ad una worstation per ottenere immagini mip , mpr e sequenze mip - cine . lacquisizione d - mra stata seguita da una sequenza assiale t1w volumetrica ad alta risoluzione isotropica ( thrive ) in fase venosa per una completa valutazione postcontrastografica del parenchima ( 100 slice con spessore 2 mm , fattore sense 4 , fov 350380 , rfov : 65%70% , tempo di acquisizione in apnea : 1921secondi )  . 
se necessario stata acquisita unulteriore sequenza thrive a circa 1 ora dalliniezione del mezzo di contrasto ( mdc ) , in fase epato - specifica . analisi delle immagini la mscta e la d - mra sono state interpretate indipendentemente da due radiologi con il medesimo grado di esperienza nellimaging epatico con tc ( aasi , 15 anni ) e mri ( as , 12 anni )  . 
con entrambe le tecniche sono stati considerati i seguenti parametri : la presenza di telangiectasie ( lesioni ipervascolarizzate di diametro < 10 mm ) , grandi masse vascolari confluenti ( lesioni simili alle precedenti di diametro > 10 mm ) , disordini di perfusione ( aree a disposizione periferica e morfologia cuneiforme con ipervascolarizzazione transitoria , thads ) , e malformazioni artero - venose epatiche ( havms ) classificate come shunt artero - venosi ( avs ) , artero - portali ( aps ) e porto sistemici ( pss )  . in generale i criteri diagnostici utilizzati per la mscta e la d - mra per la definizione delle diverse havms sono stati i medesimi . 
gli avs sono stati diagnosticati quando esisteva una opacizzazione delle vene sovraepatiche in fase arteriosa precoce , mentre la diagnosi di aps stata posta se esisteva opacizzazione dei rami portali intraparenchimali o della vena porta in fase arteriosa precoce e se 34 radiol med ( 2012 ) 117 : 2945 staff radiologists with the same level of experience in liver imaging with ct ( asi , 15 years ) and mri ( as , 12 years ) who were blind to each others diagnosis . 
the following parameters were considered for both techniques : presence of telangiectases ( round hyperenhancing lesions < 10 mm ) , large vascular lesions ( similar lesions > 10 mm ) , perfusion disorders [ consisting of peripheral wedge - shaped transient hepatic attenuation differences ( thads ) ] and havms classified as avs , aps and pss . 
avs were diagnosed when hepatic veins were opacified in the early arterial phase , whereas aps was diagnosed if the intrahepatic portal branches or the portal veins were clearly visible before the splenic vein in the early arterial phase . 
sono state anche segnalate la presenza di qualsiasi altra anomalia vascolare o parenchimale , come aneurismi delle arterie splancniche o varianti anatomiche vascolari cos come sono stati calcolati i diametri dellarteria epatica comune e della vena porta . 
sono stati infine registrati la durata degli esami mscta ed d - mra ed il tempo complessivo del post - processing , mentre non stato considerato il tempo di preparazione del paziente . analisi statistica il confronto dei diversi parametri presi in considerazione fig . 
the presence of any other parenchymal or vascular abnormality , such as splanchnic aneurysms or variations of vascular anatomy , was also reported , in addition to the diameters of the common hepatic artery and portal vemscta and d - mara examination time as well as overall postprocessing time was recorded ; time for patient preparation was not considered . statistical analysis comparison of the various parameters between cta and mra was performed using the paired - sample t test , the independent - sample t test and the 2 test , as appropriate , with p < 0.05 being interpreted as statistically significant . 
statistical analyses were performed using prism for windows , version 5 ( graphpad software , san diego , ca , usa ) and medcalc for windows version 9 ( medcalc software , mariakerke , belgium )  . results mscta and mri findings for hht patients are summarised in table 2 . 
in 11 / 52 cases ( 21% ) , telangiectases were the sole hepatic malformation , whereas in 18 / 52 patients ( 35% ) , they were associated with other vascular abnormalities . 
in the remaining two patients , mscta could not establish the type of shunt , as neither the portal vein nor hepatic veins were visible in the con le due metodiche stato eseguito con test t di student per dati appaiati , test t di student per dati indipendenti e test 2 a seconda delle necessit considerando come statisticamente significativo un valore di p0 , 05 . 
tale valutazione statistica stata effettuata usando i software prism versione 5 per windows ( graphpad software , san diego , california , usa ) e medcalc versione 9 per windows ( medcalc software , mariakerke , belgio )  . 
in 15 / 52 ( 29% ) pazienti , la presenza di anomalie epatiche ha rappresentato il terzo criterio diagnostico di curaao ed ha permesso di formulare con certezza la diagnosi di hht . 
in 11 / 52 casi ( 21% ) le teleangiectasie rappresentavano lunica lesione presente , mentre in 18 / 52 pazienti ( 35% ) erano associate ad altre anomalie vascolari . 
la mscta e la d - mra hanno dimostrato thads in 23 / 52 pazienti ( 44% ) sempre in associazione ad altre anomalie vascolari epatiche . la presenza di havms stata evidenziata complessivamente in 25 / 52 casi ( 48% ) con entrambe le metodiche . 
nei restanti due pazienti la mscta non ha consentito di stabilire con certezza il tipo di shunt poich nella fase arteriosa precoce non esisteva opacizzazione venosa pur in presenza di dilatazione dellarteria epatica e di diffuse teleangietasie . 
si associa la presenza di aneurismi dellarteria splenica ( freccia ) e delle arterie gastriche brevi ( punta di freccia )  . radiol med ( 2012 ) 117 : 2945 fig . 
e limmagine rm assiale ssh - t2 non mostra alcuna alterazione , f - h le ricostruzioni mip di tre acquisizioni d - mra consecutive mostrano la stessa lesione individuata con la mscta ( punta di freccia )  . 
in 3 / 52 ( 6% ) pazienti ( due con fistole miste , uno senza alcuna havms ) stato osservato radiol med ( 2012 ) 117 : 2945 fig . 
b fase arteriosa tardiva e c fase venosa : le vene sovra epatiche ( frecce spesse ) , la vena porta ( freccia sottile ) e la vena splenica sono opacizzate . 
dilatazione dellarteria epatica ( punta di freccia ) con precoce e contemporanea opacizzazione delle vene sovraepatiche ( frecce spesse ) e della vena porta ( freccia sottile ) seguita dal riempimento della vena splenica . 
sulla base della d - mra stata posta diagnosi di shunt misto . the origin of the right hepatic artery from the superior mesenteric artery in six cases and the origin of the common hepatic artery from the superior mesenteric artery in one patient . 
in 1 / 52 ( 2% ) pazienti stata identificata una lesione ipervascolarizzata interpretata come iperplasia nodulare rigenerativa benigna per laspetto isodenso nella fase tardiva in msct e per luptake di gadobenato di meglumine in fase 40 radiol med ( 2012 ) 117 : 2945 fig . 
d - f mip reformations of three consecutive d - mra : multiple telangiectases ( arrowheads ) with early opacification of the intrahepatic portal branches ( thick arrows in d )  . 
mean examination times were about 5 min for mscta and 18 min for d - mra , with a postprocessing time of 10 min for both modalities . discussione minuti per la d - mra , con un post - processing di 10 minuti per entrambi gli esami . discussion liver involvement in hht is one of the most frequent manifestations of this disease , and its actual prevalence has finally been revealed due to improvements in diagnostic techniques , such as cdus and msct , which have evidenced specific vascular alterations in about 70% of patients , alterations that are , however , often asymptomatic . 
these patients can be divided into three clinical patterns related to high - output cardiac failure involving the presence of arteriovenous shunts : portal hypertension due to arterioportal shunts , ischaemic biliary disease related to portal - venous shunts [ 13 ] or , according to recent studies , large avms shunting blood from the peribiliary plexus [ 20 ]  . 
firstly , in the absence of genetic testing or in the case of an inconclusive test , the presence of hepatic abnormalities is one of the fundamental curaao diagnostic criteria and , in our series , these malformations represented the third criterion for a definite diagnosis of hht in 15 / 52 ( 29% ) patients . 
secondly , it is well known that the prevalence of havms in hht tends to increase with age ; in fact , the majority of symptomatic patients with liver involvement has a median age of 62 years [ 13 , 21 ]  . 
therefore , the possibility of an early diagnosis of liver involvement by means of accurate imaging techniques would permit an attentive selection of patients for a specific instrumental and clinical follow - up . 
lastly , knowledge of these abnormalities is important because many patients are subjected to imaging for other reasons , and abnormal liver findings may be the first indication of hht involvement . 
physicians unfamiliar with abnormal liver findings in asymptomatic patients might decide to perform a more invasive workup , including liver biopsy or endoscopic retrograde cholangiopancreatography , which could lead to complications [ 22 ]  . based on these considerations , even if mscta is considered the gold standard , evaluation of the hepatic parenchyma with less - invasive imaging methods but endowed with the same diagnostic accuracy is essential . 
theoretically , cdus would be the ideal technique due to the lack of any biological risk , but it is less sensitive than ct or mri for detecting small lesions . 
recently , a new sonographic sign has been described , that of colour spots and subcaplinteressamento epatico nellhht una delle manifestazioni pi frequenti della malattia e la sua reale prevalenza ormai conosciuta grazie al miglioramento di tecniche dimaging come il cdus e la msct che hanno consentito il riconoscimento di specifiche alterazioni vascolari in circa il 70% dei pazienti , che sono spesso asintomatici . 
infatti secondo diverse casistiche pubblicate solo il 2%10% dei soggetti mostrano una sintomatologia [ 7 , 10 , 13 ] che pu essere divisa in tre quadri clinici in relazione ad una insufficienza cardiaca ad alto flusso nei casi con importanti avs , ad una ipertensione portale nelle forme caratterizzate principalmente da aps ed ad una patologia biliare su base ischemica associata alla presenza di pvs [ 13 ] o come recentemente segnalato a grandi avms con conseguente ipoperfusione del plesso peribiliare [ 20 ]  . 
in primo luogo , in assenza di test genetico o con test inconclusivo , levidenza di lesioni epatiche costituisce uno dei criteri clinici di curaao per formulare una diagnosi di certezza e , nella nostra casistica in 15 / 52 ( 29% ) casi la diagnosi finale stata possibile proprio grazie al riconoscimento di havin secondo luogo noto come le lesioni epatiche dellhht tendano a peggiorare nel tempo e che let mediana dei pazienti sintomatici di 62 anni [ 13 , 21 ] , pertanto la possibilit di diagnosticare precocemente il coinvolgimento epatico , potrebbe consentire di selezionare i soggetti da sottoporre a follow - up pi stretto . 
infine la corretta interpretazione di queste lesioni , in esami diagnostici eseguiti per altri motivi , fondamentale per evitare che in centri con poca familiarit con lhht , si possa decidere di sottoporre i pazienti ad indagini diagnostiche invasive come biopsia epatica o lercp che potrebbero comportare severe complicanze [ 22 ]  . 
 in base a tali considerazioni , anche se la mscta rappresenta la metodica dimaging pi accurata , essenziale la ricerca di altre indagini con la stessa accuratezza diagnostica , ma con minore invasivit biologica . 
in teoria , lecotomografia con cdus sarebbe la tecnica ideale per lassenza di qualsiasi rischio biologico , ma rispetto a mscta e ad mra meno sensibile specie nel riconoscimento di piccole lesioni . 
recentemente stato descritto un nuovo segno noto come segno del color spots e dellipervascolarizzazione sub - capsulare che sembra migliorare significativamente laccuratezza del cdus e la corrispondenza con la mscta [ 14 ]  . 
tuttavia opinione comune che la valutazione ecografica dei pazienti con hht richieda radiol med ( 2012 ) 117 : 2945 sular hypervascularization , which seems to greatly increase the diagnostic accuracy of cdus and the corresponding msct [ 14 ]  . 
however , it is common opinion that a us evaluation of hht patients requires an extensively experienced operator , and the most credible results can be obtained exclusively in patients with severe liver involvement or in centres of excellence for the study of this disease [ 23 ]  . 
 in our experience , d - mra demonstrated exactly the same diagnostic accuracy as msct for detecting all vascular lesions that might characterise hepatic involvement in hht patients : that is , d - mra was as accurate as mscta for depicting hepatic vascular involvement , thus confirming the high prevalence of hepatic vascular abnormalities reported in the recent literature [ 10 , 12 ] and the low number ( 6 / 52 ; 11% ) of symptomatic patients ( three with high - output heart failure and one with portal hypertension )  . when evaluating havms , mscta and d - mra demonstrated the presence of these alterations in the same 36 / 52 patients ; morphological characteristics of hepatic artery and portal vein were similar with both techniques , and the distribution of avs , aps and mixed shunts did not show any significant differences compared with previous reports [ 10 ]  . as for diagnosis of havm types , the two procedures provided a different diagnosis in only two cases . 
it is likely that in these two patients , d - mra , owing to dynamic vascular acquisitions and a higher temporal resolution , achieved a more precise shunt classification . 
however , the lack of confirmation by dsa of these shunts , which is the main limitation of our study , makes this a speculative assertion , but invasive exploration of the liver vasculature is unadvisable in hht for diagnostic purposes alone [ 13 , 24 ] and has been discouraged by recent guidelines for diagnosing and treating hht [ 25 ]  . 
another advantage of using d - mra is that it requires a smaller amount of gadolinium - based contrast medium compared with the iodinated contrast medium of ct , with a lower risk of cardiac overload in patients with high - output cardiac failure . 
moreover , despite the greater amount of time required for the examination , d - mra permits a drastic reduction in biological invasiveness compared with mscta due to the absence of radiation ; furthermore , its high interobserver agreement [ 12 ] ensures an accurate diagnosis independent of operator experience , thereby reducing the number of repeated examinations that would increase global screening costs . 
 it is obvious that better diagnostic results might be obtained with the use of more modern msct scanners ( with more than 64 detectors ) , which are able to scan the upper abdomen in less than 2 s . 
 operatori molto esperti e che i migliori risultati si possano ottenere esclusivamente nei centri di riferimento per lo studio della malattia [ 23 ]  . nella nostra esperienza , la d - mra ha dimostrato la stessa accuratezza diagnostica rispetto alla msct per la visualizzazione delle lesioni vascolari epatiche caratteristiche dellhht , confermando lelevata frequenza di tali lesioni descritta dalla recente letteratura [ 10 , 12 ] e anche la bassa prevalenza ( 6 / 52 ; 11% ) di soggetti sintomatici ( 5 con cardiopatia congestizia , 1 con ipertensione portale )  . nella valutazione delle havms i due esami hanno dimostrato la presenza di alterazioni vascolari negli stessi 36 / 52 pazienti ; analogamente non sono state dimostrate differenze significative rispetto a precedenti casistiche per quanto riguarda le caratteristiche morfologiche dellarteria epatica , della vena porta e nella distribuzione dei diversi tipi di shunt [ 10 ]  . nella definizione del tipo di shunt la diagnosi delle due metodiche stata discordante solo in due casi . 
in questi due pazienti , la diagnosi formulata con d - mra probabilmente la pi precisa in relazione alla maggiore risoluzione temporale ed alla disponibilit di un maggior numero di acquisizioni dinamiche ; tuttavia in assenza di una conferma angiografica , che rappresenta il limite pi importante del nostro studio , tale affermazione appare speculativa , anche se lesplorazione della vascolarizzazione epatica con tecniche invasive per fini diagnostici [ 13 , 24 ] ormai scoraggiata dalle recenti linee guida [ 25 ]  . 
un ulteriore vantaggio della d - mra legato alla necessit di una minore quantit di mdc a base di gadolinio rispetto al mdc iodato della tc , con un rischio minore di sovraccarico cardiaco nei pazienti con scompenso ad alto flusso . 
 secondo la nostra esperienza , il protocollo di screening dei pazienti con hht , potrebbe essere modificato al fine di evitare lutilizzo di mdc iodato e poich , nonostante il tempo desame significativamente maggiore , la d - mra consente una drastica riduzione dellinvasivit biologica rispetto alla mscta per lassenza di radiazioni ionizzanti ; inoltre lelevato accordo tra osservatori dimostrato in letteratura [ 12 ] assicura una diagnosi accurata indipendentemente dallesperienza del radiologo con minore necessit di esami ripetuti responsabili di un incremento dei costi globali dello screening . , tuttavia , facilmente prevedibile che le possibilit diagnostiche della mscta possano in breve tempo migliorare ulteriormente grazie al diffondersi delle apparecchiature con pi di 64 detettori capaci di scansioni delladdome completo in meno di 2 secondi . 
secondo la nostra opinione , nonostante lelevata accuratezza possibile , tali indagini dovrebbero essere evitate nei pazienti hht per lelevata dose di radiazioni . nel nostro studio gli shunts porto - venosi non sono mai stati evidenziati con nessuna delle due metodiche . 
the difficulty of their identification with current imaging technologies is well known due to their insufficient spatial and temporal resolution and the fact that they are microscopic in the majority of cases [ 26 ]  . 
however , it can be hypothesised that these shunts may cause metabolic changes , which might be detected by laboratory tests , such as breath tests [ 27 ]  . in conclusion , our experience demonstrates that d - mra provides the same diagnostic results as mscta and can be considered as a safe and highly accurate imaging technique to rule out hepatic involvement in hht patients . colt nella loro identificazione ben conosciuta ed dovuta ad una insufficiente risoluzione spaziale e temporale delle tecniche di imaging e dal fatto che tali shunts sono spesso microscopici [ 26 ]  . 
belyaev springer heidelberg dordrecht london new york , 2010 isbn : 978 - 3 - 642 - 12386 - 3 e - isbn : 978 - 3 - 642 - 12387 - 0 published online : 10 july 2011 springer - verlag 2011 in this 239 page , 15 chapter book the authors present their experience regarding the thyroid ultrasound ( us ) doma this is by no means an easy or elementary medical field ; rather an important and clinically relevant field . 
 thyroid gland normal presentation , variants , difficult representation , typical and rare diseases are presented in their various manifestations as well as they can be diagnosed and possibly treated by us . 
all various us modalities are described , with stress on their different options , ensuing possible results and difficulties in handling procedures . us diagnosis of thyroid disease is followed by the description of minimally invasive us - guided procedures : fine - needle biopsy , simple percutaneous ethanol or glucocorticoid injection or more sophisticated procedures , such as percutaneous laser or radiofrequency ablation . 
very useful examples of us reports are to be found at the end of each type of disease or procedure . the book is enriched by a very impressive number of us images : unfortunately most of the time , you will find neither appropriate captions , nor arrows etc . 
the authors have the unpleasant habit of often citing in the text lay - out names and year date of publication of authors who are not , unfortunately , to be found in the references at the end of the book . this book could be appreciated by all those who have experience with thyroid diseases and us ; however those in questo volume , di 239 pagine divise in 15 capitoli , gli autori presentano la loro esperienza nel campo dellecografia della tiroide : argomento medico , quello della tiroide , affatto facile n elementare , al contrario molto importante e dal significato clinico notevole . 
 vengono descritti il quadro ecografico normale della tiroide , le sue varianti , le difficolt di rappresentazione , le malattie tipiche e rare nelle loro varie manifestazioni nonch come possono essere diagnosticate ed anche trattate mediante gli ultrasuoni . 
tutte le varie e possibili modalit di studio ecografico vengono descritte con particolare enfasi sulle loro differenti opzioni , i possibili risultati e le difficolt delle varie procedure . alla diagnosi ecografica della patologia tiroidea fa seguito la descrizione delle procedure ecografiche minimamente invasive : biopsia con ago sottile , procedure semplici come iniezioni di etanolo o glucocorticoidi , oppure pi sofisticate come lablazione percutanea mediante laser o radiofrequenza . 
 il volume arricchito da un numero veramente notevole di immagini ecografiche , purtroppo quasi sempre non accompagnate da una didascalia adeguata o da frecce ecc . , per indicarne i pi significativi ed importanti dettagli . 
alle immagini ecografiche vengono poi , talvolta , associate antiche immagini da scanner lineari . lelenco delle voci bibliografiche ne comprende 296 , la maggior parte da riviste e libri russi ed 87 ( 25 le citazioni di autori italiani ) da riviste internazionali . 
gli autori del volume hanno la spiacevole abitudine di citare nel testo nomi ed anno di pubblicazione da parte di autori che non sono poi citati nella bibliografia presente alla fine del volume . questo volume potr essere apprezzato da coloro che hanno esperienza nel campo delle malattie della tiroide e dellecografia ; coloro invece che volessero iniziarsi in radiol med ( 2012 ) 117 : 162163 willing to begin learning this art should refer cautiously to this book due to the above mentioned problems with images . questarte diagnostica dovrebbero consultarlo con precauzione a causa dei problemi sovracitati riguardo alle immagini . 
cademartiri1 , 2 1dipartimento di radiologia e del cardio - polmonare , azienda ospedaliero - universitaria di parma , c / o piastra tecnica piano 0 , via gramsci 14 , 43100 parma , italy 2dipartimento di radiologia e cardiologia , erasmus medical center , rotterdam , the netherlands 3dipartimento di radiologia e cardiologia , ospedale san gennaro , napoli , italy 4cpc centro prevenzione cardiovascolare , ospedale san raffaele , milano , italy 5dipartimento di radiologia e cardiologia , azienda asl , carrara , italy 6dipartimento di radiologia , universit di messina , messina , italy 7dipartimento di cardiologia , universit di foggia , foggia , italy 8dipartimento di radiologia , azienda ospedaliero - universitaria san martino , genova , italy correspondence to : f . 
cag demonstrated the absence of significant coronary artery disease ( cad ) in 47% ( men 42% ; women 56% ) , single - vessel disease in 25% ( men 36% ; women 22% ) and multivessel disease in 29% ( men 32% ; women 23% ) of patients . 
scopo del presente lavoro stato valutare laccuratezza diagnostica dellangiografia coronarica non invasiva con tomografia computerizzata ( ctca ) nellindividuazione delle stenosi coronariche significative ( riduzione del lume coronarico50% ) confrontata con la coronarografia convenzionale ( cag ) nella popolazione maschile e femminile . 
il 47% ( maschi 42% ; femmine 56% ) mostravano coronarie indenni o con lesioni che determinavano stenosi < 50% , il 25% ( maschi 36% ; femmine 22% ) mostrano malattia critica di un solo vaso , ed il 29% ( maschi 32% ; femmine radiol med ( 2012 ) 117 : 618 95% ; women 90% ) and 99% ( men 98% ; women 100% ) , respectively . 
nellanalisi per paziente la sensibilit , specificit , valore predittivo positivo e negativo della ctca sono risultati 99% ( maschi 98% ; femmine 100% ) , 92% ( maschi 92% ; femmine 92% ) , 94% ( maschi 95% ; femmine 90% ) , 99% ( maschi 98% ; femmine 100% ) , rispettivamente . 
la ctca una metodica diagnostica affidabile sia per lelevata sensibilit che per lelevato valore predittivo negativo anche nella popolazione femminile . parole chiave angiografia coronarica tc angiografia coronarica convenzionale maschi femmine genere accuratezza diagnostica registro introduction introduzione computed tomography coronary angiography ( ctca ) is an accurate and robust modality for diagnosing and excluding coronary artery disease ( cad ) [ 18 ]  . 
the female population is , in fact , characterised by a greater prevalence of atypical symptoms , a greater prevalence of false positive / false negative stress tests and , as a result , a poorer prognosis associated with poorer adherence to guideline prescriptions [ 17 , 24 ]  . 
 in this study , we present a patient population drawn from a multicentre ctca registry that focuses on diagnostic langiografia coronarica con tomografia computerizzata ( ctca ) una metodica accurata e robusta per la diagnosi e lesclusione della malattia coronarica [ 18 ]  . 
la popolazione femminile , infatti , caratterizzata da una maggiore prevalenza di sintomatologia atipica , da una maggiore prevalenza di test provocativi falsi positivi / negativi e , come conseguenza , anche da una peggiore prognosi legata alla minore aderenza delle prescrizioni alle linee guida [ 17 , 24 ]  . 
 radiol med ( 2012 ) 117 : 618 accuracy compared with conventional coronary angiography ( cag ) , with particular attention paid to the diagnostic performance between the male and female population . 
 in questo lavoro presentiamo una casistica derivante da un registro multicentrico di ctca a confronto con la coronarografia convenzionale ( cag ) con particolare attenzione al confronto della performance diagnostica tra popolazione maschile e femminile . 
participating centres are characterised by : volume of ctca examinations > 300 / year ; on - site or directly accessible catheterisation laboratory ; operator experience > 5 years ; ability to maintain a detailed longitudinal prospective database of all characteristics of patients who undergo ctca ; homogeneous scan protocols and image analysis ( patient pharmacological preparation , scan / reconstruction parameters , contrast agent administration ) ; systematic evaluation of examinations by at least two expert operators in 90% of cases ( double reading )  . study population from may 2004 to december 2006 , 1 , 372 consecutive patients ( 882 men , 490 women ; mean age 59.311.9 years ; table 1 ) were studied with ctca . 
diagnostic performance of ctca in identifying significant coronary artery atherosclerotic lesions , with cag used as the reference technique , is reported in terms of sensitivity , specificity , positive ( ppv ) and negative ( npv ) predictive values , with 95% confidence intervals ( ci ) calculated with binomial expansion . 
i centri partecipanti sono caratterizzati da : volume di esami ctca > 300 / anno ; presenza di laboratorio di emodinamica in loco o direttamente afferente ; esperienza degli operatori > 5 anni ; capacit di mantenere un database dettagliato longitudinale prospettico di tutte le caratteristiche dei pazienti che effettuano ctca ; impostazione omogenea dei protocolli di scansione ed analisi delle immagini ( preparazione farmacologica del paziente , parametri scansione / ricostruzione e somministrazione del mezzo di contrasto ) ; valutazione sistematica delle indagini da parte di almeno due operatori esperti in pi del 90% dei casi ( doppia lettura )  . popolazione studiata da maggio 2004 a dicembre 2006 , sono stati studiati mediante ctca 1372 pazienti consecutivi ( 882 maschi , 490 femmine , et media 59 , 311 , 9 anni ; tabella 1 ) candidati allesecuzione di una cag allo scopo di determinare la presenza , la severit e lestensione della malattia coronarica [ 2 ]  . 
il comitato etico ha approvato il protocollo di studio e tutti i pazienti hanno fornito un consenso informato . analisi statistica i dati sono presentati come prevalenze , medie e deviazioni standard . 
la performance diagnostica dellangiografia coronarica mediante ctca nellindividuazione delle lesioni aterosclerotiche coronariche significative , utilizzando la cag come tecnica di riferimento di seguito riportata come sensibilit , specificit , valore predittivo positivo e negativo con intervalli di confidenza ( ic ) al 95% calcolati con espansione binomiale . 
only 34% of patients with obstructive cad were women , whereas the 48% della popolazione si presentava con angina stabile ( 48% ; 644 / 1372 ; maschi 46% vs femmine 51% )  . 
i test strumentali provocativi hanno performance inferiore nella popolazione femminile [ 17 ] , ed il trattamento risulta essere anche meno intensivo e meno aderente alle linee guida con un conseguente peggioramento della prognosi rispetto alla popolazione maschile femminile , fig . 
lr evaluation shows how the weighting of the diagnostic accuracy by disease prevalence produces a reduction in the lr + and lr when passing from the per - segment to the perpatient evaluation . 
la valutazione dei lr dimostra come la pesatura dellaccuratezza diagnostica per la prevalenza di malattia determini una riduzione del lr + e del lrnel passaggio dalla valutazione per - segmento a quella per - paziente . 
imaging stress tests perform less well in the female population [ 17 ] , and treatment also tends to be less intensive and less adherent to guidelines , with a consequent worsening of prognosis in comparison with the male population [ 24 ]  . 
in particular , a meta - analysis of a variety of stress tests showed that the traditional exercise test has a sensitivity and specificity in the male population of 68% and 77% , which fall to 61% and 70% in the female population [ 17 ]  . 
in particolare , da una meta - analisi di vari test provocativi effettuati nella popolazione femminile risulta che il test da sforzo tradizionale offre una sensibilit e specificit del 68% e 77% nei maschi che si riduce al 61% e 70% nelle femmine , rispettivamente [ 17 ]  . 
nelle femmine la scintigrafia al tallio consente dei valori sensibilit e specificit del 78% e 64% , mentre lecocardiografia da stress fornisce una sensibilit e specificit dell86% e 77% , rispettivamente [ 17 ]  . 
in particolare la sensibilit ed il valore predittivo per paziente sono risultati del 100% e 100% , rispettivamente , con valori di specificit e valore predittivo positivo al di sopra del radiol med ( 2012 ) 117 : 618 fig . 
 when a test ( i.e. , ctca ) is positive , the probability that a patient effectively has a coronary stenosis 50% significantly increases , even when the pretest probability is low or very low ( range 020% )  . 
per un test ( in questo caso ctca ) positivo aumenta significativamente la probabilit che un paziente sia effettivamente portatore di una stenosi coronarica 50% anche con probabilit pre - test bassa o molto bassa ( range 0%20% )  . 
the cost / benefit ratio must take into account numerous factors , including biological cost ( dose of ionising radiation compared with tests that do not use ionising radiation ) , economic cost ( with respect to lessexpensive tests ) , geographic distribution of the technique 90% . 
il rapporto costo / beneficio deve tenere conto di molti fattori tra cui il costo biologico ( dose di radiazioni rispetto a test che non necessitano di radiazioni ) , il costo economico ( rispetto a test con costi inferiori ) , la disponibilit territoriale della metodica ( rispetto a metodiche diagnostiche molto pi diffuse ) , lexpertise ( ancora limitato ad alcuni centri )  . 16 radiol med ( 2012 ) 117 : 618 fig . 
positive and negative likelihood ratios ( lr + and lr ) of ctca in the female population are more favourable than those of the exercise test , spect and stress echocardiography [ 17 ]  . 
i quozienti di probabilit positivo e negativo ( lr + e lr - ) della ctca nella popolazione femminile sono pi favorevoli rispetto a quelli del test da sforzo , della tomografia computerizzata a emissione di fotoni singoli ( spect ) , dellecocardiografia da stress [ 17 ]  . 
lr , likelihood ratio ; stress ecg , test da sforzo ; spect , scintigrafia da stress ; stress echo , ecocardiografia da stress ; ctca , angiografia coronarica con tomografia computerizzata . ( compared with more widely diffuse diagnostic modalities ) and expertise ( which is still limited in some centres )  . limiti dello studio study limitations the major limitation of ctca is still radiation dose . 
however , the introduction of new hardware and software able to provide adequate image quality using prospective triggering based on electrocardiographic signal has brought dose values to < 5 msv [ 912 ]  . 
tuttavia , lintroduzione di nuovi hardware e software in grado di fornire adeguata qualit di immagine utilizzando il triggering prospettico basato sul segnale elettrocardiografico ( ecg ) consentono di portare i valori di dose al di sotto dei 5 msv [ 912 ]  . 
 i dati del nostro registro dimostrano che la ctca una metodica morfologica per la valutazione dellaterosclerosi coronarica ostruttiva , robusta ed affidabile nella popolazione femminile in cui pi difficile stratificare la presenza di stenosi significative . 
in our experience , severe acute toxic reactions are common in patients treated with radiotherapy and concurrent cetuximab , resulting in frequent breaks or incomplete treatment with potential reduction in disease control . 
nella nostra esperienza gli effetti tossici acuti di entit severa nei pazienti trattati con radioterapia e cetuximab concomitante sono stati comuni implicando interruzioni frequenti della terapia o limpossibilit di completare il trattamento con potenziale minor efficacia sul controllo della malattia . parole chiave tumori del distretto testa - collo cetuximab radioterapia tossicit 126 introduction the efficacy of radiotherapy as the primary treatment option in locoregionally advanced head and neck carcinoma is well established . 
the trial by bonner et al . [ 5 ] demonstrated the value of cetuximab in association with high - dose radiation therapy in locoregionally advanced head and neck squamous cell carcinoma . 
the authors highlight how this therapeutic regimen does not increase toxicity compared with radiotherapy alone , although no randomised trial comparing the association of radiotherapy with cetuximab and with other chemotherapeutic agents has been published to date . on the basis of these reports and with the aim of reducing toxicity and improving compliance , we prospectively studied14 patients with locally advanced head and neck squamous cell carcinoma treated at sant andrea hospital radiation oncology department with concurrent cetuximab and radiotherapy . materials and methods fourteen patients with stage iii or iv nonmetastatic squamous cell carcinoma of the oropharynx , hypopharynx or larynx where treated with concurrent cetuximab and radiotherapy from september 2007 to march 2009 . 
extent of primary disease , regional lymph node involvement and possible synchronous malignancies of the upper aerodigestive tract were evaluated with computed tomography ( ct ) scan and / or magnetic resonance ( mr ) imaging of the head and neck . 
three patients had stage iii and 11 had stage iv disease according to the 1998 staging classification of the american joint committee on cancer ( ajcc ) ( table 1 )  . 
patients presenting with karnofsky performance status 60 , normal hepatic , renal and haematopoietic function and no evidence of metastatic disease at the time of diagnosis were considered medically suitable for curative radiotherapy . 
two patients had previously undergone surgery with positive resection margins , and one radiol med ( 2012 ) 117 : 125132 introduzione lefficacia della radioterapia come trattamento primario nel carcinoma del distretto testa - collo localmente avanzato stata ben documentata ; lassociazione della chemioterapia concomitante aggiunge un beneficio con un aumento della tossicit [ 14 ]  . 
 [ 5 ] ha dimostrato il valore del cetuximab in associazione alla radioterapia ad alte dosi nei carcinomi squamosi localmente avanzati cervico - facciali ; il beneficio osservato in termini di aumento del controllo loco - regionale di malattia , di sopravvivenza libera da malattia e di sopravvivenza totale significativo . 
gli autori hanno evidenziato come questo schema terapeutico non comporti un aumento della tossicit rispetto alla radioterapia esclusiva sebbene al momento non esistano trial randomizzati che confrontino lassociazione della radioterapia e del cetuximab e della radioterapia con altri agenti chemioterapici . in base a questi dati e con lo scopo di ridurre la tossicit e migliorare la compliance al trattamento , 14 pazienti affetti da carcinoma squamoso cervico - facciale localmente avanzato sono stati trattati presso il dipartimento di radioterapia oncologica dellospedale santandrea con radioterapia e cetuximab da settembre 2007 . 
 materiali e metodi quattordici pazienti con carcinoma a cellule squamose non metastatico dellorofaringe , ipofaringe e laringe stadio iiiiv sono stati trattati da settembre 2007 a marzo 2009 con radioterapia e cetuximab concomitante . 
la diagnosi e la stadiazione sono state stabilite in base alla storia , allesame obiettivo , agli esami di laboratorio , agli studi di imaging , agli esami endoscopici e alle biopsie . 
lestensione della malattia primitiva , il coinvolgimento linfonodale e eventuali neoplasie sincrone del tratto respiratorio o gastroenterico superiore sono stati valutati con studi di tomografia computerizzata ( tc ) o risonanza magnetica ( rm ) della testa e del collo ; in 8 / 14 pazienti stato eseguito anche uno studio di tomografia ad emissione di positroni ( pet ) - tc . 
in tre pazienti la malattia era al iii stadio e in 11 al iv stadio secondo la classificazione american joint committee on cancer ( ajcc ) del 1998 ( tabella 1 )  . 
i pazienti che presentavano un karnofsky performance status60 , funzionalit epatica , renale ed ematopoietica normali e senza evidenza di metastasi a distanza al momento della diagnosi sono stati considerati clinicamente adatti per radiol med ( 2012 ) 117 : 125132 table 1 patient characteristics patient no . 
 age ( years ) gender site oropharynx hypopharynx larynx oropharynx oropharynx oropharynx oropharynx oropharynx oropharynx oropharynx oropharynx oropharynx oropharynx oropharynx hypopharynx orofaringe ipofaringe laringe orofaringe orofaringe orofaringe orofaringe orofaringe orofaringe orofaringe orofaringe orofaringe orofaringe orofaringe ipofaringe tnm t4a n2a t1 n2a t3 n0a t4a n2b t4a n2a t3 n0 t2 n2a t4a n2b t2 n2b t2 n2ca t2 n2a t3 n2b t1 n1 t3 n2c t2 n2ab tnm t4a n2a t1 n2a t3 n0a t4a n2b t4a n2a t3 n0 t2 n2a t4a n2b t2 n2b t2 n2ca t2 n2a t3 n2b t1 n1 t3 n2c t2 n2ab stage iva apatients who underwent surgery ; bpatients with relapse tabella 1 caratteristiche dei pazienti paziente et ( anni ) sesso sede stadio apazienti sottoposti a chirurgia ; bpazienti con recidiva patient had a disease relapse . 
no percutaneous endoscopic gastrostomy ( peg ) or nasogastric tube was initially recommended , but one patient , affected by nervous anorexia , received a prophylactic peg tube due to low weight before the start of treatment . therapeutic regimen radiotherapy was administered for a total dose of 64.870 gy in conventional fractions ( 1.82.0 gy ) to the primary tumour and involved nodal areas , and 50 gy to uninvolved nodal areas . 
nessun paziente aveva precedentemente effettuato un trattamento radiante o chemioterapico ; due pazienti erano stati sottoposti ad intervento chirurgico con margini di resezione positivi e un paziente aveva una recidiva di malattia . 
il posizionamento del sondino naso - gatrico o la percutaneous endoscopic gastrostomy ( peg ) a scopo profilattico non stato inizialmente raccomandato in nessun caso fatta eccezione per una paziente affetta da anoressia nervosa che stata sottoposta a peg profilattica prima dellinizio del trattamento a causa del basso peso corporeo . 
cetuximab was initiated 1 week before radiotherapy at an initial dose of 400 mg / m2 of body surface area ( bsa ) , followed by weekly 250 mg / m2 for the duration of radiotherapy . skin management all patients were educated about skin care ( avoiding irritant soaps , sun exposure , etc . ) and used moisturising lotions from the start of treatment . 
 results treatment compliance treatment was definitively stopped after 38 gy due to skin toxicity in one patient , who died of sepsis 3 weeks later ; in one patient , the combined treatment was suspended after 5 weeks due to g3 anaemia and respiratory complications , with apparent complete response , so that 12 of the 14 patients received the planned radiation dose . 
radiation therapy was completed without breaks in 6 / 12 patients and temporarily suspended in 6 / 12 , with a median interval of 8 ( range 512 ) days . 
cetuximab was delayed or definitively suspended owing to skin or mucous toxicity . skin toxicity g1 in - field rash ( dermatitis ) occurred in four ( 28% ) patients , g2 in five ( 36% ) and g3 in four ( 28% )  . 
in one patient , the reaction occurred after the first administration ( loading dose ) , in three patients after the second and in the other cases during the fourth . 
skin reactions completely resolved within 46 weeks after the end of treatment ; two patients required hospital admission . 64 , 870 gy con frazionamento convenzionale ( 1 , 82 , 0 gy ) sul tumore primitivo e sulle stazioni linfonodali coinvolte e di 50 gy sulle regioni linfonodali non coinvolte . 
i primi 10 pazienti sono stati trattati con tecnica 3d conformazionale mentre la tecnica ad intensit modulata ( imrt ) e la radioterapia guidata dalle immagini ( igrt ) sono state introdotte successivamente nel nostro dipartimento e sono state applicate negli ultimi quattro pazienti trattati utilizzando lo stesso schema di frazionamento di dose dei pazienti trattati con tecnica 3d conformazionale . 
il cetuximab stato iniziato una settimana prima della radioterapia ad una dose iniziale di 400 mg / m2 di superficie corporea , seguito da una dose di 250 mg / m2 una volta la settimana per tutta la durata del trattamento radiante . 
 cura della cute tutti i pazienti sono stati istruiti sulla cura della cute ( evitare saponi irritanti , esposizione al sole , ecc . ) e sullutilizzo di creme idratanti dallinizio del trattamento . 
il rash acneiforme stato trattato con doxiciclina per via orale alla dose di 100 mg / die e gel deosina per via topica ; in caso di persistenza del rash venivano utilizzate crme a base di corticosteroidi e antibiotici per uso topico . 
per consentire il confronto con i dati di letteratura la tossicit cutanea stata classificata sia in base al national cancer institute ( nci ) common terminology criteria for adverse events ( ctcae ) versione 3.0 sia in base al sistema radiation therapy oncology group ( rtog ) acute radiation morbidity scoring criteria ; gli altri effetti avversi sono stati classificati in base al sistema rtog acute radiation morbidity scoring criteria . 
 risultati compliance al trattamento in un paziente la terapia stata definitivamente interrotta dopo 38 gy per tossicit acuta e circa 3 settimane pi tardi avvenuto il decesso per sepsi ; un paziente ha sospeso il trattamento combinato dopo 5 settimane per anemia g3 e complicanze respiratorie con apparente risposta completa , per cui solo 12 dei 14 pazienti totali hanno ricevuto la dose di radiazioni pianificata . 
la radioterapia stata completata senza interruzioni in 6 / 12 pazienti e temporaneamente sospesa in 6 / 12 pazienti con una durata media del periodo di sospensione di 8 giorni ( range 512 giorni )  . 
la somministrazione del farmaco stata posticipata o definitivamente sospesa per tossicit cutanea o mucosa . tossicit cutanea dermatite da radiazioni in - field di grado 1 si verificata in 4 ( 28% ) pazienti , g2 in 5 ( 36% ) e g3 in 4 ( 28% ) pazienti . 
le reazioni cutanee sono andate incontro a risoluzione completa entro 46 settimane dopo la fine del trattamento ; in due pazienti stato necessario il ricovero ospedaliero . tossicit mucosa tossicit mucosa g2 stata osservata in 7 ( 50% ) pazienti , g3 in 6 ( 43% ) e g4 in 1 ( 7% ) ( tabella 3 )  . 
un paziente deceduto per sepsi durante il trattamento ; la terapia era stata definitivamente interrotta dopo 38 gy per tossicit cutanea con disepitelizzazione della cute del collo e edema di un arto superiore . 
at a median follow - up of 9.7 months , 11 patients showed complete local response ; two of them subsequently relapsed at the primary disease site , and one developed lung metastases . 
 un paziente deceduto per progressione di malattia dopo una risposta parziale e uno deceduto per altre cause e non stato possibile valutare la risposta . discussione il trial randomizzato di fase iii pubblicato nel 2006 da bonner et al . 
 [ 5 ] ha dimostrato come lutilizzo del cetuximab , in aggiunta alla radioterapia ad alte dosi per il carcinoma squamoso localmente avanzato del distretto testacollo produca miglioramenti significativi nella durata del controllo loco - regionale di malattia e nella sopravvivenza totale rispetto alla sola radioterapia ( 49 mesi vs 29 , 3 mesi ) senza la tossicit proibitiva della chemioterapia . 
 [ 6 ] confermano che lassociazione del cetuximab e della radioterapia rappresenta unopzione importante in questi pazienti ( sopravvivenza totale a 5 anni 45 , 6% nel gruppo di pazienti trattati con cetuximab e radioterapia vs 36 , 4% nel gruppo sottoposto a radioterapia esclusiva )  . 
in questo lavoro gli autori hanno sottolineato anche come lo sviluppo di rash acneiforme di grado 2 o superiore fosse associato a una maggiore sopravvivenza , anche se nel nostro lavoro a causa del piccolo numero di pazienti non stato possibile stabilire una relazione tra entit della reazione cutanea e risposta al trattamento . 
 [ 9 ] hanno osservato tassi di rash acneiforme di grado 3 o superiore del 46% , tassi di dermatite di grado 34 del 77% , tassi di disfagia di grado 3 del 54% e di mucosite radiol med ( 2012 ) 117 : 125132 vs . 
 [ 6 ] time of appearance and severity were similar to those we observed in patients with nasopharyngeal cancer or with undifferentiated carcinoma treated with radiotherapy and platinum - based chemotherapy , but areas receiving low radiation doses , such as the mucocutaneous junction of the lips , were more frequently involved . 
radiation therapy was completed without breaks in 6 / 12 of our patients and temporarily suspended in the other six , with a median of 8 days for severe mucous and / or cutaneous toxicity . 
in head and neck cancer patients receiving cisplatin during radiotherapy at our institute , radiotherapy breaks are rarely required ; however , the small number of patients enrolled in this study and the differences in patient selection criteria allow no comparison . 
 although the characteristics of our series are similar to those enrolled in bonner et al.s trial [ 6 ] , the patient group was smaller and radiation treatment technique and fractionation schemes different . 
in our experience , the possible causes of the enhanced toxicity observed can only be hypothesised and may be due to patient characteristics , inapgrado 3 del 77% in 13 pazienti trattati con cetuximab e radioterapia ad alte dosi . in questo lavoro abbiamo riportato i dati sui primi 14 pazienti con carcinoma squamoso cervico - facciale stadio iii - iv trattati nella nostra unit operativa con radioterapia ad alte dosi e cetuximab . 
nella nostra esperienza il tasso di tossicit cutanea g3 ( rtog ) o superiore stato del 36% e rash acneiforme g3 ( rtog ) stato osservato nel 56% dei pazienti ( tabella 3 ) ; queste percentuali sono significativamente pi alte di quelle riportate da bonner et al . 
i tempi di comparsa e la severit sono state simili a quelle osservate nei pazienti con tumori nasofaringei o con carcinomi indifferenziati del distretto testa - collo che sono stati trattati presso il nostro reparto con radioterapia e chemioterapia con platino , ma le aree che hanno ricevuto basse dosi di radiazioni , come la giunzione , muco - cutanea delle labbra , sono state coinvolte pi frequentemente . 
altri effetti tossici associati alla radioterapia della testa e del collo come la disfagia , il dolore , la perdita di peso , hanno avuto tassi dincidenza simili a quelli comunemente osservati . 
 [ 6 ] il 90% dei pazienti trattati con il cetuximab hanno ricevuto la dose di radiazioni prescritta nel tempo pianificato ; il trattamento stato completato senza interruzioni in 6 su 12 dei nostri pazienti e temporaneamente sospeso in altri 6 , per tossicit cutanea o mucosa severa , con una durata media della sospensione di 8 giorni . 
 sebbene il piccolo numero di pazienti inclusi in questo lavoro e le differenze nei criteri di selezione non consentano un confronto , nei pazienti con neoplasie del distretto testacollo sottoposti presso il nostro istituto a chemioterapia con cisplatino durante la radioterapia , interruzioni del trattamento sono raramente necessarie . 
 [ 6 ] , il campione piccolo e le tecniche di radioterapia e gli schemi di frazionamento sono differenti.nella nostra esperienza le possibili cause dellaumentata tossicit osservata possono solo essere ipotizzate ; potrebbero essere attribuite a le caratteristiche dei pazienti , alla gestione inappropriate della tossicit , o alla tecnica e allo schema di trattamento . il cetuximab ha mostrato di ottenere un controllo di malattia superiore alla radioterapia esclusiva nei carcinomi 132 radiol med ( 2012 ) 117 : 125132 propriate toxicity management or treatment technique and schedule . 
 our experience indicates it is useful to take into account the patients general condition ( age , performance status , comorbidities , etc . ) when deciding upon total radiation dose , fractionation , treatment technique and association with systemic therapies . 
further investigations will help us understand the mechanisms involved in the toxicity profile of combined cetuximabradiotherapy treatment and the effectiveness of this treatment in improving local control , survival and quality of life compared with standard chemoradiation treatment . avanzati del distretto testa - collo in trial randomizzati ; sulla base dei risultati della nostra piccola esperienza , il suo utilizzo potrebbe essere suggerito con maggiore cautela rispetto a quanto riportato dai lavori recentemente pubblicati . noi consideriamo la nostra esperienza comunque utile per considerare le condizioni generali del paziente ( et , performance status , comorbidit , ecc . ) nel processo decisionale sulla dose totale di radiazioni , sul frazionamento , sulla tecnica di trattamento e sullassociazione con le terapie sistemiche e per migliorare la gestione della tossicit acuta , la qualit di vita del paziente e ridurre le interruzioni di terapia e la durata totale . 
fugazzola1 1universit degli studi dellinsubria , ospedale di circolo e fondazione macchi , scuola di specializzazione in radiodiagnostica , viale borri 57 , 21100 varese , italy 2universit degli studi dellinsubria , dipartimento di fisica sanitaria , ospedale di circolo e fondazione macchi , varese , italy correspondence to : a . 
in 21 pazienti non stata osservata la presenza di endoleak : 12 / 21 presentavano una riduzione del volume ad entrambi i controlli ( 9 , 7% / 19 , 5% rispettivamente ) ; 8 / 21 presentavano un incremento iniziale ( 9 , 8% ) con una riduzione tardiva ( 10 , 5% ) ; in 1 / 21 il volume era incrementato ad entrambi i controlli ( endotension )  . 
stato osservato un endoleak in 11 pazienti ( 1 / 11 tipo i , 9 / 11 tipo ii e 1 / 11 tipo iii ) ; 4 / 9 endoleak tipo ii presentavano una riduzione volumetrica ad entrambi i controlli dopo evar ( 8 , 5% / 19 , 5% )  . 
per i controlli successivi , lanalisi volumetrica consente di eliminare luso del mdc nei pazienti asintomatici con volume dellaneurisma stabile o ridotto . parole chiave imaging tc trattamento endovascolare per aneurisma dellaorta addominale ( evar ) aorta aneurisma dellaorta addominale introduction introduzione the introduction of endovascular repair ( evar ) techniques for abdominal aortic aneurysms had led to a remarkable reduction in mortality and morbidity compared with the traditional surgical treatment [ 1 ]  . 
endoleak is the most frequent complication ( 411% , according to the most recent studies ) and in some cases involves the need for subsequent treatment to guarantee complete sac exclusion [ 25 ]  . 
ct allows not only correct visualisation of the stent - graft but also evaluation of the size of the aneurysmal sac and , by means of the injection of contrast material , identification and characterisation of endoleaks [ 8 , 9 ]  . 
according to the main monitoring protocols , the follow - up of patients after evar involves ct angiography ( cta ) 13 months after positioning of the stent - graft and , in the absence of complications , yearly thereafter [ 8 , 1013 ]  . 
aneurysms that remain stable or shrink after evar present a reduced risk of rupture and require no further intervention , even in the presence of small endoleaks [ 1419 ]  . 
volumetric analysis quantifies variations in size of the aneurysm more accurately than the commonly used linear measurements [ 14 , 15 , 2022 ]  . in their recent paper , bley et al . 
 [ 23 ] proposed serial volumetric analysis of the aneurysmatic sac with nonenhanced ct for long - term follow - up of abdominal aortic aneurysms after evar in asymptomatic patients . 
nonenhanced ct made it possible to reduce patient exposure , the use lavvento delle tecniche di riparazione endovascolare degli aneurismi dellaorta addominale ( evar ) ha portato ad una significativa riduzione di mortalit e morbilit rispetto alla terapia chirurgica tradizionale [ 1 ]  . 
la presenza di un endoleak rappresenta la complicanza pi frequente ( 4%11% negli studi pi recenti ) e comporta in alcuni casi la necessit di un successivo trattamento per garantire lesclusione della sacca [ 25 ] poich un endoleak pu insorgere in qualsiasi momento dopo il posizionamento dellendoprotesi , questi pazienti richiedono un follow - up che dura tutta la vita [ 68 ]  . 
tra le varie modalit di imaging , la tomografia computerizzata ( tc ) rimane quella maggiormente utilizzata a questo scopo ; tale metodica consente , infatti , non solo una corretta visualizzazione dellendoprotesi , ma anche la misurazione delle dimensioni della sacca aneurismatica e , mediante liniezione del mezzo di contrasto ( mdc ) , lidentificazione e la caratterizzazione degli endoleaks [ 8 , 9 ]  . 
secondo i principali protocolli di sorveglianza , il follow - up dei pazienti sottoposti ad evar prevede un esame angio - tc a 13 mesi dal posizionamento dellendoprotesi e successivamente , in assenza di complicanze , con scadenza annuale [ 8 , 1013 ]  . 
dopo evar , gli aneurismi che rimangono stabili o diminuiscono di dimensioni presentano un ridotto rischio di rottura e non richiedono ulteriori interventi anche in presenza di piccoli endoleaks [ 1419 ]  . 
 [ 23 ] hanno proposto lutilizzo dellanalisi volumetrica seriata eseguita su tc senza mdc per il follow - up a lungo termine degli aneurismi dellaorta addominale dopo evar in pazienti asintomatici ; gli autori hanno concluso che un incremento volumetrico 74 radiol med ( 2012 ) 117 : 7284 of nephrotoxic contrast agents and the costs of follow - up . 
 according to the authors , the use of contrast - enhanced ct remained mandatory up to 3 months after the procedure , as , in the short term , small endoleaks could cause volumetric modifications under the detection threshold [ 23 ]  . 
 our work aimed to assess the clinical usefulness of volumetric analysis of the aneurysmal sac for the followup of patients after evar of abdominal aorta , supporting the results of bley et al . 
 [ 23 ] , and to demonstrate operator independence of the proposed method . materials and methods ninety - nine ctas of 33 patients ( 29 men , four women ; average age 74.4 years , range 6097 years ) were retrospectively evaluated . 
the patients were selected from among 302 patients who underwent evar at our institution between june 2005 and march 2009 , according to the following inclusion criteria : presence of an abdominal subrenal aortic aneurysm treated with a bifurcated stent - graft ( ruptured aneurysms with formation of retroperitoneal haematoma and dissected aneurysms were excluded ) ; all examinations were performed with the same 64 - slice ct scanner ( aquilion 64 , toshiba medical system , tokyo , japan ) , with the following parameters : beam collimation 0.5 mm64 , gantry rotation time 0.5 s , 120 kv , automatic exposure modulation ( aec , standard deviation 12 ) , field of view ( fov ) m / l , pitch factor ( pf ) 0.8 , slice thickness 1.0 mm , reconstruction interval 0.8 mm ; all scans were performed before and after i.v. 
injection of 100120 ml of iodinated contrast material ( iomeprol 350 mgi / ml , iomeron , bracco , milan , italy ) at an injection rate of 3.5 ml / s , followed by a saline chaser of 40 ml at the same rate , using a double - head automated injector ( stellant d , medrad , pittsburgh , pa , usa ) , with arterialand venous - phase acquisitions ( delay 90 s ) ; availability of a ct examination performed before positioning of the stent - graft ( not older than 3 months before the intervention ) , an early follow - up scan ( mean interval 3.5 months , range 16 months ) and a late follow - up scan ( mean interval 14 months , range 720 months )  . datasets of the selected studies were transferred via local network from the departmental archives of our hospital to a dedicated workstation equipped with software for vascular reconstruction and volumetric analysis ( vitrea 2 , v 4.1.0 , vital , minnetonka , mn , usa )  . 
evaluation of cta studies comprised the volumetric measure of the aneurysmal sac before and after positioning of the stent - graft , and assessment of modifications during the follow - up period . del 2% rispetto allesame precedente significativo per la presenza di endoleak . 
 secondo gli autori lutilizzo del mdc rimane mandatorio nei primi 3 mesi dalla procedura in quanto endoleak di modesta entit possono non produrre variazioni volumetriche significative nel breve periodo [ 23 ]  . 
 scopo del nostro lavoro valutare lutilit clinica dellanalisi volumetrica della sacca aneurismatica nel follow - up dei pazienti sottoposti ad evar dellaorta addominale , confermando i rilievi di bley et al . 
 [ 23 ] , e stabilire la riproducibilit inter - osservatore del metodo proposto . materiali e metodi su un totale di 302 pazienti sottoposti ad evar nel nostro istituto nel periodo compreso tra giugno 2005 e marzo 2009 , sono state sottoposte a valutazione retrospettiva 99 angiotc di 33 pazienti ( 29 maschi e 4 femmine , et compresa tra 60 e 97 anni , et media 74 , 4 anni )  . 
i criteri di inclusione nello studio sono stati : pazienti portatori di aneurismi dellaorta addominale sottorenale trattati con endoprotesi aorto - bisiliaca ( sono stati esclusi gli aneurismi rotti con formazione di ematoma retroperitoneale e gli aneurismi dissecanti ) ; tutti gli esami sono stati espletati con tomografo a 64 strati ( aquilion 64 , toshiba medical system , tokio , giappone ) nel medesimo centro , con i seguenti parametri : collimazione del fascio 0 , 5 mm64 ; tempo di rotazione del gantry 0 , 5 s ; kv 120 ; mas secondo modulazione automatica dellesposizione ( aec , deviazione standard 12 ) ; campo di vista ( fov ) m / l ; pitch factor ( pf ) 0 , 8 ; spessore di strato 1 , 0 mm ; intervallo di ricostruzione 0 , 8 mm ; tutti gli esami sono stati eseguiti mediante scansioni in fase pre - contrastografica e dopo iniezione endovena ( ev ) di 100120 ml di mdc iodato ( iomeprolo 350 mgi / ml , iomeron , bracco , milano , italia ) alla velocit di 3 , 5 ml / s , seguito da 40 ml di soluzione fisiologica alla stessa velocit , mediante iniettore a doppia testa ( stellant d , medrad , pittsburgh , pennsylvania , usa ) , con acquisizioni in fase arteriosa e venosa ( ritardo di scansione 90 secondi ) ; di ogni paziente doveva essere disponibile un esame precedente al posizionamento dellendoprotesi ( effettuato non pi di 3 mesi prima dellintervento ) , un controllo precoce ( intervallo medio pari a 3 , 5 mesi dallintervento , range 16 mesi ) ed uno tardivo ( intervallo medio di 14 mesi , range 720 mesi )  . 
 i datasets delle indagini selezionate sono stati trasferiti attraverso la rete locale dagli archivi dipartimentali del nostro ospedale su una workstation dedicata dotata di radiol med ( 2012 ) 117 : 7284 fig . 
presentazione della schermata di lavoro del software utilizzato per il calcolo volumetrico della sacca aneurismatica : larea di lavoro divisa in quattro finestre dove vengono rappresentate le ricostruzioni mpr sagittale ( a ) e coronale ( b ) , limmagine assiale ( d ) e la ricostruzione 3d vr ( c )  . 
il profilo della sacca aneurismatica viene definito tracciando una serie di contorni sulle immagini assiali : la contemporanea visualizzazione sui piani coronale e sagittale assicura una corretta definizione della sacca . 
al termine del calcolo il volume viene rappresentato mediante una superficie colorata in verde sullimmagine 3d vr ( c ) , dove vengono riportati i valori di superficie in cm2 ( indicati dalla lettera a ) ed il volume in cm3 ( lettera v )  . the software presents a screen layout divided into four windows , showing the sagittal and coronal multiplanar reformatted ( mpr ) views , the axial image and the 3d volume - rendering ( vr ) image . 
the external profile of the aneurysmal sac was manually defined by drawing a series of contours on the axial images to enclose the entire volume of the aneurys the simultaneous visualisation on the coronal and sagittal planes ensured the correct definition of the sac . 
la rivalutazione delle angio - tc ha previsto la misurazione volumetrica della sacca aneurismatica prima e dopo il posizionamento dellendoprotesi al fine di rilevarne le modificazioni durante il follow - up . il software utilizzato per il calcolo volumetrico della sacca aneurismatica presenta unarea di lavoro divisa in quattro finestre , dove vengono rappresentate le ricostruzioni riformattate multiplanari ( mpr ) sagittali e coronali , limmagine assiale e la ricostruzione 3d volume rendering ( vr )  . 
il profilo esterno della sacca aneurismatica stato definito tracciando manualmente una serie di contorni sulle immagini assiali dal limite superiore dellaneurisma fino 76 radiol med ( 2012 ) 117 : 7284 table 1 distribution of patients according to the presence and type of endoleak and volume modifications of the aneurysmal sac in the series ( 32 patients )  . 
the table summarises the distribution of patients according to volume changes at early and late follow - up assessments ( reduction at both ; early increase and late reduction ; increase at both )  . 
among 32 patients , 16 ( 12 without endoleaks and four with type ii endoleaks ) showed a volume reduction at both follow - up assessments , eight ( all without endoleaks ) an early increase and a late reduction , and eight ( one without endoleak , one with type i endoleak , five with type ii endoleaks and one with type iii endoleak ) a volume increase at both follow - up assessments volume variations endoleak early follow - up late follow - up type i type ii type iii no leak decrease increase increase decrease decrease increase tabella 1 distribuzione dei pazienti per presenza , tipo di endoleak e variazione volumetrica della sacca aneurismatica nella serie personale ( 32 pazienti )  . 
in tabella sono riportati i pazienti della casistica divisi in base alla variazione volumetrica al primo ed al secondo controllo tc ( riduzione ad entrambi i controlli , aumento al primo e riduzione al secondo , aumento ad entrambi i controlli )  . 
in totale , dei 32 pazienti arruolati , 16 presentano una riduzione volumetrica ad entrambi i controlli ( 12 senza leak , 4 con leak di tipo ii ) , 8 pazienti ( senza endoleak ) presentano un aumento al controllo precoce ed una successiva riduzione a quello tardivo e 8 pazienti ( 1 senza leak , 1 con leak di tipo i , 5 con leak di tipo ii e 1 con leak di tipo iii ) un aumento ad entrambi i controlli variazioni volumetriche endoleak controllo precoce controllo tardivo tipo i tipo ii tipo iii non leak decremento incremento incremento decremento decremento incremento each volume was calculated by two blinded operators , one skilled ( ac ) , with 3 years of experience in the use of the software , and an initially inexperienced operator ( ec ) , who received a brief training of 2 weeks . 
volumetric modifications were compared for the presence of endoleak diagnosed in the contrast - enhanced phases of the study and re - evaluated by two radiologists ( cr and ff ) with experience in vascular imaging ( 5 and 6 years , respectively )  . 
the time required for postprocessing by the two operators was also compared . results one of the 33 patients initially enrolled in the study , with a type i endoleak , was excluded , as he underwent endovascular treatment of the leak between the early and late follow - up . 
nei casi in cui la dilatazione si estendeva alle arterie iliache , queste ultime non sono state incluse nel calcolo , assumendo come limite inferiore della sacca il carrefour aortico . 
le variazioni di volume sono state comparate con la presenza di endoleak diagnosticata nella fasi contrastografiche dello studio , rivalutate da due radiologi con esperienza di 6 e 5 anni nellimaging vascolare ( mm / cr )  . 
sono stati inoltre confrontati i tempi impiegati dai due operatori per il post processing . risultati dei 33 pazienti inizialmente arruolati nello studio , stato radiol med ( 2012 ) 117 : 7284 fig . 
2a - c comparison between volumes before and after placement of a bifurcated stent - graft in a patient with an abdominal aortic aneurysm with no evidence of endoleak at follow - up . 
 three - dimensional vr reconstructions of the cta examinations performed before ( a ) and after the treatment , at 6 ( b ) and 12 ( c ) months . 
2a - c confronto tra i volumi in un paziente con aneurisma dellaorta addominale trattato mediante posizionamento di endoprotesi aorto - bisiliaca , senza evidenza di endoleak ai successivi controlli . 
ricostruzioni 3d vr dellesame angio - tc eseguito prima del posizionamento dellendoprotesi ( a ) ed i successivi controlli a 6 ( b ) e 12 mesi ( c )  . 
in 1 / 9 patients with a type i endoleak , we detected a volume increment of 24.6% at the early follow - up and of 9.1% at the late follow - up ; subsequently the patient was treated with positioning of a stent - graft extension . 
in the only case of type iii endoleak , we detected a volume increase of escluso 1 paziente con endoleak di tipo i , poich sottoposto a trattamento endovascolare del leak nel periodo compreso tra il controllo precoce e quello tardivo . 
in 11 / 32 pazienti stato riscontrato al controllo precoce la presenza di un endoleak ( 1 / 11 di tipo i , 9 / 11 di tipo ii e 1 / 11 di tipo iii ) ; la presenza di tutti gli endoleak stata confermata al controllo tardivo , ad eccezione di un endoleak di tipo ii andato incontro a risoluzione spontanea . 
in 5 / 9 endoleak di tipo ii si evidenziato un incremento volumetrico medio rispettivamente del 15 , 4% al controllo precoce ( range 0%32 , 1% ) 78 radiol med ( 2012 ) 117 : 7284 fig . 
3a - f comparison between volumes before and after placement of a bifurcated stent - graft in a patient with an abdominal aortic aneurysm with a type ii endoleak and volume increase at the late follow - up assessment . 
three - dimensional vr reconstructions of computed tomography angiography ( cta ) examinations performed before ( a ) and after the treatment , at 6 ( b ) and 12 ( c ) months . 
the early follow - up cta ( b ) performed 6 months after evar , demonstrated a type ii endoleak , confirmed at late follow - up ( c - f )  . 
3a - f confronto tra i volumi in un paziente con aneurisma dellaorta addominale trattato mediante posizionamento di endoprotesi aorto - bisiliaca , con evidenza di endoleak di tipo ii ed incremento volumetrico della sacca ai successivi controlli . 
ricostruzioni 3d vr dellesame angio - tc eseguito prima del posizionamento dellendoprotesi ( a ) ed i successivi controlli a 6 ( b ) e 12 mesi ( c ) in basso a destra di ciascuna immagine riportata una sezione assiale in fase arteriosa . 
allinterno di ogni immagine 3d vr indicato il volume ( v ) della sacca aneurismatica , che dimostra un progressivo aumento , con 67 , 2 cm3 allesame pre - evar , 83 , 3 cm3 al primo controllo ( + 24% ) e 86 , 4 cm3 al secondo controllo ( + 3 , 7% )  . 
lesame angio - tc eseguito a 6 mesi evidenzia la presenza di un endoleak di tipo ii ( b ) , confermato anche al successivo controllo a 12 mesi ( c - f ) ; le ricostruzioni 3d vr ( d ) e planari curve ( cpr ) ( e , f ) dimostrano il rifornimento della porzione posteriore della sacca aneurismatica da parte di unarteria lombare destra ( frecce )  . 8% at the early follow - up and of 10.7% at the late followup . 
generally , types i and iii endoleaks are immediately treated ; the only two cases reported in our study ( one type i and one type iii ) were elderly patients , with several comorbidities and poor clinical condition at the time of the diagnosis , which contraindicated immediate intervention . 
nel paziente con endoleak di tipo i si assistito ad un incremento volumetrico pari al 24 , 6% al controllo precoce ed al 9 , 1% a quello tardivo ; successivamente il paziente stato trattato mediante il posizionamento di prolungamento protesico . 
4a - c comparison between volumes before and after placement of a bifurcated stentgraft in a patient with an abdominal aortic aneurysm with a type ii endoleak , which resolved spontaneously . 
three - dimensional vr reconstructions of computed tomography angiography ( cta ) examinations performed before ( a ) and after the treatment , at 6 ( b ) and 12 ( c ) months . 
4a - c confronto tra i volumi in un paziente con aneurisma dellaorta addominale trattato mediante posizionamento di endoprotesi aorto - bisiliaca , con evidenza di endoleak di tipo ii al primo controllo e successiva risoluzione spontanea del leak . 
ricostruzioni 3d vr dellesame angio - tc eseguito prima del posizionamento dellendoprotesi ( a ) ed i successivi controlli a 6 ( b ) e 12 mesi ( c )  . 
allinterno di ogni immagine 3d vr indicato il volume ( v ) , che dimostra una progressiva riduzione della sacca aneurismatica ( 89 cm3 allesame pre - evar , 81 , 8 cm3 al primo controllo e 73 , 3 cm3 al secondo controllo )  . 
al controllo a 6 mesi si osserva la presenza di un endoleak di tipo ii , non pi evidente al controllo a 12 mesi . from each other ; as a consequence , the volumetric measurement is reproducible and operator independent . 
the mean time necessary to evaluate one volume was 8 minutes ( range 518 minutes ) for the skilled operator and 11 minutes ( range 534 minutes ) for the inexperienced one . 
 discussion ct is the most widely accepted imaging modality for the long - term follow - up of evar to detect possible complications such as endoleaks [ 613 ]  . 
the dimensional evolution of the aneurysmal sac is the primary prognostic factor in these patients : a stable or shrinking aneurysm is associated with a low risk of rupture , even if associated with a small type ii endoleak . 
 due casi riportati nella nostra casistica ( uno di tipo i e uno di tipo iii ) riguardavano pazienti anziani , con numerose comorbilit e scadenti condizioni cliniche che controindicavano lintervento al momento della diagnosi . 
 lo scarto medio delle misure eseguite dai due operatori stato complessivamente del 0 , 9% , pari a 1 , 1 cm3 , con un range compreso tra 0%4 , 3% ( 05 , 3 cm3 )  . 
il test stato utilizzato per dimostrare che i due operatori , analizzando gli stessi dati , producono le stesse stime dei volumi tanto da essere , nella pratica , indistinguibili luno dallaltro ; di conseguenza , la misura volumetrica riproducibile indipendentemente dalloperatore . 
il valore p indica , infatti , la probabilit che i due operatori forniscano stime significativamente differenti dei volumi , quando in realt essi operano in maniera del tutto intercambiabile . 
pi tali cerchi sono allineati lungo la diagonale , pi i due operatori hanno prodotto stime simili . volumetric assessment is more accurate than common linear measurement for the follow - up of patients with abdominal aortic aneurysm after evar . 
several studies proved that diameter variations do not always represent real volume radiol med ( 2012 ) 117 : 7284 esperto ( range 518 minuti ) e di 11 minuti per laltro operatore ( range 534 minuti )  . discussione la tc la metodica pi comunemente utilizzata per il follow - up a lungo termine dei pazienti sottoposti ad evar che necessitano di una continua sorveglianza per identificare eventuali complicanze post - procedurali , come gli endoleak [ 613 ]  . 
levoluzione dimensionale della sacca aneurismatica rappresenta il principale fattore prognostico nei pazienti sottoposti a evar : alla riduzione o stabilit delle dimensioni della sacca si associa un basso rischio di rottura , anche in presenza di piccoli endoleak di tipo ii , che non richiedono perci alcun trattamento . 
 lanalisi volumetrica della sacca consente un pi accurato monitoraggio degli aneurismi dellaorta addominale ( aaa ) sottoposti ad evar rispetto alle comuni misurazioni lineari ; diversi studi hanno infatti evidenziato come non sempre le variazioni del diametro massimo rappresentino correttamente le reali modifiche dimensionali dellaneurisma [ 14 , 15 , 2022 ]  . 
il diametro infatti lespressione del cambiamento lineare dellaneurisma , mentre la valutazione del volume della sacca esprime la variazione dimensionale in tutti i piani dello spazio [ 14 ]  . 
 [ 23 ] hanno utilizzato lanalisi volumetrica seriata su tc senza mdc per il followup degli aaa dopo evar ; gli autori hanno impiegato un cut - off del 2% come limite nel definire la stabilit della sacca aneurismatica in pazienti asintomatici . 
distribution of volume determinations by each operator is represented by a box , extending from the first ( q1 / 4 ) to the third ( q3 / 4 ) quartile , and divided by the median ( q1 / 2 )  . 
il rettangolo ( box ) rappresenta i valori compresi tra il primo ed il terzo quartile ( q1 / 4 e q3 / 4 ) ed diviso al suo interno dalla mediana ( q1 / 2 )  . 
le misurazioni del volume ottenute da entrambi gli operatori sono del tutto simili ; si pu infatti notare come sia il box con le distribuzioni dei volumi tra il primo e il terzo quartile , che i minimi e massimi dei valori calcolati sono del tutto sovrapponibili . radiol med ( 2012 ) 117 : 7284 changes in aneurysm dimension [ 14 , 15 , 2022 ]  . 
concluded that the serial volumetric analysis of the aneurysmal sac with nonenhanced ct is an adequate screening test for long - term follow - up of abdominal aortic aneurysms after evar [ 23 ]  . in our experience , we recorded a volumetric decrease at the late follow - up in 20 / 21 cases without endoleak and in 4 / 9 cases with a type ii endoleak ; one of the nine cases of type ii endoleak presented a volumetric increase < 2% at the late follow - up . 
 [ 24 ] , comparing four operators ( one with a high level of experience , one with a moderate level and two with a low level ) , reported an interobserver variability of 7.2%. 
our results can be explained by a higher image quality due to the use of a 64 - slice ct scanner , whereas previous works used less - sophisticated ct devices ( singleor 4 - slice ct )  . 
furthermore , in our study , the inexperienced operator received 2 weeks training compared with 2 hours reported by caldwell . mean reconstruction time necessary for a single volume was 8 minutes for the skilled operator and 11 minutes for the inexperienced one . 
postprocessing time depends not only on operator experience but on aneurysm morphology , its extensecondo controllo post - evar un incremento volumetrico pari ad un massimo del 2% rispetto allesame precedente [ 23 ]  . 
 hanno concluso che il monitoraggio del volume della sacca aneurismatica su tc senza mdc un metodo valido per il follow - up a lungo termine degli aneurismi dellaorta addominale dopo evar [ 23 ]  . nella nostra esperienza abbiamo registrato una riduzione volumetrica della sacca aneurismatica al controllo tardivo in 20 / 21 casi di assenza di endoleak ed in 4 / 9 casi di endoleak di tipo ii ; in 1 / 9 casi di endoleak di tipo ii lincremento volumetrico al controllo tardivo stato inferiore al 2% . 
applicando il protocollo di bley alla nostra casistica , lutilizzo del mdc al controllo tardivo sarebbe stato necessario ( per entrambi gli operatori ) in soli 8 / 32 pazienti , pari al 25% . il calcolo del volume richiede operatori opportunamente addestrati , tempo e un software adeguato . 
nella nostra esperienza , la variabilit interosservatore risultata contenuta complessivamente nel limite del 0 , 9% , pari a 1 , 1 cm3 , con un range compreso tra 0 e 5 , 3 cm3 ( 0%4 , 3% )  . 
 questo ancora pi importante alla luce del fatto che uno degli operatori era esperto nellutilizzo del software , mentre laltro ha ricevuto solo un breve training , limitato a due settimane . 
i nostri risultati possono essere spiegati dalla migliore qualit delle immagini , ottenute con tomografo a 64 strati , rispetto ai lavori precedenti che hanno utilizzato apparecchi meno performanti ( tc a strato singolo o 4 strati )  . 
 [ 24 ] , un maggior numero di operatori si associa ad una maggiore variabilit delle misure ; nella nostra esperienza inoltre loperatore inesperto ha ricevuto un training di due settimane , a differenza delle sole 2 ore riportate dallautore di riferimento . il tempo necessario per il calcolo di un singolo volume stato in media di 8 minuti per loperatore esperto e di 11 minuti per laltro operatore . 
ai tempi indicati bisogna aggiungere quelli tecnici per il trasferimento dei datasets dal pacs ( picture archiving and communication system ) alla consolle dedicata , che deve essere disponibile in un ambiente adiacente alla sala tc . 
the time necessary to transfer the datasets from the picture archiving and communication system ( pacs ) to the dedicated workstation must be added to the reported time , while the workstastion must be available near the ct suite . 
 [ 23 ] , the low interobserver variability recorded in our experience allows us to omit computation of the previous volume , if already done , and thus to save time . 
nevertheless , the use of software capable of automatically calculating the volume is desirable to reduce the postprocessing time . volume assessment facilitates the detection of type v endoleak ( endotension ) in which the aneurysmal volume increases without any observable contrast leakage . 
in our experience , we observed only one case of volume increase without evident contrast leakage . volumetric analysis can be performed on nonenhanced ct examinations , which is different from the traditional algorithm that consists of a multiphasic contrastenhanced ct ( nonenhanced , arterial - phase and delayedphase acquisitions ) , with relevant radiation exposure for the patient [ 6 , 8 , 23 ]  . 
hence , this protocol reduces radiation exposure [ 25 , 26 ] and contrast - material administration in this class of patients , who present a higher prevalence of renal failure [ 27 , 28 ]  . 
in our experience , radiation dose reduction was estimated to be 23.5 msv per examination in an average - sized patient ( height 1.75 m , weight 85 kg )  . for the early follow - up ( 13 months after evar ) contrast - enhanced ct remains mandatory because volumetric changes may not be large enough to be detected . 
for the subsequent follow - up examinations , contrast - enhanced ct should be reserved for patients with a volume increase > 2% on the nonenhanced scan [ 23 ]  . 
further studies , with an extended population , are necessary to confirm our preliminary results . in conclusion , ct volumetric analysis is an accurate and reproducible modality for the follow - up of abdominal aortic aneurysms after evar . 
 [ 23 ] , la ridotta variabilit interosservatore , che risulta dallesperienza personale , rende superfluo il calcolo del volume precedente , se gi disponibile , portando ad un considerevole risparmio di tempo . 
 la misurazione volumetrica permette di identificare pi precocemente gli endoleak di tipo v ( endotension ) , in cui si assiste ad un progressivo incremento della sacca , senza segni di rifornimento visibili alle scansioni post - mdc . 
la misurazione seriata del volume dellaneurisma rappresenta il metodo pi sensibile per identificare questo tipo di endoleak , in quanto il diametro massimo non sempre varia in maniera significativa [ 22 , 23 ]  . 
nella serie personale , abbiamo osservato un solo caso di progressivo incremento volumetrico della sacca in assenza di rifornimenti evidenziabili allesame post contrastografico . lanalisi volumetrica della sacca aneurismatica pu essere effettuata con scansioni tc acquisite senza limpiego del mdc , a differenza del tradizionale protocollo che prevede unacquisizione plurifasica ( basale , arteriosa , venosa ) , gravato da una significativa esposizione radiante per il paziente [ 6 , 8 , 23 ]  . 
tale approccio consente non solo di ridurre la dose radiante [ 25 , 26 ] , ma anche di limitare limpiego del mdc in questa classe di pazienti che spesso presentano unalterata funzione renale [ 27 , 28 ]  . 
nella nostra esperienza , la riduzione di dose prevedibile in un paziente di corporatura media ( altezza 1 , 75 m , peso 85 kg ) di 23 , 5 msv per esame . al controllo precoce dopo evar ( 13 mesi ) , lo studio tc plurifasico rimane imprescindibile perch , nel breve tempo intercorso dallintervento , piccoli endoleak potrebbero produrre una variazione del volume non significativa ; ai controlli successivi , invece , lutilizzo del mdc non necessario in tutti i casi , ma andrebbe riservato a quei pazienti che presentano un incremento volumetrico della sacca superiore al 2% [ 23 ]  . 
 un vantaggio aggiunto di questo protocollo consiste nella significativa riduzione dei costi per il follow - up [ 5 ] , che nel nostro istituto sono stimabili in circa 160 euro per esame . 
ulteriori studi , con casistiche pi consistenti , sono necessari per confermare questi risultati . in conclusione , il calcolo seriato del volume alla tc un metodo riproducibile ed accurato di monitoraggio delle dimensioni degli aneurismi dellaorta addominale dopo trattamento endovascolare . 
al controllo precoce ( 13 mesi ) limpiego del mdc rimane indispensabile per identificare endoleak di modesta entit , che , nel breve periodo , induradiol med ( 2012 ) 117 : 7284 contrast - enhanced ct remains mandatory to identify small endoleaks that can cause undetected volume modifications in the short terfor later follow - up , volumetric analysis would eliminate the need for contrast material in asymptomatic patients with stable or decreasing aneurysm volume . 
nei pazienti asintomatici con volume stabile o ridotto ai controlli successivi al primo , la sola analisi volumetrica effettuata con scansioni tc basali pu essere sufficiente per monitorare levoluzione dellaneurisma senza ricorrere alle scansioni post - contrastografiche . 
magrini1 1radiotherapy department , brescia university , p.le spedali civili 1 , 25123 brescia , italy 2medical oncology department , spedali civili , brescia , italy correspondence to : m . 
the main purpose of this study was to analyse the impact of rpa in correlation with histology of the primary tumour in patients with brain metastases treated with hypofractionated radiotherapy . 
the majority of patients was treated with a total dose of 30 gy delivered in ten fractions , whereas the dose of 20 gy in four or five fractions was primarily used in patients classified as rpa class 3 . 
la maggior parte dei pazienti stata trattata con una dose totale di 30 gy erogati in 10 frazioni , la dose di 20 gy in 4 o 5 frazioni stata utilizzata per lo pi in pazienti classificati in classe rpa 3 . 
 keywords brain metastases primary histology hypofractionated radiotherapy recursive partitioning analysis conferma il ruolo del performance status generale , del numero di metastasi e della dose totale di radioterapia nel predire la os . 
 parole chiave metastasi cerebrali istologia primitiva radioterapia ipofrazionata recursive partitioning analysis introduction introduzione brain metastases represent the most common brain tumour in the adult population [ 1 ] , and their incidence is increasing worldwide [ 2 ]  . 
prognosis for patients with brain metastases is poor , with a median survival of 1 and 46 months in untreated and treated patients , respectively [ 3 , 4 ]  . 
recursive partitioning analysis ( rpa ) performed by the radiation therapy oncology group ( rtog ) identified based on a combination of factors including patient age , performance status and extension and control of the primary tumour several prognostic classes that differ substantially in terms of survival [ 5 , 6 ]  . 
the number of brain metastases is another factor closely correlated with survival and has also been included in the rpa classification systetherefore , a new prognostic classification system has been introduced : the graded prognostic assessment ( gpa ) [ 7 ]  . 
this assessment considers four risk classes that are very similar in terms of survival to those of le metastasi cerebrali sono la pi comune neoplasia dellencefalo nella popolazione adulta [ 1 ] e la loro incidenza va aumentando nel mondo [ 2 ]  . 
 il rischio di comparsa di metastasi cerebrali correlato per lo pi con listologia del tumore primitivo sia per la maggiore incidenza di alcune neoplasie , ad esempio mammella e polmone , che per la maggiore capacit biologica di dare metastasi , come nel caso del melanoma e della neoplasia renale . 
la prognosi di pazienti con metastasi cerebrale infausta , con una sopravvivenza mediana rispettivamente di 1 e 46 mesi in pazienti non trattati e trattati [ 3 , 4 ]  . 
la recursive partitioning analysis ( rpa ) eseguita dal radiation therapy oncology group ( rtog ) ha identificato , sulla base della combinazione di fattori quali let , il performance status , lestensione ed il controllo della malattia primitiva , alcune classi prognostiche decisamente diverse in termini di sopravvivenza [ 5 , 6 ]  . 
stata quindi creata una nuova classificazione prognostica : il graded prognostic assessment ( gpa ) [ 7 ] che considera 4 classi di rischio molto simili in termini di sopravvivenza a quelle radiol med ( 2012 ) 117 : 133147 the rpa , although with an additional class characterised by better survival for patients in rpa class 1 . 
many studies have validated the use of rpa within patient groups with similar tumour histology and have confirmed the importance of rpa classes in predicting survival , which is better for rpa class 1 patients and worse for rpa class 3 ones . 
histology of the primary tumour has been included in the gpa index to evaluate survival differences correlated with this parameter and test the possibility of incorporating this parameter in selecting the most appropriate treatment [ 8 , 9 ]  . 
 in this study , we analysed the prognostic value of combining the rpa classification with histology of the primary tumour for predicting survival in a group of patients with brain metastases who were treated consecutively with hypofractionated radiotherapy . 
we confirmed the role of the rpa classification in identifying patients with different prognoses and the impact of histology of the primary tumour and radiotherapy dose on survival , particularly in patients in rpa class 1 and 2 . 
the dose of radiotherapy proved to have prognostic significance in both classes . materials and methods population from january 1997 to december 2009 , 382 patients with brain metastases were consecutively treated at the radium institute of the department of oncologic radiotherapy of the university of brescia . 
 patient and disease characteristics patient , disease and treatment characteristics are reported della rpa , ma con una classe in pi caratterizzata da una sopravvivenza migliore dei pazienti in classe rpa 1 . 
 molti lavori hanno validato luso della rpa allinterno di gruppi di pazienti omogenei per istologia e hanno confermato limportanza delle classi rpa nel predire la sopravvivenza : migliore nei pazienti in classe rpa 1 e peggiore in quelli in classe rpa 3 . 
recentemente listologia della malattia primitiva stata inclusa nellindice prognostico gpa allo scopo di verificare le differenze in termini di sopravvivenza anche correlate a questo parametro e di sperimentare la possibilit di utilizzare anche questo parametro nella scelta del trattamento migliore [ 8 , 9 ]  . 
 in questo lavoro abbiamo quindi studiato il valore prognostico dellassociazione classificazione rpa / istologia della malattia primitiva nel predire la sopravvivenza di un gruppo di pazienti con metastasi cerebrali , trattati consecutivamente con radioterapia ipofrazionata . 
abbiamo confermato che la classificazione rpa importante nellidentificare pazienti con prognosi differente e che listologia del tumore primitivo e la dose della radioterapia influiscono sulla sopravvivenza soprattutto nei pazienti in classe prognostica rpa 12 . 
la dose della radioterapia risultata di rilevanza prognostica nei pazienti in classe prognostica rpa 1 e 2 . materiali e metodi popolazione da gennaio 1997 a dicembre 2009 , 382 pazienti con metastasi cerebrali sono stati consecutivamente trattati presso listituto del radio - dipartimento di radioterapia oncologica delluniversit di brescia . 
 le variabili cliniche considerate sono state let , il sesso , il performance status generale valutato secondo lindice di karnofski ( kps ) [ 10 ] , quello neurologico valutato secondo la scala del medical research council ( mrc ) [ 11 ] , la sede e listologia della malattia primitiva , il numero delle metastasi cerebrali e la presenza di malattia metastatica extracerebrale . a tutti i pazienti stata retrospettivamente attribuita la classe prognostica rpa utilizzando il kps ( maggiore o minore di 70 ) , lo stato della malattia primitiva ( controllata o non controllata ) , let dei pazienti ( > 65 o < 65 anni ) , lo stato di malattia metastatica extracranica ( presente o assente ) ed il numero di metastasi cerebrali . 
 table 1 disease characteristics tabella 1 caratteristiche della malattia radiol med ( 2012 ) 117 : 133147 percent percentuale 136 total age 65 years > 65 gender male female kps 90 < 90 70 < 70 nps ( mrc ) 0 1 2 3 rpa 1 2 3 primary lesion breast carcinoma lung carcinoma melanoma renal carcinoma other metastases in other sites yes no no . 
the most common primary tumours were lung cancer ( 217 patients , 57% ) , breast cancer ( 87 patients , 23% ) , melanoma ( 20 patients , 5% ) , renal cancer ( 14 patients , 4% ) , gastrointestinal cancer ( 19 patients , 5% ) , ovarian / uterine cancer ( eight patients , 2% ) , other histologic types ( eight patients , 2% ) , unknown histology ( nine patients , 2% )  . 
histological subtypes of lung cancer included adenocarcinoma ( 66% ) , microcytocaratteristiche dei pazienti e della malattia le caratteristiche dei pazienti , della malattia e dei trattamenti sono presentate nella tabella 1 . 
the number of brain metastases was higher than three in 43% of cases , 14% of patients were asymptomatic ; headache , nausea and vomiting and epilepsy were present either in isolation or combined in 111 patients ( 29% )  . 
kps score was 70 in 81% of patients , and the neurological performance status was 2 in 39% of theretrospective classification according to rpa classes was possible for all patients ( table 2 )  . 
il numero di metastasi cerebrali era maggiore di tre nel 43% dei casi , 14% dei pazienti era asintomatico ; cefalea , nausea e vomito , epilessia erano presenti da sole o in combinazione in 111 pazienti ( 29% )  . 
in questa serie , la maggior parte dei pazienti era classificabile nelle classi prognostiche peggiori ( rpa 2 e 3 )  . therapy terapia treatment consisted of either whole - brain radiotherapy ( wbrt ) alone or surgical resection followed by wholebrain radiotherapy ( sr - wbrt ) in 316 ( 83% ) and 63 ( 16% ) patients , respectively . 
treatment was well tolil trattamento ha previsto la radioterapia esclusiva su tutto lencefalo ( wbrt ) o , in alternativa , la radioterapia panencefalica post - chirurgica ( as - wbrt ) rispettivamente in 316 ( 83% ) e 63 ( 16% ) pazienti . 
le dosi di 30 gy in 10 frazioni e di 20 gy in 5 frazioni sono state quelle utilizzate nella maggior parte dei pazienti ( 53% e 44% rispettivamente )  . 
la maggior parte dei pazienti era gi in terapia con steroidi prima dellinizio della radioterapia ; comunque , durante la radioterapia , per il 22% dei pazienti stato necessario intensificare la terapia sintomatica . 
 statistical analysis analisi statistica the purpose of our study was to analyse the impact of the rpa prognostic classification on survival , even in relation to primary tumour histology in patients with brain metastases treated with hypofractionated radiotherapy . 
patients were considered lost to follow - up when no information was available within 2 months from the end of treatment and when the date of death was unknown . the second purpose of our study was to define other clinical or pathological variables having a potential impact on survival . 
to analyse the impact of the different variables within homogeneous patient groups , survival analysis was conducted within each rpa class , as well as in relation to primary disease histology . 
all statistical analyses were performed using the spss software , version 17 [ 12 ]  . lobiettivo dello studio era analizzare limpatto della classificazione prognostica rpa sulla sopravvivenza anche in relazione con listologia della neoplasia primitiva in pazienti con metastasi cerebrali trattati con radioterapia ipofrazionata . 
i pazienti sono stati considerati persi al follow - up se non cerano pi notizie entro due mesi dalla fine del trattamento e non era possibile sapere la data della morte . il secondo obiettivo dellanalisi stata la definizione di altre variabili cliniche o patologiche con possibile impatto sulla sopravvivenza . 
per analizzare limportanza delle diverse variabili anche allinterno di gruppi omogenei di pazienti , lanalisi della sopravvivenza stata condotta allinterno di ogni classe rpa anche in relazione con listologia della malattia primitiva . 
 results analysis of prognostic factors univariate analysis risultati analisi dei fattori prognostici analisi univariata after a median follow - up of 151 ( 12 , 089 ) days , the actuarial os for the entire series was 26% , 10% and 1% at 0.5 , 1 and 2 years , respectively . 
 the actuarial median survival calculated for the entire series was 379 , 146 and 74 days for patients with kps 90 , 7090 , and < 70 , respectively ( p = 0.0000 ) ; and 189 , 93 and dopo un follow - up mediano di 151 giorni ( 12089 giorni ) la sopravvivenza globale attuariale dellintera serie stata pari al 26% , 10% e 1% rispettivamente a 0 , 5 , 1 e 2 anni . 
 allanalisi univariata ( tabella 3 ) confermato il ruolo predittivo della classificazione rpa ( tabella 2 ) con sopravvivenze mediane pari a 283 , 149 e 67 giorni rispettivamente per pazienti in classe rpa 1 , 2 e 3 ( p < 0 , 000 )  . 
un ridotto numero di metastasi cerebrali ( < 3 ) e lassenza di altre metastasi a distanza ha un impatto statisticamente favorevole sulla sopravvivenza mediana ( p = 0 , 001 )  . per quel che riguarda listologia , ladenocarcinoma della mammella e del polmone hanno una sopravvivenza mediana migliore rispetto agli altri tipi istologici ( p = 0 , 042 )  . 
as for patients in rpa class 2 , overall and favorevolmente sulla sopravvivenza globale ( p = 0 , 000 )  . poich le classi prognostiche rpa sono una delle variabili pi importanti nel predire la sopravvivenza e allo scopo di verificare se in un gruppo omogeneo di pazienti la prognosi era condizionata dagli stessi fattori importanti nel gruppo intero , lanalisi uni variata stata eseguita anche allinterno di ogni classe rpa per tutte le variabili cliniche e terapeutiche ( tabella 4 )  . 
il performance status generale e neurologico , il numero delle metastasi cerebrali , la presenza di altre metastasi a distanza , listologia , la dose totale ( 20 o 30 gy ) e , marginalmente , la modalit di trattamento ( radioterapia post chirurgica o esclusiva , p = 0 , 006 , sopravvivenza mediana 453 giorni vs 237 ) mantengono il loro impatto sulla os per pazienti classificati in classe rpa 1 . 
none of the variables considered , except for age , had any role in modifying survival in patients in rpa class 3 ( table 4 )  . multivariate analysis multivariate analysis ( table 5 ) was performed on the entire series , taking into consideration all variables found to be statistically significant at univariate analysis . 
the analysis was repeated for each of the rpa classes , again taking into consideration only the variables that were found to be statistically significant at univariate analysis , namely : overall performance status , presence of other distant metastases , number of brain metastases , histology , treatment with or without i pazienti in classe prognostica rpa 2 il performance status generale e neurologico , la dose di radioterapia , listologia e il numero di metastasi cerebrali sono le variabili ancora significativamente correlate alla prognosi anche se in modo meno evidente che nella classe rpa 1 . 
nessuna delle variabili considerate , tranne let , ha mostrato un ruolo nel modificare la sopravvivenza nei pazienti in classe rpa 3 ( tabella 4 )  . analisi multivariata lanalisi multivariata ( tabella 5 ) stata eseguita sullintera serie considerando tutte le variabili statisticamente significative allanalisi uni variata . 
 trattamento con o senza chirurgia e la dose di radioterapia per la classe rpa 1 ; il kps , il numero di metastasi e la dose di radioterapia per la classe rpa 2 . 
lower doses ( 10 gy in a single fraction , 12 gy in two fractions or 20 gy in five fractions ) were correlated with worse disease - free ( dfs ) and os compared with the standard , even though the difference was not statistically significant [ 1214 ] ; two studies directly compared 30 gy in ten fractions and 20 gy in five fractions and found no particular advantage for the higher doses [ 12 , 15 , 16 ]  . 
higher doses ( 50 gy in 20 fractions , 54.4 gy in 34 fractions twice daily ) provided no clear advantage compared with standard treatment , even when parameters such as quality of life were considered [ 12 , 18 , 19 ]  . 
dosi minori ( 10 gy in frazione singola , 12 gy in due frazioni o 20 gy in 5 frazioni ) sono state correlate con sopravvivenza libera da malattia e sopravvivenza globale peggiori rispetto allo standard anche non statisticamente significativa [ 1214 ] ; due studi hanno confrontato direttamente i 30 gy in 10 frazioni e i 20 gy in 5 frazioni non evidenziando particolare vantaggio per le dosi pi alte [ 12 , 15 , 16 ]  . 
dosi maggiori ( 50 gy in 20 frazioni , 54 , 4 gy in 34 frazioni bigiornaliere ) non hanno evidenziato un chiaro vantaggio rispetto al trattamento standard , anche considerando parametri di qualit della vita [ 12 , 18 , 19 ]  . 
i 174 pazienti rimanenti sono stati trattati con un frazionamento pi breve ( 20 gy in 5 o 4 frazioni ) , con una sopravvivenza nettamente peggiore allanalisi table 6 median survival ( days ) for each histological type within each recursive partitioning analysis ( rpa ) class radiol med ( 2012 ) 117 : 133147 p - value breast lung ( adeno ) lung ( sclc ) lung ( squam ) renal carcinoma melanoma other histologies 144 mammella polmone ( adenocarcinoma ) polmone ( sclc ) polmone ( squamoso ) carcinoma renale melanoma altre istologie sclc , carcinoma del polmone a piccole cellule rpa 1 0.05 422 289 268 164 112 269 rpa 1 0 , 05 422 289 268 164 112 269 rpa 2 0.003 170 160 119 820 127 rpa 2 0 , 003 170 160 119 820 127 rpa 3 rpa 3 adeno , adenocarcinoma ; sclc , small cell lung carcinoma ; squam , squamous carcinoma tabella 6 sopravvivenza mediana di ogni singola istologia allinterno di ogni classe recursive partitioning analysis ( rpa ) ( giorni ) a shorter fractionation ( 20 gy in five or four fractions ) had a markedly worse survival at univariate and multivariate analysis . 
 more recently , in selected cases , wbrt alone is not considered the exclusive treatment for single or fewer than three metastases and is frequently combined with surgery or stereotactic radiotherapy . 
wbrt combined with stereotactic boost showed the best results in terms of control of brain metastases compared with wbrt or stereotactic radiotherapy exclusively in patients with fewer than three metastases [ 25 , 26 ]  . 
for this reason , 63 patients ( 16% ) , most treated during the most recent period , underwent surgery and radiotherapy , whereas only five patients underwent wbrt and stereotactic boost . 
histology of the primary tumour has never been formally analysed as a prognostic factor capable of predicting survival in patients with brain metastases and it was not included in the rpa classification systeonly recently has histology been added to the gpa prognostic scoring system , attesting to the fact that the prognostic inunie multivariata . 
 in anni pi recenti ed in casi selezionati , wbrt non considerato il trattamento esclusivo per metastasi singola o per meno di tre metastasi ed frequentemente associato alla chirurgia o alla radioterapia stereotassica . 
la wbrt adiuvante ha peraltro dimostrato in numerosi studi di migliorare il controllo locale di metastasi cerebrali operate e di ridurre la frequenza di morte legata a cause neurologiche [ 2124 ]  . 
wbrt associata a sovradosaggio con stereotassi ha evidenziato migliori risultati in termini di controllo cerebrale di malattia rispetto alla wbrt esclusiva o rispetto a radioterapia stereotassica esclusiva in pazienti con meno di tre metastasi [ 25 , 26 ]  . la nostra serie stata reclutata in un lungo intervallo di tempo e in un ospedale con una tradizione neuro - chirurgica molto forte . 
per tale ragione nella nostra serie 63 pazienti ( 16% ) , per lo pi trattati nellultimo periodo di tempo , sono stati sottoposti a chirurgia e radioterapia e solo 5 pazienti sono stati trattati con wbrt e boost stereotassico . 
listologia della neoplasia primitiva non stata mai formalmente analizzata come un fattore prognostico capace di predire la sopravvivenza di pazienti con metastasi cerebrali di diversa origine e non inclusa nel sistema di classificazione rpa . 
performed a recursive partitioning analysis on 1 , 960 patients treated for brain metastases and identified three different prognostic classes : rpa classes 1 , 2 and 3 [ 5 , 6 ]  . 
as the rpa classification proved to be the most important factor in predicting survival , univariate analysis was repeated for each class , that is , in a more homogeneous subgroup of patients . 
in patients classified as rpa 1 , almost all variables ( performance status , presence of other metastases , number of brain metastases , type of treatment and dose of radiotherapy ) proved to be statistically correlated with survival ; in rpa class 2 , kps , number of brain metastases and dose of radiotherapy proved to influence survival ( tables 4 and 5 )  . 
indeed , only one study in the literature has identified in rpa class 3 patients a subgroup showing a better prognosis and for whom treatment could result in better survival rates [ 31 ]  . 
 patients with breast or lung adenocarcinoma have the best prognosis , even when compared with patients of the same rpa class , although the difference is more evident among rpa class 2 patients . 
with the limits of a retrospective analysis , the combination of surgery and radiotherapy does not appear to have an impact on survival in patients in rpa class 1 . these data confirm the importance of patient selection for the palliative treatment of brain metastases . 
the overall performance status is of fundamental importance for deterin questa serie confermato che ladenocarcinoma della mammella , del polmone e il microcitoma polmonare portano ad una sopravvivenza migliore degli altri tipi istologici ( p = 0 , 042 )  . nel 1997 e nel 2000 gaspar et al . 
molti autori , negli ultimi anni , hanno verificato e confermato leffetto in termini di sopravvivenza dei differenti protocolli di trattamento nelle diverse classi prognostiche [ 25 ] , anche considerando casi di pazienti con unica origine istologica [ 27 30 ] e di pazienti sottoposti a chirurgia [ 30 , 31 ]  . nella nostra analisi , la differente prognosi per i pazienti nelle diverse classi rpa fortemente confermata allanalisi univariata ( p = 0 , 0001 )  . 
poich la classificazione rpa ha dimostrato di essere il pi importante fattore nel determinare la sopravvivenza , lanalisi univariata stata ripetuta allinterno di ogni singola classe rpa e cio in un pi omogeneo sottogruppo di pazienti . 
per i pazienti nella classe rpa 1 quasi tutte le variabili ( performance status , la presenza di altre metastasi , il numero di metatasi cerebrali , il tipo di trattamento e la dose di radioterapia ) sono risultate statisticamente correlate con la sopravvivenza ; nella classe rpa 2 , il kps , il numero di metastasi cerebrali e la dose di radioterapia influiscono sulla sopravvivenza ( tabelle 4 e 5 )  . 
infatti vi in letteratura solo un lavoro che ha identificato allinterno della classe rpa 3 un sottogruppo di pazienti con una prognosi migliore e per i quali un trattamento potrebbe comunque dare un vantaggio in termini di sopravvivenza [ 31 ]  . 
 tra questi pazienti , quelli con adenocarcinoma della mammella e del polmone hanno una prognosi pi favorevole , anche allinterno di ogni classe , anche se la differenza pi evidente allinterno della classe rpa 2 . 
pertanto , come suggerito dal senso comune medico , anche se listologia della neoplasia primitiva non attualmente inclusa in alcun indice prognostico , questo fattore deve essere considerato durante il processo decisionale . 
con i limiti dellanalisi retrospettiva , lassociazione della chirurgia alla radioterapia non sembra comunque avere un impatto sulla sopravvivenza anche in pazienti in classe rpa 1 . questi dati confermano limportanza della selezione dei pazienti da candidare ad un trattamento palliativo per metastasi cerebrali . 
in fact , patient selection proved to be more important in influencing survival prediction compared that did surgery , even though selected patients in rpa class 1 may benefit from wbrt combined with surgery and stereotactic boost and achieve prolonged disease control with aggressive multimodal treatment , in particular , those affected by specific primary tumour types . 
in rpa class 3 patients , a more aggressive treatment ( surgery or stereotactic radiotherapy with or without wbrt ) should be avoided , as quality of life could worsen with little benefit in terms of survival . 
di fatto la selezione dei pazienti risultata essere pi importante nel condizionare la sopravvivenza rispetto alla chirurgia , ma pazienti selezionati in classe prognostica rpa 1 possono trarre beneficio da wbrt associata a chirurgia e boost stereotassico , e possono ottenere un lungo controllo di malattia grazie a trattamenti aggressivi multimodali , specialmente se con determinate istologie primitive . 
in pazienti classificati in classe rpa 3 , trattamenti pi aggressivi ( chirurgia o radioterapia stereotassica con o senza wbrt ) dovrebbero essere evitati perch potrebbero peggiorare la qualit della vita con scarsi benefici in termini di sopravvivenza . 
 una pagina di storia della radiologia published online : 18 january 2012 springer - verlag 2012 pagando anche lo scotto di personali disagi e patimenti . grande diagnosta , al quale si ricorreva per i casi pi difficili e complessi , veniva reputato la cassazione che dirimeva ogni quesito clinico - radiologico . 
la grutta fu per lunghi anni primario allospedale civico e docente in molte scuole di specializzazione , forgiando un grande numero di valorosi allievi , che oggi ricoprono posizioni di rilievo in molti ospedali della nostra isola . 
ebbe sempre la passione per i giovani ai quali dispensava con generosit pur mostrandosi talora burbero e severo per necessit il suo patrimonio di esperienze , saperi , prassi e costumi civili . miro era , inoltre , un eccellente organizzatore . 
socio emerito della nostra societ scientifica . tali erano in lui dottrina , saggezza e capacit organizzativa che terminato il suo servizio lo chiamai per lungo tempo come consulente , senza compenso alcuno , nella fase di rinascita della radiologia del policlinico , nella mia qualit allora di direttore dellistituto universitario . 
era anche un modo , per me forse egoistico , di averlo accanto e continuare a vivere latmosfera della scuola di cignolini , facendo tesoro della sua conoscenza pratica , dei suoi preziosi pareri , della sua umanit . 
patriarca saggio e buon consigliere . come onde che rotolano sulla spiaggia , cos i pensieri cominciano a svolgersi nella mia mente e le ombre della giovent si uniscono con quelle pi recenti , suscitando nostalgia e malinconia . quando muore un marito , padre , familiare , amico , si soffre la morte altrui come unassenza importante . 
la grutta cala , a palermo , il sipario e si smorzano le luci sulla prima scena della grande rappresentazione storica della scienza delle immagini biomediche nella capitale della sicilia . dopo i pionieri della disciplina nella nostra citt gaetano cottone , valentino colombo , gioacchino scaduto , gioacchino arnone il primo insegnamento universitario della materia era stato assegnato al prof . 
la grutta miro , per gli amici inizi la sua carriera accademica divenendo aiuto di epifanio e , suc cessivamente , ricopr la funzione di direttore incaricato dellistituto di radiologia di palermo . con la chiamata , da parte della facolt medica , del grande pietro cignolini scienziato insigne e famoso , maestro diretto e indiretto di tutti i radiologi della sicilia il prof . 
la grutta fu , per lunghi anni , suo discepolo , aiuto e principale collaboratore . in un momento amaro per cignolini , a causa di ingratitudini accademiche , la lealt del prof . 
la grutta verso il suo capo - scuola non venne meno e gli rimase fedele e devoto , radiol med ( 2012 ) 117 : 160161 una parte di noi . 
rimane la memoria , che tiene in vita per chi rimane la persona con la quale abbiamo percorso un lungo tratto di strada , abbiamo sperato , operato , discusso . stata la prima persona che mi accolse e guid quando feci ingresso nel 1964 , da studente laureando , nella radiologia del policlinico universitario allora allocata in un corridoio della clinica medica , parlandomi di mio padre medico e suo buon amico . 
da un ventennio , circa , lo consideravo un fratello maggiore , sempre ben disposto al sostegno , prodigo di suggerimenti e aiuto , soprattutto nei momenti di avversit della mia vicenda scientifico - accademica . 
mi piace ripetere le parole del cardinale carlo maria martini , nel libro le et della vita : onorare lanziano significa anche e soprattutto riconoscere in lui unautorevolezza che si fonda su valori autentici , che il vecchio reca dentro di s.. 
come per casimiro la grutta . la grutta fu credente , con famigliari cattolici convinti e operanti nelle comunit ecclesiali . aveva un senso religioso della famiglia , che amava sinceramente : la moglie maria concetta , le figlie simonetta e luciana , ladorata nipotina . 
insieme abbiamo promosso lintitolazione al nostro comune mentore pietro cignolini , del quale rimango unico allievo e sono lieto che lapprovazione delle autorit comunali si sia conclusa prima della sua morte . 
 alla famiglia voglio dedicare i versi del poeta : ricordami quando me ne sar andato lontano / nella terra del silenzio ; / quando non potrai pi tenermi per mano / e a me non sar pi concesso tornare indietro da te . 
tamburrini , e - mail : tamburrini@unicz.it received : 21 december 2010 / accepted : 28 december 2010 / published online : 21 october 2011 springer - verlag 2011 abstract we review the current approach to using gadoliniumbased contrast agents taking into account data published in the literature and us food and drug administration and european medicines evaluation agency ( emea ) guidelines . riassunto scopo del nostro lavoro stato rivisitare , sulla base dei dati della letteratura e delle comunicazioni della food and drug administration ( fda ) e della european medicines agency ( emea ) , la posizione nei riguardi dellimpiego degli agenti di contrasto a base di gadolinio . keywords nephrogenic systemic fibrosis magnetic resonance contrast agent gadolinium parole chiave fibrosi sistemica nefrogenica risonanza magnetica con agenti di contrasto agenti di contrasto a base di gadolinio introduction introduzione in 2008 , we published an editorial that focused attention on nephrogenic systemic fibrosis ( nsf ) , emphasising how gadolinium - based contrast agents are believed to play a crucial role in the aetiopathogenesis of this condition in patients with advanced - stage kidney disease ( stage 4 or 5 ) or undergoing renal replacement therapy ( rrt ) [ 1 ]  . 
it is also clear that in recent years , and this is supported by data in the literature , there has been a sea change not only in the use of these contrast agents ( type , dose , etc . ) , but also in the evaluation in terms of clinical examination , laboratory tests and history of patients who are candidates for this procedure . 
 nel 2008 abbiamo pubblicato un editoriale che poneva lattenzione su unentit morbosa , la nephrogenic systemic fibrosis ( nsf ) nella cui eziopatogenesi un ruolo fondamentale si ritiene sia da attribuirsi agli agenti di contrasto a base di gadolinio ( gd ) nei soggetti affetti da insufficienza renale di grado avanzato ( stadio 4 e 5 ) o in trattamento dialitico sostitutivo [ 1 ]  . 
peraltro altrettanto evidente che , negli ultimi anni , si assistito ad un profondo cambiamento , anche sulla base dei dati della letteratura , non solo nellimpiego di questi agenti di contrasto ( tipo , dose , ecc . ) , ma anche nellinquadramento clinico - laboratoristico ed anamnestico dei pazienti candidati a questa procedura . 
today , however , a series of strategies has been adopted aimed at significantly reducing the risk , such as : ( 1 ) measuring creatininaemia and glomerular filtration rate ( gfr ) in patients suspected of having compromised kidney function ( patients > 60 years of age , with high blood pressure or with diabetes ) ; ( 2 ) reducing gadolinium dose to the minimum necessary , as there is a close correlation between dose and nsf onset [ 3 ] ; ( 3 ) avoiding repeated administrations , with an interval of at least 1 week between two magnetic resonance ( mr ) examinations with gadolinium - based contrast agents in at - risk patients , except in cases of absolute clinical urgency , which is to be assessed on a case - by - case basis ; even greater attention has been paid to patients with acute kidney injury ( aki ) , in whom the risk ( measured retrospectively ) of nsf increases with increasing creatininaemia ; ( 4 ) selecting a contrast agent considered to be safer , a rather sensitive given its implications of a commercial nature ; indeed , gadolinium - based contrast agents have different physical and chemical properties according to their structure . 
 as the excretion of the contrast agent from the body occurs via the kidneys , it follows that the probability of gd3 + ions being disassociated from the base molecule is significantly higher in patients affected by chronic kidney disease ( ckd ) having glomerular filtration rate ( gfr ) < 30 ml / min / 1.73 m2 , with the possibility of tissue toxicity . 
ma , oggi , sono state adottate strategie volte a ridurre significativamente il rischio come ( 1 ) determinazione della creatininemia e del glomerular filtration rate ( gfr ) nei soggetti con sospetta compromissione della funzione renale ( ultrasessantenni , ipertesi , diabetici ) ; ( 2 ) riduzione , al minimo necessario , della dose di gadolinio , poich esiste in effetti una stretta correlazione anche tra la dose e linsorgenza di nsf [ 3 ] ; ( 3 ) evitare le somministrazioni ripetute , con un intervallo temporale di almeno una settimana tra due esami di risonanza magnetica ( rm ) con agenti di contrasto a base di gd nei pazienti a rischio , fatto salvo il caso di assoluta esigenza clinica , da valutare caso per caso . 
ancora maggiore attenzione stata rivolta ai pazienti con danno renale acuto ( aki ) nei quali il rischio ( misurato retrospettivamente ) di nsf aumenta con lincremento dei valori di creatininemia ; ( 4 ) scelta dellagente di contrasto considerato pi sicuro : argomento questo a dire poco delicato per le implicazioni anche di carattere commerciale ; difatti gli agenti di contrasto a base di gd hanno differenti propriet fisico - chimiche in base alla loro struttura . 
e poich lescrezione del mezzo di contrasto ( mdc ) dallorganismo avviene attraverso lemuntorio renale , ne consegue logicamente che nei soggetti affetti da insufficienza renale cronica ( irc ) con gfr < 30 ml / min / 1 , 73 m2 , viene incrementata significativamente la probabilit che ioni gd3 + possano dissociarsi dalla molecola di base , espletando lazione tossica a livello tissutale . 
in addition , both the linear and the macrocyclic contrast agents stimulate in vivo proliferation of human fibroblasts , even though the latter do so at much higher concentrations [ 6 ] , thus focusing attention on the risk of high doses per se . 
lastly , in a retrospective analysis encompassing 19992009 and involving 2 , 053 patients with stages 35 ckd [ 7 ] , no cases of nsf were reported during 29 months of follow - up , even after repeated administrations in some patients . 
even more surprisingly , as many as six gadolinium - based compounds were used . the european medicine evaluation agency ( emea - europa.eu ) has classified gadolinium - based contrast agents into three categories : high risk ( gadoversetamide , gadodiamide , gadopentetic acid ) , medium risk ( gadofosveset , gadobenic acid , gadoxetic acid ) and low risk ( gadoteric acid , gadoteridol , gadobutrol ) based on the premise that the likelihood of developing nsf ( also ) depends on the type of contrast agent used and its physical and chemical properties . 
the emea , therefore , has issued recommendations with the aim of minimising the risk of nsf , also emphasising that the relationship between contrast agents and nsf is reported to be dose related , but not only dose related . 
emea also developed guidelines for the use of these products , establishing contraindications in some categories of patients at high risk and precautions for those at medium or low risk . 
in essence , whereas assessing kidney function with laboratory workup is required for the first group , this is not considered mandatory for the others , though in our opinion it is prudent . decrease in the number of examinations performed kim et al . 
 [ 5 ] riportavano la scomparsa di nsf dopo passaggio dalla gadodiamide ( chelato lineare non ionico ) al gadobenato dimeglumina ( chelato lineare ionico ) e al gadopentato dimeglumina ( chelato lineare ionico )  . 
peraltro sia i mdc lineari che quelli macrociclici stimolano la proliferazione in vitro dei fibroblasti umani anche se i secondi a concentrazioni molto pi elevate [ 6 ] , focalizzando lattenzione sul rischio rappresentato dalle alti dosi di per s . 
infine in unanalisi retrospettiva effettuata tra il 1999 e il 2009 su 2053 pazienti con irc [ 7 ] stadi 35 , non venivano riportati casi di nfs durante un follow - up di 29 mesi , anche dopo somministrazioni ripetute in alcuni pazienti . 
ancora pi sorprendentemente , ben sei erano i composti a base di gadolinio adoperati ! leuropean medicines agency ( emea ) ha classificato gli agenti di contrasto a base di gd in tre categorie : ad alto ( gadoversetamide , gadodiamide , acido gadopentetico ) , medio ( gadofosveset , acido gadobenico , acido gadoxetico ) e basso ( acido gadoterico , gadoteridolo , gadobutrolo ) rischio , sulla base della considerazione che la eventualit di sviluppare lnsf dipende ( anche ) dal tipo di mdc usato e dalle sue caratteristiche fisico - chimiche . 
la stessa emea ha formulato linee guida per luso di questi prodotti ponendo controindicazioni in alcune categorie di pazienti per quelli ad alto rischio ed alcune precauzioni per quelli a medio e a basso rischio . 
in concreto , per i primi richiesta la valutazione della funzionalit renale mediante esami di laboratorio , per gli altri la medesima considerata non obbligatoria , ma , a nostro parere , sarebbe comunque prudente effettuarla . radiol med ( 2012 ) 117 : 15 ( with and without contrast administration ) performed between july 2005 and september 2008 reported in the us veteran affairs database for a total of more than one million examinations , 38% of which performed with gadoliniu since spring 2007 , there has been a progressive reduction in the number of mr examinations performed with contrast agent . 
this policy is nonetheless blatantly contradicted by the sharp decrease ( 49% ) in mr examinations with gadolinium even in patients with gfr 3045 ml / min / 1.73 m2 and even ( 24% ) in those with gfr 4560 ml / min / 1.73 m2 , with a shift towards contrast - enhanced computed tomography ( ct ) [ 9 , 10 ]  . 
on the other hand , the constant development of technology that today makes possible vascular studies without the use of contrast agents should also be borne in mind [ 11 ]  . diminuzione del numero di esami praticati kim et al . 
 [ 8 ] hanno preso in considerazione il numero di rm ( con e senza mdc ) eseguite da luglio 2005 a settembre 2008 presenti nel database del veterans affairs usa per un totale di oltre un milione di esami di cui il 38% con gadolinio . 
parimenti si assisteva ad un marcato incremento di esami preceduti dalla determinazione della creatininemia : questa politica trovava per una palese contraddizione nella forte diminuzione ( - 49% ) di rm con gadolinio anche nei soggetti con gfr 3045 ml / min / 1 , 73 m2 e addirittura anche ( - 24% ) in quelli con gfr 4560 ml / min / 1 , 73 m2 , con uno shift verso la tomografia computerizzata ( tc ) con mdc [ 9 , 10 ]  . 
allow an appropriate time interval between one procedure with gadolinium and the next . in conclusion , the excessively loud alarm bells that sounded in 20062007 have diminished in volume following preventative measures adopted universally , thanks to periodic reports and recommendations issued by the regulatory authorities ; however , these alarms have not been completely silenced . 
their use , however , requires a thorough patient history and clinical assessment to avoid inappropriate use ( dose ) , and the choice should be tailored to the individual patient , with preference given to the more stable contrast products . 
fare trascorrere un idoneo intervallo temporale tra una procedura con gadolinio ed unaltra . in conclusione , leccessivo allarmismo degli anni 2006 2007 pu ritenersi in concreto rientrato , in conseguenza delle misure preventive ormai universalmente applicate grazie anche alle periodiche segnalazioni e raccomandazioni delle autorit regolatorie , ma non del tutto cessato . 
quindi , non bisogna lasciarsi andare a nessun terrorismo contrastografico , poich nella medicina moderna image guided non possibile rinunciare allimpiego dei mezzi di contrasto : il loro impiego necessit di unaccurata valutazione clinicoanamnestica , evitando quindi luso inappropriato dellagente di contrasto ( dose ! ) , che deve essere il pi indicato per il singolo paziente , dando la preferenza ai prodotti pi stabili . 
oresta1 1struttura complessa di radiologia , azienda ospedaliera pediatrica santobono - pausilipon , via mario fiore 6 , 80129 napoli , italy 2das diagnostica per immagini e radioterapia , universit federico ii , napoli , italy 3studio legale associato mercogliano&celestino , rossano ( cs ) , italy 4u.o. 
as there are still no guidelines available in italy for the off - label use of medications , we aim to define the duties , obligations and liability of ultrasound radiologists according to the laws in force . keywords ultrasound ultrasound contrast media off label children riassunto lutilizzo del mezzo di contrasto ecografico a tuttoggi non risulta ancora validato in et pediatrica . 
poich in italia per limpiego dei farmaci off - label non sono ancora disponibili linee guida specifiche , si cerca di definire , secondo la normativa vigente , gli adempimenti , gli obblighi e le responsabilit del medico ecografista . parole chiave ecografia mezzo di contrasto ecografico off - label pediatria introduction introduzione despite the widespread use and proven efficacy of ultrasound ( us ) contrast media in the adult population , contrastenhanced us ( ceus ) to date has not achieved the same level of diffusion in the paediatric population . 
we therefore refer to the body of legislation that regulates off - label use of medications , with particular emphasis on the possible liability of the us nonostante il diffuso impiego e la comprovata efficacia del mezzo di contrasto ( mdc ) in ecografia nella popolazione adulta , ad oggi , non si verificata la medesima diffusione in quella pediatrica . 
analizzeremo , pertanto , le cause etiche , economiche e legali che determinano la mancata autorizzazione allutilizzo del mezzo di contrasto ecografico in ambito pediatrico , se non al limite di un impiego di tipo off - label , ovvero , in maniera non conforme a quanto previsto dalle caratteristiche del prodotto . 
media are composed of microbubbles of gas , such as sulphur hexafluoride , perfluorohexane , perfluorocarbon , air or nitrogen , which are contained in a shell consisting of stabilising substances such as phospholipids , albumin or galactose [ 1 , 2 ]  . 
 us contrast media can be classified into two types first generation and second generation based on the characteristics of the interaction between microbubbles and the us beam ( table 1 )  . 
this is because they are able to overcome the difficulties due to the limited time first - generation media remain in the bloodstreathe revolution heralded by sonovue in the field of ceus has made it the driving force behind the success of this technique , especially in europe , for evaluating liver disease , the area in which the most important clinical studies have been performed . 
the pioneering use of farmaci in regime di off - label sottolineando in particolare , le possibili responsabilit che il medico ecografista assume praticando lecografia con mezzo di contrasto ( ceus ) al di fuori della indicazione certificata . 
 i mezzi di contrasto ecografici : stato dellarte i mezzi di contrasto ecografici , introdotti per via endovenosa , consentono di incrementare i dettagli delle strutture anatomiche in cui essi si distribuiscono migliorandone la riflettivit . 
sono costituiti da microbolle di gas , quali ad esempio esafluoruro di zolfo , perfluoroesano , perfluorocarburi , aria , azoto , contenute in un opportuno rivestimento formato da sostanze stabilizzanti quali fosfolipidi , albumina , galattosio [ 1 , 2 ]  . 
in base alle caratteristiche di interazione tra le microbolle ed il fascio ultrasonoro , i mezzi di contrasto si distinguono in mezzi di i e di ii generazione ( tabella 1 )  . 
 oggi , in particolare , si fa consueto ricorso a mezzi di contrasto di ii generazione di cui il sonovue rappresenta certamente il capostipite , in quanto supera le difficolt riscontrate dal tempo di permanenza ridotto nel circolo ematico dei mezzi di contrasto di i generazione . 
la rivoluzione che il sonovue ha portato nel settore dellecografia con mezzo di contrasto , ne ha fatto il principale artefice del successo che questa tecnica ha avuto , principalmente in europa , per la valutazione clinica delle malattie epatiche , ambito in cui si sono svolte le principali sperimentazioni cliniche . 
 in addition , the effectiveness and safety of contrast media use in patients < 18 years have not been evaluated , so their use in these patients is not advisable [ 6 ]  . 
these include the lower incidence of focal lesions , particularly hepatic lesions [ 7 ] in children , and technical reasons : indeed , by using higher frequency transducers , improved sensitivity to vascular flow can be achieved [ 8 , 9 ]  . 
currently , the rare reports in the literature concerning such use in chilzo dellecocontrastografia sono riassunte nella tabella 2 . il possibile campo di utilizzo della ceus pu andare ben oltre lo studio delle patologie degli organi parenchimatosi , diffondendosi ad oggi anche lutilizzo pionieristico dellecocontrastografia in ambiti clinici molto impegnativi , quali lo studio delle patologie dei grossi vasi nonch lo studio delle malattie infiammatorie gastroenteriche [ 4 ]  . applicazioni storiche , di frontiera e futuribili del mezzo di contrasto ecografico in pediatria allo stato , i mdc in ecografia , vengono impiegati di routine nelladulto , soprattutto nello studio delle lesioni focali a carico degli organi parenchimatosi . 
 inoltre , lefficacia e la sicurezza delluso di tali mdc in soggetti di et inferiore ai 18 anni non sono state valutate e di conseguenza , in questi pazienti , se ne sconsiglia luso [ 6 ]  . 
limpiego del mezzo di contrasto ecografico a tuttoggi , non risulta validato in et pediatrica probabilmente per diversi motivi fra cui la minore incidenza di lesioni focali , soprattutto epatiche [ 7 ] , nonch per motivazioni tecniche : utilizzando , infatti , sonde a pi alta frequenza , possibile una migliore sensibilit ai flussi vascolari [ 8 , 9 ]  . 
in ambito pediatrico la sperimentazione dei farmaci sempre stata limitata , per due ordini di motivi : economici : disinteresse da parte delle aziende ad investire nella popolazione pediatrica , relativamente sana , con studi specifici di efficacia , sicurezza e tossicit ; etici : difficolt che si incontrano nel sottoporre bambini al rischio insito della sperimentazione . 
 la tendenza ad escludere la popolazione infantile da studi di fase i , con conseguente rallentamento delliter , la presenza di una normativa pi rigida , limpiego di una popolazione pi piccola , la difficolt di reclutamento dei soggetti e nellottenere campioni biologici in quantit adeguata , la possibilit di alcuni eventi che potrebbero verificarsi solo a distanza di tempo e rimanere , pertanto , ignorati se non si approntano studi a lungo termine , rappresentano tutti ulteriori problemi che si incontrano negli studi farmacologici in ambito pediatrico [ 11 ]  . i problemi che risultano , dunque , dalla mancanza di farmaci impiegabili per luso pediatrico includono [ 11 ] : rischi pi elevati di reazioni avverse , tra cui il decesso , a causa di informazioni inadeguate sul dosaggio ; cure inefficaci per sottodosaggio ; non disponibilit per la popolazione pediatrica dei progressi terapeutici e di adeguati preparati e modalit di somministrazione ; radiol med ( 2012 ) 117 : 148159 dren indicate only sporadic and experimental use . impiego nella popolazione pediatrica di preparati magiexperimentation with medications in children has always strali o officinali potenzialmente di scarsa qualit . been limited , for two main reasons : economic : lack of interest on the part of companies to invest in the paediatric population , which is relatively healthy , with specific studies on efficacy , safety and toxicity ; ethical : difficulties encountered in subjecting children to the risks involved in experimentation . 
 further problems encountered in drug trials in paediatric populations include : the tendency to exclude children from phase i trials , with a consequent slowing down of the process ; the presence of stricter legislation ; use of a small patient population ; difficulty enrolling children and obtaining an adequate supply of biological samples ; the possibility of adverse events that may only become apparent in the long term and therefore go unnoticed unless long - term studies are undertaken [ 11 ]  . 
 problems linked to the lack of medications that can be used in children therefore include [ 11 ] : greater risk of adverse events , including death , due to inadequate information regarding dose ; ineffective treatment due to underdosage ; nonavailability for the paediatric population of advances in treatment , adequate medications and administration route ; use of magistral or officinal preparations with potentially poor quality . us contrast media are currently used in children off label only , i.e. 
the use of approved medications for nonapproved indications ( dose , age , administration route , indications and contraindications ) for which the scientific evidence suggests their rational use even in clinical situations not approved by regulations [ 12 ]  . 
 the possible fields of us contrast media use , as reported in the most recent literature , are summarised in table 3.this all becomes even more significant when the main advantages offered by ceus in children are considered , i.e. 
 ceus in children : off - label use ? in general , the term off - label use defines the use of medications outside the indications approved by the ministry of health and therefore the prescription of medications for indications , administration route and dosage that differ from those indicated in the product information leaflet [ 12 ]  . 
these are well - known medications with marketing authorisation issued by the italian ministry of health or the european medicines agency ( emea ) [ 31 ] but for which scientific attualmente i mdc in ecografia vengono impiegati in pediatria solo come farmaci off - label , ossia usati in maniera non conforme a quanto previsto dal riassunto delle caratteristiche del prodotto ( dose , et , via di somministrazione , indicazioni e controindicazioni ) per le quali le evidenze scientifiche suggeriscono un loro razionale uso anche in situazioni cliniche non approvate da un punto di vista regolatorio [ 12 ]  . 
tutto ci assume maggior risalto qualora si sottolineano i principali vantaggi che la ceus offre in ambito pediatrico ovvero evitare luso di radiazioni ionizzanti , evitare il ricorso alla narcosi , ottenere una ottima risoluzione , grazie allimpiego di sonde ad alta frequenza . 
 ceus in et pediatrica : uso off - label ? in genere per uso off - label di farmaci si intende correntemente limpiego di farmaci non conforme a quanto previsto nella scheda tecnica autorizzata dal ministero della salute e , quindi , una prescrizione di farmaci per indicazioni , modalit di somministrazione e dosaggi differenti da quelli indicati nel foglio illustrativo [ 12 ]  . 
si tratta di molecole ampiamente conosciute , ma per le quali nuove evidenze scientifiche suggeriscono un loro razionale uso anche in situazioni cliniche non previste nella scheda tecnica e nel foglietto illustrativo di farmaci autorizzati allimmissione in commercio dal ministero della salute o dallagenzia europea per i farmaci ( emea ) [ 31 ]  . 
in italia , luso di mdc ecografico in et pediatrica non risulta validato , sperimentato , e , pertanto , qualora per diverse necessit diagnostiche se ne faccia ricorso , si rientrerebbe in un impiego di tipo offlabel , per limpiego di farmaci off - label , non sono ancora disponibili linee guida specifiche . 
as there are no specific guidelines available for the off - label use of medications , there is an apparent need to define requirements , obligations and liability of the physician prescribing off - label medications , in accordance with the laws in force . 
we therefore examined the ethical , economic and legal reasons for the continued failure to approve the use of us contrast media in children , with reference to the body of legislation that regulates the off - label use of medications . off - label : legal provisions and liability of the ultrasound radiologist a comprehensive analysis of the relevant regulatory framework reveals that in the last 10 years , the italian national direzione di restringere gli ambiti di discrezionalit del medico che intenda prescrivere o impiegare farmaci in indicazioni , et , modalit di somministrazione e dosaggi differenti da quelli indicati nel foglio illustrativo e / o nella scheda tecnica ministeriale . 
prima del 1998 , la materia era regolata dal principio generale della responsabilit professionale : il medico era libero di prescrivere ogni medicinale , per risolvere qualsiasi condizione , qualora lo ritenesse utile per la salute del paziente . 
operava , nel contempo , la regola generale valida per ogni atto medico ( e quindi , anche per le prescrizioni di farmaci ) , vale a dire che chiunque per imperizia , negligenza , ovvero per inosservanza di norme nello svolgimento della professione medica , cagiona ad altri lesioni , danni fisici o la morte , soggiace in sede penale a sanzioni restrittive della libert personale , in sede civile ad obblighi risarcitori , in sede deontologica a sanzioni disciplinari [ 31 ]  . 
la normativa di riferimento che disciplinava la prescrizione e limpiego di farmaci , a carico del sistema sanitario nazionale ( ssn ) , al di fuori delle indicazione terapeutiche approvate dallautorit regolatoria era la legge radiol med ( 2012 ) 117 : 148159 legislation has been clearly moving in the direction of curtailing the degree of discretion a physician has when prescribing or using medications when indications , patient age , administration route and dosage differ from those indicated in the information leaflet and / or ministerial data sheet . 
at the same time , the general rule valid for all medical activity ( and therefore for the prescription of medication ) was in force : whomsoever owing to inexperience , negligence , or noncompliance with the regulations when performing the medical profession , causes injury , physical harm or death to others shall be subject in the criminal setting to sanctions restricting personal freedom , in the civil setting to compensatory obligations , and in the professional setting to disciplinary action [ 31 ]  . 
legislation regulating the prescription and use of medications chargeable to the national health service and which are used for indications outside of those approved by the regulatory authorities was italian law no . 
article 1 , paragraph 4 states : in the event there is no valid treatment alternative , the following medications included in a periodically updated list made available by the single medicines commission [ commissione unica del farmaco ( cuf ) ] can be fully charged to the national health service and used in compliance with the procedures and criteria adopted by the cuf : innovative medications which have been approved for use in other countries but not in italy , medications which have not been approved but are undergoing clinical trial , and medications which may be used for an indication different from the approved indication . the therapeutic activity of the physician is instead currently reputed to be fully legitimate only when the medication has been previously approved by the regulatory body for the same route of administration , dosage or therapeutic indication for which it is effectively prescribed to the patient [ 31 ]  . 
indeed , there is no longer the suggestion of the physicians professional liability on the basis of the original general principle , in that his or her room to manoeuvre in terms of adopting precise and nonapproved treatment choices has been bridled by the narrow framework of the provisions introduced with italian law no . 
17.2.1998 ( aka the di bella law ) , which in article 3 , paragraph 1 states : when providing a medicinal product or other industrially produced medication the prescribing physician shall comply with the therapeutic indications and the route and manner of administration provided for by the approval for commercial use issued by the ministry of health . article 3 of law no . 
1 , comma 4 , disponeva testualmente che qualora non esista valida alternativa terapeutica , sono erogabili a totale carico del ssn i medicinali innovativi la cui commercializzazione autorizzata in altri stati ma non sul territorio nazionale , i medicinali non ancora autorizzati ma sottoposti a sperimentazione clinica e i medicinali da impiegare per unindicazione terapeutica diversa da quella autorizzata , inseriti in apposito elenco predisposto e periodicamente aggiornato dalla commissione unica del farmaco ( cuf ) conformemente alle procedure ed ai criteri adottati dalla stessa . 
 lattivit curativa del medico , invece , reputata oggi pienamente legittima soltanto qualora il medicinale sia stato preventivamente autorizzato dallautorit regolatoria per le medesime modalit di somministrazione , dosaggi o indicazioni terapeutiche per le quali effettivamente prescritto al paziente [ 31 ]  . 
3 della legge 94 / 1998 ( dopo aver enunciato al comma 1 quale sia il criterio generale da adottare quale regola per la legittima prescrizione dei farmaci ) al comma 2 , tuttavia , si premura di precisare anche quale sia leccezione , circoscrivendone gli ambiti e limiti di applicazione : in singoli casi il medico pu , sotto la sua diretta responsabilit e previa informazione del paziente e acquisizione del consenso dello stesso , impiegare il medicinale prodotto industrialmente per unindicazione o una via di somministrazione o una modalit di somministrazione o di utilizzazione diversa da quella autorizzata , ovvero riconosciuta agli effetti dellapplicazione dellart . 
648 , qualora il medico stesso ritenga , in base a dati documentabili , che il paziente non possa essere utilmente trattato con medicinali per i quali sia gi approvata quellindicazione terapeutica o quella via o modalit di somministrazione e purch tale impiego sia noto e conforme a lavori apparsi su pubblicazioni scientifiche accreditate in campo internazionale . 
94 / 1998 , quindi , indica chiaramente gli ambiti entro cui pu legittimamente collocarsi la prescrizione off - label dei farmaci , individuando le precise condizioni cui deve essere subordinata la sua attuazione . 
23 december 1996 , whenever , based on the available data , the physician believes that the patient cannot be effectively treated with the medications which have already been approved for that particular indication or route or manner of administration and provided that the use is known and complies with studies published in accredited scientific publications at the international level . 
article 3 , paragraph 2 of italian law 94 / 1998 , therefore , clearly outlines the settings in which the off - label prescription of medications can take place by identifying the precise conditions that need to be present for it to be implemented . 
these conditions seem to be a halfway point between , on the one hand , the opportunity for the treating physician to make an ethical choice to responsibly identify the most indicated treatment for a specific case , and on the other hand , the need that a certain therapy has already been validated and recognised , according to scientific criteria conceived for a series of homogeneous clinical cases and analysed statistically . 
94 / 1998 appears to implicitly state that the final judgement of the ministry of health can , to a certain extent , be anticipated or substituted , provided that there exists a broadly held opinion in the international scientific community that can be verified in accredited scientific publications . now that we have defined the legal framework regulating the off - label prescription of medications , let us turn to the more specific issue of associated liability . 
the legal framework suggests two possible scenarios regarding the professional liability of the physician : when prescribing a specialty medication or other industrially produced medication , the physician fails to conform to the therapeutic indications , route and manner of administration approved by the ministry of health ; when prescribing off - label medications in individual cases , the physician , based on the available data , is unable to demonstrate that the patient cannot be successfully treated with medications that have already been approved for that particular therapeutic indication or route or manner of administration and that the use is known and conforms to studies published in accredited scientific journals at the international level . clearly , preliminary identification of an external guarantee with a scientific basis and the assumption of direct liabilrappresentare un punto di mediazione tra lopportunit che il medico curante , in scienza e coscienza , possa responsabilmente individuare la terapia pi indicata per il caso concreto , e la necessit che la validit di una cura sia gi stata preventivamente valutata e riconosciuta , secondo criteri scientifici concepiti per una generalit di casi clinici omogenei ed analizzati su base statistica . 
3 comma 2 della legge 94 / 1998 pare implicitamente ammettere che il giudizio finale del ministero della salute possa essere in qualche modo anticipato o surrogato a condizione che sia rintracciabile un parere conforme espresso dalla comunit scientifica internazionale , verificabile attraverso pubblicazioni scientifiche accreditate . una volta definiti i contorni normativi che disciplinano la tematica delle prescrizioni di farmaci fuori indicazione , possibile passare ad esaminare la tematica pi specifica delle responsabilit connesse . a ben vedere , in tale delineato e pi volte confermato quadro normativo due sono le ipotesi residuali di responsabilit professionale del medico : quando il medico , nel prescrivere una specialit medicinale o altro medicinale prodotto industrialmente , non si attiene alle indicazioni terapeutiche , alle vie ed alle modalit di somministrazione previste dallautorizzazione rilasciata dal ministero della sanit ; quando , nel prescrivere in singoli casi farmaci off - label , il medico stesso non sia in grado di dimostrare , in base a dati documentabili , che il paziente non possa essere utilmente trattato con medicinali per i quali sia gi approvata quellindicazione terapeutica o quella via o modalit di somministrazione e che tale impiego sia noto e conforme a lavori apparsi su pubblicazioni scientifiche accreditate in campo internazionale . ovviamente , la preliminare identificazione di un avallo esterno di natura scientifica e lassunzione di una responsabilit diretta rispetto alla terapia farmacologica ipotizzata non esauriscono gli obblighi cui sottoposto il medico ai fini di un legittimo utilizzo off - label dei farmaci . 
al riguardo necessario sottolineare che , in virt dei richiamati precetti costituzionali , la formalizzazione del consenso non pu giammai comportare un temperamento del livello di responsabilit qualificata richiesta al medico n laccettazione di un trattamento inadeguato o privo di radiol med ( 2012 ) 117 : 148159 ity with regard to the hypothetical pharmacological treatment do not account for all of the physicians obligations with regard to the legitimate off - label use of medications . 
one of these obligations is clearly defined by the italian constitution , at article 32 , paragraph 2 , which states that no person is obliged to undergo healthcare treatment unless required by the law ; and at article 13 , which guarantees the sanctity of personal freedom , even with respect to safeguarding ones own health and physical wellbeing . 
on the basis of these constitutional principles , the formalisation of consent can in no way whatsoever involve mitigation of the level of qualified liability required by the physician , or the acceptance of inadequate treatment or treatment lacking therapeutic justification . 
within this legal framework , the conduct of the physician in the off - label use of medications , should this be noncompliant with the setting and conditions for its application , can raise questions of professional liability , which can be qualified under the triple profile of administrativedisciplinary , civil and criminal liability . 
specifically , whereas the administrativedisciplinary aspect of the medical conduct may also originate from the recognition that such conduct has criminal significance , and the civil liability merely has a compensatory / reparative character in terms of the principle of neminem ledere , the physician , instead , runs the risk of criminal liability for professional misconduct only in the presence of the objective and subjective requirement of a crime provided for by the legal syste granted the essential nature of the existence of objective elements of the crime , such as illicit conduct , harm to the patient and a causal relationship between the former and the latter , in order to verify whether a crime has been committed , the medical conduct needs to be described in terms of a strictly subjectivepsychological profile . 
useful elements here are the criteria of negligence and ( possible ) wilfulness that , on the psychological level , indicate awareness of the professional conduct contra legem . another factor that should be considered is the hypothesis of a crime accompanied on the subjective level by possible wilfulness . 
this refers to the physician foreseeing and consequently accepting the extreme risk associated with the administration of a medication not only outside the approved indications but even in the absence of the conditions laid down by the law in force and suggested by the application of basic principles of exercising the medical profession or the principles of a given medical specialty . 
in tale sistema di norme la contingente condotta tenuta dal medico nel ricorso allutilizzo di farmaci off - label , qualora espletata in termini non conformi agli ambiti ed alle condizioni di applicazione , potr determinare ipotesi di responsabilit professionale qualificabili sotto il triplice profilo amministrativo - disciplinare , civile e penale . 
in dettaglio , se la connotazione amministrativo - disciplinare della condotta medica pu scaturire anche dallaccertamento di una sua autonoma rilevanza penale e la responsabilit di natura civilistica ha carattere meramente risarcitorio / riparatorio in applicazione del principio del neminem ledere , il medico incorrer nelle temute ipotesi di responsabilit penale per illecito professionale solo in presenza dei requisiti oggettivi e soggettivi di reato previsti dallordinamento . 
premessa la indispensabilit della sussistenza degli elementi oggettivi del reato , quali la condotta illecita , il verificarsi di un danno per il paziente ed un nesso di causalit tra la prima ed il secondo , ai fini dellaccertamento del reato sar necessario qualificare la condotta medica sotto il profilo strettamente soggettivopiscologico . 
vengono qui in soccorso i criteri della colpa e del dolo ( solo eventuale ) che debbono qualificare , sul piano psicologico , la realizzazione della condotta professionale contra legem . senzaltro residuale da considerarsi lipotesi di verificazione del reato supportata sul piano soggettivo dal dolo eventuale , ovvero della previsione e conseguente accettazione , da parte del medico , del rischio estremo collegato alla somministrazione di un farmaco non soltanto al di fuori delle indicazioni autorizzate , ma addirittura senza che ne ricorrano le condizioni imposte dalla normativa vigente e suggerite dalla applicazione di principi elementari dellesercizio della professione medica o propri di una data specializzazione . 
tale situazione potrebbe ravvisarsi qualora il medico intendesse valutare lefficacia del farmaco in via sperimentale , senza osservare i principi etici e gli adempimenti previsti dalla normativa a tutela del paziente , potendosi in tal caso verificare , in rapporto al danno effettivamente cagionato , i reati di lesioni volontarie o , addirittura , di omicidio volontario . 
 la commissione del fatto reato con atteggiamento colposo del medico ricorrer invece ogni qual volta non sussistano i requisiti e le condizioni cui la normativa subordina la legittimit della prescrizione off - label . 
3 , comma 2 , della legge 94 / 1998 e le numerose norme che vi hanno fatto seguito 156 radiol med ( 2012 ) 117 : 148159 the efficacy of an experimental medicinal product without observing the ethical principles and the requirements established by the legal framework regulating patient protection . 
 a crime committed with negligence on the part of the physician will , instead , occur whenever the requirements and conditions laid down by the law for off - label prescription do not exist . 
94 / 1998 and the many regulations that have followed undoubtedly facilitate interpretation in that violation of the conditions is in itself cause for negligence by failure to observe the laws , regulations , rules or decrees ( article 43 italian criminal code )  . 
this violation can materialise , even in the subjective sense , in the form of professional negligence , carelessness or inexperience , whenever failure to comply with the provisions of the law is reflected in clinical decisions that prove to be inadequate . 
the failure to observe each requirement for the legitimate off - label administration of medications masks a potential profile of professional negligence that can be recognised : when the patient harmed by the chosen treatment has a real and practicable alternative treatment with medications and indications already approved by the ministry of health ; when there are no available ( and therefore documentable ) significant scientific data that , on the basis of the criteria of diligence and expertness associated with the difficulty of the case in hand , allow an innovative treatment to be favoured over an approved one ; when the innovative use of the medication is not backed up by the international scientific literature . therefore , the greater the gap between the recognised best clinical practice and the treatment adopted by the physician in the case at hand , the more serious the negligence of the physician will be in the event of harm to the patient . 
 in addition , the only hypothesis of violation of article 3 of the aforementioned law that may give rise to negligence and civil liability of the physician of a contractual nature , regardless of whether there is clinical malpractice or not , regards the hypothesis of failure to acquire informed consent . 
 the absence of informed consent constitutes an autonomous source of liability whenever the treatment causes harm to or even death of the patient ; therefore , the fact that the treatment was performed correctly is totally irrelevant . for the sake of thoroughness , demanded by the complexity of the topic discussed here , it should also be pointed out that whenever the off - label prescription takes place within a hospital , civil liability may also be extended to the head physician , even when operating in the university setting . 
 tale violazione si concretizza , anche sotto laspetto soggettivo , nella negligenza , imprudenza o imperizia professionale , allorquando linosservanza di disposizioni di legge si rifletta su scelte cliniche rivelatesi di fatto inadeguate , determinando una gradazione della colpa in relazione anche alla gravit della inosservanza normativa . 
linosservanza di ciascuno dei requisiti imposti per la legittimit della somministrazione di farmaci off - label riveste un potenziale profilo di colpa professionale , che si pu ravvisare : laddove il paziente danneggiato dalla cura prescelta abbia una concreta e praticabile alternativa terapeutica con farmaci ed indicazioni gi autorizzate dal ministero della salute ; nel caso in cui non siano reperibili ( e quindi documentabili ) significativi dati scientifici che consentano , sulla base di criteri di diligenza e perizia correlati alla difficolt del caso concreto , di privilegiare un trattamento innovativo rispetto a quello riconosciuto a livello regolatorio ; qualora limpiego innovativo del medicinale non trovi riscontro ed avallo allinterno della letteratura scientifica internazionale . 
 in definitiva , quanto maggiore sar lo stacco tra la migliore pratica clinica riconosciuta e la terapia adottata dal medico nel caso di specie , tanto pi grave andr ritenuta la colpa del medico in presenza di un evento lesivo ai danni del paziente . 
3 della pi volte citata legge che d luogo a colpa ed a responsabilit civile del medico di natura contrattuale , a prescindere da una inadeguatezza di ordine clinico , riguarda lipotesi di mancata acquisizione del consenso informato , la cui assenza costituisce autonoma fonte di responsabilit qualora dallintervento scaturiscano effetti lesivi , o addirittura mortali per il paziente , per cui nessun rilievo pu avere il fatto che lintervento sia stato eseguito in modo corretto . per completezza espositiva , imposta dalla complessit degli argomenti affrontati seppure in forma estremamente sintetica , deve evidenziarsi che , qualora la prescrizione off - label sia attuata allinterno di una struttura ospedaliera , la responsabilit civile potrebbe essere estesa anche al primario , quandanche operante in ambiente universitario , posto che la responsabilit del malato attribuitagli dallart . 
 7 del dpr 128 / 1969 comporta che egli mantenga unappropriata conoscenza dello stato clinico dei pazienti e la vigilanza sullattivit del personale sanitario , comprensiva anche dellinformazione e della verifica in merito alle cure intraprese dai medici . 
pertanto , potrebbe ravvisarsi una responsabilit solidale del primario non soltanto quando radiol med ( 2012 ) 117 : 148159 this is because the liability for the patient attributed to the head physician by article 7 of italian presidential decree no . 
 128 / 1969 requires that he or she maintain adequate knowledge of the patients clinical conditions and the monitoring of the healthcare personnels activity , including information and verification of the treatment undertaken by the physicians . 
therefore , the head physician may be liable not only when the clinical protocol proven to be inadequate has been jointly developed and shared among the individuals operating within the department , but also when the head physician has failed to implement the necessary treatment monitoring activities provided by the healthcare personnel , provided that the initiative undertaken by the individual physician does not take the form of a completely unpredictable event that is deviant of approved clinical practice , and therefore foreign to any kind of treatment planning . 
 in conclusion , it should be clear that the element characterising regulation in matters of off - label administration of medications is the need for a different treatment approach ; in other words , the complete absence of valid and approved therapeutic alternatives . 
this judgement of therapeutic need must be based not only on the absence of therapeutic alternatives , but also on the significance of the disease and the existence of even preliminary data supporting a favourable risk benefit profile of the medication in the indication requested . 
 rather , the diagnostic efficacy of the product and , above all , the scarcity of its side effects provide substantial reasons for supporting the use of this kind of diagnostic instrument both in children and in adults . 
 with the aim to facilitate the development and accessibility of medicinal products for use in the paediatric population , the regulation provides for : ongoing improvement of the information available on the use of medications in different paediatric populations ; constant updating of analyses on the use of medications in paediatrics , including all forms of off - label use ; careful analysis of the existing paediatric medicinal products in order to ascertain the consistency with the favourable scientific evidence in terms of the paediatric risk benefit profile ; standardising , in the setting of a paediatric study framework , indications , dosage , contraindications and precautions for paediatric use of products that contain the same active ingredient . 
 il protocollo clinico rivelatosi inadeguato sia stato congiuntamente elaborato o condiviso dai soggetti operanti allinterno del reparto , ma anche quando il primario abbia omesso di espletare la necessaria attivit di verifica sulle cure operate dal personale sanitario , purch liniziativa intrapresa dal singolo medico non si configuri come un evento assolutamente imprevedibile e deviante dalla prassi clinica approvata , e quindi estraneo a qualsiasi logica di programmazione terapeutica . 
 in conclusione , deve osservarsi che lelemento caratterizzante le diverse discipline legislative succedutesi in materia di somministrazione di farmaci off - label rappresentato dalla necessit del diverso percorso terapeutico , in altri termini dalla inesistenza di valide ed autorizzate alternative terapeutiche . 
siffatto giudizio di necessit terapeutica non pu che basarsi , oltre che sullassenza di alternative terapeutiche , sul rilievo della patologia e sullesistenza di dati , anche iniziali , attestanti un favorevole profilo rischio / beneficio del farmaco nellindicazione richiesta . 
piuttosto , lefficacia diagnostica del prodotto e soprattutto la scarsit dei suoi effetti collaterali rappresentano le sostanziali ragioni a supporto della utilit del ricorso a tale tipo di strumento diagnostico in et pediatrica , al pari che nelladulto . 
1901 / 2006 approvato il 12 dicembre 2006 e relativo ai medicinali per uso pediatrico , il quale , con il dichiarato fine di agevolare lo sviluppo e laccessibilit di medicinali per uso pediatrico impone : il continuo miglioramento delle informazioni disponibili sulluso dei medicinali nelle diverse popolazioni pediatriche ; il costante aggiornamento delle analisi sugli usi dei farmaci in pediatria , comprendente tutte le forme di uso offlabel ; la puntuale analisi delle esistenti confezioni di farmaci pediatrici , onde accertarne la coerenza con evidenze scientifiche favorevoli sotto il profilo del rischio / beneficio pediatrico ; lobiettivo di uniformare , secondo un piano di indagine pediatrica , indicazioni , dosaggi , controindicazioni , precauzioni per luso pediatrico di prodotti che contengono lo stesso principio attivo . 
 il suddetto regolamento indica certamente una strada percorribile per una sperimentazione certa e sicura che possa approvare lutilizzo del ceus anche in et pediatri158 radiol med ( 2012 ) 117 : 148159 this regulation undoubtedly indicates a way ahead for safe and certain experimentation that can approve the use of ceus in paediatric populations and therefore enable the us radiologist to break free from the insidious practice of the use of contrast media in an off - label framework . conclusioni ca uscendo definitivamente cos dagli schemi insidiosi per il medico ecografista di un utilizzo in chiave off - label . conclusions analysis of the legal provisions regulating the prescription of medications shows , although in a manner not completely precise or unanimous , where the borders may lie in determining the negligence , harm and causal relationship in this setting of liability . 
in this setting , from the radiological point of view , us contrast media share the same problems that have already arisen and are currently debated regarding the use of iodinated contrast media in radiographic examinations and the use of gadolinium - based contrast media in magnetic resonance imaging [ 32 ]  . 
patient safety , informed consent and physician liability are the key features for the off - label use of medication , for which patients should receive detailed information regarding all the possible consequences . 
it is our hope , however , to go beyond the off - label use of ceus in children by regulating and extending its possible and often decisive use to this category of patients . lanalisi dei presupposti normativi e regolatori cui subordinata lattivit di prescrizione dei farmaci da parte del medico , evidenzia , sebbene in maniera ancora non completamente precisa ed unanimemente concorde , quali possano essere i confini in cui possano determinarsi la colpa , il danno ed il nesso di causalit rilevanti in tale fattispecie di responsabilit . 
in tale contesto , dal punto di vista radiologico , il mdc ecografico condivide le medesime problematiche gi insorte , e oggetto di discussione , riguardo luso di mdc organo - iodati per esami radiografici e limpiego di agenti di contrasto a base di gadolinio utilizzati in risonanza magnetica [ 32 ]  . 
sicurezza per il paziente , consenso informato e responsabilit del medico sono i cardini dellimpiego dei farmaci off - label per cui , i pazienti devono essere informati dettagliatamente di tutte le conseguenze di un trattamento off - label . 
il nostro auspicio , tuttavia , di poter andare ben oltre un utilizzo off - label del ceus in et pediatrica regolamentando ed estendendo cos anche a questa categoria di piccoli pazienti il suo possibile e spesso risolutivo impiego . 
passariello1 1 department of radiological sciences , university of rome la sapienza , viale regina elena 324 , 00161 rome , italy 2 department of radiology , azienda ospedaliera universitaria ( a.o.u. ) cagliari , polo di monserrato , italy correspondence to : m . 
accuratezza , sensibilit , specificit , valore predittivo positivo ( vpp ) e valore predittivo negativo ( vpn ) sono stati calcolati per ecd , angio - rm ed angio - tc . 
le differenze di performance tra le metodiche sono state valutate utilizzando il test di mcnemar , il test di wilcoxon e lanalisi delle curve receiver operating characteristic ( roc ) ( p < 0 , 05 )  . 
per la valutazione della morfologia di placca lanalisi delle auc delle quattro metodiche ha evidenziato una sostanziale equivalenza tra angio - tc ed angio - rm con ss , ma ha evidenziato una lieve differenza di entrambe le metodiche nei confronti dellangio - rm con pp ( p = 0 , 04 ) e dellecd ( p = 0 , 038 )  . 
la valutazione delle ulcere ha evidenziato una differenza statisticamente significativa tra langio - rm e langio - tc ( p = 0 , 040 , 046 ) e lecd ( p = 0 , 019 )  . 
 parole chiave aterosclerosi arterie stroke arterie carotidee introduction introduzione stroke is the third leading cause of death and one of the major causes of disability in western countries ( around 400 , 000 deaths in european union countries each year )  . 
each year , cerebrovascular ischaemic events cause around 20 million cases of permanent disability , and in 25% of these cases , the ischaemic event is the result of stenosis / occlusion of the epiaortic arteries , particularly the carotid arteries [ 1 ]  . 
 according to criteria of the north american symptomatic carotid endarterectomy trial ( nascet ) , endarterectomy reduces the risk of ischaemic events in all patients with 7099% carotid stenosis [ 2 ] and in selected patients with 5069% stenosis [ 3 ]  . 
histological and imaging studies [ 46 ] have also stressed that stroke may be dependent not only on degree of stenosis but also on the morphological features of the plaque , such as ulcers or fissures causing rupture [ 7 ] of the plaque itself . 
all of these factors therefore need to be taken into account for a correct diagnostic and preventive approach aimed at risk stratification and treatment planning to reduce the incidence and severity of acute cerebrovascular disease . 
cdus is the first - choice lictus rappresenta la terza causa di morte ed una delle maggiori cause dinvalidit nei paesi occidentali ( circa 400.000 morti per i paesi dellunione europea ) , con il 20% dei pazienti che non sopravvive allevento ischemico ed il 55% che rimane affetto da invalidit di vario grado . 
ogni anno gli eventi ischemici cerebrovascolari causano circa 20 milioni di casi di disabilit permanenti , ed in circa il 25% dei casi levento ischemico riconducibile a patologia stenoocclusiva dei vasi epiaortici e in particolare delle arterie carotidi [ 1 ]  . 
in accordo con i criteri del north american symptomatic endoarterectomy trial ( nascet ) , lendoarterectomia riduce il rischio di eventi ischemici in tutti i pazienti con stenosi carotidea del 70%99% [ 2 ] ed in casi selezionati con stenosi del 50%69% [ 3 ]  . 
studi istologici e di imaging [ 46 ] hanno inoltre sottolineato come levento ictale possa essere dipendente non soltanto dal grado di stenosi , ma anche dalle caratteristiche morfologiche della placca , come ad esempio la presenza di ulcere o fissurazioni cause di rottura [ 7 ] della placca stessa . 
tutti questi fattori indipendenti devono quindi essere presi in considerazione per un adeguato approccio diagnostico - preventivo atto a stratificare il rischio e pianificare il trattamento per ridurre lincidenza e la gravit della patologia cerebrovascolare acuta . 
tuttavia il ruolo diagnostico della dsa stato progressivamente sostituito da tecniche non invasive di primo e secondo livello , tra cui leco - color doppler 56 radiol med ( 2012 ) 117 : 5471 technique and often the only technique required . 
its limitations in terms of spatial resolution have largely been overcome thanks to the introduction of parallel imaging techniques and the recent availability of high - relaxivity blood - pool agents , such that images with anatomical detail similar to cta images can now be obtained [ 1316 ]  . 
despite the numerous published studies , there is neither official consensus regarding the indications for use of mra rather than cta nor one technique definitively shown to be superior to the other in characterising stenosis / occlusion using state - of - the - art equipment . 
the aim of this study was therefore to prospectively evaluate the accuracy of all three noninvasive diagnostic modalities in diagnosing carotid artery stenosis in a large patient population , using dsa as a reference technique . materials and methods patient population and informed consent between may 2006 and may 2010 , 416 patients ( mean age 5421.3 years ; range 4990 ; 304 men and 112 women ) with a history of suspected cerebrovascular events [ amaurosis fugax , stroke , transient ischaemic attack ( tia ) or reversible ischemic neurological deficit ( rind ) ] and suspected carotid artery stenosis underwent preliminary cdus . 
all patients with haemodynamically significant stenosis at cdus , with stenosis calculated sonographically according to the nascet criteria as > 70% or between 30% and 50% with irregular atheroma , were sent for combined evaluation with cta and mra . 
patients with an indication for treatment according to the nascet criteria based on the mra and / or cta studies subsequently underwent dsa during the classic endarterectomy procedure or as a guide for the endovascular procedure . 
the indication for one procedure rather than another was based on the surgical and clinical risk as assessed by the referring department on the basis of the following criteria : patients sent for endarterectomy had low surgical risk , particularly long stenoses ( > 20 mm ) , potentially unstable plaques with emboligenic risk during the endovascular procedure ( ipsilateral symptoms or evident ulceration ) or concentric calcified plaques at risk of rupture during stent expansion ; patients sent for endovascular treatment had high ( ecd ) , langiografia con risonanza magnetica ( angio - rm ) e langiografia con tomografia computerizzata ( angio - tc )  . 
langio - tc rappresenta la scelta pi frequente e riproducibile per lapprofondimento diagnostico , offrendo uneccellente accuratezza per lindividuazione e la caratterizzazione della patologia [ 9 , 10 ] , sia in fase di planning che di follow - up post - trattamento [ 11 ]  . 
negli ultimi anni si inoltre assistito ad un progresso tecnologico costante che ha ridefinito langio - rm come tecnica robusta e non invasiva per lo studio dei vasi epiaortici [ 12 ] ; le limitazioni inerenti la risoluzione spaziale sono state ampiamente superate grazie allintroduzione delle tecniche di imaging parallelo e recentemente dalla commercializzazione di mezzi di contrasto ( mdc ) intravascolari e ad alta relassivit con possibilit di ottenere immagini con dettaglio anatomico simile a quello dellangio - tc [ 1316 ]  . 
 attualmente , nonostante lampia produzione scientifica disponibile , non esiste un consenso ufficiale sulle indicazioni allimpiego dellangio - rm piuttosto che dellangiotc , n stata definitivamente dimostrata la superiorit di una tecnica rispetto allaltra per la caratterizzazione della patologia steno - ostruttiva su apparecchiature allo stato dellarte . 
 lobiettivo di questo studio stato pertanto di valutare prospetticamente , in unampia popolazione di pazienti , laccuratezza di tutte e tre le metodiche di imaging non invasive nella diagnostica della stenosi carotidea utilizzando la dsa come riferimento . materiali e metodi popolazione e consenso informato nel periodo compreso tra maggio 2006 e maggio 2010 sono stati sottoposti a studio preliminare con ecd 416 pazienti ( et media 5421 , 3 anni ; range 4990 anni ; 304 uomini e 112 donne ) con anamnesi positiva per sospetti eventi cerebrovascolari ( amaurosis fugax , ictus , attacco ischemico transitorio [ tia ] o deficit neurologico ischemico reversibile [ rind ] ) e sospetta stenosi carotidea . 
tutti i pazienti con stenosi emodinamicamente significativa allecd , con stenosi calcolabile ecograficamente secondo i criteri nascet come superiore al 70% o compresa tra 30% e 50% con ateroma irregolare , sono stati indirizzati a valutazione combinata con angio - tc ed angio - rm . 
i pazienti con indicazione al trattamento secondo i criteri nascet sulla base dellangio - rm e / o dellangio - tc sono successivamente stati sottoposti a dsa durante intervento di endoarterectomia classica o come guida per la procedura endovascolare . 
lindicazione alluna piuttosto che allaltra radiol med ( 2012 ) 117 : 5471 surgical risk , short stenosis ( < 20 mm ) , regular or irregular plaque but presumably with low emboligenic risk during the endovascular procedure . patients who had already undergone surgical or endovascular treatment for carotid stenosis or who had general contraindications to mr , ct or dsa were excluded from the study . 
all patients provided written informed consent after being thoroughly informed about the advantages and disadvantages of the four techniques and of the benefits and potential risks of enrolling in the study . 
 doppler ultrasonography all cdus examinations were done using an aplio xv device ( toshiba medical systems , japan ) or mylab 70 ( esaote biomedica , genoa , italy ) , with dedicated software for the vascular study and a 5 - 12 mhz multiband linear transducer . 
in the former case , colour doppler and longitudinal scans were used to measure the residual lumen at the point of maximum narrowing and the normal lumen of the internal carotid artery at the most point that could be visualised most distal to the stenosis . 
haemodynamically , the points of peak velocity were visualised at the level of the stenosis , and pulsed doppler sampling was performed at these points with an insonation angle between 40 and 60 and a sample volume of 1.5 min these cases , the degree of stenosis was determined on the basis of the maximum ( threshold value of peak systolic velocity for haemodynamic significance equal to 125130 cm / s )  . 
in all cases , a colour doppler study was nonetheless obtained of the haemodynamic effects of the plaque with an evaluation of the doppler spectrum proximal and distal to the stenosis and at the level of the stenosis . computed tomography angiography the cta study was performed in all patients with a multislice system ( sensation cardiac 64 , siemens medical system , erlangen , germany )  . 
a venous access ( 18 gauge ) was gained via the antecubital vein of the right ar the scan was done after the administration of 50 ml of nonionic iodinated contrast agent ( iomeprol 400 mgi / ml , iomeron 400 , bracco , milan , italy ) , followed by 30 ml of saline solution with a flow rate of 4 ml / s using a dual - head injector ( stellant d , medrad , warrendale , pa , usa )  . 
the optimal delay between contrast agent administration and the start of the scan was evaluated by the bolus - tracking technique , with a region of interest ( roi ) placed at the level of the aortic arch and automatic triggering at 150 hu . 
the images were acquired with the following protocol : 120 kv , procedura stata posta in base al rischio operatorio ed alla richiesta clinica effettuata dal reparto di riferimento in base ai seguenti criteri : sono stati indirizzati ad endoarterectomia i pazienti con basso rischio operatorio , stenosi particolarmente lunghe ( > 20 mm ) , placche potenzialmente instabili ed a rischio emboligeno durante procedura endovascolare ( sintomatologia ipsilaterale o ulcere ben evidenti ) , placche concentriche calcifiche a rischio di rottura durante lespansione degli stent ; sono stati indirizzati a trattamento endovascolare i pazienti con alto rischio operatorio , stenosi corte ( < 20 mm ) , placche regolari o irregolari ma comunque presumibilmente a basso rischio emboligeno durante la procedura endovascolare . sono stati preventivamente esclusi dallo studio tutti i soggetti gi sottoposti a trattamento chirurgico o endovascolare per stenosi carotidea o che presentavano controindicazioni generali allesecuzione di esami rm , tc e dsa . 
 tutti i pazienti hanno fornito un consenso informato scritto dopo essere stati informati accuratamente sui vantaggi e svantaggi delle quattro metodiche e sui benefici ed i potenziali rischi dellarruolamento nello studio . 
 eco - color doppler tutti gli esami ecd sono stati eseguiti utilizzando un ecografo aplio xv ( toshiba medical systems , giappone ) o mylab 70 ( esaote biomedica , genova , italia ) , con software dedicato per lo studio vascolare e sonda lineare multi banda da 512 mhz . 
nel primo caso , utilizzando il color doppler e scansioni longitudinali , sono stati misurati lume residuo nel punto di massimo restringimento e lume dellarteria carotide interna nel punto pi distale visualizzabile a valle della stenosi . 
emodinamicamente sono stati visualizzati i punti di massima velocit a livello della stenosi , in corrispondenza dei quali stato effettuato il campionamento doppler pulsato con angolo di insonazione compreso tra 40 e 60 e volume campione di 1 , 5 min questi casi la percentuale di stenosi stata determinata sulla base della massima ( valore soglia della velocit di picco sistolico per la significativit emodinamica pari a 125130 cm / s )  . 
in tutti i casi stato comunque eseguito uno studio color doppler degli effetti emodinamici della placca con valutazione dello spettro doppler a monte , a valle , e in corrispondenza della stenosi . angio - tc in tutti i pazienti langio - tc stata effettuata con un appa58 radiol med ( 2012 ) 117 : 5471 180 mas , pitch 0.8 , slice thickness 0.7 mm , reconstruction increment 0.5 mm , matrix 512512 , scan time 68 s , kernel b30f smooth . 
 magnetic resonance angiography all examinations were performed with a 1.5 - t system ( magnetom avanto , siemens medical system , erlangen , germany , with peak gradient strength 45 mt / m , peak slew rate 200 mt / m / ms ) , with total imaging matrix ( tim ) coil and integrated parallel acquisition technique ( ipat )  . 
the precontrast images were acquired in coronal planes with a 3d spoiled gradientecho sequence optimised for high spatial resolution and a short acquisition time ( tr 3.5 ms , te 1.2 ms , fa 30 , ta 14 s , thickness 0.7 mm , matrix 384384 , voxel 110.7 mm , ipat2 )  . 
the same sequence was repeated for firstpass ( fp ) imaging after the injection of 0.03 mmol / kg of gadofosveset trisodium ( previous denomination : vasovist , schering , berlin , germany ; current denomination : ablavar , lantheus medical imaging , north billerica , ma , usa ) , which was administered with an automatic injector at a rate of 1 ml / s through an 18 - gauge cannula placed in the antecubital vein of the right arm , followed by 15 ml of saline solution . 
the steady state ( ss ) images were acquired 4 min after the injection of contrast agent with a 3d spoiled gradient - echo sequence optimised to obtain a high - resolution acquisition ( tr 7.5 ms , te 2.3 ms , fa 30 , ta 325 s , thickness 0.7 mm , matrix 512512 , voxel 0.70.70.7 mm , ipat2 )  . 
the first injection of contrast agent at the level of the aortic arch and the subsequent images in the two views ( left and right anterior oblique ) were sufficient for identifying the common carotid arteries , the vertebral arteries and the subclavian arteries . 
after selective catheterisation of the common carotid arteries , anteroposterior , lateral and oblique ( 45 ) images were obtained , and the intracranial circulation was visualised in anteroposterior and lateral views . 
all patients received a nonionic iodinated contrast agent ( iomeprol 300 mgi / ml , iomeron 300 , bracco , milan , italy ) ; the dose was 20 ml with injection rate of 20 ml / s for images at recchiatura multistrato ( sensation cardiac 64 , siemens medical system , erlangen , germania )  . 
la scansione stata effettuata previa somministrazione di 50 ml di mezzo di contrato iodato non ionico ( iomeprolo 400 mgl / ml , iomeron 400 , bracco , milano , italia ) , seguiti da 30 ml di soluzione salina , ad un flusso di 4 ml / s per mezzo di un iniettore a doppia testata ( stellant d , medrad , warrendale , pennsylvania , usa )  . 
il ritardo ottimale tra la somministrazione del mdc e linizio della scansione stato valutato mediante tecnica di bolus tracking con posizionamento di una regione di interesse ( roi ) a livello dellarco aortico e triggering automatico a 150 hu . 
le immagini sono state acquisite con il seguente protocollo : 120 kv , 180 mas , pitch 0 , 8 , spessore di strato 0 , 7 mm , recon increment 0 , 5 mm , matrice 512512 , scan time 68 secondi , kernel b30f smooth . 
 angio - rm tutti gli esami sono stati effettuati con unapparecchiatura ad 1 , 5 t ( magnetom avanto , siemens medical system , erlangen , germania ; massima intensit dei gradienti 45 mt / m , velocit per raggiungere lampiezza massima 200 mt / m / ms , con tecnologia total imaging matrix , tim coil , e tecnica di acquisizione integrata parallela , ipat )  . 
le immagini maschera pre - contrastografiche sono state acquisite su piani coronali con una sequenza spoiled gradient - echo 3d , ottimizzata per unalta risoluzione spaziale e un breve tempo di acquisizione ( tempo di ripetizione [ tr ] 3 , 5 ms , tempo di eco [ te ] 1 , 2 ms , flip angle [ fa ] 30 , tempo di acquisizione [ ta ] 14 s , spessore : 0 , 7 mm , matrice 384384 , voxel 1 mm1 mm0 , 7 mm , ipat 2 )  . 
la stessa sequenza stata ripetuta per limaging di primo passaggio ( pp ) dopo liniezione di 0 , 03 mmol / kg di gadofosveset trisodium ( precedente denominazione : vasovist , schering , berlin , germania ; attuale denominazione : ablavar , lantheus medical imaging , north billerica , ma , usa ) somministrati mediante iniettore automatico ad una velocit di 1 ml / s attraverso una cannula da 18 g posizionata a livello della vena antecubitale del braccio destro , seguiti da 15 ml di soluzione salina ; il ritardo ottimale tra liniezione e linizio dellacquisizioni delle immagini del primo passaggio stato valutato con lutilizzo del bolus tracking . 
le immagini allo stato stazionario ( ss ) sono state acquisite 4 minuti dopo liniezione del mezzo di contrasto con una sequenza spoiled gradient - echo 3d modificata per unacquisizione ad alta risoluzione ( tr 7 , 5 ms , te 2 , 3 ms , fa 30 , ta 325 s , spessore : 0 , 7 mm , matrice 512512 , voxel 0 , 7 mm0 , 7 mm0 , 7 mm , ipat 2 )  . 
 radiol med ( 2012 ) 117 : 5471 the level of the aortic arch and 610 ml with an injection rate of 6 ml / s for the selective catheterisation at the level of the common carotid arteries . 
the images were assessed with a software client dedicated to cardiovascular applications ( aquarius thin client ; terarecon , san matteo , ca , usa ) , and the readers interacted in real time with the data sets using maximum intensity projection ( mip ) reconstructions to identify the site of stenosis , together with simple and curved multiplanar reformation ( mpr and c - mpr ) to quantify the degree of stenosis . 
the quality of the cta and mra images was evaluated according to the following criteria : optimal ( homogeneous enhancement and precise depiction of the vessel , lack of motion artefacts ) , adequate ( homogeneous enhancement and precise depiction of the vessel , possible presence of motion artefacts does not negatively influence the measurements ) and suboptimal ( inhomogeneous enhancement with poor intraluminal signal and poor depiction of the wall , motion artefacts negatively influence the measurements )  . 
degree of stenosis was evaluated according the nascet criteria : i ( 129% ) mild , ii ( 3049% ) and iii ( 5069% ) moderate , iv ( 7099% ) severe and v occlusion . 
 plaque morphology was evaluated at the vessel lumen interface : the plaque was defined as irregular in the presence of nonmeasurable surface irregularities with no evidence of a true parietal and ulcerated niche , and ulcerated when a deep niched ulcer with clear margins was visualised . 
la prima iniezione di contrasto , a livello dellarco aortico , e le successive immagini secondo le due proiezioni ( sinistra e destra antero - obliqua ) sono state dirimenti per individuare le carotidi comuni , le arterie vertebrali e le arterie succlavie . 
dopo una cateterizzazione selettiva delle carotidi comuni sono state ottenute immagini in antero - posteriore , laterale e nelle direzioni oblique ( 45 ) ed il circolo intracranico stato visualizzato in antero - posteriore e nelle proiezioni laterali . 
in tutti i pazienti stato utilizzato un mezzo di contrasto iodato non ionico ( iomeprolo 300 mgl / ml , iomeron 300 , bracco , milano , italia ) al dosaggio di 20 ml con un flusso di 20 ml / s per le immagini a livello dellarco aortico e 610 ml sono stati utilizzati , con un flusso di 6 ml / s , per la cateterizzazione selettiva a livello delle carotidi comuni . 
ogni esame stato condotto con un field of view ( fov ) di 33 cm con una matrice di 10241024 e una risoluzione spaziale di 0 , 320 , 32 mm . analisi delle immagini gli esami angio - rm ed angio - tc sono stati valutati in cieco da due osservatori indipendenti ( rispettivamente con 15 e 10 anni di esperienza in radiologia vascolare ) per la definizione della qualit delle immagini , della stima del grado di stenosi e della caratterizzazione della morfologia di placca . 
le immagini sono state valutate attraverso un software client dedicato alle applicazioni cardiovascolari ( aquarius thin client ; terarecon , san matteo , california , usa ) ed i lettori hanno interagito in tempo reale con i set di dati usando ricostruzioni a massima intensit proiettiva ( mip ) per identificare il sito di stenosi ed una ricostruzione multiplanare semplice e centroluminale ( mpr e c - mpr ) al fine di quantificare il grado di stenosi . 
the differences in performance between the three imaging modalities were assessed with the mcnemar test for dichotomous values , the wilcoxon test for classifying the degree of stenosis and lesion morphology and roc curve analysis and area under the curve ( auc ) to evaluate the differences in overall accuracy of the three modalities . 
all continuous values were expressed as mean standard deviation ( sd ) , and confidence intervals ( ci ) were identified at 95% with statistical significance set at p < 0.05 for all tests performed . results on the basis of the cdus findings , 205 patients underwent cta and mra . 
these patients ( mean age 696.5 ; age range 6290 ; 108 men and 62 women ; 97 dsa performed during stenting procedure and 73 dsa performed during endarterectomy ) comprised the final patient population in our comparative study . 
 the mean duration of the examination was 153 min for cdus , 203 min for mra , 153 min for cta and 456 min for dsa , including patient preparation . 
there were 11 cases ( 6.5% ) of complications following the dsa procedure ( one cerebral ischaemia , four pseudoaneurysms and six haematomas at the puncture site ) ; eight ( 4% ) patients suffered moderate - to - severe adverse reactions to the iodinated contrast agent . 
all adverse reacadeguata ( enhancement omogeneo e precisa delineazione del vaso , possibile presenza di artefatti da movimento non condizionanti le misurazioni ) , sub - ottimale ( enhancement disomogeneo con scarso segnale intraluminale e scarsa delineazione della parete , artefatti da movimento condizionanti le misurazioni )  . 
la valutazione del grado di stenosi stata eseguita secondo i criteri nascet : i ( 1%29% ) stenosi lieve , ii ( 30%49% ) e iii ( 50%69% ) stenosi moderata ; iv ( 70%99% ) stenosi severa ; v occlusione . 
laspetto della placca stato valutato allinterfaccia con il lume vasale : la placca stata definita irregolare in presenza di piccole irregolarit superficiali , non misurabili , senza evidenza di una vera e propria nicchia parietale e ulcerata quando si evidenziata una profonda ulcera a nicchia con profili netti . 
le differenze relative al tempo di refertazione medio per ciascuna metodica sono state studiate con il test t di student , la qualit diagnostica stata invece valutata con il test per ranghi di wilcoxon . 
lagreement stato giudicato secondo la seguente classificazione : scarso per valori di < 0 , 40 , da moderato a buono per valori di = 0 , 410 , 75 , ed eccellente per valori di > 0 , 75 [ 18 ]  . 
le differenze di performance tra le metodiche sono state valutate utilizzando il test di mcnemar per valori dicotomici , il test di wilcoxon per il grading delle stenosi e la morfologia delle lesioni e lanalisi delle curve receiver operating characteristic ( roc ) e delle relative aree sotto la curva ( auc ) per valutare le differenze nellaccuratezza globale delle tre metodiche . 
tutti i valori continui sono stati espressi come mediadeviazione standard ( ds ) e gli intervalli di confidenza sono stati individuati al 95% con un livello di significativit statistica < 0 , 05 per tutti i test effettuati . risultati in base ai criteri di valutazione stabiliti per lecd sono radiol med ( 2012 ) 117 : 5471 table 1 demographic and clinical characteristics of the study cohort . 
 mean age , body mass index , blood glucose level , total cholesterol level , high - density lipoprotein cholesterol ( hdl ) and low - density lipoprotein cholesterol ( ldl ) values are expressed as mean valuestandard deviation ( sd ) , with relative range ( min - max ) in parentheses . 
gender and risk factors are shown as numbers of patients with relative percentage in parentheses tabella 1 la tabella mostra le caratteristiche demografiche e cliniche del gruppo oggetto dello studio . 
let media , lindice di massa corporea , la glicemia sierica basale , i valori di colesterolemia totale , i valori delle lipoproteine ad alta densit ed a bassa densit , sono espressi come valore mediodeviazione standard con il relativo range ( minmax ) riportato in parentesi . 
the patient with cerebral ischaemia was hospitalised and discharged 7 days later ; the haematomas were treated with embolisation during the angiography session itself , whereas the pseudoaneurysms were reassessed during follow - up . 
 the quality of the cta images was optimal in 308 vessels stati sottoposti ad esame angio - tc ed angio - rm 205 pazienti ; in 211 pazienti lo studio ecd non ha rilevato alterazioni tali da giustificare lintegrazione diagnostica con le metodiche di secondo livello . 
sulla base dei risultati dello studio angio - rm e / o angio - tc sono stati successivamente indirizzati a trattamento e conseguentemente a dsa 170 pazienti ( et media 696 , 5 anni , range 6290 anni , 108 uomini e 62 donne , 97 dsa eseguite durante procedura di stenting e 73 dsa eseguite durante endoarterectomia ) che hanno costituito la popolazione definitiva del nostro studio comparativo . 
in due casi lesame angio - rm non stato ritenuto diagnostico a causa della scarsa qualit dovuta ad artefatti da movimento , pertanto sono state studiate complessivamente 336 arterie carotidi interne . 
 il tempo medio di durata dellesame stato di 153 minuti per lecd , di 203 minuti per langio - rm , 153 minuti per langio - tc , 456 minuti per la dsa , includendo la preparazione del paziente . 
 dopo angio - tc , reazioni avverse al mezzo di contrasto iodato di grado lieve ( rash , nausea , flushing o orticaria ) si sono verificate in 9 ( 5% ) pazienti ; 2 ( 1% ) pazienti hanno invece avuto una reazione avversa di grado moderatosevero ( broncospasmo e dispnea , ipotensione )  . 
in seguito alle procedure angiografiche si sono verificate 11 ( 6 , 5% ) complicanze dovute alla procedura ( 1 ischemia cerebrale , 4 pseudo - aneurismi e 6 ematomi nel sito di puntura ) ; 8 ( 4% ) pazienti hanno invece sperimentato reazioni avverse di grado moderato - severo al mdc iodato . 
cdus also proved to be substantially similar to the other imaging modalities ( 0.06 < p < 0.09 ) , although the values were close to the limit of statistical significance . 
for evaluating plaque morphology , the mcnemar test was unable to rule out the hypothesis of overall equality avverse al mdc sono state risolte con la somministrazione di corticosteroidi e seguite da monitoraggio clinico per almeno 24 ore dopo lesame . 
il paziente con ischemia cerebrale stato ricoverato e dimesso dopo 7 giorni , i sanguinamenti sono stati trattati nella stessa seduta angiografica con embolizzazione mentre gli pseudo - aneurismi sono stati rivalutati in corso di follow - up . 
 qualit delle immagini il tempo medio di valutazione stato di 62 minuti per langio - tc , 51 minuti per langio - rm in pp , 102 minuti per langio - rm in ss , 63 minuti per pp + ss e 42 minuti per la dsa . 
pp + ss sono risultate significative ( p < 0 , 05 ) ; non sono risultate significative le differenze nel tempo di valutazione tra angio - tc , angio - rm in pp e dsa ( p > 0 , 05 )  . 
 la qualit delle immagini nellangio - rm di pp stata ottimale in 224 vasi ( 66% ) , adeguata in 76 ( 22% ) e subottimale in 36 ( 12% )  . 
la qualit delle immagini nellangio - rm di ss stata ottimale in 284 vasi ( 84% ) e adeguata in 52 ( 16% ) ; tutti e 36 i vasi con qualit dimmagine sub - ottimale nel pp hanno ottenuto una valutazione ottimale allo ss . 
in cinque pazienti , a causa degli artefatti da movimento , stato necessario ripetere lacquisizione allo ss pi volte ( fino a 3 volte in un caso isolato ) per raggiungere una qualit dimmagine ottimale / adeguata . 
in 3 pazienti le ricostruzioni mip non sono state considerate adeguate per la diagnosi a causa di artefatti da movimento e il grado della stenosi stato valutato usando le immagini assiali . 
 in 2 pazienti lapnea respiratoria non stata possibile a causa delle condizioni cliniche ; nonostante ci , la qualit delle immagini stata giudicata adeguata per la diagnosi in tutti i casi . 
 sia gli esami ecd che dsa sono stati tutti eseguiti correttamente e con livello qualitativo adeguato alla valutazione del grading della stenosi , della morfologia della placca e di eventuale presenza di ulcerazioni parietali . grado di stenosi la figura 1 mostra le regressioni lineari ottenute dal confronto tra i valori di stenosi ottenuti con lecd , radiol med ( 2012 ) 117 : 5471 fig . 
la concordanza tra i due osservatori nella misurazione del grado di stenosi stata eccellente sia per langio - rm che per langio - tc con valori di compresi tra 0 , 84 e 0 , 86 ( tabella 3 )  . 
nel confronto inter - metodica , valutando le stenosi dal punto di vista della significativit clinica , il test di mcnemar ha confermato lipotesi di sostanziale eguaglianza globale sia tra le letture al pp ed allo ss ( p = 0 , 508 ) che tra le due letture di angio - rm ed angio - tc ( p = 0 , 50 , 9 )  . 
anche la metodica ecd si sostanzialmente rivelata sovrapponibile alle altre metodiche ( p = 0 , 060 , 09 ) anche se con valori prossimi al limite di significativit statistica . 
la migliore correlazione si ottenuta alla lettura delle sequenze allo ss sia per la morfologia di placca ( = 0 , 87 ) che per lidentificazioni di ulcerazioni ( = 0 , 97 )  . 
per la valutazione della morfologia di placca il test di mcnemar non stato capace di escludere lipotesi di uneguaglianza globale tra pp , ss , angio - tc ed ecd ( p = 0 , 40 , 9 )  . 
per la presenza di ulcere pp e ss si sono rivelati sostanzialmente uguali ( p = 0 , 118 ) , ma entrambi differenti rispetto allangio - tc ( p = 0 , 040 , 046 )  . 
secondo le linee guida internazionali , lendoarterectomia lintervento ( ma recentemente si andato affermando sempre pi anche il trattamento endovascolare ) di scelta per stenosi carotidee asintomatiche > 70% , e viene consigliata anche per stenosi del 50%69% con sintomatologia attiva [ 19 ]  . 
 bench storicamente rimanga la metodica di riferimento nella valutazione del grado di stenosi della carotide , la dsa paga i costi elevati , linvasivit e la significativa incidenza di stroke associato alla procedura , stimata intorno all1%2% , da sommare alle problematiche relative alle complicanze locali ( trombosi , dissecazione , ematoma , lesioni nervose e venose associate ) , stimate globalmente attorno al 2%5% a seconda delle casistiche considerate [ 20 ]  . 
i valori sono espressi come numero di casi plaque morphology evaluated on dsa irregular regular ulcerations evaluated with dsa ulcerated not ulcerated morfologia delle placche valutata con dsa non regolare regolare presenza di ulcerazioni valutata con dsa ulcerata non ulcerata morfologia delle placche valutata con ecd / mra - pp / mra - ss / cta non regolare regolare 146 / 148 / 164 / 168 22 / 20 / 4 / 0 32 / 28 / 12 / 0 136 / 140 / 156 / 168 presenza di ulcerazioni valutata con ecd / mra - pp / mra - ss / cta ulcerata non ulcerata 56 / 60 / 64 / 64 8 / 4 / 0 / 0 30 / 28 / 10 / 0 242 / 244 / 262 / 272 discussion the ability to precisely characterise significant carotid artery stenosis is fundamental for guiding treatment decisions . 
 according to the international guidelines , endarterectomy is the procedure ( although recently , endovascular treatment has received increasing attention ) of choice for asymptomatic carotid artery stenoses > 70% , and it is also recommended for symptomatic stenoses with a 5069% narrowing of the lumen [ 19 ]  . 
whereas dsa historically remains the reference technique in evaluating the degree of carotid stenosis , the technique is encumbered by high costs , invasiveness and an estimated 12% incidence of procedure - related stroke , in addition to which there are local complications ( thrombosis , dissection , haematoma , associated nerve and vascular damage ) globally estimated at around 25% according to the patient population considered [ 20 ]  . 
moreover , new evidence has shown that other parameters ( plaque morphology and composition ) in addition to the degree of stenosis are important for the purposes of correct stratificadiagnostico per lo studio delle patologie steno - occlusive dei vasi epiaortici [ 21 ]  . 
inoltre , nuove evidenze stanno dimostrando come altri parametri ( morfologia e composizione dellateroma ) , oltre al grado di stenosi , siano importanti ai fini di una corretta stratificazione di rischio cerebrovascolare , orientando le necessit diagnostiche pre - terapeutiche verso quelle metodiche in grado di valutare le caratteristiche di placca carotidea , oltre alla stenosi del lume vasale . 
ma se da un lato si presenta come tecnica rapida e di basso costo , dallaltro appaiono pressoch invalicabili i limiti intrinseci rappresentati dalla bassa riproducibilit sia interche intra - operatore , la cui accuratezza variabile rende difficile il monitoraggio delle lesioni nel tempo . 
lecd inoltre non permette una visualizzazione tridimensionale e completa della struttura anatomica e rende spesso necessaria lintegrazione con altre metodiche , che consentano la valutazione anche del circolo intracranico dellorigine dei tronchi sovraortici e della morfologia vasale , per un planning terapeutico completo , sia al fine di eventuale lesioni ateromasiche radiol med ( 2012 ) 117 : 5471 fig . 
4a - e colour doppler ultrasonography ( cdus ) ( a ) shows a haemodynamically significant plaque with severe stenosis of the carotid sinus and the proximal segment of the left internal carotid artery ; a focal ulceration can also be appreciated . 
4a - e lindagine ecd ( a ) evidenzia una stenosi emodinamicamente significativa , di grado severo , che coinvolge il bulbo carotideo e ed il tratto prossimale della carotide interna di sinistra ; ben apprezzabile anche una focale ulcerazione della placca . 
as a result , the pretreatment diagnostic workup includes those techniques able to evaluate not only the stenosis of the vascular lumen but also the characteristics of the carotid plaque . 
cdus has become the coesistenti , sia per valutare lanatomia vascolare quale parametro indispensabile in sede interventistica . nellultimo decennio langio - tc e langio - rm hanno fondamentale progressivamente raggiunto un ruolo 68 radiol med ( 2012 ) 117 : 5471 fig . 
5a - e colour doppler ultrasonography ( cdus ) ( a ) shows a haemodynamically significant stenosis of the carotid sinus and proximal segment of the left internal carotid artery . 
le immagini angio - rm ottenute al pp ( b ) evidenziano una placca lunga , prevalentemente fibro - lipidica che causa una stenosi di circa il 50% , nelle acquisizioni angio - rm allo ss ( c ) ed angio - tc ( d ) la stenosi invece appare del 70% circa . 
lindagine dsa ( e ) conferma la stenosi di grado severo ( 70% ) a carico del vaso . established level - one technique thanks to its diagnostic reliability and ability to provide useful morphological and flowvelocity information at the carotid bifurcation . 
on the one hand , cdus is a rapid and low - cost technique ; however , on the other hand , intrinsic limits of low interand intraoperator reproducibility appear almost insurmountable , such that the variable accuracy makes monitoring lesions over time very difficult . 
these latter techniques are also able to evaluate intracranial circulation , the origin of the supra - aortic vessels and vascular morphology , thus providing complete treatment planning both in terms of identifying possible co - existing atheromatous lesions and evaluating the vascular anatomy , an essential prerequisite for interventional procedures . over the last 10 years , cta and mra have progressively attained a fundamental role in the imaging of stenosis / occlusions of the epiaortic vessels thanks to their increasing diagnostic reliability . 
both techniques are able to rapidly confirm the clinical suspicion of vascular damage and to provide accurate information regarding compensatory intracranial vascular flow , thus proving very useful for treatment planning [ 22 , 23 ]  . continuous technological progress in the field of cta has led to improvements in acquisition techniques and image reconstruction , with a marked increase in the diagnostic capabilities of the technique [ 24 ]  . 
the advent of multidetectorrow systems of the latest generation ( 64 slices or more ) , with nellimaging della steno - ostruttiva dei vasi epiaortici grazie ad una crescente affidabilit diagnostica . 
entrambe le metodiche permettono sia di confermare rapidamente il sospetto clinico del danno vascolare , sia di dare accurate informazioni circa la vascolarizzazione di compenso intracranico consentendo un efficace planning terapeutico [ 22 , 23 ]  . il continuo progresso tecnologico nel campo dellangiotc ha consentito un miglioramento delle tecniche di acquisizione e di ricostruzione delle immagini con un notevole incremento della capacit diagnostica della metodica [ 24 ]  . 
 lavvento delle apparecchiature multistrato di ultima generazione ( 64 strati ed oltre ) , con tempi di rotazione uguali o inferiori a 0 , 5 secondi , consente attualmente lesecuzione di routine dellesame con una velocit superiore ed una dose di contrasto ridotta rispetto a quanto ottenibile con le apparecchiature a 4 e 16 strati e con qualit ottimale , soprattutto in relazione alla possibilit di evitare la contaminazione della fase arteriosa pura da parte del ritorno venoso giugulare che in condizioni di circolo normali avviene in tempi estremamente rapidi e non pertanto completamente evitabile con le apparecchiature pi lente . 
per quanto concerne la misurazione dellentit della stenosi , lassociazione tra datasets con risoluzione spaziale sub millimetrica ( voxel di dimensioni inferiori a 0 , 5 mm3 ) e ricostruzioni mpr dedicate , ottenute su piani obliqui o parallelamente al lume del vaso , consente una valutazione pi efficace dellanatomia della lesione , sia per quanto riguarda la stima del grado di stenosi , sia in relazione alla definizione della morforadiol med ( 2012 ) 117 : 5471 rotation times 0.5 s , has made it possible to perform routine examinations with higher speed and a lower dose of contrast agent than with 4and 16 - slice systems . 
the quality obtained is optimal , particularly thanks to the ability to avoid contamination in the pure arterial phase due to jugular venous return , which under normal conditions is extremely rapid and cannot be completely avoided with slower systems . 
with regard to measuring the degree of stenosis , combining data sets with submillimetre spatial resolution ( voxel size < 0.5 mm3 ) with dedicated mpr reconstructions obtained in oblique planes or parallel to the vessel lumen produces a more effective evaluation of the lesion anatomy , both in terms of measuring the percent stenosis and defining the plaque morphology . 
these include examination time , limitations in obese patients or patients with non - mr - compatible implants and the need to use state - of - the - art equipment . 
from the diagnostic point of view , despite the use of contrast enhancement , there remains the limitation due to proton dephasing in critical stenoses and the consequent risk of overestimating high - grade stenosis , particular when non - state - of - the - art equipment and sequences with suboptimal spatial resolution are used [ 27 , 28 ]  . 
in our study , this possibility was minimised thanks to the use of sequences with high spatial resolution , both during the fp phase , which was possible due to the high - performance system and use of parallel imaging , and with greater detail in the ss phase made possible with the use of the blood - pool agent . 
in addition , the particular molecular structure of the agent produces an approximately fivefold increase in the r1 effect at 1.5 t with respect to interstitial contrast media [ 29 ] , with the possibility of greater vascular enhancement and a reduction in low - velocity flow artefacts in the fp phase . 
in fact , to date , the study of stenoses / occlusions has been limited to information obtainable with a conventional laminography technique or to imaging with sequences aimed at studying plaque composition without angiographic sequences [ 3034 ]  . 
in our experience , this limitation was partially overcome by the possibility of obtaining better characterisation of plaque morphology than had been achieved with other contrast media [ 16 , 3538 ]  . 
 inoltre da sottolineare la capacit dellangio - tc di potere discriminare le componenti lipidiche , quelle fibrose ed il calcio presente negli ateromi , consentendo quindi lidentificazione di alcuni dei fattori predisponenti alle complicazioni quali emorragia o ulcerazione [ 4 , 25 , 26 ]  . 
 langio - rm , bench dotata del vantaggio di non necessitare di radiazioni ionizzanti per lacquisizione delle immagini , mantiene alcuni limiti intrinseci , quali il tempo di esecuzione , le limitazioni nei pazienti obesi o con impianti non rm - compatibili e la necessit di utilizzare apparecchiature allo stato dellarte . 
dal punto di vista diagnostico , nonostante lutilizzo delle tecniche con mdc , permane , soprattutto nelle apparecchiature non allo stato dellarte e in relazione allacquisizione di sequenze con risoluzione spaziale sub - ottimale , la limitazione dovuta al defasamento dei protoni nelle stenosi critiche ed al conseguente rischio di sovrastima delle stenosi di alto grado [ 27 , 28 ]  . 
nel nostro studio questeventualit stata ridotta al minimo , sia grazie allutilizzo di sequenze ad elevata risoluzione spaziale , sia durante la fase di pp , resa possibile con tempi brevissimi dallapparecchiatura performante e dallimpiego dellimaging parallelo , sia con maggior dettaglio durante la fase di ss , possibile con lutilizzo del mdc intravascolare . 
in particolare il mdc intravascolare permette lacquisizione di sequenze con una risoluzione spaziale pressoch sovrapponibile a quella dellangio - tc ; inoltre la particolare struttura molecolare del composto consente un incremento delleffetto r1 di circa 5 volte ad 1 , 5 t rispetto a mdc interstiziali [ 29 ] , con possibilit di maggior enhancement vascolare e riduzione degli artefatti da bassa velocit di flusso nella fase di pp . 
fino ad oggi infatti lo studio delle lesioni steno - occlusive era limitato alle informazioni ottenibili con lapproccio luminografico convenzionale o allimaging con sequenze mirate allo studio della composizione di placca ottenute senza sequenze angiografiche [ 3034 ] : nella nostra esperienza questo limite parzialmente superato per la possibilit di ottenere una migliore caratterizzazione della morfologia di placca rispetto a quanto precedentemente ottenuto con altri mdc [ 16 , 3538 ]  . 
tale numerosit campionaria ha permesso unanalisi inferenziale con risultati nettamente attendibili e leterogeneit del campione ha inoltre permesso una buona astrazione sulla popolazione , permettendoci di trarre conclusioni che , con buona approssimazione , possono essere estese a tutte le popolazioni con caratteristiche simile ed a tutti gli studi effettuati con tecniche allo stato dellarte . 
nella nostra casistica abbiamo dimostrato che sia lo studio angio - tc e angio - rm possono essere utilizzati per individuare il danno aterosclero70 radiol med ( 2012 ) 117 : 5471 possible a good abstraction of the population , thus allowing us to draw conclusions that , with good approximation , can be extrapolated to all populations with similar characteristics and all studies done with state - of - the - art technology . 
in our patient population , we showed that the cta and mra studies can be used to identify atherosclerotic damage to the carotid arteries with high levels of accuracy , sensitivity and specificity . 
a further advantage of cta with respect to other noninvasive techniques , in addition to the high accuracy , sensitivity and specificity , regards the greater accuracy in identifying and defining calcified plaque , which can be important in candidates for interventional procedures such as percutaneous transluminal angioplasty dilatation and stenting . 
in particolare langio - tc e le sequenze angio - rm ottenute allo ss si sono dimostrate altamente diagnostiche , con , rispettivamente , sensibilit 95% e 93% e specificit 98% e 97% . 
anche i valori di accuratezza dellangio - tc ( 97% ) e dellangio - rm allo ss ( 95% ) si sono rivelati sostanzialmente superiori a quanto ottenuto dalle sequenze di angio - rm al pp e dallecd , rispettivamente 92% e 76% . 
inoltre , lelevata risoluzione spaziale dello ss cosi come quella dellangio - tc mostrano unelevata capacit di evidenziare la morfologia di placca come criterio per le lesioni ad alto rischio patogenetico , in linea con precedenti esperienze preliminari [ 39 ]  . 
seppur i valori di accuratezza , sensibilit e specificit dellangiotc e dellangio - rm allo ss si avvicinino molto , l angiotc si attesta come la metodica pi accurata , sensibile e specifica per quantificare e caratterizzare la patologia stenosante carotidea . 
un ulteriore vantaggio dellangiotc rispetto alle altre metodiche non invasive , oltre alla pi elevata accuratezza , sensibilit e specificit , riguarda la miglior accuratezza nellidentificazione e definizione delle placche calcifiche che pu rappresentare un aspetto importante nel paziente candidato a procedure interventistiche quali dilatazione pta e stenting . 
la angio - rm rimane metodica altrettanto valida , ma da considerarsi leggermente inferiore rispetto alla langio - tc , anche se con lutilizzo delle sequenze ss tende ad eguagliare laccuratezza dellangio - tc . 
 complications occurred in 21 cases ( 25.6% ) : eight were major ( two stent migrations , one pulmonary embolism , one haemoperitoneum , one haemobilia , three intrahepatic haematomas ) and 13 were minor ( encephalopathy responsive to medical therapy )  . 
twenty - one patients ( 25.6% ) died due to the following causes : disseminated intravascular coagulation ( dic ) ( n = 2 ) , haemorrhage ( n = 8 ) , cardiopulmonary failure ( n = 2 ) and liver failure ( n = 9 )  . 
tra i possibili fattori prognostici di mortalit precoce sono stati studiati statisticamente il child , la conta piastrinica , il tempo di protrombina , la creatininemia e le pressioni venose pree post - tips . 
 abbiamo registrato 21 complicanze ( 25 , 6% ) : 8 maggiori ( 2 migrazioni di stent , unembolia polmonare , 1 emoperitoneo , 1 emobilia e 3 ematomi intraepatici ) e 13 minori ( encefalopatia responsiva a terapia medica )  . 
 ventuno pazienti ( 25 , 6% ) sono deceduti per : coagulazione intravasale disseminata ( 2 ) , emorragia ( 8 ) , insufficienza cardio - respiratoria ( 2 ) , insufficienza epatica ( 9 )  . 
 radiol med ( 2012 ) 117 : 4653 keywords tips emergency early mortality haemorrhage liver failure parole chiave tips urgenza mortalit precoce emorragia insufficienza epatica introduction introduzione gastrooesophageal varices develop in 3070% of cirrhotic patients with portacaval pressure gradients between 8 and 10 mmhg , and 936% of them have a high risk of rupture [ 1 ]  . 
 the mainstay of treatment for bleeding includes control of the haemorrhage , which can be achieved in 85% of cases through combined medical and endoscopic therapy [ 48 ]  . 
rebleeding , the risk of which is highest within the first 72 h after tips , occurs in 3040% of cases within 46 weeks after the first episode [ 9 , 10 ]  . 
a peculiarity of emergency tips compared with elective tips is its high early mortality rate and the higher incidence of complications , both of which are related to several clinical and laboratory factors predating the procedure [ 11 ]  . 
the purpose of this retrospective review of a large case series treated at our institute over the last 18 years is to critically analyse and discuss results , adverse events and possible clinical , laboratory , and technicalradiological predictors of mortality during the first month of follow - up . 
 materials and methods between january 1992 and december 2009 , 82 patients ( 55 men and 27 women ; age range 3182 years ; mean age 55 years ) underwent emergency tips at our institute for refractory bleeding caused by ruptured oesophageal varices . 
all patients had liver cirrhosis of different aetiology : viral in 41 cases , alcoholic in 20 , both viral and alcoholic in eight , cryptogenic in eight and biliary in five cases . procedure le varici esofago - gastriche si sviluppano nel 30%70% dei pazienti cirrotici con gradiente pressorio porto - cavale compreso tra 8 e 10 mmhg ; il 9%36% di esse presentano un elevato rischio di rottura [ 1 ]  . 
tra i capisaldi del trattamento del sanguinamento vi il controllo dellemorragia ottenibile nell85% dei casi con lassociazione di terapia medica ed endoscopica [ 48 ] ; il transjugular intrahepatic portosystemic shunt ( tips ) permette di ottenere lemostasi in un ulteriore 5%10% dei casi [ 5 ]  . 
la recidiva emorragica , il cui rischio massimo entro le prime 72 ore dal tips , avviene nel 30%40% dei casi entro 46 settimane dal primo episodio [ 9 , 10 ]  . 
peculiare dellurgenza rispetto al tips in elezione lelevata mortalit precoce e la pi elevata incidenza di complicanze , entrambe legate ad alcuni fattori clinico - laboratoristici pre - esistenti alla procedura [ 11 ] ; scopo di questo lavoro , basato sulla revisione retrospettiva di un ampia casi stica raccolta presso il nostro centro negli ultimi 18 anni , analizzare e discutere criticamente i risultati , gli eventi avversi e gli eventuali fattori prognostici clinici , laboratoristici e tecnici radiologici di mortalit nel primo mese di follow - up . 
 materiali e metodi da gennaio 1992 a dicembre 2009 presso il nostro istituto di radiologia sono stati sottoposti a tips in urgenza per sanguinamento irrefrenabile da rottura di varici esofagee 82 pazienti , 55 maschi e 27 femmine , det compresa tra 31 e 82 anni , con unet media di 55 anni . 
tutti i pazienti erano affetti da cirrosi epatica a diversa eziologia : in 41 casi virale , in 20 casi alcolica , in 8 casi virale ed alcolica , in 8 casi criptogenetica e in 5 casi biliare . 
 all patients were studied in the angiography suite with doppler ultrasound ( us ) to assess the patency , flow direction and velocity of the portal vein , hepatic veins , presence of possible hepatocellular carcinoma ( hcc ) and echogenicity of liver parenchyma . 
in one patient with suspected neoplastic portal vein thrombosis , a four - phase computed tomography ( ct ) scan was performed to help in the diagprocedura tutti i pazienti sono stati studiati in sala angiografica con eco - doppler per valutare la perviet , la direzione e la velocit della porta , le vene epatiche , la presenza di eventuali 48 radiol med ( 2012 ) 117 : 4653 nosis . 
monitoring the patients vital signs was started as soon as they entered the radiological rooall angiographic manoeuvres were performed with the anaesthetistresuscitator in attendance and according to the technique already described [ 12 ]  . 
the stents were dilated to a diameter between 8 and 10 mportal vein thromboses were treated with repeated angioplasty procedures using balloons with diameters of 814 min 17 patients ( 22% ) , persistent gastrooesophageal varices were selectively embolised using metal coils ( balt , montmorency , france ; cook , bjaeverskov , denmark ) measuring 10 mm and 16 mm in diameter . follow - up with the exception of the viatorr stent - grafts , which were checked after 710 days , in all other cases , a us examination of the abdomen was performed within 48 h of the angiographic procedure in order to assess the patency and indicative flow rate of the shunt and to exclude any possible complications , also classified according to the criteria of the society of interventional radiology ( sir )  . 
 in particular , success was considered from the following points of view : technical ( ability to create a shunt between a suprahepatic vein and an intrahepatic portal branch ) , haemodynamic ( satisfactory reduction of the portosystemic gradient to a value close to 10 mmhg and distension of gastrooesophageal and / or intestinal varices on follow - up phlebography ) and clinical ( interruption of acute bleeding with return to haemodynamic stability without any need for transfusions and / or pharmacological support )  . analysis of early mortality several clinical and laboratory parameters were considered , as suggested in the literature : childs class , creatinine levels , total bilirubin levels , platelet count , and the prothrombin time ( pt )  . 
the technical aspects included those contained in the radiology reports and representable by a number : procedure time , portal pressure , right atrial pressure and portosystemic gradient before and after tips . 
le protesi sono state dilatate ad un calibro variabile tra 8 e 10 mle trombosi portali sono state trattate con angioplastiche ripetute , utilizzando palloni di diametro variabile tra 8 mm e 14 m in 17 pazienti ( 22% ) sono state embolizzate selettivamente varici gastro - esofagee persistenti con spirali metalliche ( balt , montmorency , francia ; cook , bjaeverskov , danimarca ) di 10 mm e 16 mm di diametro . 
 follow - up entro 48 ore dalla manovra angiografica , tranne che per i viatorr il cui controllo stato eseguito a 710 giorni , stata effettuata unecografia delladdome per valutare la perviet ed una portata indicativa dello shunt ed escludere possibili complicanze , anchesse classificate secondo i criteri della societ di radiologia interventistica ( sir ) ; successivamente i pazienti sono stati sottoposti a sorveglianza clinica e ad un ulteriore controllo eco - color doppler ad 1 mese , salvo diversa indicazione clinica . 
sono stati considerati meritevoli di revisione angiografica stent con portata inferiore a 700800 ml / m analisi dei risultati lanalisi dei risultati stata condotta studiando il successo della procedura e le complicanze ad essa riconducibili secondo le linee guida sir [ 13 ]  . 
in particolare , il successo stato considerato dal punto di vista tecnico ( capacit di creare uno shunt tra una vena sovraepatica ed un ramo portale intraepatico ) , emodinamico ( soddisfacente riduzione del gradiente porto - sistemico ad un valore prossimo ai 10 mmhg e detenzione delle varici esofago - gastriche e / o intestinali alla flebografia di controllo ) e clinico ( interruzione dellemorragia acuta con ritorno ad una stabilit emodinamica senza la necessit di trasfusioni e / o di supporto farmacologico )  . 
 analisi della mortalit precoce sono stati considerati , come suggerito dalla letteratura , radiol med ( 2012 ) 117 : 4653 test , after excluding the two patients who underwent transplantation a few days after tips . results technical success was achieved in 77 / 84 patients ( 91.6% ) ; in 4 / 6 cases , the portal thrombosis was resolved , whereas two failures were caused by a cavernoma . 
mean angiography - suite time was 70 min for patients with patent portal system and homogeneous parenchyma with normal reflectivity ( 71 / 82 ) and 90 min for patients with neoplastic portal thrombosis / infiltration and / or marked steatosis . 
in 5 / 82 patients ( 6.1% ) , bleeding persisted because of liver failure , whereas in 6 / 82 ( 7.3% ) rebleeding occurred due to shunt thrombosis ( n = 1 ) , oesophageal ulceration following sclerotherapy ( n = 1 ) and liver failure ( n = 4 )  . there were 21 complications ( 25.6% ) , which did not affect prognosis . 
eight of them were major ( 9.8% ) ( palmaz stent migration into a pulmonary artery , n = 2 ; symptomatic pulmonary embolism , n = 1 ; haemoperitoneum due to failure to deflation the gastrooesophageal haemostatic balloon after tips , n = 1 ; haemobilia , n = 1 ; intrahepatic haematoma , n = 3 ) , and 13 were minor ( 15.8% ) ( portosystemic encephalopathy controlled with medical therapy )  . 
of 82 patients , 21 ( 25.6% ) died within 30 days of tips due to disseminated intravascular coagulation ( n = 2 ) , haemorrhage ( n = 8 ) , cardiopulmonary failure ( n = 2 ) and liver failure ( n = 9 )  . 
among the factors examined , the following were found to predict early mortality : childs class c , serum creatinine > 1.5 mg / dl and increase of pt ( tables 1 and 2 )  . discussion emergency tips is indicated for all cases of refractory variceal bleeding , regardless of the estimated hepatic reserve an estimation that may be difficult and inaccurate in the acute phase [ 11 ]  . 
the decrease in portosystemic gradient to a mean value of 10 mmhg allows bleeding to be arrested in > 90% of cases against an acceptable incidence of portosystemic encephalopathy ( pse )  . 
nevertheless , the technical success of tips may not be synonymous with haemodynamic and clinical success , even though the persistence or recurrence alcuni aspetti clinico - laboratoristici : la classe di child , la creatininemia , la bilirubinemia totale , la conta piastrinica ed il tempo di protrombina . 
tra gli aspetti tecnici sono stati indagati quelli riportati nel referto radiologico rappresentabili con un valore numerico : il tempo di procedura , la pressione portale , la pressione atriale destra ed il gradiente porto - sistemico prima e dopo il tips . 
per la valutazione statistica stato utilizzato lexact test di fisher , escludendo dalla nostra analisi 2 pazienti trapiantati alcuni giorni dopo il tips . risultati il successo tecnico stato raggiunto in 77 / 84 pazienti ( 91 , 6% ) ; in 4 / 6 casi stato possibile risolvere la trombosi portale , mentre i 2 insuccessi sono stati determinati dalla presenza di un cavernoma . 
dilatando lo stent ad un calibro medio di 9 mm , il gradiente porto - sistemico passato da un valore medio di 24 , 04 mmhg a 10 , 43 mmhg . 
il successo clinico si avuto in 71 / 82 pazienti ( 86 , 6% ) : in 5 / 82 pazienti ( 6 , 1% ) si avuto persistenza del sanguinamento per insufficienza epatica , mentre in 6 / 82 ( 7 , 3% ) si presentata una recidiva emorragica causata da : trombosi dello shunt ( 1 caso ) , ulcerazione esofagea successiva a scleroterapia ( 1 caso ) ed insufficienza epatica ( 4 casi )  . abbiamo registrato 21 complicanze ( 25 , 6% ) , che non hanno inficiato la prognosi del paziente , di cui 8 ( 9 , 8% ) maggiori ( 2 migrazioni di stent palmaz in arteria polmonare , unembolia polmonare sintomatica , 1 emoperitoneo per mancata desufflazione post - tips del pallone emostatico esofago - gastrico , 1 emobilia e 3 ematomi intraepatici ) e 13 ( 15 , 8% ) minori ( encefalopatia porto - sistemica controllabile con terapia medica )  . 
ventuno degli 82 pazienti ( 25 , 6% ) sono deceduti entro 30 giorni dal tips per : coagulazione intravasale disseminata ( 2 casi ) , emorragia ( 8 casi ) , insufficienza cardio - respiratoria ( 2 casi ) ed insufficienza epatica ( 9 casi )  . 
in our experience , post - tips complications , which were slightly more frequent than reported in the literature [ 13 ] , may be mostly attributed to highly insufficient coagulation and to the inadequacy of stents available in the early 1990s . mento varicoso irrefrenabile , indipendentemente dalla stima della riserva epatica , che in fase acuta pu essere difficile ed imprecisa [ 11 ]  . 
se eseguita da operatori esperti , la procedura pu essere condotta con successo nella quasi totalit dei casi ; la trombosi portale , la marcata steatosi epatica e lincostante disponibilit di operatori con consolidata esperienza ecografica ne accrescono la difficolt tecnica rispetto alle procedure delezione . 
la riduzione del gradiente porto - sistemico ad un valore medio di 10 mmhg radiol med ( 2012 ) 117 : 4653 consente di arrestare lemorragia in oltre il 90% dei casi a fronte di unaccettabile incidenza di eps . 
il buon esito tecnico del tips pu tuttavia non essere sinonimo di successo emodinamico e clinico : la persistenza o la recidiva della emorragia sono tuttavia per lo pi condizionate da fattori indipendenti dalla perviet dello shunt , come lentit della pressione portale durante levento acuto e la rapidit con cui viene eseguita la decompressione [ 14 ]  . 
tra gli aspetti tecnici angiografici abbiamo deciso di non considerare il tipo di stent impiegato , in quanto i risultati iniziali della nostra esperienza sono inficiati oltre che dallinadeguatezza del materiale allora disponibile anche dalla curva the early mortality rate of patients undergoing emergency tips is still high and has virtually remained unchanged over the last decade [ 4 , 1519 ]  . 
among the technical aspects of angiography , we chose not to consider the type of stent implanted , as the results of our initial expecreatinine ( mg / dl ) fig . 
3 rapporto tra sopravvivenza e tempo di protrombina ( pt ) nei pazienti sottoposti a tips in urgenza . pt ( % ) 52 radiol med ( 2012 ) 117 : 4653 rience were influenced not only by the inadequacy of the material available at the time but also by the operators learning curve . 
scientific evidence of the superiority of polytetrafluoroethylene - covered stents has persuaded us to use the viatorr stent - graft for the past year [ 23 ]  . to conclude , our results , based on one of the largest published case series , suggest that within the first month of emergency tips , the patients prognosis is only affected by pre - existing clinical and laboratory factors and not by the angiography technique . di apprendimento degli operatori ; levidenza scientifica della superiorit degli stent ricoperti in politetrafluoroetilene ( ptfe ) ci ha indotto nellultimo anno ad utilizzare il viatorr [ 23 ]  . in conclusione , i nostri risultati , ricavati dalla una delle pi ampie casistiche mai pubblicate , indicano come , entro il primo mese dal tips durgenza , la prognosi del paziente sia condizionata esclusivamente da fattori clinico - laboratoristici pre - esistenti alla procedura e non dalla tecnica angiografica . 
pisani2 1dipartimento di scienze biomorfologiche e funzionali , universit degli studi federico ii , napoli , italy 2dipartimento di nefrologia , universit degli studi federico ii , napoli , italy 3dipartimento di medicina clinica e scienze cardiovascolari ed immunologiche , universit degli studi federico ii , napoli , italy 4istituto di biostrutture e bioimmagini , cnr , napoli , italy 5azienda ospedaliera - universitaria di parma , parma , italy correspondence to : m . 
imbriaco , via posillipo 196 , 80123 napoli , italy , tel . : + 39 - 081 - 5757370 , fax : + 39 - 081 - 5457081 , e - mail : mimbriaco@hotmail.com received : 10 december 2010 / accepted : 12 january 2011 / published online : 10 july 2011 springer - verlag 2011 abstract purpose . 
anderson - fabry disease is a multisystemic disorder of lipid metabolism secondary to x - chromosome alterations and is frequently associated with cardiac manifestations such as left ventricular ( lv ) hypertrophy , gradually leading to an alteration in cardiac performance . 
la malattia di anderson - fabry un disordine multi - sistemico del metabolismo lipidico , secondario ad una alterazione del cromosoma x ed frequentemente associata a sintomi cardiaci come lipertrofia ventricolare sinistra , che gradualmente conduce ad una alterazione della performance cardiaca . 
dopo 48 mesi di terapia , si osservata una significativa riduzione dei valori di massa e dello spessore di parete del ventricolo sinistro ( vs ) : 18759 g vs . 
in patients with anderson - fabry disease undergoing enzyme replacement therapy with agalsidase beta , mri documented a significant reduction in myocardial t2 relaxation time , a significant decrease in maximal myocardial thickness and in total lv mass . 
nei pazienti affetti da malattia di andersonfabry ed in terapia enzimatica sostitutiva con agalsidase beta , la rm documenta una significativa riduzione del tempo di rilassamento t2 miocardico , una significativa riduzione degli spessori massimi miocardici e della massa ventricolare totale sinistra . 
la rm non rileva un significativo miglioramento della funzionalit sistolica globale del ventricolo sinistro , tuttavia assistiamo ad un miglioramento della classe funzionale nyha , compatibile con un miglioramento della funzionalit diastolica . 
 parole chiave rm malattia di anderson - fabry sintomi cardiaci tempo di rilassamento t2 introduction introduzione anderson - fabry disease is a rare x - linked recessive disorder characterised by the presence of affected hemizygous male and heterozygous female carriers who may nonetheless present with a milder form of the disease . 
the most severely involved organs are kidneys , heart , skin , vascular districts , central and autonomic nervous system , eyes and the audiovestibular apparatus [ 13 ]  . 
in particular , at the cardiac level , the myocardial accumulation of glycosphingolipids acts as a trigger leading to myocardial cell hypertrophy , which cannot be distinguished from hypertrophic cardiomyopathy ( hcm ) on common imaging modalities and especially on ultrasound ( us )  . 
the presence la malattia di anderson - fabry una rara malattia a trasmissione recessiva legata al cromosoma x , caratterizzata dalla presenza di maschi emizigoti affetti e di femmine eterozigoti portatrici , che possono comunque manifestare una forma blanda di malattia . 
 gli organi maggiormente coinvolti sono il rene , il cuore , la cute , i distretti vascolari , il sistema nervoso autonomo e centrale , locchio e lapparato audio - vestibolare [ 13 ] ; in particolare , a livello cardiaco , laccumulo di glicosfingolipidi a livello miocardico , agisce da spina irritativa inducendo una vera e proprio ipertrofia dei miocardiociti , indistinguibile dalla cardiomiopatia ipertrofica ( hcm ) alle comuni tecniche di imaging ed in particolare allecocardiografia . 
together with uraemia , in patients with chronic renal failure not subjected to dialysis and / or renal transplantation , cardiac damage represents the leading cause of death , in female patients in particular . 
the most common clinical manifestations include left ventricular ( lv ) hypertrophy , valvular heart disease , coronary artery disease and conduction defects , which contribute to producing congestive heart failure , arrhythmias and myocardial infarction [ 4 , 5 ]  . 
with the cloning of the - gal a gene and the advent of molecular genetics , therapeutic doses of recombinant enzymes can be synthesised that , once in the blood stream , are internalised by the vascular endothelial and parenchymal cells thanks to receptors for mannose - 6 - phosphate on the cellular surface [ 69 ]  . 
the purpose of our study was to monitor with long - term magnetic resonance imaging ( mri ) follow - up the changes occurring at the cardiac level in patients with anderson - fabry treated with enzyme replacement therapy . materials and methods patient population unevenienza molto frequente , riscontrabile in oltre il 60% dei maschi affetti e delle donne eterozigoti . 
assieme alluremia , nei pazienti con insufficienza renale cronica non sottoposti a dialisi e / o trapianto renale , il danno cardiaco rappresenta la prima causa di morte , in particolare nei soggetti femminili . 
le pi comuni manifestazioni cliniche comprendono lipertrofia del ventricolo sinistro ( vs ) , le valvulopatie , la coronaropatia e difetti della conduzione , che concorrono allinsufficienza cardiaca congestizia , allinsorgere di aritmie ed allinfarto del miocardio [ 4 , 5 ]  . 
con la clonazione del gene - gal a e lavvento delle tecnologie di genetica molecolare , ora possibile sintetizzare quantit terapeutiche di enzima ricombinante che , una volta in circolo , viene internalizzato dalle cellule dellendotelio vascolare e dalle cellule parenchimali grazie ai recettori per il mannosio - 6 - fosfato sulla superficie cellulare [ 69 ]  . 
scopo del nostro studio stato quello di monitorare con risonanza magnetica ( rm ) a lungo termine , i cambiamenti che si verificano a livello cardiaco , nei pazienti affetti da malattia di anderson - fabry e sottoposti a terapia enzimatica sostitutiva . sixteen adult patients ( ten hemizygous men , six heterozygous women ) with genetically confirmed anderson - fabry disease were studied from september 2003 to december 2009 ( mean age 3912 years )  . 
enzyme replacement therapy consisted of intravenous administration of recombinant agalsidase beta ( agalsidase beta , fabrazyme ; genzyme corporation , inc . , cambridge , ma , usa ) at 1 mg / kg body weight every other week . 
 magnetic resonance imaging mri was performed using a 1.5 - t scanner ( gyroscan intera , philips medical system , best , the netherlands ) equipped with a maximum gradient amplitude of 30 mt / m and maximum slew rate of 150 mt / m / ms . 
after acquiring images in the main cardiac planes , t2 - weighted black - blood sequences were acquired at different echo times using a four - chamber view to measure myocardial t2 relaxation time ( mt2rt )  . 
 the following parameters were used : time to repeat ( tr ) / materiali e metodi popolazione dei pazienti sedici pazienti adulti ( 10 uomini emizigoti , 6 donne eterozigoti ) con diagnosi di malattia di anderson - fabry geneticamente confermata , sono stati studiati tra settembre 2003 e dicembre 2009 ( et media : 3912 anni )  . 
tutti i pazienti sono stati sottoposti ad esame di rm cardiaca , prima dellinizio della terapia enzimatica sostitutiva ( studio basale ) e dopo un trattamento di 487 mesi ( range 3860 ; follow - up )  . 
la terapia enzimatica sostitutiva consistita nella somministrazione endovenosa di agalsidase ricombinante ( agalsidase beta , fabrazyme , genzyme corporation , inc . , cambridge , ma ) alla dose di 1 mg / kg di peso corporeo , ogni 2 settimane . 
 tecnica di risonanza magnetica gli esami di risonanza magnetica sono stati eseguiti con uno scanner da 1 , 5 t ( gyroscan intera , philips medical system , best , paesi bassi ) equipaggiato con gradienti con ampiezza massima pari a 30 mt / m e con massimo slew rate pari a 150 mt / m / ms . 
le immagini sono state acqui22 radiol med ( 2012 ) 117 : 1928 effective time to echo ( te ) 1 , 500 / 45 , 60 , 75 , 90 ; matrix 256512 ; field of view ( fov ) 400 mm ; slice thickness 10 mm ; number of slices 3 ; turbo spin - echo ( tse ) factor 23 ; flip angle 90 ; mean scanning time 22 s / slice . 
to measure t2 relaxation time , regions of interest ( roi ) were drawn at the level of the interventricular septum , apex and lateral lv wall and reproduced on the images obtained with the different echo times . 
t2 relaxation time was measured using the following formula : m ( te ) = moe - te / t2 , where te represents echo time and m ( te ) mean of the signal of all rois on the corresponding te image . 
analysis of lv mass and volumes was performed on 2d cine balanced steady - state free precession ( b - ssfp ) images by tracing endocardial and epicardial contours on all end - diastolic and end - systolic sections . 
a significant reduction in the maximum measurable wall thickness was observed between baseline ( 163 mm ) and follow - up ( 133 mm ) ( p < 0.001 ) ( table 2 )  . 
a significant decrease was observed in t2 relaxation site in apnea espiratoria utilizzando una antenna dedicata phased array a 5 canali ; per la sincronizzazione cardiaca stato utilizzato un elettrocardiogramma vettoriale ( vcg )  . 
 dopo aver acquisito i principali piani cardiaci , sono state acquisite sequenze t2 pesate a sangue nero ed a diversi tempi di eco , secondo un piano quattro camere ( 4ch ) per la misurazione del tempo di rilassamento t2 a livello del miocardio ( mt2rt )  . 
sono stati utilizzati i seguenti parametri : tempo di ripetizione ( tr ) / effective tempo di eco ( te ) 1500 / 45 , 60 , 75 , 90 ; matrice 256512 ; campo di vista ( fov ) 400 mm ; spessore di strato 10 mm ; numero di strati 3 ; turbo spin echo ( tse ) factor 23 ; flip angle 90 ; tempo di scansione medio 22 s per ogni strato . 
successivamente sono state acquisite immagini cine 2d balanced turbo field echo multiphase - multislice ( tr / effective te , 2 , 8 / 1 , 4 ; matrice , 160256 ; spessore di strato , 10 mm ; flip angle , 50 ) secondo lasse corto bi - ventricolare coprendo il ventricolo sinistro dalla base verso lapice , per un totale di 1112 sezioni per il calcolo dei volumi e della massa ventricolare sinistra . 
due operatori esperti ( 10 e 6 anni in cardio - rm ) hanno effettuato in sessione congiunta tutte le misurazioni , senza conoscere il timing di studio ( studio basale o studio di follow - up )  . 
per la misurazione del tempo di rilassamento t2 , sono state tracciate regioni di interesse a livello del setto inter - ventricolare , a livello dellapice e della parete laterale del vs e riprodotte sulle diverse immagini ottenute con i diversi tempi di eco . 
il tempo di rilassamento t2 stato calcolato usando la seguente formula m ( te ) = m0e - te / t2 , dove te il tempo di eco e m ( te ) la media del segnale di tutte le regioni di interesse sulla corrispondente immagine te . 
lanalisi dei volumi e della massa ventricolare sinistra stata effettuata sulle immagini 2d cine b - steady - state free - precession ( ssfp ) tracciando i contorni endocardici ed epicardici su tutti gli strati telediastolici e telesistolici . 
 un valore di p < 0 , 05 stato considerato statisticamente radiol med ( 2012 ) 117 : 1928 table 1 patient characteristics [ women ( men ) ] population no . 
 age ( meansd ) men / women cardiovascular risk factors hypertension dyslipidaemia diabetes smoking family history of sudden death bmi ( m2 ; meansd ) sd , standard deviation ; bmi , body mass index popolazione numero et ( mediads ) maschi / femmine fattori di rischio cardiovascolare ipertensione dislipidemia diabete fumo familiarit per morte improvvisa bmi ( m2 ; mediads ) 3912 10 / 6 4 ( 2 ) 2 ( 1 ) 3 ( 2 ) 5 ( 4 ) 3 ( 2 ) 252 3912 10 / 6 4 ( 2 ) 2 ( 1 ) 3 ( 2 ) 5 ( 4 ) 3 ( 2 ) 252 tabella 1 caratteristiche della popolazione . 
una significativa riduzione dei valori di massa del vs stata osservata tra lo studio basale : 18759 g e lo studio di follow - up : 14944 g ( p < 0 , 001 )  . 
una significativa riduzione del massimo spessore di parete misurabile stata osservata tra lo studio basale ( 163 mm ) e lo studio di follow - up ( 133 mm ) ( p < 0 , 001 ) ( tabella 2 )  . 
la maggior parte dei pazienti ( 12 / 16 ) ( p < 0 , 05 ) ha ottenuto nel tempo un miglioramento della classe funzionale nyha ( tabella 2 )  . ds , deviazione standard ; bmi , body mass index discussione time between the two studies ( p < 0.001 ) , regardless of the myocardial region analysed , particularly in the interventricular septum 813 ms vs . 
 most patients ( 12 / 16 ) ( p < 0.05 ) obtained an improvement in nyha functional class over time ( table 2 )  . discussion results of this study confirm the important role of cardiac mri in monitoring patients with anderson - fabry disease receiving enzyme replacement therapy . 
mri demonstrated a significant decline in t2 relaxation time at the level of all myocardial regions and a decrease in the signs of lv hypertrophy , both in terms of maximum measurable thickness and total mass . 
these changes were accompanied by improvements in nyha functional class , even when they were not accompanied by a significant improvement in overall systolic function . i risultati di questo studio confermano un ruolo della rm cardiaca , nel monitoraggio dei pazienti affetti da malattia di anderson - fabry e sottoposti a terapia enzimatica sostitutiva . 
la rm ha dimostrato una significativa riduzione del tempo di rilassamento t2 a livello di tutte le regioni miocardiche ed una regressione dei segni di ipertrofia del vs , sia come spessore massimo misurabile , che come massa totale . 
 la malattia di anderson - fabry una rara malattia genetica dovuta al difetto del gene che codifica per lenzima lisosomiale alfa - galattosidasi a , conosciuto anche come alfa - galattosidasi e triesosidasi ceramide . 
 gli organi maggiormente coinvolti sono il rene , il cuore , la cute , i distretti vascolari , il sistema nervoso autonomo e centrale , locchio e lapparato audio - vestibolare . 
3 valori del tempo di rilassamento t2 ( ms ) allo studio basale e dopo 48 mesi di terapia enzimatica sostitutiva con agalsidase beta , misurati a livello della parete laterale del ventricolo sinistro . radiol med ( 2012 ) 117 : 1928 table 2 ejection fraction , myocardial hypertrophy and new york heart association ( nyha ) functional class indices ef , ejection fraction ; td mass , left ventricular mass during the end - diastolic phase ; max thickness , maximum left ventricular wall thickness measured on the short - axis images during the end - diastolic phase tabella 2 frazione di eiezione , indici di ipertrofia miocardica e classe funzionale secondo la new york heart association ( nyha ) baseline ef ( % ) td mass ( g ) max thickness ( mm ) nyha 1 nyha 2 nyha 3 nyha 4 baseline fe ( % ) massa in td ( g ) spessore massimo ( mm ) nyha 1 nyha 2 nyha 3 nyha 4 653 18759 163 653 18759 163 follow - up ef ( % ) td mass ( g ) max thickness ( mm ) nyha 1 nyha 2 nyha 3 nyha 4 follow - up fe ( % ) massa in td ( g ) spessore massimo ( mm ) nyha 1 nyha 2 nyha 3 nyha 4 642 14944 133 642 14944 133 fe , frazione di eiezione ; massa in td , massa del ventricolo sinistro in tele - diastole ; spessore massimo , spessore massimo parete ventricolare sinistra misurata in tele - diastole sulle immagini ottenute in asse corto fig . 
4 analisi di bland - altman della frazione di eiezione del ventricolo sinistro misurata allo studio basale ed al follow - up , dopo 48 mesi di terapia . anderson - fabry disease is a rare genetic disorder caused by a defect in the gene that encodes the lysosomal enzyme alpha - galactosidase a , also known as alpha - galactosidase or ceramide trihexosidase . 
the most severely involved organs are kidneys , heart , skin , vascular districts , central and autonomic nervous system , eyes and auditory vestibular systechronic renal failure represents the most frequent cause of morbidity , with cardiac involvement being dono le anomalie di conduzione , le malattie valvolari , la cardiopatia ischemica e lipertrofia del miocardio ; proprio questultima manifestazione rappresenta linsidia maggiore per la diagnosi di malattia di anderson - fabry , in quanto , laccumulo di glicosfingolipidi agisce scatenando una vera e propria ipertrofia dei miocardiociti , che risulta indistinguibile dalla hcm alle comuni tecniche diagnostiche ; infatti , possiamo avere una ipertrofia simmetrica o asimmetrica , ostruttiva o non ostruttiva e tutto il corteo fisiopatologico susseguente allipertrofia , come una dilatazione 26 radiol med ( 2012 ) 117 : 1928 the leading cause of death . 
in particular , cardiac manifestations include conduction defects , valvular heart disease , ischaemic heart disease and myocardial hypertrophy ; the latter manifestation is the greatest pitfall in the diagnosis of anderson - fabry disease because the accumulation of glycosphingolipids triggers myocardial cell hypertrophy , which is indistinguishable from hcm on common imaging modalities . 
in fact , hypertrophy may be symmetric or asymmetric , obstructive or nonobstructive and may present with all pathophysiological findings characterising hypertrophy , such as atrial dilatation and diastolic dysfunction resulting from reduced compliance [ 1017 ]  . the differential diagnosis is often difficult in the absence of a detailed and costly genetic analysis , which can in turn be distorted in female patients , who may have an unbalanced inactivation of the x chromosome at the level of the different organs and tissues . 
the difficulty in differentiating anderson - fabry disease from hcm has been emphasised by some authors , who demonstrated that up to 6% of men and up to 12% of women with late - onset hcm were in reality affected by anderson - fabry disease . 
the need for a definite differential diagnosis also derives from the fact that since 2001 , anderson - fabry disease has become potentially treatable by enzyme replacement therapy [ 79 , 18 , 19 ]  . recent reports demonstrate the role of cardiac mri in studying patients with anderson - fabry disease [ 20 , 21 ] and how mri is able to differentiate this disease from other forms of cardiac hypertrophy , especially from hcm , thanks to an analysis of the intramyocardial signal . 
the rationale for signal analysis is based on the assumption that the intensity of the mri signal in the different sequences depends on the chemical and physical features of the tissue being studied . 
as a result of the accumulation of glycosphingolipids in patients with andersonfabry disease , signal analysis shows higher mt2rt values than seen in controls and in hcm patients [ 23 ]  . with replacement therapy , clearance of gb3 deposits is likely to occur , which leads in time to hypertrophy regression , as indicated by results of our study and reported by previous studies [ 24 , 25 ] , and to a decline in t2 relaxation times [ 26 ]  . 
 [ 24 ] , but in contrast with the results reported by kovacevic - preradovic et al . , who observed no significant decline in indices of myocardial hypertrophy [ 27 ]  . 
however , it should be noted that in this latter study , the indices of lv hypertrophy measured at baseline were not as high as they were in our patients . in our study , consistent with previous studies , the decline atriale ed una disfunzione diastolica da ridotta compliance [ 1017 ]  . la diagnosi differenziale spesso difficile senza ricorrere ad una dettagliata e costosa analisi genetica che peraltro pu essere falsata nei soggetti di sesso femminile che possono avere una inattivazione sbilanciata del cromosoma x a livello dei differenti organi e tessuti ; le difficolt di differenziare la malattia di anderson - fabry dalla hcm sono messe in risalto da alcuni articoli che hanno dimostrato come fino al 6% degli uomini e fino al 12% delle donne con insorgenza tardiva di hcm , erano in realt affetti da malattia di anderson - fabry . 
il dover effettuare una diagnosi differenziale certa deriva anche dal fatto che dal 2001 la malattia di anderson - fabry diventata un disordine potenzialmente trattabile , con la terapia enzimatica sostitutiva [ 79 , 18 , 19 ]  . recenti studi hanno dimostrato il ruolo della rm cardiaca nella valutazione dei pazienti con malattia di anderson - fabry [ 20 , 21 ] e come sia in grado di differenziare tale patologia da altre forme di ipertrofia cardiaca ed in particolare dalla hcm , grazie ad una analisi del segnale intra - miocardico . 
il razionale dellanalisi del segnale si basa sul presupposto che lintensit ottenuta in rm nelle differenti sequenze dipende dalla caratteristiche chimico - fisiche del tessuto in analisi ; infatti noto che nelle sequenze t2 pesate , il tempo di rilassamento t2 aumenta con laumentare del contenuto di lipidi e di acqua dei tessuti in esame [ 22 ]  . 
nei pazienti affetti da malattia di andersonfabry , proprio a causa dellaccumulo dei glicosfingolipidi , lanalisi del segnale mostra dei valori di mt2rt superiori al gruppo di pazienti di controllo e superiori al gruppo di pazienti affetti da hcm [ 23 ]  . con la terapia sostitutiva verosimile che vi sia una clearance dei depositi di gb3 che porta nel tempo ad una regressione dellipertrofia , come si evince dai risultati del nostro studio , in linea con studi precedenti [ 24 , 25 ] e ad una riduzione dei tempi di rilassamento t2 [ 26 ]  . 
in questo studio , la riduzione del tempo di rilassamento t2 , va di pari passo con una significativa riduzione della massa totale e degli spessori massimi di parete del vs . 
 [ 27 ] che non hanno osservato una riduzione significativa degli indici di ipertrofia miocardica ; dobbiamo per puntualizzare che in tale ultimo lavoro , gli indici di ipertrofia ventricolare sinistra allo studio basale , non erano elevati come nel nostro studio . nel presente lavoro , cos come in precedenti studi , con la riduzione del tempo di rilassamento t2 e con la riduzione della massa totale e degli spessori massimi di parete del miocardio , non stato osservato un significativo miglioramento della funzione sistolica globale . 
in realt , i pazienti radiol med ( 2012 ) 117 : 1928 in t2 relaxation time and the decrease in total mass and maximum myocardial wall thickness did not lead to a significant improvement in overall systolic function . 
in fact , patients with anderson - fabry disease and those with hcm both have a predominantly diastolic rather than systolic dysfunction , as the overall systolic function is preserved until the terminal stage of the disease . 
 [ 27 ] however , patients in the latter study were starting from a lower nyha class and had a less severe degree of hypertrophy at baseline than did our patients . limitations the potential limitations of our study are the lack of correlation with histopathological data , the limited number of patients and the lack of a control group of untreated patients . 
 affetti da malattia di anderson - fabry , cos come quelli affetti da hcm , hanno prevalentemente una disfunzione diastolica piuttosto che una disfunzione sistolica , essendo la funzione sistolica globale conservata fino agli stadi terminali della malattia . 
 [ 27 ] , tuttavia , tali pazienti partivano da una classe nyha inferiore ed avevano gradi di ipertrofia meno severi gi allo studio basale . limiti potenziali limiti del nostro studio sono rappresentati dalla mancanza della correlazione con dati isto - patologici , dalla ridotta numerosit del campione e dalla mancanza di un gruppo di controllo di pazienti non sottoposti a terapia enzimatica sostitutiva ; tuttavia , abbiamo ritenuto non etico negare la terapia enzimatica ad un sotto - gruppo di pazienti con malattia di anderson - fabry . 
 conclusioni conclusions results of our study confirm the usefulness of cardiac mri in monitoring the response to enzyme replacement therapy with agalsidase beta ; a decline in t2 relaxation time was identified , together with a decrease in maximum myocardial thickness and total lv mass . 
further studies are needed to monitor long - term effects of enzyme replacement therapy on diastolic function . i risultati di questo studio confermano lutilit della rm cardiaca nel monitorare la risposta alla terapia enzimatica sostitutiva con agalsidase beta , identificando una riduzione del tempo di decadimento t2 , una riduzione degli spessori miocardici massimi e della massa totale del vs . 
gemelli , roma , italy 3dipartimento di ortopedia , ospedale ramazzini , carpi , italy 4dipartimento di ortopedia , ospedale san camillo , forte dei marmi , italy correspondence to : n . 
la concordanza tra misurazioni tc 2d ( mpr ) e 3d ( vrt ) nellidentificare le dimensioni ed il tipo di difetto osseo di glena nellinstabilit glenoomerale anteriore stata cos alta da poterle considerare intercambiabili . radiol med ( 2012 ) 117 : 102111 keywords shoulder instability glenoid bone defect computed tomography parole chiave spalla instabilit glena difetto osseo tomografia computerizzata introduction introduzione glenoid - bone defect is considered one of the factors that most affect glenohumeral stability [ 15 ]  . 
several clinical studies have reported that recurrence of shoulder dislocation after surgical treatment is frequently associated with glenoid - bone defects and that the correlation between recurrence rate and percentage of glenoid - bone loss is clinically relevant [ 610 ]  . 
based on these results , the most recent guidelines for treating shoulder instability consider arthroscopic capsular repair as contraindicated and recommend open procedures , with bone reconstruction or augmentation when major glenoid - bone loss is present [ 11 , 12 ]  . several imaging techniques to measure the presence and size of a glenoid defect are described in the literature [ 1319 ]  . 
in particular , many authors report on the use of computed tomography ( ct ) to identify size , location and type ( fracture or erosion ) of glenoid defect associated with glenohumeral instability using 3d volume - rendering ( vr ) scans [ 1923 ] or 2d multiplanar reconstruction ( mpr ) [ 14 , 2427 ]  . 
the missing portion of the glenoid on ct scans can be calculated as a percentage of the area of the inferior glenoid ( circle method ) [ 15 , 19 , 24 ] or as a percentage of the maximum width of the glenoid [ 14 , 21 , 25 , 26 ]  . 
 patient selection one hundred patients who accepted our invitation to enter il difetto osseo glenoideo attualmente considerato uno dei principali fattori che inficiano la stabilit gleno - omerale [ 15 ]  . 
diversi studi clinici hanno riportato che la dislocazione ricorrente di spalla dopo trattamento chirurgico frequentemente associata con il difetto osseo glenoideo e che la correlazione tra entit di recidiva e percentuale del difetto osseo clinicamente rilevante [ 610 ]  . 
sulla ba se di questi risultati , le pi recenti linee guida sul trattamento dellinstabilit di spalla considerano la capsuloplastica artroscopica controindicata e raccomandano le tecniche a cielo aperto attraverso la ricostruzione ossea o laumento della superficie ossea in caso di difetti maggiori [ 11 , 12 ]  . differenti modalit di imaging impiegate per misurare la presenza e la dimensione del difetto osseo sono state descritte in letteratura [ 1319 ]  . 
in particolare , molti autori hanno riportato luso della tomografia computerizzata ( tc ) al fine di stabilire dimensioni , sede e tipo ( frattura o erosione ) del difetto glenoideo associato con linstabilit gleno - omerale utilizzando ricostruzioni tridimensionali ( 3d ) volume rendering technique ( vrt ) [ 15 , 1923 ] , o bidimensionali ( 2d ) multi - planar reconstruction ( mpr ) [ 14 , 2427 ]  . 
la porzione mancante della glena misurata sulle acquisizioni tc pu essere calcolata come percentuale dellarea della glena inferiore ( metodo del cerchio ) [ 15 , 19 , 24 ] , o percentuale dellampiezza massima della glena [ 14 , 21 , 25 , 26 ]  . 
 ct examination technique all patients underwent a ct scan of both shoulders with a spiral multislice ct ( lightspeed pro16 ; ge healthcare , milwaukee , wi , usa ) using filter for bone , 1.25 - mm slice thickness with reconstruction interval 0.6 mm , 200300 ma , 120 kv , field of view ( fov ) 30 cm and matrix 512512 pixels . 
images were processed on a commercially available workstation ( advantage , version 4.2 ; ge healthcare ) in mpr according to oblique sagittal planes and maintaining working axes parallel to the glenoid surface to obtain oblique sagittal images of the glenoid articular surface ( en face view )  . 
the size of the defect was expressed as a percentage of the entire circle , according to the following formula , already reported in previous studies [ 15 , 19 , 24 ] : [ ( area d / area a ) 100 ] the same scans were then processed using vr for 3d reconstruction of the glenoid . 
each examiner was blind to the results of the other measurement series . data analysis sample size calculation was based on the primary outcome ( agreement between the two measurements for quantification of glenoid - bone loss )  . 
according to estimates provided danza tra le due misurazioni nel valutare la presenza del difetto glenoideo e nel discriminare il tipo di difetto osseo ( erosione o frattura )  . selezione dei pazienti per il presente studio sono stati arruolati 100 pazienti , previo consenso informato . 
i criteri di esclusione sono stati : soggetti che presentavano instabilit di spalla controlaterale e precedenti fratture e / o interventi chirurgici ad entrambe le spalle . tecnica tc tutti i pazienti sono stati sottoposti ad esame tc delle spalle in comparativa utilizzando apparecchio tc spirale multidetettore ( lightspeed pro16 , ge healthcare , milwaukee , wi ) , usando filtro bone , strati dello spessore di 1 , 25 mm , con intervallo di ricostruzione di 0 , 6 mm , 200300 ma , 120 kv , campo di vista ( fov ) di 30 cm e matrice di 512512 pixel . 
le immagini sono state rielaborate con workstation ( advantage , version 4.2 , ge healthcare ) in mpr secondo piani sagittali obliqui mantenendo lasse parallelo alla superficie glenoidea , in modo da ottenere immagini sagittali della superficie articolare della glena ( en face view )  . 
le dimensioni del difetto sono state espresse come percentuale dellintero cerchio secondo la seguente formula , gi riportata nei precedenti studi [ 15 , 19 , 24 ] : [ ( area d / area a ) 100 ] le stesse acquisizioni sono state poi elaborate secondo ricostruzioni vrt 3d della glena . 
dopo aver eliminato la testa omerale durante la rielaborazione dellimmagine , sono state ottenute le proiezioni en face di entrambe le glene ed stata calcolata la dimensione del difetto osseo utiradiol med ( 2012 ) 117 : 102111 fig . 
b misurazione della porzione mancante della glena sulla spalla destra affetta . by bland [ 28 ] , a sample size of 100 gives a 95% confidence interval ( ci ) of limits of agreement about 0.34 s , ( s = standard deviation of the differences between the two measurements )  . 
according to this method , we calculated the difference between measurements of glenoid - bone defect obtained with the two methods and the mean of the two measurements ; we then calculated mean ( d ) and standard deviation ( s ) of the differences . 
data were reported in a scatter plot of differences ( y - axis ) against means ( x - axis ) , where upper and lower limits of agreement were considered as d2 s . 
 evaluation of agreement between the two methods in discriminating the type of glenoid - bone defect was performed considering three categories ( defect absent , bony bankart lesion and bone erosion ) and calculating percent agreement . 
 bony bankart lesion was determined by observing the presence of anterior glenoid fracture , with a free bone fragment adjacent to the glenoid rim or reattached medially on the glenoid neck . 
analysis of agreement between the two measurements in discriminating the type of glenoid - bone defect ( table 2 ) showed a highly siganalisi dei dati il calcolo delle dimensioni del campione stato basato sullo scopo principale ( concordanza tra le due misurazioni nella quantificazione della perdita ossea glenoidea )  . 
secondo le stime stabilite da bland [ 28 ] , una numerosit di 100 del campione d un 95% dellintervallo di confidenza ( ci ) dei limiti di concordanza di circa 0 , 34 s ( dove s = deviazione standard di differenze tra due misurazioni )  . 
il metodo bland - altman stato usato per valutare la concordanza tra le misurazioni ottenute con le ricostruzioni mpr e vrt per la quantificazione del difetto osseo di glena [ 29 ]  . 
secondo questo metodo , noi abbiamo calcolato per ogni paziente la differenza tra le misurazioni del difetto osseo di glena ottenute con i due metodi e la media delle due misure ; poi abbiamo calcolato media ( d ) e deviazione standard ( s ) delle differenze . 
i dati sono stati riportati in uno scatter plot delle differenze ( asse y ) sulle medie ( asse x ) , dove il limite superiore ed inferiore della concordanza stato considerato come d2s . 
la valutazione di concordanza tra i due metodi nel discriminare il tipo di difetto osseo stata eseguita considerando tre categorie ( assenza di difetto , lesione bony bankart ed erosione ossea ) e calcolando la percentuale di concordanza . 
la differenza media stata dello 0 , 62% ( linea tratteggiata centrale ) ; i limiti della concordanza erano entro il 95% e compresi tra 4 , 54% e 3 , 30% ( linee tratteggiate superiore ed inferiore ) , indicando unottima concordanza tra le due misurazioni . nificant association ( p < 0.0001 ) , with a percent agreement of 97% , and weighted coefficient equal to 0.97. discussion different ways of identifying and measuring glenoid - bone defect have been described in the literature by using preoperative imaging techniques or intraoperative arthroscopic methods [ 1 , 1317 , 19 , 30 ]  . 
arthroscopic measurement of the glenoid bone defect is based on the use of the glenoid bare spot as a landmark of the centre of the inferior glenoid [ 1 , 31 ]  . 
quantification of the defect is achieved by calculating the difference between posterior and anterior radius of the inferior glenoid and the ratio between this difference and the diameter of the intact glenoid ( equal to posterior radius 2 ) [ 1 ]  . 
however , some authors have shown that the bare spot is not exactly in the centre of the inferior glenoid [ 3234 ] and is not always recognisable [ 18 ]  . 
 [ 35 ] observed in a cadaver study that bone loss measurement with the bare - spot method can overestimate the area of the missing glenoid , especially for small defects . 
finally , it must be considered that the presence and size of a glenoid defect can influence the choice of surgical procedure , so that a preoperative assessment would be more valuable . 
il 95% ci dei limiti di concordanza erano compresi tra 5 , 1% e 3 , 98% e tra - 3 , 86% e - 2 , 74% per il limite superiore ed inferiore , rispettivamente . lanalisi della concordanza tra le misurazioni mpr e vrt nellidentificare la presenza del difetto osseo glenoideo ( tabella 1 ) ha mostrato una associazione altamente significativa tra i due metodi ( p < 0 , 0001 ) , con una concordanza percentuale del 97% , ed un coefficiente uguale a 0 , 90 . 
lanalisi della concordanza tra le due misurazioni nella discriminazione del tipo di difetto glenoideo ( tabella 2 ) ha mostrato una associazione altamente significativa ( p < 0 , 0001 ) , con una concordanza percentuale del 97% , ed un coefficiente pesato uguale a 0 , 97 . discussione differenti metodi per identificare e misurare le dimensioni del difetto osseo di glena sono stati descritti in letteratura , utilizzando metodiche di imaging preoperatorio o metodi artroscopici intraoperatori [ 1 , 1317 , 19 , 30 ]  . 
la quantificazione del difetto stabilita radiol med ( 2012 ) 117 : 102111 calcolando la differenza tra il raggio anteriore e posteriore della glena inferiore ed il rapporto tra questa differenza ed il diametro della glena intatta ( uguale al raggio posteriore2 ) [ 1 ]  . 
 [ 35 ] hanno osservato in uno studio su cadavere che la misurazione della perdita ossea con il metodo del bare spot pu sovrastimare larea della glena mancante , soprattutto per difetti piccoli . 
infine , bisogna considerare che la presenza e le dimensioni del difetto glenoideo possono influenzare la scelta della procedura chirurgica , cosa che implica che la valutazione preoperatoria dovrebbe essere pi precisa . 
alcuni autori hanno studiato luso di esami radiografici per diagnosticare un difetto glenoideo nellinstabilit anteriore di spalla , ma nessuno di questi metodi stato testato per valutarne la riproducibilit e laccuratezza nel quantificare la perdita ossea [ 7 , 13 , 17 , 30 ]  . limaging con risonanza magnetica ( rm ) considerato la prima opzione nella valutazione del danno dei tessuti molli nellinstabilit di spalla ; comunque , uno scarso numero di studi ha riconosciuto la sua utilit nel diagnosticare difetti ossei di glena [ 15 , 36 , 37 ]  . 
di contro , molti autori hanno riportato luso della tc , sia con ricostruzioni 3d ( vrt ) che 2d ( mpr ) , come la modalit di scelta nellindividuare anomalie ossee nella instabilit gleno - omerale [ 14 , 1923 , 25 , 26 , 38 ]  . 
it is based on the observation that the inferior part of the glenoid has the shape of a true circle , which can be drawn on the sagittal en face view of the glenoid [ 19 , 33 , 39 ]  . 
 [ 15 ] validated the method on 14 cadaver shoulders , showing a very good intraobserver and interobserver reliability and accuracy , although the limited number of samples analysed weakened the clinical relevance of the results . 
 [ 24 ] , combines the advantages of the circle method ( measurement of the missing area of the glenoid as percentage of the entire inferior glenoid ) with those of the mpr technique ( neither 3d reconstructions nor subtractions of images are required )  . 
 [ 14 , 25 , 26 ] , is the comparison with the contralateral shoulder , so that it cannot be applied to patients with bilateral instability . results of our study showed very good agreement between 2d ( pico method ) and 3d measurements for quantifying , identifying and discriminating the type of defect ( bone erosion or fracture )  . 
based on these results , we considered 2d superimposable to 3d scans . un metodo per la misurazione del difetto glenoideo osseo su ricostruzioni tc 3d simile a quello di griffith et al . 
entrambi i metodi sono stati validati per accuratezza utilizzando la misurazione artroscopica come tecnica di riferimento [ 21 , 26 ] ; tuttavia laccuratezza della misurazione artroscopica non stata mai stabilita in studi precedenti . 
questo metodo basato sullosservazione che la parte inferiore della glena ha la forma di un cerchio , che pu essere tracciato sulla immagine en face della glena [ 19 , 33 , 39 ]  . 
 [ 15 ] hanno validato il metodo studiando 14 spalle di cadaveri , mostrando unottima riproducibilit intra - osservatore ed inter - osservatore ed unottima accuratezza , sebbene il limitato numero di campioni analizzati indeboliva la rilevanza clinica dei risultati . 
 [ 24 ] , unisce i vantaggi del metodo del cerchio ( misurazione dellarea mancante della glena come percentuale dellintera glena inferiore ) con quelli della tecnica mpr ( non sono richieste ricostruzioni 3d , n sottrazioni di immagini )  . 
 [ 14 , 25 , 26 ] , il confronto con la spalla controlaterale , cos che non pu essere applicato a pazienti con instabilit bilaterale . i risultati del presente studio hanno dimostrato unottima concordanza tra le misurazioni 2d ( metodo pico ) e 3d per la quantificazione , lidentificazione e la discriminazione del tipo di difetto ( erosione ossea o frattura )  . 
in particolare , la differenza media tra le 2d e le 3d stata positiva , cos che sembrato che le 2d sovrastimassero le dimensioni del difetto osseo in confronto con le 3d . 
second , although ct scans would allow for the assessment of location and size ( length and width ) of the bone defect , this evaluation was not performed , because the main objective of the study was to assess agreement between 2d and 3d measurements in evaluating the size of the defect by measuring the area of the missing glenoid according to the circle method , as previously reported by other authors [ 15 , 19 , 24 , 27 ]  . 
 therefore , measuring the size of bone defect by using a different method lies beyond the scope of our study and would impair data comparability with those from previous reports . 
finally , the pico method could be theoretically used without comparison with the contralateral shoulder , as described in other studies based on the circle method [ 15 , 19 ] , although this hypothesis was not tested in the study presented here . za delle misurazioni tc , poich non avevamo un reale gold standard . 
in secondo luogo , sebbene le acquisizioni tc potessero consentire una valutazione della sede e delle misure ( lunghezza e larghezza ) del difetto , questa valutazione non stata effettuata , poich il principale obiettivo del presente studio stato stabilire la concordanza tra le misurazioni 2d e 3d nel valutare le dimensioni del difetto misurando larea della glena mancante in accordo con il metodo del cerchio , come precedentemente riportato da altri autori [ 15 , 19 , 24 , 27 ]  . 
di conseguenza , misurare le dimensioni del difetto osseo con un metodo differente oltre lo scopo del presente studio , e inficerebbe la comparabilit dei nostri risultati con quelli della letteratura precedente . 
sardanelli1 , 4 1servizio di radiologia , 2unit di chirurgia dellanca , irccs policlinico san donato , via morandi 30 , 20097 san donato milanese , milano , italy 3scuola di specializzazione in radiodiagnostica , facolt di medicina e chirurgia , universit degli studi di milano , via festa del perdono 7 , 20122 milano , italy 4dipartimento di scienze medico - chirurgiche , universit degli studi di milano , via morandi 30 , 20097 san donato milanese , milano , italy correspondence to : a . 
images were reviewed blindly by two musculoskeletal radiologists with different levels of experience who evaluated the presence / absence of soft tissue oedema or fluid collection ( when present , three - plane maximal diameters were measured ; involvement of skin / subcutaneous / deep tissues or prosthesis were estimated ; fluid was classified as serous / purulent / haematic according to signal behaviour )  . 
le immagini sono state riviste in cieco da due radiologi con differente esperienza in radiologia scheletrica che hanno valutato la presenza / assenza di edema dei tessuti molli o di una raccolta periprotesica . 
in presenza di raccolta , sono stati misurati i tre diametri maggiori , stato stimato il coinvolgimento della cute / sottocute / tessuti molli o della protesi ; la raccolta stata caratterizzata come sierosa / purulenta / ematica in base al comportamento del segnale . 
entrambi i lettori hanno riscontrato edema dei tessuti molli ( 13 / 26 , 50% ) o raccolte fluide ( 21 / 26 , 81% ) ed hanno caratterizzato la raccolta fluida come sierosa ( 9 / 21 , 43% ) , purulenta ( 8 / 21 , 38% ) o ematica ( 4 / 21 , 19% )  . 
la raccolta coinvolgeva cute / sottocute ( 16 / 21 , 76% ) , i tessuti 86 radiol med ( 2012 ) 117 : 8595 evaluations , interobserver agreement was complete ( = 1 )  . 
mri is highly reproducible in detection , localisation , quantification , and characterisation of fluid collections when the presence of implant infection is clinically suspected . keywords magnetic resonance imaging total hip arthroplasty infection fluid collection interobserver reproducibility molli profondi ( 19 / 21 , 91% ) o la protesi ( 12 / 21 , 57% )  . 
la rm una modalit diagnostica altamente riproducibile per riconoscere , localizzare , quantificare e caratterizzare raccolte fluide periprotesiche quando linfezione sospettata clinicamente . parole chiave risonanza magnetica protesi danca infezione raccolta fluida riproducibilit interosservatore introduction introduzione total hip arthroplasty ( tha ) is a widely accepted option for treating patients affected by symptomatic ficatarlet stage iii and iv osteonecrosis of the femoral head and by hip osteoarthritis [ 1 ]  . 
blood tests usually show a nonspecific increase of erythrocyte sedimentation rate ( esr ) and c - reactive protein ( crp ) , as well as neutrophil leukocytosis [ 4 ]  . 
ultrasonography ( us ) is effective in assessing superficial fluid collections but is limited by a low interobserver reproducibility ; in this setting , its diagnostic value is also limited by the deep implant location [ 5 ]  . 
nuclear imaging is the only modality not affected by the presence of an implant ; leukocyte / marrow imaging is the procedure of choice for diagnosing periimplant infection [ 4 , 9 ]  . 
this procedure is reported to have a sensitivity ranging from 28% to 92% and a specificity ranging from 92% to 100% [ 3 , 9 ]  . to date , articular implants do not represent an absolute contraindication to magnetic resonance imaging ( mri )  . 
 among the various sequences , turbo spin - echo ( tse ) and short - tau inversion recovery ( stir ) sequences are affected lartroprotesi danca unopzione attualmente largamente accettata per il trattamento di pazienti sintomatici affetti da osteonecrosi della testa femorale in stadio iii - iv secondo ficat - arlet o da artrosi dellanca [ 1 ]  . 
questa procedura pu essere complicata da infezione in fase precoce o tardiva in circa lo 0 , 5%2% dei casi [ 2 ] , condizione che rappresenta tuttoggi una sfida diagnostica non irrilevante [ 2 ]  . 
 lesame clinico pu essere utile , ma deve essere integrato da ulteriori indagini [ 3 ] , come test ematochimici ( che generalmente mostrano un incremento aspecifico della velocit di eritrosedimentazione , della proteina c - reattiva e leucocitosi neutrofila ) [ 4 ]  . 
lecografia utile nella valutazione delle raccolte superficiali , ma caratterizzata da scarsa riproducibilit interosservatore ; inoltre in questo contesto clinico altres limitata dalla sede profonda dellimpianto protesico [ 5 ]  . 
recenti avanzamenti tecnologici hanno ridotto lentit degli artefatti da protesi metallica in tomografia computerizzata [ 6 , 7 ] sebbene , tali artefatti influenzino in misura sostanziale la qualit delle immagini , in particolare in prossimit dellimpianto , ossia nella pi probabile sede delle raccolte . 
limaging nucleare la sola modalit diagnostica non influenzata negativamente dalla presenza della protesi ; la scintigrafia con leucociti marcati la procedura di scelta per la diagnosi di infezione periprotesica [ 4 , 9 ]  . 
infine , lo standard di riferimento per la diagnosi di infezione periprotesica lagoaspirazione della raccolta con coltura batterica , anche se il range riportato per la sensibilit tra il 28% e il 92% mentre quello per la specificit tra 92% e il 100% [ 3 , 9 ]  . attualmente le protesi articolari non rappresentano una controindicazione assoluta alla risonanza magnetica ( rm )  . 
 although numerous papers has investigated the diagnostic performance of mri in assessing total hip replacement [ 11 , 12 ] , few have focused on evaluating periprosthetic fluid collections [ 13 ]  . 
the purpose of our study was to demonstrate the diagnostic value of mri in measuring and characterising periprosthetic fluid collection in patients with tha and providing an estimation of interobserver reproducibility . materials and methods patients and imaging protocol institutional review board approval and patients informed consent were obtained . 
from january 2008 to april 2010 , 19 patients [ ten men , nine women ; age range 3680 years , age 5913 years ( meanstandard deviation ) ] , who underwent tha with a titanium alloy implant ( zweymuller ; alloclassic hip , zimmer , warsaw , in , usa ) and with clinical suspicion of local infection were prospectively studied with mri of the implanted hip . 
for each patient , clinical signs ( temperature , local pain , swelling , skin redness and heat , pus discharge ) and blood test results ( esr and crp ) were recorded . 
when a periprosthetic fluid collection was detected , the patient underwent us - guided aspiration as the reference standard for fluid characterisation . image analysis images were independently evaluated by two radiologists with 3 and 10 years of experience in musculoskeletal mri who were blinded to patients clinical and laboratory data . 
moreover , both observers performed a qualitative analysis by assessing the following items : involvement of skin / subcutaneous / deep tissues or prosin considerazione degli artefatti da suscettibilit magnetica da esse determinati [ 8 ] , sono definite come fattori potenzialmente limitanti la diagnosi con rm . 
tra le varie sequenze di impulsi , le sequenze turbo spin - echo ( tse ) e short - tau inversion recovery ( stir ) sono risultate gravate da artefatti di minore entit rispetto alle sequenze con struttura ad eco di gradiente [ 10 ]  . sebbene la performance diagnostica della rm nella valutazione dellartroprotesi danca sia gi stata oggetto di studio nella letteratura [ 11 , 12 ] , raramente si sono valutate le raccolte fluide periprotesiche [ 13 ]  . 
scopo del presente studio stato quindi valutare la capacit della rm di misurare e caratterizzare le raccolte fluide periprotesiche in pazienti con artroprotesi danca , stimandone altres la variabilit interosservatore . 
da gennaio 2008 ad aprile 2010 , sono stati studiati prospetticamente con rm 19 pazienti ( 10 maschi , 9 femmine ; et tra 36 e 80 anni , mediadeviazione standard 5913 anni , mediana 59 anni ) che erano stati sottoposti ad artroprotesi danca con impianto in lega al titanio ( zwueymueller ; alloclassic hip , zimmer , warsaw , in , usa ) e per i quali sussisteva sospetto clinico di infezione locale . 
 tutte le indagini sono state effettuate con apparecchiatura rm operante a 1 , 5 t ( sonata maestro class , siemens , erlangen , germania ) e bobina phased - array body a 2 canali . 
per ciascun paziente sono stati registrati la condizione clinica ( temperatura corporea generale , dolore locale , tumefazione , arrossamento cutaneo e incremento locale della temperatura , fuoriuscita di materiale purulento ) e il risultato dei test ematochimici ( velocit di eritrosedimentazione e proteina c - reattiva )  . 
in tutti i casi nei quali stata diagnostica con rm una raccolta fluida periprotesica , stata eseguita agoaspirazione ecoguidata con valutazione microbiologica , quale standard di riferimento per la caratterizzazione della raccolta . 
 analisi delle immagini thesis ; presence of a fistula ; le immagini rm sono state valutate indipendentemente da due radiologi con tre e dieci anni di esperienza in rm 88 sequence table 1 technical parameters of sequences . 
il numero di strati stato variato in base alle dimensioni del paziente sequenza tr ( ms ) te ( ms ) flip angle spessore di strato ( mm ) fov ( mm ) matrice larghezza di banda ( hz / pixel ) tse t1 - pesata assiale e coronale tse t2 - pesata assiale e sagittale stir assiale e coronalea 600 4150 500 7 , 8 114 , 0 21 , 0 150 150 150 5 mm 5 mm 5 mm 400 380 400 240320 195 230384 150 230256 130 tr , tempo di ripetizione ; te , tempo di eco ; fov , field of view ; tse , turbo spin - echo ; stir , short tau inversion - recovery . 
 atempo di interpulso = 130 ms presence of soft tissue oedema ; nature of the collection considering joint aspiration as standard of reference ; fluid signal was rated as follows : serous , when showing hypointensity on t1 - weighted and hyperintensity on t2 - weighted and stir sequences ; purulent , when showing inhomogeneous and weak hyperintense signal on t1 - weighted and hyperintense signal on t2 - weighted and stir sequences ; haematic , when showing hyperintense signal on t1 - weighted and inhomogeneous hyperintense signal on t2 - weighted and stir sequences [ 14 ]  . statistical analysis measurements obtained by the two observers were compared using the wilcoxon signed - rank test . 
using cohen statistics , mri fluid characterisation obtained by the two observers were compared each other to estimate interobserver reproducibility and with the outcome of us - guided aspiration to evaluate accuracy . results muscoloscheletrica , con modalit in cieco rispetto alla storia clinica e ai risultati di laboratorio . 
entrambi i lettori hanno valutato la possibile presenza di una raccolta periprotesica e , quando presente , hanno determinato con calibro elettronico la dimensione massima in proiezione antero - posteriore , cranio - caudale e latero - laterale . 
inoltre , entrambi i lettori hanno effettuato una analisi qualitativa relativa a : interessamento della cute , del sottocutaneo , dei tessuti profondi , o della stessa protesi ; presenza di tramiti fistolosi ; presenza di edema dei tessuti molli ; natura della raccolta ( con riferimento allesito dellanalisi citologica dellagoaspirazione ecoguidata come standard di riferimento ) ; il segnale della raccolta stato valutato come segue : sieroso in presenza di ipointensit nelle immagini pesate in t1 e iperintensit nelle immagini pesate in t2 e alla stir ; purulento , in presenza di segnale disomogeneo e debolmente iperintenso nelle immagini pesate in t1 , disomogeneo e iperintenso nelle immagini pesate in t2 e alla sequenza stir ; ematico , in presenza di segnale iperintenso nelle immagini pesate in t1 e disomogeneamente iperintenso nelle immagini pesate in t2 e alla stir [ 14 ]  . acquisition time was about 20 min , plus 35 min for patient positioning , initial scout sequences and patient removal from the mri scanner . 
no patient reported pain , heat or other local or general discomfort either during the examination or during the following 30 m on the day of mri examination , body temperature > 37c was present analisi statistica le dimensioni misurate dai due lettori sono state compra te con il test di wilcoxon . 
 angiography revealed leakage from a small collateral branch of the inferior gluteal artery that was successfully embolised . data on size measurements of the periprosthetic fluid collections are reported in table 2 . 
infection is dellagoaspirazione ecoguidata sono state valutate me diante di cohen . risultati il tempo di acquisizione dello studio rm stato di circa 20 minuti , al quale si aggiungono circa 35 minuti per il posizionamento del paziente , le sequenze di centratura , la rimozione delle bobine e la discesa del paziente dal lettino . 
il giorno dellindagine rm , stata rilevata una temperatura corporea > 37c in 15 / 26 casi ( 58% ) ; dolore locale in 23 / 26 casi ( 88% ) ; tumefazione , rossore o calore in sede cutanea in 24 / 26 casi ( 92% ) ; fuoriuscita di materiale purulento in 6 / 26 casi ( 23% )  . 
langiografia ha rivelato lorigine dellematoma da un piccolo ramo collaterale dellarteria glutea inferiore , embolizzato con successo . 90 radiol med ( 2012 ) 117 : 8595 table 3 results of the qualitative analysis . 
per tutte le osservazioni , la riproducibilit interosservatore stata completa ( di cohen = 1 ) finding ratio , n ( % ) reperto rapporto , n ( % ) presence of soft tissue oedema presence of periprosthetic fluid collection involvement of skin / subcutaneous tissues deep soft tissues prosthesis presence of a fistula nature of collection serous purulent haematic 13 / 26 ( 50 ) 21 / 26 ( 81 ) 18 / 21 ( 86 ) 19 / 21 ( 90 ) 17 / 21 ( 81 ) 13 / 21 ( 62 ) 10 / 21 ( 48 ) 8 / 21 ( 38 ) 3 / 21 ( 14 ) edema dei tessuti molli raccolta periprotesica coinvolgimento di cute / sottocute tessuti molli profondi protesi fistola cutanea contenuto della raccolta sierosa purulenta ematica 13 / 26 ( 50 ) 21 / 26 ( 81 ) 18 / 21 ( 86 ) 19 / 21 ( 90 ) 17 / 21 ( 81 ) 13 / 21 ( 62 ) 10 / 21 ( 48 ) 8 / 21 ( 38 ) 3 / 21 ( 14 ) a relatively uncommon event after tha , reported in about 1% of cases [ 16 ] , with the majority of infections occurring later than 3 months after surgery , although this complication can be seen also at earlier stages [ 17 ]  . 
such a procedure involves a first stage in which the infected prosthesis is replaced with an interim spacer , and a second delayed stage in which a new prosthesis is implanted only i risultati relative alla misurazione delle dimensioni della raccolta periprotesica sono riportati in tabella 2 , senza differenze significative tra i due lettori . 
linfezione dopo artroprotesi danca evento relativamente raro , riportato in circa l1% dei casi [ 16 ] , per lo pi oltre tre mesi dopo lintervento , sebbene questa complicanza possa insorgere anche precocemente [ 17 ]  . 
in tal caso , la ricostruzione in due fasi la procedura di trattamento pi frequente : nella prima fase la protesi infetta sostituita con uno spaziatore temporaneo mentre nella seconda fase , solo quando i segni di infezione locale sono scomparsi , si procede allimpianto di una nuova protesi [ 18 ]  . 
 sebbene la scintigrafia ossea possa essere utile per lo screening , la scintigrafia con leucociti marcati rimane la procedura di scelta per la diagnosi di infezione [ 4 ] , anche se la sua capacit di quantificare precisamente la raccolta non ottimale . 
b pi posteriormente visibile una fistola ( teste di freccia ) , che pu essere seguita lungo tutto il suo decorso fino alla cute . si richiedono indagini ripetute nel tempo . 
si consideri tuttavia che le protesi oggi in uso sono costruite con leghe metalliche ad elevato contenuto di titanio , condizione che , insieme allutilizzo di sequenze opportune , riduce gli artefatti da suscettivit magnetica . 
importanti sviluppi tecnologici sono in corso relativamente al disegno di sequenze rm che riducano marcatamente le dimensioni degli artefatti da protesi ortopediche metalliche nellimaging clinico , quali ad esempio le sequenze con codifica di fase accelerata [ 19 ]  . 
questo approccio , combinato con treni di echi standard , imaging parallelo , partial fourier imaging e tecniche inversion - recovery , si dimostrato efficace nella correzione degli artefatti dovuti a dispositivi metallici , sia nel piano che fig . 
visibile unarea centrale ipointensa ( asterisco nero ) ed alcune aree iperintense ( asterischi bianchi ) che rappresentano un sanguinamento recente . 92 radiol med ( 2012 ) 117 : 8595 when signs of local infection have disappeared [ 18 ]  . 
 combined leukocyte / marrow although bone scintigraphy may be useful for screening scintigraphy purposes , remains the procedure of choice for diagnosing infection [ 4 ] , but its capability to give a precise quantification of the collection remains suboptimal . 
 however , hip prostheses are now made of new alloys with a high content of titaniuthis , together with the use of suitable sequences , helps to relevantly reduce susceptibility artefacts . 
importantly , relevant technological improvements in terms of mri sequence design are ongoing in order to greatly reduce the size of artefacts due to metallic orthopaedic devices in clinical imaging , such as the accelerated slice encoding [ 19 ]  . 
this approach , combined with standard echo - train , parallel , partial - fourier imaging , and inversion - recovery techniques , has proven to be effective in correcting both in - plane and throughplane artefacts due to metallic devices in scan times < 11 min [ 19 ]  . 
in particular , they found that artefacts can be influenced by several factors , including pulse sequence , voxel size , gradient strength , phase - encoding direction and metallic device orientation with respect to the static magnetic field . 
visibile unarea centrale ipointensa ( asterisco nero ) ed alcune aree iperintense ( asterischi bianchi ) che rappresentano un sanguinamento recente . attraverso il piano , in meno di 11 minuti di scansione [ 19 ]  . 
in particolare , tali autori hanno analizzato come operano il tipo di sequenza , le dimensioni del voxel , lintensit di campo e la direzione del gradiente di codifica di fase e lorientamento del dispositivo metallico rispetto al campo magnetico statico . 
tali autori hanno valutato lartefatto generato da oggetti metallici allungati ( viti di sintesi ) , cercando di posizionare sia il fantoccio che il ginocchio nel quale erano impiantate viti metalliche lungo una direzione angolata in modo ottimale rispetto al vettore del campo magnetico statico . 
tale risultato connesso alle dimensioni relativamente piccole delle viti e non pu essere traslato meccanicamente a quanto ottenibile con grandi impianti protesici a l . radiol med ( 2012 ) 117 : 8595 fig . 
 presenza di fistola cutanea ( teste di freccia )  . in our series , clinical signs and blood test values were recorded and reported to give more comprehensive details about the study population . 
however , alteration of these values is not sensitive or specific for infection , as it could also be detected in the case of prosthesis loosening [ 3 ]  . 
 [ 22 ] , whose results are consistent with ours when dealing with anatomy visibility and interobserver reproducibility , we demonstrated a perfect correlation between joint aspiration and mri . nella nostra serie , i segni clinici e i risultati dei test ematochimici sono stati registrati e riportati al fine di fornire un quadro pi completo della popolazione oggetto di studio . 
sarebbe stato interessante correlare le dimensioni della raccolta alla rm con lintensit del dolore misurata su una scala di analogo visivo [ 21 ] , ma purtroppo questo dato non era disponibile nella nostra serie di pazienti . entrambi i radiologi hanno diagnosticato la presenza di una raccolta periprotesica in 21 / 26 indagini ( 81% )  . 
 [ 22 ] , i cui risultati sono simili ai nostri in termini di visibilit anatomica e riproducibilit , noi abbiamo dimostrato una perfetta correlazione tra rm e agoaspirazione . questi risultati hanno due principali implicazioni cliniche . 
secondly , in patients treated conservatively , mri becomes extremely helpful in evaluating a downsizing the collection or disappearance of soft tissue oedema , thus confirming the success of medical therapy . in our study , some limitations should be taken into account . 
however , the large agreement between the two readers in fluid collection measurements , as well as the high interobserver reproducibility in determining collection localisation , makes the outcome of our study quite reliable . 
however , recent studies demonstrate that gadolinium - based contrast material should not be routinely administered in the imaging workup of nonspinal musculoskeletal infections [ 23 ]  . in conclusion , our data suggest that mri is a highly reliable imaging technique in the detection , quantification , localisation , and characterisation of fluid collections in patients with painful tha when the presence of an infection is clinically suspected . 
being free from ionising radiation , mri seems to represent an ideal imaging technique in the follow - up of patients with tha infection . in primo luogo , localizzazione , quantificazione e caratterizzazione delle raccolte periprotesiche consentono di decidere se un paziente debba essere sottoposto a revisione chirurgica dellimpianto . 
in secondo luogo , nei pazienti trattati conservativamente , la rm si dimostra molto utile nel valutare la progressiva riduzione della raccolta o la scomparsa delledema dei tessuti molli , a conferma del successo della terapia medica . il presente studio ha alcuni limiti . 
in secondo luogo , per differenti motivi ( inclusa la non disponibilit della diagnostica nucleare nel nostro ospedale ) , non abbiamo comparato la rm con altre tecniche di imaging . 
recenti studi hanno tuttavia indicato che le scansioni dopo somministrazione di mezzo di contrasto paramagnetico non sono da considerarsi routinarie nella valutazione delle infezioni muscolo scheletriche non spinali [ 23 ]  . in conclusione , i nostri risultati indicano che la rm rappresenta una modalit diagnostica altamente affidabile nel riconoscimento , nella quantificazione e nella caratterizzazione delle raccolte fluide in pazienti sottoposti ad artroprotesi danca con sospetto clinico di infezione periprotesica . 
razek , tel : + 20 - 161 - 948567 , e - mail : arazek@mans.edu.eg , received : 16 november 2010 / accepted : 17 january 2010 / published online : 10 july 2011 springer - verlag 2011 abstract purpose . 
we carried out a retrospective study of 37 patients ( 22 male , 15 female ; age range 468 years ; mean age 41 years ) with a soft tissue mass . 
 diffusion - weighted magnetic resonance ( mr ) imaging was done using echo - planar imaging ( epi ) with b factor of 0.500 and 1 , 000 mm2 / s . 
diffusion - weighted echo - planar mr imaging is a promising noninvasive modality that may be helpful in differentiating malignant soft tissue tumours from benign masses as well as in grading malignancy . keywords diffusion mr imaging soft tissue tumour malignancy riassunto obiettivo . 
abbiamo condotto uno studio retrospettivo su 37 pazienti ( 22 maschi , 15 femmine ; range det , 468 anni ; et media , 41 anni ) con una massa nei tessuti molli . 
abbiamo osservato una differenza significativa nei valori di adc tra tumori dei tessuti molli e lesioni benigne ( p < 0 , 001 ) , e con differenti gradi di malignit ( p < 0 , 02 )  . 
la scelta di un valore di adc pari a 1 , 3410 - 3 mm2 / s come soglia per differenziare i tumori maligni dalle lesioni benigne ha dimostrato una accuratezza del 91% , una sensibilit del 94% , una specificit dell88% ed unarea sotto la curva ( auc ) pari a 0 , 869 . 
limaging rm eco - planare pesato in diffusione una promettente metodica non - invasiva che potrebbe aiutare nella differenziazione i tumori maligni dei tessuti molli dalle lesioni benigne , cos come nella definizione del grado di malignit . parole chiave diffusione imaging rm tessuti molli tumore malignit radiol med ( 2012 ) 117 : 96101 introduction treatment of soft tissue tumours requires a diagnostic tool that can differentiate malignant from benign masses in a noninvasive manner . 
positron emission tomography ( pet ) - ct is a metabolic imaging modality that may show some overlap between malignancy , infection and some benign tumours [ 5 , 6 ]  . 
routine contrast - enhanced magnetic resonance ( mr ) imaging , short - tau inversion recovery ( stir ) , dynamic contrast - enhanced mr imaging and mr spectroscopy have low specificity in the differentiation between benign and malignant soft tissue masses [ 710 ]  . 
biopsy is essential to reach the final diagnosis but is an invasive procedure that carries a risk of sampling error and may be associated with bleeding [ 11 ]  . diffusion - weighted mr imaging has been performed to evaluate musculoskeletal tumours [ 1214 ]  . 
these studies indicate that diffusion - weighted mr imaging may be useful for differentiating between malignant and benign soft tissue tumours [ 1521 ] , evaluating soft tissue infection [ 22 , 23 ] and monitoring patients with a soft tissue mass after therapy [ 24 , 25 ]  . the purpose of this study was to assess soft tissue tumour of the extremities with diffusion - weighted echo - planar mr imaging . materials and methods this retrospective study was carried out on 44 consecutive patients with a soft tissue mass of the extremities . 
the inclusion criterion was patients with an initially diagnosed soft tissue mass of the upper or lower extremity that had not undergone biopsy or treatment with radiation therapy or chemotherapy . 
exclusion criteria were poor quality of diffusion - weighted mr image due to motion artefacts ( n = 4 ) and purely cystic lesion ( n = 3 ) to avoid bias due to the high apparent diffusion coefficient ( adc ) value of cystic lesions . 
the study finally included 37 patients ( 22 male , 15 female ; age range 468 years ; mean age 41 years ) with a soft tissue mass of the upper or lower extremity . 
this study was approved by the ethics committee , and patient consent was waived due to the retrospective study design . the mr studies were performed with a 1.5 - tesla mr machine ( siemens , symphony , siemens medical systems , erlangen , germany ) equipped with a self - shielding gradient set ( 30 mt / m maximum gradient strength and 120 t / m / s slew rate ) for echo - planar imaging . 
all patients underwent t1 - weighted imaging ( time to repeat [ tr ] / time to echo [ te ] 800 / 15 ms ) , t2 - weighted fast spin - echo imaging ( tr / te 6 , 000 / 80 ms ) and spoiled gradient - echo sequences ( tr / te 37 / 20 ms , flip angle 12 ) with a section thickness of 5 mm , an interslice gap of 2 mm , a field of view ( fov ) of 3035 cm and an acquisition matrix of 256224 . diffusion - weighted imaging was obtained in an axial plane using a multislice spin - echo echo - planar imaging sequence . 
the technical parameters were tr / te 10 , 000 / 108ms ; slice thickness 5 mm ; interslice gap 2.5 mm ; number of excitations ( nex ) 2 ; bandwidth 125 khz ; matrix 256128 ; fov , 2530 c the diffusion gradients were applied in three orthogonal directions ( x , y and z )  . 
diffusion - weighted mr images were acquired with b values of 0.500 and 1 , 000 s / mm2 , and an apparent diffusion coefficient ( adc ) map was reconstructed . 
diffusion - weighted mr scanning time was < 2 min . postcontrast fat - suppressed t1 - weighted images ( tr / te 680800 / 15 ms , with two signals ) were obtained in the transverse and coronal planes after the intravenous bolus injection of 0.1 mmol / kg of gadopentetate dimeglumine ( magnevist ; schering , berlin , germany )  . 
fat suppression was accomplished with a frequency - selective presaturation pulse . the diffusion - weighted mr images were interpreted by two radiologists ( ra , gm ) blinded to the final diagnosis . 
the final adc value per lesion was the average of these three adc values . statistical analysis was done using statistical package for social science version ( spss programme version 10 , chicago , il , usa )  . 
the receiver operating characteristic ( roc ) curve was drawn to detect the cutoff point used to differentiate malignant from benign soft tissue masses , with calculation of sensitivity , specificity , accuracy , positive predictive value 98 results ( ppv ) , negative predictive value ( npv ) and area under the curve ( auc )  . and high - grade malignancies . radiol med ( 2012 ) 117 : 96101 pathology of the soft tissue masses revealed malignant tumours in 23 patients and benign tumours in 14 patients . 
there was a significant difference ( p = 0.001 ) in the adc values of low discussion several studies demonstrated the potential of diffusionweighted mr imaging in evaluation of soft tissue masses . 
 one study reported that the mean adc value of benign lesions ( 1.71103 mm2 / s ) is significantly higher than that of malignant tumours ( 1.08103 mm2 / s ) [ 16 ]  . 
the mean adc value of chronic haematoma was significantly higher than that of malignant soft tissue tumours ( p = 0.01 ) without any overlap [ 18 ]  . in this work , the mean adc value of benign soft tissue masses was significantly higher than that of malignant tumours , despite there being some overlap in their adc values . 
on the other hand , benign soft tissue masses have less restricted extracellular space , allowing spin dephasing and loss of signal on diffusionweighted images [ 1821 ]  . in this study , one patient with myxoid liposarcoma had a high adc value that was misdiagnosed as a benign tumour . 
c la mappa del coefficiente apparente di diffusione ( adc ) dimostra una restrizione della diffusione allinterno della massa con basso valore di adc ( 1 , 17103 mm2 / s )  . of myxoid tissue in the extracellular space that influences the adc value . 
the high adc value of the myxoid matrix is attributed to the large amount of free water in the extracellular spaces [ 19 ]  . two benign fibrous tumours were misdiagnosed as malignant . 
these tumours consist of spindle - shaped cells surrounded and separated from each other by collagen fibres , which are associated with restricted diffusion and low adc values . in this study , the adc value of high - grade malignancy was significantly lower ( p < 0.001 ) than that of the lowgrade malignant tumours . 
histologic grading parameters , such as cellularity , mitotic rate , matrix and presence of necrosis influence the adc value [ 21 ]  . in this study , echo - planar diffusion mr imaging was used to evaluate soft tissue tumours . 
echoplanar images are prone to artefacts , particularly magnetic susceptibility artefacts and especially at tissue interfaces such as air and soft tissue or bone and soft tissue , and geometric distortions created by eddy currents [ 1214 ]  . 
further studies are recommended using diffusiontensor imaging at higher b values with parallel imaging to reduce susceptibility artefacts on 3 - tesla machine for the evaluation of soft tissue masses . there are a few limitations to this study . 
il valore soglia di adc utilizzato nella differenziazione dei tumori maligni dalle lesioni benigne stato di 1 , 34103 mm2 / s , con unaccuratezza del 91% , una sensibilit del 91% , una specificit dell88% ed unarea sotto la curva ( auc ) di 0 , 869 . is patient heterogeneity , with different age groups and different pathological types . 
longo1 1department of radiology , irccs , ospedale pediatrico bambino ges , piazza santonofrio 4 , 00100 rome , italy 2departement of infective disease , irccs , ospedale pediatrico bambino ges , piazza santonofrio 4 , 00100 rome , italy 3department of pathology , irccs , ospedale pediatrico bambino ges , piazza santonofrio 4 , 00100 rome , italy correspondence to : l . 
a retrospective descriptive evaluation was conducted on imaging studies obtained from ten children admitted to our hospital over a 6 - year period who fulfilled criteria for a diagnosis of cns tuberculosis . 
neuroradiological findings on the first imaging study were basal meningeal enhancement ( 100% ) , hydrocephalus ( 70% ) , infarcts ( 90% ) , tuberculomas ( 40% ) and cranial nerve involvement ( 20% )  . 
i reperti neuroradiologici rilevati allindagine iniziale sono stati impregnazione delle meningi della base cranica ( 100% ) , idrocefalo ( 70% ) , lesioni infartuali ( 90% ) , tubercolomi ( 40% ) e interessamento dei nervi cranici ( 20% )  . 
in 2007 , the world health organization ( who ) estimated that there were 9.27 million new cases of tuberculosis and 1.3 million deaths from tb among hiv - negative individuals . 
after an insidious onset of nonspecific symptoms such as fever , nausea , vomiting and headache , the clinical progression of cns - tb tends to be rapid , especially in infants and young children . 
imaging features , however , may also be nonspecific and overlap with other intracranial diseases , such as cysticercosis , metastases and primary brain neoplasms [ 3 ]  . the aim of this paper is to discuss and illustrate imaging features of cns - tb on ct and mri studies in non - hivpositive children . linfezione tubercolare ( tbc ) del sistema nervoso centrale ( snc ) la forma di tubercolosi extra - polmonare con pi elevata mortalit . 
nel 2007 , lorganizzazione mondiale della sanit ( oms ) ha stimato 9 , 27 milioni di nuovi casi di tubercolosi e 1 , 3 milioni di morti per tbc tra i pazienti sieronegativi . 
il tasso di incidenza rimasto stabile in europa ed in lento declino in tutte le altre regioni delloms ; tuttavia , il numero totale di nuovi casi di tubercolosi continua ad aumentare lentamente [ 1 ]  . 
gli studi di neuroimaging sono di aiuto nella diagnosi precoce dellinfezione tubercolare del snc : in particolare la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm ) dellencefalo sono le indagini utilizzate per localizzare e determinare lestensione della malattia , anche se i reperti di tali indagini possono essere non - specifici e confondersi con altre patologie intra - craniche come cisticercosi , metastasi e neoplasie primitive dellencefalo [ 3 ]  . 
 scopo di questo studio descrivere e discutere le caratteristiche tc e rm dellencefalo nellinfezione tubercolare del sistema nervoso centrale in un gruppo di bambini non positivi al virus dellimmunodeficienza umana acquisita ( hiv )  . materials and methods we retrospectively evaluated ten consecutive patients ( five boys and five girls ) referred to our radiology department for brain ct and mri studies between 2004 and 2010 . 
 inclusion criteria for a cns - tb diagnosis were either positive mycobacterium tuberculosis culture in cerebrospinal fluid ( csf ) and / or gastric aspirate , or clinical and csf criteria suggestive of neurotuberculosis ( high protein and low glucose , pleocytosis > 20 cells / mm3 with lymphocyte predominance ) with two or more of the following : 1 . 
chest radiograph compatible with a diagnosis of primary materiali e metodi sono stati valutati retrospettivamente 10 pazienti consecutivi ( 5 maschi e 5 femmine ) inviati presso il nostro reparto di diagnostica per immagini tra il 2004 e il 2010 per essere sottoposti ad uno studio tc e / o rm dellencefalo . 
 i criteri di inclusione utilizzati per la diagnosi di tbc del snc sono stati : esame colturale positivo per mycobacterium tuberculosis del liquor e / o dellaspirato gastrico o criteri clinici associati ad alterazioni del liquor ( proteinorrachia elevata , glicorrachia diminuita , pleiocitosi > 20 cellule / mm3 con predominanza di linfociti ) associati a due o pi dei seguenti : 1 . 
cranial ct or mri findings suggestive of cns - tb . exclusion criteria were hiv - positive status , negative microbiological test , positive history of immunosuppressive or immunomodulatory drugs including steroids , transplantations , lymphoproliferative disorders and diagnosis of congenital immunosuppressive syndromes or autoimmune vasculitis . unenhanced and contrast - enhanced ct ( ct / cect ) studies were performed using a sequential technique with a single - slice ct scanner ( somatom plus 4 , siemens )  . 
half were of italian origin and the other half of romanian orig the main clinical symptoms and signs present on admission were fever ( 100% ) , vomiting ( 60% ) , somnolence ( 40% ) , seizures ( 30% ) , headache ( 20% ) and cough ( 10% )  . 
reperti tc o rm encefalo suggestivi per infezione tubercolare del snc . i criteri di esclusione sono stati : sierologia positiva per hiv , dato anamnestico di uso di farmaci immuno - soppressori o immuno - modulatori , trapianti , malattie linfo - proliferative , sindrome da immunosoppressione , vasculite autoimmune e negativit degli esami microbiologici per infezione tubercolare . lesame tc stato condotto con tecnica sequenziale con apparecchiatura a uno strato ( somatom plus 4 , siemens , germania )  . 
il protocollo di acquisizione ha incluso sequenze spin echo ( se ) t1 dipendenti ( tempo di ripetizione [ tr ] / tempo di eco [ te ] = 450 / 12 ms , matrice = 242512 ) secondo piani sagittali ed assiali , turbo spin echo ( tse ) t2 dipendenti ( tr / te = 4000 / 99 ms , matrice = 256128 ) secondo piani coronali , inversion recovery ( ir ) ( tr / te / tempo di inversione [ ti ] = 8416 / 60 / 350 ms , flip angle = 180 , matrice = 176512 ) secondo piani assiali , fluid attenuated inversion recovery ( flair ) ( tr / te / ti = 7000 / 110 / 2000 ms , flip angle = 180 , matrice = 154256 ) secondo piani assiali . 
le sequenze t1 dipendenti sono state effettuate prima e dopo somministrazione endovenosa di 0 , 2 ml / kg di acido gadoterico ( dotarem 0 , 05 mmol / ml )  . 
sono stati considerati i seguenti segni neuroradiologici : impregnazione delle meningi della base cranica dopo somministrazione endovenosa di mezzo di contrasto ( mdc ) , idrocefalo , lesioni infartuali , tubercolomi e interessamento dei nervi cranici . risultati nello studio sono stati arruolati dieci bambini con infezione tubercolare del snc di cui 5 maschi e 5 femmine . 
one patient died because of a cardiocirculatory arrest . discussion the diagnosis of early cns - tb may be difficult due to the often nonspecific presentation of symptoms and inconclusive laboratory results . 
ct and mri studies have greatly enhanced the diagnostic accuracy of cns - tb [ 5 , 6 ] , which occurs either in diffuse ( meningitis ) , localised ( tuberculoma , abscess and cerebritis ) or both forms [ 7 ]  . 
un paziente deceduto a causa di arresto cardiocircolatorio . discussione la diagnosi precoce di infezione tubercolare del snc pu essere difficoltosa per i sintomi non specifici e per i risultati radiol med ( 2012 ) 117 : 669678 fig . 
 a - c axial t2 - weighted imaging ( wi ) show tetraventricular dilatation and a periventricular hyperintensity due to seepage of cerebrospinal fluid across the white matter ( arrowheads )  . 
a - c le immagini rm assiali t2 dipendenti mostrano una dilatazione tetraventricolare e aree iperintense in corrispondenza dei corni anteriori e posteriori dei ventricoli laterali come da riassorbimento subependimale di liquido cefalo - rachidiano ( lcr ) ( punte di frecce )  . 
linfezione tubercolare del sistema nervoso centrale pu manifestarsi in forma diffusa ( meningite ) , forma focale ( tubercoloma , ascesso e cerebrite ) o mista [ 7 ]  . 
ra le manifestazioni dellinfezione tubercolare del snc la leptomeningite la pi frequente e limpregnazione delle meningi della base cranica ben dimostrata dagli esami tc e rm con mezzo di contrasto [ 8 ]  . 
a , b contrast - enhanced ct shows hydrocephalus and marked abnormal basal meningeal enhancement within the suprasellar cistern , prepontine cistern , ambient cistern , middle cerebral artery cisterns and anterior interhemispheric fissure . 
a , b la tc assiale con mdc mostra idrocefalo e marcata impregnazione delle cisterne sovra - sellari , pre - pontina , ambiens , cisterne dellarteria cerebrale media e della porzione anteriore della scissura interemisferica . 
si osservano inoltre tubercolomi non caseosi in corrispondenza del mesencefalo e del peduncolo cerebrale destro ( frecce )  . surface shows focal linear enhancement [ 3 , 6 ]  . 
on ct or t1 - weighted images ( t1 - wi ) without contrast agent , the exudate appears as soft tissue that fills the cisterns . in cns - tb , the most frequent complications are represented by hydrocephalus and infarction consequent to vasculitis . 
 periventricular hyperintensity on t2 - wi is due to csf seepage across the white matter , and it usually suggests determinata dal danno delle cellule endoteliali da parte di processi infiammatori mediante un meccanismo di immunit cellulo - mediata . 
nelle immagini basali di tc o in quelle rm t1 dipendenti , lessudato mostra rispettivamente densit dei tessuti molli o intensit di segnale di tessuto solido che riempie le cisterne . nella tbc del snc , le pi frequenti complicanze sono lidrocefalo e linfarto conseguente a vasculite . 
 gli infarti acuti dei nuclei caudati ( frecce nere ) e del putamen di sinistra ( punte di freccia bianche ) sono iperintensi in t2wi e dwi e ipointensi nelle mappe adc . 
si osserva inoltre idrocefalo tetraventricolare . hydrocephalus under pressure , which is an indication for csf diversion surgery to decompress the ventricular system . vasculitis is a complication commonly seen at autopsy in tuberculous meningitis . 
lidrocefalo non comunicante meno comune e pu essere secondario a un effetto massa determinato da lesioni parenchimali focali o a intrappolamento di una parte di un ventricolo per ependimite granulomatosa . 
liperintensit di segnale periventricolare , rilevabile nelle immagini t2 dipendenti , dovuta al passaggio di liquido cerebro - spinale nella sostanza bianca e solitamente indica idrocefalo iperteso , che una indicazione al drenaggio liquorale con decompressione del sistema ventricolare . la vasculite una complicanza comunemente rilevata allesame autoptico nei soggetti con meningite tubercolare . 
b limmagine assiale t2 - dipendente mostra un granuloma caseoso con porzione centrale ipointensa ed edema perilesionale . ( freccia ) c nelle immagini t1 - dipendenti il granuloma presenta segnale ipointenso . 
the infarcts appear as low - density regions on ct ; on mri , acute infarcts show hyperintensity on diffusionweighted imaging ( dwi ) with or without hyperintensity on t2 - wi and isoor hypointense signal on t1 - wi . 
nel nostro studio , 5 pazienti presentavano infarti dei nuclei della base e aree ischemiche cortico - sottocorticali alla prima indagine e 4 pazienti lesioni esclusivamente dei nuclei della base . 
alla rm gli infarti acuti mostrano iperintensit in diffusion - weighted imaging ( dwi ) con o senza iperintensit in t2 e iso / ipointensit in radiol med ( 2012 ) 117 : 669678 infratentorial majority of tuberculomas is supratentorial and may be solitary or multiple ; however , they can also be found in subdural , epidural and subarachnoid spaces . 
in our study , four patients had tuberculomas in the first imaging study and seven in the follow - up study . rarely , the central caseous component of the tuberculoma may liquefy , forming a tuberculous abscess . 
 only one patient showed a pattern of miliary tuberculosis in our series . in conclusion , because prompt diagnosis results in earlier treatment , it is crucial to be aware of tuberculous meningitis and its complications at imaging , especially because of the impact on patients prognosis . 
contrast - enhanced sequences are essential in these patients to detect focal or diffuse meningeal enhancement and focal intra - axial lesions , such as tuberculomas and abscesses . t1 ; il coefficiente apparente di diffusione ( adc ) ridotto nello stadio acuto , variabile nel subacuto ed elevato nel cronico . 
solo in un nostro paziente stata evidenziata una forma miliare . in conclusione , i reperti neuroradiologici di idrocefalo , impregnazione leptomeningea delle cisterne della base e lesioni infartuali dei nuclei della base consentono di formulare una ipotesi diagnostica di infezione tubercolare del sistema nervoso centrale . 
bonomo1 1dipartimento di bio - immagini e scienze radiologiche , universit cattolica del sacro cuore , largo gemelli 8 , 00168 roma , italy 2dipartimento di medicina interna , universit cattolica del sacro cuore , largo gemelli 8 , 00168 roma , italy correspondence to : p . 
forty - five consecutive patients with known or suspected coeliac disease ( 35 females , ten males ; age range 1165 years ) prospectively underwent sonography before and after ingestion of 750 ml of an aqueous solution of polyethylene glycol . 
baseline examination showed abnormal features in 13 / 25 celiac patients ( dilated fluid - filled loops , increased peristalsis , transient intussusception , mesenteric lymph nodes , intraperitoneal fluid )  . 
quarantacinque pazienti ( 35 femmine , 10 maschi ; et : 1165 anni ) con celiachia sospetta o accertata sono stati sottoposti prospetticamente ad ecografia prima e dopo somministrazione orale di 750 ml di soluzione acquosa di polietilenglicole . 
il riempimento fluido ha migliorato la visualizzazione del tenue ( lume , pliche mucose , stratificazione parietale ) nel 77 , 6% dei casi ( miglioramento notevole , discreto , o minimo in 2 , 16 , e 17 pazienti ; 4 , 4% , 35 , 5% e 37 , 7% ) ; non ha migliorato o ha peggiorato la visualizzazione nel 20% e 2 , 2% ( 9 e 1 pazienti )  . 
 radiol med ( 2012 ) 117 : 558574 keywords small bowel polyethylene glycol celiac disease bowel wall sonography parole chiave intestino tenue polietilenglicole celiachia parete intestinale ecografia introduction introduzione in recent years , tomographic imaging techniques , such as sonography ( us ) , computed tomography ( ct ) and magnetic resonance ( mr ) imaging , which can provide simultaneous visualisation of the gut wall and adjacent extramural structures , have expanded the options for the study of the small intestine and have thus become the natural and necessary complements to traditional small - bowel studies . 
because of its well - known advantages ( noninvasiveness , absence of ionising radiation , low costs ) , sonography has earned a role in the study of various diseases involving the small and large bowel [ 14 ]  . 
moreover , sonography has some fairly unique advantages , such as real - time observation which is especially useful for gathering dynamic information on bowel peristalsis and contractility and depiction of parietal layered structure . 
the drawbacks of sonography include low reproducibility and a limited field of view : unlike radiological barium studies and the newer ct and mr imaging techniques , the sonographic examination is segmental , focusing on a few loops at a time . 
moreover , small - bowel loops have thin , easily pliable , walls and are frequently obscured by their gaseous content . improved sonographic visualisation of the small intestine has been described after fluid distension of bowel loops by use of water or echo - poor fluid as an endoluminal contrast agent , either infused through a nasojejunal tube ( sonoenteroclysis ) [ 5 , 6 ] or administered orally ( oral contrast - enhanced sonography ) [ 713 ]  . 
for this purpose , we evaluated prospectively overall visualisation and specific features of the small bowel on sonography in a group of patients with proved or suspected coeliac disease ( to analyse a more homogeneous series )  . 
results of conventional sonography and orally administered contrast - enhanced sonography were rated and statistically compared on the basis of overall depiction of bowel loops and of abnormal features suggestive of coeliac disease , as reported in the literature ( increased intraluminal fluid , dilated and flaccid loops , fold thickening or effacement , reversed jejunoileal fold pattern , abnormal smallbowel motility with either increased or reduced peristaltic activity , transient intussusception , mesenteric lymph nodes , free peritoneal fluid ) [ 1419 ]  . 
this study was conducted to evaluate feasibility , patient acceptance and diagnostic yield negli ultimi anni lintroduzione delle tecniche tomografiche di imaging , quali ecografia ( us ) , tomografia computerizzata ( tc ) , risonanza magnetica ( rm ) , che permettono la contemporanea visualizzazione sia delle pareti dellintestino che delle strutture extramurali circostanti , ha ampliato notevolmente le possibilit di studio dellintestino tenue . 
per i suoi vantaggi ben noti ( esame non invasivo , che non comporta esposizione a radiazioni ionizzanti , a basso costo ) lecografia ha ormai acquisito un suo ruolo nello studio di varie patologie del tenue e del colon [ 14 ]  . 
inoltre lecografia ha alcuni specifici vantaggi quali la possibilit di osservazione in tempo reale , particolarmente utile per ottenere informazioni di tipo dinamico sulla peristalsi e lattivit contrattile dellintestino , e la capacit di visualizzare la struttura stratificata delle pareti viscerali . 
 gli svantaggi dellecografia sono rappresentati dalla scarsa riproducibilit e dal campo di vista limitato : a differenza degli studio radiologici con bario e successivamente delle tecniche tc e rm , lesame ecografico di tipo segmentario , in grado di rappresentare per ogni singola scansione solo pochi segmenti intestinali . 
 stata descritta la possibilit di una migliore visualizzazione ecografica dellintestino tenue dopo distensione fluida delle anse mediante acqua o altri liquidi ecoprivi , utilizzati come contrasto endoluminale , e somministrati per infusione tramite sondino nasodigiunale ( sonoenteroclisi ) [ 5 , 6 ] o assunti per os ( ecografia con mezzo di contrasto orale ) [ 713 ]  . 
a questo scopo abbiamo valutato in modo prospettico sia la visibilit complessiva sia pi specificamente i caratteri del tenue in un gruppo di pazienti con malattia celiaca accertata o sospetta ( allo scopo di analizzare una casistica pi omogenea ) , prima con ecografia convenzionale e successivamente dopo distensione fluida delle anse del tenue . 
 accordingly , over a 2 - year period , 45 consecutive patients ( 35 female , ten male ; age range 1165 years ) with clinically suspected ( 26 ) or known ( 19 ) coeliac disease were prospectively examined by abdominal sonography in our department . 
in 19 patients , the diagnosis of coeliac disease had already been established on the basis of previous laboratory and endoscopic examinations : four patients were untreated , and 15 were on a gluten - free diet . 
as the study was not aimed at validating the accuracy of sonography in diagnosing coeliac disease but at verifying whether oral administration of fluid can improve bowel visualisation , all 19 coeliac patients were pooled , and we searched for sonographic signs of coeliac disease before and after luminal filling by fluid , regardless of patient status ( newly diagnosed or known disease ; disease duration ; treated or untreated disease )  . 
the remaining 26 patients had no past medical history of the disease and were being investigated because they had clinical symptoms ( diarrhoea , steatorrhoea , vague abdominal pain , weight loss ) , nonspecific abnormalities ( fatigue , malaise , anaemia , bone pain ) suggestive of malabsorption or elevated antiendomysial and / or antitransglutaminase antibodies ( suggesting coeliac disease ) but who nevertheless underwent abdominal sonography as a routine part of their general assessment . 
 of the 26 patients under evaluation for abdominal or general symptoms or laboratory abnormalities suspicious for malabsorption , coeliac disease was ultimately diagnosed in six patients ( newly diagnosed )  . 
among the remaining 20 patients , 14 had other benign diseases ( five irritable bowel disease , two lactose intolerance , one type i diabetes with undetermined malabsorption , one gastrooesophageal reflux disease , one allergy to nickel , one antral gastritis and chronic pancreatitis , three crohns disease of the ileum ) , whereas no definitive abnormalities were found in the remaining six patients . 
con il presente studio ci siamo proposti di verificare la fattibilit , il grado di accettazione da parte dei pazienti , il guadagno diagnostico e i possibili vantaggi della tecnica con riempimento fluido a confronto con lecografia convenzionale nello studio dellintestino tenue . 
 materiali e metodi casistica i criteri di inclusione nel presente studio sono stati sospetto clinico ( sulla base di sintomatologia digestiva o sistemica ) o diagnosi gi accertata di malattia celiaca . 
i criteri di esclusione sono stati sospetto clinico o diagnosi gi accertata di altre patologie del tenue ( per esempio , morbo di crohn , occlusione intestinale ) o dello stomaco o del colon ( per esempio , ulcera gastrica o duodenale , diverticolite acuta , neoplasie dello stomaco o del colon )  . 
con queste premesse , nellarco di due anni presso il nostro istituto abbiamo esaminato prospetticamente con ecografia addominale 45 pazienti consecutivi ( 35 femmine , 10 maschi ; et : 1165 anni ) con celiachia sospetta ( n = 26 ) o gi nota ( n = 19 )  . 
in 19 pazienti la diagnosi di celiachia era stata gi accertata sulla base di precedenti esami di laboratorio ed endoscopici ; 4 di questi pazienti erano a dieta libera e 15 erano in dieta aglutinata . 
 poich il presente studio non era rivolto a validare laccuratezza dellecografia nella diagnosi di celiachia , ma solo a verificare se la somministrazione di fluido per os fosse in grado di migliorare la visualizzazione del tenue , tutti i 19 pazienti celiaci sono stati considerati come un unico gruppo , ricercando i possibili segni ecografici di celiachia prima e dopo distensione fluida dellintestino , indipendentemente dallo stato del paziente ( celiachia di nuova diagnosi o gi accertata ; durata della malattia ; in trattamento con dieta aglutinata o no )  . 
i rimanenti 26 pazienti non avevano alcuna anamnesi di celiachia e gli accertamenti in corso erano stati richiesti in seguito ad una sintomatologia clinica ( diarrea , steatorrea , dolori addominali diffusi , calo ponderale ) o ad alterazioni generali aspecifiche ( astenia , malessere , anemia , dolori ossei ) che facevano sospettare un malassorbimento , oppure perch erano stati riscontrati valori elevati degli anticorpi antiendomisio e / o antitransglutaminasi ( indicativi di celiachia ) , ma era comunque richiesta lecografia addominale come esame di routine nel quadro di una valutazione generale . 
 la diagnosi definitiva stata ottenuta sulla base dei criteri clinici comunemente accettati e degli esami di laboratorio , radiologici , endoscopici ed istologici , a seconda delle differenti patologie sospettate . 
the examiners were only aware of the patients diagnosis in cases of known coeliac disease , but they did not have access to the patients current laboratory data or radiological examinations . 
proof of coeliac disease was based on antigluten , antiendomysial and antitransglutaminase antibodies as well as on jejunal histology by endoscopic biopsy in all newly diagnosed patients . us examination consisted of a detailed scan of the abdomen , which was then repeated after oral administration of an aqueous solution containing ( per litre ) : polyethylene glycol 58.28 g ; magnesium sulphate ( mgso ) 7.5 g , sodium sulphate ( naso ) 2.85 g , sodium hydrochloride ( nahco ) 1.69 g , sodium chloride ( nacl ) 0.8 g and potassium chloride ( kcl ) 0.74 g , as electrolytes ( promefarm ; milan , italy ) , with a corresponding osmolarity of 280290 mosm / kg . 
the solution is commonly used as a cleansing preparation ( isoosmotic laxative group ) before radiological examinations of the small or large bowel : as water and sodium absorption within the small bowel are reduced , luminal contents remain iso - osmotic , and small - bowel distension is prolonged . 
 sonographic technique a detailed study of the gastrointestinal tract was carried out on fasting participants using commercially available equipment ( antares , siemens medical solutions , erlangen , germany ; aplio , toshiba , tokyo , japan ) with standard 4 - mhz curved - array and 8or 10 - mhz linear - array multifrequency transducers . 
dei restanti 20 pazienti , 14 avevano altre patologie benigne ( 5 colon irritabile , 2 intolleranza al lattosio , 1 diabete di tipo i con malassorbimento di natura indeterminata , 1 malattia da reflusso gastroesofageo , 1 allergia al nickel , 1 gastrite antrale e pancreatite cronica , 3 crohn ileale )  . 
altri eventuali esami radiologici pi specifici o complessi ( per esempio , studi con bario dellintestino tenue con la metodica dellesame seriato o dellenteroclisi a doppio contrasto ; enterografia / enteroclisi - tc o rm ) sono stati effettuati solo successivamente se ritenuti necessari ( a seconda dellipotesi clinica ) come esami di seconda istanza . 
 gli esaminatori erano a conoscenza solo della diagnosi di celiachia in caso di malattia gi nota , ma a parte questo non erano al corrente dei dati di laboratorio o radiologici recenti . 
per tutti i pazienti di nuova diagnosi la malattia celiaca stata verificata sulla base del titolo degli anticorpi anti - glutine , antiendomisio , e antitransglutaminasi , e dei caratteri istologici del digiuno alla biopsia endoscopica . 
 lesame ecografico consisteva in uno studio dettagliato delladdome , che era successivamente ripetuto dopo somministrazione orale di una soluzione acquosa contenente ( per litro ) : polietilenglicole ( peg ) 58 , 28 g ; mgso 7 , 5 g , naso 2 , 85 g , nahco 1 , 69 g , nacl 0 , 8 g e kcl 0 , 74 g , come elettroliti ( promefarm , milano , italia ) , con una corrispondente osmolarit di 280290 mosm / kg . 
la soluzione abitualmente usata come preparazione per la pulizia intestinale ( gruppo dei lassativi iso - osmotici ) prima degli esami radiologici del tenue e del colon : poich lassorbimento di acqua e di sodio a livello del tenue ridotto , il contenuto intestinale resta iso - osmotico e la distensione del tenue ne risulta prolungata . 
i possibili effetti avversi dopo la somministrazione comprendono senso di ripienezza addominale , alvo diarroico , nausea ; in rari casi sono stati segnalati dolori crampiformi addominali , vomito e irritazione rettale . 
 tecnica dellesame ecografico stato effettuato un esame dettagliato del tratto gastrointestinale utilizzando apparecchi in commercio ( antares , siemens medical solutions , erlangen , germania ; aplio , toshiba , tokio , giappone ) , con sonde standard multi - frequenza di tipo convex da 4 mhz e lineari da 8 o 10 mhz . 
therefore , for each patient , all quadrants of the abdomen were sequentially scanned , initially using a 4 - mhz frequency transducer for a preliminary survey and then using a high - frequency 8 or 10 - mhz transducer for a detailed , high - resolution study ( baseline study )  . 
 after completing the baseline study , each patient drank 750 ml of the abovementioned polyethylene glycol solution ; a reduced fluid volume ( 500 ml ) was administered in two paediatric patients ( 11 and 15 years old ) owing to the smaller body size and in four adults due to poor patient acceptance ( one patient was in poor general condition ; three complained of nausea while drinking the solution and refused to ingest the entire volume )  . 
bowel loops are actually visualised by sonography even when collapsed , but in such condition , they are neither clearly identified nor can their anatomical features be adequately assessed : in this regard , an indistinct appearance of bowel loops , collapsed and not separately recognisable , digiuno di alcune ore , non stata richiesta ai pazienti nessuna particolare dieta o preparazione con lassativi ; non sono stati somministrati farmaci antiperistaltici prima dellesame . 
 allistologia le alterazioni mucose proprie della celiachia si riscontrano soprattutto a livello del duodeno e del digiuno prossimale , ma possono comunque avere unestensione molto variabile e interessare solo tratti limitati o anche lintera lunghezza dellintestino tenue . 
di conseguenza per ogni paziente sono stati esaminati tutti i quadranti addominali in successione , prima con sonda da 4 mhz per una valutazione preliminare e poi con sonda ad alta frequenza da 8 o 10 mhz per uno studio di dettaglio ad alta risoluzione ( esame basale )  . 
analogamente per entrambi i tipi di sonda stata selezionata la frequenza di emissione pi adatta a seconda della costituzione fisica del paziente , in modo da avere sia una buona trasmissione in profondit che una risoluzione ottimale . 
non stata fatta alcuna analisi doppler della vascolarizzazione mesenterica , per evitare un eccessivo prolungarsi della procedura . una volta completato lo studio basale , ogni paziente ha bevuto 750 ml della soluzione di polietilenglicole precedentemente descritta ; stato somministrato un volume di soluzione ridotto ( 500 ml ) in 2 pazienti pediatrici ( 11 e 15 anni di et ) in rapporto alle minori dimensioni corporee , e in 4 adulti per scarsa tolleranza da parte dei pazienti stessi ( 1 paziente era in condizioni generali scadenti ; 3 pazienti hanno riferito nausea allingestione della soluzione e non hanno voluto assumere lintero volume previsto )  . 
dopo 30 40 minuti lesame ecografico stato ripetuto ( esame dopo contrasto ) con le stesse modalit descritte precedentemente ( ossia con sonde a bassa e ad alta frequenza ) utilizzando per ogni paziente la stessa apparecchiatura e regolazioni del precedente esame basale , e valutando se lintero intestino tenue fosse adeguatamente disteso e se la soluzione avesse raggiunto il colon ascendente . 
per ogni paziente sono stati infatti confrontati lesame pree post - contrasto , in modo da verificare se la somministrazione di fluido avesse o meno migliorato la visibilit delle anse intestinali , e se quindi fosse stata utile per identificare eventuali alterazioni dovute a malattia celiaca , secondo i criteri ecografici [ 1419 ] o radiologici [ 2125 ]  . 
 la visibilit complessiva dellintestino tenue stata valutata soggettivamente in base alla relativa proporzione tra anse del tenue ben distese e anse poco o affatto distese radiol med ( 2012 ) 117 : 558574 fig . 
1a , b baseline ( a ) and postcontrast ( b ) scans of the left lower quadrant with an 8 - mhz linear transducer in the same patient ( with the same transducer and equipment settings ) on baseline examination , the small - bowel loops contain gas with reverberation artefacts ; abnormal thickening of bowel walls , such as in chronic inflammatory disease , can be excluded , but no further assessment can be made . 
esame basale ( a ) e dopo contrasto ( b ) del quadrante inferiore sinistro delladdome , con sonda lineare da 8 mhz , nello stesso paziente ( stessa sonda e regolazioni dellapparecchio )  . 
allesame basale le anse del tenue contengono gas con artefatti da riverbero ; si pu escludere un ispessimento patologico delle pareti a tipo malattia infiammatoria cronica , ma non possibile rilevare altri elementi di valutazione . 
the wilcoxon signed rank test for two related samples was applied to determine a statistically significant difference between examination quality obtained before and after fluid distension of the small bowel . 
a p value < 0.05 was considered statistically significant . sonographic signs of coeliac disease reported in the literature include intestinal and extraintestinal abnormalities [ 1419 ] and changes of mesenteric flow on doppler evaluation . 
stato applicato il test di wilcoxon a ranghi appaiati per due gruppi correlati per determinare se vi fosse una differenza statisticamente significativa tra la qualit dellesame ecografico prima e dopo distensione fluida del tenue , considerando come statisticamente significativo un valore di p inferiore a 0 , 05 . 
nel presente studio abbiamo considerato soprattutto il riconoscimento dei segni intestinali di malattia celiaca ( agli esami prima e dopo contrasto ) , rappresentati da : incremento della quota fluida endoluminale ( che riflette laumento di permeabilit e di secrezioni ) ; dilatazione di grado moderato delle anse interadiol med ( 2012 ) 117 : 558574 results concerning patients acceptance and examination side effects , no patient refused to drink the polyethylene glycol solution or complained of significant adverse reactions . 
 one patient reported loose stools after the examination ; three adult patients reported mild nausea when drinking the solution ( and thus did not ingest the entire amount )  . 
overstinali ( diametro > 25 mm ) ; ispessimento delle pareti intestinali ( > 3 mm ) ; inversione del pattern plicare nei segmenti digiunali e ileali ( aumento di numero delle pliche ileali a fronte di riduzione o assenza delle pliche digiunali ) cos come ispessimento o appiattimento delle pliche ; alterazioni della motilit del tenue ( valutate soggettivamente , nel presente studio cos come in altri precedenti in letteratura , e interpretate come dovute ad alterazioni funzionali per effetto neurotossico del glutine , con interferenza sulla normale attivit peristaltica ) , e che si manifestano come aumento o riduzione dellattivit peristaltica , ipotonia e distensione delle anse , invaginazioni transitorie senza effetti occlusivi . 
 circa questultimo punto , un aumento di attivit peristaltica stato considerato come possibile segno di celiachia se rilevato allesame basale , e come non significativo ( ossia probabilmente dovuto alla somministrazione di fluido ) se rilevato invece solo allesame dopo contrasto . 
 risultati per quanto riguarda il grado di accettazione da parte dei pazienti e gli effetti collaterali della procedura , nessuno dei nostri pazienti ha rifiutato di bere la soluzione di polietilenglicole o ha lamentato reazioni sfavorevoli importanti . 
un paziente ha riferito alvo diarroico a seguito dellesame ; tre pazienti adulti hanno riferito lieve nausea quando hanno iniziato a bere la soluzione ( e quindi non hanno assunto lintero volume previsto )  . 
lesame dopo contrasto ( con sonda lineare da 10 mhz ) del quadrante superiore sinistro ( a ) e del quadrante inferiore destro ( b ) delladdome nello stesso paziente mostra normale calibro delle anse digiunali e ileali , e la corrispondente morfologia di parete : i segmenti digiunali ( a ) hanno rilevo plicare ben rappresentato , mentre i segmenti ileali ( b ) hanno calibro leggermente pi ampio con pareti lisce . all , however , luminal filling was most times incomplete : the ingested fluid was usually not uniformly distributed over the entire small bowel , as well - distended loops and poorly distended loops were simultaneously present due to normal bowel contractility , and a complete and continuous evaluation of the small bowel was rarely obtained . 
nellinsieme tuttavia il riempimento fluido ottenuto stato il pi delle volte incompleto : il fluido ingerito generalmente non era distribuito in modo uniforme lungo tutto il tenue , in quanto , per la normale contrattilit intestinale , erano contemporaneamente presenti anse ben distese e poco distese , e raramente si ottenuta una valutazione completa e continua del tenue . 
 i restanti casi sono stati classificati come nessun miglioramento ( 9 pazienti , 20% ) , o peggioramento ( 1 paziente , che dopo somministrazione di contrasto ha presentato un netto incremento della motilit intestinale , in assenza di dolori addominali o altra sintomatologia ; 2 , 2% )  . 
 per quanto riguarda lanalisi statistica , il test di wilcoxon a ranghi appaiati ha dimostrato una differenza altamente significativa ( p < 0 , 0001 ) tra le due modalit di esame . 
complessivamente sono state rilevate invaginazioni transitorie del digiuno o dellileo , in assenza di sintomatologia , in 6 pazienti : in 3 allesame basale , e in altri 3 dopo somministrazione di fluido . 
in 8 pazienti allesame basale si osservava un diffuso ispessimento di parete dei segmenti ileali , non confermato allesame dopo contrasto : la somministrazione di contrasto ha permesso quindi di correggere un aspetto ingannevole dellesame basale ( apparente ispessimento parietale diffuso ) in quanto ha dimostrato correttamente dei segmenti intestinali poco distesi ma in assenza di alterazioni parietali . 
in altri 3 pazienti il riempimento fluido ha permesso una netta riduzione del gas intestinale , evidenziando cos piccoli linfonodi mesenterici ( diametro massimo 1015 mm ) non rilevati in condizioni basali . 
il riscontro di versamento libero , presente in minima quantit in 4 pazienti celiaci , non stato influenzato dalla somministrazione di contrasto ed era facilmente visibile sia agli esami basali che dopo contrasto . 
transverse scan ( a ) of the right lower quadrant of the abdomen shows anechoic fluid filling the terminal ileum ( il ) and ascending colon ( c ) ; parietal folds ( callipers 2 mm ) are increased in number ( so - called jejunalised ileum )  . 
a la scansione trasversale del quadrante inferiore destro delladdome mostra lileo terminale ( il ) e il colon ascendente ( c ) distesi da fluido ecoprivo ; le pliche parietali ( calipers = 2 mm ) sono aumentate di numero ( cosiddetta digiunalizzazione dellileo )  . 
allo studio ad alta risoluzione ( b ) la distensione fluida permette di apprezzare in dettaglio la morfologia del rilievo plicare e la struttura stratificata della parete intestinale , con spessore normale ( calipers < 2 mm )  . radiol med ( 2012 ) 117 : 558574 fig . 
8a , b crohns disease of the terminal ileubaseline ( a ) and postcontrast ( b ) scans of the right lower quadrant ( 10 - mhz transducer )  . 
in three other patients , luminal filling resulted in a significant reduction of bowel gas , thus revealing small mesenteric lymph nodes ( 1015 mm ) not detected at the previous baseline examination . 
 discussione nello studio del tratto gastroenterico lecografia ha delle notevoli limitazioni , tra cui in particolare linterferenza da gas endoluminale : alcune di queste limitazioni possono essere almeno in parte superate mediante il riempimento fluido dei segmenti digiuno - ileali . 
il fluido nel lume intestinale sposta il gas che impedisce lo studio ecografico e agisce come un mezzo di contrasto acustico , permettendo cos una chiara visualizzazione delle pareti intestinali e delle valvole conniventi : si possono meglio differenziare tra loro i segmenti digiunali e ileali , e identificare condizioni di normalit o di 570 discussion with regard to study of the gastrointestinal tract , sonography has significant inherent limitations , chiefly interference by gas within the bowel lumen . 
fluid within the bowel displaces obscuring bowel gas and acts as an acoustic contrast , thus allowing clear depiction of intestinal walls and parietal - fold relief : jejunal and ileal loops can be better differentiated , and normal or abnormal conditions can be better identified based on thickness , layered structure and mucosal - fold pattern of the bowel wall . 
 small - bowel filling may be obtained by using echo - poor fluids , such as water or nonabsorbable solutions , and has also been used for the ct or mr assessment of the small bowel [ 2630 ]  . 
isotonic polyethylene glycol solutions are considered by many authors as being the most suitable for luminal distension , in different amounts as concerns the sonographic literature depending on the administration route , i.e. 
in our study , we chose a volume of solution that might be comparable with previous studies that also used oral administration , preferring , however , an amount of 750 ml to achieve better bowel - lumen distension . 
the intestinal and extraintestinal changes of the small bowel in overt coeliac disease have been described by several sonographic , ct and mr studies performed using conventional techniques [ 1419 , 21 , 23 ] or luminalfilling techniques [ 11 , 2325 , 29 , 32 ]  . 
the aim of our study , however , was not to investigate the diagnostic accuracy of us in predicting coeliac disease but rather to assess the actual value of fluid distension for demonstrating sonographic features of the small bowel . 
in fact , other small - bowel diseases , such as crohns disease , lymphoma or tumours , result in focal abnormalities with evident bowel - wall thickening , which are usually well recognised radiol med ( 2012 ) 117 : 558574 patologia sulla base di parametri quali spessore e struttura a strati delle pareti intestinali e caratteri del disegno plicare . 
 per il riempimento fluido , utilizzato nello studio del tenue anche con altre metodiche di imaging come tc e rm , si possono usare liquidi ecoprivi quali acqua o altre soluzioni nonassorbibili [ 2630 ]  . 
le soluzioni isotoniche di polietilenglicole sono ritenute da pi autori le pi idonee per una buona distensione del tenue , con volumi di soluzione differenti per quanto riguarda la letteratura ecografica a seconda della via di somministrazione , ossia per somministrazione orale [ 713 ] o intubazione con sondino naso - digiunale [ 5 , 6 ]  . 
nel nostro studio abbiamo scelto di utilizzare un volume di soluzione che potesse essere confrontabile con altri studi precedenti basati anchessi sulla somministrazione orale , orientandoci tuttavia per un volume di 750 ml allo scopo di ottenere una distensione intestinale migliore . 
le modificazioni intestinali ed extraintestinali dellintestino tenue nella celiachia conclamata sono state descritte da vari studi ecografici , tc , e rm , effettuati con tecnica convenzionale [ 1419 , 21 , 23 ] o previa distensione endoluminale [ 11 , 2325 , 29 , 32 ] : tutti questi studi descrivono la gamma dei reperti tipici della celiachia oppure sono finalizzati a stabilire laccuratezza di tali tecniche nel riconoscimento della celiachia . 
nel presente lavoro tuttavia non ci siamo proposti di stabilire laccuratezza diagnostica dellecografia nel riconoscimento della celiachia , ma piuttosto di definire leffettiva utilit della distensione fluida per dimostrare i caratteri ecografici dellintestino tenue . 
in effetti altre patologie del tenue quali morbo di crohn , linfomi , tumori si manifestano come alterazioni focali o segmentarie con evidente ispessimento parietale , che sono di solito ben riconoscibili allecografia e non necessitano quindi di una specifica tecnica di esame . 
invece la malattia celiaca ( o enteropatia da glutine ) pu interessare tutto lintestino tenue , ma i possibili segni della malattia possono essere sfumati e difficili da riconoscere per tutte le tecniche di imaging se non si effettua un esame dedicato : su queste premesse abbiamo deciso di confrontare lefficacia dellecografia convenzionale e dopo contrasto orale nella ricerca di alterazioni meno appariscenti , come sono appunto radiol med ( 2012 ) 117 : 558574 by sonography and do not require a specific examination technique . 
coeliac disease ( gluten enteropathy ) , instead , can affect the entire small bowel , but the possible signs of this condition may be subtle and quite difficult to appreciate by any imaging technique unless a dedicated examination is performed . 
in this regard , we decided to compare the effectiveness of conventional sonography and oral contrast - enhanced sonography in detecting minor abnormalities , such as those recognised as signs of coeliac disease . 
 in our experience , the main drawbacks of luminal distension by fluid are possible patient discomfort and the additional time required for progression of the ingested fluid through the bowel ; however , solution costs are negligible . 
 concerning possible adverse effects , the technique is quite feasible in the majority of patients , with the only exception being sick and debilitated patients , in whom ingestion of a large volume of fluid may induce nausea or vomiting . 
although the procedure was , on the whole , well tolerated in most cases , 3 / 45 patients ( 6.6 % ) could not ingest the entire amount of polyethylene glycol due to the onset of nausea while drinking the solution . 
such incidence of adverse effects is in accordance with two previous studies [ 5 , 10 ] , which reported one case each of severe nausea with vomiting due to contrast ingestion and mild to moderate nausea ( 6.9% ) and slight abdominal distension ( 3.9% ) [ 10 ]  . 
the time interval needed for fluid progression through the small bowel ( 3040 min ) was also in accordance with previous reports [ 810 , 12 , 31 ]  . the uniform and uninterrupted filling of the jejunoileal loops described by others [ 7 ] after oral administration was not achieved in the patients we studied . 
conversely , fluid administration is likely to be useless whenever bowel visualisation is already satisfactory in baseline conditions or when abnormal fluid distension is present ( as may be found in untreated coeliac disease )  . 
 luminal filling might thus enhance the confidence level of the examiner in defining whether a suspicious feature is truly associated with parietalor mucosal - fold abnormaliquelle ormai riconosciute come segni di malattia celiaca . 
 nella nostra esperienza gli inconvenienti principali della distensione del lume intestinale mediante somministrazione di fluido sono il possibile disagio per il paziente e il tempo di esame in pi necessario per il transito del fluido attraverso il tenue , mentre i costi della soluzione sono trascurabili . 
 per quanto riguarda i possibili effetti avversi , la tecnica del tutto fattibile nella maggior parte dei pazienti , con lunica eccezione di pazienti che stanno male e in condizioni generali scadute , in cui dover bere una grande quantit di liquidi pu indurre nausea o vomito . 
anche se la procedura stata nellinsieme ben tollerata nella maggior parte dei casi , 3 dei nostri 45 pazienti ( 6 , 6% ) non sono riusciti a bere lintera dose della soluzione di peg proprio per linsorgenza di nausea mentre bevevano la soluzione . 
tale incidenza di effetti sfavorevoli in linea con due studi precedenti [ 5 , 10 ] , che riportavano un caso ciascuno di forte nausea con vomito dovuti allingestione del contrasto , e nausea lieve o moderata ( 6 , 9% ) cos come modesta distensione addominale ( 3 , 9% ) [ 10 ]  . 
anche lintervallo di tempo necessario per il transito del fluido attraverso il tenue ( 3040 min . ) in linea con altri studi precedenti [ 810 , 12 , 31 ]  . 
 nei pazienti da noi studiati non abbiamo ottenuto un riempimento uniforme e continuo delle anse digiuno - ileali dopo contrasto per os cos come descritto da altri autori [ 7 ]  . 
al contrario presumibile che la somministrazione di fluido sia inutile qualora la visibilit del tenue sia gi soddisfacente in condizioni basali o qualora ci sia una abnorme distensione fluida ( eventualit possibile nella malattia celiaca non trattata )  . 
il riempimento fluido endoluminale potrebbe quindi aumentare il grado di sicurezza dellesaminatore nel definire se un aspetto dubbio sia effettivamente espressione di alterazioni parietali o plicari o sia invece apparente ( perch dovuto ad unansa collabita che simula un ispessimento parietale anomalo )  . 
in fact , scintigraphic studies have demonstrated that polyethylene glycol - containing preparations have a marked accelerating effect on small - intestinal liquid transit ( about 35% reduced transit time ) [ 33 ]  . 
nevertheless , in our experience , sonography coupled with luminal distension by oral administration of fluid is a feasible , low - cost technique and has the potential to provide high - quality images of small - bowel segments , besides being a means to possibly improve poor - quality examinations . 
given the noninvasiveness and almost no adjunctive costs of orally administered contrast enhancement sonography , its use coupled with a meticulous examination with high - resolution transducers seems justified to identify different bowel diseases . 
le alterazioni della motilit intestinale riportate nei pazienti celiaci [ 11 , 1418 ] comprendono distensione delle anse per incremento della quota fluida endoluminale e iperperistaltismo ( rilevati in 7 e 4 dei pazienti celiaci da noi studiati ) o anche anse flaccide ipotoniche con riduzione della motilit intestinale . 
in effetti stato dimostrato da studi scintigrafici che le preparazioni contenenti peg hanno un marcato effetto di accelerazione sul transito dei liquidi nellintestino tenue ( con riduzione del tempo di transito del 35% circa ) [ 33 ]  . 
sia un eventuale aumento del contenuto fluido che alterazioni della motilit intestinale di conseguenza devono ovviamente essere valutati in condizioni basali , per evitare di misconoscere questi segni di celiachia attribuendoli erroneamente alla somministrazione di fluido . 
 dobbiamo riconoscere che la casistica presentata non omogenea ( dato che comprendeva pazienti celiaci in trattamento e non , e pazienti non celiaci ) , e questo indubbiamente costituisce un limite del nostro studio . 
ci nonostante nella nostra esperienza lecografia accoppiata alla distensione endoluminale mediante somministrazione orale di liquidi una tecnica fattibile , a basso costo , ed potenzialmente in grado di rappresentare lintestino tenue con immagini di qualit elevata , oltre a costituire un mezzo per provare a migliorare esami di scarsa qualit . 
data la sua non invasivit e la pressoch totale assenza di costi aggiuntivi , limpiego dellecografia con mezzo di contrasto per os , unita ad un esame meticoloso con sonde ad alta risoluzione , appare giustificato in varie patologie digeradiol med ( 2012 ) 117 : 558574 abnormalities already evident on conventional abdominal sonography ; rather it should be used to detect minor abnormalities in selected cases and , broadly speaking , whenever a high - resolution and detailed study of intestinal loops is necessary . stive non come esame di routine n per confermare alterazioni gi evidenti allecografia addominale convenzionale , ma piuttosto , in casi selezionati , per ricercare alterazioni meno evidenti , e in generale ogniqualvolta sia necessario uno studio dettagliato e ad alta risoluzione delle anse intestinali . 
tunac1 1radiology department , istanbul faculty of medicine , istanbul university , millet caddesi , capa , 34390 istanbul , turkey 2pathology department , istanbul university , istanbul faculty of medicine , istanbul , turkey 3general surgery department , istanbul faculty of medicine , istanbul university , istanbul , turkey correspondence to : a . 
altri segni ecografici tipici erano diffuse formazioni ascessuali con fistole , caratterizzate da intensa eterogeneit in 12 ( 33% ) donne ed ipoecogenicit parenchimale in 5 ( 13% ) donne . 
although not characteristic for this entity , asymmetric density on mammography , solitary or multiple clustered heterogeneous hypoechogenicity with a tubular configuration on sonography and round , smooth - contoured masslike lesion with rim enhancement or segmental non - mass - like lesion on mri are the most common features of the disease . keyword idiopathic granulomatous mastitis mammography ultrasonography mr imaging breast carcinoma magnetica , lesioni masslike sono state rilevate in 24 pazienti , mentre lesioni non - masslike sono state osservate in 28 donne . 
sebbene non specifiche di questa entit , le pi comuni caratteristiche della mastite granulomatosa idiopatica sono risultate essere : lesioni con densit asimmetrica alla mammografia , lesioni eterogeneamente ipoecogne , solitarie o multiple , con configurazione tubulare , in ecografia , e lesioni masslike , rotondeggianti a margini lisci , con enhancement anulare , o lesioni segmentate non - masslike , in risonanza magnetica . 
 parole chiave mastite granulomatosa idiopatica mammografia ecografia rm carcinoma mammario introduction idiopathic granulomatous mastitis ( igm ) , first described as a specific entity by kessler and wolloch [ 1 ] in 1972 and further elaborated by cohen [ 2 ] in 1977 , is a rare chronic inflammatory breast lesion with an unknown aetiology , clinically simulating breast carcinoma [ 3 , 4 ]  . 
the most common clinical presentation is with a unilateral , firm discrete breast mass , often associated with inflammation of the overlying skin , which may lead to nipple retraction and sinus formation [ 7 , 8 ]  . 
 imaging findings of this condition have been relatively well described by mammography and ultrasonography ( us ) ; however , there are only a few case reports , and two series of seven and nine cases evaluating magnetic resonance imaging ( mri ) features [ 814 ]  . 
the purpose of this report is to describe img imaging characteristics at mammography , us and mri in a series of 36 cases , by far the largest imaging series reported in the literature . materials and methods we retrospectively evaluated 36 patients ( mean age 37 years ; range 2151 years ) with histologically confirmed igm between may 1996 and june 2008 . 
the institutional review board approved this study , and informed consent was obtained from all participants . igm was defined pathologically as a granulomatous inflammatory reaction centred on mammary lobules in the absence of caseous necrosis or any specific organisthree modalities ( mammography , sonography and mr mammography ) were available in all patients with the exception of two mammographic evaluations in two patients , of whom one had breast implants and the other who was too young ( 21 years ) to have a mammogra mammography was performed only on the affected breast in patients < 35 years of age ( n = 18 )  . 
mri was performed with two different scanners , a 1 - tesla unit ( magnetom impact , siemens medical systems , erlangen , germany ) and a 1.5 - tesla unit ( symphony , siemens medical systems , erlangen , germany ) by using a dedicated breast coil with the patient in the prone position . 
the scanning protocol included axial t2 - weighted fat - suppressed spin - echo sequence followed by an axial precontrast 3d turbo fast low - angle shot ( 3d turbo flash ) sequence . 
non - masslike enhancement is described according to the distribution ( clumped , ductal , segmental , regional or diffuse ) and internal enhancement pattern ( homogeneous , heterogeneous , clumped , punctuate or reticular )  . 
the time - signal intensity curves of the enhancing masses or non - mass - like enhancements were obtained by using dedicated software ( mean curve ; leonardo , siemens , erlangen , germany )  . 
 additional findings such as skin thickening , skin and nipple retraction and breast oedema were also noted . mri classification mammographic findings mri findings were classified according to the breast imaging reporting and data system ( bi - rads ) mri lexicon developed by the american college of radiology in 2003 . 
1a - d mammografia craniocaudale di pazienti con mastite granulomatosa : densit asimmetriche ( frecce sottili ) in a , massa densa mal definita ( freccia spessa ) in b , masse circoscritte solitarie o multiple ( asterischi ) in c e distorsione architetturale ( punte di freccia ) in d . 
skin retraction or thickening was detected in 19 patients ( 55% )  . mass lesions ultrasonography findings the most frequent us finding was solitary or multiple circumscribed heterogeneous hypoechoic masses with tubular configuration , which was detected in 19 patients ( 52% )  . 
3a - c precontrast t1and t2 - weighted magnetic resonance images and postcontrast t1 - weighted image with fat suppression of a 49 - yearold woman with granulomatous mastitis demonstrate different imaging appearances reflecting different stages of disease . 
3a - c immagini precontrastografiche t1 e t2 pesate e immagini postcontrastografiche t1 pesate con soppressione del grasso di una donna di 49 anni con mastite granulomatosa dimostrano diversi aspetti allimaging che riflettono le differenti fasi di malattia . 
in 14 cases ( 38% ) the time - signal intensity curve revealed gradual and progressive enhancement , and in 12 patients ( 33% ) , a plateau - like pattern following early contrast enhancement . 
in ten patients ( 27% ) , signal intensity showed initial increase within the first 3 min , followed by a subsequent washout of contrast mediuin addition to these findings , diffuse breast oedema was noted in 22 patients , skin thickening in 19 , skin retraction in seven and nipple retraction in four . discussion idiopathic granulomatous mastitis is a rare benign inflammatory disease of unknown aetiology . 
4a - c axial subtracted magnetic resonance images of different patients show the spiculated ( asterisk ) and smooth ( thin arrow ) contoured mass lesions with rim enhancement , oval - shaped mass lesion with homogeneous ( thick arrowheads ) enhancement , segmental non - mass - like lesion with heterogeneous enhancement ( thin arrowheads ) and the clumped non - mass - like lesions ( thick arrow )  . 
4a - c immagini assiali di sottrazione in risonanza magnetica nelle diverse pazienti mostrano lesioni masslike spiculate ( asterisco ) e liscie ( freccia sottile ) , lesioni a margini definiti con enhancement anulare , lesioni masslike di forma ovalare con enhancement omogeneo ( punte di freccia spesse ) , lesione segmentate non - masslike con enhancement disomogeneo ( punte di freccia sottili ) e lesioni nonmasslike formanti conglomerato ( freccia spessa )  . 
la curva tempo - intesit di segnale dimostra un incremento iniziale e un successivo wash - out . mri features of igm have been reported in only a few case reports and two series of seven and nine cases [ 814 ]  . 
 these reports demonstrated that igm has a wide spectrum of imaging findings , such as ring - like enhancement , intensively and strongly enhancing irregular mass and focal homogeneous enhancing masses [ 1012 , 2527 ]  . 
in this report , the mri characteristics were classified according to the bi - rads lexicon , and non - mass - like enhancement was a more common finding than mass lesions . 
the order of frequency of non - mass - like distribution pattern , enhancement was segmental , ductal and regional ( n = 12 , n = 9 and n = 8 , respectively )  . 
the most important entity in the differential diagnosis of igm is breast carcinoma . many igm imaging findings may be similar to those of breast carcinoma [ 28 , 29 ]  . 
5a - c axial subtracted magnetic resonance images of different patients demonstrate segmental ( arrowheads , a ) , ductal ( thick arrow , b ) and clumped non - mass - like lesions ( thin arrows , c )  . 
5a - c immagini assiali di sottrazione in risonanza magnetica nelle diverse pazienti mostrano lesioni segmentali ( punte di freccia ) in a , duttali ( freccia spessa ) in b e non - masslike a grappolo ( frecce sottili ) in c . 
6a - d axial precontrast t1 - weighted flash ( a ) , postcontrast flash ( b ) , subtracted magnetic resonance images ( c ) of a 51 - year - old woman with granulomatous mastitis show a non - mass - like segmental enhancement pattern ( arrowhead )  . 
6a - d immagini di sottrazione in risonanza magnetica , assiali ( a ) precontrastografiche flash t1 pesate ( b ) , e postcontrastografiche flash ( c ) , di una donna di 51 anni con mastite granulomatosa , mostrano un pattern di enhancement nonmasslike segmentale ( punta di freccia )  . 
7a - c axial subtracted magnetic resonance images of different patients with diagnoses of granulomatous mastitis shows the non - mass - like lesion with reticular and punctuate enhancement ( arrowheads , a , b )  . 
7a - c immagini assiali di sottrazione in risonanza magnetica in diverse pazienti con diagnosi di mastite granulomatosa , mostrano lesioni non - masslike con enhancement reticolare e punteggiato ( punte di freccia ) in a e b . 
axial t2 - weighted magnetic resonance images ( a , d ) , precontrast ( b , e ) and postcontrast ( c , f ) t1 - weighted images show non - mass - like heterogeneous enhancement pattern with grape - like enhancement compatible with microabscess formation ( arrowheads )  . 
immagini assiali t2 - pesate ( a , d ) , precontrastografiche t1 - pesate ( b , e ) e postcontrastografiche t1 - pesate ( c , f ) , mostrano pattern di enhancement eterogeneo non - masslike con grape - like enhacement compatibile con formazione micro - ascessuale ( punte di freccia )  . 
therefore , it is not always easy to differentiate igm from abscess , but in the presence of a fistulous tract and grape - like enhancement secondary to microabscesses , igm should be considered . 
detecting a nonenhancing fat component on mri and the presence of a history attributable to fat necrosis is important in the differential diagnosis [ 32 ]  . in our study , we evaluated the imaging characteristics of igm in a series of 36 cases , by far the largest imaging series reported in the literature , and we concluded that igm very often mimics breast carcinoma . 
the study group consisted of 42 patients with idiopathic ileocecocolic intussusception treated with us - e ( 20 patients ) or rx - e ( 23 patients ) , with one patient undergoing both procedures owing to recurrence . 
as us - e avoids radiation exposure , it should be considered the first - choice procedure for reducing idiopathic ileocecocolic intussusception , particularly in these two subgroups of patients . keywords intussusception ultrasonography hydrostatic reduction hartmanns solution enema gastrografin enema paediatric riassunto obiettivo . 
sono stati inclusi nello studio 42 pazienti ricoverati consecutivamente per invaginazione idiopatica ileo - ceco - colica e sottoposti a us - e ( 20 casi ) o a rx - e ( 23 casi ) , con 1 paziente trattato con entrambe le procedure per recidiva dellinvaginazione . 
il us - e risulta pi efficace nei pazienti di et superiore ai 12 mesi e nei casi in cui c stato esordio della sintomatologia da pi di 24 ore . 
poich il us - e non comporta esposizione radiologica , da considerarsi metodica di prima scelta per la riduzione dellinvaginazione idiopatica ileo - ceco - colica , in particolare in questi due sottogruppi di pazienti . 680 radiol med ( 2012 ) 117 : 679689 parole chiave invaginazione ultrasonografia riduzione idrostatica soluzione di hartmann gastrografin pediatria introduction introduzione the most common cause of acute bowel obstruction in infants is intussusception and primarily occurs in the first 3 years of life , with a peak incidence from 5 to 10 months . 
unlike adult intussusception , < 5% in infants are caused by a pathological lead point ( plp ) , such as meckels diverticulum , intestinal polyps , lymphomas or neoplasms . 
this rate is reported to increase up to 60% in children > 5 years of age [ 13 ]  . in the last 30 years , there has been much debate regarding the diagnostic and therapeutic management of intussusception . 
 fluoroscopy - guided liquid enema , performed with barium or water - soluble contrast material , has been the traditional means of intussusception diagnosis and the first nonsurgical procedure for reduction [ 4 ]  . 
us is used not only as the primary diagnostic tool in children suspected to have intussusception but also to guide nonsurgical reduction , performed with either warm saline , hartmanns solution , or - more recentlyair [ 1 , 69 ]  . 
reported success rates are comparable and even superior to those achieved with radiological procedures [ 10 ]  . consistent with the international trend towards the use of radiation - free procedures , in 1991 we began diagnostic us examinations in our department after training a paediatric surgeon in the use of us . 
after acquiring skills and experience with us , in 2000 , the same paediatric surgeon , with a staff of residents and nurses , began performing usguided operative procedures , including reducing intussuslinvaginazione intestinale la causa pi comune di occlusione intestinale acuta in et infantile , verificandosi per lo pi nei primi tre anni di vita e con un picco dincidenza tra 5 e 10 mesi . 
sono idiopatici circa il 95% di tutti i casi dinvaginazione in tale tipica et , legati alliperplasia del tessuto linfoide nellileo distale , che agisce da lead point patologico ( lpp )  . 
a differenza dellinvaginazione nelladulto , meno del 5% delle invaginazioni in et infantile dovuto ad un lpp , come il diverticolo di meckel , i polipi intestinali , i linfomi o le neoplasie . 
tale percentuale aumenta fino al 60% nei bambini di et superiore ai 5 anni [ 13 ]  . negli ultimi 30 anni si sviluppato un intenso dibattito circa il management diagnostico - terapeutico nellinvaginazione . 
il clisma radiologico liquido , eseguito con il bario o con mezzi di contrasto idrosolubili , stata la tradizionale tecnica per la diagnosi dinvaginazione e la procedura non chirurgica di scelta per la sua riduzione [ 4 ]  . 
in seguito il clisma radiologico pneumatico ha giovato di una crescente approvazione grazie alla maggior percentuale di successo e alla minor radio - esposizione rispetto al clisma radiologico liquido [ 5 ]  . 
recentemente lultrasonografia ( us ) diventata la tecnica dimaging di prima scelta nella diagnosi dellinvaginazione , grazie alla sua accuratezza , alla simultanea possibilit di eseguire diagnosi differenziale e alla sua non invasivit . 
lus stata utilizzata non solo come indagine di i livello nei bambini con sospetto dinvaginazione , ma anche per monitorare la sua riduzione non chirurgica , eseguita con soluzione fisiologica , con soluzione di hartmann e , pi di recente , con aria [ 1 , 69 ]  . 
la percentuale di successo riportata in letteratura comparabile se non superiore a quella ottenuta dalle procedure radiologiche [ 10 ]  . coerentemente al trend nella letteratura internazionale circa limpiego di procedure prive di radiazioni ionizzanti , nel nostro dipartimento abbiamo iniziato a eseguire esami diagnostici us dal 1991 , grazie al training di un chirurgo pediatra nellesecuzione di us . 
in principio abbiamo utilizzato lus solo quale mezzo diagnostico nelle invaginazioni , continuando a eseguire a fini terapeutici le tecniche radiologiche , nello specifico il clisma radiologico con gastrografdopo aver acquisito competenza ed esperienza nellus , dal 2000 il medesimo chirurgo pediatra , supportato da uno staff di spe cializzandi e infermieri , ha iniziato a eseguire procedure operative eco - guidate , tra cui la riduzione dellinvaginazione at traverso il clisma con soluzione di hartmann , che oggi la no radiol med ( 2012 ) 117 : 679689 ception with hartmanns solution enema , which today is our procedure of choice in managing intussusception . the aim of our study was to compare outcomes of usguided hartmanns solution enema ( us - e ) and radiological liquid enema ( rx - e ) in reducing idiopathic ileocecocolic intussusception and to evaluate which patients benefit from each procedure in relation to age and symptom duration . stra procedura di scelta nel management dellinvaginazione . scopo del nostro lavoro comparare i risultati del clisma con soluzione di hartmann us - guidato ( us - e ) e del clisma radiologico liquido ( rx - e ) nella riduzione dellinvaginazione ileo - ceco - colica idiopatica e di valutare quali pazienti possano beneficiare delluna o dellaltra procedura in funzione della loro et e della durata dei sintomi . materials and methods we retrospectively reviewed clinical records and imaging studies of all consecutive patients admitted to our department with a us diagnosis of intussusception over a 10 - year period ( 20002009 )  . 
a nonsurgical attempt at reduction was then performed by a radiologist assisted by a paediatric surgeon in the case of rx - e , and by the same paediatric surgeon in the case of us - e . 
procedure choice was based on availability of the attendant of our sonographic staff . rx - e was performed with a foley catheter of the largest appropriate size ( 1224 f ) inserted into the rectum , the balloon was inflated with saline solution and the patient was placed in a supine position with thighs pressed together to ensure a tight anal seal . 
during the procedure , fluoroscopy was used intermittently to observe flow of the contrast column into the colon and retrograde motion of the materiali e metodi abbiamo esaminato retrospettivamente le cartelle cliniche e gli esami di diagnostica per immagini di tutti i pazienti ricoverati nel nostro dipartimento con una diagnosi ultrasonografica dinvaginazione nel corso di una decade ( 2000 2009 )  . 
sono stati quindi condotti tentativi di riduzione non chirurgica dellinvaginazione , eseguiti da un radiologo in presenza di un chirurgo pediatra nel caso del rx - e , o dal medesimo chirurgo pediatra nel caso del us - e . 
 il rx - e stato eseguito con un catetere foley del maggior calibro possibile in base al soma del bambino ( 1224 f ) , inserito nel retto , con il palloncino riempito di soluzione fisiologica e con il paziente posto in posizione supina con le gambe ben strette al fine di ottenere una serrata chiusura dellorifizio anale . 
la colonna di contrasto stata ottenuta collocando la sacca con il contrasto 100150 cm sopra il livello del tavolo radiologico , al fine di assicurare una pressione massima di 120 mmhg . 
durante tale procedura la radioscopia stata utilizzata in maniera intermittente al fine di osserspontaneous resolution of intussusception patients with gross abdominal distension , signs of peritonitis or shock , treated with primary surgery intussusception other than ileocecocolic intussusception secondary to pathological lead points ( meckels diverticulum ) table 1 exclusion criteria exclusion criteria tabella 1 criteri di esclusione criteri di esclusione risoluzione spontanea dellinvaginazione pazienti con severa distensione addominale , segni di peritonite o shock , sottoposti dambl a trattamento chirurgico invaginazione non ileo - ceco - colica invaginazione secondaria a lead points patologici ( diverticolo di meckel ) patients , n pazienti , n 682 radiol med ( 2012 ) 117 : 679689 fig . 
1a - c clisma radiologico con gastrografin che evidenzia la testa dellinvaginato alla flessura epatica ( a ) ed il suo spostamento retrogrado verso la valvola ileo - cecale ( b ) fino alla riduzione completa dellinvaginazione ( c )  . intussusceptum towards the ileocecal valve . 
under sonographic guidance ( siemens g50 with 3 - 5 mhz convex and 710 mhz linear transducers ) , a column of hartmanns solution , a sodium lactate compound , isotonic with blood and extracellular fluid ( 131 mmol / l sodium , 11 mmol / l chloride , 29 mmol / l lactate , 5 mmol / l potassium and 4 mmol / l calcium ) , was delivered from a reservoir positioned 100150 cm above the table level to ensure a maximum of 120 mmhg pressure . 
those with complete reduction without surgery were monitored up to 36 h , with vare il fluire del mezzo di contrasto nel colon e il movimento retrogrado dellintestino invaginato verso la valvola ileocecale . 
sotto guida us ( siemens g50 con sonda convex da 35 mhz e sonda lineare da 710 mhz ) una colonna di soluzione di hartmann , un composto di lattato di sodio , isotonico rispetto al sangue e al liquido extracellulare ( 131 mmol / l di sodio , 11 mmol / l di cloruro , 29 mmol / l di lattato , 5 mmol / l di potassio e 4 mmol / l di calcio ) , stata rilasciata da una sacca posta 100150 cm sopra il livello del lettino medico , al fine di assicurare una pressione massima di 120 mmhg . 
il movimento retrogrado dellintestino invaginato e il fluire del mezzo di contrasto sono stati monitorati per via ultrasonografica , cos come la cavit peritoneale al fine di escludere perforazioni intestinali . 
i criteri ultrasonografici per la completa riduzione sono stati la scomparsa dellinvaginazione e il passaggio della soluzione di hartmann e delle bolle di aria nellileo distale attraverso la valvola ileocecale . 
2a - d clisma eco - guidato con soluzione di hartmann che evidenzia laspetto caratteristico a ciambella dellinvaginazione , mentre la soluzione di hartmann distende il colon distale ( a ) ; il fluido penetra gradualmente allinterno della testa dellinvaginato , causando il suo spostamento retrogrado verso la valvola ileo - cecale ( b ) ; riduzione completa dellinvaginazione con edema rediduo della valvola ileo - cecale ( c ) e passaggio di soluzione di hartmann e bolle daria nellileo distale ( d )  . a repeat us in the case of symptoms to exclude recurrence before discharge . the study population was divided into rx - e and us - e groups according to the reduction procedure used . 
each group was divided into subgroups according to age ( < 6 months , between 6 and 12 months , > 12 months ) and symptom duration before attempted reduction ( < 12 h , between 12 and 24 h , > 24 h )  . consistency regarding sex , age and symptom duration was tested between the two main groups and between subgroups by independent students t tests . 
 chi - square test was performed to check trends in differmonitorati fino a 36 ore nel nostro dipartimento , ripetendo una us in tutti in prossimit della dimissione e al bisogno in caso di sintomi , al fine di escludere una recidiva . i pazienti oggetto dello studio sono stati divisi nei gruppi rx - e e us - e in base alla procedura utilizzata per la riduzione dellinvaginazione . 
ogni gruppo stato diviso in sottogruppi , secondo let ( < 6 mesi , tra 6 e 12 mesi , > 12 mesi ) ed in base alla durata dei sintomi prima del tentativo di riduzione ( < 12 ore , tra 12 e 24 ore , > 24 ore )  . lomogeneit tra i due gruppi principali e tra i corrispettivi sottogruppi circa il sesso , let e la durata dei sintomi stata analizzata attraverso i test t di student indipendenti . 
 stato considerato statisticamente significativo un valore di p inferiore a 0 , 05 . radiol med ( 2012 ) 117 : 679689 risultati fifty - nine patients were admitted to our institution with a us diagnosis of intussusception between 2000 and 2009 . 
success rates of rx - e and us - e in each tra il 2000 ed il 2009 sono stati ricoverati presso il nostro dipartimento 59 pazienti con una diagnosi us di invaginazione . 
sono stati esclusi 17 casi ( tabella 1 ) , quindi la popola zione oggetto del presente studio consta di 42 pazienti ( 29 maschi , 13 femmine ) con unet media di 1 , 7 anni ( range 2 , 3 me si11 , 3 anni ) ed una durata media della sintomatologia precedente il tentativo di riduzione di 23 , 5 ore ( range 572 ore )  . sono stati sottoposti a rx - e 23 bambini e a us - e 20 pazienti ; un solo caso ha eseguito entrambe le procedure a causa della recidiva dellinvaginazione dopo una completa riduzione con us - e . 
come mostrato in tabella 2 , la riduzione completa dellinvaginazione , con mancata necessit di intervento chirurgico , stata ottenuta in 10 / 23 rx - e ( 43 , 5% ) ed in 15 / 20 us - e ( 75% ) ( p = 0 , 0625 )  . 
non sono state rilevate perforazioni n altre complicanze . tutti i sottogruppi divisi secondo let erano sovrapponibili circa la durata dei sintomi , fuorch il sottogruppo di bambini di et > 12 mesi , in cui il sottogruppo sottoposto a us - e mostrava una durata della sintomatologia significativamente maggiore del corrispettivo sottogruppo sottoposto a rx - e ( p = 0 , 037 )  . 
comparing outcomes of rx - e and us - e in subgroups , a statistically significant difference was found only in patients > 12 months ( p = 0.0063 ) ( table 3 )  . 
comparing outcomes between subgroups of the same procedure ( rx - e or us - e ) , no statistically significant trends were found ( p = ns )  . duration - of - symptoms subgroups were all consistent regarding age . 
comparing outcomes of rx - e and us - e in subgroups , a statistically significant difference was found only in patients with a symptom duration > 24 h ( p = 0.0361 ) ( table 4 )  . 
comparing outcomes between subgroups of the same procedure ( rx - e or us - e ) , no statistically significant trends were found ( p = ns )  . confrontando i risultati del rx - e e del us - e nei diversi sottogruppi , stata riscontrata una differenza statisticamente significativa solo nei pazienti con et > 12 mesi ( p = 0 , 0063 ) ( tabella 3 )  . 
confrontando i risultati tra i diversi sottogruppi sottoposti alla medesima procedura ( rx - e o us - e ) , non stato notato alcun trend statisticamente significativo ( p = ns )  . i sottogruppi divisi per durata dei sintomi erano sovrapponili riguardo allet . 
confrontando i risultati del rx - e e del us - e in tali sottogruppi , stata riscontrata una differenza statisticamente significativa solo nei pazienti con una durata della sintomatologia > 24 ore ( p = 0 , 0361 ) ( tabella 4 )  . 
esaminando i risultati tra i diversi sottogruppi sottoposti alla medesima procedura ( rx - e o us - e ) , non stato notato alcun trend statisticamente significativo ( p = ns )  . 686 discussion whereas there is agreement that surgery can be avoided in a significant number of children affected by intussusception , some controversial issues still exist about the best nonsurgical reduction technique . 
however , a large , prospective , comparative study is lacking , and an objective comparison between previous reports is difficult due to a lack of standardisation [ 10 ]  . 
they found a statistically significant difference between successful us - e ( 91% ) and barium enema ( 55% ) reductions , both in the overall population and considering idiopathic ileocolic intussusceptions only [ 11 ]  . 
 even if we did not reach a statistically significant difference between rx - e and us - e success rates , the trend is evident . age has been considered an important factor in predicting whether a patient has an intussusception due or not due to plp and thus the chances of reduction without surgery [ 3 ]  . 
in addition , the patient may benefit even from a partial reduction , because this minimises bowel ischaemia and the extent of intestinal resection , if needed [ 12 ]  . 
on the other hand , a considerable portion of intussusceptions in children > 1 year of age is idiopathic , and it is thus worthwhile to try a nonsurgical reduction , especially when us is negative for plp . 
furthermore , in all patients > 1 year treated with us - e , complete reduction was achieved , even though this subgroup also had a significantly longer symptom duration compared with the corresponding rx - e subgroup . 
this is why us - e should be considered the first - choice procedure for these potentially more difficult cases . it seems to be well established that lengthy symptom duration could be deemed a negative prognostic factor for nonsurgical intussusception reduction . 
it is clear that , in the majority of cases , lengthy symptom duration implies extensive impairment of vascularisation , with widespread oedema of the intussuscepted bowel segments , which is more difficult to reduce . 
several authors stated that morradiol med ( 2012 ) 117 : 679689 discussione mentre esiste consenso riguardo la mancata necessit di intervento chirurgico in un rilevante numero di bambini affetti da invaginazione , c ancora controversia circa la miglior tecnica non chirurgica da utilizzare . 
tuttavia in letteratura non abbiamo studi comparativi prospettici e consistenti , ed difficile un oggettivo confronto tra gli studi gi pubblicati , data la mancanza di standardizzazione [ 10 ]  . 
esaminando il successo della riduzione , questi autori hanno riscontrato una differenza statisticamente significativa tra il us - e ( 91% ) ed il clisma radiologico con bario ( 55% ) , sia nella popolazione totale che considerando le sole invaginazioni idiopatiche ileo - coliche . 
nonostante non ci sia una differenza statisticamente significativa tra la percentuale di successo del rx - e e del us - e , il trend evidente . let stata considerata un fattore importante nel predire se un paziente abbia una invaginazione idiopatica o dovuta a lpp , e quindi quante siano le chances di riduzione non chirurgica [ 3 ]  . 
inoltre il paziente beneficia anche di una parziale riduzione dellinvaginazione , giacch questa minimizza lischemia intestinale e quindi riduce lestensione di una eventuale resezione intestinale , se necessaria [ 12 ]  . 
dallaltro lato , in pazienti oltre il primo anno di vita un pur sempre consistente numero dinvaginazioni idiopatico , quindi risulta utile tentare una riduzione non chirurgica , specialmente se lus negativa per lpp . 
inoltre stata ottenuta una completa riduzione in tutti i casi oltre lanno di vita che hanno eseguito il us - e , anche se tale sottogruppo di pazienti mostrava una durata della sintomatologia significativamente superiore rispetto il corrispettivo gruppo di pazienti sottoposto a rx - e . 
per tale motivo il us - e dovrebbe essere considerato quale procedura di prima scelta in questi casi potenzialmente pi difficoltosi . c evidenza che una lunga durata dei sintomi possa essere considerata un fattore prognostico negativo per la riduzione non chirurgica dellinvaginazione . 
infatti , nella maggior parte dei casi , una prolungata sintomatologia implica una estesa sofferenza vascolare , con un ampio edema del tratto intestinale invaginato , pi arduo da ridurre . 
pi breve la durata dei segni e dei sintomi , maggiore sono le radiol med ( 2012 ) 117 : 679689 bidity and effectiveness of the reduction procedure depend on the time elapsed from symptom onset to treatment institution . 
beasley and glover found that a symptom duration > 24 h was associated with a lower success rate for barium enema but not for gas enema [ 14 ]  . 
in contrast , the only study in which symptom duration seemed to have little influence on the success rate of barium enema was okuyama et al.s , with no significant difference in mean symptom duration between successful and failed enema groups [ 17 ]  . 
however , us - e was demonstrated to be an effective and safe procedure , regardless of disease duration , as shown by a success rate > 83% , with no cases of perforation , in the subgroup with symptom duration > 24 h . 
 several authors have emphasised that the kind of operator training and level of experience significantly affect the success rate , especially in potentially more difficult cases [ 6 , 8 ]  . 
several authors have stated that the reduction procedure performed by paediatric surgical staff greatly facilitates availability , contributes to the acquiring of skill and experience and improves safety and outcome [ 15 , 18 ]  . 
in our series , although ours is not a paediatric hospital , the operator was always a paediatric surgeon , both for us - e ( alone ) and rx - e ( together with a radiologist )  . 
even if different paediatric surgeons and radiologists performed rx - e , they were all trained and skilled with this procedure in a comparable manner . regarding contrast media used to perform enemas : hartmanns solution was chosen for us - e because of its nearphysiological composition , implying a reduced risk of fluid intoxication compared to saline , particularly when large volumes are needed for reduction attempts [ 9 ]  . 
to perform rx - e , we traditionally choose a water - soluble contrast medium instead of barium , as supported by other authors [ 10 , 11 , 1921 ]  . 
beasley e glover [ 14 ] hanno constatato che una durata della sintomatologia > 24 ore era associata ad una minor percentuale di successo nella riduzione con clisma baritato , ma non nel caso di clisma con gas . 
 [ 17 ] hanno pubblicato lunico studio in cui la durata dei sintomi sembrava essere poco correlata con la percentuale di successo del clisma con bario , senza alcuna differenza statisticamente significativa nella durata media della sintomatologia tra il gruppo con clisma di successo e quello con clisma fallito . 
nella nostra casistica non stata riscontrata alcuna significativa associazione tra la durata dei sintomi ed il risultato del clisma , sia nel gruppo rx - e che in quello us - e . 
comunque , il us - e si dimostrato essere procedura efficace e sicura , indipendentemente dalla durata della patologia , come dimostrato della percentuale di successo maggiore dell83% nel sottogruppo di bambini con durata dei sintomi > 24 ore , in assenza di episodi di perforazione . diversi autori hanno rilevato come il tipo di training e il grado di esperienza delloperatore che esegue la riduzione influenzino significativamente la percentuale di successo , specialmente in quei casi potenzialmente pi difficoltosi [ 6 , 8 ]  . 
parecchi autori hanno affermato che le procedure di riduzione eseguite da uno staff chirurgico pediatrico migliora notevolmente la disponibilit , contribuisce allacquisizione di perizia ed esperienza e migliora la sicurezza e i risultati [ 15 , 18 ]  . 
nella presente casistica , nonostante il nostro non sia un ospedale pediatrico , loperatore sempre stato un chirurgo pediatra , sia nellesecuzione del us - e ( da solo ) che del rx - e ( insieme ad uno specialista radiologo )  . 
il chirurgo pediatra dello staff che ha eseguito il us - e sempre stato il medesimo dirigente medico , che ha quindi acquisito nel corso degli anni una ampia competenza ed esperienza in tale procedura . 
anche se diversi chirurghi pediatri e radiologi hanno effettuato il rx - e , questi avevano comunque tutti un equivalente livello di preparazione e di competenza . per quanto concerne il tipo di mezzo utilizzato per eseguire i clismi , per il us - e stata scelta la soluzione di hartmann in quanto di composizione para - fisiologica , con conseguente ridotto rischio di intossicazione da fluidi , rispetto alla normale salina , quando si rendano necessari ampi volumi di liquidi nei tentativi di riduzione [ 9 ]  . 
nellesecuzione del rx - e abbiamo tradizionalmente preferito un mezzo di contrasto idrosolubile piuttosto che baritato , cos come sostenuto da altri autori [ 10 , 11 , 1921 ]  . 
il mezzo di contrasto idrosolubile fornisce una buona definizione anatomica , sterile e presenta una sicurezza maggiore del bario in caso 688 radiol med ( 2012 ) 117 : 679689 anatomical delineation , are sterile and safer than barium in the event of perforation . 
in fact , it has been shown that barium perforation leads to severe peritoneal reaction , which is associated with higher morbidity and mortality rates than is water - soluble contrast material [ 22 ]  . 
furthermore , in most of cases of intussusception , intestinal peristalsis is reduced ; the use of a water - soluble contrast medium greatly facilitates evacuation of intestinal content , either after a successful enema or in the event of surgery . 
 however , it is known that water - soluble contrast agents , compared with barium , require a higher column to produce the same bowel pressure due to lower density . 
a second point is that the majority of patients in our series had a very long symptom duration ( 56% > 24 h ; 84% > 12 h ) , as our institution is a referral centre for a large area . 
infatti , stato dimostrato che le perforazioni con fuoriuscita di bario producono severe reazioni peritoneali , che sono associate a una morbilit e mortalit maggiori rispetto alle perforazioni con mezzi di contrasto idrosolubili [ 22 ]  . 
inoltre , la peristalsi intestinale ridotta nella gran parte dei casi dinvaginazione ; lutilizzo di mezzi di contrasto idrosolubili agevola considerevolmente levacuazione del contenuto intestinale , sia in seguito ad un clisma risolutivo che in caso di successivo approccio chirurgico . 
comunque risaputo come il mezzo di contrasto idrosolubile richieda , rispetto al bario , una colonna pi elevata al fine di ottenere la medesima pressione nel lume intestinale , a causa della sua minor densit . 
un secondo punto che nella nostra casistica la maggior parte dei pazienti presentava una prolungata sintomatologia ( 56% > 24 ore ; 84% > 12 ore ) , giacch il nostro dipartimento il centro di riferimento per unampia area geografica . 
questo potrebbe inoltre spiegare la minor percentuale complessiva di successi rispetto quanto riportato in altre casistiche . conclusions conclusioni us - e and rx - e are procedures of comparable value and safety in reducing idiopathic ileocecocolic intussusception . 
as us - e avoids radiation exposure , it should be considered the firstchoice procedure for reduction , particularly in these two subgroups of patients . il us - e e il rx - e sono procedure di efficacia e sicurezza equiparabili al fine di ridurre linvaginazione ileo - ceco - colica idiopatica . 
beomonte zobel dipartimento di diagnostica per immagini , universit campus bio - medico di roma , via alvaro del portillo 200 , 00128 roma , italy correspondence to : r . 
seven patients ( two men , five women ; age range 5270 years ; mean age 59.7 years ) were treated under computed tomography ( ct ) and ultrasound ( us ) guidance . 
contrast - enhanced ct and mr imaging at the end of the procedure and at 1 month demonstrated 100% technical success ; these results were confirmed at 3 , 6 and 12 month . 
fishers test comparing serum creatinine obtained 1 day before and 1 day after the procedure showed no case of acute renal failure ( mean serum creatinine 24 h before the procedure 1.02 mg / dl ; mean serum creatinine 24 h after the procedure 0.95 mg / dl ; p = 0.114 ; not significant )  . 
sette pazienti ( 2 uomini e 5 donne ; et compresa tra 52 e 70 anni ; et media 59 , 7 anni ) sono stati trattati sotto guida tomografica computerizzata ( tc ) ed ecografica . 
 complessivamente diciassette lesioni ( 4 corticali e 13 esofitiche , con diametro massimo compreso tra 12 e 40 mm , in media 21 mm ) non adiacenti alla pelvi renale sono state trattate . 
tc e risonanza magnetica ( rm ) sono state le metodiche scelte per il follow - up al termine di ogni procedura e a distanza di 1 , 3 , 6 e 12 mesi ; sono stati monitorati anche i valori di creatinina sierica . 
 in 2 pazienti abbiamo riscontrato la presenza di un ematoma peri - renale ed in uno di questi due pazienti sono stati riportati anche 2 episodi di ematuria , regrediti spontaneamente . 
il successo tecnico , raggiunto nel 100% dei casi , stato dimostrato grazie al controllo mediante tc o rm con somministrazione di agente di contrasto al termine di ogni procedura e a distanza di un mese ; i follow - up a 3 , 6 e 12 mesi hanno confermato questo dato . 
nessun caso di insufficienza renale acuta stato riscontrato dopo aver applicato il test di fisher comparando i valori di creatinina sierica misurati il giorno prima e il giorno dopo la procedura , ( valore medio di creatinina sierica 24 ore prima della procedura : 1 , 02 mg / dl ; valore medio di creatinina sierica il giorno radiol med ( 2012 ) 117 : 606615 keywords radiofrequency ablation renal cell carcinoma solitary kidney us guidance ct guidance dopo : 0 , 95 mg / dl ; p = 0 , 114 , non significativo )  . 
la rfa si rivelata una procedura sicura ed efficace nel trattamento dei carcinomi a cellule renali nei pazienti con rene solitario . parole chiave ablazione a radiofrequenza carcinoma renale rene solitario guida ecografia guida tc introduction introduzione the incidence of renal cell carcinoma ( rcc ) is increasing worldwide [ 1 ] , and owing to the spread of imaging examinations such as computed tomography ( ct ) and ultrasound ( us ) , rccs are now diagnosed at an earlier stage [ 2 ]  . 
however , nephron - sparing surgery ( nss ) is now considered the treatment of choice in patients with small rccs , as outcomes similar to those after radical nephrectomy have been proved [ 4 ]  . 
moreover , patients with rcc in solitary kidneys due to radical contralateral nephrectomy have a high probability of developing a new carcinoma within the remaining kidney [ 5 ]  . 
to avoid renal failure complications , a few years ago , percutaneous radiofrequency ablation ( rfa ) was proposed as a safe choice in patients with rcc in a solitary kidney [ 57 ]  . 
this paper illustrates our preliminary experience in patients with rcc in a solitary kidney treated with rfa under us or ct guidance . materials and methods patients a retrospective analysis of our database was carried out . 
between january 2009 and march 2011 , seven patients ( two men , five women ; age range 5270 years ; mean age 59.7 years ) with rccs in a solitary kidney were treated with percutaneous thermal ablation under simultaneous ct and us guidance . 
indications for thermal ablation were impaired renal function , multiple exophytic or intraparenchymal tumours ( cortical ) with maximum diameter < 5 cm , unsuitability for surgery lincidenza del carcinoma renale ( rcc ) in aumento in tutto il mondo [ 1 ] e grazie alla diffusione degli esami radiologici , quali tomografia computerizzata ( tc ) ed ecografia , gli rcc sono diagnosticati sempre pi precocemente [ 2 ]  . 
tuttavia , attualmente , la chirurgia ablativa con risparmio di parenchima renale ( nss ) ritenuta il trattamento di scelta in pazienti con rcc di piccole dimensioni , dal momento che sono stati ottenuti risultati paragonabili alla nefrectomia radicale [ 4 ]  . 
inoltre , nei pazienti affetti da rcc con rene solitario in virt di un pregresso intervento chirurgico , la probabilit di sviluppare un secondo carcinoma a carico del restante rene elevata [ 5 ]  . 
di fatto , specialmente in pazienti con rene solitario , la nss potrebbe esitare in un quadro clinico di insufficienza renale con la necessit di ricorrere ad emodialisi [ 5 ]  . 
al fine di evitare le complicanze connesse con linsufficienza renale , recentemente stata proposta lablazione percutanea a radiofrequenza ( rfa ) quale valida e sicura opzione terapeutica in pazienti con rcc in un rene solitario [ 57 ]  . 
in questo studio presentiamo la nostra preliminare esperienza in pazienti con rcc in un rene solitario trattati con rfa sotto guida tc ed ecografica . materiali e metodi pazienti stata condotta unanalisi retrospettiva del nostro database . 
tra gennaio 2009 e marzo 2011 , sette pazienti ( 2 maschi e 5 donne ; et media compresa tra 52 e 70 anni ; et media 59 , 7 anni ) con rcc in un rene solitario sono stati trattati con termoablazione percutanea sotto guida simultanea tc ed ecografia . 
exclusion criteria were centrally located tumours , maximum diameter > 5 cm , extensive metastatic disease or disease spreading beyond the kidney , systemic or urinary tract infections and bleeding disorders [ 5 ]  . 
prior to the percutaneous procedure , a total - body ct scan was obtained to rule out extrarenal spread of disease ; moreover , a ct or mr imaging scan was used to accurately detect tumour location . 
the onset of solid lesions not detectable on prior ct or mr imaging scans , showing dimensional growth over time in patients with a history of contralateral nephrectomy due to histologically assessed rcc , was regarded as suspicious for neoplastic disease ; however , in agreement with breen et al . 
thirteen tumours ( 76% ) were right - sided and four ( 24% ) left - sided . a multidisciplinary meeting of surgeons , urologists , oncologists , pathologists , radiologists and interventional radiologists taking place every week in our institution discussed all cases . 
no approval from the local ethics committee was sought owing to the retrospective design of the study . procedure treatments were performed under local anaesthesia ( carbocaine , astrazeneca spa , italy ) and mild sedation ( dormicum , roche pharma , germany ) ; vital parameters including continuous pulse oximetry , heart rate and electrocardiography were continuously recorded ; blood pressure was measured every 5 min ; the same parameters were also monitored for at least 6 h following the procedure . 
on ct scans , the area of interest was targeted by obtaining a scan with a row of needles lying on the sklesions were treated with the cool - tip rf ablation system ( valleylab , usa ) composed of a single pulsed rf electrode ( 17 gauge , 1015 cm long , 23 cm exposure ) internally cooled with chilled water . 
 le indicazioni alla termoablazione sono state : alterata funzionalit renale , neoplasie corticali intra - parenchimali o esofitiche con diametro massimo < 5 cm , pazienti non candidabili a chirurgia per elevato rischio cardiovascolare o respiratorio o pazienti che rifiutassero il trattamento chirurgico . 
i criteri di esclusione sono stati : tumori localizzati in zone centrali , diametro massimo > 5 cm , patologia metastatica o estesa oltre la capsula renale , infezioni urinarie o sistemiche ed alterazioni della coagulazione [ 5 ]  . 
prima di procedere al trattamento percutaneo stata sempre eseguita una tc total body per indagare la presenza di malattia diffusa oltre il rene ; inoltre , la tc o la rm sono servite per visualizzare accuratamente la localizzazione del tumore . 
linsorgenza di lesioni solide non evidenziate in precedenti tc o rm , con progressivo accrescimento in pazienti con storia di nefrectomia radicale controlaterale per rcc istologicamente accertato , stata considerata sospetta per malattia neoplastica ; tuttavia , in accordo con breen et al . 
 abbiamo organizzato un meeting settimanale multidisciplinare con chirurghi , urologi , oncologi , anatomo - patologici , radiologi e radiologi interventisti al fine di discutere ogni caso cosicch ogni decisione in merito al trattamento stata presa in maniera collegiale . 
non stato necessario richiedere il consenso del comitato etico locale poich si trattato di uno studio retrospettivo . tecnica le procedure sono state eseguite sotto anestesia locale ( carbocaina , astrazeneca spa , italia ) e blanda sedazione ( dormicum , roche - pharma , germania ) ; i parametri vitali , quali saturazione dellemoglobina , frequenza cardiaca ed elettrocardiogramma sono stati continuamente monitorizzati ; ogni 5 minuti stata misurata la pressione arteriosa ; gli stessi valori sono stati tenuti sotto controllo per almeno 6 ore dopo il termine dellintervento . 
le lesioni sono state trattate con kit di ablazione a radiofrequenza cool - tiptm ( valleylab , cooltip rf ablation system , usa ) , costituito da un singolo agoelettrodo pulsante a radiofrequenza ( 17 g , lunghezza 1015 radiol med ( 2012 ) 117 : 606615 cm , porzione ablante 23 cm ) , raffreddato internamente con acqua fredda . 
lesioni di diametro inferiore ai 20 mm sono state trattate con un singolo ago in una singola seduta ; qualora il diametro fosse di dimensioni superiori ai 20 mm , sono state condotte pi sedute riposizionando di volta in volta lago ; per lunica lesione con diametro pari a 40 mm stato eseguito un trattamento con una singola seduta posizionando due aghi contemporaneamente . 
gli elettrodi sono stati posizionati in modo che il volume tissutale ablato inglobasse lintera area neoplastica ; la necrosi stata considerata completa nel momento in cui larea necrotica avesse ecceduto di almeno 5 mm larea neoplastica . 
al termine di ogni procedura ablativa , gli aghi - elettrodi sono stati rimossi ablando il loro tragitto fino alla cute per evitare il rischio di disseminazione di malattia neoplastica . 
in un caso stato necessario insufflare 50 ml di anidride carbonica per separare larea da trattare dalla flessura colica destra . il giorno prima e il giorno dopo lintervento sono stati analizzati parametri ematici quali il tempo di protrombina ( pt ) , il tempo di tromboplastina parziale attivato ( aptt ) , il fibrinogeno , linternational normalized ratio ( inr ) , lemocromo e la creatinina serica . 
i controlli a distanza mediante tc con contrasto o rm sono sempre stati eseguiti in ogni pazienti dopo 1 , 3 , 6 e 12 mesi ; nel follow - up stata inclusa anche la misurazione della creatinina sierica . il test di fischer stato eseguito per comparare i valori di creatinina sierica ottenuti 24 ore prima e dopo la procedura ; sono stati considerati statisticamente significativi valori con p < 0 , 05 . statistica risultati sono state condotte dieci sedute ablative cos come pianificato e il successo tecnico stato sempre ottenuto ; le profig . 
1 ricostruzione multiplanare ( mpr ) di una scansione tc postcontrastografica ( fase tardiva ) che conferma il corretto posizionamento dellago . ingly , electrodes were deployed or composed in order to cover the entire neoplastic area , and necrosis was considered to have been achieved when the necrotic area exceeded the neoplastic area by at least 5 mwhen multiple lesions were treated in the same session , the same probe was used . 
the two patients with more than two lesions required more than one ablative session ( two sessions for the patient presenting with three lesions , and three sessions for the patient with seven lesions )  . 
in one patient , 50 ml of carbon dioxide was used to create an insulation effect between the treated area and the right colic flexure . blood chemistry of prothrombin time ( pt ) , activated prothrombin time ( aptt ) , fibrinogen , international normalised ratio ( inr ) , blood cell count , haemoglobin and serum creatinine was recorded the days before and after the procedure . 
imaging ( contrast - enhanced ct or mr ) follow - up was obtained for all patients at 1 , 3 , 6 and 12 months ; serum creatinine was monitored during the follow - up . radiol med ( 2012 ) 117 : 606615 610 fig . 
2a - f radiofrequency ablation ( rfa ) of an 18 - mm renal cell carcinoma ( rcc ) located on the medial arm of the right solitary kidney in a 59 - year - old female patient . 
one - month follow - up of the same patient shows complete necrosis of the lesion at magnetic resonance imaging with t1 - weighted fat - suppressed contrast - enhanced sequence ( c ) and t2 - weighted fatsuppressed sequence ( curved arrow , showing hyperintense signal of probe track within the scar , d )  . 
ricostruzione sul piano coronale di una tc con mezzo di contrasto in fase arteriosa eseguita 24 ore dopo la procedura che rivela la necrosi completa della lesione ( b )  . 
il follow - up dello stesso paziente a distanza di un mese conferma la necrosi completa della lesione nelle sequenze rm t1 - pesate in fase post - contrastografica con soppressione del segnale del grasso ( c ) e nelle sequenze t2 - pesate con soppressione del segnale del grasso ( freccia curva , mostrante il tragitto dellago con segnale iperintenso allinterno della cicatrice , d )  . 
in entrambi i pazienti con questo tipo di complicanze minori , non mai stato osservata n instabilit dei parametri emodinamici n significativa riduzione dellemoglobina nelle successive 24 radiol med ( 2012 ) 117 : 606615 fig . 
le scansioni tc in fase arteriosa ( b ) e tardiva ( c ) mostrano la retrazione della regione trattata senza segni di recidiva 36 mesi dopo la procedura . ore ; sono stati monitorizzati clinicamente e trattati in modo conservativo attraverso la somministrazione di liquidi per via endovenosa . 
 allinterno delle aree trattate , i controlli tc o rm con somministrazione di agente di contrasto , eseguiti al termine di ogni procedura e a distanza di un mese hanno dimostrato il successo tecnico nel 100% dei casi . 
dopo la procedura non si mai manifestato un quadro clinico di insufficienza renale ; questo dato suffragato dal test di fisher in cui sono stati messi a confronto i valori di creatinina sierica ottenuti il giorno prima ed il giorno dopo lintervento ( valore medio della creatinina sierica 24 ore prima della procedura 1 , 02 mg / dl ; valore medio della creatinina 24 ore dopo la procedura 0 , 95 mg / dl ; p = 0 , 114 , non significativo [ ns ] )  . 
i valori di creatinina sierica monitorati durante i controlli a distanza sono sempre rientrati nei limiti della norma ( 0 , 61 , 2 mg / dl , in base alle misurazioni del laboratorio di analisi della nostra struttura )  . 
i risultati sono riportati nella tabella 1 . discussione il prolungarsi della vita media , lincremento di incidenza del rcc e lintento di preservare la funzionalit del parenchima renale sono tutti elementi che hanno amplificato linteresse verso metodiche mininvasive , quali ad esempio lablazione percutanea a radiofrequenza per il trattamento del rcc [ 11 ] , specialmente in pazienti con rene solitario fig . 
in the two patients experiencing mild complications , no haemodynamic instability or significant decrease in haemoglobin were observed in the following 24 h ; they were clinically monitored and treated conservatively through administration of intravenous fluids . 
 612 radiol med ( 2012 ) 117 : 606615 contrast - enhanced ct and mr imaging at the end of the procedure and at 1 month follow - up demonstrated 100% technical success in the treated areas ,  . 
no cases of renal failure were noted immediately after the procedure , as shown by fishers test comparing serum creatinine levels obtained 1 day before and 1 day after the procedure ( mean 24 h before the procedure 1.02 mg / dl ; mean 24 h after the procedure 0.95 mg / dl ; p = 0.114 , not significant )  . 
results are summarised in table 1 . discussion the increased life expectancy , the increased incidence of small rccs and the desire to preserve renal parenchyma has amplified interest in minimally invasive techniques such as percutaneous image - guided rfa for treating rccs [ 11 ] , especially in patients with a solitary kidney [ 5 ]  . 
inoltre , rispetto alla chirurgia , la rfa richie de soltanto una blanda sedazione e non necessita di anestesia generale ; la durata del ricovero , il dolore , la morbilit , la mortalit ed i costi risultano ridotti [ 13 ]  . 
a partire dal 1997 , anno in cui stato riportato per la prima volta in letteratura un trattamento di rfa percutanea [ 15 ] , diversi casi sono stati pubblicati su riviste scientifiche . 
i risultati dei primi 3 studi per numero di casi trattati [ 1719 ] hanno dimostrato che la percentuale di successo , intesa come non evidenza di residuo di malattia , dipende principalmente dalle dimensioni e dalla localizzazione della neoplasia ; lesioni con diametro < 3 , 7 cm e lesioni situate in periferia sono state trattate con successo nel 100% dei casi . 
 [ 19 ] show that the success rate ( no evidence of viable tumour ) mainly depends on tumour size and location , as tumours < 3.7 cm and not centrally located were successfully treated in 100% of cases . 
our records are consistent with these data , as we treated exophytic and peripheral ( cortical ) lesions with a mean diameter of 21.0 mexophytic location seems to favour complete tumour ablation due to the insulation effect provided by perirenal fat tissue , which is poorly vascularized and thus does not provide heat loss [ 20 ]  . 
 [ 16 ] , who reported a 95% rate of disease - free survival at 10 - month follow - up , all our patients were able to attend the 12 - month follow - up , and none of them showed disease recurrence at imaging examinations . 
in our experience , 1and 12 - month follow - up seem to be crucial because at 1 month , it is possible to clearly differentiate residual disease from local hyperaemia that foltrattato lesioni esofitiche e periferiche ( corticali ) con diametro medio di 21 m la localizzazione esofitica sem bra favorire lablazione completa per leffetto isolante fornito dal tessuto adiposo perirenale , che poco vascolarizzato e quindi non comporta dispersione di calore [ 20 ]  . 
 [ 16 ] che hanno descritto un intervallo di sopravvivenza libera da malat tia a distanza di 10 mesi dal trattamento nel 95% dei casi , tutti i pazienti da noi studiati sono giunti al follow - up dopo un anno senza recidiva di malattia evidenziabile allimaging . 
in base alla nostra esperienza , i controlli dopo 1 e 12 mesi rappresentano un momento cruciale ; questo poich dopo 1 mese possibile differenziare chiaramente un eventuale residuo di malattia dalliperemia locale che fa seguito al trattamento ablativo e pu simulare tale reperto che mima il residuo di malattia , mentre nel followup a 12 mesi si pu effettivamente documentare la ripresa di malattia in virt del lento tasso di crescita di questo tipo di neoplasia ( 0 , 11 cm / anno ) [ 21 ]  . le complicanze riportate in seguito a questo tipo di trattamento sono ematuria , emorragia , danni neuro - vascolari e cutanei , disseminazione neoplastica e lesioni a carico del sistema collettore renale o degli organi adiacenti [ 11 ]  . 
 lelevato tasso di successo tecnico nellablazione delle lesioni esofitiche non influenzato dal contatto con organi o tessuti critici poich nella maggior parte dei casi questi 614 radiol med ( 2012 ) 117 : 606615 lows ablation , thus mimicking a still viable tumour ; at 12 months , it is possible to clearly assess disease recurrence due to the slow growth rate ( 0.11cm / year ) of rcc [ 21 ]  . reported complications after rfa are haematuria , haemorrhage , neurovascular and cutaneous injuries , neoplastic seeding and damage to the collecting system or adjacent organs [ 11 ]  . 
the high technical success in the ablation of exophytic lesions is not invalidated by the closeness of adjacent critical organs as , in most cases , those organs can be easily preserved from thermal damage by injection of insulating solutions ( 33% glucose solution ) or gas ( carbon dioxide ) , as shown in our series . alternative emerging techniques are microwave ( mwa ) and cryoablation . 
cryoablation also seems to be a promising alternative to rfa , with some technical advantages such as ablation zone visualisation ( a well - demarcated zone of hypoattenuation on ct scan ) during the procedure [ 23 ]  . 
possible reasons for such results are the ability to use as many as eight probes , thus allowing larger ablative zones [ 25 ] , and a delayed cellular death effect immunologically stimulated by the release of tumour antigens or apoptosis from cells at the periphery of the cryolesion . in conclusion , although new ablative techniques seem promising , rfa is still the most commonly used option . 
 it could also be considered a safe and reliable therapeutic choice for treating rcc in patients with a solitary kidney . possono essere facilmente preservati da un possibile insulto termico mediante iniezione di soluzioni isolanti ( soluzione di glucosio al 33% ) o gas ( anidride carbonica ) , come nel nostro caso . metodiche alternative emergenti sono lablazione a microonde ( mwa ) e la crioablazione . 
 la mwa sembrerebbe offrire alcuni vantaggi tecnici come la possibilit di trattare lesioni di dimensioni maggiori grazie a un pi ampio raggio di azione ed una ridotta incidenza del noto effetto heat - sink ; inoltre , la diffusione del calore al tessuto vitale non limitata dalla disidratazione tissutale e questo consente di raggiungere temperature maggiori allinterno della lesione tumorale [ 22 ]  . 
anche la crioablazione sembra essere unalternativa promettente alla rfa con alcuni vantaggi tecnici come la possibilit di visualizzare larea ablata ( come una zona ben definita ed ipodensa nelle scansioni tc ) durante il trattamento [ 23 ]  . 
i dati preliminari riportati in letteratura riguardo la crioablazione lasciano ben sperare , con un tasso di successo superiore al 90% e progressione di malattia descritta in un solo studio [ 24 ]  . 
le possibili spiegazioni di questo ottimo risultato sono la possibilit di utilizzare fino a otto aghi consentendo aree di trattamento pi ampie [ 25 ] ed un effetto tardivo inducente morte cellulare su base immunologica per via del rilascio di antigeni tumorali e per fenomeni di apoptosi ad opera delle cellule situate alla periferia della lesione . in conclusione , nonostante nuove tecniche ablative percutanee sembrano promettere buoni risultati , la rfa rimane ancora lopzione pi comune . 
alberti , spedali civili , piazzale spedali civili 1 , 25123 brescia , italy 2radioterapia , universit degli studi di brescia , brescia , italy 3radioterapia , ospedale careggi , firenze , italy 4radioterapia , ospedale di treviglio , bergamo , italy 5universit degli studi di firenze , firenze , italy correspondence to : l . 
at univariate analysis , survival and local control rates were significantly better in the more recent accrual periods and in the more favourable disease presentations ; treatment - related parameters mainly affect lrc . 
at multivariate analysis , patientand disease - related factors had a more evident prognostic effect than did therapeutic factors , although dose to the nasopharynx and treatment technique had a marginally significant impact on dss and os . 
sono stati studiati 883 pazienti consecutivamente trattati con radioterapia dal 1977 al 2000 a firenze ( flo , florence ) e brescia ( ira , istituto del radio alberti )  . 
allanalisi univariata , la sopravvivenza globale e il controllo locale sono risultati significativamente migliori nei periodi pi recenti e nelle presentazioni di malattia pi favorevoli ; i parametri legati al trattamento influenzano prevalentemente il lcr . 
allanalisi multivariata , i fattori legati al paziente e alla malattia hanno un effetto prognostico pi evidente rispetto a quelli legati al trattamento , bench la dose alla rinofaringe e la tecnica di trattamento abbiano un impatto marginale anche sulla dss e sullos . radiol med ( 2012 ) 117 : 690714 therapy techniques for npc , such as three - dimensional conformal radiotherapy ( 3d - crt ) and particularly intensity - modulated radiotherapy ( imrt )  . keywords nasopharyngeal cancer radiotherapy treatment techniques survival patterns of care conclusioni . 
i risultati di questo studio di riferimento potrebbero essere utili per la comprensione dellevoluzione di nuove tecniche radioterapiche per il trattamento dei tumori della rinofaringe , come la radioterapia tridimensionale conformazionale ( 3dcrt ) e specialmente la radioterapia a modulazione dintensit ( imrt )  . parole chiave neoplasia della rinofaringe radioterapia tecniche di trattamento sopravvivenza terapie introduction introduzione nasopharyngeal cancer ( npc ) is rare in europe and western countries in general [ 1 ]  . 
we therefore retrospectively analysed results obtained in a large italian series of patients with npc who were treated consecutively over more than 20 years at the florence university radiation oncology department ( flo ) and the brescia university radiation oncology department istituto del radio o . 
our aim was to define outcomes for patients treated with conventional radiotherapy , according to different clinical and therapeutic features and in the different accrual periods , as a benchmark study to better define the role of new radiation techniques that could improve outcomes . 
we divided our analysis into two companion papers : this one reports on survival results . il cancro della rinofaringe ( npc ) raro sia in europa che nei paesi occidentali in generale [ 1 ]  . 
abbiamo perci deciso di effettuare unanalisi retrospettiva dei risultati ottenuti in una vasta serie italiana di pazienti con npc , trattati consecutivamente per oltre 20 anni presso il dipartimento di radioterapia delluniversit di firenze ( flo ) e presso il dipartimento di radioterapia delluniversit di brescia , istituto del radio o . 
il nostro obiettivo quello di definire gli outcomes di pazienti trattati con radioterapia convenzionale , secondo le differenti caratteristiche cliniche e terapeutiche e in base ai differenti periodi di reclutamento , e di realizzare uno studio che rappresenti un punto di riferimento per definire meglio il ruolo delle nuove tecniche di radioterapia che potrebbero condurre ad un miglioramento dei risultati . 
abbiamo diviso la nostra analisi in due parti : questa prima parte tratta dei risultati in termini di sopravvivenza . materials and methods we retrospectively analysed the records of 883 patients consecutively treated for npc with radical intent at flo and ira between 1977 and 2000 . 
tumour and node ( tn ) categories and clinical stage were retrospectively reassigned according to the 2002 union for international cancer control ( uicc ) tnm classification [ 2 ]  . 
when needed , data were analysed according to the accrual period ( 19771985 ; 198690 ; 19911995 ; 19962000 ) : this rough subdivision was chosen for the availability of accessible clinical records and treatment documentation in both centres ( as for accrual starting date ) and because the four time intervals are characterised by different staging and treatment procedures ( as described in detail in the following paragraphs )  . 
 we chose not to include patients treated after 31 december 2000 to allow a sufficiently long follow - up period and because most patients treated after that date were submitted materiali e metodi abbiamo analizzato retrospettivamente le cartelle cliniche di 883 pazienti trattati consecutivamente per npc a titolo radicale a flo e allira fino al 2000 . 
le categorie tumore e stadio linfonodale ( tn ) e lo stadio clinico sono state riassegnate retrospettivamente secondo la classificazione tnm dellunion for international cancer control ( uicc ) del 2002 [ 2 ]  . 
i dati sono stati analizzati , ove necessario , secondo i diversi periodi di competenza ( 19771985 ; 1986 1990 ; 19911995 ; 19962000 ) : questa suddivisione stata scelta in relazione alla disponibilit di cartelle cliniche e documentazione terapeutica accessibili in entrambi i centri ( cos come per la data iniziale del periodo di raccolta dei dati ) e poich i quattro periodi scelti sono caratterizzati da modalit di stadiazione e procedure terapeutiche diverse ( come descritto in dettaglio nei paragrafi che seguono )  . 
 abbiamo scelto di non includere i pazienti trattati dopo il 692 radiol med ( 2012 ) 117 : 690714 to conformal or intensity - modulated radiation therapy ( imrt )  . clinical features the different features of the series are reported in table 1 . 
computed tomography ( ct ) and magnetic resonance imaging ( mri ) scans of the nasopharynx were available in both centres after 1980 and 1985 , respectively , and gradually replaced conventional radiology procedures used previously . 
the proportion of patients staged only with conventional radiology was equal to 47% in the period 19771985 and declined in the subsequent three 5 - year intervals to 4% , 2% and 0% . 
 therefore , some patients staged with ct also had conventional radiological examinations and a substantial number of the patients staged with mri also had a ct ( 213 / 277 , 77% )  . 
ira patients received 4550 gy on all the negative neck nodes , and 20% of them ( as opposed to < 5% flo patients ) were given < 65 gy to the primary tumour site . 
1 31 - 12 - 2000 per avere un periodo di follow - up sufficientemente lungo e anche perch la maggior parte dei pazienti trattati dopo tale data sono stati sottoposti a radioterapia conformazionale e a radioterapia a intensit modulata del fascio . caratteristiche cliniche le diverse caratteristiche delle serie di pazienti sono riportate nella tabella 1 . 
 riportata anche lincidenza di sintomi clinici allesordio di malattia che in linea con i dati riportati in letteratura [ 1 ]  . stadiazione prima della radioterapia tutti i pazienti sono stati sottoposti ad una valutazione clinica ; sono stati effettuati , inoltre , esami ematochimici di routine , radiografia del torace e faringolaringoscopia . 
tomografia computerizzata ( ct ) e risonanza magnetica ( mri ) della rinofaringe sono state disponibili in entrambi i centri dopo il 1980 e dopo il 1985 rispettivamente , e hanno gradualmente rimpiazzato le procedure di radiologia convenzionale usate in precedenza . 
la percentuale di pazienti stadiati solo con procedure radiologiche convenzionali del 47% nel periodo che corre dal 1977 al 1985 e si ridotta nei successivi intervalli di 5 anni al 4% , 2% e 0% . 
i valori corrispondenti per la ct sono 50% , 77% , 54% e 16% ; per la mri sono3% , 19% , 44% , 84% ; queste percentuali si riferiscono alle pi recenti tecniche diagnostiche usate per ogni paziente durante i periodi consecutivi di reclutamento ; una parte dei pazienti stadiati con ct quindi stata sottoposta anche ad esami radiologici convenzionali e una parte sostanziale dei pazienti stadiati con mri ha effettuato anche ct ( 213 / 277 , 77% ) .la maggioranza dei pazienti con malattia in stadio iiiv stata sottoposta a ecografia epatica e a scintigrafia ossea . trattamento le tecniche di trattamento sono cambiate attraverso gli anni in entrambi i centri e sono dunque diversi in relazione al periodo e anche al centro ( tabella 1 )  . 
i pazienti di firenze sono stati generalmente trattati con 70 gy al tumore , 60 gy ai primi livelli linfonodali negativi ( per esempio , i linfonodi regionali adiacenti a quelli patologici o al tumore primitivo ) e con 50 gy ai restanti linfonodi del collo , comprendendo quasi sempre i linfonodi sopraclavicolari . 
i pazienti dellira hanno ricevuto 4550 gy su tutti i linfonodi negativi del collo e il 20% di loro ( in opposizione a meno del 5% di quelli trattati a flo ) hanno ricevuto meno di 65 gy sulla sede del tumore primitivo . 
1 treatment geometry for cases treated with and without an anterior field to cover nasal fossae involvement and with longer or shorter parallelopposed ll fields to treat neck nodal volumes . 
1 geometria del trattamento per i casi trattati con e senza un campo anteriore per consentire un adeguato trattamento in presenza di coinvolgimento delle fosse nasali , e con campi contrapposti paralleli ll pi lunghi e pi corti , per trattare i volumi linfonodali del collo . 
 per quanto riguarda la geometria del trattamento , la tecnica di firenze stata spesso simile a quella di ho [ 3 ] , come mostrato in figura 1 e descritto in dettaglio altrove [ 4 ]  . 
la rinofaringe , e a volte la parte superiore del collo , stata trattata con campi opposti paralleli latero - laterali ( ll ) e la parte restante del collo con un campo anteriore adattato . 
in entrambi i centri , una parte dei pazienti ha ricevuto una sovradose ( boost ) alla rinofaringe con fotoni ad energia molto alta ( a firenze , con fotoni da 25 a 31 mev da acceleratore lineare o da betatrone ; a brescia , con fotoni da 18 a 22 mev da microtrone o da acceleratore lineare )  . 
nella serie di brescia , i pazienti trattati con boost con fotoni ad alta energia sono stati anche trattati con tecnica ho - like e nessuno stato trattato con le tecniche precedenti che usavano campi apposizionali di elettroni per coprire le aree linfatiche . il trattamento stato pianificato senza laiuto di sistemi di pianificazione di trattamento computerizzati ( tps ) , ma , and detailed elsewhere [ 4 ]  . 
in both centres , part of the series had the boost dose to the nasopharynx delivered with very - highenergy photons ( in flo , with 2531 mev photons from a linac or a betatron ; in ira , with 1822 mev photons from a racetrack microtron or a linac )  . 
in the ira series , patients treated with this high - energy boost dose were also treated with a ho - like technique and none with the earlier technique using appositional electron fields to cover the neck lymphatic areas . treatment was planned without the help of computerised treatment planning systems ( tps ) , but after the availability of ct and mri , findings of these examinations were used to define treated volumes at the simulator . 
2a fotografia del set - up per la tecnica di trattamento adottata a brescia con i primi casi ( prima del 1986 ) : si trattavano separatamente i linfonodi del collo con elettroni e la rinofaringe con fotoni ; b set - up usato per uno dei casi pi recenti trattati con imrt a brescia ; c rappresentazione 3d del planning target volume ( ptv , verde ) , occhi ( rosa ) , midollo ( fucsia ) e parotidi ( celeste , a rete ) in un caso recente imrt ; sono rappresentati anche il gross tumor volume ( gtv ) rinofaringeo ( celeste , a rete ) e gli angoli di ingresso dei fasci ( frecce verdi ) ; d sono rappresentate per questo piano , con tecnica imrt a 7 campi , le isodosi al ptv del tumore primitivo e del volume linfonodale ( valori assoluti in cgy ) ; sono evidenziate la dose / frazione pi alta alla rinofaringe ( 220 cgy ) e la dose / frazione meno elevata ricevuta simultaneamente dai linfonodi clinicamente indenni ( 177 cgy ) ; evidente un certo grado di risparmio dei lobi superficiali della parotide . 
 was prescribed at the midline along the central axis ( icru point ) or recalculated at the icru point for ira cases treated earlier when it was prescribed at the minimum tumour isodose . 
chemotherapywith platinum - containing con la sopravvenuta disponibilit di ct e mri , i risultati di questi esami diagnostici sono stati usati per definire i volumi di trattamento al simulatore . 
la dose stata prescritta alla mediana lungo lasse centrale ( punto international commission on radiation units and measurements [ icru ] ) ed stata ricalcolata al punto icru per i casi ira trattati nei periodi meno recenti , quando si prescriveva allisodose minima del tumore . 
for all these reasons , cht was not considered as a variable for uniand multivariate analysis . follow - up stata somministrata ad una minoranza di pazienti ( 181 / 883 , 20% , tabella 1 )  . 
 follow - up after treatment always included clinical examination every 23 months in the first posttreatment year and at longer intervals thereafter ; ct / mri scans ( after their availability ) and other imaging procedures were obtained less often and not in all patients during the follow - up period . follow - up statistical evaluation localregional control ( lrc ) , overall survival ( os ) and disease - specific survival ( dss ) rates were calculated using the kaplanmeier product limit method . 
outcomes were measured from the end of radiation therapy to the date of first failure or to the last date of follow - up for lrc and to the date of death or to the last date of follow - up for survival . 
 literature search to obtain a meaningful literature database for comparison and analysis , we undertook a systematic literature search ( pubmed ; keywords : nasopharyngeal cancer and radiotherapy ) , and we identified 2 , 487 articles . 
we then selected the hospital series recruited after 1950 and published after 1970 until 2006 , including at least 40 consecutive cases each , treated with radical intent , with sufficient stage information and meaningful survival data . 
review articles , those without an english abstract , those dealing with mixed case series ( for example , including sarcoma or lymphoma cases ) and those with relapsed or metastatic patients were excluded . 
we did not consider papers analysing only a subset of patients ( for example , those with advanced stage only ) , those dealing with paediatric il follow - up dopo il trattamento ha sempre compreso una valutazione clinica ogni 23 mesi nel primo anno dopo il trattamento e successivamente a intervalli pi lunghi ; ct / mri ( dal momento della loro disponibilit nei due centri ) e altre procedure diagnostiche sono state effettuare meno spesso e non in tutti i pazienti durante il periodo di follow - up . valutazione statistica il controllo loco - regionale ( lrc ) , la sopravvivenza globale ( os ) e la sopravvivenza specifica per malattia ( dss ) sono state calcolate usando il metodo del prodotto limite o di kaplan - meier . 
gli outcomes sono stati misurati dalla fine del trattamento radioterapico alla data del primo fallimento o alla data dellultimo controllo clinico per il controllo loco - regionale ; alla data di morte o alla data dellultimo follow - up per la sopravvivenza . 
le variabili incluse nel modello di cox sono state quelle giudicate clinicamente significative , in aggiunta a quelle per le quali era stata rilevata una differenza statisticamente significativa allanalisi uni variata . 
 ricerca della letteratura per ottenere un database significativo della letteratura per il confronto e lanalisi , abbiamo intrapreso una ricerca sistematica della letteratura ( pubmed , keywords : nasopharyngeal cancer and radiotherapy ) che ci ha consentito di identificare 2487 articoli . 
abbiamo poi selezionato le serie ospedaliere di pazienti reclutati dopo il 1950 e pubblicate dopo il 1970 , fino al 2006 , che avessero ciascuna almeno 40 casi consecutivi , trattati con intento radicale , con sufficienti informazioni relative alla stadiazione e dati di sopravvivenza significativi . 
sono stati esclusi gli articoli con revisioni della letteratura , quelli senza un riassunto in inglese , quelli che trattavano serie miste di casi ( per esempio , che includevano casi di sarcomi e linfomi ) , pazienti con ricadute o metastasi . 
 gli articoli che analizzavano solo alcuni sottogruppi di pazienti ( per esempio , solo quelli con stadio avanzato ) , quelli che trattavano di casi pediatrici e quelli relativi a studi randomizzati . 
chiaro che questa revisione , per quanto la pi accurata possibile , non include in modo esaustivo tutte le serie cliniche pubblicate negli anni 19702006 . results overall , 722 / 883 patients ( 82% ) obtained complete response ( cr ) to the treatment given . 
 univariate analysis of os , dss and lrc tables 2 and 3 show actuarial 5 - year os , dss and lrc rates according to different features , along with the differences observed at univariate analysis . 
when considering patient - related factors , age had a significant impact on uncorrected survival , with older patients showing a higher risk , but it had no impact on dss and lrc . 
among tumour - related factors , epidermoid histological subtype , increasing t and n category and more advanced clinical stage all showed a significant adverse prognostic effect at univariate analysis for all the outcomes ( table 2 )  . 
 among treatment - related features , the more recent accrual period and the treatment of the neck lymph - nodal volume ( even with a dose < 46 gy ) were significantly related with a better prognosis at univariate analysis for all the outcomes . 
the nine patients ( 1% ) not treated on the neck had significantly worse lrc , dss and os rates , even if none of them presented with clinically positive neck nodes at the time of diagnosis . 
differences between patients treated with lower and higher doses on the neck were not significant because patients with clinically positive neck nodes obviously received higher neck doses ( table 3 )  . 
 ho - like treatment technique , higher tumour dose , conventional fractionation and a more sophisticated staging modality ( including ct and / or mri ) were all significantly linked with a better lrc but not with survival at univariate analysis ( table 3 )  . 
it should be emphasised , however , that patients treated with separate nasopharynx and neck risultati complessivamente , 722 / 883 pazienti ( 82% ) hanno ottenuto una risposta completa ( cr ) al trattamento . 
le ricadute locali e regionali ( includendo i pazienti che non hanno ottenuto una cr ) sono state 281 ( 32% ) ; le metastasi a distanza si sono manifestate in 206 casi ( 23% )  . 
 le sopravvivenze attuariali a 5 anni , os , dss e lrc sono state rispettivamente 53% , 61% e 66% rispettivamente . analisi univariata di os , dss e lrc le tabelle 2 e 3 mostrano la sopravvivenza attuariale globale a 5 anni e la sopravvivenza specifica per malattia e il controllo loco regionale secondo le diverse caratteristiche dei pazienti , insieme alle differenze osservate allanalisi univariata . 
quando si considerano i fattori correlati al paziente , let ha un impatto significativo sulla sopravvivenza non corretta , con i pazienti pi anziani che mostrano un rischio pi elevato , ma nessun impatto sulla dss e sul lrc . 
tra i fattori correlati al tumore , listotipo epidermoide , categorie t ed n ed uno stadio clinico pi avanzati mostrano tutti un significativo effetto prognostico avverso allanalisi univariata , per tutti gli outcomes ( tabella 2 )  . 
 tra le caratteristiche legate al trattamento , i periodi pi recenti e il trattamento del volume linfonodale ( anche con una dose inferiore ai 46 gy ) sono correlati ad una prognosi migliore allanalisi uni variata , per tutti gli outcomes . 
 i 9 pazienti ( 1% ) non trattati precauzionalmente sul collo hanno lrc , dss e os significativamente peggiori , anche se tutti allinizio ( al momento della diagnosi ) non presentavano linfonodi del collo clinicamente positivi . 
the differences in os , dss and lrc observed in the entire series according to patient and tumour - related factors and their statistical significance remained substantially the same when the analysis was limited to n0 patients ( data not shown )  . 
si deve comunque sottolineare che i pazienti trattati con campi separati per la rinofaringe e per il collo e con dosi pi basse al rinofaringe , mostrano una dss e una oss peggiori , anche se la differenza non significativa ( valore di p compreso tra 0 , 1 e 0 , 2 )  . 
 daltronde , quando la dose al tumore stata considerata una variabile continua , un aumento della dose al tumore risultato associato ad una os migliore ( hazard ratio = 0 , 97 / gy , di significato statistico borderline p = 0 , 07 )  . con lintento di chiarire se le pi elevate dosi ai linfonodi nei pazienti di flo , o le diverse tecniche avessero un impatto sugli outcomes analizzati , abbiamo ripetuto lanalisi univariata solo per i casi n0 ( n = 192 ) , considerando gli stessi fattori scelti per le serie intere , eccetto lo stadio clinico e la categoria n . 
le differenze in os , dss e lrc osservate nelle serie intere secondo i fattori correlati al paziente e al tumore e la loro significativit statistica rimangono sostanzialmente le stesse anche quando si limita lanalisi ai pazienti n0 ( dati non mostrati in dettaglio )  . 
the initial cox model included the following variables : centre treating the patients , year of accrual , age , gender , histological subgroup , clinical stage , dose to the nasopharynx and maximal dose to the neck nodes , fractional dose , treatment technique and staging modality ( conventional radiology , ct or mri )  . 
the final model obtained after computation for the three outcomes considered ( os , dss , lrc ) is shown in table 4 . it is clear that the major prognostic factors for os and dss were patientand tumour - related factors . 
increasing age and male gender were related to a more unfavourable prognosis for both os and dss ; the same is true for the epidermoid histology and for a more advanced clinical stage . 
il modello iniziale di cox includeva le seguenti variabili : il centro in cui sono stati trattati i pazienti , lanno di reclutamento , let , il genere , listotipo ( sottogruppo ) , lo stadio clinico , la dose alla rinofaringe e la massima dose data ai linfonodi del collo , la dose / frazione , la tecnica di trattamento e la modalit di stadiazione ( radiologia convenzionale , ct o mri )  . 
il modello finale ottenuto per i tre outcomes considerati ( os , dss , lrc ) mostrato in tabella 4 . chiaro che i pi importanti fattori prognostici per os e dss sono quelli pazientee tumore - correlati . 
let avanzata e il genere maschile sono correlati ad una prognosi pi sfavorevole sia per los che per la dss ; lo stesso vale per listotipo epidermoide e per gli stadi clinici pi avanzati . 
 comunque la dose alla rinofaringe ( come variabile continua ) risultata anchessa quasi significativamente correlata alla sopravvivenza globale ( p = 0 , 056 ) e la tecnica ho - like risultata correlata ad un lieve ma significativo aumento della sopravvivenza specifica per malattia ( p = 0 , 045 )  . 
results were substantially the same as in the entire population ( data not shown )  . miglior controllo locoregionale sono lo stadio clinico meno avanzato , listotipo indifferenziato e la tecnica ho - like , specialmente se la sovradose ( boost ) alla rinofaringe era stata data con fotoni > 10 mev . 
i risultati sono sostanzialmente gli stessi che nellintera popolazione ( dati non mostrati in dettaglio )  . discussion tables 5 , 6 and 7 show results reported in 60 articles , which were selected as defined in the materials and methods section and divided into three groups : papers dealing with npc patients accrued between 1950and 1970 and onward , between 1971 and 1989 and onward and from 1990 onward . 
the fraction of cases discussione le tabelle 57 mostrano i risultati riportati in sessanta articoli , selezionati come descritto nella sezione materiali e metodi e divisi in tre gruppi : articoli che trattano di pazienti con npc reclutati dal 1950 al 1970 , dal 1971 al 1989 e dal 1990 in poi . 
ogni confronto potrebbe sembrare inaccurato , poich attraverso questo ampio intervallo di tempo gli strumenti diagnostici disponibili sono cambiati notevolmente , ma si pu osservare che la frazione di pazienti senza malattia a livello linfonodale rimasta quasi la stessa ( circa il 25% ) in tutti i periodi di reclutamento . 
os ranges from 22% to 58% , 30% to 70% and 57% to 76% , respectively , in cases recruited from 1950 to 1970 , from 1971 to 1989 and from 1990 onwards . 
valori di sopravvivenza globale pari al 22%58% , 30%70% e 57% 76% , si sono osservati rispettivamente nei casi reclutati dal 1950 al 1970 , dal 1971 al 1989 e dal 1990 in poi . 
lanalisi univariata dei nostri dati ( tabella 2 e 3 ) ha mostrato che i fattori tumore e paziente - correlati sono prognosticamente pi importanti della dose e della tecnica radioterapica . 
comunque , stato radiol med ( 2012 ) 117 : 690714 table 4 multivariate analysis of factors potentially linked with overall ( os ) and disease - specific ( dss ) survival and localregional control ( lrc )  . 
a more recent update of the hong kong experience revealed that the advantage of the boost dose ( > 66 gy ) is much less evident in patients also treated with chemotherapy [ 68 ]  . 
a better local control for patients given a boost dose for histologically verified local persistence after a full radiotherapy course was confirmed in a randomised study by yan and coworkers [ 69 ]  . 
finally , when treating patients with imrt techniques , a clear advantage for dose escalation has not been shown [ 70 ]  . at univariate analysis , a lower fractional dose , the availability of ct and mri images to determine target volumes and use of the ho technique , preferably with a highenergy nasopharynx boost , contributed significantly to better lrc but not to better survival rates . 
it is therefore difficult to define the effect on the clinical results of each of the on the other hand , even large gains in local control might produce only smaller benefits in terms of survival because of the impact of distant failures . at multivariate analysis , patientand tumour - related factors ( stage , histology , gender , age ) were significantly related with survival . 
the better survival results obtained in female patients , although less frequently reported , were also observed in the large hong kong , beijing and taiwan series [ 12 , 24 , 36 ]  . 
therefore , it could be concluded that in our series , a better targeting process coupled with a moderately high nasopharynx dose ( in the 66to 70 - gy interval ) provides improved local control and , to a lesser extent , survival in the more recent accrual periods . 
 at both uniand multivariate analyses , exclusion of neck nodes from the treated volume achieves a significantly osservato nelle serie recenti un vantaggio prognostico per dosi pi elevate alla rinofaringe . 
un aggiornamento pi recente dellesperienza di hong kong ha rivelato che il vantaggio della sovradose ( oltre i 66 gy ) molto meno evidente nei pazienti trattati anche con chemioterapia [ 68 ]  . 
infine , non stato dimostrato alcun chiaro vantaggio per la dose - escalation se si trattano i pazienti con tecniche intensity - modulated radiation therapy ( imrt ) [ 70 ]  . allanalisi univariata , anche dosi / frazione inferiori , la disponibilit di immagini ct e mri per scegliere i volumi bersaglio , limpiego della tecnica di ho , preferibilmente con sovradose alla rinofaringe con fotoni di alta energia , hanno contribuito significativamente ad ottenere un miglior controllo locoregionale ma non migliori risultati in termini di sopravvivenza . 
questa osservazione appare collegata con il fatto che molti fattori terapeutici e tecnici sono cambiati nello stesso periodo : dunque difficile stabilire leffetto indipendente di ciascuno i loro sui risultati clinici . 
daltro canto , anche un importante miglioramento del controllo locale pu produrre solo benefici relativamente pi modesti in termini di sopravvivenza , a causa dellimpatto delle ricadute a distanza . allanalisi multivariata , i fattori pazientee tumorecorrelati ( stadio , istologia , genere , et ) sono risultati significativamente correlati con la sopravvivenza . 
sebbene ci sia riportato meno frequentemente in letteratura , i migliori risultati di sopravvivenza ottenuti in questa serie nelle femmine , sono stati osservati anche nelle serie di hong kong , beijing e taiwan , che includono un numero molto elevato di casi [ 12 , 24 , 36 ]  . 
dunque si pu concludere che , nelle serie recenti , una migliore definizione del volume bersaglio associata ad una dose alla rinofaringe moderatamente alta ( in un intervallo di 6670 gy ) hanno migliorato il controllo locale e in minor misura anche la sopravvivenza nei periodi di reclutamento pi recenti . 
 sia allanalisi uniche multivariata , lesclusione dei linfonodi del collo dai volumi di trattamento implica una radiol med ( 2012 ) 117 : 690714 706 radiol med ( 2012 ) 117 : 690714 radiol med ( 2012 ) 117 : 690714 708 radiol med ( 2012 ) 117 : 690714 radiol med ( 2012 ) 117 : 690714 710 radiol med ( 2012 ) 117 : 690714 radiol med ( 2012 ) 117 : 690714 worse prognosis for lrc , dss and os . 
however , this refers only to a very small group of cases , and the fact that a dose of 45 gy , or even less , to clinically uninvolved areas does not seem related with worse nodal control deserves special mention . 
ho and coworkers initially suggested that it is not necessary to treat uninvolved neck nodes [ 3 ] , but this assumption was rejected after the retrospective analysis of more than 5 , 000 hong kong cases published by lee and coworkers in 1992 , which conclusively showed that not only local recurrence but also distant metastases rates are clearly higher in patients in whom the uninvolved neck was not treated [ 35 ]  . 
qin and coworkers analysed the beijing series of more than 1 , 300 cases and clearly demonstrated that significantly worse survival results are obtained in patients in whom uninvolved neck nodes were not treated . 
this was confirmed our analysis . conclusions our clinical material was largely recruited before the chemotherapy era , and the bulk of the literature available today , including a few randomised trials and two metaanalyses [ 72 ] , clearly demonstrate the advantage of platinum - based concomitant chemotherapy in advanced cases . 
 nonetheless , results of our analysis might contribute to the understanding of the more promising radiotherapy techniques , such as three - dimensional conformal radiotherapy ( 3d - crt ) and imrt to improve local control but not to give higher nasopharynx doses . 
there is no need for doses in excess of 70 gy , either to the nasopharynx or to neck nodes , to improve local control : our data , along with a large part of the literature , point in that direction . 
in fact , this technical solution , adopted for the more recently treated patients , seems to obtain better dosimetric results and is gaining an increasing diffusion [ 73 , 74 ]  . 
it is very likely , however , that the concomitant effect of more standardised treatment techniques and the use of more efficient imaging modalities in the diagnostictherapeutic workup of our patients contributed significantly to the better clinical results obtained in the more recent time periods . 
 comunque , ci si riferisce solo ad un gruppo molto piccolo di casi , e merita menzione il fatto che una dose di 45 gy , o anche minore , data alle aree non clinicamente coinvolte , non sembra correlata ad un peggior controllo linfonodale . 
 ho [ 3 ] aveva inizialmente suggerito che non fosse necessario trattare i linfonodi del collo non coinvolti , ma questa affermazione fu rigettata dopo unanalisi retrospettiva di pi di 5000 casi di hong kong , pubblicati da lee et al . 
 [ 35 ] nel 1992 che hanno dimostrato definitivamente che non solo la ricaduta locale , ma anche le metastasi a distanza sono chiaramente pi frequenti tra i pazienti non trattati sul collo clinicamente indenne . 
 [ 12 ] hanno analizzato la casistica di beijing di pi di 1300 casi e dimostrato chiaramente che si ottenevano risultati di sopravvivenza significativamente peggiori nei pazienti non trattati sui linfonodi del collo clinicamente indenni ; questi autori concludono che il livello di dose ottimale quello compreso tra 40 e 50 gy [ 12 ]  . 
ci stato confermato dalla presente analisi . conclusioni il nostro materiale clinico in gran parte reclutato prima dellera della chemioterapia , e la mole di letteratura disponibile oggi , inclusi alcuni trial randomizzati e due meta - analisi [ 72 ] , hanno dimostrato chiaramente il vantaggio della chemioterapia concomitante a base di platino nei casi avanzati . 
 comunque , i risultati della presente analisi possono contribuire alla nostra comprensione di come le tecniche radioterapiche pi promettenti , come la radioterapia tridimensionale conformazionale ( 3dcrt ) e limrt , possano migliorare il controllo locale senza dare dosi pi elevate alla rinofaringe . 
non necessario superare i 70 gy , sia per la rinofaringe che per i linfonodi del collo , per migliorare il controllo locale : i nostri dati , in linea con una vasta parte dei dati della letteratura , vanno in tale direzione . 
attualmente a brescia e a firenze , con luso del boost simultaneo con la tecnica imrt , considerata accettabile una dose / frazione al ctv linfonodale di 1 , 71 , 8 gy . 
infatti sembra che questa soluzione tecnica , adottata per i pazienti trattati pi recentemente , ottenga risultati dosimetrici migliori ed sia di sempre pi di ampia diffusione [ 73 , 74 ]  . infine , non si evidenziato allanalisi multivariata , un ben delineato effetto sulla sopravvivenza di ogni singolo avanzamento tecnico adottato nel periodo di reclutamento di interesse ; probabile , comunque , che leffetto concomitante di tecniche di trattamento pi standardizzate e dellinclusione nelliter diagnostico - terapeutico dei nostri pazienti di modalit di imaging pi efficienti , abbia contribuito significativamente ad ottenere migliori risultati clinici pi di recente . 
 limrt potrebbe anche migliorare i risultati , attraverso una migliore copertura dei volumi bersaglio , come ripe712 radiol med ( 2012 ) 117 : 690714 justify the enduring effort to treat our patients with imrt , which could also improve results through better coverage of the target volumes , as has been repeatedly suggested but never conclusively demonstrated . 
the effect of evolution of technical solutions over the last two decades on the incidence of the late effect of treatment given is the subject of a companion paper [ 75 ]  . acknowledgements the work described in this article was performed in the framework of the european integrated project methods and advanced equipment for simulation and treatment in radio - oncology ( maestro ) no . 
senologia clinica e screening mammografico , dipartimento di radiodiagnostica , apss trento i , viale verona centro per i servizi sanitari , palazzina c , piano terrazza , 38100 trento , italy 2servizio osservatorio epidemiologico , direzione promozione ed educazione alla salute , apss , trento , italy 3centro prevenzione screening , ulss 16 , padova , italy correspondence to : d . 
in agreement with previous studies , visual classification of mammography density according to bi - rads quantitative criteria was highly reproducible among readers ; nevertheless , attribution to the dense breast ( bi - rads d34 ) category , which might be adopted as a determinant of different screening protocols ( such as adjunct ultrasonography or yearly interval ) varied riassunto obiettivo . 
in accordo con precedenti studi la classificazione visuale della densit mammografica secondo i criteri bi - rads risultata altamente 520 radiol med ( 2012 ) 117 : 519528 among readers ( range 615% )  . 
controlled studies should be performed comparing visual with computer - density category attribution , the latter possibly being a better alternative due to its absolute reproducibility . keywords breast diagnosis mammography density riproducibile tra i diversi lettori : ci nonostante lattribuzione della categoria seno denso ( bi - rads d3 - 4 ) , che potrebbe essere adottata come determinante di protocolli di screening differenziati ( aggiunta dellecografia , frequenza annuale ) varia tra i lettori ( in questo studio dal 6% al 15% )  . 
necessitano studi controllati che confrontino la classificazione visuale con quella computerizzata , potendo questultima essere una valida alternativa per la sua riproducibilit assoluta . parole chiave mammella diagnosi mammografia densit introduction introduzione breast radiological density is an important variable in diagnosing breast cancer . 
it has been associated with breast cancer risk on an individual [ 14 ] and familial [ 57 ] basis and is likely associated with mammography sensitivity , being a determinant of interval cancer risk [ 814 ]  . 
 the method most commonly used to classify mammography density is quantitative , proposed by the american college of radiology in the breast imaging reporting and data system ( bi - rads ) [ 15 ] , which has replaced the less reproducible wolfes patterns [ 1 , 3 ]  . 
bi - rads classification is commonly determined on a visual basis [ 3 , 5 , 9 , 16 ] ; however , being subjective and associated with suboptimal reproducibility [ 1719 ] , its replacement with absolutely reproducible computerised assessment has been suggested [ 6 , 7 , 19 , 20 ]  . in this study , a set of mammograms was classified according to bi - rads quantitative density classification by a panel of radiologists involved in mammography reporting . 
the aim was to assess interobserver reproducibility of visual classification , its reliability in clinical use and the need for alternative methods such as computerised density assessment . materials and methods the study was based on a set of 100 mammograms ( digitalised mediolateral oblique and craniocaudal views of original film - screen mammograms ) of women aged 5069 years attending the florence , italy , screening programme : the same digitalised set had been used in a previous study of density classification reproducibility [ 21 ]  . 
the set was made up of 69 screening tests consecutively reported as negative and 31 reported as negative and followed by interval cancers consecutively observed in the following 2 years . 
essa stata correlata al rischio di carcinoma mammario su base individuale [ 14 ] o ereditaria [ 57 ] , ed verosimilmente associata alla sensibilit della mammografia essendo una determinante del rischio di carcinoma di intervallo [ 814 ]  . la classificazione pi comunemente usata per la definizione della densit quella quantitativa percentuale , considerata pi efficace dei patterns di wolfe [ 1 , 3 ] e proposta dallamerican college of radiology nel sistema breast imaging reporting and data system ( bi - rads ) [ 15 ]  . 
la classificazione della densit secondo bi - rads comunemente definita su base visuale [ 3 , 5 , 9 , 16 ] , anche se soffre di soggettivit e implica problemi di riproducibilit [ 17 19 ] , al punto che si suggerita come alternativa la valutazione computerizzata [ 6 , 7 , 19 , 20 ]  . lo scopo del presente studio , che stato effettuato sottoponendo un set di mammografie ad un panel di radiologi comunemente addetti alla refertazione mammografica , quello di valutare la riproducibilit interosservatore nella attribuzione della categoria di densit percentuale birads , al fine di definire se la valutazione visuale sia affidabile nella pratica clinica o debba essere abbandonata in favore a metodi alternativi pi affidabili quale quello computer - assistito . materiali e metodi lo studio si basato sulla lettura di un set di 100 mammografie digitali ottenute da immagini originali analogiche ( due proiezioni : medio laterale obliqua e cranio caudale ) di donne con et compresa tra 50 e i 69 anni partecipanti al programma di screening mammografico di firenze ; lo stesso set di immagini digitalizzate era stato impiegato in un precedente studio di riproducibilit della classificazione radiol med ( 2012 ) 117 : 519528 clinical and screening mammography ( at least 5 , 000 readings / year ) were involved . 
information was given on density reporting criteria as provided on the web site by the american college of radiology , with special mention to estimate the volume of the breast showing fibroglandular density by integrating the information of density area from the two standard mammography views [ 21 ]  . 
the set was examined independently by each reader and classified according to four density categories : d1 = 025% , d2 = 2650% , d3 = 5175% , d4 = 76100% . 
the original set of 100 digitalised images was used , but the original reports by the panel of 12 radiologists were available only for the first half of the set . 
as this did not imply selection bias , the available report set was still large ( 600 readings ) , and the 12 radiologists were not specially trained in bi - rads density reporting ( unlike radiologists in this study and most radiologists currently involved in screening reading ) , we decided to use it as a side reference standard for the purposes of the study and for determining interobserver readers . 
 agreement of the six radiologists in this study was thus assessed : ( a ) against the majority report of the panel ( set of 50 cases ) and ( b ) by comparing reports of the six radiologists in all possible pairs ( 15 , 000 cases ; 15 pairs )  . 
when considering four density categories , the weighted kappa formula was used , which takes into account the degree of disagreement ( one or two degrees ) [ 22 ]  . 
for such analysis , the sas 9.1 statistical package was used . reproducibility between single differences in the distribution of breast density category attribution between readers were checked by the chi - square test , with statistical significance being set at p < 0.05. results table 1 shows the distribution of density categories attributed by the six radiologists in the set of 100 cases . 
il set consiste di 69 esami di screening consecutivi diagnosticati come negativi e di 31 esami di screening diagnosticati come negativi e seguiti da carcinomi di intervallo consecutivi , osservati nei due anni successivi . 
hanno partecipato allo studio attuale sei radiologi esperti nella lettura della mammografia clinica e di screening ( almeno 5000 letture / anno ) ; tali radiologi non utilizzavano correntemente la classificazione bi - rads della densit mammografica , i cui principi sono stati illustrati sommariamente prima dello studio di classificazione . 
 stata fornita linformazione disponibile sul sito web dellamerican college of radiology relativamente ai criteri di classificazione , in particolare per la stima del volume di mammella occupato da densit fibroghiandolare , integrando linformazione derivata dalla stima dellarea di densit nelle due proiezioni standard [ 21 ] .ognuno dei radiologi ha visionato separatamente il test classificando ogni caso secondo una delle categorie di densit bi - rads ( d1 = 0% 25% , d2 = 26%50% , d3 = 51%75% , d4 = 76%100% del volume mammario occupato da densit fibroghiandolare )  . 
convenzionalmente valori di kappa di 0 , 000 , 20 , 0 , 210 , 40 , 0 , 410 , 60 , 0 , 610 , 80 e 0 , 811 , 00 vengono considerati rispettivamente indicativi di concordanza minima , scarsa , moderata , sostanziale e quasi perfetta [ 22 ]  . in mancanza di uno standard di riferimento per la definizione della corretta classificazione , la concordanza stata valutata in due diversi scenari . 
in un set di 50 casi era disponibile la diagnosi di maggioranza posta da un panel di 12 lettori che avevano partecipato ad un precedente studio [ 21 ] condotto con analoga finalit . 
il set originale di 100 esami digitalizzati era disponibile alluso , ma sfortunatamente le valutazioni originali da parte del panel di 12 lettori erano disponibili solo per la prima met del set . 
dal momento che questo non implicava alcun vizio di selezione , che il set era ancora sufficientemente ampio ( 600 letture ) e che i radiologi del panel non erano particolarmente addestrati alla classificazione bi - rads della densit ( come non lo erano i radiologi coinvolti nel presente studio e la maggioranza dei radiologi correntemente addetta alla lettura di screening ) abbiamo deciso di usare la valutazione del panel come standard di riferimento al fine dello studio , oltre alla valutazione della riproducibilit interoperatore tra i singoli lettori . 
table 2 shows the results of agreement assessment ( standard and weighted kappa ) on a four - category basis compared with the referimpiegate nella definizione di seno denso e non denso . 
nella valutazione che considera quattro categorie di densit stata impiegata la formula del kappa pesato che valuta diversamente il peso delle discordanze in funzione della loro entit ( uno , due o tre ordini di misura ) [ 22 ]  . 
la tabella 2 riporta i risultati della valutazione di concordanza ( kappa semplice e pesato ) dei sei lettori nella attribuzione delle quattro categorie bi - rads di densit rispetto al panel di riferimento [ 21 ]  . 
this will enable the use of breast density categories as an indicator for tailored diagnostic approaches ( such as adding ultrasonography or using shorter screening intervals in the presence of negative mammography and dense breast )  . 
it is evident that volumetric density must be estimated for such a purpose and not simply the area of density in each mammography view , which may also vary by view . 
this aspect has been discussed and detailed in a previous study [ 21 ] , and the assumption that volumetric density based on integration of area densities derived from the two mammographic views is needed is crucial to allow proper clinical use of breast - density assessments . this study was based on a reference set and a panel of readers , both of which were sufficiently large to provide reliable assessment of interobserver reproducibility in categorising quantitative breast density according radiol med ( 2012 ) 117 : 519528 e quasi perfetta per uno . 
 a parte le considerazioni statistiche , in base alle diverse coppie di lettori da 6 a 15 soggetti su 100 possono essere classificati diversamente dal punto della densit ( valutazione comparativa tra categorie d12 e d34 ) e potrebbero essere avviati a diversi regimi di sorveglianza in funzione del singolo lettore . discussione come suggeriscono i principi della classificazione birads , la valutazione della densit deve fornire una stima delleffetto mascherante della densit stessa e funzionare come predittore di un effetto negativo sulla sensibilit . 
ci consentir luso delle categorie di densit come indicatori per una scelta personalizzata del successivo approccio diagnostico ( come ad esempio laggiunta dellecografia , o ladozione di un intervallo di screening pi breve in presenza di seno denso )  . 
evidente che a tal fine la valutazione della densit deve essere volumetrica e non solo definire larea di densit nelle due proiezioni , anche in considerazione del fatto che ci possono essere differenze sostanziali tra le proiezioni . 
ad esempio una densit volumetrica di un quarto ( 25% , corrispondente ad esempio a un quadrante ) si tradurr in una area di densit del 50% in entrambe le proiezioni , mentre una densit volumetrica occupante met della mammella ( 50% , ad esempio corrispondente ad entrambi i due quadranti inferiori ) si tradurr in unarea di densit del 100% nella proiezione assiale e del 50% nella proiezione laterale . 
questo aspetto stato discusso in dettaglio in un precedente studio [ 21 ] e la consapevolezza che la definizione di una densit volumetrica , basata sulle densit di area stimate nelle due proiezioni , cruciale per consentire un uso clinico adeguato della densit . 
 lo studio si basa su una casistica di riferimento e su un panel di lettori sufficiente a valutare la concordanza della attribuzione della densit radiologica del seno secondo la classificazione quantitativa bi - rads , come dimostrato anche dai limiti di confidenza della statistica kappa che spaziano sempre solo in una categoria diagnostica adiacente a quella della stima puntuale . 
 even assuming differences in breast density as displayed at screen - film and digital mammography ( breasts with intermediate density at screen - film mammography might be attributed to a less dense category at digital mammography ) , the study addresses judgement reproducibility of density , not the prevalence of density categories . 
thus , using digitalised original screen - film mammograms should not represent a real bias in consideration of the study purpose . this study confirms that interobserver agreement in reporting breast density according to bi - rads quantitative criteria is satisfactory , which confirms the findings of a previous study on the same mammography set [ 21 ]  . 
some un appunto metodologico allo studio potrebbe riguardare il fatto che la casistica campione consiste di mammografie analogiche successivamente digitalizzate , nelle quali la densit mammaria potrebbe risultare diversa in rapporto ad un maggiore potere di risoluzione della mammografia digitale con una conseguente maggiore sensibilit nei seni densi [ 23 , 24 ]  . 
pur ipotizzando che la definizione dellimmagine in mammografia digitale sia diversa da quella analogica ( seni di densit intermedia alla analogica possono risultare meno densi alla digitale ) , il presente studio si riferisce alla riproducibilit del giudizio relativo alla densit e non alla prevalenza delle diverse densit ; ne consegue che luso di casistica originalmente acquisita con metodo analogico non dovrebbe costituire un vizio di rilievo per lo studio . lo studio conferma che la concordanza inter - operatore nella classificazione quantitativa , analogamente ad un precedente studio condotto in italia sulla stessa casistica campione [ 19 , 21 ]  . 
the latter has been reported to improve sensitivity and might become a routine reality in the future [ 2527 ]  . the idea of automatic computer assessment of density is definitely appealing , as it reduces radiologists workload and is supposed to have absolute reproducibility . 
it is worth noting that the study was performed by readers who were not particularly trained in using the bi - rads density classification and did not use it in daily practice . 
 in this study , despite the high judgement reproducibility on statistical grounds , patients with dense breast ( d34 ) , a category that might be adopted for special diagnostic protocols , differed by 615% depending on the reader . 
 although computerised density assessment may be appealing , few reports on the subject suggest that volumetric breast density values as determined by computer are systematically lower compared with visual classification [ 28 , 29 ]  . 
considering that all we know about breast density value as a risk factor or as a determinant of mammography sensitivity is based on visual classification , breast density values obtained by computer should be adapted to match commonly used visual classification categories . 
in particolare questultima opzione pare avere risvolti diagnostici positivi e potrebbe in futuro entrare nella routine [ 2527 ]  . lidea di una valutazione automatica della densit mediante computer indubbiamente allettante , sia perch solleva il radiologo da un carico di lavoro , sia perch consente una riproducibilit assoluta . 
 bene notare che il presente studio stato condotto con operatori non particolarmente addestrati alla classificazione bi - rads di densit che non era infatti impiegata nella routine di lavoro : legittimo pensare che un congruo addestramento potrebbe consentire concordanze anche superiori a quella naturale osservata . 
nel presente studio , pur in presenza di una forte concordanza di giudizio sul piano statistico , un fatto che lattribuzione di densit potenzialmente implicante diversi protocolli diagnostici , varia in questo studio dal 6% al 15% in funzione delloperatore . 
un simile impegno non pare giustificato e sarebbe meglio esplorare laffidabilit della determinazione computerizzata della densit , che ha una riproducibilit pressoch assoluta . se quindi una stima computerizzata della densit comunque gradita , dalle limitate evidenze di letteratura risulta che il valore percentuale di densit ( su base volumetrica ) fornito dal computer sia sistematicamente inferiore a quello attribuito dalluomo su base visuale [ 28 , 29 ]  . 
poich tutto quello che conosciamo sul valore della densit mammografia , sia come fattore di rischio sia come determinante della sensibilit della mammografia , si basa su categorie determinate con classificazione visuale , evidente che i valori ottenibili con la valutazione computerizzata debbano essere tradotti nellequivalente visuale di comune uso . 
per tale motivo auspicabile che vengano condotti studi controllati che confrontino la valutazione visuale e quella computerizzata , in modo da consentire la traduzione della stima computerizzata in valori comparabili alla stima visuale . 
questo faciliter luso corrente dei software per la valutazione automatica radiol med ( 2012 ) 117 : 519528 implemented as a tool in digital mammography workstations . della densit che gi cominciano a comparire in commercio come optional nelle stazioni di lettura mammografica . overall , limitations are evident for all methods of evaluating density as a ratio of fibroglandular density to absolute breast volume starting from more or less precise and reproducible values of 2d - assessed density area values . 
a more precise assessment might be possible in the future by breast density evaluation using tomosynthesis imaging , which might best fit breast density use as a covariate in breast cancer risk modelling . nel complesso evidente che ci sono limiti per qualsiasi metodo voglia valutare la densit radiologica su base volumetrica partendo da misurazioni pi o meno precise e riproducibili della densit di area su base bidimensionale . 
part ii : evolving technical choices and toxicity patterns uno studio di riferimento su 883 pazienti affetti da neoplasia della rinofaringe trattati in due centri italiani dal 1977 al 2000 . 
alberti , spedali civili , piazzale spedali civili 1 , 25123 brescia , italy 2radioterapia , universit degli studi di brescia , brescia , italy 3radioterapia , ospedale careggi , firenze , italy 4universit degli studi di firenze , firenze , italy 5radioterapia , ospedale di arezzo , arezzo , italy correspondence to : l . 
results of this benchmark study may have implications for understanding and developing new radiotherapy techniques , such as three - dimensional conformal radiotherapy ( 3d - crt ) and , in particular , intensity - modulated radiotherapy ( imrt ) for npc patients . 
sono stati studiati 883 pazienti consecutivamente trattati con radioterapia dal 1977 al 2000 a firenze ( flo , florence ) e brescia ( ira , istituto del radio alberti )  . 
i risultati di questo studio di riferimento potrebbero avere implicazioni anche per la comprensione e lo sviluppo delle nuove tecniche radioterapiche , come la radioterapia tridimensionale conformazionale ( 3dcrt ) e specialmente la radioterapia a modulazione dintensit ( imrt )  . keywords nasopharyngeal cancer radiotherapy treatment techniques complications patterns of care parole chiave neoplasia della nasofaringe radioterapia tecniche di trattamento complicanze terapie 716 introduction due to the low incidence of nasopharyngeal cancer ( npc ) in europe and western countries , the availability of large study series is limited [ 1 ]  . 
we therefore studied a large italian series of patients with npc , treated consecutively over > 20 years at the florence university radiation oncology department ( flo ) and at the brescia university radiation oncology department istituto del radio o . 
our aim was to define outcomes for patients treated with conventional radiation techniques , according to different features and in the different accrual periods , to better define the possible role of new radiation techniques to improve survival and reduce late effects of treatment . 
tumour and node ( tn ) categories and clinical stage were retrospectively reassigned according to the 2002 union for international cancer control tumour node metastasis ( uicc / tnm ) classification [ 2 ]  . 
subgroups of the t2 category ( t2a and t2b indicating , respectively , patients without and with parapharyngeal space invasion ) were not considered , however , due to variations in the staging modalities adopted throughout the accrual period to limit as far as possible the stage migration phenomenon within this group . 
consequently , the subcategories ( a and b ) of stage ii disease were not considered separately . clinical features and staging and treatment modalities adopted during the study period have been described in detail in the companion paper devoted to survival analysis [ 3 ]  . 
four subsequent accrual periods radiol med ( 2012 ) 117 : 715724 introduzione a causa della bassa incidenza del cancro della rinofaringe ( npc ) in europa e nei paesi occidentali , la disponibilit di serie numerose di pazienti limitata [ 1 ]  . 
abbiamo perci deciso di studiare una serie italiana molto ampia di pazienti con npc , trattati consecutivamente in un arco di tempo di oltre 20 anni al dipartimento di radioterapia delluniversit di firenze ( flo ) e al dipartimento di radioterapia delluniversit di brescia , istituto del radio o . 
obiettivo dello studio la definizione degli outcomes nei pazienti trattati con tecniche convenzionali di radioterapia , a seconda delle differenti caratteristiche e nei diversi periodi di reclutamento , per delineare meglio il possibile ruolo delle nuove tecniche radioterapiche nel miglioramento della sopravvivenza e nella riduzione degli effetti tossici tardivi del trattamento . 
abbiamo diviso la nostra analisi in due articoli tra loro associati : questo dedicato agli effetti tardivi del trattamento . materiali e metodi abbiamo condotto un analisi retrospettiva sulle cartelle cliniche di 883 pazienti trattati consecutivamente a titolo radicale a flo e allira dal 1977 al 2000 . 
le categorie tumore e stadio linfonodale ( tn ) e lo stadio clinico sono state riassegnate retrospettivamente secondo la classificazione union for international cancer control ( uicc ) tumore / linfonodi / metastasi ( tnm ) del 2002 [ 2 ]  . 
i sottogruppi della categoria t2 ( t2a e t2b , indicanti rispettivamente pazienti senza e con invasione dello spazio parafaringeo ) non sono stati tuttavia considerati , per limitare quanto possibile il fenomeno della migrazione di stadio allinterno di tale gruppo , a causa delle variazioni delle modalit di stadiazione adottate nellarco di tutto il periodo di reclutamento . 
di conseguenza , anche le sottocategorie ( a e b ) dello stadio ii non sono state considerate separatamente . le caratteristiche cliniche e le modalit di stadiazione e di trattamento adottate durante il periodo di studio sono state descritte in dettaglio nellarticolo dedicato allanalisi della sopravvivenza [ 3 ]  . 
la distribuzione dei casi secondo la categoria t e lo stadio clinico era la seguente : t1 , 35% ; t2 , 30% , t3 , 18% , t4 , 17% ; stadio i , 5% , ii , 32% , iii , 28% ; ivab , 35% . prima della radioterapia tutti i pazienti sono stati sottoposti ad una valutazione clinica , ad esami ematochimici di routine , radiografia del torace e faringo - laringoscopia . 
 radiol med ( 2012 ) 117 : 715724 were identified ( 19771985 , 19861990 , 19911995 and 19962000 ) , representing , respectively , 39% , 19% , 21% and 21% of the entire series . 
in these four periods , up - todate imaging modalities were magnetic resonance imaging ( mri ) and computed tomography ( ct ) ( adopted , respectively , in 3% , 19% , 44% , 84% and 50% , 77% , 54% , 16% of patients )  . 
in the years 19771985 , 47% of cases were staged with conventional radiological procedures only . regarding treatment , total and fractional doses to the nasopharynx at the midline along the central axis ( icru ) point were equal to , respectively , 65 gy , 6670 gy and > 70 gy in 15% , 64% and 21% of cases , and to > 2 gy ( but < 2.3 gy ) in 59% . 
at ira , in the first part of the accrual period ( 19771985 ) , the nasopharynx and the lymphatic regions of the neck were treated separately : the nasopharynx with parallel opposed ll fields ( 1018 - mev photons ) and the neck nodal regions with appositional electron fields of variable energy ( 912 mev ) and dimensions ( 132 cases )  . 
 all remaining patients of both centres were treated with a cobalt source or with 5to 6 - mev photons from a linac and with a ho - like technique , with ( 379 cases ) or without ( 372 cases ) a boost dose to the nasopharynx delivered with veryhigh - energy photons ( 18to 31 - mev photons ) [ 3 , 4 ]  . 
in the flo series , patients treated with this very - high - energy boost dose were also treated with a ho - like technique and none with the earlier technique using appositional electron fields to cover the neck lymphatic areas . 
 follow - up always included clinical examination every 2 to 3 months in the first posttreatment year and at longer intervals thereafter ; ct / mri scans ( after their availability ) and other imaging procedures were obtained less often and not in all patients during the follow - up period . statistical evaluation the different types of complications were noted in the clinical records and we report , as the majority of papers published on npc do , the crude incidence of late damage , relating it with some clinical and therapeutic factors . 
analysis was conducted on the entire series and then limited to patients continuously disease free after treatment to exclude a possible bias deriving from the confounding effect of symptoms linked with relapse and from the adverse effects of the treatsono stati identificati quattro periodi di reclutamento successivi ( 19771985 , 19861990 , 19911995 , e 19962000 ) includendo rispettivamente il 39% , il 19% , il 21% e il 21% dellintera serie . 
in questi quattro periodi le modalit di imaging pi evolute , risonanza magnetica ( mri ) , e tomografia computerizzata ( ct ) sono state adottate rispettivamente nel 3% , 19% , 44% , 84% e 50% , 77% , 54% , 16% dei pazienti . 
 negli anni 19771985 , il 47% dei casi era stato quindi stadiato solo con procedure di radiologia convenzionale . per ci che riguarda il trattamento , la dose totale e la dose / frazione alla rinofaringe al punto international commission on radiation units and measurements ( icru ) sono risultate pari rispettivamente a 65 gy , 6670 gy e > 70 gy nel 15% , 64% e 21% dei casi e ad oltre 2 gy ( ma meno di 2 , 3 gy ) nel 59% di essi . 
allira , nella prima parte del periodo di studio ( dal 1977 al 1985 ) , la rinofaringe e le regioni linfonodali del collo sono state trattate separatamente : la rinofaringe con campi contrapposti paralleli latero - laterali ( ll ) ( fotoni da 1018 mev ) e le regioni linfonodali del collo con campi apposizionali di elettroni di energia e dimensioni variabili ( 912 mev ) ( 132 casi )  . 
tutti i restanti pazienti di entrambi i centri sono stati trattati con una sorgente di cobalto o con fotoni da 56 mev da un acceleratore lineare e con una tecnica ho - like , con ( 379 casi ) o senza ( 372 casi ) una sovradose alla rinofaringe , rilasciata con fotoni di energia molto elevata ( da 18 a 31 mev ) [ 3 , 4 ]  . 
nella serie di brescia , i pazienti trattati con queste sovradosi ( boost ) di energia molto alta sono stati trattati anche con una tecnica ho - like e nessuno stato trattato con le tecniche pi datate , usando campi apposizionali di elettroni per coprire le aree linfatiche . 
la chemioterapia ( cht ) stata somministrata ad una minoranza di pazienti selezionati molto sfavorevolmente ( 20% ) e con schemi differenti , oggi considerati obsoleti . il follow - up dopo il trattamento ha sempre incluso una valutazione clinica ogni 23 mesi nel primo anno dopo il trattamento e successivamente ad intervalli pi lunghi ; la ct e la mri ( da quando disponibili nei due centri ) e le altre procedure di imaging sono state effettuate meno spesso e non in tutti i pazienti durante il periodo di follow - up . valutazione statistica i diversi tipi di complicanze sono stati registrati nelle cartelle cliniche e , come nella maggior parte dei lavori pubblicati sul npc , nel presente lavoro si riporta lincidenza assoluta del danno tardivo , in relazione ad alcuni fattori clinici e terapeutici . 
 718 results radiol med ( 2012 ) 117 : 715724 da malattia dopo il trattamento , per escludere un possibile errore derivante dalleffetto confondente dei sintomi correlati alla ricaduta e dagli effetti avversi del trattamento somministrato alla ricaduta . 
per il calcolo stato utilizzato il software spss 12.02 for windows ( copyright spss inc , 19892003 )  . the crude incidence of the different late effects in patients who were continuously disease free after treatment was almost the same as in the entire series and therefore is not reported in the following paragraphs . risultati incidence of late effects in the entire series xerostomia and hypoacousia were the more frequently reported long - term complications , and their crude incidence in the entire series was 45% and 8% , respectively . 
the incidence of clinically relevant xerostomia reported in the clinical notes increased from 35% to 64% ( p < 0.001 ) in the more recent accrual periods ( 19902000 ) in comparison with previous periods ( 19771989 )  . 
 similarly , in more than a quarter of patients recruited earlier ( 27.7% ) , neck volume was treated only with separate electron fields , as opposed to none in the more recent years ( p < 0.001 ) ; this might also have contributed to a lower average dose to the salivary glands in patients treated during the 19771989 period owing to exclusion of part of the gland from the treated volume [ 3 ]  . 
trismus incidence decreased from 10.5% in patients treated 19771989 to 6.4% in those treatlincidenza assoluta dei differenti effetti tardivi nei pazienti continuativamente liberi da malattia dopo il trattamento risultata quasi la stessa di quella registrata nellintera serie e pertanto non viene riportata nei seguenti paragrafi . incidenza degli effetti tardivi in tutta la serie xerostomia e ipoacusia sono le complicanze a lungo termine pi frequentemente riportate e la loro incidenza assoluta nella serie intera rispettivamente del 45% e dell8% . 
lincidenza di xerostomia clinicamente rilevante riportata nelle cartelle cliniche aumentata dal 35% al 64% ( p < 0 , 001 ) nei pi recenti periodi di reclutamento ( 19902000 ) in confronto ai periodi precedenti ( 19771989 )  . 
inoltre la percentuale di pazienti trattati con una dose alla rinofaringe ( e ai linfonodi della parte superiore del collo ) superiore a 65 gy significativamente aumentata nei periodi pi recenti ( dal 2 , 2% al 26 , 4% , p < 0 , 001 )  . 
analogamente , in pi di un quarto dei pazienti reclutati prima del 1990 ( 27 , 7% ) , il volume linfonodale del collo stato trattato solo con campi separati di elettroni , mentre negli anni pi recenti ci non mai accaduto ( p < 0 , 001 ) ; questo potrebbe aver anche contribuito ad una riduzione della dose media alle ghiandole salivari nei pazienti trattati tra il 1977 e il 1989 , a causa dellesclusione di almeno una parte del tessuto ghiandolare dal volume di trattamento [ 3 ]  . la perdita delludito e la sordit sono state invece riportate con sufficiente accuratezza , anche nei primi periodi . 
la sordit e lincompleta perdita delludito stata registrata rispettivamente nell1 , 2% e nel 7 , 6% dei casi trattati prima del 1990 ; i valori corrispondenti per lultima decade di reclutamento sono stati rispettivamente 0 , 5% e 8% . 
queste differenze non raggiungono una significativit statistica . anche lincidenza assoluta della necrosi dei tessuti molli e delle mucose stata correttamente riportata nelle cartelle cliniche dei pazienti trattati pi indietro nel tempo , ed diminuita dal 2 , 5% all1 , 2% dopo il 1989 ( p = 0 , 1 ) ; lo stesso si pu dire per lincidenza assoluta della necrosi ossea che anchessa diminuita dall1 , 0% allo 0 , 7% ( p = non significativo [ ns ] )  . 
the diagnosis was confirmed with mri in all cases but one , with severe symptoms , treated in 1985 and having a diagnosis of brain radiation damage exclusively based on clinical findings . 
this obviously does not exclude the presence of subclinical hypothyroidism , as an active search for subclinical endocrine damage was not systematically done . incidence of the effects in the different clinicaltherapeutic subgroups most complications were more frequent in patients treated with electrons only on the neck compared with those treated with the ho - like technique , especially when a very - highenergy photon boost was used ( table 1 )  . 
a fractional dose > 2 gy ( but always 2.3 gy ) was used in the majority of patients treated before 1990 ( 56% , as opposed to 39% after 1990 )  . 
a higher fractional dose was linked with an increased incidence of all side effects analysed : severe cutaneous and subcutane10 , 5% nei pazienti trattati dal 1977 al 1989 al 6 , 4% in quelli trattati pi di recente ( p = 0 , 03 )  . 
la diagnosi stata confermata con mri in tutti i casi eccetto uno soltanto , con sintomi gravi , trattato nel 1985 e con una diagnosi di danno encefalico post - radioterapico basata esclusivamente su sintomi clinici . 
 al contrario , lincidenza di un danno asintomatico allencefalo aumentata con il tempo ( 3 / 477 , 0 , 6% vs 6 / 406 , 1 , 4% ; p = ns ) , ma questo conseguenza principalmente delluso sistematico della mri per la stadiazione e il follow - up nellultimo periodo . 
questo ovviamente non esclude la presenza di ipotiroidismo subclinico , dato che non stata realizzata sistematicamente una ricerca del danno endocrino subclinico . incidenza degli effetti tardivi nei differenti sottogruppi clinico - terapeutici la maggior parte delle complicanze sono pi frequenti nei pazienti trattati sulle aree linfonodali del collo solo con fasci di elettroni rispetto a quelli trattati con tecnica holike , specialmente quando stato usato un boost di fotoni di energia molto elevata ( tabella 1 )  . 
stato inoltre registrato un aumento non significativo dellincidenza di necrosi ossea e sordit con laumentare delle dosi ( 0 , 7% , 0 , 9% e 1 , 1% e 0% , 1 , 1% e 1 , 1% nei gruppi di dose 65 , 6670 e > 70 gy rispettivamente )  . 
lincidenza del danno allencefalo aumentata significativamente con la dose ( 0 , 2% , 0 , 7% , 0 , 7% negli stessi gruppi di dose , p = 0 , 04 )  . 
stata utilizzata una dose / frazione > 2 gy ( ma sempre 2 , 3 gy ) nella maggior parte dei pazienti trattati prima del 1990 ( 56% , a differenza del 39% di quelli trattati dopo tale anno )  . 
luso della chemioterapia non ha modificato in modo significativo lincidenza delle differenti complicanze e dei sottogruppi terapeutici ( dati non riportati )  . il trisma e la fibrosi cutanea - sottocutanea grave diminuiscono con let . 
no relevant differences in the incidence of late effects according to stage were documented . un aumento dellet e lincremento dellincidenza di ipoacusia ovviamente evidente , anche se non raggiunge una significativit statistica . 
tale effetto tardivo stato infatti registrato nel 5 , 5% , 8 , 5% , 8 , 5% dei pazienti con et < 40 , 5060 , > 60 anni , rispettivamente . 
analogamente , il danno allencefalo ( sia sintomatico che no ) era sempre pi frequente con laumentare dellet ( 0 , 5% , 2 , 4% e 1 , 7% negli stessi gruppi , p = 0 , 02 )  . 
non sono documentate differenze rilevanti nellincidenza di effetti tardivi del trattamento a seconda dello stadio . discussion discussione analysis of this series confirms that the problem of late effects of treatment is a relevant one for npc patients . 
to take advantage of the large number of patients studied , we attempted to analyse in detail the crude incidence of late damage in the different accrual periods and in the different clinical and therapeutic subgroups . 
 in line with results in the available literature , the crude incidence of many late effects of treatment ( xerostomia , hypoacousia and deafness , brain damage , trismus , bone and soft - tissue necrosis ) increases with the use of higher total doses [ 1 ]  . 
the only significant exception was xerostomia , which appears to have been underreported in earlier cases of our series , in which lower doses to the parotids were also administered . 
 a few other representative reports in the literature document a similar reduction in the incidence of the main late effects of treatment in more recently accrued patients [ 57 ]  . 
tuttavia nel comparare i dati relativi alle differenti popolazioni di pazienti sono emerse molte difficolt , poich spesso la severit delle complicanze stata riportata in modo diverso e poich non inusuale che non sia neanche stata riportata , almeno per quanto riguarda alcune complicanze ( per esempio xerostomia e lieve ipoacusia )  . 
noi , quindi , per trarre vantaggio dal grande numero di pazienti che abbiamo studiato , abbiamo cercato di analizzare in dettaglio lincidenza assoluta del danno tardivo nei vari periodi di reclutamento e nei diversi sottogruppi clinici e terapeutici . in linea con i risultati della letteratura disponibile , lincidenza assoluta di molti degli effetti tardivi del trattamento ( xerostomia , ipoacusia e sordit , danno encefalico , trisma , necrosi ossea e dei tessuti molli ) aumenta in relazione allimpiego di dosi totali pi elevate [ 1 ]  . 
lunica significativa eccezione la xerostomia , che sembra essere meno riportata nei casi pi recenti della nostra serie , spesso anche perch le parotidi hanno ricevuto dosi pi basse . pochi altri lavori in letteratura documentano una simile riduzione nellincidenza dei principali effetti del trattamento nei pazienti reclutati pi recentemente [ 57 ]  . 
 [ 7 ] and including 378 cases treated from 1954 to 1992 with mainly bidimensional techniques , the incidence of severe late complications according to the accrual period decreased from 14% for patients treated from 1954 to 1971 to 10% for those treated from 1972 to 1982 to 5% for those treated from 1983 to 1992 . 
the same observation was made by perez et al . , who analysed the series of patients with npc treated at the washington university from 1956 through 1991 [ 1 , 8 ]  . it should be considered , however , that supportive care for head and neck cancer patients treated with radiotherapy gradually improved over time , thus contributing to better results in terms of reduced toxicity . 
moreover , increasing awareness of the risk of late damage prompted physicians and patients to be more compliant in prescribing and adopting preventive measures such as , for example , better dental hygiene and the use of fluorinated compounds to limit the impact of late effects of treatment on physical well - being [ 1 , 8 ]  . 
the larger part of the published literature favours the use of imrt to reduce late effects of treatment ( mainly xerostomia and xerostomia - related effects ) [ 1014 ]  . 
however , the related costs are high and in some countries may even exceed what is considered fair use of public resources designated to the health systefor example , in a very recent turkish study , health - related issues linked with radiation - induced xerostomia in a large cohort of npc patients were thoroughly analysed [ 15 ]  . 
the authors demonstrated an increase with time of xerostomia - related symptoms and argue that imrt could help solve the problem ; however , they also noted that the use of these expensive sophisticated techniques in radiotherapy will increase the expenses for cancer treatment and eventually increase the financial difficulties of individuals in developing countries such as turkey and , consequently , might adversely affect qol . 
for example , in a very recent contribution from the university of michigan , a mente con tecniche bidimensionali , lincidenza di complicanze in base al periodo di reclutamento si riduce dal 14% ( per i pazienti trattati dal 1954 al 1971 ) al 10% ( per quelli trattati dal 1972 al 1982 ) al 5% ( per quelli trattati dal 1983 al 1992 ) ; gli autori sottolineano anche lesistenza di una relazione tra le vecchie tecniche e un aumento dellincidenza delle complicanze . 
 [ 7 ] hanno fatto la stessa osservazione , analizzando la serie di pazienti con npc trattati alla washington university dal 1956 al 1991 [ 1 , 8 ]  . si dovrebbe considerare , in ogni caso , che anche la terapia di supporto per i pazienti affetti da tumori del distretto cervico - cefalico trattati con radioterapia con il tempo gradualmente , migliorata , contribuendo cos ad ottenere migliori risultati in termini di ridotta tossicit . 
inoltre , unaumentata attenzione al rischio per il danno tardivo ha spinto medici e i pazienti ad una maggiore attenzione nel prescrivere e adottare misure preventive , come , per esempio , una miglior igiene dentale e luso di composti a base di fluoro , per limitare limpatto degli effetti tardivi del trattamento sul benessere soggettivo [ 1 , 8 ]  . gli studi che abbiamo citato , cos come il presente , fanno riferimento a pazienti trattati prevalentemente con tecniche bidimensionali . 
le tecniche tridimensionali hanno migliorato significativamente sia il risparmio delle parotidi che la qualit di vita dei pazienti con npc , secondo uno studio randomizzato svolto ad hong kong [ 9 ]  . 
la maggior parte dei lavori pubblicati suggerisce luso dellimrt per ridurre gli effetti tardivi del trattamento ( soprattutto la xerostomia e gli effetti xerostomia - correlati ) [ 1014 ]  . 
ad esempio , in un recente studio turco , sono state accuratamente analizzate le questioni relative alla xerostomia indotta dalla radioterapia , in una larga coorte di pazienti con npc [ 15 ]  . 
gli autori hanno dimostrato un aumento dei sintomi correlati alla xerostomia e hanno sostenuto che limrt potrebbe essere utile nel risolvere il problema ; ma hanno anche sottolineato che : con limpiego di queste tecniche sofisticate in radioterapia aumenteranno le spese per il trattamento del cancro e alla fine aumenteranno le difficolt economiche individuali in paesi in via di sviluppo come la turchia , con un conseguente impatto negativo sulla qualit di vita . 
per esempio , in un contributo recente delluniversit del michigan , una ridotta incidenza di osteonecrosi mandibolare stata spiegata dal ricorso ad una miglior cura radiol med ( 2012 ) 117 : 715724 decreased incidence of mandibular osteoradionecrosis was attained with better dental care and only in part with improved dose distributions obtained with imrt [ 16 ]  . 
finally , there are reports documenting improvement in quality - oflife indexes reported by radiotherapy - treated head and neck cancer patients 6 months after radiotherapy , even if xerostomia actually does not ameliorate , at the same time interval [ 17 ]  . 
this might , however , cast some doubts on the effective ability of imrt to improve the quality of life perceived by long - term survivors after npc treatment . e igiene dentale e solo in parte con il ricorso a migliori distribuzioni di dose ottenute con limrt [ 16 ]  . 
infine , esistono lavori che documentano un miglioramento negli indici della qualit di vita riportati da pazienti con tumori del distretto cervico - cefalico trattati con radioterapia , 6 mesi o pi dopo la radioterapia , anche se la xerostomia effettivamente non migliora nello stesso intervallo di tempo [ 17 ]  . 
questa osservazione pu rappresentare semplicemente le difficolt dei questionari utilizzati nel documentare il vero impatto della xerostomia sulla qualit di vita ; alcune incongruenze tra la gravit dei punteggi relativi ai sintomi con i punteggi relativi alla qualit di vita globale sono stati riportati anche da altri autori [ 15 ]  . 
questo potrebbe insinuare alcuni dubbi sulleffettiva capacit dellimrt di migliorare la qualit di vita a lungo termine , percepita dai pazienti che sopravvivono , dopo il trattamento , al npc . conclusions the use of older techniques and of higher total and fractional doses entails an increased risk of late complications in npc patients . 
this may be accomplished , at least in part , with the modern conformal techniques , such as 3d conformal radiotherapy ( crt ) , and particularly imrt , for npc patients . 
the majority of reports on this subject do , indeed , show that imrt techniques may reduce xerostomia and other late effects in patients treated for npc and other head and neck malignancies [ 1015 ]  . 
a moderate increase in fractional dose to the gross tumour volume ( gtv ) could then be accepted if the total dose is kept reasonably low ( 70 gy )  . 
this concept can be applied if the simultaneous boost ( sib ) imrt technique is adopted , as in flo and ira , to simultaneously treat the gtv and the nodal clinical target volume with different fractional doses [ 3 , 18 ]  . 
some experiences showing that sib techniques may be applied with modest toxicity to npc patients are , in fact , available [ 19 , 20 ] , and this technique is gaining a larger diffusion [ 21 ]  . 
therefore , for the time being , the only undisputable conclusion that can be drawn is that the era of bidimensional treatment of npc is over . conclusioni limpiego di vecchie tecniche e di dosi totali e dosi / frazione pi alte comporta un aumentato rischio di complicazioni tardive nei pazienti con npc . 
questo si pu ottenere , almeno parzialmente , con le moderne tecniche conformazionali come con la radioterapia tridimensionale conformazionale ( 3dcrt ) e in particolar modo con limrt per i pazienti con npc . 
la maggioranza dei lavori su questo argomento mostra infatti che le tecniche imrt possono ridurre la xerostomia e gli altri effetti tardivi nei pazienti trattati per npc e per altre neoplasie del distretto cervico - cefalico [ 1015 ]  . 
si pu poi accettare un aumento moderato della dose / frazione al volume macroscopico di malattia ( gtv ) , se la dose totale tenuta ragionevolmente bassa ( 70 gy )  . 
questo concetto pu essere applicato se si adotta la tecnica imrt con boost simultaneo ( simultaneous integrated boost , sib ) , come avviene attualmente a firenze e a brescia , per trattare allo stesso tempo il gtv e il clinical target volume ( ctv ) linfonodale con dosi / frazione diverse [ 3 , 18 ]  . 
sono disponibili alcune esperienze che mostrano che si pu applicare la tecnica sib con una modesta tossicit anche ai pazienti con npc [ 19 , 20 ] e questa tecnica sta guadagnando una sempre pi ampia diffusione [ 21 ]  . 
clavien grade 2 anaemia occurred in two patients ( 5.4 % ) : one patient required 1 u of packed red blood cells ; the other required an arterial embolisation . 
due cicli di congelamento , separati da un ciclo di riscaldamento passivo , con sonde da 1 , 7 e 2 , 4 mm , in anestesia generale o sedazione in base alla posizione e allo stato respiratorio del paziente . 
abbiamo riscontrato anemia di grado 2 secondo clavien in 2 casi ( 5 , 4% ) : un caso stato trattato con trasfusione di emazie concentrate , laltro con una embolizzazione arteriosa parziale del rene . 
la pca procedura relativamente facile e sicura e pu essere considerata una valida alternativa 594 radiol med ( 2012 ) 117 : 593605 keywords renal cell cancer percutaneous cryoablation nei pazienti che non sono candidabili o che rifiutano la chirurgia , anche in tumori di media grandezza . parole chiave carcinoma renale crioablazione percutanea introduction introduzione the detection of small renal masses ( srms ) with a diameter < 3 cm is increasing due to the increasing occurrence of renal cell cancer ( rcc ) and to the wide - spread use of abdominal ultrasound ( us ) and computed tomography ( ct ) scans . 
we know that about 2030% of srm could be benign , that the probability of containing malignant tissue is somewhat proportional to size and that up to 80% of renal cancers 3 cm are low - grade neoplasms [ 2 ]  . 
long - term follow - up studies of untreated renal masses are not available in large series , but interesting data from initial experiences with active surveillance protocols seem to show a low metastatic potential in the midterm [ 3 ]  . 
 all these aspects pose a dilemma regarding the best way to manage srablative therapies address patients for whom surgery is contraindicated and those harbouring risk factors for developing multiple renal tumours ( von hippel - lindau syndrome or hereditary papillary carcinoma syndrome ) [ 4 ]  . 
the published results of lca are encouraging , with a cancer - specific disease - free survival ( dfs ) at 3 years close to 100% [ 7 , 8 ]  . 
 the recent availability of insulated smaller cryogenic probes ( 1.72.4 mm ) enabled the use of imaging - guided percutaneous ca ( pca ) , which could permit further improvement in decreasing the invasiveness of renal ablation . 
preliminary results seem to indicate a therapeutic effectiveness of 80100% [ 912 ] , although the length of follow - up in these studies is not sufficient for a complete understanding of long - term local tumour control , particularly for low - grade neoplasms . 
the most important advantages to be expected , besides reduced invasiveness , are a shorter hospital stay and an excellent control of the lindividuazione di piccole masse renali , con diametro inferiore ai 3 cm , in aumento a causa della crescente incidenza del carcinoma renale ( rcc ) e delluso esteso della ecografia addominale e della tomografia computerizzata ( tc ) nella diagnostica per immagini . 
sappiamo che circa il 20%30% delle srm pu essere benigna , che la probabilit di contenere tessuto neoplastico maligno in qualche modo proporzionale alla dimensione della lesione stessa e che circa l80% delle masse renali con diametro3 cm sono tumori a basso grado di malignit [ 2 ]  . 
follow - up a lungo termine di masse renali non trattate sono disponibili solo in casistiche limitate , ma emergono dati interessanti da esperienze iniziali di protocolli di sorveglianza attiva i quali sembrano mostrare un basso potenziale metastatico di queste piccole lesioni nei controlli a medio termine [ 3 ]  . 
la diagnosi di srm riguarda spesso pazienti anziani o che sono affetti da importanti co - morbilit che possono controindicare un trattamento chirurgico . daltra parte sia i miglioramenti delle tecniche chirurgiche che lintroduzione di nuove fonti di energia utilizzate per lablazione dei tessuti sono stati in grado di abbassare in modo significativo la morbilit delle terapie . 
le terapie ablative sono proponibili a pazienti per i quali controindicato un intervento chirurgico cos come a quelli affetti da fattori di rischio per lo sviluppo di molteplici tumori renali ( sindrome di von hippel - lindau o sindrome del carcinoma papillare ereditario ) [ 4 ]  . 
le tecniche ablative pi diffuse inizialmente comprendevano lablazione percutanea imaging - guidata con radiofrequenza ( rfa ) [ 5 , 6 ] e la crioablazione laparoscopica ( lca )  . 
i risultati pubblicati sulla crioablazione laparoscopica sono incoraggianti , con una sopravvivenza cancro - specifica libera da malattia a 3 anni attorno al 100% [ 7 , 8 ]  . 
lanalisi di tutte le casistiche pubblicate ha dimostrato una sopravvivenza cancro - specifica libera da malattia a 5 anni del 97%100% per le lesioni fino a 3 cm [ 9 ]  . la recente disponibilit sul mercato di sonde criogeniche pi piccole ( 1 , 72 , 4 mm ) ha reso possibile la esecuzione della crioablazione per via percutanea ( pca ) sotto radiol med ( 2012 ) 117 : 593605 intraoperative procedure , which is possible due to ct or magnetic resonance imaging ( mri ) , which is close to real - time imaging of the ice ball . 
pca also seems to overcome the limits of the size of masses treatable with other ablative methods , such as radiofrequency , enabling tumours > 3 cm to be treated in patients considered unfit for surgery . we report our experience with ct - guided pca for small ( < 3 cm ) and medium - sized ( 37 cm ) renal masses to evaluate the safety and initial results of the procedure in patients who are not surgical candidates . materials and methods from october 2007 to november 2009 , 225 patients with renal cancer presented at our hospital . 
of these , we treated with pca a series of small to medium renal masses ( up to 7 cm diameter ) in 37 patients aged between 52 and 82 ( median 73 ) years who were not surgical candidates or who refused surgery . 
the ideal setting included patients who were unfit for standard surgical treatment due to elderly age , and significant comorbidities that included severe heart , vascular , respiratory or renal diseases ( n = 19 )  . 
 previous renal surgery , in particular , in the case of solitary kidney ( n = 7 ) , and coexisting neoplasms ( n = 8 ) were also conditions in favour of the nonsurgical approach . 
 depending on ct images , the percutaneous access window was determined , considering the possible effects on adjacent organs and the theoretical number , gauge and length of cryogenic probes to be used . 
i primi risultati sembrano indicare una efficacia terapeutica dell80%100% [ 912 ] , anche se la durata del follow - up in questi studi non sufficiente per una completa comprensione del controllo locale del tumore a lungo termine , in particolare per le neoplasie a basso grado di malignit . 
i vantaggi pi importanti attesi da questa metodica sono rappresentati , oltre che dalla riduzione di invasivit , da una degenza ospedaliera pi breve e dallottimo controllo intra - operatorio della procedura , reso possibile dalla visione della palla di ghiaccio seguita in tempo reale dalle immagini tc o dalla risonanza magnetica ( rm )  . 
la crioablazione percutanea sembra essere anche in grado di superare i limiti posti dalle dimensioni massime delle masse trattabili che si osservano con altre metodiche quali la radiofrequenza ; infatti possibile trattare tumori pi grandi di 3 cm in pazienti considerati non idonei per la chirurgia . riportiamo la nostra esperienza di crioablazione tcguidata per il trattamento di masse renali di piccole dimensioni ( < 3 cm ) e medie dimensioni ( 37 cm ) , al fine di valutare la sicurezza e i risultati preliminari di efficacia di tale procedura in pazienti non candidati a chirurgia . materiali e metodi nel periodo compreso tra ottobre 2007 e novembre 2009 sono giunti allosservazione presso il nostro ospedale 225 pazienti con tumore renale . 
di questi abbiamo trattato con crioablazione percutanea una serie di lesioni di piccole e medie dimensioni ( sino a 7 cm di diametro massimo ) in 37 pazienti , con et compresa tra 52 e 82 anni ( mediana 73 anni ) che non erano candidabili alla chirurgia o che hanno rifiutato lintervento . 
lindicazione ideale includeva quei pazienti che non erano eligibili per la terapia chirurgica standard a causa dellet avanzata o di significative co - morbilit che includevano patologie cardiache , vascolari o respiratorie di grado severo ( 19 pazienti )  . 
altre condizioni che hanno favorito un approccio terapeutico non chirurgico sono state una pregressa chirurgia renale , con particolare riguardo alla situazione di mono - rene chirurgico ( 7 pazienti ) , e la coesistenza di altre patologie neoplastiche ( 8 pazienti )  . 
in tutti i casi stato eseguito laccertamento bioptico delle lesioni mediante biopsia percutanea che stata eseguita immediatamente prima della procedura di pca ; la biopsia stata omessa in 7 casi in cui i pazienti avevano una precedente storia di tumore renale trattato con chirurgia . 
 treatment was considered technically successful when the ice ball exceeded the tumour margins by at least 5 mm in order to obtain a target temperature ( 20c to 40c ) in the entire tumour volume [ 13 ]  . 
 two freezing cycles of 1315 min each were applied to any single lesion , separated by a passive warming cycle of 1215 mduring the freezing cycle , temperatures at the tip of each probe decreased to 100c to 140c . 
the total duration of the procedure was about 1 h , to which the time required for preparation and administration of general anaesthesia ( when done ) was added . postoperative monitoring postoperative monitoring included haematological and biochemistry evaluation 4 , 8 , and 24 h after pca , and ct examination without contrast medium 24 h after pca . 
perioperative complications occurring within 30 days after ca procedures were recorded and graded according to the latest modification of the clavien criteria [ 14 ]  . follow - up patients were imaged using a multislice spiral ct scanner ( somatom sensation 16 , siemens medical solutions ) with intravenously administered contrast agent 1 , 3 , 6 , 9 and 12 months after treatment and subsequently every 6 months for 3 years . 
radiological evaluation of response was based on mass enhancement at ct scans : complete lack of enhancement of a previously enhancing mass was considered adequate response . tecnica tutti i pazienti sono stati sottoposti ad una valutazione radiologica con tc multistrato prima della terapia ablativa , utilizzata sia per la stadiazione oncologica , sia per la pianificazione della procedura di pca . 
sulla base delle immagini tc stata scelta la via di approccio percutaneo , considerando i possibili effetti sugli organi adiacenti , ed il teorico numero , dimensione e lunghezza delle sonde criogeniche da utilizzare . 
i pazienti sono stati trattati in regime di anestesia generale o di blanda sedazione , scelte in base al decubito del paziente necessario per la pca ed alla funzionalit respiratoria . 
in tutti i casi , dopo la centratura tc eseguita con scansioni in condizioni di base , senza mezzo di contrasto ( mdc ) , il campo operatorio stato allestito secondo una tecnica sterile standard ; le sonde sono state posizionate sotto controllo diretto tc ; il posizionamento delle sonde stato stabilito in base alle caratteristiche geometriche del tumore ed alla dimensione prevista della palla di ghiaccio . 
dopo il posizionamento di ciascuna sonda stata effettuata una scansione tc standard ( 2 , 55 , 0 mm di spessore di strato , 120 kv e 240 ma ) per valutare la corretta posizione . 
il trattamento stato ritenuto tecnicamente efficace quando il volume della palla di ghiaccio formata superava i margini della lesione di almeno 5 mm , in modo da ottenere una temperatura efficace ( 20c / 40c ) in tutto il volume della lesione [ 13 ]  . tutti i trattamenti sono stati condotti con un apparecchiatura per criochirurgia con funzionamento basato sullespansione del gas argon prodotta dalla endocare ( irvine , ca ) , utilizzando sonde criogeniche percutanee dedicate , con diametri di 1 , 7 e 2 , 4 mm ; le sonde sono disponibili in differenti lunghezze e sono caratterizzate da una impugnatura ad angolo retto , in modo da permettere una adeguata manovrabilit alla tc . 
la durata totale della procedura di circa unora , alla quale bisogna aggiungere il tempo di preparazione e conduzione della anestesia generale , quando questa viene utilizzata . radiol med ( 2012 ) 117 : 593605 results between october 2007 and november 2009 , 37 patients ( 38 renal masses ) underwent a total of 40 pca procedures . 
briefly , median tumour size was 35 ( range 1270 ) mm ; 19 / 37 ( 51.3% ) patients had an american society of anesthesiologists ( asa ) score 3 . 
of the seven patients with solitary kidney , table 1 tumour characteristics ( n = 38 ) characteristics patients , n lesions , n gender , n male female median age ( years ) asa score 2 3 median size of lesion , mm side right left status of contralateral kidney , n normal absent due to rcc due to stone disease number of lesions per patient single two ( bilateral ) site of disease , n central not central intraparenchymal exophytic location of tumour in kidney , n middle posterior lateral biopsy , n no yes rcc oncocytoma nondiagnostic value 73 ( 5282 ) 35 ( 1270 ) 4 asa , american society of anesthesiologists ; rcc , renal cell carcinoma aone patient underwent a contextual cryoablation of a bone ( iliac ) metastasis ; brecurrences of previously ascertained rcc monitoraggio post - procedura il monitoraggio post - intervento prevede lesecuzione di esami ematologici e biochimici 4 , 8 e 24 ore dopo la pca e lesecuzione di un esame tc senza mdc a 24 ore dallintervento . 
le complicanze peri - operatorie accadute entro 30 giorni dalla procedura di crioablazione sono state registrate e classificate secondo lultima versione dei criteri di clavien [ 14 ]  . follow - up i pazienti sono stati valutati utilizzando una tc spirale multistrato ( somatom sensation 16 , siemens medical solutions , germania ) con controlli a 1 , 3 , 6 , 9 e 12 mesi dopo il trattamento e successivamente ogni sei mesi per tre anni . 
 tutti gli esami , prima e dopo il trattamento , sono stati condotti col medesimo protocollo di studio , con scansioni senza e con somministrazione di 120140 ml di mezzo di contrasto endovenoso ( iopamiro 370 , bracco , italia ) , iniettati alla velocit di 3 ml al secondo con acquisizioni in fase arteriosa ( 45 secondi ) , in fase nefrografica ( 90 secondi ) ed in fase escretoria ( 300 secondi ) utilizzando scansioni con spessore di strato ed intervallo di ricostruzione di 2 , 53 mm , 120 kv , 200350 ma , e tempo di rotazione di 0 , 5 secondi . 
la valutazione radiologica della risposta al trattamento stata basata sulla captazione contrastografica valutata nelle indagini tc : la completa mancanza di captazione di mezzo di contrasto in lesioni che ne erano dotate prima del trattamento stata considerata una risposta adeguata . risultati tra ottobre 2007 e novembre 2009 , sono stati trattati con crioablazione percutanea 37 pazienti ( 38 masse renali ) per un totale di 40 procedure . 
in breve , la dimensione mediana dei tumori renali trattati stata di 35 mm ( range 1270 mm ) ; 19 / 37 ( 51 , 3% ) pazienti sono stati classificati american society of anesthesiologists ( asa ) score3 . 
sette pazienti avevano una precedente diagnosi istologicamente documentata di rcc e pertanto non sono stati sottoposti a biopsia , mentre 30 pazienti sono stati sottoposti a biopsia immediatamente prima del trattamento ablativo , nella stessa seduta . 
two had recurrences following previous nephron - sparing surgery , which could only be treated with radical nephrectomy ( 52 and 74 years old , respectively ) , which is why we chose to perform pca in an attempt to preserve the kidney and renal function . patients underwent pca after providing full informed consent . 
i rimanenti 22 pazienti sono stati trattati in posizione supina e si utilizzata sedazione con midazolam associata ad analgesici , mentre un anestetico locale stato infiltrato nel sito di inserzione cutanea delle sonde criogeniche . 
non si sono osservate complicanze immediate ( intraoperatorie )  . tutti i pazienti hanno riferito comparsa di dolore lieve , controllato con analgesici minori , solo nel giorno della procedura . 
la tc di controllo effettuata dopo 24 ore ha rivelato un ematoma perirenale in 6 / 37 ( 16 , 2% ) pazienti e in due di questi ( 5 , 4% ) si osservata una significativa anemizzazione . 
 uno di questi pazienti ha ricevuto una trasfusione di 250 ml di emazie concentrate dopo 4 ore dal trattamento a causa di una anemizzazione sintomatica ( emoglobina da 11 , 3 a 7 , 5 g / 100 ml )  . 
laltro paziente stato trattato con embolizzazione trans - arteriosa con micro - particelle ( bad block 500700 micron , biocompatibles ) di un piccolo ramo arterioso intrarenale , sede di un lento ma persistente sanguinamento ( emoglobina da 11 , 7 a 8 g / 100 ml )  . 
la figura 2 mostra la nostra casistica , considerando le dimensioni della zona sottoposta ad ablazione ed i relativi valori di densitometria misurati alla tc ad ogni controllo programmato . in due casi si osservata captazione di mezzo di contrasto , rispettivamente dopo 1 e 9 mesi dalla crioablazione . 
il secondo paziente era un uomo con carcinoma renale bilaterale precedentemente trattato con nefrectomia radicale destra e resezione parziale a sinistra , con una recidiva a carico del rene residuo ( 28 mm ) che stata trattata con crioablazione . 
 according to the clavien system classification , we recorded 3 / 37 ( 8.1% ) grade i , 1 / 37 ( 2.7% ) grade ii and 1 / 37 ( 2.7% ) grade iii complications . 
the other patient was treated with transarterial embolisation with microparticles ( bad block 500700 m , biocompatibles ) of a small intrarenal arterial branch that had slow but persistent bleeding ( haemoglobin from 11.7 to 8 g / 100 ml )  . 
 in tutti gli altri casi il controllo tc dopo 3 mesi dalla pca ha mostrato ipodensit della massa trattata , senza alcuna captazione di mezzo di contrasto ( densit di 1540 hu , media 32 )  . 
a 3 mesi le dimensioni delle aree trattate risultano un po maggiori rispetto a quelle dei tumori prima del trattamento ( diametro 2075 mm , media 42 mm )  . 
tutti i pazienti sono vivi e liberi da malattia ad un follow - up mediano di 24 mesi ( range 1236 )  . discussione la resezione chirurgica rappresenta il gold standard per il trattamento di piccoli espansi renali . 
la pianificazione della chirurgia richiede la valutazione di co - morbilit , dei rischi operatori , dellaspettativa di vita e della rilevanza clinica 600 radiol med ( 2012 ) 117 : 593605 density diameter fig . 
the second patient was a man with bilateral rcc previously treated with a right nephrectomy and left partial nephrectomy with recurrence in the left kidney ( 28 mm ) , which was treated with pca . 
both patients showed no evidence of tumour recurrence at the latest follow - up after 24 months . in all other cases , ct examination 3 months after pca showed a hypodense mass without contrast enhancement ( density 1540 hu , mean 32 )  . 
all patients were alive and disease free at a median follow - up of 24 ( range 1236 ) months . discussion surgical excision is the gold standard for treating sr surgical planning requires evaluation of comorbidities , surgical risks , life expectancy and clinical relevance of the disease . 
some patients with a renal mass are not ideal candidates for surgery , although many need a less invasive therapeutic approach , which is currently made possible thanks to the evolution of thermal ablation techdella malattia . 
alcuni pazienti con una massa renale non sono candidati ideali per la chirurgia , in particolare molti di loro necessitano di un approccio terapeutico meno invasivo , che attualmente reso possibile grazie allevoluzione delle tecniche termoablative . 
tra queste procedure ablative , sulla base dei dati sperimentali e clinici disponibili [ 15 , 16 ] , abbiamo utilizzato la crioablazione ( ca ) , piuttosto che la rfa . 
una valutazione delle percentuali di complicazioni confrontando i trattamenti termoablativi con lintervento di nefrectomia laparoscopica parziale ( lap - pn ) stata proposta da weld e landman nel 2005 [ 17 ]  . 
in una recente analisi [ 18 ] stata valutata la morbilit peri - operatoria della lca in uno studio multicentrico europeo che ha coinvolto 144 pazienti e 148 procedure : eventi sfavorevoli si sono verifi cati nel 17% con una percentuale di complicanze del 15 , 5% secondo il sistema clavien ( solo il 4% di grado 3 )  . 
il sesso femminile , le dimensioni del tumore e la presenza di patologie cardiache sono risultati predittivi di eventi sfavorevoli ; in particolare ogni incremento di 1 cm delle dimensioni della neoplasia aumenta di tre volte il rischio di complicanze peri - operatorie . 
a recent analysis [ 18 ] evaluated perioperative morbidity of lca in a european multicentre study involving 144 patients and 148 procedures : unfavourable events occurred in 17% , with a complication rate of 15.5% according to the clavien system ( only 4% of grade iii )  . 
nei pazienti trattati con pca , il tasso di complicanze stata inferiore ( 22 , 2% vs 40% ) e la degenza ospedaliera stato pi breve ( 1 , 3 versus 3 , 1 giorni ; p < 0 , 0001 ) rispetto ai pazienti sottoposti a lca . 
indipendentemente da questi dati , lca e pca non devono essere considerate procedure intercambiabili , dato che ogni approccio richiede una precisa indicazione che diventa ottimale in pazienti adeguatamente selezionati . 
nella nostra esperienza , abbiamo avuto 2 ( 6% ) complicazioni di grado 23 secondo la classificazione del sistema clavien , il che in linea con latteso , accettabile e modesto tasso di morbilit di questa procedura . 
entrambi i pazienti con complicanze di grado 2 o 3 avevano lesioni con diametro maggiore di 3 cm . laltro importante aspetto riguarda lefficacia delle ter602 radiol med ( 2012 ) 117 : 593605 importantly , female gender , tumour size and cardiac conditions were predictive of unfavourable events . 
regardless of these data , lca and pca must not be considered interchangeable procedures , as each approach requires a specific setting , which becomes optimal only in adequately selected patients . 
in our experience , we had two ( 6% ) grade iiiii complications according to the clavien system classification , which is in line with the expected , acceptable and low morbidity of this procedure . 
a meta - analysis on srm management [ 16 ] found that the local recurrence rate is 7.5 - fold and 18.2 - fold higher following ca and rfa , respectively , when compared with conservative surgery . 
different numbers , followup periods , patient age and disease size could contribute to such intriguing results . long - term follow - up data regarding ca are available from the cleveland clinic [ 22 ] , where as many as 60 patients reached a minimum follow - up of 5 years following cryosurgery . 
among the 55 patients with proven rcc ( median follow - up 93 months ; range 60132 ) , the 5 - year overall disease - specific ( dss ) and dfs rates were 84% , 92% and 81% , and the 10 - year rates were 51% , 83% and 78% , respectively . 
weld e landman [ 17 ] , valutando 326 casi di ca e 277 di rf , hanno evidenziato che i tassi di persistenza / recidiva di malattia erano di 4 , 6% e 7 , 9% rispettivamente con un follow - up mediano di 10 e 30 mesi . 
secondo i recenti dati della letteratura , le percentuali di recidiva del tumore variano da 1 , 7% a 13% dopo un follow - up da 10 a 83 mesi [ 21 ]  . 
una metaanalisi sul trattamento delle piccole masse renali [ 16 ] ha rilevato che il tasso di recidiva locale maggiore di 7 , 5 volte e 18 , 2 volte rispettivamente dopo ca e rfa , quando confrontate con la chirurgia conservativa . 
 dati di follow - up a lungo termine riguardanti la ca sono disponibili presso la cleveland clinic [ 22 ] , dove ben 60 pazienti hanno raggiunto un follow - up minimo di 5 anni dopo criochirurgia . 
tra i 55 pazienti con carcinoma a cellule renali istologicamente accertato ( follow - up mediano : 93 mesi , range da 60 a 132 mesi ) , le percentuali di sopravvivenza globale a 5 anni , sopravvivenza cancro - specifica e sopravvivenza libera da malattia erano di 84% , 92% e 81% , mentre a 10 anni la percentuali erano 51% , 83% e 78% rispettivamente . 
ad analisi multivariata , solamente una precedente nefrectomia radicale ( per carcinoma renale ) risultava predittiva della sopravvivenza libera da malattia e di quella cancro - specifica ( rispettivamente , p = 0 , 023 e p = 0 , 030 )  . due aspetti importanti correlati allefficacia del trattamento riguardano lindicazione ideale alla ca e come seguire nel follow - up i pazienti trattati . 
la ca stata inizialmente proposta per gli espansi solidi renali fino a 4 c nella maggior parte delle casistiche il diametro medio delle lesioni ablate < 3 cpermpongkosol et al . 
 [ 23 ] hanno riportato i risultati di 23 espansi renali trattati con ca , di dimensioni variabili da meno di 2 cm a 5 cessi hanno evidenziato che i parametri di rischio di recidiva erano le dimensioni ( 3 / 6 recidive con diametro superiore a 3 centimetri vs 3 / 17 con diametro inferiore a 3 cm ) e la sede ( 3 / 6 recidive con tumore centrale vs 1 / 17 con tumore periferico )  . 
 la nostra casistica si differenzia in quanto la met dei nostri pazienti aveva un espanso superiore ai 3 centrambi i pazienti con recidiva di malattia presentavano un tumore iniziale 3 cm di diametro : questo fatto ci porta a ritenere che i nostri insuccessi possono non essere correlati alle dimensioni dei tumori , ma ad errori tecnici , probabilmente legati alla fase iniziale della nostra curva di apprendimenradiol med ( 2012 ) 117 : 593605 indications for ca and how to follow - up treated patients . 
our series is different in that as many as half of our patients had a mass > 3 c both patients with recurrence had an initial tumour 3 cm in diameter : this fact leads us to believe that our failures may not be due to tumour size but to technical errors , probably related to the initial phase of our learning curve . 
lesion density dropped from a mean of 100 hu to a mean of 32 hu after the first follow - up scan at 3 months and tended to remain stable thereafter . 
 experience from the cleveland clinic regarding 176 patients revealed that biopsy showed no evidence of disease among 60 patients with no ct contrast enhancement in residual masses following ca , whereas biopsy was positive in 6 / 37 masses with contrast - medium uptake [ 25 ]  . 
because of the low specificity of biopsy and the long - term evolution of these ablation treatments , experienced authors from cleveland suggest continuation of follow - up with contrastenhanced imaging rather than an early biopsy . 
nonetheless , a more difficult interpretation of enhancement on mri scans and the observation that peripheral - rim enhancement could be a frequent finding in early scans render mri still prone to an excess of subjective interpretations [ 26 , 27 ]  . 
attualmente , la riduzione dimensionale e lassenza di captazione di mezzo contrasto della lesione residua nelle indagini tc eseguite nel follow - up sono generalmente accettate come validi surrogati di remissione completa . 
la densit delle lesioni si ridotta passando da una media di 100 hu ad una media di 32 hu dopo il primo controllo a 3 mesi , mantenendosi poi pressoch stabile nelle indagini tc successive . non abbiamo usato la biopsia per valutare la persistenza di malattia . 
lesperienza presso la cleveland clinic su 176 pazienti ha rivelato che la biopsia non ha mostrato evidenza di malattia tra i 60 pazienti sottoposti a ca con assenza di captazione di contrasto nelle lesioni residue allindagini tc di follow - up , mentre la biopsia stato positiva in 6 delle 37 lesioni che captavano mezzo di contrasto [ 25 ]  . 
a causa della bassa specificit della biopsia e dellevoluzione a lungo termine di questi trattamenti ablativi , gli autori con importante esperienza in tali procedure presso la cleveland clinic suggeriscono che meglio effettuare un continuo follow - up mediante indagini radiologiche con mdc piuttosto che precoci campionamenti bioptici sulle lesioni trattate . 
tuttavia una pi difficile interpretazione della captazione di contrasto allindagine di rm e losservazione che un cercine ipervascolare periferico potrebbe essere un frequente riscontro nelle immagini di rm nel precoce follow - up , rendono tale metodica pi incline ad eccessi di interpretazioni soggettive [ 26 , 27 ]  . la versatilit uno dei vantaggi principali della pca . 
 [ 15 ] hanno pubblicato una casistica di 16 lesioni ricadute nel follow - up dopo ca , 10 delle quali furono ri - trattate sempre con termo - ablazione . 
nella nostra serie entrambi i casi di recidiva di malattia nel follow - up dopo pca sono stati ri - trattati con successo sempre con pca e sono rimasti senza evidenza di progressione di malattia dopo 2 anni . 
 abbiamo anche un paziente che stato sottoposto ad ablazione del tumore primario e di una metastasi ossea nella stessa seduta . questa serie di pazienti trattati con pca dimostra che la pca sembra essere una procedura sicura con una morbilit accettabile in una serie di pazienti selezionati in cui circa 604 radiol med ( 2012 ) 117 : 593605 could successfully undergo same - session ablation of the primary tumour and a metastatic bone site . 
 this series of patients demonstrates that pca could be a safe procedure with an acceptable morbidity rate in selected patients where about half had an asa score 3 or a mass exceeding 3 calthough the length of follow - up is relatively short , the finding of high local control rates is encouraging and supportive for using pca as an effective alternative for patients who are not surgical candidates or who refuse surgery . 
moreover pca was planned for highly selected patients who were unfit for surgery and had masses that are particularly suitable for a percutaneous posterior approach due to size and site . 
 we believe that best - management evaluation should consider disease - related information ( size and site ) , patientrelated characteristics ( general health status , age , life expectancy ) and efficacy of treatment options ( noninvasive , minimally invasive , invasive )  . 
 la met aveva uno score asa3 o un espanso superiore ai 3 csebbene il periodo di follow - up sia relativamente breve , il dato di una elevata percentuale di controllo locale di malattia incoraggiante e di stimolo per lutilizzo della pca come efficace alternativa per i pazienti che non sono candidati alla chirurgia o che rifiutano lintervento chirurgico . 
la pca ha inoltre dimostrato di essere una soluzione versatile , in grado di permettere trattamenti multipli e ripetuti , che possono includere favorevoli sedi extra - renali di malattia . le limitazioni della nostra serie sono molteplici e intrinseche allo studio . 
inoltre la pca stata pianificata per pazienti altamente selezionati , non candidabili alla chirurgia ed aventi espansi che erano particolarmente favorevoli per dimensioni e sede ad un approccio percutaneo posteriore . 
 al momento noi pensiamo che una valutazione per la migliore pianificazione del trattamento dovrebbe prevedere informazioni relative alla malattia ( dimensione e sede ) , alle caratteristiche del paziente ( stato di salute generale , et ed aspettativa di vita ) e alla efficacia delle differenti procedure terapeutiche ( opzioni non - invasive , mini - invasive ed invasive )  . 
 special attention is paid to correlating age and pathology by subdividing the population into four categories : girls up to prepubertal age , pubertal girls , women of reproductive age and postmenopausal women . 
us is the first - line imaging modality in children and women with pelvic pain , and computed tomography ( ct ) is usually requested , especially in emergency settings , in patients in whom us is inadequate for diagnosis . 
however , mri should be considered at least in urgent , if not in emergent , care given the wide range of female pelvic disorders that can be correctly assessed thanks to the excellent soft - tissue contrast , high spatial resolution and ability to depict blood products . 
 keywords magnetic resonance imaging female imaging pelvic pain riassunto questo articolo illustra le cause del dolore pelvico di natura ginecologica che possono non essere correttamente individuate o che sono dubbie allecografia e che appaiono meglio identificabili con risonanza magnetica ( rm )  . 
verr , inoltre , prestata una particolare attenzione nel correlare et e patologia suddividendo la popolazione femminile in 4 categorie : neonate e bambine fino allet pre - pubere , ragazze al menarca , donne in et fertile e donne in menopausa . 
tuttavia , quando lecografia non sia risolutiva bisognerebbe prendere in considerazione la rm , se non in emergenza almeno nei casi di urgenza differibile , in quanto essa in grado di identificare un ampio spettro di patologie responsabili del dolore pelvico di natura ginecologica grazie alla sua eccellente risoluzione spaziale e di contrasto e alla capacit di identificare i prodotti di degradazione della emoglobina . 
non bisogna inoltre dimenticare che la rm dovrebbe essere preferita nei bambini e nelle donne in et riproduttiva a causa dellassenza di radiazioni ionizzanti . parole chiave risonanza magnetica imaging della donna dolore pelvico 576 introduction ultrasound ( us ) is the primary modality for evaluating lower quadrant pain in young girls and women [ 1 ]  . 
magnetic resonance imaging ( mri ) is a reliable modality for evaluating the pelvic region because of its excellent soft - tissue contrast , high spatial resolution and ability to demonstrate blood products [ 4 ]  . 
despite its relatively high cost , lengthy examination time and reduced availability , which limit its routine use , mri is a reliable complement to us in patients with suspected gynaecological disorders , as the range of conditions correctly assessed is extremely broad . 
 moreover , mri could be a crucial diagnostic tool in virgins if transabdominal us is unable to provide a diagnosis and transvaginal us is denied . specific painful gynaecological disorders inadequately diagnosed by us but more adequately assessed by mri are analysed in this article . 
this review correlates age and pathology by subdividing females into the following categories : from childhood to prepubertal age , pubertal - age girls , reproductive age and postmenopausal age . 
the reported frequency of appendicitis in symptomatic young patients is 41% [ 6 ] , whereas vesicoureteral reflux shows an incidence of 2540% in children with urinary tract infection [ 7 ]  . 
 pelvic pain related to female genital alterations is very rare in children [ 810 ] and is usually related to torsion of an ovarian cyst , hydrocolpos or hydrometrocolpos , and to torsion of the fallopian tube and ovary . 
the isolated torsion of the ovary and the fallopian tube rarely develop before menarche [ 11 ] but can occur in children with excessive mobility of the adnexa , even without ovarian abnormalities [ 12 ]  . 
b - mode us is usually employed as a first diagnostic step in symptomatic children [ 1 ] , and in the case of torsion , an anechoic adnexal mass with corpuscular content is easily documented on sonograms . 
a corpuscular content characterised by a fluid - debris level has been described as radiol med ( 2012 ) 117 : 575592 introduzione lecografia rappresenta la modalit di prima istanza nella valutazione delle giovani donne con dolore pelvico [ 1 ]  . 
ciononostante , sia lecografia trans - addominale ( ta ) che quella trans - vaginale ( tv ) possono talvolta essere non conclusive ai fini diagnostici , anche se combinate con lo studio color doppler [ 2 ]  . 
la risonanza magnetica ( rm ) una modalit efficace nella valutazione della regione pelvica femminile per la sua eccellente risoluzione di contrasto , per lelevata risoluzione spaziale e per la capacit di identificare prodotti di derivazione ematica [ 4 ]  . 
nonostante i costi elevati , la lunga durata dellesame e la ridotta disponibilit ne limitino luso nella routine clinica , la rm rappresenta la metodica ottimale e complementare allecografia nella valutazione delle pazienti con sospetta patologia ginecologica , per lampio range di patologie che pu correttamente identificare . 
verr correlata let con la patologia della paziente , suddividendo la popolazione femminile in 4 classi : bambine dallinfanzia fino allet pre - pubere , giovani donne alla pubert , donne nellet riproduttiva ed in post - menopausa . 
verranno evidenziati gli elementi di semeiotica rm e quelli utili per la diagnostica differenziale . bambine fino allet pre - pubere nelle bambine le patologie pelviche che si associano a dolore sono pi spesso associate a disordini del tratto gastrointestinale o ad anomalie del tratto urinario [ 5 ]  . 
in giovani pazienti sintomatiche la frequenza riportata per lappendicite del 41% [ 6 ] mentre il reflusso vescico - ureterale presenta unincidenza del 25%40% in bambine con infezioni del tratto urinario [ 7 ]  . 
 il dolore pelvico correlato ad alterazioni dellapparato genitale femminile estremamente raro [ 810 ] ed usualmente associato a torsione di cisti ovarica , ad idrocolpo o idrometrocolpo , a torsione ovarica e della tuba di falloppio . 
la torsione isolata dellovaio e della tuba raramente si sviluppano prima del menarca [ 11 ] , ma possono presentarsi in bambine per iper - mobilit dellannesso anche in assenza di patologia ovarica [ 12 ]  . 
when this sign is detected within the cyst , it is usually considered as a pathognomonic sonographic feature of torsion [ 13 , 14 ] and does not require further investigation . 
however , when a pelvic mass shows uniform echogenic corpuscular content , us might not be able to characterize it adequately , as different pathological conditions can exhibit similar findings , such as hydrocolpos or hydrometrocolpos , and additional imaging modalities are needed to correctly assess the disease . hydrocolpos and hydrometrocolpos the incidence of hydrocolpos and hydrometrocolpos is 1 : 30 , 000 births [ 9 , 10 ]  . 
extreme dilation of the vagina and / or the uterine cavity can be related to vaginal abnormalities , such as imperforate hymen , vaginal membrane or atresia , or common urogenital sinus complicated by a vaginal stenosis [ 15 ]  . 
when using mri to identify a common urogenital sinus complicated by vaginal stenosis , bladder voiding is not required in order to demonstrate the common origin of urethra and vagina . 
il contenuto fluido / corpuscolato caratterizzato dallaccumulo di materiale ecogeno in sede declive con formazione di un livello deposito / fluido stato descritto come precoce segno di torsione [ 13 ]  . 
quando invece una massa pelvica presenta un contenuto ecogeno uniforme , lecografia pu non essere in grado di caratterizzarla adeguatamente dal momento che differenti condizioni patologiche , come idrocolpo o idrometrocolpo , si presentano con aspetti simili ed ulteriori indagini di imaging sono pertanto richieste per determinarne correttamente la causa . 
la dilatazione marcata della vagina e / o della cavit uterina pu essere associata ad anomalie della vagina , come imene imperforato , presenza di membrana vaginale , atresia della vagina o presenza di seno uro - genitale comune complicato da stenosi vaginale [ 15 ]  . 
lostruzione congenita della vagina distale generalmente asintomatica fino al menarca [ 16 ] , ma pu divenire sintomatica in relazione allaccumulo di una elevata quantit di liquidi e secrezioni in sede endoluminale . 
le cause di dilatazione del canale vaginale e / o della cavit uterine possono non essere identificate correttamente allesame ecografico , specialmente in caso di malformazioni del sistema uro - genitale . 
durante lesame rm nel sospetto di seno uro - genitale comune complicato da una steno si vaginale , lo svuotamento della vescica non richiesto per dimostrare lorigine comune delluretra e della vagina cos come avviene per la cistografia minzionale . 
inoltre lanatomia delladdome e della pelvi ed eventuali altre anomalie associate sono molto chiaramente evidenziabili allo studio rm . torsione tubarica the grade of adnexal vascular compromise can also be easily documented on postgadolinium scans by a reduction altra causa di dolore pelvico nelle bambine , di non facile diagnosi ecografia , la torsione isolata della tuba di fal578 radiol med ( 2012 ) 117 : 575592 fig . 
t2 - weighted mri axial view ( b ) confirms the presence of a central mass showing a thickened wall ( black arrow ) ; the right ovary ( b , open arrow ) is enlarged and oedematous ( strongly hyperintense )  . 
on t2 - weighted mri coronal view ( c ) , the uterus is deviated to the right side ( large white arrow ) ; and the ovary and pelvic mass are visible ( small white arrow and black arrow , respectively )  . 
 axial gadolinium - enhanced 3d fat - saturated t1 - weighted spoiled gradient recovery mri sequence ( d ) shows vascular stasis at the right adnexal pedicle ( calliper ) and better depicts the thickened wall of the mass ( arrow )  . 
la scansione assiale rm t2 pesata ( b ) conferma la massa pelvica centrale che presenta parete spessa ( freccia nera ) ; lovaio di destra ( b , freccia vuota ) ingrandito ed edematoso ( fortemente iperintenso )  . 
nella scansione coronale t2 pesata ( c ) lutero chiaramente deviato a destra ( freccia bianca grande ) mentre la freccia bianca piccola e quella nera indicano lovaio e la massa centro - pelvica . 
dopo somministrazione di mdc paramagnetico ( d ) si documenta stasi vascolare a livello del peduncolo ovarico ( caliper ) e meglio si documenta la parete , spessa , della massa centro - pelvica ( freccia )  . 
la diagnosi rm confermata allintervento ( e ) che documenta la torsione della tuba , marcatamente ectasica ( freccia )  . or lack of enhancement compared with the other side . 
 leco - color doppler non sempre in grado di determinare radiol med ( 2012 ) 117 : 575592 girls at puberty during puberty , pelvic pain in girls could be related to the menstrual cycle , as in the case of follicular cyst rupture , haemorrhagic follicular cysts , haemorrhagic corpus luteum and corpus luteal cysts , which can occur in every woman of fertile age . 
the accuracy of us in detecting haemorrhagic lesions is well known , and sonographic findings vary widely , as intracystic echoes depend upon the quality and quantity of blood clots [ 17 ]  . 
in the case of corpus luteal cysts , us may show many typical findings , such as an intracystic reticular pattern or a markedly vascular wall on colour doppler evaluation , which is known as a ring of fire . 
however , when a haemorrhagic cyst has a mass - like appearance or a retracting blood clot is present , us is not always able to differentiate these cysts from an ovarian neoplas therefore , us monitoring or mri examination is needed to make a correct diagnosis . 
recent studies demonstrated the added value of perfusionand diffusion - weighted mri in characterising complex ovarian masses , with 95% accuracy in differentiating benign from malignant lesions when criteria of conventional , perfusionand diffusion - weighted mri are combined [ 18 ]  . congenital abnormalities among gynaecological causes of pelvic pain seen at puberty and often requiring mri for correct assessment of disease are symptomatic congenital anomalies of the mllerian systethese anomalies are related to failure of parameso - nephric duct fusion or to incomplete canalisation of the vaginal plate , thus causing pelvic pain at menarche as the normal menstrual flow is partially or totally obstructed . 
 il grado di compromissione vascolare pu essere facilmente documentato nelle immagini t1 pesate dopo somministrazione endovena ( ev ) di mezzo di contrasto ( mdc ) quale riduzione o assenza di enhancement . 
la semeiotica rm in grado di supportare lecografia nella diagnosi di torsione ovarica verr discussa nella sezione successiva ( donne in et riproduttiva )  . giovani donne in et puberale durante la pubert il dolore pelvico nelle giovani donne frequentemente associato al ciclo mestruale , come in caso di rottura di cisti follicolare , di cisti follicolare emorragica , di corpo luteo emorragico o di corpo luteo cistico , come pu accadere in ogni donna in et fertile . 
quando non avviene la rottura del follicolo dominante , con conseguente espulsione delloocita , si sviluppa la cisti follicolare che pu essere causa di dolore in caso di crescita rapida della cisti o in caso di emorragia . 
il corpo luteo si forma dopo lovulazione sotto lo stimolo dellormone luteinizzante e pu andare incontro ad emorragia per il notevole aumento della sua vascolarizzazione durante la fase luteinica del ciclo . 
la accuratezza diagnostica dellecografia nella identificazione di lesioni emorragiche ben conosciuta e i segni caratteristici mostrano ampia variabilit poich gli echi interni della formazione cistica sono in dipendenza dalla quantit della componente ematica e prodotti di degradazione dellemoglobina [ 17 ]  . 
in caso di corpo luteo cistico lecografia mostra segni caratteristici come il pattern intra - cistico reticolare e la marcata vascolarizzazione periferica al color doppler conosciuto come anello di fuoco . 
il corpo luteo emorragico pu a volte presentarsi con un aspetto pi complesso simile ad una massa cistica , con un coagulo parietale che pu assumere un aspetto retrattile ; in questi casi lecografia non sempre in grado di differenziarlo da una neoplasia ovarica . 
inoltre , la rm preferibile allesame tc delladdome nelle giovani donne perch non espone a ra580 radiol med ( 2012 ) 117 : 575592 diazioni ionizzanti e per la capacit di mostrare i prodotti di degradazione dellemoglobina . 
studi recenti hanno inoltre dimostrato il valore aggiuntivo dellimaging di perfusione e dellimaging pesato in diffusione in rm nella caratterizzazione di masse ovariche complesse , con unaccuratezza riportata del 95% nella differenziazione tra lesioni ovariche benigne e maligne valutando contemporaneamente criteri convenzionali , di perfusione ed in diffusione [ 18 ]  . anomalie congenite tra le cause ginecologiche di dolore pelvico in et puberale che possono non essere correttamente identificate allesame ecografico , ma che possono vantaggiosamente avvalersi della rm per una diagnosi corretta , sono da menzionare le anomalie congenite del sistema mlleriano . 
esse sono dovute alla mancata fusione dei dotti para - mesonefrici o allincompleta canalizzazione della vagina e sono causa di dolore pelvico al menarca per ostruzione o rallentamento del flusso mestruale . 
la paziente presenta dolore per il flusso che si accumula durate il ciclo mestruale nel corno uterino rudimentale non comunicante , mentre laltro corno drena normalmente [ 20 ]  . 
in questi casi lecografia pu mostrare facilmente lematometra o lematocolpo mentre la presenza di tessuto endometriale allinterno di un corno rudimentale potrebbe non essere facilmente documentato e un setto vaginale potrebbe essere misconosciuto , se loperatore non particolarmente esperto . 
rm in grado di identificare sia le anomalie anatomiche dellutero che le strutture pelviche , per la pi elevata risoluzione spaziale , ed in grado di fornire quei dettagli anatomici che sono strettamente necessari ai fini chirurgici . donne in et riproduttiva fig . 
2a , b a 12 - year - old girl with pelvic pat2 - weighted mri coronal ( a ) and sagittal ( b ) views show two uterine horns ( a , arrows ) and two hemivaginas separated by a longitudinal septum ( b )  . 
le scansioni rm coronale ( a ) e sagittale ( b ) t2 pesate documentano due corni uterini ( a , frecce ) e due emi - vagine ( b ) separate da un setto longitudinale . 
in a noncommunicating rudimentary uterine horn with an endometrial cavity , the patient presents cyclic pain due to retrograde menstrual flow arising from the noncommunicating uterine cavity while the other horn drains normally [ 20 ]  . 
3a - d a 29 - year - old women with intermittent pelvic pat2 - weighted coronal mri ( a ) shows a hyperintense enlarged left ovary ( black arrow ) to which blood vessels converge ( white arrow ) , adhering to the uterus ; distally , a cystic mass is also visible ( a , open arrow )  . 
t1 - weighted axial images ( b , c ) show hyperintense foci consistent with haemorrhage ( b , white arrow ) within the enlarged left ovary and within the cyst ( c , arrow )  . 
t1 - weighted gadolinium - enhanced mri axial image ( d ) shows straight vessels draping around the lesion ( white arrow ) and poor enhancement of the ovary ( open arrow )  . 
la scansione rm coronale t2 pesata ( a ) mostra un ovaio di sinistra ingrandito , con segnale iperintenso ( freccia nera ) in cui convengono i vasi ( freccia bianca ) , adeso cranialmente allutero ; distalmente si rileva anche una formazione cistica ( a , freccia vuota )  . 
le immagini assiali t1 pesate ( b , c ) documentano foci emorragici nellovaio sinistro ingrandito ( b , freccia bianca ) che sono visibili anche nel contesto della formazione cistica ( c , freccia )  . 
dopo somministrazione di mdc paramagnetico ( d ) si documentano i vasi stirati in corrispondenza dellovaio di sinistra ( freccia bianca ) che mostra scarso enhancement ( freccia vuota )  . 
diagnosi rm : torsione ovarica associata a cisti ( conferma chirurgica )  . strate the haematometra or haematocolpos , whereas a small amount of endometrial tissue in a rudimentary uterine horn might be missed if transvaginal us is denied and the operator is not experienced . 
mri can conclusively assess the abnormal anatomy of the uterus and surrounding structures , as its spatial resolution is higher than that in us and provides the anatomical details mandatory for surgical planning . 
in the case of unilateral pain , acute appendicitis , urinary tract disorders and gastrointesidentificate correttamente allesame ecografico . quando il dolore diffuso associato con il ciclo mestruale , con i rapporti sessuali , con la defecazione o con uno stato di infertilit [ 11 ] , dovr essere esclusa la presenza di adenomiosi o di endometriosi . 
tutte queste condizioni patologiche sono usualmente indagate in prima istanza dallecografia , ma la rm pu essere richiesta e risultare utile in tutti quei casi i cui lecografia non risolutiva , come verr analizzato in seguito . 582 radiol med ( 2012 ) 117 : 575592 tinal problems need to be differentiated from gynaecological causes [ 21 ]  . 
us is usually the first imaging modality used to investigate these pathological conditions , with mri being required in some cases , especially when us is inconclusive . ovarian torsion in adults , ovarian torsion most commonly occurs in the first 3 decades of life and frequently involves the ovary and corresponding fallopian tube . 
 if rotation is complete and prolonged , a venous and arterial thrombosis can occur inducing an increase of the ovary volume and , consequently , a stretching of the capsule which causes acute pelvic paus usually show an enlarged ovary with follicles peripherally distributed [ 11 ]  . 
this is a common condition among sexually active women of reproductive age , but its incidence in young women between 15 and 19 years of age has increased due to changing sexual habits [ 24 ]  . 
most cases result from ascending infection , usually caused by a mixture of anaerotorsione ovarica in una donna adulta la torsione ovarica pi frequente nelle prime tre decadi di vita , pi spesso coinvolge lovaio e la tuba e si associa alla presenza di cisti o massa ovarica nel 50% dei casi [ 22 ]  . 
in caso di torsione parziale o intermittente , la congestione venosa e linfatica sono ridotte , ma se la torsione completa o prolungata la trombosi venosa e locclusione arteriosa determinano un aumento del volume ovarico con il conseguente stiramento della capsula ovarica che induce dolore pelvico acuto . 
tuttavia , lincidenza di tale patologia in aumento nelle donne di et compresa tra i 15 e 19 anni a causa delle modificazioni delle abitudini sessuali dei giovani [ 24 ]  . 
la pid diagnosticata clinicamente e mediante esami di laboratorio ( dolore pelvico , febbre , leucocitosi ) , ma la diagnostica per immagini ha un suo ruolo nei casi dubbi , nelle forme gravi o non rispondenti alla terapia antibiotica . 
lidrosalpinge frequentemente osservata in ecografia e lesame ecografico usualmente in grado di identificare un ascesso tuboovarico , che si caratterizza come una massa ipoecogena , unica , con vascolarizzazione ad anello periferico , associata a fluido nel cul - de - sac . 
 la tc documenta agevolmente ledema dei tessuti molli nella pelvi , lispessimento dei ligamenti utero - sacrali e la piosalpinge , che appare come una lesione densa spesso con radiol med ( 2012 ) 117 : 575592 fig . 
4a - d a 27 - year - old woman with fever and pelvic pat2 - weighted mri axial scans ( a , b ) show an obstructed enlarged left tube with internal debris ( a , open arrow ) , peritubal fluid ( a , white arrow ) and a centrally hyperintense tubo - ovarian mass with a hypointense rim ( b , white arrow ) suspicious for an abscess . 
on fat - saturated t1 - weighted mri axial image ( c ) , the tubo - ovarian mass is centrally mildly hypointense and shows a hyperintense rim ( open arrow )  . 
le scansioni assiali t2 pesate ( a , b ) mostrano una tuba di sinistra ectasica e con materiale amorfo endoluminale ( a , testa di freccia ) , fluido peri - tubarico ( a , freccia bianca ) e una massa tra la tuba e lovaio centralmente iperintensa con cercine ipointenso ( b , freccia bianca ) sospetta per ascesso . 
nella scansione assiale t1 pesata con saturazione del segnale del tessuto adiposo ( c ) la massa tubo - ovarica modicamente ipointensa e documenta un cercine iperintenso ( testa di freccia )  . 
pid is usually diagnosed clinically and by laboratory tests ( pain , fever and leukocytosis ) , but imaging studies are performed in patients with uncertain diagnosis , those who are severely ill or those who do not respond to therapy . 
hydrosalpinx is most often seen on us images , which detects a tubo - ovarian abscess as a single hypoechoic mass with a thick vascular ring associated with free fluid in the cul - de - sac , although in some cases , differential diagnosis with ovarian cancer in not easy . 
in emergency settings , ct is usually requested to complement inconclusive us imaging [ 25 ] , as ct clearly depicts oedema of the surrounding tissues , thickening of the uterosacral ligaments and pyosalpinx as a dense lesion , often with an air level , livello fluido / aereo nel suo contesto , segno utile per linquadramento della patologia flogistica . 
la rm pu essere utilizzata nella diagnosi di idrosalpinge o di ascesso tuboovarico [ 26 ] con sensibilit e specificit diagnostica rispettivamente del 95% e 89% [ 24 ] e senza impiego di radiazioni ionizzanti . 
however , mri can be usefully employed to delineate hydrosalpinx [ 26 ] and also shows 95% sensitivity and 89% specificity in diagnosing tubo - ovarian abscess [ 24 ]  . 
among its various symptoms - such as severe dysmenorrhoea , deep dyspareunia , infertility and chronic fatigue reaction - the cyclical or perimenstrual pelvic pain with or without abnormal bleeding is the most frequent clinical finding [ 29 ]  . 
mri is superior to us , as it provides a more defined characterisation of endometriomas because of its ability to detect haemorrhage on t1weighted fat - saturated images and a more adequate assessment of extraovarian lesions . 
hyperintense foci on t1 - weighted fat - saturated mri are useful in the case of peritoneal implants but are not essential for diagnosing deep endometriosis , even if it may be observed . 
the diagnosis of deep endometriosis is usually based on the presence of fibrotic nodules in typical sites , which are documented by strongly hypointense lesions on t2 - weigheted images . 
special attention should be paid to the timing of mri examinations , which should be performed after the eighth day of the cycle in order to better detect blood foci [ 4 ]  . 
 adenomyosis adenomyosis occurs in women usually ranging in age between 35 to 55 years and it is due to the abnormal implant of endometriosi lendometriosi , una delle cause di dolore pelvico nelle donne in et riproduttiva , caratterizzata dalla presenza di ghiandole endometriali e stroma in sede extra - endometriale associata a reazione infiammatoria cronica . 
il sintomo clinico pi frequente il dolore ciclico peri - mestruale associato o meno a sanguinamenti anomali ; altri sintomi e segni sono la dismenorrea , dispareunia profonda , linfertilit , e laffaticamento [ 29 ]  . 
tuttavia , la rm superiore allecografia sia nella caratterizzazione dellendometrioma , per la capacit di identificare sedi di emorragia nelle immagini t1 pesate con soppressione del segnale del tessuto adiposo , sia nella identificazione di lesioni extra - ovariche . 
foci di iperintensit nelle immagini t1 pesate con soppressione del segnale del grasso , sono tipiche delle localizzazioni sierose , ma non sono essenziali per la diagnosi di endometriosi profonda , anche se possono essere osservati . 
unattenzione particolare deve essere tenuta per la tempistica dellesame rm nel sospetto di tale patologia , che deve essere effettuato dopo lottavo giorno del ciclo per identificare meglio i prodotti ematici [ 4 ]  . 
inoltre importante conoscere eventuali interventi chirurgici precedenti per evitare errori diagnostici . adenomiosi ladenomiosi colpisce donne di et compresa tra i 35 e i 55 anni , ed associata alla presenza di impianti di endometrio basale allinterno del miometrio . 
5a - c a 38 - year - old woman in the 20th week of pregnancy with acute pelvic paon t1 - weighted mri axial scan ( a ) , a solid mass ( arrow ) not showing haemorrhage or fat is documented on the right side . 
fast imaging using steady - state free precession acquisition in the coronal plane ( c ) clearly documents that the mass is closely connected with the uterine wall ( arrows )  . 
the differential diagnosis is better achieved by means of mri : focal lesions caused by adenomyosis ( i.e focal thickening of junctional zone or pseudowidening ) tend to be ovoid and show poor defined margins and poor mass effect on the endometrium whereas fibroids tend to be round , showing well defined margins and a mass effect on the endometrium especially when are submucosal . 
mri may differentiate adenomyomas from adenomatoid tumors by showing characteristic features such as hyperintense foci on t2 - weighted images diffusely dallesame rm in quanto le lesioni focali di adenomiosi caratterizzate dallispessimento focale della zona giunzionale ( pseudowidening ) sono generalmente di forma ovoidale , a margini sfumati mal definiti e non presentano effetto massa sulla cavit endometriale mentre i fibroleiomiomi tendono ad avere una forma rotonda , margini ben definiti ed effetto massa sulla cavit endometriale se a localizzazione sottomucosa . 
 anche in questo caso lesame rm pu essere di aiuto nella diagnostica differenziale : ladenomioma si differenzia dal tumore adenomatoide per la presenza di foci iperintensi nelle immagini t2 pesate localizzati diffusamente allinterno della lesione mentre nel tumore adenomatoide , raro tumore benigno di natura mesoteliale , i foci iperintensi si dispongono alla periferia in quanto espressione di tubuli mesoteliali dilatati . 586 radiol med ( 2012 ) 117 : 575592 distributed within the mass in the case of adenomyomas and peripherally distributed in the case of adenomatoid tumors , a rare benign mesotelial tumor , since in this last case they are related to dilated mesotelial tubules . pcs pelvic congestion syndrome pcs is characterised by dilatation of ovarian veins and pelvic venous plexus in premenopausal women , suggesting a correlation between pelvic congestion and ovarian activity [ 32 ]  . 
the pain is exacerbated by movements increasing intra - abdominal pressure , such as lifting or walking , and can be associated with dyspareunia ( 70% of cases ) , dysmenorrhoea ( 66% ) and postcoital pain ( 65% ) [ 34 ]  . 
 findings include tortuous and dilated tubular structures around the ovary and uterus , with diameter > 4 mm , showing a low blood flow ( about 3 cm / s ) ; arcuated veins in the myometrium are dilated , as they communicate with bilateral pelvic varicose veins [ 34 ]  . 
mri diagnosis is easy and not invasive , documenting tubular structures around the uterus and ovaries with no signal intensity on t1 - weighted images related to the flow - void artefacts , high signal intensity on gradientecho images and low signal intensity on t2 - weighted images . fibroids fibroids are the most common gynaecological neoplasm and occur in 2030% of women of reproductive age . 
pain occurs in approximately 30% of cases as a result of torsion of pedunculated leiomyomas or acute degeneration , usually accompanied by systemic symptoms such as tenderness , fever and leukocytosis [ 35 ]  . 
degeneration is most commonly observed during pregnancy , as the increase in size of the uterus may interfere with the blood supply to fibroids and cause either cystic or red ( haemorrhagic ) degeneration . 
b - mode us can identify a non homogeneous mass , and colour doppler investigation documents regularly separated vessels at the periphery of the mass , which exhibit moderate vascular resistance . 
leiomyomas with hyaline degeneration have low signal intensity on t2 - weighted images la pcs si caratterizza per la dilatazione delle vene ovariche e del plesso venoso pelvico in donne in et pre - menopausale , suggerendo pertanto una correlazione con la congestione venosa e lattivit ovarica [ 32 ]  . 
il dolore aumenta caratteristicamente con i movimenti che determinano aumento della pressione intra - addominale , come lo stiramento e il camminare , e pu associarsi a dispareunia ( 70% dei casi ) , dismenorrea ( 66% ) e dolore post - coitale ( 65% ) [ 34 ]  . 
i reperti includono strutture tubulari tortuose e dilatate intorno allovaio , con diametro > 4 mm , caratterizzate da un rallentato flusso ( 3 cm / s ) ; si associa la presenza delle vene arcuate del miometrio dilatate che comunicano con il plesso venoso pelvico dilatato [ 34 ]  . 
la diagnosi semplice e non invasiva , documentando la presenza di strutture tubulari in sede peri - uterina e peri - ovarica , caratterizzate da assenza di segnale nelle immagini t1 pesate , in relazione allartefatto da vuoto da flusso e da iperintensit nelle immagini t2 pesate . fibromi i fibroleiomiomi sono le neoplasie ginecologiche benigne pi frequenti nelle donne in et riproduttiva , con unincidenza del 20%30% . 
il dolore presente nel 30% dei casi , come risultato della torsione di un leiomioma peduncolato o di degenerazione acuta , associato a sintomi generali quali debolezza , febbre , leucocitosi [ 35 ]  . 
t2 - weighted sagittal mri ( b ) confirms the thickened endometrium ( white arrows ) and non homogeneous signal intensity of the myometrium ( black arrow ) ; movement artefacts are present due to the patients acute pelvic paon gadolinium - enhanced 3d fat - saturated t1 - weighted axial spoiled gradient recovery sequence ( c ) , both the endometrium and myometrium ( white arrows ) are involved by an enhancing mass with poorly defined margins . 
la scansione ecografica longitudinale obliqua ( a ) mostra un endometrio ispessito ( frecce bianche ) sospetto per neoplasia endometriale e un aspetto ecostrutturale disomogeneo del miometrio ( frecce nere )  . 
la scansione rm sagittale t2 pesata ( b ) conferma lispessimento endometriale ( frecce bianche ) e da disomogenea intensit di segnale del miometrio ( freccia nera ) ; gli artefatti da movimento documentano il dolore acuto della paziente . 
dopo somministrazione di mdc paramagnetico ( c ) si osserva tessuto ad enhancement positivo che coinvolge sia lendometrio che il miometrio ( frecce bianche ) che mostra aspetto di tipo infiltrativo . 
leiomyomas with red degeneration show peripheral or diffuse high signal intensity on t1 - weighted images , probably related to proteinaceous content of the blood , and variable signal intensity with or without a low - signal - intensity rim on t2 - weighted images [ 35 ] postmenopausal women pelvic pain in postmenopausal women is rarely associated with uterine neoplasm , but dyspareunia can be present . 
il leiomioma con degenerazione rossa presenta una periferica o diffusa iperintensit di segnale nelle immagini pesate in t1 , in relazione allelevato contenuto proteico del sangue , ed una variabile intensit di segnale nelle immagini pesate in t2 , con o senza un anello periferico di ipointensit [ 35 ]  . donne in et post - menopausale il dolore pelvico in donne in et post - menopausale raramente associato con neoplasie uterine , ma pu essere presente dispareunia . 
specialmente in caso di sanguinamento vaginale dovrebbe essere esclusa la presenza di neoplasia uterina . the case of vaginal bleeding , in particular , a uterine neoplasm should be initially excluded . neoplasie 588 neoplasm it is well known that mri is the most accurate imaging technique for staging endometrial carcinoma [ 22 ] or cervical cancer . 
the differential diagnosis between endometrial carcinoma and secondary involvement of the uterus by a primary neoplasm in other sites is very difficult to obtain on the basis of us alone . 
it complicates 23% of vaginal deliveries and up to 80% of caesarean sections [ 36 ] , and it is the most common cause of fever in the postpartum period [ 37 ]  . 
sonographic findings include a heterogeneous endometrium with irregular surface , but the diagnosis of the disease is difficult , even in the presence of a clinical suspicion ( medical history , high erythrocyte sedimentation rate , elevated cancer antigen 125 ( ca - 125 ) and chest x - ray with lesions suggestive for tuberculosis )  . 
mri readily shows a supravaginal fluid - filled pelvic mass , corresponding to pyometra [ 41 ] , but it is especially useful for surgical planning , as it adds information regarding the possible involvement of the fallopian tube and ovary and clearly depicts the pelvic anatomy . 
 gartners duct cyst radiol med ( 2012 ) 117 : 575592 laccuratezza diagnostica della rm nella stadiazione prechirurgica del carcinoma dellendometrio [ 22 ] e della cervice uterina sono elevate , ma la rm rappresenta un utile strumento anche nella valutazione di eventuale interessamento metastatico dellutero che pu essere erroneamente interpretato come neoplasia primitiva allesame ecografico . 
complica il 2%3% dei parti per via vaginale e fino all80% dei parti cesarei [ 36 ] e rappresenta la pi frequente causa di febbre nel periodo post - partum [ 37 ]  . 
la bassa incidenza di endometriti nel periodo post - menopausale pu essere associato allatrofia dellendometrio , che offre un terreno non ottimale per la crescita dei batteri [ 38 ]  . 
ci nonostante alcuni autori riportano casi di endometrite tubercolare in donne in et post - menopausale [ 38 , 39 ] , con dolore pelvico associato nel 25% dei casi . 
il quadro ecografico include laspetto disomogeneo dellendometrio che presenta una superficie irregolare , ma la diagnosi risulta difficile anche in caso di forte sospetto clinico [ storia clinica positiva , antigene carboidrato ( ca ) 125 elevato , radiografia ( rx ) torace positiva per localizzazioni di malattia tubercolare ]  . 
la persistenza di massa pelvica , associata a dolore ricorrente o sanguinamento , dopo 9 mesi dal termine del trattamento anti - tubercolare , sono indicazioni al trattamento chirurgico [ 40 ]  . 
la rm pu evidenziare la presenza di una massa sopravaginale ripiena di fluido , corrispondente ad una piometra [ 41 ] , ma il suo ruolo cruciale nel planning pre - chirurgico poich in grado di identificare leventuale coinvolgimento delle tube , dellovaio , ed in grado di documentare chiaramente lanatomia pelvica . cisti di gartner an inflamed gartners duct cyst can also cause pelvic pa these cysts arise from mesonephric ducts or wolffian duct remnants and are usually located in the anterolateral wall of the proximal third of the vagina . 
the incidence of gartners duct cysts is low , 12% of the total population [ 42 ] , but they una cisti del dotto di gartner infiammata pu essere causa di dolore pelvico . 
la cisti del dotto di gartner origina dai dotti mesonefrici o residui del dotto di wolff , ed generalmente localizzata nella parete antero - laterale del iii prossimale della vagina . 
asymptomatic in 20% of cases , gartners duct cysts can cause pelvic pain in 4% of cases and can be associated with recurrent urinary tract infections in 27% [ 43 ]  . 
an inflamed gartners duct cyst could mimic an inflamed urethral diverticulum at clinical evaluation , especially when it is located distally and not in the proximal third of the vagina . 
however , these lesions show similar findings on us as a gartners duct cyst and urethral diverticulua more precise diagnosis can be made by mri , which clearly defines the anatomical site of the lesions . 
accurate assessment of the lesion site is especially useful for surgical planning . sa , 1%2% nella popolazione generale [ 42 ] , ma pu essere documentata in un quarto della popolazione di donne adulte [ 34 ]  . 
asintomatica nel 20% dei casi , la cisti di gartner pu associarsi a dolore pelvico nel 4% dei casi ed a infezioni urinarie ricorrenti nel 27% [ 43 ]  . 
lesatta localizzazione della lesione di fondamentale importanza anche ai fini chirurgici . conclusions conclusioni us is the first - line imaging modality in women with pelvic pain and is considered conclusive in most cases . 
 symptomatic uterine malformations , ovarian and tubal torsion , common and uncommon uterine cancers , usual and unusual pelvic sites of endometriosis , deep endometriosis , adenomyomas , tubo - ovarian abscess , inflamed lesame ecografico rappresenta la metodica di prima istanza nella valutazione delle cause di dolore pelvico femminile e pu essere considerata conclusiva in molti casi . 
la tc generalmente utilizzata in regime di urgenza , quando lecografia non stata dirimente , dal momento che alcune condizioni patologiche ginecologiche presentano aspetti tc caratteristici [ 26 ]  . 
in casi di esame ecografico dubbio , specie in caso di dolore pelvico cronico , la rm dovrebbe essere preferita nello studio della pelvi femminile perch in grado di determinare la diagnosi senza esporre la paziente a dose radiante . 
 malformazioni uterine sintomatiche , torsioni dellovaio e della tuba , neoplasie uterine comuni o rare , localizzazioni usuali o non usuali di endometriosi , endometriosi profonda , radiol med ( 2012 ) 117 : 575592 590 fig . 
t2 - weighted sagittal mri ( a ) documents a hyperintense lesion ( large white arrow ) characterised by a small neck ( small white arrow ) located outside the anterior vaginal wall ( open arrow )  . 
la scansione rm sagittale t2 pesata ( a ) mostra una lesione iperintensa ( freccia grande bianca ) , caratterizzata da un piccolo colletto ( freccia bianca piccola ) , localizzata al davanti della parete vaginale anteriore ( testa di freccia )  . 
 la sede della lesione ( al di fuori della parete vaginale ) differenzia il diverticolo uretrale dalla cisti del dotto di gartner . gartners duct cysts and urethral diverticula are better evaluated by mri than by us . 
the main advantages of mri are the large field of view , the multiplanar imaging capability , the excellent soft - tissue contrast resolution and its ability to detect blood products . 
mri can be especially useful when surgery must be planned , because the correct topography of the lesion is clearly depicted together with possible associated changes in the surrounding tissue and structures . 
the range of pelvic disorders that can be correctly diagnosed with mri is extremely wide , and the lack of exposure to ionising radiation is essential when evaluating children , and women of reproductive age . adenomioma , ascessi tubo - ovarici , cisti di gartner infiammate e diverticoli ureterali possono essere correttamente e meglio valutati con la rm rispetto allesame ecografico . 
simonetti1 1dipartimento di diagnostica per immagini , imaging molecolare , radiologia interventistica e terapia radiante , universit degli studi di roma tor vergata ( ptv ) , viale oxford 81 , 00133 rome , italy 2dipartimento di sanit pubblica e biologia cellulare , universit degli studi di roma tor vergata ( ptv ) , rome , italy correspondence to : c.a. 
our analysis emphasises the benefits of vab compared with surgical biopsy in terms of both costeffectiveness , and less invasiveness from a psychological and aesthetic point of view . keywords breast vacuum - assisted breast biopsy surgical biopsy cost - effectiveness riassunto obiettivo . 
presso il nostro centro , da novembre 2008 a settembre 2009 , abbiamo selezionato 200 pazienti con lesioni mammarie sospette da sottoporre a caratterizzazione istologica , che stata effettuata in 100 / 200 pazienti mediante prelievo vab e nelle rimanenti 100 / 200 pazienti mediante biopsia chirurgica . 
lanalisi da noi svolta ha evidenziato i vantaggi delle procedure vab , rispetto alla biopsia chirurgica , sia in termini di costo - efficacia che in termini di minor invasivit estetica e psicologica . parole chiave mammella biopsia mammaria vuotoassistita biopsia chirurgica costo - efficacia 540 introduction five - year survival rates for patients diagnosed with breast cancer have increased by approximately 11% over the last few years . 
to this end , minimally invasive interventional procedures enable a correct histological lesion characterisation and simultaneous evaluation of biological parameters necessary for adequate prognostic and therapeutic planning [ 46 ] , whereas in the past , recourse to surgery was inevitable . 
although cytology in expert hands can offer important diagnostic information , the rate of inadequate and false - negative results should not be overlooked [ 7 , 8 ]  . core needle biopsy ( cnb ) is a widespread , relatively inexpensive , easy and fast sampling method with a good level of concordance with the final histological diagnosis . 
 thanks to technological advances , vacuum - assisted biopsy ( vab ) has become increasingly popular as an alternative to diagnostic surgical biopsy owing to its diagnostic reliability and lower cost [ 9 , 10 ]  . 
 the advantages of vab over cnb are many , and include the larger quantity of sampled breast tissue , the absence of inadequate samples and a substantial reduction in the false - negative rate ( approximately 16% )  . 
several published studies have demonstrated that 50% of lesions diagnosed as adh at cnb contain areas of carcinoma in situ and that 30% of carcinomas in situ harbour an infiltrating component [ 11 ]  . 
compared with surgical biopsy , vab is less invasive in terms of cosmesis , with no parenchymal or skin scarring , is faster to perform and has a lower complication rate and costs . 
correct evaluation of the histological sample obtained with vab systems allows for accurate diagnosis , comparable with that of surgical biopsy but without the use of surgery for mere diagnostic purposes . 
 in this context , the use of vab systems helps to accurately select patients for surgery , with the additional advantage radiol med ( 2012 ) 117 : 539557 introduzione la sopravvivenza a cinque anni per coloro a cui stato diagnosticato un cancro della mammella aumentata negli ultimi anni di circa l11% . 
nella patologia mammaria , infatti , sempre pi spesso , appare indispensabile ottenere un corretto inquadramento diagnostico tramite unadeguata caratterizzazione cito - istologica di lesioni individuate come sospette allimaging convenzionale . 
 a tal fine , mentre in passato era indispensabile il ricorso allintervento chirurgico , attualmente , mediante procedure interventistiche mini - invasive , possibile effettuare una corretta tipizzazione istologica di tali reperti e la contestuale valutazione dei parametri biologici necessari per unadeguata pianificazione prognostico - terapeutica [ 46 ]  . 
sebbene la citologia , quando affidata a mani esperte , possa offrire importanti informazioni diagnostiche , tuttavia non bisogna disconoscere il tasso di inadeguati e falsi negativi che gravano su tale metodica [ 7 , 8 ]  . la core needle biopsy ( cnb ) considerata una modalit di prelievo largamente diffusa a costi contenuti , di facile e rapida esecuzione con buona concordanza con listologico definitivo . 
negli ultimi anni in particolare , grazie allo sviluppo tecnologico , sono andati sempre pi diffondendosi i sistemi vuoto - assistiti ( vab ) come valida metodica di prelievo istologico , sia per laffidabilit diagnostica sia per i minori costi in alternativa alla biopsia chirurgica a fini diagnostici [ 9 , 10 ]  . limportanza di tali sistemi nella pratica clinica ormai consolidata da numerosi contributi scientifici che ne hanno validato laccuratezza diagnostica [ 9 , 10 ]  . 
 i vantaggi dei prelievi vuoto - assistiti rispetto alla cnb sono molteplici : la quantit di tessuto mammario prelevato senzaltro maggiore , i prelievi inadeguati sono assenti ed i falsi negativi sensibilmente ridotti ( approssimativamente compresi tra l1% ed il 6% )  . 
numerosi studi descritti in letteratura inoltre , hanno messo in evidenza che il 50% delle lesioni diagnosticate come iperplasia atipica ( adh ) alla cnb , contengono aree di carcinoma in situ , e che il 30% dei carcinomi in situ racchiudono una componente infiltrante [ 11 ]  . 
laccuratezza diagnostica della vab rispetto alla cnb risulta aumentata e si raggiunge la definizione della lesione in termini di benignit o di malignit in una percentuale di casi compresa tra il 93% ed il 95% [ 2 , 3 ]  . 
le procedure vab consentono di ridurre sensibilmente lerrore di campionamento dovuto al non corretto posizionamento dellago ( pochi millimetri ) o ad un suo eventuale spostamento [ 6 ]  . 
 rispetto alla biopsia chirurgica , invece , lutilizzo dei sistemi vuoto - assistiti permette una minore invasivit dal punto di vista estetico , grazie allassenza assoluta di sequele cicatriziali a carico del parenchima e della cute , ai brevi tempi di esecuzione , al basso tasso di complicanze ad essi correlate ed ai minori costi . 
un ulteriore vantaggio del prelievo vab radiol med ( 2012 ) 117 : 539557 of obtaining the diagnosis prior to surgery and avoiding surgery on lesions that , after being identified as suspicious on conventional imaging , prove to be benign on percutaneous sampling . in a setting of diminishing healthcare resources , it is advisable to reduce the number of surgical procedures performed for diagnostic purposes only and to limit , through the use of these alternative systems , surgery to cases of proven malignancy . 
the aim of this study was to compare the cost - effectiveness of the two breast biopsy methods : surgery , to date considered the gold standard ; and the more recent vab technique . materials and methods patient population between november 2008 and september 2009 , 200 patients presenting with suspicious breast lesions ( microcalcifications , parenchymal distortions , nodules , areas of enhancement ) were selected for histological characterisation . 
 the study was approved by our local ethics committee , and signed informed consent was received from all patients whom , after receiving adequate information about the two biopsy techniques , procedures , benefits and possible risks , freely chose which procedure to undergo . 
 all 100 patients who opted for percutaneous breast biopsy underwent blood chemistry tests to assess coagulation profile , whereas those who selected surgical biopsy underwent , in addition to blood chemistry testing , chest xray and anaesthesiological assessment . 
with regard to the choice of imaging guidance , although based on the modality that best allowed lesion detection , ultrasound ( us ) was preferred where possible due to its lower cost and ease and speed of use . 
stereotactic guidance was used in patients with microcalcifications , who were studied with radiography of the tissue cores in the case of vab and of the surgical specimen in the case of surgical biopsy ; magnetic resonance imaging ( mri ) guidance was used for lesions visible on mri alone . 
vab sampling was carried out with the vacora breast biopsy system ( tempe , az , usa ) under sonographic guidance in 30 lesions , stereotactic mammography guidance in 50 and mri guidance in 20 / 100 lesions not visible on conventional imaging . 
la corretta valutazione del preparato istologico ottenuto tramite tali sistemi di prelievo , consente una diagnosi accurata e precisa , sovrapponibile a quella della biopsia chirurgica , permettendo di evitare lutilizzo di questultima a fini diagnostici . 
in tale contesto lutilizzo dei sistemi vab , consente quindi di selezionare i casi per cui si rende effettivamente necessario un intervento chirurgico , con il vantaggio di conoscere pre - operatoriamente la diagnosi e di evitare lintervento chirurgico nelle lesioni che , individuate come sospette allimaging tradizionale , si caratterizzano come benigne al prelievo percutaneo . sarebbe auspicabile pertanto che il numero di interventi chirurgici con esclusiva finalit diagnostica possa essere ridotto e che limpiego di tali sistemi possa limitare il ricorso alla chirurgia solo nei casi di effettiva malignit in un contesto sanitario di risorse economiche sempre pi carenti . 
 in tale ambito lobiettivo dellanalisi che segue confrontare in termini di costi ed efficacia le due modalit di biopsia mammaria : quella chirurgica , fino ad oggi considerata il gold standard , e la pi recente tecnica effettuata mediante sistemi vuoto - assistiti . materiali e metodi popolazione di pazienti nel periodo di tempo compreso tra novembre 2008 e settembre 2009 abbiamo selezionato 200 pazienti che presentavano lesioni mammarie sospette ( microcalcificazioni , distorsioni parenchimali , formazioni nodulari , aree di enhancement ) da sottoporre a caratterizzazione istologica . 
le pazienti , informate adeguatamente riguardo entrambe le procedure bioptiche ed informate sulle modalit desecuzione delle stesse , sui benefici e sugli eventuali rischi ad esse connessi , hanno liberamente scelto a quale sottoporsi . 
 prima della procedura di biopsia percutanea mammaria tutte le pazienti sono state sottoposte ad esami ematochimici , al fine di valutare lassetto coagulativo , mentre alle pazienti candidate alla biopsia chirurgica , oltre alla valutazione dei parametri ematochimici , stato richiesto un esame radiografico del torace ed il consulto anestesiologico . 
per la scelta della guida strumentale , seppur basata sullindagine diagnostica che meglio consentiva di individuare la lesione , stata preferita quando possibile quella ecografica , sia per il costo minore che per la semplicit e rapidit nellesecuzione della procedura . 
la guida stereotassica stata riservata ai casi di microcalcificazioni , in cui stato sempre effettuato 542 radiol med ( 2012 ) 117 : 539557 vab , a nonmagnetic marker clip was released at the biopsy site at the end of the procedure . 
 in the 100 patients who opted for surgical diagnostic biopsy , the suspicious lesions were all subjected to wire localisation also under guidance of the modality that best visualised the lesions ; thus a hook wire ( a 12.5 - cm - long hawkins iii needle and medi - tech localisation wire , watertown , ma , usa ; or a 7 - cm - long kopans spring - hook localisation needle , cook , bloomington , in , usa ) was released under sonographic guidance in 36 cases and under stereotactic guidance in 59 cases . 
in five cases of lesions not visible on conventional imaging , a nonmagnetic wire was placed ( ghiatas beaded breast localization wire , bard , tempe , az , usa ) under mri guidance . 
one week after the biopsy procedure , all lesions diagnosed as malignant [ invasive carcinoma or ductal carcinoma in situ ( dcis ) ] or as adh underwent excisional biopsy with placement of a localisation wire under guidance of the modality that best visualised the lesion . 
 all patients in the study were followed up at 6 months with the imaging technique that had identified the initial lesion and with conventional mammography - us at 12 months ; mri was used only in cases in which it had identified the initial lesion . cost analysis to analyse costs incurred in performing the two procedures , we considered the total costs defined as the sum of fixed costs ( equipment and facilities ) and variable costs ( staff and supplies )  . 
a deterministic approach was followed , which assumes that costs are not patient - specific but equal for all patients : that is , all patients give rise to the same resource use . 
to calculate equipment cost per procedure , the annual depreciation rate was first calculated for the dedicated equipment , assuming that these devices have a mean life and hence depreciation time of 8 years . 
with regard to the nondedicated equipment ( us system and mri scanner ) , the annual depreciation rate was divided by the total number of hours of equipment use so that the rate allocated to biopsy was calculated on the basis of the number of hours or fractions of hours the equipment was used for biopsies . 
 nelle pazienti sottoposte a prelievo vab stato utilizzato il sistema vacora breast biopsy system ( tempe , az , usa ) avvalendosi dellausilio della guida strumentale ecografica in 30 / 100 reperti , stereotassica mammografica con apparecchio dedicato ( tavolo prono fischer mammotest plus / stm , fischer medical technologies , usa ) in 50 / 100 lesioni e rm in 20 / 100 casi poich si trattava di reperti non individuabili allimaging tradizionale . 
 le lesioni sospette nelle 100 pazienti che hanno scelto la biopsia chirurgica a fini diagnostici sono state tutte precedentemente sottoposte a procedura di reperage utilizzando anche in questo caso la guida strumentale che meglio consentiva di individuare la lesione e pertanto stato rilasciato un filo uncinato ( hawkins iii 12.5 cm needle and localization wire medi - tech , watertown , ma oppure kopas 7 cm springhook localizer needle cook , bloomington , in ) sotto guida strumentale ecografia in 36 / 100 casi e sotto guida stereotassica in 59 / 100 casi ; in 5 / 100 casi di reperti non individuabili allimaging tradizionale stato posizionato un filo amagnetico ( ghiatas beaded breast localization wire bard , temple , usa ) sotto guida rm ( 5 / 100 )  . 
dopo una settimana dalla procedura bioptica stata eseguita la biopsia escissionale di tutte le lesioni diagnosticate come maligne ( carcinoma invasivo o in situ , dcis ) o come iperplasia duttale atipica ( adh ) previo posizionamento di repere utilizzando anche in questo caso la guida strumentale che meglio consentiva lidentificazione della lesione . 
 il follow - up di tutte le pazienti che hanno partecipato allo studio stato effettuato a distanza di 6 mesi mediante lindagine strumentale che aveva consentito di individuare la lesione iniziale ed a 12 mesi con limaging convenzionale mammo - ecografico e mediante rm nei casi in cui il reperto era stato inizialmente individuato con tale metodica . 
 analisi dei costi per quanto riguarda lanalisi dei costi sostenuti per leffettuazione delle due procedure , considereremo i costi totali definiti come la somma dei costi fissi ( costo delle apparecchiature e degli spazi ) e dei costi variabili ( costo del personale e dei materiali )  . 
seguiremo un approccio deterministico iporadiol med ( 2012 ) 117 : 539557 aged in the national contract , then divided this cost by the number of weeks in a year , then by the weekly working hours under the contract ( radiologist 37.98 / h , nurse 24.66 / h , radiology technician 24.66 / h , nursing assistant 22.62 / h ) ; the resulting hourly cost was divided again by the number of minutes in an hour , giving the cost / minute . 
 supply costs included all materials used for each procedure ( from patient positioning to biopsy - site dressing ) and therefore included anaesthesia , pharmaceuticals , dressing material and other disposable items ( gloves , coats , caps , sterile drapes , containers , disposable scalpel , disposable kits )  . 
in particular , with regard to the vab system , the items considered included the 10 - gauge probe and the metal clips placed at the end of the procedure , as well as the metal wires for preoperative localisation . 
 quantitative analysis of the advantages of the two biopsy techniques another element that should not be underestimated when analysing the benefits of vab over surgical biopsy is the lower cosmetic and psychological impact . 
in order to evaluate cosmetic impact , scars were reviewed after 4 weeks and 6 and 12 months ; to evaluate psychological impact , patients were invited to fill in a questionnaire ( table 7 ) designed for us to assess which of the two procedures is better from a psychological point of view and in terms of resuming everyday activities . 
the analysis of cosmetic tizzando che i costi non siano paziente - specifici , ma uguali per tutti i pazienti nel senso che tutti i pazienti comportino un uguale uso di risorse . 
per calcolare il costo per procedura delle apparecchiature stata inizialmente calcolata la quota annuale di ammortamento per le apparecchiature dedicate ipotizzando che tali apparecchiature abbiano una vita media , e quindi un tempo di ammortamento , di 8 anni . 
per quanto riguarda , invece , le tecnologie di supporto ( ecografo , tavolo prono fischer mammotest plus / stm e tomografo per la guida rm ) , che non vengono utilizzate unicamente per leffettuazione delle biopsie , la quota di ammortamento annuale stata suddivisa per il numero complessivo di ore di utilizzo della apparecchiatura e quindi la quota da imputare alla biopsia stata calcolata in base alle ore o frazioni di ore di occupazione della macchina per leffettuazione della biopsia stessa . 
 per quanto concerne il costo del personale , esso si riferisce al costo delle unit di personale sanitario e tecnico , ( medico radiologo , infermiere , tecnico di radiologia e operatore tecnico addetto allassistenza ota ) , impiegato nella procedura . 
innanzitutto abbiamo calcolato il costo / minuto partendo dal costo annuo ( comprensivo di oneri diretti e riflessi ) di ciascuna qualifica professionale previsto nel contratto nazionale , dividendo tale costo per il numero di settimane di cui si compone lanno , quindi dividendo il costo settimanale cos ottenuto per lorario settimanale previsto da contratto il costo orario cosi ottenuto ( medico radiologo 37 , 98 euro / h , infermiere 24 , 66 euro / h , tecnico di radiologia 24 , 66 euro / h ed ausiliario ota 22 , 62 euro / h ) , stato diviso ancora per il numero di minuti in unora ottenendo in questo modo il costo / minuto . 
abbiamo quindi moltiplicato il costo / minuto per il tempo medio di impiego di ciascuna unit di personale nelle specifiche procedure valutato in base alla nostra esperienza ed abbiamo cos ottenuto il costo per singola figura professionale ed il costo complessivo del personale . 
 per quanto riguarda il costo del materiale di consumo , esso comprende tutto il materiale utilizzato per ogni singola procedura vab e / o chirurgica ( dal posizionamento della paziente alla fine della medicazione )  . 
in tale voce quindi compreso il costo dellanestesia , dei farmaci , del materiale di medicazione e di altro materiale monouso ( guanti , camici , cuffie , telini sterili , contenitori , bisturi monouso , nonch del kit monouso )  . 
in particolare per quanto concerne il sistema vab sono state prese in considerazione le voci relative alla sonda 10 gauge ed alle clip metalliche , posizionate a fine procedura vab , ed infine ai reperi metallici per il reperage prechirurgico in caso di intervento . 
i costi di tali materiali di consumo sono stati calcolati in base ai prezzi medi di listino . i dati relativi ai costi delle due procedure sono riportati nelle tabelle 13 . 
 total variable costs total stereotactic guidance system costs mri guidance technologies ( fixed costs ) : total fixed costs provider team ( variable costs ) : radiologist nurse radiology technician nursing assistant supplies 10 - g cannula , disposable kit nonmagnetic radiopaque clip anaesthesia , dressing material , etc . 
la frequenza di sottostima ( fsadh = numero casi carcinoma infiltrante + numero casi carcinoma in situ / numero casi adh ; fs.dcis = numero casi carcinoma infiltrante / numero casi carcinoma in situ ) indica il numero di casi sul totale in cui la diagnosi istologica stata meno grave rispetto a quella rilevata allintervento chirurgico , in particolare per quanto riguarda ladh e il dcis . 
nelle tabelle 4 e 5 sono riportati i dati necessari per calcolare gli indicatori di efficacia mentre la tabella 6 mostra i valori delle misure di efficacia prese in considerazione . 
 analisi quantitativa dei benefici delle due biopsie un altro elemento che non bisogna sottovalutare quando si analizzano i vantaggi dei sistemi vacuum assisted rispetto alla biopsia chirurgica sono la minor invasivit estetica e psicologica . 
per valutare linvasivit estetica stata effettuata unanalisi della cicatrice dopo 4 settimane , 6 e 12 mesi mentre per valutare linvasivit psicologica stato fatto compilare alle pazienti un questionario , riportato nella tabella 7 che si pone lobiettivo di valutare se la procedura vab , rispetto alla biopsia chirurgica offre anche vantaggi dal punto di vista psicologico e di ritorno alla vita di tutti i giorni dopo lintervento . 
per quanto concerne lanalisi del danno estetico ci siamo basati sulla valutazione delle cicatrici cutanee secondo la formula creso , usata in medicina - legale , la quale prevede lo studio di 5 parametri : colore ( c ) ( isocromia , discromia , ipercromia ) ; rilievo ( r ) ( cicatrice piana , ipertrofica , ipo - atrofica ) ; estensione ( e ) ( cm ) ; sede ( s ) ( regione mammaria ) ; orientamento ( o )  . ad ognuno di questi elementi si attribuisce un valore numerico che porta ad un punteggio cicatriziale ( pc ) , che assume valori compresi tra 0 e - 100 e che viene poi tradotto in valore di danno biologico ponderato ( per fini risarcitori ) tenendo anche conto di variabili individuali quali : lo stato antecedente allatto medico , let , il sesso , leventuale trattamento correttivo . pc = c + r / 2 + e + s + o ( 1 ) per quanto riguarda invece le implicazioni psicologiche legate alla procedura vab o allintervento chirurgico , tramite la compilazione del questionario riportato nella tabella 8 abbiamo voluto indagare i vari aspetti emotivi . 
il questionario prevede 6 domande a cui rispondere assegnando un punteggio da 1 a 3 ( 1 = per niente , 2 = abbastanza , 3 = molto )  . 
le prima e la terza domanda riguardano rispettivamente lemotivit rispetto alle possibili complicanze e lefficacia della procedura ; la seconda domanda riguarda lansia creata dalla permanenza in ospedale ; la quinta domanda riguarda la preoccupazione di non poter riprendere subito le attivit quotidiane mentre lultima domanda riguarda lansia per laspetto estetico . radiol med ( 2012 ) 117 : 539557 table 8 costs and incremental efficacy 552 e , adh underestimation e , dcis underestimation e , re - biopsy surgical biopsy vs . 
vacora 509 , 4 - 0 , 017 0 , 05 - 0 , 02 dcis , carcinoma duttale in situ ; adh , iperplasia atipica ; sott , sottostima ; c , costo ; e , efficacia risultati efficacia as for the psychological implications of vab or surgery , the questionnaire in table 8 is designed to investigate various emotional aspects . 
the first and third statements concern emotions regarding possible complications and the effectiveness of the procedure ; the second concerns anxiety related to hospitalisation ; the fifth regards resuming everyday activities immediately ; whereas the sixth regards cosmesis . results efficacy data regarding the efficacy of the vab procedures showed the following results : all biopsy procedures were completed successfully without significant perior postprocedural complications and allowing , in most cases , sampling of at least 12 tissue cores ; in a minority of cases , however , the number of cores was restricted to five due to bleeding . 
histological diagnoses for the 100 vab lesions were invasive carcinoma in 26 ( 26% ) , dcis in 13 ( 13% ) , adh in eight ( 8% ) and benign lesion in 53 ( 53% )  . 
one of the 13 lesions diagnosed as dcis on vab turned out to be invasive carcinoma on excisional biopsy , whereas a lesion diagnosed as adh turned out to be carcinoma in situ . 
in two cases diagnosed as infiltrating carcinoma on vab , measuring < 5 mm , no fiper quanto riguarda i dati relativi allefficacia delle procedure vab sono stati ottenuti i seguenti risultati : tutte le procedure bioptiche eseguite sono state portate a termine con successo ovvero senza significative complicanze perie post - procedurali consentendo nella maggior parte dei casi il prelievo di almeno 12 frustoli di tessuto ; in alcuni casi tuttavia , linsorgenza di sanguinamento ha consentito di ottenere un minimo di 5 frustoli . 
la diagnosi istologica al prelievo vab stata in 26 / 100 lesioni di carcinoma invasivo ( 26% ) , in 13 / 100 lesioni di carcinoma in situ dcis ( 13% ) , in 8 / 100 lesioni di iperplasia duttale atipica adh ( 8% ) ed in 53 / 100 lesioni di benignit ( 53% )  . 
una delle 13 lesioni diagnosticate come dcis alla vab si rivelata un carcinoma invasivo alla biopsia escissionale ed una lesione diagnosticata come adh risultata invece trattarsi di carcinoma in situ . 
per due casi diagnosticati alla vab come carcinoma infiltrante delle dimensioni inferiori ai 5 mm non stato possibile avere un riscontro istologico definitivo , in quanto le lesioni sono state totalmente asportate durante la procedura vab . 
tutte le lesioni diagnosticate come benigne alla diagnosi istologica dei frustoli asportati sotto guida ecografica e stereotassica ( 45 / 100 ) sono state inserite in un programma di follow - up mammo - ecografico ogni 6 mesi e si per tutte confermata la non evolutivit allimaging . 
le lesioni caratterizzate come benigne alla diagnosi istologica su frustoli asportati sotto guida rm ( 8 / 100 ) , sono state rivalutate con esame rm dinamico dopo 1 settimana dalla procedura . 
in 5 / 8 casi stato riscontrato un enhancement radiol med ( 2012 ) 117 : 539557 table 9 questionnaire results questions answers ( n ) surgical biopsy ( % ) vab ( % ) tabella 9 risultati questionario risposte ( n ) pazienti chirurgia ( % ) pazienti vab ( % ) question 1 question 2 question 3 question 4 question 5 question 6 domanda domanda 1 domanda 2 domanda 3 domanda 4 domanda 5 domanda 6 nal histological diagnosis could be obtained , as the lesions were completely removed during the procedure . 
all lesions diagnosed as benign on histology of the cores obtained under us and stereotactic guidance ( 45 / 100 ) were referred for mammography / us follow - up every 6 months and were all confirmed to remain stable on imaging . 
lesions characterised as benign on histological diagnosis using cores obtained under mri guidance ( 8 / 100 ) were re - evaluated residuo , mentre nei 3 / 8 casi rimanenti non era pi visibile lenhancement . 
 in the 100 patients referred for surgical biopsy the following histological results were obtained : 24 invasive carcinoma ( 24% ) , 14 dcis ( 14% ) , 6 adh ( 6% ) and 56 benign lesions ( 56% )  . 
at follow - up , in one case of microcalcifications located in a previous surgical scar , mammography at 12 months demonstrated an increase in number ; the patient underwent a second biopsy procedure , and the histological diagnosis was dcis . 
in one case of a lesion detected under mri guidance , 6 - month follow - up documented an area of residual enhancement : the patient was sent for surgical re - biopsy , and histology was negative for malignancies or atypia . cost - effectiveness analysis having determined the costs and efficacy ( tables 2 , 3 and 6 ) of the two breast biopsy techniques , a cost - effectiveness analysis was conducted . 
data in table 8 show that if efficacy is measured in terms of dcis underestimation or of re - biopsy , there is a clear superiority of the vacora vab technique compared with conventional surgery in that the vacora system has greater efficacy and is less costly . 
as a result , we can state that the vab system is superior to conventional surgical biopsy on the grounds of its lower costs and greater efficacy in two out of the three intermediate measures of efficacy considered . 
 qualitative analysis as for scar appearance , the 4 - week review of all patients showed that the 100 women who underwent vab had no scar ; on the other hand , 85 of the 100 surgical biopsy patients had a 3to 4 - cm normotrophic pink scar , seven had a hypertrophic and hyperchromatic scar , three had a hypoatrophic and dyschromic scan , and the remaining patients had a retracting scar . 
 nei casi sottoposti a biopsia chirurgica sono stati ottenuti i seguenti risultati istologici : 24 / 100 casi di carcinomi invasivi ( 24% ) , 14 / 100 casi di carcinoma in situ dcis ( 14% ) , 6 / 100 casi di iperplasia duttale atipica adh ( 6% ) ed in 56 / 100 casi il riscontro stato di benignit ( 56% )  . 
nei controlli di follow - up in un caso di microcalcificazioni localizzate in corrispondenza della cicatrice di pregresso intervento chirurgico , il controllo mammografico a 12 mesi ne ha evidenziato un incremento numerico e la paziente stata quindi sottoposta a rebiopsia : la diagnosi istologica stata di dcis . 
in un caso di lesione evidenziata sotto guida rm il follow - up a 6 mesi ha documentato unarea di enhancement residua : la paziente stato sottoposta a rebiopsia chirurgica e listologico stato negativo per patologia maligna e per atipie . analisi costo - efficacia avendo determinato i costi e lefficacia ( tabelle 2 , 3 e 6 ) delle due modalit di biopsia della mammella , possiamo ora procedere nelleffettuare unanalisi costo - efficacia . 
dai dati riportati nella tabella 8 si nota come , se misuriamo lefficacia in termini di sottostima di dcis o di rebiopsia , siamo in presenza di un chiaro caso di dominanza della tecnica con vacora rispetto alla tecnica chirurgica tradizionale , presentando il vacora maggior efficacia e minor costi . 
quindi possiamo dire che il sistema di biopsia vacuum assisted domina il sistema di biopsia classica chirurgica , nel senso che comporta minori costi e maggiore efficacia , nel caso di due su tre delle misure di efficacia intermedie analizzate . 
 analisi qualitativa per quanto riguarda laspetto cicatriziale , osservando a distanza di 4 settimane tutte le pazienti abbiamo potuto notare come le 100 donne sottoposte al vab non presentavano nessuna sequela cicatriziale cutanea mentre delle 100 pazienti andate incontro a biopsia chirurgica , 85 mostravano una cicatrice rosea , normotrofica , di 34 cm , in 7 pazienti la cicatrice si presentava ipertrofica e ipercromica , in 3 casi era ipoatrofica e discromica e nei restanti retraente . 
inoltre al fine di valutare lalterazione strutturale parenchimale abbiamo sottoposto tutte le 200 pazienti ad un follow - up mammografico a distanza di 612 mesi dal quale risultato che le donne che avevano subito biopsia chirurgica mostravano la presenza di distorsioni strutturali nella sede dellintervento , mentre nessun reliquato risultava in coloro che avevano scelto la procedura vab . 
dai risultati ottenuti dalla compilazione del questionario ( tabella 9 ) abbiamo potuto evincere che le maggiori differenze tra i due gruppi di pazienti riguardano la paura delle complicanze post - procedurali , il radiol med ( 2012 ) 117 : 539557 mal changes , all 200 patients underwent mammography at 612 months , which showed structural distortions at the biopsy site in women who underwent surgical biopsy and no sequelae in those who opted for vab . 
questionnaire results ( table 9 ) revealed that the main differences between the two groups were fear of postprocedure complications , distress related to the hospital environment and cosmetic consequences . 
 discussion in the past , diagnosis of suspicious breast lesions was obtained with a strategy of watchful waiting with frequent examinations or , in more suspicious cases , diagnostic excisional biopsy [ 9 ]  . 
although always considered the gold standard for histological characterisation of suspicious lesions , surgical biopsy is perceived by patients as an invasive procedure from the psychological and cosmetic point of view [ 9 , 10 ]  . 
compared with conventional biopsy with tru - cut needles , vab provides reduced sampling errors due to needle displacement on insertion or incorrect placement relative to the lesion , especially when the lesion is small . 
the results indicate that compared with surgical biopsy , vab is not only cost effective , as shown by two of three efficacy indicators , but also less invasive from a cosmetic and psychological point of view . 
this suggests that the new biopsy systems are good alternatives in terms of cost - effectiveness compared with surgical biopsy , a procedure considered the gold distress psicologico relativo allambiente ospedaliero e le conseguenze estetiche ; in tutti questi ambiti , la biopsia vab fornisce indubbiamente un miglior conforto psicologico . 
 discussione in passato linquadramento diagnostico di lesioni mammarie sospette si eseguiva mediante lattuazione di una strategia di attesa con controlli ravvicinati o in alternativa , nei casi di maggior sospetto , mediante la biopsia escissionale a fini diagnostici [ 9 ]  . 
la biopsia chirurgica , seppur da sempre considerata il gold standard nella caratterizzazione istologica di lesioni sospette , ritenuta dalle pazienti una procedura invasiva sia da un punto di vista psicologico che estetico [ 9 , 10 ]  . 
negli ultimi decenni , quindi , grazie al continuo sviluppo tecnologico , sono stati introdotti sul mercato , e successivamente nella pratica clinica , innovativi sistemi di biopsia mammaria mini - invasiva . 
dai dati riportati in letteratura [ 12 ] , tra le metodologie di prelievo che si sono affermate , i sistemi vacuum assisted hanno permesso di ottenere i migliori risultati sia in termini di efficacia diagnostica che di tollerabilit da parte delle pazienti . 
rispetto alla core biopsy , tali tecnologie consentono infatti di ottenere frustoli integri , di ottima qualit dal punto di vista interpretativo da parte dellanatomo - patologo grazie soprattutto alle loro maggiori dimensioni ( con peso fino a 0 , 17 g ) ; rispetto ai convenzionali prelievi con aghi di tipo tru - cut il sistema ad aspirazione vuoto - assistita permette di ridurre lerrore da campionamento dovuto allo spostamento dellago durante lintroduzione allinterno della mammella o al suo non corretto posizionamento rispetto alla lesione , soprattutto qualora di piccole dimensioni , con conseguente sensibile riduzione dei valori di sottostima ( approssimativamente tra 1% e 6% ) ed aumento dellaccuratezza diagnostica [ 1315 ]  . 
 lanalisi da noi svolta ha evidenziato i vantaggi delle procedure vab , rispetto alla biopsia chirurgica , sia in termini di costo - efficacia che in termini di minor invasivit estetica e psicologica [ 16 , 17 ]  . 
i risultati ottenuti evidenziano che rispetto alla biopsia chirurgica le procedure vab risultano oltre che costo - efficaci , con riferimento a due dei tre indicatori di efficacia utilizzati , anche meno invasive dal punto di vista estetico e pi accettabili psicologicamente . 
i costi complessivi delle due procedure sono invece stati definiti come la somma dei costi fissi ( apparecchiature e occupazione spazi ) e dei costi variabili ( costo del personale e dei materiali )  . 
questo ci porta a poter affermare che i nuovi sistemi di biopsie possono essere considerati una buona alternativa , in termini di costo efficacia , alla biopsia chirurgica , procedura fino ad oggi considerata il gold standard nella tipizzazione di lesioni mammarie so556 radiol med ( 2012 ) 117 : 539557 standard for characterising suspected breast lesions . 
economic analysis also showed that vab procedures had significantly lower costs than did surgery ( tables 2 and 3 ) : costs of operating theatre are reduced , and staff employed is minimised . 
in addition , given the small size of the suspicious lesions being detected as a result of the greater awareness of women who spontaneously undergo imaging tests and the growing diffusion of screening programmes the surgical procedure increasingly requires preoperative wire localisation . 
although on one hand this increases the cost of surgical biopsies , on the other , considering that there is no difference in technique between wire localisation and minimally invasive biopsies , it further supports the desirability of obtaining adequate material for histological characterisation in the same session . the analysis also shows that the majority of suspicious lesions undergoing histological characterisation are benign and therefore do not require complete excision . 
the possibility of choosing a minimally invasive biopsy procedure means , for patients , avoiding the psychological / physical discomfort related to surgery ( table 9 ) and , for physicians , the possibility of referring for therapeutic surgery only patients with a confirmed diagnosis of malignancy . 
in addition , restricting the use of surgery to cases in which it is really necessary may contribute to shortening preoperative waiting lists when waiting times are long . with reference to the population being studied , vab proved to be more effective than surgical biopsy on the basis of two of three efficacy indicators . 
per quanto concerne il danno estetico le procedure vab hanno evidenziato assenza di sequele cicatriziali cutanee ( incisione di circa 3 mm ) e minima fibrosi parenchimale post - cicatriziale residua . 
 lanalisi delle implicazioni psicologiche delle procedure vab , sviluppata tramite la compilazione di un questionario da parte delle pazienti , ha invece evidenziato scarsa sintomatologia dolorosa nel post - operatorio e minimi tempi di ripresa della normale attivit quotidiana . 
dallanalisi economica , inoltre , emerso che le procedure vab , rispetto alle procedure chirurgiche , rappresentano anche unimportante riduzione dei costi ( tabelle 2 e 3 ) : si abbattono i costi della sala operatoria , si minimizza il personale impiegato . 
tra laltro , in considerazione delle minime dimensioni delle lesioni sospette individuate attualmente , anche per la maggior sensibilizzazione delle donne che si sottopongono spontaneamente a controlli strumentali per la maggiore diffusione di programmi di screening , la procedura chirurgica richiede sempre pi spesso il ricorso al reperaggio pre - chirurgico . 
 questo , se da un lato contribuisce ad un aumento dei costi dellintervento , dallaltro , dato che la modalit di localizzazione per il posizionamento del filo di repere non differisce da quella di biopsia mininvasiva , rende ancora pi evidente quanto possa essere preferibile poter contestualmente ottenere materiale idoneo per la caratterizzazione istologica . lanalisi svolta evidenzia ancora che il maggior numero di lesioni sospette sottoposte a caratterizzazione istologica sono benigne e quindi non necessitano di essere completamente asportate . 
poter ricorrere ad una procedura di biopsia mini - invasiva significa , allora , per le pazienti , non incorrere nello stress psicofisico legato allintervento ( tabella 9 ) e candidare solo le pazienti con diagnosi accertata di patologia maligna allintervento chirurgico a fini terapeutici . 
tra laltro , razionalizzando ai soli casi necessari il ricorso alla chirurgia potrebbe permettere , in casi in cui ci siano lunghi tempi di attesa , di smaltire le liste pre - operatorie e di attesa . possiamo allora concludere che , con riferimento al campione considerato , in termini di due dei tre indicatori di efficacia utilizzati , la modalit bioptica vab rispetto a quella chirurgica presenta maggior efficacia . 
 la biopsia vacuum assisted comporta anche , rispetto alla biopsia chirurgica , vantaggi estetici , immediato ritorno alla normale attivit quotidiana e riduzione dello stress psicofisico legato alla minore invasivit . 
katonis1 1department of orthopaedics , university of crete , crete , greece 2department of radiology , university of aberdeen , scotland , u.k. 3dipartimento di ortopedia , istituto ortopedico rizzoli , via pupilli 1 , 40136 bologna , italy 4first department of orthopaedics , attikon general university hospital , athens university medical school , athens , greece 5department of radiology , university of crete , crete , greece correspondence to : a . 
dimitriadis , tel : + 30 - 6973313476 , fax : + 30 - 28210 - 86666 , e - mail : anastasiodimitriadis@msn.com received : 10 january 2011 / accepted : 26 april 2011 / published online : 18 november 2011 springer - verlag 2011 abstract purpose . 
using open upright magnetic resonance ( mr ) imaging , we prospectively studied changes in lumbar lordosis and intervertebral discs of 25 elite long - distance runners in two sitting postures ( neutral and extended ) before and after 1 h of running and compared the results with disc height and dehydration / degeneration . 
after 1 h of running , mean lordosis in neutral posture reduced by 4 ; reduction was significant in runners with a history of low back paa significant reduction in mean lordosis in extension was not observed . 
utilizzando una risonanza magnetica ( rm ) aperta in ortostatismo , sono stati studiati prospettivamente i cambiamenti della lordosi lombare di 25 corridori professionisti nelle lunghe distanze , prima e dopo unora di corsa , nella posizione seduta neutra e in quella estesa confrontando i risultati con laltezza e la disidratazione / degenerazione dei dischi intersomatici . 
dopo unora di corsa , si osservata una riduzione statisticamente significativa della lordosi nei corridori con unanamnesi positiva per lombalgia con un valore medio di 4 gradi mentre non si osservata una riduzione significativa dei valori medi in estensione . 
 laltezza media dei dischi intersomatici si ridotta in modo statisticamente significativo in entrambe le posizioni mentre non si osservata una differenza statisticamente significativa fra i corridori con anamnesi positiva per lombalgia e quelli con anamnesi negativa . 
riduzioni variabili dellidratazione dei dischi sono state osservate in 23 corridori ( 57 dischi ) , pi frequentemente a carico del disco l5 - s1 , non si osservata per una differenza radiol med ( 2012 ) 117 : 654668 to low back pain and degenerative disc disease . 
i corridori , in particolare quelli con unanamnesi positiva per lombalgia e patologia degenerativa discale , dovrebbero essere valutati dopo gli allenamenti per preservare la normale lordosi lombare . parole chiave rachide lombare rm aperta in ortostatismo rachide lombare lordosi corridori introduction introduzione variable changes may occur in the lumbar spine of athletes due to repetitive and increased spinal strain during physical training [ 13 ]  . 
these changes include alterations in intervertebral disc - space height [ 4 , 5 ] , intradiscal pressure and dehydration [ 4 , 6 , 7 ] and alignment of the spine [ 811 ] and may significantly predispose the athlete to a higher incidence of low back pain [ 13 ] and degenerative disc disease ( 75% ) compared with nonathletes ( 31% ) of the same age [ 1 , 4 , 5 , 12 ]  . 
some authors reported a relationship between posture and increased intradiscal pressure in flexion [ 6 , 7 , 13 , 14 ] and increased disc height in extension [ 8 ]  . 
larger flexion angles imposed significantly higher risk of lumbar spine injury by increasing intradiscal pressure , annulus fibrosus strains and ligamentous and facet - joint forces [ 9 ]  . 
 however , although decreased lordosis may predispose to increased incidence of low back pain [ 11 , 15 ] , some studies found no change in lumbar sagittal alignment during axial spinal loading , although they found significant decrease in disc height at l4l5 [ 16 ]  . 
it seems possible that changes in lumbar sagittal alignment secondary to postural changes and the load carried from intense training and athletic activities may predispose to a higher incidence of low back pain and disc dehydration [ 24 , 9 , 10 , 1721 ]  . 
however , can these changes be related to long - term development of permanent intervertebral disc changes and degenerative disc disease ? is it possible that repeat changes in lumbar sagittal alignment may predispose to these changes in athletes ? we performed an in vivo study using an open upright magnetic resonance ( mr ) imaging scanner to evaluate changes in lumbar lordosis and intervertebral discs in elite long - distance road - running athletes after 1 h of running and to assess the relationship between these changes and diversi cambiamenti possono verificarsi nel rachide lombare degli atleti a causa di maggiori e ripetitive sollecitazioni durante gli allenamenti diversi cambiamenti possono verificarsi nel rachide lombare degli atleti [ 13 ]  . 
questi cambiamenti includono alterazioni dellaltezza dei dischi intervertebrali [ 4 , 5 ] , della pressione intradiscale , dellidratazione [ 4 , 6 , 7 ] e dellallineamento del rachide lombare [ 811 ] ; ci pu significativamente predisporre ad una pi elevata incidenza di lombalgia [ 13 ] e degenerazione discale negli atleti ( 75% ) rispetto a non atleti ( 31% ) della stessa et [ 1 , 4 , 5 , 12 ]  . 
alcuni autori riportano una correlazione fra la postura e laumentata pressione intradiscale in flessione [ 6 , 7 , 13 , 14 ] e laumentata altezza dei dischi intervertebrali in estensione [ 8 ]  . 
pi ampi angoli di flessione impongono un rischio aumentato di lesioni del rachide lombare determinati dallaumentata pressione intradiscale , da sollecitazioni nei confronti del cercine fibroso , forzatura dei legamenti e delle articolazioni faccettali [ 9 ]  . 
comunque , sebbene la riduzione della lordosi pu predisporre ad un pi alto rischio di lombalgia [ 11 , 15 ] , altri studi , nonostante abbiano evidenziato una significativa riduzione del disco intervertebrale l4 - l5 durante il caricamento assiale , non hanno trovato alcun cambiamento nellallineamento sagittale del rachide [ 16 ]  . 
sembra possibile che i cambiamenti dellallineamento sagittale del rachide lombare secondari ai cambiamenti posturali e il carico derivante da un intenso allenamento possano predisporre ad una pi alta incidenza di lombalgia e disidratazione dei dischi intervertebrali negli atleti [ 24 , 9 , 10 , 1721 ]  . 
seventeen runners had a history of low back pain and combined mr imaging findings of lumbar degenerative disc disease in 56 intervertebral discs ; the remaining eight runners had no history of low back pain or mr imaging findings of degenerative disc disease . 
all runners gave written informed consent to be included in this study , which was approved by the institutional review board / ethics committee of the authors institutions . mr imaging of the lumbar spine was obtained in the sitting posture in neutral and extension of the lumbar spine prior to and immediately after 1 h of running . 
 changes in lumbar sagittal alignment , disc height and dehydration / degeneration were recorded in both postures belogie degeneratiea discali ? possibile che tali cambiamenti negli atleti possano essere predisposti da ripetute variazioni dellallineamento sagittale del rachide lombare ? abbiamo effettuato in vivo uno studio con lausilio di una risonanza magnetica ( rm ) aperta in ortostatismo per valutare le variazioni della lordosi lombare e dei dischi intervertebrali in corridori professionisti nelle lunghe distanze dopo unora di corsa con lintento di valutare la relazione fra questi cambiamenti e la patologia degenerativa discale in corridori con e senza anamnesi positiva per lombalgia . 
 diciassette corridori avevano unanamnesi positiva per lombalgia e la rm ha evidenziato nel rachide lombare la degenerazione di 56 dischi intervertebrali ; i restanti 8 corridori non avevano anamnesi positiva per lombalgia o riscontri alla rm di patologia degenerativa discale . 
1 posizione seduta neutra ( sinistra ) ed estesa ( destra ) sono state studiate in una rm aperta in ortostatismo . radiol med ( 2012 ) 117 : 654668 fore and after 1 h of running . 
disc height was measured using the dabbs and dabbs method , which is the sum of anterior and posterior disc heights divided by two ; the total and mean height of the lumbar discs was calculated [ 23 ]  . 
 disc dehydration / degeneration was graded using previously reported criteria and signal intensity on mr imaging [ 24 26 ] : grade 1 ( mild degeneration , slight decrease in signal intensity of the nucleus pulposus on sagittal t2 - weighted mr images ) ; grade 2 ( moderate degeneration , hypointense nucleus pulposus on t2 - weighted mr images with normal disk height ) ; grade 3 ( severe degeneration , hypointense nucleus with disk - space narrowing )  . 
a disc was regarded as being hydrated if more than two thirds of it was hyperintese in t2 - weighted images and dehydrated if more than two thirds was hypointense [ 26 ]  . statistical analysis of the measurements of lordosis and mean total disc height before and after 1 h of running was performed using the chi - squared test ; a p value < 0.05 was considered an expression of significant results . 
however , by direct comparison of disc - height reduction in runners with and without a history of low back per almeno 1 ora ( una distanza maggiore di 10 km )  . 
questo studio stato approvato da institutional review board / comitato etico degli istituti degli autori . le immagini di rm del rachide lombare sono state ottenute nella posizione seduta neutra ed estesa , prima e subito dopo 1 ora di corsa . 
laltezza dei dischi intervertebrali stata effettuata mediante il metodo di dabbs e dabbs , ovvero la somma delle altezze posteriori ed anteriori poi divisa per due ; si viene cos a calcolare il totale delle altezze e laltezza media [ 23 ]  . 
 la disidratazione / degenerazione dei dischi intervertebrali stata classificata , con lausilio dei criteri precedentemente riportati e dellintensit di segnale alla rm [ 2426 ] , su di una scala : grado 1 ( minima degenerazione ; lieve diminuzione dellintensit di segnale del nucleo polposo alle immagini di rm pesate in t2 con una normale altezza del disco ) , grado 2 ( moderata degenerazione ; ipointensit del nucleo polposo alle immagini di rm pesate in t2 ) , grado 3 ( severa degenerazione ; ipointensit del nucleo associata ad una riduzione in altezza del disco )  . 
un disco stato considerato idratato se pi dei due terzi risultavano iperintensi nelle immagini pesate in t2 , di converso disidratati se pi dei due terzi risultavano ipointensi nelle immagini pesate in t2 [ 26 ]  . lanalisi statistica delle misurazioni della lordosi lombare e dellaltezza media dei dischi intervertebrali prima e dopo 1 ora di corsa stata eseguita per mezzo dellutilizzo del test del chi - quadro ; un valore di p < 0 , 05 stato considerato espressione di significativit statistica . 
possible mechanism contributing to these changes may be the prolonged loading of the spine in an altered sagittal alignment [ 810 ]  . there have been a number of definitions regarding the normal range of lumbar lordosis ranging from 18 to 79 [ 27 , 28 ]  . 
non stata osservata in alcuna posizione una differenza statisticamente significativa nella riduzione dellaltezza dei dischi intervertebrali tra i corridori con anamnesi positiva per lombalgia e i corridori con anamnesi negativa ( neutra , p = 0 , 822 ; estesa , p = 0 , 237 )  . 
tuttavia , dal confronto diretto fra la riduzione dellaltezza dei dischi intervertebrali nei corridori con anamnesi positiva per lombalgia e nei corridori con anamnesi negativa , emerso come sia pi alta nei pazienti con anamnesi positiva in entrambe le posizioni ( 5 , 082 mm nei corridori con anamnesi positiva per lombalgia mentre 4 , 693 mm nei corridori con anamnesi negativa )  . diversi gradi di disidratazione / degenerazione sono stati osservati dopo 1 ora di corsa in 23 corridori ( 57 dischi intervertebrali ) ; 16 / 17 avevano unanamnesi positiva per lombalgia mentre 7 / 8 avevano unanamnesi negativa per lombalgia ( tabella 1 )  . 
3a - d midsagittal t2 - weighted mr images of lumbar spine in neutral sitting posture in a 36 - year - old man ( runner 12 ) with a history of low back pain a before and b after 1 h of running ; lumbar lordosis is reduced by 31 . 
3a - d immagini di rm medio - sagittali pesate in t2 del rachide lombare di una donna di 36 anni ( corridore 12 ) con anamnesi positiva per lombalgia nella posizione seduta neutra prima ( a ) e dopo ( b ) 1 ora di corsa ; la lordosi lombare si ridotta di 31 gradi . 
immagini di rm medio - sagittali pesate in t2 del rachide lombare dello stesso corridore in estensione prima ( c ) e dopo ( d ) 1 ora di corsa ; la lordosi lombare non cambiata . to adulthood shows a gradual increase of lumbar lordosis in response to increasing body weight and spinal loading in the standing posture [ 2830 ]  . 
as the human body grows , curvatures increase to resist the increased loads ; lumbar lordosis seems to be the most important factor in maintaining neutral sagittal balance of the spine [ 8 , 17 , 31 ]  . 
non stata osservata una differenza statisticamente significativa tra le variazioni dei dischi intervertebrali tra i corridori con anamnesi positiva per lombalgia e i corridori con anamnesi negative 660 radiol med ( 2012 ) 117 : 654668 fig . 
la differenza statisticamente significativa nei pazienti con lombalgia ( p = 0 , 036 )  . age , the body cannot keep the normal lumbar lordosis and starts to decrease the lumbar curvature [ 29 , 30 , 32 ] ; patients > 40 years of age show a tendency for a more vertical sagittal alignment that is not associated with increase in thoracic or thoracolumbar kyphosis [ 29 ]  . 
tuttavia , dal confronto diretto fra il numero di dischi di grado 2 e 3 per disidratazione / degenerazione , questo stato pi elevato nei corridori con anamnesi positiva per lombalgia ( 31 dischi intervertebrali nei corridori con anamnesi positiva per lombalgia mentre 5 dischi intervertebrali nei corridori con anamnesi negativa per lombalgia )  . discussione precedenti studi hanno suggerito che significative variazioni si verificano nel rachide lombare come risultato di una sollecitazione indotta dallesercizio [ 2 , 4 , 5 ]  . 
il grafico mostra la rappresentazione della lordosi lombare in posizione neutra e in estensione prima e dopo 1 ora di corsa . tion reverses ; the hip abducts and the pelvis elevates to obtain foot clearance . 
this nearly reciprocal motion combined with slight lumbopelvic motion minimises shoulder and head movement and is one of the most important mechanisms for decoupling the intense lower - extremity motion from the trunk and head , allowing balance and equilibrium to be maintained [ 35 ]  . 
in addition , during normal running - gait cycle , the body maintains a forward lean [ 33 ] , and pelvic motion is minimised to conserve energy and maintain efficiency in running . 
however , excessive pronation of the foot , internal rotation of the tibia and femur , patellofemoral maltracking and pelvic abnormalities such as excessive anterior and lateral tilt , are observed frequently in runners and may lead to improper alignment of the lumbar spine and acute or chronic injury [ 33 ]  . there is previous evidence indicating a relationship between the posture of the lumbar spine and spinal loading , which may contribute to the pathogenesis of intervertebral disc disease [ 68 , 2830 ]  . 
mr imaging positional studies in healthy individuals measured increased intradiscal pressure during spinal loading in flexion [ 6 , 7 ] and increased disc height ( 1.1 mm ) from flexion to extension of the trunk in the supine posture [ 8 ]  . 
others observed that mechanical loading of the lumbar spine increases in a positive linear correlation from standing posture to forward bending [ 9 , 10 ] and showed that sitting posture causes the spine to lose height due to compression and grip of the intervertebral discs and postural change [ 36 ] ; lordotic posture results in less back pain than does kyphotic posture [ 11 ]  . 
un possibile contributo a queste variazioni potrebbe essere il carico prolungato sul rachide in una condizione di alterato allineamento sagittale [ 810 ]  . diverse sono state le definizioni riguardo il normale intervallo di lordosi lombare con un range da 18 a 79 gradi [ 27 , 28 ]  . 
il rachide mostra dalla fanciullezza allet adulta un graduale incremento della lordosi lombare in risposta allaumento del peso corporeo e al carico sulla colonna nella posizione eretta [ 2830 ]  . 
di pari passo alla crescita corporea si assiste allaumento delle curvature per resistere ai carichi aumentati ; la lordosi lombare sembra essere il pi importante fattore nel mantenere neutro il bilancio della colonna vertebrale [ 8 , 17 , 31 ]  . 
ad unet critica , il corpo non pu mantenere la normale lordosi lombare inizia a decrescere la curvatura lombare [ 29 , 30 , 32 ] ; pazienti oltre i 40 anni mostrano una tendenza ad un maggior allineamento verticale non associato ad aumentate cifosi toraciche o toracolombari [ 29 ]  . la corretta biomeccanica della corsa coinvolge il sincronismo dei movimenti di tutte le componenti della catena cinetica ; i corridori richiedono molto di pi dalle articolazioni e dai muscoli che i camminatori [ 33 ]  . 
7a - d midsagittal t2 - weighted mr images of the lumbar spine in a 33 - year - old woman ( runner 6 ) without a history of low back pain in sitting neutral posture a before and b after 1 h of running show 7.65 - mm total disc height reduction after running . 
7a - d immagini di rm medio - sagittali pesate in t2 del rachide lombare di una donna di 33 anni ( corridore 6 ) con anamnesi negativa per lombalgia nella posizione seduta neutra prima ( a ) e dopo ( b ) 1 ora di corsa mostrano una riduzione di 7 , 65 mm dopo la corsa . 
immagini di rm medio - sagittali pesate in t2 del rachide lombare dello stesso corridore in estensione prima ( c ) e dopo ( d ) 1 ora di corsa mostra una riduzione totale dellaltezza dei dischi di 5 , 6 mm dopo la corsa . 
in that study , the electromyographic activity of the erector spinal muscles increased in flexion , ciproco combinato con il minimo movimento lombopelvico minimizza il movimento di spalle e testa , ed uno dei pi importanti meccanismi di sdoppiamento dellintenso movimento delle estremit inferiori dal tronco e dalla testa , e perradiol med ( 2012 ) 117 : 654668 fig . 
8a - d midsagittal t2 - weighted mr images of the lumbar spine in a 41 - year - old man ( runner 15 ) with a history of low back pain taken in neutral sitting posture a before and b after 1 h of running show 8.2 - mm total disc height reduction after running . 
8a - d immagini di rm medio - sagittali pesate in t2 del rachide lombare di una donna di 41 anni ( corridore 15 ) con anamnesi positiva per lombalgia nella posizione seduta neutra prima ( a ) e dopo ( b ) 1 ora di corsa mostrano una riduzione di 8 , 2 mm dopo la corsa . 
immagini di rm medio - sagittali pesate in t2 del rachide lombare dello stesso corridore in estensione prima ( c ) e dopo ( d ) 1 ora di corsa mostra una riduzione totale dellaltezza dei dischi di 7 , 15 mm dopo la corsa . 
these data indicate that as the mechanical load on the lumbar spine increases in proportion to forward bending , inactivity or weakness of mette di mantenere lequilibrio e il bilanciamento [ 35 ]  . 
in aggiunta , durante la normale andatura ciclica della corsa , il corpo si mantiene 664 radiol med ( 2012 ) 117 : 654668 the paraspinal and abdominal muscles to maintain normal sagittal alignment of the lumbar spine could be a very important factor in the mechanism of degenerative disc disease [ 9 , 10 ]  . 
a similar study on the effect of lumbar sagittal alignment changes in lifters concluded that the role of the intervertebral discs in carrying load is influenced by the lumbar sagittal alignment and the magnitude of compression loading [ 9 ]  . 
slight flattening of the lumbar spine under significant compression reduced maximum disc - fibre strain and required equilibrating moments without adversely affecting disc pressure and ligament forces [ 9 ]  . 
during lifting tasks , passive spinal structures are protected by slight to moderate flattening in the lumbar curvature , whereas larger flexion angles impose significantly higher risk by increasing the disc pressure , disc annulus fibre strains , ligamentous forces and facet forces . 
these findings indicate high intervertebral disc strain during spinal loading that in the long term may lead to low back pain and degenerative disc disease [ 17 , 31 ]  . 
in our study , statistically significant reduction of lumbar lordosis was found only in neutral posture after spinal loading by 1 h of running in all runners ; this was also statistically piegato in avanti [ 33 ] , e il movimento pelvico minimizzato per conservare energia e mantenere lefficienza nella corsa . 
tuttavia , leccessiva pronazione del piede , la rotazione interna della tibia e del femore , alterata congruenza femoro - rotulea e alterazioni delle pelvi come uneccessiva inclinazione laterale e anteriore , sono frequentemente osservate nei corridori e possono causare un improprio allineamento del rachide lombare e lesioni acute o croniche [ 33 ]  . esiste una precedente evidenza che indica una relazione fra la postura del rachide lombare e il carico sul rachide che pu contribuire alla patogenesi della degenerazione dei dischi intervertebrali [ 68 , 2830 ]  . 
la rm posizionale studia in individui sani laumento della pressione durante il carico sul rachide in flessione [ 6 , 7 ] e laumento dellaltezza dei dischi intervertebrali ( 1 , 1 mm ) nel passaggio dalla flessione allestensione nella posizione supina [ 8 ]  . 
disc - height reduction and disc dehydration / degeneration was also observed in all runners in both postures ; these were not statistically significant between runners with and without low back pa direct comparison showed higher disc - height reduction and disc dehydration / degeneration in runners with a history of low back pa the reduction of lumbar lordosis in the neutral posture may represent an increase in carried load by the spine , which may lead to increased risk of disc disease , especially in individuals with low back pain [ 10 ]  . 
 although we did not perform electromyographic evaluation , it seems that inactivity or weakness of abdominal and / or paraspinal muscles may be responsible for the inability of runners to retain normal lumbar lordosis [ 10 ]  . 
therefore , runners , especially those with a history of low back pain and degenerative disc disease , should be closely monitored after training to improve lumbar sagittal alignment and strengthen abdominal and paraspinal muscles . we acknowledge two limitations in this study . 
for that reason , we did not attempt to adjust for several factors but only for lordosis and corpi vertebrali esercitano sui dischi intervertebrali , e variazioni posturali [ 36 ] , in quanto la postura in lordosi causa meno dolore che in cifosi [ 11 ]  . 
in uno studio , la media del carico trasferito attraverso il rachide lombare era raddoppiato dalla posizione eretta ( 645 n ) a 10 gradi di flessione ( 1277 n ) , triplicato a 20 gradi ( 1922 n ) e quasi quadruplicato a 30 gradi ( 2305 n )  . 
in questo studio , lattivit mioelettrica dei muscoli che erigono il rachide era aumentata in flessione ed unattivit quasi assente nei muscoli addominali che restavano quasi inattivi [ 10 ]  . 
questi dati indicano che il carico sul rachide lombare cresce in proporzione al grado di flessione in avanti e dunque linattivit o la debolezza dei muscoli paravertebrali ed addominali nel mantenere il normale allineamento sagittale del rachide lombare potrebbe essere un fattore molto importante nel meccanismo di degenerazione discale [ 9 , 10 ]  . 
uno studio simile sugli effetti delle variazioni nellallineamento del rachide lombare nei sollevatori di pesi ha concluso come il ruolo dei dischi intervertebrali nel sostenere il carico influenzato dallallineamento sagittale del rachide lombare e dalla grandezza del carico in compressione [ 9 ]  . 
9a , b immagini di rm medio - sagittali pesate in t2 del rachide lombare del corridore mostrato in figura 8 ( corridore 15 ) nella posizione seduta neutra prima ( a ) e dopo ( b ) 1 ora di corsa mostrano una riduzione di 11 gradi della lordosi lombare , grado 1 di disidratazione / degenerazione del disco l5 - s1 e grado 2 di disidratazione / degenerazione del disco l4 - l5 . disc changes to avoid unreliable and imprecise results . 
we acknowledge that subjective criradiol med ( 2012 ) 117 : 654668 tempo per equilibrare le forze senza alterare la pressione sul disco e sui legamenti [ 9 ]  . 
durante le prove di sollevamento le strutture spinali passive sono protette da un appiattimento della curvatura lombare da minimo a moderato , mentre pi ampi angoli di flessione impongono un pi alto rischio di incrementare la pressione discale , sollecitazioni del cercine fibroso , forzatura delle strutture legamentose e delle faccette articolari ; ci significa maggior pressione durante la flessione e il carico ed aumentato rischio di danneggiamento dei dischi intervertebrali [ 9 ]  . 
queste eventi evidenziano un alto rischio di sollecitazione , a lungo termine , dei dischi intervertebrali causati dal carico sul rachide che pu portare alla lombalgia e a patologia degenerativa discale [ 17 , 31 ]  . 
nel nostro studio , una riduzione statisticamente significativa della lordosi lombare stata trovata solo nella posizione neutra dopo un carico sul rachide determinato da 1 ora di corsa in tutti i corridori ; questo risulta statisticamente significativo anche nei corridori con anamnesi positiva per lombalgia . 
la riduzione dellaltezza e la disidratazione / degenerazione dei dischi intervertebrali stata osservata in tutti i corridori , in entrambe le posizioni ; anche se le differenze non si sono mostrate statisticamente significative tra i corridori con anamnesi positiva per lombalgia e quelli con anamnesi negativa , il confronto diretto ha mostrato una pi alta riduzione dellaltezza e disidratazione / degenerazione nei corridori con anamnesi positiva per lombalgia . 
la riduzione della lordosi lombare nella posizione neutra pu rappresentare un aumento del carico sul rachide e pu determinare un aumentato rischio di patologia discale specialmente negli individui con anamnesi positiva per lombalgia [ 10 ]  . 
sebbene non sia stata effettuata unindagine elettromiografica , sembra che linattivit o la debolezza dei muscoli paraspinali e / o addominali potrebbero essere responsabili dellincapacit dei corridori di riottenere la fisiologica lordosi lombare [ 10 ]  . 
dunque , i corridori , specialmente quelli con anamnesi positiva per lombalgia e patologia degenerativa discale dovrebbero essere strettamente monitorati dopo gli allenamenti per migliorare lallineamento sagittale lombare e il rinforzo della muscolatura addominale e paravertebrale . riconosciamo due limiti a questo studio . 
per questa ragione , non abbiamo tentato di mettere in luce molti fattori , ma solo le variazioni della lordosi lombare e dei dischi intervertebrali per evitare risultati imprecisi e non veritieri . 
tuttavia , tutte le misurazioni e le valutazioni in questo studio sono state comunque effettuate dagli autori del presente studio e dagli stessi due radiologi indipendentemente per tutti i corradiol med ( 2012 ) 117 : 654668 fig . 
10a , b immagini di rm mediosagittali pesate in t2 del rachide lombare in una donna di 51 anni ( corridore 11 ) con anamnesi positiva per lombalgia nella posizione seduta neutra prima ( a ) e dopo ( b ) 1 ora di corsa mostrano una riduzione di 13 gradi della lordosi lombare e grado 3 di disidratazione / degenerazione del disco l4 - l5 dopo la corsa . teria may lead to measurement imprecision and subjective influence . 
however , all measurements and evaluations were performed by the authors and the same two independent radiologists in all runners and were confirmed by the senior authors of this study ( fs , pjp , ah , pk ) , who are university orthopaedic surgeons with > 20 years experience in treating patients with spinal disorders . in this study , using open upright mr imaging , we aimed to evaluate changes in sagittal alignment of the lumbar spine and intervertebral discs that occur after 1 h of spinal loading during running in elite long - distance runners with and without a history of low back pa our results showed a statistically significant reduction of lumbar lordosis in neutral posture in all runners after 1 h of running , which was significantly higher in runners with a history of low back pain , a statistically significant reduction of disc height in both postures in all runners and a variable degree of disc dehydration / degeneration in 23 of the 25 runners more commonly at the l5s1 discs . 
these results show that the intervertebral discs undergo significant strain after 1 h of running , which in the long term may lead to low back pain and degenerative disc disease . 
with a larger sample size , a statistically significant difference regarding disc height and disc dehydration between runners with and without low back may have been observed . acknowledgements imaging support was provided by the department of radiology , university of aberdeen , positional mri centre , woodend hospital , eday road , aberdeen ab15 6xs , scotland uk . 
we thank carlo romagnoli , orthopaedic resident , for his help in translating and editing the italian version of this manuscript . ridori e confermati dai senior authors di questo studio ( fs , pjp , ah e pk ) i quali sono chirurghi ortopedici universitari con pi di 20 anni di esperienza nel trattamento delle patologie del rachide . nel presente studio , con lausilio di una rm aperta in ortostatismo , ci siamo posti lobiettivo di valutare le variazioni nellallineamento sagittale del rachide lombare e dei dischi intervertebrali che avvengono dopo 1 ora di carico sul rachide determinato dalla corsa in atleti professionisti con e senza anamnesi positiva per lombalgia . 
i nostri risultati hanno mostrato una riduzione statisticamente significativa della lordosi lombare nella posizione neutra in tutti i corridori dopo 1 ora di corsa , ci significativamente pi evidente nei corridori con anamnesi positiva per lombalgia , una riduzione statisticamente significativa dellaltezza dei dischi in entrambe le posizioni in tutti i corridori , e un grado variabile di disidratazione / degenerazione in 23 su 25 corridori , pi comunemente a livello l5 - s1 . 
questi risultati mostrano come i dischi intervertebrali siano sottoposti a notevoli sollecitazioni dopo 1 ora di corsa e ci , a lungo termine , pu causare lombalgia e patologia degenerativa discale . 
 probabilmente , con un campione pi ampio , potrebbe essere osservata una differenza statisticamente significativa relativamente laltezza dei dischi intervertebrali e la disidratazione / degenerazione tra i corridori con anamnesi positiva per lombalgia e i corridori con anamnesi negativa . ringraziamenti immagini fornite dal dipartimento di radiologia , universit di aberdeen , positional mri centre , woodend hospital , eday road , aberdeen ab15 6xs , scozia uk . 
ruggieri orthopaedic oncology service , department of orthopaedics , istituto ortopedico rizzoli , university of bologna , via di barbiano 1 / 10 , 40136 bologna , italy correspondence to : p . 
surgical treatment was performed in 35 patients and conservative treatment , including intralesional methylprednisolone injections and halo - vest immobilisation with or without radiation therapy , chemotherapy or embolisation , in the remaining patients . 
ricercando nellarchivio dellistituto ortopedico rizzoli tutta la documentazione relativa ai pazienti trattati per neoplasie del rachide cervicale superiore , sono stati individuati 62 pazienti in un arco di tempo di 37 anni ( da luglio 1973 ad ottobre 2010 ) , 39 uomini e 23 donne , con et media di 39 , 5 anni ( 577 anni )  . 
il trattamento chirurgico stato eseguito in 35 casi , mentre nei rimanenti casi stato eseguito trattamento conservativo mediante infiltrazioni intralesionali di metilprednisolone ed immobilizzazione con halo vest , associato o meno a chemioterapia , radioterapia o embolizzazione . 
per determinati istotipi indicata lassociazione con chemio e radioterapia . parole chiave atlante epistrofeo tumori ossei introduction introduzione a small number of patients with neck pain may have a tumour in the cervical spine . 
tumours of the upper cervical spine involving the atlas ( c1 vertebra ) and the axis ( c2 vertebra ) are rare but challenging because of the unique anatomy and proximity to vital structures [ 1 ]  . 
spasm , secondary spinal deformities such as kyphotic or scoliotic angulation , torticollis , neck stiffness , dysphagia due to compression of the oesophagus from large tumours , neurological deficits from tumours encroaching on the foramina , direct compression or spine instability may be associated symptoms [ 3 ]  . 
myelopathic symptoms related to cord compression are relatively rare [ 36 ]  . plain radiographs may show a radiolucent and destructive lesion or severe osteopenia of one or more vertebrae , which are often associated with pathological fracture , loss of a pedicle on anteroposterior view , osteoblastic lesion , bone destruction with disk preservation , paraspinal softtissue mass with or without calcification and vertebral body collapse with radiographic appearance of vertebra plana [ 1 , 8 , 9 ]  . 
computed tomography ( ct ) is more sensitive than plain films and more accurate than magnetic resonance imaging ( mri ) for bone lesions ; mri is most useful for diagnosing intraand extradural spinal lesions and soft - tissue extension [ 5 ]  . 
bone scan shows increased uptake in the majority of spinal tumours ; its disadvantage is low specificity due to the high rates of false - positive findings in coexisting degenerative spondylosis in older patients . 
additionally , in most cases , haemoproliferative tumours , such as plasmacell dyscrasias , produce little , if any , osteoblastic reaction and therefore are not evident on isotope bone scan [ 10 ]  . ct - guided true - cut biopsy has been performed successfulsolo un piccolo numero di pazienti con cervicalgia potrebbe avere una neoplasia nel rachide cervicale . 
 i tumori del tratto superiore del rachide cervicale coinvolgenti latlante ( vertebra c1 ) e lepistrofeo ( vertebra c2 ) sono rari ma di difficile trattamento a causa della conformazione di queste vertebre e della vicinanza a strutture vitali [ 1 ]  . 
spasmo , deformit vertebrali secondarie , come la cifosi o la scoliosi , torcicollo , rigidit cervicale e disfagia da compressione esofagea da parte di un enorme massa o deficit neurologici dovuti a lesioni che invadono i forami , o che determinano la diretta compressione radicolare o instabilit della colonna possono essere sintomi associati [ 3 ]  . 
sintomi da mielopatia , correlata a compressione midollare , sono relativamente rari [ 36 ]  . lesame radiografico pu mostrare una lesione osteolitica e distruttiva o una severa osteopenia di una o pi vertebre spesso associate ad una frattura patologica , lerosione di un peduncolo su un piano anteroposteriore , una lesione osteoblastica , la distruzione ossea con preservazione dei dischi , una massa nei tessuti molli paraspinali con o senza calcificazione , il collasso del corpo vertebrale con laspetto radiografico della vertebra plana [ 1 , 8 , 9 ]  . 
la tomografia computerizzata ( tc ) pi sensibile della radiografia tradizionale e pi accurata della risonanza magnetica ( rm ) per le lesioni ossee ; la rm molto pi utile per la diagnosi di lesioni vertebrali intraed extradurali , soprattutto per quello che riguarda lestensione nei tessuti molli [ 5 ]  . 
 inoltre , in molti casi , le lesioni emolinfoproliferative , come 618 radiol med ( 2012 ) 117 : 616635 ly in the cervical spine , with low incidence of tumour spreading in the surrounding tissues [ 11 ]  . 
open incisional biopsy should be performed in cases in which sufficient tissue is required ; it is best obtained through an anterior approach rather than by laminectomy to avoid contamination of the epidural space by violation of the tumour pseudocapsule [ 12 ]  . 
in a few cases , when imaging features are strongly consistent with a certain diagnosis such as recurrent primary tumour , metastatic disease , and in cases in which a certain diagnosis such as multiple myeloma is obvious biopsy can be avoided [ 13 ]  . in this article , we present the lengthy experience of a single institution regarding incidence and management of atlas and axis bone tumours and discuss the related clinical and imaging findings and treatment options in this unique area of the spine . materials and methods we searched the registry of our institution for patients admitted and treated for tumours of the upper cervical spine . 
this study was approved by the institutional review board / ethics committee of our institution . results the incidence of benign bone tumours in the upper cervical spine was 39% ( 24 / 62 patients ) and of malignant bone tumours was 61% ( 38 / 62 patients ) ( table 1 )  . 
la biopsia incisionale dovrebbe essere eseguita nei casi in cui sia necessaria una maggiore quantit di tessuto ; preferibile utilizzare un accesso anteriore piuttosto che una laminectomia , per evitare la contaminazione dello spazio epidurale , ottenuta dalla violazione della pseudocapsula del tumore [ 12 ]  . 
in pochi casi , quando limaging depone senza dubbio per una diagnosi certa , come una recidiva di un tumore primitivo , una malattia metastatica e in casi in cui una diagnosi certa come il mieloma multiplo ovvia , la biopsia pu essere evitata [ 13 ]  . in questo articolo , presentiamo la lunga esperienza di un singolo istituto sullincidenza e la gestione dei tumori ossei dellatlante e dellepistrofeo , discutendo e trattando i reperti clinici e strumentali e le opzioni di trattamento in questa particolare area della colonna vertebrale . materiali e metodi abbiamo rivisitato il registro tumori del nostro istituto cercando i pazienti ricoverati e trattati per tumori della porzione superiore del rachide cervicale . 
la radioterapia , la chemioterapia e lembolizzazione arteriosa selettiva sono stati somministrati come completamento di trattamento in 19 pazienti e come trattamento primario in 23 ( tabella 4 )  . per lobiettivo di questo studio , i dati completi di followup erano disponibili per 47 pazienti ( 75% )  . 
abbiamo condotto questo studio osservazionale per valutare lincidenza dei tumori benigni e maligni dellosso nelle prime due vertebre cervicali e discutere sia i reperti clinici e radiografici che le opzioni di trattamento in questa sede peculiare . 
coronal ( d ) , sagittal ( e ) and axial ( f ) ct scans and sagittal t1 - weighted ( g ) and t2 - weighted ( h ) mri show local tumour recurrence . 
we performed this observational study to evaluate the incidence of benign and malignant bone tumours affecting the first two vertebrae of the cervical spine and discuss clinical and imaging findings and treatment options in this unique area . 
our results show that the most common benign bone tumours of the atlas and axis were osteoid osteomas , folbenigna pi comune losteoma osteoide , seguito dalla cisti ossea aneurismatica ; come atteso , la pi comune lesione maligna la metastasi ossea , seguita dal cordoma . 
c radiografia laterale dopo embolizzazione preoperatoria , escissione completa e ricostruzione con una gabbia ed una fusione spinale posteriore . lowed by aneurysmal bone cysts ; as expected , the most common malignant tumours were bone metastases , followed by chordomas . 
la sopravvivenza non stata valutata in questo studio osservazionale perch molti dei pazienti sono stati trattati molto tempo fa e non erano disponibili completi dati di follow - up . 622 radiol med ( 2012 ) 117 : 616635 table 2 the most common benign and malignant bone tumours involving the atlas and axis in the 62 patients in this series type of tumour total , n atlas , n axis , n bone metastases osteoid osteoma chordoma plasmacytoma aneurysmal bone cyst osteoblastoma osteosarcoma giant cell tumour multiple myeloma eosinophilic granuloma chondrosarcoma epithelioid haemangioendothelioma fibromyxoma of bone metastasi ossee osteoma osteoide cordoma plasmocitoma cisti ossea aneurismatica osteoblastoma osteosarcoma tumore a cellule giganti mieloma multiplo granuloma eosinofilo condrosarcoma emangioendotelioma epitelioide fibromixoma dellosso 2 ( atlas and axis ) 1 ( atlas and axis ) 2 ( atlante ed epistrofeo ) 1 ( atlante ed epistrofeo ) tabella 2 neoplasie benigne e maligne pi comuni dellosso coinvolgenti latlante e lepistrofeo nei 62 pazienti inclusi nella nostra serie tipo di tumore totale , n atlante , n epistrofeo , n fig . 
4a - c rm sagittale t1 - pesata ( a ) e t2 - pesata ( b ) di una donna di 29 anni con un tumore a cellule giganti coinvolgente atlante ed epistrofeo . 
b guarigione della lesione a 10 mesi dopo iniezione di metilprednisolone intralesionale tc - guidata . is paramount for all bone lesions , and we recommend that biopsy always precede treatment . 
survival was not evaluated in this observational study because many patients were treated many years ago , and complete data regarding follow - up were not available . benign bone tumours a number of different histological types of benign bone tumours with variable size and biological behaviour can affect the cervical spine [ 1467 ]  . 
a persistent cervical pain in an adolescent radiol med ( 2012 ) 117 : 616635 tumori ossei benigni un grande numero di tumori ossei benigni di differente tipologia istologica , con dimensioni e comportamento biologico variabile pu colpire il rachide cervicale [ 1467 ]  . 
un dolore cervicale persistente in un adolescente o in un giovane adulto , frequentemente associato ad irradiazione allarto superiore senza una specifica distribuzione dermatomerica , spesso in concomitanza di spasmo muscolare suggestiva per un osteoma osteoide ; a differenza della localizzazione tipica , solo un terzo dei casi risponde positivamente al trattamento con acido acetilsalicico [ 15 , 16 ]  . 
sebbene siano stai riportati molti casi di regressione spontanea di osteoma osteoide , il trattamento tradizionale consiste nella completa asportazione chirurgica del nidus ; il tasso di recidiva del 4 , 5% [ 1719 ]  . 
la localizzazione cervicale corrisponde ad un terzo delle cisti ossee aneurismatiche del rachide ; il coinvolgimento dellatlante e dellepistrofeo si verifica in meno dell1% dei casi [ 4450 ]  . 
 la localizzazione pi frequente larco neurale posteriore , una parte del corpo vertebrale o la massa laterale dellatlante [ 21 , 4143 , 45 , 46 ] il dolore il sintomo pi frequente ; la compressione midollare possibile in caso di crescita circonferenziale della lesione attorno al canale midollare [ 15 ]  . 
il trattamento della cisti ossea aneurismatica in questa sede difficile ed spesso associato a significanti complicazioni dovute alla localizzazione , alla vicinanza con le arterie vertebrali e alla difficile ricostruzione [ 21 , 41 , 44 , 5154 ] ; la recidiva dopo escissione incompleta dellordine del 5%10% [ 21 , 41 , 43 , 51 , 52 ]  . 
tuttavia , entrambi i trattamenti richiedono diversi cicli di terapia per poter dare degli effetti terapeutici che si verificano nel corso di diversi mesi [ 45 , 46 ]  . 
although some cases of spontaneous regression of osteoid osteoma have been reported , traditional treatment of spinal lesions is usually complete surgical removal of the nidus ; recurrence up to 4.5% has been reported [ 1719 ]  . 
in our series , osteoid osteomas were the most common complicata dalla possibilit di infarto midollare [ 41 ] , dato che la vascolarizzazione della cisti ossea aneurismatica fornita da alcuni rami dellarteria vertebrale [ 15 , 44 ]  . 
dallo studio dei pazienti trattati con curettage con o senza radioterapia ed embolizzazione arteriosa , non sono state osservate recidive locali . gli osteoblastomi , sebbene istologicamente identici allosteoma osteoide , sono di maggiori dimensioni ( > 2 cm ) e meno frequenti [ 15 , 21 ]  . 
6a , b scansione tc assiale ( a ) e rm ( b ) di una donna di 32 anni con un osteosarcoma osteoblastico grado ii che coinvolge la massa laterale destra e larco anteriore dellatlante trattato con chemioterapia . benign bone tumours of the upper cervical spine ; the most common location was the axis . 
cervical spine aneurysmal bone cysts account for about one third of spinal aneurysmal bone cysts ; involvement of the atlas and axis accounts for < 1% of all spinal aneurysmal bone cysts [ 4450 ]  . 
the posterior neural arch , frequently one side of the vertebral body or the lateral mass of the atlas , is affected more commonly [ 21 , 4143 , 45 , 46 ]  . 
 treatment of aneurysmal bone cysts of the atlas and axis is difficult and associated with significant complications due to location , proximity of vertebral arteries and complex reconstructions [ 21 , 41 , 44 , 5154 ] ; recurrence after incomplete excision has been reported at 510% [ 21 , 41 , 43 , 51 , 52 ]  . 
in addition to resection , embolisation and percutaneous intralesional injection of calcitonin and methylprednisolone have both been tried successfully for aneurysmal bone cysts of the atlas [ 4547 ]  . 
in addition , embolisation in the upper cervical spine is associated with the risk of spinalcord infarct [ 41 ] , as the blood supply of aneurysmal bone cysts in that region is usually through branches of the vertebral artery [ 15 , 44 ]  . 
following various treatments , verifica nel rachide [ 1416 ] ; la met dei casi hanno sede nel rachide lombare con la restante quota equamente distribuita tra il rachide cervicale e toracico [ 15 ]  . 
gli osteoblastomi molto frequentemente si sviluppano negli elementi posteriori , in particolare nei processi spinosi e nelle lamine , qualche volta invadendo il corpo vertebrale [ 15 , 2225 ]  . 
 a causa della loro lenta crescita e delle grandi dimensioni , tendono a coinvolgere pi di un elemento vertebrale e tipicamente si rendono evidenti a causa delleffetto massa locale sulle strutture adiacenti e con deficit neurologici [ 15 , 16 , 26 , 27 ]  . 
 nella nostra casisitica losteoblastoma la terza lesione benigna pi frequente e latlante e lepistrofeo sono egualmente colpiti . il tumore a cellule giganti la quarta lesione pi frequente nel rachide , con un incidenza dell1 , 4%9 , 4% [ 57 ] ; la localizzazione cervicale comune come quella toracica e lombare [ 15 , 58 ]  . 
questa lesione comunemente si presenta con dolore in virt della tendenza di questa lesione ad espandersi con o senza il collasso vertebrale , con instabilit vertebrale e deficit neurologici [ 58 ]  . 
7a - f tomography ( a ) , sagittal ( b ) and axial ct scan ( c ) , and sagittal t2weighted mri ( d ) of a 67 - year - old man with a chondrosarcoma of the odontoid process . 
anteroposterior ( e ) and lateral ( f ) radiographs after curettage and occipitocervical fusion . fig 7a - f tomografia ( a ) , scansione tc sagittale ( b ) e assiale ( c ) e rm sagittale t2 - pesata ( d ) di un uomo di 67 anni con un condrosarcoma del processo odontoide . 
radiografia in anteroposteriore ( e ) e laterale ( f ) dopo curettage e fusione occipitocervicale . 628 radiol med ( 2012 ) 117 : 616635 including curettage with or without radiation therapy and embolisation , recurrences were not observed . osteoblastomas , although histologically identical to osteomas , are much larger ( > 2 cm ) and less common [ 15 , 21 ]  . 
approximately 35% occur in the spine [ 1416 ] ; about half occur in the lumbar spine , with the remaining equally distributed between the thoracic and cervical spine [ 15 ]  . 
because of their slow growth rate and larger size , they tend to involve more than one element of the spine and usually manifest via local mass effect on adjacent structures and neurological deficits [ 15 , 16 , 26 , 27 ]  . 
the atlas and axis were involved equally . giant - cell tumours are the fourth most common benign tumours in the spine , with an incidence of 1.49.4% [ 57 ] ; cervical location is as common as thoracic or lumbar [ 15 , 58 ]  . 
spinal giant - cell tumours most commonly present with pain due to the expansile lesion with or without vertebral collapse , spinal instability and neurological deficits [ 58 ]  . 
various treatments have been advocated for giant - cell tumours of the spine , including arterial embolisation , curettage , surgical excision , radiation and cryotherapy [ 59 ] ; en bloc resection is generally not possible , and preoperative embolisation followed by marginal or intralesional resection and radiation therapy is usually the treatment of choice [ 8 , 5961 ]  . 
local recurrence in the spine is reported to be lower compared with other locations ; however , progression of recurrent giant - cell tumours into aggressive sarcomas has been documented [ 66 ]  . eosinophilic granulomas of the spine account for 6.5 25% of total bone cases [ 15 , 21 , 31 , 32 ]  . 
in this setting , a differential diagnosis with ewings sarcoma tebrale , tra cui lembolizzazione , il curettage , lescissione chirurgica , la radioterapia e la crioterapia [ 59 ] ; la resezione en bloc non generalmente possibile , per cui attualmente il trattamento di scelta rappresentato dalla embolizzazione preoperatoria seguita da escissione marginale o intralesionale e successiva radioterapia [ 8 , 5961 ]  . 
lincidenza della recidiva locale a livello vertebrale minore rispetto alle altre localizzazioni ; sono stati inoltre documentati casi di progressione sarcomatosa [ 66 ]  . il granuloma eosinofilo nel rachide rappresenta il 6 , 5%25% di tutti i casi a localizzazione ossea [ 15 , 21 , 31 , 32 ]  . 
generalmente , il trattamento standard per le lesioni tipiche con un unico coinvolgimento del corpo vertebrale e assenza di deficit neurologici conservativo [ 33 , 35 , 36 ]  . 
la chemioterapia riservata ai casi con malattia sistemica [ 33 , 37 , 38 ] e a quelli in cui la sede di malattia preclude una completa e sicura escissione [ 39 ]  . 
liniezione intralesionale di metilprednisolone tc - guidata , utilizzata sia come adiuvante che come trattamento primario , si dimostrata efficace e sicura [ 40 ] , come in un paziente con granuloma esosinofilo della nostra casistica . il fibromixoma dellosso un tumore benigno fibroso raro che tipicamente coinvolge le ossa mascellari [ 67 ]  . 
lesioni extragnatiche con un abbondante tessuto mixoide sono state inquadrate come mixomi ; in presenza di un gran numero di tessuti fibrosi differenziati , queste lesioni sono state definite come fibromixomi [ 1 , 6769 ]  . 
nella nostra casistica , abbiamo riportato il primo caso di fibromixoma del rachide cervicale originante dallatlanradiol med ( 2012 ) 117 : 616635 or lymphoma is necessary [ 15 ]  . 
ct - guided intralesional methylprednisolone injection , as an adjunct or primary treatment , has been safe and successful [ 40 ] , as in one patient with eosinophilic granuloma of the atlas in this series . fibromyxoma of bone is a rare benign fibrous tumour typically involving the jawbones [ 67 ]  . 
extragnathic lesions with abundant myxoid tissue have been designated as myxomas ; in the presence of large amounts of differentiated fibrous tissue , they have been designated as fibromyxomas [ 1 , 6769 ]  . 
in this series , we report the first case of fibromyxoma of the cervical spine originating from the axis ; complete excision was performed without local recurrence at the latest evaluation . malignant bone tumours managing malignant bone tumours in the upper cervical spine is challenging [ 3 , 4 , 73107 ]  . 
in most cases , conservative , adjuvant or palliative treatments , such as curettage and piecemeal tumour excision , are the only feasible treatments owing to tumour extent and proximity to vital structures . 
several authors describe various surgical excision and reconstruction techniques using combined anterior and posterior surgical approaches and total en bloc spondylectomy [ 73 , 7584 ]  . the spine is the most common site of bone metastases , as also shown in our series . 
 metastasis to the odontoid process is of great significance despite its rarity [ 110 ] ; the mortality rate is > 50% in acute te ; lescissione completa stata eseguita senza recidiva locale allultima data di follow - up . tumori ossei maligni lincidenza e la gestione dei tumori maligni dellosso nel tratto cervicale superiore impegnativa [ 3 , 4 , 73107 ] .in molti casi , a causa dellestensione del tumore e della sua vicinanza a strutture vitali , gli unici trattamenti possibili sono quello conservativo , adiuvante o palliativo tra cui il curettage e lescissione incompleta del tumore , avendo quindi come risultato un alto tasso di recidive locali e di metastasi a distanza [ 73 , 74 ]  . 
alcuni autori hanno descritto diverse tecniche di escissione chirurgica e di ricostruzione che utilizzano approcci chirurgici anteriori e posteriori combinati insieme , oltre alla spondilectomia totale en bloc [ 73 , 7584 ]  . la colonna la sede pi frequente di metastasi ossee , come dimostrato anche dai risultati della nostra casistica . 
i sintomi si verificano a causa dellincremento dimensionale della lesione , dalla compressione delle strutture adiacenti o delle radici nervose , dallinstabilit vertebrale o dalla compressione midollare [ 108 ]  . 
le metastasi a carico del processo odontoide sono di grande rilevanza clinica , nonostante la loro rarit [ 110 ] ; il tasso di mortalit > 50% nei casi di fratture acute di tale struttura [ 110 ]  . 
come confermato anche dalla nostra serie , le metastasi ossee tendono a progredire , anche dopo il trattamento chirurgico combinato con quello adiuvante , e la prognosi a lungo termine scarsa . 
 i cordomi sono dei tumori maligni localmente invasivi , a basso grado di differenziazione e lento accrescimento , che derivano dalla trasformazione neoplastica dei residui della notocorda nei dischi intervertebrali [ 75 ]  . 
rappresentano il 33% di tutti i tumori maligni primitivi vertebrali [ 8587 ] ; il 50% si sviluppa nel sacro , il 37% nel clivus ed i restanti casi in ordine decrescente nel rachide cervicale ( 6% ) , lombare e toracico [ 1 , 21 , 75 , 86 ]  . 
sono pi frequenti nel sesso maschile ; nel rachide cervicale , si rendono evidenti prima che nel clivus e nel sacro , generalmente colpendo una popo630 radiol med ( 2012 ) 117 : 616635 odontoid - process fractures [ 110 ]  . 
as found in our series , bone metastases are progressive , even after combined surgical and adjuvant treatments , and the prognosis is poor . chordomas are low - grade , slow - growing , locally invasive malignant tumours from neoplastic transformation of notochordal remnants in the vertebral discs [ 75 ]  . 
they account for 33% of all primary malignant spinal tumours [ 8587 ] ; 50% occur in the sacrum , 37% in the clivus and the others in decreasing order in the cervical ( 6% ) , lumbar and thoracic spine [ 1 , 21 , 75 , 86 ]  . 
they mainly occur in men ; in the cervical spine , they occur earlier than in the clivus and sacrum , at a mean age of 35 and 53 years , respectively [ 87 ]  . 
a long history of mild neck pain is the most common complaint , in addition to symptoms related to a slow - growing mass , including dysphagia , upper respiratory obstruction , horner syndrome and nerve - root / cord compression [ 8 ]  . 
in most cases , only marginal or intralesional resection is feasible [ 9093 ] ; local recurrence rate is 1260% [ 90 , 93 , 94 ] within 23 years but can also occur > 10 years after excision [ 9597 ]  . 
chordomas are not sensitive to chemotherapy , and only high - dose radiation therapy , such as proton therapy and stereotactic radiation , seems to slow disease progression and achieve 2and 5 - year local control rates of 82% and 50% , respectively [ 3 , 98100 ]  . 
because of their location and proximity to vital structures , complete resection was not feasible , and multiple recurrences were common . solitary plasmacytoma and myeloma are the most common ( 30% ) primary malignant tumours of the spine ; 3% of all myeloma cases affect the cervical spine [ 1 ]  . 
surgical treatment is indicated in cases with progressive neurological deficits , spinal instability , nerve - root / cord compression lazione di et media di 35 e 53 anni , rispettivamente [ 87 ]  . 
una lunga storia di lieve cervicalgia il reperto pi comune , oltre ai sintomi dovuti ad una massa a lento accrescimento quali la disfagia , ostruzione delle alte vie respiratorie , la sindrome di horner e la compressione radicolare / midollare [ 8 ]  . 
nella maggior parte dei casi , realizzabile solo una escissione marginale o intralesionale [ 9093 ] ; la recidiva locale del 12%60% [ 90 , 93 , 94 ] in 2 o 3 anni , ma pu verificarsi anche dopo 10 anni dalla prima escissione [ 9597 ]  . 
i cordomi non sono responsivi alla chemioterapia e solo la radioterapia ad alte dosi , incluse la protontherapy e la radioterapia stereotassica sembrano rallentare levoluzione della malattia e ottenere un tasso di controllo locale della malattia a 2 e 5 anni dell82% e 50% , rispettivamente [ 3 , 98100 ]  . 
a causa della sua localizzazione e della vicinanza a strutture anatomiche vitali , la resezione completa non stata possibile e sono state osservate diverse recidive locali . il plasmocitoma solitario ed il mieloma sono le pi comuni ( 30% ) lesioni maligne primitive del rachide ; il 3% di tutti i mielomi si sviluppano nel rachide cervicale [ 1 ]  . 
il plasmocitoma solitario rappresenta approssimativamente il 3% dei mielomi , con il 50% dei casi che si verificano nei soggetti di sesso maschile di mezza et ( et media 50 anni )  . 
il trattamento chirurgico indicato nei casi con deficit neurologici progressivi , instabilit vertebrale , compressione radicolare o midollare , recidiva locale dopo la massima dose radiante possibile [ 3 , 10 ]  . 
cos come dimostrato dalla letteratura , la met dei casi progredisce in mieloma multiplo [ 3 , 85 ]  . gli osteosarcomi rappresentano il 10% di tutti i tumori maligni primitivi ossei che colpiscono il rachide [ 21 , 25 , 73 , 77 , 101103 ] ; lo 0 , 5% di tutti gli osteosarcomi si localizza nel tratto cervicale [ 1 ]  . 
sono stati riportati nel rachide casi di osteosarcomi radio - indotti e in pazienti con malattia radiol med ( 2012 ) 117 : 616635 or recurrences after maximum - dose radiation [ 3 , 10 ]  . 
in line with the literature , half of the cases progressed to multiple myeloma [ 3 , 85 ]  . osteosarcomas account for 10% of primary malignant tumours of the spine [ 21 , 25 , 73 , 77 , 101103 ] ; 0.5% of all osteosarcomas affect the cervical spine [ 1 ]  . 
in our series , osteosarcomas were the fourth most common malignant tumours of the upper cervical spine ; atlas involvement was more common . chondrosarcomas are the second most common solid spinal tumours and account for approximately 10% of primary malignant tumours of the spine ; 1.5% of all chondrosarcomas affect the cervical spine [ 1 , 3 ]  . 
various low - grade to highly malignant histological types of spinal chondrosarcomas have been reported ; most are low grade and relatively indolent and tend to recur locally before distant spreading occurs [ 76 ]  . 
however , for chondrosarcomas of the atlas and axis , piecemeal excision is frequently the only possible surgical procedure [ 3 ]  . epithelioid bone haemangioendothelioma is a low - grade malignant endothelial neoplasm with a biologic behaviour between that of haemangioma and angiosarcoma . 
although it is the most common type of malignant vascular tumour of bone , it is a relatively rare neoplasm , accounting for < 1% of all bone tumours [ 104 ] ; spinal lesions account for < 10% of all cases [ 105 ]  . 
in our series , one patient with epithelioid haemangioendothelioma of the axis was treated with two cycles of radiation therapy without evidence of local recurrence or metastases until the period of this study . di paget [ 3 , 77 ]  . 
nonostante la radioterapia adiuvante sia stata utilizzata quando la resezione ampia chirurgica non era possibile , gliosteosarcomi non sono radiosensibili e il trattamento deve essere condotto sulla base di protocolli di chemioterapia . 
nella casistica presentata , losteosarcoma la quarta neoplasia maligna pi comune del tratto cervicale superiore ; latlante la sede pi frequente . il condrosarcoma il secondo tumore solido vertebrale pi frequente , rappresentando circa il 10% dei tumori maligni primitivi del rachide ; l1 , 5% di tutti i condrosarcomi colpisce il rachide cervicale [ 1 , 3 ]  . 
 sono stati descritti vari istotipi di condrosarcoma a origine rachidea , da quelli a basso grado fino a quelli ad alto grado di malignit ; la maggior parte sono a basso grado e relativamente indolenti , con la tendenza alla recidiva locale prima che si verifichi la diffusione metastatica [ 76 ]  . 
tuttavia , per i condrosarcomi dellatlante e dellepistrofeo , lescissione frammentaria spesso lunica possibile , cosi come verificatosi nellunico paziente della nostra serie [ 3 ]  . lemangioendotelioma epitelioide dellosso una lesione neoplastica a basso grado di malignit con un comportamento biologico intermedio tra lemangioma e langiosarcoma . 
sebbene sia la pi comune lesione neoplastica maligna di natura vascolare dellosso , relativamente rara , essendo meno dell1% dei casi di tutti i tumori ossei [ 104 ] ; le lesioni vertebrali rappresentano meno del 10% dei casi [ 105 ]  . 
i pazienti con emangioendotelioma epitelioide dellosso possono essere curati con la chirurgia , con o senza chemioterapia adiuvante , radioterapia ed embolizzazione ; la recidiva locale del 13% [ 106 , 107 ]  . 
nella nostra casistica , un paziente con emangioendotelioma epitelioide dellosso stato trattato con 2 cicli di radioterapia senza evidenza di recidiva locale o metastasi fino al periodo di questo studio . 632 conclusions conclusioni radiol med ( 2012 ) 117 : 616635 bone tumours of the cervical spine are rare . 
una valutazione clinica e radiografica appropriata , la biopsia , la stadiazione oncologica e chirurgica , un adeguata tecnica operatoria e terapie adiuvanti mirate possono migliorare il risultato clinico , oncologico e funzionale . 
we studied 21 patients ( eight males , 12 females ; age range 670 years ; mean age 32.6 years ) with craniocervical instability who underwent pocf with hartshill u - shaped rod and songer sublaminar wires . 
clinical assessment using the frankel scale revealed improvement or deterioration arrest in all but two patients : one with c3 failure and halo destabilisation ; the other , who had exhibited myelopathy signs on preoperative mr imaging and persistent basilar impression , showed increasing and progressive neurological deficits despite successful pocf . 
sono stati studiati 21 pazienti ( 8 uomini , 13 donne ; range det , 670 anni ; et media , 32 , 6 ) con instabilit cranio - cervicale e sottoposti ad aocp con posizionamento di barra ad u di hartshill e fili sublaminari di songer . 
in uno di questi due pazienti , si avuta una frattura di c3 con destabilizzazione dellhalo ; laltro paziente , con segni di mielopatia allesame rm pre - operatorio e con persistenza dimpressio basilaris , ha mostrato un progressivo peggioramento dei deficits neurologici nonostante una corretta aocp . 
lo screening rm preradiol med ( 2012 ) 117 : 636653 operation , and it may suggest the need for an alternative surgical approach , such as the transoral approach . 
craniocervical instability may develop as a result of several pathological conditions , including : trauma , inflammatory arthritis , tumour , infection , extensive laminectomy , developmental abnormalities or skeletal dysplasia [ 2 ]  . 
the evolution of surgical techniques is largely related to the advent of noninvasive imaging methods , such as computed tomography ( ct ) and magnetic resonance ( mr ) imaging , which by permitting accurate anatomical evaluation of the craniocervical region help the surgeon to choose the most appropriate surgical approach and technique to obtain optimal craniocervical fusion [ 13 ]  . 
 the purpose of this study was to define the role of pre and postoperative imaging in patients undergoing pocf , focusing on songer sublaminar wires and hartshill u - shaped rod placement via a posterior approach . la giunzione cranio - cervicale dotata di motilit in flessione , estensione e rotazione ; la sua stabilit assicurata principalmente dalla integrit anatomo - funzionale delle strutture legamentose , prime fra tutte la membrana tettoria , i legamenti alari e le fibre trasversali del legamento cruciforme ( legamento trasverso ) [ 1 ]  . 
linstabilit craniocervicale pu svilupparsi in seguito a diverse condizioni patologiche come : traumi , artriti infiammatorie , tumori , infezioni , estese laminectomie , anomalie di sviluppo o displasie scheletriche [ 2 ]  . 
levoluzione delle tecniche chirurgiche legata , in buona parte , allo sviluppo di metodiche dimaging non invasive come la tomografia computerizzata ( tc ) e la risonanza magnetica ( rm ) le quali , fornendo una accurata valutazione anatomica della regione cranio - cervicale , permettono la scelta dellapproccio e dellintervento chirurgico pi idonei per ottenere una ottimale artrodesi craniocervicale [ 13 ]  . 
 scopo di questo studio stato quello di definire il ruolo dellimaging pree post - operatorio nei pazienti sottoposti ad intervento di aocp , puntando lattenzione sul posizionamento , per via posteriore , di fili sublaminari di songer e barra a u di hartshill . materials and methods materiali e metodi between january 1999 and march 2008 , 21 patients with craniocervical instability ( eight males , 13 females ; age range 670 years ; mean 32.6 ) admitted to our department of neurosurgery , were treated with pocf , which involved placing songer sublaminar wires and a hartshill u - shaped rod . 
nove dei 21 pazienti ( 2 maschi e 7 femmine ; et compresa tra 6 e 14 anni ; et me638 radiol med ( 2012 ) 117 : 636653 18 ) and os odontoideum ( patient 14 )  . 
in detail , five patients were affected by basilar impression , four cases of which were congenital ( patients 1 , 2 , 5 , 20 ) and one secondary to down syndrome ( patient 6 ) ; two ( patients 12 , 17 ) had c1c2 instability due to os odontoideum associated with hemiaplasia of the posterior arch of the atlas , which was also present in patient 1 ; one patient was affected by rheumatoid arthritis ( patient 11 ) ; one had a metastatic deposit from lung carcinoma at the posterior arch of c1 ( patient 3 ) ; three were affected by multiple myeloma ( patients 4 , 8 , 21 ) ( table 1 )  . 
x - ray included anteriorposterior and lateral views and functional radiograms at maximum flexion and extension in the sagittal plane to evaluate the degree of craniocervical instability before the procedure and possible residual instability persisting after the procedure . 
to avoid any risk of damaging the neuraxis with dynamic manoeuvres , functional radiograms were not obtained in patients with multiple myeloma ( patients 4 , 8 , 21 ) or metastasis ( patient 3 ) in view of the osteolysis detected in the previous radiological examinations . 
in 14 patients , a single - detector - row ct scanner was used ( prospeed sx advantage , ge medical system , milwaukee , wi , usa ) , whereas seven patients were imaged with 16 - slice ct equipment ( light speed pro16 , ge medical )  . 
preand postoperative mr imaging studies , performed on a signa 1.5 - t unit ( ge medical ) comprised sagittal and axial t1t2 - weighted fast spin echo ( fse ) sequences without contrast material . 
i restanti 12 pazienti ( 6 uomini e 6 donne ; et compresa tra 23 e 70 anni ; et media , 50 , 1 anni ) presentavano diverse patologie , causa dinstabilit ; cinque pazienti erano portatori di impressio basilaris di cui quattro congenite ( pazienti 1 , 2 , 5 , 20 ) , ed una secondaria a sindrome di down ( paziente 6 ) ; due ( pazienti 12 , 17 ) presentavano uninstabilit c1 - c2 da os odontoideum associata ad emiaplasia dellarco posteriore dellatlante riscontrata anche nel paziente 1 ; un paziente era affetto da artrite reumatoide ( paziente 11 ) ; un altro presentava una localizzazione metastatica da carcinoma polmonare in corrispondenza dellarco posteriore di c1 ( paziente 3 ) ; gli ultimi tre pazienti erano portatori di mieloma multiplo ( pazienti 4 , 8 , 21 ) ( tabella1 )  . 
 gli stessi esami sono stati ripetuti una settimana dopo lintervento chirurgico , ogni tre mesi sino ad un anno dallintervento e , durante il follow - up ( range 1296 mesi ; media , 53 , 1 mesi ) , ogni anno o alla comparsa di sintomatologia neurologica . 
 lesame radiografico del rachide cervicale ha incluso le proiezioni antero - posteriore , laterale ed i radiogrammi funzionali in massima flessione ed estensione sul piano sagittale , al fine di valutare linstabilit craniocervicale presente prima dellintervento e leventuale instabilit residua post - operatoria . 
per non esporre a rischio di danno il nevrasse con manovre dinamiche , lo studio radiografico funzionale non stato eseguito nei pazienti affetti da mieloma ( pazienti 4 , 8 , 21 ) e da metastasi ( paziente 3 ) in considerazione delle osteolisi rilevate nei precedenti esami radiologici . 
in 14 pazienti , stata utilizzata unapparecchiatura tc spirale a singolo detettore ( prospeed sx advantage , ge medical system , milwakee , usa ) , mentre in 7 pazienti , stata utilizzata unapparecchiatura multidetettore a 16 strati ( light speed pro16 , ge medical system , milwakee , usa )  . 
utilizzando una workstation di post - elaborazione ( advantage workstation 4.0 ge medical systems , milwakee , usa ) , le immagini assiali sono state rielaborate ottenendo immagini multiplanari ( secondo i piani sagittale e coronale )  . 
gli esami rm pree postoperatori , eseguiti con unapparecchiatura signa 1 , 5 t ( ge medical system , milwakee , usa ) hanno compreso sequenze sagittali ed assiali fast spin echo t1e t2 - dipendenti , senza somministrazione di mezzo di contrasto . 
 tutti i pazienti , inoltre , sono stati sottoposti ad esame clinico - funzionale prima dellintervento , nellimmediato post - operatorio , a tre mesi dellintervento e ogni anno durante il follow - up . 
per lesame clinico - funzionale , si fatto riferimento alla scala di frankel ( tabella 2 ) che una scala neurologica stratificata in cinque gradi ( a - e ) [ 14 ]  . 
 radiol med ( 2012 ) 117 : 636653 640 radiol med ( 2012 ) 117 : 636653 radiol med ( 2012 ) 117 : 636653 642 radiol med ( 2012 ) 117 : 636653 radiol med ( 2012 ) 117 : 636653 table 2 frankel scale grade description complete loss of both motor and sensory function below a given level some preservation of sensation ; complete motor paralysis motor uselessness ; some motor function preserved , but insufficient to be useful motor useful ; weak but useful motor function neurologically intact tabella 2 scala di frankel grado descrizione perdita completa della funzione sensitive - motoria al di sotto di un certo livello mantenimento di un certo grado di sensibilit ; paralisi motoria completa invalidit motoria ; mantenimento di alcune funzioni motorie , ma insufficienti ad essere valide validit motoria ; funzione motoria indebolita , ma valida neurologicamente intatto determination of sensory and motor function and because it requires a plain neurological examination to grade the patients injury . 
the titanium rod was bent into a u shape and cut so that the ends did not extend beyond the fused segments , and it was adapted to the lordotic contour of the occipital region . 
the occipital bone was secured by the wires to the laminae of two to five cervical vertebrae depending on the individual anatomical situation ( previous laminectomy , synostosis ) or to pass beyond vertebrae affected by osteolysis . 
for fusion with autologous bone , cortical and cancellous bone was harvested from the posterior aspect of the iliac crest and subsequently fixed to the craniocervical junction with silk sutures . 
autologous bone fusion was performed in all patients expect for those with short life expectancy , such as those affected by malignancies ; these patients were treated with polymethyl methacrylate grafts . 
the systems used were philadelphia collar , sterno - occipital - mandibular la ripetizione della stessa lettera indica che una lesione rimasta invariata ; la associazione con altre lettere indicher un eventuale recupero o aggravamento neurologico ( tabella 1 )  . 
stata utilizzata questa scala perch basata unicamente sulla determinazione della funzione sensitiva e motoria e perch richiede una semplice valutazione obiettiva neurologica del paziente , prima di classificarlo in uno dei 5 gradi . 
 intervento chirurgico il neurochirurgo , con il paziente in posizione prona e dopo aver preparato losso occipitale ed il rachide cervicale , ha applicato una barra in titanio per stabilizzare la giunzione cranio - cervicale . 
losso occipitale stato ancorato , mediante i suddetti fili , alle lamine di 25 metameri cervicali in base alla situazione anatomica locale ( pregresse laminectomie , sinostosi ) , oppure , in modo da oltrepassare le vertebre sede di osteolisi . 
per lartrodesi con osso autologo stato prelevato dellosso corticale e spongioso dal versante posteriore della cresta iliaca che stato successivamente fissato in corrispondenza della giunzione cranio - cervicale , mediante fili di seta . 
lartrodesi con osso autologo stata eseguita in tutti i pazienti tranne in quelli con bassa aspettativa di vita , come i portatori di patologia maligna ; in questi pazienti , stato utilizzato un innesto di polimetilmetacrilato . 
i sistemi utilizzati sono stati i collari philadelphia , gli sterno - occipital - mandibular immobilizers ( somi ) , oppure nei casi con eccessiva deformit o instabilit , i corsetti halo [ 1517 ]  . risultati i dati clinici e radiologici dei pazienti sono riportati nella tabella 1 . 
 tutte le sublussazioni atlo - assiali , anteriori e rotatorie , non sono risultate pi evidenti nel post - operatorio , con un ripri644 radiol med ( 2012 ) 117 : 636653 fig . 
a lateral radiograph of the cervical spine shows a likely increase in the width of the anterior atlantodental interval ( arrows ) ; the posterior arch of the atlas is not identified . 
 c sagittal t1 - weighted mr image confirms the anterior atlantoaxial subluxation and shows basilar impression associated with displacement of the cerebellar tonsils into the foramen magnum ( chiari i malformation ) ( black arrow )  . 
there is an increase in the width of the anterior atlantodental interval ( dotted line ) , signifying incompetence of the transverse ligament , such that the cranially displaced odontoid process ( o ) is compressing the cervicomedullary junction ( black arrow ) ; note the small area of decreased signal intensity within the spinal cord at the c1 level ( white arrow ) due to extradural compression that reflects myelomalacia or gliosis . 
b la scansione assiale tc passante per c1 , con finestra per osso , mostra chiaramente lemiaplasia destra dellarco posteriore dellatlante e la sublussazione atlo - assiale anteriore ( linea tratteggiata )  . 
c limmagine rm sagittale t1 - dipendente conferma la sublussazione atlo - assiale anteriore e mostra la presenza dimpressio basilaris associata a dislocazione delle tonsille cerebellari nel forame magno ( malformazione chiari i ) ( freccia nera )  . 
evidente un incremento in ampiezza dellintervallo atlo - assiale anteriore ( linea tratteggiata ) , espressione di un danno del legamento trasverso , tale che il processo odontoide ( o ) dislocato cranialmente , comprime la giunzione bulbo - midollare ( freccia nera )  . 
e limmagine assiale t1 - dipendente conferma la compressione sulla corda midollare ( freccia )  . immobiliser ( somi ) brace , or in the event of excessive deformity or instability halo vest [ 1517 ]  . results patients clinical and imaging data are reported in table 1 . 
nel post - operatorio e durante il follow - up , la tc ha permesso di escludere dislocazione e / o rottura dei mezzi di sintesi in tutti i pazienti tranne uno ( paziente 13 ) in cui ha mostrato , nellimmediato post - operatorio , la frattura della lamina destra del terzo metamero cervicale , con consensuale destabilizzazione del radiol med ( 2012 ) 117 : 636653 fig . 
b axial ct scan at the bone window confirms an anterior atlantodental interval > 5 mm ( dotted line ) and shows a slight left rotary atlantoaxial subluxation that might further predispose to occipitocervical instability ( curved arrow )  . 
c axial t1 - weighted mr image shows the odontoid process that is producing slight compression of the subarachnoid space ( arrow ) ; d this finding is not evident on sagittal t2 - weighted image . 
b la scansione assiale tc passante per le masse laterali di c1 e con finestra per osso , conferma un intervallo atlo - assiale anteriore > 5 mm ( linea tratteggiata ) e mostra una modesta sublussazione rotatoria atlo - assiale verso sinistra , che potrebbe aggravare ulteriormente linstabilit occipito - cervicale ( freccia curva )  . 
c limmagine rm assiale t1 - dipendente mostra una lieve compressione dello spazio sub - aracnoideo anteriore da parte del processo odontoideo ( freccia ) ; tale reperto non evidente nella immagine sagittale t2 - dipendente ( d )  . 
postoperatively and during the followup , ct allowed us to exclude displacement and / or fracture of the synthetic devices in all but one patient ( 13 ) , in whom it revealed , immediately after surgery , fracture of the right lamina or the c3 , with simultaneous destabilisation of the tutore esterno . 
a lateral and b anteroposterior radiographs of the cervical spine demonstrating occipitocervical fixation using the hartshill u - shaped rod secured to the occiput , and the c2 , c3 and c4 laminae by songer wires . 
c sagittal t1 - weighted and d corresponding t2 - weighted mr images show persistence of the small area of gliosis or myelomalacia ( arrow in c and d ) , note persistence of basilar impression ( small arrow in c )  . 
i radiogrammi laterale ( a ) e antero - posteriore ( b ) del rachide cervicale mostrano lartrodesi occipito - cervicale con barra ad u di hartshill fissata alloccipite ed alle lamine di c2 , c3 e c4 con fili di songer . 
lmmagine rm sagittale t1 - dipendente ( c ) e la corrispondente immagine t2 - dipendente ( d ) mostrano la persistenza della piccola lesione gliotico - malacica ( freccia in c e d )  . 
 six of 21 patients ( 28.5% ) showed an immediate clinical improvement after surgery , gaining one grade on the frankel scale ( 2 , 6 , 10 , 17 , 19 , 20 )  . 
a lateral radiograph of the cervical spine demonstrating occipitocervical fixation using the hartshill u - shaped rod secured to the occiput and the c1 , c2 and c3 laminae by songer wires ( arrows )  . 
a il radiogramma laterale del rachide cervicale mostra lartrodesi occipito - cervicale con barra ad u di hartshill fissata alloccipite ed alle lamine di c1 , c2 e c3 con fili di songer ( frecce )  . 
le immagini rm assiale t1 ( c ) e sagittale t2 - dipendenti ( d ) non mostrano compressioni dello spazio subaracnoideo anteriore . preliminary anterior decompression , showed progressive increase in neurological deficit from frankel grade d to c ( table 1 )  . 
il legamento longitudinale anteriore , il legamento cruciforme , la membrana tettoria ed il legamento nucale si inseriscono su occipite , atlante ed epistrofeo , mentre , le membrane occipito - atlantoidee anteriore e posteriore , la membrana atlanto - odontoidea ed i legamenti atlanto - odontoideo , apicale del dente ed alari si inseriscono soltanto su due dei suddetti segmenti scheletrici [ 19 ]  . linstabilit vertebrale pu essere definita come uneccessiva risposta ai carichi applicati e si caratterizza per un movimento abnorme nellunit funzionale rachidea . 
questo movimento abnorme pu essere spiegato da una danno delle strutture di contenimento ( disco intervertebrale , articolazioni inter - apofisarie , legamenti , muscoli ) [ 2022 ]  . 
b posterior view of coronal section passing through the occipital condyles and posterior arches of the atlas and axis after dissection of the dura mater , posterior longitudinal ligament and tectorial membrane . 
c transverse view from above the median atlanto - odontoid joints after dissection of the occiput , dura mater , posterior longitudinal ligament , tectorial membrane and anterior and posterior occipitoatloid membrane . 
b visione posteriore su un piano coronale passante per i condili occipitali e gli archi posteriori dellatlante e dellepistrofeo dopo dissezione della dura madre , del legamento longitudinale posteriore e della membrana tettoria . 
c visione assiale dallalto delle articolazioni atlo - assiali mediane dopo dissezione dellosso occipitale , della dura madre , del legamento longitudinale posteriore , della membrana tettoria e delle membrane occipito - atlantoidee anteriore e posteriore . 
abcl , banda ascendente del legamento cruciforme ; al , legamento alare ( porzioni occipitale ed atlantoidea ) ; aoam , membrana occipito - atlantoidea anteriore ; aol , legamento atlanto - odontoideo ; apl , legamento apicale ; dbcl , banda discendente del legamento cruciforme ; dm , dura madre ; oc , condilo occipitale ; pll , legamento longitudinale posteriore ; poam , membrana occipito - atlantoidea posteriore ; safa , faccetta articolare superiore dellatlante ; tgva , forame transverso dellatlante per larteria vertebrale ; tl , legamento trasverso dellatlante ; tm , membrana tettoria . 
the anterior longitudinal ligament , cruciform ligament , tectorial membrane and nuchal ligament attach to the occiput , atlas and axis ; the anterior and posterior occipitoatloid membranes , atlantoodontoid membrane and atlantoodontoid ligament apical ligament of the dens and alar ligaments attach to only two of the abovementioned bones [ 19 ]  . vertebral instability may be defined as an excessive response to loads applied and is characterised by abnormal movement of the functional unit of the spine . 
each functional unit ( motion segment ) is composed of two contiguous vertebrae , an intervertebral disc and interconnecting ligamentous structures . the craniocervical junction serves as a functional unit during sagittal flexion , extension , lateral bending and rotation ; however , it has a limited range of motion . 
the anatomical conformation of the occipitoatloid joint allows good sagittal flexionextension ( 25 ) but limited lateral bending ( 5 per side ) and rotation ( 5 per side )  . 
mechanical stability is ensured by the tectorial membrane , which limits sagitfunzionale rachidea ( segmento di movimento ) costituita da due vertebre contigue , dal corrispondente disco intervertebrale e dalle strutture legamentose dinterconnessione . la giunzione cranio - cervicale agisce , per lappunto , come ununit funzionale durante i movimenti di flessoestensione sagittale , flessione laterale e rotazione ; tuttavia , lampiezza di questi movimenti limitata . 
la conformazione anatomica delle articolazioni occipito - atlantoidee infatti , permette una buona flesso - estensione sagittale ( 25 ) , ma una modesta flessione laterale ( 5 per ciascun lato ) ed un altrettanto modesta rotazione ( 5 per ciascun lato )  . 
la stabilit meccanica garantita dalla membrana tettoria che limita la flesso - estensione sagittale e dai legamenti alari che limitano la flessione laterale e la rotazione [ 23 ]  . 
la conformazione anatomica delle articolazioni atlo - assiali invece , consente una buona rotazione ( 40 ) , una discreta flesso - estensione sagittale ( 20 ) ed una modesta flessione laterale ( 5 )  . 
a questo livello ( atlo - assiale ) , la stabilit meccanica legata soprattutto al dente dellepistrofeo ed alle strutture che lo circondano ( arco anteriore dellatlante e legamento trasverso ) ; inoltre , la membrana tettoria limita la flesso - estensione mentre i legamenti alari limitano la rotazione [ 23 ]  . 
appare evidente , pertanto , come la stabilit della giunzione cranio - cervicale dipenda soprattutto , radiol med ( 2012 ) 117 : 636653 tal flexionextension and by the alar ligaments , which limit lateral bending and rotation [ 23 ]  . 
anatomical confirmation of the atlantoaxial joint , on the other hand , allows good rotation ( 40 ) , moderate sagittal flexionextension ( 20 ) and limited lateral flexion ( 5 )  . 
mechanical stability at the atlantoaxial level is particularly related to dens of the axis and its surrounding structures ( anterior arch of the atlas and transverse ligament ) ; moreover , tectorial membrane limits flexionextension , and alar ligaments limit rotation [ 23 ]  . 
fusion procedures are particularly effective and are absolutely indicated in cases of craniocervical junction instability , intractable pain , definitive neurological deficit and cord compression ; relative indications include patients with radiological instability but with minimal symptoms and no neurological deficits [ 12 , 15 ]  . 
in cases of instability coexisting with irreducible spinal cord compression , osteosynthesis should be preceded by a decompression procedure [ 1517 ]  . when performing fusion procedures , the choice of surgical approach ( anterior and / or posterior ) depends on the site of the instability . 
 anterior fusion via the transoral route allows access to the anterior surface of the first cervical vertebra and is indicated in patients with atlas dislocation who are not eligible for posterior fusion due to fractures or congenital absence of the posterior arch of c1 [ 35 , 24 ]  . 
using a serrated bar , a canal is created through the medial portion of each atlantoaxial joint , where two rectangular bone grafts previously harvested from the iliac crest are inserted . 
the fusion technique described by bailey and badgley [ 25 ] is a variant that sacrifices only the central structures ( vertebral bodies ) with insertion of a bone graft , leaving posterior and lateral support structures intact . 
the latter is generally inserted into the vertebra above or below the level involved or around the screws that block the cephalad and caudal ends of the metallic construct [ 26 ]  . 
 varie sono le cause che concorrono a determinare la comparsa dinstabilit cranio - cervicale ( per esempio , alterazioni congenite , lesioni tumorali , artrite reumatoide , lesioni traumatiche , estese laminectomie ) e che determinano gravi disfunzioni neurologiche , deformit , algie . 
il trattamento chirurgico prevede la riduzione della lussazione , la stabilizzazione mediante fissazione esterna ( per esempio halo jacket ) ed infine , lartrodesi occipitale - cervicale [ 25 , 1517 , 24 ]  . 
le procedure di artrodesi sono particolarmente efficienti e trovano indicazione assoluta nei casi dinstabilit della giunzione cranio - cervicale , sintomatologia algica intrattabile , deficit neurologico definitivo , compressione midollare ; le indicazioni relative comprendono invece quei soggetti con instabilit radiologica , ma con sintomi minimi ed assenza di deficits neurologici [ 12 , 15 ]  . 
nei casi in cui coesistano instabilit ed una compressione midollare irriducibile , losteosintesi dovrebbe essere preceduta da un intervento decompressivo [ 1517 ]  . nel confezionamento dellartrodesi , la scelta dellapproccio chirurgico ( anteriore e / o posteriore ) dipende dalla sede dellinstabilit . 
 lartrodesi anteriore , per via trans - orale , permette di raggiungere la superficie anteriore dei primi metameri cervicali ed indicata nei pazienti con dislocazione dellatlante ed ai quali non possibile praticare una artrodesi posteriore per la presenza , ad esempio , di fratture o assenza congenita dellarco posteriore di c1 [ 35 , 24 ]  . 
utilizzando una barra dentellata , si crea un canale attraverso la porzione mediale di ciascuna articolazione atlo - assiale dove vengono inseriti due innesti ossei rettangolari precedentemente prelevati dalla cresta iliaca . 
la tecnica di artrodesi descritta da bailey e badgley [ 25 ] una variante che sacrifica solo le strutture centrali ( i somi ) con inserimento di un graft osseo , lasciando intatte le strutture di supporto posteriori e laterali . 
questultimo , in genere , inserito nella vertebra sopra o sottostante la zona coinvolta , oppure , in prossimit delle viti che bloccano le estremit cefaliche e caudali dei sistemi di sintesi metallici [ 26 ]  . 
la buona riuscita dellintervento dipende dalla stabilit ottenuta [ 26 ]  . lartrodesi posteriore atlo - assiale stata ideata da gallie [ 27 ] nel 1939 e consiste in un innesto di osseo autologo fissato , con un filo ad ansa , allarco posteriore dellatlante ed al processo spinoso di c2 . 
sonntag e dickman [ 8 ] hanno modificato la tecnica di gallie introducendo , quali ulteriori sistemi di fissazione , dei fili che vengono fatti passare attraverso o attorno ai processi spinosi , oppure , al di sotto delle lamine dei primi due metameri cervicali nei 650 radiol med ( 2012 ) 117 : 636653 posterior atlantoaxial fusion was developed by gallie [ 27 ] in 1939 and consists of an autologous bone graft secured with a loop wire to the posterior arch of the atlas and to the spinous process of c2 . 
magerl and seemann [ 9 ] introduced the use of transarticular screws , which do require integrity of posterior structures ( indispensable for using sublaminar wires ) and may be used in cases of injury to the posterior spinal structures . 
this technique requires considerable skill and precise knowledge of the course of the vertebral arteries ; for these reasons , alternatives have been proposed that involve using c2 transpedicular screws and screws crossing the articular masses of the atlas [ 10 ]  . 
to achieve better mechanical rigidity , this technique can be combined with screw osteosynthesis , which reduces the length of required external orthosis ; at the same time , however , it exposes patients to vascular ( vertebral arteries ) or neurological ( spinal cord or nerve root ) injury [ 15 , 16 ]  . 
success using metal screws in addition to sublaminar wires is 87100% [ 10 , 11 , 2731 ] , but the risk of vascular injury is 2.2% er screw and that of neurological injury 0.1% per screw [ 10 , 32 ]  . 
all our patients underwent wire stabilisation , which is also inexpensive ( it does not require neuronavigation ) and relatively safe in terms of radiation protection , as it does not require continuous fluoroscopic control during the procedure . 
 the goals of posterior occipitocervical fusion , with placement of songer sublaminar wires and hartshill ushaped rod , are the same as those of all the other craniocervical fusion procedures ; namely , restore normal vertebral alignment , protect nerve structures , stabilise the spine and permit an acceptable degree of spinal mobility [ 33 ]  . 
in three patients ( 6 , 13 , 15 ) , this finding , characterised by an atlantodental interval > 3 mm pazienti che necessitano di artrodesi tra atlante ed epistrofeo . 
magerl e seemann [ 9 ] hanno introdotto luso di viti trans - articolari che , non richiedendo lintegrit delle strutture posteriori ( indispensabile per lutilizzo dei fili sottolaminari ) , possono essere utilizzate nei casi di danno alle strutture rachidee posteriori . 
questa tecnica richiede una notevole capacit operativa ed una precisa conoscenza del decorso delle arterie vertebrali ; per tali motivi , sono state proposte delle alternative che prevedono lutilizzo di viti trans - peduncolari di c2 e di viti che attraversano le masse articolari dellatlante [ 10 ]  . 
per ottenere una migliore rigidit meccanica , tale tecnica pu essere integrata con unosteosintesi , mediante viti metalliche , che minimizza la necessit di sottoporre i pazienti a tanti mesi di ortosi esterna ; allo stesso tempo , per , li espone a rischi di natura vascolare ( danno alle arterie vertebrali ) o neurologica ( compressione del midollo spinale o delle radici nervose ) [ 15 , 16 ]  . 
la buona riuscita dellintervento di artrodesi mediante luso di viti metalliche , in aggiunta ai fili sublaminari , compreso tra l87% e il 100% [ 10 , 11 , 2731 ] , ma gravato da un rischio di danno vascolare pari a 2 , 2% ( per vite ) e di danno neurologico dello 0 , 1% ( per vite ) [ 10 , 32 ]  . 
tutti i nostri pazienti sono stati sottoposti a questultimo tipo di artrodesi che anche economico ( non necessita di neuro - navigazione ) e relativamente sicuro dal punto di vista radio - protezionistico non essendo richiesto un continuo controllo radioscopico durante la procedura . 
 gli scopi dellartrodesi occipito - cervicale per via posteriore , con posizionamento di fili sublaminari di songer e barra a u di hartshill , sono gli stessi di tutte le altre procedure di artrodesi cranio - cervicali e cio : ripristinare un normale allineamento metamerico , proteggere le strutture nervose , stabilizzare il rachide e permettere una accettabile motilit rachidea [ 33 ]  . 
il successo dellintervento chirurgico , tuttavia , strettamente dipendente dalla patologia che ha causato linstabilit e soprattutto , dai reperti radiologici pre - operatori [ 15 , 16 ]  . 
in this classification , which is based on atlas dislocation and the rotation axis , rotatory atlantoaxial subluxations are divided into the following four types : type i : rotatory subluxation without anterior displacement of the atlas relative to the axis of the odontoid process ; the latter serves as a pivot for rotation , and alar and transverse ligaments are intact . 
 type ii : rotatory subluxation with 3to 5 - mm anterior displacement of the atlas ; the lateral atlantoaxial joint , opposed to rotational direction , serves as a pivot for rotation , and the transverse ligament is functionally damaged . 
it is mandatory to differentiate the more common congenital basilar invaginations from secondary forms ( rickets , osteogenesis imperfecta , pagets disease , neurofibromatosis ) and from basilar pseudoinvaginations due to lysis of the articular masses of the atlas ( rheumatoid arthritis , metastasis )  . 
ct allowed us to exclude the loss of instrumentation integrity and documented the only acute complication : c3 lamina fracture with secondary displacement of the external orthosis and need for reintervention . 
in questa classificazione , che si basa sulla dislocazione dellatlante e sullasse di rotazione , le sub - lussazioni rotatorie atlo - assiali sono suddivise nei seguenti quattro tipi : tipo i : rotazione senza dislocazione anteriore dellatlante sullasse del dente dellepistrofeo . 
 indispensabile differenziare le invaginazioni basilari congenite , pi comuni , da quelle secondarie ( rachitismo , osteogenesi imperfetta , malattia di paget , neurofibromatosi ) e rispettivamente dalle pseudo - invaginazioni basilari conseguenti a processi litici delle masse articolari dellatlante ( artrite reumatoide , metastasi )  . 
la tc ha permesso di escludere soluzioni di continuo dei mezzi di sintesi ed ha documentato lunica complicanza acuta , cio la frattura di una lamina di c3 con secondaria dislocazione dellortosi esterna e necessit di un re - intervento . 
lesame rm , sia presia post - operatorio , non ha mostrato lesioni focali midollari nei sei pazienti con immediato miglioramento clinico post - chirugico ed in nove dei quattordici pazienti con stazionariet clinica ( mantenimen652 radiol med ( 2012 ) 117 : 636653 sions in the six patients with immediate postoperative clinical improvement and in the 9 / 14 patients with stationary clinical condition preoperative frankel grade preservation )  . 
 in the remaining five patients with stationary clinical condition after surgery , preoperative mr imaging showed a small area of gliosis / myelomalacia , which remained unchanged in the postoperative period . 
the spinal cord lesion no doubt played an important role but was not the only cause of the patients clinical deterioration , given that sublaminar wiring produced no clinical worsening in the five other patients with spinal cord lesions . 
the main cause was nonreduction of the basilar impression by surgery , combined with further narrowing of the spinal canal due to sublaminar wiring and , therefore , probable cord damage by ischaemia . 
 this patient would have benefited more from a double surgical procedure consisting of anterior spinal cord decompression ( proposed by the neurosurgeon but refused by the patient ) followed by ( during the same or a separate session ) instrumented posterior stabilisation , identical to that used in the other cases . 
 despite the small number of patients enrolled in the study , it appears clear that preoperative radiological assessment of the craniocervical junction is necessary for guiding the neurosurgeons choice of surgical approach and procedure , especially in patients in whom preoperative imaging evidences basilar impression . 
postoperative imaging , on the other hand , allows evaluation of the efficacy of the surgical procedure and demonstrates possible complications . in conclusion , the main goal of fusion procedures is to achieve functional decompression with an acceptable motility reduction . 
although an accurate neurological assessment is important , it is fundamental to obtain detailed documentation of the anatomicalpathological and functional situation , and this can be provided by x - ray , ct and mr imaging . 
nei restanti cinque pazienti con stazionariet clinica post - chirurgica , lesame rm pre - operatorio ha invece documentato un piccolo focolaio gliotico / malacico midollare che rimasto immodificato nel post - operatorio . 
la lesione midollare , nel paziente in oggetto , ha senzaltro svolto un ruolo importante , ma non stata lunica causa del peggioramento clinico in considerazione del fatto che negli altri cinque pazienti con lesione midollare , il passaggio dei fili sottolaminari non ha prodotto alcun peggioramento clinico . 
la causa principale da ricercare nella non riduzione chirurgica dellimpressio basilaris a cui si sommata lulteriore riduzione del diametro sagittale del canale rachideo centrale in seguito al posizionamento dei fili sottolaminari e quindi , una verosimile sofferenza ischemica midollare . 
in questo caso , sarebbe stato pi indicato un duplice intervento : in un primo tempo , si sarebbe dovuto procedere alla decompressione midollare con approccio anteriore ( prospettata dal neurochirurgo , ma rifiutata dal paziente ) , per poi procedere ( nel corso dello stesso intervento o in un secondo tempo ) alla stabilizzazione instrumentata mediante approccio posteriore , identica a quella utilizzata negli altri casi . 
 appare pertanto chiaro , nonostante il limitato numero di pazienti arruolati in questo studio , come la valutazione radiologica pre - operatoria della giunzione cranio - cervicale sia necessaria per fornire al chirurgo quegli elementi discriminanti nella scelta dellapproccio e della procedura chirurgica ottimali , soprattutto , nei casi in cui limaging pre - operatorio mostri la presenza dimpressio basilaris . 
 limaging post - operatorio , daltro canto , permette di valutare lefficacia dellintervento chirurgico e di dimostrare eventuali complicanze . in conclusione , lo scopo principale delle procedure di artrodesi determinare una decompressione funzionale con una accettabile riduzione della motilit . 
in 2000 , the response evaluation criteria in solid tumors ( recist ) classification were proposed as the new guidelines to evaluate tumour response using unidimensional measurements and were subsequently revised in 2009 [ 2 , 3 ]  . 
the percentage changes in total tumour burden that define the categories of 1 3 radiol med ( 2015 ) 120 : 430439 pr , cr , and pd were also modified to reflect differences derived from unidimensional rather than bidimensional measurements . 
but neither the recist nor the who criteria included volume measurements partly because of technical restrictions and partly because of limitations of the measurement methods available . tumour volume ( tv ) has nevertheless been demonstrated to be an independent prognostic factor in head and neck tumours and in lung cancers while its role in hepatocarcinomas , lymphomas and germ cell tumours is still being studied [ 413 ]  . 
several studies have , in fact , shown that macroscopic tv , calculated on the basis of pretreatment computed tomography ( ct ) scan , can predict local response after radiation therapy in squamous cell carcinoma arising in different subsites of the head and neck . 
 several investigators have shown that there is a stronger association between t classification and local response [ 1214 ]  . in patients with locally advanced oesophageal cancer , preoperative chemotherapy or combined chemoradiotherapy is increasingly being performed before resection . 
however , this method was relatively inexpensive , it was found to be complicated and difficult to reproduce [ 15 ]  . the ability to reproduce tumour response calculations is , of course , a major concern when tv measurements are being considered as criteria of tumour response assessment . 
modern ct workstations offer automated tools for volumetric analysis of highly contrasted anatomical structures ( such as bone or vascular system ) , but the results are less accurate when poorly contrasted structures , such as the oesophageal wall , are being assessed . 
in the light of these considerations and the need for an objective and accurate tool to calculate tv using both digital and hard - copy ct films , a new specific tumour volume estimation ( tve ) software package was developed to calculate volumetric tumour measurements . the aim of this study was to prospectively evaluate changes in tv after chemoradiotherapy as a predictor of histopathological response , and to compare the accuracy of this methodology with uniand bidimensional assessments . materials and methods software development in january 2007 , a research collaboration between the departments of oncological surgery and oncological radiology of the veneto oncology institute , the department of surgical and gastroenterological sciences of the university of padova , and the department of information engineering of the university of padova was begun with the aim of designing and developing a new software application to calculate tv measurements by utilising tomographic data . 
when the automatic setting is used : ( 1 ) the operator places at least two seeds in two different slice images of the slice image stacks ; ( 2 ) the algorithm computes all the other seeds creating a space interpolation between the slices ; ( 3 ) the software applies a region growing algorithm for each slice of the stack to automatically select a roi ( region of interest ) containing the tumour image ; ( 4 ) the software calculates the tv by interpolation of all the rois between the stack slices . 
since tumours in the oesophagus are often hard to distinguish ( low contrast ) , a modification of a standard region growing algorithm was also developed to avoid possible errors . a phantom analysis was performed during development of the project to set the accuracy of the software . 
 the estimated volumes were then compared with the actual volumes . patients thirty - five consecutive patients affected by locally advanced oesophageal cancer and admitted to the departments of oncological surgery of the veneto oncology institute and the department of surgical and gastroenterological sciences of the university of padova were prospectively enrolled in this study between july 2007 and july 2009 . 
patients with an eastern cooperative oncology group ( ecog ) performance status of less then 2 , a histologically confirmed diagnosis of locally advanced 1 3 432 radiol med ( 2015 ) 120 : 430439 squamous cell carcinoma or adenocarcinoma , a cancer stage of iib - iiib in accordance with the american joint committee cancer ( ajcc 6th edition ) staging classification , and with no medical contraindications for chemoradiotherapy or surgery were considered eligible for this protocol . 
before entering the study , all the patients were evaluated by a multidisciplinary team , which included a medical oncologist , a radiotherapist , a surgeon and a radiologist . the study was conducted in accordance with the principles of the helsinki declaration and all the patients gave their informed consent to be enrolled in the protocol . the pretreatment evaluation included a physical examination , a complete blood cell count and serum chemistry tests : barium oesophagogram , upper gastro - oesophageal endoscopy , bronchoscopy ( in upper and middle third tumours ) , endoscopic ultrasound ( eus ) , chest and abdominal helical ct and cervical ultrasound in upper third tumours . 
all diagnostic examinations were repeated at the end of the chemoradiotherapy treatment cycles and compared with the pretreatment values to assess the patients clinical response [ 1620 ]  . all the patients were treated with neoadjuvant chemoradiotherapy and clinical responders subsequently underwent surgery . 
external beam radiation with a total dose of 45 gy was given in 25 fractions of 1.8 gy , 5 fractions a week , starting the first day of the second cycle of chemotherapy . 
following chemoradiotherapy an ivor - lewis oesophagectomy with extended lymphadenectomy was performed for lower thoracic oesophagus or cardia tumours ; a mckeown oesophagectomy ( thoracotomylaparotomy and cervical anastomosis ) was performed when there were uppermiddle oesophagus tumours ; and a pharyngo - laryngo - oesophagectomy was performed for laryngeal and cervical oesophagus tumours [ 26 , 27 ]  . 
demographic information , tumour stage and location , pathological and histological data and survival rates were analysed and the patient data were collected in a specific prospective database . ct studies multidetector ct scans were routinely performed using contrast - enhanced studies : the ct imaging protocol consisted of contiguous ( 5 mm or thinner ) sections from the neck to the upper abdomen , depending on the location of the primary oesophageal tumour . 
1 computed tomography ( ct ) scan of a bulky thoracic oesophageal tumour : the boundaries and the lumen were manually drawn on each slice obtain the maximum distension of the oesophagus : the area of the oesophageal lumen was accurately identified and subtracted from the tumour area . 
moreover , we selected patients affected by locally advanced oesophageal cancer : in most of them , presenting with severe or absolute dysphagia , the ct scan showed a large tumour involving the whole circumference of the oesophagus with no longer detectable oesophageal lumen . 
in accordance with the 2009 guidelines of the recist group , only the maximal dimension of each tumour deposit ( unidimensional measurement ) was measured and the sum of these measurements was used to evaluate the treatment response which was defined as a decrease of at least 30 % in the sum of the maximal tumour dimension of individual tumours [ 13 ]  . 
in accordance with the who guidelines , the maximal tumour dimension and the greatest perpendicular dimension ( bidimensional measurements ) were measured and multiplied and the resulting cross products for all tumour deposits were summed to assess response . 
with regard to volume analysis , the recist guidelines suggest that a 65 % decrease should be considered a partial response and a 40 % increase a disease progression . differences between preand post - treatment tv , area and diameter were obtained . 
grading of the pathological tumour response to neoadjuvant treatment was considered in accordance with mandards classification : grade i ( complete regression ) absence of neoplastic cells , grade ii isolated cell nests , grade iii more residual cancer cells but fibrosis still predominates , grade iv residual cancer outgrowing fibrosis , grade v absence of regressive changes . histopathological analysis the cross - sectional area by the section thickness . 
 the disease - free survival and the overall survival time were calculated as the time neoadjuvant treatment was begun to the time of recurrence , death , or last follow - up , whichever came first , according to the kaplanmeier method . 
 a transverse section of each block was obtained and the final volume was calculated by summing the product of results patient and tumour characteristics the patients median age was 60.7 years ( range 3877 )  . 
 fifteen patients ( 43 % ) presented comorbidities : six 1 3 ogj oesophagogastric junction table 2 complete staging of patients n ( % ) prognostic value of differences in tumour volume table 1 patient and tumour characteristics 434 demographics patients ( n ) age mean ( years ) male female comorbidity all cardiovascular other tumours cirrhosis other tumour characteristics location cervical and upper middle lower and ogj histology squamous cell cancer adenocarcinoma clinical stage post - ctrt stage ct2n1 ct3n1 ct4n1 yt1n0 yt2n0 yt3n0 yt2n1 yt3n1 yt4n1 pt1n0 pt2n0 pt3n0 pt2n1 pt3n1 pt4n1 pt3n1 m1 pathological stage 60.7 ( 3877 ) 27 ( 77 % ) 8 ( 23 % ) 15 ( 43 % ) 6 ( 17 % ) 5 ( 14.3 % ) 2 ( 5.7 % ) 2 ( 5.7 % ) 26 ( 74.3 % ) 9 ( 25.7 % ) 8 ( 23 ) 22 ( 63 ) 5 ( 14 ) 5 ( 14 ) 8 ( 23 ) 5 ( 14 ) 1 ( 2.8 ) 10 ( 28.5 ) 6 ( 17 ) 4 ( 11.4 ) 9 ( 26 ) 1 ( 2.8 ) 1 ( 2.8 ) 8 ( 23 ) 3 ( 8.5 ) 2 ( 5.7 ) radiol med ( 2015 ) 120 : 430439 as squamous cell cancer and nine ( 25.7 % ) as adenocarcinoma . 
an oesophagectomy was performed in 28 patients ( 80 % resection rate ) , a palliative gastric bypass in one with a neoplastic tracheooesophageal fistula which developed after radiotherapy , only exploratory surgery was possible in three , while progressive disease contraindicated surgery in three . 
however , at survival analysis , neither tv after neoadjuvant treatment nor the difference in volume before and after chemoradiotherapy was predictive of overall survival and disease - free survival . the concordance correlation coefficient obtained comparing radiological and pathological tv was 0.68 ( 95 % 0.300.87 ) with a pearson rho ( measure of precision ) 0.003 , an accuracy of 0.77 ( 95 % ci 0.340.93 ) , p coefficient ( c b ) of 0.88 and a coefficient of determination 0.587. 
predictive values of tumour volume ( tv ) after treatment and pathological stage ( left ) and tumour regression grade ( trg ) ( right ) restaging after neoadjuvant therapy has important prognostic implications . 
at diagnosis the sensitivity and specificity of ct scans with regard to the t parameter in oesophageal cancer vary between 1177 % and 7195 % , respectively , and after neoadjuvant therapy accuracy is further limited due to fibrosis [ 18 , 3032 ]  . 
the recist classification of responses to neoadjuvant therapy has been criticised because the only factor it considers is tumour diameter which may not be representative of the entire tumour burden [ 3337 ]  . many studies have recently focused on the role of tv as a prognostic factor in cancer patients . 
as a result , we 1 3 radiol med ( 2015 ) 120 : 430439 decided to investigate the role of tv preand post - neoadjuvant therapy as a predictor of histopathological response . it was in the light of these considerations that our research group set out to develop a new specific software application to measure tv before and after neoadjuvant therapy . 
since the accuracy of ct in evaluating lymph node metastasis is low and nodal volume is small , we decided against studying lymph node status in this protocol . the results of this prospective study demonstrate that morphological tumour changes can be measured with multidetector three - dimensional ct after chemoradiotherapy in patients affected by locally advanced oesophageal and oesophagogastric junction cancer . 
compared with diameter and area , volume changes demonstrated a good correlation with histopathological stage , even if with a moderate discriminative ability and a modest predictive value . in our analysis , the difference in preand post - treatment volume of oesophageal tumours proved to be less predictive of pathological t stage than expected in the patients studied . 
a reduction of 25 % or more in tv predicted a low pathological stage ( pt1 - 2 ) with a sensitivity of 55.6 % and a specificity of 93 % . 
this was quite interesting if we consider that according to the recist guidelines , which use a mathematic geometric formula for tv determination , a greater than 65 % reduction in tv indicates a partial response to treatment . 
reduction in tv can predict the pathological stage , and this could have important implications in decisions regarding curative resectability , making it possible for surgeons to avoid unnecessary exploratory surgery in some patients and offer it to others who would have been excluded by other criteria . 
tv could then be a factor to take into consideration when resectability after chemotherapy is being evaluated and could aid multidisciplinary teams ( medical oncologist , radiotherapist and oncological surgeon ) to make therapeutic decisions after neoadjuvant treatment . 
as in the present study , griffith applied 3d tumour volumetry to assess tumour response to chemotherapy with an accuracy of 88 % in the evaluation of pathological t stage , the main pitfall being underestimation and overestimation of tracheobronchial invasion . 
however , they did not find any correlation between tv reduction and quantitative pathological assessment of tumour response or patient survival . the difference in preand post - treatment tv was also predictive of tumour regression grade ( mandard index ) although with a lower significance : differences in area had a higher significance but a lower sensitivity . 
 at baseline or any one time point , there is a good correlation between the maximal tumour diameter , bidimensional measurement and tv but the correlation is strongest with the real volume value [ 4 ]  . 
when response to treatment of an oesophageal tumour is being assessed every aspect of its size and not just its maximum diameter should be considered . as expected and as demonstrated in other studies , at survival analysis , neither tv nor differences in its size before and after treatment were predictive of survival , and the same was true for tumour area and diameter . 
this could be due to the small sample size of our protocol as well as to the fact that tumour size in oesophageal cancer is not as good a prognostic factor as lymph node involvement or tumour grade . 
surprisingly , in crhanges retrospective study on 148 patients affected by locally advanced oesophageal cancer and treated with definitive chemoradiation , the pretreatment tv was calculated using an approximate geometric formula and proved to be an independent prognostic factor for survival . 
the mean tv in our study ( 33.8 cm3 ) was much smaller than that in crhanges ( 57.5 cm3 ) suggesting that the geometric formula utilised by those investigators might overestimate tumour size . 
compared the results of the ct volume obtained in vivo and in the surgical specimen ( ex vivo ct scan ) , while in our study we compared the results of in vivo ct volume and volume calculated on the pathological slices and tumour length . using ct images to evaluate tumour response to treatment in oesophageal cancer could be considered one of the drawbacks of our study [ 38 ]  . 
it is nonetheless the standard diagnostic tool currently used to stage oesophageal cancer , and the tumour boundaries were manually drawn on each slice with tve software in the attempt to obtain the most accurate volumetric analysis [ 3033 ]  . 1 3 438 radiol med ( 2015 ) 120 : 430439 a second limitation of our study is the different technical parameters of the ct scans obtained before and after chemoradiotherapy that could have influenced the final comparison . 
since metabolic imaging has been found to be more accurate in evaluating response to chemotherapy , new studies on tv calculated on the basis of pet - ct images are warranted . acknowledgments the authors are extremely grateful to andrea bulzacchi , oncological radiologist , veneto oncology institute , for his precious contribute to the present study . 
the aim of this paper is to describe the incidence of pulmonary complications after olt during the first postoperative week and to evaluate the informative value of the chest x - ray ( cxr ) in clinical practice . materials and methods patients who underwent olt at the ancona transplant centre between august 2005 and august 2012 were included in this retrospective study . 
the cxr and , if performed , the thoracic computed tomography ( tct ) scans performed during the first 7 postoperative days were reviewed , and the radiological findings for atelectasis , pleural effusion , pulmonary oedema , ards and pneumonia were independently assessed and quantified by two radiologists according to the fleischner society criteria . 
the radiological reports produced in the clinical setting were compared with the findings . results among 259 patients included , atelectasis was observed in 227 patients ( 87.6 % ) ; pleural effusion in 250 ( 96.5 % ) ; pulmonary oedema in 204 ( 78 % ) ; ards in seven patients ( 2.6 % ) ; and pneumothorax in 37 patients ( 14 % )  . 
pulmonary oedema was underestimated in the radiological reports in 104 cases ( 40 % )  . conclusions knowledge about postoperative pulmonary complications and collaboration between the radiologist and clinician are essential for improving the management of olt recipients . keywords liver transplantation pulmonary complications lung infection chest x - ray introduction orthotopic liver transplantation ( olt ) is a lifesaving therapy for patients with end - stage liver disease . 
although advances in surgical techniques , organ preservation , immunosuppression and postoperative care have improved the survival over the last few decades , sepsis remains the leading cause of early postoperative mortality [ 1 , 2 ] , infections continue to be the cause of graft loss and morbidity [ 3 ] ; and pneumonia is the most common postoperative infection [ 4 ] and a leading cause of morbidity and mortality [ 1 ] in olt recipients . furthermore , severe , infectious or noninfectious , pulmonary complications are a major contributor to postoperative death in liver recipients more than in other solid organ 1 3 radiol med ( 2015 ) 120 : 413420 414 fig . 
2 cxr and thoracic computed tomography ( tct ) in a case of early - onset pneumonia caused by escherichia coli transplanted patients [ 5 ] , and occur in approximately 35 50 % of recipients [ 6 ]  . 
these data highlight the importance of prevention , early diagnosis and therapy . commonly encountered noninfectious pulmonary complications are atelectasis , pleural effusion , pulmonary oedema , adult respiratory distress syndrome ( ards ) , whereas the most common infectious pulmonary complication is pneumonia [ 6 ]  . 
it has been demonstrated that immediate pulmonary oedema resolving within 24 h after liver transplantation had little clinical consequence , while persistent permeability - type pulmonary oedema led to a worse outcome [ 7 ]  . 
 pleural effusion is a common and expected consequence of olt which contributed to parenchymal compression and atelectasis , and thus indirectly to pneumonia ; furthermore , when pleural effusion is moderate / severe , it can cause respiratory impairment and requires thoracentesis . 
on the other hand , presentations of ori may be atypical because of patient immunosuppression [ 3 ] ; inflammatory responses are impaired by 1 3 radiol med ( 2015 ) 120 : 413420 fig . 
3 cxr and tct in a case of late - onset fatal pneumonia caused by pseudomonas aeruginosa immunosuppressive therapy , with poor clinical and radiological findings . august 2012 , selected according to the database of the ancona surgical department and transplant centre . the radiological diagnosis of pneumonia is defined as the simultaneous presence of a positive radiological examination ( chest x - ray , cxr or thoracic computed tomography , tct ) for a new or increasing consolidation opacity ( at cxr ) or parenchymal consolidation ( at tct ) in association with positive serological samples or fluid specimens ( sputum or bronchoalveolar lavage or pleural fluid or bronchoscopy aspirates ) , and clinical symptoms such as fever , and dyspnoea , or desaturation if the patient is on mechanical ventilation [ 8 , 23 ]  . in this setting , an early diagnosis is difficult , but essential to improve patient survival [ 19 ]  . 
both the clinician and the radiologist , therefore , need to be familiar with the spectrum of pathogens , such as cytomegalovirus and fungi , and the presentations of the most common opportunistic respiratory infections . 
in the first postoperative week , in particular , the differential diagnosis between pulmonary oedema , pneumonia and ards in a dyspnoic patient is very important because therapeutic management is quite different . 
the aim of this paper is to describe the prevalence of noninfectious and infectious pulmonary complications during the first week of follow - up of olt . materials and methods this was a retrospective study on cxr and tct performed during the first 7 postoperative days in patients who under went olt at the surgical department and transplant centre of the university of ancona between august 2005 and we included patients who underwent olt at the surgical department and transplant centre of the university of ancona between august 2005 and august 2012 . 
exclusion criteria were patients with no postoperative cxr or tct due to death occurring on the first postoperative day . in all patients , cxr were performed as a supine film every day during the first 7 postoperative days , in accordance with the centres protocol . 
the radiological examinations performed in the first 7 postoperative days ( cxr and , if performed , tct ) were independently reviewed by two radiologists ( pe and ga ) , and the presence or absence of atelectasis , pleural effusion , pulmonary oedema , ards and pneumonia were assessed according to fleischner society glossary of terms for thoracic imaging [ 20 ]  . atelectasis , pleural effusion and pulmonary oedema were quantified : atelectasis was classified as mild ( involvement of less than one segment ) , moderate ( involving one or more segments of a lobe ) or severe ( involving more lobes )  . 
 pleural effusion was scored as mild ( loss of the sharpness of costophrenic or diaphragmatic sulci ) , moderate ( effusion involving less than a quarter of a hemithorax ) or severe ( involving more than a quarter of a hemithorax )  . 
pulmonary oedema was scored as mild ( interstitial oedema ) and severe ( alveolar oedema )  . ards was defined as the acute development of a diffuse patchy alveolar oedema without vascular pedicle thickening and without cardiac enlargement , with the simultaneous presence of reduced pulmonary compliance needing assisted ventilation with pao2 / fio2 200 mmhg [ 21 ]  . 
the prevalence of infectious agents in our population was also assessed . when ards was associated with superimposed pneumonia , pneumonia could not be directly identified by cxr , and the diagnosis was assessed on the basis of positive biological fluids . 
when tct was performed , ards with superimposed pneumonia could be slightly asymmetric , reflecting areas of infection , compared to the symmetric pattern of ards without evidence of pneumonia [ 22 ]  . 
among the patients who underwent olt at the surgical department and transplant centre of the university of ancona between august 2005 and august 2012 , 10 patients were excluded because death occurred on the first postoperative day and no postoperative cxr or tct was available . 
review of the radiological reports revealed that mild pulmonary oedema had been underestimated in clinical practice in 59 cases ( 42 % ) ( table 2 )  . infectious pneumonia was observed in 32 patients ( 12.3 % ) , and was fatal in five ( 15 % of infectious pneumonias , 1.9 % of the total population )  . 
twelve out of 32 ( 37.5 % ) cases of early pneumonia were due to candida spp : 11 ( 34.4 % ) to candida albicans and one ( 3.1 % ) to candida glabrata . 
six cases ( 50 % of fatal pneumonias ) developed during the first postoperative week ; among them , five cases ( 41.7 % ) of fatal pneumonia were due to candida [ c . 
among the table 2 reporting of pulmonary oedema in clinical practice compared with retrospective review type of pulmonary oedema total cases assessed by retrospective analysis ( n ) cases underestimated by radiologist in clinical practice ( n ; % ) mild severe 59 ; 42 64 ; 100 remaining six cases ( 50 % of fatal pneumonias ) with onset after the first postoperative week , three cases ( 25 % ) were due to e . 
epidermidis. discussion pulmonary complications have great importance in the clinical management of the olt recipient , particularly in the early management in the intensive care unit . among noninfectious pulmonary complications , atelectasis , particularly of the right pulmonary base , is a common finding , and can be due to postoperative diaphragmatic hypomotility , to compression from perioperative pleural effusion , to the increase of intravascular volume and retained secretions , and also to pre - existent conditions , such as right diaphragmatic hypomotility due to hepatomegalia and ascites [ 11 , 24 , 25 ]  . 
atelectasis is a risk factor for the development of pneumonia [ 8 ] ; in fact , infection establishes on the parenchymal portion involved in impaired ventilation and atelectasis [ 26 ] , and thus prevention consists of early extubation , mobilisation and early postoperative kinetic therapy with continuous positive airway pressure ( cpap ) ventilation . 
kinetic therapy , in fact , has been reported to prevent and treat respiratory complications in selected critically ill patients [ 5 ] and also noninvasive ventilation was shown to improve the outcome of these patients [ 27 ]  . 
in our population , pneumonia developed on atelectatic parenchyma in all cases , and in some cases with permanent fibrosis . pleural effusion is a common and expected consequence of olt ; usually unilateral and right - sided , it derives from a direct movement of fluid from the peritoneal cavity into the pleural space through diaphragmatic defects , and is due to residual ascites but also , in some cases , to preoperative conditions such as hepatic hydrothorax [ 10 , 11 , 28 ]  . 
pleural effusion is important because it contributes to parenchymal compression and atelectasis , and thus indirectly to pneumonia ; furthermore , when pleural effusion is moderate / severe , it can cause respiratory impairment and a need for thoracentesis . 
5 aetiological distribution and onset of fatal pneumonia cases haemorrhage and infections [ 9 ] ; moreover , in patients with hepatic hydrothorax as an underlying condition , the risk of pneumothorax arises because of the presence of fibrosis . 
pulmonary oedema in olt has been demonstrated to depend mainly on a flow volume - dependent mechanism , due to overhydration from fluid infusion , blood transfusion during surgery , and to fluid retention related to preoperative renal dysfunction or to renal failure [ 7 ]  . 
the importance of maintaining fluid balance during the perioperative period of olt has been demonstrated [ 31 ] : if the haemodynamics are stable , the appropriate negative fluid balance in the early postoperative period apparently decreases the incidence of early pulmonary complications and results in a better postoperative recovery . 
furthermore , it has been demonstrated that 1 3 radiol med ( 2015 ) 120 : 413420 immediate pulmonary oedema resolving within 24 h after liver transplantation had little clinical consequence , while persistent permeability - type pulmonary oedema led to a worse outcome [ 7 ]  . 
in our population , the comparison between our review and the radiological reports in clinical practice revealed that early pulmonary oedema , particularly when mild , had been underestimated in 104 cases ( 40 % of cases ) , and was not mentioned in the radiological reports : this could lead to an erroneous clinical management and a worse outcome . ards is due to capillary damage and loss of proteic fluid in the interstitial space and consequent diffuse alveolar damage , and is often associated with sepsis from pulmonary infections , with a high mortality rate . 
in our population , ards occurred in seven patients ( 2.6 % ) and was fatal in five cases ( 1.8 % ) , with a mortality rate of 67 % . the risk of infection in the organ - transplant patient is due to many factors : the invasive procedure the patient has undergone , in particular the duration of mechanical ventilation [ 8 ] ; the epidemiologic exposure the patient encounters , which can vary and depends on the microbiological ecology of the intensive care unit [ 6 ] ; and the net state of immunosuppression , a complex interaction of factors such as the presence of underlying diseases , postoperative metabolic factors , concurrent infection with immunomodulatory viruses , and , more importantly , the characteristics of immunosuppressive therapy required to prevent and treat graft rejection [ 32 ]  . 
improvements in infection rates are related to more selective immunosuppressive agents , resulting in a decreased incidence of cytomegalovirus infections and invasive candidiasis , and in a late occurrence of invasive aspergillosis [ 33 ]  . 
bacterial infections are less frequent , but it is important to keep in mind that antimicrobial resistance has become more common [ 3 ]  . the most important principles of patient treatment are prevention , early diagnosis and specific therapy , which should be tailored on the basis of local epidemiological data [ 2 , 34 , 35 ]  . an adequate interpretation of pulmonary imaging can have a role both in prevention and in early diagnosis ; in prevention , the detection of risk factors for pneumonia , such as atelectasis , can help to prevent pulmonary infections ; a radiological assessment of pulmonary oedema can lead to adequate clinical management ; a proper evaluation of the amount of pleural effusion can spare patients invasive procedures such as thoracentesis , which , in turn , can expose the patient to further risks that are relevant to clinical management , such as massive pneumothorax . as regards early diagnosis , it is necessary to have precise knowledge of the probability of the different opportunistic agents of pneumonia , which could superimpose on noninfectious pulmonary abnormalities . 
thus , a correct interpretation and communication of radiological findings in early pulmonary imaging of olt recipients can lead to a better outcome . conclusions olt pulmonary complications , whether infectious or not , are important causes of morbidity and mortality . 
durmaz e - mail : dr.msdurmaz@gmail.com materials and methods we retrospectively reviewed the ct and mr images of 30 patients who were diagnosed with cerebral and spinal hd between 1990 and 2014 . 
all hydatid cysts were classified according to the who classification of hepatic ce , consisting of six types . results the study group consisted of 49 ces in 27 patients with cerebral hd and 12 ces in three patients with spinal hd . 
most of the cysts were type cl and ce1 . conclusions even though characteristic imaging features could be used in the differential diagnosis of hd , sometimes the differentiation of hd from other cystic lesions may be difficult . 
gndz department of internal medicine , medical school , dicle university , diyarbakir , turkey e - mail : drercangunduz@hotmail.com hydatid disease ( hd ) is a systemic zoonosis that is endemic in sheep and cattle farming areas of asia , north and east africa , south america and the middle east [ 13 ]  . 
although hd may affect any part of the body , it most often affects 1 3 radiol med ( 2015 ) 120 : 458465 table 1 world health organization classification of cystic echinococcosis cysts and imaging futures who classification clinical group imaging futures group 1 : active group : cysts developing and are usually unilocular , with uniform content , cyst wall not visible type ce1 type ce2 fertile unilocular , simple cyst with visible cyst wall multivesicular , multiseptated cysts ; cyst septations produce wheel - like structures , and the presence of daughter cysts is indicated by rosette - like or honeycomb - like structures type ce3 group 2 : transition group : cysts starting to degenerate , but unilocular cyst which may contain daughter cysts . 
detachusually contain viable protoscoleces ment of laminated membrane ; water - lily sign type ce4 group 3 : inactive group : degenerated or partially or totally heterogeneous content , ball of wool sign which is indicacalcified cysts - very unlikely to be fertile tive of degenerating membranes type ce5 thick calcified wall cl cystic lesion , ce cystic echinococcosis the liver ( 5975 % ) , followed by the lung ( 27 % ) [ 1 , 7 , 8 ]  . 
cerebral and spinal hd accounts for only 12 % of all cases of hd [ 1 , 8 , 9 ]  . preoperative diagnosis of hd is essential , because rupture and dissemination of the cysts may result in recurrence and life - threatening complications . 
although the diagnosis of hydatid cyst ( hc ) relies on serological tests and imaging techniques [ 10 ] , in primary cerebral hd , serologic tests are not diagnostic because of the blood brain barrier , and imaging studies such as magnetic resonance imaging ( mri ) and computed tomography ( ct ) are necessary for the preoperative diagnosis . 
classical imaging findings in hd are well known but differential imaging findings of hd in unusual locations such as spine and cerebrum are less described in the literature . the first objective of our study was to describe the char acteristic mri and ct imaging features of cerebral and spinal hd in an attempt to provide an improved modality for the differential diagnosis of central nervous system hd in endemic regions . 
the second objective was to use mri and ct to evaluate whether the new world health organization ( who ) classification of hepatic cystic echinococcosis ( ce ) could be used in the classification of cerebral hd . the diagnosis of hd was confirmed by histopathology in 25 patients after surgery . 
the remaining lesions with similar or characteristic radiological appearance were accepted as hd . ct examinations were performed on two ct scanners : 16 detectors , ( toshiba activion ; toshiba medical systems , tochiqi - ken , japan ) and 64 detectors , ( brilliance ct scanner ; philips medical systems , cleveland , ohio )  . 
mr examinations were performed on mri devices supplied with 1.5t and 3t magnetic power ( achieva , philips medical systems , the netherlands ) with a standard head coil . five patients were examined with mri only and nine with ct only . 
the ct scans were performed with contrast in 11 patients , without contrast in three patients , and with and without contrast in 11 patients . the ct and mr findings were retrospectively assessed by the same experienced radiologist . 
 also the simultaneous organ involvement and distribution of cysts were noted . all hcs were classified according to the who classification of ce [ 11 , 12 ] ( table 1 )  . materials and methods results the study was approved by the institutional review board retrospectively review committee . 
as a consequence , 30 patients ( 27 cerebral hd and three spinal hd ) were included in this study . the patient sample comprised 20 males ( 66.6 % ) and 10 females ( 33.3 % ) aged 750 years . 
seven of them similar to type cl and 14 similar to type ce1 frontoparietal unilocular , isointense to csf with a well - defined , hypointense 11 m temporoparietal unilocular , isointense to csf and lacking a hypointense wall cysts cysts cysts on t2 on t2 on t2 wall on t2 on t2 all of the cerebral cysts were supratentorial and the parietal lobe was most frequently involved . 
in ce3 cysts , detachment of laminated membrane from the cyst wall produced a floating membrane appear ance ( water - lily sign ) .the cysts were oval shaped with a 510 510 510 510 510 510 510 510 510 510 1 3 461 radiol med ( 2015 ) 120 : 458465 fig . 
axial t1 - weighted a and axial t2 - weighted images b show multiple spherical , well - defined cysts isointense to cerebrospinal fluid in bilateral frontal and parietal lobes fig . 
 there were no cases of type ce4 or ce5 cysts in our study . noncomplicated or noninfected lesions demonstrated smooth , well - defined , thin - walled , spherical , homogeneous appearance , without calcification , peripheral oedema or contrast enhancement which had inner density / intensity similar to csf on ct and mri . 
two of the patients had multiple hc ( one of them had three cysts and the other one had 21 ) , and all of them were supratentorial , noncomplicated cysts . 
except for one patient , who had cardiac and muscular involvement , all patients ( n 7 ) had concomitant liver involvement and one patient had a disseminated infection . discussion all of our spinal hd cases had characteristic imaging features ; multiple hypointense masses in the vertebral since diagnosis and treatment decisions are driven by imaging , it is important to be familiar with the imaging 1 3 462 radiol med ( 2015 ) 120 : 458465 fig . 
axial t2 - weighted a and sagittal t1 - weighted image b show a mother cyst with detached membrane in the right frontoparietal region , which contains a daughter cyst peripherally features of hd . 
the diagnostic accuracy of mri and ct is high for cerebral and spinal hd with specific imaging characteristics like daughter cysts , floating membrane and hypointense walls on t2 - weighted images . 
type ce1 usually has a low - signal - intensity well - defined wall on t2 - weighted mr image ( rim sign ) which makes them 1 3 radiol med ( 2015 ) 120 : 458465 fig . 
axial t1 - weighted gadolinium - enhanced image b shows complete rim enhancement of the infected cyst table 3 patient age and sex , cyst number , type , level and location in patients with spinal hydatid disease patients number type 2 type ce2 2 type ce3 5 type ce2 2 type ce3 type ce3 level cervical and thoralumbar and sacral thoracal location extradural - intraspiextradural - intraspiparavertebral easy to distinguish from simple cysts . 
a mural nodule that represents the viable larval scolex , cyst with a dot appearance , and oedema and contrast enhancement can be used in differentiation . our demographic findings were similar to those reported in the literature . 
in our study , 19 patients out of 27 ( 70.3 % ) were between 7 and 15 years old , and 18 ( 66.6 % ) patients with cerebral hd were male . 
all of the cerebral cysts were supratentorial and the parietal lobe was most frequently involved . daughter cysts are pathognomonic for hd but this finding has rarely been reported [ 19 ]  . 
c macroscopic appearance of the daughter cysts after surgical excision the differential diagnosis of spinal hcs includes cystic masses , tuberculous spondylitis , chronic osteomyelitis , abscess and haematoma [ 21 , 22 ]  . 
mentioned characteristics include features such as spinal hcs usually having a multilocular structure , low - signal - intensity rims on t2 - weighted imaging , no enhancement ( except in complicated cysts ) , and paraspinal extension , usually without calcification , and osteoporosis and sclerosis in bone . additionally , it is important to know the different stages of ce in order to determine the treatment protocol . 
 these are surgery , percutaneous treatment of the hydatid cysts with the pair ( puncture , aspiration , injection , re - aspiration ) technique , anti - infective drug treatment and watch and wait [ 23 ]  . 
therefore , a watch and wait approach may be used for cysts which are calcified , inactive and do not lead to increased intracranial pressure in asymptomatic patients [ 25 ]  . 
the choice of treatment protocol should be made according to the risks , benefits , indications and contraindications for each case . 1 3 radiol med ( 2015 ) 120 : 458465 we used the who classification of ce for 49 ces in 27 patients with cerebral hd and 12 ces in three patients with spinal hd . 
another limitation is that our study included no patients with type ce4 and type ce5 . in conclusion , the differential diagnosis of hd is usually possible with the combined use of characteristic imaging features , laboratory and clinical information . 
tos was confirmed only after integration with the clinical history . results seventeen ( 45 % ) patients were diagnosed with predominant venous tos ( vtos ) , nine ( 24 % ) with d . 
sardanelli servizio di radiologia , irccs policlinico san donato , piazza malan 1 , 20097 milano , san donato milanese , italy predominant arterial tos ( atos ) and 12 ( 32 % ) had an indeterminate or nonvascular condition . 
it provides a supplementary early acquisition that allows for separate assessment of veins and arteries , permits the investigation of the collateral venous flow with a single injection of contrast material and provides a higher diagnostic power for vtos . 
different forms can be encountered : neurogenic ( ntos ) , arterial ( atos ) and venous ( vtos ) , according to the predominant clinical presentation [ 15 ]  . 
diagnosis is very challenging and to date there is no uniquely accepted protocol . contrast - enhanced magnetic resonance angiography ( mra ) with provocative manoeuvres has been proved useful in this setting [ 68 ]  . 
current mra protocols are performed with delayed scans after intravenous contrast injection to visualise both arteries and veins of the thoracic outlet at the same time [ 9 ]  . 
this late acquisition , however , is limited by the concurrent opacification of the central thoracic and neck veins that can mask the absence of direct flow in the subclavian vein ; second , arteries and 1 3 408 radiol med ( 2015 ) 120 : 407412 veins may overlap and a normal vein may obscure a compressed artery or vice versa [ 8 ] ; third , the patient must be repositioned to carry out acquisitions with arms in adduction , thus increasing the duration of the examination and reducing the amount of residual contrast agent in the thoracic outlet . 
to overcome these drawbacks , we developed a protocol that involves the simultaneous injection of the contrast medium in both arms during abduction [ simultaneous bilateral mra ( sb - mra ) ] , with early , late and adduction acquisitions inside a wide - bore 3t mr system that allows for separate assessment of arteries and veins without patient repositioning . bolus of saline solution of 40 ml at the same rate . 
the study group consisted of 13 males and 25 females ( mean age , 35.9 years ; median , 36.5 years ; , 11.13 ) previously clinically evaluated by the referring physician . 
incidental findings such as mediastinal masses and anatomical variants were also recorded . mr imaging protocol and postprocessing twin peripheral 20g intravenous catheters were placed in a cubital vein in both arms and connected to a single power injector ( spectris , medrad , ca ) by two lines joined with a y - shaped connector . 
this allowed for a single bolus of contrast material to be simultaneously injected in both arms . 1 , 500 ms , time of echo ( te ) 3 mm , field of view ( fov ) a 3t mr system ( siemens magnetom verio wide - bore short - length design , erlangen , germany ) was used . 
the examinations started with an unenhanced t2 - weighted turbo spin - echo sequence of the thoracic outlet with arms abducted , both in coronal and axial planes [ time of repeti95 ms , slice tion ( tr ) 360 thickness 360 mm , time of acquisition ( ta ) 34 s ( axial ) or 51 s ( coronal ) ]  . 
 then , a volumetric time - resolved angiography with interleaved stochastic trajectories ( twist ) coronal sequence 25 , slice 1.04 ms , flip angle ( fa ) [ tr 488 mm , oversam488 thickness 6.7 % ] was acquired . 
p value significance threshold was set at 0.05. 1 3 radiol med ( 2015 ) 120 : 407412 results no patients experienced adverse events related to sb - mra examinations . 
vtos is more challenging to diagnose , since only 10 % of symptomatic individuals have a significant vascular compression [ 12 ]  . mra is currently accepted as an accurate method of investigation in this setting [ 68 , 13 ] ; however , to date there are no established diagnostic pathways for this condition . 
duplex ultrasound evaluation is also used [ 2 , 14 ] , but its results are heavily dependent on operator experience , patient habitus and limits due to the superimposition of bony structures [ 15 ]  . vtos is particularly difficult to diagnose because a cer tain degree of compression is physiologically present in healthy persons [ 14 , 16 ]  . 
additionally , the consequences of a wrong diagnosis can be unnecessary surgery , as also witnessed by the presence in our group of three patients who already had a first rib resection and were still symptomatic afterwards . 
in all three , sb - mra did not show any evidence of compression and their condition was thus deemed indeterminate or nonvascular . an effective approach to maximise the results of the mra is to divide the examination into two different phases : a first phase after the injection of contrast with the patient with arms in abduction ; a second phase with arms at sides . 
these signs cannot be observed in the late phase acquisition , but are specific to the early phase of sb - mra when the flow of the contrast medium is observed in short time intervals , as would happen with traditional angiography . the sensitivity and specificity of mra for tos are difficult to report , since there is no gold standard for comparison . 
however , the readers who were blinded to the early sbmra acquisitions ( group b ) and who had to judge only the late acquisitions identified significantly fewer cases of venous compression , although their interobserver agreement remained high . 
 notably , there is a discrepancy between the severity of the findings readable in the early ( a , b ) and delayed acquisition ( c , d ) fig . 
complete absence of flow from the veins of the right arm ( white asterisk ) , par tial thrombosis of the lscv ( white arrow ) and hypertrophic compensatory veins of the thorax ( white arrowhead )  . 
the white arrow indicates a severe stenosis of the lsca 1 3 radiol med ( 2015 ) 120 : 407412 we did not measure the examination duration to statistically compare it with a standard mra protocol . conclusions sb - mra is a safe and reliable protocol for the study of suspected vascular tos which allows the detection of arterial or venous compression of various degrees . 
in addiction to traditional mra , it provides a supplementary early acquisition that allows for separate assessment of veins and arteries , permits the investigation of the collateral venous flow with a single injection of contrast material and provides a higher diagnostic power for vtos . 
the aim of this study was to evaluate the correlation between clinical response to therapy and cte findings in cd patients . materials and methods forty - five patients with proven cd underwent cte before and after medical therapy . 
the cohen kappa test , t test or anova analysis and 2 test were used for comparisons . results among 45 enrolled patients , 21 ( 47 % ) improved clinically , five ( 11 % ) worsened , 19 ( 42 % ) remained stable . 
ct judgement was in agreement with physicians clinical assessment in 34 patients ( 76 % ) , showing improved disease in 16 / 21 patients ( 76 % ) , stable disease in 14 / 19 patients ( 74 % ) and worsening in 4 / 5 patients ( 80 % )  . 
it can affect any part of the gastrointestinal tract , often affecting multiple sites in a progressive fashion , leading to disabling conditions in a significant proportion of patients , severely deteriorating quality of life [ 1 ]  . 
 although the cause of this disease is not fully understood , the prevailing model is that the intestinal flora drives an unmitigated intestinal immune response and inflammation in the genetically susceptible host [ 2 ]  . 
advances have been 1 3 450 radiol med ( 2015 ) 120 : 449457 made in the use and understanding of nutritional therapy , which represent a highly attractive approach as they treat active disease , have minimal side effects and improve the patients nutritional status . 
inhibition of tumour necrosis factor ( tnf ) is currently the most proven clinically useful therapy for refractory cd [ 3 ]  . patient monitoring is important not only to evaluate the efficacy of medical treatment , but also to stratify disease progression risk among patients , and as such it influences therapeutic decisions [ 1 ]  . 
among radiology techniques , computed tomography enterography ( cte ) and magnetic resonance ( mr ) enterography are the most widely accepted techniques even if ctor mr - enteroclysis is considered the most appropriate examination that allows adequate intestinal loop distension [ 4 ]  . 
 although mr imaging is present , at our hospital ct is the first - line radiological technique for assessing patients with small bowel disease diagnosed by endoscopy , because of accessibility issues . 
we believe that this is the case in several radiological centres in europe and worldwide . although several studies have demonstrated the validity and importance of cte in assessing disease activity and / or complications of the crohns disease [ 6 , 7 ] , limited information exists on radiological modifications following ther apeutic intervention . the aim of this study is to , therefore , evaluate cte findings in patients with crohns disease before and after medical therapy , and determine the correlation between clinical response and cte modifications . materials and methods patient selection and clinical evaluation the study was designed as a prospective , observational study . 
forty - five consecutive patients with a previous histological diagnosis of cd were enrolled in this study from january 2011 to april 2013 ( table 1 )  . for each patient the harvey bradshaw index ( hbi ) was assessed [ 8 ] and a physicians clinical evaluation was performed within 20 days of the cte . 
the hbi is a clinical index based on five items , including assessment of general wellbeing , number of last day bowel movements , abdominal pain , presence of abdominal mass at physical examination and assessment of inflammatory bowel disease ( ibd ) related extraintestinal manifestations . 
they were not communicated at radiology before the examination , and were mostly dependent on the evaluation of a clinical worsening or prior to deciding further major changes in therapy , such as the continuation or discontinuation of an anti - tnftherapy , or the use of immune suppressants or steroids . ct enterography ( cte ) enrolled patients underwent 16 or 64 row - multidetector cte before and after medical therapy . 
 all patients gave written informed consent to the procedure and obtained small bowel distension with oral administration of 2.0 l of an iso - osmotic polyethylene glycol solution ( peg ) ( isocolan , giuliani s.p.a ) administered in equal doses of 100 ml starting 30 min before the ct examination . 
the following parameters were employed : thickness 1.5 mm , interval 1.25 mm , 200700 ma , rotation time 0.9 s , pitch 0.969 mm / rot , for 64 - row ct ; thickness 1.5 mm , interval 1.25 mm , 200600 ma , rotation time 0.6 s , pitch 0.938 mm / rot , for 16 - row ct . 
reformat and maximum intensity projection ( mip ) reconstructions were also performed , in particular in the coronal plane . two gastrointestinal radiologists , who were not involved in the ct examination and were blinded to the clinical data , consensually reviewed all ct images . 
at ct , after iodinated contrast medium injection the normal wall of the distended loop ( normal parietal thickness < 3 mm ) shows a linear and homogeneous hyperdense appearance . 
in our patients the following findings were considered : presence , site and number of abnormal bowel segments ; thickness of pathological loop ( mm ) ; diameter of small bowel lumen ( diameter of the loop excluding the thickness of the wall ) ; longitudinal extension of thickened bowel loops ( mm ) ; presence of stenosis ; presence of target signs ( alternating rings of high and low density ) ; presence of comb signs ( hypervascularity of the involved mesentery ) ; presence of perienteric stranding ( loss of the normal sharp interface between the bowel wall and mesentery ) ; presence of sinus tracts ( linear extension from small bowel loop into an extra - enteric inflammatory process ) ; presence of fibrofatty proliferation ( excess of mesenteric fat ) ; presence of fistulas ; presence of abscesses ; lymphadenopathy ( diameter > 1 cm ) ; fluid in the abdomen [ 9 , 10 ]  . 
we also looked for small bowel distension ; in fact it is essential to have a good fluid - distended loop because mural wall thickening is the hallmark of intestinal disease [ 11 ]  . 
having identified the different bowel segments without pathologies in the coronal reformat images , we defined grade 3 ( complete distension ) as when most of the loops in the examined section had a complete distension , that is , well - distended lumen with thin wall ; grade 0 ( distension absent ) as when most of the segment loops examined were collapsed , that is , undistended lumen and walls not th grades 1 and 2 were intermediate forms between grade 0 and grade 3 . incomplete , 2 partial , 3 absent , 1 we also calculated the effective dose using impact ct dose calculator software of the mhra evaluation centre , and considering a standard patient ( adult patient weighing 70 kg )  . ct and clinical judgements the clinical response to therapy was judged based on clinical global assessment and classified as improved , worsened or stable disease , blindly with respect to radiological evaluations . 
global clinical assessment was based on hbi and other clinical and laboratory parameters , such as anaemia , fever , need for steroids and high levels of crp or faecal calprotectreduction or increase of hbi before and after therapy , of at least 2 points , was considered significant for improvement and worsening , respectively . the ct findings before and after medical therapy were compared and an overall judgement of the progression of the disease status ( improvement versus worsening versus stability ) was given by the radiologists . 
the radiological judgement was based on the comparison of the thickness of the bowel wall , lumen diameter , longitudinal extent of the disease , target signs , appearance of complications such as abscesses or new localisations of disease or new formation of fistulas . subsequently , radiological judgement was compared to clinical judgement . 
comparisons between radiological and clinical judgement were defined as being in agreement in case of same judgements , and no agreement when radiologists and physicians expressed different judgements . statistics mean values and standard deviation were used for numerical variables . 
a value of p < 0.05 was considered statistically significant . results a total of 45 patients ( 27 men and 18 women ; mean age , 50.8 years ) were included in this study . 
44 patients ( 98 % ) 1 3 452 table 2 degree of small bowel loop distension on ct enterography 0 absenta 1 incompletea 2 partiala 3 completea 12 ( 13.5 ) 18 ( 20 ) 6 ( 6.5 ) 2 ( 2.5 ) 2 ( 2.5 ) 1 ( 1.5 ) 12 ( 13.5 ) 6 ( 6.5 ) 5 ( 5.5 ) 6 ( 6.5 ) 24 ( 26.5 ) 18 ( 20 ) 36 ( 40 ) 54 ( 60 ) 12 ( 13.5 ) 70 ( 77.5 ) 6 ( 6.5 ) 77 ( 85.5 ) 11 ( 12 ) 72 ( 80 ) lil or nti a results are present as number of examinations with corresponding percentage of total examination number in parentheses pj proximal jejunum , dj distal jejunum , pi proximal ileum , di distal ileum , lil last ileal loop , nti neo - terminal ileum were free of medical therapy for at least a year ; one patient ( 2 % ) had never received medical therapy . 
a total of 29 patients ( 64 % ) had clinically active disease at baseline , defined as hbi > 4 ( table 1 )  . cte was successful in all patients . 
a computed tomography ( ct ) scan before therapy shows normal findings in the transverse colon ( arrow ) ; b ct after therapy shows thickening of the transverse colon ( arrow ) so the radiological judgement was worsening while the clinical judgement was improvement 1 3 454 radiol med ( 2015 ) 120 : 449457 fig . 
a intestinal thickness ; b longitudinal extension ; c lumen diameter ; d presence of target sign ; e presence of comb sign ; f presence of lymph nodes pre - tp , before therapy ; post - tp , after therapy small bowel disease , but it is essential to have a good distension of the small bowel loops because mural wall thickening is the hallmark of intestinal disease . 
fluid distension can be obtained by oral use of oil emulsions , water , air , mucofalk , peg , 45 % sodium diatrizoate , 1 % barium sulphate [ 1316 ]  . 1 3 radiol med ( 2015 ) 120 : 449457 fig . 
a ct before therapy shows thickening with target and comb sign in two ileal loops ( white arrows ) ; b ct after therapy shows reduction of thickening and longitudinal extent in both loops the technique of contrast agent administration by oral or by nasojejunal tube influences the grade of distension of the loops . 
a common drawback of oral contrast agents is that they fail to ensure suitable and uniform distension of all small bowel loops , giving rise to significant problems in differentiating between real wall thickening and inadequate distension or spasthe problem can be overcome , although with greater invasiveness , time and costs , using ct enteroclysis , a method developed in the early 1990s in which variable amounts ( 2 , 0002 , 750 ml ) of low - density ( water ) or high - density ( 45 % sodium diatrizoate , 1 % barium sulphate ) contrast material are infused by hand or with a peristaltic pump through a nasojejunal tube before the ct scan with and without i.v. 
a ct before therapy shows thickening of the transverse colon ( white arrows ) and the descending colon ( black arrow ) ; b ct after therapy shows reduction in thickness and longitudinal extent of the transverse colon ( white arrows ) and reduction in thickness of the descending colon ( black arrow ) a wide amount of data is available on the techniques and diagnostic accuracy of cte [ 6 , 19 , 20 ] , but only a few studies have evaluated cte findings before and after therapy . 
 [ 21 ] , the most commonly found lesion was thickening of the bowel wall before and after treatment , which was described as growing thinner and shorter , or changing in shape after treatment . 
 [ 22 ] studied 50 patients and found that bowel wall attenuation and thickness were significantly correlated with disease activity in a logistic regression analysis , but in this case only patients with clinical remission , identified through a combination of clinical , endoscopic and laboratory tests , were studied . in our study , we evaluated cte findings before and after medical therapy and the correlation between clinical response and cte modifications . 
in accordance with previous studies 1 3 456 radiol med ( 2015 ) 120 : 449457 in our study , a disagreement between radiological and clinical assessment was found in 24 % of the cases . 
 these cases were associated with mucosal alterations of the disease not detected by ct in a small percentage of patients , maybe because of an inadequate distension of the loops , or a deterioration of physiological conditions not paralleling laboratory or radiological assessment . 
these findings suggest a possible prognostic role for cte , which needs to be evaluated in dedicated studies . another interesting finding is that cte modifications appear in a relatively short period of time ( 11 in patients with a better outcome . 6 months ) since cd is a trans - mural disease , the use of cte should represent an important step in the diagnostic , therapeutic and prognostic management of the disease , because it is able to evaluate not only the intestinal mucosa but also the bowel wall . 
cte may be in fact employed to determine parameters such as parietal thickening , longitudinal extensions , comb signs and others , extending beyond the concept of mucosal healing , and may , therefore , provide important new information on the status of the entire bowel wall , potentially contributing to a better stratification of cd patients for a correct prognosis in response to therapy . a complete disappearance of cte alterations was not found in any patient . 
on the other hand , these findings may be due to the relatively small number of patients enrolled in the study or , less likely , to possible technical limitations of cte in terms of sensitivity and / or specificity . our study has potential limitations . 
furthermore , the patients underwent cte at different time points based on individual clinical indications , and in the case of our centre , radiology was employed together with endoscopy to assess crohns disease . 
 the aim of our study was not , however , to assess response to a specific therapy , but to evaluate cte findings before and after medical therapy and the correlation between clinical response and cte findings . 
b ct after therapy shows formation of abscesses ( inside the square ) near the ileal pathological loops ( white arrows ) in the literature [ 18 ] , we also found thickening of the bowel wall in all patients before medical therapy . 
after therapy , clinical improvement was associated with changes of the ct findings , in particular reduction of the parietal thickening , reduction of the longitudinal extension of the disease , increase of the bowel diameter and reduction in the prevalence of the target sign . 
surprisingly , detection of complications such as occurrence of a new disease localisation or formation of abscesses at cte was not significantly associated with disease worsening . 1 3 radiol med ( 2015 ) 120 : 449457 not substantially affected . 
in particular , our study suggests that the use of anti - tnfis more likely associated with radiological improvement compared to other therapies . other study limitations are the use of oral contrast medium and ionising radiation on young patients . 
even if administration of contrast agents via nasojejunal tube permits a better bowel distension than by oral administration , previous studies [ 18 ] did not find a statistically significant difference between ct enteroclysis and cte with regard to the distension of the ileum , the main sites of cd in our patients . finally , some concerns may be due to the fact that cte is a technique that requires ionising radiation , but we think that cte assessment may be performed when mr enterography is not available . 
cte radiation loads , however , have been progressively reduced with the availability of newer and faster ct scanners . other studies are needed to evaluate how to improve clinical and imaging agreement , also using other imaging techniques . 
in fact , in recent years , several radiological techniques have been developed for the study of the small bowel such us mri , ultrasonography ( us ) , contrast - enhanced ultrasonography ( ceus ) , and 99mtc - hmpao - labelled leukocyte scintigraphy ( tlls )  . 
less invasive and less costly radiological assessment toolssuch as dedicated us or mr imagingwould be desirable . acknowledgments lorenzo bonomo and antonio gasbarrini conceived of the study and participated in its design and coordination . 
 luigi larosa , rosa marra , francesco giordano , lucrezia laterza , amorino vecchioli , iolanda scoleri , viviana gerardi , giovanni bruno , eleonora gaetani participated in carrying out the studies and data analysis and helped to draw up the manuscript . 
in particular cases , it is also possible to avoid embolisation of the internal iliac artery . keywords evar isolated iliac artery aneurysms endoprosthesis endovascular treatment introduction isolated iliac artery aneurysms ( iiaas ) are the less frequent intra - abdominal aneurysms , but they are associated with a high risk of rupture and death [ 1 ]  . 
iiaas are located in the common iliac artery ( cia ) in 70 % of cases , in the internal iliac artery ( iia ) in 20 % of cases and in the external iliac artery ( eia ) in only 10 % of cases [ 4 ]  . clinical manifestations are frequently related to the compression of adjacent structures ; in the case of rupture , the patient generally complains of rapid onset abdominal pain associated with bradycardia , hypotension and sweating [ 4 , 5 ]  . 
iiaa treatment is indicated if the aneurysm is > 3 cm , if it has a growth rate > 5 mm in 6 months or > 1 cm in a year or if the patient is symptomatic [ 1 , 6 ]  . 1 3 radiol med ( 2015 ) 120 : 440448 open surgery has been the standard treatment for years [ 7 , 8 ] ; although it generally achieved high levels of technical success , it is accompanied by several complications such as bleeding , surgical infections , ureteral injury and distal embolisation with lower - limb ischaemia . 
the mortality rate of elective aneurysm surgery is relatively low ( 06.2 % ) , whereas that of emergency surgery is significant and ranges from 0 to 55.5 % [ 914 ]  . over the last decade , endovascular treatment has become a good alternative to open surgery for iiaas because it combines shorter operative times , a lower incidence of complications and perioperative mortality and excellent long - term results [ 1517 ]  . 
 the purpose of this study was to review our experience to date , which has a number of patients amongst the largest reported in the literature , and to assess the proper management of aneurysms involving iia treated in emergency and elective circumstances . materials and methods between may 2005 and september 2013 , 45 patients ( 43 men and two women ; mean age , 74 10 years ) with a total of 59 iiaas ( mean diameter 4.4 cm ) underwent endovascular treatment : an excel database was prospectively recorded and retrospectively analysed . 
table 1 shows the characteristics of the patients and aneurysms . in all cases , preliminary computed tomography angiography ( cta ) was performed to adequately assess aneurysm characteristics and to select the most suitable stent - gra prior to the procedure , all patients were informed about the benefits and risks and provided their informed consent . 
 as the study was retrospective , approval of the local ethics committee was not sought . in 18 cases , the procedure was performed in the angiography room with an integris v5000 angiography unit ( philips medical system , best , the netherlands )  . 
in 18 cases , the procedure was performed under local anaesthesia and with anaesthesiological assistance ( lidocaine 2 % ) , in 15 cases under intraspinal anaesthesia and in 12 cases under general anaesthesia . 
those with aneurysms of the cia near the aortic bifurcation ( < 2 cm ) were treated with a bifurcated aortic stent - graft ; coil embolisation of the iia origin was made if the iliac bifurcation was involved in the aneuryspatients with concomitant aneurysm of the cia and the iia were treated by stent - graft placement across the cia and coil of the iia . 
a statistical comparison of the incidence of mortality , endoleaks and pelvic ischaemia between the two treatment groups was performed by testing for proportions , placing as the threshold of statistical significance p 0.05. 
reintervention - free survival and endoleak - free survival between the two groups were then compared with log - rank test ( alpha value 0.01 ) : radiol med ( 2015 ) 120 : 440448 the results obtained were shown by kaplanmeyer curves . 
both of these deaths occurred in patients treated in emergency : perioperative mortality was therefore 16.6 % ( 2 / 12 ) in the emergency group and 0 % in elective group ( 33 patients )  . 
 statistical comparison carried out by testing for proportions documented that this difference was statistically significant only one perioperative complication occurred ( 2.2 % ) , during the elective treatment of a cia aneurysm near the aortic bifurcation with a zenith aortouniiliac stentgraft : during withdrawal of the device , the iliac extension migrated caudally up to the vicinity of the inguinal ligament , resulting in an incorrect seal between the body and the extension . 
the patient did not undergo reintervention for the type iii endoleak because he died shortly thereafter due to not graft - related causes . all treatments were carried out according to the literature data and guidelines [ 19 ] except for nine patients ( 20 % ) in whom iia embolisation was not performed . 
during follow - up ( 43 patients followed up ) , four patients died ( 9 % ) : two at around 24 months due to progression of neoplastic disease and myocardial infarction , respectively ; the other two at around 36 months , one because of end - stage chronic kidney disease , and the other one , who was the patient who presented to the emergency department with type iii endoleak , because of severe respiratory dysfunction . 
the survival rate was 86.7 % in the medium terthe mean follow - up time was of 34.3 ( range 196 ) months . we had a primary patency rate of 95.5 % ( 42 / 44 patients )  . 
there were two cases ( both in the electivetreatment group ) ( 4.5 % ) of thrombotic occlusion of the stent - graft at 1 and 6 months , respectively , resulting from a residual stenosis affecting the prosthetic branch ; both were treated successfully with intra - arterial fibrinolysis and angioplasty . 
both of these complications that required reoperation occurred in the elective - treatment group ( 2 / 33 , 6 % ) , whilst there were no reoperations in the emergency - treatment group . 
reintervention - free survival 1 3 444 radiol med ( 2015 ) 120 : 440448 the nine patients treated without preventive embolisation of the iia had the following outcomes : in three patients ( 33.3 % ) treated under emergency , we observed a type ii endoleak arising from the iia ; in the other six cases ( one emergency and five elective ) , no perfusion of the native sac was observed . 
in four cases , pelvic ischaemia was transient and resolved within months , in three cases it was persistent , and in one case it was associated with sexual dysfunction . table 4 compares the results observed in the two groups . treatment of iiaas with the endovascular approach [ endovascular iliac artery aneurysm repair ( eviar ) ] has become an attractive and effective option with a lesser degree of complications compared to open surgery [ 8 ]  . 
 [ 21 ] , in their comparison between the two treatment options , reported similar primary and secondary patency rates ( 99.6 % ) at 5 years , similar survival free from reintervention and overall survival ; however , they reported a reduction in mortality rate , postoperative complications , and hospitalisation for the eviar group . 
1 technical failure in a ruptured common iliac artery ( cia ) aneuryspreliminary computed tomography angiography ( cta ) ( a , b ) documented a severe stenosis distal to the aneurysm which made any endovascular treatment impossible . 
none of the type ii endoleaks were associated with increased size of the native sac and they were all managed conservatively by ceus follow - up every 6 months ( the patient with type iii endoleak died before reaching the operating room )  . the rate of endoleak was 23 % ( 3 / 13 , all in patients treated without embolisation of the hypogastric artery ) in the emergency - treatment group and 13.3 % ( 6 / 45 ) in the elective - treatment group . 
cta follow - up at 1 month ( c , d ) documented technical success with complete exclusion of the aneurysm and without any type ii endoleak from the iia . 
these findings remained unchanged at contrast - enhanced ultrasound ( ceus ) follow - up at 6 and 12 months we previously reported our experience with eviar ( 32 patients with 40 iiaas ) with good results in the followup period [ 18 ] ; as of now , our series has the same number of patients as the largest international series published by boules et al . 
 [ 24 ] ( 45 patients ) so we wanted to review our data to better show the effectiveness of endovascular treatment of isolated iias and to provide our innovative experience in the management of aneurysms involving the internal iliac artery . in our experience , we have observed that eviar is a safe procedure , with a low incidence of periprocedural complications and mortality , in agreement with the literature [ 2024 ] : we found only one case of technical failure in a patient with cia aneurysm and severe stenosis of the proximal segment of the same vessel that required surgical conversion . 
this complication we observed further emphasises the need to perform a preliminary cta study , making it possible to correctly identify patients who are candidates for endovascular repair and to choose the appropriate materials . according to our recent report on the treatment of ruptured aortic aneurysms [ 25 ] , also for iliac aneurysms we do not consider haemodynamic instability to be a contraindication for endovascular treatment : in 12 cases , treatment was performed as an emergency and in this group we had a perioperative mortality of 16.6 % ( 2 / 12 ) : one death in the above - mentioned patient with iliac stenosis and surgically converted and the other one patient died two days after treatment . 
in the remaining 10 patients ( 83.4 % ) with ruptured iliac aneurysm , the treatment was effective in the absence of peri - and postprocedural complications . our incidence of perioperative mortality in patients treated in emergency settings was consistent with the literature data [ 2024 ] and lower than that reported for open surgical treatment [ 914 ] and emphasises that this therapeutic approach ought to be a first choice especially in patients with haemodynamic instability , in which the miniinvasiveness of the procedure allows a significant reduction in processing time with rapid control of active bleeding . 
 however , there is a need to have a team of vascular interventional radiologists , vascular surgeons , technicians and nurses dedicated 24 h / 7 days ready to be operative within 1 3 446 radiol med ( 2015 ) 120 : 440448 fig . 
 postoperative dsa showed complete exclusion of the aneurysm ( b ) with results maintained over time at cta follow - up ( c , d ) 30 min of an emergency call . 
it also emphasises the need for elective operations to be performed in dedicated centres with a high volume of patients that can also handle any complications . a debated topic is the therapeutic management of patients with iliac aneurysm involving the internal iliac artery [ 16 , 17 , 19 ]  . 
the guidelines [ 16 , 17 ] suggest embolising the internal iliac artery in the case of aneurysms of the cia involving the iia and in cases of isolated iia aneurysms to prevent type ii endoleaks . 
it is also suggested , in the case of iia aneurysms without a good proximal neck , to embolise the two distal branches of the iia and to place a stent - graft covering its origin [ 16 ]  . 
platinum coils are the most common embolic materials used [ 18 ] ; elsewhere , according to the experience of the operator , various embolic materials can be used , such as vascular plugs [ 2 ]  . the clinical effectiveness of iia embolisation is now established in the literature and was recently confirmed by chun et al . 
 [ 2 ] who , in 88 patients ( 10 with isolated iliac aneurysms ) treated with coils , amplatzer plugs and a combination of embolic agents , observed technical success of 95.7 % , only four cases of type ii endoleak and a low incidence of complications such as buttock claudication ( 38 % ) or erectile dysfunction ( 10 % )  . 
this observation is of utmost importance as it points out that especially in patients with haemodynamic shock and ruptured cia aneurysm can avoidance of iia embolisation reduce procedural time and blood loss . 
in addition , in this group of patients we observed only type ii endoleaks , without any increase in dimension of the native sac : in such cases , we adopted a conservative management with a ceus examination every 6 months ; no case required reintervention . 
these authors carried out a retrospective study of 137 patients with aaa extended to the iliac axes treated with evar including 112 treated without embolisation of the iia and 25 cases with its embolisation and noted that there was no difference in cumulative survival and in the incidence of secondary interventions between the two groups . 
these results better show the possibility of avoiding iia embolisation in selected cases , without significant complications . even with the limits of the low number of patients and the fact that there is limited data in the literature [ 27 ] , we believe , therefore , that this therapeutic approach of not embolising the iia is a viable option in patients with haemodynamic shock or severe ostial stenosis , suggesting close 6 - month follow - up by ceus . the overall incidence of endoleaks recorded in our study ( 15.5 % ) is in line with the literature data [ 15 , 2024 ] : an important observation is the absence of a statistically significant difference in the treatment groups , which highlights that emergency treatment , although burdened by little time for adequate planning , has similar effectiveness to elective treatment . 
it is , however , mandatory to be equipped with a wide range of materials , suitable for all possible situations . pelvic ischaemia is a complication that is frequently seen after endovascular treatment of iliac aneurysms , particularly in patients with unior bi - lateral iia embolisation [ 2 , 3 ]  . 
 in this group of patients , the incidence of endoleaks was 33.3 % ( 3 / 9 ) : we have not yet found a statistically significant difference compared with the group treated with 1 3 conflict of interest the authors declare no conflict of interest . 448 radiol med ( 2015 ) 120 : 421429 doi 10.1007 / s11547 - 014 - 0465 - 1 radiotherapy the first survey on defensive medicine in radiation oncology sara ramella giovanni mandoliti lucio trodella rolando maria dangelillo received : 20 january 2014 / accepted : 30 may 2014 / published online : 30 october 2014 italian society of medical radiology 2014 abstract purpose defensive medicine occurs when doctors order tests , procedures , visits or avoid high - risk patients and procedures , primarily to reduce their exposure to malpractice liability . 
we present here the first survey of radiation oncologists views regarding malpractice liability and defensive medicine practice . materials and methods a three - page questionnaire was sent to 611 active radiation oncologists , members of the italian association of radiation oncology ( airo ) , with questions pertaining to the incidence , nature and causes in their practice of defensive medicine . results a total of 361 questionnaires were completed ( 59 % feedback )  . 
physicians practise defensive medicine by ordering further imaging studies ( 39 % ) or laboratory tests ( 35 % ) , referring patients to consultants ( 43 % ) or prescribing additional medication ( 35 % )  . 
approximately , 70 % declared that the climate of opinion that exists towards doctors is one of the major issues for practising defensive medicine . conclusion although radiation oncology is generally considered a medium / low risk speciality for defensive medicine , the present survey reflects a widespread use of this behaviour in daily practice . 
maria della misericordia , rovigo , italy medical behaviour can be advantageous for implementing programmes aimed at improving awareness of this phenomenon and to increase good clinical practice . keywords defensive medicine radiation oncology survey introduction the congressional office of technology assessment ( ota ) [ 1 ] provided a useful definition of defensive medicine in 1994 : defensive medicine occurs when doctors order tests , procedures , or visits or avoid high risk patients or procedures , primarily ( but not necessarily or solely ) to reduce their exposure to malpractice liability . 
 in 1972 , an interesting article by hershey [ 2 ] entitled the defensive practice of medicine : myth or reality underlined that defensive medicine is a deviation from medical practice that is induced primarily by a threat of liability . as this is a politically sensitive topic , the phenomenon has been studied widely in the us and europe [ 15 ] and has mainly been invoked as an argument for tort reform in the years between malpractice crisis , when other pressures for legal change have ebbed [ 6 ]  . 
in italy from 1994 to 2007 the number of accidents reported to insurance companies has jumped from 9 , 500 to 30 , 000 , a 200 % increase [ 7 ] ; for this main reason , physicians , especially among the younger age group , apply defensive medicine which consequently contributes to an increase in healthcare disbursements . 1 3 422 radiol med ( 2015 ) 120 : 421429 an accurate measurement of this kind of medicine is extremely difficult . 
some authors state that there are only two ways to estimate whether and how frequently procedures are used for defensive reasons : ( a ) asking physicians directly through surveys ; ( b ) linking differences in their actual procedure utilisation rates to differences in their risk of liability [ 8 ]  . recently , a number of authors have identified hard data for the prevalence of defensive medicine among physicians [ 914 ]  . 
several studies have identified specific specialities that are at high - risk for dispute including : emergency medicine , general surgery , orthopaedic surgery , neurosurgery , obstetrics / gynaecology and radiology . 
it was sent in may 2011 to physicians who are members of airo to their email addresses as contained in the airo website . a cover letter providing background information on the study accompanied the survey . 
the questionnaire was based upon the format of similar surveys set out in the relevant literature [ 914 ]  . a 3 - page questionnaire contained questions about practice decisions , factors that have influenced the behaviour as well as demographics data . 
physicians were asked to rate , on a scale from 1 to 8 , the frequency with which they practise the following behaviour : ( 1 ) order more tests than medically indicated ; ( 2 ) suggest invasive procedures against professional judgement ; ( 3 ) avoid caring for highrisk patients ; ( 4 ) prescribe more medication than medically indicated ; ( 5 ) order hospitalisation in a patient who can be managed as an outpatient ; ( 6 ) refer patients to other specialists in unnecessary circumstances ; ( 7 ) include in medical records additional information / remarks which would not have been included if physicians were not worried about legal problems ; ( 8 ) avoid conducting certain high risk procedures / interventions even if to the benefit of patients . respondents who answered affirmatively to one or more of the above questions were asked to indicate which factors determined their behaviour . 
the explanations proposed were : ( 1 ) fear of a claim for damages in the event of complications / adverse events ; ( 2 ) fear of legal argument in case of complications / adverse events ; ( 3 ) fear of disciplinary sanctions by their medical institution in case of complications / adverse events ; ( 4 ) fear of negative publicity , damage to their image , in the event of complications / adverse events ; ( 5 ) previous personal experience of legal problems ; ( 6 ) previous experience of legal argument against a colleague , and finally ( 7 ) the climate that exists today in public opinion towards doctors . 
doctors were asked if the time scheduled for the visits was : less than enough , enough or more than enough . multiple follow - up contacts were made with nonrespondents by mail and telephone during june and july . 
the independent variables were physician characteristics : sex , age , years in practice , professional qualification ( resident ; specialist ; director of department / institute ) and finally hospital affiliation ( public or private )  . results a total of 370 physicians completed the survey . 
after exclusion of nine questionnaires because of file format problems , 361 questionnaires were analysed ( 59 % feedback rate )  . characteristics of respondent physicians table 1 outlines the characteristics of radiation oncologist respondents ( gender , professional qualification , years in practice and primary hospital affiliation )  . 
eighty - two per cent of respondents worked in public hospitals . defensive medicine behaviours excluding 90 respondents ( 25 % ) who declared never to have been affected by this behaviour , the vast majority of respondents ( 75 % ) reported that they had performed 1 3 radiol med ( 2015 ) 120 : 421429 table 1 characteristics of respondent physicians characteristics of respondent no . 
respondent characteristics impacted differently on each of these actions ( table 3 ) : order more tests than medically indicated thirty - nine per cent of respondents reported they ordered more diagnostic tests than medically indicated . 
the vast majority did it once to three times in the last month , one respondent confirmed having done so more than four times , no respondent more than six times . 
table 5 reports how the respondents characteristics impacted differently on each of the following considerations : factors influencing defensive medicine behaviours fear of a claim for damages or of legal litigation in the event of complications / adverse events the vast majority of radiation oncologists ( 72.3 % ) were worried about legal argument and about half of all respondents stated they feared a claim for damages in the event of complications / adverse events . 1 3 424 radiol med ( 2015 ) 120 : 421429 table 2 respondents defensive medicine behaviours and their frequencies in a month order more tests than medically indicated suggest invasive procedures against professional judgement avoid caring for high - risk patients prescribe more medications than medically indicated order hospitalisation in a patient who can be managed as an outpatient refer patients to other specialists in unnecessary circumstances write in medical records additional information that would not have been included if not worried about possible legal problems never 13 times 46 times 79 times 10 times never 13 times 46 times 79 times 10 times never 13 times 46 times 79 times 10 times never 13 times 46 times 79 times 10 times never 13 times 46 times 79 times 10 times never 13 times 46 times 79 times 10 times never 13 times 46 times 79 times 10 times never 13 times 46 times 79 times 10 times fear of disciplinary sanctions by their medical institution or fear of negative publicity , loss of image in case of complications / adverse events disciplinary sanctions by the reference institution , like fear of negative publicity or damage to their image , were not major concerns for respondents ; in fact 77 and 78 % of them disagreed or agreed slightly with the reported sentences , respectively . 
the results of the survey indicate that 93 % of the physicians interviewed confirmed they had practised defensive medicine which included assurance behaviours such as testing , diagnostic procedures and referrals ( 92 % ) , as well as refusing high risk patients or procedures . 
in fact , only 39 % of respondents reported they ordered more diagnostic tests than medically indicated and more than 96 % of all respondents reported that they never suggested invasive procedures which , in their professional judgement , were unwarranted . 
forty - two per cent of respondents indicated they had actively limited their practice in the preceding 3 years in this regard . physicians practising within the high - risk specialities provided data on the impact of defensive medicine within their field and katz et al.s study [ 10 ] outlined that the fear of malpractice suits plays a significant role in decisionmaking in emergency departments and that it was also linked to an increase in hospitalisation time for patients considered low risk together with increased diagnostic testing . 
physicians in emergency departments who had faced numerous malpractice suits had an increased tendency to hospitalise low - risk patients compared with physicians who had not dealt with many malpractice suits . in a number of surveys carried out in the united states covering a number of specialities , a large number of specialists reported varying defensive medicine behaviours based on the fear of malpractice suits : 96 % of all orthopaedic surgeons [ 11 ] ; 59 % of all obstetricians and gynaecologists have increased the number of referrals for the diagnosis of breast abnormalities and 54 % for the treatment of breast disease [ 12 ] ; 4072 % of all neurosurgeons of whom 64 % considered malpractice premiums as a major or extreme burden ; and 45 % of all respondents overall avoided high - risk procedures due to liability concerns . 
furthermore , 61 % confirmed they had requested a larger number of diagnostic tests than required and 26 % had refused to care for high - risk treatment patients over and above the usual precautionary rules . the defensive medicine behaviour of over - prescription was reported by 54 % of radiologists , while 37 % reported having referred patients . 
the outcome of the survey confirmed that in italy the behaviour was practised by over 50 % of all doctors and impacted 10 20 % of all prescriptions . up to now , no data have been available with regard to radiation oncologists and the survey undertaken revealed that the impact of defensive medicine behaviour resulted in 39 % of all respondents requesting imaging studies and 35 % laboratory tests which would otherwise not have been requested , and 43 % consulted with colleagues for the same reason . table 6 outlines the comparison between results of the survey undertaken with those contained in studderts survey [ 9 ] and in the survey carried out by the medical council of rome [ 14 ]  . 
nonetheless , the problem should not be underestimated at either the national or international level and every effort should be made to improve the current situation . 1 3 radiol med ( 2015 ) 120 : 421429 1 3fl 428 radiol med ( 2015 ) 120 : 421429 1 3fi radiol med ( 2015 ) 120 : 421429 to address the problem , it is important to have a clear understanding of why this defensive behaviour is adopted and what are the underlying factors that influence it , including fear of malpractice suits and claims for damages , especially among young radiologists . 
respondents in both studderts survey ( 29 % ) and our survey ( 31.6 % ) are of the opinion that the time allocated for medical visits is not sufficient ; 62 % believe that the allocated time is sufficient while 9 % feel it is more than sufficient . one of the most important concerns deriving from defensive medicine behaviour is the high costs associated with it [ 16 ] , and the real costs incurred are hard to discern . 
a study was undertaken in 2006 by price waterhouse coopers [ 17 ] on behalf of americas health insurance plans , and the results indicated that costs associated with medical liability account for 711 % of health insurance premium dollars . 
the survey also indicated that the direct legal costs and the overall defensive medicine behaviour increases healthcare spending by 10 % , with a disproportionate increase in outpatient and physician costs . hellinger and encinosa [ 18 ] report that the existence of laws curbing malpractice payments actually decreases state healthcare payment by 34 % . 
radiation oncology in comparison with other areas such as emergency medicine , general surgery , orthopaedic surgery , neurosurgery , obstetrics / gynaecology and radiology cannot be considered a high - risk field with regard to defensive medicine behaviour . 
however , in the light of the differences in behaviours identified in this survey , it could be advantageous to investigate which radiation oncologist categories are more prone to defensive medical behaviour so as to implement programmes aiming at improving awareness of the phenomenon and to increase good clinical practice . conflict of interest dr sara ramella has no conflict of inter est to declare . 
patients in group a underwent injection of the sclerosing agent through an angiographic diagnostic catheter ( free catheter technique ) and patients in group b through an ob catheter ( ob technique )  . 
the fischers test was used for statistical analysis . results we evaluated a total of 90 patients because five patients for each group were not included in the statistical analysis owing to technical problems or complications . 
in group a , lsv rupture occurred in four cases ( 8 % ) so the procedure was completed by sclerosant injection through the ob located distally to the lesion . 
tsetis department of radiology , medical school of crete , university of crete , heraklion , greece 1 3 484 radiol med ( 2015 ) 120 : 483488 underwent ob injection to stop the flow to the shunt , and was not included for statistical evaluation . 
in group b , vein rupture with contrast leakage was noted in six cases ( 12 % ) ; nonetheless , all the procedures were completed because the ob was positioned distally to the vessel tear , obviating any retrograde leakage of sclerosant . 
in group b , in five cases ( 10 % ) , we were unable to advance the ob though the lsv ostium so the procedures were completed with the diagnostic catheter and not considered for statistical evaluation . conclusion on the basis of our data , the embolisation of the lsv obtained by injecting the sclerosant through an ob rather than through a diagnostic catheter seems to be more effective in achieving total vein embolisation , as well as allowing a controlled injection of sclerosant even in cases of vein rupture . keywords varicocele spermatic vein embolization occluding balloon sclerosing agent introduction percutaneous treatment of varicocele started approximately , four decades ago and now represents an effective alternative to surgery [ 1 ]  . 
the technique consists of injecting a sclerosing agent into the distal portion of the spermatic vein ( sv ) with common femoral , internal jugular or antecubital venous access through an angiographic diagnostic catheter ; a distal barrage near the external inguinal ring is used to prevent the sclerosant flowing into the scrotal veins during a valsalva manoeuvre . 
a variation to this technique refers to the use of a temporary proximal occluding balloon ( ob ) catheter in addition to distal barrage , to stop the retrograde blood flow ; this technique is suggested in cases of large sv , or in patients with bidirectional flow because of increased cardiac output , as suggested by a recent review [ 2 ]  . 
in this case , the sclerosant is injected through the ob catheter into the distal portion of the sv . our hypothesis in varicocele treatment is that this technique to stop the flow using an ob allows for a controlled injection of sclerosing agent and constant contact between the sclerosant and the vessel wall with the highest concentration ; with the standard technique , the concentration of sclerosant is related to the flow and the calibre of the left spermatic vein ( lsv ) and dependent on the valsalva manoeuvre held by the patient . 
no comparison exists in the literature between these two techniques for lsv embolisation . materials and methods patients from january 2012 to september 2013 , we prospectively enrolled 100 patients ( age range 14 to 38 years ; mean age 25 years ) with left varicocele and an indication for retrograde lsv sclerosis for varicocele ; the patients were previously randomised to two groups ( we wrote a list of 100 lines assigned casually with a or b and each patient was allocated to group a or b on the basis of this list )  . 
in the same period , four patients refused to be enrolled in the study . the study was approved by the institutional review board and every patient in the study provided signed informed consent to be enrolled in the study and undergo the procedure . patients in group a ( age range 1538 years ; mean 23 ) underwent sclerotic agent injection through an angiographic diagnostic catheter ( free catheter technique ) and patients in group b ( age range 1437 year ; mean 26 years ) through an ob catheter ( ob technique )  . 
total occlusion of the lsv at post - treatment phlebography with a valsalva manoeuvre was considered a technical success . in cases of incomplete occlusion of the lsv at posttreatment phlebography , the procedure was completed with coils . 
retrograde sclerotherapy was performed in the outpatient clinic with the patient under local anaesthesia . technique in both groups , an ultrasound - guided percutaneous access in the right common femoral vein was used and a 5 fr valved introducer was positioned . 
the lsv was catheterised with a 0.035 hydrophilic guidewire ( terumo corporation , tokyo , japan ) and with a c2 or c1 5 fr cobra - shaped ( terumo corporation , tokyo , japan ) angiographic diagnostic catheter in both groups . 
in all patients , a rubber band was applied at the highest level of the scrotum , as a distal barrage to avoid reflux of the sclerosant into the scrotal vein and prevent phlebitis . 
a mixture of lauromacrogol foam ( 3 % atoxysclerol , kreussler pharma , wiesbaden , germany ) and air was injected to perform sclerotherapy . standard technique after diagnostic phlebography performed using a c2 or c1 cobra - shaped hydrophilic angiographic diagnostic catheter , a hydrophilic guidewire was used to ensure that the catheter tip reached the most distal part of the lsv . 
once distal catheterisation was obtained , a rubber band was applied 1 3 radiol med ( 2015 ) 120 : 483488 at the highest level of the scrotum and contrast media was immediately injected during a valsalva manoeuvre to check that there was no reflux in the vessels below the rubber band . free catheter technique after lsv catheterisation , depending on the size of the veins at phlebography , a foam containing 25 ml of sclerosant ( 70 % ) mixed with air ( 30 % ) was injected during a smooth valsalva manoeuvre , held as much as possible . 
phlebography was then performed to visualise collaterals not previously seen with free flow and to measure the amount of contrast agent needed to fill the vein between the ob and the rubber band . 
thus , the same amount of sclerosant foam ( range 26 ml ) containing 70 % of sclerosant and 30 % of air was injected without any valsalva manoeuvre with stopped flow for 10 min ( proximal and distal barrages )  . 
if systemic collaterals were seen at pre - injection phlebography , we injected a low dose of sclerosant with contrast and the injection was stopped once the origin of the collaterals was seen . 
the ob was then deflated and if phlebographic control , during valsalva manoeuvre , revealed a reduced but persistent flow in the distal lsv , the procedure was completed by insertion of coils . data analysis complete occlusion of the lsv at post - procedural phlebography was considered a technical success . 
2 a a balloon is advanced to the distal portion of the vein and inflated ( white arrow ) while a rubber band is applied in the proximal portion of the scrotum , so there is no blood flow between the two bar rages . 
in group a , vein rupture occurred in four cases ( 8 % ) so the procedure was completed by injection of sclerosant through the ob located distally to the lesion to avoid the possible outflow of sclerosant with the risk of stricture of the ureter [ 3 ]  . 
in another case , a high flow shunt towards the inferior vena cava was detected , the patient underwent ob injection to stop the flow to the shunt also this patient was not included in the statistical evaluation . 
 the rates of vein rupture and haematoma were not significantly different between the two groups . follow - up cdus examination at 3 months detected no pathological reflux in the left pampiniform plexus in 40 patients of group a ( 88.8 % ) and in 42 patients of group b ( 93.3 % ) ; the difference was not statistically significant . discussion several embolisation techniques have been reported for spermatic vein varicocele . 
retrograde sclerotherapy can be nowadays considered the most effective and safe procedure . many authors state that if reflux persists at post - sclerotherapy phleography , the procedure must be completed with coils [ 25 ]  . 
traditional coils carry a high rate of recurrence ( 20 / 30 % ) and can be associated with several even serious complications such as coil migration , venous dissection , and venous perforation , while fewer technical complications have been reported with detachable coils [ 6 ]  . 
 also glue embolisation , frequently used in cases of persistent and recurrent post - surgical varicoceles , has been associated with serious complications such as glue migration into the pulmonary circulation , glued catheter and severe venous phlebitis [ 7 ]  . 
as has been reported to be effective in cases in which retrograde percutaneous procedure was impossible or in some surgical recurrences ; however , this technique is not widely used [ 8 ]  . a recent review recommends the use of sclerotherapy as the standard percutaneous approach for varicocele [ 2 ]  . 
the authors also indicated some important steps to make the embolisation more effective , in particular : ( a ) to perform the procedure with the catheter tip in the most distal part of the sv ( generally the catheter tip must reach the lower edge of the ischiopubic ramus ) ; ( b ) once distal catheterisation is obtained , a rubber band must be applied at the highest level fig . 
d phlebography shows the post - procedure occlusion of the left spermatic vein of the scrotum and contrast material immediately injected during a valsalva manoeuvre to check that there is no reflux below the rubber band ; ( c ) sclerosant must be injected during the valsalva manoeuvre . commonly the sclerosant is prepared in foam form , more or less as described by tessari et al . 
in 1999 for the treatment of varicose veins [ 9 ] , by mixing together the contents of two syringes , one containing the sclerosant and the other containing air , connected through a two - way stopcock . 
the rationale for using foam is because the distribution of the sclerosing agent on the endothelial surface is improved resulting in more effective embolisation , also allowing simultaneous sclerotherapy of multiple collateral branches . good results have been achieved with different sclerosing agents such as sodium tetradecyl sulphate , hydroxypolyethoxy - docanol and sodium morrhuate solution [ 1012 ]  . 
 1 3 radiol med ( 2015 ) 120 : 483488 the most popular foam sclerosing agents used in the literature include sodium tetradecyl sulphate and polydocanol ; however , no comparative study exists evaluating neither the different injection techniques nor the different sclerosing agents . this study was devised based on the rationale that by achieving the stop flow in the distal portion of the lsv , we are able to isolate the vessel between the ob and the rubber band in the distal portion of the external inguinal ring , so that the injected amount of sclerosant agent would be in contact with the vessel wall for the total time of occlusion at the highest concentration . 
the objective of brto is to completely obliterate the gastric varices with preservation of the anatomical hepatopetal flow of the splenoportal cir culation , using a controlled sclerosant injection through an ob catheter or microcatheter [ 15 ]  . use of the ob technique in the treatment of lsv does not require any valsalva manoeuvre and could therefore be even more comfortable for patients . 
when injecting the sclerosant through the diagnostic catheter , its concentration is related to the patients ability to hold a deep valsalva manoeuvre , so that the sclerosant could be diluted in cases of ineffective or intermittent valsalva manoeuvre , in particular in patients who have pain or need sedation . 
some authors between 1981 and 2005 [ 1619 ] described an air - block technique , in which a small amount of air was injected before the sclerosant injection to avoid dilution of the liquid , but this technique showed only partial effectiveness and is basically no longer used today [ 20 ]  . 
with the ob technique , by advancing the balloon through the lesion , we were able to stop the flow and inject sclerosant agents also in those cases . this study presents a major limitation . 
so far , there have been only a few sporadic reports of single - centre trials investigating computer systems for the storage of the dose [ 6 , 7 ]  . the current ct systems display on the screen of the device both the computed tomography dose index ( ctdi ) and the dose - length product ( dlp ) , before and after the execution of the examination [ 8 ]  . the ctdi is an index of local dose , which is independent of the length of the scanned volume . 
the ctdi was 1 3 radiol med ( 2015 ) 120 : 466473 developed to provide a standardised method for comparing the output level of radiation between different ct scanners using a phantom reference ( head or body , measuring 16 and 32 cm in diameter , respectively )  . 
to better represent the radiation dose in ct examinations also performed in helical mode , the ctdivol ( ctdi volumetric ) was introduced , which also takes into account the pitch [ 9 ]  . the ctdivol remains , however , a dose index independent of the length of the scan . 
the dlp is obtained by multiplying the ctdivol by the length of the scan [ 10 ]  . both of these dosimetric quantities are sensitive to the variation of scanning parameters , such as tube voltage ( kvp ) , current ( mas ) , gantry rotation time , pitch and bowtie filtration , but they are both independent of the size of the patient [ 9 , 10 ]  . 
in fact , for a given ct scan of a patient , the ctdivol and its dlp are displayed for a reference phantom ( head or body ) , the diameter of which ( 16 or 32 cm ) is selected by the scanner . 
in general , the first is selected for ct scans of the head , while the second for the examinations of the torso ( chest and abdomen ) [ 11 ]  . for paediatric patients the head phantom should always be selected , even if , for paediatric body ct protocols , some systems use the 16 - cm phantom as a benchmark and others use the 32 - cm phantothis is a problem as it may cause an underestimation of dose levels in the younger paediatric patients if the 32 - cm phantom is used as a ref . 
for these two reasons , it does not allow a specific estimate of the radiation dose for a given individual , particularly in paediatrics [ 13 , 14 ]  . radiologists , medical physicists and radiographers need computational tools which are easy to use and estimate the radiation dose as accurately as possible [ 15 ]  . 
to provide these tools , not only for paediatric ct examinations but also for ct examinations of adult patients of any size , a working group ( aapm task group report 204 , 2011 ) was appointed to develop conversion factors that could be applied to the dose index the ctdivol displayed on the ct scanner [ 8 ]  . 
this way , a new parameter is obtained that allows an estimate of patient dose according to the individuals specific dimensions , which is called a size - specific dose estimate ( ssde )  . the ssde was defined in the report of aapm task group 204 as the estimation of dose to the patient that takes into account the corrections based on linear dimensions measured in the same patient or in ct images . 
the values of the ssde are specifically based on the ctdivol reported in the ct scanner ( measured conventionally using a 16 or 32 - cm pmma phantom ) , which is normalised by factors dependent on patient size . 
this normalisation process does not take into account most of the differences between each scanner and the settings of the scanner tube voltages , but it is very important because it allows us to estimate the radiation dose to the patient depending on the type examined , finding its greatest benefits for ct scans of children or small adults [ 13 , 14 ]  . the correction factors to be applied to the ctdivol in order to derive the ssde have emerged by combining the results from four research groups that worked independently of each other [ 8 ]  . 
the measurement methods and tools used were different for each group and this further extends the experimental validity which allowed the size - dependent conversion factors to be obtained and tabulated . 
common to all the working groups , to obtain the correction factors , was the calculation of some quantities associated with the related size phantoms used and subsequently transported to the resulting tables , which are necessary to determine the appropriate correction factor for each individual patient . 
these measurements can be derived from the centring images ( scout views ) of the ct scan or from some axial ct scans acquired in certain areas of the body . the effective diameter is the diameter of the patient in a specific position along the z axis , assuming that he has a circular cross section . 
the effective diameter can , therefore , be thought of as the diameter of a circle whose area corresponds to that of a cross section of the patient on an image . 
 [ 16 ] the effective diameter is the parameter with less variation for the calculation of the ssde . our study aimed to evaluate the appropriateness of the dose indices and focuses mainly on the comparison between the ctdi and the ssde in body ct of both adult and paediatric patients , who present a more critical situation . 
for paediatric patients the acquisition protocol for abdominal and thoracic ct was : helical scan , automatic mas , 80100 kv , 1 < 1.3 , gantry rotation time 25 mm slice thickness , pitch 0.5 s , small acquisition fov . the paediatric patients were divided according to age group ( 03 , 410 , 1118 years )  . we used the software dosewatch ( ge , milwaukee , usa ) to extract and collect the dosimetric data . 
along with the collection and storage of dosimetric data , the programme also offers statistical analysis , integrated connections with ris and pacs , automatic alarms and tools to optimise the dose and the image quality . the following dosimetric data were recorded : the ctdivol , the type of phantom used for the calculation of ctdi and the dimensional parameters necessary for the ssde calculation , in particular : the lateral dimension ( lat ) , the lat dimenanterior - posterior dimension ( ap ) , the ap sion and the effective diameter . 
we calculated the patients effective diameter according to the formula : ap lat . the ssde of each patient was then calculated through the ctdivol , the effective diameter and tables that show the conversion factors , as reported by aapm report n . 
we evaluated the evolution of the sizes of paediatric patients in relation to the phantoms taken into account for the calculation of ctdi . results analysing the data of the adult patients we obtained the results shown in tables 1 and 2 . 
the average percentages of difference between the two parameters are greater than in adults and close to 50 % ( 46.9 % in thoracic ct and 48.5 % in abdominal ct )  . 
in all the cases examined , to calculate the ctdivol we used the head phantom , whose dimensions do not differ 1 3 radiol med ( 2015 ) 120 : 466473 fig . 
1 thoracic ct scan in which the patient has smaller dimensions than the phantom , for which the percentage difference between the sizespecific dose estimate ( ssde ) and the computed tomography dose index ( ctdivol ) is 65 % fig . 
2 abdominal ct scan in which the patient has smaller dimensions than the phantom , for which the percentage difference between the ssde and the ctdivol is 91 % particularly from the average effective diameter detected ( 13.38 cm ) in this age group . 
4 abdominal ct scan of a 3 - year - old patient in which the percentage difference between the ssde and the ctdivol is 129.8 % 1 3 radiol med ( 2015 ) 120 : 466473 fig . 
5 distribution of the effective diameter ( x - axis ) of thoracic ct in paediatric patients ( y - axis ) there were maximum percentage differences of 106.1 % ( 410 years ) and 84 % ( 1118 years )  . 
in these cases the ct scanner used the body phantom ( 32 cm in diameter ) for the calculation of the ctdivol , which is much larger ( even double ) compared to that of the paediatric patients examined . 
these phantoms do not reflect the general population and are also often chosen inappropriately by the ct scanner , especially in the paediatric examinations , where even if a patient has an effective diameter of about 16 cm , the ct scanner will use the 32 - cm phantom for the calculation of the ctdivol . analysing the data separately in thoracic ct and abdominal ct , very high differences ( up to 91 % ) were also detected , indicating an underestimation by the ctdivol of the radiation dose , or even negative ( up to 15 % ) which , on the contrary , indicates an overestimation of the dose . very high or negative percentage values are a consequence of the size of the patient , respectively , smaller or larger than the reference phantom used to obtain the ctdivol . 
in all these cases , the ctdivol is , therefore , inappropriate in the estimation of radiation dose , as not corresponding to the delivered dose for that patient , but referred to a standard reference phantom , the dimensions of which deviate from the actual dimensions of the patient . 
the ssde , on the other hand , takes into account the size of the individual subjected to the specifications and therefore more accurately expresses the dose delivered . analysing the overall average values of the ssde and the ctdivol in paediatric patients , without distinguishing by age , one can immediately see how the percentages of difference between the two parameters are greater than in adults , close to 50 % ( 46.9 % in thoracic ct and 48.5 % in abdominal ct )  . 
patients between 0 and 3 years old show a low percentage of difference between the ctdivol and the ssde ( 11.2 % ) , with a maximum of 26.8 % and a minimum of 1 % . 
these values reveal an inappropriateness of the ctdivol to estimate the radiation dose to the patient , since it underestimates the average dose by more than 50 % . maximum percentage differences of 106.1 % ( 4 10 years ) and 84 % ( 1118 years ) are also reached . 
in these cases , for the calculation of the ctdivol the ct scanner uses the body phantom ( 32 cm in diameter ) , which is much larger ( even double the size ) compared to the paediatric patients examined . 
6 , the peak is at 1520 cm in diameter , a value that is close to the size of the head phantom ( 16 cm ) , but which differs greatly from the body phantom ( 32 cm )  . 
 the wide range of values , however , indicates a wide dimensional variety among patients of different ages , but also between patients of the same age , which does not allow the ctdivol an accurate dose estimation , given that it refers only to two standard measures . 
for this reason , even in the abdominal ct of paediatric patients the measurement of the ssde is more precise . in most cases the ctdivol underestimates the radiation dose in small - sized adult patients and in paediatric patients with a peak percentage difference of up to approximately 130 % compared to the ssde . 
 therefore , it is not a dosimetric index specific for each patient , but above all it is a surrogate of the output of the ct scanner , as already reported by some papers [ 13 , 14 ]  . the ssde is a good tool to estimate the average radiation dose for a given patient before a ct study , based on the input parameters and the size of the specific person to be examined , but it is not correct for the differences in the distribution of the dose to organs [ 16 ]  . given that the majority of modern ct scanners can display the ctdivol before a scan , the correction factors proposed can be used by the technician or by the radiologist to estimate in advance the specific radiation dose for that patient , so as to have a feedback on the appropriateness of the parameters associated with size . 
this way , the accuracy of dosimetry is improved compared to using only the scanner output ( ctdivol ) as a surrogate of the radiation dose to the patient . conclusions the results obtained indicate that it is important that the dose recording systems appearing on the market are able to calculate and record the ssde for each patient . 
such systems are good tools for the optimisation of the examination not only from a dosimetric point of view , but also as an analysis of incorrect patient positioning with respect to the scanner coordinates , allowing for a more accurate 1 3 radiol med ( 2015 ) 120 : 466473 evaluation of the examination in general . 
the aim of our study was to evaluate the incidence of magnetic resonance ( mr ) imaging changes in the ion after surgery in a large cohort of paediatric patients and to determine their correlation with tumour grade . materials and methods we retrospectively evaluated 58 patients treated surgically for pcf tumours who underwent mr imaging between 2007 and 2014 , 1 week to 5 years after surgery . 
knowledge of this condition can prevent misdiagnoses and unnecessary investigations . keywords olivary degeneration inferior olivary nuclei guillainmollaret triangle dentato - rubro - olivary pathway mri introduction olivary degeneration is a transneuronal degeneration as a consequence of lesions involving the dentato - rubro - olivary pathway , also known as the guillainmollaret triangle [ 1 ]  . 
since fibers projecting from the dentate nucleus into the ion are mainly inhibitory ( gabaergic ) , injury to the dentato - rubro - olivary pathway determines hypertrophy and enlargement of the inferior ion ; for this reason , olivary degeneration is usually known as hypertrophic olivary degeneration ( hod )  . 
specifically , damage to the dentate nucleus and / or to the superior cerebellar peduncle leads to contralateral ion damage , while damage to the tegmental tract leads to ipsilateral damage . 
a 1 3 radiol med ( 2015 ) 120 : 474482 between pfs and bilateral ion degeneration ( p < 0.001 ; positive predictive value , ppv : 100 % ) after surgical resection of pcf midline tumours in paediatric patients . 
however , to our knowledge , there are still inconsistent data concerning mr imaging findings of ion degeneration after surgery for pcf primary malignant brain tumours in the paediatric population . therefore , the purpose of our study was to evaluate the incidence of olivary degeneration after pcf surgery in a large cohort of paediatric patients and to determine the possible correlations between tumour grade and ion degeneration . 
moreover , typical mr imaging findings of ion degeneration are described , also considering the time correlation between surgery and mr imaging evidence of ion changes . materials and methods in this retrospective study , we evaluated 58 paediatric patients , 26 male and 32 female , aged 814 years , who were treated surgically for pcf tumours in our institution . 
every patient underwent clinical and radiological follow - up by serial mr examinations ; because of this and of the retrospective design of the study , no ethical committee approval was required . we evaluated all mr studies performed between 2007 and 2014 at variable time intervals after surgery ( from 1 week to 5 years )  . 
clinical conditions arising shortly after pcf surgery and related to pfs were also examined , and they included mutism ( 12 / 58 ) , ataxia ( 16 / 58 ) and dysmetria ( 13 / 58 )  . all examinations were obtained using a 1.5 tesla system ( general electric medical systems , inc . , milwaukee , wi )  . 
the imaging protocol was acquired using thin sectionss ( 3 mm ) and included standard axial and sagittal t1 - weighted fast spin echo sequences ( fse ) ( tr 500 12 ms ) , t2 - weighted fse images acquired 650 ms ; te in the axial and coronal plane ( tr 3 , 3004 , 000 ms ; 120 ms ; ery images ( flair , tr 2 , 200 ms ) , axial t2 * weighted images gradient echo ( gre ) ( tr 2025 ms ) , and sagittal , coronal and axial contrast - enhanced t1 - weighted fse 12 ms )  . 
in all patients , sequences ( tr 90120 ms ) , axial fluid - attenuated inversion recov9001 , 300 ms ; te 500650 ms ; te 8 , 000 ms ; te fig . 
1 guillainmollaret triangle : the coronal t2 - weighted image shows the connections between the red nucleus ( black dot ) , the ipsilateral inferior olivary nucleus ( ion ) ( white dot ) , and the contralateral cerebellar dentate nucleus ( grey dot ) , through the central tegmental tract , dentato - rubro - olivary tract and olivary - dentate tract , respectively long - lasting uncontrolled excitation of the ion is responsible for neuronal death with subsequent atrophy . 
ion changes are well detectable in both pathological evaluation and magnetic resonance ( mr ) imaging findings that consist of focal ion t2w hyperintensity and possible ion enlargement [ 2 , 3 ]  . a variety of lesions involving this functional triangle may cause the development of olivary degeneration . 
in the literature , mr imaging evidence of hod is also described as a consequence of pcf surgery of primary lesions in the brainstem or cerebellum , and they mostly regarded adult populations with pontine cavernous angiomas or haemorrhages . 
as reported in the literature [ 11 ] , each examination was assessed for the following parameters : ( 1 ) signal intensity of ion in t2 - weighted and flair images ; ( 2 ) olivary dimension ( normal , enlarged , atrophic ) ; ( 3 ) signal intensity alterations and evidence of previous haemorrhages along the dentato - rubroolivary pathway ( red nucleus , dentate nucleus , central tegmental tract , superior cerebellar peduncles ) that could explain ion degeneration . the findings were analysed according to time interval between surgery and mr examinations , and divided in four groups , as reported in the literature [ 3 , 9 ] : 1 . 
pathological examination showed 14 medulloblastomas , four pilocytic astrocytomas and one anaplastic ependymoma ( table 1 )  . statistical analysis demonstrated a significant ( p 0.005 ) correlation between the mr imaging findings of ion 1 3 radiol med ( 2015 ) 120 : 474482 degeneration and high tumour grade , since 15 out of 19 patients with ion alterations were affected by high - grade tumours , while 23 out of 39 patients without ion alterations had low grade tumours . mr imaging findings in all 19 patients with ion degeneration , mr imaging showed focal high signal intensity on t2 - weighted images in ion , bilateral in 15 and unilateral in four ; olivary hypertrophy was associated with signal alterations in only 7 / 19 patients . 
other lesions along the dentorubro - olivary pathway involved the red nucleus ( 2 / 19 ) and superior cerebellar peduncles ( 10 / 19 ) ( table 1 )  . 
t2 * weighted sequences depicted haemosiderosis in the dentate nucleus in 2 / 19 patients , in the red nucleus in 2 / 19 patients and in the superior cerebellar peduncles in 4 / 19 patients . 
between 1 and 6 months the ion t2 hyperintensity was evident in all 19 patients , with higher signal intensity in 15 out of 19 ( 79 % ) compared to the follow - up during the first month . 
 between 6 months and 1 year , the ion t2 hyperintensity showed a trend to a progressive decrease , and after 1 year it became faint , with linear or punctate appearance in 11 / 15 patients ( 73 % )  . 
2. time interval versus olivary size considering time evolution of olivary size during the first month , it was generally normal , except for one patient ( 5.2 % ) who showed a mild hypertrophy . 
1 < 1 month ( 19 patients ) , 2 16 months ( 19 patients ) , 3 6 months1 year ( 17 patients ) , 4 > 1 year ( 15 patients ) after 1 year this trend inverted , with evidence of slight olivary enlargement in only 2 / 15 patients ( 13 % ) and atrophy appearing in 3 / 15 patients ( 20 % )  . 
2. discussion olivary degeneration is a transneuronal degeneration resulting in hypertrophy of the targeted region , rather than atrophy , as commonly occurs in the central nervous system ; for this reason , it is commonly called hod . 
this hypertrophic variant of degeneration is not limited to the ion , in fact it has been described in the dorsal root ganglion and dentate nucleus [ 12 ]  . 
the mechanism thought to be the cause of this alteration is trans - synaptic degeneration [ 4 , 13 ] , which has also been described in other areas of the brain , including the lateral geniculate body and fornix [ 14 ]  . 
 it is believed that the loss of a functional synapse leads 1 3 478 radiol med ( 2015 ) 120 : 474482 to anterograde degeneration and atrophy ; however , ion shows hypertrophy of both neurons and glia . 
this may be related to the increase in spiny dendrites and mitochondria , to maintain active connections , due to uncontrolled excitation of the ion . histologically the affected ion demonstrates cell body enlargement , vacuolation of the cytoplasm , astrocytic hyperplasia and proliferation , demyelination , and fibrillary gliosis [ 2 ]  . 
 [ 2 ] reported the sequence of pathological changes in ion , describing six phases of pathological changes over a time frame ranging from immediate onset to several years : ( 1 ) first hours : no olivary change ; ( 2 ) up to 7 days : degeneration of olivary amiculum ; ( 3 ) up to the third week : mild olivary hypertrophy ( neuronal hypertrophy without glial reaction ) ; ( 4 ) up to 8 months and a half : olivary enlargement ( neuronal and astrocytic hypertrophy ) ; ( 5 ) after 9 months and a half : olivary pseudohypertrophy ( neuronal loss and presence of gemistocytic astrocytes ) ; ( 6 ) after some years : olivary atrophy . 
3 post - surgical magnetic resonance ( mr ) imaging changes in the ion 1 month after posterior cranial fossa ( pcf ) surgery : axial t2 - weighted and fluid - attenuated inversion recovery ( flair ) images ( a , c ) show bilateral signal hyperintensity within both ion together with a mild hypertrophy ; the t2 * - weighted sequence ( b ) detects the presence of haemosiderin deposits along the surgical margins adjacent to the dentate nuclei ( right > left ) as a consequence of the midline approach . 
coronal t2 - weighted image ( d ) confirms the post - sur gical glioticmalacic changes in both dentate nuclei 1 3 radiol med ( 2015 ) 120 : 474482 ion changes were depicted predominantly by a t2 signal intensity alteration , while olivary enlargement ( hypertrophy ) was found in the minority of our cases ( 7 / 19 )  . 
the low incidence of olivary enlargement , when compared to the literature data [ 9 , 18 ] , is probably related to the relative lack of haemorrhagic lesions along the dentate - rubro - olivary pathway in our population . 
however , blood and derivates could play an irritative role on the dento - rubro - olivary pathway , specifically when dentate nuclei are involved , triggering an uncontrolled excitation of the ion . 
in most of our cases , however , t2 * - weighted images showed poor evidence of haemosiderin in the dentate nuclei . we also found a statistically significant correlation between the development of ion alterations and highgrade tumours , demonstrating a strong association with medulloblastomas ( 14 / 19 ) , in accordance with patay and sanverdi [ 10 , 16 ]  . 
mr imaging 1 - year follow - up ( d ) demonstrates a decrease in olivary enlargement and a persistent faint ion signal hyperintensity 1 3 480 radiol med ( 2015 ) 120 : 474482 first month , increasing with time together with hypertrophy , both reaching a peak at around 6 months . 
however , in our large patient cohort , only few of the patients among the 19 with ion changes reported symptoms of pfs , specifically four patients showed mutism , four ataxia and three dysmetria , and they were most often associated . 
on the other hand , the same symptoms were present even in patients without ion alterations ( 8 / 39 were affected by mutism , 12 / 39 by ataxia and 10 / 39 by dysmetria )  . 
furthermore , these clinical conditions might overlap with those caused by the presence of pcf tumour itself before surgery . other clinical features of olivary degeneration include palatal myoclonus , dentate - rubral ( or holmes ) tremor and ocular myoclonus [ 20 ] , and they have mostly been described in the literature as a consequence of haemorrhage and vascular malformation involving the posterior fossa [ 4 , 5 , 8 ]  . 
 however , not all cases of ion degeneration are accompanied by palatal tremor [ 20 ] , as reported in the literature [ 2124 ] ; moreover , the symptoms might be undetectable in fig . 
of course , a complete analysis of features of all the other sequences has to be done in order to achieve the correct diagnosis ; for example , a lack of contrast enhancement is against many tumours or infections , even though a case of positive enhancement has been recently reported [ 25 ]  . 
 this study was performed to investigate if magnetic resonance imaging ( mri ) - guided transrectal biopsy ( mrgb ) increases diagnostic performance in individuals with suspected prostate cancer ( pca )  . materials and methods twenty - three consecutive men with a total psa > 4 ng / ml , psa density > 0.15 , psa velocity > 0.75 ng / ml / year and suspicious mri findings were included ( average age 64 years ; age range 5375 years ; total psa levels ranging from 4.7 to 54 ng / ml ; median 9 ng / ml )  . 
mrgb was performed with a closed unit at 1.5 tesla , an mri compatible biopsy device , a needle guide , and a titanium double - shoot biopsy gun . result at prebiopsy mri , in the 23 patients , a total of 26 suspicious areas to which the mrgb should be directed were found , 23 of them in the peripheral zone and three in the transitional zone . 
the incidence of pca has increased with life expectancy , and more cancers are detected as a result of wider screening and determination of prostate - specific antigen ( psa ) level in seru determination of serum psa levels is considered useful for the early identification of pca [ 2 ]  . 
the american urological association and the american cancer society recommend that all men aged 50 years or older undergo an annual digital rectal examination ( dre ) and determination of psa level . 
patients with psa levels greater than 4 ng / ml or with suspicious find ings at dre are candidates for further diagnostic workup by means of systematic transrectal ultrasonography ( trus ) - guided biopsy . 
up to now , trus - guided biopsy ( trusgb ) , sampling 612 cores , one to two for each sextant , has been the diagnostic standard for pca for many years . 
with this method , up to 30 % of cancers are missed when performing sextant biopsies , because more than 40 % of pcas are isoechoic and the operator cannot reliably visualise tumour . 
although taking more cores seems to improve the per - patient detection rate of pca , the vastly invasive approach of placing up to 45 1 3 572 radiol med ( 2015 ) 120 : 571578 needles needs to be carefully taken into account . 
furthermore , even if random trusgb is performed with a saturation or template mapping method , it does not solve the problem due to increased costs , complications , over - detection rates and a small but significant risk of missing highgrade cancer . 
trusgb has a negative predictive value of 7080 % ; thus , up to 2030 % of patients with a negative biopsy may still have pca [ 3 ] , 23 % of whom at high risk of pca [ 2 ]  . 
second , third , and fourth repeat biopsies are reported to detect cancer in only 2527 , 524 , and 421 % of cases , respectively [ 3 , 4 ]  . 
furthermore , because pca is multifocal in 85 % of cases , trusgb may underestimate the extent and grade of cancer , which can result in gleason upgrading after radical prostatectomy ( rp )  . 
it is well documented that approximately 30 % of men who undergo rp for low - grade disease are upgraded on final pathology [ 5 ]  . at present , multi - parametric magnetic resonance imaging ( mp - mri ) which combines anatomical t2 - weighted imaging ( t2wi ) with functional techniques such as diffusion - weighted imaging ( dwi ) which highlights cell proliferation , dynamic contrast - enhanced imaging ( dcei ) which shows neoangiogenesis and mr spectroscopic imaging ( mrsi ) which displays cell metabolism is considered to be the most reliable imaging biomarker for pca diagnosis [ 610 ]  . 
multiple studies have now shown that mp - mri can help to identify tumours missed on biopsy , thus increasing biopsy yields with fewer core samples [ 10 ]  . 
many of these tumours are transitional zone tumours which are deep in the prostate and distant from the sites typically reached with a standard trusgb approach [ 10 ]  . 
currently , many studies have proved that mr - guided prostate biopsy ( mrgb ) shows a high detection rate for the diagnosis of pca compared to standard trusgb [ 1116 ]  . 
mrgb can be performed in either dedicated ( interventional ) lowfield systems or clinically widely available mri scanners ( 1.5 tesla field strengths )  . in view of the improved detection of pca with mp - mri , the purpose of this study was to describe our preliminary experience with a biopsy device developed for mrgb with a closed mr unit . materials and methods patient population the use of the devices and procedures described here was approved by the institutional ethics committee . 
all patients were informed in detail before giving their written consent . twenty - three consecutive male patients ( average age 64 years ; age range 5375 years ; total psa levels ranging from 4.7 to 54 ng / ml ; median 9 ng / ml ) , with highly suspected pca who referred to our institution from march 2014 to may 2014 , were enrolled in the study . 
dynamic contrastenhanced ( dce ) - mri in the axial plane : 3 mm thickness ; 1.0 mm ; imaging acquisition was in - plane resolution : 1.0 continued for 5 min to detect washout . 
mr spectroscopic imaging ( mrsi ) : matrix 8 phase - encoding steps with nominal voxel size < 0.5 cc ; spectral selective suppression of water and lipid signals ; automatic or manual shimming up to a line width at half height of the water resonance peak between 15 and 20 hz . 8 analysis of mr images two genitourinary radiologists , with 13 and 4 years of experience , respectively , blinded to blood test results , evaluated the images in consensus . each mri technique ( t2wi , dwi , dce and mrsi ) was assessed relying on the pi - rads score [ 17 ]  . 
for each patient , the index lesion to which to direct the targeted biopsy , defined as the largest and most aggressive lesion based on mri patterns , was identified [ 18 ]  . 
in addition , the insertion angle can be changed by rotating the needle guide about a point inside the rectu the needle guide can be rotated and moved forwards and backwards from outside the mr unit by means of a telescopic rod . 
it is thus possible to direct the needle guide to the desired prostate region with mri guidance . to reproduce the prebiopsy diagnostic mri findings , after repositioning of the patient or on a different day , coronal , sagittal and axial t2w images ( single - shot ) were performed ; moreover , axial t1w images for detection of haemorrhage with a section thickness of 3 mm were performed before biopsy in patients who underwent a previous trusgb . 
t2wi was adopted in a double - oblique orientation , parallel to the long axis of the needle guide . as a rule , two biopsy cores were obtained in each patient from the suspicious zone . 
in three patients , a suspicious lesion to which to direct the targeted biopsy was detected both in the peripheral and transitional zone , so that four biopsy cores were obtained , two for each lesion . no local anaesthesia was offered prior to the procedure , nor were medications for bowel movement reduction or fig . 
note the anterior and posterior high signal intensity streaks of contrast medium enabling a proper depiction of needle guide measurement and comparison of apparent diffusion coefficient ( adc ) values and choline / creatine - to - citrate ratio ( cc / c ) were helpful for the diagnosis . in patients with two or more suspected foci of pca with different pi - rads scores , the zone assumed to be the index lesion was the one with the highest pi - rads score . 
in patients with two or more suspected foci of pca with the same pi - rads score , the area reported to be the index lesion was the most aggressive one with the lower adc values and the highest cc / c [ 19 ]  . 
3 dynacad software enabling the proper rotation , angulation and movement of the needle guide for interventional planning radiol med ( 2015 ) 120 : 571578 local anaesthetics or sedatives used , since the procedure was very well tolerated . the overall 52 samples were separately placed in formalin solution and labelled for histopathological evaluation . 
patients were instructed to present to the department of urology if they developed complications such as prolonged haematuria , fever , or pain . results at prebiopsy mp - mri , in the 23 patients , a total of 26 suspicious areas to which to direct the mri - guided targeted biopsy were found , 23 of which in the peripheral zone and three in the transitional zone . 
histological examination demonstrated pca in 3 / 7 zones with a pi - rads score of 3 / 5 ( average gleason score 6 ) , two of which were located in the transitional zone ; in 6 / 7 areas with a pi - rads score 4 / 5 ( average gleason score 7 ) ; in all the 12 areas with a pi - rads score of 5 / 5 ( average gleason score 8 )  . 
histological examination in the four areas with a pi - rads score of 3 / 5 negative for pca revealed high - grade prostatic intraepithelial neoplasia in two zones and prostitis in the other two areas ; whereas in the area with a pi - rads score of 4 / 5 negative for pca , it detected a capsular prostatic adenoma . the duration of the procedure ranged from 35 to 55 min ( mean 40 min )  . 
4 a , b coronal t2 - weighted image , c t2 - weighted sagittal image and d axial diffusion - weighted image of a 69 - year - old patient ( psa , 7.98 ng / ml ) with only slight hypertrophy of the central gland and the index lesion located in the left third middle periapical aspect of the gland showing a pi - rads score of 5 / 5 . 
mp - mri examination shows promising results in identifying suspected pca foci suitable for a rebiopsy in patients with persistently elevated psa level and negative trusgb [ 21 , 22 ]  . moreover , because mp - mri is the most accurate imaging modality for the localisation of pca , mrgb offers the possibility of more precise targeting with the possibility to perform fewer core biopsies [ 23 ]  . 
in - bore approaches are exclusively mri - based , using prebiopsy mri to define the targets and real - time mri to guide and control , with image confirmation , all the steps of the procedure . 
out - of - bore approaches use us to guide and control the procedure ; in a fusion us - mri prostate biopsy , previously obtained prostate mr images are fused with the us images at the time of biopsy to guide the operator to the target . open and closed in - bore mri settings could be used . 
 [ 29 ] used a device for transgluteal biopsies in a closed - bore systetransgluteal biopsies minimise the risk of injury to the bladder , bowel , and iliac vessels , and no intestinal germs are introduced into the prostate . 
this technique was used first in a cadaver study , and currently it is not widely available . the advantage of open mr scanners over closed mr scanners is that a physician has direct patient access . 
the detection rates after one negative biopsy round ranged between 38 and 55.5 % [ 1113 ] ; these data are promising and demonstrate the potential clinical value of mrgb . 
 [ 14 ] included 100 patients with at least one negative trusgb , persistently elevated or rising psa and at least one lesion suspicious for pca on diagnostic 1.5 tesla endorectal coil mri . 
in 52 / 100 ( 52.0 % ) patients , pca was detected , showing a high tumour detection rate of over 50 % . the results reported by penzkofer et al . 
 [ 15 ] have shown that to date in - bore mrgb is very reliable and relatively easy , and the targeted approach has high yield with more positive lesions from adcand dce - positive sites . one study reported on 71 consecutive men with at least two negative trusgb who then underwent mp - mri : 70 had an mri - suspicious region and 68 underwent ingantry mrgb . 
the cancer detection rate was 59 % , of which 93 % were clinically significant cancers ; mrgb was compared to a matched reference group who underwent repeat trusgb , and the authors found that mrgb detected significantly more tumours than standard repeat trusgb ( 22 % for second and 15 % for third trusgb ) [ 16 ]  . 
in a separate study by the same research group , 34 men underwent mp - mri , then mrgb of dwi - derived targets , followed by rp ; the biopsy - to - prostatectomy gleason upgrading rate was compared with that of a matched cohort of 64 men who underwent standard trus 10 core biopsy followed by prostatectomy . 
the authors reported that gleason grade on dwi - guided biopsy accurately predicted the gleason grade at rp in 88 % of cases , whereas gleason grade on standard 10 - core biopsy predicted the gleason grade at rp in only 55 % of cases [ 30 ]  . 
a large series reported a detection rate of 41 % in 96 men , but this study has been criticised for only using single parameter t2wi at 11.5 t to identify suspicious regions for biopsy [ 31 ]  . as in - bore biopsies require mr scanners , and thus valuable device time , they are associated with a higher organisational overhead as a result of the magnetic field hazards . 
however , it does offer the only method which can image the target and the biopsy needle within it prior to sampling , and thus the only true image - targeted biopsy . 
 a proposed solution for this dilemma is the out - of - bore approach with fusion or registration of pre - procedural prostate mri data to trusgb which combines the detection capabilities of mri with the comparably easy set - up of trus [ 15 ]  . 
therefore , real - time trus and mri fusionguided biopsy are proposed as methods for using the highcontrast - sensitive mri data to detect the tumour and the real - time character of trus to follow the motions of the prostate during biopsy [ 34 , 35 ]  . the most straightforward approach for trus / mriguided biopsies is cognitive fusion , in which trusgb is performed knowing the localisation of mri - suspicious lesions derived from peri - procedural mri [ 15 ]  . 
despite the fact that cognitive fusion seems to improve biopsy protocols , more sophisticated devices have been developed for mri / trus fusion that use different ways of registering the intraprocedural us coordinates to the mri coordinates [ 15 ]  . 
 [ 37 ] studied a group of 101 patients from three different risk categories derived from imaging aspects ( low , moderate , high ) on a trus / mri systeall patients received 12 - core standard systematic and mri / trus - fused prostate biopsies in the same setting . 
 [ 38 ] in a recent study concluded that trus / mri biopsy is three times as likely to yield cancer diagnoses ( 21 % of performed targeted biopsies versus 7 % of systematic biopsies ) ; on a per - patient basis , many cancers were detected by systematic biopsy alone ( 84 total positive diagnoses , 38 by both methods , 15 by mri / trus alone , 31 by systematic trusgb alone )  . 
thus , the combination of systematic and trus / mri - guided biopsy seems to be the key in the detection of more cancers . in a recent paper , de rooij et al . 
 [ 39 ] determined the cost - effectiveness of mp - mri and mrgb compared with trusgb and found that the mri strategy is cost - effective in diagnosing pca compared with the trusgb strategy , assuming a sensitivity of mrgb 20 % . 
epidemiological data about the incidence and causes of death among the italian population have shown that screening programmes should be aimed first at fighting the following diseases : prostatic carcinoma , lung cancer , colorectal carcinoma , breast cancer , cardiovascular disease , cerebrovascular disease , aortic and peripheral vascular disease . 
gps do not generally give good or adequate instructions concerning voluntary prevention programmes ; gps may not even be aware of this type of prevention which could represent a valuable option together with the existing mass screening programmes . 
 therefore , in the following analysis , we aim to outline the correct diagnostic pathway for the prevention of diseases having the highest incidence in our country and which represent the most frequent causes of death . 
simonetti department of diagnostic imaging and interventional radiology , molecular imaging and radiotherapy , university hospital tor vergata , v.le oxford 81 , 00133 rome , italy e - mail : gu.manenti@gmail.com keywords health education voluntary prevention nhs savings public healthcare introduction the present paper intends to highlight the importance of the voluntary prevention programmes , both for pathologies for which no organised screening programmes exist and for those for which they do exist but may well be obsolete or inefficient . 
a further aim is to underline the importance of the role of general practitioners ( gps ) in distributing vital information about prevention to citizens and in general to stress the importance of being informed . prevention has been one of the bases of the italian healthcare regime ever since the 1978 reform : indeed prevention is considered fundamental in particular regarding diseases with a significant social impact . 
nowadays , voluntary prevention is made more effective thanks to the new sophisticated diagnostic technologies applied worldwide by diagnostic imaging . epidemiological data about the incidence and causes of death among the italian population have shown that screening programmes should be aimed first at fighting the fol lowing diseases : prostatic carcinoma , lung cancer , colorectal carcinoma , breast cancer , cardiovascular disease , cerebrovascular disease , aortic and peripheral vascular disease . 1 3 512 radiol med ( 2015 ) 120 : 511525 today it is either impossible or else extremely complicated to gain access to information about the correct diagnostic pathway for prevention . 
general practitioners ( gps ) do not generally give good or adequate instructions concerning voluntary prevention programmes ; gps may not even be aware of this type of prevention which could represent a valuable option together with the existing mass screening programmes . therefore , in the following analysis , we aimed to outline the correct diagnostic course of action for prevention of those diseases with the highest incidence in our country and that represent the most frequent causes of death . 
if used correctly , these screening programmes may contribute to the success of secondary prevention , limiting the use of tertiary prevention and thus producing savings for the italian national health system ( nhs )  . prostate cancer epidemiological aspects prostate cancer represents the most frequent neoplastic disease among male subjects ( 20 % of all diagnosed tumours )  . 
in italy in 2011 , about 42 , 000 new cases were diagnosed and 7 , 800 deaths were caused by prostate cancer ( that concerns 8 % of the overall deaths for tumours in men between 2005 and 2007 )  . 
 nowadays , despite it ranking first for incidence among the male population , prostate cancer represents the third cause of mortality from tumours ( almost all deaths over the age of 70 )  . accuracy and reliability of prostate cancer screening tests currently , digital rectal examination ( dre ) and prostatespecific antigen ( psa ) testing are applied for the largescale prevention of prostate carcinoma . dre represents the first diagnostic approach for patients presenting prostate - related symptoms . 
 however , dre has intrinsic limitations : it is possible to examine only the posterior and lateral regions of the gland . an overall review concerning prostatic screening has reported that dre allows the detection of less than 60 % of prostate cancers [ 2 ]  . 
therefore , rectal inspection alone does not have sufficient diagnostic accuracy and , consequently , it is fundamental to combine dre with a psa assay . psa is a glycoprotein produced mainly by prostatic tissue and it is the only marker routinely employed in patients with suspected prostatic disease . 
the most commonly used cutoff value is equal to 4 ng / ml . the sensitivity , specificity and positive predictive value of psa in the identification of prostatic carcinoma may vary depending on the cutoff value considered : within a limit of 4 ng / ml , psa has an estimated sensitivity ranging between 63 and 83 % for clinically significant tumours according to histo - pathological criteria , while its specificity is about 90 % and decreases with age [ 2 ]  . 
it is also necessary to take into account the fact that other pathological conditions such as prostatitis can modify blood psa levels . the combination of dre and psa seems to improve the effectiveness of screening : a research study detected an extra 26 % of prostatic carcinomas compared to psa alone but this was associated with an increase in false positives [ 3 ]  . concerning the validity of psa alone as a screening test for prostate cancer , two important trials report conflicting results . 
the american prostate , lung , colorectal and ovary ( plco ) study did not prove the existence of any significant benefits regarding mortality using psa as a screening test while in the european randomized study of screening for prostate cancer ( erspc ) the psa test resulted in a relative mortality reduction of 20 % , during a 9 - year - long observational period , and an absolute reduction of about 7 deaths for prostatic tumour out of 10 , 000 men under screening . 
a systematic review [ 4 ] states that the efficacy and benefits of psa screening are still uncertain and not easily quantifiable . the role of diagnostic imaging in prostatic cancer prevention diagnostic imaging can be useful for improving the diagnostic efficacy of conventional screening procedures : prostatic trans - rectal ultrasound , first of all , is able to increase the diagnostic sensitivity in combination with both psa and dre . 
however , a trans - rectal ultrasound alone is not recommended as an initial screening test ( according to current screening guidelines of the american cancer society and of the center for disease control and prevention ) , owing lack of data supporting a sufficient specificity and capability of achieving a significant increase in the detection rate of prostate cancer . a recent study , based on a wide data set , shows that trans - rectal ultrasound has a predictive positive value of 1 3 radiol med ( 2015 ) 120 : 511525 15.2 % in the detection of tumours versus a value of 28 % for dre ; hence , neither techniques allows one to distinguish most benign diseases that could mimic a prostatic carcinoma from true positive cases . 
moreover , the introduction of proton magnetic resonance spectroscopy ( h - mrs ) has permitted a metabolic evaluation of the prostatic gland : thanks to the possibility of a correlation between citrate and choline values and the malignancy grade of the tumour ( gleason grading ) , a better volumetric definition is also obtained . 
the information obtained helps to understand the natural evolution of the disease and to discriminate aggressive forms from indolent progression of the tumour . the recent literature about the cost - effectiveness of prevention pathways for prostatic cancer focuses on the importance of mri for patients with increased psa or with dubious prostatic areas but negative prostatic biopsies . 
the use of h - mrs , dynamic contrast - enhanced mri ( dcemri ) or diffusion - weighted mri ( dwi - mri ) can actually reduce the number of patients undergoing unnecessary biopsies and / or invasive or even radical interventional procedures in the case of uncertain results . 
the data available demonstrate that h - mrs and dwi - mri have a high sensitivity in detecting tumours in patients with moderate / high risk and that they make it possible to avoid biopsies for those patients without tumour or with associated low risk . 
it has been demonstrated that a 35 - year - old man smoking 25 or more cigarettes per day has a 13 % risk of death from lung cancer before he turns 75 . 
 the risk increases with the number of cigarettes smoked per day / year ; the risk is also related to the age of starting the smoking habit , to the nicotine and tar content and to the absence of a cigarette filter . the proposed screening technique in the past was chest radiography ( cxr )  . 
however , several studies ( north london cancer study 1959 , erfurt county study 1972 , john hopkins lung project 1970 , msklp 1970 , mayo lung project 19711983 ) underlined the inappropriateness of cxr above all in the detection of lesions smaller than 10 mm or located in peripheral areas [ 911 ]  . recently , low - dose computed tomography ( ldct ) has been proposed for the screening of lung cancer . 
the values reported in the literature up to 2006 concerning the sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) of ldct are 81 , 81 , 8 and 99 % , respectively , [ 12 ] depending on the single research taken into consideration . 
from these data it is clear that lcdt should be considered as the first - choice technique in terms of effectiveness for lung cancer prevention . currently available guidelines suggest screening subjects aged between 55 and 74 , smokers or past smokers with a consumption of 30 pack - years for no longer than 15 years , where a pack year is defined as smoking a packet of cigarettes per day for 1 year . lung cancer represents the first cause of death for tumour in industrialised countries , both in males and females [ 7 ]  . 
 in italy , the number of new cases per year is approximately 59 / 100 , 000 inhabitants , with a mortality rate of 32.6 / 100 , 000 in males and 12 / 100 , 000 in females . 
table 1 summarises the results of the main studies on the cost - effectiveness of lung cancer screening . the variety of results depends on the choice of different reference trials , on the diversity of mathematical models used in the studies considered , on the data used to evaluate the cost - effectiveness ratio , and on the different time horizons considered . according to the international association for the study of lung cancer ( ialsc ) , what is needed is to implement further cost - effectiveness studies on a national basis and to conduct new randomised controlled trials ( rct ) that include , among their aims , the economic evaluation of screening , as is being done in england with the united kingdom lung screening trial ( uklst )  . prevention of colorectal carcinoma epidemiological aspects colorectal cancer represents the third most common tumour in males ( 663 , 000 cases , 10 % of all tumours ) , and the second in females ( 570 , 000 cases , 9.4 % of all tumours ) ; moreover , it represents the fourth cause of death from cancer worldwide ( 608 , 000 deaths , 8 % of the total ) [ 22 ]  . 
in italy , colorectal carcinoma is the most frequent tumour among the italian population , accounting for 52 , 000 estimated diagnoses for 2012 . among males it represents the third most common fatal tumour after prostate and lung cancer ( 14 % of all new tumours ) , while among women , with an incidence of 14 % , it is the second most common after breast cancer [ 23 ]  . 
 in recent decades , growing attention has been paid to the reduction of risk factors and to secondary prevention . guidelines for secondary prevention of colorectal carcinoma the most detailed guidelines are related to the early diagnosis and surveillance of colorectal adenomatous lesions and cancers in adults with an average risk that can be assimilated to the risk of general population [ 24 ]  . adenomatous polypoid lesions are considered to be the benign precursor of colorectal carcinoma , with a 10 - year period required for malignant degeneration . 
taking advantage of the long pre - clinical phase , it may be possible to reduce the incidence of deaths in more than 90 % of cases [ 24 ] and prevent cancer through early detection and removal . in particular , the goal of secondary prevention is the recognition of lesions considered at high risk : adenomatous polyps with a diameter of more than 10 mm , or with a villous component greater than 25 % at histological examination , or with a high grade of dysplasia [ 25 ]  . the guidelines suggest making the asymptomatic population over 50 years of age undergo secondary prevention ; the rationale for this is the evidence that , from the fifth 1 3 radiol med ( 2015 ) 120 : 511525 decade , there is a calculated increase in the sporadic risk of cancer . 
moreover , in the case of a family history of colon cancer among firstor second - grade relatives , the patients should undergo screening starting from 10 years before the age of diagnosis of the affected or deceased relative [ 24 ]  . in many italian regions there are organised colorectal screening programmes that are generally based on faecal occult blood testing ( fobt )  . colorectal cancer and screening methods the various screening methods are divided into two categories : nonspecific tests in which a positive result leads to indepth diagnostic investigation and examinations capable of detecting any neoplastic lesions [ 24 ]  . annual fobt belongs to the first category and can be carried out with a guaiac test ( gt ) , monoclonal antibodies ( faecal immunochemical test , fit ) , or faecal dna analysis ( even though this it is not commonly used in clinical practice ) [ 2527 ]  . 
 ( 45 % for gt and 42 % for fit and 27.6 % for gt ) [ 28 ] ; these data provide proof of the high rate of falsepositive results and the consequent need for a diagnostic examination with greater specificity . the current guidelines recommend the use of one of the following techniques : total colonoscopy , flexible proctosigmoidoscopy and ct study [ 24 ]  . currently , traditional endoscopy is considered the technique of reference in all available studies and it is recommended every 10 years . 
however , this diagnostic examination is not so well accepted by patients because of its invasiveness and because of the pain felt during the examination ; moreover , in 626 % of cases it is not possible to explore the entire large intestine for reasons such as dolichocolon , diverticulosis , stenosis , tissue adhesions , etc . 
in fact , as it is not possible to perform a polypectomy for histological evaluation during the ct study , experts have directed their research to the analysis of the risk of cancerous degeneration for lesions of all dimensions . 
currently , the improvements in virtual colonoscopy allow extension of this method to smaller lesions with dimensions between 6 mm and 9 mm ( intermediate lesions ) [ 35 ]  . 
in fact , statistics show an increased risk of neoplastic evolution in these subjects , and in these cases traditional endoscopy is indicated [ 36 ]  . in the meta - analysis published in 2011 by pickhardt et al . 
all these data confirm that virtual ct colonoscopy is a suitable alter native to conventional colonoscopy for the secondary prevention of colorectal carcinoma . cost - effectiveness of colorectal cancer prevention a cost - effectiveness analysis applied to conventional colonoscopy and ct colonoscopy as a screening method for the general population is difficult to develop because of the huge patient sample that could have to be involved and followed up . 
therefore , the cost - effectiveness analysis is exclusively based on mathematical statistical models . participation in screening programmes involving the use of optical endoscopy is low because of the invasiveness of the method , while better participation rates , even if still not satisfactory , are obtained with ct colonoscopy ( lower risk of perforation , greater tolerance by patients in poor clinical condition , lack of anaesthesia - related risks )  . table 2 shows the results of several studies comparing the different techniques available for colorectal cancer screening . 
these studies show highly variable cost - effectiveness ratios [ 4246 ]  . in conclusion , despite the heterogeneity of the data reported in the literature , the efficacy of the above 1 3 516 radiol med ( 2015 ) 120 : 511525 1 3fl radiol med ( 2015 ) 120 : 511525 methods is widely recognised in the international scientific literature . 
therefore , an ideal voluntary prevention scheme should include the association of a nonspecific method on an annual or biannual basis with a more specific technique according to the previously reported time schedule . preventing breast carcinoma epidemiological aspects breast cancer is the most common cancer among the female population : at least one in thirteen women has the potential risk of developing breast cancer in her lifetime [ 47 ]  . 
in europe , 300 , 000 new cases per year have been estimated , and the estimated italian annual incidence of breast carcinoma has reached more than 47 , 000 new cases per year [ 23 ]  . 
nowadays breast disease represents the main cause of death in the female population aged between 35 and 55 , although its incidence has a peak among women aged 5055 [ 48 ]  . 
in recent decades , we have witnessed a significant decrease in mortality , not only because screening programmes have been implemented worldwide , but also because women have now learned to undergo regular diagnostic investigations . organised screening programmes , diagnostic techniques and open prevention the italian national health system ( nhs ) offers several breast cancer screening programmes that may differ from region to region , as happens in most european and noneuropean countries . 
moreover , women have shown different levels of compliance . our country has adopted widespread screening mammography system which consists of an invitation from the nhs to the target population : women aged between 50 and 69 . 
however , most of the organised screening programmes currently in place in italy have displayed some important limitations : the target population is represented by only a restricted group of women ( 5069 age group ) and the 24 - month interval appears to be too long for the early detection of breast cancer . 
digital mammography ( mx ) : this is performed using three views ( craniocaudal , oblique and mediolateral ) , and it may be completed with further projections , targeted compression and / or magnification . 
mammography shows an average sensitivity up to 7580 % , which is lower in the case of dense breasts reaching 3048 % in extremely dense breasts [ 51 ]  . 
using cad , the rate of false negatives , which is expected to be around 21 % , could be reduced by about 77 % , without increasing the call - back rate [ 52 ]  . 
breast ultrasound ( us ) : using dedicated ultrasound linear probes ( 1012 mhz ) , radiologists can achieve a valid evaluation of lesions , determining if they are solid or liquid ; colour doppler evaluates the vascular features of the lesions , leading to a complete diagnostic hypothesis [ 53 , 54 ]  . 
ultrasound examination showed an average sensitivity of just over 90 % , and the literature reports that us increases the sensitivity of mammography on its own for the detection of cancer by 1020 % . 
however , its specificity varies considerably : from 70 to 89 % , according to the recent literature [ 55 ]  . 1 3 518 radiol med ( 2015 ) 120 : 511525 table 3 breast cancer : effectiveness of different diagnostic technologies in the prevention programme recommended prevention programmes technology sensitivity ( % ) specificity ( % ) digital mammography breast ultrasound breast mri 3080 89100 7089 4 . 
 postprocessing evaluation gives an accurate analysis of wash - in and wash - out rates of gadolinium inside the lesions , an index of neovascularisation [ 56 , 57 ]  . 
mri has a sensitivity that can vary from 89 to 100 % , according to published studies [ 56 ] , but its specificity is quite low ( 62 % ) , and this can result in a significant number of false - positive cases . the effectiveness of each technique applied in prevention programmes for breast cancer has been compared in a series of published studies . 
the cost - effectiveness ratio for mammography , ultrasound and breast mri has also been evaluated ( table 4 ) and depending on the study , different measures of benefits have been used : qalys ( quality - adjusted life years ) , years of life saved and number of diagnosed tumours . an up - to - date screening programme should involve the most advanced diagnostic technologies currently available , adapting their use to the risk and needs of the patients ( personal clinical history and / or family history , breast density , other clinical factors )  . the goal should be to improve the early detection and diagnosis by appropriate use of the diagnostic tools and economic resources available . 
mammography , ultrasound and mri : dense breast and positive family history and / or genetic risk . open screening for cardiovascular disease heart disease epidemiological aspects the rate of mortality for cardiovascular disease has been estimated at around half of the total population mortality in europe . 
these results may be due to the cooperation between cardiovascular specialists and gps and to the effectiveness of continuous patient assistance outside the hospital . current prevention programmes on the basis of the available technologies , the screening pathways may vary depending on the individual cardiovascular risk . nowadays , the multivariable models of risk stratification most commonly used worldwide are the framingham heart study risk score ( frs ) [ 66 ] and the score ( systematic coronary risk evaluation ) [ 67 ] ; in italy , we have the cuore project risk score [ 68 ]  . 
the identified scores are used to estimate the risk of coronary disease for those subjects with no history of previous coronary events . however , current risk stratification methods still need to be improved and several studies in the literature show how the quantification of coronary calcium using multi - detector ct ( calcium score ) may improve the accuracy of the risk scales for asymptomatic patients [ 69 , 70 ]  . coronary angiography has always been considered the gold standard in the evaluation of the coronary arteries but nowadays coronary ct represents a valid alternative examination for cardiovascular screening with its high diagnostic accuracy showing extremely high sensitivity and specificity , equal to 9599 % and 9597 % , respectively , and an npp of 99100 % [ 7173 ]  . with regard to voluntary screening for asymptomatic patients , coronary ct ( c - ct ) is an important tool for subjects with high cardiovascular risk , especially if non - invasive approaches such as resting and exercise electrocardiogram , are doubtful or unfeasible [ 74 ]  . 
currently , however , the use of c - ct is not yet standardised for the screening of asymptomatic subjects with low and intermediate risk . costeffectiveness of prevention programmes for cardiovascular disease the literature has reported that the economic impact and cost - effectiveness of c - ct is better than that of angiography [ 75 ]  . 
have demonstrated that c - ct is the diagnostic tool with the best cost - effectiveness ratio in the evaluation of patients with a risk of coronary artery disease below 87 % before the examination . this finding leads to the assumption that multi - detector ct could be used for mass screening and it certainly represents a valid tool for voluntary screening , since cardiovascular disease has a major economic and social impact in terms of deaths and public spending ( cardiovascular disease costs 169 billion a year for the eu , with a total annual expense per capita of 372 )  . 
in particular , the focus of the international literature is on the quantification of coronary artery calcium with ct in the assessment of cardiovascular risk [ 76 ]  . potential future scenarios two different scenarios can be envisaged on the basis of the epidemiology of coronary heart disease , its high costs and the negative predictive value of coronary ct : mass screening : coronary ct for all patients over 60 ( men and women ) and with high and / or intermediate risk of coronary heart disease . individual screening : coronary ct for all asymptomatic patients ( men aged 4550 years and women 5 years after the menopause ) with at least one risk factor diagnosed in an initial examination , to obtain a personal id ( similar to that already existing in breast diagnostic imaging ) ; follow - up after 5 years if the risk factors remain stable , without any elapsing symptom . cerebrovascular disease epidemiological aspects in italy , approximately 200 , 000 strokes occur every year . 
data from the literature report that stroke is the second leading cause of death worldwide and the third leading cause of death in the g8 countries , where it is second only to cardiovascular disease and cancer . 
the rate of prevalence of stroke among the italian elderly population ( age 6584 ) is 6.5 % , with a slightly higher rate in men ( 7.4 % ) than women ( 5.9 % ) [ 77 ]  . prevention in stenotic disease of the epiaortic vessels and new technologies secondary prevention of ischaemic stroke , followed by tertiary prevention with endovascular treatment or endarterectomy , has been proved to be useful for symptomatic patients with carotid stenosis greater than 50 % and asymptomatic patients with stenosis greater than 80 % [ 78 ] , as well as for patients with vulnerable plaques assessed on baseline ct / mri . 
moreover , 1 3 520 radiol med ( 2015 ) 120 : 511525 table 5 carotid atherosclerosis : effectiveness of diagnostic technologies intracranial aneurysms colour doppler ultrasound sensitivity specificity epidemiology aspects aneurysmal vascular disease has a global prevalence of 23 % in the general population . 
however , some subgroups may be more frequently affected , and in particular families with a prevalence of 410 % when only one family member is affected or 20 % if two members are affected . 
moreover , 2034 % of affected patients have at least one other aneurysthe chance of rupture of an aneurysm is about 5 % within 5 years [ 82 ]  . prevention of intracranial aneurysms : diagnostic imaging and diagnostic efficacy ct angiography and mr angiography are the most commonly used diagnostic techniques for preventing intracranial aneurysmal vascular disease ( table 6 )  . the type of technique and the clinical indication for the examination can both affect the variability of findings . 
although colour doppler table 6 identification of intracranial aneurysms : effectiveness of diagnostic technologies stenosis plaque morphology 8589 % 8286 % colour doppler ultrasound stenosis ct angiography stenosis plaque morphology rm angiography stenosis plaque morphology rm angiography 8693 % sensitivity 7478 % 97100 % sensitivity 8894 % 9396 % 99 % 8486 % 8185 % 7697 % specificity 9396 % 96100 % specificity 8493 % 9498 % 98.1 % in the last decades several studies have demonstrated that plaque morphology is as crucial as the level of vessel stenosis for proper treatment planning [ 79 , 80 ]  . colour doppler ultrasound is accepted worldwide as the screening method for diagnosing carotid atherosclerosis . 
colour doppler ultrasound has also shown high sensitivity and specificity in the evaluation of plaque mor phology and in the assessment of average intima - media thickness ( imt )  . 
data from the literature report wide variability in terms of sensitivity , specificity , npv and ppv of doppler ultrasound , because it is strictly dependent on the operator and also because the degree of the stenosis affects the examination : 80 % stenoses are estimated up to 100 % ( table 5 )  . alternatively , ct allows a rapid evaluation of the epiaortic vessels with high - resolution images [ 81 ]  . 
moreover , dedicated coils and paramagnetic contrast agent accurately depict the fibrous cap and its disruptions , as well as allowing for a diagnosis of plaque inflammation , which is fundamental in defining a vulnerable plaque [ 79 ]  . ct angiography mr angiography sensitivity 67100 % 7097 % specificity 50100 % 89100 % 100 % 80100 % 87.5 % 59100 % 1 3 radiol med ( 2015 ) 120 : 511525 ultrasound is widely used , the use of ct and mr angiography is still not common since only expert radiologists are able to obtain important information from these diagnostic imaging tools for interventional planning . voluntary screening should be carried out by undergoing periodic doppler ultrasound combined with mr angiography ; ct angiography can be subsequently used for those cases exhibiting altered plaques regardless of the degree of stenosis . in the evaluation of intracranial disease , risk groups have been identified and nowadays screening is only useful for the identified risk groups . 
however , we know that incorporating the study of intracranial vessels in the evaluation of the carotid , despite the longer examination time and higher cost , can guarantee an early diagnosis of aneurysms in the pre - clinical phase . 
this explains why it is necessary that ct and mr of the carotid vessels include intracranic circulation . aorto - iliac atherosclerosis and peripheral artery disease epidemiological aspects the increase in longevity in western countries has resulted in a significantly increased prevalence of aortic and peripheral artery vascular disease ( peripheral arterial occlusive disease , paod ) , showing a higher incidence rate among adult subjects ( 12 % of the global population )  . care management may depend on the patients clinical symptoms : patients with intermittent claudication especially those with reduced quality of life require specific care , such as conservative surgical treatment or interventional radiology procedures , whereas patients with limb ischaemia require angioplasty , surgical revascularisation or in some cases limb amputation [ 83 ]  . 
in the case of aneurysmal aortic disease , the indication for either diagnostic follow - up or treatment relies on the size of the aneurysm compared to the baseline dimensions of the affected vessel . 
since a variety of pharmacological opportunities and new endovascular techniques have been developed , it is mandatory to use the most accurate method in the diagnosis of vascular disease . prevention solutions and effectiveness of diagnostic technologies digital subtraction angiography ( dsa ) is still considered the gold - standard technique for the diagnosis of aorto - iliac and peripheral steno - occlusive disease . 
this technique is , however , burdened by high costs , high invasiveness and several possible complications for the patient , with a rate of about 1 % during diagnostic angiography alone [ 84 , 85 ]  . 
 this explains why dsa has been used for treatment purposes only in peripheral and aorto - iliac disease . several less invasive diagnostic procedures have now become available such as doppler ultrasound , mr angiography and ct angiography . colour doppler ultrasound is the gold - standard technique in the assessment of peripheral artery disease , because of the wide availability of the equipment and because of its lack of invasiveness . 
however , it is non - reproducible and highly operator - dependent , it cannot evaluate calcific plaque components , and its images are limited to a restricted anatomical area . 
recent studies , with large samples of patients affected by atherosclerotic disease , nondiabetics with small extension of disease , evidenced a mean sensitivity of 90 % ( 7494 % ) , and an average specificity of 99 % ( 96100 % ) [ 84 ]  . 
these findings indicate a need for a level - two diagnostic approach for this pathology . mr angiography is usually considered the level - two examination : it represents a reliable tool with the use of a contrast agent . 
mra is not burdened by significant limitations related to a restricted view of vascular tract being explored [ 87 ] , as shown in the results reported in table 8 . 
mra of the aortic and peripheral district requires table 7 effectiveness of doppler ultrasound vessels above knee [ 85 ] below knee [ 85 ] below knee [ 86 ] aorto - iliac [ 86 ] femoro - popliteal district [ 86 ] sensitivity ( % ) specificity ( % ) diagnostic accuracy ( % ) ppv ( % ) npv ( % ) 1 3 522 radiol med ( 2015 ) 120 : 511525 table 8 effectiveness of mra in specific vascular tracts tract average sensitivity ( % ) average specificity aorto - iliac 94 ( range 9196 ) femoro - popliteal 95 ( range 9198 ) below the knee 92 ( range 9094 ) 96 ( range 9198 ) 96 ( range 9598 ) 93 ( range 9096 ) limbs . 
when patients show no problem on the initial doppler examination , they are referred for follow - up at 12 or 24 months , depending on their individual risk factors . 
 all patients without particular risk factors could repeat the examination after an interval of 24 months . table 9 effectiveness of volumetric ct angiography in different vascular tracts tracts average sensitivity ( % ) average specificity ( % ) aorto - iliac 96 ( range 9199 ) femoropopliteal 97 ( range 9599 ) 98 ( range 9599 ) 94 ( range 8599 ) below the knee 95 ( range 8599 ) 91 ( range 8797 ) acceptable examination times , thanks to the new available dedicated coils . 
image reading , however , may be longer for radiologists compared to the evaluation of a single vascular district . multi - detector volumetric ct angiography is also used as a level - two technique for the assessment of the peripheral arterial systethe major advantage of ct compared to mr is the better imaging of plaque morphology and vessel walls : this allows for a more accurate evaluation of the stenosis . 
the recent literature has shown values of sensitivity of 99 % , specificity 98 % , accuracy of 98 % , ppv of 96 % , and pnv of 99 % [ 88 ]  . 
furthermore , the evaluation of different vascular vessels has demonstrated the absence of statistically significant different values [ 89 ] ( table 9 )  . recommended screening strategy a screening programme for aortic and peripheral vascular disease has not yet been defined , although the diagnostic pathway for patients with vascular disease appears well organised . 
mass screening could be done with periodical follow - up in men and women ( age > 50 ) using colour doppler ultrasound of the abdominal aorta and lower limbs as level - one imaging . 
doppler ultrasound can be followed by mr angiography and volumetric ct angiography if the abdominal aorta calibre exceeds 3 cm , if blood flow is altered or if atherosclerotic plaques affect the lower conclusions and discussion the present analysis has outlined the different possibilities of voluntary screening that should accompany the existing mass screening programmes . 
the screening programmes described above concern diseases with the greatest impact in terms of incidence and mortality : prostate cancer , lung cancer , colorectal cancer , breast cancer , cardiovascular disease , cerebrovascular disease , aortic and peripheral vascular disease . 
the aims of the study were to highlight : the essential role of diagnostic imaging in screening programmes ( mass screening and voluntary screening ) ; the fundamental importance of information for the well - being of a population ; the social and economic relevance of prevention at a community level . 
as can be seen from our analysis , the role of diagnostic imaging in secondary prevention is pivotal : ultrasound and mri for prostatic cancer ; ct for lung cancer ; ct for colorectal cancer ; mammography , ultrasound and mri for breast cancer ; ct for heart disease ; colour doppler ultrasound , ct and mri in cerebrovascular disease ; digital subtraction angiography , doppler ultrasound , ct and mri in peripheral arterial disease . 
moreover , preventing often proves to be better and less expensive than curing so it is vital to inform patients about the importance of good , organised prevention programmes . as for secondary prevention , it is first highly important to identify established courses of action , as this would no doubt be more practical and less time consuming for the patients and less costly for the state . 
second , it is important to provide patients with accurate information , as this means that patients will approach secondary prevention in the correct manner and the state will not have to bear the costs of numerous irrational and sometimes unnecessary diagnostic examinations . areas in northern italy are promoting several public initiatives such as health squares and open conferences such as prevention as a way of life , in an attempt to heighten the publics awareness about the prevention of serious diseases in terms of incidence and mortality . additionally , there is a need for increased involvement of general practitioners in directing patients towards the right course of action for secondary prevention . 
pattacini department of diagnostic imaging , arcispedale santa maria nuova hospital irccs , reggio emilia , italy efficient and effective rapid mechanisms of actionreaction inside and outside the radiology department . conclusions the ris - integrated module has been the starting point for managing and monitoring errors , allowing improvement initiatives to guarantee and optimise workflow . 
 the integrated tool described in this paper is now widely used ( not only by our centre ) : radiographers and radiologists can indicate non - compliances in an efficient and effective manner , informing all the operators involved with just a click of the mouse . 
1706 / 2009 of november 09 2009 titled security of ris - pacs systems guidelines for the development of practices and strategies in public and accredited health facilities in the emiliaromagna region [ 8 ] provides more than 20 operating instructions aimed at preventing errors and defines actions to be taken should an error occur . 
in radiology , the radiographer is responsible for the technical aspects of the transmission of images , verification of personal data , and sa role [ 10 ]  . materials and methods context in the reggio emilia province , there are two public healthcare entities : the hospital - irccs s . 
ausl has five leveli hospitals located in the province of reggio emilia , all within a radius of 35 km , with a total of about 800 beds . the radiology units of both entities belong to the provincial department of diagnostic imaging and laboratory medicine . 
the department performs over 410 , 000 diagnostic imaging examinations every year ( about 190 , 000 and 220 , 000 exams in asmn - irccs and ausl , respectively )  . 
the breakdown of asmn - irccs examinations is as follows : 38 % outpatient , 28 % emergency room ( er ) , 24 % inpatient and 10 % related to screening access . 
 ausl examination distribution is 61 , 21 , 9 and 9 % , respectively . the department uses a single ris - pacs system ( ris polaris elco s.r.l. , cairo montenotte , sv , italy , and carestream pacs version 11.3 , rochester , ny , usa ) , and all studies have been online since 2003 for asmn - irccs and since 2006 for ausl . 
operators who discover a patient misidentification or examination to be reconciled can fill in a reconciliation request form directly on their ris worklist by selecting the examination to be reconciled and opening the reconciliation request webpage ( right - side click on the mouse )  . 
to fill in a request , or manage status , the system prompts operators to enter their credentials ( username and password ) in order to guarantee security and the traceability of any changes . after indicating the examination requiring reconciliation , the operator opens the request page containing the wrong identification data ( coming from the selected study ) ; they choose the type of reconciliation requested ( table 1 ) and fill in the web form with the necessary correct table 1 non - conformity types patient personal data variation wrong image projection / laterality report update / addendum images / study assigned to another patient or episode images / study assigned to another episode for the same patient patient merge data . 
this protocol , commonly recognised as the most widely used in the world , which supports clinical practice and management , delivery and evaluation of health services , has been used to integrate ris reconciliation request information to the pacs ( in real time the operator who consults images on the pacs is alerted to possible errors in clinical data matching / acquisition )  . request management for editing data on the ris - pacs system includes the following steps : the ris form is filled in with information about the study to be reconciledwhich is the responsibility of the user ( technologist or radiologist )  . 
on the ris system , a red wrench icon appears on the study to be reconciled . once the reconciliation request has be confirmed by the operators username and password , ris via hl7 messaging , updates on the pacs some fields of the study to be reconciled . 
3 percentage distribution of reported non - compliance typesazienda ausl from 2009 to 2013 radiol med ( 2015 ) 120 : 498503 been instructed to contact the radiology unit if this label appears on study images . 
on the radiologist reporting worklist , an immediate sign ( red icon ) requiring special attention to the study to be reconciled appears . the sa technologist makes the necessary correction according to instructions contained in the request . 
these types of non - compliance are certainly related to high clinical risk , which requires implementation of efficient and effectively rapid mechanisms of actionreaction , also given the possibility that wrong data may be accessed outside the radiology departments . adverse events in the care process are unexpected occurrences that can result in injury to patients , even if unintended and undesirable . 
reporting these events , defined as incident reporting , focuses on monitoring errors and near or sentinel events , and plays a key role in understanding their causes and triggers and represents the basis for the learning from error principle . 
the ris - integrated module has been the starting point for the management and monitoring of errors , allowing , for example , improvement initiatives to be undertaken by staff members . 
 to protect the accessibility and consistency of information , for example , the iconography and reports produced 1 3 radiol med ( 2015 ) 120 : 498503 by a radiology unit , it is necessary to provide integrated and effective mechanisms to manage reconciliations . 
the integrated tool described in this paper is now widely used ( not only in our centres ) : radiographers and radiologists can indicate non - compliances in an efficient and effective way , informing all involved operators just with a click of the mouse . 
hamidi department of pathology , medical school , dicle university , diyarbakr , turkey malignant thyroid nodules and may positively contribute to clinical evaluation of these nodules . keywords arfi imaging vtq thyroid nodule malignant introduction thyroid nodules are common lesions which are easily detectible on ultrasound . 
although thyroid nodules are easily detectible on ultrasound , this technique does not provide sufficient data for differentiating between benign and malignant thyroid nodules [ 3 , 4 ]  . 
virtual touch quantification ( vtq ) is an application of arfi 1 3 580 radiol med ( 2015 ) 120 : 579583 imaging that provides quantitative measurement of tissue stiffness . 
during vtq , short duration ( 0.030.04 ms ) acoustic pulses generate small ( 110 mm ) localised tissue displacements in the region of interest ( roi ) with a transducer . 
the shear wave velocity ( swv ) is the numerical value ( m / s ) which provides differentiation between hard and soft tissue . we aimed to evaluate thyroid nodules using vtq of arfi imaging and to determine a cutoff value for the differentiation of malignant thyroid nodules . materials and methods patient population a total of 101 consecutive patients admitted between february 2013 and february 2014 were enrolled in the study . 
 all patients had one or more thyroid nodules on ultrasound and had normal serum thyroid stimulating hormone ( tsh ) levels , as well as no previous history of treatment . 
the remaining patients ( 95 patients ; 21 men and 74 women ; age range , 1278 years ; mean age , 44 years 14.9 ) with quantitatively assessed ( vtq ) thyroid nodules were evaluated with arfi imaging in this prospective study . 
other exclusion criteria were as follows : patients with a nodule less than 0.5 cm in diameter , a pure cystic nodule , thyroiditis , or a nodule close to the carotid artery and involving the isthmus . 
this study was approved by the local ethics committee , and all subjects provided informed consent . technique arfi imaging with vtq was conducted using an acuson s2000 ultrasound system ( siemens , california , us ) with a linear probe ( 49 mhz ) while the patients were in the supine position . 
 the following characteristics of the nodule were evaluated via conventional ultrasound ( us ) : morphological characteristics , size , margin regularity , echo pattern , presence or absence of the halo sign , presence or absence of microcalcifications , and vascularity . 
five consecutive measurements were recorded for each nodule from the region identified with the roi , and the mean of these measurements was recorded as the swv value of the nodule . in vtq , the shear wave speed is expressed in m / s . 
several possible explanations for this phenomenon include : operator or patient movements , erroneous roi positioning , and measurements of fluid components or tissue beyond the vtq measuring range ( between 0 and 9 m / s )  . 
receiver operating characteristic ( roc ) curve analysis was used to determine a cutoff value for the differentiation of malignant nodules and to calculate sensitivity and specificity levels . results of the 95 thyroid nodules , 62 were benign ( 54 nodular goitre and eight follicular adenoma ) and 33 were malignant ( 19 papillary carcinoma and 14 follicular carcinoma ) on pathological diagnosis . 
based on morphological characteristics , margin regularity , echo pattern , presence or absence of the halo sign , and presence or absence of microcalcifications on us , 58 of the 95 nodules were suspected to be benign , and 37 were suspected to be malignant ( table 1 )  . 
ten malignant nodules table 1 evaluation of thyroid nodules using ultrasound suspected malignant ( n ) suspected benign ( n ) total ( n ) actual malignant ( n ) actual benign ( n ) 1 3 radiol med ( 2015 ) 120 : 579583 table 2 shear wave velocity ( swv ) values of the 10 malignant nodules which were suspected to be benign based on the ultrasound findings nodule no . mean swv value ( m / s ) were falsely evaluated as benign with us . 
additionally , arfi - vtq had high sensitivity and specificity in differentiating benign and malignant thyroid nodules . a number of studies have been previously conducted to determine the ability of arfi - vtq to distinguish benign nodules from malignant thyroid nodules . 
4 the area under the receiver operating characteristic ( roc ) curve for the diagnosis of malignant thyroid nodules using arfivtq imaging was 0.964 ( 95 % ci : 0.9300.997 , p < 0.001 ) 1 3 radiol med ( 2015 ) 120 : 579583 previous studies of arfi - vtq measurement of thyroid nodules identified increased stiffness in malignant nodules compared to benign nodules . 
indications for evar were the following : aaa 60 and diameter 5 cm , neck length 7 mm , angulation < 30 mm ; the presence of neck calcification and thrombosis was not considered a contraindication ; distal iliac landing a . 
carrafiello ( * ) interventional radiology , department of radiology , insubria university , viale borri , 57 , 21100 varese , italy e - mail : gcarraf@gmail.com zone length of 10 mm , and diameter between 5 and 20 m patients were treated under a common protocol , including clinical and imaging follow - up at discharge , 30 days , 6 months , and annually for 5 years . 
adverse events , clinical and imaging data and possible re - intervention were recorded . results the ovation stent graft was implanted successfully in 36 patients ( 100 % )  . 
piffaretti vascular surgery department , university of insubria , varese , italy endovascular aortic aneurysm repair ( evar ) for suitable abdominal aortic aneurysms ( aaas ) has gained wide acceptance in the past decade . 
in spite of its increasing popularity , technical aspects of graft placement , related to anatomical considerations ( arterial diameter , neck length , or angulations ) , often preclude successful endovascular repair in many patients [ 1 ]  . 
evar of aaas not fulfill ing the anatomical criteria for the neck is associated with an increased incidence of type i endoleak , migration of 1 3 radiol med ( 2015 ) 120 : 542548 the endograft and aortic neck dilatation [ 2 , 3 ]  . 
furthermore , anatomically smaller iliac arteries ( such as in short females ) where iliac diameter may be less than 1 cm or in patients with concomitant iliac occlusive disease causing iliac artery stenosis with a residual lumen between 5 and 8 mm are usually excluded for evar with conventional devices [ 3 ]  . 
the ovation abdominal stent graft system ( trivascular inc , santa rosa , calif ) is a new device that is designed to overcome the limitations of currently available stent grafts and can accommodate a broad range of aortoiliac characteristics , navigate through complex iliac and femoral access , and provide a seal in complex proximal infrarenal aortic neck morphology . 
the main body is a modular two - docking limb device with a 14f outer diameter delivery system , active suprarenal fixation , and polymer - filled proximal rings that accommodate the aortic neck for seal . the aim of this study was to evaluate the 2 - year safety and effectiveness outcomes of the ovation abdominal stent graft system ( trivascular inc , santa rosa , ca , usa ) for endovascular repair of abdominal aortic aneurysms ( aaas )  . materials and methods patients all patients gave informed consent according to the practice in two institutes . 
this retrospective study was conducted in two centres from november 2009 to may 2011 , and involved 36 patients ( 33 men and 3 women ; median age 73.6 ; range 5685 years ) with aaas ( mean diameter , 5.65 cm ) treated with the trivascular ovation device ( table 1 )  . 
patients were monitored throughout their hospitalisation and at regular follow - up visits with contrastenhanced computed tomography ( ct ) performed at 1 and 12 months after the endovascular procedure . 
mid - term follow - up was performed at 6 months with contrast - enhanced ultrasound ( ceus ) and , in the event of endoleak detection , a contrast - enhanced ct examination . 
after the first year , the protocol involved annual ct scans . baseline imaging and treatment procedure all patients underwent preoperative evaluation of their aneurysm with conventional contrast - enhanced ct imaging with thin ( 1 mm ) slice thickness and with intravenous administration of iodinated contrast media . 
optimal arterial enhancement on contrast - enhanced ct scan was achieved using the bolus - tracking technique , with a region of interest ( roi ) placed on the abdominal aorta ( at the supra - renal level ) and considering a threshold 100 hu higher than baseline density . 
patients were eligible for the procedure if they were considered to have a low - to - moderate risk for elective open repair of a non - ruptured aaa or aortoiliac aneurysm according to the society for vascular surgery ( svs ) / international society for cardiovascular surgery ( iscvs ) scores of 0 , 1 , or 2 [ 3 , 4 ]  . 
the exclusion criteria were : ( 1 ) subjects with high probability of non - adherence to physicians follow - up requirements , or ( 2 ) with current participation in a concurrent randomised control trial or investigational device / drug study which could confound the study results ; ( 3 ) life expectancy less than 1 year ; ( 4 ) pregnancy ; ( 5 ) patients with poor renal function as indicated by a serum creatinine > 2.5 mg / dl ; ( 6 ) patients with a condition likely to infect the graft and patients with known sensitivities or allergies to the device materials [ including polytetrafluoroethylene ( ptfe ) , polyethylene glycol ( peg ) - based polymers , fluorinated ethylene propylene ( fep ) or nitinol ]  . 10 mm or device description the trivascular ovation stent graft is a low - profile endovascular device designed to overcome the limitations of previous stent grafts by accommodating a broader range of aortoiliac anatomy with a 14f outer diameter ( od ) delivery system and a proximal aortic neck seal mechanism designed to conform to and accommodate the aortic neck . 
 the ovation stent graft is characterised by a trimodular design ( comprised an aortic body section and two iliac limbs ) ; the aortic body consists of a flexible hydrophiliccoated 14f od catheter , the smallest profile of any cur rently commercially available stent grathe aortic body consists of a low - permeability ptfe graft and a suprarenal nitinol stent with integral anchors to achieve active fixation to the aortic wall . 
the aortic body contains a network of inflatable channels and sealing rings that are filled during deployment with a low - viscosity , radiopaque fill polymer [ peg - based fill polymer , contrast agent ( visipaque 320 , 1 3 544 radiol med ( 2015 ) 120 : 542548 1 3 radiol med ( 2015 ) 120 : 542548 ge healthcare , usa ) , and a buffer ] that cures in situ to create a conformable seal to the patients aortic neck . 
mid - term follow - up was performed at 6 months with contrast - enhanced ultrasound ( ceus ) and , if an endoleak was detected , then a contrast ct scan was also performed . 
the main safety outcomes measured were mortality and serious adverse events ( aneurysm enlargement rupture , conversion to surgery , and secondary interventions ) , in accordance with the classification system of the society of interventional radiology [ 5 ]  . results evar was feasible in all selected patients . 
the main body of the stent graft uses two polymer - filled rings to provide seal against the wall of the aorta , while the metal stent provides fixation of the stent graft to the aorta ( a ) ; schematic image of the stent graft implanted in an abdominal aortic aneurysm ( b ) fig . 
2 computed tomography ( ct ) scan performed after 24 months reveals reduction of the sac diameter ( g ) ; volume rendering ( vr ) reconstruction of the same examination ( b ) required conversion to open surgery , and no aneurysm rupture , fracture , or migration of the endograft were observed . 
in three patients , a type ii endoleak was detected at ct scan after 12 months ( n 1 ) , respectively , but disappeared at ct scan performed after 24 months . 
no major or minor complications , serious adverse events or deaths were recorded during or after the procedure , 30 days after graft deployment or during the follow - up period . 
the rate of minor complication was 8.3 % ( 3 / 36 ) : in detail , two patients developed a transient renal failure ( serum creatinine value > 2 mg / dl ) and one patient required an arterial patch at the access site . discussion since the introduction of evar in 1991 , endovascular treatment with newer stent grafts has assumed a prominent role in the clinical management of aaa with reduced perioperative mortality and an equivalent mid - term 1 3 radiol med ( 2015 ) 120 : 542548 fig . 
3 volume rendering reconstruction of a ct scan performed during follow - up in a patient with ovation stent graft ( a ) ; ct scan performed after 1 year revealed type 2 endoleak ( b ) ; type 2 endoleak and the diameter of the sac remained stable ( c ) outcome , compared to open surgery [ 6 ]  . 
the angulation of the aneurysm neck , defined as the angle between the suprarenal aorta and the first portion of the aneurysm neck ( within the first 3 cm ) , must be considered [ 7 ]  . 
even with an initially good result , the risk of migration , stent fracture , or separation of the prosthesis components in the case of angulation > 60 is significantly increased [ 2 , 8 ]  . 
the prerequisites for successful endovascular treatment are complication - free passage of the stent graft through the iliac access vessels and anchoring in an adequate distal landing zone [ 7 , 9 , 10 ]  . 
in the case of arterial occlusive disease , the vascular segment may need to be treated pre - interventionally via stent angioplasty [ 9 ]  . on the basis of the characteristics described , a great deal of attention and research has focused on endovascular aortic repair devices to accommodate patients with hostile necks as well as concomitant iliac stenosis which may exclude larger profile devices . the ovation stent graft is characterised by a trimodular design : the aortic body is composed of a low - permeability ptfe graft with a suprarenalnitinol stent with anchors that provide active fixation . 
unlike the previous stent grafts , the ovation aortic body contains a network of inflatable sealing rings and channels that are filled with a low - viscosity radiopaque polymer during stent graft deployment . 
 [ 12 ] observed that even in patients with challenging anatomy , the ovation stent graft yielded excellent results , including 100% technical success , 97% freedom from major adverse events through 1 year , and 3.2 % freedom from major adverse events with aaa - related secondary procedures . 
the ovation stent graft has the ability to treat a wider range of patients compared with other stent grafts , especially those with narrow access vessels and short proximal necks , without sacrificing patient safety or device effectiveness . 
in 1 year of follow - up , type ii endoleaks were identified in 34 % of patients ; this endoleak rate , although higher than anticipated , is within the typically reported range [ 13 ]  . 
 [ 12 ] concluded , even in our series , the long - term trajectory of these endoleaks will be monitored and remains to be determined as patients undergo regular surveillance annually for 5 years under the study protocol . the study presented is the first with a series of patients with at least 2 years of follow - up available . 
it was a non - controlled study and , therefore , comparative performance of the ovation stent graft with alternative aaa treatments could not be directly evaluated . 1 3 548 radiol med ( 2015 ) 120 : 542548 as in the patient group reported by mehta et al . 
two radiologists in consensus assessed liver apparent diffusion coefficient ( adc ) and fraction of anisotropy ( fa ) values on adc and fa maps at four reference levels , namely : right upper level ( rul ) , right lower level ( rll ) , left upper level ( lul ) and left lower level ( lll )  . 
however , since larger left lobe adc / fa values can be attributed to artefacts , right lobe values should be considered the most reliable measurements of water diffusivity within the liver . keywords liver diffusion - weighted imaging diffusion tensor imaging magnetic resonance imaging reliability introduction diffusion - weighted imaging ( dwi ) is a magnetic resonance ( mr ) technique exploiting translational motion of water molecules in vivo [ 1 ]  . 
signal intensity patterns and quantitative information provided by dwi have been intensively investigated as indirect probes of the microscopic structure of normal and pathological tissues , with special emphasis on liver imaging [ 24 ]  . 
the most exemplifica tive research application for liver dwi is the noninvasive staging of chronic liver disease , based on the assumption that increase in liver fibrosis is detectable under the form of variations in the apparent diffusion coefficient ( adc ) [ 5 ]  . 
nonetheless , conflicting results have been reported in this field , emphasising current limitations of dwi in terms of reliability of adc measurements [ 6 ] and assessment of liver parenchyma at a microscopic scale [ 5 ]  . diffusion tensor imaging ( dti ) is a variant of dwi in which additional motion - probing gradients are applied along multiple directions of the space in order to build a tensor , i.e. , a mathematical operator which better accounts for the spatial organisation of tissue microstructure . 
thanks 1 3 490 radiol med ( 2015 ) 120 : 489497 to technical advances making dti less sensitive to physiological abdominal motions , applications for this technique are now extending from the traditional field of neuroimaging to various abdominal organs [ 7 , 8 ]  . 
liver dti ( ldti ) has been advocated as a tool to stage liver fibrosis , based on the assumption that such a technique can refine diffusion information ( a ) in functional terms , by providing more robust measurements of the adc ; ( b ) in microstructural terms , by accounting for anisotropy effects as expressed by the fraction of anisotropy ( fa ) [ 9 ]  . 
despite promising results on an animal model [ 10 ] , preliminary studies performed on humans show that conventional dwi outperforms ldti in assessing liver fibrosis [ 9 , 11 ] , suggesting that the technique is still in its infancy . 
in particular , to our knowledge no previous studies investigated to what extent quantitative parameters provided by ldti are reliable , that isby definitionconsistent and repeatable through different measurements [ 12 ]  . the aim of this study was to prospectively evaluate the reliability of quantitative ldti measurements performed on the same individuals by assessing ( a ) whether adc and fa values overlap when measured through different liver levels and / or different imaging sessions ( analysis of consistency ) ; ( b ) to what extent variability affects adc and fa measurements on an intra - session and inter - session basis ( analysis of repeatability )  . materials and methods study population this study is compliant with regulations of our country , and was performed as a part of an ethics committee - approved trial investigating the role of diffusion techniques in liver imaging . 
in both session 1 and session 2 , the ldti sequence was repeated twice , with a 1 - h pause between the two acquisitions . dti protocol this study was performed on a 3.0 t magnet ( achieva ; philips medical systems ; eindhoven , the netherlands ) 400 mm ; matrix 160 using a 16 - channel xl - torso coil . 
for each study acquisition , a preliminary t2 - weighted single - shot turbo spin echo ( ss - tse ) sequence was acquired in coronal and transverse planes for anatomical localisation and exclusion of collateral findings . 
we then transversally acquired ldti using the in - built single - shot echo planar imaging ( epi ) sequence with the following parameters : tr 5 , 870 ms ; te 60 ms ; field of view ( fov ) 300 116 pixels ; flip angle 90 ; slice thickness 4 mm ; interslice gap 0 mm ; number of slices 50 ; bandwidth in the epi frequency direction 29 , 717 hz ; number of signal averages 2 ; acquisition time 3 min 57 s . 
a maximum b value of 1 , 000 s / mm2 was chosen as a reasonable compromise between image quality and the suppression of perfusion effects [ 13 ]  . 
the ldti sequence was acquired during free breathing followed by post - processing adjustment for respiratory mismatch , which has been recently shown as the most repeatable technique to measure diffusion parameters [ 14 ]  . 
we also used the sensitivity encoding ( sense ) algorithm of parallel imaging ( acceleration factor 2 )  . phantom study we performed a preliminary phantom study to validate our model . 
 the tubes contained distilled water that reached 0 c by thermal equilibrium obtained by filling the jars with ice cubes and water 45 min before the scan [ 15 ]  . 
the phantom was then wrapped into a pad to absorb surface condensate , and subsequently positioned into the scanner for 15 min before starting with acquisitions , in order to reach the equilibrium and avoid any convective motion . 
1 the study phantom consisted of three polypropylene tubes containing distilled water , each of them fixed into a plastic jar filled with water and ice cubes ( a )  . 
after each single scan , apparent diffusion coefficient ( adc ) measurements were performed by placing a region of interest ( roi ) on the central slice of the tubes ( c ) were then calculated as the average of six measurements performed during repeated intra - session scans . image analysis using the software implemented in the vendors workstation , adc maps and fa maps were built in accordance with the standard approach [ 13 ] described in the appendix . 
for each acquisition , the read0 s / mm2 ers identified two liver reference slices on b images , located 2 cm above ( upper slice ) and 2 cm below ( lower slice ) the portal plane , respectively . 
the rois were then copied and pasted on the adc map and fa 3 mm2 / s , whereas map , where adc was expressed in fa was expressed as a dimensionless value ranging from 0 ( isotropic diffusion ) to 1 ( infinite anisotropy ) [ 1 ] , respectively . 
for each imaging session , adc and fa values were then calculated at four reference levels by averaging three rois placed on ( a ) the right lobe at the upper reference slice ( right upper level ; rul ) ; ( b ) the left lobe at the upper reference slice ( left upper level ; lul ) ; ( c ) the right lobe at the lower reference slice ( right lower level ; rll ) ; and ( d ) the left lobe at the lower reference slice ( left lower level ; lll )  . 
care was taken in positioning the rois far from vessels / biliary ducts and in a similar position in the interand intra - session acquisitions repeated on the same subject . since the calculation of variability is based on the means of repeated measurements ( see below ) , we show average intra - session adc and fa values to avoid data redundancy , in accordance with the model proposed by cutajar et al . 
overall , larger cv was 12.25 % for adc and 16.65 % for fa , with average values of 9.51 % ( session 1 ) and 9.73 % ( session 2 ) 0 s / mm2 images , according fig . 
on the upper reference slice ( a ) , three rois were placed in the right liver lobe ( segment vii lateral , segment viii medial and segment viii ) and left liver lobe ( segment iv , segment ii medial , segment ii lateral ) in order to obtain average measurements at the right upper level ( rul ) and left upper level ( lul ) , respectively . 
on the lower reference slice ( b ) , three rois were placed in the right liver lobe ( segment v , segment vi lateral and segment vi medial ) and left liver lobe ( segment iv , segment iii medial , segment iii lateral ) in order to obtain average measurements at the right lower level ( rll ) and left lower level ( lll ) , respectively versus session 2 adc and fa values obtained at the same reference level , using the paired t test . to test repeatability , we made two basic assumptions based on measurement error principles [ 16 , 17 ]  . 
 second , we assumed that repeats measured intraindividually vary around the true value because of the measurement error , which is represented by the standard deviation of repeated measurements common to all subjects , namely the within - subject standard deviation ( wssd )  . 
on this basis , we assessed the magnitude of adc / fa variability under the form of the coefficient of variation ( cv ) [ 16 ] , which was calculated as reported in the appendix . 
4 liver adc values measured on right ( rul , rll ) and left ( lul , lll ) reference levels in ldti session 1 ( a ) and session 2 ( b ) acquired 2 weeks later . 
5 liver fa values measured on right ( rul , rll ) and left ( lul , lll ) reference levels in ldti session 1 ( a ) and session 2 ( b ) acquired 2 weeks later . 
left liver lobe values are significantly larger ( < 0.005 / 6 ) than right liver lobe values 3 mm2 / s for the adc , and 12.93 % ( session 1 ) and 11.82 % ( session 2 ) for fa . 
by averaging all intrasession and inter - session measurements , the mean cv was 9.11 % in the case of adc , and 12.70 % in the case of fa . 10 according to the blandaltman analysis ( table 3 ) , the absolute magnitude of the difference between session 1 versus session 2 measurements did not exceed 3 mm2 / s ( adc ) and 0.010 ( fa ) , respectively , 0.042 corresponding to close limits of agreement . 
the difference between two measurements for the same subject was less than the coefficient of repeatability of all the inter - session measurements ( table 3 )  . discussion ldti has been advocated as a tool to refine quantitative assessment of liver diffusion [ 9 ]  . 
we showed that quantitative results of ldti are consistent , i.e. , liver adc or fa do not significantly differ when measured at the same anatomical level in different imaging sessions . 
one might speculate that , although no significant age - related variation in liver adc and other diffusion and perfusion indexes have been found [ 23 ] , greater mean age of volunteers in the above study ( 44.10 years ) compared to ours ( median age 23 years ) might have translated into changes in fa . 
however , despite the absence of a definite explanation for this discrepancy , our results better match previous dwi findings suggesting that water diffusion is nearly isotropic in liver parenchyma [ 5 , 24 ]  . the phantom study showed that adc values do not significantly vary across the field - of - view ( right , centre and left positions )  . 
 [ 14 ] on a 1.5 t magnet , suggesting that , regardless of the field strength , additional and / or different artefacts may be the cause of the right - to - left difference we observed , including the effects of cardiac motion . 
we believe that right lobe adc and fa values should be considered more reliable measurements of water diffusivity within the liver than left lobe values , unless further studies elucidate causes , solutions ( e.g. , ldti with cardiac - gated sequences ) and the potential clinical significance of our finding . 
on the bright side , right - to - left difference occurred at a similar degree on intra - session and inter - session basis , since left lobe adc and fa values were similar ( a ) during different imaging sessions and ( b ) at the same anatomical levels ( lul and lll )  . 
hence , although right - to - left difference should represent a caveat in interpreting ldti results , it can be considered as a constant and predictable effect . repeatability refers to variability associated with independent measurements performed on the same equipment at different times [ 27 , 28 ] , which is the case of this study . 
 [ 29 ] , who examined healthy subjects with conventional dwi , the average intra and inter - session cv for the repeatability of adc at 3.0 t is 14 % . 
on the other hand , our results are in line with those obtained on healthy subjects using conventional dwi sequence on a 1.5 t scanner in a different study by colagrande et al . 
in accordance with these authors , we hypothesised that such a difference might be attributed to the fact that the fa map is intrinsically noisier , as it is a calculation of difference making it an accumulated error [ eq . 
in this light , cv values of adc and fa are difficult to compare [ 16 ] , and the variations in fa we found can be considered acceptable . given the potential of adc and fa values as instruments to follow up patients with chronic liver disease over time [ 29 ] , we performed an analysis of inter - session agreement between ldti measurements . 
notably , reliability and agreement are not strictly synonymous : reliability has been related to the performance of a diagnostic tool in a certain population sample , whereas the agreement is more a characteristic of the measurement tool itself [ 30 ]  . 
as confirmed by close limits of agreement ( the largest possible differences within 95 % observations one can expect ) , such minimal shifts between measurements are unlikely to be of significance for ldti applications , e.g. , when staging / grading chronic liver disease or characterising focal liver lesions . our study shows some limitations . 
however , in order to increase data sampling ( a ) we performed repeated measurements in the same subject ( three measurements at each of the four reference levels ) ; ( b ) we scanned subjects twice during each imaging session . 
second , we did not assess reproducibility , which by definition accounts for the variability inherent to the same diagnostic examination performed with different equipment [ 19 , 28 ]  . 
low reproducibility is a serious concern in conventional dwi of the liver [ 19 ] , leading to discrepancies in adc determination that have been attributed to differences in b values , imaging sequence , te and various other factors [ 31 ]  . 
on the other hand , the literature data on ldti are still limited , and our results might represent a preliminary contribution to the technical standardisation of this technique and provide reasonable reference values for future studies in the clinical setting . in conclusion , we found that the adc and fa measurements of normal liver parenchyma provided by ldti do not significantly differ when measured at the same anatomical level across different imaging sessions , as confirmed by assessing variability with the cv . 
we observed larger adc and fa values in left liver lobe compared to right liver lobe , though right - to - left difference occurred at a similar degree on intra - session and inter - session analyses . 
since larger left liver lobe values are presumably the effect of yet undetermined confounders , right liver lobe measurements should be considered the most reliable in assessing water diffusivity with ldti . conflict of interest no financial support of any nature was provided for this study . appendix calculation of adc ( apparent diffusion coefficient ) and fa ( fraction of anisotropy ) values in brief , three main eigenvalues of diffusivity ( 1 , 2 , 3 ) were computed from the 3 3 diffusion tensor matrix , in order to calculate adc and fa as follows [ 13 ] : ( ( cid : 31 ) 1 ( cid : 31 ) 2 ( cid : 31 ) 3 ) / 3 , ( cid : 31 ) 2 ( cid : 31 ) 2 map and fa map . 3 / 2 ( cid : 31 ) ( ( cid : 31 ) 1 adc ) ( ( cid : 31 ) 2 adc ) ( ( cid : 31 ) 3 adc ) adc and fa values were then displayed on the adc ( cid : 30 ) / ( cid : 31 ) 2 calculation of the coefficient of variation the coefficient of variation ( cv ) was used as a measure of repeatability of the adc and fa measurements . 
cv was calculated according to the formula [ 16 ] : ( wssd / mean ) 100 , where wssd is the within - subject standard deviation and mean is the average of intra - session or inter - session measurements . 
the wssd is the common standard deviation of repeated measurements performed on the same subject , which enables us to measure the size of the measurement error [ 17 ]  . 1 3 radiol med ( 2015 ) 120 : 489497 calculation of the coefficient of repeatability this coefficient was proposed by bland and altman [ 17 ] , and represents the expected value of repeatability under which the difference between two measurement should lie for 95 % of pairs of observation . 
bergenfeldt department of surgery , skane university hospital , lund , sweden e - mail : m.bergenfeldt@telia.com in this small , highly selected cohort we conclusions found rfa safe and efficacious with a low local recurrence rate and a median survival above that expected with systemic treatment . 
our data are in line with previous studies and underscore the need for a large prospective study using optimal chemotherapy regimens and rfa / surgery to clarify whether intense treatment protocols can prolong survival for certain patient groups . keywords metastatic breast cancer liver metastases radiofrequency ablation introduction breast cancer is the most common type of cancer among women , with a life - time risk of almost 10 % . 
however , approximately 20 % will experience recurrence of the disease either at a loco - regional or distant level [ 1 ]  . during the past decades , adjuvant therapy has markedly improved the survival for patients with primary breast cancer . 
preferred metastatic sites from primary breast cancer include bone , lymph nodes , liver , lung and bra patients who present with bone metastasis only are known to have longer survival compared to patients with visceral metastases [ 1 , 3 , 4 ]  . 
 also , patients with hepatic metastases only seem to have improved survival compared to patients with both hepatic and other visceral metastases [ 2 , 5 , 6 ]  . 
however , all studies seem to indicate that the treatment of liver metastases might be beneficial to selected patients with no extrahepatic sites except maybe bone metastases [ 8 ]  . 
we report results from 32 non - operable patients treated with radiofrequency ablation ( rfa ) at our institution . patients and methods all consecutive patients treated with rfa at herlev university hospital in the period 1996 to 2010 were included . 
 patients were required to have histologically or cytologically confirmed mbc with maximum six liver metastases measuring maximum 5 c patients with radiological evidence of limited extra - hepatic disease , defined as bone metastases , loco - regional lymph nodes or cutaneous metastases , and stable disease for the last 6 months were included . 
progression - free survival ( pfs ) was calculated as time from first rfa to the first observation of disease progression for intraas well as extra - hepatic progression , to death from any cause or the most recent assessment . 
when the pre - set target temperature of 105 c was reached in all five sensors , the electrodes were expanded one step further and the heating to target temperature repeated . 
at the last two steps of expansion with ablation volume diameters of 4 and 5 cm , the heating prevailed for 7 min at each step after the pre - set temperature was reached in all five sensors . 
the rfa procedure was considered successful if the temperature exceeded 70 c in all of the five temperature sensors after the cool - down period . 1 3 538 radiol med ( 2015 ) 120 : 536541 fig . 
3 contrast - enhanced ultrasound ( ceus ) of the liver was performed before and after rfa in all procedures the intended ablation margin was at least 5 mm larger than the tumour border and contrastenhanced ultrasound ( ceus ) was performed before and after the ablation to ensure this had been achieved . 
if a target temperature of less than 70 c was detected after the cool - down period in any of the sensors or if the ceus evaluation visualised areas with persisting perfusion , the rfa procedure was repeated . pretreatment evaluation and followup and discharged from the hospital no later than the next day provided their condition was stable . 
if no residual tumour activity or hepatic progression was detected , follow - up continued with ct and ceus every 3 months for the first 2 years and then every 6 months . 
in the case of recurrence or residual active tumour after the first rf the procedure was repeated . pre - treatment evaluation included complete medical history , physical examination , and appropriate laboratory tests . 
 after ablation , patients were admitted for same - day care results data from 32 consecutive patients with mbc treated at the department of oncology , herlev university hospital , copenhagen , denmark , from 1996 to march 2013 were retrieved . 
fourteen patients ( 44 % ) had received adjuvant chemotherapy with an anthracycline , a taxane or both , 16 patients ( 50 % ) had received adjuvant antihormonal therapy . 
twenty - six patients ( 82 % ) had oestrogen receptor ( er ) positive tumours , four patients ( 12 % ) were er negative and er status was unknown for two patients ( 6 % )  . 
forty - seven per cent of patients had extra - hepatic metastases , eight patients ( 25 % ) had bone metastases , two patients ( 6 % ) had bone and lung metastases , two ( 6 % ) patients had bone and lymph node metastases while one patient each ( 3 % ) had lymph node , bone marrow or ovarian metastases in addition to liver metastases . 
age at time of rf treatment also differed substantially , from 30 to 83 years with a median of 54 years ( table 1 )  . a total of 52 rfa treatments were given to 32 patients . 
four patients did not receive any consolidation treatment , 26 rfa treatments were followed by endocrine therapy and 19 by a chemotherapy - based regimen , while four patients were treated with trastuzumab monotherapy ( table 2 )  . 
chemotherapy consisted of vinorelbine and docetaxel in five patients ( 26 % ) , while capecitabine and gemcitabine / carboplatin were given in three patients ( 16 % )  . 
ten patients ( 19 % ) were treated with subsequent lines of therapies including chemotherapy and an endocrine regimen . efficacy numbers of liver metastases varied from 1 to a maximum of 6 in one patient and the size of the metastases was median 20 mm ( range 950 mm ) ( table 2 )  . 
 time to intrahepatic progression was median 11 months ( range 1.6184 months ) and median time to extra - hepatic progression was 12 months ( range 2102 months )  . 
survival at 1 , 2 and 3 years were 87 , 68 and 48 % , respectively . adverse events the rfa procedure was generally well tolerated and no major complications were observed . 
most common grade 1 and 2 adverse events were abdominal pain in eight patients ( 25 % ) , nausea in seven patients ( 22 % ) , vomiting in four patients ( 12.5 % ) , fever in two patients ( 6 % ) and one patient each experiencing headache ( grade 1 ) , dizziness ( grade 1 ) , wound bleeding ( grade 2 ) and flu - like symptoms ( grade 2 )  . 
sixteen patients ( 50 % ) did not experience any side effects . discussion generally , patients with mbc have a poor prognosis with median survival ranging from 18 to 30 months [ 1113 ]  . 
however , location of the metastatic lesion has a large impact on the prognosis as median os drops to 1216 months in patients with liver metastases [ 14 , 15 ] , whereas patients with bone or lymph node metastases at first relapse live median 2430 months after diagnosis [ 4 , 16 ]  . 
however , current systemic chemotherapy can improve survival to around 25 months [ 2 , 5 ]  . traditionally bc has been regarded as incurable once the disease has disseminated beyond loco - regional sites , irrespective of the number or location of the metastases . 
 however , following the past decade of successful improvement of survival in patients with colorectal cancer undergoing minor or major hepatectomy [ 17 , 18 ] , interest has arisen in a similar approach to patients with liver metastases from bc . 
however , metastatic patterns for patients with breast cancer and colorectal cancer are not comparable and the question is whether patients with hepatic metastases from breast cancer will have the same survival benefit as patients with colorectal cancer when treated for liver metastases . in this paper we report on a small number of patients treated with a combination of chemotherapy , antihormonal treatment and doppler us - guided rfa of liver metastases . 
we report a median survival after first rf treatment of 33.5 months and 1 , 2 and 3 year survival rates of 87 , 68 and 48 % , respectively . 
however , outcome depends heavily on the patient population and includes factors such as radiol med ( 2015 ) 120 : 536541 number of extra - hepatic metastatic sites , time interval from primary diagnosis to metastatic disease and number of liver metastases allowed . 
 whereas one study performed extensive pre - operative staging to exclude patients with extra - hepatic disease [ 24 ] , we included 15 patients ( 47 % ) with one or more extrahepatic metastatic sites . 
another study reported the interval between primary diagnosis and liver metastases to be 83 months , offering an explanation for the high os of 60 months reported in that study [ 23 ]  . 
the number of treated metastases per patient also varies from studies allowing a maximum of five metastases no larger than 5 cm in diameter [ 20 , 22 ] to studies where patients with up to 13 metastases sized up to 11.5 cm were treated [ 19 , 21 ]  . the local recurrence rate in the ablation cavity was 22 % which is comparable to the recurrence rate seen in colorectal cancer [ 25 ] and indicates that rfa is an effective local treatment . altogether , data seem to indicate a benefit from rf treatment with os of 3060 months compared to around 25 months for patients with liver metastases treated with standard care chemotherapy and a local control rate of 78 % . 
all patients underwent conventional mr imaging and diffusion - weighted imaging ( dwi ) before the start of therapy , and after 1 , 3 and 6 months of therapy . 
mariotti dipartimento di oftalmologia , universit politecnica delle marche , ancona , italy results mean adc value of ocular melanomas signifi cantly increased as early as 3 months after therapy ; tumour volume significantly decreased as early as 6 months after therapy . 
the adc values of ocular melanomas before therapy significantly correlated with tumour regression . conclusions dwi may provide an early surrogate biomarker for prediction and early detection of tumour response to eye - preserving therapies in ocular melanoma . keywords ocular melanoma diffusion - weighted imaging apparent diffusion coefficient therapy proton beam introduction uveal melanoma is the most common primary intraocular tumour in adults [ 1 ]  . 
today , enucleation has been supplanted by radiotherapy as the standard of care for patients with uveal melanoma , offering patients preservation of an intact eye and , in many cases , preservation of visual function . 
treatment modalities , such as plaque radiotherapy and proton beam radiotherapy , are used in a few centres in selected cases [ 2 ]  . the diagnosis and follow - up of uveal melanoma are based upon fundoscopic examination by an experienced clinician , which is followed by further characterisation with specialised noninvasive testing techniques such as ultrasound . 
for choroidal melanomas , ultrasonography is used to help establish the diagnosis , to evaluate possible extraocular extension , to estimate tumour size for periodic observation and to plan therapeutic intervention . 
ultrasonography is excellent for evaluating intravitreous tumour 1 3 radiol med ( 2015 ) 120 : 526535 size , but is relatively insensitive to extrascleral extension [ 3 ] and relatively dependent on a skilled operator [ 4 ]  . ocular magnetic resonance ( mr ) imaging can be used to assess the extent of ocular melanoma , to visualise possible extraocular spread and to plan proton beam therapy . 
 diffusion - weighted imaging ( dwi ) helps evaluate free motility of water - bound protons within tissues [ 5 ] and is routinely used for diagnosis and management of acute stroke [ 6 ]  . 
apparent diffusion coefficient ( adc ) , the quantitative parameter of dwi , has been proposed as the technique of choice for detection of early response to treatment in brain tumours and head and neck cancers [ 79 ]  . the current assessment of response to treatment of central nervous system tumours is based on evaluating changes in tumour size on anatomical computed tomography ( ct ) or mr images several months after the end of the treatment course . 
recently reported a correlation between the minimum adc of tumour regions and cell density in human gliomas ; regions with high cell density had lower adc than regions with low cell density [ 11 ]  . 
some studies have investigated the value of dwi quantitative parameters in predicting and monitoring treatment response in metastatic or primary brain tumours ( high - grade gliomas ) [ 10 , 12 , 13 ]  . 
regional adc changes , estimated from pre and post - treatment regions of interest ( rois ) , have been proposed to predict brain tumour response to radiation / chemotherapy , with increased adc associated with a more favourable clinical course [ 12 , 13 ]  . 
such an ability to predict response might enable early termination of treatment in nonresponding patients , prevent additional toxicity , and allow for early changes in treatment [ 12 ]  . 10 recently , erb - eigner et al . 
demonstrated that ocular melanoma shows a marked diffusion restriction ( with an 6 mm2 / s ) and that dwi helps adc of less than 1 , 000 differentiate ocular tumours from retinal detachment [ 14 ]  . 
the purposes of this prospective study were to determine the adc values of ocular melanoma and to assess whether variations in adc constitute a reliable biomarker of response to proton beam therapy . materials and methods patients this study was a prospective , consecutive , case series performed between may 2012 and march 2013 . 
the study was conducted in accordance with the recommendations of the local ethics committee , and informed consent was obtained from the patients . all patients were examined by a senior ophthalmologist who specialises in ocular tumours , and the final clinical diagnosis of ocular melanoma was made on the basis of fundoscopic and ultrasonographic findings before the mr imaging examination . 
however , ophthalmoscopy is the criterion standard for diagnosing ocular melanoma , and the diagnostic accuracy is reported as high as 99.7 % [ 15 ]  . all patients underwent serial mr imaging examination ( four examinations per patient : one baseline examination and three follow - up examinations , 1 , 3 and 6 months after the beginning of the therapy , respectively )  . 
in order to avoid bias , the baseline examination was performed after the tantalum clipping . to exclude distant metastases , all patients underwent a multidetector computed tomography ( mdct ) examination of the chest , abdomen and pelvis before the beginning of the therapy . proton beam therapy protocol insertion of tantalum markers a sectoral peritomy is performed , involving only a third or half of the eye . 
before dividing any rectus muscles , the suture knot - to - limbus distances are measured and recorded ; these measurements help re - insert the muscle ( s ) more precisely by ensuring that the original knot - to - limbus distances are retained . 
 marker - tumour , markermarker and marker - limbus measurements are taken for each marker . a 3d computer model of the eye is generated according to ocular biometry , tumour ultrasonography , colour photography , intraoperative marker measurements as well as radiographs showing the marker positions . 
the direction of gaze is adjusted so as to minimise collateral damage to lens , optic nerve and fovea . 1 3 528 proton beam treatment a total dose of 5370 gy is administered in four daily fractions . 
correct positioning of the eye is checked by radiography and by observing the eye with a closed - circuit tv during administration of the radiotherapy . with choroidal tumours , proton beam radiotherapy is administered with safety margins of 2.02.5 m to prevent collateral damage to the optic nerve and fovea , these margins can be reduced with small , juxtapapillary and juxtafoveal tumours if the patient is highly cooperative and if the measurements are known to be accurate . 
wider safety margins of up to 4 mm may therefore be used in such cases [ 16 ]  . imaging technique mr imaging was performed with a closed - configuration superconducting 1.5 - t system ( signa hdxt ; ge healthcare , milwaukee , wis ) with 57.2 mt / m gradient strength and 120 t / m / s slew rate , using an eight - channel highresolution head coil with array spatial sensitivity technique ( asset ) parallel acquisition . 3 , 700 / 50 , turbo factor 3 , acquisition matrix the orbital imaging protocol included ( a ) axial and coronal t2 - weighted turbo spin - echo spectral presaturation with inversion recovery ( repetition time ms / echo 12 , number of signals time ms acquired 256 ) ; ( b ) axial 256 and coronal t1 - weighted turbo spin - echo ( repetition time 2 , number ms / echo time ms of signals acquired 224 ) 256 sequences . 
after intravenous administration of 0.2 ml gadoteric acid ( gadoterate dimeglumine , dotarem , 0.5 mol / l ; 550 / 14.9 , turbo factor 3 , acquisition matrix radiol med ( 2015 ) 120 : 526535 guerbet , roissy , charles - de - gaulle cedex ; france ) per kilogram of body weight , axial and coronal t1 - weighted spin - echo spectral presaturation sequences were performed 450 / 15.1 , turbo fac ( repetition time ms / echo time ms tor 2 , acquisition 256 )  . 
all sequences had a section thickmatrix ness of 3 mm , an intersection gap of 0.3 mm , and a field of view of 160 lids and optic chiasm . 160 mm that included all orbital structures , 2 number of signals acquired 256 all acquisitions also included axial spin - echo echoplanar dwi sequence with b - values of 0 and 1 , 000 s / mm2 ( repetition time ms / echo time ms 4 , 800 / 89.9 , asset 4 mm , intersection 2.0 , section thickness gap 0.4 mm , acquisition matrix view 8 ) performed before contrast material administration . 
adc maps were created in all patients . 200 mm , number of signals acquired 192 , field of 192 200 all mr examinations also included a standard brain study . image analysis for image analysis , data were transferred to a ge workstation . the images of conventional ocular mr were evaluated by two radiologists in consensus ( a neuroradiologist with 8 years of clinical experience and a neuroradiology fellow with 3 years of practice experience )  . 
in all sections in which tumour was present , we manually outlined this structure and calculated the tumour volume , taking section thickness into account [ 17 ] ; in particular , tumour volume was obtained by multiplying the area of tumour outlined on each contrast - enhanced axial t1 - weighted image by the slice thickness . 
the volumes from the first and fourth scans for each patient were used to calculate percentage variation of tumour volume after 6 months of therapy ( tumour percentage regression )  . 
percentage variation of tumour volume after 1 and 3 months of therapy was also calculated . the image quality of the dw images was assessed on a three - point scale in consensus by the two radiologists ( 1 , minor distortion artefact , mass c1early visible ; 2 , moderate distortion artefact , mass blurred ; and 3 , major distortion artefact , mass not visible )  . 0 , b 1000 s / mm2 in all the four time - point examinations , the quantitative measurements were performed as follows ( as previously described [ 14 , 17 , 18 ] )  . 
the roi was delineated within the tumour lesion contained in the largest tumour cross - section and was defined as slightly smaller than the actual lesions , excluding the most peripheral parts to avoid partial volume effects . 
macroscopically evident necrotic tumour tissue ( parts of the tumour showing a relatively high signal intensity on t2 - weighted images , with corresponding areas of relatively scarce or no enhancement on contrast - enhanced images ) or cystic parts was not identified within any of the ocular melanoma b fig . 
1 axial magnetic resonance ( mr ) images in a 41year - old woman with ocular melanoma of the right eye , who exhibited poor response to treatment ( ad before therapy ; eh 1 month after therapy ; il 3 months after therapy ; mp 6 months after therapy ) ( a , e , i , m t2 - weighted turbo spin - echo spectral presaturation with inversion recovery images ; b , f , j , n postcontrast t1 - weighted spin - echo spectral presaturation images ; c , g , k , o diffusion - weighted images ; d , h , l , p apparent diffusion coefficient , adc , map )  . 
b the mass shows moderate , homogeneous contrast enhancement ( white arrow ) and is hyperintense in relation to the retinal detachment along the posterior aspect of the globe ( white arrowhead )  . 
p tumour adc value slightly increases ( adc : 1 , 460 6 mm2 / s ) 10 10 10 10 neither in the baseline examination , nor in the follow - up ones . all measurements were repeated in two other different sessions , resulting in a total of three subreadings . 
the values of all subreadings were averaged . percentage variation of adc value after 1 month and 3 months of therapy was also calculated . statistical analysis all data are presented as the mean standard deviation ( sd )  . 
mean adc measurements and the mean tumour volumes of the four examination ( baseline , 1 , 3 and 6 months ) were compared by one - way analysis of variance ( anova ) and , if the difference was significant , with repeated measures followed by post - hoc multiple comparisons ( tukey kramer test )  . 
 correlation between data was also tested by means of pearsons r . the reproducibility of adc measurements was assessed by calculating two parameters , the within - subject standard deviation ( sw ) , and the coefficient of variation ( cv ) of measurements . 
the sw is the common standard deviation of the repeated measurements and was calculated as the square root of the average of the variances of the measurements of each participant . 
the cv is a ratio of the standard deviation over the mean and was calculated as the square root of the residual mean squared values of three measures , divided by the mean . 1 3 530 radiol med ( 2015 ) 120 : 526535 1 3 radiol med ( 2015 ) 120 : 526535 all analyses were performed by using statistica 7.0 for windows , and the significance level was established at 0.05. results characteristics of the patients twelve eyes of 12 patients were evaluated . 
therefore , the final study population consisted of 10 eyes of 10 patients [ eight women and two men ; mean age ( sd ) , 42 years ( 10.5 ) ; range 3055 years ] ( table 1 )  . the right eye was affected in six patients ( 60 % ) and the left eye in four ( 40 % ) patients . 
2 axial mr images in a 55year - old woman with ocular melanoma of the left eye , who exhibited good response to treatment ( ad before therapy ; eh 1 month after therapy ; il 3 months after therapy ; mp 6 months after therapy ) ( a , e , i , m t2 - weighted turbo spin - echo spectral presaturation with inversion recovery images ; b , f , j , n postcontrast t1 - weighted spin - echo spectral presaturation images ; c , g , k , o diffusion - weighted images ; d , h , l , p adc map )  . 
our results demonstrated the potential value of this technique in the evaluation of melanoma response to proton beam therapy . the purposes of this prospective study were to determine the adc values of ocular melanoma and to assess whether variations in adc constitute a reliable biomarker of response to proton beam therapy . 10 172 10 160 6 mm2 / s the first of our purposes was to determine the adc values of ocular melanoma . 
such a difference in the 891 adc values described could be due mainly to significant variability depending on the coil systems , scanners , vendors and field strengths used for mr imaging . 
although their measurement methods were very similar to ours , interobserver variability and operator dependence of roi positioning could play an important role too . similarly , to the cited authors , we did not use histogram analysis when measuring tumour adc . 
nevertheless , it is known that some tumours such as brain gliomas , especially if high grade , may demonstrate a wide spectrum of histological features , ranging from grade ii to grade iv , making the adcs widely variable between different regions of the tumour . 
image artefacts because of changes in tissue susceptibility , chemical shift , radiofrequency effects , and / or pulse sequence physics are more noticeable and sometimes harder to suppress at 3 t [ 20 ]  . 
in particular , dwi can suffer from increased warping and susceptibility artefacts at 3 t [ 20 , 21 ]  . previous studies [ 22 ] have shown that when body dw - mr imaging protocols are transferred from 1.5 to 3 t without further modifications , image quality is seriously degraded and images suffer from severe distortions and signal losses , so qualitative assessment and quantitative analysis can be problematic . 
protocol adjustment at 3 t is , therefore , mandatory because compromised image quality can have serious implications in diagnosis and quantification for treatment response monitoring . the second of our purposes was to assess whether variations in adc constitute a reliable biomarker of response to proton beam therapy . our study revealed the potential of dwi in the detection of early tumour response in ocular melanoma patients treated with proton beam therapy . 
showed that adc variations coincide with or precede volume changes in ocular adnexal lymphomas following treatment and increase the capability of mr imaging in determining early treatment response or failure [ 23 ]  . some oncological studies demonstrated that the pretreatment adc value is a predictor of response in cancer patients and have shown that tumour with low baseline pretreatment adc values responds better to therapy than tumours that exhibit high pretreatment adc values [ 24 , 25 ]  . 
they found a significant correlation between tumour adc and both cell density and necrotic fraction ; the adc of tumours decreased with increasing cell density and increased with increasing necrotic fraction . 
in addition to its simplicity in estimating adc from the dwi data , the adc value is quantitative and magnetic field independent such that it is one of the most suitable metrics for multicentre and longitudinal studies [ 7 ]  . one of the limitations and challenges to orbital dwi is image degradation and distortion as a result of susceptibility artefact from adjacent bones and pneumatised paranasal sinuses . 
ocular melanomas are located at the air - tissue interface , which increases the susceptibility artefacts on dwi sequences [ 7 ]  . recently , advances in parallel imaging echo - planar dwi techniques have led to improved image quality making this technique increasingly used in the study of orbital structures . 
further improvements in dwi sequences are warranted to improve diagnostic quality , such as periodically rotated overlapping parallel lines with enhanced reconstruction ( propeller ) , which uses fast spin - echo acquisition and central k - space oversampling , reducing susceptibility artefacts and artefacts related to gross eye motion [ 18 , 21 ]  . dwi can also represent a useful technique for staging of melanoma . 
demonstrated that although contrast - enhanced mr imaging is still required for evaluating the brain , whole - body dwi without additional whole - body mr imaging contrast - enhanced sequences is promising for the detection of extracranial metastases in melanoma patients [ 28 ]  . the present study has some limitations : first , the small number of patients did not allow us to determine a threshold of adc value change for the prediction of tumour response . 
second , in our study , we used two b - values for adc calculations : 0 and 1 , 000 s / mm2 , and we did not investigate the possible influence of other b - values on the adc of melanomas . 
third , mr examinations were performed with a head coil rather than with a dedicated coil . conclusions in conclusion , this preliminary prospective study suggests that adc might be helpful in the follow - up of ocular melanomas treated with proton beam therapy and could represent a potential biomarker for prediction and early detection of treatment response to eye - preserving therapies . 
nevertheless , further investigations with larger series and long - term follow - up are needed to validate the role of adc in studying response of ocular melanoma to proton beam therapy . 1 3 radiol med ( 2015 ) 120 : 526535 5 . 
therefore , the goal of the current study was to evaluate preoperative ultrasound characteristics as prognostic factors that could affect survival rate after liver resection for hepatocellular carcinoma ( hcc )  . materials and methods a total of 104 hcc patients who underwent resection were retrospectively reviewed with regard to their clinical data , preoperative ultrasound characteristics , and survival rate . 
preoperative ultrasound parameters included cirrhosis , tumour site , size , echo pattern , portal vein thrombosis , intra - tumour blood flow signal , peak systolic velocity ( vmax ) , and resistance index ( ri )  . 
hu department of ultrasound in medicine , shanghai institute of ultrasound in medicine , shanghai jiao tong university affiliated sixth peoples hospital , shanghai jiao tong university school of medicine , no . 
application of the cox multivariate proportional hazards model indicated that tumour size and blood flow signal in the tumours were independent prognostic factors . conclusions the overall survival for hcc patients undergoing hepatic resection can be stratified on a sonographic basis of tumour size and intra - nodular vasculature . 
these prognostic factors may be useful to determine appropriate treatment for hcc patients . keywords hepatic carcinoma ultrasound prognosis cox analysis blood flow signal introduction globally , hepatocellular carcinoma ( hcc ) is one of the most prevalent malignant tumours [ 1 ] , accounting for almost 150 , 000 deaths annually in china , and half a million deaths worldwide . 
in the past two decades , several effective therapeutic options have been developed , i.e. , systematic liver resection , transcatheter arterial chemoembolisation ( tace ) , percutaneous ethanol injection , percutaneous microwave coagulation therapy , radiofrequency ablation , arterial infusion chemotherapy for advanced hcc , and liver transplantation [ 24 ]  . 
however , even after hepatic resection , the outcome of patients with hcc remains poor because of low survival and high recurrence rates after the procedure [ 5 , 6 ]  . 
therefore , it is important to establish an 1 3 radiol med ( 2015 ) 120 : 504510 accurate prognostic system in patients with hcc to give each patient an appropriate treatment protocol . 
furthermore , it is important to decide whether to treat a patient aggressively , while avoiding the overtreatment of patients who would not tolerate the treatment , or patients whose life expectancy rules out any chance of treatment when the disease is too far advanced to live longer . 
clinically , liver cirrhosis [ 7 ] , encapsulation [ 8 ] , chronic hepatitis , alpha fetoprotein ( afp ) level [ 9 ] , histological grade [ 10 ] , aspartate transaminase ( ast ) [ 11 ] , alanine transaminase ( alt ) , albumin , childpugh classification [ 12 ] , tnm stage [ 13 ] , tumour number [ 14 ] , portal vein invasion [ 15 ] , microvascular invasion [ 11 ] , and surgical procedure are all involved . 
because ct ( computed tomography ) or mri ( magnetic resonance imaging ) is financially unaffordable for many patients in rural areas , us , a simple and effective imaging tool may serve as a risk stratification tool for selecting the appropriate therapy for each hcc patient . materials and methods patient population we retrospectively reviewed the records of 104 consecutive hcc patients with a single nodule hospitalised at nantong tumor hospital between november 2006 and december 2009 . 
inclusion criteria of patients were availability of complete clinical data and follow - up while exclusion criteria were incomplete clinical data and multiple hepatic tumours to exclude the influence of tumour numbers on prognosis . 
patients with only one nodule on us and ct were included in our research because we wanted to exclude the effects of number of tumours and focus on the prognosis of hcc ultrasound features . 
the patients ranged in age from 38 to 78 years ( mean of 56 years )  . clinical data the usual criteria for hepatic resection in terms of tumour status include absence of extrahepatic metastasis and absence of tumour thrombus in the inferior vena cava or main portal vein [ 16 ]  . 
fifty - seven patients were found to have hepatic cirrhosis ( 53 cases with hbv , 4 cases with hcv ) and 47 were non - cirrhotic on pre - surgical clinical evaluation . 
no patient was found to have extrahepatic metastases such as lung , brain , and bone after other routine examinations including x - ray , serum testing and ct scan . 
 postoperatively , hcc patients were subjected to followup examination every 36 months , including evaluation of liver function , serum afp , us , chest x - ray film , and ct if necessary . computed tomography ( ct ) in our centre , we routinely perform chest x - ray , us , and helical contrast - enhanced ct scan for patients with potentially resectable hcc . 
we rely on the ct scan for assessment of the relationship of the tumour to major intrahepatic vessels , any satellite tumour nodules , tumour invasion of the inferior vena cava , main portal vein or intrahepatic venous branches . 
multiphasic ct was performed using a 64 - section multidetector ct scanner ( somatom sensation 64 ; siemens medical systems , erlangen , germany ) ( gantry rotation speed 500 ms , 60 kw , pitch 11.5 , 120 kvp , 320 mas )  . 
the patients received a nonionic contrast medium [ iomeprol , 400 mg of iodine per millilitre ( iomeron 400 ; bracco imaging , milan , italy ) ] at a dose of 1.3 ml ( 520 mg of iodine ) per kilogramme of body weight . 
ultrasound images of hcc masses were obtained using an hdi 5000 scanner ( philips medical systems , bothell , wa , usa ) and a 3.2 - mhz electronic convex probe . 
on conventional two - dimensional us , the imaging features of cirrhotic background , location , echo pattern , capsulation , tumour size , and portal vein thrombus were studied in detail . 
the echogenicity of hcc is varied and the tumour mass may appear with a low - level , high - level or mixed echogenicity pattern in comparison with the surrounding liver tissue . 
the colour signal was used as a guide to obtain the doppler spectruthe sample volume used for the spectral analysis was 24 m only the intratumoural blood signal was evaluated . 
when the pulsed wave doppler was used to detect the blood flow velocity within the tumours , the us angle correction between the sound beam and the flow direction in the nodules was less than 60 . 
negative signal is the radiol med ( 2015 ) 120 : 504510 tumour size , presence of tumour capsulation , thrombus in the portal vein , tumour blood flow signals , v max , and ri . statistical analysis follow - up outcomes were obtained by using telephone calls and letters sent out from our hospital . 
at the time of the final observation ( january 2012 ) , all patients had been followed up for a minimum of 24 months ( median 34 months ; range 2461 months )  . 
survival time was calculated based on the date of surgery and date of death or , if the patient was still living at the end of january 2012 , their survival time was calculated using a right censoring survival model . 
during the follow - up , 45 patients suffered hcc recurrence , 23 patients suffered metastasis , including five bone metastases , 11 lung metastases , and seven brain metastases . 
on univariate analysis , shorter survival was associated with mixed echo pattern , tumour size > 10 cm , portal vein thrombus , more affluent flow signal , v max , and a shorter disease - free interval after an initial diagnosis of hcc . 
the japan integrated staging ( jis ) score , which combines the childturcottepugh classification 1 3 508 radiol med ( 2015 ) 120 : 504510 multivariate cox regression analysis showed that tumour size and flow signal were independent prognostic factors of hcc . tumour size in us is an important prognostic factor for hcc patients . 
vascular patterns of us have been found to be distinctly identifiable by gene expression profiling associated with cellular proliferation of hcc and were significantly related to hcc progression and poor prognosis [ 27 ]  . hcc is a highly vascularised tumour . 
elevated levels of vascular endothelial growth factor ( vegf ) and high microvessel density ( mvd ) have been found in hcc [ 6 8 ] , and greater expression of vegf has been associated with shorter survival in hcc patients [ 28 ]  . 
attempts to improve the classification and prognostic prediction of hcc are still evolving , and there is no agreement on the best staging system that can be recommended worldwide [ 21 ]  . 
post - operation pathological information is needed in all those staging systems , this representing a limitation for wide pre - operation clinical use . in our study , univariate analysis showed that echo pattern , tumour size , portal vein thrombus , flow signal , and vmax were prognostic factors for hcc after resection . 
 1 3 radiol med ( 2015 ) 120 : 504510 hcc as assessed by ct and well correlated to differentiation of hcc on histopathology of resected or biopsied specimens [ 30 ]  . 
in the future , we will strengthen our efforts to use these up - to - date imaging methods to study the relationship between vascularity and prognosis . the application of contrast - enhanced ct for screening of hcc would be expensive and invasive , and mri has the limitation of a low availability rate of the equipment [ 33 ]  . 
 us has the advantages of real - time observation , simple technique , and a noninvasive procedure compared to other imaging modalities . tumour size determines prognosis , which indicates that hcc should be detected in the early stage . 
they might also influence therapeutic strategies such as , for example , curative therapies for resectable tumours and antiangiogenic therapy for unresectable tumours . in general , recognition of the relationship between tumour size and intra - tumoural blood flow signal and poor prognosis may be an important factor in clinical decisionmaking and treatment selection for hcc patients . 
they first reviewed arterial imaging alone and subsequently added non - contrast and delayed phases to determine the overall performance . results the median total ced and annual ced were 224 and 104 msv per patient - year . 
fossaceca radiology department , university hospital maggiore della carit , c.so mazzini 18 , 28100 novara , italy omission of the unenhanced scan and the venous phase of the mdct angiography would have led to a significant reduction of about 60 % of the associated mdct radiation exposure in a single patient . conclusions evar patients received high radiation doses and the excess cancer risk attributable to radiation exposure is not negligible . 
this can be accomplished in an operating theatre using a mobile c - arm for x - ray guidance or in a dedicated angiographic suite using a fixed equip ment [ 3 ]  . 
it has been previously demonstrated that evar performed using a fluoroscopy c - arm resulted in an aver age patient radiation dose of about 6 msv , significantly lower than the doses obtained using a mobile angiography system ( about 64 msv ) or a fixed angiography system ( about 129 msv ) [ 46 ] , while the clinical outcomes were equivalent [ 6 ]  . after evar , patients require ongoing follow - up to ensure that the aneurysm remains excluded . 
concerns regarding the cumulative radiation 1 3 564 radiol med ( 2015 ) 120 : 563570 dose , contrast - induced nephropathy , the costs and increased demand for mdct angiography have led many groups to reconsider the necessity of mdct angiography for all evar patients [ 8 ] , the time scheduling of the mdct examinations [ 9 ] , to assess alternatives to mdct surveillance such as duplex ultrasound [ 10 ] or contrast - enhanced duplex ultrasound [ 11 ] or to explore the feasibility of reducing the effective dose associated with each mdct scan [ 12 , 13 ]  . despite these efforts , mdct still remains the current standard investigation for the follow - up of evar patients , although with follow - up regimes that are widely varied across different centres . previous estimates of radiation exposure to patients subjected to evar in the follow - up period were based on the generic protocols of the evar trials [ 1416 ]  . 
as such , these may be only regarded as first - order approximations of what happens in everyday clinical practice where the follow - up is increasingly tailored on an individual basis using many different diagnostic approaches . the aims of this retrospective observational study were to quantify the cumulative effective dose ( ced ) of ionising radiation in evar patients on an individual basis , to calculate the cumulated radiation dose to relevant organs , to assess radiation risks on an individual basis and to evaluate the clinical usefulness of mdct follow - up after evar . materials and methods data sources and study population we conducted a retrospective study of 147 patients who underwent evar in a university - based vascular surgery and interventional radiology centre between 15 july 2007 and 30 march 2011 . 
only 71 patients with a follow - up duration 1 year were included in the study . co - morbidities were obtained by reviewing medical notes , clinical summaries and patient interviews . 
details of radiological procedures related to evar and performed on patients in the cohort during the study period were obtained from the radiology information systefor mdct procedures the number of series , the length of coverage per each of the series , the anterior posterior and lateral dimension of the body part being scanned , the kv , pitch , average mas , volumetric dose index ( ctdivol ) and dose - length product ( dlp ) were obtained in each patient and in each anatomical region by the dose reports in the picture archiving and communication system ( pacs ) of the hospital radiology department . 
the data were censored at the date of the last examination recorded in the pacs after the evar procedure , to ensure a conservative estimate of the length of the follow - up . estimates of radiation doses for conventional diagnostic radiology procedures ( plain chest and abdominal / pelvic x - ray ) , we relied on the effective dose estimates summarised in a recent review [ 17 ]  . 
 the contribution of conventional diagnostic radiology was not taken into consideration for organ dose estimation and risk assessment purposes , since insufficient information was present in the databases regarding the characteristics of each exposure to allow reliable estimates of individual organ doses . for evar procedures radiation doses were measured by the dose area product ( dap ) in gy cm2 using inbuilt ionisation chambers , as described in a previous publication [ 6 ]  . 
 a backscatter factor of 1.38 was used to convert the dose in air estimated from the quotient of the dap and the area to a dose in tissue [ 18 ]  . 
imaging was posteroanterior : the distance between the anode and the patient was taken as 40 cthe effective dose and the organ doses were derived from the dap data by pcxmc 1.5 software [ stuk ( radiation and nuclear safety authority ) , helsinki , finland ]  . 
 these calculations assumed a tube voltage of 7080 kvp , depending on the radiological equipment used . size - specific dose estimates ( ssde ) in mdct were obtained by multiplying the ctdivol reported on the scanner by a correction factor ( fcorr ) based on the measured size of the patient and tabulated in the aapm report no . 
204 [ 19 ] specifically , the f corr was based on the effective diameter , defined as effective diameter apxlat , where ap is the anteriorposterior dimension and lat is the side - to - side dimension of the body part being scanned . mdct scans were all performed using a 64 - row mdct ( lightspeed vct , ge , milwaukee , wi , usa ) with 120 kv , 0.985 , helical scans and both z - axis and angular pitch tube current modulation . 
the calculation procedure was modified to consider the actual 1 3 radiol med ( 2015 ) 120 : 563570 distribution of organ dose consequent to the tube current modulation , as previously described [ 21 ]  . 
briefly , for every 1 cm thickness slab of the scanned volume , the tube current was recorded and inserted in an excel macro , that calculates the effective dose contribution of the slab and adds all the contributions to determine the total effective dose in the scanned volume . 
the accuracy of the ctdivol provided by the equipment user interface was verified by comparison with values measured during the routine quality controls , finding a maximum difference of 5 % . 
mdct angiography was counted as having multiple series within the scan to account for multiphase imaging [ 22 ]  . procedural frequencies and ced of radiation were calculated for the study population over the study period . 
 ced is expressed for each patient as a summation over the study period [ total ced ( msv ) ] including all radiological procedures and as annual ced ( msv per patient year )  . 
ct parameters used at follow - up were the same as those used for preliminary imaging . multidetector ct technique a thick - slice ( 35 mm ) unenhanced acquisition is performed to visualise the position of the stent - graft to reveal calcifications and to plan the following contrast - enhanced examination by selecting the acquisition volume and placing a region of interest in the aorta at the level of the coeliac trunk , using bolus tracking software . thin - slice ( 0.625 mm ) contrast - enhanced images in the arterial phase are obtained during the i.v. 
the cancer risks are non - zero only after a latency period ( 5 years for solid cancer and 2 years for leukaemia ) : these values are used in pcxmc software as a default . in pcxmc , lifetime risks are expressed in terms of risk of exposure - induced death ( reid )  . 
for practical purposes , at typical dose levels encountered in x - ray diagnostics , reid and lifetime attributable risks can be interpreted to present the excess radiation - induced cancer risk , and their numerical values are close enough to be interpreted as identical considering the uncertainties involved in the models . 
the user may also edit the organ doses without calculating doses with pcxmc : a radiation risk assessment can be made for arbitrary irradiation case . follow - up regime standard follow - up regime at our centre included ct angiography at 1 month , contrast - enhanced ultrasound ( ceus ) clinical assessment of mdct usefulness during evar follow - up the primary outcomes included the detection of abdominal aortic aneurysm expansion without endoleaks , thrombotic occlusion , endoleaks and device migration . 
they first reviewed arterial imaging alone and subsequently added noncontrast and delayed phases to determine the overall performance . they were asked to assess the presence / absence of thrombotic occlusion , endoleaks of type i , ii and iii and device migration . 
discrepancies were resolved by consensus . statistical analysis data were described using mean and standard deviation or median and intra - quartile range ( iqr ) for non - normal distributions . 
the k statistic was used to assess the interobserver reproducibility of the two independent readers overall , using the three phases and using the arterial 1 3 566 radiol med ( 2015 ) 120 : 563570 table 1 acquisitions parameters of the multidetector computed tomography ( mdct ) angiography examinations tube current scan time ( mas ) ctdivol ( mgy ) patient size ( cm ) unenhanced phase arterial phase venous phase 204 218 201 lat eff . 
1 cumulated doses to relevant organs due to multidetector computed tomogrpahy ( mdct ) angiography and interventional procedures in patients subjected to endovascular aortic aneurysm repair ( evar )  . 
 they comprised seven type i endoleaks treated by proximal stent - graft extension in four patients and with surgical explantation in one patient and one type iii endoleaks treated with unsuccessful surgical explantation . 
the remaining 54 endoleaks were of type ii with only one treated by percutaneous injection of thrombonly in 5 / 54 cases with type ii endoleak were the endoleaks only visible 1 3 table 4 results of ct follow - up after endovascular aortic aneurysm repair ( evar ) number of ct number of patients number of patients with reintervention 568 findings endoleaks type i type ii type iii device migration occlusive thrombosis in the venous phase of contrast - enhanced mdct . 
 this is likely because of underestimation in the previous studies of the contribution of mdct exposure : the mdct - related ceds were not estimated on an individual basis , but rather radiol med ( 2015 ) 120 : 563570 attributed according to a fixed protocol of mdct examination with a range from 5.4 to 22 msv , compared with a corresponding average of 58 msv per examination in our study . it must also be acknowledged that the dose received form a mdct scan is dependent on both patient size and scanner radiation output . 
in our patient population ssde was on average 1520 % higher than ctdivol ( table 1 ) and thus we are underestimating the radiation exposure of the subjects , with a conservative approach in estimating radiation doses and associated risks . doses of radiation from medical imaging procedures can be substantial in chronic or recurrent patients for whom the likelihood of repetitive studies is high . 
given their retrospective design , the majority of the studies included in this review used standardised procedure - specific mean effective radiation doses to calculate individual ced , instead of patientspecific dose information . 
to our knowledge , this is the first study aimed at estimating risks in evar patients using an individual estimation of organ doses . although prospective estimates of cancers and cancer deaths induced by medical radiation in a population of patients exposed to low dose ( < 100 msv ) should be considered speculative because of various random and systematic uncertainties embedded in them [ 29 ] , it must also be recognised that for evar patients we are fully in the range in which there is direct evidence of a statistically significant increase in the risk of cancer , and the corresponding related risks can thus be directly assessed from epidemiological data , without the need to extrapolate measured risk at lower doses . 
 however , evar procedures are performed to mitigate the risk of near - term and even life - threatening events , whereas the potential malignancy risk from radiation exposures is a long - term stochastic concern that can occur decades from exposure . 
nonetheless , it must be underlined that the reid variable already 1 3 radiol med ( 2015 ) 120 : 563570 takes into account the patients age , differently from risk projections based on the nominal coefficient of risk multiplied by the effective dose , which are averaged over all ages . an effective approach to reduce radiation exposure due to mdct is the reduction in the number of scans requested . 
while the percentage of mdct leading to notable findings such as detection of thrombosis , endoleaks or device migration was high , the utility of routinely performing a three - phase angiography mdct in the course of evar follow - up seems to be questionable . many researchers investigated the feasibility of modified protocols to reduce the radiation dose associated with the three - phase mdct [ 3033 ]  . 
indeed , in our study all the radiological findings leading to reintervention were visible in the contrast - enhanced arterial phase of the mdct examination and the endoleaks that were only visible in the venous phase were never associated with a change in patient management . 
thus , the unenhanced scan and the venous phase of the mdct angiography could have been omitted without compromising the utility of the examination in the course of evar follow - up . 
this would have led to a significant reduction of about 60 % of the associated mdct radiation exposure in a single patient . it must be acknowledged that newer ct radiation techniques for evar such as dual energy or low kv acquisitions [ 12 ] , as well as iterative reconstruction strategies [ 38 ] are on the horizon to reduce the burden of ct radiation doses . 
 [ 12 ] reported that a low - dose radiation exposure acquisition protocol provides substantially reduced radiation exposure while maintaining a constant contrast - to - noise ratio and good image quality . 
 the association of ceus in an alternating protocol with mdct during evar follow - up has been suggested as a useful means to reduce the radiation burden [ 39 , 40 ]  . besides ultrasound , other non ct - strategies like magnetic resonance imaging for evar follow - up have been studied as well [ 41 ] , although these are more a focus of ongoing research . these results should be interpreted in the context of some limitations . 
first and most important , the study was conducted in a single centre , while the use of radiation - related procedures is highly variable depending on both available technologies and clinical practices . 
second , the contribution of conventional diagnostic radiology to effective dose was derived from look - up tables in the existing literature and not estimated on a patients specific basis , while it was ignored in the estimation of organ dose and radiation risk . 
however , since the contribution of conventional diagnostic radiology to the ced is < 1 % , this underestimation is likely to be negligible . conclusions evar patients received high radiation doses in the course of radiological follow - up . 
the purpose of this study was to verify the presence of a possible correlation between pharmacological premedication and the percentage of hydrostatic reduction of intussusception in paediatric patients . materials and methods this study considered children with a diagnosis of idiopathic intussusception treated at our hospital between january 2007 and june 2013 . 
a second group of patients received pharmacological premedication with both a sedative and an anti - oedematous agent before the procedure . results a total of 398 patients were treated with barium enema for therapeutic purposes . 
daprano department of surgery , santobono childrens hospital , naples , italy premedication prior to barium enema ( n ( 85 % ) children achieved resolution of the intussusception . conclusions our study shows that the use of pharmacological premedication is effective for the reduction of the intussusception , as its limit patient stress , fluoroscopic time and radiation dose . 144 ) , 122 keywords hydrostatic reduction intussusception children sedation introduction intussusception is the most common form of intestinal obstruction in infancy and one of the most frequent causes of paediatric emergency [ 14 ]  . 
the most frequent type is the ileocolic form of intussusception ( 90 % of cases ) , usually idiopathic , caused by lymphoid hyperplasia of the terminal ileum ; the remaining 10 % , instead , are almost all ileo - ileal types . 
the ileo - ileal forms may be transient and asymptomatic , reducing spontaneously , or associated with the presence of a pathological lead point and therefore requiring surgery [ 5 , 6 ]  . 
the classic triad of intussusception symptoms ( abdominal pain , palpable mass and currant - jelly stool ) occurs in less than 50 % of cases [ 7 ]  . 
 ultrasound imaging is the most appropriate examination for the diagnosis of intussusception , with accuracy values near to 100 % [ 6 , 8 ]  . non - operative management for treatment , whenever possible , is the best choice although surgical treatment is indicated in the presence of complications or in the case of nonoperative treatment failure [ 911 ]  . 
currently , the standard 1 3 550 radiol med ( 2015 ) 120 : 549556 non - surgical treatment consists of enema ( air or liquid media ) [ 3 , 9 , 12 ]  . 
the non - surgical reduction of intussusception has many advantages , such as less invasiveness and morbidity , lower costs and shorter hospitalisation times , in addition to a reduction of surgical and anaesthetic risks [ 6 , 12 , 13 ]  . 
the non - surgical management of the patient with intussusception is still the subject of numerous studies aiming to identify procedures to increase the success rate of enema reduction and decrease its complications , such as transabdominal manually assisted reduction of intussusception [ 3 , 14 ] and the use of delayed and repeated reduction attempts [ 15 ]  . the role of the pharmacological premedication performed before hydrostatic reduction is still controversial [ 12 , 1618 ]  . 
the aim of this study was to verify the presence of a possible correlation between pharmacological premedication and the percentage of hydrostatic reductions of intussusception in paediatric patients . materials and methods this study analysed all children with a clinical suspicion ( abdominal pain , bilious vomiting , palpable sausageshaped mass along the course of the colon and rectorrhagia ) and imaging confirmation of ileo - colic , ileo ileo - colic or colo - colic intussusception observed at the our institute between january 2007 and june 2013 . all children initially underwent ultrasound examination to confirm or exclude the diagnosis of intussusception . 
 subsequently , plain abdominal radiography was performed to exclude a possible perforation . after an accurate clinical and radiological evaluation , all patients not showing signs of shock , peritonitis or perforation underwent hydrostatic reduction of the intussusception by barium enema . 
whenever possible , patients whose initial reduction was unsuccessful underwent an additional attempt at reduction ; however , for the purposes of this study , only the first attempt was analysed . all the childrens parents received information about the procedures and provided their consent . 
the study was approved by the local ethics committee . our study only included children with a diagnosis of idiopathic intussusception , and excluded those with surgical demonstration of intussusception secondary to the presence of pathological lead point . the two observed groups were homogeneous for age range , duration and type of symptoms , absence of a pathological lead point , degree of perfusion of the intussusception and absence of peritoneal signs . statistical analysis of the data was carried out using an online statistical calculator ( graphpad quickcalcs )  . 
during the 3 days of hospitalisation after the hydrostatic reduction none of the patients suffered any relapse . statistical analysis by chi - square test revealed a significant correlation between premedication and resolved intussusception ( table 1 )  . discussion intussusception is one of the most common causes of paediatric emergency [ 3 ]  . 
it is a strangulated obstruction leading to bowel ischaemia ; delay in diagnosis and treatment results in necrosis , perforation , peritonitis , shock and even death [ 2 , 11 , 23 , 24 ]  . 1 3 radiol med ( 2015 ) 120 : 549556 fig . 
the image refers to a patient included in the no - premedication group most cases are idiopathic ileocolic intussusceptions , without any identifiable cause ; in some cases , invagination is secondarily induced by an identifiable cause or under lying systemic disease . 
the most common pathological lead points include meckel diverticulum , duplication cyst , aberrant tissue , intestinal polyp , lymphoma and henoch schnlein purpura [ 46 ]  . ultrasound has nearly 100 % sensitivity and specificity in the diagnosis of intussusception [ 4 , 6 , 8 ]  . 
 the image refers to a patient included in the no - premedication group reduction , ultrasound - guided pneumatic fluoroscopyguided hydrostatic reduction , fluoroscopy - guided pneumatic reduction ( air enema ) and external manual reduction [ 13 , 9 , 11 , 12 , 16 , 25 , 26 ]  . 
these treatments avoid surgical and post - surgical risks , minimise invasiveness , shorten length of hospitalisation and save costs [ 6 , 12 , 13 , 27 ]  . 
barium has traditionally been used as a contrast mediu the advantages of the barium enema reduction technique are its clear delineation of the intussusception reducing process and the vast experience and familiarity with this contrast agent among radiologists ; however , it has the disadvantage of inducing chemical peritonitis in cases of bowel perforation [ 11 , 12 , 1 3 554 table 1 2 2 contingency table resolved intussusception persistent intussusception total non - premedicated group premedicated group 122 total chi square with yates correction chi squared equals 16.876 with 1 degrees of freedom the two - tailed p value is less than 0.0001 the association between rows ( groups ) and columns ( outcomes ) is considered to be extremely statistically significant 16 ]  . 
because of this risk , a water - soluble iodinated contrast medium is preferred to barium for hydrostatic reduction since it still allows appropriate anatomical delineation under fluoroscopy if diluted to iso - osmolar concentrations [ 16 ]  . 
however , recent data in the literature show that barium is still used for hydrostatic reduction , although its use is gradually decreasing [ 28 ]  . in 2007 , when we started our study , we decided to use barium as a contrast agent in the first group , and we have extensive experience , as well as equipment availability , in the use of barium , which we used until 2013 . 
in addition , we have been performing hydrostatic reduction procedures for over 15 years , so our paediatric radiologists level of skill in intussusception reduction can be considered the same in both the early and the later stages of our study . 
more recently , we also have replaced the barium with a water - soluble contrast medium in fluoroscopy - guided hydrostatic reduction . most of the children who came to our attention showed intermittent and crampy abdominal pain of varying severity , usually followed by refractory vomiting . 
by contrast , in frightened children , the increase in intra - abdominal pressure due to crying and agitated movements caused delayed progression of the barium column , thereby decreasing the success rate of hydrostatic reduction , extending the length of the procedure and increasing the radiation dose . 
the non - premedicated child may thus resist the procedure , which may consequently take longer to perform and require a higher radiation dose . these difficulties may in part be overcome using phar macological premedication . 
the use of the premedication radiol med ( 2015 ) 120 : 549556 and in particular the need for sedation in enema reduction of intussusception , although mentioned in the literature , is still controversial [ 3 , 12 , 13 , 1618 ]  . 
various kinds of sedation , such as diazepam [ 31 ] , chloral hydrate [ 32 ] , meperidine [ 18 , 25 , 33 ] , morphine [ 33 ] , propofol [ 17 ] and others have been customarily used . in our experience , we use a premedication protocol including both an anti - oedematous agent and a benzodiazepine . 
the role of this premedication is dual because it takes advantage of both the anti - oedematous and sedative effects . currently , in the literature there is no evidence of indications for the use of a corticosteroid in the non - surgical treatment of intussusception . 
the corticosteroid drug ( betamethasone ) , by reducing the wall oedema of the involved bowel loops , can decrease wall thickness and facilitate intussusception reduction under the effect of the hydrostatic pressure produced by the barium column . the mild sedative ( midazolam ) has calming , anxiolytic , muscle - relaxing and amnesic effects [ 35 ]  . 
this imidazolic benzodiazepine is widely used in paediatrics , orally or intravenously , for sedation during diagnostic and therapeutic procedures , with infrequent serious adverse effects [ 36 ]  . 
therefore , mild sedation has a calming effect that secondarily has the effect of limiting the increase in intra - abdominal pressure caused by crying . before the barium enema , we performed an additional ultrasound study since , as described in the literature , in the case of a small intussusception , the reduction in wall oedema combined with muscle relaxation can lead to a spontaneous reduction of the intussusception near the ileocecal valve [ 37 ]  . 
medications , such as muscle relaxants and sedation have been used [ 17 , 18 ] , even though there is little clinical evidence to support or condemn the use of sedation . 
sedation is generally not recommended in air enema because of the protective effect of the valsalva manoeuvre which decreases the transmural pressure and protects the colon against perforation [ 17 ] , although recent reports advocate its use [ 17 , 38 ]  . 
on the other hand , sedation is frequently used in hydrostatic reduction [ 25 ] , even though some authors have shown that the use of general anaesthesia does not contribute significantly to the success of hydrostatic reduction by barium enema [ 39 ]  . 
the disadvantages of deep sedation should also be considered ; these include an unpredictable response , even at standard doses , and the need for additional team of paediatric anaesthesiologists to 1 3 radiol med ( 2015 ) 120 : 549556 monitor the childs condition at all times during the procedure [ 12 ]  . 
as regards the use of glucagon in pharmacological premedication , it was shown that its administration does not provide any benefit to the intussusception reduction , so it has long been abandoned [ 40 ]  . 
although buscopan has been used in the past by some authors as an antispasmodic agent [ 41 ] , we consider that it has the unfavourable effect of reducing physiological bowel peristalsis . contrary to all the discordant evidence , our series demonstrates the effectiveness of pharmacological premedication based on the use of a mild sedative and an anti - oedematous agent . 
we had a significant increase in the rate of successful resolutions of intussusception without the disadvantages described above , and we saw none of the rare adverse effects of midazolam , such as respiratory depression , hypotension , nausea and vomiting . 
moreover , sedation is extremely useful during the performance of fluoroscopy - guided hydrostatic reduction with barium enema since it reduces the patients stress and pain and consequently the parents distress , thereby facilitating the procedure , reducing fluoroscopy time and decreasing the radiation dose . the limitation of this study relates to its retrospective nature . 
furthermore , the two comparison groups are homogeneous in terms of age , onset and duration of symptoms and type of hydrostatic reduction procedure , even though they belong to different periods . 
despite the limitation , the promising results of our study may be the starting point for a randomised controlled trial ( rct )  . conclusion our study shows that the use of pharmacological premedication is effective for the hydrostatic reduction of intussusception , as it limits the stress felt by the patient , and reduces fluoroscopy time and radiation dose . in our results , the rate of successful resolution of intussusception was significantly higher in the premedicated group compared to the controls , confirming the effectiveness of the premedication . 
histolog ical assessment was conducted and gd content of the skin , liver , kidneys , lungs , heart , spleen , diaphragm , and femoral muscle was measured by inductively coupled plasma mass spectrometry ( icp - ms ) at 7 days after last injection . 
nishimura department of pathology , kawasaki medical school , 577 matsushima , kurashiki , okayama 701 - 0192 , japan spleen , liver , lungs , skin , heart , diaphragm , and femoral muscle . 
histopathological investigation revealed hepatic fibrosis in the hepatorenally impaired group . conclusions compared with renally impaired rats , tissue gd deposition in hepatorenally impaired rats exposed to gd - eob - dtpa was significantly increased in the kidneys , spleen , and liver , probably due to the impairment of the dual excretion pathways of the urinary and biliary systems . keywords nephrogenic systemic fibrosis ( nsf ) gd - eob - dtpa gadolinium ( gd ) - based contrast agents ( gbcas ) hepatorenally impaired rats inductively coupled plasma mass spectrometry ( icp - ms ) introduction the concept of nephrogenic systemic fibrosis ( nsf ) is widely known to general physicians today . 
most cases of nsf following intravenous gbca injection occur in patients with end - stage renal disease ( especially in those undergoing dialysis ) , those with additional preinflammatory conditions , those who have undergone vascular surgery , and following liver transplantation [ 114 ]  . 
discovery of an association between nsf and gadolinium - based contrast agents ( gbcas ) , especially at high doses [ 12 ] , has led to hypotheses that gbca could trigger this condition . 
gadolinium ethoxybenzyl diethylenetriamine pentaacetic acid ( gd - eob - dtpa ) is a liverspecific magnetic resonance imaging ( mri ) contrast agent in which approximately half of the administered dose is 1 3 558 radiol med ( 2015 ) 120 : 557562 taken up by liver cells and excreted in the bile because of the addition of an ethoxybenzyl group ( eob group ; a lipophilic side chain ) to the conventional extracellular contrast agent gd - dtpa ( gadopentetic acid )  . 
this agent enables assessment of blood flow in early dynamic phase and evaluation of hepatocyte function in the delayed hepatobiliary phase . according to guidelines released by the european medicines agency , the various commercially available contrast agents have different risks of triggering nsf . 
the committee for medicinal products for human use ( chmp ) scientific advisory group ( sag ) for diagnostics categorised gbcas into three groups of nsf risk based on the thermodynamic and kinetic properties of each agent . 
in a previous basic investigation on nsf using 5 / 6 - nephrectomized rats , tissue gd deposition was lower in rats administered gd - eob - dtpa than in those administered other gd preparations . 
although the dose of gd - eob - dtpa was small in this previous study , the reason for this finding is thought to be because gd - eob - dtpa has the unique property of having two excretion pathways : the biliary system and the urinary system . in the state of hepatorenal impairment , it is expected that tissue gd deposition increases after gd - eob - dtpa exposure , and the risk of nsf onset is also thought to increase . 
therefore , the aims of the present study were to conduct quantitative analysis of tissue gd deposition following gd - eob - dtpa exposure in hepatorenally impaired rat models using inductively coupled plasma mass spectrometry ( icp - ms ) as well as the histopathological findings , and to compare with renally impaired rat models in the differences of the distribution of gd in major organs and tissues . materials and methods all animal experimental procedures complied with national legal requirements and internal regulatory and ethical guidelines . animals a mixture of carbon tetrachloride ( ccl4 ) and olive oil ( 3 ml / kg at a ratio of 1 : 1 , twice - weekly , from 7 weeks of age )  . ccl4 has hepatic toxicity that causes both hepatic cirrhosis and hepatocellular carcinoma in experimental animals . 
rats were provided ad libitum access to standard food and water . contrast agent administration the mri contrast agent used in this study was gd - eobdtpa , which is an approved and marketed product . 
the regular test dosage of gd - eob - dtpa for humans is 0.1 ml / kg 0.025 mmol / kg ; in the present study , however , the hepatorenally impaired rats received repeated 0.625 mmol / kg via intravenous injections of 2.5 ml / kg the tail vealthough the dosage of gd used in this study was higher than that applied clinically , injection doses of gd - eob - dtpa were determined with reference to animal experiment set - ups reported previously by pietsch et al . 
gd - eob - dtpa injection dose was set at one quarter of the dose of other gbcas [ 15 ] because the clinical dose of gd to the human body with gd - eob - dtpa is quarter of the dose with other gbcas . 
by removal of 2 / 3 of one kidney at 5 weeks of age and complete removal of the other kidney at 6 weeks of age ( 5 / 6 - nephrectomized rats )  . 
as a type of elemental 1 3 radiol med ( 2015 ) 120 : 557562 analyser , icp - ms is a mass spectrometer that uses inductively coupled plasma ( icp ; discharge plasma produced by applying high - frequency energy to argon gas at atmospheric pressure ) as the ionisation source . 
the characteristics of icp - ms are its ability to analyse numerous elements , its low detection limit because of its high sensitivity , the large linear region of the calibration curve , and its ability to analyse multiple elements simultaneously and perform rapid qualitative and semi - quantitative analysis . in preparing the measurement solution , the provided sample is weighed in a quartz beaker and then separated by adding nitric acid and heating . 
all pretreatment and measurement of samples was done in a clean room . heart , lungs , liver , kidneys , spleen , diaphragm , and femoral muscle were examined for grossly visible changes . 
after formalin fixation , samples were embedded in paraffin wax , sectioned at a nominal thickness of 5 m , stained with haematoxylin and eosin ( he ) and massons trichrome stain , and examined under light microscopy . 
he staining and massons trichrome staining of all specimens were performed 7 days after the last injection of contrast agent . statistical evaluation the nonparametric mannwhitney u test was used to determine significant differences in gd content between hepatorenally impaired rats and renally impaired rats for gadolinium measurements taken from the skin , kidneys , liver , heart , spleen , lungs , diaphragm , and femoral muscle . 
statistical analyses were performed using spss software ( spss , chicago , il )  . results gross and microscopic pathology gross and microscopic findings , histopathology animals were examined for macroscopic skin changes such as reddening , fur loss , scab formation , and ulceration prior to every injection . 
1 microscopic liver findings in renally impaired rats ( a , c ) and hepatorenally impaired rats ( b , d ) following final administration of gd - eob - dtpa [ a , b toxylin and eosin ( he ) stain , and c , d stain ]  . 
massons trichrome is the most useful stain for differentiating collagen from other fibres , producing red keratin and muscle fibres , blue or green collagen and bone , light red or pink cytoplasm , and dark brown to black cell nuclei . 
in the hepatorenally impaired group , gd was predominantly deposited in the kidneys , followed in descending order by the spleen , liver , lungs , skin , heart , diaphragm , and femoral muscle . discussion we used an animal model with hepatorenally impaired rats that were 5 / 6 - nephrectomised and had ccl4 - induced liver fibrosis , which was chosen because a previous study showed that this condition causes similar serum exposure to gadolinium as that in patients with severe renal impairment , and is an appropriate model for evaluating the potential role of a prolonged circulation time of gbcas in terms of gd accumulation [ 15 ]  . 
additionally , it is because the most validated cirrhosis model in the rat is the ccl4 cirrhosis model [ 16 ]  . gbcas used for mri contain the paramagnetic gd3 ion tightly bound by a complexing agent and are generally well tolerated [ 1719 ]  . 
numerous studies reported that the risk of nsf is higher for less stable , linear , and non - ionic gbcas [ 2224 ]  . gd - eob - dtpa is a hepatobiliary contrast agent with an ionic linear , open - chain structure . 
the various authorities and societies of europe and america have performed expert evaluations on the risk of gbcas , with classification into highand low - risk groups in terms of nsf development . 
for gd - eob - dtpa ( primovist or eovist ) , the european risk classification is intermediate because it has an ionic linear structure . icp - ms analysis in the present study using gd - eobdtpa revealed tissue gd deposition in multiple organs of the hepatorenally impaired rats , in descending order , as follows : kidneys , spleen , liver , lungs , skin , heart , diaphragm , and femoral muscle . 
it has been suggested that in excretion of gd - eob - dtpa , urinary and 1 3 radiol med ( 2015 ) 120 : 557562 biliary system excretion mechanisms have compensatory functions [ 28 ]  . 
however , our results showed that the dual excretion mechanisms in hepatorenally impaired rats were not able to function in this compensatory manner and tissue gd deposition increased . tissue gd deposition after gd - eob - dtpa exposure in hepatorenally impaired rats was higher than that in renally impaired rats in this study , but was still similar to that after the exposure of gd - hp - do3a ( prohance ) with stable macrocyclic structure in renally impaired rats in the previous studies [ 29 ]  . 
therefore , the use of gd - eobdtpa in patients with both hepatic impairment ( cirrhosis ) and renal function impairment needs to be carefully considered . there are several limitations in our study . 
second , icp - ms cannot distinguish between chelated and unchelated gd , based on the available data [ 21 , 3032 ] , and high levels of long - term deposition could indicate high gd ion release from the complex in vivo . 
the use of gd - eob - dtpa should be approached with caution in hepatorenally impaired patients because of impairment of the dual excretion pathways of the urinary and biliary systems . conflict of interest none of the authors have any conflicts of inter est associated with this study . 
the integration with angiographic methods [ postmortem computed tomography angiography and multiphase postmortem ct angiography ( mpmcta ) ] allows the examination of the cardiovascular system and it is increasingly being utilised in the field of forensic pathology . 
however , using the standardised procedure that establishes the femoral vessels on one side of the corpse as an access point to the vascular system , visualisation of the vascular tree below the cannula insertion site is excluded . 
consequently , visualisation of the vascular anatomy and morphology of the lower limbs is impossible and lesions such as thrombosis of the superficial and deep venous system may remain elusive . 
guglielmi department of radiology , scientific institute casa sollievo della sofferenza hospital , viale cappuccini 1 , 71013 san giovanni rotondo , foggia , italy bearing in mind the high incidence of pulmonary thromboembolism in forensic case studies and the difficulties in postmortem diagnosis , we propose a new axillary approach for mpmcta that allows the full detection of the vascular system of the lower limbs . keywords postmortem ct angiography axillary approach pulmonary thromboembolism deep venous thrombosis sudden unexplained death introduction postmortem computed tomography ( pmct ) is widely used in the forensic pathology setting as supplementing medicolegal investigations and being capable of providing significant data that affect final conclusions and adding new quality to recording postmortem observations . 
the integration with angiographic methods [ postmortem computed tomography angiography , pmcta and multiphase postmortem ct angiography ( mpmcta ) ] allows the examination of the cardiovascular system and it is increasingly being utilised in the field of forensic pathology [ 1 ]  . 
many methods to perform postmortem angiography exist [ 26 ] ; the approach proposed by the technical working group postmortem angiography methods ( twgpam ) is one of the most used [ 5 ]  . 
however , using the standardised procedure that establishes the femoral vessels on one side of the corpse as an access point to the vascular system [ 7 , 8 ] , visualisation of the vascular tree below the cannula insertion site is excluded and lesions such as thrombosis of the superficial and deep venous system may remain elusive . 
 bearing in mind the high incidence of pulmonary thromboembolism ( tep ) in forensic case studies and the difficulties in postmortem diagnosis , we propose a new axillary 1 3 radiol med ( 2015 ) 120 : 670673 fig . 
the first incision , no more than 5 cm long , is made along the upper third of the anterior axillary line , in correspondence with the anterior axillary fold ( anterior wall of the axilla - lower border of the pectoralis major muscle and the underlying pectoralis minor muscle )  . 
a second incision , with a maximum length of 5 cm , is made from the anterior axillary fold ( first cut ) along the medial side of the arm ( lateral wall of the axilla )  . 
the anterior surface of the axillary sheath is opened with the use of scissors followed by the blunt dissection of the brachial artery , brachial vein , median and lateral roots of the medial and lateral cords and the median and ulnar nerves . 
following the course of the brachial artery and vein , the cannulas are inserted in the so - called third part of the axillary artery ( for the arterial system ) and into the underlying axillary vein ( through to the axillary sheath )  . 
the axillary dissection almost disappears when the arm is completely adducted conclusions mpmcta is an easily applicable technique that consists of the acquisition of one native scan and three different phases of angiography : an arterial phase , a venous phase and a dynamic phase [ 5 ]  . 
with this technique , most cardiovascular pathologies can be diagnosed because the native scan and the following injection of the contrast agent and a minimum of three angiographic phases provide high diagnostic sensitivity similar to clinical ct angiography [ 5 ]  . 
however , techniquerelated artefacts and pitfalls exist and have been recently reviewed [ 9 ]  . a key question is represented by the fact that in the protocol adopted by the twgpam the venous system of the arms and legs is not specifically investigated , and legs are omitted from the protocol [ 5 ]  . 
2 the venous phase reveals the luminal filling defect of the left pulmonary artery ( a ) ; in b the axial sections represent the superior and inferior slices to the blue point , on the right the longitudinal sections are presented fig . 
pte is therefore an important disease in the forensic investigation of the cause of death [ 11 ]  . second , it may be a matter of considerable medico - legal importance to know if a pulmonary embolus arose prior 1 3 radiol med ( 2015 ) 120 : 670673 to , or subsequent to , some traumatic event . 
it is well known that the majority of emboli have been shown to originate in the veins of the legs , frequently at the level of the femoral and iliac veins , but other sources in the legs are difficult to identify also at autopsy because dissection of the veins behind the knees , calves and soles of the feet is not routinely done after death [ 10 , 14 ]  . 
in some specific but not infrequent situations ( e.g. , when the affected vessels are of small calibre or are located in poorly accessible anatomical areas of the body such as in distal thrombosis ) , identifying the exact location of the thrombus can be timeconsuming , difficult , and unsuccessful . 
further limitations and difficulties may be represented by obesity , and patients with lower extremity oedema . imaging through multiphase postmortem ct angiography can be very helpful since reliable recognition of a filling defect or inhomogeneous opacification allows the visual inspection of the exact site of the suspected venous thrombus . 
this makes it possible and easier for the forensic pathologist to check the correct site in the venous system of the lower extremities and identify the venous thrombus for subsequent histological examination . in conclusion , mpmcta is a very useful tool to investigate the vascular system with satisfactory results . 
however , through the traditional femoral approach visualisation of the vascular system of the lower extremities is impossible , reducing the detection of deep venous thrombosis . based on these observations , we suggest modifying the site of vascular cannulation for mpmcta and using the axillary approach in all the cases with risk factors for venous thromboembolism or in cases of sudden unexplained death to enhance the quality of postmortem investigations . 
a region of interest ( roi ) was used to calculate signal - to - noise ratio ( snr ) and contrast - to - noise ratio normalised to dose ( cnrd )  . 
deak ge healthcare , solingen , germany keywords computed tomography ground - glass nodules iterative reconstruction radiation exposure dose introduction the use of computed tomography ( ct ) has increased rapidly worldwide in the last few decades , and it has been estimated that more than 62 million ct scans per year are currently performed in the usa [ 1 ]  . 
in this field , the use of ct is still controversial [ 7 ] , even though 1 3 612 radiol med ( 2015 ) 120 : 611617 the national lung cancer screening trial ( nlst ) has recently demonstrated that screening of high - risk populations with the use of low - dose ct considerably reduces mortality from lung cancer [ 8 ]  . one of the main advances in knowledge associated with ct screening programmes is related to the detection , management and characterisation of ground - glass nodules ( ggn ) [ 9 , 10 ]  . 
 [ 11 ] reported that ggns have a higher malignancy rate than lung solid nodules in high - risk subjects . since however , while the detection of solid nodules is made possible by the inherent high contrast of the lung , the detection of ggn may be affected by the reduction of radiation dose as a result of the increased image noise [ 12 ]  . the conventional reconstruction method , filtered back projection ( fbp ) , is unable to consistently generate diagnostic quality images with reduced tube current - time products ( mas ) , new methods for noise reduction based on iterative reconstruction ( ir ) algorithms have been developed to preserve ct diagnostic capability at reduced doses [ 13 , 14 ]  . 
eventually , a total of 54 samples had the required characteristics and were selected as ggn simulated nodules for this study . anthropomorphic phantom and ct data acquisition the 54 artificial ggn were arbitrary divided into three groups comprising 20 , 18 and 16 nodules each , regardless of nodule size . 
the readers were previously informed about the purpose of the study but were blinded to the dose level ( standard dose , low dose or ultra - low dose ) and the image reconstruction technique ( fbp or mbir ) of each ct scan , as well as to the number , position and characteristics of ggns for each phantom configuration . 
to minimise recall bias , each reading session was separated by a 2 - week interval and the images presented to each reader in a random order . ggn side , ct scan number and diameter were reported for each nodule . 
the maximum transverse axial nodule diameter was measured with an electronic calliper at lung window using a fixed window setting ( ww 1 , 260 , wl 480 )  . image quality analysis the phantom configuration with 18 nodules was arbitrarily chosen for image quality analysis . 
contrast - to - noise ratio normalised to dose ( cnrd ) was derived from the ratio of cnr and the square root of ct dose index volume ( ctdivol )  . the estimated ctdivol and dose - length product ( dlp ) were recorded for each image data set according to the final dose report . 
the sensitivity ( se ) and 95 % conand uld fidence intervals ( ci ) of each protocol in the detection of ggns was calculated both within each phantom and considering all the 54 nodules in the three phantom configurations . 
the analyses were performed using sas software , version 9.2. results image interpretation the three readers sensitivity for ggn detection according to the different protocols is reported in table 1 for the 54 nodules . 
the snr and cnrd relative differences increase by lowering the delivered dose ( table 2 )  . tube current product , ctdivol , dose - length product ( dlp ) and effective dose ( e ) for standard dose , low dose and ultra - low dose are shown in table 3 . 
in particular , the low contrast between ggn and lung parenchyma is problematic with low - dose ct , as image noise increases with the reduction of dose . the model - based reconstruction method iterative ( mbir ) is a powerful tool to overcome the problem of image noise at low radiation dose , which consistently yields increased snr and cnrd ( table 2 )  . 
3 a the standard - dose ct scan with filtered back projection ( fbp ) reconstruction ( reference standard ) shows a small artificial ground - glass nodule ( ggn ) in the left lung of the anthropomorphic phantom ( black arrow )  . 
b the same small artificial ggn ( black arrow ) is shown at ultra - low - dose ct scan with model - based iterative reconstruction ( mbir ) cnrd . 
similar results have also been reported for nodule volume accuracy with different iterative reconstruction algorithms [ 23 ]  . our results have shown that the use of ultra - low - dose ct if combined with the mbir technique can achieve the same ggn detectability as the conventional standard dose . 
the effective dose of ultra - low dose is comparable to the average effective dose delivered with a postero - anterior and lateral chest x - ray that is about 0.1 msv ( range 0.050.24 msv ) [ 24 ]  . the influence of mbir on the detection of ground - glass opacity is still uncertaour data for sensitivity are similar to those in a previous study that assessed pulmonary nodule detection with mbir [ 25 ] even if in that study , the authors did not report the specific sensitivity in the detection of fig . 
4 blandaltman plots of differences between average ggn size measurements taken with standard - dose fbp ( reference standard ) and ( a ) low - dose fbp , ( b ) low - dose mbir , ( c ) ultra - low - dose fbp , and ( d ) ultra - low - dose mbir against the mean of the two measurements . 
the readers high sensitivity could also be related to the 0.625mm slice thickness that we used for reading , which probably improved nodule detection . moreover , we should consider that the phantom had a fixed size , but patients have different body habitus : this could influence the results , particularly for large patients and low doses . 
further in vivo studies are therefore needed to confirm our results obtained in a phantom . another limitation is represented by the lack of comparison between mbir and the previous released adaptive statistical iterative reconstruction algorithm ( asir )  . 
a previous study [ 17 ] found no significant differences in ggn ( n 18 ) detection between the low - dose asir and the ultra - low - dose mbir . 
on the other hand , it has been suggested that in low - dose ct , a significant improvement in image noise and streak artefacts is associated with the use of mbir compared with asir [ 29 ]  . 
furthermore , a recent lowdose study [ 30 ] aimed to assess the effect of iterative reconstruction in the volumetric analysis of lung nodules reported a significant improvement in the accuracy of lung nodule volumetry compared with fbp , particularly for ground - glass nodules . one of the current disadvantages of the mbir technique is the long reconstruction time that limits its clinical application to specific fields , such as lung cancer screening . 
wichmann received : 10 september 2014 / accepted : 18 november 2014 / published online : 3 february 2015 italian society of medical radiology 2015 abstract purpose this study was done to investigate the dynamic changes of the aortic root during systole and diastole in patients with coronary artery calcification ( cac ) using dual - source computed tomography ( dsct )  . materials and methods we retrospectively analysed 77 consecutive patients who underwent calcium - scoring and angiographic cardiac dsct . 
the longand short - axis dimensions , axis areas of the aortic annulus , sinotubular junction and ascending aorta at the level of the pulmonary trunk in diastole and systole were measured . 
the presence of severe cac significantly influences the flexibility of the wall of the ascending aorta . keywords aortic root cardiac anatomy coronary artery disease cardiac ct computed tomography introduction the aortic root is defined as an anatomical entity consisting of the aortic valve leaflets and attachments , the interleaflet trigones , the sinuses of valsalva , the sinotubular junction , and the aortic annulus . 
thus , evaluation of structural changes of the aortic root is crucial for preoperative assessment prior to cardiovascular surgery [ 35 ]  . prior studies have reported controversial results regarding the dynamic changes of the aortic root during the cardiac cycle . 
another study demonstrated differences in the dimensions of the aortic annulus in patients with severe aortic stenosis [ 10 ]  . coronary artery calcification ( cac ) is a marker of coronary artery atherosclerotic burden and correlates with systemic vascular disease [ 11 ]  . 
to the best of our knowledge , so far no studies have evaluated the dynamic changes of the aortic root during the cardiac cycle in patients with cac in comparison with patients without cac . 
the potential of ct to detect changes of the aortic root in patients with cac is unknown . thus , the purpose of this study was to investigate the dynamic changes of the aortic root during systole and diastole in patients with cac using dual - source ct ( dsct ) and to assess whether the presence of cac has an impact on the aortic root . materials and methods study population this retrospective study was approved by the institutional review board with a waiver for informed patient consent . 
 both the unenhanced coronary calcium scan and contrastenhanced cardiac ct images obtained during dual - source coronary ct angiography ( ccta ) from consecutive patients referred for ccta at our institution were analysed . 
a prospective electrocardiogram ( ecg ) - gated dose - saving technique with a fixed tube voltage of 120 kv and a reference tube current output of 80 mas were used . 
automated tube current modulation and pulsing - window adaptation ( care dose 4d ) were activated to reduce radiation exposure . all calcium - scoring scan series were reviewed on a commercially available workstation ( syngo mmwp , siemens healthcare ) using the dedicated calcium - scoring application . 
 a nonionic contrast medium ( iomeprol ; imeron 400 , bracco imaging , konstanz , germany ) with a concentration of 400 mg / ml was administered at 5 ml / s through an antecubital vein of the right ar the total amount of contrast volume was calculated depending on the patients body weight ( 1 ml / kg )  . 
the average diameter of the aortic annulus was determined using the formula : ( short axis dimension + long axis dimension ) / 2 the relative areal change ( %ra ) was calculated using the following formula : %ra = 100 ( as ad ) / ad where as refers to the biggest value of the area in diastole and systole , while ad refers to the smallest value [ 1214 ]  . the best diastolic and systolic phase images were then analysed in the cine application on the same workstation . 
 the endocardial and epicardial borders of the left ventricle were traced automatically on shortand long - axis images , but necessary manual adjustments were performed by the same observer if necessary . 
the dataset is then scrolled through until the most caudal attachments of the aortic valve are identified ( d ) .the nadirs of all three cusps have been identified on the transverse image , ensuring the appropriate plane for assessment of the aortic annulus . 
values of p < 0.05 indicated a statistically significant difference . a total of 77 subjects ( 56 males and 21 females ) with a mean age of 64 12 years ( range 4088 years ) were enrolled in this study . 
from the sub - group analysis between patients with and without cac ( table 1 ) , no significant differences regarding age , gender , thoracic diameters , stroke volume , ejection fraction , or heart rate were observed between the two groups . 1 3 598 radiol med ( 2015 ) 120 : 595602 fig . 
in patients without cac , no dynamic changes were observed regarding the dimensions of the aortic annulus and areas of both aortic annulus and sinotubular junction ( table 2 )  . there were no significant differences in systolic and diastolic dimensions and areas of the aortic annulus and the sinotubular junction between patients with cac and 1 3 radiol med ( 2015 ) 120 : 595602 fig . 
the ra % of the ascending aorta at the level of the pulmonary trunk showed no significant differences between patients with and without cac , but patients with severe cac demonstrated a significantly smaller ra % of the ascending aorta compared to patients with minimal - to - moderate cac . contrary findings have been reported regarding the dynamic changes of the aortic annulus and the sinotubular junction during the cardiac circle [ 9 , 10 ]  . 
in our study , we evaluated the double oblique imaging plane for exact alignment with the aortic annulus as it has shown high interand intraobserver agreement [ 15 ]  . 
we assessed the ra % as an indicator of vessel elasticity [ 13 ] , since elasticity is influenced by manifestation of adverse functional changes within the vessel wall [ 17 ]  . 
this may be explained by the fact that less elastic tissue is present in that segment of the vascular wall [ 8 ]  . a previous study reported that the mean diameter of the sinotubular junction enlarges with increasing age , but the aortic annulus diameter shows better correlation with body surface area compared to age , especially in a younger population [ 20 ]  . 
 several prior studies have shown that left ventricular function assessed by cardiac ct shows good reproducibility and correlation compared to two - dimensional transthoracic echocardiography and magnetic resonance imaging [ 2123 ]  . this study had some limitations , mainly due to its retrospective study design evaluating a relatively small number 1 3 602 radiol med ( 2015 ) 120 : 595602 of patients . 
moreover , lipid or glucose serum levels , current or prior tobacco and alcohol consumption , and drug use were not evaluated as such data could not be obtained from the electronic medical chart system for all patients . 
in addition , aortic and aortic root calcification was not evaluated . in conclusion , longand short - axis dimensions of the aortic annulus and area of the sinotubular junction show significant changes during systole and diastole in patients with cac . 
the presence of severe cac results in a restriction of the flexibility of the wall of the ascending aorta measured by a reduced %ra , indicating a complex vascular pathophysiological cascade in patients with extensive cac . 
although additional studies are necessary to evaluate the long - term clinical outcome of these findings , these initial results indicate that severe cac may also be a potential indicator of extracardiac vascular disease , potentially further influencing patient outcome [ 2 ]  . conflict of interest and source of funding no funding was received . 
some individuals had been buried inside the church ( privileged subjects ) , others outside in the parvis ( members of rural population ) , and others still to the north of the church . 
faletti radiodiagnostic unit of cto / maria adelaide , department of diagnostic imaging and radiotherapy , azienda ospedaliera citt della salute e della scienza di torino , corso bramante 88 , 10126 turin , italy e - mail : a.borre@libero.it femurs of 27 male and 28 female individuals to determine any associations between cortical index , bone mineral density ( bmd ) , gender , age and social status . results no statistically significant differences were observed in cortical index values according to gender , age or place of burial . 
more dietary calcium intake , more sun exposure and vigorous physical activity , compared to that of the privileged individuals . keywords x - ray computed tomography dxa cortical index bmd italian medieval population bone loss osteoporosis r . 
panattoni department of neuroscience , rita levi montalcini , university of torino , corso massimo dazeglio 52 , 10126 turin , italy osteoporosis is an increasingly important issue in todays society and a major public health problem afflicting western populations , especially postmenopausal women once oestrogen secretion falls . 
the multifactorial issues associated with modern life are also known to take a toll , such as sedentary lifestyle , low calcium intake and vitamin d deficiency [ 1 ]  . 
the study of osteoporosis incidence in subjects with different lifestyles is today useful to provide information on the role of socio - economic status , environmental conditions , bio - cultural context and genetics play in influencing bone loss . 1 3 radiol med ( 2015 ) 120 : 674682 with this aim in mind , a study on osteoporosis on ancient populations , who led very different lifestyles , was carried out to determine if this is a new or old pathological condition . 
a number of paleopathological studies have been performed on skeletons excavated from archaeological sites and demonstrated that osteoporosis is not simply an issue of modern lifestyle , but was also present in ancient human populations [ 211 ]  . the literature on ancient or modern individuals which evaluated cortical bone thickness using diagnostic techniques , like bones and sites , has reported differences between gender and age [ 9 , 1217 ] and that cortical thickness directly correlates with bone strength and fracture risk [ 15 , 1820 ]  . 
mechanical stress is also important in bone modelling and various activities , such as weightbearing exercises , may enhance cortical femur strength [ 15 , 20 , 21 ]  . dual - energy x - ray absorptiometry ( dxa ) is now a well - established method routinely used to measure bone mineral density ( bmd ) and an accurate method for the clinical diagnosis of osteoporosis in modern populations . 
 the last two decades have witnessed an ongoing trend in research on dxa as the elective method to assess ageand gender - related changes in bone mineral density in archaeological populations . 
moreover , as dxa is a noninvasive , nondestructive method to assess osteopoenia and osteoporosis , it does not damage or destroy ancient bones [ 22 , 23 ] and is the current technique of choice to monitor bmd in clinical practice , facilitating comparisons between ancient and modern individuals . 
the best sites for dxa scanning are the trabecular bone of the proximal femur and the vertebral body . however , there is ongoing controversy as to there being a strong correlation between cortical thickness , osteoporotic bone loss and different lifestyle factors of ancient and modern populations [ 9 , 16 , 24 ]  . the aim of this study was to investigate whether the population differences in osteoporosis observed nowadays are a reflection of the times and modern lifestyle factors , or whether they were also present in the past . 
the gender and age - at - death of all individuals were estimated by standard anthropological methods [ 26 ]  . the analyses of the spatial organisation and the typology of the burials and graves indicated that there were different social groups [ 25 ] , as follows : 1 . 
the custom of burying members of the clergy and privileged families inside churches has been documented as from the early middle ages and the archaeological evidence from trino vercellese indicates that there is no reason to doubt the presence of noble families inside san micheles church ; 2 . 
during the medieval period , this burial area was dedicated 1 3 676 radiol med ( 2015 ) 120 : 674682 to a plebeian cemetery : in the case of san michele , this space was dedicated to rural population burials ; 3 . 
the north group : 99 skeletons buried outside the church , in an area located to the north of the building ; these burials were not very close to the church and may accommodate different groups , such as military personnel or servants , and were most likely not dedicated to the local population . all the materials included in the study were dependent on its state of preservation . 
a radiological study was performed in two planes ( frontal and lateral ) with a remote - controlled system ( opera gmm , seriate ( bg ) , italy )  . 
the femurs were 43 cm cr plate ip cassette , positioned directly on a 35 fcr fujifilm , tokyo japan , at 150 cm focus - film distance ( ffd )  . 
all the x - ray and ct images were stored in the picture archiving and communications system ( pacs ) within the radiodiagnostic unit of the cto / maria adelaide ( azienda ospedaliera universitaria citt della salute e della scienza di torino )  . 
4 axial computed tomography ( ct ) scan of a femoral midshaft the total width ( tw ) and the medullar width ( mw ) were measured perpendicular to the line passing through the linea aspera were taken with fixed visualisation parameters on the pacs - stored images . 
the linea aspera was identified in the axial ct scan and considered the most posterior point : the total width and the medullar width were measured 1 3 radiol med ( 2015 ) 120 : 674682 perpendicular to the line passing through the linea aspera . 
5 dual - energy x - ray absorptiometry ( dxa ) scan of a femoral neck with the bone mineral density ( bmd ) measurement 1 3 678 radiol med ( 2015 ) 120 : 674682 categorical variables . 
 as sensitivity analysis , missing data were imputed using bootstrap method . similarly to the analysis of individual characteristic effects on the cortical index , a multivariable linear regression model was used , reporting crude and adjusted marginal effects for each variable to investigate into any association between bmd , gender , age and burial place . statistical analyses were performed by stata 11.2 ( statacorp lp , college station , tx , usa )  . results the characteristics of the individuals are described in table 1 . information on the cortical index was available in 38 skeletons ( 17 males and 21 females )  . 
there were no statistically significant differences in x - ray or ct cortical indexes according to individual characteristics : as shown in table 2 , there were no variations in the averages according to gender , age or burial place . 
incidental findings were observed in six of the femur x - rays and ct scans : one small round radiolucent lesion of the neck and five calcified areas inside the medullary canal . dxa studies were performed on 21 lumbar spines and 15 proximal femurs from males ( seven showed both lumbar spine and femurs ) and 19 lumbar spines and 21 proximal femurs from females ( nine showed both lumbar spine and femurs )  . 
when both observed bmd ( table 3 ) and estimated bmd ( table 4 ) were taken into consideration , there was a statistically significant difference according to burial place , i.e. 
 as most of the female skeletons examined were of young adults and only 4 / 55 were of women over 50 years of age , we may reasonably assume that the population was homogenous for sex hormonal status . large bones , such as the femur rather than small bones , e.g. 
metacarpi , were privileged for the evaluation of cortical 1 3 radiol med ( 2015 ) 120 : 674682 inside church parvis north group inside church parvis north group inside church parvis north group fig . 
6 boxplot of the cortical index measured by x - ray ( a ) , the cortical index measured by ct ( b ) and the bmd ( c ) measured by dxa according to the different burial places index by x - ray and ct scan as femurs are usually in a better state of preservation . 
moreover , a careful selection was made to ensure the use of bones that were as intact as possible on gross examination so as to rule out , as far as possible , the possibility that diagenetic changes had altered bone composition and accordingly density . ct was also used to evaluate the cortical index so as to identify the limit between the cortical bone and the endosteal trabecular component , using the correct visualisation parameters and an accurate measurement technique [ 28 , 31 , 32 ]  . 
ct images make for an easy identification of the linea aspera , which is the posterior point of the diaphysis , allowing for precise geometrical measurements of both the medial and lateral cortical thickness [ 33 ]  . no statistically significant differences were observed in the cortical index measured by x - ray and ct between gender , age or burial place , demonstrating an overall limited bone loss . 
therefore , it may be asserted that the individuals studied showed no signs of diseases known to lead to macroscopic alterations of the cortical bone : in particular , there was no evidence of serious bone remodelling , such as rachitism , osteomyelitis or post - traumatic signs . an interesting collateral finding of the radiological studies was the presence of some focal lesions that were not visible at gross inspection of the femurs : one small round radiolucent lesion of the neck and five calcified areas inside the medullary canal . 
sporadic reports of similar lesions can be found in paleopathological studies [ 34 , 35 ] ; it might well be of interest to compare these findings with the focal lesion patterns of contemporary populations . however , when using dxa on ancient bones , the possibility that bone diagenesis may affect dxa readings cannot be ignored . 
consequently , the material used for this study was selected according to its state of preservation to avoid significant reduction of dxa diagnostic accuracy and all the bones scanned were in good condition with normal morphological features . 
any damaged bones and / or those with artifacts , such as metal deposition or pathological features that might have interfered with the accuracy of the measurement , were excluded from this study . this study identified differences among the assumed different social groups both in males ( only lumbar spine bmd data available ) and females ( both at lumbar spine and proximal femur )  . 
in particular , individuals buried inside the church ( members of the clergy and privileged families ) had statistically significantly lower average bmd values than the individuals buried outside the church ( likely members of rural population , militaries or servants )  . 
these differences may be related to the different lifestyle led by the more privileged subjects compared to the less privileged classes who had a higher dietary calcium intake ( milk and dairy products ) , more sun exposure and vigorous physical activity . 
all patients underwent ophthalmologic evaluations , ultrasound , conventional magnetic resonance ( mr ) imaging and diffusion - weighted mr imaging before the start of therapy and 3 and 6 months after therapy . 
this examination could be used together with ultrasound in the follow - up of this treatment . keywords apparent diffusion coefficient internal reflectivity magnetic resonance imaging ocular melanoma proton - beam therapy ultrasound c . 
puzzo department gian filippo ingrassia , unit di anatomia patologica , university of catania , catania , italy the accuracy of diagnosis of posterior uveal melanoma has improved greatly over the past 40 years . 
many factors have led to increased accuracy in the diagnosis and follow - up of melanoma after proton - beam treatment , including the widespread use of the indirect ophthalmoscope , a better recognition of lesions simulating melanoma , and the development of imaging techniques including ultrasound , computed tomography and magnetic resonance imaging ( mri )  . 1 3 radiol med ( 2015 ) 120 : 634640 ultrasonography is used to help establish the diagnosis , to evaluate possible extraocular extension , to estimate tumour size for periodic observation , to plan therapeutic intervention and to follow up patients after proton - beam therapy . 
standardised echography [ 2 ] , a prescribed subset of diagnostic ultrasound , utilises specific equipment and techniques to assess the topographic , quantitative and kinetic features of a tumour . 
standardised echographic features reported to be characteristic for posterior uveal melanoma include low - to - medium internal reflectivity ( 560 % spike height ) , regular internal structure , a mushroom shape ( seen more frequently in larger tumours ) , solid consistency , sound attenuation and internal vascularity [ 35 ]  . 
in a retrospective study by ossoinig in 1983 , standardised echographic criteria were demonstrated to predict the pathologic diagnosis of melanoma accurately in 96 % of patients enucleated for suspected melanoma [ 2 ]  . 
ultrasonography is excellent for evaluating intravitreous tumour size , but is relatively insensitive to extrascleral extension [ 6 ] and relatively dependent on a skilled operator [ 7 ]  . ocular mri can be used to assess the extent of ocular melanoma and to visualise possible extraocular spread [ 8 ]  . 
apparent diffusion coefficient ( adc ) , the quantitative parameter of dwi , has been proposed as the technique of choice for detection of early response to treatment in brain tumours and head and neck cancers . 
 [ 8 ] demonstrated that ocular melanoma shows a marked diffusion restriction ( with an adc of 106 mm2 / s ) and that dwi helps in differentiat < 1 , 000 ing ocular tumours from retinal detachment . the purposes of this prospective study were to compare the ultrasound and mri parameters of ocular melanoma and to assess their variation after proton - beam therapy . methods patients were included in the study prospectively and consecutively if they underwent proton - beam therapy for choroidal melanoma at the university of catania between may 2012 and september 2013 . 
overall 15 eyes of 15 patients [ 10 women and 5 men ; mean age ( sd ) , 42 years ( 10.5 ) ; range 3055 years ] were included . this study was conducted in accordance with recommendations of the local ethics committee , and informed consent was obtained in accordance with the declaration of helsinki before the procedures . all patients were examined by a senior ophthalmologist ( a.r. ) specialised in ocular tumours and were excluded if : ( 1 ) the tumour had previously been treated by other methods ; ( 2 ) the tumour did not extend posterior to ora serrata ; or ( 3 ) the tumour was bilateral . 
we decided to perform proton - beam radiotherapy if : ( 1 ) the posterior tumour margin extended close to optic disc so that plaque radiotherapy could not be administered reliably without causing optic neuropathy ; ( 2 ) the tumour extended close to fovea so that there was a better chance of conserving central vision with proton - beam radiotherapy than with other methods ; or ( 3 ) the tumour height exceeded 5.5 mm and other forms of conservative treatment were inappropriate [ 10 ]  . all patients underwent thorough ophthalmologic evaluations of the choroidal lesions , including indirect ophthalmoscopy , and standardised a - scan and b - scan echography ( cinescan s ; quantel medical , clermont - ferrand , france ) : the final clinical diagnosis of ocular melanoma was made on the basis of both fundoscopic and ultrasonographic findings . 
after proton - beam therapy , clinical , echographic and mri examinations were performed at 3 and 6 months . ultrasound examination was performed according to a standard protocol , [ 11 , 12 ] using standardised a - scan and contact b - scan instrumentation with separate probes . 
the examination included measurements of basal diameters ( b - scan ) , tumour thickness ( band a - scan ) and internal reflectivity ( a - scan )  . according to coms [ 11 ] , eleven representative b - scan and standardised a - scan echograms were obtained from each tumour with the sound beam directed through the apex , perpendicular to both the tumour surface and the inner sclera . five echograms were obtained with b - scan , two in cross section ( transverse view ) , two in radial section ( longitudinal view ) and one in axial orientation . 
the axial view was utilised primarily to confirm findings obtained with the transverse and longitudinal orientations . six a - scan echograms , performed after calibration to tissue sensitivity , were then obtained : three at the high tissue sensitivity gain settings and three at reduced ga 1 3 636 radiol med ( 2015 ) 120 : 634640 the gain was reduced by approximately 10 db until the appropriate interfaces were clearly displayed . 
the internal reflectivity is automatically assessed by the instrument , reflecting the strength of the internal echoes , comparing the average amplitude of the tumour echo with the amplitude of the scleral peak , which is 100 % [ 11 , 13 ]  . the diagnosis consistent with melanoma primarily indicated that the photoechograms demonstrated low - tomedium internal reflectivity ( 560 % spike height ) , regardless of the shape . 
lesions with internal reflectivity that was slightly irregular or was mediumhigh or higher were also classified as consistent as long as they also exhibited a mushroom - shaped configuration and / or moderate to strong internal sound attenuation [ 14 , 15 ]  . 3 , 700 / 50 , turbo factor 3 , acquisition matrix as previously described by our group [ 16 ] , mri was performed with a closed - configuration superconducting 1.5 - t system ( signahdxt ; ge healthcare , milwaukee , wis ) with 57.2 mt / m gradient strength and 120 t / m / s slew rate , by using an eight - channel high - resolution head coil with array spatial sensitivity technique ( asset ) parallel acquisition . 
the orbital imaging protocol included : ( 1 ) axial and coronal t2 - weighted turbo spin - echo spectral presaturation with inversion recovery ( repetition time 12 , number ms / echo time ms of signals acquired 256 ) ; 256 ( 2 ) axial and coronal t1 - weighted turbo spin - echo ( repetition time ms / echo time ms 2 , number of signals acquired 256 224 ) sequences . 
after intravenous administration of 0.2 ml gadoteric acid ( gadoteratedimeglumine , dotarem , 0.5 mol / l ; guerbet , roissy , charles - de - gaulle cedex ; france ) per kilogram of body weight , axial and coronal t1 - weighted spin - echo spectral presaturation sequences were performed ( repetition time ms / echo time ms 450 / 15.1 , turbo factor 2 , 256 )  . 
the images of conventional ocular mr were evaluated by two radiologists in consensus ( a neuroradiologist with 8 years of clinical experience and a neuroradiology fellow with 3 years of practice experience )  . 
it was documented whether there was retinal detachment and whether the ocular tumour touched the lens , the iris or the ciliary body or whether there was extraocular spread . measurements of tumour volume were performed on contrast - enhanced axial t1 - weighted images with the use of a computerised image - analysis tool that is available as part of the pacs of our hospital ( centricity radiology ra 600 ; ge healthcare , milwaukee , wis )  . 
in all sections in which tumour was present , we manually outlined this structure and calculated the tumour volume , taking section thickness into account [ 17 ] ; in particular , tumour volume was obtained by multiplying the area of tumour outlined on each contrast - enhanced axial t1 - weighted image by the slice thickness . 
the volumes from the first and third scans for each patient were used to calculate percentage variation of tumour volume after 6 months of therapy ( tumour percentage regression )  . 
percentage variation of tumour volume after 3 months of therapy was also calculated . the image quality of the dw images was assessed on a 3 - point scale in consensus by the two radiologists , ( 1 ) minor distortion artefact , mass clearly visible ; ( 2 ) moderate distortion artefact , mass blurred ; ( 3 ) major distortion artefact , mass not visible . 0 , b in all the four time - point examinations , the quantitative measurements were taken as follows ( and previously described ) [ 8 , 17 ]  . 
the roi was delineated within the tumour lesion contained in the largest tumour cross section and was defined as slightly smaller than the actual lesions , excluding the most peripheral parts to avoid partial volume effects . 
values of internal reflectivity , adc and tumour volume at three examinations ( baseline , 3 and 6 months ) were compared by oneway analysis of variance ( anova ) and , if the difference was significant , by post hoc multiple comparisons ( tukey kramer test )  . 
therefore , the final study population consisted of 15 eyes of 15 patients [ 10 women and 5 men ; mean age ( sd ) , 42 years ( 10.5 ) ; range 3055 years ]  . the right eye was affected in nine patients ( 60 % ) and the left eye in six ( 40 % ) patients . 
after proton - beam therapy , tumours shrink in size and the sonographic internal reflectivity increases significantly [ 13 , 1820 ] , but tumour regression may take many months after proton - beam irradiation , from 6 months to 2 years [ 13 ]  . 
this change has been 6 months after 1148 % 35 % therapy 8 , p radiol med ( 2015 ) 120 : 634640 reported by some authors after brachytherapy or protonbeam therapy [ 1922 ]  . 
the replacement of this tissue by necrotic or fibrotic areas , giving larger interfaces , determines the increase in the reflectivity level [ 20 ]  . on mri , we found a significant reduction in melanoma volume at 6 months , suggesting that volume evaluation by this technique can be used in the follow - up . we evaluated the adc values of ocular melanoma . 
 anomas showed an adc of 1 , 180 after proton - beam therapy , the adc values significantly increased 3 months after therapy . 160 10 109 10 adc , the quantitative parameter of dwi , evaluates free motility of water - bound protons within tissues , and t fig . 
c postcontrast t1 - weighted spin - echo spectral presaturation images : the mass along the temporal aspect of the globe is homogeneously hyperintense and shows moderate contrast enhancement ( white arrow )  . 
h postcontrast t1 - weighted spin - echo spectral presaturation images 3 months 10 after therapy : the tumour demonstrates no obvious shrinkage ( white 1 , 000 s / mm2 : melaarrow )  . 
o adc map : the tumour appears less hypointense compared to the previous examinations and the tumour adc value further increases demonstrating increased diffusion 1 3 radiol med ( 2015 ) 120 : 634640 is related to tissue cellularity , as shown by the correlation between adc and internal reflectivity assessed by ultrasound . 
in addition to its simplicity in estimating adc from the dwi data , the adc value is quantitative and magnetic field - independent such that it is one of the most suitable metrics for multicentre and longitudinal studies [ 25 ]  . the main limitations of this study are the small number of patients and the short follow - up . 
in addition , in this study , we used two b values for adc calculations : 0 and 1 , 000 s / mm2 and we did not investigate the possible influence of other b values on the adc of melanomas . 
another technical limitation is related to small dimension of lesions : the section thickness of dwi sequences ( 4 mm ) could seem too high but the only two other papers in the literature investigating dwi / adc in ocular melanomas [ 8 , 23 ] used dwi sequences with a section thickness of 34 mm and 45 mm , respectively . 
to perform a dwi sequence with a 3 - mm section thickness with our head coil , maintaining a good signal - to - noise ratio would lead to an increase in acquisition time that could cause artefacts related to eye motion . 
besides , the 4 - mm section thickness of our dwi sequence was consistent with our studys inclusion criteria : tumour height exceeding 5.5 mas regards the t1and t2 - weighted conventional sequences , consistent with the previous study of sepahdari et al . 
even though 3d sequences are more appropriate for volume calculation , as previously proposed by other authors [ 26 ] , we used 2d images to obtain tumour volume by multiplying the area of tumour outlined on each contrast - enhanced axial t1 - weighted image by the slice thickness . in conclusion , the early detection of tumour changes after proton - beam therapy suggests the utility of investigating all patients at baseline by mri with calculation of adc . 
pearsons r was used to verify the correlation between the dwi findings and the hbi . results on visual assessment , the accuracy , sensitivity and positive predictive value of dwi for the detection of inflammation were 100 % . 
laghi dipartimento di scienze radiologiche , oncologiche e anatomo patologiche , sapienza - universit di roma , rome , italy correlation was found between adc of the terminal ileum and hbi . conclusion dwi sequences may be useful in differentiating actively inflamed small bowel segments from normal small bowel in cd . 
though partial , the correlation between dwi sequences and hbi confirms the utility of this technique in the study of patients with cd . keywords diffusion - weighted mri crohns disease small bowel mr enterography introduction in the last decade , magnetic resonance ( mr ) imaging has been increasingly used for the study of chronic inflammatory bowel diseases . 
this has been made possible by the recent technological development represented by fast imaging and characterised by the acquisition of breath - hold sequences [ 1 ]  . magnetic resonance has some advantages compared to the traditional imaging techniques : excellent contrast resolution , noninvasiveness , cross - sectional imaging , the possibility to obtain luminal , parietal and extra - intestinal findings , absence of radiation exposure . 
moreover , mr can provide functional information about the intestinal wall ( motility ) that cannot be obtained with other imaging techniques such as computed tomography ( ct ) [ 2 ]  . 
all these factors make mr particularly suitable for the diagnosis and follow - up of patients with crohns disease . diffusion - weighted mr imaging ( dwi ) represents a new perspective of mri applied to the study of abdominal pathologies . 
dwi is a technique based on the diffusion motion of water molecules [ 3 ] , which displays information about the extracellular compartment , tissue cellularity and 1 3 586 radiol med ( 2015 ) 120 : 585594 the integrity of the cellular membranes [ 4 ]  . 
in the oncological setting , this technique has been applied in the detection and characterisation of cerebral [ 5 ] , thoracic [ 6 ] , abdominal [ 7 , 8 ] neoplastic lesions and in the evaluation of tumour response to chemotherapeutic treatments [ 9 ]  . 
other applications are represented by the study of inflammatory diseases of the brain [ 10 ] , kidney [ 11 ] and liver [ 12 ] and by the noninvasive evaluation of function of the transplanted kidney [ 13 ]  . only in the last 5 years , dwi sequences have been applied to the study of chronic inflammatory bowel diseases [ 1416 ]  . 
diffusion - weighted images are characterised by high contrast resolution that allows disease - active intestinal segments to be distinguished from normal bowel loops [ 16 ] ; moreover , these sequences allow quantitative measurements such as the apparent diffusion coefficient ( adc ) that can be used to quantify water diffusion in vivo . the purposes of our study were to assess the diagnostic capabilities of dwi with apparent diffusion coefficient ( adc ) measurement in the detection of inflammatory activity of the small bowel in patients with crohns disease , considering endoscopic and histopathological findings as the standard of reference , and to verify the correlation between dwi findings ( signal hyperintensity and adc values of the bowel wall ) and the harvey - bradshaw clinical index ( hbi )  . materials and methods patients this study was conducted in accordance with recommendations of the local ethics committee ; informed consent was waived due to the retrospective study design . patients with a histological diagnosis of small bowel crohns disease who underwent mr examination between february 2010 and january 2013 were selected from our database . 
inclusion criteria were as follows : endoscopically active crohns disease of the terminal ileum diagnosed by means of ileo - colonoscopy performed within 2 months of mr examination ; mr enterography ( mre ) with dwi sequence ( routinely performed in our centre ) ; harveybradshaw index calculated during the gastroenterological assessment on the same day as the mr examination . according to these criteria , 20 patients were included in the study ( 7 female and 13 male ; mean age , 37 years ; age range 2270 years )  . 
in these patients , the small bowel segment ( up to 10 cm ) anastomosed to the colon ( neo - terminal ileum ) and the segment upstream to the pouch were regarded as terminal ileum . harvey - bradshaw index the crohns disease activity index ( cdai ) , widely used in the clinical evaluation of patients with crohns disease , requires eight parameters to be recorded over a period of 7 days : clinical ( subjective feeling of well - being , abdominal pain , number of evacuations with liquid / runny stools , extra - intestinal symptoms , body weight , presence of abdominal masses , anti - diarrhoeal medication ) and laboratory ( haematocrit ) ; the parameters are then multiplied by coefficients which allow one to determine if the patients disease is in remission or in the active phase ( mild , moderate or severe )  . 
unlike the cdai , the harvey - bradshaw index ( hbi ) refers to the assessment of a single day and excludes three variables ( haematocrit , body weight and medication use ) ; besides , it is obtained from the simple sum of the parameters , which must not be multiplied by any coefficient . 
several studies show that the two methods provide essentially the same information [ 17 ]  . hbi calculation : subjective feeling of general well - being ( 0 very good , poor , 3 fair , 2 abdominal pain ( 0 severe ) very poor , 4 none , 1 mild , 2 terrible ) moderate , number of evacuations with liquid / runny stools / day abdominal mass ( 0 doubtful , 2 none , 1 defined , defined and soft ) complications , as follows , with 1 point for each one : arthralgia , uveitis , erythema nodosum , aphthous ulcers , pyoderma gangrenosum , anal fissures , fistulae , abscesses . patients with a score < 4 are considered to be in clinical remission , patients with a score > 7 are considered to have severe activity , and those with a score between 4 and 7 to have mild - moderate activity [ 18 ]  . mr imaging protocol magnetic resonance imaging was performed with a closedconfiguration superconducting 1.5 - t system ( signa hdxt ; ge healthcare , milwaukee , wi , usa ) with 57.2 mt / m gradient strength and 120 t / m / s slew rate using an eightchannel high - resolution torso coil with array spatial sensitivity technique ( asset ) parallel acquisition . preparation patients fasted for 6 h before the mri examination . 
bowel distension was obtained through oral administration of a biphasic contrast agent , a polyethylene glycol solution ( peg 4000 ) ( selg - esse 1000 , promefarm , italia ) ; a total of 1 3 radiol med ( 2015 ) 120 : 585594 1 , 000 ml was administered orally to all patients over the course of 45 min before scanning [ 1 , 19 ]  . 
total scan time was about 40 min . image analysis the evaluation of the mr examinations was performed by two radiologists ( a senior radiologist with 7 years of clinical experience in body mri and a junior radiologist with 1 year of practice ) who were blinded to the clinical and endoscopic results , under the direction of a study conductor . 
the mr images were displayed on a picture archiving and communication system ( pacs ) screen . initial analysis concerned the identification of conventional mr findings in the terminal ileum : mural hyperenhancement ( segmental increased intensity of the bowel wall compared with the intensity of normal - appearing ileum ) , mural thickening ( > 3 mm ) , increased t2 signal in the wall , mural stratification ( visualisation of two or three layers within the bowel wall ) , adjacent enlarged lymph nodes ( > 5 mm in shortest diameter ) , and penetrating disease ( sinus tract , abscess , phlegmon , fistula )  . 
segments graded as 2 or 3 were considered to have active disease . on the basis of mr conventional findings , the study conductor defined two bowel segments to be used in the 1 3 radiol med ( 2015 ) 120 : 585594 588 fig . 
1 a 29 - year - old female with active crohns disease ( cd ) involving the terminal ileucoronal ssfse ( single - shot fast spin echo ) t2 - weighted image with fat suppression ( a ) and axial fiesta ( fast imaging employing steady - state acquisition ) image ( b ) show wall thickening ( white arrow ) and stenosis of the lumen in the terminal ileu note the prestenotic dilatation in b ( white arrowhead )  . 
e , f adc value measurement from the wall of the terminal ileum on magnified dw image ( e ) and corresponding adc map ( f ) : adc value 10 mm2 / s 1.20 quantitative analysis for each patient : a normal - appearing control ileal loop and the most enhancing segment of the terminal ileuin patients who had previous ileocolectomy and ileo - cecal anastomosis , the small bowel segment anastomosed to the colon ( neo - terminal ileum ) was regarded as terminal ileuin the quantitative assessment , the adc measurements were performed independently by the two radiologists in separate sessions . 
adc value measurements from the wall of the terminal ileum and normal - appearing ileal loops were carried out on a workstation with diffusion analysis software ( advantage windows version 4.6 , functool software , general electric medical systems , milwaukee , wi , usa )  . 
 mural thickening ( 95 % ) and increased enhancement ( 100 % ) were the most common findings ; mural stratification and enlarged lymph nodes were present in 15 / 20 patients ( 75 % ) ; increased t2 signal was present in 12 / 20 ( 75 % ) patients ; penetrating disease was seen in 5 / 20 patients ( 25 % )  . the harvey - bradshaw index was calculated in all patients . 
 six patients had a hbi < 4 ( clinical remitting ) ; seven patients had a hbi between 4 e 7 ( light - moderate activity ) ; seven patients had a hbi > 7 ( severe activity ) ( table 2 )  . in all patients , the dwi sequences provided images with a sufficient quality for visual assessment . 
numerous clinical indexes , laboratory and instrumental examinations have been used in the evaluation of these aspects , but no standard of reference yet exists that can meet all these questions . 1 3 radiol med ( 2015 ) 120 : 585594 590 fig . 
2 a 39 - year - old male with active cd involving the terminal ileucoronal ( a ) and axial ( c ) ssfse t2 - weighted images with fat suppression show wall thickening and increased t2 - signal in the terminal ileum wall ( white arrow )  . 
coronal ( b ) and axial ( d ) contrast - enhanced t1 - weighted 3d lava ( liver acquisition with volume acquisition ) images show significant wall thickening of the terminal ileum with stratification and increased enhancement ( white arrow )  . 
this technique , initially used in the field of neuroradiology , is based on the diffusion motion of water molecules [ 3 ] , and provides information about the extracellular compartment , tissue cellularity and the integrity of the cellular membranes [ 4 ]  . recent technical advances in the field of mri have made possible the application of dwi sequences in the study of the abdomen ; however , there are still some technical problems to be solved and no standardised protocol has been proposed in the literature . in our study , we have adopted some technical expedients . 
the acquisition of a breath - hold dwi sequence and the administration of an anti - peristaltic agent ( n - butyl - scopolamine ) during the investigation contributed to further reduce motion artefacts . 
3 a 37 - year - old male with active cd involving the terminal ileu ( a ) coronal fiesta image shows wall thickening in the terminal ileum ( white arrow )  . 
ef adc value measurement from the wall of the terminal ileum on the magnified dw image ( e ) and corresponding adc map 10 ( f ) : adc value mm2 / s 800 s / 1.04 table 3 statistical analysis . 
the sensitivity and specificity of dwi sequences in the identification of disease activity ranged between 86 and 94 % and between 81 and 87 % , respectively . 1 3 592 radiol med ( 2015 ) 120 : 585594 table 4 statistical analysis . 
the lack of patients with normal signal intensity at the level of the terminal ileum correlates with the series of our study that included patients with crohns disease endoscopically active at the level of the last ileal loop . 
increased cell density and viscosity , dilated lymphatic channels and granuloma development can narrow the extracellular space and contribute to a restricted diffusion of water molecules in the inflamed bowel wall [ 16 ]  . in the recent past , a number of clinical indexes ( cdai , biological indexes ) have been used to monitor disease activity and evaluate response to treatment , but there is no accepted reference standard that can provide all this information [ 19 , 22 , 24 , 25 ]  . 
conversely , other authors found a poor correlation between clinical indexes ( cdai ) and findings obtained with imaging techniques ( mri and contrast - enhanced ultrasound ceus ) [ 25 ]  . no study to date has carried out a comparison between the findings of dwi sequences and the harvey - bradshaw index . 
one of the goals of our work was to verify the correlation between the findings of dwi sequences ( signal hyperintensity and adc values of the intestinal wall ) and the harvey - bradshaw index . 
our study showed a good correlation between visual assessment of the last ileal loop with dwi sequences and the harvey - bradshaw index ; on the other hand , no significant correlation was found between the adc value of the terminal ileum and the harvey - bradshaw index . 
the correlation between visual assessment of the last ileal loop with dwi sequences and the harvey - bradshaw index can be a proof of the ability of mri to identify the disease and to evaluate , to some extent , the degree of clinical activity ( mild - moderate or severe activity )  . 
the harveybradshaw index reflects the degree of general inflammation ; the adc value was calculated only at the level of the terminal ileum and was not evaluated on other intestinal segments ( colon ) , possible sites of disease activity . 
 [ 29 ] found a strong correlation between the two indexes in patients with involvement of the distal ileum , but not in those with involvement of the colon ; therefore , these quantitative measures are still being validated . 
 dwi sequences are able to provide quantitative measurements which may allow for a more objective assessment of the disease , on condition that the adc measurements are reproducible , and may allow determination of the activity of regional disease identifying the site of inflammation . 
 1 3 radiol med ( 2015 ) 120 : 585594 this is important in the study of crohns disease , which is characterised by multifocal intestinal lesions [ 15 ]  . in our study , the inter - observer agreement in adc measurements was very good . 
 reproducibility is a crucial parameter in the assessment using quantitative analysis , such as adc measurement , to standardise mri reports , especially in clinical trials . the scientific contributions in the literature and our study suggest the importance of quantitative measurements that can be obtained through the dwi sequences ( adc value )  . 
 these objective measures of inflammatory activity can be used as imaging biomarkers to monitor the progress of the disease and to evaluate the effectiveness of therapies recently introduced [ 15 , 16 ]  . 
the quantitative parameters can be compared if acquired periodically in the same patient , or in different patients studied during the same period [ 16 ]  . another aspect discussed in the literature is related to the usefulness of the bowel preparation and intravenous administration of the contrast mediu in daily clinical practice , oral or rectal preparation is generally not well tolerated by patients and this may limit the use of mri in the study of the intestine . 
 [ 15 ] demonstrated the high accuracy of dwi sequences in the assessment of disease activity , especially in the small intestine ; their study was performed without bowel preparation and without administration of paramagnetic contrast agent to limit the invasiveness of the mri . 
 [ 26 ] have shown that mr colonography with dwi sequences without bowel or rectal preparation can be useful in detecting colon inflammation in inflammatory bowel disease , particularly ulcerative colitis ; their results also indicate that the intravenous administration of the paramagnetic contrast agent could be replaced by the dwi sequences with the advantage of eliminating the risks associated with the administration of gadoliniu in our study , we used a protocol that included the intestinal distension with oral contrast agent [ 1 , 19 ] and the intravenous administration of paramagnetic contrast mediu in detecting disease activity , the dwi sequences showed very high accuracy , comparable to that of the hyperenhancement of the intestinal wall , a conventional finding observed in 20 / 20 ( 100 % ) patients . 
 in this sense , the dwi sequences , owing to the high intrinsic tissue contrast , may represent a viable alternative to the t1 - weighted dynamic sequences in patients with contraindications to the paramagnetic contrast agent due to allergy to gadolinium or to a renal failure condition with a risk of developing nephrogenic systemic fibrosis . 
in our opinion , however , achieving good bowel distension and correlating the findings of dwi sequences with those of conventional sequences represent a fundamental need because the spatial resolution of dwi sequences is quite low and inadequately distended bowel loops may also show high signal intensity on dwi [ 30 ]  . the strength of our study is twofold . 
 ours is also the first study to compare the findings of dwi sequences ( signal hyperintensity and adc values of the intestinal wall ) with the harvey - bradshaw index , easier to calculate than the cdai . our study had some limitations due to its retrospective design and small sample size . 
one limitation is due to the patient population that included selected patients with a histological diagnosis of crohns disease of the terminal ileum ; the lack of true negative patients did not allow us to calculate the specificity of dwi sequences in the visual assessment . 
 one technical limitation is linked to the possibility of a partial volume effect on adc measurements , especially from normal bowel wall , despite the magnification of images we used in this procedure [ 16 ]  . conclusion our study confirms that dwi sequences could be useful in distinguishing disease - active bowel segments from normal intestinal loops in patients with crohns disease . 
palmieri daniela santovito giuseppe marano francesco minerva lara ricci felicia dalitto giuseppe angelelli giuseppe palasciano received : 31 august 2014 / accepted : 27 october 2014 / published online : 20 january 2015 italian society of medical radiology 2015 abstract purpose the american association for the study of liver diseases and the european association for the study of the liver exclude any role of contrast - enhanced ultrasound ( ceus ) in the diagnosis of hepatocellular carcinoma ( hcc ) while the italian association for the study of the liver suggests its use for larger hcc . 
ninety - three patients underwent treatment [ one resection , 23 transcatheter arterial chemoembolisation ( tace ) , 37 radiofrequency ablation ( rfa ) , 32 tace / rfa combined with sorafenib ]  . 
the diagnosis of hcc on ceus was confirmed by the typical pattern of arterial enhancement and portal and / or venous phase washout . results we performed 90 ceus for the initial diagnosis of hcc in 85 patients and 107 ceus for the diagnosis of residual hcc after 1 - month treatment in 92 patients . 
angelelli interdisciplinary medicine department , university of bari , bari , italy predictive value of ceus and ct in the initial diagnosis of hcc were : 63 vs 92 , 100 vs 100 , 100 vs 100 , 9 vs 25 for small hcc ; 77 vs 92 , 100 vs 100 , 100 vs 100 , 13 vs 22 for large hcc . 
in over 90 % of cases hcc is associated with cirrhosis , which represents the most important risk factor for its development . 1 3 628 radiol med ( 2015 ) 120 : 627633 early diagnosis of hcc is very important and is based on the follow - up every 6 months with liver ultrasound ( us ) evaluation of patients with cirrhosis [ 2 ]  . 
however , if the liver nodules are not characterised by this test , the patient is usually referred for additional imaging , such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) and contrast - enhanced ultrasound ( ceus ) , and may require biopsy when additional imaging remains uncertain [ 3 ]  . the use of contrast agents may improve the ability of us to distinguish between liver cancer and benign abnormalities and , because it can be performed at the same appointment as unenhanced us , more rapid diagnoses may be possible . ceus in the early arterial phase shows the arterial blood vessels located in the periand / or intranodular area [ 4 ]  . 
for this reason , hcc after 1530 s from the administration of contrast agent , in the arterial phase , becomes hyperechoic relative to the surrounding liver parenchyma , while in the portal phase ( 5080 s ) and late phase ( 180240 s ) , owing to the earlier clearance of contrast agent from hcc compared with the liver parenchyma , the hcc nodule becomes iso - hypoechoic [ 5 ]  . the role of ceus in the diagnosis of hcc is controversial : the american association for the study of liver diseases ( aasld ) ( 2011 ) [ 6 ] excludes a role for the diagnosis of hcc nodules in patients with cirrhosis since ceus may offer false positive hcc diagnoses in patients with cholangiocarcinoma ( ccc )  . 
based mainly on these considerations , the italian association for the study of the liver ( aisf ) ( 2012 ) has stated a specific role of ceus for hcc nodules larger than 1 cm in association with ct or mri [ 2 ] , even if the european association for the study of the liver ( easl ) ( 2012 ) has maintained the exclusion of ceus for the diagnosis of nodules in cirrhosis [ 8 ]  . dynamic ct or mri is recommended tolls for assessing response at 1 month after resection , locoregional or systemic therapies . 
follow - up strategies for the detection of recurrence include one imaging technique ( ct or mri ) every 3 months during the first year , and every 6 months thereafter to complete at least 2 years , while no role is provided for ceus . 
after that , regular us is recommended every 6 months [ 8 ]  . the aims of this study were are to evaluate the accuracy of ceus in the diagnosis of hcc before treatment and of residual of hcc 1 month after treatment and to compare the accuracy of ceus with that of ct . materials and methods all patients had one or more hcc nodules . 
when suspicious lesions were identified , the location , number , size , and sonographic features of the nodules were evaluated . all patients with suspected hcc nodules at baseline us underwent further imaging modalities ( ceus and ct ) within 1 month and liver biopsy with histological and cytological examination . 
enhancement patterns were studied during the vascular phase up to 3 min , including the arterial ( 049 s ) , portal ( 50179 s ) , and late phase ( 180 s )  . 
figures 1 and 2 represent a typical and an atypical appearance of two different hcc nodules during the ceus examination , respectively . lesions were defined as follows : ( 1 ) conclusive hcc : nodules showing intense contrast uptake during the arterial phase and distinctly detected before enhancement of the surrounding liver parenchyma , followed by washout in the portal and / or venous phase ; ( 2 ) suspicious for hcc : nodules showing early enhancement during the hepatic arterial phase without washout in the venous phase ; ( 3 ) regenerative nodules : nodules with no contrast enhancement during any of the three phases . both conclusive hcc lesion and those suspicious for hcc were grouped together as a positive ceus examination since in both cases the diagnostic pathway is completed with ct and a biopsy , if appropriate . the study was carried out by retrospective evaluation of 124 cirrhotic patients with hcc referred to our department . helical ct was performed using a multislice unit ( aquilion , toshiba ) with preand post - contrast triple - phase 1 3 radiol med ( 2015 ) 120 : 627633 fig . 
1 contrast - enhanced ultrasound image of a small ( 1.2 cm ) hepatocellular carcinoma nodule ( arrows ) : a hyperechoic enhancement during the arterial phase of the examination ( 10 after intravenous injection of 5 ml sonovue ) ; b hypoechoic structure during the portal phase of the examination ( 50 ) helical scans , obtained after i.v. 
 acquisition of the arterial , portal , and delayed phases was automatically started in the arterial phase with bolus - tacking technique , and 70 and 180 s after bolus injection [ 11 ]  . all patients underwent us - guided biopsy using an 18 - gauge biopsy needle ( zanotti medical research , suzzara , italy )  . 
the accuracy of both ct and ceus was compared with the results of the histological diagnosis . patients were classified according to the possible treatment of hcc on the basis of the criteria proposed by the barcelona clinic liver cancer ( bclc ) staging classification . evaluation of the efficacy of locoregional treatment , of chemoembolisation alone or in combination with sorafenib fig . 
2 contrast - enhanced ultrasound image of a large ( 3 cm ) hepatocellular carcinoma nodule ( arrows ) : a slightly hyperechoic enhancement during the arterial phase of the examination ( 10 after intravenous injection of 5 ml sonovue ) ; b almost isoechoic structure during the portal phase of the examination ( 50 ) was carried out with ct and ceus 1 month after the therapeutic procedures , following the world health organization ( who ) criteria that take into account tumour necrosis . 
the results of ceus after treatment were evaluated on the basis of post - treatment ct . statistical analysis the general characteristics of the patients enrolled in the study are expressed as median and range or number and proportions of observations . 
the concordance between ceus and ct examinations was calculated as percentage of positive ceus over total ct positive results and as percentage of negative ct over total negative ceus results . 
in 19 patients more than one ceus examination was performed for the evaluation of a second nodule both before and after treatment . table 2 shows the accuracy of imaging techniques for the diagnosis of hcc before treatment . 
ct accuracy was 92 % both in small and larger nodules . table 2 accuracy of contrast - enhanced ultrasound ( ceus ) and computed tomography ( ct ) in the diagnosis of hepatocellular carcinoma before treatment size of nodule ( n ) ceus ( % ) ct ( % ) 20 mm ( 27 ) sensitivity > 20 mm ( 63 ) specificity sensitivity specificity n number of nodules , ppv positive predictive value , npv negative predictive value , n.s. 
both in our study and theirs the specificity was 100 % for each technique because of the absence of false positive results . on the other hand , the data on the accuracy of ceus in our study are quite similar to the results reported by forner [ 14 ] for smaller hcc nodules , in which ceus had a sensitivity of 51.7 % , but lower than the sensitivity reported in dais study , in which the rate of correct ceus diagnosis of small hcc was 91.1 % [ 15 ]  . the difference in ceus sensitivity between our study and those of sangiovanni , forner and dai does not seem to depend on the standard of reference used for hcc detection , since in all cases histological confirmation was obtained with a biopsy performed on nodules suspicious for hcc at ct or mri and visualised on us . 
therefore , the difference in sensitivity between our study and those of the mentioned authors may be due to the different criteria adopted at baseline us for the selection of patients to be studied with ceus . 
sangiovanni and forner included only asymptomatic patients with child - pugh a - b cirrhosis with no history of hcc , in whom a new solitary , well - defined , solid nodule between 5 and 20 mm was detected by screening ultrasound . small , nodular - type hcc is often indistinguishable from a large regenerative or dysplastic nodule . 
for this reason , in many series that have reported the correlation between baseline us and pathological diagnosis of hepatic nodules in cirrhotic patients , the sensitivity of us ranges from 20 to 72 % [ 16 ]  . 
therefore , the ability to detect by us a nodule suspicious for small hcc is highly dependent on the 1 3 632 radiol med ( 2015 ) 120 : 627633 expertise of the operator performing the examination . 
this limitation is the main cause of the variability of ceus sensitivity in the diagnosis of small hcc and of the need to perform ct after a positive ceus result . the absence of false positive results for both ceus and ct is possibly due to the fact that all patients enclosed in the study were affected by cirrhosis and were enrolled during the periodic follow - up programme . 
similar considerations were made by other authors [ 13 ] , who also reported absolute specificity . more interestingly , the specificity of ceus in the diagnosis of small hcc is very high in ours and previous studies , so that we can reasonably conclude that the absence of a typical ceus pattern may lead to avoid both biopsy and further imaging techniques , as already suggested by sangiovanni [ 13 ]  . 
for this reason , we believe that ceus can be incorporated in the diagnostic algorithm of small nodules ( 20 mm ) in cirrhotic patients after baseline us , because ceus is simpler , cheaper and faster than ct , with 100 % specificity in our study and without side effects . similar conclusions may be drawn for larger hcc nodules ( > 20 mm ) for which we found a higher sensitivity of ceus compared to small nodules even though the technique does not permit a correct diagnosis in 23 % of patients . 
this result is slightly lower than that reported by other authors and implies a need for ct for the long - term evaluation of the efficacy of locoregional treatment even in the presence of a positive ceus result [ 1720 ]  . 
on the other hand , ceus specificity in the assessment of residual hcc after treatment is 100 % for both groups of nodules , as found in our study and reported by previous authors . the main limitation of this study is the retrospective nature of the evaluation of ceus accuracy in the diagnosis of hcc , even though we included only nodules with a histologically confirmed hcc diagnosis , unlike previous studies on the same topic . 
however , ceus does not replace ct in the follow - up of treated nodules because it cannot always clearly depict the border between the tumour , the surrounding liver parenchyma and the possible onset of new nodules ( relapse )  . 
moreover , in addition to nodule characterisation ct usually serves to stage the extension of the tumour . acknowledgments this study was supported by a research fund of the university of bari and it has been accepted as a poster presentation at the hcc summit of european association study liver , geneva , 1316 february , 2014 . conflict of interest the authors declare that there are no conflicts , disclosure of relationships and interests that could be viewed by others as conflicts of interest . ethical standard informed consent was obtained from each patient included in the study for utilisation of their clinical data for scientific purposes . 
lorini department of health science , university of florence , viale morgagni 48 , 50134 florence , italy e - mail : chiara.lorini@unifi.it introduction the multislice spiral ct ( msct ) , by dentascan software , is used in the volumetric study of the dental arches 1 3 radiol med ( 2015 ) 120 : 618626 and mainly for implant planning . 
in recent years a technology named cone beam computed tomography ( cbct ) has been spreading , and it is replacing dentascan - msct in the outpatient [ 5 14 ] , as it accurately studies dental arches with low radiation dose [ 1519 ] , although with longer acquisition time ( at )  . both these techniques use the same image reconstruction principle , termed back - projection , with the addition of feldkamps algorithm in the cbct to respect this law [ 20 ]  . 
 furthermore , both the cbct and the msct are affected by artifacts which disturb , more or less evidently , the electronic reconstructions , thus being the main cause of the images degradation . the literature about motion artifacts [ 5 , 2123 ] is lacking , while it is certainly superior regarding metal artifacts [ 38 , 2331 ]  . 
the majority of the works examine a limited number of cases , performed on phantoms or in vitro [ 3 , 6 8 , 21 , 2426 , 29 , 30 ]  . on this background , the aim of this retrospective study was to analyze the incidence / degree of motion / metal artifacts in patients subjected to cbct acquisitions , evaluating at the same time the administered dose by ctdi assessment . materials and methods patients between 1st january 2013 and 31st december 2013 , 500 patients aged from 6 to 81 years were screened and subjected to dental , maxillofacial or whole splanchocranium cbct examinations , irrespective of their sex , age , disease , treatment , and clinical query . 
they were not required to sign informed consent for our study ; however , they all had provided written informed consent to perform cbct examination . a single dental arch ( 126 superior and 120 inferior arches ) , both arches , maxillofacial , and the whole splanchocranium were studied in 246 , 187 , 45 , and 22 patients , respectively . all patients with any kind of metallic therapy ( orthodontic brace , screw , osteosynthesis device , implant , pin , bridge , root canal , and crown filling ) situated at less than 5 cm of the region of the clinical interest were considered metallic material bearers . 
four - hundred - sixteen patients out of 500 belonged to this group ( submitted to 113 / 108 / 167 / 23 / 5 examinations of superior , inferior , both arches , maxillofacial , and splanchocranium , respectively ) , while 84 patients were excluded because there was no oral metal ( 36 ) or there was metal at more than 5 cm far from the concerning area ( 48 )  . 
before the scan any sort of removable metallic material was removed from the head and neck and a cotton roll ( 4 1 cm ) was used to separate the arches during the acquisition , except for orthodontic exams that were acquired with shut mouth . 
each patient underwent the examination of only one of the following five areas : superior arch , inferior arch , both arches , maxillofacial , splanchocranium ; in our evaluation only the first scan performed was considered . the patients age was divided into four groups : 610 , 1118 , 1960 , and over 60 - years . this is because in the 6to 10 - year - old patients the query was orthodontic - kind , whereas in the 11to 18 - year - old needed orthodontic treatment or developmental pathology surgery ; in the 6to 10 - year - old and 11to 18 - year - old patients low - dose exposure protocols ( at 18 s ) were always applied in all fovs ; the at at 36 s was always used for the extraction or surgical implant planning in the 19to 60 - yearold patients , while in other cases the exposure time was 24 or 26 s . 
in particular , each protocol has the following features depending on at : 18 s ; 360 images ; low dose ( named standard by the producer ) 24 s ; 480 images ; low dose ( named enhanced ) 26 s ; 360 images ; high dose ( named hi - res ) 36 s ; 480 images ; high dose ( named hi - res enhanced )  . small fovs allow all ats , while large fovs only 18 and 24 - s protocols , which are preferably used for the head / paranasal sinus studies , while 26and 36 - s protocols are usually devoted to the dental arches . the 18 s protocol was carried out in all patients under 18 years and in all 18 16 cm fov exams . 
furthermore , in all implant plannings , 36 s protocol was conducted , whereas in other cases at was established referring to age and clinical query . the administered x - ray dose was measured by computed tomography dose index ( ctdi ) [ 32 ] , as read on the console monitor . 
in according to time parameter , radiant doses at 18 , 24 , 26 , and 36 s were estimated . evaluation methods metal and motion artifacts were subdivided into 4 degrees referring to the ability to express a diagnosis about the specific clinical query , analyzing the reconstructed images in all planes ( axial , coronal , sagittal , panorex , and cross ) : degree 0 : absence . degree 1 : not significant presence . 
double edge effect , mainly evident in the anterior region of the right jaw , in patient where the analysis of the left jaw was required for pre - implant purpose . 
the latter is the result represented in the following tables ( i.e. , the values presented in the result section are the mean values between two observers )  . 1 3 radiol med ( 2015 ) 120 : 618626 fig . 
however , these significant artifacts are on the same crown plane allowing the correct evaluation of the bone around the roots dose variable ( 8 18 12 at we grouped the artifact degrees ( g0 the value was equal to 0.05. 8 , 15 12 16 ) , while as for g3 )  . 
the axial section , passing through the pins and root canal fillings , highlights significant artifacts caused by gutta - percha and bismuth endodontic materials , with considerable hypodense and hyperdense streaks typical of photon starvation statistical analysis the examiners concordance was estimated by cohens kappa test . 
kappa values higher than 0.750 were indicators of excellent agreement . we used chi squared test to assess the associations between metal artifacts and two specific variables ( fov and at )  . 
 however , it is possible to determine the correct position of the canal considering the cross section passing through the mental foramen ( image 121 ) and the most distal at least 8 mm sections ( images 129 132 )  . 
for these reasons , the examination was considered diagnostic were performed using large fovs and short scan time in underage . a progressive growth of the interference was observed with age increasing : a greater prevalence of g0 occurred in 610 years old ( 68 % ) and 1118 years old ( 59.8 % ) patients , an evident incidence of g1 in 1960 years old ( 75.9 % ) patients and a considerable increase of g2 ( 44 % ) in old patients , since in those last mentioned single dental arches with small fovs and long scan times were primarily analyzed . dental arch scans showed an artifact rate of 84.3 % , whose 68.1 % not significant , in contrast to 46.4 % in maxillofacial and entire splanchocranium examinations , in which 84.6 % were not significant . 
the not specifically dental focused examinations were done in young patients and in short scan times . motion artifacts ( table 2 ) motion artifact prevalence was inversely proportional to interference intensity . 
a greater number of g0 in 6to 10 - year - old ( 68.5 % ) , 11to 18 - year - old ( 95.8 % ) , and 19to 60 - yearold ( 74.7 % ) patients was identified , whereas a greater incidence of g1 and g2 ( 79.7 % ) occurred in over 60 - year - old 1 3 radiol med ( 2015 ) 120 : 618626 discussion in our study , cbct allowed a reliable opinion in 100 and 98 % of metal and motion artifact cases occurrence , respectively , with an excellent agreement between evaluators and with a low - dose exposure . 
compared to literature , concerning a limited number of cases in vitro or phantom studies , our analysis is the first wide clinical series evaluating both metal / motion artifacts using the same in vivo method ( fov , at , age and anatomical area ) and assessing the dose . metal artifacts showed a statistically significant association with fov . 
in the large fovs prevailed no artifact ( g0 ) because they were primarily employed in the splanchocranium and sinus paranasal examinations that are anatomical areas far from the oral metal . 
at 24 s we noticed higher frequency of significant artifacts ( g2 ) because this time was widely utilized in patients with no removable full prosthesis ( metal with high atomic number ) to avoid hi - res protocols and so to soften photon starvation artifacts [ 6 , 8 , 26 , 28 , 30 ]  . 
beam hardening occurs when the x - ray beam runs into a metal with a low atomic number , such as in the case of titanium ( z 26 ) , used in implantology and in orthodontics . 
cbct metal artifacts are less powerful than msct because the amperage is lower , the dynamic range of the detector is smaller , and the cone - shaped beam allows higher number of angle reconstructions around the metal material [ 5 , 6 , 8 , 15 ]  . 
thus in our series , any kind of metallic material placed beyond 5 cm from the area of clinical interest caused no interference ( 48 g0 patients ) and we were always able to answer every clinical query . 
metal artifacts were more frequent in dental arches focused study , mainly occurring in adults , wherein the clinical query was surgical - implantkind , and so needing very high quality images , with small fovs and long scan times . 
few artifacts were found in young patients analyzed with large fovs and low ats for surgical / functional orthodontic therapies . movement artifacts in cbct technique are expected to be more relevant than in msct due to much longer at . 
a real incidence alteration of motion artifacts did not occur about different fovs ( from 35 to 42.7 % ) , except for 18 16 cm fov ( 82.2 % ) , because it was exclusively used in younger patients for orthodontic purpose . 
in fact , our study showed that the frequency of artifacts in inferior arch exams was around 60 % , while in the superior arch exams it was about 30 % . 
eighteen - second scan time was used above all in under 18 - yearold people for orthodontic reasons , while higher incidence of motion artifacts was identified at 24 - s scan time because it was almost always utilized in over 60 - year - old patients studied by 15 12 cm fov . 
our study was performed with only one horizontal 110 kv equipment although about 50 different cbct scanners are commercially available , but nearly all are vertical type with different scan time and tube voltage [ 34 ]  . 
it could lead to various results either for motion artifacts or for metal ones because increasing kv determinates beam hardening and photon starvation reduction [ 6 , 8 , 26 , 28 , 30 ]  . 
anyway , we did over these few patients and , at the second time , every exam was satisfactory . cbct ctdivol is certainly lower than msct [ 38 , 39 ]  . 
37 patients were irradiated using 2d - rt , whereas 64 cases were treated using imrt . results the median follow - up time was 15.5 months for all the patients . 
the 2 - year lffs rate and the 2 - year rffs rate in the imrt group were higher than the 2d - rt group , although no statistically significant difference was observed in lffs and rffs . 
zhang department of radiation oncology , cancer hospital , chinese academy of medical sciences , peking union medical college , beijing , china e - mail : jingweiluo2013@163.com conclusions although no statistically significant difference was observed in os , lffs and rffs between the imrt group and the 2d - rt group , the incidence of late toxicity declined using imrt , thereby resulting in an improved therapeutic ratio for patients with cescc . keywords cervical esophageal cancer treatment radiotherapy imrt survival toxicity introduction cervical oesophageal squamous cell carcinoma ( cescc ) is relatively uncommon , representing less than 5 % of all oesophageal cancers [ 1 ]  . 
 although the doseeffect relationship of radiotherapy has not been proved by randomised trials in oesophageal cancer [ 9 ] , some retrospective studies [ 10 , 11 ] found a dose response relationship . intensity - modulated radiotherapy ( imrt ) represents an important advance in radiotherapy . 
compared with the traditional conventional radiotherapy ( 2d - rt ) technique , there are several advantages of imrt including : allowing dose escalation , achieving good tumour coverage and normal organ sparing . 
although dosimetric studies [ 12 , 13 ] demonstrated the advantage of imrt in tumours of cervical oesophagus , the clinical results of imrt for cervical oesophageal squamous cell carcinoma are still limited to a few studies [ 7 , 14 ]  . 
the pretreatment workup included a complete history and physical examination , liver and renal biochemistry , complete blood count , barium contrast study , endoscopy , computed tomography ( ct ) scans of the neck and thorax , and ultrasonography of the abdominal region and the cervical region with or without fine - needle aspiration cytology when cervical nodal metastasis was detected . 
all patients underwent disease staging using the ajcc 2002 staging systethe clinical characteristics are listed in table 1 . treatment in this study , 71 patients received radiotherapy alone and 30 patients received concurrent chemoradiotherapy with cisplatin administered either weekly ( 30 mg / m2 ) or every 3 weeks ( 80 mg / m2 )  . 
although ccrt was the primary treatment for non - metastatic oesophageal cancer [ 15 ] , the use of concurrent chemotherapy was not protocolized and was used at discretion of the attending physician of individual cases . 
nine patients were given concurrent cetuximab or nimotuzumab and one patient was given concurrent tarceva in the imrt group . thirty - seven patients were irradiated using 2d techniques ( 2d - rt ) by anteroposterior opposing fields or oblique fields at a daily dose of 2 gy . 
the field of radiation covered the gross tumour with an additional radial margin of at least 1 cm and longitudinal margins of at least 3 c adjacent involved lymph nodes were included , if any , in the radiation field . 
the primary gross tumour volume ( gtvp ) and the involved lymph nodes ( gtvnd ) included all gross disease as determined by imaging , clinical , and endoscopic findings . 
the clinical target volume ( ctv ) included the gtvp with an additional radial margin of at least 1 cm and longitudinal margins of at least 3 c adjacent involved lymph nodes ( gtvnd ) were included , if any , in the ctv . 
in addition , at least a 3 - mm gap was present between the ptv and the surface of the skorgans at risk including the spinal cord , parotid glands , thyroid gland , lung , heart , larynx , trachea , and temporomandibular joints were contoured . 
the volume of ptv receiving more than 105 % of the prescription dose should not exceed 20 % , and that receiving less than 93 % of the prescription dose should not exceed 3 % . 
the dose received by organs at risk of the thorax was constrained as follows : the v20 of bilateral lungs < 30 % , v30 of heart < 40 % , and v40 of heart < 30 % . 
ct scans of 1 3 606 radiol med ( 2015 ) 120 : 603610 the neck and thorax and endoscopy were performed after the completion of treatment and then every 6 months . 
 radiotherapy - induced toxicities were assessed and scored according to the rtog radiation morbidity scoring criteria at each follow - up [ 16 ]  . statistical analyses the statistical package for social sciences , version 17.0 ( spss , chicago , il , usa ) , software was used for statistical analysis . 
the local failure - free survival ( lffs ) , regional failure - free survival ( rffs ) , and overall survival ( os ) were estimated by use of the kaplanmeier method . 
chi - square , fishers exact , and students t tests were used to compare the differences between the conventional radiotherapy group ( 2d - rt ) and the intensity - modulated radiotherapy group ( imrt )  . 
percutaneous endoscopy or surgical gastrostomy was given to three patients , nasal feeding was given to six patients and jejunostomy was given to one patient who was planned to receive preoperative radiotherapy plus surgery . 
for the patients in the 2d - rt group , the overall 2 - year local the aim of this study was to determine whether any difference in locoregional control , overall survival or toxicities could be detected as a result of the change in radiotherapy 1 3 radiol med ( 2015 ) 120 : 603610 fig . 
1 kaplanmeier curve showing overall survival ( os ) , local failure - free survival ( lffs ) and regional failure - free survival ( rffs ) of patients with cervical oesophageal squamous cell carcinoma in the study fig . 
in our study , the 2 - year os rate of patients treated by imrt was 42.5 % , which was similar to the previous studies [ 28 ]  . 
furthermore , in a phase 3 multicentre randomised controlled trial of head and neck cancer comparing imrt with conventional radiotherapy [ 17 ] , no significant differences were seen between randomised groups in locoregional control and overall survival , which was similar to the results of the present study . the dosimetric studies [ 12 , 13 ] demonstrated the advantage of imrt in tumours of the cervical oesophagus . 
 rtog 85 - 01 [ 18 ] indicated that combined chemotherapy and radiotherapy for patients with oesophageal carcinoma could increase the incidence rate of severe acute toxicities but not of severe late toxicities . 
 in a prospective study [ 20 ] , 73 patients with stage iii to iv oropharyngeal cancer receiving weekly chemotherapy ( carboplatin dosed at one times the area under the curve [ auc , auc 1 ] and paclitaxel 30 mg / m2 ) concurrent with intensity - modulated radiotherapy ( 70 gy and 5963 gy were delivered to the gross and subclinical planning target volumes , respectively , in 35 daily fractions ) sparing the important swallowing structures were included . 
at 1 year after therapy , observer - rated dysphagia was absent or minimal in all patients except four : one who was feedingtube dependent and three who required a soft diet . 
compared with the previous studies , which reported rates of abnormal diet of 2042 % at 12 months [ 21 , 22 ] and longterm feeding - tube dependency of 1231 % [ 21 , 2325 ] , the authors concluded that intensity - modulated radiotherapy could reduce post - therapy dysphagia . 
 more accurate definition of the clinical target volume through modern imaging , new advances in radiation oncology including heavy particle treatment , targeted therapy and new chemotherapy agents have all been proposed as strategies to improve quality of life , locoregional control and survival outcomes . 
although no statistically significant difference was observed in os , lffs and rffs between the imrt group and the 2d - rt group , the incidence of late toxicity had declined using imrt , thereby resulting in an improved therapeutic ratio for patients with cervical oesophageal squamous cell carcinoma . the small number of patients , the relatively short follow - up ( particularly in the imrt group ) , and the heterogeneity of patients limited the power of our study to detect small differences in outcome . 
differences between amct and pmct adrenal volumes were evaluated statistically along with differences in the degree of volume change , elapsed time to pmct , and presence of underlying malignant disease . 
ohtomo department of radiology , graduate school of medicine , the university of tokyo , 7 - 3 - 1 hongo , bunkyo - ku , tokyo 113 - 8655 , japan m . 
this may be explained by pathological findings of intracellular lipid depletion . keywords postmortem imaging forensic radiology autopsy imaging adrenal gland volume introduction the use of computed tomography ( ct ) and magnetic resonance imaging ( mri ) have begun to gain roles as adjuncts to more traditional methods in forensic medicine [ 13 ]  . 
the adrenal gland is thought to be among the first of the internal organs to undergo autolysis , and it is assumed that it generally has a normal appearance on pmct until the late postmortem stage [ 14 , 15 ]  . 
thus , we investigated the morphological and volumetric changes of the adrenal glands before and after death from amct 1 3 radiol med ( 2015 ) 120 : 662669 and pmct in the early postmortem stage ( within the first 24 h after death )  . 
if a volume change of the adrenal gland was observed , we aimed to ascertain whether the degree of change was related to the elapsed time or the underlying disease . autopsy technique materials and methods subjects this study was approved by the ethics committee of our institution , and informed consent was obtained from the families of the deceased . 
we performed amct , pmct , and conventional autopsy on 28 consecutive patients who died from non - traumatic causes at our tertiary - care academic hospital between april 2009 and september 2010 . 
the exclusion criteria were as follows : adrenal glands demonstrating a gross tumour on amct or pmct . amct imaging technique all amct studies were performed without contrast medium on a 64 - detector - row helical ct scanner ( aquilion 64 , toshiba medical systems corporation , ohtawara , japan ; discovery ct750 hd or lightspeed vct , ge healthcare , buckinghamshire , uk ) in the craniocaudal direction with the patient in the supine position with raised arms . 
image reconstruction was performed at 5 - mm intervals with a 350 - mm field of view and a 512 512 image matrix . pmct imaging technique all pmct studies were performed without contrast medium on a 4 - detector - row ct scanner ( robusto , hitachi medical corporation , tokyo , japan ) in helical mode in the craniocaudal direction ; the cadaver was placed in the supine position with the arms at the sides . 
the scan parameters were as follows : slice thickness 2.5 mm ; slice interval 1.25 mm ; rotation time 0.5 s ; tube voltage 120 kvp ; and tube current 250 ma . 
image reconstruction was performed at a 5 - mm thickness with a 350 - mm field of view and a 512 512 image matrix . all autopsies were performed by board - certified pathologists immediately following the pmct scans . 
any pathological lesions in the glands were also noted . measurements of the adrenal glands on ct images were analysed using imagej 1.46r ( wayne rasband , nih , bethesda , md , usa ) , which was downloaded from using two - dimensional axial datasets , the image analysis was individually performed by two board - certified radiologists blinded to the clinical information . 
the areas of the adrenal glands were measured on all axial images between the most cranial ( the 1st slice ; a1 , cm2 ) and the most caudal slice ( the jth slice ; aj , cm2 ) that included adrenal gland tissue . 
the volume of each adrenal gland ( v , cm3 ) was calculated by a summation of all the measured areas of the relevant adrenal gland multiplied by the slice thickness ( 0.5 cm ) , which was the same method used in previous studies [ 16 , 17 ] : fig . 
in the present study , we did not measure or evaluate the ct values of the adrenal glands . statistical analysis statistical analyses were performed using graphpad prism 6 software ( graphpad software inc . , la jolla , ca , usa )  . 
pearsons correlation coefficient was used to evaluate correlations between the reduction rate of the volume and the elapsed time from amct to death or from amct to pmct , and between the volume on pmct and the weight at autopsy . 
thus , high inter - rater agreement was achieved . comparisons between adrenal weight and volume conventional autopsies revealed that the weight of the right and left adrenal glands was 2.111.0 g ( mean 6.0 g ; median 6.1 g ) and 3.214.4 g ( mean 6.3 g ; median 5.6 g ) , respectively . 
among the adrenal glands that shrank on pmct , the reduction rates of the right and left adrenal glands were 7.871 % ( mean 32 % ; median 31 % ) and 6.6 to 68 % ( mean 24 % ; median 22 % ) , respectively . 
in the morphological analysis , raters found no morphological changes of the adrenal glands in any case when comparing amct and pmct ( 0 out of 55 total adrenal glands )  . 
the mean calculated volumes of the left adrenal gland were approximately 3.4 cm3 on antemortem ct ( a ; arrow ) and 2.6 cm3 on postmortem ct ( b ; arrow )  . 
 we observed volumetric declines in the adrenal glands after death , but did not observe morphological changes on ct . few studies on adrenal glands have focused on the relation between the volume on ct and the weight at autopsy . 
volume measurements of the adrenal glands in the present study demonstrated relatively good correlations between volume and weight . we observed volumetric declines in the adrenal glands after death ; however , the mechanism was not fully elucidated on the ct studies , as we did not observe any changes except for the volumetric changes . 
the loss of adrenocortical lipids can be observed after a prolonged survival time [ 23 ] , and the nuclei of adrenal cells decreased in size , followed by cellular shrinkage in an experiment with fowl [ 24 ]  . 
these theories suggest that the present results of declines in volume of the adrenal glands may be partly caused by lipid depletion , which was confirmed in the present conventional autopsy investigations . 
in fact , there is no definition of adrenal intracellular lipid depletion among clinical pathologists for conventional autopsy , and the diagnosis is left to the discretion of the individual pathologist . 
although we did not take microscopic findings into statistical consideration in the present study , it is hoped that a scoring system for intracellular lipid depletion might be correlated with adrenal volume shrinkage in future studies . on the other hand , a slight volume increase or decrease ( reduction rate < 15 % ) was observed in seven subjects ( cases 6 , 9 , 15 , 17 , 19 , 22 , and 27 )  . 
it was reported that prolonged stress or dying from chronic disease may induce hypertrophy or hyperplasia of the cortex and increase the weight of the adrenal gland [ 25 ]  . 
it seems that postmortem changes do not follow an even and steady course , and might be affected by various factors such as age , pathological state , drugs , and so on . 
the changes in adrenal volume varied among the subjects in the present study ; volumetric decline was observed in most subjects , but there were no significant changes in other subjects . the fact that no morphological changes on ct occurred after death and the fact that no intra - adrenal gas was identified in any patient in the present study coincide with a previous report stating that the normal appearance of the adrenal gland is retained until putrefactive gas is present [ 14 ] , as the present study group was in the early stage after death . 
decomposition is a normal postmortem process that begins to occur after death through autolysis , which is one of the first changes to appear in postmortem , and sometimes even before death if the agonal phase is long ( intravital autolysis , especially in clinical death )  . 
we 1 3 668 radiol med ( 2015 ) 120 : 662669 found that there was no significant correlation between the reduction rate of adrenal volume and the elapsed time from amct to death or from death to pmct for the bilateral adrenal glands . 
although a statistical difference in the reduction rate of the left adrenal gland was found , we considered that this was because one subject ( case 15 ) lowered the mean reduction rate . 
if there were many more subjects , a statistical significance in the left adrenal gland might not have been achieved as was observed in the right adrenal gland . the present study has some limitations . 
while it was probably large enough to make a rough statement about major changes , it is hoped that additional research will be conducted for future evaluations in a larger number of subjects using thinner slices of the adrenal region ( 1 mm or less ) on the same scanner . conclusion the present ct study revealed that there was a statistical volume reduction in the adrenal glands in the early phase after death without any visual morphological changes on ct . 
with the advent of multidetector ct ( mdct ) , radiologists are able to more effectively characterize life - threatening traumatic disorders within a few seconds in stable or stabilized patients . 
in this article , the indications for mdct in the polytrauma setting are discussed . keywords trauma polytrauma multiple trauma computed tomography multidetector computed tomography diagnosis management why mdct imaging ? the probability of survival of trauma is predominantly determined by the injury mechanis in addition , the g . 
gualdi policlinico umberto 1 , rome , italy e - mail : chiarandreoli@gmail.com preclinical and clinical trauma management within the first hour after an injury ( golden hour ) is significant and strongly influences the survival rate [ 1 , 2 ]  . the standardized trauma - related death rate for the 25 eu members is 28.5 per 100 , 000 . 
however , in the eu in general , the incidence of mva - related death is significantly decreased in the past 10 years [ 3 ]  . this development is in part not only a result of the improvement in resuscitation procedures but also due to the innovation of the radiological diagnosis , especially the implementation of ct in the early phase of the emergency management [ 46 ]  . 
by doing so , the mortality rate from highly severe trauma significantly decreased especially in cases of severe trauma . compared to mdct imaging , plain radiography of the cervical spine , the thorax , and the pelvis has substantially lower diagnostic power . 
also mdct imaging is substantially superior to plain radiography for the diagnosis of cervical spine and pelvic trauma [ 710 ]  . in the trauma setting , sonography plays a strategic role in unstable patients to detect hemoperitoneum , the presence of which may lead to the surgical treatment [ 11 , 12 ]  . 
 actually , it is a useful method for recognizing intraperitoneal bleeding in hypotensive patients who need an emergent laparotomy and for diagnosing cardiac injuries from 1 3 642 radiol med ( 2015 ) 120 : 641654 penetrating trauma [ 11 ]  . 
for this reason some trauma centers have begun performing an extended fast exam ( efast ) , evaluating for pneumoand hemothorax in addition to intraperitoneal injuries [ 13 , 14 ]  . another important issue for the early use of mdct imaging in the diagnostic algorithm of traumatized patients is that dedicated organ injury scores ( ois ) have been developed only for ct imaging [ 1517 ]  . 
however , the ois help the trauma team to predict whether the patient will need surgery or could be handled with a wait - and - see strategy . diagnosis from head to toe : the whole body protocol until a few years ago , there was a traditional diagnostic protocol approach for hemodynamically stable polytrauma patients consisting of plain radiographs of the chest , cervical spine , and pelvis and an abdominal ultrasound . 
this approach has proved to be ineffective and essentially dangerous in the assessment of high deceleration injury [ 18 ] actually , several studies published in the literature over the past 10 years have shown that the number of unexpected injuries on physical examination and x - ray / ultrasound is very high when compared with the current whole - body mdct protocol [ 19 ]  . 
the higher dose of exposure to ionizing radiation for the protocol based on mdct ( 20 msv for protocol based on ct versus 9 msv for the traditional one ) is the only price to be paid in respect of the inestimable advantage of detecting unexpected injuries [ 20 ]  . 
 [ 21 ] published an important study in which they pointed the importance of using a single - pass whole - body multi - detector ct for major trauma , which allows to significantly reduce the overall time of stay of the patient in the ct suite and access to the operating room , demonstrating the indisputable advantages of mdct in all the phases of diagnostic and therapeutic process . 
the multiphasic protocol consists in an arterial phase from the circle of willis to the iliac crests and the venous and excretory phases from the diaphragm to the pubic symphysis , preceded by a basal scan of the skull . 
d , e fracture of the skull with involvement of the left frontal sinus and massive parenchimal hematoma in the left frontal lobe , characterized by multiple hyperdense cortico - subcortical hemorrhagic foci context of major trauma . 
in 2005 the spine trauma group has developed a new classification system and an injury severity score ( thoracolumbar injury classification and severity score , or tlics ) , which may facilitate communication between physicians and serve as a guideline for treatment . 
 points are assigned for each category , and the final total points suggest the correct treatment option [ 34 ]  . thorax thoracic injury is the third most often - occurring trauma , after head and limbs injuries , being responsible for 25 % of death in polytrauma patients [ 3537 ]  . 
the role of imaging is essential to identify the whole spectrum of injuries and to indicate a timely and effective therapeutic approach . mdct is the method of choice in polytrauma stable or stabilized patients to quickly identify and clearly characterize many dangerous conditions such as small amounts of pneumothorax , hemotorax , pneumomediastinum , aortic and others vascular injuries . 
the use of intravenous cm is essential to recognize vascular lesions and the arterial phase imaging is mandatory for the depiction of thoracic vascular trauma ( table 1 ) [ 38 ]  . however , in unstable patients , chest radiograph and extended fast ultrasound are performed in the shock room for the detection of many pathologic conditions such as pneumothorax , pleural effusion , mediastinal enlargement , and rib fractures which may require an immediate treatment [ 14 ]  . 
consequently , serial scans are indicated and the radiologist is responsible for the followup and the indication for additional exams , such as mri [ 29 ]  . mdct imaging has become the imaging standard of reference in evaluating facial trauma and for determining which patients will require surgical treatment for osseous injuries . 
trauma radiologists should be aware of the major types of facial fractures such as naso - orbitoethmoid , zygomaticomaxillary complex , orbital , and le fort fractures [ 30 ]  . spinal column these injuries are observed , predominantly , as a result of motor - vehicle accidents , falls from heights and sports , and thus , young men are more affected . 
vertebral trauma is responsible for temporary or permanent disability that may be seen immediately after the traumatic event , or at a distance , as a result of mechanical instability not properly treated . mdct imaging best depicts the biomechanical parameters that have caused specific injuries , and thus , helps to provide rapid and stable therapy decisions , far superior to radiographic examination with a proper and strict 1 3 645 radiol med ( 2015 ) 120 : 641654 fig . 
they occur when the lung parenchyma is compressed between the chest wall and vertebral column . lacerations and pneumatoceles are the result of rupture or shearing of lung tissue , direct puncture by rib fractures , high alveolar pressure , e.g. , by sudden compression of a bronchus , or compression of the acini against bone . 
although surgery has traditionally been considered the treatment of choice for these injuries , recent reports show that conservative treatment can be effective in selected patients [ 44 , 45 ]  . in up to 8 % of patients , diaphragmatic injuries occur after blunt trauma often associated with others injuries , such as pelvic fracture , hepatic or splenic lesions , or aortic injury . 
many diaphragmatic injuries are small in size and often occasionally detected , whereas when associated with a thoracic herniation of abdominal organs , they may need a prompt diagnosis and treatment . 
in these cases , chest radiograph is often diagnostic , but mdct is essential to evaluate the herniated organs , their perfusion , and the effect of the compression on the thoracic content . 
the use of mpr and 3d reformatted images are useful in selected cases and should be routinely performed and compared to the axial views [ 46 ]  . abdomen abdominal trauma is a common cause of morbidity and mortality , especially among young adults . 
a contrast - enhanced axial scan ( lung window ) shows multiple , displaced rib fractures ( arrows ) determining pneumothorax ( asterisk , a ) and an area of contusion of the lung parenchyma . 
b 3d reconstruction image gives a better perspective of the costal fractures relatively rare , but responsible for a high percentage of deaths before the patients arrival to the emergency room ( 8590 % ) [ 40 ]  . 
the radiologists role at the a&e is to differentiate major from minor aortic injuries on the basis of their features [ 42 ] to the address the patients to their appropriate clinical management . 
 extensive pneumomediastinum and subcutaneous emphysema at the level of the anterior chest wall are also shown organ injury depends upon the specific injury mechanism and the vulnerability of the patient at the time of the event [ 47 ]  . the diagnostic evaluation of the abdominal traumas is included in the whole - body mdct , indicated in any polytrauma stable patient [ 48 ]  . 
the evidence of active bleeding in one of the most important factors in the choice of treatment ( conservative , interventional versus surgical ) [ 18 , 49 ]  . fast ultrasound in unstable patients is still indicated to rule out the presence and distribution of free fluid , as indicator of traumatic lesions of the abdomen and pelvis [ 11 , 12 ]  . ultrasound , also with the use of echografic contrast medium , can also be useful in the follow - up of solid organ lesions conservatively treated . 
contrast - enhanced axial ct a shows dislocation of the gastric body into the left thoracic cavity , as a result of rupture of diaphragm ( black arrows , dependent viscera sign )  . 
selection criteria for nop are represented by hemodinamic stability and grading of the lesion , considering the entity of hemoperitoneum and the presence of vascular injuries ( active bleeding or pseudoaneurysm ) [ 5053 ]  . whole - body mdct for trauma is required to detect vascular lesions ( especially the arterial lesions , studied in the arterial phase ) and to evaluate extension and characteristics of solid organ lesions , ranging from small contusion to a parenchymal hematoma or lacerations . 
also , the site of injury ( superficial or deep ) is considered in the grading of lesions , being correlated to the presence and quantity of hemoperitoneum and bleeding . the most frequently involved organs in abdominal trauma patients are liver and spleen , but also kidneys , bladder , pancreas , bowel , and mesentery can be affected . 1 3 radiol med ( 2015 ) 120 : 641654 648 fig . 
in a , b contrast - enhanced axial ct scans show a large hematoma within the right lobe of the liver with a hyperdense blush in its context in the arterial phase . 
 splenectomy increases the risk of infections and for this reason nonsurgical treatment in stable patients is preferred in absence of vascular involvement or massive hemoperitoneuthe overall success rate for conservative treatment is approximately 70 % in adults and 95 % in children [ 50 , 51 , 5457 ]  . injuries occur to the liver in 20 % of cases following blunt trauma and in up to 70 % of cases following penetrating trauma . 
however , indirect signs are considered to have an overall sensitivity as low as 2075 % [ 6164 ]  . renal injury occurs in up to 10 % of cases of significant blunt trauma . 
the diagnosis of high - grade injuries is crucial , as they often warrant operative treatment due to parenchymal laceration extending through the renal cortex , the medulla and collecting system , or progressive hemorrhage from the main renal artery or vein , hilar avulsion with a devascularization of the organ . 
renal injuries require an additional delayed mdct acquisition phase to depict iodinated urinary extravasation from the collecting system [ 65 , 66 ]  . bladder injuries usually occur in patients with severe blunt trauma who have sustained pelvic fractures . 
the distinction between intraand extraperitoneal bladder rupture is crucially important , since intraperitoneal ruptures require surgical repair , while the latter are usually treated with conservative catheter drainage [ 67 ]  . pelvis and extremities pelvic fractures are common injuries in polytrauma ( 58 % ) and their severity ranges from low - energy , stable fig . 
a there is no evidence of obvious pancreatic injury but only a moderate amount of free fluid along the renal fascia is seen ; b 2 days later , a hypodensity of the pancreatic head is seen in keeping with a laceration ( arrow )  . 
11 contrast - enhanced ct scan shows a large hematoma along the descending part of duodenum ( arrows ) with multiple free air bubbles along the border of the lesion in keeping with a duodenal perforation . 
actually , it allows to promptly direct the management of the patient ( conservative versus surgical ) or to indicate the need of the interventional radiology in the presence of active bleeding or other complications . the wide use of mdct as method of choice in stable polytrauma patients increases the survival percentage and reduces the use of plain radiography of the spine , the thorax , and the pelvis in the emergency department . 1 3 radiol med ( 2015 ) 120 : 641654 652 fig . 
a multidetector ct with volume - rendered 3d reformation shows traumatic diastasis of the symphysis pubis , fracture of the right sacroiliac joint ( arrows ) , fracture of the anterior wall of the right acetabulum ( open arrow ) , and fracture of the upper and lower pubic rib contrast - enhanced axial scan shows a large jet of active bleeding from the right internal iliac artery spreading in the extraperitoneal pelvic space . 
we evaluated recanalization rate , clinical outcome after 90 days as well as differential costs of aspiration and stent - assisted thrombectomy . results a group of 16 patients met the eligibility criteria to undergo et with a baseline nihss score of 22 ( range 1239 )  . 
curr dossi stroke unit , department of internal medicine , bolzano central hospital , via lorenz boehler 5 , 39100 bolzano , italy keywords stroke endovascular treatment mechanical thrombectomy aspiration thrombectomy introduction stroke is the third cause of death and the first cause of disability in europe . 
intravenous tissue plasminogen activator [ tpa ; alteplase ( actilyse , boehringer ingelheim ) ] is the only proven reperfusion therapy for acute ischemic stroke ( ais ) according a high - level evidence [ 1 ]  . 
endovascular treatment ( et ) with various thrombectomy devices has been recently shown to be effective up to 8 h after the onset of stroke symptoms with a low complications rate [ 46 ]  . 
moreover , mechanical thrombectomy techniques proved better recanalization rates than intravenous tpa or intra - arterial thrombolysis alone , especially in large intracranial vessel occlusion [ 7 , 8 ]  . 
although recent randomized controlled trials ( rct ) showed that et is not superior to systemic tpa for ais in terms of clinical outcome , selected patients may still take advantage of an endovascular approach [ 911 ]  . 
a limit of these rcts is heterogeneity of technical approaches to thrombectomy including intra - arterial t - pa , merci retrievers , stent retrievers as solitaire , first generation aspiration catheter of penumbra syste the aim of our study was to report preliminary results of a standardized sequential approach to 1 3 656 radiol med ( 2015 ) 120 : 655661 et of ais in patients not responsive to intravenous t - pa or with contraindications to pharmacological treatment . patient selection from july 2013 , we prospectively acquired a database of consecutive patients , who underwent sequential endovascular thrombectomy approach ( seta ) and followed them up for a period of at least 90 days . 
all patients were included in the international registry of sits ( safe implementation of treatments in stroke ) , an academic - driven , non - profit , international collaboration based at karolinska institutet and karolinska university hospital in sweden . criteria for selection of patients were : moderate to severe ischemic stroke with an nihss score 12 and a time window of less than 6 h for anterior circulation and 12 h for posterior circulation ; no or poor neurologic response to iv rt - pa ( decrease of nihss score of at least four points ) or contraindications to iv rt - pa . 
all patients with moderate to severe ischemic stroke underwent native ct to exclude hemorrhage and assess aspect ( alberta stroke program early ct ) score and immediate ct angiography to demonstrate a large - vessel occlusion , i.e. , internal carotid artery ( ica ) , m1 tract of middle cerebral artery ( mca ) and basilar artery ( ba )  . 
in patients with undetermined onset time , as for example wake - up stroke , mri was obtained to evaluate dwi / flair mismatch , defined as visible acute ischemic lesion on dwi with no traceable parenchymal hyperintensity in the corresponding region on flair imaging [ 12 ]  . 
decision to et was collegially taken by a neurologist and a general interventional radiologist . technical success was defined as recanalization of the target vessel as assessed by two experienced interventional radiologists according to tici score including score 2a , 2b and 3 ( thrombolysis in cerebral ischemia ) [ 13 ]  . 
symptomatic intracranial hemorrhage ( sich ) was defined as parenchymal hematoma type ii or subarachnoid hemorrhage with neurologic deterioration leading to an increase of national institutes of health stroke scale ( nihss ) score > 4 or leading to death within 36 h of treatment [ 14 ]  . neurologic evaluation was quantified according to nihss at admission , 24 h and 7 days after intervention . 
the latter acts as a distal access catheter facilitating delivery of the stent retriever through the occlusion site and consenting distal aspiration during retrieval . cost analysis current cost of all angiographic devices involved in standardized procedures was calculated and compared , including femoral sheath , diagnostic catheter , guide catheter and microcatheter , guidewires , reperfusion catheter and stent retriever . 
 pricing data were obtained by the bursar office of the hospital at the time of study . we excluded costs of consumable goods , negligible in the order of magnitude and common to different techniques , such as sterile table kit , syringes , needles , heparinized saline solution and drip infusion set . 
personnel and administrative costs were also excluded because they are common to different techniques and do not contribute to the differential cost . results in the period between july 2013 and march 2014 , 58 patients presented at our hospital with ais and underwent systemic thrombolysis and / or mechanical thrombectomy . 
 16 / 58 patients affected by a large - vessel ais met the selection criteria and were treated with seta , nine cases with occlusion of m1 tract of a mca , three cases with carotid 1 3 radiol med ( 2015 ) 120 : 655661 fig . 
1 treatment flow chart of patients with a documented large intracranial vessel occlusion according to the sequential endovascular approach ( seta ) adopted in our center table 1 clinical and technical data patient no . 
mean nihss score at baseline was 22 , ranging from 12 to 39 . recanalization of target vessel was obtained in 15 / 16 ( 94 % ) cases ( tici 2 / 3 ) with an optimal revascularization of distal capillary bed ( tici score 2b / 3 ) in 14 / 16 cases . 
left internal carotid angiography ( b ) confirms the mca occlusion just downstream to the lenticulostriate arteries ( white arrow ) radiol med ( 2015 ) 120 : 655661 11 / 15 ( 73 % ) cases , recanalization was obtained with firstline aspiration approach alone , i.e. , with direct aspiration technique ( adapt )  . 
in the adapt group , mean procedural time from groin puncture to recanalization was 47 min [ puncture time to recanalization ( ptr ) ] ( 24101 min )  . 
overall mortality was 4 / 16 , in one case owing to massive reperfusion hemorrhage and in one case , where thrombectomy was inefficient , to cerebral infarction with massive edema . 
the other two deceases were related to non - cerebral events . regardless of the thrombectomy technique , our common approach consisted of a femoral sheath , a diagnostic 5f catheter and a 0.035 in hydrophilic guidewire for diagnostic phase , followed by a 8f or 7f guide catheter on an exchange wire . 
previously endovascular techniques for stroke treatment included intra - arterial administration of pro - urokinase and the first world - wide available device for mechanical thrombectomy called merci retriever ( concentric medical , mountain view / ca , usa ) [ 17 , 18 ]  . 
in particular , higher recanalization rates with stent retrievers than with the merci retriever have been described [ 7 , 19 ]  . aspiration thrombectomy approach made a comeback thanks to advances in catheter technology allowing largebore catheter to reach intracranial vessels at the site of occlusion and directly aspirate the clot , a technique defined with the acronym adapt ( a direct pass first - pass aspiration technique ) [ 20 , 21 ]  . 
we adopted the largest catheter fitting the occluded vessel and that was penumbra 5max reperfusion catheter ( penumbra , alameda / ca , usa ) in all cases but one . 
when this technique is successful , it consents to reduce the use of other devices , such as stent retriever or separator , leading to a much lower device - related cost [ 23 ]  . 
in cases where aspiration technique proves ineffective , a second level technique can be adopted as , for example , by introducing a stent retriever through the same reperfusion catheter . 
moreover , distal aspiration can be performed during stent retrieval , a combinative technique that has been already described as solumbra , a crasis of solitaire and penumbra [ 24 ]  . 
such a two - step approach to thrombectomy has been already described with positive technical and clinical results [ 2225 ]  . adapt technique has proved to be faster and more effective than any series reported in the literature [ 2022 ]  . 
in addition , it is more capacious along its proximal segment , increasing its luminal volume and thereby resulting in an increased aspiration capacity and force over previous versions of aspiration catheters [ 21 , 28 ]  . four patients died during hospitalization ( 25 % ) , two for other reasons than stroke itself ( sepsis in acute cholecystitis and myocardial infarct )  . 
2 of 4 patients deceased because of stroke , both 80 years old , one with poor recanalization of the left mca ( tici 1 ) despite combined technique , and the other one after developing a post - reperfusion parenchymal hematoma with massive edema requiring craniotomy . 
despite the low number of cases , incidence of sich is much lower than the cutoff value of 12 % stipulated as standards of practice by the international multisociety guidelines of 2013 [ 30 ]  . 
complications have been reported to be higher with stent retriever thrombectomy than with penumbra system thrombectomy , albeit with similar positive clinical outcome rates [ 2022 ]  . we had two cases of emboli to new territories ( ent ) occurring one after aspiration thrombectomy and the other after combined aspirationstent retrieve technique . 
aspiration alone is considered to be associated with a lower ent rate than with other mechanical techniques because of complete engaging and removal of thrombus without its fragmentation , as possible using separator or stent retrievers . 
moreover , fragmentation of thrombus with the separator has been shown to originate small emboli that migrate in peripheral vessels , not suitable for distal thrombectomy and unfavorable for collateralization [ 31 ]  . future development thrombectomy should aim to better patient selection , as for example , on the basis of stroke etiology . 
the cause of occlusion could be related to the composition and the physical characteristics of thrombus such as hardness and elasticity and influence responsivity to different thrombectomy approaches as well as lysability [ 3234 ]  . 1 3 660 radiol med ( 2015 ) 120 : 655661 major limitation of our study is the low patients number . 
although preliminary , our results are encouraging not only in terms of technical success , similarly to other reports on the aspiration technique , but above all in terms of clinical outcome also which is reported to be approximately 40 % [ 30 ]  . 
at 90 days follow - up after treatment , 9 patients of 16 had a positive clinical outcome with mrs 0 in 5 patients , mrs 2 in 2 patients . 
 1 in 2 patients , mrs we adhered to the quality benchmarks suggested by the international multispeciality document recently issued by a consensus of many principal international societies , in particular by strictly applying selection criteria [ 30 ]  . 
time to treatment is another fundamental parameter , which affects clinical efficacy of stroke therapy and adherence to the time intervals suggested by the same paper could have positively affected clinical outcomes of our patients [ 30 , 35 ]  . our differential cost analysis considered only current price of devices we use in standardized ets . 
the cost ratio of these two devices is about 1 : 3 and mainly accounts for the high differential cost of the techniques . the use of aspiration as an initial approach is on average the less expensive method to achieve acceptable recanalization rates with low complication rates . 
 [ 22 ] , the most cost - effective approach to a large - vessel occlusion might be what we define seta , i.e. , to attempt a brief direct aspiration with a large bore first and if this fails then proceed with other devices , such as a stent retriever . 
interventional treatment strategies with adjunctive mechanical thrombectomy or intra - arterial thrombolysis appear to have an acceptable cost - effectiveness profile compared to iv tpa alone for large - vessel stroke based on currently available data [ 36 ]  . heterogeneous technique and devices have been included in recent rcts possibly limiting the demonstration of clinical efficacy of endovascular approach and resulting in non - superiority of mechanical thrombectomy to systemic treatment [ 1012 ]  . 
we consider endovascular approach as a rescue treatment in patients affected by occlusion of large intracranial vessel who receive full dose iv t - pa treatment without showing any neurological response or who have contraindication to pharmacological treatment . 
rutty1 received : 10 february 2015 / accepted : 29 may 2015 / published online : 25 june 2015 italian society of medical radiology 2015 abstract radiography has been used for identification since 1927 , and established a role in mass fatality investigations in 1949 . 
pmct offers several advantages compared with fluoroscopy , plain film and dental x - rays , including : speed , reducing the number of on - site personnel and imaging modalities required , making it potentially more efficient . 
one particular problem is that due to the fact that forensic radiology is a relatively new sub - speciality , there are no internationally established standards for image acquisition , image interpretation and archiving . 
the dvi working group of the international society of forensic radiology and imaging supports the use of imaging in mass fatality response and has published positional statements in this area . 
this review will discuss forensic radiology , pmct , and its role in disaster victim identification . keywords disaster victim identification ( dvi ) mass fatality incident ( mfi ) postmortem computed tomography ( pmct ) imaging * a . 
by comparing the unique biological features of nasal accessory and mastoid sinuses , visible on both sets of x - rays , the doctors were able to confirm that the deceased man was formerly their patient . 
this comparison of ante and postmortem radiographs is still considered to be one of the most accurate techniques to establish identity . radiology subsequently established a role in mass fatality examinations in 1949 , when it was used to help identify the victims of the great lakes liner noronic disaster in toronto , canada . 
plain film radiographs were taken of 79 of the 199 fatalities , and corresponding antemortem radiographs were obtained for 35 of these cases , providing an eventual positive identification in 24 of the most severely disfigured cases by radiology alone [ 2 ]  . 
due to acute disruption of the casualties , antemortem fractures were not of much evidentiary value , but congenital abnormalities and chronic conditions were of great value in several instances . 
four of the individuals were identified by abnormalities of the spinal column , seven by arthritis of the spine , one from arthritis of the knee and one by arthritis of the calcaneus , all of which were distinctive enough on radiographs to produce positive identifications . since then , the role of radiology in human identification and mass fatality examination has developed enormously . 
 technological advances , including the development of computed tomography ( ct ) and magnetic resonance 1 3 radiol med ( 2015 ) 120 : 866873 imaging ( mri ) , in combination with training and education have helped to unlock the true evidentiary value of these technologies for forensic investigations . 
radiology and forensic departments now work closely together , so much so that forensic radiology is considered a new sub - speciality in its own right and is a key component in any multidisciplinary team dealing with casualty identification [ 3 ]  . disaster victim identification ( dvi ) an incident is classified as a mass fatality incident ( mfi ) when it involves five or more casualties and is sub - divided into : major , mass or catastrophic , depending on the total quantity of victims . 
an mfi may be local , national or , more commonly these days , international based on the location of the incident and the country / countries of origin of the victims . 
human rights ( hr ) violations may also be considered to be mass disasters ; although they may occur over a larger geographical area and time [ 4 ]  . 
a permanent site , temporary or cbrn mortuary . for an mfi , victim identification is of primary importance , as investigators have a humanitarian and legal responsibility to identify each casualty , where possible , so that they can be returned to their next of kin [ 5 ]  . 
for example , aircraft and industrial incidents , terrorist attacks and natural disasters often present fragmentation , heat damage and commingling problems , which require a more extensive mortuary setup . the complexity of victim identification in the aftermath of an mfi can vary tremendously and depends on the context , number of fatalities , extent of body fragmentation , decay and the availability of antemortem reference material related to missing individuals . 
to ensure that bodies are identified as quickly and efficiently as possible , a multidisciplinary team is generally deployed to work simultaneously to increase the productivity of the identification process . 
this usually consists of police , pathology and odontology personnel , although with the recent trend in the use of pmct the radiologist is also becoming an integral part of the mortuary identification team . disaster victim identification ( dvi ) capability and standards are required to cover international as well as national incidents . 
to date , the international police organizations ( interpol ) resolution on dvi is the only internationally recognized legislation , which functions under international law , to specifically address this issue . 
they recommend that all 187 - member countries should adopt a common procedure for identifying victims in any type of disaster , regardless of its cause or scale [ 7 ]  . in 1984 , interpol published the first dvi manual . 
their aim was to provide information relating to mass disaster handling in general , and the identification process in particular , to increase the efficiency and effectiveness of dvi [ 7 ]  . 
the interpol dvi guide ( interpol - expertise / forensics / dvi - pages / dviguide ) assumes that postmortem intervention will be organized and describes the dvi process including three key steps . 
 these are recovery and examination of bodies to establish postmortem evidence from the deceased , search for antemortem information for possible victims and the reconciliation of antemortem and postmortem data [ 8 ]  . the interpol guidebook contains two separate specific forms for recording the antemortem ( am ) and postmortem ( pm ) information , to assist the identification process [ 5 ]  . 
these research groups are continually producing scientific data to support the introduction of pmct into the mortuary . identity excluded certainty that pm and am data sets are both too minimal to be conclusive . as well as comparative identification , reconstructive identifications can also be achieved by matching a set of pm classification criteria to a large population of am data to narrow the number of possible identities . 
likewise , internal examination may expose evidence of surgical procedures , including natural disease , prosthetics or evidence of previous trauma ; all of which may be exclusive to the individual [ 13 ]  . 
also known as a virtual autopsy , the concept of postmortem imaging developed its roots in israel in 1994 when it was first proposed that pmct could replace the need for an autopsy [ 23 ]  . in 2002 , the virtopsy group was established at the institute of legal medicine , university of berne , switzerland . 
 this group [ 24 ] , along with several other research groups [ 21 , 2527 ] , considered the possibility of using pmct to establish minimally invasive routine imaging methods in forensic pathology to supplement , or even replace , the current standard approach , as used in previous incidents such as the terrorist bombings in london in 2005 , involves moving fatalities through three separate radiological stations : fluoroscopy , to screen for potential contaminants or evidence prior to autopsy ; standard radiography , principally used for anthropological and pathological examination ; and dental radiography , for dental identification . 
this process requires the procurement and insulation of three different imaging modalities in a temporary mortuary , sufficient staff to operate them and subsequently a number of health and safety implications . 
for example , mobile fluoroscopy units require the operator to be positioned next to the body throughout the imaging process , to capture images when necessary as they move the machinery systematically along the length of the body . 
this surface investigation takes approximately 15 min and pathologists are normally responsible for interpreting and reporting the resulting radiological images , although they are often not specifically trained to do this . 
in addition , all of these imaging modalities normally need their own specific electrical power supply and a dry working environment , which presents a number of logistical problems in a temporary mortuary . using pmct has the potential to replace these three independent modalities , and therefore could improve issues relating to equipment sourcing , operational personnel and health and safety . 
 since the first radiologic identification nearly 90 years ago , radiology has been a key component in the identification process by comparing postmortem and antemortem information , on the assumption that each individual exhibits unique features [ 29 ]  . 
it has also been used to provide valuable supplementary information to help with the detection of 1 3 radiol med ( 2015 ) 120 : 866873 foreign bodies that may pose a hazard to on - site investigators , to uncover and pinpoint the exact location of material evidence and provide an image inventory of all recovered body parts that can be stored indefinitely ( for future reference ) and transferred easily to remote professionals . transporting bodies to clinical ct scanners following an mfi is possible , but can often create a number of logistical issues , particularly if the incident occurs in a remote area , a country that does not routinely use ct in general practice , or the disaster is so catastrophic that the medical infrastructure of the country is drastically affected . 
this led to rutty suggesting at numerous meetings in the united kingdom ( uk ) around 2004 that a truck - based mobile ct scanner could be deployed to the scene of an incident or temporary mortuary , instead of using clinical scanners as a potential solution to these logistical issues . 
these types of incidents require particular procedures and specialist equipment to minimize the potential contamination . the use of mobile pmct scanners in a forensic setting was first reported in japan [ 30 ]  . 
two years later in february 2006 , rutty and colleagues were the first group to implement the use of a mobile ct scanner in a small mfi [ 21 ]  . 
 as a result of this experience , this research group later developed a tele - radiology system for remote data reporting in mfis , which they termed the fimag system [ 26 ]  . 
a mobile ct scanner was deployed at the european union - funded , multi - national cbrn and conventional mortuary exercise , operation torch in 2008 , and the fimag system was internationally tested during operation hounslow in 2011 . 
during this operation , an on - site radiology team was able to report on the scans as they were being taken and the information was fed directly into the mortuary , either as a hard copy or live monitor feed into the dvi examination area . 
 pmct data were also sent to reporting teams in europe , scandinavia , japan , australia and south america . operation torch has been one of the only large - scale dvi simulation exercises to consider appropriate image reporting , secure data transfer and storage , an area that has previously received little attention . 
the data entry code was based on the national identification number system presented with the remains on the association of chief police officers ( acpo ) or interpol victim profile form ( vpf )  . 
encrypted raw dicom data were then sent from this hub via telephone line , 3g or satellite network using a virtual private network ( vpn ) to the forensic picture archiving system ( fpacs ) image router and web server . 
this method of secure data transfer should be used to maintain stringent judicial requirements . outside the uk , the virtopsy group has considered the benefits of mobile pmct as a mass fatality - screening tool and researched its ability to collect information to complete the interpol dvi forms [ 31 , 32 ]  . 
pmct played an integral role in the dvi of victims of the victorian bush fires , australia [ 22 , 34 , 35 ] , and has been used in modern military conflict areas for the examination of projectile - related injuries as well as vehicleand air - related incidents . potential role of pmct in dvi the current official dvi interpol form does not contain a specific pmct section , let alone a radiology part . 
this being said , some information would still need to be collected manually , such as an external inspection of the body and the removal of personal items , as pmct cannot clearly define words on labels , the inscriptions on rings or the natures of inked tattoos due to resolution limitations . a review of the most regularly used anthropological identification techniques , by brough et al . 
in a more recent publication [ 37 ] , the same authors suggested that it would also be possible to complete the majority of the current dvi interpol form using only pmct , an external examination ( including recovery and documentation of personal possessions ) , fingerprints and dna ( table 1 )  . 
in addition , personal effects , clothing , medical implants / interventions and natural internal disease that has been documented in an individuals medical history can be located for further inspection , using either 3d reconstructions or 2d mprs without the necessity for an invasive internal examination . 
pmct could be used to map the exact location of these items for rapid retrieval sections pmct could not complete b0 : checklist of operations for mortuary d5 ( 14 ) : fingerprint information e4 : dna information table 1 a summary of interpol requirements sections pmct could assist / complete b ( 22 ) : state of body b ( 22a ) : important id information c ( 2425 ) : clothing and footwear * c3 ( 2630 ) : personal effects * d1 ( 31 - 55 ) : physical descriptiona d4 ( described in 22 and or / 31 , 53 ) : body sketch e2 ( 7175 ) : medical conclusionsb e3 : skeletal inventory f1 ( 8385 ) : dental findings f2 ( 8691 ) : dental inventory g ( 92 ) : further information e1 ( 6065 ) : internal examination * clothing and footwear , personal effects ; pmct would be able to identify general items for inventory , but for more specific details , e.g. 
however , in scenarios where the bodies can be scanned in a sealed body bag to minimize contamination exposure , pmct would be able to map the exact location of these items for rapid retrieval a ( 33 ) except weight ; b ( 73 ) except samples taken 1 3 radiol med ( 2015 ) 120 : 866873 identification of unknown remains in an mfi , pmct could remove the necessity of an invasive examination . in addition , pmct dental reconstructions could be used in the same manner as traditional orthopantomograms ( opts ) for the estimation of age and identification of unique dental features , with the added advantage of producing a 3d dataset as opposed to a single 2d image . 
however , it is important to note that image artefacts can be produced from unremovable metal work or ( mercury based ) dental amalgam in fillings , which may limit pmcts evidentiary value , less common in a younger age group . 
artefacts include beam hardening where the density of structures are misrepresented by differential attenuation of x - rays by metal , and more significantly photon depletion where the high attenuation by metal reduces the beam intensity so drastically that a diagnostic image cannot be computed in that region , causing streaking and black areas . 
this can affect the precision of measurements used for various identification techniques , such as age estimation and comparison identifications . a more extensive investigation on a cellular level is not possible using pmct . 
this is a minimally invasive diagnostic technique that facilitates the fast and accurate collection of representative samples of organ tissue and body fluids through small punctures and has been around as long as histology [ 38 ]  . development of forensic imaging in dvi in 2012 , the dvi sub - group of the international society for forensic radiology and imaging ( isfri ) released a positional statement outlining the issues facing the field of forensic radiology , which included six key areas of development on which dedicated working groups would focus [ 39 ]  . 
this publication recommended that , where possible , a radiological examination should always form part of the dvi process and that the modality used would be dependent on the equipment available at the time and the individual requirements of each dvi scenario . 
the isfri membership suggested that the modalities used should include radiographs ( plain film , computed or digital radiography ) , fluoroscopy , computed tomography or dental radiography , either singularly or in combination . 
furthermore , they considered that although mri has been considered for postmortem imaging , its utility in dvi events is limited by additional cost , extended scan time and mobility implications and is therefore not considered suitable unless the only antemortem comparison image is mr . in may 2014 , a consensus document written on behalf of the members of isfri and supported by the international association of forensic radiographers ( iafr ) , regarding the use of pmct in dvi , recommended that it should be used for : ( 1 ) identifying the cause of , and contributory factors to , death ; ( 2 ) disaster victim identification ( dvi ) ; ( 3 ) identifying potential hazardous materials within the body ; ( 4 ) gathering evidence for criminal justice procedures [ 40 ]  . 
these protocols have been designed by the group to be applicable to both mobile ( lorry based ) and fixed site ct scanners and therefore include procedures for both at the scene of the incident or within a permanent or temporary mortuary . pmct reporting over the last decade , the frequency of pmct scanning has increased rapidly and therefore its role in dvi events has also increased . 
this presents the important questions of ( 1 ) whether pmct reporting should follow an official structured reporting format , or alternatively whether a free reporting format should be used [ 41 ] and , ( 2 ) who should be interpreting the data ? this might be dictated by legal requirements as set out by law and landmark court decisions . 
therefore , all data gathered , as well as caserelevant significant findings within any of the data ( including pmct data with reports of the presence as well as absence of relevant findings ) have to be explicitly reported . 
 without a structured reporting format in place , the readers of pmct currently use their judgment in what they want to report and how they want to formulate their written reports . 
should it be a radiologist with knowledge of forensic pathology or a forensic pathologist with knowledge of radiology ? or , should both professions work together to provide a collaborative report of the findings ? to ensure that pmct is considered for the next dvi interpol update , it is essential to develop an adequate pmct recording format , which includes an identification reporting section and to make clear suggestions regarding who should be reporting the data . in the event of a dvi , although it is possible to transfer large quantities of pmct data between different countries [ 21 ] , this process currently takes approximately 20 min per case ( or longer , if there are security measures , such as firewalls in place ) , requires a large computer memory and storage facility , and post - processing of the data can be labour intensive ( depending on the case )  . 
without language interpretation / translation storage requirements of ct data are far less problematic than whole body or tissue storagefrom both an ethical and practical standpoint ct is non - invasive , therefore virtual forensic procedures are likely to be culturally more acceptable an online , remotely accessible pmct database could be createdproviding researchers with an opportunity to improve traditional anthropoaccess to ct scanners may be limited , particularly those that are used for pmct scanning as well as clinical scanning equipment is expensive continuous excessive use of scanners can cause damage which is expensive to repair metal might cause artefacts ( particularly evident in the dentition ) not all pathologies that could potentially be used for identification by comparison with antemortem medical records can be detected dataset recording form , completed by a central investigator , which can be sent to numerous practitioners for independent analysis , could be of considerable benefit in dvi scenarios where time is of essence and victims must be identified accurately . 
a standard pmct reporting form would also ensure that an adequate amount of information about each case was recorded in a standard format ; for multiple practitioners , using numerous anthropological identification techniques to use remotely . future of forensic imaging and dvi as pmct is being increasingly accepted into autopsy practice , it is anticipated that it will , as rutty suggested nearly 10 years ago , become a significant , if not the main radiological examination modality for mfis . 
there will always remain the need for an external examination of the body , along with a dental examination , but as we move into a new era of dna technology , with the potential offered by next - generation sequencing ( ngs ) , pmct and ngs may become the principal technologies used in mfi investigations , as suggested by rutty and sajantila at the interpol dvi steering group meeting , lyon , 2014 . conflict of interest the authors declare that they have no conflict of interest . ethical standards for this type of study , formal consent is not required . 
fortunately , most of them are minor degree errors , or if serious , are found and corrected with sufficient promptness ; obviously , diagnostic errors become critical when misinterpretation or misidentification should significantly delay medical or surgical treatments . 
errors can be summarized into four main categories : observer errors , errors in interpretation , failure to suggest the next appropriate procedure , failure to communicate in a timely and a clinically appropriate manner . 
para - physiological and pathological pitfalls in neuroradiology include calcification and brain stones , pseudofractures , and enlargement of subarachnoid or epidural spaces , ventricular system abnormalities , vascular system abnormalities , intracranial lesions or pseudolesions , and finally neuroradiological emergencies . 
fortunately , most of them are minor degree errors , or , if serious , are found and corrected with sufficient promptness . errors should be distinguished into two categories , perceptual and cognitive : in perceptual errors abnormality is not perceived , and in cognitive errors the abnormality is perceived but misinterpreted [ 3 , 4 ]  . moreover , error does not equal negligence ; in fact negligence occurs when the degree of error exceeds an accepted standard . 
although human error is inevitable in medicine , including neuroradiology , it is important to distinguish medical errors from medical malpractice ; medical error is the failure of a planned action to be completed as intended ; medical malpractice is defined as a failure of the physician to exercise that degree of skill and knowledge commonly 1 3 796 radiol med ( 2015 ) 120 : 795801 applied under all the circumstances in the community , resulting in injury to the patient [ 3 ]  . in order to minimize the possibility of error , it is important to be aware of the various possible presentations of pathology , obtain clinical information , know current practice guidelines , review after interpreting a diagnostic study , suggest follow - up studies when appropriate , communicate significant abnormal findings appropriately and in a timely fashion directly with the treatment team . sources of errors in neuroradiology medical - legal literature divides missed radiologic findings into errors due to negligence and errors not due to negligence . 
 this error is due to incorrect interpretation of a malignant lesion as a normal structure after detection . there are many reasons why radiologists make errors in identifying and interpreting abnormalities . 
factors such as clinical history , presence or absence of previous studies , index of suspicion , the reading room environment , and the level of vigilance of the interpreter are various sources of error [ 6 ]  . failure to suggest the next appropriate procedure is an extremely important error . 
in fact , follow - up or additional diagnostic studies to clarify or confirm the impression should be suggested when appropriate to the neuroradiologists own judgment [ 7 ]  . errors in communication are the fourth most frequent allegation against radiologists in medical malpractice claims [ 9 ]  . 
moreover , important mistakes are the missed communication of findings that required urgent contact with the patients primary physician for possible change in treatment . workload can be a factor in increasing the likelihood of errors in radiology reporting [ 4 ] , as well as short experience of staff , inadequate equipment , inadequacy of clinical information , inappropriate expectations of the capability of a particular radiologic technique , unavailability of previous studies or reports for comparison . 
adoption of standard imaging protocols may reduce the likelihood of error or discrepancy in some areas of neuroradiology practice , especially in mri [ 6 , 7 , 11 ]  . moreover , diagnostic accuracy in neurology frequently depends on clinical assessment and neuroimaging interpretation . 
have analyzed neuroimaging discrepancy rates in reported findings between general 1 3 radiol med ( 2015 ) 120 : 795801 radiologists and neuroradiologists relative to patients from a district general hospital [ 12 ]  . 
incidental findings such as brain atrophy , pineal or arachnoid cysts , and differences in differential diagnoses were all categorized as secondary findings and differed in 21.5 % [ 12 ]  . in the literature many reports show low discrepancy rates between general or trainee radiologists and neuroradiologists [ 13 ]  . 
 [ 15 ] performed a quality control study of image interpretation discrepancies in academic neuroradiology and found 87.6 % agreements with the original report in 1000 randomly analyzed ct and mr studies . 
discrepancies were observed for neoplastic and vascular pathology . residents errors in emergency setting and in the first periods of the learning curve , as in residency , misdiagnosis / misinterpretation percentage should rise up . 
a recent study has evaluated common misinterpretations of head ct scans by radiology residents in a level i trauma center [ 16 ] : the overall misinterpretation rate was 41 % . 
 [ 17 ] showed that the period with the highest percentage of mistakes was between 0400 and 0800 , the last hours of the shift , which the authors attributed to fatigue . 
multiple previous studies found an association between rate of discrepancies and resident training level , with preliminary reports issued by first - year residents being more often discrepant [ 18 , 19 ]  . 
this finding is not surprising , as first - year residents are by definition less experienced . ct exams represent the modality of choice in the emergency room setting for on - call neuroradiology studies , and studies have shown low miss rates of significant lesions [ 18 ]  . 
mr imaging is going to be an expected level of radiology care for the diagnosis and treatment of emergency room patients ; therefore , it becomes imperative that on - call radiology residents in academic centers be trained to meet this emerging standard . for mr exams , filippi et al . 
discrepancies between the interpretations of radiology residents and the final reports of attending neuroradiologists were classified as either false - negative ( fn , failure to recognize abnormalities ) or false - positive ( fp , misinterpreting normal images as abnormal )  . 
analyzing this series , discrepancy rates between radiology residents and attending neuroradiologists on emergent mr imaging studies , including brain and spine mr examinations and neck and circle of willis mr angiograms , were low , and there was no adverse clinical outcome as a result of discrepant interpretations . paraphysiological and pathological pitfalls calcification and brain stones vascular or choroid plexus calcifications are frequently seen in the brain structures , commonly in the lateral ventricles but also in the fourth ventricle , and should not be confused with blood or even tumor . 
temporal horns calcifications are sometimes indistinguishable from intraparenchymal ones ; calcifications of the choroid plexus in the roof of the third ventricle or in the region of the foramen of monro may resemble colloid cysts or calcified neurocysticercosis [ 21 ]  . large intracranial calcifications are occasionally encountered in routine ct scans of the bra based on location , brain stones can be classified as extraor intraaxial . 
imaging findings combined with essential clinical information can help in narrowing the differential 1 3 798 radiol med ( 2015 ) 120 : 795801 diagnosis , determining disease state , and evaluating effect of therapy . 
certain mri sequences ( gradient echo t2 * and susceptibility - weighted imaging ) are considered adjunctive [ 22 ]  . pseudofractures and enlargement of subarachnoid or epidural spaces sutures , nerve canals can be interpreted as false images of pseudofracture ; the asymmetry of the jugular fossa or the internal auditory canal may suggest possible tumors [ 23 ]  . 
extra - axial lesions , particularly meningiomas , commonly show a broad dural base or a dural tail of enhancement [ 21 ] ; this may also occur in other extra - axial fig . 
eh axial t2 - weighted images : presence of a glial tumor in the same location , characterized by a non - homogeneous signal 1 3 radiol med ( 2015 ) 120 : 795801 fig . 
 ac axial t2 weighted , contrast - enhanced t1 weighted , diffusionweighted images : ring - enhancing , liquified lesion , characterized by restricted diffusion , associated with extensive peripheral vasogenic edema . 
df axial t2 weighted , contrast - enhanced t1 weighted , diffusion weighted images : ring - enhancing , colliquative lesion , characterized by elevated diffusion tumors , although less commonly . 
linear pachymeningeal ( dura - arachnoid ) enhancement occurs after surgery and with spontaneous intracranial hypotension ; leptomeningeal ( pia - arachnoid ) enhancement is present in meningitis and meningoencephalitis ; superficial gyral enhancement is seen after reperfusion in cerebral ischemia , during the healing phase of cerebral infarction , and with encephalitis ; nodular subcortical enhancement is typical for hematogenous dissemination and may be neoplastic ( metastases ) or infectious ( septic emboli )  . 
deeper lesions may form rings or affect the ventricular margins ; smooth and thin ring enhancement is typical of an organizing abscess or necrotic neoplasm [ 31 ]  . finally , technical deficiencies such as patient motion artifacts , beam hardening artifacts , position asymmetries or partial volume averaging effects may mislead the radiologist and create false images of pathology . 
pseudolesions in the brain parenchyma as the temporal lobe hypodensity or some posterior fossa abnormalities in the cerebellum may be related to beam hardening artifacts ; differential diagnosis should include cerebral contusions and white matter injuries . 
 the vermian pseudotumor is the visual effect of an hyperdense structure surrounded by the fourth ventricle and the paravermian cistern , which are hypodense structures [ 32 ]  . 1 3 800 radiol med ( 2015 ) 120 : 795801 trauma and neuroradiological emergencies error can increase the rate of mortality and morbidity in the managing of traumatized patients and other neuroradiological emergencies [ 33 ]  . 
in the cranial - cervical region , two frequent errors in the radiological procedure may result in a serious increase in morbidity and mortality : understaging of the supraaortic trunks lesions and overlooking the cause of the intraparenchymal hematomas of the bra the first type can be avoided by extending the study of the arterial chestabdominal phase to the neck , as the frequency of traumatic injuries in this vascular district is high enough ( 15 % ) , and with obviously serious consequences in terms of morbidity and mortality , to warrant assessment [ 34 ]  . 
in the second , an intraparenchymal hematoma in a polytraumatized patient is often indicative of either an arteriovenous malformation or the spontaneous bleeding of an intracranial aneuryssuch cases are best evaluated by integrating the pre - contrast study of the skull with a cerebral ctor mr - angiography [ 35 ]  . the management of cervical spine injuries remains complex and controversial . 
such injuries are much more common at the cranio - cervical junction ( 4050 % ) and at the cervicaldorsal transition [ 36 ]  . computed in 2009 , the american college of radiologists ( acr ) recommended multidetector tomography ( mdct ) with multiplanar reconstruction ( mpr ) as the method of choice in suspected spinal trauma , replacing traditional imaging studies for patients who show a suspicious clinical framework according to the criteria of nexus or the canadian cervical spine rules [ 237 ]  . how to reduce errors in neuroradiology diagnostic errors can be reduced by improvements both in individual knowledge and in organization . 
better system organization consists in improvements of working conditions and in the time available for reporting , of equipment modifications to prevent accidental error , in double reporting , and in regular dialogue between clinicians and radiologists [ 38 ]  . 
some departments have integrated peer review into their daily clinical workflow by providing previous interpretations with every new study and including a checkbox for the interpreting radiologists to indicate whether they agree with the previous interpretations and , if not , a text box to indicate why they disagree . 
 this system minimizes the time required of the reviewing radiologists [ 40 ]  . although a missed diagnosis or other forms of error may be the most feared event for a radiologist , it can also be one of the best opportunities for learning . 
learning from errors requires a critical appraisal of our own practice and the implementation of change to enhance performance levels . educational programs , morbidity meetings , and a comprehensive and respected root cause analysis process are important for decreasing the likelihood of future diagnostic errors . conclusion the main reason for studying medical errors is to try to prevent the retrospective analysis of cases in which an error is felt to have arisen has educational benefit , and an appreciation of the error along with the identification of its possible causal factors enables the appropriate modification such that in the future similar errors might be avoided . 
 although a missed diagnosis or other form of error may be the most feared event for a neuroradiologist , it can also be one of the best opportunities for learning . diagnostic errors fall into recurrent patterns . 
wherever errors are made , they should be seen as learning opportunities , not just individually , but corporately too : for neuroradiology and medical colleagues , radiology trainees , and students . identification and reduction of diagnostic error provides a measure of the efficacy of the healthcare system , as it reduces mortality , morbidity , length of hospital stay , and additional health care costs . compliance with ethical standards this article does not contain any studies with animals performed by any of the authors . 
in medical imaging , the line between the word error and misdiagnosis or discrepancy is very difficult to demarcate , mainly because the diagnostic process is not a binary relation and it is not always possible to establish if a pathological condition is present or not . 
the error in radiology is strongly related to the diagnostic process ; hence , it can be defined as a diagnostic error which represents the most common cause of medical malpractice suits against radiologists . 
secondly , some data coming from different countries were compared in order to highlight the most frequent causes leading to malpractice lawsuits in radiology and how the phenomenon of malpractice in this field is represented worldwide . keywords radiology diagnostic error error disclosure malpractice lawsuits * vittorio fineschi vfinesc@tin.it 1 department of anatomical , histological , forensic and orthopaedic sciences , sapienza university of rome , viale regina elena 336 , 00161 rome , italy 2 neuromed , istituto mediterraneo neurologico ( irccs ) , via atinense 18 , 86077 pozzilli , isernia , italy introduction the evolution of case law has reshaped the landscape of medical professional liability and it has contributed to an exponential growth of litigation , with significant economic impact on spending health . 
in medical imaging , the line between the word error and misdiagnosis or discrepancy is very difficult to demarcate , mainly because the diagnostic process is not a binary relation and it is not always possible to establish if a pathological condition is present or not [ 1 ]  . 
median payment awards varied by 14 - fold from maine ( $350000 ) to colorado ( $24105 ) , while mean payments varied ninefold from oregon ( $715707 ) to nebraska ( $74373 ) [ 3 ]  . 
therefore , what strongly emerges is that an error in radiology is mainly related to the diagnostic process ; hence , it can be defined as a diagnostic error which represents the most common cause of medical malpractice suits against radiologists . 
 the modern relationship between radiologist and patient needs to consider the right to a timely diagnosis and to receive as much information as possible , until to error disclosure / apology process [ 4 ]  . 1 3 780 radiol med ( 2015 ) 120 : 779784 the first question to be placed is how errors committed in radiology can be classified ; moreover , the authors will try to establish their impact and prevalence . the second aim of the paper is to compare data coming from different countries in order to highlight the most frequent causes leading to malpractice lawsuits in radiology and how the phenomenon of malpractice in this field is represented worldwide . the diagnostic error in radiology the term error has been defined in different ways . 
reason considers an error to have happened when a desired result is not reached [ 5 ] , excluding the intervention of chance , while merry and mccall smith focus on the intention rather than the result in order to define the term , since some errors do not change the result unfavorably [ 6 ]  . 
according to graber [ 7 ] , a diagnostic error can be expressed as a diagnosis that is missed , wrong , or delayed as detected by some subsequent definitive test or finding . different parameters can be used in order to classify the error ; green categorized errors in three groups as follows : intentional , perceptual , and errors of execution [ 8 ]  . 
perceptual error is the most common in radiology and it actually consists in three elements : adequate knowledge in order to be able to investigate an anomaly , having perceived it and finally making the judgment as to whether it is a pathological lesion , a normal variant , or an artifact . 
the causes of such failure , although being extensively investigated , remain part of a human factor extremely difficult to eliminate [ 9 ]  . the recognition of the error in radiology has a long history and one of the first studies to evaluate it dates back to 1949 by garland [ 10 ] , but the first difficult question to be addressed is if the term error is suitable for diagnostic radiology ; brady et al . 
 [ 1 ] consider more appropriate to talk about discrepancy rather than error , because the latter indicates a mistake , namely a wrong interpretation of an image in this field . 
however , it is necessary to take into consideration the subjectivity in the interpretation of the radiological image , therefore , the radiologist makes an error if he does not reach the same conclusions that a group of experts in this field would reach . 
the types of errors were classified into table 1 types of errors in radiology according to the classification of mccreadie and oliver [ 11 ] poor image interpretation ( false positive , false negative , misclassificatechnical error ( poor technique or procedural complication ) tion ) communication errors three categories , and are summarized in table 1 ; the results obtained allowed the authors of this study to identify 256 errors in 222 patients . the 88 % of errors ( 225 ) were due to poor image interpretation ( 14 false positive , 155 false negative , 56 misclassification )  . 
moreover , numerous repetitive errors during ct reporting were detected . the conclusions reached by mccreadie and oliver [ 11 ] can be summed up in the following points : error is frequently found in relation to the examination of radiological images . the majority of errors involve image interpretation , but a significant proportion results from departmental miscommunication . most of the errors are false - negative interpretations and occur during interpretation of ct examinations . frequent false - negative ct errors include failure to appreciate unexpected bowel or pancreatic malignancy , incidental pulmonary emboli , abnormality of vascular structures , bone lesions , omental disease , incidental abnormality found on targeted examinations or lesions on the periphery of the field of view . finally , it is important to highlight possible sources of errors ; in this regard , renfrew and colleagues [ 12 ] in reviewing and classifying errors in 182 cases distinguished sources of errors in causes specific to the radiologist and other causes due to system issues ; a graphic representation of this dichotomy is reported in fig . 
 [ 13 ] , who conducted a nationwide study in order to determine the most frequent motive of medical malpractice suits against radiologists in us , error in diagnosis is indisputably the most common reason 1 3 radiol med ( 2015 ) 120 : 779784 fig . 
1 sources of errors in causes specific to the radiologist and other causes due to system issues ; a graphic representation of this dichotomy is here reported ( 14.83 claims per 1000 person - years ) for a malpractice suit initiation against radiologists . 
lastly , failure to recommend additional examinations was reported as uncommon [ 13 ]  . almost a thousand 990 insurance claims of radiologists in italy between 1990 and 2004 were evaluated [ 14 ]  . 
it is worth pointing out that in approximately 6 % of all cases , radiologists were often considered to be defendants along with medical doctors , in case of patients death [ 14 ]  . a study of magnavita et al . 
in 21 cases ( 21.4 % ) , the event induced the death of patient . another study conducted in england [ 9 ] , evaluating data regarding claims against radiologists between 1995 and 2006 , found a total of 440 cases . 
a claim for a delayed diagnosis of an individual cancer and multiple missed diagnosis of breast cancer led to a pay - out of 300 000 and 464 000 , respectively [ 9 ]  . as described in a dutch study [ 16 ] , interpretation of screening mammography is considered as one of the most difficult tasks in radiology . 
however , due to the high expectation of the public concerning the efficacy of the latest screening techniques , diagnostic errors can have major legal consequences for the screening radiologist [ 16 ]  . according to traina [ 17 ] , currently , malpractice claims against physicians in italy account for 15 , 000 per year . 
 healthcare costs are likely to increase since italian physicians increasingly practice defensive medicine , thereby over utilizing resources aiming to underline carefulness , diligence , and skill to protect themselves from potential litigation , rather than targeting patient benefit . the following question which was raised by berlin in 1977 [ 18 ] does the missed radiographic diagnosis constitute malpractice ? summarizes the main problem of malpractice lawsuits . 
b second radiological investigation after 2 weeks : left leg : non - recent proximal third fibula fracture in the diaphyseal region , with initial repair considered as over and done with after the first tort reform in usa , it may still be assumed valid because of the ambiguous effects of tort reformation in medical practice . 
nevertheless this may not be so apparent for judges , lawyers , and patients who although aware of the so - called human factor often cannot distinguish between error and malpractice because of the lack of the right elements [ 19 ]  . caldwell and seamone [ 20 ] approached this issue claiming that judges should concentrate on proof of competence habits of the radiologist , to what extent the radiologist showed safe practicing habits and the usage of proper techniques . discussion and concluding remarks the following question does a missed radiologic diagnosis constitutes malpractice ? has confused not only radiologists and patients but also judges , jurors , and attorneys for more than a century , and it is more likely that this question will not be determined in the near future . 
errors are not likely to be considerably reduced unless having perfect diagnostic tests and perfect observers [ 21 ] , which is not probable to occur [ 22 ]  . patients continue initiating malpractice suit against radiologists , however , the following statements [ 23 ] can on occasion be sufficiently persuasive to lead the judgment in favor of the defendant radiologist , when claimed in the courtroom : some radiologic abnormalities appear inconspicuous . statistics showing the prevalence of errors occurred by radiologists during routine practice . evidence illustrating that the defendant radiologist was prudent and careful . expert witness stating that is impossible for any professional to adhere to a standard of perfection . as proposed by lee et al . 
an individualcentered approach concentrates on the individual who 1 3 radiol med ( 2015 ) 120 : 779784 perpetrates the error , and adopts countermeasures aimed at that person , including disciplinary measures , naming , shaming and blaming [ 2 ]  . 
the systemcentered approach accepts the fact that humans are liable to error and the inevitability of errors , and seeks to address the causes contributed to these errors , which is in accordance with the hippocrates quote : i would give great praise to the physician whose mistakes are small , for perfect accuracy is seldom to be seen . 
in the latest case what matters more is why and how defenses failed and what factors contributed to the creation of the conditions in which the error occurred and less who made the error [ 2 ]  . anyway , as it has been stated , litigation prevention largely depends on both reducing the rate of medical error and providing the patient with correct and coherent information [ 15 ]  . 
the principal factors causing adverse events or errors are said to be the scarce amount of time at the disposal of health practitioners for their patients , work overload , stress and tiredness experienced by the medical staff , miscommunication between members of the medical team , and shortage of personnel . 
the question is will apologizing increase or decrease the likelihood of a malpractice lawsuit ? anyone who knows whether it is yes or no , you should definitely refute [ 27 ]  . the clinical risk manager plays a key role in this scheme . 
thanks to this non - invasive scientific revolution , some classifications and staging systems , first based on dry bone analysis , can be applied to cadavers with no need for specific preparation , as well as to living persons . 
 virtual anthropology may also help the forensic pathologist to estimate a deceased persons age at death , which together with sex , geographical origin and stature , is one of the important features determining a biological profile used in reconstructive identification . 
for this forensic purpose , the radiological tools used are multislice computed tomography and , more recently , x - ray free imaging techniques such as magnetic resonance imaging and ultrasound investigations . 
saint - martin service de mdecine lgale , hpital trousseau , avenue de la rpublique , 37170 chambray - ls - tours , france keywords age estimation virtual anthropology radiographs multislice computed tomography magnetic resonance imaging introduction virtual anthropology consists of the introduction of modern slice imaging to anthropology [ 1 ]  . 
thanks to this non - invasive scientific revolution , some classifications that were first created on the basis of dry bone examination can be used in cadavers , with no particular soft tissue removal or bone preparation . 
radiology may also be helpful for the forensic pathologist to estimate the age at death of a deceased person , as age , together with sex , geographical origin and stature , is one of the important features determining a biological profile used in reconstructive identification [ 3 ]  . 
the various radiological tools , multislice computed tomography ( msct ) or multi - detector computed tomography ( mdct ) , as well as x - ray free techniques such as magnetic resonance imaging ( mri ) and ultrasound ( us ) investigations , are presented and discussed in this article . which kind of age are we talking about ? radiological images merely reflect biological age , which is subject to inter - individual variations [ 2 ]  . 
this is not always related to chronological , official or administrative age , and is subject to 1 3 radiol med ( 2015 ) 120 : 874886 inter - individual variations . 
 however , there may be differences between chronological and biological ages , in either direction , that can lead to over or under - estimation of chronological age [ 3 ]  . 
in deceased persons , estimated age at death corresponds to the time interval between birth and death , which is identical to the chronological age estimated in living individuals in clinical practice and which corresponds to the time interval between birth and the day of the investigation . 
of course , in cases of juveniles when only bones are preserved without any soft tissues , or when the state of preservation is poor , sex cannot be determined . age assessment may also be crucial in some judicial and administrative proceedings . 
in consequence , medical examiners , forensic odontologists , forensic anthropologist , who are professionals commonly involved in age estimation in both cadaver and the living may be called upon by the authorities to estimate the age of living persons requesting asylum and claiming to be younger than , for example , 18 years old , which in france is the age at which they are liable to be returned to their country of origforensic age estimation is also used to determine whether a suspected offender is subject to juvenile or adult criminal law . 
according to the guidelines published by the international study group on forensic age diagnostics , also called agfad ( arbeitsgemeinschaft fr forensische altersdiagnostik ) , age estimation in living individuals should consist of a physical examination , a radiograph of the left hand , and a dental examination . 
when necessary , ideally computed tomography of the clavicles may be performed [ 8 , 9 ]  . xray free imaging techniques when assessing age for forensic purposes , the physician should always keep in mind the need to reduce exposure to radiation as much as possible . 
agfad recommends radiographs and a chest ct scan in some cases ; however , these imaging procedures are performed in young adults without direct or indirect therapeutic or diagnostic medical benefit . 
 a hand radiograph involves a radiation dose of less than 0.1 microsieverts , an orthopantomogram 26 microsieverts and a clavicle ct scan a dose of 600800 microsieverts [ 10 ]  . 
bearing this in mind , non - invasive imaging procedures such as ultrasound examination ( us ) and magnetic resonance imaging ( mri ) have recently been applied to minimize radiation exposure of the individual examined [ 1115 ]  . 
it is because of the need to compare the results with those of previous plain x - ray studies that anatomical areas such as the sternal end of the clavicle , the hand and wrist , and the iliac crest have been studied . ultrasonography ultrasonography has the advantage of being readily accessible in hospitals and of being less costly than mri . 
ultrasonography showed a good correlation with the greulich and pyle method in the first 6 years of life , but unfortunately there has been no study with older children and young adults [ 17 ]  . 
like the greulich and pyle method , ultrasonography of the radial epiphysis appears to be particularly accurate up to the 14 - year - old threshold [ 14 ]  . the medial end of the clavicle was the subject of two main studies , using a 4 - stage classification created for radiography [ 20 , 21 ]  . 
the second study , using ultrasonography , showed a confusion between the first stage ( no fusion at all ) and the last stage ( complete union ) , because the ultrasound probe was not adequate to cover the whole sternal end clavicle metaphysis , leading to artifactual errors [ 20 , 21 ]  . 1 3 876 radiol med ( 2015 ) 120 : 874886 iliac crest examination yielded similar results with ultrasound and with plain x - rays , and was determined as a good method for the 14and 16 - year - old thresholds [ 22 ]  . 
with regard to the clavicle , some difficulties may arise in distinguishing between partial and complete fusion , especially with overweight individuals [ 23 ]  . magnetic resonance imaging ( mri ) mri is particularly suited to examination of the growth plate , and especially the metaphysealepiphyseal junction , which appears as a more or less complete gap between the metaphysis and epiphysis depending on the state of union . 
mri is a cross - sectional technique where thin slices are evaluated , generating more information and eliminating the disadvantage of superposition as seen in plain radiographs [ 24 ]  . 
compared with plain x - rays , mri shows an earlier age at the beginning of the fusion process and an older age of complete fusion . most mri studies focusing on bone age assessment use t1 - weighted sequences which provide a good indirect imaging of the bone and provide anatomical information [ 13 , 25 ]  . 
one study used fast spin - echo proton density - weighted images , showing a different appearance of the growth plate compared with t1 - weighted sequences [ 13 , 25 , 26 ]  . mri has been used to study the wrist in a specific context [ 2729 ]  . 
in 2003 , the federation internationale de football association ( fifa ) noted a discrepancy between the stated age of the participants in agerelated competitions open to individuals aged under 17 or 18 years old , and their physical appearance . 
a 6 - stage classification was used to analyse the length of epiphysealmetaphyseal union of the distal epiphysis of the radius in 14to 19 - year - old boys on t1 - weighted mr scans . 
in 2009 , several coaches changed more than half of their players before a competition for players aged under 17 . the sternal end of the clavicle was studied by mri using a 5 - stage classification previously tested on radiographs and ct scans . 
the results indicated that complete fusion occurred between the ages of 16 and 23 , but acquisition time ( 90180 min ) was too long for tests on living individuals . 
but it is one of the two existing markers of the 18 - year - old threshold , with fusion of at least twothirds of the sternal end of the clavicle on ct scan [ 32 ]  . other anatomical areas have been studied , such as the iliac crest in male football players , the distal tibial epiphysis and the calcaneum [ 13 , 26 , 33 , 34 ]  . 
bayesian predictive probabilities were used to assess the usefulness of ankle and foot analysis for the 18 - year - old threshold and showed excellent results for individuals over the age of majority ( over 90 % of correct estimations ) , but risks of errors in minors ( especially females , with more than 20 % of incorrect estimations ) [ 34 ]  . rather than ultrasonography , mri appears to be the most appropriate non - invasive imaging procedure for forensic age estimation . 
it may be possible to improve inter - observer reliability , as variations of grey levels within the epiphysealmetaphyseal junction have led to the development of an automated method with promising results , although it is not yet possible to use this method alone in forensic age estimation [ 35 ]  . 
left image : femoral ossification stage i with continuous horizontal cartilage signal intensity present between the metaphysis and the epiphysis , stripe - like , with a thickness greater than 1.5 mm and a multilaminar appearance ( box )  . 
 tibial ossification stage ii , with continuous horizontal linear cartilage signal intensity present between the metaphysis and the epiphysis , with a thickness greater than 1.5 mm , with increased signal intensity but without a multilaminar appearance ( circle )  . 
middle image : femoral ossification stage iii , continuous horizontal linear cartilage signal intensity present between the metaphysis and the epiphysis , with a thickness less than 1.5 mm , with increased signal intensity ( box )  . 
tibial ossification stage iv , discontinuous horizontal linear cartilage signal intensity present between the metaphysis and the epiphysis , with a thickness less than 1.5 mm , with discontinuous increased signal intensity ( circle )  . 
a thin line , similar to an epiphyseal scar , may persist radiographic and msct possibilities in bone age estimation in thanatology , msct can respond to a variety of anthropological aims : identification of lesions , comparative identification , and reconstructive identification of deceased persons . 
furthermore , after acquisition , the reconstruction stage is critical , with appropriate choice of slice thickness ( most of time millimetric ) and filters ( the most useful for study of the bone is the hard or bone filter )  . 
it contains reference images of male and female standards of the left wrist and hand , from birth till 18 years old for females and 19 years old for males . 
right image : coronal mpr reconstruction of the right wrist of a natural female mummy showing complete bone maturation , with an epiphyseal scar visible at the distal extremity of the ulna and radius ( arrows ) 1 3 radiol med ( 2015 ) 120 : 874886 graph of the subject with the nearest matching reference radiographs in the atlas . 
 although very often neglected , this is the most important part of the atlas , as it makes it possible to express results with a confidence interval . other atlases exist for different anatomical regions , such as the ankle , hip and knee [ 2 , 41 ]  . 
this method is based on the level of maturity of 20 selected regions of interest ( roi ) in specific bones of the wrist and hand in each age population [ 42 ]  . 
the sample consisted in scottish children , with radiographs performed around 1950 . some software programmes have been developed for elbow and wrist evaluation [ 43 , 44 ]  . synchondrosis closure : studies of time of closure of the spheno - occipital synchondrosis showed fusion was well under way by the age of 15 years and complete by 17 years . 
this age marker has a limited value for estimation around the age of 18 years [ 45 ]  . metric methods : an important point regarding all metric studies is that the osteometric measurements must be repeatable and there must be no significant difference between traditional and msct osteometric measurements [ 46 , 47 ]  . 
right image : stage 5 : the ossification centre is ossified , with a fully ossified epiphyseal cartilage and no visible epiphyseal scar focus on the clavicle : the clavicle has a special place in age assessment . 
during adolescence , a secondary epiphyseal ossification centre appears at the medial end of the clavicle that results in growth and remodelling of the bone , until complete fusion which occurs at approximately 22 years old . 
most of the articles are based on studies of german samples . although radiographs may be useful , it has been pointed out that the lack of standardized techniques and reference values makes interpretation difficult , with weak intraand inter - observer variabilities [ 52 ]  . 
consequently , the authors stated that plain x - rays of the clavicle should not be performed . the first publications on msct examinations also had methodological limitations : mix of sexes , mixed laterality , different slice thicknesses [ 5355 ]  . 
the initial staging 1 3 880 radiol med ( 2015 ) 120 : 874886 system had 4 stages , which were increased to 5 [ 32 , 56 ]  . 
currently , some methodological and practical points should be noted : slice thickness should be 1 mm [ 57 ]  . a hard filter must be used for acquisition and reconstruction must be done with a bone filter , for optimal bone analysis . 1 3 radiol med ( 2015 ) 120 : 874886 coronal mpr reconstructions may be helpful . 
classically , skeletal maturity is reached during the second decade of life , or at age 30 . the anthropological use of msct principally relies either on specific msct criteria and characteristics , or on the transposition of techniques applied on dry bones in physical anthropology [ 47 , 60 , 61 ]  . 
 it is not possible to cite all the different methods transposed , but the most important and the most often used are the appearance of the right fourth rib according to the iscan classification , and the auricular surface according to lovejoys classification [ 62 , 63 ]  . 
some pertinent results have been shown , such as a significant positive correlation between the length of the pubic bone and age , and the usefulness of grey - level histograms [ 66 ]  . 
some other methods defined with msct may also be helpful , such as the appearance of the trabecular bone of the auricular surface , the right first rib and the clavicle [ 54 , 55 , 62 , 67 ]  . 
3d vrt mode of the pubic symphysis ( upper left image ) , and 2d frontal mpr ( upper right image ) : stage i , suchey and brooks classification . 
one of the most likely explanations is that the development of all the deciduous dentition and part of the permanent dentition takes place before birth in a relatively protected environment whereas skeletal growth and development , although having a strong genetic basis , are influenced for a longer time by external factors such as nutrition and disease [ 3 ]  . in the foetus , the height of deciduous teeth 51 and 61 has been shown to be useful for age estimation , using a regression formula and giving an excellent correlation with foetal age [ 70 ]  . the first method described took the entire dentition into account , using an atlas [ 4 , 71 ]  . 
they cannot all be cited , but they focus on temporal changes of the crown , root , and apex of the teeth : analysis of specific teeth : moorrees [ 7274 ]  . 
the sample used by moorrees consisted in american individuals . derivation of a composite score established by demirjian on mandibular left teeth [ 7577 ] and adapted by willems [ 78 , 79 ]  . 
the sample used by demirjian was canadian children , and by willems was belgian . metric study , described by cameriere , with measurement of the open apices in teeth [ 80 ]  . 
dental age was estimated at between 7 and 8.8 years old using the moorrees technique , 10 years old 2.5 years using the ubelaker atlas , between 8 and 10 years old using the demirjian technique , and 9.5 years old using the willems technique . 
 the development of each tooth can be studied or dental restoration work can be demonstrated by generating oblique mpr or mip slices . discussion forensic age estimation has well - known limitations that have been widely discussed in the literature . 
the main limitation is that the reference methods applied to individuals living in european countries with high socioeconomic status , such as the greulich and pyle atlas or the tanner and whitehouse method for the wrist and hand , were developed in populations with low socioeconomic status . 
in individuals with delayed development as a consequence of undernourishment or other factors related to low socioeconomic status , age is most likely to be underestimated [ 6 ]  . 
 from a legal perspective , this would not result in a disadvantageous situation for individuals undergoing criminal proceedings and would be ethically acceptable . another limitation of forensic age estimation is that it is not possible to compare results obtained with different imaging procedures . 
 for example , higher magnetic field strengths may contribute to improve the signal - to - noise ratio , and potentially improving the quality of the images [ 13 , 25 ]  . compared with other imaging modalities , mri offers an important range of potential targeted contrast optimization [ 13 , 25 ]  . 
however , as no standard values for specific tissues exist and details of the tissue composition 1 3 884 radiol med ( 2015 ) 120 : 874886 of the maturing epiphyseal plate which provide the contrast are not reliably known , the finding of the different studies using different mri weightings cannot be easily compared . 
 furthermore , for these different mri explorations , the staging systems may also be different , rending the results of the different studies not comparable to each other [ 12 ]  . 
it seems consequently crucial to the further studies to be consensual concerting the different mri technical parameters . it is also difficult to determine the advantages of mri and ultrasonography in terms of accuracy regarding different age thresholds compared with plain x - rays or ct scans , methods that have been the subject of multiple studies among different populations . 
for the time being , we can only carry out further studies to confirm the useful results of examination of the hand / wrist , knee or clavicle . concerning the various methods derived from anthropology , the forensic radiologist needs to be aware of the limitations of these methods and to know the different average ages , standard deviations of the state variables used and intraand inter - observer variabilities , and should present the results in terms of probability [ 1 ]  . 
an important point to be remembered is that most estimation methods tend to overestimate age at death in younger individuals and to underestimate it in older individualsa phenomenon previously observed in a vast array of age estimation techniques [ 84 , 85 ]  . 
he attributed it to the particular age distribution of the reference sample used to construct any age estimation methodology , but it has been suggested that this error is , to a degree , the result of the statistical procedure used to estimate chronological age from biological age predictors , viz . 
the attraction results from combining individual estimates into an age structure for a given population , in which case they tend to accumulate in the middle range . although most of the presented criteria appear intended for postmortem use , clinical use is potentially possible . 
unfortunately , it is quite impossible to compare results of dry bone studies with x - rays , msct , mri or ultrasonographic examinations , because each of these methods has its own limitations and is based on exclusive specific criteria , visualized only by a single technique . 
it is clear that technology must be used to overcome the fact that age estimation , whatever the technique used , presents mostly identical limitations due mainly to the population of reference . msct and mri enable use not only in living patients , but also in the deceased . 
post - mortem changes in the vascular system and the absence of blood flow lead to specific problems that have to be considered for the performance of post - mortem angiography . 
in addition , interpreting the images is challenging due to technique - related and post - mortem artefacts that have to be known and that are specific for each applied technique . 
although the idea of injecting contrast media is old , classic methods are not simply transferable to modern radiological techniques in forensic medicine , as they are mostly dedicated to single - organ studies or applicable only shortly after death . 
with the introduction of modern imaging techniques , such as post - mortem computed tomography ( pmct ) and post - mortem magnetic resonance ( pmmr ) , to forensic death investigations , intensive research started to explore their advantages and limitations compared to conventional autopsy . 
this article gives an overview of the problems in post - mortem contrast media application , the various classic and modern * silke grabherr silke.grabherr@chuv.ch 1 university center of legal medicine lausanne - geneva , university hospital of lausanne , chemin de la vulliette 4 , 1000 lausanne 25 , switzerland 2 department of diagnostic and interventional radiology , university hospital of lausanne , rue du bugnon 46 , 1011 lausanne , switzerland techniques , and the issues to consider by using different media . keywords post - mortem computed tomography postmortem magnetic resonance imaging post - mortem angiography contrast media virtual autopsy forensic radiology introduction visualising the vascular system has always been a challenge in medicine . 
simple dissection techniques on cadavers were not sufficient for understanding the complex anatomy of this systethus , the idea was born to inject substances into the hollow vessels and produce so - called vascular casts [ 1 , 2 ]  . 
at that time , the technique of post - mortem angiography ( pma ) , the injection of radio - opaque contrast media into the vascular system of organs or bodies , was born . during the last two decades , the research field of postmortem radiology has grown considerably . 
the application of modern cross - sectional imaging techniques for forensic death investigations has been introduced in medico - legal centres all over the world , especially for multidetector computed tomography ( mdct ) and occasionally magnetic resonance imaging ( mri )  . 
since the first report of postmortem computed tomography ( pmct ) in 1983 [ 3 ] , the 1 3 radiol med ( 2015 ) 120 : 824834 number of examinations has increased significantly [ 413 ]  . 
 the advantages of pmct and post - mortem mri ( pmmr ) are evident , as they represent a possibility of documenting the interior of a body and serving as proof in medico - legal investigations [ 14 ]  . 
though pmct represents the best way to visualise the skeletal system [ 11 , 15 ] and mri being an excellent tool for investigating organ parenchyma and soft tissue [ 16 ] , none of these techniques are ideally suited for vascular diagnosis . 
this development mirrors clinical practice , in which ct - angiography ( cta ) is the most widely used method for the detection and localisation of clinically active haemorrhages of unknown origin [ 17 ]  . 
cta is also an excellent method for assessing acute and chronic coronary artery disease [ 18 ] , as it allows investigation of the arterial lumen and vascular wall diseases . as most of the classic methods of pma are only applicable to isolated organs , they were not fit to be reintroduced into modern post - mortem imaging . 
also , techniques usually used in clinical angiography are not simply transferable to post - mortem applications , as no vascular circulation is present and hydrosoluble contrast media diffuses rapidly out of the vascular lumen of the deceased . 
this article gives an overview of pma , the existing types of contrast agents , and the modern pma techniques available today . classic pma methods pma boomed during the first half of the twentieth century . 
 unfortunately , most of this knowledge has been lost , and from the hundreds of techniques that have been used , only a few are still used in the twenty first century . as recently proposed [ 2 ] , the techniques can be divided into six groups according to the nature of the injected material : ( 1 ) vascular casts , ( 2 ) corpuscular preparations in gelatine or agar , ( 3 ) corpuscular preparations in aqueous solution , ( 4 ) hydrosoluble preparations , ( 5 ) oily liquids , and ( 6 ) miscellaneous . 
corpuscular preparations consist of a corpuscular radiopaque material , which is usually soluble in water , and they can be mixed with gelatine or agar , allowing hardening after cooling , a technique originally used for histological sections . 
oily liquids were mostly used for perfusion studies , as they remain mostly intravascular , a fact that had already been recognised in 1968 by barmayer , who perfused coronary arteries with a mixture of diesel and paraffin oil to measure their flow capacity [ 20 ]  . 
at the zenith of classic pma ( end of nineteenth and beginning of twentieth century ) , hundreds of injection materials were used to render the vascular system visible for either macroscopic or radiological techniques , mostly for a combination of both . 
anatomists and other researchers have created their own injection mixtures , some of them still preserved in schoenmackers paper [ 1 ] , but most of them are probably lost forever . although the classic techniques are not the ones applied today , there are many things that we can learn from them in combination with modern post - mortem imaging . 
to develop techniques , new contrast agents , new perfusion liquids , and devices for modern pma , the information contained in the classic literature is essential to avoid unnecessary trials and to choose the best basic material and approach . contrast media to perform pma , the simple injection of contrast agent as done in clinical radiology is not sufficient . 
due to the cessation of intravascular circulation , haemostasis , agonal procedures , and post - mortem changes , most of the vascular system is empty after death , sometimes partly filled with post - mortem blood clots or gas [ 22 ]  . 
with increasing post - mortem delay , the permeability of the vascular wall increases , making it necessary to find a specific contrast agent that produces good vascular contrast without too many 1 3 826 radiol med ( 2015 ) 120 : 824834 fig . 
1 demonstration of the behaviour of different liquids in the vascular syste a due to post - mortem changes , the vascular wall becomes porous , especially due to changes in the endothelium , leading to leakage of hydrosoluble liquids throughout the vessel wall . 
thus , clinical aqueous contrast agents may produce sufficient quality directly after death , but they are not suited for pma at higher post - mortem intervals . fuelled by the introduction of mdct into post - mortem investigations and the goal to enhance pmct with contrast agent , new research aims to combine pma with pmct into post - mortem ct - angiography ( pmcta )  . 
two different approaches have been used : one using aqueous liquids and one using oily liquids . aqueous liquids although widely used in clinical radiology , hydrosoluble contrast agents face challenges in pma . 
this effect is well known , and even exploited , as in embalming procedures [ 25 , 26 ] where the increase of turgescence of the soft tissue indicates successful embalming . 
 although the easy injection and availability of aqueous contrast solutions ( mostly expired clinical contrast agents ) are an advantage , their use for whole - body pmcta is limited . 
today , their use in pma is limited to specific techniques , such as targeted angiography of the coronary arteries [ 30 , 31 ] , in which extravasation plays a less important role because only one organ is perfused , or directly after death for pma using cardiac massage [ 32 , 33 ]  . aqueous liquids mixed with polyethylene glycol ( hyperosmolar mixture ) to limit extravascular diffusion of aqueous liquids , jackowski et al . 
only a few studies with small numbers of human and animal corpses or organs have shown the possible use of such a contrast agent mixture [ 29 , 34 , 35 ]  . 
 [ 35 ] compared this mixture to an oily mixture in 10 human cadavers and concluded that the peg solution was advantageous due to tissue enhancement similar to clinical radiology . 
he also recognised that the aqueous mixture produces less extravasation in the pancreatic and gastric mucosa than the oily mixture , though the authors used low - viscosity oil , which has never been applied in another study . 
also , the contrast agent mixing with blood can be a problem , as quantifying the volume of a vital haemorrhage after pmcta is no longer possible . oily contrast agent mixture the fact that oily liquids mostly remain intravascular and occlude microcapillaries limits extravasation into the surrounding tissue and renders them useful for pma . 
by using perfusion with warm paraffin oil , percutaneous catheterisation can be performed and as an example , a newly developed self - expanding aortic valve can be delivered to the correct place [ 39 ]  . 
an initial feasibility study performed on an animal model showed the potential of the concept with the use of diesel oil as a perfusate and a roller pump as the perfusion device [ 24 ]  . 
if the viscosity is too low , artefactual extravasation is observed , especially in regions of so - called locus minoris resistentiae [ 24 ] , meaning regions with early bacterial decomposition and autolytic activities , such as the gastro - intestinal tract . 
the angiofil / paraffin oil mixture used for multiphase pmcta ( mpmcta ) is an example of a good working mixture [ 23 ]  . regardless of the contrast media or perfusate that is injected , they have consequences , as they can potentially alter the composition of fluid - based biological samples and interfere with specific post - mortem investigations . 
 in addition , water - soluble contrast agents will mix with the remaining blood , precluding the possibility of separating the two liquids during autopsy and the extravasated blood cannot be quantified . 
 the available studies pertain exclusively to mpmcta and tca and their influence on toxicology [ 41 , 42 ] , biochemistry [ 43 ] , microbiology [ 44 ] , genetics [ 45 ] , histology , and fatty embolism evaluation [ 46 , 47 ]  . 
this may be due to the fact that ct scanners are widely available , data acquisition is rapid , and the maintenance costs are affordable for some institutes of legal medicine . 
2 whole - body pmcta allows visualization of the vascular system of the head , thorax , and abdomen and twoand three - dimensional reconstructions radiol med ( 2015 ) 120 : 824834 to replace conventional autopsy in certain cases [ 49 , 50 ]  . 
though some of the techniques are single experiences [ 52 ] , others have been applied more regularly . research groups across several an overview of the methods is given in table 1 . 
in general , whole - body pmcta and targeted coronary pmcta have to be differentiated . whole body pmcta techniques multiphase postmortem ctangiography ( mpmcta ) the mpmcta is currently the most used and explored pmcta technique . 
because it was developed specifically for forensic applications , it uses standardised material and injection protocol , which should increase acceptance in court by reaching a complete filling of the vascular system while minimising artefacts , enabling improved radiological interpretation . 
a mixture of medium - viscosity paraffin oil ( paraffinum liquidum ) and an oily contrast agent ( angiofil , 6 % ) is injected via unilateral cannulation of the femoral vessels , or in some cases , the axillar vessels [ 53 ]  . 
mpmcta follows a specific injection protocol , standardising the flow rate and injected volume for each angiographic phase ( table 2 ) : an arterial phase showing the arterial system , a venous phase for investigating the venous system , and the final dynamic phase during which pmct data is acquired simultaneously with perfusion of the body , displaying the vessels during active luminal flow similar to clinical in vivo angiography . interpretation of the obtained images needs training and experience , as some post - mortem changes can mimic pathological findings [ 54 , 55 ]  . 
however , a recent study showed that the artefacts observed after mpmcta are reproducible and stable in terms of their localisation and type , making them relatively easy to recognise [ 56 ]  . a recently published study compared the overall performance of mpmcta with conventional autopsy and unenhanced pmct in 50 cases [ 15 ]  . 
though the majority of findings were detected both with autopsy and mpmcta , the latter demonstrated a higher sensitivity for identifying skeletal and vascular lesions , whereas conventional autopsy provided more information about organ morphology and pathology . 
 [ 15 ] included all cases investigated in a medico - legal centre without any inclusion criteria concerning the circumstances and cause of death , but other studies 1 3 radiol med ( 2015 ) 120 : 824834 1 3 830 table 2 protocol for mpmcta angiographic phase volume ( ml ) flow rate ( ml / min ) what is visualized / enhanced unenhanced mdct skeletal system , large vessels , organs arterial phase 1200 arterial system ( including pulmonary arterial stenosis , occlusions , extravasavenous phase 1800 arterial and venous system ( including pulmonary arteries ) , organ parenchyma dynamic phase arterial and venous system , organ veins ) parenchyma radiol med ( 2015 ) 120 : 824834 traumatic ( bone ) lesions , major lesions of organs / vessels , calcifications of vessels , determining indication for pmcta tions , signs of cardiac ischaemia ( pathological enhancement ) occlusions , venous extravasation , signs of pulmonary embolism , lesions of organ parenchyma verifying findings from the first two phases ( persistence of filling defects , stenosis , etc . ) have been carried out investigating different case groups for which cta would be indicated in a clinical setting : traumatic cases , in which a source of bleeding should be detected [ 57 ] , cases of death following surgical intervention [ 58 ] , and cases of cardiovascular disease [ 59 ]  . 
visualisation of bleeding sources and extravasation of contrast agent can also be used as a tool to visualise the trajectories of projectiles in the case of lethal gun shots , or stab wounds in cases of sharp trauma [ 60 , 61 ]  . 
in cases of sudden cardiac death due to ischaemic heart disease , mpmcta can guide direct sampling for histological examination by identifying stenosis and allow assessment of the morphology of coronary arteries , including stenoses and occlusions [ 59 ]  . 
a study performed on hospitalised patients who died unexpectedly or within 48 h of an event necessitating cardiopulmonary resuscitation showed promising results [ 62 ] , leading the authors to conclude that , in cases of unexpected death , the addition of mpmcta significantly increases the value of the post - mortem radiological exam , making it a feasible alternative for quality control and the identification of diagnoses traditionally made by medical autopsy . pmcta using cardiopulmonary resuscitation ( cpr ) this technique for visualising the vascular system was developed in japan , where the rate of pmct is high ( over 20 , 000 cases per year ) [ 12 ] and , due to traditional reasons , the autopsy rate is very low . 
for the same traditional reasons , and because any surgical intervention such as the cannulation of vessels in a deceased patient is shunned , an even less invasive and simple technique ideal for hospital application was developed based on the principles of clinical contrast agent injection and cpr [ 32 , 33 ]  . 
cpr is used to propel the contrast agent through the vascular syste normal clinical aqueous contrast media is injected into peripheral veins , such as the cubital vein , as in clinical in vivo contrast - enhanced ct investigations . 
therefore , the most common indication is currently the investigation of traumatic death in which cpr in the emergency room did not lead to success . other methods of wholebody pmcta some other approaches of whole - body pmcta have been reported in the literature without indicating specific protocols [ 28 , 29 , 34 , 35 , 52 , 54 ]  . 
other injection 1 3 radiol med ( 2015 ) 120 : 824834 protocols using mixtures of aqueous solution with or without peg have been proposed in the literature , most of them including an arterial and venous phase . 
some authors have also proposed leaving the injected contrast agent in the vessels for 1520 min before performing the ct scan , allowing it to diffuse out of the vascular bed and leading to contrast enhancement [ 35 ]  . 
unfortunately , the number of cases reported in the literature seems too small to fully appreciate the advantages and disadvantages of the method . targeted coronary pmcta in contrast to whole - body pma techniques , targeted pmcta techniques [ 30 , 31 ] consist of the filling of a specific part of the vascular system , most commonly , the coronary arteries . 
though both techniques use the left carotid artery for access , they have some differences ; the method developed in leicester consists of the injection of both air ( negative contrast ) and contrast media [ 65 ] , whereas the one developed in oxford uses only positive contrast media and makes efforts to avoid air inside the vessels [ 31 ]  . 
 the oxford system uses manual injection into the carotid artery , whereas the research team in leicester introduced a standard clinical ct power - contrast injector [ 66 ] , which allows acquisition of ct images of the coronary arteries during ongoing contrast injection , allowing their visualisation similar to the dynamic phase of mpmcta . 
 a detailed study investigating the performance of tca , compared these techniques to autopsy and histological investigations of coronary arteries [ 67 ] , revealing that , similar to whole body approaches , tca has good results identifying coronary lesions and is suited for investigating ischaemic heart disease . 
the authors also discuss whether the minimally invasive approach of pmcta has advantages over the conventional method of investigating coronary vessels , as the invasive autopsy and histology approach represent trauma for the vessels , leading to more important artefacts . first experiences with pmmr angiography although pmmr is much less frequently used than pmct , it is a powerful tool with a wide scope in forensic imaging [ 16 ]  . 
 pmmr exams are usually performed when the hospital is closed , and this limits the application in daily routine , especially as pmmr is a time - consuming exam compared to pmct . experiences with pmmr are scarce in the literature . 
this was explained by the long scan time and the absence of circulation of the contrast agent during image acquisition . 1 3 832 radiol med ( 2015 ) 120 : 824834 active research is ongoing to solve this problem , such as that within the technical working group post - mortem angiography methods ( twgpam )  . 
this international research group consisting of different worldwide institutions aims to further develop pma methods and deliver standardised methods , guidelines , and training for accurate interpretation of the images [ 55 ]  . 
as jackowski [ 7577 ] has shown in several papers , pmmr seems to have the potential to detect cardiac infarction in a way that is more sensitive than conventional autopsy and histology . 
although this research has to be further developed , a combination of mpmcta that allows the detection of coronary stenosis or occlusions with local cardiac pmmr angiography would likely open new possibilities in investigating cardiac death . conclusion the application of contrast media in post - mortem radiology is a complex subject and differs in many ways from clinical contrast - enhanced radiology . 
no circulation is present and the permeability of the vascular system is increased after death , requiring the development of specific contrast media mixtures and techniques to perfuse the vessels . 
no standardised methods are yet available , but intensive research is ongoing . acknowledgments the first author ( silke grabherr ) has had personal academic funding from the fondation leenards , lausanne , switzerland . conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2015 ) 120 : 777778 doi 10.1007 / s11547 - 015 - 0567 - 4 editorial forensic and medicolegal radiology : challenges , issues and new perspectives giuseppe guglielmi1 , 2 michelangelo nasuto1 antonio pinto3 published online : 2 august 2015 italian society of medical radiology 2015 during the last decades the radiologists world has been significantly influenced by the waves of technological progress . 
higher anatomical detail and multi - parametric analysis of pathological changes have widened the imaging spectrum and set new health quality standards demanding a more complex professional figure . medico - legal radiology has thus reflected this evolution through a dichotomous path : one bridging radiology with forensic medicine , and the other focusing on issues and malpractice lawsuits . both sides of this evolution rely in this special feature , which encloses the contributions of international experts in the fields of forensic radiology and legal medicine with the aim to provide a comprehensive overview on the state of the art and new perspectives on future developments . the radiologists deeper involvement in the diagnostic and clinical management of the patient revealed a duality of new , attractive challenges versus growing duties , liabilities , higher risks , and more sources of diagnostic errors . 
moreover , the evolution of case law [ 1 ] and the growing awareness of healthcare safety have dramatically raised the legal claims and , as a consequence , the phenomenon of the defensive medicine [ 2 ]  . 
malpractice lawsuits against radiologists are commonly related to diagnostic errors , improper use of * giuseppe guglielmi giuseppe.guglielmi@unifg.it 1 department of radiology , university of foggia , viale luigi pinto 1 , 71100 foggia , italy 2 department of radiology , scientific institute casa sollievo della sofferenza hospital , viale cappuccini , 1 san giovanni rotondo , 71013 foggia , italy 3 department of radiology , a . 
even the increasing use of contrast media requires extensive knowledge in terms of use appropriateness , choice of the right contrast agent , management of the emergency scenarios and providing proper informed consent to the patient . an adequate understanding of these main medico - legal issues could positively influence the radiologists clinical routine and the behaviour of patients and referring physicians , leading towards a significant reduction of errors and malpractice legal claims . on the other side , forensic radiology has arisen from two disciplines both based on the interpretation of anatomicalpathological findings . 
before the advent of multi detector computed tomography ( mdct ) , the forensic role of radiology remained substantially circumscribed to the identification of foreign bodies ( bullets above all ) by conventional radiology [ 5 ]  . nowadays the improvements in cross - sectional imaging and post - processing techniques have ensured that mdct plays a key - role in the emergency assessment of hemodynamically stable patients with penetrating wounds . 
the identification of wound track , its extension and its relationships with the surrounding organs are crucial for the therapeutic choice and can be very challenging for the forensic radiologist , who is supposed to know the different patterns of injuries and even the related legal aspects . besides the in vivo setting , the true revolution in forensic radiology has come for post - mortem imaging , which for decades constituted a marginal , ancillary technique of autopsy [ 6 ]  . 
in addition to the identification of foreign bodies , a comparison of ante - mortem with post - mortem radiographs was adopted since the 1930s for the crosscheck of 1 3 778 radiol med ( 2015 ) 120 : 777778 unique anatomical details and , together with dental x - rays , is still considered as an effective technique for human identification [ 7 ]  . 
to this regard , a recent field of research called virtual anthropology merges x - ray , ultrasound , mdct , and magnetic resonance imaging ( mri ) with anthropological criteria in order to estimate age , sex , geographical origin and stature in living and ( above all ) dead people [ 8 , 9 ]  . the introduction of mdct in post - mortem imaging had a huge impact on the forensic field , due to its three - dimensional and multi - parametrical acquisition of the state of the cadaver before the irreversible changes made by autopsy and thanatological processes . 
multiple ( eventually remote ) re - evaluations and advanced post - processing techniques allowed by digital data collection have enhanced the role of post - mortem mdct ( pmct ) as useful procedure to be conducted before the autopsy [ 10 ]  . 
the detailed visualisation of bone structures and the detection of internal haemorrhage and foreign bodies in locations less accessible to conventional techniques of examination , revealed mdct to be particularly suitable for the diagnosis and identification of homicide and disaster victims [ 11 ]  . 
however , poor soft tissue contrast and weak visualisation of vessels has limited its diagnostic value to major vascular lesions . during the last years , the idea of a contrast - enhanced pmct angiography ( pmcta ) capable of improving the diagnostic performances in coronary heart disease , pulmonary embolism and other vascular pathologies has become a target of several centres worldwide [ 12 ]  . 
the absence of blood flow and the post - mortem changes of the vascular system such as blood clots and augmented permeability of vessel walls led to the proposal of various injection and circulation techniques with specific mixtures of contrast agents [ 13 ]  . 
although the scattered distribution on the territory and the different degree of validation among all the approaches , in some centres pmcta has become a routine investigation showing promising results in comparison with conventional autopsy , particularly in the detection of the source of bleeding and coronary occlusions / stenosis [ 14 , 15 ]  . despite the impressive advances highlighted in this collection , the complexity of this emerging subspecialty still requires intensive research , standardisation , and accreditation by the international communities . 
in order to overcome these limitations , in recent years , contrast medium has been introduced in postmortem cases , with the development of several techniques of pmct angiography ( pmcta ) and standardized protocols to make them easily reproducible . 
 the aim of this review is to highlight the advantages and pitfalls of pmct and pmcta in forensic investigation , * vittorio fineschi vfinesc@tin.it 1 department of anatomical , histological , forensic and orthopaedic sciences , sapienza university of rome , viale regina elena 336 , 00185 rome , italy 2 neuromed , istituto mediterraneo neurologico ( irccs ) , via atinense 18 , pozzilli , 86077 isernia , italy 3 department of radiology , university of foggia , foggia , italy 4 department of radiology , scientific institute hospital casa sollievo della sofferenza , san giovanni rotondo , fg , italy 5 department of radiology , azienda ospedaliera ospedali 6 department of radiology , a . 
cardarelli hospital , riuniti , foggia , italy naples , italy 7 department of internal and experimental medicine magrassi - lanzara , second university of naples , naples , italy 8 department of radiological sciences , oncology and pathology , sapienza university of rome , rome , italy taking into consideration the broad spectrum of applications both for natural and unnatural deaths and the numerous methods currently used . 
secondly , in the light of the considerable progress in this field and the attempt to develop standardized protocols of pmcta , the authors aim to evaluate the diagnostic value of pmcta in comparison both to pmct and conventional autopsy . keywords virtopsy postmortem angiography postmortem - computed tomography postmortemcomputed tomographyangiography introduction with the discovery in 1895 of x - radiation by rentgen of wrzburg ( germany ) , medical practitioners throughout the world were provided with an important new tool . 
since it has been introduced , many improvements have been made in the field of radiological sciences , but only more recently have these been applied to forensic investigations , and the following of specific methods have been developed with the aim to support the forensic pathologist in establishing cause of death and in certain cases an attempt to substitute the conventional autopsy [ 2 , 3 ]  . 
in the field of postmortem - computed tomography ( pmct ) , the first application reported in accredited literature dates back to 1983 in a case of a diving fatality , where it was possible to demonstrate the distribution of gas , by cerebral - computed tomography , in the head of a 20 - year - old navy diver who died while diving at a depth of 43 m [ 4 ]  . currently , the use of multidetector - computed tomography ( mdct ) represents a reality routinely used in several forensic institutes , for the numerous advantages that this 1 3 radiol med ( 2015 ) 120 : 810823 diagnostic tool can provide ; costs are becoming increasingly lower ; data acquisition is always faster and once acquired may be revalued at any time . 
in order to overcome these limitations , in recent years , contrast medium has been introduced in postmortem cases , with the development of several techniques of pmct angiography ( pmcta ) [ 57 ] and standardized protocols to make them easily reproducible . presently , the most used pmcta techniques are four , each of which has variants . 
they defined a protocol for high - quality multiphase pmcta ( mpmcta ) with the aim to obtain a better interpretation of the findings by completely filling the vascular system in order to decrease as much as possible the artifacts caused by perfusion . 
 postmortem circulation is established by using a pressurecontrolled perfusion device ( virtangio ) , which injects a contrast agent mixture composed of 6 % of angiofil and paraffin oil into the femoral vessels which are cannulated on one side of the body . 
variations of this technique have also been developed , for example , with the cannulation of the axillary artery and vein on one side of the body instead of the femoral artery and vein [ 9 ]  . 
otherwise , it uses a different perfusion devices ( modified heartlung machine , different perfusion protocol , in fact no standardized protocol exists ) , different liquids ( use of contrast agents in watery solutions and different combinations of polyethylene glycol ) , and therefore , the interpretation of the images is very different . 
once the contrast agent has entered the heart cavities , it then goes into the body circulation thanks to cpr and images of the major arterial and venous system can be obtained [ 13 , 14 ]  . 
the femoral artery of a young man involved in a road accident was catheterized using ultrasound , and a pump was used for the injection of a mixture of iodinated contrast medium and water , which allowed the visualization of diverse principal arterial injuries . the aim of this review is to highlight the advantages and pitfalls of pmct and pmcta in forensic investigation , taking into consideration the broad spectrum of applications both for natural and unnatural deaths and the numerous methods currently used . 
secondly , in the light of the considerable progress in this field and the attempt to develop standardized protocols of pmcta , the authors aim to evaluate the diagnostic value of pmcta in comparison both to pmct and conventional autopsy . the databases some databases , from 1990 to december 2014 , were searched : medline , cochrane central , scopus , web of science , sciencedirect , embase , and google scholar , using the following keywords : virtopsy , virtual autopsy , minimally invasive autopsy , postmortem angiography , multiphase postmortem - computed tomography angiography ( mpmcta ) , postmortem with imaging , or ct or cta . 
the 459 sources found after the initial screening in order to exclude duplicate sources and reviews , were examined according to the inclusion criteria by four independent physicians ( two forensic pathologists and two forensic radiologists )  . 
the following inclusion criteria were used ( one of the first two at least other two ) : inclusion of case reports , series of cases , or retrospective studies postmortem tc / tca protocol used research / original articles autopsy confirmation circumstantial data and / or clinical data seventy - one sources were identified . 
1. all figures included in the present paper have extracted by authors from the archives of their institutions , with authorization of the ethical committee and consent of relatives of the deceased and here reported in anonymous form . discussion bleedings and hemorrhages acute bleedings and hemorrhages with a fatal outcome can be a tough challenge for forensic pathologists especially in identifying the source of bleeding . 
a no contrast phase : evidence of a large amount of left haemothorax associated with haemopericardiuthe arterial phase confirms the extravasation of contrast material supported by rupture of the antero - lateral wall of the left ventricle . 
the ventricular lesion is also confirmed by mpr ( arrows , b ) and mip reconstructions ( c ) table 1 identification of the source of bleeding by mpmcta in eight cases reported by palmiere et al . 
 [ 23 ] ; only in three case ( highlighted in column ) , the autopsy was able to confirm the mpmcta findings , whereas in the remaining five case because smaller vessels were involved , it was not possible to identify by autopsy the exact source of bleeding age / sex circumstances pmcta autopsy 23 / m 57 / f 72 / f 78 / m 82 / m 87 / f 15 / f 50 / m pedestrian pedestrian driver pedestrian ski accident driver multiple lacerations of the spleen branches of the right middle cerebral artery left renal vein and branches of the superior mesenteric artery multiple lacerations of the spleen natural death cerebellar arteriovenous malformation cerebellar arteriovenous malformation paragliding accident branches of internal iliac arteries and veins retropubic arteries and veins right hepatic artery superior sagittal sinus superior sagittal sinus palmiere et al . 
it is interesting to compare the mpmcta results with the autopsy ; only in three cases , the autopsy detected the exact source of bleeding ( multiple laceration of the spleen , cerebellar arteriovenous malformation , and superior sagittal sinus ) whereas for the remaining 5 cases , because smaller vessels were involved , it was not possible to identify the exact source of bleeding , and only hypotheses were formulated taking into consideration the presence of surrounding hematomas . 
 [ 24 ] reported a rare case of post - whiplash pseudoaneurysm of the right common carotid artery , which led to acute massive hemorrhage and the death of a 38 - year - old man several days after the initial trauma . 
in this case , the application of pmcta allowed the identification of the rupture of the pseudoaneurysm affecting the right common carotid artery with the contrast agent leaking into the mouth . 
the autopsy confirmed later the pmcta findings and highlighted a large hemorrhagic clot extending to the right side of the neck and mediastinum . a research group of chiba university ( japan ) [ 25 ] investigated the utility of postmortem cerebral angiography using multidetector row ct ( mdct ) by injecting a 1 3 814 radiol med ( 2015 ) 120 : 810823 contrast medium through a catheter inserted into the internal carotid and vertebral arteries of 10 subarachnoid hemorrhage cases . 
one of the most important aspects in the forensic investigation of subarachnoid hemorrhage is to determine whether the cause is intrinsic or extrinsic taking into consideration the legal consequences of the different causes of the subarachnoid hemorrhage [ 26 , 27 ]  . 
although pmcta has been shown to be able to detect aneurysms , however , it is sometimes difficult to identify the aneurysm and bleeding sites because of the large amount of contrast medium which can leak into the extravascular space . 
in order to overcome this limitation , the japanese research group developed a dynamic cerebral angiography method , in which the same area is scanned several times during the injection of the contrast agent allowing real - time observation of the contrasted vasculature and capturing the exact moment when the contrast agent leaks from the hemorrhage site . 
this method although very useful in the detection of the exact source of bleeding shows some limitations : it is selective angiography for the cerebral arteries , not for the entire vascular system ; therefore , systemic vascular conditions or pathologies with subsequent involvement of the cerebral vessels cannot be detected ; secondly , this technique is unable to detect lesions at the proximal level of the internal carotid artery and vertebral artery due to the placement of the catheter [ 25 ]  . among natural causes of bleeding , aortic dissection is by far the most common and serious condition affecting the aorta . 
in case of dissections of the ascending aorta , the major aortic branches are occluded , resulting in rapidly fatal complications such as cardiac tamponade , major stroke , or massive myocardial infarction [ 2931 ]  . 
if , on the one side , the evaluation in living subjects of cardiac tamponade due to a hemopericardium , using diagnostic imaging techniques with special regard to the ct , allows a good interpretation of the anatomy and the pathology of the pericardium [ 32 , 33 ] , on the other side , in postmortem investigations , only a few studies have used pmct imaging to investigate cardiac tamponade in the last decade [ 3438 ] ( see table 2 ) and the results obtained show the feasibility of using the pmct technique to diagnose haemopericardium and cardiac tamponade in cadavers . 
however , despite the advantages of mdct in terms of performance simplicity , data acquisition , and cost effectiveness , this technique has the disadvantage of limited organ parenchyma and vascular system visualization ; therefore , a greater contribution for the detection of cardiac tamponade can be made using the pmcta technique , application of which is presently very limited . 
 [ 39 ] have recently reported a case involving a 72 - year - old man , in which mpmcta was helpful in defining the diagnosis , detecting a haemopericardium and the ruptured wall situated in the posterior part of the left ventricle . 
the autopsy was then performed , totally confirming the ct angiography findings . ischemic heart disease ischemic heart disease ( ihd ) as a consequence of atherosclerosis represents the most common cause of mortality in developed countries [ 40 ]  . 
in postmortem investigation , the diagnosis of ihd is usually made after a complete autopsy , supported by macroscopic and microscopic examination of the heart , with the classical histological stainings and also table 2 papers reported in the literature during the last decade , in which pmct imaging was used to investigate cardiac tamponade study age ( years ) / sex causes pmct findings n . 
 [ 37 ] nonoperable aortic aneurysm dissection ( stanford type a ) hypertension car accident chest trauma dissected aneurysm of the no autopsy ascending aorta aneurysm of the ascending aorta pericardial effusion no autopsy haemopericardium no autopsy ebert et al . 
 [ 34 ] mean age : pericardial effusion 46 / 10 m5 f lethal trauma ( 8 ) rupture after myocardial infarction ( 6 ) sepsis ( 1 ) shiotani et al . 
 [ 38 ] from 40 to natural causes 101 / 15 m15 f pericardial effusion large pericardial effusion autopsy findings autopsy confirmation no autopsy 1 3 radiol med ( 2015 ) 120 : 810823 the contribution of immunohistochemistry . 
however , in recent years , postmortem cardiac imaging has been introduced with both targeted coronary ct angiography techniques [ 41 , 42 ] using minimally invasive approaches and mpmcta involving the whole body [ 8 ] , which allows the filling of the arterial and venous systems , including coronary arteries . 
the postmortem investigation of ihd differs in several aspects from the clinical one , because the application of certain techniques , such as electrocardiography and several laboratory analyses , after death is not possible [ 43 ]  . regarding postmortem coronary angiography , two english centers , leicester [ 41 ] and oxford [ 42 ] , independently developed two separate postmortem coronary cta techniques , both using the left carotid artery to insert a urinary catheter . 
 some differences can be highlighted between the leicester and the oxford method ; according to the first one [ 41 ] , both air and contrast media are injected , whereas in the oxford method only , the contrast agent is injected [ 42 ]  . 
moreover , the extent of calcification does not correlate with the degree of coronary artery stenosis and plaques involved in acute thrombosis show a lower degree of calcification than the ones associated with clinically stable angina [ 47 , 48 ]  . according to michaud et al . 
the results reported in this study support the application of mpmcta as a reasonable tool to use in order to exclude coronary artery stenosis and to highlight possible occlusions to point out the subsequent sampling for histology . 
 [ 22 ] , a pathological enhancement of the myocardium , which is considered an indirect sign of myocardial ischemia , was found . pathological enhancement of the myocardium was also observed by palmiere et al . 
 pathological enhancement was found in some of the cases showing coronary luminal filling defects without collateral vessels , as well as in others presenting complete or incomplete coronary arterial luminal filling defects and the presence of collateral vessels . 
 [ 49 ] , myocardial enhancements detected at angiography seem to correspond well to the areas of infarction as long as the infarction is not in its acute phase . lastly , another point worthy of attention highlighted both by michaud [ 22 ] and palmiere [ 49 ] in both series of cases is that although pmcta allows a reliable diagnosis of acute coronary thrombosis , the precise location and extent of suspected coronary thrombi cannot be exactly established before the pmcta ; therefore , their eventual dislodging due to the introduction of the contrast medium into the vascular system cannot be definitely excluded . as stated by michaud et al . 
 [ 22 ] , the advantage of mpmcta is that there is no direct mechanical manipulation of the coronary arteries , because the site of cannulation is placed in one of the two inguinal regions and the perfusion pressure is very low ( 1.200 ml in 90 s for the arterial phase ) ; therefore , the perfusion flow in the coronary arteries is slower than in vivo . pulmonary thromboembolism thromboembolism ( vte ) includes pulmonary venous thromboemboli ( pe ) and deep venous thrombosis ( dvt ) , typical of the pelvic and lower - extremity veins . 
pulmonary emboli have been estimated to occur in more than 600 , 000 patients per year in the united states and result in 50 , 000200 , 000 deaths annually . 
 [ 54 ] for the interpretation of pmctpa images for the diagnosis of pe diagnostic criteria for the interpretation of pmctpa images presence or absence of symmetrical filling of segmental pulmonary arteries by contrast presence or absence of discrete filling defects and allied to this diagnostic feature determination of a continuous filling defect extending from the right ventricle into the pulmonary outflow tract , main pulmonary artery , and left and right main pulmonary arteries . moreover , the identification of pulmonary thromboembolism as a cause of sudden death may lead to the identification of a familial clotting disorder and could subsequently be lifesaving for relatives of the deceased [ 54 ]  . 
recently , a few reports of pmcta for the diagnosis of pe have been reported in literature [ 9 , 54 , 55 ]  . a research group of the victorian institute of forensic medicine in melbourne , examined 13 cases where pt was clinically suspected . 
 [ 54 ] for the interpretation of pmctpa ; all of them refer to filling defects , and they are summarized in table 3 . in seven of the 13 cases examined by the australian group , pmctpa allowed the following diagnosis : pt to major vessels in 5 cases , massive pt in 1 case , and probable segmental pt in another case . 
it is noteworthy to highlight that in the 13 cases reported by burke and colleagues , there were no false negatives ; the six cases where the pmctpa excluded the presence of pt , were all confirmed successively following autopsy . an italian group of the university of foggia developed an alternative approach suitable in cases of fatal pe [ 9 ] ; they modified the standard procedure established by the technical working group postmortem angiography methods [ 8 ] , which uses the femoral vessels on one side of the corpse as an access point to the vascular system by isolating and then cannulating the axillary artery and vein on one side of the corpse . 
this alternative approach allows , in comparison to the traditional one [ 9 ] , which excludes the vascular tree below the cannula insertion where lesions such as thrombosis of the superficial and deep venous system remain elusive , a reliable recognition of a filling defect or inhomogeneous opacification , facilitating therefore a visual inspection of the exact site of the suspected venous thrombus . 
b the hyoid bone ( hb ) and laryngeal cartilages ( lc ) , including the thyroid cartilage ( thc ) and the cricoid cartilage ( crc ) are visualized in a perfect way to compare autoptical findings system of the lower extremities and identify the venous thrombus for subsequent histological examination [ 9 ]  . further applications of pmct and pmcta in forensic investigation vogel et al . 
evaluated in two different studies [ 56 , 57 ] the most significant findings provided by pmct and pmcta after transvascular cardiac interventions [ 56 ] and cardiac surgery [ 57 ]  . 
in those cases , in which the death of a patient occurs during the surgical intervention or shortly after , is very important to establish if the cause of death is due to a complication of the surgical procedure , a medical error or if it was not related to surgery . 
 [ 56 ] examined pmct and pmcta findings after coronary angiography , coronary angioplasty ( ptca ) , stent placement , transarterial valve implantation ( tavi ) , mitral clips , transvascular annuloplasty , and pacemaker placement . 
pmct detected previous contrast medium injections , the presence of blood ( e.g. , in pleura , mediastinum , 1 3 radiol med ( 2015 ) 120 : 810823 1 3 818 radiol med ( 2015 ) 120 : 810823 1 3 radiol med ( 2015 ) 120 : 810823 1 3 820 group 1 group 2 group 3 table 5 artifacts / pitfalls of mpmcta identified by bruguier and colleagues [ 89 ] and divided into three groups incomplete venous opacification of the head and neck vessels artifactual contrast enhancement or extravasation of the gastrointestinal tract contrast layering in the nondependent aspect of vessels or incomplete filling of the arterial or venous system radiol med ( 2015 ) 120 : 810823 pericardium , groin ) and its amount , and the presence or absence of air bubbles in vessels . 
currently , the management of a mdct unit is easier , and its maintenance costs are more affordable , making it a valid tool available in numerous forensic science centers [ 8588 ]  . the diagnostic value of mdct compared to full autopsy has been broadly investigated , and numerous papers have been published in this field . 
however , if , on one the hand , native ct is able to detect major vascular lesions ( e.g. , aortic rupture ) , on the other hand , its main limitation is represented by its low ability to visualize the vascular system together with the soft tissue . 
the recent introduction of some techniques of pmcta with the injection of a contrast medium into the vessels has allowed the visualization of the whole vascular system in a minimally invasive way [ 712 , 85 ]  . 
 some standardized protocols have been developed and published ; their application would allow making the procedure more easily reproducible and the operators aware of possible artifacts that its application can generate . 
in this regard , bruguier and colleagues [ 89 ] have recently published a study in which they have evaluated technique - related artifacts in 54 cases in which the mpmcta was performed according to the protocol proposed by grabherr et al . 
the identification and categorization of these artifacts according to their type , anatomical location , and timing of appearance during the angiography are of utmost importance , because the mpmcta technique was developed with the aim of applying it in routine forensic investigations . 
the results obtained by this preliminary study [ 88 ] show essentially three groups of artifacts / pitfalls which may be misinterpreted for pathological findings ; they are reassumed in table 5 . 
the identification of these artifacts and an understanding of their meaning are fundamental in order to guarantee a proper interpretation of pmcta images . however , if on the one side , the application of pmcta protocols has numerous unquestionable advantages , on the other side , some disadvantages need to be discussed ; the application of certain protocols requires the use of further equipment to be coupled to mdct and the employment of dedicated personnel which result in costs that small institutions cannot always financially cope with . pmcta techniques are relatively new , and much more research is needed in this field . 
presently , pmcta still seems to be far from replacing the conventional autopsy , but it may represent a valid diagnostic complementary tool with encouraging prospects in the near future . 
however , digital autopsy is and will remain merely an aid in the practice of forensic medicine and one that is not always available and that cannot be considered an alternative to conventional postmortem procedures [ 90 ]  . 
the increasing use of cm is likely to give rise to a wide range of pitfalls , including compliance with and appropriateness of indications for the use of cm themselves , the choice of the best contrast agent , off - label use , evaluation of special populations of patients , and competence to tackle emergency scenarios following the administration of cm . 
even more prominent , and potentially more important , is the issue of informed consent which brings with it a duty to inform patients awaiting the administration of cm with regard to the nature of the procedure , the existence of alternative procedures , the extent of the risks relating to the use of cm and , finally , the risks relating to refusal of the procedure . 
 all these issues may give rise to concerns about liability for failure to offer adequate information to patients or to carefully evaluate and balance the potential risks and benefits of the procedure or , finally , for being unprepared in the event of adverse reactions to cm , especially when these are severe and life - threatening . 
educational and training programmes for radiologists are likely to shape change in the medical liability environment in the coming years . keywords contrast media adverse reaction informed consent off - label use medical liability introduction contrast media ( cm ) enhance the quality of images , revolutionizing the radiologists ability to differentiate softtissue densities . 
nonetheless , risks associated with cm have not been eliminated : varying degrees of adverse reactions continue to occur , and , in some situations , their use is problematic [ 27 ]  . 
a recent united states nationwide research showed that the commonest causes of medical malpractice suits against radiologists were diagnostic errors and procedural complications , followed by inadequate communication with either patient or referring physician [ 14 ]  . 
it is a process which implies the doctors duty to inform patients of the benefits and potential risks of the treatment options , to answer their questions openly and honestly , to help patients in their choice and , finally , to accept that choice [ 18 ]  . special scenarios and caveats regarding the practice of radiology and particularly the use of cm need to be discussed . one key question is that the patient - radiologist relationship tends to be brief and episodic , so that radiologists are unlikely to have an established relationship with the patient [ 19 ] , and may not feel comfortable discussing the risks and complications of their procedures with the patient [ 20 ]  . 
 [ 17 ] report that , despite the fact the appropriate time for obtaining informed consent is considered to be more than 24 h prior to the procedure , very often it is obtained on the same morning or immediately before the procedure itself . 
finally , also the time that radiologists spend with patients is critical in ensuring that patients are satisfactorily informed [ 23 ]  . another key point is the amount of information , especially with regard to risks , that should be given to patients ; and in radiological practice the use of cm exacerbates the issue [ 2426 ]  . 
the appropriateness of the use of cm , any alternative procedure , the risks and benefits of not undergoing the proposed diagnostic or interventional procedure with cm have to be outlined in the informative process . 
in the acr manual on cm [ 13 ] it is stated that because of the documented low incidence of adverse events , intravenous injection of contrast media may be exempted from the need for informed consent , but this decision should be based on state law , institutional policy , and departmental policy . 
other authors seem to take the same view [ 31 ]  . contrarily , we believe that the low statistical frequency of complications , specifically those which are life - threatening , does not exempt radiologists from the duty to inform patients of these specific risks . 
obtaining consent for all radiological cm procedures is an ethical duty , regardless of the nature of the agent used and the incidence and severity of the possible adverse events . 
a correct informative process is one in which physicians communicate the gist of the message to the patients , i.e. , that there is some risk involved in the use of cm . 
communicating the gist without referring to statistics , tailoring information to the patients needs and facilitating peoples understanding are essential elements of informed consent when radiologists are using contrast agents . finally , the form of informed consent ( written or verbal ) that is mainly based on state laws , and institutional and departmental policies . 
there is wide agreement that a multimedia approach combining videos , verbal communication , audio tape , pamphlets , and interactive methods of communication may improve the patients comprehension and participation in the decision - making process [ 32 ]  . 
the readability of informed consent forms is a critical issue [ 33 ] as many informative leaflets are written in such a way as to be incomprehensible to the average patient . the above - mentioned criticisms arise particularly in emergencies where an inherent difficulty with obtaining adequate informed consent exists [ 34 , 35 ]  . offlabel use the first point concerns the definition of off - label contrast medium ( olcm ) which depends on the regulatory environment of different countries . 
in general terms , off - label use means use other than the originally tested and licenced indications , and the obtaining of licences depends on drug laws which may vary from country to country . in the european normative framework , cm fall within the definition of medicinal product ( ec directive 2004 / 27 / ec 31 march 2004 ) : any substance or combination of substances which may be used in or administered to human beings either with a view to restoring , correcting or modifying physiological functions by exerting a pharmacological , immunological or 1 3 804 radiol med ( 2015 ) 120 : 802809 metabolic action , or to making a medical diagnosis [ 36 , 37 ]  . 
 in the united states off - label use generally means that a medical product is not administered for the specific use approved by the food and drug administration ( fda ) and listed in the drug - labelling information . 
to sum up , off - label use of a medical product is its prescription and use in a manner and for purposes other than those approved by competent authoritative agencies and national drug laws . 
since these agencies regulate only the labelling of the medical products and do not regulate the practice of medicine , the off - label use of drugs and medical products is becoming increasingly common [ 38 ]  . to fully understand the medico - legal implications of olcm , the differences existing between cm and other drugs have to be taken into account . 
as outlined by thomsen in his editorial , cm are not designed to have therapeutic effects and they are administered in one dose , under medical supervision , and provide their effect under the principles of physics , not those of pharmacology [ 39 ]  . 
according to current regulations cm are officially approved for some specific uses and for body areas ; their use in imaging the rest of the body is considered off - label [ 39 ]  . 
for all these reasons , often the approved indications do not match the real clinical and diagnostic needs and in daily practice the off - label use of the cm is extremely common , mostly involving gadolinium - based contrast agents ( gbcas ) , especially in mr angiography , cardiac and paediatric applications [ 36 , 40 ]  . the most striking example is contrast - enhanced ultrasound ( ceus ) , particularly in the paediatric population , that is increasingly practised since it may reduce the use of ionizing radiations , and nowadays it is an established technique for many organs . 
cardiac application of ultrasound contrast agent is approved in the united states , but it is not known when or if ultrasound contrast agents will be approved for non - cardiac applications there [ 42 ]  . 
there is widespread use in europe [ 44 ] , and there are ongoing efforts by the society for paediatric radiology and international contrast ultrasound society to push for paediatric ceus in the united states [ 45 ]  . 
therefore it may be expected that ceus will be increasingly used throughout childhood [ 46 ]  . liability profiles may result from olcm use since , despite widespread clinical practice , it is still formally outside the regulatory boundaries [ 37 ]  . 
it is known , for example , that with increasing off - label use , significant differences have not been observed in the incidence of severe adverse reactions between approved and unapproved use of cm [ 39 ]  . 
 nevertheless , in the case of adverse reaction , especially if severe and life - threatening , the radiologist must demonstrate that the off - label use of that cm was fully supported by scientifically valid evidence and that there were no contraindications for the safety of the patient . 
making a clear distinction between cm off - label uses that are well supported by the best scientific evidence available and those that are not is the gordian knot of the issue [ 47 ]  . 
 the fda states that if a physician uses an off - label drug or medical device , he or she should base judgment on sound medical evidence and should maintain a record of the products used and their effects [ 48 ]  . 
in a similar vein is the position of the society of interventional radiology which supports the lawful use by a physician of a drug product for an unlabelled indication when such use is based on sound scientific evidence and / or sound medical opinion [ 49 ]  . 
the second vital point , again with regard to the professional responsibility of the radiologist and possible requests for damages arising from the off - label use of the cm , is the information supplied to the patient prior to doing the exa since the radiologist uses a cm which the regulatory body has not stated is safe and effective for that specific use , we believe that he / she is obliged to provide exhaustive information to patients and obtain formal consent before using an olcm . 
some authors agree that it is not acceptable for a physician to neglect to tell patients of a medical products off - label status while some others have contended that off - label status is irrelevant to the actual medical risks posed [ 5052 ]  . 
while aware of the specific nature of the cm with regard to traditional medicines , we consider that the radiologist is still obliged to inform the patient of the off - label use of the cm , to explain the clinical and scientific reasons supporting it , to highlight the advantages in terms of effective diagnosis , to explain any alternative diagnoses and finally to obtain informed consent to the off - label use of the cm [ 40 ]  . in conclusion , some key points can be drawn . 
they must also base its use on firm scientific rationale and on sound medical evidence when alternative labelled products are not of equally proven efficacy , and fully inform patients of the potential adverse effects of the product . finally , it should also be pointed out that it is the duty of radiologists to report any suspect adverse reaction associated with olcm use to local / national authorities responsible for drug safety monitoring . 
radiologists should be made aware that the reason for collecting information on olcm use is to ensure the highest standard of patient 1 3 radiol med ( 2015 ) 120 : 802809 safety , possibly further to a review by ad hoc local and national committees of incidents involving olcm use and to subsequent appropriate actions . reaction , six to tenfold by asthma , and to a considerable extent by a history of allergic reactions to other drugs [ 66 , 67 ]  . medical liability the principles regulating medical liability differ from country to country and between common law and civil law systems , and malpractice in radiology varies across the globe [ 53 ]  . 
in daily practice , around 35 % of radiological analyses contain errors [ 5660 ] ; errors in interventional procedures and adverse events occurring during a radiological examination take second place in this negative ranking [ 61 ]  . the issue of medical liability and malpractice is not unique to radiologists ; however , some key points have to be stressed , focusing particularly on the use of cm [ 2 , 3 , 62 , 63 ]  . indication for the examination , and specifically the use of contrast media except for screening tests , radiologists generally receive the requests for examination from a referring physician . 
existing guidelines may strongly assist the radiologist in making the most appropriate imaging decision for a specific patient [ 64 , 65 ]  . investigation into medical history careful investigation into the patients medical history with special attention to eventual previous reaction to cm is critical . 
it is noteworthy that risk is increased sixfold by a history of adverse careful attention to special populations even more attention is required before administering cm to special populations . pregnant and breastfeeding women beyond the risks related to the exposure of the foetus to ionizing radiations and high magnetic fields , the administration of cm may be a further hazard for the foetuses and neonates [ 68 ]  . cm cross the human placenta , thus entering the foetus . 
however , the lack of adequate and well - controlled studies regarding these possible effects in humans has induced the acr to recommend the use of iodinate - contrast media in pregnant women only when : ( 1 ) the information requested cannot be acquired without contrast administration . 
 ( 3 ) the referring physician is of the opinion that it is not prudent to wait to obtain this information until after the patient is no longer pregnant [ 64 ]  . 
also , the updated version of esur guidelines [ 65 ] recommends that the use of iodine - based cm in pregnant women should be limited only to exceptional circumstances and that following their administration , thyroid function should be checked in the neonate during the first week . 
regarding the use of gadoliniumbased contrast agents , the revised guidelines recommend the administration of the smallest possible dose of the most stable gbcas only when there is a very strong indication . both iodinateand gadolinium - based cm are thought to be safe for mothers and children . 
a recent position paper of the italian society of radiology , the italian society of paediatrics , the italian society of neonatology and the task force on breastfeeding , italian ministry of health [ 71 ] states that breastfeeding is safe for the nursing infant of any postconceptional age after administration to the mother of all iodine - based contrast media and most gadolinium - based 1 3 806 radiol med ( 2015 ) 120 : 802809 contrast media . 
there is no need to discontinue breastfeeding for 1248 h after the administration of contrast media and no use in expressing and discarding breast milk following the imaging . in conclusion , although the regulatory statements and clinical practice for the use of contrast media in pregnancy and lactation differ [ 70 ] , caution is strongly advised and radiologists must be aware that the use of contrast media in pregnant women must be limited to cases when the benefits outweigh the potential risks . 
accurate information and written informed consent to the procedure are strongly advised . patients who take metformin they need special attention before the administration of cm since their use , and specifically iodine - based cm , may increase the risk of lactic acidosis patients taking metformin with known , borderline , or incipient renal dysfunction [ 72 ]  . 
management varies according to the recurrence and / or severity of renal impairment : no discontinuation of metformin nor creatinine control in patients with normal renal function and no comorbidities is required ; discontinuation at the time of examination and for 48 h in patients with multiple comorbidities and apparently normal renal function , followed by the reassessment of renal function before restarting metformin is required . 
in patients with renal dysfunction , metformin should be suspended at the time of the contrast injection , and cautious follow - up of renal function should be performed until safe reinstitution of metformin can be assured . 
no special precautions are requested for gbcas [ 65 ]  . patients with previous renal insufficiency they are at greater risk of developing contrast - induced nephropathy ( cin ) than patients whose function is normal . 
cin is a well - described iatrogenic effect of the use of iodinate - contrast medium that occurs more frequently in patients with previous renal insufficiency [ 73 ]  . 
 statements from scientific associations provide specific recommendations on how to manage these patients [ 64 , 65 ]  . premedication premedication is critical in possible liability scenarios linked to the use of cm . 
we refer to patients with previous reactions to cm for whom a pre - treatment regimen , including administration of corticosteroids with or without antihistamines or other medications , is thought to be safe . 
a recent review of the existing literature shows that in unselected patients , the usefulness of premedication is doubtful , and data supporting the use of premedication in patients with a history of allergic reactions are lacking [ 78 ]  . 
local institutional policies may exclude the use of cm in patients with prior moderate or severe reactions and in pre - medicated patients whose previous reactions were mild [ 77 ] ; however , the contrast media safety committee of esur considers the use of premedication , although evidence of its effectiveness is limited in patients with previous moderate or severe acute reactions [ 65 ]  . several different premedication regimens have been proposed to reduce the frequency and / or severity of reactions to contrast media . 
the possible switch to other contrast agents , and the strict observation of the patients ( 20 / 30 min after the contrast medium injection , having drugs and equipment for resuscitation quickly and readily available ) are also suggested as precautions for radiologists [ 79 ]  . 
 however , radiologists are reminded that they should be prepared to deal with the possible reactions [ 64 , 65 ]  . in conclusion , the take - home message is that radiologists must be wary of reactions in patients with a previous history of life - threatening reaction , bronchospasm or asthma , hypotension or shock from an underlying illness and allergies and be aware that premedication does not completely eliminate the risks of severe and lifethreatening reactions in those patients . 
the statement that physicians who are dealing with these patients should not rely on the efficacy of premedication [ 78 ] must be kept in mind by radiologists when deciding whether or not to use cm in patients with prior reaction . appropriateness and timeliness of adverse reaction management finally , radiologists can be sued if the management of the adverse reaction induced by a contrast agent is not prompt and correct . 
rapid identification of alarming , life - threatening symptoms and adequate therapeutic strategies are 1 3 radiol med ( 2015 ) 120 : 802809 recommended according to the kind and the severity of the adverse reaction [ 80 , 81 ]  . 
however , knowledge of the management of acute contrast reactions is lacking among radiologists [ 82 ] and training and educational programmes are of paramount importance to help them to improve their performance in emergency scenarios following the administration of cm [ 82 , 83 ]  . conclusions the increasing use of cm is likely to give rise to a wide range of pitfalls , from compliance with and appropriateness of indications , to the choice of the best contrast agent . 
 moreover , off - label use , evaluation of special populations of patients , and readiness to deal with emergency scenarios following the administration of cm are some of the most challenging issues for radiologists . 
even more prominent , and potentially more important , is the issue of informed consent which implies a duty to inform patients awaiting the administration of cm of the nature of the procedure , the existence of alternative procedures , the extent of the risks related to their use and , finally , the risks of refusing the procedure . all the above - mentioned issues may give rise to concerns about liability for failure to offer adequate information to patients or to carefully evaluate and balance the potential risks and benefits of the procedure or , finally , for being unprepared in the event of adverse reactions to cm , especially when severe and life - threatening . 
volterrani1 received : 28 january 2015 / accepted : 8 june 2015 / published online : 25 june 2015 italian society of medical radiology 2015 row computed abstract multidetector tomography ( mdct ) represents the technique of choice for the majority of pathologies today and is responsible for the majority of diagnoses . 
however , despite the low number of studies dedicated to errors in mdct , ct reporting seems especially prone to generating errors and errors are an inevitable part of mdct practice . 
most of these arise during image interpretation but , differently from other radiological techniques , the awareness of radiologists regarding technical ct aspects and pathologies substantially contribute in generating errors , in particular because ct technology expands rapidly and radiologists do not routinely receive specific and appropriate training for its use and because ct examinations are not the same for each patient and each pathology and the choice of the most appropriate ct examination ( including the dose exposure to the patient ) presumes a very large awareness from radiologists . 
this review is aimed at increasing awareness regarding the type of errors in mdct and in particular to also highlight technical and procedural errors . keywords multidetector row computed tomography medical error diagnostic error dose ct * m . 
in particular , errors in imaging may lead to suboptimal treatment in cases of failure to recognise a pathology or to unnecessary hospital admission or surgery in case of a false - positive diagnosis [ 2 ]  . 
the main reason for studying medical errors is to try to prevent them and the essential condition to prevent medical errors is the precise awareness of each problem , both in terms of identification of the critical point and in terms of analysis of the causes of the error . 
in radiology , errors can be more complex than in other fields of medicine , because they can arise from an inappropriate utilisation of the diagnostic technique or equipment ( ct , mr , us system , etc . ) , which evolve rapidly with technological developments , requiring a constant update by radiologists . 
however many errors in computed tomography ( ct ) are not recognised as such because they do not produce a legal effect and on the other hand , the detection of errors in ct is in proportion to knowledge of radiologists . 
 this review is aimed at increasing awareness regarding the type of errors in multidetector row computed tomography ( mdct ) and in particular to also highlight technical and procedural errors . error : what does it mean in radiological practice today ? the institute of medicine defines an error as the failure of a planned action to be completed as intended or the use of a wrong plan to achieve an aim ; however , other definitions of error are present in medical literature [ 3 ]  . 
in addition , medical errors are defined as mistakes made in the process 1 3 786 radiol med ( 2015 ) 120 : 785794 of care that result in or have the potential to result in harm to patients . 
mistakes include the failure of a planned action to be completed as intended or the use of a wrong plan to achieve an aithese can be the result of an action that is taken ( error or commission ) or an action that is not taken ( error of omission ) [ 4 , 5 ]  . 
in diagnostic activity , an error generally occurs as a consequence of inappropriate organisation , management processes ( latent error ) or in the perception or interpretation of diagnostic images ( human error ) [ 1 ]  . 
radiological errors in daily clinical diagnostic practice occur at a rate of about 30 % and errors that arise in relation to ct constitute the bulk of such errors ; in particular mccreadie and oliver , in a study of 222 patients , reported 256 errors , of which 159 ( 62 % ) arose in relation to ct examination [ 6 , 7 ]  . multidetector row computed tomography : the titan of diagnostic imaging medical imaging is an essential tool for making often definitive diagnoses today , and mdct is responsible for the majority of these diagnoses . 
it has become the investigation of choice in the workup of trauma , nontraumatic thoracic and abdominal emergency , oncologic patients and thoracic pathologies thanks to its high diagnostic accuracy , fast execution of examination and wide availability in public and private healthcare centres [ 8 , 9 ]  . 
this large diffusion has two main consequences : first mdct is not a niche technique but a technique routinely utilised by the majority of radiologists ( even if they have not received specific and appropriate training for its use ) and furthermore a dosimetric consequence , leading to about 80 % of medical absorbed dose to the entire population , because of an increase not only in the absolute table 1 errors in mdct errors in exam recommendation errors in exam execution acquisition parameters ( collimation , reconstruction interval , field of view , etc . ) anatomical volume to be covered diagnostic modality ( spiral , axial , distention of viscera ) dose exposure to the patient observer errors perceptual errors ( scanning and recognition ) decision - making errors exam interpretation medical report organisation failure to suggest the next appropriate procedure failure to communicate in a timely and clinically appropriate manmdct multi detector computed tomography number of ct examinations , but also in terms of both length of coverage and number of phases obtained while scanning ( baseline , arterial , venous and late phases ) [ 10 ]  . 
however , despite the importance of mdct there is little diffusion of standardised and shared ct examination protocols so radiological malpractice in using this technique and the possible errors that could originate are many and from different aspects of its use ( table 1 )  . 
 moreover , mdct technical equipments are very different in terms of slices , dose exposure and diagnostic possibilities so that a lot of errors or a suboptimal use of the ct machine can occur if the radiologist is not experienced about the scanner used . type of error in mdct unappropriated ct examinations a more common error regarding ct is the appropriateness of its use . 
in particular , both radiologists and clinicians should evaluate the riskbenefit ratio of a ct examination , choosing a diagnostic examination which takes into account the smallest amount of dose exposure to the patient with equal diagnostic results . 
 furthermore , the clinicians and radiologists should know the previous diagnostic examination / s performed on the patients , the clinical history of the patient and any possible clinical contraindications to the administration of contrast media ( if it is not possible to administer intravenous contrast media and the unenhanced ct examination is not useful for clinical suspicion , it is an error to suggest a ct examination )  . 
for example , in the diagnostic evaluation of pelvic pathologies or focal liver lesions , magnetic resonance imaging ( mri ) is generally more appropriate than ct , also for the absence of ionising radiation . 
so it could be an error to perform a ct examination for the characterisation of a pelvic mass in a woman , especially in the reproductive age , or a ct examination for the characterisation of a focal liver lesion detected at us examination , especially in a young girls , even if both setting ( for example emergency ) and patient symptoms could influence this choice [ 11 , 12 ]  . 
1 errors in exam recommendation : contrast - enhanced ( a ) and unenhanced ct ( b ) axial images of pelvis performed after us examination for a clinical suspicion of sigmoid diverticulitis in a 30 - yearold woman with a history of acute left lower quadrant pain : both the contrast - enhanced and unenhanced ct showed a left adnexal mass , slightly hyperdense upon unenhanced ct image ( white arrows )  . 
2 errors in exam recommendation : contrast - enhanced ct ( a ) and contrast - enhanced mr ( b ) axial images performed in a patient with a tumour of oral cavity ( white arrows )  . 
in this clinical case , radiologists errors in performing ct examination instead of mr examination were due to the choice of an inappropriate radiological technique and specifically related to a technical issue errors in exam execution errors in exam execution are more common in mdct examination than in any other diagnostic technique , both because of the complexity of the ct technique and because of the multiple variables that can influence the choice of the different technical parameters for each ct examination . 
for example , in performing a high resolution ct examination of the thorax , some ct technical parameters are essential : the use of thin sections ( 0.51.5 mm ) , a high resolution algorithm for the reconstruction of images , the smallest field of view ( fov ) that will encompass the lungs , and finally it is essential to obtain the hrct images during a suspended full inspiration . 
however , radiologists should be also able to complete the hrct examination with an expiratory or postexpiratory scan ( for example to confirm the presence of an obstructive airway disease ) or to decide when the hrct examination should be performed using prone scanning ( for example for differentiating early lung fibrosis from depend lung density )  . 
radiologist is also responsible for the dose exposure to the patient that should be the smallest to obtain useful images on a quality level to perform a diagnosis and consider the type of patient and the kind of pathologies to perform a ct examination tailored both to the patient and the specific pathology characteristics . 
 regarding this issue , it is important for radiologists to know the technical possibilities of ct machines to reduce the dose exposure to patients , for example the adaptive statistical iterative reconstruction algorithms . 
for example , it is totally different to perform a ct examination on a young patient suffering from an hodgkin lymphoma ( hl ) that has a 5 - year overall survival of 96.6 % presenting the possibilities to eventually develop a radiation - induced cancer in their remaining life . 
on the other hand , it is totally different to perform a ct examination on a 65 years old patient suffering from an inoperable lung cancer where both the poor prognosis of the neoplastic disease and the age of the patient are not sufficient to warrant a survival that will eventually develop into a radiation - induced cancer in their remaining life . 
furthermore , they should personally choose the anatomical volume to be covered in relation to the clinical suspicion ( for example , in clinical suspicion of ovarian cancer , a ct examination should cover the entire abdomen and thoracic bases and be performed with a very thin collimation , even if the clinicians have only requested a pelvic ct examination , in order to depict and localise small lesions of peritoneal carcinomatosis and to eventually verify the presence of neoplastic pleural effusion ) , choose the appropriate diagnostic modality ( for example , for a thoracic ct examination radiologists should choose to perform an high resolution ct examination or not based on clinical suspicion or they should consider some additional modality to improve the ct accuracy in some neoplastic diseases , like gastric distention in gastric cancer ct staging ) , and finally choose the number of ct acquisition fig . 
3 errors in exam execution : 2d multiplanar reconstruction on coronal plane of a contrast - enhanced ct examination in two different patients during a follow - up for hodgkin lymphoma : the dose exposure to the patient was 629 dlp ( mgy - cm ) in the ct examination reported in ( a ) whereas resulted in 2793 dlp in the ct examination reported in ( b ) without a significative difference about the image quality . 
to address this type of error , retrospective analysis of previous errors as well as conducting double reading ( image is read independently by two people ) is effective [ 17 ]  . 
sensory errors , are the results , as common sense would have it , of the failure to visually register an objective , abnormal radiological finding . perceptual errors , described by kundel et al . 
classification as a scanning error or a recognition error , are included together with decision - making errors into observer errors ( see table 1 ) [ 18 ]  . 
4 errors in exam execution : 2d multiplanar reconstruction on coronal plane ( a ) and axial image ( b ) , at the level of right renal pelvis , of a contrastenhanced ct examination in a 22 - year - old man after a motor vehicle accident . 
the radiologist correctly chose to perform an excretory phase ct limiting the anatomical volume to be covered at the right renal pelvis ( c ) , because of the diagnostic suspicion of renal pelvis fracture . 
in this clinical case , the radiologist , limiting the anatomical volume to be covered in the ct excretory phase , significantly reduced the dose exposure to the patient of failure of the radiologist to fixate in the area of the lesion whereas a recognition error involves fixating in the territory of the lesion yet failing to detect the lesion . 
in particular , perceptual errors , in general , are related to multiple psychophysiological factors , including level of observer alertness , observer fatigue , duration of the observation task , any distracting factors , conspicuity of the abnormality , and many other factors [ 20 ]  . 
this type of perceptual error , called an alliterative error , occurs because the radiologist reads the old report before looking at the images , if the first radiologist missed it , the next radiologist is likely to miss it as well [ 21 ]  . 
the increased complexity of ct studies means that they take longer to review , even if , in recent years , for most radiologists , the time available to report these studies has remained static or reduced , and the time pressure this creates may lead to elements of the examination being omitted , such as a meticulous review of images on bone windows . 
these included : ( 1 ) missed vascular contrast extravasation ; ( 2 ) missed hemoperitoneum ; ( 3 ) missed right retroperitoneal and / or adrenal haemorrhage , whereas isolated errors included : ( 1 ) missed sentinel clot and mesenteric triangles ( fluid trapped between the leaves of the mesentery ) which were suggestive of a bowel injury ; ( 2 ) missed oral contrast extravasation due to bowel perforation [ 2 ]  . 1 3 790 radiol med ( 2015 ) 120 : 785794 or conversely realise a false - positive diagnosis . 
a cognitive error , is the result of the failure to correctly interpret a perceived radiological abnormality because of insufficient experience or knowledge or an underestimation of one or more other signs that would have prompted the correct diagnosis . 
 there are many reasons why radiologists make errors in exam interpretation , the most important being the vastness of the pathology and the need to know the clinical presentation , pathology and treatment of the majority of pathologies both to realise a correct interpretation of the images ( and then to perform a correct diagnosis ) and to produce an appropriate medical report ( meaning a useful report for the clinical and therapeutic management of that pathology )  . 
examples of errors in exam interpretation are the lack of an appropriate evaluation of the response to therapy in a restaging ct performed on an oncologic patient without appropriate criteria or the lack of a correct diagnosis of non - occlusive mesenteric ischaemia in a patient with a suitable clinical suspicion [ 2325 ]  . however , the exam interpretation error could be reduced , at least partially , if the correct diagnostic predictions based on clinical information were suggested . 
increases in false - positive rates by providing clinical information have also been reported [ 29 ] but this appears to be due to interpretative errors , rather than perceptual errors , since clinical information improved the detection of small lesions in another study [ 30 ]  . 
5 errors in exam execution : a thorax ct scan ( a ) and a ct scan optimised for the study of the solitary pulmonary nodule discovered on the right upper lobe ( b , collimation 0.625 mm , field of view : 10 cm , acquisition modality : axial , kernel : bone plus , kv140 , ma 330 )  . 
this clinical case demonstrates the significant difference achievable about image quality in the characterisation of pulmonary nodule using a dedicated ct technique ( in this clinical case a small lung adenocarcinoma measuring 10 mm ) besides perceptual errors , decision - making errors are also included into observer errors . 
in particular , an incorrect interpretation of a malignant lesion as a normal structure is not common in ct whereas it is more common to fail a lesion interpreted as an artefact or a benign lesion 1 3 radiol med ( 2015 ) 120 : 785794 fig . 
6 observer errors : a contrast - enhanced ct examination performed in a 60 - year - old woman during a follow - up for a previous adenocarcinoma of the colon showed an urothelial carcinoma of the left upper urinary tract ( a and b ) missed by the radiologist and discovered 2 years later because of the appearance of recurrent haematuria ( c and d )  . 
in this clinical case , the radiologist committed a scanning error medical report organisation the ct report is another important point of the medical diagnosis process and it assumes particular importance in ct examinations where the findings that radiologists could report are usually more than in any other radiological technique and often crucial for the management of the patient . 
it should be clear and concise and should firstly report the essential data about the found pathology and secondly any other collateral data that are not strictly related to the main pathology but that could also be important for the patient [ 34 ]  . 
if a precise diagnosis is not possible with the ct examination alone , radiologists should write the most likely diagnostic impression and suggest the next procedure to obtain or confirm the diagnosis . 
failure to suggest the next appropriate procedure is another achilles heel of medical reporting by most radiologists , because it is really difficult to have good knowledge of all specialities in medicine today [ 5 ]  . 
however , if the patient becomes a plaintiff in a lawsuit against the ordering physician , the radiologist can almost be assured that the ordering physician will claim ignorance as to what to do next because the radiologist did not specify what to order next [ 3 ]  . 
the american college of radiology ( acr ) practice guideline for communication of diagnostic imaging findings states that follow - up or additional diagnostic studies to clarify or confirm the impression should be suggested when appropriate [ 34 ]  . 
8 observer errors ( decision - making error ) : a contrast - enhanced ct examination performed in a 55 - year - old - man after an high - energy road traffic accident . 
the scout view ( a ) shows the incorrect position of the arms ( both on the same plane ) that prevents an optimal evaluation of a liver injury ( b )  . 
7 observer errors ( scanning error ) : a contrast - enhanced ct staging examination performed in a 65 - year - old - woman suffering from a breast cancer showed multiple liver metastasis ( a ) ; the breast lesion was also reported ( b , right breast )  . 
errors in communication are the fourth most frequent allegation against radiologists in medical malpractice claims and failure to communicate is one area in which the radiologist can take a direct role in reducing the risk of malpractice [ 35 , 36 ]  . 
when communication is not documented , the radiologist risks losing a lawsuit when there mdct represents the technique of choice for the majority of pathologies today and is responsible for the majority of diagnoses . 
despite the low number of studies dedicated to errors in mdct , ct reporting seems especially prone to generating errors [ 2 , 9 , 2628 , 33 , 38 , 39 ]  . 
the reasons for the previous sentence are numerous and from different origin : ( 1 ) the volume of imaging procedures has accelerated enormously in recent years ; ( 2 ) current ct studies frequently generate a mean value of 700800 images or more ; ( 3 ) for most radiologists , the time available to report these studies 1 3 radiol med ( 2015 ) 120 : 785794 fig . 
9 observer errors ( decision - making error ) : a contrast - enhanced ct staging , performed in a 66 - year - old - man suffering from a lung cancer on the right upper lobe ( a ) , shows a strict artefact in the superior caval vein that prevent the correct evaluation of the mediastinal lymph nodes in both stations 4r and 2r ( b , c and d )  . 
in this case , the radiologist could commit a decision - making error has remained static or reduced , in spite of evidence showing that reporting errors increase as case throughput increases and reporting time per examination reduces ; ( 4 ) ct technology expands rapidly and radiologists do not routinely receive specific and appropriate training for its use , even if technical errors represent a large part of errors in mdct ; ( 5 ) finally , ct examinations are not the same for each patient and each pathology and the choice of the most appropriate ct examination ( including the dose exposure to the patient ) presumes a very large awareness from radiologists . in conclusion , errors are an inevitable part of mdct practice . 
most of these arise during image interpretation but , differently from other radiological techniques , the awareness of radiologists regarding technical ct aspects and pathologies substantially contribute in generating errors . 
retrospective analysis of cases where an error is felt and continuous clinical and technical updates both have an educational benefit and should be considered an essential tool for improving ct diagnosis [ 40 ]  . acknowledgments the authors thank julia hassall for reviewing the english language and susanna guerrini for editorial assistance in the manuscript and images preparation . conflict of interest the authors declare that they have no conflict of interest . 
penetrating wounds can be classified into two different entities : gunshot wounds , or more technically ballistic traumas , and sharp penetrating traumas , also identifiable with non - ballistic traumas . 
the type of injuries caused by sharp pointed objects depends on the nature and shape of the weapon , the amount of energy in the weapon or implement when it strikes the body , whether it is inflicted upon a moving or a still body , and the nature of the tissue injured . 
in the assessment of hemodynamically stable patients with sharp penetrating wounds , the main imaging procedure is multidetector computed tomography ( mdct ) , especially used in complicated cases of penetrating injuries with an important impact on the final therapeutic choice . 
moscati hospital , aversa , italy 4 department of radiology , university of foggia , scientific institute hospital casa sollievo della sofferenza , san giovanni rotondo , foggia , italy 5 department of health science , university of molise , campobasso , italy keywords sharp penetrating trauma neck spine chest abdomen peripheral vascular mdct imaging introduction blunt traumatic injury consists of the largest part of civilian traumas in europe , while in the usa penetrating gunshot wounds are quite frequent [ 1 ]  . 
penetrating wounds can be classified into two different entities : gunshot wounds , or more technically ballistic traumas due to high - speed or low - speed projectiles , and sharp penetrating traumas , also known as non - ballistic traumas [ 2 ]  . 
among the spectrum of sharp pointed objects that can determine a penetrating wound , the majority of stab wounds are caused by knives , but they may also be caused by other sharp instruments or objects . 
knife wound tracks may be difficult to recognize : it is crucial for the radiologist to discover the wound track , its extension and its relationships with the surrounding organs . 
imaging , especially multidetector computed tomography ( mdct ) , is of key importance in the assessment of stab wounds , with a crucial role in guiding the final therapeutic choice . 
the aim of this review is to illustrate the range of different imaging findings related to non - ballistic penetrating trauma in the emergency setting ; legal aspects related to sharp penetrating injuries are also discussed . sharp penetrating injuries to the head head penetrating injuries can be classified as non - penetrating ( superficial or tangential ) , penetrating ( object 1 3 radiol med ( 2015 ) 120 : 856865 penetrates and remains within the calvarium ) , and perforating ( object penetrates and exits the calvarium ) [ 3 ]  . 
the main objective in the clinical and imaging evaluation of the patient is to locate the whole intracranial section of the sharp tool , highlighting its relationship with vital areas of the nervous system , such as the brain stem and cranial arteries and veins , either located inside and outside of the skull [ 4 ]  . 
radiologist should identify the presence of the entry wounds , which are multiple in many cases , fragmented and non - fragmented bone lesions , foreign bodies , pneumocephalus , and intracerebral or even intraventricular bleeding . 
considering that many vessels of major importance are lodged in the head , and that a foreign body might hit them in its course , causing vascular damage and hemorrhage , a head mdct angiography ( mdcta ) should be performed during the course of the primary assessment of the patient , in spite of possible artifacts . 
such damage may occur extracranially in the cervical region , along the intraosseous course of the carotid artery within the skull base , along the course of the vertebral or basilar arteries , or to major intracerebral fig . 
moreover , considering that primary brain injuries are severe but secondary brain injuries can even be worse in terms of prognosis , after excluding the presence of metallic foreign bodies , magnetic resonance imaging ( mri ) is to be chosen to further and better assess the patient [ 2 ]  . 
 traumatic cerebral edema , hydrocephalus , post - traumatic ischemic stroke , compression of the ventricular cavities and low parenchymal attenuation , carotid - cavernous traumatic fistula , intracranial dissection due to growing hematomas in the vascular wall , and brain death are all complications of a brain penetrating injury [ 2 ]  . sharp penetrating injuries to the spine penetrating non - missile spine traumas might be due to criminal inflicted injury or unintentional impalement . 
 [ 5 ] reported that they account for just the 25 % of the whole of the spine lesions ( road accidents and gunshot lesions being the most frequent ) , especially concerning the thoracic region . 
very small metallic fragments belonging to the foreign offending object might not be recognized on the plain film or at the ct scan [ 4 ] ; these fragments are identified at mri , because they cause the presence of small areas of susceptibility artifacts . 
in the emergency setting , in the presence of penetrating traumas , therapeutical options are to be chosen after considering the neurological performance of the patient , evaluating the severity of bone and ligamentous lesions and the stability of the spine , assessing the path traced by the offending object and the degree of canal involvement , and locating any retained fragments [ 10 ]  . 
surgical treatment in spinal penetrating traumas can be opted for in the presence of progressive neurological deficits or continuous cerebrospinal fluid leakage , or when there is imaging evidence of spinal compression with no nervous symptoms [ 11 ]  . sharp penetrating injuries to the neck lesions of the neck vessels are most commonly due to penetrating injuries . 
the major vessels of the neck , especially the carotid artery which is injured in 510 % of arterial lesions , are frequently damaged by sharp penetrating injuries [ 12 ]  . 
3 a mri examination shows increased cord signal at the c2 level indicating edema with associated bleeding ( b ) due to fracture of the posterior arch ( c , ct scan ) diagnostic assessment in hemodynamically stable patients with penetrating neck traumas . 
considering that the neck is packed with vital areas , and in the case of nervous , respiratory , and vascular damage , a quick clinical decline is absolutely possible . 
4 cross section of neck cta scan showing different three entrances of wound tract ( a , arrows ) and multiple gas bubbles delineating the wound track ( b , arrows ) without vascular damage admission in the emergency setting , patients with quickly increasing hematomas , pulsatile hemorrhage , declining neurological performance , need no further diagnostic assessment and are brought directly to the operating room [ 1315 ]  . managing patients with stable vital signs is controversial [ 16 ]  . 
routine neck exploration of all wounds penetrating the platysma is not performed because results are often negative and the procedural morbidity reaches 51 % [ 17 , 18 ]  . 
cervical spine radiographs , ultrasound , angiography , bronchoscopy , esophagoscopy , and contrast swallow studies can be expensive and time - consuming and have a low yield [ 16 ]  . 
using mra has been described in the setting of cervical spinal cord injuries where mra can be added to assess for vascular injury [ 20 ]  . direct signs of arterial injury on mdcta include rapid changes in caliber , contrast extravasation , irregular margins , and filling defects within the vessel lumen . 
indirect findings suggesting damage to blood vessels consist of confusion in the fat planes around the vessels , perivascular hematoma , or bone fragments within 5 mm from a major vessel . 
frequently , when metallic fragments are situated near to the vessel , streak artifact obscures anatomic details and direct signs of wound [ 19 ]  . mdcta of the neck can be limited by a variety of artifacts and technical limitations . 
beam hardening artifact from the shoulders of fat patients , vascular calcifications , metallic foreign bodies , and contrast in the subclavian vein can obscure details at the base of neck [ 16 ]  . 
in addition to the artifact from the shoulders and venous contrast , the path of the subclavian artery in the axial plane makes its assessment difficult on axial images [ 16 ]  . sharp penetrating injuries to the chest pulmonary , pleural , and chest wall are involved in between 88 and 97 % of patients with chest penetrating trauma [ 21 , 22 ]  . 
a pivotal part in the diagnostic assessment and therapeutical management of patients with thoracic penetrating injuries is played by diagnostic imaging . up to 62 % of patients referring to the emergency department with penetrating thoracic trauma present with no symptoms and a first negative chest plain film [ 2 ]  . 
the fact that the complications tend to appear with a delay is well known , even in patients with a negative first radiograph : in fact , 812 % of these patients tend to develop complications in the subsequent 5 days [ 23 ]  . 
chest plain films are usually satisfactory enough to diagnose simple rib fractures , and therefore , further imaging assessment is 1 3 860 radiol med ( 2015 ) 120 : 856865 fig . 
c sagittal view of ct scan ; arrows are pointing at muscle hematoma of the thoracic wall and massive hemothorax 1 3 radiol med ( 2015 ) 120 : 856865 fig . 
cross section of cta scan : arrows evidence of air bubbles in the left thoracic wall ( arrows ) without vascular injuries followed by stab wounds , and 22 % involve multiple chambers ; overall survival approximates 30 % with markedly improved odds after stab wounds ( 65 % ) and significantly decreased survival after resuscitative thoracotomy ( 14 % ) [ 28 ]  . 
while mortality after penetrating cardiac injuries is considerable , patients can rarely present with normal vital signs [ 29 ]  . mdct is an important procedure and plays a key role in the detection of hemopericardium in patients with chest penetrating traumas and can expose wound paths , pericardial and / or myocardial abnormalities , pneumopericardium , and heart herniation [ 29 ]  . in case of traumatic aortic damage , as for other arterial injuries , mdct is being steadily used as the primary imaging technique ; angiography is reserved for selected cases only . 
in road accidents with penetrating lesions , lower neck or upper chest injuries , instrumental tests , heavy emesis or foreign object ingestion , and oesophageal injuries are to be suspected , even though are not so common . 
oesophageal lesions are to be investigated and followed up over time with mdct , first and foremost ; it is the first imaging modality to be used , especially in the mapping of lesions that can be treated without a surgical approach [ 30 , 31 ]  . diaphragmatic injuries represent 15 % of all thoracic and abdominal lesions ; blunt traumas tend to determine greater and more easily detectable lesions , so that the diagnosis can be made rather early [ 32 ]  . 
penetrating traumas determine lesser lesions that are usually diagnosed later : the incidence of late detection being 836 % in penetrating traumas , and much lower , 314.6 % in blunt traumas fig . 
in terms of detection of a pneumothorax and sensitivity , and in the identification of the incorrect position of the thoracostomy tube , e.g. , outside of the chest or inside the pulmonary parenchyma , mdct is superior to the plain film [ 25 ]  . sharp penetrating thoracic traumas with an entry wound that can be defined as juxtacardiac , that is , placed in an area defined by the two midclavicular lines on the sides , clavicles , and costal margin , may definitely damage the heart , intrapericardial aorta , and pulmonary vessels [ 2 ]  . 
sagittal and coronal mdct reconstructions significantly improve the accurate diagnosis of a diaphragmatic lesion [ 36 ]  . abdominal and gastrointestinal tract sharp penetrating injuries to better assess the actual need of a surgical treatment in patients with abdominal penetrating injuries , the specific option to be considered is a triple - contrast ( oral , intravenous , and rectal contrast ) mdct of the abdomen [ 2 ]  . patients with penetrating wounds to the flank may silently harbor injuries to retroperitoneal structures without evidence of peritonitis . 
in the event of a lesion inflicted with a knife , the tool must pass through the vessel to determine damage such as vessel laceration , pseudoaneurysm formation , blood loss , limb thrombosis , ischemia or necrosis , arteriovenous fistula with or without high - flow cardiac failure [ 2 ]  . the prognosis of vascular damage inflicted by penetrating injuries is significantly better than that of vascular lesions in blunt trauma [ 43 ]  . foreign objects and bone lesions that may cause neurovascular compromission might be detected using a plain film : high - velocity weapons , like other causes of highenergy trauma , cause severely comminuted fractures with extensive soft tissue injury . 
low - velocity weapons may result in no fracture or only minimal fracture when the bullet hits the bone . the accuracy , specificity , and sensibility of mdcta are rather high , reaching up to 90 % for diagnosing traumatic vascular injury [ 2 ]  . sharp penetrating injuries : legal aspects sharp penetrating injuries have been known for a long time . 
the type of injury caused by some mechanical force depends on the nature and shape of the weapon , the amount of energy in the weapon or implement when it strikes the body , whether it is inflicted upon a moving or a still body , and the nature of the tissue injured . 
cross section of unenhanced ct scan ( c ) and enhanced ct scan ( d ) : arrows are pointing at air and muscle hematoma with free air in abdomen . 
deliberate stabbings , either self - inflicted or perpetrated by others , are steadily increasing and common , and are to be considered a tangible social issue [ 45 ]  . traumas carry both medical and legal repercussions ; in the case of head traumas , things are even more obscure , because the actual entity of the damage cannot be evaluated rapidly , but generally after some time from the day of the injury . the degree of penetration , which might involve just the scalp , scalp and calvarium , or even the deeper structures 1 3 864 radiol med ( 2015 ) 120 : 856865 fig . 
this article is published with open access at springerlink.com abstract post - mortem computed tomography ( pmct ) has been proven for its appropriateness to become an integral part of routine pre - autoptic forensic investigations either in the field of forensic investigation of fatal medical error or in hospital quality management . 
the autoptic investigation of unexpected and peri - interventional deaths can be usefully guided by post - mortem imaging which offers significant added value in the documentation of misplacement of medical devices before dissection with the risk of artificial relocation and the detection of iatrogenic air embolis post - mortem ct angiography ( pmcta ) augments pmct in the search for sources of hemorrhages and for the documentation of vascular patency and unimpaired perfusion after general and cardiovascular surgery or transvascular catheter - assisted interventions . 
thromboembolic complications including pulmonary embolism , the differentiation of ante and post - mortem coagulation and the detection of myocardial infarction remain areas with compromised diagnostic efficiency as compared to autopsy . 
post - mortem imaging * axel heinemann heinemann@uke.de institute for legal medicine , university medical center hamburg - eppendorf , butenfeld 34 , 22529 hamburg , germany could also assume a new role as an alternative in a clinicopathological setting if autopsy is not achievable when the probability in the individual case is acceptable to answer specific questions . keywords medical error fatal outcome forensic radiology post - mortem ct post - mortem ct angiography introduction during the last 10 years , post - mortem computed tomography ( pmct ) has developed to become a tool for routine work in more and more institutes of forensic medicine across europe and worldwide [ 18 ]  . 
pmct complements the internal examination of the body by being implemented in pre - autopsy routines while new techniques are under development for post - mortem application and the new subspecialty of forensic radiology is developing [ 9 , 10 ]  . 
 there are a lot of forensic scopes of application for imaging methods but pmct attracts the most attention in the forensic scientific community due to its easier accessability and greater significance in skeletal diagnosis in comparison to other methods . 
the use of imaging for the detection of errors in treatment dates back to 1895 , when it was first accepted as evidence in court [ 11 ]  . there is a rising number of reports about the advantages of post - mortem imaging in cases with fatal outcome after medical intervention [ 1218 ]  . 
autopsy can be guided by pmct not only in case of skeletal trauma but also by typical features like fatal complications after medical treatment such as misplaced catheters , guidewires , tubes and drainages , sources of interventionrelated hemorrhages and gas embolism . 1 3 836 radiol med ( 2015 ) 120 : 835845 hence , pmct shows the potential to become a valuable tool that adds further information after unsuspected in - hospital deaths even if an autopsy diagnosis is not achievable due to patient / family consent [ 15 , 19 ] , inoculation risks or ethnic doctrines [ 2022 ]  . 
however , post - mortem imaging has not been established yet as an acknowledged tool for quality control in hospitalswhich may be due to the fact that unlike to the forensic pathologists the interdisciplinary cooperation between radiologists and clinical pathologists has not been established yet at a significant level in many countries . taking into account the experiences of forensic radiologists and forensic pathologists with the application of postmortem imaging in the assessment of suspected medical malpractice , pmct has established its role for radiologically accessible morphological findings which are indicative for or against an iatrogenic injury caused [ 17 ]  . 
the limited validity for a range of typical causes of death can be enlarged by combination with ct angiography and magnetic resonance imaging [ 7 , 15 , 23 , 24 ]  . since some years , post - mortem ct angiography has expanded the range of options in the reconstruction of potential medical error since it facilitated the search for hemorrhage sources [ 16 ] as well as the documentation of an impaired or unimpaired perfusion after different sorts of surgery and intervention [ 7 ]  . 
key criteria for the decision to perform post - mortem imaging and for its interpretation can be obtained from the preliminary inspection of the medical history of a deceased patient [ 13 ]  . methods in the hamburg institute of legal medicine , over a period of 6 years about 2000 pmct investigations have been performed after in - hospital deaths . 
the responsibility of the institute of legal medicine for the morgue includes fatalities with unknown manner of death from the city of hamburg but also all in - hospital deaths from the university medical center hamburg - eppendorf . 
this enables the postmortem ct examination on request by clinical colleagues in cases of naturally certified deaths as well as in cases in which public prosecution decides to stop further investigations in primarily certified unclear manner of death . 
a wholebody ct from top to thigh ( slice thickness 1 mm , pitch 1.5 , 130 kv , 180230 mas ) is the standard ; additionally , dedicated scans of the cranium , the brain and the thorax with higher resolution ( slice thickness 0.8 mm , pitch 1.0 , 130 kv , 180230 mas ) may complement the exam . 200 hospital fatalities have been examined with multiphase post - mortem ct angiography ( mpmcta ) after performance of pmct according to reported standard methods [ 25 ]  . 
the interpretation was made by a board certified radiologist , assisted by a board - certified forensic pathologist . fatal outcome in clinical settings : common case groups intensive care unit and emergency medicine post - mortem computed tomography contributes greatly to perpetuate evidence of the position of foreign bodies at time of death and before any autopsy procedure could artificially displace it . 
it remains challenging in pmct to detect a source of gas / air escapes , especially in the thoracic and abdominal cavity but following their 3d - path in soft tissues has advantages over the autopsy . 
the transvenous placement of central venous lines , gastric tubes and electrodes from cardiac pacemakers or defibrillators with irregular loops and bending or misplaced pleural drainages are quite illustrative on 3d reconstructions . 
figure 1ad illustrate the misplacement of a sheldon catheter perforating bilaterally small arterial branches at the base of the neck resulting in massive swelling with fatal upper venous congestion and respiratory failure . in intensive care units , ventricular assist devices , aortic balloon pumps and extracorporal membrane oxygenation ( ecmo ) systems have become increasingly in use in patients with cardiac and respiratory failure as a bridge for recovery , transplantation or ultima ratio . 
depending on the type of system used , conclusions can be drawn on the underlying organ dysfunction in the terminal phase of life of the patient ( left or right ventricular assist , venovenous for respiratory or veno - arterial ecmo for cardiac support )  . coronary angiography and transvascular cardiac interventions after percutaneous coronary intervention ( pci ) , the myocard sometimes shows an enhancement which seems to be 1 3 radiol med ( 2015 ) 120 : 835845 fig . 
conclusion obviously , the aberrant catheter tip damaged the right , but also left inferior thyroid artery crossing even the midline of the neck ( there was no indication for an additional leftside skin lesion or jugular puncture ) due to contrast medium deposits that still have not been washed out completely . 
if these areas correspond to the drainage of a coronary artery , this may be taken as an indication for sudden interruption of coronary perfusion before death or immediate cardiac arrest after contrast medium application . if a series of gas bubbles is observed in a coronary artery after fatal outcome during a pci procedure , it should be clarified if a gas embolism could have happened even though safety devices should prevent unobserved gas bubble transport through the angiography catheter . 
emergency treatment with covered stents in the position of the rupture of the vessel wall may impede the post - mortem demonstration of leakage sometimes ; if not , the bleeding , its amount and its origin can be detected . pmcta may rarely fail to demonstrate the exact source of a bleeding which resulted in a cardiac tamponade . 
the tamponade is usually firmly clotted in these cases and prevents contrast medium from leaking out of a rupture due to the massive pressure in the pericardial sac and adherence of blood clots to the surface of the traumatized tissue . transvascular valve placement refers predominantly to the transcatheter aortic valve implantation ( tavi ) which utilizes bioprostheses made of bovine pericardium mounted on a balloon - expandable stainless - steel or cobalt - chromium 1 3 838 radiol med ( 2015 ) 120 : 835845 perforation into the pericardial sac with resulting tamponade . perforation into the mediastinum and / or the pleural space if the rupture continues above the level of the pericardial reflection lines on the great vessels . pmcta facilitates the diagnosis by following the path of extravasated contrast agent . endovascular aneurysm repair endovascular aneurysm repair ( evar ) has been widely adopted for abdominal aneurysmsextendable into the iliac arteriesand thoracic ( tevar : thoracic evar ) aortic aneurysms . 
the blood flows through the endograft which represents an artificial lumen reducing the pressure in the aneurys there is a growing application of endovascular graft stenting even in emergencies with ongoing aneurysm ruptures or aortic dissections . a major cause of complications in abdominal evar is the failure of the seal between the proximal , infra - renal aneurysm neck and the endovascular graft ; unsuitable fit between the aortic wall and the graft with compromised seal and an instable anatomy may elevate the risk [ 26 , 27 ]  . 
in general , pmcta demonstrates a high cardiovascular morbidity including cerebral infarctions in these patients . general and cardiothoracic surgery the diagnostic value of pmct ( a ) after fatal outcome of open surgical interventions is generally much higher with the detailed knowledge of the preexisting morbidity , the sequence of ante - mortem interventions and preceding complications to the last operation . 
2 a 71 - year - old female patient was admitted in a hospital emergency room due to severe chest paon the day after acute cardiac failure occurred during coronary catheterization which had been performed due to abnormalities in ecg . 
diagnosis aortic dissection type de bakey i originating in the ascending aorta , propagating in the innominate artery and thoracoabdominal aorta until the bifurcation , perforating into the pericardial sac , mediastinum and left pleural cavity . 
the positioning of the valve , its relation to the coronary ostia with potential constriction effects and the unimpeded perfusion of the aortic outlet as well as signs of incompatibility of the aortic diameter and the expanded frame with the risk of valve insufficiency can be visualized by pmcta . 
the lower border of the valve graft is at risk to interfere with the anterior sail of the mitral valve and its papillary suspension which is observable via 3d reconstruction and virtual endoscopy [ 13 ]  . the valve may be implanted via a transfemoral or transapical approach which could result into additional suturing problems at the points of sheath / catheter entry after termination of the intervention . 
pmct / pmcta demonstrates resulting hemorrhages into the soft tissues of thigh and retroperitoneum ( transfemoral approach ) or into the pleural space and into the mediastinum ( transapical )  . a catheter - induced trauma may also refer to balloon dilatations of the aortic valve , to transcatheter approaches of the mitral valve such as annuloplasty and mitraclip or to catheter radiofrequency or cryoablations , mostly at the level of the openings of the pulmonary veins into the left atrium for the treatment of cardiac arrhythmias . these procedures may result into perforations from one into another cardiac chamber . myocardial contrast medium deposits in case of incomplete disruptions . 1 3 radiol med ( 2015 ) 120 : 835845 fig . 
3 ad a 76 - year - old male patient had received a hybrid intervention due to an aneurysm of the thoracic and abdominal aorta 2 years before he died from cardiac and respiratory failure . 
blue arrow replacement of ascending aorta , major thoracic branches sewed on the prosthesis ; red arrows fenestrations for renal arteries , reinforced with proximal stents ( snorkel / periscope technique )  . 
d 3d reconstruction in a front left view with celiac artery bypass ( 1 ) , superior mesenteric artery snorkel ( 2 ) and extravasation of contrast agent [ ( 3 ) , endoleakage ] clinical pathology , but it is not self - evident in the forensic area for the time of post - mortem reporting . a typical scenario of suspected medical error is a challenged decision to wait and see instead of starting surgical exploration in case of abdominal pa figure 4ad illustrates a case with unexpected death after inconclusive diagnostic approaches . the majority of patients following thoracotomy or laparotomy - based adverse events die of protracted multi - organ failure with circulatory shock . 
pmct shows laparotomyrelated complications of abdominal surgery such as postoperative ischemia of the bowel with indirect radiological signs as in the living , a paralytic ileus with bowel distension and the presence of multiple gasfluid levels . 
peritonitis from suture insufficiency after bowel resection , postoperative respiratory failure with pneumonia , wound infections with abscess formation or pyelonephritis are suspected reasons for a septic multi - organ dysfunction syndrome but mostly pmct offers indirect signs of these conditions only . general soft tissue edema as well as fluid in the peritoneal and pleural cavities is indicative of failure of kidneys , heart and liver . 
the extracardial distribution of contrast medium deposits in the kidneys or in extra - renal organs indicate ante - mortem contrast enhanced imaging in excretion mode - dependent shortterm intervals before death and creates an impression of the extent of renal failure . hemorrhages from dehiscent vessel anastomoses or ligatures after resections of abdominal organs are visualized ; however , a collapse of major vessels as a sign of hemorrhagic shock is usually missing because of massive transfusion or hyperhydration . liver failure is associated in pmcta with a general elevated tissue enhancement and simultaneous enhancement of arterial and portal structures on the arterial phase images indicating the presence of open arterioportal venous shunts . fatal outcome after preceding liver transplantation could be due to hepatic artery / portal vein stenosis or thrombosis which are caused by rejection , clamp injury , 1 3 840 radiol med ( 2015 ) 120 : 835845 fig . 
the patient died of paralytic ileus due to mesenteric infarction which had been accompanied by cardiac failure with myocardial ischemia intimal injury by perfusion catheters or anastomotic ischemia due to a disrupted vasa vasorufigure 5 demonstrates a dehiscence with hemorrhage at the site of the portal vein anastomosis and a disconnected hepatic artery anastomosis in a patient dying in the operating room of acute transplant failure with reperfusion syndrome . coronary bypass surgery includes aortocoronary venous bypasses , left internal mammary artery ( lima ) and right internal mammary artery ( rima ) bypasses which are identified in pmct by clips in characteristic formation [ 12 ]  . 
pmcta illustrates the patency of the vessel as well as of calcifications and stents in the graft . gastroenterology the diagnosis of gastric or duodenal ulcers could involve the forensic question how successful a laceration of a bleeding artery at the ulcer bed has been terminated by gastroduodenoscopy . 
even at autopsy given the sutured ulcer bed this question may be difficult to assess if gastric and bowel contents do not allow to differentiate within a short time interval . 
pmcta helps to identify the sufficiency of vessel closure if not hindered by unspecific contrast extravasation due to post - mortem gastric mucosal destruction . retrograde cholangiopancreatography ( ercp ) may be complicated by a rupture of bile duct or endoscopic 1 3 radiol med ( 2015 ) 120 : 835845 fig . 
displaced catheter for haemodynamic monitoring in the right atrium with irregular loops ( 2 ) , the tip finally propagating retrogradely through the superior vena cava and the brachiocephalic vein into the left superior mediastinudisconnected hepatic artery anastomosis with ligated recipients supplying artery ( 3 ) as an ultima ratio for intraoperative temporary limitation of reperfusion effects ( in the intraoperative state , the donors proximal common hepatic artery had been sewed on a branch of the recipients superior mesenteric artery )  . 
aorta ( 6 ) pancreatic duct which causes post - ercp pancreatitis , often promoted by papillotomy or by sampling of suspicious adjacent tissues by endosonographically guided fine - needle aspiration . 
the post - mortem pmct diagnostic criteria are direct and indirect signs of bleeding , edema of pancreas and surrounding tissues and accentuation of the renal fascia ; in exceptional cases this is combined with the risk of air embolism if gas insufflation into the duct system has not been stopped in time . specific complications such as a compromised organ perfusion by relocation of vessel disposals should be proved by means of mpmcta . 
this is also true for hemodynamically significant dissection or leakage . neurosurgery pmct after neurosurgical interventions refers to hemorrhage , stroke and traumatic brain injury , the latter indicated by fracture lines , coup and contrecoup lesions . 
the early post - mortem change with dedifferentiaton of gray and white matter of the brain in pmct as well as an impaired rendering in the posterior cranial fossa limits sometimes the diagnostic validity and post - mortem mri could sometimes be the better option for guidance of neuropathological examinations . 
the usual procedure in the majority of cases is a forensic autopsy the result of which is commonly used with the preliminary information from the medical files of the patient to decide whether a peer review for the final evaluation of the case in question is needed . if the patient dies from the effects of treatment failure , negligent homicide , grievous bodily harm with lethal consequences or even manslaughter come into consideration . 
nevertheless , this process has an acknowledged effect with regard to secondary medical error prevention [ 29 ]  . frequent underlying causes of medical errors are lack of error culture , possibilities for confusion ( drugs , right left confusion , mistake of patients ) , communication errors among those administering treatment , workload , lack of clarity about the responsibilities and inadequate patient monitoring . 
note the contrast agent enhancement in the right posterior lobe ( arrows ) representing a potential source of hemorrhage hospital , sometimes in the context of medical malpractice allegations , are sudden and fatal deteriorations after surgical and minimally invasive intervention , delayed or fault diagnosis and treatment , death after failed resuscitation ( suspicion of delayed action , inadequate performance , particularly problems with intubation ) , and generally a mismatch between low estimated and risk fatal outcome . 
however , under - / overdosage of medical drugs necessitate toxicological investigations and allergic reactions to medical drugs and contrast agents will be evaluated mainly by medical history and laboratory markers . a decline of clinical autopsies results in an overestimation of the sensitivity of clinical ante - mortem diagnosis [ 21 ]  . 
the application of pmct in case of deceased patients from an intensive care unit at a university medical center shows a high accordance rate of clinical major and minor diagnoses between imaging and autopsy results and pmct may supplement clinical diagnoses in cases of missing autopsy [ 17 ]  . 
the same setting was investigated for the efficiency of pmctathis study found a confirmation rate of 93 % of all diagnoses identified from ante - mortem medical records for pmct / pmcta as compared to a rate of 80 % for conventional autopsy . 
the higher accordance remained true even in the subcategory of cardiovascular diagnoses ; however , a major limitation was still that ante - mortem known myocardial infarctions were confirmed in pmcta by potential coronary culprit lesions only [ 18 ]  . mpmcta turns out to be a new method with a highly standardized and evaluated methodology [ 7 , 25 , 33 ] which is more easily implementable in pre - autopsy practice than post - mortem cast angiography with silicone which also proved to discover graft twists after bypass surgery remaining undetected at autopsy [ 34 ] , to detect fresh cerebral infarctions as well as neurovascular main stem thrombosis , aneurysms and arteriovenous malformations [ 14 , 34 , 1 3 radiol med ( 2015 ) 120 : 835845 35 , 36 ]  . 
in case of infectious complications imaging can facilitate sterile post - mortem puncture of radiologically suspicious areas for microbiological investigations before autopsy [ 37 ]  . multiphase post - mortem ct angiography contributes to the detection of hemorrhage sources even in cases in which autopsy fails [ 7 , 14 ]  . 
hence , as compared to trauma cases in forensic daily routine medical error cases often challenge the forensic pathologist at autopsy with the preponderance of discrete bleeding sources in small arterial branches venous leakages without recognizable lacerations of small venes / venoles , which is typical for the renal bed , mesenterial veins and venous plexus in the pelvic region bleedings through miniscule defects caused by perforations with tiny instruments such as catheter tips multiple bleeding sources which succeed each other at varianother obstacle is the early post - mortem change [ 41 ] with hypostatic fluid transgression between different anatomic compartments which result in diagnostic pitfalls in the radiological assessment of the lung . 
depicting the heart by pmct at different post - mortem intervals demonstrates considerable changes in volume and tension as well as alterations in shape and position either ; for the diagnosis of terminal or chronic dilation , dilatative and other cardiomyopathies a degree of caution is strongly advisable [ 13 ]  . arrhythmogenic cardiac deaths due to coronary heart disease are a further example of the limits of current postmortem imaging [ 17 ]  . 
however , the conventional approach to certify a sudden cardiac death by safeguarded exclusion of a common standard set of alternative causes of death would be unreliable based solely on imaging . ous time points conclusions the concept of mpmcta distinguishes arterial and venous sources nevertheless early venous enhancement does occur in the arterial phase , particularly in the portal vein [ 38 ]  . 
the intensity of the leakage of contrast medium into body cavities frequently corresponds to the extent of vessel damage ; however , this is not necessarily the case in soft tissues when ante - mortem extravascular hemorrhage exerts a compressive effect or has coagulated . due to the reluctance of medical doctors concerning informed autopsy consent and inadequate prioritization by the legislature [ 39 ] post - mortem imaging should assume a new role as an alternative . 
this could apply for unexpected deaths in the context of medical treatment ; however , the necessary standardization of protocols for pmct and post - mortem magnetic resonance imaging ( mri ) is still pending [ 21 ]  . limitations of pmct the evidence for an isolated use of the results of postmortem imaging in forensic cases is still limited : autopsy remains the gold standard for the morphological diagnosis of thromboembolic complications as post - mortem imaging is restricted to probabilistic approaches concerning the quality of obliterating material in a vessel . 
myocardial infarction remains an autopsyand histology - based diagnosis [ 30 ] even if mpmcta indicates sometimes myocardial damage and post - mortem mri could help with promising indications for peracute myocardial damage [ 40 ]  . post - mortem cross - sectional imaging has demonstrated essential benefits as an adjunct to forensic autopsy . 
the availability of these techniques should be considered in appropriate cases . post - mortem imaging allows comparisons with antemortem imaging in individual cases and could help in the experts delimitation of ex ante and ex - post judgements by clarification of situational conditions in the very moment of a challenged medical action or decision . taking into account the still limited availability of expertise in post - mortem radiology , a cooperative assessment via teleradiology expert networks could be a preferable option [ 42 ]  . the combination of imaging and autopsy , histology and toxicology could enhance the cost efficiency of criminal proceedings by accelerated setting the course and avoidance of costly follow - up assessments [ 14 ]  . 
furthermore , multimodal post - mortem examinations providebeyond the forensic scopea new opportunity to place an emphasis on clinical mortality analysis according to quality management principles . compliance with ethical standards conflict of interest none of the listed authors declares a conflict of interest . 1 3 844 radiol med ( 2015 ) 120 : 835845 ethical statement all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
as is shown , the results of evaluation of post - mortem computed tomography allow better diagnosis , documentation and visualisation of forensic examinations . keywords post - mortem examination forensic autopsy forensic radiology post - mortem computed tomography homicide investigation introduction in everyday clinical work , it is obvious that any doctors activities regarding the patient have to be reported accordingly in medical records . 
due to the fact that a very special kind of evidence is under examinationthe human corpse , it is only possible to do it completely once : any consecutive examination will have limitations due to previous autopsy procedures as well as changes due to decomposition , and in some cases it would even be impossible to repeat the examination due to cremation of the corpse . 
at present , due to technological developments , we have another opportunity to take advantage of different means of digital data collection , enabling us to register the actual state of the cadaver ( in three dimensions3d ) before it is changed due to conventional autopsy procedures , including photogrammetry and laser scanning , post - mortem computed tomography ( pmct ) , and post - mortem magnetic resonance imaging ( pmmr ) [ 14 ]  . 
these methods are related to the registration of both external and internal changes , giving us the unique opportunity to make the autopsywhich can be performed fully only onceinto a kind of repeatable examination , with the ability to analyse the same information at a later time . 
among them there are a 1 3 radiol med ( 2015 ) 120 : 846855 considerable number of autopsied cases related to accidental violent death , as well as sudden and unexpected death due to disease . 
as is widely known for forensic pathologists , the purpose of forensic autopsy is not only to reveal the actual cause of death , but to secure evidence related to other important problems , including estimation of the time of death , verification of the identity of the victim , recording the injury patterns , identification of the weapon of crime , etc . 
the data obtained during postmortem examination , combined with the information from the files of the case , are necessary for the forensic reconstruction of the event . postmortem imaging in modern forensic investigation of death cases laser scanning and photogrammetry are methods useful not only for registration of external body changes ( they are the best for this purpose ) , but also for gathering valuable data from the scene where the body was found , as well as relating to the possible weapon of crime [ 7 , 8 ]  . 
by comparing with further investigation data , a reconstruction of the event can be shown [ 10 , 11 ]  . regarding internal examination , it refers to pmct and pmmr . 
 pmmr , on the other hand , is much more time consuming and expensive , but it is of a bigger efficiency when it comes to evaluating changes in soft tissues . 
 [ 16 ] reported the finding of an occult gunshot wound of the face with pieces of the projectile ( it was irrelevant to the actual cause of deathtension pneumothorax )  . 
in some cases , the findings can even lead to primary conclusions about the cause of the ( violent ) death ( aspiration of blood [ 17 ] , haemopericardium [ 18 ] as in fresh corpses we are able to differentiate body fluids [ 19 ] )  . 
2 a case of a victim of homicide due to blunt trauma to the head : a volume rendering technique ( vrt ) reconstruction based on native pmct , left anterior viewfragmentation of the facial part of the skull with the line of fracture going to the back part of the skull , tooth dislocation ( arrow ) , b thin mip in oblique axial plane showing aspiration of blood and a foreign bodythe tooth on the right side ( arrow ) fig . 
3 axial slice based on native pmctthe neck of a victim of homicide with subsequent burning of the corpse : lack of integuments , fractured mandible , a foreign body ( the projectile ) at the back ( arrow ) this can even be done remotely by other doctors . 
 pmct data give us the opportunity to make a visualisation of both external ( mostly localisation without specific features , due to limitation of the method ) and internal changes , which can be understandable and emotionally secure for non - professionals . 
eventually , it will be possible to prepare models by 3d printing for better understanding of important aspects of forensic investigation [ 29 ]  . radiol med ( 2015 ) 120 : 846855 gunshot injuries at the present time , we can strongly state that the gold standard for forensic post - mortem examination in cases of gunshot injury is forensic radiology combined with conventional autopsy . 
the pmct examination has to be performed prior to conventional autopsy ( both external and internal examination ) in some cases the best order would be pmct between conventional external and internal examination . 
the possibility of finding the location of external injuries in pmct examination is more likely when the wounds are located in the anterior or sides of the body when the corpse was lying face up during acquisition , without covering by layers of clothing soaked with blood . 
in a number of cases , the results of native pmct can help with the differentiation between the entrance and the exit wounds : by the shape of injuries , comparison between ( two ) external injuries on different sides ( areas ) of the corpse and the location of displaced pieces of broken bones . 
with the application of pmctangiography ( pmcta ) [ 30 , 31 ] , we have the opportunity to see the location of wounds by focal extravasation of contrast mediu metal objects ( such as lodged projectiles ) can be indicated quite easily in native pmctrecovered projectiles are valuable pieces of evidence . 
in many cases , it is easy to obtain the pattern of the whole injury track of the head if there are injuries of the skull especially with 1 3 849 radiol med ( 2015 ) 120 : 846855 fig . 
4 cases of pneumothorax : a thin mip in axial plane of a victim of homicide due to multiple blunt injuries to thoraxfractured ribs on both sides , bilateral pneumothorax , collapsed lungs , gas spaces between layers of soft tissue of the chest , b thin mip in coronal plane based on pmcta at the arterial phase : tension pneumothorax on the left fig . 
injuries of the brain at the location of cavitation ( with air bubbles , pieces of broken bone , or even blood ) can be shown based on native pmct . 
 the most problematic are missile injuries of the abdomen . in some cases , the direction of fire does not simply reflect the closest path between the entrance wound and the location of the missile / exit wound , because the bullet can be deflected due to contact with bones . 
 [ 32 ] reported pmcta in a case of firearm injury of the heart . the papers referring to the post - mortem imaging in ballistic trauma are scoped on feasibility of the methods fig . 
6 thick mip reconstruction in coronal plane based on pmcta at the arterial phase : the path of the projectile in a case of the immediate vicinity gun shot ( perforating from the right to the left ) shown by broken bones ( with bevelling ) and extravasation of contrast medium 1 3 850 radiol med ( 2015 ) 120 : 846855 fig . 
7 thick mip reconstruction in oblique sagittal plane based on the pmcta at the dynamic phase : the knife left inside the body , perforating the heart and the stomach ; contrast medium extravasation to the pleural cavity [ 33 , 34 ] as well as case reports [ 3537 ]  . 
a research paper was presented referring to the problem of distinguishing between ferromagnetic and non - ferromagnetic projectiles , which could be an important step in the preparation of the corpse for pmmr examination in projectile injury cases by native pmct examination [ 39 ]  . sharp trauma cases in general , sharp trauma cases can be even more complicated than ballistic trauma casesdue to the parameters of injuries inflicted mainly by knives . 
for the estimation of the injury track , we can utilise the presence of air spaces , gas bubbles , blood and bone / cartilage injuries from a native pmct examination . 
8 thick mip reconstruction in sagittal plane based on pmcta at the arterial phase : the injury of the wall of the left ventricle of the heart ( arrow ) with contrast medium extravasation to the pericardial sac fig . 
9 thick mip reconstruction in oblique coronal plane based on pmcta at the arterial phase : the injury canal due to stab wound of the chest at the right side of thorax , leading to the aortic arch , contrast medium leakage to the superior vena cava studies [ 45 ] and case reports [ 4648 ]  . 
there are also published research works referring to the direct contrast filling of injuries [ 49 , 50 ]  . 1 3 851 radiol med ( 2015 ) 120 : 846855 fig . 
10 vrt reconstruction based on native pmct of a victim of homicide due to blunt trauma to the head : a right anterior view , b left anterior view ; multiple fractures of the anterior part of the skull fig . 
11 vrt reconstruction based on native pmct of a victim of homicide with injuries due to an axe : a superior anterior view , b right ( slightly superior ) view ; multiple fractures of the facial part of the skull , injuries due to the blade of the axe fig . 
12 reconstructions based on native pmct of a victim of homicide , showing multiple fractures due to numerous blunt traumas to the skull : a thin mip reconstruction in coronal planemultiple fractures at the base of the skull on the left side , gas inside the skull , b vrt reconstruction left anterior viewmultiple fractures with small pieces of broken bones ( due to iterative trauma to the region ) 1 3 radiol med ( 2015 ) 120 : 846855 852 fig . 
13 vrt reconstruction based on native pmct of a victim of homicide due to blunt trauma to the head : a anterior ( slightly right superior ) view , b left anterior ( slightly superior ) view ; multiple fractures of the skull fig . 
13 : a at the arterial phase in axial plane , bd at the dynamic phase in ( b ) axial plane , ( c ) sagittal plane , ( d ) coronal plane : multiple fractures of the anterior ( and superior ) part of the skull , massive contrast medium extravasation at the facial part of the skull , no significant extravasations to the brain blunt trauma cases as mentioned above , the same opportunities and limitations are related to the victims of homicide due to blunt trauma . 
 [ 56 ] outlined the problem of a pitfall in the evaluation of post - mortem computed tomography : atlantoaxial rotatory subluxation . injury reconstruction with weapon identification as more general research [ 57 ] , as well as case report papers , was presented [ 58 ]  . 
it is important to mention that in some situations , even the data obtained from clinical ( ante - mortem ) ct acquisition can be highly valuable for forensic reconstructive opinion [ 59 , 60 ]  . other homicidal cases there are publications referring to the findings based on native pmct in strangulation cases , referring to hyoid bone and cartilages of the larynx [ 61 , 62 ]  . 
in cases of neonaticide , the results of evaluation of native pmct are reported as diagnostic for the proof of live birth [ 63 ] , and for decomposed bodiesrecognised as superior in the estimation of gestational age [ 64 ]  . the value of post - mortem imaging ( pmct ) is reported in cases of decomposed bodies [ 65 , 66 ] , but even in such cases it is possible to perform successful pmcta [ 67 ]  . even in cases of death related to poisoning ( which can also be potentially homicidal ) , the changes are reported [ 68 ]  . 
there is a publication referring to the estimation of time of death based on virtual forensic entomology ( microct examination ) [ 69 ]  . conclusions as shown above , post - mortem cross - sectional imaging ( in the form of pmct ) has an important role in forensic evaluation of homicidal cases . 
in some cases , information obtained from imaging methods can be crucial for the final forensic opinion ; these methods should be considered as a gold standard ( together with conventional autopsy procedures ) , at least in all cases where suspicion of homicide is present . it appears that placing imaging as competitive to conventional autopsy belongs to the past . 
understanding the fact that pmct examination prior to autopsy should simply be a routine order of investigation and can be increasingly widespread not only among the professionals , but also among financing authorities as well . 
technical success , defined as cor rect deployment without adjunctive manual compression , blood count and us evaluation of the arterial puncture site was done at 24 h and at 3 months . 
in the control group four ( 2.65 % ) major complications occurred : cfa occlusion managed with surgical bypass , cfa dissection solved by surgical bypass , two pseudoaneurysms solved with manual compression . 
several studies have validated their efficacy and analysed their cost - effectiveness [ 24 ]  . although infrequently , complications such as acute femoral arterial stenosis , arterial occlusion , infection , and distal embolisation , may set in during and after vcd insertion and make treatment more difficult . to reduce the incidence of such complications ultrasound ( us ) guidance can be very helpful because it allows not only to clearly visualise each step of vcd insertion but also to assess how correctly the vcd operates . 
we report the results of a retrospective comparative analysis of commercially available vcds deployed under us guidance or with the standard blind technique evaluating technical success and complication rate . materials and methods a retrospective analysis was performed between two groups of patients , one group having vcds inserted under us guidance ( study group ) vs . 
indications for using a vcd were the same in both groups : presence of a native cfa with a diameter greater than 5 mm and without severe calcified plaque on the anterior wall [ 5 , 6 ]  . 
the study was approved by the institutional review board and a written consent form was signed by all patients before the procedure . before vcd insertion digital subtraction angiography ( dsa ) was obtained in all cases in order to evaluate the artery entry site , not involving the femoral bifurcation and the caliber of the artery . 
vcds , in both groups , were inserted immediately after the interventional procedure with an act ( activated coagulation time ) ranging between 215 and 265 s ( mean value 220 s )  . 
also in this group cfa puncture was performed under us guidance . there were no statistical differences between the study group and the control group in terms of demographic data ( table 1 ) and vcds employed ( table 2 )  . after the procedures , patients were placed at bedrest for at least 6 h . 
blood count and us evaluation of the arterial site area were done 24 h and 3 months after the procedure . 1 3 radiol med ( 2015 ) 120 : 283288 fig . 
1 longitudinal b - mode ultrasound scan of the femoral access showing the phases of angioseal vip deployment : a insertion of the angioseal vip sheath ; b the rectangular 1 10 mm co - polymer footplate attached to a 18 - mg bovine biodegradable collagen plug is opened ( arrow ) ; c retraction of the footplate lining parallel to the inner wall of the artery ; d the footplate is withdrawn until it reaches the arterial wall achieving complete sealing of the percutaneous access ( arrow ) fig . 
2 longitudinal b - mode ultrasound scan immediately after the procedure a showing complete sealing of the percutaneous femoral access with no evidence of pseudoaneurysm or haematoma in the soft tissue ; the access site is clearly visible ( arrow )  . 
 then cfa patency and the complication rate at 24 h and at 3 months were equally evaluated and compared between the two groups . statistical analysis all analyses were carried using spss for windows ( spss , chicago , il , usa )  . 
significance was assumed at p < 0.05. results there were no statistically significant differences in terms of demographic characteristics between the study group and the control group ( table 1 )  . technical success , that is , correct vcd deployment without any need for adjunctive manual compression , was achieved in the study group in 98 % of patients . 
three cases required an adjunctive short ( 5 min ) manual compression to achieve complete sealing of the arterial puncture site . in the study group only one major complication ( 1.1 % ) occurred 24 h after the procedure : a starclose se - related pseudoaneurysm , 13 mm in diameter , which was easily solved with subsequent manual compression . 
minor complications ( haematoma and recurrent wound bleeding ) were reported in 4 % of patients . in the study group us guidance prevented wrong deployment of the vcd in four cases . 
in another case the footplate of the angioseal vip was entrapped within a parietal plaque but under us guidance the device was gently advanced , rotated and correctly replaced . in the control group technical success was achieved in 94 % of cases . 
the results are summarised in table 3 . discussion vascular closure devices have been introduced in percutaneous endovascular interventions to minimise those factors that may lead to the failure of manual compression . 
several studies have validated the role of vcds in reducing patient discomfort , number of complications , time to haemostasis and time to ambulation [ 1 , 713 ]  . clearly , the use of vcds cannot completely exclude technical failure or serious complications such as common femoral artery occlusion , laceration and stenosis , dissection , vascular bleeding , arterio - venous fistulae , and groin infection [ 1420 ]  . two key elements should be considered to reduce the incidence of complications and to improve technical success : patient selection and operators experience [ 5 , 6 , 21 ]  . 
one of the main problem of vcds is that their insertion , when performed blindly , gives no possibility of visualising and consequently checking the different steps of the deployment 1 3 radiol med ( 2015 ) 120 : 283288 phase . 
thus technical success is directly correlated with the operators skill , experience and sensitivity . according to the different types of closure devices or to the introducer size . a number of papers have addressed the use of fluoroscopic guidance to facilitate the correct insertion of vcd , although no improvements have been reported [ 1 , 22 , 23 ]  . 
a non - statistically significant trend was a minor incidence of pseudoaneurysms when using fluoroscopic guidance . ultrasound guidance seems to be very useful not only to perform a correct arterial puncture but also to insert correctly the vcd . 
other advantages are the possibility of evaluating arterial morphology , arterial calibre , and presence of calcified arterial plaques . some vcds ( angioseal vip and femoseal ) are based on the presence of a biodegradable collagen plug attached to a footplate producing a sandwich closure of the arteriotomy [ 21 ]  . 
the same complication may occur using the perclose proglide that requires system retraction after insertion into the arterial syste using ultrasound guidance the footplate and system retraction can be clearly visualised and followed , preventing complications . we know from our experience that all systems available on the market can be deployed under us guidance but visualisation may differ depending on the device selected . 
the reason seems to be correlated with the very fast movement of its two needles associated with their small size ( table 3 )  . it should , however , be stressed that the use of us is not time consuming , does not increase costs and does not compromise the procedure in terms of clinical results . 
moreover , it is not randomised conclusion our study highlights the advantages on the use of us guidance for vcd insertion in terms of higher technical success and lower rate of complications and device failure . conflict of interest all authors have nothing to disclose . ethical standard all procedures followed were in accordance with the ethical standards of the responsible committee on human experimentation ( institutional and national ) and with the helsinki declaration of 1975 , as revised in 2008 . 
for each target lesion in the breast , the adc value was compared with regard to major prognostic factors : histology , tumour grade , tumour size , lymph node status , and age . results a total of 289 patients with a mean age of 53.49 years were included in the study . 
gemelli 8 , 00168 rome , italy keywords diffusion apparent diffusion coefficient breast cancer aggressiveness prognostic factors introduction breast carcinoma is a heterogeneous disease with different molecular characteristics and variations in biological behaviour , clinical course , and prognosis [ 1 , 2 ]  . 
all the diagnostic imaging modalities that are currently used to evaluate malignant breast masses have factors that appear to correlate with the biological behaviour of the tumour ; indeed , recent studies have evaluated whether magnetic resonance imaging ( mri ) can be used as a prognostic method for breast cancer [ 36 ]  . in recent years , diffusion - weighted imaging ( dwi ) has been used to evaluate breast lesions ; most recently , it was integrated into standard mri breast examinations . 
however , dwi and the apparent diffusion coefficient ( adc ) have been used mainly to differentiate between benign and malignant lesions [ 3 , 7 , 8 ]  . 
only a few studies have investigated potential correlations between adc values and prognostic factors [ 916 ]  . diffusion - weighted imaging is an unenhanced mri sequence that measures the mobility of water molecules and provides different and potentially complementary information to dynamic mri . 
the water mobility in tissue mainly depends on the number and morphology of the cells , their relative arrangement , and the extracellular matrix in which the cells are embedded . 
the adc is the unit of measure used to quantify the water diffusion in tissue [ 1719 ]  . the traditional prognostic factors for breast cancer are histology , stage ( size and axillary node involvement ) , tumour grading , and molecular markers [ 2028 ]  . 
previous 1 3 radiol med ( 2015 ) 120 : 268276 studies found that there is a statistically significant correlation between tumour grade and adc value , probably because the histological grade of the tumour reflects the cellularity and the microenvironmental arrangement of the tissue , which may be associated with the mobility of water molecules [ 10 , 11 ]  . the purpose of this study was to examine the clinical utility of dwi in the characterisation of breast cancer and to determine if adc values can be used to predict breast cancer aggressiveness . our primary objective was to confirm the correlation between adc value and tumour grade based on a larger case series and by using a single region of interest ( roi ) for each adc measurement [ 29 ]  . 
our secondary objective was to explore possible correlations between the adc value and important prognostic factors such as age , tumour size and nodal status . materials and methods from january 2008 to june 2011 , all consecutive patients with definitively diagnosed breast cancer who under went breast mri and subsequent surgery in our hospital were enrolled in this study . 
in accordance with national research ethics service guidelines , ethical approval for the study was not required because the study was performed retrospectively on routinely acquired images [ 30 ]  . 
written informed consent was obtained from all patients before they underwent mri . inclusion criteria were written informed consent , complete bilateral coverage of both breasts , mri and dwi images of diagnostic quality suitable for assessment by radiologists , histologically proven breast cancer , and a definitive pathology report obtained at our hospital after surgical excision by the same dedicated pathologist . 
exclusion criteria were incomplete or nonoptimal mri study , pathological diagnosis obtained from an outside facility , and mri obtained during / after neoadjuvant chemotherapy ( to avoid any alteration in tumour tissue not due to histology or grading )  . 
all patients underwent the same mri protocol , which included a diffusion sequence acquired using b values of 0 and 1 , 000 s / mm2 . mri protocol mri was performed with a 1.5 t unit with 23 mt / m gradient strength ( signa excite ; ge medical systems , milwaukee , wi , usa ) with the patient in a prone position . 
sensitising diffusion gradients were applied sequentially in the x , y , and z directions , with b values of 0 and 1 , 000 s / mm2 . ( 3d ) three - dimensional gradient - echo fast - spoiled ( fspgr ) fat - saturated coronal sequence : flip angle ( fa ) , 15 ; tr , < 30 ms ; te , < 5 ms ; nex , 0.5 ; thickness , 23 mm ; inter512 matrix ; and fov , 3438 cthis sequence val , 0 ; 512 was acquired before and five times after intravenous administration of 0.1 mmol / kg gd - dtpa ( gadopentetate dimeglumine )  . 
contrast medium was injected with a 10 - s timing delay into the antecubital vein with an 1820 g needle at a flow rate of 2 ml / s followed by a flush of 20 ml of saline solution . three - dimensional fspgr post - contrast sequence : tr , < 30 ms ; te , < 5 ms ; fa , 15 ; 512 512 matrix ; thickness , 23 mm ; interval , 0 ; fov , 2226 cm ; and nex , 2 . sagittal three - dimensional fspgr axial post - contrast sequence : 512 matrix ; thicktr , < 30 ms ; te , < 5 ms ; fa , 30 ; 512 ness , 23 mm ; interval , 0 ; fov , 3438 cm ; and nex , 2 . the acquisition time for the complete mri protocol was 1820 min . mri analysis we used dynamic - enhanced mri as a reference for detecting breast lesions . 
in cases of multifocal or multicentric cancer , only the largest lesion was considered for data analysis . the dynamic and diffusion images were evaluated at a dedicated workstation ( advantage workstation , windows 4.1 ; ge healthcare ) in consensus by two radiologists with many years of experience ( p.b. , 20 years and m.c. , 15 years ) in breast imaging , who were unaware of the pathological results . 
dwi was considered able to detect the target lesion if it appeared hyperintense . the adc distribution was shown in an axial adc colour map , in which red represents high adc values and blue 1 3 270 radiol med ( 2015 ) 120 : 268276 represents low adc values . 
the formula was intensity obtained at b directly applied by the programme . a single roi was manually drawn around the borders 1 , 000 s / mm2 diffusionof the target lesion on the b weighted image in which the maximum axial diameter was presented . 
the placement of the roi was also confirmed by consensus between the two radiologists . pathological examination each lesion was examined by the same pathologist , who assessed histology and tumour grading . 
for histological examinations , tissues were fixed in 10 % buffered formalin and embedded in paraff sections were stained with haematoxylineosin and , if necessary or indicated , with ck 14 , p63 , calponin , a - sma , and e - cadherin antibodies [ 33 ]  . grading was assessed by the nottingham modification of the bloomrichardson grading system , which evaluates three features of cancer : the percentage of the cancer composed of tubular structures , nuclear pleomorphism , and mitotic count . 
a tumour with a final sum of 35 points was considered a grade 1 tumour ( well differentiated ) , a sum of 67 points was considered a grade 2 tumour ( moderately differentiated ) , and a sum of 89 points was a grade 3 tumour ( poorly differentiated ) [ 34 ]  . data and statistical analysis for each malignant lesion , the relationship between adc and age , histology , tumour grade , size , and lymph node status was analysed . 
in cases of multifocal / multicentric cancer , only the largest lesion was considered . data are presented as mean standard deviation ( continuous variables ) or as percentages ( categorical variables )  . 
for the execution of correlation analyses , either pearsons ( two continuous variables ) or spearmans ( one continuous and one categorical variable ) correlation coefficients were employed . to assess the ability of the adc value to predict breast cancer aggressiveness , two groups of disease were considered : the less - aggressive group , which included ductal in situ carcinomas and grade 1 invasive carcinomas and the more - aggressive group , which included grade 2 and grade 3 invasive carcinomas . a multiple logistic regression model was built to identify the factors independently associated with the moreaggressive status of breast lesions . 
the capability of the adc value to correctly discriminate between a more - aggressive lesion and a less - aggressive lesion was described by means of diagnostic performance analysis [ calculation of a receiver operating characteristic ( roc ) curve and calculation of the area under the roc curve ]  . 
the sensitivity , specificity , and accuracy of two different cut - off values of adc in the detection of a more - aggressive lesion were calculated . results out of a total of 872 patients with proven breast cancer who underwent contrast - enhanced mri and dwi in our department during the study period , 289 women aged 27 88 years ( mean 53.49 years and sd 12.32 years ) were ultimately included in the study . 
the mri study was not optimal in 16 cases , while 28 patients were treated outside and 539 patients had been treated with neoadjuvant treatment . histology revealed 220 invasive ductal carcinomas ( idc ) , 33 invasive lobular carcinomas ( ilc ) , 26 ductal carcinomas in situ ( dcis ) , and ten other invasive forms of cancer ( four tubular carcinomas , one medullary carcinoma , one colloid carcinoma , and four undifferentiated carcinomas )  . 
the mean diameter is reported in mthe mean adc is reported in node negatives , n a 4 tubular carcinomas , 1 medullary carcinoma , 1 colloid carcinoma , 4 undifferentiated carcinomas node positives , idc invasive ductal carcinoma , ilc invasive lobular carcinoma , dcis ductal carcinoma in situ 10 a careful analysis of 19 cases of cancer with adc val3 mm2 / s revealed that ten cases ues higher than 1.4 were very low - grade tumours ( grade 1 ) and three cases were grade 2 tumours without lymph node involvement . 
 of the six high - grade ( grade 3 ) tumours , three were in situ form with low - aggressive potential and two had an adc 3 and value only slightly higher than the cut - off ( 1.43 3 mm2 / s , respectively )  . 
the adc value varies significantly according to the biological features of breast cancer , although the relationship between restricted diffusion and cancer aggressiveness is not well understood [ 916 ]  . several studies have shown that lower adc values in breast malignancies are primarily attributed to higher cell density and high histological grade with high mitotic rates and nuclear / cytoplasmic ratios [ 10 , 11 ]  . 
4 receiver operating characteristic ( roc ) curve : diagnostic performance of adc for the prediction of lesion aggressiveness is a complex system that includes tumour cells , stromal cells ( such as adipocytes , fibroblasts , endothelial cells , and infiltrating immune cells ) , and extracellular matrix . 
 in particular , tumour stroma acquires a pattern that promotes cell proliferation , cell adhesion and invasion , and extracellular matrix remodelling [ 13 , 14 , 35 , 36 ]  . 
it is likely that all the characteristics assumed by the tumour microenvironment have a role in restricting the diffusion of water molecules . few studies have analysed the relationship between prognostic factors and adc values , and their results have varied [ 916 ]  . 
according to the findings of other studies [ 8 , radiol med ( 2015 ) 120 : 268276 10 , 11 , 15 ] , the mean adc of invasive carcinomas was significantly lower than that of in situ lesions ; however , no differences in adc values were observed between ductal and lobular invasive cancer . according to our previous preliminary study [ 11 ] and to those of nakajo et al . 
in the present analysis of the relationship between adc values and prognostic factors , we detected a significant association between adc values and lymph node status , as reported nakajo et al . 
this concept is strengthened by the findings of the roc analysis , which identified 3 mm2 / s as the appropriate cut - off for sufficient 0.9 detection of more - aggressive lesions . 
while the diagnostic performance of the adc value must be strengthened by further refinements of the technique and by technological advancements , these observations are a step towards the routine assessment of histopathology through diagnostic imaging . 10 we did not observe a significant correlation between adc value and tumour size or age . 
in the new molecular era , several studies [ 1 , 2 ] have revealed that breast cancer is a heterogeneous disease in which the biological aggressiveness , radiological appearance , and outcome varies considerably among individuals . 
age was historically considered a risk factor for breast cancer , but there is an evidence that more - aggressive tumours are often associated with younger age [ 38 , 39 ]  . 10 finally , in agreement with martincich et al . 
in our study , a cut - off value 3 mm2 / s was sufficient to identify lesions with of 0.9 a higher biologically aggressive profile that is generally associated with invasion , high grade , and the presence of lymph node involvement . 
finally , we only analysed traditional prognostic factors without investigating the molecular profiles of individual breast cancers . 1 3 radiol med ( 2015 ) 120 : 268276 conclusions the biological mechanisms of breast cancer and the major pathways involved in tumour progression and metastasis remain incompletely understood . 
the aim of our study was to evaluate the role of virtopsy performed through computed tomography ( ct ) in the forensic diagnosis of drowning . materials and methods we retrospectively examined the ct data of four cadavers recovered from sea water and suspected to have died by drowning . 
each patient underwent a full - body post - mortem ct scan , and then a traditional autopsy . results all the cadavers showed uid in the airways and patchy ground - glass opacities in the lung . 
only one patient had no uid in the digestive tract ; this patient had a left parietal bone fracture with a large gap and other multiple bone fractures ( nose , clavicle , rst rib and patella )  . 
procaccianti department of biotechnology and legal medicine , university of palermo , via del vespro , 129 , 90127 palermo , pa , italy conclusion to date , there are no autopsy ndings pathognomonic of drowning . 
this study proves that virtopsy is a useful tool in the diagnosis of drowning in that it allows us to understand if the victim was alive or dead when he entered the water and if the cause of death was drowning . keywords autopsy ( cid : 2 ) virtopsy ( cid : 2 ) drowning , computed tomography ( cid : 2 ) forensic medicine ( cid : 2 ) post - mortem changes introduction drowning is the third leading cause of unintentional injury death worldwide , accounting for 7 % of all injury related deaths [ 1 ]  . 
the forensic diagnosis of drowning is based on macroscopic and microscopic ndings but the pathological proof is often difcult or even impossible to obtain [ 2 , 3 ]  . 
furthermore , the macroscopic and microscopic ndings in the fresh drowned corpse are non - specic and will disappear with putrefaction [ 4 ]  . at present , in the autopsy diagnosis of drowning , the demonstration of diatoms in the submerging uid and in the body of the victim is the gold standard [ 2 ] ; however , there are no reliable tests permitting an unequivocal diagnosis of drowning . 
the main limit in the diagnosis of drowning is that even if a body is recovered from water , it may not have drowned and the proof that death was due to drowning may constitute one of the most difcult problems in forensic medicine . 
computed tomography ( ct ) virtual autopsy ( virtopsy ) radiol med ( 2015 ) 120 : 304308 represents an effective imaging modality in the diagnosis of drowning , even if drowning can not be diagnosed solely through ct [ 510 ]  . 
in drowning victims , inhaled and aspirated uid enters the paranasal sinuses as it passes through the nasal cavity ; hence , as proved by recent reports , the ct nding of uid accumulation in the maxillary and sphenoidal sinuses is supportive of the diagnosis of drowning [ 1012 ]  . the aim of our study was to verify the role of multidetector ct in the forensic diagnosis of drowning and as a tool to differentiate a death by drowning from a nondrowning death . materials and methods the ct data of four cadavers ( two male , two female ; mean age , 34 years ) recovered from water and suspected to have died by drowning were retrospectively examined . two of the cadavers were recovered after the air crash of a tuninter atr 72 which ditched off the coast of palermo on the 6th of august 2005 . 
the other two bodies were found in 2012 close to palermo in an area of the sea below a cliff - top . each patient underwent a full - body post - mortem ct scan without contrast medium administration . 
the two cadavers recovered in 2005 ( a 39 - year - old man and a 52 - year - old woman ) were studied with a 40 - channel multidetector ct scanner ( brilliance 40 , philips medical systems , cleveland , oh , usa ) using the following parameters : increase in layer 1.5 mm , 120 kv , 280 mas , lter b . 
the two cadavers found in 2012 ( a 25 - year - old man and a 21 - year - old woman ) were studied with a 128 - channel multidetector ct scanner ( somatom denition as ? siemens 128 , siemens medical solutions , erlangen , germany ) using the following parameters : slice thickness 0.6 mm , increase in layer 0.3 mm , 120 kv , 225 mas , lter b - 20 . slice thickness 3 mm , acquired images were transferred to a dedicated postprocessing workstation for the visualisation with volume rendering technique as 3d and multiplanar reconstruction images . all ct scans were evaluated by the same radiologist and the following ndings were recorded : presence of uid in the paranasal sinuses ; presence of uid in the mouth and in the upper airways ; presence , extent and distribution of ground - glass opacities in the lung ; presence pneumothorax ; effusion pleural extent presence of uid in the oesophagus , stomach and bowel ; presence of air in the cardiac chambers , in the arteries and veins ; presence of any anomaly in the head , neck , mediastinum , abdominal and pelvic viscera and skeleton . after the ct scan , each cadaver underwent conventional autopsy , and histological , chemical and toxicological examinations on the collected uids and tissues were performed . 
in the second patient who precipitated from the rocky cliff instead , the absence of uid in the digestive tract and the presence of a skull fracture with signicant brain lesion suggest that the primary cause of death had occurred before immersion in sea water . discussion forensic thanatology is a part of forensic medicine devoted to the study of the phenomena of death . 
moreover , this cadaver had other multiple bone fractures ( nose , clavicle , rst rib , humerus , femur and patella ) : in particular , he showed a displaced multi - fragmented fracture of the nasal bones and septum with severe soft - tissue swelling of the left orbital area and chin area and avulsion of teeth 31 and 32 and blood and air in the adjacent subcutaneous tissue . the forensic reconstruction revealed that one of the two dead bodies fallen from a 20 - m rocky cliff , despite having suffered a major head injury that led to the fracture of the zygomatic process and of the greater wing of sphenoid bone without signicant brain lesion , did not die because of the head injury ; these fractures indeed did not cause immediate death as demonstrated by the fact that sea water fig . 
4 axial mdct image shows uid level in the stomach ( arrow ) radiol med ( 2015 ) 120 : 304308 diagnosis has several limits primarily related to the inability to certainly state whether the cause of death of the recovered corpse occurred before or after the dive . internally , the autopsy diagnosis of drowning is based on macroscopic and microscopic ndings [ 2 , 3 ]  . 
externally , the presence of foam at the mouth or nostrils , or both , is important . lungs are waterlogged , over - distended often to a degree which causes them to overlap the pericardium , and , sometimes , increase in weight . 
regarding the microscopic ndings , classical histological examination through haematoxylin and eosin staining shows intra - alveolar oedema and dilatation of the alveolar spaces with secondary compression of the septal capillaries . 
however , the macroscopic and microscopic ndings in the fresh drowned corpse are non - specic and will disappear with putrefaction . at present , in the autopsy diagnosis of drowning , the demonstration of plankton and , more especially , diatoms in the submerging uid and in the body of the victim is the gold standard [ 2 ]  . 
 [ 3 ] suggested a dna coprecipitation method for the detection of diatoms in heart blood as a simple and safe tool for the diagnosis of drowning . to overcome the limits of the conventional autopsy in the diagnosis of drowning , post - mortem radiological imaging techniques are taking a prominent role . 
the progressive development of medical technologies led to revolutionise the autopsy process , until the birth of the virtopsy project in the institutes of forensic medicine , radiology and neuroradiology at the university of bern , in switzerland [ 5 ]  . the use of virtopsy contributes both to the identication of the corpse and to hypothesise the cause of death . 
currently , ct is the most widely used diagnostic tool virtopsy . post - mortem ct proved to be useful in imaging victims who have suffered a water - related death . 
 [ 11 ] , ct images from victims who were conrmed to have died by drowning showed uid in the paranasal sinuses and mastoid air cells , and ground - glass opacity in the septal lines . 
 [ 11 ] , postmortem ct did show conclusive radiological signs of drowning as primary cause of death . in our retrospective evaluation of cadavers recovered from sea water , we noticed that characteristically all the cadavers had uid in the airways and patchy ground - glass opacities in the lung . 
among the four cadavers , only one had no uid in the digestive tract ; the absence of water in the stomach suggests either rapid death by drowning , or death prior to submersion . 
this patient had a left parietal bone fracture with a large gap ; moreover , he had multiple bone fractures ( nose , clavicle , rst rib and patella )  . 
on the other hand , one of the three patients with uid in the digestive tract did not show uid in the paranasal sinuses ; this latter patient showed cerebral oedema with subarachnoid and intraventricular haemorrhage , multiple bone fractures ( orbital oor , ribs , sacrum , acetabular edge ) and air in the heart , in the aorta and in bowel loops . the most important limitation of the present analysis was the limited number of cadavers evaluated . 
moreover , we did not use contrast mediufurther observations and analyses based on larger cohorts of drowned cadavers are needed . conclusions as widely known in the literature , there are no autopsy ndings pathognomonic of drowning . 
this study shows that post - mortem ct performed prior to autopsy may help to understand if the victim was alive or dead when he entered the water and if the cause of death was drowning . 
the sign0al - to - noise ratio of the liver ( snrliver ) and the contrast - to - noise ratio of the portal vein to muscle ( cnrpv to m ) were measured . 
for qualitative analysis , image noise , visibility of small intrahepatic vascular structures , beam - hardening artefact , lesion conspicuity , and overall image quality were graded by two radiologists . results quantitative analysis demonstrated that image noise was significantly reduced along with the increasing level of idose and that the values of snrliver and j . 
choi department of radiology , research institute of radiation medicine , seoul national university college of medicine and hospital , 101 daehak - ro , jongno - gu , seoul 110 - 744 , south korea e - mail : jmlshy2000@gmail.com cnrpv to m were significantly better with idose than those of fbp images . 
qualitative assessment also showed significantly better results with idose compared with fbp ( p < 0.05 ) and the parameters for subjective image quality were highest with idose level 4 . conclusions the hybrid ir technique is able to reduce image noise and to provide better image quality than fbp , and an intermediate strength of idose ( level 4 ) provided the highest quality images . keywords hybrid iterative reconstruction ct image quality reconstruction algorithm introduction the explosive growth of the use of computed tomography ( ct ) can be attributed to its wide availability , speed , and diagnostic benefits [ 1 , 2 ]  . 
while this increase is associated with significant improvements in diagnostic performance , it has also caused an increase in radiation exposure and the risk of radiation - induced cancer [ 3 ]  . 
not only for patients who undergo multiple ct studies during the course of their follow - up , but also for paediatric patients who are sensitive to radiation hazards as well as the general population who undergo ct scans for routine checkups , radiation dose reduction is an important issue [ 4 ]  . 
owing to the radiation dose concerns associated with ct , several approaches , including automated tube current modulation , new image acquisition , and new reconstruction algorithms , have been used to reduce the radiation dose [ 5 , 6 ]  . 
 amongst these approaches , several iterative reconstruction ( ir ) algorithms of major vendors are widely used to achieve radiation dose reduction without image degradation [ 6 ]  . 1 3 260 radiol med ( 2015 ) 120 : 259267 results of recent studies [ 57 ] have shown that new ir algorithms produce up to 66 % radiation exposure reduction without significant image degradation , compared with standard dose ct using filtered back projection ( fbp )  . 
 however , an image - based ir method such as iterative reconstruction in image space ( iris , siemens healthcare ) , resulting in profound changes in image appearance with higher levels of iterative weighing [ 9 ] and excessive image noise reduction , often results in plastic , blotchy or pixilated images which could adversely affect overall image quality or diagnostic accuracy [ 8 ]  . 
more recently , following prior versions of the image - based ir technique , such as iris , several hybrid ir algorithms working in both image space and the raw data space , such as adaptive statistical iterative reconstruction ( asir , ge healthcare ) , idose ( philips healthcare ) , and sinogram - affirmed , iterative reconstruction ( safire from siemens healthcare ) were launched to solve image - quality - related problems and are believed to be more effective than image - based ir techniques [ 8 , 10 ]  . therefore , the purpose of our study was to determine , through an evaluation of the objective and subjective image quality , whether the hybrid ir algorithm ( idose ) can improve the image quality of liver ct by reducing image noise , and to assess which level of ir strength is acceptable for clinical use . materials and methods patient population we obtained approval for this retrospective study from the institutional review board of our institution , and informed consent was waived . 
from december 2011 to february 2012 , 75 consecutive patients ( m : f 41 : 34 , mean age , 59.5 years ; age range 3583 years ) with a known or suspected intra - abdominal malignancy underwent two - phase liver ct using a 64 - channel , multidetector ct ( mdct ) scanner ( philips ingenuity , philips healthcare , best , the netherlands )  . 
in addition , in the other six patients , the hepatic lesions noted on the liver ct were clinically diagnosed as metastases either based on their characteristic magnetic resonance ( mr ) findings for metastases , including irregular or ill - defined borders which displayed high signal intensity on high b value diffusion - weighted imaging ( dwi ) and the lower apparent diffusion coefficient ( adc ) value of the lesion compared with that of the adjacent liver parenchyma or interval growth in the longest axial diameter of at least 20 % on the next follow - up ct . 
the cysts or haemangiomas in 14 patients were diagnosed based on characteristic imaging features on liver ct or mr imaging and absence of interval growth on follow - up ct scan . ct technique for all patients , two - phase liver ct consisting of precontrast and portal phase images was performed . 
the ct parameters were as follows : rotation time , 0.5 s ; beam collima0.6 mm ; reconstruction section thickness , 3 mm ; tion , 64 beam pitch , 0.891 ; field of view , 32 ~ 38 cm ; and matrix size , 512 512 pixels . 
the tube potential was fixed to 120 kv and the automatic tube current modulation technique ( z - axis dose modulation ; philips healthcare ) was used with a reference current of 180 mas . 
3 - mm section thickness and a 2 - mm interval , during the portal phase and using a standard fbp algorithm with a standard , soft - tissue kernel and an idose algorithm with a level from 1 to 6 . 
fbp , idose level 1 ( idose - 1 ) through idose level 6 ( idose - 6 ) were generated from the same raw data for each patient and were then sent to and archived in our picture archiving and communications system ( maroview 5.4 , infinitt , seoul , korea )  . 1 3 radiol med ( 2015 ) 120 : 259267 idose is provided with an additional parameter , i.e. 
 23 % , 4 11 % , 2 45 % , and 7 the idose level ( scale 17 ) , which is used to define the strength of the ir technique for reducing image quantum mottle noise . 
for example , if the original scan at 200 mas is associated with the contrast - to - noise ratio of 200 mas ( cnr ) , then using an idose reconstruction with a level of 4 for a scan performed with 100 mas would compensate for the increase in noise in the same homogeneous region of interest ( roi )  . 
 dose reduction , image quality improvement or a combination of both . qualitative analysis two radiologists independently assessed the image noise , visibility of small intrahepatic vascular structures , beamhardening artefact , lesion conspicuity , and the overall image quality as determined on portal phase ct images . 
 the reading was performed at a workstation ( advantage windows 6200 , hewlett - packard , ca , usa ) with a spatial resolution of 1600 1200 ( totoku , japan ) using our picture archiving and communications system ( maroview 5.4 , infinitt , seoul , korea )  . 
if there were multiple lesions , the readers were asked to grade the smallest lesion with a diameter of at least 1 cm . suboptimal visibility , 3 above average visibility , and 5 subjective image noise level was assessed using a fiveabove averunacceptable image noise , 2 point scale ( 1 average image noise , 4 less than average age noise , 3 noise , and 5 minimal image noise ) , and visibility of small structures such as small portal vein branch vessels , was unacceptable visualigraded using a five - point scale ( 1 acceptable visibility , sation , 2 excellent visualisation )  . 
subjective visual lesion conspicuity was assessed using a five - point scale ( 1 probably an artefact mimicking a mimicking a lesion , 2 well - seen lesion with poorly lesion , 3 visualised margins , and 5 well - seen lesion with well - visualised margins )  . 
in addition , but not affecting interpretation , 3 present and affecting image interpretation , 2 margins definitely an artefact subtle lesion , 4 overall image quality including artificial sensation was unacceptable diagnosassessed using a five - point scale ( 1 tic image quality with severe blotchy , or pixilated appearance impairing lesion evaluation , 2 sub - diagnostic image quality with obvious blotchy , or pixilated artefacts impairing average diagnostic image quality with lesion evaluation , 3 better image quality subtle blotchy or pixilated artefacts , 4 than average with subtle pixilated appearance , and 5 better image quality than average with better edge delineation and no pixilated appearance )  . 
the image quality attributes assessed in our study have been described in the european guidelines on quality criteria for computerized tomography document [ 12 ] and have been used in numerous previous studies published in the radiology literature [ 13 ]  . quantitative analysis quantitative measurements were performed at a commercially available workstation ( advantage windows 4.2 ; ge healthcare ) by experienced radiology research personnel who was blinded to the image review results . 
we measured the image noise and attenuation values of the liver , portal vein , and paraspinal muscle , as also described in previous reports [ 14 , 15 ]  . 
objective image noise was measured for 525 image sets ( seven image sets each from 75 patients ) as the standard deviation of the pixel values from a circular or ovoid roi ( 1050 mm2 ) placed in a homogenous region of subcutaneous fat of the anterior abdominal wall . 
to ensure consistency , all measurements were performed three times at the level of the main portal vein , after which the mean values were calculated . mean ct attenuation values ( in hounsfield units ) of the portal vein , liver parenchyma , and paraspinal muscle were obtained on the portal phase of ct scanning . 
the liver attenuation was recorded as the mean of the measurements of four rois ( 50100 mm2 ) in the medial and lateral segments of the left hepatic lobe and in the anterior and posterior segments of the right hepatic lobe [ 14 ]  . 
the attenuation of the paraspinal muscles was recorded as the mean attenuation of two rois ( 1050 mm2 ) , while taking care to avoid macroscopic fat infiltration in the right and left paraspinal muscle at the level of the right portal vefor all measurements , the size , shape , and position of the rois were kept constant by applying the copy - and - paste function at the workstation . the cnr values relative to muscle ( m ) for the portal vein ( pv ) were calculated using the following equation 1 3 262 radiol med ( 2015 ) 120 : 259267 ( roipv [ 16 ] : cnrpv to m roim ) / sdn , where roipv is the mean attenuation of the portal vein , roim is the mean attenuation of the paraspinal muscle , and sdn is the mean image noise . 
the all statistical analyses were performed using commercially available software ( medcalc , version 12.3.0.0 , 2012 ; medcalc , mariakerke , belgium ) and data are graphically presented as mean kruskalwallis test was used to determine the results of the qualitative analysis data . 
 the scale for the k coefficients for interobserver agreement was as follows : < 0.20 , poor ; 0.210.40 , fair ; 0.410.60 , moderate ; 0.610.80 , substantial ; and 0.811.00 , almost perfect [ 17 ]  . 
interobserver agreement for the qualitative analysis was moderate to almost perfect ( table 1 )  . quantitative analysis an increased idose level was associated with a linear noise reduction , no change in ct attenuation , and a linear improvement in snr and cnr ( table 2 )  . 
compared with fbp , the mean noise reduction was 13 , 18 , 23 , 28 , 34 , and 41 % for reconstructions with idose levels 1 through 6 , respectively . 
compared with fbp , there was a mean increase in liver snr of 12 , 17 , 23 , 29 , 36 , and 43 % for reconstructions using idose levels 1 through 6 , respectively . 
the snr of the portal vein , compared with fbp , showed a mean increase of 12 , 17 , 23 , 28 , 35 , and 43 % for reconstructions using idose levels 1 through 6 . 
 the cnr of the portal vein also showed a mean increase of 11 , 16 , 22 , 28 , 35 , and 42 % for reconstructions using idose levels 1 through 6 when compared with fbp . 
our study results were in good agreement with those of previous studies regarding various ir techniques such as asir ( ge healthcare ) [ 6 , 14 , 18 ] , or with an iris ( siemens healthcare ) [ 1921 ] or adaptive iterative dose reduction ( aidr , toshiba healthcare ) [ 22 ] , both of which demonstrated that ir has the potential to provide improved image quality at lower radiation doses than fbp . 
furthermore , in the qualitative analysis , intermediate strength ir ( level 4 ) was more preferred than fbp or higher strength ir ( level 5 or 6 ) , despite the fact that quantitative analysis showed better results of image noise , snrliver , and cnrpv to the m as the strength of the ir increased . 
based on our study results on noise reduction , we believe that the use of idose with intermediate ir strength can be used to reduce the radiation dose of routinely used abdominal ct while maintaining image quality . in our study , when we evaluated the appropriate level of ir strength , i.e. 
the idose level , idose effectively reduce image noise , while the images did not have an artificial , blotchy , pixilated or plastic appearance , up to the intermediate strength of ir . 
in addition , although the ct vendor , philips , claimed that idose is able to preserve the image texture and its natural appearance by minimising the shift of noise power spectrum ( nps ) , even at the maximum noise removal to reproduce the noise texture of classical fbp images that radiologists expect to achieve [ 23 ]  . 
idose uses a combination of processing in the projection and image domains , thus providing clinical advantages such as the ability to effectively remove photon starvation - related artefacts , e.g. 
with regard to subjective image noise ( a ) and beam - hardening artefact ( c ) , the higher idose level used , the lower image noise and beam - hardening artefacts noted ( higher score )  . 
however , visibility of small intrahepatic vascular structures ( b ) , lesion conspicuity ( d ) , and overall image quality ( e ) are highest with idose level 4 modulation transfer function ( mtf ) and concluded that there is no decline in spatial resolution while noise level and radiation dose decreased [ 10 , 11 ]  . 
consequently , the noise texture of images reconstructed with idose and fbp did not differ , although the noise itself was significantly reduced by 1 3 264 radiol med ( 2015 ) 120 : 259267 in a fig . 
images obtained during the portal phase with a fbp , b idose level 2 , c idose level 4 , d idose level 6 shows gradually reduced images image noise with increasing idose level . 
however , both reviewers of our study preferred intermediate strength reconstruction ( level 4 ) because some of the images reconstructed with idose - 5 or idose - 6 appeared artificial . 
for example , 50 % ( 1 / 2 ) less radiation exposure was achieved by increasing the noise index ( ni ) by a factor of 2 [ 25 ]  . 
according to a previous study , it has been reported that when using idose in the clinical routine , the clinician has the opportunity to reduce the radiation dose up to 80 % while preserving the image quality or maintain the radiation dose to improve the spatial resolution up to 68 % [ 11 ]  . 
in other situations , where image quality , spatial resolution , is of a higher priority than dose reduction , such as in the assessment of coronary stent patency , idose allows significantly improved spatial resolution . 
however , based on our study results on noise reduction , we believe that the use of idose at intermediate level of dose reduction could reduce the radiation dose up to 40 % of routinely used abdominal ct dose while maintaining image quality . 
currently , at our hospital , based on these study results , we were able to reduce the radiation dose up to 30 % for liver ct scanning with idose level 4 reconstruction compared with the conventional scanning method using fbp . currently , several types of ir techniques are being developed by many vendors and are being used at many medical centres as a tool to reduce the radiation dose or to improve image quality . 
in our study , we used different levels of iterative strengths of the hybrid ir algoriththe idose algorithm can be classified as a hybrid ir technique , and , theoretically , it can be more successful than imagebased iterative techniques , such as iris , as it uses projection - based data as well as image - based data . 
recent studies reporting on safire and aidr 3d , which are also classified as hybrid ir technique since they iterate in both the raw data space and the image space , have shown that radiation dose reduction up to 5052 % with mean objective image noise reduction of 31 % without altering diagnostic information is possible [ 7 , 26 ]  . 
safire is provided with five reconstruction strength levels and the noise modelling is supported by raw data : in each iteration , the noise content is estimated in each voxel by analysing the contribution of raw data to this voxel , after which noise is removed . 
the vendor declares that a dose reduction of 75 % or more is possible based on the assumption that noise in ct images is inversely proportional to the square root of the applied dose [ 7 ]  . 
unlike asir , veo is a fully iterative method working in the raw data domain which models not only the data statistics but also the geometry of the scanner itself by considering the voxel volumes of the scanned object , the focal spot size , the active area size of the detector , etc . 
however , although veo seems to mark a major breakthrough in ct reconstruction , it requires a high computational power leading to a reconstruction time as long as 30 min ~1 h , and is therefore not yet suitable for all clinical situations [ 22 ]  . our study has some limitations . 
first , our study design was retrospective and nonrandomised and was comprised 1 3 266 radiol med ( 2015 ) 120 : 259267 of a small number of patients seen at a single medical centre . 
second , we did not investigate the performance of idose in terms of image quality improvement depending on the patients body habitus and using the body mass index ( bmi )  . 
third , as lesion conspicuity was assessed using hepatic metastases seen on the portal phase , we did not evaluate arterialphase image quality on the hybrid ir algoriththerefore , the lesion conspicuity of hypervascular tumours , such as hepatocellular carcinomas , should be evaluated in future studies . 
lesions were categorised as benign ( n 36 ) and infectious ( n 5 ) in origthe shear wave velocities ( swvs ) of the tumours and the intact parenchyma were determined by arfi quantification , and the differences in the swvs were compared among groups . 
yavuz ( * ) department of radiology , yuzuncu yil university , school of medical science , geve kampus , ercis yolu , 65100 van , turkey e - mail : dralpyavuz@hotmail.com however , the swv values of the infectious lesions and leiomyoma corresponded well with the malignant lesions . 
 a receiver operating characteristic ( roc ) analysis demonstrated a cut - off value of 2.34 m / s between benign and malignant lesions , while sensitivity and specificity were determined to be 88 and 54 % , respectively . conclusion arfi elastography with arfi quantification may be useful for differentiating benign renal lesions from malignant renal tumours . keywords elastography ultrasound renal tumors introduction ultrasound ( us ) is often the first step in evaluating renal masses , as it is commonly used to detect and characterise the computed tomography ( ct ) or magnetic resonance ( mr ) imaging are generally needed for further characterisation if a renal mass appears to have solid parts . 
contrast - enhanced ct and mr imaging are the modalities of choice for differentiating benign and malignant lesions , as these techniques have high sensitivity and specificity [ 26 ]  . 
however , the need to maintain an intravenous line , the long amount of time between the technique and a diagnosis , the potential for allergic reactions to the contrast agents , and the higher costs of ct and mr can limit their use in daily clinical practice . 
one study reported that 1 3 radiol med ( 2015 ) 120 : 296303 6.9 % of patients who underwent surgery for suspected renal cell carcinoma ( rcc ) had pathologically confirmed angiomyolipoma after partial nephrectomy , despite a thorough expert review of preoperative imaging studies [ 7 ]  . 
acoustic radiation force impulse ( arfi ) can be an additional technique to conventional grey - scale us in the differentiation of benign and malignant lesions since the diagnostic accuracy of grey - scale us is low especially in tumours smaller than 3 cthe purpose of this preliminary study was therefore to prospectively evaluate the diagnostic performance of arfi imaging for differentiating benign lesions from the malignant renal tumours . materials and methods arfi imaging was routinely performed along with conventional us of the kidney in 60 patients with focal renal lesions who had been randomly sent to the us examination room ( equipped with an acuson s2000tm scanner , siemens medical solutions , mountain view , ca , usa ) between april 2013 and december 2013 . 
lesions with sufficient solid components that swv quantification could be revealed by arfi were evaluated the solid parts cross - sectional area of the lesions should at least fill the region of interest ( roi ) area of the arfi which has the shape of a rectangle with the sizes of the size of each mass was measured with b - mode us . 
all of the aml were diagnosed based on a combination of typical findings using either contrast - enhanced ct or mr imaging and no increase in tumour size for at least 12 months . 
in the remaining 14 cases , the angiomyolipomas were diagnosed by the presence of bulk fat on ct or mr imaging ( or both ) performed before or after the sonography [ 10 , 11 ]  . the diagnosis of metastatic renal tumours was determined by clinical diagnosis in seven patients . 
the origins of these seven metastatic tumours were as follows : one from bladder adenocarcinoma , one from renal cell carcinoma ( rcc ) , three from lung non - small cell carcinoma , and two from lymphoma . arfi elastography was performed by one experienced radiologist with 10 years of clinical experience in abdominal us imaging and 1.5 years of experience in elastography using an acuson s2000tm scanner with a curvilinear transducer array operating at 4 mhz ( 4c1 , siemens medical solutions , mountain view , ca , usa )  . 
then , the shear wave velocity ( swv , expressed in metres per second ) was measured in a central window of 5 mm axial by 4 mm width within the roi that was graphically displayed at 1 cm axial by 6 mm width . 
to reduce cardiacand respiration - related tissue motion in the roi , all quantification was performed with the patients in the right and left decubitus positions 1 3 radiol med ( 2015 ) 120 : 296303 298 fig . 
1 shear wave velocity ( swv ) measurements of the renal tumours were revealed by placing the region of interest ( roi ) in the ventral margin of the tumour . 
b swv measurement of a histopathologically confirmed chromophobe cell renal carcinoma in the left kidney of a 32 - year - old female patient during a brief breath hold ( neither full inspiration nor full expiration )  . 
after identifying the target lesion on a b - mode us image , arfi imaging was performed using the same probe . at least five swv values were obtained at different areas within the renal tumours . 
in addition , at least five swv values were obtained for the intact renal parenchyma at different areas of the renal cortex around the tumours and away from the renal vessels and medullary sinus . 
the difference in the swv between each tumour and the adjacent renal parenchyma was calculated by subtracting the median swv of the intact renal parenchyma from the median swv of the focal renal tumour . the variations in the median swvs of the tumours and the normal renal parenchyma and the variations in the median swv difference between the tumours and the adjacent parenchyma in each tumour group were expressed as means and standard deviations . 
when differences among them were found to be statistically significant ( p < 0.05 ) , each group was compared with every other group using the least significant difference ( lsd ) test . 
the mean size of the benign cortical lesions 86 mm ( range 1.550 mm ) and of the malignant cortical lesions ( n 21.5 mm 24 ) was 47.3 ( range 30130 mm )  . 
the haematomas can easily be confused with the transitional cell carcinomas ( tcc ) especially at conventional b - mode us imaging ; however , the swv values of the haematomas were significantly lower than the swv values of the tcc . 
4 swv measurement of a renal angiomyolipoma in the left kidney of a 41 - year - old male patient applied in clinical studies to investigate intra - abdominal tissues [ 12 , 1618 ]  . 
in recent years , this technique has been successfully applied to lesions of the breast , prostate , pancreas , lymph nodes , thyroid gland , testes , and liver . 
one of the main restrictions with arfi imaging is that no quantification could be achieved from cystic lesions which are pure cystic , septated or with semisolid - cystic nature with prevalent cystic components . 
the roi should completely be filled with the solid part of the lesion for a successful swv quantification ; if not , the error expression such as x.xx m / s will be determined on the monitor by the swv measurement . 
this aspect was the main rationale for the exclusion of cystic lesions from our study ; thus , arfi imaging should be considered a potential additional imaging tool to conventional us when investigating visceral lesions , renal masses in this particular study . as rcc is the most common solid renal neoplasm , the diagnosis of a renal mass is virtually a differentiation of rcc from other neoplasms . 
5 receiver operating characteristic ( roc ) curve formed for cut - off measurement of benign and malign lesions elastography techniques , such as acoustic radiation force impulse ( arfi ) elastography and shear wave elastography , have been introduced and are currently being used in the kidney and in other organs [ 79 , 12 , 13 ]  . 
however , these studies have some limitations , including that a relatively small number of focal renal lesions were examined and that the arfi quantification was not applied to all of the patients . 
additionally , an important advantage of arfi imaging in comparison with conventional elastography is that it gives an absolute velocimetric value ( in m / s ) within a restricted area of tissue [ 15 ]  . 
thus , evaluation of deep tissues is more feasible , and this approach has been successfully 1 3 302 radiol med ( 2015 ) 120 : 296303 than those of the renal sinus , and is usually much higher than the hyperechogenicity of small rccs . 
in addition to hyperechogenicity , small rccs often show intratumoural cysts and a thin hypoechoic riother rare renal tumours ( e.g. , renal metastasis from osteogenic sarcoma or thyroid cancer ) may also be hyperechoic [ 11 ]  . 
the amls included in our study were with evident fat content that could be detected with either ct or mr examinations ; unfortunately , amls with poor fat content were not included in present study due to the lack of patients . 
thus we are of the opinion that future prospective studies should be encouraged to reveal the efficiency of swv quantification by arfi in the differential diagnosis of amls with minimal amounts of fat from other solid renal masses including rccs . 
however , it may be difficult to distinguish between the stiffness due to the process of granulomas that form in the kidney from malignant lesions . there are some limitations to our study . 
in addition , elastography for pure cystic lesions and / or cystic lesions with septations does not provide useful information , and the compression of the solid portion may be affected by the lack of strain of the fluid portion [ 20 , 21 ]  . 
furthermore , various factors such as lesion size , depth , and density can affect the performance of elastography , and it can be difficult to achieve optimal image quality for every case . in conclusion , our prospective study shows that arfi imaging may be useful for differentiating between benign renal lesions and malignant renal tumours . 
mean follow - up time was 2 , 364 days . results surgical correction was required in 3 / 13 patients ; in 8 / 13 cases , there was complete disappearance of clinical symptoms without bile duct dilatation ; in one case , an asymptomatic persistent bile duct dilatation was detected while in the other case , the liver is currently in cirrhotic degeneration ( 69 % clinical success including the asymptomatic patient with biliary dilatation )  . 
citta` della salute e della scienza di torino , via genova 3 , turin 10126 , italy were two cases of long - term restenosis and two cases of transient haemobilia . conclusions percutaneous procedures effective therapeutic options for the treatment of biliary strictures after paediatric liver transplantation . safe interventional radiology ( cid : 2 ) liver keywords transplantation ( cid : 2 ) bile duct stenosis ( cid : 2 ) percutaneous transhepatic biliary drainage ( cid : 2 ) bilioplasty interventional radiology liver transplantation abbreviations lrlt living related liver transplantation ptbd percutaneous transhepatic biliary drainage introduction liver transplantation ( lt ) represents the treatment of choice for paediatric patients with congenital metabolic liver disease , acute hepatic failure , early - stage malignancy and cirrhosis [ 1 ]  . despite renements of surgical techniques , biliary complications are one of the most relevant follow - up issues of paediatric lt and they still remain a major challenge . the reported incidence of complications is 1030 % of paediatric lt [ 2 ]  . 
the most common complications are bile leaks and strictures which can cause post - transplant morbidity , graft loss and death . in recent years , treatment modalities have changed towards primarily nonsurgical approaches , leaving the surgical option for lesions which are not otherwise curable . interventional is therefore increasingly considered the rst - line option for biliary stenosis , and both radiology ( ir ) 290 radiol med ( 2015 ) 120 : 289295 ischaemic ( usually nonanastomotic and probably due to arterial insufciency ) and brotic ( usually anastomotic and secondary to scar tissue causing retraction of the common bile duct ) obstructions can be treated [ 3 ]  . nevertheless , no prospective or randomised studies have been published that investigate the safety and the efcacy of ir . 
the biliodigestive anastomosis was involved in all cases , and the intrahepatic bile ducts were also involved in four cases . mean time to onset of the stricture was 463.3 days ; in one case , the stenosis was due to previous surgical treatment of a bile leak . 
as for ischaemic ( or nonischaemic ) aetiology , all intra - hepatic stenoses ( four patients ) were ischaemic , as were six of the extrahepatic strictures ( four of them were associated with intrahepatic stenoses )  . the study of the hepatic artery was always performed with ultrasound ( us ) examination as a rst approach ; in order to avoid radiation exposure , computed tomography ( ct ) angiography was performed only in cases requiring a preoperative assessment . a diagnosis of biliary stenosis was established in one case on the basis of us and magnetic resonance ( mr ) cholangiography demonstration of bile duct dilation without clinical symptoms , in eight cases based on cholangitis ( including one case of severe sepsis ) and in the remaining nine cases based on increased cholestasis on routine laboratory tests . two of bile leaks were never treated percutaneously , whereas 13 / 18 biliary strictures underwent percutaneous treatment ( 13 patients )  . 
the other 5 / 18 patients , after multidisciplinary assessment , underwent surgery : them because of a concomitant vascular problem at the anastomosis level ( one arterial and one portal anastomosis ) ; another two cases because the stenosis was considered not passable at percutaneous transhepatic cholangiography ( ptc ) and therefore no percutaneous attempts were made ; in one case , one of the two ducts of the split liver was occluded during transplantation . and missed procurement during anaesthesia , deep sedation and antibiotic coverage anaesthesia and deep sedation were always performed by experienced staff ; patients younger than 4 years were generally intubated and sedated in the operating room and then transported to the angiographic suite . 
strict monitoring of vital parameters with pressure measurement , heart rhythm ( ecg ) evaluation and arterial oxygen saturation determination was carried out throughout the procedure and in the hours following the radiological treatment . as for antibiotic coverage , third generation cephalosporins were routinely administered , according to the weight of the patients , within 1 h before the procedure and for the following 7 days . table 1 transplant indications transplant indication no . 
patients radiation protection biliary atresia hepatoblastoma ossalosis type i haemangioendothelioma primary sclerosing cholangitis ? ulcerative colitis primary non - function cholangitis ? chronic rejection in accordance with the alara ( as low as reasonably the following achievable ) principle of optimisation , radiation protection measures were taken : us guidance whenever possible , use of pulsed uoroscopy with intervals as large as possible ; thin collimation , use of the last image hold instead of exposures ; reduced kv and ma ( 68 kv and 1.5 ma ) , use of leaded protection for the portions of the body out of the operative area . 
subsequently , a dilation is performed with a cutting balloon catheter ( 5 mm diameter ) ( d , e ) and then with a conventional balloon catheter ( 6 mm diameter ) ( f , g )  . 
final control demonstrates the good result of the procedure ( h ) assessments , where , in any case , few seconds of radiation exposure were needed . equipped with a my lab 25gold esaote system ( esaote spa , genoa , italy )  . procedural technique at our department , the percutaneous treatment of biliary complications in paediatric lt is performed in two interventional suites , equipped with multi - diagnost iii philips ( philips medical systems , best , netherlands ) and allura xper fd 20 philips , respectively . 
in patients who had received a whole graft , percutaneous access was chosen on the right side next to the midaxillary line , while the epigastric approach was preferred in patients with reducedor splitliver grafts or lrlt . in order to catheterise the biliary tree , a biliary access system ( pbn medicals , stenolse , introducer coaxial 292 radiol med ( 2015 ) 120 : 289295 denmark ) was inserted into the bile duct under us and uoroscopic guidance . 
 [ 10 ] , the cutting balloon was inated to 10 atm for 35 mafter that , it was deated , rotated less than 90 ( cid : 3 ) and reinated at the same site for another 35 min . at the end of the procedures , an externalinternal biliary drain was placed ( 47 fr ) , and usually kept in place for 57 days . 
subsequently , percutaneous transhepatic biliary drainage ( ptbd ) was repositioned for other 57 days . mean time was 2 , 364 days follow - up ( range 9284736 days )  . evaluation of results we dened technical success as the ability to cross the stenosis and to perform the balloon dilation . 
clinical success was considered the complete disappearance of symptoms in the presence of normal laboratory and us ndings and absence of relevant stenosis at the last cholangiographic study . restenosis was diagnosed when , after removal of the biliary drain , clinical symptoms ( jaundice , cholangitis ) together with laboratory and radiological ndings ( us and mr cholangiography ) led to suspect a biliary restenosis . 
therefore , the patients underwent surgery resulting in healing in one case , moderate cholestasis with persistence of biliary dilatation in one case and retransplantation in one case ; in these patients the drainage was left in place so as to provide a bile duct landmark during surgery and a useful support for reconstruction of the anastomosis . ten out of 13 patients ( 77 % ) underwent percutaneous treatments only : in 6 / 10 cases , a single session of bile duct balloon dilation was performed , in 2 / 10 patients two bile duct balloon dilations , in 1 / 10 patient three balloon dilations , while in 1 / 10 patients ve sessions of balloon dilation were needed . 
the patient ( 1 / 13 ; 7.7 % ) treated with ve sessions of balloon dilation is currently , after 382 days of followup , in a condition of cirrhotic degeneration ( positive biopsy for hepatic brosis )  . of the ve patients who underwent surgery as a rst approach , two ( 40 % ) had a postsurgical stricture which needed percutaneous revision ( a single session of balloon dilation ) : in these cases , a complete clinical success ( 100 % ) was obtained . overall , the clinical success of ir ( in the thirteen patients treated with the percutaneous approach as the rst - line treatment ) was 69.2 % ( 9 / 13 patients , including patients with asymptomatic biliary dilatation )  . 
during follow - up , two patients after 571 and 2 , 070 days , respectively , had a restenosis which required percutaneous treatment ( with the use of cutting balloon in one patient ) : these two patients are currently asymptomatic , with complete clinical success . with the exception of two cases of transient haemobilia with spontaneous regression ( both during cutting balloon procedures ) which can be reported as minor complications , the procedures were not burdened by other minor or major complications . discussion in the 13 patients who underwent the percutaneous treatment as the initial approach , there was a 100 % ( 13 / 13 ) technical success . 
in three cases ( 23 % ) , early restenoses were promptly detected at the rst cholangiographic study biliary complications are one of the most important issues in the follow - up of paediatric lt . 
their incidence varies , depending on reported series , from 10 to 30 % of transplants [ 2 ] , and the role of radiology in their diagnosis and treatment is becoming increasingly important [ 5 ]  . results radiol med ( 2015 ) 120 : 289295 294 radiol med ( 2015 ) 120 : 289295 table 3 percutaneous treatment of biliary strictures after paediatric liver transplantation : literature review series no . 
in paediatric transplantation , however , surgery is the treatment of choice for bile leaks [ 2 ] , but not for stenoses where it is burdened with high morbidity and mortality [ 1 , 2 ] : therefore , percutaneous therapy can be considered an effective treatment option , according to the experience of many liver transplantation centres . as noted by miraglia et al . , there are no prospective randomised studies on the management of biliary complications after liver transplantation . 
 [ 9 ] ( where technical success varied from 67 to 85 % ) and in other studies ( table 3 )  . moreover , although many series agree on a low complication rate [ 1 , 7 , 8 ] , moreira et al . 
review [ 4 ] reported a higher rate of minor complications : 125 minor complications were reported ( in this group , however , smaller events were included such as localised skin abscesses at catheter insertion site , dislocations or partial obstruction of the drainage ) in 64 patients . 
 [ 4 ] performed a very large number of percutaneous transhepatic cholangiography for diagnostic purposes only ( table 3 )  . our series , in accordance with other reports , conrms the safety of the percutaneous treatment : only two minor complications ( two cases of transient haemobilia , 2 / 13 patients , 15.4 % ) and no major complications were reported . as for drainage infection , the number of infectious complications , as pointed out by moreira et al . 
 [ 4 ] , is proportional with the increased time of drain allocation . therefore , the absence of infectious complications in our series can be explained not only with full adherence to aseptic measures but also with the short time of drain allocation : 34 days for our series , 122 days in miraglia et al . 
it must be noted , however , that they considered success as the complete resolution of the stenosis after only one session of bilioplasty ; even adopting this strict criterion our restenosis rate would have been 40 % ( 4 / 10 patients )  . 
in particular , the use of these balloons is useful in the dilatation of particularly resistant stenoses in which the traditional balloon catheter performs poorly , even reaching the maximum recommended pressure for the various types of catheters ( 1220 atm )  . 
in these cases , we consider it crucial to perform a preventive dilatation using a cutting balloon catether ; then the anastomosis is reshaped with a traditional balloon catheter , 12 mm diameter higher than the previous one . 
even more interesting is the use of these cutting balloon catheters in eccentric stenoses where traditional balloons tend to mainly dilate the nonbrotic portion of the stenosis with good immediate results but with a constant tendency to elastic recoil restenosis . 
in these cases , the cutting balloon can shape also the brotic portion , making the result more permanent . in a recently published editorial , de ville [ 11 ] emphasises the radiological risks of paediatric patients undergoing interventional procedures or radiological examinations ; he radiol med ( 2015 ) 120 : 289295 also emphasises the presence of papers reporting highly complex interventional procedures ( as are these procedures ) with excellent results in terms of efcacy but with little or no regard or data about the radiation protection issues . to our knowledge , our group has published the single article reported in the literature on the radiation protection of paediatric patients during percutaneous biliary procedures [ 12 ]  . 
furthermore , our radiation protection measures were extremely restrictive in accordance with the alara ( as low as reasonably achievable ) principle of optimisation . they also substantially coincide with the safety campaign guidelines for radiation protection proposed in 2010 by the seattle childrens hospital and boston childrens hospital through the image gently , step lightly campaign to raise awareness of radiation protection [ 13 ]  . 
 [ 4 ] , where uoroscopic guidance only was used , our group used us guidance as far as possible . conclusion our experience conrms the feasibility , safety and efcacy of the percutaneous treatment of biliary strictures after paediatric liver transplantation . 
a reduced time of allocathe drainage catheter after balloon dilatation tion of decreases the risk of infectious complications ; the use of a cutting balloon has an important role in limiting the risk of restenosis also in paediatric patients . 
in fact dent [ 3 ] and kreipe [ 4 ] suggested that senile osteoporosis is a paediatric disease . the mechanisms of bone homeostasis are influenced by both environmental and genetic factors , and it is known from the literature that specific genes have a strong influence on bone formation and resorption , as demonstrated by the higher correlation level of osteocalcin found in monozygotic twins compared with dizygotic ones [ 511 ]  . although several studies have explored the genetic contribution to bmd and osteoporosis in general [ 6 , 7 ] , most of them have been based on a quantitative assessment of 1 3 278 radiol med ( 2015 ) 120 : 277282 bone mass per surface unit ( g / cm2 ) by dual - energy x - ray absorptiometry ( dxa ) [ 11 , 12 ] , and of volumetric unit ( g / cm3 ) by quantitative computed tomography ( qct ) [ 13 , 14 ]  . 
however , the associated structural bone impairment observed in osteoporosis encouraged the search of genetic factors influencing bone architecture and , therefore , the identification of alternative techniques , capable of assessing not only bmd , but also bone quality . quantitative ultrasound ( qus ) has been recently proposed as a noninvasive method of estimating bone tissue properties such as structure and elasticity [ 1518 ]  . 
this technique is safe , easy to use , and radiation - free ; the equipment can be transported , and it is relatively cheap in comparison with more expensive densitometric techniques such as dxa and qct . 
clinical studies showed qus capability to discriminate between osteoporotic and healthy women [ 1924 ] , and it may predict fracture independently of bmd [ 19 , 24 ]  . 
up to now two peripheral sites have been mostly investigated by qus : calcaneus and hand phalanges . in this cross - sectional observational study we investigated the qus parameters of the hand phalanges in two groups of monozygotic twins divided by age into growing individuals ( up to the age of 18 years ) and adults ( more than 18 years of age )  . we used the qus technique to examine the phalanges due to its capability to provide different information on ultrasound propagation : besides measurement of the velocity of transmission ( amplitude - dependent speed of soundad - sos ) , it enables quantification of the mor phological changes in the characteristics of the ultrasound wave propagated through the bone tissue . 
thus , the purpose of this study was to evaluate the similarities and differences in bone mass and structure between couples of monozygotic twins as measured by means of the qus technique at the hand phalanges , outlining the differences between growing subjects and adults . materials and methods subjects one hundred and twenty - nine pairs of monozygotic twins were measured by qus at the phalanges at a twins community convention in italy ; of these , 42 pairs of paediatric age ( range 118 years , 30 girls and 12 boys ) and 87 pairs aged 1871 years ( 51 males and 36 females )  . 
zygosity was self - reported by the examined subjects and evaluated by clinical observation . the study was approved by local institutional review board and informed consent for the study was obtained from all human subjects according to the declaration of helsinki . qus measurement qus measurements were performed using a dbm sonic bone profiler ( igea , carpi ( mo ) italy ) , an ultrasound device emitting 1.25 mhz ultrasound frequency pulses by piezoelectricity [ 15 , 16 , 18 ]  . the device consists of a transmitting and a receiving probe attached to a calliper that measures the thickness of the phalanx . 
the qus measurement was performed at the distal meta - diaphyseal region of the proximal phalanges of fingers 25 of the non - dominant hand ; however , studies have demonstrated that no differences could be observed in qus measurements between the dominant and nondominant hand [ 23 ]  . 
the device automatically calculates the average ad - sos ( amplitude - dependent speed of sound unit : m / s ) through the finger phalanges of the four acquisitions . 
amplitude - dependent speed of sound means that the speed of sound is calculated when the signal reaches a fixed amplitude threshold of the ultrasound - received signal by dividing the measured thickness of the phalanx by the time elapsed between emission and reception of the ultrasound pulse at the probes . 
the device also stores and analyses the digitised waveform of the received ultrasound signal after it has crossed the phalanx ; this analysis involves the calculation of a set of parameters for each ultrasound signal . 
 we considered in this study the analysis of bone transmission time ( btt ) , expressed in s , which is the interval between the first received signal and the received signal that is propagated through soft tissue only ( speed of sound in soft tissue is 1 , 570 m / s )  . 
btt seems to reflect bone tissue properties that are different from bmd , linked to bone structure and mechanical competence [ 22 , 24 ]  . measurements were performed using two cross - calibrated devices ; calibration was done with a plexiglas phantoin vitro precision in a single device using the plexiglas phantom was 0.4 % ; the two devices were cross - calibrated and a difference in plexiglas velocity between the two devices was lower than 10 m / s . 
measurements were made by two technicians with 5 years experience of phalangeal qus measurements . the short - term in vivo precision was calculated by measuring five times , once a week for a period of about 1 month in ten healthy young adult women . 
the short - term 1 3 radiol med ( 2015 ) 120 : 277282 in vivo precision was 0.5 % for ad - sos and 1.8 % for btt in our centre [ 22 , 26 , 27 ]  . statistical analysis the analyses were performed for the whole population and separately for children and adults . 
we aimed to describe the bone tissue quality similarities and differences between growing twin subjects and twin adults to estimate the capability of qus to disclose the relevance of epigenetic changes in the modulation of such a hereditary character between twin subjects . 
in fact , recent evidence shows that although monozygotic twins share the same or a very similar dna sequence , their gene expression and dna modification patterns can be significantly different and may play a crucial role in phenotypic outcomes . 
 processes regulating gene expression do not involve dna sequence but are based on epigenetic mechanisms , which are heritable and potentially reversible chemical modifications of dna and / or of the chromatin structure [ 28 ]  . 
epigenetic control of gene expression is mainly based on dynamic processes of dna methylation which can change through different developmental stages and in different tissues and can be subjected to environmental factors , and stochastic events . 
studying epigenetic modifications and their effects on gene expression in monozygotic twins discordant for phenotype may increase the understanding of diversity from common normal traits to diseases [ 29 , 30 ]  . we studied the intrapair association of qus parameters in growing twins and adult ones , demonstrating that the linear associations of qus parameters with age , height and weight are significantly higher in children than in adults . 
 furthermore , the positive association among qus parameters and age , height and weight in children clearly reflects the effects of growth , whilst the negative association found in adults among qus parameters and age , indicates the effect of increasing incidence of osteoporosis with age . 
 these results are expected as already observed in the literature in healthy children and adult populations [ 31 , 32 ]  . 1 3 280 radiol med ( 2015 ) 120 : 277282 fig . 
1 scatter plots showing correlation coefficients for amplitudedependent speed of sound ( ad - sos ) ( m / s ) and bone transmission time ( btt ) ( s ) between pairs of child and adult twins . 
in child pairs ( upper scatter plots ) , data points are closely plotted along a straight line ( high correlation ) going from the origin out to high xand y - values ( positive correlation )  . 
 [ 34 ] , where groups of monozygotic and dizygotic twins were analysed . even though correlation coefficients were extremely high for adults , in children they were significantly higher and close to the maximum value ( r 0.987 ) , emphasising how similarity between twins is more evident in children than in adults . 
even the analysis of correlation among differences in ad - sos and btt with age 0.374 results in a significantly positive association ( r and r 0.400 , p < 0.0001 for ad - sos and btt , respectively ) , indicating a progressive linear trend toward increasing diversity between twins with increasing age . 
 this aspect strengthens the hypothesis that environmental factors such as personal behaviour and lifestyle would co - regulate bone homeostasis influencing its progressive differentiation . similar results were observed in another study conducted on an italian twin cohort of males and females , where a positive correlation between differences in adsos and age was observed for females [ 36 ]  . 
in that study the majority of subjects were adults , the group of children was limited to few cases and a separate analysis on children only was not possible . 1 3 radiol med ( 2015 ) 120 : 277282 our study suffers some limitations : the lack of an extensive distribution of this group over all ages , especially older age : it was expected that only mobile older twins would have attended the meeting , introducing a bias in the population selection . 
furthermore , measurements were taken only at one skeletal site and a genetic investigation to further investigate its contribution to qus parameters was not feasible . apart from these limitations , separate analysis on child twins still remains an important strength of this study , showing qus capability to highlight the genetic contribution to bone mass and quality . 
the programs selected all meet the basic requirements such as free availability , stand - alone application , presence of graphical user interface , ease of installation and advanced features beyond simple display monitor . 
capabilities of data import , data export , metadata , 2d viewer , 3d viewer , support platform and usability of each selected program were evaluated on a scale ranging from 1 to 10 points . results twelve programs received a score higher than or equal to eight . 
among them , five obtained a score of 9 : 3d slicer , medinria , mitk 3m3 , volview , vr render ; while osirix received 10 . conclusions osirix appears to be the only program able to perform all the operations taken into consideration , similar to a workstation equipped with proprietary software , allowing the analysis and interpretation of images in a simple and intuitive way . 
this application is also a good tool for teaching activities because it facilitates the attainment of learning objectives among students and other specialists . keywords open source post processing diagnostic imaging g . 
giovagnoni pediatric and special radiology , univpm , aou ospedali riuniti , ancona , italy introduction open source software ( oss ) is a model for development , dissemination and cooperation in the field of information technology , created in 1985 with the establishment of the free software foundation ( fsf ) and formalised in the socalled general public license ( gpl ) [ 1 , 2 ]  . 
according to that document , a developer must make available all the source code and information necessary to compile ( dependencies , libraries , technical documentation ) the application to allow others to : duplicate / install multiple copies within their organisation ; change / extend or incorporate it into other systems ; commercialise the extensions made , being only constrained to provide the source code of the extensions made [ 3 , 4 ]  . over the years , it became clear that an ideological redefinition of free software was needed to highlight the 1 3 310 radiol med ( 2015 ) 120 : 309323 advantages both as a model of development and in terms of commercial prospects ; fsf duly created the open source initiative which coined the term open source and has encouraged the spread of less restrictive licenses than the gpl [ 5 ]  . oss software is free but not necessarily freeware ; oss is not an alternative to commercial software ; their model does not preclude the presence of commercial distribution , suppliers of added value or support services . 
it is more correct to define oss as an alternative to the conventional licensing model ( closed source ) , where access to the source code is not granted and in which the software developer retains the rights to their own product , selling the user a temporary or permanent license to use , which allows them to use it without , in any way , acquiring property rights [ 6 ]  . the process of sharing applications and their source code has played an important role in the management and dissemination of digital images in the biomedical field . 
the processing of medical images implies , in fact , a series of activities that must be performed by specific software : first , applications need to read the input data from one or more files , previously created by a diagnostic imaging device [ 7 ]  . 
this is not always easy because the data may be available in many different proprietary formats even though the introduction of the dicom standard is now an indispensable element of uniformity of the format of radiological images , allowing shared management between systems with different hardware and software [ 8 ]  . moreover , several frameworks and support structures have been developed in which software can be arranged and designed and then used in different applications , facilitating the work of programmers by avoiding unnecessary duplication of effort . 
this operating model has created a huge number of freely available libraries and application program interfaces for the analysis and management of medical images , present in many programs , in terms of cross - platform applications [ 9 ]  . 
among the various frameworks for reading and writing common image formats , it is appropriate to mention the insight tool kit ( itk ) , designed to be easily extensible to different types of files that are used in medical image processing , such as dicom , interfile or other proprietary formats [ 10 ]  . 
another item of oss is the vtk library which contains many algorithms for 2d / 3d image design visualisation and processing , and allows both volume rendering and various surface rendering techniques . in this paper , the authors attempt to verify the number of and describe the functionality offered by , freely available and accessible oss applications , as well as their potential in the management ( production , storage , processing and transmission ) of biomedical images to assess their abilities in comparison to those offered by proprietary software ( closed source )  . materials and methods the study was carried out with methods similar to those used in an earlier scientific paper that tried to collect , describe and compare the characteristics of software applications freely available and accessible on the internet [ 11 ]  . the basic software requirements were : free availability , that is , applications must be freely downloadable from the net ; stand - alone , i.e. , the software is not just a plug - in for a generic image viewer ; the presence of a graphical user interface ( gui ) , to allow the interaction of the user with the software without the need for a command line interface ; easy installation : applications were excluded if their installation involved the execution of commands from the terminal or required other programs . advanced features beyond simple monitor display . the selected programs ( split into two categories : windowslinux and macintosh ) are shown in tables 1 and 2 . 
in particular , the presence or otherwise of functions ( data import , data export , metadata , 2d viewer , 3d viewer ) is listed , and an assessment of usability was made with a score from 0 to 10 in terms of gui , speed and simplicity . the overall evaluation was scored from 0 to 10 based on the average value of the item usability with the increase or decrease of one point because of presence or otherwise of 2d and 3d functions of each program . the programs were tested using four different sets of images ( table 4 ) on personal computers having the characteristics shown in table 5 . results 3d slicer the results of the comparison are shown in tables 6 and 7 . 
the application is platform - independent ( windows , linux or mac osx ) and has an intuitive and userfriendly interface ( for example , it allows you to load data using drag and drop )  . 
among its strengths are tools for navigation and visualisation of multimodal and multidimensional images : 2d / 3d viewer , 4d viewer ( 3d series with temporal dimension , e.g. , cardiacct ) and 5d viewer ( 3d series with temporal and functional dimensions , e.g. , cardiac - pet - ct )  . 
it is extremely simple and intuitive . the features supported by most software analysed rarely meet all the real needs of operators : some have simple and intuitive interfaces , but lack basic operations in 2d ( imagevis3d ) , or while supporting the viewer function do not offer additional tools ( aeskulaps , amide , dicompyler , endrov , eviewbox , imagevis3d , irad , itk - snap , nukak3d , tudor dicomtools and weasis )  . 
in other cases , programs do not offer satisfactory direct import of dicom images , resulting in significant information loss , and need conversion tools ( bioimagexd and imagevis3d )  . 
among those that have integrated almost all the post - processing tools , some require a large amount of memory and high performance hardware ( gimias , imagevis3d , mayam , mipav and mitk 3m3 ) or do not offer practical possibilities for volumetric analysis ( madena )  . 
this situation does not depend on issues in software development , but on the fact that software is usually developed on linux or unix machines by users with mediumhigh experience who are able to interact with the software by command line . 
in contrast , on windows systems , with users typically with low - to - medium knowledge , 1 3 316 radiol med ( 2015 ) 120 : 309323 1 3 radiol med ( 2015 ) 120 : 309323 the community usually develops stable software with a gui and therefore does not require interaction from the terminal . it should be pointed out that no software was awarded the maximum score , because none fulfils all the real application requirements . 
this application has all the characteristics of a suitable tool for postprocessing : able to analyse the images in the different representations , very fast in drawing 3d , most complete and interactive menu , but it fails to integrate all the functionality of a workstation , such as curved planar reformation . as for the macintosh platform ( table 7 ) , vr render , volview and medinria deserve special mention , and appear to be the most mature and fully functional projects , offering comprehensive tools associated with easy and accessible interfaces . 
each one has various possibilities for improvement that the community certainly will not take long to implement ( ability to perform mpr curves or ssd ) [ 15 ]  . osirix deserves a separate discussion ; the analysis shows it to be the only software able to perform all operations on par with dedicated workstations with proprietary software . in view of the undoubted potential of oss applications , it should be emphasised that an essential regulatory aspect is crucial for the diagnostic use of such software [ 16 ]  . 
according to the definition of eec directive 93 / 42 on medical devices , implemented in italy by legislative decree n.46 / 1997 , pacs systems are medical devices , by virtue of being used for diagnostic purposes . 
the main factor that prevents the certification of oss applications distributed with the source code is because there is no guarantee that the certified software is the same device that you are using since anyoneeven the same usercould change the code and consequently invalidate its certification . 
with proprietary software there is no possibility of changing the code because no one can access the source code and modify it , thus there is no possibility of making unauthorised changes . 
an oss application will be approved for diagnostic use if the developer ( or the distributor of the product ) has fine - grained control of the distributed version and inhibits access to the source code , failing which the penalty would be loss of certification [ 17 ]  . 1 3 318 radiol med ( 2015 ) 120 : 309323 fig . 
long - term survival can be expected in some of these patients and late toxicity can be observed , becoming essential to evaluate organs at risk , particularly the parotid glands even in metastatic patients . 
we compared the 2d with 3d technique to evaluate parotid glands involvement and received dose , and coverage of the clinical target volume . materials and methods seven patients were considered . the prescribed dose was 30 gy in ten fractions . 
dannunzio university , chieti , italy conclusions planning whole - brain radiotherapy with only the 2d technique involves a risk of including parotid glands in the eld and not covering the clinical target volume . 
the 3d technique should be systematically performed and the parotid glands should be regarded as an organ at risk in whole - brain radiotherapy . keywords whole - brain radiotherapy ( cid : 2 ) parotid gland ( cid : 2 ) computed tomography introduction whole - brain radiotherapy ( wbrt ) is applied as part of the curative treatment in patients affected by primary central nervous system lymphoma ( pcnsl ) and it plays a prophylactic role in patients with small - cell lung cancer ( sclc ) [ 1 , 2 ]  . 
in most cases wbrt is performed as standard therapy in patients with multiple brain metastases [ 3 , 4 ] that represent a major cause of morbidity and mortality in patients with cancer [ 5 , 6 ]  . in patients with pcnsl subjected to curative wbrt alone , a 5 - year overall survival of approximately 18 % can be observed , and in patients with sclc and limited disease an overall survival of 2025 % at 5 years can be expected [ 7 , 8 ]  . 
in the context of palliative wbrt , local control , palliation of the brain symptoms , prevention of neurological morbidity and maintenance of good quality of life are the main objectives [ 6 ]  . when radiation therapy is performed in patients with multiple brain metastases , it may happen that the potential radiation - induced complications are relatively neglected because of the unfavourable prognosis . 
however , in certain patients with brain metastasis long - term survival can be expected , especially in the case of age \65 , number of radiol med ( 2015 ) 120 : 324328 metastases \3 , good performance status , recursive partitioning analysis ( rpa ) class 12 , and favourable primary site ; in such cases late toxicity can be observed [ 6 , 9 ]  . given the improved survival of patients with favourable prognostic features , toxicity should be considered and possibly avoided , evaluating the organs at risk ( oar ) of toxicity . 
wbrt is technically simple and the prescription dose ( 30 gy in ten fractions or 20 gy in ve fractions ) is usually low but potentially able to damage the parotid glands . 
a low mean dose of radiotherapy on the parotids can induce unexpected salivary dysfunction in the acute phase and salivary dysfunction can result in caries , impaired swallowing , malnutrition , deterioration of the these alterations become important quality of life ; all whenever a long - term survival can be expected . however , the parotid glands are not routinely delineated as oars in wbrt and palliative brain treatment is often planned with a 2d technique that does not allow one to see if the parotid glands are included in the eld and to know the dose received by the glands . this study compared executive 2d techniques with 3d techniques for wbrt to evaluate inclusion of the parotid glands in the wbrt elds and to know the received dose . we also evaluated the coverage of the clinical target volume ( ctv ) obtained with the two planning methods . materials and methods the 2d and 3d techniques were compared in seven patients with brain metastases referred to our institution . all patients were diagnosed with brain metastasis or primary brain tumour and received palliative wbrt . 
according to calculation data , we analysed the dosevolume statistics of the parotid glands ( mean dose and v15 ) to estimate the risk of developing xerostomia ; we also analysed coverage of the ctv . 
palliative wbrt is the standard therapy in patients with multiple brain metastases , which represent a major cause of morbidity and mortality in patients with cancer [ 15 ]  . 
when prophylactic cranial irradiation is performed in patients affected by scls with complete response after chemotherapy and radiotherapy , the purpose is to reduce the risk of brain metastases , while it is not certain that an increased long - term survival can be obtained [ 1 , 6 ]  . in the context of palliative wbrt , the main objectives are local control , palliation of the brain symptoms , and prevention of neurological morbidity , while a prolongation of survival cannot always be expected . 
in particular , the parotid glands have not been regarded as an oar in wbrt , because of both the unfavourable prognosis and than head and neck lower the prescription dose 326 radiol med ( 2015 ) 120 : 324328 radiotherapy . 
however , a low mean dose of radiotherapy to the parotid gland can induce unexpected salivary dysfunction in the acute phase and salivary dysfunction can result in severe deterioration of the quality of life . moreover , long - term survival can be expected in selected patients with brain metastasis . 
these include those aged \65 , with number of metastases \3 , good performance status , rpa class 12 , and favourable primary site . as a result , late toxicity could develop and chronic salivary dysfunction will be problematic in these patients [ 9 , 12 , 13 ]  . 
given the improved survival of patients with favourable prognostic features , toxicity should be considered and possibly avoided , and the parotid glands should be routinely delineated as oars and quality of life should be maintained even in these patients . furthermore , palliative brain treatment is often planned with a 3d technique that allows one to see if the parotid glands are included in the eld and to know the dose received by glands . the size and position of the parotid glands are highly variable among patients and these factors affect the irradiated parotid volume . 
particularly , the distance between the borders of the parotid glands and the tuberculum anterior of the atlas can vary considerably and the 2d technique does not represent this distance . 
therefore 3dconformal radiotherapy ( 3d - crt ) should be performed to visualise the glands [ 6 , 14 ]  . the salivary glands are known to be more sensitive to radiotherapy , compared to other normal organs involved in wbrt ; consequently , salivary function can be easily impaired , inuencing quality - of - life . 
linked the salivary ow rate with the average dose and parotid ow rate with the parotid in 88 volumes of patients treated for head and neck cancer between 1994 and 1997 . 
the measurement of salivary ow rate was performed at rest and after stimulation , before and after the same radiation treatment at months 1 , 3 , 6 , and 12 . 
eisbruch also put in relation with parotid volume dose values more than 7 , 15 , 30 , and 45 gy to relate the risk of g4 toxicity [ 15 , 16 ]  . 
in agreement with eisbruch , we considered the v15 \66 % . in our study , we attempted to compare wbrt with 2d and 3d technique in seven patients to evaluate if the parotid glands were included in the wbrt elds when 3dcrt is not employed ; dosevolume characteristics of the parotid glands were also analysed . 
in all cases but one the minimum dose on the ctv was much lower than 95 % of the total prescribed dose and the dose distribution was unacceptable . using the 3d technique we found that a signicant volume of the parotid glands was located within in the wbrt elds , whereas planning with the 2d technique left the ctv uncovered . 
 [ 18 ] compared wbrt carried out with two distinct methods in the treatment of brain metastases : one using a multileaf collimator for eld shaping and protection of oars , and a second one with eld rotation to avoid the eyes . 
the widespread introduction of intensity - modulated radiotherapy ( imrt ) into clinical practice allowed for better sparing of oars by creating steeper dose gradients and increasing conformation of the delivered dose [ 19 ]  . 
3 axial images showing brain and parotid glands coverage and non - coverage 328 radiol med ( 2015 ) 120 : 324328 gland - sparing imrt was compared with conventional radiotherapy [ 20 , 21 ]  . based on these ndings , we can state that the 3d technique in wbrt and thermoplastic masks are indispensable to guarantee visibility of the parotid volume included in the irradiated volume , to ensure set - up reproducibility and to create a treatment plan that can spare the parotid glands while offering the best possible coverage of the treatment volume . conclusions the parotid dose in wbrt signicantly varies due to the variability of the volume and position of the parotid glands and neck position . 
according to our results and the potential risk of xerostomia , the parotid glands should be regarded as an oar in wbrt . moreover , wbrt planned with a 2d technique involves a failure to cover the ctv . 
the 3d technique in wbrt and thermoplastic masks are mandatory to guarantee the visibility of the parotid volume included in the radiation eld , to ensure set - up reproducibility and to create a treatment plan that spares the parotid glands while offering the best possible coverage of the treatment volume . 
use of the parotid - sparing technique should be decided on the basis of prognosis and is mandatory in paediatrics where excellent results can be expected . conict of interest marianna trignani , domenico genovesi , annamaria vinciguerra , angelo di pilla , antonietta augurio , monica di tommaso , giampiero ausili ce`faro , marta di nicola declare no conict of interest . radiol med ( 2015 ) 120 : 11701176 doi 10.1007 / s11547 - 015 - 0555 - 8 radiotherapy moderate hypofractionation and simultaneous integrated boost by helical tomotherapy in prostate cancer : monoinstitutional report of acute tolerability assessment with different toxicity scales giuseppe ferrera1 gianluca mortellaro1 mariella mannino2 giovanni caminiti3 antonio spera3 vanessa figlia3 giuseppina iacoviello4 gioacchino di paola5 rosario mazzola3 antonio lo casto3 filippo alongi6 maria pia pappalardo1 roberto lagalla3 received : 4 march 2015 / accepted : 11 may 2015 / published online : 24 may 2015 italian society of medical radiology 2015 abstract introduction based on radiobiology evidence , hypofractionated radiotherapy has the potential of improving treatment outcome in prostate cancer patients . 
in this study , we evaluated the safety , in terms of acutetoxicity , of using moderate hypofractionated radiotherapy delivered with helical tomotherapy ( ht ) to treat prostate cancer patients . materials and methods between december 2012 and april 2014 , 42 consecutive patients were treated with hypofractionated radiotherapy using ht . 
epic evaluation showed a negligible difference in urinary and bowel function post - treatment , that did not reach statistical significance . conclusions our experience confirms the safety of moderate hypofractionation delivered with ht in prostate cancer patients with low , intermediate and high risk . keywords prostate tomotherapy side effects quality of life introduction prostate cancer ( pc ) is the most commonly diagnosed nonskin cancer in men and it is estimated as the second leading cause of cancer death [ 1 ]  . 
with intensity - modulated radiation therapy ( imrt ) , doses up to 81 gy can be safely delivered , given that this technique is characterized by a high degree of conformality , which allows dose escalation to the target volume while significantly reducing normal tissue involvement [ 5 ]  . 
another important benefit of imrt in pc radiotherapy treatment is that it allows delivery of various doses to different volumes in the same number of fractions : this technique , known as 1 3 radiol med ( 2015 ) 120 : 11701176 1171 simultaneous integrated boost ( sib ) , is applied to irradiate lymph nodes , seminal vesicles , and prostate concomitantly during the same session [ 6 ]  . 
one of the main challenges of imrt in pc is that the steep dose gradient achieved with this technique introduces the need to take into account prostate interfraction and intrafraction motion to ensure an accurate delivery of the prescribed dose . 
different modalities of image - guided radiation therapy ( igrt ) are used to reduce variations in the coverage of the planning target volume , allowing at the same time organ at risk sparing [ 7 ]  . 
various schedules were tested in these studies , from 2.53 gy per fraction ( moderate hypofractionation ) to 7 gy per fraction ( extreme hypofractionation ) [ 1418 ]  . 
patients characteristics are shown in table 1 . in accordance with nccn , three risk groups were identified : low risk ( clinical stage t1t2a , gleason score psa 10 ng / ml ) , intermediate risk ( clinical stage t2bt2c or gleason score 7 or psa 1020 ng / ml t1t2 , gleason 6 , psa > 10 or clinical stage t1t2 , gleason > 6 , score psa 10 or clinical stage t3 , gleason score < 6 , psa < 10 ) , and high risk ( clinical stage t1t3a , gleason score 810 , psa > 20 ng / ml ) [ 19 ]  . most patients received neoadjuvant , concomitant , and adjuvant hormonal therapy of variable duration , according to the stage , the risk group , and the physicians decisions . 
to reduce discrepancies in bladder and rectum volumes between simulation and treatment , each patient followed a predefined bladder - filling protocol : patients drank 500 ml of water , 30 min before the ct scan , to achieve a comfortably full bladder , and emptied their bowel by a self - administered enema . 
clinical target volumes ( ctvs ) and organs at risk ( oar ) were contoured on the pinnacle planning system ; rectum , bladder , and femoral heads were contoured as solid organs , small bowel as whole intestinal cavity . 
planning target volumes ( ptv ) 1 and 2 were defined , respectively , as ctv 1 and 2 plus a 0.8 cm margin except for the prostate - rectal interface , where a 0.6 cm margin was used ; ptv3 was generated adding a 0.5 cm margin to ctv3 . 
target dose coverage for ptv1 was evaluated by homogeneity index ( hi ) and conformity index ( ci ) [ 20 , 21 ]  . we chose this fractionation schedule based on the results of the largest patient series reporting the safety of hfrt compared to conventional fractionation [ 22 , 23 ]  . 
to address the possible under reporting of certain side effects using a single scale , acute toxicity was prospectively recorded according both to rtog and common terminology criteria for adverse events ( ctcae v3.0 ) [ 24 , 25 ]  . 
acute genitourinary ( gu ) and gastrointestinal ( gi ) toxicity was defined as an increase of any symptom during radiation or within 3 months after the end of treatment . 
 the expanded prostate cancer index composite ( epic - 26 ) questionnaire at baseline and at 3 months follow - up was used to evaluate health - related quality of life ( hrqol ) after treatment relatively to bladder and gastrointestinal function [ 27 ]  . 
rectum and bladder dosimetric parameters were retrospectively evaluated for the statistical analysis . statistical analysis continuous variables were analyzed with descriptive statistics ( mean , median , iqr , max , min , range )  . 
end points were analyzed using univariate , multiple logistic regression and contingence tables with fishers exact test for the association between gu and gi toxicity , dose - volume , and clinical parameters . 
we used the wilcoxon signed - rank test to compare the baseline and the 3 month follow - up epic scores . results the median follow - up was 12 months ( range 320 months )  . 
according to the risk group classification , 16 ( 38 % ) , 10 ( 24 % ) and 16 ( 38 % ) patients were classified as low , intermediate , and high risk , respectively . 
 according to the epic questionnaire scores , there was no statistical difference in urinary function ( p 0.7735 ) and bowel function ( p 0.3326 ) between the baseline and the 3 month evaluation ( table 5 )  . discussion our preliminary clinical experience with moderate hypofractionation with sib using helical tomotherapy confirmed that , with this delivery technique , acute toxicities are quite low and similar with other moderate hypofractionation experiences in this setting , as shown in table 6 . 
 [ 28 ] found that gu toxicity g2 was correlated , in a multivariate analysis , with total radiation dose 70 gy and dose per fraction > 2.52 gy , but not with the percentage of bladder volume receiving a specific dose . 
efficacy of this approach is currently questioned , given that several reports demonstrated that variation in bladder filling throughout radiotherapy treatment is not eliminated , despite the use of various protocols table 3 toxicity assessed by rtog , ctcae v3.0 , and ctcae v4.0 toxicity criteria toxicity rtog no . 
consistent with these findings are the results of a retrospective analysis we performed on 15 patients from our series , evaluating changes in bladder volume by recontouring this organ in all daily mvcts : we observed a considerable bladder volume variation , which was significantly correlated with the received dose . 
with regard to gi side effects , we observed only a single episode of rectal bleeding in one patient , which we scored as g3 according to the rtog scale and g2 in the other two systems . 
this favorable toxicity profile confirms the safety of expanding the ptv posteriorly with a margin of 0.6 cm , which was larger than those used in the three studies mentioned above . 
bauer1 thomas lehnert1 received : 29 january 2015 / accepted : 28 april 2015 / published online : 16 may 2015 italian society of medical radiology 2015 abstract objectives to compare radiation exposure and image quality of second - generation 128 - slice dual - source ct ( dsct ) coronary angiography ( ccta ) protocols . materials and methods we retrospectively analyzed data from four groups with 25 patients , each examined by one of the following dsct ccta protocols : prospectively ecg - gated high - pitch ( group 1 ) or sequential ( group 2 ) acquisition , retrospectively ecg - gated acquisition in dualenergy ( dect , group 3 ) or dual - source ( group 4 ) mode . 
during the last decade , several electrocardiogram - gated ( ecg ) techniques for ccta have been introduced to reduce the resulting radiation dose for the patient to even below 1 msv [ 3 , 4 ]  . 
however , in clinical practice not all patients can be evaluated using the proposed protocols with very low radiation exposure due to arrhythmia , tachycardia or body habitus [ 57 ]  . 
 in addition , some indications for ccta require functional analysis of the complete heart cycle which is usually performed using retrospectively ecg - gated protocols [ 8 , 9 ]  . dual - source ct ( dsct ) can be used to reduce examination times during cardiac ct and has also been shown to lower the resulting radiation dose [ 1012 ]  . 
on secondgeneration 128 - slice dsct , two prospectively ecg - triggered ( high - pitch spiral and sequential mode ) and two retrospectively ecg - gated ( dual - energy and dual - source mode ) protocols are available for ccta . 
the prospectively ecg - gated protocols are usually used to achieve substantial radiation dose savings in patients requiring anatomical analysis of coronary artery patency [ 3 , 5 , 7 ]  . 
both retrospectively ecg - gated protocols are mainly used in patients requiring functional analysis of the myocardium during the complete heart cycle or in patients with severe arrhythmia [ 5 , 6 ]  . 
however , to our knowledge there is no published study comparing these four protocols regarding radiation dose and image quality using the same second - generation dsct in clinical practice . therefore , the purpose of the present study was to retrospectively compare the effective dose estimates , measurements of objective image quality and assessment of subjective image quality for clinically indicated ccta examinations using the available prospectively and retrospectively ecg - triggered data acquisition protocols on the same second - generation 128 - slice dsct . coronary morphology is of interest and a regular heart rate with < 55 bpm can be established . 
we use the prospectively ecg - triggered sequential mode if the heart rate even after betablocker application remains above 55 bpm but below 70 bpm or if the heart rhythm is not completely regular . 
 we use the retrospectively ecg - gated spiral acquisition in dual - energy mode in patients referred to us from the emergency department to evaluate wall motion and myocardial perfusion at the same time with coronary morphology . 
above a heart rate of 70 bpm or in case of unstable heart rhythm , the conventional retrospectively ecg - gated dual - source spiral acquisition mode is used in emergency room patients as well as in patients referred to cardiac ct with the dedicated question for functional analysis . retrospective database analysis revealed that in this time span 25 patients had been examined using a prospectively ecg - triggered protocol in high - pitch spiral mode , thus representing the smallest group in terms of patient numbers . 
 hence , to improve comparability of data , 25 patients in the other three groups were randomly selected out of the total cohort . therefore , we included a total of 100 patients who underwent ccta on the same second - generation dsct between january 2012 and february 2013 at our institution to rule out cad . 
 however , segments with a diameter below 1.5 mm , stented segments with an inner stent diameter < 3 mm and vessel segments distal to occlusions were excluded from subjective image quality analysis . materials and methods image acquisition patient selection and study design this retrospective single - institution study was approved by the local medical ethics committee with waiver of the requirement for informed consent . 
data acquired from patients examined using the same second - generation 128slice dsct ( somatom definition flash , siemens healthcare , forchheim , germany ) between january 2012 and february 2013 who had been referred to our department to rule out cad were included in this study . at our institution , we apply the prospectively ecg - triggered high - pitch spiral in cases in which only cardiac and if no contraindications to - blockers were present and the heart rate was above 65 bpm ( beats per minute ) , metoprolol tartrate ( beloc , astrazeneca , wedel , germany ) was administered intravenously in fractions of 5 mg up to a maximum dose of 20 mg prior to the examination . 
first , a 70 ml bolus of iodinated contrast material ( iomeprol ; imeron 400 , bracco imaging , konstanz , germany ) was injected , followed by a mixed second bolus ( 50 ml of a 30 % contrast and 70 % saline solution ) and a final third phase ( 50 ml of a pure nacl bolus )  . 
the test bolus technique ( a bolus of 15 ml of contrast material and 30 ml of nacl bolus ) was used to determine the scan delay time for the angiographic phase . images were acquired in craniocaudal direction in inspiratory breath hold . 
the anatomic range was manually adjusted and confined to the heart as seen on the anteriorposterior and lateral scout images . the data set for the angiographic visualization of the coronary arteries for group 1 and 2 was acquired using a prospectively ecg - triggered protocol in either high - pitch spiral ( group 1 ) or sequential ( group 2 ) mode while data for groups 3 and 4 were acquired using a retrospectively ecg - triggered spiral protocol in either dual - energy ( group 3 ) or dual - source ( group 4 ) mode . 
the resulting average scan time was ~1 s for group 1 and ~8 s for groups 24 . 64 for all examination protocols , automated dose modulation ( caredose , siemens healthcare ) and tube modulation were enabled and z - flying focal spot technique was used . 
dual - energy cta was reconstructed using the qca hybrid algorithm combining highand low - pass filtered data from the highand low - energy spectra as described by nance et al . 
the effective dose [ ed ( msv ) ] was estimated using the method proposed by the european working group for guidelines on quality criteria in ct derived from the product of the dlp and a weighting factor of 0.017 msv / mgy / cm [ 15 ]  . as the electronic chart system of the hospital did not contain current data about the patients body weight at the day of the ccta examination , the two largest axial thoracic diameters [ anterior - posterior ( ap ) and right - to - left ( lat ) ] were measured in each patient to allow for comparison of body habitus as previously described [ 16 ]  . 
first , the following formula was used to calculate the effective diameter : effective diameter ( cm ) a conversion factor based on the effective diameter and the 32 cm diameter phantom reference numbers provided by the aapm report no . 
204 was selected for each patient and ssde was calculated using the following formula [ 17 ] : ssde ( mgy ) ctdivol conversion factor . assessment of objective image quality objective image quality of the right ( rca ) and left coronary artery ( lca ) were evaluated using the region - ofinterest ( roi ) technique . 
image noise , signal attenuation , contrast , signal - to - noise - ratio ( snr ) and contrast - to - noiseratio ( cnr ) were measured for both vessels : the ascending aorta and the interventricular cardiac septuto ensure data consistency , each roi measurement was performed three times and mean values were calculated . 
image noise was defined as the standard deviation ( sd ) measured in an roi placed in the area in front of the sternum of the patient . intraluminal coronary artery signal attenuation was measured by placing rois centrally in the proximal segments of the left main ( lm ) , lad , left circumflex ( lcx ) and rca . 
based on these measurements , snr and cnr were determined according to the following formulas : attenuation in the ascending aorta / image a : snr noise b : cnr attenua ( attenuation in the ascending aorta tion of the interventricular cardiac septum ) / image noise estimation of the ct radiation dose evaluation of subjective image quality patient protocols of all performed ccta examinations were assessed and dose length product ( dlp ) and volume according to the 15 - segment model proposed by the american heart association [ 18 ] , each coronary artery segment was 1 3 radiol med ( 2015 ) 120 : 11121121 1115 evaluated regarding subjective quality by two observers with 3 and 4 years of experience in evaluating ccta examinations . 
image quality was assessed using a four - point rating scale ranging from 1 to 4 ( 1 : excellent image quality ; 2 : acceptable , not compromising diagnostic image quality ; 3 : poor image quality for single coronary segments ; 4 : non - diagnostic )  . 
segments with a diameter below 1.5 mm , stented segments with an inner stent diameter < 3 mm and vessel segments distal to occlusions were excluded from analysis similar to prior studies [ 16 ]  . statistical analysis statistical analysis was performed using dedicated software ( bias 9.08 , epsilon verlag , frankfurt , germany )  . 
 patient age , heart rate , measured thoracic diameters , attenuation values , snr , cnr , ctdi , ssde , dlp and ed are expressed as mean values standard deviations . 
to test for rejection of the null hypothesis of random distribution , comparison of these variables from all four groups was performed using the analysis of variance test ( anova )  . 
a p value of < 0.05 was considered statistically significant . the inter - rater agreement between the two observers regarding the evaluation of subjective image quality was calculated using cohens kappa ( )  . 
the mean heart frequency during the examination for the vari2 bpm ; ous study groups was as follows : group 1 53 4 bpm ; group group 2 64 13 years in 81 group 1 , 57 8 years in group 3 , 11 years in group 4 . 
groups 1 and 4 consisted of and 65 24 % female patients ( n 6 ) while group 2 included eight females ( 32 % ) and group 3 included five females ( 20 % )  . 
3 : p < 0.01 all others : n / s group 1 prospectively ecg - triggered high - pitch spiral acquisition group 2 prospectively ecg - triggered sequential mode group 3 retrospectively ecg - triggered spiral acquisition in dual - energy mode group 4 retrospectively ecg - triggered spiral acquisition in dual - source mode table 2 qualitative assessment of image quality and radiation dose of patients examined using different protocols for coronary dsct angiograparameter group 1 group 2 group 3 p value total no . 
in patients requiring functional analysis of the complete cardiac cycle , dual - energy spiral acquisition should be preferred over dual - source spiral mode to reduce radiation exposure . we focused on retrospectively comparing four available ccta protocols on a second - generation dsct in clinical routine . 
the combination with iterative reconstruction techniques for ccta has been demonstrated to allow for dose reduction down to 0.58 msv [ 20 ] or even below 0.1 msv [ 21 ]  . 
while these studies show that there is still potential for further dose savings , 1 3 radiol med ( 2015 ) 120 : 11121121 1117 the patient groups that these protocols can be applied to are limited and not representative for clinical routine . 
for patients with moderately higher heart rates up to 70 bpm or slight arrhythmia , the prospectively ecg - gated sequential acquisition mode is a useful alternative to high - pitch spiral acquisition as it also significantly reduces radiation exposure compared to retrospectively ecg - gated protocols . 
 figure 2 demonstrates a case examined with this protocol . retrospectively ecg - gated spiral acquisition protocols are still commonly used for ccta in clinical routine [ 8 , 9 ]  . 
the retrospectively ecg - gated dual - energy spiral mode allows for functional analysis of the left ventricle as well as the display of myocardial iodine distribution as a measure of myocardial perfusion and thus detection of myocardial ischemia [ 24 , 25 ]  . 
hence , this is our preferred examination mode in emergency room patients referred for evaluation of acute chest pafigure 3 demonstrates a case with acute occlusion of the left anterior descending artery and corresponding dual - energy perfusion images . 
however , dect requires a low and stable heart rate since the temporal resolution with 140 ms is significantly lower than with the dualsource mode ( 75 ms )  . 
axial arterial ( a ) and curved multiplanar reconstructions ( b ) ( aquarius intuition , terarecon , foster city , ca ) demonstrate a high - grade stenosis of the left anterior descending artery proximal to a large intravascular calcification ( big arrows )  . 
additional invasive coronary angiography confirmed both findings in this patient ( c ) with severe 3 - vessel coronary artery disease who later underwent coronary artery bypass grafting 1 3 1118 radiol med ( 2015 ) 120 : 11121121 fig . 
patient was clinically stable during preparation for ct imaging and showed a stable sinus rhythm of 69 bpm and was , therefore , examined using a retrospectively ecggated dual - energy protocol . 
axial images ( a ) demonstrate a complete occlusion of the left anterior descending artery ( big arrow ) and curved multiplanar reconstructions ( b ) ( aquarius intuition , terarecon , foster city , ca , usa ) furthermore depict multiple intracoronary calcifications . 
dual - energy perfusion images ( c ) reconstructed on a dedicated workstation ( heartpbv , siemens healthcare ) show a perfusion deficit ( big arrow ) in the corresponding vessel territory . 
the patient underwent invasive reperfusion and stenting in multiple coronaries due to severe 3 - vessel coronary artery disease in patients with heart rates above 70 bpm in whom functional analysis is required . 
figure 4 demonstrates a case in which retrospectively gated dsct spiral acquisition was selected due to atrial fibrillation and a coronary aneurysm was detected . as cardiac dsct can provide accurate and reproducible assessment of left and right ventricular function in comparison with magnetic resonance imaging [ 27 , 28 ] , retrospectively ecg - gated acquisition protocols for ccta are still commonly used to gain information of the full cardiac cycle although the resulting dose is higher compared to prospectively ecg - gated protocols . 
 [ 29 ] also highlighted the importance of assessing left ventricular function as it may improve the diagnostic accuracy for acute coronary syndrome in patients with acute chest pa takx et al . 
 [ 30 ] demonstrated that prospectively ecg - triggered cardiac dsct may permit accurate quantification of left and right ventricular function and reported a mean radi1.8 msv for this technique . 
 therefore , in our opinion , dual - energy ccta currently remains a reliable , dose - saving protocol which allows for retrospectively ecg - gated analysis of left and right ventricular function . the results of this study should be interpreted in the context of the study design and consequent limitations . 
as the patient had been diagnosed with chronic atrial fibrillation and presented with a heart rate of 96 bpm , a retrospectively ecg - synchronized dualsource acquisition technique was selected . 
images from curved multiplanar reconstructions ( b , c ) and virtual rendering techniques ( d ) ( both aquarius intuition , terarecon , foster city , ca , usa ) improve depiction of the aneurysm ( big arrows ) image quality for ccta using dsct [ 3 , 5 , 16 ]  . 
third , severity of cad was neither documented nor compared as it was not aim of this study and did not interfere with any measurement of objective image quality in this study determined by the observers . 
fourth , iterative reconstruction techniques were not used , as this was not goal of the study and differences between the various iterative reconstruction techniques may have compromised the comparability of image quality . 
however , prior studies have demonstrated that iterative reconstruction allows for noise reduction and hence improvement of image quality and potentially reduction of radiation dose [ 20 , 31 ]  . in conclusion , our results demonstrate that prospectively ecg - gated ccta protocols result in significantly less radiation dose exposure than retrospectively ecg - gated dsct protocols in a clinical routine setting . 
if data of the full cardiac cycle are required , e.g. , for functional analysis , the dual - energy spiral acquisition mode should be preferred in patients with low and regular heart rate over the dualsource mode as it results in significant dose reduction without compromising diagnostic image quality . conflict of interest ralf w . 
during the treatment , the aspiration catheter was placed from the right femoral vein to the ivc thrombi , and a 20 - ml syringe was connected with the aspiration catheter for thrombus aspiration . 
long - term ivc patency was achieved in 15 of 17 patients . conclusion combined thrombus aspiration and ivc recanalization can be a safe and effective method for bcs patients with ivc thrombosis . keywords buddchiari syndrome inferior vena cava thrombosis aspiration introduction buddchiari syndrome ( bcs ) is a rare disease involving hepatic venous outflow obstruction at the level of hepatic vein ( hv ) , inferior vena cava ( ivc ) , or both [ 14 ]  . 
standard ivc recanalization ( balloon dilation / stent insertion ) is considered to be a contraindication in these patients because of the risk of acute fatal pulmonary embolism ( pe ) [ 4 ]  . currently , combined catheter direct thrombolysis and ivc recanalization is widely used for bcs patients with ivc thrombosis [ 46 ] ; however , catheter direct thrombolysis requires a long treatment period and has the attendant risk of hemorrhage , especially for patients with upper gastrointestinal bleeding . 
the risk factors of bcs , including jak2 mutation , factor v leiden mutation , protein c deficiency , and protein s deficiency , were not present in any of these patients . 
patients liver function was evaluated by child - pugh grade ( a 4 , b 11 , c 2 )  . the diagnosis of bcs was established on patients history and results of abdominal ultrasonography and magnetic resonance imaging ( mri )  . 
the catheter was a commonly used 8f brite - tip guiding catheter ( cordis , hialeah , fl , usa )  . ivc thrombus aspiration all procedures were performed by three interventional radiologists with 3 , 8 , and 16 years of interventional procedures experience under fluoroscopic and local anesthesia . 
h abdominal doppler ultrasonography showed the patency of ivc at 3 months after treatment oxygen saturation were monitored throughout the entire procedure . thrombi visible on ivc venography ; and ( b ) persistence of not removable mural thrombi . an 8f catheter sheath was placed in the right femoral vein , and a 5f pigtail catheter ( cordis , hialeah , fl , usa ) was advanced into ivc for venography . 
the ivc thrombosis was confirmed by venography , and we rapidly injected 20 ml of physiologic saline and 100 , 000 unit of urokinase ( biochem , tianjin , china ) via the pigtail catheter into ivc to loosen the thrombi . the pigtail catheter was withdrawn , and the aspiration catheter was advanced to the level of thrombi . 
 the endpoint of thrombus aspiration was as follows : ( a ) no if the syringe was difficult to suction , it was suspected that the thrombi were at the tip of the catheter . 
in case of the thrombi persisting at the valve of the catheter sheath , we advanced a guide wire through the sheath into the femoral vein and retained the guide wire . 
then , the catheter sheath was advanced again to the femoral vein via the guide wire . ivc recanalization after thrombus aspiration , the right jugular vein was punctured and a 5f catheter sheath was placed . 
 because all patients had at least one patent hv or accessory hv , the patients did not undergo hv recanalization . after treatment , all patients received subcutaneous lowmolecular - weight heparin for 3 days , followed by warfarin sodium for 12 months . 
the international normalized ratio was maintained at 23 . definitions and end points technical success of combined thrombus aspiration and ivc recanalization was defined as elimination of the ivc obstruction and collateral circulation as determined by ivc venography without any major procedure - related complications . 
 patients underwent abdominal doppler ultrasonography and physical examination at 7 days , 1 month , 3 months , and every 6 months after treatment to confirm the long - term patency of the ivc . 
if patients felt chest congestion or in bcs - related manifestations after dyspnea , chest computed tomography ( ct ) was performed to confirm whether or not there was a pe . 
 all statistical calculations were performed using spss 16.0 ( spss , chicago , il , usa )  . results assessment of treatment combined thrombus aspiration and ivc recanalization was technically successful in all of the patients ( table 2 )  . 
two patients experienced the re - obstruction of ivc without thrombosis recurrence at 6 and 8 months after treatment , and were successfully treated with repeat ivc balloon dilation ( table 2 )  . 
all patients were alive at the time of this report . discussion this study evaluated the feasibility and effectiveness of combined thrombus aspiration and ivc recanalization in the management of bcs patients with ivc thrombosis . 
no patient experienced chest congestion or dyspnea after treatment and during the follow - up . in western countries , hv thrombosis continues to be most common in bcs patients [ 9 ] ; however , ivc obstruction is more common in asia [ 9 ]  . 
 [ 10 ] used catheter direct thrombolysis and oral warfarin to manage 132 and 16 bcs patients with ivc thrombosis before ivc recanalization , respectively ; complete resolution of thrombi was achieved in 90 and 88 % patients , respectively . 
although no patient experienced bleeding complications during the management of the thrombi in these two studies , the patients still had bcs - related symptoms during the management of the thrombi because the ivc could not be opened before effective management of the thrombi . ivc thrombi should be cleared rapidly , safely , and effectively in bcs patients . 
currently , the mechanical thrombus aspiration device ( aspirex ; straub medical , wangs , switzerland ) has been widely used in thrombus clearance instead of thrombolysis [ 11 , 12 ]  . 
this device consists of a high - speed rotating spiral located in the body of the device that creates negative pressure through an l - shaped aspiration system that can macerate and remove the thrombus [ 11 ] ; however , use of this device is very expensive . 
one lumen carries high - pressure saline that loops back through the distal end into the second lumen , creating a low - pressure vortex that macerates and aspirates the thrombus [ 13 ]  . 
 [ 14 ] also successfully used a 6f angiographic catheter ( imager ii ) to aspirate the thrombus for one patient with superior mesenteric vein thrombosis . in the current study , we used a normal 8f guiding catheter as the aspiration catheter to clear the ivc thrombi . 
although there were 5 patients who had the ivc mural thrombi which could not be aspirated , it was difficult to entirely dislodge the mural thrombus to drop off [ 9 ]  . 
long - term ivc patency following ivc recanalization after thrombus aspiration was 88 % , which is comparable to a previous study regarding ivc recanalization after catheter direct thrombolysis for bcs patients with ivc thrombosis [ 6 ]  . this study had some limitations . 
third , there was no control group in this study . in conclusion , although further clinical trials are needed , our results demonstrated that combined thrombus aspiration and ivc recanalization can be a safe and effective method for bcs patients with ivc thrombosis . 
the 8f guiding catheter can be a good choice as the aspiration catheter . 1 3 radiol med ( 2015 ) 120 : 10941099 1099 conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
citt della salute e della scienza , via genova 3 , 10126 turin , italy keywords hepatocellular carcinoma microwave ablation transarterial chemoembolization radiofrequency ablation combined therapy introduction in spite of many efforts and major advances in the treatment of hcc , this tumor is still the sixth most common cancer and the third cause of cancer - related death [ 1 ]  . 
 imaging - guided loco - regional therapies can be considered , in selected patients , the most appropriate and potentially curative treatments [ 2 ]  . among these therapies , radiofrequency ablation ( rfa ) is currently offered as a first line treatment in nodules less than 2 cm ( very - early stage , according to bclc classification ) , and in patients unfit for surgery , it is the best treatment option even for early stage patients ( single or up to 3 nodules 3 cm in diameter ) [ 2 , 3 ]  . an important limitation affecting rfa is its reliability in ablating all neoplastic tissue , creating an adequate ablation zone , with sufficient safety margins . 
in fact , when target tumors exceed 3 cm , rfa efficacy decreases : in such cases , the combination with tace can improve the maintained complete ablation , according to several previous retrospective studies [ 4 , 5 ] and one rct [ 6 ]  . more recently , microwave ablation ( mwa ) has been demonstrated as a potentially more powerful technique , emerging as a possible valuable alternative to rfa in case of larger hcc nodules . 
 written informed consent to undergo the procedure has been obtained by all the patients enrolled in the study . all examinations and treatments were performed in the full respect of the guidelines of our institutional review board and the helsinki declaration . patient selection data were retrieved from a consecutive database of 787 hcc image - guided ablation procedures performed at our department since january 2008 . 
a retrospective analysis was conducted on 36 patients with one or two hypervascular hcc nodules exceeding 3 cm , treated up to september 2013 . seventeen patients with 19 tumors were submitted to mwa ( group 1 , g1 )  . 
they were compared with our last group that had undergone rfa combined with tace selected on the basis of comparable characteristics ( 19 consecutive patients with 19 tumors ; group 2 , g2 )  . nodules mean diameter was 43 mm ( sd 7.5 ) in g1 and 45 mm ( sd 8.4 ) in g2 ; 11 nodules in g1 and 10 in g2 were larger than 4 cboth in g1 and g2 , 14 treated lesions were in the right lobe and 5 in the left lobe . 14 nodules in g1 and 5 in g2 were far less than 1 cm from the liver surface ; 14 and 8 lesions , respectively , were far less than 5 mm from main vessels . 
every 4 months , ablated nodules were then re - evaluated with cross - sectional imaging ( multiphase ct scan or dynamic gd - enhanced mr , preferably chosen in case of previous injection of iodized oil , unfavorable for ct evaluation )  . 
 all other complications were considered minor . statistical analysis the mannwhitney u test , chi squared test , and fisher exact test were used to analyze the differences in baseline fig . 
complete ablation ( ca ) of both nodules at the first ct control : arterial ( c ) , portal ( d ) and delayed phase ( e ) 1 3 1180 fig . 
 moreover , the correlation between adverse events and possible predictors ( tumor size , hepatic lobe , liver surface , and vessels distance ) was neither significant nor different in the two groups ( p ns )  . pad software ( la jolla , ca , usa )  . technique effectiveness and outcome results baseline characteristics table 1 shows the characteristics of the mwa group versus those of the rfa - tace group . 
also hepatic lobe and proximity to liver surface or vessels did not reach prognostic values for ca both in g1 and g2 . 1 3 radiol med ( 2015 ) 120 : 11771183 1181 fig . 
in fact , according to several studies [ 46 ] , tace prior to rfa reduces the cooling effect of hepatic blood flow on thermal coagulation by decreasing hepatic arterial flow , enhancing the nodule ablation . more recently , microwave ablation has emerged as a treatment with the potential to address the limitations of 1 3 1182 radiol med ( 2015 ) 120 : 11771183 rfa . 
this allows for a direct and potentially more homogeneous energy deployment , without the detrimental effects of tissue impedance , and can yield a more rapid and larger ablation [ 10 ]  . at our knowledge , there are no studies in the literature comparing combined rfa and tace versus mwa for hcc nodules larger than 30 mm . thus , this pilot study has been designed to compare the two methods in terms of safety and efficacy in a mid - term perspective ( one - year follow - up )  . safety as for safety , no major complications were counted ( 0 / 19 treated nodules ) and only 3 minor complications were observed in mwa group . 
this is consistent with the data reported in a joint study published by 14 institutions in which no deaths and an incidence of serious complications of 2.9 % were reported [ 11 ]  . 
even though no significant statistical differences were found between g1 and g2 for mca , mwa rate resulted still inferior than combined therapy and did not reach the percentages ( 67.5 % ) recently reported by liu et al . g1 results in nodules bigger than 4 cm still seem below expectations . g2 results in nodules up to 4 cm ( 67 % ) have been consistent with others already reported ( 70 % ) [ 6 ]  . 
moreover , despite a lower overall mca rate , also mwa mean diameter of mca subgroup resulted smaller than that of nodules with ltp , confirming the size of the tumor as the leading factor that affects local recurrence [ 15 ]  . 
studies with larger population groups , possibly randomized , will be eventually able to find out a statistically significant difference . in conclusion , according to our data , mwa seems to be so safe and effective to carve out a role in the treatment of hcc nodules between 3 and 4 cits standardization as a care for these tumors would be desirable , considering the longer hospital stay and the higher costs of the combined therapy . 
even though no statistically significant differences were found between the two treatments , due to the apparently noticeable difference in terms of local efficacy , a larger preferably randomized study should be designed to confirm mwa as a valid alternative to the combined therapy in case of hcc larger than 3 cm . conflict of interest all the authors declare no conflict of interest . ethical standards this is a retrospective study of prospectively collected data . 
all examinations and treatments were performed in the full respect of the guidelines of our institutional review board and the helsinki declaration . radiol med ( 2015 ) 120 : 1137 doi 10.1007 / s11547 - 015 - 0568 - 3 erratum erratum to : reliability of frontal sinus by cone beamcomputed tomography ( cbct ) for individual identification gianguido cossellu1 stefano de luca2 , 5 roberto biagi1 giampietro farronato1 mariano cingolani3 luigi ferrante4 roberto cameriere2 published online : 18 july 2015 italian society of medical radiology 2015 erratum to : radiol med doi 10.1007 / s115470150552y in the original publication , except the second authors name , the first and last names of all the authors were interchanged . 
 among them , 17 patients with segmental obstruction ( obstruction length > 1 cm ) of hv experienced failure of the routine transjugular hv recanalization and underwent retrograde puncture assisted hv recanalization . 
data on technical success , clinical success and follow - up were collected and analyzed retrospectively . results retrograde puncture assisted hv recanalization was technically successful in 14 of 17 ( 82 % ) patients . 
it can serve as an additional treatment option for patients who experience the technical failure of routine transjugular hv recanalization . keywords retrograde puncture hepatic vein buddchiari syndrome introduction buddchiari syndrome ( bcs ) is a rare disease characterized by hepatic venous outflow obstruction [ 13 ]  . 
however , transjugular hv recanalization may be difficult with a high failure rate ( 31 % ) in some bcs patients due to the segment obstruction of the hv [ 4 ]  . to overcome these problems , we used the retrograde puncture skill in hv recanalization . 
during this procedure , we directly punctured the hv and built a track of guide wire as external - target hv - inferior vena cava ( ivc ) superior vena cava ( svc ) - right jugular vein - external , after which the hv recanalization was performed via this guide wire . 
in this study , we reported our clinical results of retrograde puncture assisted hv recanalization for bcs patients with segmental obstruction of hv who experienced technical failure of routine transjugular hv recanalization . 1 3 radiol med ( 2015 ) 120 : 11841189 materials and methods patients selection this study was approved by our institutional review board . 
baseline data ( age , gender , history , clinical presentation , imaging findings , and liver function ) of these patients were collected . diagnosis and definition diagnosis of bcs was established by reviewing patients history , as well as the results of abdominal ultrasound and magnetic resonance angiography ( mra ) / computed tomography angiography ( cta ) findings . bcs with obstruction of hv is defined as the obstruction of three hvs [ 4 ]  . 
 segmental obstruction of hv was defined as an obstruction length > 1 cm , and membranous obstruction of hv was defined as an obstruction length 1 cm [ 4 ]  . 
symptomatic bcs is defined if a bcs patient has any one of of the following clinical manifestations : abdominal pain , abdominal distention , jaundice , ascites , variceal bleeding , or encephalopathy [ 3 ]  . puncture of hv all procedures were performed by three interventional radiologists . 
blood pressure , heart rate , arterial oxygen saturation , and respiration rate were monitored throughout the treatment . all enrolled patients underwent retrograde puncture assisted hv recanalization immediately after the failure of routine transjugular hv recanalization . 
the puncture point was chosen at the space under the xiphoid if the left or middle hv was the target ve afterwards , 5 ml 2 % lidocaine was administered at the puncture point , and a 21g chiba needle ( cook , bloomington , indiana , usa ) was punctured into the target hv . guide wire transfixion guide wire transfixion was performed under the fluoroscopic guidance . 
1b , hv recanalization when the stiff guide wire was established , a 1215 mm diameter balloon catheter ( cook , bloomington , indiana , usa ) was sent from the jugular puncture site to the obstructed site via the guide wire . 
if there was more than 30 % residual stenosis on hv venography after balloon dilation , a 1416 mm diameter stent ( bard , karlsruhe , germany ) was inserted [ 5 ]  . 
 ( d , e ) the venography revealed the patency of the right hv after balloon dilation clinical assessment technical success was defined as elimination of hv obstruction as determined by venography , along with the disappearance of the intrahepatic collateral circulations . 
the liver function test was performed before and 7 days after treatment . all patients were followed by abdominal ultrasound 7 days , 1 , 3 , 6 months , and then annually after treatment to confirm the long - term patency of hv . 
follow - up ended at the time of setting this study ( december 2014 ) , patients death , or the date if the patient underwent transjugular intrahepatic portosystemic shunt ( tips ) insertion , surgical shunt , or liver transplantation . statistical analysis variables were using continuous standard deviation . 
 in these 14 patients , risk factors of bcs , including jak2 mutation , factor v leiden mutation , protein c deficiency , and protein s deficiency , were not found in any of these patients . 
there was no evidence of hv re - obstruction in the remaining 11 patients . discussion this study evaluates the feasibility and effectiveness of retrograde puncture assisted hv recanalization for bcs patients . 
during the followup , the long - term patency of hv was achieved in 11 of 14 ( 79 % ) patients . the purpose of hv recanalization is relieving the hepatic congestion and improving patients symptoms [ 46 ]  . 
currently , hv recanalization is usually performed via the transjugular approach , because ( a ) puncture of jugular vein can be easily performed , and ( b ) the angle between hv and proximal ivc is usually relative large , and it is easy to send the guide wire into the hv [ 46 ]  . however , transjugular hv recanalization is usually hard for bcs patients with segmental obstruction . 
first , during the procedure of transjugular hv recanalization , we should hold the proximal tip of the guide wire to make the distal tip of the guide wire pass through the obstructed site . 
 second , even though the guide wire sometimes passes through the obstructed site , when we send the balloon catheter , the guide wire can only be fixed at the proximal side . 
 therefore , it cannot provide enough holding power to make the balloon catheter pass through a segmental obstruction [ 7 ]  . tips insertion has been widely used for bcs patients who fail to undergo hv recanalization [ 8 , 9 ]  . 
although tips can effectively decrease the portal vein pressure and significantly improve the patient symptoms , hepatic encephalopathy occurs in 1735 % patients undergoing tips insertion [ 9 , 10 ]  . 1 3 radiol med ( 2015 ) 120 : 11841189 1189 the relative high technical success rate ( 82 % ) of retrograde puncture assisted hv recanalization in this study may be attributed to the following factors : ( a ) the puncture of hv was managed under the guidance of ultrasound and ( b ) the hepatic puncture site was near the hv obstruction and we could hold the front part of the guide wire to control the distal tip of the guide wire . 
third , retrograde puncture assisted hv recanalization cannot be used in bcs patients with total obstruction of three hvs . although further clinical trails are needed , we can believe that the retrograde puncture assisted hv recanalization is a simple , safe , and effective treatment for bcs patients due to segmental obstruction of hv . 
it can serve as an additional treatment option for patients who experience the technical failure of routine transjugular hv recanalization . conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
it is a useful method , particularly if fat deposition is heterogeneous , and should be considered as a new reference standard . keywords fat quantification proton density fat fraction hepatic steatosis mr spectroscopy introduction hepatic steatosis is a condition in which large vacuoles of triglyceride fat accumulate in liver cells . 
nafld is the most common cause of chronic liver disease in western societies and is closely associated with the metabolic syndrome , a constellation of diseases including type 2 diabetes mellitus , hypertension , obesity , and dyslipidemia . 
because the earliest and most reliable feature of nafld is steatosis , early and accurate diagnosis is important so that proper management may be used to prevent long - term complications [ 1014 ]  . currently , core liver biopsy is considered the reference standard for diagnosing and grading steatosis . 
due to the fact that hepatic steatosis is often heterogeneous , quantifying liver fat using a core biopsy may lead to sampling bias and thus underestimation or overestimation of steatosis [ 1517 ]  . 
therefore , a noninvasive , objective , quantitative diagnostic alternative to the core liver biopsy is needed for more accurate whole - liver diagnosis of steatosis . magnetic resonance ( mr ) techniques , such as mr spectroscopy ( mrs ) , the dixon method , and imaging with and without fat saturation , have been used for detection and quantification of steatosis [ 18 , 19 ]  . 
among such techniques , mrs is regarded as the most accurate method for the assessment of hepatic triglyceride content and uses 5.56 % as the diagnostic threshold for steatosis [ 20 ]  . 
when performed correctly , mrs measures the hepatic proton density fat fraction ( pdff ) , which is platform and protocol independent , and can be used as a measurement of liver fat content . 
also , sampling bias , when working with small sample volumes , has been reported because only one voxel - of - interest ( voi ) is usually measured [ 2022 ]  . mr imaging - based proton density fat fraction ( mripdff ) calculation is a recently described chemical shiftbased technique that uses either magnitude or complexbased algorithms to separate water and fat . 
this method also corrects for factors that confound the mr signal , such as t1 bias , t2 * decay , spectral complexity of fat , eddy currents , and noise bias [ 2326 ]  . 
additionally , recent studies have shown that mri - pdff correlates well with liver biopsy results , as well as in phantom and in vivo patient studies [ 2833 ]  . 
however , previous studies estimated mri - pdff from a relatively small area using a round or elliptical region - of - interest ( roi ) measurement that has the potential to affect the accuracy of the overall hepatic fat measurements because hepatic steatosis is often unevenly distributed throughout the liver [ 34 , 35 ]  . 
 thus , the aim of this study was to evaluate the diagnostic performance of mri - pdff with variable roi measurement , including free - drawn roi measurement to quantify hepatic fat over nearly the entire liver using mrs as the reference standard . materials and methods study population this is a retrospective , single - center study that was approved by the institutional review board of our hospital and informed consent was obtained . 
patients were excluded if : ( a ) a severe mr artifact was present ( n 10 ) , ( b ) parenchyma was replaced by large space - occupying lesions ( > 5 cm or infiltrative lesions ) ( n 31 ) , or ( c ) the mrs voxel was inappropriately placed during the procedure ( n 2 )  . 
to estimate mri - pdff , an investigational variant of hybrid multi - step adaptive fitting approach with multi - echo volume interpolated breath - hold examination ( vibe ) acquisition was used , which combines the strengths of both magnitude and complex - based methods and provides liver pdff and r2 * maps for hepatic iron quantification [ 26 , 31 ]  . 
the parameters of this sequence were as follows : repetition time 1.23 ms with ( tr ) 6 echoes collected with te 5 ; 32 cm ; slice thickness 256 matrix 1 ; bandwidth 1090 hz / pixel ; bipolar readout . 
a parallel acceleration technique ( controlled aliasing in parallel imaging results in higher acceleration , caipirinha ) was used , with acceleration factors of 2 in both phase encoding and partition directions [ 26 , 31 ]  . 
the images were processed using online software to create water / fat images , water / fat r2 * maps , an effective r2 * map , and water / fat percentage maps . 42 165 ; number of signals acquired 9.2 ms ( ms ) ; first echo time ( te ) 1.23 ms ; flip angle 4 mm ; field of view single - voxel high - speed t2 - corrected multiple - echo 1h - mr spectroscopy ( svs ) [ 36 ] was performed , which is a single - voxel stimulated echo acquisition mode ( steam ) 1 3 radiol med ( 2015 ) 120 : 10831093 1085 30 10 ms ; tr 3000 ms ; te 1200 hz ; sampling points spectroscopy sequence with five different tes to serve as the reference standard . 
the parameters included mixing 12 , 24 , 36 , 48 , time ( tm ) and 72 ms ; bandwidth 1024 ; voxel size of 30 30 mm , and total acquisition 15 s . 
the voxel was placed in the posterior segment time of the right hepatic lobe ( segment vi or vii ) , taking care to avoid major blood vessels , bile ducts , or any space - occupying abnormalities and was shimmed automatically . 
the fat and water peaks retrieved from the spectroscopy data were detected automatically , fat and water values were integrated over each peak , and then the different te values were fitted to an exponential . 
the fat percentage was calculated from 0 and the the fat and water values extrapolated to te result was reported as a dicom text report . image processing all roi measurements were performed by one radiologist with 3 years of clinical experience reading liver mris . 
these rois were copied to the fat percentage map using the copy and paste function of the pacs system ( maroview 5.4 ; marotech , seoul , korea )  . 
a weighted average using the roi size was calculated such that an average fat fraction across the liver was reported . statistical analysis all statistical analyses were performed using spss software , version 20.0 ( ibm corp , armonk , ny , usa )  . 
all results are expressed as a mean standard deviation ( sd )  . all patients were dichotomized into either the steatotic or the non - steatotic group based on whether they were above or below the svs - determined fat percentage of 5.56 % [ 20 ]  . 
an independent t test was used to compare liver fat content between two lobes of liver for each mri - pdff method ( voi - pdff , segmental - pdff , freedrawn - pdff , and free - drawn - pdff - 2 ) as well as svs . 
blandaltman analysis was performed to estimate the agreement between each of the pdff methods . the liver fat content difference between the right and the left lobe was compared using free - drawn - pdff - 2 with an independent t test . 
to test segmental heterogeneity , repeated anova with one repeated factor was also used to compare the fat content of seven segments using segmental - pdff . diagnostic performance of each method was compared using mcnemars test . 
a p value of less than 0.05 was considered to be a statistically significant difference . results liver fat content the mean fat percentage of each method in all patients , the steatotic group , the non - steatotic group , and separately in each liver lobe were estimated ( table 1 )  . 
1 a 66 - year - old male with 6.17 % fat fraction ( ff ) in svs : three square - shaped rois from three contiguous slices were placed on the same location of a single - voxel of interest ( voi ) used in svs . 
the elliptical region - of - interest ( roi ) was placed on the fat percentage map at seven couinaud segment locations from ii to viii ( segmental - pdff )  . 
three free - drawn rois were made using a tablet pen along the liver margthe mean ff value of the three free - drawn rois ( 5.4 % ) was defined as free - drawn - pdff ( eg )  . 
the mean ff values of the six free - drawn rois of both lobes ( three each for right and left lobe ) were defined as free - drawn - pdff - 2 ( h , i ) blandaltman plots between voi - pdff and segmentalpdff , voi - pdff and free - drawn - pdff , free - drawn - pdff and segmental - pdff , and free - drawn - pdff and freedrawn - pdff - 2 . 
the maximum difference between 1 3 1088 radiol med ( 2015 ) 120 : 10831093 using svs as a reference , the area under the roc curve ( auroc ) was calculated for mri - pdff methods . 
it is similar to the iterative decomposition of water and fat with echo asymmetry and least squares estimation ( ideal ) , which has been used for hepatic fat quantification and has shown good histologic correlation [ 28 , 30 ]  . 
 our mri - pdff is different from ideal in that it uses both magnitude and complex data calculations , combining the strength of both methods , in which the insensitivity to phase errors / eddy current effects inherent to magnitudebased methods and the broader dynamic range of complex - based methods [ 31 ]  . 
many other factors , such as t2 * decay , t1 bias , and multi - peak fat modeling , are also taken into account in this method for accurate fat quantification . 
finally , separate measurements of water and fat r2 * are obtained , which may also be informative . in this study , we found the best correlation to be between the svs and the voi - pdff methods . 
 considering there have been no previous in vivo studies on multi - echo vibe acquisition with adaptive fitting with a large patient cohort , we showed that this technique enables accurate hepatic fat quantification . recent studies showed that pdff was well correlated with histological methods , but there were some important differences in agreement . 
one of the reasons for the low accuracy of agreement is that , when using the pdff method , one estimates the proportion of mobile protons contained within fat molecules in a three - dimensional liver fig . 
using voi - pdff with the same cut - off value as with svs ( 5.56 % ) , 51 patients ( 32.7 % ) were classified as having hepatic steatosis . 
when using segmental - pdff for diagnosing hepatic steatosis , 44 patients ( 28.2 % ) were diagnosed , and sensitivity and specificity were calculated as 81.5 and 100 % , respectively . 
using free - drawn - pdff with the same cut - off value , 46 patients ( 29.5 % ) were classified as having hepatic steatosis , and a sensitivity and specificity of 85.2 and 100 % were calculated . 
using the free - drawn - pdff - 2 technique , 46 patients ( 29.5 % ) were diagnosed , and a sensitivity and specificity of 85.2 and 100 % were calculated . 
another reason for the agreement difference is the possibility for liver fat content to change over time , which may be due to the time interval that passes between liver biopsy and pdff analysis . 
interobserver and intraobserver variability is another well - known limitation of histological assessment [ 17 , 37 , 38 ]  . additionally , the heterogeneity of fat deposition in the liver could simultaneously affect mr fat quantification and biopsy results . 
 [ 34 ] also found that steatosis is usually greater in the right lobe than the left lobe ; they further found that heterogeneous fat deposition can sometimes lead to a misdiagnosis of hepatic steatosis . 
in support of this theory , they cited that portal blood flow , which is conveyed via the superior mesenteric vein , contains dietary fat and flows mainly into the right liver and blood from the splenic vein flows mainly into the left liver [ 39 ]  . 
 [ 34 ] cited a need for methods that quantify steatosis over a larger region . 1 3 1090 radiol med ( 2015 ) 120 : 10831093 area estimation such as free - drawn - pdff and free - drawnpdff - 2 had relatively lower agreements to the voi - pdff . 
 although there is a lack of statistical evidence to prove that free - drawn - pdff is superior to the conventional reference standard , we speculate that mrs has a relatively low agreement and the difference in diagnostic performance is due to the large - area coverage as a means of whole liver fat quantification that is achievable with free - drawn - pdff . 
therefore , this technique could be regarded as a new method to accurately measure liver fat content . with an emphasis on the cut - off value for discriminating the grade of steatosis , three recent studies comparing core needle biopsy or 1 - cm3 - sized surgical specimen results and mri - pdff with a mean fat percentage of eight to nine couinaud segments had different cut - off values compared with previous studies [ 28 , 30 , 40 ]  . 
 [ 30 ] showed that the sensitivity and specificity was 93 and 85 % with an mri - pdff measured cut - off value of 15.03 % to differentiate moderate or severe steatosis from mild or no steatosis . 
another study with living liver donors showed that an mri - pdff determined cut - off value of 5 % resulted in 100 % sensitivity and 91 % specificity for detecting more than 5 % steatosis [ 40 ]  . 
discrepancy of these cut - off values may be due to various reasons , as previously mentioned , however , the small sampling size of liver biopsy compared to multiple roi measurements using mri - pdff is likely a key aspect . 
 therefore , hepatic fat heterogeneity could be considered in novel standards for pdff and our method will be particularly useful to establish new reference values . our study has several limitations . 
first , it was a retrospective study and our study population had a limited number of patients with alcoholic liver disease and homogeneous fatty liver , which may have biased our results . 
4 waterfall plot highlighting between the right and left liver lobe the differences in steatosis the findings of our study were similar to those cited above regarding heterogeneity of liver fat content . 
since the right lobe had a relatively higher fat content as compared to the left lobe , svs results may have had a tendency to overestimate the fat content of the liver , particularly if the difference between the two lobes was large . 
there were five discrepant cases in our study in which the fat content of one side of the liver was high enough to qualify as steatotic while the other side did not meet such criteria . 
5 an 18 - year - old female with hepatic steatosis : in - phase ( a ) , opposed - phase ( b ) and pdff fat percentage map ( c ) show uneven fatty distribution . 
a free - drawn region - of - interest ( roi ) was placed at the umbilical portion of the left portal vein as representative image of free - drawn - pdff ( d ) , the free - drawn roi of the right lobe ( e ) , and the free - drawn roi of the left lobe ( f ) were placed at the same level as representative images of free - drawn - pdff - 2 . 
however , based on previous studies regarding the accuracy of mrs , we first compared voi - pdff and mrs to show that our pdff method is accurate and feasible for estimating a wide range of fat percentages . 
fourth , as mentioned above , because there is not yet a clear cut - off value for diagnosing steatosis via pdff , we adopted 5.56 % as the cut - off value . 
there have been no studies focusing on the mri - pdff - determined cut - off value and therefore a large , prospective study with healthy subjects without a history of liver disease or risk factors for hepatic steatosis is needed . 
we assume that after further studies , the cut - off value may shift from the 5.56 % mrs - determined value used in this study [ 20 ]  . in conclusion , free - drawn - pdff measurements provide fast , accurate , and more generalized information regarding hepatic fat deposition ; this is particularly true if fat deposition is heterogeneous . 
corresponding 3d volumes were generated and maximal dimensions along 3 directions ( x , y , z ) , xm , ym , zm ( in mm ) , total volume area ( in mm3 ) , vt , and total surface ( in mm2 ) , st , were calculated . 
it has proven particularly useful when antemortem ( am ) dental records are not available , when teeth are missing postmortem ( pm ) , or in cases in which soft tissues are decomposed or burned [ 79 ]  . some typical features of frontal sinus morphology make it a very reliable part of the human skeleton for human identification [ 10 ]  . 
 lastly , it is highly variable in nature and shows differences even between monozygotic twins [ 16 ] , as demonstrated by several radiographs , among which researchers could not find two identical ones [ 19 , 20 ]  . am and pm radiographs of the frontal sinuses can be compared by overlapping or coding systems [ 18 , 21 ]  . 
overlapping is accepted as a reliable method but it does cause some problems which are overcome by coding systems [ 2225 ]  . in spite of the large number of publications relating to the uniqueness of frontal sinuses , there is a real need for more research aimed at quantification [ 25 ]  . 
as christensen 1 3 radiol med ( 2015 ) 120 : 11301136 1131 stated [ 20 , 25 ] , although many claim that the frontal sinuses are unique to each individual , no empirical studies have ever rigorously tested this statement . some recent publications have stressed the possibility of studying frontal sinuses by computed tomography ( ct ) [ 2629 ]  . 
they also present several advantages over conventional radiographs : superimposition of structures beyond the plane of interest can be avoided , allowing visualization of small differences in density [ 26 , 27 , 29 ] ; internal points for evaluation can be easily shown by image segmentation ; craniometric points can be precisely located and measurements more accurately performed than on conventional radiographs . 
hence , volumes and areas can be determined [ 27 , 28 , 31 ]  . cone beam - computed tomography ( cbct ) has recently begun to emerge as a potentially low - dose cross - sectional technique for visualizing bony structures in the head and neck [ 26 , 30 ]  . 
the software can then apply a particular algorithm to reconstruct the images into a threedimensional ( 3d ) dataset [ 32 ]  . comparatively low dosing requirements , high - quality bony definition and the compact design afforded by cbct scanners have made them attractive for office - based and intra - operative scanning of frontal sinuses [ 32 ]  . 
the machine can be transported and easily positioned in place like a cart , allowing its use on virtually any levelled temporary facility [ 33 ]  . in this context , the most commonly used techniques are based on evaluation of both metric and non - metric characteristics of frontal sinus patterns . 
 [ 19 ] proposed a system of classification based on the following morphological characteristics : area size , bilateral asymmetry , superiority of area size , outline of superior borders , partial septa and supra - orbital cells were collected and classified with code numbers . 
the authors state that the possibility of having the same code for two different individuals is one every 23 , 040 cases . in 2005 , to improve the performance of the above method for individual identification , cameriere et al . 
 [ 34 ] proposed a new system of classification based on the following morphological characteristics : ratio between left frontal sinus area and left orbital area ( sor1 ) and ratio between right frontal sinus area and right orbital area ( sor2 ) , instead of the area size and bilateral asymmetry of yoshinos method . 
reconstruction of the coronal ( xz ) , sagittal ( yz ) and transversal ( xy ) planes were analysed . according to the minimal and maximal threshold values , one layer of the relevant structures ( airways ) was called the mask , and was defined and colour - coded . 
 because of the connection of the air to the surroundings , pixel need to be erased with mask editing so the field of view can be excluded from the surroundings . 
the contour interpolation algorithm is used to visualize the 3d model of the frontal sinus and the grey 1 3 1132 radiol med ( 2015 ) 120 : 11301136 fig . 
the world medical association ( wma ) developed the declaration of helsinki as a statement of ethical principles for medical research involving human subjects , including research on identifiable human material and data . to test intra - observer reliability , a random sample of 30 cbct scans were each re - examined twice , at two - week intervals . 
assessment of inter - observer reliability was carried out by two observers , each of whom evaluated 30 randomly selected cbct scans . randomly selected means that each scan among the analysed cbct has an equal and independent chance of being selected to belong to the sample of 30 cbct scans used to test reliability of the method . 
effectively , the function sample of the statistical environment r has been used to take a sample of 30 scans from 150 numbered cbct . intraand inter - observer reliability was studied with the intra - class correlation coefficient ( icc ) [ 35 , 36 ]  . statistical analysis in this preliminary study , only the quantitative variables characterizing 3d frontal sinus patterns were analysed . 
those with correlation coefficient r such that |r| < 0.9. six quantitative variables ( parameters ) measured have been taken for each skull : maximal dimensions of sinuses along 3 directions ( x , y , z ) , xm , ym , zm ( in mm ) , total volume area ( in mm3 ) , vt , and total surface ( in mm2 ) , st , of the whole structure of the frontal sinuses . 
 this means that the second subject is different from the first one , with a probability 5 % of erroneously rejecting the hypothesis that the two scans belong to the same subject . 
 consequently , st was excluded from the variables used in the identification procedure , because it carried a very small amount of information with respect to that obtained from the other four variables . 
the choice to include vt and to remove st is related to the variability among subjects of vt which is greater than the variability of st . once the variables considered for individual identification by frontal sinus had been selected , the re - examined cbct scans were used to assess the intra - observer variability of the chosen statistical variables . 
within - subject variability was characterized by assuming that it was only due to errors on repeated measurements of the same scan , and that these errors were normally distributed . the tolerance region at level 1 for each individual was then evaluated . 
this region consists of measurement vectors x satisfying : ( cid : 31 ) ( x ) ( x ) 2 k ( 1 ) where x is a k - dimensional vector of measurements of a 3d frontal sinus pattern chosen for identification , is the known k - dimensional vector of measurements of a 3d frontal sinus pattern in the given individual and is the estimated covariance matrix associated with within - subject variability due to inter - observer error measurement . 
lastly , k ( 1 ) indicates the quantile function for probability of the chi squared distribution , with k degrees of freedothat is , if a k - dimensional vector of measurement of a 3d frontal sinus pattern , x , is located out of the region of tolerance with centre , it does not refer to the same ( cid : 31 ) 1 3 1134 radiol med ( 2015 ) 120 : 11301136 far more information . 
in the last few years , self - shielded cbct machines have also reduced radiation , compared with multi - slice ct ( msct ) scanning and conventional radiography ; its relative low cost make acquisition more feasible ; it can be also used in a wider range of subjects , and easily transported and operated for either office or mobile morgues [ 37 , 38 ]  . 
lastly , the cbct machines are user - friendly and limited training is necessary to use thealthough cbct has not yet gained wide acceptance in forensic community , sarment and christensen encourage its use for many forensic applications [ 33 ]  . in this study , frontal sinuses were separate in 21 subjects ( 14 % ) , fused in 67 ( 44.6 % ) and found on only one side ( unilateral ) in 9 ( 6 % total , 2.6 % in females and 3.4 % in males )  . 
 the frequency of frontal sinus agenesis is variable between different populations [ 40 ]  . the term fused sinus is used here to describe adjoining of the right and left sinuses [ 19 ]  . 
the high agreement renders frontal sinus identification system to be a simple method for establishing the identification of unknown persons for whom frontal sinus x - rays exist . of the variables considered for identification purposes , total surface ( st ) was not used in this study because it is highly correlated with volume ( r 0.976 ) and therefore does not increase the quantity of identifying information . each cbct scan corresponds to a point , p , in the four - dimensional space identified by xm , ym , zm and vt . 
 compared with traditional 2d techniques , 3d images yield 1 3 radiol med ( 2015 ) 120 : 11301136 1135 measured distances are quantitative characteristics and may vary , depending on manual reconstruction of the images , so it was concluded that one and the same skull always show an identical value for a certain measured parameter . 
conversely , a point which does not belong to this region represents a different subject , with a small fixed probability , , of yielding a false - negative error . as regards the probability of obtaining a positive identification error , i.e. 
two different subjects belong to the same tolerance region , none of the 150 individuals in this sample fell in the tolerance region of another individual . conclusions the technique described in this study could increase the usefulness of the frontal sinus identification method in new forms of 3d examinations such as cbct . 
forensic researchers are expected to achieve more numerous identifications in the future by applying cbct scanning . acknowledgments the authors would like to thank the staff of the unit of orthodontics and pediatric dentistry , university of milan ( italy ) for their assistance on this project , and also gabriel walton for editing the english text . 
krestin3 roberto lagalla1 roberto pozzi mucelli2 filippo cademartiri3 , 4 massimo midiri1 received : 25 january 2015 / accepted : 30 april 2015 / published online : 16 may 2015 italian society of medical radiology 2015 abstract purpose the aim of the study was to evaluate the prevalence of collateral findings detected in computed tomography coronary angiography ( ctca ) in a multi - center registry . materials and methods we performed a retrospective review of 4303 patients ( 2719 males , mean age 10.2 years ) undergoing 64 - slice ctca for sus60.3 pected or known coronary artery disease ( cad ) at various academic institutions between 01 / 2006 and 09 / 2010 . 
collateral findings were recorded and scored as : non - significant ( no signs of relevant pathology , not necessary to be reported ) , significant ( clear signs of pathology , mandatory to be reported ) , or major ( remarkable pathology , mandatory to be reported and further investigated )  . results we detected 6886 non - cardiac findings ( 1.6 non cardiac finding per patient )  . 
overall , 2095 ( 30.4 % ) non - significant , 4486 ( 65.2 % ) significant , and 305 ( 4.4 % ) major findings * ludovico la grutta ludovicolagrutta@hotmail.it 1 department of radiology , dibimed , university of palermo , via del vespro 127 , 90100 palermo , italy 2 department of radiology , university of verona , verona , italy 3 department of radiology , erasmus medical center , rotterdam , the netherlands 4 department of radiology , azienda ospedalierouniversitaria , parma , italy 5 cardio - vascular imaging unit , giovanni xxiii hospital , monastier di treviso , italy 6 department of radiology and cardiology , azienda asl , carrara , italy were detected . 
in every center , most prevalent significant findings were mediastinal lymph nodes > 1 c in 256 patients , collateral findings were clinically more relevant than coexisting cad and justified the symptoms of patients . conclusions the prevalence of significant and major collateral findings in ctca is high . 
radiologists should carefully evaluate the entire scan volume in each patient . keywords computed tomography coronary angiography collateral findings coronary artery disease non - cardiac findings introduction non - invasive imaging of the coronary arteries represents an important clinical application since ct coronary angiography ( ctca ) has proven to be an accurate imaging method alternative to conventional coronary angiography [ 13 ]  . 
ctca may be employed in patients with low - tointermediate pre - test probability of coronary artery disease ( cad ) and negative or equivocal findings on exercise stress testing [ 410 ]  . the increasing demand of non - invasive imaging of the coronary arteries has determined the emerging issue of non - cardiac collateral findings in ctca [ 1116 ]  . 
in most of the cases such findings are incidental and without any significance , but in other cases they are significant or even responsible of major pathology to be further investigated . 
 previous papers have addressed this issue but only on a single center level with a limited number of patients [ 1116 ]  . the aim of our study was to assess the prevalence of non - cardiac collateral findings at ctca in a multi - center registry . 1 3 radiol med ( 2015 ) 120 : 11221129 1123 materials and methods ctca protocol patient population this is a retrospective review of ctca examinations performed for clinical reasons at various academic institutions applying comparable scan and image analysis protocols ( table 1 )  . all examinations were performed with 64 - slice ct scanners ( sensation 64 cardiac , siemens , forcheim , germany in centers 1 and 2 ; vct , gehc , milwaukee , usa in center 1 ; brilliance 64 , philips , best , the netherlands in centers 3 and 4 )  . 
institutional review board approval was not required since retrospective data of standard cardiac ct examinations were used . inclusion and exclusion criteria all centers applied the same inclusion and exclusion criteria . 
eighty to 100 ml of non - ionic iodinated contrast material ( iomeprol 400 mgl / ml , iomeron , bracco , milan , italy ; iodixanol 320 mgi / ml , visipaque , gehc , usa ) were intravenously administered at a flow rate of 5 ml / s , followed by 40 ml of saline solution at the same rate . 
contrast material was administered in all centers with a dual - syringe automatic injector ( stellant , medrad , pittsburgh , usa ) connected to an 18g cannula placed in a right arm antecubital vethe synchronization of the scan with the passage of contrast material was performed with the bolus - tracking technique . the image datasets were reconstructed during the mid - to - end diastolic phase , with reconstruction windows set at 6080 % of the rr interval . 
when mildly irregular heart rates were encountered , such as bundle branch blocks or premature beats , the temporal variability in the reconstruction phase was compensated manually with ecg editing . 
in all centers an image dataset with a large field of view ( including the entire thorax ) was always reconstructed in each patient with the following parameters : slice thickness 1 mm , increment 0.6 mm , convolution filters medium - soft and sharp . image evaluation and followup of findings the radiologists of every center participating to the study had a consensus meeting before the start - up of the review and decided the classification of findings . all scans were reviewed in each center by two radiologists unaware of ct official report and with at least 6 year of training in cardiac and chest ct . 
additional multiplanar reconstructions with different slice thicknesses were performed to assess non - cardiac findings . radiologists set the classification after acknowledgement of the existing literature [ 1215 ] and arrangement of a specific scoring method aiming at clinical relevance of findings . 
 in case of significant or major findings medical records of patients were reviewed in every center to check clinical follow - up , subsequent examinations ( i.e. , laboratory tests or imaging studies such as chest or column x - ray , ct of the neck , thorax or abdomen , and abdominal us ) or surgical procedures in the 12 months after ctca . statistical analysis findings are expressed in terms of absolute values and percentages . 
2 collateral findings : liver cyst ( arrow ) as an example of nonsignificant finding ( a ) ; liver haemangioma ( thin arrow ) as an example of major finding , and hiatal hernia ( thick arrow ) as an example of significant finding in the same patient ( b ) ; vertebral haemangioma ( arrow ) as an example of significant finding ( c ) fig . 
3 examples of collateral findings in the thorax : a bilateral pulmonary embolism ( arrows ) as an example of major finding ( a ) ; pulmonary emphysema as an example of significant finding ( b ) fig . 
most prevalent major findings were as follows : pulmonary nodules > 1 cm in 35.1 % ( n 15 ) in center 2 , lung infections in 37 % ( n 10 ) in center 3 , and hepatic haemangioma in 24.2 % ( n 16 ) in center 4 . 
they reported 38 % of noncoronary findings as located in the heart or pericardiu moreover , they included a large number of minor , relatively insignificant abnormalities , such as scars , granulomata , atelectasis , degenerative arthritis , and rib fractures . 
the higher prevalence of findings was mainly due to a systematic and accurate analysis of each finding which can be present in the chest ; only 211 ( 41.9 % ) patients in their series were completely free of any additional finding . 
the result deriving from 1 3 radiol med ( 2015 ) 120 : 11221129 1127 1 3 1128 radiol med ( 2015 ) 120 : 11221129 a multi - center registry amplifies the need of a thorough review of image datasets by radiologists . 
 furthermore , non - cardiac findings , such as pulmonary embolism and aortic dissection , may be incidentally displayed in the clinical setting of non - cardiac chest pain [ 8 , 17 ]  . 
the first center had the lowest prevalence of major findings ( 3 % ) , although the population was the largest ; this aspect accounts for the high variability of findings in different populations and may reflect the different attention of radiologists to deal with non - cardiac findings in ctca . 
a recent metanalysis found that extracardiac malignancies occur in 0.7 percent of patients who underwent cardiac ct , and more than 70 % of previously unknown malignancies were lung cancers [ 18 ]  . 
at our institutions large fov images were reconstructed , however they do not include the entire lungs because the upper regions were often excluded from dedicated cardiac ct examinations . several limitations occur in our study . 
sixty - four - slice ct equipment fulfills current standards to perform cardiac examinations [ 8 ] , despite available more recent ct generations may effectively reduce the radiation dose to patients [ 79 ]  . conclusions in conclusion , a considerable number of non - cardiac findings are reported in ctca examinations across different centers . 
radiologists should carefully take into account and describe significant and major non - cardiac findings in ctca reports . conflict of interest none of the authors have potential conflict of interests or financial disclosures concerning the material of this study . ethical standards this article contains a retrospective study ; for this type of study formal consent is not required . 
kirchin2 jonas stroeder1 peter fries1 arno buecker1 received : 25 march 2015 / accepted : 28 april 2015 / published online : 19 june 2015 the author ( s ) 2015 . 
this article is published with open access at springerlink.com abstract objective to evaluate low - dose gadobenate dimeglumine - enhanced mri for the differential diagnosis of malignant renal tumors . methods sixty - two consecutive patients with unclear diagnosis at mdct / ultrasound underwent dynamic cemri of the kidneys with 0.05 mmol / kg gadobenate dimeglumine . 
minimal artifacts that did not compromise diagnosis were noted in 4 / 62 patients . conclusion low - dose dimeglumineenhanced mri is effective for the differential diagnosis of malignant renal tumors . gadobenate keywords gadobenate dimeglumine kidney renal mri renal cell carcinoma introduction although renal cell carcinoma ( rcc ) is the most common malignant epithelial tumor of the kidney accounting for 8590 % of all solid renal tumors in adults and representing 5 % of all cancers in men and 3 % in women [ 1 , 2 ] , benign solid neoplasms such as angiomyolipoma ( aml ) and oncocytoma represent 1014 % of all resected solid renal tumors [ 35 ]  . 
a major clinical need therefore is to accurately differentiate rcc and other malignant renal lesions which typically require urgent surgical attention from benign solid neoplasms for which conservative management is usually indicated . whereas contrast - enhanced ultrasound ( ceus ; [ 68 ] ) and multi - detector - computed tomography ( mdct ; [ 911 ] ) are frequently first - line imaging techniques that reveal the presence of renal masses , often incidentally , subsequent work - up of patients with suspected malignant renal disease is usually performed using contrast - enhanced mr imaging ( ce - mri ) because of the wide versatility of this technique and its ability to accurately identify fat within renal tumors . 
 several studies have demonstrated the effectiveness of cemri not only for the differential diagnosis of renal tumors but also for the accurate differentiation of different rcc sub - types [ 1219 ]  . 1 3 radiol med ( 2015 ) 120 : 11001111 1101 to date , most recent protocols for ce - mri of the kidney have utilized gadolinium - based contrast agents ( gbcas ) at a dose of at least 0.1 mmol / kg bodyweight [ 1318 ]  . 
 moreover , the contrast agents used have invariably been conventional gbcas such as gadopentetate dimeglumine which have standard r1 relaxivity values of approximately 1 at 1.5 t [ 20 ]  . 
the aim of our study was 4.2 l mmol to retrospectively determine the diagnostic performance of ce - mri for the accurate diagnosis of malignant renal masses using a lower dose ( 0.05 mmol / kg bw ) of the much higher relaxivity gbca gadobenate dimeglumine ( multihance ; bracco imaging spa , milan , italy )  . 1 s methods and materials patients between january 2008 and december 2013 , 184 consecutive patients at our institution underwent abdominal cemri with 0.05 mmol / kg bw gadobenate dimeglumine with specific emphasis on dynamic ce - mri of the kidneys . 
 of these 184 patients , 122 ( 66.3 % ) underwent ce - mri for follow - up of prior surgical resection of known malignant lesions or for routine - scheduled follow - up of known benign lesions . 
for contrast - enhanced imaging , a dynamic t1 - weighted gradient - echo sequence ( 160210 / 4.54.8 ; flip angle , 70 ; slice thickness , 56 mm ; gap , 1 mm ; matrix 154180 256 ; fov , 3545 cm ) was used when using a siemens magnetom vision or sonata . 
in the equilibrium phase , a t1w gradient - echo sequence with chemically selective fat saturation was acquired ( 134160 / 2.32.7 ; flip angle , 70 ; slice thickness , 5 mm ; gap , 1 mm ; matrix 154 195 256320 ; fov , 3545 cm )  . 
a dixon t1w sequence with the following parameters was acquired : tr 6.77 ms ; te 2.38 ms ; slice thickness 3 mm ; fov , 380 mm2 ; breath - hold acquisition time 21 s , permitting acquisition of the following 4 t1w images at each slice level : in - phase image ( standard t1 ) , opposed - phase image , water - only image ( fat suppressed t1 ) , fat - only image . contrast - enhanced t1 - weighted gradient - echo acquisitions were obtained dynamically in the cortico - medullary and nephrographic phases after administration of a bolus of 0.05 mmol / kg bodyweight of gadobenate dimeglumine at a rate of 2 ml / s followed by a 20 - ml saline flush . 
for early examinations , the first pass was timed to the corticomedullary phase by best guess ( 25 s post - start of contrast injection ) while the nephrographic phase was acquired at approximately 5 min post - contrast injection . 
with the newer vibe sequences , multiple phases were acquired and the appropriately timed sequences were chosen from the acquired data . routine diffusion - weighted imaging ( dwi ) for patients with suspected rcc was introduced into our department in september 2010 when the magnetom aera was installed . 
 of the 62 patients included in this assessment , dwi was performed for 29 patients using an echo planar imagingspin echo ( epi - se ) sequence with free breathing . 
based on ce - mri diagnosis in conjunction with available findings from prior diagnostic imaging studies , patients were referred either for surgical resection of the detected lesion ( s ) or for conservative management . 
typically , lesions that show no evidence of homogeneous fat 1 3 1102 radiol med ( 2015 ) 120 : 11001111 distribution on unenhanced mr images but which demonstrate contrast enhancement following contrast administration are malignant in nature . 
final lesion diagnosis was based on the histopathologic results for the specimen obtained at surgical resection or on imaging follow - up obtained after at least 1 year . subsequent retrospective evaluation of images was performed qualitatively by two readers ( pf , ab ; 8 and 15 years experience in abdominal mri , respectively ) in consensus who were not involved in the conduct of the studies and who were fully blinded to the clinical history of the patients , the results of all diagnostic imaging examinations , and to the final clinical diagnosis . 
assessments were performed in terms of quality of kidney visualization ( insufficient , poor , moderate , good , excellent ) , presence of artifacts ( severe , moderate , minimal , none ) , extent of diagnostic information ( unsatisfactory , partial , satisfactory , complete ) , and overall diagnostic value ( limited , satisfactory , high )  . 
additional assessments were performed of lesion size and of any additional diagnostic information . statistical analysis diagnostic performance for the characterization of lesions as malignant or benign was performed at the patient level for all 62 patients using ce - mri images plus unenhanced axial dual - echo t1 - weighted in - phase and opposed - phase gradient - echo images for the analysis of fat content . 
for this evaluation , patients diagnosed with malignant renal lesions at ce - mri which were confirmed as malignant at final diagnosis were considered true positive ( tp ) while patients diagnosed with benign renal lesions or no lesions at ce - mri which were confirmed as benign or absent at final diagnosis were considered true negative ( tn )  . 
patients with renal lesions diagnosed as malignant at ce - mri which were confirmed as benign at final diagnosis were considered false positive ( fp ) while patients with renal lesions diagnosed as benign at ce - mri which were confirmed as malignant at final diagnosis were considered false negative ( fn )  . 
based on these findings , determinations were made of the sensitivity , specificity , accuracy , positive predictive value ( ppv ) , and negative predictive value ( npv ) of cemri with 0.05 mmol / kg gadobenate dimeglumine for the diagnosis of malignant renal tumors . results based on ce - mri findings alone , 39 / 62 ( 63 % ) patients were diagnosed with malignant renal lesions . 
based on its appearance at ce - mri ( solid , hypovascular , showing almost no contrast uptake , and without characteristic features of a benign lesion ) , the lesion was recommended for resection . 
the t2w haste sequence ( a ) reveals a small lesion in the left kidney ( arrow ) together with enlargement of the left renal vein , filled with material that is isointense to the normal renal parenchyma ( arrowhead )  . 
on the corresponding t1w image ( b ) the tumor is hyperintense and no flow void is visible within the left renal ve after injection of gadobenate dimeglumine at a dose of 0.05 mmol / kg bw the tumor and left renal vein show inhomogeneous enhancement in the early phase ( c ) with early contrast wash - out in the later phase ( d )  . 
the necessary imaging information needed to make a diagnosis was considered complete in all 62 patients ; the value of this diagnostic information was considered high in 61 patients and satisfactory in just one patient . an early prospective assessment of the diagnostic performance of ce - mri for the differentiation of patients with malignant renal lesions from patients with benign renal lesions determined values for sensitivity , specificity , ppv , and npv of 93.8 % ( 15 / 16 ) , 66.7 % ( 8 / 12 ) , 78.9 % ( 15 / 19 ) , and 88.8 % ( 8 / 9 ) , respectively [ 9 ]  . 
in that study , all oncocytomas were falsely classified as carcinomas ( fp lesions ) while three amls and three inflammatory lesions were correctly classified as benign ( tn lesions ) resulting in an overall per - patient - based accuracy of 82.1 % ( 23 / 28 )  . 
in common with other studies focused on the ce - mri evaluation of renal masses [ 1318 ] , the study utilized a conventional gbca at a dose of 0.1 mmol / kg bodyweight [ 9 ]  . 
our retrospective study , performed as part of routine clinical practice in patients referred for abdominal / renal mri because of unclear findings on multiphasic mdct , utilized gadobenate dimeglumine at a dose of only 0.05 mmol / kg bodyweight . 
on the vibe sequence with acquisition of in - phase , opposed - phase , and dixon fs - images ( bd ) in one single breath - hold , the lesion demonstrates a hypointense rim on the in - phase image ( b ) , some hypointense areas in the center on the opposed - phase image ( c ) indicating fat within the tumor , and a homogeneous hypointense signal in the 50 , 400 , 800 fat suppressed image ( d )  . 
the diffusion - weighted images and the adc - map ( e ; b adc from left to right ) reveal restricted diffusion and a hypointense appearance of the tumor in the adc - map . 
although comparison with a full dose of another gbca was not performed in our study , our results suggest that equivalent diagnostic performance might be achieved with just half the amount of gadolinium if gadobenate dimeglumine is the utilized gbca . 
in this regard , a previous intra - individual crossover comparison of 0.05 mmol / kg gadobenate dimeglumine with 0.1 mmol / kg gadopentetate dimeglumine in patients undergoing ce - mri of the liver revealed clear equivalence during the dynamic phase of 1 3 radiol med ( 2015 ) 120 : 11001111 1105 fig . 
2 continued contrast enhancement with significant superiority for gadobenate dimeglumine during the delayed hepatobiliary phase [ 21 ]  . clearly , these findings are potentially very important given the risk of nephrogenic systemic fibrosis ( nsf ) in patients with severe renal insufficiency given the possibility of compromised renal function in patients with renal tumors and the fact that new - onset post - operative chronic kidney disease ( ckd ) is a relatively frequent occurrence in patients undergoing curative surgery for renal cell carcinoma , particularly in patients aged 60 years or older and in patients with already decreased preoperative renal function [ 2226 ]  . 
in this regard , although symptoms of nsf typically manifest within approximately 3 months of gbca administration , longer lead - times are not unknown [ 27 , 28 ]  . 
notably , no unconfounded cases of nsf have yet been reported for gadobenate dimeglumine despite its regular use in patients at heightened risk of developing this disease [ 2932 ]  . 
although this level of hepatobiliary excretion does not alter the pharmacokinetic profile of gadobenate dimeglumine relative to the profiles of conventional gbcas [ 44 , 45 ] or the characteristic dynamic enhancement patterns of frequently encountered tumors in the liver [ 4651 ] and breast [ 5255 ] , it is sufficient to permit delayed hepatobiliary phase imaging of the liver for the improved detection and characterization of liver lesions [ 4651 ]  . 
on the one hand , the similar dynamic enhancement behavior of gadobenate dimeglumine relative to conventional gbcas , even at half the dose [ 21 ] , may explain the similar diagnostic performance of gadobenate dimeglumine for renal mri not only in 1 3 1106 radiol med ( 2015 ) 120 : 11001111 fig . 
the areas of increased signal on the t1w image are hypointense on the opposed - phase image ( c ) and the t1w fs image ( d ) , indicating fat within the tumor . 
taken together these findings indicate multiple angiomyolipoma , which were proven after nephron sparing surgery of the largest lesion ( performed because of the risk of bleeding ) terms of the accurate detection of malignant lesions but also the accurate differentiation of malignant from benign lesions . 
in this regard , the fp lesions detected in our study ( 5 oncocytoma , 3 atypical aml i.e. , aml without visible fat ) are typical of the fp lesions detected elsewhere [ 9 , 15 , 1719 , 56 , 57 ]  . 
the t2w haste sequence ( a ) shows an inhomogeneous cystic lesion ( arrow ) of the upper pole of the left kidney surrounded by a hypointense rithe lesion is almost isointense to the renal cortex and medulla on the unenhanced t1w image ( b )  . 
the t1w fs image during the equilibrium phase ( e ) shows persistent enhancement of the rim ( arrowheads ) , indicating a wall of inflammatory tissue surrounding an abscess formation many radiologic features with certain types of rcc [ 12 , 18 , 58 ] making accurate and consistent differentiation challenging . 
atypical aml without visible fat accounts for approximately 5 % of all amls [ 18 , 56 ] , while oncocytomas account for approximately 37 % of all adult renal neoplasms [ 59 ]  . 
on the other hand , the additional possibility to acquire delayed hepatobiliary phase images of the liver during the same imaging session may be of value for patients diagnosed with aggressive and potentially metastatic rcc or with other incidental findings detected during the initial dynamic acquisition . 
although in all cases these findings were noted on dynamic phase acquisitions of the liver as hypervascular lesions , reflecting the typical enhancement pattern of metastases from rcc , such patients may benefit from an additional hepatobiliary phase exam at no extra cost or inconvenience and with no additional gbca administration , particularly given that as many as 30 % of patients with rcc present with metastases [ 6062 ] and that metastatic rcc has a relatively poor prognosis ( 5 - year survival rate approximately 20 % [ 63 , 64 ] )  . 
in this regard , gadobenate dimeglumine is specifically approved in europe and elsewhere for mr imaging of the liver at a dose of 0.05 mmol / kg bodyweight [ 68 ]  . 
as noted elsewhere [ 29 , 31 , 69 ] , the partial hepatobiliary elimination of gadobenate dimeglumine combined with the 1 3 1108 radiol med ( 2015 ) 120 : 11001111 fig . 
diagnosis based on ce - mri was multiple rcc ; however , histology confirmed the lesions to be multiple oncocytoma administration of a reduced dose in at - risk patients may in part explain the absence of nsf in patients given this gbca . our study has several limitations . 
 one such study [ 15 ] showed that the addition of adc information to ce - mri findings led to the reclassification of 3 of 6 oncocytomas and 2 of 2 multilocular cystic nephromas that had originally been misdiagnosed as malignant on ce - mri alone , thereby increasing specificity from 89 to 96 % . 
on the dwi image with a b - value of 800 ( c ) the liver metastases as well as the tumor in the left kidney are hyperintense indicating diffusion restriction . 
the outcomes assessed were the 2to 5 - year overall survival ( os ) , disease - free survival ( dfs ) , and laryngectomy - free survival ( lfs ) results the search identified ten studies which were used for the meta - analysis ( n 2013 patients )  . 
laryngectomy provided a better rate of dfs than ct and rt , but os were similar across the different larynx - preserving treatments and laryngectomy . keywords chemotherapy laryngeal cancer laryngectomy meta - analysis radiotherapy introduction a key goal of treating patients with locoregional advanced laryngeal cancer is to preserve larynx function [ 14 ]  . 
often surgery for advanced laryngeal cancer is a total laryngectomy which , although it offers good local control , has significant functional consequences and can greatly impact a patients quality of life [ 3 , 5 ]  . over the past several years there has been a change in the strategies to treat locoregional advanced laryngeal cancer . 
there has been an increase in the number of patients treated with radiation therapy ( rt ) and chemotherapy ( ct ) and a decrease in the number of patients treated with surgery [ 3 , 6 ]  . 
several well - designed randomized trials have evaluated the effects of a number of different 1 3 1154 radiol med ( 2015 ) 120 : 11531169 nonsurgical treatments that are aimed at optimizing larynx preservation [ 1 , 2 , 79 ]  . 
the use of rt or ct ( alone , in combination , or sequentially ) is associated with a high incidence of acute toxicity and disruption in laryngeal function , particularly in patients treated with concurrent rt and ct [ 1114 ]  . 
to our knowledge , this is the first metaanalysis to address this issue . methods search strategy and study selection medline , cochrane , embase , and google scholar databases were searched ( until may 5 , 2014 ) for studies that evaluated total laryngectomy rt and three larynxpreserving strategies in patients with advanced laryngeal cancer . 
the following search terms were used : larynx / laryngeal cancer , hypopharyngeal cancer / carcinoma , chemoradiotherapy / chemotherapy / radiotherapy , preservation / preserving , larynx - preservation , laryngeal preservation , and organ - preserving . 
the analysis was performed in adherence to the prisma guidelines . data extraction data were extracted by two independent reviewers and a third reviewer was consulted in the case of any uncertainty or disagreement . 
the following information / data were extracted from the included studies : the name of the first author , year of publication , study design , number of participants in each treatment group , participants age and gender , tumor location , cancer stages , patient performance status , treatment regimens , and outcomes of measures ( os , dfs , lfs rates )  . quality assessment the quality of the studies and included data was evaluated using the cochrane risk of bias tool [ 15 ]  . 
similar to study inclusion and data extraction , two independent reviewers performed the quality assessment and a reviewer was consulted for any disagreement . statistical analysis the outcomes assessed were 2to 5 - year rates of os , dfs , and lfs . 
either a q statistic with p < 0.10 or an i2 statistic > 50 % indicated heterogeneity existed among the studies , and hence a random - effects model ( dersimonian - laird method ) of analysis was used . 
all statistical analyses were performed using the comprehensive meta - analysis version 2.0 ( biostat , englewood , nj , usa ) along with microsoft excel 2007 . 1 3 radiol med ( 2015 ) 120 : 11531169 1155 fig . 
following a full - text review , 17 studies were excluded for not reporting outcomes of interest ( n 9 ) , not being retrospective in design ( n 5 ) , not being a full - text article ( n 1 ) , and reporting the same study as another article ( n 2 )  . 
eighteen studies [ 1 , 2 , 79 , 1628 ] were included in the systematic review of clinical outcomes and ten [ 1 , 2 , 79 , 1620 ] in the meta - analysis . 
 the ten studies included in the meta - analysis encompassed 2013 patients . clinical outcomes most of the included studies were randomized controlled trials ( 10 / 18 ) ( table 1 )  . 
the age of patients ranged from 53 to 69.5 years , most were males , and most of the patients in each study received larynx preservation treatment ( table 2 )  . 
across the studies the location of tumors varied and tumor stages ranged from ii to iv , and generally , most were t3 and n0 ( table 1 ) ; in 10 of the 18 studies the frequency of t3 tumor stage was 50 % 40 % . 
across the studies , inclusion criteria regarding functional impairment varied both in the assessment scale used and in criteria ( table 1 ) ; of the studies that reported inclusion criteria performance status , six studies 50 , nine used a used a karnofsky performance score of 1 3 1156 radiol med ( 2015 ) 120 : 11531169 1 3 radiol med ( 2015 ) 120 : 11531169 1157 who performance status of scale ( either the studies and are summarized in table 2 . 2 , and two used the ecog 2 or > 2 )  . 
treatment regimens differed across os , dfs , and lfs decreased with greater number of years following treatment both for the randomized controlled trials , which compared different treatments regimens , and the single arm studies ( table 3 )  . 
 [ 18 ] also showed selection bias due to not using a random sequence generator for randomization and allocation concealment . sensitivity analysis using the leave - one - out approach found that , in general , the direction and magnitude of the combined estimates did not change markedly after excluding individual studies , indicating that the meta - analysis had good reliability ( tables 4 , 5 , 6 )  . 
these features enable the standardization of the entire set of clinical data exchange of a health system [ 8 ]  . dcm4chee supports the ihe ( integrating the healthinterface care enterprise ) workflow : it contains an 1139 personalized for type of users supported by a web browser . 
 dcm4chee can connect dicom modality ( ct , mr , cr , us ) workstations and store any type of dicom object and apply a data compression , if necessary . 
5 screenshot of nexus 7 ( google android tablet ) using the google chrome browser via the wlan discussion the archive configuration was quite intuitive , although it should be noted that this operation must be carried out by professionals with specific knowledge and experience in the field of computer networks . the application dcm4chee , having achieved a score of 41 / 50 , does not reach the maximum evaluation . 
this suggests that its performance could be improved with some implementation . the best performance of dcm4chee was in the patient search in archives , resource management system , and os compatibility . the worst performance of dcm4chee was query / retrieve exams and languages supported . however , it is necessary to emphasize that the results obtained were very satisfactory , enabling the creation of a small domestic radiological network able to meet all the characteristics and specificity of a commercial pacs . in this experience , the archive has proved optimal performance without highlighting problems or at least critical as you might expect from an open - source application . 
in homemade lan the software was compatible with all systems ; it has proven to respond very quickly and with a good view of dicom images in terms of resolution , on all screens used . 
according to user experience , dcm4chee is a very simple system for managing dicom archives , but at the same time , it is very complex , developed , and prepared for the various operators basing on their skills . 
 being only a pacs system still managed to gather all the historical images of individual patients , putting them on one screen . the main limitation in the use of oss devices lies in their very essence : the availability of the source code for the user and the possibility of a change make it unthinkable to certify them as medical devices [ 9 ]  . this situation does not occur for proprietary software , since no one can access the source code and , therefore , make unauthorized changes . it is important to underline that the medical device certification is not mandatory in situations where the pacs has to do archive and simple search of clinical imaging . 
following the medical device definition in directive 2007 / 47 / eec [ 10 ] , the point 8.4 of manual on 1 3 radiol med ( 2015 ) 120 : 11381145 table 3 results of the analyzed parameters functions graphical user interface ( gui ) managing users and roles patient search in archives trash archive managing remote hosts resource management system query / retrieve exams receiving exams languages supported os compatibility total 1143 points 41 / 50 borderline and classification in the community regulatory framework for medical devices ( version 1.16 ) [ 11 ] and the guidelines on the qualification and classification of stand - alone software used in healthcare within the regulatory framework of medical devices ( meddev 2.1 / 6 ) [ 12 ] , we can observe that pacs that are only intended for archiving or storage of data may not fall within the definition of a medical device , provided that data are not manipulated . 
in this case , if the pacs system ( archive and viewer ) is intended to be used for one or more of the medical purposes set out in the medical device definition ( article 1 directive 2007 / 47 / eec ) [ 10 ] , it is possible to use a certificated viewer ( class i ) and a not certificated pacs . 
7 system and queue information ( active and past ) of all processes in and out of the archive itself pacs do not need features that require the medical device classification , like driving device , influencing the use of a source device , controlling image acquisition for image enhancing . conflict of interest the authors declare that they have no conflict of interest related to the publication of this article . ethical standard this article does not contain any studies with human participants or animals performed by any of the authors . informed consent argument of this article . informed consent is not necessary due to the radiol med ( 2015 ) 120 : 11461152 doi 10.1007 / s11547 - 015 - 0542 - 0 radiotherapy the treatment of patients with 13 brain metastases : is there a place for whole brain radiotherapy alone , yet ? a retrospective analysis michela buglione1 sara pedretti1 stefano gipponi2 luciano buttolo3 paolo panciani3 pietro luigi poliani4 roberto liserre5 paolo borghetti1 ludovica pegurri1 loredana costa1 luca triggiani1 nadia pasinetti1 paolo ghirardelli1 sara pandini1 alessandro padovani2 stefano maria magrini1 received : 22 february 2015 / accepted : 16 april 2015 / published online : 28 april 2015 italian society of medical radiology 2015 aim to evaluate the efficacy of whole brain radiotherapy ( wbrt ) with or without other treatments in patients ( pts ) with 13 brain metastases ( bm )  . materials and methods toxicities and survival of 134 pts treated between 2009 and 2013 with wbrt alone ( 58 pts ) , wbrt plus surgery ( sur - wbrt : 42 pts ) or wbrt followed by stereotactic or integrated boost radiotherapy ( srt - wbrt : 34 pts ) were analyzed . 
about 60 % of patients had mild acute toxicity ( g1 ) , especially headache ( 51 % ) and fatigue ( 34 % ) ; only 2 patients ( 2 % ) had severe ( g3 ) headache and 5 patients ( 4 % ) severe fatigue ( g3 ) reversible with oral steroids . 
among 80 pts followed up with mri , 12 ( 15 % ) had leukoencephalopathy ( equally distributed across subgroups ) and 5 ( 6 % ) radionecroses , 4 / 5 asymptomatic , 5 / 5 in pts given intensified treatments . conclusions this analysis confirms the known prognostic factors for bm , emphasizing the importance of intensified treatments in a population with favorable features . on behalf of the neuro - oncology group , spedali civili hospital and brescia university . keywords brain metastases radiotherapy prognostic factors survival stereotactic radiotherapy surgery * michela buglione michela.buglione@unibs.it 1 radiation oncology department , spedali civili hospital , brescia university , p.le spedali civili 1 , 25123 brescia , italy 2 neurology department , spedali civili hospital , brescia university , p.le spedali civili 1 , 25123 brescia , italy 3 neurosurgery department , spedali civili hospital , brescia university , p.le spedali civili 1 , 25123 brescia , italy 4 pathology department , spedali civili hospital , brescia university , p.le spedali civili 1 , 25123 brescia , italy 5 neuroradiology department , spedali civili hospital brescia , p.le spedali civili 1 , 25123 brescia , italy introduction historically , the treatment of brain metastases entailed the use of exclusive whole brain radiotherapy ( wbrt ) , to treat the sites of disease and to prevent the recurrence in other cerebral areas [ 1 , 2 ]  . 
instead , patients with 13 bm are often amenable to treatments alternative or integrated with wbrt such as surgery , stereotactic radiosurgery or concomitant fractionated integrated boost ( sib ) [ 3 ]  . 
the therapeutic choice is 1 3 radiol med ( 2015 ) 120 : 11461152 1147 conditioned not only by the number of brain lesions but also by other prognostic factors : performance status , age , absence of extracranial metastases and control of primary tumor . 
these prognostic factors are all present in the graded prognostic assessment ( gpa ) classification [ 4 ] , whereas in the recursive partitioning analysis ( rpa ) classification [ 5 ] the number of lesions is not considered . the end - point of the study has been to evaluate the toxicities and survival in a retrospective series of 134 patients affected by 13 brain metastases and treated with three different modalities : wbrt alone ( wbrt ) , surgery plus wbrt ( sur - wbrt ) and stereotactic boost or simultaneous integrated boost radiotherapy plus wbrt ( srt - wbrt )  . materials and methods from january 2009 to december 2013 , 134 patients with 13 brain metastases , good performance status and stable primary disease or asymptomatic synchronous primary tumor were consecutively treated at the radiation oncology department , spedali civili , brescia university . whole brain radiotherapy was delivered with two parallel opposite fields and standard doses ( 3 gy / fraction for 10 fractions or 4 gy / fraction for 5 fractions ) ; patients were immobilized with a 3 - point thermoplastic mask ( wbrt and sur - wbrt )  . stereotactic radiotherapy was provided with tomotherapy , with a single dose defined according to the volume to be treated as per rtog protocol 90 - 05 ( srs ) [ 6 ]  . 
patients treated with wbrt and concomitant integrated boost were also treated with tomotherapy in 10 fractions : for each fraction , 3 gy were given to whole brain and 4.5 gy to the metastatic site ( s )  . 
both the subsets of patients in this group ( srt - wbrt ) were immobilized with a 5 - point thermoplastic mask ; the target definition was done after co - registration of brain magnetic resonance imaging ( t1 contrast - enhanced sequence ) with planning ct and gtv was expanded directly to ptv ( 3 mm - isotropic expansion )  . the toxicity was considered acute if detected in the period between the start of radiotherapy up to 30 days after the end of the treatment , while late toxicity was registered from 90 days after the end of treatment until the last follow - up visit . 
the late toxicity , in terms of incidence of leukoencephalopathy and radiation necrosis , was evaluated only for patients who had neuroradiological follow - up with mri ( 80 patients60 % )  . local response and the pattern of local recurrence in the metastatic sites were evaluated at 3 and 12 months and correlated with treatment modalities , using chi - square test . 
 overall survival ( os ) , neurologic disease - specific survival ( dss ) and neurologic disease - free survival ( dfs ) were analyzed and compared , for the three treatment groups . 
the following events were considered to define , respectively , the three survival endpoints : death ( os ) , death caused by brain metastases ( dss ) and brain disease progression ( dfs )  . univariate analysis was done using the kaplanmeier estimator ( log - rank test )  . 
then the factors linked with significant differences in outcome at univariate analysis were entered into the multivariate stepwise cox proportional hazard ratio model , along with the variables judged to be clinically relevant . 
statistical analyses were obtained using the proprietary software spss17.0 ; a p value < 0.05 was considered statistically significant . results the characteristics of patients and disease are shown in table 1 . in our series , 58 patients underwent wbrt alone , 42 surgery and radiotherapy ( sur - wbrt ) and 34 more nonsurgical patients had wbrt and concurrent ( 21 patients ) or sequential ( 13 patients ) boost on the disease sites ( srt - wbrt )  . the primary tumor type was lung adenocarcinoma in the majority of patients ( 58 % ) , breast cancer and melanoma contributed for 15 % each ; different cancer types constituted the remaining 26 % . 
in the whole series , about two - thirds of the patients had the diagnosis of brain metastases at the same time or within 1 year from that of the primary tumor ( 42 and 15 % , respectively ) ; 32 and 11 % of them , respectively , from 1 to 5 years and more than 5 years after primary tumor diagnosis . 
only one case of radiation necrosis was submitted to surgical removal ( sur - wbrt group ) , the other four having been diagnosed with mri in asymptomatic patients ( they were all in the srt - wbrt group )  . 
green line stereotactic radiotherapy or simultaneous integrated boost plus whole brain radiotherapy ( srt - wbrt ) , blue line surgical treatment plus wbrt ( sur - wbrt ) , red line wbrt alone type , the use of chemotherapy after radiation therapy , radiotherapy modality and the tumor response . patients in rpa class i ( p 0.002 ) , who had intensified treatments ( p < 0.001 ) , who were given systemic therapy after radiation therapy ( p < 0.001 ) and who had a complete or subtotal partial response to radiotherapy ( p 0.003 ) have a longer os . 
some special parameters such as the interval between the appearance of metastases and primary tumor diagnosis [ 8 ] , response to steroid therapy [ 9 ] and tumor volume [ 10 ] were considered only 1 3 1150 radiol med ( 2015 ) 120 : 11461152 in rare cases . 
the most important difference between these two systems is that the second one considers as a prognostic factor also the number of metastases and the primary site of disease [ 11 ]  . 
the analysis of the present series has confirmed the prognostic significance of almost all the factors identified in the two classifications . the use of different hypofractionated schedules for wbrt ( 30 gy in 10 fractions vs 20 gy in 5 fractions ) was not related , in a few papers [ 12 , 13 ] , to a difference in overall survival but only to an increase in acute toxicity for the more rapid fractionation schedule . 
in the present series no survival differences were evident according to the fraction dose ; however , an increase in acute toxicity with the shorter schedule was not documented . multimodal combined treatment with wbrt , for patients with 13 brain metastases , has become the standard in the last decades [ 14 ] , thanks to advances in radiation techniques and to improvement of surgical techniques [ 15 ] , with a marked reduction in periand post - operative mortality . the efficacy of surgery followed by wbrt for single brain metastasis has been investigated in three randomized clinical trials . 
 [ 16 ] demonstrated that combined treatment ( surgery plus wbrt ) led to a longer survival , longer functional independence , and a lower recurrence rate compared to radiotherapy alone . 
the third randomized trial [ 18 ] failed to demonstrate an improvement in survival for the patients treated with combined treatment ; since patients with diffuse extracranial disease and poor performance status were recruited , it was confirmed that this group of poor prognosis patients , should not be offered an intensified treatment . literature data on survival have been confirmed in the present series : surgery followed by wbrt obtained longer overall survival and better response to treatment compared to wbrt alone ; no differences were found in recurrence rate in metastasis site . the efficacy of a stereotactic boost associated with wbrt has been shown in two randomized clinical trials . 
 in the rtog 9508 trial [ 19 ] 333 patients with 13 brain metastases were randomly allocated to either wbrt or srt - wbrt : wbrt and stereotactic boost treatment improved functional autonomy for all patients and survival for patients with a single metastasis . 
a smaller trial [ 21 ] showed that combined wbrt and radiosurgery for patients with two to four brain metastases significantly improves control of brain disease , without improvement of survival . present analysis confirmed a better local control and a better response to treatment in patients treated with srtwbrt compared to wbrt alone , as documented in the literature , and a longer overall survival has been documented both in the whole series and in the rpa class ii . almost two - thirds ( n 21 ) of the patients of the present series treated with stereotactic techniques had wbrt with concomitant integrated boost ( sib ) , as opposed to about a third ( n 13 ) treated with wbrt followed by sequential stereotactic boost ( srs )  . 
 [ 22 ] in 2013 published a retrospective review of 500 patients treated with srs alone or sib - wbrt : no differences in os were found but sib was associated with a reduced intracranial failure rate likely due to the wbrt component of the treatment ; however , srs patients did not have wbrt , at variance with the present series . few authors compared the different intensified treatments for 13 brain metastases . 
a better overall survival was documented but only in rpa class ii . the high rate of local recurrence after surgery alone has led many authors to add a stereotactic treatment targeting the surgical cavity only [ 2528 ]  . 
these studies have shown good tolerance to treatment and better 1 and 2 years local control , a lower risk of progression with other brain metastases , combined with a moderate increase in late toxicity ( radiation necrosis in 5 % of cases ) when compared to wbrt alone . 
many clinical studies addressed the issue of a possible neurocognitive detrimental effect of wbrt [ 29 ] to justify the elimination of wbrt from the therapeutic options for brain metastases . 
a prospective observational trial on neurocognitive function in relation to different radiotherapy modalities ( wbrt , srt - wbrt , srs alone ) and other disease and treatment variables is now ongoing in italy , promoted by the central nervous system study group of italian association of radiation oncology ( airo )  . conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent for retrospective studies formal consent is not required . radiol med ( 2015 ) 120 : 975981 doi 10.1007 / s11547 - 015 - 0528 - y radiotherapy postsurgical therapeutic approaches to glioblastoma patients submitted to biopsy ( ba ) or partial resection ( pr ) : the possibilities to treat also them without renunciations . 
study from the brescia neurooncology group michela buglione1 paolo borghetti1 sara pedretti1 luca triggiani1 marco maria fontanella2 giannantonio spena2 salvatore grisanti3 roberto liserre4 luigi pietro poliani5 stefano gipponi6 luigi spiazzi7 stefano maria magrini1 received : 7 december 2014 / accepted : 24 february 2015 / published online : 15 march 2015 italian society of medical radiology 2015 abstract the extent of surgery predicts overall survival ( os ) in patients treated for glioblastoma ( gbm )  . 
this strategy , combined with an increased use of chemotherapy , resulted in reduced treatment burden , in an improved 2 - year os rate and prospectively in better quality of life , even in this prognostically worse subset of glioma patients . keywords glioblastoma radiotherapy partial surgery biopsy temozolomide introduction glioblastoma ( gbm ) is the most common malignant primary central nervous system tumour in adults . 
for more than three decades , standard treatment of gbm has been considered surgery and postoperative radiotherapy ( rt ) , rarely combined with chemotherapy ( cht ) [ 13 ]  . 
since 2005 , chemotherapy with temozolomide ( tmz ) ( in a concomitant and adjuvant setting ) has been the standard treatment of patients with gbl submitted to surgery , having obtained a statistically significant improvement of overall survival ( os ) [ 4 , 5 ]  . several factors , also combined in prognostic classes [ 6 ] , affect the prognosis of patients with gbm , including age , preoperative performance status , tumour location and preoperative mr imaging characteristics of the tumour [ 711 ]  . it is also well known that the extent of surgery is an important prognostic factor for predicting os [ 1 , 5 ]  . 
however , extensive resection of malignant gliomas is often difficult ; these tumours , in fact , are frequently invasive and widely infiltrative and often involve functional areas [ 12 , 1 3 976 radiol med ( 2015 ) 120 : 975981 13 ]  . 
moreover , biopsy alone ( ba ) or partial resection ( pr ) is generally applied in patients with poor medical conditions and / or tumours located in deep areas of the brain [ 1 , 8 ]  . 
this group of patients represents the majority of those treated with postoperative rt [ 5 ]  . the optimal approach for patients submitted to pr or ba continues to be controversial [ 1 , 3 , 13 ] , and the factors affecting survival in this group of patients are not well known . the main purpose of this study was to identify clinical and therapeutic variables that effectively predict better survival in gbm patients not submitted to macroscopically radical surgery . 
moreover , an attempt has been made to ascertain if the treatment burden and the outcome of these unfavourably selected patients were affected by the changing treatment paradigm ( in particular , the introduction of tmz chemotherapy )  . materials and methods from 1985 to 2010 , 439 patients affected by gbm were consecutively treated with rt at the istituto del radio radiation oncology department of brescia university . 
among the 172 patients who underwent partial surgery , 70 had a partial resection demble while , for the remaining 102 patients , an initially planned complete resection could not be accomplished due to the extent of the disease . 
the distribution of clinical and therapeutic parameters in the different subgroups is shown in tables 1 and 2 . rt volumes were defined as extended when the whole brain was included , with or without a boost , and limited when confined to the site of disease with margin , with / without a boost dose . 
since fractional dose , total dose and treatment duration are not independent variables from a radiobiological point of view , it should be clearly acknowledged that patients who have undergone complete resection are often submitted to more rapid treatments . 
the intent behind this choice is to spare the patients treated for palliation from unnecessarily long treatments , by increasing the treatment biologic efficacy , thanks to the higher fractional dose and shorter treatment duration . 
 multivariate analysis with the cox regression model ( in the entire cohort of patients and in the already defined subgroups ) was employed ; the initial model included all the variables statistically significant at univariate analysis . all the differences were considered statistically signifi0.05. 
however , in order to better elucidate the relative effect of these factors on survival , it has been decided to present results analytically for these three parameters . tmz was associated to rt using the stupp - schedule [ 14 ] ( concomitant and sequential ) in patients treated with high doses rt . 
tmz chemotherapy in patients treated with hypo - fractionated rt consisted only of a sequential treatment ( 200 mg / mq / die / 5 dies q 28 )  . 
however , detailed analysis of these data will not be reported . statistical considerations differences in the distribution of clinical and therapeutic variables in the different groups of patients were evaluated with the 2 test . patients and treatment features one hundred twenty - four ( 53 % ) patients were treated in the pre - tmz - era ( 19851999 ) and 108 patients ( 47 % ) in the following years ( 20002010 ) ; 60 patients had biopsy alone ( 26 % ) and 172 ( 74 % ) had partial resection . 
performance status and dose per fraction were the only significant factors in patients submitted to pr and ba respectively ( table 5 )  . discussion standard treatment for gbm is based on surgical resection followed by high dose , conventionally fractionated rt combined with concomitant and adjuvant tmz . 
a retrospective analysis combining 416 patients with newly diagnosed and recurrent gbm concluded that survival is significantly improved when a surgical resection of at least 98 % of tumour mass is performed [ 9 ]  . in the modern era , this report has often been referred to by the neurosurgical community , justifying an all - ornone approach , often practiced in the surgical management of gbm . 
on the other hand , analysis of more recent data from a series of 500 patients affected by gbm has shown a significant survival advantage with as little as 78 % of tumour resection , and stepwise improvement in survival was evident even in the 95100 % region [ 13 ]  . 
actuarial os rates at 1 and 2 years were 30 and 13 % for ba ; 40 and 19 % for pr ; 42 and 18 % for radical surgery [ 5 ]  . despite this , it is well known that partial surgery is a very common event , due to surgical drawbacks , compromised performance and neurological status or deep site of disease . this retrospective series analysed the clinical and therapeutic factors possibly affecting os in a cohort of 232 patients with gbm treated with partial surgery or biopsy alone over a long accrual period ( 19852010 )  . 
this was done to evaluate the possible impact of the progressive introduction of tmz and of more sophisticated rt techniques in the therapeutic armamentarium . no consistent differences in the clinical features of the patients belonging to the tmz and the pre - tmz era were observed , with the exception of more frequent use of mri after 1999 . 
while the proportion of patients submitted to biopsy only was substantially unchanged in the two recruitment periods , whole brain rt ( with or without a boost ) associated to high doses was largely predominant in the 80 and 90 s . 
this last observation might well be related to a prognostic advantage derived by the use of both tmz and high dose rt , especially for the pr patients with better kps . however , the use of hypo - fractionated treatments could also be associated with tmz , thus reducing the number of hospital visits , ameliorating compliance and decreasing toxicity . 
the tolerance of hypo - fractionated rt and tmz has already been tested [ 15 ] ; relatively good results were reported in the literature in selected patients [ 16 ] , and the survival data of the present series seem to substantiate theafter the introduction of tmz , the disease itself could be better treated with short course rt and tmz , also in patients submitted to partial surgery or biopsy alone for gbm who are not suitable / eligible for the standard radio - chemotherapy regimen . 1 3 980 conclusion the impact of chemotherapy ( tmz ) on survival in patients treated with radical surgery and high doses of rt ( concomitant and adjuvant ) has already been demonstrated . while the prognosis of gbm patients may be affected by several factors , postsurgical residue has also been recently reported to have a negative impact on survival , also taking into account many other potentially confounding factors [ 17 ]  . 
the extent of surgery has a significant impact on survival at multivariate analysis also in a recent italian multiinstitutional series including part of the patients of the present mono - institutional series [ 18 ]  . thus , in the present series of negatively selected patients submitted to partial surgery and biopsy alone , at multivariate analysis , a favourable effect on the survival of higher total doses was documented in the whole series and is more significant in patients undergoing partial resection ; an advantage for the use of small treated volumes has been also demonstrated . the addition of chemotherapy is related with a survival advantage at multivariate analysis , in the whole series and in both pr and ba patients , even if ba patients are more often treated with short hypo - fractionated schedules and with lower doses . thus , a potential advantage in treating even those patients who are usually considered as negatively selected with radioand chemotherapy , also after biopsy alone , cannot be excluded . however , the guidelines of the italian society for radiation oncology ( airo , online at oterapiaitalia.it / ) do not include the association of radio and chemotherapy as a standard for these patients with poor prognosis . 
interand intrareader variability was evaluated in a subset of 40 patients , using interclass correlation coefficient ( icc ) and bland altman plots . 10 10 results of 115 lesions , 53 ( 46.1 % ) were assessed as ki67 positive and 62 ( 53.9 % ) as ki67 negative . 
moderate agreement in adc measurement could be a limitation . keywords breast neoplasms diffusion - weighted imaging magnetic resonance imaging ki67 antygen tumor markers introduction * paola clauser clauser.p@hotmail.it 1 department of medical and biological sciences , institute of diagnostic radiology , azienda ospedaliero - universitaria , s.maria della misericordia , p.le santa maria della misericordia , university of udine , udine , italy 2 department of oncology , azienda ospedaliero - universitaria , s.maria della misericordia , university of udine , udine , italy the term breast cancer includes a complex and heterogeneous variety of pathologies , with different histological subtypes , as described according to the who classification [ 1 ]  . 
however , these histological differences are not helpful in predicting clinical behavior or response to treatment [ 2 ]  . various characteristics are useful in distinguishing clinical behavior of different types of cancer , like histological grade , presence of lymph nodes metastasis or 1 3 912 radiol med ( 2015 ) 120 : 911918 vascular invasion , but there is still need for more information regarding behavior and prognosis of breast cancer . 
in the past few years , the evaluation of biomarkers has been suggested with this aibiomarkers more frequently used include : estrogen ( er ) and progesterone receptors ( pgr ) , her2 status and the expression of the proliferation index ki67 . 
molecular markers seem to be a strong predictor of prognosis and response to therapy [ 2 , 3 ]  . dynamic contrast - enhanced breast magnetic resonance imaging ( mri ) has been increasingly used , thanks to its ability to give information on both morphology and vascular pattern , and to its high sensitivity and specificity [ 46 ]  . 
 new mri techniques , like diffusion - weighted imaging ( dwi ) , also allow to obtain functional information that can be related to tumor biology [ 7 ]  . 
these values tend to be lower in malignant lesions , where motion is restricted . several studies showed the capabilities of dwi to differentiate benign from malignant lesions [ 810 ]  . 
 according to these findings , the hypothesis that dwi could be related to the expression of biomarkers has been developed : if that was the case , dwi could be used not only to diagnose breast cancers , but also to differentiate more aggressive breast diseases . 10 the aim of our study was to evaluate whether quantitative adc values correlate with different levels of ki67 expression , histology , grade and clinicalpathological subtype in breast cancer . 
interand intra - reader variability was also evaluated in a subset of patients . materials and methods patients selection all patients with a diagnosis of breast cancer that met the inclusion criteria and underwent breast mri in our institution between april 2013 and november 2013 were included in the study . 
approval to this study was obtained from the institutional review board and informed consent was waived due to the retrospective study design . inclusion criteria were : diagnosis of invasive breast cancer at image - guided needle biopsy ; breast mri performed before or at least 2 weeks after biopsy , to ensure absence of post - procedural artifacts ; surgery performed within 3 weeks after mri ; and availability of complete immunohistochemistry pattern with biomarkers ( hormonal receptors status , her - 2 , ki67 / mib1 )  . 
examinations excluded because of significant artifacts were those in which image quality was too low to clearly identify the target lesion . mri study breast mri examination was performed on a 1.5 t magnet ( magnetom , avanto siemens medical system , erlangen , germany ; software numaris 4 version syngo mr b17 ) with dedicated , bilateral , four - channel coil . 
the t1 - weighted sequence was a 3d fast low - angle shot sequences with repetition time 9 ms , echo time 4.76 ms , field of view 340 340 mm , slice thickness 2 mm and matrix 512 . 512 dwi was acquired in the transverse plane using single - shot echo planar imaging ( ss - epi ) , with fat suppression with spair technique , tr 7100 ms , te 84 ms , fov 85 pixel , in plane spatial res330 2 mm2 , slice thickness 4 mm , 24 slices , nex 5 , olution 2 b values 0 and 1000 s / mm2 , acquisition time of 229 . 165 mm , matrix 164 pathological analysis pathological analysis was conducted on surgical specimens after surgery . 
grading was defined according to the elston - ellis classification system [ 13 ] and hormonal receptor status was defined using immunohistochemistry with monoclonal antibody approved by uk nequasbreast hormonal receptor module . her - 2 status was evaluated according to published guidelines [ 16 ] , considering positive a result 3 at immunohistochemistry evaluation on more than 30 % of the cancer cells ( herceptest )  . 
when result was equivocal , fish was used . ki67 proliferation index was measured with the monoclonal antibody mib1 , by reporting the percentage of 1 3 radiol med ( 2015 ) 120 : 911918 reactive cells between the 2000 cells selected randomly from the periphery of the lesion . image analysis two readers with more than 5 years of experience in breast imaging and breast mri reviewed the images in consensus to define the target lesion and measure adc values . 
one of the two readers repeated the measurements in 40 cases , the first 20 consecutive ki67 positive and the first 20 consecutive ki67 negative patients , to assess intra - observer variability . 
to evaluate inter - reader agreement , a third reader with more than 2 years of experience in breast mri was asked to perform measurements on the 40 cases in a separate session . 
all readers were blinded to histological subtype and biomarkers status of the lesions . mri examinations were evaluated on a dedicated workstation ( syngo multimodality workplaceleonardo , siemens healthcare , erlangen , germany )  . 
care was taken to avoid areas of t2 shine - through , such as cystic or necrotic portions of the tumor , shown as areas of high signal intensity on t2w images and adc map . 
the range of the diameter of the roi varied between 6 and 12 msmall rois were used in small lesions to safely avoid surrounding tissue . statistical analysis since the adc values did not follow a normal distribution using shapirowilk test , we used median and interquartile range as summary statistic . patients were divided into two groups according to the ki67 percentage : < 20 % was considered low ( ki67 - negative ) , while 20 % was considered high ( ki67 - positive ) , as according to the st . 
the optimal cutoff able to distinguish the two subtypes of patients according to low or high ki67 level was retrospectively calculated from the data distribution on the roc curves . interand intra - reader agreement was assessed with interclass correlation coefficient ( icc ) and blandaltman plots . statistical analysis was performed using statistical software commercially available ( medcalc software version 9.1.0.1 , ostend , belgium )  . results a total of 118 patients with a diagnosis of breast cancer at needle biopsy were evaluated . 
high levels of ki67 are associated with less cell differentiation and worst prognosis [ 22 ] : this difference in adc values has the potential to differentiate more aggressive disease . 
this could be related to the lower cell differentiation and higher cellularity of high - grade lesions [ 2325 ]  . studies published on the correlation between adc and various tumor characteristics show a wide variability in design and results . 
0.93 for high ki67 ( 0.89 onishi [ 27 ] , in a small subset of patients , used a cutoff level of 14 % , and found a correlation between adc values and proliferation index only for mucinous carcinomas . 3 mm2 / s )  . 10 10 10 10 low proliferation 3mm2 / s and 1.03 on the other hand , martincich [ 19 ] did not find significant differences in the adc values between high index , with median adc of and 3mm2 / s , respectively . 
 same results as martincich were obtained also by jeh [ 28 ] , using a cutoff of 15 % , and kim [ 29 ] , who did not use a cutoff value but interpreted ki67 as a continuous . 
no differences were found when adc value was correlated with histology : same results were also found by martincich and kim [ 19 , 29 ]  . clinicalpathological classification luminal a luminal b - her2 negative luminal b - her2 positive her2 enriched triple negative idc invasive ductal carcinoma , ilc invasive lobular carcinoma median adc for the three grades was : 1.06 mm2 / s for g1 , 0.93 3 mm2 / s for g2 , 0.86 10 mm2 / s for g3 . 
at the immunohistochemical analysis , ki67 expression was 75 % ( > 20 % ) , er was positive ( 90 % ) , pgr was negative and her2 status was equal to 3  . 
 a t1w image before contrast medium ( cm ) injection ; b t1w image with cm shows multifocal cancer with intense enhancement ; c sub0 s / mm2 in which tracted image ; d diffusion - weighted image at b the two lesions demonstrate the same signal intensity of the normal breast parenchyma ; e diffusion - weighted image at b 1000 s / mm2 in which the two lesions appear as hyperintense ; f adc map : the biggest lesion , included in the study , shows an adc value of 0.73 3mm2 / s 10 fig . 
at the immunohistochemical analysis , ki67 expression was 5 % ( < 20 % ) , and er was positive ( 90 % ) , pgr was positive ( 90 % ) and her2 status negative . 
a t1w image without contrast medium ( cm ) injection ; b t1w image with cm shows a lesion with intense enhancement ; c subtracted image ; d diffusion - weighted image at was not visible ; e diffusionweighted image at b 1000 s / mm2 in which the lesions show a mild hyperintense signal ; f adc map : the lesion shows an adc value of 1.13 10 mm2 / s 0 s / mm2 in which the lesion the level of expression of ki67 is also used to distinguish luminal a and luminal b - her2 - negative cancers : luminal a type is characterized by a low proliferation index compared to luminal b - her 2 negative . 
to our knowledge , this is the only study that addresses this topic ; martincich [ 19 ] found a significant difference in a multivariate analysis of subgroups , but only evaluated tumors her2 enriched vs . 
 [ 30 ] evaluated ki67 in patients with luminal type breast cancers , and obtained results similar to that of our study , using a different subset of cases and a different method to position rois . 
using an adc threshold of 1.097 mm2 / s , sensitivity , specificity , positive predictive value , and negative predictive value were 82 % ( 36 of 44 ) , 71 % ( 30 of 42 ) , 75 % ( 36 of 48 ) , and 79 % ( 30 of 38 ) , respectively . a tendency towards lower values of adc in high - grade cancers has already been found in various studies , with or without significant differences in the two groups [ 19 , 29 , 3133 ]  . on the other hand , kamitani et al . 
4 blandaltman plots for intra - observer ( a ) and interobserver ( b ) variability , calculated on a subset of 40 patients , 20 consecutive patients with negative ki67 and 20 consecutive patients with positive ki67 . 
 r1 consensus reading , r2 third reader , i first reading , ii second reading er - negative , pr - negative cancers , but no significant differences were found when analyzing vascular invasion , nuclear grade and her2 status . intraand inter - reader variability showed no systematic difference and an acceptable range when using blandaltman plots . 
other studies showed a low inter - reader variability in evaluating adc of breast lesions [ 35 , 36 ]  . in our study , we found a correlation between high proliferation index and low adc values : it is likely that adc values calculated in breast cancer might be useful to evaluate response to neoadjuvant chemotherapy , and also as to predict the response to treatment [ 13 , 14 , 37 , 38 ]  . 
this could be an interesting application for the future , which needs further studies to be confirmed . the most relevant limitations of this type of studies are the absence of a standardization of the immunohistochemistry panel used to define the proliferation index and the other markers used to classified breast cancer and the absence of a consensus in the cutoff value to define ki67 positivity . 
another important problem , when evaluating dwi , is the lack of standardization in the sequences : different vendors , in fact , use different parameters and there is no standardization in the modalities to measure adc . 
when possible , sequence with artifacts was repeated , thus allowing for an overall high image quality in diffusion - weighted images . in conclusion , dwi could become an important tool to study breast pathologies , thanks to its rapid acquisition times and the ability to provide important information concerning aggressiveness and biology of the disease . 
suboptimal measurement reproducibility and readers agreement are still present and could determine a limitation in this application of dwi . conflict of interest all the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . research involving human participants and / or animals the institution review board approved this retrospective study . 
the overall agreement among different consulted specialists was evaluated and ranked using the cronbachs correlation coefficient ( ) at two time points : after the first and the second round of consultation . results the cronbach index was 0.84 at the end of the first round and 0.93 at the end of the second round . 
the number of disagreements dropped from an overall of 115 , from the first to the second round . conclusions the experts were able to produce an informed consent for ctc , hoping that this may be the beginning of a process focused on implementation of quality standards in ctc . keywords tomography virtual colonoscopy informed consent colonography computed * ennio biscaldi ennio.biscaldi@gmail.com 1 department of radiology , galliera hospital , via mura delle cappuccine 14 , 16128 genoa , italy 2 section of radiology , s . 
massimo hospital , penne , italy 3 department of radiological , oncological and pathological sciences , sapienza university of rome polo pontino , rome , italy 4 department of sciences for health , university of milan , azienda ospedaliera san paolo , unit operativa radiologia diagnostica e interventistica , milan , italy 5 radiology unit , institute for cancer research and treatment , candiolo , italy 6 diagnostic and interventional radiology , department of oncology transplants and advanced technologies in medicine , university of pisa , pisa , italy ct colonography ( ctc ) or virtual colonoscopy is a radiological technique for colon evaluation , with inherent peculiarities : minimal invasiveness [ 1 , 2 ] , good patient compliance [ 3 ] and high sensitivity in detecting clinically significant mucosal lesions [ 47 ]  . technical standardization of the examination protocol [ 8 ] and the diffusion of the technology essential to its execution ( multidetector ct 16 rows and dedicated software for image analysis ) will allow a further diffusion of ctc , particularly in peripheral centers . 
thanks to the recent publication of esge ( european society of gastrointestinal endoscopy ) esgar ( european society of gastrointestinal and abdominal radiology ) guidelines on indications for ctc [ 9 ] ; a further increase in patient referrals from gastroenterologists will be expected . 1 3 900 radiol med ( 2015 ) 120 : 899904 the first consequence of an increased number of examinations will be the risk of a reduced quality of ctc and a downturn in accuracy . to guarantee quality control , avoiding inhomogeneities or technical improperness [ 10 ] , the section of gastrointestinal and abdominal radiology of the italian society of radiology decided to constitute a working group dedicated to develop and codify the standards of quality in ctc . the first activity of this group was dedicated to the production of a common informed consent , shared by different italian researchers active in ctc . the purpose of this work was to realize an informed consent to be diffused by the italian society of radiology , aimed to make patients and referring physicians aware of ctc examination protocol , advantages and disadvantages , limits and potential related risks . materials and methods a group of four members ( eb , nf , fi , gj ) of the gastrointestinal and abdominal section of the italian society of radiology , supervised by the president of the section and three expert members on ctc ( al , en , dr ) , worked together using a modified delphi method [ 11 ] aimed to write a model of informed consent . 
a member of this group ( eb ) chosen as a facilitator was charged with writing a first model of informed consent , merging the informed consents used in other italian and foreign centers of references for ctc [ pisa university , la sapienza university of rome , institute for cancer research of candiolo ( turin ) , s.paolo hospital , milan , and the kings college in london ]  . that text is gathering complete and quick information , written in an easy italian form , understandable to any potential patient . 
the choice of these specialists was made on the basis of essential categories : ( 1 ) curriculum vitae , ( 2 ) daily activity in centers where a minimum of 400 ctcs / year are performed , ( 3 ) the candidate must have participated to italian courses of ctc , ( 4 ) he must have participated in publications with impact factor , in the last 24 months , having a main focus on ctc . an evaluation of each paragraph of the consensus text has been requested to all elected specialist , and they were requested to express their agreement or disagreement or partial agreement , choosing one of the given options . 
in this first phase , every specialist also had the option to give a free answer : allowing the participant to give us some suggestions , with personal impressions . the suggestions , sent by mail , were integrated respectively in each paragraph . in a second step , after a meeting between experts in the group , the facilitator and the president of the study section , any statement marked completely disagree was modified and re - built in a new digital questionnaire . four months following the previous consultation , this new form of the consensus was sent to the same researchers , for a second consultation . 
the only exception was forbidding any modification of the statements , asking the participants only to express their agreement or disagreement to the statements . statistical process of data we evaluated the overall agreement , concerning every voted paragraph , among different consulted specialists . 
statistical software ( spss , 15.0 statistics , chicago , usa ) was used for the entire analyses . results the cronbach index , calculated among the interviewed physicians on the basis of the degree of their agreement about different paragraphs of the consensus , was 0.84 at the end of the first consultation or round . 
the number of disagreements dropped from an overall of 115 , from the first to the second round . table 2 reports the results at the end of the first round and shows the precise indication of agreement / disagreement observed in any statement proposed . the statements that were modified are those evaluated either with i dont agree from almost two interviewed experts , or i completely disagree , even by a single expert . 
 table 3 reports results at the end of the second round . in the paragraph preparation to the examination and modalities of technique , all methods of intestinal cleansing and fecal tagging , available for patients , were listed , because the preference for a specific method depends on the reference center . 
 the use of either room air or co2 for colon distention is considered , since not all centers are equivalent from this point of view . after this first round of consultation , all points of agreement or disagreements were gathered and evaluated . 
as an example , the term neoplastic transformation was modified into if it becomes a tumor . we added a separate paragraph to manage the quick description of the limits of ctc to help the patient ( and the referring physician ) in easily detecting ctc limits during the discussion of the informed consent . 
in this paragraph , in particular , we addressed the issues of low x - ray dose and detection of extracolonic lesions and the potential underestimation of flat lesions . the paragraph the risks of ctc was focused , apart from risk of colon perforation , on vasovagal reactions . the final part of the questionnaire , the same in all versions of the informed consent , is required to guarantee the validity of the consensus , because it is mandatory that patient freely chooses to give his permission to the examination . 
signatures requested at the bottom of the document must be legible . discussion the expert group produced an informed consent model for ctc , with an overall agreement of 93 % . the purpose of writing this consensus was to guarantee maintenance of an acceptable level of technical quality in every center where ctc examination will be performed . 
 to obtain this result , the informed consent to ctc gathered more specialists , working in writing and discussing the text , showing that the standardization process is possible , realizing a document shared and accepted following different integrated opinions . 1 3 904 radiol med ( 2015 ) 120 : 899904 the role of the facilitator and that of the consulted specialists , all members of the section of abdominal and gastrointestinal radiology of the sirm , allowed modifying the paragraphs more critically . the agreement degree was maximum for paragraphs of preparation and technique of the examination presumably because the literature favors the sharing of preparation and technical protocols among virtual colonoscopists . 
radiologists show maximal observance of prescription and they agree with rules and modalities of examination , where the literature is clear , showing maximal clearness and unity of judgement . some minor criticisms were explained on the basis of the excessive brevity of the text : in some experts opinion , this conciseness prevents a correct discussion and description of benefits , risks and limits of the ctc . 
nevertheless , the reduction of the text was essential to make use of the consensus content for all the patients and involved physicians easier and understandable . the need of a partial autonomy for every center , which uses the consensus , was respected . 
in relationship to the intestinal preparation modality and the use of fecal tagging , the text allows some options but the choice is free among them . to optimize the understanding of the italian text , we followed the indications of the literature [ 13 ] to improve the simplicity of the italian text : we used a layout from the left side of the page , simple sentences , briefs , without technical words . 
we substituted expressions as neoplastic proliferation with an easier growing of the tumor , or in simple description of the feeling along the intestinal distension , we used more known terms ( abdominal distension in substitution of abdominal bloating )  . on the same a4 format , we arranged the first part of the text , regarding information to virtual colonoscopy for the patient and the second part , more properly regarding the consent . 
on the second page , the last part , the agreement or disagreement is traced ( i give my consent or i dont give my consent )  . in conclusion , the group of experts was able to produce an informed consent for ctc , hoping that this may be the beginning of the proliferation of similar initiatives , focused on quality assurance in ctc procedures . conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . appendix : contributors duccio buccicardi1 , lapo sali2 , francesca coppola3 , claudio fioroni4 , silvia venturini5 , ignazio salamone6 , massimo galia7 1imaging department , san paolo hospital , savona , italy 2department of experimental and clinical biomedical sciences , university of florence , 50134 florence , italy 3radiology unit , department of digestive disease and internal medicine , s . 
orsola malpighi hospital , bologna , italy 4department of radiology , azienda ospedaliera di perugia , italy 5radiology unit , national cancer institute , aviano , italy 6radiology unit , g . 
the natural outcome is sodium and water retention , intrarenal vasoconstriction , renal failure , and finally death [ 2 ]  . although a consensus exists among investigators with regard to the vasodilation in the splanchnic circulation of cirrhotic patients , reports on the remaining vascular beds are conflicting [ 2 , 3 ] , possibly due to recruiting patients with varying severities of the disease [ 2 ] , or because of deficient methodologies [ 4 ]  . duplex doppler examination is a noninvasive , valid , and reproducible technique for estimating vascular impedance and evaluating arterial blood flow ; and has been widely used in cirrhotic patients with or without ascites [ 5 ]  . 
the resistive 1 3 radiol med ( 2015 ) 120 : 982988 and pulsatility indices ( ri and pi , respectively ) are known as reliable indicators of vascular blood flow in patients with cirrhosis [ 6 ]  . 
pulsatility index , in comparison with ri , is preferred because it is more sensitive in detecting waveform abnormalities ; it is not affected by the angle between the direction of the doppler beam and the blood vessel , yielding a high observer agreement ; and it is along with small interobserver variability in various vascular beds [ 4 ]  . the carotid arteries are important principally by virtue of their major role in the brain blood supply and their contribution to hemodynamic stability on account of the presence of baroreceptors in the carotid sinuses [ 7 ]  . to the best of the authors knowledge , the hemodynamic status in the carotid arteries of cirrhotic patients has not been investigated in the literature . this study sought to compare vascular doppler waveform indices including those obtained from the common carotid arteries between cirrhotic and healthy subjects . materials and methods study design and participants the ethics committee of the tabriz university of medical sciences approved this study . 
a total of 60 patients with biopsy - proven , class - b cirrhosis according to the child turcottepugh classification were enrolled in this prospective , cross - sectional , single - center study . 
blood pressure and heart rate were assessed during doppler ultrasound examination using an automatic sphygmomanometer . the common carotid arteries were examined on both sides with the patient in the supine position and a slight extension of the neck away from the side under examination immediately after a normal expiration . following previously described methods [ 8 ] , the same observer measured pi and ri values in the renal , celiac , and superior mesenteric arteries by doppler ultrasonography . 
in the brachial and common femoral arteries only pi values were measured due to technical limitations . to ensure maximum quality only waveforms with clear envelopes and stable signals were accepted . 
at the time of imaging all subjects were hemodynamically stable and the heart rate was within normal ri = ( maximum minimum velocity ) / maximum velocity pi = ( maximum minimum velocity ) / mean velocity to ensure intra - observer agreement , data from three sets of all measurements in the same session were compared in 15 randomly selected patients . 
due to difficulty in obtaining accurate results from the splanchnic 1 3 984 radiol med ( 2015 ) 120 : 982988 arteries , doppler ultrasonography was preformed after paracentesis in this patient . serum albumin less that 3.5 g / dl was considered hypoalbuminemia . 
the mean pi and ri in the other arteries did not differ significantly between the two groups ( table 2 )  . sample size calculation and statistics controls versus patients with and without ascites at a significant level of 5 % , the power of 90 % , and a standard deviation of 0.07 for pi of the renal arteries in cirrhotic patients [ 10 ] , at least 41 patients were required in each wing to detect at least 0.05 difference between the groups . 
accordingly , no significant difference was found between the two groups . discussion many previous studies have shown hemodynamic changes in patients with cirrhosis , including peripheral arterial vasodilation and vasoconstriction in the renal circulation [ 4 , 1013 ]  . in agreement with these reports , the mean pi and ri in the celiac artery were significantly higher in our healthy subjects as compared with those in cirrhotic patients . 
excessive synthesis and release of local vasodilating factors such as nitric oxide , calcitonin - gene related peptide , endogenous cannabinoids , adrenomedullin , and carbon monoxide ; the presence of an extensive systemic or portosystemic collaterals ; and a poor liver function all have been implicated [ 2 ]  . some authors believe that high diastolic velocities in the splenic arteries take place as an adoptive response to abnormally hypokinetic venous flow in portal hypertension [ 14 ]  . 
due to portal hypertension , splanchnic vascular resistance progressively decreases because of arteriolar vasodilatation or translocation of intestinal bacteria and / or their vasoactive products such as carbon monoxide and nitric oxide [ 2 ]  . 
 at this stage , major endogenous vasoconstricting and sodium - retaining systems such as the reninangiotensinaldosterone system , the sympathetic nervous system and antidiuretic hormone ( adh ) become activated and consequent renal vasoconstriction and sodium and fluid retention develop [ 15 ]  . despite the presence of a partial consensus on hemodynamic changes in the splanchnic vasculature , reports regarding the status of blood flow in the extremities of cirrhotic patients are conflicting [ 16 ]  . 
they demonstrated an enhanced shear stress - induced peripheral vasodilation in patients with cirrhosis . we did not find a significant difference between the two groups with and without cirrhosis for the mean pi values in either the brachial or femoral arteries . 
it has been suggested that arterial vasodilation in peripheral vessels such as the brachial and femoral arteries cannot be induced under resting conditions unless a physiological stimulus of shear stress is instigated [ 12 ]  . 
concomitant renal failure [ 18 ] and different classes of cirrhosis [ 13 ] may also contribute to this heterogeneity . hepatorenal syndrome , which is the development of renal failure in the absence of any identifiable causes of renal pathology , is a frequent finding in patients with advanced cirrhosis with an estimated frequency of 40 % [ 19 ]  . 
this syndrome with extremely constricted renal vasculature , significant reduction of renal blood flow and diminished glomerular filtration rate ( gfr ) is the most severe complication of cirrhosis [ 2 ]  . 
it is along with low arterial pressure , significant sodium and water retention , high blood level of renin , antidiuretic hormone , and norepinephrine , and elevated renal vascular resistance [ 20 ]  . 
 it is thought that the hepatorenal syndrome takes place because of vasoconstriction of the renal circulation , which is a compensatory physiologic response to intense systemic arteriolar vasodilatation secondary to splanchnic pooling of blood [ 10 , 19 , 21 , 22 ]  . 
in other words and briefly , this syndrome is a consequence of disturbances in the systemic activation of vasoconstrictors and the local synthesis of vasodilators [ 23 ]  . renal doppler of interlobar arteries has been found as an accurate , noninvasive method for detecting renal hemodynamic disturbances in cirrhotic patients at very early stages , even when clinical manifestations are not emerged [ 24 ]  . 
according to available data , cirrhotic patients have considerably higher renal ri and pi compared with their healthy counterparts [ 2 , 10 , 22 , 25 , 26 ]  . 
a direct connection between renovascular impedance and the severity of cirrhosis , refractory ascites and mortality has been also reported [ 10 , 24 ]  . in line with previous reports , the mean renal pi and ri were significantly higher in our cirrhotic patients compared with those in the control group . at initial stages of the disease , vasoconstriction in efferent arteries causes decrease in renal blood flow , which is more striking than the fall in gfr . 
 1 3 radiol med ( 2015 ) 120 : 982988 prostaglandins , nitric oxide , kinins , and natriuretic peptides are the main intrarenal vasodilators that contribute to maintain renal blood flow and activation of the main vasoactive systems in cirrhotic patients [ 27 ]  . 
in addition to renal vasoconstriction , concomitant interstitial nephritis or vacuities particularly in those with cirrhosis secondary to infectious etiologies [ 30 ] , and destruction of renal vessels , which is evident in hepatorenal syndrome , may also underlie renal pathogenesis in cirrhosis [ 25 ]  . to the best of the authors knowledge there is no doppler ultrasonographic study on the carotid arteries in cirrhosis . 
 hemodynamic changes in the carotid arteries are of critical importance from two aspects : ( 1 ) the carotid arteries are main blood suppliers to the brain ; and ( 2 ) the most important arterial baroreceptors are located in the carotid sinus at the bifurcation of external and internal carotids [ 31 ]  . the mean carotid pi and ri were significantly lower in our cirrhotic patients than in healthy controls . 
an inverse , albeit insignificant , correlation between these parameters and pi and ri in the celiac arteries , as well as an observation of insignificant correlations between pi and ri in the carotid arteries and renovascular impedance may indicate that the baroreceptors are intact in the carotid sinuses [ 32 , 33 ] and they act independent of renal regulation at least in our class of patients . in line with previous reports [ 2 , 11 , 18 ] , we found significant differences between cirrhotic patients with and without ascites in terms of vascular impedance values in the renal , celiac and carotid arteries . 
according to previous data , however , inter - observer variability of pi and ri measurements in various vascular beds in cirrhosis is small , especially when the observer is experienced [ 36 ]  . while some studies have found good correlations between child class and renal hemodynamic changes in cirrhotic patients [ 28 , 37 ] , such associations with other splanchnic and extrasplanchnic vascular hemodynamics are probably different [ 13 ]  . 
to draw a solid conclusion in this regard , however , future studies including class a and c patients are recommended . while hemodynamic changes in cirrhotic patients might be of great prognostic value [ 38 ] , the common carotid artery , as a major central trunk with consequential clinical influences in the body [ 39 , 40 ] , has not been adequately examined in this regard . 
although investigation of such clinical contributions was out of the scope of the present study , our findings could pave the way for relevant researches in the future . finally , hemodynamic status in the venous districts has been attributed to physiopathology of arterial hemodynamic changes [ 2 ]  . 
2 test , students t test and analysis of covariance were used for comparison of variables . results in the study group , 58 over 77 patients had a successful outcome ( responders )  . 
moreover , in the same group was present a statistically significant discs shrinkage in the sixth month of follow - up ( p < 0.05 ) as showed by idva . conclusions t2 shine - through effect in dwi is present before morphological disc reduction and moreover could be considered as a predictive sign of response to oxygen ozone treatment . keywords diffusion - weighted imaging ( dwi ) apparent diffusion coefficient lumbar disc herniation chemiodiscolysis with oxygenozone mixture percutaneous discolysis m . 
gallucci e - mail : massimo.gallucci@cc.univaq.it 1 3 942 introduction about 80 % of adults suffer from low back or leg pain [ 13 ] and 4 % of these patients have a lumbar disc herniation [ 4 ] , with l5 and s1 nerve roots involved in approximately 95 % of cases [ 57 ]  . 
in two - thirds of cases , the herniated portion of the disc tends to regress , with partial or complete resolution after 11 months with conservative therapy [ 8 ]  . 
the basic principle of action of intradiscal injection of oxygenozone mixture , is the reduction of proteoglycans [ 11 ] , consequent dehydration and shrinkage of the disc ; moreover the histological changes include micro and macrovacuolar degeneration with small halos of necrosis and interstitial oedema [ 12 , 13 ]  . 
diffusion - weighted imaging ( dwi ) sequence , already used in the evaluation of water diffusivity of the discs treated with ozone nucleolysis [ 15 ] , may have application in the evaluation of micro and macrovacuolar degeneration induced by ozone ; in fact , in our previous study we showed that these histological changes of the disc are not evident from the base sequences t1 and t2 [ 15 ] weighted . 
therefore , in this study , we take into account the t2 shine - through effect in dwi for evaluating these changes and predicting shrinkage of lumbar disc herniation after o2o3 discolysis . materials and methods patients between july 2012 and february 2014 , a total of 172 patients were selected for prospective double - blind trial approved by the medical ethical committee of our institution . 
a clinical neuroradiologist with 30 years experience administered to all patients visual analog scale ( vas ) [ 16 ] questionnaire ranging from 0 to 10 at the presentation and subsequent follow - up at second , fourth , and sixth month classifying as successful if the pain value was no greater than 2 , and unsuccessful otherwise . radiol med ( 2015 ) 120 : 941950 injection technique the procedures were performed by two interventional neuroradiologists ( 35 and 5 years experience ) , under ct guidance ( somatom plus 4 ; siemens medical systems , erlangen , germany ) after intravenous premedication with 1 g of cefuroxima ( curoxim ; glaxosmithkline ) and 50 mg of ranitidine ( zantac : glaxosmithkline )  . 
sagittal se - t1 - wi images were acquired with 500 / 20 / 2 ( tr / te / nex ) and with same remaining parameters of sagittal fse - t2 and t2 fat - wi . 
dwi were obtained in sagittal and axial plane using isotropic multishot spin - echoplanar mr imaging with 1215 / 80 / 6 ( tr / te / nex ) , matrix , 128 for obtaining a good signal to noise ratio [ 17 ] and 128 with the same slice thickness , spacing and fov of t2 and t1 - weighted images . 
the dwi images were acquired with a b value of 0 and 400 s / mm2 for minimizing diffusion - related loss of signal intensity in disc tissue and subsequent inaccuracy in adc measurement [ 18 , 19 ]  . qualitative and quantitative image analysis two neuroradiologists , respectively , 25 and 6 years experience , blinded to the patients administered drugs , independently reviewed mr images . 
the t2 shine - through effect was identified in dwi images when compared to corresponding adc maps with a 3point scale : ( a ) absence ; typically patients with dehydrated discs . 
for 11 patients from the study group , no matching control subject could be found , resulting in 66 matched pairs ( table 1 )  . data and statistical analysis the intra and interobserver reliability of the mri evaluations for qualitative analysis was estimated using agreement percentage and kappa statistics according to landis and koch [ 21 ]  . 
in this case , before percutaneous treatment , dwi and adc map do not show hyperintense signal indicative of t2 shine - through effect 1 3 944 radiol med ( 2015 ) 120 : 941950 fig . 
3 axial t2 ( 1 ) , corresponding dwi image ( b value 400 ) ( 2 ) and adc map ( 3 ) show the case 3 ; 39 years - old woman with a low back pain due to protrusion bulging disc in l4l5 with associated spinal canal stenosis . 
these images , and in particular dwi image ( b value 400 ) ( 2 ) and adc map ( 3 ) do not show discal microcystic areas after o2o3 therapy but only homogeneous and normal t2 signal disc . 
fse t2 - weighted mr image ( 2 ) shows entire disc and herniated parts included in the roi for idva analysis coefficients ( icc ) and by calculating the mean difference between raters and the 95 % confidence interval ( ci )  . 
all analyses were also performed using multiple logistic regression analysis and analysis of covariance to check for the influence of age , sex , injection level , bmi and herniation volumes as covariates . 
in the fourth month after treatments , dwi signal was also different with statistical significance ( 2 73.10 , p < 0.001 ) ; significant dwi signal score 2 was present in 27 ( 35.06 % ) responders of study group patients , but it was also found a significant dwi signal score 1 in 24 ( 31.16 % ) non - responders of 77 control group patients and a significant dwi signal score 3 in 24 ( 31.16 % ) non - responders of 77 control group patients ( table 2 )  . 
this mri follow - up showed the significant presence of dwi signal score 1 in 27 responders ( 35.06 % ) and 38 non - responders ( 49.35 % ) out of 77 patients of the control group ( 95 % ci ) ( table 2 )  . 
the images and in particular mr - dwi ( 2 ) and corresponding adc map ( 3 ) show the average water diffusivity of the annulus fibrosus and nucleus pulposus with hyperintense signal within the disc compatible with t2 shine - through effect classified as dwi signal score 2 yielded by the overall analysis . 
in these 66 pairs , dwi signal score 2 was more common in the mri follow - up of the study group and in particular in the sixth month after ozonolysis ( 2 117.02 , p < 0.001 , effect size 0.65 , good power 0.86 ) ( table 2 )  . 
the mean interobserver differences for the measurements of disc volume were less than 1 mm3 while 3 mm / for the adc measurements were less than 3 sec in the mri follow - up . 
 no statistically significant difference was detected in adc measurements between responders and non - responders groups during follow - up ( p > 0.05 ) ( table 4 )  . diagnostic performance of t2 shine - through effect in dwi diagnostic accuracy , sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) of t2 shine - through effect are detailed in table 5 . 
in the study group , 35 patients ( 45.45 % ) between responders and non - responders showed t2 shine - through effect in the second month follow - up and significant volume reduction of the hernia in the sixth month follow - up ( table 5 )  . 
in the control group , none of 6 ( 7.79 % ) patients with dwi signal 2 score at the second month of follow - up recovered instead of 3 ( 3.89 % ) patients with dwi signal score 3 and 27 ( 35.06 % ) patients with dwi signal score 1 . 
in the subsequent fourth mri follow - up , we observed in particular an increment of sensibility ( 95.4 % ) in the ability of dwi to highlight the response to treatment . 
in this mri follow - up the area under the receiver operating characteristic curve ( auc ) was 97.7 % for identifying responders in study group ( table 5 )  . 
in the sixth mri follow - up , t2 shine - through effect was detected in fiftythree of 77 study group patients ( 68.8 % ) in comparison to 2 of 77 ( 2.59 % ) patients in the control group . 
the dwi sequence obtained , in the study group , sensitivity of 98.1 % , specificity of 83.2 % with an area under the receiver operating characteristic curve ( auc ) of 98.7 % ( table 5 )  . discussion in this work , in the study group fifty - eight out of 77 patients ( approximately 75 % ) had successful outcomes 1 3 948 radiol med ( 2015 ) 120 : 941950 1 3 radiol med ( 2015 ) 120 : 941950 ( the responders ) while nineteen patients showed unsatisfactory results ( the nonresponders ) in a follow - up period of 6 months . 
dwi sequence , already used in the evaluation of water diffusivity of the discs treated [ 14 ] , has application for predicting shrinkage of herniation ; in addition we have tried to show that , the t2 shine - through effect in dwi may be useful in evaluating micro and macrovacuolar degeneration with small halos of necrosis and interstitial oedema [ 11 , 12 ] as a predictive sign of shrinkage of disc herniation . 
we observed an increment of signal intensity in dwi images of the treated discs with ozonolysis confirmed as t2 shine - through effect in adc map in the first mri follow - up . 
furthermore , in the sixth month of mri follow - up , there was the presence of statistical significance t2 shine - through effect in 53 out of 58 responders of study group patients and absence in 38 non - responders out of 77 control group patients confirming the pharmacological actions of o2o3 mixture on the discs [ 12 , 13 ]  . 
the limit of the our study is the use of single shot echo - planar imaging ; in fact some studies show that many diffusion mr imaging with these techniques , are not useful for spine imaging because of the inhomogeneous magnetic environment and the high lipid content of the vertebral bodies that can lead to strong geometric distortions and chemical shift artifacts [ 22 ]  . 
it would be very interesting eventually to correlate anisotropy with the severity of degenerative change to determine if there are significant changes in diffusion anisotropy in discs at different stages after ozone therapy as reported by same authors [ 23 ]  . conclusions we report a statistically significant increment of t2 shinethrough effect , in the study group from the second mri follow - up after percutaneous treatments with ozonolysis . 
therefore , we could say that in the treated discs , the presence of t2 shine - through effect provides additional diagnostic information about the water diffusivity and predicts shrinkage of lumbar disc herniation ; furthermore it may be useful in clinical practice when qualitative assessment of dwi during imaging interpretation by radiologists is of critical importance because quantitative analysis of dwi requires additional time . conflict of interest the authors declare no conflict of interest . ethical standards this article contains research involving human participitants . 
four intrapancreatic isodense nodules in three patients were undetected on cect . conclusion the described patterns of fdg uptake findings may be helpful for a better characterisation of pancreatic metastases although semiquantitative analysis using suvmax could not be used as a criterion for differentiating pancreatic metastases from primary pancreatic cancer . 
 thus , it is a useful adjunct to the described features on ct . keywords pancreatic metastasis pancreas 18f - fdg - pet / ct contrast - enhanced ct introduction pancreatic involvement by metastasis from other primaries is rare , and accounts for approximately 24 % of pancreatic tumours [ 13 ]  . 
the importance of detecting pancreatic metastases and differentiating them from pancreatic adenocarcinoma is underlined by the disparity in management of patients with 1 3 888 radiol med ( 2015 ) 120 : 887898 primary and secondary pancreatic tumours [ 2 , 4 ]  . 
therefore , it is important to distinguish pancreatic metastases from the more common pancreatic adenocarcinoma for adequate patient management . recent reports have documented the value of computed tomography ( ct ) and magnetic resonance imaging ( mri ) in showing the presence of pancreatic metastases [ 3 , 5 , 6 ]  . 
to our knowledge , the fluorodeoxyglucose positron emission tomography / computed tomography ( fdg - pet / ct ) findings of pancreatic metastases have been rarely reported [ 711 ]  . 
in this paper , we illustrate the fdg - pet / ct findings in 19 cases of pancreatic metastasis , including the patterns of fdg accumulation and the ct characteristics of pancreatic metastasis . materials and methods the study protocol conforms to the ethical guidelines of the 1975 declaration of helsinki ( 6th revision , 2008 ) as reflected in a priori approval by the institutions human research committee . 
informed consent was obtained from each patient included in the study . patient population we searched the medical database of our institution between august 2010 and december 2013 and found 42 patients with suspected pancreatic metastatic lesions who had fdg - pet / ct scans available for review . 
image fusion of pet and ct data , as well as postprocessing , was performed using a multi - modality workstation . ct examinations ct examinations were performed for 14 patients using a lightspeed vct 64 ( ge medical systems , milwaukee , wi , usa ) or a brilliance 16 scanner ( philips medical system )  . 
six patients underwent dual - phase ct scans including arterial and portal venous phase , whereas the other eight underwent triplephase ct including arterial phase , pancreatic phase and portal venous phase . 
the delay times of arterial , pancreatic and portal venous phase were 25 , 3545 and 6575 s , respectively , from the beginning of the intravenous infusion . imaging analysis all 18f - fdg - pet / ct images were qualitatively and semiquantitatively interpreted by two experienced nuclear medicine physicians independently , and differences in assessment were resolved through consensus . qualitative imaging analysis visual analysis of pet , ct and petct fused images was performed on the multi - modality workstation in axial , coronal , and sagittal projections . 
the pet / ct scans were compared with the corresponding ct images for accurate localisation of the tumours , and a consensus was reached for each scan ; ( 2 ) the fdg uptake pattern of the pancreatic lesions and ( 3 ) lymphadenopathy , vessel and presence of extrapancreatic involvement . semiquantitative imaging analysis the number and size of pancreatic lesions were recorded by measuring the maximum diameter ; the maximum standardised uptake values ( suvmax ) on 1 h routine scan was obtained . 
histological confirmation by surgical resection of the tumour ( n 3 ) , including two patients who underwent pancreatoduodenectomy and one a distal pancreatectomy and splenectomy ; endoscopic ultrasonography - fine - needle aspiration ( eus - fna , n 11 ) was taken as the gold standard in 14 patients , whereas the other five patients were confirmed by clinical and imaging follow - up ( including doppler sonography , ct or mri )  . statistical analysis mean standard deviation and range were used as descriptive statistical analysis . 
fdg - pet / ct scan ( a axial ct , b pet , c fused pet / ct image , d maximum intensity projection image ) demonstrates marked hypermetabolism ( suvmax , 11.5 ) in the head of the pancreas ( long arrow ) , as well as hepatic ( l ) and l1 vertebral metastases ( short arrow )  . 
2 a 57 - year - old male with gastric adenocarcinoma , fdg - pet / ct scan ( a ct , b pet , and c fused pet / ct ) detected multiple nodular lesions in the pancreatic body and tail tending towards confluence . 
four lesions in three patients ( cases 4 , 7 and 16 ) had a size range 0.81.6 cm and were missed on cect contrastenhanced ct findings in patients with primary pancreatic carcinoma cect detected all the 20 primary pancreatic cancer lesions . 
distal parenchyma atrophy occurred in 6 / 20 ( 30 % ) patients , dilatation of the main pancreatic duct was observed in 14 / 20 ( 70.0 % ) cases , and seven ( 35 % ) patients had involvement of extrapancreatic arteries and veins . 1 3 radiol med ( 2015 ) 120 : 887898 fig . 
pet / ct scan ( a transverse ct , b corresponding pet , and c fused images ) shows segmental fdg uptake in the pancreatic body and tail ( arrows )  . 
d a maximum intensity projection ( mip ) pet image shows multiple hypermetabolic lesions in the bilateral adrenal gland , axillary lymph nodes , abdominal and pelvic cavity and subcutaneous tissue . 
pet / ct scan ( a transverse ct , b corresponding pet , and c fused images ) demonstrated a small fdg - avidity in the body of the pancreas ( arrows )  . 
pancreatic metastasis was confirmed by histopathology following pancreatoduodenectomy discussion in most studies , the most commonly reported primary tumours metastasising to the pancreas are lung , gastrointestinal tract , kidney , breast tumours , colorectal cancer , and hepatobiliary tract cancer and melanoma . 
the key aims of this study , therefore , were to evaluate the imaging characteristics and specific patterns that may facilitate the diagnosis of pancreatic metastases in the future . 18f - fdg - pet / ct , as a whole - body scan , is a powerful tool for oncology imaging ; fdg - pet can show simultaneous accumulation in the primary tumour and extrapancreatic lesions and provide additional value to ct in differentiating secondary from primary pancreatic lesions for whole - body scanning . 
in our series , three pancreatic lesions initially missed on cect were detected as areas of fdg high uptake on pet / ct . metastatic tumours to the pancreas are uncommon , even though autopsy data indicate that a wide variety of primary three types of metastatic involvement of the pancreas have been described in the literature : a solitary mass , 1 3 radiol med ( 2015 ) 120 : 887898 fig . 
5 a 59 - year - old male was found to have a pancreatic body lesion 2 years after resection of hepatocellular carcinoma on the pet / ct scan , a transverse ct showed a hypodense area in the pancreatic body , b fused pet / ct images showed nodular fdg uptake in the corresponding location , contrast - enhance ct scan c arterial phase and d portal venous phase demonstrated homogeneous enhancement . 
the last pattern was the least frequent ( 10.5 % ) , and was given by a segmental infiltration of the pancreas , leading to a segmental enlargement and high fdg uptake of the pancreas . these fdg uptake patterns were nonspecific and can be seen in many pancreatic entities [ 16 ]  . 
the most common pattern in our study ( 12 / 19 , 63.2 % ) , a solitary lesion with high fdg uptake , may resemble the more common pancreatic adenocarcinoma . 
our study suggested that pancreatic metastases had slightly higher fdg uptake than primary pancreatic cancer , but it was difficult to distinguish them on the basis of their suvmax . pancreatic metastases may also have certain features on cect that are more characteristic of metastatic tumours than of primary ductal pancreatic adenocarcinoma . 
pancreatic metastases from renal cell carcinomas are often described as hypervascular 1 3 896 radiol med ( 2015 ) 120 : 887898 1 3 radiol med ( 2015 ) 120 : 887898 fig . 
6 a 73 - year - old female presented to our hospital for 2 months abdominal papet / ct scan ( a mip image , b transverse ct , c corresponding pet image , d fused pet / ct ) demonstrates focal area of increased fdg uptake in the uncinate process of the pancreas ( long arrow ) ; the contrast - enhanced ct ( e arterial phase , f pancreatic phase and g portal venous phase ) demonstrates a poorly defined hypoattenuating lesion . 
most other metastases are typically hypovascular , showing homogeneous enhancement with delayed fillthe primary pancreatic cancer lesions were hypoattenuating with homogenous or heterogeneous enhancement after contrast agent injection . cect visualises other morphological features that can help to differentiate pancreatic metastases from primary carcinoma . 
our study found the distal parenchyma atrophy was found in six ( 33.0 % ) cases of pancreatic carcinoma , but no case of pancreatic metastases showed the same sign . 
by combining the fdg uptake pattern , extrapancreatic findings , lesion enhancement and primary tumour history , we might achieve a more dependable diagnosis . solitary or multiple patterns may mimic functional pancreatic endocrine tumours on pet / ct imaging [ 19 , 20 ]  . 
 when hypervascular pancreatic lesions are depicted on cect , it is difficult to distinguish between the two lesions , and a ct - guided biopsy need be performed . segmental patterns may mimic autoimmune pancreatitis . 
the lack of a true gold standard in some of the cases may have introduced bias in the analysis of this study . in conclusion , we found that three fdg uptake patterns in pancreatic metastases were detected on pet / ct , including solitary , multiple and segmental patterns . 
pancreatic metastases can be diagnosed by carefully evaluating different patterns in pet / ct and cect features , and often the combination of signs is highly suggestive of the right diagnosis . 
the described patterns of fdg uptake findings may be a useful adjunct to the described features on cect and useful for differential diagnosis with other pancreatic lesions . acknowledgments this study was supported by the national nature science foundation of china , no . 
two radiologists at baseline hrct distributed 70 patients with fibrotic iip into three groups on the basis of the 2011 guidelines : uip pattern ( group 1 ) , possible uip pattern c . 
the different abnormalities ( honeycombing , reticulation , groundglass and traction bronchiectasis ) , fibrotic score ( reticulahoneycombing ) and overall ct score were visually tion scored at baseline and during the follow - up ( total hrct 178 )  . 
in group 1 , baseline honeycombing rate higher than 25 % , fibrotic score higher than 30 , overall ct score greater than 45 and traction bronchiectasis in more than 4 lobes defined the worst prognosis . conclusion hrct classification based on 2011 guidelines showed high accuracy in stratifying fibrotic changes because in our study uip , possible uip and inconsistent with uip pattern seem to be correlated with different disease progression and mortality rate . idiopathic interstitial pneumonia usual keywords interstitial pneumonia ( uip ) idiopathic pulmonary fibrosis ( ipf ) prognosis p . 
sbragia 1st radiology unit , university hospital of pisa , via paradisa 2 , 56124 pisa , italy e - mail : p.sbragia@med.unipi.it idiopathic pulmonary fibrosis ( ipf ) is defined as a specific form of chronic progressive fibrosing interstitial pneumonia introduction 1 3 radiol med ( 2015 ) 120 : 930940 of unknown cause occurring primarily in older adults , limited to the lungs [ 1 , 2 ]  . 
the american thoracic society and the european respiratory society ( ats / ers ) [ 1 ] published an international consensus statement on the diagnosis and treatment of this disease in 2000 . 
 the ats / ers 2002 statement [ 2 ] included ipf among the seven diseases defined as idiopathic interstitial pneumonias ( iips ) and detailed the specific clinical , radiologic and histologic features . 
a recent update of the classification included ipf among the major idiopathic interstitial pneumonia , together with insip , rb - ild , dip , cop and aip [ 3 ]  . surgical lung biopsy and pathological pattern of uip are able to predict the mortality rate and the long - term outcome in patients with ipf [ 4 , 5 ]  . 
nevertheless , surgical lung biopsy is not frequently performed due to sampling problems [ 6 ] and to possible complications in patients with more advanced disease [ 710 ]  . 
the positive predictive value of a hrct diagnosis of uip is high , but in patients whose hrct does not demonstrate a uip pattern , surgical lung biopsy may still demonstrate uip pattern on histopathology . 
recently , was suggested that surgical lung biopsy sampling might not be necessary also in patients with possible uip pattern on hrct [ 16 ]  . this is a new approach with respect to 2002 recommendations [ 2 ] which stated that the histologic patterns provide the primary basis for the various categories of iip and that a highly probable diagnosis of ipf can be made without a lung biopsy , whereas a definitive diagnosis can be established only with the aid of a surgical lung biopsy . 
estimated overall extent of lung abnormality was 65 % ; predominant features are honeycombing ( black arrow ) , reticulation ( white arrow ) , and bronchiectasis ( arrowhead ) impact of the new guidelines on the estimation of prognosis and life expectancy of patients with ipf has not been evaluated yet . on the basis of the concept that in a clinical classification diagnosis is prognosis [ 6 ] , the objective of this study is to determine whether hrct criteria for uip , possible uip or no - uip pattern recommended by ats / ers / jrs / alat 1 3 932 radiol med ( 2015 ) 120 : 930940 guidelines 2011 are able to predict progression and prognosis of the disease in a group of patients with fibrotic iip . materials and methods patients selection one hundred forty - four patients consecutively admitted at cardiothoracic dept . , university hospital pisa , italy , from january 1996 to february 2012 with a previously made diagnosis of fibrotic interstitial lung disease , in which the diagnosis of ipf was not excluded , were retrospectively evaluated . 
seventy - four patients were excluded through multidisciplinary discussion , due to the following : chemotherapy - related and postradiation therapy pneumonia , environmental exposure , clinical and serologic evidence of collagen vascular disease , history of ards or sarcoidosis . 
we also excluded patients who did not complete clinical and radiological follow - up , patients with lung cancer and without definitive diagnosis of interstitial lung disease . all 70 patients included in the study received a diagnosis of fibrotic iip based on the clinical manifestations and presence of an hrct pattern showing reticular opacities and / or traction bronchiectasis in association with honeycombing or ground - glass opacities on the basis of american thoracic society and european respiratory society international consensus statement 2002 [ 2 ]  . 
the videoassisted thoracic surgery lung biopsies were available in nine patients . this was a retrospective study and has received the approval of the ethics committee , with no prescription about the patients informed consent . methods pulmonary function tests such as percentage of predicted slow vital capacity ( svc ) , forced vital capacity ( fvc ) and diffusing capacity of the lungs for carbon monoxide ( dlco ) , blood gas analysis , 6 - min walking test , bronchoscopy , bronchoalveolar lavage , differential cell count , chest x ray and hrct were performed at the first visit and during the follow - up at variable time intervals . all the patients included in the study had hrct examination with 1.0 - mm - thick sections at 1 - cm intervals throughout the entire lung during inspiratory apnoea in the supine position . 
estimated overall extent of lung abnormality was 15 % ; predominant features are reticulation ( arrowhead ) and ground glass ( white arrow ) 1 3 radiol med ( 2015 ) 120 : 930940 two thoracic radiologists with 25 and 15 years of experience , belonging to a multidisciplinary group composed by pneumology , radiology and pathology specialists , blindly and independently examined the baseline and follow - up hrct scans ( total n 178 ) in separate sessions and made a subjective visual assessment , in percentage ( % ) of the total lung sections of the overall extent of the pulmonary parenchymal abnormalities ( overall ct score ) , approximated to the nearest 5 % according to shin et al . 
the extent of ground - glass opacity , reticulation and honeycombing were similarly scored , in such a way that the sum of these abnormalities corresponded to the overall extent of the interstitial involvement . 
the uip pattern was characterized on hrct by all the four features : the presence of honeycombing with or without traction bronchiectasis , reticular abnormalities , subpleural and basal predominance and the absence of features listed as inconsistent with uip pattern . 
the possible uip pattern was characterized by all the three features listed below : reticular abnormality , subpleural basal predominance and the absence of features listed as inconsistent with uip pattern . 
 the features listed as inconsistent with uip are : upper or mid - lung predominance , peribronchovascular predominance , extensive groundglass abnormality , profuse micronodules , discrete cysts , diffuse mosaic attenuation / air trapping , consolidation in bronchopulmonary segment ( s ) / lobe ( s )  . 
survival in the three groups of patients was compared using the log rank test and displayed using kaplanmeier curves [ 24 ]  . in the patients belonging to uip group we evaluated , for each abnormality with age - corrected cox regression analysis [ 24 ] the more accurate threshold to differentiate patients with different life expectancy and compared the different survival curves . 
cox proportional hazard models were constructed for honeycombing , reticulation , ground glass , overall ct score and fibrotic score thresholds ranging from 5 to 45 , in increments of 5 . 
 the distribution of overall ct score and traction bronchiectasis was not significant . the overall follow - up was 3029 days , ( mean follow - up 1386 days , ds 915 , range 730 days )  . 
the total number of hrct observed in the 70 patients was 178 , 103 for group 1 , 37 for group 2 and 38 for group 3 . time distribution of overall ct score is shown in fig . 
the a series of possible thresholds , which better differentiate patients with different life expectancy , was found in group 1 3 936 radiol med ( 2015 ) 120 : 930940 fig . 
c , d hrct images of a patient belonging to possible uip group at the baseline ( c ) and after 2 years of follow - up ( d )  . 
the aim of our study is in line with this strategic prospective . the currently accepted iip classification derives from the 2002 ats / esr consensus [ 2 ] and from the 2013 update [ 3 ] , but there is wide experience that patients do not fit into ats / esr categories and the categorization of the fibrotic disease is often problematic for clinicians , radiologists and pathologists [ 25 ]  . idiopathic pulmonary fibrosis is the most frequently seen severe disorder in the iip group , with a prognosis worse than that of many cancers , and it is the more important condition to rule out . 
the new ats / esr / jrs / alat [ 15 ] guidelines have evidenced hrct as an essential component of the diagnostic pathway in ipf and have defined the criteria for uip pattern , possible uip pattern and inconsistent with uip pattern . 
the latter categorization [ 15 ] seems easier to use , is potentially more reproducible than the 2002 classification and may have a significant prognostic value , even without lung biopsy . in our study , hrct has been used to characterize ipf according to the 2011 ats / ers / jrs / alat statement . 
the role of hrct has been evaluated to identify the uip pattern to recognize progression of the different abnormalities and to predict mortality . the hrct abnormalities were simply scored to the nearest 5 % of parenchymal involvement based on the percentage of lung parenchyma that showed evidence of each abnormality . 
it was obtained evaluating the hrct time ( years ) overall ct score <= 45 overall ct score > 45 time ( years ) honeycombing <= 25 honeycombing > 25 time ( years ) bronchiectasis lobes <= 4 bronchiectasis lobes > 4 fig . 
7 multivariate cox regression curves for patients of group 1 with overall ct score above and below 45 ( a ) , for patients with honeycombing score above and below 25 % ( b ) , and for patients with traction bronchiectasis in more and less than 4 lobes ( c ) sections ( 2030 images ) and the results were determined in order of minutes . on the contrary , the difficulty to diagnose ipf on the basis of the hrct and to distinguish uip from nsip and other interstitial patterns , such as classified in 2002 and 2013 consensus statement , is well known in the literature 1 3 938 radiol med ( 2015 ) 120 : 930940 [ 28 ]  . 
 [ 29 ] , the level of agreement on the definition of uip and nsip pattern between the hrct readers has been fair to moderate and , as stated by sverzellati et al . 
 [ 30 ] , thin - section ct findings in patients with ipf overlap with those of other chronic interstitial lung diseases , particularly nsip , chronic hypersensitivity pneumonitis or sarcoidosis ; as much as 62 % of biopsy - proved ipf was regarded as alternative diagnoses in his study . in our experience , the difference of distribution of honeycombing , reticulation and ground glass , the subpleural and basal predominance , the absence of features inconsistent with uip , allowed for an easy and reproducible categorization of the fibrotic disorder on the basis of 2011 consensus statement , with a significant prognostic implication . 
this result is in apparent conflict with the view taken by raghu [ 16 ] in which 79 out of 84 patients with possible uip pattern on hrct have had a biopsy confirmation of uip . 
in this paper , however , no data are provided on the prognosis and evolution of these subjects , which , free of honeycomb by definition , may express a less advanced and / or less progressive ipf . 
a threshold honeycombing score of 25 % , a threshold fibrotic score of 30 % , a threshold overall ct score of 45 % and traction bronchiectasis in more than 4 lobes were able to determine a major or minor life expectancy in multivariate and / or univariate analysis . 
as mentioned in ats / ers / jrs / alat statement 2011 [ 15 ] , several groups have demonstrated that the extent of fibrosis and honeycombing on hrct are predictive of survival in ipf . 
 [ 27 ] study , ct features predictive of a worse outcome were coarse reticulation , honeycombing traction bronchiectasis and overall extent of parenchymal abnormality , whereas lee et al . 
 [ 19 ] in 2012 showed on univariate and multivariate analysis that the overall extent of parenchymal abnormalities was a prognostic factor predictive of poor survival duration in fibrotic interstitial pneumonias with little honeycombing . 
however , our hrct analysis first demonstrated the different time progression of overall ct score , fibrotic score and individual abnormalities in the three iips groups determined on the basis of the ats / ers / jrs / alat 2011 guidelines . 
in particular , in the uip group , the time progression of honeycombing , fibrotic score and overall ct score was demonstrated and increased about 23 points / year , more than in no - uip patients , whereas only bronchiectasis progressed significantly in the possible uip group , ( table 2 )  . 
 [ 19 ] showed on serial scan that honeycombing and reticulation progressed in extent and ground glass decreased differently in uip and in fibrotic nsip . finally , our study seems to indicate the utility and the accuracy of the classification based on the 2011 statement which emphasizes the role of hrct and gives the opportunity to verify the progression and the mortality rate considering three different patterns ( uip type , possible uip and inconsistent with uip ) on the basis of simple morphologic ct criteria , obviating surgical biopsy in many cases . our study had some limitations . first , the study is retrospective and the hrct examinations were not homogeneous for ct scanner and technical parameters . the second limitation is that the surgical lung biopsies were available only for nine patients , due to the potential risks associated with this procedure , which are often greater than the attended benefit . the third limitation is that during the follow - up , the ct scans were not performed at regular time intervals and the functional parameters and dlco were not available at the same time , so that a reliable confrontation with ct as regard to the evaluation of progression and prognosis of ipf was not possible . conclusion hrct classification based on ats / ers / jrs / alat 2011 guidelines showed high accuracy in stratifying fibrotic changes because , in our study , uip , possible uip and inconsistent with uip pattern seem to be correlated with different progression and mortality rate of fibrotic iip . as a consequence , is possible to stratify the risk of individual patient on the basis of belonging to one of the 1 3 radiol med ( 2015 ) 120 : 930940 three groups and , among the uip - type group subjects , on the basis of the extent of the abnormalities presented , even without biopsy confirmation . 
borghi radiologia ospedale , valduce , como , italy 1 3 920 radiol med ( 2015 ) 120 : 919929 conclusion cct is performed with different workloads in participating centers . 
it is a safe procedure and its results have a strong impact on patient management . keywords heart diseases coronary artery cardiac ct indications registry forty - seven sites were involved in this multicenter and multivendor registry . 
the aims were to evaluate the clinical indications , the spectrum of acquisition protocols , the impact on clinical decision - making and the safety profile of cardiac ct . introduction cardiac computed tomography ( cct ) is now an established diagnostic tool for cardiac diseases and coronary artery disease ( cad )  . 
this is the result of several years of ongoing technical development and protocol optimization combined with improved international guidelines and appropriateness criteria that cover a wide spectrum of clinical indications [ 17 ]  . the number of hospitals and imaging centers that perform cct investigations has been constantly growing as is the number of patients that undergo the test . 
however , most clinical information about the use and diagnostic performance of cct derives from relatively few large - scale clinical trials or from selected populations enrolled in highly specialized centers . 
there are currently position statements , recommendations and guidelines on the clinical use of cct and some documents on appropriateness upon which the various centers base their activities [ 811 ]  . the italian registry of cct is an open - access forum ( no restriction criteria or proof of specific competence is required from participating centers ) which was set up to provide a national overview of cardiac ct utilization that offers a more radiological view of the current clinical role of cct in daily practice . 
the italian registry was promoted by the sub - society of cardiac radiology of the societ italiana di radiologia medica ( sirm ) , which currently includes almost 700 members ( cardio )  . knowledge of the geographic distribution of cct programs , as well as the use and spectrum of technological equipment and different diseases assessed in each participating center , might be of great importance not only for epidemiological analyses , but also to create a large common national database of patients for further pathologyfocused studies . 
barile ospedale di villa dagri , masciovetere , italy materials and methods data collection the data were prospectively collected during a 6 - month period ( januaryjune 2011 )  . 
during this period 3 , 455 consecutive patients underwent cardiac ct in one of the 47 participating centers . centers were initially recruited via email from the mailing list of the sirm members ( approximately 9 , 000 members ) and each site , after acceptance , appointed a referral physician ( a radiologist ) who was locally responsible for data integrity , interpretation and collection and represented the direct contact for the steering committee of study . referral physicians were not required to exhibit any specific sub - society - based certificate of competency in cct imaging as the aim of the present registry was to provide a real - world snapshot of cct utilization in italy , without limiting patient enrollment only to the most experienced national groups . similarly , acquisition protocols were individually defined and tailored by each center according to the main clinical request , without following any established , predefined or standardized protocol . data collection preliminary general reports and case report forms ( crf ) were completed at each center . in each electronic form , the following sections had to be filled in : 1 . 
clinical indications for the examination , which were listed and readapted following the accf / acr / scct / appropriateness scmr / asnc / nasci / scai / sir criteria for cardiac computed tomography and cardiac magnetic resonance imaging published in 2010 ( calcium scoring , suspected coronary artery disease ( cad ) , follow - up in patients with known coronary disease , follow - up in patients after coronary artery bypass grafting , acute chest pain , study of cardiac anatomy , other )  . 1 3 radiol med ( 2015 ) 120 : 919929 3 . 
complications caused by acute adverse reactions to contrast media ( i.e. , within 60 min after administration ) were defined according to the american college of radiology criteria . adverse events were scored as mild , moderate or severe using the following predefined criteria readapted from dorfman et al . 
 [ 11 ] : ( a ) mild : transient change in condition , not life threatening and rapidly returning to baseline , required monitoring and / or minor intervention such as holding a medication , obtaining laboratory test ( s ) , etc . ( b ) moderate : transient change in condition , may be life threatening if not treated , returning to baseline if properly treated and required monitoring and / or intervention such as reversal agent , additional medication or transfer to icu . ( c ) severe : change in condition , life threatening if not treated and potentially permanent , may have required hospitalization or transfer to icu , required monitoring and / or major intervention such as invasive procedure , intubation , hemodynamic support and blood transfusion . 
means ( with standard deviation [ sd ] ) were computed as appropriate to describe the patient population . results the overall database of the present registry included 3 , 455 patients who underwent cct during the study period . 
the mean height and weight were 167 31 kg ( range 44190 ) kg , respectively ( table 1 )  . 14 cm ( range 143198 cm ) and 76 12 pediatric patients were also examined . 
therefore , the geographic distribution of the patient population demonstrated a clear north - to - south gradient , with the largest proportion ( 2 , 050 [ 59.5 % ] ) of patients enrolled in the north , followed by central regions ( 942 [ 27.3 % ] ) and the south and islands ( 451 [ 13 % ] patients )  . most ( 3 , 283 [ 95.35 % ] ) patients underwent cct for non - urgent reasons . 
the mean ct examination was 110.4 per center with large differences between 90.2 each other ; 12 centers performed more than 100 examinations , 5 more than 200 examinations and only 1 more than 500 examination in 6 months . 
none of these studies were performed in the emergency department . clinical indications for the examination the most frequent indications for cct were suspected cad ( 44.8 % ) , calcium scoring ( 9.6 % ) , follow - up postfollow - up post - cabg angioplasty / stenting ( 7.5 % ) , assessment of cardiac anatomy , especially studies of the pulmonary veins and atria ( 4.22 % ) , assessment of patients with known cad ( 4.1 % ) and acute chest pain ( 8.3 % ) , acquisition data most investigations ( 73.02 % ) were performed with 64 - slice scanners . 
the distribution of latest generation scanners ( 128 or more slices ) was equally divided between the north ( 3 ) , center ( 2 ) and south / islands ( 2 )  . 
the mostly commonly used contrast material was iomeprol 400 mg / dl ( 76.1 % ) ; the average contrast media ( cm ) volume was 3 ml ( range 30180 ml ) and the average flow rate 0.6 ml / s ( range 46.7 ml / s ) ( table 3 )  . there was no relationship between the number of slices and flow rate , although a trend toward an inverse relationship between number of slices and volume of cm administered was noted . 
the total mean dlp was 618 4.3 mgy ( range 632370 mgy )  . adverse clinical events occurred during or immediately after the procedure ( < 60 min ) in 26 cases ( 0.75 % ) ; 23 cases were described as mild and 3 as moderate . 
in 14 cases the adverse event was attributed to contrast agent administration ( mild allergic reaction : nausea in 6 cases , skin rash in 2 cases , cough in 1 case , sneezing in 2 cases and itching in 3 cases )  . 
the events were not attributed to just one contrast agent , but were noted across all contrast agents utilized without clear differences between each other , considering the small number of cases reported . 
nevertheless in the majority of the patients ( 56.8 % ) , the absence of coronary diseases was able to exclude previous pathological suspects . overall , only 101 ( 2.9 % ) examinations were non - diagnostic and had no clinical relevance . 
two of these nondiagnostic examinations were due to adverse events during the examination caused by drugs or the patients basal 1 3 924 radiol med ( 2015 ) 120 : 919929 fig . 
there was no relationship between non - diagnostic investigations and heart rate ( mean hr in non - diagnostic cases 74 0.6 bpm ; range 6094 bpm ) and scanners 64 slices . 
in our series , cardiologists alone made up just 0.02 % of reporting physicians ( only 1 case )  . discussion this italian cct survey was designed to evaluate diffusion and geographic distribution of the various national centers performing the examination , recording scanner types , number of slices , protocols adopted , safety profile and spectrum of clinical indications . the registry represents a relatively large patient population recruited in a relatively short time interval ( 3 , 443 adult patients during a 6 - month period of enrollment ) and derived from the experience of 47 different centers distributed throughout italy , with a north - to - south gradient ( 2 , 050 examinations performed in 27 centers in the north 1 3 radiol med ( 2015 ) 120 : 919929 table 3 technical parameters of the concerned radiation and contrast material parameter value total population ( mean sd ; range ) 43 mgy ( 632 , 371 ) radiation dose ( dlp ) 16 slice ( mean sd ) 64 slice ( mean > 64 slice ( mean contrast agent sd ) sd ) type iobitridol 350 iohexol 350 iodixanol 320 ioversol 320 iopromide 370 iomeprol 400 unknown 618 1 , 409 616 , 94 422 13 mgy 13.1 mgy 21 mgy 3 , 185 ( 92.1 % ) 60 ( 1.73 % ) 97 ( 2.8 % ) 75 ( 2.17 % ) 2 ( 0.05 % ) 325 ( 9.4 % ) 2 , 614 ( 76.1 % ) 268 ( 7.8 % ) volume ( mean flow rate ( mean sd ) sd ) side effects 3 ml ( 7180 ) 0.7 ml / sec ( 16.7 ) 26 ( 0.75 % ) missing data in 18 patients ( i.e. , investigations ) of the country , 942 in 11 centers in the center and 451 in 9 centers in the south and islands ) , using multivendor equipment and contrast agents and covering variable levels of cct expertise . 
the strength of the study lies in its openaccess nature and absence of specific enrollment criteria . although cardiac ct was predominantly performed by radiologists , collaboration between radiologists and cardiologists was evident at a few sites . 
in the vast majority of cases ( 73.0 % ) , cct was performed using scanners with 64 slices and these types of scanners were also the most common of all in the national territory [ 12 ]  . 
while the number of centers performing the examination was larger in the north , the distribution of the latest scanner generation was evenly divided across the country . our study showed that the number of slices was inversely proportional to radiation dose : in those centers that used scanners with > 64 - slices the dlp was lower . 
this aspect is difficult to understand , but could be partially explained by the difficulty in performing a cardiac ct examination in the acute phase around the italian territory . cct has a high diagnostic performance in the followup of patients after cabg . 
in those cases , the examinations were performed mostly for the study of pulmonary veins and atria [ 2224 ]  . finally in most of the cases ( 55.8 % ) , ct was useful to exclude the presence of disease avoiding the need of more invasive and expensive tests as coronary angiography [ 25 ]  . our patient cohort data confirm the good safety profile of cct with only 26 ( 0.7 % ) adverse events recorded during or immediately after the procedure . 
in a the retrospective technique was used ( 2.8 msv ) , instead the prospective gated acquisition was used ( 1.9 msv ) in b with the evidence of a slight misalignment af the middle descending artery these data showed the quite large utilization of cardiac ct in the field of different cardiac pathologies . 
in fact , the mean hr in non - diagnostic cases was 0.6 bp moreover , the acquisition time was also related to non - diagnostic examination and it was more prevalent for 16 - slice scanners . 
differences in the technologies and expertise also affect the homogeneity of the data ; only five centers performed more than 40 examination per month . oslo missed information about specific changes in the management of the patients provided by the evidence of pathological findings on cardiac ct . finally , our study design did not include information on patient follow - up after contrast administration , thus excluding the possibility of identifying late contrast - related adverse reactions . 
however , such reactions have virtually been eliminated by preventive measures in all patients requiring ct evaluation . conclusions our italian registry revealed a wide diffusion and geographic distribution of cct - dedicated centers with more centers and investigations performed in the north as compared to the central and southern regions . 
cct is mainly performed and reported by radiologists . the limited incidence and low severity of adverse clinical events observed in our registry confirms that cct has a good safety profile , similar to data reported elsewhere . our data also show that cct is important in clinical management of patients . the further research focus of cct registries would probably be systematic clinical follow - up of patients enrolled to analyze midand long - term implications of cct findings , fig . 
5 flash technique also obtained in a single heartbeat at 1.5 msv our study has shown that cct is a safe technique and that it is useful in patient management . the main limitation of the study is related to the information of the outcome of these patients . 
the purpose of the present study was to develop a classification of the us features of non - mass - like breast lesions correlated with pathology , so as to improve the diagnostic accuracy of us in non - masslike breast lesions . materials and methods a total of 854 breast lesions in 836 consecutive women scheduled for us - guided core - needle biopsy or us - guided vacuum - assisted biopsy between may 2008 and october 2011 were initially included in this study . 
the us features of the 80 non - mass - like breast lesions were classified and their correlation with pathology was analysed . results of the 80 non - mass - like breast lesions , 43 cases ( 53.8 % ) were malignant and 37 cases ( 46.2 % ) were benign . 
fifty - two cases ( 73.7 % ) appeared as a hypoechoic area , 22 cases ( 21.1 % ) appeared as a hypoechoic area with sporadic or clustered microcalcification , four cases appeared as architectural distortion , and two cases appeared as solid echogenicity within a duct . 
us had a high sensitivity but a low specificity in the diagnosis of non - mass - like breast lesions and a definitive diagnosis requires a us - guided biopsy . lesions keywords non - mass - like breast lesions ultrasonography microcalcification introduction owing to advances in ultrasound ( us ) technology , optimal us techniques with a high - frequency transducer can identify more and more breast lesions . 
breast us is currently considered to be an important examination method for both detection and characterisation of breast lesions [ 1 ]  . the lexicon of features seen on breast us includes three types of lesions : masses , calcifications and special cases . 
however , in clinical work , we often encounter breast lesions that manifest as non - mass - like lesions that do not meet the strict criteria of a mass , such as ill - defined geographic hypoechoic lesions , architectural distortions , calcification , and so on . 
it is reported that some breast carcinomas , such as ductal carcinoma in situ ( dcis ) , could manifest as a non - mass - like lesion on us [ 35 ] , and identification 1 3 906 radiol med ( 2015 ) 120 : 905910 of non - mass - like breast lesions on us is , therefore , very important in enabling accurate interpretation of the us features of these non - mass - like breast carcinomas . in the guideline of 2004 , non - mass - like breast lesions were classified as follows : duct dilatation , multivesicular pattern , low echo area in the mammary gland and architectural distortion [ 6 ]  . 
but all these were mainly cited from mri non - masslike lesions findings , which were unsuitable for us findings . the aim of the present study was to develop a modified classification of the us features of non - mass - like breast lesions correlated with pathology to improve the diagnostic accuracy of us in non - mass breast lesions . materials and methods patients a total of 854 breast lesions in 836 consecutive women scheduled for us - guided core - needle biopsy or us - guided vacuum - assisted biopsy between may 2008 and october 2011 were initially included in this study . 
the conventional us findings were retrospectively reviewed and classified as mass or non - mass - like lesion by two breast radiologists ( wang zl and li n )  . 
the us examinations were performed by one of two experienced breast radiologists ( li jl and wan wb ) with 12 and 11 years of experience in breast us , respectively . 
among the 80 cases , 18 cases ( 22.5 % ) were classified as category 3 ( suggestive of benign ) , 21 cases ( 36.3 % ) as category 4a ( low suspicion for malignancy ) , 10 ( 12.5 % ) as category 4b ( intermediate suspicion for malignancy ) , 13 ( 13.8 % ) as category 4c ( moderate suspicion for malignancy ) and 18 as ( 15.0 % ) category 5 ( highly suggestive of malignancy )  . 
eighteen birads 3 lesions underwent biopsy at the patients request because of strong anxiety . bi - rads categories 13 were taken as benign and the bi - rads scores of 4 or 5 were taken as malignant . image interpretation two radiologists ( wang zl and li n ) with more than 10 years experience in breast us who were blinded to the clinical , mammographic and histopathological results evaluated the us images during a single review session . 
we defined the non - mass - like lesions as a conventional us image that did not meet the strict criteria of a mass , which was defined as a space - occupying lesion seen on two different projections according to the bi - rads lexicon for us . 
the distribution patterns were classified into four categories as follows : hypoechoic area , hypoechoic area with sporadic or scattered microcalcification , architectural distortion and solid echogenicity within a duct . 
hypoechoic area referred to an area with low - level echo ; hypoechoic area with sporadic or scattered microcalcification referred to a hypoechoic area with microcalcification , with either sporadic or scattered distribution ; architectural distortion referred to an area with disordered organisation structure compared to normal breast tissue ; and solid echogenicity within duct referred to a solid lesion within a duct . 
the lesion was demonstrated to be high - grade ductal carcinoma in situ by surgery comparison between us imaging parameters and pathology the comparison between the us imaging parameters and pathology can be seen in table 2 . 
among them , two cases changed from bi - rads 4b to 4a with pathology demonstrating that one was an intraductal papilloma , one an adenosis and one case changed from bi - rads 4c to 4b which was demonstrated to be an dcis by pathology . discussion although areas with indistinct boundaries on us have been encountered in clinical practice for some time , the recognition of abnormal lesions and a description of the findings differed significantly based on the us operator owing to a lack of unified terminology . 
one study has demonstrated that 95 % non - mass - like breast lesions on us also appeared as non - mass enhancement on magnetic resonance imaging ( mri ) , and it was also difficult for mri to provide a differential diagnosis for these non - mass breast lesions [ 7 ]  . 
also , it has been reported that the histological agreement rate between us - guided core - needle biopsy and surgical histological diagnosis was significantly better for mass lesions than for non - mass - like lesions on us [ 810 ]  . 
therefore , an in - depth study of the us features of non - mass - like breast carcinoma appears to be of major importance . in our study , non - mass - like lesions were classified according to their us characteristics as follows : hypoechoic area in the mammary gland , hypoechoic area with microcalcification , architectural distortion and solid echogenicity within duct . 
the difference of the classification of non - mass - like breast lesions on us between our study and the previous guideline [ 6 ] might be caused by the different samples and different recognition of breast lesions by sonologists . 
simple duct dilatation was very common on clinical us examination , and we did not consider it could cause misdiagnosis and , therefore , did not include it in our study . 
multivesicular pattern was not often seen on clinical us examination and modern us could easily distinguish it from a solid lesion ; for these reasons , it was not included in our study . 
in our study , many other malignant lesions , such as idc , lymphatic metastatic poorly differentiated adenocarcinoma , adenocarcinoma and acute lymphatic leukaemia also appeared as non - mass lesions . 
studies have demonstrated that infiltrating lobular carcinoma ( ilc ) , primary small cell carcinoma and breast lymphoma could show a non - masslike pattern on us as well [ 11 , 12 ]  . 
not only malignant lesions , but also non - malignant lesions can also appear as non - mass - like lesions , such as adenosis , intraductal papilloma and plasma cell mastitis . 
some studies classified the hypoechoic area into ductal hypoechoic area and nonductal hypoechoic area according to whether they describe patterns reminiscent of the milk duct system or those reminiscent of glandular tissue [ 13 ]  . 
in fact , it is difficult to discriminate between a ductal hypoechoic area and a non - ductal hypoechoic area on us imaging . it has been reported that microcalcification can be seen in about 4050 % breast carcinomas [ 14 , 15 ] and that dcis usually appear as microcalcification on mammography [ 15 ]  . 
ultimately , we suggest that hypoechoic area with microcalcification should undergo biopsy . both architectural distortion and solid echogenicity within duct were not common appearances of non - mass - like breast lesions , and further study should include more cases of these two kinds of us findings to judge their significance in the diagnosis of non - mass - like breast carcinoma . in this study , non - mass - like lesions caused major difficulty for the us diagnosis with bi - rads 4 lesions accounting for 55.0 % ( 88 / 160 )  . 
in the 37 cases of benign lesions , 21 ( 56.8 % ) cases were diagnosed as bi - rads 45 categories , and only 16 cases ( 43.2 % ) were accurately diagnosed as bi - rads 3 category . one limitation of this study was that there were no cases of ilc in this study . 
a study with more cases would allow a more exact evaluation of these two us findings . in conclusion , with the development of us technique , high - resolution us allows for identification of small , clinically occult non - mass - like findings . 
 us had a high sensitivity but a low specificity in the diagnosis of non - mass - like breast lesions , and a definitive diagnosis requires a us - guided biopsy . acknowledgments this work was supported by a grant from the national natural science foundation of china no . 
since even bbb permeability relates to glioma malignancy grade , we carried out a comparative evaluation between cbv and psr to characterise cerebral gliomas . materials and methods forty - nine patients with cerebral gliomas were studied with mr perfusion imaging . 
maria hospital , terni , italy e - mail : marco.muti@tin.it compared to all gliomas excluding glioblastomas was assessed . results a significant difference between low - grade and high - grade gliomas with both cbv and psr was demonstrated . 
finally , superior sensitivity and specificity of psr compared to cbv in identifying low - grade gliomas was demonstrated both compared to all gliomas and all gliomas excluding glioblastomas . conclusion the psr evaluation proved better than cbv for determining the grade of brain and is therefore a useful tool to be considered in the mr evaluation of gliomas . keywords glioma permeability magnetic resonance perfusion imaging introduction cerebral gliomas are a very heterogeneous group of tumours in terms of pathological aspects , and clinical and natural history . 
indeed , while high - grade gliomas have a poor prognosis because they grow rapidly and are highly vascular , low - grade gliomas can remain quiescent for many years [ 1 ]  . the grading of gliomas is based on the histopathologic analysis of the tumour , which is achieved by brain biopsy or surgery ; however , there are inherent limitations with these techniques and their interpretation , and one of the most frequent problems is that the biopsy sample or surgical specimen does not include the most malignant foci of the tumour [ 2 ]  . 
in detail , 18 patients had low - grade gliomas , while 31 had high - grade gliomas ( table 1 )  . the study consecutively included only treatment - free patients ; all of them underwent mr from march 2010 to january 2013 , and both conventional and perfusion evaluations were performed during the same examination . 
the study was performed according to the world medical association declaration of helsinki . imaging technique contribution of magnetic resonance ( mr ) imaging may be significant for the diagnosis . the malignancy grade of gliomas is proportional to their neovascularisation since the neoplastic cells produce neoangiogenetic factors according to their anaplastic grade , with a higher percentage of immature and hyperpermeable vessels [ 3 , 4 ]  . perfusion mr imaging with the dynamic susceptibility contrast ( dsc ) technique has been used to assess the microvessel status of cerebral gliomas . 
after contrast medium administration , axial , coronal and sagittal t1 - weighted images were acquired . perfusion evaluation was performed by means of multishot echoplanar sequence [ 3d presto / gre - epi t2 * ; 5 mm thickness ; tr 20 ms ; te 29 ms ; flip angle ( fa ) 128 ; fov 230 mm ; nex 1 , with 40 8 ; matrix 64 dynamic phases and a time resolution of 1.67 s ] acquired in a dynamic manner immediately after contrast medium administration . the paramagnetic contrast medium ( prohance , bracco , milan , italy ) was administered intravenously with a 18 - gauge needle using an automatic injector at the infusion rate of 5 ml / s . 
the contrast medium dose was 0.25 mmol / kg in all cases since a 0.05 mmol / kg prebolus was administered followed by a 0.2 mmol / kg diagnostic gadolinium bolus . quantitative analysis postprocessing evaluation was made at a later stage of the data acquisition by two of the authors independently , blinded at the time of analysis to the histological data . 
1 receiver operating curves ( roc ) for relative cerebral blood volume ( rcbv ) and percentage of signal intensity recovery ( psr ) to differentiate low - grade gliomas from all gliomas carried out with a dedicated workstation ( view forum , philips medical system , eindhoven , the netherlands )  . 
in order to calculate the maximum cbv value for each patient , multiple ( about four ) regions of interest ( roi ) of 2550 pixels were manually placed where the highest cbv values were identified on the colour maps , including neoplastic solid tissue ( identified on postcontrast images or on t2 - weighted images if enhancement was absent ) , excluding necrotic tissue . 
 [ 8 ] : psr = 100 % ( cid : 31 ) s1 smin ( cid : 30 ) / ( cid : 31 ) s0 smin ( cid : 30 ) , where s1 is postcontrast t2 * - weighted signal intensity ; s0 is precontrast t2 * - weighted signal intensity , and smin is minimum t2 * - weighted signal intensity . as no software is available that provides in real - time recovery data , the values were obtained by calculating the mean signal intensity level before ( s0 ) and after ( s1 ) the curve drop and evaluating the minimum signal intensity level at the peak time ( smin )  . 
 multiple psr values for each patient were calculated in the same rois selected before for rcbv evaluation , and then between these rois , the minimum psr value was selected for statistical analysis . 
the minimum psr value had to be chosen since it is inversely proportional to breakdown of the bloodbrain barrier ( bbb ) and then minimum psr foci are those with the higher malignancy grade . statistical analysis statistical evaluation was performed with the following steps : ( 1 ) the kolmogorovsmirnov test was done to evaluate the normal distribution of maximum rcbv and minimum psr values ; ( 2 ) the t test was used to compare the maximum rcbv and minimum psr values of the tumours studied . 
contrast - enhanced foci in t1 - weighted images depict a bbb breakdown which is usually associated with higher tumour grade ; however , contrast enhancement is not always accurate in predicting the tumour grade . 
 often grade iii gliomas fail to enhance after gadolinium administration although the lack of enhancement is not a specific finding for low - grade glioma , which may also enhance to varying extents , with some grade i gliomas showing intense enhancement ( i.e. , pilocytic astrocytoma ) [ 12 , 13 ]  . 
moreover even in high - grade gliomas with pathological contrast enhancement , the foci of gadolinium accumulation do not always reflect the areas of greater angiogenesis or vascular permeability [ 16 ]  . 1 3 radiol med ( 2015 ) 120 : 967974 ( flair ) fig . 
3 axial a fluid - attenuated t2 - weighted image , axial b postcontrast t1 - weighted image , cbv map ( c ) and perfusion curve ( d ) of a left temporal grade ii astrocytoma . 
in the perfusion curve ( d ) , the venous phase signal recovery , compared to the arterial phase , is almost complete if an in vivo grading of glioma is required , it can be performed in an optimal way by using advanced magnetic resonance techniques . 
perfusion imaging of brain tumours can also be used for stereotactic biopsy guidance , for better delineation of tumour margins and also for assessing treatment response [ 18 ]  . because angiogenesis is an important feature in malignant gliomas , perfusion mr imaging may provide additional important information . 
for this reason , high - grade gliomas have elevated rcbv mean values and low psr mean values in comparison with low - grade brain tumours [ 19 ]  . 
the correlation between the histopathological grade of cerebral gliomas and rcbv has been evaluated several times with perfusion mr imaging studies [ 6 , 16 , 2022 ]  . more recently , a new haemodynamic parameter has been extrapolated from the mr perfusion curves . 
in practice , if the mr signal recovery in the venous phase is complete , it means that all of the contrast medium has passed into the veins and therefore there is no bbb damage . 
instead , if the venous phase mean signal is lower than that of the arterial phase , it means that a part of the contrast medium has not arrived in the venous circulation and passed into the interstitial space because of bbb breakdown . 
the psr is defined as the ratio between mean venous phase signal intensity and mean arterial phase signal intensity and if it is less than 1 , then there is a pathological vascular permeability because under normal conditions the contrast medium does not pass through the bbb . vascular proliferation and vascular permeability can predict transition from low - grade to high - grade glioma and also help the evaluation of response to treatments . 
several methods based on the acquisition of postcontrast dynamic sequences have been developed in previous studies in order to obtain quantitative 1 3 972 radiol med ( 2015 ) 120 : 967974 fig . 
4 axial a flair t2 - weighted image , axial b postcontrast t1 - weighted image , cbv map ( c ) and perfusion curve ( d ) of a right temporal anaplastic astrocytoma . 
hyperperfused foci are not evident on the cbv map ( c ) , but in the perfusion curve ( d ) , the signal recovery in the venous phase is incomplete due to increased vascular permeability compared with the norm but not sufficient to cause the gadolinium accumulation in the interstitial space that results in enhancement ( b ) data on brain tumour vascular permeability [ 2325 ]  . 
 [ 23 ] calculated vascular permeability using dynamic 3d gradient echo ( ge ) t1 postcontrast sequences and correlating the appearance of the enhancement curve of fully vascular rois with that of the enhancement curve of neoplastic tissue rois . 
 [ 25 ] evaluated the vascular permeability of brain tumours by extrapolating the data from signal intensity / time curves obtained after the acquisition of dynamic postcontrast t1 - weighted sequences . 
furthermore , some studies regarding the evaluation of k ( trans ) have been published [ 26 , 27 ] ; this is a pharmacokinetic constant proportional to permeability between two compartments and has been used in order to assess the bbb breakdown in brain tumours . in recent years , a new method has been adopted to assess vascular permeability . 
it consists in the evaluation of the signal intensity recovery between the venous phase ( washout ) and arterial phase ( wash - in ) in the perfusion curves obtained with the dsc technique . 
the percentage of signal recovery ( psr ) is related to the contrast medium leakage in the interstitial space during the capillary phase and therefore allows estimation of vascular permeability . 
 [ 28 ] adopting psr evaluation in 41 high - grade gliomas were able to demonstrate a statistically significant difference between those in grades iv and those of grade iii . 
studies on the vascular permeability of brain tumours performed by evaluating the perfusion imaging curve psr are not so numerous and are almost always heterogeneous clinical series that included metastases , gliomas as well as some lymphomas [ 9 , 10 ]  . 
5 axial a flair t2 - weighted image , axial b postcontrast t1 - weighted image , cbv map ( c ) and perfusion curve ( d ) of a right temporal glioblastoma . 
in the cbv map ( c ) , the lesions solid tissues appear markedly hyperperfused and the signal recovery in the venous phase ( d ) is very incomplete , caused by a considerable bbb breakdown our study is the first that uses this method to evaluate vascular permeability in order to characterise the low - grade gliomas compared to high - grade ones . 
in our study , the psr evaluation allowed us to characterise in a statistically significant manner low - grade compared to high - grade gliomas , as has been shown in previous papers with other advanced mr techniques such as spectroscopy and rcbv evaluation with dsc perfusion imaging [ 57 , 16 , 2022 ]  . 
the assessment of the vascular permeability of gliomas with psr is therefore useful for their characterisation and adds to the traditional perfusion techniques ( cbv ) and spectroscopy ; psr evaluation can be used in conjunction with these in order to increase the diagnostic potential of mr . a relative limit of this evaluation is that a specific software enabling automatic calculation of the psr value is required to facilitate the calculation . 
if this software is not available , as in our case , the psr value must be calculated manually , and this task quite time consuming and thus not compatible with a routine use of the technique . 
a limitation of this study is the relatively small number of grade iii gliomas , which were , however , sufficient to obtain statistically significant results . the most important result we obtained with our study was the possibility to differentiate low - grade from grade iii gliomas in a statistically significant manner . 
the differential diagnosis between low - grade gliomas and anaplastic ones is a major challenge in neuro - oncology because the prognosis of grade ii or grade iii glioma is very different . 
in the first case , there is usually a long survival , while in the second case , 5 - year mortality is high [ 1 , 19 ]  . 
conversely , no similar difference exists between grade i and grade ii gliomas , both having long survival time , or between grade iii and grade iv gliomas , since both easily recur and are responsible for the death of the patient [ 1 , 19 ]  . 
moreover , while glioblastomas are usually easily detectable even with conventional mr sequences due to some typical features ( i.e. , abundant oedema , macroscopic necrosis , corpus callosum involvement , considerable size and hypointense foci on t2 - weighted images ) , often the anaplastic gliomas have similar morphological characteristics to those of grade ii lesions ; in many cases even the anaplastic gliomas show poor or null enhancement after contrast agent administration , therefore displaying identical appearance to low - grade gliomas [ 1215 ]  . 
therefore the differential diagnosis between grade iii and low - grade gliomas is often very difficult using only the morphological mr technique , even if it is very important for patient management . 
the importance of the differential diagnosis in vivo is due to the fact that these tumours 1 3 974 radiol med ( 2015 ) 120 : 967974 are not always operable , and in the case of biopsy , evaluation of malignancy grade may be underestimated if sampling was not carried out in the most malignant foci of anaplastic tumour . 
malignancy grade can also be underestimated when a partial removal of the tumour is possible , and the surgical sample does not include the most malignant fraction ; unfortunately , it often happens that this is the deepest part of the lesion which is also the portion that is most difficult to be removed . 
the ability to establish an in vivo differential diagnosis between low - grade gliomas and grade iii gliomas is therefore an important tool in neurooncology . conclusion in conclusion , we confirm that it is useful to complete the mr study of brain gliomas with an evaluation of vascular permeability by calculating the psr . 
up to now , the surgical hematoma evacuation and the bonding of blood vessels were considered the most appropriate treatment , while at present , the percutaneous management by means of selective catheters and embolization of the bleeding vessel is considered to be the most used option . 
our purpose is to report our experience in the endovascular spontaneous rectus muscle bleeding treatment in the elderly patients . materials and methods from the data base and medical reports of the hospital , we selected 144 medical reports . 
 we focused on those cases that showed the following criteria : patients with rectus muscle hematoma undergoing anticoagulation therapy and / or non - traumatic spontaneous hematoma and with persistent bleeding revealed on ct examination despite a pharmacological treatment aimed to timely reverse coagulopathy . 
the criteria for this treatment were hemodynamic instability and the continuous bleeding despite the correct medical therapy . results ct imaging detected rectus muscle hematoma in 18 / 18 patients and active bleeding in 7 / 18 patients . 
in 14 patients , one single vessel was responsible for the bleeding , while in the other four patients , more than one vessel were involved : in two patients , we also found the involvement of the superior epigastric artery ; while the other two patients showed also the involvement of the deep iliac circumflex artery . 
the material for embolization was compatible coils with microcatheters in 17 / 18 patients , and glue for 1 / 18 patient . conclusions patients with large rectus muscle hematoma , which have not yet recovered with conservative therapy , should then consider undergoing endovascular treatment . 
it is difficult to determine when surgery is necessary when there is very poor data provided by scientific literature review , so the decision to use surgery can be suggested when embolization is unsuccessful or when it is necessary to evacuate a complex huge fluid mass in peritoneal cavity . keywords rectus muscle hematoma endovascular management embolization computed tomography arteriography 1 3 952 introduction the rectus muscle hematoma is a blood collection in the sheath of the anterior rectus muscle , due to epigastric artery damage or the tearing of one or more muscle fibers , usually located beneath the umbilicus where blood vessels are not protected by external aponeurotic fascia [ 1 ]  . non - traumatic spontaneous hematoma of the rectus abdominal muscle is not a common cause of pain in ordinary medical treatment , and it is not considered a critical condition [ 2 , 3 ]  . 
nevertheless , it can be a serious complication in some patients due to continuous and / or consistent bleeding [ 4 ]  . the most frequent cause of spontaneous rectus muscle hematoma is the anticoagulation therapy [ 5 , 6 ]  . 
nevertheless , a large hematoma can develop and / or cause a severe hypovolemia that requests not only an early and accurate medical instrumental diagnosis and treatment , but also an adequate therapy with an inversion of the coagulation cascade , liquid infusion and hemostatic treatment [ 8 ]  . in some patients , despite a correct and early medical therapy , the continuous bleeding requests a more radical handling [ 8 , 9 ]  . 
up to now , the surgical hematoma evacuation and the bonding of blood vessels were considered the most appropriate treatment , while at present , the percutaneous management by means of selective catheters and embolization of the bleeding vessel is considered to be the most used option [ 10 ]  . our purpose is to report our experience in the endovascular spontaneous rectus muscle bleeding treatment in the elderly patients . materials and methods going through the data base and medical reports of the hospital , we focused on those medical cases that emphasized rectus muscle hematoma in the main diagnosis , radiol med ( 2015 ) 120 : 951958 which occurred between the year 2001 through 2011 . 
from the selected 144 medical reports , we focused on those cases that showed the following criteria : patients with rectus muscle hematoma undergoing anticoagulation therapy and / or non - traumatic spontaneous hematoma and with persistent bleeding revealed on ct examination despite a pharmacological treatment aimed to timely reverse coagulopathy . these criteria were found in 18 patients : 15 females and 3 males , with a median age of 73 ( range 6481 years )  . 
a delay ranging from 30 to 40 s was used for the arterial phase and from 70 to 80 s for the venous phase . because of clinical conditions , all patients were moved on the angiographic room for diagnostic arteriography and embolization ( oec 9800 plus - general electric )  . 
1 ultrasound : diagnostic study , carried out with a 15 - mhz linear probe , detects a subcutaneous fluid collection , with a superior hypoechoic portion and a slightly hyperechoic inferior part : the patients position determines the obliquity of the blood level gathered in the fluid collection 1 3 radiol med ( 2015 ) 120 : 951958 fig . 
the ct basal phase a reveals a mass effect developing toward the abdominal cavity in the same level shown in us examination , with a slightly low hyperdensity , as if a recent bleeding had occurred . 
lower level scans c allows to follow the bleeding arterial branch , the lower epigastric artery in this specific case , providing important data to request interventional radiology for further management fig . 
in 11 / 18 1 3 954 radiol med ( 2015 ) 120 : 951958 procedures ; 3 / 18 patients died during hospitalization ( the first after 12 h , the second after 2 days and the last after 8 days ) , due to multiorgans failure as a result of hemodynamic disorders due to the hematoma : severe kidney failure in two cases and heart failure in one case . discussion rectus muscle hematoma is a clinical disorder relatively common in the elderly patients . in order to better understand the pathogenesis of this medical case , it is important to focus on the abdominal anterior wall anatomy . 
they start from the superior margin of the pubis , and they end in the ventral portion of the 5th , 6th , 7th cartilaginous ribs and on the xiphoid process of the sternu they are separated by a central alba line while the side edge is represented by the semilunar line . 
they are formed by several fibers wrapped in sheaths and supplied by vessels from the epigastric artery . the rectus muscles are divided in two separate portions ( upper and lower muscle ) by the arcuate line located 5 cm below the umbilicus . above the arcuate line , there is the aponeurosis of the external and internal oblique and transverse muscles . 
 below the arcuate line , there is any muscular insertion and only the transversalis fascia and the peritoneum divide the muscle mass from the posterior abdominal viscerum , thus allowing the hematoma to expand easily beyond the midline and descending toward the bladder in retzius space : this communication creates a natural dissection level between the rectus muscle back face and the bladder [ 11 , 12 ]  . the artery supply to the rectus muscle is given by the superior and inferior epigastric arteries . the inferior epigastric artery originates from the external iliac : it starts from the inguinal ligament and curves forward in the subperitoneal tissue , and then , it ascends obliquely along the medial margin of the abdominal inguinal ring ; continuing its course upward , it pierces the transversalis fascia and , passing in front of the arcuate line , ascends between the rectus muscle and the posterior lamella of its sheath . during the contraction of the rectus muscle , the length of the muscle changes and the artery adapts accordingly to prevent stretching . the combination of the insertion of the inferior epigastric artery with the stabilization provided by the insertion of the muscle fibers makes the artery sensitive to the pressure in the insertion points during intensive physical activity . the superior epigastric artery enters the sheath at the 7th cartilaginous rib and then descends between the rectus fig . 
4 ct : large left - sided rectus muscle hematoma extending its mass effect to the homolateral flank ; it is possible to depict a wellshaped mass rim , a mass effect toward the inside , a fluid level with hyperdensity of the declive portion due to recent bleeding and the presence of an active bleeding . 
in 14 / 18 patients , one single vessel was responsible for the bleeding , while in the other 4 / 18 patients , more than one vessel were involved : in two patients , we also found the involvement of the superior epigastric artery , while the other two patients showed also the involvement of the deep iliac circumflex artery . the embolization material used was compatible coils with micro - catheters in 17 / 18 patients , and glue for one patient . 
embolization was carried out with success , since no active bleeding was revealed during arteriography at the end of the endovascular treatment . 15 / 18 patients were submitted to an 18 - day ct followup . 
during this period , no further or new bleeding was revealed , and hemodynamic levels were stabilized : blood pressure had become normal in 14 / 18 patients ; only four patients were treated with blood transfusion to correct anemia , and only one patient needed platelet therapy . 
the hematomas progressive increase in size and the worsening of the hemodynamic conditions requested a ct study ( b ) , which confirmed the presence of a non - malignant mass with an inside active bleeding . 
the selective study of the external right iliac artery ( c ) allowed to confirm not only the presence of active bleeding shown through the collection of contrast material outside the physiological vascular flow , but also an increase in the collection during further phases of the artery study . 
this procedure also identified the artery responsible for the bleeding , which was then treated with micro - catheters ( d ) and coils for embolization muscle and the posterior lamella of its sheath . 
the two arteries form anastomosis in the level of the umbilicus , which are microscopic and help lower the possibility of blood vessel trauma during an important muscle strain ; given the artery supply , hematoma concentrates mainly in the posterior muscle area , thus creating diagnostic problems [ 13 ]  . hematoma above the arcuate line is usually due to the damaging of the superior epigastric artery or of its perforating arteries : patients usually show a small spindled unilateral mass ; hematoma is isolated by the rectus sheath and by the tendons that allow the self - limiting bleeding . hematoma below the arcuate line is a consequence of the inferior epigastric artery damaging or of its perforating branches . 
it is generally located at posterior muscle area and has spherical shape because in this point the rectus muscle is supported only by the transversalis fascia and parietal peritoneu hematoma can cause blood loss and can extend easily because there are no tendons that can stop it expansion . 
hematoma can also go beyond the midline and become bilobar [ 12 ]  . the main cause of hematoma is the anticoagulant therapy ; the exact pathogenesis of this association is still unknown . 
it is thought to be a heparin - induced micro - angiopathy , involving a sublayer of a preexisting vascular arteriosclerosis ; further damaging issues concern the clinical condition such as abdominal strains , e.g. , coughing , asthmatic reaction , an abrupt torsion of the chest and a valsalva maneuver . 
all of these aspects can lead to rectus muscle hematoma [ 8 , 14 ]  . the increase in the number of clinical cases is also due to the extended overall age length and to the major implementation of anticoagulant therapies in elderly people and arteriosclerotic patients . 
given the benefits that the therapy 1 3 956 radiol med ( 2015 ) 120 : 951958 guarantees in various clinical cases ( arterial fibrillation , deep vessel thrombosis and pulmonary embolia treatment ) , recently there has been an increase in patients undergoing double antiaggregation to obtain patency of vascular stents [ 2 , 5 , 6 , 14 , 15 ]  . it has been reported that there has been a threefold increase in female patients , due to less abdominal muscular mass [ 16 ]  . the rectus muscle bleeding can determine clinical symptoms according to the size of the hematoma : ranging from a weak abdominal pain with hematoma within the muscle to an acute strain pain with abdominal hematoma , the latter case presenting problems in the diagnosis phase , especially in pregnancy [ 1719 ]  . 
in particular , the physical examination of the patient could suggest a diagnosis , but the imaging gives a detailed pathology and allows to depict a non - pulsating mass , non - mobile despite the breathing , more or less depictable according to the patients obesity : the fothergills sign can be used to determine whether the mass is part of the abdominal wall ( the patient is in supine position and bends both head and legs at the same time , and the hematoma does not change with flexion but is more painful , and more stretched and even more depictable while an abdominal mass is less distinct and less stretched ) [ 13 , 20 ]  . in large rectus muscle hematoma , the purpose of standard diagnostic techniques , ultrasound ( us ) and ct , are used to reveal its real size and extension , but also to depict the existence of the active bleeding . in particular , us can show a different aspect of the hematoma according to its dating : solid or mixed mass ( non - homogeneous ) , liquid part or with septa . 
the intravenous contrast medium administration allows to depict the active bleeding : hyperdense focal areas in the hematoma during artery phase and the persistence of the bleeding in the late study phase [ 22 , 23 ]  . comparing clinical data and ct reports , it was possible to determine the size and severity of hematoma and divide it into three main groups : weak / type i , moderate / type ii and severe / type iii [ 24 ]  . brief , type i consists in an enlarged rectus muscle . 
the hematoma within the muscle creating a limited unilateral swollen area in the abdominal wall and the prognosis leads to a positive outcome , within a month , without the need of any type of surgery intervention . type ii is often a bilateral hematoma with blood loss between muscle and transversalis fascia with inside fluid levels linked to a significant fall in hemoglobit requires a short - term hospitalization period , to confirm the diagnosis and begin an appropriate medical treatment , e.g. , drainage and / or blood transfusion when requested . type iii is the case of a large hematoma , mainly as a consequence of a traumatic iatrogenic event , easily recognizable ( paracentesis , intracutaneous heparin injection , needle biopsy ) [ 2528 ] ; the patient requests hospitalization due to the worsening of general conditions ; there is a significant fall in hemoglobin , and hemodynamic stabilization may request not only medicines but also a surgical treatment and vascular therapy . all our patients treated belonged to type iii . with the multislice ct , it is possible to exactly visualize the course of the inferior epigastric artery , its perforating branches , and detect the location of the bleeding [ 29 ]  . there is usually a natural and good outcome in most cases of rectus muscular hematoma only through conservative therapy , with spontaneous self - limited evolution [ 14 , 16 , 30 ] ; vitamin k and platelets subministration are useful to stabilize the hemocoagulation status if the patient is undergoing heparin or protamine solphate . 
the decision of undergoing a blood transfusion depends on the patients hemodynamic status and the presence of other pathologies such as severe coronaropathy or anemia [ 31 ]  . despite correct medical treatment , some patients can develop a large hematoma causing a consistent hypovolemia or persistent bleeding , which requests an even more radical intervention . 
even if hematoma surgery evacuation and the bonding of concerned bleeding vessels have , in the past , been the most used procedures in hemostatic treatment of a severe rectus muscle hematoma [ 32 , 33 ] , with very good results , still it was quite difficult to identify the bleeding artery concerned . at present , the endovascular percutaneous treatment is the gold standard . 
selective catheterization , the use of micro - catheters and the versatility of embolization material allow a correct management in any type of situation [ 10 ]  . selective arteriography , being the first phase of percutaneous endovascular therapy , is the most useful image technique to identify the presence and location of the bleeding ; it provides information on the involved artery branches that support the bleeding and its exact location [ 34 , 35 ]  . 
the use of a micro - catheter allows to stop the bleeding in a precise and selective way reducing eventual dispersion of permanent embolization material or mechanical material . the material used is basically and exclusively coils , which allow a more precise handling at the given location , which immediately stops the bleeding , especially when little vessels are concerned . 
glue was used only in one of our cases , but we avoided further use of this material , due to difficulties encountered in the catheter removal . this technique must be used when bleeding is persistent , despite an adequate medical approach . 
it is known that hematoma can involve several blood vessels due to 1 3 radiol med ( 2015 ) 120 : 951958 the natural gap between inferior and superior epigastric arteries . for this reason , it is suitable to study in detail the origin of the bleeding and undergo embolization all around the bleeding location in order to stop the blood supply a tergo . our experience was similar to medical literature reports cases concerning isolate cases of spontaneous rectus muscle hematoma , with considerable hemodynamic alteration [ 2 ]  . 
levine max wintermark received : 21 april 2014 / accepted : 16 june 2014 / published online : 1 march 2015 italian society of medical radiology 2015 abstract purpose the aim of this study was to systematically compare a comprehensive array of magnetic resonance ( mr ) imaging features in terms of their sensitivity and specificity to diagnose cervical lymph node metastases in patients with thyroid cancer . materials and methods the study included 41 patients with thyroid malignancy who underwent surgical excision of cervical lymph nodes and had preoperative mr imaging 4weeks prior to surgery . 
using the pathology results as reference , the sensitivity , specificity and interobserver agreement of each mr imaging characteristic were calculated . results on multivariate analysis , no single imaging feature was significantly correlated with metastasis . 
wintermark department of radiology , centre hospitalier universitaire vaudois , lausanne , switzerland general , imaging features demonstrated high specificity , but poor sensitivity and moderate interobserver agreement at best . conclusions commonly used mr imaging features have limited sensitivity at correctly identifying cervical lymph node metastases in patients with thyroid cancer . 
a negative neck mr scan should not dissuade a surgeon from performing a neck dissection in patients with thyroid carcinomas . keywords thyroid cancer neck dissection metastatic lymph nodes mri accuracy introduction in patients with thyroid cancer , the presence of cervical nodal metastasis , a relatively common finding , is a negative prognostic indicator in patients older than 45 years of age and significantly impacts therapy . 
given the concerns regarding evaluating patients with contrastenhanced computed tomography ( ct ) due to iodinated contrast interfering with radioactive iodine uptake , alternative imaging approaches have been recommended including neck ultrasonography and magnetic resonance ( mr ) imaging . 
when assessing for cervical nodal metastasis , mri may have advantages over ultrasonography because of its ability to assess retrosternal and retropharyngeal lymph nodes , which cannot be evaluated by ultrasonography . a number of investigations have been performed regarding the mr imaging features of lymph nodes harbouring metastatic cancer , e.g. 
however , few studies have evaluated the characteristics of metastatic thyroid 1 3 960 radiol med ( 2015 ) 120 : 959966 cancer and mr imaging features have not been compared to each other either alone or in aggregate in terms of their accuracy to predict metastatic involvement . 
the goal of our study was to systematically evaluate all previously reported mr imaging features in terms of their diagnostic accuracy for cervical lymph nodal metastasis in patients with thyroid cancer . materials and methods study design with the approval of the university of virginia institutional review board who granted us a waiver of consent , we retrospectively reviewed medical records for all patients with a diagnosis of thyroid malignancy who underwent surgery in the department of otolaryngologyhead and neck surgery from june 2004 through march 2011 . 
of the 193 patients who met these criteria , 41 patients fulfilled the following inclusion criteria : ( 1 ) confirmed tissue diagnosis of thyroid cancer , ( 2 ) lateral and / or central compartment neck dissection completed and pathology results reported by level , and ( 3 ) preoperative mr imaging performed at uva within 4 weeks prior to neck dissection . 
at uva , all head and neck surgeons remove neck dissection specimens en bloc and place these specimens on a neck board that visually isolates the nodes at each level for histopathologic review . 
the neck board bearing the neck dissection specimen is transported to surgical pathology for processing where the specimen is divided into nodal levels based on its position on the board . 
the radiologists were blinded to each other , to the clinical information except for the presence of thyroid cancer , to the original clinical interpretation of mr studies , and to the neck dissection results . the reviewers assessed the quality of mr images as good ( 2 ) , intermediate ( 1 ) , or poor ( 0 )  . 
for each lymph node , they characterised as series of mr imaging features , including exaggerated enhancement , signal on t1 - weighted images , signal on t2 - weighted images , node shape , node size y , node size x , node size z , edge , vascular encasement , and necrosis . it was not possible to match exactly the lymph nodes characterised on imaging and the lymph nodes resected during surgery . 
for this reason , we did not perform a nodeby - node comparison , but rather level - by - level ( levels ivii ) and neck - by - neck ( right lateral nodes , left lateral nodes and central compartment nodes ) comparisons between imaging and histology , as detailed below . each level in each patient was assigned a single value for each imaging feature . 
for levels that did not show any lymph nodes , the size recorded was zero , and the imaging features listed above were all considered negative . a similar approach was used for the histology : a level was considered positive if any node within the level exhibited metastatic cancer on histopathology , and the level was considered negative if all the nodes at within the level were free of cancer . using the histology as a reference standard , we first performed a strict level - by - level analysis , comparing each level in each patient on imaging and on histology . 
given the possible variability in surgical and pathological assignment of nodal levels ( see above ) , a lenient level - by - level analysis was also performed , which considered that an abnormal lymph node noted on imaging in one level may have been surgically assigned to an adjacent level , e.g. 
 conversely , if all the lymph nodes at a particular level were negative on histopathology , the binary variable was assigned the value 0 . predictor variables the imaging characteristics assessed as potential markers for the identification of metastatic lymph node levels in patients with thyroid cancer were exaggerated enhancement , signal on t1 - weighted images , signal on t2 - weighted images , node shape , node size y , node size x , node size z , edge , vascular encasement , and necrosis . analyses binomial univariate analyses followed by a multivariate generalised estimating equation ( gee ) regression model were utilised to examine whether one or more of the aforementioned imaging characteristics were associated with histopathology . 
it is important to note that , unlike traditional logistic regression , which is commonly utilised to analyse partial associations between a binary outcome variable and a set of predictor variables , the gee model provides accurate regression parameter estimates even when the binary outcome data cannot be presumed to be uncorrelated , which in the present case is unlikely to be true , since multiple lymph node levels were examined per patient . 
the gee regression model variance and covariance parameters that were utilised in hypothesis testing were estimated via the huber and white sandwich estimator assuming within cluster measurement dependence [ 15 ]  . hypothesis testing with regard to hypothesis testing , the gee modified version of the type iii wald chi square statistic was utilised to test for significant partial associations between histopathology and imaging characteristics . 
 reported predicted probabilities for a positive metastatic lymph node histopathology classification were calculated based on the inverse - logit transformation of the gee multivariate regression model logit predictions . lenient levelbylevel analyses the level - by - level analysis was repeated allowing for discrepancies in the definition of the levels between imaging and surgery . 
more specifically , we repeated the analysis described above , this time considering that each of the levels was positive on histology if it contained a positive lymph node or if any of its immediate neighbour contained at least one positive lymph node . 
this lenient levelby - level analysis was designed to yield the best - case scenario results in terms of the accuracy of imaging , whereas the strict level - by - level analysis was designed to yield the worse case scenario results . neckbyneck analyses the diagnostic agreement analyses , when conducted based on the neck classification ( right neck , left neck and central neck ) , were carried out in exactly the same way as the diagnostic agreement analyses conducted based on the level classification . interobserver agreement analyses the analyses described above were conducted independently for the three reviewers , and the results are reported in the tables as the range of values for the three reviewers , to demonstrate the interobserver variability . 
statistical significance was set at 0.05. statistical software the genmod procedure of sas version 9.2 ( sas , institute inc . , cary , nc ) was utilised to conduct the gee regression analysis and the software of spotfire splus 8.2 ( tibco inc , palo alto , ca ) was utilised to conduct the diagnostic agreement analyses . results study patients a total of 193 patients were considered for enrolment in this study . 
the 41 patients in the study cohort represent 492 total neck levels ( 205 left , 205 right , and 82 central ) of which 260 levels demonstrated no nodes on mr imaging . 
the types of thyroid cancer and lymph node status for each are summarised in table 1 . the total number of lymph nodes that were surgically excised and underwent histopathological examination was table 1 distribution of lymph node status by thyroid cancer histological subtype thyroid cancer type papillary , follicular papillary variant follicular medullary total lymph node pathology 26 ( 76 % ) 2 ( 50 % ) lymph node pathology 8 ( 24 % ) 2 ( 50 % ) 0 ( 0 % ) 0 ( 0 % ) 2 ( 100 % ) 1 ( 100 % ) 28 ( 68 % ) 13 ( 32 % ) total 1 3 962 radiol med ( 2015 ) 120 : 959966 1 , 304 ; of these , 196 harboured metastasis and 1 , 108 were negative . 
of these 164 levels , 79 levels were positive for thyroid cancer metastasis on pathology , while 85 were negative ( table 2 )  . imaging studies all patients underwent t1and t2 - weighted sequences and post - contrast t1 imaging , except for one patient without postcontrast imaging . 
 in the multivariate analysis , no single mr imaging feature was independently significant ; however , a model built from all the features included in the multivariate analysis was significantly correlated ( p < 0.05 ) with the presence of metastatic disease . 
the overall accuracy across the three readers was similar and ranged from 49 to 56 % . lenient level - by - level analysis and neck - by - neck analysis the lenient level - by - level comparison yielded similar results to the strict level - by - level analysis , suggesting that errors in level identification in the operating room and surgical pathology have little impact on the correlation between imaging finding and histologically proven metastatic disease . 
as for the strict level - by - level approach , the models built from all the features included in the multivariate analysis were significantly correlated with the presence of metastasis . 
the overall accuracy was similar across the three readers for both the lenient level - by - level analysis ( 4955 % ) and the neck - by - neck analysis ( 5155 % )  . multivariate model the multivariate model including all imaging features ( conglomerated lymph nodes , node size , t1 signal , exaggerated enhancement , shape , as well as necrosis and encasement ) had an overall sensitivity and specificity of 3356 % and 9093 % , respectively . 
the patient without gadolinium administration has only one negative lymph node in right level two in bilateral neck b signal on t1or t2 - weighted images were assessed by comparing with the corresponding intensity of the sternocleidomastoid muscle discussion preoperative evaluation of thyroid cancer has conventionally included ultrasound of the neck to detect metastatic lymph nodes . 
the t1 hyperintensity is likely due to the presence of thyroglobulin within the metastatic lymph node nodes not easily accessed by ultrasound such as in the central compartment [ 17 ]  . 
however , preoperative contrastenhanced ct is discouraged in patients with differentiated thyroid carcinomas due to the concern that intravenous iodinated contrast agent could affect radioactive iodine uptake for months , thus interfering with postoperative radioiodine therapy [ 18 ]  . the other imaging options available include contrastenhanced mr imaging and fluorodeoxyglucose positron emission tomography ( fdg - pet ) imaging . 
the latter is best used in surveillance of treated thyroid malignancy especially in a setting of rising thyroglobulin levels when conventional radioiodine nuclear imaging and ultrasound are negative [ 19 ]  . 
 [ 21 ] , petct did not appear to confer a significant advantage over ultrasound or ct in the preoperative evaluation of lymphadenopathy from thyroid cancer . mr imaging , with its multiplanar capability and superior soft tissue resolution , appears to be an attractive alternative . 
also , gadolinium - based contrast medium does not interfere with future radioiodine administration [ 22 ]  . our study evaluated multiple imaging features of lymph nodes that have been previously reported as imaging predictors of lymph node metastasis . 
it demonstrates the post - contrast fat - suppressed homogeneous enhancement on t1 - weighted image lymph nodes with a sensitivity of only 41 % using the presence of cystic change and a size cut off of 13 mm [ 23 ]  . 
in a series of 26 patients with thyroid cancer studied by gross et al . , using the criteria of nodal size , t2 signal , cystic change and compression of adjacent structures , the average overall percent sensitivity , specificity , positive predictive value , negative predictive value , and accuracy of mr imaging were 95 , 51 , 84 , 78 , and 83 % , respectively . 
the three neuroradiologists who reviewed the study images were specialised in head and neck imaging , and they originally agreed on criteria to assess the different imaging features before reviewing the imaging studies independently . of note , our results apply mainly to papillary thyroid carcinomas , as these constituted the large majority of our study population . 
papillary thyroid carcinomas are the most frequent type of thyroid cancer and tend to spread to lymph nodes more so than the other types of thyroid cancers , making the issue of imaging diagnosis of metastatic lymph nodes in patients with papillary thyroid cancer particularly relevant . the quality of contrast - enhanced mr imaging was less than other sequences , most likely because these were the last sequences obtained and are therefore prone to motion artefacts . we acknowledge several limitations to our study . 
however , since none of the imaging features had a particularly high sensitivity , this was not an issue . in conclusion , individual mr imaging characteristics have limited sensitivity at identifying metastatic lymph nodes in patients with thyroid cancer . 
we analysed the technical feasibility , safety and efficacy of this treatment performed via an innovative transbrachial approach , rather than the traditional transfemoral approach . materials and methods between 2009 and 2013 , 115 patients were treated with embolization of the uterine arteries for one or more symptomatic leiomyomas . 
after having placed the tip of the angiography catheter at the level of l4 to check the aortic bifurcation , the uterine arteries were catheterised and embolized with calibrated particles . 
the time of occupation of the angiography suite was 118 ( range 95155 ) with the femoral approach , compared to 92 ( range 65123 ) with the transbrachial approach . 
no immediate complications involving the brachial artery were recorded . discussion in the treatment of symptomatic uterine fibromas , embolization of the uterine arteries performed via a transbrachial approach was shown to be safe and technically valid with regard to reducing the overall time of the intervention , ease of selective catheterisation , and shorter times spent in hospital , as well as being better accepted by patients . keywords leiomyoma embolization uterine arteries transbrachial approach introduction uterine leiomyomas are benign tumours that occur most frequently in women of reproductive age [ 1 ]  . 
although they are frequently asymptomatic , in more than 50 % of cases , affected patients present with menstrual cycle disorders , with symptoms related to compression of adjacent pelvic organs or to disorders of fertility or reproductive function [ 2 ]  . 
if medical management fails , there are valid surgical solutions , with asportation of the uterus or fibroma by a laparotomic or laparoscopic method , depending on the case [ 3 ]  . in 1995 [ 4 ] , embolization of the uterine arteries was described as a treatment for symptomatic leiomyomas ; since then this therapeutic option has gained widespread 1 3 760 radiol med ( 2015 ) 120 : 759766 popularity , becoming a valid part of the armamentarium of the specialist gynaecologist both because of its safety and efficacy [ 2 ] , but also because of its mini - invasiveness [ 5 ]  . in the context of contributing to less hospitalisation and a quicker return to activities for patients with the purpose of decreasing exposure to radiation , shortening occupancy of the angiography suite and facilitating selective catheterisation of the uterine arteries , we introduced a transbrachial approach for the treatment of symptomatic uterine fibromas , building on our substantial experience in venous conditions [ 68 ] , and compared this approach with the traditional transfemoral approach . 
initially used only occasionally in patients with very abundant adipose tissue or patients who refused a transfemoral approach for personal or religionrelated reasons , given the results , the new transbrachial approach became used systematically and routinely . we report here our preliminary experience , albeit limited to a small group of patients , mainly analysing the technical aspects , safety and exposure to radiation related to this alternative arterial access . materials and methods considering that embolization of uterine fibromas , using a transfemoral access , is performed regularly , the ethical committee was not requested to give permission for this intervention , since only the arterial access was modified ; however , the informed consent that the patients were asked to sign included the statement transbrachial access instead of transfemoral access . between 2009 and 2013 , 115 patients underwent embolization of symptomatic uterine fibromas in our department ; of these , only 20 underwent treatment via the transbrachial access . most of the patients were recruited by specialist gynaecologists in our hospital . 
all patients had expressed a desire to avoid surgery . we explored the transbrachial approach for many reasons : at the beginning for the overweight women , the first five patients [ difficulty in entering the femoral artery excessive depth of the vessellong time for uterine arteries catheterization ] and for resistance to the transfemoral access for religion or personal related reasons . 
given the results , then , we systematically used this approach in all the others . an endometrial biopsy was performed to ensure that none of the patients had a neoplastic disorder or an underlying infection . at the same time as the gynaecological examination , all patients underwent ultrasound investigations using a transvaginal probe , to confirm the clinical suspicion of a uterine fibroma ; subsequently all underwent magnetic resonance imaging [ advanto 1.5 teslasiemens , germany ] , which was considered a prerequisite for inclusion in the list of patients for subsequent embolization . 
the imaging protocol required a baseline study of the pelvis with axial and sagittal t1 and t2 weighted sequences , before and after administration of a contrast agent [ gadovistbayer healthcare , germany ]  . 
details were obtained of the type and site of origin of the uterine arteries and it was excluded that the ovarian artery contributed to the blood supply of the fibroma to be treated . the embolization of the uterine arteries was performed in the angiographic suite , after induction of profound sedation and the beginning of the pharmacologica protocol for the pain control [ continuous infusion of morphine 3 mg via an elastomeric pump , with anti - infiammatory drugs ] , started as soon as the first uterine artery had been catheterized . the embolization procedure , carried out on the same day as the planned admission , was performed in the first 10 days of the womans menstrual cycle , after having excluded the possibility of a pregnancy following unprotected sexual intercourse . 
in contrast to the 85 patients in whom a unilateral , percutaneous femoral approach was used , in the 20 of 115 women in whom the transbrachial approach was used , the artery was systematically punctured under ultrasound guidance to ensure that only the superficial wall of the artery was damaged . 
a bladder catheter was not placed in any of these 20 patients , in contrast with the practice in the other women . after having inserted a specific vascular introducer [ prelude short , 5 cm , 4 frmerit medical systems , utah , usa ] , on a hydrophilic guide [ standard version , 180 cm long , j tip , first 3 cm flexibleterumo europe , leuven , belgium ] , a specifically designed diagnostic catheter was introduced [ multipurpose 4 fr , 100 cm long , with lateral holescordis , miami lakes , florida , usa ] , to inject a first , small amount of contrast agent by hand [ optiray 320mallinkrodt italia , segrate , milan , italy ] , once the tip of the catheter reached the level of l4 . 
subsequently the uterine artery with the smaller diameter was catheterised , inclining the x - ray source , on the basis of the information already acquired from the magnetic resonance imaging . 
 once the vertical tract of the uterine artery was reached , another angiographic image was acquired to determine the anatomical characteristics , course and collateral circulation of the artery ; having identified the origin of the cervico - vaginal artery , this was crossed by the microcatheter [ progreat microcatheter system , 2.8 frterumo europe , 1 3 radiol med ( 2015 ) 120 : 759766 leuven , belgium ] whose proximal extremity was placed in the ascending tract of the artery . 
the particles had been mixed with contrast medium in order to make the embolization of the peripheral branches and initial reflux within the horizontal part of the artery clearly visible . 
the fluoroscopy times and data on exposure to radiation , drawn from the angiography equipment [ integrisphilips , germany ] were recorded immediately , while the data on occupancy of the angiography suite were obtained from the suites records . once the procedure had been completed and the introducer removed , the patient was sent to the ward . 
pain control was ensured by the continuous infusion pump and the prescription of non - steroidal anti - inflammatory drugs , antibiotics and analgesics every 6 h after the end of the continuous infusion . 
four of the 20 women treated via a transbrachial approach were not italians ( table 1 )  . metrorrhagia was the most common symptom , being present in 15 patients ( 75 % ) , while 11 ( 55 % ) women had dysmenorrhoea , and 8 ( 40 % ) had compression symptoms ; severe anaemia , requiring systemic intake of iron and derivatives was present in 9 ( 45 % ) patients , while 7 ( 35 % ) women had a haemoglobin concentration below 9 g / dl . 
 only two of the fibromas were intramural with strictly submucosal growth and invasion of the endometrial cavity ; the others were intramural , with only one patient having a subserosal growth which deformed the outline of the uterus , but which was not pedunculated . 
all the fibromas showed intense uptake in the arterial phase , with an increase in the magnetic resonance signal intensity , which enabled a clear demarcation from the uterus . in all 20 patients treated with the transbrachial approach , selective catheterisation of the uterine arteries was achieved easily with the angiography catheter , using the information deduced from the magnetic resonance angiography to incline the x - ray tube appropriately . 
the mean time to catheterise the uterine arteries via the transbrachial access was 25 ( range 1245 ) , compared to 72 ( range 35125 ) using the femoral approach . 
the time of occupancy of the angiography suite , including entrance of the patient and cleaning the suite , was 118 for the transfemoral approach ( range 95155 ) compared to 92 ( range 65123 ) for the transbrachial approach . no complications , infections or brachial haematomas associated with the procedures were recorded . 
the mean time spent in hospital was 1.8 days , which was shorter than the mean of 2.4 days required by the patients who underwent the embolization procedure via a femoral approach . the patients were followed up at 3 , 6 , and 12 months ; symptoms improved in 19 / 20 ( 95 % ) , with disappearance of abdominal pain , regularisation of the menstrual cycle , and return to normal activities with recovery of quality of life . 
the reduction in the volume of the uterus , evaluated by magnetic resonance imaging with measurements in three planes ( anteroposterior , lateral and longitudinal ) , was 35 % at 3 months , while the reduction in the size of the dominant fibromas was greater than 50 % at 3 months in 12 / 20 patients ( 60 % ) and less than 40 % in 4 / 20 ( 20 % ) ; in 4 / 20 ( 20 % ) cases the dominant fibroma disappeared completely . 
during the 1 - year follow - up , no women required further gynaecological interventions ; one woman above the age of 45 had transient amenorrhoea ( 2 months )  . in the seven women who underwent echo - colour doppler follow - up 1 year after the endovascular intervention , no changes were found in the morphology or blood flow of the brachial artery . discussion uterine leiomyomas are a major problem in gynaecology . 
they are associated with two types of problems : changes in the characteristics of the menstrual cycle and problems with fertility [ 1 ]  . they are associated with a broad range of symptoms . 
 although they can be asymptomatic and found incidentally , they often present with changes in the menstrual cycle and / or marked loss of blood with weakness and impaired quality of life because of a debilitating chronic anaemia , abdominal pain during the menstrual cycle and symptoms due to compression of the adjacent pelvic organs [ 2 ]  . medical therapy alone has been shown to be valid in the short - term control of symptoms ; gonadotropin releasing hormone antagonists cause shrinkage of fibromas and a reduction in symptoms within 23 months , but their effect is limited in time and so suspension of these antagonists leaves the problems unaltered , if not worsened [ 3 , 9 ]  . 
our patients had been treated in this way ; despite a significant , initial improvement in symptoms , after 23 months the women were forced to increase the dose to maintain good clinical control and the onset of side effects necessitated suspension of the medical treatment which was followed by reappearance of the symptoms , sometimes with increased intensity . traditionally , surgery , in the form of hysterectomy , has been the definitive therapeutic solution to the problem ; this drastic solution is not , however , suitable in young women who still want to have children . 
nevertheless , besides the problem of regrowth of the fibroma , this strategy does have problems related to the less than perfect integrity of the uterine wall , which could necessitate caesarean section during labour , and the formation of adherences , which could complicate future surgery [ 5 ]  . 
in our group of 20 women , three had previously undergone myomectomy which had been ineffective . in the last few decades , less invasive therapeutic solutions have been proposed , including embolization of the uterine arteries , which has been reported to be a valid , less invasive alternative to surgery [ 10 ]  . 
first described in 1995 [ 4 ] , numerous studies have demonstrated the safety and clinical efficacy of this strategy [ 5 ]  . briefly , it is a therapeutic option performed via a percutaneous route , guided by imaging techniques and carried out by expert interventional radiologists . 
it involves placing an angiography catheter within the uterine arteries , usually through a unilateral or bilateral femoral access , and then releasing an embolizing drug [ 1 ] , for example hydrophilic particles of predetermined calibre , as in our case . the right femoral artery , closer to the operator , is usually the preferred approach , because it makes the procedure easier [ 11 ]  . 
replacement of the angiography catheters to treat the uterine arteries on both sides , difficulties related to catheterisation and the prolonged times to inject the embolizing drug have stimulated research into alternative solutions to shorten the time the patient is exposed to radiation ; such alternatives include a bilateral femoral approach and the presence of two operators to carry out the embolization contemporaneously [ 12 ]  . we started to use the transbrachial approach , which is not an absolute novelty in uterine embolization [ 9 ] , after a critical review of the difficulties encountered during a procedure in a woman with a large amount of adipose tissue : 1 3 radiol med ( 2015 ) 120 : 759766 the depth of the femoral artery prevented easy identification of the vessel by palpation ; furthermore , the deep position of the artery necessitated the use of longer needle than the traditional seldinger one ; the adipose tissue hampered the movements of the angiography catheter and its replacement . 
in the search for an alternative solution , and also to resolve the first case of a woman who wanted to undergo embolization of the uterine arteries instead of surgery , but who was very resistant to a femoral approach for religious related reasons , we chose the brachial access rather than the radial route , widely used in haemodynamics . we , therefore , carried out the first transbrachial access , under ultrasound guidance in order to puncture only the superficial part of the artery so that the procedure was less traumatic and compression was easier at the end of the procedure . 
in our opinion , this access provides a good compromise between the calibre of vessel in which to work , ease of puncture , characteristics of mini - invasiveness and possible outpatient performance of the intervention . 
in fact , with early walking , feasible already 23 h after the transbrachial embolization , the patient can safely avoid the placement of a bladder catheter and its related complications , thus enabling autonomous management of body functions , without the embarrassment of requiring the help of someone else . 
 furthermore , the fact that the patient can see the percutaneous brachial access leads to more frequent control of haemostasis compared to that of a femoral access , which must be inspected by nursing staff . 
given the clear advantages , including easier catheterisation , of the transbrachial approach , following the first , occasional use of this technical solution , we wanted to use it systematically also to determine whether the related exposure to radiation and its safety were favourable . as far as concerns the shape of the angiography catheter , while the bilateral femoral approach involves the contemporaneous use of two catheters , generally cobra - shaped , the unilateral femoral approach requires the use of two different catheters , cobra - shaped for the contralateral uterine artery and sidewinder 1 for the ipsilateral one . 
the time required to exchange the catheters on the guidewire obviously increases the fluoroscopy time , the overall duration of the intervention and the time that the angiography suite is occupied . 
although using only a sidewinder shortens the overall duration of the intervention , this necessitates the systematic use of a microcatheter to ensure the selectivity of the intervention . the transbrachial access and the use of a multipurpose 4 fr catheter , 100125 cm long , undoubtedly have practical advantages . 
1 from the percutaneous approach at the level of the brachial artery , the hydrophilic guide wire , entered through the introducer , was easily able to continue into the descending thoracic aorta , since the straight course that this vessel has in young patients . 
the tortuosity of the vessel and the view of the arterial blood flow , allowed by the bulk of the angiography catheter itself , will determine whether the embolization can be completed with only this catheter or whether a sophisticated , expensive microcatheter must be deployed . 
2 preceded by the guide wire , the multipurpose angiographic catheter is brought up to the level of the origin of the internal iliac artery , usually the one with the lower calibre , preferring before to deal with the more difficult one , leaving the most hypertrophied for the second part of the embolization of the uterine arteries fig . 
4 to use the push of arterial flow , in this patient , it is preferred to advance the microcatheter until the ascending segment of the uterine artery , bypassing the emergency of the cervico - vaginal artery , withdrawing back the diagnostic catheter only few centimetres . 
in this way you can have more certainty on the performance of microcalibrated particles and obtain a more accurate embolization , not distorted by artificial reduction of arterial flow fig . 
3 due to the extremely low calibre and orientation of the catheter tip , in certain cases , when the arteries are hypertrophied , the 4 fr diagnostic multipurpose is adequate to perform the selective catheterisation of the uterine arteries obstructive angiographic material and echo - colour doppler documentation of the integrity of the brachial artery , and normal blood flow within it , at 1 year after the embolization . this study has some limitations . 
5 at the end of the procedure , control arteriography , done 5 after the end of the embolization , confirms the fibroid devascularization 1 3 radiol med ( 2015 ) 120 : 759766 fig . 
6 pre - embolization assessment with sagittal tse t2w ( a ) , axial tse t2w ( b ) , and sagittal post - gadolinium tse t1w ( c ) sequences , demonstrating the presence of a bulky intramural / subserosal fibromatous growth , about 5 5.2 cm , in the posterior wall of the uterine body . 
post - embolization magnetic resonance assessment 6 months after the procedure , with sagittal , post - gadolinium tse t1w ( d ) and axial post - gadolinium tse t1w ( e )  . 
the mini - invasiveness ensured by the femoral approach can be further improved by the transbrachial approach , which has been demonstrated to be better accepted by the patients and facilitates early ambulation , without adversely affecting the clinical results . 
 additionally , signal - to - noise ratio ( snr ) , contrast - to - noise electronic supplementary material the online version of this article ( doi : 10.1007 / s11547 - 015 - 0508 - 2 ) contains supplementary material , which is available to authorized users . ratio ( cnr ) , and apparent diffusion coefficient ( adc ) values for normal gland , benign and malignant lesions were compared . 
although these lesions were seen with both techniques , dwi - spair evidenced higher score for lesion visibility in nine of thesnr and cnr were comparable , except for snr in benign lesions ( p < 0.01 ) , which was higher for dwi - spair . 
nogueira school of applied health sciences , oporto polytechnic institute ( estsp / ipp ) , rua valente perfeito , 322 , 4400 - 330 vila nova de gaia , portugal r . 
to date , most of the published work relates to apparent diffusion coefficient ( adc ) quantification at 1.5 t [ 1 , 2 ] , and publications focusing on 3.0 t are still scarce . 
also , signal - to - noise ratio ( snr ) and contrast - to - noise ratio ( cnr ) are strongly correlated with the quality of fat suppression . 
chemical shift selective ( chess ) pulses are easily included in most pulse sequences but work poorly in regions with inhomogeneous b0 [ 4 ] , which may lead to insufficient fat suppression , especially when compared to short ti inversion recovery ( stir ) [ 5 ]  . 
as stir uses a spatially selective 180 rf pre - pulse with short inversion time to suppress lipid signal , it is a more robust approach to cope with b0 inhomogeneities and susceptibility changes [ 36 ]  . 
nevertheless , the fact that stir leads to an inherent t1 - weighting , suppressing signal from tissues with t1 similar to fat is a limiting factor to its use . in the case of spectral pre - saturation with inversion recovery ( spir ) and spectrally attenuated inversion recovery ( spair ) , spectral pre - saturation pulses are added to the inversion recovery module [ 7 ]  . 
for t1or t2 - weighted fat suppression , spair uses adiabatic ( frequency - varying ) inversion pulses [ 8 ] to invert fat spins , and a spoiler to destroy any residual transverse magnetisation . 
this process reduces the effect of b1 inhomogeneities , which are frequent on high - field mri , but increases rf absorption rate [ 9 ]  . given that signal intensity may depend on the fat suppression technique , different options for breast dwi should be considered in the clinical setting , since it may affect lesion identification and the demarcation of the region - ofinterest ( roi ) to calculate the adc . 
this may have a true impact on lesion classification , as the adc value is used to distinguish benign from malignant lesions [ 10 , 11 ]  . therefore , the purpose of this study was to compare stir and spair for breast dwi at 3.0 t , through the evaluation of the homogeneity of fat suppression and lesion detection , snr and cnr . 
the focus was to evaluate lesion classification by investigating the influence of several parameters of dwi , namely the best set of b values , the fat suppression technique , and signal intensity fitting models . this preliminary study was carried out between july 2009 and january 2010 , and includes the first sets of data . 
single - shot - se - epi - stir and - spair pulse sequences with multiple b values were acquired unilaterally in the sagittal plane for both breasts before gadolinium injection . 
total examination time was approximately 38 min . image analysis a senior radiologist , with 5 years experience on breast mri ( j.l. ) prospectively reported the clinical mr examinations according to the birads - mri lexicon [ 14 ]  . conventional and dwi pulse sequences were transferred to a workstation . 
uniformity of fat suppression was encoded as follows : 0homogeneous fat suppression ; 1evidence of heterogeneous fat suppression , though with no impairment in lesion analysis ; 2images with major fat suppression problems that make lesion identification unfeasible . 
lesion visibility was scored by using : 0lesion is not seen ; 1lesion is poorly seen , requiring t1 - w postcontrast images for identification ; 2lesion is visible , but not as conspicuous as in t1 - w post - contrast images ; 3the lesion is easily visible , equivalent to t1 - w post - contrast images . 
for uniformity of fat suppression , the score of 0 was opposed to scores 1 and 2 that were grouped ( given that for either , fat suppression was not homogeneous )  . 
additionally , the strength of agreement between stir and spair was assessed for the two variables . quantitative assessment using the stir and dynamic contrast - enhanced images for visual guidance , fixed circular 0.25 cm2 regions - ofinterest ( rois ) were manually drawn on the b400 s / mm2 diffusion images , and then copied on to the other b values and the adc map . 
of malignant lesions size of malignant lesions ( mm ) malignant histopathological subtype ductal carcinoma in situ ( dcis ) lobular carcinoma in situ ( lcis ) invasive ductal carcinoma ( idc ) invasive lobular carcinoma ( ilc ) mucinous carcinoma other malignant ( nos ) a no . 
the wilcoxon rank test was used to compare the mean values of signal intensity , snr , cnr and adc for each of the fat suppression techniques and tissues ( normal fibroglandular tissue , benign and malignant lesions )  . 
 the differences in the adc values between benign and malignant lesions for each fat suppression technique were assessed by the mannwhitney test . the adc optimal cutoff point was selected based on the receiver operating characteristic ( roc ) curve . 
statistical significance was considered for p < 0.05. results subjects and lesions dce dynamic contrast enhancement , dwi - spair diffusion - weighted imaging - spectrally attenuated inversion recovery , dwi - stir diffusion - weighted imaging - short tau inversion recovery , n absolute number , sd standard deviation a other malignant lesions ( nosnot otherwise specified ) fibroglandular tissue demarcation , the roi was positioned in the mid - sagittal slice , behind the nipple and avoiding fat . 
the selection of the b400 s / mm2 images was based on a compromise of having image contrast between the lesion core and its outer limits , but still higher snr than that of b1 , 000 s / mm2 . snr and cnr for each type of lesion and normal fibroglandular tissue ( measured on the contralateral breast ) were calculated at b1 , 000 s / mm2 using the appropriate equations [ 15 , 16 ]  . 
a descriptive analysis was used to characterise from the 51 patients initially enrolled in this study , four were excluded due to the presence of motion artefacts on the dwi , which prevented image analysis . 
morphological ( left column ) and dwi - stir ( diffusion - weighted imaging - short tau inversion recovery ) and - spair ( spectrally attenuated inversion recovery ) images ( b50 s / mm2 ) and the corresponding apparent diffusion coefficient ( adc ) maps show a large tumour in the upper quadrant ( arrowhead ) with diffusion restriction and low adc . 
susceptibility artefacts in the interface between the adipose and the fibroglandular tissues ( black arrows ) , as well as in the anterior thoracic wall ( white arrows ) are far more evident on the dwi - spair images all the lesions detected on dwi were visible on both sequences . 
 at b1 , 000 s / mm2 , which is the most frequently used diffusion - weighting factor , p values were p 0.001 , and p 0.02 for fibroglandular tissue , benign and malignant lesions , respectively . 
two more false positives were found for dwi - stir ( two fibroadenomas , two fibrocystic changes , one epithelial proliferative lesion , one sclerosing lesion ) , than for dwi - spair ( two fibroadenomas , one fibrocystic change and one epithelial proliferative lesion )  . 
 both techniques detected four false - negative cases : one mucinous carcinoma , and three invasive ductal carcinoma for dwi - spair ; and one mucinous carcinoma , one ductal carcinoma in situ , and two invasive ductal carcinoma for dwi - stir . discussion papers regarding breast dwi at 3.0 t are still scarce , but this field strength seems to be advantageous for characterising breast lesions [ 1922 ]  . 
also , recent scanners can apply dual - source rf excitation with independent rf shimming that improves signal homogeneity and fat suppression by reducing the dielectric effects , thus enabling the use of short trs and low rf absorption rate ( sar ) [ 23 , 24 ]  . in our study , there were no major fat suppression problems in the dwi datasets that prevented lesion identification . 
to maximise scanning success rate , we have established some strategies to improve image quality , such as the use of volume shimming , manual lipid frequency peak identification , small field - of - view and the use of parallel imaging [ 2 ]  . 
dwistir outperformed dwi - spair in fat suppression homogeneity in six cases , which was most probably related to its higher insensitivity to b0 inhomogeneities and susceptibility artefacts [ 36 ]  . ninety percent of the lesions were detected in both sequences , in accordance to what was found by other authors [ 1 , 26 ]  . 
 [ 19 ] found high visibility scores at 3.0 t even for lesions smaller than 10 mthe minimum lesion size on dwi in this study , as defined by the longest dimension on the dynamic acquisition , was 7.4 mm , which is acceptable considering the 5 - mm slice thickness . 
a decrease in the slice thickness to 34 mm could have enabled the detection of even those small lesions , although at the cost of lowering the snr . normal fibroglandular tissue presented lower signal intensity when compared to lesions at b1 , 000 s / mm2 , due to a less compact structure and good suppression of the fat component . 
we found higher signal intensity , snr and cnr values on dwi - spair when compared to dwistir , although not all statistically different , an exception being the snr for benign lesions . 
even though these results could perhaps be related to the variety of their histological types , this can potentially be explained by the fat suppression technique itself [ 27 , 28 ] , as all other geometric and timing parameters were kept the same . 
moreover , most tissues recover more slowly than fat and , therefore , the snr decreases . as in other studies , malignant lesions presented higher snr and cnr at 1 , 000 mm2 / s when compared to benign ones in both sequences , due to their increased cellular components and diffusion restriction . 
 [ 30 ] at 3.0 t found a 1 3 radiol med ( 2015 ) 120 : 705713 higher cnr for malignant lesions at b850 and b500 s / mm2 , respectively . 
the histological type of the lesions or the fat suppression technique may explain these differences , as the authors used dwi - stir and dwi - special ( spectral inversion at lipid ) ( similar to spir ) pulse sequences , respectively . the adc value is used to differentiate between benign and malignant breast lesions . 
two more false positives were found for dwi - stir ( two fibroadenomas , two fibrocystic changes , one epithelial proliferative lesion , one sclerosing lesion ) than for dwi - spair ( two fibroadenomas , one fibrocystic change and one epithelial proliferative lesion )  . 
the additional complex sclerosing lesion found when the dwi3 mm2 / s may be assostir cutoff point was 1.49 ciated to the presence of different fibrotic degree and proliferative cell activity that constrain water diffusion and decrease the adc value [ 3740 ] that , in our study , was similar to malignant lesions . 10 concerning the false negatives , both techniques showed four misclassified lesions , three of which were misleading lesions in the same patients ( one mucinous carcinoma and two invasive ductal carcinomas )  . 
the high adc of mucinous carcinoma may be due to the presence of mucus in the extracellular space and the decreased cellularity [ 3 , 37 ] , whereas invasive ductal carcinomas are often heterogeneous and have haemorrhagic focus . 
the false negative on dwi - stir was a low - grade ductal carcinoma in situ , which may have ambiguous signal intensity , even at higher b values , due to rapid signal decay [ 10 , 26 , 41 ]  . there are certain limitations in our study . 
second , the scanning time for the clinical protocol and both the dwi - stir and - spair sequences was almost 40 min , resulting in a few cases of motion artefacts . 
however , an optimised acquisition with only two b values ( b50 and 1 , 000 s / mm2 ) would enable reducing the te and shorten the acquisition time . 
although performing two unilateral acquisitions may increase the scanning time , the use of small field - of - view for sagittal imaging enables good spatial resolution , better volume shimming and less magnetic susceptibility phenomena . to further complement our results , a comparative analysis of nonparallel imaging will be performed , to check its benefit on image quality . 
this method seems promising , achieving homogenous fat suppression with reduced acquisition time and sar , which is particularly beneficial at high field strength . even though stir enabled more homogeneous fat suppression , spair provided better visibility for some lesions . 
with the help of built - in dual - source ct perfusion software , color perfusion images of hepatic arterial perfusion ( hap ) , portal vein perfusion ( pvp ) and hepatic arterial perfusion index ( hapi ) of all hcc lesions were obtained , and the above perfusion parameters were measured on the color images . 
lower hap and hapi and higher pvp were observed in active cancer tissues after operation as compared with those before operation . conclusions the 320 - row ct upper abdominal one - stop examination can display the whole liver perfusion well , especially the abnormal perfusion of hcc tissues and postoperative active tissues . 
270 , rongdu avenue , jinniu district , chengdu 610083 , sichuan , china e - mail : gumingchd@126.com keywords hepatocellular carcinoma computed tomography 320 - detector row ct perfusion introduction hepatocellular carcinoma ( hcc ) is the most frequent primary malignancy of the liver . 
in the past decades , the management of hcc has improved substantially , and nowadays , patients also with advanced stages of disease can be offered an effective treatment [ 1 ]  . 
transcatheter arterial chemoembolization ( tace ) is the current standard of care for patients with unresectable hcc , which takes advantage of the well - known hypervascular characteristic of hcc . 
intraarterial injection is followed by embolization of the feeding blood vessels , thereby inducing tumor necrosis [ 24 ]  . obtaining triple - phase ct of the liver is mandatory to integrate clinical and laboratory data in evaluating the appropriateness and the therapeutic effect of tace for hcc . 
developments in ct technology , especially optimized detector geometry with thinner slice collimation and increased gantry rotation speed , have improved temporal and spiral resolution as well as visualization of small abdominal vessels and detection of anomalies . 
recently , a new generation of ct systems with 320 - detector rows ( area - detector ct or adct ) has become clinically available and is capable of performing volumetric imaging . 
these systems provide a single rotational acquisition , which covers 16 cm in the z - direction , and avoids inter - slice stitching artifacts and data interpolations , which is a substantial improvement over standard helical ct acquisitions using singleand multi - detector row ct systems . 
with this 1 3 radiol med ( 2015 ) 120 : 690694 system , a complete volume data set covering the entire heart and / or brain can be acquired at a single rotation , and several investigators have discussed the utility of adct for cardiac and brain imaging [ 58 ]  . 
however , there are few reports about the application of this technique for assessment of liver diseases and therapeutic effects of tace . the purpose of this study was to evaluate the clinical value of 320 - detector row ct in tace treatment for hcc . materials and methods patient population the study was performed in accordance with the ethical principles of the declaration of helsinki . 
surgical therapy or radiofrequency ablation was not indicated according to the interdisciplinary clinical tumor board . exclusion criteria of this study were : ( a ) thrombosis of the portal vein , ( b ) extrahepatic metastasis , ( c ) cardiac failure , ( d ) liver cirrhosis child c , and ( e ) known allergic reaction to contrast agents . ct scanning examinations all examinations were performed with a 320 - detector row ct ( aquilion one ; toshiba medical systems , ohtawara , japan ) by means of volumetric scan mode . 
a 19 - gage catheter was placed in the antecubital vein and 70 ml of nonionic contrast material ( iopamiron 370 ; bayer health - care , guangzhou , china ) was administered at a rate of 7 ml / s with a power injector ( ulrich , germany ) , followed by 20 ml of saline chaser . 
x - ray cube current of 100 ma was selected for larger patients with 350 m the a field of view of more than 300 mm first seven scans were performed every 2 s for 30 s . 
the examination was repeated in all patients using the same technique before and 4 weeks after tace . ct image data processing the ct images were then transferred to a prototype workstation ( toshiba medical systems ) , and ct perfusion 3.0 ( ge medical systems ) was used for analysis . 
a reference arterial input curve was obtained by placing a region of interest ( roi ) in the aorta ( range 1015 mm2 ) manually , and a reference input curve of portal vein was obtained by placing a roi in the portal vein ( range 812 mm2 ) manually . 
subsequently , hepatic arterial and portal vein perfusions ( hap and pvp ; ml / min / 100 ml ) and hepatic arterial perfusion index ( hapi , % ) were calculated with the two - input maximum slope method . tace technique all patients underwent tace with palliative intention . 
after access to right femoral artery with standard seldinger technique , the angiography of celiac artery trunk and superior mesenteric artery with 5 - f yashiro catheter was conducted to map the arterial hepatic anatomy , respectively , as well as selective hepatic arteriography when necessary . 
the total volume of emulsion was judged by tumor size and achievement of stagnant arterial flow . statistical analysis standard deviation results obtained were given as mean ( sd )  . 
no major adverse effects were observed in this study . there is an increasing trend in the application of perfusion ct in the field of oncology including lesion characterization , diagnosis of occult malignancies , and provision of prognosis and monitoring the efficacy of treatment [ 9 ]  . 
the 320 - detector row ct covered 16 cm in the z - direction and almost the whole upper abdomen was scanned by means of serial rotational acquisitions at a single location in the z - direction . 
scanning with this ct provided isotropic and isophasic anatomical and functional information of all the organs in the upper abdomen or certain organs [ 5 , 10 , 11 ]  . 
 this was of great advantage , because it not only eliminated the errors caused by patients horizontal movements and time differences in the process of the images , but also avoided additional radiation exposures that were present in spiral scanning . 
it can , therefore , be seen that 320 - detector row ct scanning is a promising method for the evaluation of hemodynamic changes in hcc microcirculation . the implementation of adct in routine clinical practice has led to the suggestion that the wider cone - beam angle and scattering radiation result in misaligned geometry on the adct images . 
although image degradation may be due to misaligned geometry and cone - beam artifacts , our results indicate that adct with one - step scanning of livers provides excellent liver vascular images that are at least equivalent to those obtained with 64 - detector row ct system , and can be used for preand post - treatment assessment of tace on hcc . normal liver obtains 7080 % of its blood supply from the portal vein and the remaining 2030 % from the hepatic artery . 
in our study , the data on ct perfusion , including values of hap , pvp and hapi , were consistent with the previous finds [ 15 ] , indicating that hcc can cause direct or relative increases in arterial perfusion . in oncology , evaluation of treatment efficacy is crucial . 
in terms of treatment evaluation , hcc shows a fall in blood flow , blood volume and permeability after antiangiogenic therapies or transarterial chemoembolization [ 18 , 19 ]  . 
the decreased hap and hapi within liver tumors indicate the reduction of vascular capacity and microvessel density , which are due to the lipiodol embolisthe value of pvp was increased after treatment , suggesting involvement of hepatic portal vein during tumor advancement . however , there are some limitations to this study . 
however , manually obtained blood samples from the peripheral arteries are used for the estimation of arterial input , and this is a slightly invasive technique and the differences between peripheral and visceral arteries may lead to errors in perfusion estimates . 
median kaplanmeier survival was 11.0 months ( 95 % confidence interval : 8.014.0 months ) overall and 12.0 months in liver - only disease ( lung micro - nodules )  . 
angelelli e - mail : bruna.angelelli@aosp.bo.it 1 3 768 radiol med ( 2015 ) 120 : 767776 keywords colorectal cancer liver metastases radioembolization yttrium - 90 selective internal radiation therapy sirt introduction colorectal cancer represents the second most commonly diagnosed cancer and is second only to lung cancer as the most common cause of cancer - related death in europe [ 1 ]  . 
for those eligible for hepatic resection , 3 - year survival rates of 6074 % are a realistic expectation compared with 3 - year survival rates of 19 % or less with chemotherapy alone [ 3 , 4 ]  . 
radioembolisation using yttrium - 90 ( 90y ) - bound resin microspheres as the local radiation source is a form of intra - arterial brachytherapy for liver - dominant mcrc which is characterised 90 % when applied as a by high disease control rates of first or second line associated with chemotherapy [ 1315 ] and 5272 % in the salvage setting [ 16 , 17 ]  . 
in this paper , we report on target lesion response in the liver , safety and survival following radioembolisation for chemotherapyrefractory liver - dominant mcrc . materials and methods study design this study was a prospective case series evaluation of 52 consecutive patients with liver - only or liver - dominant mcrc who were treated with 90y - re at a single centre . 
study endpoints were target lesion response ( using the choi criteria ) , median kaplanmeier estimates of survival and safety . patients and treatment the decision to treat patients using 90y - re was only undertaken after a detailed pre - treatment work - up and the collective assessment of patients by a multidisciplinary tea all patients had an eastern cooperative oncology group ( ecog ) performance status of < 2 , normal liver ( total bilirubin < 1.5 mg / dl , serum albumin > 3.5 mg / dl and aspartate transaminase ( ast ) / alanine transaminase ( alt ) less than four times the upper limit of normal ) and bone marrow function ( leukocyte count > 500 / mm3 , platelet count > 100 , 000 / mm3 ) and adequate renal function ( creatinine < 1.5 mg / dl )  . 
immediately after the angiographic study , patients were transferred to nuclear medicine , and while the catheter was in still place , 45 mci of technetium - 99m - labelled macroaggregated albumin ( 99mtc - maa ) was administered intra - arterially . 
 liver - to - lung shunting was assessed using a planar single photon emission ct ( spect ) gamma camera to ensure that the lung - shunt fraction did not exceed 20 % . 
with the data obtained from the liver volume and liver - lung shunting , the activity of 90y - resin microspheres ( sir - spheres microspheres , sirtex medical , sydney , australia ) was calculated using the body surface area ( bsa ) methodology [ 18 ]  . 
within 2 weeks of the pretreatment work - up , selective or superselective hepatic intra - arterial infusion of 90y - resin microspheres was performed according to the preset dose , and targeted treatment confirmed by ct / positron emission tomography ( pet )  . 
1 a the pretreatment computed tomography ( ct ) scan showing liver colorectal cancer metastases ( mcrc ) in the iv segment as visualised in the arterial phase and in the portal - venous phase in a patient who had had a prior right lobectomy . 
b the pretreatment angiogram carried out with selective catheterisation of the left hepatic artery confirms the lesions in the iv segment ; in this patient , prophylactic embolisation with microcoils ( arrow ) of the right gastric artery was performed to minimise the risks of hepatoenteric flow . 
all patients had received standard - of - care systemic chemotherapy for mcrc and the majority ( 94.9 % ) had received 2 prior lines of chemotherapy ( fluoropyrimidine plus oxaliplatin and / or irinotecan , with or without bevacizumab , cetuximab or panitumumab ) , with 18 patients ( 46.2 % ) receiving 3 lines . 
disease control in the target lesions was still evident in 4 patients at 912 months post - 90y - re , including three patients who continued to have a pr in target lesions . progression in nontarget lesions occurred in 88.5 % ( 23 of 26 patients ) , and 86.7 % ( 13 of 15 patients ) at 3 , and 6 months after treatment , respectively . 
early adverse events reported in all 52 patients within the first 24 h of the procedure included : mild fever ( 12 patients ; 23 % ) , abdominal pain ( 9 patients ; 17 % ) , and asthenia ( 3 patients ; 6 % ) which persisted for some days after treatment . 
subsequent adverse events thought to be related to the nontarget distribution of 90y - resin microspheres were radioembolisationinduced liver disease ( grade 1 ulceration ) ( 1 patient ; 2 % ) , radiation gastritis ( grade 2 ulceration ) ( 1 patient ; 2 % ) and gastric ulcer ( grade 3 ulceration ) ( 1 patient ; 2 % )  . 
long - term responses ( pr of target lesions at 912 months ) were also recorded in three patients who survived a median of 41 months post - re ( without further liver - directed treatment )  . 
we found that both number and spread of lesions across the liver were significant predictors of survival varying from 8 months in patients with bilobar ( and / or > 5 liver lesions ) to 1516 months in patients with lobar ( and / or 25 lesions ) and > 26 months in patients with < 2 nodules . 
this echoes the results of the recently published metastatic colorectal cancer liver metastases outcomes after radioembolization ( more ) study in > 600 patients which identified both disease stage ( extrahepatic metastases , extent of liver involvement ) and liver function as statistically significant independent variables for survival at the time of 90y - re [ 27 ]  . 
many surgical studies in mcrc have also shown that even with complete resection of lesions in the liver , the durability of response and subsequent survival is determined by the number and size of the lesions in the liver as well as the presence of regional lymph node metastases [ 4 , 28 , 29 ]  . 
with increasing lines of chemotherapy , the proportion of patients with liver - only disease becomes more and more rare with survival diminishing proportionally after 90y - re [ 30 ]  . 
for this reason , a number of groups have evaluated 90y - re with either single ( 5fu ) [ 26 ] or double chemotherapy ( modified folfox or folfiri , with or without the resumption of anti - vegf / egrf 6 weeks postre ) [ 31 ] to delay progression of nontarget lesions even in chemotherapy - refractory patients . 
ongoing study of minimally invasive procedures such as thermal percutaneous ablation for the management of discrete small liver metastases , an addition to therapies such as radioembolisation , is also a promising area of ongoing research [ 32 ]  . overall , we found that 90y - re was well tolerated with a low incidence of severe grade 3 procedure - related events [ 3 patients ( 6 % ) ] , which is consistent with the findings from a recent systematic review [ 33 ]  . 
 notably , the choi criteria have recently been found to correlate well with metabolic treatment response evaluated by 18f - fluorodeoxyglucose ( fdg ) - pet [ 35 ]  . 
however , early post - radioembolisation ct imaging artefacts at 46 weeks such as peri - tumoural oedema ( as well as necrosis ) can make the assessment of response more difficult and so only response at 3 months and beyond post - radioembolisation was presented . 
ongoing research into techniques which accurately assess the burden of viable tumour post - radioembolisation is clearly needed to determine prognosis and provide any early indication for retreatment [ 37 ]  . this study was limited by the evaluation of patients from only a single centre and without an active comparator . 
we believe that techniques such as radioembolisation would compare favourably with targeted systemic treatments in terms of cost effectiveness . in conclusion , our results confirm the effectiveness and safety of 90y - re in patients with mcrc who were heavily pre - treated and refractory to standard - of - care systemic chemotherapy . 
90y - re can also be considered , even in this end - stage population , as a bridge therapy to subsequent treatments including surgical resection and ablation . acknowledgments an educational grant was provided by sirtex medical ltd to aid in the analysis of data and the editing of the manuscript . 
the final version of the manuscript has been approved by all authors . conflict of interest golfieri has been a speaker for bayer ag ( leverkusen , germany ) , boston scientific ( natick , ma , usa ) and sirtex medical ltd ( sydney , australia )  . 
the deposition of teeth secondary dentine and consequent decrease of pulp chamber in size are well known as aging phenomena , and they have been applied to the forensic context by the development of age estimation procedures , such as kvaalsolheim and cameriere methods . 
the present study takes into consideration canines pulp chamber volume related to the entire teeth volume , with the aim of proposing new regression formulae for age estimation using 91 cone beam computerized scans and a freeware open - source software , in order to permit affordable reproducibility of volumes calculation . keywords forensic radiology age estimation dental age teeth volume cbct canines d . 
cattaneo labanof , laboratorio di antropologia e odontologia forense , sezione di medina legale , dipartimento di scienze , biomediche per la salute , universit degli studi di milano , via l . 
 dannunzio , chieti - pescara , italy introduction methods of estimation of biological age are constantly evolving and find daily application not only in clinical fields such as the differential diagnosis of dysmetabolic disease or orthodontic therapies , but also in forensic radiology field in cases concerning the determination of the chronological age of a corpse or of a living subject . age estimation of unidentified bodies is a crucial step in the reconstruction of biological profile . 
age estimation on a living person is more frequently approached by forensic pathologists and anthropologists and often concerns migrants from foreign countries without identity papers or information from a civil registry [ 1 ]  . 
teeth and bone development are frequently used for age estimation of subadults and give more precise results if compared to methods commonly used for age estimation of adults . on the other hand , dental methods have several advantages because teeth are very resistant to chemical and physical factors . 
in 1950 , gustafson [ 3 ] published a method that takes into consideration , among other factors , pulp chamber contraction ; however , the method cannot be applicable to the living persons , since it requires a thin tooth slice . 
these methods are 1 3 732 radiol med ( 2015 ) 120 : 731736 based on the correlation between chronological age and ratio between linear measurements on a tooth radiograph [ 410 ]  . 
all these methods are therefore based on monoor bi - dimensional measurements performed on a radiograph of three - dimensional structures . the use of computerized tomography ( ct ) allows the operators to reach a more precise quantitative volume evaluation of all the dental tissues . 
as a consequence of the technological improvement , in the last years , the 2d and 3d image - based volumetric studies have acquired a growing importance , as also shown by the number of publications concerning the different applications of such technology [ 1618 ]  . literature shows that studies in the field of correlation between teeth volume ratios and chronological age are still at the beginning and are worth being analyzed in depth by further studies . 
teeth commonly used by authors are monoradicular ones , often canines ; radiographic images come from micro - ct , mdct and cbct ; volumes are calculated via commercial license software . 
from the literature review , it also appears how the proposed regression formulae are different among authors , perhaps because of the different geographic origin of the population or the different population age distribution . 
the present study starts from these considerations , with the aim of proposing new regression formulae using cbct images , as cone beam tomographs are nowadays quite common in dentistry . 
canines were taken into consideration since they usually survive than other teeth regardless of age , are less subjected to wear , and have the biggest pulp chamber among monoradicular teeth . 
in addition , a freeware , open - source software was used in order to permit affordable reproducibility for calculating volumes . materials and methods cbct from 91 subjects , 42 males and 49 females aged 1780 ( table 1 ) were used to determine pulp chamber volumes and entire dental volume of the upper right canines . 
only sound , completely developed teeth with closed apices were taken into consideration . the machine used was an i - cat next generation ( imaging sciences international , hatfield , pa ) with the following setting : voxel size 0.4 mm , scan time 8.9 s , ma 5 , mas 19 , kv 120 , scan width 23.2 cm , and scan height 17 c dicom files were then elaborated via the freeware and open - source software osirix [ 19 ]  . 
pulp chamber and entire dental volumes were calculated highlighting on axial slices the entire tooth and the pulp chamber perimeters by the tool roi ( region of interest )  . 
osirix can automatically generate rois on slices between two manually created rois , so , via the tool , pencil rois were generated every 34 slices , from the tooth apex to the most occlusal point of the crown . missing rois were then automatically generated by the software by the function generate missing rois and were verified analyzing each axial slice to correct them if necessary . 
teeth volumes ( dv ) , pulp chamber volumes ( pv ) , and their ratios ( pv / dv ) were then calculated . in order to verify the correlation between volumetric pv / pd ratios and age , a linear regression analysis was conducted , in which the pv / pd ratio and age were considered , respectively , as dependent variable and independent variable . 
the estimation of uncertainty degree of the regression was measured using the parameters r ( correlation coefficient or pearson product moment correlation coefficient ) e r2 ( coefficient of determination )  . 
regression formulae obtained are shown in table 2 with respective r and r2 parameters . pv / dv ratio turned out to be moderately correlated to chronological age with linear function for the female group and less correlated , but statistically significantly , for the male and the whole population . 
in the last few years , different authors have studied the correlation between chronological age and the ratio between the volume of the pulp chamber of a tooth and its entire volume adopting images from micro - ct , mdct e cbct processed by commercial software . 
 [ 20 ] were the first to use a micro - ct on 43 monoradicular teeth to assess the correlation between chronological age and the ratio between the pulp chamber volume and the entire tooth volume by specifically developed software . 
 [ 21 ] used 100 lower premolars to develop an age estimation method based on the ratio between the pulp chamber volume and the entire tooth volume determined via a micro - ct and 3d reconstruction via tri / 3dbon software . 
 [ 23 ] found a moderate correlation coefficient from a linear regression ( r 0.29 ) using the ratio between volumes of pulp chambers and of the entire tooth of 28 monoradicular teeth . 
 [ 25 ] adopted the software simplant pro in order to calculate volumes from 111 teeth cbct ; they found a higher correlation between volume ratios and chronological age in females than in males ( r2 0.37 females ; r2 0.30 males ) and a higher correlation using incisors ( r 0.27 ) if compared to canines . 
 [ 26 ] performed cbct of 188 canines and calculated pulp chamber and tooth volume via a software by ge systems , usa ; they elaborated a regression formula with a lower error ( r 0.63 ) than yangs one ( 2006 )  . 
cbcts were used because nowadays , and they are quite common among dental practitioner ; canines were chosen because they are already analyzed in previous studies and frequently found to be more sound than other teeth in situ ; lastly a freeware , open - source software was used in order to render more affordable reproduction of the proposed method and formulae . linear models published by star et al . 
 [ 25 ] and by tardivo [ 28 ] ( who studied the correlation between canines volumes and age ) have correlation indices ( r ) ranging between a minimum of 0.27 and a maximum of 0.68. 
the higher correlation among the female group is probably due to a steadier distribution even in higher values of pv / dv ( > 0.05 ) , while in the male group , a higher density was observed in intermediate values . age estimation adopting the proposed regression formulae has a prediction interval of 12 years with 60 % confidence interval ; however , with 95 % confidence , the 30 years . 
the error range is higher prediction interval is than those reported by methods of age estimation usually applied to subadults , but is comparable with data reported by methods commonly applied to the adults , both in cases of unknown decedents [ 2 ] and living people [ 2 , 8 , 13 , 14 ]  . 
 in addition , the large diffusion of ct scan technology will enable the operators to provide a more detailed analysis of pulp chamber size and therefore will improve the development of methods based on the deposition of secondary dentine , which will gain in the next future more and more importance , not only in the forensic context , but also in the clinical practice ; in fact one has also to consider that , for example , migrants without identity information need to be adequately assessed from a clinical point of view , although different biological parameters have to be evaluated by comparing their degree of development with the real age in order to provide an early diagnosis . 
from this point of view , reliable age estimation has a clinical impact , with consequent improvement of the patients health conditions . in conclusion , the exposed data suggest that the study of pulp chamber contraction for age estimation is promising and is worth being analyzed in depth by further studies focused on larger samples , characterized by a steady age distribution . 
it is our firm opinion that an erroneous reporting of hiatal hernia in ct exams performed with colonic distention may trigger a consecutive diagnostic process that is not only unnecessary , inducing a unmotivated anxiety in the patient , but also expensive and time - consuming for both the patient and the healthcare systethe purposes of our study were to determine whether colonic distention at ct with water enema and ct colonography can induce small sliding hiatal hernias and to detect whether hiatal hernias size modifications could be considered significant for both water and gas distention techniques . methods we retrospectively evaluated 400 consecutive patients , 200 undergoing ct - we and 200 undergoing ctc , including 59 subjects who also underwent a routine abdominal ct evaluation on a different time , used as internal control , while a separate group of 200 consecutive patients m . 
savarino department of surgery , oncology and gastroenterology , unit of gastroenterology , university of padova , via giustiniani 2 , padua , italy who underwent abdominal ct evaluation was used as external control . 
two abdominal radiologists assessed the ct exams for the presence of a sliding hiatal hernia , grading the size as small , moderate , or large ; the internal control groups were directly compared with the corresponding ct - we or ctc study looking for a change in hernia size . 
 we used the students t test applying a size - specific correction factor , in order to account for the effect of colonic distention : these corrected values were then individually compared with the external control group . results a sliding hiatal hernia was present in 51 % ( 102 / 200 ) of the ct - we patients and in 48.5 % ( 97 / 200 ) of the ctc patients . 
internal control ct of the 31 patients with a hernia at ct - we showed resolution of the hernia in 58.1 % ( 18 / 31 ) of patients , including 76.5 % ( 13 / 17 ) and 45.5 % ( 5 / 11 ) of small and moderate hernias . 
comparison ct of the 28 patients with a hiatal hernia at ctc showed the absence of the hernia in 57.1 % ( 16 / 28 ) patients , including 68.8 % ( 11 / 16 ) and 50 % ( 5 / 10 ) of small and moderate hernias . 
in fact , we observed in clinical practice a worrisome rate of hh reported as incidental extracolonic finding during ct with water enema ( ct - we ) and ct colonography ( ctc )  . 
as a fact , it has been already demonstrated that abdominal obesity by increasing intra - abdominal pressure promotes reflux and the development of hiatus hernia [ 3 ]  . hiatal hernia is a well - known factor impacting on most mechanisms underlying gastroesophageal reflux ( low sphincter pressure , transient lower esophageal sphincter relaxation , esophageal clearance , and acid pocket position ) , explaining its association with more severe disease and mucosal damage [ 46 ]  . 
therefore , although hh itself is a not life - threatening condition , its diagnosis may induce on patients , often not correctly instructed , worries and psychological distress that notably impact on quality of life . the search for the presence of hh should then be limited on subjects with typical manifestationssuch as epigastric pain , belching , heartburn , and regurgitation , especially when refractory to treatment or when alarm signs are present . 
therefore , it is our opinion that an erroneous reporting of hh may trigger a consecutive diagnostic process that is not only unnecessary , inducing a unmotivated anxiety in the patient , but also expensive and time - consuming for both the patient and the healthcare system [ 12 ]  . 
as a consequence , the purposes of our study were to determine whether colonic distention at ct - we and ctc can induce a small incidental physiological sliding hiatal hernias and to detect whether hiatal hernias size modifications could be considered significant for both water and gas distention techniques . materials and methods inclusion of patients this was a retrospective study , approved by our institutional review board . 
the primary study groups were derived from 400 consecutive patients , 200 undergoing ct - we and 200 undergoing ctc at our unit of radiology starting from january 1 , 2013 . 
among the patients with a hh at ct - we and ctc , pacs record review identified 59 subjects ( 31 in the ct - we group and 28 in the ctc group ) who also underwent a routine abdominal ct evaluation on a different time , and this group of patients served as internal control subjects ; a total of 44 abdominal ct examinations were performed before ct - we ( 21 ) or ctc ( 23 ) , and 15 ct examinations were performed after ct - we ( 10 ) or ctc ( 5 )  . 
all the studies were performed for a variety of diagnostic indications ( e.g. , suspect ibd , evaluation of colon cancer , evaluation of diverticulitis ) ; emergency cases and er patients , unable to undergo a proper intestinal preparation before the ct exams , were not included . ct - we and ctc techniques bowel cleansing consisted in a low - fiber diet for 3 days before the ct - we or ctc examination . 
the day before the examination , after a low - fiber meal at noon , each patient was instructed to drink continuously four doses of a granular powder ( isocolan ; bracco , milan , italy ; each dose contains 34.8 g polyethylene glycol 4 , 000 , 1.42 g anhydrous sodium sulfate , 0.42 g sodium bicarbonate , 0.36 g sodium chloride , and 0.18 g potassium chloride ) dissolved in 2 l of water . 1 3 radiol med ( 2015 ) 120 : 683689 ct - we technique was performed as previously described by paparo et al . 
all examinations were performed with a 64 - slice multidetector ct scanner ( light speed vct , ge medical systems , milwaukee , wi ) with the patient in supine position and end - inspiration apnea . 
 contrast - enhanced ct was performed using the following scanning parameters : 120 kv , 300400 mas ( with automatic ma modulation in the z axis ) , 0.6 s rotation time , detector collimation 40 mm , section thickness 5 mm , and table speed 35 mm per rotation . 
a lubricated enema tube was inserted into the rectu the tube was connected to a bag containing 2 , 000 ml of lukewarm tap water , which was gently infused through gravity in 34 min , with the patient placed supine on the ct table . 
 the flow rate was set at 3.23 ml / s with an automatic injector and acquisition was started in the portal phase , 45 s after the arterial peak in the upper abdominal aorta using a bolus - tracking software . 
immediately before ct acquisition , bowel hypotonia was obtained by iv injection of 2 ml hyoscine - n - butylbromide 20 mg / ml ( buscopan , boehringer ingelheim ) , in order to reduce abdominal discomfort of patients and to avoid motion artifacts during the acquisition . 
the estimated mean effective dose for ct - we protocol was 11 msv . ctc technique was performed for the purpose of colorectal evaluation [ 14 ] , as described in previous works [ 15 ]  . 
the preimaging protocol for colonography included bowel preparation ( as described for ct - we ) and , the day before examination , fecal tagging with 100 ml of oral iodinated contrast media . 
gas distention of the colon was obtained with room air gently pumped using a hand - held squeeze bulb in the rectum through a short cannula [ 15 ]  . 
supine and prone acquisitions were obtained with the same 64 - slice multidetector ct scanner with the following protocol : 120 kv , 80 ma , 0.6 s rotation time , detector collimation 40 mm , section thickness 5 mm , and table speed 35 mm per rotation . 
only the supine series were used in this study to evaluate for the presence of hh . for the internal and external abdominal ct control groups , standard diagnostic supine imaging used routine technique without colonic distention performed at endinspiration apnea . 
these ct exams were performed for various indications and comprehended both unenhanced and contrast - enhanced ct examinations , with acquisitions tailored on the basis of the clinical query . hiatal hernia evaluation retrospective assessment of the ct study groups for the presence or absence of a sliding hiatal hernia was performed by two board - certified abdominal radiologists , both with more than 5 years of experience in abdominal ct interpretation . 
the findings used to identify a hh at ct included : gastric rugal folds ; soft tissue fullness separate from the tubular esophagus ; lobulated or irregular enteral contour above the esophageal hiatus ; a combination of these signs . 
after the assessment of the single groups , the internal control groups of ct - we and ctc groups were directly compared with the corresponding ct - we or ctc study to evaluate for a change in hernia size . 
if more than one routine ct study was available for the internal control groups , the closest examination before / after ct - we or ctc was used . statistical analysis data were analyzed with spss software ( ibm , statistical package for social science )  . 
a sizespecific correction factor was empirically derived and was applied to the baseline hernia rate using the results from the internal control group , in order to account for the effect of colonic distention at ctc . 
specifically , the percentages of hernias that resolved or decreased in size in patients with an internal control examination were used to estimate the expected underlying baseline hernia rates at ct - we and ctc : these values were then individually compared with the external control group . results no statistical significant differences were found among the groups enrolled in terms of demographic and epidemiological characteristics ( table 1 )  . a sliding hiatal hernia was present in 51 % ( 102 / 200 ) of the patients belonging to the ct - we cohort and in 48.5 % ( 97 / 200 ) of the patients in the ctc group . 
 * * the correction factor is based on the estimated 68.8 and 50 % reduction in small and moderate - sized hiatal hernias , respectively , without colonic distention with ctc fig . 
1 small hiatal hernia ( arrow in a ) seen at ct with water enema ( ct - we ) in a 76 - year - old man , undergoing the investigation as follow - up of crohns disease . 
none of the three large hernias among the internal control patients at ct - we was absent at comparison abdominal ct , and the routine ct compared with ct - we showed a reduction in hernia dimension in seven additional patients . 
after applying the correction factors for the ct - we and the ctc groups , the estimated residual prevalences ( 16 and 18.5 % , respectively ) were much closer to that of the external control patients ( p 0.160 for ct - we and p 0.455 for ctc ) , as shown in table 2 . 
there was no statistical significant difference in terms of dimension of the hh between gas - induced and water - induced distention . discussion the main source of inspiration for this work was the study by pickhardt et al . 
2 scout ( a ) and supine axial ( b ) images of a 66 - year - old woman , undergoing screening ct colonography ( ctc ) evaluation , show the presence of a small hiatal hernia ; note the mass effect on stomach determined by the gaseous distention of the splenic flexure ( arrow in a )  . 
 since the amount of unnecessary workup for the wide variety of benign extracolonic findings is particularly relevant for ctc [ 16 , 17 ] , radiologists have to correctly assess extracolonic findings of ct - we studies as well . 
it is therefore important to underline , if possible , when additional evaluation may not be required . with this precondition , incidental findings should be considered according to the clinical background , and the presence of hh is a classic circumstance in which lack of specific symptoms of gastroesophageal reflux disease may suggest scanty clinical relevance [ 18 ]  . 
these latter usually consist in barium swallow radiology or esophagogastroduodenoscopy , which do not affect the management of the patient and do not provide information about the esophageal function and gastroesophageal barrier competency in controlling gastroesophageal refluxes . 
specifically for the upper digestive tract , a very recent review reported as a significant proportion of patientsup to 61 %reporting heartburn without any proved pathologies improve under antidepressant therapy . 
several meta - analysis showed a negative impact on work productivity , defined as absence from work ( absenteeism ) as well as reduced effectiveness while working ( presenteeism ) [ 2022 ]  . 
although these processes are commonly experienced during our clinical routine , this study did not asses the effect of the diagnosis of hh on patients quality of life , as it was not part of the aims . 
the finding was confirmed at the routine ct performed 16 months before ( b ) used as internal control that shows no modifications of the hernia radiol med ( 2015 ) 120 : 683689 considered a mere speculation . 
although more sophisticated , traditional manometry presents also some limitations due to the low number of pressure sensors and the inter - individual variability , thus potentially jeopardize the reliability of a landmark such as the pressure inversion point . 
high - resolution manometry ( hrm ) seems to overcome these shortcomings , allowing real - time detection of lesser degrees of axial separation between the lower esophageal sphincter and crural diaphragm , distinguishing swallow and distention related artifacts [ 2 , 24 , 25 ]  . 
 in addition , the employment of physiopathologic methodologies allows the recognition of esophageal dysmotilities , which is of capital importance in the eventuality of fundoplicatio to avoid a complete therapeutic failure and postoperative complications [ 11 ]  . our results confirm the relationship between ctc technique and small sliding hernias showed by pickhardt et al . 
 [ 1 ] , as well as the substantial matching between the external control group and the residual prevalence of hiatal hernias after excluding the estimated subset of small sliding hh most likely due to gaseous colonic distention . 
in particular , we believe that small 1 3 radiol med ( 2015 ) 120 : 683689 sliding hiatal hernias should not be reported in patients with symptoms not related to reflux disease undergoing ct - we or ctc , or they should be most likely referred to a technique - related finding . 
thali lorenzo bonomo received : 2 october 2014 / accepted : 29 january 2015 / published online : 19 february 2015 italian society of medical radiology 2015 abstract objectives when hemopericardium ( hp ) is found at autopsy , it represents a challenge for the forensic pathologist when having to assess its role in causing death . 
in fact , a proper diagnosis of pericardial tamponade ( pt ) must be based on clinical and instrumental data , which are not often available at post - mortem investigation . 
the aim of this study was to individuate post - mortem ( pmct ) findings indicative for the diagnosis of pt . materials and methods we revised pmct images and autopsy reports of 14 cases with fatal hp and intact pericardiufrom autopsy reports , we obtained volume and cause of hp . 
a control group of 11 cases submitted to pmct prior to autopsy was selected with the following criteria : absence of relevant pericardial effusion , venous system congestion and bleeding . results of the 14 pt subjects , 13 had a double - concentric stratification of hp and compression of the coronary sinus and / or of the pulmonary trunk , all showing a flattening of the anterior surface of the heart ; other findings indicative of venous system congestion were variably observed . 
thali department of forensic medicine and imaging , institute of forensic medicine , university of zurich , winterthurerstrasse 190 / 52 , 8057 zurich , switzerland the exception of a distended or non - completely collapsed superior vena cava ( 11 / 11 cases )  . conclusions pmct is able to provide some findings indicative of pt . 
this study suggests the possibility to use pmct findings to retrospectively demonstrate a clinical condition , such as pt . keywords post - mortem ct hemopericardium pericardial tamponade cardiac tamponade forensic radiology forensic pathology introduction hemopericardium ( hp ) , the pathological condition of blood in the pericardial sack , is frequently observed at autopsy . 
thus , when hp is detected at autopsy , it represents a challenge for the forensic pathologist who has to determine the cause of death [ 1 , 2 ]  . 
in fact , hp results in the life - threatening condition of pericardial tamponade ( pt ) only when the accumulation of blood causes intrapericardial pressure to exceed the cardiac chamber diastolic pressure , thus preventing and impairing cardiac filling . 
symptoms of pt include , but are not limited to , dyspnoea , tachypnea and fatigue , while common signs include tachycardia , jugular venous distension , a quiet precordium , hypotension and pulsus paradoxus ( inspiratory drop in systolic blood pressure of 10 % 1 3 724 radiol med ( 2015 ) 120 : 723730 or 10 mmhg )  . 
echocardiography is the primary clinical diagnostic method for the initial detection of pericardial effusion and can be rapidly carried out at the bedside [ 3 , 4 ] ; the diagnosis of pt is based on one or more bimodes and doppler echocardiography diagnostic criteria [ 3 , 4 ]  . computed tomography ( ct ) , cardiac magnetic resonance imaging ( mri ) [ 3 , 5 ] and fluoroscopic imaging are not recommended for diagnosing pt , mainly because they are time - consuming . 
nevertheless , in some cases a ct scanning performed for other purposes may detect the presence of a pericardial effusion . the clinical literature reports some in vivo ct findings in cases of imminent pt [ 515 ]  . 
they include pericardial effusion , flattened heart sign ( fhs ) , bowing of the interventricular septum , compression of the coronary sinus and of the pulmonary trunk , dilatation of the superior vena cava ( svc ) ( with a diameter similar to or greater than that of the adjacent thoracic aorta ) and of the inferior vena cava ( ivc ) ( with a diameter greater than twice that of the adjacent abdominal aorta ) , distension of the hepatic and renal veins , periportal oedema and reflux of contrast into the azygos vein and ivc . 
all these ct findings are related to the effects of the increased intrapericardial pressure on the intrapericardial vessels and the cardiac chambers ( compression ) , and on the venous vascular system ( distension ) and to the obstacle to the progression of the blood and consequently the contrast media towards the cardiac chambers . 
although these in vivo ct signs , when seen individually , cannot be considered specific for pt , their simultaneous evidence , particularly in the presence of a large pericardial effusion , strongly suggests a diagnosis of an imminent pt [ 15 ]  . in the field of forensics , while the autopsy detection of hp is quite frequent , clinical and instrumental data in the ante - mortem period are only rarely available to differentiate between fatal and non - fatal hp . 
two hundred millilitres of clotted blood has been proposed [ 2 ] , but amounts up to 300400 ml are generally measured at autopsies , with some authors reporting even greater volumes [ 16 , 17 ]  . 
moreover , in trauma cases , the presence of a pericardial defect should be considered because , even after fatal hp , a perimortally acquired tear may facilitate a postmortem drainage of blood from the pericardium , particularly if intensive resuscitation manoeuvres have been performed . thus , when hp is found at autopsy , it does not necessarily constitute the primary cause of death . few studies in the forensic literature were focused on the use of pmct imaging in cases of hp [ 1824 ] and even fewer on the possibility to use post - mortem imaging for the assessment of the diagnosis of pt due to hp [ 18 , 23 , 24 ]  . this work focused on autopsy cases with a clear , based on ante - mortem clinical and / or instrumental records , diagnosis of pt , submitted to pmct whole - body scanning prior to autopsy . 
the aim was to individuate which pmct finding can be considered as indicative for the diagnosis of pt ( that is , for fatal hp ) and , thus , to create a reference for other forensic cases where ante - mortem data are not available and other pathological conditions may have caused or concurred to cause the death . materials and methods the study was approved by both our institutional review board and the public prosecution department . 
image reconstruction was carried out using a soft and hard tissue convolution kernel with a slice thickness of 1 mm and an increment of 0.6 mm , in an abdominal and lung window . 
all the bodies were scanned within 48 h since the estimated time of death . all image data sets were interpreted using a sectra workstation ids7 ( version 14.3.5.136 , sectra , linkoping , sweden ) , to describe the pmct appearance of the hp , with particular attention being paid to hyperdense armoured heart ( hah ) , the pmct sign described by shiotani et al . 
 in particular , the presence of the following ct findings was assessed : fhs , distension of hepatic and / or renal veins , compression of the coronary sinus and / or of the pulmonary trunk , periportal oedema . 
other signs , such as the angulation or bowing of the interventricular septum , and other findings related to reflux of contrast material were excluded because contrast injection was not performed and a reflux of contrast is not documentable on pmct angiography . a control group of 11 non - pt cases submitted to pmct prior to autopsy was retrospectively selected with the following macroscopic criteria : an intact pericardium , absence of relevant pericardial effusion on autopsy reports , venous system congestion and bleeding . a preferential research was conducted between deaths caused by intoxication , and suffocation related to smothering , choking , or reduction of the oxygen concentration in the respired atmosphere , as it occurs with co intoxication , or when a plastic bag is placed over the head down to neck level . 
 finally , some periportal oedema was observed in 3 / 14 cases . control group the results of the retrospective pmct imaging analysis are summarized in the table 2 . 1 3 726 radiol med ( 2015 ) 120 : 723730 fig . 
1 the ct axial images ( a , b , c ) at the cardiac level , referred to three cases of the study group show a double density stratification of the hemopericardiuthe images a and b show the inner ring homogeneous in thickness , but thinner in ( b ) than in ( a )  . 
the images a and b show the flattening of the anterior surface of the right chambers ( fhs ) , more pronounced in ( b ) with respect to ( a )  . 
 in c and d , the coronary sinus ( c ) and the pulmonary trunk ( d ) appear not compressed 1 3 727 radiol med ( 2015 ) 120 : 723730 fig . 
5 the ct axial images at the infrahepatic level are referred to a case of the study group ( a ) and to a case of the control group ( b )  . 
in this case , pmct imaging showed a serial rib fractures , a transverse fracture of the sternum , hp and dilated svc and ivc , as well as bilaterally distended renal veins . 
the authors explained this particular imaging appearance of hp , named hah , as due to the stratification of blood cells on the epicardial surface ( high - density ring ) and of serum along the pericardium ( low - density outer ring )  . huang and shiotani [ 18 , 20 ] did not carry out autopsy , but the assumed causes of death were based on comprehensive health records and information on the medical history . recently , filograna et al . 
 [ 23 , 24 ] in a research study about pmct imaging in cases with hp and in a case report about an hp due to ruptured aortic dissection suggested the possibility to use pmct imaging results to retrospectively assess the diagnosis of pt . 
in these two papers , the authors advice the opportunity to consider both the pmct appearance of hp , as described by shiotani [ 20 ] , but also the in vivo ct findings reported in the radiological clinical literature as suggestive of pt , to support the post - mortem diagnosis of fatal hp . in line with this suggestion , this work investigates on the possibility to define a forensic reference for the post - mortem diagnosis of pt due to hp based on pmct . although the clinical literature does not describe hah sign [ 20 ] , it was observed in pmct images of 13 / 14 cases of the study group . according to the previous studies [ 20 , 23 , 24 ] , we attribute the presence of this double - concentric stratification to fibrination induced on the blood cells in contact with the epicardial surface by the beating movements of the heart originating the densest inner ring , and to defibrinated plasma , constituting the low - density outer ring . 
thus , finding an hah in cases with hp might mean that the heart was beating at the moment of the intrapericardial bleeding and that it maintained his mechanical function for a while after the bleeding occurred . 
an inferior sensitivity of pmct in the detection of hah , with respect to pmmr , could be also the explanation of the absent detection of hah in the case no . 
 [ 23 ] , next to the pmct appearances of hp , other clinical ct findings have to be considered in the assessment of the diagnosis of pt on post - mortem imaging . 
in this regard , the present study demonstrates firstly that most of the in vivo ct findings proposed in clinical literature as highly suggestive of an imminent pt might be detected also on images acquired in the post - mortem period . 
although periportal oedema was observed only in three cases of the study group , it was never identified in the control group . 1 3 radiol med ( 2015 ) 120 : 723730 finally , while svc was never collapsed in both groups , the ivc in the infrahepatic tract appeared to be collapsed only in 5 / 14 cases of fatal hp , against the 10 / 11 cases of the control group . 
this means that also the distension of ivc can be considered a frequent finding in pt deaths . nevertheless , if the particular setting of the present analysis is conceived , some considerations have to be taken . 
a progressive reduction of the diameters of the circulatory system , especially the aorta , on pmct scans was pointed out by ishikawa [ 25 ] , and a distension of cardiac chambers was described by shiotani [ 30 ]  . 
on the other hand , personal experience shows that the distension of the abdominal venous system is a common finding in cases of death due to cardiac diseases . a spontaneous question is whether these same pmct findings could be detected also in cases with non - fatal hp . 
nevertheless , we agree with restrepo [ 15 ] , when he states that , although the reported clinical findings , when isolated cannot be considered specific for the diagnosis of an imminent pt , their simultaneous detection can strongly suggest this diagnosis , particularly in the presence of a large pericardial effusion . 
 [ 24 ] suggests that although hah sign and fhs could be individually detected in both fatal and non - fatal cases of hp , the association of both signs can be observed only in deaths due to pt . regarding the limitations of the study , the limited number of cases should be considered the major one . 
a large study population might better sustain our hypotheses . in conclusion , this work demonstrates the potentials of post - mortem imaging in the assessment of the diagnosis of pt . 
particularly , the study shows that in cases with hp and an intact pericardium , the diagnosis of death due to pt could be supported by the co - presence of hah , fhs , compression of the coronary sinus and / or pulmonary trunk , distension of hepatic and renal veins . 
nevertheless , our results suggest also that pmct might be considered superior or even substitutive to autopsy , the actual gold standard , in those cases with hp and an intact pericardium where perimortem clinical or instrumental data are not available . 
 other important benefit of using pmct with respect to autopsy is the fact that it is a minimally invasive , reproducible and operator - safe technique , which could be used also as a screening method ; this is even truer considering the decline of autopsy rates over the last years . 
we are aware that it is not often possible to perform a pmct examination on all deaths , especially in those institutions where a dedicated ct scanner is not available for forensic purposes . 
gentile massimo galia federico midiri alessia pepe massimo midiri giovanni donato aquaro received : 10 june 2014 / accepted : 18 november 2014 / published online : 10 february 2015 italian society of medical radiology 2015 abstract purpose this study was conducted to assess the role of atrial function by cardiac magnetic resonance ( cmr ) for the evaluation of diastolic physiology in patients with hypertrophic cardiomyopathy ( hcm ) compared to healthy controls . materials and methods we enrolled 23 consecutive patients affected by hcm and 43 healthy subjects as agematched control cases ( cc )  . 
midiri university hospital p giaccone university of palermo , via del vespro 127 , 90127 palermo , italy introduction hypertrophic cardiomyopathy ( hcm ) is a complex but relatively common form of genetic heart muscle disease that occurs in 1 out of 500 people [ 1 ]  . 
hcm is the most common cause of heart - related sudden death in people under 30 years of age , and can also be responsible for exercise disability at almost any age . 
the generally accepted definition of hcm is a disease characterised by unexplained left ventricular ( lv ) hypertrophy associated with nondilated ventricular chambers in the absence of other cardiac or systemic disease that itself would be capable of producing the magnitude of hypertrophy evident in a given patient [ 2 ]  . 
 diastolic dysfunction is a common feature in hcm due to marked lv hypertrophy , interstitial fibrosis and myocardial ischemia [ 3 ]  . 1 3 radiol med ( 2015 ) 120 : 714722 the noninvasive assessment of diastolic function is still an open issue . 
more recently , tissue doppler imaging ( tdi ) , which is relatively independent of loading conditions and image quality , has been found to be useful in the assessment of lv diastolic function [ 4 , 5 ]  . 
in addition , the ratio between early diastolic mitral inflow ( e ) and early diastolic mitral annular tissue velocity ( e ) was found to correlate well with lv filling pressure , and are now widely used to diagnose diastolic dysfunction [ 6 , 7 ]  . 
 moreover , combined information of mitral inflow and tdi is able to differentiate between normal and pseudonormal diastolic dysfunction . cardiac magnetic resonance ( cmr ) can be used to evaluate diastolic function and provides advantages over echocardiography in selected patients . 
in addition to anatomical imaging , measurement of blood flow velocity can be performed at any location , and this can produce inflow velocity data for the mitral valve and pulmonary veins [ 8 ]  . the haemodynamic implications of atrial diastolic function in the normal and pathological heart have shifted the interest towards the study of diagnostic morphological and functional information about the atriu the aim of the current study was to assess the role of atrial function by cmr for the evaluation of diastolic function in patients with hcm compared to healthy controls . materials and methods we enrolled 23 consecutive patients ( 16 men and 7 women , mean age 42 14 ) affected by hcm with no more than stage i diastolic dysfunction ( e / a < 1 ) assessed by echocardiography . 
the diagnosis of hcm was established according to the recommended criteria [ 9 ]  . we also enrolled 43 healthy subjects ( 19 men and 24 women , mean age 41 17 ) as age - matched control cases ( cc )  . 
all the healthy subjects were voluntarily enrolled with the following inclusion criteria : ( 1 ) absence of symptoms , ( 2 ) normotensive status , ( 3 ) absence of cardiovascular risk factors ( calculated risk < 10 % ) , ( 4 ) no clinical history of cardiac or extracardiac disease , ( 5 ) normal physical examination , ( 6 ) normal electrocardiogra exclusion criteria for both hcm and healthy controls were : ( 1 ) claustrophobia , ( 2 ) contraindication to mri ( 3 ) presence of arrhythmias , ( 4 ) severe heart valve disease , ( 5 ) congenital anomalies of pulmonary venous return . all subjects gave written informed consent to the protocol . 
the ethics committee approved the study . mri protocol cmr was performed using a 1.5 - t scanner ( ge excite hdxt , milwaukee , wi ) with an eight - element ( four anterior and posterior ) phased - array receiver surface coil and retrospective electrocardiographic ( ecg ) triggering for capture of the entire cardiac cycle . in all subjects the study of atrial and ventricular function was obtained by acquiring cine ssfp ( steady - state free precession ) , end - expiratory breath - hold images on sections perpendicular to the major axis of the left ventricle from left ventricular apex to cover the entire left atriupatients with hcm completed the study after the intravenous administration ( 0.1 mmol / kg ) of paramagnetic contrast agent ( gadobutrol , gadovist , bayerschering , berlin , germany ) , to evaluate delayed enhancement ( de )  . 
during this latter phase , a variable amount of blood ( very small in healthy subjects ) regurgitates into the pulmonary veins because of the absence of valves . diastolic abnormalities of the left ventricle may involve both the conduit and booster phase of left atrial function . 
initially the first impairment of diastolic function consists in abnormal relaxation that may alter the conduit phase of the left atrium by an increase of ventricular stiffness and a decrease of passive suction . 
during this stage , the left atrium compensates for the decrease of atrial passive emptying by enhancing the booster function ( producing an inversion of the e / a ratio of mitral inflow at doppler evaluation )  . 
1 screenshot of the software used for atrial ( a ) and ventricular ( v ) function ( tracking tool ) function , the atrial contraction becomes less able to compensate for the increased ventricular stiffness to maintain adequate emptying , and the left atrium enlarges . 
automatically starting from the selected centre the signal of each voxel positioned along 72 equiangular rays ( separated by an angle of 5 ) of progressively increasing length was measured . 
the endocardial contour of the atrial and ventricular myocardium was defined when the signal intensity , measured in voxels along the rays , was less than 5 standard deviations the average signal in the region of interest . 
peaks of the ventricular dv / dt curve are already known : the first positive peak is defined the peak of early filling ( e ) , the second peak is the peak of late or atrial filling ( a ) which represents the maximum speed of passive filling and the maximum speed of filling secondary to atrial contraction , respectively . 
we also calculated parameter ivrt ( isovolumic relaxation time ) normalised to the heart rate and an index of left ventricular contractility ( estimation of elastance ) independent of preload obtained using ( max dv / dt ) / edv [ 11 ]  . 
briefly , the first negative peak , representing maximal emptying during the conduit phase was calculated and identified as the early atrial peak emptying rate ( atrial pere )  . 
the systolic atrial filling velocity ( safvmax ) was also measured as the first positive peak of the atrial dv / dt curve , representing the maximal filling rate during the reservoir phase of atrial function . the extent of de was measured in the postcontrast t1 - weighted ir - gre pulse sequence using a previously validated method [ 12 , 13 ] and expressed as percentage of lv mass . statistical analysis statistical analysis was performed by medcalc software ( version 12.2.1medcalc software , broekstraat 52 , 9030 mariakerke , belgium )  . 
3 performance volume / time curves of the left ventricle ( a ) and left atrium ( b ) from which we derived ventricular ( c ) and atrial ( d ) dv / dt curves . 
in the latter the s peak is distinguishable , determined by ventricular emptying and consensual atrial filling ; peak e of early ventricular filling or premature atrial emptying ; peak a due to late ventricular filling following atrial contraction results table 1 characteristics of the study population the characteristics of the study population are shown in table 1 . during the examination all patients and controls had a normal sinus rhythm with an average heart rate of 10 bpm in the control group . 11 bpm in the hcm group and 64 we evaluated the association between nyha class i and > i and the parameters of diastolic dysfunction . 
 [ 18 ] used ssfp sequences acquiring short - axis cine images on which are plotted atrial endocardial contours for all phases , so as to obtain a calculation of the volume through postprocessing software . 
they calculated the maximum atrial volume , providing dimensional indexes of normality based on geometric measurements borrowed from 2d echocardiography [ 18 ]  . in a previous study , hudsmith et al . 
 [ 14 ] applied the method to the arealength ssfp images acquired in the horizontal and vertical long axis to calculate the atrial volume of 108 healthy volunteers , obtaining values of minimum and maximum atrial volume similar to those obtained in our study . 
descriptions of the peaks of the atrial volume curve and the curve of atrial dv / dt have not been previously reported . the american society of echocardiography puts the recommendations in the study of diastolic function , la volume measurements in conjunction with a patients clinical status , other chamber volumes , and doppler parameters of lv relaxation [ 19 ]  . in our population of hcm patients the maximal atrial volumes were significantly greater than in the healthy controls . 
the added value of the assessment of atrial function may be that it permits evaluation of initial impairment also in the absence of atrial dilatation . some studies have proposed to evaluate the longitudinal contraction of the atrium using tissue doppler imaging [ 20 ] .the poor reproducibility , the angle - dependence , signal artefacts and the inability to obtain information on the curved portions of the atrial wall are inherent limitations to the calculation of strain by tissue doppler imaging . a recent study of vu et al . 
atrial function and mitral inflow were quantified by a computer analysis and atrial function was defined as atrial contraction ( a - wave ) volume divided by total inflow volume . 
the authors found a wide variability in left atrial function and a significant association between left atrial function and left ventricular ejection fraction [ 21 ]  . we did not perform phase - contrast images on the mitral valve because these are associated with many limitations such as shortening of the lv axis that produces a great shift of planes eventually passing from the atrium to the lv . 
therefore , we proposed to evaluate diastolic function by comparing the atrial and ventricular dv / dt curve , which is acquired easily in all cardiac mri studies . the indexes of atrial function calculated in our work were adapted from the indexes of diastolic function already validated in mri for the left ventricle . 
 [ 22 ] , the correlation index of atrial function in patients with hcm and normal subjects showed significant differences , probably because we selected hcm patients with only early diastolic impairment at echocardiography ( stage i dysfunction )  . 
however , we had a trend for a difference ( p 0.09 ) , and increasing the hcm population could perhaps make this difference significant . the new european guidelines for the management of hcm patients recommend to perform mri on all hcm patients and to repeat mri every 2 years in the presence of fibrosis . 
however , further studies evaluating large populations of hcm patients should be performed to demonstrate the real advantage of assessing atrial function in this cardiomyopathy [ 23 , 24 ]  . some differences were found between ours and previous studies of cardiac catheterisation and echocardiography . 
 the differences are probably due to some limitations of our study : a correlation with the atrial / ventricular pressure curves derived from invasive analysis was not attempted , but none of the patients with hcm had a clinical indication for cardiac catheterisation considering the risks associated with the procedure ; only a minority of healthy subjects underwent echocardiography . 
for this reason , it was not possible to perform a correlation between the two methods . cmr has lower temporal resolution than echocardiography and this may appear as a major limitation of this technique . 
the variable ventricular e / a does not show any statistically significant difference between hcm patients and controls ( a ) , unlike the variable atrial e / a which , with a value of p < 0.0001 , is significantly different between the two populations ( b )  . 
the same applies to the variable pfre ventricular ( early peak filing rate ) indexed for the end - diastolic volume ( edv ) and pere atrial ( early peak emptying rate ) indexed for maximum atrial volume ( c , d ) with higher accuracy than echocardiography . 
the measurement of the dv / dt curve of the left atrium enables direct assessment of the three components of atrial function : reservoir , conductance ( atrial pere ) and booster ( atrial pera ) functions . 
in a physiological range of heart beats , using 30 cardiac phases as in this study , mri has a temporal resolution of phases ranging from 40 to 20 ms allowing for a negligible error . 
in 1 / 23 ( 4.3 % ) hcc , the presence of peripheral residual tumor was suspected by both 2d and 3d ceus , but it was not confirmed by sor . 
an accurate assessment of therapeutic response is of crucial importance , considering that a complete tumor ablation significantly increases patient survival , whereas residual unablated tumor calls for additional treatment [ 3 , 4 ]  . 
imaging modalities play a pivotal role in this task , although they have been reported to be fairly insensitive in demonstrating residual disease after lrt when compared to histology [ 5 ]  . 
computed tomography ( ct ) , magnetic resonance imaging ( mri ) , and contrast - enhanced ultrasound ( ceus ) suggest a successful procedure when a previously enhancing , hypervascularized hcc nodule shows lack of contrast enhancement after treatment , whereas still viable tumoral tissue is typically depicted as an arterial - enhancing focus with portal venous washout [ 6 ]  . more recently , three - dimensional contrast - enhanced us technique ( 3d ceus ) has been reported to improve the study of tumor vascularity , thus allowing the response evaluation of radiofrequency ablation in the three orthogonal planes [ 7 ]  . 
nevertheless , it has been suggested that the spatial resolution of the current 3d probes may be limited , 1 3 696 radiol med ( 2015 ) 120 : 695704 3d ceus and volumetric acquisition of the data may be associated with distortion of the volume as a result of motion when using mechanical probes [ 8 ]  . hence , we undertook this study in an attempt to investigate diagnostic performance of 3d ceus compared with 2d ceus in the assessment of therapeutic response of hcc treated with lrt . 
the influence of 3d ceus on clinical outcome was also evaluated . in the same session , with an interval time of at least 15 min to allow for contrast clearance of the previous contrast injection , the same radiologist who performed baseline ultrasound and 2d ceus , also performed 3d ceus scanning by means of the same iu22 unit provided with a volumetric mechanical v6 - 2 mhz probe and pulse inversion imaging software . 
we decided to use a full bolus of 4.8 ml of sulfur hexafluoride in order to compensate for some technical advantages of c5 - 1 mhz probe over v6 - 2 mhz probe , such as operating frequency and purewave technology crystals , which provide a better nominal penetration power for the c5 - 1 mhz probe . 
in suspended respiration , 3d sweep was started and three volumetric datasets were acquired in the arterial , hepatic venous , and extended hepatic venous or late phase ( i.e. , 2540 , 6090 , and 200300 s from the beginning of injection , respectively )  . 
each examination lasted about 5 min after bolus injection . all images and cineloops were digitally stored both as raw data in a pc - based workstation connected to the us units via a standard ethernet link and sent to our pacs ( impax , agfa - gevaert , milan , italy )  . image analysis two abdominal radiologists ( more than 10 years of experience ) randomly reviewed off - line by consensus 2d and 3d ceus examinations . 
the readers were not involved in the scanning and were blinded to the final diagnosis , as well as to the identification , clinical histories , and other imaging findings of the patients . 
two consecutive interpretation sessions with a 7 - day interval to avoid recall bias were held to complete the review process . 3d volumes were reviewed using a commercially available proprietary software ( qlab , philips ultrasound , bothell , wa , usa ) approved for clinical use and capable of volume rendering mode and islice mode . 
this latter mode provides the capability of displaying the dataset in multiple , contiguous , parallel 2d slices , similar to ct and mr , in three orthogonal planes , i.e. , plane a , which can be translated from front to back , plane b , which can be translated from right to left , and plane c , which can be materials and methods patient population and imaging techniques institutional review board approval was obtained and full written informed consent was obtained for this prospective study . 
the us contrast agent used in the present study was sulfur hexafluoride ( sonovue , bracco , milan , italy ) , which was injected intravenously as a 2.4 ml bolus followed by 10 ml of normal sterile saline flush using a 20or 22 - gauge peripheral intravenous cannula . 
residual viable tumor was also categorized as ( 1 ) ingrowth pattern , when a hypervascular focus was detected within the edge of a treated nodule and ( 2 ) outgrowth pattern , when a hypervascular focus was detected around a necrotic treated nodule and in continuity with its border [ 11 ]  . 
the presence of a uniform and thin ( 45 to 78 - mm thick ) peripheral rim of contrast enhancement surrounding the treated zone was regarded as benign reactive hyperemia [ 6 ]  . 
the time needed for a complete evaluation of each single 3d volumetric dataset , including defining and zooming the area of interest , choosing the appropriate depth , number , and spacing of slices was also measured . the influence of both methods on clinical outcome was evaluated on a three - point scale : ( 1 ) 2d ceus imaging changed diagnosis and consequently lesions management ( score 1 ) ; 3d ceus and 2d ceus studies provided the same diagnosis ( score 2 ) ; 3d ceus imaging changed diagnosis and consequently lesions management ( score 3 )  . reference standard the final diagnosis was obtained by magnetic resonance imaging ( mri ) with hepatocellular specific gadoliniumbased contrast agent ( n 17 ) and multidetector row computed tomography ( mdct ) ( n 6 )  . 
diagnostic criteria for complete treatment at mri / mdct were the absence of any enhancing portion within or at the margin of the ablation zone during the hepatic arterial phase , as previously reported [ 12 ]  . 
diagnostic criteria for residual viable tumoral tissue at mri / mdct were any nodular arterially enhancing area within or along the margin of the treated hcc [ 10 ]  . follow - up by means of both ct and / or mri , laboratory data , and clinical assessment were also used to confirm the diagnosis obtained one month after treatment . ct studies were performed by means of a 64 - slice mdct ( brilliance 64 ; philips medical systems , eindhoven , the netherlands )  . 
to determine the scanning delay for the hepatic arterial phase , the time - to - peak aortic enhancement was assessed using an automatic bolus - tracking technique with automated scan - triggering software ( bolus pro ultra , philips medical systems , eindhoven , the netherlands )  . 
a triphasic dynamic contrast - enhanced study was obtained after the administration of a iv bolus of 0.1 mmol / kg of gadobenate dimeglumine ( multihance , bracco , italy ) injected into an antecubital vein at a flow rate of 2 ml / s through a 20 - gauge intravenous catheter by means of a power injector ( mr spectris ; medrad , pittsburgh , pa , usa ) and flushed by 20 ml of sterile saline solution . 
images were acquired using automated bolus detection technique ( smartprep technique , ge healthcare ) during the arterial ( 16 s after bolus detection ) , hepatic venous , and delayed phase ( 60 and 180 s after bolus injection , respectively )  . 
the statistical significance of the difference between 2d ceus and 3d ceus in the assessment of therapeutic response of hcc - treated lrt was tested by two - tailed mcnemars test with the continuity correction . the statistical significance of the difference between complete and incomplete responses for lesions size and depth was tested through the kruskalwallis equality - ofpopulations rank test . 
a oblique ascending right subcostal baseline us image in a 57 - year - old man shows a 2.7 - cmsized inhomogeneous hypohyperechoic area in the vii hepatic segment ( arrow ) without detectable flow at color doppler evaluation ( box ) , b at 2d ceus in the arterial phase ( 34 s after sonovue injection ) , the lesion shows lack of contrast enhancement ( left , arrow ) ; c 3d i - slice reconstruction ( slice thickness 2 mm ) confirms the same finding throughout the lesion , slice by slice ( arrows ) the use of 3d us after the administration of microbubblebased contrast agent ( 3d ceus ) aids in the characterization of focal liver tumors by evaluating their vascular patterns [ 14 , 15 ]  . 
by presenting several slices continuously , changing thickness and distances between two slices 3d ceus can make it easier to detect enhancement in different portions of tumors [ 15 ]  . 
this latter feature of 3d ceus has been suggested to be beneficial in monitoring the response of hcc treated by means of radiofrequency ablation [ 8 , 13 ]  . 
luo and co - workers have compared 3d ceus with contrast - enhanced ct in the evaluation of the effect of radiofrequency ablation of hccs , finding good concordance of 3d ceus with ct and reporting sensitivity , specificity , and accuracy values for detecting 1 3 700 radiol med ( 2015 ) 120 : 695704 fig . 
a axial baseline image of the left lobe in a 52 - year - old woman shows a 6.7 cm highly inhomogeneous mass ( calipers ) ; b 2d ceus in the arterial phase ( 17 s after sonovue injection ) shows a clear - cut hypervascularity within the treated area ( arrows ) ; c 3d i - slice reconstruction ( slice thickness 7.4 mm ) depicts the same finding slice by slice ( arrows ) adequate ablation of 97 , 100 , and 97 % , respectively [ 16 ]  . 
in our series , we did not encounter a clinically relevant limitation of spatial resolution of the mechanical 3d probe regarding the nonlinear imaging modes used in contrast - enhanced 3d studies as described by leen and co - workes [ 8 ]  . 
besides the intervening technological improvement , an explanation for this finding may be also found : ( 1 ) in the amount of contrast agent administered in our study : a full bolus of 4.8 ml of sulfur hexafluoride instead of the usually administered 2.4 ml dose , which allowed a better sensitivity of the technique to small vessels ; ( 2 ) in the capability of displaying the region of interest as individual slices with a gap as thin as 0.1 mm , thus allowing the radiologist to better assess the presence of tiny foci of neovascularisation . these latter observations may also explain the similar diagnostic performance of 3d ceus to that of 2d ceus observed in our series with excellent intermodality 1 3 702 radiol med ( 2015 ) 120 : 695704 fig . 
a oblique ascending right subcostal baseline us image in a 45 - year - old woman with hcc treated by rfta shows a barely visible area in the viii hepatic segment ( right , arrowhead )  . 
at 2d ceus in the arterial phase , the lesion shows a deeply located hypervascular focus at the periphery of the treated area suggestive of viable tumoral tissue ( left , arrow ) ; b residual tumor is not appreciable in any slice of 3d i - slice reconstruction ( slice thickness 1.5 mm ) agreement , thus encouraging a more extensive use of 3d ceus in order to exploit the volumetric acquisition for a better assessment of tumoral geometry and orientation . nevertheless , in our series , such an improvement of sensitivity did not allow 3d ceus to detect a residual tumor after rfa of a deeply located ( 100 mm ) hcc sized 2 c this focus of still viable tumoral tissue was detected by 2d ceus , probably because of its intrinsic capability of realtime evaluation of tumoral vascularisation . 
to this regard , 3d ceus is more similar to mri and ct , and further studies are needed to evaluate the improvement in spatial and temporal resolution provided by the recently introduced new electronic matrix probes . 
despite lacking real - time features , 3d ceus appears to be promising in the calculation of tumor volume , definition of spatial geometry , and in detecting new foci of hcc occurring in patients already treated by means of lrt [ 8 , 17 , 18 ]  . in our series , both 2d and 3d ceus misdiagnosed a successfully rfa - treated hcc as residual tumor because of the presence of a peripherally located centimetric hypervascular nodule . 
a axial baseline image of the right lobe in a 80 - year - old woman shows a 3 - cm subcapsular hypoechoic area in the segment v ( arrow )  . 
b 2d ceus in the arterial phase shows a hypervascular focus ( arrow ) at the periphery of the treated area ; c 3d i - slice reconstruction ( slice thickness 0.9 mm ) confirms the same finding slice by slice follow - up with mr and ct confirmed the stability of this area , eventually considered as an arterial - dependent hyperperfusion defect following rfa which showed increased arterial contrast enhancement on all imaging modalities , including ct , mri , and ceus [ 19 ]  . 
although some authors consider any nodular arterially enhancing area within or along the margin of the ablated zone suspicious of viable tumor , our finding suggests that including the washout sign may improve the specificity in the detection of viable tumoral tissue after lrt [ 10 , 20 ]  . 
the rim of hyperemia may sometimes be difficult to differentiate from actual residual tumor , but usually it should be thin , regular , completely surrounding the ablation area , and disappearing over time [ 6 ]  . time consumption does not seem to represent a major limitation of 3d ceus technique , considering that in our experience a complete evaluation of each volumetric dataset lasted on average less than a minute . this prospective study had some limitations . 
this is the reason why we have only relied on vascularisation criteria of response to ablation and we have not 1 3 704 radiol med ( 2015 ) 120 : 695704 performed a volumetric assessment of treated area . 
further studies are needed to address this specific issue . in conclusion , in our preliminary experience , 2d and 3d ceus provided similar diagnostic performance in the assessment of therapeutic response of hcc treated with lrt . conflict of interest the authors declare no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2015 ) 120 : 753758 doi 10.1007 / s11547 - 015 - 0512 - 6 radiotherapy organ sparing and clinical outcome with stepandshoot imrt for head and neck cancer : a monoinstitutional experience rosario mazzola giuseppe ferrera filippo alongi mariella mannino boris abbate teresa cucchiara giuseppina iacoviello francesco scium gioacchino di paola manuela federico livio blasi antonio lo casto roberto lagalla domenico messana received : 11 march 2014 / accepted : 12 may 2014 / published online : 7 february 2015 italian society of medical radiology 2015 abstract purpose intensity - modulated radiotherapy has been suggested as the technique of choice for locally advanced head and neck cancer patients . 
we report our experience for parotid gland and constrictor muscle sparing with intensitymodulated radiotherapy in head and neck cancer using a step - and - shoot technique . methods thirty - four consecutive patients with squamous cell carcinoma of the nasopharynx , oropharynx and larynx treated between june 2008 and june 2011 were retrospectively evaluated . 
blasi medical oncology , arnas civico hospital , palermo , italy surgery and radiotherapy , with or without chemotherapy , represent the standard treatment approach for most patients with head and neck cancers ( hnc )  . 
several studies have shown that conventional 3d conformational radiation therapy ( 3d - crt ) can significantly affect quality of life of head and neck cancer patients , causing acute and delayed side effects , such as xerostomia and dysphagia [ 1 ]  . it has been also shown that , due to the possibility of producing concave dose distributions with better avoidance of dose - limiting structures , intensity - modulated radiotherapy ( imrt ) reduces acute and late toxicity rates 1 3 754 radiol med ( 2015 ) 120 : 753758 without compromising clinical outcome [ 210 ]  . 
in particular , doses to the pharyngeal constrictors and larynx have been associated with dysphagia [ 11 , 12 ] , while doses to the parotid glands are correlated with xerostomia [ 4 , 1316 ]  . 
the ability to paint the dose with imrt introduces the need for more precise contouring of organs at risk ( oar ) and planning target volume , due to a greater risk of missing the target compared with traditional radiation therapy techniques [ 1722 ]  . 
to minimise the risk of xerostomia , the parotid glands have been evaluated in terms of volumes and doses changed and several trials have stated that imrt re - planning is mandatory in selected cases . 
in this paper , we report our experience and results of parotid gland and constrictor muscle sparing using step - and - shoot imrt in patients with early and loco - regionally advanced hnc . materials and methods we reviewed the records of 34 patients with primary hnc , treated between june 2008 and june 2011 . 
of these , 12 patients ( 35 % ) received imrt as definitive treatment and 22 ( 65 % ) as post - operative treatment with or without sequential and / or concurrent chemotherapy ( platinum based )  . 
patient characteristics are shown in table 1 . initial evaluation included clinical and laboratory examination , computed tomography ( ct ) and / or magnetic resonance imaging ( mri ) scans of the head and neck region and endoscopy with histological confirmation . 
each patient underwent a ct scan without contrast media and with 2.5 mm slice thickness using an individual head - neck mask for patient positioning . in the radical setting , gross tumour volume ( gtv ) , highrisk subclinical disease ( clinical target volume 1 , ctv1 ) and low - risk subclinical disease ( clinical target volume 2 , ctv2 ) were defined on ct scan after simulation procedure . 
pc was outlined as a single structure for which the cranial limit was the caudal tips of the pterygoid plates and the caudal limit was the inferior border of the cricoid cartilage . acute and late dysphagia and xerostomia were assessed according to the rtog / eortc scale at 6 , 12 and 24 months . imrt was performed with a 6 mv photon beam and step - and - shoot technique delivered with a linac integrated mlc collimator ( primus siemens healthcare usa )  . 
oar contoured routinely , and relative dose constraints were as follows : spinal cord and brain stem with a maximum dose ( d1% ) of 45 and 54 gy , respectively ; larynx and parotid glands with a mean dose < 50 and < 26 gy , respectively . 
the measured distribution was compared with the calculated one by evaluating gamma criteria of 3 % / 3 mm using a threshold of 10 % . to assess side effects , patients were examined weekly during radiotherapy , and after treatment completion , they were seen every 3 months for the first year and every 46 months thereafter . 
time to recurrence and overall survival were calculated from the date of diagnosis . results planning end points were achieved for each study case : in all imrt plans , the dose constraints reported above were respected according to the dose prescription to the ptvs . 
 the average dose to the pharyngeal constrictors was between 51.8 gy ( 10 cc ) and 52.86 gy ( 13 cc )  . the median follow - up period of the study was 43 months , with a range of 2364 months . 
late toxicity was assessed at 6 , 12 and 24 months with an actuarial incidence of g2 xerostomia and dysphagia after 2 years of 12 and 23 % , respectively . at 24 months , late xerostomia g1 was associated with a mean dose to the contralateral parotid glands 26 gy ( p < 0.001 ) ( table 3 )  . 
 decreased saliva output causes alterations in speech and taste and difficulties with mastication and swallowing , with strong correlation with dysphagia - related quality of life [ 30 ]  . 
in our series , a mean parotid contralateral dose > 26 gy showed 1 3 756 radiol med ( 2015 ) 120 : 753758 a threefold increase in the risk of xerostomia 24 months . g1 at the pharyngeal constrictors are also involved in late dysphagia . 
including only the lateral retropharyngeal nodes in the target and excluding the medial ones , rarely a site of metastasis , it is possible to spare a large part of the muscle [ 35 ]  . 
this result could be due to inter - observer variability in the delineation of oar , as suggested by the wide range of average doses recorded for the pharyngeal constrictors . 
however , a limit of the present analysis is the fact that the pharyngeal constrictors were defined at planning in only 53 % of patients . even though a comparative analysis with another conventional technique was not available at the moment of the present evaluation , the toxicity profile of our imrt study seems to be acceptable . 
starting from this background , we are collecting data of pre - treatment symptoms prospectively and we will report a comparative analysis , comparing also toxicity with a historical population subjected to conventional 3d - crt . the potential advantage of imrt in physical dose distribution , with its tight conformality due to steep gradients , could translate into a higher risk of geographical missing . 
 some imrt series reported a higher incidence of marginal failure and intra - parotideal recurrence [ 4 , 38 , 39 ] , and one randomised study showed more in - field failures in the imrt group compared with conventional radiation [ 36 ]  . 
in our series , the two local recurrences occurred in field with no correlation with the attempt to spare the parotid glands or pharyngeal constrictors . although imrt has been reported as the best choice to reduce toxicity , especially in terms of xerostomia , the findings of local control and outcome are still inconclusive . 
 keeping in mind that our study includes different cancer sites and has a short follow - up , our results are in line with other series in terms of overall survival and local control [ 1 , 40 ]  . different primary tumour sites were found to be associated with different rates of both preand post - therapy 1 3 radiol med ( 2015 ) 120 : 753758 swallowing abnormalities . 
the main criticism of the present report is represented by the heterogeneity of the population of study in terms of site of the primary tumour affecting doseresponse relationships . conclusions acceptable rates of late dysphagia and xerostomia were achieved with optimal disease control . 
two radiologists and two ophthalmologists , divided into pairs , measured peak systolic velocity ( psv ) , end - diastolic velocity ( edv ) and resistivity index ( ri ) of each vessel using a different cdi device for each group . 
the concordance between two measurements was evaluated with lins concordance correlation coefficient ( ccc )  . results globally , very good degrees of intra - operator concordance were obtained for the psv ( 0.859 cm / s ) , edv ( 0.834 cm / s ) and ri ( 0.859 ) of the oa . 
there was moderate concordance for psv ( 0.574 cm / s ) and edv ( 0.594 cm / s ) and good concordance for ri ( 0.694 ) for the cra . 
de silvestri clinical epidemiology and biometric unit , foundation irccs policlinico san matteo , pavia , italy intra - operator and inter - operator concordance , rules should be adopted for timing of the examination and positioning of the probe to minimise the pressure applied on the eye . keywords colour doppler imaging ocular blood flow reproducibility introduction primary open - angle glaucoma is a wide range of chronic , progressive optic neuropathies , which have in common progressive retinal ganglion cell death with characteristic morphological changes at the optic nerve head and retinal nerve fibre layer , and visual field loss associated with these changes [ 1 ]  . 
however , the fact that there are people with statistically elevated iop without glaucoma , others that deteriorate despite significant reduction in iop and glaucoma patients with statistically normal iop ( normal tension glaucomantg ) , suggests that there are other contributing factors . 
an accurate and reproducible method to assess ocular haemodynamics could help to identify subjects at risk and improve knowledge about the disease and its progression . retrobulbar blood flow velocity can be assessed by using colour doppler imaging ( cdi ) which combines b - scan greyscale imaging of tissue structure , coloured 1 3 738 radiol med ( 2015 ) 120 : 737744 representation of blood flow based on doppler shifted frequencies and pulsed doppler measurement of blood flow velocities [ 4 , 5 ]  . colour doppler imaging is nowadays well standardised and widely used for the evaluation of the haemodynamics of supra - aortic trunks . 
however , uniform diagnostic criteria and standard assessment methods using this particular technique are not defined with regard to its use for evaluating retrobulbar blood flow : only few centres use cdi with this aim and the literature relating to this topic is relatively poor . in fact , the use of cdi for the evaluation of ocular haemodynamics is limited not only by several peculiar characteristics of retrobulbar blood flow ( the retrobulbar vessels are very small , and there is a very high inter - individual variability in their anatomical position , calibre and number ) but also by an intrinsic limitation of the technique itself ( the method is both operator dependent and device dependent )  . therefore , it was necessary to start to evaluate retrobulbar blood flow in healthy subjects first in order to establish physiological values of retrobulbar haemodynamic parameters ( peak systolic velocity , end - diastolic velocity and resistivity index ) to use as reference values for further studies in pathological subjects . 
to date , several studies have been performed to evaluate intra - operator reproducibility of cdi measurements of retrobulbar vessels ( ophthalmic artery , central retinal artery and short posterior ciliary arteries ) , and a minority have tested interoperator reproducibility [ 610 ] ; however , to our knowledge , none of them used the devices available in our clinic . the aim of our study was to evaluate intraand interoperator reproducibility of cdi in assessing blood flow velocity in the ophthalmic ( oa ) , central retinal ( cra ) and short posterior ciliary arteries ( spca ) in healthy volunteers . 
the study was carried out using two different cdi devices and four masked operators . materials and methods eligibility visit the study group comprised 16 healthy volunteers of both sexes aged over 18 years and without systemic or ocular disease . 
 the subjects gave written informed consent , and the study was conducted in accordance with the helsinki declaration . exclusion criteria were as follows : any ocular pathology in either eye , family history of glaucoma in first - degree relatives , best - corrected visual acuity < 85 ( etdrs ) in one or both eyes , one or both eyes , iop > 21 mmhg measured during the eligibility visit in an occludable angle in either eye ( shaffer grading < 2 ) , use of any ophthalmic medications , high systemic blood pressure ( bp ) during the eligibility visit ( bp > 140 mmhg and / or diastolic bp > 90 mmhg ) , any systemic disease and / or use of any systemic medications . each subject was asked to refrain from smoking and caffeine intake for at least 30 min prior to cdi examination to minimise the influence of these substances on blood flow [ 11 , 12 ]  . subjects were interviewed to obtain the history of ophthalmic diseases , systemic diseases and systemic medications . 
the final bp value was considered as the average of two readings taken at least 5 min apart in the same arm . the eye examination included uncorrected and best - corrected visual acuity testing with early treatment diabetic retinopathy study ( etdrs ) charts , slit - lamp biomicroscopy , applanation tonometry , gonioscopy and nondilated fundus examination . 
the measured waveforms represent the mass effect produced by a bundle of vessels , rather than from individual ciliary vessels as individual short posterior ciliary vessels cannot be distinguished by cdi . 
2 central retinal artery and vein antares stellar plus device identified by siemens measurements were performed with the subject in the supine position after a resting period of at least 5 mthe central artery of the retina and its vein lie close together in the centre of the optic nerve and cannot be measured separately with cdi . 
 the concordance correlation coefficient , _c ( ccc ) , can be expressed as the product of pearsons r ( the measure of precision ) and c_b ( the measure of accuracy )  . 
the altman and bland limits of agreement ( loas ) , with their 95 % confidence interval ( ci ) , within and between raters were reported as well : these represent the interval within which the absolute difference between two repeated test results may be expected to lie with a probability of 95 % [ 16 ]  . two - sided p values < 0.05 were considered statistically significant . 
however , we believe that this value does not bias the reproducibility of the cdi measurements because concordance was evaluated between two measurements obtained from the same subject . the mean and standard deviation of psv , edv and ri obtained in the first and second measurements by the four operators are reported in table 2 . 
while we found a negative correlation between the ri of the ophthalmic artery and age , no significant correlation was identified between flow doppler parameters and iop . oa ophthalmic artery , cra central retinal artery , spca short posterior ciliary artery , psv peak systolic velocity , edv end - diastolic velocity , ri resistivity index the intra - operator reproducibility was evaluated between the first and second measurements . 
good degrees of concordance were obtained for the measurements of the spca . tables 4 and 5 show the detailed results of the intraoperator reproducibility obtained by pair 1 using the esaote ultrasound machine and by pair 2 using the siemens ultrasound machine . 
however , concordance for pair 1 with the esaote ultrasound machine was moderate , with very good accuracy and precision for the oa and fair moderate for the cra and the spca . analysis of inter - operator concordance within the two pairs using the different cdi devices is detailed in tables 6 and 7 . 
an accurate and reproducible method to assess ocular haemodynamics could help identify subjects at risk and improve knowledge about disease and its progression . cdi is an ultrasound technique that can be used to noninvasively assess blood flow velocities in retrobulbar vessels . 
the slight decrease in velocities between the first and second measurements could be caused by a reduction of blood pressure and heart rate of the subject during the cdi procedure and possibly by operator factors during the examination . 
moreover , lying supine causes an increase in iop which , if associated with a reduction in blood pressure , could effect a reduction in ocular perfusion pressure and retrobulbar blood flow velocities [ 17 ]  . 
it would be useful to establish 1 3 radiol med ( 2015 ) 120 : 737744 the relation between these variables and cdi parameters by measuring blood pressure and iop before , during and after the cdi procedure with the subject in a supine position . the results of our study have highlighted the absence of correlation between retrobulbar blood flow velocities and iop ; however , our group was small and homogeneous for age and iop , and the situation may be different in a group with glaucoma . 
this was highest for the ophthalmic artery as previously published [ 13 ] and probably the result of an easier identification of the artery . the concordance values obtained in our study for the ophthalmic artery are better than those reported in a recent meta - analysis [ 13 ]  . 
the central retinal artery and the short posterior ciliary arteries had moderate - to - good concordance similar to the mean of the data reported in the literature [ 13 ]  . inter - observer reproducibility was higher in the pair of operators using the siemens ultrasound machine ( tables 4 , 5 )  . 
the poor inter - observer concordance , shown by the results reported in tables 6 and 7 , highlights the high operator dependency of the cdi examination in retrobulbar blood flow assessmenta well - known limitation of the technique . several variables contribute to this : identification of the vessel in a fixed position , angle correction , different pressure transmitted by the probe on the eye , manual doppler velocity spectrum analysis , the fact that readings are taken at different times ( the radiologist always performed cdi before the ophthalmologist )  . 
this last point is a possible confounder , and it may have been better to randomise the order of examination within the pairs . a recently published paper showed that the level of concordance obtained was good or very good . 
however , this result was obtained after an intensive training programme and manual doppler velocity spectrum analysis of all the data carried out by a single observer [ 18 ]  . if different operators obtain different data on the same subject , it is not possible to define which is the correct measurement . 
better results can be obtained after training the operators [ 19 ] ; in fact , the second measurement of the parameters showed higher levels of concordance at least in pair 2 ( table 7 )  . the low degree of concordance can also been explained by the small sample size . 
in samples , a single datum captured at odds with others is sufficient to greatly reduce precision and degree of concordance . blood flow velocities are measured with cdi , but as the diameter of the vessels cannot be measured it is not possible to directly correlate velocities to perfusion . 
to minimise these effects , it is important to keep acquisition times to a minimu it is important to understand that cdi does not provide direct evidence of perfusion at the optic nerve head . 
similarly , only a small proportion of blood flow in the short posterior ciliary arteries is responsible for the perfusion of the optic nerve head , with most going to the choroid . in this study , we have shown that measurements are operator dependent . 
to increase the concordance between observers , rules should be adopted for : timing of the examination ; position of the examiner and probe to minimise the pressure applied on the globe ; vessel identification and the angle correction ; and manual doppler velocity spectrum analysis to correctly identify psv and edv . 
in clinical practice , cdi is used to evaluate blood flow velocity in arteries larger than retrobulbar vessels , and therefore , it is highly important to optimise the settings of each ultrasound machine to obtain the most precise measurements . 
milano declare that there is no conflict of interest in this study . ethical standards all procedures followed were in accordance with the ethical standards of the responsible committee on human experimentation ( institutional and national ) and with the helsinki declaration of 1975 , as revised in 2008 . 
specific imaging findings including tumour site , maximum tumour size , shape , margin , density or signal intensity , bone invasion , periosteal reaction , calcification , and cystic areas were documented . results there were five males and four females , with median age of 34 years . 
mr scanning was performed in seven patients who demonstrated a round , oval , spindle - shaped or multilobular soft tissue mass near or inside the joint with cortical destruction and intraosseous soft tissue . 
two lesions showed heterogeneous low - to - moderate signal intensities on t1wi and mixed low signal intensities on t2wi . conclusions gctts is a benign soft tissue mass that may present as an intraosseous lesion near extremity joints and frequently occurring in foot and hand on radiological examinations . 
gctts with bone invasion should be considered when mri shows solid mass with characteristic low signal on t2 - weighted images . keywords soft tissue neoplasms giant cell tumours computed tomography scanners x - ray magnetic resonance imaging introduction giant cell tumour of tendon sheath ( gctts ) , also known as tenosynovial giant cell tumour , pigmented nodular tenosynovitis , xanthogranuloma , benign synovioma and fibrous xanthoma of synovium , is one of the most common benign soft tissue tumours [ 1 , 2 ]  . 
some scholars think that gctts with bone invasion is more aggressive and that the local recurrence rate after surgery is relatively high [ 9 ]  . gctts is a benign non - osseous lesion . 
intraosseous invasion of gctts occurs rarely and may mimic a primary 1 3 746 radiol med ( 2015 ) 120 : 745752 bone tumour , making diagnosis more challenging [ 1 ]  . 
 to the best of our knowledge , the previous literatures concerning gctts with bone invasion included only a small amount of patients with limited radiographic evaluation or principally reviewed from a clinical and / or therapeutic perspective , and most of them were case reports [ 1 , 9 16 ]  . 
therefore , clinical and radiological characteristics of gctts with bone invasion are yet to be clarified . in this study , nine cases that surgically and histologically confirmed gctts with bone invasion were retrospectively analysed . 
the purpose of this study was to analyse the x - ray , ct , mr imaging and clinical features of gctts with bone invasion . materials and methods patient population the authors institutional review board approved the present retrospective study , and the requirement for informed consent was waived . 
the clinical information including age at presentation , sex , history , symptom duration , and surgical and pathological reports was available for all nine patients . imaging procedures all patients underwent anteriorposterior and lateral or oblique plain radiographs routinely , and exposure factors varied depending on diseased region . 
ct examination was performed in four cases with a 16 - slice multidetector spiral ct scanner ( bright speed , general electric medical systems , milwaukee , wi , usa ) , according to an established protocol . 
a combination of axial , sagittal and coronal images was obtained using a t1 - weighted spinecho ( se ) sequence ( tr range / te range 360590 / 1321 ; matrix size 256 256 ) and a t2 - weighted fast se ( fse ) sequence with and without fat suppression ( tr range / te range 3 , 0005 , 180 / 62101 ; matrix size 256 256 )  . 
 contrast - enhanced images of axial , sagittal and coronal planes were obtained in four patients using a t1 - weighted se sequence with and without fat suppression ( tr range / te range 360590 / 1321 ; matrix size 256 256 ) after the injection of 0.1 mmol / kg of body weight of gadopentetate dimeglumine [ magnevist ; schering ( now bayer healthcare ) ] injected at 2 ml / s , followed by a 20 ml normal saline flush . 
field of view , slice thickness and interslice gap varied depending on diseased region and tumour size . imaging interpretation all images were reviewed retrospectively and independently by two board - certified radiologists with five or more years of experience in musculoskeletal radiology . 
data collection included tumour site , maximum tumour size , shape , margin , density or signal intensity ( with respect to adjacent skeletal muscle ) , bone invasion , periosteal reaction , calcification and cystic areas . results clinical features nine patients with a histologically proven diagnosis of gctts with bone invasion were identified . 
the symptom duration of ankle foot region was 7 months to 6 years ( median 42 months ; interquartile range 48 months ) , and two cases in hand were 6 and 8 months , respectively . 
3a , 1 3 radiol med ( 2015 ) 120 : 745752 table 1 summary of the clinical features of gctts with bone invasion patient no . sex / age location and bone invasion symptoms duration of symptoms ( min ) maximum diameter ( cm ) m / 37 f / 83 m / 27 f / 44 f / 25 m / 34 f / 56 first metatarsophalangeal joint with phalange and painful mass metatarsal bone invasion intertarsal joint with talus and calcaneus invasion painless mass cubital fossa with radius invasion painless mass distal tibiofibular joint with tibia invasion intermittent pain and swelling 72 second metacarpophalangeal joint with metacarpal painless mass bone invasion patellofemoral joint with femur invasion painful mass distal interphalangeal joint of index finger with midpainless mass dle phalanx invasion m / 20 intertarsal joint with talus invasion pain without mass after m / 29 first interphalangeal joint of foot with proximal painless mass after hallux phalanx invasion sprained ankle injury fig . 
a , b anteriorposterior and lateral radiographs showed eccentric geographic osteolytic lesions with well - defined margins in the distal tibia , c axial ct scan , d , e sagittal and coronal 2d reconstruction . 
 ct scanning showed intraosseous soft tissue mass with partial sclerotic edge , f sagittal t1wi , g sagittal t2wi , h sagittal fat - suppressed t2wi , i sagittal contrast - enhanced scan . 
the history of trauma is noted in about 721 % of cases [ 9 , 1820 ] , and pathological features of joint degeneration and osteoarthritis are presented [ 21 ]  . 
so trauma may be one of the causes of the disease . most patients present between the third and fifth decades , with a peak incidence during the fifth decade [ 22 , 23 ]  . 
the localized form is the most common and occurs most frequently in the hand [ 25 ] , and the second most frequent site of occurrence is the 1 3 radiol med ( 2015 ) 120 : 745752 fig . 
3 gctts with bone invasion in the first phalange in a 29 - yearold man : a , b anteriorposterior and oblique radiographs demonstrated an eccentric geographic osteolytic lesion with well - defined margin in proximal phalanx . 
although rates of bone destruction or invasion may be affected by different imaging modalities , rates of bone destruction or invasion on account of gctts are considered rare [ 5 , 26 , 27 ]  . radiological manifestations of gctts include soft tissue mass and bone changes [ 21 , 26 , 27 ]  . 
the high attenuation of the soft tissue mass due to haemosiderin - containing deposition or bleeding on ct may , however , be a clue in making the diagnosis [ 14 ]  . 
mri typically manifests as a localized or diffuse solid soft tissue mass with round , oval , spindle - shaped or multilobular shape which is mainly near or inside the joint . 
low , intermediate or mixed signal intensities may be presented due to different amount of haemosiderin , haemorrhage and 1 3 750 radiol med ( 2015 ) 120 : 745752 fig . 
4 gctts with bone invasion in the second metacarpal bone in a 44 - year - old woman : a oblique radiograph demonstrated an eccentric , well - defined osteolytic lesion with local soft tissue mass in the head of the second metacarpal bone , b , c coronal t1wi and t2wi , d , e coronal and axial fat - suppressed t2wi . 
mri presented a local solid soft tissue mass which was moderate signal on t1wi , slightly high signal on t2wi and mixed high signal on fat - suppressed t2wi collagen fibres . 
the blood supply may have nothing to do with intraosseous growth of gctts . the differential diagnosis of gctts with bone invasion mainly includes lesions that also exhibit low signal intensity on t2 - weighted images , such as pigmented villonodular synovitis , fibromatosis ( desmoid ) , haemophilic pseudotumour , amyloidosis , mineralized lesions and foreign bodies . 
haemophilic pseudotumour , amyloidosis , mineralized lesions and foreign bodies may be seen as a low signal mass on both t1and t2 - weighted images but can be identified by careful evaluation of radiographs and correlation with the patients medical history and clinical examination [ 17 ]  . several limitations of our study should be mentioned . 
third , the ultrasound had not been used widely in our institution to evaluate soft tissue 1 3 radiol med ( 2015 ) 120 : 745752 table 2 imaging manifestations of gctts with bone invasion imaging manifestations no . 
all these would be the focus of our future research work . in summary , gctts is a benign soft tissue mass that may present as an intraosseous lesion near extremity joints and frequently occurring in foot and hand on radiological examinations . 
it is useful to improve diagnostic accuracy , guide clinical treatment and follow - up . conflict of interest the authors declare no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2015 ) 120 : 10711077 doi 10.1007 / s11547 - 015 - 0533 - 1 radiotherapy clinical outcomes and toxicity after exclusive versus postoperative radiotherapy in supraglottic cancer : new solutions for old problems ? the case of stage i and ii disease michela buglione1 sara pedretti1 loredana costa1 federica foscarini1 marta maddalo1 ludovica pegurri1 nadia pasinetti1 stefano ciccarelli1 sandro tonoli1 stefano maria magrini1 received : 3 january 2015 / accepted : 16 march 2015 / published online : 28 march 2015 italian society of medical radiology 2015 abstract purpose to compare acute and late toxicities , survival , and laryngeal preservation after radiotherapy alone ( rr ) or radiotherapy after partial laryngectomy ( plr ) in early supraglottic laryngeal cancer . materials and methods from 1984 to 2012 , 172 patients were treated in our department . 
younger age and a good performance status persisted as a predictive factor of better survival ( os and dss ) at multivariate analysis . conclusion radical radiotherapy appears to be a viable alternative to conservative surgery , even in elderly patients with poor performance status and comorbidities . 
the optimal treatment , however , remains controversial , mostly because of the absence of definitive prospective trials comparing the therapeutic options . treatment of patients with advanced supraglottic larynx cancer is completely different : conservative surgery is unusually used and demolitive surgery or radiochemotherapy represents the possible options . 
again , patients with risk factors are usually given postoperative radiotherapy . from january 1984 to december 2012 , 708 patients with supraglottic larynx cancer were treated with radiotherapy at the radiation oncology department at spedali civili hospital , brescia university . 
in this paper , we describe the results obtained with the analysis of the early - stage subgroup , while in a companion paper we will illustrate the case of advanced - stage disease . 1 3 1072 materials and methods the endpoint of this retrospective study is to compare acute and late toxicities , survival , and laryngeal preservation rate after different treatment options for patients with supraglottic laryngeal cancer : radiotherapy alone ( rr ) and radiotherapy after partial laryngectomy ( plr )  . in our series , from 1984 to 2012 , 708 patients affected with supraglottic cancer were treated consecutively with radiotherapy at the radiation oncology department , spedali civili hospital , brescia university . 
four patients were excluded from the statistical analysis : three patients affected by locally advanced disease and treated with conservative surgery and inadequate radiation therapy and one who refused to continue treatment at a dose of 38 gy . even if , for retrospective studies , formal consent is not required , all the analyses have been performed according to the ethical standards of the institution and / or national research committee and to the 1964 helsinki declaration and its later amendments . the subgroup of 172 patients with early - stage supraglottic cancer was analyzed in this paper , while the remaining 532 patients with locally advanced tumors will be the subject of a companion paper . the acute and late toxicities were retrospectively re - categorized according to ctcae v 4.0 , using both the information and the rtog scale scores reported in the medical records . 
the toxicity was considered acute if detected in the period between the start of radiotherapy up to 30 days after the end of the treatment , while late toxicity was registered from 90 days after the end of treatment until the last follow - up visit . acute toxicity was recorded in all patients , while the late one was recorded in 156 patients , excluding 16 patients , who continued the follow - up visits in other oncological centers . 
we considered as acute toxicity : mucosal and skin toxicity , dry mouth , dysphagia , and laryngeal and neck edema ; as late toxicity : skin toxicity , dry mouth , dysphagia , jaw necrosis , and laryngeal and neck edema . 
the incidence of toxicities in the two different groups identified according to treatment modality ( rr and plr ) was compared with the chi - square test . an analysis of the cumulative incidence of late toxicities was also performed : we took into account the period between the end of radiotherapy to the onset of toxicity or last follow - up visit . 
the analysis of cumulative toxicity was done with the kaplanmeier estimator ( log - rank test ) : we considered as event the toxicity onset , either of any grade or of high grade only ( g34 )  . we analyzed and compared , for the two treatment groups , the following survival data : overall survival ( os ) , ( dss ) , disease - free survival disease - specific survival radiol med ( 2015 ) 120 : 10711077 ( dfs ) , local relapse - free survival ( lrfs ) , nodal relapsefree survival ( nrfs ) , and metastasis - free survival ( mfs )  . 
 the following were considered events , respectively : death for any cause ( os ) , death caused by cancer or its treatment ( dss ) , any type of treatment failure ( dfs ) , failure at the tumor site / tumor bed ( lrfs ) , nodal failure ( nrfs ) , and distant failure ( mfs )  . 
then the factors linked with significant differences in outcome at univariate analysis were entered into the multivariate stepwise cox proportional hazard ratio model . laryngeal preservation was analyzed by comparing the number of salvage total laryngectomies performed , both for toxicity and for recurrence , in the two treatment groups ( rr and plr ) ( chi - square test )  . 
the pharyngolaryngeal preservation rate was evaluated as the percentage of patients alive after 1 and 3 years from the end of radiotherapy without salvage total laryngectomy and with normal pharyngo - laryngeal functionality ( no tracheostomy nor severe laryngeal edema , no severe dysphonia , and no severe swallowing disorders such as 3 - month nasogastric feeding tube ) [ 5 ]  . 
the relationship between these events and treatment modality was analyzed with log - rank test . statistical analysis was performed using the proprietary software spss 17.0 ; p < 0.05 was considered statistically significant . results in this subgroup with early - stage cancer , 142 patients underwent radical radiotherapy and 30 were given adjuvant radiotherapy after partial laryngectomy . 
until the last decade of the past century , all patients were evaluated firstly in the ent department and there they decided the therapeutic options , in relation to comorbidities , age , or performance status . 
the multidisciplinary evaluation of all patients affected with head and neck cancer was carried out at our institution over the last 20 years : in this occasion , all clinical cases are discussed at diagnosis and the therapeutic options are defined in relation to the clinical features of disease . 
in the rr group , only four patients underwent fine - needle aspiration cytology ( no cancer cells detected ) because of the suspicious appearance of an enlarged lymph node at neck ultrasound , whereas in the plr group 14 patients had a selective dissection , five patients a radical nodal dissection , and only 11 patients were not submitted to neck dissection . forty percent of the patients had no pre - treatment instrumental examination but the ent visit , and the remaining 60 % had ct , mri , and / or ultrasound of the neck . 
the staging modality of laryngeal cancer has changed over the last decades : 67 % of patients treated before 1990 ( 40 pts ) were staged only with laryngoscopy and clinical examination , while progressively in the 90s the use of ct and ultrasound of the neck ( 69 pts80 % ) has been implemented ; in the last decade , all patients ( 24 pts100 % ) were staged with instrumental examination ( mri or ct and ultrasound of the neck )  . the majority of the patients were accrued before the year 2000 ( 149 patients )  . 
therefore , for 85 % of patients ( 148 / 172 ) a 2d technique was adopted , treating the posterior neck nodes with electrons after 40 gy ; 9 % ( 14 patients ) with a simpler 3d technique ( three half beams , one frontal and two lateral ) and seven patients with conformal 3d radiotherapy . 
patient age , performance status , grading , clinical t , and comorbidities did not influence the choice of the radiotherapy technique that was influenced only by the accrual period : before 2000 , 98 % of the patients received a 2d treatment , whereas after 2000 only 3d and imrt techniques were used ( 88 and 12 % of the cases , respectively )  . approximately 30 % of patients ( n 55 ) were given radiotherapy to the site of disease / tumor bed , while the remaining 70 % ( n 117 ) had also a prophylactic treatment on the neck ( levels iiiv bilateral )  . 
1 cumulative incidence of late mild dry mouth ( p more frequent among plr patients ( b ) 0.02 ) is higher among rr patients ( a ) , whereas skin toxicity ( any grade , p 0.05 ) is discussion both surgery and radiotherapy as primary treatment for early laryngeal cancer have their advocates ; many papers have been published in the literature describing the results of both modalities [ 68 ]  . 
 [ 9 ] , in a retrospective study of 653 patients treated over a 45 - year period , reported the longterm treatment results for supraglottic laryngeal cancer with nine different treatment modalities . 
no treatment modality produced a survival advantage , but subtotal supraglottic laryngectomy obtained the best rate of laryngeal preservation and it consequently recommends its use in eligible patients ; the importance of clear resection margins is stressed . in a study comparing surgery to radiotherapy in early glottic and supraglottic cancer , jones et al . 
however , a large number of patients treated surgically did not undergo elective staging and / or treatment of the neck at the time of primary tumor resection . a comparison remains elusive also because of difficulties in defining early disease and because of the differences in the staging modality ( clinical staging may not correlate with pathologic staging )  . 
thus , understaging is obviously a possibility when patients are treated with radical radiotherapy , because only clinical staging is available [ 10 , 11 ] , as documented by the surgical series . in our series , 83 % of patients with clinical stage i and ii have been subjected to radiotherapy alone and 17 % to complementary radiotherapy after partial laryngectomy for positive margins , because pathologic stage was different from the clinical one . 
most patients in the surgical group ( 70 % ) were understaged : all the patients , staged t2 after surgery , were staged as t1 at clinical staging . also the type of involvement of metastatic cervical lymph nodes has an impact on survival . 
patients with extracapsular spread involving multiple nodes have worse survival rates , reflected by a higher rate of locoregional and distant metastases , when compared with those with extracapsular spread in a single lymph node [ 12 ]  . understaging is also associated with the risk of occult nodal metastases and consequently to undertreatment and to a worse prognosis . 
in our series , 53 patients of the radical radiotherapy group did not undergo neck imaging ; all nodal recurrences were found in this group of patients , treated before 1995 , when instrumental imaging was not routinely used , and 26 patients underwent radical radiotherapy directed only to the tumor site , without prophylactic treatment of cervical nodes . 
in our series , patients undergoing radical radiotherapy , especially if treated before 1995 , were thus negatively selected because they were understaged . also , in our series , a direct comparison of patients receiving radiotherapy with those treated with surgery alone is not possible . 
our results with radical radiotherapy should therefore be compared with the surgical series of the literature . many retrospective studies about the use of conservative surgery for early supraglottic larynx cancer are available in the literature , and several surgical approaches were evaluated : open partial laryngectomy and more recently transoral robotic or laser approaches . 
both of these approaches obtained good local control rates . mostaf and youssef [ 13 ] retrospectively analyzed a series of 216 patients who underwent open partial laryngectomy , with good local control of disease and a dfs of 90 % at 1 year after treatment . 
the incidence of total laryngectomy for recurrence was 3 % in the laser group and 7 % in the transcervical group , with no significant differences between the two groups . 
 [ 16 ] reported a 5 - year disease - specific survival rate of 89 % with transoral microsurgery versus 80 % with the transcervical surgery , with no significant differences between the two groups in survival or organ preservation rates . 
functional results of transoral resection are generally better than those of the conventional open approach in terms of the time required to restore swallowing , tracheotomy rate , and hospital stay . 
 functional results depend from the extent of the resection : higher postsurgical swallowing and eating scores have been found in patients with complete supraglottic laryngectomy than in patients receiving a partial resection . 
local control was 89 % at 1 year and 78 % at 5 years ; consequently , only 9 ( 6 % ) salvage laryngectomies and rare severe pharyngolaryngeal toxicities were registered : the larynx preservation rate is similar to that of the surgical series in the literature . conclusion in early - stage supraglottic cancer , radical radiotherapy appears to be a viable alternative to conservative surgery , with similar results in terms of locoregional control , even in elderly patients with poor performance status and many associated diseases . 
the reduced incidence of xerostomia 1 3 radiol med ( 2015 ) 120 : 10711077 1077 in these patients can be explained with the use of smaller treated volumes , nowadays safer because of a more careful staging of the neck nodes . salvage laryngectomy rates ( for both recurrent disease and toxicity ) and incidence of severe swallowing toxicities in the rr group was compared favorably with those reported in other conservative surgery series and in the group treated postoperatively of our series . the long - term results obtained in this large historical series , mostly accrued in the 2d radiotherapy era , therefore , seem to underline the role of exclusive radiotherapy in the treatment of these patients , due to the present availability of more effective conformal techniques and of accurate imaging for nodal staging . conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with animals . 
this analysis , even if is a retrospective analysis and doesnt need a formal informed consent , has been conducted according to the ethical standards of the institution and / or national research committee and with the 1964 helsinki declaration and its later amendments . radiol med ( 2015 ) 120 : 10211023 doi 10.1007 / s11547 - 015 - 0537 - x editorial editorial on the european society of gastrointestinal endoscopy ( esge ) and european society of gastrointestinal and abdominal radiology ( esgar ) guideline on clinical indications for ct colonography in the colorectal cancer diagnosis andrea laghi1 emanuele neri2 daniele regge3 received : 20 january 2015 / accepted : 31 march 2015 / published online : 12 april 2015 italian society of medical radiology 2015 abstract european society of gastrointestinal endoscopy ( esge ) european society of gastrointestinal and abdominal radiology ( esgar ) guideline was generated jointly by a team of researchers , including gastrointestinal radiologists and endoscopists , and represents the first full collaborative effort between the two specialties after years of turf battles involving ct colonography ( ctc ) and colonoscopy ( cs )  . 
this guideline has a main educational purpose and it represents the attempt to find a consensus about the use of ctc in clinical practice based on the best current available evidence . 
main recommendations include the use of ctc as the radiological examination of choice for the diagnosis of colorectal neoplasia , the use of ctc in the case of incomplete cs , and the possible use of ctc as an acceptable and equally sensitive alternative for patients with symptoms suggestive of colorectal cancer ( crc ) , when cs is contraindicated or not possible . 
esgeesgar guideline does not recommend ctc for population screening , but considers that ctc may be proposed as a crc screening test on an individual basis ( opportunistic screening ) provided the screenee is adequately informed about test characteristics , benefits and risks . 
hospital , sapienza - universit di roma , 04100 latina , italy 2 diagnostic and interventional radiology , university of pisa , pisa , italy 3 candiolo cancer institute - fpo , irccs , str . 
knowledge about ctc is in continuous evolution and this means that a revision might be necessary in the future as new data appear . keywords computed tomography colonography virtual colonoscopy ct colonography , indications ct colonography , guideline the twentieth anniversary of ct colonography ( ctc ) ( 19942014 ) sets another milestone in the history of this technique , following the publications of the first two randomized clinical trials on asymptomatic subjects [ 1 ] and symptomatic patients [ 2 , 3 ] , respectively , and the updated edition of guidelines on ctc examination protocols [ 4 ]  . 
in fact , the first guideline on indications for ctc was recently and simultaneously published on european radiology [ 5 ] , the official journal of the european society of radiology ( esr ) and its sub - specialty societies , in this case the european society of gastrointestinal and abdominal radiology ( esgar ) , and on endoscopy [ 6 ] , the official journal of the european society of gastrointestinal endoscopy ( esge )  . 
this guideline , the result of the collaboration between esgar and esge was generated jointly by a team of researchers , including gastrointestinal radiologists and endoscopists , and represents the first full collaborative effort between the two specialties after years of turf battles involving ctc and colonoscopy ( cs )  . 
simultaneous publication in the respective leading european journals , and particularly , in the endoscopic journal , is an extremely important signal towards the full implementation of ctc in the gastroenterological community , also in centres , which are still reluctant . 1 3 1022 radiol med ( 2015 ) 120 : 10211023 esgeesgar guideline gives an updated and shared view about ctc in different situations encountered during clinical practice and related to colorectal cancer diagnosis . the first statement , on one side , recommends ctc as the radiological examination of choice for the diagnosis of colorectal neoplasia , and on the other side , does not recommend barium enema ( be ) in this setting any more . 
although obvious in academic and non - academic referral centres , the use of ctc is still far to be implemented in local environments where turf battles still exist , because radiologists are often not trained and therefore may not have adequate expertise to implement ctc in the local practice . reasons for discouraging the use of be are plenty , but probably unknown to the medical community outside research centres . 
with the term medical , we refer not at radiologists and gi specialists , but particularly to general practitioners , who are in many cases unaware of the advantages of ctc in comparison with be and the absolutely clear disadvantages of be , namely lower sensitivity and specificity than ctc for detecting colorectal polyps > or 6 mm , which are the lesions recommend for polypectomy [ 7 ] , higher patient discomfort [ 8 ] and higher level of radiation exposure [ 9 ]  . the most important indication for ctc remains incomplete cs , to be performed preferably on the same day . 
if the reason for incomplete cs was an obstructing colorectal cancer , good clinical practice includes the use of intravenous contrast medium to perform a complete pre - operative staging of the neoplastic lesion [ 11 ]  . 
moreover , more and more frequently , elderly and frail patients , with significant comorbidities and / or in therapy with anticoagulant drugs , are immediately referred to ctc after a first unsuccessful attempt with cs . 
nonetheless , the ability to detect and remove early colonic lesions , the possibility to perform histologic analysis of diagnosed crc and the higher sensitivity for the detection of colitis and anal pathology remain potential advantages of cs over ctc . 
further research is needed in this area to better stratify the patients to refer those with higher probability to find a lesion to cs and the others to ctc . another important problem encountered in clinical practice is the need for endoscopic polypectomy after a lesion is detected at ctc . 
esgeesgar recommends the referral to polypectomy in case of polyps 6 mm in diameter detected at ctc , and suggests ctc surveillance only in those who do not undergo polypectomy for any reason . 
for this reason , esge and esgar do not recommend ctc as a primary test for population screening , but since there is clear evidence of the high diagnostic accuracy of ctc , both societies consider that ctc may be proposed as a crc screening test on an individual basis provided the screenee is adequately informed about test characteristics , benefits , and risks . 
this statement follows the recommendation of the american cancer society in 2008 that included ctc in the list of optional screening tests for asymptomatic average - risk individuals [ 19 ]  . concerning screening for individuals with a positive firstdegree family history of crc , the evidence is still limited [ 20 ] and at the moment clear recommendations cannot be provided . 
this is similar to the potential use of ctc for surveillance after curative - intent resection of crc or in patients with high - risk polyps in surveillance after polypectomy . 
in both situations , cs is still the examination of choice and ctc should be considered only if cs is unfeasible . finally , ctc is contraindicated in patients with active colonic inflammation and in those who have recently undergone colorectal surgery . other statements of great interest for those performing or willing to perform ctc are available in the full papers , downloadable from the web . esgeesgar guideline represents the first attempt of a radiological and a gastroenterological endoscopic society 1 3 radiol med ( 2015 ) 120 : 10211023 1023 to find a consensus about the use of ctc in clinical practice based on the best current available evidence . 
2692 / 3110 ( 87 % ) hcc were hypointense on gd - eob - dtpa - enhanced hepatocyte - phase mri , 134 ( 4 % ) isointense ; 106 ( 3 % ) hyperintense and 178 ( 6 % ) iso - hyperintense . 
 among moderately differentiated hcc , 774 ( 88 % ) were hypointense , 8 isointense ( 1 % ) , 27 hyperintense ( 3 % ) , 74 iso / hyperintense ( 8 % )  . 
delle grazie , pozzuoli , napoli , italy institute of bio - structure and bio - imaging of the national research council ( cnr ) , naples , italy hccs , 245 ( 98 % ) were hypointense , one isointense , one hyperintense and four iso - hyperintense ( 2 % )  . 
conversely , the percentage of lesions hypointense is significantly more represented in poorly differentiated hcc compared to well - differentiated and moderately differentiated hcc . keywords hcc contrast medium liver introduction hepatocellular carcinoma ( hcc ) is the fifth most common tumour worldwide and the third most common cause of cancer - related death , after lung and stomach cancer [ 1 ]  . 
according to the american association for the study of liver diseases ( aasld ) [ 3 ] , contrast - enhanced multidetector computed tomography ( ce - mdct ) and magnetic resonance imaging ( mri ) are the best imaging modalities currently available in the diagnosis and staging of hcc [ 4 ]  . 
 two combined extracellular and hepato - biliary gadoliniumbased contrast agents are currently available with the aim to assess hepatocellular function , in addition to vascularity , the gadobenate dimeglumine ( multihance , bracco , italy ) and the gadolinium - ethoxybenzyl - diethylenetriamine - pentaacetic acid ( gd - eob - dtpa ) , also known as gadoxetate 1 3 radiol med ( 2015 ) 120 : 10021011 1003 disodium / gadoxetic acid ( primovist , eovist , bayer schering pharma , germany )  . 
in relation to its more favourable pharmacokinetic and pharmacodynamic properties [ 5 ] and to the reported higher sensitivity in identifying hepatocellular carcinoma [ 6 ] , gd - eob - dtpa seems to be the most helpful diagnostic tool in predicting stepwise carcinogenesis in cirrhotic liver . 
in particular , current literature demonstrated that the hepatocyte - specific properties of gd - eob - dtpa could give some important additional information , especially when dynamic mri or ct imaging shows atypical vascular features [ 7 , 8 ]  . 
in the hepatocyte phase , typical hccs are well described as areas of low signal intensity relative to the surrounding liver parenchyma because they do not have the ability to take up gd - eob - dtpa [ 9 ]  . 
to our knowledge , there is no systematic report or review about qualitative and / or quantitative analysis of enhancement patterns of hccs on gd - eob - dtpa hepato - biliary phase and only limited data regarding the association with the hepatocyte function are currently available . 
therefore , the aim of the present study was to perform a review of previous articles , about the contrast behaviour of hccs on gd - eob - dtpa hepato - biliary phase mr imaging , to elucidate whether there is a correlation with histological tumour grading . materials and methods this systematic review was completed in accordance with the recommendations outlined in the preferred reporting items for systematic reviews statement [ 10 ]  . 
pubmed , embase , web of science , cochrane library and the chinese biomedical literature database were searched using the terms hepatocellular carcinoma or hcc , gadoxeticacid or gd - eob - dtpa or gadoxetate - disodium or primovist / eovist , magnetic resonance imaging or mri or contrast - enhanced dynamic mri , hepatobiliary phase or hepato specific phase , focal liver lesions , cirrhotic liver or cirrhosis , liver specific contrast agents ( last search update september 2013 )  . 
they independently studied full text copies to make a decision as to which studies met the inclusion criteria . inclusion and exclusion criteria inclusion criteria were : ( 1 ) patients suspected of having hcc , undergoing hepatic gadoxetic acid disodiumenhanced mr imaging including the triple dynamic postcontrast ( arterial , portal , venous ) phase and hepato - biliary phase ; ( 2 ) patients receiving a diagnosis of hcc based on surgical findings ( pathological examination or intraoperative ultrasound ) , findings at percutaneous / ultrasound core - needle biopsy , or on a follow - up period including a typical clinical history with tumour marker levels in combination with lipiodol uptake after transhepatic arterial chemoembolization ( tace ) , or the progression of the disease as depicted at follow - up diagnostic ( ct / mr ) imaging performed at least 36 months after the initial imaging ; ( 3 ) where available hepatocellular carcinoma was histologically classified , according to the definition of the world health organization [ 11 ] on the basis of edmondson and steiner criteria [ 12 ] as follows : well - differentiated , moderately differentiated , poorly differentiated ; ( 4 ) mr image analysis performed in consensus by at least two radiologists with at least 5 years of abdominal radiological experience . 
studies were excluded if ( a ) any one of the inclusion criteria was not met ; ( b ) multiple reports were published for the same study population ( in this case , the publication with the most details and / or most recently published was chosen ) ; and ( c ) the study included patients who had previously undergone treatment for liver tumours . 
all mri examinations were performed using either a 1.5 or 3 t imaging systefor dynamic imaging , in all patients a dose of 0.1 ml / kg of body weight of primovist ( 0.025 mmol / ml of gd - eob - dtpa , bayer schering pharma , berlin , germany ) was injected intravenously at a flow rate of 2 ml / s , followed by 2030 ml saline flush . 
in all the reports included in our work , qualitative analysis of signal intensity ( si ) of hccs on hepato - biliary phase was performed : the relative si of hccs compared with that of the surrounding liver parenchyma was graded and recorded as low , iso , and high si . 
 according to si characteristics , on hepato - biliary phase imaging , lesions were classified into two major groups : ( a ) hypointense lesions ; ( b ) iso / hyper / iso - hyperintense lesions . 
signal intensities of the liver parenchyma and 1 3 1004 radiol med ( 2015 ) 120 : 10021011 hepatic tumour lesion were calculated and measured by placing regions of interest ( rois )  . 
the roi of the tumour was determined as the maximum oval / round area at the level of the largest diameter of the tumour ; a similar - sized roi was set over the adjacent liver parenchyma . 
the following quantitative parameters were evaluated : ( 1 ) the relative intensity ratio ( rir ) either on pre - contrast ( rirpre ) and post - contrast ( rirpost ) mr images equivalent to sinod / sipar , where sinod is the si of the nodule , and sipar is the si of the liver parenchyma ; ( 2 ) the relative enhancement ratio ( rer ) equivalent to rirpost / rirpre ; ( 3 ) the contrast enhancement ratio ( er ) of hepatocarcinoma nodule equivalent to ( post - contrast sipre - contrast si / precontrast si ) 100 . statistical analysis statistical differences in percentage of tumour uptake of gd - eob - dtpa on hepato - biliary mr imaging among the tumour differentiation degree were determined using a c2 test ( spss statistical analysis )  . 
fifteen articles were excluded because they studied the added value of gadoxetic acid mri imaging without clarifying the si of hepatocarcinoma on hepato - biliary phase gd - eob - dtpa mri . 
the number of patients ranged from 11 to 192 patients per study , with a total of 2550 patients evaluated in all included studies ( 1908 male patients )  . 
the other 604 lesions were diagnosed on radiological features as hccs on the basis of definite characteristics revealed on a follow - up period , as mentioned in materials and methods section . 
2692 out of 3110 ( 87 % ) of hccs were hypointense on gd - eob - dtpaenhanced hepatocyte - phase mr imaging , whereas 134 out of 3110 ( 4 % ) lesions were isointense ; 106 out of 3110 ( 3 % ) lesions were hyperintense and 178 out of 3110 ( 6 % ) were iso - hyperintense . in 31 out of 41 articles , the final histological classification of hccs was systematically reported , but only in 26 out of 41 of them [ 1518 , 2123 , 25 , 28 , 3137 , 4547 , 5157 ] a specific correlation between histological tumour grading and signal intensity on gd - eob - dtpa hepatobiliary phase was expressed . 
among well - differentiated hccs , 445 ( 86 % ) were hypointense on gd - eob - dtpa hepatobiliary phase , 12 isointense ( 2 % ) , 9 hyperintense ( 2 % ) , 53 iso / hyperintense ( 10 % )  . 
among moderately differentiated hccs , 774 ( 88 % ) were hypointense on hepato - biliary phase mr imaging , 8 isointense ( 1 % ) , 27 hyperintense ( 3 % ) , 74 iso / hyperintense ( 8 % )  . 
among poorly differentiated hccs , 245 ( 98 % ) were hypointense on hepatospecific phase , one isointense , one hyperintense and four iso - hyperintense ( 2 % )  . 
in particular , the percentage of lesions classified as iso / hyper / iso - hyper was the same when considering well - differentiated and moderately differentiated hccs ; when considering poorly differentiated hccs , the percentage of lesions iso / hyper / iso - hyper was significantly lower . 
in particular , kogita [ 15 ] and okada [ 32 ] , in a total of , respectively , 83 and 37 hccs , showed that the relative intensity ratio ( rirpost ) on hepato - biliary phase images of well - differentiated hccs were significantly higher than those of moderately and poorly differentiated hccs . 
 [ 47 ] demonstrated that the degree of tumour enhancement , which included the rirpre , the rirpost , and the rer for well - differentiated hccs was significantly higher than the degree of tumour enhancement for moderately differentiated and poorly differentiated hccs . 
 the contrast enhancement ratio ( er ) compared with background liver has also been used as a quantitative parameter of tumour enhancement on gd - eob - dtpa hepato - biliary 1 3 radiol med ( 2015 ) 120 : 10021011 1005 1 3 1006 radiol med ( 2015 ) 120 : 10021011 phase imaging , showing a correlation with the differentiation degree of hccs . 
accurate and early detection of hcc is crucial in cirrhotic patients and investigating about non - invasive diagnostic imaging modalities has a noteworthy impact in terms of prognosis and therapy . our review demonstrates that 87 % of 3110 hccs were hypointense on gd - eob - dtpa hepato - biliary phase . it has been well established that the hypointensity of hccs is due to diminished normal function of hepatocytes in the tumour [ 9 , 16 ] , whereas the uptake of hepatocyteselective agents occurs in normal liver parenchyma and in focal liver lesions of hepato - cellular orig in addition , it has also been demonstrated that the hepatocyte - specific properties of gd - eob - dtpa could contribute to early hcc detection and characterization [ 8 , 57 ] with reported increasing sensitivities when hepato - biliary images are obtained [ 14 ]  . according to our systematic review , 418 out of 3110 ( 13 % ) of hccs show uptake of gd - eob - dtpa in the hepatocyte phase ; appearing as iso - hyperintense lesions relative to the surrounding parenchyma on qualitative analysis . 
 [ 16 ] ; in particular , an iso - hyperintense nodule on gd - eob - dtpa hepato - biliary phase images may not be a benign nodule , especially in patients with evidence of risk of hccs . 
1 summary of study design and final histological classification of hcc that may help to characterize hyperintense lesions seen in the hepato - biliary phase of gd - eob - dtpa - enhanced mr examination and concluded that hyperintense hccs more commonly present focal defects in uptake , nodule - in - nodule appearance , absence of a central scar , internal septation and a hypointense rim in comparison to benign lesions . 
 further studies should be performed to clarify this issue ; however , it is clear that pre - contrast and vascular postcontrast mr sequences are needed for the final differential diagnosis . in our systematic review , we observed that on qualitative analysis of hepato - biliary phase images , well - differentiated and moderately differentiated hccs showed a similar percentage of hypointensity ( respectively , 86 and 88 % ) and iso - hyperintensity ( 14 and 12 % ) ; only poorly differentiated hccs showed higher incidence ( 98 % ) of hypointensity on delayed phase images , compared with 2 % of iso - hyperintense nodules . 
early studies performed on experimental liver tumours and on induced hccs in rats demonstrated that the hepatocyte - selective uptake of gd - eob - dtpa reflects tumour differentiation grade [ 38 , 40 , 41 ]  . 
 [ 16 ] demonstrated that two out of four well - differentiated hccs , in patients with liver cirrhosis exhibited an exceeding or equal uptake in comparison to the surrounding parenchyma , whereas no uptake was depicted in four moderately or poorly differentiated hcc . 
later additional experimental and clinical studies have not confirmed a correlation between hcc grade and gd - eob - dtpa uptake [ 21 , 39 , 42 , 43 ]  . 
it has been suggested that in human hepatocytes organic anion - transporting polypeptide 8 ( oatp8 ) is the most probable uptake transporter for gd - eob - dtpa , 1 3 1008 radiol med ( 2015 ) 120 : 10021011 particular , kitao et al . 
 [ 25 ] showed that moderately differentiated hccs might have a different cellular origin from the ordinary type of hccs or that they might undergo to a genetic reversion to their original hepatocyte nature during hepato - carcinogenesis . 
on the basis of our results , we can state that the percentage of lesions classified as iso / hyper / iso - hyper is the same if we consider well - differentiated and moderately differentiated hccs . 
there are few articles in the literature considering the correlation between the histological tumour grade and the quantitative analysis and , in addition , they employ different quantitative parameters ; as a consequence , it is hard to evaluate their statistical significance . 
on the basis of our literature review , in a small subset of nine articles , we have found discordant results regarding the correlation between either the relative intensity ratio ( rirpost ) on hepato - biliary phase or the contrast enhancement ratio ( er ) with tumour differentiation grade [ 15 , 32 , 33 , 36 , 47 , 51 , 56 ]  . 
 [ 9 ] in a small group of 25 patients with hccs , showed that , when considering all the tumours , hypo and iso - hyperintense within the same quantitative analysis , the ers did not differ significantly for the different tumour grades . 
 [ 33 ] used the static t1 value for measurement of the contrast enhancement ratio , because it has linearity with contrast agent concentration and is more reliable for quantitative evaluation . 
 the variable flip angle method used in their study has been proven to be useful for calculating the enhancement ratio in gd - eob - dtpa contrast - enhanced mr imaging . 
they found that , when excluding those atypical hccs showing iso - hyperintensity on hepato - biliary phase imaging , the er significantly decreased in comparison to the background liver , as the tumour differentiation declined . 
they also confirmed a significative positive correlation between the er and the grade of immunohistochemical oatp8 expression , showing a decrease from well - differentiated hccs to poorly differentiated hccs . 
therefore , according to these results , the contrast enhancement ratio might be considered a useful tool to evaluate multi - step hepato - carcinogenesis , if we consider as exception 10 % of hccs which are isohyperintense on hepato - biliary phase images and show a higher contrast enhancement ratio . 
although these hypotheses need to be confirmed in further studies and in larger patient population ; it is possible that standardizing the quantitative measurement of the enhancement ratio could fig . 
2 graph shows the percentage of signal intensity of hcc on gd - eob - dtpa hepato - biliary phase , in relation to the histological tumour differentiation which is subsequently excreted into bile secretions by mrp3 , a multidrug resistance protein [ 25 , 44 ]  . 
 [ 23 ] investigated the enhancement ratios ( ers ) and expression levels of the organic anion transporter oatp1b3 ( that is a synonymous of oatp8 ) in 22 confirmed hccs , six of which , all moderately differentiated , accumulated gdeob - dtpa in the hepato - biliary phase and showed high er . 
they showed that hccs with gd - eob - dtpa uptake overexpressed oatp1b3 compared with hccs without gdeob - dtpa uptake , consequently concluding that expression of oatp1b3 determines the hyperintensity of hccs in hepato - biliary phase , rather than tumour differentiation or bile production . 
 [ 36 ] and by kitao in two later works including a wider patient population , respectively , 32 hccs [ 25 ] and 70 hccs [ 33 ] , in which it was clearly underlined the correlation between the uptake of gd - eob - dtpa of focal lesions in hepato - biliary phase images and the oatp8 expression . 
 in addition , these authors also showed that the immunohistochemical expression of oatp8 significantly decreased , from well - differentiated hccs to poorly differentiated hccs and so they suggested oatp8 might be considered as a marker of the multi - step hepato - carcinogenesis . our results are in agreement with previous articles based on smaller patient population about the higher incidence of moderately differentiated hccs among iso - hyperintense hccs . 
the reason why this happens is still not clear ; in 1 3 radiol med ( 2015 ) 120 : 10021011 1009 table 2 quantitative analysis of tumour enhancement at hepatobiliary phase imaging inrelation to the histological grade of hccs radiol med ( 2015 ) 120 : 10781082 doi 10.1007 / s11547 - 015 - 0541 - 1 radiotherapy fourdimensional computed tomography in accelerated partial breast irradiation planning : single series from a phase iii trial icro meattini1 livia marrazzo2 margherita zani3 fabiola paiar1 stefania pallotta2 , 3 gabriele simontacchi1 marta bucciolini2 , 3 lorenzo livi1 , 3 received : 7 november 2013 / accepted : 1 april 2014 / published online : 24 april 2015 italian society of medical radiology 2015 abstract purpose the aim of our study was to evaluate the usefulness of the four - dimensional computed tomography ( 4dct ) in accelerated partial breast irradiation ( apbi ) planning . materials and methods at our institute , we have been treating the index quadrant with external intensity - modulated radiation therapy in a phase iii trial . 
on both 3dct and 4dct , we recorded the clinical target volume ( ctv ) and the planning target volume ( ptv ) and the coordinates of the ptv centroid . 
we calculated the treatment plans , according to our protocol , using the contours drawn on the 3dct and 4dct and evaluated target coverage and sparing of organs at risk ( oar )  . results median age of the patients was 63.5 years ( range 5275 )  . 
 concerning centroid coordinates , the average absolute differences were 0.1 mm in the latero - lateral , 0.7 mm in the antero - posterior and 0.3 mm in the supero - inferior direction . 
no statistically significant differences were observed both in ptv coverage and oar sparing ; the 4d ptv * icro meattini icro.meattini@unifi.it 1 radiotherapy unit , azienda ospedaliero - universitaria careggi , largo g . 
brambilla 3 , 50134 florence , italy 2 medical physics unit , azienda ospedaliero - universitaria careggi , florence , italy 3 university of florence , florence , italy contour is adequately covered when the plan based on the 3d contours is used . 
conventional 3dct - based planning is adequate for apbi . keywords partial breast irradiation four - dimensional computed tomography imrt breathing motion breast cancer introduction in the era of conformal therapy and intensity - modulated radiation therapy ( imrt ) , there is an increased desire to raise tumour dose to facilitate improved survival and decrease normal tissue dose to reduce toxicity [ 13 ]  . 
however , the accuracy of the setup and the internal motion limits the reduction in margins [ 5 ]  . the target volume for breast radiotherapy ( rt ) after conservative surgery for breast cancer ( bc ) may be affected by breathing motion . 
many experiences concerning breathing motion in whole breast treatment showed a minor relevance in postoperative rt treatment for both segmented and wedge tangential field techniques [ 6 , 7 ]  . conversely , we hypothesised a possible significant impact of breathing motion on target volume and position in accelerated partial breast irradiation ( apbi )  . 
currently , a randomised phase iii clinical trial is underway at our centre [ 8 ] to compare apbi with imrt versus conventional fractionated tangential fields to the whole breast . the aim of our study was to evaluate the usefulness of 4dct in apbi planning . materials and methods at our institute , the index quadrant has been treated with external imrt in a highly selected group of patients [ 8 ]  . 
inclusion criteria were age at presentation > 40 years , tumour size < 25 mm , wide excision or quadrantectomy with clear margins ( > 5 mm ) , clips placed in tumour bed , and full informed consent from the patient . 
treatment plans are generated with pinnacle ( version 9.2 ) treatment planning system ( tps ) ( philips radiation oncology systems , andover , ma ) with four or five coplanar step - and - shoot imrt beams . 
beam energy is 6 mv from an elekta ( crawley , uk ) synergy bm linac , for all cases . for patient setup verification , a cone - beam kvct is performed before each treatment fraction and compared to the planning ct . 
all the corrections found by the registration results are automatically applied . for this study , we selected a sample of 10 patients with rightor left - sided bc and surgical clips at the excision site . 
for this sample of patients , 3d contours were still used in a clinical setting . all patients were imaged on a brilliance big bore ct scanner ( philips healthcare , eindhoven , the netherlands ) with 512 512 resolution and 3 mm slice thickness . for generating 4dct datasets , a respiratory sensor ( an air bellows belt ) , integrated with the ct scanner reconstruction , is placed on the patients chest . 
a maximum intensity projection ( mip ) reconstruction over all the respiratory phases is used as 4dct to delineate volumes . the clinical target volume ( ctv ) was drawn with a uniform 1 - cm three - dimensional margin around the surgical clips . 
the ptv was allowed to extend 4 mm inside the ipsilateral lung and was limited to 3 mm from the skin . the ipsilateral and contralateral breast , ipsilateral and contralateral lung , the heart , and the spinal cord were contoured as oars . 
all the regions of interest were contoured according to the recommendations of the international commission of radiation units and measurements reports 50 and 62 . ctv and ptv volumes and the coordinates of ptv centroids ( defined as the mean position of all the points of the contour in all of the coordinate directions ) were defined on both 3dct and 4dct and were then co - recorded . 
 the main clinico - pathological features of the analysed patients are summarised in table 1 . the average of ctv and ptv volumes together with the mean variations in centroid coordinates is summarised in table 2 . 
 the average absolute difference is submillimetric for all the directions ; the maximum shift is 0.2 mm in the laterolateral , 5.0 mm in the antero - posterior and 0.8 mm in the supero - inferior direction . 
1 comparison of planning target volumes ( ptv ) between 3dct and 4dct plans discussion 4dct acquisition is commercially available , and provides important information on the shape and trajectory of the tumour and normal tissues [ 9 ]  . breathing motion was of minor relevance in postoperative rt treatment of bc for both segmented and wedge tangential field techniques . 
there were no significant differences in the mean breast volumes contoured on the 3dct scans , 4dct full inspiration phase , 4dct full expiration phase and the 4dct - derived average ct scans . 
4d plan prescribed dose levels were significantly lower ( p < 0.05 ) than 3d plan levels for all of the following : ipsilateral breast v100 , ipsilateral lung v30 and contralateral lung v5 . 
therefore , expanding the freebreathing ctv by 8 mm will result in the ptv extending to the skin surface and lung / chest wall interface in the anteroposterior direction , leading to increased irradiation of normal tissues . 
moreover , they found that the target range of motion was less than 2 mm in the latero - lateral and supero - inferior directions and hypothesised that expanding the free - breathing ctv by 7 mm in these directions would be sufficient . 
the authors concluded that the use of 4dct could lead to improvements in target definition and decreases in normal tissues irradiation . in accordance with previously published data , our results indicate a larger motion in the antero - posterior fig . 
 [ 7 ] , for 10 patients with left - sided bc , generated rt treatment plans based on conventional 3dct studies : two techniques ( segmented and wedge - based tangential fields ) were compared . 
the influence of breathing motion on the dose to the target and oars was evaluated with 4d dose calculation based on respiration - correlated cts . differences in dose distributions were small between segmented and wedge techniques based on 3d studies . 
 [ 6 ] investigated in 10 patient differences between conventional and 4dct - based treatment planning and whether gating could improve dose volume parameters . the maximum movement of the surgical clips was determined in the axial , sagittal and coronal reconstructions of the 4dct scans . 
the average 3d vector displacement was 3.7 mm ( range 1.76.5 mm ) , which was correlated to diaphragmatic motion and similar in 1 3 1082 radiol med ( 2015 ) 120 : 10781082 direction compared to the other directions , while the average displacements are smaller compared to those previously reported . in our analysis no significant differences between target volumes , target coverage and oars sparing were evidenced when comparing the 3dct and 4dct plans . the optimal ctv for apbi is yet to be determined ; many authors recommend that at least a 10 - mm margin around the tumour bed should be used [ 7 , 12 , 13 ]  . our study does not aim to reduce margins . 
we consider it pointless to verify the fairly obvious fact that decreasing ptv expansion allows for better oars sparing . our purpose was exclusively to try to understand , in this era of technological progress and wide availability of new tools in radiotherapy in which cost - effectiveness should always be considered , if 4dct is an absolutely essential modality to perform hypofractionated apbi with the imrt technique . the dosimetric comparison between plans generated on 3d and 4d contours did not show any significant difference in terms of both target coverage and oars sparing . 
 moreover , 4d - ptv contour is adequately covered when the plan based on the 3d contours is used , thus suggesting that planning on single - phase ct is actually adequate for apbi planning . conclusions in our experience no significant differences between ptv volumes , ptv coverage and oars sparing are evidenced when comparing 3dct and 4dct plans . 
in evaluating the lar of thyroid cancer incidence , a frequency of 0.02 per 100 , 000 from 2.94 per 100 , 000 males and a frequency of 0.10 per 100 , 000 from 16.23 per 100 , 000 females were found . 
it was concluded that beneficial exams in the medical field should not be prohibited because of a statistically small risk , although acknowledgement of the dangers of ionizing radiation is necessary . keywords entrance surface dose ( esd ) lifetime attributable risk ( lar ) organ doses monte carlo simulation pcxmc introduction diagnostic radiology is the largest source of radiation exposure among the various fields in which man - made artificial radiation is used . 
however , diagnostic radiology is a fundamental stage in the diagnosis and evaluation of modern diseases and is the basic engine , along with antibiotics , that is leading modern medical science . 
according to the korean ministry of food and drug safety , the annual amount of diagnostic radiation exposure per person increased from 0.93 msv in 2007 to 1.4 msv in 2011 , a rate of 51 % for 5 years . 
the numbers of radiation exams were 1 3 1044 radiol med ( 2015 ) 120 : 10431049 also shown to have increased from 3.3 per person in 2007 to 4.6 in 2011 [ 1 ]  . 
however , it is extremely rare for medical radiation exposure to be a cause for cancer , because the medical tests involve low - dose radiations that have a radiation dosage of less than 100 msv , which is nearly equal to that of natural background radiation [ 2 , 3 ]  . the neck ( cervical spine ) simple x - ray is the most commonly used trauma and disease diagnostic method . 
for this method , ct and mri are used optionally in order to check the neck for abnormality ( e.g. , soft tissue inflammation , infection , or tumors of the laryngopharynx ) , although they are basic test methods . 
the incidence in the risk of thyroid cancer in children and the youth exposed to radiation because of radiography tends to be 88 percent higher per 1 gy [ 4 ]  . 
according to seaberg , thyroid cancer caused by radiation exposure is likely to be more malignant compared to that of patients who have not been exposed to radiation , and the radiation exposure itself is the cause of the tumor , whether benign or malignant [ 5 ]  . 
its review of available data supports the so - called linear no - threshold risk ( lnt ) model for lowdose exposure to low - linear energy transfer radiation such as x - rays , in which the risk of cancer proceeds in a linear fashion with no lower threshold [ 3 ]  . radiation exposure contains sufficient energy to change the structure of human cells , including that of deoxyribonucleic acid ( dna )  . 
according to such mechanisms , radiation is a grade i carcinogen , and it is classified as a carcinogen by the international cancer society [ 7 ]  . taking these recent research results into account , it is apparent that damage can occur as a result of medical radiation exposure . 
chronic side effects of radiation , however , continue to occur even at low doses , and it is clear that radiation negatively influences the human body , which includes increased incidences of cancer . therefore , this study has three aims : evaluation of radiation exposure doses using a phantom ( neck ; cervical spine ) , measurement of entrance surface doses ( esd ) , and calculating the thyroid and neighboring organs doses using monte carlo simulations . 
 an auto exposure control , set according to the guidelines established by the korean ministry of food and drug administration ( kfda ) [ 12 ] and the national radiological protection board ( nrpb ) [ 13 ] , was employed . calculation of organ doses pcxmc is a pc - based monte carlo program used to calculate patient dose in medical x - ray examinations ( radiography and fluoroscopy ) and developed by stuk ( the finnish radiation and nuclear safety authority )  . 
this software uses the phantom model developed by cristy and eckerman [ 14 ] , and the phantom , projection angle ( ap , both lat . , pa : postero - anterior ) , x - ray tube ( tube voltage ( kvp ) , added filter thickness , and anode angle ) , height , weight , the parameters used in the examination , and other details for use in the calculation can be edited and selected . the effective doses show the risk for organs and tissue when the full body is under radiation exposure . 
the tissue - weighting factors are set by the international commission on radiological protection ( icrp ) 60 and 103 , as given in [ 15 , 16 ]  . 
the monte carlo simulation in this study was based on the phantom , which has patient - representative height and weight , kvp , focusimage distance ( fid ) , and projection angle . 
in terms of exposure area , the focusskin distance ( fsd ) and beam field size were calculated using fid ( ap : 110 cm , lat . : 180 cm ) values and image field size ( 25 30 cm ) , using the pcxmc software . in this study , each of the investigated x - ray tube voltages , an anode , and a total inherent filtration ( tube and collimation ) system were used . 
lateral , sd standard deviation 0.001 gy ( 1 mgy ) to the breast from a mammograthe table shows the estimated lifetime risk of being diagnosed with breast cancer for a female exposed to 0.1 gy at the age 40 as 1.41 per 100 , 000 ( approximately 1 in 70 , 000 )  . 
the results of this research indicate that , for a 0 - year - old , the following lars are likely : all cancer incidence , 65.61 per 100 , 000 males and 122.29 per 100 , 000 females ; all solid cancer incidence , 59.54 per 100 , 000 males and 117.55 per 100 , 000 females ; leukemia cancer incidence , 6.06 per 100 , 000 males and 4.73 per 100 , 000 females ; and thyroid cancer incidence , 2.94 per 100 , 000 males and 16.23 per 100 , 000 females ( table 3 )  . as regards radiation exposure , the lar showed that , females have an approximately two times higher risk for all cancers compared to males , when the age of the exposed group is lower , along with an approximately 5.5 times higher risk of thyroid cancer . 
2 trend curve of occurrence of thyroid cancer from radiation exposure according to age group discussion as the use of radiation medical equipment increases , interest in reducing the risk of cancer grows simultaneously . 
the american cancer society recently identified environmental carcinogens and radiation exposure as cancer risk factors as a result of the increased use of x - rays and computed tomography ( ct ) [ 17 ]  . 
in addition , the medical use of sunlamp , which is used for cosmetic reasons and to cure acne or other skin diseases , was included as a dangerous factor [ 18 ]  . 
this model applied the linear no - threshold ( lnt ) model , stating that even for very small doses , a minor increase in the risk of cancer can potentially cause a patient to develop cancer . 
on the other hand , current radiation protection guidelines assign a radiation weighting factor of 1 to x - rays , although some biological evidence suggests that the biological effectiveness per unit - absorbed dose of x - rays may be twice that of high - energy photons [ 3 ]  . 
while there are subtleties in the positions of each of these organizations , the majority basically conclude that lnt best fits the data and should remain the standard for radiation protection . however , in our research , the organ doses produced using the monte carlo simulation program to evaluate the risk of cancer and lar of cancer incidence have sufficient credibility . 
according to the results of this research , regarding a 0 - year - old , the lars of thyroid cancer incidence are likely to be 2.94 per 100 , 000 males and 16.23 per 100 , 000 females ( table 3 )  . 
this is said to be related to the frequency of radiology exams in each country [ 19 ]  . according to the ministry of food and drug safety in the republic of korea , the number of annual diagnostic radiography examinations was 160 , 000 , 000 in 2007 , which increased to 220 , 000 , 000 in 2011 , a rate of increase of approximately 35 % over 5 years [ 1 ]  . 
because radiation exposure doses accumulate , not only should the risk for the exposed patient should be considered , but also the genetic effects this exposure might have on his or her offspring should be taken into consideration . 
in addition , life expectancy is extended and , in recent medical trends , more scientific diagnostic methods such as radiography are applied , rather than diagnoses based on experience . 
this value is lower than the threshold dose 100 msv giving deterministic effect in 1 3 1048 radiol med ( 2015 ) 120 : 10431049 for thyroid cancer , when the exposed patients age is lower than average , while female patients , compared to males , are more likely to develop cancer . 
such results show that it is difficult to say that the recovery rate of cells in low - dose cases is good and that , therefore , a health risk does not exist . 
lowdose radiation is proven to cause chromosome damage in experimental settings , but has not been shown to be an actual cause of disease in the human body to date . 
therefore , it is not wise to ignore the fact that there is a possible lifetime risk of cancer due to low - dose medical radiation exposure , simply because it is low - dose . 
ultimately , it is not correct to say that , since no side effects have been determined , low - dose exposure is safe ; more research is required and , until then , the risk of radiation exposure should be minimized when using medical diagnostic radiography systems . there were certain limitations to our research : ( 1 ) the research sample was small and , because the study was based on cervical spine x - ray radiography , the focus was limited to thyroid cancer . 
if possible , longterm tracking observation research is necessary in the future . in our research , however , it is meaningful that we could evaluate organ doses and the lar of incidence , considering biological probable influence , to determine the actual influence on patient thyroids of cervical ( neck ) spine radiology . 
furthermore , this research is contributing to a new acknowledgement of the risks of ionizing radiation by confirming the influence of radiation on cancer incidence . conclusion the amounts of radiation absorbed by the thyroid and surrounding organs during cervical spine x - ray radiological procedures and the resultant lar of cancer incidence were found to have low values . 
even though the increase in the cancer incidence rate due to medical radiation is quite small , if other radiography exams are repeatedly conducted , the accumulated exposure will increase the incident rate of diseases including cancer . 
in the medical field , even though there is no standard base for radiation exposure doses , necessary radiology exams must be taken and , therefore , efforts to reduce radiation exposure for those undergoing frequent exams should be considered . 
this research is meaningful in that it provides information to examiners and patients who make use of medial radiation , allowing them to acknowledge the risk of ionizing radiation and helping them to make related decisions wisely . acknowledgments the authors wish to thank the 94 medical institutions within the korean central district used in this study for their cooperation . conflict of interest this study was not funded by anyone . 
the findings of several studies have shown that ultrasonography ( us ) can represent a useful and cost - effective tool in the evaluation of blunt abdominal trauma both in adults and children . 
the correct use of ceus could therefore identify and select the children who need further diagnostic investigation computed tomography ( ct ) , avoiding unnecessary radiation and iodinated contrast medium exposure . 
sensitivity , specificity , ppv , npv , and accuracy were determined for us and ceus compared to mdct . results 6 / 73 patients were negative at us , ceus , and mdct for the presence of organ injuries . 
 ceus identified 67 / 67 patients ( 67 / 67 ) with parenchymal lesions : 21 lesions of the liver ( 28.8 % ) , 26 lesions of the spleen ( 35.6 % ) , 7 lesions of right kidney ( 9.6 % ) , 13 lesions of left kidney . 
thus , the diagnostic performance of ceus was better than that of us , as sensitivity , specificity , ppv , npv , and accuracy were 100 , 100 , 100 , 100 , and 100 % for ceus and 38.8 , 100 , 100 , 12.8 , and 44 % for us . 
in some patients ceus identified also prognostic factors as parenchymal active bleeding in 8 cases , partial devascularization in 1 case ; no cases of vascular bleeding , no cases of urinoma . 
parenchymal active bleeding was identified in 16 cases , vascular bleeding in 2 cases , urinoma in 2 cases , partial devascularization in 1 case . conclusions ceus is more sensitive and accurate than baseline us and almost as sensitive as ct in the identification and characterization of solid organs lesions in blunt abdominal trauma . 
nowadays , this modality is widely accepted in europe and is becoming part for the triage of blunt abdominal trauma patients also in the united states [ 8 ]  . however , many parenchymal injuries are not correctly visualized at baseline us examination and , moreover , the absence of peritoneal free fluid does not enable serious organ lesions to be excluded [ 9 , 10 ] : some researchers have reported that 2934 % of solid organ lesions can occur in trauma patients without hemoperitoneum [ 11 , 12 ]  . ct therefore remains the radiologic standard for evaluating patients with abdominal trauma [ 13 ]  . 
the correct use of contrast - enhanced ultrasound ( ceus ) in the triage of pediatric patients with history of blunt abdominal trauma could therefore identify and select the children who need further diagnostic investigation ( ct ) , avoiding unnecessary radiation and iodinated contrast - medium exposure . radiol med ( 2015 ) 120 : 9891001 table 1 atls criteria for major trauma : physical findings adult major trauma ( including traumatic cardiac arrest ) for the purpose of this protocol , major trauma is present if the patients physical findings or the mechanism of injury meets any one of the following criteria : physical findings minute 1 . 
according to the atls guidelines [ 20 ] a major trauma is defined basing both on clinical ( table 1 ) and dynamic criteria ( table 2 ) ; all the patients who are not classified as major traumatic patient could be identified as patient with history of minor trauma or low - energy abdominal trauma . patients with hemoperitoneum at us examination but with unstable vital signs were immediately referred to surgery and therefore were excluded from the study , as already declared . patients with negative us findings were also excluded , were submitted to 24 h clinical observation and then discharged without further abdominal imaging . the remaining 73 patients , who had a history of minor trauma , hemodynamic stability and at least one positive finding at baseline us , such as abdominal free fluid , 1 3 radiol med ( 2015 ) 120 : 9891001 perirenal fluid collection , signs of hepatic , splenic , or renal injury , were subjected both to ceus and ce - mdct . written informed consent from parents was always obtained , including the information that the use of contrast medium that is used is not recommended for children . 
 ( c , d ) axial and coronal mdct images that confirm the ceus findings 1 3 992 radiol med ( 2015 ) 120 : 9891001 study was conducted to detect the presence of free intraperitoneal fluid in the perihepatic area , the morrison pouch , the epigastric region , the perisplenic region , the paracolic gutters , and the douglas pouch and the presence of perirenal fluid collection . 
intraabdominal organs were specifically evaluated for evidence of injury . ceus was performed immediately after baseline us . adequate ultrasound technology consisting of a contrast - specific software which operates in real - time at a low mechanical index ( pulse inversion technology ) was applied . 
an abdominal scanning of 3 consecutive minutes was performed for each bolus , starting from the right and left kidney , liver and pancreas ; last , the spleen . a traumatic lesion was identified as the presence of an hypoechoic area which persisted unchanged during all the acquisition phases , with a subcapsular distribution in the case of hematoma or a parenchymal localization in the case of lacerations . 
the presence of intralesional hyperechoic spots was interpreted as a sign of active bleeding . biphasic ce - mdct examination was performed using a mdct 16 scanner ( lightspeed 16ge healthcare , usa )  . 
2 splenic laceration in 9 - year - old child who beated the left flank against the school desk ( a ) longitudinal scanning at baseline us shows normal findings . 
baseline us did not detect any case of parenchymal active bleedings , vascular bleeding , and urinomas . on ceus examination , organ injuries appeared as strongly hypoechoic areas with or without interruption of the anatomic profile . 
a at baseline us is visible a mild hyperechoic area within the middle - third of the right kidney , without evidence of renal fracture ( white arrow )  . 
b ceus examination shows a linear renal fracture not < 1 cm parenchymal depth in renal cortex ( white arrow ) with associated perirenal hematoma ( arrowhead ) , ii grade renal injury , confirmed at mdct ( c ) 1 3 994 radiol med ( 2015 ) 120 : 9891001 fig . 
ceus identified all parenchymal lesions ( 100 % ) , 8 / 16 parenchymal active bleeding ( 50 % ) , 1 / 1 partial devascularization , 0 / 2 vascular bleeding , 0 / 2 urinomas . thus , in the evaluation of parenchymal lesions the diagnostic performance of ceus was much better than that of us , as sensitivity , specificity , ppv , npv , and accuracy in the evaluation of parenchymal lesions were , respectively , 100 , 100 , 100 , 100 , and 100 % for ceus and 38.8 , 100 , 100 , 12.8 , and 44 % for us ( table 5 )  . no adverse effects were observed for both ceus and ce - mdct . discussion ce - mdct is the most used and sensitive imaging modality in traumatic lesion assessment . 
it is able to depict both parenchymal and vascular lesions ( including active bleeding ) which are the major predictors of nonsurgical management [ 2123 ]  . baseline us has a low sensitivity in the detection of parenchymal lesions and , as hemoperitoneum is not always present in patients with solid organ injuries , it is 1 3 radiol med ( 2015 ) 120 : 9891001 fig . 
 [ 27 ] found that up to 31 % of ctproved intra - abdominal injuries do not have associated free fluid and that us has a very low sensitivity in directly demonstrating organ injuries , especially splenic lacerations , even with optimal condition of use . 
this consideration is disappointing , if we consider the fact that trauma to the splenic parenchyma can result in massive and unpredictable delayed bleeding [ 2831 ]  . regarding pediatric population , emery et al . 
 [ 32 ] found that 34 % of us negative examination children had an intra - abdominal injury at ct and so reached the conclusion that screening us for the depiction of blunt abdominal trauma should be approached with caution . in our population , we found that the presence of free intraperitoneal fluid is not always due to traumatic causes : in the 8.2 % of cases it was related to other different causesgynecological ( 50 % ) , gastroenteritis ( 33.3 % ) , miscellaneous ( 16.7 % ) and it should not be considered a reliable specific indirect sign of organ traumatic injuries . the introduction of us contrast agents has led to an increase in the diagnostic accuracy of us in many organs and many studies conducted to assess trauma in adults have showed that its sensitivity is almost the same as that of 1 3 996 radiol med ( 2015 ) 120 : 9891001 fig . 
b longitudinal and transverse c ceus images of the same patients in which it is evident a renal fracture with an associated perirenal collection ( arrowhead ) and evidence of hyperechoic spots within it ( white arrow ) that at a subsequent angiography examination showed to be an active bleeding from a segmental renal artery and not extravasation from the urinary syste d , e mdct urographic - phase : the perirenal collection showed to be a perirenal hematoma with evidence of active bleeding ( white arrow ) ; a clot is visible in the right urinary system ( black arrowhead ) ce - mdct [ 13 , 28 ]  . 
few studies exist on the use of ceus in childhood [ 33 ] , because the use of ultrasound contrast agents in children has not been officially approved since these contrast media are not licensed for pediatric use . 
b , c ceus shows a well - defined renal fracture and the presence of a perirenal collection that seems to be a perirenal hematoma ( white arrows )  . 
however , in these last cases , both us and ceus identified massive hemoperitoneum which represents an indirect sign of severe abdominal organ injury and put the clinical indication to perform a ct . another significant limitation is that ceus can not detect direct signs of peritoneal bleeding due to injuries of the intestine and mesentery . 
however , should be considered that these lesions , unlike those of solid organs that are the object of the present work , occur more frequently in highenergy trauma , rather than in the minor trauma . 
moreover , both baseline ultrasound and ceus are able to detect the presence of free fluid in the peritoneal cavity , thus placing the suspected diagnosis of a traumatic injury . conclusions in conclusion , our findings show that ceus in children is more sensitive and accurate than baseline us and almost as sensitive as ct in the identification and characterization of blunt abdominal trauma . 
9 9 - year - old boy , domestic accident ( a ) baseline us shows only a mild and irregular hyperechoic areas within the right hepatic lobe ( white arrows )  . 
b at ceus examination , the traumatic lesion appear as a strongly hypoechoic area ( white arrows ) that can be classified as a iv grade lesion according to the aast classification . 
twenty randomly selected patients suffering from pfs for a total of 40 knees were studied by static ct scans in order to assess patellar tilt , patellar displacement , patellar and trochlear morphology and inferior limb alignment . 
all known parameters were measured ; the variability of the measurements between observers was evaluated by boxplots , pearsons correlation coefficients , and infraclass correlation coefficient [ icc ( 2 , 1 ) ] based on a two - way random effect model . 
patellar tilt parameters appeared equally reliable ; patellar displacement is best measured with botot that showed an icc of 0.889 ; morphology is best measured with wibergtot , with an icc of 0.862 ; lastly , for the inferior limb alignment parameters analysis , ftv outperformed the others in terms of reliability . 
the present study allowed us to select a limited number of reliable parameters * luca dei giudici lucadeigiudici@gmail.com 1 clinical orthopaedics , department of clinical and molecular science , school of medicine , universit politecnica delle marche , via tronto , 10 / a , 60126 ancona , italy 2 department of radiology , universit politecnica delle marche , azienda ospedaliero - universitaria ospedali riuniti , ancona , italy 3 department of methods and models for economy , territory and finance , sapienza universit di roma , rome , italy in the evaluation of patello - femoral and inferior limb alignment . 
the use of these parameters may also result in a more reliable comparison of studies on pfm and in a better evaluation of the treatment outcomes . keywords patello - femoral joint patello - femoral malalignment reliability ct scans limb alignment introduction patello - femoral malalignment ( pfm ) is a pathological condition that determines an abnormal patellar tracking , which is defined as the patellar movement in relation to the trochlear groove during flexionextension movements [ 1 ]  . 
patello - femoral malalignment can cause an aberrant dispersion of the joint reaction force ; it can predispose to joint line reduction and is associated with oa progression and pain increase [ 2 ]  . the diagnosis of patello - femoral malalignment is based on clinical data and several instrumental examinations . 
ct and mri make it possible to obtain , without distortion , images of axial sections of the patella with the knee in the first 30 of flexion and with the femoral condyles as a reference plane [ 3 ]  . 
ct , moreover , permits to study the patello - femoral joint even with the quadriceps contracted , so that the dynamic effects of the quadriceps muscle are taken into account . 
with these methods , in the instability range of movement , trochlea and patella are in the same section , and there is better sensibility and specificity [ 5 ] ; also , since patellar displacement and tilting is strictly 1 3 1032 radiol med ( 2015 ) 120 : 10311042 connected to the quadriceps vector , the possibility to obtain scans with muscular contraction can unveil some pfms that would appear normal with conventional imaging [ 5 ]  . various authors have identified [ 610 ] several parameters for the assessment of the patello - femoral and inferior limb alignment in normal subjects and in patients with pfs . 
these parameters allow us to evaluate several aspects which may be associated with pfs : patellar and trochlear morphology , patellar displacement , patellar tilt [ 9 ] , femorotibial valgism , femoral neck anteversion , tibial tuberositytrochlear groove distance ( tttg ) and tibial torsion [ 11 ]  . 
moreover , in the literature , there are no studies comparing each and every measurement in its specific field , therefore leaving the surgeon with a handful of validated measurements for each aspect of patello - femoral imaging with an unclear idea as to which one of them is better than the other and which one is to be preferred , if possible , while analysing a specific aspect of a patellofemoral alignment . 
the selection of reliable parameters is , therefore , of utmost priority in order to compare different case series and to assess clinical outcomes [ 11 ]  . thus , the aim of the present study was to identify the most useful and reliable parameters for measuring patellofemoral and inferior limb alignment by ct . materials and methods since march 2002 , the radiological protocol of our institution for diagnosis and management of a pfs requires x - rays in 3 projections ( anteriorposterior , lateral and axial view ) and static and dynamic ct scans of the bilateral patello - femoral joint . 
out of 511 confirmed cases in our database , 20 patients were randomly selected using the ms excel random formula . exclusion criteria were the history of recurring patellar dislocation , post - traumatic anterior knee pain , meniscal and ligamentous injuries , previous knee surgery , apophysitis , osteochondrosis and rheumatic diseases ; excluded cases were replaced with other randomly selected cases . 
males were also excluded from the study in consideration of the epidemiology of this particular pathology , mostly present in females patients , in an attempt to limit an eventual confounding factor . 
the study group consisted of 20 females aged between 20 and 33 years ( mean age 25.35 years old ) for a total of 40 analysed knees . ct examination was performed with the patient in supine position at 15 of knee flexion , obtained with hard support and fixed with strips [ 12 ]  . 
on the static acquisitions , five slices were traced , one on the maximum transversal patellar axis , the others 5 and 10 mm above and under this line , respectively ; each acquisition was performed by the same ct specific technician . 
measurement parameters were distinguished in four different groups : ( 1 ) patellar tilt , ( 2 ) patellar displacement , ( 3 ) patellar and trochlear morphology , and ( 4 ) inferior limb alignment , and calculated for each of the 40 knees . patellar tilt was assessed according to : lateral patellar angle ( lpa ) and lateral patellar tilt ( lpt ) [ 13 ] , both referred to trochlear groove ( lpat , lptt ) and to the condyles ( lpac , lptc )  . patellar displacement was assessed according to congruence angle ( ca ) [ 9 ] , lateral patellar displacement referred to trochlear groove ( lpdt ) and to the condyles ( lpdc ) [ 8 ] , and patellar displacement ( pd ) [ 14 ]  . 
bisect offset ( bo ) , divided into total portion ( botot ) and only lateral portion ( bolat ) , and condylar patellar angle ( cpa ) were measured , as described in the original paper [ 5 ] , but they were not shown in figures . patellar and trochlear morphology patellar morphology was assessed according to wibergs criteria [ 15 ] and measuring both total length and lateral only portion ( wibergtot , wiberglat )  . 
trochlear morphology was assessed by sulcus angle ( sa ) [ 16 ] , trochlear axis variation ( tav ) and condylar axis variation ( cav )  . inferior limb alignment was assessed measuring femoraltibial valgism ( ftv ) , femoral neck anteversion ( fa ) , tibial tuberositytrochlear groove distance ( tttg ) , and tibial torsion ( tt ) , as they are the most used parameters in the literature . the schematic description of each measurement is provided in figs . 
all measurements were performed independently by four specialists , three orthopaedic surgeons and one radiologist , using the same software ( centricity web v3.0 , ge medical systems information technologies )  . statistical analysis was performed by a professional analyst . 
sa angle between the lines passing by the deepest trochlear point and the anterior knee condyles , tav the difference in the angle formed between the line passing by the anterior condyles and the horizontal line , calculated at the mid - patellar section and the same angle calculated at the roman arch section , cav the difference between the angle formed between the line passing by the posterior condyles and the horizontal line , calculated at the midpatellar section , and the same angle calculated at the roman arch section , wiberg length of patellar major axis ( total ) and the portion lateral to the sagittal axis passing by the articular apex ( lat ) , ftv angle between the femoral and tibial major axis , fa angle between the line passing by the posterior condyles and the line passing by the centre of the femoral head and neck , tt angle between the line tangent to the posterior tibial surface and the line passing by the centre of the malleoli 1 3 radiol med ( 2015 ) 120 : 10311042 1035 boxplots . 
for each analysed parameter and for each technique , pearsons correlation coefficients between the observers were computed : the larger the correlations , the more reliable the techniques . the interobserver reliability was formally evaluated using an infraclass correlation coefficient [ icc ( 2 , 1 ) ] based on a two - way random effect model ( observers and subjects are treated as random effects )  . 
blandaltman mean differences and 95 % limits of agreement were computed for each pair of measurements . results patellar tilt all four techniques can be considered reliable tools for measuring patellar tilt . 
this was confirmed by the correlation coefficients that were computed for each couple of observers : all measurements were strongly correlated , but the measurements done by observer 1 with lptt technique showed correlation coefficients lower than 0.75. 
this was confirmed by the correlation coefficients that have been computed for a couple of observers : lpdt , bolat , botot and cpangle showed strong correlation between the observers . 
on the other hand , correlation coefficients were lower for the other methods ranging from 0.502 ( lpdc , correlation between observer 1 and 2 ) to 0.881 ( ca , correlation between observer 1 and 4 )  . 
it should however be noticed that the confidence intervals corresponding to the ca method were very large , highlighting the fact that ca was less reliable than the other methods . patellar and trochlear morphology wiberlat and wibergtot were very reliable methods : wibergtot can be considered to be the most reliable one . all measurement methods showed large variability , with the exception of wiberglat and wibergtot whose boxes fig . 
note the lines drawn to evaluate lpdt 1 3 1036 radiol med ( 2015 ) 120 : 10311042 no significant fixed observer bias was detected for all methods since the null value was covered in all confidence intervals of the blandaltman statistics . boxplots for each observer and each measurement are provided as graphical results in fig . 
6. detailed statistics is provided in tables 1 , 2ab . discussion the present study showed that some of the measurements commonly used to evaluate patello - femoral alignment are not reliable . patellar tilt was best measured by lpa , but all methods are reliable . 
on the other hand , lpd had higher sensibility with an agreement of about 89 % [ 14 ] ; it is sufficient to consider , as reference points , the patellar apex and the deepest point of trochlea in order to maintain this measurement independent of the anatomical variation [ 20 ]  . 
 [ 22 ] obtained 92.7 % of sensibility when they considered lpt > 11 as pathological in patients suffering from patellar instability . patellar and trochlear morphology was best measured by wibergtot and wiberglat , the portion of the major patellar axis included between the lateral border and the point representing the intersection between the major axis and the perpendicular line passing by the deepest point of the interfacet crest . 
in contrast with the literature , the present study showed low reliability of sa , actually considered a fast , easy , very reproducible and reliable measurement [ 23 ]  . 
this result could be explained considering that , in the other studies , sa was measured on merchants x - ray view that provides a standardized image but not always properly showing trochlear morphology ; when this measurement is applied to a ct scan , it needs , instead , to first select the ct section showing the deepest point of the trochlear groove , and then to evaluate sa . in the assessment of inferior limb alignment , ftv and to a lesser extent tttg were the most reliable measurements , while fa turned out to be the least reproducible . 
the substantial disagreement of the measurements between the observers was confirmed by the correlation coefficients : sa , tav and cav measurements were very weakly correlated between the observers , and in some cases , the correlation was negative . 
on the other hand , measurements done with wiberglat and wibergtot were correlated between the observers , and for wibergtot , the correlation indices denoted a strong correlation ; sa , cav and tav presented very low icc indices while wiberglat and wibergtot confirmed to be more reliable tools . no significant fixed observer bias was detected for all methods since the null value was covered in all confidence intervals of the blandaltman statistics . 
correlation coefficients obtained with the other methods were very variable , ranging from 0.294 ( tt , observer 2 and 3 ) to 0.955 ( tt , observer 1 and 3 )  . 
means and variances have also been reported : a patellar tilt ; b patellar displacement ; c patellar and trochlear morphology ( notice that sa measurements are divided by 10 for visualizing them in the same graph of the other techniques ) ; d inferior limb alignment measured in approaching a patient with patello - femoral problems , and it is only estimated by inspection or , as an alternative , by measuring the q angle [ 24 ]  . 
unfortunately , there are some concerns about the q angle ; it is considered pathological when not normal or generally increased , but it is influenced by many factors like extension , flexion , quadriceps contraction , gender and the patients position during the exam [ 24 ]  . 
since ftv and tttg were found to be reproducible measurements in evaluating the relationship between inferior limb alignment and patello - femoral joint , authors of this paper suggest using these ct measurements rather than q angle in the evaluation of patients affected with patello - femoral problems , in line with the findings of other recent papers [ 26 ]  . fa is commonly considered a very relevant parameter in the evaluation of inferior limb alignment and hip morphology and should therefore be always part of pre - op planning 1 3 radiol med ( 2015 ) 120 : 10311042 1039 1 3 1040 radiol med ( 2015 ) 120 : 10311042 1 3 radiol med ( 2015 ) 120 : 10311042 1041 [ 11 , 27 ]  . 
unfortunately , several confounding factors play a role in its measurement , such as the patients positioning , technicians skills and medical interpretation [ 27 ] ; nonetheless , different and difficult calculations are needed to estimate the proper axis of the femoral neck on which to assess the anteversion [ 28 ]  . 
thus , new methods , like 3d reconstruction , should be developed to increase the reproducibility of fa measurement in order to be considered as a valid preand post - op tool [ 31 ]  . this paper could attract some criticism since the main limitations are the small study group and the presence of possible confounding factors such as the patients positioning , technicians skills and probably medical interpretation . 
 it is possible to say , although , that the patients included in this study are very representative of the generic population as they are all females in the same age group , with a patello - femoral - derived form of anterior knee pain , thus representing a proper ground on which to test those parameters . 
patients positioning was also standardized via hard supports and fixed strips [ 12 ] , and eventual acquisition biases were limited to a minimum by the several - yearslong experience of the technician that performed the ct scans . 
in fact , the goal of this paper is representative of reality . the main strength of this study is the inclusion of every known parameter described in the literature for the specific aspects of the patello - femoral imaging selected and their evaluation by different observers in order to attempt to understand which one is better than another . 
 [ 18 ] published in the early 2000 . in conclusion , the present study allowed us to select a limited number of reliable parameters to evaluate patellofemoral and inferior limb alignment . 
 radiation absorbance is not a matter of concern as it has been demonstrated that the effective dose for a static and dynamic ct scan is less than 1 % of the maximum dose absorbable in 1 year by a radiological technician [ 31 ]  . 
safety and accuracy was correlated with patient - related and lesion - related factors . results 61 biopsies were performed under us - guidance , 750 under ct - guidance , and 13 under combined guidance . 
us - guidance , absence of perilesional * marco busso busso.marco@gmail.com 1 radiology unit , department of oncology , university of torino , regione gonzole 10 , 10043 orbassano , to , italy 2 pathology unit , department of oncology , university of torino , regione gonzole 10 , 10043 orbassano , to , italy 3 pulmonary oncology unit , department of oncology , university of torino , regione gonzole 10 , 10043 orbassano , to , italy 4 thoracic surgery unit , university of torino , regione gonzole 10 , 10043 orbassano , to , italy emphysema and minor depth of the target lesion from the skin resulted as favorable predictors against major complications . 
in the targeted therapy era , cb with larger needles can be safely applied when the need for larger amounts of tumor tissue is presumed . image - guided lung biopsy keywords lung tumor lung biopsy core biopsy image - guided biopsy targeted therapy introduction lung cancer leads cancer - related mortality in the world [ 1 , 2 ]  . percutaneous transthoracic needle biopsies have gained wide acceptance for diagnosing malignant and benign lung lesions . 
in fact , with the development of fine needle aspiration biopsy ( fnab ) and core biopsy ( cb ) , these procedures have reached a large range of use , becoming some feasible alternatives for other diagnostic procedures . during the last decade , research in lung cancer has yielded important advances in the development of targeted therapies that target driver oncogenes [ 3 ]  . 
the most prevalent mutated or rearranged oncogenes identified in non - small cell lung cancers ( nsclcs ) are v - ki - ras2 kirsten rat sarcoma viral oncogene homolog ( kras ) , epidermal growth factor receptor ( egfr ) , anaplastic lymphoma kinase ( alk ) , ros1 , braf , erbb2 and ret 1 3 radiol med ( 2015 ) 120 : 10241030 1025 [ 4 ]  . 
ttnb can safely and efficiently provide an accurate cytological or histological diagnosis [ 5 ] , and should become a standard tool in the routine diagnostic workup of lung lesions . our aim is to identify procedure related risk factors for the adverse events and determine the diagnostic yield and predictors of image - guided thoracic biopsies in a retrospective review of 811 subjects at a single institution . coagulation status was corrected when appropriate , according to specific guidelines [ 6 ]  . the ct - guided procedures were performed with the patient in a prone , supine , or lateral decubitus position , depending on the location of the lesion , and according to the best track for the biopsy . 
this retrospective study has been approved by our ethics committee on the basis of the written informed consent obtained from all the patients . the records of a consecutive series of 811 patients who underwent 824 usor ct - guided biopsies of a pulmonary lesion at our hospital were retrospectively reviewed . 
all biopsies were performed between july 2009 and october 2013 . the study population included 546 male ( 67.3 % ) and 265 female patients , with an age ranging from 30 to 87 years ( average 68 years )  . the lesion side ( right or left lung ) and diameter ( range and average ) were recorded . as possible predictors of safety and accuracy of the image - guided biopsy , we also considered the operators ( radiologist and pathologist ) , the depth of the target lesion from the skin ( intended as the shortest and safest needle pathway to the target ) and the presence of perilesional emphysema . procedure prior to each procedure , indication , risks and benefits of biopsy were discussed by a multidisciplinary tumor board . the referring physician or surgeon always gave the indication to biopsy , while the interventional radiologist evaluated its technical feasibility . 
2 in case of a wide pleural contact of the lesion , biopsy can be easily monitored by real - time us - guidance 1 3 1026 radiol med ( 2015 ) 120 : 10241030 fig . 
these categories should be described further : in our series , malignant diagnoses were those of primitive tumors , metastases , lymphoma or other malignancies ; negative diagnoses were infectious or inflammatory diseases , benign neoplastic lesions or other non neoplastic findings , including not cytologically diagnostic samples . 
according to this classification , no samples were considered inadequate , but only negative for the search of malignant neoplastic cells . the truthfulness of the pathologic reports on biopsy specimens was divided into assessable and non - assessable , according to the possibility of having a definitive diagnosis or not , due to patients lost at follow - up or the lack of a gold standard diagnosis ( e.g. , patients submitted to ablative therapies )  . 
the accuracy of biopsy in terms of sensitivity , specificity ; ppv , npv for malignancy and statistical analysis of predictors , was differently evaluated according to the therapeutic iter . 
in detail , for patients who underwent surgery , it was evaluated on histology ; whereas for patients treated with medical therapy , it was assessed in terms of clinical response and / or radiological outcome at imaging follow - up . in particular , a biopsy result was considered true positive for malignancy based on surgical confirmation , evidence of local or metastatic progressive cancer , or in case of regressive lesion during an oncological treatment . 
 in case of comparison of means ( patient age , size and depth of the lesions , number of samples ) , the unpaired t test was used to assess significance . 
in the 2011 nhs guidelines [ 8 ] , it is stated that ctor us - guided transthoracic needle biopsy have to be offered to patients with peripheral lung lesions when treatment can be planned on the basis of this test . the success of a biopsy can be measured in terms of high diagnostic accuracy and a low rate of complications . 
 many authors estimate an improvement of success rates of image - guided lung biopsy associated with a decrease in complications in centers with high level of experience [ 9 ]  . the most common complications after percutaneous biopsy of the chest are pneumothorax and pulmonary haemorrhage . 
the overall frequency of pneumothorax in our study ( 195 / 824 , 23.6 % ) is widely within the range reported in previous studies [ 9 , 10 ]  . 
this could depend on the management of drained pneumothorax in our center , where surgeons do not discharge these patients before the third day of hospitalization due to the peripheral location of our hospital . 
in addition , our results were also favorable for bleeding as a major complication ( suggested qi threshold 2 , 0.5 % in our series )  . previous studies have reported that many factors could influence the complication rate of image - guided thoracic biopsies . 
 these findings are similar to others by previous authors , which described a significant association between the traversed lung length , lesion size and lesion depth with the rate of pneumothorax and bleeding [ 1013 ]  . in the last few years , the advent of new molecularly targeted agents for specific cancer subtypes has partially changed the role of cb in the diagnosis of lung cancer . 
 the identification of activating mutations of the epidermal 1 3 radiol med ( 2015 ) 120 : 10241030 1029 growth factor receptor ( egfr ) in nsclc and rearrangement of anaplastic lymphoma kinase ( alk ) in lung adenocarcinoma , are important parts of the recent discoveries in the field of lung cancer treatment [ 14 ]  . 
for the management of lung cancer , a crucial issue is the availability of adequate and sufficient tumor tissue not only for pathological diagnosis , but also to allow additional immunohistochemical and molecular studies [ 15 ]  . 
to meet the challenges of histopathological and molecular analysis , the size of biopsy needle used to obtain adequate sample for mutation analysis have become an important considerable factor for the biopsy procedure . 
ct - guided cb allows acquisition of material for predictive analysis using either 18 - gauge or 20 - gauge tru - cut biopsy needles via 17 - gauge or 19 - gauge coaxial needles [ 16 ]  . 
 [ 16 ] , even though the evidence is still insufficient to determine whether fnab , cb , or some combination thereof should be the standard of care for diagnosing lung malignancies in patients with a lung lesion , no available evidence suggests that , compared with fnab , cb leads to a higher rate of pneumothorax or hemoptysis . 
also in our experience cb versus fnab and a larger needle size did not result in a significant difference in occurrence of adverse events . the overall sensitivity , specificity and diagnostic accuracy of image - guided biopsy in our study are 96.5 , 100 and 97 % . 
in fact , previous studies have already shown that on site evaluation of fna specimens can improve the diagnostic ability of ct - guided lung biopsies [ 10 , 19 ] : in our practice , the decision to switch from a fnab to a cb ( particularly useful in confirming the suspicion of a benign lesion [ 16 ] ) and , more generally , to carry out further sampling , is very often based on the extemporaneous judgment of the pathologist . in our study variables related to the patient or linked to imaging or technical differences , were not associated with a false negative result . 
however , a tendency was found for the association with chronic inflammation and fibrosis within and around the larger lesions ( mean size of nondiagnostic biopsies about 7 mm larger than the diagnostic biopsies )  . 
this was similar to another study , in which factors associated with false negative results included increased size of lesion , fewer adjustments of the needle , lack of positive cultures , and the occurrence of a pneumothorax [ 20 ]  . in conclusion , our study confirms that image - guided lung biopsy has low complication rates and high accuracy for diagnosing thoracic lesions . 
large , solitary or massive - growing nodules with lobulated or irregular contour , capsule - like enhancement , heterogeneous signals or lower adc values supported the diagnosis of phnen compared with mhnen . 
primary hepatic neuroendocrine neoplasm ( phnen ) is a rare tumor type originating in the liver , with no more than 200 cases having been reported in the english - language literature [ 27 ] , accounting for 15 % of all liver neoplasms , and 0.84.0 % of systemic neuroendocrine tumors [ 5 , 6 ] ; these tumors usually have a rather benign course and a relatively good prognosis [ 2 , 8 ]  . 
nevertheless , liver is a common site for nen metastases , especially gastroenteropancreatic nens , as the portal vein drains directly into the liver [ 9 ] ; and metastatic hepatic neuroendocrine neoplasm ( mhnen ) may be the first manifestation in up to 4090 % of cases [ 10 ]  . 
differentiation between primary and secondary hepatic nens is impossible by histology alone [ 3 ] ; imaging examination , 1 3 radiol med ( 2015 ) 120 : 10121020 1013 especially magnetic resonance imaging ( mri ) which is of better soft tissue contrast , may improve preliminary differential diagnosis . 
to date , a few studies have analyzed the mr features of primary or secondary nen in the liver [ 57 , 10 , 1215 ] , but their comparison has not yet been explored . 
as accurate characterization of them can improve diagnostic accuracy as well as provide guidance for clinical treatment and information for long - term prognosis , this study would be the first to compare the two groups and determine which mr features were the best predictors in differentiation . materials and methods patients this retrospective study was approved by the institutional review board and informed consent was waived . 
 more than half of the patients were symptomless ( n 21 ) at the time of initial medical evaluation , and the most common complain was abdominal discomfort ( n 16 ) , none of the patients had clinical signs of endocrine hyperactivity . 
diffusion - weighted imaging ( dwi ) matrix , 180 was required with a transverse single - shot spin - echo echo2400 / 66 ms ; section thickplanar sequence ( tr / te ness , 5 mm ; intersection gap , 1 mm ; matrix , 168 320 ) with two b values ( 0 and 500 s / mm2 )  . 
 gadopentetate dimeglumine was administered at a dose of 0.1 mmol / kg at a rate of 2 ml / s , followed by a 20 ml saline flush using a power injector ( spectris ; medrad , pittsburgh , pa )  . 
the field of view was optimized to the patients body habitus at 285 214308 380 mm . image analysis all images were evaluated using a picture archiving and communication system ( pacs ; pathspeed , ge medical systems integrated imaging solutions , prospect , il , usa )  . 
the reviewers knew that the patients had liver tumors but were unaware of all other information regarding patients history , laboratory , and final pathological results . qualitative analysis for the morphological features , the observers measured the tumor size , number ( single / multiple ) , distribution ( massive / diffuse ) , contour ( round / lobulated or irregular ) , as well as the presence of necrosis or cystic degeneration , 1 3 1014 radiol med ( 2015 ) 120 : 10121020 hemorrhage , hepatic capsule retraction / bulging , fluidfluid levels ( ffl ) , vascular invasion , cancer embolus and positive lymph nodes ( minimum diameter 10 mm or central necrosis )  . 
the massive type was defined as a dominant tumor with or without surrounding small tumors in the liver , while the diffuse type was defined as multiple tumors of similar size scattered diffusely in the liver . 
tumor contour was determined by the dominant category in cases of multiple tumors . for the signal features , lesion homogeneity was defined as homogenous or heterogeneous on t2 - weighted imaging . 
signals on each different phase after contrast administration were registered as ( a ) globally hyperintense ; ( b ) partially hyperintense ; ( c ) circularly hyperintense ( d ) isointense ; ( e ) hypointense . 
dynamic enhancement patterns were defined as ( a ) progressive : the range or intensity of enhancement progressed over time , including centripetal enhancement ; ( b ) persistent : the enhancement remained invariable through all three phases ; ( c ) degressive ( wash - in without wash - out ) : decreasing hyperintensity over time without hypointense appearance on portal or delayed phases ; ( d ) wash - in with wash - out : contrast uptake during arterial phase followed by contrast wash - out which showed relative hypointensity on portal or delayed phases . 
 for multiple tumors , the dominant characteristics were evaluated . quantitative analysis signal intensity ( si ) of the tumor , liver parenchyma and standard deviation ( sd ) of the background noise during dynamic - enhanced imaging were recorded using a region of interest ( roi )  . 
in roi placement of the lesion , the enhanced portion within the tumor as large as possible was chosen , and the roi of the liver parenchyma was set in the same slice where the roi of the lesion was set , great care was taken to avoid large vessels , necrosis , hemorrhage and artifacts . 
two measurements were taken for each roi by one radiologist ( r.f.s ) , and the average was used for analysis . pathological analysis all pathologic specimens with hematoxylineosin and immunohistochemical staining were reviewed by a pathologist ( y.h.x. , with 6 years of experience in liver pathology ) according to the revised who classification . 
the who classification 2010 divides nens into well - differentiated endocrine tumors with benign or uncertain behavior ( g1 ) ; well - differentiated endocrine tumors with low grade malignant behavior ( g2 ) ; and poorly differentiated endocrine carcinomas with high - grade malignant behavior ( g3 ) [ 2 ]  . statistical analysis patients were divided into the phnen and the mhnen group . 
 the accuracy of the adc values for the diagnosis and differential diagnosis of phnens and mhnens was evaluated by calculating sensitivity , specificity , positive predictive value , negative predictive value , and receiver operating characteristic ( roc ) curve . 
the agreement was rated on the following scale : 00.20 , slight agreement ; 0.210.40 , fair agreement ; 0.410.60 , moderate agreement ; 0.610.80 , substantial agreement ; and 0.81 or greater , excellent agreement [ 16 ]  . 
as was displayed by our results , there was a wide range of age at presentation for nens , without definite gender specificity or any association with particular tumor markers , and most patients are symptomless with no carcinoid syndrome presenting , which also coincided with previous researches [ 2 , 17 ]  . 
clinical features may not be sufficient in correct diagnosis and differentiation due to the overlaps ; thus , the mr examination which provides satisfied soft tissue contrast is necessary and plays a crucial role in the diagnosis and differential diagnosis of phnens and mhnens . in our study , morphological and signal features including the tumor size , number , distribution , contour , lesion homogeneity and the presence of capsule - like enhancement were valuable predictors for differentiation . 
the heterogeneity of phnens may be associated with the relatively larger size of these primary tumors , as infarction and liquefactive necrosis are more frequent when tumors grow larger ; while in contrary , necrosis is rarely presented in mhnens owing to their high vascularity and relatively small size [ 1 ]  . 
capsule - like enhancement is defined as a thin rimlike enhancement along the periphery of the tumor during the portal or delayed phases and is histopathologically correlated with fibrous capsules . 
 four patients in our cases showed intra - lesion ffls , and they were all in the metastasis group , which can also be regarded as an indicator of mhnen . 
 [ 10 ] , in which 19 / 69 patients with mhnen showed ffls . hepatic nens are typically hypervascular after contrast agent administration , with their blood supply from the hepatic artery [ 10 , 12 , 1820 ]  . 
b transverse t1 - weighted vibe images show relative hypointensity with enhanced separated shadow in the center of the lesion on arterial phase ( asterisk ) and c , d a progressive enhancement pattern with sustained enhanced separated shadow ( asterisk ) and capsule - like enhancement during portal and delayed phases ( arrow head )  . 
researches revealed that hypovascularization was associated with early tumor progression and a decrease in overall survival , thus , an early and active treatment was necessary for these patients [ 19 , 23 ]  . 
 moreover , a spectrum of contrast - enhanced behaviors including progressive , persistent , degressive and wash - out pattern were exhibited ; the various enhancement patterns 1 3 radiol med ( 2015 ) 120 : 10121020 1017 1 3 1018 radiol med ( 2015 ) 120 : 10121020 fig . 
c transverse t1 - weighted vibe images show global hyperintensity in most tumors on arterial phase , and d , e a dominant degressive pattern with global isointensity during portal and delayed phases . 
all nens appeared as marked hyperintensity on dwi and low adc values compared with surrounding liver parenchyma , this can be explained by the small round cells with high nucleicytoplasm ratio , and stromal fibrosis at histologic examination , which could lead to reduced diffusion ability of intraand extracellular water molecule [ 7 , 25 ]  . 
in our study , phnens presented lower adc values compared to mhnens , and when the cutoff 3 mm2 / s was used , satisfied specitivity value of 1.049 and excellent positive predictive value could be achieved , indicating that dwi and adc values are of great help in accurate discrimination . 
while at the same time , adc values are of relatively low reproducibility , and there are substantial overlaps in the range of adcs between phnens and mhnens [ 25 ] , they should be interpreted concurrently with other mr sequences to make an exact radiologic diagnosis . 10 the major limitations of our study are the relatively small study population and the retrospective nature , thus selection bias may exist , and further point - to - point radiologicpathologic correlation study would be necessary . 
 the aims of the current study were to investigate diffusion changes in the crus cerebri in patients with striatocapsular infarction using diffusion tensor imaging ( dti ) , and analyze the relationship between such changes and upper extremity motor dysfunction . materials and methods fifteen patients with acute onset of striatocapsular infarction and unilateral upper extremity motor dysfunction for the first time were studied prospectively . 
the secondary changes in the ipsilateral region distal to this kind of infarction and the relationship between these changes and the corresponding neuromotor dysfunction have been studied by a number of researchers . 
diffusion tensor imaging ( dti ) has become the neuroimaging detection method commonly used in such studies due to its specific advantages in the evaluation of white matter fibers [ 57 ]  . 
the vectorial or preferential motion of water molecules is measured with this magnetic resonance imaging ( mri ) technique and information can be obtained with regard to the integrity of cells and pathology [ 9 ]  . 
also , the occurrence of chemical degradation of the myelin sheath can be observed in white matter fibers [ 7 , 10 ]  . a number of studies that included measurement of fractional anisotropy ( fa ) , which is used to measure the direction of water molecule motion , a reflection of the consistency and integrity of cell and tissue structure arrangement , with a high value indicating a strong regularity of anisotropy of the tissue structure arrangement , have found that there is a correlation between ipsilateral fractional anisotropy ( fa ) values and motor function outcome in patients with cerebral ischemic stroke [ 11 ]  . 
in a study in which 15 chronic stroke patients were compared with age - matched healthy controls it was found that measures derived from dti , fa , and directional diffusivity , were useful for predicting the functional motor recovery potential [ 12 ]  . 
investigation of the relationship between dti indicators and the degree of contralateral upper extremity motor impairment can provide a reference for evaluating the prognosis of ipsilateral motor function and developing a rehabilitation program . though there have been many studies that have evaluated the secondary changes in the pyramidal tract after cerebral infarction using dti , some specific types of deep brain infarcts including striatocapsular infarcts , which are subcortical infarcts that are located in the area supplied by the lenticulostriatal arteries , have been rarely studied [ 13 , 14 ]  . 
the aims of this study were to investigate the diffusion changes in the affected crus cerebri of patients with isolated striatocapsular infarction ( lesions involving the striatum and internal capsule simultaneously , i.e. , caudate nucleus plus the internal capsule , or putamen plus the internal capsule ) and to qualitatively analyze the relationship between these changes and the motor function in the affected upper extremity . data and methods general data this prospective study was approved in advance by the hospitals ethics committee and patient consent was obtained after patients were informed about the whole research process . 
the clinical data were collected by neurosurgeons . inclusion criteria were the following : ( 1 ) acute onset of striatocapsular infarction and unilateral upper extremity motor dysfunction for the first time ( the time interval from symptom onset to the hospital visit should be less than 24 h ) ; ( 2 ) met the diagnostic standard of brain infarction recommended by the fourth national conference on cerebrovascular disease [ 15 ] ; ( 3 ) unilateral upper extremity motor dysfunction ; ( 4 ) brain mri checked within 1 week after disease onset , and the images suggested unilateral striatocapsular infarction with a maximum length more than 2 cm and no involvement of other areas of the cerebral cortex ; ( 5 ) no depression , anxiety , or mental and behavioral disorders according to the evaluation performed using the neuropsychiatric inventory and hospital anxiety - depression scale ; ( 6 ) right - handed . exclusion criteria were the following : ( 1 ) non - ischemic stroke ( cerebral hemorrhage and subarachnoid hemorrhage ) ; ( 2 ) symptoms more than 24 h at admission ; ( 3 ) abnormal signals outside the unilateral internal capsule of the striatum on conventional mri ; ( 4 ) a medical history of important central nervous system disorders , such as encephalitis , cerebral spinal tumors , brain trauma , etc . ; ( 5 ) serious internal diseases or surgical diseases or diseases affecting extremity function ; ( 6 ) contraindications to mri examination including pacemaker implantation , prosthetic valve surgery , in vivo ferromagnetic foreign bodies , claustrophobia , etc . 
the enrolled patients underwent medication with statins ( 10 mg rosuvastatin , once per night ) and anti - thrombotic drugs ( 0.1 g aspirin , once per night ) within 2 weeks after disease onset . clinical features the fugl - meyer assessment of motor recovery was used during the current study [ 1618 ]  . 
the data were analyzed using the volume one l.64 and diffusion tensor visualizer ii ( dtv ii ) software system [ 1921 ] to obtain images of fractional anistropy ( fa ) and mean diffusivity ( md ) , an indicator used to measure the mean amplitude of water molecule diffusion which mainly reflects the size and integrity of cells in the tissue ; a high md value indicates a great amount of free water content . 
ai was calculated as follows : ai = |fa as faus| / [ ( faas + faus ) / 2 ] 100 faas is the fa value of the affected side and faus is the fa value of the unaffected side . the dti data were collected in a double - blind manner by two radiologists . 
the results also showed that the ai was high when the fuglmeyer assessment score was low ( which represents severe motor dysfunction of the affected upper extremity ) , and that the ai was low when the fugl - meyer assessment score was high ( which represents mild motor dysfunction of the affected upper extremity ) , and that there was a significant fig . 
2 lesion of striatocapsular infarction on the left side of the basal ganglia at the acute stage involving the head of the caudate nucleus , putamen , and posterior limb of the internal capsule . 
left ( a ) : fa image is from the same side as the striatocapsular infarction ; the white arrow shows that the signal in the crus cerebri on the ipsilateral side was weaker than on the contralateral healthy side . 
previous functional neuroimaging studies showed that wallerian degeneration of the pyramidal tract in patients with cerebral infarctions and impaired motor pathways is the most commonly seen secondary lesion [ 7 ]  . diffusion tensor imaging has relatively significant advantages for detecting the secondary injury of these fiber bundles . 
causes of the injuries generally include ischemic cerebral infarction , cerebral hemorrhage , demyelinating disease , arteriovenous malformations , tumors , etc . , with ischemic cerebral infarction being the most common . 
 therefore , changes of anisotropy in the diffusion in the crus cerebri may be related to the typical wallerian degeneration of the pyramidal tract . previous studies of the mouse model showed that cytoskeleton disintegration of the axons distal to the ischemic lesion occurred within 30 min after stroke , axon degeneration could be observed 27 days after stroke in the brain stem , and chemical degradation of myelin and astrocyte proliferation occurred 2 weeks later [ 22 ]  . 
sensitivity of the conventional mri sequence in this kind of early degeneration is low and these microscopic pathological changes could not be detected easily , and the severity of damage could not be quantified [ 23 ]  . 
 [ 7 ] carried out dti scanning for 9 patients with acute supratentorial cerebral infarction 216 days after disease onset , and observed diffusion change of the pyramidal tract in the ipsilateral crus cerebri within 2 weeks after 1 3 radiol med ( 2015 ) 120 : 10641070 1069 the onset of infarction , and the fa value of the affected pyramidal tract was reduced by 13 % compared to that of the unaffected side , whereas no abnormality was found on the conventional mri scan . 
 [ 11 ] carried out dti of the cerebral peduncle 321 days after stroke onset and found that the fa values were significantly decreased on the ipsilateral side compared with the contralateral side . 
our findings , which showed that the fa value of the affected crus cerebri was significantly lower than that of the unaffected crus cerebri 2 weeks after disease onset in patients with striatocapsular infarction and consequent upper extremity motor dysfunction , are consistent with the findings of these previous reports . 
the reduced fa value in the affected crus cerebri suggests damaged integrity of the fibrous structures including the pyramidal tract in the region of interest , which fits the pathological basis of axon membrane disintegration and myelin sheath dissolution during wallerian degeneration . 
another factor that can cause the reduced fa value on the affected side is the change of local anisotropic structures due to the glial cell proliferation in the affected area [ 28 , 29 ]  . in theory , dissolution of the axon membrane and myelin sheath should be associated with increased content of local water molecules . 
one of the possible reasons is that accumulation of the fragments produced during disintegration of the axonal membrane obstructs the free spread of the local water molecules , and another reason is that the proliferation of astrocytes limits the diffusion magnitude of the water molecules in the affected region to a certain extent [ 28 , 29 ]  . 
 [ 30 ] found that there were certain differences between the region of initial infarction and the region of secondary injury in the features of diffusion in the pyramidal tract . 
they found the fa value decreased and the md value increased in the region of initial infarction , while the fa value decreased and the md value did not change in the region of secondary injury . 
the results of dti detection in the current study meet the feature of diffusion in the region of secondary injury , which proves that the abnormal diffusion in the crus cerebri of patients with striatocapsular infarction is a secondary change but not a new infarction . previous studies showed that the structural integrity of the white matter and the level of overall injury of the neural pathway can be evaluated more objectively by observing the asymmetrical ratio between the fa value of the affected side and that of the unaffected side [ 31 , 32 ]  . 
 fugl - meyer assessment ( fm ) can reflect the interaction of various factors in the process of functional recovery of the affected extremity , and thereby be used to evaluate the motor function of the affected extremity quite accurately . 
this assessment instrument has various items including five domains such as upper and lower extremity motor function , balance , sensory function , joint range of motion , joint pain , etc . 
 data obtained in the current study showed that there was a significant negative correlation between the ai of the fa value of bilateral crus cerebri and the fugl - meyer motor function score of the affected upper extremity . 
this suggests that the motor function of the affected upper extremity in patients with striatocapsular infarction is closely related to the structural integrity of the corresponding pyramidal tract , and that pyramidal tract degeneration significantly affects motor function . 
 [ 9 ] reported that the ratio of the fractional anisotropy values at the first week and second week after pyramidal tract degeneration was negatively correlated with the motricity index obtained after 1 year and positively correlated with the national institutes of health stroke scale score . our study was limited because the patients did not represent a more homogenous population with respect to medical history . 
we compared the dti measures for the ipsilateral and contralateral sides of the same patient . conclusion in conclusion , dti was sensitive for detecting the diffusion abnormality of the crus cerebri in patients with striatocapsular infarction , the integrity of the pyramidal tract in the crus cerebri is closely related to the motor function of the affected upper extremity , and dti can provide an imaging reference for the quantitative evaluation of striatocapsular infarction . 
our findings suggest that information obtained using dti potentially might provide important clinical value for predicting the needs for rehabilitation of upper extremity motor function in 1 3 1070 radiol med ( 2015 ) 120 : 10641070 patients with striatocapsular infarction . 
a longitudinal study is needed to explore the relationship between the early - stage secondary injury of white matter fiber distal to the original lesion and long - term neuromuscular recovery . 
with this prospective study we sought to determine the correlation between contrast enhancement of the plaque and cerebral microembolization after carotid stent deployment and to evaluate the clinical impact of the neurological injury . materials and methods thirty - five consecutive patients with carotid artery stenosis and indications for endovascular stenting were enrolled . 
no correlation was found between neurocognitive test scores and microembolization or plaque enhancement . conclusion contrast enhancement of the carotid plaque is strongly associated with post - procedural microembolization and for this reason it can be considered a reliable tool for an accurate selection of patients undergoing this endovascular treatment . 
it is mainly due to the accidental embolization from the aortic arch or during the crossing of the internal carotid stenosis with the guide wires and catheters or due to the plaque morphology ( soft ulcerated plaques are at higher risk ) during stent deployment [ 2 ]  . 
 a valuable technique to define plaque enhancement and potential risk of embolization is contrast - enhanced ultrasound ( ceus ) [ 58 ] , while diffusion - weighted magnetic resonance imaging ( dw - mri ) is a highly reliable imaging method for detecting recent ischemic brain lesions [ 9 ]  . 
 the aim of this study is to compare plaque enhancement as evaluated by ceus with new cerebral ischemic lesions after cas and to define the clinical impact of the neurological injury . methods the prospective study has been approved by an ethic committee and it has been performed in accordance with the ethical standards laid down in the declaration of helsinki and its later amendments . 
preoperative neurologic assessment included head magnetic resonance ( mr ) examination ( philips achieva 1.5 t , head coil ) and neuropsychological test [ ray auditory verbal learning test ( ravlt ) ]  . 
the mr protocol was performed with t1 - weighted sagittal , t2 - weighted axial , fluid - attenuated inversion recovery ( flair ) axial and diffusion - weighted imaging ( dwi ) with quantitive analysis using apparent diffusion coefficient ( adc ) maps . 
ischemic lesions of the cerebral hemispheres , size , and location were recorded and analyzed by a single operator . 1 3 radiol med ( 2015 ) 120 : 10501055 1052 fig . 
b analysis of the same plaque with quontrast above a color map representing in red the area of higer enhancement and in green the area of lower enhancement , below computer assisted evaluation of ceus pattern with si max and si mean calculation . 
c , d comparison between preand post - procedural dw - mri of the same patient showing new microembolization areas ( red arrows ) cas procedure data collection and statistical analysis angiography was performed in local anesthesia after the administration of a load dose of 300 mg clopidogrel , through a percutaneous femoral access ; a cerebral protection filter ( spiderfx , covidien , plymouth , mn ) was then deployed into the internal carotid downstream the stenosis . 
 cas was performed with a bard vivexx stent ( bard , new providence , nj ) in 30 cases , a carotid wallstent ( boston scientific , natick , ma ) in 3 and an xact ( abbott vascular , redwood city , ca ) in 2 . 
a 1 - month course of double antiplatelet therapy [ clopidogrel 75 mg and acetylsalicylic acid ( asa ) 100 mg ] was initiated , followed by lifelong single antiaggregation therapy with asa . postprocedural patient evaluation and followup before discharge , a second dw - mri study was performed 48 h after cas to detect potentially new brain ischemic lesions . 
follow - up examination included echo - doppler ultrasonography ( at 1 , 6 , 12 months , and then yearly thereafter ) performed by the same operator and clinical and cognitive evaluation ( ravlt ) at 1 month after the procedure . all data from ceus , dw - mri and ravlt scores were collected blinded of the other results to avoid any confounders . 
ceus images were analyzed with quontrast 4.0 dedicated software ( bracco , milan , italy ) , as described in a previous study [ 5 ] , and the maximum and mean signal intensity ( si max and si mean ) were calculated . 
ravlt p value was evaluated in the same group before and after cas for the statistical analysis , the variables , reported as mean standard deviation ( sd ) , were compared with the non - parametric mannwhitney test . 
the categorical variables , reported as counts and percentages with 95 % confidence interval , arranged in row column contingency tables , were analyzed with the chi square test ( with yates correction for 2 2 ) or fishers exact test . 
neurologic postprocedural complications arose in two patients ( 6 % ) : one case of facial paresthesia which completely regressed before hospital discharge and one case of contralateral brachial weakness and numbness which partially resolved at 6 - months and totally regressed at one year follow - up . 
the difference for si mean values was not statistically significant ( p 0.2 ) ( table 2 )  . at 30 days , follow up with echo - doppler ultrasound , we found two patients ( 5 % ) with a moderate degree of intrastent restenosis that remained stable at 6 months and 1 year control . 
because of the significantly higher risk of periprocedural embolization during primary cas as compared with carotid endoarterectomy , ceus can be advantageously applied as a useful imaging system for 1 3 1054 radiol med ( 2015 ) 120 : 10501055 the assessment of plaque morphology [ 12 ]  . 
dw - mri is a highly sensitive method for the early detection of ischemic brain regions by virtue of its ability to identify cytotoxic edema , one of the first hallmarks of brain injury [ 9 ]  . 
data from the literature suggest that , as compared with traditional carotid endarterectomy , postprocedural microembolization is associated with faster neurocognitive decline particularly in memory function [ 3 , 4 ]  . 
therefore , we compared neuropsychological ravlt score before cas and at 1 - month follow - up . we found a direct association between plaque enhancement and postprocedural microembolization , which is consistent with our previous findings on plaque vulnerability and with published data [ 5 , 6 ]  . 
the cut - off values of si mean do not reach statistical significance ( p 0.2 ) however the distribution of values reveal a trend towards a difference between the two groups and this result might be attributable to the small population size . we found no correlation between ceus results and the number of the cerebral lesions or a significant difference between the number of lesions and clinically relevant neurological symptoms . 
as this is an ongoing study , it is important to confirm these results on a larger population study and to investigate other neurocognitive domains with multiple tests and for a longer follow - up . conclusion contrast enhancement of the atherosclerotic plaque is strongly associated with the risk of microembolization after carotid stenting deployment . 
qualitative visual assessment of cerebral wm signal intensity on t2wi was performed by two readers on 78 vlbw infants , scanned on a 1.5 t - mri at term equivalent age . 
both periventricular and subcortical mean adc values were correlated with the neurological follow - up , evaluated with the griffiths mental developmental scale at 36 months . results there was no agreement between the visual qualitative assessment of white matter dehsi and corresponding adc values ( p values 0.42 for periventricular wm ; p values 0.18 for subcortical wm )  . 
 most infants with neurocognitive deficits do not exhibit any definite patterns of injury on magnetic resonance imaging ( mri ) examination , suggesting that more subtle changes may occur [ 3 ]  . 
it has been recently proposed that diffuse white matter damage related to injury of late oligodendrocyte precursors could be a possible cause of neurodevelopmental abnormalities [ 4 , 5 ]  . in the last years mri has contributed to a better understanding of the different patterns of white matter injury in preterm infants such as delayed myelination , enlarged ventricles , loss of white matter volume , punctate lesions and cystic white matter pathology [ 6 , 7 ]  . 
diffuse excessive high signal intensity ( dehsi ) on t2 - weighted mr imaging has been described as a common finding in very low birth weighted ( vlbw ) infants , occurring in up to 75 % of infants at term equivalent age [ 8 , 9 ]  . 
however , the anatomical meaning of dehsi is still controversial and it is uncertain whether it represents diffuse white matter injury or delayed maturation [ 10 , 11 ]  . 
 therefore , the clinical impact of dehsi on the neurodevelopmental outcome of vlbw infants is still not well known . in the last decades mr studies have been showed that vlbw infants with dehsi had white matter apparent diffusion coefficient ( adc ) values higher than healthy term babies , but similar to those of preterms with major focal lesions , suggesting that dehsi could be a possible correlate of diffuse white matter injury [ 1315 ]  . 
also diffusion tensor imaging ( dti ) studies lately showed that both axial and radial diffusivity are significantly elevated in the white matter of preterm infants with dehsi compared with preterm infants with normal - appearing white matter ( wm ) and term control infants . this hypothesis , however , is still debated to date . objective measurements and correlation with the neurological outcome is therefore necessary to evaluate whether dehsi represents itself an overt wm abnormality or it is just a physiological delay in the brain maturation process of vlbw infants . the primary aim of our study is to establish an objective and reproducible method of defining dehsi in vlbw infants , by performing both a qualitative assessment on conventional t2 - mri and a quantitative assessment through adc calculation . 
the secondary aim is to investigate the clinical relevance of dehsi correlating mri biomarkers with neurodevelopmental outcome evaluated at 36 - month corrected age . methods patients 32 weeks and / or birth weight we retrospectively enrolled 78 vlbw infants ( 37 males and 41 females ) , from a group of 497 vlbw babies who were admitted to the neonatal intensive care unit ( nicu ) of our institute from january 2007 to december 2009 . 
the exclusion criteria were : presence of major and minor brain lesions ( defined as cystic periventricular leukomalacia , punctate lesions , intraventricular hemorrhage , focal parenchymal lesions and brain malformations ) , chromosomal or metabolic disorders , congenital malformations and congenital infections . 
none of the twins affected by twin - to - twin transfusion syndrome ( ttts ) during fetal life gave ischemia of the wm . we excluded 15 neonates due to the presence of excessive motion artifacts on mri imaging . 
obstetrics findings ( multiple pregnancy and intrauterine growth restriction ) and common complications of prematurity , such as neonatal sepsis and respiratory distress syndrome , were considered in our analysis . 
term healthy babies were scanned due to diaphragmatic hernia : they did not show any neurological symptoms and no brain lesions at mri . mr imaging technique mr imaging examinations during 20072008 were performed with a 1.5 - t unit ( siemens magnetom avanto syngo ) using a four channel head coil . 
two different observers , expert in nicu brain imaging ( 25 and 13 years , respectively ) analyzed the images separately , scoring the wm signal in : the mean periventricular and subcortical adc values were calculated and compared with the mean adc values of a group of healthy term babies used as reference . suggested upper limits of normality for adc values were defined as two standard deviations above the mean for a group of ten children born at term with normal visual appearances on mr images , based on the values previously described by boardman et al . 
the gmds gives an overall developmental quotient ( dq ) with subscales assessing six different skills : locomotor , personal social , hearing and speech , eye and hand co - ordination , performance , and reasoning . 
 the mean dq score for the general population is 100 ( with 15 ) and the test is considered nora standard deviation of mal when dq > 88 , indicative of mild neurological delay when dq 7587 , and indicative of severe neurological delay when dq < 74 . 
this scoring system was based on the authors arbitrary decision , due to the absence in literature of a standardized and objective method to assess hyperintensities on t2wi [ 12 , 16 , 17 ]  . the second method was a quantitative assessment with the calculation of the adc values of cerebral wm , calculated by a single observer blinded by all mri reports . 
clinical characteristics of our population are summarized in table 1 . mri qualitative analyses a weak interobserver agreement for the periventricular ( k coefficient 0.35 ) and subcortical ( k coefficient 0.49 ) wm visual assessment was found . 
results are shown in table 2 . the incidence of dehsi was equal both to the philips and the siemens time period of scanning . mri quantitative analyses the intraobserver agreement over repeated adc measurements in six rois was good for all the rois drawn on periventricular and subcortical wm , with pearsons correlation coefficients of 0.83 ( p values < 0.001 ) for frontal periventricular wm , 0.88 ( p values < 0.001 ) for parietal periventricular wm , and 0.81 ( p values < 0.001 ) for subcortical wm . no agreement between the visual qualitative assessment of wm on t2 - weighted images and their corresponding adc values ( p values 0.42 for periventricular wm ; p 0.18 for subcortical wm ) was observed . 
in our study the correlation between the qualitative t2wi evaluation and the quantitative adc analysis was relatively weak , mainly with regards to mild and moderate high signal on t2wi ( score 0 and 1 ) , and these results are concordant with data found in literature . a better correlation was found between the highest signal on t2wi images ( score 2 ) and quantitative analysis , but this result does not seem to be significant due to the small amount of infants ( four preterms )  . 
the only clinical variable that was associated with lower mean adc values was sepsis ; however , the number of infants in this subgroup ( n 4 ) was very small , making any statistical inference poorly significant . a further aim of our study was to evaluate if increased adc values in vlbw infants can be used as a biomarker for neurodevelopmental abnormalities . 
it was initially suggested that even in cases of isolated dehsi , the increased signal intensity and the changes in adc values , also without further lesions , could potentially reflect an insult during myelination with subsequent neurological impairment . we evaluated a possible correlation between adc values in wm of vlbw , and the neurological outcome , assessed by the gmds studies [ 21 , 26 ]  . compared to previously reported studies we extended the follow - up evaluation until 36 months to detect minor neurological abnormalities presenting later in child development [ 14 , 16 , 17 ]  . 
during this period major changes occur , such as language acquisition , motor development , socialization , and connection between visual and motor functions . in agreement with previous data our findings showed no significant correlation between the increasing adc values and both the total dq and the six different items separately , confirming that adc is not a good biomarker for motor and cognitive long - term outcome in vlbw infants . the correlation between adc values and high personalsocial performance is an unusual result , with poor statistic significance and difficult interpretation . 
this result may be further investigated . a more recent study [ 27 ] try to assess dehsi using dti , showing that it could be a phenomenon related to altered wm integrity and to altered maturational trajectory . 
 these results supported the idea that dehsi reflects alteration at the microstructural level , without correlation with neurodevelopmental outcome . all these data support the hypothesis that dehsi in preterm infants is more likely a sort of delayed maturation of wm rather than a true pathological entity . 
in addition , dehsi seems to be an age - related phenomenon , usually no longer detectable after the 45th week of corrected age [ 8 ]  . this study has some limitations . 
nevertheless , a longer follow - up is advisable , to detect minor neurobehavioral , as well as social - emotional impairments that manifest themselves later in childhood . conclusions in conclusion , visual appearances of dehsi on mr imaging following preterm birth are subjective . 
in the case of stenosisobstruction and stulas ( 104 complications ) , the rst therapeutic step was placement of a nephrostomy catheter , followed by balloon ureteroplasty , placement of external internal catheters and double - j stents ; 14 / 33 collections were drained under ultrasound guidance . results in all 118 percutaneous interventions , we were able to place a nephrostomy or drainage catheter , with a technical success rate of 100 % . 
the long - term success rate was 49.6 % : in 57 / 115 ( three patients were lost to follow - up ) we obtained the complete resolution of the complication . 
however , post - transplant complications , which arise , according to the literature , in 415 % of patients , continue to be a cause for concern as they are responsible for a relatively high number of organ losses and sometimes of patients [ 1 ]  . 
the major urological complications include steno - obstructions and stulas ( categorised in the literature as early and late , based on a cut - off of 3 months for stenoobstructions and 15 days for stulas ) as well as periand para - renal collections [ 13 ]  . 
their treatment is currently the remit of interventional radiology ( ir ) which has signicant advantages over open surgery , and namely : shorter hospital stay , fewer infectious complications , better preservation of renal function with lower mortality and reoperation rates [ 4 ]  . surgical revision , subject to a 1030 % risk of severe complications [ 5 ] , is now reserved for selected cases including late diagnoses , impassable stenoses , and failure of ir . 
gandini department of surgical sciences , radiology institute university of torino , a.o citta` della salute e della scienza di torino , via genova 3 , 10126 turin , italy e - mail : paolo.fonio@unito.it materials and methods the kidney transplantation centre of our institution , 1 , 146 kidney transplantations were performed between radiol med ( 2015 ) 120 : 206212 2000 and 2010 . 
there were 146 major urological complications in 98 patients ( 59 m , 39 f ; age range 3178 years ; mean 55.7 years ) divided as follows : 77 steno - obstructions , 36 stulas and 33 collections . 
of these , 118 ( 80.8 % ) complications in 91 patients were treated with ir procedures . clinical presentation stenosis the most frequent symptoms were haematuria and fever , in some cases very mild ; only a minority of patients were asymptomatic . 
seventy - four of 77 patients had increased serum creatinine ( 26.2 mg / dl , mean 3.23 mg / dl ) , with oligo - anuria and uid retention . 
in 3 / 77 patients with normal creatinine levels ( \1.2 mg / dl ) and slight reduction in diuresis , the only indication for treatment was a sonographic nding of hydronephrosis . 
an ultrasound ( us ) examination , always performed as a rst - line investigation , demonstrated urinary tract dilatation ( mean diameter of the renal pelvis of 23 mm 7.8 ) in 97 % of cases . 
dynamic renal scintigraphy ( 27 patients ) and magnetic resonance imaging ( mri ) and / or computed tomography ( ct ) ( 12 patients ) were also carried out to complete the diagnosis of ureteral obstruction . 
depending on the time of onset ( cut - off used : 3 months ) , the 77 stenoses obstructions were divided into early ( 30 / 77 ; 39 % ) and late fig . 
1 a uretero - vesical anastomotic stricture demonstrated at antegrade pyelograb 8 - mm diameter balloon dilation of the stricture . c ureteral stent placement ( 10 french ) after ureteral balloon dilation ; a small calibre nephrostomy catheter is positioned as well 208 radiol med ( 2015 ) 120 : 206212 table 1 stenosis sites and aetiology site of the stenosis number ( % ) early late pyelo - ureteral junction proximal ureter middle ureter distal ureter multiple sites total vesico - ureteral anastomosis 18 ( 23.4 ) 8 ( 10.4 ) 5 ( 6.5 ) 17 ( 22 ) 22 ( 28.6 ) 7 ( 9.1 ) 77 ( 100 ) table 2 leakage sites and aetiology of stulas site of the stula number ( % ) early late pyelo - ureteral junction proximal ureter middle ureter distal ureter vesico - ureteral anastomosis uretero - ureteral anastomosis multiple sites unknown total 3 ( 8.33 ) 1 ( 2.78 ) 3 ( 8.33 ) 9 ( 25 ) 11 ( 30.55 ) 4 ( 11.12 ) 3 ( 8.33 ) 2 ( 5.55 ) 36 ( 100 ) ( 47 / 77 ; 61 % ) ; the most frequently involved locations were the pyelo - ureteral junction ( 18 / 77 ; 23.4 % ) and the vesicoureteral anastomosis ( 22 / 77 ; 29 % )  . 
aetiologically , stenoses were classied as follows : 57 intrinsic stenoses , three stones , nine obstructions due to blood clots , eight extrinsic ureteral compressions due to uid collection ( 1 case ) , brosis ( 4 cases ) , renal cyst ( 1 case ) , and spermatic cord causing compression on the pyelo - ureteral junction ( 2 cases )  . fistulas the predominant symptoms were localised pain , increased creatinine although with lower values than seen in the steno - obstructions ; ( mean 2.55 mg / dl ) and reduction in diuresis . 
in early stulas , urine leakage was observed from the surgical drain ; in the remaining cases , the leakage occurred from the insertion site of the recently removed drain or from the surgical scar . 
onset of the 36 stulas ( cut - off used : 15 days ) was categorised as early in 19 cases ( 52.7 % ) and late in 17 table 3 first - line treatment : medical , surgical and percutaneous options in kidney transplants type of complication number medical therapy no . 
us enabled identication of the collection in all cases , but the diagnosis was possible only by analysing the uid leaking out from the surgical drains or drain insertion sites or aspirated under us guidance . only the larger collections manifested with pain , fever , leukocytosis ( abscess ) , and elevated creatinine levels . treatment seventy - ve out of 77 ( 97.4 % ) steno - obstructions and 29 / 36 ( 80.5 % ) stulas were treated percutaneously in the rst approach : only 2 / 77 ( 2.6 % steno - obstructions ) and 2 / 36 ( 5.5 % ) stulas were treated with a surgical approach . five out of 36 ( 14 % ) minor stulas , diagnosed on the basis of urine leakage from the surgical drainage , resolved spontaneously . 
all patients provided their written informed consent . acid the observation period lasted until march 2011 , allowing a follow - up period between 6 months and 11 years ( mean follow - up , 52 months )  . major complications were dened as graft loss , sepsis , severe haematuria and accidental puncture of adjacent organs . 
among the minor complications ( not requiring included arterial obstruction and / or dislocation of catheters and stents , ureteral infections treatable with medical therapy , and subcapsular or perirenal haematomas . lesion , mild haematuria , surgery ) , we embolization and / or results immediate in the analysis of the results , we evaluated immediate long - term success and any possible technical success , procedure - related complications . technical success refers to the restoration of the continuity of the stenotic or damaged urinary tract . 
clinical success is the resolution of the complication with removal of the stent and / or drainage catheter not compromising renal function . in all 91 patients with steno - obstructions and / or ureteral stulas and in 14 patients with associated uid collections we were able to place a pyelostomy catheter or perform a us - guided drainage with an immediate technical success rate of 100 % ( 91 / 91 , 14 / 14 ) with no related complications . steno - obstructions the 75 steno - obstructions undergoing percutaneous treatment , three patients were lost to follow - up , including one treated with balloon dilatation and two with double - j stent placement ( without prior balloon dilatation )  . 
among the tion ; one of them was lost remaining 36 patients , despite a satisfactory immediate result ( resolution of the stenosis ) in all cases , the long - term clinical success was 44.4 % ( 16 / 36 )  . 
in 20 / 36 cases , either the stenosis recurred or it was not possible to remove the stent and / or catheter without worsening renal function . worse results were found in the treatment of the stenoses of the uretero - vesical anastomosis ( 7 / 22 ; 35 % ) and of the fig . 
2 antegrade pyelogram demonstrates ureteral leak in proximity of uretero - vesical anastomosis double - j ureteral stents without prior dilatation , and 24 ( 32 % ) with only nephrostomy catheter without additional in 37 / 75 steno - obstructions percutaneous procedures . treated with ureteral balloon dilatation , the number of dilations performed for each patient varied between 1 and 4 ; in particular , 24 patients underwent one session , seven underwent two , ve underwent three and one underwent four . 
of pyelo - ureteral the 20 / 36 restenoses , 13 / 20 were treated with surgery , 4 / 20 with long - term double - j stent , 1 / 20 with long - term internal external catheter . 
finally , in 2 / 20 cases it was necessary to explant the transplanted kidney , in one case because of urothelial neoplasm and in the other because of chronic rejection . fourteen out of 75 patients were treated with a double - j stent not associated with balloon dilatation and of these two were lost to follow - up . 
in all other cases , however , ir helped to restore impaired renal function and to perform surgery in stabilised clinical conditions . fistulas in this group , no patients were lost to follow - up . 
in a period between 20 days and 4 months , in 5 / 20 patients , after healing of the stula , a residual stenosis was detected : in 4 / 5 cases ( 80 % ) the site of stenosis coincided with that of the stula ( ureteralvesical anastomosis )  . 
overall , the long - term success of exclusive percutaneous treatment of stulas was 58.6 % ( table 4 )  . collections associated with stenoses / stulas us - guided drainage of the collections was possible in all 14 / 14 cases with an immediate technical success of 100 % . in all cases , the collection was associated with a stula , treated with insertion of a pyelostomy , but only in 9 / 14 patients ( 64.3 % ) , positioning of the drainage tube represented a complete clinical success . 
the remaining ve patients ( 35.7 % ) underwent surgery ( table 4 )  . overall success and complications the percentage of overall long - term success , including the types of complications percutaneous treatment of all ( steno - obstructions , stulas and collections ) was 49.6 % ( 57 / 115 cases ) ( table 4 )  . there were 15 minor complications ( 14.4 % ) : 2 / 15 stent obstructions due to blood clots ; 8 / 15 dislocations of stents that were subsequently repositioned correctly ; 1 / 15 cases of ureteral rupture , and 4 / 15 cases of gross haematuria which , however , did not require interventional or surgical treatment . 
only one patient out of a total of 91 ( 0.8 % ) developed a major complication represented by an infection accompanied by urine peritonitis . discussion major urological complications , represented by stenoobstruction and stulas , are among the most important concerns in the short - , mediumand long - term follow - up of transplant patients . 
 [ 5 ] found early and late stenoses to be evenly balanced . as for stulas , there is a substantial uniformity in the literature regarding the time of onset of stulas , which usually arise in the early period due to ischaemic injury to the distal third of the ureter or because of problems at the level of the anastomosis . 
correlation of the time of appearance and location of the complication reveals that anastomotic leaks are early in the 90 % of the cases , consistent with the aetiology of surgical dehiscence of the anastomosis . for many years , the treatment of choice for urological complications after renal transplantation was surgery , but this is burdened by a high rate of complications ( 1030 % ) , including graft loss [ 5 ]  . 
in the present study , the immediate technical success of nephrostomy was 100 % : the procedure was successfully performed in all of the 104 cases , with a rate of major complications equal to 0 . for obstructions due to stenosis , the subsequent therapeutic procedure was to perform ureteral dilatation ( with cutting balloon in the most resistant case ) and position a stent or internalexternal drainage . 
although the authors emphasise that the characteristics of these stents prevent ingrowth and allow for endoscopic removal , we believe that they may represent a serious obstacle to a subsequent surgical revision . in our experience , in contrast to early stenoses ( 48.3 % clinical success ) , late stenoses ( 39.5 % clinical success ) resulting from chronic ischaemic brosis of the ureteral wall showed a higher incidence of recurrence despite the good morphological results obtained immediately after dilation . 
nevertheless , we believe that these results still justify a preference for percutaneous treatment as a rst - line approach to stulas , in 212 radiol med ( 2015 ) 120 : 206212 consideration of the minimal invasiveness of the procedure which is compatible with subsequent surgical repair . ( obtained success a few studies in the literature analyse the percutaneous treatment of associated uid collections , reporting a success rate between 50 and 85 % [ 14 , 24 ] ; carrafello et al . in 3 / 4 included only lymphoceles patients , 75 % )  . 
as for urinomas , we only considered urinomas requiring drainage ; other cases of small extraluminal urine leakages due to the stulas were solved with placement of a nephrostomy catheter only . in our series , the rate of major complications of percutaneous procedures ( not always reported in the literature ) was 0.8 % ( only one case of severe infection )  . 
miele e - mail : vittoriomiele@alice.it free peritoneal uid on us and ceus , and sensitivity for the grading of lesions on ceus were calculated compared with the ct ndings , in accordance with the american association for the surgery of trauma criteria . results ce - mdct identied 84 abdominal traumatic lesions ( liver = 28 , spleen = 35 , kidney = 21 ) and 45 cases of free intraperitoneal uid . 
us depicted 50 / 84 traumatic lesions and 41 / 45 cases of free peritoneal uid ; ceus identied 81 / 84 traumatic lesions and 41 / 45 free peritoneal uid . 
the sensitivity , specicity , ppv , npv and overall accuracy for the identication of traumatic abdominal lesions were 59 , 99 , 98 , 83 and 86 % , respectively , for us and 96 , 99 , 98 , 98 and 98 % , respectively , for ceus . 
the values for the identication of haemoperitoneum were 91 , 99 , 95 , 98 and 97 % , respectively , for us and 95 , 99 , 95 , 99 and 98 % , respectively , for ceus . 
ceus successfully staged 72 / 81 traumatic lesions with a sensitivity of 88 % . conclusions isolated abdominal trauma us should be replaced by ceus as the rst - line approach , as it shows a high sensitivity both in lesion detection and grading . 
ce - mdct must always be performed in ceus - positive patients to exclude active bleeding and urinomas . patients with low - energy keywords traumatic injury ( cid : 2 ) hematoma ( cid : 2 ) laceration ( cid : 2 ) active bleeding ( cid : 2 ) urinoma ( cid : 2 ) ultrasound ( cid : 2 ) contrastenhanced ultrasound ( cid : 2 ) second - generation blood - pool contrast agent ( cid : 2 ) contrast - enhanced multidetector computed tomography introduction trauma patients involved in a high - energy accident who are in stable condition or whose vital functions have been radiol med ( 2015 ) 120 : 180189 stabilised are rapidly examined with total - body computed the most accurate and panoramic tomography ( ct ) , imaging tool in the assessment of polytrauma [ 1 ]  . abdominal ultrasound ( us ) performed in the emergency room on unstable patients is termed fast ( focused assessment with sonography for trauma ) , and is real - time sonographic scan of four regions for the detection of free peritoneal uid [ 2 ]  . the management of patients with mild or low - energy trauma is still the subject of controversy ; evaluation of the patients clinical presentation and the mechanism of the injury are fundamental for the decision to immediately perform ct or assess the patient with conventional radiographs , sonography , and clinical observation [ 3 ]  . baseline abdominal us is the rst step in the protocol in many emergency centres and it is recommended to be performed before the ct study . 
us is a rapid , repeatable , noninvasive and inexpensive examination that has high sensitivity for the detection of free intra - abdominal uid but fairly low sensitivity ( even below 50 % in the literature ) for the detection of abdominal solid organ traumatic lesions [ 4 ]  . contrast - enhanced us ( ceus ) in traumatic patients has been shown to be more sensitive than us for the detection of solid organ injuries , improving the identication and lesions with levels of grading of traumatic abdominal sensitivity and specicity similar to ct ( up to 95 % in the literature ) [ 24 ]  . 
the aim of this study was to evaluate the accuracy of ceus in the detection and staging of abdominal traumatic lesions in patients with low - energy isolated abdominal trauma in comparison with baseline us and contrast - enhanced multidetector ct ( ce - mdct ) , considered the gold standard . materials and methods patients we performed a retrospective review of a case series that included 256 consecutive patients who arrived at our emergency department between january 2006 and december 2012 ( 159 males , 97 females , age range 782 years , mean age 41 years ) , with a history of lowenergy isolated abdominal trauma and in stable haemodynamic condition ( pulse pressure [ 90 mmhg , heart rate \100 beats per minute , respiratory rate \20 respirations per minute ) , categorised yellow or green using the start triage acuity scale . 
of patients motorcycle and car crashes working trauma accidental trauma sport trauma informed consent was obtained from all the patients or from their relatives in the case of minors . examination technique conventional us and ceus examinations were performed with a siemens acuson sequoia 512 system ( siemens medical systems , forchheim , germany ) using a curvedarray 4 mhz multi - frequency probe . baseline abdominal us was followed by ceus performed in the same session with an intravenous bolus injection of a second - generation blood - pool contrast agent ( sonovue , bracco ) consisting of stabilised microbubbles of sulphur hexauoride gas covered by a stabilising phospholipidic membrane . 
immediately after the rst bolus the right - sided organs ( right kidney and liver ) were explored for 13 mwith the second dose the leftside organs ( left kidney and spleen ) were focused on for a further 34 min [ 9 ]  . 
all ceus examinations were performed by highly experienced radiologists , with at least 5 years experience in emergency radiology and with specic expertise in trauma imaging ( us , ceus , mdct )  . all patients underwent ce - mdct examination within 1 h after ceus , using a standard arterial and venous protocol , with a 16 - detector - row ct scanner ( 16 lightspeed , ge healthcare , usa )  . 
no patient received oral contrast medium and all underwent a pre - contrast acquisition series . a volume of nonionic contrast medium of 100150 ml was injected at a rate of 24 ml / s through an 1820 - gauge angiography catheter . 
a delay ranging from 40 to 50 s was used for the arterial phase and from 80 to 100 s for the second acquisition ; in the presence of collections , a late182 radiol med ( 2015 ) 120 : 180189 phase study ( at 315 min ) was performed to identify any active bleeding or urinoma . data collection in this study we analysed only traumatic parenchymal injuries of liver , spleen and kidneys ; no pancreatic lesions and no mesenteric or bowel lesions were depicted . positive ndings on us were solid organ injury and peritoneal uid . 
on us a parenchymal traumatic lesion was depicted as an intraparenchymal hyperor hypoechoic area or distortion of the normal echoic structure [ 9 , 10 ]  . on ceus examination positive ndings were parenchymal lesions , intraparenchymal or subcapsular haematoma , active blush and peritoneal uid . 
1 41 - year - old female involved in a motorcycle crash : a ultrasound ( us ) examination shows an inhomogeneous hypoechoic parenchymal area of the liver and a subcapsular haematoma ; b contrast - enhanced us ( ceus ) scan shows grade iii traumatic laceration on hepatic segment vii with a parenchymal and subcapsular haematoma ; c axial multidetector computed tomography ( mdct ) examination shows the hyperdense subcapsular and intraparenchymal haematoma ; d ce - mdtc scan shows identical ndings to ceus radiol med ( 2015 ) 120 : 180189 fig . 
2 49 - year - old male involved in a motorcycle vs car accident : a us image shows a ne distortion of the normal echoic structure on hepatic segment v ; b ceus scan shows a hypoechoic grade iii traumatic lesion on segment v ; axial ( c ) and coronal ( d ) ce - mdct scans show identical ndings to ceus results in the 256 patients included in the study , ce - mdct identied 84 ( 32 % ) abdominal positive traumatic ndings of the liver ( n = 28 ) , spleen ( n = 35 ) and kidney ( n = 21 )  . in 45 / 256 patients ce - mdct depicted free intraperitoneal uid . on the basis of the ce - mdct ndings , considered as the reference standard , we analysed the capacity of us and ceus to identify the traumatic lesions . 
us yielded one false positive in the identication of traumatic injuries ( one lesion of the liver segment viii which turned out to be a focal liver lesion on ct ) and two false positives in the detection of haemoperitoneum ( two young women with a small amount of free uid in the pouch of douglas )  . ceus identied 81 / 84 traumatic injuries ( liver = 27 / 28 , spleen = 34 / 35 , kidney = 20 / 21 ) ( table 2 )  . 
ceus yielded three false negative results ( one liver lesion \1 cm in segment viii , one splenic lesion \1 cm and one small contusion of the left kidney ) and one false positive result ( a hypoechoic lesion of the spleen which turned out to be an ischaemic area on ct )  . 
the number of true positives , false positives , true negatives and false negatives yielded by us and ceus compared with mdct in the detection of traumatic injuries and free peritoneal uid are reported in tables 3 and 4 . 
the sensitivity , specicity , positive and negative predictive values and accuracy for the identication of traumatic abdominal lesions were , respectively , 59 , 99 , 98 , 83 and 86 % for us and 96 , 99 , 98 , 98 and 98 % , respectively , for ceus ( table 5 )  . 
the four understaged lesions were distributed as follows : two liver lesions ( one ceus grade i was grade ii on ce - mdct ; one ceus grade ii was grade iii on ce - mdct ) and two splenic lesions ( two ceus grade i were grade ii on ce - mdct )  . in the identication of active bleeding ce - mdct depicted ten cases , six from the liver ( one of which with capsule rupture and blushing into the peritoneal cavity ) and four from the spleen . 
4 78 - year - old female involved in a domestic accident : a difcult baseline us in noncooperative patient does not show any parenchymal splenic lesion but only a small amount of perisplenic uid ; b ceus examination shows a hypoechoic grade ii traumatic laceration involving the capsular surface of the spleen ; c , d axial ce - mdct and coronal multiplanar reconstruction ( mpr ) conrm the ceus ndings 186 radiol med ( 2015 ) 120 : 180189 fig . 
this is a rapid , complete , and reproducible imaging study which allows rapid detection of all the possible body injuries in a single examination ( head , spine , chest , abdomen , pelvis and extremities ) , with the possibility to promptly detect prognostic negative factors ( such as active bleeding ) and so to direct the polytrauma victim to conservative or surgical management . in haemodynamically unstable patients the fast examination can be done in the emergency setting without interrupting resuscitation manoeuvres and has a reported sensitivity for the detection of intraperitoneal free uid between 63 and 96 % [ 1 ] ; its major limitations are poor sensitivity in the direct detection of solid abdominal organ lesions and in the visualisation of haemoretroperitoneum . radiol med ( 2015 ) 120 : 180189 fig . 
6 8 - year - old male involved in a sport accident : a baseline us shows an inhomogeneous hypoechoic parenchymal area on hepatic segment vii ; b this ceus scan shows a hypoechoic grade iv laceration and parenchymal haematoma involving the capsule ; c this ceus image clearly depicts the active bleeding with interruption of in patients with mild or low - energy trauma , there is a large spectrum of possible imaging modalities : ct , conventional radiography , or us can be performed on the basis of clinical presentation and laboratory parameters . 
in the diagnostic assessment of trauma patients abdominal us is frequently used as a rst - step modality for its safety , repeatability and noninvasiveness , and ability to determine the need for abdominal ct . 
systematic use of ct after low - energy trauma , in fact , may lead to inappropriate delays in patient care , is costly , and involves radiation exposure to a young patient population [ 1 ]  . the sensitivity of us for the detection of free abdominal uid varied from 63 to 99 % but the reported sensitivity for the detection of solid organ lesions is quite low , below 50 % [ 24 ]  . 
peritoneal uid can be related to trauma but it can also be present in other conditions such as ovulation , ascites etc . the introduction of second - generation contrast agents into clinical practice has improved us accuracy in the organ prole ( red arrow ) ; d axial mdct shows the parenchymal and perihepatic hyperdense haematoma ; e , f axial and coronal cemdct scans conrm the ceus ndings with evidence of capsule rupture and blushing out in the peritoneal cavity ( red arrow ) injury after blunt detecting parenchymal abdominal trauma , increasing the lesion identication rate with sensitivity values in the denition of lesion size , relationship with the capsule and vessel peduncle similar to those of ct [ 24 , 614 ]  . 
ceus can additionally identify ndings undetectable at conventional us , such as infarcts and contrast extravasation [ 5 , 1517 ]  . in our study only parenchymal injuries of the liver , spleen or kidneys were evaluated ; no pancreatic lesions were depicted . 
us identied 50 traumatic injuries of the 84 depicted on ct , with a sensitivity of 59 % ; the sensitivity of us in the detection of free peritoneal uid was higher ( 91 % )  . 
the use of contrast medium greatly improved the number of detected lesions but also the quality of ndings , with a better denition of lesion extension , margins and relationship with the capsule and vessels . 
ceus correctly identied 81 / 84 traumatic lesions depicted on ce - mdct , increasing the value of sensitivity for the detection of traumatic abdominal injuries from 59 % of us to 96 % . 
7 7 - year - old female involved in an accidental trauma during outdoor game : a longitudinal us does not show any lesion but only a ne cortical parenchymal inhomogeneity of the left kidney with perirenal uid ; b blood clot in the bladder , indirect sign of a traumatic lesion of the collector system ; c ceus very well depicts the renal fracture and the presence of perirenal uid ; d axial mdct shows a hyperdense perirenal collection ; e axial ce - mdct in the venous phase depicts the renal fracture and conrms the perirenal uid that in the late phase ( f ) turned out to be a urinoma ( red arrow ) false negative ndings on ceus were all grade i lesions , due to minor injuries , without relevant consequences for patient management and prognosis . 
in lesion grading ceus correctly staged 72 of the 81 detected lesions using the aast criteria , with a sensitivity of 88 % : nine lesions were understaged on ceus ( four of the liver , four of the spleen and one of the kidneys )  . 
in four cases , ceus only understaged minor traumatic injuries that required a conin four cases servative , nonsurgical management , but ceus understaged traumatic lesions because of failure to identify the presence of contrast pooling ( in 2 / 6 liver lacerations and in 2 / 4 splenic injuries ) ; nally in one case ceus failed to detect a lesion to the urinary tract ( understaging a grade iv kidney lesion on ce - mdct )  . therefore , in our experience the main limitations of ceus are its poor visualisation of active bleeding and its inability to demonstrate lesions to the urinary tract . 
indeed , in our series ceus did not recognise the presence of active bleeding in 40 % of cases ( 4 / 10 lesions ) with a sensitivity of 60 % ; in one case ceus did not demonstrate lesions to the urinary tract . 
in our experience , when positive ndings are demonstrated on ceus , ct becomes necessary to identify any negative prognostic factors such as active bleeding or lesions to the urinary tract . conclusions in patients with low - energy isolated abdominal trauma , conventional us has low sensitivity in the identication of organ injuries and should , therefore , be replaced by ceus as the rst - line approach . 
ceus has shown a high sensitivity both in the detection and grading of traumatic lesions . patients with negative ceus may be discharged , monitoring the clinical and laboratory ndings , without undergoing ct examination because only lower grade injuries could be missed . 
ceus in fact can clearly demonstrate most of the aspects relevant for management with radiol med ( 2015 ) 120 : 180189 a high sensitivity in both detection and grading . 
a more is the sensitivity of ceus in the controversial aspect detection of contrast - medium extravasation , as well as its inability to depict lesions to the urinary tract , ndings which are clearly depicted on ct . 
uterine bre architecture was depicted by mr - dti with 3d tractography reconstruction providing quali - quantitative analysis of bre , described as reduction of number of longitudinal bres that run through the uterine scar . results six subjects were excluded . 
according to 3t - mr morphology , scars were described as linear ( n = 12 ) and retracting ( n = 12 ) ; disagreement with tvus was 54 % . the thickness of myometrium at the scar level was found to be signicantly greater with 3t - mr compared to tvus in f . 
among retracting scars , bre reduction was signicantly higher compared to linear scars , p \ 0.016. conclusions the added value of 3t - mr with dti lies in the prompt evaluation of muscle bre remaining at scar level . keywords caesarean scar ( cid : 2 ) fibre tracking 3t - mri ( cid : 2 ) diffusion tensor imaging ( cid : 2 ) introduction the overall rate of caesarean section ( cs ) has dramatically increased in developed countries over the last decade [ 1 ]  . this has led to an increase in abnormalities of placentation such as placenta previa and / or accreta [ 26 ] and uterine rupture [ 710 ]  . 
the who global survey on maternal and perinatal health , a large cross - sectional study conducted across 24 countries , concluded that cs is associated with an increased risk of both maternal and fetal morbidity and mortality [ 11 ]  . 
therefore , most guidelines advocate trial of labour after prior cs ( pcs ) [ 12 , 13 ]  . thus , investigators have focused on nding a more precise method of scar evaluation in order to create an objective tool to predict which pregnancies are at risk following pcs . 
to select women with the lowest risk of uterine rupture , some authors [ 1420 ] suggested the use of the sonographic measurement of the lower uterine segment radiol med ( 2015 ) 120 : 228238 ( lus ) thickness near terunfortunately , this did not become recommended clinical practise because the optimal cutoff values and measurement techniques remain controversial . 
according to these studies , large scar defects have been found in various proportions of women who have undergone cs , and the rate of large scar defects increases with the number of caesarean deliveries [ 2224 ]  . currently , the clinical importance of large scar defects is unknown . 
it is possible that they entail a greater risk of complications in subsequent pregnancies ( such as uterine rupture or abnormalities in placentation ) than intact scars or scars with only small defects . 
however , this remains an open issue . magnetic resonance ( mr ) is another imaging modality that has a well - established role in studying the female pelvis , especially at high eld strengths ( 3 t ) [ 2731 ]  . 
mr with diffusion tensor imaging ( mr - dti ) and bre tracking reconstruction is a novel noninvasive imaging technique that could characterise tissue morphology by measuring the amount of random diffusion ( brownian motion ) of water molecules throughout the tissue [ 32 ]  . 
as water molecules diffuse more easily along organised structures , such as than across them , mr - dti can muscle bres , highlight the muscle bre architecture of the uterus . 
recently , our research group showed that this method could be used to describe the uterine muscle architecture in vivo and that women with pcs showed various degrees of disarray [ 34 ]  . rather therefore , the aims of the present study were as follows : to compare tvus with 3t - mr in the morphological evaluation of caesarean scar , and to investigate the potential added value of mr - dti with bre tracking reconstruction in assessing uterine scars in women with pcs . materials and methods subjects this was an observational open study . 
primiparous women with one previous vaginal delivery served as the control group . gestation delivered by elective cs ( with a low transverse uterine incision ) without labour within 24 months . 
exclusion criteria were the following : multiple gestations , more than two pcs , trial of labour after the rst cs , women with uterine myomas , uterine retroversion or retroexion , use of hormonal contraception , and women with other previous uterine scars , post - partum endometritis , pelvic inammatory disease and tubal ligation , as well as those with generic exclusion criteria for mr . study design all volunteers underwent tvus ( esaote mylab 50 xvision ) and 3t - mr with dti ( philips achieva , the best , netherlands ) within 2 days of each other . 
women were examined during the follicular phase and a negative pregnancy test was required . to compare tvus to 3t - mr in the morphological assessment of caesarean scar at the hysterectomy site , the myometrial thickness was measured , by both methods , from the endometrial interface to the serosa at the following three levels : at level , upstream and downstream of the scar . the scar all subjects underwent 3t mr - dti with bre tracking reconstruction for the assessment of the uterine scar , which provided supplementary quali - quantitative information about the microstructural disarray of the uterine myometrial bres . methods tvus technique all tvus were performed using transvaginal 7 mhz ultrasonography ( esaote mylab 50 x vision )  . 
subsequently , myometrial morphology and echogenicity were evaluated , and the myometrial thickness was measured . 3t - mr technique inclusion criteria were 1845 years , caucasian ethnicity , and a prior singleton following : all patients underwent 3t - mr imaging ( achieva , philips medical systems , best , the netherlands ) using a 6 - channel 230 radiol med ( 2015 ) 120 : 228238 fig . 
a single - shot turbo spin - echo ( ssh - tse ) t2 image on the uterine proper long axis with reported measurement at scar level ( scar classied as linear ) , b tse t2 image on uterine proper long axis with reported measurement at scar level ( scar classied as linear ) coil - phased array synergycardio in the supine position . the maximum gradient strength was 40 mt / m , and the maximum slew - rate was 200 tm - 1s - 1 . 
the study protocol included preliminary morphologic spin - echo ( se ) sequences of the female pelvis ( from the renal hila to the pubic symphysis ) , three fast sequences ( single - shot turbo spinechossh - tse ) on the proper long and short axes of the uterus in order to plan a diffusion - weighted sequence for the multiple directions used for dti imaging . 
the para - sagittal plane was acquired considering the body sagittal plane rotated on the long axis of the uterus . parasagittal t2 tse sequence : te 80 , tr [ 2500 , fov 35 9 25 9 15 cm , matrix 256 9 328 , thickness 3 , gap 0.5 , nsa 2 , clear yes . a diffusion - weighted sequence is a fast echo - planar sequence ( ssh - epi ) , where multiple echoes are acquired in order to minimise artefacts from movement [ 32 ]  . 
uterine contractions and intestinal peristalsis can create artefacts that disturb image acquisition and invalidate the results . diffusion - weighted ssh - epi was acquired with spectral fat saturation and half - fourier sampling along 16 directions to obtain tensor imaging ( dti )  . 
sequences were obtained with b = 600 mm2 / s . diffusion - weighted ssh - epi was performed on the parasagittal plane with the following parameters : te 70 ms , tr [ 5000 ms , fov 31 9 31 9 84 cm , thickness 2.1 mm , nsa 2 , epi matrix 140 9 140 , factor 135 , fold - over ap , b = 600 mm2 / s . 3t - mr image post - processing diffusion - weighted ssh - epi images were processed on a dedicated workstation for data pre - processing with medinria software ( medinria v2.0 , medical image navigation and research tool by sophia antipolis , research project asclepios )  . 
diffusion eigenvalues and eigenvectors were estimated in each voxel in order to calculate fractional anisotropy and the apparent diffusion coefcient map ; then , through a proper visualisation tool ( deterministic dti track ; medinria 2.0 ) , bre tracking is performed . 
tracking was continued until the chosen criteria were met ( for example , minimal fractional anisotropy ( fa ) of 0.2 and a maximal angle change of 10 ( cid : 3 ) per integration step )  . 
within 510 min , all bres were appreciable , but if bres of all the voxels that constitute the uterus were used in this fashion , it resulted in no visible structures . 
the dimension and the location of the different regions of interest ( roi ) were drawn on the basis of what we wanted to visualise , and thus to obtain simple to complex structures following different interpretations . 
2 morphological subjective description of the caesarean scar ; comparison between transvaginal ultrasound ( tvus ) and magnetic thickness resonance imaging at 3 tesla ( 3t - mr ) ; myometrial evaluation over the scar , upstream and downstream of the scar . 
to identify longitudinal or circular bres , different roi were placed on the uterus , particularly on the isthmus . maximum distance between the endometrialmyometrial interface of the anterior to the posterior wall of the uterus [ 29 ]  . the feasibility of the techniques described above has been validated in a previous study on nulliparous volunteers and volunteers with previous vaginal or caesarean deliveries [ 34 ]  . image analysis scars were subjectively classied by tvus and 3t - mr as follows : linear , if the endometrial prole was not altered ; retracting , if the endometrial prole was altered or the myometrium was thinned , or in the presence of endometrial dehiscence . 
after a qualitative reconstruction of bre orientation , a quantitative analysis of the number of longitudinal bres that ran through uterine scar ( on the anterior isthmus ) was performed comparing the bres running in the posterior wall at the same level . these quantitative data were compared with the number of cs and the time elapsed between cs . statistical analysis endometrial thickness was measured in both modalities the uterus as the in a median longitudinal plane of statistical analysis was performed using both parametric and nonparametric tests , as required . 
3 longitudinal and circular brers running between the regions of interest ( rois ) using 3t - mr with diffusion tensor imaging ( dti ) with ber tractography postprocessing software . 
the spearman correlation test was used for the analysis of the association between the time elapsed since the cs and the percentage reduction in myometrial bres running through the scar . 
values are expressed as the mean sd or numbers with percentage in brackets or as the median with the iq range . results forty - two women were enrolled in the study . 
these latter received only 3t - mr examination and served as controls . three subjects ( group 1 ) were later excluded after both evaluations because of a retroexed / retroverted uterus . 
one woman ( group 1 ) was unable to continue the 3t - mr due to claustrophobia , and one woman ( group 2 ) refused to undergo 3t - mr examination after receiving a tvus evaluation . 
one woman ( group 2 ) was also excluded after 3t - mr because of artefacts disturbing image acquisition due to an unreported tubal ligation during the second caesarean delivery . 
the characteristics of the different groups are described in table 1 . tvus and 3t mr morphological comparison as reported , uterine scars were subjectively classied as either linear or retracting . 
according to 3t - mr , 12 cases were assessed as linear and 12 cases as retracting . according to tvus , 20 cases were dened as linear and four cases as retracting . 
however , 236 radiol med ( 2015 ) 120 : 228238 of the echo - train length ; moreover , the higher signal - tonoise ratio at 3 t helped in providing better image resolution despite the concomitant snr increase . 
echo - train se has achieved widespread use , being insensitive to breathing artefacts whereas conventional t2 se sequences are lengthy and suffer from patient motion and increased examination time . 
the major disadvantage of echo - train sequences is that t2 differences between tissues , especially at tissue - fat interface are decreased , but this is not to our case since the endometrialmyometrial relevant border was clearly identiable . 
motion due to the contracting bowel can cause image deterioration , and was responsible for the worst artefacts found in our study because no anti - peristaltic agent could be administered as per the study proinuence scar these artefacts did not tocol . 
furthermore , bladder lling can cause major artefacts but only in dti post - processing reconstruction since water protons of the urine can be mistaken by the software as belonging to water bound to myometrial bres , lengthening the postprocessing and re - processing times , so that the tse sequence was performed as the last sequence of the study protocol . 
for all the above reasons , we decided to report the measurements taken on sstse and we suggest that 3t - mr could show a more accurate and reliable measurement both of myometrial thickness and scar morphology than tvus . 
obviously , the true thickness could only be obtained with direct tissue evaluation but that could not be performed in this population of women . a signicant difference between the two methods was found in the measurement of the myometrial thickness at the scar level . 
such thinner myometrial underestimation could be one reason why screening for uterine scar defects or lus thickness by tvus is not very accurate at predicting future pregnancy complications [ 23 , 24 , 3739 ]  . 
for this reason , some authors suggest that tvus evaluation of lus should be combined with other information ( previous single - layer closure of the uterus or inter - delivery interval ) and such a multifactorial system seems to better predict the occurrence of uterine rupture during trial of labour [ 14 ]  . 
the discrepancy of this nding might be explained by population differences or by measurement differences at tvus techniques , although the measurements seem to have been taken in a similar manner as reported in the two studies [ 23 , 25 ]  . 
our study shows a large discrepancy in the mapping of uterine scars between tvus and 3tmr and in terms of morphology ; tvus described 17 % of scars as retracting and 3t - mr 50 % of cases , conrming the large variability in scar description reported in the literature . 
discordance in scar classication ( as linear or retracted ) was found in almost half of the cases , that is , 3t - mr and tvus were concordant in 46 % and discordant in 54 % in morphological scar description . 
the different scar classication at 3t - mr and tvus in our study could be explained by the higher contrast resolution of the 3t - mr technique , as well as the objective nature of mr evaluation compared with the more subjective nature of the tvus examination . 
surely the real - time imaging of tvus favours that are orthogonal to the endometrial cavity , but also mri with its intrinsic multiplanar acquisition potential can obtain proper uterine long and short axis , where morphological evaluation can be easily and accurately performed . moreover , the obtained quantitative data from dti reconstruction support the mr qualitative description . 
no signicant variations were found , especially when measuring scar thickness . the blurring artefact is well known in the literature [ 35 , 36 ] but we used sense in image acquisition , which is known to reduce blurring artefacts due to the shortening the acquisition of sections radiol med ( 2015 ) 120 : 228238 labour in women with pcs and none has been validated prospectively to improve outcomes , as recently summarised by berghella [ 39 ]  . as described in our previous feasibility study [ 34 ] , the mr - dti microstructural analysis conrmed that the highly arranged uterine architecture is not preserved throughout the cs scar . 
quantitative data obtained with 3d tractography reconstruction showed a varying degree of muscle bre disruption within the scarred tissue and a reduction in the number of longitudinal bres that run through the scar . indeed , there was a signicant decrease of longitudinal myometrial bres in the scar tissue in subjects with pcs compared with primiparous women having had a vaginal delivery . 
the mode of delivery of the volunteers in future pregnancies . reconstruction supports unexpectedly , no difference in the extent of bre reduction was found in women having had 1 vs 2 pcs . again , there was no relationship between the number of pcs and the morphology of the scar tissue , with an equal distribution of linear and retracting morphology seen among the two groups . 
this is quite surprising , as previous studies with tvus showed that multiple caesarean sections is a risk factor for larger scar defects [ 25 , 40 , 41 ] and that the rate of uterine rupture is higher in women with increasing numbers of pcs [ 13 ]  . 
in any case , most obstetric guidelines advocate a trial of labour after pcs independently from the number of cs , and our quantitative data seem to support recent studies where also pregnant women with two pcs were admitted , if not contraindicated by other risk factors , to trial of labour [ 39 ]  . one possible reason for this difference is the limited number of patients in our study , as well as the heterogeneity of time elapsed since pcs . 
another explanation could originate from bre tracking reconstruction software , as it is adapted from functional neurology , and it is possible that some of the disrupted muscular bres could be erroneously quantied , which would lead to overestimation . the evidence we found in the amount of bre disruption induced by cs could support the current theory that associates abnormal placental insertions in the subsequent pregnancy of a scarred uterus [ 11 , 40 , 41 ]  . 
anecdotally , the subject with one pcs who went on to develop placenta previa in our series had the highest percentage reduction of longitudinal myometrial bres ( - 95 % ) within the retracting scar of the anterior isthmus region . in conclusion , the results of our study challenge the idea that tvus could be the gold standard for the assessment of lus or scar defects in women with pcs . 
they comprised histopathologically proven liver metastasis of colorectal ( 19 cases ) and gastric ( 10 cases ) adenocarcinoma without local recurrence at the site of the previously resected primary tumour , along with 17 subjects with haemangioma . 
gholamrezanezhad department of radiology , case medical center , case western reserve university , cleveland , oh , usa e - mail : ali.gholamrezanezhad@gmail.com than higher those with assessment using multislice computed tomography to calculate total volume of hepatic lesions . results the mean dpi of patients with colorectal ( 36 2 % ) and gastric ( 39 6 % ) metastasis was signicantly haemangioma ( 14 2 % ) ( both p \ 0.001 ) , whereas metastatic groups did not exhibit any difference in terms of mean dpi . statistically signicant correlations were found between dpi values and calculated total volume of lesions in patients with colorectal and gastric metastasis ( r = 0.55 , p = 0.01 and r = 0.85 , p = 0.002 , respectively ) while this correlation was not demonstrated in the haemangioma group . 
worldwide , over one million individuals will develop colorectal cancer each year and the disease - specic mortality rate is nearly 33 % in developed countries [ 2 ]  . 
almost 70 % of colorectal cancer patients 172 radiol med ( 2015 ) 120 : 171179 experience liver metastasis during the course of disease [ 3 ]  . gastric cancer is also currently the fourth most common malignancy in the world and the second leading cause of cancer death in both sexes [ 4 ]  . 
at the time of diagnosis , 35 % of gastric cancer cases present with evidence of distant metastases and 414 % have metastatic disease to the liver [ 5 , 6 ]  . a growing number of studies suggest that altered liver haemodynamics can aid the detection of hepatic metastasis even in the absence of overt focal lesions [ 711 ]  . 
previous studies using colour doppler ultrasound have shown that the doppler perfusion index ( dpi ) as the ratio of hepatic arterial to total liver blood ow can detect liver metastasis [ 7 , 8 ]  . 
a relatively higher contribution of hepatic artery to total liver blood ow in patients with colorectal and gastric metastases has been stated in previous studies [ 9 , 10 ]  . 
the potential diagnostic ability of dpi for detection of hepatic involvement has been the main interest of these studies , especially focusing on occult metastatic lesions , while investigation of any relationship between liver perfusion indices and the size of lesions may provide valuable information for the management of patients with known liver metastasis . 
in other words , as dpi alteration can help to detect occult metastases , determination of how this index might be affected by the size of overt metastatic lesions could be of value for assessment of treatment response in the patients followto the best of our knowledge no previous study has evaluated dpi changes in relation to the total volume of focal liver lesions either benign or metastatic . 
to investigate this relationship , a comparison between haemodynamic measures of benign and metastatic lesions with similar ultrasound appearance could also be useful assess the diagnostic value of dpi to differentiate them . haemangioma as the most common benign hepatic lesion which is increasingly being discovered incidentally in routine ultrasound [ 13 ] can mimic hyperechoic liver metastases from colorectal or gastric malignancies . 
patients with metastasis were deemed to have had a potentially curative resection of the primary tumour , with a median postoperative period of 13 months ( range 546 months )  . 
they met the following inclusion criteria : ( 1 ) histopathologically proven diagnosis , ( 2 ) no history of chemotherapy , ( 3 ) no gross local recurrence at the site of resected primary tumour . 
the subjects with liver haemangioma were included according to the following criteria : ( 1 ) typical appearance of haemangioma on contrastenhanced triphasic ct scan as peripheral nodular enhancement and delayed central lling , least 18 months of follow - up without signicant change in size . the local ethics committee of our institution approved the study protocol , based on the ethical principles of human research and experimentation . 
all measurements were done by a single radiologist ( a.h. ) with more than 10 years experience in this eld who was blinded to the demographic data of the patients . 
the common hepatic artery was found in its longitudinal axis by a transverse scan at the epigastriuthe doppler cursor was placed over the lumen as close to the origin as possible to calculate the time average velocity of the hepatic artery over four cardiac cycles . 
1 measurement of hepatic arterial blood ow in a 52 - yearold male patient with liver metastases due to adenocarcinoma of sigmoid . a three hyperechoic liver metastases ( arrows ) in segment four and eight on ultrasound examination . 
c measurement of the hepatic arterial time average velocity over the four cardiac cycles ( 3358.8 cm / min ) by multiplying mean velocity ( 55.98 cm / s ) by 60 s . 
subjects were asked to hold their breath during measurements . values of hepatic arterial and portal venous ow were calculated from the product of the time average velocity and the cross - sectional area for each vessel . 
dpi was determined as the ratio of hepatic arterial ow to total liver blood ow . according to the previous studies dpi values of 30 % and higher were considered abnormal [ 10 , 11 ]  . ct volumetric measurement total volume of the lesions for each patient was calculated using a 16 - detector - row ct scanner ( somatom , emotion , siemens ) by a single experienced radiologist ( a.r. ) who was blinded to the subjects characteristics and clinical data . 
intravenous nonionic contrast [ ultravist , iopromide ( 300 mi / l ) , schering , berlin , germany ] was administered at an injection rate of 3 ml / s ( maximum total amount of 150 ml , depending on body weight )  . 
for each examination , 5 - mm - thick postcontrast slices were taken during the venous phase 70 s after the contrast agent had been injected to determine the exact delineation of the lesions contour . 
 ( bd ) multislice computed tomography ( ct ) scan in the portal venous phase ; multiplanar reformation in axial ( a ) , sagittal ( b ) and coronal ( d ) views with a slice thickness of 1.5 mm for better delineation of the lesion ( thick arrows ) and its contour . 
to explore the frequency of abnormal dpi values in studied groups , the odds ratio ( or ) [ 95 % condence intervals ( ci ) ] and p value for v2 were calculated . 
correlations between dpi values and total volume of the liver lesions were assessed using pearson correlation coefcient . finally , to explore how the increment of volume can affect dpi values , simple linear regression analysis was applied . a p value of 0.05 or less was dened as signicant . 
there was no signicant difference between all three groups in terms of mean total volume of the hepatic lesions . as shown in table 2 , the mean hepatic arterial blood ow and dpi values were signicantly higher in patients with colorectal and gastric metastasis than in the haemangioma group ( p = 0.001 and p \ 0.001 , respectively ) , while no signicant difference was demonstrated between patients with gastric and colorectal metastasis . 
in the current study , we demonstrated that an increase of total volume of metastases is accompanied by a statistically signicant increment in dpi values , which , to our 176 radiol med ( 2015 ) 120 : 171179 table 2 mean values for liver haemodynamic parameters and volumetric measurements in all studied groups haemangioma ( n = 17 ) colorectal mets . 
we also found that dpi could be of great value to differentiate haemangioma from hyperechoic liver metastasis . in apparently disease - free liver of patients with gastric [ 10 ] and colorectal malignancies [ 15 ] after at least 4and 5 - year follow - up , respectively . in 1991 , leen and colleagues [ 7 , 8 ] introduced dpi as a valuable technique for detection of liver metastasis . 
they suggested that dpi is more sensitive than intraoperative ultrasound to predict occult colorectal liver metastasis [ 9 ] ; likewise , the higher sensitivity of dpi was demonstrated in comparison with ultrasound ( us ) , computed tomography ( ct ) and laparotomy for detection of hepatic metastasis from colorectal malignancies [ 11 ]  . 
this potential ability of dpi was also supported practically when they predicted occult metastasis increased arterial perfusion has been shown using ct perfusion imaging in patients with known metastatic disease . 
 [ 12 ] found that ct measurements of hepatic enhancement , ct perfusion and doppler perfusion indices are broadly equivalent to show increased hepatic arterial circulation in patients with breast and colonic metastasis . 
the clinical value of perfusion magnetic resoimaging has also been described which nance ( mr ) enables dynamic whole - liver three - dimensional imaging without the risks of radiation and therefore seems to be the further most promising future approach . 
however , radiol med ( 2015 ) 120 : 171179 challenges in exploration of optimal techniques for faster image higher - resolution liver processing have remained , which have to be optimised [ 16 ]  . imaging and subsequent to explain the haemodynamic changes of the liver in patients with hepatic metastasis several hypotheses have been suggested . 
another possible mechanism could be a decrease in portal venous ow which could be caused by mechanical obstruction of intrahepatic portal branches by tumoural bulk [ 18 ] or role of circulating vasoconstrictive mediators produced either by tumoural tissue or as part of host response [ 19 ]  . 
 [ 20 ] suggested that the primary tumour makes a relatively minor contribution in inducing elevated dpi in patients undergoing curative resection for colorectal cancer reecting the role of occult metastases and associated host response . by volumetric assessment of focal liver lesions and adjustment of mean total volume between all groups , we tried to eliminate the confounding effect of bulk of hepatic lesions for better evaluation of dpi in patients with different types of liver masses . 
a positive correlation between hepatic arterial blood ow and increased intrahepatic metastatic bulk was also detected . as a matter of fact , proliferation of tumoural tissue could be accompanied by internal necrotic changes which do not necessarily result in higher hepatic arterialisation . 
estimated total volume of the liver using ct scanning to express haemodynamic parameters relative to liver size , and showed decreased total liver blood ow relative to the liver volume in colorectal hepatic metastasis in addition to the reduced portal ow and elevated arterial ow and dpi values . 
they concluded that a humoural mediator mechanism caused portal ow reduction by increasing mesenteric vascular resistance which should be accompanied by an additional intrinsic hepatic haemodynamic event [ 21 ]  . 
they reported that even by isolated very small groups of metastatic foci haemodynamic changes could be triggered prior to hepatocyte involvement due to some kind of humoural tumour effect [ 22 ]  . 
 [ 23 ] revealed intrahepatic microhaemodynamic events in mice prior to the development of visible colorectal cancer metastases suggesting upregulation of endothelial receptors with reduction of sinusoidal blood ow , whereas during tumour growth , portal ow reduction was found resulting from mechanical tumour compression and / or peritumoural vessel lumen narrowing due to leukocyte adherence . in the present study , we could not demonstrate a signicant decrease in portal ow in metastatic group , and portal ow was not signicantly correlated with volumetric measurements . 
emphasising the role of the hepatic artery in liver metastasis has been the point of interest in previous studies , but there are published data focusing on the contribution of the portal vein , either directly or through the sinusoids in the blood supply of hepatic metastases [ 24 ]  . 
most of the studies dealing with haemodynamic alterations in liver metastasis might have neglected the importance of arterioportal anastomoses by accentuation of investigations in reduced portal ow . animal models are decient because they only examine small metastatic foci , which is usually in contradistinction to larger size of human tumours . 
morphological assessment of colorectal cancer liver metastases by scanning electron microscopy has indicated contribution of portal vein through sinusoidal connections at the periphery of metastatic lesions [ 25 ]  . in current daily practice of liver us , there are many focal liver lesions with similar ultrasonographic appearance . 
this has been a matter of concern to increase the probability of correct judgement about the malignant or benign nature of a focal hepatic mass without recommendation of unnecessary further imaging modalities . 
so , we also focused on the potential role of dpi to discriminate metastatic from benign liver lesions with equivalent sonographic characteristics . our results amplify the diagnostic value of dpi to differentiate a hyperechoic metastasis from a haemangioma . signicantly increased dpi values , hepatic arterial blood ow and cross - sectional area of the hepatic artery in metastatic group were in accordance with ndings of earlier clinical studies supporting the concept of hepatic arterialization in liver metastasis [ 711 ]  . 
unlike previous publications [ 7 , 8 ] , we could not conrm a statistically signicant decrease in portal venous ow in the metastatic group , although a signicant reduction in cross - sectional area of the portal vein in metastatic subjects may be noteworthy . there are also limited studies that could not demonstrate signicantly diminished portal blood ow in patients with liver metastasis [ 26 ]  . what could be the practical applications of our ndings in this study ? firstly , described ndings about volumerelated alterations of dpi values in hepatic metastasis can 178 radiol med ( 2015 ) 120 : 171179 open a new era of research which may help clinicians to monitor reduction in volume of tumour bulk indirectly by regular assessments of dpi values as an indicator of treatment response . 
secondly , the dpi can be of great value to differentiate haemangioma as the most common benign liver tumour from sonographically similar hyperechoic metastases which may reduce further diagnostic work - up , considering that the costs of advanced cross - sectional imaging are high and rapidly growing . the ndings of our study should , however , be interpreted with some limitations . 
no gross internal necrosis was found in the evaluated hepatic lesions of this study ; however , we caution the readers that even microscopic necrotic foci of tumours might interfere with volume - based changes of dpi values . in conclusion , dpi changes are directly correlated with the total volume of the metastatic lesions ; dpi measurement could be a valuable method to distinguish liver haemangioma from hyperechoic metastasis of gastrointestinal malignancies . 
the location of the hmcas , the extension of the ischaemic lesion and its prognostic value were also assessed . materials and methods the ct examinations of 654 patients with symptoms related to acute cerebral stroke were retrospectively reviewed . 
patients were divided into three groups according to the hmcas site ( m1m2m3 ) and the alberta stroke program early ct score ( aspects ) on dw - mri was calculated . 
the aspects average score in 41 patients , was correlated with the national institutes of health stroke scale ( nihss ) and modied rankin scale ( mrs ) at 3 months . results the presence of hmcas was conrmed ( 71 % sensitivity ; 100 % specicity ; interobserver reliability k , 84 % )  . 
after hmcas was found to be independently associated with a poor outcome ( mrs [ 2 ) at 3 months after adjusting for age , nihss on admission , risk factors and aetiology of stroke . conclusions our study demonstrated that hmcas obtained with multidetector ct can be detected in more than 70 % of patients with large acute ischaemic lesion and it is an unfavourable prognostic sign . regression logistic keywords multidetector ct ( cid : 2 ) acute cerebral ischemia ( cid : 2 ) hyperdense middle cerebral artery ( cid : 2 ) diffusion - weighted images a . 
pierallini department of radiology , ircss san raffaele pisana , rome , italy in the early hours following the onset of symptoms related to acute cerebral ischaemia noncontrast computed tomography scan ( ct ) can be normal and / or show subtle signs related to cytotoxic oedema ( early hypodensity ) or vessel occlusion ( hyperdensity of middle cerebral artery sign : hmcas )  . 
hmcas is a well - known sign of cerebral ischaemia in the middle cerebral artery ( mca ) area [ 15 ] with specicity close to 100 % and sensitivity ranging from 27 to 54 % [ 47 ]  . 
partial volume effects , haemoglobin levels , radiologists experience and thickness of ct slices can explain the low - sensitivity values . radiol med ( 2015 ) 120 : 222227 the presence of hmcas provides strong evidence of mca occlusion although the thrombus extent and the severity of vessel stenosis or occlusion are not directly detectable . 
it is usually correlated to severe clinical status and worse prognosis [ 813 ] and often supported by cardioembolic pathology [ 10 ]  . in some instances , the diagnosis of ischaemic stroke cannot be clear from the clinical ndings and any radiological sign supporting this suspicion , including hmcas , can be helpful . the study purpose was to determine the sensitivity and specicity of hmcas obtained by multidetector ct ( within 4.5 h after onset of symptoms ) in predicting acute cerebral ischaemia using diffusion - weighted ( dw ) magnetic resonance imaging ( mri ) ( performed within 12 h after onset of symptoms ) as the reference standard . 
to evaluate the prognostic value of the hmcas , we also correlated its location along the artery with : the alberta stroke program early computed tomography score applied to mr images ( aspects ) [ 11 ] the national institutes of health stroke scale ( nihss ) [ 12 ] at baseline the modied rankin scale ( mrs ) [ 13 ] at 3 months . two independent observers evaluated the ct scans . 
sensitivity , specicity and interobserver reliability was evaluated for all phases . phase i phase ii patients were randomised and compared to a control group consisting of 175 patients without acute ischaemic lesions . this entire group ( 350 patients ) was blindly evaluated for hmcas ( independently from its extent and location )  . 
this evaluation was performed by reading the partition ct images with the possibility ( not obliged ) of image reformatting on a dedicated console ( ge advantage window )  . materials and methods we retrospectively reviewed the ct examinations of 654 patients who came to the emergency department from january 2008 to december 2011 with stable or worsening symptoms possibly related to an acute cerebral stroke . the same neuroradiologists were asked to analyse the ct images of 130 patients in whom subsequent dwi conrmed mca stroke while also being aware of the clinical symptoms ( side of decit and / or aphasia )  . 
they were also asked to identify the site of hmcas ( from m1 to m3 )  . radiological evaluation phase iii all examinations were acquired with a 16 - slice multidetector ct scanner ( helical scan acquisition time of 11 s , 140 kw , 493 ma , acquisition thickness 1.25 mm ) without intravenous contrast medium . patients with lacunar or cortical ischaemic lesions \2.5 cm at dw - mri were excluded and the hmcas was sought on the remaining 56 patients . 
for each patient with hmcas , the aspects score on dw - mri was calculated . inclusion criteria were ct examination within 4.5 h from the onset of symptoms , no ct evidence of other pathologies or cerebral haemorrhage follow - up mri with dw sequences ( 1.5 tesla siemens sonata , erlangen , germany ; tr 3000 , te 84 , b factor = 1 , 000 ) within 12 h from onset of symptoms to conrm the presence of the recent cerebral ischaemic event . exclusion criteria were evident hypodensity on ct scan . clinical evaluation demographic characteristics , risk factors , ischaemic event aetiology according to the toast ( trial of org 10172 in acute stroke treatment ) classication [ 14 ] , emergency treatment and secondary prevention were considered for each patient . 
interobserver reliability was k = 84 % . radiol med ( 2015 ) 120 : 222227 phase ii reading the ct scans of those patients ( n = 130 ) with mca area involvement with awareness of the symptoms led to the following results : sensitivity 26 % ( reader 1 ) , 31 % ( reader 2 ) , interobserver reliability : k = 84 % . reading the ct scans of the 56 patients with mca area ischaemia greater than 2.5 cm ( thus excluding cortical table 1 baseline patient characteristics lesions and lacunar infarcts ) led to the following results : sensitivity 60 % ( reader 1 ) , 78 % ( reader 2 ) , interobserver reliability : k = 85 % . consensus of the three neuroradiologists conrmed the presence of hmcas in 41 patients ( sensitivity : 71 % )  . 
the radiological ct nding which excludes patients for thrombolysis is a hypodensity over 1 / 3 of the mca area . vascular hyperdensity at baseline ct ( mainly the mca ) is a sign of thromboembolic occlusion of the vessel . 
it is present in percentages ranging from 40 % up to 60 % of patients with acute stroke and has a highly signicant predictive value ( around 95 % )  . 
the medical literature agrees that hmcas is highly specic ( almost 100 % ) but with a low or variable sensitivity ( around 30 % ) [ 4 ]  . 
it is well known that some patients do not show the hmcas despite angiographic conrmation of vessel occlusion [ 9 ]  . this can be related to an early fragmentation of the embolus for physiological thrombolysis and early recanalization [ 18 ]  . 
on the other hand , false positives may be due to vessel calcications , bromide therapy , use of cocaine and high haematocrit [ 4 ]  . according to somford et al . 
 [ 19 ] , the ct sensitivity for this sign also depends on thickness of ct scan and on delay of the examination relative to the onset of symptoms . pressman [ 2 ] and schuierer [ 20 ] demonstrated that using a 10 - mm thickness led to mca hyperdensity underestimation . 
this percentage can be achieved when small lesions ( such as lacunae ) are excluded and when knowledge of symptoms is available . few studies [ 19 ] analysed the relationship between the site of hmcas and the prognosis . 
in our study , proximal hmcas was associated to the lowest aspects values ( at dw - mri ) , while more distal hyperdensity ( m2m3 ) resulted in higher aspects values . 
 [ 21 ] demonstrated , using angiographic studies , that systemic thrombolytic therapy is more effective for distal occlusions , with rates of complete recanalization of 48 % , compared to proximal occlusions ( more likely showing hmcas ) whose rate of recanalization is 38 % . the main limitations of this study are its retrospective design and the absence of an angiographic conrmation of ct hyperdensity . 
we set out to ascertain the possibility that plain ct could detect hmcas in patients with acute stroke ( in different radiological and clinical conditions ) and to correlate those ndings with clinical status and prognosis . 
whether hmcas could impact subsequent treatment is unknown and is beyond the results of this study . radiol med ( 2015 ) 120 : 222227 conclusions our study demonstrated that hmcas can be detected in more than 70 % of patients with large acute ischaemic stroke ( [ 2.5 mm and excluding lacunae ) when clinical symptoms have been reported to the radiologist . 
although hmcas has no impact on treatment decision making , in our opinion , this sign should always be investigated and reported in conjunction with the reading of a plain ct for several reasons . 
we sought to evaluate the tissue distribution of 131i - hyp in a large animal model and to explore the theranostic utilities of 131i - hyp after radiofrequency ablation ( rfa )  . materials and methods this animal experiment was approved by the institutional ethics committee . 
ni ( & ) radiology section , university hospitals , ku leuven , herestraat 49 , 3000 leuven , belgium e - mail : yicheng.ni@med.kuleuven.be distributions of 131i - hyp were monitored dynamically by single - photon emission computed tomography / computed tomography ( spect - ct ) , gamma counting , autoradiography , and uorescent and light microscopy at different time points up to 14 days . 
131i - hyp gradually accumulated in the rfa - induced necrosis with a peak concentration occurring within 2 days and lasting over 2 weeks as visualised by in vivo spect - ct and ex vivo autoradiography and uorescent microscopy , and quantied by radioactivity and uorescence measurements . accumulation of 131i - hyp was low in both the necrosis centre and normal liver tissue . 131i - hyp showed persistent high afnity to conclusion hepatic thermo - coagulative necrosis , but only a transient uptake by normal liver in dogs . 
necrosis caused by rfa could be indicated by 131i - hyp on nuclear imaging , which suggests a supplementary measure for tumour detection and therapy . keywords hypericin ( cid : 2 ) necrosis ( cid : 2 ) radiofrequency ablation ( cid : 2 ) radiopharmaceutics introduction radiofrequency ablation ( rfa ) has gained broad applications in tumour therapy owing to its minimally invasive features and denite effects . 
the temperature in the centre of the target can reach above 60 ( cid : 3 ) c and usually results in an immediate 214 radiol med ( 2015 ) 120 : 213221 coagulation necrosis zone with the diameters of 15 cm depending on the exact energy delivered . 
even if this passive damage was not present , apoptosis can be evoked . furthermore , the heat - treated tumour cells may activate the antitumour immunoreactivity of the organism to kill remnant live tumour cells [ 1 , 2 ]  . in clinical practice , due to the various sizes , shapes , and densities of the tumours , often rfa cannot completely eradicate the whole tumour . 
thus tumour recurrence after rfa is closely linked to the residual malignant cells . dening the exact boundary between the malignant and normal tissues still remains a real challenge for rfa [ 2 , 3 ]  . despite the wide use of imaging techniques such as ultrasound ( us ) , computed tomography ( ct ) , and magnetic resonance imaging ( mri ) , they are still not robust enough to discriminate the necrotic from unaffected tissues after rfa [ 25 ]  . hypericin ( hyp ) , a small natural molecule present in plants of the hypericum genus , belongs to the highly reduorescent polycyclic aromatic naphthodianthrones . 
this makes radiolabelled hyp not only to function as a marker for tumour diagnosis but also help to eradicate the viable tumour cells around the necrotic centre through the lethal radiation emitted from the radiolabelled isotopes [ 10 , 11 ]  . 
pilot studies have demonstrated the potential use of hyp in tumour dualtargeting treatment and diagnosis [ 814 ]  . previously , it was reported that hyp tended to concentrate in the necrosis while normal tissues contained much smaller amounts of hyp in animal models of hepatic and myocardial infarction [ 9 , 10 ]  . 
recently , however , by using rabbit models to study the dual - targeting anticancer therapy , we found that a large amount of hyp could be detected in the normal liver , which is not in accordance with what was found in the rat and mouse models [ 13 , 14 ]  . thus , we speculated that the tissue distribution of hyp might be species - dependent among different animals . 
iodine - 131 labelled hyp ( 131ihyp ) was prepared and intravenously injected , and its systemic and regional distributions were recorded by radioactive counting , autoradiograpy , and uorescence microscopy . 
as previously described [ 12 , 13 ] , lugols solution was home prepared for oral intake to block radioiodine uptake . hyp of 2 mg was dissolved in 2 ml dmso and mixed with 300 lg iodogen . 
131ihyp : iodine - 131 - labelled hypericin ; autorx autoradiography , ct computed tomography ; iv intravenous ; n number of animals , rfa radiofrequency ablation , tgc tissue gamma counting , spect single - photon emission computed tomography connected with rf generator ( radionics cool - tiptm rf ablation system , manseld , ma , usa ) , an 18 - gauge electrode with a 1 cm uninsulated tip was inserted into the right liver lobe . 
under temperature control mode ( 90 ( cid : 3 ) c ) , rf current was delivered into the liver for over 20 s and stopped when the temperature reached 90 ( cid : 3 ) c . 
after the procedure , the abdominal incision was closed by layered sutures . spect / ct imaging the canines were scanned consecutively with spect - ct ( symbia t2 , siemens , malvern , pa , usa ) on day 1 , 2 , 5 , 9 , and 14 after injection of 131i - hyp , using a high energy and low resolution collimator . 
the imaging acquisition parameters were : energy peak of 340 kev 10 % , magnication of 1.00 , matrix of 128 9 128 , and acquisition counts of 300 k ( 64 projections with 10 s for each )  . 
the iteration was 8 and gaussian was 6 mm . autoradiography liver tissue blocks were sampled , embedded in medium ( tissue - tek medium , miles inc . , elkhart , usa ) , frozen in liquid nitrogen , cryostat sectioned into 50 and 5 lm - thick slices , and thaw - mounted on standard glass slides . for macroscopic autoradiography , the 50 lm section slides were exposed for 24 h to a high performance storage phosphor screen , which was then scanned by molecular imager fx ( bio - rad , shanghai , china )  . 
the radioactivity values were calculated by quantity one software ( biorad , shanghai , china ) peripheral necrosis , and the normal liver tissues . the necrotic centre , for microautoradiography , in a dark room , the 5 lm section slides were dipped in type iv nuclear emulsion , stored at 4 ( cid : 3 ) c for 57 days of exposure , developed and then counterstained with haematoxylin and eosin ( h&e ) light microscope . photographed examination under fluorescence microscopy the cryostat 5 - lm sections were also examined by uorescence microscopy ( nikon eclipse 80i , nikon , melville , ny , usa ) with the exciting wavelength of 510560 nfor necrotic centre , peripheral necrosis , and normal intensities of every eight regions of interest ( rois ) were recorded by nis - elements d software ( nikon , melville , ny , usa )  . 
after subtraction of the background intensities , intensity the uorescent values were compared among different regions . the uorescent liver , histopathology histopathological examinations were conducted in accordance with what has been previously reported [ 12 ]  . 
eventually , h&e stained tissue slices were examined for conventional light microscopy and photomicrography . tissue radioactivity counting twenty - ve canines ( n = 5 for each time point ) were killed on day 1 , 2 , 5 , 9 , and 14 after administration of 131ihyp by intravenous injection of 2030 ml of 10 % potassium chloride . 
a spect static image taken on day 2 after 131ihyp injection displays the tracer distribution as hotspots at rfainduced necrotic lesion ( red arrow ) , the gallbladder ( green arrow ) and the gastrointestinal regions ( brown arrow )  . 
tissue relative radioactivity was calculated as described elsewhere [ 15 ]  . results general conditions all canines survived the anaesthesia , surgery , rfa , and imaging procedures without any drug administration - related deaths or side effects . 
after recovery from rfa and surgery , all dogs did not show weakness , loss of mobility or appetite , and decrease of body weight . statistical analysis spect - ct imaging numerical data were expressed as mean sd . 
nevertheless , necrosis - to - liver activity ratio kept constantly high whether the peripheral or central part of necrosis was taken into account , resulting in ratios of 40 and 10 times on day 14 , respectively ( table 1 )  . 
b corresponding low - power uorescent microscopic view of the same liver tissue section reveals intense red uorescence mainly at the peripheral necrosis ( pn ) due to the easy access and afnity of 131i - hyp to coagulative liver necrosis . c corresponding macroscopic autoradiographic image conrms higher amount of radioactivity ( 131i - hyp ) present in the region of peripheral necrosis ( pn )  . 
a lack of uptake at the necrotic centre ( cn ) was due to poor access resulting from vascular destruction by rfa . d corresponding image of h&e - stained histomicrograph ( original magnication 950 ) superimposed with microscopic autoradiography displays a larger amount of dark silver grains ( reecting the presence of 131i - hyp ) mainly at the peripheral necrosis ( pn ) , corroborating the above ndings ( ac ) of the necrosis centre during the whole test period . 
peripheral necrosis tissue was the only region that was abundant of 131i - hyp during the whole experimental period ( p = 0.02 ) with peak absorption on day 2 . postmortem morphological ndings the ndings from macroand microscopic autoradiography , uorescent microscopy and histopathology were highly consistent as illustrated in fig . 
5 comparison of the uorescence intensity ratios between different regions in the liver by phosphor screen imaging data . ( cn ) the necrosis centre ; ( pn ) peripheral region of the necrosis centre . 
in the liver parenchyma , these grains were also enriched in the glissons capsule especially near small bile ducts and the portal veins . discussion as one of its multiple medicinal utilities , hyp has been intensively studied as a tumoritropic photosensitiser in photodynamic therapy ( pdt ) where it was found to condense mostly in mitochondria and lysosome [ 16 ]  . 
this property has been exploited for developing a dual - targeting pan - anticancer theragnostic strategy where a vascular disrupting agent ( vda ) is synergistically combined with 131i - hyp to improve cancer management [ 814 ]  . 
rfa is a minimally invasive necrotising method and has been successfully applied in the treatment of solid malignancies including primary and metastatic liver cancers , although incomplete ablation still remains a concern for tumour relapse [ 18 ]  . in this study , we evaluated the biodistribution of 131ihyp in different tissues or organs and the targetability of 131i - hyp to thermal coagulative necrosis in canines as a large animal model after intrahepatic rfa . 
in contrast to an early quick hepatic uptake and clearance of 131i - hyp in rats and mice [ 14 , 17 ] , early uptake and slow hepatic clearance of radioiodinated hyp were observed in rabbits by our group and documented by the literature [ 19 , 20 ]  . 
thus , the present study becomes particularly important as an intermediate step towards future clinical trials of 131i - hyp mediated anticancer strategy . the spect - ct results indicated that 131i - hyp mainly accumulated in the gallbladder and the gastrointestinal the beginning , suggesting that 131i - hyp was tracts at mainly taken up by hepatocytes and quickly excreted through bile into faeces . 
limited by the lower spatial resolution , spect alone could not depict the necrosis precisely , which has now been improved by combined dual modalities of spect - ct as shown in the present study . gamma counting results demonstrated that the peak concentrations of 131i - hyp occurred within one day and then constantly decreased in all tissues or organs as shown in table 1 . 
technically , it was uneasy to accurately sample necrotic tissue by totally excluding the non - necrotic parts , so the real radioactivity ratios between the necrosis and the normal tissue might be even higher than the presented ones . indeed , the necrosis avidity of 131i - hyp could be qualitatively conrmed by macroand microscopic autoradiography as well as uorescent and light microscopy and their quantitative outcomes . 
while histopathological results showed that a distinct boundary could be marked by 131i - hyp , the ratios of necrosis to normal liver calculated by radioactivity counting and by phosphor screen autoradiography were consistent and mutually supportive . 
on microscopic autoradiography , most of the particles developed due to 131i - hyp accumulation were condensed along the boundary between the normal and the necrotic tissues . the conned dissemination of 131i - hyp to the region where the normal and the necrotic tissues were bordered suggests that rfa caused blood vessel damage and restricted access for 131i - hyp to enter the whole necrotic regions , especially the necrotic centre . 
rfa results in necrosis and inammatory inltration in local regions and such reactions last for days , weeks , or months as tissue recovery events after injury [ 15 ]  . 
during this process the degraded necrotic components will be absorbed by phagocytosis and replaced by granulation tissues which 220 radiol med ( 2015 ) 120 : 213221 eventually become brosis . 
secondly , with a higher therapeutic dosage , 131i - hyp helps to irradiate remnant viable tumour cells by beta particle crossre radiation , meanwhile visualising the process by spect - ct . although to a lower extent and shorter duration in comparison with that in the necrosis , the non - necrotic tissues especially the liver , lung , spleen , and intestines also took up 131i - hyp , which deserves cautious attention in developing this approach . in a preliminary dosimetry study , the thyroid , lung , and intestines were regarded as dose - limiting organs with potential overexposure of radiation [ 24 ]  . 
the lung uptake can be minimised by improving the formulation of 131i - hyp [ 25 ] and overall unnecessary radioexposure can be signicantly reduced by efcient bile drainage during the rst hours to days after 131i - hyp administration [ 26 ]  . to our knowledge , this is the rst study where the afnity of 131i - hyp to necrosis was clearly evidenced in canine models with liver rfa . 
for instance , we did not directly evaluate the anticancer theranostic potentials of 131i - hyp due to in dogs . hardly available tumour burden models besides , the detailed mechanisms underlying the afnity of hyp to necrosis were not addressed in this study . 
all these leave room for further investigational endeavors . in conclusion , we demonstrated a high afnity of 131ihyp to rfa - induced liver coagulative necrosis in dogs . similar to the ndings in rodents but dissimilar to those in rabbits , normal liver in dogs showed only transient uptake of 131i - hyp , which appears favourable for further clinical development of this radiopharmaceutical . 
tumour necrosis caused by rfa can be targeted by 131i - hyp , which may help therapeutic assessment by nuclear imaging and adjuvant irradiation of remnant cancer cells to improve the efcacy of the rfa therapy . acknowledgments this study was partially supported by national natural science foundation of china ( 81201169 ) , national high technology research and development program of china ( 2012aa022701 ) and liaoning s&t project ( 2012225016 )  . 
this review summarises the technical and interpretation key points of perfusion cardiac magnetic resonance scan , the clinical indications , the most recent available literature about its diagnostic performance and prognostic value , and how perfusion cardiac magnetic resonance compares with other noninvasive techniques . keywords cardiac magnetic resonance perfusion imaging ischaemia coronary artery disease r . 
thomas hospital , london se1 7eh , uk introduction cardiac magnetic resonance ( cmr ) allows noninvasive assessment of cardiac anatomy , function , structure , and ischaemia without ionizing radiation . 
perfusion cmr ( pcmr ) has been developed and optimised in the past decade , and its safety profile and increasing availability have made pcmr one of the diagnostic modalities of choice for the detection of myocardial ischaemia . 
perfusion cmr has been validated against other diagnostic methods such as quantitative coronary angiography ( qca ) , noninvasive diagnostic techniques ( single photon emission computed tomography , spect ; positron - emission tomography , pet ) , and invasive haemodynamic measurements ( fractional flow reserve , ffr )  . 
the aim of this article is to review the evidence currently available in the literature on pcmr , summarising the acquisition protocols , interpretation criteria , clinical indications , and the most recent data about its diagnostic and prognostic value . physiology of the coronary circulation heart rate ( hr ) , wall stress and contractility are the main determinants of myocardial oxygen consumption . 
1 coronary autoregulation is an efficient mechanism in compensating the effects of fixed epicardial coronary stenoses on myocardial perfusion : an epicardial artery stenosis is balanced by a reduction of the downstream arteriolar vessel resistance . 
during stress , the arteriolar vessel resistance beyond a stenosis are already low , while those beyond the normal epicardial vessels may significantly reduce pointing out the low perfusion distal to a intermediate or severe epicardial artery stenosis mbf is defined coronary flow reserve ( cfr ) [ 2 ]  . 
there is a physiological transmural gradient of oxygen demand in the left ventricle ( lv ) , as the endocardial layer at rest consumes more oxygen than the epicardial layer due to higher metabolis in the case of increased cardiac workload a transmural increase of cardiac contraction is matched by a proportional increase of mbf and the transmural epicardialendocardial perfusion gradient disappears . 
at rest , 8090 % angiographic stenoses may have normal perfusion [ 3 ] , making perfusion imaging at rest not useful alone for the detection of coronary artery disease ( cad )  . 
 while these mechanisms are usually elicited by increased myocardial metabolism following physical efforts not easily reproducible in the mr scanner , vasodilator drugs ( adenosine , dipyridamole , regadenoson ) are administered to stimulate a hyperaemic state and reproduce any mbf abnormalities in perfusion territories supplied by significantly diseased vessels . functional versus anatomical assessment of stenosis the anatomical assessment of cad by coronary angiography ( ca ) and multidetector computed tomography coronary angiography ( mdct - ca ) does not offer any direct information on their haemodynamic significance . 
therefore , the anatomical diagnostic methods have progressively lost their status of standard of reference ( sor ) for cad evaluation [ 6 ] , and have been superseded by functional methods . 
the invasive assessment of ffr ( ratio between the maximal coronary blood flow in the presence of stenosis and the maximum achievable blood flow if all epicardial obstructions were absent ; normal values > 0.8 ) is currently considered the sor for functional cad assessment [ 7 ]  . 
2 progression of the ischaemic wave front ( modified from [ 5 ] ) through the myocardial wall over time in presence of flow - limiting coronary artery stenosis : an epicardial vessel stenosis determines a reversal of the transmural perfusion gradient , with higher epicardial perfusion and the onset of subendocardial ischaemia . 
proportionally with the severity of the coronary lesion and of the mismatch between oxygen demand and supply , the subendocardial ischaemia may extend to the mid - myocardial and epicardial layers fig . 
the gd first - pass assessment allows to follow the gd through the ventricular cavities and detect the following left ventricular intra - myocardial wash - a thin subendocardial pd ( arrowhead ) is appreciable in the inferior wall ( mvd ) , causes a slower intra - myocardial gd wash - this is detectable on qualitative analysis , visually assessing the myocardium for regions of lower signal intensity ( si ) relative to normally perfused segments during hyperaemic condition and indicative for pd . 
4 indications for adenosine stress first - pass pcmr for the diagnosis of cad are scored on the clinical symptoms as appropriate , uncertain , and inappropriate ( a )  . 
similarly , adenosine stress first - pass pcmr is appropriate as post - test assessment in patients with previous coronary imaging ( angiography or mdct - ca ) showing stenosis of unclear significance ( b ) fig . 
the detection of an inhomogeneous distribution of gd during the pharmacological stress with the presence of a darker area within the myocardium allows the identification of pd distal to a clinically significant stenosis : a subendocardial pd ( arrowheads ) of mid - basal anterior septum ( lad vascular territory ) is well shown on the stress - perfusion scan ( a ) , and not present at rest ( b ) technique : stress agent the most frequently used drug for pcmr is adenosine , a nonselective agonist for different receptors ( a1 , a2a , a2b , a3 ) of arteriolar vascular smooth cells , as extensively reported [ 21 ] , able to induce arteriolar vasodilatation with a good safety profile . 
however , adenosine is not a selective activator for the subtype a2a - receptors and some side effects ( flushing , chest pain , dyspnoea , hypotension ) may occur . 
more serious side effects ( bronchospasm , high - grade atrioventricular - block ) are less frequent and may resolve quickly after infusion interruption , because of its very short half - life ( < 10 s )  . 
for the same reason , adenosine administration requires a continuous iv injection ( 140 g / kg / min ) for at least 3 min before and during the perfusion scan . 
however , dobutamine is currently mainly used to assess inducible wall motion abnormalities and not as a stressor for perfusion studies [ 23 ] , as the high hr can cause severe artefacts in pcmr image quality . 
 furthermore , its usefulness has been reported in patients with asthma / lung disease , resulting in being less affected by recent caffeine - intake , with less frequent related side effects ( chest discomfort , headache , nausea , flushing , hypotension , hr increase ) , and a time window for pcmr in the average of 2 min from the injection [ 2729 ]  . 
however , the accurate selection of candidates for pcmr and nuclear perfusion imaging has been recently underlined by a food and drug administration warning regarding both adenosine and regadenoson [ 30 ] , highlighting the need for available cardiac resuscitation equipment and trained staff before administering both drugs . 
when using high - relaxivity contrast agents , the recommended dose is 0.075 mmol / kg , repeated twice for stress and rest ; for lower - relaxivity contrast agents , a dose of 0.1 mmol / kg ; is generally used . 
when quantitative analysis is needed , the 1 3fi radiol med ( 2015 ) 120 : 190205 saline neat gd 25 s dual - bolus technique ( 10 % diluted gd saline ) is preferable as previdelay time ously described [ 17 ]  . 
depending on the clinical indication , the gd dose injected for stressand rest - pcmr can be topped up to double dose ( 0.2 mmol / kg ) for better late gd enhancement ( lge ) image quality [ 31 ]  . 
the maximum in - plane spatial resolution ( sr ) depends on the sequence , ranging from 1.2 to 3 mthe superior sr is one of the advantages table 4 volumes of gd using a dual - bolus technique patients body weight ( kg ) pre - bolus ( 0.1 mmol / ml of gd ) ( ml ) main bolus ( 1 mmol / ml of gd ) ( ml ) top - up ( 1 mmol / ml of gd ) ( ml ) total injection volume volumes of gd for a bolus dose of 0.075 mmol / kg / body weight , including the corresponding diluted gd injection using a dual - bolus technique . 
the main bolus uses a 1.0 mmol / ml solution of gadoliniu the pre - bolus uses a 10 % diluted solution of gadolinium ( 0.1 mmol / ml ) , according to ishida et al . 
6 the evaluation of myocardial perfusion during the first pass of gd is performed by the continuous and fast acquisition of 3 ( or 5 ) short - axis slices ( or combination of short and long axis ) on every heartbeat , with a slice thickness of 810 mm covering all vessel territories of the lv ( a : diastole ; b : systole ) 1 3 196 radiol med ( 2015 ) 120 : 190205 over nuclear medicine techniques , where sr is generally 810 mas ischaemia affects earlier and more severely the subendocardial layers , higher sr facilitates the detection of thinner subendocardial pd that might be missed by other modalities . 
moreover , a high sr is usually associated with a lower incidence and severity of subendocardial darkrim artefacts , resulting in a further improvement of the diagnostic accuracy ( da )  . 
pre - pulses are triggered on the qrs - complex of the ecg to null the longitudinal magnetization of blood and myocardium , and generate the t1 - contrast which depends on gd administration . 
they can be either inversion recovery or saturation recovery : the former allows better signal suppression , but multiple ir pulses , as needed for multislice imaging , should not be repeated more frequently than several multiple of myocardial t1 , leading to a reduction of the temporal resolution . 
8 regardless of the type of image readout adopted ( turbo gradient echo imaging or steady - state free precession ) , perfusion sequences are usually built with a 90 saturation pre - pulse ( sp ) to generate the t1 contrast . 
9 cmr scan protocol including stress and rest perfusion scan : stress - pcmr is usually followed 1015 min later by rest perfusion imaging and therefore lge , with the time between stress and rest scan generally used to acquire cine - imaging for functional assessment table 5 technical requirement for pcmr sequences high temporal resolution ( 1 image / heartbeat ) shorter acquisition window ( < 100 ms / slice ) to limit the respiratory / cardiac movement related artefacts constant magnetization per image / slice high spatial resolution coverage of all standard 16 aha segments regardless of the pre - pulse used to increase the t1 - weighting and of the technical solution adopted to increase the acquisition speed , several different readout schemes can be used : segmented gradient echo imaging ( turbo field echo , fast gradient echo , turbo flash ) , echoplanar or hybrid echoplanar ( epi ) , or steady - state free precession ( ssfp : true - fisp , balanced - ffe , fiesta )  . 
in general , epi has lower signal - to - noise ratio ( snr ) , while ssfp has lower contrast - to - noise ratio ( cnr )  . 
a first strategy exploits k - space correlations and allows acceleration by reducing the amount of information acquired in every heartbeat by partial fourier , reduced - phase field of view ( fov ) , or speeding up the acquisition by implementing parallel imaging techniques ( asset , ipat , grappa or sense ) coupled with phasedarray coils [ 33 , 34 ]  . 
the third strategy is a combination of the above methods : the k - space is undersampled and the missing data points are obtained using a training dataset reacquired only in a minority of dynamics [ 35 ]  . 
while pcmr is inherently a high sr technique in comparison with other imaging modalities for ischaemia detection , the most recent technical developments such as k - space and time sensitivity encoding ( k - t sense ) or broad - use linear acquisition speed - up technique ( k - t blast ) in combination with higher magnetic field 3t scanners allow fur ther improvements of in - plane sr with favourable snr [ 36 ] , allowing a reliable cad detection and good results in comparison with ffr [ 37 ]  . 
the use of a turbo ge sequence rather than ssfp , higher sr , lower gd doses or the dual - bolus gd injection [ 17 ] can help in reducing this artefact . 
a true pd is generally not circumferential ( excluding mvd ) , not black but presenting as a grey transmural gradient which persists for several heartbeats ( > 5 ) after the beginning of gd wash - in in the lv myocardiu a true pd generally extends to more than one pixel transmurally , 1 3 radiol med ( 2015 ) 120 : 190205 198 fig . 
10 the qualitative analysis of pcmr is based on visual ( subjective ) assessment of velocity and homogeneity of intra - myocardial gd wash - in during the stress / rest perfusion scan for the detection of myocardial regions with lower si in comparison with normal myocardial segments : 68 - yearold patient with hypercholesterolaemia and hypertension , complaining of anginal chest painvasive coronary angiography showed a 75 % lesion on the right coronary artery with a ffr of 0.51. 
 stress images demonstrate a large perfusion deficit ( arrowheads ) in the right coronary artery territory , with subendocardial location persisting more than three heartbeats beyond peak enhancement of the most normal surrounding myocardiutable 6 summarises some of the most useful reading criteria for pcmr qualitative assessment . 
the software divides each short - axis view into six or more radial segments , while the si of the lv cavity is marked ; therefore , the myocardial si is analysed for each segment , applying a chromatic scale and obtaining the relative maximum upslope of si . 
11 the rim artefact on pcmr is typically represented by a very thin ( 1 pixel ) subendocardial rim - like black area appreciable along the endocardial border of the lv myocardium ( arrows ) during the first - pass transit of the gd in the lv cavity . 
in order to minimise some signal inhomogeneities due to differences of surface coils for data acquisition , the normalised maximum upslope of myocardial si during gd wash - in is used rather than the slope itself . 
moreover , myocardial si normalisation for si upslope in the lv cavity ( arterial input function , aif ) also corrects the result for possible differences in velocity of the gd bolus due to stress - induced changes in cardiac output . quantitative analysis 4 - point scale ( 0 normal ; 1 probably normal ; 2 probably abnormal ; 3 abnormal ) this analysis , proposed more than 10 years ago and mainly used as a research tool , is not yet routinely applied , mostly fig . 
the presence of pd in stress scan but not in rest suggests inducible ischaemia , while matching defects at stress and rest suggest artefacts or the presence of scarring that should be confirmed with lge sequence . 
matching of subendocardial hypoenhancement ( static lesion ) ( white arrows ) at stress ( a ) and rest scan ( b ) , with positive lge ( black arrows ) due to myocardial scar fig . 
13 semi - quantitative analysis : subendocardial segments show lower perfusion compared with corresponding epicardial segments , indicative for area of subendocardial ischaemia in the right coronary artery territory 1 3 200 fig . 
14 visual assessment ( a ) and quantitative analysis ( b ) with high - resolution pixel - wise perfusion map by fermi deconvolution in the same patient as fig . 
the dual - bolus technique [ 17 ] can help , as the first low - dose contrast bolus allows a more accurate aif measurement and the second high - dose contrast bolus measures the tissue function with high snr . 
the main advantages for a quantitative analysis are a reduced interpreter bias , a potential role for detection of balanced multivessel ischaemia ( i.e. , three - vessel disease ) , the differentiation of moderate from severe stenoses in patients with known / suspected cad [ 44 ] , and the quantification of response after therapeutic interventions . 
 [ 45 ] ( 1 , 183 patients , 14 studies , cad prevalence 57.4 % ) , pcmr showed a sensitivity of 91 and 84 % and a specificity of 81 and 85 % , respectively , on a per - patient and on a coronary territory analysis for the detection of ischaemic segments . 
with regard to the perterritory analysis ( 2 , 709 territories , 17 studies ) , pcmr showed a sensitivity of 82 % ( 7984 % ) and a specificity of 84 % ( 8285 % )  . 
main factors which may play a role in explaining the high false - positive rate determining a common low pcmr specificity on per - patient analysis are : dark - rim artefacts [ 42 ] , presence of mvd , and presence of microvascular obstruction ( mvo ) in an infarcted area , with unobstructed supplying coronaries either following medical treatment or spontaneous thrombolysis [ 39 , 48 ]  . 
 by contrast , a false - negative ca could be also considered a possible explanation , because of the angiographic assessment of the morphology rather than the functional significance of a stenosis in the presence of angiographically invisible small vessel disease inducing subendocardial ischaemia [ 39 , 49 ] ; this potential error could be avoided by evaluating the haemodynamic significance of lr of 4.43 ( 95 % ci 3.645.23 ) , and a 1 3 radiol med ( 2015 ) 120 : 190205 fig . 
15 diagnostic accuracy of pcmr versus invasive coronary angiography for the detection of analysis in a set of high cad prevalence 50 % coronary stenosis at per - patient level stenosis by ffr assessment during the same invasive procedure [ 5054 ]  . 
the association of lge for the identification of myocardial infarct ( mi ) showed an increase of the overall accuracy ( 88 % ) , in particular a higher specificity ( from 58 to 87 % ) compared to ca [ 38 ]  . 
recently , different studies have assessed qualitatively , semi - quantitatively , or quantitatively pcmr da to detect haemodynamically significant stenosis , with ffr as reference [ 4952 ]  . 
 [ 50 ] ( 43 patients with suspected / known cad ) showed a 1.5 t pcmr sensitivity of 88 % ( ci 74100 % ) and specificity of 90 % ( ci 8496 % ) in distinguishing haemodynamically relevant from nonrel10 mm , evant stenoses , using a pcmr sr of 2.7 and an ffr cut - off value of 0.75. 
 [ 51 ] in 2007 obtained for 1.5 t pcmr a sensitivity and specificity of 92 % and 92 % in detecting significant stenosis in 19 patients with known cad , using a ffr cut - off value of 0.75 and a pcmr sr of 2.72.9 8 min 30 patients enrolled in a prospective study , costa et al . 
 [ 52 ] assessed a 1.5 t pcmr sensitivity and specificity of 92 and 56.7 % , respectively , in differentiating significant from nonsignificant stenoses , with an ffr cut - off value of 0.75 , and a pcmr sr of 23 8 m more recently , 23 lockie et al . 
 [ 53 ] showed in patients without mi higher sensitivity on qualitative analysis for pcmr in comparison with spect for significant cad detection , using qca as the gold standard . 
in particular , in 69 patients who underwent both pcmr and stress - spect , the sensitivity for significant stenosis of at least one coronary artery was 94 % with pcmr and 82 % with spect . 
for the detection of single - , double - , and triple - vessel disease , pcmr showed a sensitivity of 90 , 100 , and 100 % , respectively , compared to a spect sensitivity of 73 , 88 , and 100 % , respectively . 
the mr - impact study [ 11 ] was the first double - blind multicentre ( 18 centres ) , multivendor trial to assess diagnostic performance for pcmr versus qca and spect : the roc analyses showed that pcmr is a useful technique for cad detection with a sensitivity of 85 % and a specificity of 67 % , in comparison with a gated - spect sensitivity of 75 % . 
the recent ce - marc study [ 14 ] assessed the da of multi - parametric cmr in comparison with spect , with qca as the reference standard in patients with suspected cad , and prospectively enrolled . 
so far , these results show that in a large population of patients suspected of having angina pectoris , cmr is a useful alternative to spect for the detection of clinically significant cad , yielding a better sensitivity and npv , and overcoming the well - known limitations of spect ( ionizing radiation , limited sr , attenuation artefacts )  . 
the authors of the ce - marc study underline that these results should be also considered in the context of published spect data , usually heterogeneous for population , protocols , stress modality , and radioisotope tracer , underscoring that theirs is the first study comparing prospectively spect with qca in such a large number of patients . 
more recently , the myocardial perfusion reserve assessed by pcmr and pet for significant cad detection proved to be comparable and very accurate [ 43 ] , but with a weak correlation for absolute perfusion values , showing the need for further refinements for quantitative pcmr . accuracy versus dobutamine stresscmr in the comparison between adenosine - pcmr with highdose dobutamine stress - cmr ( ds - cmr ) for the assessment of patients with suspected cad , the meta - analysis of nandalur [ 45 ] reported , at a per - patient level , similar good sensitivities ( pcmr : 91 % , ds - cmr : 83 % ) and specificities ( pcmr : 81 % , ds - cmr : 86 % ) , with overlapping values at the coronary level . 
 [ 54 ] assessed the da of both ds - cmr and adenosine - pcmr in 79 consecutive patients , with suspected / known cad without a previous history of mi , and scheduled for ca . 
 [ 55 ] have performed a head - to - head comparison of adenosineand high - dose dobutamine - pcmr in 41 patients with known / suspected cad , with qca as the sor . 
recently , mdct perfusion imaging has been tested as a potential tool for ischaemia detection , with preliminary studies showing its incremental value on mdcta - ca for the detection of obstructive cad in high - risk populations in comparison with ca , and its safety profile . 
in particular , the integration of mdct - ca with mdct perfusion imaging showed a significant increase of both specificity and ppv ( 83 and 80 % ) in high - risk patients in comparison with mdct - ca alone ( 61 and 67 % )  . 
however , mdct perfusion imaging cannot yet be regarded as clinical routine , because it is still limited by radiation exposure , contrast load , lack of a standardised acquisition protocol and low number of published trials . 
potentially , mdct perfusion imaging should be considered in patients with contraindications for other imaging modalities [ 58 ]  . prognostic value of pcmr the usefulness of pcmr in acute settings to exclude / confirm significant cad with excellent one - year prognosis has been demonstrated by ingkanisorn et al . 
in this study , in patients presenting to the emergency department with chest pain but in whom an acute mi was excluded by negative troponin , pcmr predicted patients with significant cad ( stenosis > 50 % , abnormal stress test , mi , death ) during 1 - year follow - up , with 100 % sensitivity , 93 % specificity , 71 % ppv and 100 % npv . 
a positive stress - cmr allowed identification of high - risk patients for subsequent cardiac event ( death , nonfatal - mi ) , while a normal scan was associated with a very low event rate at 2 years . 
 the cumulative event rate in patients with a negative test was 0.8 % at 3 years , versus 16.5 % for patients with a positive test , and on multivariate analysis an abnormal stress test remained the only independent predictor of events . 
 [ 61 ] , performed to assess the pcmr prognostic value in patients with intermediate - to - high risk for cad but without known cad or previous mi , the npv for the composite mace end - point was 99.5 % at 6 months and 99.1 % at 12 months . 
kirchin gianpaolo pirovano xiaoying wang yuan li roberto iezzi francesco de cobelli received : 30 october 2013 / accepted : 13 march 2014 / published online : 3 september 2014 ( cid : 2 ) italian society of medical radiology 2014 abstract purpose the authors prospectively compared single dose ( 0.1 mmol / kg bodyweight ) gadobenate dimeglumine with double dose ( 0.2 mmol / kg bodyweight ) gadopentetate dimeglumine for contrast - enhanced magnetic resonance angiography ( ce - mra ) in patients with suspected or known steno - occlusive disease of the carotid , renal or peripheral vasculature using an intra - individual crossover study design . materials and methods twenty - eight patients with suspected or known steno - occlusive disease of the carotid ( n = 16 ) , renal ( n = 5 ) or peripheral arteries ( n = 7 ) were randomised to receive either 0.1 mmol / kg gadobenate dimeglumine or 0.2 mmol / kg gadopentetate dimeglumine for a rst ce - mra procedure . 
quantitative ( signal - to - noise and contrast - to - noise ratio ) enhancement based on 3d maximum intensity projection reconstructions was compared . results no differences were noted for any qualitative parameter . 
quantitative enhancement was similar for single dose gadobenate dimeglumine and double dose gadopentetate dimeglumine . conclusions under identical examination conditions a single 0.1 mmol / kg body weight dose of gadobenate dimeglumine can fully replace a double 0.2 mmol / kg body weight dose of gadopentetate dimeglumine for routine cemra procedures . keywords magnetic resonance angiography ( cid : 2 ) gadobenate dimeglumine ( cid : 2 ) gadopentetate dimeglumine ( cid : 2 ) vascular disease ( cid : 2 ) comparative trials x . 
de cobelli radiologia diagnostica , uo di risonanza magnetica , ospedale san raffaele , via olgettina , 60 , 20132 milan , italy 240 introduction the dose of magnetic resonance ( mr ) contrast agent used in routine contrast - enhanced mr angiography ( ce - mra ) procedures has recently become a matter of great concern given the risk of nephrogenic systemic brosis ( nsf ) among patients with severe renal insufciency . 
in part this concern stems from the fact that higher - than - standard doses of gadolinium contrast agent ( up to 0.4 mmol / kg body weight ) have frequently been used for routine cemra procedures . 
the clinical need is therefore to reduce the dose of gadolinium administered while maintaining sufcient contrast enhancement and image quality to achieve an accurate diagnosis and / or to accurately plan interventional procedures . of the mr contrast agents currently available multihance ( gadobenate dimeglumine ; bracco imaging spa , it possesses markedly milan , italy ) is unique in that increased r1 relaxivity relative to conventional gadolinium agents due to weak and transient interaction of the gadobenate contrast effective molecule with serum albumin [ 13 ]  . 
this increased r1 relaxivity translates into increased signal intensity enhancement relative to that achieved with conventional gadolinium agents at equivalent dose [ 412 ]  . previous studies have shown that a single 0.1 mmol / kg bodyweight dose of gadobenate dimeglumine can fully replace a double 0.2 mmol / kg body weight dose of gadopentetate dimeglumine for specic mr imaging applications , including ce - mra [ 1319 ]  . the aim of our study was to determine whether a single dose of gadobenate dimeglumine can fully replace a double dose of gadopentetate dimeglumine across all routine cemra applications in a typical radiology department setting . 
to this end , an intra - individual crossover study design was employed in which each patient received both contrast agents in two otherwise identical ce - mra examinations separated by 35 days . materials and methods twenty - eight patients referred to our centre for known or suspected steno - occlusive disease of the supra - aortic , renal or peripheral arteries were evaluated . 
finally , patients were ineligible if they were pregnant or lactating or if they had any medical condition or other circumstances that would decrease the chances of obtaining an adequate examination or which would preclude proximity to a strong magnetic eld . mra examinations ce - mra was performed at on a 1.5t unit ( sonata ; siemens medical solutions , erlangen , germany ) equipped with a gradient of at least 40 mt / m and automatic moving table . imaging of the supra - aortic vasculature was performed from the brachiocephalic trunk up to and including the carotid bifurcation and the extracranial internal carotid artery ( ica )  . 
images were acquired with repetition time : 3.4 ms ; echo time : 1.29 ms ; ip angle : 30 ( cid : 3 ) ; excitations : 1 ; eld - of - view ( fov ) : 300 9 250 ; matrix : 384 9 240 ; slice thickness : 1.0 mm ; acquisition time : 19 s . imaging of the renal / abdominal vasculature included the left and right main renal arteries ( from the ostium to the subdivision in the dorsal and ventral segmental branches ) , the abdominal aorta ( from approximately 2 cm above the origin of the celiac trunk to the iliac bifurcation ) and the left and right common iliac arteries ( including the common iliac artery bifurcations )  . 
images were acquired with repetition time : 2.84 ms ; echo time : 1.06 ms ; ip angle : 25 ( cid : 3 ) ; excitations : 1 ; eld - of - view ( fov ) : 300 9 083 ; matrix : 384 9 192 ; slice thickness : 1.5 mm ; acquisition time : 17 s . imaging of the peripheral vasculature was performed across three stations ( pelvis , thigh , calf )  . 
the pelvic station was acquired with repetition time : 2.50 ms ; echo time : 0.98 ms ; ip angle : 20 ( cid : 3 ) ; excitations : 1 ; fov : 400 9 083 ; matrix : 384 9 192 ; slice thickness : 2.0 mm ; acquisition time : 15 s . the thigh station was acquired with repetition time : 3.50 ms ; echo time : 1.23 ms ; ip angle : 25 ( cid : 3 ) ; excitations : 1 ; fov : 400 9 069 ; matrix : 512 9 194 ; slice thickness : 2.0 mm ; acquisition time : 17 s . 
the calf station was acquired with repetition time : 4.36 ms ; echo time : 1.49 ms ; ip angle : 30 ( cid : 3 ) ; excitations : 1 ; fov : 400 9 081 ; matrix : 512 9 271 ; slice thickness : 1.2 mm ; acquisition time : 38 s . radiol med ( 2015 ) 120 : 239250 ( 0.4 ml / kg ) 0.2 mmol / kg ce - mra of all patients was performed after administration of 0.1 mmol / kg ( 0.2 ml / kg ) gadobenate dimeglumine gadopentetate dimeglumine . 
contrast administration was performed as a biphasic injection to patients undergoing ce - mra of the peripheral vasculature with two - thirds of the total dose administered in a rst injection and one - third as a second injection . 
the interval between the two examinations in each patient ranged between 3 and 5 days . to ensure identical bolus geometry for the two examinations in each patient , the two fold greater volume of gadopentetate dimeglumine administered to each patient was injected at a two fold faster rate . 
the choice of contrast agent injection rate was at the discretion of the investigating radiologist based on patient - related factors ( age , size , venous status , etc . ) and was selected to ensure that bolus arrival within the vessels of interest coincided with acquisition of the lowest order phase encoding steps in k - space to obtain maximum vessel enhancement . 
in all cases the injection was timed precisely to ensure a total administered dose of 0.1 mmol / kg body weight for gadobenate dimeglumine and 0.2 mmol / kg body weight for gadopentetate dimeglumine . 
whereas global diagnostic preference was assessed at the patient level , both vessel anatomical delineation and disease detection / exclusion were assessed by vascular station [ two stations ( neck vessels and carotid bifurcation / extracranial ica ) for patients undergoing carotid mra , one station for patients undergoing renal mra and three stations ( pelvis , thigh and calf ) for patients undergoing peripheral mra ]  . 
all qualitative comparisons were performed using 3 - point scales from - 1 ( exam 1 superior ) through 0 ( exams equal ) to ? 1 ( exam 2 superior )  . quantitative measurements of signal intensity ( si ) were made by each reader at regions - of - interest ( rois ) positioned in the vessels under investigation . 
rois were typically circular and large enough ( c0.5 cm2 ) to obtain reliable measurements at areas of maximum si within the lumen and on homogenous regions the two of muscle . 
for the renal / abdominal and peripheral vasculature the 4 - point scale comprised : 1 = vessel with no or mild stenosis ( \25 % ) ; 2 = vessel with moderate stenosis ( c25 % but \51 % ) ; 3 = vessel with clinically relevant disease ( c51 to \100 % ) and 4 = vessel with occlusion ( 100 % lumen blockage )  . 
for the supra - aortic vasculature the 4 - point scale comprised : 1 = vessel with no or mild stenosis ( \30 % ) ; 2 = vessel with moderate stenosis ( c30 % but \60 % ) ; 3 = vessel with clinically relevant disease ( c60 to \100 % ) and 4 = vessel with occlusion ( 100 % lumen blockage )  . all assessments were made visually on the basis of the experience of the blinded readers and as routinely performed in clinical practice ; there was no use of digital calipers to determine the degree of stenosis . 
in all cases , the degree of stenosis was determined by comparing the part of the vessel in question with an area of normal artery with parallel walls that was beyond any post - stenotic dilatation . stenoses detected at ce - mra were labelled on maximum intensity projection ( mip ) images for lesion matching with stenoses detected subsequently at digital subtraction angiography ( dsa )  . digital subtraction angiography ( dsa ) dsa was performed in 20 of the 28 patients who underwent ce - mra . 
the approach to dsa was as performed as part of clinical routine , involving injection of an iodinated contrast medium with an iodine concentration of c300 mg i / ml through a pigtail or straight 45 f catheter inserted via a femoral artery puncture using the seldinger technique . 
images were acquired using anteroposterior and right and / or left anterior oblique projections at angulations of 15 ( cid : 3 ) 30 ( cid : 3 ) as appropriate . 
stenoses detected at dsa were labelled for subsequent matching with ndings from the blinded reading of ce - mra images . safety assessments all subjects were monitored for adverse events for 24 h after administration of each agent . 
evaluation of laboratory parameters was performed on samples acquired within 24 h before and within 24 h after each administration . statistical analysis diagnostic preference , vessel anatomical delineation and disease detection / exclusion were summarised descriptively . 
comparison of quantitative enhancement was performed using a mixed model with subject , period , sequence and contrast agent group as variables . determinations of diagnostic performance [ sensitivity , specicity , accuracy , positive and negative predictive values ( ppv , npv ) and 95 % condence intervals ( ci ) ] for the detection of clinically relevant disease were performed using dsa as reference standard . 
non - inferiority for 0.1 mmol / kg gadobenate dimeglumine compared to 0.2 mmol / kg gadopentetate dimeglumine was demonstrated if the lower limit of the 95 % ci was within - 5 % . 
differences in ppv and npv were compared using the wald test derived from radiol med ( 2015 ) 120 : 239250 general estimating equation with intra - individual correlation accounted for . inter - reader agreement was determined using generalised weighted kappa ( j ) statistics and measured as percentage agreement . 
the seven patients with suspected peripheral arterial occlusive disease included four with mild claudication ( stage iia according to fontaines classication [ 20 ] ) and three with moderate - tosevere claudication ( stage iib )  . overall , 13 patients received gadobenate dimeglumine for the rst ce - mra examination while 15 received gadopentetate dimeglumine for the rst ce - mra examination . 
a total of 61 vascular stations were assessed qualitatively across these 27 patients : 32 ( 16 9 2 ) stations for 16 patients undergoing ce - mra of the carotid vessels ; 5 stations for 5 patients undergoing ce - mra solely of the renal / abdominal vessels , and 18 ( 6 9 3 ) peripheral stations ? 6 renal stations for the 6 patients undergoing combined ce - mra of the peripheral and renal arteries . a total of 20 patients also underwent dsa and were available for analysis of diagnostic performance . 
these patients comprised 12 who underwent ce - mra of the carotid arteries , three who underwent ce - mra solely of the renal arteries and ve who underwent ce - mra of both the peripheral and renal arteries . qualitative evaluation reader assessment of qualitative enhancement in matchedpairs revealed no marked differences ( table 2 )  . 
there was no vascular station , anatomical station or qualitative endpoint in which any reader consistently preferred ce - mra images enhanced by one agent over ce - mra images enhanced by the other . 
a comparison of diagnostic performances in each specic vascular territory is presented in table 4 while examples of the quality and diagnostic efcacy achieved with 0.1 mmol / kg gadobenate dimeglumine and 0.2 mmol / kg gadopentetate dimeglumine in the different territories are shown in figs . 
no clinically meaningful worsening was noted for any parameter . discussion in this study we compared a single 0.1 mmol / kg dose of gadobenate dimeglumine with a double 0.2 mmol / kg dose of gadopentetate dimeglumine using an intra - individual crossover study design . 
1 mean signal - to noise ratio ( snr ) and contrast - to - noise ratio ( cnr ) after 0.1 mmol / kg gadobenate dimeglumine and 0.2 mmol / kg gadopentetate dimeglumine as determined by three independent blinded readers . 
values based on 56 combined vascular territories for readers 1 and 2 and 59 combined vascular territories for reader 3 ; p values from paired t tests diagnostic performance dsa reference standard ndings were available for 267 vascular segments across the 20 patients who underwent dsa and both ce - mra examinations . 
these 267 segments comprised 105 in patients who underwent supraaortic mra , 48 in patients who underwent renal ce - mra either as a distinct examination or as part of a combined peripheral / renal ce - mra procedure and 114 who underwent peripheral ce - mra . 
similarly , intra - individual crossover comparisons between single dose gadobenate dimeglumine and double dose gadopentetate dimeglumine have revealed equivalent or better imaging performance with the former agent and dose [ 1315 , 18 , 19 ]  . 
our study extends these studies to assess the diagnostic performance achieved on ce - mra across a range of routine ce - mra applications performed as standard in our imaging centre . 
our ndings conrm those of previous studies in showing that a single dose of gadobenate dimeglumine is fully comparable to a double dose of gadopentetate dimeglumine not only in terms of image quality and quantitative contrast enhancement , but also in terms of diagnostic performance for the detection of clinically relevant steno - occlusive disease . the implications for routine practice are potentially dramatic , not only in terms of costs and convenience but also in terms of patient safety . 
notably , the vast majority of cases of nsf have occurred in patients undergoing cemra with conventional gadolinium contrast agents at doses greater than the approved dose of 0.1 mmol / kg body weight [ 2126 ]  . 
 [ 28 ] who compared gadobenate dimeglumine interindividually with the more concentrated ( 1 m ) agent gadobutrol [ gadovist ( gadavist ) , bayer healthcare , berlin , germany ] at an equivalent total volume of 0.1 ml / kg body weight ( corresponding to 0.1 mmol / kg gadobutrol but only 0.05 mmol / kg gadobenate dimeglumine )  . 
in their study , three blinded , independent readers found no differences in quantitative enhancement , image quality or diagnostic accuracy indicating that the t1 shortening achieved per unit time with 0.05 mmol / kg gadobenate dimeglumine is equivalent to that achieved with 0.1 mmol / kg gadobutrol . as noted elsewhere [ 49 ] the higher in vivo r1 relaxivity of gadobenate dimeglumine is due to weak , transient interaction of the gadobenate contrast - effective molecule with serum albumin [ 3 , 29 ] which slows its molecular tumbling rate leading to greater shortening of the t1 relaxation time and thus substantially increased si enhancement . a possible limitation of the study is that only 28 patients were enrolled . 
the mip images acquired after 0.1 mmol / kg gadobenate dimeglumine ( 13 ml injected at 1.3 ml / s ) reveal occlusion ( open arrow ) of the left common carotid artery / bifurcation / ica a and a c60 % stenosis ( closed arrow ) of the right carotid bifurcation / ica b this severe stenosis is conrmed on the volume - rendered ( vr ) image c similar ndings are seen on the analogous mip and vr images df acquired after 0.2 mmol / kg gadopentetate dimeglumine ( 26 ml injected at 2.6 ml / s )  . 
digital subtraction angiography ( dsa ) g , h conrms both the occlusion ( open arrow ) and the severe stenosis ( closed arrow ) radiol med ( 2015 ) 120 : 239250 fig . 
the mip image a acquired after 0.1 mmol / kg gadobenate dimeglumine ( 11 ml injected at 1.1 ml / s ) reveals severe stenoses of both the left and right main renal arteries ( arrows )  . 
both stenosis are apparent on the vr image b similar ndings are seen on the analogous mip and vr images c , d acquired after 0.2 mmol / kg gadopentetate dimeglumine ( 22 ml injected at 2.2 ml / s )  . 
the mip images after biphasic administration of a 0.1 mmol / kg gadobenate dimeglumine ( rst injection 10 ml at 1 ml / s ; second injection 5 ml at 0.5 ml / s ) , and b 0.2 mmol / kg gadopentetate dimeglumine ( rst injection 20 ml at 2 ml / s ; second injection 10 ml at 1 ml / s ) reveal severe stenoses of the left and right renal arteries and right supercial femoral artery ( closed arrow ) and occlusion of the left supercial femoral artery ( open arrow )  . 
for intra - individual crossover studies smaller patient populations are needed to demonstrate differences in contrast agent effectiveness than would be required for statistically powered in which parallel - group inter - individual patients receive just one of two or more comparator agents . in conclusion , our study conrms that 0.1 mmol / kg gadobenate dimeglumine can fully replace 0.2 mmol / kg gadopentetate dimeglumine for ce - mra of the supraaortic , renal and peripheral vasculature . comparisons conict of interest xiaoying xing , xiangzhu zeng , xuan , qiang zhao , miles a . 
kirchin , gianpaolo pirovano , xiaoying wang , yuan li , roberto iezzi , francesco de cobelli declare that bracco imaging spa provided nancial support for the enrolment of patients . 
nevertheless , certain image acquisition parameters and physical features of patients have to be considered when designing low - dose protocols in the 3d mode . purpose the aim of this study was to compare images acquired in 2d and 3d modes and establish a low - dose protocol for use in pet / ct imaging , decreasing patient exposure to radiation without compromising results . methods a total of 30 patients , aged 472 years , participated in this prospective study , which was conducted at albert einstein hospital , sao paulo , brazil . 
images were evaluated for picture quality , presence / absence of lesions and the number of lesions that were detectable in both acquisition modes . results the results consistently showed that the loss in image quality in the 3d mode did not affect exam interpretation and lesion detection when compared with 2d at higher dose and for a longer time . conclusions we therefore conclude that administration of 3.7 mbq [ 18f ] - uorodeoxyglucose ( fdg ) / kg for an s . 
lederman departamento de diagnostico por imagem , universidade federal de sao paulo , sao paulo , brazil acquisition time of 3 min per fov ( eld of view ) is optimal for image acquisition in the 3d mode . 
this protocol , which reduces the acquisition time and radiation dose , is quite benecial , especially for children . 18f - fdg ( cid : 2 ) pet / ct ( cid : 2 ) 2d ( cid : 2 ) 3d ( cid : 2 ) acquisition ( cid : 2 ) keywords dose reduction introduction in recent decades , there has been a signicant increase in the number of diagnostic imaging examinations using ionizing radiation , increasing the risk of disease development induced by radiation exposure . the use of positron emission tomography combined with computed tomography ( pet / ct ) has brought about signicant technological advancement in diagnostic imaging , but proper use of this technology requires greater attention to the increased patient exposure to radiation [ 1 , 2 ]  . some pet / ct scanners use bismuth germanate ( bgo ) detectors and are designed to capture images in both 2d and 3d . 
image acquisition in the 2d mode uses septa between detector blocks to reduce detection of events originating from photon scattering and attenuation , resulting in reduced sensitivity [ 3 , 4 ]  . 
conversely , acquisition in the 3d mode , without septa , is able to detect a higher number of events , but the increased sensitivity results in detection of unwanted events , leading to deterioration of the image quality [ 3 , 57 ]  . currently , there is a tendency toward reducing the use of 2d imaging , which requires higher [ 18f ] - uorodeoxyglucose ( 18f - fdg ) activity and longer acquisition time . recent studies have evaluated pet / ct scanners and shown that the 3d acquisition mode also delivers results of 252 radiol med ( 2015 ) 120 : 251255 good quality [ 810 ]  . 
the reduction in radiation dose received by patients undergoing pet / ct scans has a major impact on the healthcare management of children and adolescents , who are more susceptible to the harmful effects of radiation [ 1114 ]  . however , certain patient characteristics and acquisition mode parameters , such as weight , body mass index ( bmi ) , and image acquisition time , have to be considered and accounted for when designing low - dose protocols in the 3d mode . previous studies have used these features to optimize acquisition time and the dose of injected 18f - fdg to preserve image quality [ 1517 ] and the ability to detect lesions [ 18 ]  . because bgo detectors are less sensitive than other detectors used in pet / ct equipment such as lutetium oxyorthosilicate ( lso ) crystals , and also because the 3d mode detection ability is higher than that of the 2d mode , choosing 3d mode enables the use of a lower 18f - fdg dose and shorter image acquisition times [ 7 , 19 ]  . 
however , increased 18f - fdg activity , combined with increased patient body weight , results in image deterioration , which requires an adjustment of the protocol to obtain satisfactory results . an optimal protocol should use the lowest 18f - fdg activity possible and be adjusted for patient bmi in both adults and children . 
the protocol used in the study was based on patient body weight with 18f - fdg activity set at 7.4 mbq / kg and acquisition time per eld of view ( fov ) at 4 min for the 2d mode . 3d images were acquired 2 h after the start of the 2d acquisition , taking advantage of the radioactive decay of 18f - fdg to achieve approximately half of the initial activity ( 3.7 mbq / kg )  . 
the time per fov was 3 mtotal examination time for an average 8 fovs was 32 min for a 2d acquisition and 24 min for a 3d acquisition . image reconstruction image reconstruction was performed using iterative methods : ordered subsets expectation maximization ( osem ) for the 2d mode ( 2 iterations and 21 subsets ) and fourier rebinning ( fore ) - osem for the 3d mode ( 2 iterations and 28 subsets )  . 
for this experiment , these parameters could not be modied to improve the image quality . image analysis visual analysis of the images was performed by two observers with extensive experience in reading pet / ct images . the images of each acquisition mode were separately made available for random analysis in the xeleris workstation ( general electric medical systems , milwaukee , wisconsin , usa ) , at a minimum 2 - month interval between each mode . the observers had no access to patient information or acquisition mode under analysis . 
during analysis , image quality was characterized as suitable when it followed the usual pattern established in the sector or unsuitable when noise made it difcult to characterize the lesions . 
red arrows indicate the presence of lesions clinical cases the comparison between images captured in 2d and 3d modes from two clinical cases in which lesions were detected is shown in figs . 
2 are from a patient whose 254 radiol med ( 2015 ) 120 : 251255 detection sensitivity in the 3d mode was not affected when the 18f - fdg activity was reduced to half that used in the 2d mode . 
 ( 2010 ) [ 19 ] recommended that for acquisitions in the 3d mode 18f - fdg activity should be calculated according to the formula 2.96 mbq / kg for a xed time of 5 min , or in the case of equipment with a higher count rate capability , a correction factor should be used to reduce the exam time , multiplying the ratio body weight per fov time [ 13.8 9 ( kg / min ) ]  . 
in this study , the activity used for image acquisition in the 3d mode ( equivalent to 3.7 mbq / kg ) was even lower than the values used in majority of previous studies , and close to those recommended by boellaard et al . 
therefore , the success of a pet / ct imaging protocol relies on acquisition of high - quality images with minimum risk , without compromising important information for interpretation of the exato address this issue , two protocols have been suggested by alessio et al . : the rst with an activity of 5.18 mbq / kg and a time of 3 min per fov , and the other for children with body weight \22 kg ( 3.33 mbq / kg , 5 min per fov )  . 
in fact , discomfort in long exams may cause patients to move , generating artifacts in the image and the potential need to repeat the exam [ 23 ]  . 
taking this into consideration , the greatest advantage of the protocol used in this study is that a single protocol can be used in both pediatric patients and adults while reducing exam time and radiation dose . among the factors that may inuence image quality , such as equipment conguration , patient characteristics and parameter choice for image acquisition and processing , there is no consensus over which features are decisive for acquiring suitable images . 
previous studies also reported similar results for equipment using both bgo , lso and gso crystals [ 15 , 18 , 20 , 22 , 24 ] , but the loss in image quality did not affect exam interpretation and lesion detection . therefore , bmi should also be taken into account when developing image acquisition protocols . 
nevertheless , the results consistently showed that the loss in image quality did not affect exam interpretation and lesion detection , as no differences in image analysis were observed between acquisition modes . studies comparing different pet / ct acquisition times in the 3d mode found an increase in image quality for acquisitions between 4 and 5 min per fov [ 7 , 10 ]  . 
this provided increased comfort to patients during the examoreover , shorter exam times help reduce the need for sedation during whole - body pet / ct scans , which is particularly desirable in the case of children or debilitated patients . this reduction in acquisition time was possible despite the fact that bgo crystals lack the desirable physical characteristics for use in 3d mode [ 5 , 21 ]  . interestingly , radiol med ( 2015 ) 120 : 251255 mode , we strongly recommend that only 1 min / fov should be added for every bmi point above overweight ( [ 29.9 ) , while setting the acquisition time limit at 5 min instead of increasing the injected activity . conclusion the protocol proposed in this study for image acquisition in the 3d mode using scanners equipped with bgo crystals calls for administration of 3.7 mbq / kg 18f - fdg with an acquisition time of 3 min per fov , corrected for bmi in obese patients . 
moreover , no differences in exam results were observed when 2d and 3d acquisition modes were compared using this protocol . this study showed that a lower radiation dose and shorter acquisition time yielded very similar results to those indicated in the guidelines by boellaard et al . 
this protocol may be used with other types of equipment and future studies should conrm its veracity . acknowledgments the authors acknowledge scientic support from the instituto de pesquisa e ensino em medicina diagnostica e terapeutica ( ipmed )  . conict of interest solange a . 
goh antonio pinto mariano scaglione received : 11 july 2014 / accepted : 11 august 2014 / published online : 10 october 2014 italian society of medical radiology 2014 abstract to avoid detection at border crossings or airport customs , drug trafficking is increasingly performed by intracorporeal concealment . 
body packers may ingest packets of varying size and containing varying drugs ( mostly cocaine , heroin and cannabis ) mixed with other compounds , while body pushers will insert packets in the rectum or vaginal cavity . 
body packing may lead to potential life - threatening complications with acute overdose syndromes after packet rupture and intestinal obstruction with possible ensuing bowel rupture being the most significant complications . 
 although conventional radiography has long been and still is the most important imaging modality for screening for presence of intestinal packets , the better test characteristics in conjunction with the decreasing radiation exposure , will likely render computed tomography ( ct ) more important in the future . 
besides these modalities , ultrasound and magnetic resonance imaging will be discussed in this paper , together with more general background and clinical information . keywords computed tomography body packing body pusher drug smuggling mri cocaine heroin abdominal x - ray emergency introduction in europe , around one - third of the adult population has tried illicit drugs and approximately one person dies every hour as result of an overdose . 
although the percentage of people using illicit drugs in the world approximately remains stable , in an ever - growing global population production and abuse of substances in absolute numbers have to be increasing [ 2 ]  . 
albeit rough estimates , the drug trade is projected to make up 0.60.9 % of the worldwide gross domestic product ( gdp ) , in the us alone adding up to us$ 400 billion / year [ 3 ]  . although the majority of illicit substances are transported around the world by sea , road / train or air transport in different ways of packaging , concealment within a persons body remains a frequent mode of transportation for lesser quantities . 
b axial , c coronal and d oblique coronal reformats displaying a very large intravaginal heterogeneous packet ( big black stars ) and smaller intestinal packets ( small black stars ) or ( drug ) mules [ 4 ]  . 
 body stuffing , another term used in the literature , in its most appropriate use is reserved for people who in unexpected encounters with law - enforcement officers try to conceal small amounts of hastily wrapped drugs by swallowing [ 5 ]  . identifying the correct individuals as drug smugglers by profiling and imaging , as deemed fit , aims to eliminate false - negative assessments ( allowing drugs to be carried past customs ) as well as false positives ( putting innocent individuals in detention )  . 
in this review , we will detail further general considerations on corporeal illicit drug concealment , highlight clinical implications and focus on specifics of imaging modalities used to assess presence of packets and complications thereof . general and clinical background since illicit drugs are mostly produced in countries remote from the countries of final destination , transportation will often cross international borders . 
for doctors and other medical personnel , the most important method of transportation to be aware of is intra - corporeal concealment , first described in the medical literature by deitel and syed [ 6 ]  . 
so - called body packers on average swallow 20 packets ranging 25 cm in size , but cases have been 1 3 120 radiol med ( 2015 ) 120 : 118132 fig . 
body packing : a abdominal radiograph and b coronal ct reconstruction with layered and very linear lucencies / hypodensities representing air between and around money bills in packets located in the stomach and intestines ( arrows )  . 
body pushing : c sagittal and d axial ct reconstructions displaying a large intravaginal packet containing money bills , with layered air between and around the bills ( arrows ) described with more than 200 packets swallowed . 
each packet contains 812 g of substance of different purity , with smugglers on average carrying 1 kg ( up to around 2 kg ) [ 5 , 7 ]  . 
wrapping material used , type of drugs and purity will influence appearance on imaging examinations , as detailed below . 1 3 radiol med ( 2015 ) 120 : 118132 1 3 122 fig . 
c axial , d oblique axial and e oblique coronal ct reformats without oral contrast showing relatively hypodense uniform powder cocaine packets with dense wrapping material ( white stars ) and very hyperdense loosely configured liquid cocaine packets ( black stars ) to slow down intestinal transition time for long - haul flights , spasmolytics and constipating agents may be used to prevent passage of packets . 
complications by intestinal obstruction and acute intoxication now estimated to be below 5 % [ 9 ]  . if asymptomatic , a conservative approach allowing packets to pass is commonly accepted to be safe . 
predictors for hospital referral were delayed production of packets , cigarette smoking and country of origpercentage of need for surgical intervention did not differ between airport detention referrals or self - referrers [ 10 ]  . 
 imaging for screening purposes will usually take place at radiol med ( 2015 ) 120 : 118132 the airport or border crossing instead of collecting two or three consecutive stools . 
if individuals suspected of body packing suffer from signs and symptoms of bps , they are usually brought to hospital and will undergo imaging studies as deemed fit , most often consisting of radiography or computed tomography ( ct )  . 
in addition to these relatively well - studied imaging technologies , full - body low - dose radiography , ultrasound and mri have been investigated to varying extents in the setting of body packing . with any of the imaging techniques , the more packets are present in the intestines , the higher the likelihood of visibility on imaging studies . 
 [ 12 ] demonstrating that residual cocaine - filled packets were missed on pre - discharge abdominal x - rays by at least one reader in 70 % when compared to ct . 
detectability is further influenced by the shape and size of the packets , mechanically produced packets being fairly uniform and handmade packets being more variable in size and shape [ 13 ]  . 
for studies making use of ionizing radiation ( conventional / low - dose radiography and ct ) , photon attenuation as demonstrated by radiological density will depend on the type of drug , its purity and the composition of other mixed - in substances [ 14 ]  . 
equally , caution should be taken to estimate the exact number of drug packets within the intestines , especially if there are many , since a very recent study found poor correlation [ 15 ]  . radiography sensitivity for detection of drug packets by initial abdominal x - rays varies widely in the published literature with lower limits suggested to be 40 % and upper limits over 90 % in past decades [ 5 , 8 ]  . 
liquid cocaine furthermore is especially difficult to detect in that it more closely resembles stool owing to flexibility of the packet and lower density of the 1 3 radiol med ( 2015 ) 120 : 118132 content compared to densely packed powder . 
specificity of radiographs is excellent , mostly reported over 90 % , with false positives mainly due to missed interpretation of scybala , calcifications , other foreign bodies 1 3 124 fig . 
duodenal wall thickening with intraluminal fluid ( white star ) and stranding of the peri - duodenal fat ( white arrows ) demonstrates severe duodenitis after possible spill of packet content . 
 case 2 : c axial and b oblique sagittal ct reformat showing cocaine packets of different density ( black stars ) with focal extraluminal intra - peritoneal gas configurations ( white stars ) indicating bowel per foration . 
case 3 : d sagittal reformat of contrast enhanced ct immediately after surgery for ( obstruction / perforation ? ) ( arrows ) shows residual pre - sacral packets ( black stars )  . 
given the low sensitivity of dr and lsdr , the authors conclude that lowdose ct protocols should be further evaluated primarily to reduce radiation exposure in this most reliable test for investigating suspected body packers . computed tomography given the better contrast and spatial resolution of ct when compared to conventional radiography , not surprisingly radiol med ( 2015 ) 120 : 118132 fig . 
b packets located in the pelvis show the double condom sign , made up by air between different layers of packet wrapping , seen between the dense packet content ( stars ) and the outermost wrapping layer ( arrows ) sensitivity and specificity are reported to be much better . 
 all studies performed in the last decade with multidetector ct ( mdct ) demonstrate sensitivity and specificity to be between 95 and 100 % , more or less irrespective of the type of drugs , wrapping material or number of packets [ 4 , 11 , 12 , 1922 ]  . 
the liquid cocaine packets are easily detected by much higher density compared to other tissues , displayed in rectal location ( rectangle in b ) , small bowel and large bowel location ( arrows in c , d )  . 
expulsed packet demonstrating flexibility of wrapping material ( e ) with ct in body packing [ 23 ] ; however , intestinal contrast opacification was used and may have influenced detectability . 
the protocol now most commonly described in the literature in cases of suspicion of body packing , pushing or stuffing is abdominal and pelvic ct without intravenous or intestinal contrast . 
in subjects with clinical concern for bowel obstruction or perforation , intravenous contrast can be given and a routine abdominal and pelvic ct should be performed . the appearance of drug packets on ct varies depending on the type of drug , purity , state and method of wrapping . 
even though pure cocaine may have hu below zero , in our experience cocaine packets are almost always hyperdense due to mixing with other compounds ( see multiple included figures )  . 
the advent of dual - energy ct and scanning with low tube voltage may prove to be helpful with respect to imaging and content assessment [ 27 ]  . the complete intestines from stomach to rectum and in women the vaginal cavity should be evaluated for packets . 
studies that compared ct to abdominal x - rays invariably show much better sensitivity and specificity in the same population [ 4 , 11 , 12 , 1922 ]  . reduced - dose ct the drawbacks of routine abdominal and pelvic ct for screening are cost , availability at the airport and , most importantly , radiation dose . 
b improved visibility with adjusted window / level ( 450 / 170 ) displaying packets ( stars ) , now also visible in stomach ( rectangle ) 1 3 radiol med ( 2015 ) 120 : 118132 fig . 
the lowest estimated dose achieved in our practice is 0.36 msv , resulting in interpretable noisy images , worked up with a more time - consuming full model - based iterative method . 
packets can be seen on both immediately available data as well as less noisy reformats after more time - consuming full modelbased iterative reconstruction data ( arrows in ac )  . 
estimated radiation dose was 0.31 msv ( d ) 1 3 radiol med ( 2015 ) 120 : 118132 one recent study , 31 incidentalomas were found in 18 out of 100 subjects undergoing ct for evaluation of residual packets before discharge from the hospital [ 28 ]  . ultrasound known benefits of ultrasonography in general are the widespread availability , mobility allowing bedside use , relative low cost and importantly the lack of ionizing radiation . 
bowel obstruction may also be visualized . in screening for the presence of intestinal packets , even though meijer and bots [ 29 ] reported over 90 % sensitivity in an airport screening setup , sensitivity of ultrasound is generally thought to be lower than abdominal x - ray , due to the presence of stool and gas in the intestines . 
free intra - peritoneal gas / air would be very difficult to discern on mri images , rendering , in our opinion , mri less useful if bowel perforation as a complication of intestinal obstruction is suspected . 
a long axis ultrasound of classic appearance of drug packet with hyperechoic superficial interface ( arrow ) and lack of posterior ultrasound penetration ( stars ) in cocaine body packer . 
solid - state packets on both t1and t2 - weighted images had signal intensity comparable to air , while liquid content appeared hypointense on t1 - weighted and slightly hyperintense on t2 - weighted sequences . 
scan time ranged 710 m in the one falsepositive case , colonic gas mimicked the form of a packet , which was demonstrated on a ct performed to confirm the diagnosis of one packet . 
two suspects received a true negative interpretation of their mri study . since solid - state packets have signal intensities comparable to air , detection could be difficult , especially in a gas - distended colon . 
 the authors justly conclude that larger further studies are required to investigate the merit of mri . summary intra - corporeal concealment of illicit drugs for international transportation seems to be increasing , despite the health risks involved . 
to minimize morbidity and mortality , as well as to discourage the act of body packing or pushing , imaging is increasingly being used , both for screening for the presence of packets and for investigating possible clinical complications once brought to medical attention . radiologists should be aware of the imaging characteristics and test performances of radiography and ct to minimize false negatives , false positives and maintain good accuracy . 
ct with reduced radiation dose in our opinion will likely be used more in the future , especially since technical advancements will decrease radiation dose levels to the abdominal x - ray equivalent . 
the radiologist , in fact , is asked not only to identify the signs of trauma but also to provide an indication of their clinical significance , suggesting the chance of conservative treatment in the cases of mild and moderate , non - complicated or self - limiting injuries and focusing on life - threatening conditions which may benefit from immediate surgical or interventional procedures . 
biondetti fondazione irccs , dipartimento di radiologia , ospedale maggiore policlinico mangiagalli e regina elena , 20122 milan , italy keywords blunt abdominal trauma bowel injury mesenteric injury blunt intestinal and mesenteric injuries multi - detector computed tomography introduction the bowel and the mesentery represent the structures most frequently involved in blunt abdominal trauma ( bat ) after the liver and the spleen [ 15 ]  . the relative infrequency of such injuries , along with the limited ability of radiologists not sufficiently trained in the field of emergency to recognize their signs at imaging and the scarce specificity of the associated clinical signs and laboratory findings , explains the high rates of delayed and missed diagnoses . 
in particular , proximal 1 3 22 radiol med ( 2015 ) 120 : 2132 jejunum near the ligament of treitz , distal ileum near the ileo - cecal valve , intestinal segments close to bridles and adhesions are mostly exposed to damage being close to points of anatomical or constituted fixity , where mobile and fixed portions of the gut are contiguous and , therefore , susceptible to shearing force [ 13 ]  . colon injury from bat is uncommon ( 20 % ) , being diagnosed in about 0.5 % of all major blunt traumas and in 10.6 % of patients undergoing laparotomy [ 1416 ]  . 
the ascending and descending colon , fixed , partially retroperitoneal segments , are generally exposed to more severe injuries compared to the transverse and the sigmoid colon , wrapped in their own meso and , therefore , characterized by a certain mobility . the duodenum represents the structure less frequently involved in blunt intestinal and / or mesenteric trauma ( bimt , 10 % ) [ 1214 ]  . 
its anatomical features ( mainly retroperitoneal organ , in close contact with the thoracic spine ) explain the peculiarity of diagnostic findings in cases of perforation and the frequent association with signs of pancreatic injury ( isolated duodenal lesions in adults are very rare )  . rapid deceleration represents the primary mechanism of duodenal injury from bat , with visceral tearing at the junction of the intraperitoneal ( free ) and retroperitoneal ( fixed ) portions of the duodenum , such as between the third and fourth portions [ 1 , 5 ]  . pathophysiology of injury the leading cause of intestinal and / or mesenteric injury from bimt is represented by road traffic accidents ( rta , 7085 % ) [ 4 , 14 , 17 , 18 ] , followed by aggressions and falls from heights . with regard to rta , an increase in intestinal and / or mesenteric lesions has been registered after the introduction of seat belts , which compress the intestinal loops at impact creating a closed hollow viscus and cause a sudden increase of the intraluminal pressure resulting in bursting injuries . 
however this technique is limited , as well as by practical factors , by excessive sensitivity for injuries of intraperitoneal organs ( even minor , self - limiting injuries may be emphasized ) , low specificity in assessing the site and the extent of the intraperitoneal damage and lack of sensitivity for traumatic perforations of retroperitoneal viscera . 1 3 radiol med ( 2015 ) 120 : 2132 radiologic studies diagnostic imaging plays an important role in the recognition , evaluation , and follow - up of traumatic bowel and / or mesenteric injuries . 
the broad spectrum of the possible imaging findings is mainly related to the anatomical features of the affected organ , the type and intensity of the traumatic force , and the coexistence of lesions of other abdominal viscera [ 14 , 18 ]  . conventional radiography ( cr ) sections can potentially improve the accuracy of mdct in the detection of bowel and / or mesenteric injury [ 3437 ]  . for these reasons , the above - mentioned cr and us remain limited to very selected conditions to date ; us , in particular , may be of some utility in the follow - up of patients with peritoneal fluid from bowel and / or mesenteric injury , initially evaluated with mdct . mdct study protocol identification of extraluminal free air in the case of traumatic perforation of a hollow viscus , and evidence of changes in caliber and tone of intestinal loops ( so called acute intestinal behaviors ) [ 24 ] represent , to date , the only rationale for cr in the acute patient with suspected bimt . in the era of mdct , all exams must be performed with a high - resolution protocol , with slice thickness and a reconstruction interval values equals to 1 mm , and completed by multiplanar reconstructions [ 4 , 14 , 17 , 18 ]  . ct scans before contrast medium administration are essential in patients with suspected bimt for several reasons : ultrasonography ( us ) at f.a.s.t. 
assessment , now universally accepted as valid tool in the initial evaluation of the patient with suspected injury of the abdominal viscera , even small amounts of peritoneal fluid from bowel and / or mesenteric injury may be identified . 
according to the whole body ct protocol for trauma , an acquisition in the late phase , 35 min after starting the infusion , may be useful to rule out low - flow active bleeding [ 4 , 14 , 38 , 39 ]  . in the past decades , usefulness of oral contrast medium administration in patients with suspected bowel and / or mesenteric injury was the subject of controversy between various centers . 
moreover , the administration of oral contrast material in the emergency patients with suspected bimt represents a potential source of pitfalls and misdiagnoses : the spread of the iodine - based , endovenous contrast medium from an intraperitoneal traumatic rupture of the bladder may mimic the spillage of the oral contrast material from intestinal loops and extraluminal oral contrast material from injured bowel loops may mimic extravasated contrast medium from ruptured vessels [ 4 , 14 , 4043 ]  . features and ct classification of traumatic intestinal injuries the effects of a trauma on the intestine depend on several factors : the type of traumatic force itself , the anatomical features of the intestinal segment on which the force acts , the degree of distension of the lumen , and the type of intestinal contents ( a high content of dietary fibers is a recognized risk factor )  . traumatic injuries of the bowel can be classified , according to a prognostic criterion , into major and minor [ 44 ]  . the only major intestinal injury is the full - thickness tear of the intestinal wall resulting in the spillage of enteric contents into the abdominal cavity : a continuity is created between the septic intraluminal ambient and the peritoneal cavity with consequent risks of chemical peritonitis . 
these conditions demand proper and timely interventions in the quickest time possible [ 12 ]  . minor intestinal injuries are represented by incomplete tears of the intestinal wall , intramural hematomas , and parietal contusions ; such alterations of the bowel wall , although may rarely evolve into a secondary perforation due to focal - segmental metabolic and / or vascular disorders , are now widely managed non - operatively [ 45 ]  . 
a axial mdct scan shows a focal interruption of the parietal lining of the proximal - middle descending colon on its lateral aspect , with evidence of an air nucleus adjacent to the wall ( arrow )  . 
flexiondistraction fractures of l1l2 ( so called chance fracture ) have been reported in association with duodenal intramural hematomas [ 13 , 14 , 18 ]  . in case of duodenal involvement , bowel thickening may be observed in association with fluid in the anterior pararenal space , making it challenging to differentiate a wall hematoma from a traumatic duodenal perforation . 
in a limited percentage of cases complications are observed in the form of luminal stenosis or obstruction [ 4649 ]  . nonspecific ct signs of traumatic intestinal injuries extraluminal air collection ( intraperitoneal , mesenteric or retroperitoneal ) free extraluminal air represents a non - specific but highly suggestive sign of intestinal injury from bat [ 26 , 30 , 33 ]  . 
 when observed even in the absence of specific ct signs ( interrupted intestinal wall , extraluminal spillage of enteric contents , intramural hematoma ) , a bowel injury should always be sought . 
this sign may suggest the site of a bowel injury . a traumatic perforation of the duodenum and of the dorsal sides of the ascending and descending colon may cause a pneumoretroperitoneum : extraluminal air extends through the fascial planes and may dissect them , being so detectable even at a great distance from the site of perforation . as a general rule , in all patients with suspected hollow viscus injury from bat , ct images should be reviewed with lung or bone window settings , in addition to the routine soft tissue ones , to assess even small amounts of free abdominal air . intraperitoneal fluid in most of the cases , intraperitoneal fluid may be the only sign of a significant bowel injury at the first ct evaluation 1 3 26 radiol med ( 2015 ) 120 : 2132 fig . 
c axial scan and d minip axial reformation image shows small air nuclei ( arrows ) behind the posterior aspect of the ventral parietal peritoneal sheet in the right iliac fossa . 
therefore , management of patients with intraperitoneal fluid as the sole finding on ct scans includes 68 h follow - up ct examination , depending on the clinical context [ 29 , 51 , 52 ]  . non - physiologic amounts of free intraperitoneal fluid ( > 75 ml in minimally resuscitated women of child bearing age , > 25 ml in minimally resuscitated adult males and > 25 ml in children ) without evidence for intraperitoneal solid organ injury raises the suspicion of occult hollow viscus injury [ 29 , 51 , 52 ]  . distribution of fluid collections may indicate potential organ injury involvement . 
in the case of a serosal laceration , in fact , blood spreads through the mesenteric folds with a v - shaped morphology , with the base corresponding to the loop and the apex to the mesenteric root . 
mesenteric infiltration is also appreciable ( arrowhead ) origin of a peritoneal fluid collection may be also deduced from its densitometric characteristics : a lowdensity collection ( average densitometric values lower than 20 hu , comparable to those of the bile inside the gallbladder or of the urine in the bladder ) suggests spillage of fluid from the intestine , a medium - density collection ( > 25 hu ) in general largely consists of extravasated 1 3 radiol med ( 2015 ) 120 : 2132 interpreted as a sign of intestinal traumatic injury , being only apparent , caused by the stratification of the intestinal contents [ 55 ]  . shock bowel represents a transient condition source of false positivity for post - traumatic bowel wall thickening in patients with bat : diffuse parietal thickening , fluid distension of the loops , and increased bowel wall enhancement may be secondary to deep hypotension with hypoperfusion complex . 
b air nuclei are appreciable in the axial scan in the window setting ( arrows ) blood , and a high - density collection ( > 120 hu ) is attributable to extravasation of contrast medium from damaged vessels or to the spillage of oral contrast material through bowel wall full - thickness tears [ 14 , 54 ]  . 
a non - circumferential parietal thickening , limited to the declivous side of the loop should not be 1 3 28 acute intestinal behaviors variations in tone , motility , shape , and location of the intestinal loops may represent the first hint of a small bowel or colonic traumatic injury even in the absence of small amounts of free fluid and air [ 24 ]  . in most of the cases , reflex spastic ileus ( rsi ) due to per sistent contracture of bowel with a complete absence of intestinal gas is the first sign in order of appearance . 
when hyper tonic spastic reaction ends , the bowel loops relax and the tone decreases leading to reflex hypotonic ileus ( rhi ) [ 24 ]  . rsi and rhi are characterized by an intrinsic evolutivity and should not be considered as separate entities , with the transition of each of these in the other at any time in response to internal or external stimuli [ 24 ] being possible . features and ct classification of traumatic mesenteric injuries mesenteric injuries include a broad spectrum of traumatic findings from simple contusion to mesenteric avulsion . in the majority of the cases traumatic lesions of the mesentery are isolated , rarely associated with lesions of the intestine and parenchymal organs [ 31 , 57 ]  . 
similarly to traumatic bowel injuries , mesenteric injuries are distinguished , based on a surgical and prognostic criterion , in major and minor [ 31 ]  . major mesenteric injuries , essentially represented by active blood extravasation , avulsion of the meso resulting in intestinal ischemia and full - thickness tear of the meso , require urgent operative treatment . minor lesions include partial lacerations of the meso , focal mesenteric contusions , and the stable mesenteric hematomas ; these conditions are treated conservatively , with a careful clinical and instrumental observation . also for mesenteric traumatic injuries specific and non - specific ct signs are described [ 14 , 18 , 30 ]  . 
specific ct injuries are essentially represented by avulsion of a meso resulting in ischemic changes of the loop , active bleeding , and mesenteric hematoma , while nonspecific ct signs include mesenteric infiltration and fluid collections . specific ct signs of traumatic mesenteric injuries avulsion of the meso with intestinal ischemia an injury to the meso in correspondence to its insertion on the intestinal loop , manifesting at ct as a triangular - shaped radiol med ( 2015 ) 120 : 2132 fig . 
b axial mip reformation in the same patient better depicts the refurnished hematoma within the meso ( arrow ) fluid collection , with the base corresponding to the loop and the apex facing towards the mesenteric root , may compromise the vascular supply of the loop . 
therefore , in this condition , mesenteric anomalies at ct are associated with signs of intestinal ischemia , varying depending on the severity of the injury , the vessel involved ( arterial , venous or combined injury ) and the mechanisms of compensation [ 33 ]  . 
axial scans in the arterial ( a ) and venous ( b ) phases of the exam show conspicuous increase in the amount of the extravasated contrast medium in the time interval between the two phases . 
 mip coronal image depicts the contrast medium blush from the mesenteric arterial tree ( c ) ( specificity rates of 100 % ) [ 54 ] , suggests the need for an urgent operative treatment . in cases of mesenteric traumatic injury resulting in active extravasation , significant traumatic forces are gener ally involved . 
for this reason potential major lesions of the adjacent loops should be carefully excluded [ 54 ]  . mesenteric hematoma as written , traumatic tears of the walls of mesenteric vessels are associated with the appearance of a mesenteric hematoma , whose management varies significantly depending on its degree of stability ( we define stable a not - refurnished , contained hematoma , without signs of active bleeding in the vicinity )  . 
 when associated with a focal - segmental thickening of the intestinal wall , this densitometric alteration of the mesentery is suggestive of ischemic sufferance of the intestine due to injury of the afferent or efferent vessels . free abdominal fluid free abdominal fluid represents the non - specific sign most frequently associated with bimt . 
in the absence of traumatic injuries of abdominal parenchymatous organs , as a general rule , detection of free abdominal fluid , especially if hyperdense , a bimt should always be excluded through the search of possible associated signs . analogous to what described for intestinal lesions , abdominal fluid from a mesenteric traumatic injury fig . 
c a later , venous acquisition highlights the spread of the extravasated contrast medium among the loops usually assumes a peculiar distribution , between the intestinal loops and / or within the mesenteric sheets , forming polygonal - shaped collections . 
in the case of injury of the serosal surface of the loop , a typical v - shaped triangular collection appears , with the base corresponding to the base of the loop itself and the apex directed towards the mesenteric root . 
as already written , the density of this collection at basal scans may indicate its nature and provenance . retroperitoneal fluid collections tend to remain confined for a longer time at ct controls compared to peritoneal collections [ 53 ]  . 1 3 radiol med ( 2015 ) 120 : 2132 conclusions clinical assessment alone of patients with suspected intestinal and / or mesenteric injury from bat is associated with unacceptable diagnostic delays . 
focused assessment with sonography for trauma is widely used to detect free intra - abdominal fluid , but its role is controversial , because the absence of free fluid does not exclude the presence of injuries to abdominal organ . 
thus , in trauma patients , following early assessment with conventional us imaging , a contrast - enhanced us ( ceus ) can provide a more reliable evaluation of solid organ injuries and related vascular f . 
ceus cannot replace abdominal ct , but it represents a noninvasive and repeatable imaging tool capable of providing a reliable assessment of trauma severity and expedite the patients treatment . keywords ultrasound contrast media trauma emergency radiology introduction on admission , patients with blunt abdominal trauma are usually investigated with us to exclude the presence of free abdominal fluid [ 1 , 2 ]  . 
this method is referred to as focused assessment with sonography for trauma ( fast ) , and it has been formally incorporated into the trauma protocol [ 1 , 3 , 4 ]  . 
fast enables a reliable identification of haemoperitoneum : its sensitivity , specificity , and overall accuracy in detecting free fluid have been reported to be 8194 , 88100 , and 8698 % , respectively [ 4 , 5 ]  . 
however , this technique requires the operators expertise [ 6 ] ; moreover , injuries to solid organs can be overlooked at conventional us and free abdominal fluid may be missing in patients with traumatic abdominal injuries . 
accordingly , to provide a complete assessment of patients sustaining severe trauma , contrast - enhanced ct represents the most used and sensitive imaging modality [ 7 ] : nevertheless , to decrease unnecessary radiation exposure , a limited use of ct in selected series , such as paediatric patients , females of reproductive age and low - energy trauma patients has been advocated [ 5 ]  . 
to overcome this dualism , in the last decade , a new us technique has been developed using new generation us contrast agents ( ucas ) [ 812 ] , with the possibility of recognising or excluding abdominal solid 1 3 radiol med ( 2015 ) 120 : 311 fig . 
1 18 - year - old male admitted to hospital after a motor vehicle accident : a conventional ultrasound ( us ) shows an inhomogeneous hyperechoic area in the right lobe of the liver . 
 after illustrating the ceus findings of traumatic injuries to abdominal organs , this review article will discuss the possible role of this technique in the assessment of blunt abdominal trauma in the stable patient . contrastenhanced ultrasound ( ceus ) technique ( liver , pancreas , spleen and kidneys )  . 
the examination is stored as a movie and can be carefully evaluated at the end of the procedure . the ceus technique can be carried out in a variety of scenarios , including bedside , operating room , and trauma suite . 
ceus skills can be acquired after 4050 examinations , after which most radiologists become confident in the technique [ 16 ]  . ucas commonly used in our practice consist of stabilised gas microbubbles , of 110 m of diameter , surrounded by a phospholipid shell [ 14 ]  . 
then a bolus of 1.22.4 ml of uca is administered , depending on available equipment , followed by a 5to 10 - ml saline flush via a cannula in the antecubital fossa . 
a total of 36 min is required for investigating all the solid abdominal organs normal abdominal organ enhancement microbubbles are blood pool agents that remain within the vessels , both in macroand in micro - vascularity without interstitial extravasation . 
this feature , in addition to specific software using dynamic low mechanical index ( mi ) [ 17 ] , enables differentiation of the signal between background tissue and gas - filled microbubbles , without bursting the latter . 
ceus findings mainly overlap those obtained at ct and magnetic resonance ( mr ) during arterial phase imaging , but there is no similarity in the venous and the delayed phases , because ct and mr contrast 1 3 radiol med ( 2015 ) 120 : 311 fig . 
e 3 months later , the follow - up t1 - weighted magnetic resonance ( mr ) sequence with fat suppression shows the well - demarcated haematoma , surrounded by an hyperintense rim , due to fibrous reparative tissue media spread out into the extravascular interstitiu at ceus , the arterial phase starts approximately after 10 20 s and proceeds up to 3040 s . 
this phase is followed by the venous and the late phases , in which the contrast agent is distributed to the whole capillary bed and the concentration slowly decreases followed by the removal of contrast agent through the lungs . 
while inaccurate timing of ct or mr acquisition phases may result in the inadequate characterisation of a focal parenchymal injury , ceus allows continuous depiction of the lesion through all the vascular phases . contraindications and adverse reactions major contraindications include right - to - left shunts , severe ( pulmonary artery pressure pulmonary hypertension > 90mmhg ) , uncontrolled systemic hypertension , and patients with adult distress syndrome . ucas are widely marketed and used in the clinical practice throughout europe and in some eastern asian countries . 
ucas do not interact with the thyroid gland . finally , because of absence of renal excretion , they are not nephrotoxic , so that ucas can be safely employed in patients with renal insufficiency . 1 3 6 radiol med ( 2015 ) 120 : 311 fig . 
because of its dual vascular supply , the hepatic phases after the arterial phase include the portal phase ( 30120 s after contrast injection ) and the sinusoidal ( or late ) phase ( 120300 s after contrast injection ) [ 24 ]  . 
although uca injection does improve the sensitivity of conventional us imaging for identification of renal injuries , the role of this technique has to be still clarified : in fact , injury to the renal collecting system may be overlooked at ceus because of a lack of urinary excretion of microbubbles . pancreas after the contrast agent injection , the pancreas shows a mounting enhancement of its intensity . 
injury to the pancreas is relatively uncommon , occurring in < 2 % of blunt abdominal trauma : nevertheless , due to its anatomic location , mortality is quite high . 
in the first case , a 5 - year - old child was diagnosed with a laceration of the pancreatic tail ; in the second case , a 53 - year - old male patient suffered from a contusion of the pancreatic head . discussion ct has extreme importance for evaluating traumatised patients in that it provides not only a fully comprehensive assessment , but it can also grade trauma severity and help decide on the most appropriate patient management [ 34 , 35 ]  . 
nevertheless , despite the latest dose reductions of state - of - the - art ct scanners , today a large number of otherwise healthy patients with minor blunt abdominal trauma are subjected to ct radiation to rule out abdominal injuries . 
 reducing the radiation burden is crucial to this concept and the use of the safest method is paramount . to overcome these limits , selective replacement of ct by ceus examination has been advocated [ 36 ]  . 
ceus can be intended as a useful imaging method to be used between conventional us and ct , in that it provides additional data not achievable with conventional us imaging and can reduce radiation exposure . 
the use of ceus in children is still considered off - label , and it is allowed only after the parents ( or legal guardians ) have been adequately informed and given their specific consent . 
b ct confirms this finding kidney following contrast administration , normally the kidneys have a rapid , intense , and provisional enhancement , as a consequence of lacking glomerular filtration . 
in particular , ceus has been found to detect 8081 % of traumatic renal parenchymal injuries demonstrated at ct 1 3 8 radiol med ( 2015 ) 120 : 311 fig . 
c ceus , in the early arterial phase , reveals a splenic laceration ( arrow ) , with multiple haematomas ( arrowhead ) and haemoperitoneum ( void arrow )  . 
b cect confirms a grade i rupture of the pancreas the us contrast media in children [ 30 , 3639 ] , and several international paediatric and radiological societies are pushing for its wider registration , including paediatric use [ 40 ]  . 
in nontrauma series , ceus costs proved to be lower than those calculated for contrast - enhanced ct and contrast - enhanced mr [ 41 , 42 ]  . in trauma patients , ceus outperforms conventional us for the detection of abdominal solid organ injuries [ 4345 ]  . 
 in particular , it improves the detection of traumatic lesions allowing a better definition of the extension to the organ capsule , which is an important criterion for surgical evaluation [ 46 ]  . 
 [ 28 ] showed , in a large series , that conventional us at admission had a sensitivity of 41 % in revealing an abdominal traumatic injury , while the detection rate rose to 60 % at conventional us performed after ct , and up to 76 % at ceus imaging . 
moreover , in isolated blunt abdominal trauma , ceus has proven to be more accurate than conventional us imaging in determining the number and size of injuries ; in the evaluation of retroperitoneal solid organs , valentino et al . 
 [ 30 ] missed no major renal injury in their trauma patient series . with regard to grading post - traumatic abdominal solid organ injuries , to our knowledge , no paper has yet shown how ceus can grade traumatic injuries according to the organ injury scaling provided by the american association for the surgery of trauma [ 47 ]  . 
 [ 49 ] compared the value of ceus versus contrast - enhanced ct for the detection of different grades of solid organ injuries in blunt abdominal trauma in animals , with high levels of concordance between the ct and ceus findings . emergency ceus has a number of limitations to be considered : the lack of panoramic view typical of ct and the fact that it does not allow a complete abdominal survey . 
in addition , it does not usually allow the rescue of a nondiagnostic us examination ; difficult patients , including those with obesity , gas - containing collections , subcutaneous emphysema , and abdominal wall obstacles ( wounds , medications , colostomies , enterostomies , and drainages ) are difficult to scan . 
finally , ceus , like conventional us imaging , cannot depict some types of lesions , including diaphragmatic ruptures , bowel or mesenteric traumatic injuries . there is still debate as how to integrate ceus in the trauma patient workup [ 28 , 43 , 48 ] : after being tested in trauma practice for more than a decade , this technique may now have an important role in the prompt evaluation of the stable patient sustaining blunt abdominal trauma . 
current indications include ceus in the follow - up of trauma patients conservatively managed until discharge [ 23 , 50 ] , both in order to reduce unnecessary ct examinations and to overcome poorly visible traumatic injuries at conventional us , better revealed using microbubbles . 
 a multicentric study oliviero caleo giorgio bocchini sonia paoletta anna maria ierardi alessandra scionti michele tonerini franco guida giacomo sica alessandra perillo gianpaolo carrafiello mariano scaglione received : 14 september 2014 / accepted : 28 november 2014 / published online : 9 january 2015 italian society of medical radiology 2014 abstract purpose the purpose of this multicentric study is to assess the usefulness of multiphasic computed tomography in the identification of spontaneous non - traumatic retroperitoneal hematoma ( srh ) and its management , with references to the role of interventional radiology . materials and methods from january 2011 to june 2014 , 27 patients with srh were selected . 
scaglione department of radiology , po pineta grande , castel volturno , italy results ct identified srh in all cases ( 100 % ) , showing the source of bleeding in 11 cases ( 40 % ) and pointing out the source of bleeding in 15 cases ( 55 % )  . 
ct has identified a contrast medium extravasation in the arterial phase in 17 patients ( 63 % ) , treated successfully by percutaneous embolization in 13 and by open - surgery in two cases . 
ten patients ( 37 % ) were non - operatively treated successfully with clinical , laboratory , and imaging follow - up . conclusions multiphasic ct is the gold standard for the identification of a srh . 
technical skill , expertise , and recognition of ct signs of arterial active bleeding are critical features influencing patients management . keywords spontaneous retroperitoneal hemorrhage computed tomography ( ct ) computed tomography angiography ( cta ) digital subtraction angiography ( dsa ) retroperitoneal hemorrhage management introduction g . 
sica uo radiologia , ospedali riuniti della valdichiana , stabilimento ospedaliero di nottola , montepulciano , siena , italy spontaneous retroperitoneal hemorrhage ( srh ) without aortic rupture , trauma , or iatrogenic causes represents a 1 3 134 table 1 correlation between ct imaging , treatment and final diagnosis case age anticoagulant ct diagnosis of bleeding emergency treatment final diagnosis ct arterial active bleeding pancreatico - duodenal artery pancreatico - duodenal artery aneurism yes pancreatico - duodenal artery no / venous conservative confirmed / exitus before dsa radiol med ( 2015 ) 120 : 133148 confirmed / exitus during surgery pancreatico - duodenal artery pancreatico - duodenal artery right subphrenic artery left subphrenic artery sacral artery renal artery aneurysm renal artery aneurysm - mav obturator artery obturator artery right testicular artery lumbar artery lumbar / ileo - lumbar artery lumbar artery ileo - lumbar artery ileo - lumbar artery renal cystic lesion renal malignant neoplasm renal malignant neoplasm renal malignant neoplasm renal angiomyolipoma adrenal metastasis adrenal carcinoma renal cystic lesion , polycystic kidney no / venous no / venous angiography angiography angiography conservative angiography angiography angiography surgery angiography angiography angiography angiography angiography angiography conservative angiography conservative conservative conservative surgery conservative conservative conservative surgery angiography conservative confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed confirmed left subphrenic space , uncertain origin yes adrenal metastasis rare and insidious condition that recognizes different etiologies [ 1 ]  . 
most frequent causes are parenchymal diseases related to vascular rupture of retroperitoneal organ expansive lesions , most often spontaneous rupture of renal carcinomas and angiomyolipomas [ 2 ] and adrenal expansive lesions [ 3 ] ; further causes include vascular diseases related to the rupture of splanchnic artery aneurysms or small vessels injuries [ 46 ]  . 
according to the etiology , symptoms may vary from mild abdominal pain to acute abdomen until cardiovascular collapse [ 1 ]  . ultrasound ( us ) and plain film of the abdomen provide insufficient and often non - specific diagnostic information . 
 multidetector computed tomography ( mdct ) plays a primary role because of its ability to identify , with high sensitivity and specificity , the presence and cause of hematomas into the retroperitoneal space , significantly influencing the subsequent management [ 7 ]  . current literature is mainly focused on classification of etiologies and clinical management of the disease . 
the current multicentric study has the primary purpose to assess the usefulness of mdct in the diagnosis of srh , pointing out how ct can influence patients management approach . materials and methods from january 2011 to june 2014 , we retrospectively evaluated data of four emergency radiology departments , selecting patients who performed a ct examination for suspected retroperitoneal hemorrhage . 
1 a 51 - year - old man suffering severe left flank panon - contrast enhanced ct scan shows a hyperdense fluid collection , with well - defined margins , in the left kidney ( a ) , associated with fluid in the adjacent perinephric space . 
the multiphasic ct study after intravenous injection of iodinated contrast material in the arterial ( b ) , portal ( c ) , and delayed phases ( d ) allows classifying the lesion as intraparenchymal hematoma due to the spontaneous rupture of a large cystic lesion . 
the patient was treated conservatively and underwent follow - up with ct and us bolus tracking technique , followed by a portal phase at about 70 s from the beginning of the injection of the contrast mediua delayed phase at 180300 s has been done in all patients for characterization of vascular lesions or differentiation between vascular and urinary injuries . 
postprocessing techniques were routinely performed with multi planar reconstruction ( mpr ) and maximum intensity projection ( mip )  . digital subtraction angiography ( dsa ) was performed using a c - arm angiography system ( philips allura xper fd 20 )  . 
2 a good health 45 - year - old man admitted with left lumbar pa ct scan shows a large perirenal hematoma secondary to the rupture of a large , inhomogeneous fatty - like mass within the middle and lower third portion of the left kidney in keeping with an exophytic angiomyolipoma ( a )  . 
different embolic materials were used : microcoils , absorbable gelatin sponge , glue , and polyvinyl alcohol ( pva ) microspheres . dsa was performed at the end of each procedure to confirm the cessation of the bleeding . all patients were clinically monitored and followed up with a ct scan or ultrasound in an interval period between 2 days and 2 months . results cause of the bleeding was properly vascular in 18 patients ( 67 % ) and parenchymal in nine cases ( 33 % ) as detailed in table 1 . ct allowed a rapid diagnosis of retroperitoneal hemorrhage in all cases ( 100 % )  . 
the multiphasic ct study demonstrates a large para - duodenal hematoma secondary to the rupture of an aneurysm in the territory of the pancreatic - duodenal arch ( a ) , with signs of active bleeding ( b )  . 
mip reconstruction image in the coronal plane ( e ) gives a further perspective of the abovementioned findings , allowing optimal depiction of other smaller aneurysms distributed along the branches of the hepatic artery . 
however , in one case ( 5 % ) , the bleeding origin was not recognized at ct , identified at surgery as small 1 3 138 radiol med ( 2015 ) 120 : 133148 fig . 
4 a 75 - year - old woman submitted to chronic antiplatelet treatment suffering severe epigastric and right flank pa the ct scan shows a heterogeneously hyperdense retroperitoneal collection with contextual fluidfluid levels ( a )  . 
the axial ct scan acquired in the arterial phase demonstrates signs of active bleeding ( b ) with evidence of the so called signal flare sign ( c )  . 
5 a 62 - year - old man suffering sudden epigastric pa noncontrast axial ct scan ( a ) shows a well - defined fluid collection with blood density values ( mean 50 hu ) adjacent to the second portion of the duodenu the ct scans in the arterial ( b ) , portal ( c ) , and delayed phases ( d ) show no signs of active bleeding . 
therefore , the patient was successfully treated conservatively and underwent clinical and instrumental follow - up ten patients ( 37 % ) with srh were treated non - operatively with clinical and laboratory monitoring and followup with ct or ultrasound examinations , until resolution of the hematoma . 
particularly , in three cases , ct showed signs of active venous low - flow bleeding , detectable only in the portal phase and , for this reason , patients received a non - operative management . 
ct revealed retroperitoneal hematomas without active bleeding in remaining seven patients . discussion spontaneous retroperitoneal hemorrhage is a rare disease associated with data limited to case reports and small case series , with a prevalence in elderly patients undergoing chronic antiplatelet or anticoagulant treatment [ 4 ] or dialysis [ 8 ]  . 
they can be represented by general abdominal pain in the epigastric region , in the region of the hips or radiated to the lumbar region , pelvis , and legs [ 24 ]  . 
in cases of massive spontaneous bleeding , with initial onset of cardiovascular decompensation , suspicion of bleeding is more suggestive . main causes can be essentially divided into parenchymal bleeding and vascular bleeding . parenchymal bleeding parenchymal bleeding is often related to renal or adrenal injuries . wunderlichs syndrome is a clinical condition defined as a spontaneous renal bleeding of non - traumatic origin [ 9 ]  . 
ct scan clearly depicts both the primary tumor and signs of spontaneous rupture [ 13 ]  . cases of spontaneous rupture of adrenal masses include pheochromocytoma [ 14 ] , myelolipoma [ 15 ] , cortical adenoma , adrenocortical carcinoma , and metastases [ 16 ]  . 
ct of adrenal hemorrhage appears as a round solid adrenal mass with attenuation comparable to soft tissue , which decreases 1 3 140 radiol med ( 2015 ) 120 : 133148 fig . 
6 a 51 - year - old man suffering severe left flank pa arterial phase ct scan shows a circumscribed high - density fluid collection in peri - pancreatic space without signs of medium contrast extravasation ( a )  . 
ct scan performed 1 week later in arterial ( c ) and portal ( d ) phases illustrates spontaneous cessation of bleeding in size during follow - up [ 17 ]  . 
mr is very sensitive and specific for diagnosing adrenal hemorrhage and determining if blood is the sole component of the hematoma [ 18 ]  . vascular bleeding primary causes of vessel injuries include rupture of splanchnic arteries aneurysms [ 19 , 20 ] , arteriovenous malformations [ 21 ] , or disease resulting from atherosclerotic or inflammatory small vessels injuries [ 22 , 23 ] with a prevalence in patients with antiplatelet agents or anticoagulants [ 1 ]  . 
in these patients , ct can identify the presence of aneurysmal dilatation and vascular abnormalities or suggest the origin related to the site of hematoma and of contrast extravasation [ 1924 ]  . current literature reports more frequently rupture of aneurysms and pseudo - aneurysms of the superior mesenteric artery branches , renal artery aneurysms , and pancreatic - duodenal artery aneurysms , the latter often associated with stenosis of the celiac artery [ 2531 ]  . lumbar , ileo - lumbar and obturator artery were identified as source of bleeding in six patients ; these sites represent fig . 
7 a 85 - year - old man submitted to anticoagulant and antiplatelet therapy due to venous deep thrombosis and pulmonary embolis arterial ( a , b ) and venous ( c ) phase scans show active bleeding in more than one area ( arrows )  . 
angiographic scans after positioning of two microcoils of 3 - mm injection of spongeal and a 4 - mm vascular plug ( f ) and one microcoil of 2 - mm injection of spongeal showing the stoppage of bleeding ( g )  . 
axial ct ( h ) , coronal ( i ) , and sagittal ( j ) images performed after 2 weeks before patients discharge confirmed the evidence of organized hematoma , without blushing or signs of infection other sources of non - traumatic retroperitoneal hematoma frequently described in the literature [ 2527 ]  . imaging x - ray and ultrasound examination are often the first imaging examination for patients with mild to moderate symptoms as pain in the epigastric region , hips , and back . 
tract perforation and for identification of other more common causes of acute abdomen , especially if related to 1 3 radiol med ( 2015 ) 120 : 133148 1 3 142 radiol med ( 2015 ) 120 : 133148 fig . 
known limits of us in the evaluation of the retroperitoneum are generally related to meteoric distension of the intestinal loops and poor patients cooperation in the majority of cases [ 735 ]  . ct scan is usually performed in patients with drugresistant pain symptoms or in case of uncertain ultrasound diagnosis ; more often , a ct scan is performed as the first exam to quickly get the correct diagnosis of any intra and / or retroperitoneal disease in patients with severe symptoms , worsening of hemodynamic conditions , or clinical suspicion of an abdominal bleeding source . 
for this reason , ct plays a primary role in the detection of retroperitoneal bleeding , its location , size , and source , with high sensitivity and specificity [ 1 , 3 , 7 , 34 ]  . 
some authors have highlighted the importance of a deep knowledge of the anatomy of the retroperitoneal fascial planes [ 36 ]  . the execution of ct with injection of intravenous contrast with multiphase acquisitions is an essential issue both for early diagnosis and management of patients with suspected abdominal and / or retroperitoneal bleeding , allowing optimal detection and characterization of vascular structures [ 3639 ]  . at baseline acquisition , a recent hematoma appears as a soft tissue density mass ( 3050 hu ) that sometimes displaces the adjacent structures . 
in the first hour after bleeding , an area of higher density surrounded by serum of relatively lower density , the sentinel clot sign , may suggest the bleeding site [ 37 , 38 ]  . 
furthermore , ct can help detection of contained vascular lesions such as aneurysms or pseudo - aneurysms within a hematoma . a technically correct ct exam allows , with high diagnostic confidence , to exclude significant arterial supply in the context of a hematoma . 
this distinction is essential from a management view - point [ 41 ]  . on ct - angiography imaging , hemorrhage is defined as free extravasation of contrast media that persist and enlarge on delayed images and pseudoaneurysm as a round or ovoid cavity , communicating with an injured vessel wall , that shows wash out on delayed phase . 
arteriovenous fistula is defined as early , simultaneous vessel enhancement of both artery and vefrom a therapeutic view - point , arterial active bleeding lesions can be safely treated with angiographic embolization . 
on the other way , exclusion of a significant arterial supply in the context of a hematoma initially addresses the patient toward a nonoperative management , with laboratory and instrumental 1 3 radiol med ( 2015 ) 120 : 133148 fig . 
non - contrast ct scan demonstrates a large retroperitoneal hematoma in the context of the iliopsoas muscle , with excellent representation of the hematocrit effect , a blood - plasma level seen with acute re - bleeding into an older blood collection ( a )  . 
arterial phase ct scan shows an active bleeding in more than one area ( b , arrows ) , with signal flare , corresponding to the layering of the contrast medium between cellular and fluid component . 
actually , in these patients , dsa is recommended [ 4244 ]  . several studies on vascular traumas support the notion that a rigorous multiphase ct technique can address patients to a tailored managementi.e. , intervention , surgical or conservative [ 4548 ]  . 
our data also show a high prevalence of active arterial bleeding among patients with retroperitoneal hematoma with source of vascular origthis finding supports the relationship that exists between this event and a small vessels chronic disease [ 47 ]  . conclusions spontaneous retroperitoneal bleeding represents a pathological entity of difficult clinical classification , in which early diagnosis is crucial to prevent a severe involvement of clinical conditions . 1 3 144 radiol med ( 2015 ) 120 : 133148 fig . 
axial ct scans show active bleeding in the context of the right rectal muscle ( a , arrow ) and the obturator muscle ( b , arrow ) , respectively . 
digital substraction angiography confirms the presence of active bleeding from right inferior epigastric artery ( c ) and from a branch of the right obturator artery ( d ) respectively . 
ultrasonography performed after 1 month illustrates organized hematomas of the right rectus muscle ( g ) and of the obturator muscle ( h ) , respectively 1 3 radiol med ( 2015 ) 120 : 133148 fig . 
10 a 50 - year - old man affected by hiv and acute renal failure with acute severe right back panon - contrast axial ct scan shows a large high - density fluid collection in the anterior right para - renal space ( a )  . 
the selective catheterization of the right testicular artery documented the presence of at least 2 minute areas of contrast medium leakage at the level of the proximal third of the artery ( e )  . 
embolization of the proximal tract of the artery with metallic coils and spongostan results in vessel occlusion with absence of persistent signs of arterial bleeding ( f ) multiphasic ct is the gold standard for the identification of a spontaneous retroperitoneal hematoma . 
11 a 67 - year - old man admitted to the er with dyspnea and acute back pa multiphasic ct scans at baseline ( a ) , arterial ( b ) , portal ( c ) , and delayed phases ( d ) depict the presence of a large retroperitoneal hematoma spreading toward the subphrenic space with signs of contrast medium active extravasation . 
the mpr reconstruction images in the coronal ( d ) and sagittal ( e ) planes also demonstrate the presence of an unsuspected , large exophytic neoplastic lesion at the middle third of the left kidney . 
injection of a contrast medium may give to the radiologist additional information to that obtained at baseline us and doppler examination , since real - time , contrast - enhanced us ( ceus ) may allow observing findings in the abdomen not recognizable at baseline us or even at color doppler imaging . 
the purpose of this review is to illustrate the possibilities and limitations of abdominal ceus in the acute setting , with special emphasis on the detection and characterization of acute inflammatory processes , infarcts , and hemorrhages . keywords ultrasound contrast - enhanced ultrasound emergency abdomen introduction injectable , second - generation solution of sonography ( us ) contrast media is prepared very quickly and is immediately administrable . 
additionally , these agents are very well tolerated and can be injected in patients with hypotension , shock , renal failure , and other acute conditions , without any need for fasting or preliminary laboratory testing . 
the commercialization of transportable scanners with ceus facilities allows using this imaging modality in a variety of scenarios and locations , ranging from the radiology department to the operation room to the bedside . 
however , a wide spectrum of clinical applications has been assessed by now in a number of publications and some very definitive opportunities have been established . in this article , we review the possibilities and limitations of abdominal ceus in the non - traumatic emergency setting , focusing on a number of major clinical scenarios such as acute inflammation , ischemia , and hemorrhage . 
petrillo department of radiology , national cancer institute fondazione pascale , 80131 naples , italy e - mail : orlandcat@tin.it a reasoned , selective use of ceus can allow obtaining a quick and effective diagnosis . 
the choice for injecting the microbubbles solution should be based on the clinical and laboratory data as well as on the initial us and color doppler findings color and power doppler technique should always be employed first , to better assess any indeterminate 1 3 74 radiol med ( 2015 ) 120 : 7384 us finding , particularly in the case of vascular abnormalities . 
infarctions , abscesses , hemorrhages , and other acute abnormalities are better or solely identified or fully understood with ceus adjunct . injection of a contrast medium may give the radiologist relevant additional information , useful for the diagnosis and therapeutic management of critical patients [ 1 , 2 , 5 , 6 ]  . 
 in general terms , microbubble injection allows increasing the lesion - to - parenchyma contrast gradient with the detection of a larger number of abnormalities in comparison with baseline us and with a more effective definition of their shape and size . 
these include global or partial perfusion defects ( ischemic hypoperfusion , infarctual aperfusion , torsion , gangrene , etc . ) , hyperperfusion ( inflammatory hyper emia , reactive perifocal hyperemia , etc . ) , vascular fistulas , pseudoaneurysms , intraorgan contrast collections ( the classical contrast pooling from angiographic to ct semeiotics ) , and extraorgan contrast extravasation . adjunct of a contrast medium injection may offer additional information to the radiologist performing a bedside us study in an acute patient . 
the transfer of the critically ill patients to the radiology department is itself potentially dangerous , so radiologists are frequently asked to perform bedside ultrasound ( us ) studies in intensive care unit ( icu ) , surgical or medical department , sterile area , and operatory roo this is possible because modern us equipment is portable , reasonably cheap , and allows bedside examination without requiring patient manipulation . 
this allows taking relevant decisions , such as to directly bring the patient straight to the operatory room or to transfer him / her to the radiology department for an emergency ct study , also because there are no limitations in injecting consecutively the us and the ct contrast mediu not uncommonly , it is difficult to mobilize bedside patients , such as those in the icu , in the sterile area , or in the early post - operative days . 
the extemporary decision to use a contrast medium may allow recognizing potentially life - threatening conditions and so it is important for the radiologist to always bring a contrast medium package when examining at the bedside [ 7 ]  . acute inflammatory processes as mentioned previously , the lesion - to - parenchyma contrast is significantly higher in ceus than on baseline us . 
 this is particularly true in inflammatory diseases in which contrast media allow detecting typical hyperemia , which corresponds to an increased organ microcirculation . by injecting a contrast medium , it is possible to better evaluate complicated inflammations , by differentiating abscesses from phlegmons . 
it should be investigated if ceus can find a definitive place between us and doppler assessment and ct imaging . in a study using the first - generation agent levovist and power doppler imaging , it was possible to achieve 98 % accuracy and 100 % sensitivity in the diagnosis of acute appendicitis [ 11 ]  . 
all cases with purulent and gangrenous appendicitis were correctly diagnosed . in the case of complicated gastrointestinal inflammations , such as in patients with acute diverticulitis , appendicitis , or crohn disease , ceus can be useful in differentiating an abscess from a phlegmon , two complications requiring a different management [ 3 , 9 , 12 ]  . 
ceus also allows determining the true size of the collections , another parameter influencing their practical management . ceus is useful in the detection and characterization of abscesses within the liver , spleen , kidney , and peritoneal spaces [ 1416 ]  . 
aside from its location , an abscess shows enhancement of the walls and internal septa , lack of enhancement within the necrotic , liquefactive content through all vascular phases , and perifocal hyperemia during the arterial phase . 
although some may overall exist with necrotic and infected tumor masses and cysts , ceus usually allows achieving a definitive diagnosis and to guide the diagnostictherapeutic puncture of the abscess . in patients with acute renal infections , the inflammatory foci are better demarcated in comparison with the baseline appearance , owing to the increased lesion - to - parenchyma contrast gradient [ 3 , 1720 ]  . 
however , it should be considered that ceus too can be falsely negative in the very early stage of pyelonephritis , since the vascular damage needs some time to develop . 
in general terms , ceus can be helpful in the patient with acute flank pain , both with and without combined fever , to detect or rule out renal causes such as nephritis and segmental infarctions . the diagnosis of epiploic appendagitis , a disorder consisting of an ischemia and inflammation of an epiploic appendage of the large bowel , can be difficult on the sole basis of unenhanced us , particularly if the operator is not aware of this uncommon occurrence . 
ceus ( c ) : the contrast medium shows the gallbladder wall discontinuity with formation of the pericholecystic collection it is frequently difficult to examine patients with acute pancreatitis with us techniques , because of the pain and meteorisadditionally , ct allows a more comprehensive display of the pancreatic area with a more defined grading of the process . 
gvhd is a threatening occurrence after allogenic peripheral blood stem cell transplantation , requiring early detection and an adequate differential diagnosis with other acute conditions . ischemia and infarction as mentioned previously , the lesion - to - parenchyma contrast is significantly higher in ceus than on baseline us . 
these perfusion changes are not recognizable with baseline us and only partially 1 3 78 radiol med ( 2015 ) 120 : 7384 the intestinal wall [ 33 , 34 ]  . 
an 85100 % sensitivity and a 98100 % specificity have been reported in the diagnosis of intestinal infarction , aside from its etiology [ 35 ]  . abdominal hemorrhage non - traumatic bleeding can be secondary to diagnostic or therapeutic procedures ( biopsy , drainage , ablation , etc . ) , rupture of aneurysms ( abdominal aorta or other vessels ) , femoral artery puncture for transcatheter procedures , spontaneous rupture of abdominal masses , spontaneous hemorrhage within cystic lesions , or anticoagulant therapy [ 36 ]  . 
 the hemorrhage may develop , at least initially , within a solid organ , into the peritoneal cavity , in the retroperitoneal space , or within the lumen of a hollow viscus . 
additionally , us , even with the adjunct of doppler imaging , rarely allows determining if the bleeding has stopped at the moment of investigation or it is still ongoing . 
this has been reported first experimentally [ 37 , 38 ] and then in a number of cases and series of non - traumatic bleeding [ 39 , 40 ]  . 
the contrast extravasation image is continuous or subcontinuous ( pulsatile ) , appearing shortly after the afferent vessel enhancement , increasing in size over time , vanishing , and immediately reappearing after any high - mechanical index flashes . 
the contrast pooling is absent at baseline and is not recognizable in the fundamental mode part of the monitor when dual - mode , split screen ceus is performed [ 28 , 39 , 40 ]  . in patients with a ruptured aneurysm , at the level of the aorta or of other abdominal vessels , it is possible to identify the enhanced blood passing through the luminal thrombosis and the arterial wall defect and pooling adjacently [ 4143 ]  . 
consequently , ceus can be employed as a selective alternative to ct to achieve proper diagnosis and to determine the extent of the process [ 26 , 30 ]  . 
additionally , serial ceus may allow following up the infarction treated conservatively . a recent application of ceus is the evaluation of acute kidney injury thanks to its ability to determine and quantify changes in renal microcirculation that is expected to be found in the critically ill patient in various situations , such as septic shock , low cardiac output states , hepato - renal syndrome , and hypovolemia . 
the recent progress in ultrasound with contrast - enhanced ultrasound gives the opportunity to assess not only the kidney macrocirculation , but also the kidney microcirculation in the icu [ 31 , 32 ]  . intestinal infarction can be secondary to decreased or absent arterial perfusion , venous thrombosis , or intestinal obstruction complicated by strangulation . 
it is usually rather difficult to examine a patient with intestinal ischemia or infarction using us , owing to the pain , agitation , and gas distention of the bowel . 
ceus ( c , d ) delayed perfusion of the gland with areas of necrosis and hemorrhage in the case of ruptured abdominal mass , ceus will detect , if the bleeding is still persistent , the contrast spread within the tumor or into the adjacent hematoma or free effusion [ 28 , 44 ]  . 
in complicated , hemorrhagic cysts a contrast injection allows ruling out an active bleeding , but also permits excluding a solid mass by demonstrating the total lack of enhancement of the pseudosolid component within the cyst [ 45 , 46 ]  . 
ceus can differentiate solid vesical tumors from endoluminal clots , recognize and measure a vesical tumor within a large clot , and rule out any mural abnormality with patients with massive urinary bleeding from other causes such as anticoagulant therapy . contrast extravasation must be differentiated from other causes of focal hyperechogenicity , including calcifications , intraluminal gas , normal enhanced vessels , and normally perfused areas within an abnormal parenchyma [ 28 , 39 , 40 ]  . 
however , both these conditions require an emergent treatment by surgery or embolization and consequently there is a limited practical interest in differentiating a pseudoaneurysm and a free hemorrhage . ceus is effective in recognizing active bleedings , even when they are slow or of venous origin [ 28 , 43 ]  . 
on the other side , a ceus study being negative for an active hemorrhage may allow managing the patient conservatively , at least at the beginning , by carrying a careful monitoring of the blood pressure and hematocrit and performing serial us or ceus 1 3 80 radiol med ( 2015 ) 120 : 7384 fig . 
ceus ( c ) owing to the intravascular nature of us contrast media , ceus allows to perfectly differentiate the necrotic from the still viable areas within the markedly inhomogeneous gland . 
additionally , ct is more accurate in establishing anatomically the exact vessel responsible for the hemorrhage . it should be mentioned that , at least for traumatic bleeding , there is some initial experience , both experimental and clinical , on the percutaneous management of the process by using ceus as a real - time guide to the targeted injection of antihemorrhagic substances [ 48 , 49 ]  . 
these microbubbles can be administered orally or rectally and can be introduced through fistulas or tubes and catheters , such as for post - surgical drainages , vesical catheters , nephrostomy catheters , and so on . 
as a matter of fact , the contrast medium exits from the percutaneous or transluminal catheter and pools where the device ends , allowing to correctly identify the course of the catheter and to properly establish the position of the tip . 
perfect agreement between ceus ( a ) and ct ( b ) in the detection of a wedge - shaped , nonenhancing area within the enhanced liver parenchyma ( arrows ) the accuracy of this screening role and avoids the use of the more expensive and more invasive contrast - enhanced ct modality in a number of cases . 
injection of microbubbles always follows a rapid , albeit accurate unenhanced us exploration and is never employed without a preliminary us study . ceus has several advantages in the setting of emergency imaging . 
these microbubbles can be regarded as safe in the critical patient , owing to the lack of renal or hepatic effects [ 3 , 27 , 28 , 51 ]  . 
adverse events are unusual and mild and may include headache , weariness , itching , palpitations , nausea , dizziness , dry mouth , altered sense of smell or taste , dyspnea , fig . 
this safety , combined with the lack of ionizing radiations , allows a very quiet use of this imaging modality , without need for fasting or any preliminary laboratory testing . 
it should be noted that the administration of us contrast media does not interfere with the possible , subsequent contrast - enhanced ct study , which can be performed even immediately thereafter . 
finally , ceus can be performed at the bedside or in other places outside the radiology department . it is rather difficult , at least at the present time , to strictly categorize the clinical indications for emergency abdominal ceus . 
beyond the guidelines [ 4 ] , it is basically the radiologist expert on ceus imaging who decides to inject the contrast whenever he / she feels that the microbubbles may help in solving unclear or indeterminate aspects at baseline us . emergency ceus however has a number of limitations to be considered [ 13 ]  . 
first , it basically shares all the well - known limitations related to us , including obesity , meteorism , free intraperitoneal air , gas - containing collections , subcutaneous emphysema , abdominal wall obstacles ( wounds , medications , colostomies and enterostomies , drainages , etc . ) , and patient agitation . 
there are some critical areas such as the liver dome , the deepest splenic pole , and the retroperitoneum which are difficult to investigate using us or ceus , particularly in the fat patient or in the subject unable to breathe the main reason for a false negative diagnosis at ceus is due to the difficult or missed exploration of a given abdominal area . 
particularly related to active bleeding , it should be kept in mind that hemorrhages being deep , or multifocal , or just located elsewhere from the scanned area will be lost at ceus . 1 3 radiol med ( 2015 ) 120 : 7384 fig . 
the percutaneous placement of a catheter is indicated conclusions ceus is a simple and safe imaging modality that plays an increasingly important role in the assessment of nontraumatic abdominal emergencies , such as acute inflammations , infarcts , and hemorrhages . 
technical success ( ts ) , clinical success ( cs ) , late success ( ls ) and mortality rate ( m ) related to the angiographic procedure and complications were evaluated . results ce - mdct and digital subtraction angiography ( dsa ) identified active bleeding sites in 18 cases ( 18 / 20 )  . 
pinetagrande , castel volturno , italy conclusions pte could be considered a safe and effective first line approach to treat sb associated with anticoagulation therapy . keywords percutaneous transcatheter embolization spontaneous bleeding emergency radiology anticoagulant therapy introduction long - term anticoagulation therapy is a specific treatment adopted to prevent thromboembolic disorders in high - risk patients . 
some precautions are strongly linked to the administration of these drugs , especially the narrow therapeutic range and the frequent laboratory tests needed to calibrate the exact dosage for each specific patient and monitor the anticoagulant effect [ which is therapeutical when international normalized ratio ( inr ) is kept within an appropriate range of 23 ]  . 
patients with a lower inr are out of any therapeutic effect , thus being at risk for thrombosis , whilst an inr > 5 increases the risk of bleeding more than 30 % / year [ 3 ]  . 
considering the large number of patients undergoing anticoagulant therapy , it is important to know the possible risks of such treatment and in particular the correct approach to the related spontaneous bleeding ( sb )  . 
 in patients who receive oral anticoagulant therapy , some authors reported the risk of a major haemorrhagic event to range between 0.2 and 3 % / year / patient [ 4 , 5 ]  . 
therefore , an accurate digital subtraction angiography ( dsa ) , is able to identify arteriosus active bleeding and a possible percutaneous embolization treatment ( pte ) , has been widely accepted as a good strategy to overcome the limitations described above . 
our purpose was to evaluate the safety and clinical efficacy of percutaneous transcatheter embolization ( pte ) performed as first line treatment for sbs in patients who underwent anticoagulation therapy . materials and methods this retrospective study was approved by our institutional review board . 
 informed consent for emergency angiography and embolization was obtained from the patient , when possible , or from a family member . patients from january 2007 to december 2012 , 20 patients ( 10 males and 10 females , mean age 75.8 , range 6891 years ) with sb associated with anticoagulant therapy were retrospectively evaluated . 
haemodynamic instability was defined as hypotension with systolic pressure < 100 mmhg and heart rate > 100 bpm or clinical shock secondary to blood loss not responding to conservative medical treatment including blood transfusion . 
subcutaneous sodic enoxaparin ( clexane , sanofi - aventis , milano , italy ) was the anticoagulant therapy in seven patients ; 6 , 000 ui ( 0.6 ml / die ) in five patients ( 25 % ) and 8 , 000 ui ( 0.8 ml / die ) in 2 ( 10 % )  . 
 ten patients ( 50 % ) were in treatment within a range from 5 to 10 mg / die of sodic warfarin ( coumadin , bristol - myers squibb , sermoneta , latina , italy ) , periodically adjusted in accordance with their needs ; three patients ( 15 % ) received sodic enoxaparin and sodic warfar patients referred to our radiology department due to other bleeding causes table 1 patients age , number of procedures of embolization , type of drugs employed and associated disorders sex age number of procedures anticoagulant and antiplatelet associated disorders vte pulmonary embolism heart disease ( heart failure , atrial fibrillation ) cardiac valve replacement surgery arterial vascular disease ( aortic aneurysm , peripheral disease ) enoxaparin warfarin m 72 enoxaparin warfarin m 83 m 75 m 85 m 85 m 88 m 72 m 77 m 74 m 81 warfarin enoxaparin enoxaparin warfarin warfarin warfarin enoxaparin enoxaparin warfarin enoxaparin warfarin warfarin enoxaparin warfarin enoxaparin warfarin warfarin enoxaparin warfarin vte venous thromboembolism 1 3 radiol med ( 2015 ) 120 : 149157 table 2 haematoma sites and respective prevalences in our series site of haematoma on cect abdominal wall retroperitoneum iliopsoas gluteum intraperitoneum thigh n ( % ) 7 ( 36.8 ) 3 ( 15.7 ) 3 ( 15.7 ) 1 ( 5.2 ) 4 ( 21 ) 2 ( 10.5 ) table 3 bleeding arteries demonstrated through dsa arteries involved number of cases deep femoral artery branches lumbar splenic epigastric gastro - duodenal haemorrhoidal hepatic artery branches inferior mesenteric artery branches superior mesenteric artery branches note some patients had more than one bleeding vessel ( known history of trauma , post - surgical hospitalization , history of cancer ) were excluded from this series . 
all patients were admitted to our emergency department and underwent a cect scan ( somatom sensation 40 - slice , siemens , erlangen , germany ) , while vital signs were monitored . preoperative imaging evaluation 64 ; field of view large , gantry rotation all patients underwent 64 slices multidetector ct ( aquilon 64 , toshiba , tokyo , japan )  . 
optimal arterial enhancement was achieved using the bolus tracking technique , positioning a region of interest on the abdominal aorta ( at the supra - renal level ) with a threshold 100 hu higher than the basal density . 
dsa and pte were routinely performed using a 0.028lumen microcatheter ( micro catheter system progreat , terumo , tokyo , japan ) with a compatible 0.018 - guidewire passed through different 5f angiographic catheters as follows : cobra catheter ( cordis , johnson & johnson company , miami lakes , florida ) , simmons catheter ( cordis , johnson & johnson company , miami lakes , florida ) , vertebral catheter ( cordis , johnson & johnson company , miami lakes , florida ) and berenstein catheter ( cordis , johnson & johnson company , miami lakes , florida )  . 
local anaesthesia of the femoral puncture site was achieved after a subcutaneous injection of a 10 ml of 2 % mepivacaine solution ( pfizer pharmaceuticals group , new york , usa )  . 
diagnostic angiography through the main bleeding vessel ( s ) was performed to confirm the extravasation of contrast mediuthe microcatheter was advanced as close as possible to the bleeding site in all cases . 
different embolic materials were used : fibre platinum microcoils ( vortx , boston scientific , la garenne colombes , cedex , france ) , absorbable gelatin sponge pledgets ( spongeal , gelita - spon , gelita medical , amsterdam , netherlands ) , n - butyl 2 cyanoacrylate synthetic glue ( glubran 2 , gemitaly , viareggio , italy ) , 300500 m polyvinyl alcohol hydrogel microspheres ( bead block , terumo europe , leuven , belgium )  . 
heart rate , electrocardiogram , oxygen saturation , respiratory frequency , and blood pressure were continuously monitored throughout the procedure . 1 3 152 radiol med ( 2015 ) 120 : 149157 fig . 
1 axial images obtained by means of abdominal computed tomography ( ct ) of a haematoma in right postero - lateral wall of rectal ampulla in a 72 - year - old man under anticoagulant and antiplatelet therapy due to venous thromboembolism ( vte ) and abdominal aortic aneurysm treated with endoprosthesis . 
c venous phase scan before and d late phase scan obtained after 5 min from contrast injection confirmed in both cases the active bleeding ( arrowhead ) analysis technical success ( ts ) was defined by exclusion of bleeding , and restoration of peripheral flow on final angiogram . clinical success ( cs ) was defined as cessation of symptoms and stabilization of laboratory data in 24 h and within 1 week after endovascular procedure ( i.e. , decrease in pain and swelling , absence of recurrent decrease of haemoglobin by more than 1.5 g / dl , circulatory stabilization )  . 
late success ( ls ) was defined as the absence of reperfusion of bleeding during follow - up and the proportion of cases that did not required a second endovascular treatment or subsequent surgical intervention . 
contrast extravasation on dsa was identified from a single arterial branch in 11 cases ( 11 / 20 ) , 2 branches in 3 cases ( 3 / 20 ) and more than 2 branches in 4 cases ( 4 / 20 )  . 
 twenty - three embolization treatments were performed in 20 patients ( table 1 ) ; in 20 ( 20 / 23 ) cases a single session of pte was performed ; a second session of pte was necessary in 3 ( 3 / 23 ) cases . 
the first embolization treatment was achieved in 12 ( 12 / 23 ) cases using fiber platinum microcoils ( vortx , boston scientific , la garenne colombes , cedex , france ) and absorbable gelatin sponge pledgets ( spongeal , gelita - spon , gelita medical , amsterdam , netherlands ) , in 5 ( 5 / 23 ) cases with microcoils only , in 1 ( 1 / 23 ) case with microcoils and a solution of n - butyl 2 cyanoacrylate , synthetic glue ( glubran 2 , gemitaly , viareggio , italy ) , in 1 ( 1 / 23 ) case with 300500 m microparticles ( bead block , terumo europe , leuven , belgium ) , microcoils and spongeal , while spongostan alone was used just in 1 ( 1 / 23 ) case . 
d angiographic scan after the positioning of two microcoils of 3 mm and injecting spongeal showed the cessation of bleeding patients with recurrent bleeding episode , a ce - mdct was performed to check the bleeding site before the new procedure . 
pte - related mortality was 0 % ; 3 patients ( 15 % ) died more than 1 year after endovascular embolization for the following causes : myocardial infarction , aspiration pneumonia leading to respiratory failure , sepsis or other chronic disease related to patients clinical history . 
no major or minor complications were recognized as directly attributable to dsa or pte . discussion the increase in the prevalence of anticoagulant treatments is directly related to the increase in the incidence of the diseases requiring these medications . 
more interest in the anticoagulation therapeutic management is growing in the scientific community due to some large trials that demonstrated the effectiveness of anticoagulation in preventing strokes , particularly in patients with atrial fibrillation [ 8 ]  . 
in literature , many papers and case reports describe cases of sb ; sb is defined as bleeding without a known trauma in history or underlying abnormalities [ 912 ]  . 
the exact mechanism is unknown , but several hypotheses have been suggested , including forceful muscular strain , diffuse small vessel 1 3 154 radiol med ( 2015 ) 120 : 149157 fig . 
3 axial images obtained by means of abdominal computed tomography ( ct ) of right iliopsoas and transverse muscle haematoma in a 81 - year - old man under anticoagulant therapy due atrial fibrillation and cardiac valvular placement surgery . 
transarterial embolization after the positioning of three microcoils of 3 mm and injecting spongeal showed the cessation of bleeding ( b ) arteriosclerosis , heparin - induced immune microangiopathy and unrecognized minor trauma [ 13 ]  . 
some centres perform contrast - enhanced ultrasound ( ceus ) to detect and grade abdominal traumatic lesions in patients with low - energy isolated abdominal trauma or in stable patients with the suspect of haemorrhages . 
ce - mdct must always be performed in ceus - positive patients to exclude active bleeding [ 21 , 22 ]  . ce - mdct reduces the time between diagnosis and treatment , allowing the identification of the exact bleeding site , the quantification of the bleeding and its origin ( arterial or not ) ; these information are essential for the planning of treatment [ 23 , 24 ]  . 
in our experience , ce - mdct identified correctly all haematoma sites , whilst dsa did not confirmed active bleeding in two patients ; although , in these two cases dsa depicted the presence of small tortuous vessels within the haematoma , without active contrast medium extravasation . 
our ce - mdct results are in accordance with literature [ 2528 ] ; in our opinion it is mandatory to underline the pivotal role of ce - mdct and its scanning technique ; in addition to non - contrast scan , it is essential to perform a multiphase examination with at least an arterial and a late phase ( dual - phase scan ) to enhance the visualization of very small active bleedings within the hematoma site [ 2527 ]  . 
cloth sign , represented by an area of higher density surrounded by a zone of lower density , is characteristic of the first hours after the bleeding [ 29 , 30 ]  . 
 haematocrit effect is characteristic of the next phases , and it is represented of a fluidfluid level in the context of the haematoma [ 29 , 30 ]  . during an active bleeding the signal flare may be observed and it is generated by the different gravitational weight that determines the layering of the contrast medium between cellular component and component fluid [ 29 , 31 ]  . once identified the arterial bleeding site , the choice of appropriate management is strictly based on the patients clinical conditions ; a multidisciplinary team ( anaesthesiologist , surgeon , interventional radiologist and interested clinicians ) on the basis of the information available , will decide on treatment approach . 
in our experience , a revision and discussion of each case after treatment represent a crucial step to confirm the correct therapeutical approach and its effectiveness even for future similar cases . conservative management is the most common therapy for hematoma because the lesion usually is self - limited . 
 the coagulation profile of patients treated with anticoagulation medications can be corrected suspending their therapy and administering vitamin k and fresh frozen plasma or protamine sulphate in patients treated with heparan advantage of surgery may be represented by the possibility to evacuate very large haematomas in the same session , even though surgeons have appeared reluctant to perform open surgery in this setting , relating to difficulties to identify and / or bind bleeding vessels within a haematoma [ 25 ]  . 
 most recent series [ 9 , 10 , 2628 ] have suggested that dsa is effective to confirm ce - mdct data , and transcatheter embolization performed in the same session could be an effective treatment of sb . 
in the first series , embolization 1 3 156 radiol med ( 2015 ) 120 : 149157 was performed in seven patients ( 70 % ) and in the second one session of pte was performed in all patients ( 100 % )  . 
moreover the procedure is repeatable ; three of our patients underwent a second pte , with the final result to stabilize patients conditions and to avoid a surgical approach . some technical aspects may be commented , in particular the use of different embolic agents . 
the choice and / or the combination of different embolic materials ( fiber platinum microcoils , absorbable gelatin sponge pledgets , synthetic glue , microparticles ) is strictly linked , primarily , on the operator confidence . 
it is possible to consider the possibility to use only the absorbable gelatin sponge pledgets in cases in which a clearly active bleeding is not appreciable on dsa , but some small tortuous vessels remain at the haematoma site . 
finally , the glue could be a valid alternative to microcoils , being less expensive . a crucial point is the clinical management of these patients ( vital parameters , laboratory tests ) that must be obtained very quickly , immediately before and after each procedure , considering that sometimes multiple vessels could bleed within the same haematoma , so that more than a single treatment to stabilize the patients becomes necessary . 
moreover , considering the absence of major complications related to dsa and / or pte , the endovascular approach could be recommended as a safe alternative to open surgery , and it may be considered as first line approach to treat sbs . moreover , using this approach , immediate ts was obtained in all cases , with total cessation of the bleeding and limitations of the dose of ionizing radiation to which the patients were exposed , as reported in other recent experiences [ 3336 ]  . nevertheless , being percutaneous embolization and surgical treatment not mutually exclusive , surgery should be reserved to patients in which endovascular treatment failed or as second step of treatment with the aim to evacuate very large haematoma . 
in fact , large haematoma can become infected or compromise breathing or mobility . in conclusion , pte could be considered a repeatable first line approach to treat sbs following anticoagulation therapy . 
this has brought about a new concept and culture of emergency care in which time to intervention and optimising human and technological resources are crucial to avoid the loss of human lives . 
this cultural revolution in emergency care gained momentum during the past twenty years just as several fields of medicinesuch as radiology , anaesthesiology , emergency medicine and surgery and trauma medicinewere undergoing important technological advances [ 1 ]  . however , the cultural revolution in emergency care has gone well beyond the boundaries of medical science , extending to computer science , communication , architecture , urban planning , materials , etc . 
scaglione european society of emergency radiology ( eser ) , vienna , austria in this contest , radiology has gained a prominent role affirming as a distinct disciplineemergency radiologyand dedicated radiologists 24 / 7emergency radiologistsas consultants with a special interest and committment in acutely , illed patients . 
ct and sonography have replaced diagnostic peritoneal lavage , the sole purpose of which was to demonstrate hemoperitoneu non - operative management has become the standard of care for all but the most severe trauma patients , while surgery being just limited to the management of catastrophic injuries . 
high - field magnetic resonance has moved beyond its traditional application in cranio - vertebral pathology , with exciting scenarios being configured also in emergency abdominal and pelvic imaging [ 2 ]  . in this contest , recognition of the need of dedicated , full coverage 24 / 7 emergency radiologists in the emergency room has been the true difference with the old conception of radiology and emergency care . 
it is now well accepted that radiologists play a pivotal role not only in the 1 3 2 radiol med ( 2015 ) 120 : 12 diagnosis but also in the timely management approach . 
these life - threatening injuries are often very subtle and difficult to diagnose if an accurate ct examination , with an advanced protocol of study is not performed by skilled radiologist , with a special expertise in emergency radiology . 
gross monica ragucci serena monti marcello mancini shana elman hubert vesselle lorenzo mannelli received : 6 april 2014 / accepted : 16 june 2014 / published online : 13 august 2014 italian society of medical radiology 2014 abstract radiologists are familiar with the use of radiographs , computed tomography , magnetic resonance imaging and ultrasound in the acute clinical setting . 
it is important for the radiologist to be aware of these techniques to be able to guide the clinician to use those tools , which may result in optimal patient care . 
in this article , we will discuss those nuclear medicine studies which have application in the setting of an emergency radiology practice . keywords nuclear medicine emergency hida gastrointestinal bleeding tagged red blood cells brain perfusion brain death ventilation / perfusion vq scan ventriculo - peritoneal shuntogram vp shuntogram mag3 renogram introduction use of nuclear medicine imaging in the emergency care setting is probably the most under - appreciated aspect of the discipline . 
while radiologist are usually familiar with the more common imaging including radiographs , computed tomography ( ct ) , magnetic resonance imaging ( mri ) and ultrasound ( us ) procedures , many are not aware of the significant contributions nuclear medicine can make in the management of patients in acute care [ 17 ]  . 
although nuclear imaging is frequently used as a problem - solving tool after other non - nuclear imaging has failed to answer the clinical question at hand , there are common emergency care scenarios where nuclear medicine should be the first line of imaging . 
mannelli department of radiology , memorial sloan - kettering cancer center , 1275 york ave , new york , ny 10065 , usa gastrointestinal bleeding evaluation with tc99m tagged red blood cells acute gastrointestinal ( gi ) bleeding is a potentially lifethreatening emergency that may require surgical or radiological intervention . 
under such circumstances , two options should be considered : technetium ( tc ) - 99m tagged red blood cell ( rbc ) scan and angiography [ 9 , 10 ]  . 
ct angiography is a newer technique that is sometimes used to diagnose gi bleeding ; however , it is less sensitive than an rbc scan in fact can detect only bleeding happening at the exact time of ct image acquisition , while the rbc scan can be used to image bleeding happening within few hours . 
in the setting of intermittent lower gi bleeding , angiography can only be diagnostic if intravenous contrast is injected right at the time of an episode of active bleeding , which cannot be predicted . 
the radiolabeled red blood cells are then re - injected into the patient intravenously while the patient is under the gamma camera with dynamic imaging already started , so as not to miss an early bleed . 
activity seen outside of this physiological distribution , which changes over time and conforms to a bowel loop pattern ( small or large ) , represents extravasated blood from the site of active bleed . 
small bowel bleeds give rise to patterns of luminal radiotracer distribution that matches the shape of the small bowel , namely that of multiple loops of bowel with multiple twists and narrow diameter . 
1 a anterior view images from 60 min acquisition ( one image per minute , minutes 1 to 30 not shown ) from a tc - 99m rbc scan in a 60 - year - old man presenting with rectal bleeding . 
a focus of radiotracer activity is localized in the right lower quadrant ( black arrow in a and b ) : this increases over time , assumes the tubular configuration of the bowel and moves antegrade , finally assuming the course of the large bowel and displaying hepatic flexure ( black arrow point )  . 
findings are consistent with active gastrointestinal bleeding in the right lower quadrant , likely cecunote bladder activity ( asterisk in b ) and penile blood pool ( white arrow ) below the bladder base accurate interpretation of labeled red cell studies . 
if bleeding is still not revealed and because the labeled red cells remain intraluminal in the vessels , the patient could be brought back for additional investigative nuclear imaging 46 h later or sooner if another bout of rectal bleeding occurs . 
localization is most accurate ( 95100 % ) if the site of bleeding is seen in the first 120 min , as opposed to later ( 5565 % ) [ 12 ]  . urinary activity and penile blood flow are potential pitfalls in interpretation . 
with the advent of single - photon emission computed tomography ( spect ) ct hybrid imaging , challenging cases such as postoperative patients with altered anatomy or with a static focus of bleeding often benefit from spectct imaging for more accurate localization . 
once the supplying vascular territory has been identified , coiling of the vessel can be attempted in the interventional radiology ( ir ) suite . brain perfusion study for brain death diagnosis brain death signifies irreversible loss of function of all brain , including brainste brain death needs to be differentiated from severe brain damage , because life support becomes futile following brain death [ 13 ]  . 
a scintigraphic brain death study is noninvasive , simple to perform even in the intensive care unit ( icu ) setting ( portable ) and reliable , making it the modality of choice to establish imaging evidence supporting the clinical diagnosis of brain death [ 1417 ]  . 
clinical findings of brain death must have been present for 624 h [ 18 ]  . 1 3 160 radiol med ( 2015 ) 120 : 158170 1 3 radiol med ( 2015 ) 120 : 158170 fig . 
2 static images in the anterior a and right lateral b projections after injection of tc - 99m hmpao of a 24 - year - old male victim of a motor vehicle accident . 
 although some centers prefer brain - specific radiopharmaceuticals such as tc - 99m hmpao ( hexamethylpropyleneamine oxime ) or tc - 99m ecd ( ethyl cysteinate dimer ) , there is no clear evidence that they are more accurate than nonspecific agents such as tc - 99m dtpa ( diethylene - triamine pentaacetic acid )  . 
spect is usually not necessary unless an area of equivocal residual tracer uptake is seen . image interpretation the radionuclide angiogram generated from the blood flow distribution images demonstrates that the injected radioactivity can be followed from the common carotid arteries to the base of the skull . 
the tracer is redirected into the external carotid artery distribution and the face , causing increased activity in the mid - face on the radionuclide angiograthere may , however , be some flow to the scalp , which should not be misinterpreted as intracranial blood flow . 
as a result , if a small amount of perfusion remains on an initial scintigraphic study of a clinically brain dead patient , a repeat scan in 24 h will usually confirm complete absence of cerebral radiotracer uptake / activity [ 18 ]  . cholescintigraphy ( hida scan ) cholescintigraphy ( hida scan ) is commonly performed in the setting of suspected acute cholecystitis , where it provides a very high negative predictive value once the gallbladder is seen filling with radiotracer [ 3 , 19 ]  . hida scan is less commonly performed for evaluating the presence of an active bile leak . 
in the setting of suspected biliary leak , a variety of imaging modalities , including ultrasound , ct , mri and endoscopic retrograde cholangiopancreatography ( ercp ) can be used [ 3 , 1923 ]  . 
a needle aspiration yielding 1 3 162 radiol med ( 2015 ) 120 : 158170 bile - containing fluid does not prove there is an active leak , because this bile may have been present since the recent biliary injury . 
in selected cases , spectct imaging may help with interpretation of planar scintigraphic findings . technique although fasting for more than 4 and less than 24 h is required for optimal sensitivity and specificity of hida scan when evaluating for acute cholecystitis ( due to gallbladder physiology being affected by food intake ) , no patient preparation is needed in the setting of a suspected bile leak . radiopharmaceuticals used for the study are either tc99m mebrofenin or tc - 99m disofen111185 mbq of the tracer is administered intravenously and dynamic images are acquired over at least 60 min [ 3 , 1923 ]  . 
as with other nuclear medicine studies , addition of spectct can be extremely beneficial in equivocal cases . image interpretation the dynamic images demonstrate clearance of the radiotracer from the blood pool and its accumulation in the liver parenchyma . 
in challenging cases , spect or preferentially spectct could be helpful . ventilation / perfusion lung scan ( vq scan ) pulmonary embolism ( pe ) is common and can be fatal . 
risk factors for pe include prolonged immobilization , recent surgery , underlying malignancy , pregnancy , estrogen supplementation and other hypercoagulable states . the wells score is used to risk stratify patients suspected of harboring an acute pe . 
clinical signs and symptoms of deep venous thrombosis ( dvt ) , clinical likelihood of pe , heart rate , immobilization for at least 3 days , surgery in the past 4 weeks , previous dvt or pe , hemoptysis and cancer diagnosis within 6 months are taken into account and scored . 
a score of less than 2 indicates a low clinical probability , whereas a score between 2 and 6 is intermediate and a score above 6 carries a high probability of pe . serum d - dimer is also measured . 
although not specific , as it can be elevated in several other conditions , it is considered to have a high negative predictive value for acute pe . once the clinician is convinced further investigation for pe is required , the first imaging modality is usually a ct angiogram ( cta ) with pe protocol . 
if no prior anatomic imaging ( chest x - ray or chest ct ) is available , a chest radiograph is required for comparison with the vq scan , to exclude other causes of shortness of breath including , but not limited to , pneumothorax , pneumonia and pulmonary edema . technique no patient preparation is required . 
technegas , or tc - 99m labeled ultrafine carbon suspension has a more uniform distribution but is currently not fda - approved for use in the united states [ 3 , 33 ]  . for the perfusion study , an intravenous dose of 185 mbq of tc - 99m maa ( macroaggregated albumin ) is administered slowly over 35 respiratory cycles , with the patient in supine position . 
3 a anterior view images from 30 min acquisition ( one image per minute ) from a hida scan in a 39 - year - old female with a history of laparoscopic cholecystectomy and hepatitis c , 1 day following liver biopsy . 
a concurrent ct scan ( c ) demonstrated free fluid in the peritoneal cavity ( white arrow ) 1 3 164 radiol med ( 2015 ) 120 : 158170 in patients with pulmonary hypertension , those with right to left shunting , and in children . 
spectct is used if necessary to elucidate any atypical radiotracer distribution . a chest x - ray , obtained subsequent to the initiation of the patients pulmonary symptoms and at least within 4 h of the vq scan , is required at the time of interpretation . image interpretation on a normal perfusion scan , there should be homogeneous distribution of tc - 99m maa particles throughout both lungs . 
 obstruction of the blood flow to a segment of a lung by a pulmonary embolus will result in wedge - shaped hypoperfusion downstream from the embolus with corresponding lack or decrease of maa particle deposition . 
identification of such vq mismatches is the basis of vq scan interpretation . although experienced nuclear medicine physicians could reach high diagnostic accuracy by gestalt method , this is not feasible for the less experienced , and diagnostic criteria are required . 
other scan probabilities need to be weighed with respect to the wells criteria through bayesian analysis to determine the proper course of action for the patient . ventriculoperitoneal ( vp ) shuntogram hydrocephalus is the accumulation of abnormally high amounts of cerebrospinal fluid ( csf ) in the ventricles , and / or subarachnoid space . 
obstructive hydrocephalus is associated with increased intracranial pressure , which will cause dilatation of frontal and temporal horns of the lateral ventricles , elevation of the corpus callosum , stretching of the white matter tracts , and thinning of the gray matter over the cerebral convexity . since the 1960s , ventricular shunts have been used to manage this condition . 
the shunt consists of a proximal limb , a shunt reservoir and valve , and a distal limb ; the proximal or afferent limb of the shunt connects the ventricle to the shunt reservoir and valve placed underneath the scalp . 
the distal limb tubing extends distally from the reservoir / valve system to either the peritoneum , cardiac atrium , or less commonly , pleura , allowing excess csf to be evacuated to a space from which it will be reabsorbed . 
 increased intracranial pressure will result in drainage of the csf from the ventricles into the afferent , and then the efferent limb and subsequently into the peritoneum / atrium / pleura . 
 for modern valves , the pressure setting can be subsequently adjusted by an external programming device . clinical complications of ventricular shunts include obstruction , infection , disconnection , pseudocyst formation , and perforation of bowel . 
although change in the size of ventricles can occur and can be identified on head ct / mri when shunt obstruction occurs , the location of and mechanism for this obstruction may not be revealed [ 3841 ]  . technique no patient preparation is required . 
4 perfusion ( first and third rows ) and ventilation ( second and fourth rows ) images and multiple anterior and posterior projections ( rt right , lt left , lat lateral , lao left anterior oblique , rao right anterior oblique , rpo right posterior oblique , lpo left posterior oblique ) in a 48 - year - old female presenting with shortness of breath and a heart rate of 120 / mthe patient had a history of breast cancer and allergy to iodinated contrast media . 
perfusion images demonstrate at least two large wedgeshaped peripheral defects ( black arrow points ) and overall decrease in perfusion to the entire right lung ( black arrow ) when compared to the leto these perfusion abnormalities correspond normal ventilation ( white arrow points and white arrow )  . 
these scan findings carry a high probability for the presence of acute pulmonary embolus is started as 7.4 mbq of tc - 99 m pertechnetate , tc - 99 m dtpa or in - 111 dtpa is injected into the shunt reservoir . 
there is no csf flowing in the shunt system ; therefore , the injected radioactivity might travel a short distance in the distal tubing , but will not go farther . 
if obstruction is due to pseudocyst formation at the end of distal limb , accumulation of tracer may be forced into the cystic structure by manually pumping the reservoir surface , if the intracystic pressure allows , but without free diffusion into the drainage cavity . 1 3 166 radiol med ( 2015 ) 120 : 158170 fig . 
5 right lateral view images from 10 min acquisition ( one image every 20 s ) from a ventriculo - peritoneal shuntogram scan a in an 18 - year - old male with right parietal ventriculo - peritoneal ( vp ) shunt , presenting with headache . 
b magnification of a single frame with demonstration of region - of - interest ( roi ) placement for quantification of the activity in the skull region ( asterisk ) ; a second roi is placed to measure the background activity . 
there is visualization of the reservoir ( black arrow ) with retrograde movement of the tracer into the lateral ventricle ( black arrow point ) implying that the proximal limb is patent and will not need to be surgically replaced . 
overshunting while the patient is supine , the tracer will travel very rapidly down the distal limb and into the drainage cavity as soon as it is injected into the reservoir . a timeactivity curve is generated by placing a region of interest over the shunt reservoir location of the dynamic image sequence . 
6 a anterior view images from 34 min acquisition ( one image per minute ) from a tc - 99 m mag3 scan in a 49 - year - old man 4 days after renal transplant with rising creatinine and decreased urine output . 
presence of radioactivity in this bag confirms that radiolabeled urine has leaked outside of the urinary system 1 3 168 radiol med ( 2015 ) 120 : 158170 tc99m mercaptoacetyltriglycine ( mag3 ) renogram renal transplantation is the optimum treatment for endstage renal disease . 
currently , 1 - year survival rates for renal grafts are 80 % for mismatched transplants from deceased donor , 90 % for nonidentical living donors and 95 % for hla - matched grafts [ 4244 ]  . 
the half - life of grafts from living related donors ranges between 13 and 24 years , depending on the match [ 4247 ]  . the transplant is usually placed in the right lower quadrant . 
in the early postoperative period , surgery may be complicated by perirenal fluid collections containing blood or lymph or urine , the appearance of which may be nonspecific on other imaging modalities . 
when urinary leak is suspected , percutaneous aspiration of the fluid collection for diagnostic purposes is avoided , because it is invasive and would not differentiate between old and active urinary leaks . 
 acute rejection and acute tubular necrosis ( atn ) are common early post - transplant complications , which present with transplant dysfunction and rising creatinine in the first week after surgery . 
on a tc99m mag3 study , the graft will demonstrate normal blood flow , prolonged parenchymal retention of the tracer and delayed cortical transit of tracer into the collecting syste this is distinguished from acute rejection where renal flow will be compromised . kidney , the tracer is therefore seen in the renal cortex . 
transit into the urinary collecting system occurs by 5 mthe next phase is drainage of the tracer via the ureter into the urinary bladder . at the completion of the study , the tracer had drained into the bladder and cortical activity approached baseline levels . 
with a normal timeactivity curve , a peak of activity is seen , with rapid decline toward baseline levels . conclusions in conclusion , we illustrated some nuclear medicine imaging techniques which in emergency could be complementary to other radiological imaging to establish the correct diagnosis , confirm suspected pathologies or simply char acterize known conditions . 
the aim of this manuscript is instead to inform radiologists of the existence of these additional imaging tools . to describe in detail the different techniques and illustrate all the possible clinical scenarios are far beyond the scope of this manuscript and we refer to the available nuclear medicine textbooks . 
fap include several common and uncommon etiologies , which can be demonstrated both in the native aorta , mainly in acute aortic syndromes , and in the post - surgical aorta or after endovascular therapy . 
the expanding , routine use of millimetric or submillimetric collimation of current state - of - the - art mdct scanners ( 16 rows and higher ) all the time allows the identification and char acterization of these small ulcer - like lesions or irregularities in the entire aorta , as either an incidental or expected finding , and provides detailed three - dimensional pictures of these pathologic findings . 
in this pictorial review , we illustrate the possible significance of fap and the discriminating mdct features that help to distinguish among different types of aortic protrusions and their possible evolution . 
monaldi , 80131 naples , italy e - mail : tullio.valente@gmail.com knowledge about aortic diseases has grown considerably and continues to evolve with ongoing research into pathophysiology , technological advances in detection , and improved therapeutic options [ 1 ]  . 
focal aortic projections ( fap ) are protrusion images of the contrast medium ( focal 1 3 radiol med ( 2015 ) 120 : 5072 contour irregularity , breaks in the intimal contour , outward lumen bulging or localized blood - filled pouch ) projecting beyond the aortic lumen in the aortic wall and are commonly seen on multidetector computed tomography ( mdct ) scans of the chest and abdomen . 
they include several common and uncommon etiologies , which can be demonstrated both in the native aorta , mainly in acute aortic syndromes , and in the post - surgical aorta or after endovascular therapy ( thoracic endovascular aortic repair , tevar / evar )  . 
the images , acquired from software - assisted centerline reconstructions , can be used either to generate reliable and reproducible measurements or to carefully assess changes in luminal diameter and contours . 
a contrast - enhanced thoracic acquisition should be obtained with retrospective electrocardiographic ( ecg ) - gating ( table 2 ) when feasible and in cases of suspected complications involving the aortic valve or aortic sinus , valve plane , aortic root and proximal ascending aorta . 
the higher temporal resolution of ecg - gated mdct angiography dramatically improves the detectability of some typical findings such as the primary intimal tear in thrombosed aortic dissection ( ad ) or ulcerative plaque in penetrating atherosclerotic ulcer ( pau ) [ 2 , 3 ]  . 
1 the multidetector computed tomography ( mdct ) report of a focal aortic projection ( fap ) always includes its measurements ( depth , width and height ) , its location on the aorta and maximal diameter of the aortic lumen at the site of the fap . 
diagrams show fap measurements on ( a ) axial and ( b ) orthogonal images : depth ( a , blue arrow ) , height ( b , green arrow ) , and width ( c , black line ) ; a , b and c correspond to the biometry of the focal aortic projection . 
 contrast - enhanced mdct ( c ) axial and ( d ) sagittal maximum intensity prjection ( mip ) reconstructions show an example of fap measurements ( proximal descending aorta fissured thrombus in unstable aneurysm )  . 
various postprocessing techniques such as multiplanar reformation ( mpr ) , maximum intensity projection ( mip ) , and volume rendering ( vr ) , help to facilitate understanding of complex aortic pathology and to expedite communication with the surgeons and the attending physicians . 
 the common pathological denominator of aas is mainly disruption of the media layer of the aorta with bleeding ( imh ) , along the aortic media resulting in separation of the wall layers ( dissection ) , or transmurally through the wall in the case of ruptured pau or trauma [ 4 , 5 ]  . 
 among the aas , imh is characterized by a higher incidence of fap at initial diagnosis with mdct or along its course . acute imh acute imh is classically defined as a localized separation of the aortic wall layers , with partially or totally clotted blood ( hematoma ) in the aortic wall . 
it is distinguished from classic double - barrel ad by the absence at imaging of any evident demonstrable intimal tear or intima - medial flap ( as an aortic dissection without an intimal tear )  . 
the rupture of the vasa vasorum in the media is the presumable reason why intramural hematoma occurs [ 18 ]  . intramural hematoma , commonly classified according to the stanford classification used for ad , has been found in 520 % of patients who present clinical signs suggestive of aas , and may , however , be asymptomatic [ 48 ]  . 
the etiology of imh remains controversial , but four major different pathophysiological processes can lead to intramural hematoma formation [ 10 ] : ( a ) in patients with mild or no atherosclerosis , spontaneous rupture of the vasa vasorum may initiate aortic wall degeneration , which leads to hematoma formation in the aortic wall , splitting of the medial layer , with no blood flow within the media ( not pau - associated imh )  . 
cases of imh observed without an intimal tear at autopsy or during surgery support this theory ; ( b ) imh may be an ad with intimal defect and early closed and thrombosed false lumen without re - entry tear . 
this type was defined as thrombosed - type acute 1 3 radiol med ( 2015 ) 120 : 5072 aortic dissection , such as in an otherwise classic ad with an entry tear without flow in the false lumen ( early thrombosed false lumen - type acute ad or dissection variant imh or imh with intimal tear ) [ 1113 ]  . 
 some recent reports suggest that most imh result from an entry tear similar to classic ad [ 1012 ] ; ( c ) bleeding associated with an atherosclerotic ulcer that penetrates into the internal elastic lamina and allows hematoma formation within the media of the aortic wall , a penetrating atheromatous ulcer or pau ( pauassociated imh ) [ 13 ] ; ( d ) more rarely , imh can occur secondary to blunt or iatrogenic traumatic aortic injury , to incomplete wall involvement ( trauma - induced imh )  . nonetheless , at imaging a definitive distinction cannot be made between pau - associated imh and re - entry sites of imh , because of the lack of radiological - pathological correlation studies . 
 this may provoke a secondary tear , causing a classic overt ad ( in 2847 % of patients )  . the natural imh evolution , described in the literature , includes various remodeling patterns : ( 1 ) spontaneous healing ( 1040 % of cases ) ; ( 2 ) saccular aneurysm formation ( ulcer - like projections , ulps ) ; ( 3 ) fusiform aneurysm formation ; ( 4 ) progression to classic open acute dissection ( 1647 % ) ; ( 5 ) rebleeding ; ( 6 ) proximal or distal imh aortic progression ; ( 7 ) aortic rupture ( in 2045 % ) [ 115 ]  . this variable natural history and remodeling processes , even during the chronic phase , indicate that imh is a more vulnerable or dynamic condition than classic ad , suggesting the absolute need for close imaging surveillance to avoid progressive dilatation and rupture , especially within the first 3060 days [ 5 ]  . in addition , increased permeability of the aortic wall may lead to pericardial or pleural effusions or a mediastinal hemorrhage . 
 b contrast - enhanced mdct axial scan depicts a smooth , nonenhancing , crescentic region of aortic wall thickening ( black arrow ) without a spiraling intimal flap 1 3 54 radiol med ( 2015 ) 120 : 5072 fig . 
 predictors of early mortality or adverse outcome include an initial maximal aortic diameter ( cutoff value of 40 mm or greater ) in patients with distal imh , an imh thickness of greater than 11 mm and ascending aortic involvement [ 5 , 6 , 8 ]  . unlike stanford type a aortic dissection ( for which surgical management is standard ) , controversy remains in the 1 3 radiol med ( 2015 ) 120 : 5072 1 3fi 56 radiol med ( 2015 ) 120 : 5072 initial medical or surgical management of stanford type a imh . 
surgical or endovascular treatment may be employed in case of complications such as progression , luminal dilatation , penetrating ulcer , enlarging of the imh , or overt dissection . tiny imhassociated ulcers in order to avoid confusion and misunderstanding , it is possible to use the term dissection variant imh for a thrombosed ad that has no complete flow channel . 
tiny communications ( opening neck < 3 mm ) between the true and false lumen in the descending thoracic aorta and tiny or small ulcers associated with imh in the acute phase at initial imaging may commonly exist , and clearly show differentiation from other aortic diseases with hemorrhagic content within the aortic wall [ 15 ]  . 
the causes of these tiny ulcers remain uncertait has been postulated that they represent the site of an intimal tear or erosion in a thrombosed open aortic dissection [ 22 , 23 ] , the site of occlusion or detachment of the orifice of aortic branches , a prior atheromatous ulcer , or small areas of intimal rupture after intramural hematoma [ 21 ]  . 
new ulcer - like projections ( ulps ) as re - entry sites of the imh or a ( primary ? ) intimal defect / tear that exists already at the onset of imh [ 7 ] ; 2 . 
penetrating atheromatous ulcers ( pau )  . newly developed ulps , also referred to as imh reentry sites from the decompression of imh , are new intimal tears or disruptions , secondary to hematoma expansion 1 3 radiol med ( 2015 ) 120 : 5072 or re - opening ( primary or re - entry tears ) intimal defects , ulcers developing during the evolution of imh and appearing on imh imaging follow - up . 
therefore , these lesions ( not observed at the site of the imh on cross - sectional images at the time of initial diagnosis ) are a possible indicator of the formation of a flow channel between the true and thrombosed false lumen . 
on mdct , they generally are defined as [ 9 , 1623 ] : ( a ) a localized outpouching of cm , isodense with the aortic lumen with a clear and evident communication with aortic lumen with usually wide opening ( > 3 mm ) or wide - mouth communication ; they do not communicate with aortic branch arteries ; ( b ) the focal intima usually shows no atherosclerotic plaque , which is frequently noted in a pau ; ( c ) they are usually not noted at initial mdct . 
they can develop within the lesion in about one - third of patients commonly within 14 months , but the complication can be delayed ; ( d ) location : descending aorta > ascending aorta > arch ; ( e ) representing a site of new intimal disruption , portends a poor prognosis and unfavorable outcome ( a significant risk factor for evolution to an overdissection , rupture or , often saccular aneurysmal dilation )  . development of an ulp appears to be associated with a higher incidence of disease progression under medical therapy , whereas the absence of ulp may suggest a stable disease course in patients with ad with complete thrombosed false lumen [ 7 , 15 , 16 , 22 ]  . 
the most frequent adverse sequel of ulp is saccular or less often fusiform aneurysm development , also at a later phase ( 48 months after the initial episode ) [ 7 , 21 ]  . 
a newly developed ulp , during the follow - up period has a much higher risk than a ulp seen on the initial ct scan for the development of aortic aneurysm [ 22 ]  . 
in the literature , these ulps appearing in the evolution of imh , are also termed localized dissection , aortic outpouching or protrusion , pseudoaneurysm or saccular aneurysm , therefore increasing confusion related to this entity [ 15 , 24 ]  . acute penetrating atheromatous ulcer ( pau ) in pau of the aorta , an atherosclerotic plaque ulcerates and disrupts the internal elastic lamina , and is therefore a manifestation of a diseased intima and not media , as in classic ad or imh . 
although this patient was managed with aggressive medical therapy , c 7 - day follow - up mdct sagittal mip reconstruction shows disease progression : a clear fap due to intimal tear has replaced the intimal erosion visible on the initial mdct ( arrow ) ; the patient was treated by thoracic endovascular aortic repair ( tevar ) 1 3 58 radiol med ( 2015 ) 120 : 5072 fig . 
4 - day follow - up ( c ) unenhanced and ( d ) contrast - enhanced mdct axial scans at the same level show enlargement of the intimal defect and enhancing ulcer - like projection with a wide neck ( > 3 mm ) from the aortic lumen into the imh ( white arrow ) , a finding suggestive of overt intimal tear fig . 
6 fap due to new ulps in the imh follow - up in a 74 - yearold man with type b acute onset of intramural hematoma and chest / back pa a initial unenhanced mdct coronal mip reconstruction , b contrast - enhanced mdct axial scan and c sagittal mip reconstruction show a 16 - mm diameter type b intramural hematoma ( arrows )  . 
d contrastenhanced mdct axial and e sagittal scans obtained 3 weeks after acute initial event show a new ulp in the distal arch / proximal descending aorta ( arrows )  . 
clinically , the typical profile of a patient with pau is an elderly individual with multiple risk factors for atherosclerosis and often already documented manifestation of atherosclerotic disease , such as coronary aortic disease , cardiovascular disease , and peripheral arterial disease or abdominal aortic aneurysm [ 2629 ]  . the plaque may precipitate a localised intra - medial dissection associated with a variable amount of hematoma within the aortic wall , which can spread into the adventitia , forming a saccular aneurysm or pseudoaneurysm , or may also cause transmural rupture . 
in rare cases , pau may lead to aortic dissection , but dissections arising from a pau tend to be less extensive and demonstrate a thick , calcified static flap in a location atypical for entrance tears . 
 often , these lesions are asymptomatic and accompanied by atheromatous plaques and intimal calcifications , typically recognized as an irregularity along the luminal surface of the aortic wall in contrast - enhanced ct images . 
they are often associated in other sites , apart from the ulceration , which may be absent in imh . most authors have also considered these entities , irrespective of their location , to have a poorer prognosis than classic aortic dissection with a higher incidence of aortic rupture [ 2629 ]  . 
patients with a pau ( and associated imh ) that initially measured 20 mm or more in maximum diameter or 10 mm or greater in maximum depth have a high risk of disease progression and thus should be considered candidates for early surgical or endovascular repair [ 2830 ]  . 
 it is apparent that not only paus in the ascending aorta or arch but also those in the proximal descending aorta had a more malignant course , compared with that observed for paus in the middle and distal descending aorta [ 29 ]  . pau involving the ascending aorta is rare ; however , the ulcer usually ruptures and is commonly lethal . 
thus earlyurgent or emergent operative intervention is clearly recommended in these elderly patients with comorbidities , endovascular stent grafting is an attractive therapeutic modality [ 16 , 29 ]  . intramural blood pool ( ibp ) or branch artery pseudoaneurysm ( bap ) another fap that can also be seen in association with imh is an ibp or bap or focal contrast enhancement within the imh . 
secondary to damage caused by imh propagation across the origin of the aortic branch ( bronchial , intercostal , intercostobronchial , pericardial , lumbar ) artery that is partially or completely torn , ibps become a natural re - entry site of the imh , characteristically occurring at the location of a aortic branch vessel take - off [ 7 , 24 , 3037 ]  . 
they are blood - filled spaces without their own wall confined within an imh / otherwise thrombosed false lumen that communicate with both the aortic true lumen and an adjacent branch vessel [ 3739 ]  . 
imh with intramural blood pools at multiple levels has been described as the chinese ring sword sign on mdct coronal reconstruction of the descending aorta [ 32 ]  . 1 3 60 radiol med ( 2015 ) 120 : 5072 fig . 
case 1 : pau in the aortic arch in a 73 - year - old man with back pa a contrast - enhanced mdct axial scan shows a penetrating ulcer in the aortic arch ( arrow ) and localized imh ( star )  . 
case 2 : paus in a 76 - year - old man with back pab contrast - enhanced mdct axial scan shows pau ( arrow ) and extensive , circumferential calcification of the distal descending aorta ( por celain aorta ) fig . 
8 fap due to acute ( pau ) in a 74 - year - old man with sudden onset of chest pa a unenhanced and b contrast - enhanced mdct axial scans show a fap image ( small penetrating ulcer ) in the aortic arch ( arrow ) with high - attenuation imh ( star ) on mdct imaging ibp / bap is described as : ( a ) a localized island - like cm - filled pool or collection isodense with the aortic lumen , lacking its own wall , it is typically located along the non - pleural circumference of the aorta at the origin of the aortic branch arteries , inside the imh on enhanced mdct images ; ( b ) usually , but not always , there is a communication between the pool / collection and the affected aortic branch artery ; ( c ) the communication at systemic arterial pressure between the cm - filled pool and the true lumen exists , but at imaging it is no obvious or is a tiny orifice ( 1 2 mm in diameter ) visible only using thin collimations ( 0.61.2 mm ) and high temporal resolution of the latest generation mdct systems [ 39 ] ; ( d ) they may propagate along the aortic circumference and in a craniocaudal direction , from a few millimeters up to several centimeters , with a possible confluence of pseudoaneurysms arising from aortic branch arteries adjacent to each other [ 38 ] ; ( e ) ibp / bap typically appears in imh involving the descending aorta with a thickness of greater than 10 mm ; ( f ) the clinical course of bap is usually benign and selflimited and not associated with a poor outcome ; the majority of baps spontaneously regress in size over time and / or completely disappear on follow - up mdct [ 24 , 3739 ]  . 1 3 radiol med ( 2015 ) 120 : 5072 fig . 
 case 1 : follow - up mdct of acute imh progressed to overt aortic type b dissection in a 64 - year - old hypertensive patient admitted because of chest pain radiating to the back . 
contrast - enhanced mdct ( a ) axial and ( b ) sagittal mip reconstructions show that a lumbar artery originating from the true lumen is not affected by dissection and runs normally across the false lumen ( arrows )  . 
case 2 : fap due to aortic branch artery pseudoaneurysms associated with imh in a 61 - year - old hypertensive patient with acute chest pacontrast - enhanced mdct ( c ) axial and ( d ) oblique sagittal mip reconstructions show the presence of a pseudoaneurysm of the left intercostal artery at t9 level in the context of the thoracoabdominal imh ( arrows ) in the absence of clinical symptoms or sustained growth , ibp / bap needs no specific treatment . 
according to this classification , later adopted by the european society of cardiology [ 41 ] and reiterated in the guideline of the american college of cardiology foundation and the american heart association in 2010 [ 1 ] , there are classic type dissections ( class 1 ) with association of intimal tear and the presence of dual lumen ; intramural hematoma ( class 2 ) ; intimal tear without hematoma ( limited dissection ) and eccentric aortic bulge ( class 3 ) ; atherosclerotic penetrating ulcers ( class 4 ) ; iatrogenic / traumatic dissection ( class 5 )  . limited intimal tear ( class iii ) , also known as incomin 1999 , svensson et al . 
 [ 40 ] suggested a five - class classification of ad , depending on the pathogenetic mechanisms plete tear , is a rare variant of ad qualified as subtle , discrete dissection in which the limited stellate or linear 1 3 62 radiol med ( 2015 ) 120 : 5072 intimal tear is associated with exposure of the aortic media or adventitial layer and focal eccentric bulge at the tear site . 
 it has no extensive progression , significant separation of medial layers , and an intima - medial flap and does not result in a second flow channel , as seen in classic ad , or an evident intramural hematoma . patients often present with the classic symptoms of dissection and may also have associated aneurysms , aortic regurgitation , or pericardial effusion . 
although the incidence of limited intimal tears is not well known and is likely underestimated because of general unfamiliarity with this dissection variant , imaging techniques such as ct , magnetic resonance imaging ( mri ) , or transesophageal echocardiography ( tee ) may fail to detect this type of dissection . 
in fact , each of these modalities depends on the presence and identification of an intimal flap or true and false lumen for the diagnosis , although chirillo et al . 
an aneurysm is unstable if shows rapid enlargement and / or signs of impending rupture . the intraluminal thrombus ( ilt ) adheres to the aneurysm wall and it is often circumferential and most commonly thicker on the ventral side of the aneurys the growth rate of aa is related to thrombus growth and the growth of the ilt is associated with an increased risk of rupture [ 43 ]  . 
 from the imaging point of view , there are three ilt characteristics that may help to identify the risk of aneurysm rupture : ilt size and growth rate , presence of fissures and structural inhomogeneities in the ilt , and the presence of calcifications in the ilt [ 43 , 44 ]  . 
in symptomatic patients , ilts may break or fissure , and their internal structure may be inhomogeneous ; thus , the pathophysiology is different from that of an intramural hematoma in which the hemorrhage occurs from within the aortic wall . 
pseudoaneurysms ( psa ) have fewer than three aortic layers and are contained by the adventitia or periadventitial tissues , and are typically saccular with a narrow neck [ 45 ]  . 
infected aneurysm ( or mycotic aneurysm ) is defined as an infectious break in the wall of an artery with formation of a blind , saccular outpouching that is contiguous with the arterial lumen [ 46 ]  . 1 3 radiol med ( 2015 ) 120 : 5072 staphylococcus and streptococcus species are the most common causes of infected aneurysms . 
the infectious agents can either travel through the bloodstream and harbor in the vasa vasorum of the arterial wall or implant on damaged intima , ulcerated arteriosclerotic plaques , or mural thrombus . 
alternatively , the infectious agents can also reach the artery either by contiguous spread of adjacent infectious process or by traumatic and / or iatrogenic inoculation [ 45 ]  . 
11 fap due to limited intimal tear with intramural hemorrhagic content in a 58 - year - old male with sudden onset of chest and back paa transesophageal echocardiogram of the ascending aorta shows a linear echogenic projection partially enclosing an echolucent space ( white arrow ) and b an eccentric one - sided bulge of the aortic wall ( white arrow )  . 
contrast - enhanced mdct ( c , d ) axial scans demonstrate a linear filling defect with subtle undermined edges ( arrow ) and eccentric medial one - sided bulge of ascending aorta ( solid arrow ) without clear intimal - medial flap or false lumen visualized ; this was initially diagnosed as a focal sinusal projection . 
f 3d - vr coronal reconstruction confirms the aortic bulging and shows a teardrop - shaped intimal tear with a localized intimal flap ( white arrow ) at its inferior border . 
although the abdominal aorta is the most frequently involved part of the aorta , the combined involvement of the descending thoracic , thoracoabdominal , and suprarenal aorta , accounts for more cases than the infrarenal aorta . 
earlier detection of infected aneurysms is critical for timely treatment to optimize patient outcome , because their no treatment or delayed treatment often leads to fulminant sepsis , spontaneous arterial rupture , and death [ 46 ]  . 
in general , small , asymptomatic , and unruptured infected aneurysms can be managed with a trial of intravenous antibiotics for 46 weeks along with surveillance imaging . acute traumatic aortic injury fap approximately 90 % of blunt traumatic aortic injuries occur at the anteromedial aspect of the aortic isthmus , 8 % in the ascending aorta , 2 % in the descending aorta at the level of the diaphragm , 5 % in the abdominal aorta , and 6 % multiple sites [ 4750 ]  . 
12 fap due to fissured thrombus in unstable aneurys a contrast - enhanced mdct axial scan obtained in a symptomatic 78 - year - old woman shows an ulcer - like extravasation of luminal contrast media through the mural thrombus in the descending thoracic aorta aneurysm ( arrow ) ; note the high - attenuation fluid in both pleural spaces , a finding that represents acute hemothorax . 
c contrast - enhanced mdct oblique coronal vr reconstruction enhances the ulcer - like morphology of the fissuring thrombus ( arrow ) 1 3 radiol med ( 2015 ) 120 : 5072 fig . 
unenhanced mdct ( a ) axial scan obtained in a symptomatic 70 - year - old man shows a hyperdense crescent sign due to an acute hemorrhage within the thrombus . 
contrast - enhanced mdct ( c ) axial scan shows focal discontinuity of the intimal calcifications ( arrow ) or missing calcium sign ; this finding should also be reported in that it is a sign of impending rupture , especially if the intimal calcification points away from the aneurysm ( tangential calcium sign ) imh ( ib ) , intimal injury with periaortic hematoma ( ii ) , partial aortic transection with pseudoaneurysm ( iiia ) , multiple aortic injuries ( iiib ) , free rupture ( iv ) [ 5154 ]  . 
depending on location , careful attention should be paid to intercostal arteries , internal mammary arteries , lumbar arteries and arch branch vessels as they may be the source of bleeding . 
grade i and ii injuries in hemodynamically stable patients can be treated non - operatively with anti - impulse therapy ( - blockers ) and followed with repeat mdct angiography or alternative effective technique ( interval imaging should be done within 4872 h ) , until they have demonstrated resolution or stabilization of the injury . 
in minimal aortic injury ( approximately a quarter of blunt thoracic aortic injuries ) conservative management with close imaging follow - up has been recommended and is associated with an excellent outcome [ 57 ]  . mimics and pitfalls in interpretation 1 . 
it can be observed by scrolling images up and down and tracing out the vein back to its insertion into the left subclavian vein . 1 3 66 radiol med ( 2015 ) 120 : 5072 fig . 
14 fap due to infected aneurys case 1 : images obtained in a 66 - year - old woman with infected proximal descending aortic aneurysm , steroid - dependent rheumatoid arthritis and - hemolytic streptococcus sepsis . 
contrast - enhanced mdct a axial and b coronal mip reconstructions show a focal , contrast - enhancing saccular dilatation with acute margins and lobulated contours ( arrows ) , a saccular aneurysm with prominent periaortic inflammation and fluid . 
case 2 : infected aneurysm of the aortic isthmus in a 58 - year - old man with methicillin - resistant staphylococcus aureus sepsis due to an inflammatory complication of urolithiasis . 
d contrast - enhanced mdct axial scan and e sagittal mip reconstruction show small pocket - like saccular aneurysms of the arch with fat stranding and thick , heterogeneous , hypoechoic rind due to inflammatory tissue . 
a contrast - enhanced mdct coronal multiplanar reconstruction ( mpr ) shows a small tear , localized wall bulging and sudden change in aortic caliber ( pseudocoarctation ) at the aortic isthmus with minimal periaortic hematoma ( arrow ) , classified as a grade ii injury . 
b contrastenhanced mdct axial scan shows intimal tear or flap of descending thoracic aorta with contour abnormality and filling defect projecting into the lumen ( arrow ) , classified as a grade i ( minimal aortic ) injury ; collapsed lung mimics hematoma . 
the focal bulging of aortic contour arising distal to the aortic annulus by valsalva sinuses , the right atrial appendage , superior pericardial recess , and left inferior pulmonary vein , may play a role in interpretive errors . 
 familiarity with these structures , the multiplanar imaging , and a close attention to the true relationship of these structures relative to the aortic wall , are usually sufficient to eliminate these concerns . postsurgical aorta mimics and pitfalls in post - surgical aorta open repair of the thoracic aorta is performed using an impermeable dacron tube of variable length , which may be grafted using either the interposition or the inclusion technique [ 59 ]  . 
the dacron graft is not detectable on chest radiographs but is visualized on non - enhanced mdct images as a high - density , thin - walled , curvilinear tubular structure with a smooth and uniform appearance . 
polytetrafluoroethylene ( ptfe ) felt material ( felt pledgets ) also can reinforce sites of arterial cannula placement from cardiopulmonary bypass ( cpb ) , puncture sites used to evacuate air bubbles and coronary artery reimplantation sites to reduce the tearing of vessels [ 59 , 60 ]  . 
graft margins can be seen on sagittal oblique mpr / mip images as an abrupt change in caliber , contour or angulations at the junction of the graft and the native aorta , all of which are normal except in the case of significant luminal nar rowing . 
another potential pitfall in the interpretation of postoperative ct scans , after aortic root reconstruction with a composite graft , lies in the variable appearance of the coronary artery anastomosis . 
with composite graft replacement , the coronary ostia are dissected with a rim of surrounding aorta ( button technique ) and reanastomosed individually to the composite grathe buttons along the proximal graft anastomosis can occasionally be rather prominent and may produce a small bulge at the anastomotic site , simulating a psa [ 61 , 62 ]  . 1 3 68 radiol med ( 2015 ) 120 : 5072 fig . 
a in a 26 - yearold man involved in a motor vehicle collision , contrast - enhanced mdct axial scan shows evident linear flow and a mild contour irregularity in medial aspect of proximal descending thoracic aorta without mediastinal hemorrhage ( arrow ) , consistent with a partially patent ductus . 
c 3d oblique sagittal vr image shows expected findings of composite graft with prosthetic valve ( blue arrow ) , coronary button anastomoses ( white arrow ) , and distal anastomosis of aortic graft to native aorta ( yellow arrow ) with teflon felt rings used to reinforce the anastomotic site 5 . 
during open surgery of abdominal aortic aneurysms , when the native proximal aorta is friable or severely diseased , a ptfe belt may be used on the outside of the aortic neck to reinforce a potentially friable proximal aortic anastomosis . 
a chronic perigraft / paravalvular collection can serve as a site of secondary infection , particularly in patients who are bacteremic , and a correlation should be made with clinical indicators of infection . 
mdct findings suggestive of an infected perigraft / paravalvular collection and psa include [ 5963 ] : ( a ) contrast enhancement of the collection , bubble or pockets of air within the collection , increasing size of collection on serial scans and fistulous connections to other adjacent structures or extension into other compartments ; ( b ) valve vegetations in the form of small , round , hypoattenuating masses located on the sewing ring or leaflet component , usually on the ventricular surface of the prosthesis ; ( c ) ulcer - like leaks , valve ring abscesses , and extension of the infection into adjacent tissues ; ( d ) valve dehiscence appears as a gap between the aortic annulus and the opposing margin of the artificial valve that allows visualization of an ulcer - like or continuous column of cm from the left ventricular cavity into the aortic root . dehiscence of the suture line can lead to a broad range of complications ( anastomotic psa , perigraft perfusion , confined perforation , suture line failure with hemorrhage )  . 
partial dehiscence of a suture line can occur at any anastomotic site , but most commonly either proximal or distal to the graft , at cannulation sites , or ascending aorta needle puncture site ( needle inserted for pressure measurement , to purge the aorta of air , or to inject cardioplegic solution )  . 
17 fap due to post - surgical pseudoaneurysm in a 65 - yearold man with ascending composite aortic interposition graft and reimplantation of coronary arteries ( button bentall procedure ) for aortic aneurys 8 - day postoperative contrast - enhanced mdct ( a ) axial and ( b ) oblique sagittal mip reformatted images obtained because of mild chest pain before hospital discharge show active contrast extravasation arising from the right coronary anastomosis site ( yellow arrow ) and extending in a large contained pseudoaneurysm ( psa ) ( blue arrow ) encompassing the ascending aortic graft projecting morphology , of variable origin , flow rate , size , and location and is classified into types i to v according to the source of blood flow : type i , leak at the attachment site ; type ii , leak from a branch artery ; type iii , graft defect ; type iv , graft porosity and type v , endotension [ 61 ]  . 
because endoleaks have variable flow rates , they can be detected at variable times after cm injection and delayed phase imaging , in particular , it is critical for what els can demonstrate as they are not visualized during the arterial phase . 
the former are managed by securing the attachment sites with angioplasty balloons , stents , or stent - graft extensions , and the latter by covering the defect with a stent graft extension . 1 3 70 radiol med ( 2015 ) 120 : 5072 fig . 
18 fap due to type iii endoleak in a 72 - year - old man after tevar for emergent , ruptured , descending thoracic aortic aneurys contrast - enhanced mdct ( a ) axial and ( b ) oblique sagittal mip reformatted images of the thoracic aorta show contrast material outside the double - stented aorta in the excluded aortic lumen ( white arrows ) directly communicating with the native aorta , consistent with a type iii endoleak ; note the large right mediastinal hematoma ( blue arrow ) and bilateral pleural effusion ( star ) mimics type ii els are defined as retrograde flow through collateral vessels into the perigraft space , preventing thrombosis of the sac and creating a risk of continued aneurysm expansion and possible rupture . 
the most common culprit vessels are lumbar arteries , inferior mesenteric artery or internal iliac artery , whereas , in thoracic endografts , type ii endoleaks depend on the bronchial and intercostal arteries . 
embolization of the branch vessel is only indicated if the aneurysm sac continues to expand in size . conclusions fap may be present in a complex and dynamic group of conditions affecting the aorta ; although our understanding of these entities continues to evolve , mdct plays the dominant role in their evaluation because various findings help to distinguish among different types of aortic protrusions . 
the role of the radiologist begins with proper protocol design and the use of advanced display techniques for image processing to optimize fap ; prompt and accurate detection and characterization ; radiologists should be aware of the features , potential complications , and management options of these patients , because some lesions require treatment whereas others may be followed . 
detailed evaluation and knowledge of some related and distinguishing high - risk mdct features in fap , may improve our understanding of aortic diseases , can be essential to provide the surgeons with the necessary information for appropriate patient triage and management decisions . this type of leak has been reported in up to 25 % of cases . 
since multiple injuries are common among children , the emergency physician has to assess all the organs of a high - energy injured child , independent of mechanism of the trauma . 
even if the principles of polytrauma management are identical both in children and in adults , the optimal pediatric patient care requires a specific understanding of some important anatomical , physiological , and psychological differences that play a significant role in the assessment and management of a pediatric patient . 
 in the hemodynamically stable patients whole - body ct scanning is the most immediate radiological procedure that allows the examination of all the body parts of a polytraumatized child , reducing the number of minor injuries that might otherwise be neglected . keywords pediatric polytrauma trauma management trauma diagnostic imaging pediatric emergency radiology v . 
pinto department of diagnostic radiological imaging , marcianise hospital , marcianise , ce , italy introduction trauma is the cause of over 45 % of deaths in children aged 1 to 14 years ; more than 5 , 000 traumatic deaths occur in this age group every year , 80 % of which are unintentional and 47 % are directly related to road accidents [ 1 , 2 ]  . 
the mortality estimates of children admitted to hospitals following an accident are uniformly low , however , most trauma deaths occur at the scene and then prior to the arrival at a health facility . 
this is the reason why the overall mortality rates have been underestimated . statistics show that the mortality rate , as a result of road accidents , has risen dramatically among children in the age group of 13 years and above , since a young car occupant is much more vulnerable . 
drowning is the cause of about 1015 % of injuries , burns account for about 510 % , and falls account for 2 % of deaths [ 35 ]  . 
furthermore , the percentage of children suffering abuses should not be underestimated and in fact , even though a significant reduction in these events has occurred , about 13 % of deaths in the age group of 114 is related to homicide [ 2 , 6 ] ( table 1 )  . in children , the area more frequently affected by trauma is the skull [ 7 , 8 ] ; then the thoracicabdominal associated injuries [ 13 , 7 , 8 ]  . 
since multiple injuries are common among children , the emergency physician has to assess all the organs of an injured child , independent of the mechanism of the trauma . even if the principles of polytrauma management are identical both in children and in adults , the optimal pediatric patient care requires a specific understanding of some important anatomical , physiological , and psychological differences that play a significant role in the assessment and management of a pediatric patient [ 9 ]  . 
a comprehensive 1 3 table 1 leading causes of traumatic deaths in children 114 years of age in the united states 2004 [ 2 , 6 ] motor vehicle accidents etiology homicide drawing burn suicide suffocation other outline of the anatomical differences and of their implications in a polytraumatized patient are listed in table 2 . in general , the body of a child has higher elasticity , so that even severe internal injuries may occur without any recognizable external signs . 
children are particularly at risk of severe injuries since , proportional to weightheight ratio , they have bigger and more adjacent solid organs , less subcutaneous fat , and less muscular protection than in the adults . besides , because of the large volume of the head compared to the body and the larger body surface in relation to weight , each force will be more widely distributed making the most significant probability that multiple lesions may occur . 
the imbalance between the large body surface and the weight leads the child to a greater amount of heat loss in relation to a higher evaporation . all these factors prove that the energy level and the caloric requirement of a polytraumatized child is much larger than that of an adult . 
physiologically each child responds to the trauma in a different way , depending on the age and severity of the injury , but each procedure relative to free water and electrolyte maintenance is to be amplified . unlike adults , children have a great ability to maintain their blood pressure despite a significant and acute blood loss ( from 25 to 30 % )  . 
small changes in heart rate , arterial pressure , and perfusion of the extremities may indicate an imminent presentation of cardio - respiratory failure and , therefore should not be neglected . 
finally , children do not have the ability to better manage an environment that is not 38 , 2 13 , 3 13 , 2 16 , 3 radiol med ( 2015 ) 120 : 3349 their usual and , for this reason , they are excessively irritable , making their health status assessment even more difficult [ 10 ]  . recent data have shown that 25 % of children involved in road accidents will show signs of post - traumatic stress disorder following the discharge [ 11 ]  . 
the pediatric patient needs a calm , sometimes unconventional , approach in such a way to reduce their state of anxiety . primary survey the primary objective of management of a young trauma patient is to identify and address immediate life - threatening injuries . the initial assessment and the arrangement of possible resuscitation procedures can and should be rapid ( 510 min ) ; it is convenient to follow the logical sequence abcde ( airwaysbreathingcirculationdisability exposure ) , remembering that an airway obstruction is potentially deadly faster than a respiratory problem which , in turn , can turn fatal faster than a circulatory problem , etc . 
in children , the dimensional proportion between head and body , with the typical prominent occiput , requires almost always to raise slightly the trunk in order to allow the cervical spine to stay in - line . table 2 anatomic differences in adults and children , and implications for pediatric trauma management the childs body size allows for a greater distribution of traumatic injuries , therefore multiple traumas are common the childs greater relative body surface area also causes greater heat loss the childs internal organs are more susceptible to injury based on more anterior placement of liver and spleen and less protective musculature and subcutaneous tissue mass the childs kidney is less well protected and more mobile , making it very susceptible to deceleration injury the pancreas is less protected by the abdominal muscles and fat , and is therefore more susceptible to injury from impact against the spine the childs head - to - body ratio is greater , the brain less myelinated , and cranial bones thinner , resulting in more serious head injury 1 3 radiol med ( 2015 ) 120 : 3349 fig . 
1 pediatric trauma management the airway patency may be impaired by the hypotonia of the tonguehypopharyngeal muscles , as well as by secretions , blood , vomit , foreign bodies , direct injuries of the facial bones / skull , or of the airways [ 12 ]  . the final maneuver of stabilization of the airways is represented by the tracheal intubation to be performed only by skilled care providers . basic indications for tracheal intubation are : airway protection from aspiration of blood , vomitus airway obstruction or risk of obstruction due to trauma , burns of the face , and / or of the neck insufficient oxygenation despite a high fi02 shock severe impairment of the levels of consciousness ( gcs < 9 ) b ( breathing ) ventilation and oxygenation a consequential step immediately following the verification and obtainment of a patent airway is monitoring the effectiveness of respirationspontaneous ventilation . an efficient respiratory activity depends on the anatomical integrity of the rib cage and the pulmonary parenchyma , in addition , of course , to an efficient neural drive . as in adult patients , it is absolutely necessary to seek and rule out clinically life - threatening conditions such as tension pneumothorax and open pneumothorax , using the classic cornerstones of physical examination : inspection , palpation , auscultation , respiratory rate observation , sp02 . tension pneumothorax still represents a dangerous and unrecognized killer , responsible for many preventable trauma deaths . in children and even more in infants any impairment in diaphragmatic excursion may significantly decrease ventilation . 
does not open eyes table 4 avpu system alert responds to verbal stimuli responds to painful stimuli unresponsive it is beyond the present study for a detailed survey of the infusion strategies and the relative clinical target in different traumatic situations ( head trauma and / or closed and / or penetrating trauma )  . 
however , it is important to remember that a careless volemic expansion , above all if performed without heating the fluids , can cause a harmful coagulation impairment , from hemodilution and hypothermia . as in adults , a shock condition in traumatized children is attributed to hemorrhage , until proven otherwise ; in relation to the context , of course , different and concurrent causes should be assessed , such as myocardial dysfunction after contusion due to thoracic trauma , or medullary impairment with neurogenic shock ( hypotension without increase of heart rate or vasoconstriction ) due to head and neck injuries [ 10 ]  . d ( disability ) neurological assessment primary survey is to be completed assessing levels of consciousness , papillary size , and reaction and possible lateralizing signs . the level of consciousness can be examined using the glasgow coma scale ( gcs ) ( table 3 ) or the simplest score avpu ( table 4 )  . a modified version of the gcs scale , the pediatric coma scale ( pcs ) ( table 5 ) , has been studied for preschool children . among the causes of neurological alterations in a pediatric trauma patient , it is necessary to consider a possible reduced intake of o2 ( respiratory or cardio circulatory causes ) and hypoglycemia ( easily exhaustible glycogen stores )  . it is always required to identify the presence of any source of external bleeding with a systemic approach , by applying direct pressure ; in children , in particular , the bleeding from the skull can be very massive and hemodynamically significant ; in presence of uncontrolled bleeding from limbs , it is required to immediately use pneumatic tourniquets of proper fit . all the polytraumatized pediatric patients should be connected to a multi - parameter monitor in order to have a continuous reassessment of the respiratory and circulatory parameters . it is essential to obtain , as soon as possible , 1 or , preferably , 2 vascular access for the replacement of fluids and the delivery of medications . 
when a vascular access is unavailable within few minutes , it is suggested to install a intra bone passage in the tibial , femoral , or humeral site [ 14 ]  . in case of hypovolemic shock in a pediatric patient , the infusion plan involves the administration of a rapid 20 ml / kg bolus of crystalloids that can be repeated up to three times to a total of 60 ml / kg . 
as in adults , also in children the administration of colloids is highly controversial . table 5 pediatric coma scale ( pcs ) eyes ( 14 points ) verbal ( 15 punti ) motor ( 16 punti ) 4 . 
for this reason , in emergency management , the sensitivity of a radiological investigation is more important than its specificity , with the major aim of excluding any condition requiring a prompt treatment . in the diagnostic evaluation of a polytraumatized patient , the path to follow is completely different depending on whether the patient is in clinical conditions of hemodynamic stability or instability . whole - body ct scan can be performed for a thorough and detailed examination of all the body parts , both visceral and somatic ; on the contrary , in hemodynamically unstable patients , ct scan cannot be performed due to lack of time and , therefore , life - saving x - ray and us investigations are to be already performed in emergency , during the primary survey stage [ 11 ]  . upon arrival of polytraumatized patients at the emergency setting , the radiologist plays a key role in the primary survey , and , in this scenario , x - ray and us examinations play a definite role , capable of providing a first effective diagnostic confirmation of some potentially life - threatening clinical situations . imaging tests to be performed during this stage are : chest x - ray ( cxr ) on ap view , cervical spine x - ray on ll view , pelvis x - ray on ap view , and e - fast scan ( extended focused assessment with sonography for trauma ) with the patient lying in a supine position while the resuscitators try to monitor and stabilize the pediatric patients vital signs . 
the whole - body ct , as already said , on the contrary , is a diagnostic aid of the secondary survey , and it is performed only after the achievement of the hemodynamic stability so as to meet a detailed and complete evaluation of all the body parts [ 1619 ]  . in the study protocol for the high - energy trauma in children ceus is not included . 
ceus is used both in adults and children in low - energy trauma . chest x - ray ( cxr ) as a matter of fact , in hemodynamically stable patients or in patients stabilized after primary resuscitation , a the cxr study on ap view , at bedside , of the polytraumatized patient in the emergency room , can be performed 1 3 38 fig . 
pnx preferably collects in the lower - anterior portion of the chest , above all , in the anteromedial and subpulmonary site , where the flap , interposed between the base of the lung and the diaphragm , can locate both at the front and posteriorly . 
a post - traumatic pneumatocele occurs within few days of the occurence of the trauma , but , in some cases , it may occur after some months ; the size is usually between 2 and 5 cm . pulmonary atelectasis following a closed trauma may be obstructive , ( mucus plug , foreign body , endobronchial blood , or airway rupture ) , passive , compressive , or adhesive . 
right large lacerated and contused area , with unhomogeneous parenchymal thickening ( a ) corresponding to contusions and hematoceles at ct scan ( bc ) of atelectasis in a trauma patient are variably associated . 
the rise of the left hemidiaphragm is also visible the ap projection , recommended by the program atls ( advanced trauma life support ) performed during the primary survey , provides much information about the mechanism of injury . anteriorly , the ap projection , allows the identification of the presence and extent of the diastasis of symphysis pubis and / or the fracture of the obturator ring . 
posteriorly , it recognizes the presence and extent of dislocation of the injured side of the pelvis , dislocations of the sacroiliac joint , or fractures of l5 transverse apophysis . 
when the patient lies in the supine position , the area of interest corresponds to the anterior and inferior part of the chest on both sides of the thorax , approximately the thirdfourth intercostal space between the parasternal and the mid - clavicle lines . 
10 fast ( a ) and e - fast ( b ) has no sensibility in detecting bowel and mesenteric injuries , but they are diagnosable with ct scan . therefore , the effectiveness of ultrasound lies in its high diagnostic accuracy in detecting the hemoperitoneum and fig . 
fast shows hemoperitoneum ( a ) , with huge blood collection in the pelvic cavity confimed by ct scan ( c ) , that allows also to detect the complete splenic fracture 1 3 radiol med ( 2015 ) 120 : 3349 the first important dynamic sign to be checked is the lung sliding . 
these artifacts are the result of multiple reflections of the ultrasound beam between two elements with opposite acoustic impedance , such as the alveolar air and the fluid of interlobular septa . 
 in pnx , their significance is indirect , because visualization of even one isolated b line represents a safe demonstration of the adherence of the visceral pleura to the parietal pleura . 
obviously , the absence of b lines is not a powerful indicator of pnx . when a sonographic pattern suggestive of pnx ( i.e. , absent lung sliding and absent b lines ) is detected in the fig . 
13 chest traumaefast ( a ) only in real time observation shows the absence of pleural sliding , consisting of the sliding of the visceral pleura over the parietal pleura . 
adrenal gland hematoma ( b , e ) associated with renal fracture ( c , e ) and splenic lesion ( b , d ) anteriorinferior chest area of the supine patients , diagnostic confirmation can be achieved by gradually moving the probe toward the lateralinferior chest areas . 
this maneuver is targeted at the detection of a point on the chest wall where a respiratory pattern ( i.e. , lung sliding and / or b lines ) is visualized again and intermittently replaces the motionless pleura . 
the injection of a saline solution is always recommended to ensure a compact progression of the contrast bolus ( table 7 )  . unenhanced ct scans scans without contrast medium are appropriate for the examination of head and facial mass . 
neck , thorax , abdomen and pelvis are not routinely explored during this stage to avoid excessive radiation exposure . contrastenhanced ct the contrast - enhanced ct scan includes the examination of neck , thorax , abdomen , and pelvis . 
in whole - body ct scanning the arterial phase starts from the circle of willis and extends to the pubic symphysis using the bolus tracking 1 3 48 radiol med ( 2015 ) 120 : 3349 technique with the region of interest ( roi ) located in correspondence of the ascending aorta . 
the late excretory phase is only required in patients with suspected injuries in the excretory / urinary system . as in adults , the arterial and venous phase is mandatory for the examination of the pediatric patient with high - energy trauma to exclude vascular and parenchymal lesions . the coronal and sagittal multiplanar reconstructions ( mprs ) are routinely performed for the evaluation of the spinal column in the cervical , thoracic , and lumbar regions as well as the evaluation of the thoracic and abdominal structures . 
the mips ( maximum - intensity projections ) and vr ( volume rendering ) reconstructions are required in case of vascular injuries or fractures of the spine and pelvis . the use of the whole - body ct scan is rapidly increasing in the management of pediatric polytraumatized patients . 
 as mentioned above , we should consider the risk associated with the exposure to ionizing radiation directly related to this technique , but the same , we should carefully consider the cases of cancer and , therefore , of early death directly related with it [ 54 ]  . 
although it is prudent to obtain a high image quality to achieve a satisfying diagnosis , it is suggested to use a low - dose protocol to reduce the number of oncological diseases in future life . 
some studies have , in fact , documented that it is possible to reduce the radiation dose compared to that commonly used , maintaining a ct image quality to be more than satisfying [ 55 ]  . a weight and cross - sectional dimension - based adaptation of scanning parameters ( tube current and tube potential ) has also been recommended to reduce the radiation dose associated with ct scanning [ 56 ]  . during ct scanning , a user can manually set the scanning parameters to reduce or adjust the radiation dose according to patient size , clinical indications , and body region being scanned . 
these scanning parameters may include tube voltage , tube current , gantry rotation time , pitch , and beam collimation or detector configuration . the automated tube current modulation is a wellestablished method to maintain uniform study quality by changing the mas to keep a uniform predetermined noise level throughout the study [ 57 ]  . 
leung luigia romano nicola gagliardi gianluca ponticiello mariano scaglione received : 21 april 2014 / accepted : 13 june 2014 / published online : 13 august 2014 italian society of medical radiology 2014 abstract diaphragmatic injury is an uncommon traumatic condition . 
in this review article , we illustrate the mdct appearance of blunt and penetrating diaphragmatic injuries and emphasize the role of the emergency radiologist in detecting these entities . keywords diaphragmatic injury trauma multidetector computed tomography introduction diaphragmatic injury ( di ) was first reported by sennertus in 1591 . 
scaglione department of radiology , pineta grande medical center , castel volturno , italy vast majority of the cases of di are due to blunt trauma [ 2 , 3 ]  . 
in contrast , penetrating injuries , most commonly due to gunshot wounds ( gsw ) , account for the majority of the traumatic diaphragmatic injuries in the united states [ 4 ]  . 
 however , when a conservative approach is chosen , it is estimated that blunt diaphragmatic injury remains undiagnosed at initial presentation in 766 % of cases [ 6 ]  . 
for penetrating di , one study estimated that 7 % of cases can be occult [ 7 ]  . there are multiple explanations for the suboptimal detection rate of diaphragmatic injury . 
in addition , diaphragmatic injury usually occurs in polytrauma patients and its presentation can be overshadowed by associated injuries , which have been reported in 52100 % of patients in different series [ 8 , 9 ]  . from an imaging standpoint , the diagnosis of diaphragmatic injury can be challenging . 
furthermore , the defects in penetrating diaphragmatic injury are notoriously difficult to detect due to their small size ( 12 cm )  . 1 3 radiol med ( 2015 ) 120 : 1220 unfortunately , diaphragmatic injury does not heal spontaneously . 
 positive - pressure ventilation eradicates this gradient while the patient is intubated but with extubation after improvement of the patients clinical status , herniation of abdominal organs into the thoracic cavity can develop . 
the stomach , colon , omentum and spleen are the most common herniated structures when the patient has a left - sided di while the liver can herniate in cases of right - sided injury [ 6 ]  . 
the advantages of mdct make it ideally suited for the evaluation of the diaphragm and provide hope for a solution to the diagnostic conundrum of diaphragmatic injury . approach to the patient with suspected diaphragmatic injury the detection of diaphragmatic injury requires a high index of suspicion . 
the forces from impact lead to increased intraabdominal pressure with subsequent rupture of the diaphragavulsion of the attachments of the diaphragm after a lateral blow to the chest wall and direct injury of the diaphragm by fractured ribs have also been proposed as mechanisms of injury [ 9 ]  . 
blunt diaphragmatic injury occurs more often on the left side due to congenital weakness of the posterolateral area of the left hemidiaphragm and the protective effect of the liver on the right side . 
in addition , the steering wheel is located on the left side in the majority of countries , resulting in more left - sided injuries related to impact from the steering wheel . 
left - sided tears have been reported in 5686 % of cases [ 8 , 9 ] , in comparison with right - sided injuries which are estimated to occur in 11 39 % of cases . 
penetrating di often occurs ( 42 % ) in patients with wounds in the thoracoabdominal area defined by the nipple line superiorly and the costal margin inferiorly [ 4 ]  . 
stab wounds usually penetrate the left hemidiaphragm due to the predominance of righthanded attackers . despite its low sensitivity , chest radiographs can have a useful role in the initial imaging evaluation of patients with suspected diaphragmatic injury . 
they include the presence of gas - containing hollow viscera within the thoracic cavity and an abnormal course of the nasogastric tube with its distal end projecting above the diaphragm [ 16 ]  . 
nonetheless , most patients with di show nonspecific signs on chest radiographs including obliteration of the diaphragmatic contour , mild elevation of the injured diaphragm , shift of the mediastinum to the contralateral side , or evidence of additional traumatic thoracic injury ( pneumothorax , pleural effusion , or rib fractures ) [ 6 ]  . 
however , when these findings are present , the emergency radiologist should raise suspicion for diaphragmatic injury and advise the clinicians to carefully inspect 1 3 14 radiol med ( 2015 ) 120 : 1220 the diaphragm during surgery . 
the interpretation of chest radiographs in trauma patients requires significant expertise and emphasizes the essential role of the emergency radiologist embedded in the trauma bay . conventional ct had a low sensitivity for detection of diaphragmatic injury ( ranging 1461 % ) and moderate specificity ( 7699 % ) [ 12 , 17 ]  . 
 [ 19 ] reported a range of sensitivities from 73 to 100 % and a range of specificities from 50 to 92 % for the diagnosis of penetrating diaphragmatic injury using 64 - section mdct . 
some indirect signs like the band sign , described below , are better appreciated on coronal multiplanar reformations of images obtained in portal venous phase . mdct signs of diaphragmatic injury there are numerous ct signs of diaphragmatic injury . 
we would like to focus on the signs that we find useful in our combined experience of more than 50 years of interpretation of trauma imaging . a segmental diaphragmatic defect or discontinuous diaphragm is a highly specific but non - sensitive sign of diaphragmatic injury . 
as expected , higher sensitivity ( up to 90 % ) was shown in cases of blunt diaphragmatic injury due to the typically larger size of the defects [ 15 ]  . 
c sagittal reformation in the same patient clearly demonstrates a diaphragmatic defect ( white arrows ) and herniated bowel loops ( white arrowheads ) 1 3 radiol med ( 2015 ) 120 : 1220 fig . 
2 sagittal reformation of axial contrast - enhanced 64 - mdct shows a large left diaphragmatic defect ( white arrows ) with herniation of omental fat ( white arrowheads ) and the stomach ( black arrowheads ) [ 15 , 19 ]  . 
the shortened acquisition time of 64 - section mdct scanners eliminates these artifacts and improves the quality of mprs . the specificity of the presence of a segmental defect ranges from 90 to 100 % in blunt and penetrating injuries [ 6 , 17 , 19 ]  . 
b contrast reformation in the same patient confirms the diaphragmatic injury discontinuity of the posterior diaphragm is an anatomic variant described in 11 % of normal patients [ 22 , 23 ]  . 
therefore , the sensitivity of abdominal herniation on mdct for right - sided blunt di is 850 % versus 4291 % for left - sided injury [ 6 ]  . 
the radiologist has to consider that a collar sign can be seen in congenital and acquired nontraumatic diaphragmatic hernias and strive to corroborate this sign with additional evidence of diaphragmatic injury . the ongoing challenge to detect right - sided injuries coupled with advancements in imaging technology , including the routine use of multiplanar reformations , led to the description of two additional signs of right - sided injury the hump and band signs [ 9 ]  . 
4 axial contrast - enhanced 64 - mdct in a patient after a motor vehicle accident shows a nontraumatic defect of the left hemidiaphragmeticulous review failed to identify any signs of diaphragmatic rupture or injury to other organs is better appreciated on coronal mprs . 
its sensitivity for the detection of di is 54 % and specificity is 98 % [ 18 ]  . visualization of abdominal visceral or fat herniation into the pleural cavity is an important sign of diaphragmatic injury . 
7 a coronal reformation of axial contrast - enhanced 64 - mdct depicts a large left segmental diaphragmatic defect ( white arrows ) with herniation of small bowel loops ( black arrows ) and a colonic loop ( white arrowheads )  . 
b sagittal reformation in the same patient shows thickening of herniated small bowel loops ( white arrowheads ) and colon ( white arrows ) suggesting bowel ischemia that the band of low density is created as a result of compression of the liver by the injured diaphragm with subsequent hepatic hypoperfusion . 
the radiologist should be cautious not to misinterpret the band sign as a linear hepatic laceration [ 21 ]  . in healthy subjects , intraabdominal organs are always separated from the posterior chest wall by the costophrenic sulcus . 
in patients with di , the abdominal organs are no longer supported posteriorly by the diaphragas a result , they fall to a dependent position , obliterate the sulcus , and abut the posterior ribs . 
it has a sensitivity of 90 % and specificity of 100 % in cases of blunt di [ 25 ] , but is not helpful in cases of penetrating diaphragmatic injury due to the small size of the rents . 
10 axial contrast - enhanced 64 - mdct depicts the dependent viscera sign due to rupture of the left hemidiaphraga colonic loop ( white arrows ) abuts the left posterior chest wall . 
9 axial contrast - enhanced 64 - mdct in a patient with rupture of the right hemidiaphragm shows the dependent viscera sign with the right lobe of the liver abutting the posterior chest wall ( white arrows ) cause diaphragmatic thickening . 
reported a sensitivity of 36.3 % for detection of left - sided blunt injury and a sensitivity of 100 % for right - sided blunt injury [ 20 ]  . the constant search for new sensitive and specific signs of penetrating diaphragmatic injury led to the description of a new sign by bodanapally et al.the contiguous injury sign [ 4 ]  . 
when a weapon penetrates the diaphragm , it creates a contiguous injury on both sides of the diaphrag of note , the diaphragmatic defect itself can be missed in these cases due to its small size . 
this is more applicable to lowenergy knife wounds , as opposed to high - energy gunshot wounds , which can cause secondary cavitations without direct penetration [ 4 ]  . 
as with multiple signs described above , the contiguous injury sign is better appreciated on mprs . a rent of the diaphragm disrupts the thoracoabdominal border and allows free passage of air and fluid from the thorax to the abdomen and vice versa . 
therefore , the simultaneous presence of pneumothorax and pneumoperitoneum and / or hemothorax and hemoperitoneum are indirect ct signs of diaphragmatic injury [ 6 , 17 , 20 ]  . 
the simultaneous presence of blood on either side of the diaphragm should be regarded as a marker of severe injury and lead to a prompt assessment of the diaphragm as well as a search for the more sensitive signs of di . 
it can be an onerous task because blood may mask segmental diaphragmatic defects [ 17 , 18 , 27 ]  . summary despite advances in imaging technology , diaphragmatic injury is still a challenging condition for prospective radiological interpretation . 
therefore , the radiologist must remember to look for indirect signs , such as the presence of contiguous injuries on both sides of the diaphragthe radiologist must also pay special attention to multiplanar reformations , since many described signs of di are better appreciated on the reformations . 
64 - section or higher mdct with its high resolution and better quality of multiplanar reformations is the modality of choice for the evaluation of trauma patients with this often life - threatening entity . 
in contrast , almost 90 % of cases in adults are secondary to various pathologies that serve as a lead point , such as polyps , meckels diverticulum , colonic diverticulum , or malignant or benign neoplasthe aim of the present study was to assess the capabilities of multislice computed tomography ( msct ) in the diagnosis and correct characterisation of intussusception , especially in distinguishing between intussusceptions with a lead point and those without . 
 indeed , although the msct findings that help to differentiate between lead point and non - lead point intussusceptions have not been well studied , abdominal msct remains the most sensitive radiological tool to confirm bowel intussusceptions . 
grassi dipartimento medico chirurgico di internistica clinica e sperimentale magrasi e lanzara - sezione di diagnostica per immagini , seconda universit di napoli , piazza miraglia 2 , 80138 naples , italy f . 
massimo , penne , asl pescara , pescara , italy for directing the patient towards the most appropriate treatment , avoiding surgery when not necessary . keywords adult intussusception computed tomography multislice abdominal imaging intestinal disease introduction intussusception is defined as the telescoping of a proximal segment of intestinal tract ( intussusceptum ) into the adjacent distal segment ( intussuscipiens ) [ 15 ]  . 
rarely , it may happen that a distal segment of the bowel telescopes into the lumen of the adjacent proximal segment , which is known as retrograde intussusception [ 6 ]  . 
because paediatric intussusception is usually idiopathic and lacks a lead point ( sine materia intussusception ) , most cases are treated with nonoperative reduction [ 1 , 8 , 9 ]  . 
in contrast , almost 90 % of the cases of adult intussusception are secondary to pathological conditions , such as malignant or benign neoplasms , polyps and meckels diverticuluthese conditions serve as leading points by altering bowel motility and are usually discovered intraoperatively [ 15 , 919 ]  . 
adult colonic intussusception is associated with primary carcinoma in 6570 % of cases [ 20 , 21 ] , while adult small bowel intussusceptions are secondary to a malignancy in 3035 % of cases [ 4 , 9 , 13 , 20 , 22 ]  . 
as a result , most authors recommend operative exploration to prevent or treat the resultant bowel obstruction and diagnose or exclude an underlying malignancy [ 9 , 20 ]  . 
in the past , the 1 3 106 radiol med ( 2015 ) 120 : 105117 diagnosis was mostly based on surgical findings in patients with obstructive symptoms [ 13 , 17 , 23 ]  . 
nowadays , intussusceptions are almost entirely recognised by radiologists on multislice computed tomography ( msct ) , by detecting the typical bowel - within - bowel appearance [ 1 , 2 , 16 , 19 , 2431 ] , even though the aetiology may remain obscure [ 2 , 16 ]  . 
moreover , with the increased use of msct , cases of transient intussusceptions , previously considered only as a paediatric condition , are now diagnosed even in adults [ 14 , 15 , 3236 ]  . 
transient non - leading point intussusceptions ( nlpi ) are more likely to resolve spontaneously , while leading point intussusceptions ( lpi ) are to be considered serious conditions with an underlying cause likely to persist or recur without surgery [ 18 , 19 , 37 , 38 ]  . 
we present a series of patients with bowel intussusceptions with the aim of reviewing all the radiological features of this disease in adults , with regard to the findings that help to differentiate nlpi from lpi and therefore to avoid unnecessary surgery . materials and methods population all abdominal msct scans performed from january 2008 to december 2012 at our department of radiology were reviewed by two radiologists . 
forty - seven consecutive adult patients ( 46.81 % male , 53.19 % female , age range 3971 years , median age 49 years ) with radiological or surgical evidence of intussusception were retrospectively selected . 
our institutional review board approved this retrospective single - centre study . imaging all patients underwent at least one abdominal and pelvic msct with distension of the bowel loops by enteroclysis , using water as an oral contrast agent . 
to adequately enhance mesenteric vessels and bowel wall , intravenous ( iv ) injection of contrast medium was performed in all patients with an injection rate of 4 ml / s . 
then , all possible associations between the different symptoms reported at presentation were studied using the chi - square test modified by yates and the fisher exact test , as shown in table 2 . 
further tests were performed using the chi - square test and the standardised residuals method to verify correlations between all the parameters shown in table 1 : the most significant tests are listed in table 3 . 
a previous abdominal trauma was described in 3 / 16 ( 18.75 % ) of patients with idiopathic intussusception . imaging the target pattern corresponds to an early intussusception with only minimal obstruction and no sign of ischaemia at pathology . 
this feature was found in 14 / 16 ( 87.5 % ) patients with idiopathic intussusception and in 20 / 31 ( 64.5 % ) with an underlying pathological process . 
the reniform pattern is described as a bilobed density with peripheral high attenuation and lower attenuation centrally , as a result of thickening bowel wall surrounding the 1 3 108 radiol med ( 2015 ) 120 : 105117 table 4 aetiology : underlying cause in patients with intussusceptions parameter : aetiology no . 
only percentages in bold type refer to the whole population a indicates postoperative intussusceptions intussusceptuthis feature was detected in 2 / 16 ( 12.5 % ) patients with idiopathic intussusception and in 8 / 31 ( 25.8 % ) with an evident leading point . 
the sausage shape results from alternating areas of low and high attenuation related to the bowel wall , mesenteric fat and fluid , intraluminal fluid , contrast material or air . 
on the contrary , 25.8 % ( 8 / 31 ) of all lpi were double intussusceptions and 6.38 % ( 2 / 31 ) were complicated with msct evidence of mesenteric vascular impairment . 
among the nonsurgical patients , no one required subsequent operative exploration for intussusception at a mean 13.2 - month follow - up . treatment operative treatments were performed in 68.1 % ( 32 / 47 ) of patients . 
on the contrary , adult intussusception is considered a rare condition , representing only 5 % of all intussusceptions [ 1 , 79 , 13 , 17 , 18 ] , and thus accounting for 15 % of all adult intestinal obstructions [ 7 , 39 ]  . 
the growing use of msct imaging has increased the radiologists ability to detect intussusceptions , even those without any clear evidence of underlying diseases [ 9 , 16 , 18 , 19 , 23 , 24 , 31 ]  . 
 among all the retrospective studies found in the literature , only few enrolled more patients than this study , whereas none of them classified bowel intussusceptions in adults according to as many parameters as we did . 
1 , 2 , 3 , 4 , 5 , classification : location according to this parameter , intussusceptions can be divided into : ( a ) entero - enteric , when confined to small bowel ; ( b ) colo - colonic , when involving only the large bowel ; ( c ) entero - colonic , which can be ileo - caecal when the ileo - caecal valve is not prolapsed , or ileo - caecal - colonic in case of prolapsed ileo - caecal valve [ 3 , 20 , 40 , 41 ]  . 
by contrast , adult patients may present with a variety of symptoms depending on the underlying cause : lpi due to malignancy may result in abdominal pain , nausea , vomiting , obstructive symptoms , weight loss or bleeding [ 4 , 19 ] , while no obstructive symptoms are 1 3 radiol med ( 2015 ) 120 : 105117 110 fig . 
the leading point is a mass in the ascending colon , which proved to be a colon cancer ( b arrowhead ) 1 3 radiol med ( 2015 ) 120 : 105117 fig . 
 [ 48 ] , the most common findings in adult intussusceptions at presentation were abdominal pain in 73 % of patients , partial bowel obstruction in 48 % , a palpable mass in 15 % , heme - positive stools in 14 % and complete bowel obstruction in 2 % . 
similarly , in our series , abdominal pain was the most common finding at presentation , occurring in 33 / 47 ( 70.21 % ) , followed by partial bowel obstruction in 21 / 47 ( 44.68 % ) and palpable mass in 6 / 47 ( 12.77 % ) , but heme - positive stools and complete bowel obstruction were slightly more frequent , occurring in 9 / 47 ( 19.15 % ) and 5 / 47 ( 10.64 % ) , respectively . 
with regard to postoperative intussusceptions ( poi ) , symptoms mostly arise < 1 week after the initial operation [ 50 ] , with the typical nonspecific clinical presentation of idiopathic intussusceptions [ 51 ]  . 
in contrast , patients with intussusceptions due to postoperative adhesions in our study became symptomatic 3.2 weeks after surgery on average . to summarise , adult intestinal intussusception may present as : ( a ) cold intussusception , which is incidental and asymptomatic with no sign of bowel obstruction ; ( b ) subacute intussusception , which is incomplete and transient with temporary and recurrent obstruction and no impairment of mesenteric vessels ; ( c ) acute or warm intussusception , in case of complete and irreversible bowel occlusion with the onset of mechanical ileus [ 40 ]  . 
in the case of delayed surgical treatment , acute intussusception may rapidly complicate with mesenteric vessel involvement , bowel wall ischaemia and / or engorgement and , eventually , necrosis with perforation and peritonitis [ 40 ]  . classification : aetiology with regard to aetiology , it is well known that the exact mechanism of bowel intussusception in adults is unknown ( primary or idiopathic ) in 820 % of cases and is more likely to occur in the small intestine [ 1 , 9 , 52 ] , while secondary disease is believed to start from any pathological lesion of the bowel that involves the normal peristaltic activity and serves as a leading point , initiating invagination [ 9 , 31 ]  . 
actually , idiopathic intussusception ( also defined as sine materia ) has been depicted as an intussusception whose aetiology cannot be identified by imaging , exploration and / or pathological evaluation , regardless of symptoms [ 53 ]  . 
moreover , small bowel intussusception may be either secondary to intraor extraluminal lesions ( inflammatory lesions , meckels diverticulum , postoperative adhesions , lipoma , adenomatous polyps , lymphoma and metastases ) or iatrogenic , e.g. 
although intestinal intussusception secondary to inverted meckels diverticulum in adults is rare , it should be considered in the differential diagnosis for patients 1 3 radiol med ( 2015 ) 120 : 105117 112 fig . 
a , b axial scans show the telescoping of a proximal segment of intestinal tract ( intussusceptum ) into the adjacent distal segment ( intussuscipiens ) with its vascular peduncle . 
the multiplanar reconstruction displays all the different components of the lesion : intussusceptum ( inner cylinder ) , intussuscipiens ( external cylinder ) , the polypoid mass which serves as the leading point , the eccentric vascular peduncle ( d black arrowhead ) presenting with abdominal pain and bowel obstruction [ 60 ]  . 
furthermore , intussusception may also occur after surgery , such as after retroperitoneal tumour resection , ladds procedure , roux - en - y gastric bypass , diaphragmatic operation and pancreatectomy and in 0.080.5 % of patients undergoing laparotomy [ 6166 ]  . 
different theories try to explain the mechanisms that lead to poi , including altered peristalsis , early postoperative adhesions , prolonged and excessive bowel manipulation , electrolyte disturbances in lengthy surgical procedures , anaesthetic drugs , opioid analgesics and neurogenic factors [ 67 ]  . 
since the poi occurs in a wide range of procedures , whether abdominal or non - abdominal , the mechanism may be explained by more than one of these theories . 
however , a higher incidence of poi has been reported after retroperitoneal resection [ 68 , 69 ]  . classification : morphology early and accurate diagnosis is essential to avoid intestinal ischaemia , perforation and peritonitis , thus preventing fatal outcome [ 9 , 70 , 71 ]  . 
 non - hodgkin lymphoma of the terminal ileum ( white arrowhead ) telescoping of a proximal segment of the intestinal tract within the lumen of an adjacent segment ; ( b ) double intussusception , which represents an extremely rare variety of intussusception with some sporadic reports in the literature [ 71 , 72 ] and means the telescoping of previously intussuscepted ileum within the lumen of the distal ileal or colonic segment ; ( c ) complicated intussusceptions , which are established in the case of complications , such as ischaemia , ascites and perforation . 
 in our series , single intussusceptions occurred overall in 80.9 % of cases , and 14 / 16 ( 87.5 % ) of patients with nlpi and 24 / 31 ( 77.4 % ) of patients with lpi . 
moreover , double intussusceptions were identified overall in 21.3 % of patients , and in 2 / 16 ( 12.5 % ) of patients with nlpi and 8 / 31 ( 25.8 % ) of patients with lpi . 
ultrasonography may be useful also in adults [ 80 , 81 ] , showing the classical 1 3 114 radiol med ( 2015 ) 120 : 105117 target or doughnut sign on the transverse view and the pseudo - kidney or hay - fork shape on the longitudinal view [ 81 , 82 ]  . 
however , abdominal msct is nowadays considered the most sensitive radiological technique to detect and confirm intussusception , with a reported accuracy of 58100 % [ 1 , 17 , 31 , 45 , 8388 ]  . 
indeed , msct correctly defines several features of the disease , such as : the presence and intestinal origin of underlying masses ; the site of intussusception and the intestinal segments involved ; lesion edges ; mesenteric vascular impairment ; involvement of peri - visceral fat , surrounding tissues and / or loco - regional lymph nodes [ 40 ]  . 
moreover , msct may provide tumour staging in patients with malignant leading points [ 77 ]  . with regard to patient preparation and image acquisition parameters , abdominal msct with bowel distension by enteroclysis is considered the best technique to identify intussusceptions . 
furthermore , contrary to traditional positive oral contrast agents , water does not interfere with three - dimensional volume rendering ( 3d - vr ) , which is valuable for visualising impaired mesenteric vessels during surgical planning for complicated intussusceptions . 
for example , using 64 - msct , we would choose the 0.65 - collimator setting and create 0.75mm slices reconstructed every 0.5 mm for 3d - vr review [ 89 ]  . 
the real strength of msct enteroclysis lies in the ability to differentiate between presence or lack of underlying leading points : the first may result in bowel obstruction , evidence of leading masses and bowel wall oedema with loss of the classic three - layer appearance due to impaired mesenteric circulation ; the latter lacks signs of proximal bowel obstruction , target - like or sausage - shape masses and layering effect , as reported by kim et al . 
in adults , this differential is crucial to avoid unnecessary surgery : indeed , intussusceptions with no underlying pathological cause of obstruction on msct are generally self - limiting and do not require operation , while the presence of a leading mass on msct is strongly associated with cancer and needs operative treatment [ 48 ]  . 
in the same series , it is reported that operative exploration for asymptomatic incidental intussusceptions was routinely negative , suggesting that in the case of no clinical sign or specific radiographic finding of leading points , an incidental intussusception detected on msct may represent a transient , clinically unimportant event , even more common than previously thought [ 48 ]  . 
 [ 37 ] described three patterns of intussusception on msct as three different stages of the same disease : the target - like pattern , the reniform pattern and the sausage - shape pattern . 
the first appearance corresponds to an early - stage intussusception with only minimal obstruction and no sign of ischaemia at pathology ; it occurs when an intraluminal soft - tissue mass and eccentric fat density are seen as a result of the intussusceptum and the intussuscepting mesentery . 
the second pattern is described as a bilobed density with peripheral high attenuation and lower attenuation centrally , as a result of thickening bowel wall surrounding the intussusceptum , probably due to the underlying ischaemia . 
the latter pattern results from alternating areas of low and high attenuation related to the bowel wall , mesenteric fat and fluid , intraluminal fluid , contrast material or air . actually , intussusception often presents as a complex mass on abdominal msct enteroclysis . 
on axial section , the target - like pattern appears as an odd number of concentric 1 3 radiol med ( 2015 ) 120 : 105117 rings of tissue with different density , due to the alternation of bowel wall and fat . 
the same image may result in a hayfork shape on longitudinal section or in a sausage - shape pattern on oblique section . conclusion abdominal msct with bowel loop distension by enteroclysis is currently the most sensitive radiological tool to confirm bowel intussusceptions in adults . 
the radiologist can readily make a correct diagnosis , detecting specific msct findings such as the bowel - within - bowel appearance and the three different features known as target - like pattern , reniform pattern and sausage - shape pattern . 
any symptom , if present , may help guide the surgeon , but only the imaging pattern effectively helps to identify complications such as mesenteric vascular involvement and bowel wall ischaemia , thus differentiating incidental and transient disease ( cold intussusception ) from the acute and irreversible form ( warm intussusception ) , the latter needing prompt surgical treatment . 
therefore , the radiologists task is to recognise intussusception , but also to do the following : ( 1 ) define locationentero - enteric , colo - colonic or enterocolonic , which can be ileo - caecal or ileo - caecal - colonic ; ( 2 ) describe morphologysingle , double or complicated intussusceptions ; ( 3 ) focus on aetiologyevaluate suggestive symptoms and underlying pathology . 
it could involve all the abdominal parenchymas and viscera and the whole gastrointestinal tract ( from the oesophagus to the rectum ) , insomuch that the involvement of the entire colon should be considered a distinctive tract in diagnosing this condition in respect of the occlusive forms of ischaemia . 
 recognition of the characteristic ct appearances and the variations associated with a reperfusion event may help in the accurate interpretation of ct in the diagnosis and management of nomi . keywords nonocclusive mesenteric ischaemia multidetector computed tomography mesenteric infarction reperfusion injury superior mesenteric artery mesentery introduction nonocclusive mesenteric ischaemia ( nomi ) is an acute mesenteric circulatory disorder that is not caused by an organic occlusion of blood vessels , in contrast to a mesenteric arterial occlusion , which is induced by a blockage of the blood flow by emboli and thrombi [ 1 ]  . 
it may involve all abdominal parenchymas and viscera and the whole gastrointestinal tract ( from the oesophagus to the rectum ) , insomuch that the involvement of the entire colon should m . 
volterrani department of medical , surgical and neuro sciences , diagnostic imaging , university of siena , viale bracci 10 , 53100 siena , italy e - mail : mmazzei@sirm.org be considered a distinctive tract in diagnosing this condition in respect to the occlusive forms of ischaemia . 
many more cases have been described since then and today nomi is reported to be responsible for approximately 2030 % of all intestinal ischaemic events , although its incidence has increased due to an ageing society , the high number of cardiothoracic and major abdominal surgeries , and an increase in the dialysis population [ 1 , 3 ]  . intestinal vasospasm due to persistent low perfusion is the principal cause of the ischaemic disorder in nomi and therefore the principal aim of current therapy is to reduce the spasm and improve perfusion of the mesenteric artery using vasodilators . 
conversely , surgery should be limited to the excision of irreversibly necrotised intestine , in particular when reperfusion , a very frequent event in nomi , appears to be ineffective [ 1 , 4 , 5 ]  . 
however , because of the uncertain clinical status and the fact that many nomi patients are misdiagnosed , the prognosis of nomi is extremely poor and its mortality rate has not changed over time [ 6 , 7 ]  . 
that being so , the role of imaging in diagnosing nomi is crucial : firstly for the early identification of this critical condition , to plan the correct therapeutic approach , which is based on a different treatment from those of the occlusive forms of acute mesenteric ischaemia ( ami ) , then to recognise the presence of reperfusion , characterise its effectiveness , and guide the surgical excision of irreversibly necrotised intestinal tract [ 3 , 8 ]  . 
this review aims to increase awareness regarding the pathogenesis and the clinical , laboratory and imaging features of nomi , and in particular to describe the ct findings of nomi with and without a reperfusion event and to correlate these with pathological features . 1 3 86 radiol med ( 2015 ) 120 : 8595 fig . 
1 vessel and mesentery computed tomography ( ct ) findings in the early phase of nonocclusive mesenteric ischaemia ( nomi ) : contrast - enhanced coronal image of abdomen in a 76 - year - old man hospitalised for heart failure and with abdominal pain : a narrowing of the superior mesenteric artery ( sma ) with poor demonstration of the branches of the arteries is shown ( a ) ; a reduction in calibre and number of mesenteric vessels is also shown in axial ct image ( b ) pathogenesis regarding pathogenesis , in nomi bowel ischaemia and infarction can occur because of a reduction in the mesenteric blood supply without vascular occlusion due to an intestinal vasospasm for a persistent low perfusion . 
it usually develops during an episode of cardiogenic shock , septicaemia , dehydration or a state of hypoperfusion in which excessive sympathetic activity results in secondary vasoconstriction of the mesenteric arteries ( superior and inferior ) , which is often superimposed on a pre - existing atherosclerotic plaque . 
however , pharmacological factors ( administration or abuse of digitalis , ergotamine or other vasoconstrictive agents ) can also represent common causes of nomi [ 13 , 9 , 10 ]  . 
the ischaemic injury in nomi may range from reversible superficial damage , localised to the watershed areas , to a more severe form that extends to the entire bowel , depending also if reperfusion occurs [ 11 ]  . 
2 mesentery and bowel wall ct findings of nomi with an ineffective reperfusion event : unenhanced ct coronal ( a ) and axial ( b , c ) images of the abdomen in a 49 - year - old man with a history of surgical intervention for a type a aortic dissection , hospitalised for heart failure during a wedding party : both mesenteric fat stranding and free peritoneal fluid due to a reperfusion event are shown in ( a ) ; thickened loops with high attenuation of the wall is also shown in the axial ct image ( b )  . 
3 bowel wall ct findings of nomi with an effective reperfusion event : contrast - enhanced ct axial ( a , b ) and coronal ( c , d ) images of the abdomen in a 74 - year - old woman with a diagnosis of nomi with reperfusion after a cardiogenic shock during major abdominal surgery : thickened loops ( duodenum and jejunum ) with mural oedema and mucosal hyperenhancement are shown at first ct examination ( a , c ) ; the ct examination performed after 5 days of medical therapy demonstrated a significant reduction of bowel wall mural oedema ( b , d ) area also in a nonconsecutive manner and histopathological findings including haemorrhagic and necrotic changes , as well as small veins without fibrin plugs [ 12 ]  . 
the discontinuous segmental necrosis is a marked distinguishing feature of nomi from occlusive mesenteric ischaemia / infarction , in which the mesentery and the intestine are involved and eventually necrotised from the site of the thrombus , forming a sphenoidal necrotic area in the region served by the artery or vein ( continuous necrosis ) [ 12 ]  . clinical aspects and laboratory findings nomi occurs more frequently in elderly patients who have associated comorbidities such as systemic atherosclerotic disease , congestive heart failure , cardiac arrhythmias , coronary artery disease , or hypovolemia and hypotension due to various causes [ 13 ]  . 
clinically , nomi can be present with abdominal pain , nausea , vomiting , gastrointestinal haemorrhage and ileus symptoms , but the characteristic early symptoms and laboratory test results are unclear [ 1315 ]  . 
 in particular , the detection of subjective symptoms is difficult in cases that develop and advance after surgery because the patients clinical condition and the effects of general and epidural anaesthesia may conceal the symptoms and disease may develop and advance unnoticed [ 3 , 16 ]  . 
different plasma biomarkers such as d - lactate , intestinal fatty acid binding protein ( i - fabp ) , alphaglutathione s - transferase and d - dimer have been tested in humans . 
i - fabp and alpha - glutathione s - transferase are both located in the mucosa of the small intestine , and d - lactate originates from bacteria in the intestinal lumen as a normal product of bacterial fermentation . 
 as intestinal damage during ami starts from the intestinal mucosa , all these markers seem to have the potential to be used as diagnostic tests in the early phases of intestinal ischaemia . 
in particular , in contrast to l - lactate , the d - isomer of lactate ( d - lactate ) is metabolised very slowly by the liver , and elevated levels may be an indicator of bacterial translocation , intestinal mucosal injury and , although not exclusively , ami [ 17 ]  . 
however , none of the proposed plasma - derived tests for ami has , as yet , entered routine clinical practice because the performance of the currently 1 3 88 radiol med ( 2015 ) 120 : 8595 fig . 
4 bowel wall ct findings of nomi without an with reperfusion event : contrast - enhanced ct axial ( a ) image of the abdomen in a 63 - year - old man with a prolonged cardiac arrest during pacemaker implantation . 
both a focal absence or reduction of contrast enhancement of the bowel wall and free peritoneal fluid were present ( a ) ; a surgical specimen demonstrated a discontinuous segmental necrosis ( b ) : the patient survived the surgical procedure . 
both thickened loops with mural oedema and small bowel mucosal hyperenhancement are shown ( c ) : a surgical exploration demonstrated signs of effective reperfusion ( d ) : the patient received medical treatment available serological markers is suboptimal for routine clinical use . 
furthermore , because the diagnosis of nomi is clinically difficult to be suspected , the routine blood biomarkers are not always tested before imaging and often the tested biomarkers , like white blood cell ( wbc ) count or lactate dehydrogenase ( ldh ) , may provide a normal result in particular in hospitalised patients , who often arrive for a ct examination during the early phase of nomi . 
as a result , the clinical lesson about blood biomarkers should be that when a patient suffers from vague abdominal symptoms soon after a major cardiovascular or abdominal operation , even if the blood markers , such as an elevation of lactic acid , ldh , and / or ck are absent , nomi should be considered as one of the presumed causes [ 3 , 16 ]  . diagnostic imaging because early diagnosis is difficult , today nomi represents the most lethal form of ami with a mortality rate ranging from 70 to 90 % [ 6 ]  . 
indeed , medical treatment , and in recent years perfusion therapy using vasoactive substances ( continuous administration of vasodilators such as papaverine , peg1 , and nitroglycerine into the mesenteric artery ) has gained an important role in the successful treatment of nomi , confining only the advanced forms with necrosis of the involved tract to surgery [ 4 , 5 ]  . 
in this context , imaging plays a pivotal role in the differential diagnosis between occlusive and nonocclusive forms of ischaemia [ 4 , 5 , 8 , 2124 ]  . 
despite the technical evolution of noninvasive methods , such as multi - detector ct ( mdct ) , many authors claim that angiography should still be considered as the gold standard diagnostic technique which reliably establishes an early diagnosis of nomi by demonstrating the narrowing of the branches of the superior mesenteric artery as described by boley et al . 
 ( the so - called string - of - sausages sign : alternate dilation and stenosis of the superior mesenteric arterial branches ) , spasm of the intestinal marginal artery , and poor contrast enhancement of veins into the muscular layer , as the many features of vasospasm associated with nomi [ 2528 ]  . 
5 ct evaluation of attenuation differences ( hounsfield unit measurements ) of the bowel wall between the unenhanced and contrast - enhanced ct in a case of ineffective reperfusion event : there is high attenuation of the bowel wall without a significant hu difference between the unenhanced ( a ) and contrast - enhanced ct ( b ) , which could represent a sign of ineffective reperfusion ; a surgical specimen of that loop showed both signs of necrosis and reperfusion ( c , d ) : the patient survived the surgical procedure or unstable systemic conditions , and an angiography may not be possible due to its complexity and invasiveness ; however , today mdct can provide high - quality images that are comparable to an angiogram with less invasiveness and less time [ 29 , 30 ]  . 
firstly , mdct represents a fast noninvasive study that also evaluates other causes of abdominal pain and secondly it is a fast and noninvasive diagnostic tool for evaluating both vascular ct findings , like the narrowing of the superior mesenteric artery ( sma ) with poor demonstration of their branches , and nonvascular ct findings , such as abnormalities in the bowel wall , mesentery and peritoneal cavity and not only restricted to the mesenteric vessels [ 31 ]  . 
at the time of writing , there are only a few articles relating to the effectiveness of mdct for the diagnosis of nomi and some with only a small case series ( four patients ) [ 4 , 5 , 29 , 30 ]  . 
moreover , these authors underline the effectiveness of mdct for the diagnosis of nomi by assessing the morphology and diameter of the sma on multi - planar reconstructed images , comparing it to an angiography examination . 
nevertheless , the great advantage of mdct is the possibility to also show the bowel wall abnormalities that often guide the treatment of the patient ( surgical or nonsurgical )  . 
mdct is also the best diagnostic modality to investigate possible reperfusion events , which are more frequent in nomi than in the occlusive type of ami ; as such , also the appearances of nomi at imaging could be different depending on these reasons and on the timing of the ct examination [ 23 , 24 ]  . ct examination mdct imaging protocol and suggestion for imaging evaluation oral and rectal administration of contrast material is not recommended ( or useful ) for accurate ct examination and assessment of acute bowel ischaemia , as it does not add any additional information for the final diagnosis , but also because of the severe clinical condition of the patient and the need to keep the investigation time to a minimuct images should be obtained from the dome of the liver to the perineum to cover the entire course of the intestine . 
the examination should be performed with a spiral technique in the cranio - caudal direction ( from the base of the lungs to the pelvic brim ) and with the patient in the supine position . 
 with mdct scanners , the following technical parameters could be used : effective slice thickness of 3.75 mm for plain 1 3 radiol med ( 2015 ) 120 : 8595 fig . 
6 consecutive abdominal x - ray examinations ( ac ) of a 84 - year - old man with a history of chronic heart failure and acute abdominal pain : a progressive bowel dilation involving also the entire colon is shown . 
ct examination ( d ) performed immediately after the last x - ray examination demonstrated a colonic pneumatosis : the patient died 1 h after the ct examination acquisition and 12.5 mm for contrast - enhanced ct ( both late arterial , 4550 s , and portal venous phase , 7080 s ) , beam pitch of about 1 , reconstruction interval of about half or less than half of the effective slice thickness to improve the multi - planar 2d reconstruction and the ct angiography analysis ; tube voltage of 120140 kvp and reference mas of 250500 mas according to the patients body mass index . 
the main roles of unenhanced ct are to identify a possible high attenuation of the bowel wall ( reperfusion condition or intramural haemorrhage ) or to obtain a baseline attenuation measurement of the bowel wall for the assessment of its enhancement . 
it also could be useful for monitoring the patient after medical treatment in the case of reperfusion , evaluating the reduction or increase of free intraperitoneal fluid or of the dilation of the bowel lumen , and for detecting signs of bowel wall necrosis like the presence of intestinal pneumatosis [ 32 ]  . 
on the other hand , the main roles of contrast - enhanced ct are : to make a differential diagnosis with occlusive ischaemia ( by identifying thrombi in the mesenteric arteries and veins ) or other causes of acute abdomen ( including ischaemic changes in bowel obstruction ) , to evaluate the degree of bowel wall contrast enhancement ( absent in the case of necrosis ) , and the presence of hypoperfusion phenomena of other organs . 
 contrast - enhanced scans should be performed in the late arterial phase ( start delay 4550 s ) and in the portal venous phase ( start delay 7080 s ) with an intravenous injection of 2 ml / kg of nonionic contrast material followed by 40 ml of saline solution using an automated power injector ( 34 ml / s flow rate ) , with an 18 - gauge needle in the antecubital ve it is always recommended to visualise the ct images with different window and level settings . 
in fact , a window set on the soft tissue values ( width , w : 300350 ; level , l 4050 ) could demonstrate alterations of the bowel wall , abdominal organs , mesentery and vascular structures ; the window setting used to visualise the lung parenchyma ( w : 450100 ; l : 1000 ) will aid the recognition of extraluminal 1 3 radiol med ( 2015 ) 120 : 8595 regarding the arterial findings are superimposable to those of angiography . 
in particular , the original axial images and mpr images show irregular narrowing of the sma and ima , spasm of the arcades of mesenteric arteries , and impaired filling of intramural vessels . 
however , the calibre of the sma and ima could be regular during and after the reperfusion event . mesentery the most common feature described regarding the mesentery in ami is mesenteric fat stranding . 
mesenteric fat stranding and ascites appear with transudation of fluid in the mesentery or peritoneal cavity caused by an elevation of mesenteric venous pressure , which is commonly seen in strangulating bowel obstruction and veno - occlusive bowel ischaemia [ 23 , 24 , 33 ]  . 
on the contrary , in patients with nomi , as in arterial occlusive mesenteric ischaemia , mesenteric fat stranding appears only when reperfusion occurs or in advanced conditions of ischaemia with transmural infarction , when hypoperfusion results in increased vascular permeability that leads to extravascular leakage of plasma , red blood cells ( rbcs ) , or both into the bowel wall , mesentery , and peritoneal cavity . 
7 ct findings of peritoneal cavity ( 1 ) : axial contrast - enhanced ct image of abdomen in a 64 - year - old woman waiting for heart transplantation and hospitalised for abdominal pain showed hypoperfusion phenomena involving the spleen ( a ) and both kidneys ( b ) gas [ 21 ]  . 
in cases of nomi , 2d multi - planar reconstruction ( mpr ) and maximum intensity projection ( mip ) are useful for evaluating the morphologic appearance and diameter of the superior mesenteric artery , by searching for the same angiographic criteria addressed by siegelman et al . 
 [ 27 ] for the diagnosis of mesenteric vasospasm : ( 1 ) narrowing at the origins of the major branches with involvement of segments of the superior mesenteric artery ; ( 2 ) irregularities at the origins of the major branches of the superior mesenteric artery ( beading sign or string - of - sausage sign ) ; and ( 3 ) spasm of the arcades of mesenteric artery , and impaired filling of intramural vessels . ct findings mesenteric vessels no sign of sma , inferior mesenteric artery ( ima ) or superior and inferior mesenteric vein ( smv / imv ) thrombosis or occlusion were found at contrast - enhanced ct examination . 
in the early phase of nomi , ct appearances bowel wall ct findings in nomi are similar to those observed in acute arterial ischaemia [ 36 , 37 ]  . 
in particular , in the early phase of nomi or when reperfusion does not occur , the bowel wall appears paper - thin because there is no 1 3 92 radiol med ( 2015 ) 120 : 8595 fig . 
8 ct findings of peritoneal cavity ( 2 ) : axial ( a ) and sagittal ( b ) contrast - enhanced ct images of the abdomen in a 76 - year - old woman with a cardiogenic shock during major abdominal surgery . 
on unenhanced ct , it is possible to observe low attenuation of the bowel wall that indicates bowel wall oedema caused by a reperfusion event , or high attenuation of the wall that generally represents a condition of intramural haemorrhage or haemorrhagic infarction in the late phase of ineffective reperfusion . 
from a pathological point of view , the bowel wall can become thickened in cases of reperfusion due to the effects of the reperfusion that are superimposed on the ischaemic damage by hypoperfusion , with oedema and thickening of the submucosa , marked vascular congestion , and granulation tissue [ 12 , 36 ]  . 
 a contraction of the bowel loops could be observed in the early phase of nomi ( spastic reflex ileus ) , whereas in the following phase the bowel lumen is often dilated because of an interruption of normal bowel peristalsis with only a gasfilled appearance ( hypotonic reflex ileus ) , whereas in the late phase of nomi both the fluid - filled appearance ( paralytic ileus ) and intestinal pneumatosis could be observed . 
in our case series , it was present in 78.57 % of ct examinations whereas free air in the peritoneal cavity was observed rarely and as a consequence of bowel wall perforation owing to an ineffective reperfusion event . 
the increase of peritoneal free fluid , like mesenteric fluid , has a negative prognostic meaning as it occurs in the late stage of ischaemia or during an ineffective reperfusion event . 
however , amongst various conditions of mesenteric ischaemia , nomi is the most difficult to diagnose at imaging because it is often a dynamic condition owing to the reperfusion event . 
today ct represents an essential diagnostic tool in this critical condition thank to the possibility of demonstrating both vascular and nonvascular findings ; however , for a correct diagnosis , a technically appropriate ct examination and an accurate interpretation of images are mandatory . 
the evaluation of the ct findings of mesentery , bowel wall , and peritoneal findings , in addition to the vessel features , suggests a possible diagnostic utility for discriminating nomi with and without reperfusion as well as a possible prognostic value ( table 1 )  . 
therefore , the introduction of mdct in the decision tree of nomi treatment may bring the benefit of an early identification of this critical condition , so as to plan the correct therapeutic approachwhich is based on different treatments from those required by the occlusive forms of amito recognise the presence of reperfusion and to characterise 1 3 94 radiol med ( 2015 ) 120 : 8595 its effectiveness and to guide the surgical excision of irreversibly necrotised intestinal tract . 
laghi department of radiological sciences , oncology and pathology , sapienza university of rome , icot hospital , via franco faggiana 34 , 04100 latina , italy e - mail : andrea.laghi@uniroma1.it and if associated with portomesenteric vein gas , when observed in an acute abdominal setting should raise the suspicion of mesenteric infarct and prompt a careful search for other signs of intestinal involvement , so as not to miss cases of life - threatening intestinal infarct or allow them to further evolve into extensive necrosis with worse prognosis . 
pneumatosis can occur as a primary ( or idiopathic ) form in 15 % of cases or as a secondary form in 85 % of cases [ 2 ]  . 
nevertheless , these findings have been reported in a wide range of pathological conditions including intra - abdominal abscess , diverticular disease , pylephlebitis , inflammatory bowel disease , acute gastric or intestinal dilatation , hepatic transplant , barium 1 3 radiol med ( 2015 ) 120 : 96104 pathogenesis although ip and pmp are usually discussed separately in the literature , they have always been considered to be related phenomena ; in fact , passage of gas into the mesenteric and portal veins starts from the bowel wall collection of gas . 
another theory , which is better applied to the congenital form of ip pneumatosis cystoides intestinalis , suggests that increased intestinal permeability would permit penetration of anaerobic , gas - producing bacteria into the intestinal wall , with subsequent ip [ 2830 ]  . 
 the subsequent step after ip is migration of gas along the mesenteric veins draining the intestine to the portal vein and its branches into the liver [ 2 , 6 , 31 ]  . 
this particular peripheral localisation of gas also permits an easy distinction from pneumobilia in which fluid pushes the gas in the opposite direction , towards the hepatic hiluin this pathogenetic model ip precedes pmp and we can expect that isolated ip is associated with less advanced conditions . 
 gastric pneumatosis can also be seen ( black arrow ) enema , umbilical catheterisation , chronic pulmonary disease , corticosteroid therapy , gastric volvulus , intestinal hernias , ingestion of corrosives , carcinoma of the colon , colonoscopy either optical or virtual , drugs , ulcerative disease , and trauma [ 625 ] ( table 1 )  . 
 portal pneumatosis ( black arrow ) and parietal gastric pneumatosis ( white arrowheads ) in intestinal infarct table 1 causes of intestinal pneumatosis ( ip ) and portomesenteric pneumatosis ( pmp ) ( a ) increased mucosal permeability pneumatosis cystoides intestinalis drugs ( corticosteroids , chemotherapeutic agents ) abdominal infections neoplasms solid organ and bone marrow transplantation inflammatory bowel diseases intra - abdominal abscess infectious diseases ( b ) mucosal disruption intestinal ischaemia bowel obstruction ulcerative disease blunt trauma diverticular disease ingestion of corrosives intestinal carcinoma iatrogenic causes acute gastric or intestinal dilatation endoscopy feeding tube ( naso - gastric and naso - jejunal ) post - surgical anastomoses drugs ( corticosteroids , antineoplastic agents ) ( c ) pulmonary conditions ( alveolar rupture with interstitial dissection chronic obstructive pulmonary disease ( copd ) , bronchitis , by air bubbles ) emphysema asthma cystic fibrosis positive end - expiratory pressure ( peep ) is clinical and experimental evidence that bacteria are involved in the pathogenesis since the gas was found to be nitrogen on pathological specimens , the experimental radiol med ( 2015 ) 120 : 96104 fig . 
a small amount of gas located in a mesenteric vein ( white arrow ) is clearly visible thanks to the proper window that allows a clear distinction of gas from fat injection of bacteria in the intestinal submucosa caused pneumatosis , and in some cases pneumatosis resolved after antibiotic or hyperbaric therapy [ 2832 ]  . 
in one case it was observed in the systemic veins ( gluteal veins , haemorroidal plexus , periprostatic veins , femoral veins ) associated with portomesenteric pneumatosis and an extensive intestinal infarct [ 34 ]  . 
6 linear pattern of intestinal pneumatosis in intestinal infarct ( white arrowhead ) ip and pmp have long been considered a capital sign of advanced intestinal infarction and a predictor of poor prognosis . 
 b circumferential pattern of pneumatosis in the oesophagus of a patient with a massive intestinal infarct ( black arrows ) 1 3 100 radiol med ( 2015 ) 120 : 96104 of portal pneumatosis was questioned and it appeared due to many pathological processes and no longer associated with high mortality rates . 
analysed the correlation between ip or pmp , or both , the severity of mural involvement , and the clinical outcome in 23 patients with bowel ischaemia concluding that these findings do not allow prediction of transmural bowel infarction because they may be observed with only partial ischaemic bowel wall damage ; furthermore they state that both these signs are unrelated to advanced infarct also in the setting of bowel ischaemia [ 33 ]  . the clinical significance of ip and portomesenteric venous gas ( pvg ) changed significantly over time , with the findings appearing more closely related to advanced intestinal infarct , and their prognostic value appearing strongly reduced , with important repercussions on clinical practice . wiesners group also noted a difference between the ip patterns , with the band - like pattern being more closely correlated to transmural infarction than the bubble - like pattern ( 90 % versus 70 % of patients )  . 
they also observed that pmp was associated with transmural bowel infarction in 81 % of patients , and pronounced pmp was slightly more often associated with transmural bowel infarction ( 86 % ) than mild pmp ( 78 % )  . 
finally if both ct findings of pneumatosis and portomesenteric venous gas were seen , their presence was associated with transmural bowel infarction in 91 % of patients , regardless of their aspect and extent [ 33 ]  . to better understand the relevance of ip and pmp our group analysed a large number of patients with pmp . 
out of 47 patients with pmp , 91.5 % had a surgically proven necrosis along the gastrointestinal tract , the majority had arterial infarcts , perhaps because of fluid congestion preventing air penetration into the bowel wall and mesenteric vessels . 
among these patients , there was a high mortality rate ( 68.1 % ) , which rose to 79.5 % if only subjects with infarct were considered [ 22 ]  . in a subsequent study we examined 102 patients with ip . 
most of these papers were case reports so that the unusual findings were magnified compared to the more common conditions . in 1997 , faberman and mayo - smith [ 37 ] analysed a series of 17 patients with portal venous gas detected by ct and they found an unexpected low mortality in these patients , passing from a previously reported overall mortality of 75 % and of 85 % in non - iatrogenic cases to 29 % . 
 the authors noted that ct has a greater capacity to recognise portal gas compared to plain radiographs ; however , they also note the lack of correlation between mortality and the amount of portal gas . 
gas in mesenteric vein ( portomesenteric pneumatosis , pmp ) ( white arrowhead ) 1 3 radiol med ( 2015 ) 120 : 96104 underlying ip , mainly , but not exclusively , arterial infarcts . 
ip was associated with death in 30.4 % of patients , a linear pattern was present in 79.2 % of infarcted patients who died , and in advanced cases there was a larger amount of air contributing to ip and pmp . 
the mortality rate was 50 % when ip was associated with pmp ; this rate rose to 72.2 % if only infarcted patients with ip and pmp were considered [ 21 ]  . 
pneumoperitoneum with peritoneal fluid and air - fluid level ( white arrowhead ) , pneumoretroperitoneum ( black arrow ) , portal pneumatosis ( white arrow on the right ) , gas in the spleen ( white arrow on the left ) , gastric pneumatosis ( black arrowhead ) ; mesenteric vein gas is also present fig . 
16 careful use of window settings allows for clear distinction between intestinal pneumatosis ( white arrow ) and parietal wall lipomatosis ( white arrowhead ) in a patient with long - standing steroid treatment for crohns disease cases . 
their role has been strongly questioned but , although it is well recognised that they can be observed in a large variety of conditions with very different prognoses , their association with intestinal ischaemia is well documented , and in some studies a high mortality rate has been observed , especially when a linear pattern of ip was found and when ip was associated with pmp . recognition of ip and pmp in the appropriate clinical setting should raise a suspicion of mesenteric infarct and prompt a careful search for other signs of intestinal 1 3 radiol med ( 2015 ) 120 : 96104 fig . 
note the associated portal branch ( black arrowhead ) involvement so as not to miss cases of intestinal infarct or allow them further evolve into wide necrosis , with worsen prognosis . conflict of interest the authors declare no conflict of interest . radiol med ( 2015 ) 120 : 406 doi 10.1007 / s11547 - 014 - 0450 - 8 erratum erratum to : carm conebeam computed tomography in interventional oncology : technical aspects and clinical applications chiara floridi alessandro radaelli nadine abijaoudeh michael grass mingde lin melanie chiaradia jeanfrancois geschwind hicham kobeiter ettore squillaci geert maleux andrea giovagnoni luca brunese bradford wood gianpaolo carrafiello antonio rotondo published online : 7 august 2014 italian society of medical radiology 2014 erratum to : radiol med doi 10.1007 / s1154701404295 the affiliations of a . 
the correct affiliations are : in the original version of the article unfortunately some authors names and affiliations were wrongly reported . the authors names micheal grass , ming de lin , hishman kobeiter are misspelled . the correct names are michael grass , mingde lin , hicham kobeiter a . 
the aim of our study was to provide anatomical boundaries for the identification and delineation of the following critical organs at risk in the head and neck district : brachial plexus , cochlea , pharyngeal constrictor muscles and optic chiasm . patients and methods one patient was initially selected to elaborate our atlas . 
this patient was subjected to a planning computed tomography of the brain and head and neck district ; axial images of 3 - mm thickness at 3 - mm intervals were obtained . 
the obtained images were fused based on anatomical landmarks and used by a radiation oncologist , supported by a neuroradiologist , to provide anatomo - radiological limits for the identification d . 
the objective of radiation therapy ( rt ) is to concentrate the highest dose to the target achieving the highest probability of cure with the lowest toxicity on healthy tissue . 
in this regard , high - precision 3d conformal radiotherapy ( 3d - crt ) and intensity - modulated radiotherapy ( imrt ) are currently used to optimally cover the tumoural target and to maximally avoid normal tissues [ 2 ]  . 
however , using these techniques higher doses can be 1 3 radiol med ( 2015 ) 120 : 352360 released to the tumour , with increased potential damage to organs at risk ( oars )  . 
moreover , radiation oncologists are expected to have considerable knowledge of the computed tomographic ( ct ) and magnetic resonance ( mr ) imaging anatomy of this region to accurately characterise tumour extent and to define the oars of potential radiation injury [ 3 ]  . 
recently , several authors have performed studies to define oars , such as the brachial plexus and pharyngeal constrictor muscles ; the effect of oar delineations on the dosimetric parameters can be critical and can influence treatment planning and outcomes in both clinical trials and daily practice [ 37 ]  . contouring guidelines are the main prerequisite for standardising oar delineation , in order to exactly understand dose volume histogram ( dvh ) parameters and in order to adequately analyse and predict toxicity of radiation treatment [ 7 ]  . the aim of our study was to present our institutional ctbased guidelines for the identification and contouring of the following critical oars in the h&n district : brachial plexus , cochlea , pharyngeal constrictor muscles and optic chiasm . materials and methods anatomy textbooks and radiology atlases were reviewed for descriptions of the brachial plexus , cochlea , pharyngeal constrictor muscles and optic chiasm [ 8 , 9 ]  . 
 the h&n district is a fairly rigid site , without conspicuous anatomical differences between male and female sex and where a rigid set - up contributes to reduce organ variability . 
a field of view ( fov ) adapted to the patient and sized to include the patient contour , a 512 - square matrix , and a standard reconstruction algorithm were used . 
the mr scan was performed on philips achieva 1.5 tesla scanner using a 512 - square matrix , turbo spin echo ( tse ) t2 - weighted sequences in the axial and coronal scan planes with and without fat suppression and 3d fast field echo ( ffe ) t1 - weighted sequences with fat saturation before and after intravenous gadolinium ( 0.2 mmol / kg ) administration ; the scan length for the coronal and axial sections was 260 and 210 mm , respectively . 
two neuroradiologists , having more than 10 years of experience , supported the radiation oncologist in identifying the brachial plexus , cochlea , pharyngeal constrictor muscles and optic chiasm and the other adjacent structures . 
to validate the identified anatomical landmarks , the oars were also contoured by the radiation oncologist and the neuroradiologists on three consecutive patients ( two male , one female ) , who were subjected to the same ct and mr imaging study . 
the boundaries of the atlas were indicated by the neuroradiologists to the radiation oncologists and constituted part of a work leading to create a textbook for delineation of oars in radiation therapy [ 13 ]  . brachial plexus the brachial plexus is a large network of nerves , which innervate the upper limbs . 
nerve roots of the plexus arise from c5 through t1 and they pass through t1 , vertebral body interspaces c4 5 , c5 2 , respectively , joining in the neck to form and t1 trunks ( c5 middle trunk , inferior trunk )  . 
1 three representative axial images of the brachial plexus : the most cranial ( a ) , an intermediate image ( b ) and the most caudal ( c )  . 
 [ 13 ] anterior and middle scalene muscles into the neck and clavicular fossa ; then , they merge to form cords , which pass over the first rib ( marking the entry point of the brachial plexus into the axilla ) and continue under the clavicle posteriorly to the subclavian artery [ 3 ]  . 
 t1 neural along the course of the brachial plexus , c4 t1 vertebral pedicles represent its medial foramina or c4 limits ; lateral boundaries are the sternocleidomastoid muscle in the upper portion of neck and the subclavian and axillary neurovascular bundle in the inferior part of neck , where the nerves run along the clavicular fossa . 
the anatomical boundaries were delineated as follows : the cranial limit is represented by the petrous apex of the temporal pyramid ; the caudal limit is represented by the carotid canal ; the medial limit is defined by the temporal pyramid ; the lateral limit is represented by the medial wall of the tympanic cavity ; the anterior limit is represented by the anterior and superior surface of the petrous bone ; the posterior limit is represented by the anterior aspect of the internal auditory canal ( iac )  . 
3 three representative axial images of the constrictor muscles of the pharynx : the most cranial ( a ) , an intermediate image ( b ) and the most caudal ( c )  . 
 [ 13 ] pharyngeal constrictor muscles the pharyngeal constrictor muscles are three circular muscles which constrict the pharynx ; they are distinguished into the superior pharyngeal constrictor ( sc ) , middle pharyngeal constrictor ( mc ) and inferior pharyngeal constrictor ( ic )  . 
from superior to inferior , the delineation of sc starts at occipital condyle and ends at the superior edge of the hyoid bone , which represents the inferior limit ; on the lateral side , it is contained within the parapharyngeal space , which represents lateral limit with the palatine tonsil as well . 
at that point , the optic chiasm forms an x shape , which is located just superior to the sella turcica , with the nerves crossing anteriorly to the pituitary stalk . 
we define the upper limit of optic chiasm located 0.5 cm above the anterior clinoid processes ; the lower limit includes the cavum sellae ; anteriorly it corresponds to a line passing through the anterior clinoid processes ; posteriorly , it is delineated along the mesencephalon ( anterior aspect of the cerebral peduncle ) with the posterior clinoid which has to be included ; the lateral limit is defined as the medial sur face of the uncus hyppocampi and as the temporal horn of 1 3 radiol med ( 2015 ) 120 : 352360 fig . 
inaccuracies in clinical volume contouring impair the precision of radiotherapy planning and could be a major source of uncertainties in clinical outcome and toxicities . contouring atlases represent a good reference tool for accurate delineation of oars in radiotherapy planning , especially in the h&n district ; the complex geometry of this area makes it difficult to encompass the target volume with sufficient dose of radiation , simultaneously sparing the surrounding normal tissues . 
even though new techniques ( imrt , volumetric techniques , stereotactic radiotherapy ) improve therapeutic index , an accurate oar delineation in the h&n district is required to spare these critical structures [ 2 ]  . 
nevertheless , slight discrepancies in both geometry and volume may lead to potential underor overestimation of the dose received by these oars [ 17 ]  . our interdisciplinary study provides anatomical boundaries to identify and contour the brachial plexus , cochlea , pharyngeal constrictor muscles and optic chiasm on treatment planning ct . 
recently , nelms et al . , quantifying variation in the contouring of oars in an oropharyngeal cancer clinical test case , observed that contour variances affect mean and maximum dose per oar . 
they concluded that variation in h&n oar contouring , even if sophisticated rt modalities were applied , can play an important role on the final treatment plan with an increased risk of misadministration [ 18 ]  . the impact of oar contouring on dosimetric calculations of the treatment planning system ( tps ) was not evaluated in our study ; nevertheless we examined a large number of oars in the h&n district whereas most studies focused on single oar descriptions . several studies about brachial plexus contouring have been reported [ 35 , 17 ]  . 
they showed that brachial plexus variation in geometry and in volume contour can affect optimisation of radiotherapy treatment plans and they observed that the brachial plexus routinely receives doses in excess [ 4 ]  . 
this study concludes that , although the rtog atlas is an important tool , delineation of the brachial plexus remains critical and burdened by considerable variability [ 17 ]  . 
in our 1 3 358 radiol med ( 2015 ) 120 : 352360 contouring atlas , muscles , bones and vessels were provided as landmarks to identify the brachial plexus course along the neck towards the axilla on a planning ct , where this organ is not detectable . delineation of the brachial plexus can vary depending on set - up position for radiotherapy planning . 
generally h&n cancers are irradiated with the patient holding the arms along the trunk ; when treating breast cancers or other thoracic tumours the arms could be positioned over the head . 
 some atlases are available for both h&n cancer and thoracic cancer so as to standardise the delineation of the brachial plexus in these different conditions [ 4 , 5 ]  . 
however , to date , endorsed recommendations for brachial plexus contouring in thoracic radiotherapy are lacking ; consequently the tolerance dose for this oar is still largely debated [ 5 ]  . the cochlea is a critical structure for brain and h&n radiotherapy treatment . 
a dosevolume analysis is not feasible for this oar due to its small volume and to limitations associated with its contouring , but an accurate delineation of cochlea seems crucial to improve definition of dose - effect relationships . 
several studies have attempted to relate mean or median cochlear dose to sensorineural hearing loss ( snhl ) , which is a common otological toxicity after radiotherapy , while , to our knowledge , few studies investigated the delineation of this structure [ 14 , 1922 ]  . 
in addition , due to its complex anatomy and dimension , the cochlea seems particularly difficult to contour even for expert radiation oncologists [ 23 ]  . based on this limited evidence , guidelines and endorsed recommendations for correct contouring ( in terms of location , bone window , level and image thickness ) are needed and our interdisciplinary work could represent a pioneering study in this particular regard . institutional ct - based guidelines for the delineation of oars involved in radiation - induced swallowing dysfunctions ( swoars ) have been proposed by christianen et al . , because differences in delineation of pharyngeal constrictor muscles can influence the dose - effect relationships [ 7 , 24 ]  . 
 in this study the definitions of the swoars were described by a panel of experts , including two experienced h&n radiation oncologists and an specialised h&n radiologist ; in particular , the swoars were delineated by one radiation oncologist and reviewed by the other experts , on a contrast - enhanced planning ct scan from an edentate female patient with a t2n0 nasal cavity tumour . 
the guidelines as presented in this paper are ct - based , although the authors noted that the visualisation of relevant anatomical swallowing structures could be improved by using mr imaging and that the use of co - registered mr in conjunction with ct may improve and facilitate the delineation of the swoars [ 7 ]  . 
 these studies showed that late dysphagia following treatment for h&n cancers is considerably associated with the dose to the pharyngeal constrictors , particularly the sc , but the exact relationship between radiation doses to the constrictors and post - radiation dysphagia is still unclear , and it is difficult to separate out the individual role of chemotherapy and rt in these swallowing disorders [ 2527 , 30 , 31 , 33 ]  . the optic chiasm represents another relevant structure involved in treatment of central nervous system and h&n tumours . 
visual damage from radiation - induced optic neuropathy ( rion ) is disabling but uncommon , and it consists in a painless rapid visual loss , whose pathogenesis is related to vascular injury and it could result in bilateral vision loss [ 15 , 3538 ]  . 
 the obtained results were satisfactory for all the parameters evaluated , such as position or volume , for the larger organs ( eyes , brain stem and cerebellum ) , while for the optic chiasm the contour positioning obtained with automatic segmentation was satisfactory but the volume was largely underestimated . 
in our experience the ct - based atlas could assist the radiation oncologist to identify the boundaries limiting in each direction this critical oar on planning ct images . our study attempted to answer to critical issues characterising each of the considered organs . 
therefore , we produced an institutional ct image - based atlas to be used easily in daily clinical practice in order to improve interobserver homogeneity in contouring and reliably establish 1 3 radiol med ( 2015 ) 120 : 352360 dosevolume relationships . 
however , an evaluation of inter - observer variability with and without the atlas is expected . conclusion differences in delineation of clinical volumes particularly for the oars can be critical and can influence treatment planning , clinical outcomes and the evaluation of clinical trial results . 
a uniform guideline to contour the oars should generate more reproducible data both from clinical trials and from clinical practice ; this could be useful for more accurate future analyses [ 5 ]  . 
our ct - based atlas model seems to provide accurate definitions of anatomical boundaries of the brachial plexus , cochlea , pharyngeal constrictor muscles and optic chiasmoreover , this multidisciplinary experience led to the production of an institutional reference tool that could represent a useful aid for radiation oncologists when performing brain or h&n treatment planning in clinical practice and a further tool to facilitate learning of contouring procedures . 
during the treatment , the distal tip of the ventilation catheter was placed across the stenosis into one of the main bronchi and the proximal tip of the catheter was linked to the oxygen tube for oxygen supplementation . 
data on technical success , clinical outcome and follow - up were collected and analysed . results ventilation stenting under local anaesthesia was technically successful and well tolerated in all patients . 
 however , if airway stenting or interventional bronchoscopy is performed directly under local anaesthesia , the procedure is usually poorly tolerated , and patients may experience asphyxia because the stent introducer sheath or bronchoscope can aggravate hypoxia . 
 the tumour stage of all patients was evaluated by the criteria of the american joint committee on cancer / international union against cancer ( ajcc / uicc ) [ 6 ]  . ventilation catheter the ventilation catheter was a 4f angiographic catheter , and the angle of the catheter tip was 135 , which complied with the angle between the trachea and main bronchus . airway stents all stents were uncovered self - expanding nickel - titanium alloy stents ( micro - tech , nanjing , china ) and chosen on the basis of the results of the preoperative evaluation . 
for the y - shaped stents , the diameter and length of the body ( tracheal stent ) varied from 18 to 20 mm and from 30 to 40 mm , respectively ; the diameter and length of the two bronchial limbs varied from 11 to 12 mm and 15 to 30 mm , respectively . placement of the ventilation catheters all procedures were performed by three interventional radiologists under fluoroscopic guidance , while the patients breathed autonomously . 
the patients blood pressure , heart rate , sao2 , and rr were monitored throughout the 1 3 340 radiol med ( 2015 ) 120 : 338344 cover the stenosis . 
the entire stent within the introducer sheath was advanced further so that the two bronchial stents passed over the two guide wires into two main bronchi , and the two bronchial stents were deployed by retracting their retaining threads , after which the tracheal stent was deployed by withdrawing the introducer . 
 in addition , aerosol was administered once a day for 3 days after treatment to dilute sputum and alleviate chest pa the effect of the stent placement was evaluated according to the improvements of the hughjones ( hj ) classification grade [ 3 ] , sao2 , and rr after stenting . technical success was defined as exact placement of the stents without any major procedure - related complications . 
 the major and minor complications were defined according to the society of interventional radiology guidelines [ 7 ]  . the patients underwent thoracic ct or bronchoscopy 714 days , 1 month , and every 23 months after treatment to evaluate the long - term efficacy of the stents and the stentrelated complications . 
the follow - up ended at the point of patients death . statistical analysis statistical analysis was performed using the paired samples t test ( spss version 16.0 , chicago , il , usa )  . 
a p value of less than 0.05 was considered statistically significant . results assessment of the procedure ventilation stenting under local anaesthesia was technically successful and well catheter - assisted airway fig . 
the ventilation catheter was inserted into the trachea via a 0.035 - inch guide wire ( terumo , tokyo , japan ) from the nasal cavity , and then airway mucosal anaesthesia was performed by sprinkling 5 ml of 2 % lidocaine via this catheter . 
 another 4f angiographic catheter and the 0.035 - inch guide wire were inserted through the mouth across the stenosis into one of the main bronchi , and then the 0.035 - inch guide wire was exchanged for a 0.035 - inch stiff guide wire ( terumo , tokyo , japan )  . 
the 14f stent introducer sheath was passed over the guide wire into the trachea , and the stent was positioned in the trachea with a pusher catheter to 1 3 341 radiol med ( 2015 ) 120 : 338344 fig . 
to improve patient safety , we should both establish an effective oxygen supplementation model and eliminate influences on the oxygen supply during the procedure . in this study , the tip of the ventilation catheter was sent across the stenosis into the main bronchus to permit oxygen to be delivered directly to the alveolus to promote oxygenation . 
meanwhile , the patients autonomous respiration persisted throughout oxygen supplementation , and expiration was performed by their autonomous respiration . moreover , the oxygen supplementation was not altered during the procedure of airway stenting because oxygen supplementation and airway stenting were performed via separate paths . 
in addition , the patients rr and tolerance to the procedure were improved in conjunction with the improvement of hypoxia , and the improvement in tolerance helped to improve the accuracy of stent insertion . in this study , the stents were released over the ventilation catheter to ensure that oxygen supplementation could be maintained throughout the procedure . 
because of the extremely small diameter of the catheter and the flexibility of the airway wall , the space could be sealed rapidly upon self - expansion of the stent . the subcarinal position of the ventilation catheter may increase the risk of barotrauma because the dead space will be reduced and the alveolar volume will be enlarged [ 810 ]  . 
this risk can be minimised by reducing the oxygen flow because it can reduce the ventilation capacity and 1 3 344 radiol med ( 2015 ) 120 : 338344 the resistance to expiration [ 810 ]  . 
it was found that the patients inoperative sao2 could be maintained above 90 % under 23 l / min oxygen flow over a treatment time of 824 min and a ventilation time of 520 min . recently , both covered and uncovered self - expanding nickeltitanium alloy stents have been used to treat malignant airway stenosis [ 11 ]  . 
 in addition , stent migration usually occurred several days to 2 weeks after stent insertion , whereas tumour ingrowth usually occurred 240 months after stent insertion [ 2 , 12 ]  . 
based on the characteristics of the stents and our patients , uncovered stents were chosen for our patients to reduce sputum retention and migration rates . this study had some limitations . 
 based on the microhistological examination , the patients were divided into three groups [ rs without hyperplasicproliferative lesions ( hpl ) ; rs with hpl ; rs with cancer ] and we assessed the risk of cancer associated with rs in the first and second group . 
castellano dipartimento di scienze biomediche ed oncologia umana , azienda ospedaliera citt della salute e della scienza di torino presidio molinette , universit di torino , via santena , 7 , 10126 turin , italy l . 
bergamasco dipartimento di scienze chirurgiche , azienda ospedaliera citt della salute e della scienza di torino presidio molinette , universit` di torino , corso bramante 88 , 10126 turin , italy results based on the microhistological examination , 51 / 80 patients were included in the first group ( 9 of them not subjected to surgery ) , 25 / 80 in the second group and 4 / 80 in the third one . 
at the final histological examination , there were 7 / 42 ( 16.7 % ) cancers in the first group and 8 / 25 ( 32 % ) in the second group . 
tomosynthesis was useful to detect parenchymal distortions . keywords breast neoplasms radial scar mammography breast tomosynthesis introduction the radial scars ( rs ) are benign proliferative breast lesions associated with breast cancer in a percentage between 7 and 31 % of cases [ 17 ]  . 
mammographically , rs is characterized by an area of architectural distortion and according to the criteria of tabar and dean it is indicated by : ( 1 ) the presence of a central radiolucency ; ( 2 ) the presence of radiating , long thin spicules ; ( 3 ) different appearance across different projections ; ( 4 ) radiolucent linear structures parallel to the spicules ; and ( 5 ) the absence of palpable lesions or skin changes [ 8 ]  . rs lesions are also visible during ultrasound examination , where they appear as hypoechoic areas [ 9 ]  . histologically , rs is characterized by a central core that entraps small fibro - elastic tubules within a double 1 3 378 radiol med ( 2015 ) 120 : 377385 epithelial and myoepithelial layer , in addition to the radiating ducts and lobules associated with various degrees of epithelial hyperplasia , ductal ectasia , adenosis and papillomatosis . 
 several authors have occasionally used the definition of complex sclerosing lesions to describe lesions composed of multiple fibroelastotic areas situated adjacent to or a centimeter above them [ 10 ]  . 
rs is frequently associated with hyperplasic - proliferative lesions ( hpl ) , such as the typical ductal hyperplasia ( din1a ) , the atypical ductal hyperplasia ( din1b ) , the atypical lobular hyperplasia ( lin1 ) , and in situ classic lobular neoplasia ( lin2 ) , according to the who ( 2003 ) , or with papillary lesions , in situ carcinoma , or invasive carcinoma . generally , malignant lesions associated to rs lesions are low - grade ductal carcinomas in situ ( dcis ) and tend to have favorable prognoses [ 1113 ]  . 
according to previous studies , the risk of malignant disease occurring in association with rs is greater in patients older than 50 years old [ 14 , 15 ] , it depends on the size of the rs , and it seems to increase with the tumor diameters > 1 cm [ 16 ]  . this study aimed to assess the risk of breast cancer associated with microhistological diagnosis of rs . 
the analysis considered the following : the presence of hpl at the microhistological examination following a core biopsy , the association between age , presence or absence of cancer or hpl at the pathological examination following surgical excision , the percutaneous biopsy method used and the lesion classification according to the bi - rads lexicon [ 17 ]  . finally , we compared the performance of analog and digital mammography and digital breast tomosynthesis in the diagnosis of rs and with regard to mammographically visible lesions . materials and methods between march 2002 and november 2011 , 6 , 713 breast core biopsies were performed in the breast imaging serviceradiologydepartment of diagnostic imaging and radiotherapy , university hospital san giovanni battista of tureighty lesions were confirmed as being rs using microhistology and retrospectively re - evaluated . radial scar lesions with associated malignancies , diagnosed using needle core biopsy ( ncb ) , were excluded from the study . for all rs lesions identified during microhistological examination , surgical excision was indicated during multidisciplinary meetings of the institutional breast unit . 
9 / 80 patients chose to not undergo surgery , and imaging followup was performed . out of the 71 patients who underwent surgery , 52 / 71 ( 73 % ) underwent 14 - g tru - cut ncb : 20 / 71 ( 28 % ) by ultrasound ( us ) guidance and 32 / 71 ( 45 % ) by stereotactic ( stx ) guidance . 
the remaining 19 patients ( 27 % ) underwent vacuum - assisted breast biopsy ( vab ) , using 11 g mammotome device ( ethicon endo - surgery , cincinnati , oh , usa ) by stx guidance with fischer digital prone table . 
the needle size and number of specimens obtained were recorded . we evaluated the correlation between the findings of the microhistological and pathological examinations , according to the type of device used for the percutaneous biopsy and the imaging used for guidance purposes ( ultrasound or stereotactic )  . the patients were divided into three groups according to the results of the percutaneous biopsy : 1 . 
ultrasound examination was performed in all patients ( esaote technos mpx , logos hitachi hivision or esaote my lab twice ) using a 10to 18 - mhz probe . for patients undergoing digital mammography in combination with tomosynthesis , the contribution of the 3d mammography to the identification of rs was also assessed . 1 3 radiol med ( 2015 ) 120 : 377385 table 1 features of rs associated with cancer identified at percutaneous biopsy mammographic features size ( mm ) bi - rads sonographic features needle size ( g ) guidance no . 
of samples pathological examination architectural distortion architectural distortion calcifications calcifications no ultrasound abnormality hypoechoic mass no ultrasound abnormality no ultrasound abnormality dcis low grade dcis low grade dcis low grade stx stereotactic , us ultrasound , dcis ductal carcinoma in situ , idc invasive ductal carcinoma statistical analysis sd , and continuous variables were reported as mean were assessed by anova . 
a value of p < 0.05 was taken to indicate statistical significance . results radial scar lesions represent 1.2 % ( 80 / 6 , 713 cases ) of the breast lesions subjected to core biopsy in our center . concerning the microhistological examination , 51 / 80 ( 64 % ) patients were included in the first group ( rs not associated with hpl , of which only 42 patients underwent surgical excision ) ; 25 / 80 ( 31 % ) were included in the second group ( rs associated with hpl ) and 4 / 80 ( 5 % ) in the third group ( rs associated with cancer )  . out of the 71 patients who underwent surgical excision , 19 ( 26.7 % ) received a definitive histologic diagnosis of tumors associated with rs ; analyzing the results of the pathological examination , 7 / 42 ( 16.7 % ) belonged to the first group and 8 / 25 ( 32 % ) to the second group . 
we observed only one case with lymph node metastases ( 2 / 18 lymph nodes involved )  . the nine patients in the first group who chose not to undergo surgery ( mean age 59 7.7 years ) were subjected to clinical and imaging follow - up ( mean followup 49 months ) , whose results have been negative so far . 
regarding the results of the 51.88 the second group ; and 61.5 the third group contained a significantly greater number of older patients ( p definitive histological examination , patients were classi19 ) ; rs fied as follows : rs associated with cancer ( n 18 ) ; and rs not associated with associated with hpl ( n 34 )  . 
the mean number of core samples collected in the 15 patients with a failed diagnosis at percutaneous biopsy of tumor associated with rs was 4 ( range 212 )  . 
two of these four in terms of the degree of underestimation of vab compared to the ncb , vab appears to be associated with 1 3 radiol med ( 2015 ) 120 : 377385 fig . 
1 on mammographic standard projections ( a , b ) , in the outer - upper quadrant of the left breast , we can observe a parenchymal distortion of 4.5 cm ( birads r5 )  . 
a stereotactic core biopsy ( 14 g ) was performed : the microhistological diagnosis was rs with atypical ductal hyperplasia ( din1 b ) , histologically confirmed greater diagnostic accuracy ; however , it should be taken into consideration the low power of the statistical test used ( table 2 )  . using the stx guidance , we observed 12 cases of underestimation out of 51 cases ( 5 rs cases not associated with hpl at the microhistological examination were associated with tumors at the pathological examination ; 3 rs cases associated with hpl were associated with tumors and 4 rs cases not associated with hpl were associated with hpl )  . underestimation occurred in 7 out of 20 cases using ncb with us guidance ( 2 rs cases not associated with hpl at the microhistological examination were associated with tumors at the pathological examination and 5 rs with hpl were associated with tumors )  . the rates of underestimation using the stx guidance vs . 
sixteen of 71 cases ( 27 % ) were classified as bi - rads 3 ( all microcalcifications ) ; all these lesions , based on medical history ( family history or past use of hormone therapy ) , or according to the wishes of the patient , underwent biopsy . 
between may 2008 and october 2009 6 / 80 lesions ( 7 % ) were detected using digital mammography ; between october 2009 and november 2011 , 12 / 80 ( 15 % ) were detected using 2d digital mammography , and 24 / 80 ( 30 % ) were detected using 2d digital mammography with tomosynthesis . 
two - dimensional digital mammography alone detected 18 / 24 lesions [ ( 75 % ) ; 95 % ci 54.888.3 % ] ( 6 / 18 lesions were detected by mammography alone in a single projection )  . 
the present study reported a rate of upgrade to cancer of 22.3 % ( 15 of 67 cases ) , of which 7 cases belonged to the rs without hpl group , and 8 to the rs associated with hpl group . 
 [ 21 ] reported that surgery could be avoided when hpl is absent and the biopsy is performed using more than 12 samples , and mammographic findings are reconciled with histologic findings . 
 [ 23 ] reported an association between rs and tumor in 8.3 % of cases without hpl using ncb with an 18 - g tru - cut needle . the majority of patients ( 52 of 71 ) were subjected to core biopsy using a 14 - g needle , across an average of three specimens ( range 25 )  . 
although the difference was not statistically significant , the average size of lesions subjected to ultrasound or stereotactic biopsy was greater compared to the size of lesions subjected to vab . 
the degree of underestimation could , therefore , depend on sampling error due both to the small number of specimens taken ( > 5 specimens is recommended , if rs is suspected ) and the size of the lesion [ 7 , 24 ]  . we also found that more accurate preoperative diagnoses could be made using stereotactic guidance , which appears to 1 3 radiol med ( 2015 ) 120 : 377385 fig . 
2 conventional 2d mammographic projections ( a , b ) and tomo synthesis 3d images ( c , d ) : we can observe in tomosynthesis images in the inner - upper quadrant of the left breast a parenchymal distortion with radiopaque core of 7 mm , which was an hypoechoic inho mogeneous mass at us ( e )  . 
this may be due to an increased likelihood that the core of the lesion is sampled , but also to the sampling of the spicules , where atypical hyperplasia or carcinoma is present most frequently [ 25 , 26 ]  . the preoperative diagnosis carried out on material taken by the vab system has proven to be more accurate ; the good agreement obtained in the final histological examination seems to deal with the greater caliber of the needle ( 11 g ) , which allows to sample a greater amount of tissue making the study of its histological features more straightforward . 
it should be highlighted that the majority of tumors associated with rs are likely to be low - grade dcis or invasive carcinomas with favorable prognostic factors ( positive estrogen and progesterone receptors with low proliferative index ) [ 19 , 27 , 28 ]  . 
 the low aggressiveness of these lesions accounts for the good prognoses of the patients [ 11 , 28 , 29 ]  . the age of patients at diagnosis appears to influence the risk of developing cancer associated with rs ; many authors agree that breast cancer is rare in rs patients below 50 years old [ 14 , 30 , 31 ]  . 
our study demonstrates a predominance 1 3 384 radiol med ( 2015 ) 120 : 377385 of tumors in older females , not only with ncb of carcinomas associated with rs but also with a definitive histologic diagnosis of rs associated with cancer . 
therefore , at more advanced ages the presence of hpl could be an indicator of early - stage neoplastic transformation [ 25 , 27 , 32 , 33 ]  . radiologic appearance of rs is not clearly distinguishable from cancers [ 1 , 4 , 6 , 15 ]  . the majority ( 72 % ; 51 / 71 ) of the lesions were classified as bi - rads 4 ( suspicious , possibly malignant ) , due to the lack of recognizable radiological features . 
reconstructed images allow for superior visualization of the thin , spicule - like characteristics of rs lesions , and for the identification of the predominantly radiolucent core , resulting in more accurate localization of the lesion , which is often not possible in 2d ( especially in cases where the rs is evident in a single projection )  . 
therefore , tomosynthesis could represent a useful , multi - modal diagnostic tool for this type of lesion . despite the increased rate of rs detection , there has been no concomitant increase in the number of associated cancers . 
 using a multiple regression model , tibiofemoral cartilage loss was found to correlate independently with mme conclusions medial meniscal extrusion , evaluated with an open - configuration , rotating mr scanner , increased from the clinostatic to the orthostatic position . 
in a recent study on a large cohort of 1 , 527 patients with ( or at risk for ) knee oa , meniscal extrusion in the medial tibiofemoral ( tf ) compartment significantly correlated with meniscal tears , varus malalignment , and cartilage damage [ 3 ]  . 
in other studies , meniscal extrusion was shown to be an independent predictor of tf cartilage loss [ 2 ] and degenerative subchondral bone marrow lesions [ 4 ]  . 
tearing of the meniscus is related to meniscal extrusion , reduces the weight - bearing capacities of the tf compartment , leads to 1 3 330 radiol med ( 2015 ) 120 : 329337 damage in the articular cartilage and subchondral bone , and contributes to the progression of knee oa and the related mechanical impairment [ 57 ]  . 
conventional , weight - bearing knee radiographs obtained with specific x - ray projections dedicated to accurately demonstrate the tf joint space ( e.g. , lyon - schuss view [ 8 ] ) , are the most widespread and standardised imaging modality to examine patients with suspected or known oa . 
to the best of our knowledge , only one study has focused on mr examination of the knee joint in patients with oa in loading / weight - bearing conditions . 
employed a 3t mr scanner equipped with an axial loading device [ 12 ] , which was used to generate a load of about 50 % of the patients body weight in the knee joint , intended to mimic static standing conditions . 
the main limitation of this device is that , during the examination , the patient is lying supine on the mr table , and the weight - bearing condition is only simulated . 
in contrast , we employed a peculiar low - field ( 0.25 t ) , rotating permanent - magnet mr system which allows patients to be examined while lying supine or while standing in a true weight - bearing position . 
the present study had two main objectives : the first was to assess the influence of weight - bearing on different oa features of the medial tf compartment [ including medial meniscal extrusion ( mme ) ] ; the second was to study possible correlations between mme and compartmental cartilage loss , subchondral bone marrow oedema , subarticular cysts / geodes , bone attrition , marginal osteophytes , and meniscal damage . materials and methods in this pilot study , 26 patients [ 18 ( 69.2 % ) women and eight ( 30.8 % ) men ; mean age , 67 9.7 years , range 5281 years ] with medial tf knee oa were prospectively enrolled in the rheumatology outpatient clinic . 
knee oa was diagnosed on the basis of clinical and radiographic findings according to the american college of rheumatology ( acr ) criteria [ 13 ] ( i.e. , pain in the knee and five of the following : patients age over 50 years , less than 30 min of morning stiffness , crepitus on active motion , bony tenderness , bony enlargement , no palpable warmth of synovia )  . 
after written informed consent was obtained , the study knee was examined with a low - field rotating clino - orthostatic mr scanner ( g - scan , esaote biomedica , genoa , italy ) in both supine and true weight - bearing position using a dedicated sequence protocol . 
two different sets of sequences were applied for the clinoand orthostatic position ( table 1 )  . in order to avoid vasovagal attacks , which were reported in 14.3 % of patients from a previous study where the same rotating mr - scanner was used [ 15 ] , we decided to perform the orthostatic examination before the clinostatic one and to reach a maximum vertical tilt of the table of 82 . 
in addition , the orthostatic part of the mr examination was intentionally shorter than clinostatic imaging ( three versus five sequences , respectively ) 1 3 332 radiol med ( 2015 ) 120 : 329337 fig . 
3 in order to help the patient stand comfortably during the weight - bearing part of the magnetic resonance ( mr ) imaging examination , a suitable position can be reached by rotating the permanentmagnet / patient table complex by 82 . 
the explanation is the following : given wt the vector representing the total weight , and the angle of rotation of the mr magnet , for between 80 and 90 the projection of the vector wt approximates to w 82 the weight that the patients knee bears is w sin ( )  . 
the first line ( a ) was drawn in correspondence to the border of the medial tibial plateau , excluding bone spurs ; the second one is parallel to the peripheral margin of the meniscus body . 
the mr examinations were scored considering 14 distinct articular features according to the semi - quantitative worms scoring system : cartilage signal and morphology ( csm ) , subarticular bone marrow abnormality ( ma ) , subarticular bone cysts ( bc ) , subarticular bone attrition ( ba ) , marginal osteophytes ( op ) , medial and lateral meniscal integrity ( mi ) , anterior and posterior cruciate ligament integrity , medial and lateral collateral ligament integrity , synovitis , loose bodies and periarticular cysts / bursae . 
six examined features ( i.e. , csm , ma , bc , ba , op , mi ) are related to the articular surfaces ( tf and patellofemoral joints ) , which were divided into 15 subregions using bony landmarks in mtc ( medial tibia central ) mfp ( medial femur posterior ) the fully extended knee . 
medial tf joint is composed of five articular subcompartments [ mfc ( medial femur cenmta ( medial tral ) tibia anterior ) mtp ( medial tibia posterior ) ] , while the anterior portion of the femoral condyle is considered part of the patellofemoral joint . 
since the original worms 8 - point scale for cartilage scoring was developed for high - field mr devices and magnetic field intensity affects the quality of articular cartilage imaging [ 17 ] , a simplified system proposed by kladny et al . 
this consists of a 5 - point scale where normal cartilage ( grade 0 ) has a continuous layer with no surface irregularities , grade 1 is defined as fibrillations with slight inhomogeneity , grade 2 as a loss < 50 % of cartilage thickness ( the hyaline cartilage in a non weight - bearing area is used as a reference ) , grade 3 as marked surface irregularity extending by more than 50 % of the total thickness , and grade 4 a full - thickness cartilage defect . 
this scoring system was applied to all six cartilage compartments of tf and patellofemoral joints ( lateral and medial patella , lateral and medial femoral condyle , lateral 1 3 radiol med ( 2015 ) 120 : 329337 and medial tibial plateau )  . 
changes in meniscal morphology were assessed separately in six regions ( medial and lateral : anterior horn , body , posterior horn ) using a fourlevel scale ( grade 0 , normal ; grade 1 , intra - substance abnormalities , minor radial tear or parrot - beak tear ; grade 2 , non - displaced tears including horizontal and vertical tears ; grade 3 , displaced tears including displaced flap tears and bucket - handle tears ; grade 4 , complete maceration or destruction )  . 
the presence of meniscal root tears , which is not considered in the original worms system , was also assessed in both menisci and considered equivalent to a grade 3 lesion ( displaced tear )  . 
a meniscal tear was defined as a linear area of abnormal signal intensity ( hyperintense on t2 - weighted images ) reaching the articular surface of the meniscus on at least two consecutive sagittal or coronal sections [ 19 ]  . 
the worms global score ( wgs ) , which includes the sum of the scores obtained for all oa features in all articular subcompartments , was calculated and further used to assess intraand inter - observer reliability . 
in reading session a , six worms parameters ( csm , ma , bc , ba , op , mi ) related to the medial tf joint were scored by both observers also on the orthostatic mr sequences . 
it was measured in a mid - coronal plane , i.e. , the section where the medial tibial spine is seen in its greatest volume , as the distance between the peripheral border of the meniscus and the central margin of the tibial plateau , excluding osteophytes . statistical analysis due to the nature of the study ( pilot study ) no specific sample size calculation was performed . 
six worms parameters ( csm , ma , bc , ba , op , mi ) related to the medial tf joint were assessed by the two readers on the mr sequences performed in both the clinostatic and orthostatic position during reading session a . 
mme was independently measured in millimetres ( mm ) by the two radiologists in both reading sessions ( a and b ) on dedicated workstations by means of a calliper . 
univariate analysis was performed calculating the spearmans rank correlation coefficient between mme ( clinostatic , orthostatic and mme values ) and patients age , bmi , kl score , wgs , and the scores of individual worms parameters in the medial compartment of the knee ( csm , ma , bc , ba , op , mi )  . 
type i error was controlled using the bonferroni adjustment , and the a priori alpha level ( 0.05 ) was divided by the number of correlations ( n 10 ) , thus resulting in a level of significance of 0.005. 
a multiple regression model was used to assess the independent association of each oa parameters to mme , the dependent variable in the model . results kellgrenlawrence score the median kl radiographic score was : 3 ( 95 % ci for the median from 2 to 3 ) , including 5 ( 19.2 % ) patients with a kl score of 1 ; 7 ( 26.9 % ) patients with a kl score of 2 ; 7 ( 26.9 % ) patients with a kl score of 3 ; and 7 ( 26.9 % ) patients with a kl score of 4 . 
all patients with a kl score of 1 had oa symptoms more pronounced in the medial tf compartment . intraand inter - observer agreement of worms scoring system in session a , reader 1 and reader 2 obtained a median wgs of 57.5 ( range 25107 ) and 56.5 ( range 27106 ) , respectively . 
table 3 demonstrates intraand inter - observer reliability , as assessed by the 1.8 mm for the clinostatic position and 5.7 the presence of a significant variation in mme from clinostatic to orthostatic position was assessed by means of the student t test for paired samples , using measurements obtained in the reading session a by both readers . 
the presence of significant cor relations between clinostatic , orthostatic , mme and worms parameters of the medial tf joint was tested on the worms scores obtained by the reader 1 in the session a by calculating the spearman rank correlation coefficient ( table 4 )  . 
under loading conditions there is also a reduction of the width of the medial tf joint space , filled with hyper - intense synovial fluid ( thin arrow ) , as well as an increase in extrusion of the medial meniscus ( mme 2 mm )  . 
compartmental cartilage loss proved to be the only independent predictor of mme . discussion we assessed the cross - sectional association of age , bmi , and several oa features ( kl score , tf cartilage damage , subchondral marrow abnormalities , bone cysts / geodes , bone attrition , osteophytes , meniscal tears , wgs ) with mme ( clinostatic mme , orthostatic mme and mme ) in the same tf compartment . 
in a large population - based cross - sectional study with over than 1 , 500 patients [ 3 ] , clinostatic mme was associated with meniscal tears , varus malalignment , and cartilage damage . 
 in this previous study , meniscal extrusion was semi - qualitatively assessed using a 3 - point scale ( grade 0 , no extrusion ; grade 1 , extrusion 50 % of the body ; grade 2 , extrusion > 50 % of the body )  . 
 from the results of multiple regression analysis , using mme as a dependent variable , tf cartilage loss proved to be the oa feature most significantly correlated with mme ( p 0.0499 ) , a result which is in keeping with those of the multicenter osteoarthritis study group [ 3 ]  . 
 in fact , meniscal tears are not the only factors associated with meniscal extrusion , because other oa features , such as tf cartilage damage and knee malalignment , are independently associated with meniscal extrusion [ 3 ]  . 
to overcome this problem , at least in part , a simplified scoring system for the articular hyaline cartilage based on a 6 - point scale ( from 0 to 5 ) was used . 
on the other hand , the low magnetic field intensity of our rotating mr scanner may have hindered the detection of changes in hyaline cartilage thickness from the unloading to the loading position , which were reported in a previous study by stehling et al . 
in two of them , the dynamic range of motion of normal menisci in asymptomatic volunteers was examined , and both studies were performed in an openconfiguration mr system , which allows mr imaging of the knee in positions other than the neutral clinostatic one [ 22 , 23 ]  . 
they defined as meniscal extrusion a meniscal displacement 3 mm in the mid coronal plane using as reference a line paralleling the medial outermost edge of the articular cartilage of the tibial plateau [ 24 ]  . 
the meniscus is an integral part of the complex biomechanical system of the knee , crucial in sharing the load by increasing the tf contact surface area , and providing uniform distribution of weight bearing across the articular surfaces [ 25 ]  . 
high - grade meniscal degeneration and different types of meniscal tears , in particular those with a radial component , may lead to extrusion [ 26 , 27 ]  . 
extrusion of medial meniscus from the tibial plateau margin may lead to early osteoarthritis due to a decreased tf contact area and an increased contact pressure [ 3 ]  . 
the results of our study confirm the correlation between tearing of the medial meniscus , as defined in the worms , and mme ( p < 0.001 ) , despite cartilage loss was the only independent predictor of mme . 
bone marrow lesions are frequently observed in mr imaging studies of patients with knee oa ; ma consist of a number of heterogeneous histological abnormalities including bone marrow necrosis , trabecular abnormalities , bone marrow fibrosis and oedema [ 28 ] , and have been shown to be strongly associated with knee pain and progression of oa [ 29 , 30 ]  . 
 [ 3 ] who speculate that an increased bmi may modulate the effect of other concomitant risk factors ( e.g. , meniscal tears and cartilage damage ) , but bmi itself has no effect on meniscal position . 
sampling time and the number of frustules collected were considered ; sensitivity , specificity , diagnostic accuracy , positive and negative predictive value ( ppv , npv ) of both procedures were evaluated , considering the final histological examination as reference ( b1 , b3 , b5 lesions underwent surgical excision ; b2 lesion were considered confirmed after a negative follow - up of at least 1 year )  . results there were no statistically significant differ ences between the two groups of patients according to the number of procedures ( s1 82 / 169 ; s2 87 / 169 ) , average age , birads category ( 4a , b ) , and average size of g . 
the systems differed only in sampling time ( s1 80 ; s2 63 s ) , but not in total procedure time . conclusions our study confirms the effectiveness of vabb in the assessment of microcalcifications and highlights the lack of significant differences between the two systems in terms of diagnostic performance . keywords breast cancer vacuum - assisted core biopsy microcalcifications introduction it is widely recognised that the development of systems for minimally invasive needle biopsy ( tru - cut needle biopsy and vacuum - assisted breast biopsy , vabb ) has increased the diagnostic accuracy of percutaneous needle biopsies . 
 in particular , the introduction of vabb systems into clinical practice has allowed researchers to reduce the amount of surgical biopsies performed for diagnostic purposes , so reducing the associated costs [ 1 ]  . 
the major advantage of vabb is the chance to withdraw a number of samples sufficient for an accurate diagnosis with a single insertion of the needle and even , in some cases , to completely remove the lesion . 
vabb also removes a greater amount of material , thus reducing the likelihood of preoperative underestimation , as well as the need to repeat the procedure due to the inadequacy of sampled tissue [ 2 ]  . 
the vabb systems ( gauge 711 ) can be used with stereotactic guidance ( either using upright devices or prone table systems ) , ultrasound or 1 3 370 radiol med ( 2015 ) 120 : 369376 magnetic resonance . 
according to the european guidelines [ 3 , 4 ] they can be considered the method of choice for sampling nonpalpable lesions , such as : groups of microcalcifications with indistinct morphology , for which the removal of a greater volume of tissue for accurate histological evaluation is required ; groups of microcalcifications distributed in small clusters , difficult to sample ( < 5 mm ) ; groups of microcalcifications suspected of malignancy , to increase the chances of detecting invasive foci ; discordant results ( b1 , b3 , or b4 ) after needle biopsy using 14g conventional core biopsy ; architectural distortion ; diagnostic excision of papillary lesions after core biopsy . the effectiveness and accuracy of a vabb system is generally evaluated in the literature by using parameters such as the percentages of underestimation of proliferative risk lesions , classified as b3 ( most frequently atypical ductal hyperplasia ( adh ) versus ductal carcinoma in situ ) and the underestimation of malignant lesions in situ , usually ductal carcinoma in situ ( dcis ) versus infiltrating malignant lesions [ 5 ]  . there are various vabb systems on the market ( suros , vacora , mammotome , encor ) which have in common the use of forced aspiration and the option of using largecalibre needles ( 147g ) [ 6 ]  . the different systems are divided mainly into open or closed , depending on whether the tissue sampling is performed manually or automatically . 
in this study , we compared two vabb devices , one open with manual sampling mammotome ( devicor medical products , inc . , cincinnati , ohio , usa ) and one closed with automated sampling ( encor , senorx , aliso viejo , ca ) to evaluate their diagnostic performances . materials and methods study design between january 2011 and july 2012 , we compared two different vabb systems . 
over this period , 169 consecutive vabb procedures were performed in all cases with the aim of evaluating areas of suspicious mammographic microcalcifications not associated with other signs ( asymmetric densities , structural distortions masses or opacities )  . 
all procedures were performed using a fischer stereotactic prone table ( fischer medical technologies , usa ) with mammotome probes , 11g ( mammotome , devicor medical products , inc . , cincinnati , ohio , usa ) or encor 10g ( encor , senorx , aliso viejo , ca )  . the patients were divided into two groups according to the device used for each procedure . 
in all cases , a complementary ultrasound examination was performed . all vabb procedures were performed after obtaining the informed consent of the patient . biopsy technique a stereotactic digital mammotest fischer prone table was used ( fischer medical technologies , usa ) connected to a computer equipped with mammovision software . 15 and the initial localisation phase is the same for both procedures . 
evaluation of the lesion is made with a radiographic scout view at 0 and then subsequently two stereotactic projections at 15 are run . after selecting the type of biopsy needle system to use and the relative calibre of needle , the software follows stereotactic principles and transmits the numerical values that govern the placement and depth of the needle into the lesion to the device command unit , where the probe is to be installed . local anaesthesia is performed with 1 % lidocaine 15 ( 10 ml ) , followed by two stereotactic projections at and 15 to confirm the correct target . if , after the injection , the target is not correct , it is recentred . 
this procedure is not necessary with the encor probe ( 10 gauge g , with a standard chamber biopsy opening of 19 mm ) , equipped with a tri - concave tip . subsequently two stereotactic pre - fire projections are performed to verify the correct distance between the needle tip and the lesion , and then two post - fire projections to check that the target is at the centre of the biopsy needle chamber . 
the sampling phase comes next , during which the breast tissue is excised by a rotating blade , in conjunction with forced aspiration , and placed in the sample chamber . with the mammotome probe the position of the camera is controlled manually and the samples must be removed individually by the operator ( open system ) and placed on 1 3 radiol med ( 2015 ) 120 : 369376 an appropriate support such as absorbent paper and adequately irrigated with physiological saline solution . the encor is an automatic sampling system with preprogrammed probe , the number and location of the samples are all that is needed before starting . 
this is not available with the mammotome system that we used ( our model of original mammotome st , calibre 11g , came with the opening of the biopsy needle chamber at 20 mm ) , which provides the alternative of a small reducer to place above the biopsy needle chamber before the procedure . 
the needle picks up the encor frustules that are expelled into a separate chamber , from which they are extracted at the end of the sampling ( closed system )  . 
the system is supplied with a cleaning function to cleanse the chamber with saline solution . for both procedures , when used for the characterisation of microcalcifications , mammograms are performed with direct radiological magnification of the cores to assess the presence of microcalcifications in the tissue samples . 
all cores are then placed in a container with 10 % formalin , the samples containing microcalcifications being marked with indian ink . at the end of both procedures it is possible to position a marker consisting of a nonmagnetic metal clip that identifies the site of the needle biopsy . at about 2 weeks after the procedure , all patients underwent mammographic evaluation of the correct positioning of the clip and the possible presence of residual microcalcifications . interpretation of results according to the european guidelines , the microhistological examinations of the samples obtained by vabb were classified into five categories : b1 malignancy , b5 lesion of uncertain significance , b4 malignant [ 8 ]  . benign , suspected normal , b2 table 1 characteristics of the two study groups the lesions classified as benign ( b2 ) were monitored with follow - up mammograms at 612 months . for all lesions classified as b1b3 , diagnostic surgical biopsy after multidisciplinary consultation was advised . 
 the lesions classified as b4 or b5 underwent surgical excision . definitive histological examination was considered the gold standard for the comparison of results and the diagnostic performance of the vabb probes . 
in cases of b4 or b5 lesions completely removed by vabb and no longer histologically present we proceeded to the pathological evaluation of the samples collected by needle biopsy for appropriate cancer treatment . 
for both systems we evaluated the sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) , diagnostic accuracy , sampling time and the number of cores taken . statistical analysis the continuous variables , expressed as averages with standard deviation , were analysed with students t test and the nonparametric mannwhitney test . 
the concordance between the results of the microhistological examination and the definitive histological examination was calculated using cohens coefficient . results the radiological characteristics of the lesions in the two groups of patients divided according to the device used for the vabb procedure ( mammotome or encor ) were comparable ( table 1 ) with no statistically significant differences . the average time taken for the removal of 6 cores was respectively 63 s with probe encor vs . 
in particular , during the check performed 2 weeks after the procedure , we found four blood collections after biopsy with the encor probe and three with the mammotome probe ( for both systems , the collections had ultrasound dimensions between 1 and 2 cm )  . the lesions classified as b2 , with follow - up mammography performed for at least 1 year , were negative in all cases . all vabb with microhistological results classified as b3 received surgical biopsy after multidisciplinary discussion in the course of diagnostic - therapeutic consultations at the breast unit . 
1 magnification views of a 5 - mm cluster of heterogeneous and polymorphous microcalcifications classified as birads 4b , which underwent mammotome vacuum - assisted biopsy in four cases of malignant lesions in situ complete excision was achieved of the area of microcalcifications with the mammotome probe : at final histology , in two cases ( average size 10.5 mm ) there were no malignant cells in the surgical specimen , in the other two cases ( average size 11 mm ) a complex sclerosing lesion with foci of 1 3 radiol med ( 2015 ) 120 : 369376 fig . 
1 : the microhistological finding was b5b ( infiltrating lobular carcinoma ) , confirmed at the final histological examination atypical ductal hyperplasia ( din1b ) and flat epithelial atypia ( din1a ) were present . 
with the encor probe two areas of microcalcifications were totally excised : one area ( diameter 7 mm ) was classified as b3 at microhistological examination and on final pathology no residual lesion was found ; similarly , the other totally excised area of microcalcifications ( diameter 10 mm ) was classified as b5a at microhistological examination and on final histology no residual in situ or invasive carcinoma was found ( tables 4 , 5 )  . 
the complete excision of microcalcifications is not to be considered an advantage compared to other techniques for percutaneous vabb needle biopsies since the goal is not therapeutic [ 13 ]  . 
in this regard , a reduction of the underestimation of malignancy with an increase of the diagnostic accuracy of the procedure was observed in the case of a complete excision of the lesions [ 14 ]  . both vabb system results are highly sensitive and specific in the assessment of suspicious microcalcifications with values similar to those obtained in the study of zuiani et al . 
taking into account these variables , the technical characteristics of the vabb system used do not seem to have the potential to increase the ppv . the strength of the vabb systems lies , however , in their high predictive value for the absence of malignancy ( vpn )  . 
 in this study and in our previous wider experience [ 1 ] in no case of vabb microhistological findings classified as benign did we later find the onset of a malignant lesion in the vabb sampling site , in agreement with other studies [ 8 , 13 , 19 , 20 ]  . a second advantage of using vabb systems compared to core biopsy with conventional semiautomatic systems is the reduction of the underestimation of lesions of uncertain biological potential or malignant in situ lesions . 
both vabb systems used give very accurate results in our series 1 3 376 radiol med ( 2015 ) 120 : 369376 and the underestimation of these types of lesions was inferior to other studies with respect to which it is probably not comparable due to the small sample size . 
as regards the processing time , the use of a closed system with automated vabb sampling compared to an open one with manual sampling resulted in a significant reduction only of the time taken to sample the cores ( calculated on an average of at least 6 cores )  . 
the overall duration of the procedures ( positioning of the patient , preand post - fire checks , etc . ) did not reveal statistically significant variations ( table 2 )  . 
clinical follow - up ( mean follow - up time 244 days ) was performed using the international prostate symptoms score ( ipss ) , quality of life ( qol ) , the international index of erectile function ( iief ) , blood prostatic specific antigen ( psa ) testing and transrectal prostatic ultrasound ( us ) scan with volume and weight calculation at 3 , 6 and 12 months . 
we obtained a reduction in ipss ( mean , 17.1 points ) , an increase in iief ( mean , 2.6 points ) , an improvement in qol ( mean , 2.6 points ) and a volume reduction ( mean , 28 % ) at 12 months . conclusions consistent with the literature , our experience showed the feasibility , safety and efficacy of pae in the management of patients with luts related to bph . 
pae may play an important role in patients in whom medical therapy has failed , who are not candidates for surgery or transurethral prostatic resection ( turp ) or refuse any surgical treatment . 
arena e - mail : arena.g@ospedale.cuneo.it 1 3 362 radiol med ( 2015 ) 120 : 361368 keywords prostatic arterial embolization benign prostatic hyperplasia lower urinary tract symptoms clinical and laboratory assessment introduction benign prostatic hyperplasia ( bph ) has a high incidence in men over 50 years of age [ 1 ] and it is more common with age [ 2 ]  . 
bph is often associated with lower urinary tract symptoms ( luts ) [ 3 ] , most frequently the sensation of incomplete emptying , hesitancy , decreased urinary stream , greater frequency , urgency , and nocturia [ 4 ]  . 
these treatments , even if minimally invasive such as those using microwave thermotherapies and other laser ablation , are not free from complications such as incontinence or urinary retention , sexual dysfunction ( retrograde ejaculation and impotence ) , and bleeding [ 79 ]  . two authors recently described prostatic artery embolisation ( pae ) as an alternative and minimally invasive technique for relief of luts in patients with prostatic enlargement [ 5 , 10 ]  . 
 [ 11 ] were the first to describe pae in a patient with bph to control spontaneous bleeding , with subsequent progressive reduction of prostatic volume and weight . our primary aim was to report the feasibility and effectiveness of pae in luts management in patients with bph with an indwelling catheter who were not eligible for surgical or endoscopic treatment . 
our secondary aims were to evaluate prostatic volume and weight , and ipss before and 6 months after pae . materials and methods from may 2012 to september 2013 , 13 patients underwent pae . 
all patients were ineligible for traditional surgical endoscopic treatment because of associated comorbidities ( american society of anesthesiologists score iii or iv ) , and two patients refused surgical treatment . 
before and 6 months after pae , patients underwent a clinical evaluation that included digital rectal evaluation , ipss scoring , uroflowmetry , prostatic surface antigen ( psa ) level measurement , transrectal ultrasound ( us ) examination , and computed tomographic angiography ( cta )  . 
iodine contrast material , 120 ml ( 350400 mg / ml ) , was injected at a rate of 5 ml / s followed by a 30 ml bolus of saline solution . 
aortic and pelvic angiography was performed first , followed by selective bilateral hypogastric artery and bilateral prostatic catheterisation performed 1 3 radiol med ( 2015 ) 120 : 361368 1 3fi 364 radiol med ( 2015 ) 120 : 361368 fig . 
1 computed tomography angiography ( cta ) shows chronic total occlusion of the left iliac axis ( white arrow ) in volume rendered ( vr ) ( a ) and maximum intensity projection ( mip ) ( b ) reconstruction . 
 multiplanar reconstruction ( mpr ) image ( c ) shows superior gluteal artery ( black star ) , glutealpudendal trunk ( white star ) and anterior vesical artery ( black arrow )  . 
digital subtraction angiography ( dsa ) shows the hypogastric artery trifurcation ( d ) and selective prostatic artery originating from the anterior vesical artery ( e ) ( white star ) using a telescopic technique with a 5 - f hydrophilic cobrashaped catheter ( terumo , tokyo , japan ) , a 2.4 - f microcatheter ( renegade stc 18 , boston scientific , natick , usa ) , and a 0.016 inch guidewire ( fathom , boston scientific , natick , usa )  . 
embosphere spherical particles ( biosphere medical , roissy - en - france , france ) and 300500 micron embozene microspheres ( celonova biosciences , newnan , ga , usa ) were used for the embolisation procedure . 
ipss , international index of erectile function ( iief ) , and quality of life ( qol ) scoring follow - up was performed using anamnestic interviews at a mean of 244 days following pae . results technical aspects pae was technically successful in 12 / 13 patients ( 92 % )  . 
 catheterisation was not possible in the other two cases because of tortuosity and atherosclerotic changes in the iliac arteries . procedure details and duration the pae procedure lasted from 120 to 240 min ( average 165 min ) and fluoroscopy time ranged from 41 to 110 min ( average 69 min )  . 
there were no intraor periprocedural complications or post - embolic syndrome , no patients felt pain after pae , and no adjunctive analgesic 1 3 radiol med ( 2015 ) 120 : 361368 fig . 
blood psa levels improved by 5.5 % at short - term ( 3 months ) follow - up , with a 39.4 % decrease at 6 months , and an increase of 45.7 % at 12 months . follow - up the prostatic volume in 10 patients showed a mean reduction of 32.8 % at the 3 months follow - up , 15.8 % at 6 months in five patients , and 33.9 % at 12 months in two all 12 patients showed a reduced ipss score ranging from 30 to 8 points ( mean 17.1 points ) , a qol improvement of 2.6 mean points , and an improved iief of 2.6 mean points at a mean follow - up of 244 days ( table 2 )  . 
clinical success , defined as improved symptoms post - procedure , was obtained in 100 % of the cases . 1 3 366 radiol med ( 2015 ) 120 : 361368 it was not possible to apply unior multi - variate statistical analysis to the data because of the small number of patients treated . 
the percentage data obtained were compared with the literature . discussion experimental studies of pae in pigs and dogs have reported safety and effectiveness in reduction of prostatic volume and weight [ 12 , 13 ]  . 
the rationale for pae in the treatment of bph is motivated by both the induced ischaemia and subsequent cell necrosis , theoretically reducing the blood levels of free testosterone that may act on prostatic cells . 
 pae may also reduce alpha - 1 adrenergic receptors resulting in reduced neuromuscular tone [ 12 ]  . previous studies allowed the patient to choose freely between pae and turp [ 20 ]  . 
 however , pae is a relatively long procedure ( fluoroscopy exposure duration averaged 69 min in our study ) with exposure peaks of 110 and 240 min of total procedure duration . because prostate size is not related to the severity of the symptoms , we expected that unilateral embolisation may have efficacy in bph , and two different authors [ 5 , 16 ] have reported the effectiveness of unilateral pae . 
this trend can be explained by initial acute involution related to the ischaemia caused by the procedure , followed by a phase of adjustment of the parenchyma , and then by a slight increase in volume as part of the physiological process of prostatic evolution . 
in fact , in the short - term follow - up ( 3 months ) , psa values increased , likely related to cell necrosis with the release of prostatic antigen into the bloodstreain the medium term ( 6 months ) , we observed a significant drop in psa values related to inactivity of the prostatic parenchyma and then in the long - term ( 12 months ) , a recovery , likely related to secondary blood supply from the creation , over time , of minor collateral circulation , as suggested by antunes et al . 
 comparing the pre - treatment data with current symptoms , we found a marked improvement in the ipss score as well as a significant increase in quality of life and an improvement trend in sexual function . 
4 transrectal ultrasound before pae ( ac ) and after pae ( d , e ) shows reduction of prostate volume reduction ( vp ) and weight ( peso ) of 515 % , and studies of pae have demonstrated a lack of complications associated with transurethral therapies , including bleeding , sexual dysfunction , incontinence , and dilutional hyponatraemia [ 21 ]  . the results of our study agree with the current literature [ 5 , 10 , 22 , 23 ]  . 
our experience , despite the limited data precluding the demonstration of statistical significance , confirmed the feasibility , safety , and effectiveness of pae in the management of patients with luts associated with prostatic hypertrophy , confirming previous results reported from larger studies . 
we showed that pae may have a role in patients for whom medical therapy has failed , who are not candidates for surgery or turp because of concomitant diseases , or who have refused surgery . 
we obtained encouraging results both in terms of quantity ( gland volume and serum psa ) , and of quality ( reduction of ipss , improved qol scores , and increased iief ) with no peri - procedural complications or side effects . conclusions our preliminary experience confirmed that pae is a promising interventional radiological procedure in bph . 
this article is published with open access at springerlink.com abstract positron emission tomography , most commonly with 18f - fluorodeoxyglucose , is being used for evaluation of tumour response to therapy . 
limitations of this method are associated with ( 1 ) fluorodeoxyglucose pharmacokinetic properties , ( 2 ) the detection system , ( 3 ) discrepancies between metabolic and anatomic images , and ( 4 ) acquisition standardization . 
response to therapy may be evaluated with qualitative ( deauville score ) , semiquantitative ( standardised uptake value ) , and quantitative methods ( european organization for research and treatment of cancer ; positron emission tomography response criteria in solid tumours )  . 
increased clinical use of these methods will depend on the development and validation of intuitive and simple analytic tools . keywords cancer treatment imaging metabolism introduction most malignancies incorporate glucose much more than normal tissues . 
damico ( * ) department of diagnostic positron emission tomography , maria skodowska - curie memorial cancer centre and institute of oncology , ulica wybrzeze armii krajowej 15 , 44 - 101 gliwice , poland e - mail : adamico@io.gliwice.pl basis of positron emission tomography ( pet ) scanning in oncological imaging . 
unlike glucose , fdg cannot be catabolised in the glycolytic pathway and remains in the form fdg6 - phosphate for the duration that the molecule remains radioactive and visible on pet . 
the distribution of radiolabelled fdg reflects the biodistribution of glucose and its phosphorylation in the different regions of the body . in 1931 , the german scientist otto heinrich warburg showed a relation between the degree of conversion of glucose to lactic acid and tumour growth , and this became the basis of cancer imaging with fdg . 
the production of adenosine triphosphate by the metabolism of glucose to lactate is caused by up - regulation of several enzymes and transporters ( glucose transporter 1 , hexokinase ii , pyruvate kinase m2 , and lactate dehydrogenase ) [ 1 , 2 ]  . 
despite the lower efficiency of energy production by aerobic glycolysis than mitochondrial respiration , glucose catabolism may generate precursors for the synthesis of proteins , nucleic acids , and membranes that are essential for cell proliferation . 
therefore , the warburg effect occurs in cancers and other rapidly proliferating eukaryotic cells such as yeast cultures and is a universal mechanism that may provide growth advantages [ 35 ]  . a small amount of fdg , much lower than obtained with pharmacological doses , may cause a concentration of radioactivity within a tumour that may be detected easily with modern pet computed tomography ( pet - ct ) or pet magnetic resonance imaging ( pet - mri ) devices . 
 the degree of fdg accumulation in healthy tissues may 1 3 346 radiol med ( 2015 ) 120 : 345351 enable the identification of pathological areas in most body regions , with some restriction for organs that have exclusively glucose - based metabolism such as the brain or that participates in fdg excretion such as the kidneys and urinary system . the most common applications of fdg - pet in oncology involve the evaluation of disease extent . 
this fact is very important for lymph node localisation , and diagnostic accuracy is greater for fdg - pet scanning than ct or mri scanning without pet [ 6 , 7 ]  . false negative results with pet scanning may occur with tumour pathologies that have low levels of fdg accumulation such as prostate , stomach , or neuroendocrine tumours . 
false negative results also may occur with lesions that are below the limits of resolution of the pet scanner ( currently , 45 mm ) or lesions that are anatomically close to a structure that is moving during the pet examination such as the diaphraghowever , false negative results may be minimised with careful patient selection and awareness of the inherent limitations of the method . false positive results are currently a greater clinical problem than false negative results because many non - neoplastic diseases may have a high level of glucose metabolism , such as infections or inflammatory conditions with lymph node involvement . 
however , false positive results may be minimised with careful patient preparation and experience of the nuclear medicine specialist . imaging with fdg - pet is useful because of the early and marked reduction in tumour metabolism in response to chemotherapy or radiation therapy . 
the fdg - pet scan may detect a treatment response in a very early phase of treatment , and this may enable the identification of chemoresistant tumours that may benefit from alternative treatments . 
in addition , it may be important to detect residual disease after treatment is completed . current pet scans are usually performed with pet - ct scanning , but pet - mri scanners are becoming available . 
the ability to detect the photons emitted from the patient is similar , and the quality of metabolic imaging is comparable , between pet - ct and pet - mri devices . 
the petmri scan may provide greater inherent contrast to visualise soft tissues , which could be advantageous in evaluating pelvic tumours and sarcomas , but pet - ct is better for oncological imaging of the lungs . 
in children , pet - mri is preferred because of the lower radiation dose than with pet - ct scanning [ 8 ]  . quantification of tumour with positron emission tomography nuclear medicine techniques including pet scanning have limitations that differ from other radiographic studies . 
 these limitations are associated with ( 1 ) fdg pharmacokinetic properties , ( 2 ) the detection system , ( 3 ) discrepancies between metabolic and anatomic images , and ( 4 ) acquisition standardization . the pharmacokinetic properties of fdg enable a dynamic method of image acquisition . 
the sequential data obtained after administration of the radiotracer , ( corrected for attenuation , scatter , and radioactive decay ) enable determination of the concentration of radiotracer in the body region . 
the most common compartmental model for the analysis of pet data is the patlak plot , a graphical analysis technique that assumes three compartments : the arterial blood compartment , the compartment of radiotracer - free distribution , and the compartment of specific and irreversible binding [ 9 ]  . 
quantitative assessment of tumour metabolism is performed with pharmacokinetic constants that express radiotracer passage between compartments . clinical evaluation of dynamic data may be limited because of the need to shorten the time of image acquisition for each patient , the difficulty of arterial blood sampling to evaluate the input function , and the small field of view of the pet scanner ( approximately 20 cm )  . 
in addition , small differences in time between fdg administration and pet scanning for different scans ( before and after treatment ) may cause major errors in interpreting radiotracer accumulation . current pet scanners have a spatial resolution of approximately 4 m radiotracer uptake in lesions that have diameter < 3 times the scanner resolution is affected by partial volume effect , which causes loss of apparent activity . 
for example , in a pet scanner that has spatial resolution 4 mm , the image of a radioactive phantom with 6 - mm diameter may show a maximum measured 60 % real activity concentration [ 10 ]  . modern pet - ct devices typically require 10 min between the initial ct scan and pet image acquisition in more distal body parts . 
 1 3 radiol med ( 2015 ) 120 : 345351 furthermore , the acquisition of each pet image requires 90 s , and breathing movements make it impossible to quantify accurately the metabolism of lesions near the diaphrag acquisition techniques such as pet gating for breathing may be helpful , but these methods lengthen the time of acquisition and data processing and are not used frequently in clinical settings [ 11 ]  . standardised acquisition protocols of the european society for therapeutic radiology and oncology and european association of nuclear medicine include information about the calibration of the pet scanner , radiotracer uptake time , and approach for definition of regions of interests . 
in contrast with ct scanning , it is not possible to compare quantitative measurements of pet scans performed in different institutions . qualitative and visual evaluation methods comparative visual assessment of pet images is commonly practised and frequently enables reliable judgements about decreased tumour metabolism after therapy . 
in these cases , the uptake by the tumour may be similar to physiological activity present in other regions that have a stable level of metabolisreference organs typically include the liver and mediastinal tissues . early investigation of malignancy by pet was performed with lymphoma , and the earliest systems to assess treatment were proposed for these neoplasms . 
in contrast , the metabolic response may be detected after 13 cycles of chemotherapy and is correlated with overall and diseasefree survival [ 1417 ]  . the deauville score is a popular method for the evaluation of qualitative response to treatment of hodgkin lymphoma . 
this score is based on a simple classification table 1 deauville scoring system for evaluation of hodgkin lymphoma with 18f - fluorodeoxyglucose positron emission tomography deauville score radiotracer uptake no lesion uptake > background lesion mediastinum mediastinum < lesion liver lesion moderately > liver lesion markedly > liver new lesion uptake unlikely related to lymphoma adapted from meignan et al . 
 lesions that have fdg radiotracer uptake liver ( deauville score 1 , 2 , or 3 ) are metabolically negative , and lesions that have fdg uptake > liver ( deauville score 4 or 5 ) are positive ( table 1 ) [ 18 ]  . 
the deauville score was validated in a multicentre trial with many patients [ 19 ]  . in contrast , pet scanning is unsuitable for assessing the activity and extent of tumours that have moderate radiotracer accumulation , such as renal clear cell carcinoma , primary liver tumours , and adenocarcinoma of the prostate [ 20 ]  . methods based on the standardised uptake value the suv , a semiquantitative indicator of fdg uptake by tumours , is the ratio between the concentration of radioactivity measured in a body part and the hypothetical concentration of radioactivity that should be measured with a homogeneous distribution of radiotracer in the entire body [ 21 ]  . 
activity in a tumour may be expressed as the voxel that has maximum suv in the whole tumour volume ( suvmax ) : suvmax = [ c ( ci / ml ) / id ( ci ) ] / w , where c is the activity at a pixel within the tissue identified by regions of interest , and id is the injected dose per kilogram of the patients body weight ( w )  . 
this patient had lymph node metastatases from a planocellular nasopharyngeal carcinoma of the right neck ( solid arrow ) coexisting with hodgkin lymphoma at the left neck ( dotted arrow )  . 
the problem of reliability necessitates highly standardised protocols for pet imaging to provide the same conditions of acquisition and data processing between pet examinations for proper comparisons [ 22 ]  . the first quantitative criteria to monitor tumours were proposed by the european organization for research and treatment of cancer ( eortc ) in 1999 . 
the eortc criteria defined tumour response to treatment as changes in suv > 15 % after the first cycle of chemotherapy ; changes in suv > 25 % afte > 1 cycle of chemotherapy ; changes in fdg accumulation > 20 % ; or new foci of pathological fdg uptake [ 23 ]  . the pet response criteria in solid tumours ( percist ) is a more detailed classification and requires a more rigor ous standardisation for data acquisition and analysis than the eortc criteria ( table 2 ) [ 24 ]  . 
the percist criteria define limits for maximum acceptable glycaemia , injected dose , and acquisition timing , and these criteria are suitable only for examinations performed with hybrid pet - ct scanners . 
the tumour activity is quantified by the suv peak , which considers the average concentration of radioactivity in a spherical area ( radius , 1 cm ) centred on the most active part of the tumour . 
in addition , an analysis of the reference uptake ( hepatic or mediastinal ) is required in percist to ensure the absence of significant differences in fdg biodistribution from before to after therapy . 
however , it is important to quantify tumours < 2 cm correctly , and partial volume correction methods are being developed [ 2528 ]  . methods under evaluation metabolic tumour volume several methodological errors may confound the quantification of tumour metabolism when using the suv parameter . 
however , 1 3 radiol med ( 2015 ) 120 : 345351 table 2 classification systems for positron emission tomography evaluation of response to treatment of solid tumours , adapted from wahl et al . 
alternatively , the suv threshold may be calculated as the percent maximal tumour uptake of fdg in tissues surrounding the tumour or other reference organs such as the liver [ 2932 ]  . 
in addition , other systems are available that are not based on the suv threshold and that use complex mathematical models to detect the tumour - background interface [ 3339 ]  . 
very high repeatability is feasible with some techniques [ 4 ]  . total lesion glycolysis heterogeneity of fluorodeoxyglucose uptake in addition to the volumetric parameters , additional features may be extracted from pet images by computational methods such as tumour texture and heterogeneity [ 44 ]  . 
mathematical models that measure the level of heterogeneity may be useful in selected patients [ 45 , 46 ]  . the calculation of metabolic tumour volume is based on the definition of tumour boundaries . 
the total lesion glycolysis is the product of the average tumour suv ( which is an index of the density of neoplastic cells ) and conclusions it is feasible to perform early measurement of the effect of therapy on cancer , and functional tomographic techniques such as fdg - pet may be useful in addition to morphological imaging methods . 
the accuracy in measuring tumour 1 3 350 radiol med ( 2015 ) 120 : 345351 response is limited by the difficulty in performing dynamic analysis of tumour metabolism after the radiopharmaceutical agent is given . 
kent yucel received : 7 august 2014 / accepted : 27 august 2014 / published online : 26 september 2014 italian society of medical radiology 2014 to the editor , we read the article by sperandeo and colleagues [ 1 ] with great interest . 
overall , this was a thoughtful approach to the emerging uses of ultrasound for thoracic disease . this article also stresses the use of ultrasound as an important auxiliary technology for chest diagnosis , as well as the limitations of ultrasound in the chest . 
while it may be possible to distinguish pulmonary parenchymal disease such as tumor versus pneumonia with ultrasound , further evaluation is indicated to make a definitive diagnosis . there are issues involved in applying ultrasound technology in routine clinical practice ( point - of - care ultrasound )  . 
yucel department of radiology , tufts medical center , 800 washington street , boston , ma 02111 , usa e - mail : jkatz@tuftsmedicalcenter.org evidence , and are of questionable validity if applied in the care of patients . while it is very appealing to be able to make a diagnosis quickly , cheaply , and without radiation , it is much more important to have an accurate diagnosis , made with properly maintained equipment by someone who is aware of how best to use the equipment , interpretive pitfalls , technical look - alikes , false positives and false negatives . it is understandable that clinicians would like a widely available tool that is free of radiation and that would help to guide their management of disease processes . 
with the publication of multiple articles advocating the use of point - of - care ultrasound in a variety of areas , each specialty exerts pressure on its practitioners and trainees to provide this technology . 
very little attention is paid to the nuts and bolts of acquiring high - quality images or to understanding the physics involved in generating these images and artifacts ; there is very little high - quality data in the pulmonary , cardiac or emergency medicine literature with prospective blinded studies comparing point - of - care ultrasound to gold standard imaging tests or good clinical follow - up . in addition , before applying this technology in clinical practice , it is necessary to take care to ensure that all practitioners are well trained and supervised while they are early in their experience . 
passing the technique on from practitioner to practitioner in an uncontrolled manner , while simultaneously taking care of sick patients in a high - pressure environment ( the emergency department or the intensive care unit ) is a recipe for bad clinical outcomes . 1 3 radiol med ( 2015 ) 120 : 404405 in medicine today , there is so much pressure to be efficient that clinicians often behave as though the history and physical examination are less productive than an imaging study . 
while the clue to a diagnosis may be available on a radiographic or ultrasound study , the findings are often non - specific , and the clinical infor mation is critical to making an accurate diagnosis . 
the shock index ( ratio of heart rate to systolic blood pressure ) and measured cta parameters were compared between the high - risk group and the low - risk group , and the correlation between the measured cta parameters and shock index was analysed . results the shock index and ratio of false / true lumen were compared between stanford type a and type b , and no statistically significant differences were found . 
with the improvement of the medical imaging technology , computed tomography angiography ( cta ) is able to display the extent of false lumen and 1 3 radiol med ( 2015 ) 120 : 386392 intimal tears in ad patients . 
the characteristics of measured cta parameters were related to the transportation risk of ad patients , and the correlation between these characteristics and the shock index was analysed . materials and methods general information from march 2009 to january 2014 , the cta images of the initial examination ( within the first 24 h after onset ) and the follow - up results ( after transfer ) of 36 ad patients were reviewed . 
the scan parameters were : helical scan , 0.35 s / rot , 120 kv , 350 ma , collimator width 40 mm , standard mode and slice thickness 0.625 ma dose of 90 ml nonionic contrast medium ( iohexol , 300 mgl / ml ) was injected at a rate of 4 ml / s , followed by 30 ml saline at the same rate . 
this retrospective analytical process was performed by two experienced physicians with a double - blind method . diameter of intimal tear indicated the maximum diameter which was measured during processing the cta image . 
the shock index was the ratio of heart rate ( beats per minute ) to systolic blood pressure ( millimetres of mercury ) , which was recorded by electrocardiographic ( ecg ) monitoring when the patients were examined with cta . data analysis and statistical methods on the basis of the cta examination , 36 cases of ad were 18 cases ; type divided into two groups ( stanford type a 18 cases ) , and the shock index and the measured cta parameters were compared between the two groups . 
then the 36 ad cases were divided into a high - risk group and a low - risk group in accordance with the modified early warning score ( mews )  . 
linear correlation analysis was used in the shock index and other measured cta parameters ( diameter of intimal tear , maximum diameter of aorta and the length of involved aorta )  . 
the 36 ad patients confirmed with 64 - slice vct were divided into a high - risk group and a low - risk group based on the modified early warning score ( mews ) [ 5 ] ( table 1 )  . 
fourteen patients ( age range , 1474 years ; mean age , 53.4 years ; 13 males and 1 female ) with mews 5 or above were allocated to the high - risk group . 
the other 22 patients ( age range , 3683 years ; mean age , 56.2 years ; 14 males and eight females ) belonged to low - risk group . ct angiography parameters and shock index outcome of transfer the ratio of false / true lumen was the maximum ratio of false lumen to true lumen of the ad on the axial cta image . 
the there were 11 cases of death among the 36 ad patients ; of these , six cases were in the high - risk group and five cases 1 3 388 score table 1 modified early warning score systolic blood pressure ( mmhg ) 7180 heart rate ( bpm ) respiratory rate ( bpm ) temperature ( c ) neurological 81100 4150 101199 51100 914 3538.4 alert 101110 1520 111129 2129 38.5 reacting to voice reacting to pain unresponsive radiol med ( 2015 ) 120 : 386392 were in the low - risk group . 
the other nine patients ( four in the high - risk group and five in the low - risk group ) died within the first 48 h after arrival at destination . 
in addition , three patients in the low - risk group did not undergo surgery and their condition was stable after 6 months follow - up . comparative analysis of stanford a and b the shock index and the measured cta parameters were compared between the stanford type a and type b groups . 
there were no obvious differences between the groups , p > 0.05 ( table 2 )  . comparative analysis of high - risk group and low - risk group according to the modified early warning score ( mews ) , 14 cases were allocated to the high - risk group and 22 cases to the low - risk group . 
2 cta axial image of aortic dissection shows the severe compressive deformation of the true lumen , and the false lumen occupying almost the entire aortic lumen , so as that the false lumen is much larger than the true lumen . 
 ( t indicates the true lumen and f the false lumen ) differences in mortality and other measured cta parameters were not obvious between high - risk group and low - risk group , p > 0.05 ( table 3 )  . 1 3 389 radiol med ( 2015 ) 120 : 386392 fig . 
 ( red arrows indicate the false lumen , and the white arrow in image b shows the contrast agent overflow from the abdominal aorta ) correlation between the shock index and other measured cta parameters ( the diameter of intimal tear , the maximum diameter of aorta and the length of involved aorta ) , p > 0.05. discussion aortic dissection ( ad ) is a life - threatening condition , in which an intimal tear in the aortic wall forms a dissection membrane creating a true and a false intramural lumen [ 6 ]  . 
 depending on its location , ad has potential fatal complications such as malperfusion of brain , coronary arteries , spinal cord , kidneys , bowel and lower extremities as well as aortic rupture , shock or uncontrollable hypertension [ 7 ]  . 
according to literature reports , the prehospital mortality of aortic dissection reaches 2030 % , and the mortality within 48 h after onset reaches 50 % [ 8 , 9 ]  . 
in local hospitals , it is a general problem for ad patients to be transferred to a specialised hospital in a timely and safe manner . the ability of a modified early warning score ( mews ) to identify patients at risk of catastrophic deterioration in fig . 
 ( t indicates the true lumen , f the false lumen , and the arrow shows the intimal tear ) analysis of correlation between shock index and cta parameters in this study , the correlation between the shock index and the measured cta parameters in the 36 patients with ad confirmed with 64 - slice vct was analysed ( table 4 )  . 
according to literature reports , the shock index has been widely used in risk prediction for many diseases , such as trauma , pulmonary embolism , severe pneumonia , ectopic pregnancy , etc . 
6 scatter plot showing a significant correlation between the ratio of false / true lumen and the shock index 0.54 in the high - risk group , and it was significantly currently , most scholars consider a shock index of 0.9 as an indicator of the risk of shock and even death for patients [ 13 , 14 ]  . 
at the same time , our findings also support that it is possible to consider the shock index an important clinical indicator for predicting the transportation risk of ad patients . the true lumen of ad will be subjected to different pressure due to the formation of the false lumen , and the diameter of the false lumen is larger than that of the true lumen most of the time [ 2 , 15 ]  . 
considering that the shock index has become a critical and important indicator to predict risk of death and critical level of patients , the ratio of false / true lumen may become an important imaging evaluation to predict the transportation risk in ad patients . 
there are still very different viewpoints in the literature reports regarding whether aortic diameter is able to predict the occurrence and prognosis of ad [ 16 , 17 ]  . 
in terms of shock index and all of the considered cta parameters , there were no obvious differences between the stanford type a and type b groups ( p > 0.05 ) , but this finding should be further confirmed in consideration of the small size of study sample . 
this may be related to the successful performance of artificial vascular replacement or intravascular stent surgery for some aggravated cases . in conclusion , the shock index and the ratio of false / true lumen were the essential clinical and radiological indexes for assessing the risk of transportation of ad patients . 
 there is a significant correlation between the ratio of false / true lumen and shock index , and there is great clinical value in assessing the risk of transportation in ad patients . acknowledgments we are grateful for the support of the radiology department and clinical colleagues in the research process . 
secondly , we thank the hospital management for its support and care , and we extend a special thanks to professor xue yanshan of the second hospital of shanxi medical university for his help in all aspects . 1 3 conflict of interest the authors declare no conflict of interest 10 . 
cozzi carlo catalano received : 30 december 2013 / accepted : 5 june 2014 / published online : 28 october 2014 italian society of medical radiology 2014 abstract purpose this study was done to evaluate the role of fetal magnetic resonance imaging ( mri ) in the study of gastrointestinal malformations in comparison to prenatal ultrasound ( us )  . materials and methods a prospective ( 20102012 ) study of 38 fetal mri scans was performed on 38 fetuses between 24 and 38 weeks of gestation . 
all fetal mri diagnoses were compared with postnatal us findings , autopsy or sur gical reports . results fetal mri was able to confirm the sonographic findings in nine of 38 fetuses ( 23.7 % ) , to provide additional information in 23 of 38 fetuses ( 60.6 % ) , to exclude the us diagnosis in five cases ( 5.2 % ) and to change it in l . 
in addition , its sensitivity in the detection of gi anomalies depends on the features of the pathology , and it is not always possible to reach an exact prenatal diagnosis , such as in cases of abdominal masses , which are often difficult to characterize during us examination [ 69 ]  . fetal mri is , therefore , necessary either when a us examination is inconclusive or when additional information is necessary for prognostic or therapeutic findings [ 7 , 10 ]  . 
 although mri is not recommended in the first trimester of pregnancy , there is no evidence of adverse effects of this technique on fetal development [ 11 ]  . 1 3 394 radiol med ( 2015 ) 120 : 393403 the introduction of ultrafast sequences provided an excellent evaluation of fetal anatomy with marked reduction of motion artifacts [ 12 ]  . 
due to its multiparametricity , mri allows an optimal tissue characterization , which is useful for determining the content of abdominal masses and distinguishing between meconium and urine [ 13 ]  . in our study , we evaluated the role of mri in confirming , providing additional information about us findings , and changing or excluding the us diagnosis of fetal gi anomalies . materials and methods patients and study table 1 data used as gold standard to confirm fetal mri findings mri diagnosis postnatal us autoptic findings surgical findings diaphragmatic hernia choledochal cysts fluid collection bowel atresia cloacal malformation meconium pseudocyst esophageal atresia isolated ascites normal total n number of cases from december 2010 to march 2012 , we performed 224 fetal mri examinations at our university hospital . 
the mean maternal age was 30 years ( range 2342 years ) and the mean gestational age was 27 weeks ( range , 24 - 38 weeks )  . this single - institution study project was approved by the ethics committee of our hospital and written informed consent was obtained from all mothers . our inclusion criteria were : visualized or suspected fetal gi pathologies at a recent prenatal us ( from 0 to 7 days before mri ) , the agreement of the mothers to give information about the course of the pregnancy , the delivery and the newborn , as well as a gestational age at the time of the mri examination of more than 19 weeks ; the gestational age > 19 weeks was adopted as an inclusion criterion because obtaining sufficient spatial and contrast resolution to provide diagnostic or additional information with respect to us examinations is not considered possible before 19 weeks and all major developmental steps have taken place only by this age of gestation [ 5 ]  . exclusion criteria were fetal abdominal abnormalities of suspected genitourinary ( gu ) origin ( e.g. , cystic kidney disease , hydrometrocolpos , ovarian cyst ) , abdominal solid masses of non - gi origin ( e.g. , sacrococcygeal teratoma , neuroblastoma ) on us as well as general contraindications to mri of the mother , claustrophobia and gestational age us ultrasound , mri magnetic resonance imaging , puv posterior urethral valve < 19 weeks . 
we did not include in our study fetuses with defects of the abdominal wall ( e.g. , omphalocele , gastroschisis ) because to date there is no evidence of greater accuracy than us , and the indication for fetal mri may be for surgical planning and defining the manner of birth rather than for diagnostic purposes per se [ 5 ]  . amniocentesis was performed on 15 / 38 patients , resulting in a normal karyotype in all the 15 cases ( nine fetuses 46 , xy ; six fetuses 46 , xx )  . of the 38 fetuses included in the study , 33 ( 87 % ) were brought to term , with 27 / 33 fetuses being born with natural birth and 6 / 33 with cesarean section ; 5 / 38 pregnancies ( 13 % ) were voluntarily terminated due to the presence of cloacal malformation in one case and diaphragmatic hernia with severe cardiomediastinic shift and lung damage in four cases . 
three cases of diaphragmatic hernia and two cases of esophageal atresia died after birth due to the presence of respiratory complications . of the 38 fetuses in the study , 22 ( 58 % ) were males and 16 ( 42 % ) were females . follow - up was available for all fetuses . 
fetal mri findings were compared to after - birth us in six cases , to autoptic data in 10 cases and to surgical findings in 22 cases ( table 1 )  . mri technique all fetal mri examinations were performed on a 1.5 - t superconducting magnet ( siemens avanto , erlangen , germany ) using one or two phased - array surface coils , depending on the maternal abdomen size . 
diaphragm. results fetal mri confirmed the us findings of gi anomalies in nine of the 38 fetuses ( 23.7 % ) , provided additional information in 23 ( 60.5 % ) , excluded the us diagnosis in five ( 5.2 % ) , changed it in two ( 5.2 % ) and failed in two cases ( 5.2 % ) ( table 2 )  . fetal mri correctly diagnosed : bowel atresia in 11 cases , cloacal malformation in one case , meconium pseudocyst in one case , posterior urethral valve ( puv ) in one case , esophageal atresia in five cases , isolated ascites in one case , intra - abdominal cysts in three cases and diaphragmatic hernia in eight cases . in 12 of the 15 fetuses with a us diagnosis of bowel dilation , mri provided more information than us because it identified the level of obstruction by evaluating the caliber of the bowel loops and the meconium and / or amniotic fluid content . 
b , c a truefisp axial mr image shows hypointense dilated bowel loops ( b , white arrows ) , which are hyperintense on a fat - saturated t1 - weighted axial mr image due to the meconium content ( c , black arrows )  . 
d , e a truefisp coronal mr image ( d ) and a t2 - weighted haste sagittal image ( e ) show the subhepatic ( d , open arrow ) and anterior ( e , white arrow ) location of the dilated bowel loops in the fetal abdomen . 
in one fetus with us findings of an abdominal cyst in the right upper quadrant of the abdomen , the cyst was detected neither on fetal mri examination nor on postnatal us . 
it was not possible to characterize the cystic lesion in 2 / 6 fetuses : in one case , the mr findings led us to suspect a choledochal cyst , but after birth a careful surgical evaluation made a diagnosis 1 3 radiol med ( 2015 ) 120 : 393403 fig . 
bf axial ( b ) , sagittal ( d ) , coronal ( f ) truefisp mr images and a coronal t2 - weighted mr image ( e ) show hyperintense dilated stomach ( open arrow ) and duodenum ( white arrow ) , which are hypointense on a t1 - weighted mr axial image ( c ) , due to the presence of amniotic fluid . 
dilated small bowel loops ( asterisks ) , hyperintense on truefisp ( b , f ) and t2 - weighted ( e ) images and slightly hyperintense on the t1 - weighted image ( c ) due to the poor content of meconium , present thin wall because of the increased intraluminal tension ( f , black arrow ) of gastric duplication ; in the other , mr only confirmed the sonographic finding of a cystic mass , but the absence of septa led us to suspect a fluid collection . 
the final diagnosis of abdominal cystic lymphangioma was made on postnatal surgical evaluation . mri confirmed the us finding of isolated ascites , excluding the presence of any gi or genitourinary ( gu ) tract anomalies . 
postnatal us examination showed disappearance of the ascites one month after birth . in the three cases of feb without any abdominal anomalies , fetal mri and postnatal us examinations confirmed the absence of bowel dilation or other fetal gi abnormalities . discussion several authors have compared the efficacy of us and mri in the diagnosis of fetal anomalies , revealing that mri provides additional information in comparison to us in 3657 % of cases [ 1417 ]  . 
most of them evaluated the accuracy of mri in the diagnosis of central nervous system diseases , which are the most common indications for fetal mri [ 1820 ] , but little has been written on the use of fetal mri in confirming or excluding us diagnosis of fetal gi abnormalities [ 1 , 2 , 10 , 21 ]  . thanks to a wide field of view , its intrinsic multiparametricity and multiplanarity mri provides a detailed 1 3 radiol med ( 2015 ) 120 : 393403 398 fig . 
 the mri findings are highly suggestive of a meconium pseudocyst evaluation of the whole fetal gi tract and could be helpful in identifying the various intestinal segments [ 1 , 2 , 10 ]  . 
 in cases of bowel obstruction , sonography usually detects only the dilated loops proximal to the atresia [ 22 ] without providing any significant information about the presence of meconium and / or amniotic fluid . 
in our study , in 12 of the 15 fetuses with a us diagnosis of bowel dilation , mri detected the level of obstruction , determining the content and the caliber of both the preand post - atresic bowel loops and rectu as previously reported , the signal of the bowel content depends on the site of the atresia . 
in a proximal atresia , only fluid will accumulate , with a high t2 and a low t1 signal , whereas in a distal atresia mri shows high pre - atresic bowel loops signal on t1and low signal on t2 - weighted images , due to the presence of more or less hydrated meconium [ 1 ]  . 
in our study , mri showed high t2 and low t1 signal intensity proximally to the obstruction , due to presence of amniotic fluid , in fetuses with jejunal and duodenal atresia and intermediate t1 and t2 signal , for the simultaneous presence of meconium and amniotic fluid , in fetuses with ileal atresia . 
in the case of multiple atresia and in the three fetuses with colonic atresia , the pre - atresic bowel loops had meconium - like signal , high on t1and from low to intermediate on t2 - weighted images ; in these fetuses mri also detected a microcolon , showing a reduced caliber of the bowel distal to the obstruction and rectum along with a poor meconium content with low to intermediate t1 signal intensity . 
this last finding is often undetected on us although its diagnosis is important for optimal surgical planning [ 1 ]  . in fetuses with cloacal malformation , the urinary tract , the vagina and the rectum converge above the perineum , create a common channel with a single external opening . 
 in our case , mri provided additional information revealing a dilated rectum and colon with abnormal increased t2 and decreased t1 signals , indicating communication between the urinary tract and rectum , which was separated from the bladder wall by a third structure with intermediate t1 and t2 signal . mri also distinguished between bowel and ureteral dilation in the case of puv described , because urine has high signal intensity on t2 - weighted and low on t1 - weighted 1 3 radiol med ( 2015 ) 120 : 393403 fig . 
be the dilated ureters ( white arrows ) are hyperintense on a t2 - weighted haste axial ( b ) and a truefisp coronal ( d ) image and hypointense on t1 - weighted axial ( c ) and coronal ( e ) mr images , because of the presence of urine ; the rectosigmoid colon ( open arrow ) is located in the middle of the fetal abdomen and presents low signal intensity on t2 - weighted ( b ) and truefisp ( d ) images and high signal intensity on t1 ( c , e ) , due to its meconium content . 
f the typical keyhole sign ( open arrow ) on a t2 - weighted haste sagittal image suggests the diagnosis of puv sequences [ 13 , 24 ] and showed the typical keyhole sign , which refers to the appearance of the dilated posterior urethra associated with thick - walled distended bladder [ 25 ]  . meconium peritonitis is caused by a bowel perforation linked to various conditions , such as the presence of intestinal atresia , meconium ileus [ 26 ] or intussusception [ 27 ]  . 
mri also showed the meconium content of the cyst due to the high t1 signal , allowing differentiation of other intra - abdominal cysts , such as mesenteric or duplication cysts . in a case of us diagnosis of bowel dilation , fetal mri did not show any abnormality . 
feb is a us finding which can be observed in cases of cystic fibrosis , prenatal infections or other fetal pathologies , where it is often associated with other us findings , such as ascites or bowel dilatation [ 29 ]  . 
however , because feb is associated with 33.3 % of poor perinatal outcome and 5.5 % of perinatal mortality [ 29 ] , it is important to exclude other fetal associated anomalies in case it tends to persist during the pregnancy . some studies have demonstrated the usefulness of fetal mri in determining the origin [ 1 , 2 , 14 , 30 ] and in providing an accurate characterization of abdominal fetal cystic 1 3 400 radiol med ( 2015 ) 120 : 393403 fig . 
5 a 28 - week fetus with diaphragmatic hernia on the left side of the diaphraga an axial sonogram of the fetal abdomen performed 2 days before mr examination shows an increased echogenicity of the left side of the thorax suggesting the presence of a diaphragmatic hernia ( black arrow )  . 
bd axial ( b ) and coronal ( c ) t2 - weighted mr images show the presence of small and large bowel loops in the left emithorax ( b , c , circle ) associated with shift of the heart to the right side of the thorax ( white arrow )  . 
ef coronal ( e ) and sagittal ( f ) haste t2 - weighted mr images show the presence of the upper pole of the left kidney ( open arrow ) and of the right lobe of the liver ( white arrow ) in the thorax along with compressed parenchyma of the right lung ( e , asterisk ) masses [ 7 , 14 , 21 ]  . 
some authors reported the mri diagnosis of this abnormality [ 14 , 31 ] , but in our case the absence of septa , which are usually present in this kind of anomaly , led us to wrongly diagnose a fluid collection . 
in the second , the proximity of the cystic formation to the biliary tract directed us to the incorrect diagnosis of choledochal cyst , but the postnatal examination revealed a gastric duplication . 
in the other three cases , the evident connection of the cystic lesion to the biliary tract , not visualized at us , and the fluid content of the lesion , led us to correctly diagnose the presence of a choledochal cyst , confirming the role of mri in recognizing this fetal malfor mation , as previously reported by chen [ 32 ]  . 
in one fetus , the us detection of an abdominal cyst located in the right upper abdomen was not confirmed by mri and was likely to be of hepatic origthe intrauterine disappearance of a hepatic cyst can be expected especially when the cysts are peripheral [ 33 ]  . in the eight cases of diaphragmatic hernia mri detected the site of the defect , the extent , the content of the herniation , and the mass effect of the herniated organs on the thoracic structures , with the presence of cardiomediastinic shift and lung damage [ 34 , 35 ]  . 
a axial sonogram of the fetal abdomen performed 2 days before mr examination shows an anechoic cystic mass ( white arrow ) adjacent to the liver with significant posterior acoustic enhancement . 
bc a subhepatic cystic formation of 3 cm is hyperintense on a t2 - weighted haste axial mr image ( b , open arrow ) and hypointense on a t1 - weighted fs image ( c , white arrow ) due to its fluid content . 
de a t2 - weighted cholangiographic coronal image and a t2 - weighted haste coronal image show the cyst ( open arrow ) and the stomach ( white arrow )  . 
f a t2 - weighted haste sagittal image confirms the subhepatic location of the cyst ( white arrow ) and the connection to the biliary tract ( black arrow )  . 
the bladder is located below the abovementioned cystic formation ( open arrow ) liver , relatively hyperintense compared to the heart , from the colon , typically hyperintense because of the presence of meconiu furthermore , mri was superior to us in the assessment of the position of the liver and the kidney in relation to the diaphragm , which is considered an independent predictive factor and defined as liver up versus liver down and kidney up versus kidney down [ 36 ]  . another frequent abdominal finding is the presence of ascites , usually caused by an obstructive uropathy or a gi disorder . 
some authors believe that if no factor is etiologically correlated with the presence of ascites , this could be related to the presence of a chylous peritoneal fluid , caused by the obstruction of lymphatic vessels or the presence of a lymphatic dysplasia [ 37 ]  . 
this finding disappeared without any intervention and no abnormality was present at birth [ 38 ]  . finally , our study revealed that mri can confirm the us suspicion of esophageal atresia showing the presence of a small stomach and polyhydramnios , although matsuoka demonstrated that mri can also provide several additional findings to us diagnosis of this fetal abnormality [ 39 ]  . there were some limitations in the present study . 
until recently , computed tomography ( ct ) has been the imaging technique of choice in children with cancer , but nowadays there is an increasing interest in the use of functional imaging techniques like positron emission tomography and singlephoton emission tomography . 
these later techniques are often combined with ct allowing for simultaneous acquisition of image data on the biological behaviour of tumour , as well as the anatomical localisation and extent of tumour spread . 
because of the small but not negligible risk of radiation induced secondary cancers and the significantly improved overall survival rates of children with cancer , there is an increasing interest in the use of alternative imaging techniques that do not use ionising radiation . 
magnetic resonance imaging ( mri ) is a radiation - free imaging tool that allows for acquiring images with a high spatial resolution and excellent soft tissue contrast throughout the body . 
 moreover , recent technological advances have resulted in fast diagnostic sequences for whole - body mr imaging ( wb - mri ) , including functional techniques such as diffusion weighted imaging . 
box 85500 , 3508 ga utrecht , the netherlands keywords mri whole - body imaging dwi paediatric oncology introduction the recent technical developments in computed tomography ( ct ) , magnetic resonance imaging ( mri ) and nuclear medicine have changed the role of imaging in the evaluation of children with cancer revolutionary [ 1 , 2 ]  . 
the functional imaging techniques that play a central role in paediatric cancer imaging include positron emission tomography ( pet ) using the radiotracer [ 18f ] - 2 - fluoro - 2 - deoxy - d - glucose ( fdg ) , and single - photon emission computed tomography ( spect ) using the radiotracer iodine - 123 metaiodobenzylguanidine ( i - 123 mibg )  . 
this small but not negligible health risk is of particular concern in children as their tissues are more radiosensitive than adults and they have more years ahead in which cancerous changes might occur . 
that is why there 1 3 radiol med ( 2016 ) 121 : 442453 is an increasing interest in the use of alternative imaging techniques that do not use ionising radiation , such as ultrasonography ( us ) and mri [ 1 ]  . although us is a child - friendly imaging technique that can provide real - time detailed images of most body parts , it is less useful for the evaluation of large masses , extended disease , deeper - lying tissues , and tissues located behind bones and air - containing tissues . 
on the other hand , with mri it is possible to acquire images with a high spatial resolution and excellent soft tissue contrast throughout the body , which makes it an ideal radiation - free tool for the detection of pathology , especially in parenchymal and bone marrow locations . 
moreover , recent technological advances have resulted in fast diagnostic sequences for whole - body mr imaging ( wb - mri ) , including functional techniques such as diffusion weighted imaging ( dwi ) [ 310 ]  . 
this review will focus on the current status of the technique and major clinical applications of wb - mri in children with cancer . technique until now , there is no standardised technique or protocol for performing wb - mri [ 3 , 6 ]  . 
it usually involves imaging of the entire body ( from vertex to toes ) but in oncology , it is often restricted to the skull or skull base to groin region in line with most hybrid imaging techniques . 
most modern mri scanners are equipped with a moving table top for sequential movement of the patient through the magnet during imaging without the need for repositioning . regarding the choice of coils , the use of phased - array surface coils is preferred over the use of the quadrature body coil integrated in the magnet bore , because of the better spatial resolution and signal - to - noise ratio ( snr ) of the first over the latter . 
one approach , the so - called sliding table and repositioning surface coil approach , uses tabletop spacers to place an additional table platform on the original mr table allowing manipulation of the lower part of a non - integrated phased - array surface coil without repositioning the patient [ 15 ]  . 
however , nowadays , on several modern mri scanners dedicated multichannel surface coil systems are available allowing for whole - body imaging without the need to reposition the coil at each station [ 6 ]  . sequences that are typically used in wb - mri include short tau inversion recovery ( stir ) , t1 - weighted fast spin echo ( fse , tse ) , and contrast material - enhanced ( ce ) t1 - weighted three - dimensional gradient echo ( vibe , thrive , lava ) sequences . 
stir is the most commonly used sequence in wb - mri because most pathologic tissues are proton rich with prolonged t1 and t2 relaxation times resulting in high signal intensity on stir images . 
furthermore , it facilitates the combination of better local tumour staging and evaluation of metastatic disease . with the introduction of diffusion - weighted wholebody imaging with background body signal suppression ( dwibs ) in 2004 by takahara et al . , it became possible to perform whole - body dwi under free breathing within a clinically acceptable examination time [ 5 , 7 , 16 , 17 ]  . 
to improve lesion conspicuity high b - values of up to 1000 s / mm2 are applied and either a stir pre - pulse or a frequency selective ( chemical shift selective , chess ) pre - pulse is used for fat suppression to optimise background body signal suppression . 
the choice of the method of fat suppression may depend on the organ / body region under examination , although stir usually results in the most robust fat suppression over an extended field of view , in particular in the neck / shoulder region and lower extremities . 
in case quantitative measurements of the diffusivity ( apparent diffusion coefficient , adc ) in pathological tissues are required , the use of at least three b - values is recommended ( including b0 )  . the choice of scan plane will depend on the region of interest , type of malignancy , and diagnostic information required for optimal treatment planning and followup . 
the 3d ce t1 - weighted gre and dwibs sequences are usually acquired in the axial plane , but the obtained images can be easily post - processed for multiplanar reconstruction ( mpr ) and maximum intensity projection ( mip )  . 
the anatomical imaging of thorax and abdomen 1 3 table 1 wb - mri protocollymphoma ( 1.5t , ingenia , philips healthcare , best , the netherlands ) 444 parameter repetition time ( ms ) echo time ( ms ) inversion time ( ms ) receiver bandwidth ( hz ) slice orientation slice thickness ( mm ) slice gap ( mm ) no . 
this is especially relevant if the abdomen is the site or predisposed area of the ( known or suspected ) primary malignancy . in tables 1 and 2 examples are given of two different wb - mri protocols used in our centre for paediatric oncological indications . clinical applications bone marrow imaging bone marrow has three primary components : osseous matrix , red marrow and yellow marrow . 
shortly after birth , the transition to yellow bone marrow occurs at an orderly and predictable sequence , which begins in the peripheral bones and progresses in a symmetrical manner to the central skeleton . 
in the first decade of life the vertebral marrow is predominantly haematopoietic except for some yellow bone marrow around the central vertebral vein [ 18 ]  . mri is a sensitive method for assessing bone marrow ; however , it lacks specificity . 
 especially in young patients it can be challenging to detect bone marrow disease , because the high cellularity of normal red marrow can be misdiagnosed as diffuse bone marrow infiltration or mask tumour deposits . 
chemical shift imaging ( oppose phase imaging ) could be used as a complementary tool in order to differentiate between malignant bone marrow infiltration and normal red marrow by detecting small quantities of fat . 
previous studies have shown that chemical shift imaging allows distinction between benign and malignant causes in adult patients [ 19 , 20 ]  . dwi in assessment of bone marrow disease is , especially in young patients , of limited value , as the high cellular haematopoietic marrow will exhibit impeded diffusion . 
they found that homogenous low t1 signal had the highest sensitivity ( 88 % ) , whereas a heterogeneous pattern on the post - gadolinium was highly specific ( 97 % ) , but relatively insensitive ( 65 % ) for detecting metastasis . malignant lymphoma lymphoma [ hodgkin disease ( hd ) and non - hodgkin lymphoma ( nhl ) ] is the third most common form of malignancy in children , after leukaemia and brain tumours [ 23 ]  . 
paediatric lymphomas are staged using the modified ann arbor and murphy classifications for hd and nhl , respectively [ 24 , 25 ]  . current guidelines encourage the use of fdg - pet / ct in staging and response assessment of fdg - avid lymphomas [ 24 ]  . 
 [ 27 ] reported very good agreement between wb - mri compared to an fdg - pet / ct reference standard for nodal and extranodal disease , despite only using stir for whole - body imaging . there is an increased interest for the use of dwi in lymphoma due to the clear visualisation of the lymphoid tissue with dwi that is thought to increase the detection rate while decrease reading time . 
an important issue with dwi is that several normal extranodal structures ( including brain , salivary glands , waldeyer ring , thymus , spleen , gallbladder , adrenal glands , prostate , testes , penis , endometrium , ovaries , spinal cord , peripheral nerves and bone marrow ) may demonstrate impeded diffusion . 
 this better detection of lymphomatous involvement in the reticuloendothelial system ( res ) depends on the uptake of uspio through macrophages in the non - involved res and the non - uptake by metastatic tumour deposits . assessment of response to therapy is important for determining treatment effectiveness and predicting clinical outcome . 
a the image of a 3 - year - old girl with proven bone marrow involvement illustrate the diffuse low signal intensity of the bone marrow of the spine compared to the intervertebral disk that is suggestive for diffuse bone marrow infiltration , whereas normal hematopoietic bone marrow is slightly hyperintense to the intervertebral discs of the spine at t1 weighted imaging . 
c transverse t2 - w image demonstrates the intraspinal extension with spinal cord compression ( arrow , see also the arrow in b ) as well as the vascular encasement and the lifting of the aorta ( arrowheads ) that is considered one of the key imaging features of neuroblastoma 1 3 447 radiol med ( 2016 ) 121 : 442453 fig . 
2 coronal whole - body short tau inversion - recovery ( a ) , t1 - w ( b ) and maximum intensity projection greyscale inverted diffusion - weighted ( c ) images of a 12 - year - old boy with anaplastic large cell lymphoma illustrate nodal involvement at both sides of the diagram ( arrows ) and an enlarged spleen ( splenic index 763 cm3 ) indicating splenic involvement diagnosed with whole - body mri . 
the paraaortal and left parailiacal involvement as illustrated at the diffusion - weighted image is not seen at the coronal stir and t1 - w images as this area was not included in these slices with fdg - pet / ct in lymphoma has received considerable attention last years , however it is still not officially recommended outside clinical trails [ 24 ]  . 
 [ 31 ] recently published their results of their prospective study in 64 adult lymphoma patients that showed that wb - mri with dwi could serve as a feasible alternative for fdg - pet / ct during follow - up and treatment response assessment . 
several , mostly pilot , studies compared the quantitative data from fdg - pet / ct ( suv ) with dwi ( adc values ) for interim response assessment with inconclusive results . 
 they reported presence or absence of an inverse correlation between adc and suv [ 3235 ]  . although fdg - pet / ct is the imaging technique of choice for treatment response assessment , the value of interim and end - of - treatment fdg - pet / ct in predicting outcome was demonstrated to be unsatisfactory by recent meta - analyses [ 36 , 37 ]  . 
therefore , prospective studies that correlate dwi results with patient outcome measures instead of fdg - pet / ct will provide reliable evidence . histiocytosis langerhans cell histiocytosis ( lch ) is a rare disease that is characterised by lesions that include cd207 dendritic cells with phenotypic similarity to epidermal langerhans cells on a background of inflammatory cells [ 38 ]  . 
for prognostic purposes , patients are usually divided into a clinical high - risk versus lowrisk group , based on the presence or absence of liver , spleen and / or bone marrow involvement . 
high - risk lch patients have a > 85 % long - term survival rate , whereas the survival rate of low - risk lch patients approaches 100 % . adequate staging at diagnosis is essential , not only for determining prognosis , but also for choice of therapy , as lesions in more than one site usually impact the need for systemic chemotherapy . 
bone scintigraphy has been used for the evaluation of lch , and although lesion detection is usually higher when compared to the skeletal survey , the scintigraphic appearance of lch may vary especially when the lesions are small or fail to incite a significant osteoblastic response [ 39 , 40 ]  . 
 axial proton density weighted image ( a ) , t2 - weighted image ( b ) , and sagittal t1 - weighted images before ( c ) and after the administration of intravenous contrast material ( d )  . 
 after contrast material administration there is a predominantly peripheral enhancement pattern , less often seen in lch lesions ( arrow in d ) reported , and several recent studies have shown high sensitivity and specificity of this imaging technique superior to the skeletal survey and bone scintigraphy [ 41 ]  . 
additional skeletal lesions were identified by wb - mri in 3 out of 8 patients compared with plain radiography ( 38 % ) , and in 2 out of 8 patients compared with scintigraphy ( 25 % )  . 
4 a 7 - year - old girl with langerhans cell histiocytosis ( lch ) presenting with back pa sagittal t2 - weighted ( a ) , stir ( b ) , t1 - weighted ( c ) , and contrast - enhanced fat saturated t1 - weighted ( d ) images of the spine showing involvement of multiple vertebral bodies ( small arrows ) as well as a vertebra plana at the level of th3 ( large arrow )  . 
interestingly , a combined analysis of pet and mri decreased the number of false - negative findings at primary staging , whereas no advantage over pet alone was seen in terms of false - positive or false - negative results during follow - up . neuroblastoma neuroblastoma ( nbl ) is the most common solid extra - cranial tumour in children and infants . 
nbl is an embryonic tumour arising from primordial neural crest cells that are the precursors of the sympathetic nervous syste the most common site of the primary tumour is within the abdomen ( the adrenal medulla in 35 % ) , but it can occur anywhere along the sympathetic chain from neck to pelvis [ 44 ]  . 
some tumours behave aggressively , while others , often in the younger age group , may spontaneously regress [ 44 ]  . ninety percentage of patients are diagnosed before the age of 6 , with a peak incidence around 23 years [ 44 ]  . 
some tumours produce hormones that can cause high blood pressure , increased heart rate , flushing or diarrhoea . since 1986 , the international neuroblastoma staging system ( inss ) has been used as a post - surgical staging syste in 2009 a new staging system was published [ the international neuroblastoma risk group staging system ( inrgss ) ] , shifting focus to pre - treatment staging with identification of imaging defined risk factors ( idrf ) [ 45 ]  . 
 these idrfs describe the relationship between the tumour and adjacent structures that ideally should not be injured during surgery ( i.e. , major vascular encasement , airway compression or cns infiltration )  . the combination of nuclear medicine and radiological examinations are crucial for accurate staging , defining resectability and follow - up during treatment . 
besides , there was a considerable overlap in adc values between these groups . cancer predisposition syndromes wb - mri is a promising imaging tool in the evaluation of genetic cancer predisposition syndromes ( cps ) , especially because of its lack of ionising radiation [ 48 , 49 ]  . 
children with cps ( including neurofibromatosis type 1 , beckwithwiedemann , multiple endocrine neoplasia , li - fraumeni , von hippel - lindau , and rhabdoid tumour syndrome ) are at a significantly increased risk of developing cancer , but when and in which organs tumours will develop is difficult to predict . 
several publications already did mention the use of wb - mri as a screenings method in cps , but studies on the performance of this technique in children is scarce . 
 another recent ( retrospective ) study , which included 50 wb - mri examinations in 24 children with genetic cps , did show that wb - mri is a valuable screening tool with a high sensitivity of 100 % ( 95 % ci 6100 % ) , specificity of 94 % ( 8298 % ) , and negative predictive value of 94 % ( 90100 % ) [ 49 ]  . 
of the 4 highto moderate - risk lesions , only one lesion appeared to be malignant resulting in a positive predictive value of only 25 % ( 95 % ci 178 % )  . 
the other lesions and all low - risk lesions had a benign orig of interest , this study did also show that incidental findings were detected in 23 of 24 patients , most of which did not require imaging follow - up . 
 both studies conclude that , although wb - mri can be regarded as a valuable screening tool , larger cohort studies are needed to validate its role and cost - effectiveness in this specific group of patients . 
 [ 49 ] recommend that interpretation of these studies should be reserved to radiologists that are familiar with wb - mri to appropriately risk stratify abnormalities and minimise unnecessary interventions . future perspectives in children , the choice of imaging modality is driven mainly by reducing the radiation dose as much as possible . 
as illustrated in this review , wbmri is already widely used in paediatric oncology , despite the fact that validation of the technique is mainly based on retrospective data in relatively small patient groups . 
there is a strong need for large prospective cohort studies to better validate the role and cost - effectiveness of wb - mri in children with cancer , both for diagnosis as well as therapy response assessment . 
however , due to the comparatively low incidence of most paediatric malignancies , most institutions will not have sufficient patient volume to perform clinical trials that will result in definitive and statistically significant data . 
this obviates the need for increasing international multi - institutional collaboration and set up of multicentre clinical trials [ 50 ]  . in oncology , the role of imaging is moving from structural ( anatomic ) imaging to combined structural and functional ( molecular ) imaging , enabling better tumour characterization , prognostication , response assessment , and prediction of outcome of therapy . 
that is why research on wb - mri in children not only should focus on further optimization of anatomic sequences ( including reduction of scan duration ) but also on the introduction and validation of new functional techniques . 
 magnetic resonance spectroscopy ( mrs ) allows for a noninvasive separation of the mri signal from a given tissue 1 3 451 radiol med ( 2016 ) 121 : 442453 fig . 
coronal acquired 3d t2 - weighted image ( a ) with axial reconstruction ( c ) demonstrates the primary tumour arising from the left adrenal gland ( arrows ) with compression upon the left kidney , vascular encasement and lifting of the aorta ( arrowhead )  . 
there is diffusion restriction seen as high signal at the b1000 image ( d ) with corresponding low signal at the adc map ( e ) 1 3 452 radiol med ( 2016 ) 121 : 442453 into its different chemical components , which may improve lesion characterization and prediction of clinical outcome . 
in this scope , the recent development of integrated pet / mri systems is very interesting , combining the superior structural imaging of mri with the functional ( molecular ) information of both imaging techniques while decreasing the radiation dose . 
although the first publications in children show promising results , it currently remains a technical challenge to construct and use these hybrid systems [ 5153 ]  . conclusion wb - mri is a very promising and already widely used imaging technique in paediatric oncology . 
owens1 received : 30 september 2015 / accepted : 27 october 2015 / published online : 20 november 2015 italian society of medical radiology 2015 abstract diffuse interstitial lung disease in children differs markedly from interstitial lung disease in adults and is a distinct entity . 
the childhood interstitial lung disease ( child ) classification , devised in 2010 separates conditions into those occurring in infancy , and those not specific to infants , the later group containing many conditions related to systemic diseases ( including connective tissue diseases and depositional / storage disorders ) , and conditions occurring in immunocompromised children . 
we illustrate this with cases from our institution and emphasize the more recently recognised conditions including pleuroparenchymal fibroelastosis and filamin a deficiency - related lung disease . keywords childhood interstitial lung disease paediatric ct diffuse lung disease pleuroparenchymal fibroelastosis filamin a deficiency - related lung disease introduction diffuse interstitial lung disease ( dild ) represents a heterogeneous group of disorders characterised clinically by * catherine m . 
as these diseases occur in children with ongoing development and maturation of the lungs and immune system , the clinical presentation and disease progression is modified by comparison with fully mature adult equivalents [ 1 ]  . 
thus , dild often differs markedly in presentation , clinical features , and progression from interstitial lung disease ( ild ) in adults , and it is inappropriate to extrapolate from adults to children . 
it is important to understand the normal growth and development of the lungs in children so as to understand the development of ild [ 2 ]  . normal growth and development of the lung and immune system ild may present soon after birth , suggesting an antenatal onset in some cases . 
the mature airway pattern is determined by week 16 of gestation [ 3 ] and is driven by growth factors produced by mesenchyme and extracellular matrix ( including fibronectin , tenascin , the integrins , syndecans , and cadherins ) , and epimorphin and the epidermal platelet - derived and insulin - like growth factors [ 4 , 5 ]  . 
thus , ild and its treatment , particularly 1 3 radiol med ( 2016 ) 121 : 352361 early in life , may profoundly affect long - term pulmonary function . setting , at a width of 1500 hounsfield units ( hu ) and at a level of 500 hu . the immune system is immature at birth and the immune - pathogenesis of ild , therefore , is different in children compared to adults . 
the pattern of cytokine secretion is variable : levels of production of interleukin 2 ( il - 2 ) are controversial [ 12 ] , but secretion of il - 4 and interferon - gamma is markedly reduced [ 13 ]  . b - cell function is reduced , and whether this is intrinsic or secondary to reduced t cell function is unclear . 
peripheral blood monocyte function , by contrast , seems relatively mature , although alveolar macrophages appear to be functionally deficient [ 14 ]  . morbidity and mortality associated with paediatric ild are high ( range 1439 % ) with a higher mortality in younger infants . the diagnosis may be delayed , but once suspected , the aim is to confirm the presence and severity of ild , to uncover any predisposing factors and identify the dominant pathology of the ild . although it is sometimes possible to make a diagnosis without biopsy , the majority of patients will require histological studies using either open lung biopsy , video - assisted thoracoscopic ( vats ) biopsy or high - resolution computed tomography ( hrct ) - guided percutaneous biopsy . the general classification includes disorders of known aetiology ( aspiration , chronic infection , hyper - sensitivity pneumonitis , lipid storage diseases ) , unknown primary pulmonary disorders or systemic disorders with pulmonary involvement , and finally those diseases unique to childhood . ct technique because the chest radiograph is often non - specific , and relatively insensitive , thin section ct has been shown in adults and children to increase the accuracy at diagnosis of diffuse lung disease . the trade - off in sensitivity and specificity of hrct over chest radiography is related to radiation dose , which is significantly higher with conventional spiral or volumetric ct . 
however , the use of low - dose ( 50 ma , 0.75 s ) limited ( 1 - mm slices interspaced every 1520 mm ) hrct in inspiration , with three supplementary expiratory scans ( when small airways disease may be present ) allows accurate assessment of the presence and the extent of diffuse lung disease at a dose equivalent to approximately ten chest radiographs [ 15 ]  . 
images are reconstructed on a high spatial resolution algorithm and displayed with a wide window if a child is unable to breath - hold , the scans can be performed during quiet breathing , and decubitus scans can replace expiratory scans ( the dependent lung behaving as the expiratory lung ) when air trapping is thought to be possible clinically . in more recent years with the rapid advances in temporal resolution and dose saving measures , spiral acquisition of contiguous volumetric data has become easy , efficient and reproducible with excellent spatial resolution and image quality . 
this can be acquired at ultralow doses with the newest scan technology , with superb image quality even at sub - millisievert effective doses , even in small infants with high heart and respiratory rates . 
ultrafast spiral acquisition allows high quality mediastinal and lung parenchymal datasets to be obtained , facilitating the use of sophisticated post processing techniques to be incorporated into diagnostic pathways for all children . the role of chest ct in paediatric ild is evolving . 
the histospecific accuracy of hrct compared with chest radiographs in making a correct first - choice diagnosis in an adult population with diffuse lung disease ranges from 46 to 75 % for hrct and from 38 to 63 % for chest radiography [ 1618 ]  . 
a correct first - choice diagnosis was made in 61 % of the cases on hrct compared with 34 % on chest radiographs . in children , the diseases that were correctly diagnosed on ct with a high degree of confidence were alveolar proteinosis , pulmonary lymphangiectasia and idiopathic pulmonary haemosiderosis . 
differentiation between nonspecific interstitial pneumonitis ( nsip ) , desquamative interstitial pneumonitis ( dip ) and lymphocytic interstitial pneumonitis ( lip ) was , however , less reliable . there are several pitfalls in the interpretation of hrct in children . 
deciding on whether the areas of decreased attenuation represent , for example , small airways disease , or 1 3 354 radiol med ( 2016 ) 121 : 352361 the areas of increased attenuation ( ground glass opacity ) represent diffuse infiltration can be challenging . 
use of lateral decubitus imaging ct with the dependent lung simulating expiration may be helpful . ct features of diffuse interstitial lung disease in children idiopathic interstitial pneumonitis non - specific interstitial pneumonia ( nsip ) , desquamative interstitial pneumonia ( dip ) and lymphocytic interstitial pneumonitis ( lip ) in childhood appear to share common ct appearances . 
there are no unique discriminating features for the radiological appearances of dip , which includes widespread ground glass opacification and has a wide differential including sub acute extrinsic allergic alveolitis , opportunistic infections such as pneumocystis jirovecii pneumonia and sarcoidosiswhich is very rare in children . 
 ground glass opacification is the dominant ct pattern and often has a lower zone predominance . however , the few reported cases of childhood nsip appear to have a distinct pattern of involvement . 
in a review of cts of six cases of biopsy - proven nsip , a distinct upper zone predominance of honeycomb pattern with parenchymal distortion on a background of diffuse ground glass opacification was seen in three children [ 22 ]  . 
 [ 20 ] , one case of dip resembled nsip with predominant upper lobe involvement . the existence of uip ( usual interstitial pneumonitis ) in childhood is controversial and said to be vanishingly rare . lip is a condition characterised histologically by a diffuse interstitial infiltrate of polyclonal lymphocytes , plasma cells and histiocytes . 
1 extensive centrilobular and randomly scattered nodules in a child with vertically acquired hiv and known lip autoimmune diseases and lymphoproliferative disease secondary to underlying congenital immunodeficiency . chest radiographs show reticulonodular change with or without areas of consolidation . 
there is usually marked resolution of the striking radiological appearances with therapy for hiv disease ; however , if there has been chronic interstitial disease , fibrosis and ensuing traction bronchiectasis may result . follicular bronchiolitis is a term coined to described a form of lip where the lymphoid aggregates congregate around the small airways . chronic pneumonitis of infancy ( cpi ) is a recently described pathological entity and its ct appearances have been reported in a single biopsy - proven case . 
aspiration pneumonitis secondary to abnormal oesophageal peristalsis may result in acute and chronic parenchymal change with bronchiectasis / bronchiolectasis . sle - induced vasculitis manifests as patchy areas of ground glass attenuation . 
these conditions are inherited in an autosomal recessive manner and , when severe , can present in the neonatal period with clinical and radiological features otherwise indistinguishable from hyaline membrane disease ( hmd )  . the differential diagnoses ( with very similar features ) include congenital viral infections . 
the more recently described chronic pneumonitis of infancy ( cpi ) is characterised by alveolar septal thickening , alveolar pneumocyte hypoplasia and an alveolar exudate , containing macrophages and cellular debris , which also has similar appearances . the later secondary form of pap usually occurs between a few months and several years of age [ 24 ]  . 
the ct appearances of lymphangiomatosis can be easily predicted knowing the anatomical distribution of the lymphatic system within the lungs , with smooth thickening of the interlobular septa , peribronchial thickening , patchy ground glass opacification and increased attenuation of the mediastinal fat with bilateral pleural effusions and pleural thickening [ 25 ]  . 
the childhood form of iph usually presents before the age of 3 years with no specific gender prevalence [ 27 ]  . on hrct , acute haemorrhage is characterised by ground glass opacification or consolidation . 
 there appear to be two distinct types of sarcoidosis in children [ 28 , 29 ] with the majority presenting at 1315 years of age with a multi - system disease inseparable from the adult type . 
lymphadenopathy and pulmonary involvement are common with systemic symptoms of fever and malaise , and ct appearances are identical to adult disease . 1 3 356 radiol med ( 2016 ) 121 : 352361 fig . 
the radiograph c demonstrates diffuse bilateral ground glass opacification , as seen in hyaline membrane disease of prematurity , but in a term neonate not responsive to exogenous surfactant treatment . 
the histology demonstrates a dilated ectatic lymphatic channel ( c ) in contrast , children under 4 years of age [ 28 , 29 ] present with a distinct systemic form of the disease characterised by rash , uveitis and arthritis / tenosynovitis . 
although pulmonary involvement has been reported , it is very rare in young patients . phase , diffuse ground glass shadowing is seen in the lungs with small , poorly defined centrilobular nodules [ 30 , 31 ]  . 
in the chronic phase , interstitial fibrosis supervenes [ 33 ]  . extrinsic allergic alveolitis langerhans cell histiocytosis extrinsic allergic alveolitis ( hypersensitivity pneumonitis ) is uncommon in children and is due to an immunological response to a variety of inhaled allergens . 
in the infant , recurrent episodes of unexplained respiratory distress related to feeding with perihilar consolidation , especially in the dependent right upper and / or superior segments of the lower lobes should make one consider aspiration fig . 
ct demonstrates mosaic attenuation with smooth interlobular septal thickening ( circled in b ) , dilatation of the pulmonary arterial trunk ( c ) and peripheral plexiform lesions ( circled in e ) with surrounding ground glass representing cholesterol granulomata . 
the cxr shows enlarged pulmonary arteries , kerley b lines , pleural effusions and mediastinal lymphadenopathy . ct demonstrates pulmonary arterial enlargement , mediastinal lymphadenopathy and normal main pulmonary veins but shows smooth interlobular septal thickening due to peripheral pulmonary venous congestion . 
the purpose of this narrative overview is to provide a useful educational tool in daily clinical practice for radiologists with a broad perspective of csvt including a discussion of more common potential pitfalls related to misinterpretation of images in children . 
this paper will also review the normal venous anatomy , its variants , risk factors that contribute to cause csvt ( neonates with their specific causes of csvt are not included in this review ) and the practical imaging feature of cerebral sinovenous thrombosis on mri and ct . 
finally , a brief overview of frequent and severe csvt conditions in children with key points in imaging is shown . keywords cerebral sinovenous thrombosis children ct venography mr venography tof * chiara carducci chiara1.carducci@opbg.net giovanna stefania colafati gstefania.colafati@opbg.net 1 neuroradiology unit , department of imaging , bambino ges childrens hospital irccs , rome , italy introduction cerebral sinovenous thrombosis ( csvt ) is a cerebrovascular disease , relatively rare and potentially life - threatening in children , yet underestimated . 
other authors have reported a similar high proportion in this age range [ 4 , 5 ]  . the data from the italian registry of childhood thrombosis are in substantial agreement with the recent literature , analyzing a pediatric population ranging between the 29th day of postnatal life and 18 years of age , presenting acute onset of headache , seizure , lethargy or focal neurological deficit . 
in this italian group only two patients ( 2 / 66 csvt events ) died , one death was related to the thrombotic event , and the other to infectious complications of transplant . 
one or more neurological deficits were reported at discharge in 28.33 % csvt events [ 6 ]  . the clinical onset is non - specific and may be subtle , depending on patient age , extent , location , and acuity of csvt . 1 3 table 1 the clinical onset in case of csvt reported by suppiej et al more common clinical onset less common clinical onset 330 headache lethargy seizure papilloedema diplopia strabism hemiparesis coma ataxia anisocoria tetraparesis dystonia speech disturbance cranial nerve palsy diffuse or focal neurological abnormalities in childhood , the clinician should consider csvt diagnosis in a wide range of acute neurological settings , even if the more frequent clinical onset in children are seizure and focal signs and symptoms of increased intracranial pressure [ 2 , 7 ]  . 
other authors include frequent irritability , headache , seizure , encephalopathy , onset papilledema , cranial nerve palsies , motor weakness and coma [ 2 , 7 ]  . due to the persistence of the underlying diseases , the reappearance of conditions inducing thrombosis or the onset of new risk factors may cause csvt to relapse . transverse sinus thrombosis is the most common single csvt . 
multiple sinuses are involved in more than 70 % of patients [ 4 ] and are particularly found in the contiguous transverse and sigmoid sinuses . hedlund adds bacterial meningitis and iron deficiency anemia to the more known local and systemic causes of sinus venous thrombosis like trauma and dehydration [ 2 ]  . in this clinical setting , the associated brain parenchymal injury can vary in a spectrum of findings including vasogenic and cytotoxic edema and hemorrhagic venous infarction . the clinical outcome of the parenchymal associated lesions may include one or more neurological deficits . 
 even post - thrombotic complications such as hydrocephalus and papilledema , may cause long - term morbidity [ 2 , 4 , 79 ]  . due to the non - specific and often subtle clinical onset , the wide spectrum of cause factors and clinical manifestations , neuroradiological imaging of csvt is essential to reach the diagnosis ; due to this reason , the improvement of imaging techniques plays an important role to detect and define most cases of csvt . radiol med ( 2016 ) 121 : 329341 the aim of this narrative overview is to present a broad perspective on the topic , pull many pieces of information together , and provide a useful educational source for radiologists in case of pediatric csvt . 
to provide a context for the discussion of abnormal findings , the normal venous anatomy and variants are also revised , and potential pitfalls related to misinterpretation of images are described . normal sinus venous anatomy the cerebral venous system has two major compartments : the dural venous sinuses and the cerebral veins . the dural venous sinuses are the major drainage pathway of the cerebral veins . 
1 2d tof dural venous sinuses anatomy : superior sagittal sinus ( sss ) , inferior sagittal sinus ( iss ) , straight sinus ( ss ) , sinus confluence ( torcular ) , transverse sinuses ( tss ) , sigmoid sinuses and giugular bulbs fig . 
a axial and b sagittal reformatted ct images show increased attenuation in the transverse dural sinuses ( arrows ) inflammation or infection may have a prothrombotic tendency that becomes clinically evident due to extension of the inflammatory state from the bone to the sinus wall [ 17 ]  . more than one risk factor predisposing the patient to csvt may be present ; consequently , even if a causative factor is detected , a blood screening for thrombophilic and / or prothrombotic conditions should be always performed . 
 in fact , in case of a prothrombotic condition , the patients family should be advised that prompt administration of anticoagulant could be necessary in all clinical events predisposing thrombosis . neuroradiological techniques the neuroradiological evaluation is crucial in the early detection of csvt and the improvement in imaging techniques is playing an important role in identifying venous thrombosis , secondary brain damage and in some conditions it can even help to identify the causes of cerebral sinus thrombosis . in past decades , digital subtraction angiography ( dsa ) , an invasive technique with considerable risks , was the diagnostic gold standard ; nowadays it is not performed and has been almost completely substituted by mri , magnetic resonance venography ( mrv ) , ct , and ct angiography . 
a axial and b sagittal images show a normal elevated attenuation of the dural sinuses due to the relative polycythemia at this age and to the hypodensity of the adjacent immature brain for incomplete myelination ( arrows ) fig . 
a , b axial images show a focal distention and hyperdensity of superior sagittal sinus and an increased attenuation of cortical veins ( cord sign ) all findings on unenhanced ct ( table 2 ) , including the hyperdense venous sinus , are often subtle and non - specific in the early stages . 
 [ 20 ] evaluate the density ( hounsfield units ) of cerebral venous sinuses on unenhanced ct in patients with csvt , comparing these results with a large matched control group without csvt , to verify if this could be considered a useful and quite objective additional diagnostic tool . 
their results show a wide range of hu in the sinuses of the control group ; moreover the hu measurement of an old thrombus may show a low density and mislead . 
furthermore , the authors highlight that sample groups were not sufficient to use this method to increase the cvst diagnostic confidence . the hyperdense appearance of a thrombus on unenhanced ct usually disappears in 7 days , but may be present longer in case of larger clots . 
in the acute stage , the hyper dense clot may result in false - negative on contrastenhanced ct ( cect ) if a density difference between the clot and the empty enhanced sinus is not noted . 
the previous unenhanced ct may help the diagnosis , showing a natural hyperdensity corresponding to the clot that will became less hyperdense compare to the sinus on cect . 1 3 radiol med ( 2016 ) 121 : 329341 table 2 direct and indirect signs on unenhanced and contrast - enhanced ct indirect signs direct signs unenhanced ct sign hyperattenuating thrombus in the partial or totally occluded sinus / cord focal distension of the dural venous compartment occluded pial veins as linear hyper - attenuation on the brain surface , hemorrhagic parenchymal infarction in the drainage area of obstructed flowing into the dural sinus vein / sinus contrastenhanced ct direct visualization of thrombosed sinus as relatively hypodense and surrounded by contrast - enhanced dural wall and collateral venous channels ectasia / tortuosity of the vein proximal to involved sinus empty delta sign ( central intraluminal filling defect , caused by enhancing dura surrounding non enhancing thrombus ) [ 2 , 22 ] the thrombus changes signal intensity according to the interval between its appearance and the time of mr imaging [ 1 , 24 , 25 ]  . 
these changes on t1and t2 - weighted mri are related to the paramagnetic effects of the products of the hemoglobin breakdown . acute stage ( 03 days ) : thrombus predominantly isointense on t1w images and hypointense on t2w images ( deoxyhemoglobin in red blood cells trapped in the thrombus )  . 
 at this stage the thrombus detection is easier , due to the more abnormal signal of the sinus . chronic stage ( > 15 days ) : incomplete recanalization of the sinus with the thrombus isointense / hyperintense on t2w images and isointense on t1 - weighted sequence . 
the heterogeneity of mr signal intensity of chronic thrombus may mimic normal slow - moving venous blood [ 2 , 29 ]  . to confirm the diagnosis and better define a csvt , a 3d ultrafast gradient enhanced t1 weighted sequence ( 3d - mprage , 3d - spgr , 3d - tfe ) with and without contrast media is strongly suggested , allowing excellent visualization of dural sinuses on multiplanar reconstructions and mrv . to improve diagnostic accuracy in case of partial thrombosis or chronic stage , t2 * gradient - echo ( gre ) and / or susceptibility - weighted imaging ( swi ) sequences can be considered as part of the mri protocol [ 2 , 3032 ]  . 
axial image documented triangular - shaped central intraluminal filling defect at superior sagittal sinus ( arrows ) , due to an enhancing dura surrounding non enhancing thrombus magnetic resonance imaging ( mri ) unenhanced mri is more sensitive for the detection of venous thrombi than unenhanced ct [ 2 ]  . 
the absence inside the sinus of the flow void effect on t2 weighted images ( t2wi ) and the hyperintensity on t1 weighed images ( t1wi ) , are direct findings of thrombosis on unenhanced mr imaging [ 1 ]  . 
the appearance of csvt on unenhanced mr is often conditioned by different elements , affecting clot features ( age , location , extension , and patient hydration ) , mr unit and sequences choice . 1 3 radiol med ( 2016 ) 121 : 329341 334 fig . 
 enhanced image ( c ) shows an isointense thrombus compare to the sub - acute phase ( g ) when the thrombus into the sinus and the collateral vein is spontaneously hyperintense . 
f axial tse t1w images show thrombus predominantly hyperintense on t1w and more isointense on t2w images compare to the previous study performed 7 days before phases for an indirect sign : the local cortical and medullary veins dilatation . 
hedlungs recommendation was to not replace gre with swi , although the last shows microbleeds better , because swi shows both the low signal intensity in normal , and clot - containing veins / dural sinus as hypointense structures [ 2 ]  . the brain parenchymal involvement results in edema , often reversible , and subcortical hemorrhagic infarction [ 2 , 33 ]  . the signal coming from blood flow can be coded using various mrv techniques , some of which are without a contrast mediuthe most diffuse are 2 - dimensional time - of - flight ( 2d tof ) [ 16 , 34 , 35 ] and phase - contrast ( pc ) [ 34 ]  . magnetic resonance venography ( mrv ) is widely used and considered as a sensitive imaging technique in the diagnosis of csvt [ 1 ] , nevertheless we believe that it has to be considered as a part of a complete mri evaluation and not as the only sequence to consider . 2d tof is particularly useful in the chronic stage when it continues to demonstrate absence of flow . 
this finding may be a combination of small sinus size , image acquisition plane not perpendicular to the sinus and a slow flow rate . phase - contrast mr venography is based on velocityinduced phaseshifts imparted upon the moving spins to distinguish high signal flowing blood from the suppressed signal of the surrounding stationary tissue . 
advantages of pc versus 2d tof are the absence of the clot / hematoma signal hyperintensity , resulting in background being suppressed , and the possibility to reach a quantitative determination of the flow . 
it is also helpful when contrast medium is contraindicated but it has a longer acquisition time compare to 2d tof . although 2d tof and pc have improved , there are still false negatives , technical artifacts and limitations in the diagnostic evaluation , strongly reduced using contrast media . mrv with contrast media is also useful to depict abnormal collateral channels ( e.g. , enlarged medullary veins )  . the contrast - enhancement mra ( ce - mra ) can be 3d or 4d with a temporal resolution that is not particulary useful in cvst diagnosis [ 34 ]  . the findings obtained with mrv - contrast - enhancement are similar to findings obtained with dsa but with a noninvasive technique . the complementary use of mri and mrv improves test performance to a sensitivity of 100 % [ 16 ]  . 1 3 radiol med ( 2016 ) 121 : 329341 fig . 
d axial se t2wi , e axial enhanced t1wi and f sagittal enhanced 3d ultrafast gradient t1wi , show right posterior temporal lobe herniation ( isointense on t2wi with surrounding hyperintensity of the csf ) into the right transversal sinus ( arrows ) diffusion weighted imaging ( dwi ) dwi is a part of the mr study and has to be routinely used in case of csvt , allowing the early detection of brain edema and secondary parenchymal ischemia and improving the outcome prognosis [ 37 ]  . 
detected , inside large affected sinuses , a high signal on dwi ( low adc ) in 41 % of the mri showing a csvt , in the presence or absence of cerebral lesions . 
the recanalization of occluded vein ( s ) or sinus ( es ) was less frequent when high signal on dwi ( low adc ) was present at the corresponding size of the initial mri . 
although these results are interesting , we believe that nowadays the adc evaluation of the thrombus inside the sinus is not a recommended finding to look for in case of csvt . perfusion imaging perfusion - weighted imaging ( pwi ) is performed by injecting a contrast agent and then obtaining a rapid series of mri images using an ultrafast technique . 
the images track the passage of the contrast agent through the bra this technique can be used to assess cerebral blood flow ( cbf ) and cerebral blood volume ( cbv ) in various brain regions [ 23 ]  . 
the goals of pwi in csvt [ 39 ] are the same of any other clinical condition of abnormal blood circulation but this technique is not included in the routine mri of cvst . arterial spin - labeling ( asl ) perfusion - weighted magnetic resonance imaging is a non - invasive mri technique to measure cbf without administration of contrast mediuthe labeled water in the arterial blood is used as an endogenous medium contrast . 
even if asl is not invasive and can be useful to detect brain areas with low perfusion as well as pwi , it is not considered a routine sequence in case of csvt . pitfalls to obtain the prompt and correct diagnosis of csvt it is mandatory to consider the potential pitfalls , to avoid false - positive / negative . the radiologist has to know the age - related normal appearance of the anatomical structures , its variants and how the normal sinuses appear in the different neuroradiological techniques . 1 3 336 radiol med ( 2016 ) 121 : 329341 fig . 
a axial tse t2w , b axial tse t1 - weighted , and c coronal tse t2w images show a bridging vein ( black arrows ) ending into the subdural clot without drainage into the sinus ( arrow ) fig . 
a axial unenhanced ct image shows an epidural hematoma ( arrow ) , b axial contrast - enhanced ct image with bone windowing reveals a skull fracture ( arrow ) , c axial enhanced ct images shows a sinus compression with filling defect in the right transversal sinus ( arrow head ) , d 3d cta of the some finding . 
eh 7 - year - old girl with head trauma : mastoid fracture with air bubbles ( arrows ) and thrombosis of the sigmoid sinus ( open arrows ) the age of the pediatric patient is important in the evaluation of both ct and mr findings . 
the normal mri flow void of the sinuses is , at the same age , conditioned by several factors : increased turbulence , intraluminal heterogeneity , voxel dephasing and artifactual flow gaps into the sinuses , particularly the superior sagittal sinus . the most common anatomic variants involve the transverse sinuses and are : congenital dominant transverse sinus ( usually the right ) , always associated to a larger jugular foramen compared to the contralateral . hypoplastic transverse sinus , common in the nondominant sinus . 
coronal tse t2w ( d ) , axial enhanced tse t1w images ( ef ) showing sinus thrombosis and cerebellitis the identification of these anatomic variants can be quite simple , when you know them ; more difficult can be the correct attribution of neuroradiological findings mimicking csvt . aracnoid granulations ( ag ) are normal anatomical structures , mostly located in the superior sagittal sinus , torcular herophili and transverse sinuses . 
 axial gre t2 * images ( f , g ) show associated blood hemorrhages , enlarged and likely thrombized cortical veins surrounding csf into the dural venous sinuses and / or calvarium , have a prevalence of 0.32 % on a large group of not selected consecutive brain mr studies [ 40 ]  . 
battal shows that intrasinus brain herniations are generally asymptomatic and incidental , although headache might be an associated symptom . an emergent topic that can mimic csvt , is the real incidence of cortical sinus and venous thrombosis in non accidental head trauma ( naht )  . recent attention has focused on abnormalities of the cerebral venous sinuses and cortical veins in non accidental head trauma and their interpretation has been introduced in legal proceedings as a potential mimic of naht [ 41 ]  . 
in a retrospective study involving all children < 36 months who presented naht and had mri and mrv , found frequent signs of bridging vein injury , such as subdural hemorrhage , cortical vein compression or displacement , and the lollipop sign [ 28 ]  . 
the analysis of clinical features and all mri and mrv findings , interpreted by an experienced pediatric neuroradiologist with knowledge about the limitations and pitfalls of mr venography should allow the appropriate diagnosis of trauma as the etiology of the venous abnormality . a worthy condition is the bridging vein thrombosis ( bvt ) in infants with naht . 
observed a particular bvt shape , the tadpole sign ; an ovaltoround shaped body representing a thrombus within the subarachnoid space and a bent tail reflecting a torn bv expanded by clotted blood . 
13 chronic renal failure in a 7 - year - old - boy axial t1wi unenhanced ( a , b ) , axial t2wi ( c ) , axial ( d , e ) and sagittal ( f ) contrast - enhanced t1wi reveal the thrombosis of the transversal sinus and the inferior portion of the superior sagittal sinus ( arrows ) axial view , but coronal view appeared to be more sensitive for locating and evaluating this condition . technical artifacts are to be considered as potential pitfalls , mimicking intravenous thrombosis . 
to differentiate csvt from adjacent bone skull on non - enhanced ct , it is suggested to use a window wider than that used for brain parenchyma . beam - hardening artifact at the skull base may cause increased attenuation of the adjacent venous structures [ 32 ]  . other less common conditions that can mimic a cvst pattern are : hight hematocrit , diffuse cerebral edema , unmyelinated brain and subdural hematoma . 
gaslini , largo gaslini 5 , 16147 genova , italy in the paediatric population , the technique is used for oncological and non - oncological applications [ 1 ]  . among emerging non - oncological potential applications of wbmri , rheumatological diseases play an important role . rheumatological wbmri applications may include the evaluation of chronic multifocal recurrent osteomyelitis , myopathies , dermatomyositis , fever of unknown origin , arthritis , and connective tissue diseases [ 2 ]  . technical details wbmri is targeted for maximum coverage of the body within the shortest time possible using the minimum number of sequences . 
over the past few years , wbmri has gained increasing application also in paediatrics thanks to the combination of fast sequences and rapid table movement . even if no standardization of the examination technique has been determined , patients are usually scanned in supine position with extended legs and arms , the latter at the sides , and usually head first [ 2 ]  . scanning is performed on coronal planes that enable coverage of larger parts of the body . 
however , as compared to the axial plane scan , the coronal plane has a lower sensitivity [ 5 ] when evaluating some anatomical structures such as the chest cage and the skull [ 3 , 4 ]  . therefore , additional sequences acquired in sagittal plane are necessary for a more accurate evaluation of vertebral spine . wbmri is usually performed with acquisition of one , two , three , or more image sets , depending on the size of the patient and on the region to be scanned . 
the same coil is used , and the slice selection gradients match exactly at each station , making possible automatic direct image realignment after acquisition and thus creating a whole - body 1 3 radiol med ( 2016 ) 121 : 454461 acquisition time usually ranges from 20 to 40 min making sedation seldom necessary . 
 accurate staging is required in oncology to determine the most appropriate method of management , and up - to - date ct scans remain the mainstay imaging modality for this purpose . wbmri is a technique that can now be used on a routine basis and is promising in paediatric oncology . 
its role in respect to nuclear medicine examinations still has not clearly been determined , even though the number of studies demonstrating the similar efficacy of these two methods is constantly increasing [ 10 ]  . 
thus , in some cases , an additional examination of the arms , placed above the head , has to be performed [ 8 ]  . in most centres , baseline sequences include turbo spin - echo ( tse ) t2 - weighted sequences with fat saturation or short inversion recovery ( stir ) and t1 - weighted sequences . in our studies , stir sequences are used . 
t1weighted sequences are also essential , in our experience , in the evaluation of normal bone marrow conversion and in differentiation from bone lesions [ 9 ]  . knowledge and familiarization with areas of hematopoietic bone marrow and fat transformation are extremely important for correct interpretation of wbmri or mri of any region of the body in paediatrics [ 3 , 9 ]  . intravenous gadolinium injection is not recommended [ 1 ]  . 1 3 456 radiol med ( 2016 ) 121 : 454461 fig . 
2 pie chart of the distribution ( total number and percentage ) of the wbmr studies performed in our institute in the period 2010 2015 : a oncological / non - oncological studies ; b rheumatological studies according to different indications ; and c rheumatological / nonrheumatological studies wbmri in dm and pm juvenile dermatomyositis ( jdm ) is a rare multisystem autoimmune disease characterized by chronic inflammation primarily of skeletal muscles and skclinical manifestations consist of typical skin rash , proximal muscle weakness , raised muscle enzymes , myopathic changes on electromyography ( emg ) , and typical muscle biopsy patterns . it represents the most common idiopathic inflammatory myopathy ( iim ) in childhood with an estimated incidence of 23 cases per million children per year [ 1113 ]  . the only validated diagnostic criterion currently used in jdm was described by bohan and peter in the 1970s [ 14 16 ]  . 
according to the bohan and peter criteria , a definite diagnosis is made if a characteristic skin rash is present in combination with three of the four criteria [ 17 ]  . the early diagnosis and aggressive treatment of jdm with steroids and immunosuppressive drugs has dramatically improved the morbidity and mortality of the disease [ 14 , 18 ]  . prompt evaluation of disease activity is fundamental in order to establish therapeutic strategies and avoid permanent disability . 
stir sequences are useful in active jdm , as the increased signal intensity in the affected tissues [ 20 , 21 ] reflects the presence of oedema in these tissues . 
furthermore , wbmri is able to demonstrate flogistic changes of subcutaneous and myofascial tissue , clinically often undetectable [ 11 ] , that are also potential markers of disease severity being associated with a higher burden of muscle inflammation . 
a recent study performed by our group [ 11 ] represents the first application of the wbmri to a series of 41 jdm patients ( 19 boys , 22 girls ; median age 8.8 ) in our experience , this technique allows a more accurate assessment of total inflammatory burden compared to clinical examination as it establishes the distribution and severity of the inflammatory process throughout the whole body . 
3 coronal whole - body short inversion recovery ( stir ) mri obtained at disease onset in an 8 - year - old girl with dermatomyositis showing a typical diffuse muscle inflammation . 
the abnormal hyperintense areas tended to be diffusely and homogeneously distributed within the skeletal muscle , affecting all the muscles throughout the body groups ( 19 / 41 patients )  . 
thus , in our experience , wbmri provides additional information to clinical evaluation and represents a promising tool in estimating total inflammatory burden , tailoring treatment , and monitoring its efficacy . wbmri in crmo chronic recurrent multifocal osteomyelitis ( crmo ) , also known as non - bacterial osteomyelitis or chronic nonbacterial osteomyelitis ( cno ) , is characterized by recurrent flares of inflammatory bone pain related to aseptic osteomyelitis . the term crmo was coined by probst in 1978 [ 2426 ]  . although crmo is considered a benign disease , it can substantially impair quality of life due to persistent symptoms or sequelae ; furthermore , extraarticular manifestations are also described in association with crmo such as fig . 
note diffuse muscular atrophy with fatty replacement of muscle fibres palmoplantar pustulosis , psoriasis , crohns disease , arthritis , fasciitis , and parotitis [ 2729 ]  . by definition , the bone lesions seen in crmo are culture negative and have no demonstrable organism on histopathology . the pathophysiology of crmo remains unknown : some authors classify it as the juvenile form of sapho syndrome ( synovitis , acne , pustulosis , hyperostosis , osteitis ) and others as an autoinflammatory disease . however , recent genetic data suggest that crmo may belong to the large family of autoinflammatory diseases with multifactorial pattern and osseous expression [ majeed syndrome , papa syndrome ( pyogenic sterile arthritis , pyoderma gangrenosum , and acne ) ] , and dira syndrome [ deficiency of the il - 1r antagonist ] [ 3032 ]  . crmo is therefore a diagnosis of exclusion and is established by the clinical presentation , imaging studies , and a culture - negative bone biopsy . 
 images reveal hyperintense areas in distal femoral metaphyses ( thick arrows ) and proximal tibial metaphysis ( thin arrows ) with bilateral talus involvement ( arrowheads ) symptobone lesions tend to cluster around the metaphysis , can occur at atypical locations for bacterial osteomyelitis such as the clavicle , and when multifocal , often have a symmetric distribution . according to literature , 75 % of bone lesions are perimetaphyseal . 
constructed a composite score to improve the management of crmo ; this score was designed to assist in the determination of whether bone biopsy is necessary to confirm the diagnosis in a given patient [ 35 , 36 ]  . we have retrospectively analysed clinical and radiological data in a subgroup of 48 patients ( 33 m , 15 f , median age at onset 9.6 years ) evaluated at istituto giannina gaslini for crmo . 
 in our cohort , the most frequent radiologically involved skeletal segments are spine ( 33 % of total lesions ) and distal tibia ( 14.7 % of total lesions )  . 
wbmri allowed a comprehensive and precise localization of bone sites and soft tissue involvement , thus resulting in a useful diagnostic tool in crmo . wbmr in fever of unknown origin ( fuo ) fuo is defined as a temperature greater than 38.3 c , for more than 3 weeks , or failure to reach a diagnosis after 1 week of inpatient investigations . 1 3 radiol med ( 2016 ) 121 : 454461 fig . 
 juvenile rheumatic arthritis and systemic lupus erythematosus are the connective tissue most frequently associated with fuo . diagnostic approach to fuo includes detailed history and examination supported with investigations . [ 39 , 40 ]  . the issue of fuo in paediatrics is rather hazy and still represents a challenging diagnostic dilemma . the major difficulty in establishing a diagnosis is that the characteristic features rendering specific disorders clinically recognizable are absent or subtle . no diagnostic algorithms are actually available , and clinicians must rely on a very careful step - by - step evaluation of the single patient . 
fevers with no reasonable explanation and no localizing signs often conceal different common diseases in children , which tend to display an unusual or atypical pattern . in patients with fuo , we performed wbmri in children with non - specific and unclear clinical findings with the aim to rule out haemato - oncologic diseases and occult abscess . wbmri offers a non - radiating , one stop shop evaluation of bone marrow signal and distribution and soft tissue signal anomalies ; at the same time , we looked for the presence of enlarged lymph nodes , serositis , and parenchymal involvement . 
imaging for and after uti is still a heavily debated topic with different approaches , as thorough evidence to decide upon a definite algorithm is scarce . content and objective this review article tries to address the clinical rational of the various approaches ( general imaging , top - down or bottom - up , selected and individualized imaging concepts ) , describes the available imaging modalities and the respective findings in imaging children with uti , and proposes an imaging algorithm for the workup of children during and after uti discussing the pros and cons of the different attitudes . conclusion in summary , imaging by us is generally considered for all infants and children with a febrile or complicated ( upper ) uti , particularly without previously known urinary tract anatomy . 
nevertheless , particularly in the first year of life the clinical presentation can be unspecific and diagnosis may be more difficult . treatment of uti is based on antibioticsthe selection and duration of the antibiotic vary with bacteria characteristics and patient defined aspects such as age or co - existing malformation [ 2 , 5 ]  . utis per se occur at any age and with or without urogenital malformations ; there are many other risk factors than just an anatomic or functional alteration of the urinary tract . 
 however , there are some differences in age distribution and gender variations , and an associated urinary tract malformation poses a higher risk for developing long - term sequelae [ 2 , 69 ]  . 
these long - term sequelae are the most important reason for not only treating but also imaging neonates , infants , and children with uti , as detecting treatable conditions will help prevent long - term damage and ensure proper long - term renal growth and function . 
 therefore , depiction of this renal involvement and the differentiation of upper versus lower uti is of enormous importance , as this has therapeutic implications and as only those with either recurrent uti and / or with renal involvement will need monitoring and follow - up . 1 3 392 radiol med ( 2016 ) 121 : 391401 what is the role of imaging in infants and children with uti ? in generalwhichever kind of imaging one applies , there must be a justifying indication , meaning that imaging will serve the patient in terms of impact on either therapy and management or prognosis . 
this so - called diagnostic thinking efficacy has increasingly become the most relevant paradigm of deciding on if and which kind of imaging should be applied , not only for economic reasons ; avoiding unnecessary investigations helps reduce patient burden , potential side - effects from imaging or contrast agent application , and decreases the pediatric radiology workload the latter becoming particularly important in these times when pediatric radiologist are becoming a rare species . 
as stated above , differentiation of upper versus lower uti , detection of potentially associated malformations and of complications , and monitoring the further development in those with upper and / or recurrent uti are questions where imaging is irreplaceable at present . what can imaging provide in childhood uti ? imaging can aid establishing the diagnosis of uti , particularly important with equivocal laboratory and clinical findings or atypical and unspecific clinical presentation as seen in newborns and infants . 
imaging further helps with workup of potential differential diagnoses . secondly , only imaging can provide information on potential urinary tract malformations that may increase the risk for a complicated course and long - term sequelae thus indicating a more intense treatment . 
the most common malformations associated with childhood uti are vesicoureteral reflux ( vur ) or obstructive uropathies such as pelvi - ureteric junction obstruction and megaureter ; rarer , but very important are also bladder outlet conditions such as posterior urethral valves . 
increasingly , the importance of voiding dysfunction is being recognized as a major risk factor for developing ( recurrent ) uti , secondarily leading to vur or obstruction at the uretero - vesical or pelviureteric junction by scarring or bladder wall thickening [ 2 , 1013 ]  . the third task of imaging is the detection of atypical or severe diseasessuch as lobar nephronia ( focal bacterial nephritis ) , granulomatous pyelonephritis , pyonephrosis , and necrosis / necrotizing pyelonephritis , of complications , such as abscess formation , and eventually also scarring and consecutive impairment of renal growth with secondary renal hypertension or ( rarely ) chronic renal insufficiency . finally , imaging is used for following - up children after severe uti and / or with urinary tract malformations and dysfunctions associated with utis , to monitor the development of the malformation and its further evolution as well as renal growth , and to detect scarring with its implications . 
sometimes imaging is also necessary to provide guidance for treatment such as percutaneous nephrostomy or abscess drainage . which imaging method is available and useful ? the most commonly used imaging modality is ultrasonography ( us )  . 
originally , this was considered just a first orienting step with compulsory additional imaging ; today with the modern developments using sophisticated techniques such as high - resolution imaging with speckle reduction filters , harmonic imaging , broadband multi - frequency , and multi - focus transducers , and also applying ( amplitudecoded ) color doppler sonography [ ( a ) cds ] and potentially contrast - enhanced us ( ce - us ) , us has become the major and oftenparticularly initiallysufficient imaging in the diagnosis and the follow - up of childhood uti [ 1417 ]  . 
 hydration must be granted ( not to miss potential obstructive conditions ) , sufficient bladder filling is mandatory ( not to miss vur and bladder conditions ) , and a post - void evaluation is an essential part of every comprehensive urinary tract us examination [ 18 , 19 ]  . 
particularly in baby boys , a study of the urethra using a perineal approach during voiding enables depiction of all relevant urethral pathology , thus reducing the need for other studies [ 1923 ]  . 
and , by installing us contrast agents ( uca ) into the urinary bladder via a bladder catheter , a reliable sonographic vur detection by contrastenhanced voiding uro - sonography ( ce - vus ) has become possible and is an established alternative to fluoroscopic voiding cysto - urethrography ( vcug ) or radionuclide cystography ( rnc ) [ 2428 ]  . fluoroscopic vcug is the commonly used modality in the setting of ( febrile , upper , or neonatal ) utinot in the primary assessment but after the infection has been treated , to assess for vur . 
still it remains essential ; a standardized technique with pulsed digital fluoroscopy and last image hold documentation should be applied to reduce the radiation burden [ 15 , 17 , 29 , 30 ]  . 1 3 radiol med ( 2016 ) 121 : 391401 renal scintigraphy in some countries is still regularly used for either depiction of acute renal involvement or for follow - up to monitor scaring and / or growth and function impairment . 
rnc is used less commonly and only in a few centers because of its reduced anatomic resolution and more restricted availability ; in older children ( i.e. , after being toilet - drained ) , the indirect rnc is a non - invasive and reliable option to assess for vur as well as urinary drainage problems . 
it offers a less invasive and most physiologic way ( no bladder catheter is required ) for vur detection [ as the study is performed after a normal diuretic renal scintigraphy ( tc99m mag3 ) [ 15 , 31 ]  . intravenous urography has become outdated and obsolete in this clinical setting . 
the same accounts for ( ce - ) cteven for assessment of renal complications such as abscesses and necrosis , modern us and mri offer alternative radiation free options and thus have almost completely replaced ce - ct of the pediatric urinary tract in the setting of uti . mri is performed also for assessment of underlying malformations or complications ; but particularly using modern approaches such as diffusion weighted imaging ( dwi ) mri has been shown to be excellent for detection of renal involvement and even scarring in and after uti [ 32 , 33 ]  . 
 combining this approach with the potential of ce - mri , a reliable evaluation of renal complications as well as assessment of potential differential diagnoses can be achieved potentially even without the need for intravenous contrast administration . 
as for scintigraphy , also mri can only be used for renal functional assessment ( e.g. , split renal function , urinary drainage and excretion ) well after the uti this assessment , however , should be avoided during the first months after such an uti . 
assessment of scarring should also be delayed at least for four to six months after the infection , and assessment of drainage impairment should only be performed after the neonatal kidney has maturatedi.e. , preferably after the first months of life . imaging findings in childhood uti typical findings in the acute infections are thickening of the bladder wall ( best depictable with sufficient bladder filling ) with potentially hazy margins and hyper - vascularisation on cds . 
however , in the acute infection these findings should not be mistaken as a prove of a bladder or voiding function disturbance ; only weeks after the uti bladder function normalizes and then these indirect signs can be used for assessing dysfunction . 
a urinary particles ( cells , crystals ) producing floating echoes in the urinary bladderin this case in a girl with acute uti ; note that this finding is unspecific , particularly if these particles have sedimented often other phenomena ( e.g. , concentrated urine , haematuria ) are the reason for this appearance . 
c axial section through the urinary bladder : bilaterally thickened ureteral wall and prominent ureters ( indicating the ureteric lumen ) visualized behind the bladder ( note necessity to properly adapt the tgc - curve ) ; only the left ureter was eventually refluxing , not the right one too ( in spite of the wall thickening ) note that the wall thickening was obviously only due to the inflammatory swelling and resolved completely after the uti 1 3 394 radiol med ( 2016 ) 121 : 391401 fig . 
a swollen right kidney with diffuse cortically increased echogenicity and focally inhomogeneously altered parenchymal echogenicity ( nearly with a pseudo - tumorous appearance ) and thickened urothelium ( arrow ) indicating severe renal involvement in upper uti . 
on scintigraphy , these areas show up as a photogenic lesionwithout additional underlying anatomic information scintigraphy , however , cannot differentiate between acute and chronic defects or other focal lesions such as cysts . 
 however , usually they respond quickly to antibiotic treatment and thus monitoring during the course of disease will often solve the query . 1 3 radiol med ( 2016 ) 121 : 391401 fig . 
 focal perfusion defects either in regions with only little parenchymal changes ( a rather regionally hypoechoic cortex with disruption of the normal cortico - medullary differentiation ) or in kidneys with severely and even more diffusely altered parenchymal echogenicity due to acute pyelonephritis ( b echogenic and hugely swollen appearance ) ; in c the decreased vascularity of the hypoechoic cortical regions in the involved lower pole is nicely demonstrated . 
d segmental linear minimal perfusion defect on power doppler ( ddx : upper parenchymal junction line vs post - inflammatory scar ) in a subacute residual perfusion deficit on the lateral aspect of this axial view of a right kidney 3 weeks after severe uti with renal involvement ( recurrent utis ) after uti these changes gradually improvehowever , the bladder and the kidney as well as the urothelium take time to normalize . 
follow - up imaging ( if necessary at all ) should be delayed at least 46 weeks to allow for normalization of renal size and parenchymal structure , resolution of the urothelial swelling , and a pacified bladder with a normal function . 
therefore , the best time for vur assessment is also after this normalization has occurredas residual laxity of the ureter , residual thickening and swelling of the bladder wall or the urothelium , as well as reactive parainflammatory bladder and voiding dysfunction may impair depiction and grading of vur . 
however , if for organizational or compliance reasons an earlier vur assessment is necessary , vcug ( or ce - vus ) can be performed as soon as the urine is cleared from bacteria , keeping potential restrictions in mind . 
vur assessment is commonly still performed by vcug fluoroscopically after bladder puncture or catheterization using a standardized methodical approach with pulsed fluoroscopy , digital image amplifying , and last image hold documentation ( see recommendations from the uroradiology task force ) [ 19 , 29 ]  . 
in 2008 , the espr uroradiology task force has published a recommendation primarily based on evaluating the kidney in the early phase and assessment of vur in the later phase only in those where either renal involvement or damage has been depicted or other sonographic signs remained obvious that hint towards vur . 
b contrast - enhanced t1 weighted axial image showing the reduced enhancement of the same left renal lesion as shown in aconsistent with a central necrosis in a focal lesion in acute pyelonephritis . 
c contrast - enhanced coronal t1 - weighted image depicts a large abscess in the upper third of the left kidney , in a girl with recurrent and multifocal pyelonephritis ; note that the remaining kidney also shows multifocal inflammatory foci fig . 
a the pelvic wall is diffusely swollen and thickened ( ) in this axial section of a right kidney with acute pyelonephritis ; also note the diffuse increased echogenicity of the widened peripelvic tissue in the renal hilus . 
b on this longitudinal section through the central kidney the huge and echogenic thickening of the entire pelvic wall and peripelvic tissue is obviousthis was due to hemorrhage due to drug intoxication , demonstrating that the urothelial sign is an unspecific finding . 
c pus sedimentations and fluid level in a child with an infected renal cyst ; note that in cysts usually no urothelial sign can be seen even in severe and long standing infection 1 3 radiol med ( 2016 ) 121 : 391401 fig . 
b high - grade urinary tract dilatation ( pelvicaliceal system and ureter ) these structures ( < - > ) are completely filled with echogenic material ( pus )  . 
note that in spite of clinically obvious ( uro - ) sepsis , the urine analysis was nearly normal ( due to the lacking drainage from the infected urinary tract ) during the annual espr congress in graz in june 2015 , this topic has been re - addressed and re - discussed under the aspect whether we need to change and adapthowever , at present no real new convincing evidence has been published that would alter these suggestions or rectify a new imaging algorith the much more restrictive indications for imaging proposed by the nice guidelines a couple of years ago are still discussed controversially ; it has also been shown that by applying these criteria some children with significant malformations and thus a considerable risk for renal damage would have been missed if these criteria would have been applied and no imaging would have been performed [ 43 , 44 ]  . 
this demonstrates that economically driven recommendations are potentially dangerous , and that the absence of evidence for a certain measure does not necessarily imply that there is no benefit for children as there usually is also any evidence that not performing the study is safe . bearing all these considerations in mind , it seems reasonableduring the acute stageto at least image all neonates , infants , and young children with the first uti usually by us , if there has not been any previous imaging study that has shown a normal urinary tract anatomy ( e.g. , by fetal or neonatal screening , by a us examination for other reasons )  . 
as potentially existing urinary tract malformations may pose the kidney at risk , these investigations should be done during the first days of the uti and should be performed thoroughly in a standardized fashion . 
furthermore , at least a detailed us study should be performed in the acute setting in all children , when the differentiation of upper versus lower uti is not achievable clinically . 
definitely all children with a prolonged or complicated course , no proper response to treatment , or known urinary tract malformations have to undergo imagingusually us is sufficient in the acute setting . 
further imaging may be indicatedwhich then is performed best by mri , such as differentiation of pseudotumorous lesions from real tumors , or evaluating the extent of a huge abscess with perinephric involvement . 
in rare cases , a ct may become necessary particularly if infectious stones are associated or for assessing conditions that go along with calcifications such as xanthogranulomatous pyelonephritis or renal tuberculosisin these instances , dedicated pediatric ct protocols have to be applied . the follow - up and work - up of children after uti depends on the initial situation . 
a child with a single potentially not febrile normal uti without renal involvement or scarring , with an also otherwise normal urinary tract sono - anatomy , will not always have to undergo a vur studyhere the indications have become much more rigid , and far less vcugs are being performed to avoid unnecessary investigations with a low yield , high costs , and significant invasiveness as well as radiation burden to quite a number of children [ 2 , 12 , 15 , 38 , 4648 ]  . 
it is different for children with uti and renal involvement particularly if with scares , altered urinary tract anatomy , significant urinary tract malformations , or sonographic signs which indicate the existence of a vur such as a gaping ostium , a duplex system with dilated lower pole ureter and collecting system ( thus being highly suspicious for vur ) , persisting urothelial thickening , or varying dilatation of the renal pelvis during the course of the disease . 
in these children , a vur test should be performedoptimally around 46 weeks after the infection , when alteration of the bladder wall and the urothelium has ceased and the ureter will have recovered his normal peristalsis and tonus . 
this then can be performed by which ever methodincreasingly , ce - vus is used for radiation protection issues ; in children 1 3 398 radiol med ( 2016 ) 121 : 391401 fig . 
8 ce - vus in vur first the native images of the relatively normal right kidney ( a ) and the left kidney with gross distention of the pelvicaliceal system ( b ) as well as of the corresponding ureter ( c )  . 
 after filling of the urinary bladder with saline infusion using a bladder catheter and fractionated instillation of us contrast agent ( sonovue , bracco / italy ) , vur into the non - dilated right ureter ( d axial view , e parasagittal oblique section , arrow ) and the dilated left ureter ( f , ) is seen . 
during voiding the urethra is clearly visiblewithout any outflow obstruction , using a perineal access ( i ) who are toilette - drained , an indirect rnc ( after a mag3 diuretic renal scintigraphy ) is probably the least invasive and most physiological way to assess for the existence of vur at low radiation burden without the need for a bladder catheter . 
particularly in older children ( after the bladder has matured ) , the importance of voiding and bladder dysfunction is increasingly recognizedthese have to be detected and treated , as even surgery for vur is eventually not successful in some of those children ; if the dysfunction is left untreated , a high re - occurrence rate of operated vur is observed . 
these children are depicted by a detailed history specifically asking for symptoms of voiding disorders and observing indirect us signs such as a constantly open bladder neck , wall thickening and trabeculation even without vur , atypical bladder capacity , and pathological post - void residual urineor by direct visualization of the dysfunction on vcug when using a modified protocol allowing for functional assessment [ 1113 , 17 , 38 , 49 ]  . 
this usually is achieved by a us follow - up ( best done not before 68 weeks after the infection ) andif there is a high suspicion for scarring or after a severe infectiona dmsa static renal scintigraphy at 69 months after the infection . 
the latter can be replaced 1 3 radiol med ( 2016 ) 121 : 391401 by mri if available at reasonable costsparticularly when applying functional mr that allows for assessment of split renal function and glomerular filtration rate . so what imaging should be practically performed practically in neonates , infants , and children with uti ? still there is no ideal universal imaging algorithm available for imaging infants and children with or after uti . 
discussion on imaging following uti is based on the correlation of uti with renal scarring , vur , other malformations of the kidneys and the urinary tract , and non - neurogenic bladder - sphincter dysfunction [ 2 , 12 , 15 , 35 , 3739 , 41 , 46 , 50 , 51 ]  . 
more than a decade ago , the american academy of pediatrics and a swedish state - of - the - art conference recommended us and vcug in all infants and young children up to two years of age with uti to detect vur [ 39 , 52 ]  . 
 even according to these recommendations , the number of investigations can be reduced and vcug not necessarily has to be performed in all children with uti , only those with indirect signs on us or complicating clinical circumstances . 
in infants with febrile uti an us investigation of the bladder and the kidney should be performed during the first two days of treatment to identify serious complications such as pyonephrosis or abscesses ( or an underlying malformation that poses a high risk for renal damage or a complicated course ) particularly when the clinical situation is severe or if there is no improvement . 
taking all this into account , it appears reasonable to perform an early comprehensive us study in all infants with ( febrile ) utiparticularly those with severe clinical symptoms , clinically equivocal situations , and yet unknown urinary tract anatomy . 
 in all patients with significant renal involvement or obvious scaring a vur test and , after four to nine months , a dmsa scan ( or in future potentially an mri ) are recommended ; in older patients also a basic assessment for functional voiding / bladder disturbances should be considered . discussion urinary tract infection is one of the most common indications for imaging work - up in pediatric radiology . 
with new insights into pathogenesis , the focus has changed towards the kidney and many other factors that pose a risk to renal involvement and scarring after uti have been identified ; thus , vur has become less important . 
this as well as refinement of imaging methods impacted imaging algorithms where new developments have widened and changed the imaging armamentarium . today still a rather generous indication for a us study of the urinary tract is advocated in infants , neonates , and children with uti particularly if with complicated course or without information on the urinary tract anatomy from previous studies . 
indications for some sort of vur assessment are much more restricted and well chosen based on clinical and imaging informationusually vcug and ( if available ) ce - vus are used ; in older children , an indirect rnc is a very good and noninvasive alternative , whereas mr - vcu has not been established probably for cost reasons , availability , and technical challenges . 
the main focus , however , will remain on those children in whom renal damage and scarring is detected and those with significant urinary tract malformations associated with ( recurrent ) utis : they will need long - term monitoring of renal health , growth , and functionmostly achieved by us , scintigraphy , and / or mri . 
the regular follow - up of a potential vur has also become less important , and intervals between follow - up studies are being prolonged as well as antibiotic prophylaxis is partially being replaced by cystoscopic vur treatment using injection of bulging agents . 
however , the story and the discussion is not yet over , and i am sure we will see new proposals coming up again . summary and conclusion us remains the mainstay for imaging in febrile ( recurrent ) childhood uti . 
the task of pediatric radiology is to provide high - quality imaging , particularly , to guarantee high - quality us and make it available 24 / 7 to help selecting patients for vur studies properly , using the proper technique at the lowest possible radiation burdentrying to avoid invasiveness whenever possible . 
but it is also important to suggest a useful urinary tract imaging adapted to the clinical situation and presentation ( and individual patient ) by us , 1 3 400 radiol med ( 2016 ) 121 : 391401 potentially vcug ( or rnc / ce - vus ) , and / or scintigraphy / mri , if potential information from the study will influence patient management , morbidity , and outcomeavoiding invasive and / or irradiating studies in all where there is no impact on therapy , management , or prognosis / outcome . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . disclosure no relevant items to declare in connection with this topic / review article . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2016 ) 121 : 327328 doi 10.1007 / s11547 - 016 - 0633 - 6 editorial pediatric radiology : current status and perspectives paolo tom1 claudio granata2 italian society of medical radiology 2016 pediatric radiology is a subspecialty of radiology and has peculiar characteristics depending on anatomical development and specific clinical conditions related to the different stages of growth . 
other peculiarities specifically related to pediatric radiology include radiation protection issues and the need of dedicated environments and approaches . in europe , training , job positions , and salaries of pediatric radiologists are quite varied . 
furthermore , most radiological examinations are performed by general radiologists , who are more numerous and better paid than pediatric radiologists . all this emerges from a survey conducted in 2009 by paolo tom and freddy avni ( esr survey on the status of pediatric radiology in europe ) through a questionnaire which was submitted to 40 national radiology societies . teaching of pediatric radiology is a mandatory part of board certification in radiology in 82.5 % of european countries , whereas in the remaining 17.5 % no specific teaching is provided . 
pediatric radiology is officially recognized as a subspecialty of radiology in just the 30 % of european countries . the mean number of academic departments with exclusive or significant pediatric radiology practice is limited to 5.5 for country , whereas the number of full professors in pediatric radiology is just 2.9 ( none in italy )  . 
teaching of pediatric radiology is provided by full time pediatric * claudio granata cgranata@sirm.org irccs , rome , italy genoa , italy 1 department of imaging , bambino ges children hospital , 2 department of radiology , istituto giannina gaslini , irccs , radiologists in 50 % of cases , general radiologists in 44 % , and by others in 6 % ( average for country )  . pediatric radiology teaching is a mandatory part of the training program of radiographers in just 40 % of countries , whereas is facultative in 50 % or absent in 10 % of the remaining european countries . 
a scientific society dedicated to pediatric radiology is present in just the 67 % of european countries . in europe , the mean percentage of the pediatric population aged < 15 years is 22 % ( range 1534 % ) ; in italy , it is 17 % , in the usa 25 % . 
in italy , some radiologists exclusively deal with pediatric patients , with high skill and expertise , however they have not the possibility of influencing the policy of residency schools . 
for this reason , subspecialties such as pediatric radiology are considered too expensive , as they are required only by a small number of patients and for specific diseases . in addition , residency programs are carried out over 4 years instead of 5 , which does not favor the development of subspecialties , thus reducing the possibility of having a sufficient number of experts . 1 3 328 radiol med ( 2016 ) 121 : 327328 overall , the number of pediatric radiologists and pediatric radiology units in europe is decreasing , due to lack of turnover and to the fact that units are merged with general radiology units . 
as a consequence , working as a pediatric radiologist is not attractive , mainly due to poor chances of career . finally , education and training in pediatric radiology is often inadequate due to the paucity of teachers with qualified expertise . 
tom1 received : 21 january 2016 / accepted : 31 january 2016 / published online : 24 february 2016 italian society of medical radiology 2016 abstract liver transplantation has become an established curative treatment in adult patients with acute or chronic end - stage liver diseases . 
in pediatric cases the number of cadaveric donor livers is not sufficient and to overcome the shortage of appropriate - sized whole liver grafts , technical variants of liver transplantation have been practiced . 
 reduced - size cadaveric and split cadaveric allografts have become an important therapeutic option , expanding the availability of size - appropriate organs for pediatric recipients with terminal liver disease . 
the number of pediatric deaths awaiting liver transplantation has been reduced by the introduction of living - related liver transplantation , developed to overcome the shortage of suitable grafts for children . 
a , b tc sign ( thickness of 3 mm or more of the anterior wall of the right portal vein measured near the portal bifurcation ) , seen as hyperechogenicity of the liver hilum and anatomically corresponding to the extrahepatic bile ducts replaced by a dense fibrous mass . 
although data are limited in children , swe can likely be used to establish the presence of fibrosis as well as assess the progression of liver fibrosis in ba over time [ 17 , 18 ]  . the diagnostic gold standard of ba , after dedicated cdus examination , is a percutaneous liver biopsy followed by an intraoperative cholangiogram if inconclusive [ 19 ]  . hepatoblastoma and hepatocellular carcinoma hepatoblastoma ( hbl ) and hepatocellular carcinoma ( hcc ) are the most common primary liver cancers in infancy and childhood . 
hbl accounts for 91 % of all liver tumors diagnosed in children younger than 5 years , hcc occurs in children 1014 years of age and is rare under the age of 5 years [ 20 , 21 ]  . most cases of hbl are sporadic , but a genetic component has been recognized associated with congenital abnormalities , such as beckwithwiedemann syndrome [ 22 ]  . predisposing conditions in hcc include ba , familiar cholestatic jaundice , glycogen storage disease type 1 , 1 - antitrypsin deficiency , wilson disease , hereditary 1 3 radiol med ( 2016 ) 121 : 378390 380 fig . 
 d enlargement of the hepatic artery diameter tyrosinemia and cirrhosis in addition to hepatitis b or c infection [ 20 , 2325 ]  . at least 90 % of patients with hbl and 70 % of patients with hcc show abnormal elevation of - fetoprotein ( afp ) level , a useful marker to monitor therapy and detect recurrence [ 26 , 27 ]  . the diagnostic approach should be chosen for each child , based on age and clinical data , such as the serum afp level . cdus is the first imaging modality in the evaluation of hbl and in the screening of hcc in pediatric patients . the selection of the appropriate imaging should consider that children require imaging strategies with a higher resolution due to smaller anatomic structures and that children may require sedation or anesthesia . 
the use of imaging tests with ionizing radiation should be minimized ( children are more susceptible than adults to the long - term effects of radiation exposure )  . the importance of high - quality cross - sectional imaging to evaluate children with hbl and hcc is paramount because the stratification risk that defines treatment depends on imaging analysis . the pre - treatment extent of disease ( pretext ) , staging system from the international society of pediatric oncology liver tumor study group ( siopel ) , offers the opportunity to monitor the effect of preoperative chemotherapy and to assess both the surgical resectability of the tumor and the required type of resection before surgery . 
for unresectable or unresponsive to chemotherapy hbl and hcc liver transplantation is now the preferred treatment option [ 22 ]  . hbls range in size from a few centimeters to more than 15 cm and generally show lobulated borders . 
6 unenhanced ct scan ( a ) , contrast - enhanced ct scan in an arterial phase ( b ) , and in a venous phase c show a solitary hcc , hypoattenuating in unenhanced ct scan ( a ) , hyperattenuating in the hepatic arterial phase after intravenous administration of iodinated contrast medium ( b ) , and its rapid washout in a venous phase ( c )  . 
note a small lesion in the transplanted liver characterized by a low - intensity signal on t1w sequence ( a ) , a high - intensity signal on t2w sequence ( b ) , and after gadolinium administration , in a venous phase , it shows a low signal intensity with a peripheral late enhanced rithese mri features are characteristic of hcc lesions ( hemorrhage , necrosis , fat and calcifications )  . 
the tumor capsule is usually hypointense on t1 and t2w images with delayed enhancement [ 33 , 34 ]  . living donor liver transplant living donor liver transplant ( ldlt ) avoids the lengthening waiting period for a deceased donor transplant , reduces the ischemic period of the transplanted organ and changes the operation from an emergency into a scheduled procedure . 1 3 383 radiol med ( 2016 ) 121 : 378390 fig . 
d the umbilical or scissural vein , draining segment iv , as a tributary of the ivc radiologist plays an important role in the evaluation of the living donor to identify anatomic variations that may switch the surgical approach . the risk for the donor from ldlt is estimated to be 0.5 % mortality and up to 21 % postoperative morbidity [ 26 ]  . us is most useful as the initial screening test in detecting hepatic parenchymal abnormalities ( fatty infiltration and focal lesions ) , while ct or mr are the modalities of choice in the demonstration of vascular and biliary anatomy of the potential liver donor , to assess the hepatic parenchyma and perform volumetric analysis . 
ct and mr have largely replaced invasive techniques such as catheter angiography , percutaneous cholangiography and endoscopic retrograde cholangiopancreatography [ 35 , 36 ]  . identification and accurate quantification of diffuse liver disease like fatty infiltration is critical for both the donor and the recipient . 
us has also been used , but these are useful only for the detection of moderate and severe degrees of steatosis . recently mr chemical shift imaging ( csi ) and mr spectroscopy ( mrs ) are considered to be the most accurate non - invasive methods to measure fat content of the liver [ 37 ]  . 
csi is more advantageous than mrs because it requires a short image acquisition time and one scan supplies enough data to quantify the fat content in any part of the liver , useful for evaluation of hepatic fat deposition in living liver donors [ 38 , 39 ]  . 
the minimum graft - to - recipient body weight ( grbw ) ratio is usually considered to be 0.8 % if corrected for the degree of steatosis or other diffuse liver disease . 
a donor liver up to 20 % larger than the estimated optimal volume is acceptable [ 40 ]  . hepatic artery knowledge of the arterial supply to the liver is of utmost importance to the surgeon when planning an arterial reconstruction because variations in the hepatic arterial anatomy occur in approximately 45 % of patients [ 40 ]  . 
they can either exist in addition to the vessels of the textbook type or replace them completely [ 41 ]  . the origin and location of the artery supplying segment iv of the liver should be identified preoperatively . 
 in this case , if the left portal vein is resected at the bifurcation , segment iv as well as segments v and viii will be deprived of portal perfusion , resulting in devascularization . exclusion of potential liver donors from surgery because of portal vein variants appears to be as high as 20 % [ 40 ]  . the estimation of the portal vein diameter is also important and should be measured in the area of expected anastomosis . hepatic veins preoperative mapping of the hepatic venous system is indispensable to the success of living - related liver transplantation , as the transection plane is determined by the anatomic distribution of the hepatic veins . 
in part this is due to the technical difficulty of performing biliary reconstruction on small caliber ducts [ 46 ] and because of leakage from even minor branches that cross the transection line and are , therefore , cut during surgery [ 47 ]  . 40 % of the population has anomalous biliary tract anatomy and to prevent complications , the transplant surgeon needs a preoperative map of the biliary tree . 
although an interoperative cholangiogram is the standard of reference , this approach runs the risk of aborted operations if complex anatomy is discovered . mrcp can be used to evaluate bile duct anatomy without the aid of contrast agents . 
b left lobe 3d volumetry ( in green ) hepatic volumetry performed manually requires sliceto - slice manual contouring of the liver surface on axial images on at least one - fifth of all the native venous phase images in the data set , depending on the liver shape . 
intermediate contours get calculated automatically using shapebased interpolations . with automated ct volumetry software , liver margins can be outlined automatically on the basis of the difference in attenuation between the liver and surrounding tissues . 
 once all the liver margins have been traced along the hepatectomy plane , the right and left lobe liver volumes are calculated , along with graft weight / remnant volume [ 48 , 49 ]  . radiological assessment of posttransplant vascular and biliary complications pediatric lt is technically challenging due to the reduced size of the vasculature and biliary tree . 
pediatric whole lt ( wlt ) is associated with better outcomes than technical variant liver transplantation ( tvlt ) [ 50 ]  . cdus plays a vital role in decreasing the incidence of graft failure providing the necessary stimulus to serial us studies or to further diagnostic procedures ( ct or mri ) [ 51 , 52 ]  . we routinely perform the first cdus examination in the operating room in all transplantations . 
us examination of transplanted liver includes grayscale evaluation of hepatic parenchyma and biliary tree , survey of the perihepatic spaces for the presence of fluid collection and doppler study of the hepatic vasculature to ensure proper functioning of the liver gra the anastomoses of hepatic artery , portal vein , inferior vena cava ( ivc ) and the hepatic veins are examined with color and pulsed doppler us . cdus examination of the hepatic artery includes measurements of the resistive index ( ri ) and systolic acceleration time ( sat )  . 
satthe interval from end diastole to the first systolic peakis a measure of the rapidity of the upstroke and it should be less than 80 ms . any deviation from this pattern must be carefully watched and followed up with serial cdus . cdus features of hat include complete absence of both proper hepatic and intrahepatic arterial flow with a wall thump on doppler imaging . cdus shows a sensitivity of 100 % , a specificity of 99.5 % , a ppv of 95 % and npv of 100 % and overall accuracy of 99.5 % in early diagnosis of hat [ 58 ]  . after thrombosis , arterial collateral vessels can develop and abnormal intrahepatic flow may be identified with a tardusparvus pattern : an sat greater than 80 ms and an ri less than 0.5. 1 3 386 radiol med ( 2016 ) 121 : 378390 fig . 
in the left hemiliver , the umbilical fissure represents the left lobectomy parenchymal plane and it is indicated by the first part of the lhv , the umbilical part of left portal vein and the ligamentum teres ( lt )  . 
in lateral segment transplantation , segments ii and iii along the left hepatic vein , left portal vein , left hepatic artery , and left bile duct go with the grathe middle hepatic vein and middle hepatic artery ( segment iv ) are preserved . 
cdus image obtained during the first postoperative day after segmental lt shows a normal monophasic waveform in the intrahepatic portal vein with mild turbulence and increased velocity ( 80 cm / s ) a result of decreased portal resistance in the presence of increased splanchnic flow ( b ) , a normal main hepatic arterial waveform with a rapid upstroke ( ri 0.66 peak systolic velocity , 35 cm / s ) ( c ) , and a monophasic waveform with slightly reduced peak velocity in uncomplicated transplantation of the hepatic vein ( d ) mr angiography is a useful and non - invasive method for evaluating the patency of the hepatic artery [ 59 ] and may play an important role in identifying patients who require angiography with therapeutic options , including thrombectomy , fibrinolytic endovascular therapy or angioplasty . hepatic artery stenosis rates range from 4 to 10 % of pediatric transplant recipients , most frequently at the anastomotic site , although it may also be found more distally [ 50 ]  . 
doppler spectral waveform analysis provides excellent screening for the detection of hepatic allograft arterial stenosis with a reported sensitivity of 100 % , a specificity of 99.5 % , a ppv of 95 % and npv of 100 % and overall accuracy of 99.5 % [ 58 ]  . 
associated turbulences distal to the stenosis are commonly observed at cdus . mr or ct angiography is an alternative non - invasive technique for a better evaluation of the anastomosis and the entire hepatic artery . 
conventional arteriography is currently reserved for endovascular treatment of the stenosis ( balloon dilatation )  . portal vein complications the risk of portal vein complications , both stenosis and thrombosis , is reported to be greater in segmental ldlt and tvlt invariably related to surgical difficulties with an incidence rate of 8 and 30 % [ 59 , 60 ]  . 
portal vein complications presenting during the early postoperative period ( < 3 months ) have worst outcomes compared with the latepresenting cases [ 61 ]  . 1 3 radiol med ( 2016 ) 121 : 378390 at us , portal vein stenosis is diagnosed when a reduction of the vessel lumen of 50 % or more is observed at the site of narrowing relative to the prestenotic area , or when the caliber of the vessel is 2.5 mm or less at the site of narrowing . 
the spectral waveform shows a systolic velocity greater than 20 m / s or a velocity in the stenotic segment that is three to four times greater than that in the prestenotic segment . hepatic venous outflow obstruction ( hvoo ) published case series have reported incidences ranging between 0 and 27.7 % of hvoo among recipients of tvlt [ 64 ]  . grayscale us demonstrates reduction of the caliber of the ivc at the anastomosis site . 
at pulsed doppler , there is a three to fourfold increase in velocity through the stenosis relative to that in the prestenotic segment associated with color doppler aliasing , and absence of phasicity in the ivc . 
contrast - enhanced ct is useful in demonstrating congestive changes in the liver parenchyma as a manifestation of blocked outflow but is of little help in depicting the stenosis itself . 
frequently , cavography with pressure gradient measurements is required to confirm the stenosis and to distinguish physiologically significant lesions from pseudostenoses . biliary complications biliary complications are the most common cause of postoperative morbidity observed in 7.5 % after wlt and fig . 
cdus image obtained on the first postoperative day after ldlt shows a tardusparvus waveform in the main hepatic artery , secondary to proximal anastomotic stenosis , which may cause focal narrowing and a dampened tardusparvus waveform distally . 
13 doppler ultrasound of the portal vein following segmental lt shows an echogenic thrombus ( white arrow in a ) within the vein with lack of color filling ( b )  . 
immediate conversion to a meso - rex shunt , using the recipient jugular vein as a bridge between the superior mesenteric vein and the graft rex recessus , allowed excellent portal revascularization of the transplanted liver ( c ) 1 3 388 radiol med ( 2016 ) 121 : 378390 fig . 
14 mr t2w axial ( a ) , and coronal image b show the obstruction of hepatic venous outflow secondary to caval compression due to fluid collection in abdomen in a 13 - year - old child after one month from ldlt . 
 end - to - end anastomoses between the donor and recipient ivcs are performed above and below the allograin the piggyback technique , the donor hepatic venous confluence is anastomosed with the recipient ivc . 
 with the use of piggyback technique , however , the incidence of hepatic venous outflow obstruction ( hvoo ) has increased 18.8 % after split organ transplantation and 17.5 % in ldlt with a mortality rate of less than 5 % within the first 3 months following transplantation , although biliary strictures can be a late manifestation [ 66 ]  . the method of biliary reconstruction and vascular insufficiency are factors that influence the frequency of biliary complications : stenosis with bile duct dilatation , sludge , anastomotic leakage and biloma . stenosis can occur at both anastomotic and non - anastomotic sites . non - anastomotic strictures are caused by hepatic arterial insufficiency and may result in bile duct strictures anywhere in the biliary tree , or leaks , increasing the risk of cholangitis , sepsis , and abscess . 
anastomotic strictures often require surgical intervention and are secondary to scar tissue causing retraction at the suture site . cdus shows low diagnostic accuracy in identifying biliary complications , particularly in early anastomotic stenosis without a significant intrahepatic biliary dilatation [ 67 ]  . 
 mrcp is used to delineate the anatomy and morphologic features of bile ducts and to screen for biliary strictures [ 68 ]  . leaks at the biliary anastomosis are associated with significant morbidity and occasional mortality . 
us is an accurate tool for evaluating also necrosis , bilomas or abscess of the graft . conclusion imaging studies are important for early diagnosis of posttransplantation complications because clinical manifestations are frequently non - specific and vary widely . 
radiologist needs to be aware of the spectrum of manifestations of vascular and non - vascular complications that can occur in the immediate postoperative period as well as during long - term follow - up . it is possible to have excellent outcomes combining a multidisciplinary team approach , technical expertise and strict patient and donor selection . cdus plays the leading role in the postoperative evaluation of pediatric patients . 
early detection of vascular complications by postoperative doppler imaging plays a vital role in decreasing the incidence of graft failure . mr may provide a comprehensive evaluation of the transplanted liver , reveal abnormalities of vascular structures , bile ducts and liver parenchyma and depict extrahepatic tissues . 
if available , mr imaging should be used when us is inconclusive . ct is a valuable complement to us in the evaluation of complications involving the hepatic parenchyma as well as extrahepatic sites , especially the thorax . 
by performing mre , it is possible to obtain results comparable to those obtained with endoscopy in terms of identifying and assessing disease activity and better than other cross - sectional imaging techniques , such as ct , in the evaluation of the fibrosis and complications of disease . 
the mr imaging of diffusion mr is a technique which enables medical staff to add important additional information and which may replace the use of intravenous contrast agents in the near future . 
familiarity with common and pathognomonic imaging features of cd is essential for every clinician involved in the treatment of inflammatory bowel disease and the care of patients . keywords crohns disease pediatric radiology mr enterography perianal fistula diffusion - weighted mri introduction there has recently been a significant incidence rise of crohns disease ( cd ) , particularly in pediatric patients . the typical lesions of the disease that affect the whole gastrointestinal tract may extend to extra - luminal and join fistulae , abscesses and lymphadenopathy . the gold standard for the diagnosis and follow - up of cd is an endoscopic evaluation of the colon and the terminal ileum ; however , mri is a non - invasive test that does not entail exposure to ionizing radiation , allows for an accurate study of intraand extra - luminal of the whole gastro - intestinal tract characterized by a multiparametric and multiplanar approach and high spatial and contrast resolution . an ever growing number of studies shows that mr enterography ( mre ) is the optimal technique of crosssectional imaging for the diagnosis and evaluation of cd activity . dwi has recently been associated with mre for studying cd , with a good degree of correlation between the restriction of diffusion parietal and mri findings specifically associated with disease activity . the purpose of mre with dwi is to avoid using paramagnetic contrast for identifying and assessing disease activity . 1 3 radiol med ( 2016 ) 121 : 362377 mri represents the gold standard technique for studying the pelvis and perineum , and has proved to be a highly effective means of identifying fistula perianal complications related to cd , both in adults and children . the disease appears to be more aggressive in children over 8 years of age . 
the most recent studies have found significant differences between adults and children with regard to the stenotic complications that arise in 13 % of the cases involving children compared to 4 % of adult cases 4 years after the diagnosis of the disease . 
 [ 19 ] observed that while 59 % of individuals suffering from cd aged < 18 years are affected in both the small and large intestines , 89 % of children under the age of 10 are only affected in the large intestine . based on these observations , the classification of paris ( 2009 ) re - examines the classification of montreal ( 2005 )  . 
 the very early onset inflammatory bowel disease ( veoibd ) is considered a form of its own and patients aged < 10 years at disease onset ( a1a ) are classified differently from those aged > 10 years ( a1b ) [ 20 ]  . children aged under two at diagnosis are more likely to suffer from a more aggressive phenotype [ 2123 ] and have a clear genetic predisposition to immune deficiency . finally , the timeliness with which immunosuppressive therapy is carried out has a significant effect on the development of complications [ 12 ]  . clinical aspects abdominal pain , fever and weight loss are common symptoms of juvenile cd onset ( < 16 years )  . 
the main complications are intestinal perforation , progressive stricture and subsequent intestinal obstruction . nutritional deficiencies , stunted growth and delayed puberty occur in percentages ranging between 65 and 85 % of patients with childhood cd onset . 1540 % of these patients continue to suffer from stunted growth throughout the course of the disease [ 2426 ]  . it is also noted a high prevalence of oral manifestations , attributable to bad absorption [ 12 ] , a greater involvement of the upper gastrointestinal tract [ 12 , 27 ] and a higher incidence of perianal lesions [ 12 , 14 , 27 , 28 ]  . 
perianal involvement in children is observed in 2538 % of cases [ 26 , 29 , 30 ] ; it affects males four times more frequently than females [ 4 , 30 , 31 ] and begins with a fistula in over a third of cases . 
abdominal compression favors the distension of the intestinal loops and enables us to decrease the number of slices , thus reducing examination time thanks to the reduction in the thickness . however , in the presence of abundant intraluminal gas magnetic susceptibility artefacts may occur at epigastric and peri - umbilical level . we used n - butylbromidehyoscine ( buscopan ) as anti - peristaltic drug . 
0.25 mg / kg of this drug is administered intravenously to patients weighing < 20 kg and from 0.5 mg / kg to a maximum of 20 mg , into patients weighing mr imaging protocol the mr enterography examinations are performed with a body coil in 1.5 t ( philips achieva , nova qasar ) and 3 t ( philips ingenia 3 t ) magnet , according to the protocol described in the table ( table 1 )  . firstly , we assess the degree of bowel distension by means of very thick single - shot fast spin echo sequences , with fluoroscopic effect . 
if the intestinal distension is not sufficient , we administrate an additional dose of sorbitol solution . dynamic assessment of intestinal peristalsis by cine imaging is an integral part of the protocol , because it allows for a better identification of pathological features . it is possible to identify the bowel segments affected by active inflammation , characterized by a reduced or absent motility as well as the fibro - stenotic segments that appear aperistaltic with pre - stenotic dilatation and the upper portion which is hypo - peristaltic . 
the cine - mri sequences provide us with useful information even in the presence of an insufficiently relaxed intestine , since they enable us to appreciate the distension of a normal loop even if this is initially collapsed . correlation with some inflammatory markers such as c - reactive protein is good [ 4446 ]  . sequences of diffusion ( dwi ) are very quick and can be carried out in free breathing or in breath hold and constitute a source of alternative contrast compared to the relaxation time . recent studies have shown reduced diffusivity in intestinal segments affected by cd . 1 3 radiol med ( 2016 ) 121 : 362377 fig . 
the axial btfe image ( c ) shows wall thickening , which appears hyperintense on diffusion - weighted image ( dwi ) ( d ) and shows restricted diffusion on adc map ( e )  . 
coronal volume interpolated gre ( thrive ) image ( f ) and axial contrastenhanced t1 - weighted with fat suppression image ( g ) show intense enhancement parietal with layered appearance the mechanism according to which this kind of phenomenon occurs is not known with certainty [ 4749 ]  . it is assumed that the infiltration of inflammatory cells , in particular of the aggregates of lymphocytes , lymphatic dilatation and the development of granulomas lead to a reduction in the extracellular space , thus restricting the mobility of water molecules [ 48 ]  . the reduced diffusion may represent a new radiological non - invasive bio - marker of cd activity . 
adc map ( c ) and dwi image ( d , e ) show parietal restriction of diffusivity in the right pathological ileal loops and lower positivity in those in left quadrants with positive lymph node ( e )  . 
these findings express the various degrees of disease activity in different pathological traits with coexistence both of acute inflammation and fibrosis , as confirmed by the different degree of enhancement on axial contrast - enhanced t1 - weighted with fat suppression image ( f ) stenotic sections due to fibro - adipose involution or in sections with mural fibrosis and superimposed active inflammation . the imaging of diffusion must be integrated with other morphological and cine sequences and with the type and degree of enhancement . finally , it is possible to provide documentary evidence of a reduction in diffusivity even in not dilated or collapsed loops , in which there are also aspects of wall thickening and enhancement which do not correspond to the actual situation . imaging findings some authors simply distinguish between active disease and chronic illness [ 41 , 43 ]  . we prefer to distinguish three main forms of cd : uncomplicated active inflammatory disease ( no fistulas or strictures ) ; penetrating disease ( deep ulcers , fistulas or abscesses ) ; fibrostenosing disease . imaging diffusion must still be an integral part of mre because of the amount of information that it provides concerning cd patients . this type of classification better answers the clinical needs and helps to direct clinicians toward a more or less intensified medical therapy or surgery [ 51 ]  . the speed of execution is also essential in the case of erythema and superficial aphthous ulcers are the earliest younger patients who are generally more intolerant . macroscopic lesions in active cd [ 52 ]  . 1 3 367 radiol med ( 2016 ) 121 : 362377 fig . 
axial turbo spin echo ( tse ) t2 - weighted image ( a ) and coronal sstse ( single - shot turbo spin echo ) t2 - weighted image ( b ) show significant wall thickening of the ascending colon with fibrofatty proliferation . 
submusal fat infiltration causes the separation of the collagen fibers that , with an orientation parallel to the surface , create a characteristic layering effect 1 3 radiol med ( 2016 ) 121 : 362377 known as halo sign that must be distinguished from the so - called target sign of the submucosal edema [ 57 ]  . the cine imaging completes the study showing a marked reduction or even the disappearance of peristaltic activity at the stricture . the reliability of imaging criteria alone is not absolutely certain , since there are often both inflammatory and fibrotic changes in the same intestinal segment . comparison with histological standards confirms a high level of accuracy ( 87 % ) of the mre in the identification of disease and it is significantly lower in the evaluation of mural fibrosis [ 43 ]  . the regenerative processes cause mucosal atrophy associated with the emergence of regenerative polyps . in these cases , there is neither a significant thickening of the wall nor a significant increase of enhancement and unlike what occurs in chronic disease , stenosis and prestenotic dilation are not characteristic findings . pelvic mr in perianal disease assessment in radiological imaging , the correct interpretation of perianal disease is based on pelvic anatomy evaluation , pathophysiology aspects and the correct classification of the various types of fistula [ 65 ]  . 
in children inadequate treatment , following a wrong diagnostic classification , almost always leads to a significant increase in morbidity , thus causing deep extension of the pathological process that affects the pelvic muscles and perianal areas . 
in children , the presence of fistulas and / or perianal abscesses is one of the main causes of incomplete response to medical or surgical treatment and relapse . anatomy of the anal canal [ 66 ] the anal sphincter is composed of two types of muscles : the external voluntary anal sphincter ( es ) and that internal involuntary anal sphincter ( is )  . between the es and the is lies the inter - sphincteric space ( iss ) , consisting in a thin layer of mainly adipose connective tissue . 
the es merges anteriorly with the perineal body and above with the puborectalis muscle ( pr ) , the latter continuing posteriorly with the levator ani muscle ( la )  . the is extends from the ano - rectal junction up to 11.5 cm below the dentate line and is an offshoot of the circular musculature of the rectum . the es is the medial edge of the ischio - anal fossae ( iaf ) or ischio - rectal fossae ( irf ) , composed of loose and fibrous connective tissue , vessels and some nerves ( inferior rectal and perineal branch of the fourth sacral nerve )  . the lateral border of iaf is represented by the internal obturator muscle ( io ) , while the superior border is represented by the la ; the posterior border is formed by the sacrotuberous ligament and gluteus maximus muscle ( gm ) , while anteriorly it is delimited by the superficial and deep transverse muscles . between the la and the ano - coccygeal ligament , there is a horseshoe connection that links the ischioanal space and deep post - anal space . mr anatomical landmarks [ 2 , 67 ] the axial and coronal planes are oriented at right angles and parallel to the anal sphincter , respectively , to allow for an accurate definition of the anatomical structures of reference . the t2 - weighted images enable us to distinguish the various components of the sphincter in relation to the characteristics of the signal , which is relatively hyperintense at is level compared to es . 
is , es , la and the iaf are well visualized in t1w unenhanced sequences and post - contrast medium acquisitions and define the relationships with abscess vehicles , especially on the coronal plane which is the main anatomic reference . the is also shows a normal homogeneous signal enhancement on post - contrastographic t1w sequence . the iss shows a fat - type signal in all sequences , therefore on t2w sequences with suppression of fat signal it differs greatly from is . the main fistulae , their secondary branches and abscesses appear hyperintense on long tr sequences , which allow for a good differentiation of the muscles and the sphincter . the course and relationships of fistulae and abscesses are best evaluated on post - intravenous contrast agents t1w sequences , particularly in the coronal plane , which is the main anatomical reference . mri technique let us outline the fields of application of the mr in the diagnostic and treatment procedure of perianal disease in diagnosis and classification of fistulas ( disease status ) , planning , pre - surgical treatment and follow - up . unlike what occurs for mre , pelvic mr does not require specific preparation and is , therefore , well tolerated by young patients . 
the dwibs sequence acquired in free breathing ( diffusion - weighted imaging with background body subtraction , tr > 5000 ms , te shortest 70 ms , 180 ms ti , epi factor 47 , b - factor 1000 s / mm2 ) represents something of a compromise between dwi and stir ; it suppresses the normal tissues and organs and it enhanced through a strong hyperintense signal pathological tissues , providing striking images - like pet [ 72 , 73 ]  . pathophysiology and epidemiology of perianal fistulas at present , the crypto - glandular etiopathogenetic hypothesis is the most accepted even if controversial [ 8 , 74 ]  . 
the anal glands , located on the same level as the dentate line between the columns of morgagni , are involved in the lubrication process of the anus through the secretion of mucus in the anal crypts . 
the alteration or obstruction of the drainage of crypts is probably at the origin of a local inflammatory / infectious process that results in an abscess which may resolve itself spontaneously due to direct drainage into the anal canal or lead to the formation of fistulas [ 75 ]  . abscess and fistula would then be acute or chronic manifestations of a single disease process , since 87 % of the patients develop fistulas following an acute perianal abscess [ 67 ]  . other causes of perianal fistula , less significant in statistical terms than cd , are tuberculosis , diverticulitis , pelvic infections , trauma and complications of surgery [ 76 , 77 ]  . 
 there is perianal involvement in patients with more than 38 % cd with a ratio of four males to one female ( due to the fact that males have more anal glands than females )  . 
james university hospital classification ( morris et al . ) is an adaptation of parks classification of diagnostic imaging [ 31 ]  . in this classification , the categories identified by park are maintained , while the surgical references are replaced with radiologic anatomy on pelvic mri and additional parameters are introduced , such as the presence of secondary sinus tract and / or abscess formation . according to morriss classification , there are five different types or degrees of perianal fistulas : 1 . 
complex transphincteric fistula with abscess or secondary fistulous tract within the iaf or irf ( grade 4 ) that has similar characteristics to simple trans - sphincteric fistula , but it is complicated by secondary tracts or abscesses . 
supraand extra - sphincteric fistula that forms complex fistulas ( grade 5 ) : supra - sphincter fistula exits the iss 1 3 radiol med ( 2016 ) 121 : 362377 fig . 
the fistula tract does not involve the external sphincter ( se ) as evident in coronal t2 - weighted image ( a ) and coronal short t1 inversion recovery ( stir ) image ( b )  . 
axial diffusion - weighted whole - body imaging with background body signal suppression ( dwibs ) image ( c ) shows a high signal tract which matches with intense enhancement shown on axial contrast - enhanced t1 - weighted with fat suppression image ( d ) consistent with active disease . 
6 grade 2 ( morriss ) intersphincter fistula ( a , arrow ) which is limited by the external sphincter ( se ) with cryptoglandular abscess ( b , dashed arrow )  . 
7 grade 3 ( morriss ) transphincteric fistula with an internal opening at 910 oclock and which penetrates the sphincterial complex and in particular the external anal sphincter ( se ) as shown on axial t2 - weighted image ( a ) and on the corresponding axial dwibs image ( b )  . 
coronal stir image ( c ) , coronal dwibs image ( d ) and coronal contrast - enhanced t1 - weighted with fat suppression image ( e ) show penetration through the ischio - rectal fossae ( fir )  . 
james university hospital is more descriptive and is based on mr anatomy , parks classification is preferable in pediatrics as it is based on the coronal plane rather than the axial plane . 
in fact in children , the anal canal is much shorter than in adults , for which it is particularly difficult to classify a type of fistula on the axial plane correctly . therefore , the description of secondary vehicles and the associated abscesses must be included in the radiological reports when referring to parks classification as they are the main causes of inadequate response to treatment ( medical or surgical ) and relapse in children . for descriptive purposes when reporting mr , the socalled anal clock [ 80 ] of the surgical field is generally used to locate the origin of the fistula with respect to the anal canal exactly . 
the anal clock is an axial section comparable to a clock face in which the pubic symphysis indicates 12 oclock , the buttock crease 6 oclock , and the right and left buttocks 9 and 3 oclock , respectively . imaging findings in the structure of the sphincter complex and pelvic muscles , a fistula is distinguished as a hypointense linear structure on t1 - weighted sequences and hyperintense on t2w and t1 - weighted sequences ( especially with fat saturation )  . 
active fistula or abscesses are characterized by a marked positivity on dwibs images and a corresponding enhancement on t1 post - contrastographic sequences . a loss of t2 - weighted imaging hyperintense signal or lack of enhancement on t1 - weighted post - contrastographic sequences correlated with a progressive inactivation of the disease process [ 82 ]  . 
these changes are reliable predictors and make the mr study particularly useful in the follow - up of peri - anal disease , especially as an instrumental assessment of the response to treatment [ 4 , 83 , 84 ]  . equally important is the contribution provided by mri in the evaluation of deep tissue , peripheral to the fistula , with particular regard to the irf or iaf . 
edema , signal and structural distortion of fibro - adipose components and postcontrast - enhancement of the signal indicate deep and persistent inflammation in the tissue . the first element to be assessed is whether there is a main tract or not and the total number of fistulas present [ 32 , 81 ]  . the fistula must be characterized and classified according to its course and its relationship with the sphincter 1 3 radiol med ( 2016 ) 121 : 362377 fig . 
most fistulas are of posterior origin and must be localized according to the anal clock [ 85 ]  . therefore , the description of secondary tracts and the associated abscesses must be included in the radiological reports when referring to parks classification as they are the main causes of inadequate response to treatment ( medical or surgical ) and relapse in children . 
the secondary tracts are identified separately and described according to their relationships with the main fistula , localizing them with respect to the anal sphincter , the la and any skin outlet skin , if independent . 
the perianal abscesses tend to show high signal intensity on t2 - weighted sequences as fistulas , but may appear uneven and hyper intense in t1 - weighted baseline sequences with peripheral characteristic peripheral enhancement in post - contrastographic sequences . 
mr images enable us to view and correctly assess post - surgical findings , particularly in the presence of setons [ 86 , 87 ]  . the identification of collateral findings is particularly important in children , especially in pelvic mri . 
9 grade 5 ( morriss ) supralevator fistula with abscess : right supralevator fistula that penetrates levator ani ( ea ) above the puborectal muscle which shows an anomalous signal on axial t2 - weighted image ( a ) and on axial t1 - weighted image ( b ) , hyperintense and discontinued signal on coronal stir image ( c ) and abnormal enhancement on t1 - weighted image with fat suppression following contrast agent administration ( d )  . 
presence of late gadolinium * nicol schicchi schicchi.n@alice.it 1 radiologia pediatrica e specialistica , azienda ospedaliero universitaria , ospedali riuniti di ancona , via conca 71 , torrette , 60126 ancona , italy 2 department of imaging , bambino geschildrens hospital irccs , rome , italy 3 department of medical - surgical sciences and translational medicine , university of rome sapienza , rome , italy 4 department medical and surgical of pediatric cardiology , bambino geschildrens hospital irccs , rome , italy 5 scuola di specializzazione in radiodiagnostica , universit politecnica delle marche , ancona , italy enhancement suggesting myocardial macroscopic fibrosis seems to play a prognostic and diagnostic role even in this field . keywords congenital heart disease cardiac magnetic resonance pediatric imaging introduction the prevalence of congenital heart disease ( chd ) is very close to 1 % at birth in the united states [ 1 ]  . 
nowadays incidence of adult patients with chd has significantly increased due to the major improvements over the last decades in chd long - term survival [ 1 ]  . in chd imaging is fundamental in diagnosis and is crucial at all stages of patient care . 
 the lack of ionizing radiation and the ability to provide detailed anatomic and functional information make cardiac magnetic resonance ( cmr ) a versatile and thorough modality for the evaluation and follow - up in this setting . echocardiography is still the most economic , immediate and non - invasive approach for the evaluation of anatomy and function of cardiovascular system in patients with chd both pediatric and adults , however , could be hardly affected by a poor acoustic window [ 3 ]  . angiography catheterization in chd allows the evaluation of great vessels , flows and pressures ; furthermore permits in selected cases a therapeutic approach [ 4 ]  . 
although interventional approach can be advantageous for the therapeutic implications , it is an invasive procedure requiring the use of ionizing radiation and it is operator dependent [ 5 ]  . 
therefore , cmr ( cmr ) is progressively replacing its diagnostic role [ 6 ]  . 1 3 radiol med ( 2016 ) 121 : 342351 cardiac computed tomography ( cct ) can be useful to assess with excellent spatial resolution morphology and ventricular function of heart and great vessels when mri is contraindicated [ 2 ]  . 
disadvantages of cct are the use of ionizing radiation and administration of iodine contrast agent . thus , cmr is able to provide information that range from quantification of volumes and flows to morphology of cardiac and vascular structures , and might be useful both for therapeutic planning and for follow up after the intervention [ 79 ]  . nowadays , despite the presence of intrinsic limitations of the cmr ( spatial resolution , contraindications in - patient with metallic devices , uncooperative patients ) , it has expanded its role in the management of pediatric patients and adults with chd , becoming a crucial diagnostic technique . technical details cmr acquisition acquisition with anesthesia or sedation in order to improve the image quality of cmr , it is advisable to perform the examination in uncooperative patients under general anesthesia . 
however , several studies in literature have shown the relative safety of the cmr performed in general anesthesia or deep sedation [ 10 12 ]  . acquisition without anesthesia cmr performed without anesthesia needs important cooperation of the patient , to avoid both motion and respiratory artifacts . sequences all the sequences used in cmr are synchronized with ecg . 
it is advisable to acquire all the sequences in breathhold in order to reduce artefacts caused by respiratory motion . t1 black blood fast spin echo t1 black blood fast spin echo ( bbfse ) sequence generates images where flowing blood appears dark while more stationary tissues show various shades of grey depending on signal intensity . 
t1 bbfse are used to provide anatomic information and they are less susceptible to metallic artefacts [ 13 ]  . ecggated cine imaging retrospectively ecg - gated balanced steady state free precession ( b - ssfp ) cine images , acquired in any plane and typically during breath hold , can be useful for the evaluation of cardiac function as well as for the qualitative assessment of valvular function [ 14 , 15 ]  . short axis cine images are used to perform quantitative evaluation of ventricle volumes and cardiac function , using an off - line workstation with a dedicated software through different algorithms [ 16 , 17 ]  . target spatial and temporal resolution parameters in our 57 mm center are respectively , 1.52 mm in pixel size slice thickness , and 3040 ms . optimized and customized shimming box must be used in order to reduce artifacts due to magnetic field in - homogeneities . more robust cine images such as spoilt - gre can be alternatively performed to reduce metal artefacts , or in presence of turbulent flow disturbances . magnetic resonance angiography mr angiography ( mra ) is a powerful tool to investigate complex vascular patterns in chd [ 13 ]  . 
compared to cct and common invasive angiography cmr it can produce images of the great vessels without using ionizing radiation and with or without injection of contrast agent [ 18 ]  . time of flight sequence is based on the difference of signal intensity between static tissue and blood . 
usually two or three sequential acquisitions are performed , in order to allow visualization of the entire chest vascular systeafter introducing some technical upgrades to improve the time resolution , a new ce - mra sequence is more recently made available . 
faster k - space data filling algorithm permits to acquire multiple 3d volume sets as the contrast agent passes through the vessels , producing a time - resolved mra [ 20 ]  . the 3d datasets generated by mra allows volume rendering ( vr ) and maximum intensity projection ( mip ) reconstructions , which are extremely important especially 1 3 344 radiol med ( 2016 ) 121 : 342351 for non - cmr specialists , because they clearly depict complex spatial relationships of normal and pathological structures often seen in chd [ 18 ]  . tetralogy of fallot examples of clinical indications coronary imaging ( cmra ) the high - speed gradient technique and cardiac coils contributed to a huge boost for development of 3d ssfp protocol for coronary mr angiography ( cmra ) in the early 90s . 
during cmra respiratory trigger is used to minimize the respiratory artifacts , and defining cardiac cycle phase could be crucial in order to visualize each coronary artery [ 21 , 22 ]  . 
cmra with a large field of view can be also applied for the visualization of other chest vascular structures . phase contrast phase contrast ( pc ) sequence is the gold standard for flow volume quantification , enabling the profiling of flow acceleration jets , with velocity estimation and it is useful to assess blood flow pattern [ 23 ]  . considering the phase shift proportional to the flow speed , it is important during the setting of the sequence to use a proper encoding rate to avoid aliasing artifacts . 
partial volume effects are strictly dependent on the thickness and orientation of the slice during the acquisition [ 24 ]  . a classical example of use of pc is in valvular disease because it allows to quantitatively establish flow , regurgitant fraction and peak velocity [ 25 ]  . late gadolinium enhancement as shown already in 2001 by simonetti et al . 
using t1 weighted single - shot inversion - recovery turbo flash images around 1015 min after injection of paramagnetic contrast , it is possible to suppress the signal of normal myocardium and thus visualize an infarcted area . 
the high signal intensity of the fibrotic area is the expression of a slow wash - out of gadolinium due to the cellular damage and increased extracellular volume [ 27 ]  . evaluation of late enhancement can be important in patients with chd , particularly in those who underwent surgical procedures involving coronary arteries manipulation [ 28 , 29 ]  . table 1 shows the sequences helpful for the evaluation of chd . tetralogy of fallot ( tof ) is the most common cyanotic chd characterized by the presence of the following findings : right ventricular outflow tract obstruction , ventricular septal defect , overriding aorta and hypertrophic right ventricle ( rv )  . 
sometimes this pathology can be associated to other congenital pathological conditions , such as 21 trysomy , deletions of chromosome 22q11 [ 30 ]  . cmr is particularly important in the post - operative follow - up [ 3133 ]  . 
despite excellent mid - term results , homografts and xenografts , usually implanted for rv outflow tract restoration , are affected by late dysfunction and failure , committing patients to further interventions [ 34 ]  . timing of pulmonary valve replacement is thus a delicate balance between progressive rv dilatation and dysfunction , and risk of high morbidity and re - operation . cmr is the gold standard technique for rv assessment and plays a key role in this setting . 
associated findings , especially pulmonary artery stenosis , which often must be managed surgically , could be also accurately detected by cmr . cine images are useful for the evaluation of ventricular function and volumes while degree of pulmonary regurgitation could be quantified using phase contrast sequences table 1 cmr sequences used in patients with chd primary techniques of cmr to evaluate chd : relationship between sequences and diagnostic imaging morfologic images functional images t1 bbfse cine b - ssfp cine b - ssfp flight , phase contrast magnetic resonance angiography ce - mra , time resolved mra 3d navigator ssfp , 3d time of flow tissue characterization late gadolinium enhancement 1 3 radiol med ( 2016 ) 121 : 342351 [ 37 ]  . 
mra provides information about the anatomy and morphology of pulmonary arteries [ 38 ]  . an example of the utility of cine ssfp sequences and phase contrast in patients with tof is shown in figs . 
however , cmr is fundamental in the postoperative assessment [ 2 ]  . baffles , diverging systemic venous return to the left ventricle and pulmonary venous return to the right ventricle . 
 this creates a physiological correction of the problem with a very abnormal anatomy , and a systemic rv sustaining the systemic circulation . cmr patients submitted to operation is fundamental to evaluate , using cine images , the systemic right ventricle function , the degree of tricuspid regurgitation , the presence of left ventricular outflow tract obstruction and patency of baffles . 
furthermore , the presence of late enhancement in systemic right ventricle is associated with a worst prognosis [ 42 ]  . the first surgical approach performed for this condition was the senning and the mustard procedures ( atrial switch operations ) , characterized by the creation of intra - atrial nowadays , the most used surgical technique for this condition is the arterial switch operation [ 43 ] , which provides both physiological and anatomical correction , connecting fig . 
 analysis of flow pattern confirm the severe pulmonary regurgitation ( b ) 1 3 346 radiol med ( 2016 ) 121 : 342351 the aorta to the left ventricle and the pulmonary artery to the right ventricle . despite the excellent long term outcome , patients after arterial switch operation could be affected by serious complications related to the surgical procedure . the more frequent complications are mainly pulmonary artery or branch pulmonary artery stenosis . 
concerns about possible ischemic sequelae are also present , since coronary arteries re - implantation is required during the procedure [ 43 ]  . cine images may provide data regarding dyskinetic areas , and late enhancement assessment can be useful to evaluate presence and extension of infarcted area as a result of coronary damage [ 28 , 41 ]  . 
cine ssfp show patent systemic veins baffles connected to the left ventricle ( arrowhead , a ) and patent pulmonary veins baffle connected to the right atrium ( arrow , b ) fig . 
 cmra allows the evaluation of the origin of right ( arrowhead , b ) and left ( arrow , b ) coronaries after the implantation 1 3 radiol med ( 2016 ) 121 : 342351 interposition of a sub - pulmonary ventricle . 
thus , the systemic venous pressure and the respiratory mechanics are the only forces supplying pulmonary blood flow to the lungs [ 39 , 44 , 45 ]  . even if some centers and some authors advocate a key role for cmr in the pre - operative planning [ 46 ] , the postsurgical care is the setting where cmr is vastly utilized . single ventricle function and atrio - ventricular valvar function , can be evaluated using cine images . 
pc flow study in multiple planes allows the evaluation of cardiac output , and presence and estimation of systemic to pulmonary collateral flow [ 47 ]  . mra with or without contrast cine images , can provide information regarding the anatomy of the great vessels and the patency whole circuit [ 47 ]  . figure 5 shows an example of sequences used in a patient underwent to fontan operation . aortic coarctation aortic coarctation ( ac ) is a common chd with an incidence of 58 % [ 48 ]  . 
suggest to acquire cine images of the aortic arch and of the left ventricle to quantify the volumes , assess the function and myocardial mass ; the latter could be increased due to the increased left ventricle afterload . 
 ce - mra of the thorax shows the connection ( arrowheads , a ) between the inferior and superior vena cava with right pulmonary artery ( arrow , a ) , the latter appear patent . 
phase contrast of aortic isthmus allows the evaluation of peak velocity and pattern of flow 1 3 348 radiol med ( 2016 ) 121 : 342351 subsequently , they suggest to acquire a stack of cine images parallel to the aortic root , in order to visualize the aortic valve morphology , often bicuspid in this setting . 
at last they suggest to acquire a phase contrast on the site of coarctation , to estimate the peak velocity and distal descending aorta and to observe the presence of the typical diastolic antegrade flow . 
inferior dislocation of septal and posterior leaflets of tricuspid valve ; the right ventricle included between the real valvular annulus and the displaced leaflets , is thus atrialized ( small and dysplastic ) fig . 
black blood images ( a , b ) ; vr reconstructions ( c , d , e , f , g ) ; ce - mri images ( h , i ) conclusion and future perspective cross - sectional imaging of chd is swiftly growing . 
this is happening mainly because many palliative and healing treatment are lengthening life expectancy in these patients . patients with chd need constant follow - up and cmr obviously plays a key role in the one stop shop anatomical and functional assessment , thanks to its non - invasiveness and the absence of ionizing radiation . 
however , cmr may be limited in its use in less cooperative patients and 1 3 350 radiol med ( 2016 ) 121 : 342351 contraindicated in case of implant of certain metallic and electronic devices . general anesthesia is required in patients with chd younger than 7 - years - old , however , careful evaluation of clinical indication and safety procedures in the mr field is recommended . newer and implemented imaging techniques are being developed to perform cmr more quickly and to provide additional clinical information . 
in fact , accelerated cine and flow sequences with a more rapid process of acquisition and reconstruction of mr data are validated and diagnostically equivalent to conventional ones ; those developments may be applied on less cooperative patients and in case of cardiac arrhythmias [ 51 , 52 ]  . 
furthermore , quicker protocols and optimized reporting workflows are also fundamental to improve cmr staff efficiency ; this is particularly true in imaging centers constantly facing with unsustainability issues . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . financial support this study was not funded by any organization . ethical approval this article does not contain any studies with animals performed by any of the authors . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
strouse3 received : 27 november 2015 / accepted : 9 december 2015 / published online : 2 february 2016 italian society of medical radiology 2016 abstract sports related injuries are common in children and adolescents , with a reported incidence of around one in ten children each year . 
sports injuries seen in children under 10 - years of age are non - specific , including contusions , mild sprains , and extremity fractures , usually salter fractures of the physes ( growth plate ) or plastic fractures . 
strouse , karen rosendahl ( 2013 ) specific aspects of sports related injuries of the pediatric musculoskeletal systein : hodler j , von schulthess gk , zollikofer chl ( eds ) musculoskeletal diseases 20132016 , springer - verlag italia , milan pp 194202 . 
we will concentrate on injuries that are specific for the growing skeleton , with a brief mention of those seen after fusion of the physes . keywords sport injury children musculoskeletal imaging sports injury of the pediatric musculoskeletal system factors affecting the incidence and anatomic distribution of sports injury in pediatric patients include age , gender , the type of sport , intensity of participation and the position played [ 13 ]  . 
in a study from the united kingdom , approximately 4 in 5 of children between the ages of 5 and 15 years old were participants in an organized sport [ 4 ]  . 
chance for injury is greater with contact or jumping sports , with american football followed by wrestling , basketball , soccer and baseball in the likelihood for injury [ 5 ]  . 
sports injuries seen in children under 10 years of age are non - specific , consisting of contusions , mild sprains , and extremity fractures , usually salter fractures of 1 3 432 radiol med ( 2016 ) 121 : 431441 the growth plate or plastic fractures ( i.e. , buckle or greenstick factures )  . 
in the very young athlete , sports injury of the ligaments or muscle is rare as are spine or head injuries . with growth and adolescence , the intensity of sports involvement increases and sports become more competitive , more intense and more physical . 
the physes are the weakest link in the anatomic cha injury mechanisms which cause ligament injury in individuals with closed physes are prone to cause physeal injury in a skeletally immature athlete . 
after the physes fuse , ligamentous injury is seen with patters similar to adults . adolescents are not only prone to stress injury of the physes , but also stress injury away from the growth plate within the bones . 
these stress injuries are very similar in clinical presentation and imaging appearance to those occurring in adults . underlying congenital anomalies ( i.e. , tarsal coalition , os trigonum ) may predispose to stress injury or may become symptomatically evident with increased participation in sport . 
post - traumatic myositis ossificans may mimic an aggressive soft tissue neoplasthose interpreting imaging for sports injury in children need be familiar with the imaging patterns of injury and processes that may predispose to injury , mimic injury and occur as a consequence of injury . we will present sports injuries that are specific to children and adolescents . 
less emphasis will be placed on injuries which are more common in adults and occur principally in older adolescents with fused physes . shoulder injuries of the shoulder are more common in the latter half of the second decade , and with participation in contact sports such as wrestling , american football and hockey [ 9 ]  . 
treatment with cessation of activity leads to abatement of symptoms and resolution of radiologic findings . another type of overuse injury seen at the shoulder in children , however , rare , is intra - articular disorders ( i.e. , internal impingement of the shoulder ) [ 10 ]  . 
displacement of greater than 3 mm is usually considered an indication for surgical reduction and pinning . adolescent throwing athletes are also prone to other injuries of the elbow , including osteochondritis dissecans of the capitellum , stress injury of the medial epicondyle physis , flexor tendinopathy , ulnar collateral ligament injury and stress injury of the olecranon [ 13 ]  . 
medial epicondylar physeal stress injury may be labeled as medial epicondylitis or little leaguers elbow ; however , classic little leaguers elbow , as originally reported , is an acute medial epicondyle avulsion fracture [ 13 ]  . 
pitch or inning limits are imposed in youth baseball aim to prevent injuries to the elbow . osteochondral injury of the capitellum is a consequence of valgus stress injury [ 13 ]  . 
the distal radial physis is widened with irregularly of its metaphyseal marg symmetric abnormality was noted on the contralateral side unstable osteochondral fragments may become loose bodies within the elbow joint . stress injury of the olecranon is uncommon and is likely due to the stress of triceps muscle contraction occurring during the throwing motion [ 13 , 14 ]  . wrist and hands wrist injuries in child and adolescent athletes are common . 
however , continued gymnastic activity will predispose premature physeal fusion , resulting in relative radial shortening and positive ulnar variance ( the ulna is long relative to the radius ) this predisposes to carpal impingement and triangular fibrocartilage complex injury . injury to the carpal bones is rare in children . 
4 acute avulsion of anterior superior iliac spine ( asis , arrow ) and chronic avulsion of ischial tuberosity ( arrowheads ) in a 16 - yearold boy soccer player . 
carpal ligament injury in uncommon before puberty . patterns of metacarpal and phalangeal injury in children are different than in adults due to the composition of the bones and the presents of the physes active children are subject to physeal injuries of the metacarpals and phalanges which are sometime subtle on radiographs . pelvis and hips at the pelvis and hips , there are six apophyseal growth centers : the iliac crest , the anterior superior iliac spine ( asis ) , the anterior inferior iliac spine ( aiis ) , the ischial apophysis , the greater trochanter and the lesser trochanter [ 18 ]  . 
posteromedial displacement of the left femoral head relative to the left femoral neck and growth plate widening are better seen on the abduction view ( b ) the site of injury . 
if a child is unable to bear weight on the extremity , the scfe is termed unstable if the child is unable to bear weight and stable able to bear weight [ 19 ]  . 
on the order of 20 % of patients will have bilateral scfe ; however , in the absence of an underlying predisposing condition 1 3 radiol med ( 2016 ) 121 : 431441 findings are rarely symmetric at presentation . 
symmetric presentation , particularly in a younger child , is suggestive of an underlying endocrinopathy . the diagnosis of scfe is made by identifying malalignment of the femoral head and the femoral neck . 
ancillary findings include external rotation of the proximal femur , sclerosis or buttressing in the femoral neck , and decrease in height of the femoral head due to its rotation on the femoral neck . 
patients with fai present with locking and / or decreased range of hip motion suggestive of associated labral tears or with pain which occurs in extremes of flexion . knee open physes at the knee are weaker than ligaments . 
on cross - table lateral views , a fat / fluid level is often present , indicative of an intra - articular fracture . injury to the cruciate and collateral ligaments and menisci is uncommon before skeletal maturing . 
mri also shows bone marrow edema of the medial patella and disruption of the medial retinaculum and the medial patellofemoral ligament . stress injuries can occur at the tibial apophysis ( osgood schlatter disease ) or at the inferior pole of the patella ( sinding - larsenjohansson disease )  . 
 juvenile ocd has been hypothesized to represent a stress injury of the epiphyseal physis with possible difference in etiology than adult ocd [ 29 ]  . bipartite patella is a common normal variant . 
on mri , bone marrow edema is indicative of stress or injury . ankle and foot the juvenile tillaux and triplane fractures are called transitional fractures as they occur in patients who are skeletal maturity in whom the distal tibial physis is partially fused . 
injuries of the tendons of the ankle and foot are uncommon in children . tarsal coalition most frequently presents near the onset of the second decade as the ossification of the bones nears completion and the foot becomes less flexible [ 31 ]  . 
tarsal coalition predisposes patients to ankle sprains , ocd of the talar dome and foot / ankle tendinopathy . an accessory navicular bone may cause symptoms due to stress at its synchondrosis with the underlying navicular bone [ 33 ]  . 
with impingement , mri shows edema within the os trigonum , if present , and within adjacent soft tissues . avulsion fracture of the fifth metacarpal tuberosity is common in adolescents [ 34 ]  . 
tuberosity fractures have a good prognosis for healing while jones fractures are more prone to non - union . stress fracture as with adults , active adolescents can develop stress fractures with repetitive activity [ 35 ]  . 
 radiography and ct are most useful for demonstrating vertebral fracture , while mri is helpful for evaluating paraspinal musculature , spinal ligaments , intervertebral disks , and the spinal cord [ 38 ]  . fortunately , acute spine injuries from sports are rare , but constitute up to one - fourth of all acute cervical spine injuries in children . 
any level in the cervical spine can be affected , but most spinal injuries occurring below the age of 12 years involve c1 and c2 at the atlanto - axial or atlanto - occipital joints . 
with approximately 75 % of these cervical spine injuries , no radiographic abnormality is detected ( spinal cord injury without radiographic abnormality , sciwora ) ; however , mri demonstrates spinal cord edema and / or hemorrhage . 
11 schmorl nodes in a 7 - year - old female skier , presenting with lower back pa lateral radiograph showing a defect ( arrow ) in the upper end plate of the fourth lumbar vertebrae , anteriorly , and reduced disk height at level l3 / l4 . 
schmorl nodes are common in the lower thoracic and upper lumbar spine of adolescents , and can be accompanied by pa they may also be seen in association with scheuermann disease ( juvenile kyphosis )  . 
this phenomenon is noted in adolescents and may represent failure of fusion of the ring apophysis ( limbus vertebrae )  . scheuermann disease of the spine is defined as kyphosis of the thoracic and upper lumbar spine with at least three adjacent wedge shaped vertebrae ( each with anterior wedging of greater than 5 )  . 
13 spondylolysis and spondylolisthesis in a 12 - year - old male football player , presenting with low back pa lateral radiograph shows a linear defect in the pars interarticularis ( arrow ) consistent with spondylolysis at l5 , with grade i anterior spondylolisthesis of l5 on s1 . 
when a pars defect is identified radiographically , further imaging usually is not needed spondylolysis is defined as defect within the pars interarticularis between the superior facet and inferior facet of a vertebra . 
 if radiography is negative or inconclusive , a tailored ct or 1 3 440 radiol med ( 2016 ) 121 : 431441 mr using reversed angle axial images ( approximately 45 caudal angulation ) will demonstrate the pars defect and show any foraminal encroachment . 
mr findings may aid in guiding treatment by distinguishing between an acute or healing lesion and an inactive lesion representing a fibrous union . conclusion modern children and adolescents are extremely active in sports . 
avni1 valerie leroy2 audrey riquet3 lucile gogneaux4 received : 12 may 2015 / accepted : 20 july 2015 / published online : 29 july 2015 italian society of medical radiology 2015 abstract introduction tuberous sclerosis complex ( tsc ) involves frequently the kidneys . 
the disease can be associated with autosomal dominant polycystic kidney disease leading to the contiguous gene syndrome ( cgs ) the objectives of the present study were to review the us appearances of the renal involvement in children affected by classical tsc or by the cgs and to verify whether it is possible to differentiate between both entities . 
 clinical data reviewed included age at diagnosis , genetic assessment and complications ; us data reviewed included renal size , type of lesions ( angiomyolipomaaml , or cysts ) , number and location as well as their evolution with time . 
group 1 ( 9 patients ) displayed microscopic ( diffuse ) aml ; group * arthur robert arthur.robert.lille@gmail.com 2 ( 3 patients ) displayed macroscopic aml ; group 3 ( 9 patients ) displayed only renal cysts and group 4 ( 9 patients ) displayed the association of aml and cysts . 
the disease occurs in 1 in 6000 live births [ 1 ] and is related to mutations in the tumorsuppressing genes tsc1 and tsc2 located on chromosome 16 [ 2 , 3 ]  . 
these genes lie very close to the gene pkd1 involved in the autosomal dominant polycystic kidney 1 3 radiol med ( 2016 ) 121 : 402408 table 1 diagnostic criteria for tuberous sclerosis complex major features minor features facial angiofibromas or forehead plaque gingival fibromas non - traumatic ungueal or periungual fibroma hamartomatous rectal polyps hypomelanotic macules ( more than three ) shagreen patch ( connective tissue nevus ) multiple retinal nodular hamartomas confetti skin lesions non - renal hamartoma retinal achromic patch cerebral white matter migration lines cortical tuber subependymal nodule lymphangiomyomatosis renal angiomyolipoma subependymal giant cell astrocytoma multiple randomly distributed pits in dental enamel cardiac rhabdomyoma , single or multiple bone cysts multiple renal cysts disease ( adpkd )  . 
this vicinity explains the description of cases presenting the association of classical tsc and symptoms of adpkd determining the so - called contiguous gene syndrome ( cgs ) [ 4 , 5 ]  . tuberous sclerosis complex is called so because of the appearance of the tumours developed by patients suffering from this disease : tuberous , from latin tuber ( swelling ) , and sclerosis from greek skleros ( hard )  . 
in children , like in adults , the diagnosis is ascertained when two major and two minor criteria are present ; it is probable when one major and two minor criteria are found ; it is possible when only one major and one minor criteria are demonstrated [ 1 ]  . pediatric patients affected by the tsc will display the various typical lesions but with variable frequency . 
the latter is exceptional during childhood and more frequent in adults ( at a younger age than the usual renal carcinomas ) [ 6 ]  . renal involvement in tsc is mainly an incidental finding . 
all these complications are rare in children but are the main causes of morbidity and mortality in adult patients [ 8 ]  . in children , most renal lesions will be detected and characterized by ultrasound ( us ) , whereas in adults ct scan is more often used to evaluate the extent of the renal involvement and its complications [ 1013 ]  . the tumoral volume of some specific tumors developing in tsc like renal angiomyolipoma or subependymal giant cell astrocytoma ; therefore , a better evaluation of the renal tumoral involvement and its evolution would be helpful to select patients that might benefit from these treatments . 
 furthermore , as mentioned above , complications may differ in patients with the classical tsc and in patients with the cgs . therefore , the aims of the present study were to : redefine the various us patterns of the renal involvement in a series of children with tsc . find criteria that would help to differentiate between the classical tsc and the cgs . evaluate the evolution with time of the renal involvement . verify the rate of complications in childhood . materials and methods we have reviewed the clinical and imaging files of 55 patients ( 28 boys27 girls ) with tsc from the registry of the centre de rfrence rgional du nord pas de calais de la sclrose tubreuse de bourneville ( tsc )  . 
the us examinations were optimized to patient 1 3 404 radiol med ( 2016 ) 121 : 402408 table 2 comparison of renal involvement between cgs and tsc groups age and weight . 
the us images were analyzed systematically by two pediatric radiologists ( either on hard films or on a pacs when available ) and the conclusions were drawn after consensus between the for each us examination , the data that were analyzed included the following : renal lengthmeasured on a mid - sagittal scan expressed in standard deviation to the mean in relation with the age of the patient . cortical echogenicity as compared to the liver or spleen ( defined as increased , equal to or decreased )  . cortico - medullary differentiation ( cmd ) expressed as present , absent or reversed . pyelo - calyceal dilatation above 10 mm measured on a transverse scan of the kidney ( present or absent )  . presence of renal lesions hyperechoic lesions aml ( macro angiomyolipoma > 3 mm ; microangiomyolipoma < 3 mm ) hypoechoic echofree lesions cysts ( > or < 10 mm diameter ; > or < 10 lesions ; location )  . other tumor ? complicated cysts or aml ? whenever a ct scan was performed , the technique was optimized according to the childs age and weight to limit irradiation . 
mr imaging sequences were optimized as well in relation to the patient age and weight as well as according to the type of lesion . results there were 55 patients with tsc , and among them 5 had the cgs ( 9 % ) ( one with antenatal diagnosis )  . 
the mean age at diagnosis was 7.6 months ( 119 months ) for patients with classical tsc ; 5.6 months ( 115 months ) for the cases with cgs . imaging data were collected for 53 out of 55 children . 
no single patient with cgs had an aml as an isolated finding ( table 2 )  . according to the type of lesions demonstrated on us , the series was split into four groups . 
renal cysts encountered in patients with the classical form of tsc measured less than or 1 cm for 14 patients , and 3 cm in 1 single patient . the renal size was normal for 51 children . 
both were also the only ones to display no cmd . the pyelo - calyceal system was never dilated . the us and clinical findings in tsc with and without the cgs are detailed and compared in tables 2 and 3 . as mentioned , 32 patients had more than one us examination . 
one patient with a cgs had a renal failure stage 2 at 7 years . discussion tsc corresponds to a phacomatosis with dominant transmission trait that is related to mutations of two specific genes , tsc1 and tsc2 [ 2 , 3 ]  . 
the association remains quite rare representing only 5 / 55 patients ( 9 % ) in our series . the morbidity and mortality in patients ( mainly adults ) affected by the disease is mainly in relation with the renal involvement . 
complications of aml are usually related to bleedings , whereas infection and renal failure are the main complications of the cgs [ 14 ]  . 1 3 radiol med ( 2016 ) 121 : 402408 406 fig . 
the kidney is markedly enlarged , there is no cmd there are few descriptions of the range of renal lesionsand especially the cystic lesionsin a large pediatric cohort affected by classical tsc or the cgs [ 15 ]  . 
as the complications that develop in classical the tsc and in csg are clearly different , it would be interesting to differentiate between the two . renal involvement was demonstrated in 30 / 53 patients ( 56.5 % ) of our series which is slightly higher than in most series ranging from 40 to 55 % [ 6 , 10 , 15 ]  . 
seventyfive percent of the renal lesions in our series were detected before the age of 10 years . as expected , two types of renal lesions were encountered aml and cysts as isolated lesions or in combination . 
the diagnosis of tsc and of the renal involvement ( especially of the cysts ) was achieved at a younger age when it was part of the cgs ( at a mean age of 7.6 for classical tsc compared to 5.6 months for cgs )  . 
some us criteria can help to suggest the diagnosis of cgs including the larger number of cysts , their larger size and earlier discovery of renal lesions compared to classical tsc . 
the mechanism of trauma is quite similar to that of the adults , but there are important physiologic differences between children and adults in this field , such as the smaller blood vessels and the high vasoconstrictive response , leading to the spreading of a non - operative management . 
the early imaging of children undergoing a low - energy trauma can be performed by ceus , a valuable diagnostic tool to demonstrate solid organ injuries with almost the same sensitivity of ct scans ; nevertheless , as for as urinary tract injuries , mdct remains still the technique of choice , because of its high sensitivity and accuracy , helping to discriminate between an intraperitoneal form a retroperitoneal urinary leakage , requiring two different managements . 
 in this review we present various imaging findings of blunt abdominal trauma in children . keywords emergency radiology trauma imaging blunt abdominal trauma pediatric radiology solid organ injury contrast - enhanced ultrasound ceus contrast media multidetector computed tomography mdct * vittorio miele vmiele@sirm.org 1 department of emergency radiology , azienda ospedaliera s . 
camillo - forlanini , circonvallazione gianicolense , 87 , 00152 rome , italy 2 department of medicine and health sciences , universit del molise , campobasso , italy introduction trauma is the main cause of mortality and morbidity in pediatric patients , and the abdomen is the second most common site of injury . 
the leading cause of injury is related to high - energy trauma , as occurs in vehicle accidents , car vs pedestrian accidents , and falls ; but these causes vary according to the age : toddlers with hometraumas , children with sports trauma , and teenagers with vehicle road accidents . 
in these conditions , a multi - organ involvement must be considered , including not only the abdomen but also head , chest and limbs [ 1 , 2 ]  . the clinical - anamnestic exam and the triage of a child may appear very difficult , in relation to the patients age , or in case of unconsciousness . 
1 blunt abdominal trauma : flow chart of diagnostic imaging in high - energy trauma and lowenergy trauma radiol med ( 2016 ) 121 : 409430 ct is performed , which is the gold standard in the evaluation of the injured patient [ 59 ]  . after the initial evaluation and during follow - up procedures , the injured child must be monitored according to radioprotection criteria ( alara principles ) , keeping in mind the patients medical condition and laboratory exams [ 10 , 11 ]  . a child reports less frequently bone fractures ( e.g. , ribs ) due to a major flexibility in the bone structure of his body . 
 this is why the absence of bone fractures in a child does not imply a low - level energy impact , whereas the presence of bone fractures confirms a high - level energy trauma . besides , the protection provided by the lower ribs on abdominal parenchymal organs in the child is lower , both for the major flexibility of the ribs and for the relatively bigger dimension of liver , spleen , and kidneys which protrude from the ribs , thus being directly exposed to the impact . 
the diaphragm muscle itself , which is in a more horizontal position , pushes down the liver and the spleen contributing to the protrusion from the ribs . in addition , the abdominal wall is thinner ; there is less fat tissue in both subcutaneous and the intra - abdominal site , where it wraps parenchymal organs and all structures , partially absorbing the impact energy involved . in the management of traumatized pediatric patient , non - operative strategy is highly followed with respect to an adult patient , thus requesting surgery only if strictly needed . non - operative management is ideal for pediatric patients as their blood vessels are smaller than those in adults , and there is a major vasoconstrictive response , so visceral organ bleeding tends to be self - limited despite the severity of trauma [ 12 , 13 ]  . at present , the choice of considering surgery is not strictly linked to the severity of the lesions or to the number of organs involved , but to the capacity of normalize the hemodynamic condition despite all the pharmacological therapy in a maximum range of 6 h . liver , bowel , and spleen are highly vascularized organs , so the risk of heavy bleeding is quite serious . 
in all issues , the ct active bleeding detection is a sign of severity and alarm , but still it does not mean that surgery is needed if hemodynamic values are normal . only bowel lesions always need surgery due to the high risk of bacterial contamination in the peritoneal cavity in case of traumatic perforation , not like parenchymal lesions [ 14 ]  . imaging techniques in high - energy blunt abdominal trauma , emergency us is performed in the emergency room on the unstable patient through e - fast technique to depict the eventual hemoperitoneum in the four standard abdominal areas . 
the aim of the exam was to depict in real - time a huge hemoperitoneum , that may be the cause of hemodynamic instability , which requires an immediate surgery . 1 3 radiol med ( 2016 ) 121 : 409430 in low - energy or localized trauma , basic us is fundamental not only to evaluate the presence of hemoperitoneum but also to highlight parenchymal injuries [ 1517 ]  . for the latter purpose , its diagnostic efficiency highly improved by the introduction of second - generation blood pool contrast agent , performing the contrast - enhancedultrasound ( ceus )  . 
furthermore , it can depict active bleeding as a negative prognostic factor even if in a less accurate way as to ct [ 1821 ]  . few studies have been carried on the diagnostic performance of ceus in children [ 2224 ] , because ultrasound contrast agents are still off - label in pediatric field . 
nevertheless , a large survey was performed about this topic , including the use of contrast media in intravenous route also : the findings suggest a favorable safety profile of ultrasound contrast agents ( uscas ) in children [ 25 ]  . the examination , for which it is necessary to obtain parents informed content , requires the injection of us contrast medium , consisting in perfluorocarbon or sulfur hexafluoride , encapsulated by a very resistent phospholipid shell , composed by stabilized gas microbubbles ( 17 micron ) , which are blood - pool agents with a non - linear reverberation . 
 the overall time needed is around 5 min . the us contrast medium elimination is rapid : after around 15 min all the microbubbles break and the sulfur is eliminated through the lungs . 
2 ceus technique possible and correct to perform a second dose of us contrast medium to solve any type of diagnostic doubt [ 3033 ]  . the main benefits of us and ceus concern different aspects , as to its rapid performing , the accuracy and the possibility of avoiding unnecessary ct exams , thus reducing radio - exposure risks . ceus limits are quite similar as those of basic us : the cost of contrast media , need for scanners with dedicated softwares , longer examination times and lack of full and wide view ; it is strongly operator - dependent and it does not allow a complete abdominal survey because of problems related to lesion location ( such as pancreas behind bowel or stomach , aorta in obese patients , a fatty liver ) ; but the largest limit of ceus , also according to our experiences [ 34 ] , is the poor ability to detect active bleeding and injuries to the urinary tract . 
as for as the latter one , we have to remember that uscas are intravascular and are unsuitable for demonstrating extravasation in the renal collecting system , also because they are characterized by lung excretion . ct is the imaging method of choice in the evaluation of abdominal and pelvic injuries after blunt trauma in hemodynamically stable children . ct scans are obtained from the lower chest to the pubic symphysis . 
unenhanced ct scan , if instead performed , allows highlighting abdominal presence of free air , parenchymal or mesenteric hematoma and bone fractures . 1 3 412 radiol med ( 2016 ) 121 : 409430 fig . 
ce - ct , c axial scan and d coronal reconstruction confirm the intraparenchymal laceration without perihepatic fluid cllection study with oral contrast medium administration is not recommended , due to the little advantage compared to the complexity of its administration in major trauma patients [ 3537 ]  . a 3 - mm thickness scan allows performing good quality imaging and subsequent good quality reconstructions without exposure to excessive radiation . 1 3 radiol med ( 2016 ) 121 : 409430 fig . 
ce - ct , c axial scan and d coronal reconstruction confirm ceus findings the iodine intravenous contrast medium volume traumatic injuries depends on the patients weight ( approximately 2 ml / kg )  . the ct technique has two contrast - enhanced phases : an arterial phase which is extended to all the body , to depict vascular injury or active bleeding , and an abdominal portal phase , to evaluate parenchymal and hollow viscera injury . in the suspect of urinary tract injury , if the patients clinical conditions are favorable , a later phase after 5 min is performed . in alternative , in case of bladder injury suspect , a retrograde distension with air may allow to better demonstrate the wall injury , especially in the anterior wall . ct exam must always be completed with bidimensional reconstructions , on sagittal and coronal images , which are of fundamental help in understanding the extension of the injury . 
for bone component evaluation , 3d reconstructions with volume rendering ( vr ) can be used . liver hepatic lesions are to be found in 1030 % blunt abdominal trauma ; in many statistics the liver is considered the most involved organ , both with isolated lesions and with lesions involving other organs , mainly the spleen . 
lesions are often asymptomatic and in 70 % of the cases they can be treated in a non - operative way . hepatic parenchymal lesions can extend and involve biliary ducts and blood vessels . 
b ce - ct , axial scan , confirms ceus finding by peritoneum ; in these cases the blood expansion will occur in the retroperitoneal space [ 38 , 39 ]  . the most used classification of the severity range of hepatic lesions is that of the american association for the surgery of trauma ( aast )  . 
in pediatric patients , in which the trauma management tends to be non - operative , the grading of parenchymal lesion is not the main factor in the treatment decision ( surgical or conservative ) , but other elements are involved , such as the hemodynamic stability and the multi - organ involvement . 
the severity of the lesion will determine the hospitalization period and the restrictions to be adopted after hospital discharge . right hypochondrium location , immediately below the diaphragm , rib cage , and the intestinal gas cause an even more difficult us evaluation of hepatic dome and of the lateral segments , especially in non - cooperative patients . 
even if in small amounts , the hemoperitoneum detection appears very clear , while hepatic lesion us evaluation , especially in the smallest lesions , can be difficult . lesions can present different shapes , unclear borders , and iso - hyperechoic echostructure for the presence of fresh blood . 
in some cases it is possible to see the presence of hyperechoic spots due to active bleeding in the anechoic lesion [ 3941 ]  . in a study performed by valentino et al . 
on 133 hemodynamically stable patients undergoing blunt abdominal trauma , the authors compared the diagnostic performance of ceus with that of the ct , considered as the gold standard ; ceus revealed 81 / 84 traumatic injuries identified at ct and ruled out traumatic injuries in 48 / 49 negative at ct , demonstrating the high accuracy of ceus with respect to us , proposing this technique as a valuable first - line approach for the early evaluation of patients with blunt abdominal trauma [ 42 ]  . in us follow - up , the size of the lesion will decrease , changing the echostructure from iso - hyperechoic to anechoic in time ; even the hematomas will show the same echostructural changes together with the decrease in the size until the disappearing of the hematoma itself . 
with ceus the avascular area will show a progressive reduction in size and well - defined margins . contrast - enhanced ct well depicts a hepatic laceration as a hypodense area , with a variable shape . 
when the laceration reaches the capsular surface and breaks the glissonian capsule , the hemoperitoneum always occurs ; this is depictable through unenhanced ct scans , appearing as a high - density fluid , around 40 uh . when the laceration does not reach the capsule , hematoma occurs , and it can be intraparenchymal and / or subcapsular . 
when it is intraparenchymal , it is possible to depict in basal phase ct , as a fuzzy hyperdense zone in the hepatic parenchyma , due to recent bleeding ; after intravenous contrast medium administration , hematoma will appear hypodense compared to the normal enhanced parenchyma ; active bleeding in the hematoma can be appreciable . 
avascular segments will appear hypodense after intravenous contrast mediuwhen post - traumatic hepatic artery pseudoaneurysm is seen through ct as hyperdense focus in arterial phase within hepatic laceration , it is necessary to suggest an emergency hembolization , even in case of hemodynamic stability , as there is a high risk of rupture ( around 80 % )  . the significance of periportal low hypodensity zones has been matter of discussion ; they have been considered a specific sign of hepatic trauma in the past . 
in fact , this issue is not only appreciable in traumatic lesions ; it seems to be linked not only to specific organ lesion but also to an overflow in linfatic vessels in periportal spaces , due to a sudden increase in the central venous pressure caused by too much fluid provided during the rescue phase [ 43 , 44 ]  . during the follow - up , lesions treated non operatively after 1 month appear hypodense , due to reabsorbing of the corpusculated component ; they gradually reduce their volume , usually to complete resolution , eventually leaving a small parenchymal cyst or a calcification . complications in hepatic trauma are rare ; they usually occur in the first month and the clinical symptoms are fever , hypotension , peritonitis , etc . 
further complications may include : ascessualization of the lesion in the first weeks : biloma , occurring between 12 days and 6 weeks ; hepatic artery pseudoaneurysm , subcapsular hepatic hematoma due to late bleeding and choleperitoneum . spleen the spleen is the most vascularized organ of the body : in fact around 350 l of blood flows through it every day ; this is why its injury is a potential life - threatening situation , exposing the patient to a massive hemoperitoneuwhile in adults the spleen is partially protected by the rib cage , in children , it is bigger and protrudes from ribs cage and it is often involved in blunt abdominal trauma , with a frequency of 25 % of the cases both as isolated lesion and as multiorgan lesions . even for splenic lesions , as for hepatic lesions , the most used injury severity classification is that of aast , which is not directly linked to the need of an operative management . 
 in fact , if the patient is hemodynamically stable , despite hemoperitoneum or self - limited bleeding , the conservative management is recommended , considering its advantages , both because the immunitary function of the organ is preserved and because early and late complications caused by surgery are prevented , shortening hospitalization . 
hemodynamic instability or the possibility of its happening is the main factor to perform splenectomy . splenic injuries have different shapes , linear or branched or complex ; they can be associated to the presence of hemoperitoneum , in case of splenic capsula rupture , or to subcapsular or intraparenchymal hematoma , if the capsula is undamaged , around 25 % of cases . hemoperitoneum linked to capsular lesion is most frequent when the hilum region is involved ; furthermore , in this case , blood will flow along the splenorenal ligament at first , but then it will reach the retroperitoneal zone , in the anterior left pararenal space and around the pancreatic tail , as demonstrated by sivit et al . 
ce - ct , c axial scan and d coronal ct reconstruction confirm size and shape of the lesion and also the presence of active bleeding ( black arrows ) young patients undergoing blunt trauma [ 45 ]  . 
the authors demonstrated that in 96 patients with splenic blunt trauma , extraperitoneal fluid was observed in 8 ( 8 % ) of them , restricted to the anterior pararenal space ; this fluid was seen to separate the splenic vein and pancreas in 25 % of cases , and in 38 of the 1608 patients with blunt trauma not causing splenic injury , was associated with pancreatic injury in 17 / 38 ( 45 % ) children . 
the authors stressed to keep in mind that fluid in the anterior pararenal space and between splenic vein and pancreas might be seen in isolated splenic injuries , a feature useful to reduce errors in interpretation . the spleen is considered to be a difficult organ to be evaluated by us , because of the interposition of coasts and the splenic flexure , especially as for as the upper pole and the subphrenic region . 
 often , the most evident sign of splenic lesion is the presence of an hypo - anechoic fluid collection in the subcapsular or perisplenic space [ 46 ]  . parenchymal lesions can be very difficult to recognize , especially when perisplenic fluid is not reported . 
parenchymal lesions evaluation must be performed during venous phase , 120240 s after contrast medium injection , when normal parenchyma shows high homogeneous echogenicity which is absent in arterial phase . 
ceus aspect of splenic lesions is anechoic , clearly highlighted as to normal hyperechoic parenchyma the extension of the lesion to the splenic capsula and the capsular interruption is highly recognizable . 
ceus sensitivity in depicting splenic parenchymal lesions is very similar to that performed by ct , allowing a detailed follow - up even during the bed - rest phase , without radiation exposure [ 31 ]  . the sensitivity and specificity of ct in the detection of splenic injury is close to 100 % . splenic lesions are correctly shown in the portal phase , and are usually represented by lacerations , that can involve 1 3 radiol med ( 2016 ) 121 : 409430 fig . 
9 female , 8 years old , direct trauma on the left hypocondriua ceus , b ce - ct : subtle laceration of spleen lower pole ( white arrow )  . 
c sagittal and d coronal reconstructions : evidence of posttraumatic intraparenchymal artero - venous fistula , also well demonstrated in e 3d vr reconstruction fragments that go along with huge hemoperitoneum , can be clinically related to hemodynamic instability . 
these lesions request urgent surgery as they represent a high death risk as a consequence of hemorrhagic shock . the presence of congenital clefts can lead to misinterpretation and false - positive patients . 
we have to consider that congenital clefts have regular and homogeneous welldefined profiles as to the lacerations that appear more irregular and are often linked to subcapsular and / or perisplenic fluid [ 47 , 48 ]  . besides being used in shattered spleen management , operative handling is performed in case of intraparenchymal active bleeding and especially in peritoneal cavity active bleeding . 
angiographic technique is reported to be more safe compared to the surgery , and it carries a mortality rate in the first 6 months of around 2.4 % compared to 8 % . urinary system : kidneys , urinary tract , bladder and urethra the kidneys are the third most involved organ in blunt abdominal trauma ( about 80 % of the cases ) , followed by external genitals , bladder , urethra and ureter . parenchymal lesions are usually the result of a direct impact , while decelerative forces cause vascular and / or urinary tract lesions [ 49 , 50 ]  . clinical evaluation of renal trauma in pediatric patients is often difficult ; the typical and more specific symptom is hematuria . 
gross hematuria is the most significant sign of renal trauma , found in more than 95 % of cases , but not always related to the severity of the trauma . 
ce - ct , c axial scan and d coronal reconstruction confirm the renal fracture and the perirenal fluid collection can also be found in severe traumatic lesion as in 24 % of patients with renal artery thrombosis , and in up to 1 / 3 of cases of pyelo - ureteral junction lesions . 
gross hematuria is more frequent in penetrating trauma compared to blunt trauma and it is rare in trauma due to deceleration force . aast classification divides renal trauma into five classes according to the renal damage parenchymal extension , to the urinary system involvement or to the vascular pedicle injury . 
the two kidneys must be explored separately with two different boluses ; their exploration can sometimes be difficult because the left one , in particular , can be hidden by artifacts and bowel gas . at ceus lesions appear as hypo - anechoic areas in the context of highly echogenic renal parenchyma . 
before contrast medium injection the renal contusion can be seen as a hyperdense parenchymal area ; after contrast medium , it appears as a focal or diffuse region of delayed contrast enhancement . renal lacerations appear as linear low - attenuation areas in the parenchyma . 
active bleeding can be detected within the tear [ 50 , 51 ]  . in a series of 25 children with blunt renal and ureteral trauma , siegel et al . 
 the authors demonstrated that the perirenal or periureteral fluid collection did not correlate with the extent of renal injury , whereas interfascial , anterior pararenal and psoas muscle fluid correlated in such a way with renal fracture and pedicle avulsion [ 51 ]  . a segmental renal infarct occurs in case of injury to a segmental renal artery : at enhanced ct scan it is like a peripheral wedge - shaped area of non - enhancing parenchyma . 
ce - ct , c axial scan and d coronal reconstruction confirm the complete fracture of the middle part of the horseshoe kidney , with separation of renal fragments injury and must be treated promptly because permanent , progressive loss of renal function begins 2 h after trauma . subcapsular or perinephric hematoma can be found in any renal trauma . 
a subcapsular hematoma is limited in its extension by the renal capsule , causing mass effect on renal profile , whereas a perinephric hematoma is distributed throughout the perirenal space , if it is relevant can be dislocate the kidney . 
at the unenhanced ct scan , the hematoma is typically hyperintense , while it becomes hypointense after intravenous contrast mediuthe assessment of any active bleeding in the early stages after contrast medium is very important ; in fact in case of severe bleeding the management of the patient changes from conservative to operative . the assessment of any lesion of the urinary tract must be done with delayed scans . 
seldom , urinary leakage and / or hemorrhage may reach the pelvis due to direct communication between the perirenal space in the abdomen and the prevesical extraperitoneal space in the pelvis . 
usually the management of renal collecting system injury is non - operative , mostly if the leak is confined to the perirenal space ; sometimes , urinary tract obstruction requiring surgical repair may result [ 51 ]  . bladder and urethra due to its anatomical position , well protected by the pelvic ring , injuries of the bladder are rare , occurring in 12 % of trauma patients , most commonly secondary to blunt trauma due to a high - energy injury . 
the bladder in children is considered an intraperitoneal organ in contrast to the adult where it is considered an organ mainly extraperitoneal . pelvic fractures , especially those in the pelvic ring , mostly the bilateral ones , are frequently associated with lower urinary tract injuries , nearly 8090 % of cases , though only 510 % of pelvic fractures result in bladder injury . 
two mechanisms are involved : the first involves shearing forces at deceleration resulting in injury at the fixed sites of pelvic 1 3 422 radiol med ( 2016 ) 121 : 409430 fig . 
intraperitoneal blunt injury is due to rapid deceleration that determines a sudden increase of intravesical pressure , resulting in a burst - type injury . the distention at the time of the trauma allows the rupture of the bladder . traumatic lesion starts from wall contusion to the rupture . 
however , the overall incidence is lower because the pelvic fracture is also lower in children [ 5458 ]  . gross hematuria is believed to be associated with more significant injuries , as in case of rupture , while microhematuria has been more commonly related to bladder contusion . in addition to hematuria that is present in approximately 90 % of bladder trauma , the inability to void or suprapubic pain may occur . imaging of the bladder , if indicated , may consist of cystography and is performed in the clinically stable patient . 
 ct cystography is performed more liberally because of the central role of ct scanning in trauma assessment . the ct has 95 % sensitivity and 100 % specificity in the detection of bladder rupture ; some studies point to a lower accuracy in intraperitoneal rupture , with values of sensitivity and specificity of 80 and 99 % . 
in a study performed by sivit et al . , ct revealed iv contrast medium extravasation in all patients with bladder rupture , recognizing if intra or retro - peritoneal in a very precise way ; this latter point is even more important knowing that an intraperitoneal rupture needs surgical repair , while the extraperitoneal one does not [ 54 ]  . for ct cystography , the bladder is filled retrograde with contrast medium and the scan is performed after 300 400 ml of contrast is instilled . 
characteristic patterns of intraperitoneal contrast leakage include pooling in the cul - de - sac , paracolic gutter , or retrohepatic space on ct or outlining of bowel loops . another way to evaluate the integrity of the bladder through ct exam is the retrograde gas distension . 
the advantage is the easier air distribution which allows even in absence of overdistension of the bladder , to hypothesize the presence of a rupture , through the flow of extraluminal air bubbles , even in case of small lesions , or lesions located on the anterior wall . most of the extraperitoneal bladder injuries can be managed conservatively with catheter drainage ; in other cases , such as for penetrating injuries , surgery is requested . traumatic lesions of the urethra are , for anatomical reasons , more frequent in males . female urethral injuries are uncommon , 06 % , because the urethra itself is very short , and usually all involved injuries are associated with pelvic fracture as a result of laceration by bone fragments [ 58 ]  . the clinical suspicion in the male is confirmed by gross blood at the urethral meatus and / or scrotal hematoma , while in the female by vaginal bleeding , pelvic fracture and bleeding , perineal ecchymosis and pelvic fracture . 1 3 radiol med ( 2016 ) 121 : 409430 when gross blood is present at the urethral meatus , retrograde urethrography ( rug ) is indicated before catheterization ; if blind catheter placement is performed , a partial injury can accidentally become a complete injury . early management of most posterior urethral injuries involves urinary diversion with a suprapubic catheter . 
most posterior injuries can be managed with urinary diversion and delayed ( 36 months ) reconstruction , following resorption of the pelvic hematoma . endoscopic techniques of primary realignment show promise in potentially decreasing rates of stricture formation while providing equivalent results with regard to continence and erectile disfunction . pancreas pancreatic trauma is less common because of its deep position , relatively protected by the abdominal wall and the surrounding fat . 
in the child , however , this protection is less effective than in the adult , due to the reduced development of the muscle wall and the relatively poor quantity of superficial and deep adipose tissue and , owing to its retroperitoneal location , mortality is quite high , ranging from 70 to 80 % when there is also involvement of aorta , the superior mesenteric artery or vena cava . the pancreatic trauma happens in 312 % of blunt abdominal trauma : it rarely occurs as isolated injury but usually 60 % of cases are associated with lesions of the liver , spleen or the duodenu this means that in patients with pancreatic lesions morbidity and mortality increase [ 59 , 60 ]  . the detection of lesions limited to the parenchyma may allow conservative treatment , while in case of duct injury the management depends on the site of the lesion . 
if the distal portion on the left side of the spine ( grade iii ) is involved , duct stenting or surgery for partial resection of the pancreas is needed . 
lesions in the proximal part of the duct are of greater severity ( grade iv ) , but surgical treatment is more complex for their deep location ; therefore , they are managed more often by the positioning of a stent , preventing surgery . the pancreatic trauma is the leading cause of pancreatitis in children . because of its deep position and the interposition of intestinal gas content , the pancreas is a difficult organ to evaluate through us exam ; however , in children the evaluation is easier , mainly because of their physical structure . the pancreatic lesions typically appear as total or partial glandular lacerations , in this case with organ separation into two parts . the direct sign of injury is the detection of a tear as a hypoechoic intraparenchymal rhyme ; it can be difficult to find it on ultrasound exa indirect signs can be more easily depictable : focal or diffused pancreatic swelling , unclear organ profiles , focal or diffuse hyperechogenicity of the parenchyma and presence of fluid periglandular collection [ 46 ]  . there are few reports on the use of ceus in pancreatic trauma [ 60 ]  . in one of these , lv et al . , in a series of 22 consecutive patients undergoing blunt pancreatic trauma , reported an excellent sensitivity of ceus in detecting pancreatic injuries compared with ct as the gold standard . 
the presence of hypodense fluid due to lesion of the pancreatic duct , or the presence of hyperdense fluid in case of hematoma within the anterior pararenal space and / or periglandular , although not specific , is a good indicator of pancreatic trauma and can suggest the suspicion of traumatic lesion . 
 periglandular post - traumatic collections , due to duct injury , often evolve into pseudocysts and tend to resolve spontaneously or be subsequently subject to percutaneous drainage or surgery [ 3 , 5 ]  . 1 3 424 radiol med ( 2016 ) 121 : 409430 fig . 
moreover , the use of oral contrast medium is not widely used in the traumatized patient because it takes more time in carrying out the exam . the complete rupture of the intestine most commonly occurs in the mid to distal part of the small intestine . 
ce - ct , ac axial scans show the fracture of the left hepatic lobe ( open arrow ) and the laceration of the pancreatic head ( white arrow )  . 
traumatic adrenal lesions are more frequent in high - energy trauma with an injury severity score ( iss > 15 ) , associated with other lesions up to 50 % . usually traumatic adrenal lesion is unilateral ( > 90 % ) with a considerable prevalence for the right adrenal gland ( 8590 % ) , depending on three main causes : abrupt compression between the liver and lumbar vertebral bodies ; the damage of small vessel due to a deceleration ; the sudden increase of adrenal venous pressure due to a compression accidental . us technique has low sensitivity in detecting traumatic adrenal lesions , especially for their association with multiorgan lesions , rib fractures and pneumothorax . ct is the gold standard exam in detecting traumatic adrenal gland lesions . 
main ct details are hematoma around 6083 % , overall adrenal hemorrhage around 943 % , the homogeneous swelling of the adrenal gland around 10 % , and the adrenal rupture that is very rare . furthermore , it is possible to detect signs associated with traumatic lesion such as hemorrhagic suffusion of periadrenal fat , retroperitoneal hemorrhage and active bleeding . unrecognized adrenal lesions can cause late hemorrhage and infections . 
in case of massive hemorrhage , ivc can be compressed causing thrombosis . bilateral traumatic adrenal lesions are very rare , less than 1 % ; it is still unknown if they can cause severe endocrin abnormalities , i.e. 
 ce - ct , b axial scan , c coronal and d sagittal reconstruction s demonstrate a large hematoma of the third duodenal portion , displacing and narrowing the intestinal lumen fig . 
a axial ct scan and b coronal ct reconstruction show a fluid collection in the mesentery of the right hypochondrium , with active bleeding ( white arrow ) 1 3 radiol med ( 2016 ) 121 : 409430 fig . 
it is also appreciable a large adrenal hematoma , with active bleeding ( white arrow ) hypoperfusion complex more than 80 % and many of these children have severe associated multisystem injury [ 63 , 64 ]  . regardless of the hypovolemic shock causes , the radiologist must recognize and identify a complex set of ct details indicating a severe hypoperfusion and that are suggestive of a transition state between severe but compensated hypovolemia and the decompensated state . 
in these cases we have a caliber reduction of aorta and inferior cava vein , a widespread fluid distension of intestinal bowel with thickened and irregular enhancement of bowel wall after contrast medium injection ( shock bowel )  . there will be a considerable enhancement of the mesentery , kidneys and adrenal glands , which will then decrease in the pancreatic and spleen parenchyma . 
it is possible to find periportal low - attenuation zones , peritoneal and retroperitoneal fluid . the detection of these ct details suggesting hypoperfusion is a predictor of a poor outcome ; in fact the reported mortality rate in children with this set of findings at ct is conclusions in a traumatic setting the triage of a child may appear very difficult ; therefore , diagnostic imaging plays an important role in the complex evaluation of an injured child [ 36 ]  . in low - energy trauma and in isolated trauma , the first diagnostic approach in the child can be performed by x - ray , if needed , and ultrasound ( us ) , whose diagnostic accuracy is highly improved because of the introduction of contrast enhanced ultrasonography ( ceus ) , which remarkably increased its sensitivity and specificity in the early detection of solid organ injuries [ 1821 , 33 , 34 , 46 ]  . in high - energy trauma , in the hemodynamically unstable young patient , the first evaluation is performed by e - fast 1 3 428 radiol med ( 2016 ) 121 : 409430 to recognize a possible hemothorax , pneumothorax , and hemoperitoneum . in all stable patients with high - energy trauma , and in those who have been stabilized , contrast - enhanced ct is performed , which is the gold standard in the evaluation of the injured patient [ 59 ]  . when performing a ct scan in a young patient one should always keep in mind the alara principles , because children are particularly susceptible to the associated increased risk of developing malignancy later in life [ 10 , 11 ]  . 
neverthless , the use of ct in the injured child allows a quick evaluation of the entire body in a relatively few time , resulting in improved triage and reducing morbidity and mortality . 
in addition , it has enormously contributed to shift from an operative to a non - operative management . ct staging of solid injuries has been shown to be useful for estimating the time course of healing . 
however , some authors stated that the follow - up imaging of solid injury in asymptomatic children who sustained low - energy or an isolated trauma is probably not necessary [ 3 ]  . 
nevertheless , in the recent years some research advocated the application of ceus in the follow - up of patients with trauma conservatively managed until discharge , both in order to reduce unnecessary ct examinations and to overcome poorly visible traumatic injuries at conventional ultrasound , better revealed using uscas [ 33 , 53 , 6567 ]  . 
taking into account some limits of ceus , such as being operator - dependent , a low coverage and the inability to detect some possible complications , such as bilomas , abscesses , urinary tract , and vascular lesions , the authors obtained interesting results in the follow - up of a cohort including 152 patients , many of them children , with low - energy trauma who underwent follow - up with both ceus , performed at 24 and 72 h and at 1 month from trauma , together with mr [ 68 ]  . 
in this series , mr allowed to better depict the integrity of urinary tract ( not visualized by ceus ) and to highlight the presence of two adrenal glands injuries , dismissed by ceus . 
so , due to its panoramicity , and its high contrast resolution , mr permits a better morphological and temporal trauma staging with respect to the ceus and allows excluding all negative prognostic factors , such as late bleeding , rupture of the urinary tract or additional injuries . 
in total 61 lesions were treated , so subdivided : 10 true aneurysms , 26 pseudoaneurysms , 5 iatrogenic arteriovenous fistulae , 20 arterial ruptures , lacerations or perforations . results immediate technical success was obtained in 60 of 61 lesions ( 98.3 % ) ; in 1 case ( pseudoaneurysm of hepatic artery ) additional embolization of the gastroduodenal artery with microcoils was needed . 
follow - up was available for 57 patients and 59 lesions ; mean period was * gianpaolo carrafiello gcarraf@gmail.com 1 unit of interventional radiology , department of radiology , university of insubria , 71110 heraklion , crete , greece 2 unit of interventional radiology , department of radiology , faculty of medicine , university hospital of heraklion , university of crete , 71110 heraklion , crete , greece 3 vascular surgery department , university of insubria , viale borri , 57 , 21100 varese , va , italy 4 unit of vascular surgery , faculty of medicine , university hospital of heraklion , university of crete , heraklion , greece 5 department of radiology , luigi sacco university hospital , via g.b. 
as summarized in the table 1 , etiologies were iatrogenic ( 27 lesions ) , anastomotic ( 10 lesions ) , traumatic ( 10 lesions ) , atherosclerotic ( 10 lesions ) , post - pancreatitis ( 2 lesion ) , post - radiation ( 1 lesion ) and due to neoplastic infiltration ( 1 lesion )  . usguided compression was attempted , but failed in all non - anastomotic femoral and popliteal pseudoaneurysms and arteriovenous fistulas , while percutaneous thrombin injection was not considered as treatment option due to neck absence . before the intervention , the potential risks and benefits of the procedure were explained in detail , and informed written consent was obtained from each patient . the procedures were performed under local anesthesia through percutaneous femoral approach in 55 cases and through percutaneous axillary / brachial approach in 4 cases . following diagnostic angiography , the arterial lesion was crossed with a 0.035 180 cm hydrophilic angled guide wire ( radiofocus ; terumo , tokio , japan ) supported by a 5f catheter ( glidecath , terumo , tokio , japan ) ; then the hydrophilic guide wire was exchanged with a 0.035 180 or 260 cm super stiff guide wire ( amplatz , boston scientific , miami , fl / usa )  . 
when stiff guidewire was left in visceral arteries , it must not move : a second skilled operator pulls the guidewire when the first operator push the stent in the desired position making sure that the guidewire does not go ahead . 
this manouvre is useful to avoid iatrogenic injuries of the artery . the dimension and the number of stent grafts necessary for the treatment were determined according to the lesions morphology . 
in addition to angiographic success , stabilization of the haematocrit and hemoglobin values was considered as signs of clinical success in cases of arterial laceration , rupture or perforation . follow - up was carried - out by color doppler ultrasound ( cdu ) and ct at 1 , 3 , 6 and 12 months and yearly thereafter . patient and procedural characteristics , as well as clinical outcome are summarized in table 1 . 
in one patient a microcoil ( 4 mm ) was deployed in a branch of deep femoral artery to embolize a pseudoaneurysm of deep femoral artery associated with an iatrogenic femoral arterovenous fistula . 
procedural complications were observed in 5 patients ( 15.3 % ) : 1 haematoma in right iliac fossa and 3 small pseudoaneurysms in the arterial puncture site which resolved spontaneously and 1 distal thrombus embolism of the ipsilateral leg treated by fogarty embolectomy . follow - up was performed for a mean period of 23.52 months ( range 160 months ) ; follow - up is not available for 3 patients because they arrived from near hospitals and transferred after their stabilization . 
two patients died , 9 and 4 months after the procedure , due to pathologies irrelevant to vascular disease treated . during follow - up the following complications were encountered : abscess with retroperitoneal hemorrhage in a patient treated for external iliac artery pseudoaneurysm , which required the removal of the stent graft 1 month after the procedure ; stent graft occlusion ( at 15 and 38 months , respectively ) in 2 patients treated for pseudoaneurysm of subclavian / axillary arteries . 
secondary patency was defined as a patent stent after reintervention for occlusion . in the present study the 1 - year primary patency was 89.47 % , whereas the secondary patency was 96.4 % ( table 2 )  . discussion the fluency plus is a self - expandable eptfe ( expanded polytetrafluoroethylene ) coated nitinol device that carries , on each end , four radio opaque markers , as an aid for precise positioning under fluoroscopic guidance . even if the in - label indications for the employment of the fluency stent graft are the residual stenosis after angioplasty , dissections and occlusions , the device is also well behaving in the treatment of aneurysms , pseudoaneurysms , arteriovenous fistulae and penetrating arterial injuries : the 1 3 radiol med ( 2016 ) 121 : 482493 fig . 
angiography after treatment revealed completely exclusion of aneurysmal dilatation with two fluency stent grafts ( arrow ) fluency stent is flexible , and being made of nitinol , is selfexpandable and thus adapts itself on the vessel wall , reaching an adequate diameter thus excluding these non - obstructive lesions . the vascular lesions treated with the fluency stent graft in this study were iatrogenic arteriovenous fistulae , pseudoaneurysms , aneurysms and arterial ruptures , lacerations or perforations located in peripheral or in visceral arteries . 
 we decided to use stent grafts instead of open surgery due to some important advantages of endovascular repair : local anesthesia , less blood loss and tissue damage , reduction of operative time and morbidity , shorter hospital stay and recovery periods , better tolerance , and reduced healthcare costs . 
in particular , in patients with associated co - morbidities that complicate surgical approaches , stent grafts may be lifesaving in many cases . however , endovascular therapeutic approaches have their own complications , such as stent occlusion , deformation and kinking , loss of vessel branches and intimal hyperplasia after stent graft placement [ 8 ]  . 
moreover , the main disadvantage of stent grafting is related to the adverse events associated with the use of a large introducer sheath , which predisposes to local puncture complications , such as haematoma and pseudoaneurysms . 
 for example , the treatment of visceral arterial lesions with stent graft is often challenging due to the tortuosity and the small caliber of the vessels [ 911 ]  . for many years the only therapeutic option for peripheral aneurysms , pseudoaneurysms and fistulae was surgery , especially in emergency settings [ 12 ]  . 
often a large tissue incision and a large vessel exposure are necessary to achieve vessel repair thus resulting in prolonged hospitalization with associated morbidity [ 13 ] ; furthermore general anesthesia may be inappropriate in patients with multiple co - morbidities . usguided compression repair , a method which initially became popular at many institutions as a less invasive alternative repair method for iatrogenic femoral pseudoaneurysms and arteriovenous fistulas , is both time and labor intensive , and is associated with high failure rate . 
in our cases of non - anastomotic femoral and popliteal pseudoaneurysms and arteriovenous fistulas , initial usguided compression failed , while the injection of thrombin was contraindicated due to the morphology of the pseudoaneurysm ( neck absence ) and the associated risk of thrombosis of the mainstream artery . generally the stent graft is used when it is necessary to guarantee the vessel patency [ 1517 ]  . 
however , especially in non - emergent cases , surgical repair should be discussed as an alternative in young patients , considering the location ( pseudoaneurysms of the popliteal artery , arteriovenous fistula of the common femoral artery / vein )  . 
on the basis of literature data , primary arterial repair without grafting is usually not feasible in a chronic popliteal pseudoaneurysm , due to the chronic nature of the pseudoaneurysm and the presence of fibrosis and inflammation [ 1 , 18 ]  . 
in these cases polytetrafluoroethylene grafts are usually not recommended because the reported frequent thrombosis and graft failure [ 18 ]  . aneurysm resection and primary end - to - end repair can be a safe alternative in particular if they are small - sized aneurysms ( 24 cm ) , surrounded by minimal perianeurismal fibrosis and chronic inflammatory changes [ 18 ]  . 1 3 radiol med ( 2016 ) 121 : 482493 490 fig . 
 post - treatment angiography shows exclusion of arteriovenous fistula by deployment of fluency stent graft ( c ) endovascular repair of peripheral artery pseudoaneurysms seems very attractive , because it theoretically implies low morbidity rates and shorter hospital stay . 
however , experience is still limited , and especially in cases of younger patients , the implantation of a metallic stent for the rest of life seems controversial [ 18 ]  . an additional factor of skepticism may be the deployment of stent graft in highly mobile joint ( knee , shoulder , hip )  . 
there are not in literature studies about surgical approach to repair arteriovenous fistula . in literature most studies describe the treatment of vascular lesions in a single body district : fluency stent grafts have been used for the treatment of several peripheral lesions : subclavian and axillary artery [ 1922 ] , iliac artery and femoral artery [ 4 , 5 , 8 , 14 , 2326 ] , celiac trunk [ 4 , 27 ]  . a recent review underlines the role of endovascular treatment of traumatic subclavian and axillary artery injuries reporting promising results [ 28 ]  . 
literature data from other centers include only few cases and revisions [ 29 ] concluding that endovascular therapy with stent grafting is safe , effective and lifesaving procedure especially when surgery in contraindicated . regarding the treatment of arterial aneurysm and pseudoaneurysm an important step could be a randomized study between the use of covered and flow - diverting stents . 
4 angiography demonstrates contrast extravasation of the right proximal superficial femoral artery due to arterial laceration caused by knife stab wound of the thigh ( a ) ; posttreatment angiography shows sealing of blood extravasation by placement of a 6 40 mm fluency stent graft ( b ) the treatment of visceral and peripheral aneurysms yielded satisfactory results [ 30 ]  . in literature the technical success in the positioning of a fluency stent graft is reported in 100 % of cases , whereas in our series is 98.3 % ( 58 / 59 lesions ) because in 1 case of hepatic common artery pseudoaneurysm it was also necessary to embolize gastroduodenal artery with microcoils . 
 the long - term mean follow - up in our study is longer compared to that reported in previous studies ( 23.52 versus 18 months , respectively ) ; primary patency rates were 89.47 1 3 492 fig . 
reviewing the lung window on non - contrast abdominal ct can be helpful in detection of drug mules . keywords body packer drug smuggling computed tomography windowing introduction drug mules who are carriers with internal concealment of illicit drugs have been a real challenge for emergency radiologic departments for their medico - legal aspects . 
 in contrast , body stuffers , who may be abusers themselves , ingest small amounts of either unwrapped or poorly wrapped drugs pellets when fearing apprehension by the authorities , to dispose of evidence . 
as a result , symptoms of toxicity are more likely to occur in body stuffers due to poor packaging [ 18 ]  . diagnostic imaging plays a crucial role in the early and accurate detection of drug mules . 
although plain radiograph has been used as a screening tool , it is of limited value in body packers with a leakage of the main part of the 1 3 radiol med ( 2016 ) 121 : 472477 packets and also in body stuffers [ 911 ]  . 
computed tomography ( ct ) has become widely accepted as an accurate imaging modality with a high sensitivity and specificity in detection of drug mules ; however , there are legal restraints related to overexposure to radiation , and ct examinations are therefore generally performed in cases with negative abdominal plain films but a high index of suspicion of package concealment . 
in this retrospective study , we evaluated the usefulness of adding lung window to conventional abdominal window in the detection of drug mules on ct . materials and methods institutional review board approved this retrospective study , and informed consent requirement was waived . patients from april 2012 to july 2013 , 42 consecutive individuals with a suspicion of internal concealment of illicit drugs were considered for enrollment in this study . 
a clinical suspicion of drug mule was made by our emergency medicine physicians in subjects who were either brought by the police from airport , prison , or city patrols or in those who came to the emergency unit themselves . 
two subjects who had not an available abdominal ct were excluded from the study . after reviewing the medical record of the subjects , the content ( stimulants , opioids , or a mixture of them with other hallucinogens ) and cover ( nylon , digit , or zipped pack ) of the illicit drugs were recorded . 
if present , clinical symptoms of drug toxicity and results of urine test strip for common illicit drugs were also recorded . identification of positive drug carriers was based on the retrieve of packets from feces in a guarded drug toilet or through the surgery . 
the container leak was assumed in the presence of signs and symptoms of toxicity ( either narcotics or stimulants ) or positive strip test in subjects without a previous history of addiction . 
on the other hand , the passage of three drug free stools was considered a negative result [ 1 ]  . ct scan all abdominal ct scans were performed without intravenous or oral contrast using a single slice ct scanner ( shimadzu 7800 sct scanner , kyoto , japan )  . 
 the images were reviewed by a board certified radiologist with 6 years experience in abdominal imaging and by a radiology resident with training in forensic radiology , who were blinded to the results of the stool examinations or surgery . 
first , the scout ct views were examined especially in cases without a first plain radiograph , and the scans were interpreted in abdominal window ( level 50 ; 500 ; width 450 )  . 
the sensitivity , specificity , negative predictive value ( npv ) , positive predictive value ( ppv ) and accuracy of non - contrast ct were calculated before and after the addition of lung window in all drug mules and in each group of body packers and body stuffers . 
 in addition , youdens index was calculated as follows : sen1 paired t test was used for comparsitivity ing the number of packets detected before and after adding lung window . 
the definite diagnosis was based on the stool exam results and the open surgery 35 ; average age 32 1 3 474 radiol med ( 2016 ) 121 : 472477 fig . 
lung window ( b ) in the same slice apparently shows more packets in stomach which are barely visible in abdominal window findings in 26 and 2 subjects , respectively . 
seven subjects were body packers ; while , 21 subjects were body stuffers . in the body packers group , 4 ingested the body packets , 1 was rectal pusher , and 2 were mixed oral body packer and rectal pusher . 
two body packers ( 28.6 % ) showed symptoms of drug toxicity and positive urine exam ; they ended up in open surgery with ruptured packets being discovered in the operation room . in the body stuffers group , all subjects ingested the illicit drugs . 
more number of packets could be detected in lung window in two cases ( 18 instead of 15 packets in one case ; 10 instead of 8 packets in the other one )  . 
on ct examination , 5 subjects ( 50.0 % ) of the true positive cases had pellets in their stomach and the remainder 5 cases ( 50.0 % ) had the drugs in their colon . 
 in two cases , hyperdense material conforms to the shape of the bowel lumen which was in favor of ruptured drug pellets in the absence of a history of previous contrast material intake . 
table 1 depicts an overview of diagnostic performance of non - contrast ct in total cases , body packers , and body stuffers . discussion on abdominal ct scan of drug mules , detection of illicit drugs in their gastrointestinal tract is usually made by either different density of the drugs from other luminal contents or their distinct and uniform shape or coverage . 
packets composed of radio - dense materials can be easily diagnosed even on plain abdominal x - ray or ct scout view ; however , diagnosis of isodense or hypodense drugs is more difficult . 
 in a case report , manipulation of the image windowing ( level 175 ; width 600 ) on ct has revealed drug packets in the bowel which had been undetected in abdominal windows [ 17 ]  . 
addition of lung window on non - contrast ct examination may make the concealed illicit drugs more conspicuous because the drugs may have a hypodense cover ( e.g. , latex or plastic ) or they may be surrounded by a crescent of air trapped while sealing ; the latter has been described as double condom appearance [ 1 , 6 ]  . we found that accuracy of ct scan for detection of body packers was 100 % which was in concordance with previous studies [ 13 , 16 , 19 ]  . 
in addition , using lung window resulted in detection of a more number of concealed illicit drugs . the small amount of drug pellets in the stuffers in comparison to body packers makes their detection more difficult . 
 [ 12 ] mentioned in their study , the outer halo surrounding an inner spherical high - attenuating 1 3 476 radiol med ( 2016 ) 121 : 472477 fig . 
3 abdominal window ( a , b ) depicts small hyperdense pellets in ascending colon in this body stuffer which are not detectable in their respective slices in lung window ( c , d ) since they do not have enough covering wrap around to make them recognizable especially in lung window structure , corresponding to the cocaine , is the key radiological feature in detection of small drug pellets and is better visualized by lung window . 
this also corresponds to relatively high rate of ruptured stuffers and positive toxic signs in the subjects . the diagnostic value of adding positive oral contrast medium to plain radiographs and ct scans is somehow controversial depending on the density and coverage of the packets . 
non - contrast ct was also shown to be a better option for the diagnosis of body stuffing because of the lack of proper coverage around the drug substances in body stuffers in addition to the hyperdense content of the baggies [ 24 ]  . 
moreover , contrast agents stimulate the peristalsis determining an osmotic intestinal inflow , which would be contraindicated in small bowel obstruction . the ct number is not a reliable indicator for the type of drug being transported by a body packer because it is highly dependent on concentration and compression of the substance . 
the heroin body packs had higher attenuation values with increasing tube voltage while cocaine body packs showed lower attenuation values with increasing tube voltage . the ct characteristics of drug pellets vary , depending on their geographic origin , and further studies are encouraged in this regard . 
 however , at the cost of a longer interpretation time , it may 1 3 radiol med ( 2016 ) 121 : 472477 be beneficial in the evaluation of suspected drug mules , and further investigation in a larger group of subjects seems necessary to generalize the results of this study . 
our study had other limitations as well ; ct scans had been performed with a single row detector scanner with slice thickness of 10 mm and no multiplanar reconstruction was available which would partially explain our low sensitivity in body stuffers . 
the number of subjects in each subgroup ( packers and stuffers ) was small which would have decreased the validity of our statistical analysis . in conclusion , the results of our study showed that the diagnostic performance of non - contrast ct was 100 % in body packers even without the addition of lung window scans . 
chi - square , students t test and univariate analysis were used for statistical analysis . results there were no statistically significant differences in demographic features and nodule properties from diagnostic results of fine needle aspiration biopsy of thyroid nodules . 
no : 27 , okmeydan - s isliistanbul , 34384 istanbul , turkey 2 sisli hamidiye etfal education and research hospital , radiology clinic , istanbul , turkey conclusion obtaining adequate material in fine needle aspiration biopsy from thyroid nodules is a challenging issue and the results are controversial . 
since we obtained the best ratio with 23 g needles , we recommend interventional radiologists to use 23 g needles as far as possible and not to consider needles thicker needles than 22 g or thinner than 25 g . 
nodule features and demographic features did not have an effect on obtaining adequate cytological material . keywords needle aspiration biopsy inadequate material thyroid nodules fine introduction thyroid nodules are common and present difficulties in clinical diagnosis . 
although thyroid nodules are often seen , thyroid malignancies are rare and represent only 1 % of all malignant neoplasms [ 1 ]  . thyroid malignancies usually show an indolent nature and life expectancy is long after diagnosis , though early diagnosis is still important . 
the main problem of detected nodules in the thyroid gland is making a distinction whether nodule is benign or malignant . thyroid function tests , scintigraphy and usg are routinely used in the diagnosis of thyroid nodules [ 3 ]  . 
today fnab is the most valuable method used in the diagnosis of thyroid nodules [ 46 ]  . fnabs most important limiting feature is the possibility of obtaining inadequate target cells from the sample material and even when there is sample material , the cells may be masked by other cells especially by red blood cells . 
 in summary , fnab is not the gold standard , but is a good screening method for diagnosis . the main causes of insufficient material can be summarized as follows : lack of sufficient cells from cystic , necrotic and calcified areas , small and inaccessible nodules , nodules showing compact architecture and blood cells masking target cells as a result of the traumatic effect of the procedure [ 7 ]  . on the other hand , onsite adequacy assessment of thyroid fnas significantly reduces the number of nondiagnostic aspirates [ 8 ]  . 
 to our knowledge , our study represents the largest series in evaluating three different sizes of needles ( 22 , 23 and 25 g )  . the aim of this prospective study was to evaluate factors that can affect the diagnostic result ratio in fine needle aspiration biopsy of thyroid nodules . patients and methods patients a total of 664 patients and 696 thyroid nodules were prospectively reviewed by performing usg guided biopsy in institute between february and november 2015 . 
 table 1 summarizes the baseline characteristics of the study . only nodules larger than or equal to 1 cm in size were evaluated to exclude the effect of nodule size . fnab procedure before the procedure , all patients were questioned for contraindications such as anticoagulant medications or overanxiety preventing the procedure . 
these include demographic features , nodule size , nodule composition , vascularity , mc and needle thickness [ 7 ]  . patient dependent causes are limitation of throat motion and patient unexpected activity as a result of anxiety during the operation [ 8 ]  . each group contained similar numbers of nodules with mc and cystic predominance ( cp )  . 
in evaluation of their results we realized that thinner size needles offer better results so we 1 3 radiol med ( 2016 ) 121 : 510514 22 g 25 g 23 g female male 17 , 3 16 , 8 22 , 7 16 , 9 16 , 9 needle gender architecture fig . 
after facing some problems obtaining 24 g needles from the medical market we finally decided to compare 22 , 23 and 25 g needles . in our study , 565 of 696 ( 81.1 % ) samples obtained from female patients . 
 [ 12 ] also did not find a significant difference between the two genders in their study that included 140 patients . in comparing patient age , there was no statistically significant difference for different ages . 
if nodules with a size of 1 cm were included in the study , non - diagnostic results would be higher since the area with mc would increase proportionally . as a second feature internal content was evaluated . 
this can be an important reason why the cp nodule diagnostic results were not lower . nodules smaller than 1 cm were already excluded to obtain comparable results with respect to their size . the patient population was chosen with a similar mean age , including the same number of mc and internal content for each needle thickness . 
 [ 13 ] compared 20 , 22 and 24 g needles and did not find a significant difference in their study with 270 patients . on the other hand , tangpricha et al . 
 [ 15 ] compared 21 g and 25 g needles in their study with 50 patients and declared that 21 g needles provided more cellular samples than 25 g needles in fine needle aspiration biopsy of the thyroid , but may not provide increased diagnostic accuracy . 
 [ 17 ] also found a statistically significant difference in obtaining adequate cm in comparison of 21 and 25 g needles in their study including 252 thyroid nodules . in our experience , using needles as thick as 22 g may provide more specimen , but traumatic effects will increase . 
on the other hand using thin needles is less traumatic , but of course the observer cannot obtain as much specimen . especially when using needles thinner than 25 g , the specimen containing needle can be clogged easily , causing 1 3 514 radiol med ( 2016 ) 121 : 510514 another proble with this background the 25 g needle was chosen as the thinnest choice . to take the middle course , the best ratio was obtained with 23 g needles . 
in the absence of significant changes in evoked potentials , and based on clinical neurological 1 3 464 radiol med ( 2016 ) 121 : 463471 indications , several conservative therapies are indicated ; in fact , in two - thirds of cases there is partial or complete resolution of symptoms after 11 months due to spontaneous or drug - induced regressive tendencies of the herniated portion of the disc [ 5 ]  . 
patients who do not respond to standard conservative treatments may take advantage of the o2o3 discolysis which has a good success rate of about 7080 % [ 7 , 8 ]  . 
 [ 11 , 12 ] report , in their experience of sciatica treatment , results of pain reduction in 7475 % of the cases in 618 months of follow - up . 
 thereafter , patients underwent clinical follow - up in the second , fourth and sixth months after procedures using a visual analog scale ( vas ) [ 14 ] , ranging from 0 ( no pain ) to 10 ( the worst pain one can imagine ) to 10 with cutoff 3 ; in particular a successful outcome was considered a pain value no > 3 , and unsuccessful otherwise . 
inclusion criteria comprised lumbar disc pathologies documented on mr images , pain for at least 8 weeks that does not respond to conservative therapies ( physiotherapy or oral and intramuscular drugs ) , and initial mean vas [ 14 ] > 3 . 
exclusion criteria were previous lumbosacral spine surgeries , allergies to medications administered during procedures , pregnancy and the presence of conditions mimicking a pain from sciatica as facet syndrome , sacroileitis , bone lesions . 
according to the recommendations of the combined task forces of the north american spine society , the american society of spine radiology and the asnr [ 15 , 19 ] , the type of herniated disc was classified as protrusion , extrusion and bulging . 
 [ 16 ] based on disc signal intensity mri pattern and ranging from a type i homogenous disc to a type v collapsed disc . injection technique the procedures were performed by two neuroradiologists of 35 and 5 years experience , under ct guidance ( somatom plus 4 ; siemens medical systems , erlangen , germany ) with the patient in prone position . 
the o2o3 gas mixture was achieved using an ozone generator ( ozo2 futura ; alnitec , cremosano , italy )  . after local anesthesia , performed with administration of 6 mg of mepivacaine ( about 23 ml of 2 % mepicain : monico spa , venice , italy ) , the spinal needle ( 9 or 13 cm 22 gauge ) was advanced to the intraforaminal and interlaminar space , through paravertebral or interlaminar approach , 1 3 radiol med ( 2016 ) 121 : 463471 patients received only 4 mg of betamethasone administered through paravertebral approach and near periganglionic area . 
the procedures lasted an average of about 2530 m during and after all the procedures , patients were carefully evaluated by the interventional neuroradiologists to recognize any possible complications . matching between study and control groups at the presentation , the clinical neuroradiologist matched study and control group patients , according to the criteria of same sex , age ( differing by no more than 3 years ) and disc pathology level , similar body mass index ( bmi ) ( dif5 kg / m2 ) , same type of disc herfering by no more than niation and disc degeneration . 
this last evaluation was performed to exclude potential confounding factors , resulting in 218 matched pairs ( table 1 ) , since no matching control subject could be found for 39 patients of the study group . statistical analysis the intraand interobserver reliability of the mri evaluations was estimated using agreement percentage and kappa statistics [ 17 , 18 ] with a consensus readout performed after all the data were collected . 
the success rates of the vas questionnaire were entered in a database and compared by means of the kruskalwallis test with p < 0.01 considered to indicate a statistically significant difference . 
1 axial ct a image shows a 68 - year - old woman suffering from right lumbosciatica and treated by intradiscal injection of o2 o3 through paravertebral approach at the level of l4 - l5 . 
the axial body ct image b shows a 40 - year - old woman suffering from left lumbosciatica and treated by intradiscal injection of o2o3 through interlaminar approach at the level of l5s1 respectively , with an angle 4560 and 7590 . 
complications such as allergic reactions , blood pressure fluctuations induced by medications , infections or neurological deficits never occurred . 1 3 468 radiol med ( 2016 ) 121 : 463471 fig . 
the o2o3 mixture is distributed after the injection inside the disc , epidural space and near perigangliar sites discussion in our experience , intradiscal o2o3 and intraforaminal steroid with local anesthesia injections got higher success rates compared to treatments with only steroid and local anesthetic after follow - up of 6 months in terms of pain reduction . 
about 42 and 35 % of study group patients , respectively , with discal extrusions and protrusions had successful outcomes , while there was no significant difference between the responders and non - responders to fig . 
axial ct c image shows the o2o3 mixture distributed in the disc , epidural space and near perigangliar sites 1 3 radiol med ( 2016 ) 121 : 463471 fig . 
axial ct d image shows the o2o3 mixture distributed inside the disc , epidural space and near perigangliar site oxygenozone ( o2o3 ) discolysis in the presence of bulging disc . 
in addition in case of mild and moderate degenerated ( grade i , ii and iii ) discs , the success rate was statistically significant in 176 out of 257 study group patients while there was no significant difference in treatment response in case of severe disc degeneration and dehydration ( grades iv and v )  . 
the better outcome of the study group patients than control group patients should be related to the o2o3 intradiscal actions , because o2o3 discolysis is the only difference between the two groups . 
intradiscal o2o3 mixture injection produces a dehydration and chemiodiscolysis of nucleus pulposus proteoglycans , because ozone causes an oxide reduction process called ozonolysis [ 18 ] ; in this process , ozone reacts with organic molecules containing double or triple bonds , leading to a condition of disc shrinkage and , consequently , to a reduction of compression of the nerve roots [ 6 , 23 ]  . 
moreover , 1 3 470 radiol med ( 2016 ) 121 : 463471 ozone also acts on radiculitis , an action that is achieved with injection of the mixture in the perigangliar site [ 27 ]  . 
 because o2o3 has long - acting effects , we observed that the difference in success rate between study and control groups became significant only after 6 months , probably because , on the contrary , the efficacy of steroids and anesthetic drugs administered to both groups is temporary . 
the more relevant inflammatory component present in hernias and protrusions than in the bulging disc could be the reason to explain the difference in treatment response [ 28 ]  . 
 in our experience , o2o3 discolysis performed under ct guidance is very practical and safe , since ensures the correct positioning of the needle tip in the central part of the disc , allowing an adequate control of gas diffusion in the disc and reducing the risk of complications . 
other studies [ 30 ] show the results of procedures performed under fluoroscopic guidance , but there are no data in the literature which demonstrate the superiority of the method compared to another . 
it would be also useful to perform an mri follow - up to demonstrate whether the reduction of pain can be related to morphological and structural changes in disco - somatic pathology . 
in conclusion , the addition of intradiscal injection of an o2o3 mixture with steroids in perigangliar and epidural spaces leads to rapid relief in sciatica symptoms ; more correct treatment indications and a more accurate patient selection could improve therapeutic success rate . 
furthermore , we can assume that in our experience oxygenozone discolysis obtains the best results in case of extrusions and protrusions and even in the presence of discal degenerative aspects ranging from mild to moderate grade . compliance with ethical standards conflict of interest the authors declare no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
 the sensitivity , specificity , positive predictive value ( ppv ) and negative predictive value ( npv ) of pet / ct , mri and their combined use were assessed in t and n staging . 
histopathology and follow - up imaging results were used as the gold standard . results trans - compartmental extensions , pet - mri showed 93 % sensitivity , 88 % specificity , 94 % ppv , and 88 % npv , as compared to the 94 and 53 % sensitivity , 75 and 75 % specificity , 89 and 82 % ppv , and 86 and 43 % demonstrated by mri and pet , respectively . 
in the identification of pathological lymph nodes , pet - mri showed 92 % sensitivity , 89 % specificity , 96 % ppv , and 89 % npv , whereas pet / ct displayed 72 % sensitivity , 89 % specificity , 95 % ppv and 53 % npv . 
the majority of these tumours are squamous cell carcinomas ( sccs ) [ 2 ] , and selection of the optimal therapeutic strategy requires accurate staging and localization by carefully assessing the soft tissue infiltration and pathological lymph node involvement . accurate t and n staging enables optimization of treatment planning ( radiotherapy and / or surgery as appropriate ) and , therefore , improves the outcome of patients with head and neck scc . 
currently , patients with nodal involvement but no distant metastasis ( m0 ) are treated with radiotherapy or lymphadenectomy , with or without chemotherapy . morphological assessment is carried out by either ct or mri , with the latter being the method of choice for tumours of the head and neck due to its high anatomical , spatial and contrast resolution [ 5 ] , which makes it particularly advantageous for evaluating trans - compartmental extensions with respect to ct . 1 3 radiol med ( 2016 ) 121 : 502509 table 1 patients , tumour grading ( g2 pharynx , h undifferentiated ) and localization ( n hypopharynx ) moderately , g3 nasopharynx , o poorly , oropatient grading localization however , the diagnostic accuracy of ct in tumour staging can be significantly enhanced by the integration of [ 18fluoro - deoxy - glucose fdg ] pet imaging ( 18fdgpet / ct ) [ 6 , 7 ] , and pet / ct is very sensitive in the detection and evaluation of the degree of infiltration of the primary or metastatic tumours of the head and neck region [ 8 ]  . 
nevertheless , in addition to low spatial resolution ( mainly for lesions smaller than 4 mm ) [ 10 ] , the functional method has other disadvantages , such as the possibility of incurring false negatives [ 11 ] ( given the low glucose metabolic of necrotic tissues ) and false positives [ 12 ] ( inflammatory processes )  . 
furthermore , the physiological uptake of 18fdg in the brain impedes proper assessment of skull base infiltrations by such tumours . moreover , it is often difficult to differentiate between metastatic and reactive non - metastatic lymph nodes with either pet / ct or mri imaging [ 1012 ]  . 
therefore , some authors [ 3 , 1318 ] have proposed multimodal imaging evaluation , by fusing ( pet - mri scanner or retrospective pet - mri fusion software ) or combined interpretation of pet / ct and mri images ( pet - mri ) , as a means of improving diagnostic accuracy . to extend this line of research , we set out to assess the additional diagnostic value of multi - modal imaging evaluation , achieved by combining short tau inversion recovery ( stir ) and diffusion weighted imaging ( dwi ) mri sequences with 18fdg - pet / ct ( through a specific software platform ) in t and n staging of head and neck scc with respect to each method on its own . materials and methods we retrospectively enrolled 25 patients ( age range 25 and 77 years ) with head and neck scc , who had undergone mri and pet / ct before any treatment between march 2010 and january 2013 . 
 as the study was retrospective , approval of the local ethics committee was not sought . imaging technique mri was performed using a 1.5 tesla scanner ( achieva , release 2.4.5 , philips medical systems , the netherlands ) and a head and neck coil ( synergy multichannel sense , synergy )  . 
t1 sequences with adipose tissue signal suppression were acquired after contrast medium injection ( gadovist 1 molar , administered intravenously at a dose of 0.1 ml / kg )  . 
only stir and dwi sequences were considered for the purposes of this study , in which isotropic dw images were reconstructed for b 400 s / 800 s / mm2 ; adc maps were automatically mm2 and b 800 s / mm2 and b calculated from b 0 images by the scanners software . 
mean adc maps , measured on an axial section , were generated as follows : ( a ) four independent 0 s / mm2 , b 1 3 504 radiol med ( 2016 ) 121 : 502509 table 2 mri protocol used in the study sequence t1w - tse t2w - tse t2w - stir t2w - stir t1w - spir plane tr ( ms ) te ( ms ) ti ( ms ) sense matrix thk ( mm ) gap ( mm ) epi factor axial axial 3805 axial 3474 coronal 3474 axial 256 170 256 170 276 200 276 200 256 172 124 124 axial 5411 fov ( mm ) 250 211 199 250 211 199 250 198 230 198 199 250 211 199 250 250 160 10 mm2 circular region of interest ( roi ) measurements , considering only the lowest value ( minimum adc ) ; ( b ) including pathological tissue ; and ( c ) excluding cystic / necrotic regions and calcifications [ 4 ]  . pet / ct scans were acquired on a hybrid siemens ( siemens , erlangen , germany ) system consisting of a lutetium oxyorthosilicate pet scanner ( hi - rez ) with pico - 3d electronics and a 16 - row ct device ( somatom sensation 16 )  . 
 imaging was performed 1 h after intravenous administration of 3.5 mbq / kg of 18fdg under fasting conditions , and multiplanar sections were reconstructed after attenuation and scatter correction ( 128 128 pixel size 5.3 , 2 mm slice thickness , two iterations with eight subsets )  . image analysis we created a score sheet for each patient bearing their identification code ( id ) , the dates of the pet / ct and mri exams , evaluation grids of t and n parameters , the imaging techniques being evaluated ( stir , dwi , pet / ct , pet - mri ) , and later study data and histopathology - derived tumour grades . 
images from pet / ct and mri were interpreted by a nuclear medicine specialist ( gms , 10 years of experience in pet - ct ) and a radiologist ( as , 11 years of experience ) , respectively , each blinded to the results of the other imaging modalities , each others interpretation , and histopathology findings . the t parameter was evaluated taking into account the region of origin of the tumour ( supra - hyoid or sub - hyoid ) , axial location ( right , left , bilateral , median ) , and the presence or absence of trans - compartmental extension . 
tumour invasion was assessed according to the following radiological criteria : ( a ) unilateral change in anatomy with respect to the normal contralateral side , ( b ) nodular or infiltrative abnormal tissue signals , and ( c ) appearance of mass effect or fat displacement [ 19 ]  . n staging was performed by mapping the neck lymph nodes on a grid , assigning values provided by the radiologist and nuclear medicine physician . 
lymph nodes were considered positive with all / one or more of the following : ( a ) a short axis measurement greater than 1 cm ( measurements were reported only on stir images ) ; ( b ) high signal intensity at b 200 , 400 , 800 s / mm2 and low adc values ; ( c ) evidence of coalescent lymph nodes or masses ; and ( d ) lymph nodes present in regions where usually there are no lymph nodes . 
the presence of central necrosis was considered a sign of malignancy , regardless of the size of the lymph node ( i.e. , rouviere lymph nodes ) [ 1923 ]  . 
an initial double - blind analysis of the stir , dwi and pet / ct images was performed using a semi - quantitative approach , on a scale from 0 ( absolutely negative ) to 2 ( positive )  . subsequently , a data set of co - registered multimodal images for combined reading was prepared by a medical physicist . 
co - registration of the pet / ct and mri images was performed on a multimodality workstation leonardo ( siemens medical solutions ) using the dedicated image analysis software in manual mode . the co - registered pet - mri images were then analysed by the two specialists by consensus . 
 in the remaining 15 patients ( 60 % ) who underwent radiotherapy , reference scores were given on the basis of : ( a ) remission / persistence of the signal alteration ; ( b ) uptake / no uptake of the radioactive tracer at the site of a previous neoplastic focus ; and ( c ) disappearance / persistence of lymphadenopathy and / or reduction of the volume at least of 50 % . 
such evaluations were confirmed in at least two successive diagnostic follow - ups after radiotherapy , for a total time span of roughly 15 months . statistical analysis sensitivity , specificity , positive predictive values ( ppv ) and negative predictive values ( npv ) were calculated 2 continfor each diagnostic method by means of 2 gency tables . 
unlike n staging , in t staging , the diagnostic accuracy of mri was calculated integrating stir sequences with dwi images , because of poor anatomical details definition on dwi and adc maps . 
a receiver operating characteristic ( roc ) curve was used to evaluate the diagnostic value of adc and suv in the differentiation of benign from malignant lymph nodes , and we determined the adc value threshold that provided the greatest accuracy in terms of discriminating benign from malignant lymph nodes . 
medcalc software ( medcalc software , belgium ) was used for all statistical analyses . results transcompartmental extension mri assessment of trans - compartmental extension displayed 94 % sensitivity , 75 % specificity , 89 % ppv and 86 % npv . 
this was compared with the 53 % sensitivity , 75 % specificity , 82 % ppv and 43 % npv calculated for pet - ct , whereas pet - mri displayed 93 % sensitivity , 88 % specificity , 94 % ppv and 88 % npv ( table 4 )  . 
the optimal adc threshold for differentiating between benign and malignant cervical lymph nodes , determined by roc curve analysis , was found to 3 mm2 / s , roughly in line with literature valbe 1.03 ues [ 4 ]  . 
 [ 17 ] , who compared the performance of pet - mri software fusion with pet / ct , mri and ct for the assessment of deep tissue invasion in 17 patients with advanced buccal scc . 
 concluded that , in advanced buccal scc , pet - mri is more reliable than pet / ct , mri or ct for the assessment of local invasion and for the delineation of tumour size . likewise , kanda et al . 
 [ 3 ] evaluated the clinical value of retrospective image fusion of mri and fdg - pet from pet / ct in 30 patients with oral cavity and hypopharyngeal scc , comparing the respective t and n staging performances of pet - mri , pet / ct and mri with histopathology . 
in another case , however , the extensive inflammatory reaction of a localized tumour in the oropharynx was incorrectly interpreted as positive by pet / ct , mri , and co - registered images ( table 4 )  . 
nevertheless , overall , pet - mri image assessment provided better diagnostic accuracy than either mri or pet / ct in terms of t staging ( table 4 )  . in terms of n staging , as mentioned above , mri is not always able to differentiate metastatic from reactive lymph nodes , mainly due to the size criterion . 
in our series , dwi showed to be more specific ( 67 vs 56 % ) and lesser sensitive ( 84 vs 100 % ) than stir sequence , although these differences were not statistically significant . 
therefore , dwi seemed not to have a significant impact on nodal detection compared to morphological sequences and it should be always interpreted in conjunction with a complete diagnostic mri protocol . pet / ct has proven to be highly accurate in identifying nodal metastases . 
the glucose analogue 18fdg is a marker of the metabolic activity of the tumour based since cancer cells have a higher carbohydrate metabolism than normal cells [ 24 ] , meaning that 18fdg - pet is able to detect even small metastatic foci in morphologically normal lymph nodes [ 25 ]  . 
in two of these four cases , pet - mri image assessment incorrectly interpreted the peri - tumoral lymphadenopathies as tumour infiltration , since the adipose cleavage was not easily distinguished from the tumour . ( b ) in three cases , necrotic lymph nodes were detected by mri , but not by pet / ct due to a lack of fdg uptake . 
4 mri sequences a allowed to identify the correct localization of a non - infiltrating nasopharyngeal tumour , distinguishing it from an adjacent pathological lymph node , whereas on pet / ct , b it was not possible to distinguish the tumour extension and lymph node involvement with any certainty pet / mri combined assessment of lymph nodes provided significantly higher sensitivity , specificity , ppv and npv than those of the single techniques alone . 
in our cases , the high specificity of pet / mri assessment is due to the addition of pet / ct ( exactly the same specificity , 89 % )  . 
in fact , as discussed above , there were no significant differences between dwi and stir sequence ; therefore , the added role of dwi is questionable in this setting . 
 they demonstrated that pet / mri without dwi and pet / mri with dwi detected the same number of malignant lesions ( 49 , including primary tumours , distant metastases and pathologic lymph nodes )  . 
the above findings confirm that dwi does not add significant information as part of whole - body pet / mri examination in lesion detection ; this is important given the necessity to optimize pet / mri protocols , with regard to patient comfort and efficacy . 1 3 radiol med ( 2016 ) 121 : 502509 conclusions in staging head and neck sccs , assessment of combined multimodal imaging through co - registered mri sequences and pet / ct data enabled more accurate detection of radiotracer uptake overlapping area of suspected infiltration , increasing the diagnostic value of t and n parameters . 
as integration of the two methods increased the sensitivity , specificity and diagnostic accuracy with respect to the individual methods alone , combined multimodal imaging may , therefore , be a valuable technique for the detection and staging of tumours of head and neck . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . informed consent informed consent was obtained from all participants . 
one - way between - groups pairwise analysis of variance ( anova ) and blandaltman plot analysis were used for comparing radiological and anatomical measurements . results unenhanced msct images did not identify the wound channels , whereas unenhanced mri evidenced the wound cavity in 50 % of cases . 
after the instillation of cms , both msct and mri depicted the wound channel in all the investigated stabbings , although the morphology of the cavity was irregular and did not resemble the shape of the blade . 
the radiological measurements of the wounds * chiara giraudo chiara.giraudo@meduniwien.ac.at 1 legal medicine , university of verona , piazzale ludovico antonio scuro , 10 , 37134 verona , italy 2 legal medicine and toxicology , university - hospital of padova , via falloppio 50 , 35121 padua , italy institute of radiology , university - hospital of padova , via giustiniani 3 , 35121 padua , italy 4 division of neuroradiology and musculoskeletal radiology , department of biomedical imaging and image - guided therapy , medical university of vienna , waehringer guertel 18 - 20 , 1090 vienna , austria depth , after the application of cms , exhibited a high level of agreement ( about 95 % at blandaltman plot analysis ) with the anatomical measurements at dissection . 
a similar systematic underestimation , however , has been evidenced for msct ( average 11.4 % ; 95 % ci 717 ) and mri ( average 9.6 % ; 95 % ci 613 ) data after the instillation of cms with respect to wound dissection measurements . conclusion msct and mri after the instillation of cms can be used for depicting the morphometric features of stab wounds , although depth measurements are affected by a slight systematic underestimation compared to layer - bylayer dissection . keywords forensic radiology multislice computed tomography magnetic resonance imaging stab wounds contrast medium solution introduction stab wounds are of major importance in forensic pathology as they are extremely common , especially in domestic disputes and street violence [ 13 ]  . an accurate assessment and an objective recording of the surface and internal features of the wounds are the basis for any subsequent analysis [ 4 , 5 ]  . 
whereas surface features can be easily observed , measured , and photographed by the inspection of the skin , an unbiased evaluation of the internal features , such as the depth of the stab wound , is more complicated . 
thus far , probing and wound dissection ( wd ) are the main techniques for the internal assessment of stab wounds [ 68 ]  . in the recent literature , schnider et al . 
 [ 6 ] demonstrated that multislice computed tomography ( msct ) is a useful tool for the evaluation of sharp injuries , while bolliger 1 3 radiol med ( 2016 ) 121 : 494501 et al . 
three stabbings were inflicted on the posterior surface of each calf limb with a minimum distance of 5 cm between each pair of injuries . contrast medium solution an iodinated contrast agent , omnipaque 300 ( iohexol , ge healthcare ) , was blended with sterile ultrasound gel . 
 multiplanar reconstruction ( mpr ) images were obtained . mri scans were performed using a siemens magnetom avanto 1.5 tesla ( siemens ag medical solution , erlangen , germany )  . 
the mri protocol included a sagittal proton density - weighted turbo - spin - echo fat - suppressed ( pd - fs ) sequence ( tr / te 3861 / 37 ms , flip angle 150 , slice thickness 3 mm , slice gap 20 % , read fov 300 mm , phase fov 70 % , matrix resolution 320 224 )  . 
this specific sequence was selected because of its intrinsic sensitivity to fluids and / or blood [ 11 ] and its high signal - to - noise ratio [ 12 , 13 ]  . 
before the instillation of the cms , a a small air bubble in the soft tissues ( white asterisk ) and a small skin interruption ( white circle ) where the blade penetrated into the skin were evident . 
before the instillation of the cms , c a small air bubble in the soft tissues ( white asterisk ) and a small skin interruption ( white circle ) were visible . 
comparison between msct - cmsd , mri - cms - d , and wd - d values were performed by one - way between - groups pairwise analysis of variance ( anova ) inclusive of bonferroni correction of p - values for multiple comparisons ( wd - d assumed as a reference value )  . 
subsequently , blandaltman plot analysis was performed to investigate the agreement between the radiological measurements ( msct - cms - d , mri - cms - d ) and the reference value ( wd - d )  . 
a two - sided p < 0.05 was taken to indicate statistical significance for all analyses . dissection of the wound results after radiology , the contrast medium was removed from each wound cavity by careful and abundant injection of distilled water . 
after the instillation of the contrast medium solution ( msct - cms and mri - cms ) , the morphological assessment of the wound channel was feasible for all the 21 stabbings . 
after the instillation of the cms , b the wound channel ( white arrow ) is easily recognizable and measurable overall shape of the cavity was irregular and did not resemble the morphology of the blade . 
the remaining two stabbing trials showed a massive leakage of the methylene blue solution , which permeated the tissues close to the stab wounds and hampered an accurate distinction of the single wound channels from the surrounding muscular tissue . depth of the stab wounds ( quantitative analysis ) the depth of the stab wounds and a statistical summary of the reckoned data are reported in table 1 , and herein fig . 
a proper estimation of the wd - d was not feasible for two stabbings because of the above - mentioned massive lateral leakage of the methylene blue solution into the surrounding muscular tissues . 
a quite obsolete alternative is post - mortem probing , which however may harm previously intact anatomical structures . in the last decade , several authors have explored the potentiality of post - mortem msct , a non - destructive , rapid , and repeatable procedure , for characterizing the morphometric features of stabbings [ 69 , 14 , 15 ]  . 
all radiological techniques , indeed , have the advantage of allowing a late , even after years , second review of the dataset , when decomposition , autopsy , or cremation of the body has already occurred [ 9 ]  . more recently , the use of contrast agents has been proposed in the forensic setting [ 16 , 17 ] mainly , but not only , for post - mortem angiography , post - mortem angioct , and post - mortem angiomr demonstrating , among other fig . 
thick dashed line showing the upper and lower limits of agreement at 1.96 standard deviations of the systematic difference evidences , the potentiality and ability to detect vascular injuries due to stab wounds because of the expected extravascular leakages of contrast medium [ 18 , 19 ]  . 
aiming at performing post - mortem morphometric evaluations of stab wounds , several investigations with extra - vascular local application of contrast media have also been proposed [ 69 ]  . 
these studies , all performed on animal models using msct , have demonstrated a very clear depiction of the stab directions and a quite accurate estimation of the depth of the inflicted wounds ( underestimation of about 10 % compared to layer - by - layer dissection ) [ 8 ]  . 
in our investigation , the stabbing trials were performed in post - mortem conditions using human legs surgically amputated for medical 1 3 radiol med ( 2016 ) 121 : 494501 reasons . 
the possibility to occasionally identify the wound channel without cms could be attributable to the high signal - to - noise ratio of mri and to its high sensitivity to blood in the selected pd - fs sequence [ 11 ]  . 
investigated stab wounds through msct using ioversol ( optiray 300 ) [ 7 ] , while leth et al . , in their experimental setting , used two different contrast agents , pure iodixanol ( visipaque 270 ) and iodixanol mixed with polyethylene glycol ( 50 % w / w ) [ 9 ]  . 
in our study , the ultrasound gel was chosen to provide a high signal - to - noise ratio on the selected fluid - sensitive mr images ( proton density - weighted turbo - spin - echo fat - suppressed sequence ) because of its viscosity ( i.e. , higher than water ) ; this latter property , indeed , could prevent or at least minimize the spilling or absorption in the surrounding soft tissues [ 20 ]  . 
 the iodinated contrast medium was added to guarantee a good contrast enhancement on msct images [ 20 ]  . the overall direction of the stab wound assessed by msct - cms and mri - cms was consistent with the perpendicular direction of the inflicted stabs , which was a known variable under our experimental conditions . 
did not mention this phenomenon because , as can be seen in their iconography [ 7 ] , the wound cavities were entirely included in singular muscular bundles of pork haunches [ 5 , 6 ]  . 
however , the systematic underestimation of the wounds depth , probably related to the difficulty / impossibility of the cms to reach the deepest and tiniest portion of the wound channel , must be taken into consideration . interestingly , in two stab wounds ( in close proximity to each other , 5 cm distance ) the layer - by - layer dissection ( wd ) did not permit the measurement of the depth of the wounds because of a generalized leakage of the methylene blue staining in the surrounding muscular tissue , which hampered the differentiation of the two wound cavities . 
a possible explanation for this finding could be the greater viscosity of the cms with regard to the methylene blue solution ( i.e. , an aqueous solution ) , which could have reduced the leakage along the muscular bundles . 
we believe that in a different scenario ( i.e. , post - mortem analysis of vital injuries in which an active bleeding into the wound cavity occurred ) unenhanced mri [ 21 ] could exhibit better results in terms of wound channel depiction and measurement . 
the proposed radiological methods have been tested only on stab wounds produced on calves , and , consequently , can be applied , at most , to the evaluation of injuries located at the extremities . in the experimental trials , the knife was always inserted and extracted orthogonally to the skin surface , whereas in real forensic casework the blade can have different directions . 
to overcome this limit , further trials with different angulation of the blade will be necessary . conclusion in the present study , a protocol for the radiological assessment of the internal features of stab wounds by msct and mri using a single cms suitable for both techniques has been developed and tested in a post - mortem setting . 
after the instillation of cms , both msct and mri depicted the wound channel in all the investigated stabbings , although the morphology of the cavity was irregular and did not resemble the shape of the blade . 
however , a similar systematic underestimation has been evidenced for msct ( 11.4 % ; 95 % ci 717 ) and mri ( 9.6 % ; 95 % ci 613 ) data with respect to wd measurements . further studies are required to develop new contrast media capable of reaching the deepest part of the wound cavity and , thus , increasing the accuracy of the radiological measurements , which are currently affected by a slight systematic underestimation compared to layer - by - layer dissection . 
moreover , real forensic casework with injuries located in different anatomical areas , more stabbing directions , and produced by diverse weapons will have to be analyzed before msct and mri can be routinely applied for the forensic morphological and metrical analysis of stab wounds . funding the authors state that this work has not received any funding . compliance with ethical standards conflict of interest all the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
although , till now , gadolinium brain deposits have not been associated to any kind of neurological signs or symptoms , they oblige the radiology community to modify the actual approach in using gadolinium contrast media in daily practice , to reduce unknown possible risks for patients . keywords gadolinium contrast agents magnetic resonance human brain accumulation safety trace elements chronic contrast adverse reaction those of us involved in the early development of clinical application of magnetic resonance imaging ( mri ) , in the late 1980s , remember very well the excitation and the surprise , after the injection of a small amount of mri contrast medium , in creating a superb differentiation between perfused and not perfused lesions . 
gadolinium ion was , at that time and is still nowadays , the responsible of this enhancement , due to its seven unpaired peripheral electrons , that create a quick exchange of water molecules , at over one million time per second [ 1 ]  . * bruno beomonte zobel b.zobel@unicampus.it 1 department of medicine , unit of diagnostic imaging , universit campus bio - medico di roma , via alvro del portillo 21 , 00128 rome , italy gadolinium is toxic for humans : its ionic radius is close to that of calcium , so it works as a potent blocker of many types of voltage - gated calcium channels and as an inhibitor of calcium - activated enzymes , at nanomolar and micromolar concentration [ 2 ]  . 
to reduce its toxicity , to less than one - fiftieth , and to assure its complete renal excretion in 2448 h , the biological half life for the elimination of gadolinium contrast media is around 70120 min [ 5 ] , gadolinium ion needs to be chelated in the contrast molecule , so the first gadolinium - based contrast agent ( gbca ) , commercialized in 1987 , was gadoliniumdtpa ( diethylene triamine pentaacetic acid ) , gadopentetate dimeglumine , where the dtpa is a well - known chelator . the pharmaceutical industry , later , produced several other types of chelates that structurally are either linear or macrocyclic , so that we have now basically four different classes of compounds : ionic macrocyclic , non - ionic macrocyclic , ionic linear and non - ionic linear chelates [ 6 ]  . gbca do not diffuse through plasma membranes and are therefore considered unable to cross the intact blood brain barrier ( bbb ) [ 7 ] , so they are very efficient contrast media for detecting any kind of bbb disruption , in central nervous system lesions , and for improving mri detection and characterization of lesions in different organs . 
 moreover , they were considered safety enough to be used in more than 300 million administrations [ 8 ] , with a very low frequency of acute adverse events [ 9 , 10 ]  . 
however , in 2006 two different studies [ 11 , 12 ] suggested a relationship between gbca and a new and not well - known disease , characterized by high morbidity and mortality : the nephrogenic systemic fibrosis ( nsf )  . 
subsequent reports clearly showed that in patients with reduced renal function 1 3 radiol med ( 2016 ) 121 : 478481 ( glomerular filtration rate less than 30 ml / m / 1.73 m2 ) , the incomplete excretion and the prolonged presence in the body of the gbca , led to a dissociation of gadolinium ion from its chelating molecule and the induction of a group of reactions that resulted in the clinical manifestations of nsf [ 13 , 14 ]  . 
from a chemical point of view , we have two different kind of stability : the thermodynamic stability , which is the thermodynamic equilibrium , in a solution , between the dissociated gadolinium ion , the ligand and the whole contrast molecule , and the kinetic stability , which is the speed at which the dissociation equilibrium is reached : if it is high , the speed is low and vice versa . 
 in other words , the risk of dechelation of the gadolinium ion is much higher with linear rather than with macrocyclic chelates , and with non - ionic rather than with ionic chelates . 
 a study published in 2008 , reported gradual release of free gadolinium ion , in human serum , at 37 c and ph 7.4 , the same values of human blood , in the following order : nonionic linear gbca > ionic linear gbca > macrocyclic gbca , over a period of 15 days of incubation [ 15 ]  . thus , many international and national scientific societies , together with important health authorities , like the food and drug administration ( fda ) and the european medicines agency ( ema ) , established specific safety policy for the use of gbca . 
they divided gbca into three groups : high , intermediate and low risk to develop nsf and suggested to avoid the use of gbca , at high and intermediate risk of nsf , in patients with glomerular filtration rate less than 60 ml / m / 1.73 m2 [ 16 ]  . 
a significant decrease of the number of nsf cases was observed after these guidelines were released and no new case was reported after 2009 , excluding rare isolated exceptions [ 17 ]  . recently , other events modified again the relationship between the risks and the benefits of using gbca in radiology practice . 
in 2014 , a new report , by kanda et al . , suggested that the observed hyperintensity , on t1 weighted images , of the globus pallidus and of the dentate nucleus , in the brain of lung cancer patients , with normal renal function , was related to the repeated administrations of gbca [ 18 ]  . 
this first observation was confirmed by other clinical studies , during the same year [ 19 ] and in 2015 [ 2023 ] , in other groups of patients , with different diseases , all of them undergone to repeated administrations of low stability gbca . 
the unenhanced t1 hyperintensity increases with the number of administrations of low stability gbca , in patients without any kind of renal disease , probably because of the crossing of gadolinium through the normal bbb and its long - term deposit in some cerebral and cerebellar nuclei . these experimental results radically modified two previous acquired concepts in the radiology community : ( 1 ) the complete elimination of gadolinium from the body , after its injection in the form of gbca , in about 2448 h , in subjects with normal renal function ; ( 2 ) the inability of gadolinium to cross an intact bbb . 
the first concept has already been challenged by some investigational studies [ 2426 ] , where the presence of gadolinium was demonstrated in bone tissue , in the form of gadolinium phosphate ( gdpo4 ) and other insoluble compounds , after the administration of less stable gbca . 
mcdonald and his group evaluated 13 autopsy specimens , from patients with a glomerular filtration rate of 49 ml / m / 1.73 m2 or more , who received at least four administrations of gadodiamide ( non - ionic linear chelate ) and found gadolinium inside the nervous tissue , not only in the globus pallidus and in the dentate nucleus but also in the pons and in the thalamus , although at a lower concentration . 
the group of mcdonald found a direct relationship between the amount of retained gadolinium in the brain and the number of less stable gbca previous injections ; most of the gadolinium deposits were observed in the endothelial layers of brain vessels and a variable part of them ( 1842 % ) were located in the extra - cellular interstitium , as an effect of the crossing an intact bbb . 
 in this publication , gadolinium was found not only in the brain gray matter nuclei but also in the frontal lobe cortex , in the frontal lobe white matter and in the cerebellar white matter . in a subsequent animal study , published by robert et al . 
 in march 2015 [ 29 ] , it was reinforced the idea that only with repeated administrations of a non - ionic linear gbca , but not of a ionic macrocyclic agent , you can record an accumulation of gadolinium in the bra this study also showed that there is no evidence of a reduction of t1 hyperintensity , after a wash out period of 5 weeks from the last injection , not only in deep nuclei but also in other brain structures . although the analytical methods used to measure the presence of gadolinium in the brain are not able to distinguish between free and chelated gadolinium , all these 1 3 480 radiol med ( 2016 ) 121 : 478481 experimental data , give more strength to the hypothesis of in vivo dechelation of gadolinium ion , from less stable gbca , its crossing the intact bbb and its progressive concentration in the brain , in all patients , regardless the presence of a renal dysfunction , with a clear doseeffect relationship . there are still many aspects that need to be better understood on this matter but , among all , it is mandatory to know what are the other biological factors that increase or decrease the gadolinium chelates dissociation . 
probably , considering the close correlations between nsf and brain nuclei hyperintensity on t1 weighted images , a part of them are already been studied . + , zn2 + or cu2 in fact , we know numerous studies concerning the in vivo transmetallation between gadolinium ion and body cations , such as fe2 + , ca2 + , in the contrast molecules , although some of them were conducted in rats [ 3032 ]  . 
furthermore , it is well known the high affinity of gadolinium ion with phosphates , to form gadolinium phosphate ( gdpo4 ) , that provokes its accumulation in bone tissue of normal renal function patients [ 2426 ] , or a higher speed of dechelation , in patients with nsf [ 14 ] , after the administration of less stable gbca . 
 [ 33 ] in the skin of a nsf patient , with the highest levels present in the walls of subcutaneous blood vessels and the lowest levels in the subcutaneous connective tissue . it is also important to try to identify the molecules that bound gadolinium in the bra in fact , using mr imaging , we are able to identify a clear hyperintensity , on t1 weighted images of some deep nuclei but not of other brain structures ( pons , thalamus , cerebral and cerebellar white matter etc . ) , although lower concentration of gadolinium deposits are present in these structures too . 
these limitations of mri are produced by an expected low sensitivity , at lower gadolinium concentration , but it could be also explained by the presence of insoluble gadolinium salts , such as phosphate , bicarbonate , and hydroxide , that have little or no influence on the relaxation times of protons [ 34 ]  . 
 [ 29 ] , clearly demonstrated that mri is not able to assess all the gadolinium deposits that are present in human tissues , following repeated administration of less stable gbca . on 27 july 2015 , the food and drug administration ( fda ) made a safety announcement reporting that the risk of brain deposits , following repeated use of some type of gbca , is under investigation and asked the research community to refer any adverse event related to the use of gadolinium contrast media . till now , no clinical signs of neurological toxicity , due to gadolinium deposits in the brain , have been reported in patients , but we do not know the end of the story , at the moment . 
while the fda investigations will probably produce specific guidelines , it is important that the radiology community considers the new available experimental evidences , about the brain gadolinium deposits , after repeated injections of low stability gbca , and does its best to reduce any possible risk for the patients . 
practical recommendation is to maintain the dosage of gbca to a minimum and try to avoid the use during pregnancy and in small children , although we do not have any published research dealing with these two groups of individuals but only a case report [ 35 ]  . 
we agree with kanal and tweedle [ 36 ] , who underline the ethical conflict we are going to experience as radiologists , between the need to give patients crucial and life - saving information , obtained from contrast - enhanced mri , and the deontological appraisal of the new available scientific evidences , regarding gbca safety . 
in the meantime , as a temporary solution to these issues , we propose to rigorously follow the ema suggestion ( 1 july 2010 ) [ 37 ] , establishing a personal contrast medium card , that patients , particularly outpatients , should carry on , where each facility can report the date , type and amount of gbca used . 
patients with a prior angio - ct scan were included in the study and they were then retrospectively divided into two groups : patients with suitable anatomy that were treated within guidelines of the manufacturers ( wifu : 94 patients , four treated in emergency ) and those with unsuitable anatomy that were treated outside of said guidelines ( oifu : 70 patients , 16 treated in emergency )  . 
all the patients of the wifu group were treated with a stentgraft with under - renal sealing while in the oifu group always an over - renal stent - graft was used . 
since the introduction of evar in clinical practice in 1991 [ 1 ] , given the enormous clinical applications , both the technology of implanted devices ( stent - graft ) and the competence and experience of the operators , interventional radiologists and vascular surgeons , has encountered a great development : in fact , studies show that up to 6070 % of aortic 1 3 radiol med ( 2016 ) 121 : 528535 aneurysms can be treated with stent - graft currently available on the market [ 2 , 3 ]  . 
the ability to offer a less invasive treatment than open surgery in patients with large aaa , with multiple comorbidities and contraindications to surgery has determined , on a global scale , a net change of trend in the management of aaa , evar has established itself as a first - instance both in elective cases than emergency / urgency situations [ 4 ]  . evar has established itself as a first - line treatment in patients with suitable anatomy , in accordance with the manufacturers recommendations , on the contrary , in patients with unfavorable anatomy endovascular treatment is still a subject of great debate [ 3 ]  . 
all measurements were made in accordance with the standards published in the literature [ 12 ]  . patients without preliminary angio - ct studies and without follow - up examinations were excluded from the study . according to the adopted exclusion criteria , 15 patients were excluded from the study due to the presence of perianastomotic pseudoaneurysm while the remaining 76 were excluded due to the absence of viewable preoperative tests for a proper categorization into one of the two treatment groups . the follow - up that we usually carry out at our institution provides cta at 1 month , ceus at 6 months , cta at 12 months and then alternately ceus and cta every 12 months in the absence of complications , vice versa if a type ii endoleaks is found the follow - up interval becomes 6 months . we reviewed all cta follow - up of patients included in the study , to assess the incidence of complications such as endoleaks ( focusing on type ia endoleak , expression of inadequate proximal sealing of the endoprosthesis or cranial progression of disease ) , migration , complete or partial thrombosis or infection of the prosthesis . 
the group oifu therefore consists of 90 patients with complete follow - up which are the subject of the study ; of these , 16 ( 17.7 % ) were treated in emergency . 
the value of statistical significance was placed for p < 0.05. the postoperative mortality was 6.3 % ( 6 / 94 patients initially included in the study ) in the wifu group while was 7.8 % ( 9 / 115 patients initially included in the study ) in the oifu group . 
in 12 patients ( 13.3 % ) an aorto - monoiliac stent - graft with a contralateral plug and subsequent femoralfemoral bypass was positioned ( seven patients treated with a cook stent - graft and five patients with a medtronic device )  . 
in choosing the size of the endoprosthesis to be implanted , it has been employed an oversizing of 1520 % . the selection of patients and the interventions were carried out by a multidisciplinary team of interventional radiologists and vascular surgeons with experience of 15 years in the endovascular treatment of aaa [ 1318 ]  . in both groups , in only one case ( 1.4 % wifu vs 1.1 % oifu ) a placement of a proximal cuff was required during the procedure due to the detection of a significant type ia endoleak . in 17 patients ( 18.8 % ) of the oifu group angioplasty on the proximal neck after placement of endoprosthesis fig . 
preliminary angiography demonstrates the presence of aneurysm of the abdominal aorta with proximal neck suitable for endovascular treatment , with a proximal neck > 3 cm ( a )  . 
preliminary angio - ct shows the presence of aneurysm of the abdominal aorta with hostile neck : it is possible to observe the neck length of 9 mm and angle of 95 ( a )  . 
mpr ( b ) and 3d ( c ) with emphasis on the angle of the neck between the longitudinal axis of the vessel and the longitudinal axis of the aneurysm : this feature , together with the presence of neck extremely short ( < 10 mm ) makes the evar treatment complex . 
particularly in emergency / urgency conditions , evar in cases oifu , is essential to save the patients life 1 3 532 radiol med ( 2016 ) 121 : 528535 fig . 
preliminary angiography documents the presence of a big aaa with extremely short neck ( a ) , successfully treated by placement of an aorto - mono - iliac stentgraft ( b )  . 
the first four patients oifu with a type ia endoleak were treated by the addiction of a proximal cuff ; among these , two patients , at 1 month follow - up , showed persistence of type i endoleak , and therefore were subjected to surgical conversion with explant of the endoprosthesis . due to such complications , to prevent the persistence of type i endoleak in patients with very short neck , in the following four cases of type i endoleak , we experienced the placement of an aorto - monoiliac device within the previous bifurcated endograft , obtaining good results . 
we tested this technique , not reported in the literature , in cases of extremely short neck ( < 10 mm ) in consequence of the failure of the positioning of a proximal cuff in the 50 % of cases so treated . 
the rationale is to achieve greater stability on the proximal neck in the event of a short and angled neck and , in our view , this can be achieved best by placing an aorto - monoiliac stent - graft that a cuff . 
in two cases in the wifu group , type ii endoleak was associated with an increased size of the native sac and was treated with trans - lumbar injection of bovine thrombin and metal coils inside of the sac . in each group a case of an infected endoprosthesis was found and treated with explantation of the stent - graft . in each group a case of endoprosthesis thrombosis was reported : in the oifu group there was complete thrombosis of the main body of the endoprosthesis with the development of side vessels that revascularized the iliac arteries . 
despite the technological evolution of the available materials , the development of increasingly compliant endoprosthesis and greater experience of the operators , the proximal neck is still the main determinant of the feasibility of evar [ 4 ] : in particular , the main limiting factors are represented by the length and the angle of the proximal neck [ 7 , 8 ]  . 
the problem of a short neck has been addressed by manufacturers through the development of innovative devices , a branched [ 20 ] or fenestrated [ 21 ] configuration and the introduction of chimney / snorkel technique [ 22 ] to help ensure the patency of the renal arteries and possibly also of the visceral vessels . such devices and endovascular techniques have had little spread as of today due to a greater technical difficulty required for positioning and therefore the problem of the proximal neck continues to be a decisive factor in the feasibility of endovascular treatment . subject of great debate in the literature is the efficacy of endovascular treatment with conventional devices in patients with hostile neck ; the aim of our study was to report our experience in this field , by comparing patients treated according to the instructions of the manufacturers ( wifu ) and off label ( oifu )  . in our experience we have found a high technical success in oifu group ( 95.3 % ) : according to what reported by lee et al . 
 [ 10 ] , we believe that the reason for this success is to be attributed to the use , in all cases , of supra - renal endoprosthesis , which ensure a good proximal sealing in such patients with short neck . 
in particular in our study the oifu group presented a very short neck ( 34.4 % of patients with neck length < 10 mm ) and in this condition a supra - renal fixation is mandatory . in cases of intraoperative identification of type ia endoleak , we believe angioplasty on the proximal neck a safe and effective procedure to achieve the resolution of the complication , ensuring a complete sealing of the endoprosthesis to the proximal neck . 
this maneuver can be associated with complications such as fissures or aortic dissections , and therefore is to be performed with extreme caution , inflating the balloon for a few seconds and always within the endoprosthesis : in our experience we have not observed complications , but we got the resolution of endoleak in almost all patients treated , reserving for a single case the positioning of proximal cuff . the presence of short neck is burdened with a higher risk of significant intraprocedural complications , such as occlusion of the renal arteries . 
in our study we have indeed observed a statistically significant difference in intraoperative occlusion of the renal arteries , with five cases that have occurred in the oifu group and have been associated , in two cases , to the death of the patients ( who had nevertheless ruptured aaa ) and in three cases dialysis ; only one case occurred in the wifu group for cranial migration of the prosthesis . it is important to consider , however , as we found no statistically significant difference in postoperative mortality ( six deaths in the wifu group and nine in the oifu group ) , despite the greater number of ruptured aneurysms in the oifu group : even in cases anatomically unfavorable , evar ensures a high clinical success especially in emergency / urgency . the further complication associated with the presence of hostile neck is represented by type ia endoleak being an urgent matter and requiring immediate treatment . 1 3 534 radiol med ( 2016 ) 121 : 528535 in our experience , characterized by results in the medium / long term , we found type ia endoleak in 2.8 % of wifu patients and in 8.8 % of oifu patients , with statistically significant difference . 
for this reason , in this selected group of patients with extreme short neck complicated with type ia endoleak , we adopted the strategy to deploy an aorto - monoiliac device inside and above the bifurcated stent - graft instead of the simple addition of a proximal cuff . 
we obtained good results without any persistence of endoleak or surgical conversion and we therefore believe that in such patients with endoleak , the aorto - uniliac stent - graft strategy could be successfully . 
 [ 26 ] reported a higher incidence of intra and postoperative [ 25 ] and long term [ 26 ] complications , deducing that the application of evar outside the parameters of the specific anatomical ifu has a greater negative effect on the long teralthough treatment outside of the ifu presents good results ( 1.8 % of postoperative mortality ) ; evar in these circumstances should be undertaken with caution and not in all patients who may be candidates for traditional surgery [ 26 ]  . however , it is to be considered that recent studies with large series provided encouraging results in the feasibility of evar outside of the common guidelines of the manufacturers [ 10 , 2729 ]  . in particular , lee et al . 
 [ 10 ] , in a study comparing the treatment of 143 wifu and 75 oifu patients , found a rate of migration of the prosthesis , reoperations , regression of the aneurysm sac , endoleaks and aneurysm - related mortality similar between the two groups , concluding that the evar can be performed safely in high - risk patients with unfavorable anatomy through the use of devices available on the market . nowadays the treatment of complicated aneurysms is a difficult problem , which is dealt with on a daily basis in clinical practice , in particular in urgency / emergency condition , as recently shown in one of our previous experience [ 14 ]  . our study has limitations that should be considered when interpreting the results and are represented by the retrospective nature and lack of randomization , which , however , are difficult to obtain in the management of this disease and this is demonstrated by the absence of prospective randomized studies in the literature on the treatment of aaa necked hostile . 
the use of energy 6mv is preferable and its strongly recommended not to * francesca salerno fra - salerno@libero.it 1 department of radiation oncology , policlinico umberto i sapienza , university of rome , viale regina elena 326 , 00161 rome , italy 2 department of radiation oncology , azienda ospedaliera san giovanni addolorata - roma , via santo stefano rotondo 5 / a , 00184 rome , italy 3 department of cardiology , azienda ospedaliera san giovanni addolorata - roma , via dellamba aradam 9 , 00184 rome , italy exceed a total dose of 2 gy to the pm and 1 gy for icd . 
for this reason , a close collaboration between cardiologist , radiotherapist and physicist is necessary . keywords guidelines implantable cardioverter defibrillator ionizing radiation pacemaker pacingdependent risk class introduction in the last decade , the annual rate of radiation therapy courses in patients with pacemakers ( pm ) or implantable cardiac defibrillators ( icd ) quite increased . the proper functioning of pm and icd can be affected by radiation treatment due to the direct or diffuse effects of ionizing radiation and / or electromagnetic interferences produced by linear accelerators on cardiac devices . after radiation therapy , device failure occurs in about 2.5 % of patients with pm and 6.8 % of patients with icd [ 1 ]  . there is still a significant lack of knowledge regarding the safe management of cancer patients with implantable cardiac devices facing radiation treatment . for these recommendations , we refer to the german society of radiation oncology and cardiology degro / dgk ( deutschen gesellschaft fr radioonkologie / deutschen gesellschaft fr kardiologie ) guidelines [ 2 ] ; to the society of cardiology australia and new zealand statement drawn in 2015 [ 3 ] ; to the guidelines in force in the netherlands compiled by hurkmans , et al . 
in 2012 [ 4 ] and , finally , to the italian association of radiation oncology ( airo ) 1 3 516 radiol med ( 2016 ) 121 : 515520 recommendations as reported in the 2013 guidelines for the treatment of breast cancer [ 5 ] in patients with cardiac implantable electronic devices ( cied )  . the clinical conditions of cardiac patients and their state of dependency on the device must be assessed and monitored in close cooperation with the cardiologist in charge before , during and after radiotherapy . 
they generally include a thin generator of electrical impulses , usually implanted subcutaneously in the left infraclavicular region above the pectoral muscles , and flexible insulated leads , placed within the heart , which carry these impulses from the generator to the heart muscle and are also able to sense the hearts intrinsic electrical activity , carrying signals back to the pacemaker generator . 
the modern pacemakers also have sophisticated programmable software and facilities for recording events [ 6 ]  . icd , more sophisticated devices , are pacemakers that have also the ability to deliver a high voltage shock in case of a life - threatening ventricular tachycardia or ventricular fibrillation . 
icd have revolutionised the treatment of patients at risk of sudden cardiac death due to ventricular tachyarrhythmia [ 6 ]  . modern cied contain complementary metal oxide semiconductor ( cmos ) technology . 
with this technology , silicon is combined with various diffused impurities and deposited metals to create circuits at a low cost , but with wide - ranging functionality [ 7 ] and smaller devices characterized by less energy consumption and higher reliability . 
 in comparison with bipolar transistors that were used in older models , these modern cmos are more sensitive to damaging events caused by ionizing radiation [ 2 ]  . in vitro [ 812 ] and in vivo [ 1317 ] clinical studies have shown that ionizing radiation and electromagnetic fields can cause permanent and / or latent damages to cied due to ionization of semiconductors present in the circuits of these devices , to changes in voltage and to creation of aberrant electrical pathways induced by irradiation itself [ 7 ]  . 
greater magnitude malfunctions , with higher risk for patients , such as prolonged inhibition or complete interruption of device functioning [ 3 , 1820 ]  . malfunctions can lead to different clinical consequences for patients , ranging from symptomatic bradycardia , hypotensive crisis , cardiogenic shock and angina pectoris , to more critical and extreme conditions as asystole , ventricular fibrillation , stroke and death [ 2 , 21 , 22 ]  . predictive factors of devices failure in the case of direct irradiation or with the use of energy higher than 6 mv [ 1 , 2 ] , the devices can suffer significant damages . 
note that the excess rate of secondary neutrons generated into the head of the linear accelerator by the use of energy equal to or higher than 10 gy , can damage the ram ( random access memory ) and the additional semiconductors of modern devices [ 11 , 23 ]  . how high is the risk for the patient ? the estimated radiation dose to the cardiac device depends on the location of the tumor as well as on the radiation fields , as suggested by hurkmans , et al . 
in patients with upper abdominal or pharynx targets , for example , the pm / icd estimated dose should be between 2 and 10 gy . functional abnormalities can be deleterious for patients dependent on the device . 
the condition of dependency is defined as the absence of a cardiac intrinsic rhythm of 30 beats per minute for which the abrupt cessation of cardiac pacing due to the abnormal operation of the implanted device , creates a situation of extreme emergency [ 24 , 25 ]  . 
 when the target volume is located in zone ( c ) , the dose to the device is probably less than 2 gy ; in zone b is between 2 and 10 gy ; while in the zone a is higher than 10 gy . 
for example , in patients with upper abdominal or pharynx targets , the device valued dose should be between 2 and 10 gy independent pacing patients as well as dependent pacing patients could have different risk related to relative adsorbed dose of the device , as figuring in table 2 . recommendations for irradiation of patients with pm or icd [ 25 ] before radiation treatment 1 . 
for low - risk patients , follow the general protocol for the irradiation as explained previously ( visual observation of the patient during radiation therapy , consulting specialist cardiologist and a technician )  . 
for intermediate - risk patients , the safety protocol includes a weekly specialist check of the device and appropriate equipment during each session of radiation therapy ( such as ecg monitor and defibrillator )  . 
in addition , include an electrocardiogram monitoring during each session of radiation therapy and have a specialist control the device within 24 h after the end of each session . during radiation treatment after radiation treatment general measures 1 . 
analysis of any anomaly of the device taking into account that even clinically insignificant changes in parameter settings can precede major defects . 1 3 radiol med ( 2016 ) 121 : 515520 fig . 
train patients to recognize the symptoms of an altered device function ( irregular or low heart frequency , dizziness , syncope ) and alarm sounds emitted by the device . the management of patients with cied and indicated rt is reported in fig . 
2. conclusion because a risk failure after radiotherapy ranging from 2.5 % for pm to 6.8 % for icd as reported before , more attention for patients with similar devices is required . 
for 1 3 520 radiol med ( 2016 ) 121 : 515520 high energy photons ( > 10 mv ) , malfunctions are likely due to neutrons that interact with some elements present in the devices . 
in lowand intermediate - risk patients with an icd and in intermediate - risk patients with a pm , a weekly device check during the full period of radiation therapy is recommended . 
equipment for cardiopulmonary resuscitation should be available during the treatment period . compliance with ethical standards ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . conflict of interest the authors declare that they have no conflict of interest . radiol med ( 2016 ) 121 : 521527 doi 10.1007 / s11547 - 016 - 0621 - x ultrasonography the utility of the highresolution ultrasound technique in the evaluation of autologous adipose tissue lipofilling , used for the correction of postsurgical , posttraumatic and postburn scars maria scotto di santolo1 marco sagnelli1 giovanni tortora2 maria angela santoro3 pier luigi canta3 guido molea3 fabrizio schonauer3 massimo imbriaco1 received : 29 september 2015 / accepted : 13 january 2016 / published online : 4 february 2016 italian society of medical radiology 2016 abstract purpose lipofilling technique is significantly increasing and the need of a non - invasive method to assess the success of the procedure is becoming mandatory . 
in particular , us can be considered an alternative method to mri for evaluation of tissue lipofilling due to the simplicity and easy access of the technique and can be also used for monitoring the efficacy of the surgical procedure . 
to evaluate the effectiveness of such treatment serial ultrasound examinations were performed at both the region affected from skin dimorphism through the adjacent skin region , using a high frequency transducer . 
furthermore , it was assessed the presence of complications ranging from oedema or hematoma to necrosis or adipocyte migration of the gra finally , was calculated the average percentage of one - year survival of autologous fat transplant . results quantitative evaluations obtained with time series of ultrasound showed that the greatest benefits of autologous adipose tissue lipofilling , are found at the level of the hypodermis , but that also all the other layers of the skin can benefit from this procedure . conclusion the data acquired demonstrate that the eco color doppler with high resolution can be considered a valid non - invasive tool for the assessment of morphological and quantitative degree of engraftment of autologous adipose tissue transplanted . 
lipofilling is an accurate and effective choice for the correction of congenital or acquired skin disorders for its filler effect and consequent benefit for all tissue layers . keywords skin ultrasound color - doppler highresolution ultrasound skin lesions lipofilling 1 department of advanced biomedical sciences , university of naples federico ii , via pansini 5 , naples , italy 2 uoc department radiology , aos dei colli monaldicotugno - cto , via l . 
in recent years , diagnostic imaging procedures have 1 3 522 radiol med ( 2016 ) 121 : 521527 table 1 site of injection in patient population patient site of injection fig . 
white arrowhead : epidermis , black arrowhead : dermis , black arrow : muscle fascia , white arrow : subcutaneous adipose tissue right arm right forearm left arm glabella frontal region left eyebrow glabella frontal region breastbone left leg lower lip left ankle glabella right cheekbone frontal region right cheekbone left lower lip frontal region left palm hand right cheekbone left eyebrow right neck region left neck region frontal region right peri - auricular region fig . 
2 ultrasound examination obtained in the transverse view at the level of the skin region affected by dismorphism and at the adjacent region with thickness measurement of the epidermis and dermis undergone a profound transformation in parallel with the rapid evolution of technology and computer science [ 1 ]  . 
 the development of the ultrasound technique in the dermatological field is tied to the availability of high frequency transducers ( > 15 mhz ) , the introduction of techniques that reduce the artifacts and optimize the power of resolution and the possibility of studying the vascularization of expansive lesions of the skin and the formation of new vessels with color - doppler technique [ 19 ]  . 
alexander and miller in 1979 used for the first time ultrasound to study the skin , generating a one - dimensional scanning of the skin with rudimentary equipment and with insufficient spatial resolution [ 2 ]  . 
in the study of superficial organs , and in particular in the dermatological field , the depth of the region to be investigated is 12 cm and pathology frequently regards lesions with less then 1 mm thickness , it is therefore necessary to use high frequency probes , with high resolution and reduced scan depth [ 1 ]  . 
therefore , the use of these probes , allowing high - resolution imaging , is of paramount importance ; nevertheless , currently used 5to 17 - mhz linear arrays probes also allow the visualization of deep layers up to 3.5 cm ( depth ) , with an axial resolution of 0.090 mm , thus permitting to complete the study of superficial tissues [ 1 ]  . 
the highresolution ecd has also been used for the study of diffuse skin diseases like psoriasis , scleroderma , erythema nodosum , sarcoidosis and lymphedema as well as for the evaluation of local complications due to the application of topical medications and of implantable materials for esthetic use [ 111 ]  . 
the aim of this study was to demonstrate , the utility of the high - resolution ecd technique in the evaluation of autologous adipose tissue lipofilling , used for the correction of post - surgical , post - traumatic and post - burn scars . materials and methods the study was performed retrospectively on the material and data available in our department and has therefore been performed in accordance with the ethical standards laid down in the declaration of helsinki in 1964 and its subsequent amendments . 
3 ad serial ultrasound examinations in the transverse views , performed both at the level of the skin region affected by dismorphism and at the adjacent region , ( time 0 , 1 week , 1 month and 1 year after the surgical procedure ) their consent for the use of such material for cumulative and statistical studies . 
twenty - five patients ( 21 females ) , aged between 14 and 62 years , underwent surgical correction of scars with lipofilling technique [ 1016 ] ( table 1 )  . 
exclusion criteria were : pregnancy or breast - feeding , general contraindication to surgical or anhestetical procedures and patients with psychological problems . deriving from the greek lipos fat and english to fill infiltrate , the term lipofilling means the grafting of autologous adipose tissue , a surgical technique that can correct the volumetric defects of the soft tissues caused by trauma , resection of cancer , congenital defects and aging [ 1016 ]  . in our study a lipofilling or lipostructure by coleman [ 1014 ] was performed in all patients . 
figure 4 shows ultrasound examination at the level of skin region affected by dismorphism and at the adjacent region , with measurement of autologous fat implant . the vascular signal has been evaluated at the same site of the injection using the colorand power - doppler parameters that have been set for the study at low speed blood flow ( color - doppler : prf 500 hz , wall filter 27 hz , gain 75 % , persistent media ; power doppler : prf 350 hz , wall filter 45 hz , gain 85 % , low optimization ) [ 1 ]  . 
possible complications , 1 3 524 radiol med ( 2016 ) 121 : 521527 table 2 us - detected serially evaluated hypodermal thickness thickness of hypodermis ( cm ) patient time 0 1 week 1 month 6 months 1 year regions , more pronounced within the first month , allowing sometime to distinguish the superficial and deep dermal layers . 
5. given the possibility to have quantitative data at ultrasound examination representing the various skin and subcutaneous layers in serial evaluations after surgery ( table 2 ) , it was possible to calculate the average percentage of one - year survival of autologous implanted fat . 
4 ultrasound examination obtained in the transverse view at the level of skin region affected by dismorphism and at the adjacent region , showing measurement of the autologous fat implant ranging from edema or hematoma to necrosis or adipocyte graft migration , were evaluated . 
this formula , the so - called fat graft survival ( fgs ) ( % ) , expresses the ratio between the hypodermal thickness ( in cm ) detected at high - resolution ecd 1 year from lipofilling and the hypodermal thickness ( in cm ) detected at us 1 week from lipofilling 100 . ecd criteria to assess the efficacy and the survival of the autologous implanted fat , included the following : ( 1 )  . 
 ( 3 ) assessment by means of ecd of changing in vascularity in the peri or intra - implantation area , as expression of complications such as inflammatory phenomenon or granulomas . results the high - resolution ultrasonography of the skin performed before the surgical procedure , showed mild echogenic disorganization , with evidence of a slight thickening reduction of all dermal regions , in addition , there was poor differentiation between the superficial and deep layers of the dermis , with associated extensive hypo echogenicity . 
conversely , immediately after the surgical procedure and in the successive controls , it was observed the presence of an area of hyper echogenicity corresponding to the implanted adipose tissue , with regular margins , that became progressively smaller in the following controls at 1 and 6 months , due to natural phenomena of reabsorption , disappearing completely at 1 year . 
5 an example of patients scar tissue in the frontal view of the sternal region , in a 42 - yearold woman , before ( a ) and after lipofilling correction ( b ) table 3 average percentage of lipoaspirate fat graft survival ( % ) patient fat graft survival rate ( % ) survival of autologous implanted fat in our study was identified at approximately 72 % . 
no significant complications were detected . the beneficial and regenerative effects of adipose implanted tissue were detected not only at physical examination of the patients , but also at quantitative high - resolution ecd analysis , which showed an increase both in the thickness not only of the subcutaneous adipose tissue , but also of the dermis and epidermis ( tables 4 , 5 )  . using colorand power - doppler , a slight increase in the vascular signal in the region of the implant of adipose homologous tissue and in the surrounding skin region was found . 
no complications such as oil cyst were observed , after the lipofilling correction . discussion fat and english to deriving from the greek lipos fill infiltrate , the term lipofilling means the grafting of autologous adipose tissue , a surgical technique that can correct the volumetric defects of the soft tissues caused by trauma , resection of cancer , congenital defects and aging [ 1016 ]  . lipofilling represents an ideal filler due both to its filling and regenerative effect , being the adipose tissue an unlimited source of stable , biocompatible and inexpensive material [ 1013 ]  . 
many experimental clinical and radiological studies have demonstrated the survival of adipocytes in the receiving site [ 1013 ] ; both in humans and animals , histological evidence of surviving transplanted fat grafts has been collected [ 3 , 1217 ]  . 
human studies have been performed both for experimental purposes and in the context of follow - up of patients undergoing autologous fat transplant procedures [ 16 ] through the histological analysis of tissue biopsies . 
among the radiological techniques mean value useful for verifying the level of engraftment of autologous transplanted adipose tissue , particular interest has risen in the ultrasound techniques and magnetic resonance imaging ( mri ) [ 12 , 13 , 15 , 16 ]  . 
the ultrasound exam makes it possible to study with a non - invasive , fast and low - cost technique the subcutaneous tissue , to achieve a preoperative planning and to confirm the effectiveness of the surgical technique used , documenting the increase in volume [ 12 , 13 , 15 , 16 ]  . in recent years , with the widespread of the lipofilling techniques , mri has been considered the reference imaging method for evaluation of adipose tissue . 
this technique has proven to be a very reliable technique for the follow - up of these patients , especially as a preoperative study in cases with complex multi - tissue involvement and in the evaluation of complications . 
conversely , due to its lower cost and its wider availability , the ultrasound examination has mainly shown the possibility of a qualitative visual assessment of the affected area treated with this surgical procedure ; nevertheless , in our study we have drawn up the possibility of a quantitative assessment using standardized measurements of certain dermal areas and of the transplant itself at established times , thus obtaining a numerical value ( % ) expressing the survival rate of adipose implanted tissue . 
ultrasound performed with high resolution and multifrequency transducers ( 517 mhz ) is cost effective and allows widespread examination , answering the fundamental question that surgeons arise when performing this type of surgery , that is how much adipose tissue has taken root . 
 a potential limitation of the study is the limited number of patients recruited and the slight difference in terms of thickness between dermis and epidermis , that might be a potential source of error . conclusions lipofilling represents a slightly invasive , but effective technique for the correction of congenital or acquired defects of the skin , due to its filler effect and consequent tissue growth benefit despite the majority of patients seem to have lost a percentage of the injected fat over time [ 1013 ]  . 
what radiologists need to know about this syndrome consists in the heterogeneity of appearances : emphysema is mainly paraseptal and fibrotic pattern could be variable , including the variant of airspace enlargement with fibrosis which needs to be differentiated from honeycombing . 
thus , the role of radiologists in the management of these patients is crucial as it involves diagnosis , detection of complications and could possible concerns the identification of patients at higher risk . keywords combined pulmonary fibrosis and emphysema emphysema idiopathic pulmonary fibrosis high - resolution computed tomography emphysema and idiopathic interstitial fibrosis ( ipf ) are two entities defined by distinct clinical and functional features ; emphysema is characterized by a poorly reversible * federica ciccarese ciccarese.f@gmail.com 1 radiology unit , cardio - thoracic - vascular department , s.orsola malpighi university hospital , via massarenti 9 , 40100 bologna , italy and progressive airflow limitation , whereas in ipf a restrictive pattern is associated with impaired diffusion capacity . 
 moreover , they show different radiological and histopathological appearances as far as they involve different pulmonary regions ( upper lobes versus lower lobes ) [ 1 ]  . however , the conventional clinical dichotomy between emphysema and fibrosis should not be further considered as pathologic changes of coexisting patterns can be commonly observed in smokers , ranging between 5 and 10 % of interstitial lung diseases [ 2 ]  . the combination of both pathologies was first described in the 70s [ 3 ] and , with the advent of ct imaging , subsequently mentioned in case reports or short series in the 90s [ 4 , 5 ]  . 
since then , there is an increasing interest in this new entity and several trails have been published . patients with both pulmonary fibrosis and emphysema have different pulmonary function tests and outcomes than patient with pure emphysema or pure fibrosis . 
indeed , these patients show relatively preserved spirometric values ( due to the opposite effect of emphysema and fibrosis ) and decreased diffusing capacity of the lung for carbon monoxide ( dlco )  . 
essentially , cpfe syndrome should be considered in three settings : normal or near normal spirometry and lung volumes , but a severely diminished dlco ; in particular , when dlco is < 40 % predicted , which is also a criteria to suspect pulmonary hypertension ( ph ) [ 7 ] , up to 16 % of patients show cpfe . 1 3 radiol med ( 2016 ) 121 : 564572 fig . 
1 hrct appearance of combined pulmonary fibrosis and emphysema ( cpfe ) : upper lobe emphysema ( mixed type centrilobular and paraseptalblack arrow ) and lower - lobe fibrosis ( usual interstitial pneumonia pattern , characterized by thickening of interlobular septa , honeycombing and traction bronchiectasiswhite arrow ) patients with severe breathlessness and / or oxygen requirement out - of - proportion compared to spirometric abnormalities . patients with ph and abnormal lung function , especially with a mixed obstructive / restrictive pattern [ 8 ]  . in such complex clinical scenery , the role of radiology becomes crucial as it could assess the coexistence of both pathological processes fig . 
moreover , differences in radiological findings have not been taken into account in most of studies . herein , we review the main clinical and radiological features of patients with cpfe , focusing on the heterogeneity of hrct appearances . epidemiology and risk factors the exact prevalence of cpfe syndrome is still not known . 
2 typical cpfe features include the frequent association between paraseptal emphysema ( a black arrow ) and uip pattern ( b white arrow ) however , these criteria lack specific quantitative methods to assess the degree of emphysema and fibrosis ; reyerson et al . 
proposed to consider only patients with an emphysema extension 10 % ( because of clinical relevance in identifying gold stage ii equivalent disease ) , reporting 8 % of cpfe patients in idiopathic pulmonary fibrosis ( ipf ) [ 9 ]  . 
on the other hand , chae has recently documented cpfe in 3 % of asymptomatic smokers , with a mean emphysema extension of 8.2 % , thus below the cut - off proposed by reyerson [ 10 ]  . 
hence , the criteria proposed by reyerson may result in an underestimation of the syndrome , especially in asymptomatic subjects , who also require a diagnosis and a follow - up . 
in the same way , the definition of significant fibrosis proposed by cottin has never been defined . the reason for the coexistence of pulmonary fibrosis and emphysema remain unclear . most patients with cpfe share the same features , which are history of smoking and male sex . 
cigarette smoking is considered the principle risk factor , as 98 % of subjects 1 3 566 radiol med ( 2016 ) 121 : 564572 are either current or former smokers . 
the association could be explained by the role of smoking in the pathogenesis of both diseases , even if other factors could be involved : it is still not clear why some patients develop emphysema or fibrosis , while others a mixed pattern . 
similarly , though both emphysema and fibrosis are more frequently in men , the association between male sex and these pathologies could not explain by itself the disproportionate male predominance noted in cpfe ( 9 : 1 male : female ratio ) [ 2 , 10 , 11 ]  . however , other associations are reported in cpfe as dust exposure ( asbestosis , silicosis , and talcosis ) and hypersensitivity pneumonitis . 
recently found an interest association between paraseptal emphysema and uip pattern ; they demonstrated that patients with paraseptal emphysema most commonly show a higher extent of fibrosis with uip pattern ; on the other hand , a predominance of centrilobular emphysema may be associated with a higher extent of emphysema and an nsip - hrct pattern [ 15 ] and fig . 
2. main criteria for differential diagnosis between fibrotic patterns are reported in table 1 and [ 1619 ]  . among them , aef was recently identified as a smokingrelated change in the lung , occurring in 617 % of smokers submitted to lobectomy [ 20 ] ; this pattern is supposed to be another distinct feature of cpfe [ 12 , 21 ] and consists in thick - walled large cysts of the lower zones of the lung , where reticulation is present ; it is always associated with emphysema and is supposed to represent the development of pulmonary fibrosis in the setting of emphysematous lung , with enlargement of the cysts due to retraction forces fig . 
as they involve the same lung regions ( lower zones ) , the differential diagnosis between aef and uip is crucial as aef did not show significant progression ; the main criteria for differentiating them consist in dimension ( > 2.5 cm in aef versus 0.31.0 cm in uip ) and wall thickness ( 0.9 mm in aef versus 2.1 mm in uip ) ; the presence of a wall thickness is also crucial for the differential diagnosis with emphysema [ 22 ] and fig . 
 described three different patterns of distribution in cpfe : diffuse emphysema ( centrilobular and / or bullous ) with zone of transition between bullae and honeycombing ; paraseptal emphysema with predominant subpleural bullae of enlarging size at the bases ; separate processes , with independent areas of fibrosis and emphysema [ 23 ]  . the imaging findings above reveal that cpfe may have different phenotypes and should no longer be considered as a unique entity . 
further studies are needed to address if the variability in appearances may reflect differences in clinical presentation and outcome . natural history and prognosis longitudinal changes in forced vital capacity ( fvc ) and dlco have been usually considered as prognostic factors in ipf , but they should not be considered as endpoints in cpfe ; indeed , because of the coexistence of fibrosis and emphysema , patients with cpfe experienced a slower decline in fvc and a progressive increase of airflow limitation ( represented by forced expiratory volume fev1 / fvc ) [ 24 ]  . 
found that longitudinal changes in fev1 was most predictive of mortality in cpfe [ 25 ] ; however , also the annual decrease of dlco corrected for alveolar volume should be considered [ 24 ]  . a part from the decline in lung function , patients with cpfe show a poor prognosis for the possible coexistence of other comorbidities , mainly represented by : ph this is the most common complication , occurring in up to 50 % of patients with cpfe [ 6 ] , usually more severe than in patients with only ipf . 
once develops , it represents one of the most important prognostic factor ( in association with decline in fvc and other parameters above mentioned ) , with 1 - year survival of only 60 % [ 26 , 27 ]  . 
to confirm the diagnosis of ph , right heart catheterization is required ; however , radiological manifestations of ph are well known : thus , radiologists should pay particular attention to vascular and cardiac signs which may reflect an underlying ph ( such as dilatation of main pulmonary arteries and right heart enlargement ) [ 28 ] and fig . 
5. lung cancer several authors reported a high prevalence of lung cancer in cpfe patients , which appeared to be more frequent than in ipf and copd [ 2931 ]  . 
thus , lung nodules should be considered with extreme suspect in these patients and strictly followed over the time acute lung injury patients with cpfe show a potential vulnerability to additional lung insults , such as chemotherapy or thoracic surgery , with increased risk of acute lung injury [ 8 ]  . 
3 airspace enlargement with fibrosis ( aef ) pattern in cpfe : it consists in the association of emphysema ( a usually mixed type , i.e. , centrilobular , arrow head , and paraseptal , white arrow ) and large cystic spaces at the lung basesb black arrow 1 3 568 radiol med ( 2016 ) 121 : 564572 fig . 
4 tips and tricks in differential diagnosis between honeycombing and other patterns ; honeycombing is characterized by small cystic spaces with wall thickness ( a ) , arrow ; airspaces enlargement with fibrosis consists in large cystic spaces ( > 2.5 cm ) with a thinner wall ( b arrow ) , in lung regions where reticulation is present ; bronchiectasis in non specific interstitial pneumonia ( nsip ) could also resemble honeycombing ( c black arrow ) : in these cases , multiplanar reconstruction ( mpr ) with minim intensity projection ( minip ) help in the visualization of the connection between bronchiectasis and bronchial tree ( d , e ) to excessive fibroproliferation , with fibrosis and bronchiectasis , clearly detrimental in cpfe patients [ 32 ] and fig . 
demonstrated a worse survival than in patients with emphysema [ 33 ] , while it is still not clear whether cpfe has a worse or a better prognosis compared to pulmonary fibrosis . 
mejia reported a worse survival than in patients with ipf as well as cottin had previously done [ 6 , 26 ] , while others have found comparable or better survival [ 9 , 29 , 34 , 35 ]  . the reasons for these conflicting results may be several , but primary due to different criteria of enrolment . 
has recently considered the influence of smoking history , finding that current smokers showed a radiological progression in 72.7 % of cases , while former smokers did not progress in 95.0 % [ 10 ]  . 
thus , also smoking status should be taken into account as a prognostic factor . interestingly , no - one has never investigated the influence of different fibrotic patterns on prognosis ; as already mentioned , uip is most commonly detected , but other smoking - related lung diseases have been reported including nsip , rb - ild , dip , aef , srif . 
in the preliminary results of a recent research , which considered 21 cpfe patients during a short follow - up , uip pattern showed a progression in 60.0 % of cases versus 18.2 % of interstitial aef or nsip ( p 0.05 ) , while emphysema showed a nonsignificant progression during the same period [ 37 ]  . 
we would expect that uip pattern is associated with a worsen prognosis , as in pure fibrotic changes of the lung parenchyma , but further studies are needed to better clarify this point . thus , the heterogeneity of appearances may reflect a different natural history . 
this could be the key to better target the management of patients as no treatment has been established yet and it is still questioned whether patients with cpfe should be included in trials of therapy for idiopathic pulmonary fibrosis [ 14 , 39 ]  . 1 3 570 radiol med ( 2016 ) 121 : 564572 fig . 
6 patients with cpfe ( aef variant ) , showing two common complications of this syndrome : acute lung injury , characterized by diffuse ground glass ( a , b , c , black arrow ) , small peripheral lung cancer at the right bases ( c white arrow ) and nodal mediastinal metastasis ( b asterisk ) conclusion radiologists play an important role in the detection of cpfe syndrome . 
indeed , traditional spirometric tests have a limited role in the recognition of this syndrome , while hrct scan could easily identify the coexistence of emphysema and fibrosis as well as possible complications ( such as pulmonary hypertension , lung cancer and acute lung injury )  . however , a consensus definition has not been reached and actual criteria do not define the degree of emphysema and fibrosis for the diagnosis of cpfe . 
in patients with wilson disease , defective atp7b function due to mutation of the gene atp7b results in impaired biliary excretion of copper and reduction of incorporation of copper into ceruloplasmin , thus leading to excessive copper accumulation in many tissues , including the liver and the brain [ 1 , 2 ]  . the main clinical manifestations of wilson disease are hepatic or neurological abnormalities . 
the severity of liver involvement greatly varies , depending on the stage of the disease at the time of diagnosis and whether or not the patient receives specific treatment [ 13 ]  . 
 another issue that remains unanswered is to what extent liver involvement in wilson disease may display suggestive or specific features that would allow discriminating between liver involvement by wilson disease and liver involvement by chronic hepatitis . the goal of this study was twofold . 
first , we wished to describe the mri presentation of liver involvement in adult patients with wilson disease and determine the most indicative appearance of this condition using a retrospective casecontrol study . 
second , we wanted to determine if liver involvement in wilson disease displays suggestive or specific features on mri that differ from the more common diffuse chronic liver diseases . materials and methods patients we considered 23 consecutive patients with wilson disease who had mri of the liver at 1.5 - t in our department between january 2011 and february 2015 inclusively . 
the diagnosis of wilson disease was based on clinical examination , biological tests ( low serum ceruloplasmin level and increased 24 - h urinary cooper excretion ) , genetic tests and presence of kayser fleischer rings . 
seventeen patients were receiving specific treatment ( trientine hydrochloride , n 6 ; zinc acetate , 5 ; d - penicillamine , n 2 ) at the time of mri examination . 4 ; oral zinc sulfate , n the clinical files of these 23 patients ( referred as to the wilson group ) were retrieved by the study coordinator to determine the status of liver involvement . 
the severity of liver involvement was determined by histopathological analysis of liver specimen after percutaneous liver biopsy in 5 / 23 patients ( 22 % ) using the metavir score [ 13 , 14 ] or the results of liver stiffness measurement in 18 / 23 patients ( 78 % )  . 
liver stiffness measurement was performed by transient elastography using the fibroscan m probe ( echosens , paris , france ) by an experienced hepatologist the same day than mri [ 1720 ]  . 
similar to patients of the wilson group , 11 / 23 patients ( 48 % ) had liver cirrhosis and 12 / 23 patients ( 52 % ) had liver fibrosis . 
in this group , the severity of the liver disease was determined on the results of liver biopsy and transient elastography , using the same criteria than in the wilson group . 
not applicable , tse turbo spin echo , trufi true fast imaging with steady - state free precession , 3d vibe three - dimensional volumetric interpolated breath - hold gradient - echo , grappa generalized autocalibrating partially parallel acquisition this retrospective study was conducted following the recommendations of our institutional review board and informed consent was obtained from all patients . mr imaging all patients underwent mri examination of the abdomen using a 1.5 - t system ( magnetom avanto , siemens healthcare , erlangen , germany , running software syngo mr b17 )  . 
high - resolution free - breathing fat - suppressed t2 - weighted turbo spin - echo ( tse ) sequence with respiratory triggering using prospective acquisition correction ( pace ) , fat - suppressed true fast imaging with steady - state free precession ( trufi ) sequence in the coronal plane , unenhanced inand out - of - phase fatsuppressed tse sequence , and fat - suppressed three - dimensional volumetric interpolated breath - hold gradient - echo ( 3d vibe ) sequences after intravenous ( iv ) administration of a gadolinium chelate ( gadoterate meglumine or gadoteric acid , dotarem , laboratoires guerbet , roissy - charles de gaulle , france ) were obtained in all patients . 
the pace technique interleaves the imaging sequence with a navigator sequence so that image acquisition is synchronized with the patient breathing cycle and images are acquired during the end - expiration phase . 
 consequently , the repetition time ( tr ) varied depending on the respiratory cycle length but was approximately of 22002000 ms , resulting in an acquisition time of approximately 2 min 30 s . 
in - phase and out - of - phase breath - hold fat - suppressed t1 - weighted sequences were acquired with a dual echo technique , allowing perfect registration between corresponding images [ 22 ] during suspended respiration at end expiration . breath - hold fat - suppressed t1 - weighted 3d vibe sequences were performed in the transverse plane before and at four times after iv of 0.1 - mmol of gadoterate meglumine ( dotarem , guerbet , roissy - charles de gaulle , france ) per kg of body weight followed by a 20 - ml saline flush , at injection rate of 2 - ml / s , using a power injector ( optistar ; mallinckrodt , cincinnati , oh , usa )  . 
 1 3 radiol med ( 2016 ) 121 : 546556 table 2 classification of criteria used for image analysis on mr imaging in 23 patients with wilson disease and 23 patients with chronic viral hepatitis who served as a control group quantitative criteria ( continuous data ) categoric criteria ( binary data ) hepatic height ( cm ) portal vein diameter ( mm ) splenic index ( cm3 ) caudate to right - lobe - ratio liver contours hepatic dysmorphy global hepatic atrophy honeycomb pattern signal intensity of liver parenchyma on t1 - weighted images signal intensity of liver parenchyma on t2 - weighted images spontaneous portosystemic shunts hepatic steatosis cholelithiasis portal thrombosis ascites signal intensity of liver parenchyma was evaluated relative to that of the spleen the second acquisition ( portal dominant phase ) was performed 70 s after the administration of contrast material . 
 the third acquisition was obtained 120 s after contrast material administration and the final acquisition ( equilibrium phase ) was performed 5 min after the start of iv administration of contrast material . 
all acquisitions were performed during suspended respiration at end expiration . mr image analysis for this retrospective casecontrol study , two independent radiologists reviewed the mri examinations in a random manner on a picture archiving and communication system ( pacs ) viewing station ( directview , 11.3 sp1 version , carestream health inc , rochester , ny , usa ) using a standardized for to minimize review bias , they were blinded to any patient information . 
the diameter of the portal vein was measured in the transverse plane by the two radiologists as its largest diameter one centimeter distal to the confluence of the splenic and superior mesenteric vein [ 24 ]  . 
the si was used to estimate the splenic volume and was calculated as the product of the height , width , and thickness of the spleen , each expressed in centimeters [ 25 ]  . 
height was determined on coronal images as the greatest height of the spleen ; width was the greatest splenic diameter on any transverse image ; thickness was the distance between the inner and outer borders of the spleen , as measured at the level of the splenic hilum [ 25 ]  . 
cl / rl was calculated with electronic calipers using the right portal vein as a landmark to separate the caudate and the right lobe following the description of awaya et al . 
hepatic dysmorphy was considered present when global or localized hepatic atrophy was present , when hypertrophy of the left lateral section ( segments 2 and 3 ) , hypertrophy of segment 1 or gallbladder fossa widening was visible , or when marked confluent fibrosis was identified [ 2729 ]  . the honeycomb sign was considered present when multiple hypointense nodules surrounded by thin hyperintense septa resulting in a reticulate pattern were present on t2 - weighted mr images [ 5 , 12 ]  . the signal of the liver parenchyma was categorized as hyperintense , isointense or hypointense relative to the signal of the spleen on t1 - and t2 - weighted mr images . steatosis was considered present when a marked drop in signal intensity was found between in - phase and opposed phase t1 - weighted mr images [ 3032 ]  . 
to identify variables associated with the diagnosis of wilson disease at mri , we compared patients with wilson disease and those with chronic diffuse liver disease of the control group . 
sensitivity , specificity and accuracy were calculated with their corresponding 95 % confidence radiol med ( 2016 ) 121 : 546556 intervals ( cis ) for each qualitative mr variable . 
sensitivity of a given qualitative mr variable was defined as the number of wilson disease patients in whom this sign was present divided by the total number of wilson disease patients . 
the results of descriptive analysis for quantitative data are given in table 3 . no significant differences were found between the two groups for hepatic height , portal vein diameter , si and cl / rl value . 
this finding that consists in multiple low - intensity nodules surrounded by hyperintense septa on t2 - weighted images has been considered as a unique imaging pattern [ 5 , 7 , 12 ]  . 
however , as observed in our study , this finding is not specific and may be also present in patients with chronic viral hepatitis . the honeycomb pattern has been reported by ko et al . 
in their report , the abnormalities were located in segments 1 and 4 of the liver and were considered as possibly due to copper accumulation on the basis of histopathological analysis . 
however , experimental studies in rats showed that excessive copper accumulation does not alter the signal intensity of the liver on t1and t2 - weighted mr images [ 34 , 35 ]  . 
all percentages were rounded to the nearest first digit cohort study of patients with wilson disease , liver biopsies revealed variable degrees of hepatic involvement ; 37 % of patients had cirrhosis , 36 % had an unspecified stage of fibrosis and 54 % had steatosis [ 36 ]  . we observed contour abnormalities of the liver in only 10 / 23 patients ( 36 % ) with wilson disease . 
however , it has been reported that mri underestimates the presence of liver contour irregularities by comparison with ultrasound [ 6 ]  . in our study , the presence of hepatic steatosis was subjectively evaluated using signal drop of liver parenchyma on inand out - of - phase t1 - weighted mr images . 
t2 - weighted ( tr / fat - suppressed 2310 / 27 ms ) mr image in the transverse plane shows multiple hypointense liver nodules ( arrowheads ) surrounded by hyperintense septa displaying the honeycomb pattern . 
a in - phase t1 - weighted fast spin - echo ( tr / te 119 / 4.75 ms ) mr image shows hyperintense hepatic parenchyma ( arrowheads ) relative to the spleen ( arrow )  . 
b out - of - phase t1 - weighted fast spin - echo ( tr / te 119 / 2.35 ms ) mr image shows marked drop of signal intensity of hepatic parenchyma ( arrowheads ) by comparison with in - phase mr image in a to further steatohepatitis [ 36 ]  . 
on liver biopsy specimens , 54 % of patients with wilson disease have steatosis , in association with either cirrhosis or fibrosis [ 36 ]  . in our study , caudate lobe enlargement as evidenced by a cl / rl value > 0.90 was found in only 7 / 23 patients ( 30 % ) with wilson disease . 
these authors observed that the hypertrophied caudate lobe extends further to the right side , which corresponds to the bifurcation of the right portal vethey found that a modified cl / rl with use of the right portal vein to set the lateral boundary was more accurate for the diagnosis of 1 3 554 radiol med ( 2016 ) 121 : 546556 hepatic cirrhosis [ 26 ]  . 
 our results indicate that a majority of patients with wilson disease has a normal cl / rl value , similar to patients with chronic viral hepatitis . in our study , splenic volume was assessed using the splenic index . 
we did not use a specific threshold splenic index for determining splenomegaly because such a definite and uniformly accepted threshold value does not exist in the literature [ 38 ]  . we observed that in patients with wilson disease the mean portal vein diameter was not different from that in patients with chronic viral hepatitis . 
have reported that in a series of 148 patients without liver disease , the mean portal vein diameter was 11 mm 2 mm ( range 515 mm ) [ 24 ]  . 
third , a large proportion of patients with wilson disease had only transient elastography for the classification of the severity of liver involvement , thus potentially introducing bias in the reference standard . 
odds ratio and 95 %cis are not shown for some variable because a zero value for corresponding data in table 3 led to unstable estimates of these parameters enlarged caudate lobe results from binary transformation of cl / rl value when cl / rl was > 0.9 si signal intensity * all effects are present vs . 
absent frequency of corresponding variable ; data are percentages ; raw numbers are in parentheses exact conditional logistic regression 1 3 radiol med ( 2016 ) 121 : 546556 the metavir score based on histopathological analysis of liver specimens [ 17 , 19 , 41 ]  . 
moreover , histopathological analysis of liver specimens is subjected to variability to reach the correct diagnosis because of heterogeneous distribution of liver lesions in chronic liver diseases [ 42 , 43 ]  . 
 fourth , our population of wilson disease patients was heterogeneous in terms of treatment received by the patients at the time of mri examinations and this might have influence the general results of our study in terms of imaging presentation [ 3 ]  . in conclusion , our analysis demonstrates that mri shows a constellation of findings in association with liver involvement in wilson disease although most of them are nonspecific because they can be also observed in chronic viral hepatitis . 
it is assumed that familiarity with this finding may clarify the cause of diffuse hepatic parenchymal abnormalities in the detection of unknown wilson disease . compliance with ethical standards funding this study did not receive any specific funding . conflict of interest all authors declare that they have no conflict of interest to disclose . ethical approval all procedures were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or similar ethical standards . 
 such patients also underwent an mri examination under basal conditions , and with four dynamic phases , as well as a hepatobiliary phase acquired after at least 20 min and recognized by the excretion of contrast agent into the bile duct , following intravenous administration of 0.05 mol / kg of gadoxetic acid ( gadoxetate disodium , primovist ; bayer , osaka , japan )  . 
in another case , there was an overdiagnosis of a hcc with a typical nodular pattern ( false positive ( fp ) ) , but which most likely should have been attributed to a previous echinococcus cyst . 
mri analysis , in combination with the study of the hepatobiliary phase , also showed a greater sensitivity , the same specificity , and a greater diagnostic accuracy compared to mri evaluated only in the dynamic phases ( with an average percentage between the two operators , respectively , of 75.7 , 90 , and 78 % )  . conclusions mri with gadoxetic acid shows a diagnostic accuracy superior to contrast - enhanced mri , allowing for the diagnosis of additional lesions , and it could be considered as an imaging method to carry out a more appropriate management of waiting lists for liver transplants . 3 liver unit , university hospital tor vergata , rome , italy 4 pathological anatomy unit , university hospital tor vergata , keywords hcc diagnosis hcc therapy mri contrast agent liver transplant histopathological correlation 1 3 radiol med ( 2016 ) 121 : 588596 introduction table 1 previous interventions liver transplantation represents the best available treatment for hepatocellular carcinoma ( hcc ) , as it offers the chance to eradicate also the underlying disease , i.e. , cirrhosis [ 1 ] ; however , in a regime of low availability of organs , a proper selection of patients judged to be candidates for this complex operation is crucial . to date , magnetic resonance imaging ( mri ) with nontissue - specific contrast media has been reported to be an excellent imaging technique for preoperative staging and tumor size measurement [ 24 ]  . 
subsequently , the two radiologists performed a review of the mri examinations , in order to evaluate the diagnostic accuracy of the dynamic and hepatobiliary phases . 1 3 radiol med ( 2016 ) 121 : 588596 patients patients 37 ( 1 fp ) 3 ( 1 fn ) table 3 characteristics of nodules histology ( n ) gadoxetic acid mri ( n ) total no . 
of identified in particular , it was compared the number of lesions ( tp and tn ) identified only by dynamic mri positive phases ( typical pattern ) , mri with dynamic and hepatobiliary positive phases ( typical pattern ) , and the mri dynamic negative phases , but positive only with the aid of hepatobiliary phase ( atypical patterns , i.e. , cases in which the use of the hepatospecific contrast agent is essential for the diagnosis )  . lastly , a restaging of patients was performed , in agreement with the data obtained through hepatospecific contrast - enhanced mri , and was calculated by the number of patients as follows : subjects who met the milan criteria with standard dynamic mri but not with the mri using gadoxetic acid . 
of nodule ( s ) / patient 1 nodule 2 nodules 3 nodules 4 nodules 5 nodules 6 nodules nodule characteristics hcc complete necrosis dysplastic nodules grading hcc ( edmondsonsteiner ) histopathological analysis of explanted livers the organ was removed , weighed , and subsequently dissected into 1 - cm explants to be closely examined ; the hepatic artery , portal vein , bile duct , and gallbladder were cut longitudinally . for each tumor lesion , the following features were described : the seat , or the anatomical segment ; the dimensions ; the cellular grading based on nuclear characteristics according to the classification of edmondsonsteiner ; the presence of microscopic vascular invasion ; and the possible presence of satellite nodules , i.e. , located within 2 cm of the primary lesion . results a total of 46 nodules were identified on the basis of a histopathological examination ( average 2.7 nodules for each patient ; range 16 nodules / patient )  . 
some of these hccs showed areas of partial necrosis , and most of them were moderately or poorly differentiated ( grade iiiii of the edmondsonsteiner scale )  . the histological data are summarized in table 3 . histologically , the nodules showed an average size of 17.2 mm ( range 556 mm )  . 
in this case , the time interval between the analysis and the explant was particularly high ( 88 days )  . in another case , a nodule was diagnosed as a hepatocellular carcinoma with a typical nodular pattern , although likely it should have been referable to a previous inflammatoryinfectious event ( echinococcus cyst ) , as reported in the medical history of the patient . mri assessment , together with the hepatobiliary - phase analysis , also showed greater sensitivity , the same specificity , and greater diagnostic accuracy ( 94.6 , 90 , and 93.6 % ) 1 3 592 radiol med ( 2016 ) 121 : 588596 fig . 
1 hepatospecific ce - mri ( gadoxetic acid ) and t1 spoiled gradient - echo fat - sat show hcc nodule ( 28 31 mm ) with typical pattern located in the vi liver segment . 
2 hepatospecific ce - mri ( gadoxetic acid ) and t1 spoiled gradient - echo fat - sat depict two nodules : one hcc with atypical pattern and another one with typical pattern both in the vii liver segment . 
these 3 patients were found to be outside the transplantation criteria currently in use , and the diagnosis was confirmed histologically . the comparison between the staging performed through hepatobiliary mri with hepatospecific contrast medium , and that deduced from the histological analysis , showed a high correlation , except for two patients who were not included in the milan criteria with standard mri . 
of these , one result was a false positive , and the other had been excluded from the milan criteria due to an overestimation of the size , although it fit the up - to - seven criteria . discussion given the low availability of organs and the related allocation inadequacy , a proper selection of patients eligible for liver transplantation is crucial , especially in light of the ethical controversies that emerged with the current scoring system , which seems to favor patients with hcc compared to those with other diseases [ 7 , 8 ] , leading to the so - called meld - exception ( model for end - stage liver disease )  . mri and ct with dynamic use of extracellular contrast agents are currently considered the preferable choice for noninvasive diagnosis and staging of hepatocellular carcinomas greater than 1 cm , and with a typical pattern ( intense contrast enhancement in the blood phase and the presence of washout in the portal phase and / or late phase ) [ 9 ]  . a correct diagnosis has gained more importance following the recent expansion of the criteria for inclusion in the transplant list : the milan criteria are often replaced by the up - to - seven criteria proposed by mazzaferro et al . 
hepatospecific ce - mri ( gadoxetic acid ) and t1 spoiled gradient - echo fat - sat in the arterial phase show a nodule ( 17 mm ) in the vii liver segment with intense enhancement ( a ) and a washout with pseudocapsule evidence during the late phase ( b )  . 
histological findings : infectiousinflammatory sequelae [ 10 ] , as these ensure a patient survival rate of 71.2 % at 5 years from transplantation , which is indeed similar to that of patients who fit the conventional criteria . the introduction of the mri studies with hepatospecific contrast media has increased the diagnostic performance of this method , especially in the identification and characterization of lesions with atypical patterns , i.e. , those which do not show one or more of the typical characters described above ( lesions that do not show a significant washout in the portal and / or late stages or lesions characterized by washout with small or no obvious enhancement in the arterial phase )  . the analysis of the hepatobiliary phase in which we can appreciate the excretion of the contrast agent formerly taken up by liver cells , in the bile ducts , adds valuable information about the degree of cellular anaplasia : liver cells which have lost cell differentiation will likely have a different behavior than the surrounding liver parenchyma and appear hypointense . our study showed a high sensitivity ( 94.6 % ) of hepatospecific mri contrast agents and a specificity of 90 % , equal to the specificity of non - hepatospecific mri contrast agents . 
however , the hepatobiliary - phase imaging appearance of hcc was not included in the new optn / unos ( organ procurement and transplantation network / united network for organ sharing ) policy for liver transplant allocation because the consensus meeting took place shortly after food and drug administration approval of the agent for clinical use in the united states [ 13 ]  . we think that it could be interest to evaluate the added value of the hepatobiliary phase also for novice reader in order to quantify the real contribution to the final diagnosis in clinical practice . the high incidence of hepatocellular carcinomas ( 100 % ) in our sample of patients , who were already considered candidates for transplantation on the basis of a ct - total - body examination , could also have influenced the assessments made by the two operators , with a tendency toward overestimation of tumor lesions . 
thus , it cannot be excluded that the patients considered in these studies had additional injuries , undiagnosed with standard imaging analysis , with an underestimation of lesions actually present and a consequent overestimation of diagnostic accuracy . the peculiarity of our study lies in the population itself of the patients selected , as we considered only transplant candidates with a histological assessment of the actual number of tumor lesions present or not in the organ 1 3 594 radiol med ( 2016 ) 121 : 588596 considered as a whole ; this brought us to a more accurate and reliable evaluation of diagnostic performance . 
the diagnostic accuracy as evaluated through the analysis of mri with hepatospecific contrast medium is also more than just a dynamic study , with the diagnosis of eight further hepatocellular carcinomas , corresponding to an additional 28.6 % of diagnosed lesions . in our experience , the mean time on waiting list was 149 days , and the interval for imaging before orthotopic liver transplantation ( olt ) was 47 days . 
as reported by singh et al . , imaging of the recipient liver should be performed as close to the time of transplantation as possible because tumors may grow rapidly , invade local structures , or metastasize , which may affect the stage of disease , management perspective , and surgical technique [ 16 ]  . several recent studies have evaluated mri data with gadoxetic acid in patients eligible for transplantation and compared it with findings from the histological examination of the liver in toto [ 1619 ]  . 
 [ 18 ] compared different combinations of diagnostic criteria , obtained by considering only the arterial and hepatobiliary phases , reporting very low sensitivity values ( ranging between 22.5 and 69 % )  . 
these results could be explained by the time lag between the diagnostic test and the liver removal ( in 1 / 3 of the cases of more than 4 months ) and also by the high prevalence of moderately differentiated or well - differentiated hepatocellular carcinomas in the study population . criticism toward this methodological approach was addressed to the excessive number of false positives that the assessment of hepatobiliary phase can generate , resulting in reduced specificity . 
to overcome this limitation , in our study we considered positive only the cases in which the intensity of the lesions was markedly and unequivocally lower than that of the surrounding parenchyma . moreover , our study shows that mri with gadoxetic acid can influence and change the diagnostic classification of patients , and thus re - establish available therapeutic strategies . 
further studies with a large population should be performed to verify the potential of hepatobiliary imaging , especially in patients with advanced liver cirrhosis . conclusions mri with hepatospecific contrast medium shows high sensitivity and specificity in the diagnosis of hepatocellular carcinomas in liver cirrhosis . 
our results show that the diagnostic accuracy was superior to that of the dynamic mri alone , leading to the diagnosis of 8 additional hccs ( 28.6 % of the total lesions )  . the clinical use of this method , especially in patients whose perspectives are liver transplantation , could play a primary role , allowing for a more appropriate management of waiting lists , with a reduced squander of economic and health resources and , above all , a minimization of the waste of organs that could instead be assigned to those patients who could potentially show greater benefits in terms of outcome . 
the accuracy , sensitivity , specificity , positive predictive value ( ppv ) , and negative predictive value ( npv ) of pet / ct , mri - dwi , and pet / mri - dwi image fusion were calculated on a per - patient basis and on a per - node basis . 
however , the figo staging system does not take into account lymph node ( ln ) metastasis ( so - called n staging ) , despite its known adverse impact on survival in gynecological cancer [ 2 , 3 ]  . 
although ln resection before radiotherapy results in improved survival in patients with macroscopically enlarged pelvic and para - aortic lns , routine pre - surgical staging is not generally recommended , even though a lack of assessment of ln involvement may lead to suboptimal treatment [ 49 ]  . indeed , the gold standard for diagnosing ln metastases is currently surgical assessment [ 10 ] , but this is a highly specialized , time - consuming , costly and invasive procedure that increases the patients risk of immediate and delayed complications . 
in this context , computed tomography ( ct ) and magnetic resonance imaging ( mri ) are widely used to assess lns in patients with malignant 1 3 538 radiol med ( 2016 ) 121 : 537545 table 1 demographic and clinical characteristics of the study population tumors , including uterine cancer . 
as the state of the art progresses , various functional imaging techniques , including diffusion - weighted mri ( mri - dwi ) , and combined positron emission tomography and ct ( pet / ct ) using 18f - fluoro - deoxy - glucose ( fdg ) , have been proposed as a method of improving diagnostic performance . to date , there have been three reports on apparent diffusion coefficient ( adc ) obtained with dwi for the detection of ln metastasis [ 1113 ] , and several on pet / ct [ 1420 ] for uterine cancer . 
hardware - based image fusion is performed by means of hybrid scanners , which enable the real - time acquisition and fusion of two different imaging modalities within a single device . 
retrospective software - based image fusion , on the other hand , relies on dedicated software to fuse two separate imaging datasets , most often from ct or mri and single - photon emission tomography ( spect ) or pet . 
this technique , called image registration , is used to align both sets of data so that each voxel corresponds to the same anatomical landmarks in both images [ 22 ]  . as yet , however , there have been few studies [ 23 , 24 ] on the ability of fused pet / mri imaging to identify metastatic lns in patients with uterine endometrial and cervical cancer . 
the purpose of this study was , therefore , to assess the accuracy of retrospective image fusion pet / mri - dwi to pet / ct in detecting metastatic lns in patients with newly diagnosed cervical and endometrial carcinoma , comparing pet / mri - dwi findings with those of both pet / ct and mri - dwi alone . materials and methods patients this retrospective study involved 27 untreated female patients with either endometrial ( n 14 ) or cervical cancer ( n 13 ) ( demographic and clinical data are reported in tables 1 , 2 , 3 ) from october 2011 to december 2013 . 
the time interval between mri scan and pet / ct scan was 033 days ( mean : 10 days )  . subsequently , 11 patients received chemotherapy alone and 2 chemo - radiotherapy . 
as the study was retrospective , approval of the local ethics committee was not sought . pet / ct imaging whole body pet / ct images were obtained using a pet / ct scanner biograph 16 hi - rez ( siemens , hoffman estates , il )  . 
pet images were reconstructed onto a 128 128 matrix using the attenuation - weighted fourier rebinning ( fore - osem ) iterative reconstruction , with two iterations and eight subsets , and a post - reconstruction gaussian volume filter with fwhm 4 mpet , pet / ct , and ct images were analyzed using a dedicated leonardo workstation ( siemens medical solutions )  . 
the processed images were displayed in coronal , transverse , and sagittal planes . mr imaging all patients were scanned using a 1.5 - tesla mri scanner ( achieva intera 1.5 t , philips medical solutions , the netherlands )  . 
pelvic mr images were acquired using a body - sense four - channel phased array pelvic coil for signal reception , with a parallel factor of 1.2 , as follows : axial t2 - weighted turbo - spin - echo spair images ( tr / te : 4760 / 100 ms , slice thickness / intersection gap : 3 / 1 mm , echo train length : 11 , 432 mm )  . 
axial dwi matrix : 560 was performed during free breathing using a stejskaltanner spin - echo echo - planar imaging sequence and a body synergy four - channel coil with parallel factor of zero at the following parameters : tr / te : 8160 / 73 ms ; flip angle : 90 ; nex : 6 ; readout bandwidth : 2369.3 hz / pixel ; matrix : 384 384 ; fov : 370 mm 370 mm ; and slice thickness / gap : 5 / 0 mm , b values : 0 and 800 s / mm2 . 560 , fov : 432 mm image analysis all pet and mri series were retrospectively and manually fused using dedicated image - fusion software , available on the leonardo multimodality workstation ( siemens medical solutions )  . 
mr and pet / ct images were stored in a shared database , and the mr images ( t2 and dwi ) were co - registered to ct images of pet using a semi - automatic voxel - based algorith after image registration , the coregistered images were reconstructed and visualized in the axial plane . 
alignment was assessed by checking the body outline and the position of motionless metabolically active organs ( bone and spine ) in all three planes ( axial , coronal , and sagittal )  . 
when accurate image fusion was not feasible , pet - mri fusion was evaluated by assessing pet / mri - dwi - fused images side - by - side with pet and mri images . 
pet / ct images were interpreted by a nuclear physician ( ms , 17 years experience ) and mr images by an abdominal radiologist ( as , 15 years experience )  . 
on dwi images , lns were classified as cancer positive in the presence of focally abnormal signal intensity higher than the signal intensity of the spinal cord in a location corresponding to the ln chains on t2 - weighted images . 
as adc value differentiation of lns in uterine cancer is reportedly controversial [ 11 , 12 ] , lns in our series were classified on the basis of visual dwi criteria , irrespective of either adc value or size . 
on pet / ct and fused pet / mr images , lns were classed as cancer positive in the presence of either focally appreciable metabolic activity above that of normal muscle , or asymmetric metabolic activity greater than that of normal - appearing lns at the same level in the contralateral pelvis in a location corresponding to the ln chains on the ct or mr images , respectively [ 18 ]  . 
as in a previous study [ 14 ] , lns were grouped according to anatomical landmarks into eight regions : right common iliac , left common iliac , right external iliac , left external iliac , right internal iliac , left internal iliac , right obturator fossa , and left obturator fossa . negative findings , 1 equivocal , needs further follow - up , 3 pet / ct and fused pet / mri - dwi images were interpreted visually using a five - point scoring system as follows : insignificant yet visible lesion , probably metastasis , 4 significant metastasis [ 25 , 26 ]  . 
we created a score sheet ( excel , microsoft , us ) for each patient to enable evaluation of ln region involvement by pet / ct and mri exams , grids of n parameters , imaging techniques ( mridwi , pet / ct , pet / mri ) , and histopathological data . 
images were examined directly on a computer workstation screen . statistical analysis sensitivity , specificity , accuracy , and positive and negative predictive values were calculated for each diagnostic method on a per - patient basis and on a per - node basis , adopting histopathological and follow - up imaging ( ct , mri , and pet / ct ) results as the gold standard . 
medcalc software ( medcalc software , belgium ) was used to perform all statistical analyses . results ln metastases were identified by histopathology in 8 of 27 patients ( 29 % ) , specifically in 37 of the 216 ln regions ( 17 % ) examined . findings on a perpatient basis dwi was true positive for nodal metastases in 7 / 8 ( 87 % ) of patients with ln metastases , and true negative for 13 / 19 ( 68 % ) of patients without node metastases . 
similarly , pet / ct and pet / mri - dwi were true positive for nodal metastases in 7 / 8 ( 87 % ) of patients with node metastasis , but true negative in 16 / 19 ( 84 % ) of patients without node metastasis ( table 4 )  . 
dwi was true positive for 32 of the 37 ( 86 % ) metastatic node groups , and true negative for 119 of the 179 ( 66 % ) non - metastatic node groups . 
pet / ct was true positive for 26 of the 37 ( 70 % ) metastatic node groups , and true negative for 162 of the 179 ( 90 % ) non - metastatic node groups . 
pet / mri - dwi fared better , being true positive for 33 of the 37 ( 89 % ) metastatic node groups and true negative for 164 of the 179 ( 91 % ) nonmetastatic node groups . table 4 parameters of diagnostic performance including fp , fn , tp , tn , sensitivity , specificity . 
the identification of metastatic lns by both ct and mri is based on measurements of node size , and the most widely accepted criterion for diagnosis of nodal involvement , a short - axis diameter greater than 810 mm , has a sensitivity rate for the detection of ln metastasis in endometrial cancer between 27 and 66 % , and a corresponding specificity rate between 73 and 99 % [ 2732 ]  . 
in uterine cervical cancer , ln metastasis detection by these methods is between 30 and 73 % sensitive and between 44 and 93 % specific [ 14 , 31 , 3337 ]  . 
 however , pet / ct shows low sensitivity and high specificity for detecting metastatic lns in patients with uterine cervical and endometrial cancer , whereas dwi shows high sensitivity and low specificity [ 38 ]  . dwi is an mri technique that depicts molecular diffusion , which is the brownian motion of water protons in biological tissues . 
it has been used in oncological imaging for the depiction and characterization of tumors , as well as for differentiating benign from malignant lesions in various kinds of tumors , including uterine cancer [ 13 , 39 ]  . 
the extent of water diffusion can be related to microstructure , microcirculation , cell organization and density , thereby enabling dwi to provide information about the biophysical properties of tissues in vivo . 
however , dwi not only visualizes pathological areas in malignant lesions but also benign pathologies with restricted diffusion [ 39 ]  . 1 3 542 radiol med ( 2016 ) 121 : 537545 kitajima et al . 
 [ 38 ] reported that dwi shows higher sensitivity and lower specificity than pet / ct in detecting ln metastasis in patients with uterine cancer ( endometrial cancer and cervical cancer )  . 
however , the quantitative adc value used is controversial for differentiating malignant from benign lns in uterine cancer [ 1113 ] , suggesting that adc analysis is not acceptable for the preoperative evaluation of ln metastasis in patients with uterine cancer . 
this explains why we performed no adc analyses in our study . studies documenting the accuracy of fdg - pet / ct for detecting ln metastasis in uterine cancer [ 1420 ] have reported that pet / ct tends to show low sensitivity and high specificity ; this observation is confirmed in our series , and may be explained by the tendency of this technique to underestimate standardized uptake values in tiny lns due to the partial volume effect . 
this makes the usual cutoff ( 2.53.0 ) for differentiating malignant from benign lns unreliable , and many studies have failed to perform semiquantitative analysis to determine a standardized value for fdg uptake in nodal lesions [ 1517 ]  . 
fdg - pet / ct is also unable to detect microscopic metastasis , which is unsurprising as pet has a mean spatial resolution value of 0.5 cm ( range 0.40.6 cm ) , making small lymph nodal metastases almost undetectable [ 1417 ]  . to our knowledge , this is the first reported study to have investigated the validity of retrospectively fused dwi / t2 - mri to pet / ct images from different scanners for nodal staging of endometrial and uterine cervical cancer . 
the differences between these three parameters were not statistically significant likewise , we found no statistically significant differences between either pet / ct and mri - dwi or pet / ct and pet / mri - dwi on a per - patient basis . 
 the t2 - weighted mr sequence a , b there is a slightly hyperintense pathologic tissue ( circled in red ) in the uterine cervix and bilateral obturator enlarged lymph nodes ( circled in green )  . 
dwi c and the co - registered pet / dwi images d show the same findings 1 3 radiol med ( 2016 ) 121 : 537545 nevertheless , in our sample there were three false - positives cases with dwi , but true negatives with pet / ct and pet / mri - dwi . 
however , on a per - node basis , our sensitivity , specificity , ppv and npv values for fused pet / mridwi were greater than those of pet / ct . 
nevertheless , since the establishment of surgical staging as the standard initial step in the management of most patients with endometrial and cervical cancer , pelvic and para - aortic lymphadenectomy as part of surgical staging has become more common , due to reports showing diagnostic and therapeutic advantages fig . 
dwi b shows a focal area of restriction of diffusivity in the left external iliac location ( white arrow ) , scored as possibly metastasis ( score 3 )  . 
 indeed , nodal resection often does not confer a survival benefit in these patients [ 4347 ] , and routine pelvic lymph node dissection may itself expose the patient to risks such as intraoperative vascular injury , as well as , serious complications such as lymphedema and lymphocyst in the long teralthough these risks decrease in the hands of an experienced surgeon [ 48 , 49 ] , the risk of lymphedema and lymphocysts appears to be related to the number of lns removed [ 49 , 50 ]  . 
it follows , therefore , that a group of lowrisk patients exists who may not need routine lymph node dissection . in light of our findings , pet / mri - dwi may prove to be an accurate and non - invasive tool for the pre - planning of surgical procedure and guidance of minimally invasive node resection in low - risk patients . 
moreover , pet / mri - dwi evaluation could be considered in a preoperative prediction model ( comprising other parameters such as serum cancers markers , mri to assess invasion , histological grade , and clinical stage ) to determine which patients can avoid lymph node dissection , thereby obviating the need for a pathologist to be present during intraoperative assessment . however , this study has several limitations . 
specifically , our case series was relatively small and a larger number of patients will need to be studied to more accurately evaluate the role of pet / mri - dwi in ln metastasis detection . 
furthermore , in our fused sequences , considering pelvic mr images rather than whole body mri , we could only assess pelvic , but not para - aortic lns , whose involvement has nevertheless been assigned an important prognostic value [ 14 , 15 ]  . 
moreover , scores were subjective and given by only two readers on the basis of visual interpretation of the images . conclusions although we found no statistically significant differences between pet / mri - dwi and pet / ct either on a perpatient or per - node basis , indicating that they have similar diagnostic accuracy in n staging in uterine cancer , pet / mri - dwi did show higher sensitivity , specificity , ppv and npv than fdg - pet / ct on a node - by - node basis . 
judging by our results , in the absence of other non - invasive n - staging methods for these types of cancer , the potential of imaging fusion techniques deserve further investigation . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards informed consent was obtained from all participants . 
mr dacryocystography was performed by using heavily t2 - weighted fast spin echo sequence in the coronal and axial planes after the topical administration of normal saline drops into the conjunctival sacs . results in mr dacryocystography , stenosis / obstruction at the canalicular level was correctly diagnosed in nine patients ( 100 % )  . 
most primary acquired obstructions are due to idiopathic inflammation , fibrosis , and scarring of the nasolacrimal duct [ 1 ] , and obstruction can occur at any level along the lacrimal drainage : punctum , canaliculus , sac , nasolacrimal duct , or nasal ostiu to select the proper surgical procedure , it is important to know the etiology and location ( so called positional diagnosis [ 2 ] ) of the obstruction . 
assessment of nasolacrimal duct obstruction had been primarily conducted by dacryocystography as the conventional radiographic imaging technique [ 3 ] , and followingly conducted by ct dacryocystography with topical instillation of contrast material [ 4 ]  . 
since mr dacryocystography does not require cannulation , ionizing radiation and chemical contrast media with high viscosity , some studies showed that mr dacryocystography was an easily and safely performed imaging technique to identify the presence or absence of obstruction and its level , compared with conventional dacryocystography and ct 1 3 radiol med ( 2016 ) 121 : 580587 dacryocystography [ 3 , 69 ]  . 
more recently , dacryoendoscopy [ 2 , 1012 ] has been developed that allows direct visualization of the internal condition of the lacrimal passage , and has been reported to be a useful technique to directly diagnose the site of obstruction with accuracy in nasolacrimal duct obstruction . 
in this study , we aimed to compare the findings of mr dacryocystography with those of dacryoendoscopy and subsequent surgery in patients with nasolacrimal duct obstruction and to determine the efficacy of mr dacryocystography in the positional diagnosis of nasolacrimal duct obstruction . materials and methods study population this retrospective study was approved by our institutional review board , and the requirement for informed consent was waived . 
from july 2004 to july 2008 , 31 patients ( 13 men and 18 women ; mean age 64.6 years ; range 3884 years ) with clinically suspected nasolacrimal duct obstruction underwent mr dacryocystography , and were included in this study . 
patients with nasolacrimal duct obstruction related to neoplasms and previous dacryocystorhinostomy were excluded from this study . mr imaging technique mr imaging was performed using a 1.5 - t superconducting mr scanner ( signa excite high speed ; general electric , milwaukee , wi , usa )  . 
before the mr scanning , eyedrops using a sterile 0.9 % nacl solution were applied into the conjunctival sac of both eyes of each patient ( two drops / min per eye over a duration of 5 min ) while the patient were in spine position . 
immediately after final eye drop , mr dacryocystography was performed by heavily t2 - weighted fast spin echo sequence in the coronal and axial planes using the following parameters ; tr / 20.83 khz , signal averages 15 cm , 0.5 mm , slice thickness 192 . 
additional mr imaging sequences matrix 550 / 12.4 ms , included axial t1 - weighted ( tr / te 2 ) and t2 - weighted 20.83 khz , sig ( tr / te 3 ) fast spin echo sequences ( field nal averages 3 mm , of view 15.53 khz , signal averages 4000 / 102 ms , bw 3 , field of view 3 mm , interslice gap 8000 / 255258 ms , band width ( bw ) 15 cm , slice thickness 15 15 256 256 0.5 mm , matrix 3139 / 1295 ms , bw interslice gap 192 ) , and coronal t2 - weighted half - fourier single - shot fast spin echo 20.83 khz , sequence ( tr / te 16 cm , signal averages slice thickness gapless , 192 )  . 
 overall mr imaging time was less 25 min . 3 , field of view 16 4 mm , interslice gap 256 image analysis mr dacryocystography was reviewed independently by two radiologists who were blinded to any clinical information of the subjects , and was evaluated for the detection of obstructed points in the nasolacrimal drainage system according to three levels ( canaliculus , lacrimal sac and nasolacrimal duct )  . 
values were interpreted as follows : less than 0.20 indicates poor agreement , 0.210.40 indicates fair agreement , 0.410.60 indicates moderate agreement , 0.610.80 indicates good agreement , and 0.80 or higher indicates excellent agreement . 
coronal and axial mr dacryocystography show no fluid in the lacrimal sac ( arrows in a , b , d and e ) and nasolacrimal duct ( arrows in c and f )  . 
stenosis / obstruction involved at the canalicular level in 9 patients , at the lacrimal sac level in 16 , at both the canalicular and the lacrimal sac level in 3 , and at the nasolacrimal duct or nasal ostium level in 3 patients ( table 1 )  . 
in mr dacryocystography , stenosis / obstruction at the canalicular level was correctly diagnosed in nine patients ( 100 % ) based on the finding of no fluid in the lacrimal sac and nasolacrimal duct . 
regarding stenosis / obstruction at the lacrimal sac level , 14 ( 87.5 % ) of 16 patients were correctly diagnosed in mr dacryocystography while there were discrepancies between mr dacryocystography and dacryoendoscopy in the assessment of stenosis / obstruction sites in the remaining two of 16 patients . 
in these two patients , stenosis / obstruction was assumed to be at the nasolacrimal duct or nasal ostium level on mr dacryocystography , whereas stenosis / obstruction was seen at the lacrimal sac level on dacryoendoscopy . 
coronal and axial mr dacryocystography show incomplete filling of fluid in the dilated sac ( arrows in a , b , d and e ) , with no filling of the nasolacrimal duct ( arrows in c and f )  . 
thickened mucosa of the nasolacrimal duct with intermediate signal can be observed both the canalicular and the lacrimal sac level on dacryoendoscopy , all three patients were misinterpreted as stenosis / obstruction at the canalicular level on mr dacryocystography . 
in these three patients , fluid was not observed in the lacrimal sac and nasolacrimal duct , probably due to coexistent stenosis / obstruction at the canalicular level proximal to the lacrimal sac . 
the overall accuracy of mr dacryocystography in depicting the stenosis / obstruction in nasolacrimal system was 84 % . discussion dacryoendoscopy can directly visualize lacrimal drainage system , and correctly diagnose the location of the obstruction preoperatively in patients with the nasolacrimal duct obstruction , and therefore , can provide useful information for the subsequent endoscopy - guided surgical procedures [ 2 , 10 , 1215 ]  . 
several studies have reported that mr dacryocystography provided detailed information about the nasolacrimal system without risks associated with cannulation , and could be a useful method for depicting nasolacrimal duct obstruction [ 5 , 8 , 9 , 16 ]  . 
in this study , mr dacryocystography can correctly depict the stenosis / obstruction in nasolacrimal system in 26 ( 84 % ) of 31 patients who were confirmed by preoperative dacryoendoscopy . 
coronal and axial mr dacryocystography show the dilated sac filled with fluid normally ( arrows in a , d ) , with the filling of the nasolacrimal duct ( arrows in b , c , e and f ) table 1 stenosis / obstruction level of nasolacrimal duct obstruction on dacryoendoscopy in all 31 patients stenosis / obstruction level number of patients canalicular level lacrimal sac level both canalicular and lacrimal sac level nasolacrimal duct or nasal ostium level dacryocystographic images allowed detailed assessment of luminal changes . there are three locations of physiologic narrowing in the nasolacrimal duct system [ 8 ]  . 
in this study , dacryoendoscopy with subsequent surgery revealed that a total of 19 ( 61 % ) of 31 patients with nasolacrimal duct obstruction had stenosis / obstruction at lacrimal sac only , and the level of the lacrimal sac ( 16 both the canalicular and the lacminal sac ) , suggesting a common condition in nasolacrimal duct obstruction . 
in these 16 patients with stenosis / obstruction at the level of the lacrimal sac only , 14 patients were correctly diagnosed in mr dacryocystography , whereas , stenosis / obstruction was assumed to be at the level of the nasolacrimal duct or nasal ostium in the other two patients . 
otherwise , these two patients had stenosis at the level of the lacrimal sac , but did not have complete obstruction , showing administered saline fluids flowed into the nasolacrimal duct . 
additionally , all three patients with coexistent stenosis / obstruction at both the canalicular and the lacrimal sac level were misinterpreted as stenosis / obstruction at the canalicular level on mr dacryocystography . 
since stenosis / obstruction at the lacrimal sac level occurs most frequently , it will be important to consider that stenosis / obstruction in the lacrimal sac level may coexist when the obstruction in canalicular level was seen . mr dacryocystography has some advantages over digital dacryocystography and ct dacryocystography . 
mr 1 3 radiol med ( 2016 ) 121 : 580587 table 2 comparison of stenosis / obstruction level of nasolacrimal duct obstruction between mr dacryocystography and dacryoendoscopy in all 31 patients patient fluid in lacrimal sac fluid in nasolacrimal duct mr dacryocystography dacryoendoscopy concordance of both studies presence presence presence presence presence presence absence absence absence absence absence absence presence presence presence presence presence presence absence presence absence presence absence absence presence presence presence presence presence absence absence absence absence presence absence absence presence absence absence absence absence absence absence absence absence absence presence absence presence absence absence absence absence absence absence absence presence absence absence absence absence absence both canalicular and lacrimal nasolacrimal duct nasolacrimal duct nasolacrimal duct nasolacrimal duct canaliculus both canalicular and lacrimal lacrimal sac lacrimal sac lacrimal sac lacrimal sac canaliculus canaliculus canaliculus canaliculus canaliculus lacrimal sac lacrimal sac lacrimal sac canaliculus lacrimal sac canaliculus lacrimal sac canaliculus canaliculus lacrimal sac lacrimal sac lacrimal sac lacrimal sac canaliculus canaliculus nasolacrimal duct lacrimal sac nasolacrimal duct lacrimal sac lacrimal sac lacrimal sac lacrimal sac sac level canaliculus canaliculus canaliculus canaliculus sac level lacrimal sac lacrimal sac lacrimal sac lacrimal sac lacrimal sac lacrimal sac canaliculus lacrimal sac canaliculus lacrimal sac canaliculus canaliculus lacrimal sac lacrimal sac lacrimal sac lacrimal sac canaliculus sac level nasolacrimal duct nasolacrimal duct both canalicular and lacrimal dacryocystography uses no ionizing radiation that focuses on the lenses of the eyes , and requires no local anesthesia , no cannulation of the punctum , and no injection of viscous contrast media , and has no risk of iatrogenic trauma on the punctu in this study , mr dacryocystography was performed by using the topical administration of normal saline drops into the conjunctival sacs although some previous studies have performed mr dacryocystography with the use of diluted gadolinium contrast medium , which is an off - label use for mr dacryocystography [ 5 , 7 , 1619 ]  . 
we preferred saline solution because , as compared to gadolinium contrast medium , the saline solution has a lower viscosity , and therefore , causes less irritation in the mucosal structures . 
regarding image quality , one study has compared topical applications of saline solution and gadolinium solution [ 20 ] , and reported that the images obtained after the application of the gadolinium solution had artifacts caused by the susceptibility effect , compared with those obtained after the application of the saline solution . 1 3 586 radiol med ( 2016 ) 121 : 580587 furthermore , mr dacryocystography has some advantages over dacryoendoscopy . 
accordingly , for the positional diagnosis of nasolacrimal duct obstruction , mr dacryocystography may be replaced for dacryoendoscopy . one limitation of this study was that it was retrospective in nature , and the number of patients was limited . 
when combined with t1and t2 - weighted fast spin echo sequences , mr allows anatomic imaging of extraductal soft tissues and neoplastic lesions within the lacrimal system although this evaluation was not pursued in this study . 
it will be important to compare the images obtained before and after the administration of normal saline drops to differentiate the chronically retained fluid collection in the lacrimal duct system from administered saline solutions . 
further studies comparing images before and after the administration of normal saline drops will be necessary to validate the diagnostic role of mr dacryocystography . in conclusions , mr dacryocystography after the topical administration of normal saline drops into the conjunctival sacs is a well - tolerated , minimally invasive imaging technique to identify the level of stenosis / obstruction in patients with nasolacrimal duct obstruction , and could be used as a reliable preoperative method prior to dacryoendoscopy and subsequent surgery . acknowledgments we thank jou sakai , department of ophthalmology , kasai city hospital , for technical procedure of dacryoendoscopy . compliance with ethical standards conflict of interest hiroki higashi declares that he has no conflict of interest . 
vogl1 tatjana gruberrouh1 received : 10 august 2015 / accepted : 14 march 2016 / published online : 21 april 2016 italian society of medical radiology 2016 abstract objective evaluation of the intimal flap visibility comparing 2nd and 3rd generation dual - source high - pitch ct . methods twenty - five consecutive patients with aortic dissection underwent ct angiography on a second and third generation dual - source ct scanner using prospective ecggated high - pitch dual - source ct acquisition mode . 
the visibility of the intimal flap as well as the delineation of the different vascular structures was evaluated . results in 3rd generation dual - source high - pitch ct we could show a significant improvement of intimal flap visibility in aortic dissection . 
however , to generalise these findings larger trials are needed . keywords ct angiography aorta high - pitch ct dual - source ct introduction aortic dissection is a potentially fatal clinical emergency . 
conservative therapy is the treatment of choice in the majority of stanford type b dissections while stanford type a dissections are referred for surgical or interventional treatment in nearly all cases [ 5 ]  . 
repeated imaging to exclude aortic rupture by assessment of the aortic dissection and the aortic diameter is an essential element when monitoring patients under conservative treatment [ 4 , 6 ]  . 
 available imaging modalities for follow - up of type b aortic dissections include computed tomography ( ct ) , magnetic resonance imaging ( mri ) , ultrasound and conventional angiography [ 5 ]  . 
current generation dual - source ct scanners are capable of pitch values above 3 [ 7 ] , which makes full length aortic scanning in sub - second levels feasible [ 812 ]  . 
 dual - source high - pitch acquisition is especially beneficial in the evaluation of the thoracic aorta where heart and aortic motion artefacts can mimic aortic dissection [ 10 , 13 ]  . 
all patients were examined for follow - up of their aortic dissection under conservative treatment . materials and methods subjects this study was performed using a single - centre , observerblinded , retrospective design . 
all primary patients who underwent clinically indicated cta of the entire aorta for follow - up of aortic dissection from october 2013 to october 2014 were included in this study . this patient cohort consisted of 25 individuals ( table 1 )  . 
 each patient had received two scans : the first scan on a second generation dual - source ct ( somatom definition flash ; siemens healthcare , forchheim , germany ) , and the second scan on a third generation dual - source ct ( somatom force ; siemens healthcare , forchheim , germany )  . 
 1 3 radiol med ( 2016 ) 121 : 573579 contrast medium volume was kept constant between both groups at 90 ml of iodinated contrast material ( iodine concentration : 400 mg / ml , imeron 400 , bracco imaging , konstanz , germany ) followed by a 50 ml saline chaser bolus . 
an 1820 g intravenous access on the patients forearm was used for contrast injection with a flow of 4 ml / s using a double - syringe power injector ( injektron ct2 , medtron , saarbruecken , germany )  . 
cta was automatically triggered by the bolus - tracking technique ; the roi was placed in the descending thoracic aorta at the height of the pulmonary trunk and the trigger threshold was set at 200 hu . 
the start delay was set to 7 s in both groups . transverse images were reconstructed at 0.75 mm slice thickness with 0.5 mm increment , a matrix size of 512 512 and a cta window ( centre : 100 hu ; width : 700 hu )  . 
group 2 images were reconstructed using a medium - soft convolution kernel in filtered back projection technique ( bv 36 ) [ 14 ]  . image analysis objective image analysis ability to rule out type a and b dissections , to define the startand end - point of each dissection , as well as to visually delineate the intimal flap at mid distance between these two points . 
the rating further included visualisation of the coronary ostia for analysis of movement artefacts ( 5 no moderate artefacts ; artefacts ; 4 minimal artefacts ; 3 extensive artefacts ; 1 severe artefacts )  . radiation exposure ct dose index ( ctdivol ; in mgy ) was recorded from the patient protocol , which is automatically generated at the end of each examination . 
mas settings using automated dose control software ( table 1 )  . statistical analysis all statistical analyses were performed using dedicated software ( stata / ic 13.1 , statacorp lp , texas , usa )  . 
a cohens kappa analysis was performed to determine inter - observer agreement for subjective image quality scoring . results measures of objective image quality were performed by a radiologist with 5 years of experience in ct angiography on a commercially available pacs workstation ( centricity 4.2 , general electric healthcare , munich , germany )  . 
several region - of - interest ( roi ) measurements were drawn using a circle tool ( ascending aorta , descending aorta , aorta at celiac trunk , femoral artery )  . 
based on these measurements , the signal - to - noise ratio ( snr ) was determined according to the following equation : snr attenuation / image noise . all ct examinations were of diagnostic image quality ; no examinations had to be excluded from analysis . 
contrast enhancement was rated as sufficient in all patients . objective image quality median snr of the aorta at the level of the coeliac trunk was 36.6 for group 1 and 41.2 for group 2 ( p 0.03 ) ( table 4 )  . 
for evaluation of the intimal flap , we evaluated , based on the quality of the images , the readers moderate ; 2 excellent ; 4 good ; 3 fair ; 1 visual comparison of the intimal flap revealed a significant difference in the visualisation of the proximal as well as the distal intimal flap region ( table 3 )  . 
imaging time and imaging length were comparable in both groups and did not reach statistical significance ( table 4 )  . in our study , we showed a significant improvement of image quality in evaluation of the proximal and distal ends of the intimal flap using 3rd generation dual - source highpitch ct . this improvement of intimal flap visualisation is directly related to the readers ability to judge progression of the intimal tear . 
as image reconstruction did not differ , we think that the main driver in this setting is the higher tube output in the new 3rd generation ct scanner compared to the 2nd generation ct scanner [ 15 ]  . in clinical routine a verification of the intimal flap along the patient z - axis is one of the main questions of the referring clinician . 
imaging on 3rd generation dual - source ct has clearly visualised the dissection membrane ( left hand side ) 1 3 radiol med ( 2016 ) 121 : 573579 fig . 
3 dissection membrane ( stanford a - dissection ) in 3rd generation dual - source ct ( force ) intimal flap description is at need and if a small dissection , in the end , really changes the therapy . 
larger trials are needed to focus on these questions . radiation dose was found to be roughly constant , while automated tube current modulation and automated tube potential selection ( care kv , siemens healthcare , forchheim , germany ) were enabled in both groups ( image quality parameters in table 1 )  . 
because the examined patients were the same in both groups , we consider this assessment of radiation dose valid , as far as can be evaluated with a population group of this size . 
reported a radiation dose of 3.2 msv for a thoraco - abdominal examination , with a coronary ct angiography protocol at a pitch of 3.2 imaged with 120 kvp using automated tube potential selection [ 16 ]  . 
found a significant reduction of radiation exposure as well as contrast material using 70 kev as well as dual - source high - pitch ct for the imaging of cardiac vessels [ 17 ]  . 
the radiation dose reduction is likely to be a result of the adjustment of the tube potential to 70 kev . in our data , contrast enhancement was adequate in all cases within our study . 
this is in line with enhancement values of vessel enhancement reaching 200 hu or higher reported in the literature [ 1820 ]  . in this study , a threshold of 200 hu was used , since a lower threshold will result in higher delay - times . 
there are two common strategies for the timing of contrast bolus : either the test - bolus or the bolus - tracking method is used [ 21 , 22 ]  . 
however , as ongoing developments have led to increased imaging speeds [ 18 ] , there has been a trend considering the higher attenuation thresholds necessary for adequate vessel enhancement in ct angiography . 
the bolus - tracking technique , however , remains a gold standard for imaging of the aorta from the results of this study , since it is both easy to use and does not require a second injection of contrast material . limitations we are aware of several limitations of this study . 
the resulting interobserver agreement was good , suggesting that observer bias was low . another limitation is the retrospective approach ; however , this observational study might be a first step for further evaluations . finally , due to the fast table movement , the ct tube operates at a tube current close to its absolute capacity . 
according to protocol output , however , the capacity of tube output was not reached in either examination . conclusion third generation high - pitch dual - source ct significantly improves delineation of proximal and distal ends of the intimal flap in aortic dissections . 
however , to really verify if a better delineation leads to a change in clinical treatment , larger trials are needed . 1 3 radiol med ( 2016 ) 121 : 573579 compliance with ethical standards conflict of interest no funding was received for this work . 
the authors declare no potential conflict of interest . ethical standards the local ethics committee approved this study , and informed consent was waived because of the retrospective nature of the study . 
the current article reports the prevalence and correlates of a smrv and a tmrv 5000 among italian breast screening radiologists . materials and methods a questionnaire survey was carried out in 20132014 by the italian group for mammography screening ( gisma )  . 
multivariate factors and 163 ( 73.4 % ) a tmrv positively associated with both characteristics included : the number of years of experience reading mammograms ; the percentage of total working time dedicated to breast imaging and breast care ; the participation in diagnostic assessment ; and the availability of digital tomosynthesis at facility . 
these include several personal characteristics [ 13 , 511 ] as well as facility - level factors ( for example , the number of interpreting radiologists at facility ) [ 2 ]  . 
however , because the volume of procedures has been shown to be a strong determinant of quality in numerous medical fields [ 12 ] , the experience - related factor that has received the most attention in the literature is the annual mammogram reading volume ( mrv ) [ 13 , 611 ]  . 
 expectedly , most studies have consistently demonstrated a close independent association between mrv and radiologists accuracy [ 6 , 7 , 11 , 13 ]  . this notion is reflected in the european guidelines for quality assurance in breast cancer screening and diagnosis , which state that each radiologist should : have had specific training both in screening and in clinical mammography ; participate in a continuing medical education programme ; be involved both in basic screening and in assessment of women with abnormal screening results ; and read a minimum of 5000 screening mammograms per year [ 14 ]  . 
the more recent european society of breast cancer specialists ( eusoma ) position paper for specialist breast centre certification states that each breast radiologist working in a centre must read a minimum of 1000 mammography cases per year , which rise to 5000 , including both screening and clinical mammograms , if he participates in a screening programme [ 15 ]  . in 20132014 , the italian group for mammography screening ( gruppo italiano screening mammografico , gisma ) , the scientific society that promotes communication and dissemination of knowledge across the mammography screening community in the country , carried out a questionnaire survey aimed ( 1 ) at evaluating the distribution of italian breast screening radiologists by the main experience - related characteristics , and ( 2 ) at acquiring a list of screening centres offering training opportunities . 
 our aim was to evaluate the prevalence of radiologists with a mrv 5000 and the factors significantly associated with it , in order to find clues to improvement in this critical indicator of radiologists experience . materials and methods setting in italy , mammography screening is implemented on a health care district basis . 
detailed information on geographic coverage , target population , performance indicators , and impact indicators can be found elsewhere [ 1619 ]  . questionnaire the questionnaire was developed by two of us ( dm and lb ) after consultation of the relevant literature , was amended by a third author ( lg ) , and was tested on a randomly selected group of radiologists . 
the items were divided in two sections : one devoted to the characteristics of the screening centre and of employed radiologists ( see appendix ) , and the other to the offer of training opportunities . the questionnaire was saved as a microsoft excel file with locked cells and , in june 2013 , was sent via e - mail to all radiologists enrolled in the gisma . 
the deadline for responding was december 31 , 2013 , although a small number of questionnaires were received in early 2014 . items of information we used a subset of items of the questionnaire . 
from among the radiologists experience - related characteristics ( personal characteristics ) , we selected the following : number of screening mammograms read per year , calculated as the average of the last 3 years ; number of clinical mammograms read per year , calculated as the average of the last 3 years ; years of experience in reading both screening and clinical mammograms ; percentage of total working time dedicated to breast imaging and breast care , calculated as the average of the last 3 years ; and regular participation in diagnostic assessment sessions for women with abnormal screening mammography results . 1 3 radiol med ( 2016 ) 121 : 557563 results response with respect to the facility - level factors supposedly associated with the mrv , we used the following : geographic area ( north , centre , south ) ; year of implementation of the screening programme ; number of interpreting radiologists at facility ( each single facility in multi - facility screening programmes ) ; availability of digital mammography ; availability of digital tomosynthesis ; and availability of vacuum - assisted biopsy . 
for reasons of quality of information , the year of implementation of the screening programme was taken from a set of data that the gisma and the national centre for screening monitoring ( italian : osservatorio nazionale screening , ons ) collected in 2013 from local screening programmes . data for 235 radiologists from 51 health care district screening programmes were received . 
the 51 surveyed programmes accounted for 46.8 % of the 109 active programmes known to the ons . data analysis characteristics of radiologists the total number of breast radiologists working in the screening centres in italy is unknown , because their registration with official bodies is not mandatory . 
 under these conditions , we estimated the approximate surveys coverage in two alternative ways : first , as the proportion of respondent radiologists out of the number of radiologists enrolled in the gisma ; and , second , as the proportion of surveyed programmes out of the number of active programmes notified to the ons [ 17 ]  . 
the first was the screening mrv ( smrv ) , defined according to the european guidelines for quality assurance in breast cancer screening and diagnosis [ 14 ] , and the second was the total mrv ( tmrv ) , i.e. 
the sum of screening and clinical mammogram readings , defined according to the eusoma position paper [ 15 ]  . differences in proportions were tested for significance with the fishers exact test and the 2 test for heterogeneity , and trends in proportions with the 2 test for trend . 
given the skewed distribution of percentages of working time dedicated to breast imaging and breast care , the variable was also categorised into tertiles and both models were run again . the 222 eligible radiologists were mostly ( 163 or 73.4 % ) from northern italy . 
the median number of clinical mammograms read per year was 1400 ( range 010 , 000 )  . factors associated with a smrv and a tmrv 5000 the right part of table 1 shows the results of univariate and multivariate analysis . 
both approaches demonstrated that the geographic area , the number of radiologists at facility , and the availability of digital mammography were not significantly associated either with a smrv or a tmrv 5000 . factors significantly associated with the probability of 5000 in multivariate analysis included an early a smrv year of implementation of the screening programme , a high number of years of experience in reading mammograms , a percentage of working time dedicated to breast imaging 75 % , a regular participation in diagnostic and breast care assessment sessions , and the availability of digital tomosynthesis at facility . 
this was entirely explained by the fact that the variable was strongly and positively associated ( p 0.007 ) with the year of implementation of the programme ( data not shown ) , that 1 3 560 table 1 breast screening radiologists experience - related characteristics and facilitylevel factors associated with a screening mammogram reading volume ( smrv ) and a total ( screening and clinical ) mammogram reading volume ( tmrv ) 5000 per year radiol med ( 2016 ) 121 : 557563 factor total no . 
the availability of vacuum - assisted biopsy at facility was significantly associated with the outcome variable in univariate analysis , but not after simultaneous adjustment for confounders . the pattern of associations with tmrv was similar , but not equal , to that for smrv . 
the availability of vacuumassisted biopsy at facility emerged as a significant independent determinant , whereas the year of implementation of the screening programme was not retained in the multivariate model . 
more important , a high percentage of working time dedicated to breast imaging and breast care and a regular participation in diagnostic assessment sessions had a much stronger influence on tmrv than on smrv . after categorising the percentage of working time dedicated to breast imaging and breast care into tertiles , we ran both models aga as shown in table 2 , using the 10 to 50 % category as a referent , the odds ratio for a fig . 
note : the annual number of mammograms ( 73.4 % ) a tmrv reported by radiologists was rounded to the nearest multiple of 100 1 3 radiol med ( 2016 ) 121 : 557563 table 2 association of the percentage of working time dedicated to breast imaging and breast care , categorised into tertiles , with a screening mammogram reading volume ( smrv ) and a total ( screening and clinical ) mammogram reading volume ( tmrv ) 5000 per year percentage of working time dedicated to breast imaging and breast care ( tertiles ) ( % ) 1050 5199 total no . 
these variables were removed if the likelihood ratio statistic based on the maximum likelihood estimates had a probability > 0.1 or odds ratio , ci confidence interval a p < 0.05 ( test for trend ) 5000 was not significant for a percentage varysmrv ing between 51and 99 % , while raising to above 11 among radiologists with full - time dedication . 
both indicators were above the recommended threshold for more than 90 % of radiologists with full - time dedication . discussion in italy , there never have been nationwide data on the experience - related characteristics of breast screening radiologists . 
this provided a strong rationale for the present study . since mammography screening and diagnostic breast imaging are increasingly integrated into multidisciplinary specialist breast centres [ 15 ] , we took both smrv and tmrv as endpoints of analysis . 
conversely , the finding that the probability of a smrv 5000 was lower in those screening programmes that have been implemented in the most recent years was unexpected and disappointing . 
if so , our observation might predict other unfavourable characteristics of recent programmes . smrv and tmrv increased with increasing number of years of experience [ 1 , 3 , 7 , 10 ]  . 
because both associations were adjusted for the working time dedicated to breast imaging and breast care , the most likely interpretation is that the more the years of experience the greater the reading volume per time unit . 
in this time of budget difficulties , this finding deserves attention . an association between the percentage of working time dedicated to breast imaging and breast care and both mammogram reading volumes has already been reported by others [ 1 ]  . 
 although screening authorities in italy recommend that breast radiologists spend at least half of their time reading mammograms [ 21 ] , this is not sufficient to reach the standard smrv . 
the percentage of working time dedicated to breast imaging and breast care had an even stronger effect on tmrv , with a 47 - fold increased probability of reaching a level 5000 for full - time dedication . 
as many as 98 % of full - time radiologists were in line with the eusoma requirement [ 15 ]  . a high percentage of working time dedicated to breast imaging and breast care was also likely to increase the probability for radiologists to participate in diagnostic assessment sessions [ 1 , 5 ]  . 
 the explanation we suggest is that reading volumes and participation in diagnostic assessment were both associated with a third radiologist characteristic , that is , a high degree of commitment to breast imaging and breast care . in screening centres equipped with digital tomosynthesis , the probability of radiologists reporting a smrv and a tmrv 5000 was higher . 
a plausible interpretation for our finding is that those radiologists who are interested in digital tomosynthesis have high expertise and strong 1 3 562 radiol med ( 2016 ) 121 : 557563 commitment to breast imaging and breast care . 
this technique is used by breast radiologists who spend much working time in the clinical mammography setting , where they are also employed in the assessment of women with abnormal screening results . 
the fact that these radiologists have a higher tmrv but not a higher smrv is plausible . although a smrv and a tmrv 5000 per year remain important targets , a balanced workload allocation is also needed on the other side of the distribution because there could be an upper limit above which the readers performance deteriorates . 
a mately 2 %reported a smrv and a tmrv study from the uk has demonstrated a lower cancer detection rate in the group of screening radiologists who read 25 , 000 mammograms in a 3 - year period [ 9 ]  . there are two limitations of this study that warrant mention . 
first , although the proportion of missing values was very low , some study variables were subject to the recall bias and other potential sources of error associated with self - reporting . 
in fact , we do not know whether the true rate is nearer to the proportion of respondent radiologists out of the number of radiologists enrolled in the gisma , i.e. 
the reported median number of four radiologists per screening centre , which is above that expected , indicates that the participation was higher among largestaffed centres . conclusions we performed this study with the objective of finding modifiable factors for the likelihood of a smrv and a tmrv 5000 , that is , of finding clues to improvement in these major indicators of radiologists experience . 
first , the year of implementation of the screening programme is not modifiable ; second , the number of years of experience will inevitably decrease in the next few years because of the projected retirement of a substantial part of the medical workforce of the italian national health service , including numerous experienced radiologists ; and third , the complex relationships that link smrv and tmrv to regular participation in diagnostic assessment and to technical level of the screening centre do not suggest appropriate actions in an objective manner . 
conversely , our results point to an increase in the proportion of radiologists with full - time dedication to breast imaging and breast care as a clear and effective way to improve both mammogram reading volumes . acknowledgments the authors thank the radiologists who participated in the survey . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest and that the study has been carried out without any financial support . ethical standards this article does not contain any studies with patients or animals performed by any of the authors . appendix items of the questionnaire . 
the questionnaire was divided into two sections : one devoted to the characteristics of the screening centre and of employed radiologists , and the other to the offer of training opportunities . 
 surgery was in 14 non - responder patients . conclusions ultrasound - guided alcoholization demonstrated a safe profile , relieved neuropathic symptoms in a majority of patients and improved their quality of life . 
1 intermetatarsal bursa ; 2 neuroma ; 3 deep transverse intermetatarsal ligament ; 4 common digital nerve ; asterisk plantar side radiol med ( 2016 ) 121 : 597604 current views support an entrapment of the nerve between the anterior margin of the deep intermetatarsal transverse ligament and the third and fourth metatarsal heads as the etiopathogenetic cause of the disease , with forefoot postural overloading as a predisposing factor . 
pathology specimens are characterized by a hyaline degeneration of endoneurium , endoneural edema and endoand peri - neural connective tissue deposition [ 1 , 5 ]  . the clinical presentation is known as civininimorton syndrome ( cms ) or civininimorton metatarsalgia . 
patients experience neuropathic pain due to cms [ 24 , 69 ] which can present together with a component of nociceptive pain [ 10 ] , possibly due to comorbid conditions . mn diagnosis is mainly based on its clinical features and physical examination [ 2 , 11 , 12 ]  . 
if the result after the third session was unsatisfactory , the patient was offered either extended evaluation for forefoot comorbidities or up to two or more sessions of alcoholization or surgical neurectomy , depending on clinical evaluation and the patient preference . data collection clinico - demographic data were collected from clinical records : age , sex , time from onset of symptoms to referral , fig . 
b neuroma in third intermetatarsal space ( asterisk ) ; flexor digitorum tendons ( arrows ) under metatarsal heads patients for each patient , we performed as part of the general assessment for metatarsalgia : detailed anamnestic evaluation , focusing on pain features suggestive of neuropathic pain ( sudden pangs and feelings of burning or electric shock radiating to the corresponding toes ) and nociceptive pain ( dull pain , non - radiated or proximally radiating , referred to the plantar or dorsal side of the metatarsal heads ) , its duration and potential triggers in everyday activities . clinical examination , with evaluation of the pain site , palpation of neuroma , pain evocation with mulders maneuver and other clinical signs suggesting forefoot comorbidities ( hallux valgus , hammer toe , metatarsophalangeal joint capsulitis and bursitis )  . dynamic foot ultrasound with focus on the intermetatarsal spaces . 1 3 600 radiol med ( 2016 ) 121 : 597604 fig . 
3 puncture of the neuroma under sonographic guidance : live ( a ) and sonographic ( b ) view that shows the needle ( long arrows ) inside the neuroma ( short arrows ) pain intensity during paroxysm using a numeric rating scale ( nrs : 010 pts ) [ 34 ] , pain features ( neuropathic / nociceptive pain ) [ 9 ] , limitation in everyday activities ( score 03 pts ) [ 35 ] , presence of comorbidities and the occurrence of peri - procedural complications . patients were followed up for 1524 months after the last session of treatment and were interviewed about their pain intensity , pain features , limitation in everyday activities and on the need for rescue therapy with neurectomy . data analysis a reduction in nrs pain score 50 % [ 35 ] or a complete disappearance of the neuropathic component of pain was assumed as a satisfactory response to treatment . for normality assumptions , the shapirowilk test was performed on quantitative and ordinal variables . 
thirty - four ( 11.8 % ) patients were excluded : 4 patients for synchronous non - forefoot overload - related conditions ( 2 with giant cell tumor of the tendon sheath , 2 with rheumatoid arthritis ) , 8 patients for multiple symptomatic neuromas in the same foot , 15 patients for single symptomatic neuromas in both feet , and 7 patients for incomplete dataset . 
black line and box median , first and third quartile ; whiskers : highest and lowest case within 1.5 iqr ; circles outliers 1 3 radiol med ( 2016 ) 121 : 597604 602 fig . 
only data from the first cycle were considered for statistical analysis . none of the variables evaluated in the backward stepwise regression analysis ( patient age , sex , pain at onset , number of years from onset , neuroma size , location , limitation of activity at presentation , nociceptive pain at presentation ) were found to be predictive of clinical response . discussion although the management of cms due to mn currently lacks structured guidelines , most authors suggest a stepwise approach [ 19 ]  . according to a previous systematic review of the literature [ 36 ] , first line of therapy with foot orthotics , in particular metatarsal pads , seldom relieves pain and frequently shows a rapid recurrence of symptoms . historically , surgical treatment with excision of the mass or decompression of the intermetatarsal space was the option of choice , associated with a considerable success rate ( 8096 % ) [ 36 ]  . 
however , it has high costs and a considerable risk of post - operative complications such as wound infection , hypersensitive scars or keloids in up to 23 % cases [ 3 ]  . in the last decades , several mini - invasive treatments had been attempted , aiming at a safer profile while allowing rescue therapy with surgery and could then possibly be considered as an intermediate therapy before surgery . 
 among the most studied ones , steroid injection yields a variable short - term satisfaction rate ( 2282 % ) [ 19 , 22 ] , but has a high relapse rate and could result in skin and soft tissue alterations . 
radiofrequency ablation seems a promising novel technique , but its use is possibly limited by its costs and low availability [ 3032 ]  . percutaneous alcohol injection has been first proposed by dockery in 1999 to achieve chemical neurolysis of the 1 3 radiol med ( 2016 ) 121 : 597604 affected nerve [ 25 ]  . 
the different studies analyzing neuroma alcoholization demonstrated a high sample variability with regard to either patient numerosity ( 8101 patients ) or selection criteria [ 2429 ]  . we observed a success rate similar to previous groups ( 6094 % ) , with the notable exception of a 22 % success rate in one small study [ 2429 ]  . 
even though the most recent ones adopted a standardized pain scale ( either vas or nrs ) , there is still no consensus on the definition of treatment responder . while neuropathic pain has been explicitly or implicitly described as a typical feature of cms by previous groups , it is a novelty to assess for the presence of both subtypes of pain ( neuropathic and nociceptive ) and to integrate it in the outcome . 
our view is that this distinction could aid the clinician in the evaluation of a pain syndrome associated with forefoot overload pathology and in placing the patient in the correct perspective . 
an improvement of neuropathic symptoms is to be expected in most patients , instead nociceptive pain , commonly found in cms patients , is not modified by treatment as it probably reflects occult or overt comorbid conditions , which are found in up to 1 / 3 of patients with an unsatisfactory response . on the functional outcome level , a previously described scale [ 35 ] was adopted to further characterize patients outcome . 
a substantial improvement in everyday activities was observed , suggesting a clinically significant result for the patient . a positive response to treatment should not be excluded based on the clinical and demographic variables evaluable at presentation , as none of them was found to predict the outcome . 
 in our clinic , a higher alcohol concentration was chosen to minimize the relapse rate ( 5 % after 18 months using a 30 % alcoholic concentration : personal data ) , with no major adverse events observed at follow - up . 
in accordance with most previous studies , we prefer a us - guided approach , as it allows a more precise identification of the neurovascular bundle . as a retrospective study , there is no control group against which to ascertain the efficacy of the treatment ; still it has to be considered that cms is a chronic and non - remitting disease and that post - treatment hypo / anesthesia could be a surrogate sign of actual induced nerve impairment . 
a 19 months follow - up is a longer period than in most previous case series , but we could possibly have missed late relapses ; this issue has recently been raised in a 5 - year study [ 29 ]  . conclusions our results show that us - guided alcoholization is a safe , effective and relatively inexpensive technique , advisable for most patients ; it does not preclude surgical treatment and it is our point of view that it can be recommended as first - line therapy for mn treatment in case of failure of conservative measures , leaving the surgical option for resistant cases . 
failure to achieve a clinical response should prompt a thorough patient evaluation for forefoot comorbidities , as they may act as confounding factors in mn diagnosis and at follow - up . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards all procedures performed were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments . 
data on patients characteristics , treatment response and follow - up were collected and analyzed . results a total of 142 cycles of transcatheter arterial chemical infusion were administered to the 40 patients ( 3.55 cycles per case )  . 
in 21 patients , only the bronchial artery was the tumor feeding artery , while in the remaining 19 patients , other arteries in addition to the bronchial artery served as the tumor feeding arteries . 
however , many patients cannot tolerate the intensive therapy due to elder age or poor eastern cooperative oncology group ( ecog ) performance status ( ps ) [ 46 ]  . 
in this study , we aim to evaluate the long - term outcome of tai in treating advanced nsclc and predict the risk factors of influencing overall survival . materials and methods this is a single - center study . 
each patient received the detailed information of tai , and provided the written informed consent . 1 3 606 radiol med ( 2016 ) 121 : 605610 patient selection and study design from may 2008 to august 2014 , a total of 40 consecutive patients with advanced nsclc ( tumor stage iiia ) who underwent tai were enrolled in this retrospective study . 
 the inclusion criteria were as follows : ( 1 ) a definite pathologic diagnosis of advanced nsclc , and ( 2 ) contraindications of venous chemotherapy and radiation therapy , or unwilling to be treated with venous chemotherapy or radiation therapy . 
the exclusion criteria were as follows : ( 1 ) simultaneous treatment of venous chemotherapy , radiation therapy , and / or surgery , and ( 2 ) significant dysfunction of blood coagulation , active infection , and / or active bleeding . 
 data on patients characteristics , treatment response and follow - up were collected and analyzed . diagnosis diagnosis of nsclc was established based on the results of thoracic computed tomography ( ct ) and pathology . 
all patients also underwent brain and abdominal ct or positron emission tomography - ct before treatment to confirm whether or not the distant metastases were present . arteries , and internal thoracic arteries to localize the tumor feeding arteries . 
then we smoothly injected the mixture of 35 ml of lipiodol and 35 mg of doxorubicin to embolize the tumor feeding arteries when the microcatheter was successfully sent to the distal side of the tumor feeding arteries , and no embolization was performed when we could not achieve this . tai was performed for at least four cycles ( once every 46 weeks ) or until disease progressed or toxicity became intolerable . 
dose modification following the first chemotherapy procedure was based on nonhematologic and hematologic toxicity [ 4 ] ( table 1 )  . tai procedure assessment tai was performed under fluoroscopic guidance by three interventional radiologists . 
a 5f cobra catheter ( cordis , warren , nj , usa ) was successively sent to the bilateral bronchial arteries , intercostal arteries , inferior phrenic the tumor staining grade was evaluated for each patient . 
 tumor staining was graded on a scale of i to iv , which represents the ratio ( % ) of the tumor stained area on tumor feeding artery angiography to the entire lesion fig . 
thoracic ct was performed 1 month after each cycle of tai , and then every 23 months after the last cycle of tai to confirm the treatment response and ttp . 
all statistical calculations were performed using spss 16.0 ( spss , inc . , chicago , il , usa )  . the baseline data of the 40 patients are demonstrated in table 2 . 
no patient underwent surgical resection or venous chemotherapy before tai . baseline data of tai procedure a total of 142 cycles of tai were performed for these 40 patients ( 3.55 cycles per case )  . 
eight patients declined further treatment after one cycle ( n 6 ) or 2 cycles ( n 5 ) or deteriorated status ( n 2 ) of tai because of economic reason ( n 3 )  . for these 40 patients , 72 bronchial arteries and 32 nonbronchial arteries were identified as the tumor feeding arteries . 
twenty - one patients were shown to have the bronchial artery only as the tumor feeding artery while 19 patients were shown to have other arteries in addition to bronchial artery as the tumor feeding arteries . 
among the 19 patients , 18 patients had 13 intercostal arteries as the additional tumor feeding arteries , while one patient had one internal thoracic artery and 1 intercostal artery as the additional tumor feeding arteries . 
these data are also and 13.1 comparable with those of previous studies regarding the use of tai for treating advanced nsclc [ 46 ]  . although surgical resection is still the best treatment for nsclc , most patients were diagnosed at the advanced stage and were not candidates for surgical treatment [ 10 12 ]  . 
in addition , tai can be effective in the treatment of cancer of the lung hilum and lymph [ 13 ]  . percutaneous lung ablation has also been used in the treatment of lung tumors [ 1416 ]  . 
however , the incidence of pneumothorax after lung ablation was reported at 3839 % [ 1416 ]  . from the univariate and multivariate analyses , we found that more tumor feeding arteries in addition to the bronchial artery was an independent predictor of decreasing ttp and overall survival . 
therefore , tumor feeding arteries in addition to the bronchial artery may be associated with a shorter ttp and overall survival in the current study . 1 3 610 radiol med ( 2016 ) 121 : 605610 in the current study , although the tumor stage was not associated with the overall survival , airway , esophagus , or svc involvement was another independent predictor of decreasing overall survival . 
involvement of the airway , esophagus , or svc is not only essential in tumor stage evaluation , but can also cause dyspnea , dysphagia , or svc syndrome [ 1820 ]  . 
third , tai has a limited effect on the prevention of distant metastases . in conclusion , although further clinical trials are needed , our results indicate that tai can be used as an easy and effective method to manage patients with advanced nsclc who have contraindications for venous chemotherapy and radiation therapy , or do not want to undergo venous chemotherapy and radiation therapy . 
tai can also provide a favorable long - term outcome . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
zambrini2 gianfranco chiari1 ilaria montermini1 carmelinda manna1 tito poli3 davide lanfranco3 enrico sesenna3 elena thai4 nicola sverzellati1 received : 8 april 2016 / accepted : 23 may 2016 / published online : 4 june 2016 italian society of medical radiology 2016 abstract purpose to compare diagnostic performance between computed tomography ( ct ) and magnetic resonance imaging ( mri ) for the detection of bone infiltration from oral cancer , and to test interobserver agreement between radiologists with different expertises . materials and methods pre - surgical ct and mri were reviewed independently by two radiologists with different expertises in head and neck oncology . 
receiving operator curve was calculated and area under the curve ( auc ) was compared between ct , mri , and both methods together . results interobserver agreement was moderate : the trainee under - reported periosteal reaction on ct and inferior alveolar canal involvement on mri . 
imaging findings associated with histologic evidence of bone infiltration were : periosteal reaction and cortical erosion on ct ; bone marrow involvement , contrast enhancement within bone ; and * mario silva mario.silva@unipr.it 1 sezione di radiologia , dipartimento di scienze chirurgiche , universit degli studi di parma , parma , italy 2 sezione di radiologia , dipartimento di diagnostica per immagini e medicina di laboratorio , irccs arcispedale s . 
in mri positive cases , diagnostic integration with combined review of ct and mri is suggested for optimal diagnostic performance . keywords oral cancer bone infiltration computed tomography magnetic resonance imaging diagnostic performance interobserver agreement introduction the prevalence of mandibular bone invasion ranges from 12 to 56 % in head and neck tumors [ 1 , 2 ]  . 
the diagnosis of mandibular invasion has paramount importance for the pre - operative planning , because the surgical treatment is selected accordingly , with relevant influence on radical treatment as well as quality of life ( from periosteal stripping to mandibulectomy ) [ 36 ]  . 
therefore , the best accuracy of imaging technique or algorithm is needed to tailor surgical approach with optimal balance between radical treatment and anatomical conservation . magnetic resonance imaging ( mri ) and computed tomography ( ct ) are the imaging techniques with the best accuracy for the description of local neoplastic invasion . 
conversely , there is debate about the optimal diagnostic accuracy for the detection of bone invasion , because mri has high sensitivity but low specificity compared to ct [ 9 ]  . 
to date , there is no definite indication to one or the other technique ; indeed , diagnostic protocols reported in the literature are extremely heterogeneous [ 2 , 911 ]  . the principal aim of this study was to compare diagnostic performance between ct and mri for the detection of bone infiltration , with histology as reference standard . 
second , we sought to test interobserver agreement between radiologists with different expertises and to describe its clinical relevance . materials and methods study population the local institutional review board approved this study ; informed consent was waived for retrospective review of data . 
subjects who undergone surgery for oral cancer between november 2008 to april 2014 were retrieved from the local archive of the section of maxillofacial surgery of the university hospital of parma . 
inclusion criteria were as follows : ( a ) availability of both volumetric computed tomography ( ct ) with iodinated contrast agent and magnetic resonance ( mr ) with paramagnetic contrast agent within 4 weeks from surgery and ( b ) pathological assessment of bone infiltration . 
exclusion criteria were as follows : ( a ) heavy beam hardening artifacts on ct with nondiagnostic image quality and ( b ) motion artifacts on ct or mri with non - diagnostic image quality . 
ct protocol included scans without contrast agent and 90 s after injection of 90 ml iodinated contrast agent iomeprol at a concentration of 400 mg iodine / ml ( iomeron 400 , bracco , italy ) , followed by 40 ml saline chaser ; injection rate was 1.5 ml / s by double - syringe electronic injector ( medrad stellant , bayer ag , germany )  . 
acquisition protocol was as follows : ( 1 ) 3 - plane survey ; ( 2 ) pre - contrast t1 - weighted spin - echo images ( tr 564 ms te 1o ms ) on axial and coronal plane ; ( 3 ) t2 - weighted spin - echo images ( tr 4431 ms te 80 ms ) on axial plane ; ( 4 ) short - tau inversion - recovery ( stir ) sequences t2 - weighted images ( tr 2280 ms te 55 ms ) on axial and sagittal plane ; and ( 5 ) post - contrast t1 weighted spin - echo images ( tr 597 ms te 10 ms ) with fat saturation ( spir ) on axial , coronal , and sagittal plane . 
scan volume was set from skull base to the origin of supra - aortic vessels ; slice thickness varied 35 mvisual assessment of images was performed during exam acquisition for quality assessment . 
in the case of low quality image , clinically relevant sequences were repeated up to three times to achieve diagnostic quality . image scoring all images were independently reviewed by one radiologist with 18 - year expertise in head and neck oncologic imaging ( gc ) and a trainee in radiology with specific experience in head and neck imaging ( eiz , 3 years of training )  . 
ct and mri were visually evaluated 4 weeks apart with the aim of describing bone infiltration by each imaging method , as follows . ctpost - contrast images were reviewed according to a scoring system adapted from lenz et al . 
 [ 12 ] : ( a ) periosteal reaction , described as focal thickening of bone surface ; ( b ) cortical erosion , described as focal tapering or complete interruption of cortical bone adjacent to the primary tumor ; ( c ) abnormal attenuation of bone marrow , described as reduction or absence of trabecular bony structure and / or focal obvious contrast enhancement within spongy bone [ 13 ] ; and ( d ) pathological fractures , described as bone fractures without major traumatic event . mrthe images were reviewed according to a scoring system adapted from imaizumi et al . 
 [ 14 ] , as follows : ( a ) mandibular cortical invasion on t1 - weighted images , defined as loss of hypointense signal of the cortical bone adjacent to the tumor mass ; ( b ) bone marrow involvement , hyperintense t2 - weighted signal in bone marrow contiguous to the primary tumor ; ( c ) contrast enhancement within bone , evaluated on t1 - weighted images and in relation to tumor - bone contiguity ; and ( d ) inferior alveolar canal involvement , bone 1 3 706 radiol med ( 2016 ) 121 : 704710 marrow involvement reaching the inferior alveolar canal with contrast enhancement of the nerve on t1 - weighted images . a third radiologist with 10 - year expertise in head and neck oncologic imaging ( im ) reviewed ct and mr simultaneously according to the aforementioned scoring system , with the aim of describing bone infiltration by the combination of the two different imaging methods . imaging finding periosteal reaction cortical erosion table 1 interobserver agreement by cohens k test pathologic reference pre - surgical biopsies and surgical specimens were evaluated by a pathologist with 5 - year experience ( et )  . 
all specimens were rated according to a binary score for the presence of bone infiltration and used as reference standard for the assessment of diagnostic accuracy of imaging descriptors . statistical analysis the radiologic scores were compared between the experienced radiologist and trainee in radiology by cohen test to assess the differences related to expertise in reading bone infiltration by ct or mri . 
 cumulative scores were created , including all ct findings ( scorect ) , mri findings ( scoremri ) , and by combined ct and mri findings ( scorecomb ) , to grant a simulation of different clinical scenarios , as the actual practice is based on heterogeneous imaging protocols , namely : ( a ) ct only for pre - surgical staging ; ( b ) mri only for pre - surgical staging ; and ( c ) combined ct and mri for pre - surgical staging . 
the fishers exact test or the chi - squared test was used as appropriate to assess association between the histological evidence of bone infiltration : ( a ) each consensus imaging finding and ( b ) cumulative number of imaging findings . 
furthermore , sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) , and accuracy were calculated according to histological reference for each consensus imaging finding and for the three scores . 
statistical analysis was performed by medcalc ( version 15.8 , ostend , belgium )  . results interobserver agreement seventy - seven patients underwent both ct and mri with overall moderate agreement between the two readers . 
mri findings associated with histologic evidence of bone infiltration were : bone marrow involvement , contrast enhancement within bone , and inferior alveolar canal involvement . the highest sensitivity was observed for signs of cortical invasion on both ct and mri ( e.g. , cortical erosion on ct and mandibular cortical invasion on t1 - weighted mri images )  . 
this sign could be referred to as in the case of positive mri , because the high npv of periosteal reaction could improve diagnostic accuracy of the majority of mri findings , which are characterized by low ppv ( table 3 )  . 
pathological fractures on ct showed perfect specificity ( 1.00 ) , but extremely low sensitivity ( 0.05 ) , which makes this sign not suitable for accurate pre - surgical assessment . there was association between histological evidence of bone infiltration and the cumulative number of positive imaging findings in both ct and mri ( table 4 ) , suggesting that the presence of more than one finding increased the likelihood of actual bone infiltration . sensitivity , specificity , ppv , npv , and diagnostic accuracy of scorect , scoremri , and scorecomb , the three scores , are reported in table 5 . 
the comparison between different techniques showed the complementary value of ct and mri , namely , suggesting that ct could play a role in the case of positive finding at mri , especially when ct and mri images are read simultaneously . in the literature , the diagnostic accuracy of ct and mri for the detection of mandibular invasion varies between different researchers ( table 6 ) [ 4 , 8 , 11 , 1421 ]  . 
this observation is in line with the technical basis of this imaging method : ( a ) good contrast resolution for high - density structures and ( b ) spatial resolution up to 0.6 m indeed , the high density of normal mandibular bone is an intrinsic ct feature that allows confident detection of pathological infiltration by soft tissue ( e.g. , focal low - density notch on cortical bone )  . 
diffusion - weighted imaging was negative in all mris and , in particular , 22 / 29 ( 76 % ) lesions were 3 mm2 / s , hyperintense but showing adc values > 1.4 while the remaining 7 / 29 ( 24 % ) lesions were hypointense . 
in four cases , linear non - mass - like enhancement was detected at the periphery of surgical cavity ; these patients were addressed to a short - term follow - up , and the subsequent examinations showed the resolution of these findings . 10 * michela giuliani micgiuli@yahoo.it 1 department of radiology , catholic university of the sacred heart , largo agostino gemelli 8 , rome , italy 2 department of general surgery , catholic university of the sacred heart , largo agostino gemelli 8 , rome , italy 3 largo francesco vito 1 , 00168 rome , italy conclusion when applied to surgical residual cavity , orc can lead alterations in surgical scar . 
this could induce radiologists to misinterpret ultrasonographic and mammographic findings , addressing patients to mri or biopsy ; so knowledge of mri specific features of orc , it is essential to avoid misdiagnosis of recurrence . keywords magnetic resonance imaging oxidized regenerated cellulose absorbable implants breastconserving surgery oncoplastic procedures introduction breast - conserving surgery ( bcs ) combined with post - operative radiotherapy is considered the procedure of choice for women who are affected by early stage tumors [ 1 ]  . 
the aim of bcs is to ensure complete removal of breast cancer preserving the shape , appearance , and natural symmetry of mammary glands , offering the same survival rate as compared to mastectomy [ 24 ]  . oncoplastic surgery represents a major advance in bcs . 
the purpose of this technique is combining principles of surgical oncology with those of reconstructive surgery , allowing a more radical local tumor excision , which potentially reduces margins involvement and local recurrence , while achieving an acceptable cosmetic result [ 5 , 6 ]  . 
1 after complete tumor excision , adequate reshaping of the gland is performed by dissecting the residual breast parenchyma from the pectoralis major fascia and then from the superficial subcutaneous tissue . 
with this dissection , two opponent superficial advancement flaps ( i.e. , skin and subcutis ) and two opponent deep advancement flaps ( i.e. , breast parenchyma ) are obtained ( a )  . 
this sterile , bio - absorbable material , swells into a gelatinous brown - black mass when applied into the surgical cavity , allowing local control of bleeding and reducing the risk of post - operative infections [ 9 , 10 ]  . 
in this regard , in a previous study , ultrasonographic ( us ) and mammographic ( mx ) features of orc were extensively analysed , underlining peculiar properties of this material and related mammary and scar changes , to correctly interpret them [ 21 ]  . 
there are some studies describing mri appearance of orc in intra - abdominal or retroperitoneal surgery , while its appearance in breast surgery has not been investigated yet [ 20 , 22 , 23 ]  . thus , the purpose of this study is to describe specific mri features of orc when used in breast - conserving surgery . 
in fact , orc implantation into the surgical cavity is not , in itself , an indication to perform breast mri during follow - up . all patients underwent post - operative mri examination between 1 and 2 years after surgery ( mean time 2 months )  . breast mri technique mri was performed using a 1.5t scanner with 23mt / m gradient intensity ( signa excite ; ge medical system , 1 3 690 radiol med ( 2016 ) 121 : 688695 milwaukee , wi , usa )  . 
following patients informed consent and exclusion of contraindications , patients were transferred into the gantry , placed in prone position , and examined using bilateral breast surface coils . mri protocol was as follows : short tau inversion recovery ( stir ) axial sequence 68 , 17 , bandwidth 4167 , 4 mm , 0 interval , field3234 cm , and number of excitation [ repetition time ( tr ) echo train length ( etl ) 480 of - view ( fov ) 12 ]  . ( nex ) 320 matrix , thickness 5900 , echo time ( te ) 5150 , te min , frequency - phase 96 96 , thickness 3234 cm , nex diffusion - weighted imaging ( dwi ) axial sequence 96 , ( tr 4 mm , 0 interval , and matrix 96 fov 6 )  . 
sensitizing diffusion gradients were applied sequentially in the x - , y - , and z - directions with b values of 0 and 1000 s / mm2 . 15 , tr < 30 ms , te < 5 ms , nex 23 mm , 0 interval , 320 three - dimensional ( 3d ) fast spoiled gradient echo ( fspgr ) fat saturation ( fat sat ) coronal sequence ( flip angle ( fa ) 0.5 , thickness 320 matrix , and 3438 cm ) before and five times after intravefov nous administration of 0.1 mmol / kg of gadopentetate dimeglumine ( gd - dtpa )  . 
contrast medium was injected with 10 s of timing delay into the antecubital vein with a 1820 g needle at a flow rate of 2 ml / s followed by a flush of 20 ml of saline solution . 3d fspgr sagittal post - contrast sequence ( tr < 30 , 288 matrix , thick2226 cm , and 15 , 288 23 mm , 0 interval , fov 2 )  . te < 5 , fa ness nex 3d fspgr axial post - contrast sequence ( tr < 30 , te < 5 , 23 mm , 0 30 , 512 interval , fov 256 matrix , thickness 2 )  . 3438 cm , and nex acquisition time of this complete mri protocol was 1820 min . dynamic images were transferred to a workstation ( advantage windows 4.1 ) and post - processed . 
subtracted images , maximum intensity projection ( mip ) , and multiplanar reconstruction ( mpr ) functions were obtained and studied in cine loop . all post - contrast images were subtracted , and resulting images of second post - contrast sequences were used for measurements . with a post - processing software that showed signal intensity changes in a given point of space in time ( functool program ) , dynamic time / intensity curves were obtained after placing a region of interest ( roi )  . image analysis two radiologists with more than 5 - years experience in breast imaging reviewed in consensus all breast mris . mri images were examined for the evidence or absence of signal abnormalities and mass - like or non - mass - like enhancement , according to the american college of radiology breast imaging reporting and data system mri criteria [ 25 ]  . 
time / signal intensity curves patterns obtained from dynamic contrast - enhanced images and apparent diffusion coefficient ( adc ) values on adc maps obtained from dwi images were also evaluated . mri was considered negative in the absence of areas of suspicious enhancement or signal abnormalities . rois were placed on areas with the highest visual enhancement on post - contrast images , to obtain timesignal intensity curves ; patterns of enhancement were classified as persistent , plateau , and washout , according to the breast imaging reporting and data system mri guidelines [ 24 ]  . adc values were obtained placing two rois within a given lesion corresponding to the same area of enhancement in post - contrast images in which an roi was placed for kinetic analysis ; thereafter , the average adc of the two rois was obtained . 
the size of rois was never smaller than 40 mm2 and typically ranged from 40 to 60 mm2 . dwi was considered positive when adc < 0.0014 mm2 / s , negative when adc > 0.0014 mm2 / s or in the absence of areas of hyperintensity [ 25 ]  . results in 22 / 51 ( 43 % ) mris , no significant alterations were detected . 
dwi was negative in all of the examined mri , and , in particular , 22 / 29 ( 76 % ) lesions were hyperintense but showing adc val3 mm2 / s , while the remaining 7 / 29 ( 24 % ) ues > 1.4 10 lesions were hypointense . 1 3 691 radiol med ( 2016 ) 121 : 688695 fig . 
2 stir axial images show a hyperintense collection with an internal oval , hypointense nodule representing orc ( a ) not enhancing in 3d - fspgr axial post - contrast fat - suppressed sequence ( b ) in the left breast . 
this lesion ( pattern 1 ) shows rim enhancement on t1w axial and sagittal images obtained in the late phase of the dynamic study ( b , c )  . 
this pattern perfectly matches to us imaging that shows a wellencapsulated hypo - isoechoic lesion with circumscribed margins and internal hyperechoic nodule ( d ) that we named ile flottante fig . 
3 stir axial images show a completely hyperintense collection without solid internal nodules ( pattern 2 ) ( a ) , with a rim enhancement in 3d - fspgr axial and sagittal post - contrast fat - suppressed sequences ( b , c ) in the left breast . 
when applied in surgical residual cavity , orc gradually reabsorbs and it is first bounded by granulation tissue , and is further enclosed with fibroblastic tissue later [ 26 , 1 3 radiol med ( 2016 ) 121 : 688695 692 fig . 
4 stir axial images show a completely hypointense lesion ( pattern 3 ) ( a , b ) with rim enhancement in 3d - fspgr sagittal post - contrast fatsuppressed sequence ( c ) in the right breast . 
3d - fspgr sagittal post - contrast fat - suppressed images depict multiple foci of enhancement at the upper margin of surgical collection and non - mass enhancement with linear distribution in the lower posterior margin ( b ) which may suggest residual pathological tissue . 
the kinetic curve measured in the area of enhancement shows a pattern of progressive - persistent enhancement ( type 1 ) and this finding supports the hypothesis of benign post - surgical changes instead of a residual - recurrent disease ( c ) 27 ]  . 
this process results in specific imaging patterns that could be misinterpreted as tumor recurrence at follow - up radiological examinations [ 2830 ]  . in a previous study , us and mx specific features of orc were analysed , and the importance for radiologists to be aware about these peculiar properties was underlined , to understand the corresponding mammary and scar changes and correctly interpret them [ 21 ]  . 
nevertheless , sometimes mx or us findings were considered equivocal , and patients were consequently addressed to mri in the suspicion of recurrence . there are few studies describing mri appearance of orc only concerning with intra - abdominal or 1 3 radiol med ( 2016 ) 121 : 688695 fig . 
6 in this patient , 3d - fspgr axial post - contrast fat - suppressed sequences reveal irregular enhancement at the periphery of surgical collection ( ac ) which may suggest residual pathological tissue . 
 the early follow - up mri examination shows no areas of abnormal enhancement at the periphery of the lesion ( df ) confirming that the previously described abnormalities were due to inflammatory changes related to orc implantation retroperitoneal surgery , reporting conflicting data regarding specific features of this material in different mri sequences [ 20 , 23 ] , probably related to the different surgical procedures . in our series , orc shows marked hypointensity and well - defined margins on t2w images , which are most sensitive in the detection of this material , as demonstrated by oto et al . 
 this pattern is similar to the one already described at us imaging , characterized by the presence of hyper - isoechoic nodules within complex cystic mass and named ile flottante [ 21 ]  . it is also possible to find completely hypointense lesions . 
 in our experience , this pattern is most frequent during the early post - operative phase , and it is referrable to the signal of the clot that has caused saturation and swelling of orc fibers , as already proposed by oto et al . 
 [ 20 ] ; this finding is similar to hypo - anechoic lesions already described at us imaging [ 21 ]  . at last , completely hyperintense collections on stir / t2w images are due to partial reabsorption of orc , which is no longer visible , with persistence of residual surrounding fluid . 
this pattern corresponds to completely anechoic collections with thick walls at us imaging without internal hyperechoic nodules [ 21 ]  . in all our series , the lesions showed rim enhancement on late phase of t1w post - contrast images and the kinetic curve pattern was progressive persistent ( type 1 ) , indicative of benignity [ 24 ]  . 
these findings are probably indicative of 1 3 694 radiol med ( 2016 ) 121 : 688695 10 the compression exerted by orc on surrounding tissues or of granulation tissue around the surgical site and have to be interpreted as benign post - surgical changes , according to the subsequent negative follow - up ( both us - mx and mri examinations )  . 
besides that , since our study was retrospective , not all the patients who underwent bcs with orc implantation were addressed to mri ; furthermore , because mri is a second - level technique in followup of breast cancer , it has been performed only in the cases , where first - level techniques ( us and mx ) showed suspicious abnormalities ; therefore , mri was not carried out when us and mx findings were normal . 
moreover , mri was not performed at the same timing after bcs in all patients , so we could not correlate different imaging patterns with changes of orc over time . 
limitations in the analysis of temporal changes induced in breast tissues by the use of orc also depended on the small number of patients who underwent more than one mri examination and on the short - time interval of available follow - up examination . 
at last , since our institution is a referral centre for breast cancer diagnosis and treatment , all examinations were evaluated by breast radiologists yet experienced in recognizing breast changes induced by the use of orc ; therefore , it could be expected that our number of patients addressed to short - term follow - up might be smaller than in other centres , and this could be a bias in our series . in conclusion , when applied to the surgical residual cavity , orc helps in controlling of local haemorrhage and to reduce the risk of post - operative infections , but it could lead to alterations in surgical scar . 
this could induce radiologists who are not aware of particular properties of this material to misinterpret us and mx findings as tumor recurrence , addressing patients to mri or biopsy . thus , the knowledge of specific mri features of orc , for which there are not currently reports in the literature , it is essential for breast radiologists to correctly interpret them and to avoid misdiagnosis of tumor recurrence with the subsequent unnecessary procedures . compliance with ethical standards conflict of interest michela giuliani declares that she has no conflict of interest . 
the current study aimed to provide a valid comparison of tttg distance in the healthy knees with those with patellar instability . materials and methods patients with a history of two or more episodes of patellar dislocation in the same knee who were referred to our department for the assessment of tttg distance were included . 
box : 14117 - 18541 , tehran , iran could still be considered as an indicator of knee instability and even the need for surgery if considered in addition to other factors . keywords knee patellar dislocation tomography , x - ray computed tibial tuberositytrochlear groove distance introduction patellar dislocation is a very painful and disabling condition commonly caused by either direct trauma to the patellar joint or sudden rotation of the leg . 
its prevalence is reported to be about 5.8 per 100 , 000 normal populations [ 1 ] , which can be as high as 2943 per 100 , 000 normal populations aged 1017 years [ 1 , 2 ]  . 
while the chance of patellar dislocation recurrences is 544 % after the first event , it will increase to at least 50 % after the second episode of patellar dislocation [ 1 , 3 ]  . 
moreover , it has been estimated that even after the first episode of patellar dislocation , more than half of these patients suffer from activity limitations at least up to 6 months after patellar dislocation and around the same number will not be able to successfully perform the same physical activities they would have performed before this event [ 4 ]  . 
it is well known that recurrent patellar dislocations result in patellofemoral joint damage , chronic knee pain , work disability and impaired quality of life [ 1 ]  . morphological abnormalities of patellofemoral joint result in patellar instability predisposing it to recurrent dislocations . 
an increase in tttg distance in patients with patellar instability has 1 3 730 radiol med ( 2016 ) 121 : 729734 been reported by many authors [ 5 , 7 , 8 ]  . 
nonetheless , during the past decade , the reliability and validity of tttg distance as a measure of patellar instability have become a matter of controversy [ 10 , 11 ]  . 
furthermore , some studies , albeit with serious concerns regarding their reliability and validity , have shown a significant negative correlation between tttg distance and quadriceps angle which is another indicator of patellar instability [ 9 ]  . 
 [ 12 ] compared tttg distance of symptomatic and asymptomatic knees of the same patients , the current study is the first to compare the tttg distance of symptomatic knees of the patients with unilateral patellar instability in comparison to both their own asymptomatic knees as well as knees of healthy individuals with no past or present history of complaints in patellar joint problems . 
 [ 13 ] and provide a valid comparison of tttg distance in healthy knees with those with patellar instability . materials and methods study design the current observational casecontrol study was performed between june 2014 and june 2015 . 
patients with a history of two or more episodes of patellar dislocation in the same knee who were referred to our department for the assessment of tttg distance were prospectively included . 
it should be noted that every two patients were matched to one control , equal to every symptomatic knee to one asymptomatic ( control ) knee . ethical considerations the ethics committee of our university reviewed and approved the process of the study and ruled out the need of obtaining signed informed consents from patients with unilateral patellar instability . 
the process and aim of the study were explained in detail to all healthy controls who volunteered for enrollment in the study and they were asked to sign an informed consent . 
a minimum number of the controls were included to prevent unnecessary radiation exposure of healthy individuals . radiological evaluations upon visiting the radiology department at our hospital , thorough medical history taking and physical examination were performed for all patients . 
 to evaluate tttg distance , long leg scans on both sides were performed by computed tomography ( ct ) scan in all study subjects ( brightspeed elite ct scanner , ge healthcare , uk )  . 
 using the tagt command of the aw volumeshare 2 software ( ge healthcare , united kingdom ) , a first line was horizontally drawn connecting the posterior borders of the femoral condyles . 
thirty records , ten from patients symptomatic knees , ten from patients asymptomatic knees and ten from controls which were selected randomly were also evaluated in a blind fashion by another 1 3 radiol med ( 2016 ) 121 : 729734 fig . 
figure 2 demonstrates the tttg distance in the three study groups . patients characteristics categorical tttg distance measures out of a total number of 42 patients , 14 ( 33.3 % ) were male and 28 ( 66.7 % ) were female . 
on the contrary , there was a significantly higher number of cases with tttg distances equal to or greater than 20 or 15 mm in both groups of symptomatic and asymptomatic knees of patients compared to controls knees ( p < 0.001 for all tests )  . discussion the main finding of the current study was the lack of a statistically significant difference in the tttg distance between the symptomatic and asymptomatic knees of patients with unilateral patellar instability . 
the other major finding of the current study was a statistically significant lower tttg distance in controls knees compared to either of symptomatic and asymptomatic knees of patients with recurrent unilateral patellar instability . 
the number of patients in the current study sufficed the previously calculated sample size , and the p value of the test performed to compare symptomatic and asymptomatic was much higher than the level of significance . 
it should be noted that tttg is only one of the factors used in decision - making in patients with patellar instability , and surgeons generally consider the whole clinical presentation and preference of the patients [ 16 ]  . 
nonetheless , our findings do not provide statistical evidence supporting an independent role for tttg as a sole predictor of the need for surgery . even though our findings are in line with the results of the study by caplan et al . 
 [ 13 ] could not determine the exact cause of this observed difference , but suggested that their use of a dynamic modality in contrast to the static modality used by caplan et al . 
 [ 12 ] , as well as in the current study , and variability in patient selection could contribute to this finding . in our study population , the mean tttg distances of symptomatic and asymptomatic knees of patients and controls knees were around 19 , 17 and 10 mm , respectively . 
in our study population , 83.3 % of symptomatic and 64.3 % of asymptomatic knees of patients had a tttg distance of equal to or greater than 15 mon the other hand , all controls knees had a tttg distance within the normal ranges . 
here , we found out that 35.7 % of symptomatic and 28.6 % of asymptomatic knees of patients had a tttg distance of equal to or greater than 20 mthis finding indicates that the currently used cutoff point of 20 mm as one of the factors considered in favor of surgical interventions in patients with patellar instability is not accurate enough to be considered as a main factor for decision - making in favor of surgical interventions . 
 [ 12 ] reported a tttg distance of equal to or greater than 20 mm in 30 % of symptomatic and 20 % of asymptomatic knees of patients with unilateral patellar instability . 
 [ 12 ] found a lesser number of asymptomatic knees with a tttg distance of equal to or greater than 20 mm may be explained by the greater mean tttg distance in our study population , which was about 2 mm greater in each one of symptomatic and asymptomatic groups of patients knees than those values reported by caplan et al . 
 [ 5 ] found a tttg distance of equal to or greater than 20 mm in 56 % of symptomatic and 24 % of asymptomatic knees of patients and 3.5 % of controls knees . 
 [ 13 ] has reported a mean tttg distance of 21 mm in asymptomatic knees of patients with patellar instability , but did not comment on the number of cases with a tttg of greater than 20 mon the other hand , this measure in asymptomatic knees was higher in the current study compared to both the study by caplan et al . 
this may in part explain the slight difference in their findings with other studies . the greater tttg distance of asymptomatic knees of patients compared to controls knees may be explained by two observations . 
first , it has been previously shown that 1 3 radiol med ( 2016 ) 121 : 729734 some hereditary traits , developmental factors and personal characteristics such as family history of patellar dislocation , structural abnormalities , female sex and a body mass index of greater than 25 are associated with increased risk of patellar instability [ 2022 ]  . 
if this speculation is true , tttg truly predicts patellar instability , although its accuracy in determining the need for surgical interventions may be in doubt since many asymptomatic knees of such patients exceed the cutoff point of 20 mm . the second observation is provided by previous reports on the follow - up of patients with unilateral patellar instability . 
interestingly , about 30 % of asymptomatic knees in our study population had a tttg of more than 20 mm , which may indicate that these cases are likely to develop signs and symptoms in their asymptomatic knees during the next few years . 
this may indicate that patients with unilateral knee instability may simply favor their symptomatic knee , putting extra pressure on the contralateral knee , or are predisposed to patellar instability in both knees , which may have already happened in one knee due to external pressures such as traumatic incidents , or the affected side is simply the dominant one in that individual . 
it may be concluded that a longer course of disease is likely to result in more similarities in tttg distance of symptomatic and asymptomatic sides of the knee joint in the same patient . 
on the contrary , it is likely that during the first stages of patellar instability , there is a greater difference in tttg of two sides since the contralateral knee joint is less affected . the current study provides a valid comparison of tttg distance in knees with and without recurrent patellar instability . 
first , although much unlikely , it is still possible that the lack of differences of tttg distance between symptomatic and asymptomatic knees of patients with recurrent patellar instability could be due to the relatively small sample size deployed here . 
nevertheless , ct scan is widely used as the standard method for the assessment of tttg distance and any possible bias in the sole usage of ct scan affects all symptomatic and asymptomatic knees alike . in conclusion , since the results of the current study showed similar tttg distance between symptomatic and asymptomatic knees of patients with unilateral instability , the use of this measure as an independent factor in decision - making for surgical interventions is not supported by the currently available body of evidence . 
however , greater tttg in both asymptomatic and symptomatic knees of patients compared to controls indicates that this measure could still be considered as an indicator of knee instability and a predictor of further instability and onset of symptoms in the asymptomatic knees in the next few years . 
the aim of this prospective study was to define the strain index ( si ) and resistivity index ( ri ) values in the same ckd group for each kidney separately at the same time , and also to compare the efficacy of si and ri in the differentiation of normal population and ckd patients . materials and methods toshiba aplio 500 usg device and 3.55 mhz convex probe were used for usg , cdusg , and usg elastography examinations . 
healthy volunteers according to laboratory and clinical examinations were selected from non - kidney disease patients . results a total of 121 ckd ( 68 men , 53 women ) and 40 healthy volunteers ( 19 men , 21 women ) were participated . 
the sensitivity and the specificity of the si were higher than ri . conclusion the ri and si values of kidneys in ckd patients were significantly higher than those of apparently normal kidneys . 
ckd is defined as kidney damage of three or more months duration caused by structural or functional abnormalities with or without a decreased glomerular filtration rate ( gfr ) by the kidney disease outcomes quality initiative ( kdoqi ) guidelines . 
stage 1 indicates kid90 ml / min / 1.73 m2 , stage 2 ney damage with gfr indicates gfr 6089 ml / min / 1.73 m 2 with evidence of kidney damage , stage 3 indicates gfr 3059 ml / min / 1.73 m2 , stage 4 indicates gfr 1529 ml / min / 1.73 m2 , and stage 5 ( end - stage renal failure ) indicates < 15 ml / min / 1.73 m 2 [ 1 ]  . 
parenchymal corruption occurs during the ckd period [ 2 ]  . color doppler ultrasonography ( cdusg ) is a noninvasive real - time pulse - wave method that evaluates blood flow in vascular structures . 
color flow and spectral modes give the operator pulsatility index ( pi ) , resistivity index ( ri ) , flow volume , and the other flow parameters about related vascular structure [ 3 ]  . 
in the measurement of intrarenal arterial resistance , ri is frequently used . elastography is a developing modality , in which working principle is based on tissue elasticity that requires dedicated probe and elastography software [ 6 ]  . 
 strain elastography is operator dependent due to the probe compressions and decompressions , while shear - wave does not need operator compressions by the aid of generating electro - mechanical waves [ 7 , 8 ]  . organ damage affects the ri and si values , which increase in ckd patients [ 2 , 911 ]  . 
there are various studies about ri and si separately , but , to the best of our knowledge , there is no published study comparing ri and si at the same in ckd patients . 
determining cut - off si and ri values between normal and diseased renal parenchyma can help in the diagnosis and follow up of ckd patients . the aim of this study was to define the si and ri values in the same ckd group for each kidney separately at the same time , and also to compare the efficacy of si and ri in the differentiation of normal population and ckd patients . 
 to the best of our knowledge , this is the first study comparing ri and si in ckd patients . material and methods informed consent form was obtained from all patients , and the study was performed in accordance with the ethical guidelines of the helsinki declaration and approved by the local ethics committee . 
demographic data ( age and sex ) , creatinine in urine , and proteinuria ( g / day ) of the patients were recorded in nephrology and endocrinology cliniques , while ri and si values of both right and left kidneys were recorded in radiology clinique . 
there was no significant time interval between the radiologic measurements and blood and urine sampling . the stages of the ckd were recorded , but the statistical analyses were not made by grouping according to ckd stages , because the aim of the study was not about the difference of ri and si among stages . toshiba ( toshiba medical systems , co , ltd , otawara , japan ) aplio 500 us device and 3.55 mhz convex probe were used for usg , cdusg , and usg elastography examinations . 1 3 radiol med ( 2016 ) 121 : 681687 fig . 
the spectral analysis is shown under the color doppler image the sonographic evaluations were made by a six - yearexperienced radiologist who was completely blinded to the clinical information . color doppler usg examination ( cdusg ) usg examinations were performed with the patient lying in supine , right decubitus , and left decubitus positions . 
the distance of the reference roi to the usg transducer effects the strain ratio measurements ; thus , we tried to adjust the reference roi which was in the perirenal fat tissue to the closest position to sampling roi in axial plane to obtain the most optimal measurement . 
si and ri cut - off values were calculated for each kidney and for the left kidmean right and left kidney values [ ( right kidney ney ) / 2 ]  . 
roc curve was made to calculate the cut - off value of si and ri . 1 3 radiol med ( 2016 ) 121 : 681687 continuous variables were expressed as arithmetical standard deviation ; categorical variables were mean expressed as percentages ( % )  . 
in recent studies , the availability of si is researched in the diagnosis and follow - up of ckd , and showed also correlation with ckd [ 11 , 14 , 15 ]  . in our study , the ri and si values in both kidneys of ckd patients were higher than the normal population . 
furthermore , the most important result according to our study was that the sensitivity and the specificity of si were higher than ri . ri is a value related with the blood flow , and shows increment with the ckd stages and renal damage [ 2 ]  . 
reported that the shear - wave velocity of the ckd patients was higher than the normal healthy population in which arfi method was used [ 14 , 15 , 21 ]  . 
in our study , the si values of each kidney were not affected by age or gender , and were higher than those of apparently normal kidneys . to the best of our knowledge , cardiovascular disorders do not affect the si , unlike ri . 
it is revealed that vascular lesions ( arteriosclerosis , systemic vasculitis , ) , antihypertensive drugs ( ace inhibitors , arbs ) age , and systolic blood pressure affect the ri value [ 4 , 5 , 2224 ]  . 
in ckd disease , chronic progression causes fibrosis and fibrosis causes increase in si value [ 11 , 12 , 15 ]  . the major limitations of our study are as follows : there are various etiologic factors of ckd . 
degree of anisotropy , and the level of vascular and urinary pressure may have an impact on shear - wave velocity , and , therefore , on the elasticity values of the kidney tissue ( more particularly the cortex )  . 
there should be more studies about anisotrophy and strain elastography [ 23 ]  . 1 3 radiol med ( 2016 ) 121 : 681687 in conclusion , the ri and si values of kidneys in ckd patients were significantly higher than those of apparently normal kidneys . 
this studys purpose was to check whether there was indeed the added value of neonatal mri performed in the mr - compatible incubator ( inc ) after fetal examination . materials and methods material consists of 25 neonates ( 14 girls ) who underwent prenatal and postnatal mri in a 1.5 t scanner , the latter in inc . 
mean time of prenatal mri was 30th gestational week , of postnatal mri16th day of life . results in 14 cases ( 56 % ) postnatal findings were the same as prenatal ones . 
in 11 ( 44 % ) postnatal mri showed some different / new / more precise results , in two the differences were attributed to other factors than the advantage of postnatal mri over prenatal one . 
altogether then postnatal results were partly discordant with prenatal ones in 9 / 25 cases ( 36 % )  . conclusions in most cases there was no added value of postnatal mri as compared to prenatal one . 
on the other hand , mr examination performed with use of the dedicated neonatal coils in the mr - compatible incubator is a safe and reliable method of visualization of these small details with better spatial resolution * monika bekiesinska - figatowska zaklad.rtg@imid.med.pl 1 department of diagnostic imaging , institute of mother and child , ul . 
although the mothers uterus is a safe incubator for the sick fetus , currently we have a secure equivalent of it for a newborn which is the mr - compatible incubator ( inc ) , offering the safe environment during mri procedure even for unstable neonates [ 4 , 5 ]  . 
thanks to the dedicated neonatal coils built in our inc ( eight - channel phase - array head coil and whole body twelve - channel phase - array coil consisting of two elements : eight - channel part integrated with the incubator bed and four - channel separate surface coil ) we are able to examine not only the neonatal brain but also other organs and systems . to the best of our knowledge there are no papers in the literature comparing the value of prenatal and postnatal mri , with the latter performed in this most up - to date equipment . 
prenatal mri was performed between the gestational ages of 19 and 38 weeks ( mean in the 30th gestational week , gw ) , postnatal mri between day 1 ( day of birth ) and the age of 3 months ( mean in the 16th day of life )  . 
in all cases included , the study was performed with use of a nomag ic 1.5 incubator , equipped with three coils : an eight - channel , phased - array head coil and a twelve channel phased - array coil for the whole body , consisting of an eight - channel coil integrated in the incubator and a separate four - channel surface coil . in postnatal scans , the same sequences were used , and additionally , depending on region of interest ( head or body ) , fluid attenuated inversion recovery ( flair ) and short ti inversion recovery ( stir ) were included in the protocol . 
the parameters used are shown in table 2 . results in 14 cases ( 56 % ) the mri findings obtained after birth were the same as in the prenatal examination ( s )  . 
in the remaining 11 cases ( 44 % ) postnatal mri showed some different or new or more precise results as compared to the fetal one : subependymal heterotopia , callosal hypoplasia , agenesis of the anterior commissure , optic nerves hypoplasia and cranial nerves v , vii , viii emerging together from the brainstem , cleft palate , subcutaneous hemangioma and not the intraosseous one , atretic encephalocele , unicornuate uterus , multiple enhancing nodules as an addition to the enormous cystic tumor in the abdomen and pelvis in a case of blue rubber bleb nevus syndrome ( brbns )  . 
in another baby with clinically evident microcephaly , cerebellar hypoplasia that was diagnosed prenatally was not confirmed as such on postnatal mri which revealed proportionally small cerebrum and cerebellualtogether then the results of postnatal mri were partly discordant with prenatal one in 9 / 25 cases which accounts for 36 % of all the cases . 
besides in two cases there were additional postnatal findings related most likely to perinatal insult , such as subependymal bleeding and ischemic focus in the brathe discrepancies between prenatal and postnatal examinations are shown in table 4 . 
these diagnoses included ventriculomegaly / hydrocephalus , stenosis , rhombencephalosynapsis , cerebellar hypoplasia , callosal aqueductal agenesis / hypoplasia , interhemispheric cyst , pericallosal lipoma , gray matter heterotopia , transsphenoidal encephalocele , face tumor , microphtalmia , cleft lip and palate , neck cyst , chiari ii malformation , ectopic kidney and abdominal cyst . several studies compared the results of prenatal mri with postnatal one . 
in our material there are also studies of other organs and systems : vertebral column and spinal canal in one case , head and neck in three cases , and abdomen and / or pelvis in three , which accounts for 28 % of the study group . 
although congenital abnormalities / damage to cns still remain the main indication in case of neonatal mr examinations , there is a growing role of this method in body imaging . 
the technical progress and development of dedicated neonatal body coils which vendors had started to build in the inc allowed evaluation of other parts of the body and not only the brain which is the only organ that has been described in previous 1 3 722 radiol med ( 2016 ) 121 : 719728 1 3 radiol med ( 2016 ) 121 : 719728 fig . 
enhanced nodules in the right lobe of the liver behind the main mass , in the chest wall on the right side and in the diaphragm on the left studies . 
regardless of which organ or system they relate to , prenatal mr examinations allow early planning of postnatal interventions , speeding up the postnatal diagnostic process and minimizing delay in treatment after delivery . 
although fetal mri has gone far beyond t2 - weighted imaging alone and numerous other sequences are available nowadays [ 10 ] , it still does not have the same diagnostic quality and variety of pulse sequences as are available in the postnatal examination . 
therefore , for example in oncological cases , the clinicians wish to have accurate information about the origin of the tumor , the invasion of adjacent organs , and the presence or absence of metastases after birth . 
we diagnosed this case as a malignant tumor with metastatic spread but we were wrong as these turned to be venous malformations in brbns . 1 3 724 radiol med ( 2016 ) 121 : 719728 fig . 
on the left side cranial nerves v , vii and viii emerge together from the brain steon the right only cranial nerve v is visible in this section tiny structures are in general difficult to see on prenatal mri . 
searching in pubmed for fetus , cranial nerves , mri we have not found any reports concerning fetal mri in vivo . also subependymal gray matter heterotopia belongs to the list of tiny elements that are difficult to appreciate on prenatal mri . 
this is in line with the results of other authors who explain the difficulty in identifying subependymal heterotopia with the fact the nodules have small size and signal intensity similar to the adjacent germinal matrix [ 8 ]  . if the corpus callosum of the fetus is only hypoplastic , the typical mri symptoms indicating its agenesis , such as enlargement of the ventricular atria and the occipital horns ( colpocephaly ) , marked separation of the bodies of the lateral ventricles , laterally positioned frontal horns with concave medial borders , elevation of the third ventricle and radial disposition of the sulci on the internal aspects of the hemispheres , may be absent [ 12 ]  . 
14 and 22 , and we missed the diagnosis of callosal hypoplasia in these fetuses . usually , if we deal with clefts of the primary palate it means cleft lip and alveolus which is diagnosed properly on fetal mri [ 13 ]  . 
also , isolated cleft palate without cleft lip is difficult to diagnose although mri is more helpful in this aspect than sonography in which shadowing from the surrounding facial bones is very disturbing . 
however , mr images are also disturbed by fetal motion between and during image acquisitions [ 14 ] and we also appreciated isolated bilateral cleft palate as late as in postnatal examination . as stated above it is not always easy to find the place of origin of the lesion on prenatal mri . 
one can only state that it does not enhance examination uterus can be identified as a tiny structure between the urine - filled t2 - hyperintense , t1 - hypointense bladder and meconium - filled rectum which is t2 - hypointense and t1 - hyperintense at this gestational age ( 31 weeks )  . 
with the advent of twodimensional fast imaging employing steady - state acquisition ( fiesta / 2d ) technique with parallel imaging , which was also used in this study , prenatal mri achieved temporal resolution at less than half a second and quite high spatial resolution [ 16 ] , however , it is still lower than that of neonatal mri . 
this might be the future for obtaining better images of fetuses with more anatomical and pathological details but for now most of fetal studies are performed on 1.5 t units and we do not see everything . 
fortunately , most of the changes that went unnoticed on prenatal studies in our material had no significant impact on the management of newborn babies at this very moment of their lives . 
however , we do remember that many of these patients are syndromic ones and that the small undetected details cannot be underestimated as far as a final diagnosis is concerned . a limitation of our study is that the sample size is relatively small . 
this limitation could be overcome by performing postnatal mri on all children who undergo fetal one but it would be unethical to sedate a neonate only for research purposes . another limitation is inhomogeneity of the material which consists of both neuroimaging and body imaging . 
 howeverin our opinionbeing a limitation , it is also an advantage sinceas mentioned abovethe collected material reflects the whole spectrum of indications for which both prenatal and postnatal mri is performed at present time . conclusions the obvious advantage of imaging in the mr - compatible incubator is that a baby that has already been born is diagnosed , and not the tiny fetal body in a mothers body , which improves image quality and provides opportunity to visualize tiny elements of anatomy as well as tiny pathological lesions , but still in most of our cases there was no added value of postnatal mri as compared to prenatal one . 
summarizing the data , the most used protocol is characterized by t2 sequences in three orthogonal planes plus t1 sequences in one plane ( either axial or sagittal ) without contrast medium injection . conclusion there is a lack of a standard protocol . 
a tailored protocol to answer the diagnostic question , reducing costs and time of examination , is characterized by t2 sequences in three orthogonal planes plus at least a t1 sequence ( either axial or sagittal plane )  . * andrea alessandro esposito rxandreaesposito@yahoo.it 1 department of radiology , fondazione irccs ca granda ospedale maggiore policlinico hospital , via francesco sforza , 35 , 20121 milan , italy 2 school of radiology , university of milan , via a . 
 sforza , 35 , 20121 milan , italy keywords emergency mri penis fracture tailored protocol urology introduction penile traumas represent 2 % of uro - genital traumas and differ in penetrating and non - penetrating injuries [ 1 ]  . 
the latter recognize two different conditions , depending on whether they occur with a flaccid penis or during erection ; in this last condition , they are called penile fracture [ 1 ]  . in most cases , the diagnosis of penis fracture is exclusively based on clinical presentation , followed soon after by surgical treatment ; therefore , patients do not always come to imaging [ 24 ]  . in experienced hands , ultrasound can be an excellent diagnostic tool , but it is operator dependent ; it is difficult to gain experience in a condition which occurs so infrequently , and often edema , hematoma and live pain may significantly limit the diagnostic potential of the ultrasound technique . mri is not a strictly operator - dependent technique , giving an overview of the whole penis with no limitations due to patient pa furthermore , it is of fundamental aid in doubtful forms with faded clinical presentation and for the precise location of the tunica albuginea lesion , crucial for a proper surgery plan . 
in fact , on the basis of mri findings , the urologist can choose the most suitable surgical approach for the patient , using more strategically minimally invasive incisional techniques [ 58 ]  . the use of mri in this context is , however , conditioned by several factors : it is an expensive examination and not always accessible , especially in emergency , as is the case of penile fracture . 
the names of the first author of each study were noted as were the specialty and if indicated : the magnetic field strength , fov ( field of view ) , matrix , slice thickness , inter - slice gap , the use of contrast agents and the type of coil used . 
we also extracted the number of patients included . 1 3 radiol med ( 2016 ) 121 : 711718 data extraction and analysis results we chose a systematic approach : the same data extraction approach was applied across all studies for a consistent transparent and systematic process . the quality assessment of diagnostic accuracy studies ( quadas ) tool was used to assess the methodological quality of the included studies [ 9 ] , to perform a systematic review and an associated meta - analysis to find out a tailored mri protocol in suspected penile fracture , reducing costs and time of examination . search strategy and study selection figure 1 depicts study selection in a flowchart . 
of these , we could find full text of 37 articles of which only 12 were eligible as there was a clear description of the sequences and planes used in the fig . 
in the other 25 articles out of 37 , in fact , although mri examinations were carried out on patients with suspected penile fracture , no complete information was provided about planes and sequences used . study and design characteristics there were no original articles focusing on mri accuracy and technique with valid results . 
 [ 17 ] 2013 avery and scheinfeld [ 18 ] coronal one not specified plane injection not specified not necessary not necessary may be useful in some cases not necessary not specified not specified considering the reviews , the most used protocol is characterized by t2 sequences in three planes ( axial , coronal and sagittal ) with t1 sequences in one plane , either axial or sagittal . contrast agent injection is not routinely necessary for these reviews . 
in this case the sequences most used were twoor three - dimensional fat - saturated t1 - weighted gradient echo before , during and after the dynamic administration of intravenous gadolinium chelate ( preferably in the coronal plane )  . other characteristics of the mri protocol for reviews and case reports / clinical series are reported in table 4 . discussion traumatic penile fracture is a rare urological emergency caused by a sudden increase in intracorporal pressure due to an external force , tearing the thinned albuginea of the erect penis . 
the majority of injuries occur during vigorous sexual intercourse , as a result of non - physiological bending of the penis during self - manipulation or forced detumescence or the patient rolling over in bed with an erection [ 8 ]  . the most common penis fractures are characterized by unilateral or bilateral rupture of corpora cavernosa albuginea with urethral involvement in 2030 % of cases [ 5 ]  . in most cases , the diagnosis of penis fracture is exclusively based on clinical presentation , followed soon after by surgical treatment ; therefore , patients do not always come to imaging [ 24 ]  . sonography is the first choice examination because it is easy to perform , non - invasive , widely available and inexpensive . 
 the one small study ( four patients ) that compared us and mr imaging found that us was not helpful , whereas mr imaging was much more informative [ 8 ]  . mri is a non - invasive procedure which provides optimal contrast and spatial resolution in the study of soft tissue , in the absence of ionizing radiation . 
mri offers the ability to demonstrate penile anatomy in three orthogonal planes , with an excellent display of the pendulous portion of the penis [ 21 ]  . penile fracture is an emergency situation and early surgical intervention is mandatory to prevent later complications [ 22 ]  . 
therefore , performing mri will not delay treatment [ 8 ]  . 1 3 716 radiol med ( 2016 ) 121 : 711718 table 4 other characteristics of the mri protocol for reviews and case reports / clinical series year / study matrix slice thickness interslice gap surface coil tesla t1 / tr t1 / te t2 / tr t2 / te not specified not specified not specified not specified not specified not specified not specified 2001 pretorius et al . 
on the basis of mri findings , the urologist can in fact choose the most suitable surgical approach for the patient , using more strategically the minimally invasive incisional techniques , thus limiting the use of more extensive techniques , such as sub - coronal degloving , associated with a higher rate of post - operative complications [ 5 ]  . an mri , though expensive , by aiding in directing the incision to the site of the lesion , avoids unnecessary degloving of the penis and its attendant complications like edema , skin necrosis , and penile curvatures [ 6 ]  . mri examination in clinical suspected penile fracture helps urologists to answer the following questions : is there or not a lesion of the tunica albuginea ? if there is , where is the localization of the lesion ? the integrity of the tunica albuginea is the most important factor in determining the necessity for surgical intervention . 
accurate assessment of the location and severity of the rupture is essential for urologists in determining the optimal site and extent of the incision [ 13 ]  . but the use of mri in this acute condition is , however , conditioned by several factors : it is an expensive examination and it is not always accessible . in fact , being an examination required in urgency it has to be included among the routinely planned daily exams . therefore , we need to be prepared for such an eventuality and in this respect the choice of the correct mri protocol becomes strategic and crucial to reduce the costs , the duration of the examination and the subsequent time of machine usage , as well as answering diagnostic questions . with this paper , reviewing the literature , we aimed to help all the radiologists who have to face these problems in their daily practice activity , suggesting an evidence - based tailored mri protocol for suspected penile fracture . 1 3 radiol med ( 2016 ) 121 : 711718 fig . 
a axial , b sagittal , c coronal t2 - weighted and d axial t1 - weighted mr image demonstrate discontinuity of the low signal intensity tunica albuginea ( white arrow ) with surrounding hematoma ( gray arrow )  . 
d axial t1 - weighted mr image shows a small , round intracavernosal hematoma , with high signal intensity ( black arrow ) with this purpose , analyzing articles that deal with penile fracture , we searched those describing patients who underwent an mri for suspected penile fracture , to evaluate the protocol used . 
a protocol was considered eligible for our study , if at least the sequences and orthogonal planes used were described . after an analysis of the literature , we did not find any trials evaluating the diagnostic accuracy of an mri protocol for penis fracture , so we could not perform a meta - analysis . in our research , we found only few case reports / clinical series fitting our requirements : only five . 
 although contrast is better with t2 sequences , t1 may help to detect more subtle fractures when low signal intensity of an acute hematoma in t2 images can mimic an intact tunica albuginea [ 5 ]  . contrast agent injection is not considered routinely necessary . if , after the visualization of the images documented with the above described protocol , there is still a diagnostic doubt , the use of intravenous contrast medium injection could be useful . 1 3 table 5 suggested mri protocol in penile fracture ethical standards the manuscript does not contain clinical studies or patient data . radiol med ( 2016 ) 121 : 711718 718 tesla matrix slice thickness interslice gap surface coil t1 tr / t1 te t2 tr / t2 te imaging planes on t2 imaging plane on t1 140320 mm 1.5 t 3 mm 1 mm 285600 ms / 815 ms 21005000 ms / 90100 ms axial , coronal , sagittal one plane either axial or sagittal in fact acute hematoma may have a similar intensity to the corpora cavernosa with t1 - weighted sequences , so that intracavernosal hematoma can be seen clearly only as an enhancement defect after contrast material administration [ 5 , 15 ]  . other most used protocol characteristics suggested in the articles recovered by us are : the use of small fields of view , high definition matrix , thin slice thickness , not superior to 4 mm , with an inter - slice gap not superior to 1 mm , with a strength magnet of 1.5 t , preferably with a surface coil . to validate the tailored protocol described above and resumed in table 5 , which aims to reduce costs and time of examination , studies are needed that compare the diagnostic accuracy of this protocol . 
kaplanmeier actuarial estimates of overall survival ( os ) , progression - free survival ( pfs ) , freedom from lr ( fflr ) and freedom from dm ( ffdm ) in different subgroups were compared with the log - rank test . 
the total number of recurrences was 118 ( 64.4 % ) : 44 ( 24 % ) and 74 ( 40.4 % ) for lr and dm , * paolo borghetti paolobor82@yahoo.it7 1 department of radiation oncology , spedali civili of brescia , p.le spedali civili 1 , 25124 brescia , italy 2 department of radiation oncology , brescia university , 3 department of thoracic surgery , spedali civili of brescia , 4 department of pathology , spedali civili of brescia , brescia , 5 department of pneumology , spedali civili of brescia , brescia , italy brescia , italy italy brescia , italy respectively . 
n1 status covers a heterogeneous group of patients , included in stage iia , iib and iiia , according to the 7th edition of the american joint committee on cancer ( ajcc ) [ 1 ]  . 
 1 3 radiol med ( 2016 ) 121 : 696703 moreover , the number of patients who can benefit from this adjuvant treatment is limited because chemotherapy has been frequently withhold in elderly patients , with poor performance status or comorbidities [ 5 ]  . the role of postoperative radiotherapy ( port ) is as well controversial . 
in 1998 , a meta - analysis reported a benefit in terms of recurrence - free survival , despite a detrimental effect in overall survival , especially in patients with early stage ( n0n1 ) completely resected , suggesting that port should not be used routinely for such patients [ 6 ]  . 
this meta - analysis , however , included patients treated with 2d or 3d radiotherapy techniques , and the authors themselves suggest the need to investigate the role of more modern radiotherapy techniques , such as conformal radiotherapy or hyperfractionated radiotherapy , in all stages ( i , ii , and iii ) of completely resected disease . 
thus , there has been a growing interest among radiation oncologists that aim to properly select n1 cases that could potentially benefit from port [ 2 , 6 , 7 ]  . the present study retrospectively analyzes a singleinstitution series of n1 nsclc patients surgically treated , to define the patterns of recurrence and the risk factors for local and distant relapse , focusing on nodal descriptor to emphasize the rationale of local adjuvant treatment . materials and methods between 2001 and 2011 , all consecutive patients who underwent surgery for nsclc at our hospital and who have been post - surgically classified as n1 were retrospectively reviewed . 
patients deceased perioperatively ( in - hospital death within 30 days from surgery ) were also removed . clinical and therapeutic data were collected from medical records and all the histological examinations were reviewed . 
follow - up information was obtained by medical records , reports of general practitioners and radiographic exams ( x - ray , computed tomography , positron emission tomography , bone scans , bronchoscopy , endobronchial ultrasound , guided transthoracic needle biopsy and mediastinoscopy )  . local recurrence ( lr ) was defined as disease relapse at bronchial stump , ipsilateral hilum and mediastinum ; all other sites of failure , including supraclavicular fossa and contralateral hilum were considered as distant metastasis ( dm ) , as considered by others authors [ 2 , 8 ]  . 
progressionfree survival ( pfs ) was calculated from the date of surgery to the date of first event of failure ( local or distant recurrence ) or until the date of the last visit of follow - up or death . 
lr and dm were scored separately and censored as first event , to evaluate the freedom from local recurrence ( fflr ) and freedom from distant metastasis ( ffdm )  . 
overall survival ( os ) was measured from the date of surgery to the date of death ( any cause ) or until the date of the last follow - up . among the variables investigated , the number of examined lymph nodes ( ln ) was categorized dichotomously : < 10 and 10 , as recommended for an acceptable ln dissection [ 9 ]  . 
the optimal cutoff point of 0.15 was determined by generating a receiver operating characteristic ( roc ) curve and calculating the maximal youdens index . the kaplanmeier method was used to estimate pfs , os , fflr and ffdm . 
all the variables grouped by type ( clinical , therapeutic and nodal ) were considered for multivariate analysis that was performed using the cox proportional hazard regression model . a p value < 0.05 was considered statistically significant . 
for all of them , a complete pathology report ( histology , grading , tumor stage , visceral pleural invasion , extra capsular extension ( growth over the nodal capsule ) - ece - , positive and examined ln , ln location and lnr ) and the main therapeutic features ( surgical procedure , type of ln dissection , chemotherapy ) were available . 
 median follow - up of the entire population was 39 months ( range 1166 ) , while median follow - up of living patients was 76 months ( range 13150 )  . the median age at diagnosis was 67 years ( range 4383 )  . 
 ece occurred in 18 cases , corresponding to 8.9 % of cases ; the median number of positive ln was 2 ( range 111 ) and the median number of examined ln was 8 ( range 149 )  . 
no other significant correlations were found with all the other considered variables . fifty - nine patients ( 29.2 % ) were alive at the time of the analysis , and 34 ( 16.8 % ) of them without evidence of disease . 
the involvement of both hilar and peripheral ln ( p 0.037 ) , the presence of ece ( p 0.005 ) and a high lnr ( p 0.011 ) were all related to a worse pfs . 
notably , the lace meta - analysis , favoring the use of platinum - based chemotherapy , reported also a not negligible acute neutropenia rate and an excess of cardiovascular / pulmonary deaths independently from the drug combination and the use of port [ 10 ]  . 
however , it is currently a diffuse opinion that some of the suggestions derived from that metaanalysis need to be reviewed , since they are mostly based on randomized trials dating back up to four decades before the first edition , published in 1998 . 
2 kaplanmeier curves showing freedom from local recurrence ( fflr ) and freedom from distant metastasis ( ffdm ) for entire cohort radiol med ( 2016 ) 121 : 696703 the original version [ 1214 ]  . 
indeed , the trials collected in port meta - analysis are characterized by a huge heterogeneity in terms of radiation sources ( cobalt machines or linear accelerators ) , techniques , treated volumes , fractionations and doses . 
the evidence that port with modern linear accelerators improves loco - regional control and survival with a lower and acceptable toxicity is proven for pn2 lung cancer patients [ 15 ]  . 
their findings supported the hypothesis that morbidity of postoperative 3dcrt is acceptable [ 16 ]  . several factors may affect prognosis and predict patterns of recurrence in the heterogeneous population of patients with pn1 nsclc . 
lr occurred in approximately one - fourth of the evaluable patients and constitute more than a third of the causes ( 37.3 % ) of the first disease progression after treatment . 
to date , data suggest that , when feasible , adjuvant port could favorably alter the natural history of resected lung cancer , by reducing lr rate ; consequently , factors predicting an higher lr rate could be used to select pn1 patients for whom the benefit of radiotherapy is greater [ 2 , 3 ]  . 
 similar results have been found also in other neoplasms ; ece has been identified as an independent prognostic factor for breast cancer , head and neck carcinoma , bladder and rectal cancer [ 1824 ]  . on the contrary , the prognostic value of lnr has been the object of many retrospective studies , as an index of both the extent of lymphadenectomy and the 1 3 702 radiol med ( 2016 ) 121 : 696703 number of positive nodes [ 7 , 9 ]  . 
in a large series of 6551 pn1 nsclc patients obtained from the surveillance , epidemiology and end results ( seer ) database , showed a significant worsening of os along with increasing lnr values [ 7 ]  . 
similar results have been found also for breast , esophageal , pancreatic , biliary duct cancers , remarking lnr - independent role to predict prognosis [ 28 31 ]  . 
moreover , lnr seems to have a role as a predictor not only of lr but also of os and thus it should be considered a cornerstone to select a population who can benefit from adjuvant radiotherapy . conclusions unfavorable prognostic factors such as nodal risk factors should be considered to select patients that might be the advantage of port . 
perspective studies based on accurately selected patients and modern radiotherapy could be the key to re - evaluate port in pn1 . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent for this type of study ( retrospective study ) , formal consent is not required . radiol med ( 2016 ) 121 : 735743 doi 10.1007 / s11547 - 016 - 0650 - 5 radiotherapy radiotherapy in the multidisciplinary treatment of liver cancer : a survey on behalf of the italian association of radiation oncology francesco dionisi1 alessia guarneri2 veronica dellacqua3 mariacristina leonardi3 rita niespolo4 gabriella macchia6 tiziana comito5 maurizio amichetti1 pierfrancesco franco2 savino cilla7 luciana caravatta8 filippo alongi9 giovanna mantello10 received : 10 february 2016 / accepted : 9 may 2016 / published online : 2 june 2016 italian society of medical radiology 2016 abstract purpose to report the results of the first italian survey investigating the role of liver - directed radiotherapy in the multidisciplinary approach of primary and metastatic liver cancer . materials and methods a 21 - item , two - section questionnaire was sent to all italian radiotherapy centers on june 2014 . 
the two sections aimed at : ( 1 ) evaluating the presence of a multidisciplinary liver tumor board and describing the role of radiation oncologists within the latter , ( 2 ) analyzing radiotherapy treatment details and differences between centers . results a total of 37 centers completed the survey . 
a multidisciplinary liver tumor board was available in most centers ( 73 % ) , with a radiation oncologist routinely attending the latter in the majority of cases ( 85 % )  . 
dose was prescribed at the ptv margin in most cases . conclusion liver - directed radiotherapy represents a new field of interest which is currently adopted by 10 % of all italian centers . 
 the variations observed in the treatment regimens reflect the lack of a well - established standard schedule . keywords hcc liver metastases radiotherapy sbrt introduction liver is a common site of primary and metastatic cancer disease . 
hepatocellular carcinoma ( hcc ) is the fifth most frequent malignancy ( 5 % of all cancer cases ) and it is * francesco dionisi francesco.dionisi@apss.tn.it 1 proton therapy unit , department of oncology , azienda provinciale per i servizi sanitari , apss , via al desert , 14 , 38123 trento , italy 2 department of oncology , radiation oncology , university of torino , turin , italy 3 division of radiation oncology , european institute of oncology , milan , italy 4 department of radiation oncology , san gerardo hospitaluniversity of milan - bicocca , monza , italy 5 radiation oncology department , humanitas clinical and research center , italy cancer center , rozzano , milan , italy 6 radiation oncology unit , research and care foundation giovanni paolo ii , catholic university of sacred heart , campobasso , italy 7 medical physics unit , research and care foundation giovanni paolo ii , catholic university of sacred heart , campobasso , italy 8 radiation oncology department , san francesco hospital , 9 radiation oncology , sacro cuore - don calabria hospital , nuoro , italy negrar - verona , italy 10 department of oncology and radiotherapy , azienda ospedaliero universitaria ospedali riuniti , ancona , italy 1 3 736 radiol med ( 2016 ) 121 : 735743 characterized by a high short - term mortality being the third leading cancer - associated death cause worldwide [ 1 ]  . 
in italy , hcc represents 2.3 % of all cancers ( males / females ratio : 2 : 1 ) with about 13 , 000 new cases expected for 2015 and a gradual increase in the next two decades [ 2 ]  . 
on the other hand , liver metastases occur in about 3050 % of cancer patients [ 3 ]  . several loco - regional treatment approaches for primary and metastatic liver cancer have been evaluated ; radiation therapy ( rt ) historically has been rarely proposed as a therapeutic choice , playing a minor role in this specific setting . 
the reason of the exclusion of rt from the context of liver cancer disease could be related to the limited tolerance of surrounding healthy liver parenchyma and to the high doses required for local tumor control , with a consequent narrowing of the therapeutic window . however , in the last decades , continuous technological advancements in the field of rt have allowed clinicians to prescribe focused and high tumoricidal doses to the tumor site and at the same time sparing surrounding healthy tissues . 
in particular , the most relevant innovations in rt include : ( a ) accurate target volume delineation with the support of rigid - deformable image registration tools between simulation and morphological and functional diagnostic imaging [ 4 ] , ( b ) organ motion quantification and incorporation into planning ( 4d computed tomography , breath hold , gating and tracking techniques ) [ 5 ] , ( c ) new delivery techniques as stereotactic body radiotherapy ( sbrt ) [ 6 ] , ( d ) new on board imaging devices for preand post - treatment set - up verification , i.e. , cone beam computed tomography ( cbct ) [ 7 ]  . 
all these advances can enlarge the therapeutic window for liver cancer patients , allowing for a better tailoring of the target volume , the further increasing of the dose prescription while sparing the nearby healthy tissues . nevertheless , rt used in treating primary and secondary liver malignancies still remains not well recognized as a valid treatment option in the multidisciplinary scenario of liver cancer disease due to the lack of robust evidence and the fear of potentially life - threatening liver toxicity [ 8 , 9 ]  . in 2012 , the italian association of radiation oncology gastrointestinal group ( airo - gi ) published a handy , pocket - sized hand book that summarizes the main relevant guidelines in the field of gastrointestinal oncology ( available on line at ) ; the rt use for primary and metastatic liver cancer was included in the guidelines as an area of investigational challenge . 
therefore , in 2014 the airo - gi group promoted a survey among all italian rt centers aimed to investigate the role of italian radiation oncologists in the multidisciplinary approach of primary and metastatic liver cancer , to acknowledge the number and type of centers nowadays performing liver irradiation , and to describe the clinical features and techniques most used for hepatic irradiation . materials and methods survey design and questionnaire the study questionnaire was designed by airo - gi liver subgroup on april 2014 , and approved in its final form on may 2014 . 
the first section , entitled multidisciplinary approach , was aimed at ( 1 ) evaluating the presence of a multidisciplinary liver tumor board in surveyed hospitals ; ( 2 ) describing the role of radiation oncologists within the latter . 
it included five sub - sections exploring : ( 1 ) demographic data of surveyed centers , ( 2 ) set - up features , ( 3 ) treatment volume identification , ( 4 ) radiotherapy dose prescription and treatment planning details , ( 5 ) treatment verification procedures . 
 frequencies and / or percentages were used to present data distribution . results between june and november 2014 returned questionnaires were centrally collected at the hospital of trento . a total of 37 centers ( 21.5 % of all italian rt centers ) completed and resubmitted the survey with a good representation of all the italian regions ; 16 of 20 regions ( 80 % ) had at least one center that had responded to the questionnaire . section 1 ( multidisciplinary approach ) a multidisciplinary gastrointestinal and / or liver tumor board was available in 27 centers ( 73 % ) , with a radiation 1 3 radiol med ( 2016 ) 121 : 735743 fig . 
 the majority of centers were private ( 39 % , n 7 ) accredited by national health care or academic centers ( 28 % , 4 ) or private centers ( 11 % , n 5 ) ; the remaining were public ( 22 % , n 2 )  . an overview of start - up timing and the overall figures of irradiated patients for hcc and liver metastases among surveyed centers is reported in table 1 . simulation ct procedures in most cases motion assessment was performed by a four dimensional computed tomography ( 4dct ) approach . 
 specifically , the use of anatomical surrogates ( diaphragm , liver surface ) or the use of contrast 4dct were the most adopted techniques to define tumor motion ( 50 % , n 9 )  . six centers ( 33 % ) acquired a 3d - ct scan in both inhale and exhale respiratory phase during simulation . 
2 the centers explanation in case the use of radiotherapy was not considered for liver disease treatment ( multiple answers were allowed ) radiol med ( 2016 ) 121 : 735743 table 1 overview of start - up timing and number of irradiated patients for hcc and liver metastases among surveyed centers centers liver metastases year of starting hcc irradiation irradiated patients since the starting irradiated patients in 2014 year of starting liver metastases irradiation irradiated patients since the starting irradiated patients in 2014 2006 2013 2011 2014 2002 2013 2011 2013 2012 1995 2013 2006 2009 2005 > 20 > 20 > 10 2012 2002 2007 2012 2012 2011 2014 2002 2006 2007 2012 2003 1995 2014 2013 2006 2009 2005 > 30 > 20 > 20 > 30 > 30 > 30 > 10 > 10 > 10 > 10 > 20 treatment techniques and fractionation schedules hypofractionated sbrt was adopted by all centers . 
in fact , higher response rates ( ranging from 39 to 50 % ) have been registered when similar surveys were reserved to radiotherapy centers already treating liver cancer , as in the international survey on liver metastases radiotherapy reported by lock et al . 
interestingly , the majority of radiation oncologists considered hcc and metastases rt as the third line choice , when surgery and other loco - regional therapies ( i.e. , radiofrequency ablation , chemo - embolization ) were not indicated or technically feasible . 
furthermore , rt is not yet considered a treatment option for hcc and liver metastases in about one - third and one - fifth of the surveyed centers , respectively . 
these partially unexpected findings could be justified by the frequent hepatic impairment accompanying hcc patients who are often exposed to a higher risk of radiation - induced liver toxicity than metastatic ones [ 12 ]  . 
 moreover , the use of rt in the treatment of hcc is not recognized as a worldwide standard of care ; it is generally considered as an alternative to ablation / chemoembolization for unresectable hcc in american and asiatic policies [ 9 , 13 ] , whereas european guidelines are unwilling to include rt as a treatment option for this disease [ 14 ] due to the lack of high - level evidence and the potentially lifethreatening liver toxicity . 
conversely , the involvement of radiation oncologists in the multidisciplinary team evaluating oligometastatic colorectal cancer along with the use of sbrt as an alternative for patients with liver metastases not amenable to surgery is recommended by the recently published guidelines of the european society of medical oncology ( esmo ) [ 15 ]  . however , according to the current survey , the controversy within international guidelines on the rt role for liver cancer did not represent the main reason to exclude radiation from liver cancer treatment scenario : the major issue indicated by more than one - third of respondents was indeed represented by the lack of expertise in treating liver disease . 
this interesting finding could be historically explained by the role of liver rt that has been mainly utilized to control symptoms due to poor liver tolerance [ 16 ]  . 
 moreover , the first reports about the modern irradiation techniques including sbrt are relatively recent [ 17 ] , and even more recent are the first robust data about its safety and efficacy for primary [ 18 ] and for metastatic liver cancer [ 19 ]  . 
the blooming in the last decade of a vast arsenal of alternative therapies [ 20 , 21 ] , together with the lack of sbrt expertise might justify the here reported results . however , we found that liver irradiation is , currently employed by a tenth of all the italian centers , with 44 % ( secondary cancer ) and 57 % ( hcc ) of center shaving adopted this approach in 2010 or later . 
the use of sbrt will probably increase in the coming years due the technological revolution in the radiotherapy field . as shown in table 1 , a considerable variability between overall hcc and metastatic treated patients was registered , as in the total number of patients as well in patients treated last year : again , the scarce amount of hcc patients could be firstly explained by the aforementioned concern in the irradiation of cirrhotic patients requiring specific skills . several interesting findings resulted from the clinical and technical details provided by the respondents . 
 the basis for this choice could be the assumption that the microscopic extension beyond the main tumor is function of the tumor and the liver status in hcc patients , with a maximum of 4 mm for tumors larger than 5 cm as reported in the study of wang et al . 
however , this study did not allow definitive and precise conclusions to be drawn about the need of an extra margin in sbrt planning to compensate for microscopical extension ; indeed , even with the most conformal techniques a certain amount of high dose beyond the gtv is unavoidable thus compensating the need for an extra gtv margin . stereotactic body radiotherapy was employed as the unique rt technique by all centers but one : in the majority of centers ( 61 % ) the treatment was delivered on consecutive days . stereotactic body radiotherapy has several advantages in comparison with standard 3d radiotherapy , including the delivery of higher doses per fraction with potential radiobiological gain over conventional fractionation [ 25 ] , especially for radioresistant tumors , along with the reduction of the overall treatment time , which could be strategically of interest considering the possible integration of radiotherapy into the standard treatment course of liver cancer patients [ 26 ]  . 
in this context , the currently ongoing rtog 1112 ( nct01730937 ) phase iii trial aims to determine if the addition of sbrt improves survival in hcc patients treated with standard therapy ( sorafenib )  . 
nevertheless , a more accurate treatment workflow and a consequent specific expertise is needed in comparison with 3d radiotherapy [ 26 ]  . there was a broad range of dose prescriptions among the centers : this was somewhat expected considering the relatively recent implementation of sbrt and it has been already reported by other surveys [ 11 ]  . 
however , the existence of a doseoutcome relationship has been clearly reported for both hcc and liver metastases [ 27 , 28 ]  . 1 3 742 radiol med ( 2016 ) 121 : 735743 the huge variation in fractionation schedules reflects the lack of high - level evidence regarding the proper radiation dose to deliver for both hcc and metastases . moreover , the presence of several patient and tumor characteristics ( target size , liver function , disease site , number of lesions , etc . ) to be considered for dose prescription hampers the adoption of unique and universally adopted fractionation schedules . 
in light of this , in our analysis , centers with the highest experience in radiotherapy liver treatment did not show a clear trend towards the use of a more biologically effective prescription dose . however , the most commonly reported dose prescription was 5 gy in three fractions for both hcc and liver metastases , which is consistent with the prescription dose reported for liver irradiation by both the survey regarding sbrt conducted in usa by pan et al . 
 similar results came from the eastern world : according to a recently published survey about the use of sbrt in korea , the most common schedule for hcc was 60 gy in three fractions followed by 45 gy in three fractions . 
the most common schedule for treatment of liver metastases was 45 gy in three fractions [ 22 ]  . the present survey aimed also to register the different dose prescription methods adopted by the centers . 
there are two methods to account for dose in the target in sbrt [ 29 ] : the former aims to maintain dose homogeneity in the target , while in the latter the dose is prescribed at the ptv margin with variable dose inhomogeneity within the target . 
 in our survey , in the great majority of centers rt dose was prescribed with the latter method , with the result of maximum doses within the target even superior to 30 % of the prescribed dose . 
there could be sensible variations in the total accumulated dose with potential differences in outcome according to the two methods : thus , in our opinion , this information remains crucial and it should be always reported . in conclusion , the main findings resulting from the present survey could be summarized as follows : in italy , rt could have a role in treatment of primary and secondary liver cancer , mainly as an alternative or in case other loco - regional therapies are not indicated or technically suitable . 
survival after stent insertion ranged * chi cao xzcaochi@126.com 1 department of operation room , xuzhou central hospital , 199 south jiefang road , xuzhou , jiangsu , china 2 department of interventional radiology , xuzhou central hospital , 199 south jiefang road , xuzhou , jiangsu , china from 96 to 432 days ( median 165 days )  . 
airway stent insertion had been reported as a safe and effective palliative method in patients with inoperable airway stenosis [ 14 ]  . when the obstruction is located in the carinal region , the use of straight stents is limited due to the y - shaped anatomy of the carina . 
 [ 8 ] designed an integrated self - expanding y - shaped airway stent ( micro - tech , nanjing , china ) , which can be placed under fluoroscopic guidance and local anesthesia . 
in addition , y - shaped stents have also been used for other bifurcated anastomotic stenosis , such as stenosis after gastrojejunostomy ( billroth ii ) and hilar biliary stenosis [ 9 , 10 ]  . 
in this study , we described our clinical results of integrated selfexpanding y - shaped airway stent placement in patients with carinal stenosis . 1 3 radiol med ( 2016 ) 121 : 744750 materials and methods the study was approved by our institutional review board . 
tumor stage was evaluated based on the criteria of the american joint committee on cancer / international union against cancer ( ajcc / uicc )  . study design from may 2010 to march 2015 , 12 consecutive patients with carinal stenosis , treated by placement of integrated self - expanding y - shaped airway stent , were included this retrospective study . 
baseline data included patients history , clinical presentations , and imaging findings . diagnosis the integrated self - expanding y - shaped airway stents were covered or uncovered nickel - titanium alloy stents ( microtech , nanjing , china ) and chosen based on the results of the preoperative examination . 
the covered stents were used for patients with carinal stenosis and fistula , and the uncovered stents for patients with simple carinal stenosis . the diameter and length of the body ( tracheal stent ) varied from 18 to 20 mm and from 30 to 40 mm , respectively ; the diameter and length of the two bronchial limbs varied from 11 to 12 mm and 15 to 30 mm , respectively . treatment procedure carinal stenosis was diagnosed based on patients history and results of thoracic computed tomography ( ct )  . 
b the photo of integrated self - expanding y - shaped airway stent 1 3 746 radiol med ( 2016 ) 121 : 744750 anesthesia ( 5 ml of 2 % lidocaine aerosol ) with nasal cannula oxygen supply ( 26 l / min ) was routinely used . 
a 4 - f angiographic catheter ( cordis , warren , nj , usa ) and 0.035 - inch radifocus guide wire ( terumo , tokyo , japan ) were inserted through the mouth across the stenosis into one of the main bronchi , and then , the guide wire was exchanged for a 0.035 - inch stiff radifocus guide wire ( terumo )  . 
the entire stent within the introducer sheath was , then , advanced further , so that the two bronchial stents passed over the two guide wires into the bilateral main bronchi . 
 clinical success was defined as an improvement of at least one grade in the hj classification grade 3 days after treatment . all patients underwent thoracic ct 37 days , 1 month , and every 23 months after treatment to evaluate the long - term patency of the stents . 
the follow - up ended at the time of starting this study ( september 2015 ) or patients death . statistical analysis the variations before and after treatment were compared by paired t - test . 
two patients experienced re - ste6.5 nosis of the stent due to tumor growth ( n 1 ) or tissue granulation ( n 1 ) , 75 and 78 days after treatment , respectively . 
 this study evaluated the feasibility , effectiveness , and prognosis of integrated self - expanding y - shaped airway 1 3 747 radiol med ( 2016 ) 121 : 744750 fig . 
these results indicate that integrated self - expanding y - shaped airway stent placement is an effective treatment for patients with carinal stenosis . approximately 30 % of malignant airway stenosis patients have carinal stenosis [ 2 ]  . 
integrated y - shaped stent is superior to y - configuration made by two straight stents in management of carinal stenosis : ( a ) integrated y - shaped stent can completely cover the stenotic site . 
 ( b ) integrated y - shaped stent has less opportunity to migrate , because its three - tier structure confirms to the anatomy of the carina . the most commonly used integrated y - shaped airway stent is silicone dumon stent , which needs to be placed using bronchoscope under general anesthesia [ 35 ]  . 
in a retrospective study of bronchoscopy - guided dumon y - shaped stent insertion in 86 patients with malignant carinal stenosis , both the technical and clinical success were 100 % [ 4 ]  . 
however , dumon y - shaped stent needs 1 3 radiol med ( 2016 ) 121 : 744750 after stent insertion was 165 days , which is comparable to the previous studies . this study had some limitations . 
third , there was no control group . in conclusion , although further clinical trials are needed , this study demonstrated that integrated self - expanding y - shaped airway stent placement is a simple , safe , and effective method for patients with carinal stenosis . compliance with ethical standards funding none . conflict of interest the authors declare that they have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the authors dem5 rats , that application onstrated , in an experiment on 2 of 0.625 mmol / kg gd - eob - dtpa resulted in significantly higher gadolinium tissue deposition in hepatorenally impaired rats compared to renally impaired rats . 
the effect was statistically significant in kidneys , spleen and liver but not in other organs . based on the methodology used to detect the tissue gadolinium ( gd ) , the time point of the analysis and the missing validation of the animal model , we think that this experimental setting does not allow any conclusions on gadolinium tissue deposits . the authors state that icp - ms cannot distinguish between chelated and unchelated gd . 
at this early time point , it is reasonable to assume that the measurements not only assessed gd * jan endrikat jan.endrikat@bayer.com 1 global medical and clinical affairs , radiology , bayer healthcare medical care , mllerstrasse 178 , 13342 berlin , germany 2 department of gynecology , obstetrics and reproductive medicine , university medical school of saarland , 66421 homburg / saar , germany 3 global medical and clinical affairs , radiology , bayer healthcare medical care , 100 bayer boulevard , whippany 07981 , nj 4 mr and ct contrast media research , radiology , bayer healthcare medical care , mllerstrasse 178 , 13342 berlin , germany deposits but also chelated soluble gd . 
 would be the earliest reasonable time point for determination of gd tissues deposits . the excretion kinetics of gd - eob - dtpa of the animal model was not thoroughly described prior to start of the experiments . 
and would compromise the conclusions on gd tissue deposits . in addition , the hepatocyte - specific uptake and hepatobiliary excretion of gd - eob - dtpa are based on the saturable uptake by anion - transporting polypeptide 1 transporters ( oatp1 ) [ 2 ]  . 
in the rare case that patients have both severe renal and severe liver impairments , even more caution would be exercised . 1 3 radiol med ( 2016 ) 121 : 238239 in conclusion , based on the methodology used to detect the tissue gd , the time point of the analysis and the missing validation of the animal model , we think that this experimental setting does not allow any conclusions on gadolinium tissue deposits . 
in this study , the frequency and the reporting rate of cardiovascular findings in chest ct examinations were retrospectively assessed . materials and methods this study was approved by the institutional review board of each participating center . 
a total of 220 / 447 ( 53.7 % ) and 227 / 447 ct ( 46.3 % ) examinations were evaluated and reported by junior and senior chest radiologists , respectively . 
inter - observer agreement was assessed using the kappa coefficient of agreement ( k )  . results the study inter - observer agreement between reviewers was moderate to good ( 0.40.73 ) for most of the incidental cardiovascular findings . 
at least one incidental cardiovascular finding not documented in the original report was identified by the study reviewers in 225 / 409 ( 55 % ) of chest ct examinations . 
gramsci 14 , 43100 parma , italy 2 department of radiology , sdn foundation , irccs , naples , italy 3 radiologia clinica , di.s.c.o. , universit politecnica delle marche , ancona , italy 4 uos radiologia toracica e tc , istituto di radiologia fondazione policlinicio san matteo irccs , pavia , italy 5 radiology unit , cardio - thoracic - vascular department , university hospital s . 
orsola - malpighi , bologna , italy 6 section of integrated imaging and radiological therapies , department of neuroscience , university of chieti , chieti , italy 7 division of radiology , department of experimental , diagnostic and specialty medicine ( dimes ) , s . 
 orsola - malpighi hospital , university of bologna , bologna , italy institute of radiology , university of turin , aou san luigi gonzaga , orbassano , turin , italy 9 department of radiology , erasmus medical center university , rotterdam , 3015 rotterdam , the netherlands 10 department of bioimaging and radiological sciences , catholic university of rome , rome , italy 1 3 radiol med ( 2016 ) 121 : 190199 conclusions several cardiovascular abnormalities can be reliably identified on standard chest ct . 
yet , they are often under - reported , even when they might be relevant to the patients work - up . materials and methods study design keywords cardiac findings chest computed tomography incidental overlooking introduction cardiac and vascular diseases are often first diagnosed or suspected based on findings on chest radiography ( cxr ) [ 1 ]  . 
a similar approach should be also adopted when reporting chest computed tomography ( ct )  . a number of cardiovascular findings , such as coronary artery calcification ( cac ) , mediastinal vessels enlargement and cardiac chambers abnormalities , are easily identifiable on chest ct , albeit without any electrocardiography ( ecg ) synchronization [ 26 ]  . 
these findings may represent important supporting information for the interpretation of chest ct in patients complaining of thoracic symptoms ( e.g. , chest pain and haemoptysis ) that may carry an underlying cardiac cause or association . 
in addition , some cardiovascular abnormalities even if they are not the primary target of the investigation may actually be the main finding and have prognostic relevance [ 4 , 7 ]  . 
showed that an unselected population undergoing chest ct for various indications contains a substantial proportion of subjects that are at high risk for cardiovascular events , which may be predicted by considering a few conventional clinico - demographic risk factors and assessing the severity of cardiac calcification and the heart size on chest ct through a simple visual scoring system [ 8 ]  . while the problem of reporting unsuspected thoracic findings that are visible on cardiac ct examinations has been extensively investigated over the last decade , it remains unclear whether ( and , to what extent ) radiologists ( particularly chest subspecialists ) look at and report cardiovascular abnormalities on chest ct [ 9 , 10 ]  . 
it has been shown that cts requested for the exclusion of pulmonary embolism have a high yield of cardiac abnormalities , which were reported only in a small minority of cases [ 11 ]  . 
each of these centers was asked to provide 120 ct scans of patients aged 18 years and older consecutively evaluated during the year before the study start - up ( 2008 )  . 
 each 120 - ct dataset had to include a series of studies investigating specific groupings of pulmonary disease entities more likely associated with cardiovascular disease , as follows : 40 high - resolution ct ( hrct ) scans that had been evaluated for any lung fibrosis ( either with an usual interstitial pneumonia or nonspecific interstitial pneumonia radiologic pattern ) , 40 ct scans that had been evaluated for suspected pulmonary embolism , 40 ct scans that had been evaluated for lung cancer staging . 
furthermore , one half of each group of cases had to be reported by a senior local radiologist ( with more than 10 years of experience in chest imaging ) and the other half by a junior local radiologist ( with 15 years of experience in chest imaging )  . 
slice thickness varied according to the ct indication and corresponding protocol but had to be no greater than 2.5 mm for ct pulmonary embolism or lung cancer staging , and 1.5 mm for hrct to be eligible . 
ct scans for both pulmonary embolism and lung cancer staging had to be performed with and without contrast 1 3 192 radiol med ( 2016 ) 121 : 190199 medium , and both scans were provided for review . 
hrct images were instead provided at lung window setting , which could however be manipulated by the study reviewers . the ct scans were reported by eight radiologists , two for each center , whose characteristics are outlined in the supplementary table 1 . image evaluation all the study cases were anonymized and transferred via digital supports for review . 
the study reviewers , who performed the readings independently , were blinded to each others identity as well as to the results of original evaluation of the images . reviewers were asked to fill a preformatted score sheet for the assessment of cardiovascular findings ( table 1 )  . 
some cardiac findings , such as individual cardiac chamber enlargement , left ventricle myocardium hypertrophy , left ventricle pseudo / aneurysm , filling defect in any cardiac chamber , were scored only for contrast studies . by understanding of the current ct literature knowledge , a number of cardiovascular findings were regarded as worthy of further clinical / diagnostic work - up or treatment , and were subgrouped as potentially clinically significant . 
main pulmonary artery enlargement was assessed by comparing its diameter with that of the adjacent ascending aorta ; a ratio greater than one was regarded as abnormal [ 22 ]  . 
reviewers were allowed to use the electronic caliper for measuring both vessels and cardiac chambers size , manipulate the window setting and use multiplanar reformations to assimilate all features present on the ct images . score sheets with the reviewers results were returned for data analysis . 
for each patient , the original ct reports were manually scrutinized by one registrar ( kk ) to evaluate whether any cardiovascular finding had been identified prospectively by the local radiologists . data analysis the reviewers scores and the cardiovascular findings mentioned in the original reports were compared using the kappa coefficient of agreement ( k )  . 
they include : ( 1 ) presence of cac , regardless of its severity ; ( 2 ) presence of any valvular calcification ( even without specifying individual valves ) ; ( 3 ) and presence of any pericardial effusion ( regardless of its severity )  . 
similarly , any valvular calcification or pericardial effusion was , respectively , re - scored as any valvular calcification , any pleural effusion . the mcnemar test was performed for paired frequency comparisons . 
the chi - square test for trend was also used to verify if the referring hospital , the observer experience , and disease grouping were factors influencing the reporting rate of the most frequent cardiovascular abnormalities . a p value < 0.05 was considered statistically significant . 
therefore , the final study cohort 9.8 , included 447 subjects ( mean age 70.8 years old range 3497 ; 276 men , mean age 71 years old , range 4796 ; 171 women , mean age 70.3 years old , range 3497 ) who underwent 286 / 447 ( 64 % ) contrast enhanced ct ( 140 / 286 for suspected pulmonary embolism and 146 / 286 for lung cancer staging ) and 161 / 447 ( 36 % ) hrct examinations . the kappa values between the study reviewers were to good for most cardiovascular findings moderate ( table 2 )  . 
the kappa values between the study reviewers were substantially higher than those recorded between the study reviewers and the local 1 3 194 radiol med ( 2016 ) 121 : 190199 fig . 
1 unreported left ventricular aneurysm in a 66 - year - old man with pulmonary embolisthe thin apical myocardium is markedly dilated and curvilinear foci of fat attenuation ( arrow ) can be also noted reports scores are compared in table 1 , supplementary tables 2 and 3 . 
these also included other findings ( indicated under the term others in table 1 ) such as one ( 0.3 % ) non - patent coronary artery bypass graft ( cabg ) , one ( 0.3 % ) aortic arch aneurysm , one ( 0.3 % ) myocardium metastasis ( 0.3 % ) , and three ( 1 % ) penetrating aortic ulcers . 
the chest radiologists of one institution tended to report more frequently cac ( p 0.04 ) , while those of other two indicated more frequently the main pulmonary artery enlargement ( p < 0.0001 ) as compared to the other ones . 
2 abnormal thinning and lipomatous metaplasia of the left ventricular wall ( arrow ) , akin with sequelae of myocardial infarction in a 55 - year - old man with lung fibrosis . 
the latter were poor to fair for most parameters , and moderate only for pericardial effusion , pericardial calcification , right cardiac chambers and main pulmonary artery enlargement ( table 2 )  . after consensus , 409 / 447 ( 91.5 % ) chest cts were scored by the study reviewers as showing at least one cardiovascular finding . 
the study reviewers and the original this study highlights that several cardiovascular abnormalities can be detected on non - ecg - synchronized ct scans performed for evaluating pulmonary diseases , and that even radiologists with training in chest imaging tend to underreport them . the moderate to good levels of agreement between the study reviewers for most cardiovascular findings suggest that their identification is reliable on standard chest ct . 
a training session with illustrations of all findings on the standardized score sheet might further improve the observers agreement . the poor agreement between the study observers and the local chest radiologists is due to the substantial underreporting of cardiovascular abnormalities by the latter . 
of note , 177 / 447 ( 39.6 % ) of the study subjects were scored as having some potentially clinically significant cardiovascular findings by the study reviewers , but 65 % of them were unmentioned in the original reports . 
for example , myocardium infarction may be silent and detection of its sequelae ( i.e. , fatty areas in the left myocardium , left ventricle aneurysm ) may imply a more specific clinical assessment also in candidates for lung cancer surgery or explain the patient symptoms ( e.g. , chest pain or dyspnea ) [ 7 , 24 ]  . 
left - sided heart chambers enlargement may corroborate a diagnosis of heart failure or valves disease , whereas in the presence of a right ventricle enlargement cor pulmonale should be excluded ( especially if associated with other signs ) in subjects with pulmonary embolism [ 2 , 25 ]  . in line with the results reported by choy et al . , cac and valvular calcification were the most frequent findings [ 12 ]  . 
3 unreported left ventricular myocardial hypertrophy in a 73 - year - old woman with lung cancer calcifications in the heart are a marker of increased risk for cardiovascular morbidity and mortality [ 21 , 26 ]  . 
although usually indicative of sclerosis ( by aging ) , valvular calcification might also suggest hemodynamically significant stenosis ( or regurgitation ) that may be unknown to referring physicians [ 12 , 27 ]  . 
 likewise , ascending aortic calcification was also underreported despite representing a manifestation of early as well as generalized atherosclerosis [ 28 ]  . cac was present in 72 % of our study cohort but was recorded in the final radiology report as present in only 25.8 % of these subjects . 
we could not stratify the prognostic value of cac in our study cohort as the study observers applied a different cac classification system . several factors may explain the observed under - reporting of cardiovascular findings . 
it is likely that more experienced chest radiologists were more aware of the importance of looking at the heart in chest ct , because this assessment was more defined several decades ago for cxr . 
4 unreported dilated right heart chambers ( a ) in a 64 - year - old man with acute severe pulmonary embolism ( b ) extra - coronary calcification were more often reported on hrcts , likely because non - contrast image set was more overlooked in contrast ct studies ( i.e. , those acquired either for lung cancer staging or suspected pulmonary embolism )  . more importantly , the absence of consensus on the definition and classification of the cardiovascular findings on chest ct might lead radiologists not to consider the indeed , it is unclear which cardiovascular findings are relevant and which are not in individual patients subgroups , although this should be addressed in the future . 
for example , despite the aforementioned prognostic value , reporting any calcification in patients with lung cancer may be 1 3 radiol med ( 2016 ) 121 : 190199 fig . 
these findings were not reported by the local radiologist identifiable on chest ct , but to evaluate the reliability , and reproducibility of their identification , and to provide a snapshot of their reporting rate in clinical practice . 
 although underreporting of the cardiovascular findings cannot be regarded as diagnostic errors ( for the reasons outlined above ) , at least this study snapshot suggests that the cardiovascular findings were not totally ignored by radiologists who probably need some benchmark data . 
these aid in structured reporting and clinical interpretation of readily available incidental information by chest ct readers in routine practice [ 8 , 33 ]  . this study has some limitations . 
 nevertheless , the observed high prevalence of cardiovascular findings highlights the importance of looking carefully at the heart , which is more assessable nowadays with the use of multidetector ct scanners with very high temporal and spatial resolution . 
however , the size and the characteristics of this study population may still be not sufficiently comprehensive to fully understand whether and how radiologists report the cardiovascular findings on standard chest ct . 
5 unreported calcified aneurysm of the aortic arch depicted on both axial ( a ) and reformatted sagittal ( b ) ct image of a 62 - year - old man undergone contrast ct scanning for suspected pulmonary embolism useless or even misleading for referring physicians ; the value of assessing the right ventricle enlargement ( particularly on non - cardio - synchronized ct scanning ) is uncertain as some studies failed to show prognostic differences between patients with and without right heart enlargement in pulmonary embolism [ 30 , 31 ] ; pulmonary artery dilatation may be found in the absence of pulmonary hypertension in patients with pulmonary fibrosis and is therefore an unreliable sign in these patients [ 32 ]  . however , the purpose of this study was not to establish the clinical relevance of the cardiovascular findings 1 3 198 radiol med ( 2016 ) 121 : 190199 influence the reporting rate of the cardiovascular findings as clinical information on the cardiovascular disease are seldom provided to radiologists before reporting chest ct . 
 further data are needed to establish whether and to what extent some cardiovascular findings other than cardiac calcification can be observed in other settings ( e.g. , normal subjects , screening participants )  . in conclusion , this study shows that several cardiovascular abnormalities can be detected on standard chest ct examinations , but , regardless of their potential relevance , they are often under - reported . 
although this study cannot show if routine chest ct should be considered a screening tool for cardiovascular disease , it suggests that it might be worth systematically evaluating cardiovascular abnormalities to discuss their significance and further diagnostic work - up with clinicians . 
at a total median 0.95 ; icc * francesco giganti giganti.fra@gmail.com 1 department of radiology and centre for experimental imaging , san raffaele scientific institute , vita - salute university , via olgettina 60 , 20132 milan , italy 2 vita - salute san raffaele university , milan , italy follow - up of 19 months ( 249 months ) , 4 patients had died . 
dwi might be introduced into clinical practice as a promising and reliable technique in the diagnostic pathway of this tumour . 10 keywords oesophageal cancer diffusion - weighted magnetic resonance imaging apparent diffusion coefficient prognosis neoadjuvant therapy surgery introduction the incidence of oesophageal cancer in the european union is 4.5 cases / 100 , 000 year and despite the considerable geographical differences among the countries , prognosis is dramatically poor for advanced stages ( 5 - year survival rates varies between 4 and 10 % ) [ 1 ]  . 3 department of surgery , san raffaele scientific institute , the two most important prognostic indicators are local vita - salute university , milan , italy invasion [ 2 ] and nodal involvement [ 3 ]  . 4 pathology unit , san raffaele scientific institute , milan , italy 5 department of oncology , san raffaele scientific institute , vita - salute university , milan , italy as a result , according to preoperative staging , treatment can range from endoscopic mucosal resection to preoperative chemo / radiotherapy , strongly recommended for locally 1 3 174 radiol med ( 2016 ) 121 : 173180 advanced cases [ 4 , 5 ]  . 
nevertheless , early tumour invasion of the adjacent structures is frequent and curative resection is possible only in a small percentage of patients at the time of presentation , particularly in western countries where screening is not widespread [ 4 ]  . 
 [ 22 ] have correctly emphasised the need of more clarity regarding the application on dwi in oesophageal cancer . hence , the purpose of this report was to provide our personal experience related to dwi in oesophageal cancer . 
we investigated the role of adc as a potential prognostic biomarker of this tumour . materials and methods this single - centre , prospective study followed the standards for reporting of diagnostic accuracy ( stard ) guidelines . 
of signalsb axial , sagittal shortest axial 2400 150a axial axial single heartbeat shortest shortest overcontiguous slice 104a tr repetition time , te echo time , ss single - shot , ssepi single - shot echo - planar imaging , dwi diffusion weighted imaging . 
gastric distension was obtained by oral administration of 500 ml of water and ferumoxsil ( lumirem ; guerbet , roissy cdg cedex , france ) to investigate siewert i tumours . 
in the absence of contraindications , an intramuscular injection of scopolamine - butylbromide ( 20 mg , buscopan , boehringer ingelheim gmbh , ingelheim , germany ) was administered after patient positioning . 
according to the literature [ 14 , 26 ] , we performed ( table 1 ) a t2 - weighted study , with and without fat suppression , followed by dwi ( b : 0 and 600 s / mm2 ) and a dynamic t1 - weighted study with fat suppression during intravenous injection of 0.1 ml / kg of body weight of gadobutrol ( gadovist , 1 mmol / ml ; bayer schering pharma , berlin , germany ) with an automatic injector ( spectris mr , medrad europe , maastricht , the netherlands ) at a rate of 2 ml / s . cardiac and respiratory triggering was applied . total imaging time was approximately 40 min . image analysis two designated radiologists , with 21 and 6 years of experience in abdominal imaging , respectively , reviewed independently all the scans . both readers were privy only to tumour location . 
care was taken to avoid necrotic areas in dwi , contouring only the enhanced pathological tissue identified on the dynamic study . the anatomical appearance of oesophageal wall layers and depth of infiltration ( t ) were evaluated according to earlier studies [ 27 , 28 ]  . 
on t2 - weighted mr images , the mucosa shows high - signal intensity , the muscularis propria is seen as a discrete low - signal intensity band and the adventitia shows a high - signal intensity . 
the axial t2 image a shows a pathological wall thickening ( arrow ) , corresponding to the hyperintense ( b ) and hypointense ( c ) image on dwi and adc map , respectively . 
mean adc value was 0.79 3 mm2 / s 10 only deaths from oesophageal cancer were considered dwmr imaging statistical analysis patient survival was determined from the date of dw - mri evaluation to the most recent follow - up examination ( the database was locked on the 31 december 2013 ) or patient death . for the purposes of the study . continuous variables are presented as mean standard deviation and categorical data are presented as frequencies and percentages . inter - observer consensus and agreement in measuring adc values were evaluated by means of the spearmans correlation coefficient and the intraclass correlation coefficient ( icc )  . 
confidence intervals ( cis ) at level 0.95 were evaluated by bootstrap with adjusted percentile . differences in the mean adc between the two subgroups ( surgery - only and chemo / radiotherapy ) were analysed using mannwhitney u test . the adc optimal cut - off was determined by using the best prognostic cut - off approach and considering patients survival ( log - rank statistic ) as the dependent variable . survival curves were fitted by means of the kaplan meier estimator and the log - rank test was used to verify differences between curves . all the survival analyses were performed considering both the whole set of patients and , separately , those subjects undergoing immediate surgical resection or neo - adjuvant therapy before surgery . exact p values were computed by means of permutations to avoid any distributional assumption or asymptotic approximation . 
the top solid line shows the upper 95 % limit of agreement and the bottom solid line shows the lower 95 % limit of agreement , with the mean difference between the longaxis and short - axis measurements ( 1.96 times the standard deviation )  . 
 [ 30 ] suggested that an adc value of 3 mm2 / s during neo - adjuvant treatment ( at the 1.00 time of 20 gy ) could be of use to estimate the outcome after chemo / radiotherapy for squamous cell carcinomas [ 30 ]  . another recent study by wang et al . 
secondly , a significant lower initial 1.4 adc is found in patients treated with chemo / radiotherapy compared to the surgery - only group , supporting the idea of different treatments according to pre - treatment adc values . overall , all the aforementioned results emphasise the fundamental importance of tailoring therapy to the individual patient with oesophageal cancer . therefore , our results give further evidence to the potential role of dwi in the management of oesophageal cancer and strengthen the importance of pre - treatment mr imaging as an important diagnostic tool for this disease . we acknowledge that the small population , mainly due to our restrictive exclusion criteria , represents the major limitation of our study . owing to this fact , we believe that non - significant results ( such as the prognostic role of adc in the chemo / radiotherapy group ) are primarily attributable to the scarce number of patients ( n 9 ) ; however , these findings are promising and should deserve confidence . furthermore , another important limitation is represented by the lack of standardised dw - mri protocols for oesophageal cancer , with particular regard to the use of proper b values . 
our protocol included b values of 0 and 600 s / mm2 , as already reported in the literature [ 14 , 19 , 28 ] but , as an example , other studies [ 20 , 30 ] were performed using b values of 0 and 1000 s / mm2 . 
therefore , the choice of a standardised b value is crucial for the reproducibility of adc calculation and further studies should address this issue , using more than two b values . finally , an adequate multivariate analysis would require a higher number of patients . 
on the article tissue gadolinium deposition in hepatorenally impaired rats exposed to gdeobdtpa : evaluation with inductively coupled plasma mass spectrometry ( icpms ) by tomohiro sato , tsutomu tamada , shigeru watanabe et al . 
first , regarding the time point for tissue sampling and the gd analysis , we administered gd - eob - dtpa 12 times over a period of 6 weeks , and then , performed tissue sampling and the gd analysis 7 days after last gdeob - dtpa administration . 
clinical studies showed that the onset of nsf was approximately 210 weeks after gd contrast agent exposure , and that the median time to onset was 25 days to 5 weeks [ 1 , 2 ]  . 
therefore , considering possible onset timing of clinical nsf , we performed the gd analysis in 7 weeks ( later than 5 weeks ) after the first gd - eob - dtpa administration . 
 [ 3 ] , it was pointed out that chelated and unchelated gd might be mixed in tissue gd deposition analysis in 7 days after the last gd - eob - dtpa administration ( 7 weeks after the first gd - eob - dtpa administration )  . 
although there may be that possibility , we believe that our results could provide additional information regarding probable unchelated tissue gd deposition to the organs and nsf onset at this time point . 
we would like to consider the investigation of tissue gd deposition during longer time periods using the hepatorenally impaired rats in the future study . secondly , regarding gd - eob - dtpa excretion kinetics , pharmacokinetics of gd - eob - dtpa in hepatorenally impaired rats may not be fully verified . 
however , in our previous study of tissue gd deposition after the gbca expose in renally impaired rats [ 5 ] , the tissue gd deposition after gd - eob - dtpa administration was small as compared to other gbca , indicating that compensatory hepatobiliary excretion functioned through the dual excretion pathway specific for gd - eob - dtpa . 
the present study suggested that the tissue gd deposition after gdeob - dtpa administration increases in the hepatorenally impaired rats because of the impairment of this compensatory mechanism . finally , regarding gd - eob - dtpa dose , injection doses of gd - eobdtpa were determined with reference to animal experimental setups reported previously by pietsch et al . 
high - dose injections in this experimental study were used to simulate prolonged exposure to gd - eob - dtpa , as occurs in clinical cases of renal impairment . in conclusion of this study , after the gd - eob - dtpa exposure , the gd content in the kidneys , spleen , and liver was significantly higher in hepatorenally impaired rats , compared to renally impaired rats , possibly leading to unchelated tissue gd deposition . 
these results suggested that a careful use of gd - eob - dtpa will be recommended in hepatorenally impaired patients although our experimental data may not be directly applied to the clinical practice . 1 3 radiol med ( 2016 ) 121 : 240241 compliance with ethical standards 2 . 
in none of the three cases , the lesions showed any clinical correlate and eventually presented a striking reduction in size while gadolinium enhancement disappeared despite no specific therapy administration during the follow - up . 
hitherto , a similar behavior has been described only in scattered cases and we believe these findings may be of particular interest for the clinical management of patients affected by neurofibromatosis type keywords neurofibromatosis type 1 gliomas gadolinium lesions magnetic resonance imaging * marta lucchetta lucchetta.marta@gmail.com 1 clinical genetics unit , department of woman and child health , university of padova , via giustiniani 5 , 35128 padua , italy 2 neuroradiology , university of salerno , salerno , italy irccs s . 
camillo , venice , italy 4 paediatric residency program , department of woman and child health , university of padova , padua , italy neurofibromatosis type 1 ( nf1 ) is one of the most common autosomal dominant conditions [ 1 ] and it is caused by loss of function mutations in the tumor suppressor gene nf1 [ 2 ]  . the hallmark of this condition is neurocutaneous involvement . 
central nervous system manifestations are very common and frequent mri findings in patients with nf1 include possibly hazardous optic pathway gliomas ( opg ) [ 3 ] and brainstem astrocytomas [ 4 , 5 ]  . 
nevertheless , these lesions show a more indolent course compared to sporadic ones and they may also spontaneously regress [ 68 ] ; a wait and see approach is therefore frequently applied by clinicians [ 6 ]  . brain t2 - hyperintense areas without gadolinium enhancement are observed in up to 90 % of nf1 patients usually within the globus pallidum , the brainstem and the cerebellu these lesions , that are considered regions of dysmyelination , are called ubos ( unidentified bright objects ) and they usually disappear during or after the second decade and have minimal or no clinical impact [ 9 ]  . gadolinium - enhancing lesions have been also reported in patients with nf1 ; they have undetermined nature and behavior and raise the suspicion of a potentially life - threatening glial tumor . 
however , they have been poorly studied and their disappearance has been described just in few scattered cases [ 1013 ]  . here , we present three nf1 patients whose mri followup showed the regression of gadolinium - enhancing lesions . all patients were diagnosed nf1 according to the international criteria [ 14 ] ; they all displayed the typical neurocutaneous feature of nf1 with presence of an opg or optic nerve thickening . 
mri scans revealed the appearance of 1 3 radiol med ( 2016 ) 121 : 214217 1 3 216 radiol med ( 2016 ) 121 : 214217 a small gadolinium - enhancing lesion in the left cerebellar peduncle ( patient #1 ) , in the left cerebral peduncle ( patient #2 ) and in the inferior portion of the right parietal lobe ( patient #3 )  . 
in the first case , lesion regression developed after an initial enlargement ( from 3 to 7 mm ) , followed by a 10 - year period without changes ; in the other two cases , the lesions regressed after a shorter period ( one and 3 years , respectively )  . 
in these rare cases , the lesions , which involved the brainstem [ 11 ] or the forebrain [ 10 , 12 , 13 ] showed a spontaneous regression during the follow - up without therapy administration or clinical changes . in our cases , the disappearance of the gadoliniumenhanced lesion occurred in a short period of time in 2 out of the 3 nf1 patients , as in previously reported cases [ 10 ] , but unlike the patients with spontaneous involution of nonoptic gliomas [ 7 , 8 ]  . gadolinium enhancement represents a marker of blood brain barrier breakdown , but it does not always demonstrate the presence of tumor activity [ 15 ]  . 
our cases and the few already reported [ 1013 ] illustrate how also malignantlooking lesions may have unexpected positive evolution . in patients affected with nf1 , who can manifest both benign lesions as ubos and proliferative glial tumors , clinical management may be challenging and the appearance of gadolinium - enhancing lesions may lead to an aggressive therapeutic approach . hence , in our opinion , these findings may play a role in the clinical management of patients affected by nf1 and suggest that the wait and see approach might be applied also in cases of enhancing lesions outside the optic pathway and the brainstem . follow - up , fig . 
upper row at the age of 12 , axial ( a ) and coronal ( b ) images show an enhancing lesion involving the left cerebral peduncle ; middle row at the age of 13 , the midbrain lesion has disappeared ( c ) while a new enhancing lesion is evident in the white matter of the left temporal lobe ( d )  . 
dwi may detect renal failure prior to a rise in creatinine . keywords diffusion - weighted imaging kidney failure renal function introduction early diagnosis and treatment are the cornerstone of slowing down the progression of chronic kidney disease ( ckd )  . 
between june 2012 and february 2013 , for a total of 8 months , 62 patients with ckd were included in this retrospective study . firstly , the cr cl of the patients was detected with 24 - h urine collection . 
the patients were divided into groups classified by their progression through the five stages of ckd according to the definition of the kidney disease outcome quality initiative ( k / doqi ) ckd ( table 1 )  . in the same week , abdominal mris with dwi were obtained . 
serum creatinine starts to increase after 50 % of the renal function is lost 186.3 scr ( mg / dl ) 1154 age0.203 mri technique split renal function cannot be assessed with these methods as well . there is neither a noninvasive nor a quantitative radiological method that detects ckd at an early stage . ultrasonography cannot detect very early kidney function deterioration and is user dependent . 
computerized tomography ( ct ) scanning and intravenous pyelography ( ivp ) are also not widely accepted techniques to evaluate renal function because of the nephrotoxicity of the contrast agents and the radiotoxicity produced by the procedures . 
however , it was reported that gadolinium - based contrast agents may cause systemic nephrogenic fibrosis when used in patients with severe ckd [ 510 ]  . recently , diffusion - weighted imaging ( dwi ) , which is a sequence obtained using mri without the need for contrast material injection , provided promising results , especially in oncologic imaging , inflammatory conditions , and early ultrastructural changes in the abdominal organs . 
before dwi , axial 3d fat - saturated t1 - weighted spoiled gradient - echo liver acquisition with volume acqui4.5 ms , echo time sition ( lava ) ( repetition time [ tr ] 38 cm , [ te ] 192 ) , axial breath - hold fs - fse t2 - weighted matrix 2100 ms , te > 100 ms , thickspatial fat saturation ( tr 90 , acquisition ness 1 , acquisition matrix 2d ) , axial t1 - weighted fast spoiled gradient - recalled type 2.1 ms echo dual - echo ( fspgr - de ) ( tr and 4.3 ms , flip angle 43 cm , 192 ) , coronal t2 - weighted single - shot matrix 90 ms , flip 2625 ms , te fast spin - echo ( ssfse ) ( tr angle 192 , 200 40 cm , matrix 40 breath - hold , images ) , and axial dwi under normal breathing were applied using a single - shot echo - planar imaging 90 ms , sequence in axial orientation ( tr field of view 2 ; 41 160 ; nex bandwidth slice , slice thick1.0 mm with b values of 50 , 5.0 mm , interscan gap ness 500 , and 1000 s / mm2 , acquisition time 54 s )  . 
isotropic dwi was generated using three orthogonal - axis images and by combining the diffusion signal from all three vectors . 160 41 cm ; matrix 250 khz , diffusion direction 130 ms , te 43 70 , field of view 90 , field of view 12 , 000 ms , te 320 1 3 radiol med ( 2016 ) 121 : 163172 b values the dwi sequence was performed three times with very low , low , and high b values ( 50 , 500 , and 1000 s / mm2 ) to determine the effect of the b value . 
normal tissues and water molecules display normal diffusion ; however , tissues like damaged renal parenchyma reflect restricted diffusion since there is loss of water molecules and decreased extracellular space . 
this effect becomes more conspicuous with a higher b value . sequence details were as follows : bandwidth 250 khz , fov 41 cm , section thickness 5 mm , intersection gap 1 mm , nex 2 , matrix 160 160 . 
the adc maps were produced at a different workstation ( advantage workstation 4.4 - ge medical systems ) using a software program ( functool )  . interpretation of the images the images of the patients were extracted from pacs , and evaluation was done on the workstation after the transfer of the images . 
the two radiologists completely agreed with each other . the visibility of the parenchymal focal lesions and the corticomedullary differentiation was examined after the renal dimensions were measured in the conventional sequences . 
 adc maps were acquired automatically by the software program at the workstation ( functool , ge medical systems )  . quantitative measurements were performed on the adc maps from the upper , middle , and lower sections of each kidney in agreement . 
rois were inserted in the cortex excluding medulla on the coronal maximum intensity projection ( mip ) image . in subjects with poor corticomedullary differentiation , rois were placed on the outer one - third region of the renal parenchyma , corresponding to the kidney contours . 
differences were considered to be significant when the two - tailed p value was less than 0.05 with a 95 % confidence interval . results a total of 62 patients and 124 kidneys were included in the study . 
out of all the patients , 26 ( 41.9 % ) had diabetes mellitus , 19 ( 30.6 % ) had hypertension , and 7 ( 11.3 % ) had chronic glomerulonephritis . 
the etiology of ckd in 10 ( 16.1 % ) of the patients was unknown . the mean adc values for the right and left kidneys according to the cr cl stages of the patients are shown in tables 2 and 3 , respectively . 
the degree of diffusion in an organ is denoted as adc [ 12 ]  . in the case of the kidneys , the dw images are also influenced by the water content of the kidneys , renal perfusion , and renal blood volume [ 12 ]  . additionally , the intrarenal physiologic processes , such as blood flow , tubular flow , and water content , may change the adc [ 12 , 13 ]  . stage 1 kidney disease includes very small changes either in structures or in function , so usually no disturbance can be detected in kidneys . 
however , adc values allowed the differentiation of stage 1 of the disease from the other stages . it seems from the results that the adc value at all b values is good at differentiating stage 1 cr cl from stage 2 , yet this is only a minor drop in egfr . 
 [ 14 ] investigated the reliability of dwi in the evaluation of normal kidney and above - mentioned lesions of the kidney . in our study , measurements , as suggested by cova et al . 
it should be in the center of the corticomedullary junction and in the middle of the kidneythe part that is affected the least . the cortical adc was found to be higher than the medullary adc presumably because of the higher perfusion 1 3 168 radiol med ( 2016 ) 121 : 163172 fig . 
 [ 18 ] , a b value of 500 s / mm2 has been used for the assessment of patients with mild , moderate , and advanced renal failure and normal volunteers kidneys . 
in these four groups , there was a positive correlation between the adc values and the gfr . essentially , we provided cr cl by 24 - h urine collecting and used five stages according to k / doqi . xu and his colleagues used the cockcroftgault formula and therefore defined three groups . 
 measurement of the adc value with round rois from the upper and lower poles and mid - zone of the kidney a coronal dwi image of the right kidney with b 1000 s / mm2 , b coronal adc map of the right kidney , c coronal plane colored adc map of the same patient quality was adequate . 
statistically significant differences of adc values was found between stage 1 , stage 2 , stage 3 and stage 45 values at high b value dwi ( 1000 s / mm2 )  . 
they found that only the average adc values of the patients with gfr < 30 ml / min / 1.73 m2 were markedly lower than the other groups , but the difference was not significant . 
they reported that failure to find a significant difference could be due to the small changes in the renal function compared with only gfr values [ 19 ]  . in the present study , which used cr cl , we found a precise relation so that dwi should be used in clinical practice not only to diagnose kidney disease earlier but also to discriminate acute or chronic illness quantitatively in a single examination . 
the concept of normalized adcusing a reference organ for proportionis relatively new and has been found to improve reproducibility and reduce variability in adc measurement of the normal parenchyma and focal lesions . 
 however , potential pitfalls , such as diffuse parenchymal diseases , should be considered when using normalized adc [ 2023 ]  . in this context , even though the values of the right kidney were obtained more striking in this study , the adc values of the left kidney and the averages of both kidneys were considered to be beneficial since these 1 3 radiol med ( 2016 ) 121 : 163172 measurements were statistically significant as well . 
this heterogeneity may be due to the fact that we did not investigate the normalized adc values , as mentioned in our limitations . there are some limitations in our study . 
firstly , water restriction and the diuretic treatment were not used . since the adc is dependent on capillary perfusion and water diffusion , blood and tubular flow as well as water content may change the adc . 
water deprivation may affect water content , and diuretics can also influence renal blood flow and capillary perfusion due to vasodilation in afferent arterioles of the glomerulus . consequently , water deprivation may provide true results or avoid overestimation . 
since we did not investigate normalized adc values , it is not well known to what extent the use of normalized adc may help detect renal function impairment , and this warrants further studies . overall , the widespread use of dwi is currently hindered by the often time - consuming post - processing and by the lack of the standardization of technique . conclusion renal adc values show a significant correlation with clinical stages of ckd . we determined that there was a decrease in the average renal adc values correlating with the decreased cr cl values of the patients . 
halefoglu1 received : 25 june 2015 / accepted : 25 september 2015 / published online : 13 october 2015 italian society of medical radiology 2015 abstract introduction the aim of this prospective study was to evaluate the value of diffusion - weighted magnetic resonance imaging ( dw - mri ) in patients with osteonecrosis . 
patients were divided into two subgroups as avascular necrosis ( avn ) of femoral head for adult group and legg calvperthes ( lcp ) patients for children . patients and methods seventeen patients with femoral head avn ( mean age 42.3 years ) and 17 patients with lcp ( mean age 8.2 years ) were included in this study . 
diagnosis confirmed with clinical and other imaging procedures among the patients complaining hip padw images were obtained using the single - shot echo planar sequence and had b values of 0 , 500 , 1000 s / mm2 . 
the apparent diffusion coefficient ( adc ) values were measured from adc maps in epiphysis of patients with avn , both from metaphysis and epiphysis in patients with lcp , respectively . 
 dwi is a fast , without - contrast administration technique and provides quantitative values additional to conventional mr techniques ; we believe dwi may play an additional assistance to the diagnosis and treatment for lcp patients . 
no : 27 , okmeydan s isli , 34384 istanbul , turkey introduction diffusion - weighted magnetic resonance imaging ( dwmri ) is a non - invasive functional technique that evaluates random motion of water protons in body . 
since the water molecules show various amount of diffusion according to their interaction with cell membrane , dwi can provide additional information about the tissue characterization by quantitative analysis with the apparent diffusion coefficient ( adc ) map obtained from dw - mri [ 1 , 2 ]  . osteonecrosis means ischemia , results to death of the bone marrow cellular components . 
there are studies which report that ischemic area shows diffusion limitations and if the treatment begins at this critical period , prognosis could be affected positively in the first 72 h [ 5 , 6 ]  . furthermore , dwi is used in ischemic issues of neuroradiology efficiently , especially in early diagnosis of cerebrovascular events . 
however , there are few publications about the use of osteonecrosis [ 79 ]  . the aim of this study was to determine the utility of adc measurements of ischemic necrosis of the femoral head in both children and adult patients . materials and methods patients the study included 17 adult patients diagnosed as avn and 17 patients diagnosed as lcp in pediatric age group , those admitted to the radiology clinic , because of hip pain between may 2009 and january 2011 in our center . this study was approved by institutional ethics committee and all persons gave their informed consent prior to their inclusion in the study . 
diagnosis performed as a result of further investigation and follow - up . avn diagnosis was performed with single line sign which is diagnostic for t1w images and double line sign on t2w images . 
control group was created this way : in bilateral avn cases , metaphyseal adc values were obtained from tissue adjacent to the lesion area without any abnormal signals in conventional mri sequences . 
for unilateral affected cases , contralateral femoral head adc values were obtained . lcp diagnosis of proximal femoral epiphysis was established by monitoring of deformed appearance such as irregularity of contour , height loss , sclerotic appearance , subchondral fracture fragmentation , the existence of the loss of roundness and flattening of the femoral head . 
as a control group , contralateral epiphysis and metaphysis were evaluated for statistical analysis . in literature , there are not enough data about adc values in the normal pediatric femoral epiphysis for different age groups and early childhood of up to 5 years , which is considered to be homogeneous . 
routine mri protocol consists of t1w in the axial and coronal and t2w in the coronal and sagittal images . dwi was obtained when using single - shot echo planar imaging ( epi ) sequence in the axial plane . 
epi sequence was obtained using tr 4000 , te 76 , thickness 5 mm , section spacing of 1 mm , matrix 156 400 , nex : 3 different b value ( 0 , 500 and 1000 s / mm2 ) gradients . 192 , fov all patients were first assessed visually in terms of signal characteristics . 
specific mean adc values were obtained to make separate measurements of each lesion . for pediatric age , contralateral femoral epiphyseal and metaphyseal head normal adc values were considered as normal reference . statistical analysis data were summarized as mean standard deviation for continuous variables and frequencies for categorical variables . 
dwi has also assessed a number of musculoskeletal disorders , including vertebral fractures , bone marrow infection , bone marrow malignancy , primary bone and soft tissue tumors ; post - treatment follow - up has also been evaluated [ 10 ]  . 
discrimination between benign and malignant epi : adc a according to mitchell staging system , r right , l left , b both 10 3 mm2 / s table 2 demographic data of lcp cases and adc values case placement path . 
coronal t1 - weighted ( a ) , coronal t2 fatsaturated ( b ) , axial t1 - weighted ( c ) , axial t2 fat - saturated ( d ) images demonstrate on the right femoral head double string sign and edematous signal change in medullar bone . 
the adc value of right femoral head was measured as 1.008 3 mm2 / s ( f ) 10 vertebral fractures by dwi and following of therapy response have shown excellent results [ 10 ]  . 10 the mean adc value of muscle tissue was measured as 3 s / mm2 , the mean adc value of liver tissue 1.21.7 3 s / mm2 , respectively . 
 coronal t1 - weighted ( a ) , coronal t2 fat - saturated ( b ) , axial t1 - weighted ( c ) , axial t2 fat - saturated ( d ) images demonstrate subcortical fissure lines and adjacent medullar edematous signal changes on both femoral head superior anterior regions . 
our high adc values in accordance with the increased diffusion were similar to jaramillo and menezes s findings in the femoral head avn [ 17 , 18 ]  . correlation between adc values and stage of osteonecrosis of the femoral head is a debatable question . 
reported statistically significant increase in adc values in the pathological side and was correlated with catterall classification on their study that included 27 children with lcp disease [ 20 ]  . 
reported statistically significant increase in adc values in the pathological side and was correlated with herring classification on their study with 31 patients with unilateral involvement lcp [ 21 ]  . 
reported , pathological epiphyseal and metaphyseal femoral head adc values were significantly higher compared with control side in their study including 12 patients with 512 age group lcp [ 15 ]  . 
in our study , adc values of normal and pathological bone marrow findings were similar to those previously made studies in literature . an increase in interstitial bony fluid occurs in bone marrow edema ( bme )  . 
3 adc values of the normal bone tissue and avn bone lesions study statistical comparison between the phases of disease because we did not have any patient with stage b . 
coronal t1 - weighted ( a ) , coronal t2 fatsaturated ( b ) , axial t1 - weighted ( c ) , axial t2 fat - saturated ( d ) images demonstrate contour irregularity and height loss on the left epiphysis . 
multicenter studies including many patients can make contribution to this issue . compliance with ethical standards conflict of interest author betul duran ozel md declares that she has no conflict of interest . 
 to analyze how often lm can be visualized by high - resolution heavily t2 - weighted 3d - mri prior to etv , and to find out potential reasons for diagnostic failure . materials and methods preoperative 3d - mr images of 37 consecutive patients ( 19 female , median 42 years ) were retrospectively analyzed . 
preoperative imaging findings were compared with intraoperative findings . results patients were subdivided into group 1 ( no segment of lm identified , n 18 ) , and group 2 ( at least one segment of lm was identified , n 19 )  . 
other variables , such as the distance between tip of the pons and the mamillary bodies as well as the image quality , were not significantly different between both groups . 
operative failure , serious complications or stoma failure may occur if an unnoticed membrane below the floor of the third ventricle is present , such as liliequists membrane ( lm ) [ 1 , 2 ]  . 
microsurgical studies [ 4 , 5 ] revealed that lm frequently comprised two layers , a mesencephalic and 1 3 radiol med ( 2016 ) 121 : 200205 diencephalic membrane . 
they reported that at least one segment of lm can be visualized by 3 - d - ciss ( constructive interference steady state ) - mr in more than 80 % of healthy volunteers without signs of hydrocephalus [ 6 ]  . 
in another ciss - mr study , the authors found complex basal and pontine membranes in 19 of 42 ( 45 % ) patients with hydrocephalus prior to etv [ 1 ]  . 
 unfortunately , the authors did not analyze the morphology and visibility of these membranes more in detail . our purpose was to analyze how often lm can be visualized by 3d - ciss - mri prior to etv , and to find out potential reasons for diagnostic failure . materials and methods patients we retrospectively analyzed preoperative mr imaging of 37 consecutive patients ( 19 female , 18 male , median 42 years , range 177 years ) suffering from obstructive hydrocephalus caused by aqueductal stenosis and scheduled for treatment with etv within days . 
imaging was performed using a 1.5 - tesla mr imaging system ( magnetom vision ; siemens healthcare , erlangen , germany ) with a regular ( quadrature ) head coil . 
 [ 6 ] , a qualitative threescore scale was used for identification of the three segments of lm : 0 highly probable identification and 2 positive identification . no identification ; 1 3 . 
2 left ( a ) sagittal ciss image obtained in a 66 - year - old male shows the sellar and diencephalic segments of liliequists membrane ( arrow )  . 
right ( b ) in a 38 - year - old female with an obstructive hydrocephalus caused by an obstruction of the foramina of luschka and magendie , all three segments of liliequists membrane are visible . 
 the mesencephalic segment spreads from the dorsum sellae to the pons ( arrow head ) , while the sellar and diencephalic segments spread from the dorsum sellae to the mamillary bodies ( small arrow ) .in both cases , psd and msd were 6 mm and image quality was scored as excellent lm as well the accuracy of measurements , image quality was scored by a qualitative three - score scale : poor ( 1 ) restricted delineation of anatomical structures due to artificial blurring of the anatomical edges , but examination still diagnostic ; moderate ( 2 ) slightly restricted delineation of anatomical structures due to minor to modest artifacts ; excellent ( 3 ) clear delineation of all anatomical structures of interest , no artifacts . equality of variances was tested with levenes test . 
no patient fulfilled the criteria of a long - standing overt ventriculomegaly in adults ( lova ) [ 7 ]  . patients were subdivided into two groups : group 1 , no segment of lm identified , and group 2 , at least one segment of lm was positively identified or highly probably identified . the baseline characteristics of both groups and of the mr image quality are given in table 1 . 
no significant difference between both groups was found for the diameters of the third ventricle ( table 3 )  . operative reports were available in all but one patient of group 2 . 
in 14 out of 18 ( 78 % ) patients of group 2 , an arachnoid membrane below the third ventricle was to our knowledge , this is the first study systematically evaluating the visibility and potential findings for failure of visualization of lm by 3d - ciss - mri in patients prior to etv . 
furthermore , the dimension of the space below the floor of the third ventricle ( represented by the mpd ) and the 3d - ciss - mri image quality were also important but not statistically significant parameters for lm visualization in our series . 
 we used the same subdivision of the lm into three segments ( sellar , mesencephalic , diencephalic ) as fushimi and co - workers [ 6 ] and found at least one segment of lm in 19 out of 37 ( 51 % ) patients with obstructive hydrocephalus prior to etv . 
the conflicting results on the incidence of lm might be accounted for by several reasons : first , lm is described as an inconsistent and variable arachnoid layer [ 4 , 10 ]  . 
for instance , there is disagreement on the exact superior and lateral attachment of lm in the literature , while the dorsum sellae is widely accepted as the lower attachment [ 3 , 5 , 10 ]  . 
considering this , even radiological findings are limited , too , since , due to the given spatial resolution of the 3d ciss - mri , it is not possible to reliably measure structures with a size of 1 3 radiol med ( 2016 ) 121 : 200205 lm visible on mri ( group 2 ) lm not visible on mri ( group 1 ) 204 fig . 
indication and preoperative imaging including the precise location of the basilar and posterior cerebral arteries in relation to the planned stoma are essential for avoiding intraoperative complications such as arterial damage [ 12 ]  . 
a successful stoma was cre1 m ated in as many as fifteen patients with a ppi of similarly , psd ranged from 0 to 13 mm ( mean 4.9 mm ) in our series . 
 [ 14 ] measured the distance between the infundibular recess and the tip of the basilar artery in 271 subjects ( mean age 54.7 years ) without intracranial disorders , and in 8 patients with hydrocephalus by conventional mri . 
conversely , we and the group of souweidane [ 13 ] observed considerable differences in the dimensions of the space below the floor of the third ventricle in patients with hydrocephalus prior to etv . 1 3 radiol med ( 2016 ) 121 : 200205 apart from neuroanatomical discussions , understanding the anatomy of lm is essential for clinical neuroradiologists and radiologists , too . 
 most likely , the hemorrhage is frequently confined to the prepontine and interpeduncular cisterns by the anatomy of lm [ 6 , 10 , 15 , 16 ]  . in accordance with previous imaging studies on the value of 3d - ciss , we could show that a complex membranous structure located in the subarachnoid space can be reliably and clearly visualized by this high - resolution mr technique [ 1 , 6 , 12 ]  . 
nevertheless , lm is an inconsistent finding and of variable anatomy in patients prior to etv . compliance with ethical standards conflict of interest the authors declare that there is no conflict of interest . research involving human participants and / or animals for this type of study formal consent was not required . informed consent prior to detailed retrospective evaluation , all patient data were carefully anonymized , so that neither backtracking of personal data was / is possible nor identifying information about participants are available . 
to evaluate radiological involvement , the semi - quantitative evaluation proposed by warrick was used to assign a score for each lesion based on the severity and extent of the pulmonary damage . 
considering also the subclinical course of the disease , such factors unfavorably affect the disease monitoring , follow - up of abnormalities and early treatment decisions [ 7 ]  . 
the initial stage in the natural 1 3 182 radiol med ( 2016 ) 121 : 181189 course of ra - associated ild includes active alveolitis which is characterized by acute inflammation ; if treated quickly and adequately , this stage may be reversible . 
high - resolution computed tomography ( hrct ) allows such differentiation and also has a number of advantages including its non - invasive nature , it has also the ability to detect the extent of the disease and to provide early findings with a very good assessment of parenchyma [ 8 , 9 ]  . 
in the present study , we aimed to establish risk factors for radiological lung damage associated with ra and to determine whether clinical findings and pfts were correlated with warrick score calculated on the basis of hrct . materials and methods study population a hundred and thirty patients meeting the 1987 american college of rheumatology classification criteria for rheumatoid arthritis [ 11 ] who were seen and followed at the rheumatology outpatient clinic between january 2009 and january 2012 were included in the study through retrospective screening if they ever had a hrct scan for any reason . 
forced vital capacity ( fvc ) , forced expiratory volume in 1 s ( fev1 ) , total lung capacity ( tlc ) and diffusing lung capacity for carbon monoxide ( dlco ) were measured and expressed as a percentage of the predicted value . 
abnormal results were recorded when % 75 of predicted valfvc , fev1 , dlco or tlc were ues [ 12 , 13 ]  . hrct study patients underwent chest hrct with a 64 - detector scanner ( aquillion 64 ; toshiba medical systems , tokyo , japan ) in supine position with full inspiration without contrast enhancement . 
scanning parameters were as follows : 120 kv , variable mas according to the patient size using an automatic exposure control system , slice thickness 1 m the images were reconstructed in a 512 512 matrix with 1 mm non - overlapping slices , applying a standard hrct reconstruction algorith prone scans limited to the lung bases were obtained when there were ground - glass opacities in the posterobasal subpleural region to exclude gravitational opacities . 
each elementary lesion has its own quantitative point value and a total severity score was generated by summing the values for each lesion observed on hrct images [ 10 ]  . 
1 a high - resolution computed tomography scan at the subcarinal level shows bilateral ground - glass opacities ( arrows ) that are hyperdense compared to normal parenchyma and have hazy borders . 
d in the left column , early honeycombing can be seen as small , thick - walled cystic spaces arranged in multiple concentric layers in the subpleural region at the lung base ( white arrow )  . 
e hypodense , thin - walled and single - layered cystic structures at the lung bases are consistent with subpleural cysts ( asterisks ) we assessed the extent score of each patient according to the number of segments involved for each elementary lesion . 
each lesion type was assigned a score from 1 to 3 where 1 indicated that the lesion is present in one to three segments , 2 indicated that the lesion is present in four to nine segments and 3 indicated that the lesion is present in more than nine segments [ 10 ]  . 
 since radiological ground - glass pattern correlates with alveolitis in most of the cases , an alveolitis index was calculated by summing the severity ( 01 ) and extent ( 03 ) scores of ground - glass opacities [ 8 ]  . 
the severity and extent scores of the remaining four elementary lesions ( irregularities in the pleural margins , septal lines , honeycombing and subpleural cysts ) which primarily indicate parenchymal 1 3 table 1 criteria used for calculating the warrick score8 , 10 lesions and lung segments score the multivariable logistic regression analysis ( backward , conditional )  . 
all tests were two - sided and the level of statistical significance was set at p < 0.05. radiol med ( 2016 ) 121 : 181189 184 parenchymal abnormalities ground - glass opacities irregularities in the pleural margins septal / subpleural lines honeycombing subpleural cysts disease severity score results number of lung segments disease extent score demographic and clinical characteristics of ra patients demographic and clinical characteristics of ra patients are summarized in table 2 . 
 there were 100 patients ( 80 % ) with rheumatoid factor ( rf ) positivity and 72 ( 67 % ) with anti - cyclic citrullinated peptide antibody ( anti - ccp ) positivity . 
the sum of the two scores formed the fibrosis index which ranged from 0 to 26 [ 8 ]  . statistical analysis statistical analyses for the present study were conducted using spss for windows 20.0 ( spss , chicago , il , usa ) software package . 
for between - group comparisons , independent t test was used for normally distributed numerical variables and categorical variables were analyzed using chi - square test for or fishers exact test where appropriate . 
spearmans test was used to calculate correlation coefficients and statistical significance for associations between variables when at least one of the variables was ordinal or showed non - normal distribution . 
curve estimation is a curve - fitting program that can be used to compare and select suitable curve relationships ( such as linear , logarithmic , inverse , compound and so on ) to illustrate the relationships between variables , which are illustrated in figures with r values . 
17 patients ( 13 % ) had ground - glass density , 55 patients ( 42 % ) had irregularities in the pleural margins , 40 patients ( 31 % ) had septal / subpleural irregularities , 15 patients ( 11.5 % ) had honeycombing appearance and 3 patients ( 2.3 % ) had a subpleural cyst . 
2 relationship between warrick score and age at study onset values are expressed as mean cated sd or n ( % ) unless otherwise indifev 1 forced expiratory volume in 1 s ; fvc forced vital capacity , dlco lung diffusion capacity for carbon monoxide , tlc total lung capacity , hrct high - resolution computed tomography fig . 
all risk factors associated with radiological lung damage were included in the univariate logistic regression analysis and variables with a p value below < 0.10 were included in the multivariate logistic regression analysis . 
in addition , given the association of warrick score with clinical findings and pfts as shown in our study , it is considered that this semiquantitative method might provide additional information for assessment of pulmonary damage in ra . hrct is a valuable non - invasive imaging method to detect the presence , type and extent of pulmonary abnormalities and also to determine prognosis and evaluate the response to treatment [ 14 , 15 ]  . 
 [ 19 ] this variability may be explained by differences in inclusion and exclusion criteria . advanced age [ 2022 ] , increased disease activity [ 23 ] , rf positivity [ 21 ] , anti - ccp antibody positivity [ 24 ] and male sex [ 25 , 26 ] were all reported to be associated with increased prevalence of pulmonary involvement of ra . 
 dyspnea has been reported as the most common symptom [ 27 ] and a considerable association was shown between pulmonary involvement and presence of respiratory symptoms in ra patients [ 27 ]  . 
in our study , the group with abnormal hrct findings had a greater number of male patients and patients at an advanced age who reported a higher occurrence of respiratory symptoms . 
in addition , in the current study , we showed that advanced age , dlco % predicted values below 75 % and presence of respiratory symptoms were independent risk factors for radiological lung damage . 
also , a significant correlation was found in the present study between warrick score and age , presence of respiratory symptoms and rf positivity . few studies exist in literature that explored associations between pfts and morphological changes detected by hrct in ra [ 21 ]  . 
in retrospective studies with a small number of patients , ra - ild presence was shown to be associated with restrictive pft pattern and decreased percent - predicted dlco [ 16 , 29 ]  . 
in a separate study , a dlco % predicted value below 54 % was reported to be an independent predictor for progression of ild in ra [ 30 ]  . 
this suggests that hrct abnormalities may also develop in the early stages of disease process in ra . the majority of ra patients in our study were on longterm methotrexate monotherapy or combination therapy with biological agents . 
our study results are similar to those reported by other studies in literature which reported no association between pulmonary damage and treatment in ra [ 21 , 33 , 34 ]  . 
contrastingly , a recent meta - analysis reported a small but significant risk for increased pulmonary damage in ra patients receiving methotrexate compared to ra patients using 1 3 188 radiol med ( 2016 ) 121 : 181189 other dmards or biological agents [ 35 ]  . 
thus , in the context of our study results , pulmonary damage induced by methotrexate toxicity seems to be a confounding factor . smoking was shown to be associated with ild development in ra patients . 
 although we could not demonstrate an association between smoking and warrick score , smoking appears to be another confounding factor in our study since there was limited information on the amount and duration of exposure . remy - jardin et al . 
 [ 37 ] have reported that among patients without honeycombing on hrct , those who displayed ground - glass density had lower percent - predicted dlco values versus those who did not . 
it was reported that patients with limited honeycombing ( < 15 % ) could still have normal spirometry values but those with diffuse honeycombing exhibited restrictive pattern as shown by spirometry [ 37 ]  . 
consistent with literature , impaired gas exchange was shown using lower dlco % predicted in subclinical ra - ild in the current study but pfts were found to be a non - sensitive method for diagnosis of subclinical raild [ 38 ]  . our study has several limitations mainly attributed to its retrospective design . 
second , there was a significant bias in patient selection as all subjects had clinical indications for ct scans , although many of these indications were unrelated to the diagnosis of interstitial lung disease , i.e. , a lung nodule or chest pa third , not every subject included in this study who had a ct scan had pft data available , adding another source of bias and limiting the generalizability of the results . 
lastly , the limited number of subjects with data available for this study hindered our ability to perform multivariate analyses adjusting for such confounders as ra disease severity , comorbidities , and medication - induced pulmonary changes . since the majority of study patients were asymptomatic , a high prevalence of asymptomatic pulmonary lesions was found based on hrct findings . 
it is considered that this semi - quantitative method may add value in early diagnosis , appropriate treatment decisions and follow - up when taken into account together with risk factors associated with pulmonary damage in ra . compliances with ethical standards funding support there was no funding support in this study . conflict of interest baris yilmazer declares that he has no conflict of interest . 
ayse cefle declares that she has no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent ual participants included in the study . informed consent was obtained from all individradiol med ( 2016 ) 121 : 229237 doi 10.1007 / s11547 - 015 - 0586 - 1 radiotherapy prognostic factors in patients with locally advanced head and neck cancer treated with concurrent radiochemotherapy davide franceschini1 , 3 fabiola paiar1 calogero saieva2 pierluigi bonomo1 benedetta agresti1 icro meattini1 daniela greto1 monica mangoni1 fiammetta meacci1 mauro loi1 giacomo zei1 lorenzo livi1 giampaolo biti1 received : 6 november 2013 / accepted : 19 march 2014 / published online : 24 september 2015 italian society of medical radiology 2015 abstract purpose this study was undertaken to evaluate the association of individual parameters and outcome in patients with unresectable locally advanced head and neck cancer treated with radiochemotherapy . materials and methods we retrospectively reviewed data from 126 patients treated in our institution between 1998 and 2010 for a locally advanced head and neck cancer . 
sixteen individual parameters were evaluated for association with specific outcomes such as overall survival , persistence of disease , disease - specific survival and disease - free survival . results six factors influenced overall survival on kaplan meier survival analysis and on univariate cox regression analysis : smoking , body mass index , site , haemoglobin ( hb ) nadir , total dose of radiotherapy and comorbidities . 
only performance status maintained the significance on multivariate * davide franceschini davide.franceschini@unifi.it 1 department of radiation - oncology , university of florence , florence , italy 2 molecular and nutritional epidemiology unit , cancer research and prevention center ( ispo ) , florence , italy 3 department of radiotherapy , university of florence , largo g.a. 
disease - specific survival was correlated with five parameters : body mass index , site , hb nadir , therapy interruption and total dose ; on multivariate analysis , hb nadir , therapy interruption and site maintained a statistically significant association . conclusions hb nadir during treatment , body mass index , smoking , stage , comorbidities and performance status are prognostic factors of outcome and response to radical treatment with radiochemotherapy . keywords prognostic factors head and neck oncology radiation therapy introduction the incidence of head and neck ( h&n ) cancer has significantly increased over the past decade , representing today the sixth most common cancer worldwide . 
the management of head and neck squamous cell carcinoma ( hnscc ) is often a clinical challenge , since in more than 60 % of patients , the disease is locally advanced at diagnosis : a combined modality therapy with surgery , radiotherapy ( rt ) and chemotherapy ( cht ) is generally recommended [ 1 , 2 ]  . 
when the disease is deemed unresectable or an organpreservation goal is pursued , the current standard treatment is represented by the combination of radiation and chemotherapy ( rt - cht )  . 
 in recent years , several published studies [ 3 ] and metaanalyses [ 4 , 5 ] have shown that aggressive protocols such as cisplatin - based rt - cht and altered fractionated radiotherapy determine a significant improvement in outcome in terms of overall survival ( 8 % at 5 years ) compared to 1 3 230 radiol med ( 2016 ) 121 : 229237 conventionally fractionated radiotherapy alone . 
however , it has also been shown that the inherent advantage in intensified treatment modalities , in particular concomitant rt - cht , comes at the expense of enhanced acute and late toxicity . 
in current practice , cisplatin - based rt - cht cannot be considered the most suitable choice for every patient affected by locally advanced hnscc : careful patient selection is essential to maximise the therapeutic ratio related to this combined therapy . 
in h&n oncology , the lack of welldefined prognostic and predictive factors limits the possibility to tailor the best therapeutic approach on an individual basis . the aim of our work was to retrospectively evaluate the association of 16 parameters with specific outcomes in terms of disease control in a cohort of 126 patients treated in our centre in an attempt to identify predictive and prognostic factors that could help clinicians in the prescription of the most appropriate treatment . materials and methods this retrospective study included 126 patients with stage iii , iva and ivb h&n cancer radically treated with concomitant rt - cht in our institution between 1998 and 2010 . 
all patients were evaluated in a multidisciplinary meeting , and a nonsurgical approach was chosen because of site of disease ( for instance , oropharyngeal and hypopharyngeal cancer ) , medical reasons or in an attempt at organ preservation ( patients with advanced laryngeal cancer )  . 
further patient characteristics such as baseline body mass index ( bmi ) ( that is , before the start of rt - cht ) and weight loss throughout the treatment course were also analysed . 
haemoglobin ( hb ) levels were collected just before the first day of treatment and then weekly until the end of rt . rt was delivered with linear accelerators , normally with 6 mv photons . 
three clinical target volumes ( ctv ) were identified : ctv1 included macroscopic disease and involved nodes with a margin of 1 cm , ctv2 included nodal areas considered at high risk of microscopic disease and ctv3 included all other nodal levels considered at low risk of involvement . 
for both 3dcrt and imrt plans , igrt ( image - guided radiotherapy ) was performed with portal images for the first three days of treatment and then once weekly . 
induction cht consisted of tpf schedule ( docetaxel 75 mg / m2 on day 1 , cisplatin 100 mg / m2 on day 1 , 5 - fluorouracil 1000 mg / m2 from day 1 to day 4 ) and was used only in seven cases with advanced glottic cancer . 
a computed tomography ( ct ) or magnetic resonance ( mr ) scan to evaluate the response to treatment was performed after 2 or 3 months , every 4 months thereafter for 2 years , then every 6 months until the end of the fifth year . 
diagnostic imaging was performed in any patient with signs and symptoms suggesting recurrence or distant metastasis . after rt - cht , complete response ( cr ) was defined as no visible gross tumour , partial response ( pr ) as more than 50 % decrease , stable disease ( sd ) as < 50 % decrease and progressive disease ( pd ) as more than 25 % increase of gross tumour volume ( gtv ) or appearance of new lesions [ 7 ]  . 
persistence of disease included partial response , stable and progressive disease . statistical analysis the association between individual characteristics and specific outcomes was evaluated by the fisher exact test or the chi - square for trend , as appropriate . 
 the primary endpoint was the association of these characteristics with overall survival ( os ) , and secondary endpoints were their association with persistence of disease , disease - specific survival ( dss ) and disease - free survival ( dfs )  . the end of rt was used as the start of observation for survival analyses . 
prognostic factors can guide the physician in selecting the best possible treatment for each patient , possibly increasing the therapeutic index . in our analysis , many evaluated factors show an association with one or more of the outcomes . 
for instance , comorbidities show a negative impact on the prognosis of patients included in our analysis , as confirmed in a recent meta - analysis on 22.392 patients with head and neck cancer [ 8 ]  . 
the negative prognostic impact of both these parameters can be probably related to tumour hypoxia . it is well known that tumour hypoxia can increase radioresistance and also reduces the effect of certain chemotherapeutic agents [ 9 ]  . 
it has also been shown that the oxygen - carrying capacity of the blood represented by the hb level can affect tumour oxygenation [ 10 ] and that patients with severe anaemia are likely to have hypoxic tumours [ 11 ]  . often , patients with cancer suffer also from anaemia , mainly related to a chronic inflammatory status , and the condition tends to worsen because of treatments ( surgery , radiotherapy , chemotherapy )  . 
the french study , published by denis et al . , showed a correlation of low hb levels with poorer loco - regional control , disease - free survival and overall survival [ 12 ]  . 
similar results were confirmed in many other studies [ 13 , 14 ]  . performance status ( ps ) < 90 ( p nadir 10 ( p 0.0008 ) and comorbidities ( p 0.0001 ) , hb 0.024 ) in our experience , pre - rt hb value did not have a significant impact on any explored outcome . 
we also looked for a relationship between anaemia at any point before , during or after treatment and comorbidities , but no significant correlation was found . in our opinion , there is an interesting observation in this series , which can contribute to the discussion on the prognostic value of anaemia . 
the hb nadir during treatment showed a statistically significant correlation with persistence of disease , overall survival ( however not confirmed at multivariate analysis ) , disease - specific survival , and disease - free survival in our experience , with a cut - off of 10 / dl . 
we thought that interruption of treatment could have been correlated with the decrease of hb under the level of 10 g / dl and this could have explained the poor prognostic significance of hb nadir . 
analysed preoperative , postoperative , pre - radiotherapy and nadir levels of hb during radiotherapy , but they did not find a statistically significance for the latter [ 14 ]  . 
were not able to find a prognostic significance for hb level at the onset or after radiochemotherapy considering a cut - off of 12 g / dl in women and 13 g / dl in men [ 15 ]  . 
in a series of operated patients who underwent only adjuvant rt , reported by van de pol et al . , hb before and after rt did not show a statistically significant impact on outcome [ 16 ]  . our results are quite different from these experiences . 
who described a significantly higher incidence of lymph node metastases in a murine model in response to acute hypoxia [ 18 ]  . smoking habit is not only a well - known causative but also prognostic factor in hnscc [ 19 ]  . 
unfortunately , we only recorded smoking habits of our patients when they first presented at our clinic , but we could not evaluate if cessation of smoking had some impact on survival . 
therefore , according to our data , we can assert that the greater persistence of disease in smokers is related to less responsiveness to treatment of the tumour cells in this population and to hypoxia but not to a reduced compliance with therapies . all these results and considerations raise the issue of correction of tumour hypoxia . 
in 2007 , overgaard published a paper summarising the various attempts at correction of tumour hypoxia that can be found in the literature [ 21 ] , including the use of radiosensitisers [ 22 ] , methods to increase the delivery of oxygen through blood [ 23 ] and hypoxic cytotoxins [ 24 ]  . another simple way to correct tumour hypoxia should be by correcting anaemia in these patients . 
however , most studies conducted to date with the use of blood transfusion or erythropoietin failed to show any benefit [ 25 ] or , surprisingly , showed a detrimental impact on survival [ 26 ]  . 
hpv - positivity is a consistent determinant of superior survival irrespectively of the treatment approach used [ 27 , 28 ] and of many traditional prognostic factors , such as t stage or n stage [ 29 ]  . 
 for this reason , these data are not available for most patients in our series , making it impossible to obtain a significant analysis . apart from hpv , many other biological parameters have been studied as prognostic factors in head and neck cancer patients . 
for instance , a recent meta - analysis on 6.781 patients confirmed the negative impact of epidermal growth factor receptor ( egfr ) overexpression , especially in laryngeal squamous cell carcinoma [ 30 ]  . 
unfortunately , as for hpv , our analysis did not investigate and discuss such parameters , because data were missing in a significant proportion of patients included in this series . despite these limits , we feel that our study can give a contribution in identifying prognostic factors for h&n cancer patients , because all the data we considered in this series are easy to collect in any department . 
 we also decided to include in the analysis only patients treated in a sufficiently homogeneous way , in terms of doses and volumes of rt and doses and schedules of cht . 
 these limitations obviously reduced the total number of this series , but allowed a more homogeneous and complete analysis . we were unable to find in our analysis any significant factor that may constitute a contraindication for the combined approach with rt and cht , and identify patients for whom a palliative approach or best supportive care could be preferred . anaemia in h&n cancer patients is one of the more discussed topics . 
studies addressing this topic are ongoing and , hopefully , they will clarify this controversy in the next few years . conclusion our experience showed that hb nadir during treatment , bmi , smoking habits , stage , comorbidities and performance status are prognostic factors for outcome and response to radical treatment with radiochemotherapy . 
selcuk simsek4 fatma teke5 cemil goya6 received : 13 may 2015 / accepted : 19 october 2015 / published online : 5 november 2015 italian society of medical radiology 2015 abstract purpose we aimed to evaluate the effectiveness of the brain region imaging in fdg - pet / ct scanning of patients with suspected or diagnosed lung cancer . materials and methods we performed the study retrospectively on the medical charts of 427 patients . 
the most widely used pet / ct pharmacological tracer is f - 18 2 - fluoro - 2 - deoxy - d - glucose ( fdg ) , which is a radiolabelled analogue of glucose . 
fdgpet / ct whole - body imaging is frequently used for staging , restaging , and treatment - monitoring of numerous tumor types and it may be considered a whole - body scan ; however , it is usually limited to a certain body area that includes the region between the base of the skull and the proximal / mid - thigh . 
the fdg - pet / ct limited wholebody imaging technique is an accepted procedure and has been entered into the guidelines [ 1 , 4 , 5 ]  . recently , several studies have been published to evaluate the clinical contribution of brain imaging with fdg - pet / ct in cancer patients [ 613 ]  . 
however , to the best of our knowledge , the effectiveness of brain imaging has not yet been evaluated by comparing with body regions routinely included in the fdg - pet / ct field of view ( fov )  . 
all patients had diagnosed or suspected lung cancer , and we classified these patients into three groups : the lung cancer group , the solitary pulmonary nodule ( spn ) group , and the solitary pulmonary mass ( spm ) group . 
prior to the study , we obtained ethical approval from the institutional ethics committee , and all study protocols were approved by the committee . imaging procedure we performed fdg - pet / ct imaging according to the guidelines ( 1 , 4 , 5 )  . 
 a biograph 6 pet / ct scanner ( siemens medical systems , knoxville , tn ) was used for the imaging , and the ct scan was performed before the pet scan . 
ct and pet imaging was initiated at the head , and scanning was acquired in as many as six or seven bed positions ( from vertex to proximal / mid - thigh )  . 
the ct component of the integrated scanner was 6 - slice and the slice thickness was 6 mtrued software program was used for image evaluation . materials and methods image evaluation and analysis patient population we performed the study retrospectively on the medical records of 427 patients from elaz education and research hospital that were dated january 2010 to december 2012 . 
 patients had synchronous tumors or whose fdg - pet / ct scans were repeated in the same year were excluded from in our clinic , we routinely scan from vertex to proximal / mid - thigh ; therefore , the brain regions of the patients are within the scanning area . 
 the area between the skull base and the c7t1 intervertebral space was considered the headneck region , and the area between the diaphragm and the l4l5 intervertebral space / upper border of the iliac crest was considered the 1 3 220 radiol med ( 2016 ) 121 : 218224 abdominal region . 
the pelvic region was classified as the area between the l4l5 intervertebral space / upper border of the iliac crest and the lower border of the fov ( proximal / mid - thigh )  . 
each metastatic finding in these regions was assessed by a medical oncologist and a radiation oncologist with regard to the potential to modify the disease stage , chemotherapy protocol , radiotherapy protocol , or surgical management if it was assumed that any region would have been excluded from the fov . 
if the metastatic findings had the potential to modify any treatment protocols or surgical management , we named this situation a clinical contribution . we considered the average width of the fov as one bed position for the brain and headneck region and two bed positions for the abdominal and pelvic region . 
 we calculated the rates of the metastatic findings separately for each region by dividing the number of patients with metastasis in a certain region by the total number of patients . 
then , using the same calculation method for each region , we calculated the rates of the clinical contribution and the effective clinical contribution , based on the potential to modify the disease stage , chemotherapy protocol , radiotherapy protocol , or surgical management . 
one hundred seventy - three patients were in the lung cancer group , while 142 were in the spm group and 112 were in the spn group . the metastasis ratio , effect on disease stage , effect on chemotherapy and radiotherapy protocols , effect on surgical management and the clinical contribution of the body regions in the lung cancer , spm and spn groups are documented in tables 1 , 2 and 3 . total metastases , total clinical contribution and total effective clinical contribution ratios of the brain , head neck , abdominal and pelvic regions in the fdg - pet / ct imaging are shown in figs . 
2 , 3 and 4 . the metastatic findings , clinical contribution and effective clinical contribution ratios were the highest in the lung cancer group and the lowest in the spn group for all of the body regions ( tables 1 , 2 , 3 )  . 
metastatic findings were detected in only one patient for the brain and headneck region in the spn group , but these findings did not have any features that could change the disease stage or any treatment protocol ( table 3 )  . 
the limited whole - body imaging area is defined in the guidelines as the fov between the skull base and the proximal / midthigh [ 1 , 4 , 5 ]  . 
in addition , the guidelines recommend applying a true whole - body imaging procedure for tumors with a high likelihood of brain or lower extremity involvement [ 1 , 4 ]  . 
due to this situation , different imaging procedures are administered in different clinics . there is no doubt that the addition of other body regions to the limited whole - body pet / ct imaging fov may provide a greater clinical contribution . 
in addition , we decided to evaluate the clinical contribution of the brain region in lung cancer because previous studies have 1 3 radiol med ( 2016 ) 121 : 218224 fig . 
management , n number of patients spn ( n : 112 ) brain region headneck region abdominal region pelvic region spn solitary pulmonary nodule , cht chemotherapy protocol , rt radiotherapy protocol , m . 
therefore , we could not compare the accuracy of our results with any other studies . the highest metastatic findings ( 30.6 % ) and clinical contribution ratios ( 9.8 % ) were found in the abdominal region in the lung cancer group . 
the highest metastatic and clinical contribution ratios found in the abdominal region may be related to proximity to the primary lesion , the large extent of the imaging fov ( two bed positions ) and the coverage of potential metastatic sites , such as the surrenal glands , the liver and lumbar vertebrae in this region . 
however , the effective clinical contribution ratio drops to 4.9 % because the abdominal fov is two bed positions , which partially explains why the abdominal region falls behind the brain region . 1 3 radiol med ( 2016 ) 121 : 218224 fig . 
2 metastasis ratios in the brain , headneck , abdominal , and pelvic region in the fdg - pet / ct imaging of patients with lung cancer ( ca ) , solitary pulmonary mass ( spm ) , and solitary pulmonary nodule ( spn ) fig . 
4 effective clinical contribution ratios of the brain , head neck , abdominal , and pelvic region in the fdg - pet / ct imaging of patients with lung cancer ( ca ) , solitary pulmonary mass ( spm ) , and solitary pulmonary nodule ( spn ) in the brain region were high . 
moreover , it has been stated in a guideline that limited - area tumor imaging can be considered when critical abnormalities are likely to be localized in a known region of the body ( e.g. , solitary pulmonary nodule , probable lung cancer , evaluation of hilar lymph node involvement , diagnosis of head and neck cancer , and monitoring of therapy of locally advanced breast cancer ) [ 1 ]  . 
moreover , we advise that histopathology and tumor size should be considered in the fov determination for each tumor type . conclusions the addition of the brain region to the limited whole - body fov in fdg - pet / ct scanning seems to be effective in the lung cancer and spm groups but not in the spn group . 
 considering the histopathology and tumor size for each tumor type may be clinically beneficial in the determination of the fdg - pet / ct scanning fov . compliance with ethical standards conflict of interest the authors declare that they have no financial relationship with any organization related to the research . 
the uptake of 99mtc - hynic - toc was considered to be physiologic in patients with normal findings at dedicated abdominal ct or mr and lack of neoplastic lesions in clinical follow - ups . 
among the 36 patients without any evidence of malignancy in ct , mr and follow - up , 7 ( 19.4 % ) showed increased uptake in the uncinate process . 
in neuroendocrine tumors ( net ) , in particular , there is an overexpression of somatostatin receptors at the neoplastic cell membrane , allowing their detection in vivo by radiolabeled somatostatin analogs . 
this is the case of somatostatin receptor scintigraphy ( srs ) using 111in - dtpa - octreotide , as well as of positron emission tomography ( pet ) with recently introduced somatostatin analogs labeled with the positron emitter isotope 68 ga ( 68 ga - dota peptides )  . 
both methods have been successfully used for the diagnosis , therapy monitoring and follow - up of net patients [ 1 , 2 ]  . however , an increased physiologic uptake of both 68 ga - dota peptides in the uncinate process of the pancreas , which mimics malignancy , has been described in up to 23 % of cases . 
consequently , the distinction between a neoplastic lesion and the physiologic uptake of these tracers in the uncinate process may be particularly difficult in patients with known or suspected pancreatic net [ 3 ]  . recently , 99mtc - hydrazinonicotinamide - tyr - octreotide ( 99mtc - hynic - toc ) , a somatostatin analog labeled with technetium - 99m , has been introduced into clinical practice . 
 although the biodistribution of 99mtc - hynic - toc is similar to that of 111in - dtpa - octreotide , previous studies have shown that 99mtc - hynic - toc has a higher sensitivity and improved clinical performance than 111in - dtpaoctreotide [ 4 , 5 ]  . 
this study was approved by the institutional ethics review board . images were acquired after venous administration ( octreor , of 555 mbq of 99mtc - hynic - toc radiopharmacus , brazil ) using a dual - head gamma camera ( infinia ; ge medical systems , milwaukee , usa )  . 
1 spect / ct axial slices show increased 99mtc - hynic - toc focal uptake in uncinate process of the pancreas in a patient whom abdominal mr and clinical follow - up during 8 months excluded pancreatic net 1 3 radiol med ( 2016 ) 121 : 225228 uptake ( lesser , equal to or greater than the normal uptake in the liver parenchyma )  . 
positive scintigraphic findings were compared to abdominal ct or mr obtained in the same period of the srs , as well as with clinical and anatomical imaging in follow - up visits . 
the increased focal uptake in the uncinate process was considered to be physiologic when the ct or mr showed normal pancreatic density without focal lesions in the head of the pancreas . results for five patients , the focal increased uptake of 99mtchynic - toc in the pancreas was attributed to the presence of net lesions , as evidenced by the detection of tumoral pancreatic lesions in the abdominal mr or ct obtained shortly after the spect / ct procedure . 
interestingly , for all these cases the patterns of pancreatic uptake were the same in their subsequent studies ( slight uptake in one , focal uptake with lesser intensity than the liver in 3 , and no uptake in 3 patients )  . discussion the observed increase of 99mtc - hynic - toc uptake by the uncinate process in over 17 % of those subjects without any evidence of net in the pancreas is consistent with previous studies showing an increased physiologic uptake of 68 gadota peptides ( noc , toc and tate ) in the pancreatic uncinate process which may also mimic tumoral lesions [ 3 , 6 , 7 ]  . 
this is in line with previous findings using 111in - octreotide , which suggest that spect / ct has an incremental value over planar and spect imaging in the evaluation of net [ 8 ]  . 99mtc - hynic - toc , our observation that the pattern of uptake in the uncinate process is stable over time , with the same pattern repeatedly and consistently found for the same patients , agrees with the notion that the expression of somatostatin receptor ( sst ) subtypes in the pancreas is stable [ 3 ]  . 
 the reasons for individual variation in the physiologic 111in - dtpadistribution octreotide and 68 ga - dota peptides in the uncinate process have not been clearly elucidated yet , but may be related to the variability both in sst subtype expression and in the distribution of endocrine cells within the pancreas . 
hynic - toc and 111in - dtpa - octreotide , as well as 68 ga - dota peptides , the increased uptake of these labeled somatostatin analogs in the uncinate process by some individuals may be triggered by individual differences in the distribution of sst2 - expressing cells [ 9 , 10 ]  . the patient , availability , cost and because of the well - known physical advantages of technetium - 99 m over indium111 in terms of radiation burden image resolution , as well as the fact that the spect / ct modality is more prevalent than pet / ct , 99mtc - hynic - toc is an important tool for the evaluation of somatostatin receptorexpressing tumors . 
we have shown here , however , that physiologic uptake of 99mtc - hynic - toc in the uncinate process may be increased in some patients , indicating that caution should be taken to avoid the misinterpretation of a neoplastic lesion . 
the differences and compliance between the readers in the parameters assessed were investigated . results out of 619 segments ; reader 1 considered 187 segments ( 30.2 % ) and reader 2 considered 177 segments ( 28.6 % ) to have poor and inadequate mr image quality . 
non - invasive imaging techniques that are routinely used for the examination of pad include doppler 1 3 radiol med ( 2016 ) 121 : 916925 ultrasonography ( doppler us ) , computed tomography angiography ( cta ) and magnetic resonance angiography ( mra ) [ 3 ]  . 
digital subtraction angiography ( dsa ) is the gold standard for diagnosis ; however , it is invasive and expensive . today , contrast - enhanced mra is essential to assess arterial diseases [ 3 ]  . 
however , after an association between gadolinium - based contrast agents and nephrogenic systemic fibrosis as well as brain deposits of gadolinium was discovered , safety concerns have led to increased interest in unenhanced mra [ 6 ]  . 
the findings were compared to mdct angiography as a reference imaging technique ; the latter has high sensitivity and specificity in the diagnosis of pad [ 5 ]  . materials and methods the study was conducted prospectively with 37 patients who were suspected of or showed positive doppler ultrasound for pad between june 2014 and october 2014 . 
no surgical or medical treatment was given to the patients during this process . mdct angiography parameters mdcta examinations were performed using a 128 - mdct device ( definition as , siemens medical solution , forchheim , germany )  . 
imaging parameters were ascertained as 120 kv , gantry rotation time 0.3 s , pitch 0.8 , collimation 128 0.6 mm , reconstruction slice thickness 512 matrix , reference tube flow 200 mas , 0.6 mm , 512 tube flow range 180240 mas and table rate 100 mm / s . 
 ultravist 370 ( iopromide , bayer schering healthcare , berlin , germany ) and omnipaque 350 ( iohexol 350 ge healthcare , milwaukee , wi , usa ) were used for cta examinations . 
bolus tracking ( care bolus , siemens medical solution ) method was used to determine the time delay between the administration of contrast agent and the initiation of screening for each patient . 
a round roi ( region of interest ) sized between 10 and 15 mm2 was placed in the abdominal aorta lumen at the infrarenal level to measure the hu value . 
medium soft - tissue deconvolution algorithm ( b20 kernels ) was used routinely for image reconstruction . native space mr angiography parameters mra examinations were performed on a siemens magnetom avanto mr syngo b13 at 1.5 t ( siemens medical solutions , erlangen , germany )  . 
the parameters used for 34 ms , flip angle this region were : tr 165 , matrix 300 384 and fov 430 min the second step , femoral and popliteal arteries were assessed ( femoropopliteal region )  . 
a single slice native td cine scout image passing distal to the common iliac arteries was acquired for the aortoiliac region , passing through the middle section of the both superficial femoral artery for femoropopliteal region and passing through the middle section of the calf for subpopliteal region . 
if the td for peak arterial flow differed between the two legs , a longer delay was used . image analysis images acquired were evaluated independently and separately by two radiologists with more than 8 years of experience with mra and ct on workstations ( osirix , pixmeo , switzerland )  . 
these segments were the abdominal aorta , common iliac artery , external and internal iliac artery , proximaldistal part of superficial femoral artery , main and deep femoral artery , popliteal artery , peroneal artery , posterior and anterior tibial artery . 
parallel imaging with generalized autocalibrating partially parallel acquisition ( grappa ) acceleration factor 2 was used for each of these three steps . native space mr imaging sequence is based on the subtraction of ecg - triggered data with and without arterial peak flow . 
two native space data - sets could be obtained with the delay of different ecg triggering : ( 1 ) systole period images in which the arteries appeared to be flowvoid where arterial flow rate was maximum in the cardiac cycle and ( 2 ) diastole period images in which the arteries appeared to be bright due to a slower flow rate . 
the stenosis could be seen both in source images and full mip images . following the quality analysis , segments contained in groups 1 and 2 were determined inadequate in terms of diagnosis and excluded from the evaluation of stenosis . patients were divided into two groups : under 50 years of age ( n 9 ) and older 51 years of age ( n 21 )  . 
thus , two groups were formed and their correlation with age was investigated . arterial segments considered to be diagnostic in both the cta and native space mra examinations were analyzed in terms of stenosis . 
grade 1 : no stenosis , grade 2 : stenosis less than 50 % , grade 3 : significant stenosis between 50 and 90 % , grade 4 : preocclusive stenosis greater than 90 % and grade 5 : occlusion [ 3 ]  . 
the sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) and accuracy of native space mra examination were calculated and compared with cta as the reference . 
when compared to cta , sensitivity , specificity , diagnostic accuracy of native space mra are given in table 6 for reader 1 and in table 7 for reader 2 . 
2 cta and mr angiography of a 65 - year - old woman with bilateral limb paa 3d - volume rendering reconstruction of ct angiography , most of the lower limb bones were removed . 
3 a 64 - year - old female diabetic patient with typical lower limb paa aortoiliac vascular is seen with excellent signal quality in maximum intensity projection reconstruction of ct angiography . 
there is occlusion of bilateral superficial femoral artery ( arrows ) table 5 rates of normal , stenosis and can not be evaluated segments in mra as a reference cta normal stenosis not evaluated cta normal 306 ( 46.7 ) 292 ( 44.6 ) 62 ( 9.5 ) 23 ( 3.5 ) 30 ( 4.6 ) cta stenosis 19 ( 2.9 ) 49 ( 7.4 ) 81 ( 12.3 ) 114 ( 17.5 ) 157 ( 24.0 ) 32 ( 4.9 ) 145 ( 22.1 ) ( % ) , r1 : reader 1 , r2 : reader 2 1 3 922 fig . 
5 mip reconstruction of cta and mr angiography in a 51 - year - old female with right limb paa there is severe stenosis in posterior tibial artery in cta . 
it can make it appear larger than it really is , leading to an overestimation of a vascular stenosis or suggest a spurious occlusion [ 8 , 9 ]  . 
this is one of the drawbacks of this technique [ 3 , 5 , 8 ]  . diagnostic image quality of arterial segments in this study was 69.8 % according to reader 1 and 71.4 % , according to reader 2 . 
 [ 8 ] reported that image quality was good or excellent only in 8 % of the vessels in the pelvic region , 40 % in the femoral region and 38 % in the popliteal and lower limb arteries [ 8 ]  . 
 [ 3 ] achieved good or excellent quality images in aortoiliac region in 38 % of the patients , in femoropopliteal region in 58 % of patients and in subpopliteal region in 64 % of the patients [ 3 ]  . 
in addition , image quality in the femoropopliteal and subpopliteal regions was better than in the aortoiliac region , a finding corroborated by other studies [ 3 , 8 , 1214 ]  . 
image quality of the native space sequence was significantly poorer than in the reference imaging ( contrast - enhanced mra , dsa and cta ) [ 3 , 8 , 1214 ]  . a significantly lower image quality was seen in patients who were above 51 years of age in the native space sequence . 
this can be explained by the age - related increase in the incidence of pad ; it is thought that multiple stenoses in this current - dependent sequence had an adverse affect on image quality [ 3 , 8 ]  . 
however , acquisition of a better image quality with younger people ( younger than 50 years ) indicates that this sequence is more effective in this age group . the overall specificity , sensitivity and npv in identifying stenosis in peripheral arteries were found to be 7593 , 8689 and 8998 % , respectively , in studies conducted with the native space technique in the literature [ 3 , 8 , 12 , 13 , 15 ]  . 
however , when the poor and average image quality segments were added , the detection rate of stenosis and occluded segments was even lower ( 31.5 and 37 % , respectively )  . 
native space mra examination can be performed in patients in whom contrast - enhanced mra or cta fail or cannot be performed for the purpose of pad detection due to their high negative predictive value . 
another advantage of this technique is the ability to easily repeat the examinations . improved image quality and higher diagnostic accuracy have been obtained in peripheral arteries in studies performed using the fbi ( toshiba ) and trance ( philips ) unenhanced mra methods ( unenhanced 3d turbo spin echo mr angiography ) [ 10 , 16 , 17 ]  . 
in the same study , the authors reported that the difficulty in diagnosis for smaller arteries was attributable to reduced speed of blood flow in distal vessels [ 17 ]  . 
sensitivity and specificity values in studies conducted with the fbi sequence were higher than those in the current study and in studies conducted with the native space technique [ 16 , 17 ]  . 
 [ 17 ] were 9796 and 9897 % , respectively . to the best of our knowledge , this is the first study to compare the native space technique with cta . 
this may suggest that the percentage of 1 3 924 radiol med ( 2016 ) 121 : 916925 the segments with good and excellent image quality in the current study was higher than in the study by partovi et al . 
non - homogenous low quality images and advanced level of stenosis may have made it difficult to assess the vascular lumen leading to an unsatisfactory level of agreement [ 18 ]  . 
this can be reduced by evaluating the images acquired in the diastolic phase when both arteries and veins appear to be bright . the low image quality and sensitivity in the current study may have resulted from various factors . 
the decreased image quality in the aortoiliac region in the current study may have resulted from bowel movements , breathing and attenuation of the signal due to the increased distance between the rf coil and the artery in obese patients . 
 [ 6 ] have reported that different delay time calculations should be performed for each artery region to be imaged , since the distance between heart and different artery segments differ . 
 [ 19 ] have reported that delay times should be calculated separately for each lower extremity since varying extents of stenoses in different locations in both the lower extremities may affect flow rates ; additionally , the delay times between the extremities may vary . 
last , since the cardiac output of patients was not measured , its effect on the quality of mri could not be evaluated . to conclude , the unenhanced 3d turbo spin echo mr angiography sequence should not be used to assess arteries in the aortailiac region due to poor image quality . 
however , it can be used as the first - step imaging method before contrast - enhanced examinations in assessing pad in the femoral region and calf arteries in patients with chronic renal failure who are at high risk of atherosclerosis and nsf . 
 image features were evaluated for the following : cortical destruction , tumor border and pattern , calcification mode , intensity , peritumoral soft - tissue mass , density / signal edema , acetabular ( cartilage ) destruction , diffuse signal changes in acetabulum , mass inside hip joint , femoral head involvement , enhancement manifestations and the maximum length of the tumor . 
these image features between lgcs and hgcs were also assessed . results the most common ct and / or mr findings included cortical destruction , punctate , ring - and - arc and linear calcification , soft - tissue mass , lobulated border , high signal intensity with low signal septa on t2 - weighted image , peritumoral edema , hip joint infiltration , peripheral and septal enhancement on post - enhanced mr image . 
statistical analysis showed that the image features , such as * guangbin wang wgb7932596@hotmail.com 1 shandong medical imaging research institute , shandong university , jinan 250021 , shandong , peoples republic of china 2 department of radiotherapy , liaocheng peoples hospital , liaocheng 252000 , shandong , peoples republic of china 3 department of radiology , ruijin hospital , shanghai jiao tong university school of medicine , no . 
cortical destruction , soft - tissue mass , hip joint infiltration and tumor size can differentiate hgcs from lgcs . keywords bone neoplasm para - acetabulum chondrosarcoma computed tomography magnetic resonance histopathological grade introduction chondrosarcoma ( cs ) is relatively common primary malignant tumor of bone , first definitely described by lichtenstein and jaffe in 1939 [ 1 ]  . 
based on the presence of cellularity , cellular atypia and mitosis , cs is histopathologically differentiated into grade 1 , grade 2 and grade 3 [ 3 , 4 ]  . 
tumor grade , margin status ( healthy or invasive ) and acetabulum involvement were correlated with a reduced survival rate [ 7 ]  . 1 3 898 radiol med ( 2016 ) 121 : 897904 the majority of cs occurs in the long tubular bones , it also frequently occurs in the para - acetabulum [ 1 ]  . 
to the best of our knowledge , however , the image features with histopathological grades of para - acetabular cs have not been sufficiently described and reported [ 2 , 5 , 810 ]  . 
the purpose is to enhance the awareness of the characteristic imaging features and assess the difference between lgcs and hgcs . materials and methods patients institutional review board approval was obtained before this retrospective study and informed consent was not required for patient data review . 
the exclusion criteria were as follows : ( 1 ) secondary cs ; ( 2 ) not central cs in pathology ; ( 3 ) not in the para - acetabulum in anatomy ; ( 4 ) pathological fracture . 
all patients with an hgcs underwent wide excision ( n 4 ) or intralesional excision ( n 20 ) and grade 3 ( n 6 ) , grade 2 ( n 25 )  . imaging procedures ct was performed in all 31 patients . 
mr examination was performed in 21 patients , of which 12 were undergone contrast - enhanced scanning . as the ct scanning was performed at two institutions , the ct systems and scanning parameters varied . 
the 512 , imaging parameters were as follows : matrix 512 tube voltage 100120 kv , tube current 200240 ma , section thickness and intervals 2.55.0 mthe range of scanning included the pelvic and the head and neck of femur , so it can cover the whole lesion . 
after thinning to section thickness and intervals of 1.25 mm , the bone window and soft - tissue window and 2d or 3d reconstruction were used for observation . the mr systems and scanning parameters also varied , because the mr scanning was performed at two institutions . 
the images were analyzed for the following features : cortical destruction , tumor border and pattern , calcification mode and distribution , soft - tissue mass , density / signal intensity of tumor , peritumoral edema , acetabular ( cartilage ) destruction , diffuse signal changes in acetabulum , mass inside hip joint , femoral head involvement and enhancement manifestations . 
based on the intralesional excision and wide excision specimen , the final histopathology report and the grading was documented according to widely accepted definitions [ 11 , 12 ]  . 
the correlation between the image features and histopathological grade was assessed by two radiologists . statistical analysis the correlations between patient age and tumor size and tumor grade were calculated using linear regression analyses . 
fishers exact text showed that the ct features between lgcs and hgcs were statistically significant ( p 0.000 ) , including soft - tissue mass , cortical and acetabular destruction . table 2 summarized the mr imaging features in 21 patients with lgcs and hgcs . 
three cases of hgcs were seen diffuse enhancement in at least in one portion of the lesion . discussion central cs is a subtype of primary chondrosarcoma that frequently develops 40 and 50 years of age and demonstrates a slightly high male predilection [ 2 ]  . 
because of the delay in onset of clinical symptoms , css of the para - acetabulum are often large lesions at initial evaluation relative to patients with tumors in extremities [ 14 , 15 ]  . 
in our series , soft - tissue mass was detected in 81 % cases and the mean maximum diameter of lesions was 6.5 chowever , a palpable soft - tissue mass was only detected in 55 % patients . 
 because of the complex anatomy , soft - tissue mass of paraacetabular css often grow into the pelvic cavity . 1 3 900 radiol med ( 2016 ) 121 : 897904 fig . 
1 a 43 - year - old female patient with high - grade chondrosarcoma in the left para - acetabulu a axial ct scan revealed cortical destruction with soft - tissue mass ( arrow ) , punctuate intraosseous calcification and acetabular destruction . 
d axial gadolinium - enhanced t1 - weighted mr image demonstrates peripheral and septal enhancement of the tumor ct imaging , primarily because of its superior density resolution , is the best radiologic modality with which to identify cortical destruction and matrix mineralization , particularly when it is subtle and the lesion is in a complex area of anatomy , such as para - acetabuluit was reported that calcification was detected in 6078 % of cs , and the characteristic mode was ring - and - arc [ 2 , 13 , 16 , 17 ]  . 
acetabular destruction was also more commonly seen in hgcs ( p 0.000 ) , which indicated hip joint infiltration . 1 3 radiol med ( 2016 ) 121 : 897904 fig . 
2 a 62 - year - old male patient with high - grade chondrosarcoma in the left para - acetabulua thin - slice helical acquisitions with 2d reconstruction was performed in coronal planes , cortical destruction , soft - tissue mass ( white arrow ) , punctuate and ring - and - arc calcification ( black arrow ) , acetabular destruction ( arrow head ) was clearly observed . 
peritumoral edema was clearly seen on stir image mr imaging has a better contrast resolution and multiplanar imaging features , which provide the best method for depicting the soft - tissue mass , tumor border and pattern , extent of marrow involvement in para - acetabular cs [ 2 , 5 , 13 , 2124 ]  . 
small high signal intensity foci were seen in 20 % of our series on t1 - wis , which was also less common in cs of long bone , but more common in enchondroma [ 2 , 13 ]  . 
it is believed that these areas result from the lobular growth pattern , which leaves intervening residual areas of normal bone marrow , and this feature is the most important distinction between low - grade chondrosarcoma and enchondroma [ 13 ]  . 
3 a 63 - year - old male patient with low - grade chondrosarcoma in the left para - acetabulu a axial ct scan reveals low density area , fine linear intraosseous calcification ( arrow )  . 
as previous reports , css of the para - acetabulum often demonstrate typical prominent , septal and / or peripheral enhancement on contrast - enhanced mr image [ 21 ]  . 
our study also found diffuse enhancement in 3 hgcss but in no lgcs . acetabular cartilage functions as a barrier against the extension of bone tumors [ 26 , 27 ]  . 
radiological features of hip joint infiltration included acetabular cartilage destruction , diffuse signal changes in acetabular tumors , a mass inside hip joint , femoral head involvement [ 27 ]  . 
diffuse signal changes in 1 3 radiol med ( 2016 ) 121 : 897904 acetabulum were detected in all cases , while the feature in all lgcs was negative in pathology . 
it might be difficult to distinguish between inflammatory changes and the tumor itself with mr images , which may lead to miss diagnosis of diffuse signal changes [ 27 ]  . 
these features of hip joint infiltration suggest wide extraarticular resection , because the incidence of local relapse is high after inadequate surgery and ineffective adjuvant modalities [ 7 , 27 ]  . when encountering a single osteolytic mass in the para - acetabulum , the differential diagnosis should include enchondroma , aneurysmal bone cyst ( abc ) , eosinophilic granuloma , ewing sarcoma , osteosarcoma , solitary plasmacytoma . 
eosinophilic granuloma is often present between 5 and 15 years of age , and it is often detected on bone sclerosis in surrounding zones and well - defined sclerotic margin with iliac lesions [ 31 ]  . 
sclerotic components are most frequent in the intraosseous component , while cortical thickening , pathologic fracture , expansile bone remodeling , soft - tissue calcification , well - marginated lesion are not commonly observed in ewing sarcoma of pelvic [ 32 ]  . 
 furthermore , contrast - enhanced mr examination did not undergo in every patients in our study , we were not able to sufficiently evaluate the difference between lgcs and hgcs in this feature . 
larger series and further studies are needed to greater insight into this disease . in conclusion , the most important and characteristic imaging features of para - acetabular cs include an osteolytic lesion with cortical destruction , soft - tissue mass , lobulated border , punctate , ring - and - arc , linear calcification , high signal intensity with low signal intensity septa on t2 - weighted mr image , and peripheral and septal enhancement on post - enhanced mr image . 
spn is characterized radiologically as an intraparenchymal lung lesion which is single and well marginated , has rounded opacity with 3 cm diameter , and is not associated with atelectasis , adenopathy and pneumonia and pleural effusion [ 13 ]  . there are many cases such as benign tumors , infectious lesions and lung cancer , as well as malignant conditions , in the differential diagnosis of spn . 
the prevalence of malignancy in spn varies between 1 and 12 % in various studies [ 46 ]  . positron emission tomography / computed tomography ( pet / ct ) with 18f - fluorodeoxy - glucose ( fdg ) is widely used in the imaging workup of various malignancies for diagnosing , staging , restaging and surveillance [ 7 ]  . the combination of the ct into pet offers several advantages over pet alone , and the most important is the ability to accurately localize increased fdg activity . 
additionally , it provides procedures with shorter image acquisition time , as well as serving as a parameter for correcting the attenuation at the emission images [ 810 ]  . 1 3 radiol med ( 2016 ) 121 : 944949 it is known that when the pet scan is positive , the probability of malignancy is high , but the evaluation of pulmonary nodules by fdg - pet / ct is limited because of the several factors . 
this attenuation may cause image distortion and impair adequate quantification , especially in small size lesions . nowadays , attenuation correction is routinely used in pet imaging for correction of these effects . 
for these reasons , there has been disagreement about the desirability of attenuation correction in pet imaging . as a result , the impact of attenuation correction on lesion detectability and interpretation of pet for oncological purposes is not well established . the purpose of this study is to determine the sensitivity , specificity and diagnostic accuracy of nonattenuation - corrected ( nac ) and attenuation - corrected ( ac ) fdg - pet / ct images in patients with spn . materials and methods this study was conducted as a retrospective cross - sectional study at the nuclear medicine department of the private osm - ortadou hospital . a total of 41 patients with spn , consisting of 28 males and 13 females , were included in the study . 
ct imaging was performed ( 130 kv , 30 ma , 5 mm slice thickness ) within 1 min before pet imaging with the patient in precisely the same position . 
if the interval was longer than 1 month , they were excluded . the final diagnoses of spn were based on histopathology whenever available , but on clinical follow - up ( 18 36 months ) and imaging modalities ( ct ) if not available . patient preparation and pet / ct imaging protocol all patients fasted , except for glucose - free oral hydration , for at least 6 h before the iv injection of 370555 mbq ( 1015 mci ) of fdg . 
at the time of the tracer injection , blood glucose levels were checked and confirmed to be less than 150 mg / dl in all patients . all patients were examined using a pet / ct system ( biograph lso ; siemens medical solutions ) , combining a dedicated , full - ring pet scanner . 
twenty - two ( 54 % ) of the spns were 50.2 malignant and 19 ( 46 % ) were benign based on the histopathology and imaging data . while 25 spns were diagnosed as malignant or benign nodules with biopsy ( biopsy was made after the pet study in 15 patients and during follow - up in others ) , the remaining 16 spns were considered to be like a benign process either by absentmild fdg uptake ( < 2.5 suvmax values ) on pet study and stability of the lesion on ct over the clinical follow - up period ( 1836 months )  . 
 in other words , the sensitivity and npv were found to be 100 % in the detection of spns for both methods . in the nac image , the visual scoring of 22 malignant spns was found as follows : 4 points in 14 spns , 3 points in 7 spns and 2 points in 1 spn . 
1. we also analyzed the fdg uptake intensity of the nodules based on the location for both methods . the visual scores of centrally located spns were found for nac and ac methods , respectively , as : 4 point score in 8 / 14 , 7 / 14 ; 3 point score in 5 / 14 , 5 / 14 ; 2 point score in 1 / 14 , 2 / 14 . 
the visual scoring points of centrally located spns were not significantly different in both the methods . the visual scores of peripherally located spns were found for the nac and ac methods , respectively , as : 4 point score in 7 / 27 , 3 / 27 ; 3 point score in 6 / 27 , 11 / 27 ; 2 point score in 14 / 27 , 13 / 27 . 
in the peripherally located nodules , while the number of nodules with visual scoring 4 points was more in the nac method , the nodules with visual scoring 3 points were more in the ac method . 1 3 radiol med ( 2016 ) 121 : 944949 fig . 
2. the visual scores of spns based on the location for both methods are shown in table 2 . discussion the differential diagnosis of solitary pulmonary nodules ( spns ) is very important for successful treatment . 
 they have demonstrated that fdg - pet / ct has higher accuracy and sensitivity for characterization of solitary pulmonary nodules . the prevalence of malignancy in patients with spn is observed to be in a wide range such as 3885 % in pet studies [ 1315 ]  . 
when we look at the 15 patients who underwent biopsy after pet scan , it was 1 3 948 radiol med ( 2016 ) 121 : 944949 found that % 86.6 of patients have malignant spn . 
these results are compatible with reality that pet is a successful method for the prediction of the characterization of spns . the standardized uptake value ( suv ) is a semiquantitative measurement of [ 18f ] fluorodeoxyglucose ( 18f - fdg ) uptake . 
there are several suv parameters such as suvmax , suvmean , suvpeak , corrected suv , etc . , but there is no clear consensus about the best of the although suvmax is widely used because of its simplicity , it has well - known restrictive limitations . 
in addition to the suv parameters , visual assessment is also important for the analysis of pet imaging . the quantitative and visual analyses of lesions by fdgpet / ct is limited because of several factors . 
this feature could be one of the reasons for better performance of the nac methods . however , several studies have shown to be similar to the visual analyses of nac and ac images for the detection of lesions [ 1719 ]  . in the present study , the sensitivity and npv were found to 100 % in the detection of spns for nac and ac images . 
these results are consistent with information that attenuation correction may cause noise and even artifact . on the other hand , our study showed that for all spns and spns 2 cm , the nac image method had a higher diagnostic performance for the spn characterization as malignant or benign , when compared with the ac image method . 
concerning these , the lesion size is an important factor for suvmax and , when the lesion size is smaller than the transaxial spacing , partial volume - averaging effect occurs on pet imaging [ 22 ]  . 
in the current study , the mean suvmax was significantly lower in spns 2 cm , but we think that partial volume - averaging effect does not occur because the smallest nodule diameter is 12 mthe other evidence supporting our thoughts is that the visual scoring points of spns 2 cm are not found significantly different between the both methods . as it is mentioned in the study of houseni et al . 
similar to this study , we found that the mean suvmax value was significantly higher in centrally located spns compared to those peripherally located . however , the visual scoring points of centrally located nodules were not significantly different between the two methods . 
carbonaro7 francesca caumo8 beatrice cavallomarincola9 paola clauser10 , 11 chiara fedato12 alfonso frigerio13 vania galli14 livia giordano15 paola golinelli16 giovanna mariscotti17 laura martincich18 stefania montemezzi19 doralba morrone5 carlo naldoni20 adriana paduos15 pietro panizza21 federica pediconi9 fiammetta querci22 antonio rizzo23 gianni saguatti24 alberto tagliafico25 rubina m . 
trimboli7 chiara zuiani11 francesco sardanelli7 , 26 received : 13 june 2016 / accepted : 16 august 2016 / published online : 6 september 2016 the author ( s ) 2016 . 
this article is published with open access at springerlink.com abstract women who were previously treated for breast cancer ( bc ) are an important particular subgroup of women at intermediate bc risk . 
their breast follow - up should be planned taking in consideration a 1.01.5 % annual rate of loco - regional recurrences and new ipsilateral or contralateral bcs during 1520 years , and be based on a regional / district invitation syste this activity should be carried out by a department of radiology integrating screening and diagnostics in the context of a breast unit . 
we recommend the adoption of protocols dedicated to women previously treated for bc , with a clear definition of responsibilities , methods for invitation , site ( s ) of visits , methods for clinical and radiological evaluation , follow - up duration , role and function of family doctors and specialists . 
these * francesco sardanelli francesco.sardanelli@unimi.it 1 romagna cancer registry , romagna cancer institute ( irst ) irccs , via piero maroncelli , 40 , 47014 meldola , forl , italy 2 dipartimento di scienze radiologiche , universit cattolica del sacro cuore , largo agostino gemelli , 8 , 0168 rome , italy 3 zadig scientific communication agency , via arezzo 21 , 00161 rome , italy 4 dipartimento di radiologia , u.o. 
della misericordia 15 , 33100 udine , italy 12 regional screening coordinating centre , veneto region , venice , italy turin , italy modena , italy italy italy 13 regional reference centre for breast cancer screening , 14 mammography screening centre , local health authority , 15 epidemiology unit , centre for cancer prevention , turin , 16 medical physics service , local health authority , modena , 17 dipartimento di diagnostica per immagini , radiologia 1u , universit di torino , a . 
citt della salute e della scienza di torino , via genova 3 , 10126 turin , italy 1 3 892 radiol med ( 2016 ) 121 : 891896 women will be invited to get a mammogram in dedicated sessions starting from the year after the end of treatment . 
 the planned follow - up duration will be at least 10 years and will be defined on the basis of patients age and preferences , taking into consideration organizational matters . 
 dedicated screening sessions should include : evaluation of familial / personal history ( if previously not done ) for identifying high - risk conditions which could indicate a different screening strategy ; immediate evaluation of mammograms by one or , when possible , two breast radiologists with possible addition of supplemental mammographic views , digital breast tomosynthesis , clinical breast examination , breast ultrasound ; and prompt planning of possible further workup . 
the following research issues are suggested : further risk stratification and effectiveness of follow - up protocols differentiated also for bc pathologic subtype and molecular classification , and evaluation of different models of survivorship care , also in terms of cost - effectiveness . keywords breast cancer follow - up mammography screening survivorship care introduction this position paper on recommendations for breast imaging follow - up of women with a previous history of breast cancer ( bc ) is the result of an agreement between the 18 u.o. 
radiologia senologica , irccs ospedale san raffaele , via olgettina 60 , 20132 milan , italy 22 department of prevention , screening centre , local health authority , sassari , italy 23 pathology department , local health authority , asolo , italy 24 senology unit , local health authority , bologna , italy 25 department of experimental medicine , dimes , institute of anatomy , university of genova , via de toni 14 , 16132 genoa , italy 26 department of biomedical sciences for health , universit degli studi di milano , via morandi 30 , san donato milanese , 20097 milan , italy italian group for mammography screening ( gisma ) and the italian college of breast radiologists ( icbr ) by the italian society of medical radiology ( sirm )  . 
the decision to provide this paper was taken at the end of a joint gisma / icbr - sirm workshop held in reggio emilia on may 8 , 2015 in the context of gisma annual meeting . 
the text has been approved by the gisma coordination board and the icbr - sirm board of directors . background in italy , according to the italian association of cancer registries ( airtum ) [ 1 ] , female bc survivors in 2015 were about 693 , 000 , equal to 2.2 % of female population and to 42 % of overall cancer prevalence among women . after conservative treatment , a peak of ipsilateral true loco - regional recurrences is observed during the first 5 years , in particular the first 2 years ; thereafter , this risk is progressively fading [ 2 ]  . 
conversely , the risk of a new primary contralateral bc and its cumulative incidence increase over time : the majority of these events are observed after the first 5 follow - up years [ 4 , 5 ]  . 
thus , the overall incidence of true loco - regional recurrences and of new primary bcs shows a steady annual rate of 1.01.5 % during 1520 years [ 7 ] , resulting in a continuous increase of the cumulative incidence [ 4 , 8 ]  . studies reporting higher relapse rates during the first 3 years [ 3 ] or 35 years [ 2 , 9 ] included true loco - regional recurrences , new primary ipsilateral bcs , and distant metastases but excluded the new primary contralateral bcs . 
women with a previous bc history should be considered as an important particular subset of women with an intermediate bc risk , lower than that of brca or p53 mutation carriers and higher than that of women with neither personal nor familial bc history , or with only sporadic bcs among their relatives [ 11 ]  . no evidence is available from randomized controlled trials on effectiveness of breast imaging follow - up in terms of mortality reduction . 
observational studies comparing 1 3 radiol med ( 2016 ) 121 : 891896 women undergoing different follow - up strategies including annual or biannual mammography versus no follow - up reported variable mortality reductions or an increased longterm survival independent of lead time [ 1215 ]  . 
no studies reported a comparison in terms of effectiveness between clinical / radiological follow - up in a diagnostic context versus invitation to a population - based organized screening program [ 16 ] ; moreover , no studies reported on the effectiveness of annual versus biannual follow - up mammography [ 15 ]  . the value of clinical breast examination ( cbe ) for women with a previous personal bc history is uncerta technical development of mammography ( in particular from film - screen to digital [ 17 ] ) and quality assurance programs reduced the rate of relapses diagnosed with cbe to only 15 % [ 10 ]  . 
moreover , cbe is a relevant occasion for getting information about the patients personal and family history in the context of a cancer survivorship care , paying also attention to psychological issues . no studies demonstrated a survival benefit from an earlier diagnosis of asymptomatic breast recurrence / relapse using magnetic resonance imaging ( mri ) [ 11 , 18 ] or breast ultrasound [ 11 ]  . international guidelines differ in many important issues of breast follow - up of women with a previous bc history : frequency of clinical mammography and possible cbe ; ( re ) inclusion in population - based organized screening programs and timing for this inclusion ; frequency of screening mammography also considering the individual risk profile [ 1923 ]  . 
as mentioned above , some medical societies and governmental bodies recommend a higher frequency of mammography and cbe during the first 35 years [ 19 , 22 , 23 ] , even though the temporal trend of the true locoregional recurrences and new primary ipsilateral and contralateral tumors does not support this recommendation . for population - based organized screening programs , the management of women previously treated for bc is an open issue . 
different policies are adopted at the regional level in some countries such as in canada , where some regional programs invite women previously treated for bc to screening mammography even though the data are excluded from standard statistical analysis of the programs performance [ 30 ]  . in italy , the gisma has so far recommended to exclude from invitation only those women who are certainly followed up at clinical centers . 
this practice is a matter for debate [ 31 , 32 ] because only half of health care districts are served by an active follow - up service and only half of programs ( re ) invite these women after a variable time since the bc event ( 2015 gisma survey , unpublished data )  . follow - up protocols also vary greatly in the diagnostic / clinical context , given the lack of reliable effectiveness studies [ 33 ]  . 
the screening practice too , whether organized or spontaneous , contributes to this variability : screendetected cancers amplify the heterogeneity of biological profiles of bcs as a length bias effect [ 34 ]  . 
only one model for risk estimation of annual loco - regional recurrence has been developed [ 35 ]  . the definition of breast imaging follow - up protocols for women previously treated for bc is necessarily influenced by the debate on organizational issues for bc care and , in a more general perspective , on follow - up in cancer patients . 
 on the one side , the breast unit model is increasingly applied as a territorial facility for multidisciplinary breast care , formally addressed by the european parliament in 2006 to support its general application in the european union from 2016 [ 36 ] and recently adopted in italy by the conferenza stato - regioni1 [ 37 ]  . 
on the other side , the concept of cancer survivorship care ( i.e. , the survival status as a phase of a continued cancer care ) [ 38 ] is progressively adopted by health systems . 
this phase starts at the end of primary treatment and should offer specialized comprehensive answers to the persons needs : information on life styles ; management of comorbidities and of side effects of treatments ; identification of long - term physical , psychological , and social effects of the disease and disease - related treatments ; identification of disease effects on families ; evaluation of survival quality . 
the complexity of these issues makes the breast unit the most appropriate facility for offering a comprehensive follow - up service to these women . however , we should not use the concept of cancer survivorship care to change the condition of women previously treated for bc into long - term survivors , taking into consideration also the economic impact of long - term intensive surveillance protocols . 
if we really evaluate the psychological impact of a bc diagnosis and of the subsequent recovery , after a first phase of intensive relationship of the patient with the facility where the treatment has been done , it appears to be important that we consider these women not as survivors but as an important subset of women at increased risk for bc . 
as a consequence , these 1 in official italian documents , the breast unit denomination has been translated into centro di senologia . 1 3 894 radiol med ( 2016 ) 121 : 891896 women should be included into invitation lists of screening programs , with a frequency and modalities adapted to the increased risk level . 
this strategy is derived from a comprehensive evaluation , not only from considering economic cost of prolonged intensive surveillance in the clinical setting . in this perspective , follow - up of women previously treated for bc should be active , i.e. , using a centralized invitation system , and have a territorial basis as an institutional activity dedicated to all prevalent bc cases . 
this approach should also protect all women previously treated for bc , providing them with a planned access to mammography also when , in the case of spontaneous surveillance , for different reasons such as other relevant familial events and psychological removal of the bc occurrence , the mammogram would be deferred or not performed at all [ 31 ]  . 
 moreover , in this way we could also offer a protection to those women who are treated for bc at major hospitals or cancer centers but live in different regions , as frequently occurs in italy . the general perspective is that screening and clinical breast imaging will be offered by the same department of radiology , in the context of a breast unit . 
the current implementation of the breast units in italy and their connection with screening programs have to be considered a transition process , which is relevant for the following recommendations . recommendations the breast unit should define a dedicated follow - up protocol for women already treated for bc . 
role and function of family doctors and bc specialists should be also defined . women already treated for any bc ( screen - detected bcs from organized population - based programs , interval cancers , bc cases diagnosed outside screening programs in asymptomatic or symptomatic women ) should not be excluded from screening invitation lists . 
screening programs , in the context of the breast unit , should invite for a mammogram those women treated for bc who reside in the catchment area , independently of the age at diagnosis and current womans age , at least up to 74 years of age , starting from the year following treatment . 
the follow - up duration should not be shorter than 10 years and will be defined on the basis of womans age and local considerations . if another service or center has included one of these woman in a follow - up program ( e.g. , the cancer center where the bc was treated ) and informs the breast unit of this , the breast unit should be open to make an agreement with the other service for excluding or including that woman in the invitation list . 
if the invited woman declares to prefer to be followed by another service , the breast unit should notify to this service the womans willingness and plan not to invite her for the time indicated by the other center . the dedicated screening sessions should be organized according to a defined protocol , here summarized as an indicative reference : investigation of personal / familial history ( if not already done ) to identify high - risk conditions for which a different screening strategy should be adopted ; 2 . 
cbe and possible breast ultrasound performed by a breast radiologist in the case of bilateral mastectomy ; immediate mammogram reading by a breast radiologist ( single reading ) or , when possible , by two breast radiologists ( blinded double reading ) ; immediate performance of supplemental investigations ( cbe , other mammographic views , tomosynthesis and / or breast ultrasound , and , whenever possible , needle sampling ) ; fast scheduling ( preferably within ten working days ) of further workup including , if indicated , mri , according to guidelines [ 17 , 18 , 39 ]  . the key point of the protocol should be the immediate communication of the results of the session to the woman , possibly with personal interaction between the breast radiologist and the woman and with a written report . in the case of single reading to reach a diagnostic conclusion to be immediately communicated to the woman , the second reading is waived considering that the comprehensive clinical evaluation can also include the above - mentioned supplemental techniques . 
however , although psychological issues would advise against a delayed second reading , this option can be considered if a high - quality interaction with the woman is undertaken.2 the breast unit should coordinate as much as possible the breast follow - up rounds and other follow - up visits , trying to allow the woman to have all visits on the same day . 2 when the delayed second reading is applied , the breast radiologist who works as first reader , in the case of suspicious finding ( s ) , will perform all suitable workup , while , in the case of negative evaluation , will give the woman the negative report in order to reassure her . 
however , at the same time , the radiologist will inform the woman that her mammograms will be read also in a delayed time by second reader ( according the usual protocol for screening mammography ) who occasionally could recall the woman for further workup . 
this information will be also included in the negative written report . 1 3 radiol med ( 2016 ) 121 : 891896 considering the special features of these dedicated sessions , costs should be specifically evaluated . 
payments should be differentiated from those of screening mammography offered to the general female population in the absence of bc history . data about screening results of women already treated for bc should be hived off from those regarding the general female population invited to screening and should be presented in dedicated annual reports , as happens in other countries [ 30 ]  . 
in particular , among the other usual indicators , attention should be paid to : crude and adjusted response rate ; prevalent bc cases ; quantity and quality of the offered service ; and womens satisfaction evaluation . 
 results from both single reading protocols and blinded double reading protocols ( either with immediate or delayed second reading ) will undergo an evaluation by the breast unit , paying careful attention to : ipsilateral or contralateral relapse diagnosed at stage t2 or greater ; interval cancer analysis ; in the case of delayed second reading , additional recall rate due to the second reading and compliance rate in the following rounds . from the viewpoint of the economic impact , apart from the already mentioned specific reimbursement negotiations , the authors evaluate that the cost cannot be superior to that implied by the current practice of annual cbe and mammography with or without breast ultrasound , commonly performed in women with previous bc history . 
however , the implementation of such a protocol will require time and specific organizational choices , also considering the inhomogeneity of breast unit organization in the italian regions . follow - up of women already treated for bc should be considered as a strategic area of bc research . 
value of double reading ( immediate or delayed ) when screening women already treated for bc , with studies specifically designed ( blinded sequential reading with or without arbitration , randomized controlled trials ) and including both ipsilateral and contralateral cases ; 2 . 
usefulness of a further risk stratification and effectiveness of different follow - up protocols , which may be tuned to pathologic and biomolecular features of the first bc and patients age and history and may be evaluated using surrogate endpoints ; 3 . 
farag2 received : 15 july 2016 / accepted : 16 august 2016 / published online : 1 september 2016 italian society of medical radiology 2016 abstract lung imaging radiopharmaceuticals are helpful agents for measuring pulmonary blood flow and allow detection of pulmonary embolism and lung cancer . 
99mtc - zolmitriptan is not a blood product and so it is more safe than the currently available 99mtc - maa , and its lung uptake is higher than that of the recently discovered 123i - ipmpd , 99mtc ( co ) 5i and 99mtc - dhpm . 
the physiological aspects of lungs are evaluated using radionuclidic lung imaging which allows diagnosis of pulmonary embolism and assessment of pulmonary perfusion before performing lung transplantation [ 2 ]  . 
besides , lung - specific radiopharmaceuticals are used for diagnosis and treatment of lung cancer [ 3 ]  . the most currently used radiopharmaceutical for lung perfusion scan is 99mtc - maa ( macroaggregated albumin ) [ 46 ]  . 
being obtained from human serum albumin is a major limitation of 99mtc - maa since it may cause infection by blood transmitted diseases as hepatitis b , hepatitis c and hiv [ 7 ]  . 
 research continues for new radiopharmaceuticals of higher lung affinity to be used as better lung imaging agents . lungs were discovered to function as a reservoir for compounds with high affinity to the serotonin transporter in 1998 [ 10 ]  . 
consequently , radiopharmaceuticals containing ligands with serotonin receptor affinity are expected to show good lung uptake . in this work , zolmitriptan ( a selective serotonin receptor agonist ) was radiolabeled with 99mtc to be used as a 1 3 936 radiol med ( 2016 ) 121 : 935943 potential radiopharmaceutical for lung scintigraphic imaging [ 11 ]  . 
the reaction mixture was shaken and left at different temperatures for different time intervals ( 5120 min )  . experimental materials and equipment zolmitriptan was obtained as a gift from amoun pharmaceutical industries company , cairo , egypt , and all other chemicals and solutions were purchased from merck co . 
on whatman paper sheet ( 2 cm width and 47 cm length ) , 57 l of the reaction mixture were placed at 12 cm far from the cathode edge of the paper sheet . electrophoresis is carried out for 1 h at voltage of 300 v using normal saline ( 0.9 % w / v nacl solution ) as electrolytes source solution . 
after complete development , the paper was removed , dried , and cut into strips , each strip is 1 cm length , and then each strip was counted in a welltype - counter . 
the percentage of radiochemical yield was calculated as the ratio of the radioactivity of 99mtc - zolmitriptan to the total activity multiplied by 100 . 1 3 radiol med ( 2016 ) 121 : 935943 determination of in vitro stability of 99mtczolmitriptan gamma scintigraphy the reaction mixture was left at ambient temperature for 24 h and 35 l samples were taken from it at different time intervals . 
the radiochemical yield of the samples was measured by paper chromatography , tlc and paper electrophoresis . molecular modeling of 99mtczolmitriptan molecular modeling was performed to predict the most favorable structure of 99mtc - zolmitriptan and to ensure that complexation with 99mtc will not affect the binding of zolmitriptan to its target . 
molecular modeling is the application of computers to generate , manipulate , calculate and predict favorable molecular structures and associated properties [ 15 , 16 ]  . the main strategy is taking in consideration the energy of the produced complex and the bond length between 99mtc atom and the proposed coordinating atoms in the zolmitriptan molecule . 
the decrease in the energy of the radiolabeled molecule indicates the high stability of such complex and increases the probability of its formation . biodistribution studies of the 99mtczolmitriptan in normal mice the experimental procedures of the biological studies were done in accordance with the guidelines set out by the egyptian atomic energy authority and were approved by the animal ethics committee , labeled compounds department . 
aliquots of 150 l containing 6.2 mbq of the 99mtc - zolmitriptan were injected into each mouse via the tail veeach mouse was weighed then anesthetized by chlorofor samples of fresh blood , bone and muscle were collected in pre - weighed vials and counted . 
 were reported and all the results were given as mean the level of significance was set at p < 0.05. gamma scintigraphic imaging was done in the nuclear medicine unit of the national cancer institute , cairo university , egypt . 
the body distribution profile in mice was recorded in the gamma camera with a 5 - mm pinhole collimator , window setting of 140 kev , and 20 % width . 
as noticed , there is no colloidal species other than 99mtco2 obtained in the reaction which is a major advantage of using na2s2o4 as a reducing agent in preparing technetium radiopharmaceuticals avoiding colloidal stannic oxide interference for stannous chloride prepared radiopharmaceuticals [ 24 , 25 ]  . 1 3 939 radiol med ( 2016 ) 121 : 935943 % 99mtc - zt % free 99mtc % r - h 99mtco2 table 1 2d , 3d structures and potential energies of the proposed 99mtc - zolmitriptan complexes complex zolmitriptan e = 0.35748 kcal / mol 2d structure zolmitriptan 3d structure reaction temperature ( c ) fig . 
reaction conditions : 2 mg zolmitriptan , 30 mg of na2s2o4 , 20 l ( 51.5 mbq ) of 99mtco4 solution , ph 6 , 45 min ( a ) ( most favorable ) e = 135.265 kcal / mol 2d structure effect of reaction time results in fig . 
increasing the reaction temperature to higher degrees ( 4080 c ) increased the rate of side decomposition reactions causing a significant decrease in labeling yield [ 22 ]  . in vitro stability study the effect of time on the in vitro stability of the 99mtc - ligand complex was studied in order to determine the most suitable time during which the radiopharmaceutical kit can be used . 
 oxidation or hydrolysis of the 99mtc - ligand complex may take place during storage after being labeled with technetium , this occurs in addition to the effect of ionizing - radiation [ 27 ]  . 
 99mtc - zolmitriptan showed a good in vitro stability up to 24 h . molecular modeling results 3d structure ( b ) e = 256.27 kcal / mol 2d structure 3d structure the different probabilities of the complexation pattern of zolmitriptan with 99mtc were energetically minimized using protocol of discovery studio module ( table 1 )  . 
the bond lengths between zolmitriptan and 99mtc were measured and the energies of the resulting molecules were calculated by charmm force - field simulation algorithm . 1 3 940 table 1 continued ( c ) e = 193.9 kcal / mol 2d structure radiol med ( 2016 ) 121 : 935943 3d structure ( d ) e = 200.04 kcal / mol 2d structure 3d structure ( e ) e = 310.766 kcal / mol 2d structure 3d structure complexes ad represent coordination manner between two molecules of zolmitriptan with one atom of technetium , while complex e represents coordination manner between one molecule of zolmitriptan with one atom of technetium . the most energetically favored proposed complex was a as it has the lowest energy ( e 135.265 kcal / mol )  . 
since zolmitriptan is a selective serotonin receptor agonist of the 1b and 1d subtypes , two essential sar requirements are presence of indole ring and linkage of the basic nitrogen to the 3 - position of the indole ring [ 28 ]  . 
in addition , 99mtc - zolmitriptan showed a good retention in lungs up to 1 h post - injection which allow a sufficient time for lung imaging with a good resolution . 
the patients were preliminarily studied with mri and suprapubic and transvaginal ultrasound examination including rte ; the follow - up was performed immediately after treatment , at 3 months and 12 months with the same technique . 
at the time of statistical analysis , 12 / 21 patients reached the 12 - month follow - up : they showed a further reduction of sr . conclusion rte is a valid method able to support standard ultrasound examination in the evaluation of uterine fibroids , since it allows demonstrating the decrease of rigidity , which can be quantified with the sr parameter . 
it could be included in a pre - treatment multiparametric evaluation of patients looking for mrgfus eligibility and in followup when it could assess the response to treatment . keywords mrgfus ( magnetic resonance - guided focused ultrasound surgery ) ultrasound elastography uterine fibroids transvaginal us introduction uterine fibroids are the most frequent benign tumors of myometrial origin with an incidence ranging from 20 to 40 % in reproductive age women [ 1 , 2 ]  . 
they are composed of the same smooth muscle fibers as the uterine wall and fibrous connective tissue in various percentages . estrogens , growth hormone and progesterone influence their growth rates [ 3 ]  . in 5060 % of cases , fibroids are asymptomatic and their diagnosis is incidental . 
the most common symptoms are 1 3 radiol med ( 2016 ) 121 : 926934 abnormal uterine bleeding [ 4 ] , dysmenorrhea , bulk symptoms of pressure , pelvic pain and infertility . the severity of symptoms plays a crucial role in the choice of the therapeutic approach , which can range from medical treatment ( gnrh analogs , oral contraceptive and progestins ) to surgery . 
other uterinesparing therapeutic options include myomectomy , uterine artery embolization ( uae ) and magnetic resonance guided focused ultrasound surgery ( mrgfus ) [ 6 ]  . mrgfus is a totally non - invasive thermal ablation procedure for treating symptomatic uterine fibroids [ 7 ]  . mrgfus is based on the use of high - intensity focused ultrasound waves delivered by an extracorporeal transducer to generate high temperatures within the target tissue ( > 56 c ) with consequent cell death and coagulative necrosis without damage to the surrounding area . careful selection of patients is crucial for the success of the treatment : potential candidates are screened with pelvic mri to determine if they meet the patient selection guidelines outlined by yoon et al . 
the aim of the treatment is to ablate as much of the fibroid as possible , with multiple sonications targeting different portions [ 9 ]  . according to other clinical experiences , the resulting non - perfused volume ( npv ) , as assessed at post - treatment magnetic resonance with gadolinium , at more than 70 % represents an effective treatment [ 10 , 11 ]  . real - time elastography ( rte ) is a us complementary technique that studies the elastic properties of the examined tissue , improving the characterization of lesions . real - time elastography is based on slight external tissue compression by the us probe on the examined structures ; this compression produces displacement within the tissue , with subsequent calculation of the strain profile along the axis of compression . strain is the level of deformation and is inversely proportional to stiffness : soft tissues are more easily compressible , presenting a higher value of stra real - time strain ratio ( sr ) between healthy and pathological tissue is a useful quantitative parameter that is possible to calculate . according to the color map scale , the stiffness of the tissue is represented in a range of colors from red ( soft ) to blue ( hard )  . although uterine fibroids are composed of the same smooth muscle fibers as the myometrium , they are many times denser ; this is the reason why they appear stiffer at rte . mrgfus on uterine fibroids determines the colliquative necrosis of the treated lesions and , as shown in the literature , reduction of symptoms without substantial reduction of volume . 
mri with gadolinium shows reduction of vascularized tissue ( npv ) in patients effectively treated , but the reason why symptoms reduce is still not clear . we assume that fibroids become softer and less compressive on endometrial layers , leading to reduction of bleeding and pain and increase of fertility . ultrasound elastography could explore the elastic pattern of fibroids before and after treatment . the objective of our study was to evaluate the usefulness of rte in the characterization of uterine fibroids before and after treatment with mri - focused ultrasound . materials and methods twenty - eight women , with a total of 34 uterine symptomatic fibroids ( average age 38 years , range 3048 years ) , had been selected for mrgfus treatment ( exablate 2000 ; insightec , haifa , israele ) in a time period of 1 year and were enrolled . the research ethics committee approved this prospective study and all patients signed the informed consent form . inclusion criteria required at most three fibroids eligible for mrgfus treatment ( symptomatic patients , who had not undergone surgical approach before , with at least one fibroid bigger than 10 cm , hypointense on t2 - weighted mri , not exophytic or pedunculated ) and good visualization of the fibroid with transvaginal scan . 
exclusion criteria were : more than three treatable fibroids , mri imaging indicative of leiomyosarcoma , hypointense lesion on t2w imaging , distance from the skin and the fibroid more than 12 cm , fibroids close to the lumbosacral plexus or to another bone surface , air - containing tissues or bone between transducer and fibroid , poor visualization of the fibroid with transvaginal us and no possibility to perform transvaginal examination . the eligible patients were preliminarily studied with suprapubic us , with convex probe 25 mhz , then with transvaginal us , with intracavitary probe 3.38.8 mhz ( aplio 500 , toshiba medical systems europe , zoetermeer , the netherlands )  . 
this preliminary us study ( t0 ) included assessment of the lesions in b - mode ( max diameter ) , color and power doppler with measure of resistance index ( ri ) , and elastographic study . 
the preliminary mri study ( discovery mr750 3 - tesla machine general electric , milwaukee , wi , usa ) was performed with t2 - weighted and t1 - fat suppression weighted sequences , before and after contrast media acquired in multiple planes and was useful for collecting volume and maximum diameter information ( respectively , cm3 and cm )  . after mrgfus treatment , follow - up with transvaginal rte was planned immediately after treatment ( within 2 h after treatment conclusion , t1 ) and at 3 months ( t2 )  . 
the protocol consisted of two cycles of compressions ; the correct pressure could be checked as a sinusoidal curve on a chart appearing in real time at the bottom of the elastogram . the sr measurement was determined by comparing the strain in two manually selected regions of interest ( roi ) on the best elastograthe target roi is centered on the leiomyoma ( size 1015 mm ) and the reference roi is placed on the surrounding myometrium at the same depth . 
different sizes of target roi were drawn : big target roi , the same size as the fibroid , and small target roi , of similar size to reference roi , placed in five standard regions of the fibroid . the sr is the ratio between the target roi and reference roi . we selected five big target roi and five small target roi for each cycle of compression , and the strain ratio was automatically calculated for each roi by toshibas software . at the end of the mrgfus procedure , the non - perfused volume ( npv ) was measured . all patients were evaluated at t0 , t1 and t2 ; only 12 patients reached the t3 follow - up at the time of the statistical analysis . as of today , no previous experience in the literature regarding the elastographic evaluation of uterine fibroids treated with mrgfus is available . 
the npv ratio of the 27 treated fibroids was 69 % ( range 1699 % ) ; 14 / 27 fibroids had an effective treatment with npv > 70 % , and the remaining had incomplete treatment ( npv < 70 % )  . 
therefore , the statistical analysis was performed on big roi data . discussion it has been widely demonstrated in the literature that the clinical outcome of mrgfus fibroid treatment primarily depends on the non - perfused volume ( npv ) measured on contrast - enhanced t1 - weighted imaging immediately posttreatment [ 12 , 13 ]  . the literature shows npv from 30 to 80 % , with very variable volumetric decreases ( from 15 to 40 % ) [ 14 ]  . 1 3 930 radiol med ( 2016 ) 121 : 926934 fig . 
b t1 postgadolinium axial plane shows the highly perfused fibroid sufficiently distant from the sacral surface and with minimum distance from the skc at the end of the mrgfus treatment , t1 - weighted gadolinium - enhanced axial image is performed to demonstrate the effect of the ablation and to calculate the area of nonperfused volume corresponding to coagulative necrosis ( npv 71 % )  . 
 axial t1 post - contrast scan at 3 months ( d ) and 12 months follow - up ( e ) showing the fibroid volume reduction good selection of patients is the most important parameter able to predict treatment success : patients have to be symptomatic and symptoms must be correlated with uterine fibroids . 
they showed that ultrasound strain imaging does provide differentiation between normal uterine muscle tissue and pathologies such as leiomyomas , and that a uterine leiomyoma may be better distinguished from the normal surrounding myometrium on strain images by the presence of a slipping artifact at the boundary of the leiomyoma [ 12 ]  . in 2009 , the french group of ami performed real - time transvaginal elastography in ten patients with uterine fibroids to demonstrate the feasibility of the technique to map and characterize these lesions [ 13 ]  . our experience is the first in vivo study exploring the utility of elastography to evaluate the modifications of elasticity in uterine fibroids after mrgfus treatment . 
these results are concordant with those in the literature [ 13 , 15 ]  . 1 3 radiol med ( 2016 ) 121 : 926934 of sr values ( average increase of 50 % ) immediately after treatment , demonstrating our hypothesis : rte parameters can be used immediately after treatment to verify effective treatment , adding useful information to ce - mri . the percentage of sr decrease at 3 months follow - up is positively and significantly correlated with symptom reduction ( p 0.001 ) : patients who responded well to the treatment had a decrease of sr , while patients who did not respond had an increase of sr already after 3 months . therefore we can state that in our cohort of patients , elastographic evaluation could predict the treatment efficacy and could have an important role during the follow - up of patients with uterine fibroids treated with mrgfus . our experience needs to be confirmed with more data , which are necessary to consolidate these results and could draw attention to some pre - treatment characteristics . in our study , we had some ineffective treatments . 
two patients presented an increase of volume , a worsening of symptoms and increase of sr as compared to t0 : these patients had an ineffective treatment with an npv of 30 and 16 % . multiparametric usrte could be useful to complete the evaluation of patients treated with mrgfus and support mri examinations during follow - up , as it is able to fig . 
the strain ratio is evaluated by comparing the mean strain in a region of interest centered on the myoma ( big , light pink target roi ) , with the mean strain in a region of interest in the surrounding myometrium ( small , light yellow reference roi ) , and by choosing the best curve in the elastograthe strain ratio value was 4.47 at t0 ( a ) , 22.1 at t1 ( b ) , 3.56 at the 3 months follow - up ( c ) and 2.70 at t3 ( d ) immediately after treatment , the evaluation of the same myomas showed a significant increase of sr , with a median of 7.68. 
we explained this response with a reactive change : the treated fibroids , especially the ones efficiently treated ( npv > 70 % ) , had an increase in their stiffness within 2 h after treatment , since coagulative necrosis and inflammatory fall from mrgfus produce intralesional tension with increase of rigidity of the lesion itself . 
on these days , the inflammatory reaction is replaced with complete coagulative necrosis and granulation tissue , which will determine the decrease of stiffness and symptoms . we showed that all patients with > 70 % npv at t1 technically efficient treatmenthad significant increase table 2 summary of volume , symptoms , resistance index and strain ratio changes in case 1 , figs . 
a at time 0 , t2 coronal mri image shows hypointense fibroid with hyperintense central area ( hyaline degeneration ) , b highly perfused on t1 post - gadolinium axial plane . 
 note how the b - mode ultrasound imaging at t0 showed a heterogeneous hyperechoic fibroid , as hyaline degeneration 1 3 radiol med ( 2016 ) 121 : 926934 table 3 summary of volume , symptoms , resistance index and strain ratio changes in case 2 of figs . 
3 and 4 volume ( t0 ) volume ( t2 ) volume t0 / t2 symptoms ( t0 / t2 ) 158 mm3 48 % 210 mm3 33 % ri resistance index , sr strain ratio , npv non - perfused volume 24 % 113 % 37 % one more observation concerns the menometrorrhagic symptoms , which could be caused by other gynecologic pathologies , leading to wrong interpretation . 
in few occasion the trans - vaginal ultrasonographic anatomy and the location of the fibroid compared with the myometrium imposed us to draw the target roi deeper than the reference roi , with consequent possible bias . the introduction of recent techniquesas new elastographic software with the automatic positioning of the roi and the possibility to control the cycles of compression with a reference boxseems to be a good method to improve the reliability . however , this preliminary study permitted to gain experience in endocavitary elastography and opened the door to future studies . conclusions mrgfus is a method for treating uterine fibroids in symptomatic patients who want to preserve fertility . 
 this event can be explained by the reduction of the stiffness of the fibroids , due to the substitution of the solid tissue with coagulative tissue . rte allowed us to demonstrate that after treatment , the fibroids show a decrease of their rigidity , which can be quantified with the sr parameter . 
if the results are confirmed in a much larger study population , usrte could even substitute mri at the 3 months follow - up . significant symptom reduction was found already at the 3 months follow - up , with a median decrease of 36 % . 
we observed a variable response to the treatment in patients with partial ablation , not completely reasonable , varying from the significant symptom increase in patients with an npv of 40 % to a remarkable and not - justified symptom reduction ( up to 60 % ) in incomplete treatments ( npv 32 % )  . these results led us to some observations . 
first of all , the questionnaires to evaluate the symptoms are tentative to quantify a complex symptomatology and this leads to discordant results compared to the real modification of symptoms . 
this is the reason why the fsfi and kh - qol questionnaires , first included in the protocol , were then excluded from statistical evaluations , since patients showed difficulties in the interpretation of questions , with consequent lack of data . 1 3 934 radiol med ( 2016 ) 121 : 926934 the same treated fibroids time , successfully ( npv > 70 % ) presented a significant increase of their sr immediately after treatment : coagulative necrosis and inflammation produce intralesional tension and increase the rigidity of the lesion itself . at the 3 months follow - up , patients with npv > 70 % had a good reduction of symptoms , a little decrease of size and a significant decrease of sr , compared with not efficiently treated patients . in conclusion , real - time elastography could be a valid method , able to support standard ultrasound examination in the evaluation of uterine fibroids . 
especially in symptomatic patients , it may be included in a pre - treatment multiparametric evaluation to allow a better selection of patients for the most suitable treatment . real - time elastography could also be important during follow - up : immediately after treatment ( when the multiparametric evaluation could predict the response to treatment ) and at 3 months follow - up ( when it has the potential to substitute mri ) , since it is able to evaluate the decrease of size and vascularization , as well as changes in stiffness . compliance with ethical standards conflict of interest chiara marigliano declares that she has no conflict of interest . 
visual analog scale ( vas ) score was used to evaluate treatment efficacy in terms of pain palliation while adc maps obtained by dwi sequences , and dce data were used for quantitative assessment of treatment response at imaging . 
on the basis of vas score , 16 ( 69.6 % ) patients were classified as complete clinical responders , 6 ( 26.1 % ) as partial responders and only one ( 4.3 % ) was classified as a non - responder . 
similarly to what happens for other non - surgical treatment modalities , including radiation therapy and percutaneous ablation , also for mrgfus clinical scores are the main instrument for the assessment of pain palliation , since objective imaging indicators of clinical outcome are still a matter of research and clinical debate . 
in particular , imaging evaluation of treatment response in bone metastatic disease relies on the identification of morpho - dimensional changes of target tumors by morphologic imaging , including computed tomography ( ct ) and magnetic resonance imaging ( mri ) , as well as on the demonstration of treatment effects on tumor activity with functional imaging , including bone scintigraphy and ct - pet [ 5 ]  . 
in this scenario , an earlier assessment of treatment response using a non - invasive and objective imaging technique is appealing , as it might allow treatment regimens changes depending on the effective tissue response [ 8 ]  . 
functional and metabolic mri techniques may provide the ability to assess biological changes acting as indicators of therapy response [ 912 ] ; in particular , some authors proposed that dwi and dce would be useful in the evaluation of lesions during the early phase of therapy , providing tools to evaluate the efficacy of treatments targeting bone lesions [ 1317 ]  . 
the objective of this study was to assess the correlation between functional mri , including adc values obtained from dwi and dce , and clinical outcome in patients with bone metastases treated with mrgfus . materials and methods patients and study design local ethics committee approved this prospective study and written informed consent was obtained from all the patients . 
among 42 initially screened patients , twentyeight consecutive subjects ( mean age , 62.1 years ; range , 3782 years ) with symptomatic bone metastases from known primary cancer referred for palliative mrgfus treatment fulfilled all inclusion and exclusion criteria ( table 1 ) and were included in the current study between february 2013 and december 2014 . 
five patients were dismissed from the study after initial inclusion ( two for informed consent refusal , two for death before follow - up , one lost at follow - up )  . 
the final study population included 23 subjects . mrgfus treatments were performed with a focused ultrasound phased - array treatment system ( exablate 2100 , insightec , tirat carmel , israel ) integrated within the mri scanner . preprocedure preliminarily to mrgfus , all patients underwent unenhanced ct scan ( somatom sensation 64 - mdct , siemens , erlangen , germany , 120 kv , 200 mas , detector configura0.6 , slice thickness 1 mm , reconstruction intertion : 64 val 1 mm ) and mri ( 3t unit , discovery 750 , ge healthcare , milwaukee , wi , usa ) with conventional sequences ( axial and coronal t1 - weighted sequences , axial and coronal t2 - weighted sequences , axial and coronal t1and t2 - weighted sequences with fat signal saturation ) , dwi and dce sequences and a final post - contrast t1 - weighted sequence ( table 2 )  . 
eligible patients underwent a pre - procedural evaluation by a radiologist and anesthesiologist , discussing the indications , benefits , and additional risks of the procedure with each patient and his / her immediate family . procedure based on preliminary imaging findings , patients were placed in the optimal position to align the metastatic lesions with the ultrasound transducer housed in the scanner table . 
treatment planning started with the acquisition of sagittal and axial t1 - weighted and t2 - weighted mr images with and without fat suppression in order to localize the target lesion and to allow correct 3d planning . 
the system generates a patient - specific treatment plan including the optimal energy level and the number of sonications required , avoiding damage to non - target tissue and minimizing the total duration of the treatment . 
although mr thermal maps cannot be calculated directly in the bone itself ( due to the absence of moving protons in the cortical zone ) , heating due to conductive processes from the bone surface within the adjacent soft tissue was measurable and considered adequate for treatment monitoring [ 18 ]  . 
only patients who required general anesthesia remained in the hospital overnight . postprocedure to evaluate treatment efficacy in terms of symptoms palliation , pain severity was evaluated using the vas score . 
treatment response was defined based on international bone metastases working party guidelines on palliative radiotherapy endpoints for clinical trials , according to which partial response ( pr ) is defined as a drop of two points in the vas score without an increase in pain medications or a drop of 25 % in pain medication without increase in the reported pain score , complete response ( cr ) is defined as a pain score of 0 on the vas score without medication increase , while no response ( nr ) is defined as no drop in the vas score and no changes in medication use [ 19 ]  . 
the percentage of increase in adc ( adc % ) was evaluated as a quantitative parameter of treatment response by comparing pre - treatment and post - treatment values , as previously described . 
the average mrgfus treatment length was 110.4 min ( range : 55 - 180 min ) , with a mean of 23.5 ( range 1529 ) sonications , with mean sonication energy of 1644 joule ( range : 8602899 j ; mean acoustic power : 114 watt )  . 
figure 1 shows the vas score changes at follow - up in both responder groups . imaging evaluation on the basis of clinical outcomes patients were divided into two different groups : 16 were classified as complete responders and 6 as partial responders . 
non perfused volume ( npv ) in terms of percentage was evaluated basing on the comparison between preand post - treatment final post - contrast t1 - weighted sequence . statistical analysis we analyzed data distribution using a descriptive statistical examination . 
the adc and dce data value were considered as continuous variables , while vas scores did not show , as expected , a gaussian distribution and were therefore considered a non - parametric variable . 
we evaluated the significance in differences between baseline and posttreatment adc and dce data using the paired sample t test for comparison of means , while vas score differences were assessed by wilcoxon test for ordinal scales . 
the relationships between the per - patient vas score and adc and dce parameters , from baseline through follow - up examinations , were evaluated by the spearman rank correlation coefficient ( scc ) test to assess the ability of the different parameters to indicate palliative and radiological response induced by treatment . 
among other dce parameters , ktrans significantly changed in complete responders ( 3 months ktrans kt 52.65 % p < 0.01 ) and was not significantly different in partial responders ( 3 months ktrans 0.042 / min ; kt 11.39 % p > 0.01 ) , whereas ve did not revealed significantly different changes between complete ( 19 % p > 0.01 ) and partial responders ( 5.6 % p > 0 , 01 )  . 
in this patient , npv was 20 % at 1 , 3 and 6 months . discussion metastatic bone disease is a common manifestation of advanced cancers with a greater prevalence in breast and prostate cancers ( more than 70 % ) , causing much of the morbidity and disability in these patients . 
3 iliac bone metastasis from breast cancer ( arrows ) with dwi hyperintensity in premrgfus exaadc values were significantly modified by mrgfus treatment , in particular adc parameters showed a steady increase over follow - up exams . 
 in this case , vas value decrease from 8 to 1 and the patient was classified as complete responder ( cr ) ( radiation therapy , radiofrequency ablation , mrgfus )  . 
 therapy goals are to delay progression , symptoms palliation , improve quality of life and lead to survival benefit if possible [ 20 , 21 ]  . non - invasive response biomarkers for treated bone metastases are currently needed , since there are not fully accepted methods for assessing tumor response in skeletal sites with disease . 
bone scintigraphy or cross - sectional imaging , such as computed tomography ( ct ) or magnetic resonance imaging ( mri ) are the commonest imaging methods used to evaluate bone marrow metastases ; several pet tracers have been also used to monitor bony therapy response . 
with regard to mri , different sequences have been taken into account for this purpose ; among conventional sequences , t1 - weighted spin echo , t2 - weighted sequences with fat suppression and short tau inversion 1 3 radiol med ( 2016 ) 121 : 905915 fig . 
 after treatment , the adc value increased at 1 - month follow - up and then showed a decreasing trend at 3and 6 - month controls recovery are usually considered as the most useful in bone evaluation [ 20 , 21 ]  . 
in particular , various studies successfully evaluated the role of dce in the assessment of metastasis and normal bone marrow vascularization , with emphasis on the decrease of perfusional parameters after chemotherapy [ 22 , 23 ]  . 
even more encouraging results have been obtained with the use of dwi sequences adapted to bone imaging ; indeed , the role of dwi in the identification , characterization and post - treatment followup of solid tumors has been explored in several clinical scenarios , ranging from liver to lung tumor [ 24 , 25 ] , and the results obtained in the evaluation of bone lesions are in line with those described in these studies . 
in particular dwi is extremely sensitive to restriction to water diffusion in tissues with high cell density and bone marrow perfusion [ 22 , 26 ] and can easily identify effects of chemotherapy and radiation therapy in various types of bone tumors [ 20 , 21 , 27 ] , with excellent correlation with conventional metabolic imaging modalities , such as bone scintigraphy and pet [ 28 ]  . our study evaluated the potential role of adc values obtained from dwi sequences and dce parameters in assessing the clinical response to focal ablative therapy , by examining statistically significant changes in their values and the correlation with vas analysis in patients with bone metastases treated with mrgfus . 
after tests in several preclinical and animal models [ 29 , 30 ] , dwi with adc maps has been clinically proved to be a promising non - invasive imaging technique to assess response to conventional and biological treatment in various solid tumors , including primary [ 31 ] and secondary lesions [ 32 ] , and to be capable of prospective prediction of treatment outcome [ 3337 ]  . 
the potential role of dce in normal and abnormal bone marrow and in benign and malignant musculoskeletal lesions has been studied in early clinical trials , obtaining useful information on tumor response to new treatments , such as those targeting tumoral angiogenesis [ 3840 ]  . 
in six patients there was a clinical partial response to mrgfus treatment with a significant decrease in the vas scale at 1 month and no significant modifications at three and six ; also in these patients the adc values were increased , but while at the 1 - month follow - up the trend was similar to that of complete responders , at 3 and 6 months there was a slight decrease of adc values , from the baseline exam , but with a sharp drop compared to previous control . 
 in light of these results , even though observed in a small patients population , we can assume that the different trend of adc values and dce data between complete and partial 1 3 912 radiol med ( 2016 ) 121 : 905915 fig . 
this observation is in agreement to what reported in previously published studies [ 15 , 43 ] performed in other organs after conventional therapies [ 23 , 25 , 27 , 44 ]  . 
the proposed mechanism for mrgfus - induced pain palliation is the thermal lesion of periosteal pain receptors ; however , the coexistent ablation of the tumor mass may reduce the pressure on adjacent healthy tissues , contributing to pain palliation [ 45 ] ; hence a relevant increase in adc values of ablated bone metastases could reflect pathophysiologic alterations that occur after ablative therapy not only in the periosteum but also in the tumor mass , including bone remodeling with osteocytic and interstitial elements replacing necrotic cancer tissue [ 23 , 25 , 27 , 44 ]  . 
at the same time , it should be noted that a slight increase in the adc value or instability of this increase at follow - up may correspond to a suboptimal mrgfus ablation , with persistence of viable 1 3 radiol med ( 2016 ) 121 : 905915 tumor tissue in the ablation area and incomplete symptoms control during time [ 23 , 25 , 27 , 44 ]  . 
lastly , for what can be observed in the single case of complete treatment failure , a minimal increase in the adc value 1 month after ablation would be indicative of no response to treatment . 
 with regards to dce , shortly after contrast media injection , the tracer diffuses into the extravascular space , inducing changes in the signal intensity which can be studied either qualitatively , semi - quantitatively or quantitatively , resulting in different parameters to be analyzed . 
since ktrans significantly changed in complete responders , but not in partial responders , a potential role of dce in precociously assessing treatment response can be hypothesized , even though no significant correlation has been observed between other dce data and vas . 
unfortunately , dce studies have not been widely used in clinical practice ; several dce parameters have been evaluated in previous studies ( maximum intensity , slope of the curve and contrast washout among others ) , but they have been studied with special focus on normal vertebral marrow more than on pathological conditions [ 20 ]  . 
last , for what regards the usefulness of npv , our data demonstrate a low reliability of this technique , probably due to the fact that mrgfus - induced pain palliation can be obtained by direct tumor ablation ( with subsequent devascularization of bone lesions ) , by periosteal denervation ( without effective ablation of underlying tumor tissue ) or a combination of both ; in our population , the correlation between vas and npv was not significant and npv values were similar in the complete responders and partial responders groups , in accordance with the above mentioned factors . our study has several limitations . 
first of all , the sample size was relatively small and our results are therefore to be regarded as preliminary ; specifically , the presence of only one non - responder patient makes the study less effective for what regards the evaluation of treatment failure and related factors . 
another relevant limitation is represented by the absence of a control group ; at this regard , a phase ii study is ongoing at our institution , enrolling patients in a double arm , randomized trial with radiotherapy as a second ar finally , histological evidence was not available for comparison with adc and dce parameters changes , since percutaneous biopsy or surgical resection of bone metastases is performed just occasionally and obtaining histological samples of lesions that have been previously confirmed as metastases at imaging would not have been ethical in this clinical setting . in conclusion , our results demonstrate that mrgfus is a feasible and effective procedure for palliative treatment of bone metastases and that adc and dce parameters modifications in treated lesions correlate with clinical findings and could be used to predict treatment outcome ; anyway , these correlations need to be confirmed in a larger cohort of patients . 
the aim of this study was to explore whether the ratio of hepatic arterial to total liver blood flow ( hepatic perfusion indexhpi ) and the area under the enhancement curve ( auc ) of selected liver areas in patients with hepatic metastases from colorectal cancer treated with first - line chemotherapy could predict response and / or be a prognostic variable . patients and methods sequential liver dce - mri studies with morphological imaging reconstruction were performed in 43 consecutive patients at baseline and every 3 months during oxaliplatin - based first - line chemotherapy . 
 data about hpi of the whole liver , and auc of metastatic and healthy areas were calculated at each time - point and compared both at baseline and sequentially during the treatment . results baseline hpi and auc values did not discriminate patients responsive to chemotherapy , nor those with better survival outcomes . 
luigi hospital , university of torino , orbassano , turin , italy discussion our results did not support the hypothesis of a predictive or prognostic role of hpi and aucs calculated by dce - mri in liver metastatic crc patients , thus the primary endpoint of the study was not reached . 
curative resection in selected patients has been proposed since early 60s and became largely accepted in the 80s [ 3 ] , because a higher proportion of long - term survivors was observed with the surgical approach than in unselected series of patients treated with chemotherapy alone . 
in this context , any predictive and / or prognostic variable that may help to identify the best therapeutic strategy would be clinically useful . 1 3 radiol med ( 2016 ) 121 : 950957 the efficacy of chemotherapy depends not only on drug pharmacodynamics , but also on several other factors , such as the delivery of cytotoxic drugs through the tumor vasculature , drug uptake and retention in tumor cells , metabolic activation of pro - drugs , intrinsic chemosensitivity of tumor cells , catabolism and excretion of drugs , and by the total amount of drugs reaching tumor cells . 
portal vein perfusion accounts for 6080 % of the total physiological liver blood supply , because only a limited proportion of blood supply to the normal liver comes through the arterial vessels , whereas in liver metastases the vascular supply derives predominantly from the hepatic artery . 
the ratio of hepatic arterial to total liver blood flow ( hepatic perfusion index , hpi ) was first investigated using dynamic scintigraphy and was found to be abnormal in 88 and 58 % of colorectal cancer patients with and without liver metastases , respectively [ 5 ]  . 
in these studies , hpi was determined preoperatively in patients without metastases who underwent curative resection of the primary tumor , and patients with higher hpi presented shorter disease free and overall survival . 
in the metastatic setting hepatic basal hpi , measured by dce - mri , was increased in metastatic patients [ 9 ] but no data are available about hpi changes following chemotherapy . using dce - mri , the area under the enhancement curve ( auc ) is another parameter that can be used to assess the blood flow of selected areas of the liver . 
decreases in auc calculated from a region - of - interest ( roi ) including the whole liver were demonstrated to correlate with tumor shrinkage and with a better time to progression in patients treated with standard chemotherapy plus bevacizumab [ 10 , 11 ]  . however , in all the above - mentioned studies , imaging acquisition and reconstruction protocols did not allow a morphological evaluation of the liver , preventing any measurement of the metastases . 
the aim of this study was to prospectively evaluate the correlation between hpi and activity of first - line chemotherapy in terms of response rate and survival , and to assess the potential role of auc computation in normal and neoplastic hepatic areas by dce - mri , based on a protocol of image acquisition and reconstruction that in addition allows the morphological evaluation of the liver . patients and methods study design patients with liver metastases from colorectal cancer , without contraindications for first - line chemotherapy , received an abdominal dce - mri at baseline , at 3 months , and eventually at 6 months after the initiation of chemotherapy . 
the study aimed to demonstrate an increase in overall response rate ( orr ) in patients with hpi values > 0.3 ( hpi high group ) with 0.3 ( hpi low group )  . 
hypothrespect to those with hpi esizing an orr of 50 % in hpi high group and of 25 % in hpi low group , with error of 0.5 and error of 0.2 , the total number of patients to be enrolled was 106 ( 53 per arm )  . 
 hpi and auc were calculated using philips viewforum perfusion t1 software . hpi represents the ratio of hepatic arterial to total liver blood flow and it is calculated from a time intensity curves derived from regions of interest ( roi ) drawn manually in the aorta , liver and spleen . 
arterial perfusion ( part ) is calculated by dividing the peak gradient in the liver during 1 3 arterial phase ( gart ) by the peak enhancement of the aorta ( iaorta ) , while portal perfusion ( pport ) is derived from gradient after subtraction of the arterial component from the liver curve ( g * port ) , normalized by the enhancement of the aorta ( iaorta )  . 
on the basis of previous studies assessing hpi values in healthy subjects and in patients with clinically detected hepatic metastases in patients with crc , values above 0.3 were considered as abnormal [ 8 , 14 ]  . 952 while hpi is calculated considering the entire hepatic parenchyma , tumour metastases auc was evaluated on a single metastatic nodule , followed throughout the entire study as a target lesion , drawing manually a roi of 20 pixel in the hyperintense zone of the metastasis to exclude necrotic and not vascularized areas . 
the auc was calculated as the area under the time - intensity curve of the selected roi over the entire procedure , normalized by the time of imaging acquisition expressed in seconds . 
this cut - off threshold was chosen as it represents the median of baseline normal auc values of our patients . results radiol med ( 2016 ) 121 : 950957 group were calculated and plotted using the kaplanmeier method and compared using the log - rank test . similarly to hpi , patients were grouped according to tumor response and auc values and their variations along time were compared using the mannwhitney u test . 
progression free survival and overall survival for patients stratified according the cut - off value of 1000 were calculated and plotted using the kaplanmeier method and compared using the log - rank test . 
finally , patients were grouped according whether their tumor progressed at 3 months , responded or remained stable at 3 months and then progressed at 6 months , or responded or remained stable at 6 months . 
patients not progressing or alive at the time of data analyses were censored at the time of the last follow - up examination . statistical analyses to explore the relationship between hpi and response to chemotherapy , patients were divided into two groups : responders vs non - responders ( including progressive or stable disease )  . 
similar results were obtained when patients were divided using an arbitrary cut - off of 30 % in auc variation at 3 months compared to baseline . as an exploratory unplanned analysis , patients were further divided into three groups : patients progressing at 3 months ( g1 ; 7 patients ) , patients not progressing at 3 months and progressing at 6 months ( g2 ; 7 patients ) , and patients who were progression - free at 6 months ( g3 ; 29 patients )  . 
as far as normal liver auc was concerned , in g1 median values increased at 3 months compared to baseline 1 3 radiol med ( 2016 ) 121 : 950957 fig . 
while this procedure did not affect hpi algorithm , the graph of signal intensity over time from which auc is calculated was dependent from the total time of image acquisition , different for any single scan . 
it is worth to remember that the plasmatic half - life of the contrast agent is sufficiently long ( 1.8 h ) [ 15 ] to prevent significant decrease of signal intensity in the time range of our acquisitions . another possible bias that may lead to discordant results could be the difference in magnetic induction power of the scanners . 
thus , we can conclude that the dce - mri assessment in our limited series of patients did not support the hypothesis of a difference in orr according to hpi at baseline , primary endpoint of the study . 
moreover , the data of our study in metastatic colorectal cancer patients did not support the hypothesis of any correlation between the hpi changes during first line systemic chemotherapy , or aucs of metastases or normal liver , and chemotherapy activity in terms of tumor response , ttp and os . 
moreover , hpi and auc data suggest a possible control of the entire liver vasculature by substances directly produced and released into the bloodstream by tumor cells such as inflammatory cytokines . hpi data of our study agree with others already published [ 16 ] , with median baseline hpi value of 0.249 , radiol med ( 2016 ) 121 : 950957 suggesting a reproducibility of this variable . 
both tumor and normal liver area aucs increased in progressing patients , a slightly different trend was shown in those patients not progressing at 3 months and progressing at 6 months . 
we believe this preliminary observation should be tested in a larger number of patients to verify whether variations of tumor auc could be an early predictor of tumor progression , as this might be useful in the early switch to other active chemotherapeutic regimens . despite these negative results , some interesting findings are worth of discussion . 
first , it should be pointed out that in our study hpi reduction was observed following chemotherapy administration alone without the addition of an anti - neoangiogenetic agent as published elsewhere [ 17 ]  . 
 this finding raises several doubts about the interpretation of those studies in which reduction of perfusion parameters after administration of chemotherapy combined with antiangiogenetics have been indicated as an efficacy index of this latter class of agents . second , we have shown a direct correlation between tumor and normal liver aucs and their variations at each time point . 
this could be easily explained by external 1 3 radiol med ( 2016 ) 121 : 950957 factors such as the total amount of contrast agent administered at each time . 
this was unexpected as metastases have a higher arterial blood flow than normal liver due to the tumor neoangiogenesis and thus only lesioned aucs were supposed to be influenced by tumor response . 
furthermore , the correlation coefficient of 0.6 between changes in tumor vs normal aucs accounts for the observation of a decrease in hpi in responding patients , as in these patients arterial blood reduced more than portal blood flow . conclusion hpi could be easily assessed by routine dce - mri . 
while its putative prognostic role should be analyzed in a larger number of patients , its baseline values did not support the idea of a correlation between response to first line chemotherapy and patient outcomes . 
auc assessed by an image acquisition protocol which permits morphological evaluation of the liver metastases did not demonstrate to be useful in predicting response rate and survival and it should be eventually reserved to the experimental setting . compliance with ethical standards conflict of interest the authors have no conflict of interest to declare . ethical statement all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . radiol med ( 2016 ) 121 : 958965 doi 10.1007 / s11547 - 016 - 0674 - x radiotherapy imageguided radiation therapy ( igrt ) : practical recommendations of italian association of radiation oncology ( airo ) paola franzone1 alba fiorentino2 salvina barra3 domenico cante4 laura masini5 elena cazzulo6 liana todisco1 pietro gabriele7 elisabetta garibaldi7 anna merlotti8 maria grazia ruo redda9 filippo alongi2 renzo corv3 received : 25 july 2016 / accepted : 16 august 2016 / published online : 6 september 2016 italian society of medical radiology 2016 abstract the use of imaging to maximize precision and accuracy throughout the entire process of radiation therapy ( rt ) delivery has been called image - guided rt ( igrt )  . 
antonio e biagio e cesare arrigo hospital , alessandria ( to ) , italy 7 radiation oncology department , ircc , candiolo , italy 8 radiation oncology department , s.croce e carle hospital , 9 radiation oncology department , ospedale mauriziano , cuneo , italy turin , italy keywords radiotherapy image - guided radiation therapy computed tomography magnetic resonance imaging introduction the use of imaging to maximize precision and accuracy throughout the entire process of radiation therapy ( rt ) delivery has been called image - guided rt ( igrt )  . by comparing these images to those obtained during simulation , the patients position and / or the geometry of the radiation beams may be adjusted to more precisely address the radiation dose to the target . rt has long been image guided : in fact , historically , the portal films or , later on , electronic megavoltage images ( obtained with electronic portal imaging devices , epid ) represented an early form of igrt . 
due to these uncertainties , it is inevitable to include a larger volume of normal tissue in the planning target volume ( ptv ) to ensure target coverage . the advances in rt planning and delivery , producing much more conformal dose distributions with sharper dose gradients , need a greater accuracy and precision in treatment reproducibility . 
modern igrt techniques , improving soft tissue localization , coupled with frequent imaging / repositioning cycles ( ideally , before each treatment session ) , reduce uncertainties , therefore , allowing margins 1 3 radiol med ( 2016 ) 121 : 958965 reduction and possibly less toxic treatments . 
thus , igrt is particularly useful when high tumoricidal doses are prescribed with highly conformal treatment modalities , including 3 - d conformal - rt ( 3d - crt ) , intensity - modulated rt ( imrt ) , stereotactic body rt ( sbrt ) or stereotactic ablative rt ( sabr ) , proton therapy [ 13 ]  . a broad range of igrt modalities is now available and adopted [ 4 ]  . 
the target location may be determined by several methods for localization of surrogates , including implanted fiducial markers , external surface markers or of anatomical features [ by planar imaging , fluoroscopy , kv or mv computed tomography ( ct ) , magnetic resonance imaging ( mri ) , ultrasound ( us ) and x - ray imaging , electromagnetic localization or optical surface imaging ]  . 
this practice parameter addresses qualifications and responsibilities of personnel , clinical igrt implementation , documentation , quality control and improvement , safety and patient education . the aim of the present review is to define practical recommendations for igrt . igrt system the components of any igrt system are the follows : an image acquisition system . a set of reference images for comparison . a software for the comparison match between reference images and ct planning . a protocol that defines the correction method . two kinds of procedures are used for the correction strategies : online and off - line method [ 5 , 6 ]  . the online correction strategies include the analysis of images information immediately after the acquisition and , if necessary , the application of the correction before each rt session [ 57 ]  . 
the disadvantage is that the process of analysis and correction needs to be fast , simple , and unambiguous . with the off - line correction instead , the images data were stored , and analyzed and corrected at a later time [ 7 , 8 ]  . 
usually , with this strategy , verification of sequential images in a sufficient number of initial fractions ( usually 35 fractions ) is performed : thus , the off - line protocols correct the average systematic error but not the daily error [ 5 ]  . 
statistical analysis of these data allows to calculate the mean value ( m ) and the relative standard deviation ( sd ) of the systematic component of the setup error . 
it has been estimated ( with biological and physical models ) that the number of daily images needed to obtain a reliable systematic error evaluation is equal to about 10 % of the total number of sessions [ 9 , 10 ]  . in general , online strategies allow a greater reduction of the geometrical uncertainties with respect to off - line methods , but with an increased workload , treatment time and radiation dose . an online approach is to be preferred especially when the high dose volume is close to anatomical structures critical for organ function , in the dose - escalation programs or for hypofractionated treatments . 
the radiation oncologist ( ro ) in charge of the patient should , therefore , define the preferred procedure for each individual case . independent of the correction procedure method , a tolerance margin ( tm , acceptable error range of the setup ) should be determined for each disease and location of target , considering also the priority of ptv coverage , organ at risk ( oar ) functional relevance , the extent of organ motion and the patient individual features . the next step is the definition of action levels . 
two possible procedures are possible in off - line correction protocols : no action level ( nal ) and shrinking action level ( sal )  . the nal is the procedure more frequently used : the systematic error , calculated as the average of the errors identified in the first n fractions , is corrected systematically in all the subsequent sessions , without tolerance limits . 
if the measured error is less than the tm , no further corrections are suggested ; if tm is exceeded , the acquisition of more images to identify any residual systematic error is warranted . in the sal protocol , the correction is performed if the measured error exceeds the tm . direct comparisons between the sal and nals show that nal protocol may be more cost effective in terms of number of images needed for the systematic error reduction [ 11 ] , but both procedures may be used , depending on ros clinical evaluation in the individual case . igrt modality we refer the interested reader to a recently published comprehensive description of igrt modalities , with the pertinent geometric uncertainties and basic technical features [ 12 ]  . 
however , a short description of the main igrt techniques follows . 1 3 960 radiol med ( 2016 ) 121 : 958965 electronic portal image systems orthogonal portal images are produced by the source of the linac . 
the bone structures are evaluated . tomographic cone image systems with high ( megavolt , mv ) and low ( kilovolt , kv ) energy cone beam computed tomography ( cbct ) is the most widespread three - dimensional igrt syste it utilizes an x - ray tube source . 
the x - ray source and a flat panel detector are mounted on the gantry of the linear accelerator ; it is not only possible to acquire planar images , but also multiple projections during a 360 rotation in about a minute resulting in a cone - beam ct scan used for a volume reconstruction in transversal , coronal and sagittal slices providing 3d bone and soft tissue image information . 
a compact ( ~40 cm long ) 6 mev s - band ( 3 ghz ) linear accelerator generating a 6 mv photon beam is mounted on the rotating gantry and attached to the slip ring . 
using a separate collimation ( jaws ) system above the multileaf collimators , the slice thickness can be varied between 0.5 and 5 c the on - board megavoltage ct detection system is from a conventional , commercial diagnostic scanner using xenon detectors . 
the ct detection system can be used for patient setup verification and repositioning , if necessary , verification of leaf positions during treatment , and reconstruction of the actual dose delivered to the patient with the possibility of making corrections in subsequent fractions . quality of image definition ; a possible disadvantage could be represented by the minimum setup errors in the passage of the treatment couch from the imaging to the treatment position . ultrasound images the ultrasound probes are able to provide volumetric images using special software that allows the comparison between the current position and that of planning . 
this system is used mainly for igrt in prostate cancer and breast cancer . igrt and dosimetric issues clinical - dosimetric evaluation of the additional dose delivered to the patient with the use of igrt is a somewhat overemphasized issue . 
the main advantage of this system is the excellent we refer the interested reader to the comprehensive description of igrt of the british national radiotherapy igrt and anatomical district 1 3 radiol med ( 2016 ) 121 : 958965 implementation group ( nrig ) that developed a strategy for the use of igrt [ 17 ]  . 
thus , only a short description of site - specific recommendations for igrt use follows ; however , several general principles may be applied to all sites , including : a . 
continuous update of igrt internal procedures , according to the literature , since igrt is still an evolving area . excluding rare tumors , the most common anatomical districts to which igrt procedures are applied are listed below . breast epid - based igrt is commonly used to assess reproducibility for breast rt . 
when appropriate immobilization is used , systematic and random errors are approximately of 34 mhowever , an acceptable tm for setup error is 5 mif this value is exceeded , patients setup re - imaging could be suggested and if the tm is still exceeded re - simulation / replanning should be advised . in case of partial breast irradiation , sequential tumour bed boost or simultaneous integrated boost , 2d paired images or 3d imaging could be required , especially when tumour bed ptv margin is less than 5 mm . when reduction of ptv margins is required , 2d imaging ( with a non - opposed pair of images ) and 3d volumetric imaging , resolving the displacements in all directions accurately , could be useful in selected cases [ 17 ]  . brain brain structures are not affected by large position variations , and image guidance is , therefore , based on imaging of bone structures . 
igrt is , therefore , strongly suggested for these patients , at least to define systematic errors [ 19 , 20 ]  . in head and neck cancer , there are several factors that affect the patients setup , including the accuracy of immobilization systems , the anatomical changes , and the reduction in tumor volume . 
for example , it is well recognized that during treatment the parotid glands volume decreases with the subsequent risk of receiving more than the planned dose [ 21 ]  . 
thus , cbct , with direct visualization of anatomical changes during the entire course of treatment , could be very helpful also for assessing the timing of replanning [ 2228 ]  . although the published literature relating to the suitable ctv - ptv expansion is limited , it is shown that , to ensure adequate coverage of the target without daily igrt , ctvptv margins in the three directions should be of about 45 mm [ 29 ]  . 
thus , when margins are reduced to less than 5 mm , daily cbct is strongly suggested [ 30 ]  . prostate cancer several igrt systems are available for prostate localization : planar , volumetric images ( kv or mv ) , electromagnetic or ultrasound systems . the prostate gland can move inside the pelvis up to 2 cm , and its position is strongly influenced by the rectal and bladder filling , as well as by respiratory motion or by intestinal peristalsis . 
such organ motion could produce an insufficient coverage of prostate volume and / or an increasing exposure of the surrounding healthy tissues , especially for imrt treatment [ 31 ]  . ctv - ptv margins of 10 mm in all spatial directions except posteriorly ( 5 mm ) are usually applied to cover the prostate volume [ 32 , 33 ]  . 
 thus , daily execution of cbct could be suggested [ 36 ] ; other igrt procedures may , however , be acceptable , also depending on the fractionation schedule adopted ( hypofractionated regimens may require more sophisticated igrt procedures )  . 1 3 962 rectal / anal cancer considering the large treatment volumes needed for these diseases , some studies reported a reduction in toxicity using imrt / vmat with igrt [ 37 , 38 ]  . 
thus , the choice of the best igrt approach depended on the technique utilized [ 39 , 40 ]  . gynecological cancer in the treatment of uterine carcinoma , 3d - crt and imrt / vmat / ht guarantee an high conformity of the dose to the target and a simultaneous reduction of the undesired exposure to surrounding oars : small intestine , bladder , rectum , bone marrow ( and also kidneys and the spinal cord for extended para - aortic fields ) [ 41 , 42 ]  . the displacement of the position of the organ can be caused both by the physiologic mobility of the uterus according to the different filling of the rectum and bladder in subsequent fractions ( interfraction motion ) , and also by the tumor regression as a response to radiotherapy [ 43 ]  . several authors have shown that during rt , interand intra - fraction motion of intact uterus and cervix were in the range of 318 mm in every direction [ 4446 ]  . thus , 3d - crt may carry a risk of gastrointestinal side effects due to the generous safety margins that must be applied to compensate for organ motion [ 4751 ]  . 
this problem could be reduced by the application of igrt procedures ; in addition , the inhomogeneity of dose distribution with imrt techniques suggests to verify the reproducibility of the daily setup with volumetric igrt to avoid geographic miss , resulting in worse clinical results compared to those obtained with conventional techniques [ 50 ]  . lung cancer lung cancer is one of the most difficult neoplasms to be treated due to significant intrafraction tumor motion . 
most lung cancers are subjected to respiratory excursions up to 34 cm , especially if they were near to the diaphragm and cbct reduced both the systematic and random errors [ 52 , 53 ]  . if the role of 3d verification systems is undisputed , it is not so clear how often these checks should be performed . 
 [ 54 ] retrospectively simulated several schedules of igrt verification : no igrt , weekly cbct , cbct in the first five fractions and subsequently every week , and cbct every other day . 
the systematic error reduction , however , allows a significant reduction in margins with the increasing frequency of igrt procedures . radiol med ( 2016 ) 121 : 958965 higgins et al . 
 [ 55 ] conducted a similar study in which igrt reduces the magnitude and frequency of the setup error : an error 5 mm in cc direction was evidenced in 21 % of cases in the absence of igrt versus 2 % with cbct . 
thus , the execution of cbct could be suggested . paraspinal lesions in relation to the proximity to the spinal cord , rt with curative doses of paraspinal lesions , for primary cancer or oligometastatic patients , often requires the use of imrt / vmat / ht supported by igrt techniques [ 5658 ]  . 
the childhood cancer survivor study reported the results of 14 , 359 patients cured of a childhood cancer : 1402 of them developed a second neoplasm , with a cumulative incidence at 30 years of 20.5 % in a multivariate analysis , rt associated with age ( < or > 15 years ) , the initial diagnosis , female sex and exposure to chemotherapy ( platinum ) , appeared to be the major risk factors [ 64 ]  . thus , in these patients , it is theoretically important to assess carefully also the doses received with igrt . 
in a recent review , the authors propose a reduction in the use of methods based on ionizing beams , and if it is not possible to realize a treatment without the use of volumetric igrt , they recommend an assessment of some parameters : age , gender , anatomical site of the target , decreasing amperage , use of filters , use of protocols with lower exposure doses , using custom protocols for the frequency of igrt and careful documentation of the dose received at the target and to all healthy tissues [ 65 ]  . 1 3 radiol med ( 2016 ) 121 : 958965 conclusions in summary , in the modern rt era , igrt seems to be crucial in terms of increasing precision of therapeutic radiation delivery , to increase target coverage and maximize oars sparing [ 66 ]  . 
specific protocols for the individual treatment sites and based on the available technology are needed to optimize igrt use and rt departments logistical problems . acknowledgments the authors would like to thank elvio g . 
russi , airo president , stefano maria magrini , airo president - elect , claudio arboscello , marco gatti , alessia guarneri , pietro gabriele , elisabetta garibaldi , anna merlotti , andrea ballar , renato chiarlone , giuseppina gambaro , filippo grillo ruggieri , marco krengli , maria rosa la porta , gregorio moro , fernando munoz , umberto ricardi , paolo rovea , tindaro scolaro , maria tessa , and alessandro urgesi . compliance with ethical standards ethical approval the manuscript does not contain clinical studies or patient data . 
the aim of this work was to review advanced imaging modalities employed to study thoracic spine and spinal cord in injured patients . keywords spinal trauma imaging techniques magnetic resonance imaging computed tomography fracture introduction injuries of the thoracic spine are less common than those involving the cervical or lumbar spine or the thoracolumbar junction . 
fractures of the thoracic spine account for 20 % of all spinal fractures and occur most frequently at the thoracolumbar junction ( t10l2 ) ; about 16 % of thoracolumbar injuries involve the tract t1 - t10 [ 1 ]  . fractures of the thoracic spine are most frequent among males and are typically caused by high - energy trauma , such as motor vehicle accidents in middle age individuals , while children and adolescents are at higher risk for injuries during sports and recreational activities . 
associated injuries increase morbidity in patients with thoracic spine fractures : pulmonary disease and shock are major responsible for short - term mortality , while paralysis , sepsis , and the need for spinal stabilization are the frequent causes of long - term morbidity . 
he consequently divided the original anterior column into two by introducing a middle column , stating that the third column is represented by the structures that have to be torn in addition to the posterior ligament complex to create acute instability [ 11 ]  . according to this classification , the anterior column includes the anterior spinal ligament , the anterior annulus fibrosus , the intervertebral disc , and the anterior two - thirds of the vertebral bodies . 
the posterior column includes the whole spine posterior to the longitudinal ligament , i.e. , posterior arch and posterior ligamentous complex ( ligamentum flavum , interspinous ligament , and supraspinous ligament ) [ 1214 ]  . 
 [ 16 ] more recently , magerl and coworkers tried to solve this situation by proposing a comprehensive classification primarily based upon the morphopathological aspects of the injuries [ 17 ] ( table 1 )  . 
 however , none can be considered all - encompassing . anatomy and biomechanics of the spine in the majority of individuals , there are 12 thoracic vertebral bodies , with increasing size proceeding caudally [ 18 ]  . 
 the thoracic vertebral segment is composed of a vertebral body , the right and left transverse processes , a posterior spinous process , and right and left superior and inferior facet surfaces connected to the vertebral body by a pedicle . 
the lateral costotransverse ligament , the articular capsule , the superior costotransverse ligament , and the intra - articular ligament provide flexible stability between the transverse process and the rib facets . 
due to this stability supplied by the rib cage , the orientation of the facet joints , and the interaction of the vertebrae with ligaments , discs , and muscles , the thoracic spine is more rigid than the cervical or lumbar spine [ 69 ]  . the forces acting on the spine can be represented as vectors that produce rotation and / or linear displacement and can occur isolated or in combination . 
most thoracic spine injuries occur during flexion and axial loading ; due to these mechanisms of injury , fracture dislocations are more common than compression and burst fractures . imaging : conventional radiology the radiologic evaluation must include anteroposterior ( ap ) and lateral radiographs of the entire spine . 
the ap radiogram is useful to assess vertebral alignment and vertebral body cortical disruption , the lateral radiograph to evaluate the posterior vertebral body ( normally mildly convex anteriorly ) , and to exclude a displaced fragment into the canal [ 17 ]  . in severely injured patients , it is important to maintain spinal casts , until injury is excluded by physical examination and / or imaging studies , to avoid severe injuries to the spinal cord . 
1 lateral view on plain film showing fracture of a thoracic vertebral body : note the disruption of the anterior vertebral cortex and the anterior wedging indirect signs of thoracic spine injury are sternal and rib fractures , with or without associated costovertebral dislocation [ 22 ]  . some of the radiological signs of soft tissue injuries associated with thoracolumbar spine fractures are loss of the psoas line , paraspinal soft tissue widening , hemothorax , and pneumothorax . the degree of confidence in the initial identification of thoracic spine fractures on the conventional radiograms is influenced by some technical factors , such as the size of the patient , patient movement , and the type of radiologic equipment available . it is also important to remember spinal anomalies that may be mistaken for a fracture : horizontal residual venous sinus grooves , epiphyseal margin on the anterior corners of the vertebral body and ossification centers at the ends of the transverse processes in young children , occult spina bifida , or congenital butterfly vertebral body ( it appears as a compression fracture in the lateral projection )  . 
other pitfalls include the superimposed shadows of the glenoid process of the scapula that may simulate a compression fracture in the lateral projection views , or the outline of the mandible that may suggest a fracture in an anterior view . imaging : computed tomography ( ct ) ct is a valuable diagnostic tool which has replaced the conventional radiography in many trauma centers for the assessment of thoracic spine fractures , especially in patients with high - energy trauma . 
ct is also used as a second line imaging examination when the conventional radiographic findings are inconclusive , in disagreement with the clinical status [ 23 ] , or when a fracture detected on plain radiographs needs to be further characterized . 
ct is faster 1 3 radiol med ( 2016 ) 121 : 780792 and less expensive than mri , and provides the main information needed for the initial evaluation of patients with spinal injury . 
false - negative ct results may occur in the cases of chronic stress injuries and in severe osteoporotic end - plate fractures [ 25 ]  . assessment of the spinal cord is difficult on ct imaging due to beam hardening artifact from bone and relatively poor soft tissue contrast in the spinal column [ 24 ]  . to determine stability , ct provides also a detailed assessment of associated soft tissue and visceral injuries and a more accurate assessment of specific column involvement . imaging : magnetic resonance imaging ( mri ) the main advantages offered by mri are multiplanar imaging , high spatial and contrast resolution ( especially for soft tissues ) , and the absence of ionizing radiations ; for all these reasons , mri is superior to other imaging modalities , especially for the detection of ligamentous injuries , posttraumatic disc herniation , epidural hemorrhages , and spinal cord injuries [ 20 ]  . 
it is particularly useful in patients with neurological deficits . in comparison to ct , mri provides superior definition of extra - axial causes of spinal cord injury , such as disc herniation and epidural hematoma . mr imaging is also clearly superior to plain radiographs and ct in detection of ligamentous injury , and thus in assessing spinal instability . mri is not the gold standard imaging modality to evaluate bone lesions , but some mr imaging pulse sequences , such as short tau inversion recovery ( stir ) technique , are particularly sensitive to detect marrow edema , which is a clue of acute fracture and can sometimes help to detect subtle fractures not readily evident . 
fat suppressed sequences are particularly sensitive to detection of marrow edema , which is a clue of acute fracture and can sometimes help to detect subtle fractures not readily evident . 
the detection of bone marrow edema can help to distinguish acute from chronic fractures 1 3 784 radiol med ( 2016 ) 121 : 780792 can also detect some indirect signs of fracture , such as paraspinal edema or hemorrhage , epidural bleeding , and sprains of paraspinal and intraspinal ligaments [ 22 ]  . longitudinal ligament ( pll ) , ligamentum flavum ( lf ) , interspinous ligaments ( isp ) , and supraspinous ligament ; they appear hypointense on all mr pulse sequences [ 32 ]  . ligament injuries , best depicted on t2 - weighted and thin - section t1 - weighted images , include rupture , stripping of the intact ligament , partial avulsion or attenuation of the ligament and osseous , and ligamentous injury . 
stir images , useful for detecting interspinous hemorrhage in patients with posterior ligamentous disruption , show hyperintensity in and around a ruptured ligament , with a focal discontinuity indicating complete rupture . 
the pll is not significant in the the main disadvantages of mr imaging in the trauma setting are related to the long duration of mr scans , the limited ability to monitor the patients during the mr examination , due to the closed configuration of the mr scanner , and the need to have mr - compatible cardiovascular monitoring devices and ventilatory support machines . 
moreover , unresponsive trauma patients need to be accurately checked for the presence of metallic foreign bodies . the main indications to mr imaging of acute spinal trauma include loss of neurologic function , suspected spinal cord injury , extra - axial hematoma , and disc herniation that cannot be detected by ct [ 24 ]  . false - positive and false - negative findings can often result from movement artifacts near the site of injury ; metal artifacts may also mask spinal fractures . 
in these cases , the administration of intravenous contrast medium can help in the diagnosis . mr studies of patients with spinal trauma should include sagittal t1 - weighted spin - echo ( se ) and t2 - weighted fast spin - echo ( fse ) sequences covering the site of primary trauma , and axial t1 - weighted se sequences covering at least the vertebral body above and the vertebral body below the injured level . 
other useful sequences include gradient echo t2 * weighted images to evaluate the presence of cord hemorrhage [ 2630 ]  . in spinal mr imaging , a dedicated phase - array is used to achieve high signal - to - noise ratio ( snr ) which provides better spatial resolution . osseous injuries mr is unique in its ability to detect compressive injury of the marrow components without a fracture deformity or cortical disruption . 
the vertebral bodies appear hypointense on t1 - weighted and hyperintense on t2 - weighted images , especially with fat - saturated t2 - weighted images , such as stir [ 31 ]  . 
 assessment of spinal ligaments helps to determine whether a fracture is stable or unstable 1 3 radiol med ( 2016 ) 121 : 780792 determination of spinal stability , while disruption of the all indicates some rotational component to the injury ; prevertebral swelling and hyperintensity are important secondary signs of all rupture and are particularly common in hyperextension injuries . rupture of the supraspinous ligament leads to instability of thoracolumbar burst fractures [ 34 ]  . mri is also valuable to detect subtle damage to the joint capsule ; widening of the facet joint with hyperintensity on t2 - weighted images due to increased fluid within the joint space is a sign of a distraction injury . 
this finding of hyperintensity may also be seen with degenerative facet disease and should be interpreted as pathologic in all cases [ 35 ]  . epidural hematoma and disc and nerve root injury spinal epidural hematomas occur with tear of the epidural venous plexus and extravasation of blood into the anterior epidural space . 
the hypointense dura helps to differentiate the epidural compartment from the subarachnoid space . disc injuries related to acute spinal trauma include intradiscal hemorrhage / edema , annular rupture , avulsion from the end plate , and herniation into the epidural space or into the vertebral body [ 22 ]  . hemorrhage / edema of the disc appears as hyperintense on t2 - weighted sequences in the acute stage . 
rupture of the annulus is generally associated with flexion - distraction and hyperextension injuries . acute post - traumatic disc herniation has a similar mr appearance to a non - traumatic disc herniation , but is usually accompanied by hemorrhage . 
traumatic disc herniations occur less frequently in the thoracic spine than in the cervical spine , and are most commonly seen with hyperextension injuries and fracture dislocations ; in such cases , they are frequently associated to significant neurologic damage . 
the height of the injured disc may be either reduced or increased . mr is not reliable in demonstrating traumatic nerve root avulsions , though post - traumatic root pouch cysts , frequently associated with nerve root avulsion , can be identified with high sensitivity . spinal cord injuries complete spinal cord injury associated with thoracic fractures occur more frequently than in cervical or lumbar spine fractures , due to the narrow thoracic spinal canal . most of these injuries occur by hyperflexion mechanisms . 
the patterns of acute cord injury shown on mr images are edema , hemorrhage , and mixed central hemorrhage and edema . hemorrhage in the spinal cord has significant clinical implications , as it is a predictor of poor potential for neurologic recovery . 
 in the acute stage , the epidural hematoma is isointense with spinal cord parenchyma on t1 - weighted images and isointense with csf on t2 - weighted images 1 3 786 radiol med ( 2016 ) 121 : 780792 the brain ; however , the conversion from deoxyhemoglobin to intracellular methemoglobin may be delayed for up to 8 days in the spinal cord , due to local hypoxia in comparison with the brain . acute hemorrhage is seen as a central cord hypointensity on t1and t2 - weighted spin - echo and gradientecho sequences , surrounded by edema ( hyperintense on t2 - weighted images and hypointense on t1 - weighted images )  . 
mr may be helpful in predicting the recovery of neurologic function after acute spinal cord injury ; cord abnormalities associated with progressive neurologic deficits are intramedullary cysts and post - traumatic myelomalacia . 
occasionally , mr also demonstrates evidence of wallerian degeneration in the dorsal columns above the level of injury [ 17 ]  . fractures fractures of the spine can be divided into two groups . 
 minor injuries , which account for more than 15 % of the fractures , include isolated fractures of transverse processes , spinous processes , articular processes , facet articulations , and the pars interarticularis . 
the major injuries have been classified by denis into hyperflexion compression fractures , burst fractures , flexiondistraction ( chance - type fractures ) , and fracture dislocation [ 3642 ]  . hyperflexion compression fractures compression fractures ( wedge fractures ) represent the majority of thoracic spine fractures . 
if the middle column is not involved , these fractures are considered stable [ 43 ]  . patterns of fracture can include disruption of the superior end plate ( in simple hyperflexion compression ) , inferior end plates , or both . 
when a lateral bending is associated with axial forces , a lateral wedge - compression fracture can result [ 19 ]  . these kinds of fractures are rarely associated with spinal cord injury and are considered stable unless multiple contiguous vertebral bodies are involved . later plain film views clearly demonstrate the loss of height of the anterior aspect of the body ( usually less than 50 % ) with wedge deformity . 
in higher energy traumas , loss of more than 50 % of the anterior body height may occur with possible subluxation or dislocation of the facet joints secondary to posterior ligamentous failure . 
ct is sometimes useful to assess the extent of the fracture and the involvement of the middle column [ 44 ] , but usually these fractures may be difficult to demonstrate on axial ct scans as the fracture lines nearly parallel to the imaging plane , and multiplanar reconstructions need to be obtained . 
6 sagittal t1 ( a ) and t2 weighted ( b ) images showing acute cord edema ( hyperintense on t2 - weighted images and hypointense on t1 - weighted images )  . 
7 sagittal t1 mri scan ( on the left ) , sagittal and axial view on ct ( on the right ) showing compression fracture with more than 50 % of vertebral body involvement . 
this kind of fracture ( type ib ) tend to involve the middle and posterior columns , they are usually unstable and may require stabilization two different subtypes of compression fractures have been described : ia and ib [ 45 ]  . 
however , about 88 % of patients with compression fractures are neurologically intact . burst fractures burst fractures account for about 14 % of spinal fractures ; they are caused by direct axial vector forces without bending . 
if the axial compression is combined with translational forces , it may result in burst dislocation fractures , in which there is also destruction of the inferior vertebral body posterior elements and subsequent anterolistesis of the superior vertebral body . 
the posterior elements are involved bilaterally in 50 % of cases and unilaterally in 40 % [ 46 ]  . due to the potential for neurologic deficit , burst fractures should be considered unstable during the initial evaluation . in up to 25 % of cases , burst fractures are misdiagnosed on the conventional radiographs , because of the failure to recognize involvement of the posterior aspect of the body and the displacement of fragments into the spinal canal . the conventional radiographic findings include anterior wedging and posterior body height loss . 
ct scan can detect posterior column fractures missed on the plain radiographs and clearly demonstrates the degree of spinal canal compromised by the retropulsed fracture fragments , especially on sagittal reconstructed images . 
mr is useful in assessing the status of the thecal sac and spinal cord , and the integrity of the spinal ligaments . 1 3 788 radiol med ( 2016 ) 121 : 780792 flexiondistraction injuries ( seatbelt fractures or chance fractures ) an intact spinous process help to differentiate this fracture from the classic chance fracture [ 42 ]  . these fractures , first described by chance and also called seat - belt fractures , because are commonly associated with use of a lap seat belt in high - speed motor vehicle crashes [ 3638 ] , are caused by shearing and distractive forces when flexion is coupled with a fulcrum located anterior to the vertebral column ; there is disruption of the middle column , making these fractures unstable . these injuries occur less frequently in the upper thoracic spine , due to the rigidity provided by the rib cage . 
typically , they are located in the lower thoracic region near or at the thoracolumbar junction . these injuries can involve purely osseous structures , purely ligamentous structures , or both . 
this usually involves one level , between l1 and l3 [ 42 ]  . the second type of horizontal injury is also known as the smith fracture , where injury initially disrupts the supraspinous and interspinous ligaments with the fracture occurring at the junction of the lamina and spinous process without involving the spinous process itself and extends to involve the posterior body . 
 on imaging , the widening of the interspinous distance and the third type of fracture involves the posterior elements on one side only secondary to a rotational force . chance fractures are infrequently associated with neurologic deficits , but if present , they should be further evaluated with mr imaging to exclude neural compression . 
both mr and ct with sagittal reconstructions are valuable for delineating the path of injury ( through bone and / or soft tissues ) [ 47 ]  . on the conventional radiographs , the horizontal fractures are best seen on the lateral view . 
 thin axial cuts and sagittal and coronal reconstructions are essential to detect the fracture and any malalignment due to ligamentous injury [ 48 ]  . mr will demonstrate subtle marrow edema and is also very useful to exclude an associated ligamentous injury [ 49 ]  . fracture dislocation injuries fracture dislocations are the result of violent complex forces ( compression , tension , rotation , or shear ) with failure of all three columns and subsequent extreme instability . 
9 sagittal ( on the left ) and axial ( on the right ) ct images showing type i chance fracture of a thoracic vertebral body with involvement of the through the posterior arch and pedicles . 
 the fracture runs orizontally extending anteriorly to involve the posterosuperior aspect of the body just anterior to the neural foramen 1 3 radiol med ( 2016 ) 121 : 780792 and rotation forces leading to a tear of the posterior longitudinal ligament . 
the rate of neurologic injury is highest ( 75 % ) with this latter injury subtype [ 11 ]  . these fractures are potentially unstable as the ligamentum flavum , interspinous ligament , and supraspinous ligament are usually torn . 
the injury may either go through the disc ( it is then accompanied by wedging of the vertebral body below ) , or it may go right through the body itself leading to a slice type of fracture . 
these fractures are differentiated from burst fractures in that the interpediculate distance remains constant , as the ring of the neural arch is not disrupted in this type of injury . 
the posterior arch of the dislocated vertebra is fractured at several levels , there are free floating lamina , fractures of multiple spinous processes in the upper segment , and fracture of the superior facet of the lower vertebra . 
the flexiondistraction type injuries resemble the seat - belt type of injury ; with both the posterior and middle column rupture under tension and the annulus fibrosus torn , the vertebra above can sublux or dislocate on the vertebra below . 
10 sagittal t2 and t2 with fat suppression ( on the top ) and axial t2 ( on the bottom ) showing fracture and displacement of the fourth thoracic vertebral body fracture - dislocations are the result of violent complex forces with failure of all three columns and subsequent extreme instability . 
note that one vertebral body is usually displaced with respect to another , compromising the spinal canal with resulting severe spinal cord injury vertebral bodies , spinal canal , and facet involvement , and for detecting dislocated articular processes . 
axial ct images demonstrate the double rim sign due to vertebral body overlap [ 50 ]  . sagittal ct reconstructions and sagittal mr images provide information about the nature and extent of canal compromise . 
the midsagittal ct reconstruction can also help to determine prognosis . true bilateral fracture dislocations of the lumbar spine are rare and are usually related to major pelvic trauma , fall from a height , or ejection from a motor vehicle . 
many are associated with sacral fractures [ 48 ]  . miscellaneous fractures hyperextension injuries are extremely rare in the thoracolumbar spine and usually occur in the mid - lumbar region . 
 the resultant deformity is posterior compression and anterior distraction [ 51 ]  . 1 3 790 radiol med ( 2016 ) 121 : 780792 radiographic findings include widening of the anterior disc space , retrolisthesis , fractures of the pars interarticularis , and triangular avulsion fractures from the anterosuperior vertebral body . 
anatomical features of the thoracic spine , magnitude and direction of the impact , and the patients postural alignment are all the conditions concurring to the severity of a spinal injury . the early and correct diagnosis is of paramount importance to prevent severe spinal marrow damage . the clinical management of patients with spinal injury depends on the accuracy of imaging studies . 
in the acute stage , a complete assessment of the injuries to the bony , ligamentous , disc , and neural structures can help to determine the stability of the injury and decide to have a conservative or a surgical approach . 
conventional radiography , computed tomography , and magnetic resonance imaging are all useful diagnostic instruments to evaluate spinal trauma , and are often employed in combination . among the imaging techniques , magnetic resonance imaging ( mri ) emerged as the most sensitive one to detect most types of spinal injuries [ 52 ]  . the conventional x - rays are generally used as initial diagnostic modality , since they help to detect the presence of vertebral fractures and / or subluxations , thereby identifying specific levels of abnormality . computed tomography ( ct ) provides additional information on the bony structures of the spinal column . 
ct also reveals traumatic lesions of the adjacent soft tissue structures ; however , minor abnormalities can be overlooked on ct [ 53 ]  . magnetic resonance imaging ( mri ) plays a fundamental diagnostic role , as it is the only imaging tool able to detect spinal cord injury and involvement of osteoarticular soft tissue structures , covering large segments or even the entire spine [ 54 , 55 ]  . 
 the early detection of these entities is important , as prompt surgical correction can help to preserve neurologic function . diagnostic imaging of the spine in trauma patients requires thorough knowledge of anatomy , traumatic mechanisms , and injury patterns . 
this knowledge is necessary for the optimal management of spinal injuries . acknowledgments the authors wish to thank angela martella for linguistic editing . compliance with ethical standards the study did not have any funding . conflict of interest author alessandra splendiani declares that she has no conflict of interest . 
 comparison among different diagnostic imaging exams in a prospective singlecenter study giuseppe lo re1 rossella de luca2 filippa muscarneri1 patrizia dorangricchia1 dario picone1 antonio pinto3 massimo midiri1 antonio russo2 roberto lagalla1 giuseppe cicero2 federica vernuccio1 sergio salerno1 giuseppe la tona1 received : 2 january 2016 / accepted : 1 june 2016 / published online : 22 june 2016 italian society of medical radiology 2016 abstract objective every patient could feel anxious when he waits in a radiological department to undergo diagnostic exams . 
 the aim of our study is to evaluate the impact of the radiological exams on patient anxiety . materials and methods we evaluated 343 patients ( mean age 54.83 years ) who underwent different types of diagnostic exams in the department of diagnostic imaging at our hospital from april 2013 to august 2014 . 
31 % of the patients were submitted to mr , 18 % to breast imaging , 10 % to x - ray , 22 % computer tomography and 19 % to ultrasound , as previously described . 
therefore , it was found that high levels of anxiety were present in most ( about 91 % ) of the patients and the scores varied according to the imaging examination and to the examinations reason : anxiety level was higher in non - oncological patients ( 54 % ) and in patients waiting to undergo to mri exams ( 29 % )  . conclusion our data suggest that the diagnostic exams are stressful events for the patient , also in non - oncological patients . 
also , further studies are needed to evaluate the anxiety level and the quality of the images , because the anxiety can result in a somatic disorder with hyperactivity of the autonomic nervous system which may affect the patients physical examination , causing problems in the evaluation of radiological images making to non - cooperative patient . 
 mri imaging is the examination that more of all led to an anxious state of patients but the main stressor is not related to the type of diagnostic examination , but to the uncertainty of the diagnosis , therapy and prognosis . keywords anxiety quality of life social support oncology diagnostic imaging stai palpitations and paresthesia , thoracic pain and dyspnoea , urinary urgency and gastrointestinal symptoms [ 5 ]  . chronic anxiety may present in many significant clinical scenarios such as generalized anxiety , simple phobia and social phobia . therefore , patients waiting to undergo diagnostic radiological procedures may feel a high emotional experience , characterized by a degree of anxiety that is different for each patient , and can be responsible for a strong psychophysical stress and impairment during the examination [ 6 ]  . the purpose of our study was to find stressors factors , in order to enable specific strategies to reduce anxiety in patients , improve compliance and optimize the execution of diagnostic examinations . introduction materials and methods in the last decades , there has been an increasing request of radiological examinations . 
due to the increase in life expectancy of the general population , spreading and increasing adherence to screening programs , and the effectiveness of medical and surgical therapies that increased the prevalence of oncological diseases , there has been an exponential increase in the number of radiological examinations performed for screening , diagnosis , and follow - up of diseases [ 1 ]  . however , these procedures may often lead to emotional impairment of patients , as anxiety that appears to a common feeling . 
anxiety is mainly due to the fear of the uncertainty of procedure , results of the examination , and possible consequence of invasive or not and health impairment [ 2 ]  . uncertainty and worry lead to anxiety as a primary physiological adaptation , which can result in a simple emotional reaction to a possible dangerous condition in some patients or , for other patients , it can result in a psychological disorder . 
both these kinds of anxiety may be acute or chronic [ 3 ]  . acute anxiety is felt in critical moments as during the execution of exams , waiting for the report , during the communication of the diagnosis and diagnostic procedures and during the treatment ( surgery , chemotherapy , radiotherapy ) or when the patient is told about the recurrence of his disease . 
this form of anxiety may present with both psychological and somatic symptoms [ 4 ]  . the first consists in concern for health ( e.g. , worries for future own problems and for relatives ) , in the sense of anxious waiting , in the worry , fear and expectation of danger , restlessness and difficulty in concentrating . 
on the other hand , somatic symptoms cause a hyper activation of the central nervous system , thus causing motor restlessness , tremors , headache , sleep disturbances , autonomic symptoms ( sweating , hot flashes or chills ) , dry mouth , dizziness , from april 2013 to august 2014 , 343 patients waiting to undergo diagnostic examinations in the radiology department of the university hospital of palermo were recruited . 
 according to the diagnostic examination performed , five different randomized groups were distinguished : breast examinations , ultrasound ( not breast ) , x - ray , computed tomography and magnetic resonance . 
the institutional review board approved this prospective single - centre study . before being submitted to the respective exam , all patients were asked to sign an informed consent for being submitted to the exam , making them aware of the respective imaging technique ( ionizing radiation , electromagnetic waves ) and the related risks , as adverse drug reaction related to contrast medium ( if planned )  . moreover , all patients were informed before being submitted to the psychological test about the aim and modalities of this study and an informed consent to participate was obtained . 
then , the patients received the questionnaire that was divided into two parts , respectively : the first part about the socio - demographic information ( age , sex , level of education , occupation and marital status ) and the second part about the clinical data related to the type of technique and reason of examination ( first diagnosis , screening or follow - up ) and referring reason distinguishing specifically for oncological diseases . 
all the completed questionnaires did not contain any personal data that could indicate the identity of patients in any way . state and trait anxiety inventory test the evaluation and measurement of anxiety levels have been performed administering the state and trait anxiety inventory test ( s.t.a.i. ) , in particular the scale y 1 that investigates the anxiety status [ 7 ]  . 1 3 radiol med ( 2016 ) 121 : 763768 s.t.a.i. 
tests were evaluated by a team of clinical psychologists and radiologists . they considered several parameters including the type of examination and reason of the examination ( first diagnosis , screening or follow - up ) , with a particular reference to patients with known oncologic disease and to patients waiting for mammography ( referring reason suspected cancer not screening )  . 
to compare levels of anxiety between oncologic and not - oncologic patients . thereafter , a descriptive analysis was performed ( mean , standard deviation sd , percentages )  . in particular , the fisher exact test was used to compare differences in discrete or categorical variables . 
on the other hand , considering oncologic patients , 11 % had severed anxiety levels while most of them had moderate / mild levels ( table 3 )  . patients with higher school education ( university degree ) showed lower anxiety levels compared to those with lower school education ( elementary , middle and high school ) , table 1 epidemiological data married or in a stable union gender male female marital status single separated widow education elementary or below middle school high school university or higher occupation intellectual - scientific business , services public service farming / fishing technical unemployed 1 3 766 radiol med ( 2016 ) 121 : 763768 table 4 correlation between anxiety level and instruction 0 ( % ) 1 ( % ) 2 ( % ) 3 ( % ) anxiety level education elementary or below middle school high school university or higher total table 5 correlation between anxiety level and gender anxiety level 0 ( % ) 1 ( % ) 2 ( % ) 3 ( % ) gender male female total discussion nowadays , the increase in longevity and the development of new diagnostic and therapeutic strategies lead to a raise in the number of people submitted to diagnostic , screening or follow - up examinations [ 2 ]  . 
the fear to undergo a new radiological procedure , the possibility of risks examination and the uncertainty about the outcome of the diagnosis are responsible for patients fear and anxiety [ 8 ]  . this means that medical staff must support patients that should experience severe levels of anxiety , since their anxiety may be clinically significant . our study proved a difference in the levels of stress related to the type of diagnostic imaging technique : patients waiting for an mri scan showed highest levels of anxiety compared to those waiting for ct , although mri does not imply the use of ionizing radiation . 
although electromagnetic waves used in mri are not harmful for human health , patients are worried more when they have to undergo an mri examination rather than tc ; this is probably due to the fact that ct is a more common investigation , requires less time , is generally best known and , therefore , patients are more aware of this examination [ 9 ]  . according to our data , anxiety is not directly correlated with the imaging technique but with the fear of being submitted to a second level examination . 
1 distribution of the diagnostic examinations table 2 correlation between anxiety level and types of exams anxiety level 0 ( % ) 1 ( % ) 2 ( % ) 3 ( % ) types of exams breast imaging ultrasound x - ray total patients oncologic non - oncologic total table 3 correlation between anxiety level and oncologic disease anxiety level 0 ( % ) 1 ( % ) 2 ( % ) 3 ( % ) with a significant p value ( p < 0.0005 ) : anxiety was felt in just 13 % of university graduated patients , in 30 % of patients graduated at high school , in 29 % of patients with middle school and in 28 % of patients with primary school ( table 4 )  . moreover , women showed higher levels of anxiety ( 61 % ) than men ( 33 % ) and , among females , the higher scores were obtained in patients waiting for mammography ( table 5 )  . 1 3 radiol med ( 2016 ) 121 : 763768 moreover , in our study the highest levels of anxiety were seen in patients waiting for ultrasound examinations ; this is probably a bias related to the fact that in our department of diagnostic imaging the ultrasound report is delivered to the patient at the end of the examination , while ct , mri and mammography reports will be delivered within a few days . 
hence , patients waiting for us examination experienced highest levels of anxiety probably because of the likely imminent delivery of the report ( table 2 ) [ 9 ]  . higher anxiety levels have also been found among patients with suspected oncologic disease : the mere suspicion of a cancer diagnosis can therefore elicit strong emotional reactions in patients , as the fear of possible need of surgery , or long and difficult medical treatments and even the fear of death [ 10 ]  . the diagnosis of cancer is such a traumatic event that it can induce the patient to a redefinition of his life . 
on the other hand , oncologic patients waiting for follow - up examinations showed lower levels of anxiety ; hence , the biggest stressor is the fear of the unknown both considering diagnosis and subsequent eventual therapy . 
these symptoms can make the patient less cooperative during this examination [ 15 ]  . understanding the causes and the reasons for those fears is the first and necessary step to develop specific measures aimed at preserving the mental and physical patient health as well as to improve his compliance . concerning women who are waiting for breast imaging , their anxiety may be related to the fear of a sever disease , the breast carcinoma , that is one of the most frequent diagnosis in females . conclusion our clinical practice suggests that the diagnostic exams are stressful events for the patient , also in non - oncological patients . also , further studies are needed to evaluate the anxiety level and the quality of the images , because the anxiety can result in a somatic disorder with hyperactivity of the autonomic nervous system which may affect the patients physical examination , causing problems in the evaluation of radiological signs and making the patient less cooperative during the exam [ 16 ]  . 
 as revealed in this study , mri imaging is the examination that more of all led to an anxious state of patients but the main stressor is not related to the type of diagnostic examination , but to the uncertainty of the diagnosis , therapy and prognosis . the final quality of the images obtained is inversely proportional to patients levels of anxiety [ 17 ]  . 
several studies have shown that the level of preoperative anxiety is a predictor of the pain experienced during procedures ; moreover , more anxious patients tend to require longer treatments , with the administration of a greater number of drugs and an increase in the risk of adverse events . 
radiologists and medical staff are not trained and do not have adequate skills and time to provide psychological support to patients . for these reasons , resources should be reorganized : in order to reduce patient anxiety while waiting the examination and make him more cooperative during the exam , it might be useful to pay attention to the anxiety level of patients in the radiology waiting rooms , as it commonly happens in oncologic ambulatories , mainly in breast imaging and mri units [ 18 ]  . 
furthermore , there is surely the need for closer cooperation among the various professionals ( radiologists and clinical psychologists ) to optimize patients outcomes and improve the efficiency of radiologic services and diagnosis . finally , should be useful professionalize the radiological staff to receive the patient , to inform him and perform exams with emotive involvement with a targeted education . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . informed consent this prospective single - center study was approved by our institutional review board . 
informed consent was waived due to its retrospective nature . radiol med ( 2016 ) 121 : 805810 doi 10.1007 / s11547 - 016 - 0659 - 9 radiotherapy threedimensional surface imaging for detection of intrafraction setup variations during radiotherapy of pelvic tumors giuseppina apicella1 gianfranco loi2 sara torrente1 silvia crespi1 debora beld1 marco brambilla2 marco krengli1 , 3 received : 23 february 2016 / accepted : 30 may 2016 / published online : 14 june 2016 italian society of medical radiology 2016 abstract purpose surface - based image guided radiotherapy ( igrt ) allows positioning and / or monitoring patients in 3 dimensions ( 3d ) , without the use of ionizing radiation . 
in this study , we report on intra - fraction motion measured by acquisition of multiple images of 3d body surfaces . materials and methods twenty - nine patients treated for pelvic tumors were enrolled . 
setup variations ( sv ) through three consecutive body surfaces acquired by the optical igrt system align - rt ( vision - rt , london , uk ) were analyzed before , during and at the end of treatment delivery . 
displacements along the main axes ( x , y and z ) from initial ( i ) to mid - treatment ( mt ) and final ( f ) acquisitions were recorded . 
these findings suggest that the initial setup control cannot not to be sufficient to guarantee treatment reproducibility , especially for long - lasting rt treatments . keywords radiotherapy surface imaging intrafraction setup organ motion igrt introduction image guided radiotherapy ( igrt ) is considered nowadays an essential tool to safely deliver high dose radiation to pelvic tumors by 3 - dimensional conformal or intensity modulated radiotherapy ( 3dcrt / imrt )  . most igrt techniques are able to determine the position of the target itself rather than surrogates based on skin marks or bony anatomy . 
based on that , various technologies can be used such us cone beam computed tomography ( cbct ) , electronic portal imaging device ( epid ) with fiducials , ultrasounds ( us ) , electromagnetic transponders and surface imaging systems . igrt may allow detecting setup variations between different sessions ( inter - fraction variations ) or during each radiotherapy session ( intra - fraction variations )  . 
 a few technology devices have been used for real - time monitoring of target position during radiotherapy delivery to detect intra - fraction organ motion [ 2 , 3 ]  . 
surface - based monitoring technology has been recently introduced in clinical practice , with the advantage of verifying and / or monitoring patient setup in 3d , without the use of ionizing radiation [ 46 ]  . the purpose of the present study was to investigate intra - fraction setup variations ( sv ) in the pelvic district acquiring multiple body surface images captured by a noninvasive 3d surface imaging system during each radiotherapy session . materials and methods twenty - nine consecutive patients affected by pelvic tumors and treated with imrt at our institution were enrolled in the present study after obtaining the informed consent following the ethical rules of our institution . 
twenty - two were males and 7 females with a median age of 72 years ( range 4887 ) and median body mass index ( bmi ) of 28 ( range 1839 )  . 
patients were treated in supine position using a leg immobilization system ( combifix - sinmed , civco , kalona , ia , usa )  . three skin tattoos , two lateral and one anterior , were marked for position verification by laser alignment . 
simulation was performed by spiral ct scanner ( lightspeed , general electric , milwaukee , wi , usa ) acquiring the pelvic district from l4 to 2 cm below the ischial tuberosities with slices thickness of 3 m a bladder filling protocol was adopted to obtain bladder comfortably full at the time of planning and during treatment . 
the dicom 3 images were transferred to the treatment planning system ( tps ) 1 3 radiol med ( 2016 ) 121 : 805810 pinnacle ( philips , eindhoven , the netherlands ) by local network . the quality assurance ( qa ) procedure for setup verification was performed by the surface imaging acquisition system alignrt ( visionrt , london , uk ) and by portal imaging . the alignrt system has been implemented at our institution since 2006 and the main aspects of its use and performances were described in previous papers [ 7 , 8 ]  . 
in brief , alignrt is a video - based three - dimensional ( 3d ) surface imaging system which is used to capture images of the body surface of the patient before and during the radiotherapy session . 
the system consists of advanced software , a computer workstation , two 3d camera units , cables and a template that is used for camera calibration of the treatment isocenter . 
the system is non - invasive , does not require the use of body markers and produces no irradiation during the imaging process . to verify patient setup in the treatment room , alignrt uses a reference surface that in our clinical setting is the dicom structure of the body contour automatically segmented by the tps on the simulation ct and imported via a local network . at the first patient setup , qa was performed according to the protocol adopted at our institution : initial patient positioning is performed by lasers and skin tattoos alignment , then , prior to each treatment session , the patient position is imaged and co - registered to the reference by the system surface matching software . 
the parameters of the rigid transformation that map the body surface captured in the treatment room are matched to the reference surface to obtain the translations and rotations to apply for the daily patient setup adjustments which are manually done by moving the treatment table . 
before starting irradiation , portal imaging is performed daily for the first five sessions and then weekly to cross - validate setup accuracy with bone anatomy matching . in the present study , intra - fraction movements were analyzed comparing three consecutive surface images : before ( initial , i ) , at the mid - treatment ( mt ) and at the end of treatment delivery ( final , f )  . 
the i images corresponds to the daily surface image acquired for each patient before starting irradiation . linear translation mismatches on the three axes ( x , y and z ) between the first surface imaging ( i ) and the further ones ( mt and f ) were recorded . 
the variables considered as potential source of intra - fraction sv were the followings : time of image acquisition during the treatment ( i , mt , f ) , direction of variation and fraction number along the treatment course ( fn )  . 
post hoc scheffs test was performed to asses intra - group statistical significance for each factor identified by anova as predictive for variability of setup mismatches . results a total of 6272 images from 792 fractions of 29 patients were available for the analysis . 
most of the literature studies focused on prostate gland intra - fraction motion , assuming that a shift of the target could be given principally from bladder and rectal filling or , extremely , from respiratory movements . 
the results from studies analyzing the movements of the prostate gland can probably be considered as the sum of the organ motion and the movements of the entire pelvis , being these two components not necessarily concordant in terms of directions and magnitude [ 10 , 14 ]  . in the present study , we focused on intra - fraction patient movements independently from target position by using a 3d surface imaging system to monitor sv during radiotherapy sessions for tumors of the pelvic district . 
we used the same surface imaging system ( alignrt , vision rt , london , uk ) already employed in a previous study to analyze the setup reproducibility of 16 prostate cancer patients . 
to our knowledge , the present study is the first report describing the use of 3d surface imaging as a igrt tool to analyze the total pelvic movements during a radiotherapy session . our study showed that the major sv occurs during the first part of treatment session ( from i to mt )  . 
in this regard , the setup time before igrt should be long enough to reduce the initial patient discomfort and the contraction of pelvic muscles just after positioning on the table . quite similar observations were reported by other literature studies investigating prostate gland movements . 
 [ 16 ] , a comparison of mean , random and systematic displacements between the groups of patients with long ( 11.1 min ) and short ( 4.8 min ) treatment times was performed . 
 [ 14 ] reported a 66 % of fractions showing pelvic motion outside a range of 2 mm in a time scale of 57 mthey also found a reversal of motion direction in many patients , concluding that it is insufficient to deduce intra - fraction motion just from an initial and end - treatment setup verification . actually , considering that patients can move during the time frame between two image acquisitions , movement occurring during treatment delivery could be missed . 
1 effect of time acquisition during the rt session on intra - fraction setup variations ( sv ) ; the vertical bars represent the 95 % confidence interval ( ci ) fig . 
2 effect of direction on intra - fraction setup variations ( sv ) ; the vertical bars represent the 95 % confidence interval ( ci ) first half of treatment delivery corresponding to a mean time span of 78 min from the start of treatment delivery . 
x ( p < 0.000001 ) , meaning that svs in the 3 directions can occur independently one from each other . discussion igrt has became a fundamental instrument for highly conformal radiotherapy techniques to reduce irradiation of non target tissues . 
other literature studies described intra - fraction organ motion , using 1 3 radiol med ( 2016 ) 121 : 805810 the ideal frequency to intercept intra - fraction motion . 
after a standard epid based setup control , they performed in - treatment megavoltage images for each treatment field , concluding that analysis of intra - fraction motion at specific time points during treatment is not as robust as having a continuous tracking device . 
contraction of pelvic muscles related to patient discomfort immediately after the setup can be envisaged as the most likely cause of this shi other studies , investigating target intra - fraction motion during prostate cancer radiotherapy , without considering the entire pelvis movements , reported similar findings . 
 [ 11 ] analyzing intra - fraction shifts relative to the skin - mark - based setup by multimodality igrt methods ( ultrasound , epi , cbct , implanted gold - seed markers and electromagnetic transponders ) during prostate cancer imrt found higher mean values and standard deviations in a - p direction ( 3.6 mm with us - based imaging )  . 
the four ways analysis and post hoc sheffs test suggested that setup variations can strongly depend from patient related characteristics , but no correlation between setup variation and age , gender , bmi , cancer type and duration of rt session could be performed because of the limited number of patients and the uniformity of these parameters in the analyzed series . 
in a next study , we plan to increase the number and the heterogeneity of patients in order to analyze more in depth the setup variability pattern in different clinical settings . conclusions monitoring patients through consecutive acquisitions of 3d surface images allowed detecting remarkable intra - fraction setup variations during rt sessions of patients with pelvic malignancies . 
contraction and relaxation of pelvic muscles , possibly related to initial patient discomfort after the setup procedure , can be identified as the most likely cause of this shithese findings suggest that the initial setup control , acquired just after patient positioning , could not to be sufficient to guarantee optimal treatment reproducibility , especially for long - lasting rt treatments . 
wood5 gian luca forni4 received : 10 december 2015 / accepted : 1 june 2016 / published online : 22 june 2016 italian society of medical radiology 2016 abstract purpose in magnetic resonance imaging ( mri ) relaxometry , various software programs are available to perform r2 * measurements and to estimate the liver iron concentration ( lic )  . 
the main objective of our study was to compare r2 * lic values , obtained with three different software programs based on specific decay models and calibration curves , with lic estimates provided by r2 - relaxometry ( ferriscan )  . methods this retrospective study included 15 patients with 15 baseline mris and 34 serial examinations . 
 ospedali galliera , mura delle cappuccine 14 , 16128 genoa , italy 2 department of medical physics , asl n.5 spezzino , via xxiv maggio 139 , 19124 la spezia , italy 3 medical physics unit , e.o. 
the monoexponential - plusconstant model provided the best agreement with r2 lic estimates . keywords liver iron overload - thalassemia liver iron concentration ( lic ) magnetic resonance imaging biopsy introduction the quantification and monitoring of body iron burden play a pivotal role in the clinical management of patients with inherited hemoglobin disorders such as thalassemia , hereditary hemochromatosis and sickle cell disease [ 1 , 2 ]  . 
liver biopsy provides a direct quantification of liver iron overload , but , owing to its invasiveness , it is not suitable for the longitudinal monitoring of patients ; furthermore , it is prone to sampling errors [ 3 ]  . magnetic resonance imaging ( mri ) - based techniques are able to produce effective estimates of liver iron concentration ( lic ) over the entire range of clinically relevant values [ 4 ]  . 
mri quantifies iron indirectly , by detecting the paramagnetic effects of hepatic iron ( stored as ferritin and hemosiderin ) , which interacts with the nearby protons [ 5 , signal intensity ratio techniques , depending on t2 or t2 * contrast [ 79 ] , have been proposed in various studies as a smart method for the assessment and quantification of 1 3 752 radiol med ( 2016 ) 121 : 751762 liver iron . 
 [ 8 ] have shown that the analysis of highly t2 - weighted gradient - recalled - echo sequences with a dedicated algorithm is a simple , rapid , and cost effective technique to detect and quantify liver iron overload . 
the main limitation of these techniques is that they are based on the use of a reference tissue , in which it is assumed that iron is not generally deposited ( usually paraspinal muscles ) [ 4 ]  . 
furthermore , they are characterized by a limited range of sensitivity ( the upper limit for hepatic iron estimates is 21 mg fe / g dry liver weight ) [ 10 ]  . both t2 and t2 * relaxation times shorten in the presence of iron . 
relaxometry methods can be used to calculate r2 [ 11 ] or r2 * values [ 12 ] the reciprocals of t2 and t2 * by fitting a decay model to the average signal intensity at various echo times [ 13 ]  . 
signal intensity ratio techniques depending on t2 or t2 * contrast [ 79 ] have been proposed in various studies as an immediate method for the assessment and quantification of liver iron . under conditions of iron overload , the signal intensity from the liver parenchyma decreases at increasing echo times and the rate of decay is proportional to iron loading . 
however , so far there is no consensus concerning the optimal relaxation rate parameter for lic estimation , since r2 and r2 * values generate comparable noninvasive estimates of lic [ 17 , 18 ]  . the st pierre et al . 
this technique has obtained food and drug administration ( fda ) approval , and is currently regarded as a noninvasive surrogate for liver biopsy in clinical trials [ 10 ]  . 
hepatic r2 measurements showed a curvilinear relationship with lic over the entire range of lics , with prediction errors comparable to those expected from the variability in liver biopsy [ 11 ]  . various methods and post - processing techniques have been developed for obtaining lic estimates from r2 * relaxometry [ 12 , 1416 ]  . 
analysis of the t2 * decay curves can be performed using various decay models , including the single exponential ( also called monoexponential ) decay and non - monoexponential models [ 13 ]  . 
the latter category comprises the monoexponential - plus - constant offset model [ 12 , 18 , 19 ] , which provides correction for noise and other artifacts in later echo images , and the truncated model , which allows the operator to manually discard from data fitting the echo times below the noise level [ 19 , 20 ]  . assuming constant acquisition parameters for the multiple gradient echo sequence , other factors that can influence the r2 * - derived lic estimate are the shape and size of the region of interest ( roi ) [ 10 ] , pixelwise versus non - pixelwise data fitting [ 21 ] , and the selection of the technique - appropriate calibration curve used for converting r2 * into the corresponding lic values [ 19 ]  . the main objective of our single center , retrospective study was to compare noninvasive quantification of liver iron overload from lic estimates obtained from three different r2 * relaxometry techniques with lic estimates provided by the ferriscan technique , which was used as a reference standard . methods patients the study protocol was approved by the local ethics committee ; informed consent was waived given the retrospective observational design of the study . 
the mean age was 34.7 ( range 1259 years ) ; eight patients were males ; eight had a diagnosis of - thalassemia major and seven had - thalassemia intermedia . 
a 1000 ml bag of saline solution was positioned at the left side of the patient to provide an external long t2 reference for the correction of instrumental gain drift [ 11 ]  . 
the image datasets for r2 measurements were sent through a secure electronic link to a central laboratory ( resonance health , western australia ) where lic reports were produced using a dedicated algorithm [ 11 , 17 ]  . 
ferriscan lic estimates were considered the reference standard . t2 * / r2 * measurement two - dimensional , spoiled , multiple gradient echo sequence was performed in the axial plane to measure hepatic t2 * / r2 * relaxation . 
 other imaging parameters were : 10 mm section thickness , 0 intersection gap , 125 khz bandwidth , one signal 96 average , and rectangular field of view with a 128 matrix adjusted to individual body habitus and breath - hold capacity [ 23 , 24 ]  . 
the multiple gradient echo sequence of each mri examination was analyzed using three commercially available software programs ( functool v.4.4 , general electric , milwaukee , usa ; cmrtools / thalassemia tools , cardiovascular imaging solutions , london , uk ; quanta hematology , camelot biomedical systems srl , genoa , italy )  . 
data were analyzed using functool software program according to a previously described method [ 23 , 25 ]  . 1 3 754 radiol med ( 2016 ) 121 : 751762 fig . 
1 43 - year - old woman with - thalassemia intermedia and severe hepatic iron overload ( > 15 mg / g as assessed by the reference method )  . 
the software program provides the t2 * / r2 * values ( mean and sd ) , calculated for a roi in the liver drawn freehand by the operator [ 26 , 27 ]  . 
generally , a multiple gradient echo sequence with 16 echoes was analyzed . in patients with severe iron overload , the multiple gradient echo sequence with eight echoes was processed to achieve a better fit with the monoexponential decay curve [ 23 ]  . 
the signal intensity of the liver parenchyma was measured in each image of the multiple gradient echo sequence , and values were plotted against the echo time for each image . 
r2 * values were converted into lic ( mg / gdw ) using garbowski et al.s equation [ 16 ]  . quanta hematology quanta hematology is a stand - alone software program dedicated to the voxel - wise measurement of t2 * / r2 * decay for the quantification of heart and liver iron overload and liver proton density fat fraction [ 24 ]  . 
the histogram of pixel distribution with mean , median and sd of t2 * / r2 * and lic values is computed in a freehand , elliptical or rectangular user - adjustable roi . 
in each voxel , the value of r2 * is estimated by fitting the signal intensity ( si ) , assessed at different tes 1 3 radiol med ( 2016 ) 121 : 751762 fig . 
a , b screenshots of the cmrtools software , where the region of interest is shown on the left side and the signal decay fit is shown on the right side . 
in this patient with severe iron overload , the last echo times were excluded by means of manual deselection to obtain an optimal fit ( r2 > 0.99 ) to the monoexponential decay model . 
after manual deselection of later echo times ( b ) , the final t2 * was 1.94 ms , corresponding to a r2 * of 526.3 hz and a lic of 16.5 mg / g fig . 
2 : si ( te ) = a exp ( te / t2 ) + b where , a and b are constants and te the different echo times . the quality of the fit is evaluated using the r2 statistical parameter , and the operator can exclude voxels with low quality fit from further processing . 
r2 * and lic values were recorded and used for further statistical analysis . a medical physicist identified the slice corresponding to that used for r2 - relaxometry assessment in the multiple gradient echo sequences ( with 8 and 16 echoes )  . 
after anonymization , selected slices were analyzed and a random list generated to guarantee nonconsecutive assessment of serial examinations . mri images underwent analysis and post - capture processing by an abdominal radiologist ( fp ) with 3 years of experience in liver t2 * / r2 * - relaxometry . 
 continuous data that followed a normal ( gaussian ) distribution were expressed as mean and sd , while continuous data without a normal distribution were expressed as median and range ( minmax )  . 
 furthermore , lic estimates were stratified , according to the classification of olivieri and brittenham [ 28 ] , into normal ( < 3.2 mg / g ) , mild ( 3.27 mg / g ) , moderate ( 715 mg / g ) and severe ( > 15 mg / g ) iron overload . 
the percentage difference between quanta hematology r2 * ( exponential - plus - constant fit ) and cmrtools r2 * ( monoexponential decay model with truncation of later echo times ) was 23 % . 
in untransformed lic units , 95 % cis for the mean difference between ferriscan and quanta hematology lics were 76 % ( lower ) and 132 % ( upper )  . 
horizontal lines indicate the mean difference and the limits of agreement , which are defined as the mean difference plus and minus 1.96 times the sd of the differences 1 3 radiol med ( 2016 ) 121 : 751762 fig . 
when repeated lic measurements obtained by the reference method were stratified according to the olivieri and brittenham algorithm [ 28 ] , three measurements were classified as normal , 21 as mild , 17 as moderate and eight as severe . 
 however , they are inherently less precise than relaxometry [ 4 ] and they are characterized by a limited range of sensitivity [ 10 ]  . both r2 and r2 * mri measurements , by means of dedicated spin - echo and multiple gradient echo imaging sequences , produce accurate noninvasive estimates of hepatic iron over the entire clinically relevant range [ 18 ]  . 
 lack of homogeneity in the external magnetic field and susceptibility artifacts , such as metal clips and airtissue interfaces , have less influence on r2 techniques [ 4 , 10 , 17 ] , 1 3 760 radiol med ( 2016 ) 121 : 751762 which are insensitive to the size and shape of the imaging voxel [ 10 , 12 ]  . 
by contrast , r2 relaxometry is susceptible to motion artifacts and has a poor signal - to - background noise ratio at longer echo times [ 10 , 12 ]  . 
 r2 * - based techniques are more readily available and easy to perform , and are less sensitive than r2 measurements to variations in the size and distribution of iron particles [ 29 ]  . our work analyzes three r2 * - based methods for lic estimation and compares them with the widely used r2 technique ( ferriscan ) , which was originally validated to liver biopsy in 105 subjects [ 11 ] , and the calibration model confirmed in a subsequent sample of 233 subjects [ 17 ]  . 
in addition , quanta hematology and functool employ the traditional pixelwise mapping approach , where the fitting is performed for each pixel in the roi , yielding a complete r2 * map . 
by contrast , cmrtools uses a region - based fit , where all the pixels within the roi are averaged together for each te , and the fitting is performed for this averaged decay curve [ 21 ]  . this is the first study to compare various software programs and post - processing approaches for r2 * lic estimation with r2 - relaxometry . 
according to a previous report [ 19 ] , software programs employing the exponential - plus - constant fit for signal decay , like quanta hematology [ 24 , 30 ] , provide r2 * values that average higher than those obtained with other models , including the monoexponential decay curve ( functool ) [ 26 , 27 ] and the monoexponential decay curve with truncation of later echo times ( cmrtools / thalassemia tools ) [ 19 , 20 ]  . 
in the cross - sectional analysis of baseline data , r2 averaged higher than the quanta hematology lic , as reported in a previous study [ 18 ]  . this trend to overestimation becomes evident with increasing lic values . 
if there is no significant contribution to the overall signal intensity from bile , blood or fat , the truncated monoexponential decay model would be more appropriate [ 31 ]  . 
in the present study , we used a freehand - drawn roi including the whole liver profile within each selected slice , avoiding large blood vessels , biliary ducts and focal lesions . from the analysis of the blandaltman plots of the longitudinal assessment , it is evident that the differences between the ferriscan and r2 * lic values show constant directional changes according to increasing iron burden . 
in particular , r2 * lic values tend to be higher than r2 lic at iron levels < 7 mg / gdw , while r2 lic averages higher than r2 * lic at higher levels of iron , with substantial discrepancy between the two techniques for iron burdens of more than 25 mg / gdw . 
the calibration curve for ferriscan is curvilinear [ 11 ] , while that of r2 * techniques have shown a linear relationship with the 1 3 radiol med ( 2016 ) 121 : 751762 histological quantification of iron overload [ 12 ]  . 
in addition , the ferriscan calibration curve was obtained by means of paraffin - embedded specimens , while fresh specimens were used for the liver r2 * calibration curve proposed by wood and colleagues [ 12 , 18 ]  . 
indeed , chemical analysis of paraffin - embedded biopsies may produce artifactually higher licdw values due to the loss of lipophilic tissue during dewaxing [ 32 ]  . in two previous studies [ 18 , 33 ] , wood and colleagues used the longitudinal r2 and r2 * lic measurements to calculate the iron chelation efficiency , which is the molar change in total body iron divided by the moles of drug consumed . 
values from both cmrtools and quanta hematology were in good agreement with the reference method ; in particular , quanta hematology produced the lowest mean difference with closer limits of agreement in the blandaltman analysis for repeated measurements per subject . with regard to the clinical classification of iron overload according to the olivieri and brittenham algorithm [ 28 ] , no significant difference ( p > 0.05 ) was seen among the various software programs evaluated in this study . 
we found that the different values for concordance with the reference method were not close to 100 % ; this may be related to the high prevalence ( 77.6 % ) of examinations showing mildto - moderate lic values , in the region of the cutoff value of 7 mg / g . 
in patient cohorts characterized by significant skewedness toward heavy iron overload , the incidence of misclassification would probably be less evident . our study has several limitations ; the main drawback is related to the small number of patients included in the study , resulting in only 15 baseline examinations for the cross - sectional analysis . 
however , the use of dedicated statistical tests to manage repeated lic measurements allowed us to perform an effective longitudinal analysis that finally confirmed the preliminary cross - sectional assessment . conclusions in conclusion , in both the cross - sectional and longitudinal settings , the software program based on the monoexponential - plus - constant decay model provided the best agreement with r2 lic estimates . 
the exponential - plus - constant decay model systematically produced higher r2 * values than the model with monoexponential fit with truncation of later echo times ; however , it is possible to obtain a better agreement between the two fitting methods by applying the appropriate calibration curves for converting r2 * into the correspondent lic values ,  . 
r2 * lic values tend to be higher than r2 lic at iron levels < 7 mg / gdw , while r2 average lic values are higher than r2 * lic with increasing iron burden . 
increase or decrease in these angles are helpful in the diagnosis of conditions such as hindfoot varus or valgus , congenital talipes equinovarus ( clubfoot ) , pes cavus / planus congenital vertical talus , skewfoot deformities and calcaneal fracture [ 3 , 4 ]  . 
in the literature , there are some studies investigating the role of angle measurements in orthopedic diseases such as femoroacetabular impingement [ 5 ] , ischiofemoral impingement [ 6 ] or wrist degeneration [ 7 ]  . 
the purpose of this study is to evaluate the relationship between talar ocds and foot angles and their usability in the diagnosis , especially in stage 1 , in which the edema is the only magnetic resonance imaging ( mri ) finding [ 8 ]  . 1 3 802 radiol med ( 2016 ) 121 : 801804 fig . 
2 the lateral talocalcaneal angle was measured as the angle between the mid - talar axis and the mid - calcaneal axis ( parallel to the calcaneal inclination axis ) materials and methods we retrospectively explored patients who underwent ankle mri and conventional radiography ( cr ) in our department between september 2013 and january 2015 . 
we also measured the calcaneal inclination axis by drawing a line between the most inferior portion of the calcaneal tuberosity and the most distal and inferior point of the calcaneus at the calcaneocuboid joint on a lateral foot radiograph . 
the variables were investigated using analytical methods ( kolmogorovsmirnov ) to determine whether or not they are results fifty - four patients ( 33 females , 21 males ) with a mean age 14.5 years ( range 1867 ) were included in the of 43.77 1 3 radiol med ( 2016 ) 121 : 801804 study . 
no relationship was observed between ocds and calcaneal inclination angle or bohlers angle . discussion ocds of the talus are common lesions and its etiology is generally considered to be traumatic [ 1 ]  . 
 [ 15 ] reported an ocd grading system based on mri , grade 1 ; thickening of articular cartilage , grade 2 ; breached articular cartilage and low signal rim behind fragment , grade 3 ; articular cartilage is breached with high signal t2 changes behind fragment , grade 4 ; loose body with defect of articular surface . 
 the lateral talocalcaneal angle is drawn on a weight - bearing lateral foot radiograph as the angle between the mid - talar axis and calcaneal inclination axis [ 16 ]  . 
to our knowledge , this is the first study evaluating the relationship between the foot angles and talar ocds . acknowledgments no financial support was received for this paper . compliance with ethical standards conflict of interest safiye tokgoz ozal declares that she has no conflict of interest . 
the collateral findings were classified into three classes , according to their clinical significance , as follows : not or low significant ( class 1 ) , moderately or potentially significant ( class 2 ) , and significant ( class 3 )  . 
 a chi - square ( 2 ) test was performed to assess the statistical significance of differences in the incidence of collateral findings based on age ( 50 and > 50 years old ) , gender and histology ( hodgkin and non - hodgkin lymphoma )  . results ninety - one of 114 patients ( 79.8 % ) had one or more incidental findings on wb - mri . 
collateral findings were more frequent in class 1 ( 43 % ) ; abnormalities found in 35 patients ( 30.7 % ) were considered potentially significant , whereas seven patients ( 6.1 % ) demonstrated significant collateral findings requiring immediate treatment or * domenico albano albanodomenico@me.com 1 department of radiology , dibimed , university of palermo , via del vespro 127 , 90127 palermo , italy 2 department of hematology i , azienda ospedali riuniti villa sofia - cervello , viale strasburgo 233 , 90146 palermo , italy 3 dipartimento di scienze biomediche avanzate , universit degli studi federico ii , via pansini 5 , 80131 naples , italy 4 dipartimento di diagnostica per immagini , aorn a . 
patients underwent wb - mri both for staging of lymphoma in a specific research protocol and to monitor the disease during and after treatment along with fdg - pet / ct . inclusion criteria were absence of contraindications to mri ( such as claustrophobia and implanted pacemakers or neurostimulators ) , histologically confirmed lymphoma , age over 14 and performance status with values from 0 to 2 according to ecog scale ( eastern cooperative oncology group )  . the demographic characteristics of the study population are shown in table 1 . wbmri protocol wb - mri was performed by a 1.5 t ( t ) mr scanner ( achieva , philips healthcare )  . no intravenous contrast agent was administered . 
coronal t1 - weighted ( t1w ) turbo spin - echo and half - fourier multishot t2 - weighted short inversion time inversion recovery ( t2w - stir ) turbo spin - echo whole - body images and axial dwibs images were acquired , using the built - in body coil ( achieva , philips healthcare ) for signal reception . 
 three orthogonal directions with b high - resolution maximum intensity projection ( mip ) images were reconstructed and blackwhite inverse greyscale was used in all cases . seamless coronal whole - body t1wand t2w - stir images were created by merging separately acquired stations using software implemented in the standard operating console . 
the applied wb - mri protocol yielded a craniocaudal coverage of 185.5 cm , which was deemed to be sufficiently large to image the area from the cranial vertex to the toes in the majority of patients . 
however , if the patients length exceeded 185.5 cm , the most caudal part of the body ( corresponding to the patients feet and / or distal tibiae ) was not included in the image volume . 
of signals averaged total scan time ( min ) free breathing ( fb ) , breath hold ( bh ) , or respiratory triggering ( rt ) fb and bh image interpretation and categorization of collateral findings all images were retrospectively interpreted by two radiologists , respectively , with 15 and 8 years of experience in mr imaging , who were blinded to the results of other diagnostic exams . 
disagreements were resolved by consensus . if the finding had not a univocal interpretation , the radiologists evaluated other available diagnostic exams performed by patients before the wb - mri scan . the findings detected on wb - mri scans were considered as collateral if were not related to lymphoma . we categorized collateral findings using the same criteria as those used by cieszanowski et al . 
among those of class 3 , six findings remained in this class after subsequent imaging work - up or / and histologic diagnosis , whereas two of them were downgraded . 
coronal t1w ( a , b ) , coronal t2w - stir ( c ) , and mip greyscale inverted dwi ( d ) images show a prostate enlargement ( b , c , d ; arrowheads ) and an intramuscular lipoma ( b ; circle ) in a patient with splenomegaly and multiple locations of lymphoma in right cervical , right axillary , aortic , and bilateral iliac nodal stations ( a , b , c , d ; arrows ) fig . 
coronal t1w ( a ) , coronal t2w - stir ( b ) , and mip grey - scale inverted dwi ( c ) wb - mri images show a complex ovarian lesion with fat areas . 
the number of mri scans has more than tripled between 1995 and 2005 [ 26 ] , and there is an unavoidable increase in detection of collateral findings [ 27 ]  . the present study estimates the frequency of collateral findings identified on wb - mri . to our knowledge , there are different studies evaluating collateral findings on wb - mri that were all examining healthy general population [ 1116 ]  . 
thus , our study is the first on patients with lymphoma undergone wb - mri . in our study , the rate ( 36.8 % ) of collateral findings with potential or significant clinical relevance ( class 2 and 3 ) was in line with other studies regarding wb - mri [ 13 ]  . there are many clinical , social , and economical advantages associated with the diagnosis of collateral findings : first , the early detection of significant disease leads to a timely treatment and improvement of prognosis ; second , the occasional early diagnosis of many diseases reduces the costs for healthcare system ; in addition , some of these findings turn out to be quite useful in case of surgery ; finally , an extensive evaluation of patients clinical features provides data which could be useful for a prognostic value . however , many downstream consequences are negative , indeed , the risk is the depiction of a substantial number of incidental lesions which can not be accurately characterized on wb - mri images , with the consequent possibility to overestimate a suspicious finding . for this reason , it is crucial to find a balance between benefits of an early diagnosis and risks of further unnecessary investigation to protect patients from severe psychological distress . 
 [ 12 ] analyzed the psychosocial impact of communicated incidental findings from wb - mri concluding that disclosed incidental findings may lead to substantial psychosocial distress for patient . a limitation of our study is the lack of a statistical comparison with previous studies performed on healthy population , but it is hard to compare the results of other studies due to different mri systems and protocols used for image acquisition , various methods of data analysis , and absence of standardization for the classifications of detected lesions . in our study , the incidence of collateral findings ( 79.8 % ) is lower than that previously reported by cieszanowski et al . 
 [ 11 ] of random participants in imaging research , in which the incidence of the majority of abnormalities increased with age . there were not statistically significant differences related to gender , and these data are in line with previous studies [ 13 , 14 ]  . collateral findings detected with wb - mri altered the management of lymphoma in two patients of our study population . 
both of them had follicular lymphoma in complete remission after induction chemotherapy with r - chop and could not start rituximab maintenance therapy because of the diagnosis of lung adenocarcinoma . wb - mri is a well - established modality , especially in some diseases , such as multiple myeloma . 
it allows to avoid radiation exposure and contrast administration and provides images of the human body from head to toe with high spatial resolution and high sensitivity and specificity [ 28 , 29 ]  . 
 furthermore , it accurately evaluates bone marrow with an excellent reliability for marrow involvement assessment in oncologic diseases [ 30 , 31 ] and also allows to identify important findings , such as osteonecrotic lesions which are very common in patients who receive chemotherapies [ 32 ]  . in conclusion , wb - mri is a useful procedure that allows to detect collateral abnormalities of organs not involved by disease . 
 however , in several cases , the detection of collateral findings can also result in the identification of insignificant findings that could be stressful and harmful for patients . compliance with ethical standards conflict of interests the authors declare that they have no conflict of interest . 1 3 800 radiol med ( 2016 ) 121 : 793800 ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the neeof lesions was 4.4 dle path was carefully planned and calculated on the cbct virtual navigation guidance system , which acquired 3d ct - like cross - sectional images . 
diagnostic performance , procedure details , complication rate , and patient radiation exposure were investigated . results the technical success rate of pnb under cbct virtual navigation system was 100 % ( 100 / 100 )  . 
for example , tumors , such as thymoma , are often treated with surgery , whereas lymphoma or metastatic lesions would be treated with chemotherapy or radiotherapy [ 3 ]  . 
however , the conventional ct guidance has limitations in the lack of real - time monitoring and gantry tilting for a more accessible needle pathway to the target lesion [ 6 , 7 ]  . 
the cbct systems offer the real - time visualization of tnb procedures and more flexibility in the orientation of the detector system around the patient compared with the traditional ct systems [ 8 , 9 ]  . 
therefore , the pnb 1 3 770 radiol med ( 2016 ) 121 : 769779 procedures assisted by advanced 3d needle guidance systems can be performed in a sterile workspace with flexible system angulation capability as well as instantaneous fluoroscopic feedbacks [ 10 ]  . 
indeed , owing to this systems ability to facilitate more accurate and safer needle placement , it has already been shown to provide excellent diagnostic accuracy for biopsy of the lung lesions [ 2 , 8 , 9 , 1119 ] ( table 1 )  . 
this paper describes our preliminary experience with pnb for mediastinal lesions biopsy under the cbct guidance system . methods and materials patients this retrospective study was approved by the institutional review board of the first affiliated hospital of zhengzhou university with waiver of patient informed consent . 
the lesion size was recorded as the maximum diameter in the image data by one chest radiologist ( han xw , 20 years of experience in image - guided pnb )  . image acquisition 3d cbct images of the patients were acquired with a rotational angiographic system ( artis zeego , 30 40 cm fd detector , siemens healthcare , forchheim germany )  . 
the time from the end of the data acquisition to the presentation of multiplanar images on the workstation ranged between 43 and 45 s . needle path planning and guidance procedure as the second step , the needle path was planned on the same workstation using the commercially available software ( syngo iguide , siemens healthcare )  . 
figures 1 , 2 and 3 demonstrated this procedure for a 2.50 cm lesion in middle mediastinufigure 4 demonstrated this procedure for a 3.50 cm lesion in posterior mediastinufigure 5 demonstrated this procedure for a 1.80 cm lesion in middle mediastinuthe reconstructed 3d volume was first loaded . 
the needle orientation was adjusted until both the tip and hub of the needle in the fluoroscopic image were superimposed and located at the center of the circle and the cross . 
the patient was placed in either supine or prone position according to location of the lesion , and local anesthesia was given ( 1 % lidocaine , 10 ml )  . 
a 16 - gauge needle ( quick - core , cook medical inc . , bloomington , in , usa ) was advanced along the planed path under real - time fluoroscopy . 
thereafter , post - procedure ct images were 1 3 radiol med ( 2016 ) 121 : 769779 1 3 772 radiol med ( 2016 ) 121 : 769779 fig . 
the patients remained in the hospital for 24 h for observation after the procedure . lesion characteristics and procedural records operators documented lesion characteristics as well as the procedural records in our database . 
we recorded several factors during tnb ; the patients positions during pnb , skinto - target distance , the number of biopsies , the number of ct acquisitions , needle approach , total procedure time ( defined as the duration from local anesthesia injection to the end of post - procedure cbct )  . 
we recorded the total coaxial introducer indwelling time and effective radiation exposure dose during the entire procedure ( fluoroscopy dose and cbct dose )  . pathological results , diagnostic accuracy the pathological reports of biopsy specimens , surgical specimens , or follow - up images were reviewed to evaluate the final diagnosis of target nodules . 
the needle was advanced along the planned needle path ( dotted line ) from skin entry site ( white cross ) to target lesion site ( white circle ) fig . 
3 cbct scan confirmed the needle position in multiplanar ( ac ) and volume - rendering ( d ) images 1 3 774 radiol med ( 2016 ) 121 : 769779 fig . 
cbct scan confirmed the needle position ( e , f ) a malignant or a specific benign pathology , such as thymoma or sarcoidosis , it was accepted as the final diagnosis . 
 ( 3 ) in the cases of non - specific benign pathology ( negative for malignancy , chronic inflammation , etc . ) , follow - up ct helped to decide whether the lesion would be truly or falsely benign , or indeterminate . 
 ( 4 ) if a nodule of non - specific benign pathology did not show a sufficient interval decrease in size nor had follow - up images , its final diagnosis was defined as indeterminate . 
pneumothorax was evaluated with post - procedural cbct and follow - up chest radiographs during the hospitalization . all data analyses were performed using the excel 2010 ( microsoft , redmond , wa ) and spss software ( version 1 3 radiol med ( 2016 ) 121 : 769779 table 2 lesion characteristics and procedure records of flat detector cone - beam ct - guided percutaneous needle biopsy of mediastinal lesions 13.0 ; spss , chicago )  . 
76 lesions were located in the anterior mediastinum , 12 lesions in the middle mediastinum , and 12 in the posterior mediastinuthe patients underwent tnb in the supine position in 85 cases and in the prone position in 15 cases . 
with regard to the mediastinal needle approach used , the parasternal approach was used for 78 lesions , the paravertebral approach for 12 lesions , and transpulmonary approach for 10 lesions . 
the final diagnosis of benign lesions was made on the basis of surgical pathology ( n 4 ) , including the conventional open surgery ( n 2 ) and endoscopic surgery ( n 7 )  . 
 the other three patients ( one with hd and two with nhl ) had completed the entire treatments , and tumor volumes were reduced more than 80 % compared with pretreatment . 
puncture point was oppressed for 20 min , and bleeding was stopped . discussion imaging - guided pnb is regarded as an adequate technique for characterizing mediastinal lesions to be used before invasive surgical diagnostic procedures ( mediastinoscopy , thoracoscopy , anterior mediastinotomy , and exploratory thoracotomy ) [ 21 ]  . 
moreover , the cbct systems offer real - time visualization on tnb procedures and more flexibility in the orientation of the detector system around the patient compared with the traditional ct systems [ 25 ]  . 
 [ 26 ] demonstrated that the cbct was the preferred modality over ct , irrespective of the level of operator experience , in terms of accurate needle placement in difficult guidance procedures requiring double - angulated needle paths . 
another sampling system is core biopsy , which relies on the use of special semiautomatic or automatic cutting needles with a quick - release mechanism and a 14to 18 - gauge caliber . 
the larger amount of tissue harvested allows sophisticated laboratory investigations , such as electronic microscopy , immunohistochemistry , and tumor - marker analysis , and all factors improve diagnostic specificity [ 27 ]  . 
we believe that this low incidence of pneumothorax was possible , as the virtual navigation system enabled us to select a safer and more accurate targeting route in navigating the needle approach to the target . 
 of the three patients who had pneumothorax , all patients had pulmonary emphysema along the needle pathway , and this may suggest that considering emphysema in the needle pathway would be more likely to lead to the occurrence of pneumothorax . 
considering the intrinsic disadvantage of cbct , in which the large cone angle increases scattered radiation as well as noise , which in turn can disturb the discrimination of low - contrast objects , vascular injury during cbct - guided pnb is of significant concern . 
however , after scrupulous review of the diagnostic contrastenhanced ct data taken prior to the procedure , the estimation of the lesion boundary and the safe range for needle advancement was feasible [ 20 ]  . 
 the other there patients ( one with hd and two with nhl ) had completed the entire treatments , and tumor volumes were reduced more than 80 % compared with pretreatment . 
the lesion may be malignant , but the sample obtained may lie outside the nodule borders or come from a necrotic area , thus preventing pathologists from establishing a correct diagnosis . 
on the basis of our results and the data from the literature regarding lung biopsies performed with cbct guidance , despite the limited amount of currently available data and the lack of homogeneity , a slight reduction in dose could be hypothesized with the use of iguide guidance . 
 the radiation dose of cone - beam ct - guided biopsy may not be a substantial problem , although a continuous effort must be made to reduce the radiation dose through use of a small field of view or collimation . the limitations of this technique should also be mentioned . 
as patient movements may result in motion artifacts and affect the registration accuracy of the projected path , the key factor for achieving successful needle guidance is to generate high - quality 3d cbct images . 
normalization ability was defined as reduction in blood pressure , decrease in number of antihypertensive medicine use , reduction in serum aldosterone , and increase in serum potassium level . results there was no statistically significant demographic difference in both groups . 
the mean tumor size was 18 ( 825 ) mm in rfa and 19 ( 1125 ) mm in la groups , * sung - lang chen cshy650@csh.org.tw 1 department of urology , chung shan medical university hospital , no . 
110 , chien - kuo north rd . , section 1 , taichung 402 , taiwan 2 department of medical imaging , chung shan medical university hospital , taichung , taiwan 3 department of physical medicine and rehabilitation , chung shan medical university hospital , taichung , taiwan 4 school of medicine , chung shan medical university , taichung , taiwan respectively . 
the treatment goal for pa is to normalize blood pressure ( bp ) , serum aldosterone , and potassiuafter being first described in 1992 [ 2 ] , laparoscopic adrenalectomy ( la ) has gradually become the gold standard treatment for apa over the past few decades . 
the cost , prolonged learning curve , 1 3 812 radiol med ( 2016 ) 121 : 811819 and length of recovery are also relative disadvantages [ 3 ]  . 
 therefore , therapeutic options with lower invasiveness may be more appealing to patients , especially in patients with high surgical risks . percutaneous intervention ( pci ) has shown promising results in the treatment of nonfunctional adrenocortical carcinoma or adrenal metastasis and has been developed to reduce invasiveness [ 46 ]  . 
pci methods that have already been used to treat adrenal tumors include chemical injection ( acetate or alcohol ) [ 4 ] , cryotherapy [ 5 , 6 ] , microwave [ 7 , 8 ] and radiofrequency ablation ( rfa )  . 
although both la and rfa were available in clinical treatments of adrenal neoplasm , there still existed limited data to compare therapeutic effects between la and rfa in apa . the purpose of our study was to retrospectively compare the efficacy and safety between la and rfa in treating adrenal apa . 
we also demonstrated the difference and equivalence of normalization ability including reduction of bp , plasma aldosterone level , antihypertensive medicine use , and increase of serum potassium level in both of our study groups . materials and methods after obtaining institutional review board approval and waiver of informed consent , we retrospectively evaluated images and medical records of all patients with solitary adrenal apa who received la and rfa between september 2009 and september 2013 . 
in the rfa group , one patient was unsuitable for la due to old age and cardiovascular comorbidity ; the others were unwilling to receive surgical intervention . all patients with hypertension , systolic blood pressure ( sbp ) > 140 mmhg or diastolic blood pressure ( dbp ) > 90 mmhg , and hypokalemia were examined if pa was impressed . 
 the diagnosis of pa was then established if the oral sodium loading test revealed 24 - h urinary aldosterone elevation after a 3 - day high - salt diet [ 13 ]  . 
adrenal vein sampling , however , was not a routine in our department . as our adrenal apa treatment routine , all patients had been reviewed by our endocrinologists to optimize bp control and correcting hypokalemia . 
immediately before treatment procedure , a prophylactic dose of parenteral antibiotics ( intravenous cefazolin 1.0 g ) had also been administered 1 h before operation . of the 18 patients , 13 received laparoscopic adrenalectomy ( la - a ) , 5 received retroperitoneoscopic adrenalectomy ( la - r ) due to previous abdominal surgery . 
they were put into the prone position on ct scanner examination table after general anesthesia with continuous monitoring of bp , heart rate , electrocardiography ( ecg ) tracing , and oxygen saturation . 
the cool - tip radiofrequency system was used with a 200 - w radiofrequency generator ( cool - tip rf generator ; covidien , boulder , co , usa )  . 
once a successful puncture was achieved , a standard 6 or 12 - min cycle of ablation and impedance - control algorithm was applied while the patient was in the same position . 
imaging guidance with ct allowed visualization during the course of treatment which had been reported in numerous literatures over the past few decades [ 911 , 15 , 16 ]  . 
b axial ct image obtained in prone position shows radiofrequency electrode needle extending into right adrenal tumor scans were typically obtained at 120 kv and 270 mas with a slice thickness of 35 mm and a pitch of 1 . 
tyan. the ablation procedure would immediately cease if ( 1 ) the systolic bp increased above 180 mmhg or diastolic bp above 110 mmhg , or ( 2 ) the occurrence of any possible life - threatening events . 
all patients were performed in an inpatient setting to ensure safe monitoring . during outpatient follow - up after treatment , serum potassium level and aldosterone level were routinely repeated at the 16 - month intervals . 
at 36 - month interval after operation , we usually performed a contrast - enhanced ct scan to check for the completeness of tumor ablation . we defined complete responses when there was no positive contrast enhancement on the residual adrenal lesion as shown in the follow - up ct scan in the rfa group . 
overall , rfa was defined as successful in treating apa both when tumor ablation was radiologically complete and pa was biochemically cured . the operative time , hospital stay , and post - operative pain scale were routinely obtained and recorded in medical charts . 
we established four recorded parameters : ( 1 ) bp ( the mean of three separate recordings at the clinic ) , ( 2 ) plasma serum aldosterone level , ( 3 ) the lowest measured serum potassium level , and ( 4 ) the current number of antihypertensive medicine use , as the normalization ability . 
the normalization ability before and 6 months after procedures was compared between both groups for the bp might improve as long as 6 months after surgical intervention [ 18 ]  . any complication occurring within 30 days after the procedure was recorded and illustrated in the charts . 
once peri - procedure events occurred , they were immediately managed by the stand - by anesthesiologists . statistical analysis we use independent students t test to compare before after therapeutic effects of rfa and la groups . 
paired students t test was used to determine whether the la and rfa share the same normalization ability in the bp , plasma aldosterone , serum potassium , and reduction of antihypertensive medicine use . 
there was one case of chronic kidney disease stage 4 , one case of diabetes mellitus , one case of permanent atrial fibrillation , and one case of chronic hepatitis b and coronary artery disease with congestive heart failure in the rfa group . 
in contrast , four of seven ( 57.1 % ) patients in rfa group used mineralocorticoid antagonist . the mean of lowest measured potassium level was 2.4 mmol / dl in la group and 2.3 mmol / dl in rfa group 1 3 radiol med ( 2016 ) 121 : 811819 fig . 
ten of 18 patients ( 55.6 % ) in the la group received potassium supplements , while six of seven patients ( 85.7 % ) in the rfa group received potassium supplements . 
 the mean serum aldosterone level was 609 and 525 pg / ml in la and rfa group before treatment , respectively ( p 0.663 ) ( table 2 )  . 
there was no statistical difference in the pre - procedure bp , number of antihypertensive medicine use , lowest measured potassium level , and serum aldosterone level . after treatment parameters comparison histopathological examination of the resected adrenal glands confirmed the diagnosis of adrenocortical adenoma in all patients in the la group . 
notably , reduction in bp , decrease in number of antihypertensive medicine use , reduction in serum aldosterone and increase in serum potassium level , which we considered as normalization ability , were compared between these two groups . 
the other nine patients in the la group and five patients in the rfa group experienced partially improvement in bp , as there was reduction in the number of antihypertensive medication required . 
however , there was no significant difference in the hospital stay between the two groups ( p 0.075 ) ( table 3 )  . hypertensive crisis and other complications of all the patients in our study , only one patient presented with intraoperative hypertensive crisis during the rfa procedure . 
in the 6 months of follow - up , the patients bp and serum potassium level all normalized ( 123 / 68 mmhg and 4.0 mmol / dl )  . 
besides traditional outcome parameters , we analyzed normalization ability between both groups to demonstrate the non - inferior effect of rfa compared with la . la had been the gold standard for the treatment of apa with extraordinary therapeutic effects over the past few decades . 
furthermore , vascular or adjacent organ injury complication , the need for general anesthesia , and the relatively steep learning curve may preclude the limited usefulness of therapeutic options [ 21 ]  . 
thus , less invasive and easy - to - use therapy must be developed . laparoscopic adrenalectomy was associated with significantly reduced parenteral pain medication requirements and more rapid resumption of a regular diet compared to open adrenalectomy [ 22 ]  . 
however , some patients complained about intolerable shoulder pain caused by carbon dioxide insufflation and wound pain caused by multiple trocar insertions of abdominal wall after la [ 23 ]  . 
the possible discomfort after this scarless technique may be the single cool - tip radiofrequency needle puncture papain during and after the ablation procedure is categorized in the side effect according to the guidelines for the standardization of terminology and reporting strategies of imaging - guided ablation [ 24 ]  . 
the vas is the most frequently used tool as the outcome measure in clinical research , which usually consists of a 10 - cm line anchored at one end by a label such as no pain and at the other end by a label such as the worst pain imaginable . 
 [ 26 ] had used a vas to evaluate the factors related to 1 3 radiol med ( 2016 ) 121 : 811819 intra - procedure and post - procedure pain during percutaneous rfa of hepatocellular carcinomas . 
for adrenal tumors , an electrode tip temperature exceeding 50 c with a treatment time of approximately 810 min was considered sufficient for tumor necrosis , which is a widely accepted procedure [ 29 ]  . 
previous reports [ 4 , 5 , 9 , 11 , 15 , 16 ] demonstrate the treatment efficacy and safety of adrenal lesion with relatively low ( 1.8 % ) major complications needing further intervention , which includes one required pneumothorax chest tube insertion and one mi . 
we believe that small size apa may be successfully ablated with a shorter time interval to minimize the risk of the procedure . the therapeutic effect of rf treatment was significantly dependent on tumor size . 
 [ 14 ] treated liver metastasis with rfa , and their results disclosed 33 of the 38 lesions 3 cm in greatest dimension to have undergone complete ablation , only 8 of 15 lesions > 3 cm had a complete tumor response . 
 [ 30 ] reported percutaneous rfa of adrenal tumor ( size 1234 mm ) in 11 patients with conn syndrome or cushing syndrome resulting in not only short hospital stay and low complication rate but also normalization of hormone secretion , improvement in bp , and reduced need for antihypertensive drugs . 
 besides the ablation procedure risk , some reports argued that hypertension , hypokalemia , and excessive secretion of aldosterone may associate with the increased risk of cardiovascular events and renal toxicity [ 3133 ]  . 
regarding the normalization ability , these two groups disclosed equivalent therapeutic effects without statistical difference , which makes rfa treatment for apa more promising . despite the effectiveness of rfa , we cannot neglect hypertensive crisis as a major possible complication during the procedure [ 6 , 34 ]  . 
catecholamines may be released into the systemic circulation via the adrenal vein when the normal adjacent adrenal gland encounters heat stimulus causing cell death and cytolysis [ 35 , 36 ]  . 
some researchers [ 12 , 29 , 37 ] advise premedication with and - blockers before rfa to prevent htn crisis , but these have not been routinely prescribed except for pheochromocytoma . 
 [ 36 ] mentioned the possibility of balloon occlusion to the adrenal vein during adrenal rf ablation ; however , it is currently impractical due to the small size of the vein and its variable anatomic location . some limitations to our study need to be mentioned . 
lastly , inaccessible nodule near greater vessels may preclude the safety of rfa as it reduces the external generalization of rfa . conclusion ct - guided rfa could be an effective and safe method for treating small adrenal apa . 
the nodules were in right lung in 123 patients ( 49 % ) , in left lung in 126 patients ( 51 % ) , the upper , lower and middle lobe localizations were , respectively in 122 ( 49 % ) , 100 ( 40 % ) and 17 ( 6 % ) patients . 
gemelli hospital - catholic university , rome , italy 3 unit of clinical and molecular epidemiology , irccs san raffaele pisana , rome , italy 4 department of thoracic surgery , catholic university of sacred heart , largo f . 
in particular , ct - guided transthoracic fine - needle ago - biopsy ( fnab ) is a well - established method in the cytologic or histologic diagnosis [ 1 ]  . it is useful both in case of advanced cancer and in case of suspected lung cancer suitable for surgery , investing a pivotal role to plain surgical or medical treatment [ 2 ]  . although overall sensitivity , specificity , and accuracy are over 95 % in the literature , in some cases diagnosis is not certain and it is hard to obtain by ct - guidedfnab [ 3 , 4 ]  . pneumothorax is the most common complication of ctguidedfnab , and it occurs in 1726.6 % of patients , with a chest tube insertion rate ranging from 1 to 14.2 % of patients [ 5 ]  . 
we also analyzed patient and nodule risk factor for its appearance . objectives of this work are : identify nodule characteristics favorable for diagnosis by fnab ; 1 3 636 fig . 
a axial mip image , needle in thoracic wall ; b axial mip image , correct attempt ; c same attempt of b , sagittal mip image radiol med ( 2016 ) 121 : 635643 identify patients characteristics which increase the risk of pneumothorax and other complications ; identify the best way to obtain a diagnosis in solitary lung nodules with the minimum risk of complications . materials and methods data from 249 patients who underwent fnab in our operative unit from january 2010 to december 2012 were analyzed retrospectively in this observational study . 
chronic obstructive pulmonary disease ( copd ) was present in 30 patients ( 12 % ) and in particular , 6 patients were affected by middle grade emphysema ( 2 % )  . nodules were located in the right lung in 123 patients ( 49 % ) and in left lung in 126 patients ( 51 % ) , with upper , lower and middle lobe localization in 122 ( 49 % ) , 100 ( 40 % ) and 17 ( 6 % ) patients , respectively . 
the number of retries ranged from 1 to 12 , depending on difficulty to reach the lesion , with an average of 2.57 ( table 1 )  . the biopsy was made when , after scan control , the needles tip was located between the outer third and the geometric center of the lesion . 
in lesions with necrotic component , the levy was made once the tip of the needle was found to be located in the portions of the lesion with solid density values . after biopsy , taken sample was placed on a glass slide , and fixed with solution , and subsequently sent to cytological analysis . 
all these procedures were made by the radiologist and the specialized nurse after a training with the pathologist . all the procedures were made by an interventional radiologist with more than 10 years of experience in ct - guided procedures . statistical analysis the sample characteristics were summarised in table 2 as absolute and relative frequencies for categorical variables , standard deviations for continuous variaand as means bles . 
 the students t test was applied to continuous variable , with correction for unequal variances when required , and the pearsons chi - squared test ( or the fishers exact test for expected cell frequencies less than 5 ) , for categorical variables ( p values not reported )  . 
for each outcome , simple logistic regression analysis was carried out to estimate the pure effect of all factors ; subsequently , multiple logistic regression analysis was implemented to identify predictors of all outcomes and to obtain adjusted estimates of effect . 
according to a forward selection procedure , after adjusting for tumor dimension , all other potential predictors were fitted into the model one at a time , but none was found to be a statistically significant predictor of ct - guided fnab positive results . 
the model fitting tumor dimension as the solely explicative parameter correctly classifies 65 % of observations , and has a sensitivity of 81 % , a specificity of 40 % , and an area under the roc of 63 % . 
the model fitting pleural passages as the solely explicative parameter correctly classifies more than 75 % of observations , with a specificity of 100 % and an area under the roc of 66 % . 
all results from the multiple regression analysis are shown in table 4 . radiol med ( 2016 ) 121 : 635643 discussion in last 30 years , several different techniques to typing lung lesions have been developed , ranging from endoscopic techniques to chest biopsy . in particular , percutaneous transthoracic needle biopsy is possible using fluoroscopic or ultrasonographic guidance , computed tomography and ct - fluoroscopy guidance , with good results in terms of accuracy , specificity and sensibility [ 6 ]  . 
in particular , we described the presence of colliquative necrosis when it was present in more than 50 % of the nodule volume . we did not find any other factors determining the diagnosis rate , either analyzing our technique variables such as needle diameter , number of passage , etc . 
we are in agreement with kucuk et al . , affirming that multiple passages are not necessary to obtain a diagnosis [ 13 ] , even if other works have reported an increase in accuracy if the number of passage is 3 or more [ 14 , 15 ]  . 
2 a assial direction of the needle , b biopsy , c small pneumothorax after procedure , d chest x - ray control after 3 h showed increase of the pneumothorax radiol med ( 2016 ) 121 : 635643 the method , so also using multiplanar reconstruction could help a precise needle introduction and obtain diagnosis in less passages [ 16 ]  . experience , we have noticed that by increasing the number of pleural passages , we increase only the risk of complications and not the diagnostic rate . the perilesion hemorrhage rate was of 5 % , while pneumothorax rate was of 25 % , with chest tube insertion in only 25 % of this group . 
we did not find a relationship between hemorrhage and pneumothorax , as authors like de filippo [ 17 ] and nour - eldin [ 18 ] did , reporting a less incidence of pneumothorax in presence of hemorrhage . 
theoretically , the question is open for every patient , because it is difficult to raise the equilibrium between the number of attempts and the diagnostic outcome , and in our another point of interest is the location of the lesion . 
however , in our experience , the distance between the nodule and the chest wall did not influence the pneumothorax occurrence . in fact , fnab operator had many difficulties to raise nodule in the apex or covered by the scapula , and in this case , many attempts were made , increasing the risk of complications . 
mean effective radiation dose and subjective and objective ( noise or n , signal to noise ratio or snr , contrast to noise ratio or cnr ) image quality , were evaluated . 
concerns over radiation risks of ccta prompted the ct scanner manufacturers to develop several techniques to lower the radiation exposure , such as ecgbased tube current modulation , prospective ecg gating , noise reduction filters , automatic exposure control systems , low tube voltage protocols and iterative methods of image reconstruction ( asir , mbir , iris , aidr , idose ) [ 3 ]  . 
several studies showed that a low tube voltage protocol allows to lower mean radiation dose keeping diagnostic image quality . although , to the best of our knowledge , there is no study relating the effects of a low tube voltage protocol with the 1 3 radiol med ( 2016 ) 121 : 618625 effective radiation dose and the image quality using an automatic exposure control systein this regard , the main purpose of this study is to evaluate the impact of a 100 kv tube voltage protocol on image quality and radiation dose and compare them with a 120 kv tube voltage setting . materials and methods patients in this active control trial , a total of 550 subjects , referred for coronary - ct angiography ( ccta ) at san salvatore hospital of laquila , were scanned with 320 - row ct scanner ( aquilion one , toshiba medical systems )  . 
exclusion criteria were : poor kidney function ( serum creatinine > 1.5 mg / dl ) , prior coronary artery surgery , coronary stents , heart rate ( hrs ) > 65 beats per minute ( bpm ) after beta - blocker treatment . 
in both groups tube current ( ma ) was adjusted by an automatic exposure control system ( sure exposure 3d ) and images were reconstructed by the adaptive iterative algorithm ( aidr - 3d )  . 
written informed consent before ct scan was obtained from all individual participants and the study was approved by the san salvatore hospital irb . acquisition protocol all ct scans were performed using a 320 row ct scanner . 
sixty milliliteres of nonionic contrast medium ( visipaque 320 ; ge healthcare srl , milan , italy ) was injected into the antecubital vein at a rate of 6 ml / s , followed by 40 ml of saline solution at the same flow rate . 
sureexposure ( toshiba medical , tokyo , japan ) , the aec systems that we employed , supplies both patient - size and z - axis aec [ 3 , 6 ]  . 
 in this study , we employed one of the latest iterative reconstruction system , the aidr - 3d , which operates in both the raw data and the image doma the aidr - 3d performs an automatic weighted combination between an original fbp image and an image obtained from the iterative process . 
in the process of setting the ma , the aec system considers the aidr - 3d which is incorporated in the current modulation systethe target noise value ( expressed as sd , standard deviation ) was set as 33 ( sd33 )  . 
for each patient , the system ( phasexact ; toshiba medical systems corporation , tochigi , japan ) traced a movement diagram of the sinogram and automatically selected the phase with the least movement artifact . 
the maximal number of reconstructed slices was 640 with 0.3 mm thickness and 0.25 mm interval by the means of the proprietary double slice technique and cone - beam reconstruction algorithm ( conexact ; toshiba medical systems , tochiki - ken , japan )  . subjective image quality analysis subjective assessment of images quality was performed by two experienced cardiac radiologists ( edc and ag ) , who were blinded to details of ct datasets . 
each radiologist rated the subjective quality of all evaluable coronary artery segments using a 5 - point scoring system graded as follow : 4 ( excellent ) excellent wall delineation and opacification of the artery lumen , 1 3 620 radiol med ( 2016 ) 121 : 618625 fig . 
measurement of signal within rois in the middle part of both left main coronary artery ( b ) and right coronary artery ( c ) without movement artifacts and noise - associated blurring ; 3 ( very good ) very good wall delineation and opacification of the artery lumen , with minimal movement artifacts good wall delineation and and image noise ; 2 ( good ) opacification of the artery lumen , with moderate movement artifacts and image noise ; 1 ( adequate ) severely impaired wall delineation and opacification of the artery lumen , because of severe movement artifacts and / or image noise ; 0 ( non - diagnostic ) poor artery wall delineation ( because of severe movement artifact and / or marked image noiseassociated blurring ) and lack of vessel attenuation [ 5 , 810 ]  . 
the radiologists analyzed internal and external wall delineation , the grade of motion - related artifacts , the differentiation between artery lumen and plaque ( calcified and non calcified ) [ 5 ]  . 
nevertheless , the end evaluation was an assessment of the general appearance of the artery and the probability of getting a confident diagnosis . objective image quality assessment objective image quality assessment of the proximal coronary arteries was performed by two experienced cardiac radiologists ( xx and yy ) , who , as previously indicated , assessed noise ( n ) , ct density ( hu ) , signal to noise ratio ( snr ) and contrast to noise ratio ( cnr ) [ 5 , 8 , 11 ]  . 
 56 patients were excluded because of prior coronary artery surgery ( coronary artery by - pass graft ) , 31 patients because of a heart rate ( hrs ) > 65 beats per minute ( bpm ) after betablocker treatment and 193 subjects because they did not have overlapping propensity scores . in table 1 demographic and clinical features of the study population were given . 
there were no significant differences between the two groups regarding age , cardiovascular risk factors , clinical presentations , hr , scanning range and length ( 13.524 cm in 100 kv group and 13.39 cm in 120 kv group )  . 
in the 120 kv group , 40 patients ( 29.6 % ) did not have significant stenosis , 47 ( 34.8 % ) had onevessel disease , 27 ( 20 % ) had twovessel disease and 21 ( 15.6 % ) had three - vessel disease . 
interobserver agreement of subjective image quality was deemed as very good for both groups ( k 0.88 for the 100 kv group and 0.86 for the 120 kv group )  . 
 at the level of rca , a 1.83 ( 95 % ci of mean difference 1.31 ) mean snr increment and a 2.1 ( 95 % ci of mean difference 1.34 ) mean cnr incre2.86 to ment ( table 3 ) was observed . 
nevertheless , low tube voltage is inevitably accompanied by an increase in image noise and , thus , its use is advisable only for patients with a bmi ( body mass index ) lower than 2530 [ 1820 ]  . 
 [ 21 ] who selected the tube voltage ( kv ) and current ( ma ) not only on the basis of patients bmi but also according to clinical indications , patients body shape and , above all , chest wall attenuation . 
this was performed by both visual examination of the patient prior the scan and by evaluation of the coronal scout image and axial test - bolus image ( obtained before the scan ) [ 21 ]  . 
however , as concluded by these authors , this approach is not completely realistic in the clinical routine due to its subjective nature and because it is not always possible to have a physician experienced in cardiac imaging technique at every scan . 
the range in tube current is narrow ( 50500 ma ) and , thus , when the patient attenuation profile requires more than 500 ma , the system increases also the tube voltage to avoid underexposure . 
the system also works in the same way when the patient attenuation profile requires less than 50 ma and , in this case , reduces the tube voltage to avoid overexposure . 
our study , performed with a 320 - detector ct scanner , evaluated the effects , on radiation exposure and image quality , of a 100kv protocol in comparison with a conventional 120 kv protocol demonstrating that 1 3 radiol med ( 2016 ) 121 : 618625 fig . 
2 coronary computed tomography angiography ( ccta ) images obtained with an aec ( automatic exposure control ) system and , respectively , a 120 kv tube voltage protocol ( a , b , c ) and a 100 kv tube voltage setting ( d , e , f )  . 
ccta images obtained with a 120 kv tube voltage setting show a ct density of 442 hu and a noise of 30.7 , while ccta images acquired with a 100 kv tube voltage protocol present a ct density of 617.7hu and a noise of 31.6. 
 mean effective dose was similar between the two subjects : 2.9 msv in the 120 kv protocol and 2.8 msv in the 100 kv setting a 100 kv protocol , in association with aec , significantly improves the image quality without reducing the radiation exposure . 
subjective image quality analysis showed that the rate of non - diagnostic segments was significantly higher in the 120 kv group although this figure did not parallel with the percentage of subjects with at least one non - diagnostic segment . 
to the best of our knowledge , only one previous study [ 18 ] evaluated the effects , on radiation exposure and image quality , of a 100kv protocol in comparison with a conventional 120 kv protocol . 
our data may seem to be in contradiction with zhangs results [ 18 ] but this discrepancy may be explained by a number of different parameters included in our study . 
in his study , zhang [ 19 ] used a 100 kv protocol only in subjects with bmi < 25 , while using a 120 kv protocol for overweight patients . 
these results can be explained by the fact that a lower tube voltage translates into lower effective photon energy ( effective photon energy is approximately one half of the kv ) and , when the effective photon energy is closer to the k - edge of iodine ( 33.2 kev ) , ct attenuation increases [ 21 ]  . 
without the use of an automatic 1 3 624 radiol med ( 2016 ) 121 : 618625 exposure control system , a low tube voltage protocol is inevitably accompanied by an increase in image noise , and , thus , without a careful selection of eligible patients , it leads to a lower image quality , which could compromise the diagnostic quality of the images . 
we would like to evaluate , in the future , image quality and radiation exposure of protocol with higher level of acceptable image noise to identify the noise level , which offers the best compromise between image quality and radiation exposure . 
as demonstrated in previous study [ 2224 ] , the contrast material has to produce a high intra - coronary attenuation , that allows more reliable visualization of coronary arteries . 
 [ 24 ] , which recently demonstrated that different iodinated cm have an analogous impact on plaque attenuation profile ( in terms of snr and cnr ) depending on the iodine load , we employed low concentration cm ( 320 mgi / ml ) with high flow - rate of 6 ml / s and , consequently , high iodine load ( idr 1.920 gi / s ) in both protocols . 
a focal point of our study is the use of a propensity analysis , which helped us to obtain two groups of subjects virtually randomized for main clinical characteristics and made the results less prone to methodological biases in comparison with other usual statistical methods . 
in our opinion , the latter is the main limitation because we did not assess the diagnostic accuracy of a 100 kv protocol in the evaluation of calcified plaque , as the severity of calcified plaque is the most likely to be overestimated using a 100 kv protocol considering that , theoretically , a low voltage setting may increase blooming artifacts [ 25 , 26 ]  . 
nevertheless , unlike zhang [ 19 ] , we did not report a higher number of unassessable segments due to calcification in 100 kv group than in 120 kv one . conclusion our study shows that , using a 320 row ccta with aec , it is preferable to use a 100 kv tube voltage setting because compared to 120 kv tube voltage protocol , it seems to significantly improve subjective and objective image quality , without significantly lowering the mean effective radiation dose . 
our aim was to evaluate whether these risk factors should prompt skin testing for diagnosing cm allergy . methods the study was conducted among patients referred for allergy testing with cm . 
after completion of tests patients were telephonically queried on their symptoms of reactions . results 151 risk patients ( 53 men , 98 women ; mean age 55.2 ) were included in the study . 
maltepe , istanbul , turkey 2 department of pulmonology , sreyyapasa chest diseases and thoracic surgery training and research hospital , istanbul , turkey 3 department of immunology and allergy , istanbul medical faculty , istanbul university , istanbul , turkey be beneficial in patients with a history of cm allergy and cannot be recommended for patients with well - controlled asthma , rhinitis , atopic dermatitis or history of drug allergy . keywords contrast media allergy radiocontrast media skin prick test intradermal test introduction with the evolution of iodinated contrast media ( cm ) from ionic , high - osmolality to non - ionic , low - osmolality , the incidence of hypersensitivity reactions to cm used for computed tomography ( ct ) and angiography has decreased . 
hypersensitivity reactions to cm may be due to ( 1 ) a direct membrane effect related to the osmolality or chemical structure of the cm ( pseudoallergy ) ; ( 2 ) an activation of the complement system ; ( 3 ) direct bradykinin formation ; or ( 4 ) an ige - mediated mechanism [ 5 , 6 ]  . 
current evidence suggests that a subset of immediate reactions is likely mediated by ige and most non - immediate skin reactions are most likely caused by t cells [ 79 ]  . the most common risk factor for hypersensitivity reactions to cm is a previous reaction . 
atopy , history of drug allergy , atopic disease , 1 3 radiol med ( 2016 ) 121 : 660666 age between 20 and 29 years or more than 55 years may also increase the risk of cm hypersensitivity reactions [ 12 19 ]  . 
in addition , the presence of cardiovascular disease ( cvd ) and asthma is associated with a more serious reaction [ 18 , 20 ]  . researchers tried to predict cm - induced hypersensitivity reactions by injecting a small amount of cm intravenously before the formal injection . 
currently hypersensitivity to cm can be tested with skin prick tests ( spts ) , intradermal tests ( idts ) , patch tests ( pts ) , and provocation tests according to the type of reactions [ 9 , 22 , 23 ]  . 
in a study in which the exact cm agent causing the reaction was known , undiluted cm for idt was used and showed that the sensitivity of skin tests reached up to 64.7 % [ 26 ]  . 
these are post - event diagnostic skin tests ; however , we still have insufficient evidence that these tests have sufficient value in reducing the risk of hypersensitivity reactions to cms in patients with allergy histories other than cm allergy . 
 our aim was to evaluate whether these factors indicate an increased risk of developing allergic reactions to cms , whether testing for these factors is required , and the diagnostic value of performing skin tests with cms . materials and methods patients this study was conducted on patients referred to our immunology and allergy department by physicians for testing for cm allergy due to a history of adverse reactions to drugs ( who gave a reliable history of urticaria / angioedema , nasoocular symptoms , bronchospasm after ingesting drugs ) cvd , beta blocker use , atopy , atopic disease , or advanced age . 
the participants were evaluated using a standard questionnaire for the following : demographic data , history of atopic disease , previous exposure to cm , history of reaction with cm , severity reactions with cm , latent period from administration to reaction , time interval between reaction and testing , use of beta blockers , cvds and adverse reactions with nsaids or antibiotics . 
the total ige levels and eosinophil count were analyzed for each patient . immediate cm allergic reactions were assessed using the ring and messmer scale for estimating the severity of reaction : [ 27 ] grade 1 ( generalized cutaneous and / or mucocutaneous symptoms ) , grade 2 ( mild systemic reactions ) , grade 3 ( life - threatening systemic reactions ) , or grade 4 ( cardiac and / or respiratory arrest )  . 
non - immediate reactions were graded using the scales suggested by the european network of drug allergy ( enda ) [ 28 ] and european academy of allergy and clinical immunology ( eaaci ) interest group on drug hypersensitivity : [ 10 ] mild when no treatment was required ; moderate when the patient responded readily to appropriate treatment and no hospitalization was needed ; and severe when the reaction required hospitalization or was life - threatening . lung function tests were performed in patients with symptoms of airflow limitation or asthma , such as episodic breathlessness , wheezing , cough , and chest tightness after exercise , exposure to airborne allergens or pollutants . 
 management of asthma was based on the assessment of disease control as stated by the global initiative for asthma ( gina ) guidelines [ 29 ]  . atopy was defined as a positive skin prick test ( spt ) to at least one of the aeroallergens and nutritive allergens ( solupricksq , alk - abello a / s , hrsholm , denmark )  . 
a 1 - mm tip disposable lancet was used to puncture the skin , and a mean wheal diameter of 3 mm or greater than the control solution was considered positive . 
this study was approved by the hospital ethics committee . protocol spt was performed on the volar forearm with non - ionic cm ( iohexol , iopromide , iomeprol , iobitridol , ioversol ) , or gadolinium cm ( gadodiamide , gadoterate meglumine , gadobenate dimeglumine , gadoversetamide , gadobutrol ) 1 3 662 radiol med ( 2016 ) 121 : 660666 table 1 baseline characteristics of the study participants recommended by a radiologist . 
it was considered positive if the size of the initial wheal increased by 3 mm or more in diameter after 20 m in patients with a history of any adverse drug reactions , tests were made 36 months after the last reaction . 
in a patient with a history of hypersensitivity reaction to a cm , the drug which caused the previous reaction was not re - administered and the idt was performed with 1 : 1000 diluted cm . 
even though the tests were negative in patients with a history of cm hypersensitivity reactions , a premedication protocol was used with 40 mg of methylprednisolone administered 13 , 7 , and 1 h before injecting cm , and 45.5 mg / 2 ml of pheniramine maleate administered 1 h before the injection [ 12 ]  . 
in patients with a history of maculopapular reactions after administration of cm , a graded provocation test was performed depending on the time course of the primary reaction ( e.g. , one - tenth of the full dose on day 1 , one half of the dose on day 2 , and the full dose on day 3 )  . 
sixty - three patients ( 41.7 % ) had asthma , 20 ( 13.2 % ) had rhinosinusitis , 6 had atopic dermatitis ( 4 % ) , and 17 had chronic urticaria ( 11 % )  . 
according to the patients , 29 ( 19.2 % ) had suffered a reaction to nsaids and 74 ( 49 % ) had suffered a reaction to antibiotics ( mostly penicillin )  . 
ten patients had immediate reactions ( grade i : 4 ; grade ii : 5 ; and grade iii : 1 ) .three patients had non - immediate reactions ; one had a severe maculopapular eruption after 24 h , and two had moderate urticaria after 610 h . 
the statistical package for social sciences ( spss ) for windows version 14.0 ( chicago , il , usa ) was used to analyze the data . results all of the tests for cm allergy were negative or non - ionic cm ( 28 iopromide , 68 iohexol , 3 iomeprol , 1 ioversol , 1 iobitridol ) and gadolinium cm ( 9 gadoterate meglumine , 10 gadobenate dimeglumine , 8 gadoversetamide , 22 gadodiamide , 1 gadobutrol )  . 
the result of the provocation test was negative . after the tests patients were asked about their symptoms over the telephone : eleven patients ( 7.2 % ) could not be reached and four gave up the process ( ct , angiography or mr imaging ) required for cm . 
only one patient reported urticaria within 12 min after administration of cm , and another had shortness of breath , dizziness , and a burning sensation in the throat after 12 mfor these two patients , the tests were repeated after 6 weeks with iopromide and gadodiamide , which caused the initial reaction , and other alternatives ( first with iohexol , iomeprol , ioversol , iobitridol ; second with gadoterate meglumine , gadobenate dimeglumine , gadoversetamide , gadobutrol )  . 
further provocation tests were refused by the patient . the risk factors for cm allergy ( only age , sex and atopy ; because of small number of patients ) in those ( tested , phoned , contacted and cm administered ; n 134 ) with and without a history of cm allergy are shown in table 3 . nevertheless , the sensitivity of the skin tests for cm hypersensitivity was not clear because those cases with a history of cm allergy ( 13 patients ) were offered a standard premedication protocol . 
among those patients who were contacted by telephone , who were administered cm and who did not have a history of cm allergy ( total of 121 patients ) , one ( 0.8 % ) of them developed a reaction , although tests were negative before and after the reaction . discussion testing for cm allergy in this study showed negative results , which suggests that cm allergy testing is unjustified in patients with the aforementioned risk factors . 
in comparison , our study had fewer patients but all of them had at least one risk factor for cm allergy , e.g. , 63 patients had asthma , 20 had a . 
in our study of the 13 patients with a history of cm allergy most of the reactions were mild ( only one patient grade iii immediate ; one patient severe non - immediate ) , and the tests were negative . 
in addition because the time interval between the reaction and the test was more than 6 months , there was an increased likelihood for the test to be negative and only three patients were aware of the exact drug that caused the reaction . 
only in one patient ( grade 1 ) who did not have a history of cm allergy but reacted , skin tests on the drug in question , and four alternatives , were negative . 
 depending on the cross reactions between non - ionic cms , positive alternative tests are described to be positive up to 41.7 % in the study conducted by ahn et al . 
but in our study some of the patients history was almost 1020 years ago , and reactions history may have been due to ionic cms rather than non - ionic cms , probably so cross reaction can not be occurred . 
overall , it appears that skin tests for cm allergy are inefficient , unnecessary , and time - consuming in patients with risk factors , or those with a history of mild reactions with cms . when we compare patients who had a history of cm allergy with the other patients , those with a history of cm allergy had higher rates of atopy . 
our study supports the findings from previous studies that atopy is associated with an increased risk of hypersensitivity reactions to cm [ 14 , 15 , 17 , 18 ]  . 
this is in contrast with other studies that showed that cm hypersensitivity reactions were most common in the age of 2029 [ 14 , 15 ]  . premedication is recommended in patients with a history of adverse reactions to cm . 
 [ 33 ] who showed that prophylactic therapy should beprescribed according to degree of asthma control as assessed by clinical / functional parameters and in well - controlled asthmatics no premedication is required . 
premedia is not recommended in asthmatics prior to injection of cm ( grade c ) but for uncontrolled asthma , if possible delaying the injection is recommended ( expert opinion ) [ 34 ]  . 
also we did not premedicate allergies 1 3 radiol med ( 2016 ) 121 : 660666 requiring treatment ; only one patient with chronic urticaria experienced a non - severe reaction , which suggests that premedication should not be performed in patients with atopic diseases such as well controlled asthma , allergic rhinitis , or atopic dermatitis and history of drug allergy . previous studies have shown that premedication could prevent only hypersensitivity reactions with ionic cm , but could not reduce the risk of hypersensitivity reactions with non - ionic cm [ 12 ]  . 
however , a recent study , based on 30 patients , premedicated patients with a history of an immediate hypersensitivity reaction with non - ionic cm and only five had reactions in spite of premedication ( breakthrough reactions ) [ 35 ]  . 
in our study , none of the 13 patients with cm allergy history had symptoms of breakthrough reactions , after non - ionic cm was administered with suggested premedication protocol . conclusion atopy is associated with an increased risk of cm allergy . 
this article is published with open access at springerlink.com abstract purpose to assess how frequently foci are identified on mri in high - risk patients , and their association with malignancy , breast density , and background parenchymal enhancement ( bpe )  . materials and methods in this multicentric study , two readers , in consensus , retrospectively reviewed screening breast mri of 245 high - risk women , performed between 2009 and 2014 . 
eligible patients had at least two consecutive screening mri , and a follow - up of at least 1 year after a lesion was first detected ; histology was available for all suspicious findings . 
chi - square test was used to define significant correlations . results 166 women ( mean age 43 years ) , who underwent a median of 4 mri ( range 26 ) during the study period , were included . 
during follow - up , two foci increased in size ( 2.9 % , 95 % ci 0.810.1 % ) and at biopsy , a cancer was found ( 1 high - grade ductal carcinoma in situ , 1 tubular carcinoma )  . 
ripamonti 435 , 20141 milan , italy 4 radiology department , apss - trento , via degasperi 79 , 38123 trento , italy 5 division of cancer prevention and genetics , european institute of oncology , via g . 
this increased risk is related to several factors , the more relevant being : the presence of a gene mutation ( brca 1 and brca 2 being the more common ) , family history of breast or ovarian cancer ( the first - degree relatives , with an early onset of the disease ) [ 1 , 2 ]  . 
malignant lesions found in these women are characterized by an early onset and by a high proliferation rate , thus being often more aggressive , as compared to the cancer usually diagnosed in the general population [ 3 , 4 ]  . in consideration of this evidence , various dedicated screening programs have been developed to allow early diagnosis in high - risk patients . 
these programs start at a young age , usually 30 years old or as soon as the risk factor 1 3 612 radiol med ( 2016 ) 121 : 611617 is found . 
along with the traditional imaging modalities , such as mammography and ultrasound , breast magnetic resonance imaging ( mri ) plays a central role [ 1 , 5 ]  . 
breast mri has the highest sensitivity in breast cancer detection [ 6 ] ; several multicentric studies proved that mri , compared to mammography and ultrasound , is able to identify a higher number of cancers and at an earlier stage [ 710 ]  . mri is also able to detect very small enhancing lesions , with 5 mm or lower maximum diameter , which might be difficult to further characterize . 
per definition , foci cannot be accurately assessed with respect to margin or internal enhancement : if these characteristics can be assessed , the finding should be considered a small mass [ 11 ]  . 
foci are frequently associated with an increased hormonal stimulation , and they can sometimes be seen when a benign lesion is present ( fibroadenoma , cyst and fibrocystic changes , lymph node ) , but they can also represent the early onset of a malignant lesion [ 12 , 13 ]  . 
studies addressing the malignancy rate of foci found in the general population showed highly variable results , with percentages ranging from 0.6 to 23 % [ 12 , 14 ]  . 
despite this , not many studies addressed the frequency of foci detected during screening mri in high - risk patients and the malignancy rate of foci in this population . the aim of our study was to determine how frequently foci are identified on breast mri in high - risk patients , and how frequently foci are found to be malignant . 
we further correlated the presence of foci and malignancy with breast density and background parenchymal enhancement . materials and methods patients collection this retrospective study involved two institutes , both with dedicated breast units . 
in both institutions , women with family history of breast and ovarian cancer ( more than one close relative , at a young age ) are sent to genetic counselling . 
the risk and the likelihood of detecting a pathogenic gene change are calculated using a standard risk assessment modality ( such as cagene ) , and when deemed necessary , the patient undergoes genetic testing . screening is performed with annual breast mri and ultrasound ; digital mammography is performed annually in women older than 35 years . 
all breast mris performed for screening in high - risk women between january 2009 and october 2014 were reviewed . patients were included in this retrospective analysis when : at least two rounds of mri screening were available ; at least 1 year follow - up was available after a focus was detected for the first time ; histological verification or follow - up of at least 1 year for all findings classified as birads 3 or higher was available . 
cases that did not meet the inclusion criteria , incomplete mri examinations , cases with previous bilateral mastectomy , and cases for which information about risk factors was not available , were excluded . the high - risk databases of the two institutions were reviewed to collect data on gene mutation and family history for the included patients . 
the standard protocol used for the clinical evaluation consisted of an axial short - tau inversion recovery ( stir ) t2 - weighted sequence and an axial spoiled gradient - echo 3d ( flash ) t1 - weighted sequence acquired before and five times after the injection of contrast material for the dynamic study ( gadobenate dimeglumine , multihance , bracco ; 0.01 mmol / kg of body weight , injected at the rate of 2 ml / s , followed by a flush of 20 ml of saline solution )  . 
1 a small focus was detected in the central area of the left breast in a screening mri performed in a 46 - year - old woman ( a , arrow )  . 
histology showed a high - grade ductal carcinoma in situ ( screening ) , but they were blinded to the number and type of lesions present in the data set . performed using the statistical software commercially available ( medcalc software v.20 , ostend , belgium )  . for each mri examination , readers had to evaluate presence or absence or foci . 
the bi - rads definition of a focus was strictly followed [ 11 ] , and lesions that could be further characterized by evaluating preand post - contrast t1w sequences , t2w sequences , or dwi were not considered , even when presenting a diameter equal or lower to 5 mm ( i.e. , cysts , small spiculated masses , and lymph nodes )  . 
for all detected foci , readers had to state whether in the subsequent examinations , the lesion was disappearing , reducing in size , stable , increasing in size , or showed any change in morphology suggesting malignancy . 
number of foci per patient was also considered . breast density was evaluated on pre - contrast t1w sequences and classified according to the bi - rads lexicon : ( a ) almost entirely fat ; ( b ) scattered fibroglandular tissue ; ( c ) heterogeneous fibroglandular tissue ; and ( d ) extreme fibroglandular tissue . 
pattern of background parenchymal enhancement ( bpe ) was defined on the post - contrast study , according to the bi - rads lexicon : ( a ) minimal ; ( b ) mild ; ( c ) moderate ; and ( d ) marked . statistical analysis overall number of newly appearing foci was calculated . 
proportions are presented as percentages with 95 % confidence interval ( 95 % ci )  . the relation between presence of foci in patients with different breast densities or in mri with different bpes was evaluated using the chi - square test . finally , the presence of malignant lesions was compared in patients with or without foci , and considering breast density and bpe , using the chi - square test . 
nine foci disappeared during follow - up ( 13.2 % , 95 % ci 7.123.3 % ) , 1 or 2 years after the examinations where they were first detected . 
2 a small focus was detected in the retroareolar region of the left breast in a screening mri performed in a 62 - year - old woman ( a , arrow )  . 
histology showed a tubular carcinoma table 1 number of patients presenting with foci , number of foci , and cancer cases according to breast density distribution breast density patients with foci foci cancer cases single focus multiple foci n 7 ( 19.4 ) 13 ( 36.1 ) 19 ( 34.5 ) 11 ( 28.2 ) 0 ( 0.0 ) 1 ( 2.8 ) 2 ( 3.6 ) 5 ( 12.8 ) percentages are given in brackets follow - up . 
overall , 2 on 5 cancers detected during the study period ( 40 % ) were initially visible as foci , without any further suspicious characteristic . breast density distribution and distribution of foci and malignancy in the various density classes are shown in table 1 . 
of note , we obtained a malignancy rate well within the lower limits of the range presented in the literature for the general population [ 12 , 14 ]  . 
in some studies [ 14 , 21 , 22 ] , lesions visible on pre - contrast t1w or t2w sequences , and thus amenable of further characterization , were classified as foci on the basis of their maximum diameter . 
 [ 12 ] analysed a small group of high - risk patients and found a similar percentage of malignancy in their evaluation , also not different from the malignancy rate of the general population . management of foci is still a topic of discussion . 
 according to most of the literature , foci might represent cancer in more than 23 % of the cases , and thus in specific single cases , ( synchronous breast malignancy , patients decision ) biopsy should be considered [ 24 ]  . 
on the other hand , it is highly unlike that the decision to biopsy all foci would be cost - effective , as in most of the cases , biopsy can only be performed under mr - guidance and the majority of the lesions will turn out to be benign [ 17 , 24 ]  . 
the only sign on which various studies agree to define a focus as suspicious is the increase in size [ 24 ] ; thus , indication for biopsy should be given only when an increased focus is found . 
furthermore , modification in the appearance of the focus , related or not to a modification in size , should be considered suspicious and indicate the need for a biopsy . 
short - term follow - up could help in the earlier detection of lesions increasing in size but , on the other hand , a small increase might be undetected when performing a short - term evaluation . 
malignancy was more frequent in dense breasts , but no correlation with bpe was found . foci on breast mri can be associated with hormonal stimulation or with a wide variety of findings , being most often related to benign proliferative or non - proliferative changes of the breast , cysts , or small lymph nodes . 
rarely , they might represent an early sign of malignancy . foci were detected in a higher number of patients , as compared to other studies [ 14 , 16 ]  . 
this difference might have various explanations : high number of young patients with dense breast , thus with a higher hormonal stimulation , 1 3 616 radiol med ( 2016 ) 121 : 611617 several studies already showed the importance of breast density as a risk factor for breast cancer [ 26 ] , and these were also seen in our study . 
the relatively small number of cases included in our analysis might have limited this evaluation . our study has some limitations : though two centres were involved , the overall number of foci and cancer detected was not high and it is not possible to draw conclusions on management . 
 we believe that this result is mainly related to our case selection : some cancer cases were not included in the study , as not enough follow - up was available . 
 these patients were excluded as the modifications related to the therapy might have affected image interpretation . in conclusion , we found that foci are a relatively frequent finding in screening breast mri performed in highrisk women , but they are rarely related to malignancy . 
whether the best management of a newly detected focus is biopsy , short - term follow - up or 1 - year follow - up is still under discussion ; and further studies will be necessary to clarify this issue . acknowledgments open access funding provided by medical university of vienna . compliance with ethical standards the current study received no funding . conflict of interest all authors of this manuscript , p . 
zuiani declare that they have no conflict of interest . ethical standards all procedures performed were in accordance with the ethical standards of the institutional research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
members of italian society of medical radiology ( sirm ) were given 2 weeks to perform the survey . results a total of 1599 radiologists , corresponding to 17 % of all sirm radiologists , participated into the online * francesca coppola francesca.coppola@aosp.bo.it 1 radiology unit , department of diagnostic medicine and prevention , s . 
orsola malpighi hospital , 15 , albertoni street , 40138 bologna , italy 2 snr foundation , via farini 62 , 00185 rome , italy 3 radiology unit , department of medicine and surgery , magrassi - lanzara , second university of naples , naples , italy 4 medical physics unit , santorsola - malpighi hospital , bologna , italy 5 user co - chair ihe - italy , servizio di radiologia , misericordia hospital , azienda usl toscana sud est , grosseto , italy 6 monaldi hospital , via leonardo bianchi , 80131 naples , italy 7 department of translational research , university of pisa , uo radiodiagnostica 1 - aoup , edificio 30a , via paradisa 2 , 56124 pisa , italy 8 department of surgery science , university of torino , candiolo cancer institute , strada prov . 
as a result , 62 % of participants have a positive opinion on teleradiology , while 80 % including 18 % with a negative opinion believe that teleradiology will have a future . 
the majority of users adopt intramural teleradiology for coverage of emergencies ( 47 % ) , of night and weekend shifts ( 37 % ) or to even out distribution workload ( 33 % )  . 
in particular , they think that teleradiology is too impersonal ( 40 % ) , and that it is responsible for insufficient communication with the referring clinician ( 39 % )  . conclusions the majority of italian radiologists are favorable to teleradiology . 
however , they have concerns that teleradiology may further reduce communication with the referring clinician ad patient . keywords teleradiology italian survey insourcing outsourcing picture archiving communication systems introduction in the recent update of the white paper of the european society of radiology teleradiology ( tr ) is defined as the exchange of radiological images and patient - related data between geographically different locations for purposes of primary interpretation , expert consultation and / or clinical review by digital transmission [ 1 ]  . 
tr is part of a largest effort of the european community ( ec ) , with an aim of improving the quality of the health system and of reducing healthcare costs [ 2 ]  . 
implementation of high speed information technology ( it ) highways , the availability and low costs of large data storage facilities , and the diffusion of picture , archiving and communication systems ( pacs ) 1 3 radiol med ( 2016 ) 121 : 652659 is rapidly closing the technological gap and favoring the implementation of tr . 
according to the e - health benchmarking iii report of the european commission , pacs availability is highest in northern europe ( i.e. , > 95 % of health facilities have one ) while it is still scarcely distributed in some southern ec countries [ 3 ]  . shortage of radiologists and geographical concerns ( i.e. , large distances between healthcare facilities , low population density areas and adverse climatic conditions ) are the main drivers of tr demand . 
in many northern european countries , tr has become part of the regular workflow for purposes of workload balancing or to provide remote , offhour radiological coverage , for emergency readings and to a lesser extent for subspecialty readings [ 4 , 5 ]  . 
in the past decade , several national and international commercial tr providers have emerged in europe , facilitating the outsourcing of diagnostic readings [ 4 , 6 , 7 ]  . 
on the opposite , in southern european tr is still in its infancy possibly due to the technological gap , to the larger availability of radiologists in some countries and to the more restrictive legislation and guidelines [ 8 ]  . 
however , the market analysts are expecting a growing demand for non - invasive diagnostic imaging that could lead to an increased usage of tr in the coming years [ 1 , 2 ]  . according to a recent european survey , most radiologists look favorably at tr as it allows improved collaboration between peers , can be used to organize radiologists workload , thus improving the quality and efficiency of radiological services , especially , those of rural and underserved areas [ 2 , 9 ]  . 
in this context , italy stands out as the country with the second lowest number of inhabitants per radiologist and with one of the most careful and patient centered tr guidelines [ 8 ]  . in june 2014 , the italian society of medical radiology ( sirm ) promoted an online survey to gain information on the it infrastructure of healthcare facilities throughout its territory and on the current usage of tr . 
space was left below each question where participants could add their personal comments . the first set of questions was aimed at collecting information on the geographical location , age , institution and working position of radiologists . 
the second section included questions on the working environment of radiologists , i.e. , whether a pacs system was present in their institution , if digital signature was adopted , etc . 
radiologists were then asked to answer to a third set of questions , related to their experience with tr only if they were actually participating , in some form , to a tr project . 
each radiologist was sent a personal email from the president of the college of informatics by sirm with an invitation to participate into the survey , which was accessible through an email link . 
survey monkey statistical tools were used for the analysis of the quantitative data [ 11 ]  . results population characteristics one thousand five hundred ninety - nine of the 9662 members of the sirm ( 17 % ) participated into the survey . 
 thirty - one percent of participants where 5665 years old ; 26 % where 4656 years old ; 22 % where 3645 years old ; 17 % where 2535 years old . 
the majority of responders were from the northern italy ( 43 % ) ; central and southern italy followed with a response rate of 30 and 27 % , respectively . 
participants into the survey were either academic or directors of radiology units in 29 % of cases ; only 8 % were residents . teleradiology infrastructure two radiologists ( fc , dr ) created an online electronic survey using the survey monkey web - based tool [ 10 ]  . 
the first draft of the questionnaire was sent to a multidisciplinary eighty - nine percent of responders had a pacs available in their working environment ; no difference in pacs 1 3 654 statement table 1 recapitulated requirements that responders considered important for implementation of tr ( total number of responders 816 , multiple choices allowed ) radiol med ( 2016 ) 121 : 652659 responders that consider the statement important ( % ) 1 . 
patient clinical data and previous imaging studies should always be available for comparison 261 ( 32 % ) 225 ( 28 % ) 316 ( 39 % ) 160 ( 20 % ) 177 ( 22 % ) 482 ( 59 % ) 558 ( 68 % ) table 2 summarizes the usage of tr in italy ( total number of responders 896 , multiple choices allowed ) statement responders ( % ) 1 . 
tr is used to report examinations performed in the institution where i work ( remote management procedures 424 ( 47 % ) of intra - company deferrable urgent / emergency ) 2 . 
of the remaining , 737 ( 48 % ) adopted tr in - hospital on dedicated workstations , 137 ( 9 % ) worked from home and 92 ( 6 % ) on mobile devices ( note that multiple answers were allowed for this question )  . the large majority of users ( 75 % ) sent their report through a direct connection with the radiology information system ( ris )  . 
in reverse , patients clinical information was obtained with a direct connection with ris in 53 % of cases ; by phone in 27 % ; by fax in 8 % ; through a dedicated platform in 7 % , by e - mail in 4 % and by instantaneous messaging in the remaining 1 % . 
of the 874 responding radiologists ( 55 % ) that used tr in their clinical practice , the majority adopted an intra - mural solutionthey report examinations from a radiology unit located either within the same hospital or in a different hospital but of property of the same institutionfor emergency calls ( 47 % ) , for night and weekend coverage ( 37 % ) or to even out distribution workload ( 33 % )  . 
only 12 % of responders adopt an extra - mural option , i.e. , where the interpreting radiologist is working for another company , not affiliated to the institution that is providing the examinations [ 1 ]  . 
on the opposite , approximately half of responders send out request for a second opinion for the following reasons : neuroradiology consultancies ( 30 % ) ; examination of any kind if particularly complex ( 18 % ) , evaluation for interventional radiology procedures ( 8 % ) or for pediatric radiology examinations ( 5 % )  . perceived advantages , disadvantages and threats of teleradiology sixty - two percent of participants into the survey had a positive opinion on tr while 80 % including 18 % with a negative opinion , are convinced that tr will have a future . 
those already using tr have a better opinion of it ( 68 % ) with respect to radiologists that are not using tr in their clinical practice ( 53 % )  . 
radiologists working in private practices on average have a higher opinion of tr ( 72 % ) with respect to radiologists working in public institutions ( 59 % )  . 
academic radiologists and directors of radiology units were generally more positive on tr ( 70 % ) with respect to radiologists working in other positions ( 60 % )  . 
radiologists value most the possibility to discuss cases in a collaborative network to improve the efficiency of the radiological service and to reduce costs . approximately , half of radiologists participating into the survey use tr in their clinical practice , in the large majority of cases as an intra - mural solution . 
with this form of tr the presence of at least one radiologist must be guaranteed within the hospital facility ; health personnel must comply with the newly published italian guidelines [ 12 ]  . outsourcing is rare in italy ( table 2 ) [ 8 ] and is mainly adopted in private practice . 
second , italy has adopted the restrictive guidelines of the istituto superiore di sanit on the implementation of tr , which is allowed in outsourcing only for screening examinations such as mammography , as it requires double reading [ 8 ]  . 
italian guidelines allow routine intra - mural tr between different locations if these are within the same radiological unit and within the same hospital , or between radiology units or departments of the same institution . 
tr is allowed between different hospitals only for emergency studies if one of the facilities does not have radiologist on duty or on call due to the small number of performed examinations [ 8 ]  . 
it has been recently debated on whether technologist may be allowed to perform conventional radiograms without contrast media injection to outpatients with the prescription of the general practitioner , without the radiologist being present in the health facility to justify the examination and to obtain informed consent . 
finally , if supported by adequate it infrastructure , the prevailing opinion in this survey is that insourcing could actually bring about an improvement in communication between imaging doctor , patient and referring clinician . 
accordingly , the italian radiologist feels that the most important advantage of tr is the possibility of working in a collaborative network and contextually his major point of concern is that it is too impersonal and that the contact with the patient and referring clinician may be lost . 
indeed , the european society of radiology ( esr ) and the american college of radiologist acr white papers state that patients are the primary focus ; first and foremost , all tr relationships should be patient centred [ 18 , 21 , 22 ] and that the royal college of radiologists ( rcr ) similarly affirms that the optimum radiology service is one provided locally where radiologists can maintain a regular dialogue with both referrers and those acquiring the images , only in this model can patients benefit fully from the integration of imaging into the pathway of care [ 2325 ]  . 
italian radiologists seem to believe that the optimum radiology service is one provided locally where radiologists can maintain a regular dialogue with both referrers and those acquiring the images ; only in this model can patients benefit fully from the integration of imaging into the pathway of care . 
however , they also believe that there are circumstances in which tr can be beneficial , most significantly when seeking a specialist second or subspecialty expertise opinion or for peripheral disadvantaged areas or disaster . there is a significant methodological limitation to this study as only 17 % of radiologists of the sirm responded to the survey . 
 for this reason , it is not possible to affirm that the results 1 3 radiol med ( 2016 ) 121 : 652659 of this survey reflect the opinion of the entire italian radiological community . in conclusion , the majority of responders are in favor of tr and believes that it will have a future . 
second or subspecialty opinion is another common application of tr . compliance with ethical standards conflict of interest the authors do not have any competing interest to be disclosed . ethical approval this article does not contain any studies with human participants performed by any of the authors . appendix shows all 19 questions with answers of the survey 1 . 
how are radiological images stored in your institute ? on a analog archive 5.73 % each diagnostic modality has its 5.02 % own archive on a pacs system on pacs of the department on pacs of 2 or more health facilities on pacs ; images and clinical data are accessible from electronic health records 7 . 
muellerlisse1 received : 5 january 2016 / accepted : 18 april 2016 / published online : 6 may 2016 italian society of medical radiology 2016 abstract purpose to compare contrast - enhanced low - dose multidetector - row computed tomography ( ce - ldct ) of the chest with unenhanced ( un - ) ldct and contrast - enhanced standard - dose ct ( ce - sdct ) in regard to the delineation of intrathoracic lymph nodes . materials and methods based on the international association for the study of lung cancer ( iaslc ) grouping of thoracic lymph nodes , two independent radiologists retrospectively assessed lymph node delineation in 9 ce - ldcts ( 64 rows , 120 kv , p < 30 mas / slice ) and in 2 control groups of 36 un - ldcts and 36 ce - sdcts , each matched for gender , age , chest / lung diameters , and clinical history . 
at a significance level of p < 0.025 ( bonferroni - correction for two control groups ) , two - tailed chi - square and fishers exact tests were applied . 
measurable lymph nodes did not significantly differ in size between cases and controls . conclusion at ce - ldct of the chest , delineation of mediastinal and hilar lymph node groups was superior to un - ldct and similar to ce - sdct . 
ce - ldct may be a promising alternative for patients with non - malignant lung disease , unclear chest x - ray findings , or the need for follow - up . keywords chest ct low dose lymph node delineation iaslc classification introduction radiation protection has become an increasingly important issue in the field of computed tomography ( ct ) over the last two decades , since different studies and meta - analyses have revealed that ct is the most relevant reason for medical diagnostic radiation exposure [ 13 ]  . 
one of the most important aspects of radiation protection is the integration of the alara ( as low as reasonably achievable ) principle in clinical care , that means reducing radiation exposure while maintaining a sufficient diagnostic image quality at the same time . it has often been recommended to apply unenhanced , dose - reduced chest ct examinations for medical questions related to lung tissue [ 4 , 5 ] , lung nodules [ 6 , 7 ] or pneumonia [ 8 ] , accepting a loss of information on mediastinal and hilar structures . 
a supplementary contrast - enhanced ct examination , which is usually based on standard - dose protocols , may be required to differentiate between enlarged lymph nodes , other mediastinal masses , and benign anatomical variants , because both the extent and the pattern of intra - thoracic lymphadenopathy are useful in the diagnosis of different benign [ 9 ] and malignant [ 10 ] diseases . 1 3 radiol med ( 2016 ) 121 : 644651 fig . 
1 schematic diagram of the casecontrol study design it has already been demonstrated that dose - reduced ct protocols can be applied after the application of intravenous ( i.v. ) contrast media , to identify mediastinal masses , since they still provide satisfactory diagnostic information in the follow - up of different oncological patient groups [ 11 , 12 ]  . 
current results show that ultra - low - dose mdct protocols ( ctdi < 0.9 mgy ) [ 13 ] and dose - reduced ct protocols involving iterative reconstruction techniques ( irts ) [ 1417 ] have the potential to delineate enlarged lymph nodes in non - obese patients . 
however , these studies did not focus on the delineation of lymph nodes in different intra - thoracic locations . thus , a detailed assessment of the delineation of individual intra - thoracic lymph node groups , according to the established international association for the study of lung cancer ( iaslc ) classification [ 18 ] , has not yet been performed in low - dose ct of the chest ( ldct )  . 
hence , our retrospective study evaluated the delineation of different mediastinal and hilar lymph node groups according to the iaslc classification in contrast - enhanced ldct ( celdct )  . 
ct images in our study were reconstructed using filtered back projection ( fbp ) , with a soft tissue kernel , in axial and coronal planes . patients the retrospective study group consisted of nine patients ( cases five women / four men , mean age 47.3 years , range 2572 years ) who had contrast - enhanced low - dose - mdct of the chest ( ce - ldct ) within one 3 - month time period at our institution under stable scan conditions . 
only patients with a body mass index ( bmi ) of less than 25 kg / m2 were included , since this was the institutional precondition for a greatly dose - reduced ct protocol . 
one control group consisted of patients with unenhanced low - dosemdct of the chest ( un - ldct ) and the other of patients with contrast - enhanced standard - dose - mdct of the chest ( ce - sdct )  . materials and methods ethical considerations image acquisition this retrospective matched casecontrol study was based on data previously acquired during the course of routine clinical care , performed in accordance with the declaration of helsinki and approved by the local ethics committee . examinations were performed on a 64 - row mdct scanner ( brilliance 64ct , philips healthcare , hamburg , germany ) at a tube charge of 120 kvp ( collimation 64 0.5 mm , pitch 1.173 , rotation time 0.5 s , dose modulation , filtered 1 3 646 radiol med ( 2016 ) 121 : 644651 back projection , reconstruction algorithm c and ya , effective primary reconstruction slice thickness 0.625 mm , reformatted axial slice thickness for soft tissue structures , 5 mm )  . 
ce - ldct and ce - sdct scans were obtained 33 s after starting the bolus injection of intravenous contrast media with 350 mg of iodine / ml ( volume 70 ml , flow rate 3 ml / s , followed by 50 ml of normal saline solution at 3 ml / s )  . radiation dose estimation on a set of two diagnostic monitors certified for cross - sectional medical imaging , with one image per display , at soft tissue window settings ( window center , 50 hu ; window width , 350 hu )  . 
based on the idea that image information can only be diagnostic or non - diagnostic , lymph nodes in each zone were separately evaluated in two categories , either as measurable or non measurable . 
prior to the evaluation , the two radiologists jointly assessed three cases of ce - sdct that were not included in this study . the approximate effective dose according to icrp 103 [ 19 ] was determined . 
for calculation , the phantom - based ct dose index ( ctdi ) and the dose length product ( dlp ) were used , as automatically computed by the scanner software . statistical analysis mdct evaluation based on the international association for the study of lung cancer ( iaslc ) grouping of thoracic lymph nodes [ 18 ] , two radiologists ( r1 , r2 ) with different clinical work experience retrospectively assessed mediastinal and hilar lymph node delineation in ce - ldct , un - ldct , and cesdct scans , independent of each other . 
r2 was a radiology resident with 3 years of post - graduate clinical work experience , including a 1 - year ct training rotation with approximately 50 % of the case load involving chest ct assessments . 
however , it may also be applied as a general anatomical classification system , since the extent and pattern of thoracic lymphadenopathy may aid in the diagnosis of different pulmonary and extrapulmonary diseases [ 9 ]  . 
in our analysis , radiologists assessed intra - thoracic lymph node subgroups at the zone levels of the current iaslc classification [ 18 ] , including the superior mediastinal , aortic , subcarinal , posterior mediastinal , hilar and peripheral lymph node subgroups . 
comparison of chest and lung diameters between cases and controls yielded significant differences for p < 0.05 at two - sided testing with students t test under the assumption of different variance according to glantz [ 22 ]  . for inter - observer comparison , kappa values were calculated according to landis and koch [ 24 ]  . 
 average and standard deviation of the calculated effective dose , as provided by the ct scanner for each individual patient , were recorded for cases and control groups . 1 3 radiol med ( 2016 ) 121 : 644651 results retrospective study group ( cases ) for all iaslc lymph node zones together , the two independent radiologists agreed on delineation of measurable lymph nodes in 47 of 54 ( 87 % ) lymph node zones at ce - ldct . table 1 demonstrates the delineation of measurable lymph nodes between the iaslc lymph node zones of the mediastinum , hila , and lung for the retrospective study group ( cases , patients with ce - ldct )  . 
patient numbers with at least one measurable lymph node in a certain lymph node zone and corresponding p values referring to two - tailed fishers - exact - testing ( significant at p < 0.025 ) for inter - group comparison are stated . 
patient numbers with lymph nodes > 1 cm in short diameter detected by r1 and r2 are given in parenthesis 1 3 648 radiol med ( 2016 ) 121 : 644651 fig . 
2 ct scans of six different patients ( columns ) in axial orientation showing intrathoracic lymph nodes of corresponding zones according to the iaslc - classification ( rows )  . 
contrast enhanced ( ce - ) ldct slices of the test group ( columns a , b ) are surrounded by ct slices of two matched controls , respectively : left neighbouring , unenhanced ( un - ) ldct , right neighbouring , contrast enhanced ( ce - ) sdct . 
in the female patient with acute tuberculosis ( a ) , enlarged lymph nodes are delineated in the upper mediastinal and subcarinal zone ( arrows ) as well as in the aortopulmonary , hilar and lower mediastinal zone ( arrow heads )  . 
we applied the iaslc schematic [ 18 ] , which has originally been designed for intrathoracic cancer staging , to describe and compare lymph node anatomy as delineated by different ct protocols . radiation exposure was reduced by about three quarters at average , from about 4 msv at ce - sdct to about 1 msv at ce - ldct , without apparent loss of intrathoracic lymph node delineation in different lymph node zones . 
 they described an acceptable delineation of mediastinal and hilar structures , including the reliable detection of enlarged lymph nodes , with an effective dose of 0.5 msv at 256 - row - mdct . 
this may be clinically useful in the follow - up of target lesions in cancer patients , or in the differentiation of smaller lymph nodes , anatomical structures and incidental findings [ 25 ]  . 
 previous research shows that the detection of small but suspicious paraesophageal lymph nodes may have crucial diagnostic and therapeutic consequences [ 26 , 27 ]  . compared with recent studies on low - dose ct of the chest based on different techniques of iterative image reconstruction ( irt ) [ 1417 ] , our study revealed at least equivalent potential for dose reduction based on fbp . 
that study reported improved delineation of mediastinal structures compared with fbp , such that it may be assumed that irt could add benefit to reduced - dose ct protocols with contrast enhancement for chest imaging such as ours . prior studies on contrast - enhanced , reduced - dose ct protocols have delineated mediastinal masses and enlarged lymph nodes in the follow - up of patients with esophageal or urogenital cancer [ 12 ] and patients with lymphoma or extrapulmonary cancer [ 11 ]  . 
however , in contrast to our approach , those studies did not use a specific or generally accepted lymph node classification syste moreover , our study group included non - oncological patients and patients without preceding ct examinations . 
while lymphadenopathy in the peripheral lymph node zone may be assumed when suspicious changes are found in lung - window images , our lymph - node - zone - based findings in axial and coronal soft tissue reconstructions imply that contrast enhancement may be crucial in the delineation of hilar and interlobar lymph nodes their distinction from other tissues . 1 3 650 radiol med ( 2016 ) 121 : 644651 the significantly improved lymph node delineation in the hilar zone in contrast - enhanced ldct scans compared to unenhanced ldct scans correlates with former findings with a standard dose protocol [ 28 ]  . 
in that context , the limited overall lymph node delineation rate of 81 % in the ce - sdct control group of our study was mainly due to poor results in the lower mediastinal lymph node zones . 
that in turn may be explained by the small degree of lymph node enlargement found in this zone , and by the presence of vertebral vessels that affected lymph node delineation . 
the same delineation problems also appeared in the study group and in the second control group , possibly as an effect of our detailed patient matching procedure . some limitations apply to our analysis . 
first , we performed a retrospective single - center study of ct examinations performed with one specific 64 - row - mdct scanner , with a fixed low - dose mdct protocol adjusted for nonobese patients . 
in particular , it cannot be excluded that other scan parameters or reconstruction methods would allow for further dose reduction , or would possibly be applicable even in obese patients . 
limitations due to this restriction were balanced with a high level of inter - observer agreement in our results , which was similar for all patient groups and all lymph node zones despite the difference in the observers clinical work experience ( only those lymph node zones were called measurable that were delineated by both observers )  . 
as differences in the lymph node status between cases and controls cannot be completely ruled out using matching criteria , however , the number and localization of lymph nodes within a single zone were not taken into account in detail in our zone based matched casecontrol analysis . 
this limitation was balanced by oversampling and individual matching of different physical variables in the control groups based on well - established sample size calculation [ 23 ] : a difference of less than 15 % in lymph node delineation for all zones together was accepted as non - significant at a statistical power of 0.80 assuming that lymph nodes would measurably delineate in less than 75 % of cases and more than 90 % of controls . 
however , even if ce - ldct seems to provide similar information about the intrathoracic lymph node status in comparison to ce - sdct , it certainly cannot be excluded that future studies with greater sample sizes would reveal more subtle differences . conclusion ce - ldct of the chest seems to be an alternative to standard dose ct when supplementary information on the intrathoracic lymph node status in different lymph node zones according to the current iaslc classification could be diagnostically helpful . 
further studies with larger sample sizes will be required to validate ce - ldct of the chest . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical standards this was a retrospective study . 
khoury2 received : 28 october 2015 / accepted : 5 april 2016 / published online : 23 april 2016 italian society of medical radiology 2016 abstract objective of the study to assess the prevalence of cortical bone invasion ( cbi ) with secondary extramedullary hematopoiesis ( emh ) in patients with non - transfusion - dependent thalassemia ( ntdt ) , to determine its predilection sites on thoracic and abdominal imaging , to determine whether there is an association between various clinical and hematological parameters , and to evaluate its various findings mainly on magnetic resonance imaging ( mri ) , in addition to computed tomography ( ct ) scans . materials and methods this is a retrospective cohort study of 57 patients with ntdt imaged by ct or mri . 
an imaging scoring system was used to describe the appearance of cbi by mri . results twenty - seven patients ( 47.4 % ) were found to have cbi and emh with the most common location being the thoracic spine . 
box 11 - 0236 , riad el - solh , beirut 1107 2020 , lebanon 3 division of hematology - oncology , department of internal medicine , american university of beirut medical center , beirut , lebanon 4 faculty of medicine , american university of beirut , beirut , lebanon conclusion cbi and secondary tumefactive emh are common findings in patients with ntdt , with distinct imaging and clinical characteristics . 
an increased risk was seen in patients with splenectomy and lower hemoglob the imaging scoring system described is helpful in diagnosing and describing this entity , hence precluding unnecessary biopsies . keywords non - transfusion - dependent thalassemia extramedullary hematopoiesis cortical bone invasion soft tissue lesion introduction non - transfusion - dependent thalassemias ( ntdt ) are part of a group of inherited hemoglobinopathies previously known to be endemic to certain areas of the world ; however , lately they have been recognized as a growing global health concern [ 1 ]  . 
 however , they do suffer from complications due to ineffective erythropoiesis as well as hemolytic anemia , typically related to iron overload [ 3 ] and extramedullary hematopoiesis ( emh ) [ 4 ]  . traditionally , emh is defined as a non - neoplastic proliferation of hematopoietic tissue outside the bone marrow and peripheral blood [ 5 ]  . 
these masses can be discovered incidentally or can grow large enough to cause significant symptoms . 1 3 radiol med ( 2016 ) 121 : 626634 bone marrow expansion in thalassemia manifests as typical craniofacial changes [ 7 ] ; however , deformities and thinning of the cortices of long bones and vertebrae , especially in the thoracic region , and to a lesser extent the lumbar region , also occur [ 4 ]  . 
there can be secondary , cortical breaks or cortical bone invasion ( cbi ) by the expanded trabecular bone and by the formation of adjacent foci of erythropoietic tissue [ 8 , 9 ] , usually termed emh in the literature . 
however , in our opinion , the term cbi better reflects the bone marrow expansion , cortical disruption , and subsequent formation of peri - / para - skeletal foci of erythropoiesis / hematopoiesis . hence , in our opinion , the concept of emh should include two pathophysiologically different phenomena : cbi and emet . 
both are related to chronic hemolytic anemia and ineffective erythropoiesis ; however , these two phenomena are different since one involves a systemic activation of hematopoietic cells outside the musculoskeletal system such as the spleen or liver , and the other involves overacting bone marrow and expansion of the intramedullary space into the soft tissues through a cortical break . 
 the question as to whether there is an association between cbi and various clinical and hematological parameters in patients with ntdt has not been previously addressed . the aims of this study were to assess the prevalence and characteristics of cbi in patients with ntdt , to determine the predilection sites of cbi on thoracic and abdominal imaging , to determine whether there is an association between various clinical and hematological parameters in these patients and to evaluate the various findings of cbi mainly on magnetic resonance imaging ( mri ) , as well as computed tomography ( ct ) imaging . radiological review the imaging modalities were not uniform since this was a retrospective review of patients . 
these mr examinations were performed using axial t2 - based spin - echo ( se ) and fast field echo ( ffe ) sequences as follows : tr 1000 ; 618 ( 1.5 t philips ingenia , the netherlands ) ; or 618 ( 1.5 t philips intera , the neth2500 , te erlands )  . 
the images were evaluated for the presence of cbi , which was defined as bone marrow expansion with cortical disruption and adjacent secondary soft tissue formation representing emh . a previously described scoring system was used based on mr imaging , which included five different variables : cbi score , fat score , homogeneity score , margins score , and bone marrow signal ( bms ) score ( table 1 ) [ 10 ]  . 
bms and bm expansion were assessed in all patients regardless of their cbi score . materials and methods cbi score patients this is a retrospective cohort study of all patients at the chronic care center , which specializes in the treatment of patients with thalassemia , and who have been diagnosed with ntdt and imaged by mri and / or ct scans for any reason . 
institutional review board ( irb ) approval has been obtained for this study . clinical data were gathered on ntdt patients from the medical records , including basic demographic information ( age , sex , diagnosis ) , hemoglobin concentration at the time of imaging , platelet count , transfusion history , splenectomy status , fetal hemoglobin concentration , serum ferritin , and liver iron concentration . 
a mri obtained for liver iron overload evaluation using t2 - ffe ( tr 9 ) ; showing paravertebral emh with bone expansion , cbi score of 1 ; the emh on the right ( arrow ) has relatively homogeneous predominantly fat signal ( fat score 3 ) , and the emh on the left ( arrowhead ) shows rather homogeneous red marrow signal , iso - intense to the bone marrow ( fat score 0 )  . 
 b ct scan of the spine performed 3 years earlier , more superior cuts showing thoracic vertebral body expansion with cortical irregularities and erosions , along with surrounding soft tissue lesions due to emh 1 3 radiol med ( 2016 ) 121 : 626634 fig . 
c axial ct scan however clearly identified anterior cortical invasion ( cbi score 2 ) with large pre - sacral soft tissue structure containing sheaths of bone trabeculae and representing emh independent - samples t - test for continuous variables and the fishers exact and spearmans test for categorical variables . 
the right paraspinal lesion has relatively similar proportions of fat and red marrow signal ( fat score 2 ) results patients characteristics a total of 57 patients who fit the diagnosis of ntdt , with available imaging studies and laboratory values , were 1 3 630 radiol med ( 2016 ) 121 : 626634 1000 , te fig . 
a axial t2 - weighted mr ( tr 9 ) of the lower chest shows expansion of multiple ribs with surrounding soft tissue lesions due to definite cbi ( score 2 ) and secondary emh . 
t2 - ffe ( tr 12 ) , axial mr image obtained at the level of a thoracic disk space shows left paraspinal lesion appearing heterogeneous with both red and fat signal intensity ( fat score 2 )  . 
no lesions were encountered within the spinal canal . with regard to the fat score , five contained soft tissue isointense to red marrow but no fat ( 0 ) , nine were primarily composed of non - fatty soft tissue ( 1 ) , four had similar proportions of fat and soft tissue isointense to red marrow ( 2 ) , and nine were primarily composed of fat ( 3 )  . 
sixteen patients had mild bone marrow expansion . among the four patients imaged with ct scans , one had a large sacral cbi with emh , one had similar but diffuse skeletal changes involving the ribs , spines , and iliac bones , and another had a paravertebral location of emh . cbipositive versus cbinegative patients table 4 summarizes the findings comparing clinical variables of cbi - positive ( cbi score of 1 or 2 ) and cbi - negative ( cbi score of 0 ) patients . 
the majority of patients had cbi at multiple sites , most commonly at the thoracic paraspinal area near the costovertebral junctions seen in 25 patients in the present study , almost half of ntdt patients imaged for various purposes had evidence of cbi with emh . 
it might represent a difficult diagnosis , especially when the location , distribution , and size of the masses raise the possibility of other differential diagnoses , such as lymphomas and primary bone tumors [ 13 ]  . 
in most of the reported cases in the literature , tissue biopsy or surgical resection was needed ; however , these procedures carry a risk of hemorrhagic complications particularly that the lesions are usually highly vascular [ 14 ]  . 
when characteristic imaging findings are recognized in patients with ntdt as cbi , invasive diagnostic procedures , such as biopsies , are not necessary . currently , mri is the modality of choice in evaluating patients with emh in thalassemia . 
the lesions are usually characterized by lobular masses with increased signal intensity when compared to that of the red marrow in the adjacent vertebral bodies , on t1 - weighted and t2 - weighted images [ 16 ]  . 
usually , the lack of enhancement post - gadolinium administration helps its differentiation from other lesions such as abscesses , primary bone tumors , or metastases [ 17 ]  . 
however , ct scan is accurate in differentiating between probable and definite cbi , since cortical breaks are , as expected , not always easily apparent on mr images and much better seen on ct scan . 
approximately two - thirds of our patients showed predominant red bone marrow signal due to anemia , the same number had homogeneous soft tissue lesions , and all but three had well - defined margins . 
hence , in the clinical setting of ntdt , expanded red bone marrow along with 1 3 radiol med ( 2016 ) 121 : 626634 cortical irregularity associated with adjacent well defined , mostly homogenous , soft tissue lesions showing either predominant isointense signal to red marrow or predominant fatty signal would be highly suggestive of cbi with secondary emh . 
threshold values for our scoring system that resulted from these findings were not analyzed since the variable appearance of these lesions may lead to variable scoring , rendering such values of limited use . 
the importance of this scoring system was to provide a systematic approach to interpret and recognize the variable appearances of these lesions . the most common site of cbi in our study was the thoracic spine , at the costovertebral junction , whereby it was seen in over 90 % of patients , followed by the ribs . 
these data differ from a previous clinical and radiographic study on emh , which found that the most common musculoskeletal location is the ribs , followed by the vertebrae [ 18 ]  . 
 this may be due to the fact that we did not have complete thoracic imaging for all patients , which may have underrepresented the number of rib lesions . patients with positive findings of cbi in the present study were more likely to have undergone a splenectomy , and have lower hemoglobin and a higher platelet count . 
 splenectomy is also associated with increased risk of infection and pulmonary hypertension . a recent prospective study found that serum transferrin levels could be predictive of emh in splenectomized patients [ 20 ] ; however , this was not found to be predictive of cbi in our study . 
those with positive findings of cbi in the present study were less likely to never have been transfused and much more likely to have been occasionally transfused than those with negative findings . 
this raises the possibility that two different processes take place in the development of paraspinal emh , one that results from cbi and the other , which may be related to penetrating vessels from the vertebral body . 
 although this theory may be valid , we did not however encounter in our series any case of paraspinal masses adjacent to normal bone or any lesion away from bone . 
one explanation of this difference in our findings is that the slice thickness of the ct scan used in the tsitouridis study was 5 mm with no high bone window resolution whereas the slice thickness in our study was 1.5 m penetrating vertebral vessels might contribute to this phenomenon along with the presence of cortical invasion as seen in our series . this study has limitations inherent to all retrospective studies . 
 furthermore , clinical data , which had been gathered prospectively on this patient population for a previous study and was readily available , were missing history on pulmonary hypertension , hydroxyurea intake , and laboratory data such as nucleated red blood cells . in conclusion , our data suggest that cbi and secondary emh are common findings in patients with ntdt . 
the majority of the extramedullary lesions were well defined , homogenous , showing either minimal or significant amount of fat , and mainly located at the costovertebral junction of expanded thoracic vertebral bodies , rich in red marrow . 
information about population was collected ( anthropometric data , sport activity , taken therapy and associated conditions / pathologies )  . results statistically significant correlation was found between bmi and eus findings ( p 0.007 ) and between eus aspect and us diagnosis ( p 0.039 ) both to the right tendon . 
the multivariate analysis showed that eus results are correlated only with bmi ( high bmi corresponds to the best eus results ) , independently from smoke and associated conditions on right side . 
the 60 % of volunteers has * emanuela capalbo emanuelacapalbo@tiscalinet.it 1 scuola di specializzazione di radiodiagnostica , universit degli studi di milano , via di rudin , 20142 milano , italy 2 dipartimento di scienze diagnosticheuoc di radiologia , ospedale san carlo borromeo , via pio ii , 3 , 20147 milan , italy played sports that may lead overload of the achilles tendon . 
statistically significant correlation was found between eus aspect and us diagnosis on the right tendon but not on the left correlation between thickness and eus aspect was calculated : no correlation was found . 
however , the flexed ankle position , needed to properly examine the distal third by us , alters the elasticity of the tendon and causes false negative results to eus . 
according to its anatomy , achilles tendon can be divided into three third : proximal third or musculotendinous junction , middle third 26 cm from calcaneal 1 3 668 radiol med ( 2016 ) 121 : 667674 insertion , and distal third at the insertion at the calcaneus [ 1 ]  . tendon alterations can result from the level of sports activities [ 2 , 3 ] , from the use of corticosteroids , fluoroquinolones and oestrogen medications [ 4 , 5 ]  . 
also tendon elasticity decrease with increasing age [ 7 ]  . proximal third pain is not very common [ 8 ] ; middle third is commonly affected by tendon ruptures , particularly in athletes , but also in nonactive individuals . 
distal third alterations depends on the overload and they are influenced by the type of used footwear [ 9 , 10 ] ; also , condition is more complex compared to middle third , since tendon , bursae and bone ( and combination of these ) can be involved [ 3 ]  . 
a prominent posterior angle of the calcaneal bone may cause impingement on the tendon [ 11 ]  . for tendon investigation , the ultrasound ( us ) is an accurately and non - invasively method , to assess the morphological and dynamic aspects of tendon structure [ 2 ]  . 
to support the diagnosis , a method for evaluating the tissues elasticity : the ultrasound elastography or sonoelastography ( eus ) in recent years has been joined to the us investigation [ 12 , 13 ]  . 
the principle of eus is that tissue compression produces a displacement within the tissue , and this strain is less in hard tissue than in soft tissue [ 13 ]  . 
recently , it was applied to muscle - skeletal system [ 1 , 12 , 1517 ]  . there are several eus techniques [ 15 ] : one of these is axial strain elastography , in which the compression is applied manually . 
real - time axial - strain eus is the simplest technique allowing direct visualisation of the elastogram superimposed on the b - mode image [ 12 ]  . the aim of this study is to evaluate eus findings of distal third of achilles tendon in asymptomatic volunteers and to correlate with subject characteristics and us findings . 
 successively , we want to calculate the inter - observer concordance for reproducibility of method . materials and methods study population in this prospective study , from january to may 2012 , 80 consecutives achilles tendons were examined with us and eus in 40 consenting asymptomatic volunteers . volunteers were asymptomatic at the examination time ; they were questioned both about tendon injury , inflammation , surgery , or painful and about traumas on the lower limbs in general . 
we dont find subjects with a history of tendon rupture . information was collected about associated conditions that may determine a change in the load on the distal third of the tendon ( e.g. , congenital or post - traumatic limb dysmetria ) or pathologies that may involve the tendons ( e.g. , rheumatological diseases , collagen abnormalities , infectious diseases , neurological conditions ) [ 4 ]  . 
sporting activity was classified intense if performed four or more times / week , moderate if about three times / week and mild if one or two times / week . 
potential sports overload was also considered . examination protocol two radiologists , specialised in muscle - skeletal imaging ( with 10 and 4 years of experience ) , independently performed us and real - time axial - strain eus using the same ultrasound system ( hi vision preirus , hitachi medical ) and the same linear transducer at a frequency range of 1315 mhz . subject was placed in prone position with the feet hanging free below the foot - end of the examination table with the ankle flexed to 90 to allow a correct visualisation of the distal third of the tendon . the insertional third was examined in longitudinal scanning , measuring the anteroposterior diameter and analysing the echogenicity and echotexture in longitudinal and transverse view . 
transducer was positioned perpendicular to the tendon to avoid anisotropy . the tendon measure in anteroposterior view has been considered normal for thickness up to 57 mm [ 18 ]  . 
we found : previous neoplasm ( 2f , 1 m ) , arterial hypertension ( 5f , 4 m ) , gastric ulcer ( 1 m ) , anemy ( 2f )  . the multivariate analysis showed that eus results are correlated only with bmi ( high bmi corresponds to the best eus results ) , independently from smoke and associated conditions on right side . 
correlation between thickness and eus aspect was calculated : no correlation was found ( table 4 )  . interoperator correlation was excellent ( k 0.89 for left tendon and k 0.91 for right tendon )  . discussion sonoelastography has been recently introduced to assess muscle and tendons elasticity [ 2 , 13 ]  . 
 b us shows areas of fusiform hypoechogenicity , so the tendon is tendinosic tendon is the most studied structure since it is a simple target to examine [ 1 , 12 , 13 , 18 , 21 , 22 ]  . 
in literature , there is no work about only the distal third , so we decided to examine it . some parameters are known to be related to various alterations of the achilles tendon : age , sports , sex , dominant - side , inflammatory and autoimmune conditions , medications [ 4 ]  . 
moreover , this could be linked to the right predominance of study population ; it is necessary to enrol a population with higher rate of left predominance to demonstrate it . 
in our opinion , the association between higher bmi and eus best results could be due to a greater influence of the sports overload on the health of the tendon , with respect to the overload linked to a higher bmi . 
 although statistically significant correlation between activity and eus appearance has not been found , the relationship between sport and degeneration of the tendon is known , in fact , in our sample , 61.5 % of patients with bmi 25 did not practise sports , while 63.6 % of the volunteers with bmi < 25 was sportingly active . regarding the smoke : in some works , a significant correlation between smoking and thickness / degeneration of the tendons has not been demonstrated [ 24 , 25 ]  . 
 in our opinion , these data is influenced by examination position of ankle ( 90 of flexion ) : in fact when the achilles tendon is maximally stretched , elasticity increases [ 27 ]  . 
a major part of works use the relaxed position [ 1 , 12 ] and we found only one study in literature comparing elasticity at different levels of flexion [ 27 ]  . therefore , position alters the elasticity of the tendon and causes false negative results ( tendon might be harder )  . 
to avoid this problem , it would be appropriate to carry out the eus study of the distal third in relaxed position , perhaps using a gel pad to ensure the probe adhesion . 
it is also possible to use the semiquantitative method provided by the machine software but the qualitative interpretation may be more useful in clinical practise [ 12 ] ; it is more immediate and reduces the examination time . 
5 a visual indicator on the screen gives an optimal dynamic range of pressure : it is necessary that the graph of compressions remains within the minimum and maximum lines to get the right pressure shows that reproducibility of eus is excellent when performed qualitatively and poor when semi - quantitatively evaluation ( strain ratio ) was used [ 15 ]  . a possible limit of the method is that the application of pressure to the probe is relatively operator dependent [ 13 ] and there is significant differences in both the maximum and the mean value of the elastic modulus of the muscles and tendons when different transducer pressure were applied [ 23 ]  . 
however , the flexed ankle position , needed to properly examine the distal third by us , alters the elasticity of the tendon and causes false negative results to eus . 
then for the eus study of the distal third , it would be appropriate the relaxed position , with a gel pad to optimise the probe adhesion . in conclusion : this study provides many opportunities to improve the routine use of eus . 
further studies would be needed to investigate aspects highlighted by our study . compliance with ethical standards conflict of interest the authors declare that she has no conflict of interest . funding none funding have this study . ethical approval all procedures performed in the studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent informed consent was obtained from all individual participants included in the study . radiol med ( 2016 ) 121 : 675680 doi 10.1007 / s11547 - 016 - 0641 - 6 ultrasonography evaluation of tablet ultrasound for routine abdominal interventional procedures anna maria ierardi1 federico fontana1 francesca giorlando1 giuseppe de marchi1 antonio pinto2 alessandro radaelli3 stephanie schampaert3 massimo tonolini4 raffaele novario5 gianpaolo carrafiello1 received : 8 december 2015 / accepted : 11 april 2016 / published online : 30 april 2016 italian society of medical radiology 2016 abstract aim the aim of the study was to establish if a novel tablet ultrasound ( us ) may replace a high - end us machine during routine interventional radiology activities . materials and methods thirty consecutive patients were evaluated by two operators comparing the performance of the new us tablet system ( visiq , philips healthcare ) against a high - end us system ( iu22 , philips healthcare ) using a curved probe ( c5 - 2 )  . 
a structured questionnaire was used to rank on a 4 - point scale the ability of each system to locate a target as detected by previous examinations and visualize needles and path during an interventional procedure . 
necessity for conversion from the tablet us to the high - end us system was registered ; body mass index ( bmi ) was annotated for each patient . results agreement between the operators was found for every patient . 
conversion to the high - end system was registered in 40 % of cases : in most cases ( 66.6 % ) * gianpaolo carrafiello gcarraf@gmail.com interventional radiology unit , department of radiology , university of insubria , viale borri , 57 , 21100 varese , italy 2 department of radiology , cardarelli hospital , naples , italy 3 philips healthcare , best , the netherlands 4 department of radiology , luigi sacco university hospital , via g.b. 
grassi 74 , 20157 milan , mi , italy 5 department of biotechnology and life sciences , medical physics , university hospital of varese , varese , italy the decision was due to the absence of a dedicated needle guide for the tablet us . conclusions the novel tablet us was found to provide sufficient image quality for the majority of routine interventional procedures . 
dedicated accessories and additional experience with this new generation us device may be needed to replace bulky high - end us systems . keywords tablet ultrasound interventional radiology introduction ultrasonography ( us ) is a valuable , noninvasive and widespread imaging examination technique [ 1 ]  . 
us imaging is routinely used alongside computed tomography ( ct ) and magnetic resonance imaging ( mri ) and is recommended by most international scientific bodies , such as the american association of physicists in medicine , american institute of ultrasound in medicine , and american college of radiology [ 24 ]  . 
however , a standardized set of criteria for quality assurance has not yet been formally established and only nonspecific standards are currently available [ 1 , 4 ]  . the use of ultrasound in interventional radiology has been growing over the years and ultrasound machines are available in most labs as supportive equipment or connected to and controlled from the angiographic table . ultrasound guidance is commonly used for vascular access prior to catheterization [ 5 ] , to guide percutaneous biopsies and ablations [ 6 , 7 ] , to deploy thoracic and abdominal drainages [ 8 ] , and , although less frequently , to support percutaneous embolization procedures ( pseudoaneurysms , visceral aneurysms or abdominal aneurysms , etc . ) [ 9 , 10 ]  . 
in addition , modern ultrasound machines provide image fusion and contrast - enhanced modes , which 1 3 676 radiol med ( 2016 ) 121 : 675680 10 years experience in ultrasound imaging compared the image quality of the new us tablet system ( visiq , philips healthcare ) against a high end cart - based us machine ( philips iu22 , philips healthcare ) , judging the ability to perform the following tasks : ( 1 ) locate a lesion or a target detected by previous examinations ( ct , mri , ect ) , ( 2 ) visualize and guide needle insertion during an interventional procedure . 
1 high end cart - based us machine ( philips iu22 , philips healthcare ) and the new us tablet system ( visiq , philips healthcare ) extend the utility of ultrasound imaging in interventional oncology [ 11 , 12 ]  . one of the potential limitations for a wider use of ultrasound during interventional practice is the footprint of most high - end us systems . 
portable and tablet ultrasound machines are currently used for vascular access , for an immediate visual correlation with physical examination findings or for a quick and instant assessment in emergency settings . 
recently , a new generation of tablet ultrasound machines was introduced for obstetrics and gynecological examinations with the promise to provide performance levels close to high - end us systems . 
 in all cases in which lesions or needle were not detectable with sufficient safety to perform percutaneous procedure , low quality of the image was attributed to the low penetration . 
no clear correlation was found between the decision to convert to the high - end us system and patient bmi ( mean 25 , range 1734 ) , target location or type of interventional procedure . no complications during the procedures were observed . discussion since the establishment of ultrasound imaging as a safe and reliable modality for percutaneous diagnostic procedures , the range of applications in interventional imaging have grown at a fast pace and techniques such as doppler , image fusion , contrast - enhanced imaging , and elastography have extended its adoption and preference as a primary interventional modality . a recent trend in ultrasound imaging is miniaturization . 
4 renal lesion visualized with high - end us system ( philips iu22 , philips healthcare ) ( a ) and with us tablet system ( visiq , philips healthcare ) ( b ) fig . 
5 needle visualization with high - end us system ( philips iu22 , philips healthcare ) ( a ) and with us tablet system ( visiq , philips healthcare ) ( b ) fig . 
7 blandaltman plot test demonstered superiority of high - end us to visualize target ( a ) against a better visualization of the needle with the tablet us ( b ) fig . 
8 mountain plot test revealed superiority of the high - end us to visualize target against a better visualization of the needle with the tablet us ( ci 95 % ) pre - hospital emergency medicine [ 16 , 17 ] , showing their value in achieving a quick clinical assessment and save time . 
other studies have used pocket - size ultrasound devices to supplement computed tomography or have compared the clinical value of portable ultrasound devices with that of high - end instruments for diagnostic evaluation [ 16 18 ]  . 
in high - volume interventional radiology departments , us is routinely used for the visualization of pleural or abdominal free fluid , to detect intrahepatic bile ducts and to assist with image guided vessel or tumor punctures . 
any new us device should provide sufficient image quality to localize the targeted vascular or soft tissue structure , and to visualize needle advancement along the entire path from skin entry point to the target , considering that a definite diagnosis is normally already available . our results showed that b - mode images of the new tablet us were considered insufficient only in 3 % of the total cases examined and that needle visibility was surprisingly superior to the high - end syste in our study no correlation was found between the decision to convert to the highend us system and patient bmi , target location or type of interventional procedure ; in these cases the low penetration of the image was considered the cause . 
probably more patients and more cases are necessary to stabilize if this limit could be overcome ( using needle guidance or contrast enhanced ultrasound , ect ) and if factors like bmi , lesion location or its dimension really not influenced the choice of the operator . 
however , this did not correspond directly with the conversion rate to the high end system , proving that the adoption of such devices may still require a learning curve for confident ultrasound interpretation . 
in addition , we postulate that the availability of contrast enhanced ultrasound mode , linear probe and needle biopsy guide accessories ( although the latter may not be a key requirement for other institutions ) are necessary additions to make this novel device suitable for a wider applications range including vascular access and muscoloskeletal procedures . we did not find that the limited battery life , which needs to be recharged after a few hours [ 18 ] , would represent a significant limitation , considering that not all interventional procedures required the utilization of ultrasound and that our lab nurses could easily follow a routine recharge between cases . 1 3 680 radiol med ( 2016 ) 121 : 675680 the introduction of a small - footprint and mobile us machine in interventional practice may bring several advantages not directly evaluated in this study : time saving , given the shorter booting time , quicker transfer , and easier positioning at the patients bedside ; more comfort for the operator , who can benefit from more flexibility in device positioning ; and lower costs , with a potential availability of multiple units for labs with several operators . the major weak points of our study are the following : the low number of patients included ; only subjective visual method was adopted to evaluate the quality of the image ; only abdominal procedures were considered . in conclusion , the examined novel tablet us may provide sufficient image quality for the majority of routine abdominal interventional procedures . 
dedicated accessories and additional experience with this new generation us device may open the possibility to limit the need of a bulky high - end us systems in interventional rooms . 
more patients and more cases are necessary to verify safety of the new tablet us used in interventional procedures . compliance with ethical standards conflict of interest alessandro radaelli and stephanie schampaert declare their relationship of employee with philips . 
there was no significant difference at baseline between responders ( n 12 ) and non - responders ( n 4 ) , nor between ned ( n 11 ) pd patients ( n 5 ) , in adc values and cho / h2o ratio . 
the standard treatment has been based on surgery for figo ( international federation of gynaecology and obstetrics ) clinical stages not greater than iia , and on non - surgical therapies ( chemoand / or radiotherapy ) for stages iib and higher . 
the existence of in vivo 1 3 radiol med ( 2016 ) 121 : 838846 biomarkers able to predict the prognosis and response to treatments of advanced cervical cancer would allow ineffective treatments , frequently associated with increased toxicity and development of drug resistance to be stopped , and to avoid delays in starting alternative , potentially more effective , therapies . 
by combining detailed 3d anatomical maps with functional information , such as metabolic information about tumours , mr offers multiparametric approaches in clinical oncology to further improve in vivo tissue characterisation [ 2 ]  . 
the application of diffusionweighted imaging ( dwi ) appears particularly effective , as it provides contrast between normal tissues and tumoural lesions based on differential proton diffusion , that is influenced by cell density , and it has been proposed as possible tool to monitor and predict treatment response [ 3 , 4 ]  . similarly , mr spectroscopy ( mrs ) provides chemical information about tissue metabolites [ 5 ]  . 
although there is no tumour - specific mr - visible metabolite per se , numerous studies have reported increased levels of choline - containing compounds in cancerous tissues , as a marker of increased membrane turnover or higher cellular density [ 6 ] , and decreased choline levels in response to therapy [ 710 ]  . the purpose of this study was to prospectively assess whether adc values and choline levels within cervical cancers before , during , and after non - surgical therapy are predictive of tumour response . patients and methods patients as for institutional practice approved by the ethical committee , patients candidate to non - surgical therapies for cervical cancer ( neo - adjuvant chemotherapy , radiotherapy or concomitant chemo - radiotherapy ) undergo an mr examination before starting therapy ( initial mr ) , an mr at the end of therapy ( final mr ) and , according to clinical conditions , a mid - therapy mr examination ( mid - therapy mr ) to monitor the response and , if appropriate , to tailor the rt treatment . 
patients undergoing an mr examination at our institution for staging of cervical cancer , during the period between 25 / 10 / 2010 and 12 / 07 / 2011 , who were candidates to non - surgical therapies , were prospectively enrolled in this study . 
clinical practice for patients included in this study was not altered and informed consent was obtained from all individual participants included , to undergo the mr examinations as well as to the use of anonymized clinical and imaging data for scientific and / or educational purposes . for each patient , the following data were recorded on an excel spreadsheet file ( microsoft office excel 2010 , richmond , usa ) : date of the mr examinations ; age of the patient ; histological diagnosis obtained from pre - therapy biopsy ; type of therapy ( chemotherapy , radiotherapy , or chemo - radiotherapy ) , date of start and end of therapy ; clinical figo staging , according to the revised figo staging [ 11 ] ; mean adc values ( as described in the adc values measurement section ) for each mr examination where this value was assessable ; tumour volume of the cervical lesion at each mr ; and choline / h2o peak ratio at initial and mid - therapy mr . 
according to the results at the end of therapies , patients were divided into two groups : responders ( showing reduction or disappearance of the disease ) and non - responders ( showing increase of lesion size or appearance of distant metastases )  . 
in addition , axial dwi images were acquired at the following imaging parameters : 40 slices ; 5.0 mm ; transversal orientation ; 340 mm voxel 3.0 fov ; slice thickness 5 mm ; tr 6000 ms ; te 68 ms ; averages 4 ; ipat factor 2 ; bandwidth 1446 hz / px ; epi factor 69 ; and 5 diffusion weightings ( b values : 0 ; 50 ; 250 ; 500 ; and 900 s / mm2 )  . 
mean and standard deviation ( sd ) of adc values were recorded and used to calculate overall adc mean and sd for the entire tumour volume . if there was no residual tumour at mid - therapy and / or final mr , the dwi was not assessed . 
when , following therapies , there was remnant of the tumour ( partial response ) or larger tumour ( no response ) , the rois were traced on each slice to cover the entire tumour volume at that time - point . tumour volumes were calculated from the regions of interest ( rois ) drawn around an intermediate signal - intensity cervical mass on t2 - w axial scans ( by multiplying total roi area by slice thickness )  . mr spectroscopy 15 mr spectroscopy was performed with and without water suppression using a point resolved single - voxel spectroscopy sequence , tr 2000 ms , te 135 ms , and 192 averages . 
an additional acquisition without water suppression was acquired as reference spectrum for post - processing total mrs data acquisition took about 15 m if the manual shimming did not allow obtaining a water peak line width less than 20 hz , the mrs acquisition was considered unreliable . after fourier transform , post - processing using the manufacturers software baseline and phase correction were performed . 
the ratio between the area under the choline peak ( cho ) at 3.2 ppm on the water suppressed spectra and the area of the unsuppressed water signal was calculated taking the water peak as internal standard . patient and tumour characteristics of the study population were expressed as median and range for continuous variables and as frequency and percentage for categorical variables . baseline values of adc and cho / h2o at the initial mr were compared between responders and non - responders , as well as between patients with ned and pd , using the non - parametric wilcoxon two - sample test . 
 the analyses were performed using the sas software version 9.2 ( sas institute inc . , cary , usa )  . results patients our study cohort was comprised 16 female patients ( median age 53 years , range 3082 ) with cervical cancer . 
the mid - term mri was performed after two cycles of chemotherapy in the two patients treated with neo - adjuvant chemotherapy ; after 1 week of radiotherapy in the patient treated with only radiotherapy , mainly during the second week of treatment for the 13 patients treated with concomitant chemo - radiotherapy . 
data of mid - therapy mr were available for 15 / 16 patients , because 1 patient ( with stage iia disease , treated with concomitant chemo - radiotherapy ) showed a complete response already at the mid - term mr , and therefore , there was no lesion where to trace rois neither for dwi assessment nor for tumour volume . 
 data at final mr were available for 5 / 16 patients , because at that time , only 5 patients still showed a residual tumour where to assess dwi and tumour volume . 
these patients were 1 - stage ib2 who underwent neo - adjuvant chemotherapy ; 1 - stage ib2 who underwent chemo - radiotherapy ( this was a non - responder and showed pd ) ; and 3 - stage iiib who underwent chemo - radiotherapy , 2 of which were responders , and 1 was a non - responder and showed pd . 
in the four non - responders , the adc increase was no significant ( p value : 0.25 ) discussion in this prospective study , we investigated whether mr spectroscopy and dwi - mri can be used as early response predictors in cervical cancer patients who received non - surgical therapies ( chemoand / or radiotherapy )  . 
early knowledge of response to treatment would be clinically useful to enable an early change of treatment , to avoid unnecessary toxicity or prolonged ineffective treatment in non - responding patients . magnetic resonance spectroscopy ( mrs ) is an application of magnetic resonance that has the ability to provide chemical information about tissue metabolites . 
while the conventional mri shows morphologic anatomy by detecting the nuclear magnetic resonance signal of water in tissues , mrs depicts the resonance spectra of chemical compounds other than water , allowing for a representation of the molecular composition of tissues . 
initially developed for neurological applications , the scope of mrs has then been expanded to include research in oncology , focusing on tumour diagnosis , and on its potential role in evaluating response to therapy , in both preclinical [ 1214 ] and clinical studies [ 8 , 10 , 1517 ]  . 
showed that mrs may characterize gynaecological malignancies and found that a choline peak was present in 8 out of 11 women with cervical cancer ( 73 % ) [ 18 ]  . 
although there were no significant differences between the neo - adjuvant chemotherapy and the control groups in tumour volume , the reduction in triglyceride was slightly significant ( p 0.05 ) , but no survival advantage was seen [ 20 ]  . in our study group , the evaluation of variation of cho / h2o ratio before and during therapies did not show significant difference in percent variations in responders and non - responder patients . 
who reported reduction in peak values of choline with tumour regression and proposed the possibility of its integration with other tools [ 22 ]  . based on these conflicting results , the role of in vivo mrs as an early predictor of response for cervical cancer is limited and its value remains to be assessed in larger studies or for processes to be improved . dw - mri is a technique sensitive to the microscopic motion of water molecules and allows for non - invasive characterization of biological tissues based on their water diffusion properties [ 23 , 24 ] , that reflect tissue cellularity and the integrity of cellular membranes . 
dw - mri can be used to characterize highly cellular and acellular regions of tumours , to differentiate cystic from solid regions , as well as to differentiate changes in cellularity within the tumour over time . initial studies of dw - mri focused on brain malignancies , noting increases in adc values following treatment , which have also been demonstrated in extracranial tumours . 
in hepatocellular carcinoma , a significant adc increase was noted in 6 patients after radioembolisation [ 26 ]  . in cervical tumours , the mean adc was found to increase significantly following chemo - radiotherapy [ 27 , 28 ]  . 
in a prospective study evaluating dwmri as a biomarker of early response in 20 women receiving chemo - radiotherapy for advanced cervical cancer , adc values as well as the increase in adc after 2 weeks of therapy was found to significantly correlate with clinical as well as with the conventional mr response [ 30 ] similarly , das et al . 
demonstrated that adc can be used as a predictor of early pathological response [ 31 ]  . in our cohort , adc at initial mr , as well as percent variation of adc between initial , mid - therapy , and final mr , did not show significant difference between responders and non - responders . 
however , the percent variation of adc between initial and mid - therapy mr was > 27 % ( going as high as 44.5 % ) , and > 29 % ( going as high as 74 % ) between the initial and final mr , only in responder patients . 1 3 844 radiol med ( 2016 ) 121 : 838846 fig . 
2 50 year - old female patient with figo stage iiib squamous cell carcinoma who underwent chemo - radiotherapy : axial t2 - weighted image of the cervix at the staging mr shows the pretherapy cervical cancer ( a )  . 
dwi at b 0 ( b ) matched with the t2 - weighted image was used to trace the roi that was then applied to the corresponding image of the adc map ( c ) ; mr spectroscopy at baseline showed a peak of choline ( d )  . 
this lesion responded to therapies showing at second mr examination reduction of the volume on t2 - weighted images and increase of the intra - lesion proton diffusion ( e ) ; while reduction of cho / h2o ( 11 % ) was not significant our group of patients underwent at least 4 years of follow - up , and this permitted a further division of patients according to outcome . 
although different treatments may justify different results , in this study , group 13 / 16 patients underwent the same treatment ( concomitant chemo - radiotherapy )  . the major limitation of this study is the small number of patients included . 
however , according to our institutional tumour registry ( ieo tumour registry ) , during the period comprised between 2000 and 2011 , 875 patients ( which means about 80 / year ) were treated at our institution for cancer of the uterine cervix . 
considering that the recruitment period was 8 months ( which means an approximate access of 53 patients ) and that the percentage of locally advanced stages is about 36 % [ 32 ] , and considering that a mandatory inclusion criterium was to perform all the mr examination at our institution , it was not realistically possible to include more patients . 
a more powerful study in a reasonably short time to minimize variations in treatment and in mr technique would have required a multicentric study , which would introduce inter - site variabilities in the comparisons of mrs and adc values . 
in light of the low resulting variability , our results suggest that any multicentric study should focus on characterizing adc as a biomarker , and further effort should be dedicated to improving mrs sensitivity . furthermore , the same method to trace the rois over slices was applied to all examinations thus ensuring an optimal intra - patient comparison and consistency of dwi comparison within the cohort . another limitation is that most of the patients in this study were responders , which might lead as well to a reduced statistical power . 
however , the percentage of responder patients in this study cohort ( 12 / 16 ; 75 % ) reflects the objective response rate reported in the recent literature for cervical cancer patients treated with neo - adjuvant chemotherapy and surgery ( 84 % ) , with overall survival of 72.8 % [ 33 ] and an objective response rate of 67 % for patients treated with concurrent chemo - radiotherapy . 
however , the evaluation of a weighted mean of adc values has been demonstrated to better represent the heterogeneity of tumoural tissue [ 34 ]  . in conclusion , functional mri continues to evolve for cervical cancer . 
baldassarre3 gm giuseppetti1 received : 24 april 2015 / accepted : 23 may 2016 / published online : 2 july 2016 italian society of medical radiology 2016 abstract mammography is the gold standard for detection of early breast cancer and it is still the only diagnostic tool which shows reduction of the mortality from that . 
250 patients ( group a ) had been operated for breast cancer and 250 patients ( group b ) were healthy woman submitted to mammography according to the guideline for early detection of breast cancer . 
the source of errors amongst the fn were in 42 % of cases due to perception , in 15 % to interpretation , in 10 % to subtle / unusual lesion characteristics , in 9 % error for satisfaction of search , in 7 % to inherent limitations of mammography , in 4 % to poor technique and 13 % for inadequate clinical management . 
to reduce it , it is necessary to have a dedicated multidisciplinary staff and adequate equipment and workloads . keywords mammography diagnostic errors breast neoplasms introduction the technological development and the improvement of the diagnostic techniques allowed a significant increase in early diagnosis of breast cancer and consequently the improvement of the survival rate due to a prompt and less extensive surgery . 
the mammography is still considered the gold standard for detection of early breast cancer and it is still the only diagnostic tool which shows reduction of the mortality from that [ 1 ]  . 
the mammography has high sensitivity and specificity ( 92 and 97 % , respectively ) [ 2 ] and this can be improved by the use of complementary ultrasound , especially in case of dense breasts [ 3 ]  . 
according to that , studies of forensic medicine have shown that the greatest number of delayed or incorrect diagnoses can be associated with diagnostic errors related to breast and colon carcinomas [ 4 ]  . in screening programs the fn can be hidden behind the wider concept of interval cancer ( ic ) which is a neoplasm arose in the period of time between two screening mammograms . 
the european guidelines 1 3 radiol med ( 2016 ) 121 : 828833 table 1 radiological sign in all malignant lesions and false negative mammograms opacity ultrasound findings calcifications architectural distortion opacity and calcifications ultrasound findings and calcifications 2 % n : 0 architectural distortion and calcifications n : 7 3 % n : 3 architectural distortion and opacity 0 % n : 1 malignant lesions false negative n : 65 26 % n : 17 33 % n : 58 23 % n : 1 n : 56 22 % n : 14 27 % n : 35 14 % n : 11 21 % n : 24 10 % n : 5 recommend that the rate of ic classified as screening error should not exceed 20 % [ 7 ]  . 
in literature , the fn rate is analyzed primarily within the screening programs , it also represent an event that occurs in breast clinic with an incidence not well defined . 
the european guidelines also recommend the review of fn as an essential part of the radiological audits to reduce diagnostic errors and decrease the number of missed breast cancers [ 7 ]  . failure to correctly identify or characterize the breast cancer can be determined by intrinsic factors related to the imaging tool ( i.e. , reduction of sensitivity and specificity of mammography in dense parenchyma ) , the type of breast lesion ( i.e. , minimal features of malignancy or slow growth of the lesion ) , technical factors ( i.e. , incorrect positioning or inadequate technical parameters ) , operator related errors ( i.e. , incorrect interpretation , perception error ) and happy eye syndrome , when the detection of an anomaly interfere with the detection of other possible signs of malignancy [ 810 ]  . the aim of this study is to analyze the missed breast cancer in breast clinic and to compare the results with the literature , evaluating the possible causes of error to reduce materials and methods a blind retrospective review of 500 mammograms performed in the breast imaging clinic in our hospital in a 3 years period ( from january 2008 to december 2011 ) was carried out by two radiologists with different level of experience ( i > ii )  . 
if we defines as expert reader the radiologist with more than 5 years of practice mammography , with more than 18 , 000 total read mammograms and 5000 mammograms read in a year , only i reader can be called expert reader . 
the mammograms were randomly selected between our exam data base in order to have 250 patients ( group a ) with known breast cancer treated by surgery and 250 healthy controls ( group a ) who underwent mammogram according to the guideline for early detection of breast cancer . 
a specific chart was used for the review of the mammograms ; the chart is made completely anonymous through the use of an identification code for the examination and for the patient . 
at the top the chart must be reported the results of mammography : negative ( no change to merit investigation ) , doubt ( with abnormalities of undetermined significance , need further diagnostic study ) or positive ( presence of malignant alterations )  . 
at the bottom of the chart there is a division of the breast into quadrants to precisely define the point of the possible injury and a box to add a description of the characteristics of the lesion and of the breast . 
each radiologist read all mammograms and then the mammographic findings were classified in negative , minimal sign ( additional diagnostic examination are indicated ) and positive ; prior mammograms were always available for comparison . 
the analyzes were conducted using microsoft office excel 2007 . the request of approval for personal data processing was waived by the ethics committee given the retrospective nature of the study . results the study included 500 patients , 250 patients ( group a ) had been operated for breast cancer and 250 patients ( group b ) were healthy woman submitted to mammography according to the guideline for breast cancer prevention . within group a , 138 ( 55 , 2 % ) were true missed cancer ( interpreted as negative by both readers ) , 51 ( 20 , 4 % ) errors or false negatives , while in the remaining 61 cases ( 24 , 4 % ) were identified minimal sign . 
in group b , 204 cases ( 82 % ) were interpreted by both radiologists as negative ( true negatives ) , while 46 ( 18 % ) were doubt . from the analysis of our cases was found that the type of parenchyma in which false negatives occur more frequently is the micronodular ( 45.3 % ) , followed by fibroadipose ( 41.5 % ) and dense fibroglandular parenchyma ( 13.2 % ) , with a statistically significative difference between the subgroups ( p < 0.05 for fn versus all malignant lesion ; p < 0.01 for fn vs true interval cancer and minimal sign subgroups )  . 1 3 830 radiol med ( 2016 ) 121 : 828833 fig . 
opacity with irregular margins and architectural distortion at qse ; the review has highlighted the presence of small opacity at qse , not perceived by the radiologist we evaluated the radiological sign that occurred in malignant lesions , and it was found that the tumor was presented as opacity in 26 % , ultrasound findings in 23 % , calcifications in 22 % , distortion of the parenchyma in 14 % , with a combination of opacity and calcifications in 10 % , calcifications with ultrasound findings in 2 % , distortion of the parenchyma and calcifications in 3 % . 
we found that the error occurs primarily in micronodular breasts compared to fibro - adipose parenchyma , mainly due to the presence of most glandular component ; the low rate of false negatives in the dense breasts can be due to the fact that even in retrospect this type of parenchyma remains poorly assessed and interpretable with the mammography . 
rounded opacity with calcification , that present slow growth in different controls additional signs that capture attention , leading to the suspension of the search or interfering with the detection of other signs of malignancy [ 8 , 9 ]  . another important cause of error is related to wrong clinical management , therefore , even when the lesion is successfully identified , errors may arise in clinical management or in false negatives in second level examinations ( i.e. , cytology , stereotaxis , etc . ) , leading to diagnostic delay , which highlights the importance of continuity in the clinical management of patients and the collaboration of all professionals figures who care for them . to reduce the number of diagnostic errors , they must be analyzed and optimized on all the rings that make up the diagnostic breast chain ; it is required adequate equipment such as digital mammography system supported by adequate diagnostic workstation , performing ultrasound transducers with high - frequency surface ( 10 - 13 mhz ) , technical and medical staff properly trained and dedicated to the study of breast imaging , adequate working areas characterized by correct brightness [ 14 , 15 ]  . 
a further aid in the reduction of errors , particularly in dense parenchyma in which the overlap of tissue can reduce the visibility of the lesion , can be given by the tomosynthesis , an emerging diagnostic technique , that allows to obtain tomographic images of a volume of tissue , by the acquisition of multiple projection exposures , obtained with a digital detector from a mammographic x - ray source which moves over a limited arc angle , with a principle similar to the old stratigraphy [ 1618 ]  . 
5 satisfaction of search ; the detection of an anomaly in left breast ( a ) interfere with the detection of signs of malignancy in right side , seen in the next control ( b ) radiol med ( 2016 ) 121 : 828833 and detect the associated findings ( i.e. , dilated ducts , vessels or micro - calcifications around the mass ) [ 19 ]  . 
also the double - reading of mammograms could be considered as a method for the reduction of errors : as highlighted in the screening programs , that determines a significant increase in diagnostic accuracy , but unfortunately has drawbacks , such as the higher cost and the increase of the times of reporting . radiologists dealing with breast pathologies must be properly and regularly trained in this field with a continuously updated preparation , which affects breast disease in its totality [ 2022 ]  . 
in particular , it is needed a high level of expertise and competence in all breast imaging techniques and interventional procedures , to use them correctly with the appropriate diagnostic workup . 
diagnostic errors should also be audited and reviewed collegially on a regular base to draw an important professional enrichment . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . statement of human rights for this type of study formal consent is not required . statement on the welfare of animals this article does not contain any studies with animals performed by any of the authors . radiol med ( 2016 ) 121 : 867872 doi 10.1007 / s11547 - 016 - 0668 - 8 radiotherapy delineation of the larynx as organ at risk in radiotherapy : a contouring course within rete oncologica piemontevalle daosta network to reduce inter and intraobserver variability edoardo petrucci2 cristina piva1 valeria casanova borca2 domenico cante1 piera sciacero1 maurizio bertodatto1 caterina marta1 pierfrancesco franco3 monica viale4 giovanni la valle5 maria rosa la porta1 oscar bertetto4 on behlaf of rete oncologica piemontevalle daosta received : 31 march 2016 / accepted : 4 july 2016 / published online : 15 july 2016 italian society of medical radiology 2016 abstract aims to evaluate the usefulness of a contouring course in reducing interand intraobserver variability in the definition of the larynx as organ at risk ( oar )  . methods within the rete oncologica piemonte - valle daosta network , a contouring course focusing on larynx delineation was proposed . 
the contoured volumes obtained before and after the course were compared using descriptive statistics ( mean value , standard deviationsd , and coefficient of variationcov ) of volumes and maximum diameters . 
conformity index ( ci ) , dice coefficient ( dc ) , and percentage of overlap were used to evaluate the spatial accuracy of the different volumes compared to the reference . 
further analysis regarding the variation in the centre of mass ( com ) displacement was performed . results the mean volume was 40.4 cm3 before and 65.9 cm3 after the course , approaching the reference value . 
other specific educational activities may further increase the quality of radiation therapy contouring in this setting . keywords contouring course larynx radiotherapy introduction radiotherapy treatment on head and neck regions is frequently complicated by late effects as swallowing dysfunction , dysphagia , and dysphonia [ 1 , 2 ]  . 
nevertheless , there is no evidence in the literature data regarding the most appropriate delineation approach for this structure on planning computed tomography ( ct ) images and the consequent relationship between the absorbed dose and chronic dysfunctions [ 4 , 6 , 7 , 10 , 1316 ]  . 
the aim of this study was to evaluate the interand intraobserver variability in larynx delineation prior to and after a dedicated course targeted to radiotherapy technicians ( rtts ) to test whether this educational tool may be effective in increasing homogeneity during the contouring process . methods a contouring course endorsed by the rete oncologica piemonte - valle daosta network has been organized and 1 3 868 fig . 
1 graphic illustration on axial , coronal , and sagittal planes of the reference larynx volume ( vref ) , including glottic and supraglottic areas and a single pair contours , defined by one observer before ( vbefore ) and after ( vafter ) the contouring course radiol med ( 2016 ) 121 : 867872 held at the radiotherapy department of ivrea , a.s.l. 
to4 , with a specific focus on larynx delineation as an organ at risk ( oar )  . shows an example on axial , coronal , and sagittal planes of the reference volume and the two contours delineated by one observer , before and after the course . before the beginning of the contouring course , 26 rtts trained to contour organs at risk ( oars ) during their professional activity were requested to delineate the larynx structure as oar in a clinical case of head and neck tumour involving the oropharynx . 
at first , we used descriptive statistic [ 18 ] ; minimum , maximum , and mean values , standard deviation ( sd ) , and coefficient of variation ( cov ) were calculated for each structures data ( volumes , diameters , and centre of mass coordinates ) before and after the course . 
cov , defined as sd - to - mean ratio , provides a measure of dispersion of the distribution in a single number and it can be correlated with other parameters of interest . 
thereafter , we evaluated dice 1 3 radiol med ( 2016 ) 121 : 867872 coefficient ( dc ) and percentage of overlap among the reference structure and each volume before and after the training . 
dc is defined as the ratio between two times the intersection of the structure and the reference volume with the union of the two ; a value of 0 indicates no agreement between the structures , while a dc of 1 represents 100 % agreement . 
conformity index ( ci ) [ 18 , 19 ] assesses the correlation of the entire set of data , in our case two samples , before and after the training , and it is calculated as the ratio of the global intersection between the volumes with respect to the total union . 
3 box - and - whisker plots for laterolateral ( x ) , anteroposterior ( y ) , and caraniocaudal ( z ) diameters before ( 0 ) and after ( 1 ) the contouring course in fig . 
a two - paired wilkoxon test has been carried out over the volumes samples ; p value of 0.0001 shows a significantly difference between the set of data . discussion the radiotherapy treatment for head and neck cancer can be frequently complicated by swallowing dysfunction , xerostomia , dysphonia , and soft tissue fibrosis , affecting fig . 
4 box - and - whisker plots for laterolateral ( x ) , anteroposterior ( y ) , and caraniocaudal ( z ) coordinates of the centre of mass before ( 0 ) and after ( 1 ) the contouring course 1 3 870 radiol med ( 2016 ) 121 : 867872 the general dimension of quality of life [ 13 ]  . 
 the larynx belongs to the structures involved in the complex mechanism of swallowing , respiration , and phonation [ 36 ] , and consequently , its definition as oar is fundamental . 
 the entity of this uncertainty depends on several factors , such as the type and quality of images used for delineation , the experience and professional background of observers , and the existence of tools to help and drive the contouring process . 
contouring guidelines can lead to a higher precision in larynx delineation [ 9 , 20 ] , as well as a reduction in the interobserver variability with consequent implications on the dose distribution to oars . 
moreover , atlases of radiologic anatomy , case examples , and contouring courses could further improve the accuracy in volume delineation . the present study was designed with the aim of assessing the intraand interobserver variability among a group of rtts , experienced in oars contouring , in the delineation of the larynx in a single case of head and neck cancer . 
the contouring course was performed for radiotherapy technicians , because in the last years , the role of rtts has become of great importance in oars definition in our department to relieve the workload of radiation oncologists . 
some studies evaluated the variability in target volume delineation using descriptive statistics and parameters describing the distribution of volumes and diameters , such as mean , standard deviation , range , and dispersion of the distribution , such as cov [ 2128 ]  . 
the majority of studies deal with approaches that describe the overlapping area between contoured volumes , using metrics , such as ci and dc [ 2224 , 2631 ]  . 
moreover , when moving to 3d representation , metrics , such as variation of the com , allow to evaluate the volume displacements in space [ 27 , 32 , 33 ]  . for our study purposes , we chose to evaluate interand intraobserver variability using some descriptive statistics related to geometrical measures , variation of the com displacement , percentage of overlap , dc , and ci . 
even the ci showed a low level of correlation between the volumes in the sample before the training ( 0.06 ) , demonstrating the necessity of a single and clear contour method . as previously said , the interobserver variability in oars definition can be limited . 
 [ 34 ] conducted a study to assess whether consensus guideline - based atlas - based auto - segmentation ( abas ) reduces interobserver variation and improves dosimetric parameter consistency for oars in nasopharyngeal carcinoma , showing a significant interobserver variation for all oars in manual contouring . 
after the contouring course , compared to the reference volume , there were no major variations in diameters yet , but with lower values of standard deviation and cov between the observers . 
mean value of centre of mass displacement even showed an improvement with respect to the first sample , approaching the reference value of about 3 mthe lower variation was confirmed by an increased percentage of intersection , with a mean value of 93.83 % ( range 6899 % )  . 
wilkoxon test on structures volumes underlines the differences between the samples ( p 0.0001 ) and at the same time highlights the usefulness of the training course . referring to anatomical structures , we observed that before the training , the most important deviations concerned the craniocaudal volume extent . 
some observers contoured beyond the tip of epiglottis that may be considered the upper boundary of supraglottic larynx and / or too far below the caudal edge of thyroid cartilage . 
after the contouring course , a better homogeneity between volumes resulted in right craniocaudal delineation and in a major adherence with the cartilaginous structures . in conclusion , this study showed that , despite the observers experience , variability in larynx definition as oar among observers compared to a reference volume was significant . 
t1 relaxation time and adc value of liver were measured by three distinct roi protocols ( the whole left lobe liver , the whole right lobe liver and the individual rois )  . 
interobserver variability for the t1 relaxation times and adc values by the three distinct roi protocols was analyzed by calculating the icc . results t1 relaxation time measurements by the three distinct roi protocols on severe fibrosis stage were significantly higher than the relative values on mild fibrosis stage . 
the more reproducible results were obtained when measuring t1 relaxation time of the whole right lobe liver and the individual rois . keywords gadoxetic acid t1 relaxation time magnetic resonance imaging apparent diffusion coefficient liver fibrosis observer variation introduction chronic liver diseases represent a major public health problem , accounting for significantly morbidity and mortality worldwide [ 1 ]  . 
it can lead to hepatic fibrosis , cirrhosis , end - stage liver disease , and portal hypertension and to the development of hepatocellular carcinoma ( hcc ) [ 2 , 3 ]  . 
the early detection of fibrosis is important for determining disease progression and postponing the evolution of chronic hepatitis into cirrhosis via the implementation of prompt and 1 3 822 radiol med ( 2016 ) 121 : 821827 specific treatment . 
the patient , who should be monitored the treatment effect , will have liver biopsy repeatedly , and it will increase the rate on complications ( haemorrhage in 0.3 % of patients and mortality in 0.01 % ) [ 9 ]  . 
now the noninvasive methodologies for the assessment of fibrosis have developed , such as the indirect markers of liver injury , computed tomography ( ct ) , transient elastography ( te ) and magnetic resonance imaging ( mri ) [ 11 , 12 ]  . 
 [ 14 ] showed that hepatic mrdwi played a key role in evaluating liver fibrosis following transcatheter arterial chemoembolization ( tace ) with low doses of chemotherapy . gadoxetic acid ( primovist ; bayer - schering pharma ag , berlin , germany ) is a mr imaging contrast medium that is developed for evaluating the hepatobiliary syste many studies have showed that it is useful for the detection and characterization of focal liver lesions , hccs particularly [ 15 , 16 ]  . 
previous studies showed that patients with liver dysfunction presented with reduction of liver parenchymal enhancement using gadoxetic acid - enhanced mr imaging on hepatobiliary phase ( hbp ) by the methods of direct measurement of liver parenchymal signal intensity or calculation of perfusion parameters [ 17 , 18 ]  . an alternative approach to direct measurement of signal intensity and perfusion imaging would be to evaluate t1 relaxation time of liver parenchyma , which was directly correlated with the concentration of gadoxetic acid in theory , more reliable and less subjective . 
to our knowledge , evaluation of gadoxetic acid - enhanced mr imaging for hepatic fibrosis staging has been reported both in animal models and patients [ 19 , 20 ]  . 
it is a continuous process and it maybe distributes unevenly in the whole liver . thus , the purpose of our study is to evaluate the potential biomarker for liver fibrosis staging , and compare the results of t1 relaxation time with dwi - adc value and assess the influence of roi positioning on interobserver variability , t1 relaxation time and dwi - adc value on gadoxetic acid - enhanced mr imaging . materials and methods patients this retrospective study was approved by institutional review board of our hospital and the requirement for informed consent was waived . 
exclusion criteria consist of ( a ) non - availability of pre - treatment gadoxetic acid - enhanced mr imaging using t1 mapping ; ( b ) difficulty to measure the adc / t1 mapping values because of motion artifact ; ( c ) diffuse hepatic lesions ; ( d ) previous liver resection . 
for t1 mapping with syngo mapit , a dual flip angle 3d gradient echo sequence with volumetric interpolated breath - hold examination ( vibe ) was performed after injection of gadoxetic acid ( primovist ; bayer - schering pharma ag , berlin , germany )  . 
a parallel imaging technique ( r 2 ) was performed using generalized 1 3 radiol med ( 2016 ) 121 : 821827 autocalibrating partially parallel acquisition ( gappa )  . 
in all patients , 0.025 mmol / kg body weight of gadoxetic acid was injected manually at about 1 ml / s , by one investigator through a 20 - gange intravenous catheter placed in a cubical or cephalic veimmediately afterwards , a 20 ml saline flush was administered at the same injection rate . 
 t1 mapping was obtained at 20 min after gadoxetic acid administration for hbp . three scan trace free - breath dw images were obtained prior to gadoxetic acid injection using a single - shot spinecho echo planar imaging sequence ( tr / te , 3200 / 56 ms ; slice thickness , 5.5 mm ; matrix size , 84 128 ; fov , 380 300324 mm ) with a b value of 0 and 500 s / mm2 . 
 400 a parallel imaging technique ( r 2 ) was performed using gappa . imaging evaluation quantitative t1 relaxation time maps and adc maps were derived automatically on a voxel - by - voxel basis . 
the mr data sets were transferred to a workstation ( leonardo , siemens , erlangen , germany ) to measure the t1 relaxation time and adc value of the liver parenchyma using operator - defined roi . 
criteria for the fibrosis stages were as follows : f0 , no fibrosis ; f1 , fibrous portal expansion ; f2 , bridging fibrosis ; f3 , bridging fibrosis with architectural distortion ; and f4 , cirrhosis [ 18 ]  . a total of 150 patients , who underwent partial hepatectomy , were included finally . 
and the pathological results were as follows : hepatocellular carcinoma , n 89 ; intrahepatic cholangiocarcinoma , n 15 ; cirrhosis , n 9 ; colorectal liver metastases , n 2 ; degenerative nodule , n 3 ; hepatocellular adenoma , n 2 . 
patients were classified as mild fibrosis stage ( f score 2 ) and patients were classified as severe fibrosis stage ( f score 12 ; inflammatory nodules , n 2 ; angiomyolipomas , n 3 ; focal nodular hyperplasia , n 13 ; hemangioma , n 3 )  . effect of roi methods the mean values of t1 relaxation time and dwi - adc were displayed in table 1 for the mild fibrosis stage and severe fibrosis stage of each respective roi protocol . 
1 af examples of placement of regions of interest ( roi ) in the liver parenchyma on t1 mapping to measure the t1 relaxation time by the whole left lobe liver ( a ) , to measure the t1 relaxation time by the whole right lobe liver ( b ) and to measure the t1 relaxation time by individual rois ( c )  . 
examples of placement of regions of interest ( roi ) in the liver parenchyma on adc map to measure the adc value by the whole left lobe liver ( d ) , to measure the adc value by the whole right lobe liver ( e ) and to measure the adc value by individual rois ( f ) were significantly higher when measured by means of the whole left lobe liver ( p 0.035 ) , the whole right lobe liver ( p 0.002 ) and the individual rois ( p 0.0006 ) , compared with the relative values on mild fibrosis stage . 
 the mean adc values on severe fibrosis stage showed no significantly different when measured by means of the whole right lobe liver ( p 0.057 ) and the individual rois ( p 0.10 ) , compared with the relative values on mild fibrosis stage . 
 however , by means of measuring the whole right lobe liver and the individual rois , the mean adc values on mild fibrosis stage showed no significantly different with the relative values on severe fibrosis stage . 
 [ 21 ] indicated that the contrast enhancement index with gadoxetic acid - enhanced mr imaging was an efficient biomarker in the staging of liver fibrosis and was more accurate than adc values . 
therefore , we believed that t1 relaxation times could be differential from mild and severe fibrosis stage , which was very useful for the patients both on treatment in time and follow - up effectively . 
thus , results of adc values are the lack of a well cut - off value and it is radiol med ( 2016 ) 121 : 821827 difficult to be used in clinical practice . 
also , in our study , adc values could not differentiate mild fibrosis stage from severe fibrosis stage and were relatively low for identification of severe fibrosis stage . until the end stage , the progression of fibrosis to cirrhosis has a number of sequelae . 
first it will distort hepatic architecture and vasculature , second it will have a deleterious effect on hepatic function and the third it will increase the propensity for neoplastic transformation . 
we recommended that measuring t1 relaxation time used the roi protocols of the whole right lobe liver and the individual rois . another interesting finding was that measuring t1 relaxation time in patients by means of the three distinct roi protocols was more reproducible . 
another new technique called intravoxel incoherent motion mr imaging ( ivim ) has been used , which is a measurement of numerous points of adc at different b values [ 25 ]  . in conclusion , t1 relaxation time measurements by means of the three distinct roi protocols on gadoxetic acid - enhanced mr imaging were a potential biomarker in staging of hepatic fibrosis , which were more accuracy than dwi - adc measurement . 
the frequency of quadrant involvement , retroareolar involvement , accompanying abscess , ductal ectasia , skin thickening , breast edema , extension to pectoral muscle , and presence of fistula were investigated . 
the mean apparent diffusion coefficient ( adc ) values for lesions , contralateral normal breast parenchyma , pectoralis major muscle , and sternum were measured in patients with invasive cancers ( n 42 )  . 
fatih , istanbul , turkey 2 department of radiology , institute of oncology , istanbul university , istanbul , turkey 3 department of surgery , istanbul faculty of medicine , istanbul university , istanbul , turkey results the findings of idiopathic granulomatous mastitis on mri were total ( in all quadrants ) or wide ( 2 or 3 quadrants ) in 30 ( 71.5 % ) , retroareolar space involvement in 28 ( 66.7 % ) , skin thickening in 21 ( 50 % ) , breast edema in 21 ( 50 % ) , extension to pectoral muscle in 18 ( 42.9 % ) , accompanying abscess formation in 33 ( 78 % ) , ductal ectasia in 17 ( 40.5 % ) , and fistulas in 13 ( 31 % )  . 
the most frequent enhancement patterns were rim enhancement in 20 ( 78 % ) in masses and clustered ring in 11 ( 48 % ) in non - mass lesions . 
early enhancement pattern of igm was obtained as slow in 29 cases ( 69 % ) , medium in 11 cases ( 26.1 ) and rapid in 2 ( 5 % ) cases . 
our results had no discriminatory power for igm versus malignant lesions for either adc values and adc ratios of normal breast parenchyma , pectoralis major muscle , and sternum . conclusion although not characteristic for idiopathic granulomatous mastitis , masses with rim enhancement or clustered - ring non - mass lesions with segmental distribution on mri are the most common features of the disease . 
it is characterized by the presence of non - caseating chronic granulomatous breast lobules , in which no microorganisms are found and all other granulomatous diseases have been excluded [ 2 , 3 ]  . 
although igm treatment is controversial , use of antibiotics or corticosteroids and wide excision of the affected tissue have been reported as options . the imaging findings of idiopathic granulomatous mastitis have a wide spectrum , and they are inconclusive for differentiating malignant and benign lesions [ 6 ]  . 
ultrasound and mammography findings of this condition have been previously reported ; however , a limited number of reports evaluated magnetic resonance imaging ( mri ) features of igm in the literature [ 610 ]  . 
diffusion - weighted magnetic resonance imaging ( dw - mri ) shows high accuracy in differentiating malignant from benign by measuring the apparent diffusion coefficient ( adc ) in breast lesions [ 11 , 12 ]  . 
also , recent studies have shown that the ratio of the adc of the lesion to the adc of the different tissues had greater sensitivity and specificity than either minimum or mean adc values , particularly for heterogeneous lesions [ 13 ]  . 
in this study , we aimed to analyze mri findings of igm and compare the mean adc values and also adcr parenchyma ( ratio of the lesion adc to normal parenchyma of the contralateral breast adc ) , adcr muscle ( ratio of the lesion adc to the pectoral major muscle adc ) , and adcr sternum ( ratio of the lesion adc to the sternum adc ) of igm with breast cancer . 
in addition , we analyzed the frequency of the involved quadrants , retroareolar involvement , accompanying abscess , ductal ectasia , skin thickening , breast edema , extension to pectoral muscle , and the presence of fistula . materials and methods patients thirty - seven patients with histologically confirmed igm who underwent breast magnetic resonance imaging between may 2014 and january 2016 were included in our study . 
forty - two women with pathologically proven invasive cancer of breast who underwent mri for different indications ( preoperative staging , evaluation of multifocal and multicentric , before neoadjuvant chemotherapy ) were included in our study for comparison . 
 patients with invasive cancers were selected from relatively younger age groups to conform with the patients with igm . scanning parameters 224 ; fov 340 mri examinations were performed on a 1.5 - t system with a dedicated four - channel phased - array bilateral breast coil ( achieva , philips medical systems , best , the netherlands )  . 
mri findings of patients with igm were classified in accordance with the american college of radiology breast imaging reporting and data system ( bi - rads ) atlas 5th edition . 
masses were evaluated in terms of shape ( round , oval or irregular ) , margin ( smooth , irregular or spiculated ) , and internal enhancement characteristics ( homogeneous , heterogeneous , rim enhancement , non - enhancing internal septation )  . 
non - mass enhancement 1 3 radiol med ( 2016 ) 121 : 857866 was described according to the distribution ( focal , linear , segmental , regional or diffuse ) and internal enhancement pattern ( homogeneous , heterogeneous , clumped , clustered ring )  . 
involvement of quadrants and retroareolar area , accompanying abscess , ductal ectasia , skin thickening , breast edema , extension to pectoral muscle , and presence of fistula were determined . 
for this , a freehand roi was drawn over the enhancing component of the lesion , avoiding areas of necrosis and partial volume effects in the peripheral part of the lesion , as determined by co - registration to images obtained with conventional sequences . 
the ratio of the mean adc value of lesion ( igm or invasive cancer ) to the mean adc value of the pectoralis major muscle ( adcr muscle ) and the ratio of the mean adc value of the lesion to the mean adc value of the sternum ( adcr sternum ) were evaluated . statistical analysis all statistical analyses were performed using spss software version 17 ( spss inc , chicago , il , usa )  . 
the frequencies quadrantretroareolar involvement were assessed , and the presence of abscess , ductal ectasia , skin thickening , breast edema , extending to pectoral muscle , fistula were also analyzed . results in this study , 42 cases of mastitis in 37 women ( mean age 8 ; range 2067 years ) were evaluated . 
t2 - weighted image with fat suppression ( a ) and t1 - weighted gadolinium - enhanced subtraction ( b ) images show ectasia and periductal enhancement of ducts ( arrow ) in central and peripheral location of the breast . 
in superior quadrant of the right breast , subtraction ( c ) image shows heterogenous and clustered ring enhancement with regional distribution , also fistula ( arrow ) is seen superior - inner quadrant of the breast . 
in diffusion - weighted image , mastitis ( arrow ) shows high signal ( e ) with low apparent diffusion coefficient value ( f ) ( 1.09 3 mm2 / s ) 10 hyperintense signal on t2 - w images , most were irregularly shaped , and borders had rim enhancement . in the kinetic analysis , the early enhancement pattern of igm was classified as slow in 29 ( 69 % ) cases , medium in 11 cases ( 26.1 ) and rapid in 2 ( 5 % ) cases . 
in 27 ( 64 % ) patients , the time - signal intensity curve revealed gradual and progressive enhancement ( type - 1 ) , and a plateau - like pattern following early contrast enhancement ( type - 2 ) in 15 ( 36 % )  . 
the mri findings are shown in table 1 . dwmri findings forty - two patients ( mean age 46 11 ; range 2465 years ) with pathologically proven invasive cancer of the breast ( invasive lobular carcinoma , 12 ; invasive ductal carcinoma , 30 ) were evaluated for the comparison of adc values and ratios . 
the adcr parenchyma , adcr muscle , adcr sternum of invasive cancer measurement compared with the adcr parenchyma , adcr muscle , adcr sternum of idiopathic granulomatous mastitis was not significant ( table 3 )  . discussion is an uncommon idiopathic granulomatous mastitis benign breast disease characterized by chronic , noncaseous , necrotizing granulomatous lobulitis with or without abscess formation . 
 [ 15 ] identified four main mechanisms that might be responsible for igm formation : a chemical reaction associated with oral contraceptive pills , an underlying autoimmune process , an underlying infective etiology that cannot be detected by current means , or an immune response to extravasated secretions from lobules . 
 granulomatous mastitis can mimic breast cancer on clinical , radiologic or cytologic examination [ 18 ]  . the mammography and us findings of this entity have been well described many times , but the mri features of igm have been reported in only a few case reports and limited series [ 610 ]  . 
 these reports demonstrated that igm has a wide spectrum of imaging findings such as ring enhancement , intensively and strongly enhanced irregular masses , and focal homogeneous enhancing masses [ 1924 ]  . 
t1 - weighted gadolinium - enhanced subtraction ( b ) image shows rim enhancement of abscesses ( arrows ) and heterogenous enhancement of mass ( star ) with segmental distribution . 
in diffusion - weighted ( d ) image , mastitis shows high signal ( arrows ) with low apparent diffu10 sion coefficient value ( e ) ( 0.85 3 mm2 / s ) due to the enhancing inflamed periductal parenchyma and microabscess . 
in this study , we found that ductal ectasia and periductal enhancement commonly accompanied igm ( 40.5 % ) ; this is a very valuable finding for differentiating igm from invasive cancers . 
we also analyzed the early phase of the curves and detected slow and medium initial enhancement of igm in almost all of our patients , that was reported not reported before . 
based on these findings , the enhancement kinetics differ significantly for igm and malignant enhancing lesions and may , therefore , be used as an aid in differential diagnosis . conventional mri features , such as signal intensity and morphologic definition , cannot accurately predict fig . 
t2 - weighted ( a ) image with fat suppression shows bilateral hyperintense parenchyma because of lactation , additionally mastitis was hypointense signal ( arrow ) in the outer - inferior quadrant of the breast . 
the pectoralis major muscle and sternum were selected as adc references because they have stable adc measurements and are not affected by hormonal changes , menstrual cycles or different breast tissue types . 
as a result , adcr values of igm were not significantly different from adcr values of invasive cancer . our study has several limitations ; this study had a retrospective design and we studied a relatively small number of patients . 
another limitation is that interand intra - observer variability was not assessed . in conclusion , masses with rim enhancement and clustered - ring appearance in non - mass lesions with segmental t2 - w t2 weighted , tsi time signal intensity curve malignancy . 
therefore , we compared the adc value of igm with breast cancer , which is the main differential diagnosis 1 3 radiol med ( 2016 ) 121 : 857866 fig . 
image integrating the pseudo - color image of adc and the axial precontrast t1 - weighted magnetic resonance images : a roi is located in the thickest layer of the pectoralis majr muscle and b sternu t2 - weighted image with fat suppression ( c ) and t1 - weighted gadolinium - enhanced subtraction ( d ) images show oval and round shaped multiple hyperintense masses with irregular rim enhancement evaluated as abscesses . 
adc values do not contribute in the diagnosis of igm . compliance with ethical standards ethical approval this article does not contain any studies with animals performed by any of the authors . 
the external evaluation and description of post - mortem phenomena ( maceration ) , record of the weight and detection and the various measurements of foetal diameters were evaluated before performing autopsy . 
pmmr can provide useful information on foetal medical conditions and result in improved diagnostic * vittorio fineschi vfinesc@tin.it 1 department of anatomical , histological , forensic and orthopaedic sciences , sapienza university of rome , viale regina elena 336 , 00185 rome , italy 2 department of radiological sciences , oncology and anatomical pathology , sapienza university of rome , viale regina elena 324 , 00161 rome , italy classification . 
the association between pmmr , post - mortem examination and related histological study of the foetusplacenta unit could help reduce the percentage of cases in which the cause of foetal death remains unexplained . 
lastly , it may allow a selective sampling of the organ in order to target histological investigations . keywords post - mortem magnetic resonance foetal and perinatal autopsy histological examination introduction multislice computed tomography ( msct ) and magnetic resonance imaging ( mri ) are being increasingly implemented in forensic pathology . 
in this regard , by analysing 57 forensic cases by neuroimaging techniques such as msct and mri and comparing the results with autopsy findings , it was observed that abrasions , contusions and lacerations of the scalp were detected by mri rather than ct [ 2 ]  . 
mri and msct were superior to autopsy in the evaluation of ventricular haemorrhage , as well as the identification of lacerations in brain tissue and brainstem injuries [ 4 ]  . these technical characteristics have resulted in the progressive use of post - mortem magnetic resonance ( pmmr ) in intrauterine foetal death of forensic interest . 
foetal death is a tragic outcome of pregnancy , aggravated by the intense emotional involvement of the mother and the whole 1 3 848 radiol med ( 2016 ) 121 : 847856 family [ 58 ]  . 
however , because of the complicated patho - physiological processes involving mother , foetus and placenta , and the fact that stillbirths often result from the interaction of different processes , univocal classifications of stillbirths are often difficult to assess [ 11 ]  . up to 35 classification systems have been developed to define stillbirth and there is no international consensus on which should be used [ 12 ]  . 
lastly , it may allow a selective sampling of the organ in order to target histological investigations [ 13 ]  . the aim of the present study is to offer our experience concerning pmmr in foetal death cases and an evaluation of the differences between the findings acquired by pmmr and by forensic autopsy in 15 foetal deaths [ 1423 ]  . materials and methods population and study design fifteen foetuses were recruited from july 2014 to december 2015 . 
clinical data are reported in table 1 . mr imaging : protocol and images analysis all 15 foetuses were studied with a pmmr examination using a magnet operating at 1.5 tesla ( siemens avanto , siemens medical solutions , enlargen , germany ) , at the department of radiological sciences , oncology and pathology of the sapienza university of rome . 
we excluded from the analyses post - mortem phenomena such as small bleeding without ventricular dilation , collapse of eyeballs , small amounts of pleural effusion , and small amounts of air in the pericardial or peritoneal cavities and in the bile ducts . 
 postmortem examination the external evaluation and description of post - mortem phenomena ( maceration ) , record of the weight and detection and the various measurements of foetal diameters ( head , thoracic and abdominal circumferences , foot and femoral lengths ) were evaluated before performing autopsy . 
 the rokitansky method was used to perform an autopsy before proceeding to the formalin fixation of organs in order to highlight fine anatomic structures more easily and to avoid any artefacts due to the pathology evaluation [ 24 , 25 ]  . results out of 15 cases examined , eight were negative for structural anatomical abnormalities and / or diseases , both in the preliminary pmmr examination and the traditional autopsy . 
in the remaining seven cases , pathological findings were detected by pmmr with corresponding results at autopsy . pmmr was particularly useful in the abnormalities of the central nervous system ( cns ) , that is one of the most difficult areas to investigate at autopsy , as the neonatal brain generally collapses once it is removed from the skull , with consequent loss of its structure . 
otherwise pmmr , having the capability to evaluate cns in situ , allowed for an accurate evaluation of the anatomy of the brain , and clearly showed normal cerebral structure and the development of the sulci and gyri . 
furthermore , pmmr permitted to detect 1 3 radiol med ( 2016 ) 121 : 847856 1 3 850 table 2 sequences used for postmortem foetal magnetic resonance study sequences slice thickness ( mm ) tr ( ms ) ti ( ms ) te ( ms ) ir delay ( ms ) radiol med ( 2016 ) 121 : 847856 body imaging coronal t2 coronal t2 spir coronal t1 ir axial t2 axial t2 spir axial t1 ir sagittal t2 brain imaging axial t2 axial flair axial t1 ir 2969 3155 7000 4000 3341 7000 2969 5531 12 , 000 7000 2850 2850 tr relaxation time , ti inversion time , ir inversion recovery , mm millimetres , ms milliseconds , spir spectral presaturation with inversion recovery , flair fluid attenuated inversion recovery fig . 
tse t2 - weighted image showed the normal positioning of foetal organs : ed : right brain , es : left brain , pd right lung , ps left lung , c heart , f liver , s stomach , ca ascending colon , cd descending colon , i small intestine , arrows pleural effusion also small amounts of cerebral haemorrhage thanks to its capability to differentiate various tissue contrasts with t1 and t2 - weighted sequences . 
otherwise , the evaluation of the lungs and of the cardiac anatomy was more difficult . lung imaging was difficult with pmmr because lung parenchymas are mostly collapsed and not contain air in stillborns , for the lack of the foetal first breath . 
however , pmmr of the lungs allowed the diagnosis of major structural lesions , as for example in the case with diaphragmatic hernia , and permitted the evaluation of normal anatomical structures appearance . furthermore , foetal cardiac structures should need additional dedicated imaging planes and thinner slices to increase sensitivity for the detection of eventual cardiac abnormalities and for example of infectious diseases such as myocarditis or small atrial or ventricular septal defects . pathological findings are reported in table 3 . 
3 case 2a , b diaphragmatic hernia with visceral dislocation discussion this study presents our experience regarding the role of pmmr in intrauterine foetus death in order to evaluate diagnostic strengths and forensic utility . 
however , we must be very cautious in the interpretation of pmmr imaging because we may run the risk of interpreting changes linked to post - mortem phenomena such as diseases of the foetus or newborn [ 26 ]  . however , pmmr provided detailed information about structural abnormalities and foetus disease processes . 
in particular , a full correspondence in negative cases and a substantial correspondence in positive cases were found . the gold standard for the diagnosis of foetal death is known to be the autopsy examination [ 2729 ]  . 
c cystic cavity surrounded by poorly developed renal parenchyma 1 3 854 radiol med ( 2016 ) 121 : 847856 the classification of foetal deaths on the basis of the duration of gestation into early ( < 20 weeks ) , intermediate ( 2028 weeks ) and late ( > 28 weeks ) [ 30 ]  . 
an autopsy and the histological examination of the foetus and placenta , sometimes accompanied by standard x - rays , have until recent time been the gold standard for the diagnosis of foetal death . on 22nd november 2014 , however , the italian ministry of health approved a diagnostic protocol on foetus death , which considers not only autopsy but also other non - conventional investigations such as pmct and genetic , cytogenetic , infectious disease tests and toxicological investigations [ 38 ]  . 
pmct , microct or pmcta may be feasible although it is likely that these techniques will be performed within already established services thanks to the involvement of all the specialists concerned : neonatologists , geneticists , obstetricians , and radiologists . 
again , feasibility of pmcta in evaluating the foetal heart is discussed by comparing the results of two access techniques : injection through the umbilical cord or ultrasound - guided needle injection directly into the heart [ 4042 ]  . we believe that in foetal death cases pmmr could be a useful tool to provide more details on brain diseases with respect to conventional autopsy [ 43 , 44 ]  . 
furthermore , it is more effective in identifying intraparenchymal blood components due to the alteration of signals compared to surrounding healthy brain tissue , this event being very frequent in foetuses or very infrequent in the case of maceration . with regard to mediastinal structures [ 45 ] , pmmr investigation is reliable with particular reference to the abnormal position of the organs and of the heart chambers , although for greater definition of some cardiac abnormalities ( such as atrial septal defect or ventricular septal defect ) dedicated sequences relating to the heart are required [ 46 , 47 ]  . 
in the literature , a recent study has shown that 3d post - mortem cardiovascular magnetic resonance ( cmr ) imaging can provide equivalent structural information to that of conventional autopsy in the majority of larger foetuses , newborns , and children [ 48 ]  . in order to investigate the lungs , pmmr proves not to be fully reliable because of the air component of the lung parenchyma , but it still enables the distinction between pleural effusion from post - mortem phenomena through the use of t2 - weighted sequences that signal static liquid . for the abdominal area , pmmr is a reliable examination in the case of anomalies and / or severe abdominal diseases and allows better classification of the disease even if unspecified [ 49 ]  . certainly , to introduce pmmr as a routine examination in forensic services , in selected cases of judicial interest , it makes it necessary to verify that pmmr will be performed within established centres in terms of specialized and pluridisciplinary competences [ 50 ]  . 
however , pmmr could be a valid and valuable preliminary test with respect to traditional post - mortem examination , although some questions remain unanswered . pmmr , however , does not completely replace conventional radiology . 
third , this study was based on a small number of cases so actually we are implementing the casistic data enrolling new cases . in conclusion , in the immediate future the association between pmmr , post - mortem examination and related histological study of the foetusplacenta unit could help reduce the percentage of cases in which the cause of foetal death remains unexplained [ 5456 ]  . 
the technique may 1 3 radiol med ( 2016 ) 121 : 847856 play a role in developing less invasive autopsy methods , particularly when parents do not consent to a full autopsy being performed , to give as much information as possible to prevent intrauterine foetal death and to help parents to be fully informed with regard to this dramatic event [ 12 ]  . 
trimboli6 chiara zuiani10 francesco sardanelli6 , 15 received : 22 april 2016 / accepted : 22 june 2016 / published online : 12 july 2016 italian society of medical radiology 2016 abstract women who underwent chest radiation therapy ( crt ) during pediatric / young - adult age ( typically , lymphoma survivors ) have an increased breast cancer risk , in particular for high doses . 
the cumulative incidence from 40 to 45 years of age is 1320 % , similar to that of brca mutation carriers for whom contrast - enhanced magnetic resonance imaging ( mri ) is recommended . 
however , in women who underwent crt , mri sensitivity is lower ( 63 80 % ) and that of mammography higher ( 6770 % ) than those observed in women with hereditary predisposition , due to a higher incidence of ductal carcinoma in situ with microcalcifications and low neoangiogenesis . 
considering the available evidence , women who underwent crt before 30 receiving a 10 gy should be invited after 25 ( or , at cumulative dose least , 8 years after crt ) to attend the following program : 1 . 
citt della salute e della scienza di torino , universit di torino , via genova , 3 , 10126 turin , italy 2 dipartimento di scienze radiologiche , universit cattolica del sacro cuore , largo agostino gemelli , 8 , 0168 rome , italy 3 u.o. 
radiologia senologica , irccs ospedale san raffaele , via olgettina , 60 , 20132 milan , italy 14 department of experimental medicine , dimes , institute of anatomy , university of genova , via de toni , 14 , 16132 genoa , italy 15 unit of radiology , irccs policlinico san donato , department of biomedical sciences for health , universit degli studi di milano , via morandi 30 , 20097 san donato milanese , milano , italy 1 3 radiol med ( 2016 ) 121 : 834837 annual bilateral two - view full - field digital mammography or digital breast tomosynthesis ( dbt ) with synthetic 2d reconstructions . 
at the age for entering population screening , the individual risk profile will be discussed with the woman about opting for only mammography / dbt screening or for continuing the intensive protocol . protocollo di sorveglianza sia effettuato presso centri di radiologia senologica che rispettino i requisiti quali / quantitativi definiti da linee - guida internazionali e che tutti i dati relativi allapplicazione del protocollo , ivi compresi i cancri dintervallo , siano raccolti mediante database informatizzato al fine di consentire analisi di performance diagnostica e di efficacia su scala multicentrica . keywords breast cancer screening lymphoma survivors mri riassunto le donne sottoposte a radioterapia toracica ( rtt ) in et pediatrica o giovane - adulta , tipicamente per linfoma di hodgkin , hanno un rischio aumentato di sviluppare tumore mammario ( tm ) , in particolare quelle trattate con rtt ad alte dosi . 
lincidenza cumulativa di tm tra 40 e 45 anni del 1320 % , simile a quella delle donne brca mutate , per le quali ormai consolidata lindicazione alla risonanza magnetica ( rm ) con mezzo di contrasto ( mdc ) annuale . 
tuttavia , rispetto agli studi di screening delle donne ad elevato rischio eredo - familiare , nelle donne sottoposte a rtt si osservata una sensibilit relativamente maggiore della mammografia e relativamente minore della rm con mdc , correlate alla maggiore incidenza di carcinoma duttale in situ con microcalcificazioni e minore neoangiogenesi . 
sulla base dellevidenza disponibile , le donne sottoposte a rtt prima dei 30 anni di et con dose cumulativa 10 gy dovrebbero essere invitate a partire dai 25 anni o almeno da 8 anni dopo la rtt a partecipare a un programma di sorveglianza che preveda : 1 . 
nel caso di controindicazioni alla rm o alla somministrazione di mdc paramagnetico , sar eseguita ecografia mammaria bilaterale anche in presenza di mammografia negativa , contestualmente alla mammografia o con alternanza semestrale . 
al raggiungimento dellet per linvito ai programmi di screening organizzato , il profilo di rischio della donna sar rivalutato e discusso al fine di decidere se optare per ladesione al protocollo di screening basato su mammografia ( eventualmente tomosintesi ) annuale o biennale o per la prosecuzione dello screening intensivo con mammografia e rm annuali . 
si raccomanda che il presente background and rationale women who underwent chest radiation therapy ( crt ) during pediatric / young - adult age ( typically those treated for hodgkin lymphoma ) have an increased breast cancer ( bc ) risk , in particular those who received mantle crt with high doses . 
however , an increased risk is also associated with rt with moderate doses for non - hodgkin lymphoma , wilms tumor , leukemia , bone tumors , neuroblastoma or soft tissue sarcoma [ 1 ]  . 
the cumulative bc incidence from 40 to 45 years of age in women who underwent crt is 1320 % , higher than the incidence observed in the young female general population and similar to that of brca mutation carriers [ 1 , 2 ]  . 
bc is diagnosed on average about 15 years after crt at about 40 years [ 3 ] , compared with a mean age of about 61 years in the general female non - exposed population [ 1 ]  . 
 breast cancers in women who underwent crt are similar to those encountered in the general female population with regard to histopathologic subtype , receptor status , lymphatic invasion and nodal involvement , which play in favor of a potential role of early diagnosis . 
moreover , in these women the possibilities of treatment of bc mostly exclude radiation therapy and chemotherapy with doxorubicin [ 4 ]  . for women who underwent crt , international guidelines [ 2 , 5 , 6 ] recommend annual mammography and contrast - enhanced magnetic resonance imaging ( mri ) , starting from 25 years of age or , for those women who had crt before 30 years , 8 years after the end of treatment . 
the rationale behind is the similar bc incidence at a young age for women who had crt and for women with hereditary predisposition to bc , associated with the relatively lower sensitivity of mammography , also related to the need to start at a young age , and the higher sensitivity of mri [ 7 ]  . 1 3 836 radiol med ( 2016 ) 121 : 834837 the availability and application of guidelines / recommendations for the surveillance of women who underwent crt is relevant for good clinical practice . 
in the usa , a study published in 2009 [ 8 ] reported that of 551 women with previous crt , 47 % of those 2539 years of age never had a mammogram and only 37 % had biannual screening mammography ; the same percentages were 8 and 53 % between 40 and 50 years of age . 
the last point highlights the need for clear statements from medical bodies . before the introduction of mri , the breast surveillance of women with previous crt included annual physical examination and mammography [ 9 ]  . 
the sensitivity ranged from 67 to 70 % for mammography , from 63 to 80 % for mri , with a 92 % sensitivity reached only in one retrospective study , with a very small sample size for mri [ 18 ]  . 
importantly , in women who underwent crt , mri sensitivity is relatively lower ( 6380 % ) and that of mammography relatively higher ( 6770 % ) than those observed in women with hereditary predisposition , due to a higher incidence of ductal carcinoma in situ with microcalcifications [ 19 ] and low neoangiogenesis . 
a sensitivity close to 95 % can be obtained only using mammography as an adjunct to mri . an expert panel [ 20 ] recently compared the recommendations proposed by the following working groups : north american childrens oncology group ( cog ) , dutch childhood oncology group ( dcog ) , scottish intercollegiate guidelines network ( sign ) , and uk childrens cancer and leukaemia group ( ukcclg )  . 
as a result of this comparison , a series of harmonized recommendations were provided : physicians , health - care providers , and women who had crt should be informed of the treatment - related bc risk ( strong recommendation ) ; surveillance is recommended for doses 20 gy ( strong recommendation ) ; surveillance is recommended for doses between 10 and 19 gy , taking into account the clinical context and further risk factors ( moderate recommendation ) ; surveillance may be reasonable for doses between 1 and 9 gy , taking into account the clinical context and further risk factors ( weak recommendation ) ; surveillance implies annual check from 25 years of age or , at least , 8 years after crt up to 50 years of age using mammography , mri or both of them ( strong recommendation ) ; physical examination may be recommended in countries where only clinical surveillance is available ( weak recommendation )  . recommendations for breast surveillance of women who underwent crt considering the available evidence for women who underwent crt before 30 years , a cumulative dose 10 gy should be irecommended after 25 years ( or , at least , 8 years after crt ) and to attend the following program : 1 . 
dedicated interview about individual risk profile and potential of different breast imaging modalities in this specific setting according to this document or other recommendations [ 5 , 6 , 2123 ] ; 2 . 
annual bilateral two - view full - field digital mammography or digital breast tomosynthesis ( dbt ) with synthetic 2d reconstructions . mammography and mri can be performed at once ( preferably during only one visit ) or alternately every 6 months , considering the local conditions . 
in the case of bi - rads diagnostic category 1 o 2 after mri plus mammography , the woman will be sent to the next screening event , taking into consideration the lack of evidence in favor of ultrasound if both mri and mammography are negative . 
in the case of bi - rads 3 , the radiologist will evaluate which workup is needed , including additional mammographic views , dbt ( if not already performed ) , ultrasound , imagingguided core or vacuum - assisted needle biopsy . on reaching the age for entering a population screening program , the individual risk profile will be discussed with the woman to opt for the only mammography / dbt screening or for continuing the intensive protocol including mri . we strongly recommend this surveillance protocol to be conducted at breast imaging centers with respect to the quantitative and qualitative requirements defined by international guidelines [ 2 , 25 ] and that all data and results provided by the application of this protocol , including interval cancers , are stored on electronic databases . 
this will allow for future analyses of diagnostic performance and clinical efficacy on a multicenter scale . 1 3 radiol med ( 2016 ) 121 : 834837 compliance with ethical standards conflict of interest the authors declare no funding and no conflict of interest for this article . ethical statement this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2016 ) 121 : 873881 doi 10.1007 / s11547 - 016 - 0670 - 1 radiotherapy stereotactic ablative radiation therapy prior to liver transplantation in hepatocellular carcinoma alessia guarneri1 pierfrancesco franco1 renato romagnoli2 elisabetta trino1 stefano mirabella2 luca molinaro3 giorgia rizza2 andrea riccardo filippi1 patrizia carucci4 mauro salizzoni2 umberto ricardi1 received : 25 may 2016 / accepted : 12 july 2016 / published online : 22 july 2016 italian society of medical radiology 2016 abstract objective stereotactic ablative radiotherapy ( sabr ) is a safe treatment approach for hepatocellular carcinoma ( hcc ) with comparable effectiveness to other local therapies . 
 we present a consecutive case series investigating the role of sabr as a bridge or downstaging option in hcc patients subsequently submitted to lt . materials and methods between september 2012 and may 2014 , 8 patients for a total of 13 lesions underwent sabr prior to lt . 
inclusion criteria were a pathological or radiological diagnosis of hcc , lesion size 6 cm or lesion number 6 cm , no extrahepatic 3 with a total diameter metastases , child - pugh class ab , ecog performance 1 . 
one patient developed a non - classic rild with a fivefold increase in transaminase enzymes level and a shift in child - pugh category from b7 to c10 due to bilirubin increase . 
prospective controlled clinical trials are needed to evaluate its efficacy compared to other local therapies in this setting . keywords hepatocellular carcinoma liver transplantation stereotactic ablative radiotherapy bridge local control surgery * pierfrancesco franco pierfrancesco.franco@unito.it introduction 1 department of oncology , radiation oncology , university of turin school of medicine , via genova 3 , 10126 turin , italy 2 department of surgical sciences , liver transplantation center , university of turin , turin , italy 3 pathology unit , department of medical sciences , university of torino , turin , italy 4 department of gastro - hepatology , aou citt della salute e della scienza , turin , italy hepatocellular carcinoma ( hcc ) is the most frequent primary tumor affecting the cirrhotic liver , with a consistent contribution to cancer mortality burden worldwide and an increasing incidence during the past decades [ 1 ]  . 
specifically , lt has been shown to provide excellent local control ( lc ) and favorable long - term recurrence - free survival rates in cirrhotic patients affected with hcc meeting the 1 3 874 radiol med ( 2016 ) 121 : 873881 milan criteria [ 3 ]  . 
nevertheless , up to 2030 % of hcc patients on a waiting list for lt would experience disease progression during this period , leading to dropout from transplantation list [ 4 ]  . 
to reduce the drop - out rate , several local therapies have been proposed as a bridge to lt , such as transarterial chemoembolization ( tace ) , percutaneous ethanol injection ( pei ) and thermal ablation , either radiofrequency ( rfa ) or microwave ( mw ) ablation [ 2 ]  . 
 adjunctively , few selected patients , even if upfront ineligible to lt , may be converted to transplantation eligibility by a downstaging effect of these specific treatment strategies [ 2 ]  . 
stereotactic ablative radiotherapy ( sabr ) has been widely investigated in recent years for both intracranial and extracranial localizations , from both primary tumors and secondary lesions [ 5 , 6 ]  . 
historically , the term stereotactic has been employed to describe a technical approach using spatial coordinates to define the position in space of a specific target volume [ 7 ]  . 
in recent years , it is mostly referred to a specific cancer treatment strategy using highly focused radiation doses delivered in a single or few fractions , without mandatory spatial coordinates guidance [ 8 ]  . 
sabr has shown to be a safe treatment approach for hcc with comparable effectiveness to that of other local therapies and it is a viable option for early - stage hcc unsuitable for standard surgical or locoregional therapies [ 9 ]  . 
we herein present a consecutive case series investigating the role of sabr as a bridge or downstaging option in hcc patients subsequently submitted to lt . materials and methods selection criteria this study includes selected patients affected with hcc and referred to the liver trasplantation center and radiation oncology department of the university of turin , turin , italy . 
all cases were reviewed and discussed by a multidisciplinary tumor board including a radiation oncologist , an expert lt surgeon , a gastroenterologist , a radiologist , and a pathologist . 
inclusion criteria were : ( 1 ) pathologically proven diagnosis of hcc or radiological diagnosis based on the american association for the study of liver diseases ( aasld ) imaging criteria ; ( 2 ) lesion size 3 with a total diam6 cm ; ( 3 ) no extrahepatic metastases ; ( 4 ) child - pugh 6 cm in diameter or lesion number eter class a or b ; ( 5 ) ecog performance status 1 ; and ( 6 ) no prior radiation therapy . 
the institutional review board approved this retrospective observational study . sabr set up , planning and delivery all patients were immobilized in supine position using a dedicated stereotactic body frame ( sbf - elekta oncology system )  . 
contrast - enhanced ct scan was performed for planning purposes with a 2.5 mm slice thickness and a subsequent 2.5 mm inter - slice reconstruction from the lung apex to lower aspect of the pelvis . 
oars outlined and used during the optimization process were spinal cord , stomach , small and large bowel , duodenum , esophagus , pancreas , both kidneys , and whole liver . 
patients were prescribed 5 fractions and 3648 gy in 35 fractions ( generally 8 gy 16 gy 3 fractions ) , in 35 consecutive days according to clinical decision making and after treatment plan dosimetric evaluation . 
the corresponding biologically equivalent dose in 2 - gy fractions ( eqd2 ) at the isocenter was 60 gy for the 5 - fraction and 104 gy for the 3 - fraction schedule , considering / ratio of 10 gy for tumor control . 
liver function ( child a vs child b ) , proximity to oars ( mainly duodenum , stomach and bowel and biliary tract ) and liver volume ( minus ptv ) receiving a mean dose of 15 gy ( > or < 700 cc ) were the criteria used to select the most appropriate fractionation schedule . 
all treatments were delivered employing a volumetric imrt with the vmat solution ( axesse linac , elekta , crawley , uk ) , using a beam arrangement made up of 12 coplanar arcs and 10 mv photons . 
to check daily set up and interfraction organ motion image - guided radiotherapy ( igrt ) was employed with a daily cone - beam ct acquired prior to each session , with a rigid co - registration performed and corresponding shifts acquired . 
all translations ( cranio - caudal , latero - lateral , anteriorposterior directions ) and rotations ( pitch , jaw , and roll ) were corrected before treatment delivery . 1 3 radiol med ( 2016 ) 121 : 873881 radiological response all patients underwent radiological evaluation after sabr until lt . 
the target hcc lesions were identified , measured and followed up prior and after sabr for a quantitative comparison according to modified response evaluation criteria in solid tumors ( mrecist ) indications . 
 partial response ( pr ) was considered as a 30 % decrease in longest diameter size of the target lesion as observed in the arterial phase of contrast - enhanced compared to baseline imaging . 
stable disease ( sd ) comprehended all cases which could not be allocated either into pr or pd [ 13 ]  . pathological response the evaluation of the pathological response of gross specimens was performed by a single dedicated pathologist , by assessing the rate of tumor necrosis relative to the total tumor volume . 
late toxicity was scored starting from 3 months after sabr until the time of lt . results patients characteristics between september 2012 and may 2014 , 8 patients with a total of 13 lesions underwent sabr for primary hcc in our institutional hospital prior to lt . 
 mean time between sabr and waiting list entrance was 2.1 months ( range 1.24.5 ) for patients bridged to lt , and 3.9 months ( range 1.95.8 ) , for downstaged patients respectively . response evaluation and toxicity amongst all 13 treated lesions , 7 ( 54 % ) were followed up radiologically ( table 3 )  . 
two patients with cr also showed an important decrease in alpha fetoprotein ( afp ) levels , from 1751 and 722 to 25 and 8 ng / ml , respectively . 
 one patient developed a non - classic rild at 1 month with a fivefold increase in transaminase enzymes level and a shift with respect to child - pugh category from b7 to c10 due to bilirubin increase . 
intra - operative surgical complications were observed in three out of eight patients ( 37.5 % ) , but only in 1 case ( 12.5 % ) a modification of the surgical strategy was needed . 
in one patient , a sclero - fibrotic fusion of the vena cava with the hepatic parenchyma was observed at the level of the retrohepatic region : this finding leads to the need for a change of the surgical technique from the planned piggy back caval reconstruction to the 1 3 radiol med ( 2016 ) 121 : 873881 1 3 878 radiol med ( 2016 ) 121 : 873881 fig . 
no radiation - induced complications were observed in the post - operative period . discussion lt is presently considered the standard therapeutic option for early hcc beyond resectability criteria [ 3 ]  . 
each approach has peculiar advantages and limitations that need to be considered in the clinical decision - making process , accounting for performance status , lesions site , size , number , and underlying liver function [ 14 ]  . 
rfa may achieve response rate as high as 90100 % but it is not amenable for lesions close to gallbladder , main vessels , or located in the sub - diaphragmatic region [ 15 , 16 ]  . 
tace has been demonstrated to achieve a cr rate of 67 % and pr rate of 30 % in early stage hcc meeting milan criteria but clinically unfit for lt [ 18 ]  . 
at last , transarterial radioembolization ( tare ) with yttrium - 90 microspheres has been shown to have objective response rate up to 61 % in hcc patients [ 19 ]  . 
 historically , radiotherapy has played a marginal role in the treatment of unresectable hcc , mainly due to the low tolerance of liver tissue to radiation and to technical challenges to deliver highly focused treatments with adequate conformality and abrupt dose fall - off [ 20 ]  . 
in fact , a risk higher than 5 % of radiation - induced liver injury has been reported after uniform whole liver irradiation up to a dose ranging from 28 to 35 gy over 3 weeks [ 21 ]  . 
the most frequent clinical presentation of liver toxicity is radiation - induced liver disease ( rild ) corresponding to a clinical syndrome of anicteric hepatomegaly , ascites and elevated liver enzymes ( mainly serum alkaline phosphatase ) occurring from 1 3 radiol med ( 2016 ) 121 : 873881 2 weeks to 3 months after treatment [ 20 ]  . 
sabr , delivering dose - escalated radiotherapy to partial liver volume , is an ablative form of highly precise local therapy which may overcome the issue of normal liver tolerance to radiation . 
while the term stereotactic has been historically adopted to describe a technical approach employing spatial coordinates to define the position of a specific target volume , presently it mainly refers to a global cancer treatment strategy using highly focused radiation doses delivered in a single or few fractions not strictly under spatial coordinates guidance [ 22 ]  . 
those patients were treated with a median dose per fraction of 14 gy ( range 816 ) if classified as child a up to a median total dose of 44 gy ( range 4048 ) or with a median dose per fraction of 8 gy ( range 814 ) up to a median total dose of 40 gy ( range 3242 ) if child b . 
on the whole cohort 2 - year local control ( lc ) was 90 % and the actuarial rates of progression - free survival ( pfs ) and overall survival ( os ) at 2 years were 69 and 96 % respectively . 
no non - hematologic toxicities were seen , while 13 % of the patients had > g1 increase in hematologic / hepatic dysfunction and 20 % experienced a child class progression within 3 months of treatment . 
up to 20 % of lesions had a pathological cr , 30 % a significant pathological response ( defined as > 50 % tumor necrosis ) , 40 % a minimal pathological response ( < 50 % of tumor necrosis ) , and 20 % had viable tumor left with no necrosis . 
 a radiological objective response was observed in 37 % ( cr : 30 % ; pr : 7 % ) , while 56 % of patients were stable and 7 % progressed . 
we employed different fractionations ( 3648 gy in 3 fractions or 40 gy in 5 fractions ) tailored according to clinical decision - making ( baseline liver function , tumor size , proximity to critical structures ) , corresponding to a bed10 gy 124.8 gy for the more hypofractionated schedule , as in andolino et al . 
 two main goals should be balanced appropriately during the clinical therapeutic algorithm in hcc patients , and specifically , the need to induce total ablation of the macroscopic disease within the liver and the necessity to maintain an acceptable toxicity profile in a clinical context usually characterized by a compromised liver function . 
interestingly , predictors of pathologic cr were a favorable radiologic response and a low afp level after local therapy prior to lt , a longer time interval between local therapy and lt , and a lower model for end - stage liver disease ( meld ) score and maximum tumor diameter . 
in our cohort , among 13 pathologically evaluated lesions , 8 ( 61.5 % ) had a cr , 2 ( 15.3 % ) a minimal pathological response , 1 had a significant pathological response ( 7.4 % ) and the remaining 2 ( 15.3 % ) showed sd . 
 accordingly , in our series , lesions achieving pathologic cr were relatively small ( mean diameter 18 mm ) and were treated with higher doses ( 4548 gy / 3 fractions in 6 / 8 lesions )  . 
our patients were evaluated with post - sabr imaging at 13 months , while it has been demonstrated that the peak response timing for radiological responders is between 4 and 6 months [ 15 ]  . 
in our series , 1 month after treatment , one patient had non - classic rild with a fivefold increase in transaminase enzymes level and a child category shift from b7 to c10 due to bilirubin increase . 
even if the same study did not show any association between liver dose and child score , baseline liver function was correlated to the development of toxicity in any form and the occurrence of any increase higher than 1 grade in hematologic / hepatic dysfunction [ 23 ]  . 
 toxicity profile in our series was acceptable with only one patient who experienced a category shift in terms of liver function and surgical procedures which were not consistently affected by prior sabr ( only one case of surgical technique modification )  . 
our results add further data supporting the use of sabr as a safe , well - tolerated and effective method to provide lc prior to lt in hcc patients , with mild toxicity and low surgical morbidity . 
ioannou1 nikolaos kontopodis1 efstratios georgakarakos2 elias kehagias3 eleni metaxa4 stella lioudaki1 yannis papaharilaou4 dimitrios tsetis3 received : 12 january 2016 / accepted : 12 july 2016 / published online : 23 july 2016 italian society of medical radiology 2016 abstract purpose to investigate if the routine use of an aortic balloon within 1530 min after ovation stent graft ring inflation would resolve any inflow stenosis , which may reach 60 % , at the level of the sealing rings . 
moreover , we estimated the potential hemodynamic compromise in these patients during rest and exercise . methods following 3 - dimensional reconstruction of aaa models , cross - sectional area of the infrarenal aorta just proximal the sealing mechanism ( aaort , raort , respectively ) and internal area at the site of stenosis ( aint , rint , respectively ) were measured for 83 . 
pressure drop during rest and exercise was estimated . results technical success was 98 % and there were no perioperative deaths , one type - i endoleak , and 12 ( 14.5 % ) type - ii endoleaks . 
 the advantages of evar compared to traditional open surgical repair regard reduced peri - procedural mortality and morbidity , decreased need for blood products and intensive care unit as well as reduced hospital stay and earlier mobilization and return to normal occupational and social life [ 3 , 4 ]  . 
previous reports indicate that only 32 % of men and 12 % of women met all three neck criterion ( diameter between 18 mm and 32 mm , length > 15 mm angulation < 60 ) and had iliac lumen diameters > 6 mm , while the rest of subjects presented at least one anatomic index , out of current requirements of available stent - grafts [ 5 ]  . 
accordingly there is a constant effort of the industry in cooperation with surgeons to design and produce devices able to accommodate more complex aaa morphometric characteristics making a larger proportion of patients amenable to endovascular treatment . 
according to previously published data , devices that accommodate shorter infrarenal aaa neck length will have the greatest impact on expanding on - label evar indications regardless of gender [ 5 ]  . the ovation endograft is a modular device which has introduced a unique concept in evar technology . 
this regards the uncoupling of the sealing and fixation mechanisms with the use of a rigid nitinol stent to achieve fixation and two inflatable metal - free o - rings used to achieve proximal sealing and exclude the aneurysmal sac from systemic circulation and pressurization [ 6 ]  . 
this kind of sealing mode has been suggested to be able to achieve sealing in hostile neck anatomy and currently this endograft is the only being approved to treat aaas with necks as short as 7 mm [ 7 ]  . 
the shortand mid - term results of the ovation device , even in patients with unfavorable neck anatomy ( length < 10 mm ) have been excellent according to several previous reports . 
moreover , this modality has been suggested not to exert the chronic outward force that is seen with other stent - grafts achieving proximal sealing through the radial force of the stent portion of the device which may result in the observed neck dilatation over time [ 3 , 810 ]  . nevertheless , these advantages come at a price of an almost 60 % inflow stenosis at the site of the o - rings as ioannou et al . 
the manufacturer does not suggest the routine use of an aortic balloon at that site in order to mold the o - rings , rather leaves this maneuver at the discretion of the treating physician [ 12 ]  . 
finally , we estimated the hemodynamic impact of this stenosis , both at rest and after exercise , since in the presence of high flow ( i.e. , during exercise ) a hemodynamically non - critical stenosis may become critical causing a greater pressure drop . materials and methods study population / study design all consecutive patients undergoing evar in a single center with the use of the ovation endograft were retrospectively reviewed . 
suitable patients for the implantation of the specific endograft were selected according to the manufacturers instructions for use ( ifu ) as described elsewhere [ 3 , 11 , 12 ]  . 
 during initial experience with this device an aortic balloon was not used intraoperatively since this was not required by the manufacturer in the ifu ( patient group i )  . 
nevertheless , upon realization of the inflow stenosis at the site of the inflatable o - rings the routine use of an aortic balloon was performed intraoperatively in all patients ( patient group ii )  . 
 for this purpose , we have been using the coda balloon catheter ( cook incorporated , bloomington , in ) which is a semicompliant , polyurethane balloon used for expansion of abdominal and thoracic aortic aneurysm endografts and / or temporary occlusion of large vessels . 
balloon 1 3 884 radiol med ( 2016 ) 121 : 882889 inflation was performed under direct fluoroscopy and the balloon may be inflated more than once depending on if a stenosis remains apparent . 
a maximum of four inflation attempts was permitted to avoid possible aortic injury from the inflations . during follow - up , patients were guided to undergo a postoperative ct scan at 1 month after the procedure to determine good positioning of the device and absence / presence of endoleaks . 
accordingly the 1 - month postoperative ct scan was used to determine the degree of stenosis and compare between patients that were managed with or without an aortic balloon . image acquisition , image postprocessing , obtaining measurements the methodology regarding acquisition and post - processing of images and obtaining of measurements has been described in detail elsewhere [ 11 ]  . 
ct data were acquired with a third generation ct scanner , the somatom sensation 16 multislice helical ct ( siemens ag , forchheim , germany ) with ct acquisition parameters prescribed as follows : 260 mas , 120 kvp , slice thickness 2 mm , resolution 1.153 pixels per mm , pixel spacing 0.8671875\0.8671875 , sfov 50 cm , width 476.00 mm ( 512 ) , height 476.00 mm ( 512 ) , depth 420.00 mm ( 210 )  . the 2 - dimensional ct images were processed with the open source software itk - snap in order to perform 3 - dimensional reconstruction of the aaa lumen surface while the latter was then processed with the vascular modeling tool kit ( vmtk ) open source software [ 17 , 18 ]  . 
the degree of stenosis was determined by comparing the cross - sectional lumen area at the site of the maximal stenosis inside the o - rings ( internal areaaint ) with the corresponding lumen area just cephalad , meaning 1 mm proximal to the rings ( normal aortic areaaaort )  . 
the centerline of the aortic lumen is displayed as a black line inside the lumen while the perpendicular cross - section 1 mm apart is also presented ( yellow wireframes )  . 
the inflatable o - rings at the aortic neck are displayed with opaque white color estimation of pressure drop during rest and exercise according to hemodynamic principles a stenosis inside a rigid pipe with steady fluid flow would normally cause a pressure drop . 
according to this , the pressure drop is proportional to the flow ( q ) and the length ( l ) of the stenosis and inversely proportional to the forth power of the radius ( r )  . p = q 8nl / r4 . values for r and l were measured for all patients under evaluation and used to estimate p for every subject . 
pressure the those during rest : q drop was calculated taking into account both values of q in order to estimate effect during rest and exercise . statistical analysis regarding area and radius measurements median values and range were recorded for the whole study cohort at both levels of interest ( inside and 1 mm proximal to the o - rings )  . 
moreover , area and radius stenosis as well as pressure drop was calculated for patient groups i and ii and the median values were compared to each other using the mannwhitney test , to evaluate the effect of routine use of an aortic balloon . 
there were 12 ( 14.5 % ) type - ii endoleaks and one type - i endoleak which presented spontaneous sealing and aneurysm shrinkage at 6 - month follow - up . area and radius reduction an aortic balloon was not used in patients 149 ( group i 49 subjects ) , while it was used in patients 5083 ( group ii 34 subjects )  . 
overall , in all 83 patients , a median aint of 143 ( range 28380 ) mm2 was observed compared with a median aaort of 314 ( range 177531 ) mm2 . 
2 presents three aaas , the first presents a mild stenosis after using an aortic balloon to mold inflatable o - rings , while the second and third case did not undergo intraoperative ballooning and present severe inflow stenosis . 
 effect of neck length and angle interestingly , a significantly lower inflow stenosis was observed in patients with a short ( 15 mm ) compared to those with a long ( > 15 mm ) aortic neck within the study cohort . 
specifically , the inflow stenosis was the same among patients with a high or low neck angulations ( 52 vs 57 % , p value 0.6 ) , while additional ballooning equally and significantly reduced the degree of stenosis in both groups , but there was no difference between the groups with regard to the end stenosis ( 61 vs 45 % , p value 0.02 for angles < 45 and 55 vs 31 % , p value 0.05 for angles > 45 ) ( table 2 )  . 
in case a an aortic balloon was used and a moderate inflow stenosis of 42 % was recorded while in cases b and c this was not use and a severe stenosis of 80 % was recorded . 
with the opaque red color the aortic lumen is displayed while the light red color represents the aneurysm sac and the white opaque color represents the inflatable o - rings . 
3. discussion the promising ovation endograft may have allowed treating patients with complex aortoiliac anatomies and short / hostile necks , but according to the present results induces an inflow stenosis of ~55 % at the site of the inflatable o - rings . 
3 the curves that poiseuilles law predicts for specific n , and q during rest ( blue line ) and after exercise ( orange line ) using values obtained from the literature and l measured in our study cohort . 
it can be seen that an insignificant p may be expected during both rest and exercise even for the patients with the most severe stenosis in our study and it can be seen that all values are practically zero effect is significantly greater in patients in whom an aortic balloon is not routinely used intraoperatively . 
on the contrary , the use of this maneuver is very simple , takes about 13 min in total and may blunt this phenomenon resulting in a significantly less severe stenosis . 
in fact , according to poiseuilles law which describes viscous energy losses in idealized situations , the pressure drop is inversely proportional to the fourth power of the radius and therefore graphs based on poiseuilles law are sharply curved [ 21 ]  . 
subsequently , as the radius of a conduit progressively reduces , little effect is observed on pressure until a certain degree of stenosis is reached beyond which further reductions result is rapid decline of the pressure gradient . 
in our series the most severe stenosis was 80 % which indicates that even for these cases an insignificant hemodynamic effect may be expected . nevertheless , the pressure drop along a stenosis is largely but not solely determined by the radius . 
subsequently , a non - critical stenosis in a low - flow system ( i.e. , resting conditions ) may become critical in case of high flow ( i.e. , during exercise ) and significant drops in pressure may occur with less severe narrowing in high - flow systems than in low - flow systems . 
nevertheless , due to the reduced magnitude of this phenomenon this kind of decrease may be irrelevant from a clinical standpoint . on the contrary , it should be noted that poiseuilles law is only an approximation of what happens in reality since it is valid only for idealized conditions of steady flow of newtonian fluids in a rigid pipe , conditions that are seldom if ever present in real life [ 23 ]  . 
 therefore , the present results should be interpreted with caution . despite the fact that a hemodynamically significant effect could not be demonstrated for any of the patients examined , regardless of the use of an aortic balloon , it is certain that no treating physician would like to have a 55 % ( median ) or worse an 80 % ( upper limit ) stenosis inside the abdominal aorta . 
the long - term results of such an effect ( i.e. , disturbed blood flow , platelet activation and thrombus formation , strain of the endograft ) are not known and deserve further attention . 
nevertheless , until further long - term data are available , we suggest that an aortic balloon should be routinely used during ovation endograft implantation to blunt this phenomenon and reduce the degree of the inflow stenosis . 1 3 888 radiol med ( 2016 ) 121 : 882889 moreover , we have recorded a greater stenosis among patients with a long ( > 15 mm ) aortic neck compared to those with shorter ( 15 mm ) necks . 
this may be due to the fact that in aaas with short necks , part of the rings is inflated inside the proximal portion of the aneurismal sac thus having enough space to expand . 
on the contrary , in cases with longer necks the rings are cramped inside the neck and since they are not supposed to expand towards the aortic wall in order to avoid neck dilatation over time , they may tend to expand inwards . 
although the current analysis may be hampered by the fact that it is a single - center study with only a short - term follow - up , this is a first effort to evaluate the possible significance of the ovation device original sealing mechanism , in aneurysm neck hemodynamics which may promote further research on this topic . conclusion a significant inflow stenosis is observed after the implantation of the ovation endograft to treat during endovascular aneurysm repair . 
the hemodynamic consequences of this effect seem insignificant according to the present results but these should be interpreted with caution since the true effect of this phenomenon may be underappreciated and further investigation is warranted . 
our purpose was to describe the effectiveness and the safety of the treatment and to evaluate the magnetic resonance imaging ( mri ) , computed tomography ( ct ) and contrast - enhanced ultrasound ( ceus ) diagnostic accuracy in hcc patients treated with ire at 1 - , 3 - , and 6 - month follow - up . materials and methods in an 18 - month period , we treated 24 hcc lesions in 20 patients unfit for surgery . 
we evaluated the size , shape , signal intensity ( t1 - w , t2 - w , and dwi ) in mri , dynamic contrast enhancement pattern for ceus , ct and mri and signal behavior during the liver - specific phase for mri . results according to mrecist , at 1 month mri and ceus showed a complete response ( cr ) in 91.7 % of cases ( 22 / 24 ) tumors , while there was partial response ( pr ) in the remaining 2 / 24 ( 8.3 % ) treated nodules ; in ct study all ablated zone appeared as necrotic ( cr 100 % )  . 
 the residual viable tumor in mri and in ceus study had * orlando catalano orlandcat@tin.it 1 department of radiology , istituto nazionale tumori fondazione g.pascale , via mariano semmola , naples 80131 , italy 2 department of hepatobiliary surgical oncology , national cancer institute , fondazione pascale , via mariano semmola , naples 80131 , italy 91.7 % and pd 91.7 % and pd similar diameter ( 10 mm )  . 
at mri the diameters of the two residual viable hccs were 12 and 14 mm , at ceus the diameters were 11 and 12 mm , while at ct the diameters were 10 and 10 mno statistical difference was evaluated between cr , pr , pd percentage values for mri , ct and ceus ( p value > 0.05 at chi - square test )  . 
we found no statistically significant difference in morphology , size ( variation in the largest diameter ) , signal intensity in t1 - weighted images , in t2 - weighted images , in dwi and in the related map of the apparent diffusion coefficient ( adc ) , presence or absence of contrast enhanced during the arterial , portal , and late phase in mri , ct , and ceus , and signal characteristic during the liver - specific phase in mri of the ablation zone at 1 , 3 , and 6 months . 1 3 radiol med ( 2016 ) 121 : 122131 conclusion ire is a feasible , safe and efficient modality in the treatment of patients with non - resectable hcc . 
 we had no major complication , even when the ablated lesion was adjacent to major branches of the portal ve all images techniques showed similar accuracy during the follow - up at 1 , 3 , and 6 months in the assessment ablated zone . keywords hepatocellular carcinoma liver ablation magnetic resonance imaging computed tomography contrast - enhanced ultrasound response to treatment introduction hepatocellular carcinoma ( hcc ) is the sixth most common cancer worldwide and the third leading cause of cancer - related death [ 1 ]  . 
surgery is the mainstay of hcc treatment , and hepatic resection is the treatment of choice for hcc in patients with early - stage disease according to the barcelona - clinic liver cancer ( bclc ) classification [ 2 ]  . 
thermal ablation therapies , such as radiofrequency ablation ( rfa ) , laser ablation , cryoablation , and microwave ablation are all based on transfer of thermal energy to the tissue around the needle , electrode , or probe . 
 limitations in relation to size ( > 3 cm ) , location ( subcapsular or close to heat - sensitive structures such as the gallbladder , major bile ducts , portal vein , and hepatic veins ) , and heat - sink effect restrict the use and effectiveness of thermal ablation treatment [ 4 ]  . irreversible electroporation ( ire ) is a non - thermal technique for cancer ablation . 
the application of an electric field across a cell alters the transmembrane potential , thus , the lipid bilayered structure is disrupted and small nanopores are created in the cell membrane that allow micromolecules and macromolecules to be transported into and out of the cell , leading to apoptosis [ 58 ]  . in oncology , tumor response was initially measured according to the bidimensional world health organization ( who ) criteria [ 9 ] and afterward according to the monodimensional response evaluation criteria in solid tumours ( recist ) guidelines [ 10 ]  . 
residual tumor tissue needs to be assessed using computed tomography ( ct ) or magnetic resonance ( mri ) studies and viable hcc should be defined as a persistent uptake of contrast medium in the arterial phase of dynamic imaging studies . 
according to lencioni et al . , it is mandatory to obtain a dual - phase imaging of the liver , arterial and portal phase , while the equilibrium phase is useful but not necessary [ 11 ]  . hcc patients treated with ire require an adequate evaluation of the treatment outcomes , similarly to those subjects undergoing other percutaneous techniques . 
the objective of our singlecenter , prospective study was to describe the effectiveness and the safety of the treatment , and to evaluate the mri , ct , and contrast - enhanced ultrasound ( ceus ) diagnostic accuracy in hcc patients treated with ire at 1 - , 3 - , and 6 - month follow - up . materials and methods the study has been approved by our ethics committee . 
all the data were collected and managed according to the current privacy regulations . study population from january 2012 to july 2013 , 20 non - consecutive patients ( 12 males and 8 females , with a mean age of 65 years , range 4880 years ) , with hcc underwent ire treatment in a single cancer center . 
3 hcc nodules or less , nodule size 3 cm , child - pugh class a , ecog ( eastern cooperative oncology group ) performance status of 0 , asa ( american 1 3 124 radiol med ( 2016 ) 121 : 122131 society of anesthesiologists ) score of 3 , prothrombin time 109 / l . 
all selected ratio > 50 % , and platelets count > 50 patients had chronic liver disease which was related to hepatitis c virus infection in 8 patients , hepatitis b virus infection in 10 cases , and alcohol abuse in 2 . 
all patients were stage a according to the bclc classification and all had alpha - fetoprotein levels > 4 ng / ml ( 10320 ng / ml , mean 80 ng / ml )  . 
twenty - four hcc nodules with a mean size of 2 cm ( 13 cm ) were treated with ire ( 12 nodules , mean 1.2 per patient treated lesions )  . 
there were 20 well - differentiated hccs , 3 moderately differentiated nodules , and one poorly differentiated lesion . irreversible electroporation the nanoknife ire ( angiodynamics inc . , latham , ny , usa ) system was used for ire . 
the needles were placed in the liver parenchyma immediately adjacent to the hcc , trying to encircle the entire lesion , with a one - cm safety margin of surrounding liver tissue . 
in 4 patients with two hccs , each nodule was treated separately , in a consecutive fashion . imaging techniques according to the study protocol , all patients underwent baseline mri , ct and ceus study 57 days before ire and post - treatment at 1 , 3 and 6 months . 
long - term follow - up was carried out with ct or mri obtained every 3 months in the first year and every 6 months thereafter . ceus was always preceded by a careful us survey , assessing the size and appearance of the ablation zone and looking for any new nodule in addition to the ablated one . 
ceus was performed as a low - mechanical index , double - split mode , real - time modality ( technos mylab 70 xvg and mylab twice , esaote , genoa , italy ) , injecting 2.4 ml of a sulfur hexafluoride - based contrast medium ( sonovue , bracco , milan , italy ) per each liver lobe . 
thereafter , he / she moved the transducer to explore the remaining parenchyma of each lobe , with special reference to the segment bearing the ablated lesion . contrast - enhanced triple - phase helical mdct was performed with a 16 - detector row scanner ( brilliance 16 , philips medical systems , eindhoven , the netherlands )  . 
scans were carried out including a region encompassing liver from diaphragm dome to iliac crests as follows : hepatic arterial phase scanning began 3040 s after injection of 120 ml of a nonionic iodinated contrast media ( iomeprol , iomeron 400 , bracco , italy ) with a bolus - triggered technique ( 120 kvp ; 4060 ma ; monitoring frequency from 12 s after the contrast injection ; trigger threshold , 100 hus in descending aorta ) ; portal and equilibrium phases were obtained scanning the same region , respectively , 70 s and 180 s after contrast medium injection . 
the contrast medium was administered at a rate of 4 ml / s through antecubital vein with an automated injector system ( empower cta , e - z - em inc . , new york , ny )  . mri was performed by using a 1.5 t scanner ( magnetom symphony , with total imaging matrix package , siemens , erlangen , germany ) with 8 - element body and phased array coils . 
the mri examination consisted of images taken before iv administration of contrast medium and then dynamic sequences obtained after iv injection of a liver - specific contrast medium gadolinium ethoxybenzyl dimeglumine ( primovist , bayer schering pharma , germany )  . 
the modified mrecist are the following : complete response ( cr ) is the disappearance of any enhancement in all target lesions , partial response ( pr ) is at least a 30 % decrease in the sum of diameters of enhancing target lesions , taking as reference the baseline sum of the diameters of target lesions , stationary disease ( sd ) is any cases that do not qualify for either partial response or progressive disease , progressive disease ( pd ) is the increase of at least 20 % in the sum of the diameters of enhancing target lesions , taking as reference the smallest sum of the diameters of enhancing target lesions recorded since treatment started [ 11 ]  . four observers with at least 7 years experience in interpretation of ceus , mri , and ct images of the liver independently and randomly reviewed the images acquired after ire at the 1 , 3 , and 6 months . 
the observers recorded in consensus the presence and segmental location of the ablated zone , using a 4 - point confidence scale ( score ) based on published studies on hcc [ 13 ] : 1 , no residual hcc ; 2 , probably no residual hcc ; 3 , probable residual hcc ; 4 , definite residual hcc . 
completely ablated lesions appear as a hypoattenuating area with no foci of contrast enhancement either within the lesion or at its periphery . the following parameters were also evaluated for each single ablation zone in ceus , ct and mri at 1 , 3 , and 6 months : morphology ; size ( variation in the largest diameter ) ; signal intensity , respectively , in t1 - weighted images , in t2 - weighted sequences , in dwi and in the related map of the apparent diffusion coefficient ( adc ) for mri ; the presence or absence of contrast enhanced during arterial , portal , equilibrium phase ; the signal characteristic of the ablation zone during the liver - specific phase for mri . 
 moreover , other parameters evaluated were : morphological modifications of the surrounding normal liver parenchyma ; alterations of vascular perfusion during the arterial phase ( thid ) and the liver - specific phase ; the evidence of capsular retraction ; the occurrence of complications . 
 [ 14 ] into minor and major occurrences . statistical analysis cr , pr , sd , and pd percentage were recorded for mri , ct and ceus in according to mrecist criteria . 
a p value of 0.05 was regarded as statistically significant . results eight nodules out of 24 were classified as being located in difficult sites , while 16 / 24 were regarded as being in non - difficult sites . 
arterial phase axial t1 - weighted vibe image ( a ) , portal phase axial t1 - weighted vibe image ( b ) , arterial phase axial ct image ( c ) and portal phase axial ct image ( d )  . 
at mri the diameters of the two residual and pd viable hccs were 12 and 14 mm , at ceus the diameters were 11 and 12 mm , while at ct the diameters were 10 and 10 mm . the two residual viable hccs underwent an additional single session of ire achieving complete response and intraoperative us confirmed the diameter showed during mri study . 
axial , t1 - weighted vibe image in the arterial phase ( a ) , portal phase axial t1 - weighted vibe image ( b ) , arterial phase axial ct image ( c ) and portal phase axial ct image ( d )  . 
enhancing , residual tumor in the upper part of the ablation zone ( a ) , not visible in arterial phase axial ct image ( c ) complete response , partial response , pd percentage values for mri , ct and ceus ( p value > 0.05 at chi - square test )  . we found no statistically significant difference in morphology , size ( variation in the largest diameter ) , signal intensity in t1 - weighted images , in t2 - weighted images , in dwi and in the related map of the apparent diffusion coefficient ( adc ) , presence or absence of contrast enhanced during arterial , portal , equilibrium phase , and signal characteristic during the liver - specific phase of the ablation zone at 1 , 3 and 6 months . most ablation zones had a round shape ( 20 out 24 , 84 % )  . 
in t1 - weighted sequences all 24 lesions ( 100 % ) showed a non - homogeneous signal , with a hyperintense central core and a hypointense peripheral rim , with no signal decay during the opposed - phase gradient echo sequences . 
ceus scan ( double - split image ) taken 38 s after contrast injection showing a small globular area of persistent contrast enhancement ( large arrow ) within an otherwise avascular , necrotic nodule ( small arrows )  . 
pr 10 clearly visible at b0 s / mm2 ( 4 out of 24 , 17 % ) , there was no signal detectable at b800 mm / s2 , where only the rim showed a restricted diffusion . 
the residual tumor tissue appeared as hypointense , although to a lesser degree than the necrotic portion , in the hepatobiliary excretory phase in mri . in four peripheral ablated zones ( 17 % ) , there was a capsular retraction . 
in a prospective , multicenter study to evaluate the safety and efficacy of ire as first - line treatment in biopsy - proven , early - stage hcc lencioni et al . 
major complications were rare and included only one case of hemothorax related to electrode 1 3 radiol med ( 2016 ) 121 : 122131 in our series there was no major vascular complication , even when the ablated lesion was adjacent to major branches of the portal ve this is in accordance with the report from lencioni et al . 
 [ 26 ] showed experimentally that placing electrode needles of 1 mm in both the superior mesenteric artery and the portal vein of pigs was uneventful , with no vascular thrombosis . 
on the other hand , it is still unclear the cause of reduced concentration of the liver - specific contrast medium inside the parenchyma surrounding the lesion , during the accumulation phase . 
however , ire itself seems to be safe in the treatment of peri - biliary liver tumors , since the injuries reported are mostly mechanical and not thermal [ 27 ]  . 
ire can also determine a liver capsular retraction at level of the needle insertion and create of arteriovenous shunts [ 27 ]  . a previous study from our group [ 13 ] indicated that combined interpretation of dynamic and hepatobiliary phase mri images improves the diagnostic accuracy of gadoxetate disodium - enhanced mri for the detection of residual hcc and new hcc in ablated area after rfa compared with either dynamic mri or ct alone . 
in this study all imaging techniques have showed similar accuracy during the follow - up at 1 , 3 , and 6 months in the assessment ablated zone and we thought it depended on the few ablated zone evaluated in this study . in a previous study from our group , we have evaluated the mri findings of hcc patients treated with ire [ 28 ] follow - up at 1 month . 
no differences in morphology , size ( variation in the largest diameter ) , signal intensity in t1 - weighted images , in t2 - weighted images , in dwi and in the related map of the apparent diffusion coefficient ( adc ) , in the presence or absence of contrast enhanced during arterial , portal , equilibrium phase and in the signal characteristic during the liver - specific phase of the ablation zone there were at 1 , 3 , and 6 months . one or more imaging modalities are employed for patient monitorization , including us , ct , dynamic mri , and liver - specific mri [ 2931 ]  . 
however , there is a limited international consensus on the appropriate imaging modality to be employed , on the time interval between each follow - up study , and on the total length of time for which follow - up is to be carried out [ 14 , 32 ]  . 
the ablation zone appears hypointense on the t2 - weighted image and note dilated bile ducts adjacent to the ablated zone placement and one case of transient hepatic decompensation with spontaneous resolution [ 21 ]  . 
the latter can be the consequence of inaccurate visualization of the lesion by means of sonography , which is used to guide the insertion of the electrode probes inside the hcc . 
indeed , poor visualization of the target can cause an incorrect placement of the electrode probes inside the lesion , which occurred in one of the two cases with a partial response in our series . 
the correct placement and the adequate number of electrode probes are both crucial for developing symmetrical electrical fields which overlap over the lesion and ablate a spherical area corresponding to the nodular hcc . 
 however , it should be considered that also ct could be employed to guide ire treatment , at least in the case of lesions barely recognizable at us . the mechanisms responsible for cell death in the hcc treated with ire are not well understood , and they are still under investigation . 
in an animal study , a voltage higher than 2500 v / cm3 , which is usually delivered during ire , created nanopores in the cell membrane through which micromolecules and macromolecules are transported into and out the cell . 
the final result is a permanent alteration of cell homeostasis which contributes to the death of the cells [ 24 ]  . 1 3 130 radiol med ( 2016 ) 121 : 122131 follow - up , while ceus may be extremely useful to define local tumor progression and is indicated in the assessment of local tumor progression when follow - up ct or mri are contraindicated or not conclusive and that , in addition to ct and / or mri , ceus may be used in follow - up protocols . our study has a number of limitations . 
first , the number of patients is very small and further studies on larger series are necessary to test the efficacy of the ire treatment and to confirm the imaging findings we illustrated . 
another limitation is that we could not make any correlation between the ire response and the tumor grade , since only a bioptic diagnosis was available for our cases . conclusion in summary , the results of our study indicate that ire is a feasible , safe and efficient modality in the treatment of patients with non - resectable hcc . 
we had no major complications , even when the ablated lesion was adjacent to major branches of the portal vethis is because the use of non - thermal energy allows a successful treatment of hepatic lesions located near critical vascular structures , without damaging theall imaging techniques have showed similar accuracy during the follow - up at 1 , 3 , and 6 months in the assessment ablated zone . 
consequently , our current follow - up practice is to alternate the simpler and less expensive ceus imaging with the more comprehensive and standardized ct or mri study . acknowledgments the authors are grateful to alessandra trocino , librarian at the national cancer institute of naples , italy . compliance with ethical standards conflict of interest the authors have no conflict of interest to be disclosed . ethical statement all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the effective dose for the conventional method was 1.2 msv for rando phantom . conclusion the wbldmdct effective dose in our institution is consistent with the values reported in previous studies . 
the clinical staging , which is critical for prognosis and therapeutic planning , is based upon laboratory findings and radiological assessment of bone involvement [ 13 ]  . skeletal conventional x - ray imaging still represents the gold standard due to its wide availability and its low cost . 
 however , it has been demonstrated that the x - ray imaging sensitivity is low , especially in detecting small bone lesions . furthermore , owing to the long acquisition time ( about 30 min ) and the necessity of continuously changing and uncomfortable positions , the x - ray examination is not well tolerated by elderly patients with bone pain . first , horger in 2007 settled a whole - body low - dose multidetector computed tomography ( wbldmdct ) [ 4 ] protocol : he showed that , given the high intrinsic contrast of bone tissue , even a low - dose protocol ( 40 mas ) produces images of good quality , suitable for diagnosis , with a significant radiation dose saving comparing with a standard ct protocol ( 4.1 msv at 40 mas versus 25.5 msv at 250 mas )  . 
an advantage of the technique is also the possibility to evaluate the extraosseous localization of the disease . according to this new evidence , since august 2013 we agreed with haematologists at our institution to replace skeletal conventional x - ray examinations with wbldmdct in mm patients . 
we decided to evaluate the radiation dose of the first 29 consecutive patients with a biopsyproven diagnosis of mm who underwent wbldmdct in our institution and to compare it with both the dose levels reported by literature for this protocol and the dose of the conventional x - ray study . this is in compliance with the local decree law , ( dl 187 / 2000 ) [ 8 ] , that acknowledges the european directive 97 / 43 / euratom concerning radiological protection of persons against risks related to medical exposures . 
such a document contemplates monitoring and optimization of patients exposures and indicates quality tests of the equipment that have to satisfy acceptance criteria , and diagnostic reference levels ( drl ) checks as operative means to achieve optimization . 
an important upgrade of both the acceptance criteria and ldr is represented by the document rp 162 published in 2012 [ 9 ] that accounts for the technological evolution of the equipment and dedicates an important section also to the ct scanners . 
previous works concerning radiological evaluation of mm patients report radiation doses of about 4 msv for the wbldmdct protocol and about 2 msv for the conventional x - ray examination . 
the wbldmdct protocol , recently adopted in our institution , takes advantage not only of the high intrinsic contrast of the bone tissue , but also of the use of iterative reconstruction algorithms ( ir )  . 
such a reconstruction technique , recently introduced radiol med ( 2016 ) 121 : 93105 in ct modality [ 1012 ] as an alternative to conventional methods based on the filtered back projection ( fbp ) , is able to reduce the noise ( denoising ) acting in the image space . 
as a consequence it is possible to obtain images with a signal to noise ratio ( snr ) equivalent to those that would be obtained using fbp , but with a lower patient dose , or images with a lower level of noise at the same patient dose . 
a further value of these algorithms is the ability to uncouple the image noise from the modulation transfer function ( mtf ) properties so that the spatial resolution is preserved . given this context , in the present work , the dose to patient is evaluated for both the new ct protocol and the old conventional one . 
these physical quantities cannot be compared directly , but they can be used to estimate the effective dose , which is a radioprotection index relating to stochastic risk , that allows for the two methods to be compared . materials and methods ct modality ct subjects and scan parameters 13 years , mean the study was done for the first 29 patients with mm ( 14 males , 15 females , age 67 standard deviation ) who were examined with wbldmdct protocol in our department , using the ct scanner 64 brillance , philips medical syste the patients were positioned supine , with their arm over the head . 
b some images of the rando phantom used to simulate the conventional examination of the skeleton : ( i ) anteriorposterior skull , ( l ) lateral skull ; ( m ) pelvis ; ( n ) ribs ; ( o ) anteriorposterior dorsal and lumbar spine ; ( p ) lateral spine slices acquired simultaneously and t is the nominal slice thickness so that n t accounts for the beam width . 
the measurements are taken at the centre ( c ) and at peripheral positions ( p ) of the phantom so that the weighted ctdi ( ctdiw ) can be estimated ( ctdiw 1 / 3 ctdic 2 / 3 ctdip ) representing the average ctdi across the irradiated slab ( unit mgy )  . 
1 continued ct effective dose evaluation the effective dose e ( expressed in millisievert msv ) [ 14 , 15 ]  . is defined as e ( cid : 31 ) t wtht ht being the equivalent dose in tissue or organ , and wt being the appropriate tissue weighting factor ; the equivawr , lent dose in tissue or organ is given by ht where dm is the absorbed dose averaged in that tissue or organ ( due to radiation r ) , multiplied by the radiation weighting factor wr ( for photons wr is equal to 1 for all energies )  . dm nevertheless , e can be easily estimated by multiplying the dlp values by conversion coefficients reported in literature for different body regions , obtained by means of monte carlo simulations and anthropomorphic phantoms [ 14 , 1619 ]  . 
the dlpr of each single segment has been calculated as a fraction of the total dlp ( dlptot ) , the fraction being equal to the ratio lr ltot dlptot , where lr is the length of the seg ( dlpr ment r and ltot is the total scan length )  . 
in particular for head , neck , chest , abdomen lr ltot 1 3 radiol med ( 2016 ) 121 : 93105 and pelvis , conversion coefficients reported by deak et al . 
these coefficients are based on icrp publication 103 tissue weighting factors and adult female and male anthropomorphic phantoms that include all the organs and tissues contributing to the effective dose as defined in icrp publication 60 and the new organs and tissues not previously considered ( the salivary glands , extrathoracic tissue , lymph nodes , prostate , oral mucosa , and the nasal vestibule )  . for humera and femura , coefficients evinced from other references were used [ 20 , 21 ] concerning musculoskeletal studies . for the segments head and neck a further correction factor , experimentally measured , has been used , to account for the ratio nctdiw16 / nctdiw32 , the numerator and the denominator of the fraction being the normalized weighted dose indexes related to the phantoms of diameter 16 and 32 cm , respectively . 
 finally , correction for the body weight factor was done to account for patient body weight differences with respect to the reference human phantoms ( 73 and 58 kg for male and female phantom , respectively )  . 
in this way the dose evaluation is tailored to individual patient body segment lengths and body masses , allowing for a better approximation to be achieved [ 22 , 23 ]  . ct scanner tests the following points were also evaluated : ( a ) the accuracy of the nominal value of the ctdivol produced by the scanner ; ( b ) the gain in noise reduction achieved using the iterative reconstruction algorithm idose , installed in the scanner philips brillance 64such a parameter was evaluated considering the standard deviation of the pixel signal , expressed in hounsfield units ( hu ) in a region of interest of the image of a phantom ; ( c ) the mtf . 
for point ( a ) a pencil beam dosemeter unforsxi and a cylindrical phantom with diameter of 32 cm simulating the body geometry were used ; for points ( b ) and ( c ) the catphan phantom was used ; in particular the homogeneous section and the section containing the set of bar patterns with different spatial frequency were used , respectively , for noise and mtf evaluation . 
mtf was evaluated using the droege method [ 24 ] using the points ranging from the maximum value to 1 / 10 of it . conventional xray examination conventional xray imaging protocol in order to evaluate the dose imparted to the patient during the conventional x - ray examination , a rando phantom was exposed , using the imaging protocol that was previously employed with patients , including : skull ( anteriorposterior ap and lateral lat projections ) , cervical spine ( ap and lat ) , dorsal spine ( ap and lat ) , lumbar spine ( ap and lat ) , pelvis ( ap ) , ribs ( ap , oblique and ap inferior ) , humera ( ap ) and femura ( proximal and distal ap )  . 
it has been demonstrated that it is a valuable tool for routine dose measurements and somatic risk assessment [ 25 ]  . conventional xray effective dose evaluation a practical way to estimate the effective dose e during conventional x - ray examinations is based on measured dap values and dap - to - e conversion coefficients . the effective dose of a single radiograph ( er , p ) is estimated as the product of the dapr , p recorded during the radiograph by the dap - to - e conversion coefficient ( taken from literature ) : er , p dapr , p ( e / dap ) r , p , where r and p indicate the anatomic region irradiated and the view , respectively [ the conversion coefficient ( e / dap ) r , p represents the effective dose per unit dap ( msv / cm2 ) ]  . the effective dose of the complete examination is dapr , p ( cid : 30 ) dap ( cid : 29 ) r , p ( cid : 31 ) r , p 1 3 98 fig . 
if data are separated by sex cm are obtained for males and and kv , 397 and 368 mgy females , respectively , at 120 kv , whereas 628 mgy cm is the mean dlp at 140 kv . 
 [ 17 ] for the adult antropomorphic phantoms , male and female , considered in the above mentioned work . based on the dlp values summarized in table 2 and fig . 
 the correction factor for head and neck geometry was included , producing on average an increase of less than 6 % in the estimated effective doses , with respect to the values table 2 in this table the mean values of the wbldmdct dlps are shown , separated by patient sex ( m stands for males and f for females ) and x - ray tube high voltage ( 27 subjects were scanned at 120 kv and only 2 male subjects were scanned at 140 kv ) meandlp all subjects mgy meandlp mgy meandlp mgy the value reported in the 1st column was obtained averaging across all subjects no female subject was scanned at 140kv obtained without the correction factor . 
a further change was also produced by including the patient weight factor [ 23 , 24 ] ( data shown in the 6th column of the table 4 )  . 
1st column : values obtained using sex - averaged dlp - to - effective dose cc for all subjects ; 2nd column : values obtained using sex - specific dlp - to - effective dose ccfemale group ; 3rd column : values obtained using sexspecific dlp - to - effective dose ccmale group ; 4th column : values obtained using sex - specific dlp - to - effective dose cc and pwcffemale subjects ; 5th column : values obtained using sex - specific dlp - to - effective dose cc and pwcfmale subjects cc conversion coefficients , pwcf patient weight correction factor , f females , m males discussion ct , due to its general high - level dose , has been object of recommendations addressing radioprotection aspects [ 20 ] and still remains the main contributor to the collective dose [ 17 , 22 , 26 ]  . 
also high - level radiation doses are given to organs included in the irradiated volume , but of no interest for the examination , for instance the eye lens during a head ct or the breast during a chest ct . several studies have been carried out to estimate the cancer risk related to the ct technique , following the enormous technological development that has favoured the extension of the field of application and also an increasing interest in total body studies [ 27 , 28 ]  . in the case of the wbldmdct the radioprotection problem is reduced by the possibility of obtaining good quality imaging with low dose , thanks to the high intrinsic contrast of bone . 
an improved image quality is obtained as a consequence of the use of ir that allows image noise reduction , estimated to be 40 % for this protocol , with respect to the image noise that would be measured , for the same dose , using conventional reconstruction . 
for the same scan parameters , sex - specific conversion coefficients cause an effective dose rise higher by about 16 % on average for females with respect to males , although dlp values are lower for females with respect to males . 
in fact , conversion coefficients for females are higher than those calculated for males , owing to differences in body size , organ position and organ weighting factors [ 17 ]  . 
5. image - j was used to open and process images . conventional xrayrando dose data table 6 shows the dap values recorded reproducing the conventional protocol for the study of the whole skeleton with the anthropomorphic rando phanto the effective dose values obtained for each single image are reported in the same table . 
1st column : body region imaged ; 2nd column : kind of view ; 3rd and 4th columns : beam size ; cm2 ] ; 9th 5th and 6th columns : exposure parameters ( kv and mas ) ; 7th column : dap ; 8th column : dap - to - e conversion coefficient [ msv / gy column : estimated effective dose e [ msv ] ap anteriorposterior , lat lateral , obl oblique , l left , r right concern chest , abdomen and pelvis coefficients , whereas head and neck coefficients are very similar for males and females . body weight factors cause dose decrease for subjects with body weight greater than those of the reference phantom and dose increase for subjects with body weight lower than those of the reference phantom [ 22 , 23 ]  . 
in our study , the inclusion of the weight factor has produced a further increase of the difference between males and female from 16 to 28 % , due to a higher body weight of the males with respect to the male reference phantom ( on average 10 kg ) , with a consequent dose decrease . behind this inter and intra gender variability , the dose values estimated in our institution are consistent with data reported in literature . 
these values are lower than those due to a traditional ct investigation of a single segment like chest or abdomen , with typical dose values ranging from 6 to 15 msv [ 29 ]  . in our study the effective dose estimated for the reference male was 3.1 msv , that is about 2.5 - fold higher than the dose of the corresponding conventional x ray study . 
 nevertheless , the advantages of the ct technique with respect to the conventional x ray to study mm patients skeleton have been assessed in several studies [ 2 , 57 , 30 ]  . 
it depends on the intrinsic features of the technique : the high spatial and contrast resolution , the absence of interposition in the evaluation of complex anatomical structure , such as spine , pelvis and ribs , the ability to depict simultaneously extraosseous localizations of the disease . 
overall , in agreement with the above mentioned authors , we also found such an improvement in diagnostic accuracy of ct examination to justify the dose increment . also significant advantages are achieved for the patient , usually elderly and suffering from bone pain . another favourable aspect is represented by the age of the subjects undergoing this protocol . 
in fact , the stochastic risk decreases with increasing age , in elderly people ( years ) about 10 times lower than in paediatric population 1 3 radiol med ( 2016 ) 121 : 93105 fig . 
6 a axial ct images nicely depict small lytic lesions within the skull ( a ) , in the pelvis ( b ) , in a thoracic vertebra and the adjacent rib ( c ) , undetectable or easily overlooked in a x - ray examination ; reformatted sagittal ct image shows numerous lytic lesions and multiple compression fractures in the thoracic and lumbar spine ( d ) ; reformatted coronal ct image shows an endomedullary soft tissue nodule in the humerus with minimal scalloping ( e ) ; axial ct image shows a huge solid mass destroying the thoracic vertebra and the rib and extending in the adjacent soft tissue of the thoracic apex ( f )  . 
b incidental finding : a 16 mm left pulmonary nodule ( g ) and a right lower lobe apical segment consolidation ( h ) 1 3 104 radiol med ( 2016 ) 121 : 93105 [ 31 ]  . 
the risk averaged across the whole population is about 5 1 [ 15 ]  . 5 msv 10 in terms of economic cost , a rough estimation indicated that the two methods are equivalent . then , on the whole , the adoption of the wbldmdct as an alternative to conventional radiography is advantageous . conclusions the effective dose evaluated for the wbldmdct protocol recently adopted in our institution has shown to be on average 3.2 msv , a little bit lower than the values reported in previous studies , with a difference between males and females due to sex - specific conversion factors and body weight factor that cause in the latter on average a dose increase of about 28 % than that for the former . 
considering the mean value obtained for the standard male , the effective dose is about 2.5 times the dose evaluated for the examination of the skeleton in toto based on conventional method . 
study evaluates the pre - treatment target volume measured prior to the treatment on the ce t1 - weighted sequence and the mrgfus - treated volume ( mrgfus - tv ) , represented by the volume of the lesion ablated , measured directly by means of the mrgfus . 
adenomyosis is a disorder characterized by growth of ectopic endometrial glands and stroma deep within the myometrium that determines a diffused enlargement of the uterus which microscopically exhibits ectopic , non - neoplastic endometrial glands and stroma surrounded by hypertrophic and hyperplastic myometriuthis former adenomyosis definition , described by bird et al . 
the diffused form of adenomyosis is an ectopic and diffuse growth of the endometrium cells into the myometrium with either diffuse or focal widening of the endometrial / myometrial junctional zone . 
the common symptoms include heavy menstrual 1 3 154 radiol med ( 2016 ) 121 : 153161 bleeding ( 4050 % ) , dysmenorrhea ( 1530 % ) and metrorrhagia ( 1012 % ) that involve a great stress for women . 
 adenomyosis is asymptomatic in 30 % of the cases . diagnosis and definitive treatment for adenomyosis has been hysterectomy , but today the identification of adenomyosis is allowed through the trans - vaginal ultrasound ( tvus ) and magnetic resonance imaging ( mri ) [ 7 ]  . 
 magnetic resonance imaging ( mri ) is a highly accurate noninvasive technique for the diagnosis of adenomyosis characterized by high sensitivity ( 7088 % ) and specificity ( 6793 % )  . 
typical mr features include either diffuse or focal thickening of the junctional zone or an ill - defined area of inhomogeneous and low signal intensity in the myometrium on the t2 - weighted mr images . 
adenomyosis is diagnosed when patients present a non - uniform junctional zone , more than 12 mm in width [ 8 , 9 ]  . therapeutic approach of adenomyosis is complex , especially when it affects fertile women who desire future pregnancies . 
medical therapy , which has been widely used up to now , gives only a symptom control without an effective control on the pathological process , and hysterectomy has been the only radical therapy . 
the efficacy of these drugs in the control of the pathological process has not been demonstrated yet , nevertheless there is an improvement of symptomatology , in particular in cases of dysmenorrhea and menorrhagia . 
adenomyosis embolization is an interventional radiology procedure that induces a hyaline sclerosis process by coagulation necrosis with progressive dehydration , shrinkage and reduction in the lesion volume with resolution of symptoms in a high percentage of cases ( 8595 % )  . 
due to the risks of angiography , use of contrast media , and embolization of target and non target organs , ideal patients are women in the peri - menopausal age , who do not want a pregnancy [ 10 , 11 ]  . 
embolization is carried out to treat symptomatic adenomyosis , although medical literature does not offer such a large number as for uterine fibroids . magnetic resonance - guided focused ultrasound surgery ( mrgfus ) is a novel technology used since the 1990s and also utilized for bone lesions treatment [ 12 , 13 ] , and represents a new frontier in the treatment of adenomyosis . 
it is a largely used interventional extra - corporeal technology , already used for the uterine fibroids and other solid lesions , that allows the ablation of deep tissue without surgical skin incisions . 
the association of this technique with mri as a guide of imaging ( mrgfus , magnetic resonance - guided focused ultrasound surgery ) is the new avant - garde technology allowing a real - time treatment modification based on the anatomical variability of the patients [ 14 ]  . 
1 typical case of focal adenomyosis of anterior uterine wall in a 48 - year - old woman with a pre - treatment target volume ( pre - tv ) of 29.7 cc ( a )  . 
in the mri t1 fat - sat sequence without ce the hemorrhagic focus into the lesion is observed ( b ) 1 3 radiol med ( 2016 ) 121 : 153161 fig . 
the aim of our study was to evaluate the effectiveness of mrgfus in adenomyosis treatment and to demonstrate the efficacy in terms of imaging and clinical results . materials and methods an informed consent was obtained from the patients before all procedure , and the study was approved by the institutional research ethics committee and has been performed in accordance with the ethical standards . patients and inclusion criteria from october 2011 to march 2013 , 23 patients , aged between 28 and 51 years ( mean age 39.5 ) , affected by adenomyosis and diagnosed using mri , were evaluated in our study . 
scan plan thickness was 4 mm and spacing 0.4 mthe same mri protocol was adopted for the diagnosis and for the post - treatment control ( table 1 )  . 
five out of 23 patients were excluded from mrgfus treatment due to their specific contraindications to the treatment , according to exablate guidelines for treatments [ 16 ] ( table 2 ) , and to the absence of a proper acoustic window to the ultrasound pathway . 
patients presenting interposition of metallic devices , scars or other structures such as bowel , bone or bladder in the path of the ultrasound beam were excluded to avoid damages . 
an accurate evaluation of the distance between the pathologic lesion and the skin line led us to adopt a 14 cm limit for the ultrasound beam focalization . eighteen patients affected by adenomyosis were treated using mrgfus . 
seven out of 18 patients ( aged between 37 and 49 years ) presented a diffuse form of adenomyosis and 11 out of 18 ( aged between 28 and 51 years ) had a focal form of adenomyosis . 
in order to obtain a clinical evaluation of the symptomatology , all patients , before the treatment , filled a uterine fibroid symptom and health - related quality of life - questionnaire ( ufs - qol ) [ 17 ]  . 
the eight symptoms questions of the ufs - qol were evaluated using a scale , assigning five scores to each question with a final 1 3 156 radiol med ( 2016 ) 121 : 153161 table 2 exclusion criteria of mrgfus treatment 1 . 
patient has unstable cardiac status including unstable angina pectoris on medication ; documented myocardial infarction within 6 months of protocol entry ; congestive heart failure requiring medication ( other than diuretic ) ; currently taking antiarrhythmic drugs ; severe hypertension ( diastolic bp > 100 on medication ) 4 . 
higher score indicated more severe symptoms [ 8 ]  . mrgfus treatment method and technical approach the mrgfus platform is integrated in a table docked within a magnetic resonance ( mr ) scanner . 
the patient lies in prone position upon a gel pad coupled to a water tank that is used to propagate the ultrasound beam with the lower abdomen centered on the transducer space . 
 the treatment plan consists of drawing the target lesion , using t2 - weighted sequences mr and to identify the surrounding critical structures including the bowel , spine and neurovascular bundles . 
after this evaluation , the number of sonications ( amount ablated volume ) required for the thermal ablation is defined and the safety path of the ultrasound beam is verified . 
patients were previously prepared , using a bladder catheter which allows to keep the bladder empty and to control uterine movements during treatment and an endorectal catheter containing ultrasound gel ( approximately 180 cc ) , in order to space the uterus from the sacral region and to protect the sacral nerve from thermal injury . 
pain medication with morphine , gastro - protective agents and antiemetic drugs was administered at the end of the treatment through an infuser pump ( the process lasts 1015 h )  . 
an exablate system ( insightec - israele ) was employed in association to ge signa excite mri unit ( magnetic field strength 1.5 t ) as a guide to the treatment . 
the technical plan was characterized by the use of a high - energy - grid sonication with the possibility to use a high temperature ( up to 6000 j ) in order to treat a more vascularized part of the tissue . 
the mean energy delivered for each patient was 3450 j ( minimum value of 1300 j and maximum value of 5600 j ) according to the different sensibility of the tissue and the results of the thermic map . 
3 comparison between the pre - treatment image ( a ) and the control made at 1 year from the treatment ( b ) on the t2 - weighted images . 
substantial recovery of the uterine morphology and the jz is observed 1 3 radiol med ( 2016 ) 121 : 153161 zone was evaluated in the area of major thickness . 
at the end of the procedure , the treated volume ( mrgfus - tv ) , represented by the volume of the lesion ablated at the end of the treatment , directly obtained from the exablate measurement system , were measured . 
the follow - up was carried out with the same protocol used in the pre - treatment mri , and it was performed immediately after treatment , after 3 , 6 , and 12 months from the treatment to monitor the reabsorption of the necrotic area . 
a reduced size of the spot length of sonication was employed ( ranging from 4 to 6 mm ) to treat a peripherical small part of the lesion , and thanks to a shorter cooling time between the sonication , the longest treatment lasted about 3 h . results mri data analysis the pre - treatment target volume was measured prior to the treatment on the ce t1 - weighted fat - sat sequence and that is the area which must be treated with ultrasound beathe junctional zone thickness was measured on the t2 - weighted sequence , making a comparison between the pre - treatment and the post - treatment values ( after 1 year )  . 
6 comparison between the pre - treatment image ( a ) and the control made at 1 year from the treatment ( b ) on the t2 - weighted images . 
most of the studies were carried out on older women who underwent hysterectomy that represents the most radical treatment but not suitable for women desiring to get pregnant [ 19 ]  . 
the possibility to treat adenomyosis using adenomyomectomy ( more local surgery ) is usable in focal forms according to the type and extent of adenomyosis as well as the modes of surgery . 
adenomyosis may be treated using drug therapy such as gonadotropin - releasing hormone agonist therapy ( gnrha ) , but this therapy permits an improvement of the symptoms , but they do not permit a control of pathological process . 
uterine artery embolization is a therapeutic possibility but is suitable for peri - menopausal women and not for fertile women [ 21 , 22 ]  . mrgfus is a promising noninvasive technique that allows thermal ablation of some tumors including uterine myoma [ 8 ]  . 
it permits a personalized treatment plan with a perfect anatomical evaluation of the target area and an effective evaluation system to reach the lesion avoiding sensitive structures and to define the most direct way possible which does not damage healthy components . 
mrgfus determines ablation of the adenomyosis tissue through coagulation necrosis , subsequent reabsorption and reduction in thickness of the junctional zone , and a global reduction in the uterine volume is obtained . 
adenomyosis is often associated to uterine fibroids , and within the limits of feasibility , ablation of both lesions during the same session can be performed . our study shows excellent results in terms of final treated area , representing the part of the lesion incurred in coagulation necrosis . 
the reason can be found in the histological nature of the adenomyotic tissue , sensitive to hormone stimulation and continuously bleeding into the myometrium , determining an inelastic and soft spongy tissue . 
the mri evaluation performed after 1 year from the treatment showed in 15 patients no evidence of recurrence of the pathology in the treatment area with thinning of the junctional zone . 
these women were affected by a diffuse form of adenomyosis more difficult to treat due to the large extension of pathology and to the impossibility to treat the entire wall and to perform the treatment successfully . 
the diffuse forms of adenomyosis were treated to obtain a reduction in the symptoms in the pre - menopausal women , and avoid surgery . limitations of our study were represented by a low number of patients involved and a short follow - up . 
however , the positive results obtained regarding the reduction in the symptoms , the improvement of the quality of life and the large extension of the treated volume make this technique a valid therapeutic alternative . 
many qualitative evaluations of digital breast tomosynthesis were previously performed by using a phantom with an unrealistic model and with heterogeneous background and noise , which is not representative of real breasts . 
three algorithms were compared : a back - projection ( bp ) algorithm , a filtered bp ( fbp ) algorithm , and an iterative expectation maximization ( em ) algorithto compare the algorithms , three types of breast phantoms ( homogeneous background phantom , heterogeneous background phantom , and anthropomorphic breast phantom ) were evaluated , and clinical images were also reconstructed by using the different reconstruction algorithms . 
the in - plane image quality was evaluated based on the line profile and the contrast - tonoise ratio ( cnr ) , and out - of - plane artifacts were evaluated by means of the artifact spread function ( asf )  . 
the results showed that the cnrs of masses reconstructed by using the em algorithm were slightly higher than those obtained by using the bp algorithm , whereas the fbp algorithm yielded much lower cnr due to its high fluctuations of background noise . 
the fbp algorithm provides the best conspicuity for larger calcifications by enhancing their contrast and sharpness more than the other algorithms ; however , in the case of small - size and low - contrast microcalcifications , the fbp reduced detectability due to its increased noise . 
the em algorithm yielded high conspicuity for both microcalcifications and masses and yielded better asfs in terms of the full width at half maximuthe higher contrast and lower homogeneity in terms of texture analysis were shown in fbp algorithm than in other algorithms . 
future work using these algorithms and considering the type of the breast and the acquisition techniques used ( e.g. , angular range , dose distribution ) should include the use of actual patients or patient - like phantoms to increase the potential for practical applications . keywords digital breast tomosynthesis filtered back - projection iterative reconstruction algorithm anthropomorphic breast phantom introduction breast cancer is the most frequently diagnosed invasive cancer among females worldwide . 
it accounts for 3040 % of all female cancers and ranks second as a cause of cancer 1 3 82 radiol med ( 2016 ) 121 : 8192 death in american women after lung cancer ; these rates are much higher in developed nations than in developing ones , and the risk of breast cancer increases with an age increase . 
the significant decrease in breast cancer , which amounts to approximately 30 % since 1990 , is a major achievement in cancer research and is due in large part to detection at earlier stage of breast cancer through screening mammography . 
in the usa , women over the age of 40 are encouraged to undergo the screening mammography every 1 or 2 years [ 13 ]  . screening mammography is a diagnostic technique whose use reduces the number of deaths from breast cancer by allowing early detection based on a low - cost , fast , and noninvasive x - ray study . 
in conventional mammography , a single x - ray is acquired , or two images in craniocaudal view and mediolateral oblique view are acquired in a routine series [ 4 ]  . 
moreover , the single projection of two - dimensional x - ray images entails the superposition of objects in the image , which may cause objects of interest to be obscured , or can produce pseudoobjects that mimic a disease , for example , pseudomasses and loss of microcalcification . 
to overcome the tissue superposition problems of conventional 2d mammography , digital breast tomosynthesis ( dbt ) was developed ; in dbt , a series of projections is acquired , while the x - ray tube is rotated over a variety of angles through the compressed breast , and slices of breast are generated to allow the extraction of 3d information about the breast tissue . 
compared to computed tomography ( ct ) , in which projections are acquired over a 360 range of angles , the projections used in digital breast tomosynthesis are acquired over a limited range of angles , for example , 11 for the philips microdose system and 50 for the siemens mammomat inspiration system [ 9 , 10 ]  . 
the resulting tomosynthesis images have much better spatial resolution than those of ct images within the slice , but have poorer resolution in the depth direction , between the slices [ 11 ]  . basic tomosynthesis projections are obtained , each from a different scanning angle , while an x - ray tube is rotated over the compressed breast . 
these projections are later combined by shifting the projections relative to each other and superimposing ( adding ) them to bring different planes within the patient into focus which is called simple shiftand - add ( saa ) technique . 
in the present work , we investigated methods for quantitative evaluation of tomosynthesis reconstructions ; we used different types of breast phantom which represent different characteristic breast and also patient images to validate the effects of the algorithms on the resulting images , both quantitatively and qualitatively . 
the detector for the dbt system was optimized for very low exposures and rapid readout . for tomosynthesis imaging , 21 projections by rotating the x - ray tube over a the system acquires 25 fig . 
the pixel gain setting was chosen to be a low full mode , enabling high sensitivity with a low dose per frame ; this mode was optimized for fluoroscopy , cone - beam ct , and tomosynthesis . 
the source - to - imager ( csi surface ) distance ( sid ) was 665 mm , and the center of rotation ( cor ) of the x - ray tube was 33 mm above the detector surface . 
table 1 lists the major parameters of the tomosynthesis acquisition . the average glandular dose ( agd ) for dbt was calculated by using a simple extension of dosimetry for conventional mammography developed by dance et al . 
the feldkamp algorithm , a well - known approximate cone - beam algorithm adapted from the fan beam algorithm , was selected as the fbp algorithm used in this work . 
fbp algorithms obtain the log data ( ) based on 2d data projected by using the attenuated intensity ( i ) and the initial intensity ( i0 ) , and then this log data is fourier - transformed [ 16 ]  . 
then an inverse fourier transform is performed to obtain the tomosynthesis image . in the filtering process , a ramp - type filter is generally used to compensate for the blurring introduced by the backprojection . 
 the apodization filter used is defined as follows : ( cid : 31 ) ( cid : 30 ) 2 ( cid : 29 ) 1 + cos ( cid : 29 ) elsewhere ; a ( cid : 28 ) ( cid : 28 ) for y ( cid : 27 ) ( cid : 27 ) ( cid : 27 ) ( cid : 27 ) the parameter a ( a > 0 ) is used to suppress high frequencies and thereby noise . compared to that of conventional ct , the scanning geometry used in tomosynthesis is acquired from only a limited angular range with respect to the object . 
after applying a filter in a plane that is parallel to the detector plane , there are still increased out - of - plane artifacts due to the incomplete sampling of tomosynthesis . 
the third filter , which is called the slice - thickness filter , represents a constant depth resolution to a certain degree and controls the spatial sensitivity profile to reduce the out - of - plane artifacts typical in digital breast tomosynthesis . 
the statistical method is to reconstruct the image based on analysis of the process of x - ray photons measured by statistical means , based on an iterative algorithfbp is based on a mathematical method , and the em algorithm is one of the 1 3 84 radiol med ( 2016 ) 121 : 8192 statistical methods . 
the em algorithm is used to find the maximum likelihood parameters that maximize the probability of the true probability , and f can be obtained indirectly by means of the em method . 
in each iteration of the em algorithm , the current image estimate f is updated as follows : j = f m1 ( cid : 31 ) i mij ( cid : 30 ) mijgi ( cid : 31 ) l milf m1 where gi is the projection data and mij is the probability that a photon emitted from the jth pixel reaches the ith detector pixel . 
the phantom was designed to assess the detectability of lesions of various sizes within a tissueequivalent , complex , heterogeneous background , thereby providing more realistic challenges for this study . 
figure 2a shows the first phantom , a homogeneous background breast phantom ( model 011a , cirs , usa ) whose shape is realistic compressed breast to evaluate in terms of contrast or noise . 
simulated calcifications , fibrous ducts , to quantitatively evaluate the image quality of a reconstruction of the in - focus plane , its line profile and contrastto - noise ratio ( cnr ) were estimated . 
the mass line profile was also evaluated by using the mass size of 4.76 m eight consecutive rows across the mass were averaged and normalized to the highest intensity to compare the three reconstruction algorithms . the cnr is defined as is ( z ) ib ( z ) b ( z ) cnr ( z ) = where is and ib are the mean pixel values of the signal regions of interest ( roi ) and background roi at depth z , respectively ; b is the standard deviation of pixel values in the same background roi . 
a mass of size 4.76 mm and composed of 75 % glandular and 25 % adipose tissue was used for the cnr evaluation . to evaluate the z - resolution , which is the image blur in the z direction ( perpendicular to the reconstruction plane ) , the artifact spread function ( asf ) was calculated for the microcalcification in the first speck group . 
2 three types of breast phantom used in the present study : a breast phantom with homogeneous background , b 3d breast phantom br3d , c anthropomorphic breast phantom rachel 1 3 radiol med ( 2016 ) 121 : 8192 represents the artifact effect of features in the adjacent offfocus planes ; the artifacts are generally stronger in image planes that are closer to the plane in which the real feature is located . 
for each patient breast , the in - plane reconstructed images were evaluated with different reconstruction methods . asf ( z ) = is ( z ) ib ( z ) is ( z0 ) ib ( z0 ) results where z0 is the location of the in - focus plane of the feature and z is the location of an off - focus plane of interest ; the roi of signal was placed in a 4 4 pixel area at the center of the microcalcification , and the roi of background was measured in the same manner used for the cnr evaluation . 
the microcalcifications in the first speck group of nominal size 0.400 mm were evaluated , and the corresponding asf was estimated by averaging three replicate measurements of six microcalcifications in the speck group . 100 texture analysis was performed on anthropomorphic phantom images with different reconstruction algorithms ( matlab r2010b ; mathworks , natick , mass )  . 
contrast of a texture is defined as the variation among all gray levels in the roi , which is based on the repeated occurrence of gray - level configuration in the roi . 
in this study , the texture features were extracted using gray - level co - occurrence matrices ( glcm ) , and c is the normalized co - occurrence matrix . 
the results were normalized to the peak intensity , identified as that of the most intense pixel , and averaged by using line profiles acquired from six microcalcifications in one cluster . 
the em yielded the highest sharpness for the first cluster of microcalcifications , which were of high contrast and large size , and the rest of the results were between those from bp and em . 
microcalcifications in the speck group of nominal size 0.400 mm were selected for quantitative analysis in consecutive ten slices , and the fwhms of the asfs for this group were averaged over the six specks . 
the asf curves of the bp algorithm were wider than those of other algorithms , and those of the em algorithm diminished the most quickly with distance from the lesion layer . 
the bp algorithm results allowed all the specks to be detected , with low contrast and low background noise ; the em results clearly showed all the specks with high contrast and low background noise . 
contrastingly , the fbp algorithm amplified the background noise to a high level , making it difficult to clearly observe some of the low - contrast microcalcifications . figure 9 shows reconstructed images of three masses acquired by using the heterogeneous breast phantothe 1 3 radiol med ( 2016 ) 121 : 8192 fig . 
4 line profiles evaluated for a mass of size 4.76 mm ; eight consecutive rows across the mass were averaged and normalized to the highest intensity to compare the three reconstruction algorithms fig . 
5 reconstructed images of a group of masses acquired by using the homogeneous background phantom acquired from bp ( a ) , fbp ( b ) , and em ( c ) algorithms embedded speculated masses provided low contrast , and in particular , the second mass overlapped with complex tissue structures . 
in bp images , the first and third masses were observed with very low contrast , and it was very difficult to observe the second mass due to the algorithms blurring . 
8 to confirm the effect on small - size and low - contrast microcalcifications , microcalcification group 5 acquired from bp ( a ) , fbp ( b ) , and em ( c ) algorithms with nominal speck size of 0.165 mm was evaluated fig . 
10 cc view of anthropomorphic phantom acquired from bp ( a ) , fbp ( b ) , and em ( c ) algorithms represented by 50 - mm compressed breast with 50 % glandular tissue and 50 % adipose tissue texture as much as the fbp reconstruction did , but had the advantage that the enhancement of highand lowcontrast textures was balanced throughout most parts of the breast . evaluation of glcm texture for each reconstruction algorithms is shown in table 2 represented with contrast and homogeneity for four directions . 
11 reconstructed images from patient 1 with a soft tissue mass and breast calcifications in the right breast ( ac ) and those from patient 2 with mass in the left breast ( df ) ; bp images ( a ) and ( d ) , fbp images ( b ) and ( e ) , em images ( c ) and ( f ) bp algorithm and em algoriththe increased contrast of fbp indicated that the amount of local variations present in an roi is noticeable . 
the lowest homogeneity was estimated with fbp algorith the homogeneity showed the closeness of the distribution of elements in the region , and lower homogeneity indicated high variation . the rcc tomosynthesis images from patient 1 ( ac ) and lcc tomosynthesis images from patient 2 ( d , e ) are shown in fig . 
the border of the cancer and the conspicuity of microcalcification groups were clearly demonstrated with fbp reconstruction , although the low contrast of mass was hard to discriminate due to relatively significant background noise as shown in fig . 
the em images resulted in high visibility of low - contrast mass with clear border of soft tissue . the lmlo tomosynthesis images from patient 3 who was diagnosed with irregular shape of masses in left breast ( ac ) and lcc tomosynthesis images from patient 4 who had a spiculated margin of mass in left breast ( d , e ) are shown in fig . 
12 reconstructed images from patient 3 ( ac ) and those from patient 4 ( df ) with a breast cancer in the left breast ; bp images ( a ) and ( d ) , fbp images ( b ) and ( e ) , em images ( c ) and ( f ) radiol med ( 2016 ) 121 : 8192 discussion and conclusion in this paper , we demonstrated and validated methods for comparison of breast tomosynthesis reconstructions using different types of breast phanto although breast tomosynthesis system yielded results superior to those of conventional mammography , the optimal acquisition geometry ( e.g. , angular range , number of projections ) and optimal acquisition techniques ( e.g. , target / filter , tube voltage , exposure ) for breast tomosynthesis are still being investigated . 
 [ 22 , 23 ] previously used the same prototype tomosynthesis system used herein to compare multiple acquisition protocols , varying projection angles , and projection numbers , using uniform and nonuniform angular spacing and using uniform and nonuniform distribution of x - ray exposure ; they reported the effects of these acquisitions and demonstrated the optimized acquisition parameters led to the optimal image quality for this syste not only the acquisition parameter optimization , but also reconstruction algorithms , is required to characterize and optimize in terms of image quality and time - consuming for computation time . the digital breast tomosynthesis systems in clinical use or under development are applying different types of reconstruction methods . 
in this paper , we compared three algorithms including bp , fbp , and em and investigated the effects of the reconstruction algorithms to improve their potential use in practical situation . qualitative assessments depending on various types of reconstruction methods generally require the imaging and interpretation of test objects or a phantom with features and background structures that are not representative of those in real breasts . 
these objects were evaluated to demonstrate the compatibility of results among different breast types and make more meaningful subjective comparisons of reconstruction algorithms . all the three algorithms ( bp , fbp , and em ) used in this study were used to separate superimposed tissues observed in 2d mammograms . 
the fbp algorithm provided the best conspicuity and sharpness for large and high - contrast calcifications with homogeneous background phanto it also provides significant background noise which leads to poor detectability of small and low - contrast calcifications and masses . 
in homogeneous phantom images , the bp algorithms showed cnr results that were superior to fbp algorithms because of significantly low background noise , and however , the conspicuity of lesions was clearly better with fbp algorithms due to the high - contrast results . 
for heterogeneous 1 3 radiol med ( 2016 ) 121 : 8192 background phantom , the fbp algorithms provided high conspicuity for large calcifications compared to other algorithms , and however , few clusters of small size and lowcontrast microcalcifications were seen due to the amplified background noise with anatomic noise . 
in clinical images , the border of cancer and ductal networks was clearly seen with fbp algorithms , and the em algorithm resulted in high visibility of microcalcification and low - contrast mass and texture . 
regarding future work , because many factors need to be considered when optimizing a tomosynthesis system , the use of the dbt system with different reconstruction algorithms should be studied including the optimal filter design or threshold frequency for fbp and iteration number for em including the computation time . 
 the computation time for the iterative em reconstruction was much longer than that required for the bp and fbp reconstructions . recently , the potential and interest for the dbt system have been increasing , not only as a replacement for 2d mammography screening for breast cancer but also as an additional test for recall patients . 
moreover , considerations of the type of breast composition , the acquisition techniques , and the use of actual patient or patient - like phantoms may increase the dbt systems potential for practical applications . acknowledgments we would like to acknowledge financial support from the r&d convergence program of the national research council of science and technology of the republic of korea ( grant cap13 - 3 - keri )  . 
we have identified 249 young adult patients ( 178 men and 71 women ; age range 1440 years ) who had received more than one mdct study between june 2010 and june 2014 . 
dose distribution for the various organs analysed ( breasts , ovaries , testicles , heart and eye lenses ) shows an intense peak for lower doses , but in some cases high doses were recorded . 
17 , 90128 palermo , italy keywords mdct effective dose adsorbed dose tissue - weighting factors cumulative doses introduction multidetector computed tomography ( mdct ) is increasingly used in trauma imaging due to its efficiency as a diagnostic tool , providing simultaneously speed , high resolution and large body coverage for diagnostic evaluation of emergency patients [ 1 ]  . 
mdct represents actually the main source of radiation in trauma patients also because patients are referred to hospital for serious injuries and in a short period of time are usually submitted to multiple mdct examinations for initial diagnosis , follow - up and eventual surgical complications [ 3 ]  . in emergency care , mdct has certainly transformed patients management and its use is in constant growth ; in italy , at least 2 millions of examinations ( 29.9 % ) were recorded in 2009 in accident emergency ( a&e ) department on 6 millions of total amount of mdct examinations performed for year with an estimate annual increase rate of 8 % [ 4 , 5 ]  . 
the main concern in the use of procedures with radiation is the potential long - term effect of radiation exposure , namely the association between radiation and increased cancer risk [ 6 , 7 ]  . 
even though a cumulative risk is under strong debate and criticised by many international radiation protection authorities , some reports emphasise that some 1 3 radiol med ( 2016 ) 121 : 144152 patients receive very high cumulative dose from multiple radiological examinations [ 9 ]  . 
associated health risks from medical imaging are of major concern especially in young patients submitted to many radiological procedures in a short period of time due to trauma [ 3 ]  . 
 the aim of the present research was to evaluate the number of repeat mdct examinations in young adult patients in the last 4 years in a single trauma centre ( university hospital of palermo policlinico ) which potentially serve more than 1 million habitants . materials and methods we have identified retrospectively patients submitted to more than a mdct study for major trauma in a referral regional trauma centre . 
our centre is supplied with three mdct facilities in the a&e department and other two in the main radiology building ( the study was approved by the local ethical committee )  . 
the mdct unit dedicated in the a&e department and another emergency dedicated unit in the main radiology building are opened 24 h per day , 7 days a week ( 7 days a week , 24 h a day )  . 
from the radiology information system ( ris elefante agfa ) , we have selected younger adults ( range 1440 years ) who performed more than one mdct between june 2010 and june 2014 . 
for each patient , a spreadsheet file excel was build from ris and pacs metadata including : clinical purpose , date , age , mdct equipment , type of examination , use contrast compound , number of phases performed , body part examined and dose report . 
all the examinations were performed with two different mdct apparatuses : a 128slice mdct ( somaton definition as siemens healthcare installed in december 2011 ) and a 16 - slice mdct ( bright speed elite ge medical system installed in march 2010 ) , which is the mainly emergency dedicated apparatus . 
for each examination , the mdct scanners provided the computed tomography dose index ( ctdi vol ) and dose length product ( dlp ) values in gy * c in the examined period , the iterative software algorithm to reduce dose was not available in our department and was installed in july 2014 . 
every 6 months , both mdct apparatuses are controlled and ctdi has been measured and is measured by using phantom measure according to the european guidelines eur16262 / 1998 [ 11 ]  . 
in order to evaluate the estimated effective total dose and the effective dose to the various organs ( such as breasts , testicles , ovaries , prostate and eye lenses ) , we have used the ct - expo software version 2.2 ( hannover germany ) that provide information about estimated effective dose for various mdct apparatuses . 
once the user sets the acquisition parameters such as tension ( kv ) , current ( ma ) and duration of the examination , part of body exposed and patients gender , the software provided estimate values of the effective total dose and the estimate organ dose . 
however , the software cannot take into account the differences among patients in terms of mass , height and width ; this involves that for a given examination type the dlp values could differ slightly among patients . 
in order to overcome this issue , for each examination of each patient , the dose values were rescaled with respect to the dlp values provided by the mdct scanners . 
mdct main segments investigated were as follows : full - body examination as head , chest , abdomen and pelvis 14 ; chest , abdomen and pelvis 13 ; head and spine 11 ; head and chest 10 ; and other 11 . 
for each dose value , we have obtained the corresponding histogram plots and their average and median values . results in our department in the selected 4 - year period , we have identified 32 , 352 on 107 , 476 ( 30.01 % ) patients referred for trauma submitted to mdct . 
we found , through our retrospective analysis , 249 traumatic patients ( 71 females and 178 males ) who underwent more than one mdct ( average 2.8 examinations ) in a short period of time ( median 4 days ) for diagnosis , follow - up and eventual surgical complications due to trauma . 
many examinations were conducted with more than one phase for the use of contrast compound ; however , in 37 cases of noncontrast head ct , a second acquisition was performed due to artefact in uncooperative patients ; this event has been considered as a factor that increased dose exposure in these populations . 
second and eventual subsequent mdct scan after first examination was mainly focused on a single 1 3 147 breasts ( msv ) testicles ( msv ) heart ( msv ) eye lenses ( msv ) ovaries ( msv ) maximum value minimum value mean value median value standard deviation 1943 radiol med ( 2016 ) 121 : 144152 table 2 maximum , minimum , mean and median values of equivalent doses to various organs as : breast , testicles , heart , eye lenses and ovaries fig . 
we have observed a large variability in ctdivol and dlpw ; consequently , effective dose can vary significantly for different district examined and acquisition modality ( multiphase examinations ) used in trauma assessment , follow - up and eventual surgical follow - up or complications due to trauma ( table 1 )  . 
for the analysis of the effective dose absorbed by patients in the sample , we have estimated that the value of mean effective dose was about 27 msv ( range from 3 to 297 msv )  . 
the dose analysis performed provided also dose distributions to same organs of interest such as breasts , ovaries testicles , heart and eye lenses and pointed out the presence of an intense peak at low doses , but there is a tail of higher doses . 
 some traumatic patients received an impressive cumulative radiation dose as a 25 - year man ( suicide attempt ) rising an amount of 25 mdct examinations in 6 months ( the patient died in intensive care unit )  . 
5 distribution of testicle doses absorbed for male patients discussion mdct is the main choice in case of evaluation of traumatic patients , and their subsequent monitoring determines otherwise a significant increase in radiation exposure in general population [ 12 ]  . 
7 distribution of heart doses absorbed by patients showed that the number of traumatic young adult patients submitted to mdct is quite very high and mainly due to traffic accident . 
the data could be explained looking to the statistics of traffic accident ; in fact , in italy , in 2013 , there were 3385 deaths and 257 , 421 people seriously injured in car accident ; among them , one - third ( 968 ) had an age comprised between 20 and 44 years with a ( to ) peak for young adults of 2024 years and adults of 4044 years [ 15 ]  . 
these data lead to an increase in number of diagnostic tests , in most cases of mdct whose diagnostic benefit is beyond any doubt , but it creates the problem of multiple doses in patients with a long life expectancy . 
8 distribution of eye lens doses absorbed by patients radiol med ( 2016 ) 121 : 144152 that cumulative effective dose ( ced ) has been criticised by different authorities as radiation dose summit by nibib ( national institute of biomedical imaging and bioengineering ) that is known quantitatively about the benefits of specific imaging studies in a wide range of clinical settings and the risks of low level radiation exposure to individuals , it will be very difficult this benefit - risk trade - offs accurately [ 9 ]  . 
cumulative radiation dose is not widely accepted , but we have to emphasise that repeated examinations in a short time in young patients are certainly of some concerns [ 14 ]  . 
also looking to organ doses observed for both classical cancer effect ( breast , ovaries and testicles ) and noncancer effect ( eye lens hearth ) compared to recent ircp guidelines , we found that some trauma patients have received impressive dose that in some case exceeds limits for professional exposure . 
for cancer effect , probably two major studies emphasised risks of long - term cancer effects as pearce [ 16 ] in british childhood populations and mathews [ 17 ] data in australian children and adolescent populations . 
 eye lens dose is of concerns for the increased prevalence of eye lens opacities in staff exposed to radiation levels below the thresholds as established by the international commission on radiological protection ( icrp ) 60 in 1990 and icrp publication 103 of 2007 [ 8 ]  . 
the icrp commission has now reviewed , after recent epidemiological evidence , the set threshold in absorbed dose for the lens of the eye is 0.5 gy for the entire life span ( icrp statement on tissue reactions 2011 )  . 
for occupational exposure in planned exposure situations , the recommendation of the commission is an equivalent dose limit for the lens of the eye of 20 msv in a year , averaged over defined periods of 5 years , with no single year exceeding 50 msv [ 18 ]  . 
this recommendation is present in the new council directive 2013 / 59 / euratom laying down basic safety standards for protection against exposure to ionising radiations [ 19 ]  . 
other noncancer effect regards the circulatory syste in particular , it is well known that high doses ( > 5 gy ) of ionising radiation exposure produce damage to the heart and coronary arteries . 
in recent years , many studies have investigated cardiovascular diseases [ 2026 ] , proposing that doses higher than 0.5 sv cause an excess relative risk [ 22 , 23 ]  . 
 even though for doses smaller than 0.5 sv the assessment of damage is difficult and various studies are in progress , a possible increase in risk of cardiovascular diseases should be taken into account for repeated mdtc examinations . 
 [ 3 ] in trauma patients ( 11 , 676 ) submitted to different radiological examinations with either conventional radiograph and mdct ; cumulative effective dose ( ced ) in the 231 cases of repeated or multiple radiological examinations was 20 msv , but 27 patients received a ced of 100 msv . 
 [ 3 ] observed young traumatic patients in emergency department performing multiple diagnostic procedures , mainly mdct ; he described a mean ced per medical visit of 2.6 msv , with two age peaks between 1519 years and 4044 years . 
all the examinations were firstly justified according hospital guidelines ; the diagnostic information obtained from mdct were relevant for the survival of the patient , through the identification of lesions quickly and efficiently , but the relatively high - radiation doses associated with mdct compared with conventional radiography may raise possible long - term health risk [ 16 ]  . 
although there is no evidence and unique guideline on risks resulting from repeated exposure to ir , the growing number of repeated examinations , especially mdct examinations in young adults , is of some concern . 
young adults have , in radiobiological terms , a long life expectancy , and the lack of certain knowledge about the consequences of repeated exposure to low doses cannot be taken in account [ 16 ]  . 
mdct in trauma seems to be a victim of his own success and in many cases is the gold standard to assess trauma lesions for speed , availability and diagnostic performance ; however , use of mdct should be reduced in control examination if possible . 
when mdct scan is performed it is important to follow strictly the alara ( as low as reasonably achievable ) principle and adapt scan parameters to lower dose setting parameters . 
probably , software that monitors and tracks radiation dose may help radiologist and referring physicians to balance repeated examination and , depending on mr availability , avoid modalities that imply significant radiation dose as mdct . 
 ced in trauma patients results in a small sample to a significant radiation exposure similar or higher to professional exposure and in case of young patients is of some concerns . 
grant number : r2ffrad05 p84d . compliance with ethical standards conflict of interest all authors declare that they have no conflict of interest . ethical approval the study is retrospective , so for this type of study , formal consent is not required . 
post - therapy sensitivity , specificity , ppv , npv and accuracy of wb - mr / dwibs were 43 , 91 , 75 , 71 and 72 % , respectively . conclusion wb - mr / dwibs seems to be an appropriate method for the post - treatment assessment of patients affected by hl and anhl . 
a correct staging and monitoring of 1 3 radiol med ( 2016 ) 121 : 132143 therapy response is decisive for an early change in treatment and for a global therapeutic strategy . innovation in imaging techniques has improved the comprehensive evaluation of lymphomas , for both staging and prognostic assessment . 
it mainly consists of a higher cellularity and morphological changes in tumor cell and microenvironment [ 5 , 6 ]  . magnetic resonance ( mr ) , which allows the study of tissue ultrastructure , is without doubt the best imaging technique , and specific sequences have been recently introduced . 
in [ 7 ] , was developed on the basis of conventional diffusionweighted imaging ( dwi ) and has recently been combined with a specific free - breathing sequence for whole - body scanning ( wb - mr / dwibs ) , implementing the possibility to evaluate patients with systemic disease [ 8 , 9 ]  . the use of wb - mr / dwibs has been explored in hl and b - nhl , both retrospectively and prospectively [ 1 , 10 13 ]  . 
eligibility criteria were : at least 18 years of age , histological diagnosis performed on excisional biopsy according to the 2008 world health organization classification and measurable nodal and / or extra - nodal disease . 
exclusion criteria included contraindications to mr , such as a pacemaker , claustrophobia and metal implants , pregnant state , concomitant previous diagnosis of malignancy and / or previous chemotherapy . the local ethics committee approved this prospective study , and all patients gave written informed consent prior to entering the study . patients underwent physical examination , standard laboratory tests and contrast - enhanced computed tomography ( cect ) scans of the chest , abdomen and pelvis at baseline and at the end of therapy . 
response assessment was performed with both techniques at least 3 weeks after the completion of chemotherapy and / or 68 weeks after completion of radiation therapy . chesons revised response criteria for malignant lymphoma were used to assess tumor response at the end of the treatment course [ 4 , 15 ] , classifying patients in complete remission ( cr ) , partial remission ( pr ) , stable disease ( sd ) and progressive disease ( pd ) [ 4 , 15 ]  . 
the average acquisition time was about 25 m the examination was conducted from the head to the thighs , with four consecutive package acquisitions ( head / neck , thorax , abdomen and pelvis )  . 
in accordance with the literature , a coronal t1 - weighted ( t1w ) and stir and axial dwibs sequences were performed . the coronal t1w sequence was acquired with the q body coil for signal reception . 
dwibs axial images were reconstructed both on a radial plane ( 15 projections ) , for a volumetric view , and on a coronal plane ( slice thickness , 44 )  . 
the recon4 mm ; gap , 1 mm ; number of images structed images in the coronal plane were then merged for each station to obtain a coronal whole - body / dwibs image . 18ffdg pet / ct protocol images were acquired with a combined modality pet / ct discovery lsa ( ge healthcare , waukesha , wisconsin , usa ) that integrates a pet ( advance nxi ) with a 16 - slice ct scanner ( light speed plus )  . 
the ct acquisition parameters were : 340 ma ( auto ) , 120 kv , slice thickness 3.75 mm , tube rotation time 0.8 ms and collimation field of view ( fov ) of 50 c the ct data were used for attenuation correction of pet scanning , which was performed immediately after the acquisition of ct images . 
the average acquisition time was about 20 mpet was reconstructed with a matrix 128 , ordered subset expectation maximum iterof 128 ative reconstruction algorithm ( two iterations , 28 subsets ) , 8 mm gaussian filter and 50 cm field of view . 
 when infection or inflammation occurred as a pathologic confounding condition for visual dwibs evaluation , resulting in disagreement between morphological and visual criteria , we used morphological parameter . similarly , for each extra - nodal region , including bone marrow involvement , any areas with an altered signal in t1w or stir , showing signal intensity in dwibs higher than in surrounding tissues , were considered positive for lymphoma localization . 
when confounding conditions , as infection or inflammation , occurred , the semiquantitative analysis by using max standardized uptake value ( suv max ) was employed for a correct interpretation of pet examination . similarly , for each extra - nodal region , including bone marrow involvement , any area of visually focal or diffuse increased 18f - fdg uptake , higher than in the surrounding background , unrelated to physiologic or benign uptake , was defined as positive for lymphomatous involvement . 
by using an evaluation on a lesion - by - lesion basis , we calculated the overall agreement between the two methods in assessing both nodal and extra - nodal involvement and a specific agreement according to lymph nodal basin or extra - nodal site involvement separately . 
among them , 18 patients ( nine male and nine female ) , with a mean age of 48.9 years ( range 2381 years ) , received chemo / radiotherapy , completed the post - therapy evaluation and were considered in the analysis . 
eleven patients had a diagnosis of hl , and seven of anhl [ five diffuse large b cell lymphoma ( dlbcl ) and two mantle cell lymphoma ( mcl ) ]  . 
considering histotypes separately , sensitivity , specificity , ppv , npv and accuracy of wb - mr / dwibs resulted 100 / 20 , 80 / 100 , 67 / 100 , 100 / 60 and 86 / 64 % in anhl / hl , respectively . discussion a challenge to oncologists in the twenty - first century is to optimize individual patient treatment and avoid unnecessary toxicity and treatment delays . 
 this requires reliable methods that can assess response to therapy as early as possible , evaluating the entire body carefully . traditional methods ( ultrasonography , ct and mr ) mainly depend on the changes in tumor morphology , which need a relatively long period to regress completely [ 12 ]  . 
 previous studies showed that dwibs has great potential for clinical application in tumor staging , response assessment and follow - up [ 1015 ] , and many authors advocated wb - mr / dwibs as a potential competitor method for 18ffdg pet / ct [ 12 , 1822 ]  . 
our own previous study found good agreement between the two methods in the detection of nodal and extra - nodal localizations , in both hl and b - nhl [ 14 ]  . however , very few studies to date have compared the two imaging modalities in the treatment response assessment of patients affected by lymphomas . 
however , considering the lack of radiation with dwibs , it could have interesting implications for the pediatric age group , if these preliminary results were to be confirmed on greater sample sizes . our results demonstrated that the degree of agreement between the two methods was globally good by using an evaluation on a lesion - by - lesion basis : it resulted better in evaluating nodal involvement than extra - nodal sites of disease . 
in two patients , the discrepancy could be due to signal loss on dwibs of the small size of residual lymph nodes in the mediastinum , related to cardiac and respiratory motion . 
this disadvantage relevant for dwibs acquisition , which is performed with the patient breathing freely rather than holding their breath , is already known in the literature [ 13 , 14 , 24 , 28 ]  . 
 [ 13 ] , dwibs image interpretation is greatly influenced by the size criterion , but in the case of residual enlarged lymph nodes , the altered signal detected has to be interpreted with caution [ 1 , 23 , 28 ]  . another cause of false positive results on dwibs could be due to the effect of anticancer therapy . 
chemotherapeutic drugs produce cell membrane rupture and cause cell necrosis , resulting in decreasing cell density , which increases the mobility of water molecules accompanied with high signal intensity on dwibs [ 12 ]  . 
 one patient with splenomegaly in the staging phase , still present in re - staging , showed spleen high signal intensity on dwibs ; this false positive result was demonstrated by the subsequent follow - up . 
 however , splenomegaly alone cannot be used to establish splenic involvement by lymphoma because 30 % of normal - sized spleens can have tumor infiltration and splenomegaly can occur without tumor involvement [ 14 , 29 ]  . 
however , just one patient remained classified differently considering r / nr groups ( one anhl ) , with an agreement between the two methods in assessing response to therapy globally very good . 
discrepancies between the two methods , found mainly within hl , could be related to the different histopathological features , such as the heterogeneous cellular infiltrate consisting not only in 1 3 142 radiol med ( 2016 ) 121 : 132143 reedsternberg cells but also in an abundant reactive infiltrate with variable proportions of lymphocytes , histiocytes , eosinophils and plasma cells [ 10 , 30 ]  . 
therefore , the two methods provide complementary and not always exactly concordant information . on the other side , the patient who remained classified differently between the two methods was patient no . 
mainly , the population analyzed was small and heterogeneous for histological types ; however , the heterogeneity allowed us to investigate the role of dwibs in both hl and anhl patients with a sample number in line with the few studies in the literature . conclusion our preliminary study , performed to evaluate the reliability of wb - mr / dwibs in the therapy response assessment of patients affected by lymphomas , showed that wb - mr / dwibs could be a suitable method for this analysis , with a better performance in anhl than in hl , even if some discrepancies between the two methods have emerged from our study . 
ct could easily discriminate nf from other musculoskeletal infections , adds an important value to clinical and laboratory tests in diagnosis of nf in an emergency context when magnetic resonance imaging , which is superior to ct in this discernment , could not be performed . keywords necrotizing fasciitis lrinec score soft tissue infections computed tomography musculoskeletal infections introduction necrotizing fasciitis ( nf ) is a life - threatening soft tissue infection with high morbidity and mortality if not treated in its early stages . 
nf primarily involves the fascial layers and the subcutaneous tissue , while skin and muscle initially remain intact and it is characterized by necrosis that can lead to sepsis and multiple organ failure . when the muscular fascia is involved and necrosis is present is called necrotizing fasciitis , when the fascia is involved but is not necrotic is called non - necrotizing fasciitis ( non - nf )  . this discernment is quite important because in necrotizing fasciitis surgical debridement is mandatory instead in non - necrotizing fasciitis monitoring over time and antibiotics therapies are the first - line treatment and surgical debridement is not necessary until the necrosis appears . the most common sites of infection are the extremities ( primary the lower ) , abdominal wall and perineum [ 13 ]  . the diagnosis of nf is primarily clinical and it is supported by a clinical scoring system , the laboratory risk indicator for necrotizing fasciitis ( lrinec )  . 
lrinec score stratifies the risk of soft tissue infections in three groups : low risk with 5 points , intermediate 67 points , high risk > 8 points [ 4 ]  . on the other hand , at the state of the art , a radiological score which permits to stratify the risk to be affected by nf does not exist but some contrast enhanced computed tomography ( cect ) parameters are available to detect if fasciitis could be suspected or not but none of them was previously investigated to see how much are related with the diagnosis of nf and with the lrinec score . 
one of the most interesting parameter , which is currently quite debated in literature , is the non - enhancement of the muscular fascia after contrast medium administration ; this lack of enhancement of the fascia is generally considered predictive of necrosis permitting discrimination between nf and non - nif [ 3 , 57 ]  . features and nf and among the other musculoskeletal infections to better understand what is peculiar for each infection . the increase of the predisposing factors of nf ( diabetes , chronic infections , secondary immunodeficiency ) and the potential fatal complication of the disease make nf a reality that even if is rare must be warned by radiologists to permit to clinicians to adopt early medical interventions and to avoid fatal complications of this condition . 
different imaging techniques could identify this disease and magnetic resonance imaging ( mri ) is generally recognized as the technique that better detects nf , its extensions and complications [ 7 , 8 ]  . 
we have to say that mri , which is superior to ct in the evaluation of soft tissue infections , could not be performed by all patients especially in those who have metal implants and pacemakers , is not available in all the emergency departments , it requires more costs for the national health systems and needs more time to be performed compared to a multidetector contrast enhanced computed tomography ( mdcect ) scan . 
so we decide to evaluate the diagnostic efficacy of mdcect to address to diagnosis of necrotizing fasciitis and to differential diagnosis of the musculoskeletal infections in an a daily emergency department activity where mdcect is easily accessible and routinely performed thus giving to the readers a contribution with our emergency experience where mri is not performed in emergency condition . 
we also tried to relate ct findings with the lrinec score , which is currently used in the routine clinical practice , in order to add value to the radiological mdcect findings to the clinical context . 
we do not have to forget that a certain diagnosis of nf always requires a clear and direct evidence of the presence of necrosis among the muscular fascia : surgical exploration or biopsies of affected tissues and clinical examination are needed to confirm the presence of necrosis and to formulate the final diagnosis of nf . thus , the role of imaging , especially of mdcect , could be considered limited to suggest a suspicion of the presence of this condition to adopt early clinical and surgical strategies needed first to confirm this condition and then to treat materials and methods patients selection this retrospective study was conducted in accordance with ethical guidelines for human research and was compliant with the health insurance portability and accountability ( hipaa )  . the aim of our work is not to propose a radiological score for nf but to investigate relations between cect the study received institutional review board approval , and written informed consent was obtained from all the 1 3 108 radiol med ( 2016 ) 121 : 106121 patients before performing the contrast enhancement computed tomography scan as established in our daily practice . through the electronic database of medical records of our hospital , we searched for patients admitted from october 2012 to september 2014 to our emergency department with a suspicion of musculoskeletal infection . 
even some authors consider gas gangrene as a type iii of nf , while the type i and ii depend on the microbiological aetiology of the disease , so we decide to consider gas gangrene as a distinct entity from nf to better evaluate the differences between the two conditions [ 1 , 2 ]  . a total of 76 patients ( pts ) matching these records were found . 
subsequently , we figured out , through the picture archiving and communication system ( ris - pacs ) of our hospital , which of these 76 pts had performed a mdcect of the affected region , before and after contrast medium administration ( venous phase ) ; the number of the patients matching both criteria was 40 . 
then , through the data and service integration laboratory ( dasi - lab ) software of our hospital , we ruled out if patients had performed blood tests ( c - reactive protein , white blood cell count , haemoglobin , sodium level , creatinine and glucose ) needed to calculate the lrinec score ; patients were still 40 . 
to enrol the study patients with a diagnosis of nf or non - nif , biopsies , surgery or surgical exploration of the ill tissues must have been performed to have histologically proven diagnosis of nf or non - nif . these parameters were checked through the anatomy pathology computerized registry of our hospital and collecting all the registries of surgeries of these patients . 
the total number of the patients who matched all the criteria was in total 36 , 14 females and 22 males with a median age of 66 years . a review of the literature was performed to establish characteristic ct findings , which could be present in condition of nf and in the other musculoskeletal infections [ 3 , 57 , 9 ]  . the ct parameters analysed were ( table 1 ) : involvement and thickening of the muscular fascia , 2 . 
the acquisition protocol used was the standard emergency protocol used for body acquisition performed in our institution : 120 kv , mas 120180 , slice collimation 2.5 mm with a raw data slice collimation of 1.25 mm , pitch 1 . 
dynamic study after contrast medium consists at least of a portal phase ( 80 s of late )  . image analysis three radiologists , one with 12 years of experience and 2 with at least 4 years of experience in musculoskeletal radiology , in according reading consensus evaluated the ct images without knowing the final diagnoses of the patients ; images were interpreted as presence or absence of the above parameters ( 0 absence1 presence )  . the established parameters were evaluated for all the patients , and the radiologists made a suspicion of diagnosis among these pathologies : necrotizing fasciitis , nonnecrotizing fasciitis , myositis , abscess , cellulitis , and gas gangrene . 
to evaluate the lack of enhancement of the muscular fascia , a qualitative method was used : a no demonstrable enhancement of the fascia , in the late venous phase , must be present in order to suspect a nf , as state elsewhere [ 3 , 8 ] ; a comparative assessment of the enhancement of the surrounding not affected tissues was also taken into account to better evaluate the lack of the fascial enhancement . 
the radiologists were not involved in the patients selection process and did not know any clinical data or medical records . lrinec score and surgical evaluation lrinec score was calculated by the clinicians for all the patients considering a score < or equal to 5 as low - risk standard reference , 67 points as intermediate risk and a score > or equal to 8 as a high risk ( table 2 )  . as said before , fasciitis is a disease of the fascia so the criterion for the radiologists to assess a suspicion of nf was the fascial involvement detected at cect scan ( parameter 1 )  . the final diagnoses of patients with nf or non - nf were established by surgical explorations or direct surgery , i.e. 
to find any possible associations with the studied ct parameters and the variable presence of fasciitis and between lrinec score and the ct analysed parameters , the spearman coefficient of rank correlation ( ) and the kendall rank correlation 1 3 110 radiol med ( 2016 ) 121 : 106121 coefficient ( ) were used . 
results were calculated with medcalc software ( version 14.10.2last modified : october 16 , 2014 19932014 medcalc software bvba )  . the medical therapy used in patients with nf consisted of a combination of different antibiotics based on the result of microbiological cultures , administration of fluids and electrolytes when needed , painkillers and daily medication of wounds . 
hyperbaric therapy was not used in any patients affected by nf . results confirmed diagnoses among the 36 selected pts , the confirmed diagnoses were as follows : patients with necrotizing fasciitis ( 10 pts ) , patients with non - necrotizing fasciitis ( 2 pts ) , patients with cellulitis ( 10 pts ) , patients with soft tissue abscess ( 7 pts ) , patients with myositis ( 5 pts ) , patients with gas gangrene ( 2 pts )  . 
the diagnoses of nf or non - nif were confirmed by surgery : ten patients due to clinical , laboratory and imaging findings underwent immediate surgical debridement which confirmed the presence of necrosis ; 2 pts underwent surgical exploration with biopsies of the affected region being in those cases not necessary an immediate surgical debridement . all the other diagnoses were confirmed clinically and instrumentally and , as said before , did not need surgery . radiological suspicion of diagnosis for the radiologists , ct findings were suggestive for nf in 11 pts and for non - nf in 1 patient . 
these diagnoses were confirmed by clinical records and by surgical consult and did not require any biopsy or surgical exploration . 1 3 radiol med ( 2016 ) 121 : 106121 parameter 2fluid collections along the deep fascial sheaths were present in 2 pts . parameter 3extension of oedema into the intramuscular septa and the muscles was present in 3 pts . parameter 7subcutaneous gas was present in 7 pts . parameter 1 , parameter 2 , parameter 4 , parameter 5 and parameter 6 were detected in none patients . lrinec score of these patients : 3 pts have 6 / 8 ; the rest of the patients had 5 / 8 . myositis ( 5 patients ) in these patients , the ct parameters detected were : parameter 3extension of oedema into the intramuscular septa and the muscles was present in 3 pts . parameter 1 , parameter 2 , parameter 4 , parameter 5 , parameter 6 and parameter 7 were detected in none patients . lrinec score of these patients : all < 5 . abscess ( 7 patients ) in these patients , the ct parameters detected were : parameter 2fluid collections along the deep fascial sheaths were present in 3 pts parameter 5low attenuation areas in the deeper fascial planes suggestive for colliquative necrosis were present in 5 pts parameter 7subcutaneous gas in 2 pts parameter 1 , parameter 3 , parameter 4 and parameter 6 were detected in none patients . lrinec score of these patients : 1 patient had a score of 5 / 8 , 4 patients had a score of 6 / 8 and 2 patients had a score of 7 / 8 . statistical results ( table 6 and table 7 ) spearmans and kendalls test ( table 6 ) fig . 
cect axial plane slice taken at the level of the olecranon ( b ) and below the wrists articulation ( c ) , venous phase , shows involvement of the fascia ( single arrow ) , at the level of the anconeus and supinator muscle , which appeared unenhanced compared to surrounding tissue ( star ) , imbibition of fat tissue ( two arrows ) and fluid collections present ( three arrows )  . 
lrinec of this patient was 8 gas gangrene ( 2 patients ) in these patients , the ct parameters detected were : parameter 1 : involvement and thickening of the muscular fascia was present in 1 patient . parameter 3 : extension of oedema into the intramuscular septa and the muscles was present in 2 pts . parameter 7 : subcutaneous gas 2 pts . parameter 2 , parameter 4 , parameter 5 and parameter 6 were detected in none patients . lrinec score of these patients : both patients had 7 / 8 . cellulitis ( 10 patients ) in these patients , the ct parameters detected were : the cohort was made of 36 pts of those 12 were diagnosed with necrotizing fasciitis ( 10 with nf and 2 with non - nf ) ; the 12 pts represented the variable to compare with the five ct parameters studied in all the 36 pts . to compare the variable presence of fasciitis in the cohort of the 36 pts with the five ct parameters , the spearmans coefficient of rank correlation ( ) and the kendalls rank correlation coefficient ( ) were calculated . these tests showed that the only parameters which could be associated with the diagnosis of necrotizing fasciitis was the parameter 1 ( involvement and thickening of the muscular fascia ) with a and a of 0.888 and significance level of p < 0.001 and with a less value of association , and the parameter 5 ( a non - enhancement of the muscular fascia ) with a and a of 0.672 and significance level of p < 0.001. 1 3 112 radiol med ( 2016 ) 121 : 106121 fig . 
2 contrast enhanced ct scan of the sacral region with multiplanar reconstruction in coronal plane ( b ) and volume rendering reconstructions for soft tissue and skin ( a )  . 
3 lower limbs contrast enhanced ct , venous phase , of a 63 - year - old diabetic patients in axial ( a ) and coronal plane ( b )  . 
a the right image represents the not - ill right leg while the left image shows the affected leg where it could be appreciated at the level of the gastrocnemius - medial side , the lack of the enhancement of the fascia ( single arrows ) compared to surrounding tissue ( star ) , and the presence of small fluid collections ( two arrows )  . 
b picture shows presence of gas bubbles ( single arrows ) among fascial planes between gastrocnemius and soleus ( posterior ) and among tibialis anterior muscle ( anterior )  . 
thus , we could consider the lack of enhancement of the fascia as an helpful tool in the diagnosis of nf which could suggest the suspicion to the surgeon of the presence of necrotic tissue but could not certainly state if necrosis is present or not also considering the state of the art and other paper where more contrast - sensitive techniques such as contrast enhanced mri still have 1 3 114 radiol med ( 2016 ) 121 : 106121 fig . 
4 contrast enhanced ct scan of the lower limbs with multiplanar reconstruction in coronal plane ( b ) and volume rendering reconstructions for soft tissue and skin ( a )  . 
the right leg shows imbibition of the soft tissues with septations of the subcutaneous fat ( two arrows ) , all muscles of the left lower limb appeared enlarged ( three arrows ) compared to the contralateral one ( star ) , and fascia did not appear involved ( one arrow )  . 
5 a photograph of the pelvic region of a 60 - year - old lady shows the presence of a big eschar in the perineal region ; patient reported in her history a recent infection of the bartolinis glands . 
b cect , axial plane , shows the presence of a huge scout of gas in the perineal region ( single arrow ) , muscular fascia of the surrounding muscles appeared to be not involved ( two arrows ) , no fluid collections were observed , and some imbibition of the subcutaneous fat was observed ( three arrows )  . 
lrinec of this patient was 7 false - positive results in the evaluation of the necrosis of the fascia [ 8 ]  . regarding this patient with lack of fascial enhancement but with no necrosis confirmed at the surgical exploration we have to say he was diabetic ; so we could speculate that the lack of enhancement could be the result of the presence of the infection in addition to the altered microcirculation of the patient due to his uncontrolled diabetes which worsened the microcirculation ; but this is just an hypothesis to try to explain our results . necrosis of the fascia is a dynamic process that it establishes with time , and could not be certainly detected with 1 3 radiol med ( 2016 ) 121 : 106121 the 83 % of the patients with nf but was present also in patients with other musculoskeletal infections and did not associate in a statistical significant way with the diagnosis of nf ; thus this parameter according to our evidences could not be associated with nf being present in other infections such as gas gangrene , cellulitis and abscess . in none of the reviewed patients vascular thrombosis was present . also the third parameter , extension of oedema into the intramuscular septa and muscles , is not associated with nf being present in patients not diagnosed with nf . other findings present in our study suggest that enormous presence of gas in anatomical structures , such as perineal and genital areas , is suggestive for gas gangrene where fascia could be involved and some imbibition of the muscular septa could be present ; but gas gangrene is easily distinguishable with ct from nf as said before . ct findings in patients with others musculoskeletal infections confirm what is yet known in the literature and make stronger the concept that ct is a reliable tool for the evaluation and differential diagnoses of musculoskeletal infections : in cellulitis fascia is never involved , some oedema and imbibition of the surrounding tissue and some air bubbles could be present . 
deeper muscular structures could be involved in deep cellulitis but the fascia is never involved [ 7 ]  . in myositis fascia is not involved , and an enlargement of a group muscle compared to the others characterizes myositis , imbibition of the muscular tissue and also fluid collections could be present [ 7 ]  . 
6 contrast enhanced ct scan , axial plane , of a 55 - year - old man , drug addicted , admitted to our emergency department due to right low back pa ct findings show the presence of fluid capsulated areas tending to confluence ( single arrow ) with suppurative and lowdensity areas in the context ( two arrows ) with a thick wall and some calcifications within ( three arrows ) at the level of the right psoas ; ct findings were suggestive of abscess of the right psoas . 
lrinec of this patient was 7 both cect and mri as said before , maybe especially in its first stages when the necrosis is still not totally extended and did not total compromise the vitality and the circulation of the fascial tissue ; this is why in the doubt cases as we will explain later monitoring overtime and instrumental follow - up could be useful [ 8 , 9 , 11 , 12 ]  . the presence of subcutaneous gas which is considered by some authors [ 13 ] a specific sign of nf was present in fig . 
in this study , an intermediate to high risk of nf had , respectively , a positive and negative predictive value of 92 and 96 % [ 4 , 14 ]  . in our study , the 42 % of patients with nf had a score of 6 and the 33 % had a score of 7 which are considered intermediate risk scores , and just the 17 % had a score of 8 which is considered predictive for a high risk . 
score of eight points resulted just in patients with nf ( 2 pts ) , scores 7 and 6 were present also in patients with other musculoskeletal infection thus making the intermediate risk scores of the scale , in our study , not specific for nf . the literature shows contrast data regarding the role of lrinec score for the diagnosis of nf ; wilson et al . 
published a retrospective evaluation of laboratory - based diagnostic tools for cervical nf where they state that neither the lrinec nor the blood cell count was useful in their experience for distinguishing cervical necrotizing fasciitis from non - necrotizing neck infection [ 15 , 16 ]  . another study written by corbin concludes that the lrinec score may be a useful tool for the detection of soft tissue infections and patients with a lrinec score > 6 on admission should be carefully evaluated , while su et al . 
say that lrinec score is a robust score capable of detecting even early cases of nf and that all patients with a score of > or 6 should be carefully evaluated for nf [ 4 ]  . in our study all the patients with nf had a lrinec 6 points and just one patient with non - nf had score > or a score of 5 , so we agree with what was said by wong et al . 
15 years ago performed a study where they test the efficacy of blood tests , especially serum level of 1 3 118 radiol med ( 2016 ) 121 : 106121 sodium ( na ) and white blood cell ( wbc ) count , to find useful parameters that may help to distinguish nf from non - nf infections . 
they found out that the model based on this values of blood component had a sensitivity of 90 % and a specificity of 76 % in predicting nf , when the value 109 / l and of wbc on admission was greater than 15.4 serum sodium ( na ) was less than 135 mmol / l [ 18 ]  . the aim is not to diagnose nf when is too late or when the systemic complications of the disease appear and let increase the lrinec score to 78 points , due to the alteration of serum levels of sodium , haemoglobin and creatinine which increase when the disease is systemic . the real goal is to diagnose nf in the early stage to prevent fatal complications . 
cect permits an early detection of the disease due to its capability to identify the involvement of the fascia , which is a specific sign for nf , and not present in other musculoskeletal infections . according to our data , we could say that lrinec score could be higher than 5 also in other musculoskeletal infections and in the cohort of patients with nf was > or equal to 6 , thus a discriminating tool is necessary to assess what type of infection is present when the clinical inspection and symptoms are not clear [ 19 ]  . the need to have a discriminating tool , as said before , is fundamental being nf a potential fatal disease which needs surgical debridement of the necrotic tissue while the other musculoskeletal infections do not need . 
another distinction must be done between nf and non - nif due to the different approaches these conditions need as previously described in the text . in the management of nf must be considered also the presence of high index of suspicion ( drug abuse , presence of debilitating comorbidities such as diabetes , obesity , hiv or other acquired immunodeficiency ) , the clinical presentation of the disease ( swelling , erythema , pain , oedema outside compromised skin , ecchymosis , blisters , crepitus ) and the systemic signs ( fever , tachycardia , hypotension , shock ) [ 17 , 1921 ]  . general approach to the diagnosis of necrotizing fasciitis with our experience and the evidences given in this paper , we could suggest that if there is a clinical suspicion of nf and the lrinec score is equal or superior to 6 , a cect of the affected area could be perform to assess if the fascia is involved or not ( nf vs other musculoskeletal infections )  . 
 as stated before , the aim of our work is not to propose a radiological score for nf but to assess which cect parameters could be seen in a case of nf and in other common musculoskeletal infections and to analyse which of these parameters could be considered suggestive for the presence of nf . 
according to our result , both spearmans and fishers test , and to our experience , an involvement of the fascia at the cect study is specific for nf and the fascial behaviour after contrast enhancement administration could help in the evaluation of the presence of necrosis ; however , as explained before , the evaluation of this parameter has its limits , especially with cect , and the final diagnosis of necrosis is always clinical and surgical . 
cect parameters , analyzed in our study , are quite reliable and easily assessable by radiologists in their daily practice in the evaluation of musculoskeletal infections , even by the ones not long experienced in musculoskeletal infections . 
a particular attention must be taken by radiologists in the evaluation of the fascial involvement and for this aim muscles anatomy must be kept in mind . the aim , in our practice , is to evaluate the involvement of the fascia and its contrastographic behaviour to suspect a possible case of nf , then the rest of the cect parameters could be analysed to better depict disease and its extension . in a case of suspected musculoskeletal infection admitted to emergency department , clinicians with the evaluation of laboratory tests , clinical examination and anamnesis , make the first suspicion of the presence of nf . 
after these evaluations and surgical consult , cect could help in the discernment between nf and other musculoskeletal infections evaluating the involvement of the muscular fascia and its contrastographic behaviour which could be considered suggestive for nf . 
the analysis of the other cect parameters helps to depict other musculoskeletal infectious conditions . thus the role of cect is to suggest a possible case of nf or of another musculoskeletal infections , being necessary for the final diagnosis of nf the demonstration of the presence of necrosis among the fascia which could be clinical in the worst cases where necrosis reached the skin and the soft tissue or surgical and bioptical in those cases where necrosis is just limited to inner structures and muscles . 
in this commitment , we think that our experience , shown in this paper , could help to suggest what has to be analysed by colleagues on a cect scan in a case of musculoskeletal infection , and discriminating the findings suggestive for nf and better depicting the findings present in other musculoskeletal infections . in the following lines we will discuss the different behaviors of the muscular fascia in order to let better understand to the readers the different realities they could face and the different available strategies for the management of nf . if the muscular fascia appeared involved at cect examination , a diagnosis of nf could be established and surgical evaluation is mandatory . 
the contrast administration helps to better evaluate the fascia and it could discriminate if necrosis is present or not ( nf vs non - nf ) but not 1 3 radiol med ( 2016 ) 121 : 106121 always . 
to assess if necrosis is present or not , and so if the surgery is needed , clinical conditions and laboratory tests help in the decision if wait or to perform biopsies of the tissue ; at this time , the contrastographic behaviour of the fascia plays a strategic role . 
if the fascia enhances , no other signs of infection are present and clinical conditions are stable ; surgical consult , medical therapy and a follow - up with enhanced mri to evaluate the evolution of the disease , should be performed . if the fascia enhances but other systemic signs of infection are present and clinical conditions are not stable , surgical consult , medical therapy and a possible surgical exploration of the tissue are mandatory considering that the clinical conditions of the patient play always a strategic role . if the fascia not enhances ( necrotic ) , no systemic signs of infection are present and clinical conditions of the patient are stable ; surgical exploration is mandatory before preforming surgical debridement considering that in one patient the non - enhancing fascia revealed to be not necrotic ; if the fascia not enhances and other systemic signs of infections are present and clinical conditions are not stable , a surgical debridement must be performed [ 22 , 23 ]  . we have to say that for soft tissue infections such as nf , mri imaging is a more useful tool in the evaluation of the precise extent of the infection and its relation with the surrounding organs , to distinguish mild fascial or muscle involvement , and to determine , with a higher sensibility compared to the ct scan , if necrosis and oedema is present or not . 
on mri scan , patients with nf usually present : thick ( > 3 mm ) areas with abnormal high - signal intensity on fat - suppressed t2 - weighted images ( t2 - wi ) in the deep fascia , with a less - frequency combined areas in superficial and deep fascia of low - signal intensity on fat saturation ( fat - sat ) t2 - wi . 
a focal or diffuse non - enhancing portion in the area of the high abnormal signal intensity , in the deep fascia , in t1 - wi fat - sat post - contrast images , extensive involvement of the deep fascia and involvement of three or more compartments in one extremity could be also present [ 8 , 1013 , 2428 ]  . 
in general , fat - suppressed t2 - wi has been found to display inflammatory changes better than fatsuppressed gadolinium - enhanced t1 - wi [ 8 ]  . mri is dramatically inferior compared to ct in the evaluation of the presence of subcutaneous gas and calcifications ; on mri , calcifications result in a signal loss in t2 - wi and t1 - wi but they are not easily and readily demonstrable as on ct [ 7 , 8 , 24 ]  . 
mri as said before is more contrast sensitive compared to ct and has an higher sensibility for the soft tissue structures , so it permits a better evaluation of the precise extent of the disease and it offers an important diagnostic adjunct to the management of nif and the potential to defer or limit extensive exposure of the deep fascia [ 8 , 13 , 24 , 25 ]  . 
also in the evaluation of the fascial enhancement , mri is superior to ct considering its more contrast - sensitive nature even if in a study where mri was performed to assess the nif findings a lack of enhancement was observed also in non - nif patients or not all the nif patients did not show a lack of enhancement [ 8 ]  . 
so the lack of enhancement of the fascia , on both cect and mri , could not be considered as a certain predictive factor of necrosis but as a suggestive predictive factor of necrosis according to the other radiological and clinical findings considering that mri could better evaluate this finding compared with cect . 
the possibility of using mri with short time inversion recovery sequences ( stir ) permits also to better evaluate the presence of oedema shown as an area with increased signal intensity compared to the normal tissues [ 7 ]  . thus mri is superior to all other imaging modalities for the detection of soft tissue infections because of its remarkable capacity to better assess the changes in the soft tissues structures and could be considered , according to the literature , as the gold standard exam in a case of a suspected musculoskeletal infection . we have to say that our retrospective study was designed and performed in a simple and busy emergency context where mri is not performed as an emergency technique and where the clinicians have the need to know in a short time if a fasciitis is suspected or not to plan the right treatment . 
we decided to investigate the role of cect in nf considering that not all hospitals are equipped with mr scanners and not all patients due to the presence of metal implants or claustrophobia could perform mri . 
the aim was to prove which ct parameter could lead the radiologist to suggest to the clinician the presence of nf considering that lrinec score could be high also in other soft tissue infections and not specific for nf as confirmed by our result . 
we tried to give a stronger value to ct technique which could be easily performed in all the emergency departments not forgetting that mri is the gold standard examination for nf evaluation exam and must be performed in those centre where mri is used also in emergency condition . the justification of an exposure to radiation dose find a reason in the ability of ct to identify if the fascia is involved or not and so to discriminate nf from other musculoskeletal infections which do not have such fatal complications as nf ; ct scan is also valuable to evaluate the systemic complications of the disease ( gas , fluid collection , pleural effusion , ascites and fluids in the abdomen , vascular thrombosis , signs of sepsis ) [ 7 ]  . regarding the role of nuclear medicine in the management of nf , we could say that 99 m - technetium methylenediphosphonate ( 99 m tc - mdp ) and 67 - gallium ( ga ) studies have a fundamental role in those cases of nf where a complication of osteomyelitis is suspected . 
the retrospective nature of the study and the lack of fludeoxyglucose ( fdg ) positron emission tomography ( pet ) - ct , also with the use of radiolabelled tracers as marked leucocytes , could provide functional and morphological information thanks to the fusion with the ct images and permits to identify osteomyelitis and bone complications of soft tissue infections especially in spinal infections ( discitis and / or osteomyelitis ) , diabetic foot infections and periprosthetic infections differentiating between soft tissue and bone infections and giving information regarding the bone structure thanks to the fusion with ct images [ 29 , 30 ]  . our study as several limitations , the main limits of our study are represented by : 1 . 
the evaluation of the hounsfield units ( hu ) densities before and after contrast medium administration using different non - overlapping regions of interest ( rois ) among the fascial layers . 
due to the small sizes of these structures this process will be difficult , considering also the different extension of this disease could have , not permitting to obtain same squared areas of rois to be calculated . 
by the way , a no demonstrable enhancement of the fascia after contrast medium administration was used as a criterion of fascial evaluation also in other papers where ct was used as a detection technique of necrosis [ 3 ] and even with mri [ 8 ]  . we have to say that in our study , three reviewers carefully evaluated this parameter and a comparative assessment of the enhancement with the surrounding tissue was also taken into account . 
the final reviewed images were 2.5 mm thickened , and the raw data acquired with 1.5 mm thickness were not stored to pacs in according to our department policy which does not allows to store raw data to pacs to not overload the system and thus images at 1.5 mm thickness could not be used in the review process . 
acquisitions for reconstructions at 0.625 mm were not performed because our standard protocol for body ct in an emergency condition is settled to decrease the radiation exposure of the patient . 
mdcect is a fundamental tool in discriminating nf from the other musculoskeletal infections and this study proofed the ct parameters which significantly relate to nf ; it gives an added value to the clinical and radiological practice of physicians from different specialities . 
radiologist could express any suggestion of the presence of necrosis of the fascia evaluating the enhancement of the fascia but the role of the radiologist is to confirm or not the involvement of the fascia and the complications of the disease , the diagnosis of necrosis of the fascia remains surgical . 
if the radiologist confirm the diagnosis of fasciitis , the surgical consultation is mandatory ; is the surgeon , according with the clinical condition of the patients and with the other ct findings , who decides to 1 3 radiol med ( 2016 ) 121 : 106121 perform immediate surgical debridement or surgical exploration of the tissue or other therapeutical options . 
clinical , laboratory and radiological parameters should be evaluated together to formulate a correct diagnosis considering that ct could discriminate nf from other musculoskeletal infections in an emergency condition . compliance with ethical standards conflict of interests all authors have no conflicts of interest . ethical standards institutional review board approval was obtained for this study , no funds were asked for this study and no experimental tests on animals were performed . 
subjects were also classified as smokers , former smokers and nonsmokers . results among the 36 workers examined , we identified four ct patterns which resulted to be dependent on exposure duration and intensity , fvc , fev1 and fef2575 , but not on cigarette smoking . 
in no case it was proven an evolution of ct findings during follow - up for 10 years . conclusions liparitosis , caused by pumice inhalation , can be considered a representative example of * tommaso dangelo tommasodang@gmail.com 1 department of environment , security , territory , food and health sciences - occupational medicine section , policlinico g . 
martino , university of messina , via consolare valeria 1 , 98100 messina , italy pneumoconiosis derived by amorphous silica compounds , which are extremely widespread for industrial manufacturing as well as for applicative uses , such as nano - materials . 
 moreover , being pumice free of quartz contamination , it can represent a disease model for exposure to pure nonfibrous silicates . keywords amorphous silica computed tomography lung pleura pumice pneumoconiosis introduction pumice is an extrusive volcanic rock , produced when lava with a high content of water and gases is ejected from a volcano during explosive eruptions . it is a complex silicate containing about 70 % silica ( sio2 ) in which other oxides are dissolved ( approximately 12 % aluminium , 0.1 % titanium , 2 % iron , 0.1 % manganese , 3.6 % sodium and 4.5 % potassium oxides ) [ 1 ]  . 
the plentiful presence of ions does not allow the formation of a crystalline reticulum , therefore pumice has an amorphous but typically not fibrous structure . a pneumoconiosis related to the inhalation of pumice powder extracted in the island of lipari ( aeolian archipelago , sicily , italy ) was named liparitosis [ 2 ]  . 
despite its low incidence due to localized exposure , liparitosis deserves a great interest as it can be considered representative of pneumoconioses derived by inhalation of amorphous silica compounds , including diatomite , fullers earth and above all , artificial amorphous silica , the industrial manufacturing of which is extremely widespread . 
mechanical sieving of excavated material ( b ) after exertion ; mild chest discomfort , dyspnoea and fatigue characterize the more severe forms involving lung parenchyma with large perihilar masses . the description of pneumoconioses caused by environmental or occupational exposure to non - fibrous , amorphous silica like pumice is undoubtedly less defined than pulmonary silicosis [ 3 , 4 ]  . despite of the widespread use of amorphous silica compounds , there are only few reports in the literature about the damage due to environmental or occupational exposure [ 5 , 6 ]  . 
in particular , in the last decade only one study described three different radiological thoracic patterns involving pleural , parenchymal and mediastinal compartments due to inhalation of pumice powder in a wider study population of exposed workers [ 7 ]  . 
however , the main limitation of this study was the short duration of follow - up . the purpose of this study is to describe computed tomography ( ct ) features of the damage caused by inhalation of pumice powder in a population of workers , correlating these findings with job description and exposure modalities . 
a follow - up period was evaluated to assess the non - evolutive fibrotic nature of the lesions . methods job description extraction and commerce of pumice powder in lipari have marked more than two centuries of the social history of this island . 
as a consequence , natural history of pumice pneumoconiosis was substantially modified and the incidence of death due to pneumoconiosis collapsed between 1970 and 1985 . study population from june 1999 to november 2014 , 36 subjects employed in the quarries were evaluated for annual follow - up in a preventive medical surveillance progra they were 16.45 years , whose only male subjects ; mean age 56.92 occupational exposure to pumice resulted from work history with special regard to the duration and modalities of work . 
occupational exposure an average of 25.03 to pumice was evaluated by recording job title and description , duration of exposure ( number of years working in the quarry ) and latency of symptoms since initial exposure . 
axial ct scan visualized with lung setting shows the presence of several pleural plaques ( arrows ) localized bilaterally , without any parenchymal lesion radiol med ( 2016 ) 121 : 1926 followup protocol the medical surveillance program firstly included clinical evaluation followed by spirometric examination , standard radiography and ct of the chest without administration of contrast mediu the follow - up ct was then performed annually for the first 5 years , and then the subjects were monitored after 5 years . 
ilo classification has great medico - legal importance but it is applicable only to conventional or digital radiographs ; therefore ct has to be performed in pneumoconiosis patients to gain more information about disease extension and degree . clinical examination and spirometry were also performed annually . 
results were expressed as percentages of predicted normal values normalized for age , sex , height and weight and used for correlation analysis to evaluate their relationship with the other variables . statistical analysis analysis of variance ( anova ) was used to determine the significance of differences between groups in relation to lung function , smoking habits and years of exposure to pumice powder , using ct findings as a variable factor . 
we also performed spearman test in order to assess the correlation between ct findings and the measurements of pulmonary functions , number of cigarettes per day and years of exposure to pumice dust . 
transverse ct scan demonstrates the presence of bilateral perihilar masses ( arrows ) enclosing fine reticular calcifications , more evident on the right side results radiological findings pumice powder samples collected in the quarry of lipari were analysed by means of x - ray diffraction ( xrd with a siemens r2000 diffractometer equipped with a graphite monochromator )  . 
naf peaks were after omitted in the graphics . scanning electron microscopy ( sem ) was performed on a leo s420 ( leica - cambridge instruments , cambridge , uk ) coupled with an energy dispersive system ( edx ) ( oxford link isis series ; oxford instruments , witney , uk ) 300 with sili detector ( oxford instruments )  . among the 36 workers examined , we identified four ct patterns : a . 
no damage ( occupational activities carried out in safe conditions ) ; it was found in 22 / 36 cases , representing 61.11 % , with ilo classification in the degree 0 / 01 ; b . 
axial ct scan visualized with mediastinal ( a ) and lung ( b ) window settings show bilateral calcified perihilar masses ( asterisks ) associated to pleural plaques ( arrows , a ) and thickening of subpleural fat ( white dots , a )  . 
interlobular septa thickening and centrilobular nodules ( arrowheads , b ) are also visible characterization of pumice powder x - ray diffraction data for pumice powder in the examined specimens chemically identified them as sio2 , revealing a diffraction pattern pointing mainly to amorphous silica . 
therefore , neither quartz nor asbestos should be considered responsible for lung damage . environmental assessment as local laws did not require it yet , no environmental assessment of dust pollution was performed in the pre - technological period . 
these data are related to indoor mean levels inside pumice selection and packaging plant ; as no personal or task - specific sampling was performed , they do not reflect the contribution of the single processing stages to overall environmental pollution . 
moreover , they do not leave us any idea of outdoor dust levels , which would be important because parts of the processes ( including excavation in the quarry ) are performed outside . discussion the current knowledge about the health effects of noncrystalline forms of silica is still ambiguous . 
however pumice , as well as artificially manufactured silicates , is free of quartz contamination ; for this reason , it may be considered a disease model for inhalatory exposure to pure non - fibrous silicates . 
nano - materials , fillers in the rubber industry , anti - caking agents , liquid carriers in agrochemicals ; other uses are found in toothpaste additives , paints , silicon rubber , insulation material , liquid systems in coatings , adhesives , printing inks and cosmetics [ 10 ]  . 
epidemiological studies do not support the hypothesis that amorphous silicates have any relevant potential to induce progressive fibrosis in the workers with high occupational exposure to these substances , although one study disclosed four cases with fibrosis among subjects exposed to apparently noncontaminated amorphous silica [ 11 ]  . 
 the current study describes the characteristics of liparitosis , another pneumoconiosis due to pure amorphous , nonfibrous silica . the different presentation of this disease compared to silicosis may be explained by the mild cytotoxicity exerted by pumice on alveolar and interstitial macrophages and on mononuclear phagocytes ; pumice powder accumulates into the cells without causing their necrosis , which is responsible of the release of interleukins and other mediators provoking fibrosclerotic reaction . 
consequently , pumice powder , both free and contained in macrophages , follows an efficient lymphatic drainage towards pleural membranes and mediastinal lymphnodes determining a chronic fibrosis only after overcoming a threshold limit of dust deposit . 
 this mechanism may explain the relative clinical mildness and long evolution of liparitosis as well as its peculiar ct findings : pleural plaques and perihilar masses [ 7 , 14 ]  . 
only in two older patients ( group d ) we found parenchymal nodules in combination with perihilar masses and pleural plaques ; this pattern , never described before , was related to the exposure to massive concentrations of silica at high temperature that overcomes the possibility of lymphatic drainage , resulting in parenchymal deposit . today , probably thanks to the technological improvement of extraction and processing procedures , the massive form is still visible only in older retired workers . 
on the basis of the substantial improvement of the processing plant in 1985 , the year 1985 can be considered a borderline between a pre - technological and a technological period . 
the main interventions in the field of the workmanship of pumice were made in the 70 s , with the introduction of electrofilters in the working cycle and the change of the pumice desiccation system , from plate ovens to closed - cycle rotating ovens . 
 that duty had caused , between 1970s and 1980s , a high incidence of extremely serious forms of pneumoconiosis , which dramatically decreased with the reduction of workers exposed to the above risk . 
6 spearman correlation test between years of exposure to pumice and ct findings ( a ) and between duration of exposure and pulmonary function parameters : fvc % ( b ) , fev1 % ( c ) and fef2575 % ( d ) radiol med ( 2016 ) 121 : 1926 1 3 radiol med ( 2016 ) 121 : 1926 particles showed an almost fourfold higher mean concentration in 1981 compared to 1997 , i.e. 
consequently , a longer duration of exposure corresponds to higher intensity also . all workers belonging to the technological period were classified in group a , presenting no sign of pleural and pulmonary damage at ct . 
all subjects included in groups b , c and d had worked in the pre - technological period ; however , workers from groups c and d had been exposed to heated pumice respectively in high and massive amounts and showed bilateral perihilar masses . 
the association of masses , centrilobular nodules with interstitial thickening and pleural plaques in group d can be explained by the higher levels of inhaled silica compared to group c . it is unlikely that temperatures reached in the desiccation ovens could be high enough to convert the structure of pumice from amorphous into crystalline ; more probably , loss of humidity reduced the aerodynamic diameter of dust particles allowing them to penetrate more deeply into the airways . as regards the nature of nodules and masses , it can be observed that although in the radiological literature highdensity deposition within fibrotic mass is conventionally indicated as calcification , it has been demonstrated that silicotic masses contain both mineral dust and calcium phosphate [ 15 ]  . 
similarly , in liparitosis conglomerated masses described by the radiologist as calcifications may be due to the deposition of amorphous silica and probably , to some amount of calcium phosphate . two previous studies stated that exposure to amorphous silica cannot be completely responsible for the pulmonary functional damage observed , and postulate a synergism with cigarette smoking [ 16 , 17 ]  . 
our findings exclude the role of cigarette smoking , support the hypothesis that exposure to pumice correlates with pulmonary function and highlight the difference in exposure time and pulmonary function between the four groups . 
in group b , the minimal deviation of functional parameters from the range of normality , despite of a long exposure time , can be explained by the absence of parenchymal damage ; in fact , groups c and d presented significantly reduced lung volumes . an important weakness of our study was the absence of correlation between ilo classification and ct patterns . 
we could foresee that the introduction of low - dose iterative ct and more widespread use of ct in pneumoconioses will allow to obtain interesting data integrating ilo classification and ct patterns in the next future . another limitation is the small size of study population ; however , it should be considered that exposure to pumice was limited to a small geographical area in a small extraction plant . 
we could also hypothesize that chronic inhalation of this powder might represent a paradigm of lung disease due to occupational and environmental exposure to pure nonfibrous amorphous silicates , although further studies are necessary to confirm this suggestion . 
consequently , due to wide industrial use of amorphous silica compounds , the knowledge of clinical and ct features of liparitosis could be useful for radiologists , pneumologists and occupational physicians in order to improve their diagnostic skills . finally , we believe that delayed pleural damage could be a peculiarity of pneumoconiosis due to silicate inhalation . 
 for each subject , two apparent diffusion coefficients based on all b - factors less than 400 s / mm2 ( adc0400 ) and 800 s / mm2 ( adc0800 ) were calculated by fitting the signal intensity at different b - factors to a mono - exponential decay , respectively . 
in recent years , dwi has been applied increasingly to abdominal imaging in order to ( 1 ) detect and discriminate the different types of tumors [ 24 ] and ( 2 ) assess liver cirrhosis , renal injury , and pancreatitis [ 57 ]  . 
although nobody can accurately measure the true diffusion coefficient of a defined tissue in vivo , more and more studies are interested to the higher b - factors - based adc since it can minimize the perfusion influence on the apparent diffusion value ( adc ) measured in vivo . dwi has shown a great potential in abdominal imaging , especially for the kidneys with high blood flow and water transport functions under normal conditions [ 8 , 9 ]  . 
to date , dwi can differentiate subtypes of renal tumors and grade clear cell renal cell carcinoma [ 2 , 10 , 11 ] , can stage the severity of renal pathology or renal fibrosis [ 12 , 13 ] , and also can demonstrate the early functional state of renal allograft [ 14 ]  . 
however , what are the optimal b - factors to use to differentiate renal masses and assess renal dysfunction 1 3 radiol med ( 2016 ) 121 : 611 in vivo ? advanced technologies have enabled the clinical application of high - quality body dwi with higher and multiple b - factors [ 15 ]  . 
another study reported that both high b - factors ( 8001000 s / mm2 ) and low b - factors ( 400500 s / mm2 ) had their own strengths for the detection of renal cell clear cell carcinoma [ 19 ]  . from a practical point of view , the affected kidney , mainly in situations of chronic kidney disease , is characterized by the reduced blood flow and a decrease in renal water content [ 20 ] , implying a lower signal intensity would be obtained than for a healthy kidney on the diffusionweighted images at the same level of b - factor . 
they were admitted with symptoms of swelling , urine that is foamy , fatigue , poor appetite or trouble sleeping , and also fulfilled the inclusion criteria of persistent albuminuria [ 21 ] or microalbuminuria [ 22 ]  . 
to determine the trace of diffusion , the geometric mean of the signal in three orthogonal spatial directions was calculated . 285 mm2 , matrix 320 285 mm2 , matrix 192 coronal images were applied for anatomic identification , followed by transverse images covering the whole kidney . 
in routine workflow , conventional t1and t2 - weighted images were used to screen the space - occupying renal lesions . data analysis the parameter measurement was carried out by a radiologist , having more than 5 years of experience in interpreting abdominal images who was blinded to the clinical details of each subject . 
to minimize the possible artifacts derived from air in the digestive tract as much as possible , the transverse section of the dwi image covering the largest part of the right kidney was chosen for imaging analysis . 
a 53 - year - old male with chronic kidney disease , the regions of interest were delineated along the outline of right kidney on the transverse dwi images at different b - factors ( manual curves )  . 
the abilities of the two coefficients to differentiate sri from non - sri were compared using the receiver operating characteristic curve ( roc ) analysis , and the sensitivity and specificity were also acquired for each coefficient . 
all analyses were conducted in the statistical packages for social sciences ( version 12.0 for windows , chicago , il , usa )  . forty - four subjects were recruited into this study . 
 the area under receiver operating characteristic curve of adc0400 was not larger than that of adc0800 ( p > 0.05 ) it is well known that a simple mono - exponential model has measurable limitations in the post - procession of abdominal dwi data [ 16 , 24 ]  . 
for the dwi with low b - factors , microcirculatory blood within capillaries has no special orientation in abdominal organs , which was subscribed as pseudodiffusion that depends on the velocity of the blood flow and vascular architecture . 
in this study , the adc0400 was larger than the adc0800 in each group , which is consistent with previous studies [ 25 , 26 ] , indicating that adc0400 might contain more perfusion information than adc0800 . 1 3 10 radiol med ( 2016 ) 121 : 611 the signal intensity on a dwi depends on the microscopic mobility of molecular water , which is naturally restricted in tumor tissue . 
additionally , owing to the reduced t2 * time of chronic kidney disease [ 27 ] , the larger b - factor was applied at the expense of longer examination time at the same signal noise ratio . 
therefore , the clinical value of higher b - factor seems to be limited for assessing renal dysfunction . low b - factor dwi may especially be useful for evaluating the renal dysfunction that exhibits an inherently low signal at high b - factors . 
the advantages of low b - factor based adc are ( 1 ) dwi at low b - factors is sensitive to the reduced perfusion of renal dysfunction [ 20 ] ; ( 2 ) it preserves , at least in part , the tissue discrimination arising from the different t2 * relaxation times , since dwi is based on a t2 - weighted sequence ; ( 3 ) it reduces the total examination time using low b - factors , which also minimizes the artifacts derived from the respiratory movement and eddy current - induced distortion in turn [ 24 , 28 ] ; and ( 4 ) it improves the signal - to - noise ratio on diffusion - weighted images . 
therefore , low b - factor - based adc , a combination of perfusion and diffusion information , might be useful to detect early chronic kidney disease . consistent with a previous study [ 14 ] , moderate correlations were revealed between egfr and adc . 
first , the perfusion information for the renal tissue was not assessed directly or indirectly in this study , having been revealed using different perfusion technologies in previous studies [ 30 , 31 ]  . 
third , owing to the poor visual contrast between the renal cortex and medulla in sri group , it was too difficult to draw cortical or medullary rois for their quantitative measurements in this study . 
fourth , this study investigated the clinical value of dwi in differentiating sri from non - sri , but did not discriminate the renal dysfunction from a control group that would receive more attention from clinicians . 
fifth , there was an assumption that the renal function was similar in each split kidney because the serum biomarker based egfr was on behalf of the total renal function for each subject . 
 visual assessment was performed by two independent musculoskeletal radiologists with respect to : ( 1 ) susceptibility artefacts around the neck , ( 2 ) homogeneity of fat suppression , ( 3 ) image sharpness and ( 4 ) tissue resolution contrast of pathologies . 
 a multicentric study reported that the overall diagnostic accuracy of brachial plexus mr imaging calculated on a per - patient basis is relatively high , but false - positive cases must be taken into account , especially if a careful patient selection has not been performed [ 2 ]  . 
several mr parameters , such as tr , te , section thickness and orientation , affect the signal intensity of brachial plexus nerves in normal subjects [ 1 , 2 ]  . 
nevertheless , to study the 1 3 46 radiol med ( 2016 ) 121 : 4553 plexus , fat saturation is necessary and offers an adequate contrast of trunks and cords on fluid - sensitive sequences [ 8 ]  . 
abrupt changes in contour and density between air and soft tissue determine magnetic inhomogeneity and susceptibility artefacts , which present as regions of signal loss and architectural distortion [ 9 , 10 ]  . 
 incomplete fat suppression and anatomical deterioration are commonly encountered in fat - suppressed images obtained using the conventional frequency - selective fat suppression ( fsfs ) technique , because fsfs is sensitive to magnetic field inhomogeneity and vulnerable to susceptibility and metallic artefacts . 
recently , iterative decomposition of water and fat with echo asymmetry and least - squares estimation ( ideal ) technique using three asymmetric echo times and the three - point dixon method for separating fat and water was introduced as an alternative solution for homogeneous fat suppression and reducing metal - induced artefacts [ 1114 ]  . 
 by using asymmetric echoes to prevent fatwater swapping , which is frequently encountered using symmetric echoes , and the least - squares method , ideal technique generates a magnetic inhomogeneity field map and uses it to correct phase shift [ 15 , 16 ]  . 
a technical report described the usefulness of ideal technique in separating fat and water in head and neck mr imaging [ 18 ] and a recent report presented a successful fat quantification using this technique in parotid glands [ 19 ]  . 
all volunteers were asymptomatic and did not suffer from any disease or received any drugs altering sensory or motor function . exclusion criteria were : age under than 18 years , contraindications to mri ; pregnancy ; and history of a cardiovascular , pulmonary , endocrine , metabolic , neurological , neuromuscular , or musculoskeletal disorder , previous head and neck or cervical spine surgery . patients from november 2010 through march 2015 , 40 adult patients ( 26 women and 14 men ; median age , 53.1 years ; age range , 1875 years ) referred for brachial plexus mri were studied . 
the six - element body - array coils were combined with the three elements of the posterior part of the neck array coil , six elements of the head array coils and three elements of the spine array coils to cover the fov ( field of view ) with 18 coil elements . 
 the mri protocol included t1 - weighted turbo spin - echo ( tse ) sequences in the coronal , transverse and sagittal oblique planes and t2 - weighted turbo spin - echo ( tse ) sequences with fat saturation in the coronal , transverse and sagittal oblique planes ( as perpendicular as possible to the brachial plexus nerves ) and ideal sequences on obliquesagittal and coronal planes . 
ideal sequences are based on dixons method for fat suppression with the inand outof - phase technique : two images are acquired with different echo times ( te )  . 
averages 2500 2200 sagittal and coronal fse fast spin echo , ideal iterative decomposition of water and fat with echo asymmetry and least - squares estimation , sar specific absorption rate , te echo time , tr repetition time , 3d three dimensional , 2d two dimensional , min minutes , ms milliseconds , cm centimetres , mm millimetres , w watt , hz hertz oblique - sagittal and coronal fat - suppressed t2 - weighted ideal and corresponding fsfs t2 sequences were compared . 
tissue resolution contrast of pathologies , evaluated as the contrast - to - noise ratio for brachial plexus lesions : the signal - to - noise ratios ( snr ) for each image sequences were assessed at four levels : paraspinal , interscalene , retroclavicular and axillary . 
the snr was calculated from several regions of interest ( rois ) , as previously described in literature [ 1 ]  . the two musculoskeletal radiologists performed all image analyses independently and blinded to each other in different sessions . 
the same authors , blinded to the initial results , repeated the analyses 4 weeks after the initial session for intra - observer assessment . statistical analysis all statistical calculations and tests were performed using spss ver . 
in addition , we considered in the analysis the effects of different readers , body mass index and the distance of pathological findings from the centre of b0 as confounding factors and adjusted the statistical significance accordingly : p values < 0.01 were considered to be statistically significant for that specific purpose . intraand inter - observer variabilities at the four levels ( paraspinal , interscalene , retroclavicular and axillary ) of the brachial plexus visual assessment with respect to susceptibility artefacts , homogeneity of fat suppression , image sharpness and tissue resolution contrast of pathologies were calculated using k statistics . 
table 2 summarizes the results of quantitative analysis . tables 3 and 4 show the image quality scores for the comparison of two sets of image sequences for both oblique - sagittal and coronal planes . 
c clavicle , l lung 95 % icc intra - class correlation coefficient brachial plexus mri was requested to confirm the diagnosis of the suspicion of metastatic plexopathy from breast cancer , to assess neural infiltration in lymphomas , the presence of neuritis after a positive nerve conduction study and the number of root and cord damages after a trauma . 
b the ideal fat - suppressed t2 image shows homogeneous and complete fat suppression at the same level and clear delineation of the inferior main trunk of the brachial plexus ( arrow )  . 
to reduce patient motion , the propeller technique ( periodically rotated overlapping parallel lines with enhanced reconstruction ) and turbopropeller technique offer an effective approach to correct for motion artefacts [ 28 , 29 ] ; however , we are not aware of any employment of theses sequences for the brachial plexus . 
4 sagittal mr images in a 45 - year - old volunteer at the retroclavicular ( a , b ) and axillary levels near the pectoralis minor muscle ( c , d )  . 
ideal ( b , d ) fat - suppressed t2 image shows markedly less severe susceptibility artefacts with homogeneous and complete fat suppression and depiction of normal anatomy of the brachial plexus ( arrow )  . 
indeed , it is known that t2 signal intensity should be sufficiently reliable to identify and quantify pathological conditions in autoimmune and inflammatory neuritis affecting the peripheral nerves [ 30 ]  . 
this achievement will be useful to increase mr imaging reliability in the assessment of peripheral nerve hyperintensity . it is known that , on mr imaging , the increased signal intensity on t2 - weighted sequences of peripheral nerves has a significant overlap among patients and normal volunteers [ 31 , 32 ]  . 
these data support the hypothesis that ideal sequences are superior to standard fat - saturated sequences for the purpose of this study . we acknowledge that the acquisition time of some of the 3.0 - t images is longer than on a 1.5 - t , because the sar ( specific absorption rate ) has to be kept within limits . 
in the present study , by using fast se sequences , the image volume had to be split in several sections to overcome the sar limitation , as already done in the literature [ 1 ]  . 
also , it would be possible to reduce scan time 1 3 52 radiol med ( 2016 ) 121 : 4553 sequences in the same patient supports the reliability of our results . 
ideal may be a useful fat suppression method for brachial plexus evaluation in clinical practice . compliance with ethical standards funding this study did not receive external funding . conflict of interest the authors have no conflict of interest . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . informed consent ual participants included in the study . informed consent was obtained from all individfig . 
the questionnaire consisted of ten questions concerning general practitioners knowledge about ctc , including application of guidelines in clinical scenarios and diagnostic performance . results out of 1 , 053 general practitioners , 231 ( 22 % ) , 155 men and 76 women ( mean age 58 years ) , completed the survey . 
 of the 231 responders , 84 % were aware of the possibility * nicola flor nicola.flor@unimi.it 1 unit operativa di radiologia diagnostica e interventistica , azienda ospedaliera san paolo , via di rudin 8 , 20142 milan , italy 2 dipartimento di scienze della salute , universit degli studi di milano , via di rudin 8 , 20142 milan , italy 3 dipartimento di scienze radiologiche , oncologia e anatomia patologica , universit la sapienza , rome , italy 4 unit imaging diagnostico , ospedale icot , latina , italy 5 scuola di specializzazione in radiodiagnostica , facolt di medicina e chirurgia , universit degli studi di milano , via festa del perdono 7 , 20122 milan , italy 6 unit di radiologia , irccs policlinico san donato , san donato milanese , italy 7 dipartimento di scienze biomediche della salute , universit degli studi di milano , piazza e . 
malan , 20097 san donato milanese , italy of using ctc as a method for examining the colonrectu however , only 57 % were aware about low x - ray exposure delivered by ctc and about the possibility of using a reduced cleansing protocol . 
only 48 % were aware that ctc accuracy in diagnosing 10 - mm or larger polyps and colorectal cancers was similar to that of conventional colonoscopy , while 62 % were informed about ctc advantages in comparison with double - contrast barium enema ; 59 % thought that ctc had a potential role as a screening test ; 8586 % suggested ctc in the case of refused or incomplete conventional colonoscopy ; 79 % suggested immediate conventional colonoscopy in the case of at least one 10 - mm polyp . 
about 54 % usually prescribe one ctc every 46 months , while 36 % never have , 3 % one ctc per month , and 7 % one every 23 months . 
radiological societies should fill this gap offering dedicated educational initiatives . keywords computed tomography colonography colorectal cancer medical education survey introduction computed tomography colonography ( ctc ) represents a valid alternative to conventional colonoscopy reaching the same accuracy in diagnosing colonic polyps and colorectal cancers [ 15 ]  . 
indications for ctc are constantly increasing , and are fully accepted by clinicians and shared with gastroenterologists [ 6 ]  . there has been a significant increase in the percentage of hospitals providing ctc examinations over time and 1 3 2 radiol med ( 2016 ) 121 : 15 in the number of examinations annually performed [ 79 ]  . 
 although supported by evidence , ctc has not yet homogenously diffused worldwide . among the reasons explaining this weakness ( e.g. , conflicting recommendations ; lack of reimbursement ) , limited knowledge about this diagnostic procedure probably plays an important role . 
therefore , we focused on the general practitioners who could ask for the examination in case of incomplete or refused colonoscopy and in case of individual - based screening . the aim of this study was to verify the knowledge and interest in ctc of general practitioners working in a local community town materials and methods participant recruitment all 1 , 053 general practitioners ( 666 men and 387 women ; age range 3678 years ; mean age 58 years ) of our town were asked to fill in a ten - question , anonymous , web - based questionnaire about ctc . 
individual email addresses were downloaded from the website of our region ( crs.lombardia.it ) and physicians were emailed directly presenting a general description of the survey and an invitation to participate through a web - based link . 
recruitment of participants took place from february 2014 to march 2014 . webbased survey the questionnaire was written and reviewed by the investigators and consisted of ten questions ( table 1 ) , addressing different issues on ctc , from awareness of the technique to indications . practitioners had the option of not answering one or more questions of the survey . statistical analysis data were reported descriptively as frequencies and percentages . 
the rates of responders in males were compared with that of responders in females using odds ratio and the chi - square test . using the same tests , the age of responders was compared with that of non - responders , assuming a threshold of results responders to the invitation of a total of 1 , 053 invited physicians , 231 ( 22 % ) general practitioners ( 155 men and 76 women , mean age 58 years ) filled in the questionnaire . 
the same was true for the last five questions . of those who responded , 227 / 231 ( 98 % ) answered the whole survey , whereas four physicians skipped one to three questions . knowledge about the ct colonography technique answers to the survey are reported in table 1 . though 84 % of responders were aware of what ctc was , only 57 % knew that it implied a low x - ray exposure and that the bowel cleansing protocol generally used was more comfortable than that of conventional colonoscopy . only 48 % of responders knew that the accuracy of ctc in diagnosing polyps and colorectal cancers was similar to that of conventional colonoscopy . about 62 % of responders were informed about the advantages of ctc versus double - contrast barium enema in terms of higher accuracy in diagnosing 10 - mm or larger polyps and colorectal cancers . about 59 % of the respondes physicians trust in the potential role of ctc as a screening test . 
in the case of refused or incomplete conventional colonoscopy in patients with or without positive fecal occult blood test , a high percentage of responders ( 8586 % ) , would require ctc while 8 % of responders were in favor of double - contrast barium enema or capsule endoscopy . in the case of patients diagnosed with ctc with at least one 10 - mm or larger polyps , 79 % of responders suggested immediate conventional colonoscopy , 15 % were in favor of an conventional colonoscopy within 1 year , and 4 % suggested ctc within 1 year . about 54 % of responders declared prescribing ctc usually once every 46 months , 36 % never , 7 % once every 23 months , and 3 % once per month . we searched for difference between the mean age of ninety - four per cent of responders were favorable to responders for the ten questions . attending a course on ctc . 1 3 radiol med ( 2016 ) 121 : 15 table 1 questions and answers about ct colonography from general practitioners in [ milan ] computed tomography ( ct ) colonography is ct examination of the abdomen aimed at studying the colon and rectum , properly distended with air or carbon dioxide insufflated through a rectal catheter . 
were you informed about this before reading this questionnaire ? ct colonography is a low - radiation dose examination , not so different from what is absorbed from the environment in a year , and requires a bowel preparation generally better tolerated than that for conventional colonoscopy . 
were you informed about this before reading this questionnaire ? recent data show that the sensitivity and specificity of ct colonography in diagnosing 10 - mm or larger of polyps and carcinomas are higher than those of double - contrast barium enema . 
were you informed about this before reading this questionnaire ? do you think that ct colonography can be used as an effective technique for colorectal cancer in a patient without previous positive fecal occult blood test , in the case of refused or incomplete conventional colonoscopy , which of the following options would you choose ? double - contrast barium enema , 22 ( 10 % ) ct colonography , 187 ( 82 % ) capsule endoscopy , 18 ( 8 % ) which of the following options would you choose ? double - contrast barium enema 20 ( 9 % ) in a patient with positive fecal occult blood test and incomplete or refused conventional colonoscopy , in the case of a patient diagnosed with a 10 - mm polyp at ct colonography , which of the following ct colonography 190 ( 83 % ) capsule endoscopy 19 ( 8 % ) examinations would you request ? conventional colonoscopy immediate , 181 ( 79 % ) within 1 year , 35 ( 15 % ) within 5 years , 3 ( 2 % ) ct colonography within 1 year , 10 ( 4 % ) within 5 years , 1 ( 0 % ) 1 per month , 7 ( 3 % ) 1 every 23 months , 15 ( 7 % ) 1 every 46 months , 28 ( 12 % ) < 1 in 46 months , 96 ( 42 % ) none , 83 ( 36 % ) credits and no enrollment fee ? yes , 218 ( 94 % ) no , 13 ( 6 % ) how many ct colonography examinations do you usually order ? 10 . 
would you attend a 1 - day meeting - focused ct colonography with continuing medical education 1 3 4 discussion despite the low percentage of responders , the main result of this survey is the practitioners poor knowledge about ct colonography . 
 we could speculate that this lack of knowledge could be favored by the fact that radiologists have tried to promote this relatively new technique in the radiologic community more than in the medical community as a whole . 
in particular , it is mandatory to highlight that ctc is a lowdose radiation examination , due to the intrinsic differential between paracolic tissues and insufflated gas in the colonic lumen . 
moreover , the dose can be further reduced adopting various dose - reducing procedures ( e.g. , iterative reconstruction ; automatic tube current modulation ) which make the riskbenefit ratio more favorable [ 10 , 11 ]  . 
the lack of this kind of information can dramatically impact on the popularity of this examination among general practitioners and on the future of ctc as a screening test as well . moreover , there is strong evidence in favor of the high accuracy of ctc in detecting polyps , similar to that of conventional colonoscopy [ 15 ]  . surprisingly , practitioners poor knowledge about ctc does not substantially differ from that was reported about 6 years ago in a similar survey in the usa [ 12 ] , where the authors evaluated physicians comprehension of the role of ctc as a screening test , according to current guidelines . 
in fact , we would have expected an improvement of our data considering the time span since the previous survey , and the fact the ctc is perhaps better known in europe than in the usa . the response rate we have observed ( 22 % ) seems to be low , but it was quite expected . 
in fact , the response rate is not easily evaluable , due to the lack of an agreed standard for an acceptable minimal response rate to a survey [ 13 ]  . 
most studies have found time and workload pressure as the main self - reported reasons for low participation [ 17 , 18 ] , whereas others have suggested that negative attitudes toward research , concerns about the researchers motivations and lack of interest in the research topic also play a role [ 19 ]  . 
the study failed to identify strategies to improve participation in a research survey and the authors concluded that it could be more effective to use practitioners surveys to investigate associations instead of estimating prevalence . 
however , these authors administered their survey not only to family practitioners , but also to specialists already familiar with ctc ( general internists , gastroenterologists , oncologists , general surgeons , and radiologists from two institutions )  . our response rate was significantly lower for the years age group , and a negative relationship between response rate and age has been identified in the past [ 19 21 ]  . 
 [ 21 ] have proposed several modifications to the survey methodology for older adults . notwithstanding the poor knowledge of responders about ctc , most of them declared confidence with this diagnostic procedure : about 85 % of responders would recommend ctc among different types of examinations when conventional colonoscopy is incomplete or when the patient refuses conventional colonoscopy . 
however , it is noteworthy that 10 % of responders still suggested double - contrast barium enema as the test of choice after an incomplete conventional colonoscopy , or when conventional colonoscopy was refused . 
this result can be justified by the lack of knowledge demonstrated in this survey by two out of five general practitioners concerning the advantages of ctc over double - contrast barium enema . 
it is possible that responders were anyway more informed about and / or had a better opinion on ctc than non - responders ( vice versa is quite improbable )  . 
secondly , our response rate could have been higher if the survey had been endorsed by 1 3 radiol med ( 2016 ) 121 : 15 the general practitioners society or had more incentives ( e.g. , monetary incentives ; cme credits )  . in conclusion , this survey showed general practitioners poor knowledge about ctc and their high interest in being informed of this test . 
patients were divided into two groups : negatives , with no changes in the two positions ( supine and upright ) , and positives , with mri modifications of imaging in upright position . results orthostatic examination showed mri changes in 2870 out of 4305 ( 66.6 % ) patients , including 1252 males and 1618 females . conclusions the g - scan is useful to assess instability of the lumbar spine detecting hidden modifications of protrusions and / or herniated discs already present in the supine position . 
 mri , which is the most utilized imaging technique , has the major limitation of studying the spine in a position of relative functional rest ; indeed , images are acquired with the patient in the supine position , while the pain exacerbates in the upright position , as well as the instability of the lumbar spine [ 8 , 9 ]  . 
false negatives in mri of the spine performed in the supine position are often due to knees and hips bending associated with increasing breadth of intervertebral foramina and vertebral spinal canal ; lumbar pathological conditions related to clinical symptoms are often exacerbated by the orthostatic position and hidden in the supine position [ 8 , 9 ]  . 
magnetic resonance imaging ( mri ) enables the visualization of all structures that could cause pain , but in patients with pain originating from nerve root compression , disc herniations or protrusions , these conditions could be invisible in images obtained with the conventional supine position [ 10 ]  . 
 although results were certainly interesting , this technique , simulating a load with caudo - cranial direction , did not allow evaluation of the influence that head / body weight and muscle activation have on the lumbar spine [ 1012 ]  . 
the technological advancement of open mriscanner as g - scan ( esaote ) , which allows to obtain a 0.25 t permanent magnetic field , greater gradient homogeneity , and faster sequences , resulted in a significant improvement in signal - to - noise - ratio ( snr ) , spatial / contrast resolution and subsequently image quality . 
the purpose of this study is to retrospectively evaluate the mri - g - scan diagnostic performance in the assessment of spinal instability and the variations of some pathological conditions from recumbent to upright position . materials and methods patients we evaluated the archives of our pacs in the time interval between june 2004 and may 2014 , to identify all patients who , prior informed consent , underwent mri - g - scan lumbar examination . 
a total of 4305 patients , aged between 21 and 80 years , ( mean age 45 years ) , including 1875 males and 2430 females were selected for retrospective doubleblind study . 
this grade of rotation has been chosen to allow evaluations for a gravitational load , without creating a feeling of instability in the patient and without the need of repositioning [ 16 ]  . 
in our study we performed the examinations under physiological load first , and then , with the same sequences , in the supine position ; this mri protocol was performed in order to minimize the discomfort of the patients and to avoid possible hypotensive crisis that may arise when the patient is moved from the supine to the orthostatic stance [ 17 ]  . 
for the sagittal sequences , the acquisition parameters were a matrix of 320 mm and a 224 208 , a field of view ( fov ) of 320 1 3 40 radiol med ( 2016 ) 121 : 3844 slice thickness of 4 mm with a slice interval of 0.5 mfor 192 , fov of axial 3d hyce sequence , a matrix of 224 300 300 mm and a slice thickness of 4 mm with a slice interval of 0.5 mthe acquisition time was about 20 min for each position 5 min for the preparation / positioning . 
 all analyses were also performed using multiple logistic regression analysis and analysis of covariance to check for the influence of age , sex , bmi , type of herniated disc , spinal canal stenosis , translational intervertebral movement and changes in lordosis lumbar angle as covariates . 
the software used for statistical analysis was stata ( version 8.2 ; stata - corp , college station , tex )  . image analysis two neuroradiologists , respectively with 25 and 6 years of experience , blinded to the history and clinical objectivity of the subjects , independently reviewed lumbar mr images separately for standing and supine position . 
four mri degenerative aspects were considered in our study , including the type of herniated disc , spinal canal stenosis , lumbar segmental translational movements and postural abnormalities of the lumbar spine . 
according to the recommendations of the combined task forces of the north american spine society , the american society of spine radiology and the asnr [ 18 ] , on fse - t2 , se - t1 - weighted images and axial 3d hyce , the type of herniated disc was classified as presence or absence of protrusions and / or herniated discs , evaluated on both the sagittal and axial plane . 
the spinal canal stenosis was assessed considering the presence or absence of ligamentum flavum hypertrophy ( lfh ) [ 19 ] and calculating the midsagittal diameter of lumbar spinal canal with a cut - off of 12 mm [ 20 ]  . 
the presence or absence of lumbar segmental translational movement was evaluated considering a cut - off greater than 3 mm in the shift between two adjacent vertebrae [ 21 ]  . 
postural abnormalities of the lumbar spine were evaluated by considering changes in lordosis lumbar angle with a cut - off of 10 from sitting to standing position [ 22 ]  . 
the presence of biomechanical changes in the transition from upright to supine position was also classified by an mri evaluation of the two neuroradiologists , assigning the positive cases to the accentuation or appearance of one or more of the four degenerative lumbar aspects ; negative cases if none of these aspects did not change or did not show in standing and supine position . statistical analysis the intra and interobserver reliability concerning the analysis of the mr images performed in upright and standing positions was estimated using agreement percentage and kappa statistics according to landis and koch [ 23 , 24 ]  . 
a consensus readout was performed after all the data were results after a consensus readout of the image analysis , the total number of patients was divided into two groups : those with negative orthostatic test ( negative cases ) ( table 2 ) , with no changes in the two mr images positions ( standing and sitting ) , and those with changed mr images in the upright position ( positive cases )  . 
2 sagittal fse t2 - weighted sequences ( a and b ) images show 44 - year - old woman suffering from bilateral leg pathe mr sequence performed in supine position ( a ) shows an l3l4 median protrusion associated with retrosomatic osteophytosis which in orthostatic position creates a spinal canal stenosis ( b ) fig . 
1 sagittal fse t2 - weighted sequences ( a and c ) and axial 3d hyce images ( b and d ) show a 45 - year - old man suffering from left lumbosciatica . 
sagittal fse t2 - weighted and axial 3d hyce sequences ( c and d ) performed in orthostatic position show how the l5 - s1 protrusion increases in orthostatic position ( d ) fig . 
3 sagittal fse t2 - weighted sequences ( a and b ) images show a 57 - year - old man suffering from low back pathe mr sequence performed in supine position ( a ) shows a traslational intervertebral movement with anterolisthesis of l5 on s1 which increases in orthostatic position for an amount greater than 3 mm ( b ) 1 3 42 radiol med ( 2016 ) 121 : 3844 is also due to the number of positive cases ( p 0.0002 ) with increase or appearance of spinal canal stenosis in 9.2 % of the cases . 
the measurement is of considerable importance in the presence of suspected stenosis not detectable in the supine position , with the necessary considerations resulting from the therapeutic point of view . 
 our study showed a significant number of positive cases ( 715 out of 1178 patients , p 0.0004 ) with translational intervertebral movement greater than 3 mm and new appearance of spondylolisthesis in 9.5 % of the cases . 
progression of the degenerative phase leads to the appearance of osteophytes , with resultant restabilization and reduction in movement ; this phase of restabilization is difficult to interpret without the aid of a dynamic study of the spine especially as it regards the nerve compression at the level of foramina [ 27 ]  . 
these results as well as being due to activation of postural effects of body weight mediated by abdominal and paraspinal muscles from orthostatic to standing position [ 30 ] probably depend on vertebral instability in patient with osteoarthritis of the facet joints which may allow hypermobility of lumbosacral column [ 31 ]  . 
as we performed only a retrospective imaging evaluation another limit of the study is the lack of a more correct clinical evaluation of patients in particular in differentiating patients suffering from low back pain and sciatica . 
regarding spinal instability , dynamic mr study plays a critical role as documented by a large number of studies present in the literature although clinical and diagnostic criteria have not yet been clearly defined . 
this aspect was previously assessed in many studies [ 28 , 29 ] , but in terms of spinal canal area and a reduction of 5.2 % of the dural sac area , which was evident in the transition from the supine to the upright position , especially relating to two variables : change in position of disc and yellow ligaments . 
in our experience , the importance of mri exam performed in standing position 1 3 radiol med ( 2016 ) 121 : 3844 in conclusion , we can assume that dynamic mri exam remains an important technique for detecting degenerative aspect of the lumbar spine associated with acute and chronic low back pain for its ability to discover hidden or modifications of discal disease already present in the supine position . 
in consideration of the use of ionizing radiation and contrast media , nowadays there is a trend toward the use contrastenhanced ultrasound ( ceus ) in the follow - up of blunt abdominal trauma . 
 magnetic resonance imaging ( mri ) is a useful alternative , since its lack of use of ionizing radiation , its panoramicity , the possibility to avoid contrast media and the ability to properly evaluate even small lesions . 
the aim of this study is to evaluate the usefulness and the feasibility of mri in the follow - up of patients with low - grade blunt abdominal trauma . materials and methods we performed a retrospective review of a cohort including 270 consecutive patients with a history of blunt abdominal trauma ; among them , 118 underwent a high - energy trauma , and 152 a low - energy trauma . 
124 patients had findings of abdominal injuries at the contrast - enhanced multidetector ct ( ce - mdct ) , including 68 from the group of major trauma and 56 from the group of minor trauma . 
follow - up protocol included ceus at 24 and 72 h and ceus and mri at 1 month after trauma ; only mri was performed until the complete resolution . results ceus at 24 - h and at 72 - h from trauma showed a very good correlation with onset ce - mdct in lesions staging . 
in the remaining 28 patients , in which both ceus and mri showed disease persistence , mri , however , allowed a better definition of injury extension with respect to ceus , in terms of dimensions , edges , and morphological evolution . discussion and conclusions mri allowed to make a better assessment of injuries than ceus , allowing also a temporal stage of lesions . 
 therefore , in patients who underwent abdominal traumatic injuries conservatively treated , the follow - up at 1 month can be made by mri , due to its panoramicity and its high contrast resolution , which allow a better morphological and temporal trauma staging respect to the ceus . 1 3 28 radiol med ( 2016 ) 121 : 2737 keywords blunt abdominal trauma solid organ injury follow - up contrast - enhanced ultrasound ( ceus ) multidetector computed tomography ( mdct ) magnetic resonance imaging ( mri ) emergency radiology introduction tomography over the past two decades , there has been a shift toward non - operative treatment of patients undergoing a solid organ injury , thus requiring an increasing number of imaging studies to monitor the healing of lesions , performed by contrast - enhanced - computed ( ce - ct ) since the very beginning [ 1 ]  . 
however , in consideration of the high number of children involved in blunt abdominal trauma , the use of ionizing radiation and contrast media ( potentially related to adverse reactions ) , and the great resources of contrast - enhanced ultrasonography ( ceus ) with respect to ce - ct , nowadays there is a trend toward the use of the latter one in the follow - up of blunt abdominal trauma [ 2 , 3 ]  . contrast - enhanced ultrasound has improved us capability to detect and to better depict abdominal traumatic lesions . 
as many previous studies reported [ 46 ] , ceus , by using a second - generation contrast agent , can easily highlight the number of detected lesions , with respect to the us alone , enhancing some qualitative findings , such as lesion extension , margins , and its relationship with capsule and vessels . ceus demonstrated to be almost as sensitive as ce - ct in the detection of traumatic injuries in patients with lowenergy isolated abdominal trauma , with levels of sensitivity and specificity up to 95 % [ 7 , 8 ]  . its role seems to be really relevant in pediatric patients , as shown by valentino et al . 
 [ 9 ] who compared the sensitivity and specificity of us with those of ceus using ct as the gold standard ; in a cohort of 27 patients , ceus depicted 13 of the 14 lesions in 12 patients with positive ct scans and no lesions in the patients with negative ct scan , demonstrating that ceus was almost as accurate as ct in the recognition of solid organ injuries . however ceus has shown some limits , such as the fact that it is operator - dependent , has a low panoramicity , the small operating window reducing the visibility , and its low capability to give useful information about some complications , such as abscesses , bilomas , lesions to the urinary tract and vascular complications , requiring the use of ce - ct [ 1012 ]  . for these reasons , we have advocated the use of magnetic resonance imaging ( mri ) as a possible alternative to ceus in the follow - up of patients with low - grade isolated abdominal trauma . 
in fact , we think that all its wellknown features , such as the lack of ionizing radiation , its panoramicity , to be less operator - dependent , the possibility to avoid contrast media and the prolonged monitoring can help to better evaluate the lesion site in a follow - up setting . therefore , the aim of this study is to evaluate the usefulness and the feasibility of mri in the follow - up of patients with low - grade blunt abdominal trauma managed conservatively . materials and methods we performed a retrospective review of a cohort including 270 consecutive patients admitted to our emergency department between january 2012 and december 2014 ( 176 males , 94 females , age range 861 years , mean age 34 years ) , with a history of blunt abdominal trauma ; among them , 118 underwent a high - energy trauma , and 152 a lowenergy trauma . the 118 patients with high - energy trauma underwent at first an e - fast in the emergency room to evaluate the presence of hemo - pneumothorax and hemoperitoneum ; after obtaining the hemodynamic stability ( blood pressure > 90 mmhg , heart rate < 100 beats per minute , respiratory rate < 20 breaths per minute ) a total body contrast - enhanced multidetector ct ( ce - mdct ) was performed . the 152 patients with a low - energy abdominal trauma underwent , at first , an abdomen us and ceus . 
among these , those positive for traumatic injuries of the abdominal organs underwent a ce - mdct to obtain a proper staging of the severity of the traumatic injury . of the total 270 patients , 124 had findings of abdominal injuries at the ce - mdct , including 68 from the group of major trauma and 56 from the group of minor trauma . among them , 39 were operated for incoming lesions of liver , spleen , kidney , bowel and / or mesentery and for active bleeding ( 28 of 39 had high - energy trauma , 11 lowenergy trauma )  . 
the remaining 85 patients were treated conservatively . in our institution , in a non - operative setting , our protocol requires ceus at 24 and 72 h and a new revaluation at a middle - time by ceus and mri at 1 month from trauma . 
 any following examination is performed only by mri , until the complete resolution . among the 85 patients treated conservatively , 8 underwent surgery for delayed bleeding or because it was chosen for a surgical exploration in presence of reducing values of hematocrit and hemoglobtherefore , these patients were eliminated from the study . 
it consists of stabilized aqueous suspension of sulfur hexafluoride microbubbles with a phospholipid shell . the sequoia system has a contrast - pulse sequencing ( cps ) software which is able to recognize the fundamental non - linear response of the microbubbles ; the low - mechanical index ( mi 0.150.19 ) real - time tissue harmonic imaging ( cadence ) , instead , allows a real - time gray scale imaging [ 4 , 5 , 13 ]  . in our setting , a total of 4.8 ml of sonovue , divided into two 2.4 ml doses , were administered through a 18 - gage needle in an antecubital vein , followed by 510 ml of saline solution . 
after the first bolus the right sided organs have been explored for 13 mafter the administration of the second bolus , the left sided organs were studied for 34 min . all ceus examinations were performed by radiologists with a high level of experience , with at least 5 years experience in emergency radiology and specialized in trauma imaging . mri examinations were performed on a 1.5 t system ( magnetom avanto , siemens ) equipped with high performing gradients with phased - array coils . all the patients were required to fast for 46 h before the mri examination , in order to reduce artifacts due to bowel peristalsis . the examinations were performed on a supine position and the images were acquired on multiple planes with breath - hold haste t2 - weighted sequences ( tr : 1500 ms ; te : 95 ms ; st : 6 mm ; matrix : 384 156 ) , t1 in phase and out - of - phase ( tr : 120 ms ; te : 2.38 ms ; st : 6 mm ; 164 ) and fat - sat vibe t1 - weighted images matrix : 384 ( tr : 4.75 ms ; te : 2.39 ms ; st : 3 mm ; matrix : 352 154 ) before and after i.v. 
in particular , the latter one was employed on 71 / 77 patients ; the remaining 6 patients refused the i.v injection of contrast media . data collection this study was focused on traumatic injuries of liver , spleen , adrenals , and kidneys ; any pancreatic , mesenteric or bowel lesions were analyzed . on ceus follow - up examinations , we analyzed lesions extension in terms of dimensions , margins , location , and numbers . 
in fact , hematomas can appear as hypoechoic images without perfusion ; lacerations appear as hypoechoic linear or branched lesions , oriented perpendicular to the organ surface , usually associated with capsular discontinuity ; a bruising is usually depicted as an inhomogeneous hypoechoic area with illdefined contours with a poor definition of vessels within it ; subcapsular hematoma appear as lenticular non - enhancing area ; an active bleeding is characterized by the spreading of contrast media within the peritoneal or retroperitoneal space . ceus at 72 h and at 1 month after trauma evaluated the same parameters . 
in particular , it was assessed the extent of traumatic injury , any change of the amount of intraperitoneal fluid and of subcapsular hematoma . in the rmi at 1 month after trauma , we evaluated the size of injury , the extension to the capsule , its signal intensity related to temporal evolution ( therefore the presence of granulation tissue and peripheral contrast enhancement ) , the persistence of intraand retro - peritoneal fluid , as well as the development of any complications as bilomas , delayed bleeding , and urinomas . results ceus at 24 - h from trauma showed a very good correlation with ce - mdct in lesions staging . 
ce - ct on axial ( a ) and coronal ( b ) plane shows a small hepatic bruising localized in the vi segment , a laceration of the upper pole of left kidney and an adrenal hematoma . 
mri performed at 1 month using the out - of - phase ( e ) , haste fat - sat t2 - weighted ( f ) and vibe fat - sat t1 - weighted ( g ) sequence after gadolinium well depicts the hepatic bruising ( white arrow ) , the dimensional reduction of renal lesion and , above all , the adrenal hematoma ( black arrow ) , not shown by ceus , allowing a better definition of disease extent 1 3 radiol med ( 2016 ) 121 : 2737 trauma , of intra - peritoneal fluid and of subcapsular hematoma , showing that it was not any dimensional increasing of injury nor of hematoma . ceus performed at 1 month did not show traumatic lesions in 49 / 77 of patients . 
in the remaining 28 / 77 cases , ceus demonstrated reduction of the size of the lesions ranging from 25 % to 50 % . both at 72 - h and at 1 month , ceus was not able to give information about adrenal and urinary tract injuries , known on the ce - mdct performed at the beginning . mri performed at 1 month from trauma did not show traumatic injuries in 37 / 77 patients ; it demonstrated persistence of organ lesion in 40 / 77 patients . 
mip reconstruction ( g ) on coronal plane confirms the latter finding 1 3 32 discussion to our knowledge , until now there is not a standardized protocol for the follow - up of blunt abdominal trauma conservatively treated . table 2 number of lesions detected on ceus and mr at 1 month from trauma liver spleen adrenals kidneys ceus radiol med ( 2016 ) 121 : 2737 whereas for the detection of parenchymal lesions , there is a wide range of imaging techniques available , such as ce - mdct and ceus , instead its not the same for the follow - up management , especially when pediatric patients are involved ; in fact , in these cases , a systematic use of ct would imply an excessive exposure to ionizing radiation . in our department the protocol for the follow - up of blunt abdominal trauma conservatively treated includes a ceus at 24 and 72 h after trauma , ceus and mri at 1 month and only mri until the complete resolution or the demonstration of stabilized residual scarring . 
only in case of clinical worsening a ce - mdct is performed . this approach is related to the fact that previous studies , such as that made by miele et al . 
the mri out - of - phase sequence ( d ) performed on axial plane at 1 month from trauma shows dimensional reduction of the injury , appearing as an organizing hematoma because of a hyperintense edge , expression of extracellular metahemoglobin content . 
mri performed after 1 year from injury , using the following sequences : out - of - phase ( g ) , after contrast media on axial plane ( h ) and haste t2 - weighted on coronal plane ( i ) shows the presence of a hypointense linear streak with capsular retraction ( white arrows ) 1 3 radiol med ( 2016 ) 121 : 2737 fig . 
mri performed at 1 month ( df ) from injury using the out - of - phase ( d ) sequence demonstrates the perirenal organizing hematoma with a hyperintense edge ; after administration of gadolinium on axial ( e ) and coronal plane ( f ) there is no lesion enhancement . 
mri performed at 3 months ( g , h ) from injury shows the almost complete recovery of the perirenal hematoma ( white arrows ) of ceus to identify parenchymal lesions and the capsular involvement with an accuracy comparable to that of ct . 
 [ 12 ] ceus demonstrated to be a very effective technique in the pediatric field , showing a high correlation with ct findings . a further study by sessa et al . 
 [ 4 ] showed that ceus can be used as a technique of first approach to identify and to stage traumatic abdominal injuries conservatively treated , compared with ultrasound and ce - mdct as a gold standard . 
however , ceus proved to be ineffective to recognize 4 cases of active bleeding , and 1 case of injury of the renal pelvis . number , location , and extension of the lesions , highlighting thus its use at this stage instead of the ct , especially in young patients . however , in many experiences , ceus showed some limits because , besides being operator - dependent , it has a low panoramicity and does not provide important information about possible complications , such as the presence of bilomas , abscesses , urinary tract , and vascular lesions [ 1012 ]  . in our study , in fact , ceus did not identified 2 adrenal lesions that were already known by the onset ct , and was not able to show the state of the urinary tract in 2 patients in whom it was previously recognized a lesion of the urinary tract . in another study conducted by manetta et al . 
 [ 3 ] , ceus was employed in the follow - up of hepatic and splenic injuries , showing an excellent correlation with ct as regards as mri allowed to make a better assessment of injuries , because of the improved contrast and soft tissue resolution , allowing also a temporal stage of lesions , as several studies 1 3 34 radiol med ( 2016 ) 121 : 2737 fig . 
mri performed at 1 month ( e , f ) using the out - of phase sequence on axial plane ( e ) shows a renal hematoma with a hyperintense edge , owing to its metahemoglobin content ; vibe fat - sat t1 - weighted sequence ( f ) on axial plane doesnt show any mass enhancement . 
mri performed at 3 months after trauma with haste t2 - weighted sequence ( g ) on axial plane shows dimensional reduction of injury , with a very hypointense rim , because of hemosiderin content , as observed in chronic lesions ; out - of - phase sequence ( h ) on axial plane shows a hyperintense edge with a hypointense center , findings typical of organizing hematoma ( white arrows ) showed [ 1417 ]  . 
all these data are earned primarly from intracerebral hemorrhage infact , as for the pathophysiology , four stages of hematoma evolution are known : hyperacute stage ( 03 h ) , acute stage ( 4 h3 days ) , subacute stage ( 4 days4 weeks ) , and chronic stage ( > 1 month )  . at mri , the signal of the hematoma changes in relation with two parameters : the state of hemoglobin oxygenation ( which in turn influences the relaxation properties and magnetic susceptibility ) and the state of red blood cells membrane ( intact or lysed )  . 
during the hyperacute , the acute and the early subacute stage red blood cells are intact and the hemoglobin is transformed respectively in oxyhemoglobin , deoxyhemoglobin , and methemoglob subsequently , cell membranes lyse and the methemoglobin becomes extracellular ( late subacute stage )  . 
finally , in the chronic stage , the wall of the hematoma contains macrophages rich in hemosiderin . with se sequences , in the hyperacute phase , the signal of the hematoma appears isointense or hypointense on t1 and hyperintense on t2 - weighted images ( oxyhemoglobin ) because of the diamagnetic effect of blood rich in water and proteins . 
mri performed at 1 month using the out - of - phase sequence ( e ) and vibe fat - sat t1 - weighted ( f ) after contrast media , on axial plane , demonstrates the presence of an organizing hematoma without enhancement . 
mri performed at 1 year from injury with vibe fat - sat t1 - weighted ( g ) , vibe fat - sat t1 - weighted after contrast media on axial ( h ) and coronal plane ( i ) show the resorption of ischemic area which appears really hypointense because of superparamagnetic substances like hemosiderin and ferritin which cause a clear reduction of t1 and t2 relaxation times ( white arrows ) will be hypointense at the center in t2 - weighted images ( deoxyhemoglobin ) and hyperintense at the periphery ( oxyhemoglobin )  . 
in the early subacute stage , the intracellular methemoglobin will be responsible for a shortening of t2 relaxation times , causing a hyposignal in t2 - weighted images and a hypersignal at the periphery in the t1 - weighted images . 
during the late subacute phase , methemoglobin becomes extracellular and , being strongly paramagnetic , it will be responsible for a hyperintense signal in both t1 and hypersignal in t2 . 
in the chronic stage , the signal in t1 and t2 - weighted images is highly variable , and may be hyper , hypo , or isointense . mri , compared with ce - ct , is also able to better depict subcapsular hematoma , which is an indicator of traumatic injury , appearing as a hyperintense layer on t2 - weighted sequences ; it can also demonstrate vascular lesions , such as pseudoaneurysms , as a focular , nodular hyperintense lesion in arterial phase [ 17 ] ; a splenic infarction , appearing as a hypointense image with a hyperintense edge without contrast enhancement ; finally , it can easily demonstrate the presence of scars as hypointense linear or branched streaks with capsular retraction , as showed in our study . to our knowledge , this is the first study that describes mri aspects of the evolution of blood collection in parenchymal organs . 
mri is an excellent imaging technique for diagnosis , evaluation , and characterization of abdominal organ lesions , as liver , spleen , adrenals , and kidneys , which are parenchymal organs that we evaluate in this work . 1 3 36 radiol med ( 2016 ) 121 : 2737 fig . 
axial ( a ) and coronal ( b ) contrast - enhanced ct performed at the beginning show a wide hepatic injury of vi and v segment involving the capsule . 
mri performed after 1 month from the injury before ( d ) and after contrast injection ( e , f ) using vibe fat - sat t1 - weighted sequences on axial plane , show a complete resorption of parenchymal injury with a linear non - henancing hypointense streak with capsular retraction ( white arrows ) mri , instead , showed persistent disease in 12 of these conclusions during the phase of trauma staging , ceus at 24 - h showed a high accuracy , with a good correlation with the ce - mdct . 
it was made a simulation , assuming an exclusive use of the ct and mr equipments for cardiacct and cardiac - mr examinations , calculating the annual * maurizio centonze maurizio.centonze@apss.tn.it 1 department of diagnostic imaging , apss di trento , trento , italy 2 servizio controllo di gestione ( management control service ) , apss di trento , trento , italy 3 department of management and economy , university of trento , trento , italy 4 cardio - vascular imaging unit , giovanni xxiii hospital , monastier di treviso ( tv ) , treviso , italy 5 erasmus medical center university , rotterdam , the 6 department of radiology , ospedale ca foncello , treviso , netherlands italy 7 department of radiology , university of modena and reggio emilia , modena , italy 8 department of radiology , irccs san raffaele , milan , italy number necessary to arrive at the break even point ( bep : the point at which cost or expenses and revenue are equal )  . results on the basis of the ct costs , in order to reach the bep , performing only cardiac - ct examinations , an average of 26412752 examinations / year is needed . 
the annual time commitment of the medical professional to ensure the number of examinations to reach the bep is 26252750 h / year , equivalent to two medical doctors in a cardiology department . 
the recent cardiac - ct italian registry , in the period januaryjune 2011 , reports a number of examinations of 3455 patients in 47 different centers , distributed throughout the whole national territory . 
the annual time commitment of the medical professional to ensure the number of examinations to reach the bep is 24373125 h / year , equivalent to two medical doctors in a cardiology department . 
the recent cardiacmr italian registry reports a number of examinations of 3776 patients in 40 centers , distributed throughout the whole national territory . conclusion this research has shown that , only on the basis of costs , currently in italy is anti - economic an exclusive use of ct or mr equipment for cardiac exams , unless its not decided , regardless of the recent guidelines and clinical indications , to submit all patients with cardiac diseases ( diseases of the coronary arteries and cardiomyopathies ) to cardiac - ct and cardiac - mr examinations . 
this might likely to increase both the inappropriate examinations and either health spending and in the case of ct with important repercussions , in terms of radio - exposure , subject to forensic procedures . keywords cost analysis cardiac - ct cardiac mri 1 3 radiol med ( 2016 ) 121 : 1218 introduction the 1990s marked a turn - point in the development of economy in the italian health organizations : this discipline had a constant evolution under the qualitative and quantitative viewpoint . 
the reform of the national health service ( nhs ) , which developed through a complex and articulated sequence of measures , was characterized by the will of the law - makers at first of introducing and , later on , of promoting a managerial culture , based on the new model of corporate management on a strong responsibilization of the medical staff [ 1 , 2 ]  . moreover , the conversion of italian health structures into trade companies has made cogent the need of developing a higher attention on the topic of costs with the objective of optimizing the process of delivering services and performance , in order to meet the requirement of health and psycho - physical well - being of the population , not only in terms of efficacy ( quality of performance ) but also of efficiency ( optimization of the employed resources )  . in this range , diagnostic imaging , considered as one of the most expensive branches of modern medicine , was an excellent test of cost containment , also in relationship to the relative easiness of measuring and monitoring its performance , intended as the number of diagnostic - interventional examinations and as professional efficiency of radiologists or technologist . 
in the last 15 years , the very fast technological advancement of diagnostic imaging , especially in the field of computed tomography ( ct : multidetector equipments with high gantry speed rotation ) and magnetic resonance ( mr : equipments with homogeneous magnetic field , powerful field gradients , high slew - rate , multi - channel coils ) , enabled the development of a series of application in clinical sectors , until few years ago precluded to noninvasive diagnostic imaging : in particular , in the field of cardiology both ct and mr were established as versatile , safe and reliable methods for the evaluation of patients with suspected coronary arteries atherosclerotic disease ( ct ) and known or suspected cardiomyopathy ( mr ) [ 35 ]  . 
therefore , the number of requests for mr examinations of the heart ( cardiac - mr ) is constantly increasing and many health organizations are planning the acquisition of modern equipments , even to the extent of suggesting some devoted exclusively to cardiac imaging under the cardiologists responsibility , because cardiac - mr is an indispensable diagnostic tool and also because not always and everywhere the radiologists are enough trained to cope with this complex diagnostic field , since their diagnostic activity is very often overloaded by technically simpler tasks ( baseline musculoskeletal and neurological imaging ) , but in which the requirement of the population and the politicalsocial trust are greater . the paucity of economic resources has caused the frequent recourse by the decision makers to the methodology of health technology assessment ( hta ) , where the financial - organizational dimension ( aspects related to the various types of costs , to the scale and purpose economies , to the variation of the organizing assets prompted by the use of technology ) is acquiring an increasing importance in the processing of hta reports underlying the decisions [ 6 , 7 ]  . the purpose of this multicenter survey is to establish the congruous number of cardiac - ct and cardiac - mr examinations , in order to determine as financially justified and sustainable an investment in these two technologies for an exclusively cardiologic utilization . materials and methods the centers from july 2013 to july 2014 , the cost data of cardiac - ct and cardiac - mr examinations were collected ( respectively , computed tomography of heart without and with contrast media , code 87412 of the italian fee nomenclator and magnetic resonance of heart , code 88924 ) , related to 2012 ( consolidated data ) , from four different italian health organizations . 
the four centers which took part in the survey , in the form of filling a questionnaire prepared by the management control service of center 1 , are located in the northern - eastern and central italy ( table 1 )  . 
in addition , currently , it does not exist a nationally validated algorithm that allows an objective and indisputable allocation of indirect costs on the multiplicity of different examinations offered by a diagnostic imaging service . 
therefore , indirect costs were not included in the calculation of the cardiac - ct and cardiacmr examinations costs ; however , knowing that the margin of error is in fact minimal , because their value is very fragmented . criteria of exploitation of the examinations cost components all the various ct or mr tasks , performed by the same equipment of cardiac - ct and cardiac - mr examinations and delivered in 2012 by the single center , were multiplied by the corresponding tariff ( from the national price - list ) , in order to obtain a weighted amount of the tasks . 
then , all the weighted amounts were summed up to estimate the global weight of all the examinations performed with that equipment . ( a ) determination of the costs of depreciation and mainte1 . 
then , the cost of depreciation / maintenance of cardiacct and cardiac - mr examinations was divided by the amount of examinations performed , to obtain the cost of depreciation and maintenance per single examination . ( b ) determination of the other costs for single examination the global amount of the other costs ( various consumers , contracted services , general expenses , etc . ) of radiology unit was divided by the global number of examinations performed ( not only ct and mr )  . nance for single examination ( c ) determination of the staff cost for single examination 1 3 radiol med ( 2016 ) 121 : 1218 table 2 cost of cardiac - ct and cardiac - mr examinations in the single center and mean value center 1 center 2 center 3 center 4 mean value tariff cardiac - ct ( 87412 ) no . 
finally , the cost of the staff was calculated for each examination by multiplying the cost / minute of each individual qualification ( point 2 ) by the global time employed by the corresponding qualification for that specific examination ( point 3 ) and summing up the resulting costs by qualification . ( d ) determination of the cost of consumer goods the cost of the consumer goods employed to perform the single examination was reported as mentioned in the detection questionnaire . the sum of the costs for single cardiac - ct or cardiacmr examination results from the sum of the four cost components listed above : a when the costs of cardiac - ct and cardiac - mr examinations for single center and their mean value have been calculated , a simulation of exclusive utilization of the relevant equipment for such types of examinations was made , calculating the annual number necessary to reach the break even point ( bep denotes the amount of cardiac - ct or cardiac - mr examinations necessary to cover the costs , without profits or losses )  . 
since , in this simulation , the examinations , which should be performed by ct and mr equipment , would be , respectively , only cardiac - ct and cardiac - mr , bep is the result of the ratio between the sum of fixed costs and the tariff of nomenclator , from which the variable costs for each examination have been subtracted . results the management control service of center 1 , which has processed the data extrapolated from the questionnaires distributed to the four centers , has at first calculated the cost of cardiac - ct and cardiac - mr examinations in the single centers , extracting the mean value ( table 2 )  . before describing in detail the modes of achievement of bep , it is necessary to point out the types of cost in question , focusing in particular on the cost of the staff . 
the health organizations , typically hospitals , are characterized by a structure of the costs , which is strongly oriented towards the fixed ones and the most important topic is the cost of labor . 
this scenario is nearly never present in italy where the work relationships are more stiff , especially in the public health organizations , where the sizing of the staff is structured in such a way as to assure the complete operativeness of the various structures , from the wards to the in - patient and the outpatient services , to the diagnostic services , to the administrative offices , etc . 
in the italian health organizations , the cost of the staff is about the 3040 % of the global costs . two different scenarios of calculation of bep were suggested for both the diagnostic methods ( ct and mr ) , where the single difference consists in the type of purchase offer of the equipment , the consip oneconcessionaria servizi informativi pubblici , i.e. , the national purchase center of the italian public administration ( tables 3 / ct , mr ) versus the company one , which offers the equipment at an intermediate price versus the current market price ( tables 4 / ct , mr )  . 
in both cases , the fixed costs include the staff ( cost of one physician , one technologist , one nurse for each individual cardiac - ct and cardiacmr examination ) , the annual rates of depreciation of ct and mr equipment ( period 8 years , as established by the decree of the ministry of finance of 31.12.1988 ) and the annual fees of maintenance . 
otherwise , the cost of the staff covers a variable rate from 44 to 51 % , therefore rather high , also in 3 public centers , with a mean value of 51 % in the four centers ( tables 2 / ct , 3 / ct )  . 
similar considerations apply to cardiac - mr examinations : the cost of the examination in the private center is really higher ( 404.80 euro ) versus the three public ones ( from 203.70 euro of center 4 to 279.56 euro of center 2 )  . 
also in this instance , it is the staff , which causes the high cost of cardiac - mr examinations of center 3 ( 56 % of the total amount )  . 
this percentage is rather high also for center 4 ( 46 % ) when compared with the similar percentage of centers 1 and 2 , respectively , 37 and 29 % . 
however , the relatively low total cost of cardiac - mr examination of center 4 results from a significant spare on paramagnetic contrast media , 16.81 euro / examination against 56.92 euro of center 1 , 82.39 euro of center 2 to reach 85.12 euro of center 3 . 
this number of examinations , considering the maximum operating capacity of a modern ct scan equipment at 64 and 128 slices , can be surely performed in one shift of 6 h / day ( one examination every 30 min ) , as established in a recent official document of societ italiana di radiologia medica ( italian society of medical radiology ) [ 8 ] , whereas the reporting step ( 1 h / examination ) [ 8 ] , which includes also the complex postprocessing of native images , which is an irreplaceable component of the report , requires globally 10.5 h / day ( consip purchase offer ) or 11 h / day ( company purchase offer )  . 
on an annual basis ( 250 workdays ) , the hourly engagement of the physician , to assure the number of examinations to achieve the bep , could range from 2625 to 2750 h . concerning the cardiac - mr examinations , 2435 examinations / year ( consip purchase offer ) to 3123 examinations / year ( company purchase offer ) are necessary on average . 
differing from ct , this number of examinations , even with very performing mr equipment , can be reached in at least 2 work shifts of 6 h / day ( one examination every 60 min ) [ 8 ]  . 
considering a medical engagement in the post - processing of images ( 1 h / examination ) [ 8 ] and in the successive reporting step , respectively , 9.74 h / day ( consip purchase offer ) or 12.5 h / ( company purchase offer ) are necessary for cardiac - mr examinations . 
on an annual basis ( 250 workdays ) , the hourly debt of the physician would range from 2437 to 3125 h . accordingly , an exclusive utilization of ct and mr for cardiologic examinations would involve the need of devoting at least 2 full - time physicians . in the reality , the recent italian registries of cardiacct [ 9 ] and cardiac - mr [ 10 ] , in the period from january to june 2011 , report a number of examinations performed , respectively , of 3455 patients in 47 centers and of 3776 patients in 40 centers on the whole italian territory . 
in the light of the above described calculations of bep , an exclusive utilization in cardiologic practice of ct and mr equipment , if could produce the positive effect of reducing the default inappropriateness , resulting from an easy access to the cardiac - ct and cardiac - mr examinations , on the contrary could risk of increasing the excess inappropriateness with high health expenditure , and in the instance of ct also with remarkable repercussions in terms of undue radio - exposure , prone to medical - forensic procedures . limits this survey has used the consolidated data of activity and costs of year 2012 . 
moreover , if we want to actualize the costs , we should perform an amendment , based on the annual italian inflation rate ( 2013 : 1.2 % ; november 2014 : < 1 % )  . a remarkable difficulty during the survey was the collection of data , since the various management services , encharged along with the radiologist referees of the centers , have submitted very inhomogeneous and not always comparable data . 
this has compelled the service of the headline center ( center 1 ) under some circumstances to perform operations of normalization , to compare the results of the four centers . finally , the four survey centers are distributed into adjacent italian geographic micro - areas which are not totally representative of the whole national situation . conclusions the shortage of resources , which is characterizing the financial situation of the western countries , compels constantly the decision makersin both the political and managerial areasto rationalize the choices for the social investments . 
though the aspects of public health , in view of the sensitivity of the matter , are considered to be very important , it is impossible not to reduce the health offer , whichalong with the pension systemis the most important expenditure in the state balances . 
 though the driving forces are manyfrom efficacy to effectiveness , to juridical , ethical and social implications as stated abovethe economical aspect is the ineluctable factor for the acquisition of diagnostic imaging technology . 
this survey has demonstrated that , only on the basis of costs , at present in italy an exclusive utilization of ct 1 3 18 radiol med ( 2016 ) 121 : 1218 or mr equipment for cardiologic examinations is antieconomic , unless it is established , not considering the recent guidelines and clinical indications , to subject all the patients with cardiac pathologies ( diseases of coronary arteries and cardiac diseases ) to cardiac - ct and cardiacmr examinations . 
also considering such event , this choice could introduce unavoidably scale and purpose diseconomies , in relationship to technologies of diagnostic imaging ( echocardiography and coronary angiography ) , which are already devoted to patients with cardiac diseases . 
nevertheless , it has to be considered that the availability of ct and mr equipments , exclusively dedicated to cardiac imaging , might risk creating an increase of examinations not properly appropriate , thanks to a more easy access to examinations , resulting in increased costs for the national health service . acknowledgments we thank katia chist and angela trentin ( service of control of management of apss of trento ) for their valuable cooperation . 
moreover , we thank ernesto di cesare ( university of laquila ) and marco francone ( university la sapienza of rome ) for the advices and supply of scientific material used in this work . compliance with ethical standards funding this study was not funded . conflict of interest author maurizio centonze declares that he has no conflict of interest . 
co - author francesco de cobelli declares that he has no conflict of interest . ethical approval this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2016 ) 121 : 7079 doi 10.1007 / s11547 - 015 - 0565 - 6 radiotherapy clinical outcomes and toxicity after exclusive versus postoperative radiotherapy in supraglottic cancer : new solutions for old problems ? the case of stage iii and iv disease loredana costa1 sara pedretti2 federica foscarini2 marta maddalo2 ludovica pegurri1 nadia pasinetti1 roberta cavagnini2 stefano ciccarelli2 sandro tonoli1 stefano maria magrini1 , 2 michela buglione1 , 2 received : 3 january 2015 / accepted : 7 july 2015 / published online : 1 august 2015 italian society of medical radiology 2015 abstract purpose to compare toxicity , survival and laryngeal preservation rate after radiotherapy alone ( rr ) , radiotherapy after supraglottic horizontal laryngectomy ( shlr ) and radiotherapy after total laryngectomy ( tlr ) for advanced supraglottic laryngeal cancer . materials and methods from 1984 to 2012 , 532 patients ( pts ) were treated in our department : 273 were potentially fit for conservative surgery ( group i ) and 259 were not amenable to partial surgery ( group ii )  . results a younger age ( p 0.005 ) , a better performance status ( p < 0.001 ) , the absence of comorbidities ( p < 0.001 ) and the absence of nodal involvement ( p 0.006 ) favorably impacted on overall survival . 
the use of concurrent radical radio - chemotherapy seems to provide comparable loco - regional control to tlr . keywords supraglottic larynx cancer laryngeal preservation radiotherapy toxicity survival introduction for patients with carcinoma in situ and early - stage supraglottic larynx cancer ( slc ) conservative surgery and radiotherapy obtain similar results [ 1 ]  . 
adjuvant treatment depends on the presence of adverse features , such as positive margins [ 2 ]  . the therapeutic options in patients with advanced slc are completely different and changed over the decades . 
nowadays , selected advanced - stage slc ( t12 n or rarely very small t3 ) is managed with conservative surgery plus radiotherapy or ( more frequently ) with radio - chemotherapy [ 3 ] while more advanced tumors , if laryngeal preservation is the priority , are treated with concurrent radio - chemotherapy [ 4 ] ; concomitant high - dose cisplatin is usually preferred [ 5 ]  . 
long - term results of the rtog 9111 trial show that concomitant radio - chemotherapy obtains better local control and a higher laryngeal preservation rate than radiotherapy alone or preceded by induction chemotherapy [ 6 ]  . 1 3 radiol med ( 2016 ) 121 : 7079 even if the treatment of slc patients is considerably changed in the last 30 years , data from large retrospective series could help to understand the basis of the present therapeutic approach ; they may also be used to identify patient subsets who did not benefit from the introduction of the current treatment options ; finally , they can guide the treatment of patients not suitable for the actual therapeutic standards . 
in summary , the analysis of large retrospective databases could support the development of new solutions for old clinical problems . the large dataset of 708 patients with slc treated at the radiation oncology department , spedali civili , brescia university , from 1984 to 2012 , was therefore analyzed . 
in this paper we describe the results obtained in the advancedstage patient subgroup , including 532 patients ( pts ) , while in a companion paper the subgroup of 172 patients with early - stage disease is considered [ 7 ]  . primary endpoint of this analysis is to compare acute and late toxicity , survival and laryngeal preservation rate after different treatment options for patients with slc : radiotherapy alone ( rr ) , radiotherapy after supra - glottic horizontal laryngectomy ( shlr ) and radiotherapy after total laryngectomy ( tlr )  . 
secondary endpoint is to compare toxicity and survival registered for this retrospective series , accrued over a long time span , with those derived from the literature and obtained with the current treatment standards . to better compare the different treatment options , we further distinguished the cases potentially amenable to conservative surgery , according to contemporary selection criteria , and those for whom total laryngectomy is the only viable therapeutic alternative to radio - chemotherapy . materials and methods of the 708 patients consecutively treated for slc at the radiation oncology department , spedali civili , brescia university , from 1984 to 2012 , 4 were excluded from the statistical analysis : three pts were affected by locally advanced disease and treated with conservative surgery and inadequate radiation therapy and one patient refused to continue treatment at a dose of 38 gy . 
the subgroup of 532 patients with advanced slc , described in this paper , was divided in two subgroups : the first including 273 patients potentially fit for conservative surgery ( t1t2 n and t3 n0n1 ) and the second one the remaining 259 with locally advanced tumors , not amenable to partial surgery . 
the toxicity was considered acute if detected in the period between the start of radiotherapy up to 30 days after the end of the treatment , while late toxicity was registered from 90 days after the end of treatment until the last follow - up visit . acute toxicity was recorded in all patients , while the late one was collected in 407 patients , excluding 111 pts ( 61 pts in the first subgroup and 50 in the second one ) , who continued the follow - up visits in other oncological centers . 
we considered as acute toxicitymucosal and skin toxicity , dry mouth , dysphagia , laryngeal and neck edema ; as late toxicityskin toxicity , xerostomia , dysphagia , jaw necrosis , laryngeal and neck edema . 
the toxicities in the three different groups ( rr , shlr and tlr ) were compared with the 2 test . the pattern of recurrence analysis was performed on 476 patients , excluding 42 patients ( 23 in the first subgroup and 19 pts in the second one ) who continued the follow - up visits in other oncological centers and for whom it was not possible to get these information by phone , by contacting the physician responsible for follow - up or by consultation of the medical records of the ent department of our or other hospitals . we analyzed and compared , for the three treatment groups , the following survival data : overall survival ( os ) , disease - specific survival ( dss ) , disease - free survival ( dfs ) , local relapse - free survival ( lrfs ) , nodal relapsefree survival ( nrfs ) and metastasis - free survival ( mfs )  . 
 the following were considered events , respectively : death for any cause ( os ) , cancer or its treatment ( dss ) , any type of treatment failure ( dfs ) , failure at the tumor site / tumor bed ( lrfs ) , nodal failure ( nrfs ) and distant failure ( mfs )  . 
then the factors linked with significant differences in outcome at univariate analysis were entered into the multivariate stepwise cox proportional hazard ratio model . laryngeal preservation was analyzed by comparing the number of salvage total laryngectomies performed in the two treatment groups ( rr and shlr ) ( 2 test )  . even if for retrospective studies formal patient consent is not required , all the analysis have been performed according to the ethical standards of the institution and / or national research committee and with the 1964 helsinki declaration and its later amendments . 
patients , however , consented in writing to the collection of their anonymized clinical data for scientific reasons at the time of their treatment . statistical analyses were obtained by using the proprietary software spss 17.0 ; p value < 0.05 was considered statistically significant . 1 3 72 radiol med ( 2016 ) 121 : 7079 fig . 
1 consorts distribution of patients results treatment group i : patients potentially amenable to larynx preserving surgery ( t12 n and t3 n0n1 ) ( n 273 ) in this subgroup of advanced - stage cancer , 107 patients underwent rr , 85 patients shlr and 81 patients tlr . 
the distribution of these techniques in the three treatment groups appears homogeneous and that of the more sophisticated local recurrence nodal recurrence metastasis yes yes yes ones ( 3d , imrt ) increases significantly in the last accrual period ( data not shown )  . in approximately 5 % of patients ( 16 pts ) radiotherapy was directed to the site of disease / tumor bed ; 34 % ( 93 pts ) had also a prophylactic treatment on the neck and 61 % ( 164 pts ) had a boost on local disease ( tumor site , involved clinical nodes , r1 site , nodal extracapsular extension )  . 
significant differences in treated volumes have been documented : 60 % of the patients submitted to shlr and tlr had postoperative radiotherapy on the tumor bed and all the neck nodal regions ( total neck ) , while 94 % of the patients treated with rr had a boost dose on the disease sites and total neck prophylactic treatment . 
all these patients have been treated in the more recent accrual period . outcome and toxicity 47 local recurrences , 37 nodal progressions and 36 metastases were observed , without differences in incidence between the three groups ( rr , tlr and shlr ) [ p ( 2 ) n.s. ] ( table 1 )  . the number of salvage laryngectomies performed after rr and shlr was evaluated and compared : 8 total laryngectomies were needed , 6 in the rr group and 2 in the shlr group , without significant differences [ p ( 2 ) n.s. ] ( table 1 )  . the incidence of acute and late toxicity in the three groups was compared with the 2 test and is reported in table 2 . 
the distribution of patient features in the two groups was homogeneous and is shown in table 3 . all the patients in the rr group had a biopsy during the ent visit and all the patients in the demolitive surgery group underwent total laryngectomy . 
in the rr group 6 patients ( 10 % ) underwent a selective nodal dissection , while in tlr group 109 pts ( 64 % ) had a selective and 57 pts ( 33 % ) a radical nodal dissection , and only 5 patients ( 3 % ) were not submitted to neck surgery . the majority of the patients ( 75 % ) were treated with a 2d technique , 20 pts with a simpler 3d technique ( three half beams ) and 38 pts with conformal 3d radiotherapy . 
younger age , good ps and the absence of comorbidities resulted to predict better os and dss rates ; whereas , for the other endpoints the only prognostic factors was the nodal involvement at diagnosis ( p 0.017 ) , with a progressively worse survival in patients with more advanced n stage . discussion conservative surgery for slc should be reserved for smaller tumors ( t1t2 ) and selected t3 n0n1 cases , with invasion limited to the pre - epiglottic space [ 810 ]  . 
in our series , patients treated with such surgical procedure mainly belong to ct1 ( 14 % ) and ct2 ( 69 % ) categories and to a selected subgroup of the ct3 category ( 14 pts , 17 % ) ; ct3 patients underwent supraglottic laryngectomy extended to one pyriform sinus or the base of tongue . in 2014 the results of a survey about the role of radiotherapy after partial surgery were published [ 11 ]  . 
radiation oncologists were contacted through an online questionnaire : the majority of them recommended postoperative radiotherapy when positive / close margins or an initial involvement of thyroid cartilage were present ; in the same patient subset , ent surgeons preferred a watch and wait policy . 
the majority of radiation oncologists recommended the following doses : 6266 gy in case of positive margins , 5666 gy for close margins and 5660 gy for the initial involvement of thyroid cartilage . 
 [ 12 ] recently analyzed a series of patient with t3 laryngeal disease , treated with partial laryngectomy and nodal dissection : at 1 and 5 years the dfs rates were 96 and 78 % , respectively . 
however , a substantial percentage ( 1853 % ) of patients had adjuvant chemo - radiotherapy for positive resection margins or extracapsular extension of nodal disease : all these studies proved that partial surgery is a valid approach for 1 3 radiol med ( 2016 ) 121 : 7079 fig . 
3 dfs was significantly longer in patients treated with tlr ( p and radical radio - chemotherapy ( b ) 0.01 ) ( a ) ; no difference in dfs were found in comparison between tlr the laryngeal preservation in selected t3 cases , but often induces the need for adjuvant treatments owing to the difficulties in obtaining clear margins . 
even with the limits of a retrospective series with the main bias of a 30 years enrollment , our series reflected the data of literature : 1and 5 - year dfs was 80 , 53 and 81 , 62 % in the rr and shlr group , respectively . until the early 1990s , the standard treatment for locally advanced disease was total laryngectomy . 
this practice changed after the trial conducted by the va laryngeal cancer study group , in which induction chemotherapy ( cisplatin plus fluorouracil ) followed by radiotherapy was compared with surgery plus adjuvant radiotherapy [ 20 ]  . 
no significant difference in survival has been reported after more than 10 years of follow - up [ 21 ]  . the use of induction chemotherapy followed by radiotherapy became an alternative to laryngectomy for locally advanced laryngeal cancer in order to preserve larynx without jeopardizing survival . to determine the contributions of chemotherapy and radiotherapy to larynx - preserving treatment , the radiation therapy oncology group and the head and neck intergroup conducted a randomized trial to investigate three treatments : induction chemotherapy followed by radiotherapy , concurrent radio - chemotherapy with cisplatin and radiotherapy alone [ 5 ]  . 
this trial concluded that concurrent radio - chemotherapy is superior to induction chemotherapy followed by radiotherapy or radiotherapy alone for laryngeal preservation and loco - regional control . mostly because of the long accrual period , in our series the majority of patients affected by locally advanced disease has been subjected to total laryngectomy and radiotherapy . 
confirming the literature , even if the comparison between surgery rt and rr shows better survival for patients submitted to surgery , this is no more true comparing patients submitted to radical radio - chemotherapy and total laryngectomy . 
these results confirm the observation that , even if often used in the past , rr without chemotherapy is a sub - optimal treatment and nowadays cannot be considered the standard for locally advanced supraglottic cancer . the use of induction chemotherapy ( chemotherapy alone before local treatment ) is still controversial and it is unclear how to best incorporate it into multimodality treatment . 
recently , the results of two randomized clinical trials have been presented ( paradigm [ 22 ] and de - cide [ 23 ] ) ; induction chemotherapy followed by concurrent chemo - radiation failed to demonstrate a local control benefit over concurrent chemo - radiotherapy alone . 
however , a lower rate of distant metastatic disease was noted , suggesting that patients who are at high risk for metastatic disease might benefit from induction chemotherapy [ 24 ]  . 1 3 78 radiol med ( 2016 ) 121 : 7079 the introduction of aggressive high - dose radio - chemotherapy improved disease control at expense of higher rates of treatment - induced toxicity . 
severe swallowing disturbances and xerostomia lead to nutritional deficiency , weight loss , prolonged parenteral or gastric tube feeding , higher risk for aspiration , anxiety and depression , and diminished quality of life . 
depending on treatment ( radiotherapy alone or combined with chemotherapy ) , treated volume , radiation dose , fractionation , and overall treatment duration , the incidence of late symptomatic disturbances was reported as high as 50 % [ 2530 ]  . in our series the incidence of late xerostomia and dysphagia was 52 and 29 % , respectively ; the latter was less frequent than in literature : this may be due to the limits of a retrospective analysis ( toxicity data have been recorded with rtog scale and converted in ctcae ) and to the scarce number of patients treated with concurrent radiochemotherapy . 
recently , anatomical structures thought to be involved in developing swallowing disturbances ( i.e. , pharyngeal constrictor muscles , upper esophageal sphincter , glottic and supraglottic larynx and base of tongue ) were described and dosevolume toxicity relationships for these structures were reported [ 3133 ]  . 
a worse late skin toxicity was observed in the surgical patients of the present series , probably related to a synergistic toxic effect of surgery and radiotherapy . conclusions this analysis takes a picture of the evolution of the treatments for locally advanced supraglottic cancer during a long period ( 30 years ) and , even if nowadays some of these treatments are not the standard , it can help to understand how the addition of chemotherapy and of the new radiotherapy techniques improved already satisfactory results . 
 moreover , even if sub - optimal , these past therapeutic options ( rr alone or radical surgery rt ) could be useful in sub - optimal patients in order to obtain adequate results in terms of local and nodal disease control . in patients amenable to conservative surgery , our analysis shows that radiotherapy alone results in localregional control , overall and cause - specific survival comparable to surgical treatments ( both conservative and demolitive ) , with the only slight increase of late mild xerostomia , dysphagia and laryngeal edema , although the patients of the rr group were negatively selected . 
there is also no difference in the number of salvage laryngectomy between rr and partial laryngectomy , with comparable organ preservation . in locally advanced tumors , not amenable to conservative surgery , radiotherapy alone was significantly less effective than radical surgery followed by radiation therapy , both in local and loco - regional control of the disease , with a worse dfs . 
treatment efficacy relies on accurate staging of primary tumor and regional lymph nodes [ 6 ] , that it is performed by imaging studies such as computed tomography ( ct ) and magnetic resonance imaging ( mri ) [ 79 ]  . 
 ( 18 ) f - fluorodeoxyglucose positron emission tomography / ct ( fdg - pet / ct ) has an important role in staging and treatment planning of various tumor locations [ 1214 ] and may provide diagnostic useful information also for the anal canal cancer [ 1519 ]  . 
the recently updated european society for medical oncology 1 3 radiol med ( 2016 ) 121 : 5459 ( esmo ) clinical practice guidelines for anal cancer include pet as an optional but often recommended modality in the workup of patients [ 1 ]  . high fdg - pet / ct uptake , measured as the maximum standardized uptake value ( suvmax ) , has been shown to be predictive of recurrence and survival after radiotherapy in tumors such as cervical and lung cancer [ 20 , 21 ]  . the present study aimed at investigating the correlation amongst the baseline suvmax , and tumor characteristics , treatment response and tumor control in a series of anal canal cancer patients treated with chemo - radiotherapy . materials and methods patient population fifty - five consecutive patients , with biopsy - proven anal cancer , who underwent definitive chemo - radiotherapy after acquisition of fdg - pet / ct imaging , were prospectively enrolled in the present study after obtaining written informed consent . 
the local ethics committee approved the present work . all cases were discussed in a multidisciplinary conference with gastroenterologists , surgeons , radiation oncologists and medical oncologists . inclusion criteria were the following : age > 18 years , biopsy - proven anal canal cancer , absence of distant metastasis , absence of other concomitant tumors and no previous pelvic rt . 
pre - treatment evaluation included blood chemistries , clinical examination , endoscopy with anal biopsy , contrast - enhancement ct or mri of the abdomen and pelvis , and whole body fdg - pet / ct . 
tumor size was determined by clinical examination and inguinal lymph nodes were considered suspicious if greater than 1.5 cm on clinical or ct images or if they exhibited abnormally increased fdg uptake on pre - treatment fdg - pet / ct and biopsy confirmed , as described in a previous article [ 19 ]  . 
rt was given to all patients in a homogeneous way including the identification of the clinical target volume that was defined as the gross tumor volume plus the potential microscopic spread to the surrounding tissues and to the regional lymph nodes based on ct simulation and fdg - pet fused images as recommended by myerson et al . 
clinical and treatment characteristics of the patients series are listed in table 1 . pet / ct imaging fdg - pet / ct was performed within five working days from the ct simulation scan . 
all patients underwent fdgpet / ct with a hybrid pet / ct scanner ( biograph 16 hirez , siemens , hoffman estates , il , usa ) and ct images were used both for attenuation correction of pet data and for localization of fdg uptake . 
the pet component is a high - resolution scanner with axial diameter of field of view of 16 mm , the number of iteration was two for 24 subsets with a 168 168 pixels matrix size . 
ct images ( 5 - mm slices ) , performed without administration of intravenous contrast enhancement and with a low - dose protocol for ct acquisition ( 120140 kv : 2938 ma depending on the weight of patients ) , were obtained from the base of skull through the proximal femur . 
suv is a semi - quantitative measure of radiotracer uptake and is calculated by the following fortissue radioactivity concentration [ nci / ml ] / mula : suv [ injected dose ( mci ) / patient weight ( g ) ]  . clinical endpoints and followup data were collected to determine response to treatment , loco - regional and distant failure , disease - free survival ( dfs ) and overall survival ( os )  . 
tumor response , defined as 1 3 56 radiol med ( 2016 ) 121 : 5459 complete ( cr ) , partial ( decrease 30 % ) ( pr ) , stable ( sd ) , and progression disease ( increase > 20 % ) ( pd ) , according to the recist criteria [ 23 ] was assessed 46 months after table 1 patients and treatment characteristics treatment completion by digital examination , endoscopy with biopsy and pet / ct . 
diagnosis of recurrent tumor and distant metastasis was based on clinical and radiologic evidence of tumor relapse , possibly confirmed by biopsy . statistical analysis the wilcoxon test was used to analyze the association of primary tumor suvmax with t , n and clinical stage , pathological findings in terms of histological type and grading and tumor response . actuarial rates of disease - free and overall survival ( dfs and os ) at 2 and 5 years were calculated by the kaplan meier method and were correlated with treatment response , t - stage , histological type and suvmax by using the logrank test . 
using the log - rank test , treatment response was significantly correlated to dfs and os : patients with cr had a significantly higher os and dfs rates than patients with pr ( p < 0.0001 for both parameters )  . 
 [ 24 ] in a sample of 77 patients reported quite different results observing a significant association of higher primary tumor suvmax with an increased risk of lymph nodal metastasis at diagnosis , but not with tumor size and histology . 
the authors commented that because pet was used to stage lymph nodes , it could be a bias for the relationship between anal cancer suvmax and lymph node positivity . in our series of patients , higher values of suvmax correlated with higher tumor stage ( t3t4 )  . 
this finding could be of interest considering that other authors found a strong association of tumor size with local control and survival [ 10 , 11 , 26 , 27 ]  . in the present study , patients with higher suvmax were also at an increased risk of pr on their post - treatment evaluation , but this finding was not statistically significant . 
the same authors found that dfs was worse for patients with an suvmax > 5.6 ; however , the data had a limited statistical power ( p 0.05 ) [ 24 ]  . 
in this regard , other studies in lung , oesophageal , head and neck and cervical cancers showed that higher suvmax correlates with worse local control and diseasefree survival rate [ 20 , 21 , 28 , 29 ]  . 
on the other hand , the more recent study of bazan et al . , similarly to us , found no correlation between suvmax and dfs and os in a sample of 39 patients [ 25 ]  . 1 3 58 radiol med ( 2016 ) 121 : 5459 in clinical practice , suvmax is considered the most reproducible parameter that can estimate metabolic activity of fdg uptake . 
actually , suvmean represents the average of the intensity of uptake within a designated region of interest and mtv reflects the volume of tumor tissue with increased metabolic activity on pet . 
 moreover , the post - treatment fdg - pet / ct could allow for a better or worse prognosis prediction as observed by other authors [ 25 , 33 ]  . 
for these reasons , it would be interesting to do a multi - institutional trial although a few difficulties should be overcome including differences in pet scanners , imaging protocols , and software analysis among different institutions that could affect the measurements and modify the real impact of pet parameters . conclusion this is one of the few studies analyzing the use of pretreatment pet / ct suvmax in anal canal cancer . 
our data suggest that fdg - pet / ct for initial staging and treatment planning may also be used to identify those patients at increased risk of partial response and tumor relapse . 
our findings showed that pre - treatment fdg - pet / ct suvmax cannot directly predict tumor response and survival , but it is strongly associated with tumor characteristics such as primary tumor stage , the most important and validated prognostic factor for anal cancer . further larger prospective studies on the predictive and prognostic value of suvmax and maybe also mtv and suvmean are needed to better clarify the role of fdgpet / ct in predicting tumor response and prognosis . acknowledgments this work was supported by the lega italiana per la lotta contro i tumori lilt ( italian league against cancer ) , section of vercelli , italy . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standard the study has been approved by the local ethics committee and has therefore been performed according to the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . radiol med ( 2016 ) 121 : 6069 doi 10.1007 / s11547 - 015 - 0563 - 8 radiotherapy whole brain radiotherapy with hippocampal avoidance and simultaneous integrated boost for brain metastases : a dosimetric volumetricmodulated arc therapy study niccol giaj levra1 gianluisa sicignano1 alba fiorentino1 sergio fersino1 francesco ricchetti1 rosario mazzola1 , 2 stefania naccarato1 ruggero ruggieri1 filippo alongi1 received : 8 may 2015 / accepted : 22 june 2015 / published online : 1 august 2015 italian society of medical radiology 2015 abstract objective to develop a feasible volumetric modulated arc therapy ( vmat ) treatment in whole brain radiotherapy ( wbrt ) with a simultaneous integrated boost ( sib ) and hippocampal ( hp ) sparing in 15 brain metastases ( bms )  . methods and materials ten patients with 20 bms received a wbrt prescription of 20 gy , sib dose on bms of 40 gy / 5 fractions . 
all plans were evaluated in : homogeneity index ( hi ) , target coverage ( tc ) , maximum dose to prescription dose ratio ( mdpd ) , prescription isodose to target volume ratio ( pitv ) and paddick conformity index ( ci )  . 
planning 25 gy with acceptobjectives were for ptvwbrt , d2 % 16.7 gy ; for ptvsib able deviation of 26.7 gy and d98 % 6 gy with acceptable d95 % deviation of 6.7 gy , dmax 10.7 gy with acceptable deviation of 11.3 gy , a mean dose of 8 gy . results mean number of bms was 2 ( range 15 )  . 
about 2040 % of patients with a diagnosis of cancer will develop brain metastases during oncological history of the disease [ 1 ] and whole brain radiotherapy ( wbrt ) is considered historically the standard treatment in these patients . 
local control ( lc ) probability is considered between 0 and 71 % and median overall survival ( os ) is estimated to be between 4 and 6 months [ 24 ]  . 
in the last decades , the implementation in neurosurgical techniques and radiosurgery ( srs ) has allowed to use more aggressive local treatment with the goal to increase lc probability and potentially os . 
the literature reports a statistical advantage on os probability in patients with a single brain metastasis ( bm ) treated with a combination of wbrt and srs compared with wbrt alone . 
similarly , in patients with more than 1 bm , an advantage in the use of wbrt and srs was confirmed in terms of lc probability , intracranial time to progression , performance status improvement and decrease in corticosteroid use [ 5 ]  . nowadays , improvement in technology represented by volumetric modulated arc therapy ( vmat ) technique and other rotational intensity modulated radiotherapy ( imrt ) 1 3 radiol med ( 2016 ) 121 : 6069 associated with the introduction of image guided radiotherapy ( igrt ) allows the possibility to integrate wbrt and a simultaneous integrated boost ( sib ) to the macroscopic bms [ 6 , 7 ]  . 
the rationale is to mimic the disruptive potential of high dose per fraction prescribed in radiosurgery and stereotactic hypofractionated radiotherapy in a maximum of 5 macroscopical sites , delivering in the same time a wbrt to sterilize microscopical disease . 
this approach overcrosses the traditional srs techniques and potentially can guarantee a radiobiological advantage to reduce tumor cell proliferation and cellular repopulation that are associated with treatment failure and decrease of treatment tolerability . 
 [ 8 ] explored the feasibility of a new hypofractionated schedule in wbrt ( 20 gy in 5 fractions ) and sib ( 40 gy in 5 fractions )  . 
the use of 20 gy in 5 fractions to the wbrt can be considered an acceptable fractionations as reported by rtog determined that 30 gy in 2 weeks or 20 gy in 1 week were associated with a comparable median survival ( 1518 weeks ) and overall response rates probability ( 7580 percent for symptom palliation ) [ 9 ]  . to date , the disadvantage in the use of wbrt could be caused by the risk of neurocognitive decline related to radiation . 
recent analysis showed that hippocampal - dependent functions , including learning , memory and spatial information processing , are preferentially affected by radiotherapy [ 10 , 11 ]  . the use of wbrt with hippocampal sparing to preserve neurocognitive functions is a novel concept [ 1214 ]  . 
some clinical studies hypothesized that radiation - induced damage to neuronal progenitor cells in the subgranular zone of the hippocampi may increase cognitive decline in bms patients [ 15 , 16 ]  . hippocampal sparing is considered safe as reported by ghia et al . 
 they analyzed 272 bms suggesting that the use of hippocampal sparing was not associated with a decrease in central nervous system control probability . currently , the radiation therapy oncology group ( rtog ) is investigating whether wbrt with hippocampal sparing preserves neurocognitive function using imrt techniques including vmat ( available at : org )  . the feasibility of delivering wbrt with hippocampal avoidance and sib for bms has been reported using different rotation imrt techniques [ 14 , 16 , 17 ]  . 
aim of this study is to evaluate the feasibility of planning wbrt with simultaneous integrated boost ( sib ) and hippocampal sparing with a short schedule of 5 fractions proposed by lagerwaard et al . 
in patients with a limited number of bms . materials and methods target definition and treatment planning ten cases of patients with diagnosis of bms were planned for a vmat hypofractionated hippocampal sparing sib treatment . 
all patients presented a minimal volume of bms distance between bms and hippocampus prv inferior than 5 mthe patients underwent computed tomography ( ct ) simulation with a 1 - mm slice thickness for radiation therapy planning in a thermoplastic mask ( brainlab , feldkirchen , germany )  . 
a co - registration of volumetric t1 sequences of diagnostic magnetic resonance imaging ( mri ) , typically a 3 - dimensional spoiled gradient series with 1 - mm slice thickness was used to define target and organs at risk ( oars )  . 
gross tumour volume of simultaneous integrated boost ( gtvsib ) was defined as macroscopic contrast enhancing lesion on t1 - mri , sib clinical tumour volume ( ctvsib ) was equal to gtvsib . 
the ptvwbrt for optimization was generated by contouring the whole brain and excluding the ptvsib for each metastasis and the hippocampal avoidance structure . a linear accelerator - based radiosurgery system equipped with a multileaf collimator ( true beam , varian medical systems , palo alto , ca , and brainlab , feldkirchen , germany ) was adopted for all treatments delivery . for patient positioning , a frameless system with an optical tracking system and a cone beam computed tomography ( cbct ) were utilized . the prescription to the ptvwbrt was 20 gy with an equivalent dose in 2 gy fractions ( eqd2 ) of 23.33 gy and a / ratio of 10 gy and ptvsib of 40 gy 1 3 62 radiol med ( 2016 ) 121 : 6069 fig . 
1 hippocampal structure contoured using ct and t1 - mri ( eqd2 fractions . 60 gy - a / ratio of 10 gy ) , respectively , in 5 normal tissue sparing was quantified using the mean normalized total dose , which is the total dose given in 2 - gy fractions that would give a biologically equivalent effect as the actual fractionation schedule . 
 an a / ratio of 2 gy was assumed for the hippocampus and 3 gy for the eyes . vmat plan ct planning images and contours were transferred to the rapidarc optimization planning system environment from the eclipse ( varian medical systems , palo alto , ca ) treatment planning system using the digital imaging and communications in medicine format ( dicom )  . all plans were optimized in eclipse version 11 for 6mv photons for linear accelerator with a millennium 120 - leaf multileaf collimator ( varian medical systems , palo alto , ca )  . 
collimators were rotated of 10 to ensure that possible tongue and grove underdosage did not add up along the same lines . to reduce the inter - variability planner , an initial set of constraints , including target coverage and sparing of oars , according to previously described constraints ( table 1b ) , was defined and utilized for all treatment plans . the main planning objective was to reduce the mean dose ( dmean ) to the hippocampus without compromising coverage of the ptvsib and ptvwbrt . 
a second planning objective was to optimize the ptv dose conformity while maintaining target coverage ( tc ) for the b the same template set of constraints was used in inverse planning to ptvsib and ptvwbrt , hippocampus , eyes , optical nerves and brainstem for each plan . volume dose was calculated using the anisotropic analytical algorithm ( aaa 10.0.28 ) with a 2.5 - mm dose grid . 
cpo uses the aaa calculated plan as a starting point to compensate for differences between the simplified dose calculation algorithm used during optimization ( progressive resolution optimizer pro 10.0.28 ) and final dose calculation with aaa . to verify the delivery feasibility of rapidarc plan , quality assurance ( qa ) procedures were performed for 1 3 radiol med ( 2016 ) 121 : 6069 table 1 dose constraints of rtog and corrected for current fractionation schedule , respectively a . 
plans were delivered using 6mv photons with a maximum dose rate of 600mu / min . quantitative and qualitative evaluation of the rapidarc plans was performed using the cumulative dosevolume histogram . within each plan and for each ptvsib , the quality of rapidarc plans was assessed according to the following index : homogeneity index ( hi ) , target coverage ( tc ) , maximum dose to prescription dose ratio ( mdpd ) , vmat prescription isodose to target volume ratio ( pitv ) and a paddick conformity index ( ci )  . 
for ptvwbrt each plan was evaluated by hi and tc . homogeneity index quantifies dose homogeneity , as recommended by the international commission on radiation units and measurements [ 19 ] and as used by gutierrez et al . 
the hi was defined as the maximum dose delivered to 2 % of the target volume ( d2% ) minus the dose delivered to 98 % of the target volume ( d98% ) divided by the median dose of the target volume ( dmedian ) : hi = ( d2% d98% ) / dmedian smaller values for the hi correspond to more homogeneous dose across the target volume , and values close to 0 are optimal . tc for the target metastases and whole brain volume was measured as the volume within the target receiving a dose greater than or equal to the prescription dose ( vtpres ) divided by the target volume ( tv ) [ 14 ] : tc = vtpres / tv for tc , values can range from 0 to 1 , where a value of 1.0 represents a complete coverage . for the target metastases , we also quantified dose homogeneity using mdpd , defined as the maximum dose ( md ) divided by the prescription dose ( pd ) : mdpd = md / pd in the rtog guidelines [ 20 ] , mdpd should be < 1.25. 
in 2000 , paddick proposed an alternative conformity index with the goal of providing an objective method for comparing plan quality and eliminating false scores provided by the rtog index ( cirtog vpres / tv ) [ 22 ]  . 
the proposed index builds on the criticism of the rtog index that the overlap of the volume receiving the prescription isodose and the target volume is not accounted for . 1 3 64 table 2 patients characteristics pre - wbrt and sib patient id no . 
4. figure 5 shows the results of a gamma index distribution map ( acceptance criterion , 3 % and 3 - mm distance to agreement ) , as described by low et al . 
introduction of focal treatment as stereotactic radiosurgery ( srs ) associated with wbrt has been considered an innovative approach with the goal to increase local control and time to central nervous system progression 1 in case of limited number of lesions , not suitable for surgery only [ 24 ]  . 
the measured ( discrete points ) and calculated dose profiles ( continued line ) are in good agreement ( a blue point means a underdosage and a red point means overdosage ) 1 3 radiol med ( 2016 ) 121 : 6069 fig . 
5 a compare pop - up window with parameters for the gamma index method used in current study and institute : 3 mm for accepted spatial deviation and 3 % for accepted dose deviation for doses at the corresponding local position of reference matrix . 
b representation of color gradient gamma index : from green ( gamma index 0 ) via yellow to red ( gamma index 1.5 ) repopulation ; ( 2 ) use of a single stereotactic fraction does not guarantee the radiobiological advantages of multiple fractionated treatment , including reoxygenation and reassortment of tumor cell in the target ; ( 3 ) dosimetric uncertainty concerning wbrt and srs could combine in separated phases of planning . to date , advances in imrt , including vmat technique , permit to obtain optimal target dose coverage and oars sparing by the delivery of different doses to different volumes in the same time . 
the adoption of sib during wbrt could overcross the previous described radiobiological concerns , improving dosimetric accuracy and confirming the clinical feasibility of the procedure , as reported in the literature [ 26 ]  . in the last decades , different studies established the feasibility of sib and wbrt in multiple bms [ 27 , 28 ]  . recently , lagerwaard et al . 
the authors concluded that wbrtsib to multiple bms ( range , 15 ) for 8 patients is a rapid and accurate technique with a higher conformity index than conventional sequential wbrt and radiosurgery boost [ 8 ]  . to date , the disadvantage in the use of wbrt is determined by the risk of neurocognitive decline related to radiation and recently , several analyses showed that hippocampal - dependent functions are preferentially affected by radiotherapy [ 29 , 30 ]  . 
they found , in 10 cases with a number of bms between 1 and 5 , that ht could guarantee good results in terms of wbrt coverage , homogeneous dose distribution on bms and conformal hippocampal sparing [ 12 ]  . to our knowledge , only 3 experiences with small sample size and an overall treatment time of about 23 weeks have been published on the use of vmat technique and hippocampal sparing wbrtsib : of these , only a single report is a clinical study , 32 while the others are only dosimetric analyses [ 14 , 17 , 31 ]  . recently , kim et al . 
after a median follow - up of 14 months , a complete remission was observed in 33 % of lesions and a partial response in 45 % with a 65 % reduction of tumor volume . 
the previous to hippocampal structure was 5.23 2 analysis reported similar results in terms of dosimetric and treatment time delivery ( about 4 min ) , using different fractionations and eqd2 dose . 
moreover , they showed the equivalence in terms of excellent dose distribution of hippocampal avoidance wbrtsib with vmat technique compared to ht , and furthermore that vmat treatments can drastically reduced the time of delivery ( about onethird ) [ 17 ]  . considering the lack of literature data , this is the first dosimetric study facing the issue of sib and hippocampal sparing during extreme hypofractionationed wbrt in 5 fractions , using vmat . 
the study was designed to evaluate the feasibility of the wbrt and sib approach , very convenient in terms of overall treatment time duration for the patient and very appealing in terms of radiobiological potential advantages . 
the rationale was to mimic the disruptive potential of high dose per fraction prescribed in radiosurgery and stereotactic hypofractionated radiotherapy in a maximum of 5 macroscopical sites , delivering in the same time a wbrt to sterilize microscopical disease while sparing hippocampal regions . despite the limitations of the study ( sample size , dosimetric results , limited bms ) , the results , here presented , showed that all dosimetric parameters were satisfied in terms of target coverage and homogeneity index for ptvwbrt and ptvsib . 
when compared to the literature experiences , our analysis showed that the increasing bms number could compromise the feasibility of planning , in particular regard to the hi for wbrt . 
 moreover , the here presented schedule , with an eqd2 dose approximately of 60 gy similar to the reported literature data , offers the advantage of shorter treatment time ( only 5 fractions ) , which could be very useful in oligometastatic patients that need systemic therapy . considering the dosimetric validation of the study here reported the next step will be its application in a clinical phase ii prospective trial correlating with the use of neurocognitive test to establish the impact of wbrt , sib and hippocampal sparing in good prognosis and / or oligometastatic patients with b furthermore , other controlled prospective , also observational , studies assessing neurocognitive aspects , within daily practice , to verify the difference in neurocognitive outcome in patients submitted to wbrt or other radiotherapy regimen with or without hippocampal sparing are advocated . compliance with ethical standards conflict of interest none . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . radiol med ( 2016 ) 121 : 323326 doi 10.1007 / s11547 - 015 - 0610 - 5 radiotherapy usefulness of the dual energy fieldinfield technique in breast tangential radiotherapy hidekazu tanaka1 yuichi kajiura1 masashi kitahara2 katsuya matsuyama2 masaya kawaguchi1 takahiro yamaguchi1 sunaho okada1 masayuki kanematsu1 received : 7 july 2015 / accepted : 26 november 2015 / published online : 11 december 2015 italian society of medical radiology 2015 abstract purpose in the field - in - field ( fif ) technique in breast tangential radiotherapy , the energy of the subfield is usually the same as the energy of the main field . 
we compared two fif plans in 66 breast cancer patients : in one , the energy of the subfield was the same as that of the main field ( the mono energy plan ) ; in the other , it was higher ( the dual energy plan )  . materials and methods the photon energy of the subfield was 6 mv in the mono energy plan and 10 mv in the dual energy plan . 
the percentage of the planning target volume ( ptv ) receiving at least 105 , 100 , and 95 % of the prescribed dose ( v105 , v100 , and v95 , respectively ) was calculated , as were the maximum and mean doses delivered to the ptv ( dmax and dmean , respectively )  . 
clinical target volumes ( ctvs ) and the thickness of the breast between the chest wall and skin surface at the level of the nipple were measured . results v95 % was significantly higher in the dual energy plan than in the mono energy plan in patients with ctvs or breast thickness in the highest quartile . 
there were no significant differences in the other parameters of the two plans in these patients . conclusion these findings demonstrate the usefulness of the dual energy fif technique in patients with large breasts receiving breast tangential radiotherapy . * hidekazu tanaka htanaka - gif@umin.ac.jp keywords breast cancer breast radiotherapy breastconserving surgery field - in - field technique tangential radiotherapy introduction most patients with early breast cancer received breast - conserving treatments consisting of wide excision and postoperative whole breast radiotherapy . 
similar to mastectomy , postoperative radiotherapy reduces the risk of local recurrence and results in long - term survival [ 13 ]  . in recent years , the field - in - field ( fif ) technique has become a widely preferred method for administering tangential whole breast radiotherapy . 
several studies have reported that it better controls dose homogeneity and is useful for reducing the size of hot regions as well as cold regions [ 4 14 ]  . 
moreover , the impact of respiratory motion is smaller with the fif technique than with physical wedges [ 15 ]  . the energy of the photon beam used for breast tangential irradiation is usually 4 or 6 mv . 
however , plans in which the energy of the subfield is the same as that of the main field and plans in which it is higher have not been compared . 
herein we evaluated the usefulness of the latter plan in breast tangential radiotherapy using the former plan as the reference . 1 department of radiology , gifu university hospital , yanagido 1 - 1 , gifu 501 - 1194 , japan materials and methods 2 division of radiation oncology , gifu university hospital , yanagido 1 - 1 , gifu 501 - 1194 , japan this study was conducted with the approval of our institutional review board . 
this planning study included 66 1 3 324 radiol med ( 2016 ) 121 : 323326 patients with breast cancer ( 29 right - sided , 37 left - sided ) , all of whom had undergone breast - conserving surgery . 
computed tomography ( ct ) images were obtained using a scanner with 16 detector arrays ( lightspeed xtra ; ge healthcare , waukesha , wi , usa ) ; patients were in the supine position on a breast board with both arms above their heads and breathing freely during the scan . 
the planning target volume ( ptv ) was constructed by adding 5 - mm margins to the ctv and removing 5 - mm from the build - up region on the skin surface of the breast . 
again using mlcs for blocking , the dose to the second subfield was 24 % lower than the dose blocked in the first subfield , and beam weight was shifted as described above . 
two radiotherapy plans were created for each patient : the mono energy plan ( the energy of both the subfield and the main field was 6 mv ) and the dual energy plan ( the energy of the subfield and the main field was 10 and 6 mv , respectively )  . a dose volume histogram was calculated for each patient . 
the percentage of the ptv receiving at least 105 , 100 , and 95 % of the prescribed dose ( v105 , v100 , and v95 % , respectively ) were determined , as were the maximum and mean doses delivered to the ptv ( dmax and dmean , respectively )  . 
2 the thickness of the breast between the chest wall and skin surface at the level of the nipple was measured dosimetric parameters were compared using the wilcoxon signed - rank test . 
dmax was significantly lower in the dual energy plan than in the mono energy plan , as were the v100 and v95 % . the average v105 , v100 , v95 % , dmax , and dmean values in patients a ctv in the highest quartile ( > 598 cm3 ) are shown in table 2 . 
similar results were obtained in patients with breast thickness in the highest quartile ( > 4.7 cm ) ( table 3 )  . the average v20 gy and mld of the ipsilateral lung are shown in table 4 . 
there were no significant differences in the lung doses between the mono energy plan and the dual energy plan . discussion the fif technique has been reported to be a useful method in breast tangential radiotherapy [ 414 ]  . 
to our knowledge , this is the first report to compare the mono energy and dual energy fif techniques . in all patients in our study , v100 and v95 % were significantly higher in the mono energy plan than in the dual energy plan . 
although the mono energy plan appeared to be the better plan in all patients , it had a lower v95 % than the dual energy plan in patients in the highest ctv and breast thickness quartiles . 
 the distance between the incidence and the injection of the beam was long in large - breasted patients , and owing to the attenuation of the beam , the mono energy plan contained a region that received a dose < 95 % of the prescribed . 
 because the attenuation of 10 mv photons is less than that of 6 mv photons , the volume of the region that received a dose < 95 % of the prescribed dose was smaller in the dual energy plan than in the mono energy plan . the difference between the v95 % values in the mono and dual energy plans was small in this study . 
in patients with larger breasts than those in this study , attenuation effect would be larger , and consequently , the usefulness of the dual energy fif plan would be more evident . 
the linear accelerator in our institute produces 6 or 10 mv photons , which is why these mvs were used for the subfields in the mono and dual energy plans . 
when the energy delivered to the subfields is higher than that in this study ( such as 15 or 18 mv ) , the attenuation would be smaller and the benefits of the dual energy fif technique more apparent . 
this technique is more useful when larger breast patients are irradiated with higher subfield energy . in conclusion , the dual energy fif technique is useful in breast tangential radiotherapy for patients with large breasts . acknowledgements the authors thank all staff members in the division of radiation oncology at gifu university hospital for their valuable support . compliance with ethical standards conflict of interest the authors declare that they have no conflict of interest . ethical standard all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional review board and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
through enhanced chest scans , we obtained the tumor size values by conventional ct images , and quantitatively analyzed the densities of iodine and water in lung tumors from water - based and iodine - based material decomposition images . results tumors in 22 cases increased in size after rfa while there was no detectable change in the remaining 8 cases . 
percutaneous radiofrequency ablation ( rfa ) is a newly developed minimally invasive therapy for treating advanced primary or metastatic lung cancers that are not suitable for treatment by surgical resection . 
it is a new therapy coupled with radiotherapy and chemotherapy for the treatment of lung cancer [ 3 ]  . after rfa , the pulmonary focal area often increases , while the reactive hyperemia and fibroplasia surrounding the focus generally does not disappear . 
conventional ct cannot show the distribution of blood perfusion in lung tumors , while the spectral ct can quantitatively analyze the iodine and water density of the tumor in the lung by generating material decomposition images ( e.g. , water - based , 1 3 262 radiol med ( 2016 ) 121 : 261267 iodine - based material decomposition images ) , thus effectively reflecting the changes in kinetics of blood flow in the lung tumor under pathological conditions . 
this research examined the clinical value of quantitative iodine - based and water - based material decomposition images of spectral ct for evaluating the therapeutic effect of radiofrequency ablation in lung cancer . materials and methods patient information 30 lung cancer patients who were enrolled in this study underwent radiofrequency ablation guided by gemstone spectral imaging ( gsi ) ct examination from march 2012 to march 2013 in our hospital . 
considering the effect of spontaneous breathing by the patient during ct - guided radiofrequency ablation , the anchor - shaped rf needles were selected to be fixed inside the tumor after insertion , thus avoiding extra damage to the lung . 
after local anesthesia ( 2 % lidocaine ) was applied , the rf needle was quickly pushed in the predetermined angle to the focal area while avoiding ribs , great vessels , and bullae . 
if the tip reached the best position , the end of the radiofrequency needle was pressed so that the anchor - shaped electrode could be popped out from the sheath and its tip became umbrella - shaped . 
if the position was not appropriate , the anchor - shaped electrode was withdrawn , and the position was adjusted , and then the anchor - shaped electrode was popped out again to position at the expected location . 
the temperature was measured at a number of locations . data collection gemstone spectral ct ( discovery ct750 hd , ge , usa ) was utilized to examine the subject in a supine position . 
the specific scan parameters were as follows : gantry rotation time 0.6 s , pitch 0.984 , tube voltage 120 kv , the tube current was automatic ma , noise index 11 , and the thickness of layer and interval was 5 mm , field of view 350 mm , enhanced scan contrast agent injection trigger delay was 45 s , gantry rotation time 0.6 s , pitch 0.984 , tube current was spectral ct automatic current , tube voltage 80 kv / 140 kv instantaneous switching , thickness of layer and interval was 5 mm , field of view 350 mm , iodine - containing contrast agent was ioversol ( 320 mg / ml ) , using binoculars high - pressure syringe with 2 m / s injection rate , the total volume was 90 ml , through the cubital vein injection . data processing the spectral ct scan of each patient provided conventional mix - energy ct image ( kvp ) , 101 single energy ct images ranged from 40 to 140 kev , water - base and iodine - based density images . 
the gemstone spectral imaging ( gsi ) viewer software was used for data processing and obtaining spectral ct enhanced single energy image and water - based , iodinebased material images . 
the region of interest ( roi ) was set on the tumor , and the area of roi was 1 / 2 or table 1 the changes in area of solid tumors in 30 lung cancer cases before and after rfa 2 / 3 of the tumor region to measure the mean value of water content , the mean value of iodine content and their standard deviation ( sd ) in water - based and iodine - based images . 
water - based values and iodine - based values of the lung tumors before and after rfa were analyzed using paired sample t test to determine whether there were significant differences . 
in the iodinebased images , all 30 cases of tumor tissues after rfa ablation , resulted in significantly reduced iodine contents ( p < 0.05 ) , compared with those before rfa ablation . 
 however , in iodine - based image after rfa ( d ) , a low perfusion area could be seen clearly and the corresponding iodine value was much lower than the value before the therapy ( c )  . 
from the water - based images ( e , f ) , it can be seen that the water content of tumor was significantly increased after rfa high - speed oscillation and friction of these molecules . 
 the cancer cells stop dividing when the local temperature reaches 3940 c ; the proteins within the cell denature , the membrane lipid layer is destroyed , and the cancer cells become necrotized at 4550 c ; local tumor cells can be killed quickly at 8090 c , while the blood vessels around the tumor tissue coagulate to form a reaction zone , which cannot continue to supply blood to the tumor , thus preventing tumor evasion [ 4 ]  . 
since the normal lung tissue can release heat through blood circulation in pulmonary vessels , and the air way has an insulatory effect , the heat can be fully concentrated on the focus . 
therefore , lung tumors are very suitable for radiofrequency ablation [ 5 ]  . rfa therapy has to be carried out using imaging technology , and its efficacy should be determined by tomography examination . 
to monitor and evaluate lung cancer rfa therapy , the commonly used imaging methods including chest x - ray radiographs , type - b ultrasonic , ct , mri , or 18f - deoxyglucose positron emission tomography ( fdgpet ) are used . 
these imaging techniques can detect the echo , the change in blood supply , the degree of necrosis and the change of density in the tumors , respectively . the operator needs to know whether the tumor is inactivated by rfa completely in order to determine whether to use further treatment such as increasing the number of ablation points or performing the second ablation . 
the traditional mix - energy ct can only evaluate the efficacy based on the morphological change in the tumor , the area of low - density necrosis and the ct value . 
spectral ct can provide a comprehensive evaluation of the efficacy of rfa from a morphological perspective and as well as a functional metabolic aspect of the tumor [ 8 ]  . since gemstone is used as the detector material in spectral ct , the spectral ct has high spatial and density resolution with a concurrent reduction in the radiation dose . 
these features help determine the water content in the tumor before and after rfa , the amount of contrast agent taken up by the tumor , and their distributions within the tumor . 
 with spectral ct , it is also possible to roughly distinguish the materials within the tumor , determine the ratio of solid and necrotic portions , and provide more reliable evidence for accurate evaluation of the therapeutic efficacy . the ct scan immediately after rfa in an animal model illustrated a three - layer structure : the outermost layer was 1 3 radiol med ( 2016 ) 121 : 261267 fig . 
3 tumor was close to the right pulmonary vein and subsegmental bronchi , so the rf needle was not fully released a non - necrotizing hemorrhagic zone with a thickness of about 4.1 mm , the middle layer was alveolar exudate and the innermost layer comprising dying tumor cells characterized by condensation of cytoplasms and nuclei [ 9 ]  . 
out of 30 patients who were scanned 5 min after rfa , we found that the tumor size significantly increased in 22 of the in the water - based image , the water content of tumors in all patients after treatment increased , indicating that there was congestion and edema in the tumors . 
meanwhile , rfa also caused injuries in the surrounding blood vessels [ 10 ] , and significantly reduced tumor blood supply , leading to low - density necrosis regions to occur within the tumors , so the iodine value was significantly lower in the necrotic areas in the iodine - based images . 
taken together , the iodine - based material decomposition imaging is the main advantage of the gemstone spectral imaging ct over conventional mix - energy ct imaging . out of four cases of central lung cancer in this study , tumors in 2 of the cases were very close to pulmonary vascular ve therefore , the rf needles were not fully released . 
therefore , spectral ct can effectively identify coagulated necroses and residual tumors , thus providing more accurate radiographic evidence for therapeutic efficiency . among 30 patients , 10 cases with the tumors closed to periphery were selected for biopsy examination . 
these observations were consistent with the areas of decreased iodine content and the areas of increased water content in the tumors shown by the gsict images . the therapeutic effect of rfa for the treatment of lung cancer has been confirmed . 
 in contrast , gemstone spectral imaging ( gsi ) ct significantly reduces the radiation dose , and there are many reports about the applications of gsi - ct in the treatment of cancer [ 13 , 14 ] .gsi - ct can be used in operative positioning to guide rfa therapy for lung cancer . 
moreover , by comprehensively analyzing many factors before and after rfa treatment , including the size of the solid portion of the tumor , ct value , water content and iodine content values , gsi - ct can provide more accurate and reliable information for evaluating the therapeutic efficacy of rfa . 1 3 radiol med ( 2016 ) 121 : 261267 266 fig . 
 the monochromatic ct image ( left side ) showed that there was a low - density necrosis region ( red circle ) in the tumor after rfa , but the image contrast was low . 
in the iodine - based material decomposition image ( right side ) , the iodine content in the low - density region ( cyan circle ) was clearly lower than the rest tumor , so the coagulated necrosis region and residual tumor region can be effectively identified by the high image contrast fig . 
b showed a large number of fibrous connective tissue cells and inflammatory cells , without abnormal , or dark nuclear staining conclusion by comprehensively analyzing changes in the size of the solid portion of the tumor , ct value , water content and iodine value , gsi - ct can illustrate changes in morphology and the metabolic state of tumor tissue before and after rfa treatment . 
therefore , gsi - ct can serve as a good means for assessing preoperative tumor positioning and can be a reliable platform to determine the therapeutic efficacy of rfa . compliance with ethical standards conflict of interest no conflict of interest exists . ethical approval all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional . informed consent ual participants included in the study . informed consent was obtained from all individradiol med ( 2016 ) 121 : 252 doi 10.1007 / s11547 - 016 - 0625 - 6 erratum erratum to : mr imaging of perianal fistulas in crohns disease : sensitivity and specificity of stir sequences giuseppe lo re1 chiara tudisca1 federica vernuccio1 dario picone1 maria cappello2 francesco agnello1 massimo galia1 maria cristina galfano1 ennio biscaldi3 sergio salerno1 antonio pinto4 massimo midiri1 roberto lagalla1 published online : 1 february 2016 italian society of medical radiology 2016 erratum to : radiol med doi 10.1007 / s1154701506034 in the original publication , the first and last names of the sixth author were interchanged . 
 three radiologists assessed the subjective image quality by comparing the image series with the one acquired with the reference protocol ( 120 kv , slice thickness 0.625 , noise index 28 , asir 40 % )  . results although the highest cnr values were obtained for the 80 kv acquisitions , qualitative scores were higher for 100 and 120 kv at the same noise index . 
an optimized protocol was established with a ni of 39.2 , asir 60 % , 100 kv for smalland medium - sized patients and 120 kv for large - sized patients , with a dose reduction of 47 % . conclusion when different dose reduction parameters are available , anthropomorphic phantoms of different sizes help to find the optimal combination . 
for aorta studies , 100 kv with relative high values of noise indexes and iterative levels provides the best balance between dose reduction and image quality . keywords computed tomography radiation dose dose optimisation iterative reconstruction aorta introduction dose reduction in computed tomography is a continuous challenge for both industrial manufacturers and clinical operators . 
among other factors , tube current modulation and iterative algorithms could allow a dose reduction of about 60 % [ 1 ] , but the exact dose saving depended strongly on the parameter choice of the user . 
the iterative algorithm level is also adjustable and his strength should be calibrated to reduce image noise without introducing artefacts . after the introduction of iterative algorithms , other optimisation techniques should be revised considering the new image post processing possibilities . 
for example , several studies highlighted the advantages of reducing kv from 120 to 100 or 80 for contrast and angiographic tc studies , as a consequence of the contrast noise ratio enhancement related to the improvement of the match between the x - ray spectrum and the k - edge of the iodine contrast medium [ 2 11 ]  . 
this beam quality optimisation is limited by the size of the patient , and low kv values are suggested and practically usable only for bmi values below a specified threshold . 
above this threshold , the noise increment associated with low kv becomes intolerable , and even the tube current modulation is not able to achieve an acceptable noise as a consequence of the saturation of current values associated with x - ray tube loading limits . 
in this context , iterative algorithms could play a significant role to extend the low kv techniques , as the noise reduction they provided could allow the use of low kv also for large - sized patients . 
benefits of the use of iterative reconstruction in combination with kv reduction have been demonstrated in some recent studies [ 1219 ]  . multislice ct can be used to diagnose various abnormalities of the aorta , such as aortic aneurysms , aortic dissection , traumatic aortic transection , and congenital malformations [ 20 ]  . 
due to the multiple scan performed for each ct aorta examination ( basal , contrast and late phase ) and to the need of thin slices with acceptable noise , patient dose can reach tens of msv for each exam . the aim of this study was to optimize an aorta angiographic ct protocol , by investigation of the best combination of tube current modulation , iterative algorithm strength and kv reduction for patients of different sizes . external envelope of medium density sheets to simulate different patient sizes , described as follows : the phantom originally does not contain any vascular structure ; but after the removal of the phantom base , it is possible to insert objects within the soft organs already present . 
a 25 - mm - diameter and 38 - cm - long medical plastic corrugated tube was connected with two intravenous feeding tubes and filled with a concentration of 9.25 mg per millilitre of iodinated non - ionic contrast medium ( 370 mg iodine / ml , ultravist iopromide , bayer pharma , germany )  . 
figure 1 shows a 3d rendering of this described vascular insert . the phantom lateral diameters at the chest and abdomen level were , respectively , 29 and 26 cthese dimensions correspond to a slim patient . 
in order to explore protocol optimisation possibilities also for patients of different dimensions , radiotherapy bolus sheets were used to adapt the phantom and to simulate other two patient sizes . 
two sheets were applied to the entire phantom surface to simulate a medium body , with an effective lateral dimension of 35 cm at the chest and 32 cm at the abdomen . 
another 6 cm increase in lateral dimensions for the large patient was obtained by applying other 2 bolus sheets to the lateral and anterior surface of the phantofigure 2 shows a picture of the phantom with applied bolus and ct images of the three phantom configurations . materials and methods phantoms characteristics scan acquisition an anthropomorphic phantom ( 3d torso phantom , cirs , norfolk , virginia , usa ) was used to simulate an adult patient . 
this phantom is made of radiologically tissueequivalent material , and its internal structure includes artificial skeleton , lung and soft tissues ( muscle , heart , liver , pancreas , kidneys ) formulated to simulate the physical density and linear attenuation of actual tissues to within 2 % in the diagnostic energy range . 
for the purpose of this study , this commercial phantom was modified by the insertion of a tube with contrast medium to simulate an aorta and by the ct scans were performed with a multislice ct ( lightspeed 64 vct , ge , milwakee , wi , usa )  . 
the parameter used to specify the desired image quality was the noise index ( ni )  . for each phantom configuration , a first image series was obtained with the clinical protocol used for aorta aneurysm studies as follows : 120 kv , slice thickness 0.625 mm , ni 28 , rotation time 0.5 s , beam collimation 1 3 radiol med ( 2016 ) 121 : 291300 fig . 
2 the phantom used in the large configuration and , on the right , three sections at the same anatomical level for the three phantom sizes 40 mm ( 64 0.625 ) , pitch 0.984 , fov 36 cm , scan length 45 cm , percentage of asir of 40 % . 
we used 80 and 100 kv for the small and medium phantom , whereas for the large phantom , only 100 kv was considered , as we verified that at 80 kv the current modulation always forces tube current to the maximum value without the possibility of reaching the expected noise stated as ni . 
we did not study percentages greater than 70 % as also in previous studies [ 21 ] we found that noise pattern and edge definitions resulted to be unacceptable at greater iterative percentages . 
a total of 28 image series were acquired for both the small and medium patient , resulting from the sum of the reference protocol plus the combination of three kv , three ni and three asir levels . 
for the large phantom , the image series without the 80 kv selections were 19 . in order to observe the current modulation trend without limitations , minimum and maximum ma were always set to the absolute minimum and maximum current values of the scanner . 
in some cases , for small kv and ni values and mediumand large - sized patients , the rotation time was increased to 1 s to avoid the saturation of tube current modulation . radiation dose the volumetric computed tomography dose index ( ctdivol ) and the dose length product ( dlp ) provided by the equipment user interface were recorded for every exposure condition . 
the accuracy of these provided values was verified by comparing the values measured during the routinely quality controls , finding a maximum difference of 5 % . objective image quality quantitative noise and contrast noise ratio ( cnr ) of all the performed scans were investigated after the selection of 9 sample sections chosen at different anatomical levels : shoulders , upper lung lobes , mediastinum ( with three levels cranial , central , and caudal ) , diaphragm , abdomen ( with three levels upper , central and lower )  . 
at the lower level of the abdomen , a phantom valve was present with metallic artefacts in the image , but this was an interesting element as simulation of the presence of external devices sometimes presents also for clinical examinations . 
figure 3 shows an example of considered sections and rois positions for the small phanto analogous roi position was considered for the medium 1 3 radiol med ( 2016 ) 121 : 291300 294 fig . 
3 section and rois considered for the quantitative evaluation of image quality , for the small phantoimages were extracted from 9 different anatomical levels : shoulders , upper lung lobes , mediastinum ( with three levels cranial , central , and caudal ) , diaphragm , and abdomen ( with three levels upper , central and lower )  . 
data were analysed by using the kruskal wallis test to evaluate the statistical significance of the scoring values and of the interobserver variability . 1 ( poor ) , 0 ( equivalent ) , where r1 and r2 are the average density values of two considered rois and 1 and 2 the relative standard deviations . 
 noise and cnr average values for all the considered slices of each acquisition were then calculated and plotted versus acquisition parameters . results radiation dose subjective image quality and statistical analysis subjective image quality assessment was performed by 3 experienced radiologists on the pacs diagnostic workstation . 
 the readers performed an independent evaluation of image quality for a subgroup randomized image series obtained with different kv , noise indexes and asir percentages , comparing them with the image series acquired with the reference clinical protocol previously described , for each phantom size . 
the perceived noise , contrast , edge sharpness , vessel visualization quality , quality in volume rendering ( vr ) and in maximum the ctdivol dose values associated with all the different parameters settings are reported in table 1 . 
as a consequence of the current modulation algorithm finalized to obtain a constant noise also with different patient sizes , dose values were very different for the three phantom configurations . 
in particular , ctdivol values for the large and medium - sized patients were , respectively , about 4 and 2 times the ctdivol for the small phantothe dose reduction relative to the reference protocol was similar for 120 and 100 kv protocols , whereas for the 80 kv protocol , it was inferior . 
the relative noise is slightly lower than 1 for a ni of 33.6 and an asir percentage of 70 % , whereas it is greater for all the other protocols and it reaches a value of 80 % greater than the noise of reference protocols for the 80 kv combined with a ni of 44.8 and an asir percentage of 40 % . 
cnr values obtained with 80 kv and asir 40 % were comparable with values that were obtained with 100 kv and asir 6070 % . subjective image quality a subsample of the obtained image series was submitted to the subjective evaluation of three radiologists , with criteria of choice described as follows . 
with a ni of 44.8 , we include 80 and 100 kv series with an asir percentage of 70 % , whereas for a ni of 39.2 , we considered an asir percentage of 60 % . 
with this ni value , also a 120 kv series was considered , with asir at 70 % , which resulted in a quantitative noise similar to the reference protocol with a 20 % cnr increase . 
at the end of this selection , the radiologists evaluated 9 series for the small and the medium phantom , respectively , and 5 series for the large phanto we have decided not to include all the images in the subjective evaluation in order to concentrate the dedicated time and attention on a subgroup of selected image series . 
 figure 5 shows a sample of images extracted from these considered scans for the medium phantom . table 2 shows the resulting average scores attributed by the three radiologists to the selected image series . 
in over a total of 125 single scores , there was a perfect agreement in 47 % cases , a maximum difference of 1 point in 52 % of cases and a difference of 2 points only in 1 case . statistical analysis the application of the kruskalwallis test with multiple comparisons for each image quality parameters highlights image series with scores significantly lower than the other ( bold values in the table )  . 
despite the fact that all image series were judged as diagnostic images and almost all show little differences from the reference in terms of vessel visualization , there were several negative scores for the images obtained with the highest ni of 44.8. 
with a ni of 39.2 and 100 kv , only the vr scores for small and large phantom were significantly lower , whereas in terms of contrast , vessel visualization and mip average scores null or slightly negative were obtained . 
however , since the cnr increase with kv reduction does not correspond to higher image quality scores in the subjective analysis , we decided to perform another 1 3 296 radiol med ( 2016 ) 121 : 291300 fig . 
4 relative noise and cnr values normalized to the measurements obtained with the reference protocol ( 120 kv , ni 28 , asir 40 % ) for the three phantom sizes fig . 
 two out of the three radiologist agreed that 100 kv is the best for the small and medium phantom , whereas 120 kv is better for the large phantowe stored the 100 kv protocol in the ct user interface , with the indication of modifying it to 120 kv for patients with thorax lateral dimension greater than 38 cm . discussion after the commissioning of a new ct scanner and the implementation of a first version of protocols for each diagnostic objective , different strategies can be adopted to optimize the patient radiation dose and image quality . 
in contrast ct studies , it has been demonstrated that lowering the kv setting allows to improve contrast enhancement , offering the possibility of reducing patient dose or contrast medium concentration . 
however , in the presence of tube current modulation , a kv variation does not provide any dose reduction , as the tube current is increased to compensate the lower kv . 
also in this study , table 1 shows that protocols with 100 or 80 kv are associated with dose from 10 to 30 % higher of protocols with 120 kv and same noise index value . 
as a consequence , a low kv technique can provide an effective dose reduction only if associated with a proper tube current modulation parameter , as the noise index for the ct equipment used in this study . 
they introduced a novel index of image quality , iodine contrast to noise ratio with a noise constraint , to characterize the different image quality requirements by various clinical applications . 
this strategy was evaluated without iterative algorithms , which allow to further reduce image noise but also introduce other image appearance modifications , in terms of sharpness and artefacts . quantitative evaluations performed in this study evidenced a 20 % increase in cnr and a 40 % increase in noise as a consequence of a 60 % increase of the noise index ( from 28 to 44.8 ) in combination with 80 kv and 70 % of asir , for smalland medium - sized patients . 
however , considering the modest dose reduction related to the noise index increment of 39.244.8 ( about 10 % ) and the number of image quality scores significantly lower for the higher ni , we have decided to adopt the ni level of 39.2 for the optimized protocol . 
 [ 4 ] used different geometric phantoms to optimize an abdominal angiographic ct protocol , obtaining image quality scores for 100 and 80 kv image series equal or lower than corresponding series with 120 kv , even with higher cnr . 
the impression of the three blinded readers was that the contrast enhancement associated with low kv does not provide significantly better diagnostic information , especially for the vessel analysis usually performed in an aorta study . 
it is also possible that negative scores were in part associated simply with a perception of difference from the habitual image appearance that produces a diffidence of the radiologist in the image information . 
further investigations are needed in this field to consider the value of quantitative evaluations in relation with the perceived image quality . in terms of the final image noise , the 39.2 value of ni with a percentage asir of 60 % corresponds to a ni choice of 22.7 without iterative , as every 10 % of asir percentage a 7 % reduction of noise was expected [ 21 ]  . 
this demonstrates that iterative algorithms allow great dose saving and also major opportunities of using low kv values also for mediumand large - sized patients , which were not possible in the past . 
in fact the average tube current values observed in this study for the three phantom sizes at 100 kv and ni 39.2 were 145 ma for the small , 330 ma for the medium and 320 ma ( in combination with 1 s of tube rotation instead of 0.5 s ) for the large - sized patient . 
this fact has been previously reported in several other studies with equipments without iterative reconstruction [ 2 , 7 , 11 ] and it is the first reason of using 80 kv or 100 kv for different patient sizes . 
with the widespread availability of ct scanners equipped with iterative reconstruction , the use of low kv will be easier and more common . main results of published optimisation studies are often expressed in terms of dose reduction respect of the reference protocol . 
but with the developments of last - generation ct equipment that used different dose reduction devices , it becomes important to consider what the reference protocol is , as further dose reduction depends on the starting point . 
these are all patient studies , and the dose reduction claimed was in the range 2350 % , but for the average ctdi , there is a difference of more than ten times between the lowest and the highest dose study . 
in this study , we started from a reference protocol with asir at 40 % and a relative high ni of 28 , resulting in a ctdivol value of 10.9 for the medium phantom , lower than the optimized protocol of cornfeld et al . 
after the adoption of optimized protocol , we observed a dose reduction of 47 % with ctdivol values of 5.9 for medium - sized patients , similar to values of shindera [ 9 ]  . 
who compared the dose received by the same patients between a first chest ct angiography and a second one in the follow - up after a reduction of 20 kv of the protocol beam potential and the introduction of the iterative algorithm . to our knowledge , this is the first phantom study for ct angiography that has considered the complex interplay between different phantom sizes , kv reduction , tube current modulation and iterative algorithms , with objective and subjective image quality evaluations . 
on the other hand , there are some limitations . first of all , we have analysed only one ct equipment and only the relative iterative algoriththis is a common limitation of these kind of studies , a problem that limits the translation of the results and of the optimisation strategy to other equipments . 
comparison studies evidenced similar performances for statistical 1 3 radiol med ( 2016 ) 121 : 291300 methods , whereas model based show superior possibilities with better image quality even at very low doses [ 19 ]  . a second limitation is related to the phantom structure that does not simulate any small vessels or pathologies like endoleak , thrombus , intramural hematoma or aortic dissection . 
the optimized protocol was defined considering a parameter combination that allows to maintain the same image quality of the reference protocol . a final limitation is that we did not investigate different contrast medium concentrations . 
it is possible that with the optimized protocol that was found , there are margins to also reduce contrast , but further investigations are needed , which go beyond the purpose of this study . in conclusion , the approach used with multiple anthropomorphic phantoms allowed us to investigate dose reduction possibilities for different sized patients . 
our purpose was to evaluate the role of the stir sequence in the detection and characterization of perianal fistulae comparing it to the post - contrast t1 sequence and correlating it with rectal examination under anesthesia . materials and methods we retrospectively reviewed all clinical records of 31 cd patients , suspected of having perianal fistulas , who had been submitted to an mr study before and after contrast medium injection and surgical exploration under anesthesia within the same month . 
finally , comparison between stir and post - contrast t1 - weighted fat saturated sequences was done . results 29 fistulas were detected in 25 patients who underwent an mr study . 
 the lifetime risk for developing a fistula in cd patients is approximately 2550 % [ 1 , 2 ] , while recto - vaginal fistulas accounted for 9 % [ 3 ]  . 
the surgical examination under anesthesia ( eua ) has been considered the gold standard for assessing fistulas for years and its tested accuracy is up to 90 % [ 4 , 5 ]  . 
fistulography [ 6 ] and pelvic computed tomography ( ct ) [ 7 , 8 ] are unlikely to be sufficiently accurate . pelvic magnetic resonance imaging ( mri ) is a highly accurate non - invasive modality for the diagnosis and classification of perianal fistulas [ 9 ]  . according to the recent european crohns and colitis organization ( ecco ) guidelines [ 10 ] , mri surpassed ( eua ) in terms of accuracy and is recommended during 1 3 244 radiol med ( 2016 ) 121 : 243251 the initial diagnosis of perianal cd unless there is a need for immediate drainage of sepsis . 
mri proved to be accurate in the achievement of an optimal definition of the pelvic anatomy and in the detection and classification of superficial and deep fistulas and their relation to surrounding structures [ 1113 ]  . 
most mri protocols routinely use intravenous gadolinium contrast - enhanced images for the evaluation of perianal cd , and more recently subtraction techniques have been used as well as dynamic imaging [ 7 , 14 ]  . since 1998 , stir ( short - tau inversion recovery ) sequences , which do not require contrast medium injection , represent a proved useful tool in the classification of fistulain - ano and in the assessment of the anatomy of perianal fistulas . 
recent guidelines reported the usefulness of gadolinium - enhanced t1 - weighted sequence for the differentiation between fluid / pus and granulation tissue [ 18 ]  . however , the use of contrast medium involves higher costs and possible adverse drug reactions [ 19 , 20 ] ; moreover , it is contraindicated in some patients . this study was designed to determine the accuracy of mri using stir and post - contrast t1 - weighted fse in assessing suspected cd perianal fistulas relating the findings of these sequences to rectal eua . the study was a retrospective , double blind comparison of the usefulness of stir and gadolinium - enhanced mri sequences in the detection of fistulas using rectal eua as the gold standard . 
 only those patients who had undergone surgical eua and pelvic stir and gadolinium - enhanced mri within the same month were considered to ensure no changes in fistula anatomy between the assessments of the different diagnostic modalities . 
the interpretations of mri studies were compared to the definitive surgical findings . as standard protocol of our institution , all patients were asked to sign an informed consent to use their personal data and every patient also had to read an informative report about the tutelage of the personal data . 
no patients had undergone a previous surgical procedure for their perianal cd . exclusion criteria were age below 18 years , pregnancy , contraindications to pelvic mri ( as implanted metal devices or documented allergic reaction to contrast medium ) , and renal insufficiency . of the 137 patients who performed pelvic mri to evaluate perianal cd from january 2010 to december 2013 , just 31 ( 16 males , mean age 37.2 years , range 2058 years ) had undergone surgical eua within the same month and were enrolled in the study . mri technique all the mri was performed with an 1.5 tesla superconducting magnet ( ge medical systems , milwaukee , wi , usa ) coupled with an external eight - channel pelvic phased - array coil . 
the pre - contrastographic sequences were obtained in the three orthogonal imaging planes ( axial , coronal , and sagittal ) using a fast - spin echo ( fse ) pulse sequence . 
fistulas were classified according to the parks criteria [ 16 ] as follows : superficial ( a ) , inter ( b ) , trans ( c ) , supra ( d ) or extra ( e ) sphincteric . 
a simple fistula was defined as a superficial , inter - sphincteric , or low transsphincteric fistula that has only one opening and is not associated with an abscess and / or is not connected to an adjacent structure such as the vagina or bladder . 
in contrast , a complex fistula was defined as the higher one ( i.e. , high trans - sphincteric , extra - sphincteric or supra - sphincteric ) , has multiple openings , horseshoeing , is associated with a perianal abscess , and / or connects to an adjacent structure such as vagina [ 17 ]  . 
the location of the enteric communication ( i.e. , the internal opening ) was recorded with respect to a clock face and its level was recorded as either anal or rectal . 
a horseshoe extension was defined as any extension from the primary track that appeared to extend to both sides of the internal opening ; its presence and location ( inter - sphincteric , infralevator , supralevator ) were recorded . 
moreover , the presence and anatomic location of any abscesses were recorded as follows : superficial , intersphincteric or supralevator . surgical eua one experienced colorectal surgeon evaluated the patients and performed the eua . 
 then , mri results were given to the surgeon at the end of the examination , after his assessment ( while the patient was still under anesthesia ) to maximize his chance of detecting fistula tracks and extensions . 
for each type of fistula , the number of true - positive , true - negative , false - positive and false - negative diagnoses for both imaging techniques and eua was also assessed , so that sensitivity ( 95 % confidence interval , ci ) could be determined . 
analysis was ure of agreement , 1.0 carried out using the software statistical analysis system ( sas institute , inc . , cary , nc , usa )  . results considering the 31 patients enrolled in the study , fistulas were detected in 25 patients who underwent stir and gadolinium - enhanced mri examinations ( table 1 )  . eight patients had simple fistulas and 17 had complex perianal disease . 
the number of fistula tracks detected according to the different diagnostic modality is shown in table 2 . false - positive diagnoses were made with mri in two patients ( 6.4 % ) who presented with posterior perianal pathese patients were diagnosed with a type b fistula based on imaging , but surgical eua did not reveal any fistula . 
table 3 shows the sensitivity of stir , gadolinium - enhanced mri and surgical eua in detecting fistulas and abscesses . imaging was less sensitive than eua only for the detection of superficial fistulas . 
for the detection of perianal fistulas of any type , there was a perfect 1 3 246 table 1 diagnostic yield of magnetic resonance imaging techniques radiol med ( 2016 ) 121 : 243251 stir gadolinium - enhanced mri number of patients number of lesions number of patients number of lesions fistula type * superficial inter - sphincteric trans - sphincteric supra - sphincteric extra - sphincteric totala horseshoes internal openings abscesses superficial supralevator totalb stir short - tau inversion recovery , mri magnetic resonance imaging * according to the parks classification a some patients had more than one fistula and are thus counted more than once b one patients had more than one abscesses and is thus counted more than once fig . 
there was no statistical difference in detecting and evaluating abscesses between imaging findings and surgery eua ; moreover , all abscess was easily detected both using stir and post - contrastographic t1 - weighted sequences . 
anorectal complications develop in 36 % of all patients with cd , particularly in the 25 % with only small bowel involvement , in 67 % of patients with colonic cd and in almost all patients with rectal involvement [ 9 ]  . 
in 3681 % of cases , the development of anorectal disease may precede or occur simultaneously with ileo - cecal manifestation and it can be rarely identified as the only clinical manifestation of the disease [ 7 ]  . the presence of perianal disease , especially at the time of diagnosis , is a negative prognostic factor with greater risk of progression to surgery [ 14 ]  . 
actually , mri has an increasingly important role in the evaluation of disease activity in cd and of complicated cd and is actually considered the gold standard and recommended during the initial diagnosis of perianal cd according to the ecco guidelines ; moreover , compared to endoanal ultrasound it is comparable for the evaluation of perianal fistulas and proved to be superior for discriminating between simple and complex disease compared to clinical assessment and anal endosonography [ 10 , 3035 ]  . mri allows an accurate analysis of the fistulas with a correct view of their course , their full extension , and especially the relationship between them , the anal sphincter complex and the surrounding pelvic structures . 
in particular , the mri on the axial and coronal planes allows the identification of the connection between the fistula and the sphincter apparatus , the levator ani muscle and the ischiorectal fossa ; images on the sagittal plane are useful in the evaluation of rectovesical and rectovaginal fistulas , and in the evaluation of the presacral disease [ 11 , 13 ]  . according to the literature , in our mri examinations we used an eight - channel surface [ 3638 ]  . the most used sequence in different studies is the t2 - weighted fse , but in others studies t1 - weighted fse sequences before and after intravenous administration of contrast medium are used [ 1518 , 36 , 39 , 40 ]  . the techniques with suppression of the fat signal are applied to both t1 - weighted and t2 - weighted sequences [ 41 ]  . in a recent study , singh et al . 
 [ 16 ] stated that the contrast study can be omitted , particularly while evaluating primary / previously unoperated perianal fistulae because the results of imaging findings on t2 - weighted and postcontrast t1 - weighted fat saturated sequences were statistically similar . 
in our study , we focused on the role of stir sequences in patients with cd in the diagnosis of perianal fistulas and in the evaluation of the extension of the inflammatory process in the perianal and perirectal areas , by comparing stir and t1 - images . stir sequences are usually used in the study of anatomical regions where there is a substantial fat content and are an important application of the inversion recovery sequences [ 42 ]  . the visualization of the fistulas is related to the degree of inflammation and consequently to their content . 
 in the active phases of the disease , the fistula shows both walls containing granulation tissue and fluid or mucin in its lumen ; furthermore , it presents itself as a stria or as a band of tissue with high signal intensity , well contrasted compared to muscles and surrounding fat [ 45 ]  . 
on t1 - weighted images , acquired with fat suppression and after the use of paramagnetic contrast agents ( gadolinium and its chelates ) , the walls of fistulascontaining granulation tissueas well as the areas of active inflammation , show intense postcontrastographic enhancement [ 21 , 38 , 45 ]  . the fistulas in the active phase are often surrounded by hypointense fibrous walls , which can be relatively thin , particularly in patients with recurrent disease , or with a recent surgical operation ; however , in case of edema , the walls 1 3 radiol med ( 2016 ) 121 : 243251 248 fig . 
2 axial stir ( a ) and t1 - weighted post - contrast ( b ) images show that a fistula ( arrow ) originates from the left postero - lateral wall of the anal canal ( type c according to parks classification )  . 
the same sequences acquired on the coronal plane ( c and d ) allow a better assessment of the fistula ( arrowhead ) and its relationship with the ischio - rectal fossa fig . 
3 axial stir images ( a ) and post - contrast t1 - weighted ( b ) images show the presence of two transphincteric fistulas ( type c of parks ) with contiguous little inflammatory component ( arrows )  . 
there is a perfect agreement between the findings on the stir and post - contrast t1 - weighted images may appear hyperintense and this hyperintensity can spread into the adjacent parenchyma . relationships with the levator ani muscle and the extensions above it . the external anal sphincter is moderately hypointense and its wall contrasts with the fat of the ischio - anal fossa , both in stir and fat - sat sequences . 
the findings reported with stir technique are similar to those disclosed using post - contrastographic t1 - weighted images . indeed , the number of the fistulas and their densitometric and morphological characteristics identified in the 31 patients enrolled in our study using stir sequences were confirmed by t1 - weighted images acquired after administration of contrast medium . we also compared mri and surgical visit findings , showing a sensitivity of the method of 92 % . 1 3 radiol med ( 2016 ) 121 : 243251 complications . 
therefore , stir sequences represent a valid alternative to the se t1 - weighted fat - sat sequences acquired after the injection of contrast medium , allowing the identification of the primary fistula , of any secondary ramifications , of abscesses , of the involvement of the anal sphincter , the levator ani and of the ischium - anal and ischium - rectal fissures . the advantage of using the stir sequences lies in the possibility of obtaining the same diagnostic content of t1 - weighted images acquired after infusion of gadolinium , but without the use of the latter , thus avoiding the possible adverse drug reaction and renal function impairment related to its use . 
for this type of study , formal consent is not required . informed consent all patients enrolled were asked to sign an informed consent in accordance with the dispositions from the italian law 675 / 96 , and every patient also had to read an informative report about the tutelage of the personal data , according to the same law . 
all the patients were asked to sign an informed consent to use the images of their radiological exams for research , according to the law . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . 
iodine and water content were determined in patient ct scans and ex vivo tissue specimen scans by reconstruction of raw ct data at 65 kev ( optimal contrast )  . 
intranodular hemorrhage exhibited elevated water concentrations ( ~1100 mg / ml ) , suggesting a practical threshold of 1075 mg / ml for differentiating intra - plaque hemorrhage and solid nodular regions . 
spectral ct provided diagnostic information in 14 thyroid adenomas and four goiters ( histologically confirmed in donor specimens ) , and eight thyroid adenomas and four nodular goiters based on clinical diagnosis . 
diagnostically useful regional characteristic of intranodular hemorrhage in the thyroid was visualized via spectral ct employing material decomposition , potentially yielding additional molecular data about complex lesion characteristics no apparent in conventional imaging or laboratory methods . keywords intranodular hemorrhage thyroid nodule duel - energy computed tomography advanced spectral imaging material decomposition introduction differential diagnosis of intranodular hemorrhage in thyroid nodules is important for determining appropriate clinical care , as nodules occur in over half of adult populations , but only a relatively small percentage ( approximately 7 % ) are indicative of malignancy [ 1 , 2 ]  . 
compared to conventional computed tomography ( ct ) , duel - energy ct ( dect ) employing advanced spectral imaging has the ability to discriminate between molecular composition of tissues , with potential clinical utility for revealing information about morphological characteristics of the thyroid and surrounding tissues in patients with intranodular hemorrhage . 1 3 280 radiol med ( 2016 ) 121 : 279290 the diagnostic value of spectral ct data reconstructed from dect acquisition systems has only recently been explored in thyroid disease . 
 [ 3 ] reported that gemstone spectral imaging ( gsi ) could quantitatively detect abnormal iodine content in thyroid disease patients , suggesting that lower iodine concentrations on spectral ct could be a useful biomarker for differentiation of malignant from benign nodules . 
specifically , spectral ct can also be used to indicate localized bleeding through detection of iron in free heme released as blood breaks down in tissues adjacent to thyroid lesions , characteristic malignancy [ 3 ]  . 
these recent studies suggest that spectral ct data may be clinically useful in characterizing thyroid nodules , though further work is required to determine the efficacy of these in the non - malignant , low - risk conditions that make up the majority of the clinical patient population . several recent articles have called for limitations on over - zealous diagnosis of thyroid lesions , and corresponding overtreatment of low - risk , benign nodular tumors [ 5 , 6 ]  . 
many patients first present clinically with symptoms of inspiratory stridor or dyspnea , which may be indicative of tracheal compression or deviation related to nontoxic multinodular goiter formation [ 9 ]  . 
other possible diagnoses include benign thyroid lesions , such as thyroid adenomas , cysts , thyroiditis , or detection of initial large nodes very small , clinically unrecognizable multinodular goiters [ 1012 ]  . 
while ct scan and magnetic resonance imaging ( mri ) are not typically warranted as a primary diagnostic method during the initial exam , ct examination can be necessary to detect and characterize goiters located retrosternal , where ultrasound may be unable to clearly visualize the lesion [ 9 ]  . 
spectral ct is particularly useful in cases were conventional diagnostic methods are not able to ascertain a diagnosis with certainty , such as when lesion is partially obscured by the breast bone , that fail to disappear after aspiration , or is recurrent . 
furthermore , unlike ultrasound , iron detection can indicate bleeding , and spectral ct may allow for superior characterization of diverse tissues in and adjacent thyroid lesions , with minimal interference from distortion and motion artifacts common in mri . despite some benefits of conventional ct for differential diagnosis of complex thyroid disease , particularly in differentiation of low - risk , benign tumors and goiters seated behind obscuring anatomical structures , conventional ct is not widely utilized in diagnosis of thyroid disease . 
this is in part due to the prevalence of thyroid radiosensitivity and limited capacity of conventional ct methods to clearly differentiate between hemorrhagic and solid regions of thyroid nodules , as a result of average attenuation effects of polychromatic x - ray sources [ 13 ]  . 
the advent and increasing availability of gsi , an integrated feature of the ge healthcare discovery ct750 hd , has paved the way for new ct applications thyroid condition diagnosis and other clinical areas . 
gsi is a dect technique that can produce information about molecular composition of in vivo tissues using a range of energy ( kev ) levels , potentially useful in clinical diagnosis [ 14 ]  . 
spectral curves of materials are determined by their molecular structures ; therefore , the spectral curves of materials with different molecular structures are distinct . based on observations that hemorrhagic and solid parts of thyroid nodules have variable molecular composition , this study is being conducted to determine if different x - ray photon energy - dependent attenuation coefficients in this ct technique can aid in identification of hemorrhagic and solid regions in complex benign thyroid lesions , which are often difficult to diagnose with certainty by conventional methods . materials and methods general study design and patient data selection a retrospective study was conducted of 30 patients presenting with intranodular hemorrhage of the thyroid from march 2010 to august 2013 at huadong hospital , fudan university ( china )  . 
this study was approved by the ethics committee of fudan university , and waiver was granted for informed consent due to the retrospective nature of the study . patients included ( 1 ) were diagnosed with intranodular hemorrhage , according to endocrine society guidelines [ 15 ] ; ( 2 ) were adolescents or adults aged 15 or older ; ( 3 ) were symptomatic at the time of dect scanning ; and ( 4 ) had dect scans revealing recent , rather than old , bleeding patterns at the thyroid . 
patients excluded ( 1 ) had prior history of tracheotomy or other significant surgery to the trachea or immediately adjacent airways ; ( 2 ) did not have dect scans as part of their clinical care ; ( 3 ) exhibited near complete tracheal obstruction or compression ( as in the case of advanced goiters ) , malignancy , horners syndrome , or phrenic nerve paralysis ; or ( 4 ) did not receive a final clinical diagnosis or were lost to follow - up prior to completion of diagnostic procedures . 
if present , clinical , demographic , and histological data ( if biopsy or surgery was performed ) were collected for each included patient 1 3 radiol med ( 2016 ) 121 : 279290 record . 
ct value attenuation curve ( spectral hu curve ) generated by an x - ray beam passing through the material was used to reflect the attenuation characteristics of that material , and material attenuation can be expressed as mean ct values at different mono - energies ( kev )  . patients and biopsied thyroid specimens were scanned on a dect scanner ( discovery ct750 hd , ge healthcare , milwaukee , wi , usa ) in spectral imaging scan mode with fast tube voltage switching between 80 and 140 kvp [ 16 , 17 ] from view to view . 
dect imaging was conducted with the following parameters : 630 ma , helical scan with pitch of 0.984 : 1 , rotation time of 0.5 s , collimation thickness of 0.625 mm 64 , and reconstruction field of view ( fov ) of 25 cm ( patients ) or 10 cm ( thyroid specimens )  . 
the integrated gsi viewer was used to analyze images for optimal contrast , and a single energy ( 65 kev ) was selected for subsequent qualitative and quantitative analyses . image analysis two radiologists with more than 15 years experience blinded to diagnosis and patient management reviewed each image set . 
regions of interest ( rois ) were selected based on ct features of the thyroid gland based on degree and pattern of parenchymal attenuation , glandular size and margin , degree and pattern of parenchymal enhancement in thyroid lobes ( hu , hounsfield unit ) , and glandular attenuation and enhancement were used as basis for roi determination [ 18 ]  . 
perroi values were recorded for iodine and water concentrations based on reconstructed spectral data ( material decomposition ) , as follows ( cid : 31 ) hu = hu40 kev hu100 kev ( cid : 31 ) ( cid : 30 ) where hu represents the slope of hu curves ( representing the plot of material attenuation against x - ray photon energy ) at energy values of 40 kev ( hu40kev ) and 60 kev ( hu60kev )  . 
for each roi , zeff and mean ct values from the images were also recorded at 65 kev . histological examination histopathological classification for diagnostic and patient management purposes was carried out according to the standard of care at the site . 
thyroid function was verified by laboratory findings , including total triiodothyronine ( t3 ) or free t3 to rule out t3 toxicosis , total thyroxine tt4 to rule out thyroid - binding globulin abnormality , ft3 and ft4 to rule out hyperthyroidism , thyroid - stimulating hormone ( tsh ) to check normal thyroid activity , and neuron - specific enolase ( nse ) levels . 
all thyroid nodule specimens were fixed in 10 % buffered formalin , embedded in paraffin wax , and stained with hematoxylin and eosin ( he ) for histological examination prior to being reviewed for pathology . statistical analysis standard deviacontinuous data were expressed as mean tion ( sd ) and categorical data were expressed as counts and percentages . 
 1 3 282 radiol med ( 2016 ) 121 : 279290 the majority of those found to be ineligible were due to presence of old bleeding at the thyroid site , as observed in clinical ct scans . 
of included intranodular hemorrhage subjects , 12 patients did not undergo surgery within the study window ( 7 males aged mean 42.3 , 3363 years ; 5 females aged 43.5 , 2857 years ) and biopsied thyroid specimens were able to be attained from 18 patients ( 12 males , aged 42.3 , 1867 years ; six females , aged 43.5 , 1767 ) for use in study analyses . clinical diagnosis and histopathological results intranodular hemorrhages were identified by histological analysis and laboratory testing of excised tissues following surgery for intranodular hemorrhage of the thyroid . 
spectral ct provided diagnostic quality information sufficient for clinical differential diagnosis in all 14 thyroid adenomas and four goiters ( confirmed by study donor specimen histology ) , and eight thyroid adenomas and four nodular goiters based on clinical diagnosis ( from medical records )  . 
laboratory testing did not reveal any previously unknown underlying pathology in any cases . spectral ct measurements of intranodular hemorrhage intranodular hemorrhages were detectable on spectral ct as regions apparent negative iodine concentrations and high water concentrations , low zeff , and negative hu values . 
representative images are shown , comparing quantitative spectral data acquired from human patient ct scans conducted in vivo and ex vivo scanning of donor thyroid tissue specimens ( table 1 )  . 
a 65 kev ; b iodine density ; c water density ; d zeff indicating intranodular hemorrhage ( l3 ) ct value , iodine , and water concentration and zeff , in comparison with cystic change ( l2 ) and solid component ( l4 ) with all thyroid nodules exhibiting significantly different iodine concentration , water concentration , hu , and zeff as compared to surrounding background tissue ( p < 0.001 , table 2 )  . intranodular hemorrhage demonstrated consistently higher water concentrations in all samples ( approximately 1100 mg / ml ) , suggesting that a threshold of 1075 mg / ml for water concentration on spectral ct could be practically applied to differentiate intra - plaque hemorrhage and solid regions of thyroid nodules with excellent sensitivity and specificity . 
conversely , no significant differences in mean ct values were observed for in vivo or ex vivo samples between intranodular hemorrhage and thyroid nodules ( p > 0.05 , table 2 )  . 
in ex vivo tissue specimens , it was also noted that mean ct values of the intranodular hemorrhage and surrounding tissues were reduced significantly compared to those observed in the in vivo samples ( p > 0.05 , table 2 ) , with intranodular hemorrhage and surrounding tissues in the in vivo patient scans exhibiting more significant distinction between regions ( p 0.031 , table 2 )  . discussion the current study demonstrated good overall utility of spectral ct for differential diagnosis of benign thyroid lesions in patients with recent bleeding from intranodular hemorrhage based on gis material decomposition data . 
 across in vivo and ex vivo images , spectral ct facilitated clear discrimination of intranodular hemorrhage from surrounding ( background ) tissues , providing valuable information on iodine concentration , water concentration , hu , and zeff as compared to surrounding background tissues . 
intranodular hemorrhage ( cyan ) manifested as low hu , high ct value , low iodine , and high water concentration set for differentiation , which may have clinical implications for facilitating differentiation between intranodular hemorrhage and the solid regions of thyroid nodules . ability to non - invasively differentiate between low - risk benign lesions and malignancies of the thyroid in complex cases . differential diagnosis in intranodular hemorrhaging can be complicated phagocytosis of red blood cell hemoglobin by macrophages , resulting in abnormal iron levels in localized tissues imperceptible by conventional diagnostic imaging , but detectable by spectral ct [ 19 ]  . 
dual - source x - ray material discrimination has previously been shown to be a superior detector of iron , water , and iodine concentrations in biological tissues , noting that 100 / 140 kv acquisitions in large patient sizes could require additional filtration to minimize noise and increase contrast in low - energy images [ 20 ]  . 
 [ 3 ] reported on 87 benign thyroid lesions examined with spectral ct , indicating that benign nodules exhibited higher iodine concentration and normalized ic ( nic ) in both the noncontract and venous phase , indicating that spectral ct is generally useful for evaluation of abnormal iodine content in patients with thyroid disease . 
wide adoption of spectral ct methods may increase it can be difficult to differentiate between intranodular hemorrhage and the solid parts of thyroid nodules in conventional ct images due to the similar ct values of these tissues using routine 120 - kvp tube voltage . 
as the average energy for the 120 - kvp x - ray spectrum is around 65 kev for imaging the thyroid gland , it would be difficult to differentiate between intranodular hemorrhage and the solid parts of thyroid nodules by observing 120 - kvp images in isolation . 
 [ 21 ] demonstrated that the 1.77 kev in monomean optimal kev was obtained at 55 chromatic spectral ct images , and that such images could be useful in improving overall image quality of laryngeal and hypopharyngeal malignancy discrimination and 1 3 radiol med ( 2016 ) 121 : 279290 fig . 
furthermore , quantitative ratios of hu may be helpful for differentiating between metastatic and non - metastatic cervical lymph nodes , as demonstrated by the findings of li et al . 
conversely , spectral curves obtained via spectral ct revealed the dependence of the attenuation on photon energy , which implied that spectral curves of different tissues can be analyzed to differentiate between different tissues types quantitatively . 
using existing knowledge of the x - ray attenuation curves now defined for the overwhelming majority of elements and small molecules in the body , in vivo concentrations are detectable , particularly considering the 0 value of the spectral curve of water ( graphically a horizontal line )  . the findings of the present study are part of a small and growing body of literature that support spectral ct as a diagnostic method capable of revealing distinct molecular information not readily available by conventional imaging or laboratory diagnoses [ 3 , 4 , 16 , 17 , 20 , 22 ]  . 
as evidenced in this study , the majority of patients with low - risk , benign hemorrhagic thyroid lesions do not evidence abnormal 1 3 286 radiol med ( 2016 ) 121 : 279290 fig . 
 a 65 kev ; b iodine density ; c water density ; d 65 kev : zeff indicating intranodular hemorrhage and surrounding thyroid tissue ( l2 ) , b iodine and c water concentrations and d low zeff laboratory values ( e.g. , t3 , tt4 , and ths )  . 
similarly , in certain malignancies , including thyroid tumors with a follicular growth pattern ( such as benign , hyperplastic nodules as well as follicular adenomas , and carcinomas ) , diagnosis can be subjective and difficult to diagnosis via routine imaging or histological interpretation [ 23 ]  . 
these complex lesions could , however , be expected to evidence distinct molecular characteristics of intranodular hemorrhage detectable by spectral ct , characterized by a relatively high ct value , but effective atomic number lower than water . 
this high water concentration can be observed as negative iodine density value in the material decomposition pairs , balancing the true attenuation of the x - ray spectrum caused by intra - plaque hemorrhage . 
a histogram of iodine concentration ; b histogram of water concentration ; c zeff65 - kev ct value scatter plot ( cd cystic degeneration ; bg background ; hemo hemorrhage )  . 
d histogram of 65 - kev ct values cumulatively , these characteristics could potentially be useful in differentiation of intra - plaque hemorrhages from the solid regions in thyroid nodules . in some cases , conventional non - contrast ct images are not capable of visualizing small thyroid nodules or initial enlargement of nodules goiters [ 21 ]  . 
this limitation is further complicated by contraindication of iodinated contrast material utilized for ct scans in patients with possible thyroid disease , because scintigraphy or administration of radioactive iodine ( rai ) therapy is not suggested for a period of 12 months after such administrations . 
 thus , spectral ct imaging cannot only define intranodular hemorrhage , but also help detect very early stage thyroid nodules , which are virtually imperceptible using ultrasound and other conventional diagnostic imaging tests . 
furthermore , previous reports have indicated that nodular goiters and adenomas of the thyroid have a tendency toward cystic degeneration and intranodular hemorrhage , whereas more than 90 % of thyroid carcinomas lack cystic changes or intranodular hemorrhage [ 24 , 25 ]  . 
therefore , highly accurate detection of intranodular hemorrhage could assist in the differential diagnosis of thyroid nodules . notably , all nodules in this study were benign , and many were of small size , demonstrating the power of spectral ct to accurately differentiate between very small lesions , a benefit over other imaging modalities . 
these conclusions are , however , limited by the preliminary nature of this study and should be further validated in larger , multicenter studies the directly compare malignant and benign thyroid nodules , as well as comparing diagnostic accuracy 1 3 288 radiol med ( 2016 ) 121 : 279290 fig . 
although this study highlights the distinctive imaging characteristics of intranodular hemorrhage , it is not intended to comprehensively demonstrate the molecular character of varied lesions , which can be explored in greater detail in future studies . 
 detailed analysis of the chemical composition of intranodular hemorrhage in thyroid nodules may aid in the development of spectral ct - based diagnostic criteria , which can enable differential diagnosis in complex and challenging thyroid conditions . conclusions results of the current study indicated that reconstructed spectral ct data can be successfully used to distinguish molecular characteristic of recently bleeding intranodular hemorrhages by anatomical region , exhibiting low effective atomic number and high ct values . 
diagnostic performance , complication rate , and patient radiation exposure were investigated . results the technical success rate of tnb under iguide cbct virtual navigation system was 99 % ( 99 / 100 )  . 
although tnb can be performed with fluoroscopic or ultrasonographic guidance , ct and ct fluoroscopy - guided tnb have been widely performed in the diagnosis of pulmonary nodules [ 3 ]  . 
however , conventional ct guidance has limitations in the lack of real - time monitoring and gantry tilting for a more accessible needle pathway to the target lesion [ 46 ]  . 
to overcome the disadvantages of conventional ct guidance , ct fluoroscopy has been introduced , and this modality enables real - time monitoring of target lesions and gantry tilting [ 7 ]  . 
nevertheless , limitations include the small gantry bore , radiation exposure to operators , and limited imaging plane orientation [ 8 , 9 ]  . along with the development of cbct , a novel technique for tnb guidance recently emerged . 
the cbct systems offer real - time visualization of tnb procedures and more flexibility in the orientation of the detector system around the patient compared to traditional ct systems [ 11 , 12 ]  . 
therefore , the tnb procedures assisted by advanced 3d needle guidance systems can be performed in a sterile workspace with flexible system angulation capability as well as instantaneous fluoroscopic feedbacks [ 13 ]  . 
 this technique offers high spatial resolution of less than 1 mm , as well as contrast resolution of 10 hu , which is adequate for lung imaging as lung inherently has a high contrast ( soft tissue against air )  . 
in august 2009 , artis zeego , the multi - axis system based on robotic technology from siemens was introduced into our department , where was the first installation unit in china . 
this paper describes our preliminary experience with tnb for small ( 2.0 cm ) pulmonary nodules biopsy under iguide cbct guidance system . materials and methods patients this retrospective study was approved by the institutional review board of the first affiliated hospital of zhengzhou university , and additional informed consent was obtained from all individual participants for whom identifying information is included in this article . 
the lesion size was recorded as the maximum diameter in the image data by one chest radiologist ( han xw , 30 years of experience in image guided tnb )  . image acquisition as the first step , 3d cbct images of the patients were acquired with a rotational angiographic system ( artis zeego , 30 40 cm fd detector , siemens healthcare , forchheim germany )  . 
as an output , a total number of 397 projection images were generated with an x - ray dose of 0.36 gy / frame , projection increment 0.5 , 1 - k matrix , zoom factor 0 , and field of view 480 mwith the detector used , the imaged volume covered had a cylindrical shape with a height of 185 mm , a diameter of 225 mm , and a voxel size of 0.4 mthe patients stopped breathing for the entire 8 s 3d cbct image acquisition . the resulting raw projection images were then automatically transferred to a workstation ( syngo x workplace , siemens healthcare ) for 3d volume reconstruction . 
the time from the end of the data acquisition to the presentation of multiplanar images on the workstation ranged between 43 and 45 s . needle path planning and guidance procedure as the second step , the needle path was planned on the same workstation using commercially available software ( syngo iguide , siemens healthcare )  . 
3 the laser navigation system on the flat - panel can quickly locate the needle point on skin , thus the skin entry point could be determined ( a )  . 
the needle was advanced along the planned needle path ( dotted line ) from skin entry site ( white cross ) to target lesion site ( white circle )  . 
4 cbct scan confirmed the needle position in multiplanar ( ac ) and volume rendering ( d ) images demonstrated this procedure for a 0.5 - cm in diameter pulmonary lesion , and figs . 
the needle orientation was adjusted until both the tip and hub of the needle in the fluoroscopic image were superimposed and located at the centre of the circle and the cross . 
these two angles provided lateral views ( progression view ) of the planned needle path and helped to ensure that the needle was advanced along it 1 3 272 radiol med ( 2016 ) 121 : 268278 fig . 
a 16 - gauge needle ( quick - core , cook medical inc . , bloomington , in , usa ) was advanced along the planed path under real - time fluoroscopy . 
after sufficient tissue samples were obtained , the coaxial introducer was removed with a position change by placing the patient biopsy side down to reduce the complication rate of pneumothorax [ 14 ]  . 
in case serious symptoms in vital signs or clinical status occurred , repeated imaging and if necessary treatment was performed . 1 3 radiol med ( 2016 ) 121 : 268278 fig . 
the needle position relative to the anatomical structures was displayed in 3d using volume rendering technique ( d ) postbiopsy evaluation after obtaining sufficient tissue , the coaxial introducer was removed . 
post - biopsy complications were investigated with post - procedural cbct . procedural records we recorded several factors during tnb : the patients positions during ptnb , the number of pleural passages , the number of biopsies , the number of ct acquisitions , and total procedure time ( defined as the duration from local anaesthesia injection to the end of post - procedure cbct )  . 
the needle was advanced along the planned needle path ( dotted line ) from skin entry site ( white cross ) to target lesion site ( white circle ) 1 3 274 radiol med ( 2016 ) 121 : 268278 fig . 
final diagnosis was confirmed in four ways : ( 1 ) if the patient underwent surgical resection , the pathological report decided the final diagnosis ; ( 2 ) if the pathological result of biopsy demonstrated a malignant or a specific benign pathology such as hamartoma or tuberculosis , it was accepted as the final diagnosis ; ( 3 ) in the cases of nonspecific benign pathology ( negative for malignancy , chronic inflammation , etc . ) , follow - up ct helped to decide whether the lesion would be truly or falsely benign , or indeterminate . 
 ( 4 ) if a nodule of nonspecific benign pathology did not show sufficient interval decrease in size nor had follow - up images , its final diagnosis was defined as indeterminate . 
 pneumothorax was evaluated with post - procedural cbct and follow - up chest radiographs during the hospitalization . all data analyses were performed using excel 2010 ( microsoft , redmond , wa ) and spss software ( version 13.0 ; spss , chicago )  . 
 the 76 malignant lesions consisted of lung adenocarcinomas ( n 15 ) , small cell lung cancers ( n 2 ) , mesothelioma of pleura ( n 1 )  . 
one patients initial biopsy results were squamous cell carcinoma ( nodule size 1.0 cm ) , but was later confirmed as an adenosquamous carcinoma by post - operative pathological outcome . 
tnb procedures were performed again and the both patients were confirmed with lung adenocarcinoma . finally , the sensitivity , specificity and accuracy of tnb of very small nodules under the siemens artis zeego iguide cbct virtual navigation guidance were 98.7 % ( 77 / 78 ) , 90.5 % ( 19 / 21 ) and 97.0 % ( 96 / 99 ) , respectively . 
of patient the technical success 99 ( 99 ) rate ( % ) specificity ( % ) accuracy ( % ) 19 ( 90.5 ) 95 ( 96 ) pneumothorax rate ( % ) 10 ( 10 ) hemoptysis rate ( % ) 12 ( 12 ) malignant benign lung adenocarcinoma 48 ( 61.5 ) lung inflammation 7 ( 43.8 ) squamous cell carci15 ( 19.2 ) pulmonary tuberculosis 5 ( 32.2 ) noma small cell lung cancer 10 ( 12.8 ) hamartoma mesothelioma of pleura 2 ( 2.6 ) carcinoid 2 ( 12.5 ) 2 ( 12.5 ) metastases pulmonary blastoma 2 ( 2.6 ) 1 ( 1.3 ) developed post - operative pneumothorax with volume about 30 % and hence underwent chest tube drainage . 
post - operative hemoptysis occurred in 12 patients , but the symptom was selflimiting and disappeared within 3 days . discussion with the increasing utilisation of chest ct in clinical practice as well as in lung cancer screenings , early lung cancers manifesting as small nodules have been detected more frequently than ever before . 
so , the need for accurate diagnosis of these small lung nodules with a high suspicion of malignancy is evident [ 16 , 17 ]  . initial experiences suggested that cbct - guided tnb could be a useful , safe and accurate procedure for diagnosis of indeterminate lung nodules , with possible advantages over fluoro - ct - guided biopsy [ 10 , 18 ]  . 
it is well known that limited access due to a closed ct gantry increases the difficulty of tnb and increases radiation exposure for the operator , whereas the greater working space provided by the c - arm cone - beam system facilitates needle placement [ 10 , 19 ]  . 
in consideration of the previously mentioned diagnostic performance and technical failure rate of tnbs , we believe that cbct - guided tnb is a highly accurate diagnostic method for use with pulmonary lesions [ 4 , 21 ]  . 
 [ 23 ] reported that lesion size and safety of the method showed no significant differences between two groups of patients divided by lesion size ( 3 and > 3 cm )  . 
 we believe that the advantages of cone - beam ct guidance , such as real - time imaging guidance and great flexibility in entry site selection , can contribute to high diagnostic accuracy in small lesions . 
the bulls eye view provided by the real - time fluoroscopy capability of the cbct virtual navigation system aligns the detector , the skin entry site and the target , contributing to a more accurate and safer biopsy . 
we believe that this low incidence of pneumothorax was possible as the virtual navigation system enabled us to select a safer and more accurate targeting route in navigating the needle approach to the target . 
of the ten patients who had pneumothorax , five patients ( 50 % ) had pulmonary emphysema along the needle pathway , and this may suggest that considering emphysema in the needle pathway would be more likely to lead to the occurrence of pneumothorax . 
we think that the relatively loose compactness of these nodules may have negatively affected the natural compression of injured tissue after biopsy and that patent airways and blood vessels within the lesion could also increase the risk of haemoptysis after cutting needle biopsy . there were three cases ( 3.0 % ) misdiagnosed in the study . 
one patients initial biopsy results were squamous cell carcinoma ( nodule size 1.0 cm ) , but was later confirmed as an adenosquamous carcinoma by post - operative pathological outcome . 
the lesion may be malignant , but the sample obtained may lie outside the nodule borders or come from a necrotic area , thus preventing pathologists from establishing a correct diagnosis . 
if further growth occurs after a non - specific benign diagnosis is obtained with tnb , repeat biopsy or resection is indicated [ 26 ]  . in terms of radiation dose , a mean exposure dose was 3.1. 
on the basis of our results and the data from the literature regarding lung biopsies performed with cbct guidance , despite the limited amount of currently available data and the lack of homogeneity , a slight reduction in dose could be hypothesised with the use of iguide guidance . 
radiation dose in our study is similar to that of standard chest ct ( 7 msv ) [ 28 ] , the radiation dose of cone - beam ct guided 1 3 radiol med ( 2016 ) 121 : 268278 biopsy may not be a substantial problem , although a continuous effort must be made to reduce the radiation dose through use of a small field of view or collimation . the limitations of this technique should be also mentioned . 
as patient movements may result in motion artr , facts and affect the registration accuracy of the projected path , the key factor for achieving successful needle guidance is to generate high - quality 3d cbct images . 
the ct findings were evaluated for the morphologic appearance of ascites , peritoneum , mesenterium and omentum involvement , enlarged lymph nodes , solid abdominal viscera infiltration and metastases , and thoracic changes . 
there were significant differences in the following aspects between the two groups : ( 1 ) smooth peritoneal thickening was more frequent in patients with tbp , while irregular thickening was more frequently observed in patients with mpm ; ( 2 ) caked omentum stratification was more common in patients with mpm ; ( 3 ) mesentery involvement was less commonly observed in patients with tbp ; ( 4 ) abdominal viscera infiltration and pleural plaques were more common in patients with mpm ( 46 / 53 and 48 / 53 , respectively ) than in those with tbp ( 0 / 27 and 0 / 27 ) ; and ( 5 ) more patients in the tbp group ( 14 / 27 ) * guo - qi zheng czzxyyxhk@126.com 1 department of gastroenterology , cangzhou central hospital , cangzhou 061001 , hebei , china 2 department of magnetic resonance imaging , cangzhou central hospital , cangzhou 061001 , hebei , china displayed pleural effusion , and extraperitoneal tuberculosis was more common in patients with tbp ( 20 / 27 )  . conclusion although most ct findings analyzed are observed in both diseases , each disease has its own several unique characteristics . 
therefore , using a combination of ct findings may increase our ability to distinguish tbp from mpm . keywords malignant peritoneal mesothelioma tuberculous peritonitis computed tomography differentiation introduction malignant peritoneal mesothelioma ( mpm ) is a rare tumor with rapid progression and poor prognosis and is commonly caused by exposure to asbestos [ 1 ]  . 
mpm incidence is expected to increase globally over the next 520 years , likely because of the extensive use of asbestos in building and industrial materials in the past [ 2 ]  . 
the most common presenting signs and symptoms of mpm are serous ascites ( 70 % ) , increased abdominal girth ( 55 % ) , pain ( 45 % ) , and an abdominal or pelvic mass ( 26 % ) [ 3 ]  . 
there are several diseases with symptoms similar to mpm ; thus , mpm must be distinguished from diseases , such as tuberculous peritonitis ( tbp ) , peritoneal carcinomatosis , and ovarian cancer . tbp is a chronic , diffuse inflammation of the peritoneum that is uncommon in clinical practice , because the incidence accounts for approximately 4 % of all tb diagnoses [ 4 ]  . 
the disease is caused by infection with mycobacterium tuberculosis ( mtb ) and remains the single most 1 3 254 radiol med ( 2016 ) 121 : 253260 important fatal infection in humans . 
in patients with tbp , the most common presenting symptoms are fever ( 81 % ) , abdominal pain ( 89 % ) , and cloudy fluid ( 77 % ) [ 5 ]  . both mpm and tbp are rare diseases , and their clinical manifestations and imaging findings are similar . 
ct can be used to facilitate peritoneal disease diagnosis , to assess the severity of peritoneal disease , and to provide an objective index for treatment [ 8 ]  . 
the purpose of the present study was to determine useful ct findings to differentiate between tbp and mpm . materials and methods subjects between january 2010 and october 2012 , 27 patients with pathologically confirmed tbp and 53 patients with pathologically confirmed mpm were retrospectively reviewed . 
mpm diagnosis in the series was made in accordance with the guidelines for pathologic diagnosis of malignant mesothelioma ( mm ) in 2012 from the international mesothelioma interest group [ 12 ]  . 
the case histories were compared and analyzed according to gender , age , clinical presentation ( abdominal distention , abdominal pain , fever , weight loss , history of asbestos exposure , etc . ) , and ct findings . ct technique diagnostic ct was performed with multislice ct scanners ( lightspeed vct , ge , usa )  . 
imaging of the chest , abdomen , and pelvis was performed with the following parameters : 120 kv , 150300 ma , gantry rotation time of 0.5 s , collimator width of 0.625 mm 64 , and section thickness of 5 mthe images were obtained after administration of 75100 ml of iodinated intravenous contrast at 3 ml / s using an automated injector ( optivantage , liebel - flarsheim company , usa )  . image analysis in this retrospective study , all ct images were reviewed by three fellowship - trained radiologists with 6 , 7 , and 12 years of experience . 
if the reviewers could not reach a unanimous verdict , then a simple majority was used . observation indexes of ct images ( 1 ) changes in peritoneum , omentum , and mesentery . 
omental involvement was classified as nodular , smudged ( infiltration with ill - defined soft tissue density ) , and cake - like ( soft - tissue replacement ) appearances . 
small bowel mesentery involvement was classified as nodular , thickened soft tissue strands with crowded vascular bundles or diffuse infiltration with soft - tissue density masses . ( 2 ) the volume and density of ascites . 
ascites was categorized as extensive when it was present throughout the abdomen and pelvis , moderate when localized around the liver and spleen , and slight when only traces of fluid were present . 
ascites was defined as high - density ascites ( > 20 hu ) or low - density ascites . ( 3 ) abdominal viscera invasion or metastasis . ( 4 ) regional lymph - node enlargement . 
lymph nodes were considered enlarged if the short axis diameter was more than 1 cm in the retroperitoneal and mesenteric stations and more than 0.5 cm in the mediastinal , hilar , and cardiophrenic nodal station regions [ 14 ]  . ( 5 ) chest changes ( including asbestosis , pleural plaque , pleural effusion , tuberculosis , and pleura calcification ) were examined . statistical methods the results were analyzed using spss 13.0. 
there were twelve patients with tuberculosis , two patients with renal tuberculosis , one patient with bone tuberculosis , two patients with pelvic tuberculosis , and three patients with intestinal tuberculosis . discussion radiol med ( 2016 ) 121 : 253260 sanitation was poor [ 19 ]  . 
the most common initial symptoms are abdominal distention and papatients often develop cachexia and ascites . clinical characteristics of the patients mpm and tbp histologic features mesothelioma can arise from any coelomic epithelium covered by mesothelial cells . 
in cangzhou , hebei province , china , 93.5 % of patients with mpm have a history of asbestos exposure , and mpm incidence in women is higher than in men . 
in addition , in patients with mpm , the tumor can have a single or multicenter origin and may infiltrate around the structures of the peritoneu general pathology reveals ashen , hard pearl nodules of different sizes distributed widely in the peritoneunodule diameter can range from a few millimeters to several centimeters , and nodules can merge into a larger mass . 
the use of immunohistochemistry helps to distinguish mpm from other peritoneal cancers ( colorectal adenocarcinoma and ovarian carcinoma , among others ) [ 22 ]  . 1 3 radiol med ( 2016 ) 121 : 253260 the tbp infective pathway occurs by direct infection or hematogenous spread . 
in our study , 26 patients had wet - type tbp , while one patient had dry type which is associated with higher standards of living and early treatment . patient ct characteristics ct images revealed the general mpm and tbp pathological structures . 
the other form manifests with a large tumor mass that is usually in the upper abdomen , and there may be discrete nodules scattered throughout the peritoneum [ 24 ]  . 
in our study , 46 ( 86.8 % ) patients with mpm and 23 ( 85.2 % ) patients with tbp displayed thickening of the parietal peritoneuna - chiang mai et al . 
the mesenteric abnormalities of tbp consist of mesenteric thickening resulting from edema , 1 3 258 radiol med ( 2016 ) 121 : 253260 30100 % of patients with tbp [ 29 ]  . 
 reported that pleural plaques were encountered in approximately 50 % of patients with mpm [ 32 ]  . the major growth pattern of mpm was local infiltration , and there was no tumor metastasis . 
the ct image displays mediastinal lymph - node calcification ( short arrow ) , pleural calcification ( long arrow ) , and tuberculosis ( blue arrow ) 1 3 radiol med ( 2016 ) 121 : 253260 fig . 
there were more patients with pleural effusion in the tbp group ( 14 / 27 )  . the lymph - node enlargement rate was 35.8 % in the mpm group with 89.5 % distributed in the right heart diaphragm angle . 
lymph - node enlargement did not significantly differ between the groups . some cases of mpm and tbp can be characterized by low - density masses surrounded by thick solid rims . 
the primary ct findings include a nodular appearance of the peritoneum and omentum , retroperitoneal lymph - node enlargement , lymph - node fusion , and definite primary tumor , particularly in the gastrointestinal tract and ovaries . 
canitano2 , 8 received : 10 june 2015 / accepted : 9 november 2015 / published online : 11 december 2015 italian society of medical radiology 2015 abstract objectives many studies show that a large portion of medical prescriptions for diagnostic examinations may be not useful for patients management or unnecessary . 
 the aim of this study was to assess the appropriateness of the knee mri prescriptions . materials and methods a panel of experts found standard clinical practice guidelines in the management of knee disorders . 
secondly , the finalized set of guidelines chosen was compared with the data of 400 patients who underwent previous knee mris , which were then reported in a specific questionnaire prepared by the authors . 
the most frequent prescription indication was for meniscal disorders that account for 26.8 % of the total indications . conclusions our results demonstrate that approximately 40 % of the total prescriptions were totally inappropriate or uncertain and that most of these were made by general practitioners . 
in light of these results , the economic impact of inappropriate prescriptions on the italian healthcare system has to be seriously considered . 1 radiologia e diagnostica per immagini , i.r.c.c.s - istituto dermosifilopatico di santa maria e san gallicano , i.f.o. , via elio chianesi 53 , rome , italy 2 radiologia e diagnostica per immagini , regina elena national cancer institute roma , via elio chianesi 53 , rome , italy 3 ortopedia , regina elena national cancer institute roma , via elio chianesi 53 , rome , italy 4 reumatologia , i.r.c.c.s - istituto dermosifilopatico di santa maria e san gallicano , i.f.o. , via elio chianesi 53 , rome , italy 5 dipartimento di scienze radiologiche , asp di siracusa , c.so gelone 17 , syracusa , italy 6 unit operativa diagnostica per immagini , asp di messina , via la farina 263 / n , messina , italy 7 direzione scientifica , regina elena national cancer institute roma , via elio chianesi 53 , rome , italy 8 viale mazzini 144 , 00195 rome , italy f . 
these disorders are obviously accentuated by the increase in average life expectancy , body weight and other associated risk factors as well as common phenomena in developed countries . the correct management of these patients helps to obtain early diagnosis , may prevent unnecessary invasive procedures and may reduce healthcare service costs [ 3 ]  . 
incidentally , the overuse of healthcare services such as referring magnetic resonance imaging ( mri ) has become an increasingly recognized problem [ 48 ]  . national healthcare systems in various countries have focused their attention on this problem in order to reduce healthcare service costs . 
to do this , guidelines and appropriateness criteria have been elaborated , sometimes causing confusion as far as terminology and purpose are concerned [ 913 ]  . in this regard , the italian national agency for regional health services in 2008 produced a document entitled guidelines for diagnostic imaging following the programs of the major developed countries [ 14 ]  . even though this text is in line with the guidelines proposed by the national healthcare centers in other countries , we believe it should be referred to as a general guideline , and not solely for knee mris , particularly in the case of the musculoskeletal system as it gives only an overview of indications for the major clinical scenarios and sometimes may generate confusion . 
furthermore , these guidelines cannot actually solve the main problem of costs since it is not easy to follow and apply them in clinical practice because many healthcare services lack organization , despite numerous strategies having been suggested to improve its adherence [ 13 , 1517 ]  . the global financial crisis has worsened an already alarming condition of the italian national healthcare system . recently , during an agenzia nazionale stampa associata ( ansa ) forum , the italian minister of health has proposed to create new strategies and widely accepted protocols to limit and avoid the unnecessary and excessive use of performing mri examinations in italy which estimated to be 13 billion euros every year [ 18 ]  . as a result , we decided to evaluate the appropriateness of prescriptions for magnetic resonance imaging ( mri ) of the knee given that they are commonly requested and frequently inappropriate [ 10 ]  . 
to do this , five experts were invited to participate in a panel discussion to allow available evidence - based appropriateness criteria . our panel of experts comprised of five specialists , three radiologists ( fms , fd and ag ) , one rheumatologist ( dg ) and one orthopedist ( sn )  . 
one author ( fms ) was selected as the panel leader . at first , the expert panel started the literature review process by assessing the most related databases and web sites focusing on clinical practice guidelines and evidence reviews . 
from the selected guideline ( see results section ) , indications and a complete listing of scenarios were obtained and shared by the experts after a revision ( table 1 )  . appropriateness of prescription the experts were then invited to a meeting on consensus development . 
the experts were asked to discuss the scoring scale of the previously selected guideline for each scenario based on their professional judgment and a summary of evidence to fully accept thethe scores ranged from one ( absolutely inappropriate ) to nine ( absolutely appropriate )  . after having reached a consensus agreement , the same panel of experts made a retrospective comparison between indications and what the clinical records reported in the questionnaire . 
the meeting was conducted over three different single sessions lasting almost 5 h each . 1 3 318 radiol med ( 2016 ) 121 : 315322 table 1 list of scenarios extrapolated by the experts from the selected guideline ( 10 ) 1 . 
about 38 % of patients declared that their prescriptions were administered without a complete physical examination in addition to biomechanical assessment , while physical examination had only been performed in 62 % of the patients . 
among the different physicians prescriptions and appropriateness , orthopedists prescriptions were the most appropriate ( 57.7 % ) and gps prescriptions were the most inappropriate ( 75 % )  . 
also , gps had a large number of uncertain prescriptions comprising 53.3 % , while the other specialists had about 14.7 % of uncertain prescriptions ( table 3 )  . 
 on the other hand , 57.7 % of the inappropriate prescriptions were of patients who performed an mri as a first examination ( table 4 )  . discussion knee mris represent the majority of mri investigations of the musculoskeletal apparatus performed in italy , corresponding approximately to 65 % of the total amount of mris administered [ 21 ]  . 
the results that most relevantly stand out are that about 40 % of mri prescriptions were inappropriate or uncertain and that the gps prescribe more than one - third of mris of the knee . 
if we consider that more than two - thirds of gp prescriptions were absolutely inappropriate or uncertain on the basis of the criteria we applied , it is highly likely that almost 25 % of these mri investigations may be useless worsening the situation as they very frequently prescribe these examinations as the first examination to perform , without any preliminary inquiries . 
on the other hand , a significantly higher percentage of clinical visits carried out were reported in patients with prescriptions prescribed by orthopedists , resulting in approximately 60 % of those absolutely appropriate . 
note values in the graphics are rounded to the nearest whole number table 3 relationship between physicians and appropriateness of prescriptions ; there was a statistically significant relationship ( p < 0.0001 ) physicians appropriateness appropriate ( n ) not appropriate ( n ) uncertain other specialists 60 ( 24.9 % ) 7 ( 8.3 % ) 42 ( 17.4 % ) 63 ( 75 % ) orthopedists 139 ( 57.7 % ) 14 ( 16.7 % ) gps general practitioners 11 ( 14.7 % ) 40 ( 53.3 % ) 24 ( 32 % ) and thus tend to request and turn to costly investigations instead of drawing a clinical evaluation . 
another reason behind the gps management of these patients is the long waiting times to obtain an orthopedist consultation in our national healthcare systein fact often an mri investigation is requested before the actual visit so that the patient does not have to book further visits . substantially , the financial burden of the inappropriate examinations prescribed by gps to the national healthcare 1 3 radiol med ( 2016 ) 121 : 315322 table 4 relationship between mri performed as first diagnostic examination by the patients and appropriateness of prescriptions ; there was a statistically significant relationship ( p < 0.0001 ) was mri the first diagnostic examination ? appropriateness appropriate ( n ) not appropriate uncertain ( n ) 234 ( 97.1 % ) 36 ( 42.9 % ) 7 ( 2.9 % ) 48 ( 57.1 % ) ( 70.7 % ) by experts of another country without previously confirming whether this approach was considered the best . 
another 4 % who did not perform mri examinations also certainly contributed to these costs mainly because patients did not respect the criteria of executing thein fact , this resulted in work time loss with no possibility of being able to fill in these slots with other patients . 
among the various strategies suggested in obtaining these results , we believe that a prescription aid system similar to the one in sicily should be adopted [ 22 ] , or tout court , allowing only specialists the possibility to prescribe these types of investigations . 
considering what has been mentioned , the sicily region has recently carried out a project regarding the execution time varying on the cases severity and the clinical needs called collaboradi . 
the aim of the project is to create a software application that collaboratively helps the general practitioner ( gp ) to formulate the most appropriate application of di to answer clinical questions in accordance with the most up - to - date guidelines in diagnostic imaging [ 14 ] and priority classes , thus processing the application as provided by the system of homogeneous waiting ( rao ) lists [ 23 ] already in force in sicily . 
indeed , the collaboradi project introduces some innovative aspects in the management of prescription pathways that are not only useful to gps but neither for the radiologists that must check the path of appropriateness and finally to the controller which activates the reimbursement of benefits . 
in addition , false positives that are not appropriate for diagnostic examinations may produce an unbelievable higher number of diagnostic procedures performed further increasing healthcare costs as well as patient discomfort . 
a possible limitation of this study may be the fact that we did not elaborate new shared appropriateness criteria using a recognized method to assess the appropriateness of national healthcare services [ 26 ]  . 
due to the fact that knee mris represent the most frequent diagnostic prescriptions prescribed , it is possible to assume that one - third of the total mri prescriptions could be inappropriate or uncertain because indications are incorrect , not specific or absent . 
this trend results in and causes a financial burden on the national healthcare syste evidence - based criteria , if applied wisely and fairly , may be the most powerful tool for controlling costs and enhancing the quality of mri examinations . 
this also occurs because the criteria for diagnostic examinations depend in part on patients symptoms and activities that do not help to define the criteria . significant challenges to implementing well - designed appropriateness criteria on a national scale must be overcome . a broad consensus about the criteria must be reached . opinion leaders must be involved in developing appropriateness criteria . 
leaders should also recognize that the quality of the criteria will be enhanced if representatives of multiple clinical disciplines are included in the development processnot only radiologists and orthopedists , but also gps , rheumatologists and rehabilitation medicine specialists . acknowledgments we applied the sdc approach for the sequence of authors . 
 ccf diagnosis with ocdus was based on the finding of a reversed , arterialized and low - resistive - index ( ri < 0.5 ) blood flow in the superior ophthalmic vein ( sov )  . 
sensibility , specificity , ppv , npv , and accuracy of ocdus were calculated considering both patients and eyes , using dsa as gold standard . results dsa demonstrated 20 ccfs in 18 patients . 
 considering the eyes , in 24 / 43 ccf diagnosis was positive 43 , due to one case at both dsa and ocdus ( total eyes of sov thrombosis )  . 
congestion of 1 3 302 radiol med ( 2016 ) 121 : 301307 the venous structures determines ocular symptoms such as exophthalmos , chemosis , conjunctival congestion , and glaucoma [ 3 ]  . 
these clinical signs are more evident in high - flow fistulas , such as in direct fistulas , while dural fistulas frequently have delayed diagnosis due to more subtle manifestations [ 1 ]  . 
cerebral digital subtraction angiography ( dsa ) still remains the gold - standard technique to detect and define the abnormal vascular pattern of a fistula [ 6 , 7 ] ; angiography represents also an important therapeutic option to treat the fistula with transarterial ( or transvenous ) embolization of the cavernous sinus [ 811 ]  . 
 considering the high frequency of mild and aspecific ocular symptoms ( e.g. , in patients with dural fistulas ) and the invasiveness of diagnostic angiography , requiring hospitalization , a first - line noninvasive diagnostic approach for the evaluation of a suspected fistula would avoid unnecessary invasive examinations . 
many techniques can show dilatation of the cavernous sinus and ophthalmic veins induced by fistulas , such as ct angiography [ 1214 ] and mr angiography [ 1517 ]  . 
orbital color doppler ultrasound ( ocdus ) is a simple and noninvasive technique useful in many ophthalmological [ 18 , 19 ] , vascular [ 20 , 21 ] , and systemic diseases [ 22 , 23 ]  . 
ocdus was previously used , despite the lack of large series , for the diagnosis of high - flow ccf , based on the typical finding of a dilated superior ophthalmic vein ( sov ) with reversed , arterialized , low - resistance blood flow [ 2729 ]  . 
in the present study , our purpose was to investigate the role of ocdus as a noninvasive screening technique in the diagnosis of ccf using dsa as gold standard , particularly to assess its negative predictive value and to verify whether dsa could be avoided in patients with clinically suspected ccf but negative ocdus . materials and methods subjects we retrospectively evaluated data from all the subjects with clinically suspected ccf who underwent both ocdus and dsa at our institution from february 2000 to july 2014 . 
all patients were evaluated by experienced ophthalmologists and enrolled according to the presence of one or more of the following ophthalmologic symptoms : exophthalmos , chemosis , conjunctival congestion , elevated intraocular pressure ( > 20 mmhg ) , and cranial nerves deficit . ocdus technique all the ocdus examinations were performed by the same 25 - year - experienced radiologist and sonographer ( mv ) , blinded to the final diagnosis , before cerebral angiography . 
ocdus examinations ( atl - philips iu22 / hdi - 5000 , bothell , wa , usa ) were performed with the patient in supine position with closed eyelids , limiting as much as possible eyeball movements . 
b - mode and color doppler transversal and longitudinal scans of the orbital regions were obtained with a linear high - frequency probe ( 512 mhz ) , with adequate setting for low blood flow velocity ( acquisition parameters were optimized with a 1200 - hz pulse repetition frequency )  . 
after identification of the optic nerve as a hypoechoic tubular structure behind the eyeball , color doppler us imaging of the superior ophthalmic vein ( sov ) was performed , both in resting state and during valsalva maneuver . 
a further distinction between a normal arterial flow in the ophthalmic artery and a pathological arterialized flow in the sov was based on the resistive index [ ri , defined as ( peak systolic velocityend diastolic velocity ) / peak systolic velocity ] , higher than 0.5 in the ophthalmic arteries , lower than 0.5 in sov involved by ccf with anterior drainage . 
the finding at ocdus of a dilated sov ( diameter > 2 mm ) , with reversed , arterialized , low - resistance blood flow ( ri < 0.5 ) , was considered diagnostic for the presence of a ccf with anterior drainage , as previously reported by other groups [ 2729 ]  . 
six out of 22 patients underwent also mr angiography . cerebral dsa cerebral dsa ( philips , allura xper biplane system ) was performed in all cases with selective catheterization of the internal 1 3 radiol med ( 2016 ) 121 : 301307 fig . 
2 cerebral dsa ( left internal a and external b carotid artery selective injections in lateral view ) shows a ccf of the left cavernous sinus with anterior drainage in the left superior ophthalmic vedural branches of both internal and external carotid artery feed the fistula . 
the left superior ophthalmic vein is early opacified , abnormally dilated with reversed blood flow and external carotid and vertebral arteries on both sides ; frontal , lateral , and oblique views were acquired . 
in positive cases , the angiographic study defined precisely the site of the fistula , its arterial supply , the angioarchitecture of the shunt , and the pattern of venous drainage . 
 in the subgroup of patients who had a positive diagnosis at ocdus , ccf was confirmed at dsa in 18 / 18 ( 100 % ) cases , while in those with a negative diagnosis at ocdus , ccf was found in none . 
hence , regarding the ability of ocdus in identifying patients with ccf , sensitivity , specificity , positive predictive value ( ppv ) , negative predictive value ( npv ) , and accuracy of ocdus were all of 100 % ( table 1 )  . dsa demonstrated 20 ccfs ( 18 dural and 2 direct carotid - cavernous sinus fistulas ) in 18 patients ; 16 patients presented monolateral and two patients bilateral ccf . among the 16 patients with monolateral ccf , four patients presented bilateral sov involvement , while the remaining 12 patients demonstrated a monolateral sov involvement . considering a separate analysis of the eyes , one eye was not evaluable due to sov thrombosis ( for a total amount of 43 eyes ) ; 24 / 43 eyes ( 55.8 % ) were positive , whereas 19 / 43 eyes ( 44.2 % ) were negative at ocdus . 
in all the 24 ocdus - positive eyes , a ccf was confirmed by dsa ; in particular in 20 / 24 ( 75 % ) cases , the fistula was homolateral to the ocdus finding , whereas in the remaining four eyes , it was contralateral ( monolateral fistula causing bilateral sov involvement and , consequently , bilateral ocdus positivity )  . 1 3 radiol med ( 2016 ) 121 : 301307 table 1 ocdus diagnostic performance ocdus positive ocdus negative total fistula no fistula total positive predictive value 18 / 18 100 % negative predictive value 4 / 4 100 % sensitivity 18 / 18 100 % specificity 4 / 4 100 % accuracy ( 18 4 ) / 22 100 % in none of the 19 ocdus - negative eyes , ccf was detected at dsa ( none false negative )  . therefore , sensitivity , specificity , ppv , npv , and accuracy of ocdus in the eyes sub - analysis were all 100 % . in two out of six patients who underwent also mr angiography , mr provided a false - negative result , and both cases were low - flow dural fistulas not determining sov dilation . discussion ccfs represent 1015 % of all intracranial arteriovenous shunts [ 30 ]  . 
in case of clinical suspect of ccf , usually ct [ 1214 ] or mr angiography [ 1517 ] is the first technique employed to confirm the diagnosis and to decide for subsequent dsa . 
from 1991 , on the basis of sov blood flow arterialization , ocdus was used as noninvasive diagnostic technique to diagnose and monitor carotidcavernous and dural fistulas , in a very small number of patients [ 27 , 28 ]  . 
the sov findings reflect the intracranial venous hemodynamics because the sov reaches the cavernous sinus without a valve through the sphenoidal fissure , and no valve is present in the intracranial venous system [ 29 ]  . 
 [ 29 ] concluded their study with ocdus , based on a larger cohort of patients ( n 20 ) affected by dural fistulas previously diagnosed with dsa , with the following sentence : these findings were useful to evaluate the intracranial venous hemodynamics in dural fistulas . 
the aim of the present study , based on 22 patients , was not only to assess the sensitivity and specificity of ocdus using dsa as gold standard in ccf diagnosis , but also extended to emphasize the negative predictive value . 
sensitivity , specificity , positive predictive value , negative predictive value , and accuracy were all 100 % , considering either 22 patients or 43 eyes ( one excluded due to sov thrombosis )  . 
we have evaluated the true negatives ( 100 % ) , using dsa to accurately define either the involved or the non - involved sovs , to verify whether , in a patient with a clinically suspected ccf , a negative ocdus could avoid dsa . 
as the crucial point of a positive diagnosis of ccf with ocdus is represented by the finding of arterialized , pulsatile flow of sov , at the same way , the finding of a normal continuous venous flow of sov is essential for a negative diagnosis . 
in physiological conditions , sov usually shows a caliber less than 11.5 mm at us , a flow direction moving away from the orbit depicted as blue at color , and a spectral waveform with a typical continuous venous flow with minimal differences between maximum and a minimum velocities at doppler [ 34 , 35 ]  . 
in particular cases , significant differences between maximum and minimum velocities with cyclical , transient reversed blood flow due to the cardiorespiratory kinetic may be also recorded , as previously described [ 34 , 35 ]  . 
in case of high - flow ccf , the typical involved sov shows a dilated caliber more than 2 mm at us , a reversed blood flow directed toward the ocular globe depicted as red at color , and a spectral waveform characterized by a pulsatile , arterialized flow with a peak systolic and an end diastolic velocity at doppler . 
usually , the arterialized blood flow is characterized by a low resistive index less than 0.5 , 1 3 306 radiol med ( 2016 ) 121 : 301307 typical signal of the arteriovenous communications [ 36 ] : this aspect allows a differential diagnosis with ophthalmic artery , also characterized by a flow directed toward the globe with a peak systolic and an end diastolic velocity , but with an higher resistive index usually more than 0.7. 
the diagnosis of ccf with anterior drainage at ocdus is obviously easier in cases of high - flow fistulas compared with low - flow fistulas , where sov may be un - dilated , as in four of our cases : the identification of the un - dilated sov and the distinction between a reversed , arterialized flow and a regular , continuous venous flow is essential for a correct diagnosis . 
it is a single - center study , and as for the other previous reported experiences , the population number is limited , also because ccfs represent a relatively rare disease . 
our study was performed by single operator to avoid the interobserver bias , which would have been even more deleterious given the small number of patients . anyway , visualization of orbital vessels at retrobulbar level with ocdus through ocular globe , a water ball representing a natural acoustic window , is easy . 
experienced sonographers using adequate color doppler ultrasound technologies significantly improved in the last years ( harmonic imaging etc . ) can always be able to identify sovs , accurately setting their ocdus units for low blood flow velocities , sometimes during valsalva maneuver . 
moreover , we also believe that they can always characterize sov blood flow in physiological and pathological conditions , as for example ccfs with anterior drainage , and distinguish a normal venous from an arterialized flow , allowing an accurate noninvasive diagnosis . 
differently from ct and mr angiography , ocdus is a low - cost , simple , quick technique able in real time to provide hemodynamic information about sov blood flow and probably to diagnose ccfs , also in case of low - flow fistulas not determining sov dilation . 
as a matter of fact , in two out of six patients who underwent mr angiography , it provided a false - negative result due to the lack of sov dilation . summarizing , our study has several limitations ( single center , retrospective , small numbers even though ccf is a rare disease ) , thus we acknowledge that no definitive conclusion can be drawn . 
of note , it must be remembered all the previous similar experiences also reported very small patient populations , and none of them assessed the negative predictive value of ocdus . 
the neoadjuvant treatment regimen consisted of 50 gy of radiation delivered in 25 fractions , 5 days per week , with concurrent daily capecitabine ( 1650 mg / m2 / day , twice daily during rt course ) and weekly oxiliplatin 50 mg / m2 / qw . 
multivariable linear regression model is used to test correlation between ht and dose - volume of bm . results thirty - one patients ( 88.6 % ) had stage t34 disease , and 30 patients ( 85.7 % ) had node - positive disease . 
17 panjiayuan nanli , chaoyang district , beijing 100021 , china conclusions the irradiated volume of pelvic bm identified by mr is associated with ht in rectal cancer patients undergoing neoadjuvant concurrent chemoradiotherapy . keywords rectal cancer intensity - modulated radiation therapy magnetic resonance bone marrow hematologic toxicity introduction preoperative radiotherapy is used with radiosensitizers , such as 5 - fluorouracil , to downsize the primary tumor and to reduce the risk of locoregional failure after resection [ 1 , 2 ] , by which the acute treatment - related hematologic toxicity ( ht ) was more pronounced [ 3 , 4 ]  . 
the disadvantages of this approach are increased risk of infection , use of granulocyte colony stimulating factor , extended treatment period , and delayed surgery / adjuvant chemotherapy . it is known that both radiation and chemotherapy are myelosuppressive and more than half of the bodys hematopoietically active ( red ) bone marrow ( bm ) is located in the pelvic bones , thoracic and lumbar vertebras in adults , which are just the low - dose area of radiotherapy ( rt ) in rectal cancer [ 59 ]  . 
when chemotherapy is given concurrently , however , additional bm injury and myelosuppression increase ht to grade 3035 % , particularly leukopenia and neutropenia , predisposing patients to infection , hospitalization , and requirements for transfusions and growth factors [ 1315 ]  . 
importantly , ht can also lead to delayed or missed chemotherapy 1 3 radiol med ( 2016 ) 121 : 308314 cycles and treatment breaks , potentially compromising disease control . 
reduction of ht is , therefore , an important goal . previous studies have identified relationship between ht and the volume of pelvic bm receiving in gynecologic and other cancers during crt course [ 9 , 1624 ] , suggesting that techniques designed to reduce bm irradiation , such as intensity - modulated radiotherapy ( imrt ) , might reduce ht . 
however , the effect of pelvic active bm - sparing ( bms ) imrt ( bms - imrt ) plans to reduce ht has never been investigated in rectal cancer patients . we have since assumed that better active bm sparing is possible when the active bm is indentified by t1 - weighted magnetic resonance ( mr ) and entered as a separate constraint in the rt planning process [ 6 , 2528 ]  . 
therefore , we designed this study to test whether a separate constraint of active bm identified by mr could reduce acute ht in course of concurrent crt for patients with rectal cancer . active bm delineation and treatment planning all the patients received pelvic mr scanning no later than 7 days before computer tomography ( ct ) simulation ( ctsim )  . 
 the details of active bm identification and targets delineation are as follows . simulation patients were required to undergo ct - sim in the prone position with a full bladder and use a belly board to minimize exposure of the small bowel . 
thermoplastic immobilizations were used to immobilize patients during ct - sim and imrt with a 6 - mv photon beaoral contrast was administered prior to the ct simulation to show small bowel . 
a radio - opaque marker was placed at the anal marg the superior and inferior limits of the acquired transaxial data were the iliac crests and 5 cm inferior to the anal marker , respectively . 
intravenous contrasts were administered before ct - sim . materials and methods mr scanning we undertook a prospective , open - label , single - arm phase ii study in patients with histologically proven rectal adenocarcinoma and needed a preoperative concurrent clinicaltrials.gov registration number : nct1863420 ( crt )  . 
written informed consent was obtained from each patient before enrollment . the patients were scanned in the supine position on a 1.5 t genesis - signa mr scanner ( ge medical systems ) no later than 7 days before ct - sicare was taken to reproduce the simulation position at the time of the mr . 
the eligibility of having preoperative crt was as follows : histologically confirmed rectal adenocarcinoma located < 12 cm from anal verge ; t34 any n0 m0 or any tn m0 according to 7th edition of the american joint committee on 75 years ; a cancer tnm classification ; age > 18 and performance status of 1 or lower according to eastern cooperative oncology group ( ecog ) criteria ; adequate function of major organs ( including cardiac , hepatic , and renal functions ) , adequate bone marrow function ( hemoglobin > 10 g / dl ; absolute neutrophil count 100 , 000 / l ; leu ( anc ) 4000 / l ) ; a caloric intake greater than kocyte count 1500 kcal / day by oral route ; no previous pelvic radiation and prior treatment , no history of any other tumors except for basal cell carcinoma of the skin and carcinoma in situ of the uterine cervix . 2000 / l ; platelet count image fusion the mr images were subsequently fused with the ct - sim images using pinnacle system and syntegra image fusion software . 
the interactive mode of the fusion software was used wherein the user manually translates and rotates the mr scan to produce the best visual overlay of the two image sets . 
anti - emetics and antidiarrheal agents were prescribed when needed . results clinical characteristics end points and statistics endpoints of interest were the white blood cell count ( wbc ) , absolute neutrophil count ( anc ) , hemoglobin ( hb ) , and platelet count ( plt ) nadirs within 60 days of initiation of crt . 
hematologic toxicity and other morbidity were graded according to the radiation therapy oncology group acute radiation toxicity scoring criteria [ 31 ]  . a total of 35 patients were enrolled in this study between may 2013 and october 2014 , and all patients received bms - imrt combined with capecitabine and oxiliplatin , whose demographic and tumor characteristics are listed in table 1 . 
 thirty - one patients ( 88.6 % ) had stage t34 disease , and 1 3 radiol med ( 2016 ) 121 : 308314 table 1 patients characteristics table 2 acute hematologic toxicity and other morbidities variable patients gender male female iii median age ( years , range ) ecog performance status mean bmi , kg / m2 ( sd ) t stage no . 
of positive lymph node , n ( % ) clinical stage distance between tumor and anal verge ( cm ) 5 , < 10 cm < 5 cm bmi body mass index , ecog eastern cooperative oncology group 30 patients ( 85.7 % ) had node - positive disease . 
median distance between tumor and anal verge was 4 cm ( 08 cm )  . radiation delivery and dosimetric parameters radiotherapy was stopped at 46 and 44 gy in two patients because of grade 3 diarrhea and grade 3 perianal dermatitis . 
the other 33 patients completed planned concurrent chemoradiation , in which three patients required treatment break for grade 3 diarrhea ( n 2 ) and grade 3 perianal dermatitis ( n 1 )  . 
the details were as follows : 9 ( 25.7 % ) of grade 24 leukopenia , 6 ( 17.1 % ) of grade 24 neutropenia , 1 ( 2.9 % ) of grade 24 anemia and 1 ( 2.9 % ) of grade 24 thrombocytopenia . 
by contrast , there was no correlation between radiation dose - volume metrics and anemia , which is consistent with the result of pelvic malignancies [ 9 , 23 ]  . 
 the current study improves our understanding of the distribution of hematopoietically active bm and may enhance patient outcomes through facilitation of rt techniques designed to reduce ht . the acute ht ( grade 96 % might control the incidences of grade 2 3035 % ) by concurrent chemoradiation is the major cause to compromise treatment completion and intestification in rectal cancer patients [ 1315 ]  . 
many pre - clinical studies have demonstrated bm stem cells are sensitive to low doses of radiation , and damage to these cells is a principal cause of ht [ 10 ]  . 
previous studies have founded acute ht was significantly associated the volume of pelvic bm and lumbosacral bm receiving 10 and 20 gy radiation in pelvic cancers [ 9 , 22 , 23 ]  . 
therefore , reducing the volume of active bm receiving low - dose rt might prevent ht . on the other hand , we first evaluate the feasibility of mr identifying active bm within the pelvic bones in rectal patients and the data suggest that mr imaging is a useful adjunct to imrt planning and offer the possibility of customizing treatment based upon an individual patients active bm distribution . 
on t1 - weighted mr images , regions of active ( red ) marrow exhibit a low - intensity signal ( similar to muscle ) [ 6 , 29 ] , while regions of nonactive ( fatty ) bm have a high intensity signal similar to fat . 
 1 3 radiol med ( 2016 ) 121 : 308314 however , the results should be interpreted carefully , because it is unclear the range of entire bm parameter values in which the relationship between ht and dosimetric parameters is valid , and there is still unexplained variation in some patients with high wbc nadirs and high bm - v5 . 
 as other factors were also found to be related with ht in crt , e.g. , female gender , bmi [ 23 ] , more sophisticated models may be required to characterize accurately the dependence of ht on dosimetric and clinical factors . limitations our single - center study has several limitations , including no control setting , contouring the active bm by mr is rather arbitrary , as there is no standard signal values in mr images to discriminate active or inactive bm . 
other functional bm images with quantitative parameters might be promising , such as positron emission tomography [ 8 , 9 ]  . conclusions this study lends strong support to the hypothesis that v5 and v10 of pelvic active bm are important predictors of ht in rectal cancer patients undergoing neoadjuvant crt . 
 further test would be needed in a large group of patients to optimize and determine the clinical significance of bmsparing techniques . 80 % could significantly reduce grade 96 % , bm - v20 compliance with ethical standards this study was supported by beijing hope run special fund ( grant number lc2012b22 )  . 
the introduction systematic approach to clinical research could offer many benefits , reduce time commitment , and facilitate study conduct and data management . there should also be adequate financial compensation for clinicians who participate in multicentre clinical research projects . one area that requires attention is the provision of patient information , particularly in oncology , where disease recurrence is frequently fatal . new communication strategies are needed to ensure that information on treatment options at disease relapse reaches patients in a timely fashion , information can be so that the understood and considered in a nonthreatening way . 
at the national institutes of health ( nih ) , assignment of applications logistics of follow the does not intramural research , but instead are that focus on to disease . distributed according applications development of clinical research therefore not be strategies may assigned to the institution with the most expertise in the relevant area and may therefore not be reviewed by the appropriate people . 
 institutional these procedures research and not board review consideration of clinical studies follows an academic approach that is not appropriate for multicentre studies or the small business setting . encourage all isolated preclinical and single centre academic collaborative clinical and multicentre to develop a approach needed product and bring it to the market , or to test a treatment strategy so that it can become evidence - based therapy . 
 a recently released nih policy requires up - front definition of the composition of candidates according to ethnicity and race and makes these characteristics eligibility criteria as well as reporting criteria.2 this an undesirable selection bias , that interferes with equal opportunities for enrollment and contradicts federal directives.3 such policies discourage clinical investigators from submitting clinical research grant applications.3 introduces trial the nih is not the only funding institution with procedures and cooperative policies that make research other future of clinical multicentre clinical research difficult , neither is the usa the only country where it is difficult to obtain funding than for clinical product - development - related studies . the research depends on a change in vision and on the introduction of new methods for the conduct of studies . 
changes in planning , communication , execution , and financial reward are vital in order to motivate researchers to participate in patientoriented studies . marlies ehm van hoef transplant creations lc , 5597 seminary road , ste 2210 , falls church , va , 22041 , usa coordination , 1 unresolved crisis in clinical research . the lancet oncology 2001 ; 2 : 459 . 2 policy on reporting race and ethnicity data : subjects in clinical research . 
mortality data , derived from the registration of deaths , are available for many countries via the world health db.iarc.fr / this cdrom contains computer programs to analyse and present the cancer database . 
only reproduce with permission from the lancet publishing group . de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
only reproduce with permission from the lancet publishing group . de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
only reproduce with permission from the lancet publishing group . de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
only reproduce with permission from the lancet publishing group . de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
only reproduce with permission from the lancet publishing group . mailbox spindle cell carcinomas are uncommon his the own article tongue are we are intrigued by the statement by borislav dimitrov that most cancers spindle - cell carcinomas.1 we do not have access to the reference given by the author encyclopaedia of human nutrition.2 however , in our own experience and from the literature , it is clear that conventional squamous carcinoma is the most common cancer of the tongue . 
at the tata memorial hospital , mumbai , india , in 1995 , there were cell four carcinomas of the tongue compared spindle with 354 conventional squamous carcinomas . there are few papers on spindlecell carcinomas of the tongue in the literature , which is line with the fact that they are uncommon . 
to our knowledge , the biggest series on spindle cell carcinomas of the oral cavity was studied by ellis and corio.3 they analysed 59 cases , 12 of which tongue . 
oral surg 1980 ; 50 : 523534 . clinical testing of ukrain some remarks in the letter about ukrain in the lancet oncology ( dec 2000 ) by farrugia and slevin1 are based upon a misunderstanding , especially the assertion that we , as the producers of ukrain , are unable or unwilling to take the opportunity for a sober assessment of the drug . 
 the drug we agreed immediately to the proposal for a clinical study at st bartholomews hospital and agreed to supply free of charge . however , we assumed that a clinical study at a major european teaching hospital would be carried out according to good clinical practice ( gcp ) with independent monitoring , which is a requirement of gcp . 
 followed most of the clinical studies carried out on ukrain so far have taken place outside the european union and while have investigators guidelines of gcp the studies have been criticised because not all the formalities were observed . 
 we were therefore unable understand why farrugia and slevin were unwilling to carry out the study according to gcp with independent monitoring , a precondition which we took for granted would be met at a major european teaching hospital . 
 we would like to emphasise that we are most willing for an objective , independently monitored study accordance with gcp to be carried out on ukrain , that we are prepared to supply the drug free of charge for such a study and that we hope that the study proposed by farrugia and slevin can in fact take place . 
lancet oncol 2000 ; 1 : 204 . authors reply the proposed study , which we outlined in our letter , was in keeping with standard practice for phase ii studies and had the approval of our institutions ethics committee . 
the issue of an independent monitoring committee was never raised by nowicky and we would have no objection to this , if the company would bear the cost , although it is not a routine part of phase ii studies . it was the need for an objective assessment of this compound ( which as he rightly says , is lacking in all the clinical papers reported by nowicky and his colleagues ) , which prompted us to suggest this study . we intended to subject ukrain to the same assessment that any other anti - cancer agent would receive within the context of a phase ii study . 
it seems to us that the issue of gcp is a red herring designed to prevent the study taking place and to us why nowicky decided to withdraw his support . david farrugia * , maurice l slevin * cheltenham hospital , cheltenham , gloustershire gl53 7an , uk . 
not to be reproduced without permission of the lancet . mailbox indias new smoking laws passed with regard to the editorial in the march issue of the lancet oncology , 1 i would like to emphasise the major impact tobacco eradication will have on cancer mortality , far exceeding any other recent intervention . 
the tobacco products ( prohibition of advertisement and regulation ) bill 2000 the cabinet committee of the government of india is a diluted version of a similar law passed in goa 2 years ago.2 the goan law was passed unanimously , as a result of persuasion by sharad vaidya through the national organisation for tobacco ( india )  . eradication described as a draconian law by the tobacco industry , it has had full public support , so its implementation was much easier than anticipated . 
for the rest of the country , let us not allow the best to be the enemy of good . less there cannot be an alternative to complete eradication of the tobacco industry anything is plain hypocrisy . 
every support world * will go a long way towards getting this bill enacted . from people around for sports sponsorship encourages young children to take up smoking , by creating false positive impressions on childrens minds.2 , 3 targeting children in the developing world is a powerful the millions replacing ploy ( including 800 000 to 1 million indians ) of customers that the tobacco industry loses each year . 
there will be many other willing sponsors for our cricketers ( all non - smokers ) , as has been experience in other countries that banned tobacco sponsorship . should india concentrate on improving treatment of smokingrelated diseases ? one in two smokers dies because of smoking , so stopping a child becoming addicted equates to a 50% chance of saving a life4 a better success cancer treatments . 
 than most rate the will this law be disastrous to the tobacco industry ? i sincerely hope so . twenty - six million is a figure that has been frequently touted by the tobacco industry as the number of people in tobacco - related employment , but it is a falsely inflated figure . 
in fact , there are only 6 million people in full - time employment by the tobacco industry . there are only 1 million farmers who grow tobacco , alternately with other crops , and there are 60 cigarette factories . 
for every seven people who remain employed tobacco industry , one person has to die every year a small sacrifice ? if the tobacco industry disappears , the farmers will not suffer ; 50% of indian tobacco is cultivated on the best rain - fed fertile areas of our country , while the rest is grown on the black , fertile soil of karnataka and andhra pradesh and it depletes the soil at 23 times the rate of food crops.5 the government , through the tobacco board act , gives much more money to tobacco growers than to food - growing farmer : 450% of the cost of production to tobacco , 150% for food crops , and 250% for cotton crops . 
 the benefit of many people will be surprised that the tobacco board6 is a governmentfunded institute , whose aims are sponsoring , assisting , coordinating , and encouraging a scientific technical economical research for promotion of tobacco industry ; the board spends millions of rupees on research into tobacco science every year , via the central tobacco research institute . 
j indian med assoc 1999 ; 97 : 3546 , 359 . 4 doll r , peto r , wheatley k , et al . mortality in relation to smoking : 40 years observations on male british doctors . 
the only clear - cut examples we have of genetic selection with humans are with genes related to infection ( eg , hla , haemoglobin , blood group , and ccr5 )  . 
protection against cancer , even if it exists , is highly unlikely to have been the basis for prior selective advantage of cf mutations if the cancers concerned are predominantly post - reproductive . 
i did not suggest that all prior human genetic selection imposed a subsequent cancer risk . mir and orecchia also suggest that evolution would not ...try a fecundity advantage at any price , if this means the perpetuation of risky genotypes that may cause increased cancer incidence in future generations . 
what i suggested was that certain human selected genotypic historically under particular conditions , have subsequently become risky for cancer in the face of novel ( and mostly contemporary ) social circumstances quite unrelated to those prevailing at initial the selection . characteristics , time of mel greaves institute of cancer research , chester beatty laboratories , 237 fulham road , london sw3 6jb , uk . erratum mantle - cell lymphoma by ibrahim barista , jorge e romaguera , and fernando cabanillas . 
chemotherapy for mantle - cell lymphoma40 * chemotherapy regimens cr ( % ) cr + pr ( % ) de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
only reproduce with permission from the lancet publishing group . de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
only reproduce with permission from the lancet publishing group . mailbox indias new smoking laws passed with regard to the editorial in the march issue of the lancet oncology , 1 i would like to emphasise the major impact tobacco eradication will have on cancer mortality , far exceeding any other recent intervention . 
the tobacco products ( prohibition of advertisement and regulation ) bill 2000 the cabinet committee of the government of india is a diluted version of a similar law passed in goa 2 years ago.2 the goan law was passed unanimously , as a result of persuasion by sharad vaidya through the national organisation for tobacco ( india )  . eradication described as a draconian law by the tobacco industry , it has had full public support , so its implementation was much easier than anticipated . 
for the rest of the country , let us not allow the best to be the enemy of good . less there cannot be an alternative to complete eradication of the tobacco industry anything is plain hypocrisy . 
every support world * will go a long way towards getting this bill enacted . from people around for sports sponsorship encourages young children to take up smoking , by creating false positive impressions on childrens minds.2 , 3 targeting children in the developing world is a powerful the millions replacing ploy ( including 800 000 to 1 million indians ) of customers that the tobacco industry loses each year . 
there will be many other willing sponsors for our cricketers ( all non - smokers ) , as has been experience in other countries that banned tobacco sponsorship . should india concentrate on improving treatment of smokingrelated diseases ? one in two smokers dies because of smoking , so stopping a child becoming addicted equates to a 50% chance of saving a life4 a better success cancer treatments . 
 than most rate the will this law be disastrous to the tobacco industry ? i sincerely hope so . twenty - six million is a figure that has been frequently touted by the tobacco industry as the number of people in tobacco - related employment , but it is a falsely inflated figure . 
in fact , there are only 6 million people in full - time employment by the tobacco industry . there are only 1 million farmers who grow tobacco , alternately with other crops , and there are 60 cigarette factories . 
for every seven people who remain employed tobacco industry , one person has to die every year a small sacrifice ? if the tobacco industry disappears , the farmers will not suffer ; 50% of indian tobacco is cultivated on the best rain - fed fertile areas of our country , while the rest is grown on the black , fertile soil of karnataka and andhra pradesh and it depletes the soil at 23 times the rate of food crops.5 the government , through the tobacco board act , gives much more money to tobacco growers than to food - growing farmer : 450% of the cost of production to tobacco , 150% for food crops , and 250% for cotton crops . 
 the benefit of many people will be surprised that the tobacco board6 is a governmentfunded institute , whose aims are sponsoring , assisting , coordinating , and encouraging a scientific technical economical research for promotion of tobacco industry ; the board spends millions of rupees on research into tobacco science every year , via the central tobacco research institute . 
j indian med assoc 1999 ; 97 : 3546 , 359 . 4 doll r , peto r , wheatley k , et al . mortality in relation to smoking : 40 years observations on male british doctors . 
reproduce with permission from the lancet publishing group . mailbox spindle cell carcinomas are uncommon his the own article tongue are we are intrigued by the statement by borislav dimitrov that most cancers spindle - cell carcinomas.1 we do not have access to the reference given by the author encyclopaedia of human nutrition.2 however , in our own experience and from the literature , it is clear that conventional squamous carcinoma is the most common cancer of the tongue . 
at the tata memorial hospital , mumbai , india , in 1995 , there were cell four carcinomas of the tongue compared spindle with 354 conventional squamous carcinomas . there are few papers on spindlecell carcinomas of the tongue in the literature , which is line with the fact that they are uncommon . 
to our knowledge , the biggest series on spindle cell carcinomas of the oral cavity was studied by ellis and corio.3 they analysed 59 cases , 12 of which tongue . 
oral surg 1980 ; 50 : 523534 . clinical testing of ukrain some remarks in the letter about ukrain in the lancet oncology ( dec 2000 ) by farrugia and slevin1 are based upon a misunderstanding , especially the assertion that we , as the producers of ukrain , are unable or unwilling to take the opportunity for a sober assessment of the drug . 
 the drug we agreed immediately to the proposal for a clinical study at st bartholomews hospital and agreed to supply free of charge . however , we assumed that a clinical study at a major european teaching hospital would be carried out according to good clinical practice ( gcp ) with independent monitoring , which is a requirement of gcp . 
 followed most of the clinical studies carried out on ukrain so far have taken place outside the european union and while have investigators guidelines of gcp the studies have been criticised because not all the formalities were observed . 
 we were therefore unable understand why farrugia and slevin were unwilling to carry out the study according to gcp with independent monitoring , a precondition which we took for granted would be met at a major european teaching hospital . 
 we would like to emphasise that we are most willing for an objective , independently monitored study accordance with gcp to be carried out on ukrain , that we are prepared to supply the drug free of charge for such a study and that we hope that the study proposed by farrugia and slevin can in fact take place . 
lancet oncol 2000 ; 1 : 204 . authors reply the proposed study , which we outlined in our letter , was in keeping with standard practice for phase ii studies and had the approval of our institutions ethics committee . 
the issue of an independent monitoring committee was never raised by nowicky and we would have no objection to this , if the company would bear the cost , although it is not a routine part of phase ii studies . it was the need for an objective assessment of this compound ( which as he rightly says , is lacking in all the clinical papers reported by nowicky and his colleagues ) , which prompted us to suggest this study . we intended to subject ukrain to the same assessment that any other anti - cancer agent would receive within the context of a phase ii study . 
it seems to us that the issue of gcp is a red herring designed to prevent the study taking place and to us why nowicky decided to withdraw his support . david farrugia * , maurice l slevin * cheltenham hospital , cheltenham , gloustershire gl53 7an , uk . 
the introduction systematic approach to clinical research could offer many benefits , reduce time commitment , and facilitate study conduct and data management . there should also be adequate financial compensation for clinicians who participate in multicentre clinical research projects . one area that requires attention is the provision of patient information , particularly in oncology , where disease recurrence is frequently fatal . new communication strategies are needed to ensure that information on treatment options at disease relapse reaches patients in a timely fashion , information can be so that the understood and considered in a nonthreatening way . 
at the national institutes of health ( nih ) , assignment of applications logistics of follow the does not intramural research , but instead are that focus on to disease . distributed according applications development of clinical research therefore not be strategies may assigned to the institution with the most expertise in the relevant area and may therefore not be reviewed by the appropriate people . 
 institutional these procedures research and not board review consideration of clinical studies follows an academic approach that is not appropriate for multicentre studies or the small business setting . encourage all isolated preclinical and single centre academic collaborative clinical and multicentre to develop a approach needed product and bring it to the market , or to test a treatment strategy so that it can become evidence - based therapy . 
 a recently released nih policy requires up - front definition of the composition of candidates according to ethnicity and race and makes these characteristics eligibility criteria as well as reporting criteria.2 this an undesirable selection bias , that interferes with equal opportunities for enrollment and contradicts federal directives.3 such policies discourage clinical investigators from submitting clinical research grant applications.3 introduces trial the nih is not the only funding institution with procedures and cooperative policies that make research other future of clinical multicentre clinical research difficult , neither is the usa the only country where it is difficult to obtain funding than for clinical product - development - related studies . the research depends on a change in vision and on the introduction of new methods for the conduct of studies . 
changes in planning , communication , execution , and financial reward are vital in order to motivate researchers to participate in patientoriented studies . marlies ehm van hoef transplant creations lc , 5597 seminary road , ste 2210 , falls church , va , 22041 , usa coordination , 1 unresolved crisis in clinical research . the lancet oncology 2001 ; 2 : 459 . 2 policy on reporting race and ethnicity data : subjects in clinical research . 
mortality data , derived from the registration of deaths , are available for many countries via the world health db.iarc.fr / this cdrom contains computer programs to analyse and present the cancer database . 
the only clear - cut examples we have of genetic selection with humans are with genes related to infection ( eg , hla , haemoglobin , blood group , and ccr5 )  . 
protection against cancer , even if it exists , is highly unlikely to have been the basis for prior selective advantage of cf mutations if the cancers concerned are predominantly post - reproductive . 
i did not suggest that all prior human genetic selection imposed a subsequent cancer risk . mir and orecchia also suggest that evolution would not ...try a fecundity advantage at any price , if this means the perpetuation of risky genotypes that may cause increased cancer incidence in future generations . 
what i suggested was that certain human selected genotypic historically under particular conditions , have subsequently become risky for cancer in the face of novel ( and mostly contemporary ) social circumstances quite unrelated to those prevailing at initial the selection . characteristics , time of mel greaves institute of cancer research , chester beatty laboratories , 237 fulham road , london sw3 6jb , uk . erratum mantle - cell lymphoma by ibrahim barista , jorge e romaguera , and fernando cabanillas . 
chemotherapy for mantle - cell lymphoma40 * chemotherapy regimens cr ( % ) cr + pr ( % ) correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections published online december 11 , 2017 s1470 - 2045 ( 17 ) 30914 - 2 see articles page 27 neoadjuvant chemotherapy in breast cancer : more than just downsizing the early breast cancer trialists collaborative group ( ebctcg ) has established a new milestone in evidencebased treatment for early breast cancer . 
through longstanding collaboration , mutual trust , and data transparency , they have gathered individual patient data for 4756 women randomly allocated in ten trials to either neoadjuvant chemotherapy ( nact ) or adjuvant chemotherapy , with a median follow - up of 9 years ( iqr 514 )  . 
the results of this meta - analysis , 1 published in the lancet oncology , substantiate that nact results in higher rates of breast - conserving therapy than does adjuvant chemotherapy ( rate ratio 128 [ 95% ci 122134 ] ) , without compromising on distant recurrence , breast cancer survival , or overall survival . 
 much emphasis is given by the authors to an increase in local recurrence in the nact group ( 15 year absolute increase of 55% [ 95% ci 2486 ] )  . 
the metaanalysis by mieog and colleagues2 showed no significant difference in local recurrence between patients receiving breast - conserving surgery after nact and breastconserving surgery followed by adjuvant chemotherapy , even with inclusion of those receiving nact that were initially scheduled for mastectomy . in the meta - analysis by the ebctcg , 1 nact led to response of the primary tumour , which undoubtedly led to concomitant downstaging of the axillary lymph nodes . 
 studies3 , 4 have shown that pathological complete response ( pcr ) of the axilla is achieved in 4175% of patients with her2 - positive or triple - negative cancer lymph node dissection receiving nact . 
especially among patients with an ultrasound - positive or cytological - positive axilla who had a clinical response with downstaging to a negative axilla , controversy still exists regarding the timing and accuracy of nodal staging with sentinel lymph node biopsy.5 , 6 several studies have addressed the accuracy of nodal staging after nact and current consensus is that sentinel lymph node biopsy after nact in patients with initial positive axilla is considered accurate if at least three or more sentinel nodes are detected and examined.6 although the willingness of surgeons to omit axillary lymph node dissection or radiotherapy of the axilla in patients with complete response to nact is high , 7 no studies have yet investigated locoregional outcomes . 
a randomised phase 3 trial8 is ongoing to assess the role of axillary radiotherapy versus no axillary radiotherapy in patients who converted to pathologically node - negative disease after nact . 
 improvements as was shown in the ebctcg meta - analysis , patients with high - grade , hormone receptor - negative tumours were most likely to achieve a complete clinical response of the primary tumour after nact . 
with the introduction of targeted therapies and improved systemic strategies , substantial pcr have been seen in the past decade , especially in patients with her2 - positive or triple - negative breast cancers . 
several trials have reported consistently high pcr proportions of up to 83% among her2positive , hormone receptor - negative cancers treated preoperatively with combination chemotherapy and ( dual ) targeted anti - her2 agents.9 these complete responders are offered routine breast cancer surgery similar to patients who did not receive nact . 
 several groups are investigating the accuracy of core needle biopsies in the marked area to establish pcr after neoadjuvant treatment , in either those with radiological complete response ( micra study ; trialregister.nl , number ntr6120 ) or those with her2 - positive or triple - negative disease with partial or complete response ( nct02455791 )  . 
on the basis of initial findings of high accuracy of core needle biopsies in small studies , single - arm studies have started recruitment to establish long - term outcomes for omission of breast surgery ( nct02945579 ) .9 , 10 with the evidence generated from this meta - analysis , patients with large tumours can be recommended to have nact and subsequent breast - conserving surgery depending on response assessment . 
time to stop operating on breast cancer patients with pathological complete response ? eur j surg oncol 2013 ; 39 : 92430 . 10 van la parra rf , kuerer hm . 
 breast cancer res 2016 ; 18 : 28 . tumour infiltrating lymphocytes in breast cancer : increasing clinical relevance the immune microenvironment is now recognised as crucial in the treatment of cancer . 
the tumour immune infiltrate has been noted to be associated with better outcomes in her2 - positive breast cancer and triple - negative breast cancer ( tnbc ) , in both the early - stage and the advanced disease setting.1 , 2 incorporating the quantity of the pre - existing immune response with other prognostic clinical pathological factors , such as tumour size and nodal status , will allow clinicians to better estimate long - term survival after breast cancer diagnosis.3 such data will help clinicians improve their treatment recommendations and allow us to design clinical trials of novel treatments for the subgroups that need the most improvement in survival . in the lancet oncology , carsten denkert and colleagues4 have assessed the predictive and prognostic effect of the concentration of tumour - infiltrating lymphocytes ( tils ) , assessed by use of pretreatment haematoxylin and eosin ( h&e ) stained slides of core biopsies , from patients enrolled in six randomised trials investigating neo - adjuvant treatment in breast cancer.4 3771 patient samples were assessed , which constituted the largest pooled analysis on the effect of tils in the neoadjuvant setting to date . 
the authors confirmed the importance of til quantity in the prediction of pathological complete response , independent of breast cancer subtype , and pathological complete response was strongly associated with a better prognosis ( disease free - survival ) in patients with tnbc and her2 - positive breast cancer , but not in a small luminalher2 - negative subgroup . 
 published online december 7 , 2017 s1470 - 2045 ( 17 ) 30905 - 1 see articles page 40 vol 19 january 2018 comment instead be invested in smarter clinical trial designs that can answer relevant clinical questions , such as whether sequencing of drugs is better than combination therapies , or defining the optimal duration of adjuvant treatment . 
 fortunately , an embarrassment of riches . juan martin - liberal melanoma , sarcoma and genitourinary tumors unit , institut catal doncologia ( ico ) lhospitalet , 08907 barcelona , spain ; and molecular therapeutics research unit ( uitm ) , vall dhebron institute of oncology ( vhio ) , 08035 barcelona , spain jmartinliberal@gmail.com i have received lecture fees and travel grants from roche , novartis , msd , and bristol - myers squibb . luke jj , flaherty kt , ribas a , long gv . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
gb / document_library / summary_of_opinion_ - _initial_authorisation / human / 004579 / wc500252668.pdf ( accessed sept 5 , 2018 )  . another step towards improving oncofertility counselling of young women with hodgkins lymphoma possible chemotherapy - induced premature ovarian insufficiency is of great concern for female premenopausal patients with cancer . 
therefore , appropriate counselling on the risk of premature ovarian insufficiency is now mandatory in all countries.1 , 2 oncofertility counselling is of particular importance for women who have hodgkins lymphoma , who are often diagnosed at a young age . 
however , the counselling of these women can be quite complex because of the paucity of accurate data to estimate the effect of different chemotherapy regimens on their gonadal function . 
previous studies in this setting were mostly retrospective or relied only on menstrual function after treatment to define premature ovarian insufficiency , a measure that is not an optimal surrogate for assessing gonadal damage associated with treatment . in the lancet oncology , richard a anderson and colleagues3 report important results for helping physicians informing premenopausal women with advanced hodgkins lymphoma about the risk of chemotherapyinduced premature ovarian insufficiency associated with doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) or avd , or bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisone ( beacopp ) chemotherapy.3 in this substudy , done within the rathl trial ( nct00678327 ) , biomarkers of ovarian function during and up to 3 years after chemotherapy were assessed in women younger than 45 years at the time of diagnosis . 
specifically , 67 participants were monitored for serum antimllerian hormone concentrations and 321 participants for follicle - stimulating hormone concentrations despite a few limitations , including the small sample size of the antimllerian hormone analysis , particularly of those who were treated with beacopp , and the lack of collection of participant information from the main rathl cohort that could have had a potential effect on outcomes ( eg , use of hormonal contraceptives , previous fertility preservation procedures , and menstrual status after chemotherapy ) , this study provides more precise information than previous reports to counsel women with hodgkins lymphoma on gonadal damage induced by abvd , avd , or beacopp . 
 first , the study confirms that both the type of chemotherapy and patients age at the time of treatment remain the two major determinants of risk of premature ovarian insufficiency for all patients with cancer.4 , 5 antimllerian hormone concentrations decreased sub stantially during both chemotherapy regimens ; however , while antimllerian hormone published online september 13 , 2018 s1470 - 2045 ( 18 ) 30562 - x see articles page 1328 1264 vol 19 october 2018 comment concentrations recovered to before treatment levels in those patients given abvd or avd by 1 year after treatment , little recovery of antimllerian hormone concentrations was treatment with beacopp.3 in anderson and colleagues study , age was shown to be a crucial factor , with increased risk of chemotherapy - induced premature ovarian insufficiency after both regimens in women aged 35 years and older at the time of diagnosis . seen after second , these results highlight the need for a standardised definition of premature ovarian insufficiency . 
different endpoints ( menstrual function only , ovarian biomarkers onlyas in the present studyor a combination of the two ) and timing of its assessment ( ranging from a few months up to several years after chemotherapy ) have been used to define chemotherapyinduced premature ovarian insufficiency . 
 guidelines suggest use of a composite endpoint that includes both amenorrhoea and a hormone profile after menopause , 6 , 7 and assessing chemotherapy - induced pre mature ovarian insufficiency at least 2 years after the end of treatment.7 in the present study , recovery of ovarian function , as measured by follicle - stimulating hormone concentrations , occurred by 1 year after the end of treatment for most patients ( 75% treated with abvd or avd and 33% treated with beacopp ) , but recovery can also happen during the second year ( 18% of participants treated with abvd or avd and 50% with beacopp ) with little chance of recovery thereafter . 
these results support the expert opinionbased indication to assess ovarian function after chemotherapy no earlier than 2 years after treatment completion.7 third , although this study provides further evidence on the role of antimllerian hormone as a biomarker of gonadotoxicity , the clinical utility of its assessment during treatment and subsequent follow - up remains to be fully determined . 
as shown in other studies , 8 , 9 both resumption of menstrual function and spontaneous conception can be observed low concentrations of antimllerian hormone.8 , 9 similarly , in anderson and colleagues study , 3 some pregnancies were observed in women with very low antimllerian hormone levels . 
hence , the best predictor of infertility in cancer survivors remains to be identified . in women with finally , this study raises the crucial issue of discussing the possibility of reducing the risk of premature ovarian insufficiency.1 , 2 preservation of ovarian function ( ie , reducing the risk of chemotherapy - induced premature ovarian insufficiency ) should be distinguished from preservation of fertility ( ie , improving the chances of pregnancy after treatment ) and can be considered of important value also by women without childbearing desire . 
while cryopreservation of gametes is the first option to preserve fertility , the use of temporary ovarian suppression with gonadotropin - releasing hormone agonists during chemotherapy can now be offered for ovarian function preservation in patients with breast cancer , but its efficacy has not yet been shown in patients with hodgkins lymphoma.9 , 10 the results of anderson and colleagues study highlight the importance of discussing access to these options in women older than 35 years , irrespective of chemotherapy type , and among candidates to the beacopp regimen , irrespective of their age . 
very young women undergoing abvd or avd chemotherapy probably do not need to access these options , but they could be proposed later in life if additional treatments are required . results from the ovarian function biomarker analysis ongoing within the ahl 2011 trial ( nct01358747 ) are awaited to provide further evidence on the gonadotoxicity of beacopp chemotherapy in premenopausal women with hodgkins lymphoma . * matteo lambertini , isabelle demeestere breast cancer translational research laboratory , department of medical oncology , institut jules bordet ( ml ) and research laboratory on human reproduction , fertility clinic , cub - hpital erasme ( id ) , universit libre de bruxelles ( ulb ) , brussels 1000 , belgium matteo.lambertini85@gmail.com we declare no competing interests . 
j clin oncol 2013 ; 31 : 23139 . vol 19 october 2018 1265 comment published online september 10 , 2018 s1470 - 2045 ( 18 ) 30579 - 5 see articles page 1338 lambertini m , campbell c , bines j , et al . 
no evidence for the benefit of gonadotropin - releasing hormone agonist in preserving ovarian function and fertility in lymphoma survivors treated with chemotherapy : final long - term report of a prospective randomized trial . 
gonadotropin - releasing hormone agonists during chemotherapy for preservation of ovarian function and fertility in premenopausal patients with early breast cancer : a systematic review and meta - analysis of individual patient - level data . 
 camrelizumab for nasopharyngeal carcinoma : a new hope ? wenfeng fang and colleagues1 report on two phase 1 studies of the programmed cell death - 1 ( pd - 1 ) inhibitor , camrelizumab ( shr - 1210 ) , as a treatment for patients with recurrent or metastatic nasopharyngeal carcinoma . 
 the more interesting findings are the preliminary antitumor activity of camrelizumab in both settings : 31 ( 34% ; 95% ci 2444 ) of 91 patients who received previous treatment achieved an overall response with camrelizumab monotherapy ( two patients had a complete response ) and 20 ( 91% ; 7797 ) of 22 patients with the combination of camrelizumab and chemotherapy as first - line treatment ( one patient had a complete response )  . 
the keynote - 028 study2 showed that seven ( 26% ; 95% ci 111463 ) of 27 patients with previously treated , advanced disease achieved an objective response with pembrolizumab . 
the nci - 9741 trial3 showed that nine ( 205% ; 95% ci 98353 ; one complete repsonse ) of 44 patients with previously treated recurrent or metastatic naso pharyngeal carcinoma international studies achieved an objective response with nivolumab . 
both keynote - 028 and nci - 9741 are including 63% and 822% asian patients , respectively ; whereas the current study by fang and colleagues1 was done in an endemic chinese population . 
the proportion of who type 2 or 3 tumours in keynote - 028 was 667% , 822% in nci - 9742 , and 82% in the camrelizumab monotherapy trial of the current study . 
in terms of patient selection , keynote - 028 only included patients with programmed cell death ligand - 1 ( pd - l1 ) - positive tumours , whereas both nci - 9742 and the current study enrolled patients with unselected histologies . 
in nci - 9742 , 40% of patients had pd - l1 - positive tumours , which was associated with an improved response ( six [ 33% ] of 18 patients ) compared with pd - l1 - negative tumours ( three [ 13% ] of 23 patients )  . 
pd - l1 positivity also appears to be predictive of response to pd - 1 inhibitors in other head and neck squamous cell carcinomas.4 , 5 pd - l1 status was not reported by fang and colleagues in the current study . 
this outcome might suggest that previous priming with ipilimumab could improve the 1266 vol 19 october 2018 comment correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections editorial for more about the mid sta ordshire report see midsta spublicinquiry.com / for more on mortality associations with nursing see jama 2002 ; 288 : 198793 for the article in the washington post see news / to - your - health / wp / 2015 / 06 / 05 / the - nursingshortage - and - the - doctorshortage - are - two - very - di erentthings / for the nursing times editorial see net / opinion / editors - comment / take - action - to - protect - theright - to - strike / 5085431 . article ? blocktitle = editor%27scomment&contentid = 7874 the importance of nurses in cancer care june , 2015 , in early it became apparent that the uk national health service ( nhs ) had spent 33 billion on temporary nurses agency fees in the past nancial year . 
health secretary jeremy hunt ascribed this increased use of agency nurses partly to hospitals response to the report into the mid sta ordshire nhs foundation trust that investigated unacceptably poor levels of care in that regions health - care provision , and showed that this was partly related to chronically low sta ng levels . 
declining numbers of nurses is a global problem , and all the more so given mounting evidence showing that involving nurses in more specialist roles , such as in nurse - led clinics for patients with cancer , improves patient outcomes . 
the upcoming european cancer congress ( vienna , austria ; sept 2529 , 2015 ) has issued a special call for oncology nurses , citing their attendance as a priority for the organising committee , and including oncology nurses in many of their multidisciplinary tumour board discussions . 
an article in the washington post suggested that , in the usa , both baby - boomer nurses and their instructor counterparts in universities are reaching retirement , without an in ux from the next generation . 
the shortage of teaching nurses is especially problematic because without quali ed faculty , those who want to become nurses might be unable to do sothe american association of colleges of nursing found that about two - thirds of us nursing schools had to turn away quali ed applicants because of shortages in teaching sta  . 
the american oncology nursing society has issued a position statement of concern , stating that they believe that the nursing shortage will negatively a ect cancer care , and calling for changes to be made at both an educational and a legislative level . 
aside from the professional burnout that endangers many medical specialists , the nature of nurses work puts them at danger of developing occupational - based hazards such as musco skeletal disorders ( nursing is ranked sixth out of all professions for this risk ) , and contact dermatitis brought about by stringent handwashing measures . 
e orts by nursing unions to increase remuneration are di cult , given that the critical nature of the care that nurses provide makes it hard for unions to engage in industrial action to demand better pay . 
however , some unions have had to resort to such actioneg , nurses in victoria , australia , successfully staged walk - outs in 2012 , winning them a 1421% pay rise from the government . 
an editorial in the nursing times in the uk on june 3 , 2015 , called for nurses to act to protect the right to strike , citing the refusal of the uk government to agree to a 1% pay rise recommended by the nhs pay review body . 
this is partly driven by cost - cutting measureseg , in the uk , although estimates vary , there have been about 6000 permanent nursing posts cut since 2010 and a reduction in the number of nursing training places . 
the abrupt suspension of a national institute for health and care excellence guidance report on safe nurse sta ng levels also shows a lack of value for the work of nursing sta  . 
the fundamental disconnect between the number of nurses leaving the profession versus those entering , and the number needed in patient care versus those that payers wish to underwrite needs urgent resolution . 
as demand for nurses taking specialist roles in cancer car e rises to combat the increasing burden of disease , it is time that nurses critical role in all aspects of patient care is explicitly acknowledged through demonstrable change . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections corrections correction to lancet oncol 2015 ; 16 : 303 correction to lancet oncol 2016 ; 17 : 65 correction to lancet oncol 2016 ; 17 : e8 penson rt , huang hq , wenzel lb , et al . 
lancet oncol 2015 ; 16 : 30111in the 6 months post - cycle 1 section of table 1 of this article , in the received row of the second column ( headed cisplatin and paclitaxel plus bevacizumab ) , the data should have been 66 ( 57% )  . 
 bendamustine plus rituximab versus udarabine plus rituximab for patients with relapsed indolent and mantle - cell lymphomas : a multicentre , randomised , open - label , non - inferiority phase 3 trial . 
 lancet oncol 2016 ; 17 : 5766in this article , on page 65 , paragraph 6 , of the discussion section , reference 3 was incorrectly added to the sentence results of our published study8 in the rst - line setting . 
lancet oncol 2016 ; 17 : e8in paragraph two of this news piece , the percentage of genetic mutations in paediatric should have read 95 ( 85% ) of 1120 patients had genetic mutations in their normal tissue that increased their risk of developing cancer during childhood . 
 this correction has been made to the online version as of dec 22 , 2015 . vol 17 january 2016 corrections published online june 12 , 2015 s1470 - 2045 ( 15 ) 00056 - x correction to lancet oncol 2015 ; 16 : e227 correction to lancet oncol 2015 ; 16 : 738 correction to lancet oncol 2015 ; 16 : 747 schiller jh . 
 antibodies lancet oncol 2015 ; 16 : 73839in this comment , the chemotherapy backbone used in the squire trial was incorrectly referred to as gemcitabine and carboplatin in four instances in the third paragraph ; it should read gemcitabine and cisplat these corrections have been made to the online version as of june 29 , 2015 , and the printed version is correct . torri v , broggini m , garassino mc . 
lancet oncol 2015 ; 16 : 74648the seventh sentence of the nal paragraph of this comment should read : results for leu858arg are still inconclusive because although progression - free survival is higher in patients given all egfr inhibitors versus chemotherapy , overall survival seems to be better with chemotherapy than with afatinib for these patients . 
 this correction has been made to the online version as of june 29 , 2015 , and the printed version is correct . for future lowy dr , herrero r , hildesheim a , for the participants in the iarc / nci workshop on primary endpoints for prophylactic hpv vaccine trial . 
 lancet oncol 2015 ; 16 : e22633 in the panel , in the section on the quadrivalent vaccine for men , the second bullet point should read : approved in the eu by the ema for the prevention of vaccine - type related anal lesions and for the prevention of vaccine - type related genital warts ( ages 9 )  . 
lancet oncol 2015 ; 16 : this news e316in item , the nal two sentences of paragraph 3 read : according to the scale , treatment late - stage egfr - mutated nonsquamous lung cancer with erlotinib provides a gain in progression - free survival ( pfs ) of 85 months ( hazard ratio [ hr ] 016 [ 95% ci 010026 ] ) and an improvement in quality of life compared with carboplatin and gemcitabine , earning an esmo - mcbs score of 4 / 5 . 
in contrast , the same drug when used to treat metas tatic pancreatic cancer provides an overall gain of only 9 days compared with chemotherapy treatment , and had a score of 1 / 5 . 
this correction has been made as of june 12 , 2015 . vol 16 july 2015 e313 catching up on medical device safety after a joint investigation into the global medical devices industry , several media outlets published their findings of the implant files in 2018 . 
elsewhere , non - clinical grade materials continue to be used in breast implants , despite the 2010 pip scandal in which implants were found to be manufactured with unapproved silicone gel and were prone to rupture . 
although reports have now emerged of an alarming association between textured breast implants and the development of breast large - cell implant - associated anaplastic lymphomaa rare form of t - cell lymphoma that can occur in the fibrous scar capsule that forms around breast the underlying causal mechanisms have yet to be defined , early detection of localised disease and complete removal of the implant and capsule can lead to recovery . 
meanwhile , cases of breast implant - associated anaplastic large - cell lymphoma are increasing : 615 cases have been reported worldwide since the first report in 1997 , including 45 cases in the uk , 72 in australia , and 252 in the usa . 
the concern is so great that the french national agency for medicines and health products has recommended that surgeons switch to smooth implants as the link between textured implants and anaplastic large - cell lymphoma is investigated . for any woman undergoing mastectomy to treat breast cancer , the possibility of developing another cancer because of a medical device must be devastating . 
but , as for any medical procedure , blame cannot , and should not , be apportioned to the patient , especially when risks are not adequately recorded and reported , let alone communicated to the patient . 
data for anaplastic largecell lymphoma are scarce , highlighting a wider concern about the worldwide regulation of medical devices . many countries have systems in places for reporting adverse events associated with medical devices . 
however , such systems do not appear to be compulsoryfor example , the uk registry is not mandatory for clinicians and although large - cell lymphoma as a data item , reporting cases is optional . 
how can clinicians be expected to communicate risks to patients or make clinical decisions without accurate and reliable data ? the existing system of passive monitoring of medical device safety clearly needs to be addressed . include anaplastic it does drug safety monitoring could be a good model for the medical device industry and provide more reassurance to doctors and patients alike . 
reporting of clinical trial data on new drugs has improved , and data from robust trials , including full reporting of adverse events , are essential for any drug approval . 
the same stringent data are not needed for medical devices ; for example , in the european economic area , market approval is granted through ce certification , for which clinical trial data are not mandatory . 
similarly , a new eu regulation on medical devices , due to come into force in 2020 , includes key issues of transparency around medical devices and reinforcement of rules of clinical evidence . the steps taken by the fda and the eu are a good start in a long overdue assessment of medical devices , which undoubtedly hold much promise for many patients . 
the ndings paint a bleak picture : demand for mri and ct is expected to increase by at least 9% per year , and use of endoscopy will increase by 44% by 2020 , but sta ng , infrastructure , renewal of old equipment , and nancing is insu cient to meet these future demands . 
and for those patients who do manage to receive a timely diagnosis , access to the best treatments will also be limited : 43 medicines have been removed this year from the controversial , politically motivated cancer drugs fund a ecting 64 cancer indications . 
the so - called postcode lottery to cancer care in the uk is clearly as widespread as ever , despite the existence of the national institute for health and care excellence ( nice ) , set up to speci cally avoid such inequalities . 
is the uks national health service ( nhs ) now fundamentally and irreversibly broken ? cancer survival in the uk has historically lagged behind rates seen in other high - income countries . 
 equally , 5 - year survival for another common malignancy , colon cancer , is 538% in the uk with rates in the usa and germany of 647% and 646% , respectively . 
indeed , similar disparities exist across all common cancers and , despite considerable e orts to rectify this situation in the past 10 years , these wide survival gaps between the uk and other high - income countries stubbornly persist . 
nice recently issued new referral guidelines for general practitioners ( family doctors ) to help improve cancer outcomes by recommending a lower referral threshold to diagnostic services for patients with suspicious symptoms . 
however , given the cruk reports , it is likely that waiting lists to access necessary diagnostic tests will simply grow ever longer along with delays in communicating resultsincreasing patient anxiety and the likelihood of even worse treatment outcomes . to tackle the shortfall in diagnostic services , the cruk reports include 14 action points for improving access to mri and ct ( although there is notable absence of a pet imaging recommendation ) , and 11 recommendations for endoscopy services . 
these recommendations range from better investment and budgeting , strategic planning and recruitment , a reduction in use of agency sta , locums , and overtime in favour of more full - time regular employees , through to improved education and career development , equipment renewal , and better integrated health systems . 
these actions expand on the six strategic priorities outlined on july 19 , 2015 , by the independent cancer taskforce in their report , achieving world - class cancer outcomes : a strategy for england 20152020 . 
on the speci c issue of pet imaging , the independent cancer taskforce notes its importance for radiotherapy planning , but does not discuss the valuable role of pet imaging in treatment monitoring , which is also highly desirable both clinically and economically . so , can the nhs adapt to meet the challenges ahead ? what is clear is just how ill - prepared the nhs is to meet the future demands of e ective oncology services ; that services need to become far more patient - centric ; and the di erences in service provision between the various countries in the uk cause considerable inequalities . 
additionally , much deeper analyses , beyond those done by cruk on diagnostic services , are essential to tease out speci c tactical and truly achievable actions at local , regional , and national levels , along with assigned project teams to deliver the changes needed and implementation of timelines and metrics to monitor changes and their e ects . 
 the lancet oncology vol 16 october 2015 1273 corrections correction to lancet oncol 2011 ; 12 : 1051 correction to lancet oncol 2015 ; 16 : 634 , 637 histological sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
 independent lancet oncol 2011 ; 12 : 104552 in the discussion of this article , the second sentence of the fth paragraph should read the proportion of patients a ected by grade 34 fatigue in this study ( 7% ) is similar to that reported for trabectedin ( 78% ) or gemcitabine with docetaxel ( 16% ) .12 , 13 this correction has been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 388 kang hj , loftus s , taylor a , dicristina c , green s , zwaan cm . 
 lancet oncol 2015 ; 16 : 38594 in table 2 of the article , the dose ( mg / kg ) of dexamethasone used in the aprepitant group should read 008 ( 002019 )  . 
this correction has been made to the online version as of aug 31 , 2015 . of medical a airs , from april , 2006 , to december , 2012 , during the design and conduct of the stars trial . 
these cor rections have been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 96778 valle jw , wasan h , lopes a , et al . 
lancet oncol 2015 ; 16 : 96778 in gure 3 of the appendix of this article , parts a and b were mislabelled ; part a shows overall survival data and part b shows progression - free survival data . 
the appendix has been corrected as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 1127 moss sm , wale c , smith r , evans a , cuckle h , duffy sw . 
lancet oncol 2015 ; 16 : 112332in the fourth paragraph of the results section of this article , the absolute mortality reduction in the intervention group should read 003 per 1000 womenyears . 
this correction has been made to the online version as of aug 31 , 2015 and the printed version is correct . chang jy , senan s , paul ma , et al . 
lancet oncol 2015 ; 16 : 63037in this article , the role of the funding source should read : this analysis was designed by the principal and coprincipal investigators of both trials . 
for the stars protocol , accuray speci ed that the cyberknife platform was the sole platform to be used for the study , but did not have a role in any other aspect of the study design . 
beyond providing nancial support , neither funder was in accessing involved the raw data , collection , analysis , or interpretation of the data , or writing of the report . 
dab has received grants from accuray , and is the co - owner of berry consultants , a company that designs clinical trials for pharmaceutical and medical device companies , and international healthcare consortia . 
od was an employee of accuray , as senior vice - president responses vol 16 september 2015 e427 correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections corrections correction to lancet oncol 2014 ; 15 : 856 correction to lancet oncol 2015 ; 16 : 60 , 61 ledermann j , harter p , gourley c , et al . 
lancet oncol 2014 ; 15 : 85261 in this article , the second sentence of the rst paragraph of the results section should read on the basis local germline brca mutation testing reported on case report forms , germline brca mutation status was known for 98 ( 37% ) of 265 patients ( 50 [ 37% ] of 136 in the olaparib group vs 48 [ 37% ] of 129 in the placebo group )  . 
this correction has been made to the online version as of march 30 , 2015 . a multi - centre , topp ms , gckbuget n , stein as , et al . 
lancet oncol 2015 ; 16 : 5766in table 2 of this article , the mrd response during rst two cycles in patients with cr or crh row should not have been indented , and should have been the last row in the table . 
maturitas 2012 ; 72 : 5660 . join us at the lancet clinic on oct 5 , 2015 , we launch the rst 45 disease - speci c pages of a major new online initiative involving all lancet journals that will bring together an overview seminar and relevant reviews , clinical series , commissions , research , case reports , and clinical pictures . 
over the next 18 months or so when the lancet clinic is complete , there will be online pages for 135 diseases , which we have identi ed by a combination of global burden of disease data and clinical practice needs . 
we hope that the lancet clinic will help practising doctors make better informed decisions that ultimately lead to better lives of people worldwide , and help others who want to educate or update themselves keep abreast of the evolving evidence base . 
individual clinical editors will pull together newly published material from across the lancet journals and post links to these on the page regularly . in addition , we are continuing our regular editorial policies of commissioning more specialised clinical reviews and series across the lancet group to provide a more focused and in - depth assessment for key diseases . 
in 2014 , the lancet published the rst clinical commission on liver disease in the uk and in february , 2015 , we launched our rst clinical campaign based on this amant f , coosemans a , debiec - rychter , timmerman d , vergote i . 
can gray - scale and color doppler sonography di erentiate between uterine leiomyosarcoma and leiomyoma ? j clin ultrasound 2007 ; 35 : 44957 . brlmann h , tanos v , grimbizis g , et al , for the european society of gynaecological endoscopy ( esge ) steering committee on broid morcellation . 
further clinical commissions on asthma , hypertension , dementia , tuberculosis , traumatic brain chronic obstructive pulmonary disease , and others are underway across all lancet with these clinical commissions and campaigns , we hope to extend our goal to publish the best science for better lives to being an active partner in using this science for actual change . 
the lancet clinic invites you to be part of this endeavour . * sabine kleinert , richard horton , elena becker - barroso , niall boyce , david collingridge , justine davies , emma grainger , peter hayward , john mcconnell , zo mullan , lan - lan smith the lancet , london ec2y 5as , uk ( sk , rh ) ; the lancet neurology , london , uk ( eb - b ) ; the lancet psychiatry , london , uk ( nb ) ; the lancet oncology , london , uk ( dc ) ; the lancet diabetes & endocrinology , london , uk ( jd ) ; the lancet respiratory medicine , london , uk ( eg ) ; the lancet hiv , london , uk ( ph ) ; the lancet infectious diseases , london , uk ( jm ) ; the lancet global health , london , uk ( zm ) ; and the lancet haematology , london , uk ( l - ls ) sabine.kleinert@lancet.com copyright kleinert et al . 
open access article distributed under the terms of cc by . 1456 vol 16 november 2015 correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections the results of this study3 support the benefit of lenalidomide maintenance across different subgroups of patients and highlights the progression - free survival benefit in patients with high - risk cytogenetic abnormalities . 
however , it is important to note that lenalidomide did not overcome the poor prognosis that the presence of high - risk abnormalities confer to patients , and therefore novel treatments to improve the outcomes of these patients are needed . whether all patients need continuous maintenance therapy regardless of the quality of the response achieved with previous treatments remains unclear . 
however , next - generation sequencing and cytometry provide an opportunity to investigate the role of minimal residual disease assessment for tailoring maintenance strategies and would allow physicians to prescribe maintenance therapy and reply to a very common question raised by the patients : how many cycles of treatment does maintenance therapy include ? furthermore , long - term minimal residual disease monitoring could guide preemptive treatment preventing clinical relapses and ensuring durable responses . maintenance with lenalidomide is the standard of care , but the future has to move towards a personalised medicine approach that aims to improve overall survival and quality of life , which means giving the right drug to the right patient at the right time for the optimal duration . * mara - victoria mateos , vernica gonzlez de la calle hematology department , university hospital of salamanca , ibsal , salamanca , spain mvmateos@usal.es m - vm has received honoraria for lectures from janssen , celgene , takeda , and amgen , and for participation in advisory boards from janssen , celgene , takeda , amgen , abbvie , glaxosmithkilne , and pharmamar . 
n engl j med 2018 ; 378 : 51828 . the importance of surgery in colorectal cancer treatment in the lancet oncology , sara benitez majano and colleagues1 have engaged with a very important topic . 
 previous data have indicated poorer treatment results for colorectal cancer in both denmark and england compared with those in similar western countries.2 the continuous audit and assessment of outcomes is important to better understand the reality of cancer care each country and thus , this study is of interest to the public . majano and colleagues identified that an important difference between the countries studied regarding surgery for colorectal cancer was probably not the technique , but rather the frequency of surgical resection . 
 the proportion of patients treated with resectional surgery ranged from 684% in england to 813% in sweden for colon cancer , and from 599% in england to 708% in sweden for rectal cancer ; this range was wider for patients older than 75 years ( colon cancer 597% to 809% ; rectal cancer 457% to 619% )  . 
it is possible that attitudes towards surgery in the older patient population should be altered in england , but the data in this study do not include comorbidity , and the risk for increased perioperative mortality should not be underestimated . 
 preoperative optimisation of patients must be a focus of research , to increase the percentage of patients that are able to undergo resectional surgery in the future . what other factors could be influencing these results ? during the study period , the standardised referral pathway had already been introduced in denmark in 2010 . 
there is scarce vol 20 january 2019 published online december 10 , 2018 s1470 - 2045 ( 18 ) 30679 - x see articles page 74 comment scientific evidence that a standardised referral pathway improves survival . introduced another preoperative difference between the countries studied was colorectal cancer screening . 
perhaps the effect of screening was seen in rectal cancer , where diagnoses of stage i to iii disease were more common in england than in the other countries , but , unfortunately , this effect was not reflected in improved survival . benitez majano and colleagues study shows that the previously reported2 poorer treatment results for denmark than those for norway and sweden have improved , particularly for rectal cancer . 
perhaps this change is due to the increased use of surgical resections for rectal cancer , but the authors also suggest that improved results could be partly attributed to laparoscopic surgery , which has been shown to be safe in the long term and confers short - term advantages in the management of colorectal cancer.35 during the study period , laparoscopic surgery for rectal cancer was very differently implemented countries , with denmark having 75% of patients operated with laparoscopic technique compared with about 20% of patients in sweden , according to national quality registry data . 
taken all together , it is unlikely that laparoscopic surgery is the main reason for the improved survival in patients with rectal cancer in denmark shown in this study . four the another surgical difference that was less emphasised in guidelines in england than in recommendations from the other countries in this study was complete mesocolic excision . 
in stockholm , where the technique has been introduced in a structured manner , only about 20% of patients undergoing surgery for colon cancer between 2004 and 2012 had complete mesocolic excision.8 similar data have been published from denmark.9 nonetheless , it is interesting that recommendations for england are less specific than other countries guidelines ; does this in fact result in poorer survival because of unspecified surgical treatment ? future research must focus on including data on patient frailty and comorbidity , which should be added to registry data , as majano and colleagues have suggested . 
 the facilitation of easier interpretation and comparison of data from several national registries must also be a concern for policy makers , because benchmarking of results and making comparisons between countries might help to identify important new areas to improve survival in patients with colorectal cancer . eva angenete department of surgery , institute of clinical sciences , sahlgrenska academy at university of gothenburg , sahlgrenska university hospital / stra , scandinavian surgical outcomes research group , 413 45 gothenburg , sweden eva.angenete@vgregion.se i declare no competing interests . copyright 2018 the author ( s )  . 
lancet oncol 2015 ; 16 : 16168 . vol 20 january 2019 comment correction to lancet oncol 2017 ; 18 : e31529 correction to lancet oncol 2017 ; 18 : 150211 weller m , van den bent m , tonn jc , et al . 
 lancet oncol 2017 ; 18 : e31529in the panel of this review ( published online first on may 5 , 2017 ) , the dose of bevacizumab should be 10 mg / kg . 
the corrections have been made to the online version as of oct 31 , 2017 , and the printed version is correct . vol 18 november 2017 e642 corrections correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections correction to lancet oncol 2017 ; 18 : e35463 correction to lancet oncol 2018 ; 19 : 87100 correction to lancet oncol 2018 ; 19 : 25766 oconnor oa , lue jk , sawas a , et al . 
 for lancet oncol 2017 ; 18 : e35463 in this review , the second sentence of the abstract should read additional improvements have been reported in three phase 3 colon cancer trials when oxaliplatin was added to fluoropyrimidines , the effect was mainly on disease - free survival . 
this correction has been made to the online version as of feb 28 , 2018 although women fulvestrant johnston s , lee ks , et di leo a , al . 
buparlisib plus with postmenopausal her2hormone - receptor - positive , negative , advanced breast cancer progressing on or after mtor inhibition ( belle - 3 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
in the results section , the following sentence should have read in the 11 ( 13% ) cases of discordance , a pik3ca wild - type tumour sample and pik3ca - mutated ctdna were reported in three ( 4% ) patients and pik3ca mutations detected in the tumour sample but not in ctdna ( 9% ) patients . 
these corrections have been made to the online version as of feb 28 , 2018 . seven vol 19 march 2018 e137 corrections correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
 this correction has been made to the online version as of jan 31 , 2018 . vol 19 february 2018 corrections lancet oncol 2018 ; 19 : 2739 published online december 11 , 2017 s1470 - 2045 ( 17 ) 30777 - 5 see comment page 2 * full list of members in the appendix ( pp 1924 ) or at research / ebctcg correspondence to : ebctcg secretariat , medical research council population health research unit , nuffield department of population health , oxford ox3 7lf , uk bc.overview@ndph.ox.ac.uk see online for appendix long - term outcomes for neoadjuvant versus adjuvant chemotherapy in early breast cancer : meta - analysis of individual patient data from ten randomised trials early breast cancer trialists collaborative group ( ebctcg ) * summary background neoadjuvant chemotherapy ( nact ) for early breast cancer can make breast - conserving surgery more feasible and might be more likely to eradicate micrometastatic disease than might the same chemotherapy given after surgery . 
we investigated the long - term benefits and risks of nact and the influence of tumour characteristics on outcome with a collaborative meta - analysis of individual patient data from relevant randomised trials . methods we obtained information about prerandomisation tumour characteristics , clinical tumour response , surgery , recurrence , and mortality for 4756 women in ten randomised trials in early breast cancer that began before 2005 and compared nact with the same chemotherapy given postoperatively . 
analyses by intention - to - treat used standard regression ( for response and frequency of breast - conserving therapy ) and log - rank methods ( for recurrence and mortality )  . findings patients entered the trials from 1983 to 2002 and median follow - up was 9 years ( iqr 514 ) , with the last follow - up in 2013 . 
patients allocated nact had an increased frequency of breast - conserving therapy ( 1504 [ 65% ] of 2320 treated with nact vs 1135 [ 49% ] of 2318 treated with adjuvant chemotherapy )  . 
nact was associated with more frequent local recurrence than was adjuvant chemotherapy : the 15 year local recurrence was 214% for nact versus 159% for adjuvant chemotherapy ( 55% increase [ 95% ci 2486 ] ; rate ratio 137 [ 95% ci 117161 ] ; p = 00001 )  . 
no significant difference between nact and adjuvant chemotherapy was noted for distant recurrence ( 15 year risk 382% for nact vs 380% for adjuvant chemotherapy ; rate ratio 102 [ 95% ci 092114 ] ; p = 066 ) , breast cancer mortality ( 344% vs 337% ; 106 [ 095118 ] ; p = 031 ) , or death from any cause ( 409% vs 412% ; 104 [ 094115 ] ; p = 045 )  . interpretation tumours downsized by nact might have higher local recurrence after breast - conserving therapy than might tumours of the same dimensions in women who have not received nact . 
strategies to mitigate the increased local recurrence after breast - conserving therapy in tumours downsized by nact should be consideredeg , careful tumour localisation , detailed pathological assessment , and appropriate radiotherapy . funding cancer research uk , british heart foundation , uk medical research council , and uk department of health . copyright the author ( s )  . 
nact was subsequently extended to operable ( early ) breast cancer , mainly to allow breast - conserving surgery , and is now widely used , particularly for large tumours.24 furthermore , nact might be somewhat more likely to eradicate than might chemotherapy micrometastatic disease delayed until after surgery . nact might mitigate the hypo thesised stimulatory effect of surgery on occult disease5 and reduce tumour cell shedding during surgery . 
nact might also provide useful in - vivo information about the chemosensitivity of the local ( and , by implication , disseminated ) tumour to different chemotherapy regimens , helping to guide subsequent drug selection.6 , 7 conversely , by delaying surgery , nact might increase the risk of metastatic spread , particularly for chemoresistant tumours . several randomised trials817 have compared nact with the same chemotherapy given postoperatively . 
in certain trials , 14 , 15 some good responders to nact did not receive surgery , and high frequencies of local recurrence with nact in these trials have been attributed to omission of definitive local therapy . 
any such differences in the extent of surgery confound vol 19 january 2018 articles research in context evidence before this study the early breast cancer trialists collaborative groups ongoing extensive searches of bibliographic databases , including medline , embase , the cochrane library , and meeting abstracts up to march 2017 , identified 16 trials that compared neoadjuvant chemotherapy ( nact ) with the same chemotherapy postoperatively . 
hence , women allocated nact retained more breast tissue than did those allocated adjuvant chemotherapy , and higher local recurrence frequencies in some neoadjuvant trials than in others have been attributed to omission of definitive local therapy . 
this individual patient data meta - analysis , involving 4756 women in ten trials , found that the frequencies of clinical response and breast - conserving therapy were higher for smaller , higher - grade , and oestrogen receptor - negative and progesterone receptor - negative tumours , and for one trial using anthracycline and taxane chemotherapy . 
although responders to nact had lower distant recurrence and breast cancer mortality than did non - responders , when responders and non - responders were combined , distant recurrence and breast cancer mortality were similar for nact and adjuvant chemotherapy . 
local recurrence was , however , higher with nact than with adjuvant chemotherapy , which persisted for 10 years after treatment and was not confined to trials in which surgery could be omitted after response to nact . 
 however , nact is associated with higher local recurrence than adjuvant chemotherapy , which could be at least partly explained by wider use of breast - conserving therapy after nact than with postoperative chemotherapy . 
strategies to mitigate the increased local recurrence after breast - conserving therapy in tumours downsized by nact should be consideredeg , careful tumour localisation , detailed pathological assessment , and appropriate radiotherapy . comparisons of the efficacy of nact with that of adjuvant chemotherapy.18 , 19 another complication is that investigations of the influence of tumour characteristics on outcome need to use prerandomisation data , as analyses by postsurgical characteristics would be substantially biased by downstaging.20 to investigate such issues in more detail than was possible in reviews18 , 19 of published data , we did a patient - level meta - analysis of the trials that directly compared any nact regimen with the same regimen begun postoperatively . methods study design and participants we sought data from all randomised trials in early ( ie , operable ) breast cancer that began before 2005 and compared nact with the same chemotherapy begun after surgery ( ie , standard adjuvant chemotherapy )  . 
trial identification and data checking were as reported previously22 , 23 and the preferred reporting items for conformed systematic review and meta - analyses ( individual patient data ) .24 for every woman , we requested information from the trials principal investigator or another appropriate member of their research group about patient and tumour characteristics , treatments , dates of any local recurrence ( breast , chest wall , or regional nodes ) , distant recurrence , contralateral breast or other second primary cancer , and date last known to be alive or date and underlying cause of death . 
patient - level data for radiotherapy were unavailable . ( complete response statistical analysis a detailed description of the statistical methods has been previously published.22 primary outcomes assessed were tumour response [ no clinical evidence of disease after nact ] , partial response [ 50% reduction in initial size ] , or stable or progressive disease [ < 50% reduction , no change , or increased tumour size ] ) , extent of local therapy ( mastectomy , lumpectomy [ either with or without radiotherapy ] , and radiotherapy alone ) , local and distant recurrence , breast cancer death ( via subtraction of the log - rank statistics of death without recurrence from those of overall survival23 ) , and overall for more on trial identification and data checking see research / ebctcg / prisma - ipdstatement - for - ebctcg.pdf vol 19 january 2018 articles for data access procedures see about / data - access - policy mortality ( death from any cause )  . 
analyses were by intention to treat and are of first isolated local recurrence ( site not generally available ) , any distant recurrence ( irrespective of previous local or contralateral recurrence ) , breast cancer mortality , and all - cause mortality . 
 a statistic on one degree of freedom ( ) for testing of whether some quantity q differs significantly from zero is given by q / var ( q )  . 
a test ( on n1 degrees of freedom ) for heterogeneity can be obtained by subtracting ( oe ) / v from the sum of the separate values , one per stratum , of ( oe ) / v . 
for analyses by regression , we estimated rrs by maximum likelihood ; tests for trend and heterogeneity were by likelihood ratio . associations between baseline variables and outcome used prerandomisation values . 
subgroup analyses compare outcomes in trials in which all women allocated nact were , or were not , scheduled to receive breast surgery and in women whose initially planned local treatment was mastectomy or breast - conserving therapy ( lumpectomy with or without radiotherapy or radiotherapy alone )  . 
the writing committee had final responsibility for the decision to submit for publication . results individual patient data were available from ten817 of 16 eligible trials identified and from 4756 ( 91% ) of the 5250 women in total ( table 1 , appendix pp 2 , 6 , 17 )  . 
trial entry year for participants was 19832002 , median follow - up was 9 years ( iqr 514 ) , with the last follow - up in 2013 , and median age was 49 years ( 4357 )  . 
of the 4756 women included in the analysis , 3838 ( 81% ) were in trials of regimens that included an anthracycline , one of which ( 902 women ) also gave a taxane.13 four trials ( 918 women ) used mmm ( mitoxantrone , methotrexate , and mitomycin - c ) 11 , 12 or cmf ( cyclophosphamide , methotrexate , and fluorouracil ) 8 , 17 as nact ; in these trials , some chemotherapy in those allocated nact was women ( n ) deaths ( n ) median years per woman ( iqr ) no anthracycline or taxane8 , 11 , 12 , 17 anthracycline , no taxane9 , 10 , 1416 anthracycline and taxane13 total 2936 4756 1163 1604 70 ( 4293 ) 102 ( 49154 ) 79 ( 50107 ) 86 ( 48137 ) trials ( n ) * woman - years by years since entry ( thousands ) 1019 total 221 346 < 01 298 437 * data are missing for six small trials that randomised about 500 women , so they were not included in this analysis ( appendix p 17 )  . 
in these trials , women allocated to the neoadjuvant group completed their chemotherapy after surgery . table 1 : trials of neoadjuvant versus adjuvant chemotherapy that began by 2005 vol 19 january 2018 articles given after surgery ( table 1 , appendix pp 34 )  . 
the incidence of local recurrence was significantly higher with nact than with adjuvant chemotherapy in years 04 ( rr 135 [ 95% ci 111164 ] ; p = 0003 ) and 59 ( 153 [ 108217 ] ; p = 002 ) , with few local recurrences after year 10 . 
sensitivity analyses indicated no substantial influence of competing risks from other breast events on the rrs for local recurrence ( appendix p 18 )  . as anticipated , 18 , 19 the absolute increase in 10 - year local recurrence with nact was largest in the two trials14 , 15 in which , after nact , many women did not have breast surgery ( 133% [ 95% ci 55211 ] ; 337% for nact vs 204% for adjuvant chemotherapy ; rr 162 [ 95% ci 120219 ] , p = 0002 ; figure 3b )  . 
however , the rrs for local recurrence in these two sets of trials were not significantly different ( heterogeneity p = 019 )  . between - trial rrs for local recurrence ranged from 067 ( 95% ci 024191 ) to 459 ( 119178 ) , but this apparent heterogeneity was not significant ( 10 = 118 ; p = 030 ; figure 4a )  . 
rrs for local recurrence also did not differ significantly between the three classes of chemotherapy used in these trials ( figure 4 , appendix p 13 ) , between trials in which chemotherapy in the nact group was or was not completed after local therapy ( appendix p 13 ) , or between use or not of tamoxifen ( figure 5 , appendix p 13 )  . we noted no significant differences between nact and adjuvant treatment in 15 year distant recurrence ( 382% for nact vs 380% for adjuvant chemotherapy ; rr 102 [ 95% ci 092114 ] ; p = 066 ) , breast cancer death ( 344% vs 337% ; 106 [ 095118 ] ; p = 031 ) , or death from any cause ( 409% vs 412% ; 104 [ 094115 ] ; p = 045 ; figure 2b , c , d )  . 
the rrs for these three outcomes did not differ significantly between any subgroups of trials , including those for which use of surgery was or was not dependent on response to nact , those using different types of chemotherapy , or those using or not using tamoxifen ( figure 3 cf and figure 4b , appendix pp 7 , 13 )  . 
 three trials8 , 9 , 16 collected only first recurrence and death rather than all events ; however , sensitivity analyses omitting these trials had no material effect on distant recurrence estimates ( appendix p 18 )  . 
mortality from causes other than breast cancer was no different between the nact chemotherapy groups ( appendix p 7 )  . adjuvant and information about clinical tumour response was available for 1947 ( 82% ) of 2387 patients allocated nact ; 546 ( 28% ) of 1947 had a complete response , 803 ( 41% ) of 1947 had a partial response , and 598 ( 31% ) of 1947 had stable or progressive disease ( table 2 , appendix p 8 )  . 
 poorly differentiated than with well or tumours moderately differentiated tumours ( trend p = 0001 , even after allowance for high - grade tumours tending to be er negative ) , and was higher in the one trial13 that combined anthracycline and taxane therapy than in the other trials ( p < 00001 )  . 
age , nodal status , and planned local therapy did not affect response . the proportion of women having breast - conserving therapy in various different subgroups in the nact and adjuvant chemotherapy groups are shown in figure 1 . 
 the strongest predictors of the effect of nact on breast conservation frequency were tumour size , planned local therapy , and type of chemotherapy ( all p < 00001 )  . 
the effect of nact on surgery de - escalation was most apparent among women with large ( 2049 mm or 50 mm ) tumours ; we noted little effect of nact on breast conservation frequency in women with small ( < 20 mm ) tumours . 
 * includes institut bergoni bordeaux14 ( in nact group , 33% had radiotherapy alone ) and institut curie s615 ( in nact group , 51% had radiotherapy alone ; in adjuvant chemotherapy group , 46% had radiotherapy alone ) trials . 
however , although the rr for local recurrence among all women planned to have a mastectomy was 166 ( 95% ci 124221 ) compared with 114 for women with lumpectomy planned , the two - tailed test for heterogeneity was not significant ( p = 007 ; figure 5 , appendix pp 11 , 12 )  . ( 086152 ) heterogeneity between the rrs for local recurrence was lower across all other tumour characteristics than it was for rrs in the subgroup by planned local therapy ( figure 5 ) ; although the p value for the trend in rr with biopsy grade was 005 , this p value could have been a chance finding given that it was the most extreme from many subgroup analyses . 
despite surgery de - escalation being more common in larger tumours than in smaller tumours , and in the trial combining anthracycline and taxane13 than in trials of other regimens , the proportional increases in local recurrence did not vary significantly by tumour size or chemotherapy regimen ( figure 5 )  . 
 patient - level data for radiotherapy were not available , and trial - level data for radiotherapy intent and practice were incomplete ( appendix p 2 ) , so the effect of radiotherapy on local recurrence cannot be studied . 
radiotherapy was scheduled for most women who had breast - conserving surgery and actual use of radiotherapy was more frequent in the nact than in the adjuvant therapy groups ( appendix p 2 )  . 
the rrs for distant recurrence and breast cancer mortality did not vary by any tumour factor measured , type of chemotherapy , timing of chemotherapy use in the nact group , type of planned local therapy , or period of follow - up ( appendix p 13 )  . lower substantially as expected , distant recurrence and breast cancer complete mortality were responders than in non - responders ( appendix p 14 )  . 
ordering of trials by the percentage of patients with a complete clinical response to nact did not reveal any significant trend of improved recurrence or breast cancer mortality rrs in trials with a higher frequency of response ( appendix p 16 )  . 
no patterns emerged between trials in complete response when considering the year that the trial started or the frequency of breast - conserving therapy within a trial ( appendix p 15 )  . discussion in early breast cancer , high frequencies of complete or partial clinical response can be achieved with nact , which can lead to a higher frequency of breast - conserving therapy than with adjuvant chemotherapy . 
reassuringly , the increase in local recurrence was not associated with any significant increase in distant recurrence or breast cancer mortality . more than two thirds of patients receiving nact responded , with more than a quarter achieving complete clinical response , despite some trials using old chemotherapy regimens and four administering some of the chemotherapy postoperatively . 
within trials , response was more common in women with small , er - negative and progesterone receptor - negative , or high - grade tumours , as measured before randomisation , but was little affected by age , nodal status , or planned local therapy.817 as expected , use of nact was associated with an increase in the use of breast - conserving therapy . an increase in the use of breast - conserving therapy in women who responded well to nact and who would otherwise have had mastectomy is a likely explanation for the increase in local recurrence in patients allocated nact . 
as anticipated , 18 , 19 the absolute increase in local recurrence was greatest in the two trials14 , 15 in which surgery could be avoided completely in the event of a complete clinical response to nact . 
this apparent heterogeneity of effect was , however , not significant , and nact appeared to also have resulted in some increase in local recurrence in the aggregated results from the eight other trials . 
differing use of radiotherapy or axillary surgery in the nact group might also have contributed to local recurrence , although patient - level the higher information about this factor was not available . 
trial reports indicate that radiotherapy was scheduled for most women who had breast - conserving surgery and that actual use of radiotherapy was , if anything , more frequent in the nact than in the adjuvant therapy groups . 
indeed , even with radiotherapy , local failure is higher after breast - conserving surgery than after mastectomy without radiotherapy.30 our finding of an overall increase in local recurrence in the trials using optimal local treatment is at odds with a meta - analysis18 based on published data rather than individual patient data , but this discrepancy could be because the meta - analysis included comparisons that were confounded by differing background systemic therapy . is predictive of tumour response lower distant recurrence and death than an absence of tumour response . 
 compared with all women randomly allocated to adjuvant chemotherapy , outcomes were better for those with a complete clinical response after nact than for those with a partial response and far better than for those with little or no response to nact . 
 this finding could be because tumour characteristics that are associated with higher responsesuch as smaller tumour sizeare also associated with lower distant recurrence and are balanced between the nact and adjuvant groups by random isation . 
the ctneobc study6 reported similar findings in that efficacy as assessed by high pathological complete response at the trial level did not correlate well with long - term efficacy . a limitation of our meta - analysis is that we have not been able to assess reliably whether presurgical systemic therapy is more effective at eradicating micrometastatic disease than the same chemotherapy administered after recovery from surgery because of the confounding vol 19 january 2018 articles local recurrences prevented.30 the effect of differences in the extent of surgery between women allocated nact and those allocated adjuvant chemotherapy . 
at present , we cannot exclude the possibility that nact does moderately reduce distant recurrence compared with the same chemotherapy given postoperatively , but that this benefit was obscured by an increase in local recurrence due to less extensive surgery after nact than in patients who did not receive nact . 
trials of radiotherapy after surgery indicate that substantially decreasing local recurrence does also decrease breast cancer mortality , with about one breast cancer death prevented for every four small , non - significant excess of breast cancer mortality in patients allocated nact is consistent with this risk ratio , so could therefore be due to the increase in local recurrence , but it could equally well be a chance finding . the main aim of nact in contemporary practice is to reduce the extent of breast surgery , thereby making breast conservation feasible in women who would otherwise need mastectomy . 
in the time since the trials in this meta - analysis were done , pathology reporting , surgery , and radiotherapy have improved , and more effective systemic neoadjuvant regimens have been introduced than were available when these trials took place . 
but , although improvements in treatment mean local recurrence risk should be lower than in these trials , our findings indicate that tumours downsized by nact might continue to be associated with higher local recurrence risk after breast - conserving surgery than might tumours of the same dimensions in women who have not received nact . 
strategies to mitigate local recurrence after breast - conserving therapy in tumours downsized by nact should be consideredfor example , careful tumour localisation , detailed pathological assessment , and appropriate radiotherapy.31 prospective randomised trials would also help to establish the optimal clinical management in this context . increased the nact allows more breast - conserving therapy than does adjuvant chemotherapy and provides information about an individual patients response to a particular chemotherapy regimen . 
however , it appears to be no better than postoperative adjuvant treatment at reducing breast cancer mortality and , perhaps as a consequence of a reduction of the extent of surgery , nact is associated with moderately increased local recurrence risk , which persists for at least 10 years . p mcgale , r gray , and r peto designed and carried out the analyses with computing assistance from y wang and z wang . 
 * ebctcg secretariat , population health research unit . declaration of interests the writing committee and ebctcg secretariat declare no competing interests . acknowledgments this study is supported by core funding to the population health research unit and clinical trial service unit , nuffield department of population health , university of oxford , from cancer research uk , the british heart foundation , and the uk medical research council , as well as by the uk department of health grant rrx108 and cancer research uk grant c8225 / a21133 . 
the chief acknowledgement is to the women in these trials and the trial personnel . contributors the ebctcg secretariat ( c boddington , r bradley , j burrett , m clarke , c davies , l davies , d dodwell , f duane , v evans , l gettins , j godwin , r gray , s james , h liu , z liu , e mackinnon , g mannu , p mcgale , t mchugh , p morris , h pan , r peto , s read , c taylor , y wang , and z wang ) identified trials , obtained datasets , and had full access to the rubens rd , sexton s , tong d , winter pj , knight rk , hayward jl . 
cancer 2015 ; 121 : 254452 . surgical treatment and survival from colorectal cancer in denmark , england , norway , and sweden : a population - based study sara benitez majano , chiara di girolamo , bernard rachet , camille maringe , marianne grnlie guren , bengt glimelius , lene hjerrild iversen , edrun andrea schnell , kristina lundqvist , jane christensen , melanie morris , michel p coleman , sarah walters summary background survival from colorectal cancer has been shown to be lower in denmark and england than in comparable high - income countries . 
we used data from national colorectal cancer registries to assess whether differences in the proportion of patients receiving resectional surgery could contribute to international differences in colorectal cancer survival . methods in this population - based study , we collected data from all patients aged 1899 years diagnosed with primary , invasive , colorectal adenocarcinoma from jan 1 , 2010 , to dec 31 , 2012 , in denmark , england , norway , and sweden , from national colo rectal cancer registries . 
we used logistic regression to predict the resectional surgery status patients would have had if they had been treated as in the best performing country , given their individual characteristics . findings we extracted registry data for 139 457 adult patients with invasive colorectal adenocarcinoma : 12 958 patients in denmark , 97 466 in england , 11 450 in norway , and 17 583 in sweden . 
3 - year colon cancer survival was lower in england ( 639% , 95% ci 635643 ) and denmark ( 657% , 647668 ) than in norway ( 695% , 684705 ) and sweden ( 721% , 712730 )  . 
rectal cancer survival was lower in england ( 697% , 691703 ) than in the other three countries ( denmark 725% , 711740 ; sweden 741% , 727754 ; and norway 750% , 731768 )  . 
3 - year survival after stage ii or iii rectal cancer and stage iv colon cancer was consistently lower in england ( stage ii rectal cancer 864% , 95% ci 850876 ; stage iii rectal cancer 755% , 742767 ; and stage iv colon cancer 205% , 199211 ) than in norway ( 941% , 915960 ; 834% , 801861 ; and 330% , 310351 ) and sweden ( 929% , 908946 ; 806% , 782827 ; and 237% , 220253 )  . 
3 - year survival after stage ii rectal cancer and stage iv colon cancer was also lower in england than in denmark ( stage ii rectal cancer 912% , 888931 ; and stage iv colon cancer 235% , 219251 )  . 
the total proportion of patients treated with resectional surgery ranged from 47 803 ( 684% ) of 69 867 patients in england to 9582 ( 813% ) of 11 786 in sweden for colon cancer , and from 16 544 ( 599% ) of 27 599 in england to 4106 ( 708% ) of 5797 in sweden for rectal cancer . 
this range was widest for patients older than 75 years ( colon cancer 19 078 [ 597% ] of 31 946 patients in england to 4429 [ 809% ] of 5474 in sweden ; rectal cancer 4663 [ 457% ] of 10 195 in england to 1342 [ 619% ] of 2169 in sweden ) , and the proportion of patients treated with resectional surgery was consistently lowest in england . 
in the hypothetical scenario where all patients were treated as in sweden , given their age , sex , and disease stage , the largest increase in resectional surgery would be for patients with stage iii rectal cancer in england ( increasing from 703% to 882% )  . interpretation survival from colon cancer and rectal cancer in england and colon cancer in denmark was lower than in norway and sweden . 
differences in patient selection for surgery , especially in patients older than 75 years or individuals with advanced disease , might partly explain these differences in international colorectal cancer survival . funding early diagnosis policy research grant from cancer research uk ( c7923 / a18348 )  . copyright 2018 the author ( s )  . 
 analysts who did this research pointed to the need for research into differences in stage - specific treatment between these countries . added value of this study we used national population - based clinical data to compare stage - specific survival of patients diagnosed with primary colorectal adenocarcinoma in denmark , england , norway , and sweden between 2010 and 2012 , and to assess whether the international survival differences could be explained by differences in patient care . 
we showed that net survival up to 3 years after colon cancer was substantially lower in england and denmark than in norway and sweden , and survival from rectal cancer was lower in england than in the other three countries . 
we also found a steep declining age gradient in the probability of receiving resectional surgery in england , which was less noticeable or not evident in the other countries . implications of all the available evidence these findings have important policy implications , showing that the colorectal cancer survival deficit in england can be attributed partly to shortfalls in treatment . 
we highlight the need for more patient data on comorbidities , frailty , and additional therapies to understand these differences better . the primary treatment for colorectal cancer is surgical removal of the main tumour or tumours and affected tissues . 
total mesorectal excision became the standard surgery for rectal cancer in denmark , norway , and sweden in the mid - 1990s68 and some years later in england.9 this technique entails the removal of the rectum and surrounding tissues , including lymph nodes and fascia , 10 and requires particular surgical training and skills to secure good results . 
the surgical principle of resection in the embryological plane , which is used in mesorectal excision , was later applied to colon cancer surgery , with favourable results in terms of recurrences and survival.11 , 12 preoperative ( neo - adjuvant ) or postoperative ( adjuvant ) radiotherapy or chemotherapy can be used to reduce the risk of recurrence and treat micrometastases.13 , 14 the decision to treat patients with colorectal cancer with neo - adjuvant or adjuvant therapy depends on the extent of disease and risk of recurrence . 
in general , clinical guide lines do not recommend additional therapy for early - stage colon tumours or rectal tumours treated with surgery with adequate resection margins.1315 the use of neo - adjuvant or adjuvant therapy for stage ii or iii tumours is variable betweenand within16countries , particularly for rectal tumours.17 we used population - based data from national colorectal cancer registries to estimate stage - specific and age - standardised net survival at 3 years of patients diagnosed with colorectal cancer in denmark , england , norway , and sweden , and to compare the proportions of patients receiving resectional surgery in those countries by patient and tumour characteristics . methods study design and data sources in this population - based study , we included all patients aged 1899 years diagnosed with primary , invasive colorectal adenocarcinomas from jan 1 , 2010 , dec 31 , 2012 . 
patients diagnosed by their death certification alone and patients with records with invalid date sequences were excluded.18 in denmark , england , and norway , we extracted data from population - based national cancer registries . 
by linking individual patient records in denmark to the danish colorectal cancer group database , 19 additional clinical information was available for 11 746 ( 907% ) patients registered with colorectal adenocarcino mas in the danish national cancer registry . 
similarly , 97 185 ( 997% ) english national cancer registry records for patients with colorectal cancer were linked to at least one of the national bowel cancer audit data , hospital episode statistics inpatient and outpatient records , and the cancer waiting times monitoring data set . 
norwegian national cancer registry data are routinely linked to the norwegian colorectal cancer registry , a specialised registry that contains detailed clinical infor mation on all patients with colorectal cancer nationwide.8 the swedish vol 20 january 2019 for more on the danish colorectal cancer group see for the national bowel cancer audit see org.uk / for the hospital episode statistics see digital.nhs.uk / data - andinformation / data - tools - andservices / data - services / hospital - episode - statistics for the cancer waiting times monitoring data set see information / data - collectionsand - data - sets / data - collections / cancerwaitingtimescwt for the norwegian colorectal cancer registry see registries / clinical - registries / colorectal - cancer - registry / articles for more on the swedish colorectal cancer registry see samverkan / cancerdiagnoser / tjocktarm - andtarm - och - anal / tjock - - och - andtarm / kvalitetsregister / see online for appendix colorectal cancer registry provided clinical data on patients with colorectal cancer in sweden ; 7 its coverage for the study period was near complete.20 definitions of clinical variables ( site , stage , or treatment ) were agreed with in - country clinicians and specialised cancer registry staff to reconcile differences in coding between the various data sources . 
some further discussions with clinicians and registry staff were held to understand and reconcile differences in coding and clinical practices in those countries . all patients included in this study were followed up from time of diagnosis until death or until dec 31 , 2014 , whichever occurred first . 
tumours with morphological codes for non - adenocarcinoma were excluded from analyses . we applied consistent quality control measures to all records ( appendix pp 12 ) .18 in cases of multiple tumours diagnosed at the same site within 6 months of each other , we retained the date of diagnosis of the first tumour ; where stage and type of surgery were inconsistent between records ( n = 327 , 023% ) , we selected the most advanced stage and most extensive surgery . 
for all patients with record of more than one surgery , we selected the most extensive surgery . disease extent ( stage ) , as defined by the union for international cancer control tnm classification of malignant tumours , was characterised by applying a hierarchical algorithm previously described.22 priority was given to pathological confirmation of tumour , lymph node extension , and distant metastases ( if positive ) , over clinical tnm components . 
there is broad comparability between the main stage categories among these tnm editions.22 we defined resectional surgery as the surgical removal of the primary tumour , irrespective of the intent and outcome of surgery , done within 9 months of diagnosis . 
in denmark and england , surgical status was categorised as missing when patients were registered in the national cancer registry but were not recorded in the specialised colorectal cancer registry ( or in hospital episode statistics for england )  . 
we calculated the potential range of the proportion of patients that might have had resectional surgery in denmark and england , first assuming that all patients with missing data were treated and then assuming that they were all untreated . 
we then estimated upper and lower limits of the probable distribution of resectional surgery in each of these countries . information regarding radiotherapy and planned chemo therapy within 6 months of diagnosis was extracted from colorectal cancer registry data in denmark , norway , and sweden , and from national bowel cancer audit and cancer waiting times records in england . we hold approvals from the uk health research authority ( reference ecc 304 ( i ) / 2011 ) , the national health service research ethics service ( 11 / lo / 0331 ) , and the london school of hygiene & tropical medicine ( lshtm , 12171 )  . 
we have a data proces sing agreement with the danish cancer society and approval from the danish data protection agency to use data from the danish colorectal cancer group ; a data disclosure agreement with the cancer registry of norway to use the norwegian data ; and ethical approval from the regional ethical committee in uppsala to use the swedish data . 
data were extracted and transferred with a standard data structure protocol and file transmission procedure , in line with the concord programme for the global surveillance of cancer survival.24 outcomes our primary aim was to assess the estimated agestandardised net survival up to 3 years after diagnosis by country and disease stage and the estimated probability of patients receiving resectional surgery by stage and age in each country . 
we also estimated the hypothetical change in the probability of receiving resectional surgery that patients would have had if they had been treated as in the best performing country , given their individual characteristics . statistical analysis we compared the demographic and clinical characteristics of patients with colorectal cancer diagnosed in denmark , england , norway , and sweden , including patients age , sex , and disease stage . 
received within 6 months of diagnosis ; sources and completeness of information on chemotherapy or radiotherapy varied greatly between countries , with a high proportion of missing information in england . 
 table 1 : characteristics of patients diagnosed with colorectal adenocarcinoma , 201012 information on the cause of death , ( background mortality ) and is suitable for use in international comparisons of survival because background mortality differs between countries . 
in the absence of reliable the background mortality hazard was provided by life tables for the general population defined by country , sex , single year of age , and year.26 we used a multivariable modelling approach to estimate the excess mortality hazard ( ie , due to colorectal cancer ) and predict net survival . 
we used a model selection strategy to test for non - linearity and time dependence of the effects of sex and age on the excess mortality hazard and their interactions.27 survival was predicted by age group , defined by the international cancer survival standard . 
we used international cancer survival standard weights to produce a weighted average of the survival estimates ( age - standardisation ) , to allow for differences between countries in the age distribution of the population of patients with cancer.28 we used the stata command strcs to fit flexible parametric survival models on the log - hazard scale.29 we used multivariate logistic regression models to compare the probability of receiving resectional surgery between countries . 
subsequently , we applied the model coefficients of the best performing country to individuals from the other countries , to assess the hypothetical change in the probability of receiving resectional surgery if patients had been treated as in the best performing country , given their observed characteristics . 
the corresponding author had full access to all the data in the study , and the final responsibility for the decision to submit for publication . results we included information from 139 457 patients diagnosed with colorectal adenocarcinoma in england , denmark , norway , and sweden in our analyses . 
in patients with known disease stage , the proportion diagnosed with stage iiii colon cancer was higher in sweden than in england , vol 20 january 2019 articles norway , and denmark ; for rectal cancer , the proportion diagnosed with stage iiii rectal cancer was higher in england than in sweden , denmark , and norway ( table 1 )  . 3 - year age - standardised net survival from colon cancer was higher in sweden and norway than in denmark and england . 
3 - year survival from rectal cancer was generally similar between denmark , norway , and sweden , and lower in england ( table 2 )  . net survival decreased with the increase in disease stage ( table 2 , figure 1 )  . 
3 - year survival for patients with stage ii tumours was about 90% or higher in all countries , although survival for patients with rectal or colon cancer in england and colon cancer in denmark was notably lower than for patients in sweden or norway . 
 although generally higher than 75% , survival for patients with stage iii colon and rectal cancer was lower in england than in norway and sweden up to 3 years after diagnosis , and in denmark 1 year after diagnosis . 
resectional surgery defined as surgery to remove the primary tumour within 9 months of diagnosis , excluding diagnostic and palliative procedures . table 3 : proportion of patients diagnosed with colorectal adenocarcinoma in 201012 that received resectional surgery by age , sex , and disease stage 205% for england and 330% for norway at 3 years . 
for stage iv rectal cancer , survival was lowest in sweden and england ( 267% in sweden and 271% in england ) and highest in norway ( 385% ) at 3 years ( figure 1 )  . the overall proportion of patients who received resectional surgery was higher for colon than for rectal cancer in all countries ( table 1 )  . 
we could not establish the surgical status of some patients in denmark because they were not registered in the danish colorectal cancer group database ( 949 [ 111% ] of 8567 patients with colon cancer and 263 [ 60% ] of 4391 patients with rectal cancer )  . 
patients with colorectal cancer who were not registered in the danish colorectal cancer group database were more likely to have advanced stage disease or missing stage information and be slightly older than patients registered in the database . 
data on surgery were unavailable for 03% of patients with colorectal cancer in england because their national cancer registry records could not be linked to the additional databases ( hospital episode statistics , national bowel cancer audit , or cancer waiting times )  . 
the proportion of patients receiving resectional surgery was highest in sweden and lowest in england , for both types of cancer ( table 1 )  . in younger patients the proportion of patients treated with resectional surgery was lower in individuals aged 75 years or older than in each country , and international differences in resectional surgery use widened with increasing age of patients ( table 3 )  . 
the share of patients aged 75 years or older with colon cancer with evidence of resectional surgery varied from 19 078 ( 597% ) of 31 946 patients in england to 4429 ( 809% ) of 5474 in sweden . 
in patients aged 75 years or older with rectal cancer , the share of those with resectional surgery varied from 4663 ( 457% ) of 10 195 patients in england to 1342 ( 619% ) of 2169 in sweden . 
for rectal cancer , norway and sweden had the highest proportions of resectional surgery for all but the youngest age group , where denmark had the highest proportion of patients treated . 
england had the lowest proportion of patients treated with resectional surgery for rectal cancer in all age groups and for colon cancer in the two oldest age groups ( table 3 )  . to account for differences in disease stage distribution , we examined the proportion of patients treated by stage and age group ( figure 2 )  . 
the proportion of patients with colon cancer with evidence of resectional surgery for each stage and age group was mostly similar between the four countries for stages i and ii and in patients aged 75 years or younger . 
 however , we observed a steep decline in the proportion of patients that had surgical treatment in the older age categories in england for each disease stage and for both types of cancer , which was not evident in the other countries ( figure 2 )  . 
for instance , a higher proportion of patients received resectional surgery for stage i colon tumours in the 7584 age group than in the 85 and older age group in all countries , but the absolute difference between these age groups was 180% in england vol 20 january 2019 articles compared with 2955% in the other countries . 
information on surgery was missing for some patients in denmark and for a small proportion of patients in england : light grey areas represent the proportion of patients with unknown surgical status by stage and age group ; overall height of the bars shows the proportion of patients that would receive surgery if all patients with missing treatment data had surgical treatment . vol 20 january 2019 articles denmark england norway sweden * colon : stage i colon : stage ii colon : stage iii colon : stage iv rectum : stage i rectum : stage ii rectum : stage iii rectum : stage iv being treated with resectional surgery in any of the four countries . 
however , for patients with rectal cancer diagnosed with stage iiiiv disease , the proportion treated was lower in england than in the other countries in our study , particularly in the oldest age groups ( figure 2 )  . 
we observed an age gradient in the proportion of patients receiving resectional surgery with all rectal cancer stages in denmark , england , and sweden , with lower proportions among patients aged 85 years or older than among younger patients . 
for instance , between patients aged 7584 years and those aged 85 years or older , the absolute difference in the proportion of patients who received resectional surgery for stage iii rectal tumours was 296% in england , 209% in sweden , and 128% in denmark . 
we found no age gradient in the proportion of patients treated for rectal cancer in norway , except for patients with stage iv cancer . to assess the validity of our findings and check whether the age differences in the likelihood of patients receiving resectional surgery were driven by differences in the management of patients diagnosed at aged 90 years or older , we repeated the analyses with exclusion of this patient group . 
the patterns we observed persisted in this reanalysis ( appendix pp 3 , 67 )  . overall , sweden had the highest survival for colon and rectal cancer and the highest proportion of patients receiving resectional surgery , compared with those of the other countries ( although outcomes in norway were generally similar , or better in specific strata , to those in sweden )  . 
to highlight any groups of patients who might be at a disadvantage in the likelihood of receiving resectional surgery compared with patients in other countries , we applied the coefficients for sweden to data from the other three countries and interpreted it as the probability of a patient receiving resectional surgery if they had been treated as in sweden , given their observed age , sex , and disease stage . 
the number of events per parameter was above the recommended threshold of ten in all categories , 31 at 100 events per parameter for our most complex model in the category with fewest events ( stage iv rectal cancer )  . in this hypothetical scenario , changes in the proportion of patients with stage i colon or rectal cancer receiving resectional surgery would be minor ( figure 3 )  . 
in england , denmark , and norway there would be a higher proportion treated among patients with stage ii and iii colon and rectal cancer , if treated as in sweden . 
overall , the largest improvements in the proportion of patients receiving resectional surgery would be seen in patients with stage ii ( from 789% to 907% ) or iii ( from 703% to 882% ) rectal cancer in england . 
the proportion of patients receiving resectional surgery for stage iv colon cancer in denmark and england would increase ( from 391% to 511% in denmark and from 400% to 498% in england ) whereas in norway , the proportion would decrease ( from 556% to 499% ) if patients had been figure 3 : predicted probability of receiving resectional surgery by patient characteristics ( age and sex ) and tumour characteristics ( stage at diagnosis ) error bars are 95% ci . 
 * predicted probabilities of patients receiving resectional surgery by applying the coefficients of the swedish logistic model to the cohorts of patients in each country , on the basis of the country - specific distributions of patient characteristics . 
the overall height of the bars shows the proportion we would observe if all patients with missing treatment data had received surgery . among patients younger than 85 years with rectal cancer who were diagnosed with stage i or ii disease , we observed no significant differences in the likelihood of vol 20 january 2019 articles treated as in sweden . 
the hypothetical decrease in the proportion of stage iv patients receiving surgery in norway would be even larger for rectal cancer ( from 474% to 288% )  . patients with missing disease stage were slightly older than the mean age for each country and cancer type ( range 753773 years for colon cancer and 745754 years for rectal cancer )  . 
the proportion of patients with colon cancer without known disease stage who had evidence of having resectional surgery was lower than that of any known stage category in each country and higher in england than in the other three countries ( table 3 )  . 
additionally , survival of these patients was higher than that of patients with known stage iii disease and lower than that of patients with known stage iv disease , in all four countries ( table 2 )  . discussion in this study , to understand the mechanisms underlying international differences in cancer outcomes , we compared the characteristics of patients diagnosed with colorectal adenocarcinoma in denmark , england , norway , and sweden . 
we provide updated figures of up to 3 - year net survival in these countries , and our results support previous findings of lower survival for patients in england and , to a lesser degree , in denmark , than in sweden or norway.25 our results also support findings that denmark seems to be closing the survival gap with sweden and norway , particularly for rectal cancer.4 , 6 , 24 in the stagespecific analyses , we noted no significant differences between countries in survival for patients diagnosed with early stage ( i or ii ) colorectal adenocarcinomas , but wider international survival differences in patients with more advanced disease stages ( iii or iv )  . 
additional information on treatment , available from specialised colorectal cancer registries , helped us to understand these survival differences better . cancer survival is largely determined by receipt of potentially curative treatment , which , in the case of colorectal cancer , is primarily surgery . 
treatment options mainly depend on disease stage and the underlying health status of patients , which is determined by their comorbidities , frailty , and age . clinical guidelines for cancer treatment aim to standardise and assure adequate cancer care for a population . 
 the amount of detail in the national clinical guidelines regarding colorectal cancer management varied , with recom mendations from england being generally less specific than guidelines from denmark , norway , and sweden.14 , 15 , 32 , 33 nonetheless , indications for surgery were largely consistent between these countries , especially for rectal tumours . 
treatment guidelines for colon cancer in denmark , norway , and sweden explicitly recommend the removal of the part of the bowel that contains the tumour and its mesentery ( and en - bloc resection , if the visceral fascia is compromised because of ingrowth of the tumour into neighbouring organs ) .13 , 14 , 32 by contrast , english guidelines recognise mesorectal excision as the standard surgery for most rectal tumours but do not explicitly recommend the corresponding procedure ( dissection in the embryological plane ) for colon tumours.15 none of the guidelines for the countries in our study mentions age as an exclusion criterion for receiving surgical treatment . 
older patients ( aged 75 years or older with stage iiiv rectal cancer or stage iv colon cancer and aged 85 years or older for the other stages of rectal and colon cancer ) in england had a lower probability of receiving resectional surgery than patients of a similar age with similar disease extension in the other three countries , and a lower probability than younger patients in england . 
england had the steepest negative age gradient in the proportion of patients receiving resectional surgery and had a survival deficit in comparison with the other three countries , particularly for rectal cancer . 
conversely , we noted a higher proportion of patients younger than 85 years who were diagnosed with stage i or ii tumours who had evidence of resectional surgery in england than in the other three countries . 
of the countries studied , only england had a colorectal cancer screening programme with national coverage during the study period.34 the diagnosis and treatment of asymptomatic disease through screening might explain the high proportion of patients surgically treated for early stage disease in the eligible age group in england . 
in the other countries in our study , screening was not imple mented at national level during the study period34 and could not have affected the disease stage distribution or population - based survival . although less aggressive treatment for older patients might sometimes be justified because of comorbidity or frailty , concerns have been raised that some of the disparities in age - related cancer care in england arise because of clinical decision making on the basis of chronological age.35 a 2011 report36 showed lower resection rates in older patients with cancer in england during 200406 than those of younger patients , with less than 2% of patients aged 80 years or older having a major resection surgery for six of 13 cancers examined . although an increase in the proportion of patients receiving resectional surgery does not necessarily translate into better short - term survival because aggressive treatment might be associated with high short - term vol 20 january 2019 articles that mortality , our findings suggest international differences in survival are , at least in part , determined by differences in patient selection practices for surgical treatment . 
choices in management of older patients with colorectal cancer might greatly affect populationbased survival because the mean age at diagnosis is about 70 years.37 patients in countries with a greater proportion of patients treated with surgery and better short - term fewer complications survival might also have more access to laparoscopic surgery or better postoperative care than in the other countries . 
although there is conflicting evidence about the long - term benefit of a laparoscopic versus an open surgical approach for rectal cancer , 38 , 39 laparoscopic surgery is associated with lower perioperative mortality and surgery.40 , 41 in denmark , the increasing use of laparoscopic surgery for colorectal cancer has been associated with a reduction in perioperative mortality rates.42 differences between countries in the use of this approach might explain some of the differences in the proportion of patients receiving surgical treatment and , potentially , in survival . 
however , we were not able to account for this information in our analysis because not all datasets had sufficiently complete data for this question . than open our study has some limitations . 
these include core variables that have previously been examined for comparability and validated in these and other european colorectal cancer registries.43 however , some residual data quality issues might affect the comparability of results . 
performance status scales , which are commonly used to assess patients general condition ( such as their degree of independence ) and eligibility for specific treatments , 44 might not be ideal for older patients with cancer , especially those with mul tiple comorbidities.45 although comprehensive geriatric assessment scales have been proposed and validated , 45 they are rarely used , documented , or routinely collected.46 nevertheless , at the population level , the burden of cardiovascular disease the most common contra indication for surgeryis similar in the four countries included in our study.47 population - based all - cause mortality and life expectancy in older ages are also similar in these four countries ( appendix p 4 ) , supporting the validity of the findings in our study . the overall proportion of patients with unknown disease stage is notably higher in england than in denmark , norway , and sweden . 
the reasons for stage information to be missing are likely to differ according to how high or low the proportion of unknown stage is and , therefore , probably differ between countries . 
patients with unknown disease stage had a lower probability of receiving resectional surgery than patients with known stage , and had similar survival to that of patients with advanced disease stages . 
therefore , our complete - case analysis might overestimate stage - specific survival and the proportion of patients receiving resectional surgery in england , and provides a conservative estimate of the disparities between england and the other three countries in our study . in denmark , 93% of patients were not registered in the danish colorectal cancer group database and thus , their treatment status remained undetermined . 
by contrast with the danish national cancer registry , the danish colorectal cancer group database only includes adults with a first - time diagnosis of colorectal adenocarcinoma treated in danish public hospitals who were in contact with a surgical department.19 therefore , we calculated a potential range of the proportion of patients that might have had resectional surgery and estimated upper and lower limits of the probable distribution of resectional surgery in denmark . 
because of the danish colorectal cancer group databases exclusion criteria and the stage distribution of patients without a danish colorectal cancer group database record , it is probable that a substantial number of these patients did not undergo resectional surgery . 
assuming that none of these patients received resectional surgery , the proportion of patients with rectal cancer who received resectional surgery was still higher in denmark than in england and similar to that in sweden for most combinations of age and disease stage . 
nevertheless , these missing data might have masked some age and stage trends in the likelihood of patients undergoing resectional surgery , especially for colon cancer . we were not able to ascertain treatment intent , residual disease status , venous invasion status , or postoperative complications in patients who received resectional surgery . 
systematic differences in the distribution of such patients between these four countries , or differences in their perioperative management , might affect the between - country comparability of these results . 
 further more , patients with non - resectable tumours in better - performing countries might be more likely to be offered other treatment ( such as treatment to prolong life or make tumours amenable to resection ) than patients in worse - performing countries . 
for example , clinical the guidelines importance of neo - adjuvant or conversion treatment of metastatic tumours to render them resectable , 13 , 14 whereas guidelines in england prioritise symptom control and state that initial systemic treatment followed by surgery should be considered only if both primary and metastatic in norway and sweden describe vol 20 january 2019 articles tumours are judged to be resectable.15 moreover , in countries that frequently use neo - adjuvant therapy with delayed surgery for rectal cancer , the resulting downstaging could cause an under estimation of the differences in stage - specific survival when these countries are compared with settings where neo - adjuvant treatment is more variable or followed by immediate surgery . the completeness and granularity of the data collected by the colorectal cancer registries regarding chemotherapy and radiotherapy varied greatly during the study periodfrom complete registration of radiotherapy protocols in norway and sweden to a high proportion of missing information in england . 
adjuvant chemotherapy is associated with improved outcomes in stage iii colon cancer and is used universally , but for stage ii colon cancer and rectal cancer ( in general ) its value and therefore its use have been more variable.4850 neo - adjuvant radiotherapy decreases recur rence rates , but evidence for its effect on survival is conflicting and so use also varies within countries16 , 51 and between countries.17 the use of targeted therapy in com bination with chemotherapy might help to make tumours amenable to resection in some patients with metastatic or locally advanced disease , 52 but no survival benefit has been shown for this combination.53 for patients with metastatic disease treated with non - curative intent , optimal use of systemic therapy contributes to longer survival.52 , 54 variability between countries in the use of these additional therapies , and other differences in oncological care beyond surgery , might also contribute to the observed differences in survival . despite the limitations of the data included in our study , we have identified important international differences in the distribution of resectional surgery by age and disease stage . 
the main data quality issue ( the higher proportion of patients with unknown disease stage in england ) is likely to have led to a conservative estimate of the differences found in stage - specific survival outcomes in england compared with those of other countries . 
we noted that differences in survival between patients with colorectal cancer treated in england , denmark , norway , and sweden tended to increase with time after diagnosis , and it is possible that these differences between countries would widen with longer follow - up . changes in practice during and after the study period are likely to affect future trends . 
over the past two or three decades , colorectal cancer outcomes have improved in all the countries compared in our study.3 , 24 , 55 the centralisation and specialisation of colorectal cancer surgery have been suggested as important drivers of this improvement.4 a 2012 cochrane review56 found a clear association between operative mortality and 5 - year survival with hospital and surgeon caseload and specialisation . 
however , it is likely that centralisation and specialisation vary between the four countries in our study , and these changes in practice are also likely to affect patient survival differently in these countries.4 , 6 expedited referral routes were initiated in england and denmark in the 2000s , in response to low cancer survival related to system delays.57 , 58 similar rapid referral routes were introduced in norway and sweden in 2016 , following the danish experience . 
although diagnostic delays are important factors in cancer care , the effect of these referral routes on cancer survival remains uncertain . in denmark , a nationwide screening programme with a monitoring database was introduced in 2014.59 the norwegian directorate of health is planning to introduce a national colorectal cancer screening programme in norway in 2019 , offering a faecal immunochemical test or colonoscopy to individuals when they turn 55 years.60 similarly , a national colorectal cancer screening programme is due to be implemented in sweden in 2019 , following regional screening programmes.61 in england , a one - off screening test with flexible sigmoidoscopy for people aged 55 years is being rolled out.62 with increases in diagnosis and treatment of asymptomatic disease , it is likely that survival and the proportion of patients treated for early stage disease will increase in the future . since 2013 , surgeon - specific outcomes have been reported annually as quality measures in england.63 it is hoped that this increase in accountability will lead to improvements in patient care . 
the major reorganisation of the nhs in 2013 , 64 alongside sub stantial resource constraints in the nhs65 in the past decade , has had a potentially negative effect on cancer services . 
for instance , the 62 - day treat ment waiting time targetthe aim that a patient should wait no more than 2 months from the date that the hospital receives an urgent referral for suspected cancer to the start of their treatmenthas been missed for several quarters running , showing that services are unable to meet the demands placed on them.66 given the ongoing financial pressures and austerity in the uk and the nhs , the future trends in survival for patients with cancer in england are uncertain . our findings have important policy implications , suggesting that the colorectal cancer survival deficit in england as compared with denmark , norway , and sweden can be attributed partly to shortfalls in provision of surgical treatment . 
we showed that older patients in england , in particular , were less likely to receive resectional surgery than patients with similar characteristics in the other countries in our study . 
we posit that increases in the proportion of patients receiving resectional surgery might translate into better longer - term outcomes in england , provided that adequate postoperative care is also available . improving the capture of information on patients with colorectal cancer in specialised clinical registries , vol 20 january 2019 articles including data from individuals who are not eligible for surgery , would allow a more complete population - based comparison of colorectal cancer outcomes . 
complete and comparable data on comorbidities , frailty , and additional therapies are required to improve understanding of international differences and inequalities in cancer outcomes . contributors sw , br , mpc , and sbm designed the study . 
 jc and lhi ( denmark ) , sbm and cdg ( england ) , eas and mgg ( norway ) , and kl and bg ( sweden ) prepared national datasets according to the protocol . 
all authors had access to results at the data preparation and analysis stages , contributed to the interpretation of the results , revised and critically reviewed the manuscript , and approved the submitted version . 
sbm , cdg , sw , br , and mpc had access to all the data in the study and take responsibility for its integrity and the accuracy of the analyses . declaration of interests br reports grants from the uk department of health , outside the submitted work . 
all other authors declare no competing interests . acknowledgments this study was funded by an early diagnosis policy research grant from cancer research uk to the cancer policy programme at the london school of hygiene & tropical medicine ( lshtm ; award number c7923 / a18348 )  . 
we thank the national colorectal cancer registries in denmark , england , norway , and sweden for their sustained efforts in collecting data for patients with colorectal cancer to the highest quality standards . 
we are grateful for advice received from members of the cancer policy programme scientific advisory group ( peter sasieni , deborah ashby , paul aylin , andrew roddam , and sally vernon )  . 
we gratefully acknowledge the advice and support of members of the lshtm cancer survival group ( csg ) , especially yuki alencar ( csg coordinator ) , francisco javier rubio ( statistician ) , and adrian turculet ( csg data manager )  . correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections corrections correction to lancet oncol 2014 ; 15 : 1189 correction to lancet oncol 2014 ; 15 : 1263 dahut wl , madan ra . 
lancet oncol 2014 ; 15 : 118890in this comment , the fourth sentence of the third paragraph should read response in addition assessment was confounded because follow - up imaging was done at the discretion of the treating clinician . 
 this correction has been made to the online version as of oct 27 , 2014 . to safety , cn , prostate castellano sternberg daugaard g , et al , for the abiraterone global eap investigators . 
we investigated whether 3 months of oxaliplatin - containing chemotherapy would be non - inferior to the usual 6 months of treatment . methods the scot study was an international , randomised , phase 3 , non - inferiority trial done at 244 centres . 
 patients aged 18 years or older with high - risk stage ii and stage iii colorectal cancer underwent central randomisation with minimisation for centre , choice of regimen , sex , disease site , n stage , t stage , and the starting dose of capecitabine . 
this trial is registered with isrctn , number isrctn59757862 , and follow - up is continuing . findings 6088 patients underwent randomisation between march 27 , 2008 , and nov 29 , 2013 . 
nine patients in the 3 month group and 14 patients in the 6 month group did not consent for their data to be used , leaving 3035 patients in the 3 month group and 3030 patients in the 6 month group for the intention - to - treat analyses . 
at the cutoff date for analysis , there had been 1482 disease - free survival events , with 740 in the 3 month group and 742 in the 6 month group . 
3 year disease - free survival was 767% ( 95% ci 751782 ) for the 3 month group and 771% ( 756786 ) for the 6 month group , giving a hazard ratio of 1006 ( 09091114 , test for non - inferiority p = 0012 ) , significantly below the non - inferiority marg peripheral neuropathy of grade 2 or worse was more common in the 6 month group ( 237 [ 58% ] of 409 patients for the subset with safety data ) than in the 3 month group ( 103 [ 25% ] of 420 ) and was long - lasting and associated with worse quality of life . 
1098 serious adverse events were reported ( 492 reports in the 3 month group and 606 reports in the 6 month group ) and 32 treatment - related deaths occurred ( 16 in each group )  . interpretation in the whole study population , 3 months of oxaliplatin - containing adjuvant chemotherapy was noninferior to 6 months of the same therapy for patients with high - risk stage ii and stage iii colorectal cancer and was associated with reduced toxicity and improved quality of life . 
despite the fact the study was underpowered , these data suggest that a shorter duration leads to similar survival outcomes with better quality of life and thus might represent a new standard of care . 
the scot study was designed to test for the non - inferiority of 3 months of treatment compared with the standard 6 month duration . added value of this study worldwide , six studies have addressed this research question , of which scot is the largest . 
peripheral neuropathy was significantly worse in the 6 month group and reducing the treatment duration to 3 months more than halved the number of grade 3 or 4 peripheral neuropathy events reported . 
moreover those patients who were most severely affected by peripheral neuropathy also had a significant reduction in quality of life . implications of all the available evidence in view of the results of the scot study and the meta - analysis of all six worldwide studies conducted by the idea collaboration , 3 months of adjuvant chemotherapy will become the new global standard of adjuvant treatment for most patients who are suitable for treatment with capox , particularly those patients with t13 , n1 disease . the major cumulative chronic toxic effect of oxaliplatincontaining chemotherapy is sensory peripheral neuropathy , which can be disabling . 
this effect is recognised to be dependent on dose and duration and can be long - lasting.8 , 9 as most patients undergoing adjuvant chemotherapy are cured and will survive , long - term , irreversible peripheral neuropathy is a significant issue . the current standard duration of adjuvant chemo therapy for colorectal cancer is 6 months . 
a shorter duration of adjuvant chemotherapy would be expected to result in less chronic peripheral neuropathy , but it has been hitherto unknown to what , if any , extent cutting duration would compromise its efficacy . 
the results of one study10 using fluoropyrimidine alone , which was not powered for non - inferiority , suggested that 3 months of infused fluoropyrimidine was similar to 6 months of bolus fluoropyrimidine treatment in terms of disease - free survival.10 the scot study was designed as a stand - alone international phase 3 non - inferiority study to investigate whether 3 months of oxaliplatin - based adjuvant chemotherapy for colorectal cancer is non - inferior to 6 months of treatment with the same regimen . 
here we report the final efficacy results of disease - free survival and the toxicity and quality - of - life ( qol ) results . methods study design and participants the scot study is an international , randomised , nonblinded , non - inferiority , phase 3 trial comparing 6 months versus 3 months of oxaliplatin and fluoropyrimidine adjuvant chemotherapy in patients with high - risk stage ii or stage iii colorectal cancer . 
patients were recruited from 244 centres in six countries ( the uk , denmark , spain , sweden , australia , and new zealand )  . patients were eligible if they were aged 18 years or older and had undergone a curative resection for stage iii or high - risk stage ii ( defined as having one or more of t4 disease , tumour obstruction with or without perforation of the primary tumour preoperatively , fewer than ten lymph nodes harvested , poorly differentiated histology , perineural invasion , or extramural venous or lymphatic vascular invasion ) adenocarcinoma of the colon or rectupatients were enrolled within 11 weeks of surgery and started treatment on their allocated study group within 2 weeks of randomisation . 
other eligibility inclusion requirements included who performance status 0 or 1 , adequate organ function , and life expectancy of greater than 5 years with reference to noncancer related diseases . 
patients had to have a normal ct scan of the chest , abdomen , and pelvis before study enrolment and carcinoembryonic antigen less than 12 times the local upper limit of normal ( uln ) within 1 week before randomisation . 
exclusion criteria included chemotherapy ( except chemotherapy administered with curative intent that was completed > 5 years ago and from which there were no residual complications ) , previous long - course chemo radiotherapy ( preoperative short - course radiotherapy alone was allowed ) , moderate or severe renal impair ment ( glomerular filtration rate or creatinine clearance < 30 ml / min , as calculated with the cockcroftgault equation ) , haemoglobin less than 9 g / dl , absolute neutrophil count less than 15 10 cells per l , platelet count less than 100 10 cells per l , and aspartate aminotransferase or alanine aminotransferase greater than 25 times the uln . 
this study was approved by the west glasgow research ethics committee ( version 1.1 of the protocol ) on jan 21 , 2008 , and all subsequent amendments approved by the committee , where required ( rec reference number 07 / s0703 / 136 )  . 
 randomisation and masking by use of a minimisation algorithm incorporating a random component , patients were centrally randomly assigned ( 1 : 1 ) , to receive either 3 months or 6 months of treatment . 
the minimisation factors were centre , choice of regimen , sex , disease site ( colon vs rectum ) , n stage ( x , 0 , 1 , or 2 ) and t stage ( x , 0 , 1 , 2 , 3 , or 4 ) and , if the patient was going to receive the capox ( capecitabine and oxaliplatin ) regimen , the starting dose of capecitabine ( from feb 1 , 2010 )  . initially some participating centres were randomly allocated to randomise patients after completion of the first 3 months of treatment to either receive a further 3 months treatment or to stop treatment . 
this approach was stopped because of a poorer randomisation rate ( ie , fewer patients randomised per month ) compared with centres that randomised patients before the start of treatment.11 participants were enrolled by authorised clinicians , after obtaining patient consent , by contacting the cancer research uk clinical trials unit in glasgow , uk , to check eligibility and request an allocation . 
 the study was open - label for patients , clinicians , and those doing the data analysis . procedures patients were assigned to receive oxaliplatin - containing adjuvant treatment for either 3 months or 6 months . 
 the chemotherapy regimen , which could be folfox ( bolus and infused fluorouracil with oxaliplatin ) or capox , was chosen by the physician and patient and was not randomised . for patients receiving folfox , treatment was given every 2 weeks with the intention of delivering six cycles to patients assigned 3 months of therapy and 12 cycles to patients assigned 6 months of therapy . 
intravenous oxaliplatin 85 mg / m was given over 2 h on day one concurrently with l - folinic acid 175 mg or folinic acid ( leucovorin ) 350 mg . 
this was followed by an intravenous bolus injection of fluorouracil 400 mg / m over 5 min , then a continuous intravenous infusion of fluorouracil 2400 mg / m over 46 h . 
at the investigators discretion , patients receiving folfox who were older than 70 years could start on the bolus and continuous infusion of fluorouracil at 75% of the starting dose , if clinically indicated . for patients receiving capox , treatment was given every 3 weeks with an intention of delivering four cycles to patients assigned 3 months of therapy and eight cycles to patients assigned 6 months of therapy . 
patients older than 70 years could be considered for treatment with capecitabine at 75% of the full dose , but the decision to reduce dose was left to the discretion of the investigator , depending on the fitness of the individual patient . 
if the clinician felt that any other patient required a - priori dose reduction because of any other comorbidity , that patient could be started on a minimum starting dose of oral capecitabine 800 mg / m twice per day . 
 toxicity was assessed by the investigators after each cycle of chemotherapy treatment and graded by use of national cancer institute common terminology criteria for adverse events ( ctcae ) version three . 
for capox , if more than one delay or a delay of at least 2 weeks occurred , capecitabine and oxaliplatin doses were reduced by 25% and , if further delays occurred due to myelotoxicity , further dose reductions were allowed at the investigators discretion . 
for folfox , if more than one delay or a delay of at least 2 weeks occurred , doses of oxaliplatin and infused fluorouracil were maintained , but the bolus fluorouracil was omitted and , if further delays occurred due to myelotoxicity , the oxaliplatin and infusional fluorouracil doses were reduced by 25% . 
 also for folfox , if after the first cycle neutrophils were less than 10 10 cells per l , the bolus fluorouracil was omitted and the oxaliplatin and infused fluorouracil doses were reduced by 25% . 
patients were followed up for 8 years with full blood count , urea and electrolyte , liver function , and carcinoembryonic antigen tested at months 9 , 12 , 18 , 24 , and 36 , then 564 vol 19 april 2018 articles annually . 
ct of the chest , abdomen , and pelvis was done at months 6 , 12 , 18 , 24 and 36 . qol was assessed with the european organisation for research and treatment of cancer ( eortc ) qlq - c30 and qlq - cr29 and eq - 5d - 3l ( visual analogue scale and health index ) , with uk value sets.12 neuropathy was assessed with the fact / gog - ntx4 questionnaire . the qol questionnaires were administered at baseline and before each treatment cycle . 
subsequent assessments were made at months 9 and 12 for the eortc questionnaires and months 9 , 12 , 18 , and 24 , then annually for eq - 5d - 3l . neuropathy assessments with fact / gog - ntx4 were initially completed up to 12 months , as were the eortc questionnaires in patients who underwent randomisation before feb 16 , 2011 , from sites that opted to participate in this substudy . 
an amendment introduced in version 3.0 of the protocol on march 20 , 2012 , extended the requirement for the neuropathy questionnaire to be completed for patients who completed it at baseline to the follow - up visits at months 18 and 24 . 
a further amendment ( version 4.0 on dec 20 , 2012 ) extended the requirement for the neuropathy questionnaire to be completed to every follow - up visit ( to a maximum of 8 years ) for all new patients and existing patients already participating in the substudy . 
these amendments were made as a result of recommendations by the independent data monitoring committee . outcomes the primary study endpoint was disease - free survival , defined as the time from randomisation ( or trial registration for those randomised after 3 months of therapy ) to relapse , development of a new colorectal cancer , or death from any cause . 
assuming that the study would recruit over a period of 5 years with a subsequent minimum follow - up of 2 years , this design required 8600 patients to undergo randomisation and 2750 events ( relapses , deaths , or new colorectal cancers ) to be observed . 
to allow for losses to follow - up , our target recruitment was 9500 patients . from the outset , we recognised that reliable conclusions based on safety and qol data would not require information on all 9500 patients . 
for safety outcomes , the plan was that 700 patients ( 350 in each group ) would be sufficient to detect ( with 80% power and two - sided significance level of 5% ) a halving in the proportion of patients with grade 3 or 4 toxic effects from 12% to 6% ( 12% being the rate at which grade 3 or 4 paraesthesia the most frequent non - haematological grade 3 or 4 toxic effectoccurred in the oxaliplatin group in the mosaic trial ) .3 this same sample size would allow small changes in global qol to be detected ( assuming a difference of magnitude of 75313 and a standard deviation of 234 ) 14 with 95% power at the 1% significance level . 
this more stringent level of significance was used to allow for multiple testing across the various qol scales . we collected information on these toxicity and qol endpoints from all patients recruited until the number required was exceeded and the decision to stop was endorsed by the independent data monitoring committee and trial steering committee . 
the data monitoring committee had access to summary plots of eortc qol data , eq - 5d health status , and fact / gog - ntx4 neuropathy data by study group and study timepoints and following a committee meeting on may 28 , 2010 ( based on 1047 randomised patients ) , recommended that the collection of qol and fact / gog - ntx4 data be continued because they were concerned that the amount of missing data might undermine the comparisons at later timepoints if the original sample size estimates were used . 
they also recommended that the collection of fact / gog - ntx4 data should be extended beyond 12 months for new patients and , where possible , for patients already on the study . 
at their next meeting on the data monitoring committee nov 23 , 2010 , recommended the collection of qol and fact / gog - ntx4 data should stop once 1800 patients had been recruited . 
delays in the amendment of the protocol to implement the collection of the fact / gogntx4 beyond 12 months led to patient recruitment beyond this recommendation to ensure sufficient numbers of patients at these later timepoints . 
these extensions to data collection were made to compensate for missing data and no formal power calculations were made for these changes . that the efficacy analyses of disease - free survival and overall survival included all randomly assigned patients far as possible . 
 ( intention - to - treat population ) as vol 19 april 2018 articles kaplan - meier techniques were used to plot both disease - free survival and overall survival . 
the analysis of treatment delivery and safety was based on patients who started study treatment . the comparison of disease - free survival and overall survival between the treatment groups was based on a cox regression model incorporating the minimisation factors as covariates . 
the p value for testing the null hypothesis that the hr of 3 months versus 6 months was greater than or equal to 113 was derived from this model by comparing the log - likelihood of the fitted model with the log - likelihood of a model where the hr between the groups is set to 113 by use of a likelihood ratio test . 
the proportional hazards assumption implicit in these analyses was examined graphically via a log - minus log plot of the survival function against log time and via a test of the interaction between the treatment group and time ( logged ) obtained from a cox model time - varying covariate . incorporating an appropriate the components of the forest plot ( estimated hr for the comparison between groups and associated 95% ci ) were derived from a cox model that included separate terms for the effect of duration within each category of the relevant stratification factor or other factor being examined . 
patients could have more than one reason . 566 vol 19 april 2018 articles the impact of treatment duration varied across important patient subgroups . multiple imputation analysis15 was used to fill in the missing data and questionnaires in the qol and neuropathy scales . 
 the standardised adjusted auc was calculated for the five imputed datasets and compared between the randomised treatment groups via a generalised linear model ( with study group as an independent factor and study minimisation factors as covariates )  . 
the test statistics associated with study group from each of the five imputations were finally combined to provide an overall p value that takes into account the extent of the missing data . 
to allow for the number of scales being examined , an adjustment for multiple comparisons ( separately for the eortc and eq - 5d questionnaires ) was made with the sharpened hochberg procedure.17 the p value threshold for statistical significance was 5% after adjustment . 
comparisons of these scales at individual timepoints also made use of multiple imputation and generalised linear models . the mann - whitney u test was used for the comparison of ordered categorical variables for toxicity grade . 
 fishers exact test was used to compare the incidence of grade 35 toxic effects and the odds ratio and associated confidence interval for the incidence of grade 35 toxicity was estimated using logistic regression . about issues the study data were reviewed by the data monitoring committee approximately once per year to assess safety and efficacy from an ethical viewpoint . 
 the conditional power for disease - free survival was presented at the fifth ( june 26 , 2012 ) , sixth ( jan 7 , 2013 ) , and seventh ( oct 2 , 2013 ) meetings of the data monitoring committee . 
the data monitoring committee also had access to interim disease - free survival results from an italian study tosca ( nct00646607 ) , which was addressing the same question and had more mature data at the time . 
 table 1 : baseline patient characteristics recorded at randomisation by study group role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the study did not meet its recruitment target of 9500 patients because accrual was not as rapid as originally forecast and recruitment needed to stop to allow sufficiently complete follow - up on current patients within the available funding . 
 by increasing the recruitment period by 6 months and extending minimum follow - up to 3 years ( 88% patients were followed up for 3 year disease - free survival by the reverse kaplan - meier method , allowing for a 2 month deviation from the assessment time ) , 1482 disease - free survival events were observed , giving the study 66% power rather than the originally planned 90% power for rejecting the null hypothesis . 
results from previous adjuvant studies have shown that most disease - free survival events occur within the first 3 years of starting treatment.3 , 19 the analysis time was prespecified in the protocol and therefore no bias would be introduced as might be the case if we had allowed the timing of the analysis to be guided by the data at hand . the data cutoff for this analysis was dec 1 , 2016 . 
787 patients had died at the time of analysis . 568 vol 19 april 2018 articles the baseline demographics , stage , and site of disease for each group were balanced across the trial population ( table 1 )  . 
the largest difference between the overall population and the subgroups assessed for safety and qol was a 9% increase in the incidence of patients with performance status 1 in the ctcae safety cohort ; all other differences in individual characteristics were within 5% . at the time of the disease - free survival analysis there had been 740 events in the 3 month group and 742 events in the 6 month group . 
3 year disease - free survival was 767% ( 95% ci 751782 ) in the 3 month group and 771% ( 756786 ) in the 6 month group , giving an hr of 1006 ( 09091114 , p = 0012 ) which met the criteria for non - inferiority ( figure 2 )  . 3 year overall survival is shown in figure 2 . 
the appendix contains a breakdown of causes of death ( p 10 ) and further details of deaths related to protocol treatment ( p 11 )  . in a prespecified sensitivity analysis , we also examined the difference between the study groups according to the actual duration of treatment on the two randomised groups ( appendix p 1 )  . 
for eligible patients who received the actual assigned study duration of 3 and 6 months , the observed hr was 1158 ( 95% ci 10181317 , p = 0641 )  . forest plots by stratification factors and randomisation timepoint are shown in figure 3 . 
the most marked heterogeneity was for the dependence of the duration effect on the initial choice of regimen ( p = 0069 ) , so we did a post - hoc analysis of disease - free survival for the two durations of therapy for capox and folfox regimens ( figure 4 )  . 
 among patients with available chemotherapy duration data , 2521 ( 83% ) of 3024 of patients assigned to 3 months of treatment actually received 3 months of treatment , including 845 ( 86% ) of 980 receiving folfox and 1676 ( 82% ) of the 2044 receiving capox . 
1773 ( 59% ) of 3013 patients assigned to receive 6 months of treatment actually received 6 months of treatment , which was similar for those receiving folfox ( 585 [ 59% ] of 985 ) and capox ( 1188 [ 59% ] of 2028 )  . 
 * these estimates differ slightly because the underlying multivariable cox model on which they are based includes parameters for other minimisation variables , as well as those factors relating to stage ; the increased flexibility in the expanded stage model allows the influence of these parameters on the high risk stage ii estimates to modify . 
 see online for appendix receive 3 months ( 425 [ 14% ] of 3024 ) and 6 months ( 417 [ 14% ] of 3013 ) of treatment . 244 patients in the 3 month group and 576 patients in the 6 month group cited adverse events as the reason for stopping treatment early . 
in the 6 month group , both diarrhoea ( 150 patients ) and peripheral neuropathy ( 156 patients ) were commonly cited as reasons for stopping . figure 5 shows the dose delivery for fluoropyrimidine and oxaliplat the median percentage of full fluoropyrimidine dose delivered was 953% ( iqr 831998 ) in the 3 month group and 832% ( 567957 ) in the 6 month group . 
the number of patients who had recorded fluorouracil or prescribed capecitabine dose reductions in the 3 month group were 788 ( 26% ) of 3009 compared with 1286 ( 43% ) of 3013 in the 6 month group . 
for oxaliplatin , the corresponding figures were 906 ( 30% ) of 3009 and 1869 ( 62% ) of 3013 . given previous trial data , 20 it is known that there is a marked difference in risk of relapse between patients with n1 colorectal cancer compared with those with n2 pathology , so we did a post - hoc analysis comparing t13 , n1 colorectal cancer against t4 and n2 pathology ( figure 6 ) , and analysed these different prognostic groups according to the chemotherapy regimen they received ( folfox or capox ; appendix p 5 )  . 
for those patients with t1 - 3 / n1 disease the test for non - inferiority in this post - hoc analysis was statistically significant ( p = 0012 )  . safety was assessed by the investigators in 868 patients , 434 ( 50% ) in each group . 
sensory neuropathy , diarrhoea , neutropenia , fatigue , pain , nausea , and hand - foot syndrome were the most common grade 35 adverse events ( table 2 )  . 
the frequency of grade 35 diarrhoea ( p = 0033 ) , neutropenia ( p = 0014 ) , hand - foot syndrome ( p = 0031 ) , and sensory neuropathy ( p < 00001 ) was significantly higher in the 6 month group than in the 3 month group . 
the only side - effect for which the percentage of patients with adverse events ( p = 0031 ) , pain 570 vol 19 april 2018 articles during months 9 and 12 after patients in the 6 month group had stopped treatment . 
overall , grade 35 adverse events were reported by 150 ( 36% ) of 420 patients in the 3 month group and 243 ( 59% ) of 409 patients in the 6 month group ( p < 00001 )  . 
we compared the results from the fact / gog - ntx4 questionnaire for patients receiving 3 months of chemotherapy with those receiving 6 months of chemotherapy ( figure 7 )  . 
the neuropathy standardised adjusted auc differed significantly between the two study groups ( p < 00001 ) , with clear differences appearing at month 4 and persisting until at least 5 years ( p < 00001 )  . 
the maximum difference in means was generally seen at 6 months and , in accordance with the categories of osoba and colleagues , 13 these mean differences in functional and global health status scales represented moderate changes ( values between 1020 ) for global health status , role functioning , and social function and a ( values between 510 ) for physical little change functioning , and cognitive functioning , emotional functioning . 
thereafter , the mean values converged 3 months of treatment 6 months of treatment study group figure 5 : treatment delivery by selected adjuvant regimen box and whisker plots indicate median and iqr ( boxes ) and range ( whiskers )  . 
the standardised adjusted aucs differed significantly for both the eq - 5d self - rated visual analogue scale ( p = 000081 ) and the eq - 5d - 3l health index ( p = 000081 ; appendix p 15 )  . 
 plotting the eq - 5d scales showed that the differences between the two groups of the study were restricted to months 4 , 5 , and 6 , the period when patients in the 6 month group were still receiving treatment and those in the 3 month group had stopped . 
the maximum difference in means was at 6 months and these differences were consistent with clinically important differences ( appendix p 15 ) .21 this pattern was also noticeable for the eq - 5d selfrated visual analogue scale ; patients in the 6 month group had significantly lower qol than those in the 3 month group during months 4 , 5 , and 6 , but after this point , there were no overall clinically important differences up to the 6 year follow - up ( appendix p 3 )  . to investigate the potential effects of missing data on the results from the fact / gog - ntx4 , eortc , and eq - 5d assessments , the reasons for missing questionnaires were recorded ( appendix p 16 )  . 
similarly , an analysis of missingness according to baseline factors indicated that the patients who completed the questionnaires were representative of the patients who participated in this aspect of the study , with any associations between a questionnaire being missing and 572 vol 19 april 2018 articles l vol 19 april 2018 articles 6 months 3 months baseline 1 month 2 month 3 month 4 month 5 month 6 month 9 month 1 year 18 months 2 years 3 years 4 years 5 years 6 years assessment timepoint baseline month 1 month 2 month 3 month 4 month 5 month 6 month 9 year 1 month 18 * year 2 * year 3 * year 4 year 5 year 6 3 months treatment questionnaires completed questionnaires expected proportion of expected questionnaires received 859 1445 59% 6 months treatment questionnaires completed questionnaires expected proportion of expected questionnaires received 865 1426 61% 817 1433 57% 782 1426 55% 527 1421 37% 639 1416 45% 639 1416 45% 606 1400 43% 733 1386 53% 721 1266 53% 172 1312 13% 169 1202 14% 22% 796 1406 57% 782 1395 56% 701 1389 50% 679 1384 49% 679 1382 45% 268 1375 19% 665 1366 49% 721 1346 54% 182 1308 13% 174 1195 15% 22% 48% 42% 62% 54% figure 7 : peripheral neuropathy by study group patients reported peripheral neuropathy with the gog ntx4 questionnaire . 
 * the low completion rates at these timepoints reflect the fact that , initially , neurotoxicity data were only collected up to 12 months and there was a delay before an amendment extended the collection to the whole study period . 
low return rate because patients were assessed at the start of last cycle rather than 6 months ( which corresponds to end of cycle )  . baseline characteristics being small ( appendix p 17 )  . 
 finally , we did a sensitivity analysis to compare the primary imputed results with the results based on observed data only or the imputed results for patients who completed baseline questionnaires only . 
the results of these analyses were all very similar to the findings of the main study ( appendix p 18 )  . we did an exploratory analysis to examine the differences in qol scales between patients whose worst responses to the questions on the gogntx4 questionnaire about whether they had numbness , tingling , or discomfort in their hands or feet were quite a bit or very much and those whose worst responses were somewhat , a little bit , or not at all ( appendix p 4 )  . 
this analysis identified statistically and clinically significant poorer qol between these patient groups at 1 year , 3 years , and 5 years , apart from eq - 5d visual analogue scale at 1 year , for which the difference was not clinically significant . 
the proportion of patients recording neuropathy symptoms as being present quite a bit or very much was significantly higher in the 6 month group than in the 3 month group at each timepoint ( 248 [ 34% ] of 721 vs 99 [ 14% ] of 721 , p < 00001 at 1 year ; 63 [ 32% ] of 199 vs 30 [ 15% ] of 198 , p < 00001 at 3 years ; 49 [ 29% ] of 170 vs 30 [ 16% ] of 193 , p = 00032 at 5 years )  . discussion our results show the non - inferiority of 3 months of adjuvant oxaliplatin - containing chemotherapy treatment compared with 6 months of treatment for patients with high - risk stage ii and stage iii cancer of the colon and rectu the shorter treatment duration was also associated with reduced toxicity and less deterioration in qol . 
because this study recruited 6088 patients with conventionally defined high - risk stage ii and stage iii colorectal cancer from a large number of centres and countries and made use of standard chemotherapy regimens , the study findings are applicable to a typical patient with colorectal cancer needing adjuvant chemotherapy treatment . 
the non - inferiority boundary was set to exclude a maximum 25% fall in 3 year disease - free survival in patients in the 3 month group compared with those in the 6 month group , whichas estimated on the basis of results from previous trials would yield a predicted 3 year disease - free survival of 78% . 
this threshold of 25% was chosen because it was half the difference seen in 3 year disease - free survival between patients in the oxaliplatin - containing group and those in the fluoropyrimidine only group in the mosaic study . 
it was felt by clinicians commonly treating 574 vol 19 april 2018 articles colorectal cancer that this small difference would be an acceptable payoff to bring about a significant reduction in long - term neuropathy and potential improvement in qol to patients who achieve a long - term cure . 
this difference corresponds to an hr of 113 , which we aimed to detect with 90% power at the 25% one - sided level of statistical significance . initial ( rather than our because 6088 patients were recruited and 1482 events were recorded target of 9500 patients with 2750 events ) , the power was reduced to 66% . 
however , we were still able to show the noninferiority of 3 months of treatment compared with 6 months of treatment ( p = 0012 ) across the trial population as a whole ( stage iii and high risk stage ii disease ; colon and rectal cancer ) , with 3 year disease - free survival of 771% ( 95% ci 756 to 786 ) for patients in the 6 month group and 767% ( 751 to 782 ) for those in the 3 month group ( hr 1006 , 0909 to 1114 )  . 
patients in the 6 month group had similar 3 year disease - free survival to that seen with 6 months of oxaliplatin - containing adjuvant chemotherapy in the mosaic study ( 782% ) and nsabp c07 studies ( 761% ) , suggesting that the outcome observed in our control group was similar to that previously seen.3 , 4 however , it is important to note that in the scot trial , only 1096 ( 18% ) of 6088 patients had highrisk stage ii disease , whereas in mosaic and nsabp - c07 , 40% and 30% of patients had all - risk stage ii disease . 
at the time scot was initiated , less data were available on adjuvant chemotherapy for rectal cancer because many adjuvant studies have excluded these patients , and patients with rectal cancer were eligible to participate if they had received no preoperative chemotherapy ( short - course radiotherapy alone was allowed ) and had undergone total mesorectal excision with an r0 resection . 
the only adjuvant chemotherapy these patients received was within this study and randomised for the duration of treatment . we did comparisons of disease - free survival based on the actual duration of treatment received in the study groups , as well as the primary intention - to - treat analyses . 
 these subanalyses did not show non - inferiority , but are inherently biased by the differential exclusion of patients not able to receive prolonged therapy because of the different target treatment durations in the study groups . 
 in a setting such as this where differential compliance is intrinsic to the treatments being compared , our view is that the intention - to - treat analysis is a more accurate reflection of the impact of the intervention on actual clinical practice . in terms of our analyses of smaller subgroups , we have not been able to draw solid conclusions about the effect of treatment duration on specific patient populations such as those with high - risk stage ii disease or patients with rectal cancer because the numbers in these subgroups were relatively small and few events occurred . 
however , the forest plots did not show any differences in the effect of the duration of adjuvant chemotherapy between patients with high - risk stage 2 disease and those with stage iii disease and between those with rectal cancer and those with colon cancer . 
in clinical practice in many parts of the world , a substantial proportion of patients with high - risk stage ii disease or stage iii disease ( especially if older than 70 years of age ) receive only single - agent fluoropyrimidine for 6 months because the addition of oxaliplatin to fluoropyrimidine has not been shown to improve survival in these patients.22 other factors to consider in terms of prognosis and prediction of response to treatment include the sidedness of the cancer ( right vs left ) , ras and braf status , which affect prognosis in metastatic disease , and microsatellite instability status , which affects the outcome of adjuvant treatment.23 these questions cannot yet be answered by the results of scot , but there is a translational research substudythe transscot study , which is ongoing that will look at these factors . it is more difficult to give 6 months of treatment than 3 months of treatment . 
in the scot study , 2521 ( 83% ) of 3024 patients assigned to 3 months received 3 months of treatment , whereas only 1773 ( 59% ) of 3013 patients assigned to 6 months received 6 months of treatment . 
however , the median percentage of the full expected dose of fluoropyrimidine received varied between 94% and 98% for the 3 month group and 82% and 85% for the 6 month group , depending on regimen choice . 
given that the median fluoropyrimidine and oxaliplatin doses received were similar between the two regimens ( figure 5 ) , compliance to treatment is unlikely to explain the difference seen between the two regimens . our results showed that 6 months of adjuvant chemotherapy was significantly more toxic than 3 months of treatment . 
this difference was most marked for peripheral neuropathy , with 237 ( 58% ) of 409 patients in the 6 month group reporting grade 2 or worse neuropathy compared with 103 ( 25% ) of 420 patients in the 3 month group . 
peripheral neuropathy , as reported via a patient questionnaire , was significantly worse in the 6 month group and persisted for at least 5 years ( figure 7 )  . 
however , the vol 19 april 2018 articles effects are large , as are the significance levels , and there is no evidence that these comparisons are biased between the groups , qol , as measured by qlq - c30 global health status and eq - 5d - 3l , declined while patients were receiving chemotherapy . 
 in peripheral neuropathy , with more patients in the 6 month group reporting quite a bit or very much numbness , tingling , or discomfort in their hands or feet in the fact / gog - ntx4 questionnaire , which correlated with significantly worse qol at 1 year , 3 years , and 5 years . 
when we looked at the effect of duration for each regimen separately , capox showed non - inferiority in terms of disease - free survival for 3 months versus 6 months of treatment , but this was not the case for patients receiving folfox . 
the choice of chemotherapy regimen was not randomised but instead chosen by the physician and patient and the reasons why specific regimens were chosen for individual patients are not known . also important to note for capecitabine , an oral drug that is self - administered at home , is that we only know that we might overestimate the prescribed dose and do not have detailed compliance the data , meaning fluoropyrimidine dose intensity for patients receiving capox . 
however , in our experience , except in instances where clinicians curtail or modify doses according to intracycle toxicity , compliance with oral chemotherapy drugs is high . since the difference in the impact of treatment duration between the capox and folfox regimens does not seem to be easily explained by compliance with treatment or differences in the overall percentage of standard drug doses that were delivered , we perhaps need to consider other potential reasons for this finding . 
in the capox regimen , the dose of oxaliplatin given with each cycle is higher than that given in folfox , and therefore we presume that higher peak doses of oxaliplatin are achieved . 
additionally , although the peak dose of fluoropyrimidine will be lower with capox ( capecitabine is given twice daily orally for two out of three weeks ) than with folfox ( where the fluoropyrimidine is given as a bolus , then infused over 2 days every 2 weeks ) , the duration and continuity of exposure is greater . 
could the micrometastatic disease be rendered more sensitive by one or both of these differences ? if each of the cells in this micrometastatic setting are cycling through s phase only sporadically , does the continuity of exposure of the fluoropyrimidine in the form of capecitabine mean that there is a greater overall chance that these cells will be exposed to fluoropyrimidine at the critical part of the cell cycle , compared with fluorouracil given as bolus , then over 2 days every 2 weeks . 
this notion is supported by data from two previous adjuvant studies.10 , 28 in terms of oxaliplatin , a drug that is nearly always given over 24 h , does the peak concentration have more of an effect than the frequency , giving an advantage to the capox regimen and less attrition to efficacy when the overall duration of therapy is shortened ? additionally , a higher dose of oxaliplatin is given in the first 4 weeks of treatment with capox ( 260 mg / m ) than with folfox ( 170 mg / m )  . 
it is very difficult to prove these speculative theories without developing appropriate adjuvant models of malignancy , but the results seen will certainly be a focus of strong debate over the coming months and years . stage iii colorectal cancer is a heterogeneous disease and data from the idea collaboration and from multiple adjuvant trials have shown that patients with t13 , n1 pathology have much better outcomes than those with either t4 or n2 features.27 this has led to the evolution of the concept of a high - risk stage iii patient population , with either t4 or n2 disease , as opposed to the lower risk stage iii population ( t13 , n1 ) ; we might need to consider whether patients with high - risk stage iii disease need to be treated in a slightly different way to those with lower risk stage iii disease . similarly , our results have shown that patients with t13 , n1 disease have a much better 3 year disease - free survival than those with either t4 or n2 pathology . 
 576 vol 19 april 2018 articles we found that , in patients with t13 , n1 colorectal cancer , 3 months of treatment was non - inferior to 6 months ( hr 0908 , 95% ci 0751098 )  . 
the hr for disease - free survival is greater than 1 for the 3 months duration compared to 6 months , suggesting that there could be some small loss of efficacy , but the confidence intervals are wide , making this difference difficult to interpret with certainty . 
notably , the observed absolute deficit in 3 year disease - free survival between the 3 months and 6 months of treatment for the high - risk group ( t4 or n2 disease ) is 18% , which has to be balanced against the increased toxicity seen with 6 months of treatment . 
this is particularly important because the worsened peripheral neuropathy persists for at least 5 years after treatment and results in worse qol outcomes . for patients with t4 or n2 pathology , the absolute increase in 3 year disease - free survival with 6 months versus 3 months of treatment was 27% ( 95% ci 41 to 96 ) for folfox and 13% ( 95% ci 37 to 62 ) for capox ( appendix p 5 )  . 
in view of the difference in toxicity seen with longer treatment , many patients will accept a small reduction in disease - free survival in exchange for reduced toxicity and this is especially true if they are able to receive capox . 
there is less evidence to support a shorter duration of adjuvant treatment if it is decided that the patient needs to receive folfox or has t4 disease . across the whole trial population , scot met the criteria for non - inferiority with a difference in 3 year disease - free survival of 04% ( 95% ci 26 to 18 ) between 3 months and 6 months of treatment . 
while the study was underpowered , the 95% ci for the hr lies below the noninferiority boundary and the results are consistent with those of other individual studies by the idea group , taking into account how the duration effect depended on regimen and risk group . 
the concept that underpowered studies are more likely to produce false - positives ( ignoring the factor of publication bias , which does not apply to a large scale enterprise such as scot ) is disputed.29 as noted , the results differed with the ( non - randomised ) choice of chemotherapy regimens and we can recom mend a 3 month duration of adjuvant chemotherapy for patients with t13 , n1 disease ( 2677 [ 44% ] of the 6088 patients in the scot study ) if the patient is felt to be suitable for the capox regimen . 
we have not been able to show with any statistical certainty that 3 months of treatment was non - inferior to 6 months for patients receiving folfox , for whom there was an absolute increase in 3 year diseasefree survival with 6 months versus 3 months of treatment of 29% ( 95% ci 67 to 08 )  . despite the studys size , there are limitations to the reliability of conclusions that can be drawn for some subgroups . 
high - risk stage iii disease includes either t4 or n2 disease ( or both ) and this study has not been able to the effect of duration of adjuvant show whether chemotherapy is the same for t4 and n2 disease . 
the final decision on treatment duration and regimen used for each individual will depend on a careful discussion between the clinician and patient , taking into account the risk of recurrence , the likely absolute difference in diseasefree survival and risk of long - term toxicity , and the strength of evidence for that particular setting available both from scot and the wider idea analysis . scot is , to our knowledge , the largest single randomised study on the adjuvant treatment of colorectal cancer to date . 
 the study achieved its primary endpoint of showing that 3 months of oxaliplatin - containing adjuvant chemotherapy is non - inferior to 6 months of the same treatment in the overall trial population . 
tji , rsk , mps , ahar , ka , jm , cs , kab , ab , and jp wrote the manuscript and all authors contributed to the review of the manuscript . declaration of interests tji reports receiving honoraria from eli lilly ; serving on advisory boards for servier , roche , and celgene and receiving travel expenses from bayer and servier . 
jt reports support for being on advisory boards from amgen , bayer , boehringer ingelheim , celgene , chugai , lilly , msd , merck serono , novartis , pfizer , roche , sanofi , symphogen , taiho , and takeda . 
awa reports belonging to an institution involved in research that is funded by drug companies that provide the drugs for this study ; and has been coinvestigator in trials funded by roche which provided the capecitabine used in this study . 
all other authors declare no competing interests . acknowledgments this research was supported by the medical research council ( transferred to netsccefficacy and mechanism evaluation ; grant reference g0601705 ) , swedish cancer society , and cancer research uk vol 19 april 2018 articles core clinical trials unit funding ( funding ref : c6716 / a9894 )  . 
we also thank all international collaborative groups who led the trial in their countries ( the danish colorectal oncology group , vhio , agitg , and swedish society of gastrointestinal oncology ) , the independent trial data monitoring committee members ( hilary calvert [ chair ] , allan hackshaw , robin kennedy , and kees punt ) , and the trial steering committee members ( stan kaye , janet dunn , and alberto sobrero )  . correction to lancet oncol 2016 ; 17 : 159098 sharma p , callahan mk , bono p , et al . 
 nivolumab monotherapy in recurrent metastatic urothelial carcinoma ( checkmate 032 ) : a multicentre , openlabel , two - stage , multi - arm , phase 1 / 2 trial . 
lancet oncol 2016 ; 17 : 159098 in this article , the declaration of interests should read psh has received fees for advisory board participation for jounce and kite ; fees for consultancy from jounce , kite , bristol - myers squibb , astrazeneca , and amgen ; and stock or stock options from jounce and kite . 
eca reports research grants and / or financial support from boehringer ingelheim , roche / genentech , bristol - myers squibb , novartis , psioxus , nanobiotix janssen , abbvie , pharmamar , puma , sanofi , lilly , pfizer , merck , nektar , amcure , amgen , astrazeneca , principia , bayer , cytomx , h3 , incyte , kura , loxo , macrogenics , menarini , merck serono , merus , millenium , rigontec , tahio , and beugene tesaro ; consultancy fees from janssen - cilag , alkermes ( and travel expenses ) , seattle genetics , pierre fabre , cerulean pharma , eusa , celgene , novartis ( speakers bureau ) , nanobiotix , psioxus therapeutics , abbvie , astrazeneca , guidepoint global , roche / genentech ( and travel expeneses ) , glg , pfizer , servier , amcure , and boehringer ingelheim ; ownership from start ( leadership ) , oncoarts associated and international cancer consultants ; and employment from start and hm hospitals group ( honoraria ) and president and founder of npo foundation intheos ( investigational therapeutics oncological sciences ) , outside the submitted work . 
fdb has received consultancy fees from tiziana life sciences , bristol - myers squibb , msd , servier , eli lilly , merck serono , glaxosmithkline , and novartis , and speaker fees from bristol - myers squibb , eli lilly , roche , and accmed . 
mm has received consultancy fees from etubics and boehringer ingelheim , and speaker fees from genentech , novartis , sanofi , regeneron , lexicon , ipsen , onyx , bayer , taiho , merrimack , and celgene . 
 dj has received consulting fees from definiens , f hoffmann - la roche , curevac , roche pharma , novartis pharma , and novartis oncologynovartis farma , outside the submitted work ; and has a patent issued for intellectual property of infiltrating t - cell density predicting outcome . 
 ech has received grants from bristolmyers squibb and consultancy fees for advisory board participation from emd serono , taiho , bayer , advaxis , amgen , lilly , and castle biosciences . 
jer has received grants for study conduct from novartis ; funds for clinical trial conduct from astellas , seattle genetics , bayer , astrazeneca , mirati therapeutics , oncogenex , and roche / genentech ; has received consultancy fees from roche / genentech , astrazeneca , eli lilly , astellas , seattle genetics , bristol - myers squibb , merck , emd - serono , adicet bio , western oncolytics , pharmacyclics , sensei biotherapeutics , bayer , bioclin therapeutics , qed therapeutics , mirati therapeutics , fortress biotech , inovio ; has gritstone oncology , received honoraria from bristol - myers squibb and chugai ; has held stock in illumina and merck . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2017 ; 18 : 90416 baselga j , im s - a , iwata h , et al . 
buparlisib plus fulvestrant versus placebo plus fulvestrant in postmenopausal , hormone receptor - positive , her2 - negative , advanced breast cancer ( belle - 2 ) : a randomised , double - blind , placebocontrolled , phase 3 trial . 
lancet oncol 2017 ; 18 : 90416in this article , the declaration of interests should read jb has received reimbursement for travel , and advisory board and consulting fees from novartis , during the conduct of the study ; has received personal fees and held stock as a member of the board of directors from aura biosciences ; has received personal fees as a member of the advisory board and held stock as a founder of northern biologics ( f / k / a mosaic biomedicals ) ; has received personal fees and held stock as a member of the board of directors from infinity pharmaceuticals ; held stock as a member of the advisory board from apogen biotechnologies ; has received personal fees and held stock as a member of the advisory board from pmv pharma ; has received personal fees and held stock as a member of the advisory board from juno therapeutics ; has received personal fees and held stock as co - founder from tango ( f / k / a synthetic lethal ) ; has received personal fees and held stock as a member of the scientific advisory board and the board of directors from grail ; has received personal fees and held stock as a member of board of directors from varian medical systems ; held stock as a member of board of directors from foghorn therapeutics ; has received reimbursement for travel , e71 vol 20 february 2019 corrections and advisory board and consulting fees from eli lilly ; has received personal fees and held stock as a member of advisory board from seragon ; has received reimbursement for travel and in - kind items and services from roche , outside the submitted work . 
 s - ai reports grant support from astrazeneca and advisory consultant roles for astrazeneca , eisai , novartis , pfizer , roche / genentech and spectrum , outside the submitted work . 
hi reports grant support and personal fees from novartis during the conduct of the study ; hi was also an uncompensated member of the steering committee of this study ; hi has received personal fees in the form of honoraria and consulting fees from astrazeneca , pfizer , lilly , daiichi - sankyo , and f hoffman la - roche via chugai , outside the submitted work . 
jc reports personal fees from novartis , celgene , cellestia , astrazeneca , biothera pharmaceuticals , merus , seattle genetics , daiichi sankyo , erytech , pfizer , eisai , and samsung ; has received stock , patents , and intellectual property from medsir ; has received personal fees and research funding to his institution from roche , outside the submitted work . 
mdls reports personal fees in the form of speakers honoraria and advisory board honoraria from novartis , roche , lilly , pfizer , eisai , ipsen , and teva , outside the submitted work . 
cla reports personal fees for participation in a steering committee for the clinical trial from novartis , during the conduct of the study ; and personal fees for an expert advisory role from eli lilly , astrazeneca , genentech , millennium , celgene , pfizer , radius , and merck , outside the submitted work . 
sc also reports personal fees received in the form of honoraria for advisory boards from novartis , hoffmann laroche , pfizer , astrazeneca , and genomic health ; and institutional research support from novartis , hoffmann laroche , pfizer , astrazeneca , genomic health , genentech , merck , and bms , outside the submitted work . 
she also reports grant support from ambryx , amgen , bayer , obi pharma , bimarin , cascadian , daiichi sankyo , dignitana , genentech , gsk , lilly , macrogenics , medivation , merrimack , novartis , pfizer , pieris , puma , roche , seattle genetics , and travel support from lilly , novartis , and obi pharma , outside the submitted work . 
 reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
pv reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 15964 wolf a , naylor k , tam m , et al . 
these corrections have been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 17980 massari f , di nunno v . 
lancet oncol 2019 ; 20 ; 17980in this comment , the following sentence has been edited from time to deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab to risk of deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab . 
 this correction has been made to the online version as of feb 1 , 2019 , and the printed version is correct . vol 20 february 2019 corrections correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections corrections correction to lancet oncol 2014 ; 15 : 856 correction to lancet oncol 2015 ; 16 : 60 , 61 ledermann j , harter p , gourley c , et al . 
lancet oncol 2014 ; 15 : 85261 in this article , the second sentence of the rst paragraph of the results section should read on the basis local germline brca mutation testing reported on case report forms , germline brca mutation status was known for 98 ( 37% ) of 265 patients ( 50 [ 37% ] of 136 in the olaparib group vs 48 [ 37% ] of 129 in the placebo group )  . 
this correction has been made to the online version as of march 30 , 2015 . a multi - centre , topp ms , gckbuget n , stein as , et al . 
lancet oncol 2015 ; 16 : 5766in table 2 of this article , the mrd response during rst two cycles in patients with cr or crh row should not have been indented , and should have been the last row in the table . 
these corrections have been made to the online version as of march 30 , 2015 . after vol 16 april 2015 e158 corrections correction to lancet oncol 2015 ; 16 : 133 correction to lancet oncol 2015 ; 16 : 181 , 184 correction to lancet oncol 2015 ; 16 : 237 published online january 29 , 2015 s1470 - 2045 ( 14 ) 70483 - 8 dp . 
 radiotherapy lancet oncol 2015 ; 16 : 23739in this comment , the fth line of the third paragraph should read : by contrast , acute gastrointestinal toxicity was increased with hypofractionation [ 95% ci 372469 ] of ( 420% patients the hypofractionation group had grade 2 adverse events vs 312% [ 266358 ] in the standard fractionation di erence 108% , 90% ci 5251643 ; p = 00015 ) although were similar 3 months after treatment , and non - inferiority was not con rmed . 
these corrections have been made to the online version as of march 2 , 2015 , and have been made to the printed comment . group , cavalli f , atun r . 
lancet oncol 2015 ; 16 : 13334 in this comment , the second sentence should have been : deaths from cancer are projected to increase from the present level of around 8 million a year to more than 13 million by 2030 , with most of the burden being in poorer countries . 
this correction has been made as of jan 29 , 2015 . correction to lancet oncol 2015 ; 16 : 266 ih , williams lj , kunkler jack wjl , cameron da , dixon jm , on behalf of investigators . 
 lancet oncol 2015 ; 16 : 26673in the interpretation section of the summary , the rst sentence should read postoperative whole - breast radiotherapy after breast - conserving surgery and adjuvant endocrine treatment resulted in a signi cant but modest reduction in local recurrence for women aged 65 years or older with early breast cancer 5 years after randomisation . 
this correction has been made to the online version as o f march 2 , 2015 , and to the printed article . thomas a , rajan a , berman a , in patients with et al . 
lancet oncol 2015 ; 16 : 17786 in the key of gure 2a of this article , the text for the red line should read thymic carcinoma ( 16 / 24 failed ) and that for the blue line should read in the thymoma ( 11 / 16 failed )  . 
 key of gure 4b , the text for the red line should read no change / increase ( 0 / 18 failed ) and that for the blue line should read decrease ( 4 / 4 failed )  . 
lancet oncol 2015 ; 16 : 27483in this article , the interpretation should have read : hypofractionated radiotherapy was not non - inferior to standard fractionated radiotherapy in terms of acute genitourinary and gastrofor men with intestinal intermediate - risk high - risk and prostate cancer . 
this correction has been made to the online version as of march 2 , 2015 and to the printed article . toxicity vol 16 march 2015 e105 articles cediranib or placebo in combination with cisplatin and gemcitabine chemotherapy for patients with advanced biliary tract cancer ( abc - 03 ) : a randomised phase 2 trial juan w valle , harpreet wasan , andre lopes , alison c backen , daniel h palmer , karen morris , marian duggan , david cunningham , d alan anthoney , pippa corrie , srinivasan madhusudan , anthony maraveyas , paul j ross , justin s waters , will p steward , charlotte rees , sandy beare , caroline dive , john a bridgewater summary background cisplatin and gemcitabine is the standard rst - line chemotherapy regimen for patients with advanced biliary tract cancer ; expression of vegf and its receptors is associated with adverse outcomes . 
we aimed to assess the e ect of the addition of cediranib ( an oral inhibitor of vegf receptor 1 , 2 , and 3 ) to cisplatin and gemcitabine on progression - free survival . methods in this multicentre , placebo - controlled , randomised phase 2 study , we recruited patients aged 18 years or older with histologically con rmed or cytologically con rmed advanced biliary tract cancer from hepatobiliary oncology referral centres in the uk . 
patients were given rst - line cisplatin and gemcitabine chemotherapy ( 25 mg / m cisplatin and 1000 mg / m gemcitabine [ on days 1 and 8 every 21 days , for up to eight cycles ] ) with either 20 mg oral cediranib or placebo once a day until disease progression . 
we randomly assigned patients ( 1 : 1 ) with a minimisation algorithm , incorporating the strati cation factors : extent of disease , primary disease site , previous treatment , ecog performance status , and centre . 
this study is registered with clinicaltrials.gov , number nct00939848 , and was closed on sept 30 , 2014 ; results of the nal analysis for the primary endpoint are presented . findings between april 5 , 2011 , and sept 28 , 2012 , we enrolled 124 patients ( 62 in each group )  . 
with a median followup of 122 months ( iqr 73185 ) , median progression - free survival was 80 months ( 95% ci 6593 ) in the cediranib group and 74 months ( 5785 ) in the placebo group ( hr 093 , 80% ci 074119 , 95% ci 065135 ; p = 072 )  . 
 patients who received cediranib had more grade 34 toxic e ects than did patients who received placebo : hypertension ( 23 [ 37% ] vs 13 [ 21% ] ; p = 005 ) , diarrhoea ( eight [ 13% ] vs two [ 3% ] ; p = 005 ) ; platelet count decreased ( ten [ 16% ] vs four [ 6% ] ; p = 009 ) , white blood cell decreased ( 15 [ 24% ] vs seven [ 11% ] ; p = 006 ) and fatigue ( 16 [ 24% ] vs seven [ 11% ] ; p = 004 )  . interpretation cediranib did not improve the progression - free survival of patients with advanced biliary tract cancer in combination with cisplatin and gemcitabine , which remains the standard of care . 
although these diseases are deemed to be low incidence in most high - income countries ( < 1% of all adult cancers , with roughly 1500 cases per year in the uk1 and 9000 cases per year in the usa2 ) , global hotspots exist with much higher incidence . 
importantly , both incidence and mortality are increasing largely due to a global rise in intrahepatic cholangio carcinoma.3 most patients present with locally advanced ( nonresectable ) or metastatic disease and , even when surgery is feasible , recurrence is frequent . 
 targeting angiogenesis , one of the hallmarks of cancer and a known predictor of adverse outcome in advanced biliary tract cancer , is a logical step and has proven to be e ective in a number of tumour types ; however , no randomised studies have been done of this approach in advanced biliary tract cancer building on the cisplatin and gemcitabine regimen . added value of this study this study assessed the e ect of adding cediranib ( an oral vegfr - 1 , vegfr - 2 and vegfr - 3 receptor tyrosine kinase inhibitor , with additional activity against pdgf receptors and c - kit ) to cisplatin and gemcitabine chemotherapy in a double - bind , placebo - controlled manner . 
the study did not meet its primary endpoint ( improvement in progression - free survival ) ; however , we recorded signals that would support further anti - angiogenesis approaches . 
additionally , we showed that elevated baseline levels of the tumour markers cea and ca125 ( in addition to ca19 - 9 ) and total cytokeratin 18 and vegfr2 are prognostic in advanced biliary tract cancer . 
this is the rst study to show that the presence of circulating tumour cells confers an adverse prognosis , and o ers an opportunity to interrogate these in future studies . 
finally , baseline pdgfbb concentrations might predict for cediranib activity . implications of all the available evidence cisplatin and gemcitabine remains the reference regimen for patients with advanced biliary tract cancer ; there is no evidence that cediranib improves progression - free survival . 
the e ect of a better - tolerated anti - angiogenic in combination with cisplatin and gemcitabine , with consideration of our exploratory ndings with respect to circulating biomarkers , warrants further investigation . 
 intrahepatic cancers , 810 especially at the invasive edge of the tumour.11 the receptors for this ligand , vegfr1 and vegfr2 , are also overexpressed in the adjacent endothelial cells.12 vegf expression is associated with the presence of metastases cholangiocarcinoma ; 8 adverse prognosis in extrahepatic cholangiocarcinoma13 and increased microvascular density in both cholangiocarcinoma9 and gallbladder cancer.10 in turn , high micro vascular density independent adverse is an prognostic factor for disease - free survival after resection of extrahepatic cholangiocarcinoma11 and for overall survival in lymph - node negative intrahepatic cholangiocarcinoma14 and gallbladder cancer.10 these results make angiogenesis a logical target for treatment of biliary tract cancer . cediranib is an oral vegfr1 , vegfr2 , and vegfr3 tyrosine kinase inhibitor , with additional activity against pdgf receptors and c - kit.15 although the maximum tolerated dose of cediranib was not reached in a phase 1 study16 in patients with lung cancer , the recommended dose was 30 mg once a day in combination with cisplatin and gemcitabine ( using a di erent schedule to that of the abc - 02 study , namely 1250 mg / m gemcitabine on days 1 and 8 and 80 mg / m cisplatin on day 1 every 3 weeks )  . 
however , based on the totality of the available safety , tolerability , e cacy , pharmacokinetic , and pharmacodynamic data at the time of study setup , the manufacturers recommended dose of 20 mg cediranib once a day for combination with chemotherapy regimens was selected for this trial . in this trial , abc - 03 , we aimed to assess the e ect of the addition of cediranib to standard cisplatin and gemcitabine chemotherapy on progression - free survival in patients with advanced biliary tract cancer . investigator - initiated methods study design and participants in this multicentre , randomised phase 2 , double - blind , placebo - controlled , study , we recruited patients aged 18 years or older with a histopathological or cytological diagnosis of non - resectable , recurrent , or metastatic biliary tract carcinoma ( intrahepatic or extrahepatic cholangiocarcinoma ) , gallbladder , or ampullary carcinoma from hepatobiliary oncology referral centres in the uk . 
patients were eligible if they had an eastern cooperative oncology group ( ecog ) performance status of 01 and an estimated life expectancy of longer than 3 months . [ if patients were required to have adequate haematological function ( haemoglobin 10 g / dl ; white blood cell count 30 10 cells per l ; absolute neutrophil count 15 10 cells per l and platelet count 100 10 per l ) , hepatic function ( total bilirubin 15 times the upper limit of normal except for patients with known documented cases of gilberts syndrome ; alanine aminotransferase or aspartate aminotransferase 25 times the upper limit of normal liver metastases were present , alanine aminotransferase or aspartate aminotransferase had to be less than ve times the upper limit of normal ] and alkaline phosphatase less than or equal to ve times the upper limit of normal ) , and renal function ( serum urea < 15 times the upper limit of normal , serum creatinine < 15 times the upper limit of normal , and calculated glomerular ltration rate 45 ml / min using a validated creatinine clearance calculation such as cockroft - gault or wright formula [ if the calculated glomerular ltration rate was below 45 ml / min , an isotopic method was done to con rm the glomerular ltration rate was 45 ml / min ] )  . 
additionally , patients could not have evidence of active uncontrolled infection 968 vol 16 august 2015 articles ( patients on long - term antibiotics were eligible provided signs of active infection had resolved ) and women of childbearing potential were required to have a negative pregnancy test before study entry and to be using two methods of adequate contraception , which was to be continued for 3 months after completion of treatment . the following previous treatment was allowed ( provided there had been a full recovery ) : a non - curative operation ( ie , r2 resection [ with macroscopic residual disease ] or palliative bypass surgery only ) ; curative surgery with evidence of non - resectable disease relapse requiring systemic chemotherapy ; radiotherapy ( with or without radio - sensitising low - dose chemotherapy ) for localised disease provided there had been clear evidence of disease progression before inclusion in this study ; adjuvant chemotherapy provided neither gemcitabine nor cisplatin were used and the treatment was completed more than 6 months before trial entry ; and photodynamic treatment provided that there was clear evidence of disease progression at the local site or at a new metastatic site . 
previous systemic chemotherapy locally for advanced or metastatic disease was not allowed . patients were excluded from the study in the event of incomplete recovery ( common terminology criteria for adverse events [ ctcae ] grade > 1 ) from previous anticancer treatment ; unresolved biliary tree obstruction ; continuing severe or uncontrolled systemic diseases which , in the view of the investigator , made it undesirable for the patient to participate in the trial ( eg , unstable or uncompensated respiratory , cardiac , hepatic , or renal disease ) ; or untreated unstable brain or meningeal metastases . 
pregnant or breastfeeding women ; patients with a history of cancer likely to interfere with the response assessment ( exceptions include in - situ carci noma of the cervix treated by conebiopsy or resection , non - metastatic basal or squamous cell carcinomas of the skin , any early stage [ stage i ] cancer adequately resected for cure > 5 years previously ) ; and patients in receipt of treatment with an investigational drug within 30 days before randomisation were excluded . cediranib - directed exclusions included substantial haemorrhage ( > 30 ml bleeding or episode in previous 3 months ) or haemoptysis ( > 5 ml fresh blood ) within 4 weeks of randomisation ; poorly controlled hypertension with resting blood pressure higher than 150 / 100 mm hg in the presence or absence of a stable regimen of antihypertensive treatment , or patients requiring maximum doses of calcium channel blockers to stabilise blood pressure ; proteinuria of greater than + 1 on two consecutive dipsticks taken no less than 1 week apart , unless urinary protein less than 15 g in 24 h or protein to creatinine ratio less than 15 ; a mean qtc with bazetts correction longer than 480 ms in screening ecg or history of familial long qt syndrome ; recent major thoracic or abdominal surgery ( < 14 days ) before randomisation , or an incompletely healed surgical incision ; known hypersensitivity to cediranib or any of its excipients ; or a history of gastrointestinal impairment that would substantially a ect the absorption of cediranib or placebo . 
because of the intensity of laboratory processing of blood products , we also excluded patients with known risk of transmitting hiv , hepatitis b or c via infected blood . the trial was done according to the principles of the international conference on harmonisation of good clinical practice . 
all patients provided written informed consent before randomisation . randomisation and masking patients were randomly assigned ( 1 : 1 ) to receive either cediranib or matching placebo in addition to cisplatin and gemcitabine chemotherapy . 
treatment was assigned by computer ( undertaken centrally at ucl cancer trials centre , uk ) with a minimisation algorithm incorporating the strati cation factors : extent of disease ( locally advanced vs metastatic ) , primary disease site ( gallbladder vs bile duct vs ampulla ) , previous treatment ( none vs adjuvant chemotherapy vs other ) , ecog performance status ( 0 vs 1 ) and randomising site , and including a random element . supply and allocation of oral drug packs was managed by an interactive web - based response system ( cenduit , stirling , uk )  . 
an emergency unmasking procedure was established at each study site for patient safety . procedures once deemed eligible at study screening , all patients received 25 mg / m cisplatin and 1000 mg / m gemcitabine chemotherapy , each on days 1 and 8 of a 21 day cycle , continued to eight cycles in the absence of disease progression . 
treatment was discontinued in the event of disease progression , unacceptable adverse events , intercurrent illness preventing further treatment , a patients decision to withdraw consent , or any alteration in the patients condition justifying discontinuation in the site investigators opinion . 
in these cases , patients remained within the trial for the purposes of follow - up and data analysis according to the treatment group to which they were allocated . disease status was assessed by ct scans ( and mri scans , if appropriate ) at baseline , and every 3 months until disease progression ( including patients who discontinued treatment for any reason other than disease progression )  . 
to proceed with administration of full dose gemcitabine and cisplatin on days 1 and 8 of each cycle the following were required : white blood cell count of 2 10 cells per l or higher , absolute neutrophil count of 1 10 cells per l or higher , platelets 100 10 per l or higher , and glomerular ltration rate of 45 ml / min or higher . 
if a second deferral was needed , the treatment was omitted and the patient moved on to the next treatment cycle . only one dose reduction for cediranib , from 20 mg once a day to 15 mg once a day ( or placebo equivalent , maintaining treatment masking ) , was allowed . 
dose interruptions were used as the rst approach to manage adverse events related to cediranib ; for adverse events of grade 3 or more , dosing with cediranib or placebo was interrupted . 
 for patients with several low - grade adverse events ( eg , diarrhoea , weight loss , dehydration , and fatigue ) short dose interruptions ( ie , 25 days ) of the cediranib or 124 patients assessed for eligibility 62 randomly assigned to cediranib 62 received the allocated intervention allocation 62 randomly assigned to placebo 60 received the allocated intervention 2 did not start cisplatin and gemcitabine and allocated intervention ( not t for treatment ) 29 completed eight cycles of cisplatin and 29 completed eight cycles of cisplatin and gemcitabine gemcitabine 33 discontinued cisplatin and gemcitabine 31 discontinued cisplatin and gemcitabine 9 disease progression 5 symptomatic deterioration 2 clinician choice 1 patient decision 16 toxic eects reason why oral treatment was discontinued : 27 disease progression 24 toxic eects 5 symptomatic deterioration 3 patient decision 1 intercurrent illness 1 delay in taking oral treatment 1 did not start cediranib follow - up 18 disease progression 4 symptomatic deterioration 2 clinician choice 2 patient decision 5 toxic eects reason why oral treatment was discontinued : 34 disease progression 15 toxic eects 4 symptomatic deterioration 2 clinician decision 1 patient decision 1 delay in taking oral treatment 3 had oral treatment unblinded 3 lost to follow - up 0 lost to follow - up 62 patients analysed analysis 62 patients analysed figure 1 : trial pro le 970 placebo tablets were instituted . 
if the adverse event was deemed related to cediranib and did not resolve to grade 1 or lower with maximum supportive care and following a dose delay of up to 14 days , cediranib or placebo was restarted at 15 mg once a day . 
if the adverse event failed to resolve , and it was regarded as medically appropriate , cediranib or placebo was permanently discontinued ; if cediranib or placebo could not be restarted at either full or reduced dose after 14 days , it was permanently discontinued . 
where possible , cediranib or placebo was suspended for 2 weeks to allow clearance before any major surgery , if required . blood was collected from patients for exploratory biomarker studies and processed into edta plasma at up to 11 timepoints ; a rst pretreatment baseline sample , a second pretreatment baseline sample on day 1 of the rst cycle then on the rst day of cycles 28 , at the end of chemotherapy , and 1 month after the end of chemo therapy . 
 we measured circulating markers of angio genesis ( vegfa , vegfc , vegfr1 , vegfr2 , ang1 , ang2 , fgfb , hgf , pdgfbb , kgf , plgf , tie2 , and sdf1b ) and in ammation ( interleukin 6 and interleukin 8 ) with a validated multiplex elisa platform ( aushon biosystems , billerica , ma , usa ) , according to good clinical practice ( gcp ) standards at the cancer research uk manchester institute ( manchester , uk ) .17 con centrations of circulating total ck18 , released from epithelial cells during death ( apoptosis and necrosis ) , were measured with an m65 elisa ( peviva , nacka , sweden ) , also previously validated and implemented to gcp as described.18 whole blood ( 10 ml ) was collected in cellsave tubes at up to four timepoints ( pretreatment baseline sample , on day 1 of cycles two and ve , and 1 month after the end of chemotherapy ) for enumeration of circulating tumour cells with the cellsearch platform ( janssen diagnostics , south raritan , nj , usa ) within 4 days of blood draw.19 brie y , after immunomagnetic capture of epcampositive cells , immunophenotyping using cytokeratin ( ck ) , dapi , and cd45 allowed classi cation of circulating tumour cells as epcam + , ck + , dapi + , and cd45 . only results of the baseline circulating biomarker values are presented in this report ; analysis of cell - free dna , detailed biostatistics of longitudinal samples and exploratory analysis by subgroup ( in view of the biological heterogeneity of biliary tract cancers ) is in progress and will be published separately . outcomes the primary endpoint was progression - free survival ; secondary endpoints were overall survival , response by recist ( version 1.1 ) , assessment of adverse events , and vol 16 august 2015 articles quality of life . 
samples were also taken for exploratory biomarker analysis ( including archival tumour tissue , and blood samples for circulating tumour cells and a panel of angiogenesis elisas )  . statistical analysis the trial was designed to directly compare progressionfree survival between the two treatment groups , with 80% power and a two - sided alpha of 02 , to detect a progression - free survival hazard ratio ( hr ) of 064 . 
if the hr was less than 1 and the p value was less than 02 , the study would be deemed to have provided su cient evidence to do a larger trial , after considering toxic e ects , with a high threshold of activity . 
 * 33 patients had surgery only ( 16 in the cediranib group and 17 in the placebo group ) and 12 had surgery plus biliary stent insertions ( seven in the cediranib group and ve in the placebo group )  . 
 table 1 : baseline characteristics based on seeing an improvement in the median progression - free survival from 8 months to 125 months , with recruitment lasting for 18 months and patients followed up for 12 months beyond last recruitment ; requiring 92 progression - free survival events . 
 during the conduct of the study , the end of recruitment became xed by date ( sept 30 , 2012 ) rather than by accrual following the decision by the manufacturer to cease development of cediranib ; consequently , the power of the study was reduced to 75% and the target sample size adjusted accordingly to include at least 116 patients . we plotted kaplan - meier curves for progression - free survival and overall survival ; treatment e ect hr ( with 80% and 95% cis and p values ) were obtained from cox proportional hazards regression models . 
duration of response was measured from the date the best overall response was documented to the date of progression - free survival event . all treatment - emergent adverse events reported are presented and summarised as frequencies ; we used pearsons test of association to formally compare grade 34 adverse events occurring in at least ten patients . 
 we used the kaplan - meier method and cox regression model to compare the median time on each treatment . the associations of biomarkers ( elisa , total ck18 [ m65 ] , circulating tumour cell count , cea , ca19 - 9 , and ca125 ) with overall survival and progression - free survival were assessed with cox regression models . 
all overall survival and progressionfree survival models were adjusted for treatment group and baseline characteristics ( age , sex , ecog performance status , primary site , stage , and previous treatment )  . 
study conduct was overseen by an independent trial management group had access to all the raw data and take full responsibility for the integrity of the data and accuracy of the data analysis . 
the results between april 5 , 2011 , and sept 28 , 2012 , 124 patients were recruited from 14 uk sites ( tertiary hepatobiliary oncology referral centres ; appendix )  . 
the 972 vol 16 august 2015 articles placebo cediranib hr 093 ( 80% ci 074119 ) , p = 072 median patient age was 651 years , 50% of patients were men , and most patients ( 84% ) had metastatic disease . 
 most patients had primary tumours arising from the bile ducts ( 62% ) followed by gallbladder cancer ( 31% ) and ampullary tumours ( 6% ) ; there was a slight preponderance of patients with performance status of 1 ( 56% ) compared with a performance status of zero ( 44% )  . 
at the time of analysis ( april 28 , 2014 ) , the estimated median follow - up in all patients using censored deaths method was 122 months ( iqr 7318.5 ) ; 116 ( 94% ) patients had experienced disease progression and 100 ( 81% ) patients had died . table 2 summarises the incidence of adverse events by grade 12 and grade 34 . 
we noted no signi cant di erence between treatment groups with respect to grade 34 haematological toxic e ects , although patients receiving cediranib had more frequent grade 34 decreased platelet counts ( table 2 )  . 
we recorded a signi cantly higher incidence of grade 34 hypertension , diarrhoea , and fatigue in patients given cediranib than in those given placebo ( table 2 )  . 
in the cediranib group , there was one death attributed to treatment ( myocardial infarction ) and one death related to both cancer and treatment ( gastric haemorrhage )  . 
in the placebo group , there were three deaths attributed to treatment ( one due to peripheral ischaemia and stroke ; one due to cardiac arrest ; and one to pulmonary embolism , superior vena cava due obstruction , and metastatic gallbladder cancer )  . compared with placebo there was no signi cant di erence in the median duration of treatment ( ie , time on treatment ) with ( 46 months cediranib [ 95% ci 2880 ] with cediranib vs 55 months [ 2878 ] with placebo , hr 100 [ 95% ci 070144 ] ; p = 098 )  . 
 however , more patients the cediranib group discontinued oral treatment because of toxic e ects ( 24 in the cediranib group vs 15 in the placebo group ; gure 1 )  . 
additionally , 14 ( 23% ) of 62 patients had at least one dose reduction and 60 ( 97% ) had at least one treatment suspension in a speci c cycle or month in the cediranib group compared with four ( 7% ) of 60 and 52 ( 87% ) of 60 patients in the placebo group , respectively . 
 allocation of patients to cediranib did not a ect the delivered dose intensity of either cisplatin or gemcitabine ( data not shown )  . at the time of data cuto , 59 progression - free survival events had occurred in the cediranib group as had 57 in the placebo group . 
we noted no signi cant di erence in median progression - free survival , the primary endpoint of the study , between patients given cediranib versus placebo [ 95% ci 6593 ] with cediranib vs ( 80 months 74 months [ 5785 ] with placebo , hr 093 [ 80% ci 074119 , 95% ci 065135 ] ; p = 072 )  . 
6 - month progression - free survival was 705% ( 95% ci 574803 ) number at risk placebo cediranib hr 086 ( 95% ci 058127 ) , p = 044 number at risk placebo cediranib time since randomisation ( months ) figure 2 : kaplan - meier curves for progression - free survival ( a ) , and overall survival ( b ) by treatment in patients receiving cediranib and 613% ( 480721 ) in patients receiving placebo ; 12 - month progression - free survival was 218% ( 95% ci 124329 ) in the cediranib group and 161% ( 83263 ) in the placebo group ( gure 2a )  . 
strati ed analyses based on sex , age , ecog performance status , primary tumour site , disease status , histological grade , previous treatment , and ca19 - 9 did not identify any outliers ( appendix )  . most patients ( 113 [ 91% ] ; 59 in the cediranib group and 54 in the placebo group ) had measurable disease at baseline . 
the / xx shows the per unit increase ; for example , for cea for every 10 g / l increase , the hazard increases by 3% ( hr 103 )  . 
as a result , disease control was achieved by 46 ( 78% ) patients in the cediranib group and by 35 ( 65% ) in the placebo group ( p = 012 )  . 
the median duration of response was 51 months ( range 2224 ) in the cediranib group ( 26 events in 26 patients ) and 58 months ( 05224 ) in the placebo group ( seven events in ten patients )  . 
six ( 10% ) patients in the cediranib group and 15 ( 28% ) in the placebo group had progressive disease ( including symptomatic progressions [ ie , not objectively obsessed ] in three in the cediranib group and four in the placebo group )  . 
seven ( 12% ) patients in the cediranib group and four ( 7% ) in the placebo group had an unknown best overall response . at data cuto , 50 ( 81% ) patients in the cediranib group and 50 ( 81% ) in the placebo group had died . 
median overall survival was 141 months ( 95% ci 102164 ) in patients given cediranib and 119 months ( 92143 ) in patients given placebo ( hr 086 , 95% ci 058127 ; p = 044 )  . 
 6 - month overall survival was 853% ( 95% ci 736921 ) in the cediranib group and 790% ( 666872 ) in the placebo group ; at 12 months , 581% ( 95% ci 445694 ) of patients receiving cediranib were alive compared with 484% ( 355601 ) of patients in the placebo group ( gure 2b )  . 
 we recorded no di erence in median overall survival postprogression on rst - line treatment received in this study ( cediranib 45 months [ 95% ci 2864 ] , placebo 43 months [ 3361 ] , hr 09 [ 059137 ] ; p = 062 )  . baseline ca19 - 9 was raised in 71 ( 68% ) of 105 patients ; an additional 23 ( 22% ) of patients with normal ca19 - 9 concentrations had an increased baseline cea or ca125 ; and 11 ( 10% ) patients had normal levels of all three the tumour markers association between baseline tumour markers and overall survival ( treatment - adjusted hrs ) showed that increased baseline ca19 - 9 concentration was associated with an increased risk of death ( table 3 )  . 
cox models for number at risk < 557725 557725 to < 753613 753613 time since randomisation ( months ) figure 4 : kaplan - meier curves for overall survival , by number of circulating vegfr2 in the plasma , before treatment 974 vol 16 august 2015 articles placebo cediranib hr 147 ( 95% ci 083261 ) , p = 019 total ck18 concentrations were also prognostic , with raised baseline concentrations associated with a shorter overall survival ( table 3 )  . blood samples for circulating tumour cell enumeration were available from 95 patients before treatment ; 51 ( 54% ) of 95 patients had a circulating tumour cell count of no cells per 75 ml blood , 21 ( 22% ) had a count of one cell per 75 ml blood , and 23 ( 24% ) had a count of two cells or higher per 75 ml blood , with a median of 0 per 75 ml blood and mean of 2 per 75 ml blood ( range 044 per 75 ml blood )  . 
this same pattern was shown when the circulating tumour cell variable was divided into tertiles ( 1 vs 0 , hr 325 [ 95% ci 181583 ] ; 2 vs 0 , hr 300 [ 173522 ] , p < 00001 ; gure 3 )  . 
patients with no circulating tumour cells in their blood sample had the best overall survival ( median 181 months [ 95% ci 121249 ] ) ; the presence of one ( median 103 months [ 95% ci 47144 ] ) or two or more circulating tumour cells ( median 87 months [ 95% ci 71126 ] ) was strongly associated with a worse overall survival . most of the circulating angiogenesis - related biomarkers ( vegfa , vegfc , vegfr1 , ang1 , ang2 , fgfb , hgf , pdgfbb , kgf , plgf , tie2 , and sdf1b ) and the in ammatory biomarkers ( interleukin 6 and inter leukin 8 ) did not show prognostic signi cance for overall survival ( data not shown )  . 
however , when adjusted for treatment and baseline characteristics , we noted that raised concentrations of baseline vegfr2 were associated with an increased risk of death ( table 3 )  . 
this same pattern could be seen when we assessed vegfr2 by tertiles ( gure 4 )  . we recorded an interaction between baseline pdgfbb concentrations and treatment with cediranib for overall survival ; with the median as the cuto , we noted that patients with concentrations below the median did not bene t from cediranib ( gure 5a ) whereas patients with pdgfbb concentrations higher than the median derived bene t from cediranib in terms of overall survival ( pinteraction = 0002 ; gure 5b and appendix )  . 
sorafenib ( an oral multi - tyrosine kinase inhibitor ) was deemed to have low activity as monotherapy , albeit in a mainly second - line setting ; 20 bevacizumab ( a monoclonal antibody against vegf ) with erlotinib ( an oral egfr inhibitor ) was feasible in the rst - line setting although , with a median overall survival of 99 months , does not seem better than upfront chemotherapy.21 in another study , 22 bevacizumab was tolerable in combination with gemcitabine and oxaliplatin ; however , we could not work out the vol 16 august 2015 articles incremental value of the anti - angiogenic in this singlegroup study . 
most recently ( contemporaneous to our study ) , sorafenib has failed to improve progression - free survival when added to gemcitabine in a randomised phase 2 , placebo - controlled study of 102 patients.23 our approach is the rst to build on the cisplatin and gemcitabine chemotherapy regimen , now established as a reference regimen ; we assessed the e ect of adding cediranib , a pan - vegf receptor tyrosine kinase inhibitor with activity against pdgf receptors and c - kit in a placebo - controlled manner . 
despite this shortcoming , some e cacy ndings warrant additional attention ; namely signicantly greater number of overall responses and proportion of patients who achieved disease control in those receiving cediranib , mainly at the rst ( 3 month ) reassessment scan . 
response is notoriously di cult to assess in patients with biliary tract cancer , although the risk of bias this could introduce was mitigated by the use of a placebo control in this study . 
irrespective , patients remained on cediranib for a median of 46 months , stopping earlier the median progression - free survival ( 80 months ) , mainly because of toxic e ects ; moreover , the proportion of patients stopping treatment because of toxic e ects was higher in the cediranib group than the the placebo group . 
an examination of progression - free survival kaplan - meier curves suggests a separation in the period during which cediranib was tolerated , which rapidly converged after the median cessation point of cediranib . 
these data suggest that cediranib is e ective during the period of treatment but toxic e ects leading to cessation prevent longer - term bene t ; we postulate that a better - tolerated anti - vegf treatment might potentially result in overall bene t in combination with cisplatin and gemcitabine . than we did not note any unexpected safety signals ; the addition of cediranib to cisplatin and gemcitabine did result in a signi cantly greater incidence of grade 34 toxic e ects , which were mainly expected o - target toxic e ects for vegf inhibitors ( namely hypertension and diarrhoea )  . 
however , these toxic e ects were clearly signi cant in this study and need to be considered in any future angiogenesis - targeting studies . the e ect on the quality of life of patients is important in the event that the study had shown bene t from the addition of cediranib as part of the assessment of the relative merits of a potentially new agent . 
however , because there was no improvement in progression - free survival , quality - of - life ndings from this study will be reported separately , most likely in a pooled analysis with that of other studies of advanced biliary tract cancer . we assessed surrogates of disease volume and biology ( other than radiological extent ) including assessment of the tumour markers ca19 - 9 , cea , and ca125 and total ck18 . 
the role of ca19 - 9 as a marker of volume of disease , prognostic factor , and measure of response to treatment is well documented.24 however , because this is linked to the lewis blood - group antigen , not all patients express this ( 32% were ca19 - 9 - negative in our series )  . 
 we have been able to show that in roughly one in ve cases ( 22% ) , cea or ca125 might be used as an alternative and that each of these also has prognostic value , with increased baseline levels independently correlating with an adverse overall survival . cancers of epithelial origin contain large intracellular pools of cytokeratins ; during necrotic or apoptotic cell death ck18 and other cytokeratins are released into the blood in either their intact or their caspase - cleaved forms where they remain stable in the circulation.25 ck18 is proposed as a surrogate biomarker of drug - induced epithelial cell death26 and thus might not only represent epithelial tumour cell death but may also re ect toxic e ects in epithelial host tissues . 
we have shown here for the rst time , to the best of our knowledge , that increased baseline ck18 levels are adversely prognostic in biliary tract cancer , consistent with our previous ndings in colorectal cancer.27 the presence of circulating tumour cells is prognostic in a number of cancer types including prostate , breast , and colorectal cancers where cellsearch enumeration of circulating tumour cells is approved by the us food and drug administration for prognosis and monitoring . 
we have shown that circulating tumour cells number by cellsearch is also prognostic in lung cancer , 28 , 29 pancreatic cancer , 30 hepatocellular carcinoma , 31 and melanoma.32 our study is , to the best of our knowledge , the rst to show the presence of circulating tumour cells in patients with biliary tract cancer and , moreover , that the presence of one or more circulating tumour cells per 75 ml of blood is associated with an adverse prognosis . 
this nding ( subject to further validation ) could not only inform future study design , but might also serve as a platform for longitudinal surveillance of disease behaviour both in terms of circulating tumour cell enumeration and detailed molecular analysis of individual cells . as previously discussed , vegf and its receptors are overexpressed in patients with biliary tract cancer ; correlating with the presence of metastases and an adverse prognosis . 
baseline vegfr2 levels are associated with progression - free survival ( but not overall survival ) in cediranib studies in hepatocellular carcinoma , 33 although were not prognostic ( for progression - free survival or overall survival ) in colorectal cancer.34 assessment of a panel of angiogenesis - associated biomarkers in our study identi ed vegfr2 as a novel adverse prognostic marker for overall survival in this disease group ; however , despite this being a major target of cediranib with pharmacodynamic properties reported in the phase 1 study , 35 976 vol 16 august 2015 articles baseline concentrations were not associated with a treatment e ect ( ie , were not predictive )  . pdgf , a mitogen chemotactic factor promoting wound healing , neoplastic transformation , and tumour pathogenesis , is a dimeric molecule that , when active , exists either as a homodimer or a heterodimer of a and b chains.36 in - vitro and in - vivo studies have identi ed that myo broblast - derived pdgfbb is potentially cytoprotective to cholangiocarcinoma cells by inhibition of the trail ( death ligand ) cytotoxicity.37 in our study , increased baseline levels of pdgfbb , one of the targets of cediranib , was associated with a bene t from cediranib consistent with a potential role as a predictive biomarker ; this nding would need to be validated in an independent cohort . in summary , the addition of cediranib to cisplatin and gemcitabine chemotherapy did not improve progressionfree survival . 
however , vegf inhibition might still be an avenue worth pursuing , perhaps with an agent that has a toxic e ect pro le that allows more sustained dosing with cisplatin and gemcitabine than cediranib . 
integration into future trial designs of the circulating biomarkers identi ed in our study ( vegfr2 , total ck18 in addition to the tumour markers ca125 , cea , and ca19 - 9 ) will depend on validation of their utility . 
finally , our identi cation of circulating tumour cells in patients with biliary tract cancers will allow risk strati cation via circulating tumour cell enumeration and , coupled with our recently developed protocols for circulating tumour cell isolation and single cell genomic and transcriptomic pro ling , 38 , 39 could open up new avenues for minimally invasive monitoring and delivery of precision medicine for these patients . contributors abc - 03 was developed though and supported by the hepatobiliary subgroup of the uk national cancer research institute upper gi clinical studies group and was led by the trial management group composed of jwv , jab , hw , sb , md , al , and acb . 
md and sb were responsible for the conduct of the trial , ensuring all required approvals were in place , and for collection and veri cation of the integrity of the data . 
jwv reports personal fees from p zer , grants , personal fees , and nonnancial support from novartis , personal fees from abbott , personal fees and nonnancial support from celgene , personal fees from sirtex , personal fees and nonnancial support from ipsen , grants , and personal fees from astrazeneca pharmaceuticals , outside the submitted work . 
daa , acb , pc , cd , md , al , sm , am , km , dhp , cr , pjr , and wps declare no competing interests . acknowledgments this study was funded by cancer research uk ( grants cruk / 09 / 029 , c2930 / a11428 , and c480 / a15578 ) and astrazeneca pharmaceuticals . 
we also acknowledge the support of the ammf cholangiocarcinoma charity and support and insights from the international biliary tract cancer collaboration . editorial for the grail website see liquid cancer biopsy : the future of cancer detection ? this years jp morgan annual healthcare conference ( jan 1115 , 2016 ) in san francisco , ca , usa , saw the announcement of a new biotechnology company called graila spino from illumina ( san diego , ca , usa ; one of the worlds largest diagnostics companies )  . 
chaired by the illumina chief executive o cer jay flatley , and with a science advisory board headed by jos baselga ( memorial sloan kettering cancer center , new york , ny , usa ) , grail declared its mission to be the early detection of cancer in asymptomatic individuals through a blood screen . 
 the notion of cancer detection by liquid biopsy is not a new concept : indeed , many other companies are also developing blood - based tests to monitor cancer progression or screen high - risk asymptomatic individuals . 
however , such tests to date have focused on speci c cancer types , rather than a single test to detect all aysmptomatic cancers based on circulating tumour dna ( ctdna )  . 
is this objective possible ? and what are the wider implications for patients with cancer ? the presence of ctdna in the blood of patients with cancer is a well - recognised phenomenon and increasingly well - characterised in many cancers . 
but increased sensitivity can lead to increased genetic noise , which in turn , can make it di cult to di erentiate between tumour - associated dna mutations and non - tumour - associated dna mutationsleading to an increased risk of false positives . 
crucially , there are also other questions to address , such as what exactly the test would detect and what it could di erentiate betweeneg , not all cancers are associated with discrete and consistent early genetic mutations and many have multiple mutations that can arise at any disease stage in an unpredictable manner . 
rather , research has shown that ctdna concentrations are not only directly correlated with tumour burden , but also with ease of transit into the bloodstream overcoming obstacles such as the bloodbrain barrier or mucinous tissues . 
finally , any new diagnostic test must undergo clinical validationa necessary step for regulatory approval and far from trivial . another issue is what clinicians and the public will do with the information from a pan - tumour test . 
 overtreatment can severely worsen quality of life ; for example , present guidelines in several parts of the world no longer advocate prostatectomy on the basis of screening results and instead recommend watch - and - wait strategies . 
thus , if a universal cancer test shows a true positive , should the individual be treated immediately ? furthermore , if a positive result was found in a population - based screening programme with a universal marker , what would be the implications for obtaining health insurance for asymptomatic patients who might not need treatment for years , or at all ? and a further paradox could arise for those cancers detected that have no curative treatment . 
no matter how early some cancers are found and what treatment options are available to palliate symptoms , is the trade - o between early detection and psychological distress really a desired outcome ? the use of venture capitalists and tight timelines in grails undertaking re ects a growing trend in clinical and scienti c research of attacking a speci c scienti c or clinical problem with massive resourcesabout us$100 million in this casecombined with public demand for rapid solutions . 
ambition in some cases exceeds the realities and feasibility of a solution , and projects can become too narrowly focused on speci c avenues of research in an attempt to meet deadlines . 
 it is possible that a focus on ctdna over - and - above other biomarkers and networks in tumour biology , such as immune signatures , proteomes , kinomes , microbiomes , and other multifactorial interactions in the tumour microenvironment and host response , might be an oversimpli cation . 
in the eortc trial , eligible women had biopsy - proven international federation of gynecology and obstetrics ( figo ) stage iiic or iv invasive epithelial tubo - ovarian carcinoma . 
the main aim of the pooled analysis was to show noninferiority in overall survival with neoadjuvant chemotherapy compared with upfront debulking surgery , using the reverse kaplan - meier method . 
tests for heterogeneity were based on cochrans q heterogeneity statistic . findings data for 1220 women were included in the pooled analysis , 670 from the eortc trial and 550 from the chorus trial . 
55 ( 5% ) women had figo stage iiiiib disease , 831 ( 68% ) had stage iiic disease , and 230 ( 19% ) had stage iv disease , with staging data missing for 104 ( 9% ) women . 
in the entire population , no difference in median overall survival was noted between patients who underwent neoadjuvant chemotherapy and upfront debulking surgery ( 276 months [ iqr 141513 ] and 269 months [ 127501 ] , respectively ; hazard ratio [ hr ] 097 , 95% ci 086109 ; p = 0586 )  . 
median overall survival for eortc and chorus patients was significantly different at 302 months ( iqr 157537 ) and 236 months ( 105469 ) , respectively ( hr 120 , 95% ci 106136 ; p = 0004 ) , but was not heterogeneous ( cochrans q , p = 017 )  . 
women with stage iv disease had significantly better outcomes with neoadjuvant chemotherapy compared with upfront debulking surgery ( median overall survival 243 months [ iqr 141476 ] and 212 months [ 100364 ] , respectively ; hr 076 , 95% ci 058100 ; p = 0048 ; median progression - free survival 106 months [ 79150 ] and 97 months [ 52132 ] , respectively ; hr 077 , 95% ci 059100 ; p = 0049 )  . interpretation long - term follow - up data substantiate previous results showing that neoadjuvant chemotherapy and upfront debulking surgery result in similar overall survival in advanced tubo - ovarian cancer , with better survival in women with stage iv disease with neoadjuvant chemotherapy . 
 we found that survival data from randomised studies had been published for only two trials : the european organisation for research and treatment of cancer ( eortc ) 55971 trial , and the medical research council chemotherapy or upfront surgery ( chorus ) trial . 
both trials concluded that neoadjuvant chemotherapy followed by interval debulking surgery was not inferior to primary debulking surgery followed by chemotherapy in patients with international federation of gynecology and obstetrics ( figo ) stage iiic or iv ovarian carcinoma . 
in addition to these two trials , the scorpion and jcog0602 randomised trials concluded that perioperative morbidity was better with interval debulking after neoadjuvant chemotherapy than after primary debulking surgery . added value of this study we report a per - protocol pooled analysis of individual patient data from the eortc 55971 and chorus randomised trials , to examine the long - term outcomes in patients with advanced ovarian cancer treated with neoadjuvant chemotherapy followed by interval debulking versus upfront debulking surgery followed by chemotherapy . 
we also did subgroup analyses on the basis of stratification factors that were common to both trialsie , randomising centre , largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 cm to 20 cm , and > 20 cm ) , and clinical figo stage . 
our analysis shows that , with longer median follow - up , both neoadjuvant chemotherapy followed by interval debulking surgery and upfront debulking surgery followed by chemotherapy are associated with similar overall survival and progression - free survival . 
we also show that neoadjuvant chemotherapy is associated with better progression - free survival and overall survival in women presenting with figo stage iv disease , and patients with figo stage iiic disease with extrapelvic metastases smaller than 5 cm have better progression - free survival after upfront debulking . implications of all the available incidence earlier studies showed already that overall survival is similar in patients with stage iiiciv tubo - ovarian cancer treated with neoadjuvant chemotherapy followed by interval debulking surgery , compared with upfront debulking surgery followed by chemotherapy . 
participants in this study had figo stage iiic or iv tubo - ovarian cancer with metastatic disease with a high tumour burden at presentation , and many had a poor performance status . 
this individual patient data pooled analysis suggests that neoadjuvant chemotherapy should be the standard of care for most patients with stage iv tubo - ovarian cancer and that primary surgery should only be undertaken in exceptional circumstances in patients with figo stage iv disease on an individual basis . 
however , women with figo stage iiic disease with extrapelvic metastases smaller than 5 cm had a significantly better progression - free survival with upfront debulking surgery than with neoadjuvant chemotherapy , so these patients should first be considered for primary debulking surgery . 
in 2010 , the european organisation for research and treatment of cancer ( eortc ) published the first findings from a trial comparing neoadjuvant chemotherapy followed by interval debulking surgery with upfront debulking surgery ( eortc 55971 ) .4 this study showed both treatment strategies had similar overall survival and progression - free survival in women with international federation of gynecology and obstetrics ( figo ) stage iiic or iv tubo - ovarian cancer , and operative and postoperative morbidity was lower with neoadjuvant chemotherapy . 
these results were later substantiated in the randomised medical research council ( mrc ) chemotherapy or upfront surgery ( chorus ) trial , 5 leading to the acceptance of neoadjuvant chemotherapy followed by interval debulking surgery as an alternative to upfront debulking surgery in women with stage iiic and iv tubo - ovarian cancer.6 however , the selection of women with advanced ovarian cancer for neoadjuvant chemotherapy or upfront debulking surgery remains controversial.7 therefore , we did a pooled analysis of the long - term outcomes of the eortc 55971 and chorus trials to identify subgroups of women who could benefit from neoadjuvant chemotherapy in this setting . 
 that might benefit see online for appendix vol 19 december 2018 1681 articles n the trial steering committees of both the eortc and chorus trials agreed on a strategy for database pooling and analyses ; both trials had similar eligibility criteria , treatment , and examination schedules to facilitate pooling 2 studies prospectively selected for database pooling 1220 patients records screened 670 patients enrolled in eortc 550 patients enrolled in chorus 1220 individual patient data included in synthesis ( pooled analysis ) figure 1 : prisma flow diagram eortc = european organisation for research and treatment of cancer 55971 trial . 
eortc = european organisation for research and treatment of cancer 55971 trial . table 1 : baseline characteristics , by study eligibility criteria for these trials and their study designs have been reported elsewhere.4 , 5 the appendix includes the protocols of the eortc ( pp 1270 ) and chorus ( pp 71117 ) trials . 
a list of recruiting sites and investigators is also in the appendix ( pp 122124 )  . briefly , in the eortc trial , 4 women were eligible if they had biopsy - proven figo stage iiic or iv invasive epithelial ovarian , primary peritoneal , or fallopian tube carcinoma . 
 if a biopsy specimen was not available , fine - needle aspiration showing an adeno carcinoma was acceptable under the following conditions : presence of a pelvic adnexal mass , presence of extrapelvic metastases of 2 cm or larger ( measured during dia gnostic laparoscopy or laparotomy , or if laparoscopy or laparotomy was not done , on the basis on ct findings ) , and a ratio of cancer antigen 125 ( ca125 ) to carcino embryonic antigen ( cea ) greater than 25 ; biopsy findings were mandatory for inclusion in the trial if any of these three criteria were not present . 
the size of the largest metastasis was estimated on the basis of ct imaging only in the chorus trial . in both trials , participants were randomly allocated to receive either upfront debulking surgery followed by at least six courses of platinum - based chemotherapy , three courses of neoadjuvant platinum - based chemotherapy followed by interval debulking surgery followed by at least three additional courses of platinumbased chemotherapy.4 , 5 in women allocated to receive upfront debulking surgery whose surgery was completed without optimum cytoreduction , interval debulking surgery was permitted , and these patients were included for analyses in the upfront debulking surgery group . 
in the eortc trial , randomisation used a minimisation technique and was stratified by the following factors : institution , method of biopsy ( image - guided , laparoscopy , laparo tomy , or fine - needle aspiration ) , figo stage iiic or iv disease , and largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 to 20 cm , or > 20 cm )  . 
in the chorus trial , randomisation used a minimisation method with a random element , which stratified patients according to randomising centre , largest radiological tumour size , clinical figo stage , and prespecified chemotherapy regimen . 
for details on size of residual tumour , residual tumour per country , type of surgery , number of cycles and type of chemotherapy , and time to ( re ) initiation of chemotherapy , we refer to the original reports.4 , 5 procedures our analysis was designed in 2003 by the chief investigators of the eortc and chorus trials ( iv and sk ) and members of the eortc and mrc trial managing committees , according to a formal protocol . 
we derived median follow - up with the eortc standard method , which uses the reverse kaplan - meier method and calculates time - toevents for all patients ; in the original chorus paper , however , only the median duration of follow - up for surviving patients was calculated . the primary outcome of our pooled analysis was overall survival , and the prespecified secondary endpoint was progression - free survival . 
prespecified subgroup analyses were done on the basis of stratification factors that were common to both trials : randomising centre , largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 to 20 cm , and > 20 cm ) , and clinical figo stage . 
definitions for overall survival and progression - free survival have been published elsewhere.4 statistical analysis patients data from both trials were updated and merged into one database ( database lock for eortc was on june 6 , 2015 ; for chorus , june 3 , 2014 ) , which contained 1220 patients with tubo - ovarian cancer who had been randomly allocated to receive either upfront debulking surgery or neoadjuvant chemotherapy . 
assuming a median overall survival of 3 years , this number of events allowed assessment of noninferiority , 9 , 10 with a one - sided type i error of 005 and a power of 80% , with inferiority regarded as an increase of more than 1819% in hazard . 
applying a two - sided test of superiority at 5% , the dataset would allow detection of an 18% increase in hazard with 80% power . the principal analysis was done on an intention - totreat basis . 
 in those subgroups for which the proportional hazards assumption was violated , restricted mean survival times were calculated to provide a more useful general measure than the hr estimates and their 95% cis obtained from a cox proportional hazards model to report the average survival times between the two treatment groups.11 multivariable time - to - event analyses were done using a cox proportional hazards model , with univariate screening followed by a multi variable stepwise selection procedure.12 all baseline characteristics and results were checked for homogeneity between the two studies and stratified per trial when possible . 
all analyses were done with sas , version 9.4. role of the funding source the funders of the studies had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 upfront debulking surgery neoadjuvant chemotherapy hazard ratio 076 , 95% cl 058100 overall score stratied for study , p = 0048 time after randomisation ( years ) number at risk ( number censored ) upfront debulking surgery neoadjuvant chemotherapy 118 ( 0 ) 11 ( 0 ) 53 ( 2 ) 57 ( 1 ) 13 ( 3 ) 25 ( 3 ) 7 ( 3 ) 8 ( 4 ) 2 ( 5 ) 4 ( 6 ) 0 ( 6 ) 2 ( 8 ) figure 4 : overall survival in patients with figo stage iv disease , by treatment figo = international federation of gynecology and obstetrics . overall survival of 276 months ( iqr 141513 ) and 269 months ( 127501 ) , respectively ( hr 097 , 95% ci 086109 ; p = 0586 ) , and progression - free survival of 116 months ( iqr 79177 ) and 111 months ( 64175 ) , respectively ( hr 098 , 95% ci 087110 ; p = 0688 ; figure 2 )  . 
the lower one - sided 95% cis for overall survival and progression - free survival excluded the 18% non - inferiority margin . overall survival was significantly improved in the eortc trial as compared with the chorus trial ( median 302 months [ iqr 157537 ] vs 236 months [ 105469 ] ; hr 120 , 95% ci 106136 ; p = 0004 ; figure 3 ) , but progression - free survival was similar in the two trials ( median 115 months [ iqr 80170 ] vs 109 months [ 61181 ] ; hr 096 , 95% ci 086108 ; p = 0531 ; appendix p 1 )  . 
cochrans q for heterogeneity was not significant for either overall survival ( p = 017 ) or progression - free survival ( p = 032 )  . median overall survival was significantly different for women with figo stage iv disease compared with those with stage iii and ii cancer ( median 233 months [ iqr 124408 ] vs 300 months [ 156557 ] and 454 months [ 316not reached ] , respectively ; for stage iv vs stage ii , hr 275 , 95% ci 149508 ; for stage iii vs stage ii , 192 , 95% ci 105349 ; p < 00001 for trend ; appendix p 4 )  . 
overall survival was similar with neoadjuvant chemotherapy and upfront debulking surgery in patients with stage iiic disease ( respectively , median 308 months [ iqr 165513 ] and 284 months [ 141557 ] ; hr 104 , 95% ci 090121 ; p = 0569 ; appendix p 5 )  . 
progression - free survival was also similar with neoadjuvant chemotherapy and upfront debulking surgery in patients with stage iiic disease ( median 122 months [ iqr 84183 ] and 117 months [ 75199 ] , respectively ; hr 106 , 95% ci 092122 ; p = 0429 ; appendix p 6 )  . 
however , progression - free survival was significantly better in stage iv disease with neoadjuvant chemotherapy than with upfront debulking surgery ( median 106 months [ iqr 79150 ] vs 97 months [ 52132 ] , respectively ; hr 077 , 95% ci 059100 ; p = 0049 ; appendix p 7 )  . 
additionally , in patients with stage iv tubo - ovarian cancer , neoadjuvant chemotherapy was associated with significantly better overall survival than was upfront debulking ( median 243 months [ iqr 141476 ] vs 212 months [ 100364 ] ; hr 076 , 95% ci 058100 ; p = 0048 ; figure 4 )  . 
in patients with figo stage iiic disease and a largest metastatic tumour size less than 5 cm , progression - free survival was better with upfront debulking surgery than with neoadjuvant chemotherapy ( median 122 months [ iqr 85233 ] vs 117 months [ 83164 ] ; hr 136 , 95% ci 106175 ; p = 0017 ; figure 5a ) forest plots for progression - free survival according to largest metastatic tumour size are in the appendix ( p 9 )  . 
overall survival did not differ between upfront debulking surgery and neoadjuvant chemotherapy ( median 330 months [ iqr 135787 ] and 302 months [ 165513 ] , respec t ively ; hr 126 , 95% ci 096165 ; p = 0092 ; figure 5b )  . 
 1684 vol 19 december 2018 articles age and performance status were not predictive for treatment effect on survival ( appendix p 11 ) discussion this preplanned analysis of updated data from the eortc 55971 and chorus trials assessing neoadjuvant chemotherapy versus upfront debulking surgery in advanced tubo - ovarian cancer ( stage iiic and iv ) shows that , with long - term follow - up , neoadjuvant chemotherapy results in non - inferior overall survival and progression - free survival as compared with upfront debulking surgery . 
the planned non - inferiority margin an increase in hr of more than 1819%was well outside the upper bounds of the 95% cis ( 10% and 9% for progression - free survival and overall survival , respectively )  . 
hence , this pooled analysis with long - term follow - up substantiated previous findings showing that both upfront debulking surgery and neoadjuvant chemotherapy are potential treatment options for patients with figo stage iiic or iv tubo - ovarian cancer . 
 the analysis also showed that patients diagnosed with stage iv disease had significantly better progression - free survival and overall survival with neoadjuvant chemotherapy as compared with upfront debulking surgery , whereas women with stage iiic disease with extrapelvic metastases smaller than 5 cm had significantly better progression - free survival with upfront debulking surgery as compared with neoadjuvant chemotherapy . 
our analyses showed that in women with stage iiic disease and extrapelvic metastases at diagnosis smaller than 5 cm , survival curves for both progressionfree survival and overall survival cross in both treatment groups , indicating deviation from the proportional hazards assumptions . 
obtaining tissue for histological examination is usually possible by use of image - guided biopsy ( usually of the omental cake ) , although a laparoscopic approach is necessary in some cases and provides additional information on disease distribution , which can be included in the decision - making process.1517 both the eortc and chorus trials investigated the timing of surgery in advanced tubo - ovarian cancer , but these trials have been criticised for inclusion of low proportions of patients with no macroscopic disease ( r0 ) and because patients with poor prognosis were enrolled and died sooner than expected independent of the timing of surgery . 
however , at the time the patients in these trials were enrolled , neoadjuvant chemotherapy was not accepted as an alternative to upfront debulking surgery , and furthermore most patients recruited to these trials had extensive figo stage iiic or iv disease that was visible on ct . 
moreover , the scorpion15 and jcog060218 randomised trials compared the morbidity of interval debulking surgery after neoadjuvant chemotherapy with upfront debulking surgery and concluded that interval debulking surgery was associated with improved perioperative morbidity as compared with primary debulking surgery . 
a ran domised trial of neoadjuvant chemotherapy versus primary debulking surgery in advanced tubo - ovarian cancer ( the trust trial , nct02828618 ) is recruiting only in centres with historically documented maximum cytoreduction ( r0 ) in patients with stage iii or stage iv tubo - ovarian cancer of at least 50% . 
the results of this trial are awaited . one limitation of our pooled analysis is that only patients with figo stage iiic and iv disease were included in the eortc trial , whereas in the chorus trial a few patients with stage iiia and stage iiib disease were included . 
furthermore , the number of patients with stage iiic and stage iv disease without residual tumour after upfront debulking surgery was lower in the chorus trial than in the eortc trial . application of the findings of this analysis to the care of women with figo stage iiic or iv tubo - ovarian cancer should be assessed in the context of each patients clinical picture . 
women in the eortc and chorus studies that contributed data to this analysis had metastatic disease with a high tumour burden at presentation , and many had a poor performance status.19 this clinical scenario is not uncommon , and improving outcomes for this population is as important as for patients with better prognostic factors . 
our chemotherapy should be the standard of care for most patients with figo stage iv tubo - ovarian cancer , and primary surgery should only be undertaken in these stage iv patients in exceptional circumstances with easily resectable disease . suggest data contributors all authors contributed to study design and study implementation . 
all authors have seen and approved the final version and , after consultation with the collaborators , agreed to submit for publication . declaration of interests mn reports grants from the medical research council clinical trials unit and cancer research uk , during the conduct of the study . 
 nj reports that the royal united hospital ( his employing institution ) received support from eortc for a clinical trials nurse , who obtained and verified data from some participants in the chorus trial . 
 cm reports personal fees and travel expenses from roche farma espaa , outside the submitted work ; travel expenses from astrazeneca , outside the submitted work ; and travel expenses from pharmamar , outside the submitted work . 
tp reports personal fees and non - financial support from astrazeneca , outside the submitted work ; non - financial support from roche and igea medical , outside the submitted work ; and is co - chief investigator for the icon7 trial of bevacizumab in first - line treatment of patients with advanced ovarian cancer . 
iv , cc , gbk , mkbp , te , gcj , ams , rv , wgm , pbp , gk , ac , gs , nsr , and sk declare no competing interests . acknowledgments this study was supported by grants ( 2u10 ca11488 - 28 through 2u10 ca011488 - 36 ) from the national cancer institute ; and by a donation from the vlaamse liga tegen kanker ( flemish league against cancer ) to the eortc charitable trust . 
funding for a pilot phase of the chorus trial was provided by the royal college of obstetricians and gynaecologists and was supported by core medical research council ( mrc ) clinical trials unit funding . 
the mrc was the chorus trial sponsor , which was undertaken and analysed at the mrc clinical trials unit . correction to lancet oncol 2018 ; 19 : 94052 correction to lancet oncol 2018 ; 19 : 123946 zhu ax , finn rs , edeline j , et al . 
lancet oncol 2018 ; 19 : 94052in this article , the affiliation of dr vittorina zagonel should have been istituto oncologico veneto - istituto di ricovero e cura a carattere scientifico ( iov - irccs )  . 
 apatinib combined with oral etoposide in patients with platinum - resistant or platinum - refractory ovarian cancer ( aeroc ) : a phase 2 , single - arm , prospective study . 
lancet oncol 2018 ; 19 : 123946in this article , the statistical analysis section should have stated that at least three responses were required to continue to the second stage . 
 these corrections have been made to the online version as of aug 30 , 2018 . vol 19 september 2018 e440 corrections correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections corrections correction to lancet oncol 2014 ; 15 : 1324 correction to lancet oncol 2015 ; 16 : 324 correction to lancet oncol 2015 ; 16 : 499508 zapatero a , guerrero a , maldonado x , et al . 
high - dose radiotherapy with shortterm or long - term androgen deprivation in localised prostate cancer ( dart01 / 05 gicor ) : a controlled , randomised , phase 3 trial . 
in the fth paragraph in the results section , the number of patients in the short - term group who died of cancer , but not of the prostate , should read 14 ( 8% ) and the number in the long - term group should read three ( 2% )  . 
ramucirumab versus placebo second - line folfiri in patients with metastatic colorectal carcinoma that progressed during or after rst - line therapy with bevacizumab , uoropyrimidine ( raise ) : a randomised , double - blind , multicentre , phase 3 study . 
 lancet oncol 2014 ; 15 : 131931in gure 3 of the article , the prevalence of hpv type 18 in oral cavity in africa should read 18% , and in oropharynx in oceania hpv type 18 should appear as the second most common type after 16 , and before 35 , with a prevalence of 17% . 
 lancet oncol 2016 ; 17 : 88395in this article , the declaration of interests should read jal - m has received personal fees from reimbursement of trial - associated costs , and nonfinancial support from bristolmyers squibb . 
jb reports payments to her institution , sarah cannon research institute , from bristolmyers squibb , for the conduct of the trial ; consulting fees ( all paid to her institution and not to her personally ) from bristol myers squibb , roche , taiho oncology , amgen , genentech , merrimack , celgene , medimmune , seattle genetics , daiichi sankyo , janssen , translational drug development , five prime therapeutics , moderna therapeutics , tolero , evelo biosciences , arrys therapeutics , forma therapeutics , tanabe research laboratories , beigene , continuum clinical , and cerulean ; payments to her institution ( not to her personally ) for the conduct of clinical trials on which she served as principal investigator from abbvie , astrazeneca , emd serono , ipsen biopharma , incyte , novartis , eisai , pfizer , millennium , imclone , boston biomedical , calgb , acerta pharma , lilly , gilead sciences , leap therapeutics , macrogenics , oncomed pharmaceuticals , takeda pharmaceuticals , rgenix , novocure , merus , nv , blueprint medicine , array biopharma , armo biosciences , and agios ; jb also reports that her institution , sarah cannon research institute , conducts clinical trials and performs consulting services for several hundred companies ; the companies listed above are the ones in which jb was personally involved . 
 pao has received consulting fees from amgen and bristol - myers squibb ; and clinical trial funding from armo biosciences , bristol - myers squibb , merck , and medimmune . 
 dj has received consulting fees from definiens ag , f hoffmann - la roche ltd , curevac ag , roche pharma ag , novartis pharma ag , and novartis oncology novartis farma . 
mcp has received grant support from bristolmyers squibb to conduct this study ; personal fees from abbvie , celgene , clovis oncology , genentech , novartis ; and grants from novartis , oncomed pharmaceuticals , and stemcentrix . 
paa reports grants for research funding and personal fees for advisory / consultant role from array , bristol - myers squibb , and roche - genentech ; and personal fees for advisory / consultant role from amgen , genmab , idera , immunocore , incyte , medimmune , merck serono , msd , newlink genetics , novartis , pierre fabre , sandoz , syndax , sun pharma , sanofi , and ultimovacs . 
 lh has received research funding from astrazeneca ; served as a paid consultant for genentech and merck and an unpaid consultant for bayer , bristol - myers squibb , and xcovery ; and received lecture fees from biodesix . 
je has received grant support from astrazeneca , basilea pharmaceutica , bayer , bristol - myers squibb , celgene , clovis , daiichi sankyo , eisai , e - therapeutics , glaxosmithkline , gilead , immunocore , merck , otsuka , roche / genentech , tc biopharm , verastem , and vertex ; and served on advisory boards for and received honorarium payable to the institution from baxter , bayer , bristol - myers squibb , celgene , clovis , eisai , glaxosmithkline , immunova , karus therapeutics , otsuka , roche / genentech , tc biopharm , and transgene / jennerex . 
 ec reports research grants and / or financial support from boehringeringelheim , roche / genentech , bms , novartis , psioxus , nanobiotix janssen , abbvie , pharmamar , puma , sanofi , lilly , pfizer , merck , nektar , amcure , amgen , astrazeneca , principia , bayer , cytomx , h3 , incyte , kura , loxo , macrogenics , menarini , merck serono , merus , millenium , rigontec , tahio , and beugene tesaro ; consultancy fees from janssen - cilag , alkermes ( and travel expenses ) , seattle genetics , pierre fabre , cerulean pharma , eusa , celgene , novartis ( speakers bureau ) , nanobiotix , psioxus therapeutics , abbvie , astrazeneca , g u i d e p o i n t g l o b a l , ro c h e / genentech ( and travel expenses ) , glg , pfizer , servier , amcure , and boehringer - ingelheim ; ownership from start ( leadership ) , oncoarts associated , and international cancer from consultants ; employment start and hm hospitals group ( honoraria ) ; and president and founder of npo foundation intheos ( investigational therapeutics oncological sciences ) , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . vol 20 february 2019 corrections corrections correction to lancet oncol 2014 ; 15 : 1280 correction to lancet oncol 2014 ; 15 : 310 , 311 boughey jc . 
how do the amaros trial results change practice ? lancet oncol 2014 ; 15 : 128081the last sentence of the fourth paragraph of this comment should read with both the amaros1 and z00112 , 3 studies , the data interpreted should be with caution and should not be extrapolated to patients with three , four , or more positive sentinel lymph nodes . 
this correction has been made to the online version as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e395403 weller m , van den bent m , hopkins k , et al , for the european association for neuro - oncology ( eano ) task force on malignant glioma . 
 lancet oncol 2014 ; 15 : e395403 the appendix of this review was incorrect ; the correct appendix has been uploaded as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e591 furlow b . 
 this correction has been made to the online article as of nov 24 , 2014 . conroy t , galais m - p , raoul j - l , et al , for the fdration francophone de cancrologie digestive and unicancer - gi group . 
de nitive chemo radiotherapy with folfox versus uorouracil and cisplatin in patients with oesophageal cancer ( prodige5 / accord17 ) : final results of a randomised , phase 2 / 3 trial . 
the last sentence of the eighth paragraph in the results section should read an endoscopic complete response at week 15 was achieved in 61 ( 53% ) of 115 patients in the folfox group versus 57 ( 48% ) of 120 patients in the uorouracil plus cisplatin group . 
folfox = uorouracil , leucovorin , and oxaliplat recist = response evaluation criteria in solid tumours.21 * 115 patients assessable in the folfox group and 120 assessable in the uorouracil and cisplatin group . table 2 : tumour response to treatment correction to lancet oncol 2014 ; 15 : 1464 sestak i , singh s , cuzick j , et al . 
changes in bone mineral density at 3 years in postmenopausal women receiving anastrozole and risedronate in the ibis - ii bone substudy : an international , doubleblind , randomised , placebo - controlled trial . 
this correction has been made to the online version as of nov 24 , 2014 , and the printed version is correct . c lumbar spine d total hip 05 10 15 20 25 30 35 40 45 50 12% 40% 18% 40% anastrozole placebo baseline 12 months anastrozole placebo 36 months baseline 12 months 36 months vol 15 december 2014 e587 corrections correction to lancet oncol 2015 ; 16 : 1045 correction to lancet oncol 2015 ; 16 : 1499 tournigand c , chibaudel b , samson b , et al . 
 this correction has been made to the online version as of nov 29 , 2015 . correction to lancet oncol 2015 ; 16 : 1355 , 1363 hegewisch - becker s , graeven u , lerchenmller ca , et al . 
maintenance strategies after first - line oxaliplatin plus uoropyrimidine plus bevacizumab for patients with metastatic colorectal cancer ( aio 0207 ) : a randomised , noninferiority , open - label phase 3 trial . 
 lancet oncol 2015 ; 16 : 135569the fourth line of the findings section of the summary of this article should read bevacizumab alone was noninferior to standard uoropyrimidine plus bevacizumab ( hazard ratio [ hr ] 108 [ 95% ci 085137 ] ; p = 053 ; upper limit of the one - sided 988% ci 142 ) , whereas no treatment was not ( hr 126 [ 099160 ] ; p = 0056 ; upper limit of the one - sided 988% ci 165 )  . 
 lancet oncol 2015 ; 16 : 14931505in this article , the colours of the curves in both panels of gure 3 were inverted ; the correct version is shown below . 
 these corrections have been made to the online version as of nov 29 , 2015 . events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 49 ( 41 - 57 ) 54 ( 43 - 62 ) stratied hazard ratio 081 ( 066101 ) p = 0059 ( log - rank ) unstratied hazard ratio 078 ( 068096 ) p = 0019 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0023 events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 221 ( 196267 ) 249 ( 214289 ) stratied hazard ratio 079 ( 063099 ) p = 0036 ( log - rank ) unstratied hazard ratio 079 ( 064098 ) p = 0035 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0024 number at risk bevacizumab bevacizumab plus erlotinib time ( months ) number at risk bevacizumab bevacizumab plus erlotinib vol 16 december 2015 e589 correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections correction to lancet oncol 2017 ; 18 : e35463 correction to lancet oncol 2018 ; 19 : 87100 correction to lancet oncol 2018 ; 19 : 25766 oconnor oa , lue jk , sawas a , et al . 
 for lancet oncol 2017 ; 18 : e35463 in this review , the second sentence of the abstract should read additional improvements have been reported in three phase 3 colon cancer trials when oxaliplatin was added to fluoropyrimidines , the effect was mainly on disease - free survival . 
this correction has been made to the online version as of feb 28 , 2018 although women fulvestrant johnston s , lee ks , et di leo a , al . 
buparlisib plus with postmenopausal her2hormone - receptor - positive , negative , advanced breast cancer progressing on or after mtor inhibition ( belle - 3 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
in the results section , the following sentence should have read in the 11 ( 13% ) cases of discordance , a pik3ca wild - type tumour sample and pik3ca - mutated ctdna were reported in three ( 4% ) patients and pik3ca mutations detected in the tumour sample but not in ctdna ( 9% ) patients . 
these corrections have been made to the online version as of feb 28 , 2018 . seven vol 19 march 2018 e137 corrections corrections correction to lancet oncol 2015 ; 16 : 133 correction to lancet oncol 2015 ; 16 : 181 , 184 correction to lancet oncol 2015 ; 16 : 237 published online january 29 , 2015 s1470 - 2045 ( 14 ) 70483 - 8 dp . 
 radiotherapy lancet oncol 2015 ; 16 : 23739in this comment , the fth line of the third paragraph should read : by contrast , acute gastrointestinal toxicity was increased with hypofractionation [ 95% ci 372469 ] of ( 420% patients the hypofractionation group had grade 2 adverse events vs 312% [ 266358 ] in the standard fractionation di erence 108% , 90% ci 5251643 ; p = 00015 ) although were similar 3 months after treatment , and non - inferiority was not con rmed . 
these corrections have been made to the online version as of march 2 , 2015 , and have been made to the printed comment . group , cavalli f , atun r . 
lancet oncol 2015 ; 16 : 13334 in this comment , the second sentence should have been : deaths from cancer are projected to increase from the present level of around 8 million a year to more than 13 million by 2030 , with most of the burden being in poorer countries . 
this correction has been made as of jan 29 , 2015 . correction to lancet oncol 2015 ; 16 : 266 ih , williams lj , kunkler jack wjl , cameron da , dixon jm , on behalf of investigators . 
 lancet oncol 2015 ; 16 : 26673in the interpretation section of the summary , the rst sentence should read postoperative whole - breast radiotherapy after breast - conserving surgery and adjuvant endocrine treatment resulted in a signi cant but modest reduction in local recurrence for women aged 65 years or older with early breast cancer 5 years after randomisation . 
this correction has been made to the online version as o f march 2 , 2015 , and to the printed article . thomas a , rajan a , berman a , in patients with et al . 
lancet oncol 2015 ; 16 : 17786 in the key of gure 2a of this article , the text for the red line should read thymic carcinoma ( 16 / 24 failed ) and that for the blue line should read in the thymoma ( 11 / 16 failed )  . 
 key of gure 4b , the text for the red line should read no change / increase ( 0 / 18 failed ) and that for the blue line should read decrease ( 4 / 4 failed )  . 
lancet oncol 2015 ; 16 : 27483in this article , the interpretation should have read : hypofractionated radiotherapy was not non - inferior to standard fractionated radiotherapy in terms of acute genitourinary and gastrofor men with intestinal intermediate - risk high - risk and prostate cancer . 
this correction has been made to the online version as of march 2 , 2015 and to the printed article . toxicity vol 16 march 2015 e105 correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections corrections correction to lancet oncol 2015 ; 16 : 1013 correction to lancet oncol 2015 ; 16 : 1143 correction to lancet oncol 2015 ; 16 : 1289 declaration kopans db . 
 lancet oncol 2015 ; 16 : 1143the last line of the rst paragraph of this comment should read only this year , for example , did who add several commonly used , extremely e ective drugs , such as imatinib , trastuzumab , and cisplatin to its list of essential medicines . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the paragraph on survival with oligometastatic hcc should read the researchers found that patients with oligometastatic disease had a significantly longer overall survival than patients with extensive disease ( 104 months versus 63 months , p = 0034 )  . 
 vol 16 november 2015 e528 correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
we aimed to assess and define these genes to provide evidence for future screening guidelines . methods in this international , multicentre study , we analysed patients with medulloblastoma from retrospective cohorts ( international cancer genome consortium [ icgc ] pedbrain , medulloblastoma advanced genomics international consortium [ magic ] , and the cefalo series ) and from prospective cohorts from four clinical studies ( sjmb03 , sjmb12 , sjyc07 , and i - hit - med )  . 
dna methylation profiling was done to determine consensus molecular subgroups : wnt ( mbwnt ) , shh ( mbshh ) , group 3 ( mbgroup3 ) , and group 4 ( mbgroup4 )  . 
previously defined somatic mutational signatures were used to further classify medulloblastoma genomes into two groups , a clock - like group ( signatures 1 and 5 ) and a homologous recombination repair deficiency - like group ( signatures 3 and 8 ) , and chromothripsis was investigated using previously established criteria . 
progression - free survival and overall survival were modelled for patients with a genetic predisposition to medulloblastoma . findings we included a total of 1022 patients with medulloblastoma from the retrospective cohorts ( n = 673 ) and the four prospective studies ( n = 349 ) , from whom blood samples ( n = 1022 ) and tumour samples ( n = 800 ) were analysed for germline mutations in 110 cancer predisposition genes . 
in our rare variant burden analysis , we compared these against 53 105 sequenced controls from exac and identified apc , brca2 , palb2 , ptch1 , sufu , and tp53 as consensus medulloblastoma predisposition genes according to our rare variant burden analysis and estimated that germline mutations accounted for 6% of medulloblastoma diagnoses in the retrospective cohort . 
the prevalence of genetic predispositions differed between molecular subgroups in the retrospective cohort and was highest for patients in the mbshh subgroup ( 20% in the retrospective cohort )  . 
these estimates were replicated in the prospective clinical cohort ( germline mutations accounted for 5% of medulloblastoma diagnoses , with the highest prevalence [ 14% ] in the mbshh subgroup )  . 
patients with germline apc mutations developed mbwnt and accounted for most ( five [ 71% ] of seven ) cases of mbwnt that had no somatic ctnnb1 exon 3 mutations . 
germline tp53 mutations presented only in childhood patients in the mbshh subgroup and explained more than half ( eight [ 57% ] of 14 ) of all chromothripsis events in this subgroup . 
 germline mutations in palb2 and brca2 were observed across the mbshh , mbgroup3 , and mbgroup4 molecular subgroups and were associated with mutational signatures typical of homologous recombination repair deficiency . 
 funding german cancer aid ; german federal ministry of education and research ; german childhood cancer foundation ( deutsche kinderkrebsstiftung ) ; european research council ; national institutes of health ; canadian institutes for health research ; german cancer research center ; st jude comprehensive cancer center ; american lebanese syrian associated charities ; swiss national science foundation ; european molecular biology organization ; cancer research uk ; hertie foundation ; alexander and margaret stewart trust ; v foundation for cancer research ; sontag foundation ; musicians against childhood cancer ; bc cancer foundation ; swedish council for health , working life and welfare ; swedish research council ; swedish cancer society ; the swedish radiation protection authority ; danish strategic research council ; swiss federal office of public health ; swiss research foundation on mobile communication ; masaryk university ; ministry of health of the czech republic ; research council of norway ; genome canada ; genome bc ; terry fox research institute ; ontario institute for cancer research ; pediatric oncology group of ontario ; the family of kathleen lorette and the clark h smith brain tumour centre ; montreal childrens hospital foundation ; the hospital for sick children : sonia and arthur labatt brain tumour research centre , chief of research fund , cancer genetics program , garron family cancer centre , mdts garron family endowment ; bc childhood cancer parents association ; cure search foundation ; pediatric brain tumor foundation ; brainchild ; and the government of ontario . copyright 2018 the author ( s )  . 
following the recognition9 of four consensus molecular subgroups ( wnt [ mbwnt ] , shh [ mbshh ] , group 3 [ mbgroup3 ] , and group 4 [ mbgroup4 ] ) with distinct demographics and clinical outcomes , 10 patients with germline tp53 , sufu , and ptch1 mutations have been reported to be predisposed to develop mbshh.11 , 12 although several case studies have reported in patients with fanconi medullo blastomas arising specific anaemia , whether medulloblastoma subgroups , and whether heterozygous germline mutations13 also confer an increased risk of developing medulloblastoma , remain unknown . 
a comprehensive study14 of damaging germline mutations in cancer predisposition genes across a diverse set of paediatric cancers identified variants likely to predispose to the disease in three ( 8% ) of 37 patients with medulloblastomaa cohort size that is too small to allow these predispose these issues to be thoroughly addressed . 
owing to these uncertainties , and since knowledge about germline mutations can be useful for clinical practice , 8 assessment of larger patient series is crucial for the identification of consensus medullo blastoma predisposition genes to estimate the con tribution of genetic predisposition towards consensus molecular sub groups , and investigate whether affected patients have distinct clinical outcomes . 
a comprehensive under standing of molecular alterations in affected patients would further help in the development of clinical screening guidelines for genetic risk assessment in paediatric patients . in this study , we provide a comprehensive description of genetic risk factors across 1022 patients with medulloblastoma based on a retrospective discovery cohort and validation in a prospective clinical cohort . 
additionally , which patients would benefit from genetic counselling in the context of molecular subgroupingnowadays routinely applied in clinical trials and implemented into the revised who classification of cns tumours in 2016and whether genetic predisposition can be recognised based on familial patterns were unclear . 
additionally , several paediatric cancer centres have implemented routine multigene panel analysis and whole - exome analysis of medulloblastomas ; however , these centres encounter several germline mutations with uncertain clinical significance . 
no study has previously aimed to define a consensus set of medulloblastoma predisposition genes or has investigated under which circumstances genetic counselling and testing should be offered to patients with medulloblastoma . added value of this study this study is based on an international cohort of 1022 patients with medulloblastoma , and includes detailed information about medulloblastoma subgroups ( wnt [ mbwnt ] , shh [ mbshh ] , group 3 [ mbgroup3 ] , and group 4 [ mbgroup4 ] ) , somatic mutation landscapes , and clinical outcomes . 
we defined and characterised six consensus , clinically relevant medulloblastoma predisposition genes on the basis of rare variant burden analysis ( apc , brca2 , palb2 , ptch1 , sufu , and tp53 )  . 
half of all patients with damaging germline mutations were not recognised based on familial history of cancer ; however , these patients exhibited distinct phenotypes with respect to age at diagnosis , molecular subgroups , somatic mutation patterns , and clinical outcomes . 
about one in five patients in the mbshh subgroup developed medulloblastoma in the context of a genetic predisposition , underscoring the need for a dedicated genetic screening programme and surveillance programme in this patient group . 
damaging germline mutations in known cancer predisposition genes were rare in paediatric patients in the mbgroup3 and mbgroup4 subgroups , which indicates conservative ordering of genetic tests in these groups . 
we propose clinical guidelines for genetic screening in medulloblastoma based on routinely acquired clinical and molecular tumour phenotypes . implications of all the available evidence a significant prevalence of clinically important germline mutations in two of four molecular subgroups reveals that genetic counselling and testing should be established as a standard - of - care procedure in the management of patients with medulloblastoma . 
we obtained biological samples from all patients , who all provided written informed consent , in accordance with institutional review board guidelines . patient accrual for our retrospective cohort was done from 2003 until 2016 . 
patient accrual for the sjmb03 trial was done from sept 9 , 2003 , until march 7 , 2013 and for the sjyc07 trial was done from dec 17 , 2007 , until march 31 , 2017 . 
the age limit for eligibility in the prospective studies was 5 years or younger ( sjyc07 ) , 321 years ( sjmb03 ) , and 339 years ( sjmb12 )  . 
 patients in the i - hit - med study were excluded if they were registered in another clinical trial for the same diagnosis ( relapse is defined as a second diagnosis ) or if a valid ethical committee approval was lacking . procedures whole - genome and whole - exome sequencing data for germline and tumour samples were generated at the german cancer research centre ( icgc pedbrain ; heidelberg , germany ) , canadas michael smith genome sciences centre ( magic ; vancouver , bc , canada ) , broad institute of massachusetts institute of technology and harvard ( cambridge , ma , usa ) , and st jude childrens research hospital ( pediatric cancer genome project ; memphis , tn , usa )  . to ensure standardisation of genomic data processing , we used the same uniform computational analysis workflows for all germline and tumour samples . 
we used delly for germline genomic structural variant discovery with default settings for whole - genome sequencing samples and a custom read - depth - based copy - number variation ( cnv ) - calling pipeline for whole - exome sequencing samples . 
we based this custom pipeline on read quantification by bedtools in exome capture regions ( maq > 30 ) , followed by variance stabilising transformation of count data with the vst function from the deseq2 r package ( version 1.8.2 ) , unsupervised estimation of hidden confounders using the r package peer ( 30 hidden confounders ) , and copynumber segmentation based on standardised residuals using circular binary segmentation ( r package dnacopy , version 1.50 , default settings )  . 
raw cnv calls were filtered further for size ( to include only those > 10 kb ) , minimum number of exons ( > 2 ) , and cnv signal intensity ( > 4 sds )  . 
 any snv , short indel , and mnv that was observed at low variant allele frequency in blood ( 315% ) and high variant allele frequency in tumours ( > 50% ) was considered a putative mosaic mutation . 
we restricted the analysis to reads with mapping quality of more than 30 ( 10 log10 pr [ mapping position is wrong ] ) , base quality of more than 20 ( 10 log10 pr [ mapping position is wrong ] ) , and sites with more than 30 times sequencing coverage ( ie , number of reads )  . 
we excluded any variant that was present in public genetic archives and discovered in germline genomes of other patients with medulloblastoma . for classification of damaging germline mutations , germline variants were annotated with the ensembl variant effect predictor ( vep ; r81 )  . 
high - impact ( ie , damaging ) germline mutations were defined as frameshift , stop gain , start lost , canonical splice site , exon or gene deletions , known ( clinvar ; accessed feb 16 , 2017 ) damaging non - canonical splice site variants , and somatic mosaic mutations ( defined as mutations present in a subset of normal cells )  . 
putative damaging germline mutations were removed if the estimated minor allele frequency in at least one continental population was more than 01% , which we judged on the basis of 53 105 sequenced individuals that were assigned to known ( control ) populations and without a cancer diagnosis from the exome aggregation consortium ( exac ) resource , the 1000 genomes project , and the national heart , lung , and blood institute go exome sequencing project . 
putative gain - of - function missense variants in tp53 were further evaluated by use of information in the international agency for research on cancer tp53 database and annotated as pathogenic if tp53 mutations were classified as non - functional in experimental transcriptional activity assays . 
we estimated the primary population ancestry ( european , african , east asian , south asian , and native american ) for all patients with medulloblastoma with a supervised decomposition approach20 and ancestry - informative markers that are within exac - defined exome capture target regions . identification of somatic mutations ( snvs , small indels , and copy - number alterations ) was pursued in a standardised manner across all samples ( matched tumour or normal genome as well as exome pairs ) with the german cancer research center ( known as dkfz ) and european molecular biology laboratory cancer genome analysis workflow of the pcawg consortiu somatic snvs and indels were further stringently filtered for germline contamination using information from dbsnp and the 1000 genomes project . 
we used a highstringency structural variant set by additionally filtering somatic structural variants detected in at least 1% of a set of 1105 germline samples from healthy individuals belonging to phase 1 of the 1000 genomes project , and by requiring absence of somatic structural variants in all medulloblastoma germline samples of this study . 
for inference of high - stringency structural variants , we additionally required at least four supporting read pairs21 with a minimum mapping quality of 20 ( 10 log10 pr [ mapping position is wrong ] ) and restricted valid somatic structural variant sizes from 100 bp to 500 mb . we quantified previously defined somatic mutational signatures22 ( termed 1 , 3 , 5 , and 8 ) using tumour - specific somatic point - mutation spectra and published signature probabilities . 
 signatures 1 and 5 ( clock - like signatures ) are associated with ageing ( a clock - like accumulation of mutations ) and occur in normal , non - malignant cells , 22 whereas signatures 3 and 8 are associated with homologous recombination repair deficiency ( hrd ) and have been reported in cancer tissues . 
we used these mutational vol 19 june 2018 articles signatures to further classify medulloblastoma genomes into two groups , a clock - like group ( signatures 1 and 5 ) and a hrd - like group ( signatures 3 and 8 )  . 
somatic mutation spectra were quantified with the r package somaticsignatures ( version 2.6 ) and decomposed into contributions of known mutational signatures based on the lawsonhanson algorithm for non - negative least squares ( nnls version 1.1 , r package )  . 
the quantification error ( residual sum of squares ) was correlated with the total somatic mutation burden ( spearmans r = 074 ; p < 00001 ) and it was highest in tumours with fewer than 100 somatic snvs . 
 medulloblastomas were classified as homo logous recombination repair deficient if most ( > 50% ) somatic snvs were assigned to mutational signatures 3 or 8 . to assess the burden of rare germline snvs and indels in cancer predisposition genes , we performed case control association testing in a subgroup - specific manner as well as across all subgroups based on a collection 110 autosomal cancer predisposition genes8 , 23 ( appendix p 2 )  . 
to ensure comparability with variants found in patients with medulloblastoma , exac germline mutations were normalised with vt normalize , annotated with vep ( r81 ) , and filtered for sites that passed quality controls , as defined by exac . 
moreover , we excluded any germline mutations that were present outside exacdefined target regions to reduce any possible advantages derived from improved variant calling in whole - genome sequences ( eg , exons not being covered in exac )  . 
we assumed equal effect sizes for frameshift , nonsense , splice site , and gain - of - function missense variants , as well as for variants located at any position along a gene . 
allelic relative risks were estimated by the odds ratio ( or ) , which describes the association between medullo blastoma and damaging alleles by comparing the odds of medullo blastoma in an individual carrying a wild - type allele to the odds of medulloblastoma in an individual carrying one damaging allele . 
we assumed that the penetrance of monoallelic germline mutations was lower than that of biallelic germline mutations ( ie , homozygous and compound heterozygous mutations )  . we assessed secondary somatic gene hits in tumours on three levels : point mutations , loss - of - heterozygosity , and allele - specific gene expression . 
loss of heterozygosity was quantified by use of genotyping germline alleles in available tumour genomes or exomes with freebayes and requiring a minimum coverage of ten reads , minimum base quality of 10 ( 10 log10 pr [ base is wrong ] ) , and minimum mapping quality of 10 ( 10 log10 pr [ mapping position is wrong ] )  . 
 allele - specific gene expression was quantified at heterozygous snvs and indels and mrna sequencing data by use of freebayes ( minimum mapping quality of [ 10 log10 pr ( mapping position is wrong ) ] and minimum base quality of 10 [ 10 log10 pr ( base is wrong ) ] ) and was predicted on the basis of binomial tests , an expected ratio of 05 , and p values lower than 005 . 
 when possible , multiple sites within the same gene were phased with paired - end rna sequencing data and individual sites were merged to calculate haplotypespecific expression ratios . investigated chromothripsis using previously established criteria.24 these criteria distinguish chromothripsis from dna rearrangements occurring in a stepwise fashion . 
first , we analysed breakpoint clustering in the entire genome based on highconfidence somatic structural variant calls and did statistical analysis for non - randomness of breakpoint distributions , under the assumption of an exponential distribution ( null hypothesis )  . 
overall survival and progression - free survival were based on definitions consistent with how they were evaluated within each respective patient cohort from each prospective trial : sjmb03 , sjmb12 , and sjyc07 . 
one - sided binomial tests were used for replication analysis with the alternative hypothesis defined as a lower probability of observing germline mutations in the replication cohort . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding authors had full access to all the data and had the final responsibility to submit for publication . tumour genomes were results we analysed germline genome - sequencing and exomesequencing data ( appendix pp 89 ) from 1022 patients with medulloblastoma , of whom 673 were in the retrospective discovery cohort and 349 were in the prospective clinical study cohort ( figure 1a , appendix p 3 )  . 
patientfor matched 800 samples from both cohorts ( n = 451 retrospective and n = 349 prospective ) from whole - genome sequencing ( n = 397 ) and whole - exome sequencing ( n = 403 ; figure 1a )  . 
snvs , mnvs , small ( < 30 bp ) indels , and large structural variants were predicted across 110 paediatric - onset and adult - onset cancer predisposition genes8 , 23 and classified as pathogenic based on stringent criteria . 
most damaging germline mutations have been previously described in the literature ( in 55 [ 71% ] of 77 mutations ) and already classified as ( likely ) pathogenic ( 42 [ 55% ] of 77 ) in public archives ( clinvar , lovd ; appendix pp 1012 )  . 
in total , six genes showed a significant excess of damaging germline mutations for patients with medulloblastoma namely , apc , brca2 , palb2 , ptch1 , sufu , and tp53 ( adjusted p value for multiple testing < 005 ; figure 1b , appendix p 4 )  . 
 however , a single patient in our discovery cohort harboured a heterozygous germline mutation in msh6 ( appendix pp 1012 )  . the overall prevalence of genetic predisposition based on these six genes in the retrospective discovery cohort was 6% ( 40 / 673 ) , with a highest prevalence of 20% ( 28 / 141 ) in patients in the mbshh subgroup ( figure 1c )  . 
key patient characteristics , such as sex , age at diagnosis , and molecular tumour subgroups , were similar between both cohorts ( psex = 068 , page = 017 , psubgroup = 012 ; figure 1a )  . 
the overall prevalence of genetic predisposition in our prospective cohort ( 17 [ 5% ] of 349 ) was consistent with estimates ( p = 024 ; from our retrospective cohort figure 1d , appendix pp 1012 )  . 
notably , patients in the mbwnt subgroup also had an increased prevalence of germline predisposition in both the discovery and replication cohort , albeit more modest than for patients in the mbshh subgroup ( figure 1c , d )  . genes we closely analysed key demographic , clinical , and molecular characteristics of patients with a genetic predisposition in these six genes . 
most patients with available subgroup information developed mbshh ( 41 [ 76% ] of 54 ; figure 2a ) and age at diagnosis also differed significantly between patients with germline mutations in medulloblastoma predisposition ( p < 00001 ; figure 2b )  . 
patients with germline sufu or ptch1 mutations were typically diagnosed as infants at a median age of 20 years ( iqr 1323 ) , whereas patients with apc or tp53 mutations were diagnosed as children at a median age of 98 years ( iqr 8011 )  . 
clinical signs of a genetic predisposition were noted in 16 ( 41% ) of 39 patients and familial history of cancer in 17 ( 46% ) of 37 patients , and both were different between patients with germline mutations in medulloblastoma pre disposition genes ( p = 0017 and p = 0046 , respectively ; figure 2c , 2d )  . 
for example , only one ( 9% ) of all 11 ptch1 and sufu mutation carriers with available medical records had a family history of cancer ; however , eight ( 67% ) of records had 12 patients with available medical clinical symptoms consistent with gorlins syndrome 790 vol 19 june 2018 articles a male ( 63% ) male ( 64% ) medulloblastoma cohort retrospective : n = 673 prospective : n = 349 whole - genome and whole - exome squencing germline : n = 1022 tumour : n = 800 molecular subgroup 844 tumours 110 cancer predisposition genes age at diagnosis molecular subgroup female ( 37% ) female ( 36% ) child ( 70% ) child ( 79% ) infant ( 17% ) adult ( 13% ) infant ( 16% ) adult ( 5% ) group 4 ( 38% ) group 4 ( 40% ) ( 28% ) ( 27% ) group 3 ( 27% ) wnt ( 6% ) group 3 ( 22% ) wnt ( 10% ) sufu ptch1 tp53 palb2 brca2 retrospective cohort prospective cohort 1000 all subgroups of medulloblastoma group 3 group 4 rr ( 95% ci ) n = 349 p = 024 n = 673 group 3 group 4 group 3 group 4 n = 32 20% n = 141 n = 134 n = 189 n = 36 p = 081 14% n = 95 p = 0080 n = 78 p = 048 n = 139 p = 0051 figure 1 : discovery and replication of medulloblastoma predisposition genes ( a ) study design and patient characteristics . 
patients with damaging germline mutations in apc , ptch1 , sufu , tp53 , palb2 , and brca2 . ( eg , macrocephaly , jaw cysts , and frontal bossing ; appendix pp 1012 )  . 
by contrast , all four apc mutation carriers with available medical records had a familial history of familial adenomatous polyposis and associated cancers ( eg , adrenocortical carcinoma )  . 
of note , additional malignancies were observed in six ( 12% ) of 50 patients with medulloblastoma and all were restricted to patients with germline apc ( n = 3 ) or tp53 ( n = 3 ) mutations ( appendix pp 1012 )  . at a median follow - up of 48 months ( iqr 2878 ) , 5 - year progression - free survival for 49 patients with a genetic predisposition who were evaluable for this outcome was 52% ( 95% ci 4069 )  . 
progression - free survival ( logrank p = 00056 ) and overall survival ( log - rank p = 000032 ) differed significantly across patients with germline mutations in different medullo blastoma predisposition genes ( figure 3 )  . germline apc mutations were found in seven ( 1% ) of all 1022 patients with medulloblastoma and included one infant , five children , and one adult patient . 
two of these seven patients harboured partial or full gene deletions ( appendix p 5 ) and the remaining five patients had frameshift and nonsense mutations between codons 554 and 1113 , a region associated with classical familial adenomatous polyposis phenotypes . 
all five wnt - driven medulloblastomas lost the wild - type apc allele and the shhdriven medulloblastoma showed retention of the wild - type allele ( figure 4a )  . 
furthermore , germline apc mutations in mbwnt patients were mutually exclusive with somatic ctnnb1 exon 3 mutations ( p < 00001 ) , the primary26 somatic driver event in mbwnt ( figure 4b )  . 
 overall , germline apc mutations were identified in five ( 71% ) of seven ctnnb1 - wild - type mbwnt cases and , together with somatic ctnnb1 mutations , explained 97% ( 64 / 66 ) of all wnt - driven medulloblastomas . 
by contrast , monosomy 6a frequent somatic chromosome aberration in mbwnt ( in 55 [ 83% ] of 66 cases ) was not mutually exclusive with germline apc mutation status ( p = 019 ) ; although we observed two patients with vol 19 june 2018 articles a group 4 group 3 n = 54 ; p < 00001 patients ( % ) 100% n = 57 ; p < 00001 age at diagnosis ( years ) ( 12 ) ( 23 ) ( 35 ) ( 530 ) ( 410 ) ( 911 ) ( 711 ) brca2 * ptch1 sufu tp53 palb2 brca2 sufu ptch1 brca2 * palb2 brca2 tp53 n = 37 ; p = 0046 n = 39 ; p = 0017 adult ( 18 ) child ( 4 - 17 ) infant ( 3 ) ptch1 sufu tp53 palb2 brca2 brca2 * palb2 tp53 brca2 sufu ptch1 brca2 * figure 2 : clinical characteristics of patients with a genetic predisposition ( a ) molecular tumour subgroups . 
overall and progression - free survival for patients with apc - mbwnt was 100% ( 95% ci 100100 )  . germline tp53 mutations were found in 14 ( 1% ) of all 1022 patients with medulloblastoma and were only present in patients with mbshh ( 13 / 13 ; data missing for one patient )  . 
notably , germline tp53 mutations were identified in 13 ( 8% ) of 170 paediatric mbshh patients and 13 ( 20% ) of 63 children aged between 5 years and 16 years with mbshh . 
most germline tp53 mutations ( 13 / 14 ) clustered within the dna - binding domain ( appendix p 6 ) and somatic inactivation of the wild - type tp53 allele was detected in all 13 available medullo blastoma genomes via loss of heterozygosity ( figure 4a )  . 
all eight whole - genome - sequenced tp53deficient mbshh exhibited complex somatic genomic rearrangements consistent with chromothripsis21 and accounted for eight ( 57% ) of all 14 chromothripsis events in the mbshh subgroup . 
5 - year overall survival for patients with germline tp53 mutations was 27% ( 95% ci 1072 ; figure 3 )  . germline sufu and ptch1 mutations were detected in 20 ( 2% ) of all 1022 patients with medulloblastoma , exclusively the mbshh subgroup ( 19 / 19 ; data missing for one patient ) , and accounted for 11% ( 18 / 170 ) of all paediatric patients with mbshh and 21% ( 17 / 80 ) of all infant patients with mbshh . 
we observed somatic loss of the sufu or ptch1 wild - type allele in all ( n = 18 ) sequenced mbshh that were diagnosed in patients with germline sufu or ptch1 mutations . 
only six of 20 germline sufu and ptch1 mutations have been previously described in the literature ( appendix pp 1012 ) , suggesting either appreciable amounts of de - novo mutagenesis or poor reporting to public archives . 
in support of the de - novo mutagenesis theory , a de - novo germline ptch1 mutation was observed in a patient with mbshh from our retrospective cohort , for whom whole - exome sequences were also available for both parents . 
clinical information was frequency ranged 792 vol 19 june 2018 articles a available for one patient with a mosaic ptch1 mutation , which showed that the patient was clinically diagnosed with gorlins syndrome and the patient had no family history of cancer and no family history of gorlins syndrome . 
moreover , comparison of clinical outcomes between patients with germline mutations in sufu and ptch1 showed no differences in progression - free survival ( p = 050 , 16 patients with germline mutations ) and overall survival ( p = 091 , 17 patients with germline mutations )  . 
notably , patients with germline mutations in either sufu or ptch1 had a better overall survival than progression - free survival ( combined 5 - year progressionfree survival 56% for sufu and ptch1 mutations , 95% ci 3787 ; combined 5 - year overall survival 85% , 95% ci 67100 ; figure 3 )  . germline brca2 mutations were present in 11 ( 1% ) of all 1022 patients with medulloblastoma and included ten paediatric patients and one adult ( survival data not available for all patients with these mutations )  . 
clinical signs of a genetic predisposition or family history of cancer were noted in all four compound heterozygous patients and in four ( 80% ) of five heterozygous patients with available medical records . 
patients with compound heterozygous mutations at brca2 developed exclusively mbshh ( p = 00060 when compared with any other subgroup ; figure 2a ) and exhibited worse progression - free survival ( p = 0025 ) and overall survival ( p = 0022 ) relative to patients with heterozygous germline brca2 mutations ( figure 3 )  . 
when compared with 53 105 controls , the burden of rare germline mutations in brca2 was associated with increased risk of mbshh ( relative risk [ rr ] 138 [ 54294 ] ; p < 00001 ) and mbgroup3 / 4 ( rr 42 [ 14101 ] ; p = 00077 )  . 
 additional details about family history of cancer , parental genetic testing , and somatic mutation profiles heterozygous and compound heterozygous brca2 mutation carriers are provided in the appendix ( p 1 )  . germline palb2 mutations were found in five ( < 1% ) of all 1022 patients with medulloblastoma . 
all five damaging germline mutations were heterozygous in patients affected with medullo blastoma and were previously reported in familial pancreatic and breast cancer studies.27 all five germline mutations were classified as pathogenic according to clinvar ( appendix pp 1012 )  . 
log - rank p values indicate differences across all patient groups . adult - onset cancers ( eg , breast cancer ) , predisposition to paediatric malignancies has so far only been described in the context of fanconi anaemia.28 we excluded the predisposition to fanconi anaemia in all five cases because of an absence of additional rare germline mutations ( including protein - truncating variants , missense mutations , and inframe indels )  . 
analysis of vol 19 june 2018 articles b germline apc mutation somatic ctnnb1 mutation somatic monosomy 6 somatic ctnnb1 mutation germline apc mutation * mbwnt mutant cases wild - type cases 76% 894% 833% n = 66 ; p = 092 age at diagnosis ( years ) tp53 sufu ptch1 palb2 brca2 n = 49 signature 1 associated with ageing seen in healthy cells and tumour cells signature 3 associated with hrd seen in breast cancer signature 5 associated with ageing seen in healthy cells and tumour cells signature 8 associated with hrd seen in medulloblastoma and breast cancer patients ( % ) 100% n = 375 brca2 palb2 wild - type brca2 palb2 wild - type brca2 palb2 wild - type brca2 palb2 wild - type figure 4 : molecular medulloblastoma characteristics for patients with a genetic predisposition ( a ) patterns of somatic inactivation of wild - type alleles for all patients with a germline mutation in one of the consensus medulloblastoma predisposition genes . 
 ( b ) somatic driver events in patients with medulloblastoma in the wnt subgroup ( top panel ) and age at diagnosis for all patients with germline apc mutations and patients in the wnt subgroup with somatic ctnnb1 mutations ( bottom panel )  . 
 ( c ) association between germline palb2 ( n = 5 ) and brca2 ( n = 7 ) mutation status and somatic mutational signatures 1 , 3 , 5 , and 8 . 
additional details about family history of cancer , parental genetic testing , and somatic mutation profiles available for one affected patient are presented in the appendix ( p 1 )  . since the clinical relevance of heterozygous germline mutations in palb2 and brca2 is uncertain , we aimed to corroborate our findings through investigation of somatic mutation patterns ( mutational signatures ) in medulloblastoma genomes . 
quantification of four previously implicated mutational signatures ( signatures 1 , 3 , 5 , and 8 ) across 375 medulloblastoma genomes showed a significant association between both hrd signatures ( signatures 3 and 8 ) and germline brca2 and palb2 mutation status ( figure 4c , appendix p 7 )  . 
moreover , although the overall prevalence of an hrd - like mutation spectrum was modest in medulloblastoma ( 58 [ 15% ] of 375 ) , it was enriched in tumours as brca2 - deficient and palb2 - deficient compared with tumours with other genetic mutations ( or 190 [ 95% ci 45113 ] , p < 00001 )  . 
in total , nine ( 75% ) of 12 brca2 - deficient and palb2 - deficient tumours showed evidence for an hrd - like mutation spectru strikingly , eight ( 89% ) of nine patients with mbshh and an hrd - like mutation spectrum harboured germline mutations in consensus medulloblastoma predisposition genes ( brca2 n = 4 , palb2 n = 2 , and tp53 n = 2 ) , suggesting that hrd might serve as a biomarker for genetic predisposition in this patient group . 
we also observed five patients in the mbwnt subgroup with an hrd - like mutation spectrum and noticed that four ( 89% ) of five cases were diagnosed as adults ( p = 00003 for paediatric vs adult cases )  . 
 the only paediatric patient in the mbwnt subgroup with an hrd - like mutation spectrum harboured a pathogenic heterozygous germline mutation in atm along with somatic inactivation of the wild - type atm allele ( appendix pp 1012 )  . 
finally , we also identified heterozygous germline mutations in fanca ( n = 1 ) and fancq ( n = 1 ) in patients with mbgroup3 and mbgroup4 , respectively , and an hrd - like mutation spectru taken together , these results corroborate our genetic findings and indicate that genetic 794 vol 19 june 2018 articles alteration of homologous recom bination genes is associated with an hrd - like mutation spectrum in medul loblastoma . 
our rare variant burden analyses revealed that genetic predisposition has a major role in the cause of medulloblastoma after accounting for molecular subgroups , with a high prevalence in mbwnt and mbshh patient subgroups . 
recommendations for surveillance and clinical management of individual childhood cancer predisposition syndromes have been summarised in a series of articles29 from the american association for cancer research childhood cancer predisposition workshop . 
 our study complements these recommendations by providing additional diagnostic criteria based on clinical and molecular characteristics . the urgent need here , we identified heterozygous germline apc mutations in 68% of patients in the mbwnt molecular subgroup and showed that genetic cases were indistinguishable from sporadic cases based on age at diagnosis . 
 importantly , all patients with apc - deficient mbwnt did not have the hallmark somatic driver event of mbwntnamely , somatic missense mutations in ctnnb1 ( the gene encoding - catenin )  . 
 in our series , patients with mbwnt and germline apc mutations showed favourable clinical outcomes , which mirrors the favourable outcome for patients with mbwnt with nuclear accumulation of - catenin.30 nevertheless , several patients with germline apc mutations had an additional malignancy , which emphasises the need to provide genetic counselling for patients with mbwnt in the future , irrespective of clinical outcomes . 
additional studies will be needed to assess whether or not germline apc mutations are a genetic risk factor for mbshh . given the particularly high prevalence of damaging germline mutations in patients with mbshh , we recommend that all patients with mbshh should be counselled for genetic testing . 
patients younger medulloblastoma subgroup group 3 group 4 genetic testing of family history of brca - associated cancers , or homologous recombination repair deciency , or both genetic testing of absence of somatic ctnnb1 exon 3 mutation prioritisation of genetic testing based on age or genomic instability , or both sufu , ptch1 tp53 , palb2 , and brca2 palb2 and brca2 figure 5 : proposed clinical guidelines for genetic counselling and testing in medulloblastoma based on clinical and molecular tumour characteristics than 3 years of age should initially be tested for germline mutations in sufu and ptch1 ( especially in view of the high prevalence of sufu mutations in infant patients with mbshh in our study , which is consistent with previous reports31 ) , and children older than 3 years for germline tp53 mutations . 
based on these findings we recommend conservative ordering of genetic tests in these patient groups ( eg , those with familial history of brca - associated cancers or mutational signatures are suggestive of hr deficiency specifically signatures 3 and 8 , the latter of which has previously been reported to be associated with breast cancer ) .32 genetic counselling and testing for germline palb2 and brca2 mutations in paediatric patients has so far been pursued only in case of suspected fanconi anaemia . 
 by use of integrative genomic analyses , we showed that heterozygous mutations in brca2 and palb2 are associated with an increased risk of medulloblastoma and of hr - deficient tumours . 
all identified heterozygous germline mutations are rare in the general population ( minor allele frequency < 001% ) and were classified in most patients as ( likely ) pathogenic in clinvar . 
magnusson and colleagues33 reported that families with germline mutations in brca2 had an increased prevalence of vol 19 june 2018 articles childhood tumours compared with population - based control families . 
for example , it was shown that cells from heterozygous palb2 mutation carriers exhibited an aberrant dna replication stress response and increased amounts of spontaneous genomic instability , 34 and analysis of double - strand break repair outcomes35 revealed a shift towards error - prone dna repair pathways . 
 furthermore , one study36 presented evidence showing that naturally occurring concentrations of formaldehyde , a product of cellular metabolism , can selectively deplete brca2 via proteasomal degradation and induce genomic instability . 
moreover , consequent identification of paediatric patients with heterozygous germline mutations in palb2 and brca2 will be valuable to further evaluate whether hr - deficient tumours show a particularly favourable response to standard platinum - based chemotherapy and whether they might benefit from combination therapies with parp inhibitors . germline mutations in tp53 accounted for the highest proportion of genetic cases among paediatric patients in the mbshh subgroup . 
this finding underscores the need for a dedicated treatment protocol , which is being prepared by the international society of paediatric oncology pnet 5 medulloblastoma study group and by an international registry for this high - risk patient group.37 additionally , clinical surveillance of germline tp53 mutation carriers has been shown to result in earlier detection of tumours and therefore improved long - term survival.38 we also observed rare and damaging germline mutations with potential clinical relevance in additional genes based on loss of heterozygosity analysis and somatic mutation patterns ( eg , atm and pten )  . 
a single patient harboured a heterozygous germline msh6 mutation in our discovery cohort ; however , the meaning of this observation remains uncertain owing to the absence of tumour material for molecular analyses . our study does have some limitations . 
because of the multiple ( and in part heterogeneous ) cohorts used in our study , familial history of cancer could not be obtained in a standardised form for all patients carrying a genetic predisposition . 
 larger cohort sizes in further studies will be necessary to assess the impact of germline mutations on clinical outcomes within molecular subgroups as well as relative to patients who develop sporadic medulloblastoma due to somatic mutations in the same set of genes ( eg , ptch1 , sufu , and tp53 )  . 
 furthermore , we note that our rare variant burden analysis against exac was restricted to regions covered by whole - exome sequencing , was restricted to genes previously in cancer predisposition , and excluded pathogenic germline structural variants . 
 although these steps aimed to reduce potential biases from analysing heterogeneous sequencing cohorts , we cannot rule out that particular classes of germline variation might have been under - represented . 
finally , it is also possible that additional genes are involved in medulloblastoma predisposition , which were not previously associated with hereditary cancer syndromes . involved contributors jok , pan , smp , and smw contributed to manuscript preparation and to study design . 
ag , cb , cdb , cpk , crb , cs , dm , fmdlv , kbg , kwp , and sss contributed to data interpretation . declaration of interests smw reports grants from the european molecular biology organization ( embo ) and from the swiss national science foundation , during the conduct of the study . 
mf reports grants from the swedish research council , the swedish council for health , working life and welfare , the swedish cancer society , the swedish childhood cancer foundation , and the swedish radiation protection authority , during the conduct of the study . 
cdb reports grants from the national institutes of health ( nih ) , during the conduct of the study ; grants from the university of miami , financial activities from the university of chicago ; university of california , los angeles ; hugo ; new york genome center ; university of iowa ; rockefeller university ; alexandria ; fh foundation ; concert genetics ; national autonomous university of 796 vol 19 june 2018 articles mexico ; mexican institute of social security ; colorado state university ; macarthur foundation ; and gordon conference ; and personal fees from cdb consulting ltd , personalis , inc , 23andme roots into the future project , ancestry.com , liberty biosecurity , med - tek , identifygenomics llc , mars inc , etalon inc , fish & richardson pc , eden roc , hypatia , the nicklaus childrens hospital research institute , knox medical , arc bio llc , embark veterinary , digitalis ventures , humancode , web shield , and luna dna , outside the submitted work . 
all other authors declare no competing interests . acknowledgments this project was supported by the pedbrain tumor project contributing to the icgc , funded by german cancer aid ( 109252 ) , the german federal ministry of education and research ( bmbf ; 01ku1201a and 01ku1201c ) , and additionally through bmbf grants biotop ( 01ek1502a and 01ek1502b ) , icgc - data mining ( 01ku1505f ) , medsys ( 0315416c ) and ngfnplus ( 01gs0883 )  . 
pan is the recipient of a roman - herzog postdoctoral fellowship ( hertie foundation ) , v foundation v scholar award , sontag foundation distinguished scientist award , and is a pew - stewart scholar for cancer research ( alexander and margaret stewart trust )  . 
mdt is supported by the garron family chair in childhood cancer research , and grants from the cure search foundation , the national institutes of health ( r01ca148699 and r01ca159859 ) , the pediatric brain tumor foundation , the terry fox research institute , and brainchild . 
tissue banking was supported by funds from the faculty of medicine , masaryk university ( brno , czech republic ) and kz was supported by the project azv 15 - 30657a from the ministry of health of the czech republic . 
the medulloblastoma advanced genomics international consortium ( or magic ) project is financially supported by genome canada , genome bc , terry fox research institute , ontario institute for cancer research , pediatric oncology group ontario , funds from the family of kathleen lorette and the clark h smith brain tumour centre , montreal childrens hospital foundation , hospital for sick children : sonia and arthur labatt brain tumour research centre , chief of research fund , cancer genetics program , garron family cancer centre , brain child , mdts garron family endowment , and bc childhood cancer parents association . 
we thank the dkfz genomics and proteomics core facility , andrea wittmann ( pediatric glioma research group , dkfz , heidelberg , germany ) , laura sieber ( division of pediatric neurooncology , dkfz ) , rolf kabbe ( division of theoretical bioinformatics , dkfz ; department for bioinformatics and functional genomics , institute for pharmacy and molecular biotechnology , and bioquant , heidelberg university , heidelberg , germany ) , matthias bieg ( division of theoretical bioinformatics , heidelberg center for personalised oncology , dkfz ) , matthias schlesner ( bioinformatics and omics data analytics , dkfz ) , and bernd klaus ( genome biology unit , european molecular biology laboratory [ embl ] , heidelberg , germany ) for technical support . 
this work is dedicated to prof dr enno kleihauer , who introduced molecular genetics to the field of neuro - oncology in the early 1980s , and who was one of the most influential paediatric haematologist - oncologists in germany and beyond . correction to lancet oncol 2017 ; 18 : e31529 correction to lancet oncol 2017 ; 18 : 150211 weller m , van den bent m , tonn jc , et al . 
 lancet oncol 2017 ; 18 : e31529in the panel of this review ( published online first on may 5 , 2017 ) , the dose of bevacizumab should be 10 mg / kg . 
the corrections have been made to the online version as of oct 31 , 2017 , and the printed version is correct . vol 18 november 2017 e642 corrections correction to lancet oncol 2018 ; 19 : 58081 grob jj . 
is there any interest in a new brafmek inhibitor combination in melanoma ? lancet oncol 2018 ; 19 : 58081in the title of this comment , braf - mek inhibitor was spelt incorrectly , and in the fourth paragraph one instance of the drug encorafenib was spelt incorrectly and the dose of encorafenib should have been 300 mg . 
 lancet oncol 2018 ; 19 : 70514in the summary , the following statement should have read as follows : cohort 3 was assigned to receive a dose of 100 mg / m twice daily ( maximum 100 mg per dose ) , regardless of age , equating to a maximum of 173% of the recommended adult phase 2 dose . 
 this correction has been made to the online version as of april 25 , 2018 , and the printed version is correct . vol 19 may 2018 e229 corrections corrections correction to lancet oncol 2015 ; 16 : 1013 correction to lancet oncol 2015 ; 16 : 1143 correction to lancet oncol 2015 ; 16 : 1289 declaration kopans db . 
 lancet oncol 2015 ; 16 : 1143the last line of the rst paragraph of this comment should read only this year , for example , did who add several commonly used , extremely e ective drugs , such as imatinib , trastuzumab , and cisplatin to its list of essential medicines . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the paragraph on survival with oligometastatic hcc should read the researchers found that patients with oligometastatic disease had a significantly longer overall survival than patients with extensive disease ( 104 months versus 63 months , p = 0034 )  . 
 vol 16 november 2015 e528 particularly if chemotherapy - free interventions prove successful.9 indeed , huet and colleagues show that the prognostic effect of the previously defined expression signatures of immune response 1 and 210 was lost in the prima study cohort , demonstrating how the fortunes of these predictors can fluctuate with changes in treatment , even if a role for genes linked to the tumour microenvironment was maintained . as the potency of these scoring systems continues to improve , it is essential to develop the multicentre collaborations necessary to further validate , standardise , comparisons between and enable head - to - head these different predictors . 
the wider community of follicular lymphoma oncologists must decide which models to prioritise for either validation or adoption in clinical trials , and it is imperative that a consensus is reached on the level of discrimination needed to guide treatment , especially for an indolent disease such as follicular lymphoma where a high prognostic accuracy is necessary . 
the expected refinements might well involve increasingly complex dynamic models with imaging and cell - free dna , but it is equally important that risk models do not become unnecessarily unwieldy and impractical for routine application . this new prognostic tool is an important step towards the goal of personalised care for patients with follicular lymphoma . 
there is now a pressing need to not only validate and compare emerging prognostic tools in prospective clinical trials but to consider the robustness and feasibility of these analyses in the real - world setting . shamzah araf , jessica okosun , * jude fitzgibbon centre for haemato - oncology , barts cancer institute , london ec1m 6bq , uk j.fitzgibbon@qmul.ac.uk jf declares grants from epizyme and personal fees from roche , gilead , janssen , and epizyme , outside the submitted work . 
early relapse of follicular lymphoma after rituximab plus cyclophosphamide , doxorubicin , vincristine , and prednisone defines patients at high risk for death : an analysis from the national lymphocare study . 
integration of gene mutations in risk prognostication for patients receiving first - line immunochemotherapy for follicular lymphoma : a retrospective analysis of a prospective clinical trial and validation in a population - based registry . 
 n engl j med 2004 ; 351 : 215969 . adjuvant therapy in colon cancer : less is more the results of the scot trial reported by timothy iveson and colleagues1 in the lancet oncology establish a new standard of care in the adjuvant treatment of stage iii colon cancer . 
the investigators showed the non - inferiority of treatment with 3 months of adjuvant chemotherapy versus 6 months of the same treatment in terms of 3 year disease - free survival . 
 patients treated with the shorter duration of therapy had significant reductions in adverse events , including a more than halving in the number of grade 2 or worse sensory neuropathy events . 
these results were robust in patients with low - risk stage iii ( t3 or n1 ) disease who received 3 months of capecitabine and oxaliplat however , the non - inferiority of 3 months of therapy versus 6 months could not be shown in higher risk t4 or n2 disease . 
like scot , see articles page 562 442 vol 19 april 2018 comment non - inferiority could not be shown for the shorter duration of therapy with capecitabine and oxaliplatin in the higher risk patients . 
 therapies what are the implications for changing practice to 3 months of adjuvant chemotherapy ? a shorter duration of adjuvant therapy could permit the earlier introduction of to be investigational used sequentially or combined with chemotherapy , particularly in higher risk patients . 
furthermore , it will be necessary to await the impact of findings from correlative studies done in scot and the other idea trials , given the now recognised prognostic importance of factors such as tumour sidedness , microsatellite instability , and braf or ras mutation . less might also be more in oesophageal and gastric cancers . 
in anal cancer treated with definitive chemoradiotherapy , the addition of extra cycles of chemotherapy either before or after chemoradiotherapy has been shown not to improve survival compared with chemoradiotherapy alone.6 , 7 an argument for less chemotherapy is also seen in results from trials investigating neoadjuvant or preoperative therapy in a randomised trial8 of oesophageal and gastro - oesophageal junction cancers reported by ajani and colleagues , the addition of 2 months of fluorouracil and oxaliplatin before preoperative fluorouracil plus oxaliplatin and radiotherapy did not improve survival compared with chemotherapy given only during radiotherapy . 
in the oeo5 trial , 9 which enrolled patients with oesophageal and gastro - oesophageal junction adenocarcinoma , alderson and colleagues also reported no survival benefit with four cycles of the ecx regimen ( epirubicin , cisplatin , and capecitabine ) beyond that achieved with two cycles of fluorouracil and cisplat these results support the use of a shorter duration of preoperative chemotherapy as well as the discontinuation of the use of epirubic al - batran and colleagues have reported that the addition of docetaxel to infused fluorouracil and oxaliplatin , using the flot regimen ( fluorouracil , leucovorin , oxaliplatin , and docetaxel ) as preoperative therapy , resulted in a significant survival benefit compared with preoperative ecx in patients with gastric and gastro - oesophageal junction cancers.10 if a third chemotherapy agent is to be added to preoperative fluorinated pyrimidine platinum chemotherapy , it should be docetaxel and not epirubicin . the scot investigators deserve congratulations for their practice - changing trial that can directly improve the lives of patients receiving adjuvant chemotherapy for stage iii colon cancer . 
 david h ilson gi oncology service , memorial sloan kettering cancer center , new york , ny 10011 , usa ilsond@mskcc.org i declare no competing interests . copyright the author ( s )  . 
3 versus 6 months of adjuvant oxaliplatin - fluoropyrimidine combination therapy for colorectal cancer ( scot ) : an international , randomised , phase 3 , non - inferiority trial . 
prospective pooled analysis of six phase iii trials investigating duration of adjuvant ( adjuv ) oxaliplatin - based therapy ( 3 vs 6 months ) for patients ( pts ) with stage iii colon cancer ( cc ) : the idea ( international duration evaluation of adjuvant chemotherapy ) collaboration . 
three versus six months adjuvant oxaliplatin - based chemotherapy for patients with stage iii colon cancer : the french participation to the international duration evaluation of adjuvant chemotherapy ( idea ) project . 
perioperative chemotherapy with docetaxel , oxaliplatin , and fluorouracil / leucovorin ( flot ) versus epirubicin , cisplatin , and fluorouracil or capecitabine ( ecf / ecx ) for resectable gastric or gastroesophageal junction ( gej ) adenocarcinoma ( flot4 - aio ) : a multicenter , randomized phase 3 trial . 
 proc am soc clin oncol 2017 ; 35 ( 15 suppl ) : 4004 . vol 19 april 2018 comment correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections editorial to read more about the lancet oncologys cancer campaign and the four commissions go to campaigns / cancer / for our previous editorial on direct - to - consumer marketing see lancet oncol 2008 ; 9 : 1113 tackling the cancer epidemic rising cancer is the primary cause of death in many countries , now exceeding heart disease . 
in lower income countries , fast , creating unprecedented incidence challenges for health systems , many of which were designed in an era that did not foresee , were simply incap able of pre - empting , or knowingly ignored the future . 
 however , these remarkable achievements come at a pricethe cost of care is outpacing national budgets , the numbers of cancer patients and survivors are putting greater pressures on health - care systems , and increasing numbers of vulnerable patients from less traditional demographics , such as children and younger adults , require di erent clinical solutions that have yet to be fully conceived . this month , the lancet oncology launches a campaign focused on tackling the cancer epidemic at a systems level . 
we will document , via monthly updates , the evolution of four commissions intended for publication later this year that aim to de ne the scale of the challenge , the underlying drivers , and the improvements needed to cancer - care systems . 
these special reports will cover global access to radiotherapy , surgical resource availability and its fundamental role in cancer treatment , the intersection of primary care in a comprehensive cancer service t for the 21st century , and the ongoing oncology requirements in the low - to - middle income countries of latin america . 
 the lancet oncology dangers of direct - to - consumer advertising exposed again direct - to - consumer ( dtc ) advertising is in the headlines agaon feb 19 , 2015 , 23andme was granted approval by the us food and drug administration ( fda ) to market a genetic test for bloom syndrome . 
and on feb 25 , 2015 , the us federal trade commission ( ftc ) ned two companies for marketing melanoma detection apps ( melapp and mole detective ) and banned them from making misleading or unsubstantiated health claims in the future . 
 the decision to permit 23andme limited access to the dtc market is a remarkable turnaround for a company that on nov 22 , 2013 , received an fda warning letter instructing them to stop all marketing . 
at that time , the fda insisted the company seek approval for each speci c indi cation in their pan - genomic test along with robust evidence for each claimin line with the requirements for other over - the - counter home - use tests . 
despite the seeming appro priate ness of the decision , it creates an uneasy precedentone that could open the door to other less reliable tests if the delineations of the ruling are not rmly upheld . 
these concerns are further underscored by the jnci article showing that websites promoting person alised cancer medicine products contain more information about the bene ts than the limitations , and most focus on one or more non - standard tests . ensuring people take an active interest in their health is central to a strong health - care system , but health - care decisions need to be a bilateral process between patients and their doctors . 
in our december , 2008 , editorial , we con cluded that the marketing of tests should be restricted to health professionals , rather than the lay public , and only accessed through health - care providers on the basis of their advice . 
within standard - risk medulloblastoma , patients in the wnt subgroup are established as having a favourable prognosis ; however , outcome prediction for the remaining majority of patients is imprecise . 
we assessed the clinical behaviour of the molecularly defined wnt and shh subgroups , and identified novel independent prognostic markers and models for standard - risk patients with non - wnt / non - shh disease . 
because of the scarcity and low quality of available genomic material , we used a mass spectrometry - minimal methylation classifier assay ( ms - mimic ) to assess methylation subgroup and a molecular inversion probe array to detect genome - wide copy number aberrations . 
this cohort of 136 samples consisted of 28 ( 21% ) classified as wnt , 17 ( 13% ) as shh , and 91 ( 67% ) as non - wnt / non - shh ( we considered group3 and group4 medulloblastoma together in our analysis because of their similar molecular and clinical features )  . 
favourable outcomes for wnt tumours were confirmed in patients younger than 16 years , and all relapse events in shh ( four [ 24% ] of 17 ) occurred in patients with tp53 mutation ( tp53mut ) or chromosome 17p loss . 
in patients in the hit - siop pnet4 cohort with non - wnt / non - shh medulloblastoma , with a median follow - up of 67 years ( iqr 5882 ) , 5 - year event - free survival was 100% in the favourable - risk group and 68% ( 95% ci 575827 ; p = 000014 ) in the high - risk group . 
in the validation cohort , with a median follow - up of 56 years ( iqr 3181 ) , 5 - year event - free survival was 947% ( 95% ci 852100 ) in the favourable - risk group and 586% ( 95% ci 451761 ) in the high - risk group ( hazard ratio 941 , 95% ci 1257057 ; p = 0029 )  . 
the remaining subgroups of patients with high - risk medulloblastoma might benefit from more intensive therapies . funding cancer research uk , swedish childhood cancer foundation , french ministry of health / french national cancer institute , and the german childrens cancer foundation . correspondence to : prof steven c clifford , wolfson childhood cancer research centre , northern institute for cancer research , newcastle university , newcastle upon tyne , ne1 7ru , uk steve.clifford@ncl.ac.uk copyright 2018 the author ( s )  . 
 currently , who classification of cns tumours recog nises four distinct genetically defined entities ( wnt , shhtp53wildtype , shhtp53mut , and nonwnt / nonshh ) .1 nonwnt / nonshh medullo blastoma encompasses group3 and group4 , which were defined by epigenetic and mrna expression signatures2 and are considered provisional variants by the 2016 who classification.1 understanding the molecular pathology and clinical relevance of medulloblastoma subtypes provides sub for personalised riskadapted stantial opportunities therapies . discovery and validation of clinically meaningful medullo blastoma features in previous clinical trial cohorts have driven advances in the clinical management of the disease . 
children younger than 16 years of age at diagnosis with wntactivated medulloblastomas have research in context evidence before this study international consensus and the 2016 who classification recognise the following distinct clinico - molecular disease entities in medulloblastoma : wnt , shh - tp53wild - type , shh - tp53mut , and non - wnt / non - shh ( encompassing group3 and group4 )  . 
standard - risk , non - infant disease ( with 7585% 5 - year progression - free survival and affecting 5060% of patients ) represents the largest clinical treatment group of patients . 
application of novel methods to enable assessment of this cohort , and investigation of an independent demographically matched standard - risk medulloblastoma validation cohort , allowed derivation and validation of biomarker - driven , risk - stratification models on the basis of the molecular pathology of standard - risk medulloblastoma , including a novel whole chromosomal cytogenetic aberration signature within standard - risk non - wnt / non - shh medulloblastoma . 
 therefore , findings from this study resolve current patients with standard - risk medulloblastoma into biomarker - defined distinct favourable - risk and high - risk groups , and represent a substantial step in our ability to risk stratify and clinically manage medulloblastoma . implications of all the available evidence the results of this study redefine the concepts of risk stratification in standard - risk medulloblastoma , providing insight into its molecular subtypes , their underpinning biology , and clinical application . 
stratification of standard - risk medulloblastoma by use of the biomarkers and validated schemes we describe could allow assignment of 150200 patients per year in europe into a favourable - risk group , and such patients could benefit from reduction of treatment intensity . 
this group encompasses tumours of all variants except high risk shhtp53mut.6 , 7 diagnosis of favourablerisk , wnt disease ( around 20% of patients with standardrisk medulloblastoma ) provides a clear precedent for therapy deescalation within clinical trials . 
by contrast , patients with nonwnt , standardrisk medullo blastoma have ( 5year eventfree survival heterogeneous outcomes around 75% ) , and further actionable risk groups are yet to be identified or validated to the point of clinical application . 
 the favourable risk of patients with standardrisk , shh tp53wildtype medulloblastoma6 , 7 identified in retrospective series requires validation in clinical trials , and reproducible and clinically significant molecular pathological features with in nonwnt / nonshh tumours remain to be defined . 
trial participants were post operatively staged and randomly assigned to treat ment with standard or hyperfractionated radio therapy , followed by chemo therapy with eight cycles of cisplatin , lomustine , and vincristine . 
this analysis , alongside an independent , demo graphically matched , standardrisk medullo bla stoma validation cohort , enabled the discovery and validation of concerted whole chromosomal aberration signatures with prognostic value for patients with nonwnt / non shh medulloblastoma . 
the study investigated in patients aged 421 years using either hyperfractionated radiotherapy or standard delivery radiotherapy followed by chemo therapy.1 standard delivery radiotherapy comprised 234 gy to the craniospinal axis and 54 gy to the whole posterior fossa , and was given over 42 days in 30 fractions of 18 gy each day for 5 days per week . 
 eight cycles of cisplatin ( 70 mg / m intravenously ) and lomustine ( 75 mg / m ) on day 1 , and vincristine ( 15 mg / m intravenously ) on days 1 , 8 , and 15 , were given with a 6 week interval between each cycle.14 minute remnant material ( cytospinconcentrated cellular nuclei preparations ) or tumour sections , origi nally intended for fish and ihc , 15 were available for analysis ( samples from 147 patients )  . 
we retained tumours from patients with subtotally resected disease18 or categorised as mycnamplified to assess their prognostic value in a clinically controlled cohort.6 , 11 , 15 we excluded myc - amplified tumours because of their established poor prognosis.5 136 tumour samples met these criteria and underwent molecular investigation . 
median year of diagnosis 2006 . table : clinical and molecular characteristics of all cohorts vol 19 december 2018 1605 articles tumour samples ( clinical and molecular cohort ) and their prognostic features were consistent with the whole trial cohort ( table )  . we validated and extended our findings in a second independent , demographically matched , retrospective cohort of patients with nonwnt / nonshh standardrisk medulloblastoma ( n = 70 ) collected at uk childrens cancer and leukaemia group and european society for paediatric oncology ( siope ) associated treatment centres between 1990 and 2014 . 
patients in this cohort received equivalent therapies ( maximal surgical resection [ all patients ] , adjuvant craniospinal radiotherapy [ all patients ; standard radiotherapy in variable doseslow dose : 2427 gy , 39 patients ; high dose : 3539 gy , 27 patients ; hyperfractionated radiotherapy variable doses : 324 gy craniospinal radiotherapy plus 234 gy boost , one patient ; 60 gy hyperfractionated accelerated radiotherapy , one patient ; 31 / 59 gy , one patient ; and 39 / 54 , one patient ] , and chemotherapy [ 65 ( 93% ) of 70 patients ] )  . written informed consent for tumour collection for biological studies was obtained from patients or their parents . 
we analysed mutations in exons 49 of tp53 and exon 3 of ctnnb1 with sanger sequencing as previously described.21 we assessed mutations in apc using a customised next generation dna sequencing panel ( illumina ; san diego , ca , usa ) in samples with ctnnb1wildtype wnt medulloblastoma . 
we used gistic ( genomic identification of significant targets in cancer , v 1.0 ) to identify focal chromosomal aberrations ( appendix pp 1012 ) .22 we analysed the validation cohort samples on the illumina 450k dna methylation micro array ( illumina ; san diego , ca , usa ) , and estimated chromosomal and focal copy number changes by use of the r package conumee v 1.13.0 , as previously described.6 we defined a whole chromosomal aberration group of patients by hier archical clustering of recurrent ( ie , > 15% ) aberrations . eventfree survival was defined as the time from surgery to first event ( progression or relapse ) , or date of last followup . 
after molecular sub grouping , we observed similar cytogenetic changes and eventfree survival between the nonwnt / nonshh medullo blastomas subclassified as group3 and group4 ( appendix p 9 )  . 
because of these results and the emerging evidence of their shared biology , 6 , 12 we considered these groups together in subsequent eventfree survival analyses . to test the null hypothesis that eventfree survival was not associated with clinical , molecular , or patho logical variables in patients with group3 or group4 medullo blastoma , we constructed kaplanmeier curves and compared patient groups with logrank tests . using cox modelling , we tested the prognostic value of clinical markers ( gender , radiotherapy type [ hyper fractionated vs standard ] , resection outcome [ subtotal vs fullyresected disease ] , mycn amplifi cation [ yes vs no ] , histology type [ desmoplastic / nodular vs classic histo logy ] ) , ( recurrent whole chromo somal cytogenetic markers aberration [ presence vs absence ] ) , and cumulative numbers of total whole chromosomal aber rations ( gains vs losses )  . 
we derived pragmatic assignments of patient risk by combining whole chromosomal aberrations that were significantly different in univariate testing to define risk groups and assessed their predictive value by calcu lating total area under the curve ( auc ) , sensitivity , and specificity at 5 years since diagnosis ( appendix p 2 )  . 
residual scores from tests of association are shown ( darker shades of grey indicate stronger enrichment ) alongside p values from fishers exact tests . finally , to better understand the nature of the identified risk groups , we classified the validation cohort according the recently published refinements of epigenetically defined substructures within non wnt / nonshh medullo blastoma.6 , 12 validation cohort samples were assigned to subgroup variants according these published studies and visualised using tdistributed stochastic neighbour embedding ( appendix pp 23 )  . we set the significance threshold at p < 005 for all statistical tests in this study , and twotailed p values are reported . 
we assessed significance of association using fishers exact test , and visualised the strength of asso ciations using test residuals . further detailed methods are provided in the appendix pp 13 . 
event - free survival for patients with non - wnt / non - shh disease ( n = 91 ) grouped as ( e ) patients with mycn amplified vs non - amplified tumours , ( f ) patients with medulloblastomas presenting an i17q or not , and ( g ) patients with medulloblastomas with or without whole chromosomal aberration . 
we found no differences in terms of 5year eventfree survival between the four methylation subgroups ( figure 2 ; wnt 5year eventfree survival 885% , 95% ci 770100 ; group4 5year eventfree survival 816% , 733908 ; group3 5year eventfree survival 800 , 621100 ; shh 5year eventfree survival 753% , 569996 ; wnt vs group4 hr 061 , 95% ci 018212 , p = 044 ; shh vs group4 127 , 042386 , p = 068 ; group3 vs group4 113 , 032394 , p = 085 )  . 
both ctnnb1 wildtype tumours showed a copy neutral loss of vol 19 december 2018 1609 articles heterozygosity within chromosome 5q ( apc ) and we identified apc frameshift deletions ( e1309fs aaaag and q1062fs acaaa )  . 
 a previously reported shh disease risk model ( of chromosome 14 loss and gli2 amplification ) 11 showed significantly worse eventfree survival for patients in this cohort ( p = 000067 ; appendix pp 78 )  . 
as expected , we observed structural cytogenetic ( eg , i17q ) and focal aberrations ( including mycn amplifications , otx2 , ccnd2 , and 18q12 [ tpte2 ] gains or ampli fications , sncaip dupli cations , and 13q1112 [ setbp1 ] loss ; figure 1 ; appendix pp 1112 )  . 
moreover , previously reported prognostic ( mycn amplification , i17q alterations , and sub total resection ) 11 , 18 were not associated with worse eventfree survival ( figure 2 ; appendix p 15 ) , while the observed cohortwide prognostic significance of whole chromosomal aber rations was maintained in this subgroup ( figure 2 )  . factors we next investigated whether the observed mole cular heterogeneity within the 91 nonwnt / nonshh medullo blastoma tumours could inform its biological basis and clinical behaviour . 
the first cytogenetic group was strongly associated with a pattern of i17q in isolation , diploid karyotypes , few recurrent whole chromosomal aberrations , and more relapses ( p = 000084 )  . 
the second cytogenetic group was char acterised by a spectrum of multiple recurrent and co incident whole chromosomal aberrations ( figure 3 ) and aneuploidy ( p < 00001 ; appendix p 13 ) , and was associated with fewer relapses . whole chromosomal aberrations within nonwnt / nonshh medulloblastoma samples were associated with improved 5year eventfree survival ( figure 4 )  . 
 55 ( 60% ) of 91 nonwnt / nonshh tumours had multiple recurrent and coincident whole chromo somal aberrations and showed favourable outcomes compared with those without whole chromosomal aberrations ( hr 016 , 95% ci 005050 ; p = 00015 ; figure 4 )  . 
 when different whole chromosomal aberration numbers were assessed , timedependent auc analysis identified 0 versus 1 or more recurrent whole chromosomal losses as the best discri minator of outcome ( figure 4 ; appendix p 14 )  . 
event - free survival per ( a ) whole chromosomal aberration cytogenetic subgroup and ( b ) recurrent whole chromosomal losses ( 0 vs 1 or more changes )  . 
the standard - risk medulloblastoma validation cohort is indicated by filled and open circles according to risk , with relationship to the schwalbe and colleagues6 and northcott and colleagues12 cohorts shown by t - distributed stochastic neighbour embedding plots . 
the median eventfree survival for these patients was 56 years ( iqr 3181 )  . the characteristics , incidence , and associated event free survival outcomes of the identified whole chromo somal aberrationdefined subgroups were recapitulated ( figure 5 ; appendix p 17 )  . 
the favourablerisk whole chromosomal aberration signature , defined by chromo some 7 gain , chromosome 8 loss , and chromo some 11 loss , was observed within multiple novel methylation subgroups , and was significantly associated with mbgroup4lowrisk 6 and group3 and group4 subtypes vi and vii12 ( p < 00001 , appendix p 18 )  . 
however , patients older than 16 years did not share this good prognosis , consistent with previous reports.15 , 23 together , these data do not support therapy deescalation in patients with wnt medulloblastoma older than 16 years of age . 
these data validate independent previous findings6 , 7 and support the eligibility of these patients for deescalated or targeted therapies ( eg , smo inhibitors ) .24 development of biomarkerdriven treatment strategies for the large remaining group of patients with nonwnt / nonshh disease represents the largest ongoing chal lenge for standardrisk medulloblastoma . 
as described in this article , nonwnt / non shh medulloblastoma tumours have few recurrent mutations , and structural chromosomal abnor malities are the most common genomic features.810 when comparing group4 and group3 tumours , we found around 90% overlap of chromosomal alterations between the two subgroups and equivalent eventfree survival . 
these tumours provide a wider biological context for the poorrisk group of patients with nonwnt disease with chromosome 17p or q defects in a diploid background ( chr17 ( im ) / diploid ( cen ) ) , previously identified by interphase fish in this cohort.15 the second group was large and defined by multiple , cooccurring whole chromosomal aber rations , common polyploidy , and improved relative outcomes . in this whole chromosomal aberration group , using multivariable eventfree survival analysis and risk modelling , we deduced a whole chromosomal aberration signature ( two or more of chromosome 7 gain , chromo some 8 loss , and chromosome 11 loss ) , which best defined patients with nonwnt / nonshh medulloblastoma with 1614 vol 19 december 2018 articles favourable prognosis . 
this whole chromosomal aberration signature was detected within a number of novel methylation subgroups within nonwnt / nonshh medulloblastoma , and associated with the lowrisk mbgroup4lowrisk , 6 and group3 and group4 subtypes vi and vii.12 by contrast , the highrisk isolated i17q diploid group was associated with highrisk mbgroup4 6 and subtype viii.12 these associations suggest highrisk common biological phenotypes and evaluation of their relative contributions to risk stratifi cation could be investigated in future clinically controlled studies . biologically and clinically significant whole chromo somal phenotypes are a notable feature of childhood malignancies other than medulloblastoma . 
characteristic patterns of nonrandom whole chromosomal aberrations in neuroblastoma ( socalled wholechromosomal changes phenotype ; more than two whole chromosomal aber rations ) 25 , 26 and high hyperdiploid acute lymphoblastic leukaemia ( socalled highhyperdiploidy phenotype [ heh ] ; 5165 chromosomes ) 27 define tumour subgroups with favourable prognoses . 
additionally , choroid plexus papil lomas and adult infratentorial ependymomas ( posterior fossa ependymoma type b ) are characterised by multiple whole chromosomal abberations.1 overall , whole chromosomal aberration signatures are associated with a low number of single nucleotide mutations . this common involvement of whole chromosomal aberration signatures provides strong impetus to under stand the underlying molecular pathomechanisms , including errors in mitotic control , chromosome segre gation , and function of the spindle apparatus . 
although beyond the scope of this study , investigation of associated biology ( eg , geneexpression profiles , pathway involve ments , and driver events ) and the involvement of specific chromosomes ( ie , chromosomes 7 , 8 , and 11 ) , is essential to improve understanding and therapeutic targeting . 
for instance , vincristine ( a component of medulloblastoma treatment regimens ) directly targets the spindle apparatus , and the excellent whole chromosomal aberration signature associated outcomes might be explained by high sensitivity to such treatments . 
 combination of these newly defined subtypes with the favourablerisk wnt and shh medulloblastomas validated in our study redistributed around 50% of patients with standardrisk medulloblastoma into a favourablerisk group , who could benefit from reducedintensity therapies aimed at maintaining overall survival while reducing treatmentassociated toxicities and late effects . 
we sought to establish whether indocyanine green fluorescent dye is non - inferior to isosulfan blue dye in detecting sentinel lymph nodes in women with cervical and uterine cancers . methods in this non - inferiority , within - patient comparison study , patients aged 18 years or older with clinical stage i endometrial or cervical cancer undergoing curative surgery were randomly assigned 1 : 1 to lymphatic mapping with isosulfan blue dye ( visualised by white light ) followed by indocyanine green ( visualised by near - infrared imaging ) , or indocyanine green followed by isosulfan blue dye . 
 the primary outcome was efficacy of intraoperative indocyanine green with near - infrared fluorescence imaging versus that of isosulfan blue dye in the identification of lymph nodes , defined as the number of lymph nodes identified by indocyanine green and isosulfan blue dye , respectively ( and confirmed as lymphoid tissue by histology ) , divided by the number of lymph nodes identified intraoperatively and excised . 
the study had a 5% non - inferiority margin needed to show non - inferiority of the frequency of lymph node detection with indocyanine green to that with isosulfan blue dye with 80% power at a 5% two - sided significance level . 
the trial was registered with clinicaltrials.gov , number nct02209532 , and is completed and closed . findings between dec 21 , 2015 , and june 19 , 2017 , 180 patients were enrolled and randomly assigned to the two groups ( 90 to each group ) ; 176 patients received the intervention and were evaluable ( modified intention - totreat population )  . 
517 sentinel nodes were identified in the per - protocol population ( n = 163 ) , of which 478 ( 92% ) were confirmed to be lymph nodes on pathological processing : 219 ( 92% ) of 238 nodes that were both blue and green , all seven nodes that were blue only , and 252 ( 95% ) of 265 nodes that were green only ( p = 033 )  . 
 in total , 471 ( 97% ) of 485 lymph nodes were identified with the green dye and 226 ( 47% ) with the blue dye ( difference 50% , 95% ci 3962 ; p < 00001 )  . 
in the modified intention - to - treat population ( n = 176 ) , 545 nodes were identified , of which 513 ( 94% ) were confirmed to be lymph nodes on pathological processing : 229 ( 92% ) of 248 nodes that were both blue and green , all nine nodes that were blue only , and 266 ( 95% ) of 279 nodes that were green only ( p = 030 )  . 
the technique of lymphatic mapping and sentinel lymph node biopsy has improved surgeons ability to detect small - volume disease in lymph nodes while greatly reducing intraoperative and postoperative morbidity . 
this technique has been validated and is 1394 vol 19 october 2018 articles research in context evidence before this study before development of the concept for the film study and the production of the subsequent protocol , we reviewed the medical literature to evaluate the off - label use of indocyanine green and near - infrared imaging for lymphatic mapping and sentinel lymph node biopsy in all solid tumours . 
we searched pubmed and clinicaltrials.gov , without date or language restrictions , using the terms indocyanine green , icg , near infrared imaging , lymphatic mapping , and sentinel node . 
we identified several small , single - institution retrospective reports of interstitial injection of indocyanine green for lymphatic mapping in a wide range of solid tumours including breast , uterine , cervical , vulval , lung , kidney , and colon cancers as well as cutaneous melanoma . 
 all these studies showed that use of indocyanine green with near - infrared imaging was feasible and safe for lymphatic mapping in solid tumours and that the technique might potentially improve on substances currently approved by the us food and drug administration for mapping such as patent blue dyes and radiocolloids . 
however , no prospective , controlled studies had compared the use of indocyanine green as a mapping substance with standard of care . added value of this study although the film study was designed as a non - inferiority comparison of the efficacy of intraoperative indocyanine green with near - infrared imaging to blue dye in the identification of lymph nodes , our results showed superiority of the experimental group over standard of care . 
it also identified all sentinel nodes with metastatic disease , whereas isosulfan blue dye missed a large proportion of them . implications of all the available evidence the results of this study will serve as the basis for an application to the food and drug administration for on - label use of interstitial injection of indocyanine green combined with near - infrared imaging for lymphatic mapping . 
if it is approved for on - label use , it will hopefully become the new standard of care for lymphatic mapping and sentinel lymph node biopsy for women with cervical and uterine cancers , and could subsequently be adopted as the mapping substance of choice across multiple subspecialties in surgical oncology . widely accepted as part of the surgical treatment of vulval and breast carcinomas and cutaneous melanoma . 
 gynaecological oncologists are also starting to adopt lymphatic mapping and sentinel node biopsy for women with cervical and uterine cancers.13 in lymphatic mapping for cervical and uterine cancers , mapping agents are most commonly injected into the cervix , a practice that should result in drainage to bilateral sentinel nodes in the pelvis . 
if lymphatic mapping does not identify bilateral sentinel nodes , well accepted algorithms recommend complete pelvic lymphadenectomy on the side with no sentinel nodes detected.4 , 5 because complete pelvic lymphadenectomy increases surgical time and the risks of intraoperative vascular injury and postoperative lower extremity lymphoedema and lymphocyst formation , it is crucial that lymphatic mapping identifies bilateral sentinel nodes . historically , patent blue dye with or without radiocolloid has been the most commonly used agent for lymphatic mapping in women with uterine cancers . 
 however , blue dye alone identifies at least one sentinel node in only 80% of patients and bilateral sentinel nodes in as few as 50% of patients.6 combining blue dye with radiotracer increases the rate of detection of at least one sentinel node to 88% , but the rate of detection of bilateral sentinel nodes to only 51%.6 with either technique , therefore , almost half of women with uterine cancer undergoing lymphatic mapping might require unilateral or bilateral pelvic lymphadenectomy , which increases the risk of surgical complications and long - term morbidity . the fluorescent dye indocyanine green has been explored as an off - label alternative to blue dye for lymphatic mapping in cervical and uterine cancers . 
 small series have shown the potential of interstitial indocyanine green injection to improve frequency of sentinel node detection over that observed with blue dye.79 however , no prospective , randomised studies have compared interstitial blue dye with indocyanine green injections for lymphatic mapping in cervical and uterine cancers . 
we therefore conducted the film ( fluorescence imaging for lymphatic mapping ) trial , which was designed to compare the detection of lymph nodes after interstitial indocyanine green injection versus interstitial isosulfan blue dye injection ( the standard of care ) in women with cervical and uterine cancers . methods study design and participants the film trial was an international , multicentre , randomised , open - label , phase 3 study designed to assess the safety and efficacy of indocyanine green and pinpoint near - infrared fluorescence imaging ( stryker , kalamazoo , mi , usa ) in identification of lymph nodes in women with cervical and uterine malignancies undergoing lymphatic mapping following interstitial vol 19 october 2018 1395 articles see online for appendix cervical injection of coloured dye . 
 comparison we chose this design because it would meet our primary objective and give us reliable results with fewer patients than if we had two separate randomised groups . participating surgeons were required to have completed at least ten lymphatic mapping procedures , including at least three with the pinpoint near - infrared fluorescence imaging system , before the initiation of enrolment . 
 patients were eligible for enrolment if they were 18 years of age or older , diagnosed with international federation of gynecology and obstetrics clinical stage i cervical or uterine cancer ( any histology ) , and were scheduled for curative surgery that included lymph node assessment . 
patients were ineligible if they had previous pelvic dissection or irradiation , advanced cervical or uterine cancer , t3 or t4 lesions , cervical tumour size larger than 2 cm , hepatic dysfunction defined as a model for end - stage liver disease score of 10 or greater , renal dysfunction defined as serum creatinine of 20 mg / dl or greater , or a known allergy to indocyanine green , iodine , iodine dyes , isosulfan blue , or triphenylmethane . the protocol was approved by institutional review boards at each centre , and all patients enrolled gave written informed consent . 
the protocol is available in the appendix ( p 3 )  . randomisation and masking participants were prospectively enrolled into the film trial and underwent random assignment on the day of surgery . 
 participants were randomly assigned on a 1 : 1 basis to either lymph node mapping with isosulfan blue dye followed by lymph node mapping with indocyanine green dye and near - infrared imaging ( pinpoint ) , or lymph node mapping with indocyanine green dye and near - infrared imaging ( pinpoint ) followed by lymph node mapping with isosulfan blue dye . 
randomisation was stratified by study site , with permuted block randomisation within the opportunity for the sequence to be predicted , the block size was variable and randomly chosen from small multiples of two ( ie , two , four , or six )  . 
all participants were masked to their randomisation assignment ( because they were under anaesthesia ) until after the procedure . procedures patients were removed from the study if found to not meet eligibility criteria or if they requested removal at any time before surgery ( patients could request removal at any time during the study )  . 
after general anaesthesia was achieved , the first dye was injected in the cervix deeply and superficially at both 0300 h and 0900 h , followed by the second dye deeply and superficially at both 0300 h and 0900 h , for a total of eight injections . 
for the blue dyeindocyanine green group , the isosulfan blue dye injections were done first , and for the indocyanine greenblue dye group , the indocyanine green injections were done first . 
each blue dye injection consisted of 1 ml of a 10 mg / ml isosulfan blue dye solution ( 1% isosulfan blue ) , for a total dose of 40 mg ; each indocyanine green injection consisted of 1 ml of a 125 mg / ml indocyanine green solution ( novadaq technologies , mississauga , on , canada ) for a total dose of 5 mg . the surgeon identified lymph nodes and lymphatic vessels with white light for isosulfan blue dye ( blue nodes ) or near - infrared imaging with pinpoint for indocyanine green ( green fluorescent nodes ) depending on random isation cohort . 
to minimise the chance that leakage of blue dye or indocyanine green would interfere with mapping , mapping was done first on one side of the pelvis and then on the other side . 
in both patient groups , mapping with the first dye was completed before mapping with the second dye was started , and mapping with both dyes was completed before any lymph nodes were excised . 
mapping with indocyanine green was considered complete when the surgeon identified all green nodes or determined that green nodes could not be identified and the surgeon had scanned the full 360 - degree area within the abdominal cavity . 
 1396 vol 19 october 2018 articles 199 patients screened 19 excluded 180 enrolled and randomly assigned 3 did not receive intervention 1 due to iodine allergy 1 due to negative margins on cone biopsy 1 due to presence of intraperitoneal metastatic disease on laparoscopic exploration 6 protocol violations 2 due to pregnancy test not done on day 0 1 due to incorrect blue dye used 1 due to presence of intraperitoneal metastatic disease on laparoscopic exploration 1 due to no calculation of meld score 1 due to equipment malfunction 90 assigned to blue dyeindocyanine green 90 assigned to indocyanine greenblue dye 87 received intervention and included in mitt analysis 89 received intervention and included in mitt analysis 1 did not receive intervention 1 had excessive bleeding and did not undergo injection of mapping substances 7 protocol violations 3 due to no calculation of meld score 1 due to equipment malfunction 1 due to conversion to open surgery 1 due to incorrect dose of blue and green dye injections 1 due to participation in another trial 81 included in per - protocol analysis 82 included in per - protocol analysis figure : trial profile mitt = modified intention - to - treat . 
 bilateral lymphatic mapping was done according to published national comprehensive cancer network guidelines.4 , 5 all sentinel lymph nodes resected had confirmation of nodal tissue by haematoxylin and eosin staining . 
all participants had standard - ofcare assessments throughout the study according to the hospital or institutions standard procedures , and study - specific visits to monitor occurrence of any adverse events or adverse device effects on postoperative day 1 , the date of discharge , and day 30 ( or within 7 days before or after this date )  . 
 adverse events were characterised as mild , moderate , or severe and assigned relationship ( suspected or not suspected ) to either dyes or device . outcomes the primary endpoint was efficacy of intraoperative indocyanine green with near - infrared fluorescence imaging versus that of blue dye in the identification of lymph nodes , defined as the number of lymph nodes identified by each dye ( and confirmed as lymphoid tissue by histology ) divided by the number of lymph nodes identified intraoperatively and excised . 
secondary end points were the rate of intraoperative detection of at least one sentinel node per patient and the rate of detection of bilateral sentinel nodes with indocyanine green compared with isosulfan blue dye , and the safety of each detection method . 
two other secondary endpoints ( the proportion of lymph nodes identified from following lymphatic channels and the anatomical distribution of lymph nodes ) will be reported in a separate publication . statistical analysis we hypothesised that the use of indocyanine green and near - infrared imaging would be non - inferior to isosulfan blue dye in the detection of sentinel nodes . 
analysis of the primary endpoint was done with a two - sided 95% ci for the difference in proportions using the approach described by nam and kwon for clustered matched - pair data ( the clustering in question being lymph nodes nested within patients ) .11 formal testing for hetero geneity was not completed . 
 results between dec 21 , 2015 , and june 19 , 2017 , 180 patients were enrolled and randomly assigned to the two groups ( 90 to each group ) , of whom 176 received the intervention and were evaluable ( figure )  . 
169 ( 96% ) of 176 patients had uterine cancer and seven ( 4% ) had cervical cancer . after exclusion of 13 patients with major protocol violations ( six in the blue dyeindocyanine green group and seven in the indocyanine greenblue dye group ) , there were 163 in the per - protocol population and primary analytical cohort . 
in this population , 517 nodes were identified intraoperatively and excised , of which 478 ( 92% ) were confirmed to be lymph nodes : 219 ( 92% ) of 238 nodes that were both blue and green , all seven nodes that were blue only , and 252 ( 95% ) of 265 nodes that were green only ( p = 033 ; table 2 )  . 
in total , 471 ( 97% ) of 485 lymph nodes were identified with the green dye and 226 ( 47% ) with the blue dye ( difference 50% , 95% ci 3962 ; p < 00001 )  . 
thus , we were able to conclude that indocyanine green is not inferior to isosulfan blue dye in the identification of nodes . the mean number of nodes per patient in the per - protocol population was 32 ( sd 16 )  . 
at least one node was identified in 159 ( 98% ) of 163 patients with indocyanine green and in 124 ( 76% ) of 163 patients 1398 vol 19 october 2018 articles with isosulfan blue dye ( difference 22% , 95% ci 1732 ; p < 00001 )  . 
bilateral sentinel nodes were identified in 134 ( 82% ) patients , 52 ( 32% ) with isosulfan blue dye and 132 ( 81% ) with indocyanine green ( 49% , 4157 ; p < 00001 )  . 176 evaluable patients received at least one injection of indocyanine green or blue dye and constituted the mitt population . 
545 nodes were identified in total , of which 513 ( 94% ) were confirmed to be lymph nodes : 229 ( 92% ) of 248 nodes that were both blue and green , all nine nodes that were blue only , and 266 ( 95% ) of 279 nodes that were green only ( p = 030 ; table 2 )  . 
thus , we were able to conclude that indo cyanine green is superior to isosulfan blue dye in the identification of nodes . in the mitt population , at least one node was identified in 168 ( 95% ) of 176 patients with indocyanine green and 131 ( 74% ) patients with isosulfan blue dye ( difference 21% , 95% ci 1428 ; p < 00001 )  . 
bilateral sentinel nodes were identified in 54 ( 31% ) of 176 patients with isosulfan blue dye and 138 ( 78% ) of 176 patients with indocyanine green ( 47% , 3056 ; p < 00001 )  . in the 545 nodes ( mean 31 nodes [ sd 17 ] per patient ) identified in the mitt population , isosulfan blue dye identified 257 ( 47% ) sentinel nodes ( mean 15 [ 13 ] per patient ) and indocyanine green identified 527 ( 97% ) sentinel nodes ( mean 30 [ 17 ] per patient ; difference 50% ; 95% ci 3961 ; p < 00001 )  . 
difference estimates and 95% cis indicated that estimates of superiority were consistent throughout all sites ( data not shown )  . randomisation group did not affect the ability of isosulfan blue dye or indocyanine green to detect any or bilateral sentinel nodes in the mitt population . 
in the 87 patients in the blue dyeindocyanine green group , at least one sentinel node was identified in 63 ( 72% ) patients with isosulfan blue dye and in 83 ( 95% ) patients with indocyanine green . 
in the 89 patients in the indocyanine greenblue dye group , at least one sentinel node was identified in 68 ( 76% ) patients with isosulfan blue dye and in 85 ( 96% ) patients with indocyanine green . 
in the indocyanine greenblue dye group , isosulfan blue dye detected a sentinel node in two ( 2% ) patients without a sentinel node detected by indocyanine green . per - protocol population modified intention - to - treat population proportion detected p value p value proportion detected 033 030 219 / 238 229 / 248 indocyanine green only 252 / 265 confirmation of nodal tissue in sentinel lymph node blue dye plus indocyanine green blue dye only identification of one or more sentinel lymph nodes indocyanine green only blue dye only identification of bilateral sentinel lymph nodes indocyanine green only blue dye only 100% 159 / 163 124 / 163 132 / 163 54 / 163 100% 266 / 279 168 / 176 131 / 176 138 / 176 54 / 176 < 00001 < 00001 < 00001 < 00001 table 2 : sentinel lymph node identification by indocyanine green and isosulfan blue dye in the blue dyeindocyanine green group , isosulfan blue dye identified bilateral sentinel nodes in 28 ( 32% ) of 87 patients , indocyanine green identified bilateral sentinel nodes in 67 ( 77% ) patients , and indocyanine green identified bilateral sentinel nodes in 40 ( 46% ) patients without bilateral sentinel nodes identified by isosulfan blue dye . 
in the indocyanine greenblue dye group , isosulfan blue dye identified bilateral sentinel nodes in 26 ( 29% ) of 89 patients , indocyanine green identified bilateral sentinel nodes in 71 patients ( 80% ) , and isosulfan blue dye identified bilateral sentinel nodes in two patients ( 2% ) without bilateral sentinel nodes identified by indocyanine green . as a post - hoc analysis , we assessed metastatic disease . 
macrometastatic disease was found in eight ( 38% ) of 21 sentinel nodes , micro metastatic disease in five ( 24% ) , and isolated tumour cells in eight ( 38% )  . there were no allergic reactions or adverse events attributable to either isosulfan blue dye or indocyanine green . 
most adverse events were related to surgery ( eg , postoperative pain or ileus )  . discussion although this study was designed as a non - inferiority trial , our findings suggest that indocyanine green was superior to isosulfan blue dye in identifying sentinel lymph nodes in women with cervical and uterine cancer because indocyanine green identified sentinel lymph nodes in a much larger proportion of patients than isosulfan blue dye did . 
indocyanine green was also significantly superior to isosulfan blue dye in detecting vol 19 october 2018 1399 articles together does not seem at least one sentinel node and in detecting bilateral sentinel nodes . 
the use of indocyanine green and isosulfan blue dye be necessary , because the addition of isosulfan blue dye to indocyanine green identified few sentinel nodes beyond those identified with indocyanine green alone . 
 finally , interstitial injection of indocyanine green seems to be safe , as we recorded no adverse events related to the compound . our findings that isosulfan blue dye detected at least one sentinel node in 131 ( 74% ) of 176 patients and indocyanine green detected at least one sentinel node in 168 ( 96% ) of 176 patients in the mitt population are similar to what has been previously reported in the literature.6 however , blue dye alone detected bilateral lymph nodes in only 54 ( 31% ) patients in the mitt population , which is lower than the 5560% reported in previous studies.13 , 14 all surgeons participating in our study had attained proficiency in the mapping procedure , so it is difficult to attribute the low rate of detection of bilateral nodes with isosulfan blue dye alone to poor technique or learning curve . 
multiple single - institution studies have found indocyanine green to be superior to blue dye and radiocolloid in detecting bilateral sentinel nodes after a cervical injection , 15 , 16 but a large , multi - institutional retrospective study did not show a difference between the two techniques.17 systematic reviews and meta - analyses also present conflicting results , with some showing combination blue dye and radiocolloid equivalent to indocyanine green in detecting bilateral sentinel nodes18 whereas others show that compared with use of blue dye alone , combined tracers might improve detection of at least one sentinel node but not detection of bilateral nodes.6 although the combination of blue dye and radiocolloid might be better than blue dye alone and equivalent to indocyanine green in detecting sentinel nodes , no studieseither prospective or retrospective have compared the combination of blue dye and radiocolloid with indocyanine green . 
however , the effect was much more pronounced with blue dye alone than with indocyanine green alone.8 because of the high rate of obesity in women with uterine cancer , many gynaecological oncologists have adopted the robotic system to assist in performing hysterectomy and staging , citing as their reason that the robotic system makes it easier to perform the lymphadenectomy portion of the surgery in women with a high bmi.19 , 20 the most commonly used robotic platform , the da vinci surgical system ( intuitive surgical , sunnyvale , ca , usa ) , includes an option for intraoperative near - infrared imaging called the firefly ( originally developed by novadaq technologies )  . 
 the fires trial , 21 a prospective cohort study , showed that indocyanine green and near - infrared imaging in the da vinci system had a sensitivity of 97% in detecting metastatic disease in sentinel nodes . 
the film protocol did not require completion of lymphadenectomy after sentinel node detection , so sensitivity and negative predictive values for the pinpoint system cannot be calculated in our study . 
moreover , the pinpoint technology and image display used in our study differed from that of the firefly , so the results of our study cannot be extrapolated to robotic surgery . 
in the fires study , at least one sentinel node was identified in 293 ( 86% ) of 340 patients , which is lower than the proportion of patients shown to have at least one sentinal node with indocyanine green and the pinpoint system in our study . 
additionally , the indocyanine green used in this study ( ic2000 ) might differ from the indocyanine green used in the fires trial ( no details given in the trial )  . 
 however , we believe lymphatic mapping and sentinel node detection with indocyanine green and near - infrared imaging is probably similar in the two systems , with potential applications of the technique in other cancers , including breast cancer and melanoma . breast cancer , like uterine cancer , has highly predictable lymphatic drainage . 
 consequently , preoperative lymphatic mapping with radiocolloid and dynamic imaging ( eg , lympho scintigraphy or single photon emission ctct [ spect / ct ] ) to establish site of incision is unnecessary for lymphatic mapping in breast cancer . 
for example , a direct comparison showed that indo cyanine green detected a sentinel node in 97100% of patients with breast cancer whereas blue dyes detected a sentinel node in 8889%.22 , 23 additionally , indocyanine green detects more sentinel nodes per patient than does blue dye . 
when compared with radiocolloid , indocyanine green does not appear to detect more sentinel nodes overall but might detect more metastatic sentinel nodes.24 for melanoma , interest in indocyanine green as an alternative to radiocolloid for lymphatic mapping and sentinel node biopsy has been somewhat more tempered . 
lymphatic drainage of melanoma can often be 1400 vol 19 october 2018 articles ambiguous , especially for lesions located on the trunk , head , or neck.25 preoperative lymphatic mapping with dynamic imaging ( lymphoscintigraphy or spect / ct ) is often necessary to identify draining nodal basins and to determine sites for surgical incision and exploration . 
 the penetrance of near - infrared cameras to detect sentinel nodes through the skin is only 23 mm , so the use of indocyanine green as a substitute for radiocolloid is largely ineffective , especially for lesions located in anatomical areas with ambiguous drainage.26 lymphatic mapping and sentinel node biopsy is an image - guided , precision surgical procedure that is increasingly being adopted for the surgical staging of apparent cervical - confined and uterine - confined malignancies . 
as use of indocyanine green for lymphatic mapping in cervical and uterine malignancies becomes more routine , we should also be aware of the potential pitfalls of this new exciting technology . 
this result is likely due to the bright green effect of the imaging with a laser - based near - infrared syste occasionally , dilated lymphatic channels can lead to a very bright signal that leads to the channels being mistaken for nodes and excised . 
mistaken excision of lymphatic trunks or adipose tissue instead of a node is potentially a major pitfall as sentinel node biopsy without complete lymphadenectomy becomes more common ; failure to excise a true node could leave the disease status of an entire hemipelvis unknown . 
if the surgeon has any doubt , it is reasonable to send the presumed nodal tissue for an confirm nodal content . intraoperative pathological consultation a second major potential pitfall of lymphatic mapping and sentinel node biopsy for cervical and uterine malignancies is the removal of multiple bright green nodes that appear to be true sentinel nodes but are in fact second - echelon and third - echelon nodes . 
this pitfall also relates to the bright signal from a laser - based , nearinfrared imaging platfor unlike isosulfan blue dye , which rarely can be seen beyond the first or true sentinel node to secondary - echelon nodes , indocyanine green often produces bright green signal in not only the true sentinel node but also secondary , tertiary , and more distant nodal basins . 
further , the enhanced pathology protocol evaluation should be limited to the true sentinel nodes , which in most studies average about three per patient with uterine malignancy . although the initial capital expenditures needed to incorporate the use of indocyanine green and near - infrared imaging for lymphatic mapping in patients with cervical and uterine cancers might be prohibitively high for some institutions , the near - infrared imaging system could also be used for other purposes , such as evaluating perfusion of bowel or oesophageal anastomoses or delineating anatomy during cholecystectomy.2729 moreover , the alternative to this approach is to continue to use the combination of blue dye and radiocolloid in these patients ( since we have shown that blue dye alone for lymphatic mapping is suboptimal )  . 
although blue dye is quite inexpensive , the use of radiocolloid is not , because its administration requires additional nuclear medicine technicians , nurses , and physicians , and the use of nuclear medicine facilities . 
finally , incorporation of sentinel lymph node biopsy with indocyanine green and near - infrared imaging might be the most cost - effective approach in treating women with gynaecological cancers when compared with complete lymphadenectomy in all patients or lymphatic mapping and sentinel node biopsy with radiocolloid or blue dye.30 this study is limited in its inability to determine the sensitivity , negative predictive value , and oncological outcomes for lymphatic mapping and sentinel node biopsy in women with cervical and uterine cancers . 
 the protocol was designed only to compare indocyanine green and isosulfan blue dye as mapping substances in these patients , and not as a trial to determine the validity the sentinel node concept . 
however , although the combination of blue dye and radiocolloid might have improved detection rates in the standard group , on the basis of the literature , 31 we believe the retrospective data indocyanine green would still be superior in detecting sentinel nodes in women with cervical and uterine cancers . 
surgeons who are new to lymphatic mapping and sentinel lymph node biopsy should perform the procedure followed by complete lymphadenectomy until they are confident that they have achieved proficiency in accurately detecting sentinel nodes . 
finally , as mentioned , the results can only be assumed valid for the specific compound ( ic2000 ) and near - infrared system ( pinpoint ) used in the study . 
however , we believe that studies using other formulations of indocyanine green and other nearinfrared imaging systems will probably yield similar results to our study . the us food and drug administration indications for indocyanine green include only intravenous injection to determine cardiac output , to evaluate perfusion of solid vol 19 october 2018 1401 articles organs , and to perform ophthalmic angiography . 
the manufacturer of ic2000 indocyanine green dye has submitted an application to the food and drug administration on the basis of the results from this study for on - label use of interstitial injection of indocyanine green combined with near - infrared imaging for lymphatic mapping . 
 for women with cervical and uterine cancers , increasing evidence suggests that lymphatic mapping and sentinel node biopsy not only improves detection of disease in regional nodes but also decreases operative morbidity.32 , 33 as lymphatic mapping and sentinel node biopsy become the standard of care in the surgical treatment of cervical and uterine cancers , improving sentinel node detection , particularly detection of bilateral sentinel nodes , will become the focus of research . 
as shown in this study , the incorporation of indocyanine green cervical injection and near - infrared imaging into the mapping improvement over procedure could represent an existing approaches ( ie , blue dye , radiocolloid , or both ) and might in the future become a standard method in these and other solid tumours . contributors mf and nra - r participated in study conception and design , acquisition of data , analysis and interpretation of data , drafting of the report , and critical revision . 
dlu participated in study conception and design , analysis and interpretation of data , and critical revision of the report . declaration of interests mf reports grants from novadaq / stryker , during the conduct of the study , and personal fees from novadaq / stryker , grants from navidea , personal fees from johnson and johnson , and personal fees from genentech , outside the submitted work . 
the other authors declare no competing interests . acknowledgments mf and dlu are supported by the national institutes of health / national cancer institute under award number p30ca016672 . published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections correction to lancet oncol 2018 ; 19 : 95364 correction to lancet oncol 2018 ; 19 : 104050 correction to lancet oncol 2018 ; 19 : e386 kramer souweidane mm , pandit - taskar n , et al . 
this correction has been made to the printed article , and to the online version as of aug 1 , 2018 . moreau p , mateos m - v , berenson jr , et al . 
lancet oncol 2018 ; 19 : 95364in the methods section of this article , the exclusion criteria for new york heart association heart failure should have been class iii or iv . 
this correction has been made to the online version as of aug 1 , 2018 . vol 19 aug 2018 e382 corrections particularly if chemotherapy - free interventions prove successful.9 indeed , huet and colleagues show that the prognostic effect of the previously defined expression signatures of immune response 1 and 210 was lost in the prima study cohort , demonstrating how the fortunes of these predictors can fluctuate with changes in treatment , even if a role for genes linked to the tumour microenvironment was maintained . as the potency of these scoring systems continues to improve , it is essential to develop the multicentre collaborations necessary to further validate , standardise , comparisons between and enable head - to - head these different predictors . 
the wider community of follicular lymphoma oncologists must decide which models to prioritise for either validation or adoption in clinical trials , and it is imperative that a consensus is reached on the level of discrimination needed to guide treatment , especially for an indolent disease such as follicular lymphoma where a high prognostic accuracy is necessary . 
the expected refinements might well involve increasingly complex dynamic models with imaging and cell - free dna , but it is equally important that risk models do not become unnecessarily unwieldy and impractical for routine application . this new prognostic tool is an important step towards the goal of personalised care for patients with follicular lymphoma . 
there is now a pressing need to not only validate and compare emerging prognostic tools in prospective clinical trials but to consider the robustness and feasibility of these analyses in the real - world setting . shamzah araf , jessica okosun , * jude fitzgibbon centre for haemato - oncology , barts cancer institute , london ec1m 6bq , uk j.fitzgibbon@qmul.ac.uk jf declares grants from epizyme and personal fees from roche , gilead , janssen , and epizyme , outside the submitted work . 
early relapse of follicular lymphoma after rituximab plus cyclophosphamide , doxorubicin , vincristine , and prednisone defines patients at high risk for death : an analysis from the national lymphocare study . 
integration of gene mutations in risk prognostication for patients receiving first - line immunochemotherapy for follicular lymphoma : a retrospective analysis of a prospective clinical trial and validation in a population - based registry . 
 n engl j med 2004 ; 351 : 215969 . adjuvant therapy in colon cancer : less is more the results of the scot trial reported by timothy iveson and colleagues1 in the lancet oncology establish a new standard of care in the adjuvant treatment of stage iii colon cancer . 
the investigators showed the non - inferiority of treatment with 3 months of adjuvant chemotherapy versus 6 months of the same treatment in terms of 3 year disease - free survival . 
 patients treated with the shorter duration of therapy had significant reductions in adverse events , including a more than halving in the number of grade 2 or worse sensory neuropathy events . 
these results were robust in patients with low - risk stage iii ( t3 or n1 ) disease who received 3 months of capecitabine and oxaliplat however , the non - inferiority of 3 months of therapy versus 6 months could not be shown in higher risk t4 or n2 disease . 
like scot , see articles page 562 442 vol 19 april 2018 comment non - inferiority could not be shown for the shorter duration of therapy with capecitabine and oxaliplatin in the higher risk patients . 
 therapies what are the implications for changing practice to 3 months of adjuvant chemotherapy ? a shorter duration of adjuvant therapy could permit the earlier introduction of to be investigational used sequentially or combined with chemotherapy , particularly in higher risk patients . 
furthermore , it will be necessary to await the impact of findings from correlative studies done in scot and the other idea trials , given the now recognised prognostic importance of factors such as tumour sidedness , microsatellite instability , and braf or ras mutation . less might also be more in oesophageal and gastric cancers . 
in anal cancer treated with definitive chemoradiotherapy , the addition of extra cycles of chemotherapy either before or after chemoradiotherapy has been shown not to improve survival compared with chemoradiotherapy alone.6 , 7 an argument for less chemotherapy is also seen in results from trials investigating neoadjuvant or preoperative therapy in a randomised trial8 of oesophageal and gastro - oesophageal junction cancers reported by ajani and colleagues , the addition of 2 months of fluorouracil and oxaliplatin before preoperative fluorouracil plus oxaliplatin and radiotherapy did not improve survival compared with chemotherapy given only during radiotherapy . 
in the oeo5 trial , 9 which enrolled patients with oesophageal and gastro - oesophageal junction adenocarcinoma , alderson and colleagues also reported no survival benefit with four cycles of the ecx regimen ( epirubicin , cisplatin , and capecitabine ) beyond that achieved with two cycles of fluorouracil and cisplat these results support the use of a shorter duration of preoperative chemotherapy as well as the discontinuation of the use of epirubic al - batran and colleagues have reported that the addition of docetaxel to infused fluorouracil and oxaliplatin , using the flot regimen ( fluorouracil , leucovorin , oxaliplatin , and docetaxel ) as preoperative therapy , resulted in a significant survival benefit compared with preoperative ecx in patients with gastric and gastro - oesophageal junction cancers.10 if a third chemotherapy agent is to be added to preoperative fluorinated pyrimidine platinum chemotherapy , it should be docetaxel and not epirubicin . the scot investigators deserve congratulations for their practice - changing trial that can directly improve the lives of patients receiving adjuvant chemotherapy for stage iii colon cancer . 
 david h ilson gi oncology service , memorial sloan kettering cancer center , new york , ny 10011 , usa ilsond@mskcc.org i declare no competing interests . copyright the author ( s )  . 
3 versus 6 months of adjuvant oxaliplatin - fluoropyrimidine combination therapy for colorectal cancer ( scot ) : an international , randomised , phase 3 , non - inferiority trial . 
prospective pooled analysis of six phase iii trials investigating duration of adjuvant ( adjuv ) oxaliplatin - based therapy ( 3 vs 6 months ) for patients ( pts ) with stage iii colon cancer ( cc ) : the idea ( international duration evaluation of adjuvant chemotherapy ) collaboration . 
three versus six months adjuvant oxaliplatin - based chemotherapy for patients with stage iii colon cancer : the french participation to the international duration evaluation of adjuvant chemotherapy ( idea ) project . 
perioperative chemotherapy with docetaxel , oxaliplatin , and fluorouracil / leucovorin ( flot ) versus epirubicin , cisplatin , and fluorouracil or capecitabine ( ecf / ecx ) for resectable gastric or gastroesophageal junction ( gej ) adenocarcinoma ( flot4 - aio ) : a multicenter , randomized phase 3 trial . 
we assessed the effects of postmastectomy radiotherapy on quality of life ( qol ) in women with intermediate - risk breast cancer . methods supremo is an open - label , international , parallel - group , randomised , controlled trial . 
women aged 18 years or older with intermediate - risk breast cancer ( defined as pt12n1 ; pt3n0 ; or pt2n0 if also grade iii or with lymphovascular invasion ) who had undergone mastectomy and , if node positive , axillary surgery , were randomly assigned ( 1 : 1 ) to receive chest wall radiotherapy ( 50 gy in 25 fractions or a radiobiologically equivalent dose of 45 gy in 20 fractions or 40 gy in 15 fractions ) or no radiotherapy . 
the qol substudy , open to all uk patients , consists of questionnaires ( european organisation for research and treatment of cancer qlq - c30 and qlq - br23 , body image scale , hospital anxiety and depression scale [ hads ] , and eq - 5d - 3l ) completed before randomisation , and at 1 , 2 , 5 , and 10 years . 
the prespecified primary outcomes within this qol substudy were global qol , fatigue , physical function , chest wall symptoms , shoulder and arm symptoms , body image , and anxiety and depression . 
this trial is registered with the isrctn registry , number isrctn61145589 . findings between aug 4 , 2006 , and april 29 , 2013 , 1688 patients were enrolled internationally and randomly assigned to receive chest wall radiotherapy ( n = 853 ) or not ( n = 835 )  . 
989 ( 79% ) of 1258 patients from 111 uk centres consented to participate in the qol substudy ( 487 in the radiotherapy group and 502 in the no radiotherapy group ) , of whom 947 ( 96% ) returned the baseline questionnaires and were included in the analysis ( radiotherapy , n = 471 ; no radiotherapy , n = 476 )  . 
at up to 2 years , chest wall symptoms were worse in the radiotherapy group than in the no radiotherapy group ( mean score 141 [ sd 158 ] in the radiotherapy group vs 116 [ 146 ] in the no radiotherapy group ; effect estimate 217 , 95% ci 040394 ; p = 0016 ) ; however , there was an improvement in both groups between years 1 and 2 ( visit effect 134 , 95% ci 236 to 031 ; p = 0010 )  . 
the results of some trials investigating selective omission of radio therapy or chemotherapy have recently been reported.2 , 3 although the effects of mastectomy and chemotherapy on quality of life ( qol ) have been well documented , the additional effect of adjuvant radio therapy following mastectomy is unclear . 
chest wall pain , fatigue , anxiety about recurrence , and depressive symptoms can all hold back recovery and return to normal activities of daily living.4 adjuvant chest wall irradiation after mastectomy remains a core and highly effective component of the locoregional management of early breast cancer , reducing locoregional recurrence and breast cancer for the mortality . 
we did not identify any meta - analyses or randomised phase 3 trials comparing qol in patients with breast cancer treated by mastectomy and systemic therapy , with or without adjuvant postoperative chest wall radiotherapy . 
a few studies have investigated patient - reported outcomes , such as symptoms and qol , but most patients in these studies had breast - conserving surgery rather than mastectomy , and none of the studies involved a comparator group randomly assigned to no radiotherapy . added value of this study this substudy of the phase 3 supremo trial investigated the effect of adjuvant postmastectomy radiotherapy on qol in a randomised trial in a large , well characterised population of uk patients with intermediate - risk ( one to three positive lymph nodes ) breast cancer . 
at 2 years , postmastectomy radiotherapy was associated with worse self - reported local chest wall symptoms ( pain , swelling , and skin problems in the area of the affected breast ) compared with no radiotherapy , but the difference between groups was small , unlikely to be of clinical significance , and symptoms improved over time . 
there were no differences between groups in arm and shoulder symptoms , body image , fatigue , overall qol , physical function , or anxiety or depression , or in the secondary qol outcomes of pain , role functioning , social functioning , sexual functioning , and nausea or vomiting . implications of all the available evidence the effect of postmastectomy radiotherapy on 10 - year survival , the primary endpoint of the main supremo trial , in patients with intermediate - risk breast cancer will not be known before 2023 . 
in the meantime , both options of administering or omitting postmastectomy radiotherapy seem to be legitimate in terms of their effects on qol for patients with intermediate - risk disease . 
our data will inform shared decision making ( as recommended in the recent us guidelines on postmastectomy radiotherapy ) and put patients in a better position to make an informed value judgment on what they consider relevant for their situation regarding the data on patient - reported symptoms and qol domains presented in this report . 
both physicians and patients could be helped when weighing up the individual estimates of possible benefits of postmastectomy radiotherapy against its effects on toxicity and qol . more involved axillary nodes is robust , its role in intermediaterisk patients with one to three involved nodes is controversial and practice and guidelines vary.5 results from a metaanalysis in 2014 showed an advantage in overall survival from post mastectomy radiotherapy that included at least the chest wall in the target volume in patients with either one to three positive nodes or four or more positive nodes.6 however , the trials with different generalisability of historical standards of surgery , radiotherapy , and systemic therapy remains uncertain , especially because contem porary survival rates are much higher than those in the studies included in the 2014 metaanalysis . 
potential benefits in survival need to be balanced against the risk of locoregional and cardiopulmonary toxicity , especially when radiotherapy is given in conjunction with poten tially cardiotoxic anthracyclines and trastu zumab . 
the primary and secondary endpoints of the trial have been described previously.9 substudies include transsupremo , which seeks molecular markers of radiosensitivity , a cardiac substudy , andfor uk patients onlyqol and health economics assessments . 
 these substudies will provide an important highquality evidence base about the balance of potential benefits and treatment burden , to support patients and healthcare professionals during shared decision making . the longterm effect of breast cancer and its treatment on everyday life has been identified as a crucial knowledge gap and a key priority for breast cancer research.10 for radiotherapy , little information about treatment impact is available . 
a few trials have investigated selfreported breast , arm , and shoulder symptoms , functional out comes , and qol after radiotherapy , mainly in patients receiving breastconserving therapy.1113 patients usually report transient and shortterm effects of radio therapy , with fairly limited effects on their overall qol.14 , 15 vol 19 november 2018 1517 articles for the trial protocol see supremo%20protocol%20 version29.pdf no comprehensive qol data exist in patients having postmastectomy radiotherapy , and only a few studies have compared patientreported outcomes following breastconserving surgery versus mastectomy with and without reconstruction . 
briefly , eligible patients were women aged 18 years or older who had undergone mastectomy for unilateral breast cancer and , if they had intermediate risk breast cancer , an axillary staging procedure with axillary lymph node dissection . 
patients were eligible if they had intermediaterisk breast cancer ( defined as pt12n1 ; pt3n0 ; or pt2n0 if also grade iii or with lymphovascular invasion on histology )  . 
 exclusion criteria included previous or concurrent malignancy ( apart from nonmelanomatous skin cancer and carcinoma in situ of the cervix ) , ductal carcinoma in situ , bilateral breast cancer , pregnancy at the time of radiotherapy treatment , and male sex . the study was approved by the multicentre research ethics committee , edinburgh ( mrec 05 / 50501 / 106 ) and local research and development offices . 
patients provided written , informed consent before enrolment and had additional options to consent to the substudies , including the qol substudy . randomisation and masking patients were randomly assigned ( 1 : 1 ) postoperatively to either chest wall radiotherapy or no chest wall radiotherapy . 
randomisation was done by permuted blocks , with block length varied randomly to minimise the effect of entry bias , and stratified by treatment centre because of possible betweencentre differences in radiotherapy procedures . 
in 2011 , the eligibility criteria were widened , following a protocol amendment ( version 29 ; aug 30 , 2010 ) approved by the ethics committee , to include the use of neoadjuvant chemotherapy , according to contemporary guidelines . for patients randomly assigned to receive chest wall radiotherapy , radiotherapy was given after chemotherapy ( if administered )  . 
surgery , systemic therapy , and pathology were also subject to prespecified quality assurance . additional recorded data included cardiovascular risk factors , radiotherapy cardiac and lung exposure par ameters , systemic therapy ( type , doses , and dates ) , and any reconstructive surgery ( type , and immediate or delayed )  . 
 patients with gross protocol violations ( eg , margins involved or less than 1 mm margins for invasive cancer or ductal carcinoma in situ ) were to be removed before the final analysis of the main trial . 
serious adverse events were to be reported if they occurred during radiotherapy or within 30 days of the last radiotherapy session ( fraction ) , irrespective of whether or not they were related to the randomly assigned treatment . 
any toxicity assessed as a grade 4 or 5 acute or late morbidity score had to be reported on a serious adverse event or suspected unexpected serious adverse reaction form for the entire followup period of the trial . 
 monitoring ( source data verification ) is being done by the cancer clinical trials team in edinburgh ( edinburgh , uk ) on 10% of the patient data from the main trial , with site visits allowed in the uk . 
higher levels of monitoring by the cancer clinical trials team will be done , if requested by the data monitoring committee , or if specific safety issues ( see protocol ) are identified by the investigators or the trial management group of the trial steering committee . 1518 vol 19 november 2018 articles all patients eligible for supremo from uk centres were invited to participate in the qol substudy . 
if the baseline questionnaire was not returned to the trials office , further questionnaires could not be sent , because the patients name and address were not available to the trial coordinator . 
the european organisation for research and treatment of cancer ( eortc ) qlqc30 ( version 3.0 ) consists of 30 questions addressing five functional scales ( cognitive , emotional , physical , social , and role ) , nine symptom scales ( appetite loss , constipation , diarrhoea , dyspnoea , fatigue , financial difficulties , insomnia , nausea and vomiting , and pain ) , and one global health status qol scale.18 the eortc qlqbr23 ( version 1.0 ) focuses on breast cancerspecific issues and includes 23 questions addressing four functional scales ( body image , future perspective , sexual enjoyment , and sexual functioning ) and four symptom scales ( arm symptoms [ swelling in arm or hand , arm or shoulder pain , and difficulty raising the arm ] , breast or chest wall symptoms [ pain , swelling , oversensitivity , and skin problems in the area of the affected breast ] , systemic therapy sideeffects , and being upset by hair loss ) .19 all scores for the eortc qlqc30 and eortc qlqbr23 were transformed to a scale from 0 to 100 . 
higher scores on the functional scales and global qol scale represent a superior level of functioning and better qol , whereas higher scores in the symptom scales or items represent worse symptoms . the body image scale ( bis ) is a tenitem scale designed specifically for use with cancer patients to assess aspects of attractiveness , sexual attractiveness , and feelings or satisfaction with appearance . 
scores for each scale were graded from 0 to 3 and summed to produce a single score , with a higher score indicating more body image problems ( score range from 0 to 30 ) .20 the hospital anxiety and depression scale ( hads ) is a 14item instrument with two subscales for anxiety and depression.21 scores range from 0 to 21 on each scale , with higher scores indicating more distress . 
a combined score of 19 or higher is considered to be indicative of psychological distress . the eq5d3l questionnaire measures health status across five domains ( mobility , selfcare , usual activities , pain and discomfort , and anxiety and depression )  . 
these eq5d3l health status descriptions are converted into a single summary index ( range from 0 to 1 ) by attaching a value to each of the levels in each dimension . 
according to standard practice , these values were obtained from a large uk population study using a choicebased method of valuation.22 the resulting summary score , or utility value , can then be used directly in a costutility analysis . outcomes the primary endpoint of the supremo trial is 10year overall survival . 
qol is a secondary endpoint alongside chest wall recurrence , regional recurrence , diseasefree survival , acute and late morbidity , costeffectiveness , metastasisfree survival , and cause of death . 
in this qol substudy , we prespecified as primary outcomes global qol ; fatigue ; physical function ; chest wall symptoms ; shoulder and arm symptoms ; body image ; and anxiety and depression . 
secondary outcomes are role , social , and sexual functioning , and pain , nausea , and vomiting . 1688 patients enrolled in supremo trial 853 randomly assigned to radiotherapy group 835 randomly assigned to no radiotherapy group 632 from uk sites 626 from uk sites 145 declined to participate in qol substudy 124 declined to participate in qol substudy 487 ( 77% ) of 632 agreed to participate in qol substudy 502 ( 80% ) of 626 agreed to participate in qol substudy 16 did not complete baseline questionnaire 26 did not complete baseline questionnaire 471 ( 97% ) of 487 completed baseline questionnaire * 476 ( 95% ) of 502 completed baseline questionnaire * 4 died 10 died 388 ( 83% ) of 467 completed year 1 questionnaire 388 ( 83% ) of 466 completed year 1 questionnaire 10 died 3 died 367 ( 80% ) of 457 completed year 2 questionnaire 350 ( 76% ) of 463 completed year 2 questionnaire figure 1 : trial profile of patients participating in the qol substudy qol = quality of life . 
with 200 evaluable patients per group , the proportion of patients with a particular sideeffect or specified degree of morbidity in a qol domain could be estimated with a standard error of 35% or less . 
however , because there is usually substantial attrition over time in qol studies , to have sufficient numbers by 10 years , a target of 800 patients taking part in the qol substudy was set . 
the total sample size of supremo was reduced during the trial , following a protocol amendment approved by the ethics committee , from 3500 to 1600 , but this did not affect the qol substudy sample size . when calculating qol questionnaire or subscale scores , we followed official questionnaire guidelines on handling missing individual items . 
in general , if more than 50% of items were missing , subscale scores ware not calculated ( missing ) ; if less than 50% of items were missing , those were replaced by the mean of the answered items and a score was calculated . 
if no guidance existed , that score was recor ded as missing . to maintain the normality of the residuals , the difference from baseline to each subsequent question naire was calculated for each scale . 
however , as the comparison of radiotherapy versus no radiotherapy is the primary objective of this trial , we will discuss those comparisons if the results have a p value of 005 or lower . 
 because of the large number of models , clinical variables will only be discussed if they exceed the more conservative threshold of p < 001 . the principal analysis modelled the change in score in the prespecified qol primary outcomes ( global qol , fatigue , physical function , chest wall symptoms , shoulder and arm symptoms , body image , and anxiety and depression ) by time ( visit 1 at 12 months or visit 2 at 24 months ) of followup , age group ( < 45 , 4554 , 5569 , 70 years ) , baseline score , and treatment ( with or without radiotherapy )  . because almost all patients received some form of systemic therapy and some underwent breast recon structive surgery , secondary exploratory analyses were done to assess whether or not these treatments affected the qol outcome measures . 
the secondary analysis included a prespecified exploratory analysis of clinical 1520 vol 19 november 2018 articles covariates also considered to have an effect on qol ( extent of axillary surgery , early breast reconstruction , adjuvant chemotherapy , adjuvant hormonal therapy , and use of trastuzumab )  . 
this analysis was done by creating a basic model of age group , time , and baseline score , then adding the clinical variables in turn to create a model of best fit . 
only patients with complete data for all clinical variables were included in this modelling . published data are available for eortc qlqc30 on change scores within groups or scores difference between groups that are clinically significant , but to the best of our knowledge , no such data are available for eortcbr23 scores.23 we opted to present mean scores and sds to allow comparisons with other studies . 
to attempt to explore the clinical significance of any observed statistically significant differences in eortcbr23 scores , we used a generic approach of 05 of the sd to indicate minimally important difference.24 recent guidelines from the us food and drug administration recom mend establishing a meaningful change in patientreported outcome measures at the individual level ( ie , defining a responder ) versus at the treatment group level , 25 with the definition of a responder being a score change in a measure , experienced by an individual patient over a predetermined time period that has been demonstrated in the target population to have a significant treatment benefit . 
26 we calculated proportions of patients whose scores improved ( change score < 05 sd ) between baseline and year 1 , those who remained stable or had no change ( change score 05 sd to + 05 sd ) , and those whose scores worsened ( change score > 05 sd )  . all analyses were done by intention to treat . 
 * only recorded in protocol version 29 ( aug 30 , 2010 ) onwards ; the denominator is the total number of recorded chemotherapy treatments from protocol version 29 onwards ( qol study : radiotherapy , n = 173 ; no radiotherapy , n = 173 ; full trial : radiotherapy , n = 269 ; no radiotherapy , n = 243 )  . 
denominator is the number of recorded answers ( qol study : radiotherapy , n = 460 ; no radiotherapy , n = 454 ; full trial : radiotherapy , n = 806 ; no radiotherapy , n = 782 )  . 
denominator is the total number of recorded neoadjuvant endocrine therapy treatments from protocol version 29 ( aug 30 , 2010 ) onwards ( qol study : radiotherapy , n = 206 ; no radiotherapy , n = 200 ; full trial : radiotherapy , n = 316 ; no radiotherapy , n = 288 )  . 
denominator is number of patients who received adjuvant endocrine therapy . table 1 : patient demographics and clinical characteristics role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author and joint senior authors had full access to all data in the study and had final responsibility for the decision to submit for publication . results between aug 4 , 2006 , and april 29 , 2013 , the trial recruited 1688 patients internationally from 27 eortc centres in nine european countries ( belgium , france , germany , ireland , the netherlands , poland , spain , switzerland , and turkey )  . 
in total , 989 ( 79% ) uk patients consented to participate , of whom 947 ( 96% ) returned the baseline questionnaires ( 471 [ 97% ] of 487 patients in the radio therapy group and 476 [ 95% ] of 502 in the no radiotherapy group )  . 
patients from the uk who declined participation or did not return the baseline questionnaires ( n = 311 ) were older ( mean age vol 19 november 2018 1521 articles 577 years [ sd 119 ] ) than those who consented and returned the baseline questionnaires ( n = 947 ; mean age 561 years [ sd 110 ] )  . 
mean age did not differ between participants in the qol substudy and the remaining 741 participants in the main trial ( ie , uk patients not participating in the substudy and all patients from other countries ; mean age 556 years [ sd 116 ] )  . 
to check further for potential bias in patient selection for the qol substudy , we compared the clinical char acteristics of patients completing the substudy with those of patients in the main trial and found no differences ( table 1 )  . good patient compliance was achieved with the com pletion of qol measures , with slightly better com pliance seen in the radiotherapy group than in the no radiotherapy group at baseline and year 2 ( figure 1 )  . 
eq - 5d - 3l score , range 01 . 074 ( 022 ) 075 ( 024 ) 075 ( 025 ) 1522 vol 19 november 2018 articles clinical characteristics were well balanced between the radiotherapy and no radiotherapy groups ( table 1 )  . 
 a further review of the type of breast reconstruction suggested more frequent autologous reconstructions in the radiotherapy group , whereas there were more recon structions with an implant or expander in the no radio therapy group ( appendix p 2 )  . 
 similar propor tions of patients in the two groups received adjuvant chemotherapy , trastuzumab , and endocrine therapy ( table 1 )  . most patients in the radiotherapy group of the qol substudy received 40 gy radiotherapy in 15 fractions ( 327 [ 68% ] of 478 patients ; seven patients did not receive radiotherapy as per protocol but their participation in the qol study is not known ) , with the remaining patients equally divided between 50 gy in 25 fractions ( 52 [ 11% ] ) , 45 gy in 20 fractions ( 48 [ 10% ] ) , and other or unknown ( 51 [ 11% ] )  . 
in the main trial , 445 ( 52% ) of 853 patients in the radiotherapy group received 40 gy in 15 fractions , 227 ( 27% ) received 50 gy in 25 fractions , 57 ( 7% ) received 45 gy in 20 fractions , and 124 ( 15% ) had other or unknown . 
at baseline , patients reported relative impairment in global qol , with mean scores of 604 and 609 ( 100 on the scale is excellent ) , relative impair ment of role ( mean 630 and 652 ) and social function ( 640 and 655 ) , a high level of fatigue ( mean of 430 and 416 ; 100 is greatest degree of fatigue ) , insomnia ( mean 372 and 362 ; 100 is the worst level of insomnia ) , and a degree of arm symptoms ( mean 212 and 203 ) , chest wall symptoms ( 181 and 173 ) , and pain ( 248 and 226 ; a score of 100 would be the worst symptoms ; table 2 )  . table 3 shows the results from mixedeffects model analysis of the prespecified primary qol outcomes and pain ( a prespecified secondary qol outcome ; data for other prespecified secondary qol outcomes not shown )  . 
such effects were adjuvant chemotherapy and immediate breast recon struction ( table 3 ) , but not extent of axillary surgery , adjuvant endo crine therapy , or trastuzumab ( appendix pp 34 )  . up to 2 years , chest wall symptoms were worse in the radiotherapy group than in the no radiotherapy group ( estimate of effect 217 , 95% ci 040 to 394 ; p = 0016 ; table 3 )  . 
there was an improvement in chest wall symptoms between years 1 and 2 in both groups ( visit effect 134 , 95% ci 236 to 031 ; p = 0010 ) , but the improvement was smaller in the radiotherapy group than in the no radiotherapy group ( table 3 )  . 
to explore the clinical the observed statistically significant significance of difference between the groups for chest wall symptoms , we calculated the sd of the change score for chest wall symptoms from baseline to year 1 in the no radiotherapy group . 
in a responder analysis , we calcu lated proportions of patients whose scores improved ( change score < 865 points ) between baseline and year 1 , those who remained stable or had no change ( change score 865 to 865 ) , and those whose scores worsened ( change score > 865 points )  . 
62 ( 16% ) of 386 patients in the radiotherapy group reported clinically meaningful worse change score ( ie , change score > 865 ) compared with 46 ( 12% ) of 385 patients in the no radiotherapy group ( appendix pp 78 )  . arm and shoulder symptoms did not differ signifi cantly according to treatment ( table 3 , figure 2b )  . 
 however , chemotherapy had an effect , with patients receiving chemotherapy showing less improve ment in arm symptoms over time ( figure 2b , table 3 ) , suggesting that chemotherapy and age were confoun ding variables affecting arm and shoulder symptoms . 
significantly more patients in the younger age groups received chemotherapy than did patients in the older age group ( 130 [ 97% ] of 134 patients aged < 45 years , 318 [ 96% ] of 332 patients aged 4554 years , 305 [ 84% ] of 362 patients aged 5569 years , and 43 [ 36% ] of 119 patients aged 70 years ; p < 00001 for test )  . 
the extent of axillary surgery ( comparison of sentinel node biopsy or node sampling vs sentinel node biopsy plus axillary node clearance vs axillary node clearance ) did not affect arm or shoulder symptom scores ( appendix pp 34 )  . 
furthermore , the extent of axillary surgery did not have an effect on any of the prespecified qol variables , apart from higher hads anxiety scores in patients with sentinel node biopsy plus axillary node clearance ( p = 001 ; appendix pp 34 )  . despite the observed differences in chest wall symptoms , image problems , with patients reported few body improvement in body image scale scores in both treatment groups between years 1 and 2 ( tables 2 , 3 )  . 
some age effect was observed , with patients younger than 45 years reporting more concerns about their body image compared with patients aged 70 years or older ( estimate of effect 196 , 95% ci 053339 ; p = 00074 ; table 3 )  . 
furthermore , improvement in global qol was seen in both groups between baseline and year 1 , with further but smaller improvement by year 2 ( figure 2c )  . 
as expected , there was an age effect 1524 vol 19 november 2018 articles with patients younger than 69 years reporting better overall physical functioning than patients aged 70 years or older ( table 3 )  . patients reported high baseline levels of fatigue , probably because of the preceding surgery . 
women younger than 70 years of age reported higher levels of anxiety ( table 3 ) , with improvement from baseline to year 1 and to year 2 in both groups ( table 3 )  . 
 the mean baseline score for selfreporting of general pain was just over 20 in both groups , but without any improvement from baseline to year 1 or year 2 independent of randomisation group ( tables 2 , 3 )  . 
no effect was found for trastuzumab , chemotherapy , or endocrine therapy ( none vs tamoxifen vs aromatase inhibitors ; data not shown )  . no betweengroup differences were noted for nausea or vomiting , or for sexual , role , and social functions at any timepoint ( table 2 )  . 
we had a good completion rate for the general sexual function questions ( 914 [ 97% ] of 947 ) , but only 253 ( 28% ) of 914 patients completed the conditional sexual enjoyment questions at baseline ( table 2 )  . 
all remaining scales and items did not show any effect of radiotherapy treatment and all showed improvement or stability over time . discussion the main finding of this qol substudy of the supremo trial is that postmastectomy radio therapy was associated with worse selfreported chest wall symptoms ( pain , swelling , oversensitivity , and skin problems in the area of the affected breast ) than no radiotherapy , although these symptoms improved over time . 
the estimated effect is small , with a difference in change scores between the radiotherapy and no radiotherapy groups of 217 points ( 95% ci 040394 ; p = 0016 )  . 
our responder analysis showed that 4% more patients assigned to radiotherapy reported a likely clinically meaningful worsening of their chest wall symptoms than did those in the no radio therapy group . 
the adjusted mean for the individual groups is the mean of the change scores ( defined as change from baseline to year 1 and from baseline to year 2 in each of the treatment groups , adjusted for baseline score , visit , and age )  . 
p values indicate whether each of the means of the change scores within each individual group is significantly different from zero ( ie , improvement or deterioration in scores from baseline )  . 
 table 3 : mixed - effects models ( fixed effects ) for qol outcomes note of caution is appropriate because of the assumptions made in the calculations ( ie , the assumption that an sd of the change score of 865 is likely to indicate a clinically meaningful difference )  . to the best of our knowledge , this is the first study to investigate the effect of adjuvant radiotherapy on qol in a large randomised trial in patients treated by mastectomy for intermediaterisk breast cancer ( including patients undergoing breast reconstruction )  . 
our results show that radiotherapy to the chest wall did not affect arm or shoulder symptoms ( axillary radiotherapy was prohibited in the trial ) , body image , global qol , physical function , fatigue , or symptoms of anxiety or depression . 
in supremo , about a quarter of patients ( those with pn0 [ sn ] tumours ) in the main trial and qol substudy underwent limited axillary surgery ( sentinel node biopsy or nodal sampling )  . 
 this is perhaps an unexpected finding and could be caused by lack of sensitivity of the eortc qlqbr23 scale ( which has three items on pain in arm or shoulder , swollen arm or hand , and difficulty raising your arm )  . 
therefore , our findings are not generalisable to women treated with both an axillary vol 19 november 2018 1525 articles a chest wall symptoms b arm and shoulder symptoms radiotherapy , no chemotherapy radiotherapy , chemotherapy no radiotherapy , no chemotherapy no radiotherapy , chemotherapy c global quality of life no radiotherapy radiotherapy d physical function 05 15 20 25 e fatigue no radiotherapy , no reconstruction radiotherapy , no reconstruction no radiotherapy , reconstruction radiotherapy , reconstruction time since treatment ( years ) time since treatment ( years ) figure 2 : change in qol scores from baseline to years 1 and 2 ( a ) chest wall symptoms . 
global qol ( c ) and functional scores ( d ) range from 0 to 100 with higher score indicating good functioning ; therefore , positive change score indicates improvement . 
this treatment is generally reserved for patients with higher nodal load ( n2 and n3 disease ) than those included in the supremo trial ( pn0 or pn1 )  . neoadjuvant chemotherapy treatment was allowed in a later protocol version ( version 29 ) , but the number of treated patients was too small ( n = 8 ) for valid conclusions and therefore we did not perform any betweengroup comparisons according to this variable . we observed a low frequency of immediate breast reconstruction ( which was done in only 111 patients )  . 
this procedure was associated with higher levels of fatigue and 1526 vol 19 november 2018 articles very compared with no immediate reconstruction , but had no effect on body image or the other qol outcomes . 
the estimated effect of immediate reconstruction on fatigue was 532 , corres ponding to a small clinically meaningful difference.23 however , this was an exploratory analysis and we used generic qol and body image questionnaires , which are likely to be less sensitive to specific outcomes than are breast reconstruction instruments ( such as breastq ) .17 the observed low frequencies ( 11% ) of reconstructive surgery ( either immediate or delayed to year 2 ) should be noted . 
this finding probably reflects the pattern of care in the period of the supremo trial recruitment ( 200613 ) or might be caused by concerns of enrolling patients who had undergone breast reconstruction into a trial of radiotherapy . 
we are collecting further infor mation on delayed ( beyond 2 years ) reconstructions , which will be analysed at 5 years and 10 years to provide valuable information about rates of breast reconstruction across the uk , as well as its effect on patients experiences and satisfaction with body image . 
a direct comparison of conventional versus hypofractionation for chest wall radiotherapy after breast reconstruction is being done in the usa by the alliance for clinical trials in oncology ( nct03414970 )  . 
the trial is ongoing and will complete recruitment in 2021 , with final results expected in august , 2025 . most of the published literature relating to the effect of adjuvant radiotherapy on qol consists of non randomised studies , often of small size , which could be subject to selection bias , and in which neither surgery , radiotherapy , nor systemic treatments were subject to prespecified quality assurance . 
for example , the start trial studied the late effects of different schedules of radiotherapy at 5 years and found that up to a third of women reported moderate or notable pain in the arm and shoulder and more than 10% had arm or hand swelling.12 the trial included a small number of patients who had mastectomy ( about 20% ) and although the qol results are consistent with ours , they are not directly comparable because only 10% of patients had chemotherapy and 20% had regional nodal irradiation in addition to breast or chest wall radiotherapy . 
the experience of breast or arm symptoms over 5 years represents chronic morbidity that has stronger asso ciation longterm qol , making these than cosmesis with important outcomes in clinical trials.28 the moving beyond cancer psychosocial intervention trial27 studied the qol of 558 women with stage 1 and 2 breast cancer treated with surgery alone ( breastconserving surgery or mastectomy ) , surgery with radio therapy , or surgery followed by chemotherapy and radiotherapy over 1 year , using the sf36 questionnaire . 
however , the measures of qol differ from those used in our study and details of chemotherapy regimens and staging were not available in the absence of case record review.27 a similar pattern of improvement in a range of symptoms and qol measures in the first year after diagnosis was observed in a cohort study of 285 women with early breast cancer , treated with surgery ( > 20% of patients had mastectomy ) , adjuvant radiotherapy ( 74% of patients ) , and systemic therapy ( > 30% of patients ) .29 finally , we found that younger women reported worse body image ( if younger than 45 years of age ) and anxiety problems ( if younger than 70 years )  . 
this finding is supported by other breast cancer qol studies , is con cordant with clinical experience , and emphasises the need for targeted psychological in younger women.11 , 30 younger women also reported worse chest wall symptoms ( including pain )  . 
in a populationbased prospective study of more than 3000 patients , 31 persistent pain following breast surgery ( breast conserving or mas tectomy ) was reported by half of the patients and the pain was more common after adjuvant radiotherapy and in younger women . 
the same finding was also reported in a randomised trial of radiotherapy after breastconserving surgery.13 , 31 the wide variation in reports ( 2560% ) might relate to varying definitions of pain , different methods of pain assessment , and mixture of surgery and adjuvant therapy . 
we do not know the reasons for the low rates of patient consent in some centres , but it might be related to availability of local resources ( dedicated clinical research nurses )  . 
furthermore , guidelines on surgery , radiotherapy , and systemic therapy were standardised in the protocol , so any variations in these treatment modalities between treatment groups are unlikely to affect the results . the main limitation of this substudy is not having a true pretreatment baseline qol assessment , because all patients were randomly assigned after mastectomy . 
the low qol scores at the time of randomisation might be explained by the recent breast cancer diagnosis and the surgical procedure , and the subsequent improvement in almost all scores is to be expected . 
we did not record qol scores during or shortly after the allocated radiotherapy treatment , so any differences in acute symptoms between groups , which might predict later toxicity , have not been captured . 
additionally , because the main trial is ongoing and the locoregional control and survival status of the patients in this substudy are not known to us , it is possible that patients who had relapsed or died might have had different patterns of qol than those who survived . notably , a larger proportion of participants in the qol substudy received the dose fractionation schedule as 40 gy in 15 fractions ( 68% ) than in the main trial ( 52% ) , in which a larger proportion received 50 gy in 25 fractions ( 27% in the main trial vs 11% in the substudy )  . 
this difference reflects the variations between standard practice in uk centres versus eortc centres at the time of the trial . in this 2year analysis , we have not investigated any effect of fractionation on the qol outcomes . 
however , because the clinical significance of the increased chest wall symptoms in the radiotherapy group at 2 years might be relatively low , we do not expect a major clinical impact of fractionation at this early timepoint . 
the effects of radiation dose fractionation and technique and radiation dose parameters on organs at risk will be the subject of a more detailed analysis to be performed in the radio therapy group , including assessment of toxicity ( phy sician scoring )  . 
the results will be reported in a separate publication , focusing on the specific technical aspects of the radiotherapy . this report presents a preplanned analysis 2 years after randomisation , with the main qol analysis planned at 5 years and qol data to be collected for 10 years to capture late adverse events . 
the recent us guidelines7 on postmastectomy radiotherapy empha sise the importance of shared decision making between physician and patient in weighing up the benefits and toxicity of treatment in patients with one to three positive nodes undergoing axillary node clearance . 
late radiotherapyinduced toxicity not seen within the first 2 years ( eg , progressive chest wall fibrosis or increased cardiac toxicity due to the com bination of radiotherapy and anthracyclinebased chemotherapy ) might be detected on longerterm followup and should be captured in our 5year and 10year analyses . 
however , we recognise that late cardiac toxicity from radiotherapy could occur beyond 10 years . the effect of postmastectomy radiotherapy on 10year survival , the primary endpoint of the main supremo trial , will not be known before 2023 . 
in the meantime , the decision to administer or omit postmastectomy radiotherapy can be considered preference sensitive for patients in the supremo trial risk category of one to three positive lymph nodes , because both options are legitimate . 
patients will be in a better position to make a value judgment on what they consider relevant for them , given the data on various qol domains presented in this report . 
both physicians and patients could thus be helped when weighing up the individual estimates of possible benefits of radiotherapy against the effect of post mastectomy radiotherapy on toxicity and qol endpoints . in conclusion , chest wall radiotherapy led to more chest wall symptoms up to 2 years after randomisation , but the difference was small and unlikely to be clinically significant . 
however , indications of worse qol scores for anxiety , body image , and chest wall symptoms in younger women irrespective of whether or not they received radiotherapy warrants further investigation . 
longerterm followup at 5 years and 10 years will be needed to see if these early findings in qol are sustained . contributors gv , ljw , sw , jmd , ihk , and nsr were involved in the study design . 
gv , ihk , and nsr gave final approval of the manuscript . declaration of interests gv has received research grants from the national institute of health research ( nihr ) , cancer research uk , and yorkshire cancer research , and personal fees from roche , novartis , and eisai . 
nsr has received research grants from the dutch cancer society and the european 1528 vol 19 november 2018 articles 3 cardoso f , vant veer lj , bogaerts j , et al . 
 we thank the medical research council ( eme 09 / 800 / 31 ) , european organisation for research and treatment of cancer , cancer australia , the dutch cancer society , and the trustees of the hong kong and shanghai banking corporation ( hsbc ) for funding the study . 
 we acknowledge the support of the staff at the information and statistical division at national services scotland and specifically kathleen riddle ( principal trial manager ) ; penelope hopwood ( the christie hospital , manchester , uk ) , initial chief investigator for the quality of life substudy ( who has subsequently retired ) ; the scottish cancer trials breast group , under whose auspices the trial was run ( chair : iain macpherson ) , the trial management group , the trial steering committee ( chair : barry hancock , university of sheffield , sheffield , uk ) , and the data monitoring and ethical committee ( chair : chris frost , london school of hygiene & tropical medicine , london , uk )  . 
we also thank the national institute for health research cancer research networks in england and their equivalent nhs research and developmentfunded networks in scotland , wales , and northern ireland for inkind support . articles arsenic trioxide and all - trans retinoic acid treatment for acute promyelocytic leukaemia in all risk groups ( aml17 ) : results of a randomised , controlled , phase 3 trial alan k burnett , nigel h russell , robert k hills , david bowen , jonathan kell , steve knapper , yvonne g morgan , jennie lok , angela grech , gail jones , asim khwaja , lone friis , mary frances mcmullin , ann hunter , richard e clark , david grimwade , for the uk national cancer research institute acute myeloid leukaemia working group background acute promyelocytic leukaemia is a chemotherapy - sensitive subgroup of acute myeloid leukaemia characterised by the presence of the pmlrara fusion transcript . 
in this study , we compare a chemotherapyfree atra and arsenic trioxide treatment regimen with the standard chemotherapy - based regimen ( atra and idarubicin ) in both high - risk and low - risk patients with acute promyelocytic leukaemia . methods in the randomised , controlled , multicentre , aml17 trial , eligible patients ( aged 16 years ) with acute promyelocytic leukaemia , con rmed by the presence of the pmlrara transcript and without signi cant cardiac or pulmonary comorbidities or active malignancy , and who were not pregnant or breastfeeding , were enrolled from 81 uk hospitals and randomised 1 : 1 to receive treatment with atra and arsenic trioxide or atra and idarubic atra was given to participants in both groups in a daily divided oral dose of 45 mg / m until remission , or until day 60 , and then in a 2 weeks on2 weeks o schedule . 
in the atra and arsenic trioxide group , arsenic trioxide was given intravenously at 03 mg / kg on days 15 of each course , and at 025 mg / kg twice weekly in weeks 28 of course 1 and weeks 24 of courses 25 . 
high - risk patients ( those presenting with a white blood cell count > 10 10 cells per l ) could receive an initial dose of the immunoconjugate gemtuzumab ozogamicin ( 6 mg / m intravenously )  . 
this trial is registered with the isrctn registry , number isrctn55675535 . findings between may 8 , 2009 , and oct 3 , 2013 , 235 patients were enrolled and randomly assigned to atra and idarubicin ( n = 119 ) or atra and arsenic trioxide ( n = 116 )  . 
after course 1 of treatment , grade 34 alopecia was reported in 23 ( 23% ) of 98 patients in the atra and idarubicin group versus 5 ( 5% ) of 95 in the atra and arsenic trioxide group , raised liver alanine transaminase in 11 ( 10% ) of 108 versus 27 ( 25% ) of 109 , oral toxicity in 22 ( 19% ) of 115 versus one ( 1% ) of 109 . 
after course 2 of treatment , grade 34 alopecia was reported in 25 ( 28% ) of 89 patients in the atra and idarubicin group versus 2 ( 3% ) of 77 in the atra and arsenic trioxide group ; no other toxicities reached the 10% level . 
patients in the atra and arsenic trioxide group had signi cantly less requirement for most aspects of supportive care than did those in the atra and idarubicin group . interpretation atra and arsenic trioxide is a feasible treatment in low - risk and high - risk patients with acute promyelocytic leukaemia , with a high cure rate and less relapse than , and survival not di erent to , atra and idarubicin , with a low incidence of liver toxicity . 
 as a genetically de ned subgroup , characterised by the pmlrara fusion gene generated by the t ( 15 ; 17 ) ( q22 ; q21 ) chromosomal translocation , it has been shown to be especially sensitive to anthracycline - based chemotherapy . 
in the acute promyelocytic leukaemia subgroup of acute myeloid leukaemia , all - trans retinoic acid ( atra ) , although not able to durably control the disease as monotherapy , has been shown to greatly improve cure when added to conventional chemotherapy in several studies . 
arsenic trioxide was also shown to be e ective as monotherapy , and in due course received regulatory approval for treatment of relapsed disease ( in september , 2000 , in the usa and in october , 2001 , in the european union )  . 
the italian and german collaboration ( gimema - amlsg - sal ) did the rst randomised comparison of this combination against the standard of care ( atra and idarubicin ) and showed that atra and arsenic trioxide resulted in superior survival compared with the chemotherapy - based standard of care . 
however , this study was restricted to low - risk patients and excluded the 25% of patients who presented with a white blood count of 10 10 cells per l or higher . 
it involved an intensive schedule of up to 140 doses of arsenic trioxide given by infusion daily over a period of 6 months , and was associated with a high proportion of patients having grade 34 liver toxicity . added value of this study the randomised national cancer research institute aml17 trial , reported here , also compared atra and arsenic trioxide with atra plus chemotherapy , but included high - risk patients ( who were given a single injection of the cd33 targeted immunoconjugate , gemtuzumab ozogamicin , at diagnosis to control the initial high white blood cell count )  . 
a less frequent dosing schedule of arsenic trioxide was used ( 63 doses within 6 months ) and showed a high cure rate with low toxicity and substantially less supportive care requirements than the standard of care ( atra and chemotherapy )  . 
the results are consistent with those of the gimema - amlsg - sal trial . implications of all the available evidence the combination of atra and arsenic trioxide is highly e ective in patients with acute promyelocytic leukaemia , irrespective of risk group , with the use of a modi ed administration schedule . 
 this nding suggests that a de - escalation of therapy in this disease can be implemented , with an associated high cure rate above 90% , without a ecting quality of life . 
encouraging non - randomised data have also been reported with gemtuzumab ozogamicin in this setting.11 , 12 a further step in treatment de - escalation was the exploration of arsenic trioxide plus atra in nonrandomised trials , 13 , 14 with investigators from the md anderson cancer center ( tx , usa ) reporting excellent results in low - risk patients ( presenting with a white blood cell count < 10 10 cells per l )  . 
high - risk patients ( those with a white blood cell count 10 10 cells per l ) were more di cult to treat , with di erentiation syndrome emerging as a limitation to a completely chemotherapyfree approach . 
however , following the addition of gemtuzumab ozogamicin , treatment of high - risk patients became feasible.15 it was subsequently necessary to establish that this standard cytotoxic chemotherapy - free approach was not inferior to the anthracycline and atra standard of care . the pivotal randomised gimema - amlsg - sal trial16 compared arsenic trioxide and atra versus idarubicin and atra treatment in low - risk patients , with the primary aim of showing that the chemotherapy - free approach was at least equivalent to the chemotherapy - based standard of care . 
results showed that patients treated with arsenic trioxide and atra had signi cantly better event - free survival than those treated with standard of care and after extended follow - up of more patients , overall survival was also signi cantly improved.17 however , this study excluded the roughly 25% of patients who are high risk ( ie , those who have a white blood cell count 10 10 cells per l ) , who are known to have an increased rate of early mortality . 
 here , we report on the aml17 trial , where we adopted an alternative dosing schedule for arsenic trioxide based on previous experience in a trial for myelodysplastic syndrome , giving 63 doses of arsenic trioxide within 6 months.18 this new dosing schedule was expected to be more convenient for patients and improve compliance . 
importantly , this study assessed all patients , including those with high - risk disease , who had the option of receiving gemtuzumab ozogamicin within the rst 4 days of the rst course of treatment . 
when the trial was designed , it was already known that the standard of care resulted in most patients being cured , so this trial was designed to investigate potential improvements in quality of life while at the same time not compromising survival outcomes . 1296 vol 16 october 2015 articles see online for appendix methods study design and participants the aml17 trial is a randomised , controlled , phase 3 , open - label multicentre trial for patients with acute myeloid leukaemia and high - risk myelodysplastic syndrome ( mds ) including acute promyelocytic leukaemia ; only the results of patients with acute promyelocytic leukaemia are reported here . 
patients with clinically suspected acute promyelocytic leukaemia aged 16 years and older were enrolled from 81 hospitals in the uk , denmark , and new zealand ( appendix p 1 )  . 
for patients to be eligible for the study , the presence of the pmlrara transcript had to be con rmed molecularly by a reference laboratory ( molecular oncology unit , guys hospital , london , uk )  . 
patients could not have received previous treatment for acute promyelocytic leukaemia , and those with a concurrent active malignancy , substantial cardiac arrhythmia , ecg abnormalities or neuropathy , left ventricular ejection fraction lower than 50% , uncontrolled life - threatening disease , or severe uncontrolled pulmonary or cardiac disease , and pregnant or breastfeeding women , were excluded . 
ethics approval was provided by wales rec 3 , and all participants provided signed informed consent . randomisation and masking in this open - label trial , eligible participants were randomly assigned 1 : 1 between arsenic trioxide and atra therapy or atra and idarubicin ( the standard of care )  . 
minimisation parameters were age ( 015 , 1629 , 3039 , 4049 , 5059 , or 60 years and older ) , who performance status ( 0 , 1 , 2 , 3 , or 4 ) , and de - novo versus secondary disease . procedures treatments are shown in the appendix pp 2 , 3 . 
atra 45 mg / m daily was given in an oral divided dose ( in two equal doses per day ) for up to 60 days as part of their rst course , and then at the same dose ( 45 mg / m as an oral divided dose ) on days 115 of subsequent courses . 
in the atra and arsenic trioxide group , patients received ve courses of treatment : atra was given at the same dose as in the other group ( 45 mg / m daily in an oral divided dose ) on days 160 of course 1 or until remission , and at the same dose on days 114 and 2942 in courses 24 , and days 114 of course 5 . 
arsenic trioxide was given intravenously at a dose of 03 mg / kg on days 15 of each course , and then in weeks 28 of course 1 and weeks 24 of courses 25 at 025 mg / kg twice weekly . 
 high - risk patients ( those with a white blood cell count 10 10 cells per l at diagnosis ) , if randomly assigned to the arsenic trioxide and atra group , could receive gemtuzumab ozogamicin ( 6 mg / m ) as a single infusion within the rst 4 days of the rst course , but clinicians were advised to give them this drug on day 1 if possible and on day 4 if necessary , of the rst course . 
neither maintenance treatment nor cns prophylaxis was given to patients in either group . during induction treatment , atra could be discontinued temporarily in either treatment group if differentiation syndrome , pseudotumour cerebri , or hepatotoxicity occurred . 
arsenic trioxide could be discontinued temporarily in the presence of di erentiation syndrome , qt prolongation on ecg , or hepatotoxicity ; the drug would be discontinued permanently in the event of cardiac arrhythmias or severe neurological toxicity . 
although provision was made for clinicians to discuss treatment or dosing modi cation with clinical coordinators ( ie , with no formal guidance being part of the protocol ) , no treatment modi cations were actually needed . 
if prolongation of the corrected qt interval ( qtc prolongation ) was recorded , clinicians were advised to ensure that electrolyte levels , including that of magnesium , were corrected . molecular con rmation of the presence of a pmlrara rearrangement by a reference laboratory enabled each patient to be monitored by real - time quantitative pcr ( rtqpcr ) assays for pmlrara ( and reciprocal rarapml transcripts , if applicable ) exclusively in bone marrow after each course of treatment and at 3 - monthly intervals for 3 years , as previously described.19 patients with con rmed rt - qpcr positivity at the end of treatment were de ned as having molecularly persistent disease . 
for patients who achieved a molecular complete remission , a diagnosis of molecular relapse was de ned by rt - qpcr positivity in two successive bone marrow samples at least 2 weeks apart . 
 guidance was provided for blood product and platelet support and intervention for suspected di erentiation syndrome as set out in the british committee for standards in haematology guidelines.20 no prophylaxis for differentiation syndrome was recommended , but prompt use of dexamethasone was suggested on clinical suspicion of syndrome . 
recommended emergent di erentiation salvage treatment for patients who relapsed was treatment with arsenic trioxide , with the option of a subsequent stem cell transplant if judged appropriate . outcomes the primary outcome was quality of life , assessed with the european organisation for research and treatment of cancer ( eortc ) qlq - c30 questionnaire and the hospital anxiety and depression scale . 
toxicity was recorded using the national cancer insistute common terminology criteria for adverse events ( nci - ctc ) version 3.0. secondary outcomes were overall survival , relapse - free survival and event - free survival , and the incidence of vol 16 october 2015 1297 articles relapse ( both morphological and molecular ) , death without relapse , and treatment - related myelodysplastic syndrome or acute myeloid leukaemia . statistical analysis all analyses are by intention - to - treat on the population with con rmed acute promyelocytic leukaemia . 
to analyse continuous or scale variables we used wilcoxon rank - sum time - to - event outcomes for ( including 30 - day and 60 - day mortality ) we used log - rank tests and kaplan - meier or cumulative incidence curves . 
 * patients in these three categories of white blood cell count were high risk . table 1 : baseline characteristics figure 1 : trial pro le atra = all - trans retinoic acid . 1298 vol 16 october 2015 articles treatment - related myelodysplastic syndrome or acute myeloid leukaemia as competing risks . 
the cumulative incidence of treatment - related myelodysplastic syndrome or acute myeloid leukaemia has competing risks of death or relapse ; whereas for the cumulative incidence of haematological relapse , treatment - related myelodysplastic syndrome , acute myeloid leukaemia , and death are competing risks . 
event - free survival is de ned as time from randomisation to death , treatment - related myelodysplastic syndrome or acute myeloid leukaemia , or morphological relapse for patients entering remission ; patients who do not achieve a complete remission are de ned as experiencing an event on day 1 . in addition to overall analyses , we did prespeci ed exploratory analyses strati ed for age , sex , white blood cell count ( including high - risk and low - risk patients ) , diagnosis , performance transcript ( rarapml ) status , and pml breakpoint , with appropriate tests for interaction . 
follow - up is complete until jan 1 , 2014 . role of the funding source the funder of the study had no role in the design or analysis of the trial , data collection or interpretation , or in drafting of the report . 
the corresponding author ( akb ) had full access to all the data and had nal responsibility for the decision to submit for publication . results between may 8 , 2009 , and oct 3 , 2013 , 242 patients with suspected acute promyelocytic leukaemia were enrolled . 
 seven patients were excluded because they tested negative for the pmlrara fusion transcript and 235 eligible patients were randomly assigned to receive either atra and arsenic trioxide ( n = 116 ) or atra and idarubicin ( n = 119 )  . 
of these 235 participants , 57 were high - risk patients ( 30 in the atra and arsenic trioxide group and 27 in the atra and idarubicin group )  . 
28 ( 93% ) of 30 high - risk patients in the atra and arsenic trioxide group received gemtuzumab ozogamicin ( the other two high - risk patients did not because there was no gemtuzumab ozogamicin available at their site pharmacy so they were given an anthracycline instead ) , with a further seven low - risk patients given gemtuzumab ozogamicin for a rising white blood cell count . 
117 ( 98% ) of 119 patients allocated to atra and idarubicin received their allocated treatment in course 1 , compared with 115 ( 99% ) of 116 allocated to atra and arsenic trioxide ( gure 1 )  . 
the rate of compliance with molecular monitoring to at least 12 months post treatment exceeded 90% in both groups . arsenic levels in plasma were monitored in 41 patients who were given arsenic trioxide upfront ( n = 33 ) or in relapse ( n = 8 )  . 
hads = hospital anxiety and depression scale . vol 16 october 2015 1299 articles a total of 671 completed quality - of - life forms were received ( 156 at baseline , 137 at 3 months , 139 at 6 months , 136 at 12 months , and 103 at 24 months )  . 
in each treatment group , the numbers of completed quality - of - life forms at each timepoint were : atra and idarubicin 76 at baseline versus atra and arsenic trioxide 80 at baseline ; 64 versus 73 at 3 months ; 70 versus 69 at 6 months ; 64 versus 72 at 12 months ; and 49 versus 54 at 24 months . 
the results showed no statistically signi cant di erence on the primary outcome of global functioning ( e ect size 217 [ 95% ci 279 to 712 ] , p = 039 ; gure 2 ) , and , based on the power calculation , the con dence intervals rule out a minimally clinically important disadvantage of six points for atra and arsenic trioxide versus atra and idarubic on other measures , point estimates tended to favour atra and arsenic trioxide over atra and idarubicin , with signi cant bene ts recorded for cognitive and role functioning , although the size of any bene t was modest ( gure 2b )  . of the 235 patients , 215 ( 91% ) achieved morphological remission , which was con rmed molecularly 211 patients , with four cases of molecularly persistent disease ( one in the atra and idarubicin group and three in the atra and arsenic trioxide group )  . 
at 30 days , ve deaths had occurred in the atra and arsenic trioxide group compared with seven in the atra and idarubicin group ; 30 - day mortality did not di er signi cantly between the two groups ( table 2 )  . 
at 60 days , six patients had died in the atra and arsenic trioxide group compared with 11 in the atra and idarubicin group ; the 60 - day mortality did not di er between the groups ( table 2 )  . the causes of death at 60 days in the six patients who died in the atra and arsenic trioxide group were : three cardiac events , one infection , one renal failure , and one from several causes . 
in the 11 patients who died in the atra and idarubicin group after 60 days , the causes of death were : three haemorrhages , three infections , two pulmonary causes , one renal cause , and two cases of progressive disease . 
complete molecular remission was achieved by patients in the atra and idarubicin group at a median time of 83 days ( iqr 65124 ) and by patients in the atra and arsenic trioxide group at a median time of 111 days ( 61140 ) ; this di erence was not signi cant ( p = 0055 )  . 
more patients had con rmed molecular negativity at 60 days in the atra and idarubicin group ( 54 [ 73% ] of 74 patients ) than in the atra and arsenic trioxide group ( 46 [ 56% ] of 82 patients ; p = 003 )  . 
 di erentiation syndrome was reported in 38 ( 21% ) of 178 low - risk patients ( 23 in the atra and arsenic trioxide group , and 15 in the atra and idarubicin group ) and in 17 ( 30% ) of 57 high - risk patients ( seven in the atra and arsenic trioxide group and ten patients in the atra and idarubicin group ; overall p value for comparison = 038 )  . 
 only four patients ( two in each treatment group , three of whom were low risk and one high risk ) survived beyond day 60 without morphological remission . one case of treatment - related acute myeloid leukaemia was reported ( trisomy 11 , in a patient in the atra and idarubicin group who was con rmed as pmlrara negative 395 months after diagnosis ) , and 23 patients in both treatment groups combined exhibited either disease persistence or recurrence ( four molecularly persistent disease [ including one subsequent cns relapse ] , six molecular relapse alone , eight haematological relapse , two haematological and cns relapse , and three cases of isolated extramedullary disease )  . 
in all cases , extramedullary disease involving the skin ( n = 1 , in the atra and idarubicin group ) or cns ( n = 4 , one in the atra and arsenic trioxide group and three in the atra and idarubicin group ) was accompanied by detection of acute promyelocytic leukaemia fusion transcripts in the bone marrow . 
three patients in complete remission con rmed molecular negativity 30 - day mortality 60 - day mortality 4 - year survival 4 - year event - free survival 4 - year morphological recurrence - free survival 4 - year molecular recurrence - free survival * 4 - year cumulative incidence of death in remission 4 - year cumulative incidence of morphological relapse 4 - year cumulative incidence of molecular relapse * 4 - year cumulative incidence of treatment - related myelodysplastic syndrome or acute myeloid leukaemia table 2 : clinical outcomes atra and idarubicin ( n = 119 ) atra and arsenic trioxide ( n = 116 ) or / hr ( 95% ci ) p value 106 ( 89% ) 105 ( 88% ) 6% ( 312 ) 9% ( 516 ) 89% ( 8193 ) 70% ( 5680 ) 78% ( 6388 ) 70% ( 6283 ) 1% ( 028 ) 18% ( 1034 ) 27% ( 1845 ) 3% ( 0417 ) 109 ( 94% ) 106 ( 91% ) 4% ( 210 ) 5% ( 211 ) or 054 ( 021134 ) or 071 ( 031165 ) hr 072 ( 023231 ) hr 055 ( 021143 ) 93% ( 8696 ) hr 060 ( 026142 ) 91% ( 8495 ) hr 035 ( 018068 ) 97% ( 9099 ) hr 024 ( 009060 ) 018 043 056 022 025 0002 0004 98% ( 9199 ) hr 017 ( 008039 ) < 00001 2% ( 19 ) hr 172 ( 018166 ) 064 1% ( 017 ) hr 016 ( 006046 ) hr 012 ( 005030 ) hr 015 ( 0003748 ) 034 00007 < 00001 data are n ( % ) or % ( 95% ci ) , unless otherwise indicated . 
 1300 vol 16 october 2015 articles atra and idarubicin atra and arsenic trioxide patients observed events ( n ) expected events ( n ) patients observed events ( n ) expected events ( n ) atra and idarubicin atra and arsenic trioxide 104 * atra and idarubicin atra and arsenic trioxide 103 * 100 hr 016 ( 006046 ) , p = 00007 hr 012 ( 005030 ) , p < 00001 number at risk atra and idarubicin atra and arsenic trioxide time ( years from complete remission ) time ( years from molecular complete remission ) patients observed events ( n ) expected events ( n ) low - risk patients ( n ) observed events ( n ) expected events ( n ) atra and idarubicin atra and arsenic trioxide 117 * 104 106 atra and idarubicin atra and arsenic trioxide hr 060 ( 026142 ) , p = 025 hr 047 ( 016139 ) , p = 017 number at risk atra and idarubicin atra and arsenic trioxide time ( years from study entry ) time ( years from study entry ) high - risk patients ( n ) observed events ( n ) expected events ( n ) atra and idarubicin atra and arsenic trioxide hr 082 ( 020331 ) , p = 078 hr 082 ( 025268 ) , p = 075 patients older than 60 years of age ( n ) observed events ( n ) expected events ( n ) atra and idarubicin atra and arsenic trioxide time ( years from study entry ) number at risk atra and idarubicin atra and arsenic trioxide time ( years from study entry ) figure 3 : clinical outcomes ( a ) cumulative incidence of haematological relapse . 
 * two patients in the atra and idarubicin group ( one high risk and one low risk ) had no follow - up data available for survival or relapse . the atra and arsenic trioxide group had molecularly persistent disease ( associated with cns involvement in one case ) compared with one patient in the atra and idarubicin group . 
the number of patients who relapsed in the latter group was signi cantly higher ( 20 relapses across both groups [ 19 in the atra and idarubicin group vs one in the atra and arsenic trioxide group ] ) , of which 13 were haematological and seven were molecular alone , giving a incidence of haematological relapse of cumulative 18% ( 95% ci 1034 ) in the atra and idarubicin group versus 1% ( 017 ) in the atra and arsenic trioxide group ( gure 3a )  . 
the one patient who relapsed in the atra and arsenic group did not become molecularly negative , thus the cumulative incidence of molecular relapse at 4 years vol 16 october 2015 1301 articles was 27% ( 95% ci 1845 ) in the atra and idarubicin group versus 0% in the atra and arsenic trioxide group ( gure 3b )  . 19 ( 95% ) of the 20 patients who relapsed received arsenic trioxide salvage therapy ; the other died before salvage treatment could be given . 
of nine patients in either group treated pre - emptively for molecularly persistent disease or molecular relapse with arsenic trioxide , all achieved complete molecular remission and eight remain alive at nal follow - up . 
overall , nine patients in the atra and idarubicin group that relapsed received a transplant ( six post - morphological relapse [ three autografts and three allografts ] , ve of whom were in second complete remission ; and relapse only [ two allografts and one autograft ] ) and the patient in the atra and arsenic trioxide group also received an allograft transplant but died afterwards . 
eight of the nine patients in the atra and idarubicin group who received a transplant remain alive with median post - transplant follow - up of 76 months ( iqr 6297 )  . 
of the 20 patients in both groups who relapsed , two died ( including the only patient in the atra and arsenic trioxide who relapsed , who died from an infection 78 days after receiving a sibling allograft transplant in their second remission ) ; eight relapses occurred in 49 high - risk patients and 12 in 166 low - risk patients . three post - molecular the cumulative incidence of death in remission was low overall and did not di er signi cantly between the groups ( table 2 )  . 
event - free survival for all patients was 80% at 4 years ( 82% in low - risk patients and 76% in high - risk patients ) , and was signi cantly better in the atra and arsenic trioxide group than in the atra and idarubicin group ( table 2 )  . 
in low - risk patients , 4 - year survival was 95% ( 95% ci 8698 ) in the atra and arsenic trioxide group versus 90% ( 8195 ) in the atra and idarubicin group ( gure 3d ) compared with 87% ( 6895 ) versus 84% ( 6394 ) in high - risk patients ( gure 3e ) with no evidence of interaction between treatment and risk group ( p = 05 )  . 
excluding early mortality in a landmark analysis of survival post day 30 , overall 4 - year survival was 97% ( 95% ci 9099 ) for atra and arsenic trioxide ( 96% [ 8799 ] in low - risk patients , 100% in high - risk patients ) compared with 94% ( 8897 ) with atra plus idarubicin ( 94% [ 8697 ] in low - risk patients , 95% [ 7099 ] in high - risk patients )  . 
survival at 4 years in the 28 of 30 high - risk patients who were allocated to atra and arsenic trioxide and given gemtuzumab ozogamicin was 89% ( 95% ci 7096 )  . 
the trial included 49 patients aged older than 60 years ( 37 low - risk and 12 high - risk patients ) whose 4 - year survival did not di er signi cantly between the treatment groups : 80% ( 5891 ) in the atra and arsenic trioxide group , compared with 74% ( 5087 ) in the atra and idarubicin group ( gure 3f )  . exploratory analyses showed no signi cant interaction between treatment and baseline features , with the exception of a suggestion of heterogeneity by pml breakpoint ( appendix p 4 )  . 146 serious adverse events ( 64 in the atra and arsenic trioxide group vs 82 in the atra and idarubicin group ) , including death ( not routinely assessed for relatedness to study drug ) , were recorded in 99 patients ( 46 vs 53 in the two groups , respectively )  . 
during treatment courses 12 , grade 34 toxicities were reported in 40 patients randomly assigned to atra and arsenic trioxide and in 57 randomly assigned to atra and idarubicin ( tables 3 and 4 )  . 
for treatment course 1 , alopecia , gastrointestinal events , hyperbilirubinaemia , and cardiac events were more common with atra and idarubicin , and there was no di erence in high liver alanine transaminase ( alt ) levels between the two groups . 
 after course 1 of treatment , liver grade 34 toxicities of alt were more frequent in the atra and arsenic trioxide group than in the atra and idarubicin group ( table 3 ) , whereas liver grade 34 toxicities of aspartate aminotransferase ( ast ) did not di er between the groups , and grade 34 hyper bilirubinaemia , although rare , was signi cantly more frequent with idarubicin than with arsenic trioxide ( table 3 )  . 
 liver toxicities did not di er between the groups after treatment course 2 , and they were not increased in either course in the recipients of gem tuzumab ozogamicin ( grade 34 liver toxicity for gem tuzumab ozogamicin vs no gemtuzumab ozogamicin after course 1 : raised alt 26% vs 24% , raised ast 9% vs 20% , raised bilirubin 0% vs 1% ; after course 2 raised alt 3% vs 2% , and no grade 34 ast or bilirubin toxicities ) with no evidence of additional myelosuppression . 
after course 2 , cardiac toxicity was more common in the atra and arsenic trioxide group than in the atra and idarubicin group ( p = 0001 ; table 4 )  . dose modi cations or delays to atra occurred in 13 patients in the atra and idarubicin group and in 30 patients in the atra and arsenic trioxide group during course 1 ; idarubicin was modi ed in six patients and arsenic trioxide in nine patients , three of whom had a prolonged qtc . 
in the atra and arsenic trioxide group , two additional patients interrupted all treatment , and one withdrew from the trial during course 1 of treatment because of fungal chest complications . 
during course 2 , nine patients on atra and idarubicin had treatment modi cations or delays , including one who switched to atra and arsenic trioxide ( clinicians decision ) , whereas 18 patients in the atra and arsenic trioxide group had dose modi cations or delays , including six who switched to idarubicin ( clinicians decision )  . 
the denominators di er for the various toxic e ects because of variations in the total numbers of patients returning data for each e ect . table 4 : incidence of non - haematological toxic e ects following two courses of treatment and arsenic trioxide group were not given arsenic trioxide because of qtc prolongation . 
at day 60 , 17 patients had died ; deaths were not assessed for relatedness to treatment . supportive care requirements were signi cantly lower during the rst two courses of treatment for atra and arsenic trioxide than for atra and idarubicin on all measures except for antibiotic use in course 2 ( table 5 )  . 
 during the rst two courses of treatment , compared with atra and idarubicin , atra and arsenic trioxide treatment was associated with an average of 74 fewer days in hospital , 45 fewer units of blood , 43 fewer units of platelets , and 107 fewer days of intravenous antibiotics . discussion this study found that the quality of life did not di er signi cantly in patients with acute promyelocytic leukaemia treated with either atra and arsenic trioxide or atra and idarubic this study also con rms the feasibility and bene t of atra and arsenic trioxide atra and idarubicin atra and arsenic trioxide p value blood , units course 1 course 2 platelets , units antibiotics , days hospital stay , days course 1 course 2 course 1 course 2 course 1 course 2 95 ( 51 ) 10 ( 17 ) 128 ( 91 ) 03 ( 10 ) 192 ( 97 ) 17 ( 42 ) 59 ( 55 ) 01 ( 05 ) 88 ( 108 ) 0 ( 0 ) 93 ( 94 ) 09 ( 25 ) < 00001 < 00001 < 00001 00001 < 00001 040 < 00001 001 333 ( 96 ) ; 34 ( 2937 ) 273 ( 165 ) ; 25 ( 1534 ) 79 ( 87 ) ; 5 ( 210 ) 65 ( 98 ) ; 1 ( 010 ) data are mean ( sd ) or mean ( sd ) ; median ( iqr )  . 
atra = all - trans retinoic acid . table 5 : supportive care for patients with acute promyelocytic leukaemia in the two groups during treatment courses 1 and 2 vol 16 october 2015 1303 articles treatment as the next stage in treatment de - escalation in low - risk patients with acute promyelocytic leukaemia , with excellent outcomes . 
this experience from the present aml17 study and the gimema - amlsg - sal trial16 emerges from 81 national cancer research institute and 67 gimema - amlsg - sal centres , and thereby endorses the widespread applicability of this approach . 
here , we suggest that a similar approach is also feasible in high - risk patients , if provision is made for at least one dose of a chemotherapeutic agent during induction therapy , such as gemtuzumab ozogamicin as used in this trial , but an anthracycline might have been just as e ective . 
although known to be an e ective agent in acute promyelocytic leukaemia , and not associated with hepatotoxicity or additional myelosuppression in this study , we cannot de nitively say whether or not the single dose of gemtuzumab ozogamicin used here contributed to the notable low risk of relapse . 
49 older patients entered , with encouraging 83% 4 - year survivala promising nding in view of the fact that older patients are usually more di cult to treat and have poorer survival than younger patients . lower as was the case in gimema - amlsg - sal , 16 , 22 we recorded little signi cant di erence in quality of life between the groups in this trial . 
however , a reduced requirement for infusions would be expected to be bene cial , and the quality - of - life surveys used do not directly capture this parameter . 
in particular , in patients in the aml17 trial , the alternative dosing schedule used meant that fewer days , and a correspondingly lower cumulative dose , of arsenic trioxide treatment were scheduled ( 63 / 168 days , com pared with 140 / 180 days in the gimema - amlsg - sal protocol )  . 
in aml17 , treatment with atra and arsenic trioxide resulted in a incidence of hyper bilirubinaemia than treatment with atra and idarubicin , with little incidence and no signi cant di erences between the treatment groups in subsequent treatment courses . 
conversely , higher liver ast levels were observed in patients treated with atra and arsenic trioxide than in those treated with atra and idarubic liver toxicity was not associated with gemtuzumab ozogamicin the gimema - amlsg - sal trial , grade 34 liver toxicity was recorded in 63% of patients treated with atra and arsenic trioxide , sometimes necessitating dose modi cation . 
cardiac toxicity during courses 12 of treatment was reported in 25 ( 22% ) of 114 patients in the atra and arsenic trioxide group and was more frequent ( 11% vs 0% ) than for atra and idarubicin post course 2 . 
a further di erence the elimination of maintenance therapy in aml17 , because of previous concerns that it might contribute to treat mentrelated acute myeloid leukaemia or myelodysplastic syndrome , which has been reported as a cause of treatment failure in 12% of cases of acute promyelocytic leukaemia.5 encouragingly , we recorded only one case of treatment - related acute myeloid leukaemia in aml17 ( in the idarubicin group ) , compared with nine cases in 285 chemotherapy - treated patients in the previous aml15 trial that included maintenance treatment.5 the attenuated dosing schedule used in this trial o ers the obvious advantage of convenience for the patients compared with atra and idarubicin , but also reduces administration and acquisition costs of arsenic trioxide . 
 in our view , the main limitation of atra and idarubicin treatment has been its inability to completely eliminate early deaths , which will not appear in standard quality - oflife measures because patients will have died before their rst assessment point . 
although this treatment regimen showed some improvement in quality of life over the course of treatment in this trial ( with quality of life in survivors improving during treatment , reaching a median of 75 points out of 100 on the global functioning scale ) , its inability to eliminate early deaths remains the main reason for treatment failure . 
few deaths occurred beyond 30 days in either group and the landmark kaplan - meier survival analysis post day 30 , 4 - year survival was higher in the atra and arsenic trioxide group than in the atra and idarubicin group , especially in high - risk patients . 
mortality at day 30 was reduced in lowrisk patients from our historical rate of 5% ( in aml15 ) to 1% for atra and arsenic trioxide in aml17 and seems to endorse the strategy of giving patients arsenic trioxide from the time of diagnosis rather than in consolidation , by which time the period of greatest risk has passed.23 although 30 - day mortality was reduced in the atra and arsenic trioxide group compared with previous studies , this was also the case in the atra and idarubicin group . 
 this nding suggests that the clear guidance given to investigators within the protocol and national and international guidelines20 , 24 about early supportive care for patients with acute promyelocytic leukaemia has had an e ect in recent years . 
 acquisition costs , even for the attenuated schedule of arsenic trioxide , are clearly important , and are compounded by an absence of licensing approval for rst - line treatment . 
 the schedule for front - line therapy could possibly be attenuated further ( ie , reduced treatment and reduced toxicity , which could be especially relevant in children ) , but attention will now move to substitution with oral 1304 vol 16 october 2015 articles formulations , the experience of which suggests equivalence of e ect25 , 26 and arguably a better pharmacokinetic pro le27 with consequent potential for reduced toxicity.28 the risk of relapse on the arsenic trioxide and atra schedule is low ( 1% in aml17 and 26% in gimema - amlsg - sal ) which questions whether routine molecular monitoring is needed if arsenic trioxide and atra is adopted as the standard of care . 
a further issue is the consequences of delay in implementation of treatment , 29 which mandates prompt referral and , crucially , that relevant medication is immediately available in each treating institution . contributors akb designed the trial , interpreted the data , wrote the report , and coordinated the study . 
all authors reviewed the nal version of the report . declaration of interests akb received funding from cancer research uk , and free drug and grants from cephalon / teva during the course of the study . 
we thank cancer research uk for providing research support for the trial ; cephalon and teva for providing arsenic trioxide and a grant for assessment of arsenic trioxide levels in patient samples ; the main investigators and colleagues who enrolled patients ; guys & st thomas hospital ( london , uk ) for curation of the molecular monitoring database ; and the haematology cancer trials unit at cardi university . comment published online may 12 , 2015 s1470 - 2045 ( 15 ) 70201 - 9 see articles page 656 we declare no competing interests . evans mk , longo dl . 
n engl j med 2014 ; 371 : 497506 . cybulski c , kluniak w , huzarski t , et al , and the polish hereditary breast cancer consortiuclinical outcomes in women with breast cancer and a palb2 mutation : a prospective cohort analysis . 
in a meta - analysis that included 2447 patients with breast cancer treated in a rst - line setting , bevacizumab slightly improved progression - free survival ( hr 064 , 95% ci 057071 ; median 92 months vs 67 months ) and did not improve overall survival ( hr 097 , 95% ci 086108 ; 267 months vs 264 months ) .1 guidelines recommend this drug as an option only in selected cases because of the slight improvement in progression - free survival , lack of bene t in overall lack of predictive biomarkers , survival , high cost , and associated toxicities.2 more recently , a phase 3 randomised trial reported that bevacizumab did not improve outcome as adjuvant treatment in patients with triple - negative breast cancer.3 it is important to emphasise that this trial was done in patients with intermediate risk of relapse , and the e ect of bevacizumab in high - risk patients is still unknown . 
 overall , although the drug is still widely used in several countries , the enthusiasm associated with bevacizumab has dramatically decreased , and some countries have either restricted or stopped its use . 
 in the lancet oncology , helena earl and colleagues4 report pathological complete response results of a phase 3 randomised trial assessing the e cacy of bevacizumab in the neoadjuvant setting . 
a signi cantly greater proportion of patients treated with bevacizumab and chemotherapy achieved a pathological complete response ( 22% [ 95% ci 1827 ] ) compared with those treated with chemotherapy alone ( 17% [ 1321 ] )  . 
the magnitude of improvement was numerically more pronounced in patients with oestrogen receptor ( er ) negative ( 45% [ 95% ci 3655 ] vs 31% [ 2340 ] ) or er poor ( 51% [ 3468 ] vs 30% [ 1647 ] ) breast cancer , as opposed to those with er strongly positive breast cancer ( 6% [ 310 ] vs 7% [ 411 ] )  . 
nevertheless , this wave of randomised trials in the neoadjuvant setting , pending cooperation between the groups and support 600 vol 16 june 2015 comment from funding agencies , will certainly open a new era for the development of bevacizumab in breast cancer . 
a meta - analysis will allow better understanding about which population derives more bene t , which chemotherapy backbone is the most appropriate , and will assess the e ect of bevacizumab on outcome ( disease - free survival and overall survival ) in a large population of patients presenting with highrisk breast cancers . 
to what extent an improvement in pathological complete response translates into disease - free survival and overall survival bene t is still controversial in breast cancer , and this meta - analysis , based on a large number of patients , will certainly help . 
 several molecular predictors have already been proposed , including vascular cell adhesion molecule 1 , intercellular adhesion molecule 1 , e - selectin , and circulating vegfr - 2.8 because most trials were done in a metastatic setting , no opportunity existed until now to test tissue - based biomarkers in samples obtained at baseline before therapy . 
for example , bevacizumab has been reported to modulate the immune system through dendritic cells and regulatory t - cell functions , and could facilitate t - cell homing.9 if molecular analyses from neoadjuvant studies con rm an e ect of bevacizumab on the immune system , they could generate a rationale for immunogenic chemotherapy , anti - pd1 agents , and bevacizumab . 
 triple combination therapy of overall , the study by earl and colleagues , 4 consistent with previous trials , suggests that bevacizumab could improve pathological complete response in patients with breast cancer . 
these four trials could constitute the starting point of a new era for bevacizumab in breast oncology and could help to de ne which patients are more likely to bene t from bevacizumab , and which drug should optimally be combined with it . * fabrice andre , elise deluche , herve bonnefoi department of medical oncology , gustave roussy , villejuif , france ( fa , ed ) ; inserm unit u981 and universit paris sud , facult de medecine kremlin bicetre , kremlin bicetre , france ( fa ) ; and department of medical oncology , institut bergonie , bordeaux , france ( hb ) fandre@igr.fr fa reports grants from novartis , astrazeneca , and eisai , outside the submitted work . 
e cacy of neoadjuvant bevacizumab added to docetaxel followed by uorouracil , epirubicin , and cyclophosphamide , for women with her2 - negative early breast cancer ( artemis ) : an open - label , randomised , phase 3 trial . 
impact of the addition of carboplatin and / or bevacizumab to neoadjuvant once - per - week paclitaxel followed by dose - dense doxorubicin and cyclophosphamide on pathologic complete response rates in stage ii to iii triple - negative breast cancer : calgb 40603 ( alliance )  . 
parenthood in female survivors of hodgkins lymphoma in the lancet oncology , jurgen brmswig and colleagues1 report pregnancy outcomes in 467 female long - term survivors of hodgkins lymphoma who were younger than 18 years at diagnosis and treated in one of ve concurrent clinical trials in germany and austria between 1978 and 1995 . 
in the eortc trial , eligible women had biopsy - proven international federation of gynecology and obstetrics ( figo ) stage iiic or iv invasive epithelial tubo - ovarian carcinoma . 
the main aim of the pooled analysis was to show noninferiority in overall survival with neoadjuvant chemotherapy compared with upfront debulking surgery , using the reverse kaplan - meier method . 
tests for heterogeneity were based on cochrans q heterogeneity statistic . findings data for 1220 women were included in the pooled analysis , 670 from the eortc trial and 550 from the chorus trial . 
55 ( 5% ) women had figo stage iiiiib disease , 831 ( 68% ) had stage iiic disease , and 230 ( 19% ) had stage iv disease , with staging data missing for 104 ( 9% ) women . 
in the entire population , no difference in median overall survival was noted between patients who underwent neoadjuvant chemotherapy and upfront debulking surgery ( 276 months [ iqr 141513 ] and 269 months [ 127501 ] , respectively ; hazard ratio [ hr ] 097 , 95% ci 086109 ; p = 0586 )  . 
median overall survival for eortc and chorus patients was significantly different at 302 months ( iqr 157537 ) and 236 months ( 105469 ) , respectively ( hr 120 , 95% ci 106136 ; p = 0004 ) , but was not heterogeneous ( cochrans q , p = 017 )  . 
women with stage iv disease had significantly better outcomes with neoadjuvant chemotherapy compared with upfront debulking surgery ( median overall survival 243 months [ iqr 141476 ] and 212 months [ 100364 ] , respectively ; hr 076 , 95% ci 058100 ; p = 0048 ; median progression - free survival 106 months [ 79150 ] and 97 months [ 52132 ] , respectively ; hr 077 , 95% ci 059100 ; p = 0049 )  . interpretation long - term follow - up data substantiate previous results showing that neoadjuvant chemotherapy and upfront debulking surgery result in similar overall survival in advanced tubo - ovarian cancer , with better survival in women with stage iv disease with neoadjuvant chemotherapy . 
 we found that survival data from randomised studies had been published for only two trials : the european organisation for research and treatment of cancer ( eortc ) 55971 trial , and the medical research council chemotherapy or upfront surgery ( chorus ) trial . 
both trials concluded that neoadjuvant chemotherapy followed by interval debulking surgery was not inferior to primary debulking surgery followed by chemotherapy in patients with international federation of gynecology and obstetrics ( figo ) stage iiic or iv ovarian carcinoma . 
in addition to these two trials , the scorpion and jcog0602 randomised trials concluded that perioperative morbidity was better with interval debulking after neoadjuvant chemotherapy than after primary debulking surgery . added value of this study we report a per - protocol pooled analysis of individual patient data from the eortc 55971 and chorus randomised trials , to examine the long - term outcomes in patients with advanced ovarian cancer treated with neoadjuvant chemotherapy followed by interval debulking versus upfront debulking surgery followed by chemotherapy . 
we also did subgroup analyses on the basis of stratification factors that were common to both trialsie , randomising centre , largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 cm to 20 cm , and > 20 cm ) , and clinical figo stage . 
our analysis shows that , with longer median follow - up , both neoadjuvant chemotherapy followed by interval debulking surgery and upfront debulking surgery followed by chemotherapy are associated with similar overall survival and progression - free survival . 
we also show that neoadjuvant chemotherapy is associated with better progression - free survival and overall survival in women presenting with figo stage iv disease , and patients with figo stage iiic disease with extrapelvic metastases smaller than 5 cm have better progression - free survival after upfront debulking . implications of all the available incidence earlier studies showed already that overall survival is similar in patients with stage iiiciv tubo - ovarian cancer treated with neoadjuvant chemotherapy followed by interval debulking surgery , compared with upfront debulking surgery followed by chemotherapy . 
participants in this study had figo stage iiic or iv tubo - ovarian cancer with metastatic disease with a high tumour burden at presentation , and many had a poor performance status . 
this individual patient data pooled analysis suggests that neoadjuvant chemotherapy should be the standard of care for most patients with stage iv tubo - ovarian cancer and that primary surgery should only be undertaken in exceptional circumstances in patients with figo stage iv disease on an individual basis . 
however , women with figo stage iiic disease with extrapelvic metastases smaller than 5 cm had a significantly better progression - free survival with upfront debulking surgery than with neoadjuvant chemotherapy , so these patients should first be considered for primary debulking surgery . 
in 2010 , the european organisation for research and treatment of cancer ( eortc ) published the first findings from a trial comparing neoadjuvant chemotherapy followed by interval debulking surgery with upfront debulking surgery ( eortc 55971 ) .4 this study showed both treatment strategies had similar overall survival and progression - free survival in women with international federation of gynecology and obstetrics ( figo ) stage iiic or iv tubo - ovarian cancer , and operative and postoperative morbidity was lower with neoadjuvant chemotherapy . 
these results were later substantiated in the randomised medical research council ( mrc ) chemotherapy or upfront surgery ( chorus ) trial , 5 leading to the acceptance of neoadjuvant chemotherapy followed by interval debulking surgery as an alternative to upfront debulking surgery in women with stage iiic and iv tubo - ovarian cancer.6 however , the selection of women with advanced ovarian cancer for neoadjuvant chemotherapy or upfront debulking surgery remains controversial.7 therefore , we did a pooled analysis of the long - term outcomes of the eortc 55971 and chorus trials to identify subgroups of women who could benefit from neoadjuvant chemotherapy in this setting . 
 that might benefit see online for appendix vol 19 december 2018 1681 articles n the trial steering committees of both the eortc and chorus trials agreed on a strategy for database pooling and analyses ; both trials had similar eligibility criteria , treatment , and examination schedules to facilitate pooling 2 studies prospectively selected for database pooling 1220 patients records screened 670 patients enrolled in eortc 550 patients enrolled in chorus 1220 individual patient data included in synthesis ( pooled analysis ) figure 1 : prisma flow diagram eortc = european organisation for research and treatment of cancer 55971 trial . 
eortc = european organisation for research and treatment of cancer 55971 trial . table 1 : baseline characteristics , by study eligibility criteria for these trials and their study designs have been reported elsewhere.4 , 5 the appendix includes the protocols of the eortc ( pp 1270 ) and chorus ( pp 71117 ) trials . 
a list of recruiting sites and investigators is also in the appendix ( pp 122124 )  . briefly , in the eortc trial , 4 women were eligible if they had biopsy - proven figo stage iiic or iv invasive epithelial ovarian , primary peritoneal , or fallopian tube carcinoma . 
 if a biopsy specimen was not available , fine - needle aspiration showing an adeno carcinoma was acceptable under the following conditions : presence of a pelvic adnexal mass , presence of extrapelvic metastases of 2 cm or larger ( measured during dia gnostic laparoscopy or laparotomy , or if laparoscopy or laparotomy was not done , on the basis on ct findings ) , and a ratio of cancer antigen 125 ( ca125 ) to carcino embryonic antigen ( cea ) greater than 25 ; biopsy findings were mandatory for inclusion in the trial if any of these three criteria were not present . 
the size of the largest metastasis was estimated on the basis of ct imaging only in the chorus trial . in both trials , participants were randomly allocated to receive either upfront debulking surgery followed by at least six courses of platinum - based chemotherapy , three courses of neoadjuvant platinum - based chemotherapy followed by interval debulking surgery followed by at least three additional courses of platinumbased chemotherapy.4 , 5 in women allocated to receive upfront debulking surgery whose surgery was completed without optimum cytoreduction , interval debulking surgery was permitted , and these patients were included for analyses in the upfront debulking surgery group . 
in the eortc trial , randomisation used a minimisation technique and was stratified by the following factors : institution , method of biopsy ( image - guided , laparoscopy , laparo tomy , or fine - needle aspiration ) , figo stage iiic or iv disease , and largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 to 20 cm , or > 20 cm )  . 
in the chorus trial , randomisation used a minimisation method with a random element , which stratified patients according to randomising centre , largest radiological tumour size , clinical figo stage , and prespecified chemotherapy regimen . 
for details on size of residual tumour , residual tumour per country , type of surgery , number of cycles and type of chemotherapy , and time to ( re ) initiation of chemotherapy , we refer to the original reports.4 , 5 procedures our analysis was designed in 2003 by the chief investigators of the eortc and chorus trials ( iv and sk ) and members of the eortc and mrc trial managing committees , according to a formal protocol . 
we derived median follow - up with the eortc standard method , which uses the reverse kaplan - meier method and calculates time - toevents for all patients ; in the original chorus paper , however , only the median duration of follow - up for surviving patients was calculated . the primary outcome of our pooled analysis was overall survival , and the prespecified secondary endpoint was progression - free survival . 
prespecified subgroup analyses were done on the basis of stratification factors that were common to both trials : randomising centre , largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 to 20 cm , and > 20 cm ) , and clinical figo stage . 
definitions for overall survival and progression - free survival have been published elsewhere.4 statistical analysis patients data from both trials were updated and merged into one database ( database lock for eortc was on june 6 , 2015 ; for chorus , june 3 , 2014 ) , which contained 1220 patients with tubo - ovarian cancer who had been randomly allocated to receive either upfront debulking surgery or neoadjuvant chemotherapy . 
assuming a median overall survival of 3 years , this number of events allowed assessment of noninferiority , 9 , 10 with a one - sided type i error of 005 and a power of 80% , with inferiority regarded as an increase of more than 1819% in hazard . 
applying a two - sided test of superiority at 5% , the dataset would allow detection of an 18% increase in hazard with 80% power . the principal analysis was done on an intention - totreat basis . 
 in those subgroups for which the proportional hazards assumption was violated , restricted mean survival times were calculated to provide a more useful general measure than the hr estimates and their 95% cis obtained from a cox proportional hazards model to report the average survival times between the two treatment groups.11 multivariable time - to - event analyses were done using a cox proportional hazards model , with univariate screening followed by a multi variable stepwise selection procedure.12 all baseline characteristics and results were checked for homogeneity between the two studies and stratified per trial when possible . 
all analyses were done with sas , version 9.4. role of the funding source the funders of the studies had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 upfront debulking surgery neoadjuvant chemotherapy hazard ratio 076 , 95% cl 058100 overall score stratied for study , p = 0048 time after randomisation ( years ) number at risk ( number censored ) upfront debulking surgery neoadjuvant chemotherapy 118 ( 0 ) 11 ( 0 ) 53 ( 2 ) 57 ( 1 ) 13 ( 3 ) 25 ( 3 ) 7 ( 3 ) 8 ( 4 ) 2 ( 5 ) 4 ( 6 ) 0 ( 6 ) 2 ( 8 ) figure 4 : overall survival in patients with figo stage iv disease , by treatment figo = international federation of gynecology and obstetrics . overall survival of 276 months ( iqr 141513 ) and 269 months ( 127501 ) , respectively ( hr 097 , 95% ci 086109 ; p = 0586 ) , and progression - free survival of 116 months ( iqr 79177 ) and 111 months ( 64175 ) , respectively ( hr 098 , 95% ci 087110 ; p = 0688 ; figure 2 )  . 
the lower one - sided 95% cis for overall survival and progression - free survival excluded the 18% non - inferiority margin . overall survival was significantly improved in the eortc trial as compared with the chorus trial ( median 302 months [ iqr 157537 ] vs 236 months [ 105469 ] ; hr 120 , 95% ci 106136 ; p = 0004 ; figure 3 ) , but progression - free survival was similar in the two trials ( median 115 months [ iqr 80170 ] vs 109 months [ 61181 ] ; hr 096 , 95% ci 086108 ; p = 0531 ; appendix p 1 )  . 
cochrans q for heterogeneity was not significant for either overall survival ( p = 017 ) or progression - free survival ( p = 032 )  . median overall survival was significantly different for women with figo stage iv disease compared with those with stage iii and ii cancer ( median 233 months [ iqr 124408 ] vs 300 months [ 156557 ] and 454 months [ 316not reached ] , respectively ; for stage iv vs stage ii , hr 275 , 95% ci 149508 ; for stage iii vs stage ii , 192 , 95% ci 105349 ; p < 00001 for trend ; appendix p 4 )  . 
overall survival was similar with neoadjuvant chemotherapy and upfront debulking surgery in patients with stage iiic disease ( respectively , median 308 months [ iqr 165513 ] and 284 months [ 141557 ] ; hr 104 , 95% ci 090121 ; p = 0569 ; appendix p 5 )  . 
progression - free survival was also similar with neoadjuvant chemotherapy and upfront debulking surgery in patients with stage iiic disease ( median 122 months [ iqr 84183 ] and 117 months [ 75199 ] , respectively ; hr 106 , 95% ci 092122 ; p = 0429 ; appendix p 6 )  . 
however , progression - free survival was significantly better in stage iv disease with neoadjuvant chemotherapy than with upfront debulking surgery ( median 106 months [ iqr 79150 ] vs 97 months [ 52132 ] , respectively ; hr 077 , 95% ci 059100 ; p = 0049 ; appendix p 7 )  . 
additionally , in patients with stage iv tubo - ovarian cancer , neoadjuvant chemotherapy was associated with significantly better overall survival than was upfront debulking ( median 243 months [ iqr 141476 ] vs 212 months [ 100364 ] ; hr 076 , 95% ci 058100 ; p = 0048 ; figure 4 )  . 
in patients with figo stage iiic disease and a largest metastatic tumour size less than 5 cm , progression - free survival was better with upfront debulking surgery than with neoadjuvant chemotherapy ( median 122 months [ iqr 85233 ] vs 117 months [ 83164 ] ; hr 136 , 95% ci 106175 ; p = 0017 ; figure 5a ) forest plots for progression - free survival according to largest metastatic tumour size are in the appendix ( p 9 )  . 
overall survival did not differ between upfront debulking surgery and neoadjuvant chemotherapy ( median 330 months [ iqr 135787 ] and 302 months [ 165513 ] , respec t ively ; hr 126 , 95% ci 096165 ; p = 0092 ; figure 5b )  . 
 1684 vol 19 december 2018 articles age and performance status were not predictive for treatment effect on survival ( appendix p 11 ) discussion this preplanned analysis of updated data from the eortc 55971 and chorus trials assessing neoadjuvant chemotherapy versus upfront debulking surgery in advanced tubo - ovarian cancer ( stage iiic and iv ) shows that , with long - term follow - up , neoadjuvant chemotherapy results in non - inferior overall survival and progression - free survival as compared with upfront debulking surgery . 
the planned non - inferiority margin an increase in hr of more than 1819%was well outside the upper bounds of the 95% cis ( 10% and 9% for progression - free survival and overall survival , respectively )  . 
hence , this pooled analysis with long - term follow - up substantiated previous findings showing that both upfront debulking surgery and neoadjuvant chemotherapy are potential treatment options for patients with figo stage iiic or iv tubo - ovarian cancer . 
 the analysis also showed that patients diagnosed with stage iv disease had significantly better progression - free survival and overall survival with neoadjuvant chemotherapy as compared with upfront debulking surgery , whereas women with stage iiic disease with extrapelvic metastases smaller than 5 cm had significantly better progression - free survival with upfront debulking surgery as compared with neoadjuvant chemotherapy . 
our analyses showed that in women with stage iiic disease and extrapelvic metastases at diagnosis smaller than 5 cm , survival curves for both progressionfree survival and overall survival cross in both treatment groups , indicating deviation from the proportional hazards assumptions . 
obtaining tissue for histological examination is usually possible by use of image - guided biopsy ( usually of the omental cake ) , although a laparoscopic approach is necessary in some cases and provides additional information on disease distribution , which can be included in the decision - making process.1517 both the eortc and chorus trials investigated the timing of surgery in advanced tubo - ovarian cancer , but these trials have been criticised for inclusion of low proportions of patients with no macroscopic disease ( r0 ) and because patients with poor prognosis were enrolled and died sooner than expected independent of the timing of surgery . 
however , at the time the patients in these trials were enrolled , neoadjuvant chemotherapy was not accepted as an alternative to upfront debulking surgery , and furthermore most patients recruited to these trials had extensive figo stage iiic or iv disease that was visible on ct . 
moreover , the scorpion15 and jcog060218 randomised trials compared the morbidity of interval debulking surgery after neoadjuvant chemotherapy with upfront debulking surgery and concluded that interval debulking surgery was associated with improved perioperative morbidity as compared with primary debulking surgery . 
a ran domised trial of neoadjuvant chemotherapy versus primary debulking surgery in advanced tubo - ovarian cancer ( the trust trial , nct02828618 ) is recruiting only in centres with historically documented maximum cytoreduction ( r0 ) in patients with stage iii or stage iv tubo - ovarian cancer of at least 50% . 
the results of this trial are awaited . one limitation of our pooled analysis is that only patients with figo stage iiic and iv disease were included in the eortc trial , whereas in the chorus trial a few patients with stage iiia and stage iiib disease were included . 
furthermore , the number of patients with stage iiic and stage iv disease without residual tumour after upfront debulking surgery was lower in the chorus trial than in the eortc trial . application of the findings of this analysis to the care of women with figo stage iiic or iv tubo - ovarian cancer should be assessed in the context of each patients clinical picture . 
women in the eortc and chorus studies that contributed data to this analysis had metastatic disease with a high tumour burden at presentation , and many had a poor performance status.19 this clinical scenario is not uncommon , and improving outcomes for this population is as important as for patients with better prognostic factors . 
our chemotherapy should be the standard of care for most patients with figo stage iv tubo - ovarian cancer , and primary surgery should only be undertaken in these stage iv patients in exceptional circumstances with easily resectable disease . suggest data contributors all authors contributed to study design and study implementation . 
all authors have seen and approved the final version and , after consultation with the collaborators , agreed to submit for publication . declaration of interests mn reports grants from the medical research council clinical trials unit and cancer research uk , during the conduct of the study . 
 nj reports that the royal united hospital ( his employing institution ) received support from eortc for a clinical trials nurse , who obtained and verified data from some participants in the chorus trial . 
 cm reports personal fees and travel expenses from roche farma espaa , outside the submitted work ; travel expenses from astrazeneca , outside the submitted work ; and travel expenses from pharmamar , outside the submitted work . 
tp reports personal fees and non - financial support from astrazeneca , outside the submitted work ; non - financial support from roche and igea medical , outside the submitted work ; and is co - chief investigator for the icon7 trial of bevacizumab in first - line treatment of patients with advanced ovarian cancer . 
iv , cc , gbk , mkbp , te , gcj , ams , rv , wgm , pbp , gk , ac , gs , nsr , and sk declare no competing interests . acknowledgments this study was supported by grants ( 2u10 ca11488 - 28 through 2u10 ca011488 - 36 ) from the national cancer institute ; and by a donation from the vlaamse liga tegen kanker ( flemish league against cancer ) to the eortc charitable trust . 
funding for a pilot phase of the chorus trial was provided by the royal college of obstetricians and gynaecologists and was supported by core medical research council ( mrc ) clinical trials unit funding . 
the mrc was the chorus trial sponsor , which was undertaken and analysed at the mrc clinical trials unit . correction to lancet oncol 2018 ; 19 : 95364 correction to lancet oncol 2018 ; 19 : 104050 correction to lancet oncol 2018 ; 19 : e386 kramer souweidane mm , pandit - taskar n , et al . 
this correction has been made to the printed article , and to the online version as of aug 1 , 2018 . moreau p , mateos m - v , berenson jr , et al . 
lancet oncol 2018 ; 19 : 95364in the methods section of this article , the exclusion criteria for new york heart association heart failure should have been class iii or iv . 
this correction has been made to the online version as of aug 1 , 2018 . vol 19 aug 2018 e382 corrections published online january 11 , 2018 s1470 - 2045 ( 18 ) 30008 - 1 see articles page 169 breast cancer in young women : do brca1 or brca2 mutations matter ? young women with breast cancer have always caught the attention of both clinicians and researchers , despite this group being a rarity . 
additionally , the cancers might be associated with a previous pregnancy or have a pathogenesis that is based on a genetic predisposition ; some data even imply that both cancers associated with a previous pregnancy and a genetic predisposition to cancer might be directly connected.1 the posh prospective cohort study by ellen r copson and colleagues , published in the lancet oncology , 2 has contributed to the understanding of this patient population after recruiting nearly 3000 patients diagnosed with breast cancer when younger than 40 years , and capturing comprehensive data about patient , tumour , and treatment characteristics , along with extensive follow - up data . 
 copson and colleagues reported that patients with a brca1 or brca2 mutation had a similar prognosis as patients without these mutations : in 2733 women included in the analysis , overall survival at 2 years was 970% ( 95% ci 945984 ) for brca mutation carriers versus 966% ( 958973 ) for non - carriers ( hazard ratio [ hr ] 096 [ 95% ci 076122 ] ; p = 076 )  . 
additionally , in 558 patients with triple - negative breast cancer , those who had a brca mutation had better overall survival than did non - carriers at 2 years ( 95% [ 95% ci 8998 ] vs 91% [ 8894 ] ; hr 059 [ 95% ci 035099 ] ; p = 0047 ) , although there were no between - group differences at 5 years or 10 years.2 importantly , prognosis in the posh study meant survival after routine treatment for breast cancer . 
among other factors , young age is regarded as an indication for treatment with chemotherapy , because prognosis is generally considered less favourable in younger and untreated patients than in patients diagnosed at an older age.3 in the posh study , only a few patients did not receive chemotherapy.2 studies have suggested that brca1 and brca2 mutations have an effect on the efficacy of chemotherapy . 
the neoadjuvant geparsixto study , 4 which randomly assigned patients to either standard chemotherapy containing anthracycline and taxane alone or with the addition of carboplatin , showed that in patients with triple - negative breast cancer , a brca1 or brca2 mutation was associated with a higher proportion of patients achieving a pathological complete response and better survival compared with no mutation , regardless of the kind of chemotherapy used . 
in patients without a mutation , standard chemo therapy without carboplatin resulted in lower disease - free survival rates than with chemotherapy plus carboplatin.4 therefore , patients with triple - negative breast cancer and a brca1 or brca2 mutation might have a survival advantage because of the higher efficacy of systemic chemotherapy . 
although the geparsixto study was not restricted to younger patients , the population was relatively young ( mean age 48 years )  . understanding prognosis in young patients is important because patients with brca mutations are at increased risk of developing specific conditions , such as secondary cancers , including ovarian cancer , contralateral breast cancer , and de novo breast cancer in the same breast . 
with regard to contralateral breast cancers and de novo breast cancers in the same breast , copson and colleagues2 generated data that the survival benefit in the patients with triple - negative breast cancer might not have been caused by bilateral mastectomies . 
however , the evidence for this hypothesis is merely suggestive , and no formal comparison was done.2 results from retrospective analyses indicate that a bilateral mastectomy confers a benefit regarding overall survival for brca1 or brca2 mutation carriers.5 this important topic needs more prospective research as preventive surgical measures might have an effect on what might be a very long life after a diagnosis of breast cancer at a young age . 
the data from posh deliver a rationale for prospective studies to address these questions . with genotyping becoming cheaper and more accessible , studies that report on mutation frequencies always raise the question about which individuals and patients should get tested . 
however , only 182 ( 54% ) of 337 mutation carriers had been identified in routine health care.2 in most national and international guidelines , testing criteria include patients with breast cancer aged less than 35 or 40 years . 
the fact that in the posh study there were 155 young women diagnosed with breast cancer w ho did not know their mutation status raises the question of whether and when testing criteria for certain groups of patients can be allowed for lower mutation probabilities . 
 the interaction between pregnancies at a young age , other genetic causes such as predisposition genes , 6 and associated pathways such as rank / rankl1 are just some topics which could be addressed after the posh study . peter a fasching comprehensive cancer center erlangen - emn , university hospital erlangen , department of gynecology and obstetrics , friedrich - alexander university erlangen - nuremberg , erlangen , bavaria , 91054 , germany . 
 of note , amaria and colleagues6 enrolled patients with resectable palpable nodes , in - transit metastases ( stage iiic ) , or oligometastatic resectable stage iv disease , but not patients with melanomas that were difficult to resect or unresectable disease , which is often the case for neoadjuvant treatment approaches.7 moreover , patients in the neoadjuvant plus adjuvant group received both neoadjuvant and adjuvant dabrafenib and trametinib . 
 the study results were encouraging : after a median follow - up of 186 months ( iqr 146231 ) , more patients receiving neoadjuvant plus adjuvant dabrafenib and trametinib were alive without disease progression than those receiving standard of care ( ten [ 71% ] of 14 patients in the neoadjuvant plus adjuvant dabrafenib and trametinib group vs none of seven in the standard of care group ) and had longer event - free survival ( median 197 months [ 95% ci 162not estimable ] vs 29 months [ 17not estimable ] ; hazard ratio 0016 , 95% ci 000012014 , p < 00001 )  . 
 lancet oncol 2016 ; 17 : 88395in this article , the declaration of interests should read jal - m has received personal fees from reimbursement of trial - associated costs , and nonfinancial support from bristolmyers squibb . 
jb reports payments to her institution , sarah cannon research institute , from bristolmyers squibb , for the conduct of the trial ; consulting fees ( all paid to her institution and not to her personally ) from bristol myers squibb , roche , taiho oncology , amgen , genentech , merrimack , celgene , medimmune , seattle genetics , daiichi sankyo , janssen , translational drug development , five prime therapeutics , moderna therapeutics , tolero , evelo biosciences , arrys therapeutics , forma therapeutics , tanabe research laboratories , beigene , continuum clinical , and cerulean ; payments to her institution ( not to her personally ) for the conduct of clinical trials on which she served as principal investigator from abbvie , astrazeneca , emd serono , ipsen biopharma , incyte , novartis , eisai , pfizer , millennium , imclone , boston biomedical , calgb , acerta pharma , lilly , gilead sciences , leap therapeutics , macrogenics , oncomed pharmaceuticals , takeda pharmaceuticals , rgenix , novocure , merus , nv , blueprint medicine , array biopharma , armo biosciences , and agios ; jb also reports that her institution , sarah cannon research institute , conducts clinical trials and performs consulting services for several hundred companies ; the companies listed above are the ones in which jb was personally involved . 
 pao has received consulting fees from amgen and bristol - myers squibb ; and clinical trial funding from armo biosciences , bristol - myers squibb , merck , and medimmune . 
 dj has received consulting fees from definiens ag , f hoffmann - la roche ltd , curevac ag , roche pharma ag , novartis pharma ag , and novartis oncology novartis farma . 
mcp has received grant support from bristolmyers squibb to conduct this study ; personal fees from abbvie , celgene , clovis oncology , genentech , novartis ; and grants from novartis , oncomed pharmaceuticals , and stemcentrix . 
paa reports grants for research funding and personal fees for advisory / consultant role from array , bristol - myers squibb , and roche - genentech ; and personal fees for advisory / consultant role from amgen , genmab , idera , immunocore , incyte , medimmune , merck serono , msd , newlink genetics , novartis , pierre fabre , sandoz , syndax , sun pharma , sanofi , and ultimovacs . 
 lh has received research funding from astrazeneca ; served as a paid consultant for genentech and merck and an unpaid consultant for bayer , bristol - myers squibb , and xcovery ; and received lecture fees from biodesix . 
je has received grant support from astrazeneca , basilea pharmaceutica , bayer , bristol - myers squibb , celgene , clovis , daiichi sankyo , eisai , e - therapeutics , glaxosmithkline , gilead , immunocore , merck , otsuka , roche / genentech , tc biopharm , verastem , and vertex ; and served on advisory boards for and received honorarium payable to the institution from baxter , bayer , bristol - myers squibb , celgene , clovis , eisai , glaxosmithkline , immunova , karus therapeutics , otsuka , roche / genentech , tc biopharm , and transgene / jennerex . 
 ec reports research grants and / or financial support from boehringeringelheim , roche / genentech , bms , novartis , psioxus , nanobiotix janssen , abbvie , pharmamar , puma , sanofi , lilly , pfizer , merck , nektar , amcure , amgen , astrazeneca , principia , bayer , cytomx , h3 , incyte , kura , loxo , macrogenics , menarini , merck serono , merus , millenium , rigontec , tahio , and beugene tesaro ; consultancy fees from janssen - cilag , alkermes ( and travel expenses ) , seattle genetics , pierre fabre , cerulean pharma , eusa , celgene , novartis ( speakers bureau ) , nanobiotix , psioxus therapeutics , abbvie , astrazeneca , g u i d e p o i n t g l o b a l , ro c h e / genentech ( and travel expenses ) , glg , pfizer , servier , amcure , and boehringer - ingelheim ; ownership from start ( leadership ) , oncoarts associated , and international cancer from consultants ; employment start and hm hospitals group ( honoraria ) ; and president and founder of npo foundation intheos ( investigational therapeutics oncological sciences ) , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . vol 20 february 2019 corrections correction to lancet oncol 2017 ; 18 : e35463 correction to lancet oncol 2018 ; 19 : 87100 correction to lancet oncol 2018 ; 19 : 25766 oconnor oa , lue jk , sawas a , et al . 
 for lancet oncol 2017 ; 18 : e35463 in this review , the second sentence of the abstract should read additional improvements have been reported in three phase 3 colon cancer trials when oxaliplatin was added to fluoropyrimidines , the effect was mainly on disease - free survival . 
this correction has been made to the online version as of feb 28 , 2018 although women fulvestrant johnston s , lee ks , et di leo a , al . 
buparlisib plus with postmenopausal her2hormone - receptor - positive , negative , advanced breast cancer progressing on or after mtor inhibition ( belle - 3 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
in the results section , the following sentence should have read in the 11 ( 13% ) cases of discordance , a pik3ca wild - type tumour sample and pik3ca - mutated ctdna were reported in three ( 4% ) patients and pik3ca mutations detected in the tumour sample but not in ctdna ( 9% ) patients . 
these corrections have been made to the online version as of feb 28 , 2018 . seven vol 19 march 2018 e137 corrections correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections editorial to read more about the lancet oncologys cancer campaign and the four commissions go to campaigns / cancer / for our previous editorial on direct - to - consumer marketing see lancet oncol 2008 ; 9 : 1113 tackling the cancer epidemic rising cancer is the primary cause of death in many countries , now exceeding heart disease . 
in lower income countries , fast , creating unprecedented incidence challenges for health systems , many of which were designed in an era that did not foresee , were simply incap able of pre - empting , or knowingly ignored the future . 
 however , these remarkable achievements come at a pricethe cost of care is outpacing national budgets , the numbers of cancer patients and survivors are putting greater pressures on health - care systems , and increasing numbers of vulnerable patients from less traditional demographics , such as children and younger adults , require di erent clinical solutions that have yet to be fully conceived . this month , the lancet oncology launches a campaign focused on tackling the cancer epidemic at a systems level . 
we will document , via monthly updates , the evolution of four commissions intended for publication later this year that aim to de ne the scale of the challenge , the underlying drivers , and the improvements needed to cancer - care systems . 
these special reports will cover global access to radiotherapy , surgical resource availability and its fundamental role in cancer treatment , the intersection of primary care in a comprehensive cancer service t for the 21st century , and the ongoing oncology requirements in the low - to - middle income countries of latin america . 
 the lancet oncology dangers of direct - to - consumer advertising exposed again direct - to - consumer ( dtc ) advertising is in the headlines agaon feb 19 , 2015 , 23andme was granted approval by the us food and drug administration ( fda ) to market a genetic test for bloom syndrome . 
and on feb 25 , 2015 , the us federal trade commission ( ftc ) ned two companies for marketing melanoma detection apps ( melapp and mole detective ) and banned them from making misleading or unsubstantiated health claims in the future . 
 the decision to permit 23andme limited access to the dtc market is a remarkable turnaround for a company that on nov 22 , 2013 , received an fda warning letter instructing them to stop all marketing . 
at that time , the fda insisted the company seek approval for each speci c indi cation in their pan - genomic test along with robust evidence for each claimin line with the requirements for other over - the - counter home - use tests . 
despite the seeming appro priate ness of the decision , it creates an uneasy precedentone that could open the door to other less reliable tests if the delineations of the ruling are not rmly upheld . 
these concerns are further underscored by the jnci article showing that websites promoting person alised cancer medicine products contain more information about the bene ts than the limitations , and most focus on one or more non - standard tests . ensuring people take an active interest in their health is central to a strong health - care system , but health - care decisions need to be a bilateral process between patients and their doctors . 
in our december , 2008 , editorial , we con cluded that the marketing of tests should be restricted to health professionals , rather than the lay public , and only accessed through health - care providers on the basis of their advice . 
 the lancet oncology vol 16 april 2015 corrections published online march 25 , 2015 s1470 - 2045 ( 14 ) 71115 - 5 correction to lancet oncol 2013 ; 14 : e374 correction to lancet oncol 2015 ; 16 : e163 correction to lancet oncol 2015 ; 16 : 447 , 448 weller m , p ster sm , wick w , hegi me , reifenberger g , stupp r . 
the rst sentence should read : exposure to passive smoke among never smokers does not seem to increase the chances of acquiring somatic mutations in genes linked to non - small - cell lung cancer in smokers , a new study shows . 
 vorinostat in patients with advanced malignant pleural mesothelioma who have progressed on previous chemotherapy ( vantage - 014 ) : a phase 3 , double - blind , randomised , placebocontrolled trial . 
lancet oncol 2015 ; 16 : 44756in the a liation section , p bass should be listed at netherlands in the funding cancer section in the summary and in the a liations , merck & co has been changed to merck & co , inc . 
 lancet oncol 2015 ; 16 : 54149in the key of gure 2 of this article , the boxes should indicate patients who were ct positive for disease , not those who were circulating tumour dna positive for disease . 
this correction has been made to the online version as of april 30 , 2015 , and the printed version is correct . vol 16 may 2015 e199 comment avoiding potential systemic toxic e ects . 
 tg - 4010 was delivered concurrently with standard chemotherapy to augment the immune response.8 finally , a biomarker based on baseline concentrations of activated natural killer cells was validated to further select the population likely to respond to the vaccine . there are many hurdles for successful anticancer vaccination.9 an appropriate tumour - speci c antigen must be delivered to dendritic cells , which must have received suitable activation signals to allow processing and presentation of the antigen . 
even if all the necessary steps for successful t - cell activation occur , the stimulated t cells must track to the tumour microenvironment where they must overcome the many immunosuppressive mechanisms used by tumour cells to avoid t - cell recognition . 
as suggested by ribas , 10 the paradigm has shifted from e orts to stimulate the immune response to one of releasing the brakes of the negative regulation of t cells . 
rs reports personal fees , nonnancial support , and travel support from boehringer - ingelheim , personal fees and travel support from astrazeneca , personal fees from p zer and roche , nonnancial support from lundbeck , and travel support from bristol - myers squibb and merck , all outside the submitted work . brahmer j , reckamp kl , baas p , et al . 
magrit : a double - blind , randomised , placebo - controlled phase iii study to assess the e cacy of recmage - a3 + as15 cancer immunotherapeutic as adjuvant therapy in patients with resected mage - a3 - positive non - small cell lung cancer ( nsclc )  . 
tecemotide ( l - blp25 ) versus placebo after chemoradiotherapy for stage iii non - small - cell lung cancer ( start ) : a randomised , double - blind , phase 3 trial . 
tg4010 immunotherapy and rst - line chemotherapy for advanced non - small - cell lung cancer ( time ) : results from the phase 2b part of a randomised , double - blind , placebo - controlled , phase 2b / 3 trial . 
 132 vol 17 february 2016 comment one randomised trial ( hortis ) , 1 in which hyperbaric oxygen therapy is compared with sham treatment in 120 evaluable patients with chronic radiation - induced proctitis , included crossover of patients who had sham treatment to hyperbaric oxygen therapy shortly after completion of initial treatment . 
 results of a small , randomised study2 of hyperbaric oxygen therapy versus argon plasma coagulation for patients with radiation proctopathy suggested a better and faster response with argon plasma coagulation than with hyperbaric oxygen . 
sucralfate enemas and antibiotics are other therapies for radiation proctitis with some evidence of e cacy.3 systematic assessment and treatment of chronic radiation - induced bowel dysfunction using comprehensive management algorithm , 4 has proven to be effective in a randomised trial.5 this algorithm suggests the use of hyperbaric oxygen therapy for patients with rectal bleeding . 
however , the authors of two systematic reviews6 , 7 of hyperbaric oxygen therapy for patients with radiation - related tissue injuries concluded that evidence was too limited and that more clinical trials were needed to assess both its long - term benefit and cost - effectiveness.8 in the lancet oncology , mark glover and colleagues9 report the results of the randomised hot2 trial of hyperbaric oxygen therapy versus sham treatment for patients with chronic bowel dysfunction after pelvic radio therapy . 
with changes in the bowel component and rectal bleeding score of the inflammatory bowel disease questionnaire from baseline to 12 months after start of treatment set as the primary endpoint measures , the investigators found no evidence of a benefit from hyperbaric oxygen therapy . is the standardised analysis and treatment guided by the royal marsden algorithm for all included patients , ensuring that patients with other causes of bowel symptoms were excluded and given relevant led to a treatments . 
this approach might have highly selected study population of patients with long - lasting , difficult symptoms , but these are the typical patients who would qualify for referral for hyperbaric oxygen therapy . the negative results of the hot2 trial are disappointing for clinicians and patients who hoped for proof of efficacy of hyperbaric oxygen therapy , a form of therapy that is often tried as a last resort . 
 the results are especially relevant with respect to the burden that undergoing hyperbaric oxygen therapy can be for patients ( at least 68 weeks of daily treatments , with risk of [ transient ] vision changes and ear problems ) and for health - care providers , given the significant cost of hyperbaric oxygen therapy . the mechanism by which hyperbaric oxygen therapy is thought to promote the repair of damaged tissue is by restoring oxygen tension , which stimulates angiogenesis and improves tissue function in chronic hypoxic , atrophic , fibrotic , and damaged mucosal tissue . 
one of the secondary endpoints in the hot2 trial was photographic evidence of changes in images of rectal mucosa taken through flexible sigmoidoscopy ; assessment of this endpoint would have added essential information about the degree of tissue healing and allowed a direct assessment response to hyperbaric oxygen . 
 of changes the question remains whether the results of the hot2 trial should be understood as hyperbaric oxygen therapy having a transient and too weak an effect on the atrophic and vulnerable mucosa to result in measurable improvement or whether the results seem to refute the putative mechanism by which oxygen therapy is thought to promote tissue healing . mark glover and colleagues are to be applauded for the sham - controlled study design and 12 - month follow - up long - awaited confirmatory trial of the efficacy of hyperbaric oxygen therapy in this setting . 
the strength of this study in what has been a the results of the hot2 trial do , however , give compelling and urgent rationale for more well designed trials of hyperbaric oxygen therapy . 
random assignment of patients with chronic radiation - induced bowel dysfunction to a clinical vol 17 february 2016 comment published online december 18 , 2015 s1470 - 2045 ( 15 ) 00555 - 0 see articles page 234 sham treatment is difficult , whereas a comparison of hyperbaric oxygen therapy to other treatment approaches might be more acceptable and enable larger trials . 
2045 ( 15 ) 00461 - 1 . alectinib in crizotinib - resistant , alk - positive nsclc intensively investigated molecular targets the discovery of molecular drivers of carcinogenesis has resulted in a large - scale shift in thinking about cancer lung treatment . 
advanced non - small - cell cancer ( nsclc ) once judged a fairly homogenous entity and managed uniformly with chemotherapy is now perceived as a conglomerate of various molecular subtypes that need di erent treatments . 
alk - rearranged ( alk - positive ) disease comprises about 45% of all cases of nsclc and is characterised by frequent metastatic spread to the pericardium , pleura , liver , and cns . 
moreover , penetrance of crizotinib through the bloodbrain barrier is poor , resulting in modest e cacy in combating or preventing brain clinical activity of metastases.2 next - generation alk inhibitors , which have the ability to bypass resistance mutations and penetrate the bloodbrain barrier , ful l an unmet clinical need . in the lancet oncology , alice shaw and colleagues3 present results of a phase 2 trial assessing alectinib , a new alk inhibitor , in 87 patients with advanced nsclc who had previously received crizotinib treatment . 
notable activity of this compound was reported : an objective response was achieved by 33 ( 48% , 95% ci 3660 ) of 69 patients with measurable disease at baseline according to an independent and median progression - free survival was 81 months ( 95% ci 62126 )  . 
more than half the patients had brain metastases at enrolment ( 52 [ 60% ] of 87 ) , almost two - thirds of whom had received previous brain response is noteworthy ( 21 [ 40% ] patients to alectinib achieved an objective response , including 13 [ 25% ] who achieved a complete response ) because few radiotherapy . 
the committee , intracranial review 134 vol 17 february 2016 corrections correction to lancet oncol 2012 ; 13 : 817 , 818 , 822 correction to lancet oncol 2014 ; 15 : 1195206 correction to lancet oncol 2015 ; 16 : 52 shen q , fan j , yang x - r , et al . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . vol 16 january 2015 for the clinical oncology society australia position statement on exercise in cancer care see au / media / 332488 / cosaposition - statement - v4 - webfinal.pdf exercise and cancer treatment : balancing patient needs on may 7 , 2018 , the clinical oncology society of australia launched a position statement recommending that exercise should be prescribed to all patients with cancer as part of their treatment regimen . 
the statement which has been endorsed by 25 leading health and care organisations , including the cancer council australia , the medical oncology group of australia , and the australian physiotherapy association , and echoes similar guidelines by cancer research uk and the american college of sports medicinesays that exercise should be viewed as an adjunct to therapy to help counteract the adverse effects of cancer and its treatment . 
although the decision is a welcome move that increasingly recognises patient quality of life as a vital component of cancer care , two crucial questions remain : does the evidence base adequately support the decision , and can such an approach be suited to the diverse range of cancer types and patients who are inflicted with the disease ? it is no surprise that much epidemiological evidence in recent years has shown that , with improvements in early detection and treatment , increasing numbers of patients with cancer can expect to be alive 5 years after their diagnosis and join a growing population of cancer survivors . 
although these trends are encouraging and show that improvements in cancer treatment , prevention , and detection have translated into real improvements in survival outcomes , it cannot go unrecognised that the disease and its treatment are often associated with longterm health and psychosocial sequelae . 
these sequelae most often increased fatigue , fear of recurrence , and diminished personal relationships , as well as an increased risk of developing secondary malignant diseases and other conditions , such as cardiovascular disease , diabetes , and osteoporosis , compared with the general population . 
given such evidence , it would be no hard push to declare that those with cancer are a vulnerable population with distinct health - care needs , of which exercise will , of course , help alleviate some of these competing conditions . include depression , anxiety , although the clinical oncology group of australia statement emphasises that patients should be physically active as much as their abilities and conditions allow , it would be naive to think that there can , or should , be a one - size - fits - all approach to suit all patients . 
for example , patient comorbidities and fragility , which are often associated with increased age , are factors that need to be adequately considered when recommending the feasibility of any physical activity regimen . 
equally , a degree of sensitivity is needed in , first , recommending physical activity measures that do not shame patients into thinking their disease is solely the consequence of their lifestyle choices and , second , recognising that exercise is not necessarily the single and vital factor determining treatment success , but rather emphasising it as a way to improve quality of life and wellbeing . 
on a practical level , recommendations will need to be given within the context of a patients life , in recognition of the often - debilitating effects of chemotherapy , surgery , and radiotherapy that might otherwise prevent patients from participating in exercise , a home and work life that might already be hard pressed to find time for exercise , and the need for an appropriate support network to encourage exercise as a feasible and sustainable treatment option . moreover , caution is needed when looking at the evidence base that informed these recommendations . 
 although epidemiological evidence has shown that being physically active can provide a protective effect against cancer recurrence , cancer - specific mortality , and all - cause mortality for some types of cancer , no evidence to date has evaluated whether the effects of exercise can positively affect cancer survivalalthough there are several clinical trials underway assessing exercise as a treatment intervention . 
indeed , despite having what seems like an insufficiently robust evidence base to inform a strong move in either direction , it is hugely encouraging to see that treatment interventions that focus on a patients quality of life and wellbeing are being seriously into the patient experience , and that incorporated exercise is now considered a vitally important component of cancer care at both ends of the care pathwayboth as a treatment and as a preventive measure . interventions that increasingly incorporate quality of life , the patient experience , and cancer survivorship into the treatment programme are welcome and laudable ways to ensure that patients are at the centre of the treatment process . 
but like any therapy , physical activity measures should be personalised to adequately meet a patients physical and psychological needs , and be delivered in such a way to support exercise as a viable and supportive treatment intervention . 
 the lancet oncology vol 19 june 2018 editorial correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections articles immunogenicity and hpv infection after one , two , and three doses of quadrivalent hpv vaccine in girls in india : a multicentre prospective cohort study rengaswamy sankaranarayanan , priya ramesh prabhu , michael pawlita , tarik gheit , neerja bhatla , richard muwonge , bhagwan m nene , pulikottil okuru esmy , smita joshi , usha rani reddy poli , parimal jivarajani , yogesh verma , eric zomawia , maqsood siddiqi , surendra s shastri , kasturi jayant , sylla g malvi , eric lucas , angelika michel , julia butt , janki mohan babu vijayamma , subha sankaran , thiraviam pillai rameshwari ammal kannan , rintu varghese , uma divate , shila thomas , geeta joshi , martina willhauck - fleckenstein , tim waterboer , martin mller , peter sehr , sanjay hingmire , alka kriplani , gauravi mishra , sharmila pimple , radhika jadhav , catherine sauvaget , massimo tommasino , madhavan radhakrishna pillai , for the indian hpv vaccine study group summary background an increase in worldwide hpv vaccination could be facilitated if fewer than three doses of vaccine are as e ective as three doses . 
we originally aimed to compare the immunogenicity and frequency of persistent infection and cervical precancerous lesions caused by vaccine - targeted hpv after vaccination with two doses of quadrivalent vaccine on days 1 and 180 or later , with three doses on days 1 , 60 , and 180 or later , in a cluster - randomised trial . 
 suspension of the recruitment and vaccination due to events unrelated to our study meant that some enrolled girls could not be vaccinated and some vaccinated girls received fewer than the planned number of vaccinations by default . 
participants were unmarried girls aged 1018 years vaccinated in four cohorts : girls who received three doses of vaccine on days 1 , 60 , and 180 or later , two doses on days 1 and 180 or later , two doses on days 1 and 60 by default , and one dose by default . 
the primary outcomes were immunogenicity in terms of l1 genotype - speci c binding antibody titres , neutralising antibody titres , and antibody avidity after vaccination for the vaccine - targeted hpv types 16 , 18 , 6 , and 11 and incident and persistent infections with these hpvs . 
4348 ( 25% ) girls received three doses , 4979 ( 28% ) received two doses on days 1 and 180 or later , 3452 ( 19% ) received two doses at days 1 and 60 , and 4950 ( 28% ) received one dose . 
immune response in the two - dose hpv vaccine group was non - inferior to the threedose group ( median uorescence intensity ratio for hpv 16 112 [ 95% ci 102123 ] and for hpv 18 104 [ 092119 ] ) at 7 months , but was inferior in the two - dose default ( 033 [ 029038 ] for hpv 16 and 051 [ 043059 ] for hpv 18 ) and one - dose default ( 009 [ 008011 ] for hpv 16 and 012 [ 010014 ] for hpv 18 ) groups at 18 months . 
fewer than three doses by design and default induced detectable concentrations of neutralising antibodies to all four vaccine - targeted hpv types , but at much lower concentration after one dose . 
cervical samples from 2649 participants were tested and the frequency of incident hpv 16 , 18 , 6 , and 11 infections was similar irrespective of the number of vaccine doses received . 
the testing of at least two samples from 838 participants showed that there was no persistent hpv 16 or 18 infections in any study group at a median follow - up of 47 years ( iqr 4251 )  . interpretation despite the limitations imposed by the suspension of the hpv vaccination , our ndings lend support to the who recommendation of two doses , at least 6 months apart , for routine vaccination of young girls . 
the shortterm protection a orded by one dose of hpv vaccine against persistent infection with hpv 16 , 18 , 6 , and 11 is similar to that a orded by two or three doses of vaccine and merits further assessment . funding bill & melinda gates foundation . copyright 2015 international agency for research on cancer ; licensee elsevier . 
 introduction persistent infection with a high - risk hpv causes cervical cancer , and worldwide 6882% of cervical cancers are attributed to hpv types 16 and 18.14 prophylactic vaccines containing recombinant virus - like particles assembled from the l1 capsid proteins of hpv 16 and 18 ( bivalent vaccine ) and hpv 6 , 11 , 16 , and 18 ( quadrivalent vaccine ) are used in hpv vaccination programmes . 
one and two doses of the bivalent hpv vaccine have been shown to protect against cervical hpv 16 and 18 infections as e ectively as three doses in women aged 1525 years . 
in a randomised trial , two doses of quadrivalent hpv vaccine given 6 months apart to girls aged 913 years resulted in a non - inferior immune response at 1 month after the last dose compared with three doses given to girls aged 913 years and to women aged 1626 years on day 1 , 2 months , and 6 months . 
 we searched pubmed and medline for full - length articles published between jan 1 , 2008 , and june 30 , 2015 , using the keywords hpv vaccination , less than three doses , alternate doses , one dose , two doses , three doses , immunogenicity , hpv infection , cervical intraepithelial neoplasia , clinical trials , randomised trials , follow - up studies ; we also searched clinicaltrials.gov for ongoing clinical trials of fewer than three doses of the hpv vaccine . 
we assessed all potentially relevant articles and found that neither the immunogenicity after one dose of quadrivalent hpv vaccination nor the extent of protection against hpv 16 and 18 infections a orded by fewer than three doses of quadrivalent hpv vaccine has been reported . added value of the study our ndings con rm that two doses of quadrivalent hpv vaccine , administered with an interval of 180 days or more , are immunologically non - inferior to the three - dose schedule and a ord protection against incident and persistent hpv 16 , 18 , 6 , and 11 infection that is similar to that a orded by three doses . 
 we also report the rst evidence to our knowledge that one dose of quadrivalent hpv vaccine induced detectable titres of hpv neutralising antibodies and that lower vaccine - induced antibody concentrations after one dose of quadrivalent hpv vaccine provide similar protection against vaccine - targeted hpv infections compared with the higher antibody concentrations induced after two or three doses . implications of all the available evidence our preliminary results suggest that future trials of hpv vaccines should include a single - dose arfurther long - term follow - up of vaccinated women in our study will clarify whether protection afforded after one dose of quadrivalent hpv vaccine is long - lasting . 
administration of three doses of hpv vaccine , or two doses as recommended by who , remains a challenge , and if one dose proves to be as efficacious as more doses , vaccine uptake will be improved and costs will be reduced . 
data on immunogenicity , durability of antibody response , and the frequency of persistent infection after one dose of vaccine will expedite the introduction of hpv vaccination in national immunisation programmes . 
 the e cacy of three doses of vaccine ( either bivalent or quadrivalent ) against high - grade cervical intraepithelial neoplasia caused by vaccine - targeted hpv was almost 100% in hpv - naive populations and greater than 55% in the intention - to - treat populations.13 the administration of three doses of the hpv vaccine , or even two doses as recommended by who , 4 , 5 is a challenge , and if one dose was as e ective as two or three doses then vaccine uptake would increase greatly and costs would be reduced . 
the high immune response in pre - adolescent girls given three doses suggests that reductions in dose number could prevent cervical neoplasia.6 , 7 data on immunogenicity , durability of antibody response , and frequency of persistent infection after one dose will enable the swift introduction of hpv vaccination in national immunisation programmes . 
 in 2009 , we initiated a cluster - randomised trial in india to compare the e ectiveness of two doses versus three targeting hpv doses of a quadrivalent vaccine types 16 , 18 , 6 , and 11 , in preventing cervical neoplasia . 
 however , recruitment and vaccination of the girls in the trial was suspended midway due to events unrelated to our study , which meant that some enrolled girls could not be vaccinated and some vaccinated girls received fewer than the planned number of vaccinations by default . 
here , we describe the immuno genicity and infection results after suspension of vaccination . immune methods study design and participants we initiated a multicentre , cluster - randomised trial in india on sept 1 , 2009 , to nd out whether two doses of quadrivalent hpv vaccine would be as e ective in inducing non - inferior preventing persistent vaccine - targeted hpv infection and cervical neoplasia as three doses . 
we recruited unmarried girls who were ambulant and in good general health aged 1018 years , living in 188 geographical clusters in nine locations in india ( osmanabad , dindigul , pune , mumbai , ahmedabad , delhi , hyderabad , gangtok in sikkim , and aizawl in mizoram )  . 
we obtained a new written informed consent from girls who became 18 years old during follow - up . procedures the vaccine used was the quadrivalent hpv vaccine ( gardasil ; merck sharp & dohme , whitehouse station , nj , usa )  . 
girls were originally randomly assigned to the two - dose group with vaccination on days 1 and 180 ( or later ) or the three - dose group with vaccination on days 1 , 60 , and 180 ( or later ) by the statistician at the international agency for research on cancer ( iarc )  . 
also using the computer - generated random allocation , the two groups in each study site were then randomly assigned to the two - dose group or the threedose group . 
vaccinations occurred from study start until april 8 , 2010 , when the indian authorities suspended all further recruitment and vaccination of girls in all hpv vaccination trials in india because of events unrelated to our study . 
the suspension meant that we had four groups of girls who were vaccinated : those on days 1 , 60 , and 180 or later ( original three - dose group ) ; those on days 1 and 180 or later ( original two - dose group ) ; those on days 1 and 60 by default ( two - dose default group ) ; and those with one dose only by default ( one - dose default group )  . at each study site , dedicated health workers and nurses were recruited and trained to identify and interview eligible girls for sociodemographic and reproductive information , explain the study to the participating girls and their parents or guardian , obtain informed consent , administer the vaccines , record adverse events , and do follow - up procedures , including obtaining blood and cervical cell samples . 
participants could contact a study clinician if they needed urgent medical attention using a 24 - h telephone help line . each participant was visited every year by a health worker or nurse in her household to enquire about her general health and wellbeing . 
details about marriage , medically signi cant events , pregnancy , antenatal and postnatal events , delivery , and migration were gathered and documented through the household visits , a network of social workers , medical - care providers , hospitals , and relatives . 
samples were treated with edta and analysed with luminex ( austin , tx , usa ) based multiplex serology8 , 9 to assess the concentration of binding antibodies against the major capsid protein l1 of hpv 16 , 18 , 6 , and 11 as mean median uorescence intensity ( mfi ; appendix )  . 
mfi values as a measure of antibody concentration quanti ed by use of hpv multiplex serology are directly comparable with optical densities measured with elisa8 and mfi values for hpv 16 in natural and vaccine - induced hpv 16 - speci c antibody responses are strongly correlated with endpoint the neutralisation assay.9 seropositivity cuto s for seroconversion were calculated for each hpv type , based on the mfi values of serum samples obtained from the participants at baseline after allowing for 5% seropositivity in the total baseline samples . 
the hpv genotyping method involved hpv - type - speci c e7 pcr bead - based multiplex genotyping.10 , 11 the multiplex hpv - type - speci c e7 pcr uses hpv type - speci c primers targeting the e7 region for the detection of 19 high - risk or probable highrisk hpv types ( 16 , 18 , 26 , 31 , 33 , 35 , 39 , 45 , 51 , 52 , 53 , 56 , 58 , 59 , 66 , 68a , 68b , 70 , 73 , and 82 ) , and two low - risk hpv types ( 6 and 11 ) , with detection limits ranging from ten to 1000 copies of the viral genome . 
the method was validated at the rajiv gandhi centre for biotechnology ( rgcb ; thiruvananthapuram , india ) under the supervision of scientists from iarc and the cervical cell samples were tested at rgcb . 
we de ned incident infections that persisted for 12 months or longer without an hpv negative test ( for the hpv type in question ) between the positive tests as persistent infections . immunological assays and hpv testing were done at rgcb , where a dedicated laboratory was established with technology transfer and external quality assurance from the german cancer research centre ( dkfz ; heidelberg , germany ) and the infections and cancer biology group at iarc ( lyon , france )  . 
scientists from rgcb were trained at dkfz , and the multiplex serology hpv - l1 antibody assays were done at rgcb by trained personnel , masked to the number of vaccine doses received by participants , under the technical supervision of experts from dkfz . outcomes the primary outcomes were immunogenicity outcomes : the hpv - l1 genotype - speci c binding antibody concentrations using geometric mean mfi , antibody avidity induced after vaccination using the geometric mean avidity index , and antibody concentrations speci c for neutralising epitopes in hpv - l1 using geometric mean neutralisation titres ( gmts ) ; and infection outcomes : rst incident and persistent infections of vaccinetargeted hpv types accumulated during follow - up . 
 cervical cells were taken 6 months after delivery or 18 months after marriage , whichever was earlier , and annually thereafter for 3 consecutive years . for the hpv - l1 binding antibodies outcome , we compared the geometric mean mfis at day 1 for all participants , at 7 months ( 1 month after the last dose ) , 18 months , 36 months , and 48 months after the rst dose of vaccination in the three - dose group versus the two - dose group , and at 18 months and 36 months after the rst dose vol 17 january 2016 articles of vaccination in the two - dose default and one - dose default groups versus the three - dose group . 
for the 12 - month comparison , the mfis in the one - dose default group were compared with those in the two - dose default group because other dose regimens were not measured at that timepoint . 
for the antibody avidity outcome , the geometric mean avidity indices were compared at 7 months for the two - dose and three - dose groups and at 18 months for all vaccination groups . 
for the neutralising antibody outcome , we compared the gmts at 18 months for hpv 16 , 18 , and 6 l1 in the two - dose , two - dose default , and one - dose default groups with those in the three - dose group . the secondary outcomes were cross - protection against non - vaccine targeted high - risk hpv types : rst incident and persistent non - targeted high - risk hpv infections accumulated during follow - up . the study will be monitored and assessed over 20 years . 
 long - term outcomes , such as the frequency of cervical intraepithelial neoplasia grades 2 and 3 and invasive cancer , will be assessed by screening of participating women and using data from population - based cancer registries . statistical analysis we aimed to recruit 20 000 girls from nine locations in india ( 7000 girls from osmanabad , 3000 each from dindigul , pune , and mumbai , 1000 each from ahmedabad , delhi , and hyderabad , and 500 each from gangtok in sikkim , and aizawl in mizoram ) , with 10 000 girls living in 100 clusters randomly allocated to the two - dose group and 10 000 girls in 88 clusters to the three - dose group . 
to test for non - inferiority of antibody concentrations in di erent dose groups , we used log - transformed mean mfis in linear regression models to obtain mfi ratios and their corresponding 95% cis . 
in keeping with other hpv immunogenicity studies , non - inferiority of a vaccination group was concluded if the lower bound of the 95% ci for its mfi ratio was greater than 05.1214 in a post - hoc power calculation , using the lowest limit of 95% ci with a sample size of 40 individuals per group , we had 90% power for non - inferiority testing between each of the observational groups and the three - dose group . the antibody avidity index was calculated by dividing the mfi values of urea - treated samples by the mfi values of the untreated samples and multiplied by 100% . 
 to compare the fewer than three - dose regimens with the three - dose regimen , log - transformed avidity index values were used in linear regression models to obtain avidity index ratios and their 95% cis . 
non - inferiority of the fewer than three - dose regimens to that of the three - dose regimen was concluded if the 95% ci lower bound of the avidity ratio index was greater than 05 . 
non - inferiority of the gmt was concluded if the 95% ci lower bound of the neutralisation gmt ratio was greater than 05 . hpv 16 l1 antibodies 10 000 hpv 18 l1 antibodies three - dose group two - dose group two - dose default group one - dose default group seropositivity cuto hpv 6 l1 antibodies hpv 11 l1 antibodies 1000 10 000 1000 7 or 12 * 7 or 12 * time after rst dose ( months ) time after rst dose ( months ) figure 2 : mean mfi values for hpv types 16 , 18 , 6 , and 11 l1 antibodies dashed lines show the threshold ( cuto ) values for seroconversion . 
 * mfi values for month 7 were used for the three - dose and two - dose vaccine groups , whereas mfi values for month 12 were used for the two - dose default and one - dose default groups . 
 vol 17 january 2016 articles hpv 16 l1 hpv 18 l1 hpv 6 l1 hpv 11 l1 three doses t w o doses three doses t w o doses , default t w o doses one dose , default three doses t w o doses three doses t w o doses , default t w o doses one dose , default month 7 month 18 month 7 month 18 sample time ( months ) and number of doses received figure 3 : box plots of the avidity index of mfi for hpv types 16 ( a ) , 18 ( b ) , 6 ( c ) , and 11 ( d ) l1 antibodies at 7 months and 18 months after the rst dose mfi = median uorescence intensity . 
for this reason , all regression analyses were adjusted for the cluster design by specifying the option in the regression models that allows the variance - covariance estimator to include the clustering e ect . hpv infection outcomes are reported as frequencies of the detection of rst incident infection and persistent infections of vaccine - targeted and non - targeted high - risk hpv infections accumulated during the follow - up . for both the primary and secondary outcomes , analysis was done per the actual number of vaccine doses a participant received . 
other than the donation of the vaccines , merck did not have any role in design , protocol development , study conduct , monitoring , and assessment , analysis of data , or writing of the report . 
the corresponding author had full access to all the data in the study and all the authors had nal approval for the decision to submit . results vaccination of eligible girls was initiated on sept 1 , 2009 , and continued until april 8 , 2010 . 
of the 21 258 eligible girls identi ed for recruitment in the 188 clusters , 17 729 ( 83% ) from 178 clusters were vaccinated at least once : 4348 ( 25% ) girls received three doses on days 1 , 60 , and 180 or later ( three - dose group ) ; 4979 ( 28% ) received two doses on days 1 and 180 or later ( two - dose group ) ; 3452 ( 19% ) received two doses on days 1 and 60 by default ( two - dose default group ) ; and 4950 ( 28% ) received one dose by default ( one - dose default group ; gure 1 ; appendix )  . 
the baseline characteristics of participants in the four groups show more or less similar age distribution , whereas we noted some di erences in average monthly household income and education ( table 1 )  . 
local and systemic reactions within 15 days of administering 34 856 vaccine doses in the study included injection - site pain ( number of reactions ; n = 1092 ) , low - grade fever ( n = 293 ) , injectionsite swelling ( n = 64 ) , headache ( n = 49 ) , nausea ( n = 30 ) , skin rash ( n = 15 ) , diarrhoea ( n = 13 ) , abdominal cramps ( n = 13 ) , and fainting attacks ( n = 10 )  . 
the mfi results of the hpv - l1 binding antibody analyses are in the for seroconversion for hpv 16 , 18 , 6 , and 11 l1 were 100 , 41 , 240 , and 48 , respectively . 
analysis of 625 plasma samples ( 308 in the three - dose group and 317 in the two - dose group ) obtained at month 7 for peak hpv - l1 binding antibody concentrations indicated that all girls in both groups had seroconverted and almost all girls in the twodose group had mfis equal to or higher than the lowest mfi in the three - dose group for all four vaccine - targeted hpv types ( appendix )  . 
the peak antibody concentrations at 7 months for vaccine - targeted hpv types in the twodose cohort were non - inferior to the mfis in the threedose group ( appendix )  . 
mfi ratios for the two - dose versus three - dose group were 112 ( 95% ci 102123 ) for hpv 16 l1 , 104 ( 092119 ) for hpv 18 l1 , 104 ( 097113 ) for hpv 6 l1 , and 112 ( 106119 ) for hpv 11 l1 . the hpv - l1 binding antibody concentrations for the vaccine - targeted hpv types were similar for the threedose and two - dose groups over 48 months ( gure 2 ; appendix )  . 
the antibody concentrations in the two - dose vaccine group had similar decay kinetics and were noninferior to those in the three - dose group at 7 months , 18 months , 36 months , and 48 months , over the 48 - month period ( appendix )  . 
at least 124 ( 98% ) of 127 girls in the two - dose group had antibody concentrations equal to or greater than the lowest antibody mfi in the three - dose group at 48 months ( appendix )  . 
 the hpv - l1 binding antibody concentrations for the vaccine - targeted hpv types in the two - dose default and one - dose default groups were inferior to the concentrations in the three - dose group at 18 months and 36 months . 
 at month 36 , the number of samples analysed was 271 in the three - dose group , 513 in the two - dose default group , and 510 in the one - dose default group ( appendix )  . 
at 36 months , 511 ( > 99% ) of 513 girls in the two - dose default group and 462 ( 91% ) of 510 the one - dose default group had antibody concentrations equal to or higher than the lowest mfi value in the three - dose group ( appendix )  . 
there was no correlation between age and antibody titres in the onedose default group ( correlation coe cient = 0067 )  . the values for geometric mean avidity index for hpv types 16 , 18 , 6 , and 11 after the two - dose schedule at 7 months and after the two - dose , two - dose default , and one - dose default schedules at 18 months , were noninferior to the value after the three - dose regimen . 
 for example , the avidity index ratio of the one - dose default group compared with the three - dose group for hpv 16 l1 was 110 ( 95% ci 101119 ; gure 3 ; appendix )  . the gmts of neutralising antibodies to hpv types 16 and 6 at 18 months after the rst dose in the two - dose group were non - inferior to the gmts in the three - dose group , but were inferior for hpv 18 . 
the gmt ratio of hpv 16 l1 neutralisation titres was 100 ( 95% ci 069145 ) for the two - dose group compared with the three - dose group , whereas for hpv 18 l1 neutralisation titres , it was 042 ( 027065 ) for the two - dose group compared with the three - dose group ( gure 4 ; appendix )  . 
 the gmt after the two - dose default and one - dose default schedules for hpv types 16 , 18 , and 6 were inferior to the gmt of the three - dose group ( gure 4 ; appendix )  . 
the gmt ratio of hpv 16 l1 neutralisation titres was 023 ( 016034 ) for the two - dose default group compared with the three - dose group . the median time between rst vaccination and rst cervical sample collection from 2649 participants was 39 years ( iqr 3047 )  . 
the medians were 41 years ( iqr 3348 ) for the three - dose group , 43 years ( 3348 ) for the two - dose group , 37 years ( 2946 ) for the two - dose default group , and 37 years ( 2945 ) for the one - dose default group . 
in 838 women for whom two or more samples were available for analysis , there were no persistent hpv 16 and 18 infections in any of the four study groups at a median follow - up of 47 years ( iqr 4251 ; table 2 )  . 
higher frequencies of persistent vaccine non - targeted hpv infections were noted in the four study groups as compared with vaccine - targeted hpv infections . discussion our ndings suggest that two doses of quadrivalent hpv vaccine , administered with an interval of 180 days or more between doses , are immunologically non - inferior to the three - dose schedule and a ord protection against incident and persistent hpv 16 , 18 , 6 , and 11 infections that is similar to that a orded by three doses . 
 * incident hpv infections with no subsequent sample to assess persistence . table 2 : incident hpv infection and hpv infection status frequency of hpv types 16 and 18 infections range from 3% to 9%.2023 in this context , our initial results provide new evidence that one and two doses of quadrivalent vaccine prevent incident and persistent cervical infections with hpv types 16 , 18 , 6 , and 11 , similar to the protection a orded after a three - dose schedule during a median follow - up of 47 years ( iqr 4251 )  . to our knowledge , our study is the rst in which immunogenicity and vaccine - targeted hpv infection frequencies are reported after one dose of quadrivalent vaccine . 
although the antibody concentrations after one dose were lower than those in the two - dose and three - dose groups , the titres were stable and the mean avidity index after one dose was non - inferior to that after three doses . 
one - dose vaccination also induced detectable titres of neutralising antibodies to all four vaccine - targeted hpv vol 17 january 2016 articles types in most of the participants that were assessed , but at a much lower concentration . 
there is no known minimum threshold concentration of antibodies that is protective ; seroconversion is an arbitrary cuto and does not represent the minimum threshold for protection.1 , 24 our immunogenicity ndings after three and two doses of vaccine are consistent with the results from a canadian randomised trial25 in which 261 girls aged 913 years were allocated to vaccine with three doses of quadrivalent vaccine at day 1 , 2 months , and 6 months ; 259 girls also aged 913 years were allocated to vaccine with two doses at day 1 and 6 months ; and 310 women aged 1626 years were allocated to vaccine with three doses also at day 1 , 2 months , and 6 months . 
the antibody concentrations for all four vaccine - targeted hpv types in the girls aged 913 years given two doses were non - inferior to those in women aged 1626 years who received three doses during a 36 - month period . 
our results suggest that the low vaccine - induced antibody concentrations after one dose a ord similar protection against vaccine - targeted hpv infections as the high antibody concentrations from two or three doses during a median follow - up of 47 years ( iqr 4251 )  . 
the similar frequency of incident nonvaccine hpv types in each dose group ( table 2 ) implies that hpv exposure was similar across the di erent groups and participants sexual behaviours were not related to the number of doses received . 
a follow - up of these women is planned over 20 years to assess the e cacy endpoints for the incidence of cervical intraepithelial neoplasia grades 2 and 3 and invasive cervical cancer caused by vaccine - targeted and non - targeted hpv types in the di erent dose groups by screening of participating women and using data from populationbased cancer registries . 
we have also recruited and are following up an age - matched and residence - matched cohort of unvaccinated women ( n = 1540 )  . the protection a orded by virus - like particle vaccines is believed to be mediated by neutralising antibodies leading produced by plasma cells , 31 , 32 most of which have short in peak antibody to declines lifespans , concentrations within a few months . 
 concentrations of antibodies measured 1218 months after the last dose of a virus - like particle vaccine generally represent the activity of long - lived plasma cells and are the best predictors of antibody persistence . the patterns of antibody responses after one dose of vaccine in our study and in the costa rica and patricia trials27 , 30 seem to be similar to the pattern after a live attenuated vaccine , which usually a ords long - lasting protection . 
the stable antibody response after one dose of the hpv l1 vaccine might be due to the structure of the hpv - like particles and the antigens it displays to the immune system might eliminate the need for doses after the priming dose.27 , 33 , 34 notably , in a cohort study35 in which girls aged 1024 years and women received three doses ( n = 98 252 ) , two doses by default ( n = 112 555 ) , and one dose by default ( n = 119 046 ) of the quadrivalent vaccine , the incidence rate ratios for the occurrence of condylomas were 018 , 029 , and 031 , respectively , implying that one dose and two doses with a short interval were associated with signi cant reduction in condyloma risk compared with 926 119 unvaccinated women . due to the disruption of recruitment and randomisation because of the suspension of vaccination midway in our planned two - arm randomised trial , our study has essentially become an observational cohort study of participants in four dose groups with similar socio demographic characteristics . 
vaccination was suspended in our study in response to instructions from the indian council of medical research in the context of all hpv vaccination studies in india pending an enquiry into the causes of death of ve girls ( subsequently proven unrelated to hpv vaccination ) recruited for an hpv vaccination demonstration project in the states of andhra pradesh and gujarat . 
major limitations include the non - randomised comparison of the vaccination dose groups , an absence of memory b - cell response data , limitations in interpreting early results for girls given incomplete dose schedules , and biases that might have been introduced after vaccination interruption and loss of randomisation . 
despite these limitations , our study of hpv vaccination is representative of generalisable real - world conditions : it had varying dose schedules and a broad age range of participants in addition to the di culties and challenges inherent in running hpv vaccination studies in low - income and middle - income countries . 
moreover , the inclusion of sexually naive girls aged 1018 years ( the primary and secondary target age groups for vaccination ) , the possibility of long - term followup , and the technology transfer that allowed validated and quality assured execution of antibody assays and hpv genotyping and the resultant independence in assessing outcomes without having to rely on pharmaceutical industry laboratories or laboratories abroad are important strengths of our study . vol 17 january 2016 articles our preliminary results after one dose of quadrivalent vaccine by default , although promising , should be interpreted with caution and suggest that future trials of hpv vaccines should include a single dose arfurther longterm follow - up of vaccinated women in our study will clarify lasting protection after one dose . 
because of the programmatic advantages of one dose in terms of cost savings , logistics , and coverage , and the high proportion of participants who default after immunisation programmes , particularly in developed countries , 36 , 37 assessment of the clinical e cacy of a single dose is of substantial public health signi cance . 
a single dose of hpv vaccine , providing strong and sustained protection against hpv infection in the long term , is the best way to overcome the barriers to vaccine uptake globally . 
 the rst dose our ndings support the who recommendation to use two doses separated by 6 months or more for vaccination of young girls , and indicate that a single dose of the hpv vaccine merits further assessment . contributors rs had the initial idea for the study , and was responsible for the conception , design , and conduct , monitoring , and supervision of the study , and acquisition , analysis , and interpretation of the data . 
tg was a co - investigator , and was responsible for the overall supervision of the laboratory analyses of the cervical cell samples , and technology transfer to sta from the indian central laboratory . 
nb was the study representative for the indian authorities on behalf of all participants ; she was responsible for the on - site conduct of the study in delhi , participated in monitoring , supervision , acquisition , and interpretation of the data , and the provision of clinical services at the study site . 
bmn and sgm were responsible for the on - site conduct of the study in barshi , poe in ambilikkai , sj in pune , urrp in hyderabad , pj in ahmedabad , yv and ms in sikkim , ez and ms in mizoram , and sss , gm , and sp in mumbai , and they participated in the monitoring , supervision , acquisition , and interpretation of the data , and the provision of clinical services at their respective study sites . 
establishment of the luminex - based assays at rgcb was partly supported by the european commission - seventh framework programme grant hpv - ahead ( fp7 - health - 2011 - 282562 )  . 
 we thank the bill & melinda gates foundation for their generous nancial support without which this study would not have been possible ; peter dull ( integrated clinical vaccine development , bill & melinda gates foundation ) for his valuable support , encouragement , and advice ; merck sharp dohme for donation of hpv vaccines for use in the study ; current and past members of the data safety monitoring board : lynette denny , lutz gissmann , peter sasieni , thangarajan rajkumar , doreen ramogola - masire , raul murillo , the late arun p kurkure , and rolando herrero for their valuable advice and monitoring of the study safety and outcomes ; jan agosti ( formerly at bill & melinda gates foundation and now at the university of seattle ) for her valuable support , encouragement , and advice ; union for international cancer control for the award of international cancer technology transfer fellowships that helped technology transfer and quality assurance for immunogenicity and hpv genotyping studies at rgcb ; the district administrative , civic , education , and health authorities , and medical practitioners in the districts of india where the study sites are located for their cooperation , facilitation , and assistance in implementing the study ; the study participants , their parents , families , and legal guardians for their understanding , cooperation , excellent and continuing participation in the study , and follow - up procedures despite the challenges and misinformation after suspension of hpv vaccination ; our eld sta at our project sites in india and scientists and technicians at rgcb and at dkfz for their tremendous e ort and dedication ; christopher p wild , walter prendiville , and partha basu ( all iarc ) for their valuable suggestions on a draft version of this manuscript ; and evelyn bayle and krittika guinot ( both iarc ) for their help in preparing this manuscript . corrections correction to lancet oncol 2015 ; 16 : 1338 correction to lancet oncol 2015 ; 16 : e434 bagcchi s . 
lancet oncol 2015 ; 16 : e434in this news item , the fourth sentence of the third paragraph should read patients with ccnd1 mutations had worse 2 - year overall survival than those without ( 381% [ 95% ci 14100 ] vs 80% [ 7684 ] ; p = 0005 ) ; similar outcomes were noted with alterations in the dna repair pathways ( tp53 , atm , atr , and znfhx4 mutations )  . 
triage by methylation - marker testing versus cytology in women who test hpvpositive on self - collected cervicovaginal specimens ( prohtect - 3 ) : a randomised controlled non - inferiority trial . 
lancet oncol 2015 ; 16 : 133543in this article , the title of figure 2 should have been kaplan - meier analysis of cumulative incidence of leukaemia for children with or without enterovirus infection after accounting for death as the competing risk . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . correction to lancet oncol 2015 ; 16 : 1289 lokody , i . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the fourth paragraph on liver transplants for patients with high risk hcc has been changed to read : of these , 17 had a liver transplant . 
the 5 - year survival of these patients was superior to those high risk patients that did not have a liver transplant ( 82% vs 38% ; p = 0033 )  . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . vol 16 october 2015 e480 infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
 lancet oncol 2015 ; 16 : 1143the last line of the rst paragraph of this comment should read only this year , for example , did who add several commonly used , extremely e ective drugs , such as imatinib , trastuzumab , and cisplatin to its list of essential medicines . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the paragraph on survival with oligometastatic hcc should read the researchers found that patients with oligometastatic disease had a significantly longer overall survival than patients with extensive disease ( 104 months versus 63 months , p = 0034 )  . 
 vol 16 november 2015 e528 editorial for the lancets health in the arab world series see health - in - the - arab - world for more on qatars cancer plans see health - care development lancet oncol 2012 ; 13 : e50108 addressing the burden of cancer in the gulf on oct 2123 , 2014 , a meeting to discuss how to tackle the growing burden of cancer in the gulf region was held in riyadh , saudi arabia . 
this increase is due , in part , to longer lifestyle habits lifespans and adoption of western ( eg , greater use of tobacco ; consumption of high - fat , lowbre diets ; and greater physical inactivity )  . 
the countries that form the gulf corporation council ( gcc ) saudi arabia , united arab emirates , bahrain , oman , qatar , and kuwaitare expected to be at the higher end of these predictions for the region , while also being faced with a high burden of infectious diseases . 
the meeting culminated in a declaration to be submitted for endorsement by the executive board of the health ministers council for the gcc states , which listed areas in need of attention and called on member states to reduce cancer mortality by 25% between 2015 and 2025 . 
but can this ambitious target be achieved ? although gcc countries cannot be described as being of low - to - middle incomethey are perhaps more accurately described as industrialisingthey share many of the same barriers to universal health care that face developing countries . 
at a systems level , inadequate registration of cancer incidence and death prevents an accurate measure of the burden of the disease , thus hindering proper planning of national and regional cancer - control programmes . 
region - speci c research is clearly needed to better understand the di erences in underlying tumour biology that , for instance , result in about half of cancers in the region presenting at an early age , and to investigate why the pattern of malignancies diagnosed in the gulf di ers from that elsewhere ( eg , haematological malignancies , particularly non - hodgkin lymphomas , are very common in the gcc , possibly as a result of the high prevalence of consanguineous marriages in the region )  . 
some countries , such as qatar , have taken useful steps forward with the launch of a national cancer strategy and a national cancer research strategy , but such action is not universal . 
additionally , primary care is generally geared towards acute care rather than chronic diseases , whereas in terms of secondary care , cancer treatment facilities are limited in number and of variable quality . 
however , where funding exists , it must be used wiselyeg , is there really a need to build four proton therapy facilities in saudi arabia when the country has only half the required number of linear accelerators for its population ? at the population and patient level , cultural barriers and educational issues , which together contribute to poor awareness of the disease and of health care in general , must be addressed . 
access to essential palliative drugs is restricted in the region , a situation that is unjusti able , particularly given that most cancers present late and in non - curable stages . 
lastly , the provision of universal health care in all gulf countries should be mandatory : health is a human right , and the rights of all patients to both treatment and psychosocial support are paramount . 
 the disproportionate distribution of wealth in the region is a substantial hurdle to accessing care for a large part of the population , which hinders e orts towards universal care . implementation plan it is heartening that the riyadh meeting discussed many of these issues in depth . 
once the meetings declaration is endorsed by the gcc health ministers , it is of the utmost importance that a detailed devised with speci c means , quanti able milestones , and speci c timelines set out to meet the pledge to reduce cancer mortality in line with who directives . 
hopefully , this unique opportunity to transform words into rm action in the gulf states will not be missed and the region will be able to work together strategically to deliver good quality cancer care for all . 
 the lancet oncology vol 15 december 2014 1407 for the jamia study on medication - related clinical decision support alert overrides see j am med inform assoc 2017 ; published oct 27 . 
this somewhat ironic paradoxin which more drugs are being pushed through to the market , only to be bottlenecked through a system that relies on an automated system of prescriptionhas potentially conflicting consequences . 
on the one hand , physicians are encouraged to offer a variety of choice to the patient , but , on the other , they are exhausted by what is commonly called alert fatigue , in which their clinical expertise is overshadowed by an automatic system that apparently knows better . 
although the jamia study found that a large proportion of physicians overrode warnings because evidence suggested that the patient would not suffer from any adverse reactions , the situation does call into question whether a reliance on digital systems , such as those used for e - prescribing , underminesor at least challengesa level of expertise that can only be gained from the day - to - day experience of a doctor . 
from data analytics to artificial intelligence , to predictive modelling and machine learning , we are now seeing these systems being incorporated into all aspects of health , including those found in oncology . 
although big data offers the promise of easing workflows , ensuring treatment adherence according to guidelines , the analysis of large datasets , maintenance of a centralised records system , improving diagnostic accuracy , and monitoring disease or drug safety surveillanceall of which could be hugely beneficial for the future of health careclearly a delicate balance is needed when integrating those promises into the clinical decision - making process . 
in the case of detecting malignancies , it is now becoming increasingly difficult to refute that big data can help identify highrisk populations with ever - improving accuracy , observe trends in cancer incidence , and predict cancer rates long before such patterns can be detected by those methods used in conventional screening protocols . 
moreover , integrating data into health systems can have substantial financial advantages by reimbursement charges and potentially decreasing the overall cost of care . improving however , these advantages need to be offset against the potential difficulties that such new technological advances might bring . 
automated workflows need to be balanced against ease of use and delivered in a way that doesnt encumber workflows to those who are already under severe pressure and time constrained ; data analysis should be promoted in ways that help facilitate training and safeguard against otherwise unknown sideeffects without fostering an attitude that encourages laziness or poor judgement ; and , most crucially , we need to ensure that patients data remain private and secure , while enabling its aggregation in a de - identified manner to help support analytical tools that can help benefit the wider population . 
although new technologies might provide us with the tools and resources to fight health inequity , increase access , identify new targets for difficult - to - treat diseases , and help improve public health , our enthusiasm must be tempered against the always present reality of a doctorpatient relationship in which experience will always be key . despite the potential dangers , digital clinical decision tools are undeniably helpfulthey not only ensure that evidence - based medicine is practised , but guarantee a more consistent service that can be delivered to all by enforcing an approach that is based on guidelines . 
 but , just like any skill , a physicians craft must be developed and honed through practice ; it can only ever be augmented by digital health , not perfected by it . 
the art of medicine is based on judgement , as well as data , and the balancing of these two somewhat conflicting modes of medicine will be a difficult task in years to come . 
in the meantime , we must promote both schools of thought and not champion one over the other , to ensure that we provide patients with the best possible medical judgement . 
we aimed to identify risk factors for the extent of ovarian damage in women with hodgkins lymphoma treated with different chemotherapy regimens to inform accurate advice on options for fertility preservation . methods we recruited female participants from the randomised phase 3 rathl trial , aged 1845 years , based on availability of participants at recruiting sites in the uk . 
the rathl trial key inclusion criteria were histologically confirmed classic hodgkins lymphoma , stage iibiv or iia with adverse features ( bulky disease or more than two sites of involvement ) , no previous treatments , and a performance status of 03 . 
as part of rathl , participants were treated with two cycles of doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) or avd followed by an interim pet - ct scan . 
participants who had negative interim scans ( pet score of 1 to 3 according to the lugano classification ) were randomly assigned ( 1 : 1 ) by use of minimisation , stratified by interim pet score and study centre , to continue abvd or avd for four more cycles . 
participants with positive scans ( pet score of 4 or 5 ) were escalated to treatment with bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone ( beacopp - 14 or escalated beacopp ) for four cycles . 
for the protocol - driven prospective cohort substudy , ovarian function was assessed before treatment , during chemotherapy , and then annually for 3 years by use of serum antimllerian hormone and follicle - stimulating hormone measurements . 
at 1 year after chemotherapy , antimllerian hormone concentrations recovered to a median of 105 pmol / l ( iqr 43173 ) in the abvd - avd group , but little recovery was seen after beacopp ( median 011 pmol / l [ 007020 ] )  . 
 age also affected the extent of ovarian function recovery , with antimllerian hormone recovery in participants aged 35 years or older in the abvd - avd group to 37% ( sd 10 ) of their before treatment concentrations , compared with full recovery to 127% ( sd 12 ) in those younger than 35 years ( p < 00001 )  . 
follicle - stimulating hormone recovery to less than 25 iu / l occurred for 95% of women younger than 35 years in the abvd - avd group by 2 years and was also dependent on age ( hazard ratio 049 , 95% ci 037065 ; p < 00001 )  . interpretation reduced recovery of ovarian function observed in women older than 35 years treated with abvd or avd compared with younger women indicates that treatment could reduce their reproductive lifespan and supports discussion of fertility preservation before treatment . 
these findings warrant further investigation in large , prospective studies with fertility and reproductive lifespan as outcomes . funding medical research foundation and cancer research uk . copyright 2018 the author ( s )  . 
systemic treatment from chemotherapy regimens based on alkylating agents , which had a high risk of infertility and premature ovarian condition has evolved this for insufficiency in women , to treatment with doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) , which is the current treatment of choice for many adult patients with hodgkins lymphoma . 
both age and ovarian reserves before treatment are predictive of ovarian recovery after chemotherapy with some regimens , but their importance is unknown for treatments for patients with hodgkins lymphoma . added value of this study we found that changes in antimllerian hormone concentration could distinguish between the effects of treatment on ovarian function with doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) or avd , and bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone ( beacopp ) in patients with advanced hodgkins lymphoma , particularly from 3 years of follow - up after chemotherapy . 
treatment with abvd or avd was confirmed to have little gonadotoxcity in female patients with hodgkins lymphoma who were younger than 35 years at diagnosis ; however , in older patients ( 35 years ) recovery of ovarian function was affected by age . 
we found that among older women baseline concentrations of antimllerian hormone did not affect recovery , so reduced hormone recovery in older women was not due to the age - related decline in ovarian reserve . 
little recovery in ovarian function was seen after treatment with beacopp in women of all ages , although a similar number of pregnancies was observed in the two treatment groups . 
due to the small size of the cohorts analysed , these results warrant further confirmation . implication of all the available evidence the absence of detectable ovarian damage after treatment with abvd or avd in younger women with hodgkins lymphoma is reassuring , although longer follow - up is needed in future studies for a full assessment of potential reproductive effects . 
 the finding of reduced ovarian recovery in older women with hodgkins lymphoma treated with chemotherapy indicates that age - specific discussions and consideration of fertility preservation procedures should be considered before treatment . 
these considerations are of growing importance given the increasing age at which women are having children in developed countries . intensification could benefit patients who are at higher risk of relapse , and some clinicians advocate treatment with bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone ( beacopp ) for patients with advanced stage or high - risk early stage disease . 
however , female gonadal toxicity is high with dose - escalated beacopp resulting in amenorrhoea ( a surrogate marker of pre mature ovarian insufficiency ) in about 95% of patients older than 30 years.3 analysis of the effects of cancer therapies on the ovaries requires consideration of both the degree of loss of ovarian function during chemotherapy and changes in ovarian function thereafter . 
the degree of loss of the primordial follicle pool ( the ovarian reserve ) during chemotherapy is the most important effect since it determines the potential for any recovery of ovarian function and fertility , and subsequent age at menopause , although the degree of loss cannot be assessed in vivo . 
the full eligibility criteria for the rathl trial are available in the protocol . for this prospective cohort substudy , women and aged 1845 years ( ie , premenopausal ) were actively recruited from rathl sites in the uk ( appendix pp 35 )  . 
the protocol for the substudy is available online . this cohort substudy received centralised ethical committee approval that covered all sites ( national research ethics service , southampton and south west hampshire ) and all participants gave written informed consent . procedures in the rathl study , after initial staging and a baseline pet - ct scan , participants were treated with two cycles of abvd , intravenously , on days 1 and 15 of a 28 days cycle followed by an interim pet - ct scan ( doses and schedule in the appendix [ p 2 ] )  . 
participants who had negative interim scans by central review ( pet score of 1 to 3 per lugano criteria ) were randomly assigned ( 1 : 1 ) by the cancer research uk and university college london cancer trials centre using minimisation , with stratification according to pet score ( 1 , 2 , or 3 ) and centre , to continue abvd ( intravenously , days 1 and 15 ) or to receive doxorubicin , vinblastine , and dacarbazine ( avd ; intravenously , days 1 and 15 ) for four more cycles . 
participants with positive scans ( pet score of 4 or 5 ) were escalated to either beacopp - 14 for six cycles of 14 days or escalated beacopp for four cycles ( doses and schedule in the appendix [ p 2 ] )  . 
neither patients nor study staff were masked to allocation . ovarian function was assessed by use of serum concentrations of antimllerian hormone in participants enrolled into this substudy and follicle - stimulating hormone concen trations from all eligible participants ( women and aged 1845 years ) from the rathl trial . 
oestradiol measurements are necessary for the identification of women with premature ovarian insufficiency.11 during the rathl trial , blood samples were taken before any treatment , after two cycles of initial abvd treatment , at the end of chemotherapy , and at 1 , 2 , and taken after 3 years after chemotherapy . 
follicle - stimulating hormone measure ments were done locally as part of the rathl trial ; additional samples from participants enrolled in this substudy were taken to measure antimllerian hormone , follicle - stimulating hormone , luteinising hormone , and oestradiol concen trations by use of roche elecsys assays ( automated cobas e 411 1330 vol 19 october 2018 articles analyser , roche , burgess hill , uk )  . 
the substudy samples were sent by post to a central laboratory ( mrc centre for reproductive health , edinburgh ) , where the serum was stored at 20c until analysis . 
the antimllerian hormone assay has a limit of detection of 007 pmol / l , and for all assays the interassay and intra - assay coefficients of variation were below 5% . 
a follicle - stimulating hormone threshold of more than 25 iu / l indicated probable premature ovarian insuffi ciency.11 after recovery from chemotherapy , antimllerian hormone was additionally analysed in association with predictors from before treatment , specifically age and antimllerian hormone concentration . 
the study was not designed to assess fertility , and menstrual bleeding was not recorded since it does not help to distinguish between women with normal ovarian function and those with very depleted ovarian reserves . data on previous pregnancy or use of hormonal contraceptives were only collected from participants enrolled in the ovarian function substudy . 
decisions regarding fertility preservation procedures were between the participant and the local centre , and were not recorded as part of the study . outcomes the primary outcome of this study , specified as an exploratory outcome in the rathl trial , was assessment of gonadal function . 
the prespecified outcomes in this substudy were analysis of acute toxic effects of each treatment regimen on the ovaries , and ovarian function after treatment ( including progression to ovarian failure and recovery of ovarian function )  . 
other prespecified outcomes were the association between fertility after treatment and ovarian function before treatment , degree of acute ovarian toxic effects , which will be reported separately . statistical analysis as a secondary analysis of the rathl trial , the prespecified exploratory analyses presented here are not powered ; we aimed to recruit as many patients as possible while the rathl trial was open . 
we hypo thesised that antimllerian hormone concentrations could show differences between the gonadotoxicity of the chemo therapy regimens in the rathl trial , both during and after treatment , and that concentrations of antimllerian hormone before treatment would be predictive of recovery of ovarian function after treatment . 
we analysed antimllerian hormone and follicle - stimulating hormone concentrations in the ovarian subgroup after log transformation using anova with bonferronis multiple comparisons test for changes during treatment and recovery . 
 * one patient in this group had a missing performance status . table : baseline characteristics 4 ( 2% ) 4 ( 2% ) 4 ( 2% ) concentration of antimllerian hormone against percentage hormone recovery ( calculated as [ concentration at 2 yearsconcentration before treatment ] x 100 ) and against concentration at 2 years . 
we measured time to recovery ( follicle - stimulating hormone concentration of 25 iu / l ) from the end of treatment until the first follicle - stimulating hormone measurement of 25 iu / l or less , or a reported pregnancy ( whichever came first )  . 
patients with follicle - stimulating hormone concentrations of more than 25 iu / l at baseline were excluded , and patients who had neither event were censored at the last reported follicle - stimulating hormone measurement . 
 beacopp = bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone . hazards using schoenfeld residuals , and when it did not hold we used restricted mean survival times with a 3 year cutoff . 
all p values are two - sided and a p value of less than 005 was considered statistically significant . data analyses were done in stata ( version 15.1 ) and graphpad prism 7 . 
the corresponding author had final responsibility for the decision to submit for publication . results between dec 13 , 2010 , and dec 19 , 2012 , participants from the rathl trial were recruited for this ovarian function substudy ( figure 1 ; appendix p 3 )  . 
seven ( 10% ) of 74 registered participants were excluded from the substudy and the main trial , six for scan protocol deviations , and one for psychological reasons , leaving 391 ( 94% ) of 415 eligible ( 1845 years ) female rathl participants , of whom 321 ( 82% ) were evaluable for follicle - stimulating hormone analyses , and 67 ( 91% ) were evaluable for substudy analyses . 
of the 67 evaluable participants for the substudy analyses , 24 ( 36% ) had been treated with abvd , 33 ( 49% ) with avd , four ( 6% ) with beacopp - 14 , and six ( 9% ) with escalated beacopp . 
no difference in baseline hormone concentrations were found between treated with abvd versus avd , or partici pants beacopp - 14 versus escalated beacopp ( table ) ; thus these subgroups were combined as abvd - avd ( n = 57 ) and beacopp ( n = 10 ) , respectively , for subsequent analyses . 
the baseline characteristics of the participants who had follicle - stimulating hormone measurements from the rathl trial , and the combined abvd - avd and beacopp subgroups evaluated in this substudy are in the table . for nine participants in the substudy , data at postbaseline timepoints were not available because of disease progression and further treatment ( six in the abvd - avd group , three in the beacopp group ) , and 13 blood samples were missing or taken at incorrect timepoints . 
 eight blood samples taken from eight women during pregnancy in the ovarian subgroup were excluded from analysis . antimllerian hormone concentrations decreased in all participants during chemotherapy treatment with reciprocal increases in follicle - stimulating hormone concentrations ( figure 2 )  . 
in the abvd - avd group , concentrations of antimllerian hormone decreased from a median of 98 pmol / l ( iqr 59181 ) before treatment to 17 pmol / l ( iqr 0443 ) at the end of treatment ( p < 00001 ) , with a small rise between cycle two of initial abvd treatment and the end of treatment ( p < 00001 )  . 
after chemotherapy in the abvd - avd group , concentrations of antimllerian hormone increased to 105 pmol / l ( iqr 43173 ) at 1 year , similar to concentrations before treatment , with no change at later timepoints ( figure 2 )  . 
antimllerian hormone was undetectable in two ( 4% ) of 56 participants at the end of treatment with follicle - stimulating hormone concentration higher than 25 iu / l and low oestradiol insufconcentrations ficiency . 
for one of these participants , antimllerian hormone became detectable during recovery , and for the other , antimllerian hormone showed a transient recovery at 1 year after treatment , becoming undetectable thereafter . indicating premature ovarian 1332 vol 19 october 2018 articles 0 in the beacopp group , concentrations of anti mllerian hormone decreased from a median of 68 pmol / l ( iqr 22128 ) before treatment to 008 pmol / l ( 007024 ) at the end of treatment ( p < 00001 ; figure 2 )  . 
after treatment , by contrast with participants in the abvd - avd group , concentrations of antimllerian hormone showed very little recovery ( median 011 pmol / l [ iqr 007020 ] at 1 year ) and were undetectable in five ( 71% ) of seven participants at 3 years ( figure 2a )  . follicle - stimulating hormone concentrations had generally reciprocal changes compared with concentrations of antimllerian hormone and increased during treatment in both groups ( figure 2b )  . 
 concentrations of luteinising hormone showed the same pattern of changes , increasing from before treatment to the end of treatment in both groups ( both p < 00001 ) and then recovering after treatment to before - treatment concentrations in the abvd - avd group , but remaining significantly increased after treatment in the beacopp group ( data not shown )  . in women both antimllerian hormone concentration 2 years after treatment and follicle - stimulating hormone recovery data provide evidence of the effect of age on ovarian treated with abvd or avd recovery ( figures 3 and 4 )  . 
we saw a correlation between the concentration of antimllerian hormone before treatment and at 2 years after treatment ( r = 089 ; p < 00001 ) but not with antimllerian hormone recovery ( r = 030 ; p = 0051 )  . 
 however , significant and similar negative correlations were seen between age and antimllerian hormone concentrations at 2 years ( r = 040 ; p = 00055 ) and with antimllerian hormone recovery ( r = 040 ; p = 00080 )  . 
analysis of antimllerian hormone concentrations before treatment grouped by whether they were below or above the overall median value ( 977 pmol / l [ iqr 59181 ] ) showed that recovery was similar between the two groups ( below 123% [ sd 21 ] vs above 103% [ sd 9 ] ; p = 085 )  . 
 multiple linear regression analysis also confirmed that age had a significant effect on antimllerian hormone recovery ( = 043 ; p = 0004 ) , but that antimllerian hormone con centrations before treatment did not have an effect on hormone recovery ( = 015 , p = 030 )  . 
 r = 089 ; p < 00001 r = 030 ; p = 0051 antimllerian hormone before treatment ( pmol / l ) antimllerian hormone before treatment ( pmol / l ) r = 040 ; p = 00055 r = 040 ; p = 00080 age ( years ) age ( years ) figure 3 : correlations of antimllerian hormone recovery and before treatment hormone concentrations or age for the abvd - avd group panels show scatter plots of baseline hormone concentration versus concentration at 2 years ( a ) and versus percentage hormone recovery ( b ) , and age versus hormone concentration at 2 years ( c ) and percentage hormone recovery ( d )  . 
each dot shows antimllerian hormone concentration or recovery ; recovery was calculated for each participant as the concentration at 2 years after treatment as a proportion of the concentration before treatment . 
 thus , although overall concentrations of antimllerian hormone after treatment seem to recover to before treatment concentrations , the degree of recovery is restricted by increasing age . we also assessed the degree and timecourse of recovery of ovarian function , as indicated by normalisation of follicle - stimulating hormone concentrations , in the evaluable participants from the rathl trial ( figure 4 )  . 
folliclestimulating hormone measurements after treat ment were available from 321 women in the rathl trial , with a median follow - up ( censoring at recovery ) of 593 months ( iqr 419609 )  . 
follicle - stimulating hormone concentration recovery to 25 iu / l or lower was seen in 270 ( 96% ) of 282 of participants treated with abvd or avd , compared with 26 ( 67% ) of 39 treated with beacopp - 14 or escalated beacopp ( hazard ratio [ hr ] 037 , 95% ci 025056 ; p = 00001 )  . 
evaluable female participants ( n = 391 ) were divided by chemotherapy regimen received : abvd or abvd followed by avd ( abvd - avd group ) , and abvd followed by beacopp - 14 or escalated beacopp ( beacopp group )  . 
 kaplan - meier estimates for participants treated with abvd or avd were 75% ( 95% ci 7080 ) 1 year after treatment and 93% ( 8995 ) 2 years after treatment , whereas the estimates for those treated with beacopp were 33% ( 2052 ) 1 year after treatment and 69% ( 5284 ) 2 years after treatment . 
the relative difference in ovarian function ( between abvd or avd and beacopp ) did not differ when analysed by age ( < 35 years , hr 038 , 95% ci 023062 ; p = 00001 vs 35 years , hr 040 , 019083 ; p = 0011 )  . 
this pattern was also found when analysed by use of restricted mean survival ( recovery ) times ( < 35 years , 1546 days for abvd or avd and 4465 days for beacopp [ difference : 2919 days , 95% ci 16344204 ; p < 00001 ] vs 35 years , 3615 days for for abvd or avd and 6634 days for beacopp [ difference 3019 days , 95% ci 9415097 ; p = 0005 ] )  . 
however , age seemed to affect time to recovery among these participants , with a smaller proportion of those aged 35 years or older showing recovery at both 1 year ( 41 [ 50% ] ) and 2 years ( 64 [ 79% ] ) after treatment than those younger than 35 years did ( 176 [ 79% ] at 1 year and 211 [ 95% ] at 2 years after treatment ; hr 049 , 95% ci 037065 ; p < 00001 )  . 
 thus , the kaplan - meier estimates for follicle - stimulating hormone concentration recovery for those younger than 35 years treated with abvd or avd were 83% ( 95% ci 7788 ) at 1 year and 96% ( 9398 ) at 2 years compared with estimates for those aged 35 years and older of 54% ( 4366 ) at 1 year and 83% ( 7391 ) at 2 years . 
we saw no difference in follicle - stimulating hormone recovery between participants treated with escalated beacopp or beacopp - 14 for all ages ( hr 072 , 95% ci 033156 )  . in the rathl cohort , 64 ( 16% ) of 391 participants were recorded as having 81 pregnancies . 
in the subgroup cohort , antimllerian hormone measurements were available within the follow - up period for six women who became pregnant in the abvd - avd group and two in the beacopp group . 
at 1 year after chemotherapy , con centrations of antimllerian hormone ranged from 074 pmol / l to 269 pmol / l in those who became pregnant in the abvd - avd group , and were 019 pmol / l and 020 pmol / l in those in the beacopp group . 
two women , one in each treatment group , had follicleunde tectable antimllerian hormone , high stimulating hormone , and low oestradiol concentrations after the recorded pregnancy , consistent with development of premature ovarian insufficiency within 3 years of chemotherapy treatment . adverse event data were reported in detail previously , 17 but they did not include any data on ovarian function or fertility . 
 discussion in this prospective cohort study , we have shown that antimllerian hormone concentrations decrease in women with hodgkins lymphoma who are treated with abvd , avd , or beacopp ( beacopp - 14 or escalated beacopp ) , and although antimllerian hormone concentrations recover to baseline concentrations after treatment with abvd or avd , little recovery is seen after treatment with beacopp . 
however , we found 1334 vol 19 october 2018 articles that recovery of ovarian function after treatment with abvd or avd is dependent on age , with full recovery of antimllerian hormone seen in participants younger than 35 years , but not in women aged 35 years or older . 
follicle - stimulating hormone recovery after treatment with abvd or avd was slower in women aged 35 years or older than in those younger than 35 years , and the extent of recovery was much lower for those treated with either beacopp regimen , supporting the increased ovarian toxicity of this drug combination . 
the greater toxicity to other organ systems is also reflected in the higher incidence of febrile neutropenia and thrombocytopenia with beacopp . the potential adverse effect of chemotherapy on ovarian function in women with hodgkins lymphoma is of major concern , affecting fertility , sexual and bone health , and cardiovascular risk . 
potential loss of fertility is a key concern of young women treated for cancer18 and , when appropriate , options for fertility preservation have been established ; thus , the accurate assessment of the is of effect of different chemotherapy regimens substantial importance . 
assessment of ovarian function after treatment via menstrual function and traditional biomarkers such as follicle - stimulating hormone are not of value in detecting ovarian damage that has resulted in incomplete loss of ovarian function . 
measurement of concentrations of antimllerian hormone has emerged as a reliable biomarker to detect partial loss of ovarian function in women after cancer therapy , with the additional advantages of showing little variation across the menstrual cycle.12 although most data are from women after treatment for breast cancer and childhood cancer , 5 , 7 , 8 we have shown the merit of antimllerian hormone measurements in the assessment of ovarian function in adult women with hodgkins lymphoma . 
 specifically , younger women treated with abvd or avd showed full initial recovery of antimllerian hormone after chemotherapy , consistent with previous data2 that indicate that this regimen has little effect on age at menopause , but reduced recovery was seen in women aged 35 years or older at diagnosis . 
by contrast , treatment with beacopp resulted in noticeable and irreversible decreases in antimllerian hormone con centrations , so low in many women that the hormone was undetectable after treatment even with the highly sensitive assay we used . 
participants received either escalated beacopp or beacopp - 14 , a dose - intense version that appears to be similarly gonadotoxic to baseline beacopp.3 our data support this similarity , although the confidence intervals in our estimates were wide . antimllerian hormone concentrations decreased quickly during treatment with both regimens , consistent with both treatments resulting in loss of the growing follicles that are the source of antimllerian hormone . 
this finding is consistent with increased activation of early follicles during chemo therapy resulting from reduced inhibition of growth initiation , which is proposed to be part of the mechanism for chemotherapy - induced premature ovarian insuffi ciency . 
this mechanism has been shown for high toxicity , cyclophosphamide - based regimens , 19 but has not previously been identified for low toxicity regimens such as abvd or avd . the degree of recovery of antimllerian hormone after treatment with abvd or avd in young women could indicate a low toxic effect on the non - growing primordial follicle pool , which constitutes the true ovarian reserve and is the basis for after treatment fertility and the duration of the female reproductive lifespan . 
under physiological conditions , antimllerian hormone con centrations reflect the size of the primordial follicle population , although this population size can be perturbed under circumstances such as a new diagnosis of lymphoma.20 however , the 3 - year follow - up period in this study is likely to have been sufficient for full recovery of ovarian function and therefore restoration of physio logical associations between antimllerian hormone and the ovarian reserve . 
we saw a prominent effect of age on recovery , with substantially lower recovery in women aged 35 years or older than in those younger than 35 years , independent of their antimllerian hormone concentration before treatment . 
 this finding indicates an effect either of age alone or of age in addition to the effects of abvd or avd that result in a substantial decrease in the size of the growing follicle population , and by implication of the non - growing population , after treatment . 
chemotherapy has been shown to affect both the stroma and vasculature of the human ovary , causing fibrosis and hyalinisation of small vessels with loss of primordial follicles within areas of damage.4 changes in ovarian stromal function with age include fibrosis and other hallmarks of chronic inflammation , such as the presence of macrophages , 21 and can impair follicle development.22 these changes could be reversed by gonadotropin suppression , 22 indicating that the increases in concen trations of luteinising hormone and follicle - stimulating hormone during chemotherapy shown here could be of aetiological importance , and the pre - existing more fibrotic stroma in older women could be more susceptible to chemotherapy - induced changes than the stroma in younger women , even with so - called low gonadotoxicity regimens such as abvd or avd . 
these age - associated effects of chemotherapy could have therapeutic implications and be part of the mechanism of action of gonadotropin - releasing hormone agonists to reduce the risk of premature ovarian insufficiency after chemotherapy for breast cancer , 23 , 24 although this effect has not been confirmed for women treated for lymphoma.25 vol 19 october 2018 1335 articles the effect of age on recovery of ovarian function after both regimens , and the different toxic effects of each regimen on the ovaries , is also supported by our analysis of follicle - stimulating hormone recovery in the whole rathl study cohort . 
in this analysis , follicle - stimulating hormone was dichotomised at a value consistent with premature ovarian insufficiency.11 in addition to confirming the effect of age on recovery from treatment with abvd or avd , our analysis showed clear differences in both the speed and extent of recovery between regimens , supporting the antimllerian hormone data . 
folliclestimulating hormone concentrations are affected to a much greater extent than antimllerian hormone concentrations by changes across the menstrual cycle and use of hormonal contraception , but our analysis shows measurement of follicle - stimulating hormone concentrations is of value in large cohorts in which more detailed characterisation is difficult . previous analyses in women with breast cancer have shown that receiving treatment at a young age and high concentrations of anti mllerian hormone before treatment are predictive of recovery of ovarian function after chemotherapy , albeit with variable relative contributions.5 , 9 , 14 , 15 women with breast cancer are generally older ( approximate mean age 40 years5 , 9 , 14 , 15 ) than those with hodgkins lymphoma and treatment involves more gonadotoxic alkylating agent - based regimens , resulting in a high probability of premature loss of ovarian function , particularly in women older than 40 years . 
 these differences emphasise the need for defined populations and treatment regimens to analyse the toxic effects of chemotherapeutic regimens on the ovaries and , particularly , recovery . the data in this study support the paucity of the value of current ovarian reserve markers for the prediction of fertility in the short term , because very low concentrations of antimllerian hormone did not preclude chances of pregnancy . 
the lack of predictive value of anti mllerian hormone measurements for short term fertility has been shown in prospective cohorts of women mostly in their twenties and thirties , 26 , 27 and in women after cancer treatment.28 this study was not designed to assess chances of pregnancy after treatment , and indeed current clinical advice is that women should not attempt to conceive after chemotherapy for around 12 yearsie , most of the duration of follow - up in this study . 
we do not know how many women in each group attempted to conceive , but a similar proportion of pregnancies were seen in women in the beacopp group as in the abvd - avd group within the substudy . 
although these results show that a low concentrations of antimllerian hormone do not preclude pregnancy in the short term , they probably do indicate a reduced interval to menopause and thus a shortened duration of opportunity to achieve pregnancy in the longer term.29 thus , a low concentration of antimllerian hormone after recovery from chemotherapy could identify women who should not unduly postpone pregnancy , and inform individualised discussion ; longer follow - up studies are needed to assess this interpretation . our study had several limitations . 
we also acknowledge the limitations of using follicle - stimulating hormone measurements in isolation without a more robust evidence of premature ovarian insufficiency , which was not possible in the main rathl trial , and data on hormonal contraceptive use during and after treatment were not available . in conclusion , the results of this secondary analysis of the rathl trial indicate the value of antimllerian hormone as a biomarker of toxic effects of chemotherapy on the ovaries during and after different chemo therapy regimens for advanced hodgkins lymphoma . 
we provide additional evidence that treatment with abvd or avd has no detectable effect on gonadal function in young women , although increasing age does restrict ovarian recovery ; confirmation in larger studies is needed to confirm and define this interpretation more precisely , and determine its mechanisby contrast , beacopp shows substantial gonadotoxicity in women of all ages , although some patients might have sufficient ovarian function after to achieve pregnancy . 
concentrations of treatment antimllerian hormone after treatment could be of use in advising women treated for hodgkins lymphoma of their probable reproductive lifespan after treatment . contributors raa and pwmj designed the study ; collected , analysed , and interpreted data ; contributed to manuscript writing ; and approved the manuscript before submission . 
cr recruited patients , collected data , contributed to manuscript writing , and approved the manuscript before submission . declaration of interests raa reports non - financial support from roche diagnostics , and a grant from the medical research foundation . 
all other authors declare no competing interests . acknowledgments the rathl trial was funded by cancer research uk ( reference cruk / 07 / 033 ) , and the ovarian substudy by the medical research foundation ( reference 509909 )  . 
part of this work was done in the mrc centre for reproductive health , university of edinburgh , uk , which is funded by mrc centre grant mr / n022556 / 1 . 
we thank roche diagnostics for the supply of assay reagents , a forbes howie for hormone assays , and all investigators in rathl for their contributions to patient recruitment and management . 1336 vol 19 october 2018 articles 2 published online august 8 , 2018 s1470 - 2045 ( 18 ) 30498 - 4 see articles page 1159 increasing incidence of cancer in children and competing risks the automated childhood cancer information system ( accis ) has been registering data on cancer occurrence from birth to age 20 years in most european countries since the 1970s . 
in the lancet oncology , eva steliarova - foucher and colleagues1 report the latest accis data analysis trends for the period 19912010 for malignant neoplasms in children aged 014 years and adolescents aged 1519 years . 
first , cancer incidence in children aged 014 years has gradually increased over the 19912010 period.1 increasing incidence was observed for all cancers ( 054% ( 95% ci 044 to 065 ) per year ) , leukaemia ( 066% [ 048 to 084 ] per year ) , lymphoma ( 026% [ 001 to 054 ] per year ) , cns malignant tumours ( 049% [ 020 to 077 ] per year ) , and other cancers ( 056% [ 040 to 072 ] per year )  . 
second , for all five cancer categories investigated , incidence increases were similar in all four regions . remain the accis data reinforce the notion that the slow but steady increase in the incidence of many childhood cancers reported since the 1970s is real , and that it is particularly notable for leukaemia.24 unfortunately , epidemiological studies so far have not identified clear risk factors for childhood cancer . 
however , relating the accis data to the tremendous changes in environmental , living , socioeconomic , and public health conditions in european countries after world war 2 might provide clues as to the nature of these reasons . 
if improvements in medical imaging technology were the reason underlying the increased incidence trends of tumours of the cns , then a lower incidence of these tumours should have been observed in the early 1990s in east europe compared with west europe , with a catch up in incidence afterwards . 
however , incidence and incidence trends observed trends from 1991 to 2010 were about the same in east europe and west europe.1 another contrast across european regions concerns the use of pesticides in agriculture . 
in 2014 , the quantities of pesticide sales per capita were about three times greater in spain , italy , and france than in sweden or the uk.5 if increasing cancer incidence trends were due to pesticides , dissimilarities in incidence trends for leukaemia and lymphoma would be expected between european regions , which was not the case.1 a search for marked changes in health events specific to all european children rapidly identifies the dramatic decreases in mortality of children younger than 15 years after world war 2 . 
for example , infant mortality in europe ranged from 160775 deaths per 1000 newborns in 1960 and dropped to 2398 deaths per 1000 newborns in 2010a decrease of 44% per year on average.5 this phenomenon leads to the hypothesis that the death of some children before they reached a certain age precluded the occurrence of cancer by that age . 
death would represent a competing risk ( or event ) in the sense that cancer can no longer occur after death.6 furthermore , children who would have died could also have been at higher risk of cancer for two possible reasons . 
these hypotheses assume that if a child escapes death either because he or she has been protected against potentially deadly diseases ( eg , by vaccination or improved living conditions ) or has survived its occurrence ( eg , because of efficient therapy ) , then the risk of cancer occurrence would be greater in this child than in other children . 
this hypothesis could explain why the peak incidence of leukaemia has shifted towards younger ages over time.4 , 7 steadily decreasing mortality in the months following birth would increase the number of younger children at higher risk for leukaemia . the competing risk hypothesis essentially rests on ecological observations . 
lancet 2004 ; 364 : 2097105 . bevacizumab therapy for recurrent gliomas : another disappointment ? in their article in the lancet oncology , martin van den bent and colleagues1 report on their clinical trial of bevacizumab in the treatment of recurrent grade ii and iii gliomas , and they report the effects of this treatment on overall survival , progression - free survival , quality of life , toxicity , and neurocognitive function . 
 their study was designed as a phase 2 trial and therefore was not powered to show a definite advantage of bevacizumab in these patients , although a high number of patients ( n = 155 ) were enrolled and randomly allocated to the two treatment groups ( temozolomide plus bevacizumab or temozolomide monotherapy )  . 
 to our knowledge , this is the largest study on the use of bevacizumab , with the highest quality data , in patients with recurrent who grade ii and iii gliomas . bevacizumab was previously regarded as a promising new chemotherapeutic drug for the treatment of gliomas . 
 several large trials that used considerable resources were therefore done , although the findings from the study by van den bent and colleagues is mostly in line with the available data on bevacizumab in the treatment of gliomas . 
the authors found no evidence of improved overall survival with bevacizumab and temozolomide combination therapy versus temo zolomide monotherapy : overall survival at 12 months was achieved by 44 ( 61% [ 80% ci 5369 ] ) of 72 patients in the monotherapy group and 38 ( 55% [ 4769 ] ) of 69 in the combination group . 
the results of the study by van den bent and colleagues are disappointing and continue the pattern of failed clinical trials of bevacizumab , which was thought to be a silver bullet in the treatment of intrinsic brain tumours , but which now seems confirmed to be an ineffective chemotherapeutic drug for this indication.24 validated treatment options for recurrent intrinsic brain tumours are scarce . 
although surgery has become more aggressive in the past 1015 years ( an approach that is not supported by robust evidence ) , potent and effective therapeutic drugs for treatment of recurrent tumours are not available.5 , 6 notably , bevacizumab treatment provided no benefit in the secondary efficacy outcomes of this trial , and side - effects were more common in patients receiving bevacizumab . 
despite its failure to improve overall survival , bevacizumab is still used as an adjunct therapy because of its supposed anti - oedematous effects and reported improvements in progression - free survival of patients with glioblastomas.7 it is of note that these anti - oedematous effects and improvements to progression - free survival were only measured by mri ; however , molecular imaging methods such as aminoacid positron emission tomography scans could reveal different tumour progression or overall response to treatment than is shown by mri alone.8 if bevacizumab has a substantial effect on tumour progression and oedema in patients with glioblastoma that outweighs its side - effects , this effect was not shown in patients with who grade ii and iii gliomas in the study by van den bent and colleagues . 
there are several possible published online august 13 , 2018 s1470 - 2045 ( 18 ) 30601 - 6 see articles page 1170 vol 19 september 2018 1137 comment correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections articles hypofractionated radiotherapy versus conventionally fractionated radiotherapy for patients with intermediate - risk localised prostate cancer : 2 - year patient - reported outcomes of the randomised , non - inferiority , phase 3 chhip trial anna wilkins , helen mossop , isabel syndikus , vincent khoo , david bloom eld , chris parker , john logue , christopher scrase , helen patterson , alison birtle , john sta urth , zafar malik , miguel panades , chinnamani eswar , john graham , martin russell , peter kirkbride , joe m osullivan , annie gao , clare cruickshank , clare gri n , david dearnaley * , emma hall * summary background patient - reported outcomes ( pros ) might detect more toxic e ects of radiotherapy than do clinicianreported outcomes . 
we did a quality of life ( qol ) substudy to assess pros up to 24 months after conventionally fractionated or hypofractionated radiotherapy in the conventional or hypofractionated high dose intensity modulated radiotherapy in prostate cancer ( chhip ) trial . methods the chhip trial is a randomised , non - inferiority phase 3 trial done in 71 centres , of which 57 uk hospitals took part in the qol substudy . 
men with localised prostate cancer who were undergoing radiotherapy were eligible for trial entry if they had histologically con rmed t1bt3an0m0 prostate cancer , an estimated risk of seminal vesicle involvement less than 30% , prostate - speci c antigen concentration less than 30 ng / ml , and a who performance status of 0 or 1 . 
participants were randomly assigned ( 1 : 1 : 1 ) to receive a standard fractionation schedule of 74 gy in 37 fractions or one of two hypofractionated schedules : 60 gy in 20 fractions or 57 gy in 19 fractions . 
ucla prostate cancer index ( ucla - pci ) , including short form ( sf ) - 36 and functional assessment of cancer therapy - prostate ( fact - p ) , or expanded prostate cancer index composite ( epic ) and sf - 12 quality - of - life questionnaires were completed at baseline , pre - radiotherapy , 10 weeks post - radiotherapy , and 6 , 12 , 18 , and 24 months post - radiotherapy . 
the chhip trial is registered with isrctn registry , number isrctn97182923 . findings 2100 participants in the chhip trial consented to be included in the qol substudy : 696 assigned to the 74 gy schedule , 698 assigned to the 60 gy schedule , and 706 assigned to the 57 gy schedule . 
median follow - up was 500 months ( iqr 384642 ) on april 9 , 2014 , which was the most recent follow - up measurement of all data collected before the qol data were analysed in september , 2014 . 
 we saw no di erences between treatment groups in change of bowel bother score from baseline or pre - radiotherapy to 24 months . interpretation the incidence of patient - reported bowel symptoms was low and similar between patients in the 74 gy control group and the hypofractionated groups up to 24 months after radiotherapy . 
these studies have not usually included health - related quality of life or patient - reported outcomes ( pros ) , which detect more side - e ects than do clinician - reported outcomes . 
we searched pubmed using the terms patient - reported outcomes or quality of life and hypofractionated or hypofractionation and prostate up to oct 1 , 2002 , and retrieved eight articles . 
of these articles , none reported pros from randomised trials of conventional versus hypofractionated radiotherapy . added value of this study to our knowledge , this study is the largest randomised trial of moderately hypofractionated versus conventionally fractionated radiotherapy using modern radiotherapy techniques , and the rst to report pros up to 2 years after treatment , showing both early and late developing side - e ects . 
 other randomised trials that have included pros and have been reported since this study began used older radiotherapy techniques , or only included follow - up to 3 months after radiotherapy , therefore assessing early rather than late treatment e ects , which are usually dose - limiting . implications of all the available evidence if e cacy outcomes from chhip show non - inferiority for hypofractionated treatments , the absence of any di erence in pros between trial groups adds to the growing evidence for moderately hypofractionated radiotherapy schedules becoming the standard treatment for localised prostate cancer . 
 introduction prostate cancer is the most common cancer in men in the uk , with 41 700 patients diagnosed in 2011.1 for patients diagnosed with localised disease , external beam radiotherapy , radical prostatectomy , and brachytherapy are conventional treatments with similar control rates for organ - con ned tumours . 
patient - reported outcomes ( pros ) detect treatment side - e ects more reliably than do clinician - reported measures and might better guide treatment decisions.2 , 3 the conventional or hypofractionated high dose intensity modulated radiotherapy in prostate cancer ( chhip ) trial ( cruk / 06 / 016 ) randomly assigned men with localised prostate cancer who were undergoing radiotherapy to a standard fractionation schedule or to one of two hypofractionated regimens . 
quality of life ( qol ) was assessed in a substudy within the main trial , in which we aimed to assess whether pros di ered between patients receiving conventionally fractionated versus hypofractionated radiotherapy up to 24 months after radiotherapy . methods study design and participants chhip was a randomised , non - inferiority phase 3 trial done in three seamless stages . 
 initially , men with a prostate - speci c antigen ( psa ) concentration of less than 40 ng / ml and risk of lymph node involvement less than 30% were eligible ; on aug 1 , 2006 , these criteria were revised and a psa concentration less than 30 ng / ml and a risk of seminal vesicle involvement less than 30% were needed . 
full details of trial design , eligibility , and treatment have been reported previously.4 the study was approved by the london multi - centre research ethics committee ( 04 / mre02 / 10 )  . 
the institute of cancer research clinical trials and statistics unit ( icr - ctsu ; sutton , uk ) coordinated the study and carried out central statistical data monitoring and all analyses . 
neither treatment allocation nor ( control ) or one of 1606 vol 16 december 2015 articles clinical assessment were masked because sham radiotherapy was not given . androgen suppression short - course procedures men with nccn intermediate - risk or high - risk disease for received 36 months before and during radiotherapy ; this was optional for patients with low - risk disease . 
individuals assigned the control group received standard radiotherapy with 2 gy daily fractions ( monday to friday treatment ) for 74 weeks , to give a total dose of 74 gy in 37 fractions . 
individuals in the experimental groups received hypofractionated treatment with 3 gy daily fractions to a total dose of either 60 gy in 20 fractions in 40 weeks or 57 gy in 19 fractions in 38 weeks . 
for the hypofractionated schedules , the protocol stated that the overall duration of treatment should be at least 28 days for the 20 - fraction schedule and at least 27 days for the 19 - fraction schedule . 
further details of treatment and quality assurance have been reported previously.4 men consenting to participate in the qol substudy were eligible to complete questionnaires at trial entry if they had not already started endocrine treatment , to minimise the e ect of toxicity of hormone deprivation on qol at this timepoint . 
all men were eligible to complete further questionnaires pre - radiotherapy , and at 10 weeks and 6 , 12 , 18 , and 24 months after the start of radiotherapy . 
 from trial entry to 6 months after radiotherapy , questionnaires were administered in the clinic , and subsequent questionnaires were posted to patients from the icr - ctsu after local veri cation of their current health status . 
all qol questionnaires were selfadministered . in patients during the planning stages of the chhip trial , the university of california , los angeles prostate cancer index ( ucla - pci ) was an important qol instrument available for use in patients with localised prostate cancer.5 subsequently it became apparent that this instrument needed augmentation to better capture the broad range of urinary , bowel , sexual , and hormonal symptoms receiving external beam radiotherapy or brachytherapy , or undergoing radical prostatectomy . 
consequently the expanded prostate cancer index composite ( epic ) qol instrument was developed that had item content that better represented typical symptoms after radiotherapy.6 to maximise the sensitivity of the pros , the qol instruments were updated during the trial to include the epic instrument . 
 therefore from trial initiation to early 2009 , the ucla - pci , including the short form 36 ( sf - 36 ) and functional assessment of cancer therapy - prostate ( fact - p ) qol instruments were used.7 following a protocol amendment on march 12 , 2009 , the epic and short form 12 ( sf - 12 ) qol instruments replaced uclasome old pci , sf - 36 , and fact - p , although questionnaires were received back from participants after this date.8 epic - 50 was used for bowel and urinary domains and epic - 26 for sexual and hormonal domains.9 ucla - pci consists of 20 items organised into six domains , including bowel function ( four items ) , bowel bother ( one item ) , urinary function ( ve items ) , urinary bother ( one item ) , sexual function ( eight items ) , and sexual bother ( one item )  . 
epic - 50 includes a bowel function domain ( seven items ) and a bowel bother domain ( seven items ) , which together form the bowel summary domain , and a urinary function domain ( ve items ) and a urinary bother domain ( seven items ) , which together form a urinary summary doma epic - 26 includes a sexual function domain ( ve items ) and a sexual bother domain ( one item ) , which are combined to form a sexual summary domain ; there is also a hormonal domain ( ve items )  . 
items in the ucla - pci and epic qol instruments di ered : for example , the epic bowel function domain included rectal bleeding , faecal incontinence , and daily bowel movements , which were absent from ucla - pci , the whereas bowel distress was represented ucla - pci bowel function domain and absent from epic - 50 . 
all qol instrument scores range from 0 to 100 and a higher score represents better qol . health - related qol was assessed using the fact - p and sf - 36 instruments ( with ucla - pci ) or the sf - 12 instrument ( with epic )  . 
fact - p consists of physical , social , functional , and emotional wellbeing domains ; each domain has seven items , and scores per domain range from 0 to 28 , except for emotional wellbeing , which ranges from 0 to 24 . 
the sf - 36 instrument includes eight domains of physical functioning , social functioning , vitality , role limitations ( physical ) , role limitations ( emotional ) , mental health , general health , and bodily pain , and each domain score ranges from 0 to 100 . 
sf - 12 consists of a physical composite score ( pcs ) and mental composite score ( mcs ) , each of which have six items , and scores range from 0 to 100 . 
all questionnaires were scored in accordance with scoring manuals.1014 not all the respondents answered all questions ; all available data points were used in analyses . recommended separate qol analyses were planned after 2 and 5 years of follow - up , and this report describes pros up to 2 years . 
 outcomes the primary endpoint was the single item overall how much of a problem have your bowels been for you during the last 4 weeks ( overall bowel bother )  . 
this question vol 16 december 2015 1607 articles was chosen because it gives a good overall measure of bowel - associated morbidity and is common to both the ucla - pci and epic instruments , so was reported by all patients . 
additional secondary endpoints were individual bowel , urinary , and sexual items and domain scores assessed within epic and ucla - pci and the general health - related qol domain scores in fact - p , sf - 36 , and sf - 12 . statistical analysis for all endpoints , the control group was compared with each of the experimental groups , as per the statistical analysis plan of the main trial . 
after this analysis , a post - hoc pragmatic comparison was done between the 60 gy and 57 gy experimental schedules to support clinical management choices if both hypofractionated schedules were shown to be non - inferior to standard fractionation for disease control . 
with 443 patients per experimental group , this substudy would have 80% power and 25% two - sided signi cance to detect changes in the proportion of patients with overall bowel bother scores as follows : from 65% in the standard fractionation group to 60% in an experimental hypofractionation group for scores of 1 ( no bother ) , from 22% to 20% for scores of 2 ( very small bother ) , from 7% to 10% for scores of 3 ( small bother ) , and from 6% to 10% for scores of 4 or 5 ( moderate or severe bother )  . 
power calculations were based on comparisons of two independent groups of ordered categorical data , with constant odds ratios computed across all categories , and assumed complete data would be available for 70% of patients ( 1330 individuals ) at 2 years . 
patients were excluded from the xed timepoint analyses if their qol assessments were dated outside prespeci ed acceptable time intervals : after 1 month of endocrine treatment or after randomisation for baseline ; before 3 months or after 1 week of starting radiotherapy for pre - radiotherapy ; outside 2 weeks from the expected date of completion for 10 weeks ; and outside of 3 months from the expected date of completion for later timepoints . 
qol = quality of life . 1608 vol 16 december 2015 articles were used , guided by a bonferroni adjustment , to make some allowance for multiple testing . we did cross - sectional , time - to - event , and change - frombaseline analyses . 
cross - sectional analysis was done at each timepoint , with formal comparisons between treatment groups at 24 months via the test for trend and the mann - whitney u test . 
we did time - to - event analysis using kaplan - meier methods and the log - rank test to assess time to small or worse , and moderate or worse events for individual items . 
this analysis aimed to detect di erences in late radiation toxic e ects between treatment groups and therefore did not include the 10 - week post - radiotherapy assessment , which assessed acute symptoms . 
patients who reached the relevant endpoint at trial entry or pre - radiotherapy were excluded from that speci c time - to - event analysis . we assessed change from baseline ( post - radiotherapy score minus baseline score ) to account for di erences in pre - existing comorbidity between groups . 
for bowel and urinary items and domain scores , we used the preradiotherapy score as a surrogate baseline score unless it was missing , in which case the baseline score was used . 
 a sensitivity analysis was also done to con rm the robustness of including the baseline assessments of patients receiving less than 1 month of endocrine treatment which involved repeating analyses using baseline assessments of patients receiving no endocrine therapy beforehand . we modelled the odds of any speci c change from baseline or pre - radiotherapy to 24 months using ordinal logistic regression after checking the validity of the proportional odds assumption.15 odds ratios less than one favour the relevant experimental group . 
for the ordinal logistic regression models , the dependent variable is the post - radiotherapy score minus the baseline or preradiotherapy score , taking values of 4 , 3 , 2 , 1 , 0 , 1 , 2 , 3 , or 4 , where negative numbers represent an improvement in qol and positive numbers represent worsening qol . 
patients were excluded from the xed timepoint analyses if their qol assessments were dated outside prespeci ed acceptable time intervals , as outlined in gure 1 . no imputation of missing pro data was done . 
for absent whole instruments , the e ect of these missing data was assessed by comparison of the baseline characteristics of patients present in the analysis versus , rst , those who consented but were missing entirely , and second , those who consented but were missing at 24 months , when formal statistical testing was done . analysis was on an intention - to - treat basis and all analyses were done with stata version 13.1. 
the chhip international standard trial randomised controlled trial , number isrctn97182923 . is registered as an role of the funding source the funders provided peer - reviewed approval for the study concept but had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 table 1 : baseline characteristics and clinical history results between oct 18 , 2002 , and nov 1 , 2009 , 2100 patients were recruited from 57 centres in the uk ( gure 1 and appendix p 14 ) into the qol substudy of the chhip trial ; subsequently , the substudy closed to accrual . 
696 patients were assigned to the standard 74 gy schedule , 698 were assigned to the 60 gy schedule , and 706 were assigned to the 57 gy schedule . median follow - up was 500 months ( iqr 384642 ) on april 9 , 2014 , which was the most recent follow - up measurement of all data collected before the qol data snapshot for this analysis in september , 2014 . 
 questionnaires were returned by 1659 ( 79% ) patients pre - radiotherapy , 1470 ( 70% ) patients at 10 weeks , 1597 ( 76% ) patients at 6 months , 1551 ( 74% ) patients at 12 months , 1456 ( 69% ) patients at 18 months , and 1444 ( 69% ) patients at 24 months . baseline characteristics of patients were balanced between treatment groups except for an imbalance in t stage between the 74 gy and 60 gy groups ( table 1 )  . 
 intermediate nccn risk 1490 ( 71% ) patients had disease.16 for 46 patients reported to have consented to enter the substudy , no qol assessments were received by the icr - ctsu . 
the only signi cant di erence in baseline characteristics between groups with and without 24 - month pro data was that patients with missing questionnaires were more likely to have high nccn risk disease at trial entry than were patients who provided data ( appendix p 2 )  . 
of patients with data from at least one qol assessment , 665 ( 98% ) of 676 in the 74 gy treatment group , 674 ( 98% ) of 686 in the 60 gy treatment group , and 677 ( 98% ) of 692 in the 57 gy treatment group received endocrine therapy . 
cross - sectional analysis at 24 months showed no signi cant di erences in overall bowel bother between the treatment groups ( 74 gy vs 60 gy , ptrend = 064 ; 74 gy vs 57 gy , ptrend = 059 ; appendix p 3 )  . 
 a temporary increase in any bowel bother was seen at 10 weeks ( a change from 413 [ 27% ] of 1509 patients preradiotherapy to 745 [ 57% ] of 1309 patients at 10 weeks )  . 
at 6 months , any bowel bother had decreased ( 581 [ 38% ] of 1519 patients ) , and remained around this level to 24 months , when any overall bowel bother was reported by 441 ( 35% ) of 1258 patients . 
a sensitivity analysis showed that using pre - radiotherapy scores as a surrogate for baseline scores at trial entry for some patients was valid ( appendix p 1112 )  . 
because 252 men completed baseline questionnaires endocrine treatment , a sensitivity analysis was done , which con rmed the robustness of including patients receiving less than 1 month of endocrine treatment at baseline ( appendix p 13 )  . starting after the pattern in overall urinary bother was similar to that for overall bowel bother ( gure 2 , appendix p 4 ) and crosssectional analysis at 24 months showed no signi cant di erences in overall urinary bother between treatment groups ( appendix p 4 )  . 
the baseline incidence of overall sexual bother was higher than that for bowel or urinary bother , with 412 ( 57% ) of 719 patients having any bother at baseline , which increased to 975 ( 68% ) of 1440 patients pre - radiotherapy and improved from 6 months to 24 months ( gure 2 , appendix p 4 )  . 
bowel , urinary , and sexual domain scores assessed within ucla - pci or epic qol instruments also showed no di erence between treatments at 24 months ( table 2 )  . time - to - event analysis of small or worse overall bowel , urinary , and sexual bother showed no signi cant di erences between treatment groups for any endpoints ( gure 2 )  . 
the appendix contains absolute numbers of cumulative small or worse and moderate or worse events , the prevalence of the relevant bowel , urinary , and sexual symptoms before radiotherapy , and the hazard ratios for the time - to - event analysis time from start of radiotherapy to small or worse and moderate or worse events for all individual items in all treatment groups ( appendix pp 5 and 6 )  . 
the number of patients reporting symptoms that were represented only in epic ( faecal incontinence , rectal bleeding , daily bowel movements , dysuria , and haematuria ) was considerably lower than that for other endpoints , so these analyses were underpowered . including incontinence , although we saw no signi cant di erences between treatment groups , the cumulative incidence of some rectal faecal symptoms , bleeding , and use of urinary pads , was higher in patients treated with hypofractionated radiation than in those treated with standard fractionation ( appendix p 5 )  . 
 however , at 24 months , di erences in the prevalence of these symptoms between groups were smaller ( appendix pp 34 )  . figure 3 shows change from baseline for ucla - pci domain scores and epic domain summary scores ; additional epic domain scores are shown in the appendix ( p 10 )  . 
for all urinary and bowel items and domain scores , to maximise numbers , the preradiotherapy score was used as a surrogate baseline score unless missing , in which case the baseline score was used ; exact numbers are : 749 pre - radiotherapy plus 65 baseline for change in ucla - pci bowel function to 24 months ; 146 plus 14 for change in epic bowel summary to 24 months ; 751 plus 64 for change in uclapci urinary function to 24 months ; and 139 plus 16 for change in epic urinary summary to 24 months ( numbers per treatment group shown in appendix p 14 )  . 
 figure 3 also shows change from baseline in scores for the individual items of overall bowel bother , overall urinary bother , and overall sexual bother ; all other endpoints are shown in the appendix ( p 8 )  . 
most patients had no change in score from baseline and we noted no signi cant di erences between treatment groups in change from baseline to 24 months for any individual items . 
compared to the 74 gy control group , the odds of a one - point increase in overall bowel bother were reduced , although not signi cantly , in the 60 gy treatment group ( odds ratio [ or ] 085 [ 99% ci 057126 ] ; p = 029 ) and the 57 gy treatment group ( or 084 [ 057124 ] ; p = 025 )  . 
for some endpoints , the odds of a patient developing sidee ects were slightly increased for the 60 gy group compared with the 57 gy group , but none of these increases were signi cant ( appendix p 8 )  . 
for all urinary and bowel items and domain scores , to maximise numbers , the pre - radiotherapy score was used as a surrogate baseline score unless missing , in which case the baseline score was used . and sf - 36 between treatment groups at 24 months ( appendix p 9 )  . 
however , for domains of vitality , physical role functioning , and social wellbeing , we noted a reduction of more than 10 points between the median domain score at baseline and at 10 weeks after the start of radiotherapy in all treatment groups . 
by 6 months , median scores had increased to within 10 points of the median scores at baseline for all three measures . discussion in this qol substudy of the chhip trial , pros were not signi cantly di erent between treatment groups for any of the endpoints assessed . 
both cross - sectional analysis at 24 months and time - to - event analysis suggest an overall pattern of low incidence of bowel and urinary toxic e ects in all treatment groups . 
these acute toxic e ects had a small and short - lived e ect on general healthrelated qol , especially the sf - 36 domains of vitality , vol 16 december 2015 1613 articles important physical role functioning , and social wellbeing . 
overall , changes from baseline to 24 months for urinary , bowel , and most general health - related qol domains ( except role limitations [ physical ] ) , were less than previously reported minimally from longitudinal anchor - based methods.17 although further development of toxic e ects is possible after 2 years , recent studies have reported minimal change in late radiotherapy side - e ects after 2 years following external beam radiation therapy.18 this suggests that 2 years is an appropriate endpoint for initial pro reporting . di erences derived to our knowledge , this is the rst large randomised trial of hypofractionated radiotherapy that used modern radiotherapy techniques to report pros with follow - up to 24 months . 
radiotherapy doses were higher in hypro ( standard fractionation of 39 fractions of 2 gy in 8 weeks vs hypofractionation with 19 fractions of 34 gy in 65 weeks ) than in chhip . 
a small ( 124 patients ) randomised study of moderate hypofractionation ( 63 gy in 20 fractions ) versus conventional fractionation ( 76 gy in 38 fractions ) reported no di erence in epic scores between treatment groups up to 3 months after radiotherapy.20 the pros in this study are broadly consistent with preliminary data for clinician - reported outcomes in the chhip trial , 4 and the clinician - reported outcomes of a small ( 168 patients ) phase 3 trial in italy.21 results from another randomised trial that included 203 patients showed a non - signi cant numerical increase in clinicianreported toxic e ects with hypofractionation.22 however , the radiotherapy dose schedules used in these studies21 , 22 di er substantially from those in chhip . late gastrointestinal and hypofractionated so far , randomised trials2125 reporting the e ects of hypofractionation versus conventional fractionation have reported inconsistent results for side - e ects and do not clearly show a di erence in the rate of increase of genitourinary or gastrointestinal toxic e ects between conventional radiotherapy treatments.26 these ndings emphasise the need for outcome data from large trials of hypofractionation that use modern radiotherapy techniques . 
such studies to compare hypofractionated radiotherapy with standard fractionation , the clinician - reported outcomes from chhip , will help to con rm whether faecal incontinence , rectal bleeding , or use of urinary pads are more common at a dose of 3 gy per fraction . together with findings from a trial of hypofractionation25 that included 303 patients raised concerns about increased urinary toxic e ects after hypofractionated treatment in patients who had compromised urinary function before enrolment , as assessed by clinician - reported lent and rtog scores . 
a formal comparison restricted to patients with baseline dysfunction has not been done in our study , partly because obstructive and irritative symptoms , and consequently overall urinary dysfunction , are not well represented in the ucla - pci instrument . 
furthermore , overall urinary bother seems to decrease during the 2 years after radiotherapy , which is consistent with ndings from the rt01 dose escalation trial.27 comparison of bowel bother and distress assessed using the ucla - pci instrument in both the 74 gy group of chhip and the 74 gy group of the rt01 trial , 27 in which conventional radiotherapy planning techniques were used , suggests that patients bene t substantially from improved treatment methods that use intensitymodulated radiotherapy and the dose constraints used in chhip . 
in rt01 , 27 ( 9% ) of 289 patients reported moderate bowel bother and nine ( 3% ) patients reported severe bother in the 74 gy group at 24 months.28 this compares with 19 ( 5% ) of 410 patients reporting moderate bother and four ( < 1% ) patients reporting severe bother in the 74 gy group in chhip at 24 months . 
similarly , at 24 months , 34 ( 12% ) of 288 patients in rt0128 versus 13 ( 4% ) of 312 patients in chhip reported moderate bowel distress , and two ( < 1% ) patients in rt0128 versus none in chhip reported severe bowel distress . strengths of our study include the wide age range and large number of patients recruited from di erent parts of the uk . 
the use of di erent qol instruments was a limitation of the analysis , because it meant that fewer patients reported some important radiotherapy - related toxic e ects , including rectal bleeding and faecal incontinence , which were only represented in epic . 
to our knowledge , minimally clinically important di erences have not been published for epic - 50 , but will be a valuable addition when available . patients might acclimatise to symptoms over time and therefore the most subjective endpoints , such as overall bowel , urinary , and sexual bother , might under - represent the actual toxicity at later timepoints . 
however , more objective pros , including rectal bleeding , dysuria , and quality of erections showed similar patterns of toxic e ects over time compared with overall bother items , suggesting reliable representation of patient experience . 
bother items might incorporate a psychosocial component as well as actual that overall bother gives a 1614 vol 16 december 2015 articles functional change , but we believe that overall perception of toxic e ects is a comprehensive and comprehensible endpoint in a randomised comparison of pros . patients with missing data at 24 months were more likely to be in a higher nccn risk group than were those patients with data present . 
both nccn risk group and numbers of patients with missing data did not di er between treatment groups , therefore missing data are unlikely to have substantially biased the randomised comparisons . to complete pros at 5 years will be important to con rm our ndings . 
so far , our results show that the bowel and urinary side - e ects of moderate hypofractionation for prostate cancer delivered with modern radiotherapy techniques are low and similar to those of standard fractionation . contributors aw did statistical analyses , data interpretation and wrote the report . 
dd , eh , is , js , vk , cs , hp , jg , cc , and cg are members of the chhip trial management group responsible for the design and day - to - day oversight of the study and contributed to data interpretation . 
vk reports advisory and educational fees and nonnancial support from astellas , educational fees from bayer , nonnancial educational support from janssen , advisory and educational fees and nonnancial support from ipsen , and educational fees from tolmar . 
 acknowledgments this work was supported by cancer research uk ( cruk / 06 / 16 , c8262 / a7253 , c1491 / a9895 , c1491 / a15955 , sp2312 / 021 ) , the department of health , the national institute for health research cancer research network , and nhs funding to the nihr biomedical research centre at the royal marsden nhs foundation trust and the institute of cancer research , london . 
we would also like to thank the chhip trial management group members , past and present , and the independent data monitoring and trial steering committees for overseeing the trial . 
 helen patterson died in 2012 shortly after completion of recruitment to the trial and remains greatly missed by her colleagues . correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections violence , crime , corruption , and cuts in public spending : how to re - establish cancer control in latin america ? october , 2018 , saw the controversial far - right candidate , jair bolsonaro , win 46% of the presidential vote for brazil . 
 although just falling short of a majority , bolsonaro led a successful campaign that capitalised on fear of rising crime and corruption , championed economic freedom through the promise of privatisation , and pledged the relaxing of gun laws . 
although much of this rhetoric resonates with the populist political agenda in recent years , firm commitments to health - care policy were notably absent from his , as well as his opponents , political programmea critical omission at a time when brazil has been hit with economic and structural weakness , political precariousness , and austerity policies that have capped public expenditure on the growth and sustainability of its health - care syste although unified health system brazils ( sus ) has made substantial progress in recent years , a chronic lack of funds , suboptimal resource allocation , and poor organisation and governance , means that it is struggling to deliver its targets . the prohibition of indeed , these problems are not just isolated incidences in latin america . 
the un and the inter - american commission on human rights declared that the health system in venezuela is in a state of crisis as it witnessed the deaths of at least 16 children in one hospital as a result of deteriorating health facilities , poor sanitation , and a shortage of supplies and medicinesno doubt conditions that are symptomatic of a country suffering from extreme economic instability and political weaknesses , compounded by international humanitarian aid . 
further north , mexicoa country that elected the leftist candidate andrs manuel lpez obrador as president - elect earlier this year to combat similar fears of extreme violence , inequality , and corruptionhas seen its public health insurance scheme , seguro popular , suffer from system fragmentation , underfunding , coverage limitations , and corruption . 
similarly , in honduras , the right - wing president juan orlando hernndez has been accused of rigging elections in late 2017 , in which protestors were killed by security forces , while nicaragua is suffering from extreme political instability , with more than 200 killed in political violence earlier this year amid calls for the former guerrilla daniel ortega to leave the presidential palace . cancera disease reliant on stable , well - funded health systems for continuity and consistency in care delivery will inevitably be affected by these political disturbances . 
 indeed , it is ironic that in the lancet oncologys 2015 commission on cancer control in latin america and the caribbean , paul goss and colleagues attributed the success of the human papillomavirus vaccination programme in brazil to widespread immunisation coverage targets and financial buy - in that were secured by the then ministry of healthan initiative that is now at risk of becoming undone should bolsonaro opt for decreased public expenditure and de - centralised financing . 
hopefully , strong advocacy movements , such as those that feature prominently in brazil , will hold the government to account on their legislative obligationsbut these measures should neither be taken as guaranteed , nor should such movements be expected to become the main drivers of change when governments fail to deliver . the developments unfolding in latin america show that the struggle for democracy is no longer a politics of left versus right , realism versus extremism , or truisms versus tropes . 
in the face of such political upheavals , leaders of these nations would do well to remember that the need for cancer care and control remains unchanged , whoever is in power . 
thus , a key priority for any government is to ensure that there are policies and investments for cancer control that are enshrined in law to ensure there is a level and continuum of care that can be safely delivered to its population irrespective of temporal political disruption . the recommended actions from the 2015 commission on cancer control in latin america and the caribbean still stand today . 
consolidating fragmented health systems , focusing palliative care , improving national cancer registries and cancer control plans , increasing healthcare expenditure , training of oncology and palliative care specialists , and addressing disparities in cancer control are still essential components of effective cancer health systems . 
but only if governments , irrespective of individual party politics , recognise , respond to , and prioritise cancerand indeed all non - communicable diseasesas a persistent and growing health burden , will the fragility of health systems and the needless loss of life be overcome . 
com / journals / lancet / article / piis0140 - 6736 ( 18 ) 32396 - 1 / fulltext for more on iachr report on the venezuelan health system see iachr / media_center / preleases / 2018 / 215.asp for more on the collapse of the venezuelan health system see editorial lancet 2108 ; 391 : 1331 for more on the victory of obrador and the political instability in latin america see com / 2018 / 07 / 10 / opinion / victory - mexican - democracy . html for the 2015 lancet oncology commission on cancer control in latin america and the caribbean see lancet oncol 2015 ; 16 : 140538 vol 19 november 2018 1417 editorial published online december 11 , 2017 s1470 - 2045 ( 17 ) 30914 - 2 see articles page 27 neoadjuvant chemotherapy in breast cancer : more than just downsizing the early breast cancer trialists collaborative group ( ebctcg ) has established a new milestone in evidencebased treatment for early breast cancer . 
through longstanding collaboration , mutual trust , and data transparency , they have gathered individual patient data for 4756 women randomly allocated in ten trials to either neoadjuvant chemotherapy ( nact ) or adjuvant chemotherapy , with a median follow - up of 9 years ( iqr 514 )  . 
the results of this meta - analysis , 1 published in the lancet oncology , substantiate that nact results in higher rates of breast - conserving therapy than does adjuvant chemotherapy ( rate ratio 128 [ 95% ci 122134 ] ) , without compromising on distant recurrence , breast cancer survival , or overall survival . 
 much emphasis is given by the authors to an increase in local recurrence in the nact group ( 15 year absolute increase of 55% [ 95% ci 2486 ] )  . 
the metaanalysis by mieog and colleagues2 showed no significant difference in local recurrence between patients receiving breast - conserving surgery after nact and breastconserving surgery followed by adjuvant chemotherapy , even with inclusion of those receiving nact that were initially scheduled for mastectomy . in the meta - analysis by the ebctcg , 1 nact led to response of the primary tumour , which undoubtedly led to concomitant downstaging of the axillary lymph nodes . 
 studies3 , 4 have shown that pathological complete response ( pcr ) of the axilla is achieved in 4175% of patients with her2 - positive or triple - negative cancer lymph node dissection receiving nact . 
especially among patients with an ultrasound - positive or cytological - positive axilla who had a clinical response with downstaging to a negative axilla , controversy still exists regarding the timing and accuracy of nodal staging with sentinel lymph node biopsy.5 , 6 several studies have addressed the accuracy of nodal staging after nact and current consensus is that sentinel lymph node biopsy after nact in patients with initial positive axilla is considered accurate if at least three or more sentinel nodes are detected and examined.6 although the willingness of surgeons to omit axillary lymph node dissection or radiotherapy of the axilla in patients with complete response to nact is high , 7 no studies have yet investigated locoregional outcomes . 
a randomised phase 3 trial8 is ongoing to assess the role of axillary radiotherapy versus no axillary radiotherapy in patients who converted to pathologically node - negative disease after nact . 
 improvements as was shown in the ebctcg meta - analysis , patients with high - grade , hormone receptor - negative tumours were most likely to achieve a complete clinical response of the primary tumour after nact . 
with the introduction of targeted therapies and improved systemic strategies , substantial pcr have been seen in the past decade , especially in patients with her2 - positive or triple - negative breast cancers . 
several trials have reported consistently high pcr proportions of up to 83% among her2positive , hormone receptor - negative cancers treated preoperatively with combination chemotherapy and ( dual ) targeted anti - her2 agents.9 these complete responders are offered routine breast cancer surgery similar to patients who did not receive nact . 
 several groups are investigating the accuracy of core needle biopsies in the marked area to establish pcr after neoadjuvant treatment , in either those with radiological complete response ( micra study ; trialregister.nl , number ntr6120 ) or those with her2 - positive or triple - negative disease with partial or complete response ( nct02455791 )  . 
on the basis of initial findings of high accuracy of core needle biopsies in small studies , single - arm studies have started recruitment to establish long - term outcomes for omission of breast surgery ( nct02945579 ) .9 , 10 with the evidence generated from this meta - analysis , patients with large tumours can be recommended to have nact and subsequent breast - conserving surgery depending on response assessment . 
time to stop operating on breast cancer patients with pathological complete response ? eur j surg oncol 2013 ; 39 : 92430 . 10 van la parra rf , kuerer hm . 
 breast cancer res 2016 ; 18 : 28 . tumour infiltrating lymphocytes in breast cancer : increasing clinical relevance the immune microenvironment is now recognised as crucial in the treatment of cancer . 
the tumour immune infiltrate has been noted to be associated with better outcomes in her2 - positive breast cancer and triple - negative breast cancer ( tnbc ) , in both the early - stage and the advanced disease setting.1 , 2 incorporating the quantity of the pre - existing immune response with other prognostic clinical pathological factors , such as tumour size and nodal status , will allow clinicians to better estimate long - term survival after breast cancer diagnosis.3 such data will help clinicians improve their treatment recommendations and allow us to design clinical trials of novel treatments for the subgroups that need the most improvement in survival . in the lancet oncology , carsten denkert and colleagues4 have assessed the predictive and prognostic effect of the concentration of tumour - infiltrating lymphocytes ( tils ) , assessed by use of pretreatment haematoxylin and eosin ( h&e ) stained slides of core biopsies , from patients enrolled in six randomised trials investigating neo - adjuvant treatment in breast cancer.4 3771 patient samples were assessed , which constituted the largest pooled analysis on the effect of tils in the neoadjuvant setting to date . 
the authors confirmed the importance of til quantity in the prediction of pathological complete response , independent of breast cancer subtype , and pathological complete response was strongly associated with a better prognosis ( disease free - survival ) in patients with tnbc and her2 - positive breast cancer , but not in a small luminalher2 - negative subgroup . 
 published online december 7 , 2017 s1470 - 2045 ( 17 ) 30905 - 1 see articles page 40 vol 19 january 2018 comment comment published online june 24 , 2015 s1470 - 2045 ( 15 ) 00064 - 9 see articles page 928 investigators to assess long - term outcomes . 
report from a consensus meeting : response to chemoradiotherapy in rectal cancerpredictor of cure and a crucial new choice for the patient : on behalf of the champalimaud 2014 faculty for rectal cancer : when not to operate . 
preoperative high - resolution magnetic resonance imaging can identify good prognosis stage i , ii , and iii rectal cancer best managed by surgery alone : a prospective , multicenter , european study . 
in europe , bevacizumab is approved by the european medicines agency in combination with carboplatin and paclitaxel in newly diagnosed ovarian cancer , with carboplatin and gemcitabine in platinumsensitive relapse ovarian cancer , and with chemotherapy in platinum - resistant relapse ovarian cancer . 
these approvals were based on progression - free survival improvements , but so far no overall survival bene t has been noted with the addition of bevacizumab to chemotherapy in any overall study population.25 in the lancet oncology , amit oza and colleagues1 report the mature overall survival data from icon7 , an openlabel randomised phase 3 trial comparing bevacizumab plus six 3 - weekly cycles of carboplatin and paclitaxel chemotherapy followed by bevacizumab maintenance versus the carboplatin and paclitaxel chemotherapy regimen alone . 
the study participants were patients with newly diagnosed ovarian cancer following cytoreductive surgery or patients with advanced - stage disease who had no further surgery planned.1 the primary endpoint of this trial , progression - free survival , has been reported previously.2 concordant with the results of gog - 218 , 3 another phase 3 trial comparing chemotherapy and bevacizumab versus chemotherapy alone in upfront therapy for ovarian cancer , progression - free survival was 218 months with the addition of bevacizumab compared with 203 months with chemotherapy alone in the overall study , and 181 months versus 145 months in a prede ned high - risk population of patients with suboptimally cytoreduced stage iii or stage iv disease.2 icon7 was also designed and powered to assess overall survival , for which the mature data are now reported . 
 oza and colleagues found no overall survival di erence with the addition of bevacizumab to chemotherapy in the overall study population ( restricted mean survival 446 months [ 95% ci 432459 ] with standard in the chemotherapy vs 455 months [ 442467 ] bevacizumab group )  . 
however , in a high - risk subset of 502 patients with inoperable or suboptimally cytoreduced stage iii or stage iv disease , they did note an overall survival bene t , with a mean overall survival of 345 months ( 95% ci 320370 ) in the chemotherapy alone group compared with 393 months ( 370417 ) with the addition of bevacizumab ( log - rank p = 003 )  . 
 no overall survival bene t was recorded in any other 876 vol 16 august 2015 comment prede ned subgroups , including clear cell , early - stage high - grade , or low - grade serous tumours . when considering the various treatment options available to patients with newly diagnosed ovarian cancer , improved overall survival is an important goal . 
 thus , the ndings reported by oza and colleagues raise the question of whether or not bevacizumab should be considered as rst - line therapy for selected patients at high risk of recurrence . 
notably , however , in a post - hoc exploratory analysis in gog - 218 of a similar population to that reported by oza and colleagues ( suboptimally cytoreduced stage iii or stage iv disease ) , improvement in overall survival with bevacizumab was not signi cant , with median overall survival of 386 months on standard chemotherapy compared with 421 months with chemotherapy and bevacizumab ( hazard ratio [ hr ] 086 95% ci 071104 ; p = 0055 ) .6 when we place these ndings into clinical context , the di erent treatment options for patients with newly diagnosed advanced ovarian cancer should also be considered . 
although icon7 used a chemotherapy backbone of 3 - weekly carboplatin and paclitaxel , the jgog - 3016 trial done by katsumata and colleagues7 reported a signi cant progression - free and overall survival bene t when they substituted weekly paclitaxel for every3 - week paclitaxel . 
this bene t was most pronounced in suboptimally cytoreduced disease , with an increase in median overall survival from 335 months to 512 months ( hr 075 [ 95% ci 057097 ] ; p = 00027 ) .7 gog - 262 , which also compared carboplatin and weekly paclitaxel versus carboplatin and paclitaxel every 3 weeks but allowed bevacizumab at the discretion of the investigator , showed no progression - free survival bene t when bevacizumab was added to weekly paclitaxel ; the small percentage of patients who received weekly paclitaxel without bevacizumab seemed to have similar progression - free survival as those receiving bevacizumab.8 although based on a small subset of patients ( 112 [ 16% ] of 692 patients ) , this nding raises the possibility that either weekly paclitaxel or bevacizumab might be su cient to achieve a progression - free survival bene t in patients with advanced - stage disease . 
finally , in patients with advanced ovarian cancer , neoadjuvant chemotherapy and delayed interval cytoreductive surgery to reduce surgical morbidity has been established as a potential treatment option ; 9 , 10 however , the long half - life and side - e ect pro le of bevacizumab means that the administration of this agent in the neoadjuvant setting is problematic . 
 although the results of icon7 o er the tantalising possibility that a patient subgroup might derive an overall survival bene t from rst - line bevacizumab , caution should be exercised when interpreting subset analyses , and additional questions remain unanswered regarding the use of bevacizumab in newly diagnosed ovarian cancer . 
 only a small proportion of patients in icon7 received bevacizumab after disease recurrence , and therefore whether or not bevacizumab use in the recurrent setting could o set the overall survival bene ts recorded in this high - risk population remains unknown . 
additional studies to understand the e ect of subsequent bevacizumab treatment on survival and to further identify and validate molecular markers of anti - angiogenic response will be important to better de ne our understanding of the role of bevacizumab therapy in ovarian cancer . * joyce f liu , ursula a matulonis gynecology oncology program , dana - farber cancer institute , 450 brookline avenue , boston , ma 02215 , usa ( jfl , uam ) joyce_liu@dfci.harvard.edu jfl is the site principal investigator of clinical trials sponsored by genentech / roche , astrazeneca , merrimack pharmaceuticals , and atara biotherapeutics . 
oceans : a randomized , double - blind , placebo - controlled phase iii trial of chemotherapy with or without bevacizumab in patients with platinum - sensitive recurrent epithelial ovarian , primary peritoneal , or fallopian tube cancer . 
long - term results of dose - dense paclitaxel and carboplatin versus conventional paclitaxel and carboplatin for treatment of advanced epithelial ovarian , fallopian tube , or primary peritoneal cancer ( jgog 3016 ) : a randomised , controlled , open - label trial . 
phase iii trial of every - 3 - weeks paclitaxel versus dose dense weekly paclitaxel with carboplatin + / bevacizumab in epithelial ovarian , peritoneal , fallopian tube cancer : gog 262 ( nct0116712 )  . 
int j gynecol cancer 2013 ; 23 ( 8 suppl 1 ) : 910 . vol 16 august 2015 comment published online july 14 , 2015 s1470 - 2045 ( 15 ) 00061 - 3 see articles page 937 kehoe s , hook j , nankivell m , et al . 
 circulating dna biomarkers : a primer for metastatic colorectal cancer ? although various anti - vegf therapies have been widely adopted as part of the treatment regimen for patients with metastatic colorectal cancer , a predictive biomarker for treatment e ectiveness has not yet been established.1 , 2 ras mutation analysis is a crucial component of diagnostic testing in assessing the role of anti - egfr therapy ; 3 non - invasive approaches to the identi cation of these mutations are of great interest to physicians in view of the generally poor accessibility of archival tissue , which can be further complicated by the amount of tissue available , the remote storage location of the archival tissue , and storage conditions . 
despite these limitations , physicians often continue to attempt to retrieve the archival specimenwhich can result in unnecessary treatment delaysto avoid an additional tissue biopsy or additional nancial burden to the patient . 
 in the lancet oncology , josep tabernero and colleagues have expanded their analysis4 of the placebo - controlled phase 3 trial of regorafenib for refractory metastatic colorectal cancer ( correct ) , the results of which were previously reported.5 in correct , regorafenib , an oral multikinase inhibitor , was reported to improve overall survival bene t compared with placebo ( 64 vs 50 months , hazard ratio [ hr ] 077 , 95% ci 064094 , p = 00052 ) .5 in their exploratory analysis tabernero and colleagues used several approaches to identify potential biomarkers associated with clinical outcome : mutation analysis for kras , braf , and pik3ca by use of beaming ( beads , emulsions , ampli cation , and magnetics ) technology , quanti cation of plasma circulating dna concentrations , and assessment of pretreatment plasma protein concentrations ( high vs low ) of 15 prespeci ed proteins of interest . 
 however , they did report that , not unexpectedly , pretreatment plasma circulating dna concentrations were inversely related to overall survival ( low vs high : hr 034 , 95% ci 025047 )  . 
 distinct intrapatient tumour heterogeneity has previously been reported to potentially exist not only between the primary tumour and metastatic sites , but also between sites of metastatic disease , which might make mutation interpretation and treatment decisions more di cult.6 one advantage of non - invasive circulating dna for tumour mutation analysis is that physicians can use a real - time assessment of existing and acquired mutations associated with therapeutic imaging resistance before con rmatory diagnostic can be done or clinical progression occurs . 
di erent approaches exist to sample circulating dna , including pcr , sanger sequencing , pyrosequencing , and beaming technology.7 beaming uses known hotspot mutations from speci ed genes to give a high sensitivity of less than 01% , and is reportedly able to identify one mutant allele in 10 000 wild - type alleles.8 in the correct exploratory analysis , there was high concordance between matched plasma circulating dna and tumour tissue for both kras and pik3ca mutations assessed using beaming , 9 in smaller studies . 
 consistent with that reported a small group of individuals with archival tumour tissue originally identi ed as kras wild - type were noted to have kras mutant tumour dna in their circulating dna sample , which suggested the development of an acquired mutation . 
 from the biomarker analysis correct are unlikely to change the basis of regorafenib treatment , these exploratory ndings do show the potential usefulness of plasma circulating dna as a although results 878 vol 16 august 2015 editorial for the health secretarys announcement see conservatives.com / post / 98811391555 / jeremyhunt - speech - to - conservativeparty - conference for details of the royal college of general practitioners conference and put patients rst campaign see rcgp.org.uk / for the care quality commission report see les / 20140924_gp_out_of_ hours_ nal.pdf for the dutch cancer society report see kwfk ankerbestrijding.nl / publishingimages / summary%20 aftercare%20of%20cancer%20 patient%20 ( may%202011 ) .pdf provision for cancer patients a priority in primary care reforms on sept 30 , 2014 , uk prime minister david cameron and health secretary jeremy hunt announced major reforms to the uks primary care services whereby everyone will have a named primary care physician and access to general practitioner ( gp ) services for longer hours , every day of the week . 
although these plans will improve acute care , an increasing proportion of gps caseloads is made up of patients with chronic conditions , such as cancer in remission , which require long - term care . 
the royal college of gps ( rcgp ) 2014 annual conference was centred around resilience in general practice , to bolster the profession for the future , a theme backed by the rcgps put patients rst : back general practice campaign . 
patients could lose out unless policy makers take into account all aspects of primary care services . the care quality commission ( cqc ) report on outof - hours care provided by gps published on oct 3 , 2014 , suggested that service provision has improved . 
they are expected to be at the forefront of early detection of cancer while having to provide long - term care for patients being treated for , recovering from , or indeed dying from cancer . 
the rcgp acknowledged the positive aspects from the cqc report and noted that gps had achieved positive results with diminished resources , but their campaign calls for primary care to receive a return to a proportion of funding on a par with 200506 . several factors suggest that the burden of cancer is likely to increase pressure on primary care services . 
the positive news that uk cancer mortality is projected to fall from 170 to 142 per 100 000 people from 2010 to 2030 has to be considered against the backdrop of an increasing and ageing population , and improved detectionreferrals from primary to secondary care for cancer have increased by 50% over the past 4 years . 
acute complications can arise at any time of day or night , and urgent care services may treat patients without full knowledge of any underlying conditions . this issue highlights a major requirement for in nhs services . 
currently , medical improvement records are stored in gp practices or in hospitals without real - time shared access , and consultant - to - gp communication occurs by mailan absurd situation . 
 the government must invest in a secure method for patients electronic records to be jointly updated by physicians managing patient care on a day - to - day basis and emergency providers . 
a good example is the together as one community project in whitby , uk , which introduced new services for patients such as pain management and video - conference consultations with consultants from the patients gp surgery , thus providing more patientcentred and integrated primary and secondary care . 
the society suggested implementation of a common care pathway that can respond to patient need arising from both cancer and comorbidities . most gps provide excellent support to patients who have had a cancer diagnosis . 
however , when politicians implement their headline are drafting plans to statements about improved access to primary care for all , they should not only allocate extra resources on a per - person basis , but also take the opportunity to nance and sta gp practices to e ciently manage continuity of care for those who need extra support . 
now is a perfect time to revolutionise long - term care for patients with cancer and other non - communicable diseases , but this opportunity must not be squandered by politicians poorly conceived , throwaway election promises . 
 the lancet oncology vol 15 november 2014 1279 correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections addendum to lancet oncol 2005 ; 6 : 75156 hckel m , horn l - c , fritsch the h . 
association between mesenchymal compartment of uterovaginal organogenesis and local tumour spread in stage ibiib cervical carcinoma : a prospective study lancet oncol 2005 ; 6 : 75156the supplemental video accompanying this article has been updated . 
this addendum has been added to the online version as of june 29 , 2018 . correction to lancet oncol 2018 ; 19 : 5164 patel mr , ellerton j , infante jr , et al . 
in figure 4a , the first subheading in the inset on the graph should have referred to median progression - free survival in weeks , not months , and the second subheading in the inset on the graph should have read 6 - month pfs , rate ( 95% ci )  . 
 in the results section , last paragraph , the following sentence should have read as follows : of which infusionrelated reaction , diarrhoea , and pneumonitis were reported in more than one patient ( three , two , and two patients , respectively )  . 
also in the last paragraph of the results section , localised oedema should not have been included in the list of reasons for patients who permanently discontinued avelumab due to a treatment - related adverse event . 
 these corrections have been made to the online version as of june 29 , 2018 . correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
 lancet oncol 2017 ; 18 : 106175 in this article , the following sentence about the safety results in the findings section of the summary should have read : commonly reported treatment - related adverse events were diar rhoea ( 41 [ 16% ] ) , fatigue ( 37 [ 15% ] ) , elevated aspartate aminotrans ferase ( 33 [ 13% ] ) , and elevated alanine aminotrans ferase ( 24 [ 10% ] )  . 
the incidence of serious febrile neutropenia in the summary findings and in the main results ( fourth paragraph , first sentence ) should have been reported as 78 ( 31% )  . 
in table 2 , the percentage values for grade 12 nausea , dizziness , elevated alanine aminotransferase , and thrombocytopenia should have been reported as 19% , 19% , 13% , and 2% , respectively . 
in the results , the second sentence ninth paragraph should have read as follows : of 75 patients who achieved a composite complete remission , two ( 3% ) received the 20 mg / day dose , seven ( 9% ) the 80 mg / day dose , 27 ( 36% ) the 120 mg / day dose , 36 ( 48% ) the 200 mg / day dose , and three ( 4% ) the 300 mg / day dose . 
these corrections have been made to the online version as of june 29 , 2018 . vol 19 july 2018 e335 corrections correction to lancet oncol 2019 ; 20 : 23953 ipilimumab scherpereel a , mazieres j , greillier l , et al . 
nivolumab or nivolumab plus patients with relapsed malignant pleural mesothelioma ( ifct - 1501 maps2 ) : a multicentre , open - label , randomised , non - comparative , phase 2 trial . 
 lancet oncol 2019 ; 20 : 23953in figure 4b of this article , the position of the plotted kaplan - meier curves on the y axis has been corrected , affecting the overall survival readings . 
 this correction has been made to the online version as of march 1 , 2019 correction to lancet oncol 2019 ; 20 : 36170 saad ed , squifflet p , burzykowski t , et al . 
 disease - free survival as a surrogate for overall survival in patients with her2positive , early breast cancer in trials of adjuvant trastuzumab for up to 1 year : a systematic review and meta - analysis . 
 lancet oncology 2019 ; 20 : 36170 in the summary of this article , the fourth sentence of the findings section should read subgroups defined by nodal status and hormone receptor status yielded qualitatively similar results . 
this correction has been made to the online version as of march 1 , 2019 , and the printed article is correct . vol 20 march 2019 e132 corrections correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections farewell to four greats as we begin a new year with optimistic anticipation of further achievements in oncology , we must pause to pay tribute to four major innovators and mentors who sadly died at the start of 2019 . on jan 2 , professor waun ki hong , a pioneering physician and scientist at the md anderson cancer center ( houston , tx , usa ) , died aged 76 . 
his work contributed to notable advances in chemoprevention , organ preservation in laryngeal cancer , and personalised targeted therapy . professor bertrand coiffier , who also died on jan 2 , aged 71 , was a leading lymphoma expert , who focused on developing new drug regimens to improve outcomes for aggressive lymphoma . 
he was a professor of hematology at the hospices civils de lyon and the university claude bernard ( lyon , france ) , and was a founding member and president of the groupe detude des lymphomes de ladulte , which later merged with another group to form the world - renowned lymphoma study association . jan 7 , professor john mendelsohn , a former president of the md anderson cancer center , died from glioblastoma , aged 82 . 
he helped to develop the monoclonal antibody cetuximab , which is used to treat colorectal , head and neck , and lung cancers . martin gore , professor of cancer medicine at the institute of cancer research and medical director at the royal marsden hospital ( london , uk ) , died suddenly on jan 10 aged 67 , reportedly after a yellow fever vaccination . 
 he received a cbe in the queens 2016 birthday honours list for services to oncology . as we reflect on the untimely loss of these four inspirational , leading oncologists , this has been a sadand unprecedentedway to start 2019 . 
 the lancet oncology big influences on anti - obesity strategies obesity , the second biggest preventable cause of cancer after tobacco smoking , is a major public health problem worldwide . 
governments must take steps to address this issue ; however , recent reports suggest that chinas antiobesity policies are being influenced by external players . increasingly westernised diets , escalating rural - to - urban migration , and sedentary lifestyles have caused chinas obesity levels to more than double since 1991 . 
in response , the chinese government has launched several public health campaigns , including happy 10 minutes , which encourages schoolchildren to have daily 10 - min breaks for exercise . 
why ? according to recent studies in the bmj and the journal of public health policy , the chinese governments attempts to tackle obesity are being supported by several large multinational food companies , including coca - cola , pepsi - cola , and nestl . 
these companies fund a noninternational life profit research organisation , the sciences institute ( ilsi ) , originally established in the usa in 1978 by a coca - cola executive . 
for several decades , ilsichina has led public health initiatives emphasising the importance of exercise and physical activityrather than nutritionas key to solving the obesity proble by focusing more on physical activity than on a healthy diet , attention is diverted away from highly processed food and calorie - dense snacks and drinks . 
shaping public health policy in this way could help the funding companies to protect sales of their own products and potentially avoid food regulations , advertising rules , and sugar taxes that have been introduced elsewhere . however , diet is clearly crucial . 
governments must not allow their public health strategies to be unduly influenced by powerful multinationals who might be more concerned with protecting their own interests than helping to solve this ongoing health crisis . 
 the lancet oncology vol 20 february 2019 for the bmj report see bmj 2019 ; 364 : k5050 . for the the journal of public health policy study see j public health pol 2019 ; published online jan 9 . 
10.1016 / s0140 - 6736 ( 18 ) 32822 - 8 editorial infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
lancet oncol 2015 ; 16 : 30111in the 6 months post - cycle 1 section of table 1 of this article , in the received row of the second column ( headed cisplatin and paclitaxel plus bevacizumab ) , the data should have been 66 ( 57% )  . 
 bendamustine plus rituximab versus udarabine plus rituximab for patients with relapsed indolent and mantle - cell lymphomas : a multicentre , randomised , open - label , non - inferiority phase 3 trial . 
 lancet oncol 2016 ; 17 : 5766in this article , on page 65 , paragraph 6 , of the discussion section , reference 3 was incorrectly added to the sentence results of our published study8 in the rst - line setting . 
lancet oncol 2016 ; 17 : e8in paragraph two of this news piece , the percentage of genetic mutations in paediatric should have read 95 ( 85% ) of 1120 patients had genetic mutations in their normal tissue that increased their risk of developing cancer during childhood . 
 this correction has been made to the online version as of dec 22 , 2015 . vol 17 january 2016 3 mato ar , hill bt , lamanna n , et al . 
ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
haematologica 2015 ; 100 : e30206 . lenalidomide as maintenance for every newly diagnosed patient with multiple myeloma in patients with newly diagnosed multiple myeloma , how to maintain the responses achieved after optimal therapeutic strategies was a challenge , and maintenance therapy emerged as an option aiming to extend the duration of the response through continued treatment and thereby improving progression - free survival and overall survival . 
because maintenance treatment is administered as continuous therapy , emphasis is placed on the convenience of administration , tolerability , and toxicity.1 low - dose lenalidomide is the only approved single agent treatment for patients with newly diagnosed multiple myeloma after transplantation.2 in the lancet oncology , graham jackson and colleagues3 confirm the benefit of lenalidomide in terms of progression - free survival . 
 in transplantation - ineligible patients , the findings by jackson and colleagues also support the results reported with lenalidomide as maintenance after induction with melphalan , prednisone , and lenalidomide , and are in line with the use of full - dose lenalidomide and dexamethasone as continuous therapy reported in the first trial.4 , 5 although the debate in this setting has always been whether to use fixed or continuous therapy , the trend now is use of continuous therapy with either lenalidomide or daratumumab after induction with daratumumab in combination with bortezomib plus melphalan and prednisone.6 patient with newly diagnosed multiple myeloma , but new therapies or combinations of drugs are needed to improve overall survival in these patients . the approved dose of lenalidomide is convenient because it is administered orally , and this study did not report any unexpected toxicity data . 
additional studies assessing health - related quality of life through patient - reported outcomes are necessary to know the patients perspective . lenalidomide is 10 mg continuously with the possibility of increasing to 15 mg , but different doses and schedules have been so far used in different trials . 
whether different doses and schedules could potentially result in different outcomes is not known , but the results of this study3 regarding the median progression - free survival of 26 months ( 95% ci 2231 ) in transplantation - ineligible patients is similar to that reported in the first trial , in which lenalidomide was given at full dose combined therefore , with possible to switch to low - dose lenalidomide without dexamethasone in transplantation - ineligible patients after induction therapy ? low - dose dexamethasone . 
 it , lenalidomide maintenance seems to be effective , well tolerated , and convenient , despite the lack of overall survival benefit , because of the influence of rescue therapies in the overall survival . 
lenalidomide is , therefore , a maintenance therapy option for every new agents or combinations of these are being investigated as maintenance therapy in this setting and might result in new standards of care . 
for example , vorinostat was combined with lenalidomide in a subset of patients in this study , and we await the results . published online december 14 , 2018 s1470 - 2045 ( 18 ) 30764 - 2 see articles page 57 vol 20 january 2019 comment the results of this study3 support the benefit of lenalidomide maintenance across different subgroups of patients and highlights the progression - free survival benefit in patients with high - risk cytogenetic abnormalities . 
however , it is important to note that lenalidomide did not overcome the poor prognosis that the presence of high - risk abnormalities confer to patients , and therefore novel treatments to improve the outcomes of these patients are needed . whether all patients need continuous maintenance therapy regardless of the quality of the response achieved with previous treatments remains unclear . 
however , next - generation sequencing and cytometry provide an opportunity to investigate the role of minimal residual disease assessment for tailoring maintenance strategies and would allow physicians to prescribe maintenance therapy and reply to a very common question raised by the patients : how many cycles of treatment does maintenance therapy include ? furthermore , long - term minimal residual disease monitoring could guide preemptive treatment preventing clinical relapses and ensuring durable responses . maintenance with lenalidomide is the standard of care , but the future has to move towards a personalised medicine approach that aims to improve overall survival and quality of life , which means giving the right drug to the right patient at the right time for the optimal duration . * mara - victoria mateos , vernica gonzlez de la calle hematology department , university hospital of salamanca , ibsal , salamanca , spain mvmateos@usal.es m - vm has received honoraria for lectures from janssen , celgene , takeda , and amgen , and for participation in advisory boards from janssen , celgene , takeda , amgen , abbvie , glaxosmithkilne , and pharmamar . 
n engl j med 2018 ; 378 : 51828 . the importance of surgery in colorectal cancer treatment in the lancet oncology , sara benitez majano and colleagues1 have engaged with a very important topic . 
 previous data have indicated poorer treatment results for colorectal cancer in both denmark and england compared with those in similar western countries.2 the continuous audit and assessment of outcomes is important to better understand the reality of cancer care each country and thus , this study is of interest to the public . majano and colleagues identified that an important difference between the countries studied regarding surgery for colorectal cancer was probably not the technique , but rather the frequency of surgical resection . 
 the proportion of patients treated with resectional surgery ranged from 684% in england to 813% in sweden for colon cancer , and from 599% in england to 708% in sweden for rectal cancer ; this range was wider for patients older than 75 years ( colon cancer 597% to 809% ; rectal cancer 457% to 619% )  . 
it is possible that attitudes towards surgery in the older patient population should be altered in england , but the data in this study do not include comorbidity , and the risk for increased perioperative mortality should not be underestimated . 
 preoperative optimisation of patients must be a focus of research , to increase the percentage of patients that are able to undergo resectional surgery in the future . what other factors could be influencing these results ? during the study period , the standardised referral pathway had already been introduced in denmark in 2010 . 
the protocol , drawn up in 1997 and o cially enforced from 2005 , required 37 industrialised nations , plus the european community , to reduce their greenhouse gas emissions by 2012 , to achieve a worldwide decrease of 52% compared with concentrations in 1990 . 
although 192 countries rati ed the protocol ( the usa being a notable exception ) , many countries that were classed as rapidly developing at the time of its draftingincluding india and china were exempt . incidence of non - communicable disease the need for countries to act on climate change is enshrined in one of the uns sustainable development goals ( sdg 13 ) , which calls on countries to take urgent action to combat climate change and its impact . 
unexpected or unseasonally heavy rain can lead to ooding , which can release potentially carcinogenic environment from contaminated groundwater by washing over industrial sites or through over ow of sewage . 
 data are already showing that those that had been locked into cold water and arctic ice are now coming out of solution , and are being released into the air as the oceans warm and polar ice melts . chemicals into the climate immediate human change will have costs . 
changing weather patterns could increase food instability ( eg , through drought , or spoiled or contaminated crops ) and in turn , food security concerns might precipitate the increased use of more intensive farming practices , including greater use of carcinogenic pesticides and preservatives . 
finally , climate change risks increasing the numbers of dispossessed peoples in the world , with people eeing either from natural encroachment on their homes by ooding , or from uninhabitable conditions . 
such climate refugees would not fall under any jurisdiction for health care and there is clear evidence of the extremely poor health care , including cancer services , such migrants receive . implementation of the reductions in greenhouse gas emissions would thus not only protect against future burdens , but could also have an immediate bystander e ect by in uencing the activities of heavy polluting industries . 
for example , greenhouse emissions from industry are often released in combination with other carcinogenic pollutantseg , particulate matter between 25 m and 10 m in size , which is signi cantly associated with an increased risk of developing lung cancer . 
the 25 m particulate matter concentration , as recorded by the us embassy in beijing , was reported to be 256 g / m3more than ten times higher than the uns safe limit of 25 g / m3 . climate change is a global problem that needs a global solution . 
the lancet commission on planetary health identi ed poor governance ( de ned as implementation failures ) as an issue that must be addressed if we are to maintain or improve human health in the face of harmful environmental change . 
 the aim of the 2015 paris talksencouraging countries to agree to reduce emissions to the extent that global temperatures increase by no more than 2cneeds all countries to accept responsibility without self - interest : our health , and that of future generations , depends on it . 
 the lancet oncology vol 17 january 2016 correction to lancet oncol 2017 ; 18 : 1493501 correction to lancet oncol 2017 ; 18 : 156566 tawbi ha , burgess m , bolejack v , et al . 
 pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
this correction has been made to the online version as of dec 29 , 2017 . vol 19 january 2018 corrections relapse of wilms tumour and detection methods : a retrospective analysis of the 2001 renal tumour study groupinternational society of paediatric oncology wilms tumour protocol database jesper brok , marta lopez - yurda , harm v tinteren , taryn d treger , rhoikos furtwngler , norbert graf , christophe bergeron , marry m van den heuvel - eibrink , kathy pritchard - jones , ystein e olsen , beatriz de camargo , arnauld verschuur , filippo spreafico summary background wilms tumour is the most common renal cancer in childhood and about 15% of patients will relapse . 
 there is scarce evidence about optimal surveillance schedules and methods for detection of tumour relapse after therapy . methods the renal tumour study groupinternational society of paediatric oncology ( rtsgsiop ) wilms tumour 2001 trial and study is an international , multicentre , prospective registration , biological study with an embedded randomised clinical trial for children with renal tumours aged between 6 months and 18 years . 
the current protocol of siop surveillance for wilms tumour recommends that abdominal ultrasound and chest x - ray should be done every 3 months for the first 2 years after treatment and be repeated every 46 months in the third and fourth year and annually in the fifth year . 
in this retrospective cohort study of the protocol database , we analysed data from participating institutions on timing , anatomical site , and mode of detection of all first relapses of wilms tumour . 
the primary outcomes were how relapse of wilms tumour was detected ( ie , at or between scheduled surveillance and with or without clinical symptoms , scan modality , and physical examination ) and to estimate the number of scans needed to capture one subclinical relapse . 
 the rtsgsiop study is registered with eudra - ct , number 2007 - 004591 - 39 . findings between june 26 , 2001 , and may 8 , 2015 , of 4271 eligible patients in the 2001 rtsgsiop wilms tumour database , 538 ( 13% ) relapsed . 
the primary imaging modality used to detect relapse was reported for 251 patients , among which relapse was identified by abdominal ultrasound ( 80 [ 32% ] patients ) , chest x - ray ( 78 [ 31% ] ) , ct scan of the chest ( 64 [ 25% ] ) or abdomen ( 20 [ 8% ] ) , and abdominal mri ( nine [ 4% ] )  . 
the estimated number of scans needed to detect one subclinical relapse during the first 2 years after nephrectomy was 112 ( 95% ci 106119 ) and , for 25 years after nephrectomy , 500 ( 416588 )  . interpretation planned surveillance imaging captured more than two - thirds of predominantly asymptomatic relapses of wilms tumours , with most detected by abdominal ultrasound , chest x - ray , or chest ct scan . 
the international society of paediatric oncology ( siop ) approach is to monitor for relapse after treatment with chest x - rays and abdominal ultrasound , whereas alternating chest x - rays and abdominal ultrasound and chest and abdominal ct is advised by the childrens oncology group . 
a few , relatively small , retrospectives reports have shown that ct scans can be omitted from surveillance , while highlighting the need for larger prospective studies to assess the benefit and harms of surveillance strategies for wilms tumour . added value of this study this study provides new data about how relapse of wilms tumour is detected . 
although we acknowledge that regional and individual hospitals might make possible minor adjustments , the recommendations for surveillance in the 2001 siop wilms tumour study enabled centres to capture more than two - thirds of , predominantly asymptomatic , wilms tumour relapses . 
however , asymptomatic relapses , captured by surveillance scans , have a better prognosis than do relapses presenting with clinical symptoms between routine follow - up . implications of all the available evidence 2001 siop recommendations , which include abdominal ultrasound and chest x - ray , capture a high proportion of asymptomatic relapses . 
surveillance beyond 2 years after treatment could be consideredas is mandatory for bilateral tumours with increased risk of metachronous relapse and patients with wilms tumour predisposition syndromesbut the overall number of abdominal ultrasounds and chest x - rays needed to capture one asymptomatic relapse would be about 500 . 
randomised trials are needed to assess different surveillance regimens but are less likely to be prioritised over trials of new treatment options . occurring within 2 years after nephrectomy and only occasionally after 5 years.5 the lung is the most common site of relapse for wilms tumour ; local or regional frequently , abdominal relapses occur slightly whereas liver and especially brain and bone involvement is rare.6 , 7 overall survival after relapse is about 50% but the outcome varies depending on several factors . 
key prognostic factors used to stratify treatment for relapse are histological risk group , tumour stage , and previous treatment intensity.610 less as the number of children with wilms tumour or other childhood cancers achieving first complete remission increases , the pressure to detect recurrent tumours places a burden on the childs family and the healthcare syste the aim of such surveillance is to detect relapse at an earlier stage , when prognosis might be better or require less intensive treatment . 
however , fundamental knowledge about costs , benefits , and potential risks of different surveillance strategies for wilms tumour and other childhood cancers is scarce.11 intensive imaging could add unnecessary radiation exposure , and frequent hospital visits after treatment might cause psychological distress to the child and their family.12 , 13 efficacy of surveillance strategies and schedules for wilms tumour has never been prospectively assessed , and are unlikely to be prioritised because the focus of research in this field is on treatment ( ie , new treatment options for patient with poor prognosis [ eg , relapse ] ) and refinement of current treatment through improved risk stratification . 
the few randomised clinical trials done in adults with cancers have shown conflicting results regarding whether or not intensive monitoring for relapse improves outcomes.14 the best methods , duration , and frequency of surveillance for patients with wilms tumour after treatment are still under debate ; therefore , followup strategies can vary geographically depending on available resources and national or regional habitual practices . 
so far , nearly 6000 children and adolescents with renal tumours have been registered on the 2001 trial and study by the international society of paediatric oncology ( siop ) renal tumour study group ( rtsg )  . 
this protocol regular chest xrays and abdominal ultrasound scans for several years depending on initial tumour stage and histology ( table 1 ) .15 data from this large cohort could provide additional useful evidence about the efficacy of routine imaging for the surveillance of tumour relapse . recommended in this retrospective analysis , we describe the timing , anatomical site , and mode of detection of all first relapses of wilms tumour reported in the 2001 siop wilms tumour trial and study . 
we also estimate the number of scans needed to identify one relapse , explore prognostic factors for postrelapse survival , and use the results to evaluate existing surveillance guidelines . vol 19 august 2018 1073 articles chest x - ray abdominal ultrasound localised and metastatic wilms tumour * years 1 and 2 every 3 months every 3 months year 3 year 4 year 5 every 4 months every 4 months every 6 months every 6 months annually annually bilateral tumours and nephrogenic rests years 1 and 2 years 3 and 4 years 510 every 2 months every 2 months every 3 months every 3 months annually annually data from personal communication with national principal investigators of the 2001 wilms tumour study by the international society of paediatric oncology renal tumour study group . 
 * little individual and institutional variation in the total duration and frequency of surveillance imaging . table 1 : imaging surveillance recommendations for wilms tumour after stopping treatment methods study design and participants the siop wilms tumour 2001 trial and study is an international , multicentre registration and biological study with an embedded randomised clinical trial for children with renal tumours aged between 6 months and 18 years . 
after nephrectomy , the intensity and duration of postoperative chemotherapy , occasionally radiotherapy , was determined by tumour histopathology and stage ( appendix p 1 ) .1519 the siop histological classification of pretreated wilms tumour considers three risk groups , which account for the relative proportion of viable tumour cells and necrotic or regressive changes : low risk ( 100% necrotic or cystic tumour ) , intermediate risk ( epithelial , stromal , mixed , regressive type , and focal anaplasia ) , and high risk ( diffuse anaplasia and blastemal type )  . 
the trial closed on jan 1 , 2010 , and the reduced therapy experimental group ( without doxorubicin ) has become the new standard of care since 2011 for this subgroup of patients.15 , 16 here , we report a retrospective cohort study of eligible patients in the rtsgsiop database , which evaluated the current protocol of siop surveillance for wilms tumour that recommends abdominal ultrasound and chest xray should be done every 3 months for the first 2 years after treatment , with ongoing surveillance according to national guidance , usually repeated every 46 months in the third and fourth year ( table 1 )  . 
all participating centres accepted the surveillance scheme , with little regional and individual variation ( table 1 )  . procedures all participating institutions provided data through paper case record forms designed for initial diagnosis , followup , relapse , and end of relapse treatment . 
we collected the following data : sex , age , country , tumour histology and stage , tumour volume at nephrectomy ( based on radiological dimensions and calculated in cm as length width height 0523 ) , nephrectomy ( day 0 ) , relapse status , scan modality that detected relapse , whether a relapse was diagnosed at scheduled surveillance visits or interim ( unscheduled ) because of clinical symptoms , site of relapse , interval between nephrectomy and relapse , interval between relapse and latest normal scan , and overall survival . 
if no information ( ie , an empty box in the case record ) was provided , this was considered missing data . date the we classified any subsequent tumourrelated event in patients with initial bilateral wilms tumour or wilms tumour predisposition syndromes as relapse , but are aware that a proportion might be a new metachronous tumour . outcomes the primary outcomes of this retrospective data analysis were how relapse of wilms tumour was detected ( ie , at or between scheduled surveillance and with or without clinical symptoms , scan modality , and physical examination ) and to estimate the number of scans needed to capture one subclinical relapse . 
in relapsing patients , overall survival was calculated from the time of relapse until death from any cause . statistical analysis we used the kaplanmeier method to generate survival curves and used the logrank test for overall comparisons across all groups . 
from the computed overall survival probabilities , we calculated incidence of relapse within any time period , and accounted for competing risk events ( mortality ) in a separate analysis . 
we did non parametric estimation of the incidence of relapse in the presence of competing risks events in a twostep process.20 , 21 we calculated the kaplanmeier estimate of overall survival from any event ( ie , including relapse and death as events in this model ) , then calculated the conditional probabilities of experiencing the event of interest and used them to estimate the cumulative incidences.22 for overall survival and relapsefree interval , patients without an event at the end of follow up were censored at that time . 
we did univariable and multivariable cox proportional hazards regression analysis , stratified by country , for overall survival and relapsefree continuous variables ( patient age and time to relapse ) ; linear trend tests were based on the slope for the variable . 
hence , a missing date of nephrectomy was input as being 4 weeks ( for localised wilms tumour ) or 6 weeks ( for metastatic wilms tumour ) after the start of treatment . 
we did multiple imputations with the fully conditional method on missing patient clinical characteristics , assuming data were missing at rando this assumption was considered plausible because the absence of data was often related to the centre ( not all information from all centres could be incorporated into the database in time for our analyses ) , rather than unobserved characteristics or the missing data themselves ( appendix pp 34 )  . 
we compared overall survival among relapsed patients according to the same variables , including interval from nephrectomy to relapse , site of relapse , relapse detected at followup with or without symptoms , and interval from last scan without any signs of relapse . 
we used r ( version 3.4.1 ) and sas ( version 9.4 ) for all analyses . role of the funding source the funders of the study had no role in the study design , data collection , data analysis , data interpretation , or writing of the report . 
 table 2 : characteristics of patients with wilms tumour in the study results between june 26 , 2001 , and may 8 , 2015 , 5769 children with renal tumours were registered in the siop wilms tumour 2001 study database ( appendix pp 56 )  . 
we excluded 694 cases of nonwilms renal tumours , 121 with insufficient data , 646 not treated with preoperative chemotherapy according to the protocol or outside the age range ( 6 months to 18 years ) , and 37 patients with progressive disease during preoperative chemotherapy from our analysis . 
at diagnosis , 3409 ( 80% ) of 4271 wilms tumours were localised , 582 ( 14% ) metastatic , and 280 ( 7% ) bilateral ( table 2 )  . at a median followup from surgery of 62 months ( iqr 3293 ) , relapse was reported in 538 ( 13% ) of 4271 patients . 
the site of relapse was registered for 461 ( 86% ) of 538 patients , of which 63 ( 15% ) had combined local and distant relapse and 398 ( 85% ) had relapse confined to either local recurrence or metastatic disease ( appendix p 1 )  . 
relapse involved the lung in 291 ( 63% ) of 461 patients ( including cases with extrapulmonary sites ) , vol 19 august 2018 1075 articles physical examination only imaging only physical examination and imaging method not specified total 1 ( < 1% ) 34 ( 6% ) 54 ( 10% ) symptomatic between scheduled surveillance asymptomatic at scheduled surveillance 3 ( 1% ) symptomatic at scheduled surveillance asymptomatic between scheduled surveillance presentation not specified total 1 ( < 1% ) 1 ( < 1% ) 2 ( < 1% ) 8 ( 1% ) 203 ( 38% ) 26 ( 5% ) 13 ( 2% ) 3 ( 1% ) 279 ( 52% ) 33 ( 6% ) 21 ( 4% ) 6 ( 1% ) 7 ( 1% ) 121 ( 22% ) 2 ( < 1% ) 241 ( 45% ) 89 ( 17% ) 48 ( 9% ) 20 ( 4% ) 128 ( 24% ) 130 ( 24% ) 140 ( 26% ) 538 ( 100% ) data are n ( % ) and are from the 2001 wilms tumour trial and study by the international society of paediatric oncology renal tumour study group . 
values do not sum to 100% because of rounding . table 3 : methods used to detect wilms tumour relapse stage i within period stage ii within period stage iii within period beyond period beyond period stage iv beyond period within period beyond period stage v within period beyond period low - risk or intermediate - risk histology months after nephrectomy 131 / 1395 76 / 647 64 / 525 70 / 398 26 / 196 high - risk histology months after nephrectomy 17 / 169 24 / 119 40 / 142 34 / 75 16 / 59 > 612 > 1218 > 1824 > 2430 > 3036 > 3642 > 4248 > 4854 > 5460 > 612 > 1218 > 1824 > 2430 > 3036 > 3642 > 4248 > 4854 > 5460 based on data from the 2001 wilms tumour trial and study by the international society of paediatric oncology renal tumour study group . 
incidence within period ( eg , 06 months after nephrectomy ) or beyond ( eg , 6 months after nephrectomy ) period was calculated by summing incidences corresponding to relapse times observed in or after the surveillance period . 
 * time to end of study ( may , 2015 ) was used for patients who did not relapse to minimise the effect of very late relapses on the estimates ( ie , a best - case scenario )  . 
 table 4 : estimated % incidence of relapse by initial tumour stage , histology , time from nephrectomy , * and time period of surveillance whereas abdominal or pelvic involvement with or without extraabdominal sites was seen in 225 ( 49% ) of 461 cases . 
 abdominal relapse included cases with locoregional relapse , liver relapse , and metachronous tumours in the contralateral kidney ( appendix , p 1 )  . the method used to detect relapse was registered for 410 ( 76% ) of 538 relapses ( table 3 )  . 
of these relapses , 289 ( 70% ) were captured during scheduled followup visits ( 48 [ 17% ] with clinical symptoms and 241 [ 83% ] without )  . 
 109 ( 27% ) relapses were diagnosed at unscheduled visits 1076 vol 19 august 2018 articles in the interim between planned followup imaging ( 89 [ 82% ] with clinical symptoms and 20 [ 18% ] without )  . 
 relapse was detectable by physical examination ( either with or without imaging ) in only 129 ( 31% ) of 410 cases ; 279 ( 68% ) were not detectable by physical examination ( table 3 )  . 
the primary imaging modality used for identification of relapse was registered for 251 patients , including abdominal ultrasound ( 80 [ 32% ] ) , ct ( 84 [ 33% ] , chest 64 [ 25% ] and abdomen 20 [ 8% ] ) , chest xray ( 78 [ 31% ] ) , and abdominal mri ( nine [ 4% ] )  . 
291 ( 71% ) relapses were found by routine scans within 2 years after nephrectomy , whereas 86 ( 67% ) were found more than 2 years after nephrectomy . timing of relapse was registered for 511 ( 95% ) of 538 patients . 
of these , 408 ( 80% ) occurred within 24 months post nephrectomy , 67 ( 13% ) within 2460 months , and very late relapse ( > 60 months ) was registered for 36 ( 7% ) patients . 
subgroup analyses showed that patients with highrisk histology and advanced tumour stage ( iiiv ) had the highest incidence of relapses occurring shortly ( 012 months ) after nephrectomy ( table 4 )  . 
in a multivariable cox regression analysis of overall survival after relapse , children presenting with clinical symptoms between scheduled number of events univariable analysis multivariable analysis hr ( 95% ci ) p value hr ( 95% ci ) p value time from nephrectomy to relapse female male age group * 6 months to 2 years 24 years 4175 years < 6 months 6 months site of relapse local local and distant lung only detection of relapse symptoms only other stage of wilms tumour histological risk high intermediate volume at nephrectomy 100 ml / unit 1 ( ref ) 1 ( ref ) 071 ( 052095 ) 0021 074 ( 054102 ) 006 057 ( 031103 ) 0061 073 ( 038143 ) 036 1 ( ref ) 1 ( ref ) 154 ( 110215 ) 0011 131 ( 091189 ) 015 188 ( 138255 ) < 00001 163 ( 115231 ) 00062 1 ( ref ) 1 ( ref ) 200 ( 130310 ) 00018 122 ( 076189 ) 126 ( 089180 ) 019 110 ( 074164 ) 041 063 186 ( 129268 ) 000081 184 ( 124274 ) 00027 149 ( 072309 ) 029 123 ( 062247 ) 055 1 ( ref ) 1 ( ref ) 235 ( 136407 ) 00023 234 ( 132415 ) 00038 410 ( 245684 ) < 00001 313 ( 181541 ) < 00001 571 ( 354922 ) < 00001 433 ( 258728 ) < 00001 223 ( 110451 ) 0026 174 ( 079384 ) 017 544 ( 395748 ) < 00001 463 ( 323641 ) < 00001 1 ( ref ) 1 ( ref ) 258 ( 104642 ) 0041 200 ( 076525 ) 016 105 ( 101108 ) 0012 101 ( 097105 ) 053 follow - up without symptoms 1 ( ref ) 1 ( ref ) follow - up with symptoms 134 ( 083217 ) 023 124 ( 071217 ) 045 multiple imputation of missing values are shown for 471 of 538 relapses , with follow - up information after relapse . 
 data for volume at nephrectomy were missing for 80 ( 17% ) of 471 patients and data for detection of relapse were missing for 122 ( 26% ) of 471 . 
 table 5 : cox regression analysis of risk factors for overall survival after relapse surveillance visits had worse postrelapse survival com pared with those without clinical symptoms at scheduled surveillance scans ( median postrelapse overall survival 22 months [ 95% ci 1142 ] for sympto matic patients vs not reached for asymptomatic patients ; hazard ratio 184 [ 95% ci 124274 ] ; p = 00027 )  . 
the following variables were also significant predictive risk factors for survival after relapse : less than 6 months from nephrectomy to relapse , stage ( ii , iii , and iv ) , and highrisk histology ( table 5 )  . 
 in addition to these variables , in the univariable analyses , male sex , older age , multiple sites of relapse , and increasing tumour volume were also significantly associated with shorter overall survival . discussion our retrospective cohort study of the 2001 multicentre rtsgsiop wilms tumour protocol database showed that 13% of children with wilms tumour relapsed , and about 80% of relapses occurred within 2 years after nephrectomy and predominantly involved the lung . 
our analyses showed that relapses among patients with high risk histology and advanced stage ( iiiv ) tumours occurred relatively early after nephrectomy , whereas those with stage v tumours without highrisk histology tended to relapse later . 
for all tumour stage and histological subgroups , the absolute risk of relapse at 2 years after nephrectomy was similar across subgroups . the assumption that earlier recognition of relapse , rather than data from controlled studies , will lead to a better prognosis influences physicians attitudes toward recommending surveillance imaging . 
 knowledge about how relapse of wilms tumour is detected is scarce , and the evidence to support current surveillance strategies is weak.23 since surveillance can be a burden for families and the healthcare system , we aimed to strengthen this evidence base by analysing the large cohort of patients with wilms tumour treated according to a standardised protocol with preoperative chemo therapy in the 2001 siop wilms tumour study . 
 guided by the protocol surveillance recommendation , we found that routine followup scans found at least 70% of the relapses , whereas physical examination , usually done by a paediatrician , was unable to detect recurrence in about twothirds of children . 
furthermore , early relapse , presentation with clinical symptoms in the interval between two scheduled followup visits , advanced tumour stage ( excluding stage v ) , and highrisk histology were associated with worse overall survival in patients who relapsed . frequently the main strengths of this study are the substantial number of patients , prospective data collection , and assessment of longterm outcomes . 
for the past 15 years , patients have been treated according to the same protocol 1078 vol 19 august 2018 articles without substantial changes in disease management , except that ct scans rather than xrays are now increasingly used for the standard for upfront diagnosis ( not surveillance ) of lung metastases and that , for a subgroup of patients with intermediate risk ( stage ii / iii ) , doxorubicinbased perioperative chemotherapy has been omitted since 2011 to reduce the risk of late effects.15 as is the case with all registration studies , incompleteness of some items , which led to exclusion of a small proportion of patients from our analysesmitigated by use of statistical imputation methodsmight be some limitations of our study . 
 finally , we did not record individual and centre surveillance strategies ; therefore , we calculated the number of scans needed to detect one relapse on the basis of the assumption that all patients adhered to the surveillance protocol recommended by siop . 
we recognise that minor unrecorded deviations in the real life practice of imaging surveillance might introduce bias when interpreting our data . we observed that , up to 2 years after surgery , most children had an interval of less than 3 months from last normal imaging to relapse . 
in some cases , it was not possible to conclude whether ct scan was used upfront or only to confirm equivocal chest xray findings ( the latter being more probable ) , so this issue could not be further explored in this analysis . 
lowdose ct scanning of the chest ( 12 msv per scan ) or abdomen might detect smaller nodules but will increase the radiation burden for the patient , and the added value of routine ct surveillance is still under debate.12 , 2326 than the mortality rate was nearly twotimes higher in patients presenting with clinical symptoms between planned surveillance visits in patients with asymptomatic relapse found by planned surveillance . 
 despite this notable disparity , the benefits of surveillance remain uncertain because the difference in mortality could be confounded by other factors , such as location of the tumour and tumourspecific growth rate ( ie , biological aggressiveness )  . 
the benefits of surveil lance imaging would have been further supported if an inferior outcome was associated with parameters such as prolonged interval between last normal surveillance scan and relapse or larger tumour size at relapse . 
to our knowledge , there are no other studies of a similar size on wilms tumour or other extracranial solid tumours with which we can compare our results . one key decision when planning wilms tumour surveillance is the cutoff relapse risk for entering and continuing surveillance . 
to guide this decision , we have created a socalled surveillance map that shows the estimated incidence of relapse for subgroups of wilms tumour at different timepoints after nephrectomy ( see table 4 )  . 
since one in four relapses are detected because of clinical symptoms , we estimated the number of relapses detected solely by biannual surveillance imaging at 2 years post nephr ctomy to be about one in 130 patients . 
when calculating estimates of relapse incidence , we used a bestcase scenario ( ie , followup of patients without an observed relapse was extended up to the end of the study period ) to minimise the effect of patients with very late relapses . 
 this assumption might slightly underestimate the true incidence . similar calculations can be made for other timepoints and subgroups , but these numbers show that a substantial proportion of healthy children undergo scans ( ultrasound , xray , or ct ) with potential harmful effects.12 a pragmatic cutoff risk of 5% for developing a tumour is used to decide whether children with wilms tumour predisposition syndromes should enter a screening programme of abdominal ultrasounds every 3 months . 
this interval accounts for the doubling rate of wilms tumour ( 10 days ) and the sensitivity of abdominal ultrasound.28 , 29 our results confirm that the risk of very late relapse is low , which suggests that prolonging surveillance imaging beyond 5 years after nephrectomy is unjustified.5 the costeffectiveness of surveillance for relapse is complex to evaluate and includes the balance between additional stress for families after treatment and the reassurance or relief of continuous surveillance proving that the child remains in complete remission . 
 pragmatically , a randomised trial that compares frequent monitoring with less frequent monitoring or ct scanning with ultrasound or chest xray for highrisk patients is unlikely to be prioritised over therapeutic interventions , despite being relatively cheap to do . 
even if the concept is adequately explained to families , parents might be reluctant to consent to their child being enrolled in the experimental group of a trial that prescribes less intensive surveillance . 
finally , this area is not regarded as a research vol 19 august 2018 1079 articles priority and will probably not receive sufficient financing because the focus of research in this field is on novel agents in relapse settings . despite the gap in evidence , patients should not be precluded from monitoring and surveillance and such practices should be standard practice in children after treatment for cancer . 
additionally , the purpose of follow up is multifactorial , including social and emotional aspects , rehabilitation , physical examination , and moni toring and management of late treatmentrelated adverse effects . 
surveillance beyond 2 years post treatment could be considered , but the overall number of abdominal ultrasounds and chest xrays needed to capture one asymptomatic relapse is substantial so extended surveillance might not be costeffective . contributors all authors contributed to the conception and design of this study . 
all authors approved the final version of the manuscript . declaration of interests we declare no competing interests . acknowledgments we thank all patients and their families who were enrolled in the siop 2001 wilms tumour study , and the researchers and clinicians who provided data . 
funding was received from great ormond street hospital childrens charity , the european expert paediatric oncology reference network for diagnostics and treatment , cancer research uk ( grants c1188 / a8687 ; c1188 / a11859 ) , the uk national cancer research network and childrens cancer and leukaemia group , socit franaise des cancers de lenfant and association leon berard enfant cancreux and enfant et sant , gesellschaft fur pdiatrische onkologie und hmatologie and deutsche krebshilfe ( grant 502709gr2 ) , grupo cooperativo brasileiro para o tratamento do tumor de wilms and sociedade brasileira de oncologia peditrica , the spanish society of pediatric haematology and oncology and the spanish association against cancer , and siopnetherlands . 
the cancer research uk clinical trials unit at university of birmingham supported the uk data contribution . for cancer waiting time statistics in england see statistical - work - areas / cancerwaiting - times / ; in scotland see health - topics / waiting - times / cancer / ; in wales see wales / statistics - and - research / nhs - activity - performancesummary / ? skip = 1&lang = en for the general medical council study findings see theguardian.com / society / 2017 / nov / 26 / safety - fears - as - juniordoctors - left - to - run - aes - andother - hospital - units for the lancet oncology editorial see lancet oncol 2015 ; 16 : 1273 for the nhs statement about the budget see theguardian.com / society / 2017 / nov / 30 / nhs - bosses - waiting - timetargets - abandoned - next - year the nhs : failing to deliver on beveridges promise ? just over 75 years have passed since sir william beveridge published his report outlining the parameters for a social welfare state for the uk , which crucially included comprehensive health and rehabilitation services for prevention and cure of disease . 
although the vision of beveridge and bevanto provide free , adequate , and equally accessible health care for allremains in high regard today , the execution and delivery of their goal is currently falling short . 
is the uk in danger of losing the nhs because the government is uninterested in or incapable of the effort needed to save it ? 2017 was a year of great difficulty for the nhs . 
 moreover , and worryingly , in december , 2017 , cancer x - ray diagnostic services came under national review by the care quality commission , after the discovery that between april 1 , 2016 , and march 31 , 2017 , more than 20 000 x - ray images had not been reviewed by a radiologist or properly trained clinician . 
indeed , a study from the general medical council has shown that , due to chronic staff shortages , inexperienced doctors without sufficient training or competence are being left in charge of hospital departments . 
it is thus hardly surprising that nearly 1000 patients have received cancer misdiagnosis settlements totalling 757 million in the past 10 years and that the cost of the nhs clinical negligence scheme has in 200607 to 16 billion in 201617 . increased from 400 million such issues are regrettably reminiscent of nhs difficulties that we highlighted in a previous editorial in october , 2015 . 
long - term underfunding , which in turn has led to deficiencies prevalent for decades in staffing , training , and infrastructure , has been at least partly responsible for this deficit of care . 
 however , analyses indicate that real - term spending on the nhs is decreasing or remaining stagnant , while demand is increasing by up to 7% per year , fuelled by a growing and ageing population with a rising incidence indeed , as high as this of chronic comorbidities . 
 budgetary addition might seem , it will barely cover the cost of the clinical negligence scheme alone and will not get to the root of the problem or provide a net benefit to the systeas service needs rise and resources remain the same , services will exceed capacity and become potentially unsafe . in the late 1940s , with a world war in recent memory , british society was in favour of a social welfare state and there was near cross - party governmental support to provide services such as the nhs . 
 in response to the provision in the 2017 autumn budget , nhs england issued a damning statementit would have to ignore waiting time limits , stop prescribing some over the counter medications , and would not be able to guarantee to act on any new nice guidance , all of which would breach the nhs constitution . 
 in terms of oncology recommendations , hunt did promise to hire 500 more cancer experts , but this addition barely covers current critical shortfalls in staffing , and does not address infrastructure or treatment requirements . 
 on dec 11 , 2017 , kings college hospital nhs foundation trust chairman lord robert kerslake resigned , telling the bbc that he believes the government and regulator are unrealistic about the scale of the challenge facing the nhs . 
yet nhs governance is not blamelessfurther funding is of no use if smart and judicious decisions are not made to ensure the service is optimised around efficiency , safety , and patients . 
it is a paradox that at a time when more and more countries aspire to universal health care that the country that spearheaded the model is moving further from it . 
 the lancet oncology vol 19 january 2018 editorial corrections correction to lancet oncol 2016 ; 17 : 109 correction to lancet oncol 2016 ; 17 : 248 , 252 du y sw , dibden a , michalopoulos d , et al . 
lancet oncol 2016 ; 17 : 10914in the findings section of the summary of this article , the second sentence should read the average frequency of dcis detected at screening was 160 per 1000 women screened ( median 150 [ unit range 054356 ] per 1000 women )  . 
 addition of docetaxel or bisphosphonates to standard of care in men with localised or metastatic , hormone - sensitive prostate cancer : a systematic review and meta - analyses of aggregate data . 
 lancet oncol 2016 ; 17 : 24356in the results section , the third sentence of the second paragraph should read in the three remaining trials , 7 , 8 , 10 men aged 3691 years ( median 6366 years ) with a good performance status received androgen deprivation therapy - based treatments ( standard of care ) with or without docetaxel . 
 in figure 3 , the text under parts a and c should have read favours soc + bisphosphonate , and the text under parts b and d should have read favours soc + zoledronic acid . 
we aimed to provide conclusive results for the clinical bene ts of hyperbaric oxygen in patients with chronic bowel dysfunction after radiotherapy for pelvic malignancies . methods hot2 was a double - blind , sham - controlled , phase 3 randomised study of patients ( 18 years ) with chronic gastrointestinal symptoms for 12 months or more after radiotherapy and which persisted despite at least 3 months of optimal medical therapy and no evidence of cancer recurrence . 
participants were strati ed by participating hyperbaric centre and randomly assigned ( 2 : 1 ) by a computer - generated list ( block size nine or 12 ) to receive treatment with hyperbaric oxygen therapy or shaparticipants in the active treatment group breathed 100% oxygen at 24 atmospheres of absolute pressure ( ata ) and the control group breathed 21% oxygen at 13 ata ; both treatment groups received 90 - min air pressure exposures once daily for 5 days per week for a total of 8 weeks ( total of 40 exposures )  . 
sta at the participating hyperbaric medicine facilities knew the allocated treatment , but patients , clinicians , nurse practitioners , and other health - care professionals associated with patients care were masked to treatment allocation . 
primary endpoints were changes in the bowel component of the modi ed in ammatory bowel disease questionnaire ( ibdq ) score and the ibdq rectal bleeding score 12 months after start of treatment relative to baseline . 
the primary outcome was analysed in a modi ed intention - to - treat population , excluding patients who did not provide ibdq scores within a predetermined time - frame . 
 the trial is registered with the isrctn registry , number isrctn86894066 . findings between aug 14 , 2009 , and oct 23 , 2012 , 84 participants were randomly assigned : 55 to hyperbaric oxygen and 29 to sham control . 
75 ( 89% ) participants received 40 pressure exposures , all participants returned the ibdq at baseline , 75 ( 89% ) participants returned the ibdq at 2 weeks post - treatment , and 79 ( 94% ) participants returned the ibdq at 12 months post - start of treatment . 
in an analysis of 46 participants in the active treatment group and 23 participants in the control group , we found no signi cant di erences in the change of ibdq bowel component score ( median change from baseline to 12 months of 4 ( iqr 3 to 11 ) in the treatment group vs 4 ( 6 to 9 ) in the sham group ; mann - whitney u score 067 , p = 050 )  . 
in an analysis of 29 participants in the active treatment group and 11 participants in the sham group with rectal bleeding at baseline , we also found no signi cant di erences in the change of ibdq rectal bleeding score ( median change from baseline to 12 months of 3 [ 1 to 3 ] in the treatment group vs 1 [ 1 to 2 ] in the sham group ; u score 169 , p = 0092 )  . 
common adverse events in both groups were eye refractive changes ( three [ 11% ] of 28 patients in the control group vs 16 [ 30% ] of 53 patients in the treatment group ) , increased fatigue ( three [ 11% ] vs two [ 4% ] ) , and ear pain ( six [ 21% ] vs 15 [ 28% ] )  . 
eight serious adverse events were reported in eight patients : two were reported in two patients in the control group ( tonsillitis requiring surgery [ grade 3 ] ; recurrent cancer of the vulva [ grade 4 ] ) and six serious adverse events were reported in six patients in the treatment group ( malignant spinal cord compression requiring surgery [ grade 3 ] ; malignant paraortic lymph node involvement requiring surgery [ grade 3 ] ; recurrence of vomiting and dehydration [ grade 3 ] ; diarrhoea and fever associated with campylobacter infection [ grade 3 ] ; recurrence of abdominal pain , bloating , diarrhoea , and urinary tract infection [ grade 3 ] ; aneurysm [ grade 4 ] ) , none of which were deemed treatment - related . interpretation we found no evidence that patients with radiation - induced chronic gastrointestinal symptoms , including those patients with rectal bleeding , bene t from hyperbaric oxygen therapy . 
open access article distributed under the terms of cc by . 224 vol 17 february 2016 articles see online for appendix research in context evidence before this study hyperbaric oxygen is widely used to treat chronic adverse e ects of curative radiotherapy in long - term survivors of pelvic malignancy , especially those with rectal bleeding . 
we searched pubmed from jan 1 , 1970 , to dec 31 , 2008 , with the terms clinical trials and hyperbaric oxygen and pelvic or pelvis or bowel and radiotherapy . 
the results of a single randomised , sham - controlled trial from 2008 ( hortis ) reported signi cant clinical bene ts for patients treated with hyperbaric oxygen 2 weeks post - treatment . 
a cochrane intervention review from 2012 con rmed the retrospective nature of much research and detected no other level 1 evidence on which to base an assessment of this treatment modality for patients with chronic radiation - induced bowel dysfunction . added value of this study the results of this double - blind , sham - controlled clinical trial fail to con rm earlier positive results of hyperbaric therapy for cancer survivors with chronic bowel dysfunction , including a subset of patients with rectal bleeding , after curative radiotherapy for pelvic malignancy , with a similarly sized minority of volunteers in each randomised group reporting some improvement in symptoms . 
this trial is only the second randomised study in this important patient population . implications of all the available evidence the contribution of hyperbaric oxygen to the management of a growing population of long - term cancer survivors with severe restrictions on daily activities and impaired quality of life as a consequence of bowel injuries after curative radiotherapy for pelvic malignancy remains unclear and requires more evidence from well designed clinical trials . 
additional exclusion criteria included medical history of cancer recurrence , rectal surgery , previous hyperbaric oxygen therapy ( except for illness ) , exposure to bleomycin , claustrophobia , epilepsy , uncontrolled asthma , bullous lung disease , some types of ear surgery , and inability to equalise the middle ear . 
individuals with a past history of prostate cancer had to have three serial measurements of serum prostate - speci c antigen within the normal concentration range ( less than 3 ng / ml for men aged 5059 years , 4 ng / ml for men aged 6069 years , 5 ng / ml for men 70 years or older )  . treatment of decompression patients with symptoms attributed to radiotherapy entered a minimum 3 - month period of optimum standard treatment , including antibiotic treatment for small bowel bacterial overgrowth , treatment of bile acid malabsorption , 7 lifestyle advice , or several of these interventions , and were supervised by a gastroenterologist . 
individuals were considered eligible for the study only if the 3 - month period of optimal standard treatment was unsuccessful . vol 17 february 2016 articles for the study report see clinical - study - report.pdf for the trial protocol see trial - protocol.pdf all patients provided written informed consent . 
the study was approved by the mhra ( 2008 - 002152 - 26 ) and the nres committee north east - york ( 08 / h0903 / 40 )  . 
the full case study report and trial protocol are available online . randomisation and masking eligible participants were randomly assigned ( 2 : 1 ) to receive hyperbaric oxygen treatment or sha randomisation was arranged by a telephone call from the treating hyperbaric medicine facility to the institute of cancer research clinical trials and statistics unit ( icr - ctsu )  . 
 to deliver the correct treatment , only engineers and technicians operating the hyperbaric chamber were informed of the allocated treatment by the trials o ce , and care was taken to ensure that patients , clinicians , nurse practitioners , and other health - care professionals associated with patients care remained masked to treatment allocation . 
the most important precaution was to disallow any non - trial patient sharing the chamber with a trial patient . for the ctcae protocols see protocoldevelopment / electronic_applications / ctc.htm procedures participants attended the participating hyperbaric oxygen medicine facility most convenient for them , where they panel : bowel function component of the modi ed in ammatory bowel disease questionnaire ( ibdq ) 11 question 1 : have you had your bowel open ? question 5 : have you had loose bowel movements ? question 9 : have you been troubled by pain in your bottom ? question 13 : have you had cramp in tummy or bottom ? question 17 : have you passed a large amount of gas ? question 20 : have you been troubled by bloating ? question 22 : have you had a problem with bleeding from your bottom ? question 24 : have you felt like you need to have your bowel open but nothing happens ? question 26 : have you been troubled by accidental soiling ? question 29 : have you felt disgusted about your bowel problems ? each question is linked to the following response options on a 7 - point graded scale : 1 = more than ever before ; 2 = extremely frequently ; 3 = very frequently ; 4 = moderate increase in frequency ; 5 = some increase in frequency ; 6 = slight increase in frequency ; 7 = normal / not at all . 
the possible range of summed results for the 10 questions is 1070 , where 10 represents the most severe , and 70 the least severe , levels of e ect , this metric represents a co - primary endpoint . 
 patients in the hyperbaric oxygen therapy group received 40 pressure exposures at 24 atmospheres of absolute pressure ( ata ; 243 kpa ) breathing 100% oxygen for 90 min ( including 5 - min air breaks at 30 - min intervals ) , whereas patients in the control group received 40 pressure exposures at 13 ata ( 131 kpa ) breathing 21% oxygen ( ie , air ) for 90 min with two simulated 5 - min air breaks . 
dose reductions were not permitted . participants were asked to complete the modi ed in ammatory bowel disease questionnaire ( ibdq ) 8 and the european organisation for research and treatment of cancer ( eortc ) c30 core quality of life questionnaire ( qlq - c30 ) and cr38 colorectal module ( qlq - cr38 ) 9 , 10 at baseline , 2 weeks after end of treatment , and again at 3 months , 6 months , 9 months , and 12 months after start of treatment . 
 on the basis of results from a previous study , 14 we considered a reduction in ibdq bowel component 226 vol 17 february 2016 articles score of 7 ( sd 10 ) from baseline to 12 months to be clinically relevant . 
during the recruitment phase of the trial ( february , 2012 ) , the independent data monitoring committee agreed that the signi cance level of 5% could be split to allow additional analyses in patients reporting rectal bleeding in the ibdq at baseline . 
we estimated that 75 evaluable patients would allow us to detect a di erence in ibdq bowel symptom score of 75 with 80% power at a two - sided signi cance level of 3% . 
the bowel component is made up of ten questions , and we used all ten items in the bowel component of the modi ed ibdq to analyse overall bowel function and analysed rectal bleeding using the single rectal bleeding question in the modi ed ibdq . 
 the di erence in change from baseline to 12 months between the two study groups was analysed using the mann - whitney u test due to the non - normality of the data . 
we did two exploratory subgroup analyses of the primary endpoints ; one analysis considered the group of patients who received radiotherapy 15 years before randomisation , and the other considered the group of patients whose trial treatment was delivered by hood ( or monochamber )  . 228 vol 17 february 2016 articles we used stata version 13 for all statistical analyses . 
the trial is registered with the isrctn registry , number isrctn86894066 . role of funding source the funder had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data and had nal responsibility for the decision to submit for publication . treatment ; results between aug 14 , 2009 , and oct 23 , 2012 , 241 patients were given a rigorous initial assessment followed by a 3 - month period of optimised medication . 
84 participants were considered eligible for trial entry and were randomly assigned to treatment with hyperbaric oxygen ( active treatment group ; n = 55 ) or with sham control ( control group ; n = 29 ; gure )  . 
two - thirds of participants had faecal frequency , incontinence , or both , symptoms that suggest injury to the colon as well as rectum , and a similar proportion reported rectal bleeding . 
75 ( 89% ) participants received all 40 planned pressure exposures , and nine ( 11% ) patients received 38 exposures or less ( one patient received 38 exposures , one patient received 31 exposures , one patient received 18 exposures , one patient received 11 exposures , one patient received four exposures , one patient received three patients received no two exposures , and exposures )  . 
of the patients in the modi ed intention - to - treat population who reported slight increase in frequency or worse rectal bleeding on ibdq at baseline , ten ( 67% ) of 15 patients in the control group and 26 ( 74% ) of 35 patients in the treatment group reported an improvement of at least 1 point in the ibdq rectal bleeding score at 12 months ( absolute di erence 76% [ 95% ci 203 to 355 ] ; p = 058 ; appendix p 2 )  . 
 * others were anal canal ( n = 1 ) and vulva ( n = 1 ) in the control group and retroperitoneum ( n = 1 ) , pelvis ( n = 1 ) , rectum ( n = 1 ) , and bladder ( n = 1 ) in the hyperbaric oxygen therapy group . table 3 : patient characteristics at pretrial eligibility assessments irrespective of time of return , showed that the di erence in change from baseline to 12 months between the two study groups was consistent with the modi ed intention - to - treat analysis ( u score 071 [ p = 048 ] for overall bowel function ; u score 206 [ p = 0040 ] for rectal bleeding )  . 
40 ( 47% ) of 84 patients scored grade 15 ( clinically signi cant ) rectal bleeding on the ibdq bowel function component , compared with 57 ( 68% ) patients reporting any rectal bleeding in their medical history ( panel )  . 
planned descriptive analysis of changes in ctcae grades at baseline , 2 weeks post - treatment , and at 12 months also did not show di erences between the treatment groups ( appendix p 4 )  . 
 exploratory subgroup analyses of patients who completed radiotherapy 15 years before entering the study did not show any di erence in ibdq scores between the two groups ( u score 059 [ p = 056 ] for overall bowel function ; u score 157 [ p = 012 ] for rectal bleeding )  . 
exploratory subgroup analysis in patients receiving treatment using a hood or monochamber showed no di erence in overall bowel function but did suggest a di erence in rectal bleeding ( u score 031 [ p = 076 ] for overall bowel function ; u score 29 [ p = 0004 ] for rectal bleeding )  . we analysed toxic e ects in the safety population , which included the 81 patients who received at least one treatment ( 53 in the hyperbaric oxygen therapy group and 28 in the sham control group )  . 
the most commonly reported adverse events were eye refractive change , including myopia ( three [ 11% ] of 28 patients in the control group vs 16 [ 30% ] of 53 patients in the treatment group ) , increased fatigue or tiredness ( three [ 11% ] vs two [ 4% ] ) , and ear pain or barotrauma ( six [ 21% ] vs 15 [ 28% ] )  . 
eight serious adverse events were reported in eight patients : two were reported in two patients in the control group ( tonsillitis requiring surgery [ grade 3 ] ; recurrent cancer of the vulva [ grade 4 ] ) and six serious adverse events were reported six patients in the treatment group ( malignant spinal cord compression requiring surgery [ grade3 ] ; malignant paraortic lymph node involvement requiring surgery [ grade 3 ] ; recurrence of vomiting and dehydration [ grade 3 ] ; diarrhoea and fever associated with campylobacter infection [ grade 3 ] ; recurrence of abdominal pain , bloating , diarrhoea , and urinary tract infection [ grade 3 ] ; aneurysm [ grade 4 ] )  . 
no treatmentrelated deaths were noted . and some clinical evidence discussion despite plausible pathophysiological mechanisms justifying an expectation of therapeutic e ect of hyperbaric oxygen therapy , the hot2 trial results detected no clinically relevant bene t of hyperbaric oxygen therapy in individuals with a wide range of chronic gastrointestinal dysfunction , including rectal bleeding , after curative radiotherapy for pelvic malignancy . 
histologically , progressive obliterative endarteritis is a classic feature and ischaemic atrophy is an important element of the pathophysiology , but direct radiation e ects on other tissue elements , including epithelia , also contribute to symptoms.18 the tissues rendered ischaemic by vascular atrophy do not share the steep oxygen gradients that stimulate angiogenesis in acute surgical wounds unless these gradients are arti cially introduced.19 in studies of animal and human skin , 20 , 21 hyperbaric oxygen therapy has been shown to restore virtually normal small vessel density and tension after transcutaneous oxygen high - dose radiotherapy , an e ect that peaked after 2030 treatments in human beings . 
the proposed therapeutic mechanisms include marrow stem - cell mobilisation and consequent vasculogenesis , although our results do not suggest that these processes , if activated by hyperbaric oxygen , were of therapeutic value.22 our trial results are inconsistent with a long history of striking anecdotes and reviews of non - randomised studies.2 , 2325 a cochrane intervention review3 identi ed two randomised trials testing hyperbaric oxygen in patients with chronic gastrointestinal symptoms after pelvic radiotherapy , but the analysis was restricted to the hortis trial4 because of a high risk of bias identi ed in the other study . 
the hortis trial randomly assigned 150 patients from mexico , turkey , south africa , and australia with a 3 - month or longer medical history of radiation proctitis to breathe air at 11 ata ( sham group ) or 100% oxygen at 20 ata ( active treatment group ) for 90 min for 30 sessions within 68 weeks , with an individual ten sessions depending on additional responses . 
the hortis investigators also reported a signi cant bene t of hyperbaric oxygen in patients with bowel bother , a group of symptoms that include faecal incontinence , faecal urgency , and pa the authors of the cochrane vol 17 february 2016 articles review interpreted these results as non - signi cant and sensitive to randomised patients excluded from primary analysis but concluded that hortis supported the continued use of hyperbaric oxygen for patients with radiation proctitis . it is unclear why the results of hot2 fail to reproduce the hortis4 ndings . 
patient selection was unusually rigorous , including assessment by a gastroenterologist specialised in radiation enteropathy and a 3 - month run - in period of optimised oral drug treatment to ensure that eligible patients had radiation - induced symptoms that could not be controlled by standard measures . 
the trial population is considered representative of patients with radiation enteropathy in terms of their symptoms , although patients with severe faecal incontinence or transfusion - dependent rectal bleeding are likely to be under - represented , the former being too restricted to leave their homes and the latter considered too seriously at risk to be considered by their primary physicians for entry into a trial with a sham treatment option . 
we assessed 20 characteristics relating to bowel dysfunction at baseline , and despite small imbalances in the proportion of patients with a medical history of rectal bleeding ( 23 [ 79% ] of 29 patients in the control group vs 34 [ 62% ] of 55 patients in the treatment group ) , this imbalance did not apply to baseline ibdq rectal bleeding scores analysed as the primary endpoint . 
in other respects , symptom duration in hot2 , at a median 37 years ( iqr 2468 ) postradiotherapy , is consistent with that of the hortis population , and hot2 patient characteristics are well balanced between randomised groups . in a literature review26 of ten retrospective studies published between 1960 and 2004 reporting favourable results of hyperbaric oxygen therapy for patients with radiation proctitis , patients had an average of 24 treatments each . 
compliance with treatment in hot2 was reasonably high , with 75 ( 88% ) of 84 patients eligible for inclusion in the intention - to - treat population , as required by the analysis plan . 
pre - trial investigations designed to exclude patients with residual malignant disease ensured that only three patients developed cancer recurrence while participating in the study . other relevant points of di erence between the hortis4 and hot2 trials include the immediate post - treatment timepoint for the primary analysis in hortis , compared with the primary analysis at 12 months post - treatment in hot2 . 
exploratory analyses of the 2 - week post - treatment in hot2 showed no di erence between e ects the primary endpoint randomised groups for any of the primary or secondary endpoints . 
unlike hot2 , in which we analysed a modi ed intention - to - treat population , the primary analysis in hortis excluded 30 of 150 randomised patients who did not complete the treatment protocol ( plus one patient lost to follow - up ) , although unplanned analyses of the outcomes of clinical assessments by intention - to - treat were also consistent with a bene cial e ect of hyperbaric oxygen in hortis . 
in other exploratory analyses of hot2 endpoints ( including subgroup analysis of patients completing radiotherapy 15 years before randomisation and subgroup analysis of patients receiving treatment by hood or hyperbaric chamber rather than mask ) , we could not identify variables that might explain di erences trials . 
 randomisation appears to have resulted in a reasonably even distribution of patient characteristics between the treatment and control groups in our study , to the extent that the total e ect of these covariates would not be expected to mask any e ect of hyperbaric oxygen . 
the very small number of patients with transfusion - dependent rectal bleeding in this study prevents us from commenting on the use of hyperbaric oxygen therapy for patients referred for this potentially life - threatening complication . reported outcomes between these two our trial was designed to have a power of 80% ; with 69 evaluable patients , we had a power of about 75% to detect a di erence of the magnitude expected in the rst of the primary endpoints . 
we did not detect a clinically or statistically signi cant clinical bene t of hyperbaric oxygen therapy for patients with chronic gastrointestinal dysfunction , including rectal bleeding , after pelvic radiotherapy . 
the ndings contrast with previous reports , highlighting an urgent need for more level 1 evidence to determine with con dence whether hyperbaric oxygen therapy can be recommended as a standard of care for this group of patients . contributors jy was the chief investigator of the trial , was involved in study design , was responsible for the clinical supervision of patients and performance of the study , and contributed to the preparation and writing of the report . 
 mg , grs , hja , beb , pb , of , lg , jh , mi , gl , sm , dm , celp , sp , and gs were were study investigators responsible for patient recruitment , clinical supervision , and treatment of patients , were involved in the acquisition , analysis , and interpretation of the data , and contributed to the writing of the report . 
lm was responsible for the acquisition and analysis of the data , and contributed to the writing of the report . declaration of interests we declare no competing interests . acknowledgments we thank the volunteers and site personnel participating in this study for their support and commitment . 
we aimed to investigate whether adding bortezomib to standard therapy could improve outcomes in patients with these subtypes . methods in a randomised evaluation of molecular guided therapy for diffuse large b - cell lymphoma with bortezomib ( remodl - b ) , an open - label , adaptive , randomised controlled , phase 3 superiority trial , participants were recruited from 107 cancer centres in the uk ( n = 94 ) and switzerland ( n = 13 )  . 
eligible patients had previously untreated , histologically confirmed diffuse large b - cell lymphoma with sufficient diagnostic material from initial biopsies for gene - expression profiling and pathology review ; were aged 18 years or older ; had ecog performance status of 2 or less ; had bulky stage i or stage iiiv disease requiring full - course chemotherapy ; had measurable disease ; and had cardiac , lung , renal , and liver function sufficient to tolerate chemotherapy . 
patients initially received one 21 - day cycle of standard rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ; rituximab 375 mg / m , cyclophosphamide 750 mg / m , doxorubicin 50 mg / m , and vincristine 14 mg / m [ to a maximum of 2 mg total dose ] intravenously on day 1 of the cycle , and prednisolone 100 mg orally once daily on days 15 )  . 
during this time , we did gene - expression profiling using whole genome cdna - mediated annealing , selection , extension , and ligation assay of tissue from routine diagnostic biopsy samples to determine the cell - of - origin subtype of each participant ( germinal centre b cell , activated b cell , or unclassified )  . 
patients were then centrally randomly assigned ( 1 : 1 ) via a web - based system , with block randomisation stratified by international prognostic index score and cell - of - origin subtype , to continue r - chop alone ( r - chop group ; control ) , or with bortezomib ( rb - chop group ; experimental ; 13 mg / m intravenously or 16 mg / m subcutaneously ) on days 1 and 8 for cycles two to six . 
 this study was registered at clinicaltrials.gov , number nct01324596 , and recruitment and treatment has completed for all participants , with long - term follow - up ongoing . findings between june 2 , 2011 , and june 10 , 2015 , 1128 eligible patients were registered , of whom 918 ( 81% ) were randomly assigned to receive treatment ( n = 459 to r - chop , n = 459 to rb - chop ) , comprising 244 ( 266% ) with activated b - cell disease , 475 ( 517% ) with germinal centre b cell disease , and 199 ( 217% ) with unclassified disease . 
 at a median follow - up of 297 months ( 95% ci 290320 ) , we saw no evidence for a difference in progression - free survival in the combined germinal centre and activated b - cell population between r - chop and rb - chop ( 30 - month progression - free survival 701% , 95% ci 650747 vs 743% , 693787 ; hazard ratio 086 , 95% ci 065113 ; p = 028 )  . 
the most common grade 3 or worse adverse event was haematological toxicity , reported in 178 ( 398% ) of 447 patients given r - chop and 187 ( 421% ) of 444 given rb - chop . 
however , rb - chop was not associated with increased haematological toxicity and 398 [ 871% ] of 459 participants assigned to receive rb - chop completed six cycles of treatment . 
serious adverse events occurred in 190 ( 425% ) patients given r - chop , including five treatment - related deaths , and 223 ( 502% ) given rb - chop , including four treatment - related deaths . interpretation this is the first large - scale study in diffuse large b - cell lymphoma to use real - time molecular characterisation for prospective stratification , randomisation , and subsequent analysis of biologically distinct subgroups of patients . 
 introduction the combination of rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ) has been considered standard of care for diffuse large b - cell lymphoma for more than 15 years.1 in trials of r - chop , 5 - year progression - free survival has been reported to be 7075% and overall survival 7580% , 2 although unselected population - based studies show lower figures.3 patients with lymphoma that does not respond to r - chop or that recurs have a poor prognosis , with only a third alive at 2 years after diagnosis.4 various approaches have been attempted to improve outcomes for patients with diffuse large b - cell lymphoma , but none has so far increased overall survival . 
the recognised molecular heterogeneity of this aggressive lymphoma contributes to the complexity of this problem.5 gene - expression profiling of diffuse large b - cell lymphoma has been used to define subgroups with distinct pathogenesis . 
cell - of - origin classification recognises those cases with a gene expression similar to that of peripheral blood b cells undergoing in - vitro antigen activation , referred to as the activated b - cell subtype , whereas the germinal centre b - cell subtype resembles b cells in the germinal centre . 
retrospective analyses suggest that the patients with the activated b - cell subtype have worse outcomes , with 40% 3 - year progression - free survival after r - chop compared with 75% in the germinal centre b - cell group.5 the subtypes have distinct genomic characteristics . 
 the activated b - cell subtype shows a higher prevalence of mutations in genes involved in b - cell receptor signalling and regulators of nuclear factor ( nf ) - b ( myd88 , cd79b , tnfaip3 , card11 , traf2 , traf5 , map3k7 , and tnfrsf11a ) than the germinal centre b - cell subtype . 
constitutive nf - b activation down stream of the b - cell receptor is a feature of the activated b - cell subtype of diffuse large b - cell lymphoma . 
genomic , pharmacological , and rna interference screens have shown selective oncogenic addiction of the activated b - cell subtype to activation of this protein complex.6 bortezomib is a proteasome inhibitor and can suppress nf - b activity by preventing proteosomal degradation research in context evidence before this study we searched pubmed for publications of randomised clinical trials in english between jan 1 , 1998 , and dec 1 , 2010 , using the terms diffuse large b - cell lymphoma and cell of origin , and studies involving diffuse - large b - cell lymphoma and bortezomib . 
using gene - expression profiling to characterise patients , several retrospective studies of patients treated with rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ) or chop - like regimens had shown that the activated b - cell subtype was associated with inferior survival compared with the germinal centre b - cell subtype . 
in another phase 2 study , bortezomib in combination with dose - adjusted r - epoch ( rituximab , etoposide , cyclophosphamide , doxorubicin , vincristine , and prednisolone ) had resulted in longer progression - free survival in patients with the activated b - cell subtype than in those with the germinal centre b - cell subtype . 
bortezomib in combination with r - chop had produced similar outcomes in non - germinal centre b - cell diffuse large b - cell lymphoma ( ascertained by immunohistochemistry ) compared with germinal centre b - cell diffuse large b - cell lymphoma in a further phase 2 study . added value of this study to our knowledge , this study is the first to combine prospective gene - expression profiling of lymphoma with a targeted therapy to allow stratification and random assignment of patients to treatment within a phase 3 clinical trial . 
it is the first study to assess a novel agent in diffuse large b - cell lymphoma , prospectively powered to address subtypes defined by gene - expression profiling , and we have shown that the addition of bortezomib to r - chop ( rb - chop ) does not improve survival in the activated b - cell subgroup . 
 extensive characterisation and subgroup analyses suggest that cell - of - origin subtype and nuclear factor ( nf ) - b activating mutations are not associated with improved outcomes with rb - chop , and that bortezomib does not act as an effective inhibitor of the nf - b pathway in this disease . 
 exploratory analyses , however , suggest that different high - risk subgroupsdouble - expressor lymphoma and double - hit lymphomamight benefit from the addition of bortezomib or similar agents to standard immunochemotherapy . implications of all the available evidence the trial design provides a rational framework for future studies in diffuse large b - cell lymphoma , allowing prompt initiation of treatment while molecular characterisation is carried out . 
 we confirm that r - chop is a good standard of care for most patients with diffuse large b - cell lymphoma , but raise the possibility that high - risk subgroups could benefit from the addition of a proteasome inhibitor to standard therapy , which could guide future research . 650 vol 20 may 2019 articles see online for appendix for the tenalea system see alea / login.aspx of the inhibitor ib , thereby keeping nf - b inactive and unable to translocate to the nucleus to mediate transcription . 
when combined with infusional chemotherapy , bortezomib appeared to have preferential activity in relapsed or refractory activated b - cell diffuse large b - cell lymphoma , with a higher response rate and median overall survival than that achieved with infusional chemotherapy alone.7 for diffuse large b - cell the randomised evaluation of molecular guided therapy lymphoma with bortezomib ( remodl - b ) study aimed to investigate the clinical efficacy of r - chop in addition to bortezomib in patients with diffuse large b - cell lymphoma . 
to determine whether the cell - of - origin subtypes respond differently to the combination of bortezomib with r - chop , we used a study design that incorporated prospective randomisation stratified by whole transcriptome gene - expression profiling . 
we also incor porated molecular characterisation into our analysis to assess recognised subgroups distinct from the cell - of - origin subgroups : double - hit ( rearrangements of myc and bcl2 or bcl6 , or both ) and double - expressor lymphomas ( high expression of myc and bcl2 proteins )  . as clinical studies move towards increased application of targeted drugs against molecular phenotype , the feasibility of determining a molecular phenotype in real - time was an important objective of the study . methods study design and participants in this multicentre , open - label , randomised , phase 3 , superiority trial , we compared r - chop with r - chop plus bortezomib ( rb - chop ) in patients with newly diagnosed diffuse large b - cell lymphoma . 
in a collaboration between the uk national cancer research institute group and the schweiz arbeitsgemeinschaft fur klinische krebsforschung in switzerland , patients were recruited from 107 cancer centres in the uk ( n = 94 ) and switzerland ( n = 13 )  . 
patients were eligible for inclusion in the study if they had de novo diffuse large b - cell lymphoma confirmed by an expert haematopathologist ( cb ) with sufficient diagnostic material from previous biopsies for gene - expression profiling and central pathological review ; were aged 18 years or older ; had eastern cooperative oncology group ( ecog ) performance status of 2 or less ; had bulky stage i or stage iiiv disease requiring fullcourse chemo therapy ; had measurable disease ; and had cardiac , lung , renal , and liver function sufficient to tolerate chemo therapy . 
patients with primary mediastinal lymphoma ; clinical cns involvement ; positive serology for hiv , hepatitis b virus , or hepatitis c virus ; active malignancy in the preceding 5 years ; or other conditions precluding administration of study treatment were ineligible . 
the study was carried out according to the principles of the declaration of helsinki , principles of the international conference on harmonisation of technical requirements for registration of pharmaceuticals for human use good clinical practice , and in accordance with uk and swiss regulatory requirements . 
written informed consent was obtained from all patients . randomisation and masking participants were centrally randomly assigned ( 1 : 1 ) with block randomisation of varying block size by tenalea , a web - based system , to receive either r - chop ( control ) or rb - chop ( experimental )  . 
for the purposes of stratification , participants were grouped by their ipi scores as : low ( 01 ) , intermediate ( 23 ) , and high ( 45 ) , and those with an unclassified cell - of - origin sub type were included . 
 in cases of failed rna extraction or insufficient rna yield , participants were not randomly assigned but were given conventional r - chop treatment and followed up with the same assessments as participants in the control group , but analysed as a distinct group . 
participants , investigators , and treating clinicians were unmasked to the treatment allocation ; however , local investigators were not informed which molecular subgroup the participants were in . procedures participants underwent routine staging investigations , including ct scans and bone marrow biopsy , with examination of cerebrospinal fluid as clinically indicated . 
 tumour material was sent to the central laboratory ( haematological malignancy diagnostic service , leeds cancer cancer centre , leeds teaching hospitals , leeds , uk ) for gene - expression profiling and somatic mutation assessment . for cycle one , all participants received the r - chop regimen on a 21 - day schedule . 
the regimen comprised rituximab 375 mg / m intravenously , cyclophosphamide 750 mg / m intravenously , doxorubicin 50 mg / m intravenously , and vincristine 14 mg / m ( maximum total dose 2 mg ) intravenously on day 1 of the cycle , and prednisolone 100 mg orally once daily on days 15 . 
 from cycle 2 onwards , participants were randomly assigned to their treatment groups , either to receive five further cycles of r - chop in the control group , or five cycles of r - chop plus bortezomib ( rb - chop ) on days 1 and 8 ( 13 mg / m intravenously or 16 mg / m vol 20 may 2019 articles subcutan eously ) in the experimental group . 
further cycles were given when neutrophils had recovered to 10 10 per l and platelets to 100 10 per l ; dose reductions of bortezomib in response to neurotoxicity were closely specified according to severity of this toxicity ( appendix pp 4853 )  . on feb 28 , 2014 , we changed the route of bortezomib from intravenous to subcutaneous administration and updated the protocol after publication of data7 that suggested subcutaneous administration was associated with decreased toxicity and similar efficacy at a lower dose , and greater acceptability to patients , as compared with intravenous administration.8 patients who were already being given intraveous bortezomib continued on formulation . 
intrathecal prophylaxis with methotrexate was recommended for patients at high risk of cns relapse for three to six cycles and could be given at any time at investigators discretion at each study site . 
cross - sectional imaging was repeated 1 month after administration of the final dose of chemotherapy to assess disease response using the international working group response criteria for nonhodgkin lymphoma9 and repeated at 12 months . participants were assessed clinically at the beginning of each treatment cycle and after treatment completion every 3 months for 1 year and thereafter every 6 months until 5 years total follow - up . 
progressions were recorded after clinical assessment and imaging , determined by local investigators , according to standard criteria , 9 and at progression trial treatment was discontinued and patients were followed up until data cut off for survival . histological haematoxylin and eosin sections from formalin - fixed paraffin - embedded ( ffpe ) samples taken at diagnosis were reviewed in the central laboratory as a quality check . 
rna was extracted using an ambion recoverall total nucleic acid isolation kit for ffpe ( thermofisher , waltham , ma , usa ) according to the manufacturers protocol , with the exception that two washes in xylene and alcohol were used to remove wax , with extended digestion in proteinase k overnight . during cycle 1 of r - chop , gene - expression profiling was done ( by sb ) using illumina whole genome cdnamediated annealing , selection , extension , and ligation ( dasl ) assay ( illumina , san diego , ca , usa )  . 
patient samples were classified as activated b - cell , germinal centre b - cell , unclassified , or fail ( ie , insufficient quality or quantity of dna or failure of dasl array ) by use of the dasl automated classifier as previously described , 10 with a quality control of a score over 1 to define technical failure . 
the confidence of each sample being one of the three classes was recorded and the final classification was defined as that with the highest confidence score . for tissue micorarrays when possible , we used tissue from the biopsy sample immunohistoto construct chemistry , fluorescence in - situ hybrid isation , and dna extraction . 
specifically , we did immunohistochemistry for myc and bcl2 protein ( dual ) expression using these tissue micorarrays and abcam rabbit monoclonal antibodies ( abcam , cambridge , uk ; clone y69 ) , with a cutoff of 40% or more , and dako anti - bcl - 2 monoclonal antibodies ( agilent , santa clara , usa ; clone 124 ) with a cutoff of 50% or more , scored by two independent assessors according to recognised criteria . 
these cutoff values were used to identify categories of myc and bcl2 gene expression : high or average . dna was extracted from tumour cells enriched by microdissection on ffpe tissue sections and its quality was assessed by pcr of variously sized genomic fragments . 
a panel of 70 genes that are recurrently mutated in aggressive b - cell lymphomas were investigated for mutation by targeted sequencing using haloplexhs target enrichment ( agilent technologies , santa clara , ca , usa ) and illumina hiseq sequencing , as described previously.11 this process was carried out for participants who had dna available of adequate quantity and quality . 
duplicate experiments were done for samples of lower quality , including all those with quality control pcr showing amplification of 300 bp or fewer genomic fragments , and only those mutations that were repro ducible in both experiments were reported . 
variant calling , single nucleotide polymorphisms , and back ground noise filtering were done as previously described.11 in a further 22 samples , mutations in 20 genes ( included in the above panel of 70 genes ) were analysed in duplicate using fluidigm multiplex pcr ( fluidigm , south san francisco , ca , usa ) and illumina miseq sequencing , as described previously , because of evolution of molecular diagnostics during the study period.11 variants detected by use of these targeted sequencing methods were further assessed by use of functional prediction tools . 
as part of a post - hoc analysis , samples were tested for the possible presence of primary mediastinal lymphoma using a bayesian predictor described by the lymphoma molecular profiling project to ensure that no molecular cases of primary mediastinal lymphoma had been included.12 safety was assessed by the recording and grading of adverse events according to the common terminology criteria for adverse event reporting version 4.0 at each study visit , or between visits if notified . 
serious or severe adverse events , including mention of suspected unexpected serious adverse reactions were defined as per the medicines for human use ( clinical trials ) regulations 2004 . outcomes the primary endpoint was 30 - month progression - free survival in the germinal centre and activated b - cell popualtion , defined as time from registration to the date of progression or death from any cause . 
disease progression was determined using the international working group response criteria for non - hodgkin lymphoma.9 participants free from progres sion or death were censored at the date of their last visit . 
secondary outcomes were 30 - month progression - free survival by cell - of - origin subgroup ; the time - to - event variables of overall survival , event - free survival , disease - free survival , and time to progression ; response duration ; complete and overall proportion of patients who achieved a response ; assessment of toxicity ; quality of life ; assess ment of peripheral neuropathy up to 30 days after last treatment ; and safety . 
the proportion of patients who achieved a complete and overall response , duration of response , event - free survival , disease - free survival , time - to - progression , and quality - of - life assessments will be reported elsewhere . 
 statistical analysis we used an adaptive design based on a two - stage approach , with two interim analyses to explore the safety and efficacy in the germinal centre b - cell group treated with rb - chop after a defined number of events . 
if progression - free survival at 12 months was assessed to be below 70% in this subgroup , the trial would stop recruiting into the germinal centre b - cell group . 
the second interim analysis was to take place when 73 patients in the germinal centre b - cell group had been randomly assigned to receive rb - chop and followed up for 1 year . 
 if the progression - free survival at 12 months was assessed to be below 85% in this subgroup , the trial would stop recruiting into the germinal centre b - cell group . the trial was powered to detect an improvement in progression - free survival at 30 months of 10% in the combined activated b - cell and germinal centre b - cell groups , from 75% in the r - chop group to 85% in the rb - chop group ( corresponding to a hazard ratio [ hr ] of 056 ) , on the basis of a log - rank test with a significance level of 5% ( two - sided ) and 90% power , requiring a total of 129 events . 
the intention - to - treat ( itt ) population comprised all patients for whom geneexpression profiling was attempted ( classified as activated b - cell , germinal centre b - cell , or unclassified subgroups , or for whom gene - expression profiling failed )  . 
the safety population was formed of all patients in the itt population who received at least one dose of any study drug . we assessed the primary outcome of 30 - month progression - free survival in a modified itt ( mitt ) population comprising the activated and germinal centre b - cell subgroups who were randomly assigned to receive treatment , using a cox proportional hazards model , adjusted for cell - of - origin subtype and ipi score . secondary outcome analyses included repeating the primary outcome analysis in the activated b - cell itt population alone , the germinal centre b - cell itt population , and the unclassified itt population , adjusting for ipi score only . 
we used summary statistics to describe baseline chara cteristics for participants in the r - chop group , rb - chop group , and patients for whom gene - expression profiling had failed in the itt population , and by cell - of - origin subgroups in the itt population , with formal com parisons between cell - oforigin subgroups using pearson tests . 
 further post - hoc analyses included repeating the primary outcome analysis and adjusting for time from diagnosis to the start of treatment to ascertain whether or not the interval from diagnosis to treatment affected the progression - free survival outcome . 
we also did post - hoc analyses to assess progression - free survival and overall survival by treatment group in the mitt population in the ipi low , intermediate , and high score groups , assessed using a cox proportional hazards model , adjusted for cellof - origin subtype , and also repeated the primary outcome analysis excluding patients who had a dose reduction in any treatment drug . 
rb - chop = rituximab , bortezomib , cyclophosphamide , doxorubicin , vincristine , and prednisolone . com paring double - expressor lymphomas to all other cases , separated by treatment group ; and comparing by treat ment groups in subgroups with mutations in components of the nf - b pathway . we used stata statistical software ( version 15.1 ) for all analyses . 
 the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results between june 2 , 2011 , and june 10 , 2015 , of 3449 patients assessed for eligibility , 1128 ( 327% ) participants were registered to the study ( figure 1 )  . 
of the registered participants , a further 52 who received one cycle of r - chop were excluded for reasons including ineligibility after tumour biopsy ( n = 29 ) and insufficient tumour data 654 vol 20 may 2019 articles ( n = 5 )  . 
158 ( 147% ) of 1076 remaining participants had inadequate sample material for gene - expression profiling and so were excluded from subsequent random assignment to treatment , and instead given r - chop as per the control group . 
918 ( 853% ) of 1076 participants were stratified by cell - of - origin subtype and ipi and randomly assigned to receive r - chop or rb - chop ( figure 1 )  . 
overall , 244 ( 266% ) patients had activated b - cell disease , 475 ( 517% ) had germinal centre b - cell disease , and 199 ( 217% ) had unclassified disease . 
the planned interim analyses and safety assessments by the data monitoring and ethics committee in the germinal centre b - cell group showed the 1 - year progression - free survival to be 70% or above in the germinal centre b - cell subgroup at the first interim analysis and the 1 - year progression - free survival to be 85% or above in the germinal centre b - cell subgroup at the second interim analysis . 
hence , the trial continued to recruit to all groups . baseline characteristics were similar between the control group , experimental group , and non - randomised participants ( table 1 )  . 
for the samples from which sufficient material was extracted , only 1% ( 11 of 1076 ) failed for technical reasons . we observed clinical differences between the molecular subgroups ( table 2 )  . 
median age was higher in the activated b - cell subgroup ( p = 00045 ) and bulky disease occurred more often in the germinal centre b - cell subgroup ( p < 00001 )  . 
no significant difference was seen between the activated and germinal centre b - cell subgroups in the distribution of ipi risk group , serum lactate dehydrogenase ( ldh ) concentration above the upper limit of normal , conventional stage of disease , overall prevalence of extranodal disease , or ecog performance status ( table 2 ; appendix p 6 )  . 
post - hoc testing for the possible presence of primary mediastinal lymphoma identified 19 participants who fulfilled the criteria , 12 of whom 13 ( 68% ) had mediastinal disease . 
of these participants , 14 ( 74% ) had been allocated to the germinal centre b - cell group and five ( 26% ) to the unclassified subgroup . the primary efficacy outcome was analysed when the combined activated and germinal centre b - cell mitt population had been followed up for a median of 30 months , as stipulated in the protocol ( median follow - up 297 months [ 95% ci 290320 ] ; median follow - up of survivors : 294 months [ 286311 ] )  . 
we saw no difference in pro gression - free survival in the combined activated and germinal centre b - cell populations between the r - chop and rb - chop groups ( hr 086 , 95% ci , 95% ci 065113 ; p = 028 ; adjusted hr 084 , 95% ci 064111 ; p = 023 )  . 
after this additional follow - up , the kaplan - meier estimate for 30 - month progression - free survival in the combined activated and germinal centre b - cell mitt population was 706% ( 95% ci 655750 ) for the r - chop group and 752% ( 703794 ) for the rb - chop group . 
we saw no evidence of difference in 30 - month progression - free survival in the mitt population between the r - chop and rb - chop groups ( adjusted hr 082 , 95% ci 063108 ; p = 016 ; figure 2a )  . secondary analysis of subtypes by cell of origin showed that bortezomib did not significantly affect progressionfree survival in either the activated b - cell ( adjusted hr 078 , 95% ci 051121 ; p = 027 ) , germinal centre b - cell ( 085 , 060120 ; p = 035 ) , or unclassifiable participants ( 129 , 95% ci 077216 ; p = 034 ; figure 2 )  . 
 we saw no difference in overall survival by treatment group in the mitt population ( 72 deaths in the r - chop group and 61 in the rb - chop group ; adjusted hr 082 , 95% ci 059116 ; p = 027 ) , and the kaplan - meier estimate of overall survival at 30 months was 816% ( 95% ci 771853 ) in the r - chop group versus 831% ( 787867 ) in the rb - chop group ( appendix p 3 )  . the addition of bortezomib to r - chop was well tolerated ( table 3 )  . 
the most common grade 3 or worse adverse event was haematological toxicity , in 178 ( 398% ) of 447 patients given r - chop and 187 ( 421% ) of 444 given rb - chop . 
however , in a post - hoc analysis of adverse events between groups , we saw no significant increase in the proportion of patients who had grade 3 or worse neutropenia , febrile neutropenia , thrombo cytopenia , or anaemia . 
neuropathy of any grade was more frequent in participants given rb - chop than among those given r - chop ( 252 ( 568% ) rb - chop vs 186 ( 416% ) given r - chop ; p < 00001 ; appendix pp 811 ) but there was no significant difference in the event rate of neuropathy of grade 3 or higher ( 17 ( 38% ) rb - chop vs eight ( 18% ) r - chop ; p = 0070 )  . 
nine suspected unexpected serious adverse reactions were reported : four reactions in four participants in the r - chop group ( haemophagocytic syndrome , leukaemia secondary to chemotherapy , neutropenic sepsis , and fracture ) , and five reactions in four participants in the rb - chop group ( jejunal stricture with small bowel obstruction , bowel perforation , sepsis , and one patient had both renal failure and tumour lysis syndrome )  . 
in the safety population , 73 ( 163% ) of 447 participants in the r - chop group and 68 ( 153% ) of 444 in the rb - chop group died , with most deaths due to progressive lymphoma ( 50 [ 685% ] of 73 in the r - chop group , and 54 [ 794% ] of 68 in the rb - chop group ) ; nine treatment - related deaths were reported ( five [ 68% ] of 73 in the r - chop group , four [ 59% ] of 68 in the rb - chop group ; appendix p 13 )  . in the itt population , fewer participants in the r - chop group had dose reductions in any drug than did those in the rb - chop group ( 158 [ 345% ] of 459 vs 196 [ 429% ] of 459 , not including the non - randomsied participants ; appendix p 12 )  . 
fewer participants discon tinued from trial treatments in the r - chop group than in the rb - chop group ( 43 [ 94% ] vs 60 [ 131% ] ; appendix p 11 )  . 
however , median relative dose intensity for participants in the control and experimental groups was similar for drugs comprising r - chop and a high proportion of participants in both groups success fully completed six cycles of treatment : 418 ( 913% ) of 459 in the r - chop group and 398 ( 871% ) of 459 in the rb - chop group ( appendix p 12 )  . the median time from diagnosis to first treatment was similar between treatment groups ( r - chop 17 days [ iqr 1029 ] ; rb - chop 20 days [ 1032 ] )  . 
post - hoc analyses , repeating the primary analysis and adjusting for the time from diagnosis to first treatment interval also showed no difference in 30 - month progression - free survival in the mitt population between the r - chop and rb - chop groups ( 706% , 95% ci 655750 for r - chop , and 752% , 703794 for rb - chop ; adjusted hr 083 , 95% ci 056124 ; p = 036 )  . 
similarly , post - hoc analyses excluding patients who had a dose reduction in any treatment drug showed no difference in 30 - month progression - free survival the mitt population between the r - chop and rb - chop groups ( 689% , 95% ci 624745 for r - chop and 743% , 658810 for rb - chop ; adjusted hr 080 , 95% ci 054119 ; 656 vol 20 may 2019 articles p = 027 )  . 
post - hoc analysis of progression - free survival and overall survival by ipi score are shown in the appendix ( p 4 )  . the panel of genomic mutations confirmed the known association of different somatic changes with cell - oforigin subtypes , with a bias towards alterations in epigenetic modifier genes in the germinal centre b - cell subgroup and genes of the b - cell receptor signalling pathway in the activated b - cell subgroup ( appendix pp 2 , 6 , 7 )  . 
mutations in ezh2 were seen in 250% ( 53 of 212 ) of germinal centre b - cell biopsy samples but only 42% ( five of 118 ) of activated b - cell samples , and conversely mutations in myd88 were found in 90% ( 19 of 212 ) of germinal centre b - cell and 449% ( 52 or 118 ) of activated b - cell samples tested ( appendix pp 1 , 6 , 7 )  . 
 nf - b target genes were expressed at higher levels in the activated b - cell subgroup compared with the germinal centre b - cell group ( appendix p 2 )  . 417 biopsy samples ( 118 from the activated b - cell subgroup , 212 from the germinal centre b - cell subgroup , and 87 from the unclassified subgroup ) were suitable for construction of tissue microarrays . 
karyotypic double - hit lymphomas were rare in the activated b - cell population and were significantly associated with the germinal centre b - cell subtype ( one [ 04% ] of 244 vs 32 [ 67% ] of 475 ; p < 00001 )  . 
 conversely , the activated b - cell subtype was associated with higher concomitant expression of myc and bcl - 2 proteins ( ie , double - expressor lymphomas ) than the germinal centre b - cell subtype was by immuno histochemistry analysis ( excluding double - hit lymphomas ; 56 [ 549% ] vs 45 [ 26% ] ; p < 00001 ) and mrna ( 109 [ 447% ] vs 87 [ 183% ] ; p < 00001 ; appendix p 13 )  . 395 biopsy samples had sufficient dna of adequate quantity and quality for investigation of mutations via targeted sequencing . 
among the participants given r - chop ( including the non - randomised group ) , myc rearrangement , double - hit lymphoma , and dual high myc and bcl - 2 mrna expression were significantly associated with inferior progression - free survival after controlling for ipi ( data not shown )  . 
rb - chop = rituximab , bortezomib , cyclophosphamide , doxorubicin , vincristine , and prednisolone . table 3 : adverse events in the safety population lymphoma in the same treatment group without these rearrangements ( double - hit lymphoma in the r - chop group : 389% vs 758% , adjusted hr 307 , 95% ci 164576 ; p = 000048 ; and dual - expressor the r - chop group : 615% vs 758% , adjusted hr 181 , 126260 ; p = 00013 ; figure 3 )  . 
high con centrations of myc and bcl - 2 proteins by immunohistochemistry did not appear to have a significant effect on outcomes , although few participants had high concentrations of these proteins , resulting in wide confidence limits ( figure 4 )  . 
the effect of bortezomib on progression - free survival in these high - risk groups is shown in figure 4 . we examined the effect of the addition of bortezomib on survival in patients with mutations known to be associated with activation of nf - b , the putative target of bortezomib ( myd88 , cd79a , cd79b , tnfaip3 , tnfrsf11a ) and found no significant differences for single gene alterations ( appendix p 5 )  . discussion in this trial , we have shown the feasibility of molecular phenotyping in a large multicentre study of rapidly progressive tumours and shown that the addition of bortezomib does not affect treatment outcomes in most patients with diffuse large b - cell lymphoma . 
because patients entering clinical trials are often not representative of the wider population , for prospective testing of a complex biomarker we wished to avoid worsening the problem of generalisability by restricted enrolment and delays to the initiation of therapy . 
such delays were avoided by studying routine ffpe biopsy samples and deferring random assignment to a treatment group until the second cycle of r - chop , thereby allowing treatment to start as soon as staging investigations were completed , with molecular analysis taking place in parallel . 
rb - chop = rituximab , bortezomib , cyclophosphamide , doxorubicin , vincristine , and prednisolone . basis of their molecular phenotype will require real - time outputs , which we have shown to be feasible in this trial . 
 using a central laboratory and the dasl automated classifier , we prospectively assigned cell - of - origin categories within a clinically relevant timeframe , which allowed random assignment to treatment to be stratified by cell - of - origin subtype , with the potential for adaptive design based on interim analyses of molecular subtypes . 
the slight increase in neurotoxicity observed in participants in the rb - chop group compared with the r - chop group suggests that the bortezomib was given at a biologically active dose . 
 bortezomib was administered on days 1 and 8 of cycles 25 , at a dose that has shown efficacy in other lymphoma trials , 19 , 20 but we recognise that more potent proteasome inhibitors are now in use , as are other agents with apparent preferential effects in the activated b - cell subgroup , such as lenalidomide and ibrutinib , trials of which are in pro gress ( nct02285062 , nct01855750 )  . bortezomib did not improve outcomes for participants with the activated b - cell subtype of diffuse large b - cell lymphoma , which was confirmed to be enriched for expression of nf - b target genes , or for patients with somatic mutations associated with nf - b activation . 
 inhibition of nf - b might be insufficient to improve outcomes in addition to r - chop in diffuse large b - cell lymphoma , or bortezomib at the doses given might not have been sufficient to inhibit nf - b adequately for outcomes to improve . 
another study in patients with non - germinal centre b - cell lymphoma , selected by immunohistochemistry , did not show a difference between r - chop and the combination of rituximab , cyclophosphamide , doxorubicin , and prednisone ( r - chp ) with bortezomib given in place of vincristine , supporting our finding.20 studies1820 have shown the difficulty of improving the results of initial therapy in diffuse large b - cell lymphoma by the addition of novel drugs that had promising activity in studies treating recurrent disease with a single 660 vol 20 may 2019 articles treatment group . 
this situation might partly reflect biological selection through treatment failure : in relapsed or refractory lymphomas for which new drugs are investigated , the biology of such disease is likely to be different from that of newly diagnosed lymphomas . 
 thus , most germinal centre b - cell diffuse large b - cell lymphoma can be cured by r - chop , whereas recurrent disease is more common for those with double - hit lymphoma . 
similarly , recurrent activated b - cell diffuse large b - cell lymphoma is enriched for double - expressor lymphomas , which might account for the different results reported in our study compared with the previous studies of bortezomib treatment . 
this observation highlights the need for full molecular char acterisation of the disease being treated , both at diagnosis and in the event of initial treatment failure . in this study , the presence of a small number of participants with double - hit lymphoma in the germinal centre b - cell subgroup lowered the progression - free survival estimate for this subgroup . 
overall , however , the progression - free survival outcome for the patients with double - hit lymphoma appears to be better than that reported in some earlier studies21 and is consistent with more recent analyses.22 , 23 although clearly worse than the non - rearranged group , nearly half of double - hit lymphomas appeared to have not progressed at 30 months . 
the progression - free survival at 30 months in patients with double - hit lymphoma was 389% after r - chop compared with 588% after rb - chop , although this result was from a post - hoc analysis and was not statistically significant ( data not shown )  . this study had several limitations . 
any clinical trial is potentially prone to selective recruitment of those patients with better prognoses , but we endeavoured to minimise this effect by deferring random assignment to treatment until the second cycle of therapy , thereby allowing rapid initiation of treatment at the same time as molecular typing . 
as a result , the median time from diagnosis to initiation of therapy was lower than in similar studies , 24 and the distribution of ipi scores in this study was similar to or worse than recent trials , 2 , 18 with 47% of patients being high - intermediate or high risk . 
we were unable to do a comprehensive central histopathology review on the participants enrolled and we did not assess for the presence of epstein - barr virus in the biopsy samples . 
however , all participants were diagnosed by expert haemato pathologists by use of a procedure with high accuracy for diffuse large b - cell lymphoma ( over 96% in a recent case series from the uk25 ) , and because epstein - barr virus is present in less than 3% of diffuse large b - cell lymphoma in europe , 26 the presence of the virus would be unlikely to affect our results . 
the rb - chop group had a slight excess of vincristine dose reductions compared with the r - chop group , which could potentially have eroded a positive effect from the bortezomib . 
the use of routine ffpe biopsy samples was necessitated by the large number of recruiting centres , but resulted in a failure rate of about 15% for molecular typing and might have resulted in a larger than expected number of unclassified cases for whom poor quality rna resulted in a low probability score in the cell - of - origin classifier . in conclusion , this trial has shown that complex molecular characterisation can be done in real time , with a pragmatic treatment schedule that allows for the allocation of therapy on the basis of the molecular subtype . 
this method is likely to become increasingly relevant as our understanding of the phenotypic diversity of diffuse large b - cell lymphoma expands to encompass not only cell of origin , but also other biologically distinct categories based on genomic alterations.15 , 27 , 28 future trials that use such methods will be important to explore the mechanisms of action of investigational drugs and to redefine the groups in which they are most likely to be effective . 
the poor prognosis of double - hit lymphomas could be seen as a potential opportunity for such an approach . contributors pwmj and ad designed the study , oversaw the study , and contributed to data interpretation , writing and approval of the report . 
tec and gg contributed to data analysis , interpretation , writing of the report , and oversaw work at the southampton clinical trials unit ( southampton , uk )  . 
all authors have reviewed and approved the final version of the report . declaration of interests ad reports grants and personal fees from janssen , bayer , adc therapeutics , roche , celgene , acerta , gilead , and personal fees from kite and morphosys . 
gpc reports grants from celgene , amgen , pfizer , and celleron , and personal fees from takeda , roche , gilead , bristol - myers squibb , and merck sharpe and dohme . 
am reports personal fees from roche , celgene , novartis , bristol - myers squibb , merck sharpe and dohme , sandoz , gilead , janssen , amgen , and takeda , and grants and personal fees from pfizer . 
pwmj reports grants from janssen , bloodwise , and epizyme , and personal fees from takeda , bristol - myers squibb , novartis , celgene , boeringher ingelheim , kite pharmaceuticals , genmab , and incyte . 
individual participant data will be shared that underlie the results reported in this article , after vol 20 may 2019 articles de - identification and normalisation of information ( text , tables , figures , and appendices )  . 
anonymised data will be available beginning 3 months after and ending 5 years after publication of this article to researchers who provide a completed data sharing agreement that describes a methodologically sound proposal for the purpose of the approved proposal . 
data sharing requests are available for 5 years via the southampton clinical trials unit website . acknowledgments the trial was funded by an educational grant from janssen - cilag and endorsed by cancer research uk after independent peer review ( c328 / a12128 )  . 
a worldwide collaboration to harmonize guidelines for the long - term follow - up of childhood and young adult cancer survivors : a report from the international late effects of childhood cancer guideline harmonization group . 
eur j cancer 2007 ; 43 : 1778 - 80 . interrogating molecular data for medulloblastoma risk stratification medulloblastoma is the most common malignant paediatric brain tumour , with an incidence between 234 and 596 per million population.1 early studies on medulloblastoma biology were largely inconclusive because of its molecular heterogeneity and the small size of the cohorts analysed . 
 indeed , on the basis of gene expression , genetic aberrations , and dna methylation , medulloblastoma is now classified into several molecular subgroups.25 the 2016 who classification of tumors of the central nervous system6 combines molecular and histological features for an innovative integrated diagnosis , thus allowing stratification of patients into four prognostic risk categories : favourable , standard , high , and very high risk.3 heterogeneous , comprising 5060% of patients with medulloblastoma and encompassing shh - activated tp53wild - type and groups 3 and 4 , in the absence of highrisk features ( ie , myc amplification , anaplastic histology , or metastasis at diagnosis )  . 
 micrornas and long non - coding rnas have been shown to be important regulators of medulloblastoma biology , and could represent valuable biomarkers for risk stratification and targeted therapy.10 in conclusion , this study8 provides a tool for immediate clinical application . 
although these results require validation in a controlled multicentre study , they set the foundation that is needed to improve genomic patient characterisation for more accurate risk stratification in routine clinical settings . * elisabetta ferretti , agnese po department of experimental medicine ( ef ) and department of molecular medicine ( ap ) , sapienza university of rome , rome 00161 , italy ; and irccs neuromed mediterranean neurological institute , pozzilli , italy ( ef ) elisabetta.ferretti@uniroma1.it we declare no competing interests . copyright 2018 the author ( s )  . 
nearly half of patients at diagnosis have metastases , with a 5 - year overall survival of only 50% , despite therapeutic advances.1 initial improvements to outcome were achieved by the introduction of consolidation with myeloablative chemotherapy and autologous haemopoietic stemisotretinoin , a cell transplantation , followed by targeted therapy with differentiating agent used to treat minimal residual disease.2 next , anti - glycolipid disialoganglioside ( gd2 ) monoclonal antibodies was tested in resistant tumours . 
a worldwide collaboration to harmonize guidelines for the long - term follow - up of childhood and young adult cancer survivors : a report from the international late effects of childhood cancer guideline harmonization group . 
eur j cancer 2007 ; 43 : 1778 - 80 . interrogating molecular data for medulloblastoma risk stratification medulloblastoma is the most common malignant paediatric brain tumour , with an incidence between 234 and 596 per million population.1 early studies on medulloblastoma biology were largely inconclusive because of its molecular heterogeneity and the small size of the cohorts analysed . 
 indeed , on the basis of gene expression , genetic aberrations , and dna methylation , medulloblastoma is now classified into several molecular subgroups.25 the 2016 who classification of tumors of the central nervous system6 combines molecular and histological features for an innovative integrated diagnosis , thus allowing stratification of patients into four prognostic risk categories : favourable , standard , high , and very high risk.3 heterogeneous , comprising 5060% of patients with medulloblastoma and encompassing shh - activated tp53wild - type and groups 3 and 4 , in the absence of highrisk features ( ie , myc amplification , anaplastic histology , or metastasis at diagnosis )  . 
 micrornas and long non - coding rnas have been shown to be important regulators of medulloblastoma biology , and could represent valuable biomarkers for risk stratification and targeted therapy.10 in conclusion , this study8 provides a tool for immediate clinical application . 
although these results require validation in a controlled multicentre study , they set the foundation that is needed to improve genomic patient characterisation for more accurate risk stratification in routine clinical settings . * elisabetta ferretti , agnese po department of experimental medicine ( ef ) and department of molecular medicine ( ap ) , sapienza university of rome , rome 00161 , italy ; and irccs neuromed mediterranean neurological institute , pozzilli , italy ( ef ) elisabetta.ferretti@uniroma1.it we declare no competing interests . copyright 2018 the author ( s )  . 
nearly half of patients at diagnosis have metastases , with a 5 - year overall survival of only 50% , despite therapeutic advances.1 initial improvements to outcome were achieved by the introduction of consolidation with myeloablative chemotherapy and autologous haemopoietic stemisotretinoin , a cell transplantation , followed by targeted therapy with differentiating agent used to treat minimal residual disease.2 next , anti - glycolipid disialoganglioside ( gd2 ) monoclonal antibodies was tested in resistant tumours . 
gd2 is highly expressed on the surface of neuroblastoma cells , with normal tissue expression restricted to neurons , sensory nerve fibres , and melanocytes , thus creating an attractive target for published online november 12 , 2018 s1470 - 2045 ( 18 ) 30627 - 2 see articles page 1617 vol 19 december 2018 1549 comment correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections for cancer waiting time statistics in england see statistical - work - areas / cancerwaiting - times / ; in scotland see health - topics / waiting - times / cancer / ; in wales see wales / statistics - and - research / nhs - activity - performancesummary / ? skip = 1&lang = en for the general medical council study findings see theguardian.com / society / 2017 / nov / 26 / safety - fears - as - juniordoctors - left - to - run - aes - andother - hospital - units for the lancet oncology editorial see lancet oncol 2015 ; 16 : 1273 for the nhs statement about the budget see theguardian.com / society / 2017 / nov / 30 / nhs - bosses - waiting - timetargets - abandoned - next - year the nhs : failing to deliver on beveridges promise ? just over 75 years have passed since sir william beveridge published his report outlining the parameters for a social welfare state for the uk , which crucially included comprehensive health and rehabilitation services for prevention and cure of disease . 
although the vision of beveridge and bevanto provide free , adequate , and equally accessible health care for allremains in high regard today , the execution and delivery of their goal is currently falling short . 
is the uk in danger of losing the nhs because the government is uninterested in or incapable of the effort needed to save it ? 2017 was a year of great difficulty for the nhs . 
 moreover , and worryingly , in december , 2017 , cancer x - ray diagnostic services came under national review by the care quality commission , after the discovery that between april 1 , 2016 , and march 31 , 2017 , more than 20 000 x - ray images had not been reviewed by a radiologist or properly trained clinician . 
indeed , a study from the general medical council has shown that , due to chronic staff shortages , inexperienced doctors without sufficient training or competence are being left in charge of hospital departments . 
it is thus hardly surprising that nearly 1000 patients have received cancer misdiagnosis settlements totalling 757 million in the past 10 years and that the cost of the nhs clinical negligence scheme has in 200607 to 16 billion in 201617 . increased from 400 million such issues are regrettably reminiscent of nhs difficulties that we highlighted in a previous editorial in october , 2015 . 
long - term underfunding , which in turn has led to deficiencies prevalent for decades in staffing , training , and infrastructure , has been at least partly responsible for this deficit of care . 
 however , analyses indicate that real - term spending on the nhs is decreasing or remaining stagnant , while demand is increasing by up to 7% per year , fuelled by a growing and ageing population with a rising incidence indeed , as high as this of chronic comorbidities . 
 budgetary addition might seem , it will barely cover the cost of the clinical negligence scheme alone and will not get to the root of the problem or provide a net benefit to the systeas service needs rise and resources remain the same , services will exceed capacity and become potentially unsafe . in the late 1940s , with a world war in recent memory , british society was in favour of a social welfare state and there was near cross - party governmental support to provide services such as the nhs . 
 in response to the provision in the 2017 autumn budget , nhs england issued a damning statementit would have to ignore waiting time limits , stop prescribing some over the counter medications , and would not be able to guarantee to act on any new nice guidance , all of which would breach the nhs constitution . 
 in terms of oncology recommendations , hunt did promise to hire 500 more cancer experts , but this addition barely covers current critical shortfalls in staffing , and does not address infrastructure or treatment requirements . 
 on dec 11 , 2017 , kings college hospital nhs foundation trust chairman lord robert kerslake resigned , telling the bbc that he believes the government and regulator are unrealistic about the scale of the challenge facing the nhs . 
yet nhs governance is not blamelessfurther funding is of no use if smart and judicious decisions are not made to ensure the service is optimised around efficiency , safety , and patients . 
it is a paradox that at a time when more and more countries aspire to universal health care that the country that spearheaded the model is moving further from it . 
 the lancet oncology vol 19 january 2018 editorial published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections articles germline brca mutation and outcome in young - onset breast cancer ( posh ) : a prospective cohort study ellen r copson * , tom c maishman * , will j tapper , ramsey i cutress , stephanie greville - heygate , douglas g altman , bryony eccles , sue gerty , lorraine t durcan , louise jones , d gareth evans , alastair m thompson , paul pharoah , douglas f easton , alison m dunning , andrew hanby , sunil lakhani , ros eeles , fiona j gilbert , hisham hamed , shirley hodgson , peter simmonds , louise stanton , diana m eccles summary background retrospective studies provide conflicting interpretations of the effect of inherited genetic factors on the prognosis of patients with breast cancer . 
the primary aim of this study was to determine the effect of a germline brca1 or brca2 mutation on breast cancer outcomes in patients with young - onset breast cancer . 
 methods we did a prospective cohort study of female patients recruited from 127 hospitals in the uk aged 40 years or younger at first diagnosis ( by histological confirmation ) of invasive breast cancer . 
clinicopathological data , and data regarding treatment and long - term outcomes , including date and site of disease recurrence , were collected from routine medical records at 6 months , 12 months , and then annually until death or loss to follow - up . 
the primary outcome was overall survival for all brca1 or brca2 mutation carriers ( brca - positive ) versus all non - carriers ( brca - negative ) at 2 years , 5 years , and 10 years after diagnosis . 
 recruitment was completed in 2008 , and long - term follow - up is continuing . findings between jan 24 , 2000 , and jan 24 , 2008 , we recruited 2733 women . 
there was no significant difference in overall survival between brca - positive and brca - negative patients in multivariable analyses at any timepoint ( at 2 years : 970% [ 95% ci 945984 ] vs 966% [ 958973 ] ; at 5 years : 838% [ 793875 ] vs 850% [ 835864 ] ; at 10 years : 734% [ 674785 ] vs 701% [ 677723 ] ; hazard ratio [ hr ] 096 [ 95% ci 076122 ] ; p = 076 )  . 
of 558 patients with triple - negative breast cancer , brca mutation carriers had better overall survival than non - carriers at 2 years ( 95% [ 95% ci 8997 ] vs 91% [ 8894 ] ; hr 059 [ 95% ci 035099 ] ; p = 0047 ) but not 5 years ( 81% [ 7387 ] vs 74% [ 7078 ] ; hr 113 [ 070184 ] ; p = 062 ) or 10 years ( 72% [ 6280 ] vs 69% [ 6374 ] ; hr 212 [ 082549 ] ; p = 012 )  . interpretation patients with young - onset breast cancer who carry a brca mutation have similar survival as non - carriers . 
decisions about timing of additional surgery aimed at reducing future second primary - cancer risks should take into account patient prognosis associated with the first malignancy and patient preferences . funding cancer research uk , the uk national cancer research network , the wessex cancer trust , breast cancer now , and the ppp healthcare medical trust grant . copyright the author ( s )  . 
on dec 5 , 2016 , we did another pubmed search for studies of patients who carried a brca1 or brca2 mutation and their prognosis , using the following search terms : ( brca ) and ( survival or prognosis or outcome or mortality ) and ( breast neoplasms or breast neoplasm or breast cancer or breast tumour )  . 
previous studies and meta - analyses have reported inconsistent effects of brca1 and brca2 mutations on the outcomes of early breast cancer with better , worse , and similar outcomes for patients with a brca1 or brca2 mutation compared with patients with sporadic breast cancer . 
these conflicting results might be explained by methodological issues with ascertainment biases introduced by retrospective and selective identification of cases , incomplete genetic testing , small numbers , an absence of adjustment for clinical variables , including treatment , and short follow - up . added value of this study posh is , to our knowledge , the largest prospective cohort study to compare breast cancer outcomes of patients with a brca1 or brca2 mutation with patients with sporadic cancer . 
however , in patients with triple - negative breast cancer , brca mutation carriers might have a survival advantage compared with non - carriers during the first few years after diagnosis . 
our study was strengthened by unbiased recruitment , universal and central genetic testing at the end of the study , and comprehensive pathological , clinical , and follow - up data . implications of all the available evidence decisions about timing of risk - reducing surgery should take into account primary tumour prognosis and patient preference . published studies and meta - analyses have reported better , worse , and similar outcomes for patients with a brca1 or brca2 mutation compared with patients with sporadic breast cancer.814 a comprehensive meta - analysis of 66 studies of breast cancer survival in patients with a brca1 or brca2 mutation compared with non - carrier patients or the general breast cancer population , which assessed study quality as well as outcome data , concluded that it is not yet possible to draw evidence based conclusions about the association between brca1 [ or ] brca2 mutation carriership and breast cancer prognosis.12 we undertook the prospective outcomes in sporadic versus hereditary breast cancer ( posh ) study , the primary aim of which was to determine the effect of inherited brca1 or brca2 mutations on outcomes in patients with young - onset breast cancer.15 , 16 methods study design and participants we did a prospective cohort study at 127 hospitals in the uk ( appendix pp 12 )  . 
potential recruits were identified by local breast cancer clinicians , nurses , or research clinical trial practitioners within 12 months of initial diagnosis of invasive breast cancer and the date of diagnosis was defined as the first histological confirmation of invasive breast cancer . 
ethical approval was granted in 2000 ( mrec 00 / 6 / 69 ) and the study was approved for recruitment as part of the uk national cancer research network ( ncrn ) portfolio in 2002 , subsequently the nihr portfolio . 
 the boadicea algorithm , without adjustment for pathological subtype , was used to estimate the probability that an individual might carry a brca1 or brca2 pathogenic variant.17 pathology and imaging data were verified with copies of the original reports from sites . 
for patients treated with neoadjuvant chemotherapy , the initial diameter of the tumour was derived from radiological reports . the oestrogen - receptor , progesterone - receptor , and her2 - receptor status of the primary tumours was determined from reports of local routine pathology testing of diagnostic core biopsies or tumour resections for clinical use . 
immunohistochemical staining of tissue microarrays in some cases enabled clinical source data for oestrogen - receptor , progesterone - receptor , and her2 - receptor statuses to be corroborated ; tissue microarray scores were used to supplement missing datapoints for these receptors.16 170 vol 19 february 2018 articles dna for genotyping was extracted from whole blood recruitment . 
a multiplex samples submitted at amplicon - based library preparation system , fluidigm access array ( fluidigm uk , cambridge , uk ) , targeted a panel of breast - cancer - susceptibility genes ( including brca1 , brca2 , and tp53 ) for sequencing using an illumina hiseq2500 next generation sequencing platform ( illumina , little chesterford , uk ; appendix pp 2021 )  . 
targeted - sequence capture cannot reliably identify large exonic deletions or duplications , therefore multiplex ligation probe analysis was used for patients who met current uk guideline thresholds for clinical genetic testing.17 , 18 predicted protein truncating variants ( frameshift , nonsense , and canonical - splice site and large rearrangements ) plus other variants ( mainly mis - sense ) unequivocally defined as pathogenic on the basis of multiple lines of evidence and expert review were assigned carrier group the brca - mutation ( brca - positive )  . 
all other patients , including those with brca1 or brca2 variants of uncertain significance or very low penetrance , were assigned to the same group as no mutation found ( brca - negative ) or excluded if they were found to carry a pathogenic variant of tp53 . 
 for the purposes of this analysis , mutations in other breast cancer genes were not curated . the study protocol and patient information specified that patients would not be informed of the research genetic - testing results ; however , patient information sheets gave information about seeking clinical genetic referral . 
 genetic test reports for the study patients generated by uk national health service ( nhs ) diagnostic laboratories were collected as part of the medical record . detailed clinical follow - up data , including date and site of disease recurrence , were obtained from medical records at 6 months , 12 months , and annually thereafter , until death or loss to follow - up . 
patients were flagged in the nhs medical research information service for automatic notification of date and cause of death . outcomes the primary outcome was overall survival , defined as the time from first diagnosis to death from any cause . 
 statistical analysis the original study sample size of a minimum of 2000 patients was estimated based on a prevalence of brca1 or brca2 pathogenic mutations of 10% , and an absolute difference in event rate at 2 years between mutation carriers and non - carriers of 10% ( 20% in mutation carriers compared with 10% in sporadic cases ) .15 we also considered a prevalence of brca1 or brca2 mutations of 5% and 15% , and larger sample sizes . 
good recruitment and data returns enabled us to continue study recruitment beyond 2000 participants providing sufficient power for multivariable analyses . ( m1 at presentation we did the statistical analyses according to a prespecified plan ( appendix pp 2231 ) .19 the analysis population included all eligible patients recruited to the cohort who had available data for the primary tumour and genotyping , were aged 40 years or younger at the date of diagnosis , did not carry a tp53 gene , and who did not present with stage )  . 
 metastatic disease a prespecified subgroup of the analysis population was patients with triple - negative breast cancer ( ie , oestrogenreceptor - negative , her2 - negative , and progesteronereceptor - negative or unknown )  . 
key patient data were described by brca mutation status , and formal comparisons by brca mutation status were done using mann - whitney tests ( for continuous variables ) and pearson tests ( for categorical variables ) for patients with complete data . 
the 2 - year comparison was chosen because this timepoint was specified for the original sample size ; the 5 - year and 10 - year comparisons were chosen because they are commonly used in such studies and are clinically relevant timepoints . 
hazard ratios ( hrs ) and 95% cis for 3095 patients recruited to posh 3021 eligible patients 74 patients excluded 72 no invasive breast cancer 1 non - mutation carrier aged 4150 1 diagnosed outside the study period 288 patients excluded from this analysis 160 no genotyping data available 74 m1 stage disease 10 tp53 mutation carriers 42 aged 4150 years 2 missing primary tumour data 2733 patients in the analysis population 338 brca - positive 558 patients with triple - negative breast cancer subgroup 136 brca - positive figure 1 : trial profile brca - positive = patient with brca1 or brca2 pathogenic mutation . 
additionally , to investigate the degree of potential bias from time of diagnosis testing at to blood draw for genetic registration , a multivariable analysis model adjusting for the time from diagnosis to blood draw was generated accordingly for the analysis population only . 
defined as oestrogen - receptor - negative , her2 - negative , and progesterone - receptor - negative or unknown . table 1 : baseline characteristics and clinicopathological information for all patients vol 19 february 2018 articles underwent patients who carriers , so we repeated the analysis in this subgroup bilateral excluding mastectomy within the first year after diagnosis . 
mann - whitney tests used for continuous variables and pearson - tests for categorical variables , done on patients with complete data . table 2 : baseline characteristics and clinicopathological information for patients with triple - negative breast cancer * submit it for publication . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results between jan 24 , 2000 , and jan 24 , 2008 , we recruited 3021 eligible women , of whom 2733 ( 91% ) were included in the analysis population , and 288 ( 9% ) were excluded ( figure 1 ; appendix p 11 )  . 
of 2721 patients for whom presentation was recorded , 45 ( 2% ) were recorded as being enrolled in a surveillance programme , and 33 ( 1% ) were recorded as having screen - detected breast cancer . 
 screening was offered according to local protocols ; national guidelines were not formally established until after recruitment ended . ( 13% ) had 338 ( 12% ) of 2733 patients included in the analysis population had either a brca1 or brca2 mutation , of whom 44 large - copy - number variants ( appendix pp 37 )  . 
75 ( 22% ) of 338 patients did not meet current family history or pathology based genetictesting guidelines.18 referral for a clinical genetics consultation and brca testing occurred for 388 patients ( 14% ) , of whom 182 ( 47% ) had a pathogenic mutation . 
immuno histo chemical staining of tissue microarrays in 1336 cases , during 2012 and 2016 , enabled clinical source data for oestrogen - receptor , progesterone - receptor , and her2 - receptor statuses to be corroborated . several significant the median time from breast cancer diagnosis to study registration blood draw was 55 months ( iqr 32107 )  . 
differences in tumour characteristics between brca1 and brca2 mutation carriers were also noted in patients with triple - negative breast cancer ( table 2 )  . median follow - up was 82 years ( iqr 6099 ) ; 91 ( 3% ) patients were lost to follow - up . 
contralateral breast tumours occurred in 151 ( 6% ) patients : in 37 ( 18% ) of 201 brca1 mutation carriers , 17 ( 12% ) of ( 4% ) of 137 brca2 mutation carriers , and 97 time 2395 brca - negative patients . 
there was no difference in overall survival between groups either before or after adjusting for known prognostic factors , including adjustments for ethnicity and body - mass index ( bmi ; univariable analysis negative vs positive hr 099 [ 95% ci 078124 ] , p = 090 ; multivariable analysis hr 096 [ 076122 ] , p = 076 )  . 
additionally , comparison of overall survival in brca - negative patients versus brca1 or brca2 carriers separately showed similar results ( appendix pp 1314 )  . survival between brca - positive than years in the subgroup of 558 patients with triple - negative breast cancer , 159 ( 28% ) women developed a distant recurrence , 153 ( 27% ) died , and all deaths were due to breast cancer . 
 overall survival at 5 years was 81% ( 95% ci 7387 ) versus 74% ( 7078 ; multivariable analysis flexible parametric survival model hr 113 [ 95% ci 070184 ] , p = 062 ) ; and at 10 years was 72% ( 6280 ) versus 69% ( 6374 ; multivariable analysis flexible parametric survival model hr 212 [ 95% ci 082549 ] , p = 012 ; figure 3 )  . 
for analyses of both the overall population and the subgroup of patients with triple - negative breast cancer , results with imputation were almost identical to complete case results ( appendix pp 910 )  . 
results from tests of proportional hazards are also in the appendix ( p 17 )  . a post - hoc , multivariable sensitivity analysis of overall survival in patients with triple - negative breast cancer excluding 31 ( 6% ) patients ( 21 brca - positive and ten brca - negative ) who underwent bilateral mastectomy within the first year after diagnosis showed a significant difference in overall survival at 2 years for brca - positive versus brca - negative patients ( 95% [ 95% ci 8998 ] vs 91% [ 8894 ] ; hr 052 [ 95% ci 029091 ] , p = 0023 )  . 
 002 reduced risk increased risk figure 2 : overall survival for all patients ( analysis population ) by brca mutation status ( a ) kaplan - meier plot and ( b ) forest plot of corresponding univariable and multivariable hazard ratios . 
in ( b ) , multivariable analysis was adjusted for age , body - mass index ( bmi ; kg / m ) , grade , tumour size , her2 status , oestrogen - receptor status , ethnicity , and use of taxane chemotherapy . 
oestrogen - receptor - positive group assessed at 2 , 5 , and 10 years because the hazard ratio associated with oestrogen - positive status varies with time.16 hr = hazard ratio . 
 * number of events ( number of patients ) from complete data obtained before multiple imputation . six ( 3% ) of 201 new primary cancers in brca1 mutation carriers ( three ovarian , one primary peritoneal , one oesophageal , and one pancreatic ) and 12 ( < 1% ) of 2395 malignancies in brca - negative patients ( four haema tological , three lung , and one each of brain , colorectal , gastric , pancreatic , and sarcoma ; appendix p 8 )  . 
 176 vol 19 february 2018 articles brca negative brca positive we also repeated the primary analysis in patients with triple - negative breast cancer excluding 37 ( 7% ) patients who developed a new primary breast or ovarian cancer . 
 overall survival at 10 years for brca - positive versus brca - negative patients was 78% ( 95% ci 6985 ) versus 69% ( 6474 ; hr 124 [ 95% ci 039396 ] , p = 073 ; appendix p 19 )  . discussion the posh prospective cohort study showed no significant difference in overall survival or distant disease - free survival between patients carrying a brca1 or brca2 mutation and patients without these mutations after a diagnosis of breast cancer . 
these results did not vary between unadjusted or adjusted analyses , including adjustments for ethnicity and bmi.21 , 22 following a diagnosis of early breast cancer , brca mutation carriers are frequently offered additional management options including bilateral mastectomy . 
furthermore , clinical trials of treatments that are specifically targeted toward brca mutation carriers might need to take into account any effect of brca mutational status on primary treatment outcomes . to our knowledge , this is the largest prospective study to report the prognostic implication of germline brca mutations and the only one with a preplanned analysis of patients presenting with triple - negative tumours . 
our results are in broad agreement with more recent studies , 810 , 23 but others have reported conflicting results.2426 ascertainment biases introduced by retrospective and selective identification of cases , incomplete genetic testing , small numbers , absence of adjustments for clinical variables including treatment , and short follow - up probably explain many discrepancies , although some studies have generally used stronger methods.1114 the percentage of brca - positive patients posh ( 12% ) was higher than anticipated from historical studies of patients diagnosed aged 40 years and younger , perhaps because of more sensitive mutation - testing options.1 however , only 14% of all patients had clinical genetic testing . 
the ratio of patients with brca1 to brca2 mutations was 15 to 1 , which is similar to that large western population - based reported cohorts.2 , 23 deaths due to other malignancies were low in frequency in all groups reflecting the young age group ; however , causes of deaths in patients who were brca1 - positive included potentially preventable ovarian cancers at age 4146 years . 
 in ( b ) , multivariable analysis was adjusted for age , body - mass index ( bmi ; kg / m ) , grade , tumour size , her2 status , oestrogen - receptor status , ethnicity , and use of taxane chemotherapy . 
in the posh cohort , immediate bilateral mastectomy was not associated with improved survival , although the reported use of risk - reducing surgery was low ; bilateral salpingo - oophorectomy was recorded in 32 patients and bilateral mastectomies in 107 patients.27 this probably reflects the low level of clinical testing at the time of the study . 
although riskis highly reducing bilateral salpingo - oophorectomy effective at reducing ovarian cancer incidence , the risk of vol 19 february 2018 articles primary peritoneal cancer is not reduced and studies indicate that the previously reported effect of this procedure on future breast cancer risk in brca1 and brca2 mutation carriers might have been overestimated because of uncorrected bias.28 our analysis of the 558 patients with triple - negative breast cancer in our cohort showed an intriguing difference in overall survival over the first few years after diagnosis . 
this early survival advantage has also been observed among patients with ovarian cancer who are brca mutation carriers.29 , 30 if real , this advantage might reflect greater sensitivity of brca - mutant breast chemotherapy or the greater visibility of brca - mutant cancers to host immune attack.31 one theory that could explain the slight survival advantage for brca mutation carriers not undergoing immediate bilateral mastectomy is that a major surgical intervention might compromise host immunity at a time when this is particularly important for eradicating micrometastases . 
this hypothesis would need further exploration due to the small number of patients in this subgroup . cancers results from several published studies have suggested that the dna repair deficiency associated with brca mutations results in enhanced sensitivity to many chemotherapy agents , particularly higher response rates to platinum - based drugs , have occurred in both metastatic and neoadjuvant settings.4 , 7 only 13 patients in our cohort were treated with platinum - based adjuvant regimens for early breast cancer , including one patient with a brca1 mutation and one with brca2 . our study illustrates the high breast cancer mortality in this unscreened young population and the effect of known tumour and patient - prognostic characteristics on mortality . 
inevitably , there have been substantial changes in the management of brca1 and brca2 mutation carriers since the recruitment period of this study , including the exploration in trials of systemic therapies that exploit brca - null tumours , including platinumbased drugs and parp inhibitors . 
the association of brca mutations with improved early outcomes related to breast cancer in patients with triple - negative breast cancer has the potential to affect early results from clinical trials . 
as advanced genomic investigations increasingly become a part of routine oncological care , many patients with breast cancer now learn their brca mutation status close to the time of diagnosis . 
in many cancer centres , immediate or post - chemotherapy bilateral mastectomy has become an almost routine recommendation for brca1 and brca2 mutation carriers regardless of the size or focality of the presenting tumour . 
in the longer term , risk - reducing surgery , particularly for brca1 gene carriers is an appropriate management ; in our analysis , the rising hazard for death in brca carriers over time was negated by removing from the analysis all patients who developed a second new primary breast or ovarian cancer during the follow - up period . clinicians need to consider short - term and long - term risks and benefits in discussing risk - reducing bilateral mastectomy with patients . 
the number of patients with triple - negative breast cancer who had immediate bilateral mastectomy in our cohort was small but our analysis suggests it is unlikely that the early bilateral mastectomy accounted for the early survival advantage in the brca mutation carriers with triple - negative breast cancer . 
with modern mri - based breast screening , we conclude that patients who choose to delay additional surgery for 1 or 2 years until they are psychologically and physically recovered from their cancer treatment can be reassured that this choice is unlikely to lead to any substantial survival disadvantage . 
the importance of appropriately timed risk - reducing bilateral salpingooophorectomy , for brca1 mutation carriers in particular , is clear , but should take plans for further pregnancy into account . 
furthermore , risk - reducing bilateral salpingooophorectomy in very young women will have negative health consequences as a result of oestrogen deprivation from an early age . the strengths of the posh study include the large cohort size , few missing data , and inclusion of patients with young - onset breast cancer , which led to a large number of brca1 and brca2 mutation carriers and a high number of events , ensuring that the study was well powered for the main outcome analysis . 
our study minimised many of the biases present in other studies by recruiting patients within the first year after diagnosis from oncology clinics nationally to minimise survival and selection bias and by establishing brca mutation status for all patients included in the analysis . 
posh participants recruited from england represented 23% of the available population during the recruitment period and comparison with cancer registry data confirmed that is representative of the wider the posh cohort population.16 comprehensive details of pathology enabled us to do a separate analysis of outcome in patients with triple - negative breast tumours ; a unique contribution to this field . 
we have previously reported the significant and independent prognostic effects of obesity and ethnicity on long - term outcomes in this young patient group , and this study is the only prospective study to date to include these host factors in multivariable analyses.21 , 22 limitations of this study included the non - universal use of multiplex ligation probe analysis ; we therefore cannot exclude the possibility that some structural brca variants were not identified . 
however , even clinical diagnostic mutation testing is not 100% sensitive because of occult mutations not amenable to current methods ( eg , deep intronic splice variants ) ; the investigation of brca1 and brca2 gene sequences in this cohort was more comprehensive than in most other publications . 
 all participants were tested for tp53 mutations and 178 vol 19 february 2018 articles carriers were excluded from this analysis because of the high risk of non - breast malignancies . 
we acknowledge that other breast cancer susceptibility gene variants were not excluded ; however , these were expected to be very low in frequency or low penetrance , and there is no evidence that they specifically affect prognosis . 
the treatments given reflected modern oncological practice with almost 90% of patients receiving neoadjuvant or adjuvant chemotherapy ; in more than 95% of cases this was an anthracycline or anthracycline plus taxane combination regimen . other limitations of this study included restricting the main cohort to patients aged 40 years or younger at the time of diagnosis to enrich for brca mutation carriers . 
progesterone - receptor testing was not done routinely in many uk centres during the period of recruitment and supplementary data were derived from tissue microarrays rather than full tumour sections . 
the relevance of triple - negative breast cancer in terms of biology and treatment has only become apparent since the posh study was designed , so the study was not powered for this as the primary outcome ; notably , the only difference in overall survival in this study was seen between mutation carriers and non - carriers in this subgroup . 
recommendations for adjuvant treatment in the uk changed over the course of recruitment , with taxanes being recommended for node - positive disease from 2006 and adjuvant trastuzumab for her2 - positive breast cancer routinely available only from 2006 . 
 although we specifically collected information at 5 years about risk - reducing surgery , we cannot exclude the possibility and oophorectomy might have been done at different hospitals from the recruiting cancer centre ( eg , at specialist plastic surgery or gynaecological units )  . risk - reducing mastectomy that this study confirmed that patients diagnosed with invasive breast cancer aged 1840 years have a high breast - cancer - specific mortality , and a high proportion are brca1 and brca2 mutation carriers . 
brca mutation carriers presenting with triple - negative breast cancer might have an improved survival during the first few years after diagnosis compared with non - carriers , although immediate bilateral mastectomy did not account for this advantage . 
 finally , analysis of early outcome data from trials exploring brca - deficient tumour treatment in patients with triple - negative breast cancer should be interpreted with caution in view of the possible early survival advantage for brca mutation carriers . contributors the study was conceived and designed by dme , ps , and dga , and planned and executed by dme , dga , ps , dge , amt , pp , lj , hh , sl , re , ah , fjg , and sh . 
 all other authors declare no competing interests . acknowledgments we are grateful to all the patients , clinicians , research staff at the national cancer research institute clinical research network , and the posh research team who made this study possible . 
funding over 18 years has been provided by the wessex cancer trust , cancer research uk ( c1275 / a7572 , c22524 , a11699 , a19187 ) , and breast cancer now ( 2005nov53 )  . 
sample handling was facilitated by southampton cruk centre tissue bank and southampton university faculty of medicine dna bank ( southampton , uk ) and the barts cancer research centre ( london , uk )  . 
dna sequencing for the whole cohort took place in the strangeways research laboratories ( cambridge , uk ) , and validation sanger sequencing and multiplex ligation - dependent probe amplification was done in the wessex regional genetics laboratories ( wessex , uk )  . 
it support , histopathology image storage , and reporting software were developed and supported by the university of southampton clinical informatics support team . corrections correction to lancet oncol 2015 ; 16 : 133 correction to lancet oncol 2015 ; 16 : 181 , 184 correction to lancet oncol 2015 ; 16 : 237 published online january 29 , 2015 s1470 - 2045 ( 14 ) 70483 - 8 dp . 
 radiotherapy lancet oncol 2015 ; 16 : 23739in this comment , the fth line of the third paragraph should read : by contrast , acute gastrointestinal toxicity was increased with hypofractionation [ 95% ci 372469 ] of ( 420% patients the hypofractionation group had grade 2 adverse events vs 312% [ 266358 ] in the standard fractionation di erence 108% , 90% ci 5251643 ; p = 00015 ) although were similar 3 months after treatment , and non - inferiority was not con rmed . 
these corrections have been made to the online version as of march 2 , 2015 , and have been made to the printed comment . group , cavalli f , atun r . 
lancet oncol 2015 ; 16 : 13334 in this comment , the second sentence should have been : deaths from cancer are projected to increase from the present level of around 8 million a year to more than 13 million by 2030 , with most of the burden being in poorer countries . 
this correction has been made as of jan 29 , 2015 . correction to lancet oncol 2015 ; 16 : 266 ih , williams lj , kunkler jack wjl , cameron da , dixon jm , on behalf of investigators . 
 lancet oncol 2015 ; 16 : 26673in the interpretation section of the summary , the rst sentence should read postoperative whole - breast radiotherapy after breast - conserving surgery and adjuvant endocrine treatment resulted in a signi cant but modest reduction in local recurrence for women aged 65 years or older with early breast cancer 5 years after randomisation . 
this correction has been made to the online version as o f march 2 , 2015 , and to the printed article . thomas a , rajan a , berman a , in patients with et al . 
lancet oncol 2015 ; 16 : 17786 in the key of gure 2a of this article , the text for the red line should read thymic carcinoma ( 16 / 24 failed ) and that for the blue line should read in the thymoma ( 11 / 16 failed )  . 
 key of gure 4b , the text for the red line should read no change / increase ( 0 / 18 failed ) and that for the blue line should read decrease ( 4 / 4 failed )  . 
lancet oncol 2015 ; 16 : 27483in this article , the interpretation should have read : hypofractionated radiotherapy was not non - inferior to standard fractionated radiotherapy in terms of acute genitourinary and gastrofor men with intestinal intermediate - risk high - risk and prostate cancer . 
this correction has been made to the online version as of march 2 , 2015 and to the printed article . toxicity vol 16 march 2015 e105 infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
our aim was to describe the scale and profile of cancer incidence and mortality worldwide among 2039 year - olds , highlighting major patterns by age , sex , development level , and geographical region . methods we did a population - based study to quantify the burden of young adult cancers worldwide . 
we defined young adult cancers as those occurring between the ages of 20 and 39 years because these individuals will have passed puberty and adolescence , but not yet experienced the effects of hormonal decline , immune response deterioration , or organ dysfunction associated with chronic health conditions . 
global , regional , and countryspecific ( n = 184 ) data estimates of the number of new cancer cases and cancer - associated deaths that occurred in 2012 among young adults were extracted in four 5 - year bands from the international agency for research on cancers globocan 2012 for all cancers combined and for 27 major types as defined by the international classification of disease , tenth revision . 
we report the number of new cancer cases and cancer - associated deaths overall and by sex alongside corresponding age - standardised rates ( asr ) per 100 000 people per year . 
we also present results using four levels of the human development index ( hdi ; low [ least developed ] , medium , high , and very high [ most developed ] ) , which is a composite indicator for socioeconomic development comprising life expectancy , education , and gross national income . findings 975 396 new cancer cases and 358 392 cancer - associated deaths occurred among young adults worldwide in 2012 , which equated to an asr of 433 new cancer cases per 100 000 people per year and 159 cancer - associated deaths per 100 000 people per year . 
the burden was disproportionally greater among women and the most common cancer types overall in terms of new cases were female breast cancer , cervical cancer , thyroid cancer , leukaemia , and colorectal cancer ; in terms of deaths , female breast cancer , liver cancer , leukaemia , and cervical cancer were the main contributors . 
when assessed by development level and geographical region , the cancer profile varied substantially ; generally , the burden of infection - associated cancers was greater in regions under transition . 
cancer incidence was elevated in very high - hdi regions compared with low - hdi regions ( asr 645 vs 462 cancer cases per 100 000 people per year ) ; however , the mortality burden was 3 times higher in low - hdi regions ( asr 254 vs 92 cancer - associated deaths per 100 000 people per year ) , reflecting differences in cancer profiles and inferior outcomes . interpretation the global cancer burden among 2039 year - olds differs from that seen in younger or older ages and varies substantially by age , sex , development level , and geographical region . 
although the cancer burden is lower in this age group than that observed in older ages , the societal and economic effects remain great given the major effects of premature morbidity and mortality . 
targeted surveillance , prevention , and treatment are needed to reduce the cancer burden in this underserved age group . funding international agency for research on cancer ( iarc ) and european commissions fp - 7 marie curie actionspeoplecofund . copyright the author ( s )  . 
this notice should be preserved along with the articles original url . introduction cancer is a major cause of morbidity and mortality across all age groups in both developed and transitioning economies.1 to date , research has focused on cancer in children and at older ages . 
this focus could be because a cure in children would lead to decades of productive life and because the burden of most epithelial cancers is increasing with age and cancer is becoming a leading cause of death in many countries . 
these cancers are a bridge between paediatric and adult oncology , and represent a distinct spectrum of disease among young adults who have a vol 18 december 2017 1579 research in context evidence before this study although substantial research on cancer in children and older age groups has been undertaken , the burden of cancer among young adults ( 2039 years ) has rarely been studied in depth , and is often overlooked by cancer researchers and policy makers alike . 
to determine the current evidence describing young adult oncology globally we searched pubmed for publications in english , without any date restrictions , using the terms young adult , cancer , global , incidence , and mortality . 
from our search it was clear that there was a paucity of research on young adult cancer in countries with limited resources , with nearly all of the literature focusing on high - income countries , particularly the usa , canada , and several european countries . 
thus , we sought to describe the magnitude and patterns of cancer in young adults globally to improve the understanding of cancer in this age group . added value of this study to our knowledge , the present study is the first to explore the global burden of cancer among young adults for the given period and age group . 
 furthermore , our study explores barriers to improving cancer information and outcomes in young adults in low - income , middle - income , and high - income countries , and highlights future opportunities for improvement . implications of all the available evidence our data serve as a status report to aid young adult oncology researchers and increase awareness of cancers among this underserved age group . 
through continuous surveillance , vaccination , early detection programmes , and curative treatment the cancer burden can be reduced in this underserved age group . large proportion of their expected lifespans remaining , contribute substantially to the economy , and have an important role in caring for their families.2 thus , international research investigating the specific issues unique to this age group of cancer patients is needed to improve cancer - associated outcomes . in this study , we assess the scale and profile of young adult cancers globally . 
we report the estimated number of new cases and deaths in 2012 , as well as the corresponding incidence and mortality , describing variations by human development level and geographical region . 
 methods study design although 014 years is broadly accepted as the age range for childhood cancer and 1519 years is broadly accepted for adolescent cancer , the age range for young adult cancer is less clear because there is no uniform opinion on the upper age limit for this group , 3 with the ages 24 years , 4 25 years , 5 29 years , 6 , 7 34 years , 8 and 39 years9 all currently being used . 
for this study , we define young adult cancers as those that occur between the ages of 20 and 39 years , in line with that suggested by the adolescent and young adult oncology progress review group.9 as the group states , the rationale for using to biological and physiological maturity , with individuals having passed puberty , but not yet experienced the effects of hormonal decline , immune response deterioration , or organ dysfunction associated with chronic health conditions.9 thus , using this definition , we provide an inclusive assessment of the scale and profile of cancers in this age group that overlaps partially or entirely with that this age range relates used by other organisations involved in young adult oncology . data sources and statistical analyses to quantify the cancer burden for this age group , global , regional , and country - specific ( n = 184 ) estimates of the number of new cancer cases and cancer - associated deaths that occurred in 2012 among young adults were extracted in four 5 - year bands from the international agency for research on cancers globocan 2012.1 to make comparisons with younger and older age groups , the estimated number of new cancer cases and deaths among individuals aged 019 years , 4059 years , and 60 years and older was also extracted . 
 table 1 : estimated new cancer cases and asr per 100 000 people per year and by sex , for all cancers combined and 27 cancer types , among 2039 year - olds worldwide in 2012 leukaemia ( c9195 ) , and all sites combined excluding non - melanoma skin cancer ( c0097 , except c44 )  . we calculated age - standardised incidence and mortality rates ( asr ) per 100 000 people per year at the global and country level using the world standard population as proposed by segi11 and modified by doll and colleagues.12 case fatality , a measure of the severity of a disease , was approximated by dividing the mortality asr by the incidence asr ( m : i )  . 
to document key patterns in the cancer burden , we draw comparisons between low - income and middle - income countries ( lmics ) and high - income countries ( hics )  . 
furthermore , we present the results by geographical region , using 19 un - defined geographical sub - regions , and development level , using [ least low the human development index ( hdi ; developed ] , medium , high , and very high [ most developed ] ; appendix p 1 ) ; 13 the hdi is a socioeconomic development life expectancy , education , and gross national income . 
 indicator comprising role of the funding source the funder had no role in the study design , collection , analysis or interpretation of the data , or writing of the report . 
the corresponding author had full access to all clean data and the final responsibility to submit for publication . results 975 396 new cancer cases and 358 392 cancer - associated deaths were estimated to have occurred among 2039 year - olds worldwide in 2012 , with the disease more frequent among women ( male : female ratios of 05 for incidence and 08 for mortality ; tables 1 and 2 )  . 
common tumour types in children and adolescents , including leukaemia and cancers of the brain and cns were among the most common cancers at ages 2039 years ( figure 1 )  . 
however , common epithelial tumours such as breast cancer ( ranked first for new cases and deaths overall ) , cervical cancer ( ranked second for new cases and fourth for deaths overall ) , and colorectal cancer ( ranked fifth for new cases and sixth for deaths overall ) were more frequently observed among young adults than children or adolescents , though still to a lesser extent than those observed in older ages . breast cancer or cervical cancer were the most common cancer types in young adults for most countries in terms of incidence and mortality ( figure 2 ) , and together accounted for 301 854 ( 309% ) of the total estimated new cases and 76 661 ( 214% ) of the total estimated cancerassociated deaths ( tables 1 and 2 )  . 
other frequently diagnosed cancers included thyroid cancer ( 78 568 [ 81% ] cases ; asr 35 per 100 000 people per year ) , leukaemia ( 49 293 [ 51% ] cases ; asr 22 per 100 000 people per year ) , and colorectal cancer ( 41 117 [ 42% ] cases ; asr 18 per 100 000 people per year )  . 
notably , thyroid cancer was 4 - times more common in women than in men , with an asr of 57 per 100 000 women per year and 14 per 100 000 men per year . 
in terms of deaths , leukaemia 1582 vol 18 december 2017 articles 236 709 975 396 4 406 041 8 449 748 112 143 358 392 2 035 328 5 695 712 lung pancreas corpus uteri testis stomach nasopharynx other 019 2024 2529 3034 3539 4059 019 2024 2529 3034 3539 4059 ( 36 253 [ 101% ] deaths ; asr 16 per 100 000 people per year ) , liver cancer ( 36 228 [ 101% ] deaths ; asr 16 per 100 000 people per year ) , and brain or cns cancer ( 20 783 [ 58% ] deaths ; asr 09 per 100 000 people per year ) were additional large contributors to the burden . even among young adults , the cancer profile according to 5 - year age intervals was heterogeneous ( figure 1 )  . 
the proportion of leukaemia , lymphomas , testicular cancer , and thyroid cancer reduced with increasing age ; whereas , the proportions of cervical , breast , liver , and colorectal cancer increased . 
a similar transition was observed when deaths were assessed , with cancers more commonly observed in children or adolescents decreasing in frequency as age at diagnosis increased , with these cancer types being replaced by cancers more common in adulthood . 
although the absolute number of new cases was greatest among countries in the highhdi level , the incidence was greatest at the very highhdi level ( asr 645 new cases per 100 000 people per year ) , followed by the low - hdi level ( asr 462 new cases per 100 000 people per year )  . 
with respect to the cancer profile across the hdi levels ( appendix pp 1415 ) , breast cancer was the most common cancer and cervical cancer was the second most common cancer , in the low , medium , and high - hdi levels , while at the very highhdi level these cancers ranked first and fifth , respectively ( figure 3 )  . 
thyroid cancer , melanoma of the skin , and testicular cancer were more frequent in very high - hdi regions , whereas cancers associated with infection were more frequent in countries indexed within the low - hdi level ; indeed , one in three cancers ( 332% ) were linked to major infectious agents , including human papillomavirus ( hpv ) , human herpesvirus - 8 ( hhv - 8 ) , hepatitis b virus ( hbv ) , hepatitis c virus ( hcv ) , and helicobacter pylori , in low - hdi countries relative to one in nine ( 113% ) in very high - hdi settings ( appendix p 16 )  . 
notably , across all hdi levels , the top five incident cancers accounted for more than 50% of the total estimated number of new cases ( figure 3 )  . mortality was reduced with increasing hdi ( appendix pp 1728 )  . 
the overall case fatality of 550% ( m : i 254 / 462 ) and 491% ( m : i 161 / 328 ) in low and medium - hdi countries , respectively , was approximately 41 and 35 percentage points higher than that observed in very high - hdi populations ( 14.3% ; m : i 92 / 645 ; appendix pp 2932 )  . 
in terms of the cancer profile , breast and cervical cancer were among the top five causes of cancer - associated deaths across all hdi levels , as was leukaemia ( figure 3 )  . 
at the medium - hdi level , colorectal cancer and stomach cancer were among the most fatal cancers , while liver cancer was the leading cause of cancer - associated death in high - hdi regions . 
 new cases or cancer - related deaths ( % ) leukaemia kaposis sarcoma prostate other pharynx non - hodgkin lymphoma cervix uteri melanoma of skin gallbladder brain and cns breast oesophagus larynx hodgkins lymphoma liver lip or oral cavity bladder kidney colorectum ovary multiple myeloma thyroid figure 1 : cancer type distribution for estimated ( a ) new cancer cases and ( b ) cancer - related deaths in 2012 finally , for very high - hdi regions , brain and cns cancer and colorectal cancer were the remaining largest causes of cancer death . 
briefly , for cancer - specific case fatality , an increasing step - wise gradient with decreasing human development was observed for most cancer sites ( appendix pp 2932 ) ; the greatest disparities were observed for hodgkins lymphoma , melanoma of the skin , and cancers of the prostate , testis , thyroid , kidney , and breastall of which had an estimated case fatality at least 5 - times greater in low - hdi settings compared with very high - hdi settings . with regard to geographical variations , the incidence among 2039 year - olds was greatest in australia and new zealand , and most countries in northern america and europe , whereas parts of africa , western asia , and southern asia had the lowest incidence ( figure 4a )  . 
for example , the asr for breast cancer varied from 66 per 100 000 people per year in central america to 140 per 100 000 people per year in australia and new zealand . 
 greater variations were observed for cervical cancer , with the incidence varying 15 - fold ; it was lowest in northern africa and highest in southern africa ( figure 5 )  . 
other marked geographical differences included those of vol 18 december 2017 1583 articles a most common cancer type ( incidence ) breast ( 104 ) cervix uteri ( 48 ) kaposis sarcoma ( 11 ) thyroid ( 8 ) testis ( 6 ) melanoma of skin ( 3 ) liver ( 2 ) colorectum ( 1 ) non - hodgkin lymphoma ( 1 ) no data not applicable most common cancer type ( mortality ) breast ( 84 ) cervix uteri ( 30 ) leukaemia ( 18 ) liver ( 18 ) brain and nervous system ( 17 ) kaposis sarcoma ( 9 ) stomach ( 3 ) non - hodgkin lymphoma ( 2 ) colorectum ( 1 ) lung ( 1 ) melanoma of skin ( 1 ) no data not applicable figure 2 : global map depicting the most common cancer type by country in terms of estimated ( a ) new cases and ( b ) cancer - related deaths among 2039 year - olds in 2012 . numbers in parenthesis are the number of countries that have this cancer as their most common cancer . testicular cancer and melanoma of the skin , both of which were concentrated in northern america , europe , and australia and new zealand ( appendix pp 213 )  . 
finally , the greatest burden of thyroid cancer was observed in northern america ( asr 134 6 per 100 000 people per year ) , where the incidence was 45 - times higher than that observed in middle africa ( asr 03 per 100 000 people per year ) ; the burden was also substantial in australia and new zealand ( asr 77 per 100 000 people per year ) , western europe ( asr 61 per 100 000 people per year ) , western asia ( asr 56 per 100 000 people per year ) , and eastern asia ( asr 54 per 100 000 people per year )  . despite the incidence being greatest in the most developed countries , these regions conversely had the lowest mortality , with the mortality burden greatest in parts of africa and asia ( figure 4b )  . 
indeed , cancer fatality was greatest in western africa ( 643% ; m : i 254 / 395 ) , 1584 vol 18 december 2017 articles breast cervix uteri kaposis sarcoma liver non - hodgkin lymphoma breast cervix uteri leukaemia colorectum lip or oral cavity breast cervix uteri thyroid liver leukaemia breast thyroid melanoma of skin testis cervix uteri with proportions greater than 50% also seen in middle africa , eastern africa , and southern asiaall substantially higher than the case fatality proportions in australia and new zealand ( 113% ; m : i 86 / 764 ) , western europe ( 125% ; m : i 86 / 689 ) , and northern america ( 126% ; m : i 96 / 760 ; appendix pp 2932 )  . 
in terms of the cancer profile , the greatest mortality burden for breast cancer was observed in western africa ( asr 65 per 100 000 people per year ) , middle africa ( asr 47 per 100 000 people per year ) , and eastern africa ( asr 47 per 100 000 people per year ; appendix pp 1728 )  . 
for cervical cancer , the mortality burden varied 31 - fold , ranging from an asr of 02 per 100 000 people per year in northern africa and western asia to an asr of 51 per 100 000 people per year in melanesia , micronesia , and polynesia . 
again , the case fatality for specific cancer sites varied substantially worldwide ; however , cancers with known worse survival prospects showed less heterogeneity ( appendix pp 2932 )  . discussion to our knowledge , this is the first study to investigate cancer incidence and mortality among young adults worldwide . 
overall , the global incidence of cancer in 2039 year - olds in 2012 was 433 per 100 000 people per year , and the corresponding mortality was 159 per 100 000 people per year . 
we report considerable variations in the scale of incidence and mortality worldwide , and illustrate the heterogeneity of cancer types in this age group when stratified by age , sex , development level , and geographical region . 
furthermore , our study highlights the need to increase awareness and resources for this neglected subpopulation . cancers of the breast and cervix uteri were the major contributors to the cancer burden among young adults globally , although there was wide variability in the scale and profile of cancer according to hdi level and geographical region . 
these findings are consistent with established epidemiological transitions and cancer transitions as countries become increasingly societally and economically developed.14 variations in the young adult cancer profile globally also relate to differences in screening or detection practices , genetic predispositions , and exposure to other risk factors.2 for example , the burden of thyroid cancer is substantially greater in very high - hdi countries , with incidences highest in north america . 
this association with human development level probably corresponds to changes in diagnostic practice and overdiagnosis in the usa and canada , as well as in australia , new zealand , europe , and some hics in asia.15 similarly , a substantial proportion of breast cancers diagnosed before the age of 40 years are linked with genetic factors , and thus the elevated rates in north america , australia , new zealand , cases deaths low hdi 451% 549% 151 874cases 83 581 deaths 510% 490% 506% 494% 244 154 cases 119 362 deaths 476% 524% 509% 491% 350 234 cases 122 068 deaths 538% 462% breast liver cervix uteri kaposis sarcoma leukaemia breast leukaemia cervix uteri colorectum stomach liver leukaemia breast brain and cns cervix uteri breast brain and cns leukaemia colorectum cervix uteri medium hdi high hdi very high hdi 414% 586% 221 971 cases 31 852 deaths 441% 559% figure 3 : proportion of five most frequent cancer types for estimated new cases and cancer - related deaths among 2039 year - olds in 2012 , by hdi level hdi = human development index . and europe could relate to a higher incidence of brca1 / 2 mutations individuals of european ancestry.16 however , breast cancer incidence in west africa are strikingly similar to these western countries . 
previous research has shown that women from west africa develop breast cancer at younger ages , with a mean age at presentation of between 35 and 45 years , 1015 years earlier than women in hics ; 17 these cancers , which could include a disproportionate number of tumours with poor prognosis , 17 are probably associated with a mix of genetic and environmental factors unique to this subpopulation.18 such differences in the distribution of cancer types , with more fatal cancers generally more prominent in lmics , was in turn responsible for the worse cancer vol 18 december 2017 1585 articles a age - standardised incidence rate ( per 100 000 people per year ) > 618 496618 428496 346428 < 346 no data not applicable age - standardised mortality rate ( per 100 000 people per year ) > 219 164219 133164 92133 < 92 no data not applicable figure 4 : global map depicting the estimated age - standardised ( a ) incidence and ( b ) mortality per 100 000 people per year for overall cancer by country among 2039 year - olds in 2012 outcomes noted in our results among young adults from these regions . 
however , even within the same cancer type , mortality was higher in lmics ; this was particularly apparent for kidney , testicular , and breast cancer , leukaemia , and lymphoma , implying that these variations in case fatality are probably due to fractured health infrastructures , 2 the detection of cancers at a later stage2 because of ineffective screening tests or no early detection procedures , 19 and poor access and availability of treatment.20 with nearly one million cancers occurring among young adults worldwide in 2012 , efforts are urgently needed to address the cancer burden in this age group . 
 this population has , however , been neglected by cancer researchers and policy makers , often being referred to as a lost tribe.9 , 21 , 22 throughout the past decade , young adult oncology has attracted increasing attention in some hics , given that cancer represents the most common cause of disease - associated death for this age group23 and survival improvements have lagged behind those of both children and older adults.6 , 21 globally , however , much remains unknown in this area of oncology . 
expanding the young adult cancer agenda beyond hics remains a challenge , but one of great importance as young adults represent a large proportion of the population with an inherent potential for economic growth in many lmics . an opportunity to reduce the cancer burden in young adults lies in prevention because unlike most cancers occurring at younger ages , a substantial proportion of young adult cancers are preventable . 
in view of the substantial contribution of cervical and liver cancer to the global young adult cancer burden , national hpv vaccination programmes of hpv - naive people and hbv vaccination programmes for neonates would probably have a sizable effect in reducing cancer incidence in young adults worldwide . 
similarly , adequate treatment 1586 vol 18 december 2017 articles east africa middle africa north africa south africa west africa caribbean central america south america north america east asia southeast asia south asia west asia east europe north europe south europe west europe east africa middle africa north africa south africa west africa caribbean central america south america north america east asia southeast asia south asia west asia east europe north europe south europe west europe australia / new zealand melanesia / micronesia / polynesia age - standardised incidence ( per 100 000 people per year ) australia / new zealand melanesia / micronesia / polynesia age - standardised mortality ( per 100 000 people per year ) breast cervix uteri thyroid leukaemia colorectum brain and cns non - hodgkin lymphoma liver testis ovary stomach melanoma of skin hodgkins lymphoma lip or oral cavity lung kaposis sarcoma corpus uteri nasopharynx kidney oeosophagus bladder other pharynx pancreas gallbladder larynx multiple myeloma prostate other figure 5 : estimated ( a ) age - standardised incidence and ( b ) mortality per 100 000 people for each cancer type among 2039 year - olds in 2012 , by geographical region for hiv could further reduce the cancer burden of kaposis sarcoma , particularly in sub - saharan africa where incidence was greatest . 
although lifestyle and environmental factors drive some of the burden , many young adult cancers are not strongly influenced by the major risk factors associated with the onset of certain cancers at older ages , such as tobacco , alcohol , or nutrition . 
to target cancers representing smaller contributors to the overall burden , additional relatively inexpensive preventive strategies of known efficacy targeting should be considered , melanoma of the skin ( eg , limiting exposure to direct sunlight , increased sunscreen use , and avoidance of tanning salons ) .9 including those another relevant opportunity is ensuring timely diagnosis , with previous research suggesting that young adults experience more delays compared with children , adolescents , and older age groups.2 , 21 in hics , delays in diagnosis have been associated with psychological and social factors ; whereas , in lmics , cultural norms and geographic accessibility could represent the greatest obstacles . 
 although no age - specific screening tests are currently available for young adults , 24 our data indicate that screening and early detection programmes might have a significant effect at a limited costparticularly those targeting cervical cancer ( eg , visual inspection with acetic acid screening ) and breast cancer ( eg , self - awareness through self - examination and enhanced screening for brca1 / 2 carriers ) , with lesser but still potentially worthwhile effects for testicular cancer , colorectal cancer , vol 18 december 2017 1587 articles for cancer incidence in five continents see and melanoma of the skin in high - risk populations.9 , 24 research into such programmes specifically in young adults is needed , to determine the benefits and potential risks , particularly for breast and testicular self - examination because these recommendations24 are not currently supported by evidence . 
in general , increasing awareness of cancer in this age group at both public and professional levels is needed to bring attention to the aforementioned primary and secondary prevention measures , reduce delays , and lead to improvements in the cancer burden across all resource levels . finally , once diagnosed , young adults with cancer must be able to access high quality care . 
currently , care for these individuals is scattered ; even in hics , young adult oncology expertise is rare , with 90% of north american young adults with cancer receiving their care in community practices.25 , 26 in many cases , which treatment protocols offer this population the best chance of cure is still unclear , with extrapolations made from younger and older populations . 
this uncertainty is largely due to the low participation in the relatively few clinical trials available for this age group ; 2 , 21 thus , increasing the availability of and participation in clinical trials for this group is of paramount importance.9 even when effective treatment protocols for young adults are known , further work is necessary to ensure that all patients can access such treatment . 
for example , despite evidence proving the superiority of paediatric treatment protocols for young adults with acute lymphoblastic leukaemia ( all ) , a study25 found that the percentage of californian young adults with all treated with such protocols reduced from 31% in 200812 to 21% in 201314 . 
although freely available guidelines for young adult oncology , such as that produced by the national comprehensive cancer network , 24 might be of help , it remains uncertain whether such guidelines are appropriate for more resource - limited settings . 
several hics have built alternative models of young adult cancer care delivery , such as a nationwide network of young adult cancer units in the uk ; 27 whether these different models improve cancer outcomes is unknown . implementation of the above recommendations will require substantial investment in young adult oncology . 
 although such investments in lmics might seem too complex or costly , the economic advantages are clear given the number of potential years of life saved ; this is exemplified by the fact that this population has approximately 2545 years of their life expectancy remaining ( average global life expectancy at birth for individuals aged 2039 years in 2012 was 633 years28 ) , which is substantially greater than that observed in older adults who have not only a shorter remaining life expectancy but also poorer survival prospects after cancer diagnosis . 
because individuals in this age group are the most financially productive members of their societies , it is clear that improving equity in prevention , diagnosis , and care will not only have large societal effects , but might also be cost - effective.21 studies undertaking cost benefit analyses of improving young adult cancer care , particularly in lmics , are needed to inform policy makers and advocates . our results provide a comprehensive estimation of young adult cancers worldwide in 2012 but have several limitations . 
the globocan cancer groupings do not directly correspond with the recommended classification scheme for tumours diagnosed in young adults by birch and colleagues.29 furthermore , our results are estimates from the globocan database , which were compiled using a hierarchy of methods ; thus , accuracy was dependent on the quality and availability of the source information at a given time.1 clearly , the inclusion of uncertainty intervals for the estimates provided in this study would be useful , and collaborative work is currently underway to create such intervals that take into account deficiencies in the quality and availability of the source information at the national level , as well as inherent statistical uncertainty . 
to address both of these limitations , future research should be undertaken using available population - based cancer registry data through cancer incidence in five continents , which would allow an assessment of histologically defined cancers , including those that we were not able to address in this paper ( eg , bone cancer and soft tissue sarcomas ) , and trends , albeit for a limited number of countries or subnational regions . in summary , the global cancer burden among 2039 year - olds differs from that in younger or older ages , but also varies substantially by age , sex , development level , and geographical region . 
although cancer is less frequently observed in young adults than at older ages , its effects remain considerable because these individuals have a large proportion of their expected lifespans remaining , contribute substantially to the economy , and play a major part in caring for their families . 
because young adult cancer patients exhibit a combination of features observed in younger and older patients , progress needs to be achieved through a combination of the methods that led to improvements in these other groups : advancement of risk stratification and treatment protocols in children and implementation of effective prevention and early detection at older ages . through clinical trials contributors mmf conceived and designed the study . 
mmf , sg , is , jf , es - f , and fb critically reviewed the manuscript . declaration of interests we declare no competing interests . acknowledgments we gratefully acknowledge the many population - based cancer registries worldwide and their staff for their willingness to contribute their data , from which globocan 2012 is built . 
the work completed in this 1588 vol 18 december 2017 articles manuscript was undertaken while mmf was a postdoctoral fellow at the international agency for research on cancer , which was partially funded by the european commissions seventh framework programme marie curie actionspeoplecofund . correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections correction to lancet oncol 2017 ; 18 : e35463 correction to lancet oncol 2018 ; 19 : 87100 correction to lancet oncol 2018 ; 19 : 25766 oconnor oa , lue jk , sawas a , et al . 
 for lancet oncol 2017 ; 18 : e35463 in this review , the second sentence of the abstract should read additional improvements have been reported in three phase 3 colon cancer trials when oxaliplatin was added to fluoropyrimidines , the effect was mainly on disease - free survival . 
this correction has been made to the online version as of feb 28 , 2018 although women fulvestrant johnston s , lee ks , et di leo a , al . 
buparlisib plus with postmenopausal her2hormone - receptor - positive , negative , advanced breast cancer progressing on or after mtor inhibition ( belle - 3 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
in the results section , the following sentence should have read in the 11 ( 13% ) cases of discordance , a pik3ca wild - type tumour sample and pik3ca - mutated ctdna were reported in three ( 4% ) patients and pik3ca mutations detected in the tumour sample but not in ctdna ( 9% ) patients . 
these corrections have been made to the online version as of feb 28 , 2018 . seven vol 19 march 2018 e137 corrections malignancies interest group database , 7 5% of patients with thymic carcinomas developed myasthenia gravis ; organotypia is usually mantained in thymic carcinomas and , therefore , confers a small risk of myasthenia gravis relative to thymomas . 
thus , the possibility of heterogeneity of thymoma and thymic carcinoma in one tumour challenges the use of immune checkpoint inhibitors for the treatment of thymic malignancies , both of which are associated with immune - related adverse events . the key limitations of this study will prevent immediate adoption of pembrolizumab versus other treatment for thymic carcinoma . 
first , pd - l1 expression has not been verified to be a reliable biomarker in this or other malignancies , but there are other immune components that might be better biomarkers for response to immune checkpoint inhibitors that have been used in previous studies.810 second , thymic carcinoma comprises histologically different subtypes of cancer . 
notably , the histological subtypes within the tumours of patients in this trial were 48% squamous cell carcinoma and 15% neuroendocrine carcinoma , which does not reflect the typical distribution of histological subtypes in thymic carcinoma . are ongoing although additional trials with immune checkpoint carcinoma , thymic inhibitors important . 
the small number of reproducibility patients in phase 2 trials does not have to be a limitation to achieving treatment advances for rare cancers : replicate sample collection in translational research can counter this shortcoming with demonstrated reproducibility . 
cooperative group collaborations , such as the international thymic malignancies interest group or the thoracic alliance for cancer trials , could be useful to generate sufficient evidence to solve this problem of small patient numbers . approved drugs for rare cancers are scarce , as giaccone and colleagues have mentioned ; the high cost of these drugs , such as sunitinib and pembrolizumab , make it difficult to treat patients with thymic carcinoma worldwide because many countries cannot afford these medicines . 
globally , treatment for recurrent thymic carcinoma is still often single - agent cytotoxic chemotherapy . giaccone and colleagues plan to investigate the combination of pembrolizumab and epacadostat as an immune - combination therapy in a future expansion of this phase 2 study . 
thus , we are facing the next step to develop further therapies for thymic malignancies . yusuke okuma department of thoracic oncology and respiratory medicine , tokyo metropolitan cancer and infectious diseases centre komagome hospital , tokyo 113 - 8677 , japan y - okuma@cick.jp i declare no competing interests . kelly rj , petrini i , rajan a , wang y , giaccone g . 
 clin cancer res 2013 ; 19 : 429596 . next - generation nuclear morphology to grade solid tumours a central task for surgical pathologists diagnosing tumours is to reliably assess tumour aggressiveness from morphologic features . 
typical components of grading systems are tissue architecture , degree of resemblance to the respective benign tissue , mitotic activity , necrosis , and aberrances in nuclear morphology ( ie , nuclear pleomorphism , variations chromatin size , nucleolar prominence , and published online february 2 , 2018 s1470 - 2045 ( 18 ) 30063 - 9 see articles page 356 vol 19 march 2018 comment distribution )  . 
flemming1 coined the term chromatin in 1879 when describing nuclear structures that could be stained with basic dyes in the interphase , whereas waldeyer2 introduced the term chromosome in 1888 when describing mitotic chromat soon after , chromosomal alterations in tumours were described by bovari , 3 who also hypothesised a causal role of unequal chromatin distribution in carcinogenesis . 
the dogma of all morphologists , that function follows form , also applies to chromatin structure , which directly affects genomic activity by activating or silencing genes and gene families . in our contemporary concept , chromatin contains the whole eukaryotic genome , rather densely packaged around histones ( h2a , h2b , h3 , and h4 )  . 
posttranslational modifications of histones ( eg , acetylation , methylation ) also determine chromatin compaction , structure , and dynamics , and it is not surprising that mutations in the genes responsible for these regulatory modifications are often seen in cancer.4 advances in sequencing technologies have massively broadened our knowledge of driver oncogenes and their role during tumour progression and have helped promote the development of therapeutic drugs , but a holistic view that integrates gene expression and higher chromatin regulation is yet to be established . 
 although most pathologists know that chromatin irregularities , especially coarse and clumped chromatin as seen under the light microscope , are typical of higher graded tumours , the diagnostic value of subnuclear morphology has not been unearthed so far . 
 dna cytometry , introduced in 1966 , is a simple approach to compare overall dna content in tumour cells and normal cells.5 this technique gained popularity because aberrant dna content ( aneuploidy ) was more common in more aggressive tumours and neoplastic lesions than in benign , reactive lesions . 
today , most clinicians and pathologists do not use data on dna ploidy in patient care , even though a re - evaluation of this technique might be warranted.6 to classify image analysis chromatin patterns with modern technology is an obvious next step in developing more standardised diagnostic algorithms that could become part of tumour grading in the future . that in the lancet oncology , kleppe and colleagues7 describe nucleotyping , an automated method to reveals determine chromatin heterogeneity relevant prognostic information in various solid tumour types , including colorectal , endometrial , and ovarian carcinoma . 
although the preparatory steps are similar to conventional dna cytometry ( eg , dissection of cells , feulgen stain , multiple images , etc ) , this procedure does not yield overall staining intensity ; instead , it gives a measure of chromatin organisation computed by the entropy of pixel grey levels . 
for all analysed tumour entities , survival times were consistently shorter in patients with chromatin heterogeneous tumours than patients with chromatin homogeneous tumours , and the prognostic value of chromatin heterogeneity was independent of other parameters in a cox analysis . 
 this is an important finding , especially because the technique is applicable to formalin - fixed , paraffinembedded tissue and could easily be added to any routine workflow complement conventional tumour grading . in pathology laboratories however , some questions rema is nucleotyping easily transferable to other academic institutes ? is this biomarker robust enough to perform comparably in a decentralised setting ? how relevant are the trained personnel who identified the nuclei of interest in terms of interobserver variability of the technique ? pending clarification of these questions , this excellent study serves as an example of next - generation morphology that might enrich the pathologists armamentarium in the digital future , which is only just beginning . glen kristiansen institute of pathology , university of bonn , 53127 bonn , germany glen.kristiansen@ukbonn.de i declare no competing interests . copyright the author ( s )  . 
archiv mikrosk anat 1888 ; 32 : 1122 . 276 vol 19 march 2018 comment published online february 8 , 2018 s1470 - 2045 ( 18 ) 30075 - 5 see articles page 370 bovari t . 
 denosumab is not inferior and might even be superior to zoledronic acid in reducing skeletal - related events and improving survival in patients with certain solid tumours.2 however , in a prospective , double - blind study2 comparing denosumab with zoledronic acid in patients with solid tumours ( except breast cancer ) or myeloma ( 10% of the study patients ) , an ad - hoc analysis suggested inferior survival for patients with myeloma treated with denosumab . 
this study had several limitations and zoledronic acid remained the standard of care for patients with myeloma.3 in the lancet oncology , noopur raje and colleagues4 report a large , randomised , double - blind , phase 3 study , in which patients were randomly assigned to either 4 - weekly intravenous zoledronic acid , the present standard of care for myeloma - related bone disease , or 4 - weekly subcutaneous denosumab . 
the study met its primary endpoint of non - inferiority for denosumab versus zoledronic acid regarding the time to first skeletal - related event ( hazard ratio 098 , 95% ci 085114 ; pnon - inferiority = 0010 )  . 
study patients had a high burden of bone disease : 1144 ( 67% ) of the 1718 enrolled patients had already had a skeletalrelated event before enrolment and 376 ( 44% ) of 859 patients in the denosumab group and 383 ( 45% ) of 859 patients in the zoledronic acid group had a first onstudy skeletal - related event . 
however , 60% of first onstudy skeletal - related events occurred during the first 3 months of the study and 81% in the first 6 months , suggesting that even potent osteoclast inhibitors could not prevent skeletal - related events in the short teras such , early identification of patients at risk and timely intervention are crucial to avoid bone complications . 
 in a post - hoc landmark analysis at 15 months , denosumab was associated with fewer skeletal - related events than zoledronic acid , but this analysis has to be interpreted cautiously and cannot confirm superiority of denosumab over zoledronic acid in skeletal - related event prevention . 
 although the study by raje and colleagues4 is the largest placebo - controlled study ever done in patients with myeloma , several questions remaonly patients with myeloma - related bone disease at diagnosis were enrolled and the benefits of denosumab patients without bone disease are uncertaa survival benefit for patients treated with zoledronic acid versus clodronate1 or placebo5 has been shown , but a survival benefit for denosumab over zoledronic acid has not yet been seen , and additional follow - up is needed . 
additionally , rankl is implicated in the growth , survival , and development of drug resistance vol 19 march 2018 comment changing geographical patterns and trends in cancer incidence in children and adolescents in europe , 19912010 ( automated childhood cancer information system ) : a population - based study eva steliarova - foucher , miranda m fidler , murielle colombet , brigitte lacour , peter kaatsch , marion pieros , isabelle soerjomataram , freddie bray , jan willem coebergh , rafael peris - bonet , charles a stiller , on behalf of the accis contributors * summary background a deceleration in the increase in cancer incidence in children and adolescents has been reported in several national and regional studies in europe . 
based on a large database representing 13 billion person - years over the period 19912010 , we provide a consolidated report on cancer incidence trends at ages 019 years . methods we invited all population - based cancer registries operating in european countries to participate in this population - based registry study . 
we requested a listing of individual records of cancer cases , including sex , age , date of birth , date of cancer diagnosis , tumour sequence number , primary site , morphology , behaviour , and the most valid basis of diagnosis . 
we also requested population counts in each calendar year by sex and age for the registration area , from official national sources , and specific information about the covered area and registration practices . 
 incidence rates and the average annual percentage change with 95% cis were reported for all cancers and major diagnostic groups , by region and overall , separately for children ( age 014 years ) and adolescents ( age 1519 years )  . 
 we examined and quantified the stability of the trends with joinpoint analyses . findings for the years 19912010 , 53 registries in 19 countries contributed a total of 180 335 unique cases . 
we excluded 15 162 ( 84% ) of 180 335 cases due to differing practices of registration , and considered the quality indicators for the 165 173 cases included to be satisfactory . 
the average annual age - standardised incidence was 1375 ( 95% ci 13671383 ) per million person - years and incidence increased significantly by 054% ( 044065 ) per year in children ( age 014 years ) with no change in trend . 
in adolescents , the combined european incidence was 1762 ( 17441780 ) per million person - years based on all 35 138 eligible cases and increased significantly by 096% ( 073119 ) per year , although recent changes in rates among adolescents suggest a deceleration in this increasing trend . 
the combined age - standardised incidence of leukaemia based on 48 458 cases in children was 469 ( 465473 ) per million person - years and increased significantly by 066% ( 048084 ) per year . 
the average overall incidence of leukaemia in adolescents was 236 ( 229243 ) per million person - years , based on 4702 cases , and the average annual change was 093% ( 049137 )  . 
this notice should be preserved along with the articles original url . introduction cancer is an important disease burden in children as it is not easily prevented , with known causes explaining only a small proportion of cases . 
evidence from retrieved studies suggested that after a substantial increase in childhood cancer incidence towards the end of the last century , the rate of increase has declined in the 2000s . 
however , the limitations of most of these studies , in terms of number of cases or timeframe , might have hampered the full understanding of the dynamisms behind the observed trends in this population . added value of this study we used all quality data available in europe for the full calendar years in the period 19912010 to evaluate incidence patterns and trends in children and adolescents . 
based on the large scale of all available european data , our findings add an authoritative account on the geographical patterns and temporal trends of cancer in children and adolescents in europe . 
 implications of all the available evidence the increasing trends might have resulted from improvements in cancer diagnosis or registration in this age group , although the influence of other factors cannot be excluded . 
the paucity of evidence of stabilisation of cancer incidence in europe and the variability of the observed trends support the need for continued international monitoring and research into causal mechanisms . the past three decades , incidence increased by about 1% per annum for all cancers combined and this increase affected most major diagnostic groups , including leukaemias , lymphomas , and cns tumours.2 however , in the past decade , incidence appears to have stabilised overall and for the major diagnostic groups in european populations.310 leukaemias , lymphomas , and tumours of the cns represent 70% of all cancers observed in european populations younger than 15 years and half of all cancers in those aged 1519 years1 and therefore contribute considerably to the overall incidence . 
 monitoring these trends is important for planning health - care delivery and for aetiological research . in this study , we documented and interpreted incidence trends in europe for cancers diagnosed at ages 019 years using quality - assured population - based cancer registries . 
 we focused on the 20 - year period 19912010 , assessing the trends separately in children ( aged 014 years ) and adolescents ( aged 1519 years ) , for all cancers combined and for the major diagnostic groups . 
our results update the automated childhood cancer information system ( accis ) studies , extending the previously reported period of observation by over a decade.2 , 11 methods data acquisition invited all population - based cancer registries operating in european countries ( as defined by the un statistics division12 ) and cyprus to participate in this population - based registry study . 
we requested a listing of individual records of cancer cases , and the population in each calendar year by sex and age from official national sources , accompanied by specific information about the geographical and administrative area covered and registration practices . information on cancer cases included coded data on sex , age , date of birth , date of diagnosis , tumour sequence number , primary site , morphology , behaviour , and the most valid basis of diagnosis . 
most registries coded tumours according to the international classification of diseases for oncology , third edition ( icd - o - 313 ) as required , and international classification of diseases for oncology , second edition14 codes were converted to icd - o - 3 codes . 
subsequently , neoplasms were classified according to the international classification of childhood cancer , third edition ( iccc - 3 ) .15 we examined individual records for internal consistency , 16 verifying unlikely combinations of site with morphology , age or sex with tumour type , basis of diagnosis with morphology , and rare tumour entities . 
standardised tables , charts , statistics , lists of selected questioned records , and any relevant information provided by the registry or known from published sources were discussed at meetings of the accis scientific committee , who decided on the inclusion of each dataset in the accis database . 
only datasets with high - quality data were eligible for inclusion in the analyses . the cancers included in the analyses were all malignant tumours diagnosed during the complete calendar years 19912010 , in people younger than 20 years and resident in the contributing registration areas . 
several cancer types were excluded because they were not eligible for registration in all participating registries or during the whole study period : myelodysplasias ( icd - o - 3 m - codes starting with 998 ) , pilocytic astrocytoma ( icd - o - 3 code for more on accis see 1160 vol 19 september 2018 articles m - 9421 ) , non - melanoma skin cancer ( iccc - 3 subgroup xie and xiib with site code c44 ) , and carcinoid tumour of the appendix ( icd - o - 3 site code c18.1 and m - 8240 )  . the data used in this study were submitted and validated during the years 201516 . 
our study design was reviewed and approved by the international agency for research on cancer ( iarc ) ethics committee on june 17 , 2015 . dataset constitution an eligible registry could become a contributor if it provided quality data for all complete calendar years in the 20 - year period 19912010 . 
the paediatric registries collected and provided data for those aged 014 years , and the other cancer registries and the paediatric registry of belarus provided data for the full target age range ( 019 years )  . 
the french national paediatric registry registered haematological malignancies only . some populations in france , germany , italy , spain , switzerland , and the uk were covered by both paediatric and general cancer registries . 
to avoid double counting of cases in two registries while using the maximum number of cases for analyses in these populations , we allocated each registry to one or more datasets ( appendix p 2 )  . 
we built three datasetsone with 39 registries contributing to the analyses of all cancers , cns tumours , and other tumours in ages 014 years , a second with 32 registries contributing to the analyses of leukaemia and lymphoma in ages 014 years , and a third with 45 registries contributing to all the analyses of those aged 1519 years . 
 the first and second datasets ( ages 014 years ) differed only in the contribution from france ; the analyses of all cancers and cns tumours used a dataset that included data from the french general cancer registries , while the leukaemia and lymphoma dataset included data from the french national paediatric registry of haematological malignancies . 
the french national registry increased the person - years by ten times and provided 11 770 more haematological malignancies the combined contribution of the french regional registries . compared with subnational numbers of cases and person - years were pooled to produce national cancer incidence and countries were further pooled into four european regions ( appendix p 2 ) according to un definitions.12 the person - years available in each region are shown in the appendix ( p 3 )  . statistical analysis the number of incident cases in the covered areas of the participating registries during the study period determined our sample size . 
incidence was calculated as the number of cases divided by the number of person - years in the categories of geographical area , sex , age , and diagnostic group for the given 20 - year period and expressed per million person - years . 
as the age distribution of population at risk differs between countries and over time , we adjusted the reported incidence for the age range 014 years vol 19 september 2018 1161 articles a east overall average annual percentage change ( 95% cl ) 050 ( 021079 ) belarus bulgaria czech republic hungary poland overall b north overall average annual percentage change ( 95% cl ) 040 ( 016064 ) estonia iceland norway sweden overall c south overall average annual percentage change ( 95% cl ) 040 ( 007072 ) italy portugal slovenia spain overall d west overall average annual percentage change ( 95% cl ) 070 ( 052088 ) austria france germany netherlands switzerland overall 1990 1995 2000 calendar year 2005 2010 1990 1995 2005 2010 2000 calendar year figure 1 : incidence trends of cancer in children aged 014 years in europe , 19912010 jagged thin lines indicate annual age - standardised rates in countries and smooth red thick lines indicate modelled incidence trends in regions . for age via direct standardisation using weights 12 , 10 , and 9 for the three age groups 04 years , 59 years , and 1014 years , respectively.17 we also calculated 95% cis . 
 as each combination of calendar year , sex , and age group had a positive person - years count , we encountered no missing data . to graphically portray incidence trends for all cancers , we plotted observed incidence against calendar year for each country , and the rates for the four european regions were smoothed using a locally weighted regression18 of the incidence on year . to assess the average annual percentage change , we fit the natural logarithm of the incidence with year using generalised linear regression models adjusting for age group and region , as appropriate . 
we examined incidence trends for changes during the study period using joinpoint regression program ( version 4.1.0 ) applied to the log rates , separately for the age groups 014 years and 1519 years in the total dataset , and in each cancer category , overall and by region . 
where joinpoints were detected , we reported the annual percentage change with corresponding 95% cis for each of the linear segments identified between two significant joinpoints . role of the funding source the funders of the study external to the collaborating institutions had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had final responsibility for the decision to submit for publication . results during the full calendar years of the period 19912010 , the 53 registries contributed 13 billion person - years and 180 335 unique cases . 
in 2010 , the available population at risk represented 532 million ( 466% ) of 1141 million of the european population aged 014 years and 98 million ( 226% ) of 432 million aged 1519 years , with reference to un population estimates.20 in western europe , coverage of the childhood population was almost complete for haematological malignancies ( 279 million [ 933% ] of 299 million ) , and 175 million ( 585% ) of 299 million were covered for the other malignancies , while 21 million ( 201% ) of 106 million adolescents were covered ( appendix p 3 )  . we included all 118 265 eligible cases in patients aged 014 years in our analyses of incidence of all cancers . 
 vol 19 september 2018 1163 articles incidence the average annual age - standardised incidence was 1375 ( 95% ci 13671383 ) per million person - years and increased significantly by 054% ( 044065 ) per year on average ( table 1 ) , with no break in the time trend . 
the large fluctuation of annual incidence in iceland was due to small population size and did not visibly affect the shape of the regional curve ( figure 1 )  . 
the trend in the east was split into two segments , both with nonsignificant trends ( figure 2 )  . the national for we investigated incidence for four diagnostic groups in patients aged 014 years ( table 1 , figure 2 , appendix p 4 ) , and included all eligible cases . 
the combined age - standardised incidence of leukaemia based on 48 458 cases in patients aged 014 years was 469 ( 95% ci 465473 ) per million person - years and increased by 066% ( 048084 ) per year , with no change in slope . 
the overall age - standardised incidence of lymphoma was 158 ( 156160 ) per million person - years ( based on 18 458 cases ) and varied modestly by region . 
the overall agestandardised incidence of malignant cns tumours ( 19 413 cases ) of 222 ( 95% ci 219226 ) per million person - years was observed to rise at 049% ( 020077 ) per annum with no joinpoints ; by region , we observed an increasing trend only in the west , as the rates were stable in the three other regions . in patients aged 014 years , the combined incidence of all 43 706 other cancers increased in europe overall and in all regions except the north . 
in joinpoint analysis , the european trend increased only over the first few years , similar to the trend in the west ( figure 2 )  . in adolescents ( aged 1519 years ) , the combined european incidence was 1762 ( 95% ci 17441780 ) per million person - years based on all 35 138 eligible cases and incidence increased by 096% ( 95% ci 073119 ) per year in the period 19912010 ( table 2 ) , although no significant change in trend was seen in the second decade ( figure 3 )  . 
in addition to large variations due to small numbers of cases for some countries , we observed a large range in incidence ( between around 140 and 240 per million person - years ) for belarus . 
in the east , a decrease was noted over the time segment 19992008 ( figure 3 )  . for adolescents , the overall incidence of leukaemia was 236 ( 95% ci 229243 ) per million person - years ( based on all 4702 eligible cases ) and varied little between regions ( table 2 )  . 
lymphoma ( 9446 cases ) occurred more frequently than did leukaemia ( 4702 cases ) or malignant cns tumours ( 2983 cases ) in adolescents compared with children ( table 2 ) , and the overall incidence of 474 ( 464483 ) per million person - years varied moderately by region . 
changes in this trend were detected in the east and west , where the increase was limited to the second and first half of the study period , respectively ( figure 3 )  . 
incidence was stable overall and in the four defined regions ( figure 3 ) , with no change in the slopes . the overall rate for all other cancers in adolescents ( 18 007 cases ) was 903 per million . 
the pattern of changes in the slopes by region was similar to that observed for all cancers ( figure 3 )  . discussion in this population - based registry study , we reported on cancer incidence trends in the european population of children ( aged 014 years ) and adolescents ( aged 1519 years ) during the full calendar years 19912010 , thus extending the accis study by 10132 , 11 years of observation . 
the overall incidence for children and adolescents increased significantly over this 20 - year period . the increase in incidence was not constant by cancer type , region , or over time , and there was a suggestion of stabilisation in the trend for all cancers in adolescents in the dataset for the whole of europe ( appendix p 6 )  . 
 the most pronounced inter - regional diversities included the decreasing incidence of childhood lymphomas in the east ( compared with stable or increasing incidence in the other regions ) , an increase in the incidence of childhood cns tumours in the west ( compared with little change observed in the other regions ) , and the stable incidence of leukaemia in adolescents in the north ( relative to increasing incidence in the other regions )  . vol 19 september 2018 1165 articles a east b north overall average annual percentage change ( 95% cl ) 123 ( 062184 ) belarus bulgaria czech republic poland overall overall average annual percentage change ( 95% cl ) 062 ( 028096 ) estonia iceland norway sweden overall 1990 c south 1995 2000 2005 2010 1990 1995 2000 2005 2010 overall average annual percentage change ( 95% cl ) 178 ( 136220 ) italy portugal slovenia spain overall d west overall average annual percentage change ( 95% cl ) 108 ( 072143 ) austria france germany netherlands switzerland overall 1990 1995 2000 2005 2010 1990 1995 2000 2005 2010 calendar year calendar year figure 4 : incidence trends of cancer in adolescents aged 1519 years in europe , 19912010 jagged thin lines indicate annual age - specific rates in countries and smooth thick red lines indicate modelled incidence trends in regions . although our results are largely confirmatory and incremental from previous findings , a major strength of our study is its large size , which permits detection of a moderate rate of increase of 05% per year in the age group 014 years . 
data from large paediatric cancer registries helped to increase the coverage and creation of a specific dataset for childhood haematological malignancies enlarged the relevant person - years in the west ( 5838 million ) by 53% compared with data available for other neoplasms ( 3805 million )  . 
we examined the trends separately in children and adolescents to allow for variations in trends between these populations with a different case mix . 1166 vol 19 september 2018 articles we validated the quality and completeness of the data from the included registries during a thorough dataset assessment . 
we consider our results to provide the best available estimates of incidence trends in the european population of children and adolescents for 19912010 . a limitation of our study is the variable coverage of the regions , which might affect the representativeness of the incidence at the national and european regional levels . 
the available data do not allow speculation on what the incidence would be if coverage was complete increase of coverage and quality of registration is required for a full picture of the cancer burden . 
 meanwhile , by use of all quality information available for the study period , our results maximise the number of person - years of comparable data , and provide evidence of changing trends in european populations . we excluded several cancer types that are usually included in reports of childhood cancer incidence from our analyses . 
we plan to examine this assumption in a focused analysis of trends of all cns tumours , by behaviour and diagnostic subgroup , and by considering the differences and changes in coding and their reportability . our reported total incidence was 5% to 15% lower ( depending on the region ) than in another report assessing the period 200110.1 this disparity is explained by the exclusion of several groups of neoplasms from our study and the period starting one decade earlier , which would , in the presence of an increasing trend , result in a lower overall rate . the overall average annual change of 054% in children aged 014 years is lower than the 1% reported by an accis study based on diagnoses in the 1970s through to the 1990s2 or for the period 197897 , 21 and might indicate a deceleration in the increase of cancer incidence , although the registry datasets included differ somewhat between the studies . 
a lower rate of increase could suggest the end of an improvement in reporting , but might also reflect reduced reporting discipline , a change in classification of cancers , or other factors . 
cancer - specific studies might provide more precise interpretation of these trends . studies in european populations of smaller sizes reported stabilising of cancer incidence in children overall and in the three major diagnostic groups.310 by contrast , data collected in the longstanding registries of the surveillance , epidemiology , and end results ( seer ) program suggest continued minor increases in overall childhood cancer incidence over the most recently assessed period 19952014 , 22 consistent with our study . 
in adolescents aged 1519 years , varying incidence trends were observed in different european for leukaemia , populations lymphoma , or cns tumours.3 , 4 , 7 as for the seer data , 22 our study found an increase in overall cancer incidence and leukaemia and lymphoma incidence , but no change in trends for malignant cns tumours . 
we identified changes in overall trends that provide some evidence of a deceleration of time trends during the most recent years of our study , along with varying patterns across age groups , regions , and cancer types , although significant joinpoints should not be taken to imply abrupt changes in underlying trends in risk.19 the variability we found warrants continued monitoring of incidence patterns in large populations over long periods , as trends that are not significant over short intervals might result in significant increases over a longer timeframe , and grouping smaller populations with no trend could yield a significant change in a pooled dataset . 
these considerations might also explain the discrepancy in the measured rate of change between our study and smaller european datasets.310 kroll and colleagues24 have linked the increase in childhood cancer incidence in great britain with advances in diagnostic technology and improved cancer registration , because of the concurrence of a step increase in leukaemia and non - cns solid tumour incidence in 2002 with a registration plan enacted in 2001 . 
although we are not aware of similar studies in other countries , analogous effects on childhood cancer incidence cannot be excluded elsewhere in europe and could have affected our results . the gradual convergence of environmental factors , lifestyle , and health services across europe might have contributed to the similarities in incidence trends across the regions , although such changes will probably have less of an effect on cancer in childhood than in older age . 
nevertheless , some opposing trends ( notably for lymphoma in the east ) suggest caution should be taken in ascribing the slowly increasing trends exclusively to improved detection , at least before further detailed analyses by cancer type , age group , and geographical region are done . overall incidence in children is weighted towards leukaemia , which , in 75% of cases , is the precursor b - cell lymphoid leukaemia . 
with increasing social development over time , this peak shifts towards younger ages and becomes more pronounced.2 , 25 this change is unlikely to be driven by improved registration , which would affect all vol 19 september 2018 1167 articles ages in the same way . 
the deficit of lymphoid leukaemia cases seen in poorer settings can be ascribed in part to underdiagnosis , 26 , 27 but inequalities across social strata might also operate through relevant exposures , such as parental occupation , diet , or reproduction characteristics.28 continuous socioeconomic development and increasing awareness of primary care practitioners might have contributed to the observed increase in leukaemia cases , although reasons for the stabilisation of leukaemia incidence in northern europe are unclear . incidence of lymphoma was relatively high compared with incidence of leukaemia in children in eastern europe . 
furthermore , diagnosis of lymphoma might be delayed until older ages , especially if the decreasing trend in children is accompanied by an increasing trend in adolescents , as seen in the east over the second decade . 
the high incidence in southern europe is consistent with previous reports of possible environmental exposures.30 a further assessment of lymphoma trends by diagnostic subgroups , narrower age groups , and sex could help provide a more specific explanation of the observed temporal changes . the stability of malignant cns tumour incidence in adolescents is encouraging , although drawing firm conclusions should be postponed until incidence trends are examined using data that include non - malignant tumours in the populations in which these are ascertained completely to exclude the possible effect of changes in classification of tumours . 
in children , because of the shown persisting increase in incidence in malignant cns tumours , and the exclusion of non - malignant tumours specifically pilocytic astrocytomafrom our analyses , a further detailed assessment is warranted , especially considering the poor outcome for such tumours . the trends for all other cancers combined show that the overall increase in incidence is not explained solely by changes in the three major groups of childhood and adolescent cancer . 
this fact is especially relevant in adolescents , as many cases are germ cell tumours and carcinomas.1 the candidate explanatory groups for the increase in at least a part of the period are thyroid carcinoma , 31 testicular tumours , 32 and melanoma.33 in particular , the patterns for belarus are probably shaped by the pronounced increase and later waning of thyroid cancer incidence during the study period , reflecting exposure to the radioactive fallout from the chernobyl accident.34 these observations also merit detailed studies . in summary , in this study we aimed to provide an overview of cancer incidence trends in children and adolescents in europe , as an introduction to a detailed investigation of patterns and trends and their possible determinants by diagnostic group and other subcategories in a concerted series of studies . 
the diversity of trends across the regions and tumour groups warrants further monitoring and a more detailed assessment of the high - quality data collected by cancer registries , by specific tumour types and population subgroups . 
whether the observed increase in cancer incidence in children and adolescents is due to enhanced discovery of cases or changing risk factors , the known frequency of cancer in young people should be considered in cancer control programmes . 
without an accurate quantification of the possible causes of this increase , whether real or artifactual , it is prudent to continue aetiological research into the causes of cancer in children and adolescents and to explore possible preventive measures . contributors es - f , bl , pk , jwc , rp - b , and cas designed the study , and contributed to data acquisition and evaluation . 
es - f did the literature search and drafted the manuscript , which was reviewed , modified , and approved by all coauthors . declaration of interests we declare no competing interests . acknowledgments we gratefully acknowledge the cofunders of this study . 
data acquisition was partly supported by the federal ministry of health of the federal german government and the development of infrastructure relevant to this study was enabled through the eus seventh framework programme ( fp7 / 20072013 ) under grant agreement lsshct200821 9453 ( eurocourse )  . 
the required funding was completed by the international agency for research on cancer . correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections for the clinical oncology society australia position statement on exercise in cancer care see au / media / 332488 / cosaposition - statement - v4 - webfinal.pdf exercise and cancer treatment : balancing patient needs on may 7 , 2018 , the clinical oncology society of australia launched a position statement recommending that exercise should be prescribed to all patients with cancer as part of their treatment regimen . 
the statement which has been endorsed by 25 leading health and care organisations , including the cancer council australia , the medical oncology group of australia , and the australian physiotherapy association , and echoes similar guidelines by cancer research uk and the american college of sports medicinesays that exercise should be viewed as an adjunct to therapy to help counteract the adverse effects of cancer and its treatment . 
although the decision is a welcome move that increasingly recognises patient quality of life as a vital component of cancer care , two crucial questions remain : does the evidence base adequately support the decision , and can such an approach be suited to the diverse range of cancer types and patients who are inflicted with the disease ? it is no surprise that much epidemiological evidence in recent years has shown that , with improvements in early detection and treatment , increasing numbers of patients with cancer can expect to be alive 5 years after their diagnosis and join a growing population of cancer survivors . 
although these trends are encouraging and show that improvements in cancer treatment , prevention , and detection have translated into real improvements in survival outcomes , it cannot go unrecognised that the disease and its treatment are often associated with longterm health and psychosocial sequelae . 
these sequelae most often increased fatigue , fear of recurrence , and diminished personal relationships , as well as an increased risk of developing secondary malignant diseases and other conditions , such as cardiovascular disease , diabetes , and osteoporosis , compared with the general population . 
given such evidence , it would be no hard push to declare that those with cancer are a vulnerable population with distinct health - care needs , of which exercise will , of course , help alleviate some of these competing conditions . include depression , anxiety , although the clinical oncology group of australia statement emphasises that patients should be physically active as much as their abilities and conditions allow , it would be naive to think that there can , or should , be a one - size - fits - all approach to suit all patients . 
for example , patient comorbidities and fragility , which are often associated with increased age , are factors that need to be adequately considered when recommending the feasibility of any physical activity regimen . 
equally , a degree of sensitivity is needed in , first , recommending physical activity measures that do not shame patients into thinking their disease is solely the consequence of their lifestyle choices and , second , recognising that exercise is not necessarily the single and vital factor determining treatment success , but rather emphasising it as a way to improve quality of life and wellbeing . 
on a practical level , recommendations will need to be given within the context of a patients life , in recognition of the often - debilitating effects of chemotherapy , surgery , and radiotherapy that might otherwise prevent patients from participating in exercise , a home and work life that might already be hard pressed to find time for exercise , and the need for an appropriate support network to encourage exercise as a feasible and sustainable treatment option . moreover , caution is needed when looking at the evidence base that informed these recommendations . 
 although epidemiological evidence has shown that being physically active can provide a protective effect against cancer recurrence , cancer - specific mortality , and all - cause mortality for some types of cancer , no evidence to date has evaluated whether the effects of exercise can positively affect cancer survivalalthough there are several clinical trials underway assessing exercise as a treatment intervention . 
indeed , despite having what seems like an insufficiently robust evidence base to inform a strong move in either direction , it is hugely encouraging to see that treatment interventions that focus on a patients quality of life and wellbeing are being seriously into the patient experience , and that incorporated exercise is now considered a vitally important component of cancer care at both ends of the care pathwayboth as a treatment and as a preventive measure . interventions that increasingly incorporate quality of life , the patient experience , and cancer survivorship into the treatment programme are welcome and laudable ways to ensure that patients are at the centre of the treatment process . 
but like any therapy , physical activity measures should be personalised to adequately meet a patients physical and psychological needs , and be delivered in such a way to support exercise as a viable and supportive treatment intervention . 
 the lancet oncology vol 19 june 2018 editorial risk of subsequent primary neoplasms in survivors of adolescent and young adult cancer ( teenage and young adult cancer survivor study ) : a population - based , cohort study chloe j bright , raoul c reulen , david l winter , daniel p stark , martin g mccabe , angela b edgar , clare frobisher , michael m hawkins summary background few studies have investigated the risks of subsequent primary neoplasms after adolescent and young adult ( aya ) cancer . 
we investigated the risks of specific subsequent primary neoplasms after each of 16 types of aya cancer . methods the teenage and young adult cancer survivor study is a population - based cohort of 200 945 survivors of cancer diagnosed when aged 1539 years in england and wales from jan 1 , 1971 , to dec 31 , 2006 . 
in this analysis , we focus on the risk of specific subsequent primary neoplasms after 16 types of aya cancer : breast ; cervical ; testicular ; hodgkin lymphoma ( female ) ; hodgkin lymphoma ( male ) ; melanoma ; cns ( intracranial ) ; colorectal ; non - hodgkin lymphoma ; thyroid ; soft - tissue sarcoma ; ovarian ; bladder ; other female genital ; leukaemia ; and head and neck cancer . 
we report absolute excess risks ( aers ; per 10 000 person - years ) and cumulative incidence of specific types of subsequent primary neoplasm after each type of aya cancer . findings during the 2 631 326 person - years of follow - up ( median follow - up 168 years , iqr 105252 ) , 12 321 subsequent primary neoplasms were diagnosed in 11 565 survivors , most frequently among survivors of breast cancer , cervical cancer , testicular cancer , and hodgkin lymphoma . 
aers of any subsequent primary neoplasms were 195 per 10 000 person - years ( 95% ci 174215 ) in survivors of breast cancer , 102 ( 80124 ) in survivors of cervical cancer , 189 ( 166211 ) in survivors of testicular cancer , 557 ( 504611 ) in female survivors of hodgkin lymphoma , and 299 ( 263336 ) in male survivors of hodgkin lymphoma . 
the cumulative incidence of all subsequent primary neoplasms 35 years after diagnosis was 119% ( 95% ci 113126 ) in survivors of breast cancer , 158% ( 148167 ) in survivors of cervical cancer , 202% ( 189215 ) in survivors of testicular cancer , 266% ( 247286 ) in female survivors of hodgkin lymphoma , and 165% ( 152180 ) in male survivors of hodgkin lymphoma . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma in women , breast cancer , and hodgkin lymphoma in men , we identified a small number of specific subsequent primary neoplasms that account for 82% , 61% , 58% , 45% , and 41% of the total excess number of neoplasms , respectively . 
lung cancer accounted for a notable proportion of the excess number of neoplasms across all aya groups investigated . interpretation our finding that a small number of specific subsequent primary neoplasms account for a large percentage of the total excess number of neoplasms in long - term survivors of cervical , breast , and testicular cancer , and hodgkin lymphoma provides an evidence base to inform priorities for clinical long - term follow - up . 
the prominence of lung cancer after each of these aya cancers indicates the need for further work aimed at preventing and reducing the burden of this cancer in future survivors of aya cancer . funding cancer research uk , national institute for health research , academy of medical sciences , and children with cancer uk . copyright 2019 the author ( s )  . 
 we searched pubmed without any language or date restrictions using the keywords teenage and young adult cancer or adolescent and young adult cancer and survivor or long - term and second cancer or subsequent cancer on feb 16 , 2016 , for articles describing subsequent primary neoplasms in this population . 
a more focused search using each specific aya cancer as keywords ( eg , hodgkin lymphoma ) in place of teenage and young adult cancer or adolescent and young adult cancer was also done . 
we identified only one study that investigated the risk of subsequent primary neoplasms after the entire spectrum of aya cancers diagnosed at 1539 years of age . added value of this study to our knowledge , this is the largest study to investigate the risks of subsequent primary neoplasm after each specific aya cancer and the first to provide excess risks of specific types of subsequent primary neoplasm after each of 16 types of aya cancer . 
unlike previous studies , which focused on the multiplicative risk , we concentrated on the absolute excess riskie , the excess number of subsequent primary neoplasms beyond those expected from the general population , which is directly interpretable in terms of adverse health impact on survivors . 
additionally , we identified a small number of specific subsequent primary neoplasms that account for a substantial proportion of the total excess number of neoplasms in survivors of breast cancer , cervical cancer , testicular cancer , and hodgkin lymphoma . implications of all the available evidence our findings advance previous knowledge on the risks of subsequent neoplasms after aya cancer and provide an evidence base for identifying priorities for clinical follow - up of survivors of aya cancer . 
because lung cancer accounted for a notable proportion of the excess number of neoplasms across all aya groups investigated , there is need for work aimed at reducing this burden among future survivors . primary breast cancer and primary hodgkin lymphoma had the highest absolute excess risk ( 544 and 486 per 10 000 person - years , respectively )  . 
however , the study did not investigate the risks of specific subsequent primary neoplasms after each specific type of aya cancer . evidence from previous studies of childhood cancer survivors suggests that the principal factors determining risks of subsequent primary neoplasms relate to aspects of treatments received for the original cancer.1416 treatment of aya cancer varies greatly by cancer type and therefore , in the absence of detailed treatment information , it is essential to stratify risks by specific types of aya cancer ; such risk stratification provides an evidence base for clinical follow - up . the aims of this large - scale population - based study were to calculate risks of all and specific subsequent primary neoplasms after each type of aya cancer and to explore variation in these risks in relation to years from diagnosis , age at diagnosis , decade of diagnosis , and sex . methods study design and participants the teenage and young adult cancer survivor study ( tyacss ) was established using cancer registrations relating to neoplasms diagnosed between jan 1 , 1971 , and dec 31 , 2006 , in individuals aged 1539 years inclusive , which were obtained from the office for national statistics for english cancer registrations , and the welsh cancer intelligence and surveillance unit , public health wales , for welsh cancer registrations . 
both tumourrelated ( eg , tumour site , morphology , date of diagnosis ) and patient - related ( eg , sex , date of birth , national health service [ nhs ] number , and unique patient identifier ) information were obtained . 
the cancer registrations were checked for any errors , such as missing data in essential variables ( including sex , date of birth , date of diagnosis , tumour site , and tumour histology ) and incorrect chronology of events ( birth , cancer , death )  . 
 cancer registrations were excluded if the neoplasm was not malignant ( apart from intracranial , intraspinal , and bladder neoplasms where any behaviour was allowed ) , the histological type was not in the international classification of diseases for oncology classification , the histological type was a non - melanoma skin cancer ( these are underascertained by cancer registries ) , or if they were duplicate registrations . 
we also excluded individuals who had a previous childhood cancer included in the british childhood cancer survivor study.17 if an individual had multiple neoplasms diagnosed as an aya cancer , then the first was regarded as the index cancer for the cohort . 
ethical approval was provided by the national research ethics service and permission to process information without individual consent by the national information governance board for health and social care . see online for appendix 532 vol 20 april 2019 articles procedures information on cancer diagnosis , sex , age at cancer diagnosis , decade of cancer diagnosis , and years since diagnosis were derived from the cancer registration information . 
first primary neoplasms were grouped according to the internationally acknowledged classification scheme for tumours diagnosed in adolescence and young adulthood.18 carcinomas and germ cell tumours were further subdivided by anatomical site because of the implications of radiotherapy site for the risk of subsequent primary neoplasm ( appendix pp 35 )  . 
 we aimed to produce risk estimates after each specific first primary neoplasm ; therefore , survivors of cancers categorised as other cancers were not included ( appendix pp 2 , 6 )  . 
we focused on the risk of specific subsequent primary neoplasms after 16 types of aya cancer : breast ; cervical ; testicular ; hodgkin lymphoma ( female ) ; hodgkin lymphoma ( male ) ; melanoma ; cns ( intracranial ) ; lymphoma ; colorectal ; non - hodgkin thyroid ; soft - tissue sarcoma ; ovarian ; bladder ; other female genital ; leukaemia ; and head and neck cancer . 
 decade of diagnosis was divided into 197179 , 198089 , and 19902006 , in order to broadly describe differences in treatment given in these periods ( early chemotherapy , chemotherapy , and modern treatment era )  . 
years since diagnosis were classified using 10 - year bands following diagnosis . individual patient record linkage to national cancer registries enabled data to be obtained indicating when an individual in the cohort had a subsequent cancer registration . 
subsequent cancer registrations were classified as a subsequent primary neoplasm according to the international association of cancer registries ( iacr ) and international agency for research on cancer ( iarc ) rules for determining multiple primary tumours using the iacr / iarc tools software . 
 to reduce the likelihood of a local spread of the original aya cancer being classified as a subsequent primary neoplasm , potential subsequent primary neoplasms occurring in anatomical sites close to the first primary neoplasm were excluded ( appendix pp 78 )  . 
consequently , reported risk estimates are inevitably conservative . statistical analysis individuals were followed from 5 - year survival until the first occurrence of death , emigration , or study end date ( dec 31 , 2012 )  . 
absolute excess risks ( aers ) were calculated as the observed minus expected number of neoplasms , divided by the person - years at risk and multiplied by 10 000 . 
the expected number of neoplasms was derived by multiplying the number of person - years accrued , stratified by sex , attained age ( 5 - year bands ) , and calendar year ( 1 - year bands ) by the corresponding cancer rate in the general population of england and wales , 19 and summing appropriately . 
for aya cancers with 200 or more observed subsequent primary neoplasms , sirs are reported by specific type of subsequent primary neoplas we restrict attention to first primary neoplasm / subsequent primary neoplasm combinations with at least 100 subsequent primary neoplasms and a statistically significant sir . 
 we considered aers to be statistically significant at the 5% level ( two - tailed test ) if the 95% ci did not include 0 . incorporating aers were stratified by years from diagnosis , age at diagnosis , decade of diagnosis , and sex where there were at least 100 subsequent primary neoplasms . 
to explore the simultaneous effect of these explanatory factors , the multivariable poisson regression expected number of events was used to derive relative excess risks ( rers ) .20 rers can be interpreted as the ratio of aers adjusted for other potential explanatory factors included within the statistical model . 
aers by an explanatory factor are reported if both the univariable and multivariable tests for linear trend in the aers were each significant and the difference in the aers between the lowest and highest level of the risk factor was at least nine excess subsequent primary neoplasms . 
a likelihood ratio test was used to test for linear trend in a factor by comparing the log - likelihood of a model including the variable of interest with the log - likelihood of a model without the variable of interest . 
in deciding the percentage of the total aer attributable to specific subsequent primary neoplasms in relation to years from diagnosis , we ignored negative values for the aer and focused only on the positive values . 
thus , the total aer ( for the purposes of calculating percentages ) after each specific first primary neoplasm is the sum of the positive values for the contributing subsequent primary neoplasms . cumulative incidence was calculated treating death as a competing risk . 
other aya cancers were not included in the analysis of subsequent primary neoplasms . table 1 : cohort characteristics we did sensitivity analyses in which subsequent leukaemia was included among survivors of aya hodgkin lymphoma , leukaemia , and non - hodgkin lymphoma , and subsequent sarcoma was included among survivors of soft - tissue sarcoma and bone tumours . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results the tyacss cohort comprises 200 945 5 - year survivors of cancer diagnosed when aged 1539 years , between jan 1 , 1971 , and dec 31 , 2006 , in england and wales . 
during the 2 631 326 person - years of follow - up ( median follow - up 168 years , iqr 105252 ) , 12 321 subsequent primary neoplasms were diagnosed in 11 565 ( 6% ) of the 197 827 survivors included in the analysis . 
subsequent primary neoplasms were most frequently seen in survivors of breast cancer ( 1877 [ 15% ] of 12 321 subsequent primary neoplasms ) , cervical cancer ( 1675 [ 14% ] ) , hodgkin lymphoma ( 1606 [ 13% ] ) , and testicular cancer ( 1435 [ 12% ] ; table 1 )  . 
median follow - up was 143 years ( iqr 91223 ) in survivors of breast cancer , 202 years ( 128272 ) in survivors of cervical cancer , 177 years ( 117253 ) in survivors of testicular cancer , 193 years ( 123270 ) in female survivors of hodgkin lymphoma , and 196 years ( 121275 ) in male survivors of hodgkin lymphoma . 
investigation of all first primary neoplasm / subsequent primary neoplasm combinations with at least 100 subsequent primary neoplasms showed that neither age at diagnosis nor decade of diagnosis was systematically associated with aers , apart from age at diagnosis for breast cancer after female hodgkin lymphoma and decade of diagnosis for lung cancer after male hodgkin lymphoma ( appendix p 9 )  . 
 consequently , in this report we consider only variation of aers with years from diagnosis and sex . female survivors of breast cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 20 excess subsequent primary neoplasms per 10 000 person - years ( sir 18 , 95% ci 1718 ; aer 195 per 10 000 person - years , 95% ci 174215 ; table 2 )  . 
 sirs for subsequent primary cancers of ovarian , lung , corpus uteri , other genital , melanoma , and colorectal sites were statistically significantly increased ( table 3 )  . 
 the total aer of developing any subsequent primary neoplasm increased statistically significantly with time from breast cancer diagnosis to an aer of 256 per 10 000 person - years ( 95% ci 104408 ) subsequent to 30 years from diagnosis ( p < 00001 ; table 4 )  . 
consists of 80 small intestine , 62 gallbladder , 77 retroperitoneum and peritoneum , and 31 other or unspecified . table 3 : risk of specific subsequent primary neoplasms ( row headings ) after specific aya cancers * ( column headings ) with at least 200 subsequent primary neoplasms observed in total neoplasms ( total aer 289 per 10 000 person - years when negative aers are excluded )  . 
the total aer of developing any subsequent primary neoplasm increased with time from cervical cancer diagnosis to an aer of 323 per 10 000 person - years ( 95% ci 154491 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing lung , colorectal , and bladder cancer ( each vol 20 april 2019 articles 538 vol 20 april 2019 articles for the aers lung cancer p < 00001 ; table 4 )  . 
in patients who had survived at least ( 172 per 30 years , 10 000 person - years , 95% ci 88256 ) , colorectal cancer ( 107 , 35179 ) , and bladder cancer ( 101 , 45157 ) accounted for 37% , 23% , and 22% of the total number of excess neoplasms , respectively ( total aer 465 per 10 000 person - years when negative aers are excluded )  . 
 the cumulative lung , colorectal , and bladder neoplasms at 35 years from diagnosis were 36% ( 95% ci 3242 ) , 26% ( 2230 ) , and 13% ( 1016 ) , whereas incidences of 16% , 14% , and 04% were expected , respectively ( figure , table 5 )  . incidences of subsequent survivors of testicular cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 19 excess subsequent primary neoplasms per 10 000 person - years ( sir 18 , 95% ci 1719 ; aer 189 per 10 000 person - years , 95% ci 166211 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from testicular cancer diagnosis to an aer of 1270 per 10 000 person - years ( 95% ci 10001540 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing bladder , colorectal , lung , and prostate cancer ( each p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aers for prostate cancer ( 253 per 10 000 person - years , 95% ci 121386 ) , bladder cancer ( 228 , 130327 ) , colorectal cancer ( 196 , 92299 ) , and lung cancer ( 95 , 01188 ) accounted for 20% , 18% , 15% , and 8% of the total number of excess neoplasms , respectively . 
 incidences of subsequent primary the cumulative neoplasms at 35 years from diagnosis were 37% ( 95% ci 3144 ) for prostate , 29% ( 95% ci 2436 ) for bladder , 30% ( 2536 ) for colorectal , and 27% ( 2232 ) for lung , whereas incidences of 29% , 11% , 18% , and 20% were expected , respectively ( figure , table 5 )  . female survivors of hodgkin lymphoma had an excess risk of developing any subsequent primary neoplasm corresponding to 56 excess subsequent primary neoplasms per 10 000 person - years ( sir 31 , 95% ci 2933 ; aer 557 per 10 000 person - years , 95% ci 504611 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from hodgkin lymphoma diagnosis to an aer of 1686 per 10 000 person - years ( 95% ci 12952078 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing breast and lung cancer ( each p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aers for breast cancer ( 718 per 10 000 person - years , 95% ci 464972 ) and lung cancer ( 260 , 112408 ) accounted for 43% and 15% of the total number of excess neoplasms , respectively . 
the total aer of developing any subsequent primary neoplasm increased with time from hodgkin lymphoma diagnosis to an aer of 1219 per 10 000 person - years ( 95% ci 9131524 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing lung cancer ( p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aer for lung cancer ( 502 per 10 000 person - years , 95% ci 330673 ) accounted for 41% of the total number of excess neoplasms . 
the cumulative incidence of lung neoplasms in male survivors of hodgkin lymphoma was 51% ( 95% ci 4360 ) at 35 years from diagnosis , whereas an incidence of 14% was expected ( figure , table 5 )  . female survivors of thyroid cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 13 excess subsequent primary neoplasms per 10 000 person - years ( sir 14 , 95% ci 1215 ; aer 131 per 10 000 person - years , 95% ci 84178 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from thyroid cancer diagnosis to an aer of 219 per 10 000 person - years ( 95% ci 109 to 547 ) subsequent to 30 years from diagnosis , ( p = 003 ; table 4 )  . 
 the cumulative incidence of all subsequent primary neoplasms in female survivors of thyroid cancer was 182% ( 95% ci 161205 ) at 35 years from diagnosis ( table 5 ) , whereas an incidence of 136% was expected . 
the cumulative risks for the specific subsequent primary neoplasms add up to more than the overall cumulative risk because survivors can develop more than one subsequent primary neoplas * all subsequent primary neoplasms in female survivors excluding subsequent primary neoplasms of the breast . 
||all subsequent primary neoplasms in female survivors excluding subsequent primary neoplasms of the thyroid . table 5 : cumulative incidence of specific subsequent primary neoplasms after specific first primary neoplasms by years from diagnosis to 12 excess subsequent primary corresponding neoplasms per 10 000 person - years ( sir 14 , 95% ci 1215 ; aer 123 per 10 000 person - years , 95% ci 75171 ; table 2 )  . 
the cumulative incidence of all subsequent primary neoplasms was 139% ( 95% ci 122157 ) at 35 years from diagnosis ( table 2 ) , whereas an incidence of 123% was expected . both male and female survivors of cns tumours had an excess risk of developing any subsequent primary vol 20 april 2019 articles neoplasm corresponding to 15 and 11 excess neoplasms , respectively ( male survivors : sir 17 [ 95% ci 1519 ] ; aer 148 per 10 000 person - years [ 95% ci 107190 ] ; [ 1215 ] ; female survivors : sir 13 aer 111 [ 70152 ] )  . 
a statistically significant reduction in the sir for the development of a subsequent primary breast cancer was found ( sir 07 , 95% ci 0608 ; table 3 )  . 
the cumulative incidence of all subsequent primary neoplasms was 119% ( 95% ci 106133 ) in female survivors of cns tumours and 100% ( 87114 ) in male survivors of cns tumours at 35 years from diagnosis ( table 2 ) , whereas an incidence of 94% was expected . sensitivity analyses showed that inclusion of leukaemia after aya hodgkin lymphoma , non - hodgkin lymphoma , and leukaemia had little effect on the sirs and aers ( appendix p 10 )  . 
inclusion of sarcomas after aya softtissue sarcoma and bone tumour increased the aers , but there was substantial overlap in confidence intervals ( appendix p 10 )  . discussion we show that the excess number of subsequent primary neoplasms observed increases with increased period of follow - up from diagnosis after each aya cancer investigated . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma in women , breast cancer , and hodgkin lymphoma in men , we identified just a small number of specific subsequent primary neoplasms that account for 82% , 61% , 58% , 45% , and 41% of the total excess number of neoplasms , respectively . 
one study has previously addressed the risk of all subsequent primary neoplasms combined after each aya cancer , 3 but no study has previously considered specific subsequent primary neoplasms . in our study , the burden of the excess number of neoplasms beyond 30 years from diagnosis accounted for by lung cancer was substantial and apparent across all aya cancers investigated ( breast , cervical , testicular , and hodgkin lymphoma in males and females )  . 
additionally , smoking increases the risk of developing subsequent primary neoplasms , particularly oral or pharyngeal , oesophageal , stomach , lung , and haematological malignancies.21 kaul and colleagues22 reported that 33% of survivors of aya cancer were current smokers compared with 22% in a non - cancer comparison group matched on age , sex , and other factors . 
 although this decrease could be caused by a number of factors , it might be related to a change in smoking habits in more recent decades ( ie , a reduction in male smokers )  . 
 the evidence presented in our study , along with previous literature on smoking in cancer survivors , clearly suggests that clinical follow - up of survivors of aya cancer , particularly survivors of breast cancer , cervical cancer , and hodgkin lymphoma , should focus on subsequent lung cancer and provision of smoking cessation advice . generally , it is difficult to compare risks of subsequent primary neoplasms between survivors of aya and childhood cancer because there are so many important confounding influences . 
however , lung cancer as a subsequent primary neoplasm is an exception to this general rule in that from our population - based national cohort of survivors of childhood cancer in britain , we reported that in survivors aged 40 years and older , lung cancer was associated with an aer of only 29 per 10 000 person - years ( 95% ci 0455 ) , which accounted for just 9% of the total aer.28 by contrast , in the present analysis , the aer for lung cancer after at least 30 years from diagnosis of aya cancer was substantially higher and accounted for a much greater proportion of the total aer . 
notably , by contrast with survivors of aya cancer , the odds ratio for being a current regular smoker among survivors of childhood cancer in britain was 051 compared with the general population of britain.29 in female survivors of breast cancer , the sirs reported in our study were broadly consistent with those reported in previous literature.57 the increased risk of ovarian cancer could relate to shared hormonal and genetic ( eg , brca1 and brca2 mutations ) risk factors.30 the increased risk of uterine cancers might relate to partial oestrogen agonists used to treat the breast cancera previous large case - control study found that risk of uterine cancer increases with duration of tamoxifen treatment.31 of the six anatomical sites at which an excess of subsequent primary neoplasms was observed , only the lungs would be directly exposed if external - beam radiotherapy was used to treat the breast cancer . 
a previous large case - control study showed a dose - response relation between radiotherapy and risk of lung cancer in breast cancer survivors diagnosed at any age ( not aya - specific ) .26 existing literature suggests that chest 542 vol 20 april 2019 articles radiotherapy and smoking are both likely contributors to the substantial number of excess neoplasms accounted for by lung cancer . the bladder and bowel would be directly exposed if external - beam radiotherapy was used to treat cervical cancer . 
a large case - control study showed a doseresponse relation between radiotherapy and the risk of both bladder and rectal cancers in cervical cancer survivors.32 existing that pelvic irradiation and smoking are likely contributors to the number of excess neoplasms accounted for by lung , colorectal , and bladder cancer . 
clinical follow - up of survivors of aya cervical cancer , particularly where pelvic irradiation is used , should focus on lung , bowel , and bladder cancers . literature suggests treatment for testicular cancer can involve irradiating the para - aortic lymph nodes , which might explain the excess of subsequent primary neoplasms seen abdominal sites ( prostate , bladder , and colorectal )  . 
the excess of subsequent primary neoplasms observed in the abdomen is consistent with international studies of testicular cancer survivors.8 the excess of lung subsequent primary neoplasms might be caused by radiotherapy to the lungs , since previous studies have reported an increased risk of lung cancer in survivors of testicular cancer who were given chest radiotherapy.8 clinical follow - up of survivors of aya testicular cancer should focus on prostate , bladder , colorectal , and lung cancers . the lungs would be directly exposed if external - beam radiotherapy was used to treat hodgkin lymphoma ; previous studies of hodgkin lymphoma survivors have provided evidence of a dose - dependent increase in lung cancer risk with radiotherapy with or without chemotherapy.27 our findings are consistent with previous large - scale studies of female survivors of hodgkin lymphoma , for which a substantial amount of literature already exists , and by contrast with other aya cancers considered here , we have little to add.911 our findings support the decrease in lung cancer risk with more recent calendar period of diagnosis that was reported in a dutch study of hodgkin lymphoma survivors.9 this decrease might be due to a latency effect , where more recently diagnosed survivors simply have not had enough time to develop a lung subsequent primary neoplasm , or it might be caused by changes in treatment for hodgkin lymphoma during recent decades , including withholding the delivery of radiotherapy or radiotherapy resulting in less damage to healthy tissue than in previous decades.33 however , because a decrease in lung cancer risk was not seen after hodgkin lymphoma in women , it is possible that the decrease in lung cancer in men is caused by other environmental influences , such as changes in smoking habits . 
previous studies have reported an increase in the number of excess lung cancers with increasing years from diagnosis ; 9 , 10 however , to our knowledge , our study is the first to report the number of excess lung cancers in male and female improvements survivors separately . 
existing literature suggests that treatment ( radiotherapy and chemotherapy ) , in addition to smoking , could contribute to the number of excess neoplasms accounted for by lung cancer.9 clinical followup of male survivors of aya hodgkin lymphoma should focus on lung cancer and provision of smoking cessation advice . younger age at radiation exposure is a risk factor for the development of breast cancer in many populations exposed to radiation , including atomic bomb survivors , patients with tuberculosis monitored with x - rays , and children with benign disorders treated with radiotherapy.34 thus , the effect of age at diagnosis ( closely related to age at radiotherapy ) of hodgkin lymphoma on the risk of breast cancer in our cohort is not surprising . knowledge of late effects of cancer treatment has resulted in lower radiation exposures for treatments of good prognosis cancers in recent years ; 35 however , the multivariable regression showed the risk of developing a subsequent primary neoplasm did not vary with decade of diagnosis of aya cancer apart from lung cancer after hodgkin lymphoma in males . 
therefore , currently there is little evidence of a detectable impact . that until recently , no internationally agreed clinical guidelines existed regarding surveillance for specific types of neoplasm after aya cancer , but this is now being addressed by the international late effects of childhood cancer guideline harmonization group.36 so far , two such guidelines have been published.37 , 38 there are also guidelines in development relating to second primary cns tumours and second primary bowel cancers . strengths of our cohort study relate to its large scale and population - based design , with the inclusion of all 5 - year survivors of aya cancer in england and wales . 
our study had much greater statistical power than the only comparable previous study by lee and colleagues , 3 because we report almost double the number of subsequent primary neoplasms and an additional million person - years of follow - up . 
most previous studies investigating the risk of subsequent primary neoplasms with years from diagnosis have mainly focused on the sir , a measure of multiplicative risk that relates to an unspecified baseline risk and is therefore difficult to interpret . 
we concentrated on the aer , which is the excess number of subsequent primary neoplasms beyond those expected from the general population , and so is directly interpretable in terms of adverse health impact on survivors . 
to our knowledge , our study is the first to report aers by years from diagnosis for each specific aya cancer . a limitation of using cancer registration data is the absence of detailed treatment information . 
treatment for aya cancer varies greatly by cancer type ; therefore , in the absence of treatment data , we chose to determine risks in relation to specific cancer types . 
however , inevitably vol 20 april 2019 articles there is variation in the intensity of treatment given for a specific type of cancer , depending on the stage at diagnosis and whether the disease recurs or relapses after initial treatment . 
crude treatment information is inherent in cohort studies based on cancer registry data ; however , we are planning to conduct case - control studies with detailed treatment dosimetry , questionnaires for lifestyle and other relevant factors , and saliva collection for genotypic factors . 
a potential limitation of our study is that our results might not be generalisable to populations outside of england and wales . another limitation is the possibility that recurrence or metastases of the aya cancer could have been mistaken for a subsequent primary neoplas however , we used the iacr / iarc rules to define multiple primary cancers and further excluded any additional neoplasms close to the aya cancer site . 
thus , our estimate of the risk of specific subsequent primary neoplasms after specific aya cancers is probably conservative , and although many of the estimates we report are substantial , they are likely to be an underestimate of the true risk . in conclusion , our data show that the excess number of subsequent primary neoplasms observed increases with increased period of follow - up from diagnosis after each aya cancer investigated . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma , and breast cancer , we identified just a small number of specific subsequent primary neoplasms that account for high proportions of the total excess number of neoplasms . 
a notable finding was the excess number of neoplasms accounted for by lung cancer across all aya groups investigated in detail , in addition to subsequent primary neoplasms occurring in potentially irradiated sites . 
our findings provide an evidence base for clinical follow - up relating specifically to the aya population . contributors cjb did the literature search and data analysis , created the figure , and drafted the report . 
cjb , rcr , dlw , mmh , cf , dps , mgm , and abe interpreted the data , and reviewed and finalised the report . declaration of interests dps reports grants from teenage cancer trust , outside the submitted work . 
other funding was provided by a post - doctoral fellowship to rcr from the national institute for health research ( pdf - 2012 - 05 - 280 ) , and by the academy of medical sciences ( springboard health of the public 2040 ) and children with cancer uk . 
 study collaborators include sarah darby ( university of oxford ) ; richard feltbower ( university of leeds ) ; lorna anne fern ( university college london ) ; diana greenfield ( sheffield teaching hospital nhs foundation trust ) ; helen alexandra spoudeas ( university college london hospitals nhs foundation trust ) ; william hamish wallace ( royal hospital for sick children , edinburgh ) ; and jeremy whelan ( university college london hospitals nhs foundation trust )  . 
this report is independent research and the views expressed in this article are those of the author ( s ) and not necessarily those of nhs digital , cancer research uk , the national institute for health research , the office for national statistics , or the welsh cancer registry . relapse of wilms tumour and detection methods : a retrospective analysis of the 2001 renal tumour study groupinternational society of paediatric oncology wilms tumour protocol database jesper brok , marta lopez - yurda , harm v tinteren , taryn d treger , rhoikos furtwngler , norbert graf , christophe bergeron , marry m van den heuvel - eibrink , kathy pritchard - jones , ystein e olsen , beatriz de camargo , arnauld verschuur , filippo spreafico summary background wilms tumour is the most common renal cancer in childhood and about 15% of patients will relapse . 
 there is scarce evidence about optimal surveillance schedules and methods for detection of tumour relapse after therapy . methods the renal tumour study groupinternational society of paediatric oncology ( rtsgsiop ) wilms tumour 2001 trial and study is an international , multicentre , prospective registration , biological study with an embedded randomised clinical trial for children with renal tumours aged between 6 months and 18 years . 
the current protocol of siop surveillance for wilms tumour recommends that abdominal ultrasound and chest x - ray should be done every 3 months for the first 2 years after treatment and be repeated every 46 months in the third and fourth year and annually in the fifth year . 
in this retrospective cohort study of the protocol database , we analysed data from participating institutions on timing , anatomical site , and mode of detection of all first relapses of wilms tumour . 
the primary outcomes were how relapse of wilms tumour was detected ( ie , at or between scheduled surveillance and with or without clinical symptoms , scan modality , and physical examination ) and to estimate the number of scans needed to capture one subclinical relapse . 
 the rtsgsiop study is registered with eudra - ct , number 2007 - 004591 - 39 . findings between june 26 , 2001 , and may 8 , 2015 , of 4271 eligible patients in the 2001 rtsgsiop wilms tumour database , 538 ( 13% ) relapsed . 
the primary imaging modality used to detect relapse was reported for 251 patients , among which relapse was identified by abdominal ultrasound ( 80 [ 32% ] patients ) , chest x - ray ( 78 [ 31% ] ) , ct scan of the chest ( 64 [ 25% ] ) or abdomen ( 20 [ 8% ] ) , and abdominal mri ( nine [ 4% ] )  . 
the estimated number of scans needed to detect one subclinical relapse during the first 2 years after nephrectomy was 112 ( 95% ci 106119 ) and , for 25 years after nephrectomy , 500 ( 416588 )  . interpretation planned surveillance imaging captured more than two - thirds of predominantly asymptomatic relapses of wilms tumours , with most detected by abdominal ultrasound , chest x - ray , or chest ct scan . 
the international society of paediatric oncology ( siop ) approach is to monitor for relapse after treatment with chest x - rays and abdominal ultrasound , whereas alternating chest x - rays and abdominal ultrasound and chest and abdominal ct is advised by the childrens oncology group . 
a few , relatively small , retrospectives reports have shown that ct scans can be omitted from surveillance , while highlighting the need for larger prospective studies to assess the benefit and harms of surveillance strategies for wilms tumour . added value of this study this study provides new data about how relapse of wilms tumour is detected . 
although we acknowledge that regional and individual hospitals might make possible minor adjustments , the recommendations for surveillance in the 2001 siop wilms tumour study enabled centres to capture more than two - thirds of , predominantly asymptomatic , wilms tumour relapses . 
however , asymptomatic relapses , captured by surveillance scans , have a better prognosis than do relapses presenting with clinical symptoms between routine follow - up . implications of all the available evidence 2001 siop recommendations , which include abdominal ultrasound and chest x - ray , capture a high proportion of asymptomatic relapses . 
surveillance beyond 2 years after treatment could be consideredas is mandatory for bilateral tumours with increased risk of metachronous relapse and patients with wilms tumour predisposition syndromesbut the overall number of abdominal ultrasounds and chest x - rays needed to capture one asymptomatic relapse would be about 500 . 
randomised trials are needed to assess different surveillance regimens but are less likely to be prioritised over trials of new treatment options . occurring within 2 years after nephrectomy and only occasionally after 5 years.5 the lung is the most common site of relapse for wilms tumour ; local or regional frequently , abdominal relapses occur slightly whereas liver and especially brain and bone involvement is rare.6 , 7 overall survival after relapse is about 50% but the outcome varies depending on several factors . 
key prognostic factors used to stratify treatment for relapse are histological risk group , tumour stage , and previous treatment intensity.610 less as the number of children with wilms tumour or other childhood cancers achieving first complete remission increases , the pressure to detect recurrent tumours places a burden on the childs family and the healthcare syste the aim of such surveillance is to detect relapse at an earlier stage , when prognosis might be better or require less intensive treatment . 
however , fundamental knowledge about costs , benefits , and potential risks of different surveillance strategies for wilms tumour and other childhood cancers is scarce.11 intensive imaging could add unnecessary radiation exposure , and frequent hospital visits after treatment might cause psychological distress to the child and their family.12 , 13 efficacy of surveillance strategies and schedules for wilms tumour has never been prospectively assessed , and are unlikely to be prioritised because the focus of research in this field is on treatment ( ie , new treatment options for patient with poor prognosis [ eg , relapse ] ) and refinement of current treatment through improved risk stratification . 
the few randomised clinical trials done in adults with cancers have shown conflicting results regarding whether or not intensive monitoring for relapse improves outcomes.14 the best methods , duration , and frequency of surveillance for patients with wilms tumour after treatment are still under debate ; therefore , followup strategies can vary geographically depending on available resources and national or regional habitual practices . 
so far , nearly 6000 children and adolescents with renal tumours have been registered on the 2001 trial and study by the international society of paediatric oncology ( siop ) renal tumour study group ( rtsg )  . 
this protocol regular chest xrays and abdominal ultrasound scans for several years depending on initial tumour stage and histology ( table 1 ) .15 data from this large cohort could provide additional useful evidence about the efficacy of routine imaging for the surveillance of tumour relapse . recommended in this retrospective analysis , we describe the timing , anatomical site , and mode of detection of all first relapses of wilms tumour reported in the 2001 siop wilms tumour trial and study . 
we also estimate the number of scans needed to identify one relapse , explore prognostic factors for postrelapse survival , and use the results to evaluate existing surveillance guidelines . vol 19 august 2018 1073 articles chest x - ray abdominal ultrasound localised and metastatic wilms tumour * years 1 and 2 every 3 months every 3 months year 3 year 4 year 5 every 4 months every 4 months every 6 months every 6 months annually annually bilateral tumours and nephrogenic rests years 1 and 2 years 3 and 4 years 510 every 2 months every 2 months every 3 months every 3 months annually annually data from personal communication with national principal investigators of the 2001 wilms tumour study by the international society of paediatric oncology renal tumour study group . 
 * little individual and institutional variation in the total duration and frequency of surveillance imaging . table 1 : imaging surveillance recommendations for wilms tumour after stopping treatment methods study design and participants the siop wilms tumour 2001 trial and study is an international , multicentre registration and biological study with an embedded randomised clinical trial for children with renal tumours aged between 6 months and 18 years . 
after nephrectomy , the intensity and duration of postoperative chemotherapy , occasionally radiotherapy , was determined by tumour histopathology and stage ( appendix p 1 ) .1519 the siop histological classification of pretreated wilms tumour considers three risk groups , which account for the relative proportion of viable tumour cells and necrotic or regressive changes : low risk ( 100% necrotic or cystic tumour ) , intermediate risk ( epithelial , stromal , mixed , regressive type , and focal anaplasia ) , and high risk ( diffuse anaplasia and blastemal type )  . 
the trial closed on jan 1 , 2010 , and the reduced therapy experimental group ( without doxorubicin ) has become the new standard of care since 2011 for this subgroup of patients.15 , 16 here , we report a retrospective cohort study of eligible patients in the rtsgsiop database , which evaluated the current protocol of siop surveillance for wilms tumour that recommends abdominal ultrasound and chest xray should be done every 3 months for the first 2 years after treatment , with ongoing surveillance according to national guidance , usually repeated every 46 months in the third and fourth year ( table 1 )  . 
all participating centres accepted the surveillance scheme , with little regional and individual variation ( table 1 )  . procedures all participating institutions provided data through paper case record forms designed for initial diagnosis , followup , relapse , and end of relapse treatment . 
we collected the following data : sex , age , country , tumour histology and stage , tumour volume at nephrectomy ( based on radiological dimensions and calculated in cm as length width height 0523 ) , nephrectomy ( day 0 ) , relapse status , scan modality that detected relapse , whether a relapse was diagnosed at scheduled surveillance visits or interim ( unscheduled ) because of clinical symptoms , site of relapse , interval between nephrectomy and relapse , interval between relapse and latest normal scan , and overall survival . 
if no information ( ie , an empty box in the case record ) was provided , this was considered missing data . date the we classified any subsequent tumourrelated event in patients with initial bilateral wilms tumour or wilms tumour predisposition syndromes as relapse , but are aware that a proportion might be a new metachronous tumour . outcomes the primary outcomes of this retrospective data analysis were how relapse of wilms tumour was detected ( ie , at or between scheduled surveillance and with or without clinical symptoms , scan modality , and physical examination ) and to estimate the number of scans needed to capture one subclinical relapse . 
in relapsing patients , overall survival was calculated from the time of relapse until death from any cause . statistical analysis we used the kaplanmeier method to generate survival curves and used the logrank test for overall comparisons across all groups . 
from the computed overall survival probabilities , we calculated incidence of relapse within any time period , and accounted for competing risk events ( mortality ) in a separate analysis . 
we did non parametric estimation of the incidence of relapse in the presence of competing risks events in a twostep process.20 , 21 we calculated the kaplanmeier estimate of overall survival from any event ( ie , including relapse and death as events in this model ) , then calculated the conditional probabilities of experiencing the event of interest and used them to estimate the cumulative incidences.22 for overall survival and relapsefree interval , patients without an event at the end of follow up were censored at that time . 
we did univariable and multivariable cox proportional hazards regression analysis , stratified by country , for overall survival and relapsefree continuous variables ( patient age and time to relapse ) ; linear trend tests were based on the slope for the variable . 
hence , a missing date of nephrectomy was input as being 4 weeks ( for localised wilms tumour ) or 6 weeks ( for metastatic wilms tumour ) after the start of treatment . 
we did multiple imputations with the fully conditional method on missing patient clinical characteristics , assuming data were missing at rando this assumption was considered plausible because the absence of data was often related to the centre ( not all information from all centres could be incorporated into the database in time for our analyses ) , rather than unobserved characteristics or the missing data themselves ( appendix pp 34 )  . 
we compared overall survival among relapsed patients according to the same variables , including interval from nephrectomy to relapse , site of relapse , relapse detected at followup with or without symptoms , and interval from last scan without any signs of relapse . 
we used r ( version 3.4.1 ) and sas ( version 9.4 ) for all analyses . role of the funding source the funders of the study had no role in the study design , data collection , data analysis , data interpretation , or writing of the report . 
 table 2 : characteristics of patients with wilms tumour in the study results between june 26 , 2001 , and may 8 , 2015 , 5769 children with renal tumours were registered in the siop wilms tumour 2001 study database ( appendix pp 56 )  . 
we excluded 694 cases of nonwilms renal tumours , 121 with insufficient data , 646 not treated with preoperative chemotherapy according to the protocol or outside the age range ( 6 months to 18 years ) , and 37 patients with progressive disease during preoperative chemotherapy from our analysis . 
at diagnosis , 3409 ( 80% ) of 4271 wilms tumours were localised , 582 ( 14% ) metastatic , and 280 ( 7% ) bilateral ( table 2 )  . at a median followup from surgery of 62 months ( iqr 3293 ) , relapse was reported in 538 ( 13% ) of 4271 patients . 
the site of relapse was registered for 461 ( 86% ) of 538 patients , of which 63 ( 15% ) had combined local and distant relapse and 398 ( 85% ) had relapse confined to either local recurrence or metastatic disease ( appendix p 1 )  . 
relapse involved the lung in 291 ( 63% ) of 461 patients ( including cases with extrapulmonary sites ) , vol 19 august 2018 1075 articles physical examination only imaging only physical examination and imaging method not specified total 1 ( < 1% ) 34 ( 6% ) 54 ( 10% ) symptomatic between scheduled surveillance asymptomatic at scheduled surveillance 3 ( 1% ) symptomatic at scheduled surveillance asymptomatic between scheduled surveillance presentation not specified total 1 ( < 1% ) 1 ( < 1% ) 2 ( < 1% ) 8 ( 1% ) 203 ( 38% ) 26 ( 5% ) 13 ( 2% ) 3 ( 1% ) 279 ( 52% ) 33 ( 6% ) 21 ( 4% ) 6 ( 1% ) 7 ( 1% ) 121 ( 22% ) 2 ( < 1% ) 241 ( 45% ) 89 ( 17% ) 48 ( 9% ) 20 ( 4% ) 128 ( 24% ) 130 ( 24% ) 140 ( 26% ) 538 ( 100% ) data are n ( % ) and are from the 2001 wilms tumour trial and study by the international society of paediatric oncology renal tumour study group . 
values do not sum to 100% because of rounding . table 3 : methods used to detect wilms tumour relapse stage i within period stage ii within period stage iii within period beyond period beyond period stage iv beyond period within period beyond period stage v within period beyond period low - risk or intermediate - risk histology months after nephrectomy 131 / 1395 76 / 647 64 / 525 70 / 398 26 / 196 high - risk histology months after nephrectomy 17 / 169 24 / 119 40 / 142 34 / 75 16 / 59 > 612 > 1218 > 1824 > 2430 > 3036 > 3642 > 4248 > 4854 > 5460 > 612 > 1218 > 1824 > 2430 > 3036 > 3642 > 4248 > 4854 > 5460 based on data from the 2001 wilms tumour trial and study by the international society of paediatric oncology renal tumour study group . 
incidence within period ( eg , 06 months after nephrectomy ) or beyond ( eg , 6 months after nephrectomy ) period was calculated by summing incidences corresponding to relapse times observed in or after the surveillance period . 
 * time to end of study ( may , 2015 ) was used for patients who did not relapse to minimise the effect of very late relapses on the estimates ( ie , a best - case scenario )  . 
 table 4 : estimated % incidence of relapse by initial tumour stage , histology , time from nephrectomy , * and time period of surveillance whereas abdominal or pelvic involvement with or without extraabdominal sites was seen in 225 ( 49% ) of 461 cases . 
 abdominal relapse included cases with locoregional relapse , liver relapse , and metachronous tumours in the contralateral kidney ( appendix , p 1 )  . the method used to detect relapse was registered for 410 ( 76% ) of 538 relapses ( table 3 )  . 
of these relapses , 289 ( 70% ) were captured during scheduled followup visits ( 48 [ 17% ] with clinical symptoms and 241 [ 83% ] without )  . 
 109 ( 27% ) relapses were diagnosed at unscheduled visits 1076 vol 19 august 2018 articles in the interim between planned followup imaging ( 89 [ 82% ] with clinical symptoms and 20 [ 18% ] without )  . 
 relapse was detectable by physical examination ( either with or without imaging ) in only 129 ( 31% ) of 410 cases ; 279 ( 68% ) were not detectable by physical examination ( table 3 )  . 
the primary imaging modality used for identification of relapse was registered for 251 patients , including abdominal ultrasound ( 80 [ 32% ] ) , ct ( 84 [ 33% ] , chest 64 [ 25% ] and abdomen 20 [ 8% ] ) , chest xray ( 78 [ 31% ] ) , and abdominal mri ( nine [ 4% ] )  . 
291 ( 71% ) relapses were found by routine scans within 2 years after nephrectomy , whereas 86 ( 67% ) were found more than 2 years after nephrectomy . timing of relapse was registered for 511 ( 95% ) of 538 patients . 
of these , 408 ( 80% ) occurred within 24 months post nephrectomy , 67 ( 13% ) within 2460 months , and very late relapse ( > 60 months ) was registered for 36 ( 7% ) patients . 
subgroup analyses showed that patients with highrisk histology and advanced tumour stage ( iiiv ) had the highest incidence of relapses occurring shortly ( 012 months ) after nephrectomy ( table 4 )  . 
in a multivariable cox regression analysis of overall survival after relapse , children presenting with clinical symptoms between scheduled number of events univariable analysis multivariable analysis hr ( 95% ci ) p value hr ( 95% ci ) p value time from nephrectomy to relapse female male age group * 6 months to 2 years 24 years 4175 years < 6 months 6 months site of relapse local local and distant lung only detection of relapse symptoms only other stage of wilms tumour histological risk high intermediate volume at nephrectomy 100 ml / unit 1 ( ref ) 1 ( ref ) 071 ( 052095 ) 0021 074 ( 054102 ) 006 057 ( 031103 ) 0061 073 ( 038143 ) 036 1 ( ref ) 1 ( ref ) 154 ( 110215 ) 0011 131 ( 091189 ) 015 188 ( 138255 ) < 00001 163 ( 115231 ) 00062 1 ( ref ) 1 ( ref ) 200 ( 130310 ) 00018 122 ( 076189 ) 126 ( 089180 ) 019 110 ( 074164 ) 041 063 186 ( 129268 ) 000081 184 ( 124274 ) 00027 149 ( 072309 ) 029 123 ( 062247 ) 055 1 ( ref ) 1 ( ref ) 235 ( 136407 ) 00023 234 ( 132415 ) 00038 410 ( 245684 ) < 00001 313 ( 181541 ) < 00001 571 ( 354922 ) < 00001 433 ( 258728 ) < 00001 223 ( 110451 ) 0026 174 ( 079384 ) 017 544 ( 395748 ) < 00001 463 ( 323641 ) < 00001 1 ( ref ) 1 ( ref ) 258 ( 104642 ) 0041 200 ( 076525 ) 016 105 ( 101108 ) 0012 101 ( 097105 ) 053 follow - up without symptoms 1 ( ref ) 1 ( ref ) follow - up with symptoms 134 ( 083217 ) 023 124 ( 071217 ) 045 multiple imputation of missing values are shown for 471 of 538 relapses , with follow - up information after relapse . 
 data for volume at nephrectomy were missing for 80 ( 17% ) of 471 patients and data for detection of relapse were missing for 122 ( 26% ) of 471 . 
 table 5 : cox regression analysis of risk factors for overall survival after relapse surveillance visits had worse postrelapse survival com pared with those without clinical symptoms at scheduled surveillance scans ( median postrelapse overall survival 22 months [ 95% ci 1142 ] for sympto matic patients vs not reached for asymptomatic patients ; hazard ratio 184 [ 95% ci 124274 ] ; p = 00027 )  . 
the following variables were also significant predictive risk factors for survival after relapse : less than 6 months from nephrectomy to relapse , stage ( ii , iii , and iv ) , and highrisk histology ( table 5 )  . 
 in addition to these variables , in the univariable analyses , male sex , older age , multiple sites of relapse , and increasing tumour volume were also significantly associated with shorter overall survival . discussion our retrospective cohort study of the 2001 multicentre rtsgsiop wilms tumour protocol database showed that 13% of children with wilms tumour relapsed , and about 80% of relapses occurred within 2 years after nephrectomy and predominantly involved the lung . 
our analyses showed that relapses among patients with high risk histology and advanced stage ( iiiv ) tumours occurred relatively early after nephrectomy , whereas those with stage v tumours without highrisk histology tended to relapse later . 
for all tumour stage and histological subgroups , the absolute risk of relapse at 2 years after nephrectomy was similar across subgroups . the assumption that earlier recognition of relapse , rather than data from controlled studies , will lead to a better prognosis influences physicians attitudes toward recommending surveillance imaging . 
 knowledge about how relapse of wilms tumour is detected is scarce , and the evidence to support current surveillance strategies is weak.23 since surveillance can be a burden for families and the healthcare system , we aimed to strengthen this evidence base by analysing the large cohort of patients with wilms tumour treated according to a standardised protocol with preoperative chemo therapy in the 2001 siop wilms tumour study . 
 guided by the protocol surveillance recommendation , we found that routine followup scans found at least 70% of the relapses , whereas physical examination , usually done by a paediatrician , was unable to detect recurrence in about twothirds of children . 
furthermore , early relapse , presentation with clinical symptoms in the interval between two scheduled followup visits , advanced tumour stage ( excluding stage v ) , and highrisk histology were associated with worse overall survival in patients who relapsed . frequently the main strengths of this study are the substantial number of patients , prospective data collection , and assessment of longterm outcomes . 
for the past 15 years , patients have been treated according to the same protocol 1078 vol 19 august 2018 articles without substantial changes in disease management , except that ct scans rather than xrays are now increasingly used for the standard for upfront diagnosis ( not surveillance ) of lung metastases and that , for a subgroup of patients with intermediate risk ( stage ii / iii ) , doxorubicinbased perioperative chemotherapy has been omitted since 2011 to reduce the risk of late effects.15 as is the case with all registration studies , incompleteness of some items , which led to exclusion of a small proportion of patients from our analysesmitigated by use of statistical imputation methodsmight be some limitations of our study . 
 finally , we did not record individual and centre surveillance strategies ; therefore , we calculated the number of scans needed to detect one relapse on the basis of the assumption that all patients adhered to the surveillance protocol recommended by siop . 
we recognise that minor unrecorded deviations in the real life practice of imaging surveillance might introduce bias when interpreting our data . we observed that , up to 2 years after surgery , most children had an interval of less than 3 months from last normal imaging to relapse . 
in some cases , it was not possible to conclude whether ct scan was used upfront or only to confirm equivocal chest xray findings ( the latter being more probable ) , so this issue could not be further explored in this analysis . 
lowdose ct scanning of the chest ( 12 msv per scan ) or abdomen might detect smaller nodules but will increase the radiation burden for the patient , and the added value of routine ct surveillance is still under debate.12 , 2326 than the mortality rate was nearly twotimes higher in patients presenting with clinical symptoms between planned surveillance visits in patients with asymptomatic relapse found by planned surveillance . 
 despite this notable disparity , the benefits of surveillance remain uncertain because the difference in mortality could be confounded by other factors , such as location of the tumour and tumourspecific growth rate ( ie , biological aggressiveness )  . 
the benefits of surveil lance imaging would have been further supported if an inferior outcome was associated with parameters such as prolonged interval between last normal surveillance scan and relapse or larger tumour size at relapse . 
to our knowledge , there are no other studies of a similar size on wilms tumour or other extracranial solid tumours with which we can compare our results . one key decision when planning wilms tumour surveillance is the cutoff relapse risk for entering and continuing surveillance . 
to guide this decision , we have created a socalled surveillance map that shows the estimated incidence of relapse for subgroups of wilms tumour at different timepoints after nephrectomy ( see table 4 )  . 
since one in four relapses are detected because of clinical symptoms , we estimated the number of relapses detected solely by biannual surveillance imaging at 2 years post nephr ctomy to be about one in 130 patients . 
when calculating estimates of relapse incidence , we used a bestcase scenario ( ie , followup of patients without an observed relapse was extended up to the end of the study period ) to minimise the effect of patients with very late relapses . 
 this assumption might slightly underestimate the true incidence . similar calculations can be made for other timepoints and subgroups , but these numbers show that a substantial proportion of healthy children undergo scans ( ultrasound , xray , or ct ) with potential harmful effects.12 a pragmatic cutoff risk of 5% for developing a tumour is used to decide whether children with wilms tumour predisposition syndromes should enter a screening programme of abdominal ultrasounds every 3 months . 
this interval accounts for the doubling rate of wilms tumour ( 10 days ) and the sensitivity of abdominal ultrasound.28 , 29 our results confirm that the risk of very late relapse is low , which suggests that prolonging surveillance imaging beyond 5 years after nephrectomy is unjustified.5 the costeffectiveness of surveillance for relapse is complex to evaluate and includes the balance between additional stress for families after treatment and the reassurance or relief of continuous surveillance proving that the child remains in complete remission . 
 pragmatically , a randomised trial that compares frequent monitoring with less frequent monitoring or ct scanning with ultrasound or chest xray for highrisk patients is unlikely to be prioritised over therapeutic interventions , despite being relatively cheap to do . 
even if the concept is adequately explained to families , parents might be reluctant to consent to their child being enrolled in the experimental group of a trial that prescribes less intensive surveillance . 
finally , this area is not regarded as a research vol 19 august 2018 1079 articles priority and will probably not receive sufficient financing because the focus of research in this field is on novel agents in relapse settings . despite the gap in evidence , patients should not be precluded from monitoring and surveillance and such practices should be standard practice in children after treatment for cancer . 
additionally , the purpose of follow up is multifactorial , including social and emotional aspects , rehabilitation , physical examination , and moni toring and management of late treatmentrelated adverse effects . 
surveillance beyond 2 years post treatment could be considered , but the overall number of abdominal ultrasounds and chest xrays needed to capture one asymptomatic relapse is substantial so extended surveillance might not be costeffective . contributors all authors contributed to the conception and design of this study . 
all authors approved the final version of the manuscript . declaration of interests we declare no competing interests . acknowledgments we thank all patients and their families who were enrolled in the siop 2001 wilms tumour study , and the researchers and clinicians who provided data . 
funding was received from great ormond street hospital childrens charity , the european expert paediatric oncology reference network for diagnostics and treatment , cancer research uk ( grants c1188 / a8687 ; c1188 / a11859 ) , the uk national cancer research network and childrens cancer and leukaemia group , socit franaise des cancers de lenfant and association leon berard enfant cancreux and enfant et sant , gesellschaft fur pdiatrische onkologie und hmatologie and deutsche krebshilfe ( grant 502709gr2 ) , grupo cooperativo brasileiro para o tratamento do tumor de wilms and sociedade brasileira de oncologia peditrica , the spanish society of pediatric haematology and oncology and the spanish association against cancer , and siopnetherlands . 
the cancer research uk clinical trials unit at university of birmingham supported the uk data contribution . for more on the prosper trial see org / record / 157683 / abstract for more on the spartan trial see n engl j med 2018 ; published online feb 8 . 
depending on the stage of disease at diagnosis , prostate cancer can be managed with combinations of active surveillance , surgery , radiotherapy , and androgendeprivation therapy ( adt )  . 
however , some men have aggressive disease , in which rising concentrations of prostate - specific antigen ( psa ) herald biochemical relapse and metastatic disease , even after treatment . 
currently , is available for these men ; no standard treatment however , promising new data from two trials presented at the 2018 asco genitourinary cancers symposium ( feb 810 , 2018 , san francisco , ca , usa ) suggest that this situation might be about to change . 
 the two trials prosper and spartan both treated men with early - stage , castration - resistant m0 disease who were unsuitable for curative treatment , and who were being treated with adt , but continued to have rapidly increasing psa concentrations . 
in spartan , men receiving apalutamide had a median mfs of 405 months compared with 162 months for those receiving placebo ( hazard ratio [ hr ] 028 ; 95% ci 023035 ; p < 0001 )  . 
similarly , in prosper , men receiving enzalutamide had a median mfs of 366 months compared with 147 months with placebo ( hr 029 ; 95% ci 024035 )  . 
apalutamide was subsequently approved by the us food and drug administration on feb 14 , 2018 , under priority review for non - metastatic , castration - resistant prostate cancer on the basis of spartans findingsthe first drug to be approved for this patient population . 
for example , in 20 - year follow - up data from the pivot trial for men diagnosed localised prostate cancer , no significant with early difference was found in either all - cause or prostatecancer specific mortality when comparing men treated with either surgery or observation alone , but men in the surgery group had worse functional outcomes from surgery ( eg , incontinence , erectile dysfunction ) for up to 5 years after treatment . 
 given these outcomes , the impetus for early detection and thus early management of prostate cancer important , making recent news of faster prostate cancer diagnosis in the uk welcome . 
diagnosis in the uk typically requires multiple hospital visits to obtain scans and biopsies ; however , three london hospitals are trialling whether or not patients can be diagnosed within a day . 
 this faster approach hinges on the use of multiparametric mri scans instead of transrectal ultrasound - guided biopsy , allowing all diagnoses to be done through imaging , which is both faster and non - invasive . 
about 5000 men will be tested for prostate cancer at these hospitals over the next 2 years , before a decision can be made as to whether the new system should be rolled out nationally . 
second , it is important to be aware that despite such advances as increased time to distant metastases , the endpoint used in the latest trials do not necessarily also indicate increased survival . 
 for example , in spartan the median time to overall survivala prespecified , albeit unpowered endpointdid not differ significantly between the groups ; comparable data are still awaited for prosper . 
 the lancet oncology vol 19 april 2018 editorial published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections corrections correction to lancet oncol 2015 ; 16 : 303 correction to lancet oncol 2016 ; 17 : 65 correction to lancet oncol 2016 ; 17 : e8 penson rt , huang hq , wenzel lb , et al . 
lancet oncol 2015 ; 16 : 30111in the 6 months post - cycle 1 section of table 1 of this article , in the received row of the second column ( headed cisplatin and paclitaxel plus bevacizumab ) , the data should have been 66 ( 57% )  . 
 bendamustine plus rituximab versus udarabine plus rituximab for patients with relapsed indolent and mantle - cell lymphomas : a multicentre , randomised , open - label , non - inferiority phase 3 trial . 
 lancet oncol 2016 ; 17 : 5766in this article , on page 65 , paragraph 6 , of the discussion section , reference 3 was incorrectly added to the sentence results of our published study8 in the rst - line setting . 
lancet oncol 2016 ; 17 : e8in paragraph two of this news piece , the percentage of genetic mutations in paediatric should have read 95 ( 85% ) of 1120 patients had genetic mutations in their normal tissue that increased their risk of developing cancer during childhood . 
 this correction has been made to the online version as of dec 22 , 2015 . vol 17 january 2016 the burden of cancers and their variations across the states of india : the global burden of disease study 19902016 india state - level disease burden initiative cancer collaborators * summary background previous efforts to report estimates of cancer incidence and mortality in india and its different parts include the national cancer registry programme reports , sample registration system cause of death findings , cancer incidence in five continents series , and globocan . 
we present a comprehensive picture of the patterns and time trends of the burden of total cancer and specific cancer types in each state of india estimated as part of the global burden of diseases , injuries , and risk factors study ( gbd ) 2016 because such a systematic compilation is not readily available . methods we used all accessible data from multiple sources , including 42 population - based cancer registries and the nationwide sample registration system of india , to estimate the incidence of 28 types of cancer in every state of india from 1990 to 2016 and the deaths and disability - adjusted life - years ( dalys ) caused by them , as part of gbd 2016 . 
 we present incidence , dalys , and death rates for all cancers together , and the trends of all types of cancers , highlighting the heterogeneity in the burden of specific types of cancers across the states of india . 
we also present the contribution of major risk factors to cancer dalys in india . findings 83% ( 95% uncertainty interval [ ui ] 7986 ) of the total deaths and 50% ( 4655 ) of the total dalys in india in 2016 were due to cancer , which was double the contribution of cancer in 1990 . 
the ten cancers responsible for the highest proportion of cancer dalys in india in 2016 were stomach ( 90% of the total cancer dalys ) , breast ( 82% ) , lung ( 75% ) , lip and oral cavity ( 72% ) , pharynx other than nasopharynx ( 68% ) , colon and rectum ( 58% ) , leukaemia ( 52% ) , cervical ( 52% ) , oesophageal ( 43% ) , and brain and nervous system ( 35% ) cancer . 
among these cancers , the age - standardised incidence rate of breast cancer increased significantly by 407% ( 95% ui 70856 ) from 1990 to 2016 , whereas it decreased for stomach ( 397% ; 343440 ) , lip and oral cavity ( 64% ; 04186 ) , cervical ( 397% ; 265573 ) , and oesophageal cancer ( 312% ; 279349 ) , and leukaemia ( 161% ; 43242 )  . 
we found substantial inter - state heterogeneity in the age - standardised incidence rate of the different types of cancers in 2016 , with a 33 times to 116 times variation for the four most frequent cancers ( lip and oral , breast , lung , and stomach )  . 
tobacco use was the leading risk factor for cancers in india to which the highest proportion ( 109% ) of cancer dalys could be attributed in 2016 . lancet oncol 2018 ; 19 : 1289306 published online september 12 , 2018 s1470 - 2045 ( 18 ) 30447 - 9 see comment page 1260 see online / comment lancet 2018 ; published online sept 12 . 
 s2214 - 109x ( 18 ) 30387 - 5 , s2214 - 109x ( 18 ) 30407 - 8 , and s2214 - 109x ( 18 ) 30409 - 1 see online / articles lancet public health 2018 ; published online sept 12 . 
 s2468 - 2667 ( 18 ) 30138 - 5 * collaborators listed at the end of the article correspondence to : prof lalit dandona , public health foundation of india , gurugram 122002 , national capital region , india lalit.dandona@phfi.org interpretation the substantial heterogeneity in the state - level incidence rate and health loss trends of the different types of cancer in india over this 26 - year period should be taken into account to strengthen infrastructure and human resources for cancer prevention and control at both the national and state levels . 
these efforts should focus on the ten cancers contributing the highest dalys in india , including cancers of the stomach , lung , pharynx other than nasopharynx , colon and rectum , leukaemia , oesophageal , and brain and nervous system , in addition to breast , lip and oral cavity , and cervical cancer , which are currently the focus of screening and early detection programmes . funding bill & melinda gates foundation ; and indian council of medical research , department of health research , ministry of health and family welfare , government of india . copyright the author ( s )  . 
we found a wide variety of valuable data for cancer distribution in india and several states , but no studies that comprehensively described incidence , prevalence , mortality , and disability - adjusted life - years ( dalys ) for all cancer types in every state of india over a long period of time . added value of this study to our knowledge , this is the first report to produce comprehensive estimates of incidence , prevalence , mortality , and dalys for 28 types of cancers in every state of india over 26 years from 1990 to 2016 . 
this analysis was part of the global burden of diseases , injuries , and risk factors study 2016 that assessed all causes of disease burden , using data from all accessible sources . 
this study estimates that while the agestandardised incidence rate of all cancers considered together has not changed substantially in india during this 26 - year period , the proportion of total disease burden caused by cancers has doubled . 
this study reports the substantial heterogeneity in the incidence , mortality , and dalys of different cancers across the states of india and documents that tobacco use is the highest contributing risk to cancer burden in india . implications of all the available evidence this systematic and comprehensive description of the variations in the distribution and trends of cancer types in different parts of the country can serve as a useful reference for further planning of prevention and management of cancer across india . 
more large - scale collaborative research is needed to understand the reasons behind the changing trends of the different types of cancers in india . types of cancers in each state of india is not readily available . 
this is needed to inform action for cancer control that is commensurate with the need in each state , since delivery of health care is a state subject in india . the united nations sustainable development goals target the reduction of premature mortality from non - communicable diseases , which includes cancer , by one - third by 2030 through prevention and treatment.21 the national cancer registry programme in india was established in 1981 to generate data on the magnitude and patterns of cancer through population - based registries.22 , 23 the number of registries has grown under this programme , and other population - based registries have also been started in recent years.22 however , many populous states have no cancer registries yet , and most registries in india are in urban areas , leading to difficulties in assessing population - level cancer burden trends in all parts of the country . the india state - level disease burden initiative is a collaboration with the global burden of diseases , injuries , and risk factors study ( gbd ) to produce subnational disease burden estimates for india . 
this initiative recently reported the variable health transition across the states of india from 1990 to 2016 based on analysis done as part of gbd 2016.4 , 24 here , we report detailed trends of the incidence and health loss due to each type of cancer in every state of india from 1990 to 2016 . methods overview the india state - level disease burden initiative recently reported the overall trends of diseases , injuries , and risk factors from 1990 to 2016 for every state of india.4 , 24 this analysis was done as part of gbd 2016 , which estimated disease burden due to 333 diseases and injuries and 84 risk factors in all age groups using all accessible data from multiple sources . 
the india state - level disease burden initiative was supported by the efforts of several expert groups and a vast network of collaborators to identify and access all available data sources , assess their scope and quality for inclusion , and participate in the analysis and interpretation of the findings . 
the health ministry screening committee at the indian council of medical research and the ethics committee of the public health foundation of india approved the work of this initiative . estimation of cancer burden a detailed description of methods to estimate cancer mortality , incidence , prevalence , and disability - adjusted life - years ( dalys ) , and the analytical approaches used in gbd 2016 have been reported elsewhere , and are summarised in the appendix ( pp 316 ) .1 , 2529 briefly , the major data inputs to determine cancer mortality in india included the nationwide sample registration system ( srs ) cause of death data , the medically certified cause of death data , and 42 population - based cancer registries ( appendix pp 68 )  . 
srs verbal autopsy cause of death data on 455 460 deaths covering the rural and urban populations of every state of india from 2004 to 2013 were included.4 for states with at least one population - based cancer registry , the incidence data were trans formed to mortality by multiplying incidence data with an independently modelled urban or rural mortality - incidence ( mi ) ratio for the respective states . 
 cancer registry data were used as the gold - standard against which other data sources ( srs or medically see online for appendix 1290 vol 19 october 2018 articles substantially sources differed certified cause of death data ) were compared . 
if the from other data the registry data , they were excluded.1 , 30 because of limitations associated with the medically certified cause of death mortality data , these were used only when the cancer type was not captured by the srs cause of death data . 
 the codcorrect algorithm was used to adjust cancer subtypes to the parent cause and to adjust the sum of predicted deaths from these models for each type of cancers in an agesexstateyear group to be consistent with the results from all - cause mortality estimation . the estimation of cancer incidence was driven by registry data from india . 
the mortality estimates that were derived from transformation of incidence data using the mi ratios , as noted above , were transformed back to incidence after the codem and codcorrect model adjustments.1 10 - year cancer prevalence was estimated by modelling survival using the mi ratio as a surrogate for access to cancer care . 
lifetime prevalence was only estimated for 10 years post incidence1 and for long - term sequelae from procedures ( mastectomy , laryngectomy , stoma , incontinence cystectomy , and prostatectomy )  . 
dalys , a summary measure of total health loss , were computed by adding ylls and ylds for each cancer type for location , year , age and sex.1 , 28 the appendix provides a list of data inputs used for these estimations ( pp 1729 )  . a description of estimation of risk factor exposure and its contribution to disease burden in gbd is available elsewhere.29 briefly , this includes determination of risk exposure and disease outcome pairs based on available evidence and inclusion criteria , assessment of risk exposure from all accessible data sources , and estimation of disease burden attributable to risks based on published relative risks . 
estimates of dalys for specific types of cancers that were attributable to each risk factor were produced by location , age , sex , and year . gbd uses covariates , which are explanatory variables that have a known association with the outcome of interest , to arrive at the best possible estimate of the outcome of interest when data for the outcome are scarce but data for the covariates are available.2529 this approach was part of the estimation process for the findings presented in this report . analysis presented in this paper the findings are reported for 31 geographical units in india : 29 states , union territory of delhi , and the union territories other than delhi ( combining the six smaller union territories of andaman and nicobar islands , chandigarh , dadra and nagar haveli , daman and diu , lakshadweep , and puducherry )  . 
for trends from 1990 onwards , the data for these four new states were disaggregated from their parent states on the basis of data from the districts that now constitute these states . 
 the findings are also presented for four groups of states based on epidemiological transition level ( etl ) as described previously.4 briefly , the etl state groups were defined on the basis of the ratio of dalys from communicable , maternal , neonatal and nutritional diseases to those from non - communicable diseases and injuries combined in 2016 , with a relatively lower ratio indicating higher etl : level etl state group ( ratio 056075 ) , lower - middle etl state group ( 041055 ) , higher - middle etl state group ( 031040 ) , and high etl state group ( less than 031 )  . 
we have reported previously that epidemiological transition ratios of the states of india have a significant inverse relation with the socio - demographic index calculated by the gbd study and based on income , education , and fertility levels , which indicates broad correspondence of etl groups with sociodemographic development levels.4 low we present trends of incidence ( new cases in a year ) , mortality , and dalys due to all cancers together and different types of cancers from 1990 to 2016 for every state of india . 
we regarded dalys as the main metric for disease burden because it includes both mortality and morbidity and is recommended by the national health policy of india for tracking disease burden.31 first , we present the 1990 to 2016 trends for the overall burden from all cancers together in terms of dalys , followed by incidence and deaths . 
we also describe briefly another six cancer types that are among the ten leading incident cancers in females or males in india in 2016 , which are not included in the previous ten cancers causing the highest dalys . 
 we present both crude and age - standardised rates , since crude rates provide the actual situation in each state that vol 19 october 2018 1291 articles 1990 jammu and kashmir ( 691 ) punjab ( 580 ) haryana ( 710 ) himachal pradesh ( 698 ) uttarakhand ( 693 ) delhi ( 646 ) sikkim ( 678 ) arunachal pradesh ( 759 ) rajasthan ( 588 ) uttar pradesh ( 720 ) bihar ( 449 ) assam ( 687 ) nagaland ( 631 ) manipur ( 481 ) mizoram ( 891 ) jharkhand ( 580 ) odisha ( 686 ) meghalaya ( 690 ) tripura ( 529 ) west bengal ( 639 ) chhattisgarh ( 588 ) incidence rate per 100 000 105 901049 75899 60749 45599 449 himachal pradesh ( 916 ) uttarakhand ( 910 ) delhi ( 1029 ) sikkim ( 744 ) arunachal pradesh ( 785 ) rajasthan ( 726 ) uttar pradesh ( 790 ) bihar ( 539 ) assam ( 902 ) nagaland ( 703 ) manipur ( 643 ) mizoram ( 1217 ) jharkhand ( 643 ) odisha ( 836 ) meghalaya ( 814 ) tripura ( 690 ) west bengal ( 854 ) chhattisgarh ( 820 ) gujarat ( 555 ) madhya pradesh ( 694 ) maharashtra ( 620 ) karnataka ( 762 ) telangana ( 549 ) andhra pradesh ( 581 ) ( 525 ) tamil nadu ( 589 ) kerala ( 741 ) 2016 punjab ( 855 ) haryana ( 1033 ) jammu and kashmir ( 792 ) gujarat ( 758 ) madhya pradesh ( 831 ) maharashtra ( 802 ) telangana ( 726 ) andhra pradesh ( 766 ) goa ( 970 ) karnataka ( 1016 ) tamil nadu ( 829 ) kerala ( 1353 ) is preferred by policy makers , and age - standardised rates allow comparisons over time and between states after adjusting for the differences in the age structure of the population . 
 these were based on 1000 runs of the models for each quantity of interest , with the mean considered as the point estimate and the 25th and 975th percentiles considered as the 95% ui ( appendix p 15 ) .2528 role of the funding source some staff of the indian council of medical research are co - authors on this paper as they contributed to various aspects of the study and analysis . 
 the corresponding author had full access to all of the data in the study and had final responsibility for the decision to submit for publication . results all cancers together contributed 50% ( 95% ui 4655 ) of the total dalys and 83% ( 7986 ) of the total deaths in india in 2016 , an increase of 909% and 1128% respectively from 1990 . 
the crude cancer daly rate in india increased by 253% ( 168342 ) from 1990 to 2016 , but the age - standardised cancer daly rate did not change substantially during the same period.32 the agestandardised cancer daly rate had a 26 times variation across the states of india in 2016 ( appendix p 30 )  . 
the highest crude cancer daly rates in 2016 were in the states of mizoram , kerala , assam , haryana , and meghalaya , and the highest age - standardised rates were in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam ( appendix p 30 )  . to 1 069 000 ( 1 043 0001 101 000 ) the estimated number of incident cancer cases in india increased from 548 000 ( 95% ui 520 000576 000 ) in 1990 in 2016 ( appendix p 31 )  . 
the crude cancer incidence rate in india increased by 282% ( 95% ui 199355 ) from 634 per 100 000 in 1990 to 812 per 100 000 in 2016 , but there was no change in the age - standardised incidence rate ( appendix p 32 )  . 
crude cancer incidence rate was highest in kerala and mizoram , followed by haryana , delhi , karnataka , goa , himachal pradesh , uttarakhand , and assam ( figure 1 , appendix p 30 )  . 
age - standardised incidence rates were highest in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam , figure 1 : crude annual incidence rate of all cancers together in the states of india , 1990 and 2016 the states of chhattisgarh , jharkhand , telangana , and uttarakhand did not exist in 1990 , as they were created from existing larger states in 2000 or later . 
crude cancer incidence rate increased substantially from 1990 to 2016 in all etl state groups , with the highest increase in the high etl group ( appendix p 32 )  . the number of deaths due to cancer in india increased from 382 000 ( 95% ui 351 000412 000 ) in 1990 to 813 000 ( 767 000850 000 ) in 2016 ( appendix p 31 )  . 
the crude cancer death rate in india in 2016 was 618 ( 95% ui 583646 ) per 100 000 , as compared with 442 ( 406477 ) in 1990 ( appendix p 32 )  . 
male cancer patients had a 123% ( 95% ui 29233 ) increase in agestandardised death rate over the 26 - year time period , whereas no substantial changes over time were found in female cancer patients ( appendix p 32 )  . 
the crude death rate for both sexes combined was highest in mizoram , kerala , and haryana in 2016 , followed by assam , karnataka , odisha , uttarakhand , meghalaya , and himachal pradesh ( appendix pp 30 , 33 )  . 
the agestandardised death rates were highest in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam ( appendix p 30 )  . the crude cancer mi ratio in india in 2016 was 076 ( 95% ui 072079 )  . 
the mi ratio was higher in low and lower - middle etl state groups than the high and higher - middle etl groups in 2016 ( figure 2 )  . 
the mi ratio for males was more than 080 in all states from the low etl group and most of the lower - middle etl states , with a higher ratio in odisha in low etl , and mizoram and arunachal pradesh in the lower - middle etl state group in 2016 . 
the mi ratio was below 080 for females in most of the states in india in 2016 , except for bihar and meghalaya . the leading types of cancer in india in 2016 , those responsible for more than 5% of the total cancer dalys among both sexes combined , were stomach cancer ( 90% ) , breast cancer ( 82% ) , lung cancer ( 75% ) , lip and oral cavity cancer ( 72% ) , pharynx cancer other than nasopharynx ( 68% ) , colon and rectum cancer ( 58% ) , leukaemia ( 52% ) , and cervical cancer ( 52% ; figure 3 )  . 
the age - standardised daly rate increased significantly in india from 1990 to 2016 for liver cancer ( 512% ; 95% ui 240659 ) , non - hodgkin lymphoma ( 354% ; 207488 ) , ovarian cancer ( 281% ; 151443 ) and myeloma ( 282% ; 56631 )  . 
 age - standardised daly rates from 1990 to 2016 was highest for testicular cancer ( 592% ; 538654 ) and hodgkins lymphoma ( 548% ; 396625 ) , followed by cervical ( 387% ; 230563 ) , nasopharynx ( 335% ; 198461 ) , larynx ( 316% ; 257367 ) , uterine ( 315% ; 178400 ) , and stomach cancer ( 314% ; 237373 )  . 
the highest cancer dalys among males in india in 2016 were due to lung cancer , followed by lip and oral cavity cancer , other pharynx cancer , and stomach cancer ( figure 3 )  . among both boys and girls aged 014 years , leukaemia was responsible for the highest dalys in india in 2016 , followed by brain and nervous system cancer ( figure 5 , appendix pp 3440 )  . 
daly rates for lung cancer and stomach cancer increased in males after the age of 35 years in 2016 , while prostate cancer increased after the age of 50 years . tobacco use , alcohol use , and dietary risks were estimated by gbd to contribute the highest cancer dalys in 2016 ; they were responsible for 109% , 66% and 60% of the total cancer dalys , respectively ( appendix pp 4142 )  . stomach cancer the estimated number of incident stomach cancer cases in india in 2016 was 75 000 ( 95% ui 73 00078 000 ) and the prevalent cases were 112 000 ( 109 000116 000 ; appendix p 31 )  . 
there was a substantial reduction in the age - standardised incidence rate of stomach cancer ( 397% ; 95% ui 343440 ) from 1990 to 2016 in india ( figure 6 )  . 
in 2016 , stomach cancer was the first or second highest cause of cancer deaths in 15 states for females and in 18 states for males ( figure 8 )  . 
only a small proportion of the stomach cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( dietary risks [ 41% ] and smoking [ 35% ] ; appendix pp 4142 )  . breast cancer the estimated number of incident breast cancer cases in india in 2016 was 118 000 ( 95% ui 107 000130 000 ) , 981% of which were in females , and the prevalent cases were 526 000 ( 474 000574 000 ; appendix p 31 )  . 
breast cancer is the leading cancer in indian females , accounting for the largest crude incidence rate and prevalence of any cancer type ( appendix pp 49 , 50 )  . 
over the 26 - year period , the agestandardised incidence rate of breast cancer in females increased by 391% ( 95% ui 51855 ) from 1990 to 2016 , with increase observed in every state of the country ( appendix pp 51 )  . 
the highest crude daly rates for breast cancer were in kerala , punjab , and tamil nadu in the high etl state group , followed by delhi , maharashtra , karnataka , and haryana in the higher - middle etl group . 
only a small proportion of breast cancer dalys in india in 2016 could be attributed to risk factors included [ 49% ] and in gbd ( high fasting plasma glucose secondhand smoke [ 24% ] ; appendix pp 4142 )  . lung cancer we refer to tracheal , bronchus , and lung cancer as lung cancer in this report for simplicity . 
the number of vol 19 october 2018 1295 articles a females b males 8000 7000 6000 5000 4000 3000 2000 1000 8000 7000 6000 5000 4000 3000 2000 1000 bladder cancer brain and nervous system cancer breast cancer cervical cancer colon and rectum cancer gallbladder and biliary tract cancer hodgkins lymphoma kidney cancer larynx cancer leukaemia lip and oral cavity cancer liver cancer lung cancer malignant skin melanoma mesothelioma multiple myeloma nasopharynx cancer non - hodgkin lymphoma non - melanoma skin cancer oesophageal cancer pharynx cancer other than nasopharynx ovarian cancer pancreatic cancer stomach cancer thyroid cancer uterine cancer bladder cancer brain and nervous system cancer breast cancer colon and rectum cancer gallbladder and biliary tract cancer hodgkins lymphoma kidney cancer larynx cancer leukaemia lip and oral cavity cancer liver cancer lung cancer malignant skin melanoma mesothelioma multiple myeloma nasopharynx cancer non - hodgkin lymphoma non - melanoma skin cancer oesophageal cancer pharynx cancer other than nasopharynx pancreatic cancer prostate cancer stomach cancer testicular cancer thyroid cancer 1014 1519 2024 2529 3034 3539 4044 4549 5054 5559 6064 6569 7074 7579 age range ( years ) figure 5 : age - specific dalys for different types of cancers by sex in india , 2016 dalys = disability - adjusted life - years . incident lung cancer cases in india in 2016 was 67 000 ( 95% ui 63 00072 000 ) , 722% of which were in males , and the prevalent cases were 74 000 ( 70 00080 000 ; appendix p 31 )  . 
the crude lung cancer incidence rate in males was highest in kerala and mizoram , and in females was highest in mizoram and manipur ( appendix pp 49 , 50 )  . 
there was a substantial reduction in the age - standardised incidence rate of lip and oral cavity cancer ( 64% ; 95% ui 04186 ) from 1990 to 2016 in india ( figure 6 )  . 
the age - standardised incidence rate for lip and oral cavity cancer varied 51 times among both sexes combined across the states of india in 2016 ( appendix pp 4348 )  . 
smokeless tobacco , alcohol use and smoking were the leading risk factors in gbd for lip and oral cavity cancer in india in 2016 to which 332% , 298% , and 209% of the lip and oral cavity cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . pharynx cancer other than nasopharynx the number of incident pharynx cancer other than nasopharynx cases in india in 2016 was 65 000 ( 95% ui 58 00070 000 ) , 702% of which were in males , and the prevalent cases were 152 000 ( 137 000163 000 ; appendix p 31 )  . 
the age - standardised incidence rate for other pharynx cancer varied 98 times for both sexes combined across the states of india in 2016 ( appendix pp 4348 )  . 
alcohol use was the leading risk factor in gbd for other pharynx cancer in india in 2016 to which 30.1% of the other pharynx cancer dalys could be attributed ( appendix pp 41 , 42 )  . colon and rectum cancer the number of incident colon and rectum cancer cases in india in 2016 was 63 000 ( 95% ui 58 00066 000 ) and the prevalent cases were 185 000 ( 171 000195 000 ; appendix p 31 )  . 
colon and rectum cancer incidence rate in both sexes was higher in the high etl as compared with other etl state groups ( appendix pp 49 , 50 )  . 
dietary risks were the leading risk factor in gbd for colon and rectum cancer in india in 2016 to which 432% of the colon and rectum cancer dalys could be attributed ( appendix pp 41 , 42 )  . leukaemia the number of incident leukaemia cancer cases in india in 2016 was 34 000 ( 95% ui 30 00038 000 ) and the prevalent cases were 105 000 ( 96 000120 000 ; appendix p 31 )  . 
among children aged 014 years , leukaemia was responsible for the highest proportion of the cancer dalys ( 346% ) in india in 2016 , which was similar among boys and girls ( figure 5 , appendix pp 3440 )  . 
in males , leukaemia was the third and fifth leading cause of cancer deaths in delhi and punjab respectively in 2016 , but lower in other states ( figure 8 )  . cervical cancer cervical cancer was the second most common cancer in females in india in 2016 , with 77 000 ( 95% ui 68 00096 000 ) incident cervical cancer cases in india in 2016 and 288 000 ( 247 000342 000 ) prevalent cases ( appendix p 31 )  . 
it is important to note that other unknown risk factors could also be contributing to cervical cancer as the population - attributable fractions of different risks can add up to more than 100% . vol 19 october 2018 1299 articles for rate cancer oesophageal oesophageal cancer the number of incident oesophageal cancer cases in india in 2016 was 37 000 ( 95% ui 36 00038 000 ) , 608% of which were in males , and the prevalent cases were 41 000 ( 39 00042 000 ) ( appendix p 31 )  . 
there was a substantial reduction in the age - standardised incidence rate of oesophageal cancer ( 312% ; 95% ui 279349 ) in india from 1990 to 2016 ( figure 6 )  . 
smokeless tobacco , dietary risks , and smoking were the leading risk factors in gbd for oesophageal cancer in india in 2016 to which 226% , 215% , and 174% of the oesophageal cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . brain and nervous system cancer the number of incident brain and nervous system cancer cases in india in 2016 was 23 000 ( 95% ui 21 00028 000 ) and the prevalent cases were 49 000 ( 44 00057 000 ; appendix p 31 )  . 
among children aged 014 years , brain and nervous system cancer was responsible for the second highest proportion of the cancer dalys ( 16% ) in india in 2016 , which was similar among boys and girls ( figure 5 , appendix pp 3440 )  . 
the daly rate for brain and nervous system cancer was highest in delhi followed by sikki the ranking of deaths due to brain and nervous system cancer was relatively low in all states as compared with the other high burden cancers ( figure 8 )  . 
 prostate cancer prostate cancer had the fifth highest incidence rate among males in india in 2016 ( 48 per 100 000 , 95% ui 3858 ) , with 33 000 ( 26 00040 000 ) incident cases and 112 000 ( 87 000137 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
there were 31 000 ( 95% ui 30 00033 000 ) incident cases in india , of which 835% were in males , and there were 96 000 ( 93 000100 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
the crude incidence rate for larynx cancer in males was highest in kerala in 2016 , followed by delhi , haryana , and assam ( appendix p 50 )  . 
smoking and alcohol use were the leading risk factors in gbd for larynx cancer in india in 2016 to which 379% and 172% of the larynx cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . liver cancer liver cancer had the ninth highest incidence rate among males in 2016 in india ( 31 per 100 000 , 95% ui 29 32 )  . 
 there were 30 000 ( 95% ui 29 00032 000 ) incident cases in india , of which 689% were in males , and 12 000 ( 11 00014 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
the crude incidence rate for liver cancer in males in 2016 was highest in arunachal pradesh , followed by kerala , sikkim , and mizoram ( appendix p 50 )  . 
 to 2016 the sixth highest ovarian cancer ovarian cancer had incidence rate among females in 2016 in india ( 40 per 100 000 , 95% ui 3743 ) , with 26 000 ( 95% ui 24 00027 000 ) incident cases and 76 000 ( 69 00080 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
only a small proportion of the ovarian cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( high fasting plasma glucose [ 55% ] ; appendix pp 41 , 42 )  . gallbladder and biliary tract cancer gallbladder and biliary tract cancer had the ninth highest incidence rate among females in 2016 in india ( 26 per 100 000 , 95% ui 2328 )  . 
there were 26 000 ( 95% ui 23 00029 000 ) incident cases in india , of which 644% were in females , and there were 21 000 ( 18 00023 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
the crude incidence of gallbladder and biliary tract cancer in females 1300 vol 19 october 2018 articles was highest in the states of assam and delhi in 2016 ( appendix p 49 )  . 
91% of the gallbladder and biliary tract cancer dalys in india in 2016 could be attributed to high body - mass index in gbd ( appendix pp 41 , 42 )  . thyroid cancer thyroid cancer had the tenth highest incidence rate among females in 2016 in india ( 25 per 100 000 , 95% ui 2326 )  . 
there were 21 000 ( 95% ui 20 00023 000 ) incident cases in india , of which 743% were in females , and there were 106 000 ( 101 000115 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
the crude incidence rate of thyroid cancer was highest in females in kerala , followed by sikkim , nagaland , and goa in 2016 ( appendix p 49 )  . 
 only a small proportion of the thyroid cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( high body - mass index [ 51% ] ; appendix pp 41 , 42 )  . discussion the number of new cases and deaths due to cancer doubled in india from 1990 to 2016 , as did the proportional contribution of cancers to the total dalys and deaths in the country . 
however , there was no change in the age - standardised rates for both sexes combined , highlighting the contribution of ageing and population growth to the increasing cancer burden of the country . 
 males had higher mi ratios than females in every state of the country . the trends observed in sex - specific and cancer typespecific incidence rates over time in india are likely due to a variety of factors , such as population ageing , changes in cancer literacy , detection , health - care access , and a variety of risk factors . 
the substantial decrease in the age - standardised incidence rate of stomach cancer across the country might be due to lifestyle changes such as reduced consumption of salt - preserved foods , better availability of refrigeration , and increasing fruit con sumption , and to decreases in smoking prevalence.3234 the prevalence of helicobacter pylori remains persistently high in indians , 35 and hence this is an unlikely factor in the decreasing incidence of stomach cancer . 
for breast cancer , a substantial increase in age - standardised incidence rate is consistent with changes in some risk factors over time in india , such as later age at first birth , lower parity , and increase in overweight and obesity.32 , 36 , 37 the substantial decrease in the age - standardised incidence rate of oesophageal cancer might be partly due to the decrease in smoking prevalence over the 26 - year period and in smokeless tobacco use over the past 10 years.32 , 34 the absence of change in the age - standardised incidence rate of lung cancer in india might be related to the mixed trends of its major risk factors , which include decrease in smoking and household air pollution but an increase in ambient air pollution , but also due to the patterns of other unknown risk factors.32 , 34 the small decrease in the age - standardised incidence rate of lip and oral cavity cancer in india could be related to the reduction in use of smokeless tobacco in india during the past decade.32 the decreasing age - standardised incidence rate of cervical cancer could be inversely related to the reproductive risk factors mentioned for breast cancer increase above.36 in the absence of systematic human papilloma virus ( hpv ) testing in india , there is no evidence of changing seroprevalence of hpv and its subtypes over time in india . 
leukaemia has been associated with genetic , infectious , and environmental risks , 38 but the reasons for the substantial reduction in its age - standardised incidence rate in india from 1990 to 2016 are unclear . the interplay of the trends of the two risk factors to which the highest proportion of cancer dalys in india could be attributed , tobacco and alcohol , is interesting in relation to the trends of some of the leading cancers . 
while tobacco use in india has decreased during this period , alcohol use has increased.32 the drop in incidence rate of lip and oral cavity , oesophageal , and larynx cancers could be partly related to a larger influence of tobacco than alcohol on these cancers , and the increase in incidence rate of liver cancer could be partly related to a larger influence of alcohol than tobacco on this cancer , in addition to the trends of yet unknown other risk factors contributing to all of these cancers . 
collaborative multi - institutional research efforts on cancer risk factors can help address such knowledge gaps , as well as lead to a better understanding of the reasons for the substantial decreases or increases in the incidence of different types of cancers in different parts of india . 
detailed decomposition analyses are needed to tease apart the contribution of population structure changes , risk factors , interventions , and other determinants to the trends of leading cancers in india . the heterogeneity of the incidence rate of different types of cancers across india is vast . 
major variations exist even within the same geographical region , such as neighbouring states in the northeastfor example , a 15 times difference in age - standardised incidence rates of naso pharynx cancer between the neighbouring north - eastern states of nagaland and tripura . 
the states in the northeast of vol 19 october 2018 1301 articles india generally have high tobacco use as well as a high incidence of lung , oesophageal , nasopharynx and other pharynx cancers that are associated with tobacco use . 
 there are also unique tobacco consumption patterns in these states , such as use of tobacco - infused water in mizoram.39 , 40 hpv and cervical cancer are both high in dindigul in tamil nadu , 41 consumption of smoked or preserved meats and stomach cancer are high in mizoram , 42 and delayed childbearing and lower parity are high in kerala as is breast cancer.43 the many variations between the states indicate the need for state - specific approaches for cancer control . 
if the reasons for the heterogeneous distribution of the major cancer types in different parts of india are understood better through large - scale collaborative research , this knowledge could help plan more specific efforts to reduce the cancer burden across the states of india . the national cancer control programme was initiated by the government of india in 1975 to equip tertiary care cancer hospitals and institutions to implement systematic , equitable , and evidence - based strategies for prevention , early detection , diagnosis , treatment , and palliation , using available resources.44 state cancer institutes and tertiary care cancer centres have been established under this programme that are responsible for improved cancer awareness and management at the state level.45 despite these attempts , access to critical cancer treatment is low in the country . 
for example , availability of radiotherapy machines is poor , there are delays in treatment , and there is geographic inequity in the distribution of such resources.10 , 11 , 46 with the launch of the national programme for control of cancer , diabetes , cvd and stroke in 2010 in india , the cancer control efforts are now part of this umbrella programme for noncommunicable diseases.47 the national programme aims to tackle cancer by addressing preventable common risk factors through community - level , cost - effective screening for high - burden cancers , which include clinical breast examination for breast cancer , visual inspection with acetic acid for cervical cancer and visual examination for oral cancers.14 however , there are many challenges with these efforts , including difficulties with trained human resources , follow - up of positive tests , timely diagnosis , and well - tracked referral pathways.48 additionally , there are limited population - level screening modalities available for some of the cancers responsible for the highest cancer burden in india , such as stomach and lung cancers . 
for secondary prevention , less invasive tests for h pylori may offer cost - effective first - line tests for referrals to more invasive endoscopic tests for early detection of stomach cancer.49 faecal occult blood testing as a non - invasive , cost - effective approach to screen for colorectal cancer should also be considered.50 ideally , national and state - level efforts should coordinate to facilitate the development of a prevention - to - palliation system of upward referral for early confirmatory diagnosis and prompt treatment of cancers , and downward referral for adequate follow - up , including palliative care and pain relief . 
india pioneered the establishment and expansion of the national cancer registry programme ( ncrp ) under the indian council of medical research through a network of cancer registries during the past 30 years , which now covers 23 states and union territories.23 the gbd methods rely substantially on the ncrp data from india , but they also use data from all accessible data sources , including some registries that are not part of the ncrp , cause of death data from the 1302 vol 19 october 2018 articles srs and other sources , and a variety of covariates to arrive at the best possible estimates for states where registries do not exist . 
accordingly , differences are expected between the gbd estimates and the statistics reported by the ncrp , which are based entirely on population - based registries.23 the objectives and advantages of the gbd and ncrp approaches are complementary . 
while the ncrp adheres to a standardised methodology established by whos international agency for research in cancer , the gbd methodology provides a standardised approach that also incorporates other sources of data for estimations for all states of india , including those where registries do not exist such as the populous states of bihar , chhattisgarh , jharkhand , and uttar pradesh . 
the gbd methodology is integrated into a larger total disease framework estimation process that allows comparison of the cancer burden to that of other diseases , which has helped to highlight the increasing contribution of cancers to the disease burden in india over the past quarter century . 
it has also further highlighted the need to establish cancer registries in large states of north india where none exist , as well as adequate coverage of rural populations . the limitations of the findings in this report include the general limitations of the gbd approach that are described elsewhere.1 , 2528 input data used to generate cancer mortality can be biased in multiple ways.1 a high proportion of ill - defined cancer cases in the registry data or ill - defined causes of death in mortality data sources require redistribution of these cases , which can introduce bias . 
underreporting of cancers that require advanced diagnostic techniques ( eg , leukaemia , brain , pancreatic , and liver cancer ) can be an issue in data from areas where access to these technologies is scarce . 
in addition , risk factors for breast and cervical cancer that are related to reproductive history in women , such as age at first birth and parity , are not yet included in the gbd risk factor assessment . 
a specific limitation for india is an inadequate cause of death reporting as part of the vital registration system , which reports medically certified cause of death only for a small proportion of deaths in india so far , with variable coverage across the states . 
the srs provides cause of death data using verbal autopsy for all states in india , which is a reasonable alternative data source when the cause - specific data are not fully available from vital registration systems.4 however , this situation highlights the need to improve vital registration and improve training to code cause of death across india . 
the absence of population - based registries in major populous states of north india such as bihar and uttar pradesh leaves open questions about the magnitude of some cancers such as gallbladder cancer , which are expected by the india cancer community to be high there , but this cannot be substantiated yet because of the paucity of population - level evidence . 
in cancer datascarce locations , the estimates for the types of cancer were calculated using covariates , which are explanatory variables with a causal relation to cancer incidence and mortality.1 the strengths of the findings presented in this report were the use of standardised gbd methodology and inclusion of all accessible data from multiple sources , and the substantial contribution of a large network of cancer experts from india in the analysis and inter pretation of the findings . in conclusion , the detailed epidemiology of 28 types of cancer in every state of india over a quarter century described the substantial this report highlights variations between the states for the different types of cancer , and can serve as a useful reference for more targeted planning of cancer control that is commensurate with the trends of different cancers in each state of india . 
 the increasing overall contribution of cancer to disease burden in india should motivate more systematic and large - scale approaches to reduce this burden at the population level across the country . 
these efforts should include improved human resources and infrastructure for prevention , screening , treatment , and palliative care for cancers , as well as adequate financial protection for cancer care . 
these approaches should focus at least on the ten cancers that contribute the highest dalys in indiaie , stomach , breast , lung , lip and oral cavity , pharynx other than nasopharynx , colon and rectum , leukaemia , cervical , oesophageal , and brain and nervous system cancers . 
all authors agreed with the final version of the report . declaration of interests pma , an , rm , dks , rsd , tk , rnv , jkc , mc , pd , jm , sp , ksa , kv , and ss are or have been employees of the indian council of medical research , which partly funded this research . 
all other authors declare no competing interests . acknowledgments the research reported in this publication was funded by the bill & melinda gates foundation and the indian council of medical research , department of health research , government of india . 
 the content of this publication is solely the responsibility of the authors and does not necessarily represent the official views of the bill & melinda gates foundation or the government of india . 
 we gratefully acknowledge the ministry of health and family welfare of the government of india for its support and encouragement of the india state - level disease burden initiative , the governments of the states of india for their support of this work , the many institutions across india that contributed valuable data to the national cancer registry programme and to the other cancer registries , the valuable guidance of the advisory board of this initiative , and the large number of staff at the indian council of medical research , public health foundation of india and the institute for health metrics and evaluation for their contribution to various aspects of the work of this initiative . correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections articles screen detection of ductal carcinoma in situ and subsequent incidence of invasive interval breast cancers : a retrospective population - based study stephen w du y , amanda dibden , dimitrios michalopoulos , judith o man , dharmishta parmar , jacquie jenkins , beverley collins , tony robson , suzanne scor eld , kathryn green , clare hall , xiao - hui liao , michael ryan , fiona johnson , guy stevens , olive kearins , sarah sellars , julietta patnick summary background the value of screen detection and treatment of ductal carcinoma in situ ( dcis ) is a matter of controversy . 
we sought to estimate the association between detection of dcis at screening and invasive interval cancers subsequent to the relevant screen . methods we obtained aggregate data for screen - detected cancers from 84 local screening units within 11 regional quality assurance reference centres in england , wales , and northern ireland from the national health service breast screening programme . 
data for dcis diagnoses were obtained for women aged 5064 years who were invited to and attended mammographic breast screening from april 1 , 2003 , to march 31 , 2007 ( 4 screening years )  . 
 patient - level data for interval cancer arising in the 36 months after each of these were analysed by poisson regression with invasive interval cancer screen detection rate as the outcome variable ; dcis detection frequencies were tted rst as a continuous and then as a categorical variable . 
we repeated this analysis after adjustment with both small size and high - grade invasive screen - detected cancers . findings we analysed data for 5 243 658 women and on interval cancers occurring in the 36 months after the relevant screen . 
there was a signi cant negative association of screen - detected dcis cases with the rate of invasive interval cancers ( poisson regression coe cient 0084 [ 95% ci 013 to 003 ] ; p = 0002 )  . 
90% of units had a dcis detection frequency within the range of 100 to 222 per 1000 women ; in these units , for every three screen - detected cases of dcis , there was one fewer invasive interval cancer in the next 3 years . 
this association remained after adjustment for numbers of small screen - detected invasive cancers and for numbers of grade 3 invasive screen - detected cancers . interpretation the association between screen - detected dcis and subsequent invasive interval cancers suggests that detection and treatment of dcis is worthwhile in prevention of future invasive disease . funding uk department of health policy research programme and nhs cancer screening programmes . copyright du y et al . 
open access article distributed under the terms of cc by . introduction the bene t - to - harm balance of screen detection and subsequent treatment of ductal carcinoma in situ of the breast ( dcis ) has been a matter of debate.13 dcis was rare in the era before screening , and a major question is the extent to which diagnosis and treatment of dcis could prevent the occurrence of invasive breast cancer in the future.4 in two randomised trials of screening , an excess of dcis in the study groups was almost entirely balanced by a corresponding de cit in invasive disease.5 further , in a trial of treatment of dcis , those cases who had only received wide local excision had a 10 - year rate of subsequent breast cancer events of more than 30% , suggesting a serious potential of dcis for progression.6 the fact remains , however , that for any individual dcis case that is treated , it cannot be known for certain what would have happened if the treatment had not taken place.6 however , with su cient aggregate data , it might be possible to assess the e ect of screen detection of dcis on the subsequent incidence of invasive cancer in a population subject to screening . in this study , we sought to estimate the association between detection of dcis at screening and invasive interval cancers subsequent to the relevant screen at unit level using data from the uk national health service breast screening programme ( nhsbsp )  . methods study population and design the nhsbsp o ers mammographic screening every 3 years to roughly 2 million women older than 50 years per year in the uk as a whole , and routinely invites women aged 5070 years.7 vol 17 january 2016 lancet oncol 2016 ; 17 : 10914 published online december 4 , 2015 s1470 - 2045 ( 15 ) 00446 - 5 this online publication has been corrected . 
it is not clear the extent to which diagnosis and treatment of dcis could prevent the occurrence of invasive breast cancer in the future . we searched pubmed with the search terms ductal carcinoma in situ and screening and breast and invasive and incidence for publications reporting on studies of any design investigating the e ect of screen detection of dcis on incidence of subsequent invasive cancer , published in any language between jan 1 , 1990 , and july 31 , 2015 . 
we found a negative association between detection of dcis at screening and invasive interval cancers . implications of all the available evidence this suggests that the policy of detection and treatment of dcis in breast cancer screening can prevent subsequent invasive disease . invited we obtained aggregate data for screen - detected cancers from 84 local screening units within 11 regional quality assurance reference centres in england , wales , and northern ireland from the nhsbsp via the nhs information centre ( now the health and social care information centre [ hscic ] ) and its counterparts in northern ireland and wales . 
data for breast cancer diagnoses , including dcis , were obtained for women aged 5064 years ( age range of the programme at its to and attended inception ) who were mammographic breast screening from april 1 , 2003 , to march 31 , 2007 ( 4 screening years )  . 
patient - level data for interval cancer were obtained from the regional screening quality assurance reference centres , who in interval turn received noti cations of subsequent cancers arising in the 36 months following screening from their regional cancer registries , for the number of subsequent interval cancers arising in the 36 months after each of these screening years . 
where regional boundaries changed during the period under scrutiny , con gurations of regions and responsibilities for units were taken to be those that existed in screening year 200607 . procedures from the aggregate data , we were able to ascertain the proportion of women diagnosed with dcis and invasive tumours . 
when available we obtained dcis grade and invasive tumour size and grade ; dcis tumours are graded as low , intermediate , and high , with low and intermediate grades grouped together . 
 usually , dcis is treated with complete local excision followed by radiotherapy ; however , the nhsbsp data are recorded mainly to monitor performance and thus do not contain information regarding subsequent treatment of patients with screen - detected cancer . 
as in a previous report , 8 interval cancers were de ned as cancers diagnosed symptomatically in women within 36 months of their last screen ( the maximum speci ed interval in the nhsbsp )  . 
for this analysis , we included rst and second primary , bilateral , and recurrent invasive interval cancers , but excluded contralateral interval cancers to ensure the outcome variable consisted of new primary breast cancers and because it is unlikely that the removal of a dcis in one breast could prevent an invasive tumour in the contralateral breast . statistical analysis for our primary analysis , we estimated the association between the frequency of dcis cases diagnosed at interval cancer screening and subsequent incidence using poisson regression , 9 with the following regression equation : invasive = a + b log where i represents invasive interval cancers in the individual screening unit following screening in an individual year , s is the total number screened in that unit and year , d is the number of screen - detected dcis cases in that unit and year , and a and b are the coe cients to be estimated . 
in addition , we tabulated the incidence of invasive interval cancers by dcis detection frequency in four categories ( < 1 per 1000 ; 1 < 15 per 1000 ; 15 < 2 per 1000 ; and 2 per 1000 ) , and tted the corresponding poisson regression model . 
 this allowed us to estimate the absolute de cit or increase in terms of the number of invasive interval cancers pertaining to di erent frequencies of dcis , for without assuming a parametric the relationship . 
in addition , we tted the poisson regression models adjusted for the number of screendetected grade 3 and small ( < 15 mm in diameter ) form 110 vol 17 january 2016 articles total number screened dcis cases detected at screening screen - detected dcis cases per 1000 women screened ( unit range ) screen - detected dcis cases with grading information ( % ) high grade screendetected dcis invasive cases detected at screening invasive screendetected cases per 1000 women screened ( unit range ) invasive interval cancers invasive interval cancers per 1000 women screened ( unit range ) 200304 200405 200506 200607 1 279 007 1 286 244 1 340 046 1 338 361 2003 2033 2144 2205 157 ( 073285 ) 158 ( 067356 ) 160 ( 054285 ) 165 ( 059322 ) 1671 ( 83% ) 1708 ( 84% ) 1842 ( 86% ) 1956 ( 89% ) 1036 1119 1213 6952 7194 7504 7364 544 ( 0761 ) 559 ( 374799 ) 560 ( 385764 ) 550 ( 377777 ) 3789 3688 4000 3737 296 ( 100496 ) 287 ( 074405 ) 298 ( 127560 ) 279 ( 125461 ) dcis = ductal carcinoma in situ . table 1 : dcis and invasive cancer detection frequency , and subsequent invasive interval cancer frequency by year of screening invasive cancers , because there is evidence that high tumours detected at invasive numbers of small screening are associated with lower interval cancer incidence.10 signi cance was assessed with wald tests , with p values of less than 005 being regarded as signi cant . 
because the average interval between screening rounds varies from unit to unit ( although most units achieve an average interval of less than 36 months ) , we also reanalysed the data with only the interval cancers diagnosed within the rst 24 months following a negative screen , since no unit operated an interval shorter than this , and because 24 months is the standard screening interval in many other countries.2 , 10 we also repeated the analysis to include the data available from scotland for screening year 200304 . 
 data were analysed with stata ( version 12 )  . role of the funding source the funders had no role in the study design ; collection , analysis , or interpretation of the data ; or the writing of the report . 
the corresponding author had the nal responsibility for the decision to submit for publication . data obtained screening aggregated results for 5 243 658 women screened between april 1 , 2003 , and march 31 , 2007 . 
all analyses were done both including and excluding these women ; the results were identical so we present the results excluding data of these 550 women from the analysis . the average number of women screened annually per unit was 15 700 ( unit range 383540 146 )  . 
table 1 shows the incidence of screen - detected dcis and screendetected invasive cancers for each screening year , and screen - detected dcis per 1000 women screened figure : fitted invasive interval cancer incidence from poisson regression as a function of dcis detection frequency at the previous screen dcis = ductal carcinoma in situ . the incidence of subsequent invasive interval cancers . 
among dcis cases that were graded , there was a higher proportion of low - grade dcis in units with a detection frequency higher than 15 per 1000 than in those units with a detection frequency of 15 per 1000 or less ( 1866 [ 40% ] of 4663 vs 967 [ 38% ] of 2569 ; p = 0008 )  . 
the 1000 women screened subsequent average detection frequency of invasive interval cancers was 290 per 1000 screened ( unit range 074560 per 1000 )  . incidence screen - detected dcis the primary analysis to estimate the association and between subsequent invasive interval cancer incidence resulted in a poisson regression coe cient of 0084 ( 95% ci 013 to 003 ) , a signi cant negative association ( p = 0002 )  . 
the poisson regression coe cient equivalent to the logarithm of the relative risk ( rr ) , thus a coe cient of 0084 indicates a reduction in risk of an invasive interval cancer per unit increase in the logarithm of the detection frequency of dcis ( rr 092 [ 95% ci 087098 ] )  . 
the tted incidence of invasive interval cancers per 1000 from the poisson regression see online for appendix vol 17 january 2016 articles adjustment for small ( < 15 mm ) invasive tumours adjustment for screen - detected grade 3 invasive tumours frequency of screen - detected dcis small screen - detected tumours frequency of screen - detected dcis grade 3 screen - detected tumours poisson regression coe cient ( 95% ci ) p value 0080 ( 013 to 003 ) 00003 ( 0001 to 00004 ) 0089 ( 014 to 003 ) 00003 ( 00003 to 0001 ) 0003 038 0001 035 restriction to invasive interval cancers diagnosed within 24 months frequency of screen - detected dcis 0089 ( 016 to 0016 ) 0016 repeat of primary analysis to include the 200304 data from scotland frequency of screen - detected dcis 0086 ( 014 to 0033 ) 0001 dcis = ductal carcinoma in situ . table 2 : results of secondary analyses of association of dcis detection frequencies with subsequent invasive interval cancer incidence average dcis detection per 1000 invasive interval cancers / total screened invasive interval cancers per 1000 rr ( 95% ci ) < 1 per 1000 1 < 15 per 1000 15 < 20 per 1000 2 per 1000 085 127 172 225 1236 / 392 982 6069 / 2 063 030 4844 / 1 686 588 3065 / 1 101 058 315 294 287 278 094 ( 088099 ) 091 ( 086097 ) 089 ( 083095 ) dcis = ductal carcinoma in situ . 
for up to around 15 per 1000 women screened , there are estimated two fewer invasive interval cancer cases for every three dcis cases ; from 15 to 25 per 1000 , around one invasive interval cancer case is estimated to be avoided per ve dcis cases . 
when the analyses were adjusted for grade 3 invasive cancers or small invasive cancers ( < 15 mm ) the results remained unchanged from the primary analysis ( table 2 )  . 
 results of the poisson regressions in relation to the magnitude and signi cance of the poisson regression coe cient were similar to that of the primary analysis ( table 2 )  . to estimate the absolute change in invasive interval cancers corresponding to di erent detected frequencies of dcis without assuming a speci c mathematical form of the association , we tted the model with dcis detection frequencies as a categorical variable ( table 3 )  . 
 these data suggest that at a dcis detection frequency of 115 per 1000 , for two dcis cases detected at interval screening , one invasive cancer immediately the screen was avoided ( a di erence of 315294 = 021 per 1000 invasive interval cancers compared with 127085 = 042 per following the 1000 screen - detected dcis )  . 
previous research has suggested that the frequency of detection of small invasive cancers might be negatively correlated with subsequent interval cancer incidence10 and increased detection of dcis has been associated with similarly increased detection of grade 3 invasive cancers.11 our results were unchanged when we adjusted for the detection of small invasive cancers and when we adjusted for the detection of grade 3 invasive cancers . our results suggest that at low levels of screen - detected dcis , up to 15 per 1000 , a reduction of one invasive interval cancer is observed per 153 dcis cases detected , and that at higher levels of detection , one less invasive interval cancer is observed per ve or six screendetected dcis cases . 
on the other hand , it could be that detection of dcis above two per 1000 prevents invasive cancers more than 3 years in the future , and that our study of the single interval after screen detection is too short to observe this . 
we noted that the units with increased detection of dcis overall had increased proportions of low - grade dcis , which might be expected to progress to invasive disease over a time period longer than 3 years . 
for units with dcis screen - detection frequencies that fall within the 90% range for all units , on average one invasive interval cancer would be avoided per three additional dcis cases detected . our results are ecological , based on screening unit level data . 
both dcis screendetection interval cancer frequency would be expected to increase slightly with age.7 , 8 our ndings cannot give de nitive proof of the progressive potential or otherwise of individual dcis frequency and invasive 112 vol 17 january 2016 articles the prevention of future cases . 
our results do , however , add to the evidence that detection and treatment of dcis is worthwhile invasive disease.5 , 6 , 1214 it is also worth noting that our results are consistent with a review of interval cancer incidence from eight screening rounds within four screening programmes , which tabulated invasive and in - situ screen - detection frequency with the interval cancer incidence.15 if one calculates the crude correlation coe cient of the in - situ screen - detection frequency with the interval cancer incidence reported in table 4 of that paper , a negative correlation of 029 is obtained.15 the median frequency of dcis detected at screening was 15 per 1000 women screened , ranging from 05 to 36 per 1000 . 
several factors a ect the frequency of screen - detected dcis and invasive cancer incidence , including age distribution among screening units , varying underlying cancer incidence , experience of the relevant professionals , and equipment di erences . 
 cancers identi ed in the screening programme reports as non - invasive were classed as dcis , thus these will contain a small proportion of microinvasive cancers . the nhsbsp screens women in the age range of 5070 years.7 when the programme began in 1988 , the target age range was 5064 years , but was extended to include woman up to the age of 70 years during 200305 in england and wales and in 2010 in northern ireland . 
however , there is ongoing and highly publicised debate about the harm caused by mammography screening in regard to overdiagnosis.1618 although it cannot be known for certain what would happen for any individual dcis that is treated , our ndings suggest that the treatment of dcis is worthwhile in the prevention of subsequent invasive disease . we intend to do similar analyses to relate invasive and dcis detection incidence from the screening data to those from the next scheduled screen of the same cohorts 3 years later . 
an analysis of invasive cancers in the breast screening programme in scotland noted that a high frequency of small invasive tumours at the prevalence screen was predictive of a low frequency of large invasive tumours at the incidence screen 3 years later , although this is confounded by number of mammographic views.19 in conclusion , we have found a negative association between screen detection of dcis and subsequent invasive interval cancer incidence . 
up to the median dcis detection rate of 15 per 1000 , we observed roughly one fewer invasive interval cancer per 153 dcis cases . contributors swd conceived and designed the study , supervised the statistical analysis , and drafted the paper . 
jp directed the screening programme . declaration of interests we declare no competing interests . acknowledgments we thank the quality assurance reference centres , the nhs information centre ( now replaced by hscic ) , breast test wales , and the northern ireland health and social care public health agency for supply of the aggregate data . 
the contributions of swd , ad , and dp were made as part of the programme of the policy research unit in cancer awareness , screening , and early diagnosis . 
it is a collaboration between researchers from seven institutions ( queen mary university of london , ucl , kings college london , london school of hygiene & tropical medicine , hull york medical school , durham university , and peninsula medical school )  . e - cigarettesnew product , old tricks tobacco smoking cessation represents one of the most successful public health initiatives in the world , with smoking prevalence at its lowest during the past decade according to recent who estimates . 
however , since the introduction of e - cigarettes in 2003 , marketed as a less harmful alternative to tobacco , what should have simply been an effective tool for tobacco smoking cessation is turning into a new mainstream addiction , with tobacco companies being one of the main beneficiaries and regulators entering the debate with naive tolerance . 
 recent months have seen a substantial increase in public promotion of e - cigarettes , taking advantage of the scarcity of evidence regarding the safety and long - term effects of these products . on oct 3 , 2018 , philip morris international , via prominent branding on ferraris formula 1 racing cars , launched mission winnow , a project in which they boldly claim to want to build a better world for women and men who smoke , using our scientific and engineering expertise to deliver it . 
the promotion of this undertaking as a major corporate responsibility exercise is not only deceptive , but also worrying because it demonstrates the extent to which the tobacco industry aims to shape the scientific evidence to support their commercial strategy of e - cigarettes as harmless smoking . 
the same week , on oct 7 , 2018 , the new york times reported about a cocktail party in geneva , switzerland , that coincidentally occurred at the same time and place as the biannual negotiations of the whos tobacco treaty , which were focused on deciding whether to recommend the introduction of stricter regulations for nicotine - delivery devices . 
in this evening event , cumbersomely named nicotine is not your enemy soire and sponsored by an organisation partly funded by the tobacco industrythe consumer choice center the lack of evidence regarding the long - term safety of e - cigarettes was used to persuade guests , who were enjoying an open bar , free tapas , and e - cigarette samples , to believe that e - cigarettes are harmless . 
this effort by tobacco industry representatives to surreptitiously influence who negotiations is yet another desperate attempt to influence the global public health agenda , and although it shouldnt come as a surprise given the tobacco industrys past activities , it is nevertheless deplorable . although the doors of the who are closed to e - cigarettes lobbying parties , those of the global market are wide open , and subliminal advertising are part of the industrys marketing strategy to promote e - cigarettes as the new smoking alternative . 
at the end of october , 2018 , philip morris international was accused of cynical advertising in the uk after the launch of a series of anti - smoking advertisements while still promoting smoking in other countries . 
altria and juul labs inc also announced that they will stop selling some flavoured vaping products in the usato pre - empt the us food and drug administration crackdownamid concerns of increased underage use of flavoured e - cigarettes . 
 the orchestrated effort and huge investment of the tobacco industry to promote e - cigarettes and alternative nicotine products deserves an equally in august response bold 2018 , an editorial in the lancet covering the uks house of commons science and technology committee report on e - cigarettes concluded that it is naive and premature of the committee to confuse an absence of evidence with an absence of har indeed , although e - cigarettes are unlikely to replicate the link between nicotine addiction and lung cancer caused by tobacco smoking , the absence of long - term evidence about the safety of vaping calls for a more precautionary attitude from policy makers . 
after a century of global inaction against the tobacco epidemic , the 2003 who framework convention on tobacco control provided effective evidence - based recommendations to inform policy and keep countries accountable to global tobacco control targets . 
instead of passively waiting for history itself , non - governmental organisations and governments alike should come together with a united vision to monitor and counter disinformation on e - cigarettes . 
although the long - term effects of e - cigarettes are still unknown , we are aware of their potential to create generations of nicotine addicts , which should be enough to trigger stricter regulations on these products . 
 the lancet oncology industry repeat for more on the who report on the global tobacco epidemic , 2017 see iris / bitstream / handle / 10665 / 255874 / 9789241512824 - eng . pdf ? sequence = 1 for more on mission winnow see com / story / 01 for more on the new york times report see nytimes.com / 2018 / 10 / 07 / health / tobacco - e - cigarettestreaty.html for more on cynical advertising see news / business - 45932048 for more on altrias e - cigarette strategy see washingtonpost.com / health / 2018 / 10 / 25 / marlboromaker - altria - halt - sales - flavorede - cigarettes - amid - concernsabout - youth - vapingsurge / ? noredirect = on&utm_ term = .db5ff0fa4920 the lancet editorial is available at journals / lancet / article / piis0140 - 6736 ( 18 ) 31935 - 4 / fulltext vol 19 december 2018 1543 editorial correction to lancet oncol 2018 ; 19 : 95364 correction to lancet oncol 2018 ; 19 : 104050 correction to lancet oncol 2018 ; 19 : e386 kramer souweidane mm , pandit - taskar n , et al . 
this correction has been made to the printed article , and to the online version as of aug 1 , 2018 . moreau p , mateos m - v , berenson jr , et al . 
lancet oncol 2018 ; 19 : 95364in the methods section of this article , the exclusion criteria for new york heart association heart failure should have been class iii or iv . 
this correction has been made to the online version as of aug 1 , 2018 . vol 19 aug 2018 e382 corrections 3 versus 6 months of adjuvant oxaliplatin - fluoropyrimidine combination therapy for colorectal cancer ( scot ) : an international , randomised , phase 3 , non - inferiority trial timothy j iveson * , rachel s kerr * , mark p saunders , jim cassidy , niels henrik hollander , josep tabernero , andrew haydon , bengt glimelius , andrea harkin , karen allan , john mcqueen , claire scudder , kathleen anne boyd , andrew briggs , ashita waterston , louise medley , charles wilson , richard ellis , sharadah essapen , amandeep s dhadda , mark harrison , stephen falk , sherif raouf , charlotte rees , rene k olesen , david propper , john bridgewater , ashraf azzabi , david farrugia , andrew webb , david cunningham , tamas hickish , andrew weaver , simon gollins , harpreet s wasan , james paul summary background 6 months of oxaliplatin - containing chemotherapy is usually given as adjuvant treatment for stage 3 colorectal cancer . 
we investigated whether 3 months of oxaliplatin - containing chemotherapy would be non - inferior to the usual 6 months of treatment . methods the scot study was an international , randomised , phase 3 , non - inferiority trial done at 244 centres . 
 patients aged 18 years or older with high - risk stage ii and stage iii colorectal cancer underwent central randomisation with minimisation for centre , choice of regimen , sex , disease site , n stage , t stage , and the starting dose of capecitabine . 
this trial is registered with isrctn , number isrctn59757862 , and follow - up is continuing . findings 6088 patients underwent randomisation between march 27 , 2008 , and nov 29 , 2013 . 
nine patients in the 3 month group and 14 patients in the 6 month group did not consent for their data to be used , leaving 3035 patients in the 3 month group and 3030 patients in the 6 month group for the intention - to - treat analyses . 
at the cutoff date for analysis , there had been 1482 disease - free survival events , with 740 in the 3 month group and 742 in the 6 month group . 
3 year disease - free survival was 767% ( 95% ci 751782 ) for the 3 month group and 771% ( 756786 ) for the 6 month group , giving a hazard ratio of 1006 ( 09091114 , test for non - inferiority p = 0012 ) , significantly below the non - inferiority marg peripheral neuropathy of grade 2 or worse was more common in the 6 month group ( 237 [ 58% ] of 409 patients for the subset with safety data ) than in the 3 month group ( 103 [ 25% ] of 420 ) and was long - lasting and associated with worse quality of life . 
1098 serious adverse events were reported ( 492 reports in the 3 month group and 606 reports in the 6 month group ) and 32 treatment - related deaths occurred ( 16 in each group )  . interpretation in the whole study population , 3 months of oxaliplatin - containing adjuvant chemotherapy was noninferior to 6 months of the same therapy for patients with high - risk stage ii and stage iii colorectal cancer and was associated with reduced toxicity and improved quality of life . 
despite the fact the study was underpowered , these data suggest that a shorter duration leads to similar survival outcomes with better quality of life and thus might represent a new standard of care . 
the scot study was designed to test for the non - inferiority of 3 months of treatment compared with the standard 6 month duration . added value of this study worldwide , six studies have addressed this research question , of which scot is the largest . 
peripheral neuropathy was significantly worse in the 6 month group and reducing the treatment duration to 3 months more than halved the number of grade 3 or 4 peripheral neuropathy events reported . 
moreover those patients who were most severely affected by peripheral neuropathy also had a significant reduction in quality of life . implications of all the available evidence in view of the results of the scot study and the meta - analysis of all six worldwide studies conducted by the idea collaboration , 3 months of adjuvant chemotherapy will become the new global standard of adjuvant treatment for most patients who are suitable for treatment with capox , particularly those patients with t13 , n1 disease . the major cumulative chronic toxic effect of oxaliplatincontaining chemotherapy is sensory peripheral neuropathy , which can be disabling . 
this effect is recognised to be dependent on dose and duration and can be long - lasting.8 , 9 as most patients undergoing adjuvant chemotherapy are cured and will survive , long - term , irreversible peripheral neuropathy is a significant issue . the current standard duration of adjuvant chemo therapy for colorectal cancer is 6 months . 
a shorter duration of adjuvant chemotherapy would be expected to result in less chronic peripheral neuropathy , but it has been hitherto unknown to what , if any , extent cutting duration would compromise its efficacy . 
the results of one study10 using fluoropyrimidine alone , which was not powered for non - inferiority , suggested that 3 months of infused fluoropyrimidine was similar to 6 months of bolus fluoropyrimidine treatment in terms of disease - free survival.10 the scot study was designed as a stand - alone international phase 3 non - inferiority study to investigate whether 3 months of oxaliplatin - based adjuvant chemotherapy for colorectal cancer is non - inferior to 6 months of treatment with the same regimen . 
here we report the final efficacy results of disease - free survival and the toxicity and quality - of - life ( qol ) results . methods study design and participants the scot study is an international , randomised , nonblinded , non - inferiority , phase 3 trial comparing 6 months versus 3 months of oxaliplatin and fluoropyrimidine adjuvant chemotherapy in patients with high - risk stage ii or stage iii colorectal cancer . 
patients were recruited from 244 centres in six countries ( the uk , denmark , spain , sweden , australia , and new zealand )  . patients were eligible if they were aged 18 years or older and had undergone a curative resection for stage iii or high - risk stage ii ( defined as having one or more of t4 disease , tumour obstruction with or without perforation of the primary tumour preoperatively , fewer than ten lymph nodes harvested , poorly differentiated histology , perineural invasion , or extramural venous or lymphatic vascular invasion ) adenocarcinoma of the colon or rectupatients were enrolled within 11 weeks of surgery and started treatment on their allocated study group within 2 weeks of randomisation . 
other eligibility inclusion requirements included who performance status 0 or 1 , adequate organ function , and life expectancy of greater than 5 years with reference to noncancer related diseases . 
patients had to have a normal ct scan of the chest , abdomen , and pelvis before study enrolment and carcinoembryonic antigen less than 12 times the local upper limit of normal ( uln ) within 1 week before randomisation . 
exclusion criteria included chemotherapy ( except chemotherapy administered with curative intent that was completed > 5 years ago and from which there were no residual complications ) , previous long - course chemo radiotherapy ( preoperative short - course radiotherapy alone was allowed ) , moderate or severe renal impair ment ( glomerular filtration rate or creatinine clearance < 30 ml / min , as calculated with the cockcroftgault equation ) , haemoglobin less than 9 g / dl , absolute neutrophil count less than 15 10 cells per l , platelet count less than 100 10 cells per l , and aspartate aminotransferase or alanine aminotransferase greater than 25 times the uln . 
this study was approved by the west glasgow research ethics committee ( version 1.1 of the protocol ) on jan 21 , 2008 , and all subsequent amendments approved by the committee , where required ( rec reference number 07 / s0703 / 136 )  . 
 randomisation and masking by use of a minimisation algorithm incorporating a random component , patients were centrally randomly assigned ( 1 : 1 ) , to receive either 3 months or 6 months of treatment . 
the minimisation factors were centre , choice of regimen , sex , disease site ( colon vs rectum ) , n stage ( x , 0 , 1 , or 2 ) and t stage ( x , 0 , 1 , 2 , 3 , or 4 ) and , if the patient was going to receive the capox ( capecitabine and oxaliplatin ) regimen , the starting dose of capecitabine ( from feb 1 , 2010 )  . initially some participating centres were randomly allocated to randomise patients after completion of the first 3 months of treatment to either receive a further 3 months treatment or to stop treatment . 
this approach was stopped because of a poorer randomisation rate ( ie , fewer patients randomised per month ) compared with centres that randomised patients before the start of treatment.11 participants were enrolled by authorised clinicians , after obtaining patient consent , by contacting the cancer research uk clinical trials unit in glasgow , uk , to check eligibility and request an allocation . 
 the study was open - label for patients , clinicians , and those doing the data analysis . procedures patients were assigned to receive oxaliplatin - containing adjuvant treatment for either 3 months or 6 months . 
 the chemotherapy regimen , which could be folfox ( bolus and infused fluorouracil with oxaliplatin ) or capox , was chosen by the physician and patient and was not randomised . for patients receiving folfox , treatment was given every 2 weeks with the intention of delivering six cycles to patients assigned 3 months of therapy and 12 cycles to patients assigned 6 months of therapy . 
intravenous oxaliplatin 85 mg / m was given over 2 h on day one concurrently with l - folinic acid 175 mg or folinic acid ( leucovorin ) 350 mg . 
this was followed by an intravenous bolus injection of fluorouracil 400 mg / m over 5 min , then a continuous intravenous infusion of fluorouracil 2400 mg / m over 46 h . 
at the investigators discretion , patients receiving folfox who were older than 70 years could start on the bolus and continuous infusion of fluorouracil at 75% of the starting dose , if clinically indicated . for patients receiving capox , treatment was given every 3 weeks with an intention of delivering four cycles to patients assigned 3 months of therapy and eight cycles to patients assigned 6 months of therapy . 
patients older than 70 years could be considered for treatment with capecitabine at 75% of the full dose , but the decision to reduce dose was left to the discretion of the investigator , depending on the fitness of the individual patient . 
if the clinician felt that any other patient required a - priori dose reduction because of any other comorbidity , that patient could be started on a minimum starting dose of oral capecitabine 800 mg / m twice per day . 
 toxicity was assessed by the investigators after each cycle of chemotherapy treatment and graded by use of national cancer institute common terminology criteria for adverse events ( ctcae ) version three . 
for capox , if more than one delay or a delay of at least 2 weeks occurred , capecitabine and oxaliplatin doses were reduced by 25% and , if further delays occurred due to myelotoxicity , further dose reductions were allowed at the investigators discretion . 
for folfox , if more than one delay or a delay of at least 2 weeks occurred , doses of oxaliplatin and infused fluorouracil were maintained , but the bolus fluorouracil was omitted and , if further delays occurred due to myelotoxicity , the oxaliplatin and infusional fluorouracil doses were reduced by 25% . 
 also for folfox , if after the first cycle neutrophils were less than 10 10 cells per l , the bolus fluorouracil was omitted and the oxaliplatin and infused fluorouracil doses were reduced by 25% . 
patients were followed up for 8 years with full blood count , urea and electrolyte , liver function , and carcinoembryonic antigen tested at months 9 , 12 , 18 , 24 , and 36 , then 564 vol 19 april 2018 articles annually . 
ct of the chest , abdomen , and pelvis was done at months 6 , 12 , 18 , 24 and 36 . qol was assessed with the european organisation for research and treatment of cancer ( eortc ) qlq - c30 and qlq - cr29 and eq - 5d - 3l ( visual analogue scale and health index ) , with uk value sets.12 neuropathy was assessed with the fact / gog - ntx4 questionnaire . the qol questionnaires were administered at baseline and before each treatment cycle . 
subsequent assessments were made at months 9 and 12 for the eortc questionnaires and months 9 , 12 , 18 , and 24 , then annually for eq - 5d - 3l . neuropathy assessments with fact / gog - ntx4 were initially completed up to 12 months , as were the eortc questionnaires in patients who underwent randomisation before feb 16 , 2011 , from sites that opted to participate in this substudy . 
an amendment introduced in version 3.0 of the protocol on march 20 , 2012 , extended the requirement for the neuropathy questionnaire to be completed for patients who completed it at baseline to the follow - up visits at months 18 and 24 . 
a further amendment ( version 4.0 on dec 20 , 2012 ) extended the requirement for the neuropathy questionnaire to be completed to every follow - up visit ( to a maximum of 8 years ) for all new patients and existing patients already participating in the substudy . 
these amendments were made as a result of recommendations by the independent data monitoring committee . outcomes the primary study endpoint was disease - free survival , defined as the time from randomisation ( or trial registration for those randomised after 3 months of therapy ) to relapse , development of a new colorectal cancer , or death from any cause . 
assuming that the study would recruit over a period of 5 years with a subsequent minimum follow - up of 2 years , this design required 8600 patients to undergo randomisation and 2750 events ( relapses , deaths , or new colorectal cancers ) to be observed . 
to allow for losses to follow - up , our target recruitment was 9500 patients . from the outset , we recognised that reliable conclusions based on safety and qol data would not require information on all 9500 patients . 
for safety outcomes , the plan was that 700 patients ( 350 in each group ) would be sufficient to detect ( with 80% power and two - sided significance level of 5% ) a halving in the proportion of patients with grade 3 or 4 toxic effects from 12% to 6% ( 12% being the rate at which grade 3 or 4 paraesthesia the most frequent non - haematological grade 3 or 4 toxic effectoccurred in the oxaliplatin group in the mosaic trial ) .3 this same sample size would allow small changes in global qol to be detected ( assuming a difference of magnitude of 75313 and a standard deviation of 234 ) 14 with 95% power at the 1% significance level . 
this more stringent level of significance was used to allow for multiple testing across the various qol scales . we collected information on these toxicity and qol endpoints from all patients recruited until the number required was exceeded and the decision to stop was endorsed by the independent data monitoring committee and trial steering committee . 
the data monitoring committee had access to summary plots of eortc qol data , eq - 5d health status , and fact / gog - ntx4 neuropathy data by study group and study timepoints and following a committee meeting on may 28 , 2010 ( based on 1047 randomised patients ) , recommended that the collection of qol and fact / gog - ntx4 data be continued because they were concerned that the amount of missing data might undermine the comparisons at later timepoints if the original sample size estimates were used . 
they also recommended that the collection of fact / gog - ntx4 data should be extended beyond 12 months for new patients and , where possible , for patients already on the study . 
at their next meeting on the data monitoring committee nov 23 , 2010 , recommended the collection of qol and fact / gog - ntx4 data should stop once 1800 patients had been recruited . 
delays in the amendment of the protocol to implement the collection of the fact / gogntx4 beyond 12 months led to patient recruitment beyond this recommendation to ensure sufficient numbers of patients at these later timepoints . 
these extensions to data collection were made to compensate for missing data and no formal power calculations were made for these changes . that the efficacy analyses of disease - free survival and overall survival included all randomly assigned patients far as possible . 
 ( intention - to - treat population ) as vol 19 april 2018 articles kaplan - meier techniques were used to plot both disease - free survival and overall survival . 
the analysis of treatment delivery and safety was based on patients who started study treatment . the comparison of disease - free survival and overall survival between the treatment groups was based on a cox regression model incorporating the minimisation factors as covariates . 
the p value for testing the null hypothesis that the hr of 3 months versus 6 months was greater than or equal to 113 was derived from this model by comparing the log - likelihood of the fitted model with the log - likelihood of a model where the hr between the groups is set to 113 by use of a likelihood ratio test . 
the proportional hazards assumption implicit in these analyses was examined graphically via a log - minus log plot of the survival function against log time and via a test of the interaction between the treatment group and time ( logged ) obtained from a cox model time - varying covariate . incorporating an appropriate the components of the forest plot ( estimated hr for the comparison between groups and associated 95% ci ) were derived from a cox model that included separate terms for the effect of duration within each category of the relevant stratification factor or other factor being examined . 
patients could have more than one reason . 566 vol 19 april 2018 articles the impact of treatment duration varied across important patient subgroups . multiple imputation analysis15 was used to fill in the missing data and questionnaires in the qol and neuropathy scales . 
 the standardised adjusted auc was calculated for the five imputed datasets and compared between the randomised treatment groups via a generalised linear model ( with study group as an independent factor and study minimisation factors as covariates )  . 
the test statistics associated with study group from each of the five imputations were finally combined to provide an overall p value that takes into account the extent of the missing data . 
to allow for the number of scales being examined , an adjustment for multiple comparisons ( separately for the eortc and eq - 5d questionnaires ) was made with the sharpened hochberg procedure.17 the p value threshold for statistical significance was 5% after adjustment . 
comparisons of these scales at individual timepoints also made use of multiple imputation and generalised linear models . the mann - whitney u test was used for the comparison of ordered categorical variables for toxicity grade . 
 fishers exact test was used to compare the incidence of grade 35 toxic effects and the odds ratio and associated confidence interval for the incidence of grade 35 toxicity was estimated using logistic regression . about issues the study data were reviewed by the data monitoring committee approximately once per year to assess safety and efficacy from an ethical viewpoint . 
 the conditional power for disease - free survival was presented at the fifth ( june 26 , 2012 ) , sixth ( jan 7 , 2013 ) , and seventh ( oct 2 , 2013 ) meetings of the data monitoring committee . 
the data monitoring committee also had access to interim disease - free survival results from an italian study tosca ( nct00646607 ) , which was addressing the same question and had more mature data at the time . 
 table 1 : baseline patient characteristics recorded at randomisation by study group role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the study did not meet its recruitment target of 9500 patients because accrual was not as rapid as originally forecast and recruitment needed to stop to allow sufficiently complete follow - up on current patients within the available funding . 
 by increasing the recruitment period by 6 months and extending minimum follow - up to 3 years ( 88% patients were followed up for 3 year disease - free survival by the reverse kaplan - meier method , allowing for a 2 month deviation from the assessment time ) , 1482 disease - free survival events were observed , giving the study 66% power rather than the originally planned 90% power for rejecting the null hypothesis . 
results from previous adjuvant studies have shown that most disease - free survival events occur within the first 3 years of starting treatment.3 , 19 the analysis time was prespecified in the protocol and therefore no bias would be introduced as might be the case if we had allowed the timing of the analysis to be guided by the data at hand . the data cutoff for this analysis was dec 1 , 2016 . 
787 patients had died at the time of analysis . 568 vol 19 april 2018 articles the baseline demographics , stage , and site of disease for each group were balanced across the trial population ( table 1 )  . 
the largest difference between the overall population and the subgroups assessed for safety and qol was a 9% increase in the incidence of patients with performance status 1 in the ctcae safety cohort ; all other differences in individual characteristics were within 5% . at the time of the disease - free survival analysis there had been 740 events in the 3 month group and 742 events in the 6 month group . 
3 year disease - free survival was 767% ( 95% ci 751782 ) in the 3 month group and 771% ( 756786 ) in the 6 month group , giving an hr of 1006 ( 09091114 , p = 0012 ) which met the criteria for non - inferiority ( figure 2 )  . 3 year overall survival is shown in figure 2 . 
the appendix contains a breakdown of causes of death ( p 10 ) and further details of deaths related to protocol treatment ( p 11 )  . in a prespecified sensitivity analysis , we also examined the difference between the study groups according to the actual duration of treatment on the two randomised groups ( appendix p 1 )  . 
for eligible patients who received the actual assigned study duration of 3 and 6 months , the observed hr was 1158 ( 95% ci 10181317 , p = 0641 )  . forest plots by stratification factors and randomisation timepoint are shown in figure 3 . 
the most marked heterogeneity was for the dependence of the duration effect on the initial choice of regimen ( p = 0069 ) , so we did a post - hoc analysis of disease - free survival for the two durations of therapy for capox and folfox regimens ( figure 4 )  . 
 among patients with available chemotherapy duration data , 2521 ( 83% ) of 3024 of patients assigned to 3 months of treatment actually received 3 months of treatment , including 845 ( 86% ) of 980 receiving folfox and 1676 ( 82% ) of the 2044 receiving capox . 
1773 ( 59% ) of 3013 patients assigned to receive 6 months of treatment actually received 6 months of treatment , which was similar for those receiving folfox ( 585 [ 59% ] of 985 ) and capox ( 1188 [ 59% ] of 2028 )  . 
 * these estimates differ slightly because the underlying multivariable cox model on which they are based includes parameters for other minimisation variables , as well as those factors relating to stage ; the increased flexibility in the expanded stage model allows the influence of these parameters on the high risk stage ii estimates to modify . 
 see online for appendix receive 3 months ( 425 [ 14% ] of 3024 ) and 6 months ( 417 [ 14% ] of 3013 ) of treatment . 244 patients in the 3 month group and 576 patients in the 6 month group cited adverse events as the reason for stopping treatment early . 
in the 6 month group , both diarrhoea ( 150 patients ) and peripheral neuropathy ( 156 patients ) were commonly cited as reasons for stopping . figure 5 shows the dose delivery for fluoropyrimidine and oxaliplat the median percentage of full fluoropyrimidine dose delivered was 953% ( iqr 831998 ) in the 3 month group and 832% ( 567957 ) in the 6 month group . 
the number of patients who had recorded fluorouracil or prescribed capecitabine dose reductions in the 3 month group were 788 ( 26% ) of 3009 compared with 1286 ( 43% ) of 3013 in the 6 month group . 
for oxaliplatin , the corresponding figures were 906 ( 30% ) of 3009 and 1869 ( 62% ) of 3013 . given previous trial data , 20 it is known that there is a marked difference in risk of relapse between patients with n1 colorectal cancer compared with those with n2 pathology , so we did a post - hoc analysis comparing t13 , n1 colorectal cancer against t4 and n2 pathology ( figure 6 ) , and analysed these different prognostic groups according to the chemotherapy regimen they received ( folfox or capox ; appendix p 5 )  . 
for those patients with t1 - 3 / n1 disease the test for non - inferiority in this post - hoc analysis was statistically significant ( p = 0012 )  . safety was assessed by the investigators in 868 patients , 434 ( 50% ) in each group . 
sensory neuropathy , diarrhoea , neutropenia , fatigue , pain , nausea , and hand - foot syndrome were the most common grade 35 adverse events ( table 2 )  . 
the frequency of grade 35 diarrhoea ( p = 0033 ) , neutropenia ( p = 0014 ) , hand - foot syndrome ( p = 0031 ) , and sensory neuropathy ( p < 00001 ) was significantly higher in the 6 month group than in the 3 month group . 
the only side - effect for which the percentage of patients with adverse events ( p = 0031 ) , pain 570 vol 19 april 2018 articles during months 9 and 12 after patients in the 6 month group had stopped treatment . 
overall , grade 35 adverse events were reported by 150 ( 36% ) of 420 patients in the 3 month group and 243 ( 59% ) of 409 patients in the 6 month group ( p < 00001 )  . 
we compared the results from the fact / gog - ntx4 questionnaire for patients receiving 3 months of chemotherapy with those receiving 6 months of chemotherapy ( figure 7 )  . 
the neuropathy standardised adjusted auc differed significantly between the two study groups ( p < 00001 ) , with clear differences appearing at month 4 and persisting until at least 5 years ( p < 00001 )  . 
the maximum difference in means was generally seen at 6 months and , in accordance with the categories of osoba and colleagues , 13 these mean differences in functional and global health status scales represented moderate changes ( values between 1020 ) for global health status , role functioning , and social function and a ( values between 510 ) for physical little change functioning , and cognitive functioning , emotional functioning . 
thereafter , the mean values converged 3 months of treatment 6 months of treatment study group figure 5 : treatment delivery by selected adjuvant regimen box and whisker plots indicate median and iqr ( boxes ) and range ( whiskers )  . 
the standardised adjusted aucs differed significantly for both the eq - 5d self - rated visual analogue scale ( p = 000081 ) and the eq - 5d - 3l health index ( p = 000081 ; appendix p 15 )  . 
 plotting the eq - 5d scales showed that the differences between the two groups of the study were restricted to months 4 , 5 , and 6 , the period when patients in the 6 month group were still receiving treatment and those in the 3 month group had stopped . 
the maximum difference in means was at 6 months and these differences were consistent with clinically important differences ( appendix p 15 ) .21 this pattern was also noticeable for the eq - 5d selfrated visual analogue scale ; patients in the 6 month group had significantly lower qol than those in the 3 month group during months 4 , 5 , and 6 , but after this point , there were no overall clinically important differences up to the 6 year follow - up ( appendix p 3 )  . to investigate the potential effects of missing data on the results from the fact / gog - ntx4 , eortc , and eq - 5d assessments , the reasons for missing questionnaires were recorded ( appendix p 16 )  . 
similarly , an analysis of missingness according to baseline factors indicated that the patients who completed the questionnaires were representative of the patients who participated in this aspect of the study , with any associations between a questionnaire being missing and 572 vol 19 april 2018 articles l vol 19 april 2018 articles 6 months 3 months baseline 1 month 2 month 3 month 4 month 5 month 6 month 9 month 1 year 18 months 2 years 3 years 4 years 5 years 6 years assessment timepoint baseline month 1 month 2 month 3 month 4 month 5 month 6 month 9 year 1 month 18 * year 2 * year 3 * year 4 year 5 year 6 3 months treatment questionnaires completed questionnaires expected proportion of expected questionnaires received 859 1445 59% 6 months treatment questionnaires completed questionnaires expected proportion of expected questionnaires received 865 1426 61% 817 1433 57% 782 1426 55% 527 1421 37% 639 1416 45% 639 1416 45% 606 1400 43% 733 1386 53% 721 1266 53% 172 1312 13% 169 1202 14% 22% 796 1406 57% 782 1395 56% 701 1389 50% 679 1384 49% 679 1382 45% 268 1375 19% 665 1366 49% 721 1346 54% 182 1308 13% 174 1195 15% 22% 48% 42% 62% 54% figure 7 : peripheral neuropathy by study group patients reported peripheral neuropathy with the gog ntx4 questionnaire . 
 * the low completion rates at these timepoints reflect the fact that , initially , neurotoxicity data were only collected up to 12 months and there was a delay before an amendment extended the collection to the whole study period . 
low return rate because patients were assessed at the start of last cycle rather than 6 months ( which corresponds to end of cycle )  . baseline characteristics being small ( appendix p 17 )  . 
 finally , we did a sensitivity analysis to compare the primary imputed results with the results based on observed data only or the imputed results for patients who completed baseline questionnaires only . 
the results of these analyses were all very similar to the findings of the main study ( appendix p 18 )  . we did an exploratory analysis to examine the differences in qol scales between patients whose worst responses to the questions on the gogntx4 questionnaire about whether they had numbness , tingling , or discomfort in their hands or feet were quite a bit or very much and those whose worst responses were somewhat , a little bit , or not at all ( appendix p 4 )  . 
this analysis identified statistically and clinically significant poorer qol between these patient groups at 1 year , 3 years , and 5 years , apart from eq - 5d visual analogue scale at 1 year , for which the difference was not clinically significant . 
the proportion of patients recording neuropathy symptoms as being present quite a bit or very much was significantly higher in the 6 month group than in the 3 month group at each timepoint ( 248 [ 34% ] of 721 vs 99 [ 14% ] of 721 , p < 00001 at 1 year ; 63 [ 32% ] of 199 vs 30 [ 15% ] of 198 , p < 00001 at 3 years ; 49 [ 29% ] of 170 vs 30 [ 16% ] of 193 , p = 00032 at 5 years )  . discussion our results show the non - inferiority of 3 months of adjuvant oxaliplatin - containing chemotherapy treatment compared with 6 months of treatment for patients with high - risk stage ii and stage iii cancer of the colon and rectu the shorter treatment duration was also associated with reduced toxicity and less deterioration in qol . 
because this study recruited 6088 patients with conventionally defined high - risk stage ii and stage iii colorectal cancer from a large number of centres and countries and made use of standard chemotherapy regimens , the study findings are applicable to a typical patient with colorectal cancer needing adjuvant chemotherapy treatment . 
the non - inferiority boundary was set to exclude a maximum 25% fall in 3 year disease - free survival in patients in the 3 month group compared with those in the 6 month group , whichas estimated on the basis of results from previous trials would yield a predicted 3 year disease - free survival of 78% . 
this threshold of 25% was chosen because it was half the difference seen in 3 year disease - free survival between patients in the oxaliplatin - containing group and those in the fluoropyrimidine only group in the mosaic study . 
it was felt by clinicians commonly treating 574 vol 19 april 2018 articles colorectal cancer that this small difference would be an acceptable payoff to bring about a significant reduction in long - term neuropathy and potential improvement in qol to patients who achieve a long - term cure . 
this difference corresponds to an hr of 113 , which we aimed to detect with 90% power at the 25% one - sided level of statistical significance . initial ( rather than our because 6088 patients were recruited and 1482 events were recorded target of 9500 patients with 2750 events ) , the power was reduced to 66% . 
however , we were still able to show the noninferiority of 3 months of treatment compared with 6 months of treatment ( p = 0012 ) across the trial population as a whole ( stage iii and high risk stage ii disease ; colon and rectal cancer ) , with 3 year disease - free survival of 771% ( 95% ci 756 to 786 ) for patients in the 6 month group and 767% ( 751 to 782 ) for those in the 3 month group ( hr 1006 , 0909 to 1114 )  . 
patients in the 6 month group had similar 3 year disease - free survival to that seen with 6 months of oxaliplatin - containing adjuvant chemotherapy in the mosaic study ( 782% ) and nsabp c07 studies ( 761% ) , suggesting that the outcome observed in our control group was similar to that previously seen.3 , 4 however , it is important to note that in the scot trial , only 1096 ( 18% ) of 6088 patients had highrisk stage ii disease , whereas in mosaic and nsabp - c07 , 40% and 30% of patients had all - risk stage ii disease . 
at the time scot was initiated , less data were available on adjuvant chemotherapy for rectal cancer because many adjuvant studies have excluded these patients , and patients with rectal cancer were eligible to participate if they had received no preoperative chemotherapy ( short - course radiotherapy alone was allowed ) and had undergone total mesorectal excision with an r0 resection . 
the only adjuvant chemotherapy these patients received was within this study and randomised for the duration of treatment . we did comparisons of disease - free survival based on the actual duration of treatment received in the study groups , as well as the primary intention - to - treat analyses . 
 these subanalyses did not show non - inferiority , but are inherently biased by the differential exclusion of patients not able to receive prolonged therapy because of the different target treatment durations in the study groups . 
 in a setting such as this where differential compliance is intrinsic to the treatments being compared , our view is that the intention - to - treat analysis is a more accurate reflection of the impact of the intervention on actual clinical practice . in terms of our analyses of smaller subgroups , we have not been able to draw solid conclusions about the effect of treatment duration on specific patient populations such as those with high - risk stage ii disease or patients with rectal cancer because the numbers in these subgroups were relatively small and few events occurred . 
however , the forest plots did not show any differences in the effect of the duration of adjuvant chemotherapy between patients with high - risk stage 2 disease and those with stage iii disease and between those with rectal cancer and those with colon cancer . 
in clinical practice in many parts of the world , a substantial proportion of patients with high - risk stage ii disease or stage iii disease ( especially if older than 70 years of age ) receive only single - agent fluoropyrimidine for 6 months because the addition of oxaliplatin to fluoropyrimidine has not been shown to improve survival in these patients.22 other factors to consider in terms of prognosis and prediction of response to treatment include the sidedness of the cancer ( right vs left ) , ras and braf status , which affect prognosis in metastatic disease , and microsatellite instability status , which affects the outcome of adjuvant treatment.23 these questions cannot yet be answered by the results of scot , but there is a translational research substudythe transscot study , which is ongoing that will look at these factors . it is more difficult to give 6 months of treatment than 3 months of treatment . 
in the scot study , 2521 ( 83% ) of 3024 patients assigned to 3 months received 3 months of treatment , whereas only 1773 ( 59% ) of 3013 patients assigned to 6 months received 6 months of treatment . 
however , the median percentage of the full expected dose of fluoropyrimidine received varied between 94% and 98% for the 3 month group and 82% and 85% for the 6 month group , depending on regimen choice . 
given that the median fluoropyrimidine and oxaliplatin doses received were similar between the two regimens ( figure 5 ) , compliance to treatment is unlikely to explain the difference seen between the two regimens . our results showed that 6 months of adjuvant chemotherapy was significantly more toxic than 3 months of treatment . 
this difference was most marked for peripheral neuropathy , with 237 ( 58% ) of 409 patients in the 6 month group reporting grade 2 or worse neuropathy compared with 103 ( 25% ) of 420 patients in the 3 month group . 
peripheral neuropathy , as reported via a patient questionnaire , was significantly worse in the 6 month group and persisted for at least 5 years ( figure 7 )  . 
however , the vol 19 april 2018 articles effects are large , as are the significance levels , and there is no evidence that these comparisons are biased between the groups , qol , as measured by qlq - c30 global health status and eq - 5d - 3l , declined while patients were receiving chemotherapy . 
 in peripheral neuropathy , with more patients in the 6 month group reporting quite a bit or very much numbness , tingling , or discomfort in their hands or feet in the fact / gog - ntx4 questionnaire , which correlated with significantly worse qol at 1 year , 3 years , and 5 years . 
when we looked at the effect of duration for each regimen separately , capox showed non - inferiority in terms of disease - free survival for 3 months versus 6 months of treatment , but this was not the case for patients receiving folfox . 
the choice of chemotherapy regimen was not randomised but instead chosen by the physician and patient and the reasons why specific regimens were chosen for individual patients are not known . also important to note for capecitabine , an oral drug that is self - administered at home , is that we only know that we might overestimate the prescribed dose and do not have detailed compliance the data , meaning fluoropyrimidine dose intensity for patients receiving capox . 
however , in our experience , except in instances where clinicians curtail or modify doses according to intracycle toxicity , compliance with oral chemotherapy drugs is high . since the difference in the impact of treatment duration between the capox and folfox regimens does not seem to be easily explained by compliance with treatment or differences in the overall percentage of standard drug doses that were delivered , we perhaps need to consider other potential reasons for this finding . 
in the capox regimen , the dose of oxaliplatin given with each cycle is higher than that given in folfox , and therefore we presume that higher peak doses of oxaliplatin are achieved . 
additionally , although the peak dose of fluoropyrimidine will be lower with capox ( capecitabine is given twice daily orally for two out of three weeks ) than with folfox ( where the fluoropyrimidine is given as a bolus , then infused over 2 days every 2 weeks ) , the duration and continuity of exposure is greater . 
could the micrometastatic disease be rendered more sensitive by one or both of these differences ? if each of the cells in this micrometastatic setting are cycling through s phase only sporadically , does the continuity of exposure of the fluoropyrimidine in the form of capecitabine mean that there is a greater overall chance that these cells will be exposed to fluoropyrimidine at the critical part of the cell cycle , compared with fluorouracil given as bolus , then over 2 days every 2 weeks . 
this notion is supported by data from two previous adjuvant studies.10 , 28 in terms of oxaliplatin , a drug that is nearly always given over 24 h , does the peak concentration have more of an effect than the frequency , giving an advantage to the capox regimen and less attrition to efficacy when the overall duration of therapy is shortened ? additionally , a higher dose of oxaliplatin is given in the first 4 weeks of treatment with capox ( 260 mg / m ) than with folfox ( 170 mg / m )  . 
it is very difficult to prove these speculative theories without developing appropriate adjuvant models of malignancy , but the results seen will certainly be a focus of strong debate over the coming months and years . stage iii colorectal cancer is a heterogeneous disease and data from the idea collaboration and from multiple adjuvant trials have shown that patients with t13 , n1 pathology have much better outcomes than those with either t4 or n2 features.27 this has led to the evolution of the concept of a high - risk stage iii patient population , with either t4 or n2 disease , as opposed to the lower risk stage iii population ( t13 , n1 ) ; we might need to consider whether patients with high - risk stage iii disease need to be treated in a slightly different way to those with lower risk stage iii disease . similarly , our results have shown that patients with t13 , n1 disease have a much better 3 year disease - free survival than those with either t4 or n2 pathology . 
 576 vol 19 april 2018 articles we found that , in patients with t13 , n1 colorectal cancer , 3 months of treatment was non - inferior to 6 months ( hr 0908 , 95% ci 0751098 )  . 
the hr for disease - free survival is greater than 1 for the 3 months duration compared to 6 months , suggesting that there could be some small loss of efficacy , but the confidence intervals are wide , making this difference difficult to interpret with certainty . 
notably , the observed absolute deficit in 3 year disease - free survival between the 3 months and 6 months of treatment for the high - risk group ( t4 or n2 disease ) is 18% , which has to be balanced against the increased toxicity seen with 6 months of treatment . 
this is particularly important because the worsened peripheral neuropathy persists for at least 5 years after treatment and results in worse qol outcomes . for patients with t4 or n2 pathology , the absolute increase in 3 year disease - free survival with 6 months versus 3 months of treatment was 27% ( 95% ci 41 to 96 ) for folfox and 13% ( 95% ci 37 to 62 ) for capox ( appendix p 5 )  . 
in view of the difference in toxicity seen with longer treatment , many patients will accept a small reduction in disease - free survival in exchange for reduced toxicity and this is especially true if they are able to receive capox . 
there is less evidence to support a shorter duration of adjuvant treatment if it is decided that the patient needs to receive folfox or has t4 disease . across the whole trial population , scot met the criteria for non - inferiority with a difference in 3 year disease - free survival of 04% ( 95% ci 26 to 18 ) between 3 months and 6 months of treatment . 
while the study was underpowered , the 95% ci for the hr lies below the noninferiority boundary and the results are consistent with those of other individual studies by the idea group , taking into account how the duration effect depended on regimen and risk group . 
the concept that underpowered studies are more likely to produce false - positives ( ignoring the factor of publication bias , which does not apply to a large scale enterprise such as scot ) is disputed.29 as noted , the results differed with the ( non - randomised ) choice of chemotherapy regimens and we can recom mend a 3 month duration of adjuvant chemotherapy for patients with t13 , n1 disease ( 2677 [ 44% ] of the 6088 patients in the scot study ) if the patient is felt to be suitable for the capox regimen . 
we have not been able to show with any statistical certainty that 3 months of treatment was non - inferior to 6 months for patients receiving folfox , for whom there was an absolute increase in 3 year diseasefree survival with 6 months versus 3 months of treatment of 29% ( 95% ci 67 to 08 )  . despite the studys size , there are limitations to the reliability of conclusions that can be drawn for some subgroups . 
high - risk stage iii disease includes either t4 or n2 disease ( or both ) and this study has not been able to the effect of duration of adjuvant show whether chemotherapy is the same for t4 and n2 disease . 
the final decision on treatment duration and regimen used for each individual will depend on a careful discussion between the clinician and patient , taking into account the risk of recurrence , the likely absolute difference in diseasefree survival and risk of long - term toxicity , and the strength of evidence for that particular setting available both from scot and the wider idea analysis . scot is , to our knowledge , the largest single randomised study on the adjuvant treatment of colorectal cancer to date . 
 the study achieved its primary endpoint of showing that 3 months of oxaliplatin - containing adjuvant chemotherapy is non - inferior to 6 months of the same treatment in the overall trial population . 
tji , rsk , mps , ahar , ka , jm , cs , kab , ab , and jp wrote the manuscript and all authors contributed to the review of the manuscript . declaration of interests tji reports receiving honoraria from eli lilly ; serving on advisory boards for servier , roche , and celgene and receiving travel expenses from bayer and servier . 
jt reports support for being on advisory boards from amgen , bayer , boehringer ingelheim , celgene , chugai , lilly , msd , merck serono , novartis , pfizer , roche , sanofi , symphogen , taiho , and takeda . 
awa reports belonging to an institution involved in research that is funded by drug companies that provide the drugs for this study ; and has been coinvestigator in trials funded by roche which provided the capecitabine used in this study . 
all other authors declare no competing interests . acknowledgments this research was supported by the medical research council ( transferred to netsccefficacy and mechanism evaluation ; grant reference g0601705 ) , swedish cancer society , and cancer research uk vol 19 april 2018 articles core clinical trials unit funding ( funding ref : c6716 / a9894 )  . 
we also thank all international collaborative groups who led the trial in their countries ( the danish colorectal oncology group , vhio , agitg , and swedish society of gastrointestinal oncology ) , the independent trial data monitoring committee members ( hilary calvert [ chair ] , allan hackshaw , robin kennedy , and kees punt ) , and the trial steering committee members ( stan kaye , janet dunn , and alberto sobrero )  . corrections correction to lancet oncol 2015 ; 16 : 87 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the summary of this article ( published online first on dec 4 , 2014 ) , the interpretation section should have read olaparib plus paclitaxel and carboplatin followed by maintenance monotherapy signi cantly improved progression - free survival versus paclitaxel plus carboplatin alone , with the greatest clinical benefit in brca - mutated patients , and had an acceptable and manageable tolerability pro le . 
this correction has been made to the online version as of jan 29 , 2015 . vol 16 february 2015 articles lancet oncol 2014 ; 15 : 146068 published online november 11 , 2014 s1470 - 2045 ( 14 ) 71035 - 6 this publication has been corrected . 
we assessed e ectiveness of oral risedronate for prevention of reduction in bone mineral density ( bmd ) after 3 years of follow - up in a subset of patients in the ibis - ii trial . methods the double - blind ibis - ii trial recruited 3864 healthy , postmenopausal women at increased risk of breast cancer and randomly allocated them oral anastrozole ( 1 mg / day ) or matched placebo . 
1410 ( 36% ) postmenopausal women were then enrolled in a bone substudy and strati ed at baseline according to their lowest baseline t score at spine or femoral neck ( stratum i : t score at least 10 ; stratum ii : t score at least 25 but less than 10 ; stratum iii : t score less than 25 but greater than 40 )  . 
women in stratum ii were randomly assigned ( 1 : 1 ) to risedronate ( 35 mg / week ) or matched placebo by use of a block randomisation schedule via a web - based programme . 
the primary outcome of this per - protocol analysis ( done with all women with a baseline and 3 year dxa assessment ) was the e ect of risedronate versus placebo for osteopenic women in stratum ii randomly allocated to anastrozole ( 1 mg / day )  . 
secondary outcomes included e ect of anastrozole ( 1 mg / day ) on bmd in women not receiving risedronate ( strata i and ii ) and in osteoporotic women who were all treated with risedronate ( stratum iii )  . 
this trial is registered , number isrctn31488319 . findings between feb 2 , 2003 , and sept 30 , 2010 , 150 ( 58% ) of 260 women in stratum ii who had been randomly allocated to anastrozole and either risedronate or placebo had baseline and 3 year assessments . 
at the lumbar spine , 3 year mean bmd change for the 77 women receiving anastrozole / risedronate was 11% ( 95% ci 02 to 21 ) versus 26% ( 40 to 13 ) for the 73 women receiving anastrozole / placebo ( p < 00001 )  . 
for the total hip , 3 year mean bmd change for women receiving anastrozole / risedronate was 07% ( 16 to 02 ) versus 35% ( 46 to 23 ) for women receiving anastrozole / placebo ( p = 00001 )  . 
women not receiving risedronate in stratum i and ii who received anastrozole ( 310 women ) had a signi cant bmd decrease after 3 years of follow - up compared with women who received placebo ( 342 women ) at the lumbar spine ( 40% [ 45 to 34 ] vs 12% [ 17 to 07 ] , p < 00001 ) and total hip ( 40% [ 44 to 36 ] vs 18% [ 21 to 14 ] , p < 00001 )  . 
the 46 women allocated to anastrozole had a modest bmd increase of 12% ( 01 to 26 ) at the spine compared with a 39% ( 26 to 52 ) increase for the 60 women allocated to placebo ( p = 0006 )  . 
for the total hip , a small 03% ( 09 to 15 ) increase was noted for women allocated anastrozole compared with a 15% ( 05 to 25 ) increase for women allocated placebo , but the di erence was not signi cant ( p = 012 )  . 
the most common adverse event reported was arthralgia ( stratum i : 94 placebo and 114 anastrozole ; stratum ii : 39 placebo / placebo , 25 placebo / risedronate , 34 anastrozole / placebo , and 34 anastrozole / risedronate ; stratum iii : 21 placebo / risedronate , 17 anastrozole / risedronate )  . 
other adverse events included hot ushes , alopecia , abdominal pain , and back pain . interpretation risedronate counterbalances the e ect of anastrozole - induced bone loss in osteopenic and osteoporotic women and might be o ered in combination with anastrozole treatment to provide an improved riskbene t pro le . funding cancer research uk ( c569 / a5032 ) , national health and medical research council australia ( gnt300755 , gnt569213 ) , sano - aventis , and astrazeneca . introduction oestrogen has a major role in the regulation of skeletal homoeostasis , and therefore physiological decreases in oestrogen concentrations place postmenopausal women at high risk of osteoporosis ( low bone mineral density [ bmd ] )  . 
reduction in bmd in the rst 7 years after the menopause is 13% per year at the spine and 12% per year at the hip.1 bone loss can be treated or prevented 1460 vol 15 december 2014 articles see online for appendix with bisphosphonates , which increase bmd by inhibition of osteoclast - mediated bone resorption.2 , 3 this risk of bmd loss , and therefore fractures , is aggravated in postmenopausal women with breast cancer who are given an aromatase inhibitor as part of their treatment.4 , 5 aromatase inhibitors suppress oestrogen concentrations in postmenopausal women by inhibition of the conversion of androgens to oestrogens by the aromatase enzyme in soft tissues , especially fat . 
studies from large adjuvant trials show signi cant bmd decreases and higher fracture rates in women receiving aromatase inhibitors compared with women on tamoxifen.69 in the atac trial , anastrozole signi cantly decreased bmd at the lumbar spine ( 61% ) and total hip ( 72% ) after 5 years of follow - up , whereas a signi cant increase in bmd was noted with tamoxifen.6 similarly , the results from the big 198 con rmed a signi cant bmd loss and an increased fracture rate with letrozole compared with tamoxifen.10 most of the studies investigating the e ect of aromatase inhibitors on bone density have been done in postmenopausal women with early breast cancer receiving adjuvant tamoxifen as a comparison group . 
tamoxifen has a bene cial e ect on bmd and it is therefore di cult to determine the true e ect of aromatase inhibitors on bmd . two large prevention trials11 , 12 comparing an aromatase inhibitor with placebo in postmenopausal women at high risk of development of breast cancer have recently reported their main ndings . 
the ibis - ii trial12 compared anastrozole with placebo in postmenopausal women at high risk of development of breast cancer and noted a signi cant reduction in breast cancer with anastrozole . 
here we report the rst results of a perprotocol analysis of the placebo - controlled ibis - ii bone substudy , which assesses the e ect of 3 years of risedronate on bmd in postmenopausal women with healthy bone density , osteopenia , or osteoporosis . them methods study design and participants the ibis - ii trial recruited 3864 healthy , postmenopausal women at increased risk of breast cancer and randomly allocated to receive either 1 mg / day oral anastrozole or matching placebo.12 eligible women were o ered the opportunity to enter a bone substudy . 
study sites were those in ibis - ii that consented to do dual energy x - ray absorptiometry ( dxa ) scans as part of the elsewhere.12 detail follow - up trial ( appendix ) and deemed postmenopausal when they were aged 60 years or older ; had had a bilateral oophorectomy ; were younger than 60 years , but had a uterus and amenorrhoea for at least 12 months ; or were younger than 60 years , had no uterus , and had a concentration of follicle stimulating hormone of greater than 30 iu / l . 
exclusion criteria for the main trial included premenopausal status , any previous diagnosis of invasive cancers , present use of selective oestrogen receptor modulators for more than 6 months , intention therapy , to continue with hormone - replacement evidence of severe osteoporosis ( t score less than 40 ) , and lack of physiological or psychological tness . 
finally , osteoporotic women with a t score of less than 25 but greater than 40 or those with one to two low trauma fragility fractures ( as assessed by spinal radiographs ) were entered into stratum iii . 
 finally , women who had a t score of less than 40 and those with more than two low trauma fractures , were excluded from the bone substudy and referred for further management . 
the trial was approved by the uk north west multicentre research ethics committee and was done in accordance with the declaration of helsinki , under the principles of good clinical practice . 
 participants provided written informed consent . radiographs within regularly randomisation and masking women in stratum ii were randomly assigned to receive risedronate ( 35 mg / week ) or matched placebo . 
 all ibis - ii personnel , participants , and clinicians were masked to treatment allocation and only the ibis - ii trial statistician ( is ) had access to unmasked data . procedures all women entering the main ibis - ii study were required to have a dxa scan before study entry for strati cation vol 15 december 2014 1461 articles and exclusion purposes . 
in the bone substudy , bmd was further assessed by follow - up dxa scans at the lumbar spine and total hip at 12 , 36 , and 60 months . 
women who had a bmd loss of 6% or more at the 12 month visit were required to have a safety dxa scan at 24 months of follow - up . 
similarly , women with a bmd loss of more than 10% at 36 months had a safety scan at 48 months , and those with a bmd loss of more than 16% at the 60 months visit had an interval scan at 72 months . we calculated t scores with either the lunar14 or hologic15 manufacturers reference ranges for the lumbar spine ( l1 to l4 ) and the national health and nutrition examination survey ( nhanes ) iii reference range for the femoral neck region.16 all baseline and follow - up dxa scans were reviewed centrally by two clinical scientists with expertise in bone densitometry ( gmb and rp ) to ensure quality assurance . 
regular phantom reports from all participating centres were reviewed and investigators were requested to use the same dxa machine whenever possible throughout the study . women in stratum i were monitored only . 
women in strata ii and iii were advised to take their allocated risedronate or received oral matching placebo in an upright position upon waking in the morning on an empty stomach , and not to consume anything apart from water within the next 30 min to minimise risk of inactivation of the drug or oesophageal irritation . 
women were allowed to have a dose reduction ( ie , alternate weeks ) or go on treatment holiday from risedronate if they developed severe adverse events potentially related to the trial medication . for biomarker analyses , a 10 ml urine sample from the second void was collected at baseline and 12 months . 
ntx was expressed as a ratio to creatinine ( nmol bone collagen equivalent : mmol creatinine ) and the interassay coe cient of variation for creatinine was 18% . outcomes the primary objective of this analysis was to compare the e ect of risedronate versus placebo on bmd between baseline and 3 years at both the lumbar spine and total hip in women taking anastrozole in stratum ii . 
women ceased participation in the bone substudy if one of the following events occurred : withdrawal from main study , development of breast cancer , death , and if rapid bone loss occurred . 
the sponsor or funding bodies of this study had no role in study design , collection of data or material , data analysis , interpretation of the data , or writing of the manuscript . 
is , jc , and re had nal responsibility to submit the report for publication . results between feb 2 , 2003 , and sept 30 , 2010 , we enrolled 1410 postmenopausal women into the bone substudy with a median follow - up of 30 years ( iqr 295309 ; gure 1 )  . 
no further dxa scans were done for women who withdrew from the main ibis - ii study ( 199 in stratum i , 127 in stratum ii , 32 in stratum iii ) , developed breast cancer ( 28 in stratum i , 12 in stratum ii , four in stratum iii ) , or died ( nine in stratum i , four in stratum ii , three in stratum iii ; no deaths were treatment related ) , and these women were excluded from the analysis ( gure 1 )  . 
256 ( 72% ) of the 358 women who withdrew from the main ibis - ii study did so before the 12 month follow - up visit ( 126 in stratum i , 112 in stratum ii , 18 in stratum iii ) and therefore were excluded from this analysis . 
13 of these women did not continue with the trial medication and were therefore excluded from this analysis ( eight in stratum i , ve in stratum ii ; gure 1 )  . 
hrt = hormone - replacement therapy . table 1 : baseline characteristics for all postmenopausal women with a baseline and 36 month dxa scan available vol 15 december 2014 1463 articles 05 10 15 20 25 30 35 40 45 50 05 10 11% 26% 12% 40% 39% 12% a lumbar spine anastrozole / risedronate anastrozole / placebo b total hip anastrozole / risedronate anastrozole / placebo c lumbar spine baseline 12 months baseline 12 months 36 months d total hip anastrozole placebo anastrozole placebo baseline 12 months e lumbar spine 36 months baseline 12 months f total hip 36 months placebo / risedronate anastrozole / risedronate baseline 12 months anastrozole / risedronate placebo / risedronate 36 months baseline 12 months 36 months figure 2 : bone mineral density changes at lumbar spine and total hip at each follow - up visit ( ab ) women in stratum ii receiving anastrozole who were randomly allocated to either risedronate or placebo . 
 the baseline characteristics between women all receiving anastrozole and randomly allocated to risedronate versus placebo were evenly distributed and we noted no major 07% 35% 36 months 18% 40% 15% 03% in baseline characteristics . 
similarly , for women in stratum i and ii not receiving risedronate but randomly allocated to anastrozole versus placebo , we noted no substantial di erences stratum iii who were randomly allocated to receive placebo were older than were those randomly allocated to anastrozole ( p = 0043 ; table 1 )  . 
no major di erences between these two groups were noted for all baseline characteristics ( data not shown )  . in the analysis of women in stratum ii who had all received anastrozole and either risedronate or placebo , 150 ( 58% ) of 260 women had baseline and 36 month dxa scans available for analysis ( 77 anastrozole / risedronate vs 73 anastrozole / placebo )  . 
women randomly allocated to anastrozole and receiving risedronate had a mean bmd increase of 11% ( 95% ci 02 to 21 ) at the lumbar spine after 36 months follow - up compared with a mean decrease of 26% ( 40 to 13 ) in those not receiving risedronate ( p < 00001 ; gure 2 , appendix )  . 
although bmd for the total hip decreased by only 07% ( 95% ci 16 to 02 ) for women on anastrozole and risedronate after 36 months follow - up , the di erence was signi cant compared with women on only anastrozole , who had a decrease of 35% ( 46 to 23 ; p = 00001 ; gure 2 , appendix )  . in the analysis of women in stratum i and ii who were not randomly allocated to risedronate and received only anastrozole or placebo , 652 ( 65% ) of 1008 had baseline and 36 month dxa scans . 
 however , we noted a signi cantly larger decrease at the lumbar spine or total hip for women randomly allocated to anastrozole compared with placebo ( lumbar spine : 40% [ 95% ci 45 to 34 ] for anastrozole vs 12% [ 17 to 07 ] for placebo , p < 00001 ; total hip : 40% [ 44 to 36 ] for anastrozole vs 18% [ 21 to 14 ] for placebo ; p = 00001 ; gure 2 , appendix )  . in the analysis of women in stratum iii who had all received risedronate and either anastrozole or placebo , 106 ( 71% ) of 149 women had baseline and 36 month dxa scans . 
we noted the largest increase in mean percentage bmd at the lumbar spine for women randomly allocated to placebo ( 39% increase [ 95% ci 26 to 52 ] ) whereas we noted a smaller increase for ( 12% women randomly allocated increase [ 009 to 26 ] ; p = 0006 ; gure 2 , appendix )  . 
in stratum i , we noted a signi cant median increase of almost 9% after 12 months in women randomly allocated to anastrozole , but no di erence with placebo ( table 2 )  . 
women in stratum ii who were randomly allocated to anastrozole but not to risedronate had a signi cant median increase in ntx to creatinine ratio of almost 12% by 12 months of follow - up whereas those randomly allocated to placebo did not vol 15 december 2014 1465 articles panel : research in context systematic review we searched pubmed for randomly allocated trials in the preventive setting published in english before may 30 , 2014 , that investigated a bisphosphonate in women at high risk of breast cancer treated with an aromatase inhibitor . 
we identi ed no other breast cancer prevention trials investigating the e ect of a bisphosphonate in combination with an aromatase inhibitor in postmenopausal women at high risk of development of the disease . 
we identi ed one other prevention trial13 in postmenopausal women comparing exemestane with placebo that reported on bone mineral density changes in this study group , but did not investigate the use of a bisphosphonate . interpretation results from our trial provide the rst evidence that risedronate prevents anastrozoleinduced bone mineral density loss in postmenopausal women at high risk of development of breast cancer with osteopenia or osteoporosis . 
because aromatase inhibitors have emerged as a treatment option for the reduction of breast cancer risk for postmenopausal women , the concomitant use of a bisphosphonate is inevitable in this setting . 
however , long - term follow - up is required for the assessment of risedronate on fracture risk and for overall bone mineral density changes over the course of 5 years of anastrozole use . show a signi cant change in this marker ( table 2 )  . 
by contrast , women who were randomly allocated to receive risedronate in stratum ii had signi cant median decreases in ntx to creatinine ratios after 12 months of follow - up , irrespective of main treatment allocation ( table 2 )  . 
the di erences in ntx to creatinine ratio between randomisation groups were signi cant after 12 months of follow - up in stratum ii ( p < 00001 )  . 
we noted decreases in ntx to creatinine concentrations were observed for both treatment groups for women in stratum iii , but the di erence was not signi cant ( table 2 )  . 639 ( 45% ) of 1410 women in the ibis - ii bone substudy had adverse events ( table 3 )  . 
incidence did not di er between treatment allocations within each stratu no serious adverse events , such as osteonecrosis of the jaw or serious gastrointestinal problems , were reported after 3 years of follow - up with risedronate . 
only 85 women had a treatment interruption from risedronate between baseline and 36 months ( median 3 weeks [ iqr 25 ] ; 65 women in stratum ii and 20 women in stratum iii )  . 
 by 36 months of follow - up , two women in stratum i ( one anastrozole , one placebo ) and 23 women in stratum ii ( six placebo / placebo , ten anastrozole / placebo , and ve anastrozole / risedronate ) developed osteoporosis and subsequently stopped trial medication to start open - label bisphosphonates . 
overall , 128 fractures were reported by 109 women in the bone substudy ( 44 women in stratum i , 51 women in stratum ii , and 14 women in stratum iii )  . 
57 ( 8% ) of 711 women randomly allocated to anastrozole reported at least one fracture compared with 52 ( 7% ) of 699 in the placebo two placebo / risedronate , group . 
the incidence rate for fractures in the anastrozole arm was 137 per 1000 woman - years compared with 126 per 1000 woman - years in the placebo arm ( p = 070 )  . 
 the number of fractures is too small at present to report stratum speci c data , and further follow - up is needed . discussion the mean percentage bmd loss in women on placebo in our study is similar to that reported in the overall population of similar age.17 the ibis - ii results con rm that 3 years of anastrozole decreases bmd at the lumbar spine or total hip in healthy postmenopausal women , as previously reported ( panel ) .13 more importantly , our results show that risedronate counterbalances bmd loss induced by anastrozole in women with osteopenia or osteoporosis . 
similar ndings have been reported by two smaller studies in patients with breast cancer.18 , 19 both trials showed that the addition of a bisphosphonate normalises bone turnover in such patients receiving anastrozole after 2 years . 
risedronate was well tolerated and no serious adverse events , such as osteonecrosis of the jaw or serious gastrointestinal problems , were reported after 3 years of follow - up . bisphosphonates are well established drugs for the prevention of bone loss and reduction of fractures in postmenopausal women and men with osteoporosis.2 , 20 , 21 oral and intravenous bisphosphonates signi cantly reduce the incidence of vertebral and non - vertebral fractures.22 in the adjuvant setting , anastrozole , letrozole , and exemestane have all been assessed in postmenopausal women with early breast cancer.2326 these trials have all shown signi cant bmd loss with these drugs , but have in common that the comparator was tamoxifen , which has been shown to have a bene cial e ect on bone.6 , 7 , 9 zoledronic acid can prevent bmd loss induced by letrozole or anastrozole in postmenopausal women with breast cancer.2729 a small study assessing risedronate in women with breast cancer receiving anastrozole showed that this drug was e ective in preventing anastrozole induced bone loss.30 in a large review , the european guidelines31 for the management of aromatase inhibitor the use of induced bone bisphosphonates for postmenopausal women with breast cancer is safe and that these drugs are e ective in the prevention of bmd loss because of endocrine therapy . that treatment of osteoporosis loss concluded in the preventive setting , the bone substudy of the map.3 trial , 13 which compared exemestane with placebo , recently reported their results on bone density changes in a subgroup of women . 
however , they also reported on bmd changes at the lumbar spine and total hip by dxa as a secondary objective , and reported that women 1466 vol 15 december 2014 articles randomly allocated to exemestane had a signi cant decrease in bmd at all sites compared with placebo after 2 years of follow - up . 
other studies , in the adjuvant setting , have also shown that aromatase inhibitors are associated with higher concentrations of bone resorption makers.7 , 8 , 32 by contrast , those women who were randomly allocated to risedronate in stratum ii or osteoporotic women ( stratum iii ) receiving risedronate showed signi cant decreases in ntx to creatinine ratio by 12 months of follow - up . strengths of our analysis include an overall large sample size ( 1410 women ) , with a large proportion of women with osteopenia , long follow - up of 3 years , and a population that came from a large prevention trial with excellent clinical records . 
furthermore , this trial is the rst time that a bisphosphonate has been compared with a placebo in healthy postmenopausal woman at risk of development of breast cancer who are taking anastrozole as a preventive drug . 
this analysis reports on the 3 year bmd changes , but we will be able to present results after 5 years of treatment and are in the process of obtaining a dxa scan 2 years after treatment cessation to investigate whether bmd loss induced by anastrozole is regained . included limitations of our study include the incomplete set of bmd data at 36 months ( 903 [ 64% ] of 1410 women )  . 
this nding is mainly attributable to withdrawal from the main ibis - ii study in the rst 3 years and therefore our results might not be representative for the whole study population . 
dxa is the standard clinical technique for skeletal assessment of bmd changes and fracture risk , but does not take into account bone structure and micro architecture of the bone . 
bone structure , especially cortical structure of the bone , probably plays an important part in determination of bone strength , 13 , 33 , 34 but assessment of these bone structure changes was not possible . to our knowledge , this analysis was the rst to investigate the e ect of risedronate on anastrozoleinduced bone loss in healthy postmenopausal women in a placebo - controlled trial . 
nevertheless , loss contributors is , ss , jc , gmb , rp , rc , md , jff , ah , and re designed the study and all authors interpreted the data . 
all authors reviewed the report and approved the nal version . declaration of interests is , ss , fg , gmb , rp , jff , ah , and re declare no competing interests . 
 acknowledgments this study was funded in part by cancer research uk ( c569 / a5032 ) and national health and medical research council australia ( gnt300755 , gnt569213 ) , in part by sano - aventis and astrazeneca , who also provided anastrozole and matching placebo . 
md acknowledges support from the royal marsden national cancer research institute biomedical research centre . for the jamia study on medication - related clinical decision support alert overrides see j am med inform assoc 2017 ; published oct 27 . 
this somewhat ironic paradoxin which more drugs are being pushed through to the market , only to be bottlenecked through a system that relies on an automated system of prescriptionhas potentially conflicting consequences . 
on the one hand , physicians are encouraged to offer a variety of choice to the patient , but , on the other , they are exhausted by what is commonly called alert fatigue , in which their clinical expertise is overshadowed by an automatic system that apparently knows better . 
although the jamia study found that a large proportion of physicians overrode warnings because evidence suggested that the patient would not suffer from any adverse reactions , the situation does call into question whether a reliance on digital systems , such as those used for e - prescribing , underminesor at least challengesa level of expertise that can only be gained from the day - to - day experience of a doctor . 
from data analytics to artificial intelligence , to predictive modelling and machine learning , we are now seeing these systems being incorporated into all aspects of health , including those found in oncology . 
although big data offers the promise of easing workflows , ensuring treatment adherence according to guidelines , the analysis of large datasets , maintenance of a centralised records system , improving diagnostic accuracy , and monitoring disease or drug safety surveillanceall of which could be hugely beneficial for the future of health careclearly a delicate balance is needed when integrating those promises into the clinical decision - making process . 
in the case of detecting malignancies , it is now becoming increasingly difficult to refute that big data can help identify highrisk populations with ever - improving accuracy , observe trends in cancer incidence , and predict cancer rates long before such patterns can be detected by those methods used in conventional screening protocols . 
moreover , integrating data into health systems can have substantial financial advantages by reimbursement charges and potentially decreasing the overall cost of care . improving however , these advantages need to be offset against the potential difficulties that such new technological advances might bring . 
automated workflows need to be balanced against ease of use and delivered in a way that doesnt encumber workflows to those who are already under severe pressure and time constrained ; data analysis should be promoted in ways that help facilitate training and safeguard against otherwise unknown sideeffects without fostering an attitude that encourages laziness or poor judgement ; and , most crucially , we need to ensure that patients data remain private and secure , while enabling its aggregation in a de - identified manner to help support analytical tools that can help benefit the wider population . 
although new technologies might provide us with the tools and resources to fight health inequity , increase access , identify new targets for difficult - to - treat diseases , and help improve public health , our enthusiasm must be tempered against the always present reality of a doctorpatient relationship in which experience will always be key . despite the potential dangers , digital clinical decision tools are undeniably helpfulthey not only ensure that evidence - based medicine is practised , but guarantee a more consistent service that can be delivered to all by enforcing an approach that is based on guidelines . 
 but , just like any skill , a physicians craft must be developed and honed through practice ; it can only ever be augmented by digital health , not perfected by it . 
the art of medicine is based on judgement , as well as data , and the balancing of these two somewhat conflicting modes of medicine will be a difficult task in years to come . 
in the meantime , we must promote both schools of thought and not champion one over the other , to ensure that we provide patients with the best possible medical judgement . 
 nivolumab monotherapy in recurrent metastatic urothelial carcinoma ( checkmate 032 ) : a multicentre , openlabel , two - stage , multi - arm , phase 1 / 2 trial . 
lancet oncol 2016 ; 17 : 159098 in this article , the declaration of interests should read psh has received fees for advisory board participation for jounce and kite ; fees for consultancy from jounce , kite , bristol - myers squibb , astrazeneca , and amgen ; and stock or stock options from jounce and kite . 
eca reports research grants and / or financial support from boehringer ingelheim , roche / genentech , bristol - myers squibb , novartis , psioxus , nanobiotix janssen , abbvie , pharmamar , puma , sanofi , lilly , pfizer , merck , nektar , amcure , amgen , astrazeneca , principia , bayer , cytomx , h3 , incyte , kura , loxo , macrogenics , menarini , merck serono , merus , millenium , rigontec , tahio , and beugene tesaro ; consultancy fees from janssen - cilag , alkermes ( and travel expenses ) , seattle genetics , pierre fabre , cerulean pharma , eusa , celgene , novartis ( speakers bureau ) , nanobiotix , psioxus therapeutics , abbvie , astrazeneca , guidepoint global , roche / genentech ( and travel expeneses ) , glg , pfizer , servier , amcure , and boehringer ingelheim ; ownership from start ( leadership ) , oncoarts associated and international cancer consultants ; and employment from start and hm hospitals group ( honoraria ) and president and founder of npo foundation intheos ( investigational therapeutics oncological sciences ) , outside the submitted work . 
fdb has received consultancy fees from tiziana life sciences , bristol - myers squibb , msd , servier , eli lilly , merck serono , glaxosmithkline , and novartis , and speaker fees from bristol - myers squibb , eli lilly , roche , and accmed . 
mm has received consultancy fees from etubics and boehringer ingelheim , and speaker fees from genentech , novartis , sanofi , regeneron , lexicon , ipsen , onyx , bayer , taiho , merrimack , and celgene . 
 dj has received consulting fees from definiens , f hoffmann - la roche , curevac , roche pharma , novartis pharma , and novartis oncologynovartis farma , outside the submitted work ; and has a patent issued for intellectual property of infiltrating t - cell density predicting outcome . 
 ech has received grants from bristolmyers squibb and consultancy fees for advisory board participation from emd serono , taiho , bayer , advaxis , amgen , lilly , and castle biosciences . 
jer has received grants for study conduct from novartis ; funds for clinical trial conduct from astellas , seattle genetics , bayer , astrazeneca , mirati therapeutics , oncogenex , and roche / genentech ; has received consultancy fees from roche / genentech , astrazeneca , eli lilly , astellas , seattle genetics , bristol - myers squibb , merck , emd - serono , adicet bio , western oncolytics , pharmacyclics , sensei biotherapeutics , bayer , bioclin therapeutics , qed therapeutics , mirati therapeutics , fortress biotech , inovio ; has gritstone oncology , received honoraria from bristol - myers squibb and chugai ; has held stock in illumina and merck . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2017 ; 18 : 90416 baselga j , im s - a , iwata h , et al . 
buparlisib plus fulvestrant versus placebo plus fulvestrant in postmenopausal , hormone receptor - positive , her2 - negative , advanced breast cancer ( belle - 2 ) : a randomised , double - blind , placebocontrolled , phase 3 trial . 
lancet oncol 2017 ; 18 : 90416in this article , the declaration of interests should read jb has received reimbursement for travel , and advisory board and consulting fees from novartis , during the conduct of the study ; has received personal fees and held stock as a member of the board of directors from aura biosciences ; has received personal fees as a member of the advisory board and held stock as a founder of northern biologics ( f / k / a mosaic biomedicals ) ; has received personal fees and held stock as a member of the board of directors from infinity pharmaceuticals ; held stock as a member of the advisory board from apogen biotechnologies ; has received personal fees and held stock as a member of the advisory board from pmv pharma ; has received personal fees and held stock as a member of the advisory board from juno therapeutics ; has received personal fees and held stock as co - founder from tango ( f / k / a synthetic lethal ) ; has received personal fees and held stock as a member of the scientific advisory board and the board of directors from grail ; has received personal fees and held stock as a member of board of directors from varian medical systems ; held stock as a member of board of directors from foghorn therapeutics ; has received reimbursement for travel , e71 vol 20 february 2019 corrections and advisory board and consulting fees from eli lilly ; has received personal fees and held stock as a member of advisory board from seragon ; has received reimbursement for travel and in - kind items and services from roche , outside the submitted work . 
 s - ai reports grant support from astrazeneca and advisory consultant roles for astrazeneca , eisai , novartis , pfizer , roche / genentech and spectrum , outside the submitted work . 
hi reports grant support and personal fees from novartis during the conduct of the study ; hi was also an uncompensated member of the steering committee of this study ; hi has received personal fees in the form of honoraria and consulting fees from astrazeneca , pfizer , lilly , daiichi - sankyo , and f hoffman la - roche via chugai , outside the submitted work . 
jc reports personal fees from novartis , celgene , cellestia , astrazeneca , biothera pharmaceuticals , merus , seattle genetics , daiichi sankyo , erytech , pfizer , eisai , and samsung ; has received stock , patents , and intellectual property from medsir ; has received personal fees and research funding to his institution from roche , outside the submitted work . 
mdls reports personal fees in the form of speakers honoraria and advisory board honoraria from novartis , roche , lilly , pfizer , eisai , ipsen , and teva , outside the submitted work . 
cla reports personal fees for participation in a steering committee for the clinical trial from novartis , during the conduct of the study ; and personal fees for an expert advisory role from eli lilly , astrazeneca , genentech , millennium , celgene , pfizer , radius , and merck , outside the submitted work . 
sc also reports personal fees received in the form of honoraria for advisory boards from novartis , hoffmann laroche , pfizer , astrazeneca , and genomic health ; and institutional research support from novartis , hoffmann laroche , pfizer , astrazeneca , genomic health , genentech , merck , and bms , outside the submitted work . 
she also reports grant support from ambryx , amgen , bayer , obi pharma , bimarin , cascadian , daiichi sankyo , dignitana , genentech , gsk , lilly , macrogenics , medivation , merrimack , novartis , pfizer , pieris , puma , roche , seattle genetics , and travel support from lilly , novartis , and obi pharma , outside the submitted work . 
 reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
pv reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 15964 wolf a , naylor k , tam m , et al . 
these corrections have been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 17980 massari f , di nunno v . 
lancet oncol 2019 ; 20 ; 17980in this comment , the following sentence has been edited from time to deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab to risk of deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab . 
 the decision was based on interim results of the phase 3 bellini trial , which showed an increased risk of death for patients who were treated with venetoclax and bortezomib compared with placebo ( 41 [ 211% ] deaths in 194 patients in the venetoclax group vs 11 [ 113% ] of 97 in the control group ; hazard ratio 203 [ 95% ci 104394 ] )  . 
the fdas decision raises important questions with respect to the safety of new treatments , their justification in disease settings with existing approved drugs with similar efficacy , and a growing trend in the way innovative therapies are pushed through clinical trials at breakneck speed . in the case of multiple myeloma , drug innovation is at an all - time high . 
these early decisions certainly encourage pharmaceutical innovation and facilitate patient access to new drugs , but they also reflect a worrying trend in which regulators are arguably approving drugs too soon on the basis of early - stage results or uncontrolled phase 2 data for which the efficacy or harm of the new intervention is still too unpredictable . 
additionally , regulators should be more cautious when drugs skip early - phase testing and move straight to a phase 3 trial for diseases in which there are already proven therapies . 
in the case of the bellini trial , researchers justified the investigation of venetoclax for multiple myeloma treatment based on encouraging results of the drug in chronic lymphocytic leukaemia and acute myeloid leukaemia , each of which led to breakthrough designations by the fda . 
but decisions such as these show that different diseases will ultimately respond differently to treatment , even if they show similar disease characteristics or are based on similar trial populations . 
being aware of the ultimate risks and benefits involved is a necessary first step to ensure clinical trials are being done to generate the best possible evidence needed , not to see whether the drug is effective in as many malignancies as possible to maximise commercial opportunity . indeed , involved if the risks in a recent study in enrolling patients experimental clinical trials were apportioned the correct amount of caution , then unwarranted harms such as those seen in the bellini trial might be avoided . 
 jama internal medicine , researchers found that doctors conversations with families about care for critically ill patients failed to take the time to explain the benefits and harms of treatment options and failed to address patients values and preferences . 
when patient preference is so central a concern to deliver optimal cancer care , it is crucial that those responsible for the advent of new trialssuch as funders , ethics approval committees , regulators , doctors , and investigators themselvesaccurately communicate the dangers involved so that overtly risky or futile trials are avoided , whilst still encouraging various treatment avenues that are available to the patient . somehow , the unbridled promotion of new treatments driven by industry - sponsored research , research pressures , and treatment enthusiasm , has fostered a culture in which the promise of miraculous important questions cures overshadows more surrounding the realities of the risks and harms of treatment , the evidence base used to promote their use , and the actual need for new treatment options to be available in any given setting . 
moreover , both regulators should be any and clinicians have a duty of care to ensure risks are communicated as fully and as transparently as possible , and thus ensure that patient care , best practice , and best evidence ultimately comes first . 
 the lancet oncology vol 20 may 2019 editorial comment published online october 8 , 2014 s1470 - 2045 ( 14 ) 70491 - 7 see articles page 1361 well as further overall survival follow - up , would have substantially changed the results . 
such modelling would inform our acceptance of these data as well as the design of any future trials . whether the data from imelda are deemed practice changing or hypothesis generating , imelda has reopened important debates about the use bevacizumab and maintenance chemotherapy that will potentially change the treatment of metastatic breast cancer . adam brufsky university of pittsburgh , 300 halket street , suite 4628 , pittsburgh , pa 15241 , usa brufskyam@upmc.edu i have received consulting fees and research support from roche . 1 miller k , wang m , gralow j , et al . 
ribbon - 1 : randomized , double - blind , placebo - controlled , phase iii trial of chemotherapy with or without bevacizumab for rst - line treatment of human epidermal growth factor receptor 2 - negative locally recurrent or metastatic breast cancer . 
phase iii study of bevacizumab plus docetaxel compared with placebo plus docetaxel for the rst - line treatment of human epidermal growth factor receptor 2 - negative metastatic breast cancer . 
bevacizumab plus paclitaxel versus bevacizumab plus capecitabine as rst - line treatment for her2 - negative metastatic breast cancer : interim e cacy results of the randomised , open - label , non - inferiority , phase 3 turandot trial . 
 brufsky am , hurvitz s , perez e , et al ; ribbon - 2 : a randomized , double - blind , placebo - controlled , phase iii trial evaluating the e cacy and safety of bevacizumab in combination with chemotherapy for secondline treatment of human epidermal growth factor receptor 2 - negative metastatic breast cancer . 
phase iii , multicenter , randomized trial of maintenance chemotherapy versus observation in patients with metastatic breast cancer after achieving disease control with six cycles of gemcitabine plus paclitaxel as rst - line chemotherapy : kcsg - br07 - 02 . 
maintenance capecitabine and bevacizumab versus bevacizumab alone after initial rst - line bevacizumab and docetaxel for patients with her2 - negative metastatic breast cancer ( imelda ) : a randomised , open - label , phase 3 trial . 
semin oncol 2006 ; 33 ( 5 suppl 10 ) : 17 . surgery or topical therapy for vulval intraepithelial neoplasia squamous the incidence of intraepithelial neoplasia of the vulva has been rising for the past few decades , 1 possibly due to an increase of human papillomavirus ( hpv ) intraepithelial associated high - grade lesions , particularly in young women . 
high - grade squamous intraepithelial lesions ( vulval intraepithelial neoplasia grade 23 ) are typically multifocal and judged to cause more than 90% of all diagnosed cases of vulval intraepithelial neoplasia . 
by contrast with low - grade squamous intraepithelial lesions ( vulval intraepithelial neoplasia grade 12 ) , which are usually self - limiting with a high rate of spontaneous regression , highgrade squamous intraepithelial lesions can progress to invasive carcinoma and are , therefore , de ned as precancerous lesions . 
untreated patients have a 69% risk of progression to vulval carcinoma.2 , 3 di erentiated disease is another type of high - grade vulval intraepithelial neoplasia : it is less frequently diagnosed than high - grade squamous intraepithelial lesions ( diagnosed in 210% of cases ) , lesions are usually hpv - negative , and the disease is typically associated with vulval lichen sclerosus.4 although hpv - negative lesions are widely accepted to have greater potential to progress to invasive disease than other lesion types ( up to 30% higher ) , 3 no predictive markers are known for the progressive potential of di erent types of vulval intraepithelial neoplasia . 
 treatment for high - grade squamous standard intraepithelial lesions is surgery , either cold - knife resection or laser vaporisation , which can result in substantial morbidity and potential psychosexual dysfunction.5 the main argument for cold - knife resection over the otherwise less invasive surgical technique of laser vaporisation is possible histological detection of occult vulvar carcinoma within a preinvasive lesion . 
however , in a systematic review , occult invasive disease was noted in 3% of patients , who had mostly microinvasive cancers.2 this relatively low risk shifts the focus of management of high - grade squamous intraepithelial lesions away from detection vol 15 november 2014 1287 comment of invasive cancer and towards symptom control and prevention of carcinogenesis . 
 2030% of patients who undergo a surgical intervention have recurrence of disease , irrespective of the treatment modality , 6 and neither cold - knife nor laser surgery can treat e ectively the underlying cause of most high - grade squamous intraepithelial lesions hpv infection.7 topical treatment with the immuneis an e ective alternative to modi er surgery , with a durable complete response reported in 35% of patients and a partial response in 38%.8 sidee ects of imiquimod are pain and discomfort in the treatment area , fatigue , and headache . 
therefore , alternative topical regimens with favourable toxic - e ect pro les are needed . imiquimod for treatment of vulval in the lancet oncology , amanda tristram and colleagues present ndings of a randomised phase 2 trial of topical imiquimod and the nucleotide analogue cidofovir intraepithelial neoplasia grade 3.9 good responses were recorded with both drugs , with complete responses noted in 41 ( 46% ) of 89 patients allocated cidofovir and in 42 ( 46% ) of 91 patients assigned imiquimod . 
toxic e ects of grade 3 or higher were noted in 39 ( 46% ) of 84 patients treated with imiquimod and in 31 ( 37% ) of 84 patients treated with cidofovir . 
 the therapeutic e ect of cidofovir seems to be both antiviral and cytotoxic , which could potentially bene t immunocompromised patients ; a reasonable response to cidofovir has been reported in hiv - positive patients with anal and vulvar high - grade squamous lesions.10 the primary endpoint of intraepithelial tristram and colleagues study was a complete response 6 weeks after treatment ; since further follow - up is still ongoing , the long - term e cacy of cidofovir remains to be proven . in the future , topical treatments could evolve to become the treatment of choice for people with highgrade squamous intraepithelial lesions , with coldknife resection and laser vaporisation reserved for patients not responding to initial treatment . 
activity , safety , and feasibility of cidofovir and imiquimod for treatment of vulval intraepithelial neoplasia ( rt3vin ) : a multicentre , open - label , randomised , phase 2 trial . 
aids 2013 ; 27 : 54551 . 1288 vol 15 november 2014 corrections correction to lancet oncol 2011 ; 12 : 1051 correction to lancet oncol 2015 ; 16 : 634 , 637 histological sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
 independent lancet oncol 2011 ; 12 : 104552 in the discussion of this article , the second sentence of the fth paragraph should read the proportion of patients a ected by grade 34 fatigue in this study ( 7% ) is similar to that reported for trabectedin ( 78% ) or gemcitabine with docetaxel ( 16% ) .12 , 13 this correction has been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 388 kang hj , loftus s , taylor a , dicristina c , green s , zwaan cm . 
 lancet oncol 2015 ; 16 : 38594 in table 2 of the article , the dose ( mg / kg ) of dexamethasone used in the aprepitant group should read 008 ( 002019 )  . 
this correction has been made to the online version as of aug 31 , 2015 . of medical a airs , from april , 2006 , to december , 2012 , during the design and conduct of the stars trial . 
these cor rections have been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 96778 valle jw , wasan h , lopes a , et al . 
lancet oncol 2015 ; 16 : 96778 in gure 3 of the appendix of this article , parts a and b were mislabelled ; part a shows overall survival data and part b shows progression - free survival data . 
open access article distributed under the terms of cc by . correction to lancet oncol 2015 ; 16 : 1127 moss sm , wale c , smith r , evans a , cuckle h , duffy sw . 
lancet oncol 2015 ; 16 : 112332in the fourth paragraph of the results section of this article , the absolute mortality reduction in the intervention group should read 003 per 1000 womenyears . 
this correction has been made to the online version as of aug 31 , 2015 and the printed version is correct . chang jy , senan s , paul ma , et al . 
lancet oncol 2015 ; 16 : 63037in this article , the role of the funding source should read : this analysis was designed by the principal and coprincipal investigators of both trials . 
for the stars protocol , accuray speci ed that the cyberknife platform was the sole platform to be used for the study , but did not have a role in any other aspect of the study design . 
beyond providing nancial support , neither funder was in accessing involved the raw data , collection , analysis , or interpretation of the data , or writing of the report . 
dab has received grants from accuray , and is the co - owner of berry consultants , a company that designs clinical trials for pharmaceutical and medical device companies , and international healthcare consortia . 
od was an employee of accuray , as senior vice - president responses vol 16 september 2015 e427 addendum to lancet oncol 2005 ; 6 : 75156 hckel m , horn l - c , fritsch the h . 
association between mesenchymal compartment of uterovaginal organogenesis and local tumour spread in stage ibiib cervical carcinoma : a prospective study lancet oncol 2005 ; 6 : 75156the supplemental video accompanying this article has been updated . 
this addendum has been added to the online version as of june 29 , 2018 . correction to lancet oncol 2018 ; 19 : 5164 patel mr , ellerton j , infante jr , et al . 
in figure 4a , the first subheading in the inset on the graph should have referred to median progression - free survival in weeks , not months , and the second subheading in the inset on the graph should have read 6 - month pfs , rate ( 95% ci )  . 
 in the results section , last paragraph , the following sentence should have read as follows : of which infusionrelated reaction , diarrhoea , and pneumonitis were reported in more than one patient ( three , two , and two patients , respectively )  . 
also in the last paragraph of the results section , localised oedema should not have been included in the list of reasons for patients who permanently discontinued avelumab due to a treatment - related adverse event . 
 these corrections have been made to the online version as of june 29 , 2018 . correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
 lancet oncol 2017 ; 18 : 106175 in this article , the following sentence about the safety results in the findings section of the summary should have read : commonly reported treatment - related adverse events were diar rhoea ( 41 [ 16% ] ) , fatigue ( 37 [ 15% ] ) , elevated aspartate aminotrans ferase ( 33 [ 13% ] ) , and elevated alanine aminotrans ferase ( 24 [ 10% ] )  . 
the incidence of serious febrile neutropenia in the summary findings and in the main results ( fourth paragraph , first sentence ) should have been reported as 78 ( 31% )  . 
in table 2 , the percentage values for grade 12 nausea , dizziness , elevated alanine aminotransferase , and thrombocytopenia should have been reported as 19% , 19% , 13% , and 2% , respectively . 
in the results , the second sentence ninth paragraph should have read as follows : of 75 patients who achieved a composite complete remission , two ( 3% ) received the 20 mg / day dose , seven ( 9% ) the 80 mg / day dose , 27 ( 36% ) the 120 mg / day dose , 36 ( 48% ) the 200 mg / day dose , and three ( 4% ) the 300 mg / day dose . 
these corrections have been made to the online version as of june 29 , 2018 . vol 19 july 2018 e335 corrections corrections published online june 12 , 2015 s1470 - 2045 ( 15 ) 00056 - x correction to lancet oncol 2015 ; 16 : e227 correction to lancet oncol 2015 ; 16 : 738 correction to lancet oncol 2015 ; 16 : 747 schiller jh . 
 antibodies lancet oncol 2015 ; 16 : 73839in this comment , the chemotherapy backbone used in the squire trial was incorrectly referred to as gemcitabine and carboplatin in four instances in the third paragraph ; it should read gemcitabine and cisplat these corrections have been made to the online version as of june 29 , 2015 , and the printed version is correct . torri v , broggini m , garassino mc . 
lancet oncol 2015 ; 16 : 74648the seventh sentence of the nal paragraph of this comment should read : results for leu858arg are still inconclusive because although progression - free survival is higher in patients given all egfr inhibitors versus chemotherapy , overall survival seems to be better with chemotherapy than with afatinib for these patients . 
 this correction has been made to the online version as of june 29 , 2015 , and the printed version is correct . for future lowy dr , herrero r , hildesheim a , for the participants in the iarc / nci workshop on primary endpoints for prophylactic hpv vaccine trial . 
 lancet oncol 2015 ; 16 : e22633 in the panel , in the section on the quadrivalent vaccine for men , the second bullet point should read : approved in the eu by the ema for the prevention of vaccine - type related anal lesions and for the prevention of vaccine - type related genital warts ( ages 9 )  . 
lancet oncol 2015 ; 16 : this news e316in item , the nal two sentences of paragraph 3 read : according to the scale , treatment late - stage egfr - mutated nonsquamous lung cancer with erlotinib provides a gain in progression - free survival ( pfs ) of 85 months ( hazard ratio [ hr ] 016 [ 95% ci 010026 ] ) and an improvement in quality of life compared with carboplatin and gemcitabine , earning an esmo - mcbs score of 4 / 5 . 
in contrast , the same drug when used to treat metas tatic pancreatic cancer provides an overall gain of only 9 days compared with chemotherapy treatment , and had a score of 1 / 5 . 
this correction has been made as of june 12 , 2015 . vol 16 july 2015 e313 published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections published online february 20 , 2019 s1470 - 2045 ( 18 ) 30941 - 0 see articles page 531 sartore - bianchi a , trusolino l , martino c , et al . 
dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - of - concept , multicentre , open - label , phase 2 trial . 
several improved outcomes in childhood cancer have led to an increased focus on the cost of long - term survival : longterm physical , psychological , and financial morbidities that arise as a consequence of cancer therapy or the cancer landmark childhood cancer survivor cohorts have informed our ability to describe , predict , and minimise these late effects.1 , 2 about 80% of adolescents and young adults ( ayas ) with cancer will also achieve long - term cure.3 consequently , late effects are also highly relevant to this population , but very few aya - specific data exist , forcing clinicians to extrapolate from the literature on childhood cancer survivors . 
previous work has shown that survivors of aya cancer have a higher absolute risk of subsequent primary neoplasms than do younger or older populations , which in turn has a substantial impact on overall survival.4 , 5 cohort of more in the lancet oncology , chloe bright and colleagues6 describe the risk of subsequent primary neoplasms than in a population - based 200 000 survivors of aya cancer . 
the large sample size and more than 26 million person - years of follow - up allow the investigators to describe , comprehensively for the first time and in great detail , the risk of specific subsequent primary neoplasms after specific primary cancers . 
 the level of granularity provided in the risk estimates ( eg , by primary cancer , type of subsequent primary neoplasm , and years from diagnosis ) should assist clinicians and policy makers in determining what type of interventions would be of greatest benefit for specific populations of aya cancer survivors . beyond improving risk prediction , several implications of the data are worth highlighting . 
for example , the surprising burden of subsequent lung cancers stands in contrast to the childhood cancer literature.7 in male survivors of hodgkin lymphoma , lung cancer accounted for approximately 40% of the total number of excess subsequent primary neoplasms , with a cumulative incidence of lung neoplasms of 51% at 35 years from diagnosis . 
it is unclear whether this difference compared with childhood cancer survivors is caused by several primary aya cancers being themselves related to smoking history ( eg , cervical cancer ) , a higher probability of smoking after diagnosis , 8 increased use of treatments such as lung radiotherapy , greater attained age , or a combination of these factors . 
irrespective of the mechanism , bright and colleagues results support interventions for survivors and smoking cessation raise the intriguing question of whether lung cancer screening guidelines developed for other high - risk populations may be appropriate.9 a second difference concerns temporal trends . 
the risk of subsequent primary neoplasms in childhood cancer survivors has decreased over consecutive cohorts , largely associated with reductions in radiotherapy doses.2 , 10 in this study , treatment decade was not significantly associated with subsequent primary neoplasm risk , suggesting that no such decline has occurred in the aya survivor population . 
 alternatively , reducing the incidence of subsequent primary neoplasms in survivors of aya cancer might require a stronger focus on lifestyle factors . represents a substantial contribution , several limitations merit note . 
however , a patient with hodgkin lymphoma might receive only two cycles of chemotherapy or might undergo six cycles and radiotherapy , with consequently vastly different risks for subsequent primary neoplas without treatment data , the clinician is still left uncertain on how to counsel an individual patient on his or her personalised risk , or what screening to recommend . 
aya - specific risk prediction models that include treatment exposure are urgently needed . finally , description of risk is only a first step towards the ultimate goal of improving the quantity and quality of life for survivors of aya cancer . 
determining what health - care delivery models maximise uptake of such interventions in a population known to face substantial barriers to access will also be necessary . for decades , paediatricians have insisted that children are not just little adults . 
we must now be equally emphatic in declaring that when it comes to the late effects of cancer and cancer therapy , ayas are not just big children , but instead deserve recognition as their own unique group . sumit gupta division of haematology / oncology , hospital for sick children , toronto , on , m5g 1x8 , canada sumit.gupta@sickkids.ca i declare no competing interests . copyright 2019 the author ( s )  . 
risk of subsequent primary neoplasms in survivors of adolescent and young adult cancer ( teenage and young adult cancer survivor study ) : a population - based , cohort study . 
jama 2017 ; 317 : 81424 . pet oestrogen receptor imaging : ready for the clinic ? oestrogen signalling is a key component of normal mammary gland physiology and mediates breast cancer pathogenesis in most breast cancers.1 drugs targeting oestrogen - mediated growth in breast cancer , termed endocrine therapy , provide a key therapeutic strategy . 
 the presence or absence of oestrogen receptors is a predictor of breast cancer response to endocrine therapy ; documenting oestrogen receptor expression from a biopsy sample before initiating therapy is a well established clinical standard.1 although primary breast tumour biopsy is well developed , safe , and effective , tissue sampling and assays pose challenges in the metastatic setting . 
the portec - 3 trial was initiated to investigate the benefit of adjuvant chemotherapy during and after radiotherapy ( chemoradiotherapy ) versus pelvic radiotherapy alone for women with high - risk endometrial cancer . methods portec - 3 was an open - label , international , randomised , phase 3 trial involving 103 centres in six clinical trials collaborating in the gynaecological cancer intergroup . 
eligible women had high - risk endometrial cancer with figo 2009 stage i , endometrioid - type grade 3 with deep myometrial invasion or lymph - vascular space invasion ( or both ) , endometrioid - type stage ii or iii , or stage i to iii with serous or clear cell histology . 
women were randomly assigned ( 1 : 1 ) to receive radiotherapy alone ( 486 gy in 18 gy fractions given on 5 days per week ) or radiotherapy and chemotherapy ( consisting of two cycles of cisplatin 50 mg / m given during radiotherapy , followed by four cycles of carboplatin auc5 and paclitaxel 175 mg / m ) using a biased - coin minimisation procedure with stratification for participating centre , lymphadenectomy , stage of cancer , and histological type . 
5 - year overall survival was 818% ( 95% ci 775862 ) with chemoradiotherapy versus 767% ( 721816 ) with radiotherapy ( adjusted hazard ratio [ hr ] 076 , 95% ci 054106 ; p = 011 ) ; 5 - year failure - free survival was 755% ( 95% ci 703799 ) versus 686% ( 631734 ; hr 071 , 95% ci 053095 ; p = 0022 )  . 
grade 3 or worse adverse events during treatment occurred in 198 ( 60% ) of 330 who received chemoradiotherapy versus 41 ( 12% ) of 330 patients who received radiotherapy ( p < 00001 )  . 
 neuropathy ( grade 2 or worse ) persisted significantly more often after chemoradiotherapy than after radiotherapy ( 20 [ 8% ] women vs one [ 1% ] at 3 years ; p < 00001 )  . 
most deaths were due to endometrial cancer ; in four patients ( two in each group ) , the cause of death was uncerta one death in the radiotherapy group was due to either disease progression or late treatment complications ; three deaths ( two in the chemoradiotherapy group and one in the radiotherapy group ) were due to either intercurrent disease or late treatment - related toxicity . interpretation adjuvant chemotherapy given during and after radiotherapy for high - risk endometrial cancer did not improve 5 - year overall survival , although it did increase failure - free survival . 
continued follow - up is needed to evaluate long - term survival . funding dutch cancer society , cancer research uk , national health and medical research council project grant and cancer australia , lagenzia italiana del farmaco , and canadian cancer society research institute . copyright the author ( s )  . 
in adjusted analysis , improved progression - free survival and overall survival were reported for patients treated with chemotherapy , but with high proportions of patients with toxicity and similar event rates in both groups . 
two trials ( one in italy and one in japan ) compared pelvic radiotherapy with three cycles or five cycles of cyclophosphamidedoxorubicincisplatin chemotherapy in stage iiii disease and neither showed any difference in overall survival or relapse - free survival . 
in the italian trial , most patients had stage iii disease , and chemotherapy delayed distant metastases and radiotherapy delayed pelvic recurrence , but without differences in overall survival or progression - free survival . 
the phase 2 rtog - 9708 trial , which assessed toxicity on the chemoradiotherapy schedule on which portec - 3 is based , reported 4 - year overall survival of 85% and disease - free survival of 81% . 
the nsgo - ec - 9501 / eortc - 55991 trial was published in a pooled analysis with the unfinished mango iliade phase 3 trial , and showed significantly improved progression - free survival and a trend for improved overall survival with the addition of four cycles of platinum - based chemotherapy given sequentially before or after pelvic radiotherapy . 
the results of the gog - 249 trial , which compared pelvic radiotherapy with a combination of three cycles of carboplatin - paclitaxel chemotherapy and vaginal brachytherapy in stage iii patients with high ( intermediate ) risk factors reported overlapping progressionfree survival and overall survival curves , and significantly more pelvic and para - aortic recurrences in the chemotherapy group . 
no differences in overall or recurrence - free survival were reported , but significantly more vaginal and pelvic or para - aortic recurrences were reported in the chemotherapy group . added value of this study we report the overall survival and failure - free survival of patients with high - risk endometrial cancer treated in the international portec - 3 trial . 
the treatment duration was longer in the chemoradiotherapy group than in the radiotherapy group , and significantly higher rates of adverse events were reported in the chemoradiotherapy group during , and in the first year after , treatment . implications of all the available evidence combined adjuvant chemotherapy and radiotherapy cannot be recommended as a new standard of care for patients with stage iii endometrial cancer because no survival differences were found and pelvic control was high with radiotherapy alone . 
patients with stage iii cancer had the greatest benefit with chemoradiotherapy because of their higher risk of disease recurrence ; for these patients , combined treatment should be considered to maximise failure - free survival . 
 nevertheless , the benefits and risks should be discussed for each individual patient . introduction the majority of women with endometrial cancer present with early - stage disease and have a favourable prognosis . 
 about 15% of women with endometrial cancer are diagnosed with high - risk disease , which comprises endometrioid endometrial cancer stage i , grade 3 with deep invasion or with lymph - vascular space invasion ( lvsi ) , stage ii or iii endometrioid endometrial cancer , or non - endometrioid ( serous or clear cell ) histology . 
women with high - risk endometrial cancer are at increased risk of distant metastases and cancer - related death.14 serous and clear cell cancers have a higher risk of aggressive spread and a worse prognosis ; however , in the early stages they have similar outcomes to grade 3 endometrioid endometrial cancer.5 pelvic external beam radiotherapy has been the standard adjuvant treatment for women with high - risk endometrial cancer for many decades , although there is a improvement of survival . 
 radiotherapy was shown to delay pelvic recurrence and chemotherapy was shown to delay distant metastases , but no differences in survival were found . external beam compared have 296 vol 19 march 2018 articles correspondence to : dr stephanie m de boer , department of radiation oncology , leiden university medical center , 2333 za leiden , netherlands s.m.de_boer.onco@lumc.nl see online for appendix for the study protocol see because increased incidence of pelvic relapse has been reported with chemotherapy alone , the combination of external beam radiotherapy with chemotherapy has been explored . 
in a phase 2 trial ( rtog 9708 ) 8 among women with high - risk endometrial cancer , the combination of external beam radiotherapy with two concurrent cycles of cisplatin , followed by four adjuvant cycles of cisplatin and paclitaxel , was tested , resulting in 4 - year overall survival of 85% and disease - free survival of 81% . the combination of because radiotherapy and seemed more ( chemoradiotherapy ) chemotherapy effective than either treatment alone , and because data for toxicity and quality of lacking , the randomised portec - 3 trial was initiated to evaluate the benefit of chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer in terms of overall survival and failure - free survival improvement , as well as toxicity and effects on health - related quality of life . 
analysis of 2 - year toxicity and health - related quality of life in the portec - 3 trial showed significantly higher rates of adverse events and reduced health - related quality of life during and after chemoradiotherapy treatment , with rapid recovery thereafter.9 life were here , we present the final analysis of the primary survival endpoints of the portec - 3 trial . methods study design and participants portec - 3 was an open - label , randomised , phase 3 trial at 103 centres ( oncology centres , university hospitals , regional hospitals , or radiation oncology centres with referrals from regional hospitals ) in six clinical trial groups collaborating in the gynaecological cancer intergroup . 
participating groups were the national cancer research institute ( ncri ; uk ) , australia and new zealand gynaecologic oncology group ( anzgog ; australia and new zealand ) , mario negri gynaecologic oncology group ( mango ; italy ) , canadian cancer trials group ( cctg ; canada ) , and fedegyn ( france )  . stage ( parametrial ( figo ) 2009 patients were eligible if they had endometrial cancer with either international federation of gynecology and 1a endometrioid obstetrics endometrial cancer grade 3 with documented lvsi ; stage ib endometrioid endometrial cancer grade 3 ; stage ii endometrioid endometrial cancer ; stage iiia , iiib invasion ) , or iiic endometrioid endometrial cancer ; or serous or clear - cell histology endometrial cancer with stages ia ( with invasion ) , ib , ii , or iii . 
eligibility also included who performance score 02 ; adequate bone marrow function ( white blood cells 30 10 / l , platelets 100 10 / l ) , function ( bilirubin 15 upper normal limit [ unl ] , aspartate amino transferase aminotransferase 25 unl ) , kidney function ( creatinine clearance > 60 ml per min calculated according to cockroft and gault10 or > 50 ml per min edta clearance ) , and aged 18 years or older ( without an upper age limit , because elderly women alanine liver and might benefit from the study treatment if deemed fit enough to undergo chemotherapy )  . 
exclusion criteria were uterine ( carcino ) sarcoma ; malignancy in the 10 years before diagnosis of endometrial cancer ; previous pelvic radiotherapy , hormonal therapy , or chemotherapy ; bulky cervical involvement with radical hysterectomy ; inflammatory bowel disease ; residual macroscopic tumour ; impaired renal or cardiac function ; grade 2 or worse neuropathy ; grade 3 or worse hearing impairment ; or congenital hearing disorder . surgery comprised total abdominal or laparoscopic hysterectomy with bilateral salpingo - oophorectomy . 
 lymphadenectomy , whether systemic or sampling , was left to the discretion of participating centres , while lymph node debulking and para - aortic lymph - node sampling were recommended in cases of macroscopic positive pelvic nodes or para - aortic nodes ( or both )  . 
lymphadenectomy was not mandated in view of the lack of improvement in overall or progression - free survival in early - stage disease and its associated toxicity , mainly lymph oedema.11 , 12 for high - risk disease , the value of lymphadenectomy debated , 13 and the international statec trial14 has been initiated to address this issue . 
central pathology review by the groups reference gynaecopathologists was required before randomisation to confirm patients ' final suitability for study entry . to direct adjuvant treatment written informed consent was obtained from all patients . 
treatment was allocated with a biased - coin minimisation procedure , ensuring balance overall and within each stratum of the stratification factors ( participating centre , lymphadenectomy , stage of cancer , and histological type )  . 
 investigators were not masked to participants and treatment allocation . procedures central pathology review was done by reference gynaecopathologists ( as appointed by each participating group before the start of the trial ) to determine final eligibility . 
in case of serosal breach , metastases in the stroma of the fallopian tubes , in the ovaries , or on the peritoneal surface of the tubes or ovaries ( or both ) , the stage was defined as iiia . 
after determination of eligibility and patient consent , a tumour sample was centrally stored for future translational research . external beam pelvic radiotherapy was given in both treatment groups to a total dose of 486 gy in 18 gy fractions , 5 days a week . 
the clinical target volume was extended to include the aortic bifurcation in case of iliac lymph node involvement ; to include the lower peri - aortic region for common iliac node involvement ; and to include the higher para - aortic region in case of para - aortic involvement ( with a margin of 2 cm above the highest involved lymph node )  . 
 brachytherapy dose was equivalent to 14 gy in 2 gy fractions ( with recommended scheme of 10 gy high - dose rate [ hdr ] in fractions of 5 gy ) , specified at 5 mm from the vaginal vault surface . 
most patients were treated with a four - field technique ; use of intensity - modulated radiotherapy was allowed for centres per approval by their groups principal investigator . treatment was recommended to start within 46 weeks of surgery , but no later than 8 weeks . 
however , the trans - tasman radiation oncology group ( trog ) initiated a bench - marking and quality assurance programme for the anzgog group , 16 and in 2012 , a protocol amendment allowed a short quality - assurance programme to be activated for all other participating sites , with independent review of a single radiotherapy plan for each site . patients in the chemoradiotherapy group received two cycles of intravenous cisplatin 50 mg / m in the first and fourth week of external beam pelvic radiotherapy , followed by four cycles of intravenous carboplatin auc5 and paclitaxel 175 mg / m at 21 - day intervals . 
this schedule was based on the rtog - 9708 trial , 8 with substitution of cisplatin by carboplatin in the adjuvant phase to reduce toxicity and in view of the use of carboplatinpaclitaxel chemotherapy in metastatic disease.17 adjuvant chemotherapy was to be started within 3 weeks after completion of external beam pelvic radiotherapy , and with a 28 - day interval from the second concurrent cycle . 
details on chemotherapy stopping rules have been described previously.9 at each follow - up , patient history was taken with emphasis on toxicities and symptoms of recurrent disease , and physical and pelvic examination were done . 
long - term follow - up ( by hospital visit or information from the general practitioner ) was required at 7 years and 10 years . outcomes the coprimary endpoints were overall survival and failure - free survival . 
failure - free survival ( defined as any relapse or death related to endometrial cancer or treatment ) was defined as time from randomisation to date of first failure - free survival event . 
abdominal recurrences outside the pelvic area ( peritoneal carcinomatosis , liver , and para - aortic lymph nodal metastases ) were considered distant metastases , with specification of site . toxicity was assessed and graded with common terminology criteria for adverse events ( ctcae ) version 3.018 at baseline ( after surgery ) , at completion of radiotherapy , after each chemotherapy cycle , at 6 - month intervals from randomisation until 5 years , and at 7 years 298 vol 19 march 2018 articles and 10 years . 
for evaluation of mild ( grade 1 ) toxicities , patient - reported health - related quality - of - life symptoms were used because patient reporting of grade 1 toxicities was considered most reliable.19 serious adverse events had to be reported within 24 h , specifying adverse event grade and whether or not they were associated with study treatment . statistical analysis the portec - 3 trial was powered ( 80% ) to detect a 10% difference in 5 - year overall survival ( increase from 65% to 75% ; hazard ratio [ hr ] 067 ) , with a two - sided value of 005 . 
power calculation of the coprimary endpoint failure - free survival was based on the same principles as overall survival . the first prespecified interim analysis was done after 48 overall survival events ( a third of the required events ) had occurred in september , 2013 , only 3 months before reaching complete accrual . 
in october , 2016 , we decided , with permission from the data safety monitoring board ( dsmb ) , not to do the prespecified second interim analysis at two - thirds of overall survival events , because this would have no consequences for the trial and would reduce - spending . 
for analysis of the coprimary endpoints , failure - free survival with a overall survival and correlation between the test - statistics of the coprimary endpoints of 07859 ( based on 136 overall survival events and 186 failure - free survival events ) , a nominal of 00309 was used for each of the analyses , resulting in an overall level of 00498.20 because deaths in the portec - 3 trial were lower than expected at the time of trial design , the required number of overall survival events was not expected to be reached before late 2018 . 
for these reasons , the dsmb approved the final analysis becoming time - based rather than event - based , with final analysis at a median follow - up of 5 years and 42 months additional follow - up after inclusion of the last patient . 
for analysis of failure - free survival and recurrence , competing - risk methods were used.23 for failure - free survival , intercurrent death was used as a competing risk . 
the median follow - up was estimated with the reverse kaplan meier method . regression with this study is registered with isrctn , number and clinicaltrials.gov , number isrctn14387080 nct00411138 . role of the funding source the funding bodies had no role in study design , data collection , data interpretation , data analysis , or writing of this report . 
the central data manager ( kwv ) , the chief investigator ( clc ) , the associated investigators ( smdb , ran ) , and the trial statistician ( hp ) had full access to all the data . 
the corresponding author and chief investigator had full access to all the data and the final responsibility to submit for publication . results between nov 23 , 2006 , and dec 20 , 2013 , 686 women were enrolled and randomly assigned to chemoradiotherapy ( n = 343 ) or radiotherapy ( n = 343 )  . 
660 patients were included 686 patients enrolled and randomly assigned 343 randomly assigned to radiotherapy 343 randomly assigned to chemoradiotherapy 13 excluded 4 withdrew informed consent 9 did not meet eligibility criteria 13 excluded 9 withdrew informed consent 4 did not meet eligibility criteria 330 assigned to radiotherapy 328 received allocated treatment 2 received chemoradiotherapy 330 assigned to chemoradiotherapy 325 received allocated treatment 5 received radiotherapy only 660 patients in intention - to - treat population 330 in the radiotherapy group 330 in the chemoradiotherapy group figure 1 : trial profile vol 19 march 2018 articles in in the primary analysis ( chemoradiotherapy , n = 330 ; radiotherapy , n = 330 )  . 
median follow - up was 602 months ( iqr 481731 ) overall and was 600 months ( 478731 ) the chemoradiotherapy group and 607 months ( 487729 ) in the radiotherapy group . 
 there were seven major protocol violations : in the chemoradiotherapy group , five patients refused chemotherapy and received radiotherapy only ; in the radiotherapy group , two patients asked to switch to chemoradiotherapy ( figure 1 )  . chemoradiotherapy ( n = 330 ) radiotherapy alone ( n = 330 ) age at randomisation ( years ) 624 ( 565679 ) 620 ( 558682 ) patient characteristics were well balanced between the treatment groups ( table 1 )  . 
lymphadenectomy , lymph node sampling , or full surgical staging were done in 190 patients ( 58% ) 192 patients ( 58% ) in the radiotherapy group . chemoradiotherapy group and the radiotherapy was discontinued in one patient ( < 1% ) in the chemoradiotherapy group because of disease progression and five patients ( 15% ) in the radiotherapy group because of toxicity ( table 1 )  . 
329 ( 100% ) of 330 patients in the chemoradiotherapy group and 322 ( 98% ) of 330 patients in the radiotherapy group received an external beam pelvic radiotherapy dose between 450 and 504 gy . 
 ( table 1 continues on next column ) table 1 : patient , tumour , and treatment characteristics 300 vol 19 march 2018 articles 309 ( 47% ) patients ( 151 [ 46% ] chemoradiotherapy patients vs 158 [ 48% ] radiotherapy patients )  . 
apart from the protocol indication for brachytherapy boost ( cervical invasion ) , 28 ( 4% ) patients received a brachytherapy boost for locally perceived reasons such as lvsi , grade 3 , or stage iii . chemotherapy was both cycles of concurrent cisplatin were completed by 304 ( 92% ) of 330 patients in the chemoradiotherapy group . 
adjuvant started by 304 ( 92% ) patients , while 262 ( 79% ) patients completed all four cycles of carboplatin and 233 ( 71% ) patients completed all four cycles of paclitaxel ( table 1 )  . 
at least one dose reduction of cisplatin ( to 40 mg / m ) was recorded for five ( 2% ) patients , of carboplatin ( from auc5 to auc4 ) for 36 ( 11% ) patients , and of paclitaxel ( from 175 mg / m to 135 mg / m ) for 50 ( 15% ) patients . 
 chemotherapy was discontinued in 61 ( 18% ) patients ; in 31 ( 9% ) because of toxicity , patient decision in 20 ( 6% ) , disease progression in seven ( 2% ) , and for other reasons in three ( 1% )  . evaluation of the trog quality assurance programme for the anzgog group showed that a radiotherapy benchmarking exercise before participation in the trial ensured high conformity and low rates of both minor and major contouring deviations.16 evaluation of radiotherapy plans from centres in other countries is ongoing and will be reported separately . at final database lock on may 1 , 2017 , 136 patients had died ( 61 in the chemoradiotherapy group and 75 in the radiotherapy group ) and 186 patients had a failure - free survival event ( 83 in the chemoradiotherapy group and 103 in the radiotherapy group )  . 
among the patients assigned to chemoradiotherapy , 50 ( 82% ) had died from endometrial cancer , four ( 7% ) from a second cancer , three ( 5% ) from other intercurrent disease , and two ( 3% ) from treatment for metastatic disease . 
for the remaining four patients ( two patients treated with chemoradiotherapy and two patients with radiotherapy ) , the cause of death was uncertain one patient in the radiotherapy group , death was due to either disease progression or late treatment complications ; in two patients in the chemoradiotherapy group and one in the radiotherapy group , death was due to either intercurrent disease or late treatment - related toxicity . 
 these four deaths were counted as failure - free survival events after discussion with the dsmb . estimated overall survival adjusted for stratification factors at 5 years was 818% ( 95% ci 775862 ) for patients the chemoradiotherapy group versus 767% ( 721816 ) for patients in the radiotherapy group ( hr 076 , 95% ci 054106 ; p = 0109 ; table 2 , figure 2 )  . 
 5 - year failure - free survival was 755% ( 703799 ) in the chemoradiotherapy group versus 686% ( 631734 ) in the radiotherapy group ( hr 071 , 053095 ; p = 0022 )  . 
 without adjusting for the stratification factors , the hr events 5 - year estimate , % ( 95% ci ) hazard ratio ( 95% ci ) p value 076 ( 054106 ) 071 ( 053095 ) 0109 0022 overall survival * failure - free survival * overall survival chemoradiotherapy radiotherapy failure - free survival chemoradiotherapy radiotherapy chemoradiotherapy radiotherapy chemoradiotherapy radiotherapy vaginal recurrence ( first recurrence ) pelvic recurrence ( first recurrence ) distant metastases ( first recurrence ) chemoradiotherapy radiotherapy vaginal recurrence ( total ) chemoradiotherapy radiotherapy pelvic recurrence ( total ) chemoradiotherapy radiotherapy distant metastases ( total ) chemoradiotherapy radiotherapy 818% ( 775862 ) 081 ( 058113 ) 0213 767% ( 721816 ) 755% ( 703799 ) 076 ( 057102 ) 0067 686% ( 631734 ) 03% ( 0021 ) 099 ( 0061590 ) 0999 10% ( 0329 ) 060 ( 014249 ) 0473 03% ( 0021 ) 15% ( 0636 ) 21% ( 1044 ) 92% ( 65129 ) 224% ( 181274 ) 078 ( 058106 ) 0108 283% ( 237337 ) 21% ( 1044 ) 099 ( 037265 ) 0995 49% ( 3079 ) 051 ( 028092 ) 0026 231% ( 188283 ) 077 ( 057103 ) 0077 297% ( 249351 ) * data are chemotherapy versus radiotherapy ( cox - adjusted p value ) , adjusted for stratification factors : participating groups , type of surgery ( abdominal hysterectomy and salpingo - oophorectomy vs abdominal surgery plus lymphadenectomy vs laparoscopic procedure vs laparoscopic procedure plus lymphadenectomy ) , stage ( figo 2009 ia vs ib vs ii vs iii ) , and histological type ( endometrioid carcinoma vs serous or clear cell carcinoma )  . 
 table 2 : survival and recurrence outcomes for overall survival was 081 ( 95% ci 058113 ; p = 0213 ) and for failure - free survival was 076 ( 057102 ; p = 0067 ; table 2 , figure 2 )  . in subgroup analysis , women with stage iii lower overall endometrial cancer had significantly survival and failure - free survival than those with stage iii disease ( tables 3 , 4 )  . 
5 - year overall survival for stage iii cancer was 787% ( 95% ci 722857 ) in the chemoradiotherapy group versus 698% ( 624781 ) in the radiotherapy group ( hr 071 , 95% ci 045111 ; p = 013 ; adjusted p = 0074 )  . 
5 - year failure - free survival for stage iii cancer was 693% ( 95% ci 611762 ) in the chemoradiotherapy group versus 580% ( 493657 ) in the radiotherapy group ( hr 066 , 95% ci 045097 ; p = 0031 ; adjusted p = 0014 ; figure 2 )  . 
5 - year failure - free survival for stage iii patients was 808% ( 741860 ) in the chemoradiotherapy group versus 766% ( 695822 ) in the radiotherapy group ( 085 , 054133 ; p = 047 )  . serous cancers ( > 25% serous component ) had lower overall survival and failure - free significantly vol 19 march 2018 articles number at risk ( number censored ) radiotherapy chemoradiotherapy pcox - adjusted = 011 plog - rank = 021 , hr 076 ( 95% ci 054106 ) pcox - adjusted = 0022 plog - rank = 0067 , hr 071 ( 95% ci 053095 ) ( 11 ) ( 18 ) ( 60 ) ( 71 ) ( 123 ) ( 130 ) ( 10 ) ( 16 ) ( 50 ) ( 63 ) ( 105 ) ( 120 ) radiotherapy chemoradiotherapy number at risk ( number censored ) radiotherapy chemoradiotherapy pcox - adjusted = 0074 plog - rank = 013 , hr 071 ( 95% ci 045111 ) pcox - adjusted = 0014 plog - rank = 0031 , hr 066 ( 95% ci 045097 ) time since randomisation ( years ) time since randomisation ( years ) ( 23 ) ( 26 ) ( 53 ) ( 52 ) ( 18 ) ( 23 ) ( 44 ) ( 50 ) figure 2 : overall survival and failure - free survival kaplan - meier survival curves for overall survival ( a ) and failure - free survival ( b ) in all patients , and for overall survival ( c ) and failure - free survival ( d ) of patients with stage iii endometrial cancer . 
the number of patients and events are , however , small in these subgroups ( appendix p 3 )  . isolated vaginal and pelvic recurrences were rare , with isolated vaginal recurrence diagnosed in one ( < 1% ) patient in the chemoradiotherapy group and in one ( < 1% ) patient in the radiotherapy group ( p = 0995 ) , and isolated pelvic in the chemorecurrence in three ( 1% ) patients radiotherapy group versus five ( 2% ) patients in the radiotherapy group ( p = 0473 )  . 
most recurrences were distant metastases : 76 ( 22% ) patients in the chemoradiotherapy group versus 93 ( 28% ) patients in the radiotherapy group were diagnosed with distant metastases ( p = 0108 )  . 
the 5 - year estimate of pelvic recurrence ( both isolated and combined pelvic and distant recurrences ) was 49% ( 95% ci 3079 ) for the chemoradiotherapy group versus 92% ( 65129 ) for the radiotherapy group ( p = 0026 ; table 2 )  . in the multivariable analysis , the following covariates were included together with treatment : stage , histological type and grade , type of surgery , participating groups , lvsi , and age . 
most factors , except lymphadenectomy , were significantly correlated with failure - free survival ( table 4 )  . in multivariable analysis for failure - free survival , only age group was found to be predictive of treatment effect , with a strong treatment - by - age effect ( pinteraction = 0012 , figure 3 )  . 
women aged 70 years or older had the greatest benefit from chemoradiotherapy . grade 2 or worse adverse events were reported during treatment in 308 ( 93% ) women in the chemoradiotherapy group versus 144 ( 43% ) in the radiotherapy group , and grade 3 or worse in 198 ( 60% ) versus 41 ( 12% ; p < 00001 ; table 5 ) ; the majority of grade 3 or worse adverse events were haematological . 
table 6 shows an overview of adverse events at 6 months after randomisation , which 302 vol 19 march 2018 articles was about 1 month after completion of treatment in the chemoradiotherapy group . 
the number of patients with grade 2 or worse adverse events was 86 ( 32% ) for chemoradiotherapy versus 64 ( 24% ) for radiotherapy at 3 years ( p = 0034 ) , and 57 ( 40% ) versus 38 ( 28% ) at 5 years ( p = 0033 )  . 
the most significant and clinically relevant difference between the arms was found for grade 2 or worse sensory neuropathy , which persisted in 20 ( 8% ) women in the chemoradiotherapy group versus one ( 1% ) women in the radiotherapy group at 3 years and 12 ( 9% ) women versus no women at 5 years ( both p < 00001 )  . 
an extensive overview of adverse events during follow - up is in the appendix ( pp 45 )  . improve overall discussion the final results of the portec - 3 trial showed that the combination of adjuvant chemotherapy and radiotherapy for high - risk endometrial cancer did not significantly survival . 
patients with stage iii diseasewho had a higher risk of recurrence than those with stages iiihad a hr of 066 and 11% absolute improvement of failure - free survival with chemo - radiotherapy , which is clinically relevant and exceeds the 10% improvement used when designing the study . the improvement in failure - free survival in the chemoradiotherapy group should be weighed against the severity and duration of toxicity of combined treatment , especially since overall survival was not significantly improved . 
although significantly higher incidences of adverse events and reduced health - related quality of life were reported in the chemoradiotherapy group during and after treatment , 9 rapid recovery was seen , with no differences in grade 34 adverse events from 12 months onwards . 
grade 2 sensory neuropathy , however , persisted significantly more often treated with chemoradiotherapy , with 25% of patients reporting quite a bit or very much tingling or numbness at 2 years , compared with 6% for radiotherapy.9 sensory neuropathy is associated with lower levels of functioning and quality of life , and more fatigue.24 in patients for decades , standard adjuvant treatment for women with high - risk endometrial cancer has been pelvic external beam radiotherapy . 
randomised trials comparing adjuvant chemotherapy with external beam radiotherapy failed progression - free survival.6 , 7 retrospective studies reported substantial rates of pelvic recurrence if high - risk patients were treated without radiotherapy , supporting the combined use of pelvic to show an improvement survival overall patients events 5 - year overall survival ( 95% ci ) hazard ratio ( 95% ci ) p value total 79% ( 748839 ) chemoradiotherapy 82% ( 775862 ) 073 ( 052103 ) 77% ( 721816 ) treatment group radiotherapy age ( years ) 6069 stage stage i and ii stage iii histology and grade endometrioid grade 1 and 2 endometrioid grade 3 serous / clear cell lvsi lymphadenectomy 89% ( 850929 ) 75% ( 696806 ) 231 ( 148359 ) 67% ( 587763 ) 329 ( 199544 ) 83% ( 791873 ) 74% ( 693797 ) 86% ( 819909 ) 241 ( 166351 ) 79% ( 730857 ) 71% ( 652774 ) 176 ( 110281 ) 235 ( 148372 ) 85% ( 805894 ) 75% ( 709799 ) 136 ( 093198 ) 77% ( 714821 ) 81% ( 771852 ) 082 ( 055122 ) 0075 < 00001 < 00001 < 00001 011 033 adjusted for participating groups . 
lvsi = lymph - vascular space invasion . table 3 : multivariable analysis of prognostic factors for overall survival radiotherapy with adjuvant chemotherapy , as first explored in the rtog 9708 phase 2 trial.8 , 25 , 26 randomised studies have compared radiotherapy with the combination of chemotherapy and radiotherapy in patients with high - risk endometrial cancer . 
the nsgo - ec - 9501 / eortc - 55991 trial compared external beam radiotherapy alone with external beam radiotherapy and four cycles of platinum - based chemotherapy , given sequentially before or after external beam radiotherapy . 
 a pooled analysis with the mango iliade 3 trial27 with a total cohort of 534 patients showed , in line with our results , improved progression - free survival ( 78% vs 69% , p = 001 ) and a trend for improved survival ( 82% vs 75% , p = 007 ) with the addition of chemotherapy to radiotherapy alone . the schedule of combined radiotherapy with concurrent and adjuvant chemotherapy used in the portec - 3 trial seemed likely to be most effective because both treatments were started early after surgery and thus maximum benefit of the combination could be expected . 
a retrospective single institution study28 reporting on 40 patients with stage iiia or iiic endometrial cancer treated with the same combination of chemoradiotherapy showed 5 - year overall survival of 85% and relapse - free survival of 79% . 
 in the chemoradiotherapy group of the portec - 3 trial the 5 - year overall survival probability was 82% and the thus survival probability was failure - free 76% , vol 19 march 2018 articles patients events 5 - year failure - free survival ( 95% ci ) hazard ratio ( 95% ci ) p value total 72% ( 667767 ) 68% ( 631734 ) 75% ( 703799 ) 81% ( 753850 ) 67% ( 607724 ) 64% ( 544717 ) 79% ( 739826 ) 64% ( 580692 ) 78% ( 727831 ) treatment group radiotherapy chemoradiotherapy age ( years ) 6069 stage stage i and ii stage iii histology and grade endometrioid grade 1 and 2 lvsi lymphadenectomy 068 ( 051091 ) 174 ( 123246 ) 214 ( 141325 ) 262 ( 190361 ) 0010 < 00001 < 00001 < 00001 0054 041 77% ( 714818 ) 68% ( 634729 ) 136 ( 099187 ) 72% ( 657766 ) 72% ( 674767 ) 087 ( 061122 ) endometrioid grade 3 serous or clear cell 71% ( 645771 ) 64% ( 566704 ) 156 ( 106230 ) 215 ( 146316 ) adjusted for participating groups . 
overall and relapse - free survival in the pooled nsgo - ec - 9501 / eortc - 55991 / iliade trials27 were also similar at 82% and 78% , with only 20% patients with stage iii disease . trials in chemotherapy high - risk endometrial cancer is heterogeneous , including various histological types and stages of disease . 
 in the nsgo - ec - 9501 / eortc - 55991 trial , although progression - free survival was significantly improved for patients with endometrioid endometrial cancer , this improvement was not found for serous and clear cell cancers . 
in the portec - 3 trial , women with serous or clear - cell cancers had at least as much improvement in failure - free survival with the addition of chemotherapy as women with endometriod endometrial cancer did . 
when comparing serous cancers with other histological types , as expected , worse overall survival and failure - free survival were found for serous cancers ; patients with serous cancers had a failure - free survival benefit with chemoradiotherapy , but this benefit was not significant in view of the small numbers of serous cancers and events . the multivariable analysis indicated that women older than 70 years seemed to have a greater failure - free survival benefit from chemotherapy than younger women . 
age is a well - known risk factor for endometrial cancer and a greater benefit of chemotherapy in older women has been reported previously.7 , 30 although selection of fitter older women in this randomised trial might have occurred , physicians should not be reticent to counsel older women about the possible benefits of combined chemotherapy and radiotherapy . analysed by stage , patients with stage iii endometrial cancer who have the highest frequency of recurrence , also had the greatest absolute benefit from the combined treatment . 
the smaller failure - free survival improvement for patients with stage iii disease seems not to outweigh the cost in terms of toxicity and quality - of - life impairment . 
 this finding is in line with the results of the gog - 249 trial , in which patients with stage i and ii endometrial cancer with high - intermediate or high - risk factors were randomly assigned to pelvic radiotherapy alone or to chemotherapy ( three cycles of carboplatin and paclitaxel ) followed by vaginal brachytherapy . 
no superiority of three cycles chemotherapy plus vaginal brachytherapy over external bean radiotherapy alone was found , with overlapping progression - free and overall survival curves and significantly more pelvic and para - aortic recurrences in the chemotherapy group.31 , 32 the majority because of in 47% of all patients , a vaginal brachytherapy boost was given ( 46% for chemoradiotherapy vs 48% for radiotherapy ) ; cervical involvement and 4% because of other reasons , such as lvsi or grade 3 endometrial cancer . 
this finding is in line with other studies among patients with stage iiiii endometrial cancer.33 although the addition of a brachytherapy boost might have added to the good local control seen in both groups , we do not expect this would have affected the results , because the proportion of women receiving a brachytherapy boost was equal in the two treatment groups . the portec - 3 to compare the radiotherapy and chemotherapy trial with schedule as used chemotherapy alone for advanced stage endometrial cancer , the gog - 258 trial randomly assigned participants to receive chemoradiotherapy or six cycles of carboplatin and paclitaxel.34 final results are pending , but a presented abstract34 reported no differences in overall or recurrence - free survival , while significantly more vaginal and pelvic or para - aortic recurrences were reported in patients treated with chemotherapy alone . 
furthermore , acute gastrointestinal and genitourinary toxicity of pelvic radiotherapy will be reduced with the current standard use of intensitymodulated radiotherapy.36 portec - 3 was a multicentre trial with strong international collaboration among six participating groups and , therefore , highly representative of current practice worldwide . 
 analysis of pathology review in the netherlands and the uk ( 48% of portec - 3 participants ) revealed that 83% of patients did not fulfil the eligibility criteria after central pathology review . 
these patients did not enter the trial.15 a limitation of this trial might be that because of the death and failure - free survival event rates were lower than expected at the time of trial design , the required number of overall survival events was not reached and the final analysis was time - based rather than eventbased , with final analysis at a median follow - up of 5 years ( 42 months after inclusion of the last patient )  . 
 the number of overall survival events was 136 ( 69% of the required number of overall survival events ) , and the number of failure - free survival events was 186 ( 94% of the required events )  . 
 long - term outcomes will be analysed , especially for overall survival . the costs of chemoradiotherapy in terms of toxicity and treatment duration should be weighed against the benefits , and this costbenefit tradeoff could be seen differently from the patient or physician perspective . 
in a patient preference study done by the anzgog group among portec - 3 participants , 37 more than 50% of patients rated 5% survival improvement sufficient to make chemotherapy worthwhile . 
although the trial results are in the range of this benefit for failure - free survival , the overall survival difference was not significant , thus individual patient counselling remains essential . 
translational studies of molecular risk factors and tumour characteristics with the tumour samples of the portec - 3 participants might identify those who could most benefit from chemotherapy or targeted agents and individualise treatment of women with highrisk endometrial cancer.38 vol 19 march 2018 articles in conclusion , although treatment with chemoradiotherapy significantly improved 5 - year failure - free survival for patients with high - risk endometrial cancer compared with radiotherapy alone , there was no significant difference in overall survival . 
for each patient , the cost in terms of increased toxicity and longer treatment duration should be weighed against the benefit in terms of improvement in failure - free survival . 
however , in view of the higher risk of recurrence among women with stage iii disease , this chemoradiotherapy schedule should be considered to maximise failure - free survival , and benefits and risks should be individually discussed . contributors clc was the chief investigator of the trial . 
all authors contributed to the manuscript and approved the final manuscript . declaration of interests we declare no competing interests . acknowledgments the portec - 3 study was supported by a grant from the dutch cancer society ( ul20064168 / ckto 200604 ; the netherlands )  . 
 participation in the portec - 3 trial by anzgog and trog were supported by the nhmrc project grant 570894 ( 2008 ) and by a cancer australia grant ( awarded through the 2011 round of the priority - driven collaborative cancer research scheme and funded by cancer australia )  . 
the portec - 3 trial involved a strong international collaboration within the gynaecological oncology intergroup ( gcig ) and the support of the gcig officers and member groups is gratefully acknowledged . 
this study was presented in part at the annual meeting of the american society of clinical oncology ( chicago , il , usa ; june 26 , 2017 )  . corrections correction to lancet oncol 2014 ; 15 : 1324 correction to lancet oncol 2015 ; 16 : 324 correction to lancet oncol 2015 ; 16 : 499508 zapatero a , guerrero a , maldonado x , et al . 
high - dose radiotherapy with shortterm or long - term androgen deprivation in localised prostate cancer ( dart01 / 05 gicor ) : a controlled , randomised , phase 3 trial . 
in the fth paragraph in the results section , the number of patients in the short - term group who died of cancer , but not of the prostate , should read 14 ( 8% ) and the number in the long - term group should read three ( 2% )  . 
ramucirumab versus placebo second - line folfiri in patients with metastatic colorectal carcinoma that progressed during or after rst - line therapy with bevacizumab , uoropyrimidine ( raise ) : a randomised , double - blind , multicentre , phase 3 study . 
 lancet oncol 2014 ; 15 : 131931in gure 3 of the article , the prevalence of hpv type 18 in oral cavity in africa should read 18% , and in oropharynx in oceania hpv type 18 should appear as the second most common type after 16 , and before 35 , with a prevalence of 17% . 
 vol 16 june 2015 e262 correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
we report the long - term follow - up of the ibis - i trial , in which the participants and investigators remain largely masked to treatment allocation . methods in the ibis - i randomised controlled trial , premenopausal and postmenopausal women 3570 years of age deemed to be at an increased risk of developing breast cancer were randomly assigned ( 1 : 1 ) to receive oral tamoxifen 20 mg daily or matching placebo for 5 years . 
after a median follow up of 160 years ( iqr 141176 ) , 601 breast cancers have been reported ( 251 [ 70% ] in 3579 patients in the tamoxifen group vs 350 [ 98% ] in 3575 women in the placebo group ; hazard ratio [ hr ] 071 [ 95% ci 060083 ] , p < 00001 )  . 
the risk of developing breast cancer was similar between years 010 ( 226 [ 63% ] in 3575 women in the placebo group vs 163 [ 46% ] in 3579 women in the tamoxifen group ; hazard ratio [ hr ] 072 [ 95% ci 059088 ] , p = 0001 ) and after 10 years ( 124 [ 38% ] in 3295 women vs 88 [ 26% ] in 3343 , respectively ; hr 069 [ 053091 ] , p = 0009 )  . 
the initial report showed a signi cant reduction ( odds ratio [ or ] 068 [ 95% ci 050092 ] ) for all types of breast cancer ( including ductal carcinoma in situ ) after a median followup of 42 years ( iqr 267558 ) .6 after a median follow - up of 8 years ( iqr 635961 ) , an updated report showed the signi cant reduction for all types of invasive breast cancer continued ( risk ratio 073 [ 95% ci 058091 ] ) with tamoxifen.7 in both reports , a risk reduction by tamoxifen was only seen for oestrogen receptor - positive breast cancer and ductal carcinoma in situ . 
as has been reported vol 16 january 2015 articles elsewhere , 5 , 9 , 11 , 12 thromboembolic and gynaecological adverse events were increased with tamoxifen compared with placebo during active treatment , but the 8 - year update showed that those side - e ects were mainly con ned to the active treatment period.5 , 7 with the exception of the royal marsden trial , in which median follow - up was 13 years , 5 follow - up has been limited to 10 years or less for all other reports . 
in this article , we report an updated analysis of the ibis - i trial , which remains largely masked to treatment allocation . methods study design and participants for this randomised controlled trial , eligible women 3570 years of age from 37 centres ( genetics clinics and breast care clinics ) in eight countries ( the uk , australia , new zealand , finland , spain , switzerland , belgium , and ireland ; appendix p 2 ) and judged to be at increased risk of developing breast cancer were enrolled and randomly assigned in a 1 : 1 ratio to receive oral tamoxifen 20 mg daily or matching placebo for 5 years ( appendix p 3 )  . 
speci c details about eligibility , entry , and exclusion criteria have previously been described in full.6 , 7 in brief , women had to have risk factors for breast cancer indicating at least a twofold increased risk for the disease in women aged 4570 years , whereas this risk needed to be higher than twofold for those younger than 45 years of age . 
women with a history of any invasive cancer ( excluding skin cancer ) , deep vein thrombosis , pulmonary embolism , or who wanted to become pregnant were excluded from trial participation . 
 the trial was approved by local ethics committees for each participating centre . procedures women were actively followed up for 5 years in the clinic or by telephone at 6 - monthly intervals . 
in the non - uk centres , annual questionnaires , annual clinic visits , or hospital notes were used to collect these data , supplemented by a national registry in finland . 
an option was given to women who had not developed breast cancer after a minimum of 10 years follow - up on ibis - i to take additional preventive therapy through enrolment into the ibis - ii trial.13 randomisation and masking randomisation was done centrally by the ibis study group ( with no external input ) by telephone or fax to a central o ce in london , uk , for the european centres and in sydney , australia , for the centres in australia and new zealand . 
initial blocks of eight were created and were then randomly permuted into blocks of six or ten , to ensure that the nal entry in each block was not predictable . 
 all ibis - i personnel , participants , and clinicians were masked to treatment allocation and only the ibis - i trial statistician ( is ) had access to unmasked data . outcomes the primary endpoint was the occurrence of any type of breast cancer ( including ductal carcinoma in situ )  . 
 secondary endpoints included the occurrence of invasive oestrogen receptor - positive breast cancer , all - cause morta lity , and adverse events . statistical analysis the cuto date for this analysis was may 1 , 2014 , and events that occurred after this date were not included . 
we checked proportionality using schoenfeld residuals16 and we estimated survival curves using the kaplan - meier method.17 women who joined the ibis - ii trial and were randomly allocated to active treatment ( anastrozole ) were censored at that point . 
the corresponding author had access to all the data and had nal responsibility for the decision to submit for publication . vol 16 january 2015 articles vol 16 january 2015 articles results between april 14 , 1992 , and march 30 , 2001 , 7169 women were initially enrolled into the trial and randomly assigned to the two treatment groups . 
15 women were subsequently found to be ineligible because of previous breast cancer diagnosis ( nine of those assigned to placebo and six assigned to tamoxifen ) , leaving a total of 7154women in the trial ( 3579 in the tamoxifen group and 3575 in the placebo group )  . 
median follow - up for this analysis was 160 years ( iqr 141176 ) , and a total of 110 043 women - years of follow - up have been accrued ( tamoxifen : 55 419 , placebo : 54 624 )  . 
most women ( 6639 [ 93% ] of 7154 ) have had more than 10 years of follow - up , and the cumulative number of women - years of follow - up are 69 074 before 10 years and 40 969 thereafter . 
4002 ( 56% ) of 7154 had a body - mass index ( bmi ) higher than 25 kg / cm , and 2876 ( 40% ) of 7154 used menopausal hormone therapy at some point during the active treatment phase of the trial . 
most women ( 6939 [ 97% ] of 7154 ) were entered into the trial because of a family history of breast cancer , but a few ( 572 [ 8% ] ) were enrolled on the basis of having a benign breast lesion associated with increased breast cancer risk . for investigators largely masked at the time of data cuto , treatment allocation still remains and participating women who have not developed breast or any other cancer ( 2702 [ 755% ] of those assigned to tamoxifen vs 2646 [ 740% ] of those who received placebo )  . 
 after 10 years follow - up , 603 women joined the ibis - ii trial , of whom 302 were randomly assigned to anastrozole and were censored at that time . a total of 601 breast cancers were reported before the cuto date of may 1 , 2014 ( 251 [ 70% ] in 3579 women in the tamoxifen group vs 350 [ 98% ] of 3575 in the placebo group ; table 1 )  . 
we found a signi cant reduction in the occurrence of all breast cancers in the tamoxifen group compared to the placebo group ( hr 071 [ 95% ci 060083 ] , p < 00001 )  . 
we observed a signi cant reduction in the rst 10 years of follow - up ( hr 072 [ 95% ci 059088 ] , p = 0001 ) , which was slightly greater in subsequent years ( 069 [ 053091 ] , p = 0009 )  . 
figure 1 shows the kaplan - meier - based cumulative incidence curves for all breast cancers ( and for oestrogen receptorpositive invasive cancers ) according to follow - up period . 
 after 20 years of follow - up , the estimated risk of developing all types of breast cancer was 123% ( 95% ci 101145 ) in the placebo group compared with 78% ( 95% ci 6990 ) in the tamoxifen group , indicating that the number needed to treat for 5 years to prevent one breast cancer in the next 20 years was 22 ( 95% ci 1926 )  . 
 figure 2 shows the hazard rates by year for tamoxifen and placebo and con rms the continuing bene t of tamoxifen versus placebo over the entire 20 - year follow - up period . 
a test for proportionality of hazards indicated no departure from the proportional hazards assumption during the entire follow up period ( p = 09 )  . a similar pattern was observed for invasive oestrogen ( table 1 , gure 1 )  . 
 receptor - positive breast cancer a signi cant reduction in cancer occurrence with tamoxifen was recorded in the rst 10 years of follow - up , which was maintained in subsequent years ( table 1 , gure 2 )  . 
the number needed to treat to prevent one invasive oestrogen receptor - positive breast cancer was 29 ( 95% ci 2634 )  . a signi cant reduction for tamoxifen was also recorded for ductal carcinoma in situ , but only in the rst 10 years of follow - up ( table 1 )  . 
there were more oestrogen receptor - negative breast cancers the tamoxifen group after 10 years of follow - up than in the placebo group ( ten cancers in the tamoxifen group vs four in the placebo group ; hr 245 [ 077782 ] , p = 013 )  . 
 the preventive e ects of tamoxifen did not di er according to tumour size , nodal status , or grade , since there was substantial overlap in the con dence intervals and no signi cant trends ( table 1 , appendix p 4 )  . women who had menopausal hormone therapy during the 5 years of active treatment had signi cantly less bene t from tamoxifen than those who did not ( p = 004 ; table 1 , gure 3 )  . 
this e ect was larger for women who developed invasive oestrogen receptor - positive cancers ( users of menopausal hormone therapy hr 087 [ 95% ci 064119 ] vs non users 055 [ 042072 ] ; p = 003 )  . 
there was no signi cant di erence between women aged 50 years or younger than in older women throughout the follow - up periods ( table 1 , gure 3 )  . 
no interactions were recorded with other demographic factors ( appendix p 4 )  . 123% 83% 78% 63% 49% 43% 33% 21% follow - up ( years ) number at risk placebo tamoxifen 3575 3579 3527 3542 3474 3495 3410 3446 3358 3385 3296 3344 3239 3293 2850 2890 1901 1918 figure 1 : cumulative incidence of breast cancers over time all breast cancers ( solid lines ) and invasive oestrogen receptor - positive breast cancers ( dashed lines ) , according to treatment group and duration of follow - up . vol 16 january 2015 placebo tamoxifen articles placebo tamoxifen follow - up ( years ) figure 2 : smoothed annual hazard rate curves for breast cancer all breast cancers ( solid lines ) and invasive oestrogen receptor - positive breast cancers ( dashed lines ) , according to treatment group . all breast cancer 010 years 10 years ductal carcinoma in situ 010 years 10 years invasive cancer 010 years 10 years age ( 50 years ) 010 years 10 years age ( > 50 years ) 010 years 10 years no menopausal hormone therapy 010 years menopausal hormone therapy 010 years 10 years 10 years overall in total , 666 cancers other than breast cancer were reported ( table 2 )  . 
315 ( 8% ) other cancers occurred in women in the placebo group compared with 351 ( 9% ) in the tamoxifen group ( or 113 [ 096132 ] , p = 03 ) ( table 2 )  . 
although not signi cant , there were more endometrial cancers in the tamoxifen group than the placebo group , but the excess was con ned to the rst 5 years of active treatment , with no subsequent di erence ( table 2 )  . 
 signi cantly fewer gastrointestinal cancers occurred in women receiving tamoxifen than in those receiving placebo ( 42 in the tamoxifen group vs 63 in the placebo group ; or 066 [ 95% ci 044099 ] , p = 0038 ; table 2 )  . 
 non - melanoma skin cancers were signi cantly increased in the tamoxifen group , whereas there was a similar incidence of melanoma skin cancers between the two treatment groups ( table 2 )  . 
more cases of lung cancer were reported with tamoxifen ( 32 cases ) than with placebo ( 24 cases ) , although this di erence was not signi cant and was only observed in the rst 10 years of follow - up ( table 2 )  . 
no speci c treatment or time - period di erences were recorded for other cancers ( table 2 )  . information further data about minor side - e ects were not recorded since the last publication7 because no e ects were anticipated to occur more than 5 years after completion of treatment . 
at last data cuto ( may , 2014 ) , there was a signi cantly higher incidence of deep vein thrombosis in women receiving tamoxifen than those receiving placebo ( 50 [ 14% ] of 3579 women receiving tamoxifen vs 29 [ 08% ] of 3575 women receiving placebo ; or 173 [ 95% ci 107285 ] , p = 002 ; appendix p 3 )  . 
no signi cant di erences between treatment groups were recorded for major cardiovascular events ( 13 [ < 1% ] of 3579 women in the tamoxifen group vs 17 [ < 1% ] of 3575 women in the placebo group ; or 076 [ 95% ci 034167 ] , p = 046 ) or cerebrovascular accidents ( 30 [ 1% ] tamoxifen vs 28 [ 1% ] placebo ; 107 [ 062186 ] , p = 080 )  . a total of 348 deaths were reported up until the cuto date ( 182 [ 51% ] of 3579 women in the tamoxifen group and 166 [ 46% ] of 3575 women in the placebo group ; table 3 )  . 
 the higher number of deaths in the tamoxifen group were con ned to the rst 10 years of follow - up ( 86 deaths in the tamoxifen group vs 71 in the placebo group ) , and a similar number of deaths were reported thereafter ( 96 tamoxifen vs 95 placebo )  . 
 overall , tamoxifen had no e ect on breast cancer - speci c mortality ( 31 deaths with tamoxifen vs 26 with placebo ; or 119 [ 95% ci 068210 ] , p = 08 )  . 
a few more breast 025 071 hazard ratio favours tamoxifen favours placebo figure 3 : forest plot for subgroup analyses according to follow - up periods ( 010 years vs 10 years ) horizontal lines are 95% cis . cancer deaths occurred in the tamoxifen group after 10 years of follow - up , although this di erence was not signi cant ( 18 tamoxifen vs nine placebo ; or 200 [ 085506 ] , p = 008 )  . 
 this nding was not reported in the royal marsden trial5 , 9 or in the italian trial ( the italian tamoxifen prevention study ) , 11 , 12 and menopausal hormone therapy use was not allowed in the nsabp - p1 trial.3 , 4 understanding how the type and duration of menopausal hormone therapy a ects breast cancer risk is thus an important question that has to be addressed . 
in the overview of selective oestrogen receptor modulators , 10 the e ect of tamoxifen and other selective oestrogen receptor modulators for ductal carcinoma in situ was largely restricted to the rst 5 years , with little e ect in years 510 , but no data are available after 10 years . 
the relevance of this for breast cancer prevention is not clear , but since ductal carcinoma in situ is a precursor lesion , it could indicate that the preventive e ect of tamoxifen will not be maintained inde nitely . all women have completed the active follow - up portion of this trial , but continue to be monitored by a range of methods . 
in the uk and finland , where 4412 ( 617% ) of the participants were recruited , follow - up is covered by national agging systems and so will be essentially complete for cancer and death . 
for australia and new zealand ( 2676 [ 374% ] of cases ) , annual questionnaires were used for all participants ( four tamoxifen vs two placebo ; p = 042 )  . 
five women in the tamoxifen group died from endometrial cancers ( four within the rst 10 years ) compared with none in the placebo group ( p = 006 )  . 
we recorded no signi cant di erences in other cancers or causes of death , although there was a non - signi cant increase in respiratory deaths occurred tamoxifen group after 10 years ( 13tamoxifen vs six placebo ; or 217 [ 95% ci 077696 ] , p = 01 )  . the increase in oestrogen discussion this extended analysis of the ibis - i trial provides important evidence showing that 5 years of tamoxifen treatment reduces the incidence of breast cancer for at least 20 years . 
in the current report with 16 - year median follow - up , the number of breast cancers has almost doubled to 601 , of which 212 ( 35% ) have occurred after 10 years of follow - up . 
an increase in these tumours was also seen in the selective oestrogen receptor modulator metaanalysis but only in years 510 , 10 which was signi cant for all selective oestrogen receptor modulators ( p = 002 ) , but not for tamoxifen alone ( p = 04 )  . 
this nding could be due to tumours that would have presented earlier as oestrogen receptor - positive cancers , but were transiently held in check by tamoxifen , and then later escaped the need for hormonal stimulus and subsequently appeared as oestrogen receptor - negative cancers . 
the reason for a di erence between early and late e ects is unclear , but that trial randomly assigned a group of women who were younger and at higher risk of breast cancer than those in our trial , which could be relevant . 
nevertheless , the agreement between these two trials regarding the long - term e ectiveness of tamoxifen is important and provides strong evidence for a long - lasting reduction in number of cases of breast cancer . the bene t of tamoxifen was signi cantly greater in women who did not use menopausal hormone therapy during the treatment period than in those who used this therapy , indicating the clear loss of e cacy of tamoxifen vol 16 january 2015 articles panel : research in context systematic review a systematic review of the use of tamoxifen and other selective oestrogen receptor modulators for breast cancer prevention has recently been published , 10 but contained follow - up for only 10 years . 
this review included the four randomised trials ( including the present ibis - i trial ) that have reported about the use of tamoxifen for prevention of breast cancer.37 , 9 , 11 , 12 we identi ed one only trial ( the royal marsden trial ) with follow - up beyond 10 years , 5 but the number of breast cancers after 8 years in this trial was only 94 , compared with 212 after 10 years for ibis - i in our report . interpretation the results from the present trial provide important additional evidence that 5 years of tamoxifen treatment reduces the incidence of breast cancer in high - risk women for the entire follow - up period . 
no e ect on all - cause or breast cancer mortality was recorded , but an increase in deaths from endometrial cancer was con rmed as noted in the adjuvant trials.18 our results substantially improve the bene t - to - harm ratio for the use of tamoxifen to prevent breast cancer in high - risk women , with an estimated 22 women being needed to be treated for 5 years to prevent one breast cancer in the next 20 years . except for 44 women who have withdrawn consent for additional follow - up ( and these women were censored at that time )  . 
additionally , for this analysis we obtained up - todate clinical follow up for the remaining few cases in switzerland and belgium ( 63 [ 09% ] of cases )  . 
data about other major but non - fatal side - e ects ( eg , strokes and myocardial infarctions ) are substantially complete but are not covered by national agging systems and so are only obtained from clinic visits , note review , and postal questionnaires . 
data for minor side - e ects ( eg , vasomotor symptoms or gynaecological events ) were reported after 8 years median follow - up , 7 and since these were mostly con ned to the active treatment period they have not been collected beyond 10 years of follow - up . overall there was no signi cant di erence in all - cause mortality between treatment groups , and the excess of death in the tamoxifen group was smaller than in previous reports.6 , 7 the number of deaths was very similar in the two groups after 10 years . 
despite there being no signi cant di erence in the number of deaths from breast cancer between treatment groups , there were more deaths from breast cancer in the tamoxifen group ; this outcome could not be linked to use of menopausal hormone therapy or the occurrence of oestrogen receptornegative breast cancer . 
 however , deaths from endometrial cancer were more frequent in the tamoxifen group ( ve ) than in the placebo group ( none ) , and all but one occurred after 5 years of active treatment . 
excess deaths from endometrial cancer have also been reported in the overview of adjuvant tamoxifen trials , 18 with an annual rate slightly higher than reported here ( 19 vs 11 per 10 000 women - years ) , which at least partly represents the higher number of postmenopausal women in the adjuvant studies . 
these rates do not adjust for women who had undergone a hysterectomy , so the risk in women with a uterus would be about 50% higher than those reported here in ibis - i . 
 the apparent , although not statistically signi cant , excess of deaths from respiratory causes has not been reported in the overview of tamoxifen adjuvant trials , with only two respiratory deaths recorded in the 15 - year follow - up18 ( pan h , university of oxford , uk , personal communication ) , so this nding might well be due to chance alone . the fact that the reduced incidence of breast cancer with tamoxifen has not translated into a mortality reduction is of some concern . 
however , the ratio of deaths from breast cancer ( 57 ) to incident cases of breast cancer ( 601 ) is only 95% , so the power for analysis of mortality ( which our study was not powered to assess ) is much lower than that for incidence . 
we previously estimated that the recorded reduction in incidence would lead to an 18% reduction in breast cancer mortality.19 if this were the case , the power to detect such a reduction at this stage ( with two - sided 5% signi cance level ) would be only 12% , so the absence of a signi cant di erence is not surprising . in conclusion , our results clearly show a long - term e ect of 5 years of tamoxifen treatment to prevent breast cancer in the next 20 years . 
no new late toxicity has been identi ed , although the early excess of endometrial cancer in the tamoxifen group has translated into an increased number of deaths , which , although not signi cant in our study , has been reported in adjuvant trials of tamoxifen and therefore is important in making the decision to use the drug . 
these results substantially improve the bene tto - harm ratio for the use of tamoxifen to prevent breast cancer in high - risk women . contributors jc , ah , and jff designed the study . 
is , sc , hh , kh , and ah declare no competing interests . acknowledgments the ibis - i trial was supported in the uk by cancer research uk ( grant c569 / a16891 )  . 
in australia , it was supported by the national health and medical research council by project grant numbers 209811 , 980381 , 950319 , 920876 , awarded to the anz breast cancer trials group , university of newcastle ( callaghan , nsw , australia )  . 
we thank the thousands of women volunteers who have taken part in this study during the past 20 years , and the nurses and clinicians in the local centres for their continuing support . vol 16 january 2015 articles violence , crime , corruption , and cuts in public spending : how to re - establish cancer control in latin america ? october , 2018 , saw the controversial far - right candidate , jair bolsonaro , win 46% of the presidential vote for brazil . 
 although just falling short of a majority , bolsonaro led a successful campaign that capitalised on fear of rising crime and corruption , championed economic freedom through the promise of privatisation , and pledged the relaxing of gun laws . 
although much of this rhetoric resonates with the populist political agenda in recent years , firm commitments to health - care policy were notably absent from his , as well as his opponents , political programmea critical omission at a time when brazil has been hit with economic and structural weakness , political precariousness , and austerity policies that have capped public expenditure on the growth and sustainability of its health - care syste although unified health system brazils ( sus ) has made substantial progress in recent years , a chronic lack of funds , suboptimal resource allocation , and poor organisation and governance , means that it is struggling to deliver its targets . the prohibition of indeed , these problems are not just isolated incidences in latin america . 
the un and the inter - american commission on human rights declared that the health system in venezuela is in a state of crisis as it witnessed the deaths of at least 16 children in one hospital as a result of deteriorating health facilities , poor sanitation , and a shortage of supplies and medicinesno doubt conditions that are symptomatic of a country suffering from extreme economic instability and political weaknesses , compounded by international humanitarian aid . 
further north , mexicoa country that elected the leftist candidate andrs manuel lpez obrador as president - elect earlier this year to combat similar fears of extreme violence , inequality , and corruptionhas seen its public health insurance scheme , seguro popular , suffer from system fragmentation , underfunding , coverage limitations , and corruption . 
similarly , in honduras , the right - wing president juan orlando hernndez has been accused of rigging elections in late 2017 , in which protestors were killed by security forces , while nicaragua is suffering from extreme political instability , with more than 200 killed in political violence earlier this year amid calls for the former guerrilla daniel ortega to leave the presidential palace . cancera disease reliant on stable , well - funded health systems for continuity and consistency in care delivery will inevitably be affected by these political disturbances . 
 indeed , it is ironic that in the lancet oncologys 2015 commission on cancer control in latin america and the caribbean , paul goss and colleagues attributed the success of the human papillomavirus vaccination programme in brazil to widespread immunisation coverage targets and financial buy - in that were secured by the then ministry of healthan initiative that is now at risk of becoming undone should bolsonaro opt for decreased public expenditure and de - centralised financing . 
hopefully , strong advocacy movements , such as those that feature prominently in brazil , will hold the government to account on their legislative obligationsbut these measures should neither be taken as guaranteed , nor should such movements be expected to become the main drivers of change when governments fail to deliver . the developments unfolding in latin america show that the struggle for democracy is no longer a politics of left versus right , realism versus extremism , or truisms versus tropes . 
in the face of such political upheavals , leaders of these nations would do well to remember that the need for cancer care and control remains unchanged , whoever is in power . 
thus , a key priority for any government is to ensure that there are policies and investments for cancer control that are enshrined in law to ensure there is a level and continuum of care that can be safely delivered to its population irrespective of temporal political disruption . the recommended actions from the 2015 commission on cancer control in latin america and the caribbean still stand today . 
consolidating fragmented health systems , focusing palliative care , improving national cancer registries and cancer control plans , increasing healthcare expenditure , training of oncology and palliative care specialists , and addressing disparities in cancer control are still essential components of effective cancer health systems . 
but only if governments , irrespective of individual party politics , recognise , respond to , and prioritise cancerand indeed all non - communicable diseasesas a persistent and growing health burden , will the fragility of health systems and the needless loss of life be overcome . 
 to inform public health policy and future research , we estimated the global burden of cancer attributable to high bmi in 2012 . methods in this population - based study , we derived population attributable fractions ( pafs ) using relative risks and bmi estimates in adults by age , sex , and country . 
assuming a 10 - year lag - period between high bmi and cancer occurrence , we calculated pafs using bmi estimates from 2002 and used globocan2012 data to estimate numbers of new cancer cases attributable to high bmi . 
we did secondary analyses to test the model and to estimate the e ects of hormone replacement therapy ( hrt ) use and smoking . findings worldwide , we estimate that 481 000 or 36% of all new cancer cases in adults ( aged 30 years and older after the 10 - year lag period ) in 2012 were attributable to high bmi . 
the burden of attributable cases was higher in countries with very high and high human development indices ( hdis ; paf 53% and 48% , respectively ) than in those with moderate ( 16% ) and low hdis ( 10% )  . 
a quarter ( about 118 000 ) of the cancer cases related to high bmi in 2012 could be attributed to the increase in bmi since 1982 . interpretation these ndings emphasise the need for a global e ort to abate the increasing numbers of people with high bmi . 
 recent statistics showed that 35% of the adult population ( aged 20 years and older ) worldwide is overweight ( bmi 25 kg / m ) , including 12% that is classi ed as obese ( bmi 30 kg / m ) .1 the prevalence of high bmi ranges from about 10% in many asian and african countries to more than 90% in paci c island nations such as the cook islands and nauru . 
according to recent estimates , 1 , 2 the global prevalence of excess bodyweight in adults increased by 275% between 1980 and 2013 , although the increase has slowed in recent years in some european countries and the usa.37 continuous updates of the scienti c literature have con rmed the association between high bmi and risk of oesophageal adenocarcinoma and colon , rectal , kidney , pancreas , gallbladder ( women only ) , postmenopausal breast , ovarian , and endometrial cancers.813 the estimated increase in risk of these cancers due to high bmi ranges from 3% to 10% per unit increase in bmi.14 a recent estimate from global burden of disease ( gbd ) study15 showed that 39% of cancer mortality in 2010 could be attributed to high bmi . 
additionally , relating risk factors to mortality in the estimation of disease burden can be problematic because of the potential role of reverse causation.16 potential confounders and e ect modi ers of the association between bmi and cancer , such as the use of hormone replacement therapy ( hrt ) and smoking , also need to be taken into account.17 , 18 in this study , we aimed to estimate the global population attributable fraction ( paf ) of cancer incidence in 2012 attributable to high bmi in 2002 , acknowledging the time lag between the exposure ( high bmi ) and outcomes ( cancer incidence )  . 
we also aimed to test the robustness of the estimates in a series of sensitivity analyses , including assessment of the role of smoking and hrt use as potential e ect modi ers or confounders of the association between high bmi and cancer incidence . vol 16 january 2015 articles see online for appendix methods study design in this population - based study , we quanti ed the e ect of high bmi on cancer incidence in the adult population worldwide , the e ect of various model assumptions , and assessed the e ect of confounders and e ect modi ers . 
we applied pafs according to sex , age , cancer site , and country to national estimates of cancer incidence estimates , using data for mean bmi , cancer incidence , and corresponding risk estimates . 
 tested we used the bmi estimates reported by global burden of metabolic risk factors of chronic diseases collaborating group.1 the details of the applied model and its assumptions in the estimation of mean bmis have been reported elsewhere.19 for this study , we obtained the annual estimates of mean bmi and the corresponding sds for adults aged 20 years and older for each country by sex and age group ( 2034 , 3544 , 4554 , 5564 , 6574 , and 75 years ) in 1982 and 2002 ( appendix pp 27 )  . in our primary analysis , we included only cancers reported by the world cancer research fund ( wcrf ) as having su cient evidence to be associated with high bmi.813 these include oesophageal adenocarcinoma and colon , rectal , kidney , pancreatic , gallbladder , postmenopausal breast , corpus uteri , and ovarian cancers , collectively de ned here as high - bmi - related cancers . 
similarly , only adenocarcinoma of the oesophagus was included because of the absence of an association between excess bodyweight and oesophageal squamous - cell carcinoma . the sex - speci c relative risks ( rrs ) for the sites included in the analysis were obtained from the standardised metaanalysis estimates by renehan and colleagues14 and the wcrf continuous update project.813 in these metaanalyses , risk estimates were pooled from from cohort studies that mainly used cancer incidence as an outcome ( apart from pancreatic cancer , for which studies included mortality as an outcome )  . 
in a secondary analysis we included thyroid cancer and non - hodgkin lymphoma as additional cancer sites , which might be associated with high bmi , 14 , 20 but were not listed by wcrf as having su cient evidence . 
the exact sources and sizes of rrs are described in the appendix ( pp 89 )  . calculation of paf we calculated pafs on the basis of the approach suggested by the comparative risk assessment collaborative group , using the formula : 21 rr ( x ) p ( x ) dx rr ( x ) p * ( x ) dx paf = rr ( x ) p ( x ) dx where p ( x ) is the population distribution of bmi , p * ( x ) is the distribution of theoretical minimum bmi , rr ( x ) is the rr of cancer associated with bmi , and dx indicates that the integration was done with respect to bmi . 
the theoretical minimum distribution of bmi was de ned as a bmi distribution with a mean of 22 kg / m and an sd of 1 kg / m , at which the disease burden is assumed to be lowest at the population level.15 , 22 we used a log - logit function to characterise the shape of the rr across bmi units . 
furthermore , we assumed no risk for bmi less than 22 and no risk increase for bmi greater than 40 , since estimates of rr beyond these points were scant . 
a pictorial illustration and a more detailed description of these assumptions of the risk function are presented in the appendix ( pp 89 )  . we calculated age - speci c , sex - speci c , and countryspeci c pafs for individual high - bmi - related cancer sites . 
we then derived the number of cancer cases attributable to high bmi by multiplying age - speci c , sexspeci c , country - speci c , and cancer - speci c pafs by the corresponding numbers of incident cancers in 2012 . 
we calculated overall national , regional , and global estimates of the total attributable proportion of cancer related to high bmi by summing the numbers of attributable incident cases and dividing them by the total number of cancer cases in each subgroup . we estimated 90% uncertainty limits for pafs using monte carlo simulation . 
we also computed a counterfactual scenario ( ie , a model of incidence if mean bmis had remained at their 1982 values ) to provide a more realistic view about the preventable proportion of the current burden of cancers caused by high bmi . 
the analysis was done by replacing the theoretical minimum distribution with the bmi distribution that was reported in in 1982 , an attainable value in the past in each country and probably a more realistic goal for prevention than the mean bmi of 22 kg / m used in our main analysis . 
renehan and colleagues28 assumed a 10 - year lag time on the basis of the scienti c literature , wherein the average follow - up time of 10 years showed the bene cial e ect of weight loss on subsequent cancer risk.29 , 30 with no additional information available , we chose to assume a 10 - year lag period in this study , mapping high bmi prevalence in 2002 ( by sex , age , and country ) to cancer incidence in 2012 . sensitivity analyses in estimating the pafs of cancers attributable to high bmi , we made several assumptions about the population bmi distribution and the rrs function . 
to assess their e ect on the results , we repeated the analyses while changing the following assumptions : exposure de nition ( categorical vs continuous bmi ; appendix pp 1314 ) ; bmi distribution ( normal vs log - normal ; appendix pp 1516 ) ; shape of the rr ( linear or log - linear vs log - logit ; appendix pp 1719 ) ; and region - speci c versus global rr estimates ( appendix pp 2023 )  . 
because smoking3134 and use of hrt8 , 11 , 35 are known e ect modi ers of the association between bodyweight and cancer , we estimated pafs strati ed by current smoking status ( for pancreatic cancer ) or hrt use ( for postmenopausal breast cancer , ovarian cancer , and endometrial cancer ) and assessed the bias that might have occurred when these interactions were ignored ( appendix pp 2427 )  . 
furthermore , because studies have shown a protective e ect of high bmi on premenopausal breast cancer , 8 , 14 , 36 we also assessed the potentially adverse e ects of decreasing population bmi on the incidence of premenopausal breast cancer and its e ect on the total paf ( appendix pp 2830 )  . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results worldwide , our result show that an estimated 481 000 or 36% of all new cancers ( or 128% of all high - bmirelated cancers ) in adults in 2012 were attributable to high bmi . 
by sex , 136 000 ( 19% ) new cancers in men ( table 1 ) and 345 000 ( 54% ) in women ( table 2 ) were vol 16 january 2015 articles attributable to high bmi . 
the attributable burden was larger in countries with very high and high hdis ( paf 53% and 48% , respectively ) than in those with moderate ( 16% ) and low ( 10% ) hdis . region - speci c estimates show that all three asian regions and sub - saharan africa had the lowest pafs , ranging from 04% to 09% of total cancers ( 36% to 60% of total high - bmi - related cancers ) in men and 17% to 30% of total cancers ( 54% to 83% of total high - bmi - related cancers ) in women . 
north america had the highest pafs , at 35% of total cancers ( 208% of high - bmi - related cancers ) for men and 94% of total cancers ( 192% of high - bmi - related cancers ) for women . 
 for the remaining regions ( middle east and north africa , latin america and the caribbean , oceania , and all european regions ) , the paf ranged from 20% to 99% of total cancers ( 144% to 182% of high - bmi - related cancers ) in both sexes . with respect to the regional contribution to new highbmi - related cancers in 2012 , the north american region contributed the most ( 111 000 or 230% of the total worldwide cases attributable to high bmi ) , and subsaharan africa the least ( 7300 or 15% ; tables 1 , 2 )  . 
 eastern europe had the greatest share of attributable paf ( % ) 31 < 55 20 < 31 10 < 20 03 < 10 00 < 03 no data women paf ( % ) 85 < 127 66 < 85 39 < 66 16 < 39 04 < 16 no data figure 1 : paf of new cancer cases in 2012 caused by high bmi in men and women , by country paf = population attributable fraction . vol 16 january 2015 articles north america 1538 northern europe 1600 western europe 1663 oceania 1648 southern europe 1532 eastern europe 1433 267 249 243 252 214 174 582 427 387 400 352 385 latin america and the caribbean middle east and north africa east asia southeast asia sub - saharan africa south - central asia 636 539 807 444 234 218 206 221 1707 1404 1256 1097 862 761 incidence rate 3524 3306 3159 2990 2692 2501 women figure 2 : age - standardised incidence rate of high - bmi - related cancers and high - bmi - related cancers attributable to high bmi ( per 100 000 people ) in 2012 incidence data are age - standardised to the world standard population . 
light bars show total incidence rates of high - body - mass - index ( bmi ) - related cancers , and dark bars show those attributable to high bmi . burden among the european regions ( 66 000 or 338% of the total european cases attributable to high bmi )  . 
 despite the low paf ( 18% ) , the east asia region had the second largest number of cases attributable to high bmi ( 70 000 ) after north america , because of its large population size . country - speci c pafs for men and women are shown in gure 1 and in the appendix ( pp 3440 )  . 
the greatest between - country di erences within a region were in latin america and the caribbean , where the paf ranged from 45% in argentina to 07% in haiti and jamaica . 
in women , barbados had the highest paf , with 127% of cancers attributable to high bmi , followed by the czech republic ( 120% ) and puerto rico ( 116% )  . 
as for men , between - country di erences were largest in latin america and the caribbean , where the paf ranged from 127% in barbados to 16% in haiti . 
countries in sub - saharan africa had consistently lower overall pafs than those in other regions , of less than 2% in men and less than 4% ( with the exception of mauritius and south africa ) in women . paf also varied greatly by cancer site , ranging from 62% for rectal cancer to 333% for oesophageal adenocarcinoma in men and from 36% for rectal cancer to 340% for cancer of the corpus uteri and oesophageal adenocarcinoma in women ( tables 1 , 2 )  . 
despite having a large estimated paf of more than 30% , oesophageal adenocarcinomas accounted for only 14 000 ( or 100% ) of the total worldwide cancer cases attributable to high bmi in men and 4000 ( or 11% ) in women . 
in women , the postmenopausal breast cancer and cancer of the corpus uteri contributed about two - thirds of the new cancer cases attributable to high bmi ( 221 000 )  . we noted substantial di erences between men and women in pafs for colon cancer ( 130% vs 76% )  . 
sex di erences in the numbers of attributable cases were largest for colon cancer and oesophageal adenocarcinoma , with 56 000 and 14 000 attributable cases , respectively in men and only 29 000 and 4000 attributable cases in women ( tables 1 , 2 )  . 
particularly , in regions with a fairly low incidence of high - bmi - related cancers , such as asia and sub - saharan africa , the proportion of new cancer cases attributable to high bmi was two to three times greater for women than for men . in our counterfactual scenario , we calculated that if bmi had remained as recorded in 1982 , about a quarter ( 118 000 cases ) of cases of high - bmi - related cancers in 2012 could have been averted . 
in other words , a quarter of all high - bmi - related cancers could be attributed to the increase in bmi between 1982 and 2002 ( appendix pp 3133 )  . 
in a high - burden region such as north america , this proportion translated into more than 40 000 cases , or 356% of all attributable cancer cases that could be linked to the increase in bmi since 1982 . 
with respect to speci c cancer sites , about 107% of all oesophageal adenocarcinomas ( 5600 ) , 85% of all corpus uteri ( 27 000 ) , 49% of all kidney ( 15 000 ) and 25% of all postmenopausal breast cancers ( 28 000 ) could have been avoided if bmi had not increased between 1982 and 2002 . vol 16 january 2015 articles when paf for pancreatic cancer was corrected for smoking status , we estimated that it ranged between 06% and 183% for both men and women ( appendix pp 2425 ) , dependent on country . 
 hrt non - users had substantially higher pafs than hrt users ; pafs for hrt non - users ranged from 504% to 650% for corpus uteri cancer and from 83% to 124% for postmenopausal breast cancer and ovarian cancer , dependent on country . 
for hrt users , we noted pafs between 86% and 208% for corpus uteri cancer and pafs below 0% for postmenopausal breast and ovarian cancers , because of slightly protective rrs ( appendix pp 2627 )  . 
when comparing the pafs corrected for hrt use to the unadjusted pafs , the di erence was small for most countries , ranging from 0 to 14 percentage points for corpus uteri cancer and from 0 to 5 percentage points for postmenopausal breast and ovarian cancers . 
the di erence was larger in countries where the prevalence of hrt use was low ( < 55% ) and a large proportion of women had high bmieg , germany and russia . the results for thyroid cancer , non - hodgkin lymphoma , and premenopausal breast cancer are reported in the appendix ( pp 2830 )  . 
in the sensitivity analyses , the choice of bmi data type and distribution did not substantially a ect the results ( appendix pp 1316 ) , although pafs changed with the use of di erent rr functions ( appendix pp 1719 ) and region - speci c rrs ( appendix pp 2023 )  . discussion our results show that about 36% of all new cancers in adults aged 30 years and older ( excluding non - melanoma skin cancer ) in 2012 , or 128% of high - bmi - related cancers , could be attributed to high bmi . 
postmenopausal breast , corpus uteri , and colon cancer accounted for 725% of the total attributable cases in women , whereas in men kidney and colon cancers accounted 660% of all attributable cases . 
635% of the global cancer cases related to high bmi were in the north american and european regions , although the paf was also large in oceania , latin america and the caribbean , and the middle east and north africa . 
assuming that the association between high bmi and cancer is causal , the continuation of current patterns of population weight gain will lead to continuing increases in the future burden of cancer . 
most importantly , about one quarter of the total cases attributable to high bmi ( 118 000 cancers ) could potentially have been avoided if the global population mean bmi had remained the same as was recorded in 1982 . unequal distribution of cancer cases attributable to high bmi worldwide , we noted substantial di erences within regions ; for example , in latin america and the caribbean pafs for women ranged from 127% in barbados to 16% in haiti . 
although high - bmi - related cancers have become a global issue , 37 the transition from increasing , to stabilising , to possibly decreasing obesity prevalence occurs at di erent rates in di erent countries and regions . 
in a few countries such as the uk and the usa , where bmi increased substantially in the 1980s and 1990s , the bmi increase has since slowed , but in most countries the average bmi has continued to increase steadily since the 1980s.2 the results of our secondary analysis , in which historical bmi was used as an achievable population mean bmi , could be used to measure the changing e ect of bmi on the burden of cancer . 
taking into account both current population mean bmis and their changes over time , the increase in paf has been greatest in the middle east and north africa , latin america and the caribbean , north america , and oceania . 
by contrast , eastern europe maintained a similar ( high ) population mean bmi between 1982 and 2002 , so despite the large current paf , only very few cases are attributable to the change in bmi in that period . 
the varying pattern in bmi distribution and trends across countries emphasises the need for future research into the cumulative e ects of overweight and obesity on the burden of cancer and other chronic diseases . investigators of independent pooled studies3133 have reported an attenuated risk of high bmi in smokers for pancreatic and thyroid cancers . 
in high - income countries such as the uk and the usa , because of the high past prevalence of tobacco smoking38 and high present bmi , 1 the paf of pancreatic cancer related to high bmi was slightly underestimated in our uncorrected analysis . 
by contrast , in low - income countries such as ghana , where smoking prevalence has only started to rise , 39 the e ect of high bmi on pancreatic cancer was slightly overestimated or was not large enough to be appreciable . 
another important e ect modi er in the relation between bmi and cancer is hrt use , wherein the risk of female hormone - driven cancers related to high bmi is largely attenuated or even eliminated among hrt users.8 , 11 , 35 in our sensitivity analysis , we showed that most postmenopausal breast , ovary , and corpus uteri cancers attributable to high bmi occurred among hrt non - users . 
 the falling use of hrt since the early 2000s40 , 41 has contributed to a decrease in breast cancer incidence in countries where use was high ; this decrease in use will probably translate into a higher proportion of cases being attributable to high bmi and therefore amenable to prevention by weight loss . our results show that the issue of cancer burden related to high bmi mainly a ects higher - resource regions , particularly north america and europe . 
 previous studies have quanti ed the global cancer burden vol 16 january 2015 articles attributable to infections ( 2 million new cases in 2008 , paf 161% ) 42 and smoking ( 14 million cancer deaths in 2000 , paf 21% ) .43 ours is the most comprehensive study so far reported to provide worldwide estimates of the burden of cancer due to high bmi ( panel )  . a report from the gbd study15 provided estimates of the burden of cancer due to high bmi , but those results are not directly comparable to ours because paf was presented as a proportion of deaths or disability - adjusted life years attributable to high bmi , whereas incidence was the outcome in our study . 
furthermore , in the gbd study , information about high bmi prevalence and cancer mortality was obtained for the same year , not allowing for a lag between the exposure and cancer development and mortality . 
such di erences in estimates are to be expected , since our estimates are based on more recent data for both the prevalence of high bmi and the incidence of cancer , both of which have increased greatly over the past decade.19 , 47 another strength of this study is the use of age - speci c , sex - speci c , and country - speci c estimates of bmi and latest available estimates of cancer incidence . 
we made many assumptions when estimating the pafs ; however , our sensitivity analyses panel : research in context systematic review we searched medline for articles published in any language up to jan 1 , 2014 , using the search terms obesity , body - mass index , cancer risk , cancer incidence , attributable fraction , avoidable , and preventable . 
we identi ed several studies that provided estimates of the burden of cancer attributable to high body - mass index ( bmi ) in speci c countries or regions , 17 , 28 , 4446 as well as a report15 from the global burden of disease study that included estimates of deaths or disability - adjusted life years attributable to high bmi . 
 however , no previous study had provided global estimates of cancer incidence attributable to high bmi . interpretation our results show that 36% of all new cancers in adults in 2012 ( a total of 481 000 cases ) are attributable to excess bodyweight . 
assuming a causal link between high bmi and cancer incidence , if the current pattern of population weight gain continues , it will lead to further increases future burden of cancer , especially in regions such as latin america and the caribbean and north africa , where the largest increases in the prevalence of obesity have occurred in the past three decades.2 our results should be used to inform health policy in terms of targets for prevention programmes , while emphasising existing gaps in our knowledge about the association between bmi and cancer . showed that changing these assumptions made little di erence to the reported pafs . 
one of the assumptions that we tested was related to the evidence of non - linear associations between bmi and several cancerseg , oesophageal , colon , breast , and endometrial cancers.44 we opted for a log - logit rr function for all cancer sites included in this study instead of a linear function , which partly addressed this issue . 
in the sensitivity analyses , we tested di erent rr functions , which had only small e ects on the nal paf estimates . alongside point estimates for the paf , we presented 90% uncertainty intervals to provide a measure of reliability . 
however , these uncertainties do not take into account uncertainties in the cancer data from the globocan 2012 database , which provides a qualitative ranking of data quality for each country - speci c estimate.23 quanti cation of this uncertainty and incorporation of additional uncertainties the modelling and estimation processes remains a major challenge and therefore was not attempted in our analysis.48 , 49 from another includes this study fatness at limitation of the assumption of constant rrs across very diverse populations . 
the risks of some cancers associated with excess bodyweight have been reported to vary by ethnic group and geographical location.14 , 50 variation exists in the distribution of body fat between ethnic groups and how this is re ected in the bmi measure . 
for example , within the usa , african - american and hispanic women are more likely to be obese than white and asian - american women , yet white and asian - american women have higher body similar bmis.51 other anthropometric measures , such as waist circumference or waist - to - hip ratio , have been suggested as better predictors of obesity - related health outcomes than bmi.52 , 53 furthermore , rural and urban di erences in the prevalence of obesity have been reported.5456 in our study , some variation in the distribution of bmi between ethnic groups might have been captured by our use of countryspeci c bmi estimates . 
 because very little information is available for subnational populations such as ethnic groups and because of the absence of comparable global prevalence data for other anthropometric measures and their risk estimates , we could not do additional analyses to address these issues . another drawback is the assumption of the absence of time - dependent e ects of high bmi on cancer risk , which cannot be completely captured by age - speci c bmi data and lag time . 
we assumed a 10 - year lag in our modelling , but we recognise that the time - related e ects of excess adiposity are likely to vary between cancer types . 
 results from some studies57 , 58 have shown that the risk of cancer from high bmi accumulates with the number of years lived with excess weight , suggesting that the risk can better be predicted from years of life lived with high bmi . 
 / publications / monica / investigators.htm calci cation , a precursor of coronary heart disease.59 although this nding is in line with the biological mechanisms underlying the association between obesity and the development cancer , studies examining this aspect of obesity are a recent development and neither risk estimates nor the exposure information are available for every type of high - bmi - related cancer . igf - 1 , hence promoting lastly , the estimation of the paf is based on the assumption that the association between high bmi and each cancer type included in our study is causal.60 we thus assume that reducing bmi will lead to a reduction in the incidence of these cancers . 
excess bodyweight has been shown to increase circulating levels of oestrogens and bioactivity of the development of cancer.61 however , epidemiological studies that report risk associations between bmi and cancer are prone limitations . 
we have tried to overcome this issue by exclusively using risk estimates based on large meta - analyses that included only highquality studies and , whenever possible , only cohort studies . to several likely to based on our results , historical and continuing increases in the global prevalence of high bmi , especially in younger cohorts , are expected to translate into further increases in cancer burden in the future . 
 the large burden of cancers attributable to high bmi in north america , europe , oceania , latin america and the caribbean , and the middle east and north africa points to the importance of weight - control programmes in these regions . 
it also emphasises the need for research into e ective interventions to control weight gain to avoid further increases in the burden of cancer related to high bmi . contributors ma , np , and is contributed to data collection , study design , analysis , and wrote the rst draft of the report . 
all authors read and approved the nal report . declaration of interests we declare no competing interests . acknowledgments this project was funded by the world cancer research fund international ( grant number sg 2012 / 619 )  . 
jjm is with the cronicas centre of excellence in chronic diseases at cayetano heredia university ( lima , peru ) , supported by federal funds from the us national heart , lung and blood institute ( national institutes of health , department of health and human services ) , under contract number hhsn268200900033c . 
on the one hand , draft guidelines by the uk national institute for health and care excellence ( nice ) did not recommend the use of axicabtagene ciloleucel ( kite pharma / gilead ) for various types of b - cell lymphoma in adults , a decision contrary to the approval of the drug in the eu and by the us food and drug administration . 
on the other hand , nhs england ( in lieu of a formal nice recommendation ) struck a clandestine deal with novartis via the cancer drugs fund to pay for tisagenlecleucel for children and young adults with b - cell acute lymphoblastic leukaemia . 
the deal , agreed less than 10 days after the european approval of the drug , means that patients in england could be the first in europe to gain access to the treatmenta remarkable prospect for the beleaguered nhs . 
taken alone , these results seem promising , but the lack of control group in both trials and the choice of surrogate primary endpoints make the benefits difficult to discern . 
but these differences are misleading and are a consequence of the scant clinical evidence available currently , and the subjective nature of clinical decision making for these specific treatments . the key driver of the nice and nhs england decisions has been cost . 
axicabtagene ciloleucel is believed to cost more than 50 000 per quality - adjusted life - year ( qaly ) gained , which is at the upper limit of tolerance for cancer treatments . 
the manufacturer has proposed a commercial arrangement that might sway the eventual decision in favour of approval , although at the time of writing , nice has requested the manufacturer find more uk data from which a comparison with the current standard of care can be made . 
tisagenlecleucel , by contrast , which is presumably costing less than the 282 000 list price in the arrangement secured by nhs england , might have a more favourable cost per qaly because children have a longer life expectancy than older patients , provided toxicities are manageable and not debilitating . 
ultimately , more robust evidence is needed to be able to make appropriate decisions , but the high prices set by pharmaceutical companies do make it difficult for universal health - care systems to justify cost - effectiveness and treatment availability . 
 developments the lancet oncology immunotherapy in the vol 19 october 2018 1259 editorial corrections correction to lancet oncol 2011 ; 12 : 1051 correction to lancet oncol 2015 ; 16 : 634 , 637 histological sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
 independent lancet oncol 2011 ; 12 : 104552 in the discussion of this article , the second sentence of the fth paragraph should read the proportion of patients a ected by grade 34 fatigue in this study ( 7% ) is similar to that reported for trabectedin ( 78% ) or gemcitabine with docetaxel ( 16% ) .12 , 13 this correction has been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 388 kang hj , loftus s , taylor a , dicristina c , green s , zwaan cm . 
 lancet oncol 2015 ; 16 : 38594 in table 2 of the article , the dose ( mg / kg ) of dexamethasone used in the aprepitant group should read 008 ( 002019 )  . 
this correction has been made to the online version as of aug 31 , 2015 . of medical a airs , from april , 2006 , to december , 2012 , during the design and conduct of the stars trial . 
these cor rections have been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 96778 valle jw , wasan h , lopes a , et al . 
lancet oncol 2015 ; 16 : 96778 in gure 3 of the appendix of this article , parts a and b were mislabelled ; part a shows overall survival data and part b shows progression - free survival data . 
the appendix has been corrected as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 1127 moss sm , wale c , smith r , evans a , cuckle h , duffy sw . 
lancet oncol 2015 ; 16 : 112332in the fourth paragraph of the results section of this article , the absolute mortality reduction in the intervention group should read 003 per 1000 womenyears . 
this correction has been made to the online version as of aug 31 , 2015 and the printed version is correct . chang jy , senan s , paul ma , et al . 
lancet oncol 2015 ; 16 : 63037in this article , the role of the funding source should read : this analysis was designed by the principal and coprincipal investigators of both trials . 
for the stars protocol , accuray speci ed that the cyberknife platform was the sole platform to be used for the study , but did not have a role in any other aspect of the study design . 
beyond providing nancial support , neither funder was in accessing involved the raw data , collection , analysis , or interpretation of the data , or writing of the report . 
dab has received grants from accuray , and is the co - owner of berry consultants , a company that designs clinical trials for pharmaceutical and medical device companies , and international healthcare consortia . 
od was an employee of accuray , as senior vice - president responses vol 16 september 2015 e427 correction to lancet oncol 2018 ; 19 : 94052 correction to lancet oncol 2018 ; 19 : 123946 zhu ax , finn rs , edeline j , et al . 
lancet oncol 2018 ; 19 : 94052in this article , the affiliation of dr vittorina zagonel should have been istituto oncologico veneto - istituto di ricovero e cura a carattere scientifico ( iov - irccs )  . 
 apatinib combined with oral etoposide in patients with platinum - resistant or platinum - refractory ovarian cancer ( aeroc ) : a phase 2 , single - arm , prospective study . 
lancet oncol 2018 ; 19 : 123946in this article , the statistical analysis section should have stated that at least three responses were required to continue to the second stage . 
 these corrections have been made to the online version as of aug 30 , 2018 . vol 19 september 2018 e440 corrections articles e cacy of neoadjuvant bevacizumab added to docetaxel followed by uorouracil , epirubicin , and cyclophosphamide , for women with her2 - negative early breast cancer ( artemis ) : an open - label , randomised , phase 3 trial helena m earl , louise hiller , janet a dunn , clare blenkinsop , louise grybowicz , anne - laure vallier , jean abraham , jeremy thomas , elena provenzano , luke hughes - davies , ioannis gounaris , karen mcadam , stephen chan , rizvana ahmad , tamas hickish , stephen houston , daniel rea , john bartlett , carlos caldas , david a cameron , larry hayward , for the artemis investigators summary background the artemis trial was developed to assess the e cacy and safety of adding bevacizumab to standard neoadjuvant chemotherapy in her2 - negative early breast cancer . methods in this randomised , open - label , phase 3 trial , we enrolled women ( 18 years ) with newly diagnosed her2negative early invasive breast cancer ( radiological tumour size > 20 mm , with or without axillary involvement ) , at 66 centres in the uk . 
patients were randomly assigned via a central computerised minimisation procedure to three cycles of docetaxel ( 100 mg / m once every 21 days ) followed by three cycles of uorouracil ( 500 mg / m ) , epirubicin ( 100 mg / m ) , and cyclophosphamide ( 500 mg / m ) once every 21 days ( d - fec ) , without or with four cycles of bevacizumab ( 15 mg / kg ) ( bev + d - fec )  . 
signi cantly more patients in the bevacizumab group achieved a pathological complete response compared with those treated with chemotherapy alone : 87 ( 22% , 95% ci 1827 ) of 388 patients in the bev + d - fec group compared with 66 ( 17% , 1321 ) of 393 patients in the d - fec group ( p = 003 )  . 
grade 3 and 4 toxicities were reported at expected levels in both groups , although more patients had grade 4 neutropenia in the bev + d - fec group than in the d - fec group ( 85 [ 22% ] vs 68 [ 17% ] )  . interpretation addition of four cycles of bevacizumab to d - fec in her2 - negative early breast cancer signi cantly improved pathological complete response . 
however , the incidence of breast cancer has increased and continues to represent a major health problem worldwide.1 both the early breast cancer trialists collaborative group ( ebctcg ) overview analyses , 2 , 3 and individual trial data have shown bene t for adjuvant anthracycline46 and taxane - containing chemotherapy.79 although considerable progress has been made in early breast cancer through large adjuvant randomised these advances have been relatively slow . 
follow - up is prolonged in order to meet the prespeci ed event rate criteria for disease - free survival and overall survival analyses , as treatment trials , de ned in the statistical analysis plans.10 neoadjuvant trials in breast cancer have become increasingly common over the past 10 years , and the primary endpoint of pathological complete response can be reported more rapidly than in their adjuvant counterparts . trial and looked at neo - tango was our previous randomised phase 3 neoadjuvant the addition of gemcitabine to an anthracycline - based chemotherapy followed by taxane sequential combination , 11 and also the e cacy of giving paclitaxel rst in the treatment sequence . 
individual trials and the early breast cancer trialists collaborative group overviews had shown bene t for taxane and anthracycline chemotherapy , but intensi cation had failed to yield further rapid progress . 
neoadjuvant trials in breast cancer have been increasingly pursued with the early primary endpoint of pathological complete response as a surrogate for activity and improvement in long - term outcomes . 
in 2008 there was great interest in the role of the anti - angiogenic monoclonal antibody bevacizumab because phase 3 trials of bevacizumab had reported bene t in the metastatic setting . 
we developed the artemis uk multicentre trial to test the hypothesis that the combination of bevacizumab with neoadjuvant taxane and anthracycline containing chemotherapy might improve the proportion of patients achieving a pathological complete response in her2 - negative breast cancer , with acceptable toxicity . 
the artemis trial also collected tumour and blood from participants for future translational studies seeking molecular characteristics predicting bene t from bevacizumab , a key to optimising coste ectiveness in future . 
 added value of this study this report presents the primary endpoint of pathological complete response in artemis , showing a signi cant improvement in the proportion of patients achieving a pathological complete response with the addition of bevacizumab to neoadjuvant chemotherapy . 
we postulate that known variations between the trials in er status de nition might have resulted in varying distribution of er weakly positive patients across the dichotomised er positive and negative categories , thus explaining the apparently divergent results . 
we also hypothesise that molecular characteristics of individual tumours , similar to those recently observed in ovarian cancer trials of bevacizumab , might correlate with er status and underlie the variations in individual patient bene t observed . 
we developed the artemis randomised trial to test the hypothesis that the combination of bevacizumab with neoadjuvant anthracycline and taxane - based chemotherapy might improve the proportion of patients achieving a pathological complete response in breast cancer with acceptable toxicity . 
this study presents the results of the primary endpoint analysis . methods study design and participants the artemis phase 3 randomised trial aimed to assess the bene t of the addition of neoadjuvant bevacizumab to chemotherapy in terms of short - term and long - term outcomes in women presenting with early breast cancer . 
 we enrolled women aged 18 years or older with a histological diagnosis of early invasive breast cancer , and a radiological tumour size of more than 20 mm with or without axillary involvement . 
 patients with in ammatory cancer , t4 tumours with direct extension to the chest wall or skin , and ipsilateral supraclavicular lymph node involvement were eligible with any size of primary tumour . 
we regarded hormone oestrogen receptor ( er ) status as negative when allred score was 02 / 8 ; er weakly positive was 35 / 8 ; and er strongly positive was 68 / 8 . 
these er categories were based on those already used by our group in the tango trial14 and subsequently con rmed by petit and colleagues15 to be predictive of neoadjuvant chemotherapy response ( pathological complete response ) in er - positive tumours . 
 all patients were her2 negative , de ned immunohistochemistry of 0 / 1 + , or if 2 + , uorescence insitu hybridisation showed no evidence of ampli cation of the her2 gene . 
other eligibility criteria were adequate cardiac function ( left ventricular ejection fraction within the normal institutional range , as assessed by multiplegated acquisition scan or echocardiogram ) , adequate bone marrow , hepatic , and renal function , and appropriate ( ecog ) eastern cooperative oncology group performance status ( 02 )  . 
in view of potential side - e ects from bevacizumab , patients had to have no previous diagnosis of ischaemic heart disease , cerebrovascular disease , peripheral vascular disease , arterial or venous thromboembolic disease , cardiac failure , gastroduodenal vol 16 june 2015 articles 401 assigned to d - fec 399 assigned to bev + d - fec 800 participants randomly assigned 1 did not undergo surgery 1 protocol violator refused surgery 1 did not have lymph node examination after chemotherapy 6 withdrew consent for further follow - up before surgery that was her2 - positive 6 were ineligible 4 with tumours 20 mm or less 1 with a second breast tumour 1 with liver metastases 8 had baseline blood pressure measurements outside of the protocol stated limits 4 did not undergo surgery 3 withdrew from the trial due to early disease progression or inadequate response to chemotherapy 1 had inammatory disease after neoadjuvant chemotherapy 7 withdrew consent for further follow - up before surgery 1 ineligible because of bone metastases 6 had baseline blood pressure measurements outside of the protocol stated limits 393 included in the primary endpoint analysis 388 included in the primary endpoint analysis figure 1 : trial pro le d - fec = docetaxel 100 mg / m once every 21 days , followed by uorouracil 500 mg / m , epirubicin 100 mg / m , and cyclophosphamide 500 mg / m once every 21 days . 
bev + d - fec = bevacizumab 15 mg / kg given every 3 weeks with the rst four cycles of chemotherapy ( d - fec )  . for the trial protocol see warwick.ac.uk / go / artemis ulcer , symptomatic diverticulitis , or in ammatory bowel disease . 
additionally , no uncon trolled hypertension , de ned by a systolic pressure greater than 150 mm hg or diastolic pressure greater than 90 mm hg , with or without antihypertensive medication was allowed . 
 patients with initial increases in blood pressure were eligible if initiation or adjustment of antihypertensive medication lowered pressure to meet entry criteria . no previous exposure to chemotherapy , radiotherapy , or endocrine therapy as treatment for breast cancer was allowed . 
full eligibility criteria can be found in the trial protocol . artemis was an investigator designed and led trial , granted a clinical trials authorisation ( cta ) from the medicines and healthcare products regulatory agency ( mhra ) on feb 25 , 2009 , approved by the multi - centre research ethics committee nationally on march 26 , 2009 , and subsequently by the local research ethics committees at all participating centres . 
treatment allocations were made by telephone to the warwick clinical trials unit , where a central computerised minimisation procedure was used to ( 1 : 1 ) generate the patients random allocation . 
strati cation by minimisation was done by age ( 50 years vs > 50 years ) , er status ( negative vs weakly positive vs strongly positive ) , total tumour size ( 5 cm vs > 5 cm ) , clinical involvement of axillary lymph nodes ( yes vs no ) , and disease type ( in ammatory or locally advanced or both vs neither )  . 
the trial was open label . procedures chemotherapy regimens used were docetaxel 100 mg / m once every 21 days for three cycles , followed by uorouracil 500 mg / m , epirubicin 100 mg / m , with cyclophosphamide 500 mg / m once every 21 days for three cycles ( d - fec )  . 
bevacizumab 15 mg / kg ( genentech , south san francisco and vacaville , ca , usa ) was given every 3 weeks with the rst four cycles of chemotherapy in the experimental group ( bev + d - fec )  . we assessed adverse events for each chemotherapy cycle by grade according to common terminology criteria for adverse events ( ctcae ) version 3 . 
if neutropenic fever or sepsis occurred after a cycle of chemotherapy , the next cycle was delayed until the absolute neutrophil count was at least 10 10 cells per l . 
after a delay , either dose reduction of all drugs to 80% , or gcsf support with 100% dose were allowed , and all remaining cycles of the same three - cycle block were given at those doses . 
for persistent thrombocytopenia , the next cycle was delayed until platelets had recovered to at least 100 10 cells per l and chemotherapy doses were reduced to 80% , maintaining this dose reduction for subsequent cycles . 
however , once started , prophylactic gcsf was usually continued into the second phase of chemotherapy at the discretion of the responsible physician . if grade 2 neuropathy occurred during treatment with docetaxel , remaining doses were reduced to 75 mg / if grade 3 neuropathy occurred , docetaxel was stopped . 
if fewer than three cycles of docetaxel had been given , additional fec cycles were allowed up to a maximum of six cycles in total , at the discretion of the treating consultant . cardiac toxicity was checked by left ventricular ejection fraction before treatment started and after four cycles of chemotherapy with or without bevacizumab . 
if severe allergic symptoms occurred , including bronchospasm , angio - oedema , hypotension generalised urticaria , ( systolic blood pressure < 100 mm hg ) , or life - threatening anaphylaxis , docetaxel infusion was stopped and treatment was given with intramuscular epinephrine ( 1 ml , 1 : 1000 ) , intravenous steroids , and intravenous antihistamines ; rechallenge was contraindicated . surgery ( breast and axillary ) , radiotherapy , and adjuvant endocrine treatment were done according to local protocols . 
patients will continue to receive follow - up through the national cancer intelligence network ( ncin ) with monitoring of disease - free survival and overall survival . similar to other recent and the reporting of pathological complete response and minimal residual disease was by an independent , central , two - reader masked review of all anonymised local surgical histopathology reports undertaken by the cochief investigators ( hme and lha )  . 
a quality assurance comparison ( using a statistic ) has been done in cases reviewed to date , between central pathological review of the haematoxylin and eosin slides ( all cases done by jt ) and the local histopathology reports for the primary endpoint of pathological complete response . outcomes our primary endpoint was pathological complete response , de ned as absence of invasive breast cancer in ductal carcinoma in situ associated with tumour data are n ( % )  . 
each measurable breast tumours longest single diameter is summed within each breast for each patient , and labelled as tumour bulk ; for each patients breast with maximum tumour bulk , tumour characteristics are presented . 
 * adjusted for the ve strati cation variables ( age [ 50 years , > 50 years ] , er status [ negative , weakly positive , strongly positive ] , tumour size [ 50 mm , > 50 mm ] , clinical involvement of axillary nodes [ no , yes ] , and inammatory or locally advanced disease [ no , yes ] )  . 
tumour grade of each patients largest breast tumour at baseline . table 2 : pathological complete response and minimal residual disease in d - fec and bev + d - fec groups less of original tumour burden remaining at surgery , and has previously been reported as a potentially useful secondary endpoint in neoadjuvant studies.16 other protocol - de ned secondary endpointsthat are not reported hereinclude disease - free survival and overall survival . 
these will be analysed in early 2016 when it is anticipated that median follow - up will be at least 36 months or 120 disease - free survival events will have occurred . statistical analysis the power calculations assume a 70 to 30 split in the trial sample between er - positive and er - negative tumours , respectively . 
the proportion of patients achieving a pathological complete response with the standard treatment ( d - fec ) was estimated as about 10% for erpositive tumours and 25% for er - negative tumours . 
on this basis , a trial randomly assigning 400 patients into each of the two treatment groups would allow an absolute di erence in the proportion of patients achieving a pathological complete response in excess of 10% to be detected at the 5% ( two - sided ) level of signi cance with an 85% power . 
a 10% di erence in the proportion of patients who achieve a pathological complete response is the most widely accepted in neoadjuvant chemotherapy trials and was used in this groups previously reported neo - tango trial.11 the proportion of patients achieving pathological complete response was calculated for all patients known to have had surgery . 
 multivariate logistic regression provided p values for the treatment e ect after adjustment for strati cation factors . as a secondary analysis , the proportion of patients achieving pathological complete response in the breast alone was assessed along with those achieving pathological complete response or minimal residual disease , and comparisons across treatment groups were logistic regression with made using multivariate adjustment for prognostic factors . the sample size of our study is too small to permit multiple subgroup analyses , and so we chose not to do tests for statistical signi cance in each er subgroup separately . the methods for dose intensity calculations have been described previously.17 chemotherapy course delivered dose intensities were compared across treatment groups using wilcoxon rank - sum tests and fishers exact tests . common toxicity criteria ( ctc ) grades were recorded for each chemotherapy cycle and growth factor support ( usually gcsf ) was also recorded . 
the reports of grade 3 and 4 toxicities were examined in detail . statistical analysis was done on an intention - to - treat basis and therefore all patients who were ineligible , or whose treatment violated the trial protocol , were analysed within their randomised treatment groups . 
pathological complete response di ered signi cantly across both er status ( negative 41% [ 95% ci 3548 ] , weakly positive 49% [ 3861 ] , strongly positive 8% [ 611 ] ; p < 00001 ) and tumour grade ( grade 1 / 2 9% [ 613 ] , grade 3 32% [ 2837 ] ; p < 00001 )  . 
similarly , the proportion of patients who obtained a pathological complete response or minimal residual disease was signi cantly better in the bev + dfec group than in the d - fec group ( di erence 7% [ 95% ci 01132 ] ; p = 003 after adjustment for strati cation factors ; table 2 )  . 
the proportion of patients who obtained a pathological complete response or minimal residual disease di ered signi cantly across both er status ( negative 51% [ 95% ci 4558 ] , weakly positive 60% [ 4871 ] , strongly positive 18% [ 1522 ] ; p < 00001 ) and tumour grade ( grade 1 / 2 16% [ 1221 ] , grade 3 44% [ 3949 ] ; p < 00001 )  . 
hme , lhi , and lha had full access to all of the data and had nal responsibility for the decision to submit for publication with the agreement of all the authors and the data monitoring and safety committee . results 800 patients were recruited at 66 uk centres ( between may 7 , 2009 , and jan 9 , 2013 ) and randomly assigned to either d - fec ( 401 patients ) or bev + d - fec regimens ( 399 patients ; gure 1 )  . 
we subsequently identi ed seven patients as ineligible ; six in the d - fec group ( four with tumours 20 mm or less , one with a second breast tumour that was her2 - positive , and one with liver metastases ) ; and one in the bev + d - fec group ( with bone metastases )  . 
additionally , 14 patients ( eight in the d - fec group and six in the bev + d - fec group ) had baseline blood pressure measurements outside of the protocol stated limits . 
153 ( 20% ) of all 781 patients achieved a pathological complete response : 66 ( 17% , 95% ci 1321 ) in the d - fec group and 87 ( 22% , 1827 ) in the bev + d - fec group ( di erence 6% , 01112 ; p = 003 after adjustment for strati cation factors , p = 006 for the unadjusted analysis ; table 2 and gure 2 )  . 
er negative , er weakly positive , and grade 3 patients appeared to bene t from the addition of bevacizumab whereas er strongly positive and grade 1 / 2 patients did not appear to bene t from the addition of bevacizumab ( table 2 )  . 
an analysis of bene t for bevacizumab for each level of allred score ( er status ) , con rmed that our categories of er weakly positive ( allred 35 / 8 ) and er strongly positive ( allred 68 / 8 ) were the correct cut points both for pathological complete response rate and bene t for bevacizumab ( appendix )  . 
 table 4 : chemotherapy modi cations in the 4418 cycles number not given as per protocol number of treatment delays cycle 1 cycle 2 cycle 3 cycle 4 data are n ( % )  . 
four patients in the bev + d - fec group received no treatment cycles for the following reasons : diagnosis of colitis and patient proceeded to mastectomy with axillary surgery ; patient chose to withdraw from trial before any treatment was given ; allergic reaction and no chemotherapy given ; diagnosis of metastatic disease during the trial screening phase . 695 ( 90% ) of 775 patients ( 352 [ 90% ] of 391 patients in the d - fec group and 343 [ 89% ] of 384 in the bev + d - fec group ) who started treatment received six cycles of chemotherapy ; the main reasons for receiving fewer cycles being patient withdrawal , allergic reaction to drugs , and chemotherapy toxicities . 
no di erences in chemotherapy course delivered dose intensity between the treatment groups were detected ( d - fec 98% [ 95% ci 92100 ] vs bev + d - fec 97% [ 91100 ] ; p = 024 )  . 
665 ( 85% ) patients received a chemotherapy course delivered dose intensity of at least 85% ( d - fec 86% [ 95% ci 8289 ] vs bev + dfec 85% [ 8188 ] ; p = 058 )  . 
 the main reason for switching early was allergy to docetaxel ( 19 [ 83% ] of 23 patients ; 11 [ 79% ] of 14 d - fec patients , eight [ 89% ] of nine bev + d - dfec patients )  . 331 ( 86% ) of 384 bev + d - fec patients who started treatment received four cycles of bevacizumab . 
85% ( 95% ci 8188% ) of bev + d - fec patients received a bevacizumab course delivered dose intensity of at least 85% . the intensities both individual cycle dose for chemotherapy and bevacizumab did not show substantial attrition over time ( appendix )  . 
of the 386 ( 9% ) reports of chemotherapy dose reductions from 4418 chemotherapy cycles , dose reductions were most commonly reported in cycles 2 and 3 and again in cycles 5 and 6 , in both treatment groups ( table 4 )  . 
 reports of modi cations to bevacizumab administration were infrequent throughout the four cycles ( table 5 )  . gcsf was used in 2744 ( 62% ) of 4418 cycles with slightly higher rates in the bev + d - fec group in all treatment cycles ( appendix )  . 
full treatment details were available for 4418 cycles delivered to 775 patients ( 2234 cycles in 391 d - fec patients and 2184 cycles in 384 bev + d - fec patients )  . 
more patients receiving bevacizumab with d - fec had grade 3 infections than those receiving d - fec alone ( 68 [ 18% ] vs 40 [ 10% ] )  . 
allergies were reported separately : 43 ( 5% ) of 800 patients ( 26 d - fec patients , 17 bev + d - fec patients ) had grade 3 and 4 allergic reactions attributable to docetaxel and only one patient had grade 3 allergy attributable to bevacizumab . 
both regimens appear tolerable and deliverable . full surgery details were available for 764 ( 98% ) of 781 patients ( 378 d - fec patients , 386 bev + d - fec patients ) analysed for pathological complete response by local report review . 
the geparquinto results are supported by those of calgb 40603 , which enrolled triple - negative patients only.20 in this smaller study , the addition of bevacizumab signi cantly the proportion of patients achieving a pathological complete response ( de ned as absence of invasive disease in breast only [ ypt0 / tis ] ) in the bevacizumab group compared with the chemotherapy alone group ( 59% vs 48% ; p = 0009 )  . 
the results of these two studies are very similar to our study , in which a greater proportion of patients treated with bevacizumab achieved a pathological complete response ( de ned as no invasive disease in breast or axilla [ ypt0 / tis ypn0 ] ) than those treated with chemotherapy alone ( 22% vs 17% in the overall study population and 44% vs 32% in er / her2 - negative patients )  . 
as an example , in calgb 40603 , the signi cantly lower proportions of patients having mastectomy compared with the d - fec group ( 48% vs 51% ; p = 047 ; appendix )  . 
however , overall , signi cantly fewer patients who achieved a pathological complete response had a mastectomy compared with those who did not achieve a pathological complete response ( 42 / 146 [ 29% ] vs 335 / 618 [ 54% ] ; p < 00001 ; appendix )  . 
having a pathological complete response or minimal residual disease in the breast also signi cantly lowered the frequency of mastectomy compared with those patients who achieved neither ( 90 / 243 [ 37% ] vs 287 / 522 [ 55% ] p < 00001 ; appendix )  . discussion in the artemis study , the addition of short course bevacizumab to standard neoadjuvant anthracycline and taxane - based chemotherapy in her2 - negative , early breast cancer , was associated with a signi cant improvement in the proportion of patients achieving a pathological complete response . 
a greater proportion of er - negative ( allred 02 ) and er weakly positive ( allred 35 ) patients achieved pathological complete response compared with the er strongly positive ( allred 68 ) patients . 
the bene t of bevacizumab for er - negative and weakly positive patients is in marked contrast to the er strongly positive group in which low proportions of patients achieved pathological complete response and there was also an apparent lack of bene t from bevacizumab . 
the artemis treatment protocol was deliverable for both chemotherapy and bevacizumab , and toxicity from chemotherapy was as expected for d - fec , although there was an increase in grade 4 neutropenia in patients given bev + d - fec , as reported previously.18 the observed di erences in pathological complete response were statistically signi cant in the group as a whole . 
however , the clinical signi cance of the addition of bevacizumab appears to be most compelling within the er - negative subgroup . three other randomised studies have reported on the addition of bevacizumab to neoadjuvant chemotherapy in her2 - negative breast cancer1922 ( appendix )  . 
 in our trial , er weakly positive patients ( although a small strati ed subgroup ; n = 75 ) showed similar chemotherapy response and bene t from bevacizumab to the er - negative group . 
we believe that a meta - analysis of all four studies with uniform de nitions of hormone receptor and pathological complete response is needed to identify a subgroup of patients in whom bevacizumab increases pathological complete response . 
with that in mind , and acknowledging that the sample size of our study is too small for subgroup analyses , we chose not to do tests for statistical signi cance in each er subgroup separately ( table 2 )  . the use of pathological complete response as a trial endpoint is to some extent dependent on its role as a surrogate for meaningful clinical outcomes such as disease - free survival , distant relapse - free interval , breast cancer speci c survival , and overall survival . 
some of these have very recently been reported the geparquinto study24 and show no di erence for the addition of bevacizumab at 3 years for either disease - free for that explanation survival ( hr 103 , 95% ci 084125 ) or overall survival ( 097 , 075126 )  . 
results might be confounded because no bevacizumab was given after surgery and patients who were not responding on ultrasound assessment , at the midpoint of their neoadjuvant treatment , were o ered randomisation into a novel treatment group with everolimus . 
whereas an increased incidence of pathological complete response occurs in the well - developed primary tumour , which is angiogenesis - dependent , there might be no such advantage in terms of increased eradication of eventually lethal distant micrometastatic bone marrow disease . 
hatzis and colleagues29 have explored this in depth , and have 664 vol 16 june 2015 articles improved event - free modelled data from neoadjuvant trials and made two conclusions . 
first , that in high - risk breast cancer the design of neoadjuvant trials could increase the numbers of patients to a level that would make a positive correlation between the primary endpoint ( proportion of patients achieving pathological complete response ) and longer term outcomes more likely . 
in the ctneobc analysis of 12 trials and 11 955 patients , the coe cient of determination ( r ) was only 003 for eventfree survival and 024 for overall survival , meaning that only 3% and 24% of the variability in event - free survival and overall survival , respectively , between trial groups can be explained by di ering proportions of patients achieving a pathological complete response . 
the translational artemis group plan to explore , using samples from the artemis trial biobank , whether the same angiogenic signature in breast cancer could provide a predictive biomarker of response to bevacizumab . contributors hme and lha were responsible for the conception , design , recruitment , interpretation of the data , and drafting of the manuscript . 
lha received funding through the university of cambridge ( as sponsors of the trial ) from cancer research uk , roche , and sano - aventis , and disbursed the proportion due to nhs lotian for work on the trial ; and personal fees from roche for attendance at advisory board and international meetings . 
a - lv , ja , lh - d , ra , ig , sc , th , jt , ep , cc , and sh declare no competing interests . acknowledgments the trial was funded by cancer research uk ( cruk / 08 / 037 for trial coordination ) , roche ( provision of free study drug bevacizumab and unrestricted educational grant for trial coordination ) , and sano - aventis ( unrestricted educational grant for trial coordination )  . 
we thank the data and safety monitoring committee members : i craig henderson ( university of california , san francisco , ca , usa ) , luca gianni ( ospedale san ra aele , milan , italy ) , mark f brady ( gynecologic oncology group statistical & data center , roswell park cancer institute , bu alo , ny , usa ) , and xavier pivot ( centre hospitalier rgional universitaire et institut rgional fdratif de cancrologie , besanon , france )  . 
we thank the trials unit sta : phase 3 coordination at warwick clinical trials unit , coventry , uk ; translational coordination at university of cambridge , addenbrookes hospital , cambridge , uk and university of edinburgh department of oncology ( biobank ) ; and statistical analysis at warwick clinical trials unit , uk . published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
at a median follow - up of 5 years , ndings from our previously published randomised trial of narrow ( 1 cm ) versus wide ( 3 cm ) excision margins in patients with thick cutaneous melanomas showed that narrow margins were associated with an increased frequency of locoregional relapse , but no signi cant di erence in overall survival was apparent . 
we now report a long - term survival analysis of that trial . methods we did a randomised , open - label multicentre trial in 59 hospitals57 in the uk , one in poland , and one in south africa . 
patients with one primary localised cutaneous melanoma greater than 2 mm in breslow thickness on the trunk or limbs ( excluding palms or soles ) were randomly assigned ( 1 : 1 ) centrally to receive surgery with either a 1 cm or 3 cm excision margin following an initial surgery . 
this trial was not registered because it predated mandatory trial registration . findings between dec 16 , 1992 , and may 22 , 2001 , we randomly assigned 900 patients to surgery with either a 1 cm excision margin ( n = 453 ) or a 3 cm excision margin ( n = 447 )  . 
194 deaths were attributed to melanoma in the 1 cm group compared with 165 in the 3 cm group ( unadjusted hazard ratio [ hr ] 124 [ 95% ci 101153 ] ; p = 0041 )  . 
although a higher number of deaths overall occurred in the 1 cm group compared with the 3 cm group ( 253 vs 241 ) , the di erence was not signi cant ( unadjusted hr 114 [ 95% ci 096136 ] ; p = 014 )  . 
 surgical complications were reported in 35 ( 8% ) patients in the 1 cm excision margin group and 65 ( 15% ) patients in the 3 cm group . interpretation our ndings suggest that a 1 cm excision margin is inadequate for cutaneous melanoma with breslow thickness greater than 2 mm on the trunk and limbs . 
open access article distributed under the terms of cc by . introduction the risk of metastatic spread from a malignant melanoma is estimated on the basis of histopathological features such as the breslow thickness , mitotic rate , and the presence of microscopic ulceration.1 , 2 whether the surgical margins that are taken around the primary tumour a ect metastatic spread is unclear , despite having been the subject of several randomised clinical trials.37 historically , wide surgical margins of 5 cm or more were taken around primary melanomas in an attempt to not only excise the primary tumour but also to encompass local micrometastatic disease in the vicinity of the tumour.8 , 9 in ndings from all previously reported randomised trials comparing wide ( 35 cm ) with narrow ( 12 cm ) margins , no signi cant di erence in overall survival between the groups has been reported . 
 for melanoma - speci c survival , although no trial has shown a signi cant di erential risk associated with di erent surgical margin widths , ndings from two trials3 , 4 and the previous report of this trial10 suggest a possible detrimental e ect of narrow margins on melanoma - speci c survival . 
in a swedish melanoma 184 vol 17 february 2016 articles research in context evidence before this study we searched pubmed for articles published up to aug 1 , 2015 , on randomised trials assessing surgical excision margins in cutaneous melanoma , using the search terms melanoma , margins , excision , and surgery . 
 however , some of these studies have shown non - signi cant results favouring wider margins in minimising locoregional and distant relapse . added value of this study this study reports on long - term survival analysis and , to our knowledge , is the rst to show that wider surgical margins result in a signi cant improvement in melanoma - speci c survival . implications of all the available evidence this study , alongside the other randomised trials , reiterates current international guidelines stating that a 1 cm margin is inadequate for the treatment of a melanoma greater than 2 mm in breslow thickness . 
it lends support to further investigation of the adequacy of a 1 cm margin for melanomas between 1 mm and 2 mm in thickness , especially those with other poor prognostic features , for which most international guidelines at present still advise a 1 cm excision . 
 900 patients enrolled 742 received 1 mm margin initial excision * and randomised 158 received 1 cm margin initial excision and randomised 372 assigned to 1 cm margin 370 assigned to 3 cm margin 81 assigned to 1 cm margin ( ie , no further excision ) 77 assigned to 3 cm margin ( ie , 2 cm further excision ) 453 assigned to 1 cm margin 442 received assigned treatment 447 assigned to 3 cm margin 436 received assigned treatment 2 lost to follow - up 253 died 453 included in long - term intention - to - treat analysis 2 lost to follow - up 241 died 447 included in long - term intention - to - treat analysis figure 1 : trial pro le * initial excision by the proposed pathway . 
initial excision by the alternative pathway . study group trial3 of patients randomly assigned to excision margins of either 2 cm or 5 cm for trunk and extremity melanomas with a breslow thickness 0820 mm ( median 12 mm ) , the hazard ratio ( hr ) for melanoma deaths for narrow margins compared with wide margins was 122 ( 95% ci 088169 ; p = 024 ) with a median follow - up of 11 years . 
additionally , the intergroup melanoma surgical trial4 of patients randomly assigned to either a 2 cm or 4 cm excision margin for trunk and extremity melanomas with breslow thickness 14 mm ( median 196 mm ) showed a non - signi cant di erence ( p = 007 ) in 10 - year diseasespeci c survival between groups ( 70% for the 2 cm group and 77% for the 4 cm group )  . 
however , ndings from a second swedish melanoma study group trial6 that randomly assigned patients with melanomas of breslow thickness greater than 2 mm ( median 31 mm ) to either a 2 cm or a 4 cm excision margin showed no di erence in melanoma - speci c survival between the two groups ( hr 099 [ 95% ci 078126 ] ; p = 095 )  . ( breslow in 2004 , we reported the ndings from our randomised clinical trial10 of patients with high - risk malignant melanoma thickness 2 mm ) randomly assigned to excision margins of either 1 cm or 3 cm , with a median follow - up of 5 years . 
we now report an extended follow - up of the survival endpoints of this trial with a median follow - up of 88 years . methods study design and participants we have previously described the study design , patient eligibility criteria , trial protocol , and endpoints of the randomised trial in detail.10 brie y , between dec 16 , 1992 , and may 22 , 2001 , we did a randomised , open - label multicentre trial in 59 centres in the uk , south africa , and poland . 
the trial was done under the auspices of the uk melanoma study group , the british association of plastic surgeons , and the scottish cancer therapy network and was approved by local ethics committees of all participating centres . 
patients aged the 18 years or older with one primary localised cutaneous melanoma greater than 2 mm in breslow thickness arising on the trunk or limbs ( but not including the soles of feet or palms of hands ) were eligible for the study . 
before randomisation , the primary melanoma was excised in an initial surgery with either a 1 mm ( proposed pathway ) or 1 cm ( alternative pathway ) margin of excision . 
 table 1 : baseline characteristics of the intention - to - treat population randomisation and masking we randomly assigned patients ( 1 : 1 ) to either a 1 cm surgical excision or a 3 cm surgical excision as the measured clinical margin taken around the primary melanoma lesion . 
we did the randomisation centrally by telephone call from the patients treating centre to the institute of cancer research clinical trials and statistics unit ( icr - ctsu )  . 
elective lymph node dissection and sentinel node biopsy were not part of routine practice at the time the trial was undertaken and adjuvant chemotherapy was not allowed in the trial protocol . 
after treatment , patients were followed up for local and distant relapse and death every 3 months for the rst 2 years , then every 6 months for up to 5 years , and annually thereafter . 
 to maximise the amount of survival data obtained , we also traced uk patients ( n = 790 ) for their vital status and in january , 2012 , we requested the death certi cates of patients known to have died to identify the cause of death as stated on the certi cate . 
death was classed as melanoma - speci c if the cause of death was reported as melanoma on the clinical trial case - report form for 186 vol 17 february 2016 articles death , or if any evidence was present of distant metastatic melanoma at the time of death ( as reported in patient les or on death certi cates )  . 
attribution of the cause of death as stated on the death certi cate was masked to clinical records and treatment group . outcomes the primary endpoints of the original trial10 were locoregional recurrence and disease - free survival . 
instead , we assessed the original secondary endpoints of overall survival , measured as time from randomisation to death from any cause , and melanoma - speci c survival , measured as time from randomisation to death reported to be from melanoma . 
for the competing risks analysis , we plotted cumulative incidence functions for each cause of death ( melanoma and non - melanoma ) and compared treatment groups with grays test . 
hrs were obtained from the univariate fine and gray model.13 , 14 we also did a multivariable analysis with the fine and gray model , including the same variables as the multivariable cox model . 
to explore the e ect of age on cause of death , patients were classi ed at randomisation in ve age groups containing about equal numbers of patients ( < 45 years , 4553 years , 5463 years , 6470 years , and 71 years ) , de ned using quintiles and rounding to the nearest whole number . 
we estimated the rates of death from melanoma and other causes for each age group as 1 cm margin 3 cm margin hr 114 ( 95% ci 096136 ) ; log - rank p = 014 statistical analysis the original planned sample size was 600 patients , based on an expected 3 - year local or in - transit recurrence rate of 15% ; however , because of a lower recurrence rate than expected , the sample size was increased to 900 after discussion with the trial management group and the data monitoring committee.10 at the time of writing the protocol , we expected that 4050% of patients with a 3 cm excision would have disease recurrence within 23 years . 
 for melanoma - speci c survival , patients who died of non - melanoma causes were censored at the time of death and patients who died from an unknown cause were censored on the day before their date of death . 
to assess the robustness of these assumptions we did a competingrisks analysis , treating con rmed non - melanoma deaths as the competing event . we constructed kaplan - meier curves11 and calculated hrs using the cox proportional hazards model ; 12 we compared treatment groups using the log - rank test . 
 we calculated absolute risk di erence at 10 years with normal estimated 95% cis and assessed the e ect of individual prognostic factors in a multivariable analysis using the same cox proportional hazards model as in our previous report , 10 adjusting for age . 
variables are included in the model as categorical indicators , other than tumour thickness which was classi ed as 0249 mm , 250349 mm , 350449 mm , 450549 mm , and 550 mm or more , and tted as a linear e ect . 
for this analysis we constructed kaplan - meier curves and calculated hrs using the cox proportional hazards model for uk patients only . we did a post - hoc subgroup analysis to assess whether sex , tumour thickness , age group , site , ulceration , and proposed versus alternative pathway initial excision were associated with treatment e ect . 
we used two - sided signi cance tests throughout . this was the rst and only analysis that had been done on this dataset since the initial report of this trial . 
we did the competing risks analysis with r 3.0.2 and all other analyses with stata version 11.2. role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or n ( % ) overall survival melanoma - speci c survival 388 ( 50% ) 100 * 385 ( 50% ) 119 ( 099145 ) 128 ( 102161 ) 354 ( 46% ) 100 * 419 ( 54% ) 138 ( 111171 ) 138 ( 107177 ) tumour thickness ( mm ) 773 ( 100% ) 118 ( 110127 ) 477 ( 62% ) 100 * 296 ( 38% ) 168 ( 138204 ) 174 ( 139219 ) excision margin 3 cm 1 cm p value female male p value p value ulceration absent present p value site distal limb proximal limb age ( years ) trunk p value p value 0070 00035 < 00001 < 00001 0029 00001 244 ( 32% ) 100 * 174 ( 23% ) 123 ( 093163 ) 355 ( 46% ) 141 ( 109181 ) 100 * 0031 100 * 0013 123 ( 113133 ) < 00001 100 * < 00001 100 * 146 ( 104205 ) 171 ( 126231 ) 00026 100 * 034 400 ( 52% ) 100 * 373 ( 48% ) 149 ( 123181 ) 112 ( 089139 ) data are n ( % ) , hazard ratio ( 95% ci ) of 773 patients with available data . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between dec 16 , 1992 , and may 22 , 2001 , 900 patients were enrolled at 57 hospitals in the uk , one hospital in poland , and one hospital in south africa ( appendix ) and received an initial excision of 1 mm or 1 cm , and were then randomly allocated to either a total 1 cm surgical margin ( n = 453 ) or a total 3 cm surgical margin ( n = 447 ; gure 1 )  . 
 median follow - up for all patients was 57 years ( 68 months [ iqr 35103 ] ) and median follow - up in patients not known to have died ( censoring at death ) was 88 years ( 106 months [ 76135 ] )  . 
median follow - up for the uk patients for whom a death certi cate analysis was done ( censoring at death ) was 93 years ( 111 months [ iqr 82141 ] ) and median follow - up in non - uk patients was 63 years ( 76 months [ 62100 ] )  . 
 for three participants ( two in the 1 cm margin group , one in the 3 cm group ) , melanoma was present at the time of death but this was not the cause of death . 
four patients did not have any follow - up after randomisation and were censored at randomisation . the snapshot used for the current analysis was taken on aug 31 , 2012 , after information from the death certi cate analysis had been obtained . 
253 deaths occurred overall in 453 patients in the 1 cm margin group and 241 occurred in 447 patients in the 3 cm group ( unadjusted hr 114 [ 95% ci 096136 ] ; p = 014 ; gure 2 )  . 
194 deaths attributed to melanoma occurred in the 1 cm margin group compared with 165 in the 3 cm margin group ( unadjusted hr 124 [ 95% ci 101153 ] ; p = 0041 ; gure 2 )  . 
results from the sensitivity analysis of uk patients only ( n = 338 in the 1 cm margin group ; n = 392 in the 3 cm margin group ) showed hrs of 111 ( 95% ci 092133 ) for overall survival and 121 ( 097150 ) for melanoma - speci c survival ; the results were consistent with the primary result . 773 patients ( 385 in the 1 cm group and 388 in the 3 cm group ) had complete data for all known prognostic factors and were included in a multivariable analysis ( table 2 )  . 
when we assessed interactions between margin width and sex , 188 vol 17 february 2016 articles tumour thickness , age group , site , and ulceration in a subgroup analysis , none were signi cant for either overall survival or melanoma - speci c survival ( gure 3 )  . 
 when the e ect of competing deaths due to other causes was taken in account , the cumulative incidence of death from melanoma was higher in the 1 cm margin events ( n ) patients ( n ) hazard ratio ( 99% ci * ) 114 ( 096136 ) all patients male female < 60 years 60 years 000399 mm 400599 mm 6 mm site distal limb proximal limb trunk ulceration present absent protocol type alternative proposed all patients male female < 60 years 60 years 000399 mm 400599 mm 6 mm site distal limb proximal limb trunk ulceration present absent protocol type alternative proposed 126 ( 093172 ) 094 ( 065136 ) 135 ( 094193 ) 101 ( 074138 ) 107 ( 079146 ) 111 ( 069177 ) 181 ( 099334 ) 082 ( 051130 ) 126 ( 076208 ) 129 ( 093179 ) 135 ( 094194 ) 095 ( 067135 ) 075 ( 045126 ) 126 ( 093172 ) 137 ( 096196 ) 100 ( 064155 ) 141 ( 096207 ) 108 ( 073159 ) 124 ( 086180 ) 116 ( 068198 ) 167 ( 084332 ) 099 ( 054180 ) 147 ( 081267 ) 130 ( 090188 ) 134 ( 089202 ) 106 ( 070160 ) 078 ( 044141 ) 137 ( 096196 ) favours 1 cm favours 3 cm events ( n ) patients ( n ) hazard ratio ( 99% ci * ) 124 ( 101153 ) favours 1 cm favours 3 cm figure 3 : univariable subgroup analyses of overall survival ( a ) and melanoma - speci c survival ( b ) the dotted line shows the hazard ratio for all patients . 
the multivariable analysis done with fine and grays model for melanomaspeci c deaths showed similar results to the cox model for melanoma - speci c survival ( appendix )  . 
no di erences between the two margin widths were noted regarding the cumulative incidence of death due to other causes ( gure 4 ; point estimates of cumulative incidence at 88 years were 145% [ 95% ci 101206 ] in the 1 cm margin group , 182% [ 136240 ] in the 3 cm group )  . 
 the number of non - melanoma deaths in younger age groups was negligible , but became more predominant in later years of follow - up for older patients ( table 3 )  . 
surgical complications were reported in 35 ( 8% ) of 453 patients in the 1 cm group and 65 ( 15% ) of 447 patients in the 3 cm group . 
the most common complications were partial or complete graft loss ( ten [ 2% ] in the 1 cm group , 20 [ 4% ] in the 3 cm group ) and wound dehiscence ( seven [ 2% ] in the 1 cm group , nine [ 2% ] in the 3 cm group )  . discussion at a median follow - up of 88 years ( 106 months ) the risk of death from melanoma was signi cantly higher in the narrow ( 1 cm ) margin group than in the wider ( 3 cm ) margin group . 
 the estimated risk of death from any cause was higher in the 1 cm margin group than in the 3 cm margin group , although this di erence was not signi cant . 
 a limitation of our study is that complete data were not available for all patients ; in particular , death certi cates were not obtained for non - uk patients . 
however , the results of a sensitivity analysis of uk patients only were consistent with the primary results . findings from our previous report of this trial10 with a median follow - up of 5 years showed that , in patients with high - risk melanoma , a 1 cm excision margin was associated with a signi cant increase in locoregional relapse compared with a 3 cm excision margin that report , although the number of deaths di ered between the two study groups , the di erence was not signi cant ( 128 deaths from melanoma in the group with 1 cm excision margins compared with 105 in the group with 3 cm excision margins ; hr 124 [ 95% ci 096161 ] , p = 01 )  . 
additionally , no di erences were noted in overall survival between the two groups ( 322% in the 1 cm group vs 309% in the 3 cm group ; hr 107 [ 95% ci 075136 ] , p = 06 )  . the current analysis does not include an updated analysis of the locoregional recurrence endpoint because follow - up data for locoregional relapse beyond 5 years are sparse . 
this report describes analyses only of melanomaspeci c survival and overall survival , and shows that a narrow margin signi cantly reduced melanoma - speci c survival compared with a wider marg locoregional relapse is the most common rst site of relapse of metastatic melanoma and , accordingly , an increased risk of locoregional relapse in the narrow margin group might suggest an increased future risk of melanoma - speci c death . 
during the period of this study , when no e ective systemic therapies for metastatic melanoma were available , stage iv disease was associated with a very poor prognosis with a median survival of between 8 and 18 months depending on the pattern of metastatic spread.15 although age , sex , tumour thickness , ulceration , and tumour site all seem to be prognostic factors for overall survival , only age was shown to a ect non - melanoma deaths , which occurred in similar numbers in the 1 cm and the 3 cm groups . 190 vol 17 february 2016 articles the prognostic because sentinel node biopsy was not done routinely in this trial , 10 the trial groups might have been imbalanced in terms of clinically occult disease within regional lymph nodes at the time of randomisation , which could have biased the outcome of the trial . 
any imbalances in unobserved factors in this study would be due to chance and a chance imbalance in a study of this size is unlikely to a ect the outcomes . 
 because the trial groups were well balanced in terms of other known prognostic factors for outcome at the time of trial recruitment ( eg , sex , tumour thickness , disease site ) and ulceration was slightly more prevalent in the 3 cm group , the sentinel node status is unlikely to be worse in the 1 cm group than in the 3 cm group , although a chance imbalance remains possible . this study cannot establish whether locoregional relapse predisposes patients to the subsequent development of distant metastatic disease , or whether the development of locoregional disease is merely correlated with and predates the development of metastatic disease . 
 because a 3 cm margin resulted in a decreased number of melanoma deaths , this would suggest that surgically intervening in a micrometastatic process in the 3 cm around the primary tumour can somehow a ect the later metastatic process at more distant sites . 
previous studies have shown a signi cant increase in local recurrence rates after 1 cm excisions , 6 , 16 suggesting that 1 cm margins might not be adequate to deal with local microsatellitosis . previous randomised studies of elective1721 or selective22 lymph node dissection have not shown a signi cant di erence in melanoma - speci c survival . 
the absence of a proven survival bene t in these nodal studies is at odds with the probable biological hypothesis for an e ect on survival shown in this studyie , that removal of microsatellites around the primary tumour a ects the development of metastatic disease . 
however , because subgroup analyses in these studies raised the possibility of survival bene t for prophylactic lymph node clearance that was not detected at the point of randomisation , 22 there might be a consistent biological process underlying the e ect noted in this study and in previous studies of prophylactic lymph node clearance . current international guidelines advise a 2 cm excision for melanomas greater than 2 mm in thickness and ndings from the other major randomised study for thick melanomas6 suggested that a 4 cm excision was not better than a 2 cm excision in terms of melanoma - speci c survival . 
deaths presented as n or n ( % )  . table 3 : deaths from melanoma and other causes in di erent age groups of melanomas thicker than 2 mm , margins greater than 2 cm need not necessarily be taken . 
our study has re - emphasised that the choice of surgical margins taken around a cutaneous melanoma is important and , to our knowledge , for the rst time provides evidence to suggest that a narrower excision margin used for thick primary tumours a ects melanoma - speci c survival . 
this nding might be pertinent for speci c melanomas for which narrow ( 1 cm ) margins are presently advisedie , melanomas between 1 mm and 2 mm in thickness with other adverse prognostic features ( ulceration or high mitotic rate , or both )  . 
the possible di erence between a 1 cm and 2 cm margin for melanomas greater than 1 mm in thickness is being investigated in a randomised trial in progress ( nct02385214 )  . 
all authors were involved in the writing , review , and approval of the nal manuscript , and all agreed to the submission of the nal version of the manuscript . veronesi u , cascinelli n , adamus j , et al . 
lancet 1907 ; 169 : 9961003 . declaration of interests jmt is a trustee of the meirion thomas cancer research fund that funded the administrative fee needed to retrieve copies of death certi cates for patients within the trial . 
all other authors declare no competing interests . acknowledgments this study was funded by the north thames national health service executive , northern and yorkshire national health service executive , british united provident association foundation , british association of plastic surgeons , and the meirion thomas cancer research fund . 
 continued data collection and analysis was made possible by programme grant funding to the institute of cancer research ( icr ) clinical trials and statistics unit from cancer research uk ( c1491 / a15955 )  . 
we acknowledge the national institute for health and research biomedical research centre funding to the royal marsden nhs foundation trust and icr , the contributions of all patients who agreed to join the trial , the e orts of all the contributors and institutions as cited in the initial report of this trial , and roger ahern for his statistical input . published online october 3 , 2017 s1470 - 2045 ( 17 ) 30623 - x see articles page 1445 for more on nices interventional procedures guidance see org.uk / about / what - we - do / ourprogrammes / nice - guidance / nice - interventional - proceduresguidance for more on the national proton beam therapy programme see commissioning / spec - services / highly - spec - %20services / pbt / is competition bad for our health ( care ) ? we simply dont know in the lancet oncology , ajay aggarwal and colleagues1 apply innovative analytics to study the movement patterns of almost 20 000 patients accessing prostate cancer surgery across the national health service ( nhs ) in england between 2010 and 2014 . 
they find that , in the presence of pressures to centralise surgical services and intense competition , and in the absence of any publicly accessible measure of service quality to allow comparisons , those providers who invest in high tech , in this case robotic , surgery equipment , fare better than those who dont in attracting patients and growing their business . 
 moreover , in a previous analysis of referral patterns for specialised prostate cancer surgery , 2 the same authors showed that patients who travel longer distances , bypassing their local centres , tend to be younger , less ill , and of higher socioeconomic background than those who do not . 
 the authors conclude that , in the absence of any other reliable measure of quality or patient experience , patients are attracted by technology , contributing to what they describe as a natural selection process that shapes the market and has , thus far , unconfirmed effects on equity , overall cost , or outcomes . 
do competitive pressures end up undermining the nhss best efforts ( perhaps through the national institute for health and care excellence [ nice ] or professional guidelines and commissioning guides ) to coordinate the system to make it more efficient and effective and , ideally , more equitable ? are patients misled by high tech and smart marketing by providers investing in it ? and , most importantly perhaps , do patients exerting choice actually lead to better outcomes , and if so , for what type of patient and at what price for the nhs ? the answer is that we simply do not know ( for now )  . 
the authors analysis matters because forces us to ask all these questions , especially the so what question , when it comes to patient mobility and the competition policies that ( inadvertently or not ) trigger it . 
more questions emerge : what is the role of central entities such as nhs england or norm setters such as nice in management of service configuration and informing patient choice ? health technology assessment ( hta ) has been widely applied to pharmaceuticals through nice , but much less so to technologies such as surgical interventions . 
paradoxically , the only nice programme not to consider value for money is the interventional procedures guidance , under which surgery , including robotic surgery , is most likely to fall . 
could nice help providers to make decisions about major investment in high tech such as robots ? or would a more realistic approach be to invite bids from providers , as was the case with proton beam therapy , where nhs england set out its specification and trusts responded , with the successful ones selected through a competitive process ? an alternative to such top - down central planning might be to expand personal health budgets to actively encourage patients to shop around , hence promoting patient choice . 
but most would agree that health care is not a usual marketplace , 3 and regulation and information are both needed to make meaningful choices . somewhat depressingly , the authors are sceptical about the potential of developing an adequate measure of outcomes to benchmark providers and complement , if not substitute , technology - based marketing . 
in the nhs at least , political challenges due to inertia , confusion , or just not enough money and people to think about it all , may well outweigh the methodological challenges cited by the authors , such as the time lag between treatment and real outcomes . 
the nhs patient reported outcomes measures programme , having stalled after an impressive start a few years back , is a case in point.4 reading through the conclusions , parallels can be drawn with another case where the latest technology seemed to drive policy and investment . 
the cancer drugs fund ( cdf ) in england favours the latest cancer drugs , specifically those shown not to be good value for money by nice , at the expense of drugs for other diseases or indeed nondrug cancer interventions such as radiotherapy or surgery , as concluded recently by the same authors.5 despite a recent revamp , cdf remains a missed opportunity for 1424 vol 18 november 2017 comment generation of data on comparative effectiveness to inform patient and professional choice.6 in summary , this is a valuable study revealing the usually ad - hoc nature of policy making and its usually unstudied implications on peoples behaviour , which in turn influences health spending , outcomes , and distribution . 
instead , the authors offer a strong rationale for collecting and sharing data on ( comparative ) outcomes to inform investment choices at the central and provider level , as well as treatment choices by patients and their doctors . 
although controversial , rightly structured competition could save lives.7 , 8 we simply do not know but we must try to find out . kalipso chalkidou institute of global health innovation , imperial college london , london sw7 2az , uk k.chalkidou@imperial.ac.uk i declare no competing interests . copyright the author ( s )  . 
the bmj opinion nancy - devlin - john - appleby - david - parkin - why - has - the - promsprogramme - stalled / ( accessed aug 9 , 2017 )  . aggarwal a , fojo t , chamberlain c , davis c , sullivan r . 
 treatment choice in egfr - mutant non - small - cell lung cancer palliative therapy for patients with non - small - cell lung cancer ( nsclc ) harbouring an activating egfr mutation has improved with the approval of targeted therapy , namely the first - generation tyrosine kinase inhibitors ( tkis ) gefitinib and erlotinib , which have both shown significant efficacy in terms of tumour response and progression - free survival when compared with platinum - based chemotherapy in phase 3 trials . 
the same is true for afatinib , which is a second - generation irreversible inhibitor of tyrosine kinase activity , of not only egfr , but also all members of the her ( or erbb ) family ( a pan - her inhibitor )  . 
additionally , a combined analysis of two phase 3 trials ( lux - lung 3 and 6 ) 1 showed , for the first time , that afatinib significantly prolonged overall survival compared with platinumbased doublet chemotherapy in patients with common egfr mutations , and especially those with the del19 mutation . 
the subsequent lux - lung 7 study in 20162 was the first to do a head - to - head comparison of a second - generation and a first - generation tki . 
the difference in the primary endpoint of progression - free survival between the groups was both statistically and clinically significant : patients in the dacomitinib group had a median progression - free survival of 147 months ( 95% ci 111166 ) compared with 92 months ( 91110 ) in the gefitinib group ( hazard ratio [ hr ] 059 , 95% ci 047074 ; p < 00001 )  . 
a subgroup analysis showed that asian patients benefitted more published online september 25 , 2017 s1470 - 2045 ( 17 ) 30684 - 8 see articles page 1454 vol 18 november 2017 1425 comment risk of subsequent primary neoplasms in survivors of adolescent and young adult cancer ( teenage and young adult cancer survivor study ) : a population - based , cohort study chloe j bright , raoul c reulen , david l winter , daniel p stark , martin g mccabe , angela b edgar , clare frobisher , michael m hawkins summary background few studies have investigated the risks of subsequent primary neoplasms after adolescent and young adult ( aya ) cancer . 
we investigated the risks of specific subsequent primary neoplasms after each of 16 types of aya cancer . methods the teenage and young adult cancer survivor study is a population - based cohort of 200 945 survivors of cancer diagnosed when aged 1539 years in england and wales from jan 1 , 1971 , to dec 31 , 2006 . 
in this analysis , we focus on the risk of specific subsequent primary neoplasms after 16 types of aya cancer : breast ; cervical ; testicular ; hodgkin lymphoma ( female ) ; hodgkin lymphoma ( male ) ; melanoma ; cns ( intracranial ) ; colorectal ; non - hodgkin lymphoma ; thyroid ; soft - tissue sarcoma ; ovarian ; bladder ; other female genital ; leukaemia ; and head and neck cancer . 
we report absolute excess risks ( aers ; per 10 000 person - years ) and cumulative incidence of specific types of subsequent primary neoplasm after each type of aya cancer . findings during the 2 631 326 person - years of follow - up ( median follow - up 168 years , iqr 105252 ) , 12 321 subsequent primary neoplasms were diagnosed in 11 565 survivors , most frequently among survivors of breast cancer , cervical cancer , testicular cancer , and hodgkin lymphoma . 
aers of any subsequent primary neoplasms were 195 per 10 000 person - years ( 95% ci 174215 ) in survivors of breast cancer , 102 ( 80124 ) in survivors of cervical cancer , 189 ( 166211 ) in survivors of testicular cancer , 557 ( 504611 ) in female survivors of hodgkin lymphoma , and 299 ( 263336 ) in male survivors of hodgkin lymphoma . 
the cumulative incidence of all subsequent primary neoplasms 35 years after diagnosis was 119% ( 95% ci 113126 ) in survivors of breast cancer , 158% ( 148167 ) in survivors of cervical cancer , 202% ( 189215 ) in survivors of testicular cancer , 266% ( 247286 ) in female survivors of hodgkin lymphoma , and 165% ( 152180 ) in male survivors of hodgkin lymphoma . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma in women , breast cancer , and hodgkin lymphoma in men , we identified a small number of specific subsequent primary neoplasms that account for 82% , 61% , 58% , 45% , and 41% of the total excess number of neoplasms , respectively . 
lung cancer accounted for a notable proportion of the excess number of neoplasms across all aya groups investigated . interpretation our finding that a small number of specific subsequent primary neoplasms account for a large percentage of the total excess number of neoplasms in long - term survivors of cervical , breast , and testicular cancer , and hodgkin lymphoma provides an evidence base to inform priorities for clinical long - term follow - up . 
the prominence of lung cancer after each of these aya cancers indicates the need for further work aimed at preventing and reducing the burden of this cancer in future survivors of aya cancer . funding cancer research uk , national institute for health research , academy of medical sciences , and children with cancer uk . copyright 2019 the author ( s )  . 
 we searched pubmed without any language or date restrictions using the keywords teenage and young adult cancer or adolescent and young adult cancer and survivor or long - term and second cancer or subsequent cancer on feb 16 , 2016 , for articles describing subsequent primary neoplasms in this population . 
a more focused search using each specific aya cancer as keywords ( eg , hodgkin lymphoma ) in place of teenage and young adult cancer or adolescent and young adult cancer was also done . 
we identified only one study that investigated the risk of subsequent primary neoplasms after the entire spectrum of aya cancers diagnosed at 1539 years of age . added value of this study to our knowledge , this is the largest study to investigate the risks of subsequent primary neoplasm after each specific aya cancer and the first to provide excess risks of specific types of subsequent primary neoplasm after each of 16 types of aya cancer . 
unlike previous studies , which focused on the multiplicative risk , we concentrated on the absolute excess riskie , the excess number of subsequent primary neoplasms beyond those expected from the general population , which is directly interpretable in terms of adverse health impact on survivors . 
additionally , we identified a small number of specific subsequent primary neoplasms that account for a substantial proportion of the total excess number of neoplasms in survivors of breast cancer , cervical cancer , testicular cancer , and hodgkin lymphoma . implications of all the available evidence our findings advance previous knowledge on the risks of subsequent neoplasms after aya cancer and provide an evidence base for identifying priorities for clinical follow - up of survivors of aya cancer . 
because lung cancer accounted for a notable proportion of the excess number of neoplasms across all aya groups investigated , there is need for work aimed at reducing this burden among future survivors . primary breast cancer and primary hodgkin lymphoma had the highest absolute excess risk ( 544 and 486 per 10 000 person - years , respectively )  . 
however , the study did not investigate the risks of specific subsequent primary neoplasms after each specific type of aya cancer . evidence from previous studies of childhood cancer survivors suggests that the principal factors determining risks of subsequent primary neoplasms relate to aspects of treatments received for the original cancer.1416 treatment of aya cancer varies greatly by cancer type and therefore , in the absence of detailed treatment information , it is essential to stratify risks by specific types of aya cancer ; such risk stratification provides an evidence base for clinical follow - up . the aims of this large - scale population - based study were to calculate risks of all and specific subsequent primary neoplasms after each type of aya cancer and to explore variation in these risks in relation to years from diagnosis , age at diagnosis , decade of diagnosis , and sex . methods study design and participants the teenage and young adult cancer survivor study ( tyacss ) was established using cancer registrations relating to neoplasms diagnosed between jan 1 , 1971 , and dec 31 , 2006 , in individuals aged 1539 years inclusive , which were obtained from the office for national statistics for english cancer registrations , and the welsh cancer intelligence and surveillance unit , public health wales , for welsh cancer registrations . 
both tumourrelated ( eg , tumour site , morphology , date of diagnosis ) and patient - related ( eg , sex , date of birth , national health service [ nhs ] number , and unique patient identifier ) information were obtained . 
the cancer registrations were checked for any errors , such as missing data in essential variables ( including sex , date of birth , date of diagnosis , tumour site , and tumour histology ) and incorrect chronology of events ( birth , cancer , death )  . 
 cancer registrations were excluded if the neoplasm was not malignant ( apart from intracranial , intraspinal , and bladder neoplasms where any behaviour was allowed ) , the histological type was not in the international classification of diseases for oncology classification , the histological type was a non - melanoma skin cancer ( these are underascertained by cancer registries ) , or if they were duplicate registrations . 
we also excluded individuals who had a previous childhood cancer included in the british childhood cancer survivor study.17 if an individual had multiple neoplasms diagnosed as an aya cancer , then the first was regarded as the index cancer for the cohort . 
ethical approval was provided by the national research ethics service and permission to process information without individual consent by the national information governance board for health and social care . see online for appendix 532 vol 20 april 2019 articles procedures information on cancer diagnosis , sex , age at cancer diagnosis , decade of cancer diagnosis , and years since diagnosis were derived from the cancer registration information . 
first primary neoplasms were grouped according to the internationally acknowledged classification scheme for tumours diagnosed in adolescence and young adulthood.18 carcinomas and germ cell tumours were further subdivided by anatomical site because of the implications of radiotherapy site for the risk of subsequent primary neoplasm ( appendix pp 35 )  . 
 we aimed to produce risk estimates after each specific first primary neoplasm ; therefore , survivors of cancers categorised as other cancers were not included ( appendix pp 2 , 6 )  . 
we focused on the risk of specific subsequent primary neoplasms after 16 types of aya cancer : breast ; cervical ; testicular ; hodgkin lymphoma ( female ) ; hodgkin lymphoma ( male ) ; melanoma ; cns ( intracranial ) ; lymphoma ; colorectal ; non - hodgkin thyroid ; soft - tissue sarcoma ; ovarian ; bladder ; other female genital ; leukaemia ; and head and neck cancer . 
 decade of diagnosis was divided into 197179 , 198089 , and 19902006 , in order to broadly describe differences in treatment given in these periods ( early chemotherapy , chemotherapy , and modern treatment era )  . 
years since diagnosis were classified using 10 - year bands following diagnosis . individual patient record linkage to national cancer registries enabled data to be obtained indicating when an individual in the cohort had a subsequent cancer registration . 
subsequent cancer registrations were classified as a subsequent primary neoplasm according to the international association of cancer registries ( iacr ) and international agency for research on cancer ( iarc ) rules for determining multiple primary tumours using the iacr / iarc tools software . 
 to reduce the likelihood of a local spread of the original aya cancer being classified as a subsequent primary neoplasm , potential subsequent primary neoplasms occurring in anatomical sites close to the first primary neoplasm were excluded ( appendix pp 78 )  . 
consequently , reported risk estimates are inevitably conservative . statistical analysis individuals were followed from 5 - year survival until the first occurrence of death , emigration , or study end date ( dec 31 , 2012 )  . 
absolute excess risks ( aers ) were calculated as the observed minus expected number of neoplasms , divided by the person - years at risk and multiplied by 10 000 . 
the expected number of neoplasms was derived by multiplying the number of person - years accrued , stratified by sex , attained age ( 5 - year bands ) , and calendar year ( 1 - year bands ) by the corresponding cancer rate in the general population of england and wales , 19 and summing appropriately . 
for aya cancers with 200 or more observed subsequent primary neoplasms , sirs are reported by specific type of subsequent primary neoplas we restrict attention to first primary neoplasm / subsequent primary neoplasm combinations with at least 100 subsequent primary neoplasms and a statistically significant sir . 
 we considered aers to be statistically significant at the 5% level ( two - tailed test ) if the 95% ci did not include 0 . incorporating aers were stratified by years from diagnosis , age at diagnosis , decade of diagnosis , and sex where there were at least 100 subsequent primary neoplasms . 
to explore the simultaneous effect of these explanatory factors , the multivariable poisson regression expected number of events was used to derive relative excess risks ( rers ) .20 rers can be interpreted as the ratio of aers adjusted for other potential explanatory factors included within the statistical model . 
aers by an explanatory factor are reported if both the univariable and multivariable tests for linear trend in the aers were each significant and the difference in the aers between the lowest and highest level of the risk factor was at least nine excess subsequent primary neoplasms . 
a likelihood ratio test was used to test for linear trend in a factor by comparing the log - likelihood of a model including the variable of interest with the log - likelihood of a model without the variable of interest . 
in deciding the percentage of the total aer attributable to specific subsequent primary neoplasms in relation to years from diagnosis , we ignored negative values for the aer and focused only on the positive values . 
thus , the total aer ( for the purposes of calculating percentages ) after each specific first primary neoplasm is the sum of the positive values for the contributing subsequent primary neoplasms . cumulative incidence was calculated treating death as a competing risk . 
other aya cancers were not included in the analysis of subsequent primary neoplasms . table 1 : cohort characteristics we did sensitivity analyses in which subsequent leukaemia was included among survivors of aya hodgkin lymphoma , leukaemia , and non - hodgkin lymphoma , and subsequent sarcoma was included among survivors of soft - tissue sarcoma and bone tumours . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results the tyacss cohort comprises 200 945 5 - year survivors of cancer diagnosed when aged 1539 years , between jan 1 , 1971 , and dec 31 , 2006 , in england and wales . 
during the 2 631 326 person - years of follow - up ( median follow - up 168 years , iqr 105252 ) , 12 321 subsequent primary neoplasms were diagnosed in 11 565 ( 6% ) of the 197 827 survivors included in the analysis . 
subsequent primary neoplasms were most frequently seen in survivors of breast cancer ( 1877 [ 15% ] of 12 321 subsequent primary neoplasms ) , cervical cancer ( 1675 [ 14% ] ) , hodgkin lymphoma ( 1606 [ 13% ] ) , and testicular cancer ( 1435 [ 12% ] ; table 1 )  . 
median follow - up was 143 years ( iqr 91223 ) in survivors of breast cancer , 202 years ( 128272 ) in survivors of cervical cancer , 177 years ( 117253 ) in survivors of testicular cancer , 193 years ( 123270 ) in female survivors of hodgkin lymphoma , and 196 years ( 121275 ) in male survivors of hodgkin lymphoma . 
investigation of all first primary neoplasm / subsequent primary neoplasm combinations with at least 100 subsequent primary neoplasms showed that neither age at diagnosis nor decade of diagnosis was systematically associated with aers , apart from age at diagnosis for breast cancer after female hodgkin lymphoma and decade of diagnosis for lung cancer after male hodgkin lymphoma ( appendix p 9 )  . 
 consequently , in this report we consider only variation of aers with years from diagnosis and sex . female survivors of breast cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 20 excess subsequent primary neoplasms per 10 000 person - years ( sir 18 , 95% ci 1718 ; aer 195 per 10 000 person - years , 95% ci 174215 ; table 2 )  . 
 sirs for subsequent primary cancers of ovarian , lung , corpus uteri , other genital , melanoma , and colorectal sites were statistically significantly increased ( table 3 )  . 
 the total aer of developing any subsequent primary neoplasm increased statistically significantly with time from breast cancer diagnosis to an aer of 256 per 10 000 person - years ( 95% ci 104408 ) subsequent to 30 years from diagnosis ( p < 00001 ; table 4 )  . 
consists of 80 small intestine , 62 gallbladder , 77 retroperitoneum and peritoneum , and 31 other or unspecified . table 3 : risk of specific subsequent primary neoplasms ( row headings ) after specific aya cancers * ( column headings ) with at least 200 subsequent primary neoplasms observed in total neoplasms ( total aer 289 per 10 000 person - years when negative aers are excluded )  . 
the total aer of developing any subsequent primary neoplasm increased with time from cervical cancer diagnosis to an aer of 323 per 10 000 person - years ( 95% ci 154491 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing lung , colorectal , and bladder cancer ( each vol 20 april 2019 articles 538 vol 20 april 2019 articles for the aers lung cancer p < 00001 ; table 4 )  . 
in patients who had survived at least ( 172 per 30 years , 10 000 person - years , 95% ci 88256 ) , colorectal cancer ( 107 , 35179 ) , and bladder cancer ( 101 , 45157 ) accounted for 37% , 23% , and 22% of the total number of excess neoplasms , respectively ( total aer 465 per 10 000 person - years when negative aers are excluded )  . 
 the cumulative lung , colorectal , and bladder neoplasms at 35 years from diagnosis were 36% ( 95% ci 3242 ) , 26% ( 2230 ) , and 13% ( 1016 ) , whereas incidences of 16% , 14% , and 04% were expected , respectively ( figure , table 5 )  . incidences of subsequent survivors of testicular cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 19 excess subsequent primary neoplasms per 10 000 person - years ( sir 18 , 95% ci 1719 ; aer 189 per 10 000 person - years , 95% ci 166211 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from testicular cancer diagnosis to an aer of 1270 per 10 000 person - years ( 95% ci 10001540 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing bladder , colorectal , lung , and prostate cancer ( each p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aers for prostate cancer ( 253 per 10 000 person - years , 95% ci 121386 ) , bladder cancer ( 228 , 130327 ) , colorectal cancer ( 196 , 92299 ) , and lung cancer ( 95 , 01188 ) accounted for 20% , 18% , 15% , and 8% of the total number of excess neoplasms , respectively . 
 incidences of subsequent primary the cumulative neoplasms at 35 years from diagnosis were 37% ( 95% ci 3144 ) for prostate , 29% ( 95% ci 2436 ) for bladder , 30% ( 2536 ) for colorectal , and 27% ( 2232 ) for lung , whereas incidences of 29% , 11% , 18% , and 20% were expected , respectively ( figure , table 5 )  . female survivors of hodgkin lymphoma had an excess risk of developing any subsequent primary neoplasm corresponding to 56 excess subsequent primary neoplasms per 10 000 person - years ( sir 31 , 95% ci 2933 ; aer 557 per 10 000 person - years , 95% ci 504611 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from hodgkin lymphoma diagnosis to an aer of 1686 per 10 000 person - years ( 95% ci 12952078 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing breast and lung cancer ( each p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aers for breast cancer ( 718 per 10 000 person - years , 95% ci 464972 ) and lung cancer ( 260 , 112408 ) accounted for 43% and 15% of the total number of excess neoplasms , respectively . 
the total aer of developing any subsequent primary neoplasm increased with time from hodgkin lymphoma diagnosis to an aer of 1219 per 10 000 person - years ( 95% ci 9131524 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing lung cancer ( p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aer for lung cancer ( 502 per 10 000 person - years , 95% ci 330673 ) accounted for 41% of the total number of excess neoplasms . 
the cumulative incidence of lung neoplasms in male survivors of hodgkin lymphoma was 51% ( 95% ci 4360 ) at 35 years from diagnosis , whereas an incidence of 14% was expected ( figure , table 5 )  . female survivors of thyroid cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 13 excess subsequent primary neoplasms per 10 000 person - years ( sir 14 , 95% ci 1215 ; aer 131 per 10 000 person - years , 95% ci 84178 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from thyroid cancer diagnosis to an aer of 219 per 10 000 person - years ( 95% ci 109 to 547 ) subsequent to 30 years from diagnosis , ( p = 003 ; table 4 )  . 
 the cumulative incidence of all subsequent primary neoplasms in female survivors of thyroid cancer was 182% ( 95% ci 161205 ) at 35 years from diagnosis ( table 5 ) , whereas an incidence of 136% was expected . 
the cumulative risks for the specific subsequent primary neoplasms add up to more than the overall cumulative risk because survivors can develop more than one subsequent primary neoplas * all subsequent primary neoplasms in female survivors excluding subsequent primary neoplasms of the breast . 
||all subsequent primary neoplasms in female survivors excluding subsequent primary neoplasms of the thyroid . table 5 : cumulative incidence of specific subsequent primary neoplasms after specific first primary neoplasms by years from diagnosis to 12 excess subsequent primary corresponding neoplasms per 10 000 person - years ( sir 14 , 95% ci 1215 ; aer 123 per 10 000 person - years , 95% ci 75171 ; table 2 )  . 
the cumulative incidence of all subsequent primary neoplasms was 139% ( 95% ci 122157 ) at 35 years from diagnosis ( table 2 ) , whereas an incidence of 123% was expected . both male and female survivors of cns tumours had an excess risk of developing any subsequent primary vol 20 april 2019 articles neoplasm corresponding to 15 and 11 excess neoplasms , respectively ( male survivors : sir 17 [ 95% ci 1519 ] ; aer 148 per 10 000 person - years [ 95% ci 107190 ] ; [ 1215 ] ; female survivors : sir 13 aer 111 [ 70152 ] )  . 
a statistically significant reduction in the sir for the development of a subsequent primary breast cancer was found ( sir 07 , 95% ci 0608 ; table 3 )  . 
the cumulative incidence of all subsequent primary neoplasms was 119% ( 95% ci 106133 ) in female survivors of cns tumours and 100% ( 87114 ) in male survivors of cns tumours at 35 years from diagnosis ( table 2 ) , whereas an incidence of 94% was expected . sensitivity analyses showed that inclusion of leukaemia after aya hodgkin lymphoma , non - hodgkin lymphoma , and leukaemia had little effect on the sirs and aers ( appendix p 10 )  . 
inclusion of sarcomas after aya softtissue sarcoma and bone tumour increased the aers , but there was substantial overlap in confidence intervals ( appendix p 10 )  . discussion we show that the excess number of subsequent primary neoplasms observed increases with increased period of follow - up from diagnosis after each aya cancer investigated . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma in women , breast cancer , and hodgkin lymphoma in men , we identified just a small number of specific subsequent primary neoplasms that account for 82% , 61% , 58% , 45% , and 41% of the total excess number of neoplasms , respectively . 
one study has previously addressed the risk of all subsequent primary neoplasms combined after each aya cancer , 3 but no study has previously considered specific subsequent primary neoplasms . in our study , the burden of the excess number of neoplasms beyond 30 years from diagnosis accounted for by lung cancer was substantial and apparent across all aya cancers investigated ( breast , cervical , testicular , and hodgkin lymphoma in males and females )  . 
additionally , smoking increases the risk of developing subsequent primary neoplasms , particularly oral or pharyngeal , oesophageal , stomach , lung , and haematological malignancies.21 kaul and colleagues22 reported that 33% of survivors of aya cancer were current smokers compared with 22% in a non - cancer comparison group matched on age , sex , and other factors . 
 although this decrease could be caused by a number of factors , it might be related to a change in smoking habits in more recent decades ( ie , a reduction in male smokers )  . 
 the evidence presented in our study , along with previous literature on smoking in cancer survivors , clearly suggests that clinical follow - up of survivors of aya cancer , particularly survivors of breast cancer , cervical cancer , and hodgkin lymphoma , should focus on subsequent lung cancer and provision of smoking cessation advice . generally , it is difficult to compare risks of subsequent primary neoplasms between survivors of aya and childhood cancer because there are so many important confounding influences . 
however , lung cancer as a subsequent primary neoplasm is an exception to this general rule in that from our population - based national cohort of survivors of childhood cancer in britain , we reported that in survivors aged 40 years and older , lung cancer was associated with an aer of only 29 per 10 000 person - years ( 95% ci 0455 ) , which accounted for just 9% of the total aer.28 by contrast , in the present analysis , the aer for lung cancer after at least 30 years from diagnosis of aya cancer was substantially higher and accounted for a much greater proportion of the total aer . 
notably , by contrast with survivors of aya cancer , the odds ratio for being a current regular smoker among survivors of childhood cancer in britain was 051 compared with the general population of britain.29 in female survivors of breast cancer , the sirs reported in our study were broadly consistent with those reported in previous literature.57 the increased risk of ovarian cancer could relate to shared hormonal and genetic ( eg , brca1 and brca2 mutations ) risk factors.30 the increased risk of uterine cancers might relate to partial oestrogen agonists used to treat the breast cancera previous large case - control study found that risk of uterine cancer increases with duration of tamoxifen treatment.31 of the six anatomical sites at which an excess of subsequent primary neoplasms was observed , only the lungs would be directly exposed if external - beam radiotherapy was used to treat the breast cancer . 
a previous large case - control study showed a dose - response relation between radiotherapy and risk of lung cancer in breast cancer survivors diagnosed at any age ( not aya - specific ) .26 existing literature suggests that chest 542 vol 20 april 2019 articles radiotherapy and smoking are both likely contributors to the substantial number of excess neoplasms accounted for by lung cancer . the bladder and bowel would be directly exposed if external - beam radiotherapy was used to treat cervical cancer . 
a large case - control study showed a doseresponse relation between radiotherapy and the risk of both bladder and rectal cancers in cervical cancer survivors.32 existing that pelvic irradiation and smoking are likely contributors to the number of excess neoplasms accounted for by lung , colorectal , and bladder cancer . 
clinical follow - up of survivors of aya cervical cancer , particularly where pelvic irradiation is used , should focus on lung , bowel , and bladder cancers . literature suggests treatment for testicular cancer can involve irradiating the para - aortic lymph nodes , which might explain the excess of subsequent primary neoplasms seen abdominal sites ( prostate , bladder , and colorectal )  . 
the excess of subsequent primary neoplasms observed in the abdomen is consistent with international studies of testicular cancer survivors.8 the excess of lung subsequent primary neoplasms might be caused by radiotherapy to the lungs , since previous studies have reported an increased risk of lung cancer in survivors of testicular cancer who were given chest radiotherapy.8 clinical follow - up of survivors of aya testicular cancer should focus on prostate , bladder , colorectal , and lung cancers . the lungs would be directly exposed if external - beam radiotherapy was used to treat hodgkin lymphoma ; previous studies of hodgkin lymphoma survivors have provided evidence of a dose - dependent increase in lung cancer risk with radiotherapy with or without chemotherapy.27 our findings are consistent with previous large - scale studies of female survivors of hodgkin lymphoma , for which a substantial amount of literature already exists , and by contrast with other aya cancers considered here , we have little to add.911 our findings support the decrease in lung cancer risk with more recent calendar period of diagnosis that was reported in a dutch study of hodgkin lymphoma survivors.9 this decrease might be due to a latency effect , where more recently diagnosed survivors simply have not had enough time to develop a lung subsequent primary neoplasm , or it might be caused by changes in treatment for hodgkin lymphoma during recent decades , including withholding the delivery of radiotherapy or radiotherapy resulting in less damage to healthy tissue than in previous decades.33 however , because a decrease in lung cancer risk was not seen after hodgkin lymphoma in women , it is possible that the decrease in lung cancer in men is caused by other environmental influences , such as changes in smoking habits . 
previous studies have reported an increase in the number of excess lung cancers with increasing years from diagnosis ; 9 , 10 however , to our knowledge , our study is the first to report the number of excess lung cancers in male and female improvements survivors separately . 
existing literature suggests that treatment ( radiotherapy and chemotherapy ) , in addition to smoking , could contribute to the number of excess neoplasms accounted for by lung cancer.9 clinical followup of male survivors of aya hodgkin lymphoma should focus on lung cancer and provision of smoking cessation advice . younger age at radiation exposure is a risk factor for the development of breast cancer in many populations exposed to radiation , including atomic bomb survivors , patients with tuberculosis monitored with x - rays , and children with benign disorders treated with radiotherapy.34 thus , the effect of age at diagnosis ( closely related to age at radiotherapy ) of hodgkin lymphoma on the risk of breast cancer in our cohort is not surprising . knowledge of late effects of cancer treatment has resulted in lower radiation exposures for treatments of good prognosis cancers in recent years ; 35 however , the multivariable regression showed the risk of developing a subsequent primary neoplasm did not vary with decade of diagnosis of aya cancer apart from lung cancer after hodgkin lymphoma in males . 
therefore , currently there is little evidence of a detectable impact . that until recently , no internationally agreed clinical guidelines existed regarding surveillance for specific types of neoplasm after aya cancer , but this is now being addressed by the international late effects of childhood cancer guideline harmonization group.36 so far , two such guidelines have been published.37 , 38 there are also guidelines in development relating to second primary cns tumours and second primary bowel cancers . strengths of our cohort study relate to its large scale and population - based design , with the inclusion of all 5 - year survivors of aya cancer in england and wales . 
our study had much greater statistical power than the only comparable previous study by lee and colleagues , 3 because we report almost double the number of subsequent primary neoplasms and an additional million person - years of follow - up . 
most previous studies investigating the risk of subsequent primary neoplasms with years from diagnosis have mainly focused on the sir , a measure of multiplicative risk that relates to an unspecified baseline risk and is therefore difficult to interpret . 
we concentrated on the aer , which is the excess number of subsequent primary neoplasms beyond those expected from the general population , and so is directly interpretable in terms of adverse health impact on survivors . 
to our knowledge , our study is the first to report aers by years from diagnosis for each specific aya cancer . a limitation of using cancer registration data is the absence of detailed treatment information . 
treatment for aya cancer varies greatly by cancer type ; therefore , in the absence of treatment data , we chose to determine risks in relation to specific cancer types . 
however , inevitably vol 20 april 2019 articles there is variation in the intensity of treatment given for a specific type of cancer , depending on the stage at diagnosis and whether the disease recurs or relapses after initial treatment . 
crude treatment information is inherent in cohort studies based on cancer registry data ; however , we are planning to conduct case - control studies with detailed treatment dosimetry , questionnaires for lifestyle and other relevant factors , and saliva collection for genotypic factors . 
a potential limitation of our study is that our results might not be generalisable to populations outside of england and wales . another limitation is the possibility that recurrence or metastases of the aya cancer could have been mistaken for a subsequent primary neoplas however , we used the iacr / iarc rules to define multiple primary cancers and further excluded any additional neoplasms close to the aya cancer site . 
thus , our estimate of the risk of specific subsequent primary neoplasms after specific aya cancers is probably conservative , and although many of the estimates we report are substantial , they are likely to be an underestimate of the true risk . in conclusion , our data show that the excess number of subsequent primary neoplasms observed increases with increased period of follow - up from diagnosis after each aya cancer investigated . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma , and breast cancer , we identified just a small number of specific subsequent primary neoplasms that account for high proportions of the total excess number of neoplasms . 
a notable finding was the excess number of neoplasms accounted for by lung cancer across all aya groups investigated in detail , in addition to subsequent primary neoplasms occurring in potentially irradiated sites . 
our findings provide an evidence base for clinical follow - up relating specifically to the aya population . contributors cjb did the literature search and data analysis , created the figure , and drafted the report . 
cjb , rcr , dlw , mmh , cf , dps , mgm , and abe interpreted the data , and reviewed and finalised the report . declaration of interests dps reports grants from teenage cancer trust , outside the submitted work . 
other funding was provided by a post - doctoral fellowship to rcr from the national institute for health research ( pdf - 2012 - 05 - 280 ) , and by the academy of medical sciences ( springboard health of the public 2040 ) and children with cancer uk . 
 study collaborators include sarah darby ( university of oxford ) ; richard feltbower ( university of leeds ) ; lorna anne fern ( university college london ) ; diana greenfield ( sheffield teaching hospital nhs foundation trust ) ; helen alexandra spoudeas ( university college london hospitals nhs foundation trust ) ; william hamish wallace ( royal hospital for sick children , edinburgh ) ; and jeremy whelan ( university college london hospitals nhs foundation trust )  . 
this report is independent research and the views expressed in this article are those of the author ( s ) and not necessarily those of nhs digital , cancer research uk , the national institute for health research , the office for national statistics , or the welsh cancer registry . instead be invested in smarter clinical trial designs that can answer relevant clinical questions , such as whether sequencing of drugs is better than combination therapies , or defining the optimal duration of adjuvant treatment . 
 fortunately , an embarrassment of riches . juan martin - liberal melanoma , sarcoma and genitourinary tumors unit , institut catal doncologia ( ico ) lhospitalet , 08907 barcelona , spain ; and molecular therapeutics research unit ( uitm ) , vall dhebron institute of oncology ( vhio ) , 08035 barcelona , spain jmartinliberal@gmail.com i have received lecture fees and travel grants from roche , novartis , msd , and bristol - myers squibb . luke jj , flaherty kt , ribas a , long gv . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
gb / document_library / summary_of_opinion_ - _initial_authorisation / human / 004579 / wc500252668.pdf ( accessed sept 5 , 2018 )  . another step towards improving oncofertility counselling of young women with hodgkins lymphoma possible chemotherapy - induced premature ovarian insufficiency is of great concern for female premenopausal patients with cancer . 
therefore , appropriate counselling on the risk of premature ovarian insufficiency is now mandatory in all countries.1 , 2 oncofertility counselling is of particular importance for women who have hodgkins lymphoma , who are often diagnosed at a young age . 
however , the counselling of these women can be quite complex because of the paucity of accurate data to estimate the effect of different chemotherapy regimens on their gonadal function . 
previous studies in this setting were mostly retrospective or relied only on menstrual function after treatment to define premature ovarian insufficiency , a measure that is not an optimal surrogate for assessing gonadal damage associated with treatment . in the lancet oncology , richard a anderson and colleagues3 report important results for helping physicians informing premenopausal women with advanced hodgkins lymphoma about the risk of chemotherapyinduced premature ovarian insufficiency associated with doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) or avd , or bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisone ( beacopp ) chemotherapy.3 in this substudy , done within the rathl trial ( nct00678327 ) , biomarkers of ovarian function during and up to 3 years after chemotherapy were assessed in women younger than 45 years at the time of diagnosis . 
specifically , 67 participants were monitored for serum antimllerian hormone concentrations and 321 participants for follicle - stimulating hormone concentrations despite a few limitations , including the small sample size of the antimllerian hormone analysis , particularly of those who were treated with beacopp , and the lack of collection of participant information from the main rathl cohort that could have had a potential effect on outcomes ( eg , use of hormonal contraceptives , previous fertility preservation procedures , and menstrual status after chemotherapy ) , this study provides more precise information than previous reports to counsel women with hodgkins lymphoma on gonadal damage induced by abvd , avd , or beacopp . 
 first , the study confirms that both the type of chemotherapy and patients age at the time of treatment remain the two major determinants of risk of premature ovarian insufficiency for all patients with cancer.4 , 5 antimllerian hormone concentrations decreased sub stantially during both chemotherapy regimens ; however , while antimllerian hormone published online september 13 , 2018 s1470 - 2045 ( 18 ) 30562 - x see articles page 1328 1264 vol 19 october 2018 comment concentrations recovered to before treatment levels in those patients given abvd or avd by 1 year after treatment , little recovery of antimllerian hormone concentrations was treatment with beacopp.3 in anderson and colleagues study , age was shown to be a crucial factor , with increased risk of chemotherapy - induced premature ovarian insufficiency after both regimens in women aged 35 years and older at the time of diagnosis . seen after second , these results highlight the need for a standardised definition of premature ovarian insufficiency . 
different endpoints ( menstrual function only , ovarian biomarkers onlyas in the present studyor a combination of the two ) and timing of its assessment ( ranging from a few months up to several years after chemotherapy ) have been used to define chemotherapyinduced premature ovarian insufficiency . 
 guidelines suggest use of a composite endpoint that includes both amenorrhoea and a hormone profile after menopause , 6 , 7 and assessing chemotherapy - induced pre mature ovarian insufficiency at least 2 years after the end of treatment.7 in the present study , recovery of ovarian function , as measured by follicle - stimulating hormone concentrations , occurred by 1 year after the end of treatment for most patients ( 75% treated with abvd or avd and 33% treated with beacopp ) , but recovery can also happen during the second year ( 18% of participants treated with abvd or avd and 50% with beacopp ) with little chance of recovery thereafter . 
these results support the expert opinionbased indication to assess ovarian function after chemotherapy no earlier than 2 years after treatment completion.7 third , although this study provides further evidence on the role of antimllerian hormone as a biomarker of gonadotoxicity , the clinical utility of its assessment during treatment and subsequent follow - up remains to be fully determined . 
as shown in other studies , 8 , 9 both resumption of menstrual function and spontaneous conception can be observed low concentrations of antimllerian hormone.8 , 9 similarly , in anderson and colleagues study , 3 some pregnancies were observed in women with very low antimllerian hormone levels . 
hence , the best predictor of infertility in cancer survivors remains to be identified . in women with finally , this study raises the crucial issue of discussing the possibility of reducing the risk of premature ovarian insufficiency.1 , 2 preservation of ovarian function ( ie , reducing the risk of chemotherapy - induced premature ovarian insufficiency ) should be distinguished from preservation of fertility ( ie , improving the chances of pregnancy after treatment ) and can be considered of important value also by women without childbearing desire . 
while cryopreservation of gametes is the first option to preserve fertility , the use of temporary ovarian suppression with gonadotropin - releasing hormone agonists during chemotherapy can now be offered for ovarian function preservation in patients with breast cancer , but its efficacy has not yet been shown in patients with hodgkins lymphoma.9 , 10 the results of anderson and colleagues study highlight the importance of discussing access to these options in women older than 35 years , irrespective of chemotherapy type , and among candidates to the beacopp regimen , irrespective of their age . 
very young women undergoing abvd or avd chemotherapy probably do not need to access these options , but they could be proposed later in life if additional treatments are required . results from the ovarian function biomarker analysis ongoing within the ahl 2011 trial ( nct01358747 ) are awaited to provide further evidence on the gonadotoxicity of beacopp chemotherapy in premenopausal women with hodgkins lymphoma . * matteo lambertini , isabelle demeestere breast cancer translational research laboratory , department of medical oncology , institut jules bordet ( ml ) and research laboratory on human reproduction , fertility clinic , cub - hpital erasme ( id ) , universit libre de bruxelles ( ulb ) , brussels 1000 , belgium matteo.lambertini85@gmail.com we declare no competing interests . 
j clin oncol 2013 ; 31 : 23139 . vol 19 october 2018 1265 comment published online september 10 , 2018 s1470 - 2045 ( 18 ) 30579 - 5 see articles page 1338 lambertini m , campbell c , bines j , et al . 
no evidence for the benefit of gonadotropin - releasing hormone agonist in preserving ovarian function and fertility in lymphoma survivors treated with chemotherapy : final long - term report of a prospective randomized trial . 
gonadotropin - releasing hormone agonists during chemotherapy for preservation of ovarian function and fertility in premenopausal patients with early breast cancer : a systematic review and meta - analysis of individual patient - level data . 
 camrelizumab for nasopharyngeal carcinoma : a new hope ? wenfeng fang and colleagues1 report on two phase 1 studies of the programmed cell death - 1 ( pd - 1 ) inhibitor , camrelizumab ( shr - 1210 ) , as a treatment for patients with recurrent or metastatic nasopharyngeal carcinoma . 
 the more interesting findings are the preliminary antitumor activity of camrelizumab in both settings : 31 ( 34% ; 95% ci 2444 ) of 91 patients who received previous treatment achieved an overall response with camrelizumab monotherapy ( two patients had a complete response ) and 20 ( 91% ; 7797 ) of 22 patients with the combination of camrelizumab and chemotherapy as first - line treatment ( one patient had a complete response )  . 
the keynote - 028 study2 showed that seven ( 26% ; 95% ci 111463 ) of 27 patients with previously treated , advanced disease achieved an objective response with pembrolizumab . 
the nci - 9741 trial3 showed that nine ( 205% ; 95% ci 98353 ; one complete repsonse ) of 44 patients with previously treated recurrent or metastatic naso pharyngeal carcinoma international studies achieved an objective response with nivolumab . 
both keynote - 028 and nci - 9741 are including 63% and 822% asian patients , respectively ; whereas the current study by fang and colleagues1 was done in an endemic chinese population . 
the proportion of who type 2 or 3 tumours in keynote - 028 was 667% , 822% in nci - 9742 , and 82% in the camrelizumab monotherapy trial of the current study . 
in terms of patient selection , keynote - 028 only included patients with programmed cell death ligand - 1 ( pd - l1 ) - positive tumours , whereas both nci - 9742 and the current study enrolled patients with unselected histologies . 
in nci - 9742 , 40% of patients had pd - l1 - positive tumours , which was associated with an improved response ( six [ 33% ] of 18 patients ) compared with pd - l1 - negative tumours ( three [ 13% ] of 23 patients )  . 
pd - l1 positivity also appears to be predictive of response to pd - 1 inhibitors in other head and neck squamous cell carcinomas.4 , 5 pd - l1 status was not reported by fang and colleagues in the current study . 
this outcome might suggest that previous priming with ipilimumab could improve the 1266 vol 19 october 2018 comment farewell to four greats as we begin a new year with optimistic anticipation of further achievements in oncology , we must pause to pay tribute to four major innovators and mentors who sadly died at the start of 2019 . on jan 2 , professor waun ki hong , a pioneering physician and scientist at the md anderson cancer center ( houston , tx , usa ) , died aged 76 . 
his work contributed to notable advances in chemoprevention , organ preservation in laryngeal cancer , and personalised targeted therapy . professor bertrand coiffier , who also died on jan 2 , aged 71 , was a leading lymphoma expert , who focused on developing new drug regimens to improve outcomes for aggressive lymphoma . 
he was a professor of hematology at the hospices civils de lyon and the university claude bernard ( lyon , france ) , and was a founding member and president of the groupe detude des lymphomes de ladulte , which later merged with another group to form the world - renowned lymphoma study association . jan 7 , professor john mendelsohn , a former president of the md anderson cancer center , died from glioblastoma , aged 82 . 
he helped to develop the monoclonal antibody cetuximab , which is used to treat colorectal , head and neck , and lung cancers . martin gore , professor of cancer medicine at the institute of cancer research and medical director at the royal marsden hospital ( london , uk ) , died suddenly on jan 10 aged 67 , reportedly after a yellow fever vaccination . 
 he received a cbe in the queens 2016 birthday honours list for services to oncology . as we reflect on the untimely loss of these four inspirational , leading oncologists , this has been a sadand unprecedentedway to start 2019 . 
 the lancet oncology big influences on anti - obesity strategies obesity , the second biggest preventable cause of cancer after tobacco smoking , is a major public health problem worldwide . 
governments must take steps to address this issue ; however , recent reports suggest that chinas antiobesity policies are being influenced by external players . increasingly westernised diets , escalating rural - to - urban migration , and sedentary lifestyles have caused chinas obesity levels to more than double since 1991 . 
in response , the chinese government has launched several public health campaigns , including happy 10 minutes , which encourages schoolchildren to have daily 10 - min breaks for exercise . 
why ? according to recent studies in the bmj and the journal of public health policy , the chinese governments attempts to tackle obesity are being supported by several large multinational food companies , including coca - cola , pepsi - cola , and nestl . 
these companies fund a noninternational life profit research organisation , the sciences institute ( ilsi ) , originally established in the usa in 1978 by a coca - cola executive . 
for several decades , ilsichina has led public health initiatives emphasising the importance of exercise and physical activityrather than nutritionas key to solving the obesity proble by focusing more on physical activity than on a healthy diet , attention is diverted away from highly processed food and calorie - dense snacks and drinks . 
shaping public health policy in this way could help the funding companies to protect sales of their own products and potentially avoid food regulations , advertising rules , and sugar taxes that have been introduced elsewhere . however , diet is clearly crucial . 
governments must not allow their public health strategies to be unduly influenced by powerful multinationals who might be more concerned with protecting their own interests than helping to solve this ongoing health crisis . 
 the lancet oncology vol 20 february 2019 for the bmj report see bmj 2019 ; 364 : k5050 . for the the journal of public health policy study see j public health pol 2019 ; published online jan 9 . 
10.1016 / s0140 - 6736 ( 18 ) 32822 - 8 editorial correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections corrections correction to lancet oncol 2015 ; 16 : 1338 correction to lancet oncol 2015 ; 16 : e434 bagcchi s . 
lancet oncol 2015 ; 16 : e434in this news item , the fourth sentence of the third paragraph should read patients with ccnd1 mutations had worse 2 - year overall survival than those without ( 381% [ 95% ci 14100 ] vs 80% [ 7684 ] ; p = 0005 ) ; similar outcomes were noted with alterations in the dna repair pathways ( tp53 , atm , atr , and znfhx4 mutations )  . 
triage by methylation - marker testing versus cytology in women who test hpvpositive on self - collected cervicovaginal specimens ( prohtect - 3 ) : a randomised controlled non - inferiority trial . 
lancet oncol 2015 ; 16 : 133543in this article , the title of figure 2 should have been kaplan - meier analysis of cumulative incidence of leukaemia for children with or without enterovirus infection after accounting for death as the competing risk . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . correction to lancet oncol 2015 ; 16 : 1289 lokody , i . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the fourth paragraph on liver transplants for patients with high risk hcc has been changed to read : of these , 17 had a liver transplant . 
the 5 - year survival of these patients was superior to those high risk patients that did not have a liver transplant ( 82% vs 38% ; p = 0033 )  . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . vol 16 october 2015 e480 correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
minimal data are available on the effect of maintenance lenalidomide in more aggressive disease states , such as patients with cytogenetic high - risk disease or patients ineligible for transplantation . 
we aimed to assess lenalidomide maintenance versus observation in patients with newly diagnosed multiple myeloma , including cytogenetic risk and transplantation status subgroup analyses . methods the myeloma xi trial was an open - label , randomised , phase 3 , adaptive design trial with three randomisation stages done at 110 national health service hospitals in england , wales , and scotland . 
there were three potential randomisations in the study : induction treatment ( allocation by transplantation eligibility status ) ; intensification treatment ( allocation by response to induction therapy ) ; and maintenance treatment . 
eligible patients for maintenance randomisation were aged 18 years or older and had symptomatic or non - secretory multiple myeloma , had completed their assigned induction therapy as per protocol and had achieved at least a minimal response to protocol treatment , including lenalidomide . 
patients were randomly assigned ( 1 : 1 from jan 13 , 2011 , to jun 27 , 2013 , and 2 : 1 from jun 28 , 2013 , to aug 11 , 2017 ) to lenalidomide maintenance ( 10 mg orally on days 121 of a 28 - day cycle ) or observation , and stratified by allocated induction and intensification treatment , and centre . 
this study is registered with the isrctn registry , number isrctn49407852 , and clinicaltrialsregister.eu , number 2009 - 010956 - 93 , and has completed recruitment . findings between jan 13 , 2011 , and aug 11 , 2017 , 1917 patients were accrued to the maintenance treatment randomisation of the trial . 
 after a median follow - up of 31 months ( iqr 1850 ) , median progression - free survival was 39 months ( 95% ci 3642 ) with lenalidomide and 20 months ( 1822 ) with observation ( hazard ratio [ hr ] 046 [ 95% ci 041053 ] ; p < 00001 ) , and 3 - year overall survival was 786% ( 95% cl 756816 ) in the lenalidomide group and 758% ( 724792 ) in the observation group ( hr 087 [ 95% ci 073105 ] ; p = 015 )  . 
on prespecified subgroup analyses by transplantation status , 3 - year overall survival in transplantation - eligible patients was 875% ( 95% cl 843907 ) in the lenalidomide group and 802% ( 760844 ) in the observation group ( hr 069 [ 95% ci 052093 ] ; p = 0014 ) , and in transplantationineligible patients it was 668% ( 616721 ) in the lenalidomide group and 698% ( 644752 ) in the observation group ( 102 [ 080129 ] ; p = 088 )  . 
by cytogenetic risk group , in standard - risk patients , 3 - year overall survival was 864% ( 95% ci 800909 ) in the lenalidomide group compared with 813% ( 742867 ) in the observation group , and in high - risk patients , it was 74.9% ( 658819 ) in the lenalidomide group compared with 637% ( 528727 ) in the observation group ; and in ultra - high - risk patients it was 629% ( 460758 ) compared with 435% ( 222631 )  . 
the most common grade 3 or 4 adverse events for patients taking lenalidomide were haematological , including neutropenia ( 362 [ 33% ] patients ) , thrombocytopenia ( 72 [ 7% ] patients ) , and anaemia ( 42 [ 4% ] patients )  . 
 460 deaths occurred during maintenance treatment , 234 ( 21% ) in the lenalidomide group and 226 ( 27% ) in the observation group , and no deaths in the lenalidomide group were deemed treatment related . interpretation maintenance therapy with lenalidomide significantly improved progression - free survival in patients with newly diagnosed multiple myeloma compared with observation , but did not improve overall survival in the intention - to - treat analysis of the whole trial population . 
 in patients with high - risk disease , relapse is the result of the persistence of residual disease , 2 , 3 even at very low levels , and is associated with clonal evolution and progressive immune dysfunction.4 , 5 these biological features can impair the activity of subsequent lines of therapy ; therefore , finding strategies that could prevent relapse in this group would be a considerable step forward to improve the outcomes of these patients.6 control or elimination of residual disease clones might be achieved by maintenance therapy , and several strategies have been assessed in this setting , with lenalidomide being the most promising because of its mode of action and tolerability.79 our preceding study , the medical research council myeloma ix trial , 10 compared the use of the immunomodulatory agent thalidomide as maintenance therapy with observation in patients with newly diagnosed multiple myeloma . 
our findings were consistent with the results of other contemporaneous thalidomide maintenance studies.11 , 12 the myeloma xi study was therefore designed to assess whether the newer , better tolerated , immunomodulatory agent lenalidomide limitations of thalidomide as could overcome the maintenance improve therapy progression - free survival and overall survival in patients with newly diagnosed multiple myeloma . this setting and binding of lenalidomide to the cereblon complex13 leads to the ubiquitination of substrates , including the transcription factors ikaros and aiolos , marking them for proteasomal degradation and resulting in decreased expression of interferon regulatory factor 4 ( irf4 ) .14 , 15 lenalidomide has direct tumouricidal effects on myeloma cells and also triggers indirect immuno modulatory effects , including activation of natural killer and t cells , which might help with elimination of minimal residual disease in patients with multiple myeloma.1417 whether or not these mechanisms can help to control residual clonal disease in patients with high - risk cytogenetic disease is unknown . three previous studies have shown that lenalidomide maintenance can delay disease progression after research in context evidence before this study a search of pubmed for clinical trial reports published in english before may , 2010 , using the terms lenalidomide and myeloma and maintenance revealed no published randomised studies of lenalidomide maintenance in patients with newly diagnosed myeloma . 
we showed a significant benefit of lenalidomide maintenance therapy in terms of progression - free survival , which was consistent across both patients eligible for transplantation and those who were ineligible , as well as patients across all cytogenetic risk groups , even those with high - risk disease . 
however , a preplanned subgroup analysis indicates an overall survival benefit in transplantation - eligible patients across all cytogenetic risk groups , even those with high - risk disease , when treated with lenalidomide maintenance therapy after transplantation . implications of all the available evidence the results of the myeloma xi trial contribute to a body of evidence that suggests that the use of lenalidomide as maintenance therapy should be considered for patients with newly diagnosed multiple myeloma , of all cytogenetic risk groups , after autologous stem - cell transplantation . 
with the addition of these new data from the myeloma xi trial , a metaanalysis of all published trials of lenalidomide maintenance after autologous stem - cell transplantation , including 3179 patients , confirmed the overall survival benefit of lenalidomide maintenance therapy compared with observation in this setting ( hazard ratio 072 [ 95% ci 056091 ] )  . 
 in transplantation - ineligible patients , novel approaches to improve overall survival are warranted . vol 20 january 2019 articles autologous stem - cell transplantation in patients with multiple myeloma.79 overall survival outcomes were inconsistent between these studies , none of which was appropriately powered to make robust conclusions based on this endpoint . 
one study8 showed a clear overall survival benefit for those patients treated with maintenance lenalidomide compared with observation , whereas the other two studies7 , 9 showed no significant benefit . 
however , a recently published meta - analysis18 including these trials showed that lenalidomide main tenance can improve overall survival compared with observation in this setting , and it is now approved for use by both the european medicines agency and us food and drug administration . 
 for patients with multiple myeloma who are ineligible for trans plantation , continuous therapy with lenalidomide plus low - dose dexamethasone improved progression - free survival and overall survival compared with a combination of melphalan , prednisone , and thalidomide.19 , 20 no previous studies of either transplantation - eligible or transplantation - ineligible patients had sufficient num bers to assess the effect of lenalidomide maintenance therapy in patients with multiple myeloma and high - risk cytogenetics . here , we aimed to assess the effect of lenalidomide maintenance on the survival of patients with newly diagnosed multiple myeloma , including preplanned subgroup analyses by cytogenetic risk group and transplantation status . methods study design and participants the myeloma xi was a phase 3 , open - label , randomised , adaptive design trial with three randomisation stages ( figure 1 )  . 
there were three potential randomisations in the study : at trial entry for all patients to allocate induction treatment separately for those considered eligible or ineligible for transplantation ; after induction treatment for those patients with a suboptimal response to treatment ( minimal or partial response ) to allocate induction intensification ; and at the completion of induction and intensification or autologous stem - cell transplantation ( where applicable ) to allocate main tenance treatment . 
the trial was done at 110 national health service hospitals in england , wales , and scotland ( appendix p 2 )  . intensification the full study protocol including the inclusion criteria for each randomisation is available in the appendix ( p 34 )  . 
 patients aged at least 18 years and who had symptomatic multiple myeloma or non - secretory multiple myeloma based on bone marrow clonal plasma cells , organ or tissue impairment considered by the clinician to be myeloma related , or paraprotein ( m - protein ) in serum or initial randomisation . 
 urine were eligible for exclusion criteria for the initial randomisation included the previous or concurrent malig nancies , including myelodysplastic syndromes ; previous treatment for myeloma ( except local radiotherapy , bisphosphonates , and corticosteroids ) ; grade 2 or worse peripheral neuro pathy , acute renal failure ( unresponsive to up to 72 h of rehydration , characterised by creatinine > 500 mol / l or urine output < 400 ml per day , or requiring dialysis ) ; and active or previous hepatitis c infection . transplantation ( transplantation patients who were young and fit to tolerate autologous stem - cell eligible ) entered the intensive treatment pathway . 
however , generally , patients aged 60 years or younger entered the intensive ( younger , fitter ) pathway ; those aged 70 years or older entered the nonintensive ( older , less fit ) pathway ; and those aged 6169 years were eligible for either intensive or nonintensive therapy . 
the decision of treatment pathway was made on an individual patient basis , taking into account eastern cooperative oncology group performance status , clinician judgment , and patient preference . for the maintenance therapy randomisation , eligible patients were those who completed their assigned induction therapy according to the protocol ( a minimum of four cycles of cyclophosphamide , thalidomide , and dexamethasone [ ctd ] ; cyclophosphamide , lenali domide , and dexamethasone [ crd ] ; or carfilzomib , cyclophosphamide , lenalidomide , and dexamethasone [ kcrd ] in the intensive pathway , or a minimum of six cycles of attenuated ctd or attenuated crd in the non - intensive pathway ) , and had achieved at least a minimal response and received at least 100 mg / m melphalan if assigned to intensive treatment . the study was approved by the national ethics review board ( national research ethics service , london , uk ) , institutional review boards of the participating centres , and the competent regulatory authority ( medicines and healthcare products regulatory agency , london , uk ) , and was undertaken according to the declaration of helsinki and the principles of good clinical practice as espoused in the medicines for human use ( clinical trials ) regulations . 
the study is closed for accrual , but follow - up continues for planned long - term analysis . randomisation and masking patients considered eligible for transplantation at trial entry were randomly assigned ( 1 : 1 ) to induction treatment with either ctd or crd . 
a computer - generated minimisation algorithm was used to avoid chance imbalances in six variables measured at trial entry : microglobulin ( < 35 mg / l vs 35 < 55 mg / l vs 55 mg / l vs or unknown ) , haemoglobin ( < 115 g / l vs 115 g / l for men ; < 95 g / l vs 95 g / l for women ) , corrected serum see online for appendix vol 20 january 2019 articles induction 4420 patients randomly assigned to induction therapy * 2568 allocated to intensive treatment ( transplantation - eligible patients ) 1852 allocated to non - intensive treatment ( transplantation - ineligible patients ) 2142 excluded 368 died without progression 601 progressed and died 618 progressed and alive 478 withdrew from treatment 58 ineligible 19 unknown reasons 307 patients allocated to the lenalidomide and vorinostat group ( not part of this analysis ) maintenance 1971 randomly assigned to maintenance treatment 1137 allocated to the lenalidomide group ( intention - to - treat population ) 834 allocated to the observation group ( intention - to - treat population ) 40 patients did not commence lenalidomide 12 progressed before treatment initiation 23 withdrew consent 5 missing 1097 received allocated intervention ( safety population ) 834 received allocated intervention ( safety population ) 39 died without progression 193 progressed and died 224 progressed and alive 456 progression - free survival events and 234 overall survival events 8 progressed before randomisation and alive 2 progressed before randomisation and died 533 progression - free survival events and 226 overall survival events 13 died without progression 213 progressed and died 307 progressed and alive 7 progressed before randomisation and alive 671 patients are alive and progression free 294 patients are alive and progression free figure 1 : trial profile * randomisation occurred between may 26 , 2010 , and april 20 , 2016 . 
following a protocol amendment on june 28 , 2013 , and after the accrual of 1512 patients , patients considered eligible for trans plantation were randomly assigned ( 1 : 1 : 2 ) to ctd , crd , or kcrd . 
a similar minimisation algorithm was used to avoid chance imbalances in the six variables measured at trial entry . patients with a suboptimal response to induction treatment were randomly assigned ( 1 : 1 ) to cyclophosphamide , bortezomib and dexamethasone ( cvd ) or no cvd . 
a minimisation algorithm was used to avoid chance imbalances in three variables : allocated induction treatment ( ctd vs crd vs attenuated ctd vs attenuated crd ) , response to induction treatment ( minimal response or partial response ) , and centre . 
 patients allocated to kcrd induction treatment were ineligible for this randomisation . vol 20 january 2019 articles in induction and patients completing three variables : allocated intensification treatment ( where applicable ) and eligible were randomly assigned ( 1 : 1 ) to lenalidomide maintenance or observation . 
 a minimisation algorithm was used to avoid chance imbalances induction treatment ( ctd vs crd vs attenuated ctd vs attenuated crd ) , allocated intensification treatment ( no cvd vs cvd vs not randomised at intensification randomisation ) , and centre . 
following a protocol amendment on june 28 , 2013 , and after accrual of 615 further patients under protocol version 5.0 , patients were randomly assigned ( 2 : 1 ) to lenalidomide or observation . 
a similar minimisation algorithm was used to avoid chance imbalances in the same three variables with the same categories but with the addition of kcrd to the induction treatment options . 
these changes were made to add and remove research questions in this adaptive design study . all randomisations were done at the clinical trials research unit ( leeds , uk ) by authorised members of staff with a centralised automated 24 h telephone system according to a validated minimisation algorithm produced under the supervision of wmg . 
the funders remained masked to treatment results until data cutoff for analysis . procedures the dose , schedule , and route of administration of each drug included in the induction and consolidation regimens are in the protocol ( appendix p 34 )  . 
briefly , in transplantation - eligible patients , induction therapy with ctd , crd , or kcrd continued for at least four cycles in the absence of progressive disease , until maximum response or intolerance was observed . 
for all patients , bisphosphonates were recom mended until progressive disease and thrombo prophylaxis was recom mended for at least the first 3 months of treatment as per imwg recommendations . 
growth factor support and prophylaxis for pneumonia , varicella , fungal infection , and tumour lysis syndrome were allowed as per local practice . transplantation - eligible patients receiving kcrd proceeded to high - dose melphalan and autologous stem - cell transplantation . 
patients receiving immunomodulatory - based triplets ( ctd vs crd ) followed a response - adapted approach : those with complete response or very good partial response ( assessed according to international myeloma working group [ imwg ] criteria ) proceeded to autologous stem - cell transplantation in the transplantation - eligible pathway , whereas transplantation - ineligible patients proceeded directly to maintenance randomisation . 
for maintenance therapy , 100 days after autologous stem - cell transplantation or once a maximum response was achieved for transplantation - ineligible patients , patients initially received lenalidomide 25 mg per day ( orally on days 121 of each 28 - day cycle ) or were observed without lenalidomide therapy . 
following a protocol amendment on sept 14 , 2011 , and after accrual of 442 patients , patients were allocated ( 1 : 1 : 1 ) to receive lenalidomide 10 mg per day ( orally on days 121 of each 28 - day cycle ) , lenalidomide 10 mg per day ( orally on days 121 of each 28 - day cycle ) plus vorinostat 300 mg per day ( orally on days 17 and 1521 of each 28 - day cycle ) , or observation . 
after accrual of 615 more patients , a further protocol amendment on june 28 , 2013 , allocated patients to receive lenalidomide 10 mg per day ( orally on days 121 of each 28 - day cycle ) or observation in a 2 : 1 ratio , and the lenalidomide plus vorinostat group was discontinued . 
this change was proposed by the myeloma xi trial management group and approved by the myeloma xi data monitoring and ethics committee ( dmec ) on june 24 , 2011 . 
the change in dose was based on emerging results from previous studies using 10 mg lenalidomide weighted against the potential for late toxicity ( increased secondary primary malignancy ) , which was being reported in other trials at that time . 
patients receiving lenalidomide in combination with vorinostat will be reported elsewhere when the primary endpoint has been met in that group . response and disease progression were assessed on the basis of imwg uniform response criteria21 , 22 and reviewed centrally by an expert panel masked to treatment allocation . 
 serious adverse events were reported for all patients from the date of randomisation until 30 days after the date of disease progression except in the case of serious adverse reactions or second primary malignancies , which were collected for the duration of the trial . 
second primary malignancies were reported as serious adverse events for the duration of the study ( ie , until death for each patient or when the study closes , whichever was earlier )  . 
 on recovery , treatment was restarted at the previous dose , with the addition of granulocyte colony - stimulating factor in the case of grade 3 neutropenia with fever or grade 4 neutropenia . 
if neutropenia or thrombocytopenia occurred a second time , then the dose was reduced by one dose level as stipulated in the protocol ( eg , from 10 mg daily to 5 mg daily )  . 
full details of the dose reduction schedules are shown in the protocol ( appendix p 34 )  . cytogenetic risk profiling was performed by use of multiplex ligation - dependent probe amplification and quantitative real - time pcr using dna and rna respectively , which was extracted from cd138 - selected plasma cells from bone marrow biopsy samples taken before treatment initiation . 
quantitative real - time pcr was used to assess the expression of translocation gene partners including t ( 4 ; 14 ) : mmset , fgfr3 , t ( 14 ; 16 ) : maf , and t ( 14 ; 20 ) : mafb . 
multiplex ligation - dependent probe amplifi cation was used to assess copy number aberrations by including probe sets at sites of the commonly deleted or amplified regions in myeloma ( eg , at genes cks1b on 1q21.3 and tp53 on 17p13 )  . 
these techniques are validated and provide equivalent results to interphase fluorescence in - situ hybridisation.2325 patients were classified into three cytogenetic risk groups for the preplanned analysis of outcomes : standard risk ( no adverse cytogenetic abnormalities ) , high risk ( one adverse cytogenetic abnormality ) , or ultra - high risk ( two or more adverse cytogenetic abnormalities )  . 
adverse cytogenetic abnormalities were defined as gain ( 1q ) , t ( 4 ; 14 ) , t ( 14 ; 16 ) , t ( 14 ; 20 ) , or del ( 17p ) .2 , 3 in a post - hoc analysis , an alternative cytogenetic high - risk classification was used , including patients with t ( 4 ; 14 ) , del ( 17p ) , or t ( 4 ; 14 ) and del ( 17p ) .7 outcomes the co - primary endpoints of the maintenance evaluation of the trial were progression - free survival and overall survival . 
overall survival was defined as the time from maintenance randomisation to death from any cause or last follow - up . secondary endpoints were progression - free survival 2 , defined as the time from maintenance randomisation to the date of second progressive disease , start of third antimyeloma treatment , or death from any cause ; the time to improved response ; and toxicity . 
exploratory analyses of progression - free survival , overall survival , and response by cytogenetic risk group in the overall population and by cytogenetic risk group were prespecified by protocol and by induction / intensification treatment were prespecified in the statistical analysis plan within each pathway . lactate dehydrogenase , iu / l 262 ( 178381 ) 271 ( 183366 ) cytogenetic risk assessment available transplantation eligibility and induction regimen transplantation eligible kcrd transplantation ineligible attenuated ctd attenuated crd vol 20 january 2019 articles this in the statistical analysis the data cutoff date for this analysis was oct 23 , 2017 . 
we present here the results of the co - primary endpoints , some secondary endpoints ( progression - free survival 2 and toxicity ) , and prespecified subgroup analysis for the trial . 
for progression - free survival , the trial was designed to demonstrate a 67 - month increase in median progression - free survival lenalidomide group ( median 267 months ) compared with the observation group ( median 200 months , hazard ratio [ hr ] 075 ) when 509 progression - free survival events had been observed . 
 for overall survival , it was designed to demonstrate a 10% increase in 5 - year overall survival in the lenalidomide group ( 60% at 5 years ) compared with the observation group ( 50% at 5 years , hr 074 ) when 458 overall survival events had been observed . 
each of these calculations assumed the time to event was exponentially distributed and that recruitment would last 325 years with 4 years of further follow - up , a two - sided 5% significance level , and 90% power . 
patients randomly assigned during a transient period of the trial to the combination of lenalidomide and vorinostat ( n = 307 ) , as per the protocol modification on sept 14 , 2011 , were excluded from this analysis and will be reported elsewhere . for the co - primary endpoints , we estimated summaries of time to event per treatment group using the kaplanmeier method . 
we made comparisons between the allocated groups using the cox proportional hazards model stratified by the minimisation stratification factors , excluding centre , and to estimate hrs and 95% cis . 
we also did sensitivity analyses for progression - free survival using similar models in which those participants identified to have progressed in advance of maintenance randomisation were defined as having an event at the time of maintenance randomisation . 
subgroup analysis was prespecified for the presence or absence of individual adverse cytogenetic abnormalities , cytogenetic risk status , and induction and consolidation treatment ( cvd intensification and transplantation eligibility )  . 
we did a likelihood ratio test for heterogeneity of treatment effect using cox models identical to those used for the main analysis , with the inclusion of terms for the lenalidomide group ( n = 1137 ) observation group ( n = 834 ) ( continued from previous page ) cvd randomisation after minimal or partial response allocated to cvd allocated to no cvd received cvd after stable or progressive disease response at maintenance randomisation complete or very good partial response partial or minimal response stable or progressive disease unable to assess unknown 79 ( 7% ) 98 ( 9% ) 16 ( 1% ) 945 ( 83% ) 172 ( 15% ) 8 ( 1% ) 10 ( 1% ) 2 ( < 1% ) 63 ( 8% ) 78 ( 9% ) 8 ( 1% ) 705 ( 85% ) 118 ( 14% ) 6 ( 1% ) 1 ( < 1% ) 4 ( < 1% ) data are median ( iqr ) , n ( % ) , or n / n ( % )  . 
 stratification factor in minimisation algorithm . table 1 : baseline characteristics subgroup in question and the appropriate interaction ter the reported test for heterogeneity for subgroup analysis corresponds to a one degree of freedom test for two category subgroups and a two degrees of freedom test for three category subgroups . we summarised toxicity , in terms of adverse events , descriptively . 
we used fine and gray competing risks regression to compare the hazard of second primary malignancies by allocated treatment , adjusting for the minimisation stratification factors , with unrelated deaths specified as a competing risk . 
we calculated person - years on trial as the sum of all patients receiving at least one dose of study treatment of the time in years from randomisation to death or last date known to be alive . 
to ensure an overall significance level of 5% was maintained , we used the obrien and fleming alpha - spending function with bounds specified at the time of the interim analysis related to the proportion of information accrued ( interim analysis bound 094% , final analysis bound 47% )  . 
all reported p values are two sided and considered significant at an overall significance level of 5% . we used sas ( version 9.4 ) , stata / ic , and r ( version 3.2.3 ) for statistical analyses . this study is registered with the isrctn registry , number isrctn49407852 , and clinicaltrialsregister.eu , number 2009 - 010956 - 93 . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results the maintenance 1971 patients were accrued randomisation between jan 13 , 2011 , and aug 11 , 2017 . 
 patient and disease characteristics were well balanced between groups ( table 1 )  . lenalidomide and 20 months the median follow - up after randomisation for this analysis was 31 months ( iqr 1850 )  . 
for the primary analyses , 456 ( 40% ) of 1137 patients in the lenalidomide group and 533 ( 64% ) of 834 patients in the observation group had disease progression or died . 
median progression - free survival was 39 months ( 95% ci 3642 ) with ( 1822 ) with observation ( hr 046 [ 95% ci 041053 ] ; p < 00001 ; figure 2a )  . 
a sensitivity analysis including those patients who had disease progression before maintenance randomisation , in which events were defined at the time of maintenance randomisation rather than being censored at the time of maintenance randomisation , gave similar results ( appendix p 33 )  . 234 ( 21% ) of 1137 patients died in the lenalidomide group and 226 ( 27% ) of 834 patients died in the observation group . 
 3 - year overall survival was 786% ( 95% cl 756816 ) in the lenalidomide group and 758% ( 724792 ) in the observation group , and 5 - year overall survival was 613% ( 95% cl 566661 ) in the lenalidomide group and the observation group . 
no 566% ( 515617 ) difference was detected between lenalidomide and observation for overall survival ( hr 087 [ 95% ci 073105 ] ; p = 015 ; figure 2b )  . 
the most common cause of death was tumour load ( appendix p 25 )  . 285 ( 25% ) of 1137 patients in the lenalidomide group and 328 ( 39% ) of 834 patients in the observation group had second disease progression or died . 
median progressionfree survival 2 was 64 months ( 95% ci 57not reached ) vol 20 january 2019 articles with lenalidomide and 45 months ( 4150 ) with observation ( hr 065 [ 95% ci 056077 ] ; p < 00001 ; figure 3 )  . at the time of analysis , the median duration of therapy was 18 cycles lenalidomide maintenance ( iqr 630 )  . 
reasons for discontinuing in the 594 patients who had ceased lenalidomide maintenance were disease progression or death in 320 ( 54% ) patients , adverse events in 167 ( 28% ) patients , patient preference in 45 ( 8% ) patients , other reasons for 43 ( 7% ) patients , and unknown reasons for 19 ( 3% ) patients . 
the most common grade 3 or 4 haematological adverse reactions in the lenalidomide group were neutropenia in 362 ( 33% ) patients , thrombocytopenia in 72 ( 7% ) patients , and anaemia in 42 ( 4% ) patients . 
serious adverse events were reported in 494 ( 45% ) of 1097 patients receiving lenalidomide compared with 150 ( 17% ) of 874 patients on observation ( appendix p 29 )  . 
the 3 - year cumulative incidence of second primary malignancies was low , but higher in the lenalidomide group than the observation group ( 53% [ 95% ci 3671 ] vs 31% [ 1845 ] ; hr 185 [ 95% ci 118290 ] ; appendix p 5 )  . 
the overall incidence of second primary malignancies per 100 patient - years was 24 ( 95% ci 1931 ) in the lenalidomide group and 14 ( 1020 ) in the observation group . 
the 3 - year cumulative incidence of deaths related to second primary malignancies was low in both groups ( 20% [ 95% ci 0931 ] in the lenalidomide group vs 09% [ 0216 ] in the observation group ; appendix p 6 )  . 
 a summary of all second primary malignancies by intervention group is shown in the appendix ( p 30 )  . the most common serious adverse events were infections in both the lenalidomide group and the observation group . 
460 deaths occurred during maintenance treatment , 234 ( 21% ) in the lenalidomide group and 226 ( 27% ) in the observation group , and no deaths in the lenalidomide group were reported as treatmentrelated ( appendix p 25 )  . in the subgroup analyses , the benefit of lenalidomide on progression - free survival was seen across most sub groups of patients ( figure 4a ) , including those prespecified ( transplantation - eligible and transplantation - ineligible patients and those defined as standard risk , high - risk and ultra - high risk genetics )  . 
the only significant heterogeneity was between patients who achieved a complete or very good partial response and those who had a partial or minimal therapy ( pheterogeneity < 00001 )  . 
the table includes grade 1 or 2 adverse events occurring in at least 10% of patients and grade 3 or 4 events in at least 1% of patients ( the rest of the grade 3 and 4 adverse events are in the appendix pp 2628 )  . 
 table 2 : adverse events in patients treated with lenalidomide maintenance therapy ( n = 1097 ) vol 20 january 2019 articles progression - free survival was 57 months ( 95% ci 50not reached ) in the lenalidomide group and 30 months ( 2532 ) in the observation group in transplantationeligible patients ( hr 048 [ 95% ci 040058 ] ; p < 00001 ; figure 4b ) , and in transplantation - ineligible patients , median progression - free survival was 26 months ( 95% ci 2231 ) with lenalidomide and 11 months ( 523 ) with observation ( hr 044 [ 95% ci 037053 ] ; p < 00001 ; figure 4c )  . for the prespecified subgroup analysis by cytogenetic risk group , the baseline characteristics between patients with ( 774 [ 39% ] of 1971 ) and without ( 1197 [ 61% ] of 1971 ) cytogenetic data available were balanced ( appendix p 31 )  . 
 progression - free survival was improved in patients of all cytogenetic risk groups ( standard risk , high risk , and ultra - high risk ) who received lenalidomide compared with those on observation ( appendix p 9 ) ; the benefit lenalidomide was also seen across these risk categories when the intention - to - treat popu lation was divided into transplantation - eligible and transplantationineligible patients , with no significant heterogeneity between genetic subgroups ( pheterogeneity = 098 for transplantation - eligible patients , pheterogeneity = 076 for transplantation - ineligible patients ; appendix pp 1011 )  . 
similar results for progression - free survival were seen if the definition of high risk was restricted to patients with t ( 4 ; 14 ) , t ( 4 ; 14 ) and del ( 17p ) , or del ( 17p ) compared with those with out either t ( 4 ; 14 ) or del ( 17p ) , independently of transplantation eligibility ( appendix pp 1214 )  . 
 * likelihood ratio test for heterogeneity of effect among patients with subgroup data available . in the subgroup analysis of overall survival ( figure 5a ) , there was significant heterogeneity in outcomes based on pathway for previous induction treatment ( pheterogeneity = 00445 ) and age ( pheterogeneity = 00442 ) , with age probably acting as a surrogate for transplantation pathway eligibility . 
a significant improvement in overall survival was seen in transplantation - eligible patients treated with lenalidomide compared with those assigned vol 20 january 2019 articles to observation ( 3 - year overall survival in transplant [ 95% cl 843907 ] with eligible patients 875% lenalidomide and 802% [ 760844 ] with observation ; hr 069 [ 95% ci 052093 ] ; p = 0014 ; figure 5b )  . 
 however , lenalidomide maintenance therapy did not improve overall survival in transplantation - ineligible patients ( 3 - year overall survival 668% [ 616721 ] with lenalidomide and 698% [ 644752 ] with observation ; hr 102 [ 95% ci 080129 ] ; p = 088 ; figure 5c )  . 
the benefit of lenalidomide maintenance therapy on overall survival in the transplantation - eligible patients was also confirmed across subgroups based on age , disease stage , induction therapy , and response at baseline ( appendix p 15 )  . 
 * likelihood ratio test for heterogeneity of effect amongst patients with subgroup data available . 59 months ( 95% ci 52not reached ) for the observation group ( hr 057 , 95% ci 044073 ; p < 00001 ) ; and for transplant - ineligible patients it was 43 months ( 3948 ) for the lenalidomide group and 35 months ( 3139 ) for the observation group ( hr 072 , 058088 ; p = 00016 )  . 
the transplantationineligible group of patients had a higher frequency of nonmyeloma - related deaths ( appendix p 25 ) , and a high proportion of these patients initially assigned to the observation group subsequently received lenalidomide ( 103 [ 33% ] of 316 patients ) or ceased treatment before disease progression without intolerance ( 119 [ 29% ] of 407 patients )  . finally , to take account of all available results of lenalidomide as maintenance therapy for patients with multiple myeloma , we did a summary meta - analysis of our data with those previously published , including 3179 patients . 
these results show the hr for overall survival with the use of a lenalidomide maintenance regimen was 072 ( 95% ci 056091 ; appendix p 24 )  . the heterogeneity statistic i = 546 indicated potential moderate heterogeneity . 
no analysis of risk of bias was undertaken . discussion in this phase 3 , open - label , randomised trialwhich is , to our knowledge , the largest of its kindlenalidomide main tenance significantly improved progression - free survival compared with observation in adult patients with newly diagnosed multiple myeloma . 
however , overall survival was not improved with this treatment regimen in the intention - to - treat analysis . the progression - free survival benefit of maintenance therapy with lenalidomide seems to continue through the subsequent line of therapy with progression - free survival 2 significantly improved with lenalidomide compared with observation in both transplantation - eligible and trans plantation - ineligible patients . 
this hypo thesis is also supported by previous analyses indicating that lenalidomide maintenance did not increase genomic change or mutational load.26 , 27 a prespecified subgroup analysis suggested that continuous lenalidomide improved overall survival in transplantation - eligible patients but not in transplantationineligible patients . 
we speculate that any overall survival benefit in trans plantation - ineligible patients might have been attenuated by a high proportion of patients ceasing treatment prematurely and those initially randomised to observation who received lenalidomide in later lines of treatment . 
additional secondary and exploratory endpoints including response , survival after progression , time to progression , time to next line of treatment , changes in mean paraprotein during protocol treatment , and time to improved response will also be presented subsequently . an adverse cytogenetic profile is a major risk factor for relapse , and outcomes for patients with high - risk cytogenetics are poor.1 , 3 , 28 data supporting the use of lenalidomide maintenance in patients with adverse cytogenetics are scarce , and results thus far have been inconclusive . 
although the myeloma xi had a much larger sample size than that of previous studies , our subgroup analyses were not powered and further therefore are not conclusive and warrant investigation . 
however , baseline characteristics and outcomes were similar between patients with and without cytogenetic data available . another limitation of the trial is the lack of prospectively collected quality - of - life data . 
however , given that the time until first disease progression is often when patients with myeloma have a better quality of life , the improvement in progression - free survival and progression - free survival 2 seen in our study suggests the use of maintenance lenalidomide would be of benefit in the transplantationineligible setting . cytogenetic high risk has been defined by several groups using different markers . 
in our previous study , 3 identified adverse cytogenetic abnormalities as gain ( 1q ) , t ( 4 ; 14 ) , t ( 14 ; 16 ) , t ( 14 ; 20 ) , or del ( 17p ) , with standard risk ( no adverse cytogenetic abnormalities ) ; high risk ( one adverse cytogenetic abnormality ) , or ultrahigh risk ( two or more adverse cytogenetic abnormalities ) groups identified , and this classification was used in our prespecified analysis . 
 data using both of nevertheless , cannot equilibrate the outcomes for high - risk patients to those of standard risk , and patients with high - risk lesions still have combining maintenance lenalidomide with additional agents might be beneficial and could be investigated . 
in the myeloma xi trial , a separate group of patients received vorinostat plus lenalidomide in the maintenance randomisation because of a protocol amendment , and the outcomes of these patients will be reported elsewhere . 
in transplantation - eligible patients , three studies have shown that the addition of lenalidomide maintenance after autologous stem - cell transplantation reduces the risk of progression or death by approximately 50% compared with placebo or no maintenance.79 a significant improvement in overall survival has only been observed in one previous trial , 8 although a recent meta - analysis did suggest an overall survival improvement in patients treated with lenalidomide in this setting.15 to take account of all available results so far now including the myeloma xi study , we did a summary for transplantation - ineligible patients with multiple myeloma , a significant improvement in progression - free survival has been reported when lenalidomide maintenance was given after a regimen of melphalan , prednisone , and lenalidomide ( median progression - free survival from start of induction 31 months vs 14 months ) ; the 3 - year overall survival in this study was 70% with maintenance and 62% without maintenance therapy.29 furthermore , in a study comparing treatment with lenalidomide and low - dose dexamethasone given either continuously or for a limited number of cycles , 21 continuous treatment significantly improved progressionfree survival ( median 26 months vs 21 months from start of induction , hr 070 , 95% ci 060081 ) but there was no difference in overall survival ( median 591 months vs 623 months , 102 , 086120 )  . 
taken together , these observations suggest that alternative approaches to improving overall survival in older patients who are not eligible for transplantation are warranted . the current findings with lenalidomide maintenance compare favourably to those achieved with other novel therapies in the maintenance setting . 
thalidomide has been shown to improve progression - free survival when given as maintenance therapy in the myeloma ix trial ( median progression - free survival 22 months vs 15 months ; hr 144 , 95% ci 122170 ; p < 00001 ) , but the median overall survival was similar in both groups ( 60 months vs 60 months ; 096 , 079117 ; p = 070 ) .10 , 30 in a subgroup analysis , patients with high - risk status receiving thalidomide had no progression - free survival or overall survival benefit . 
by contrast , in this current study , we have shown that lenalidomide improves progression - free survival irrespective of cytogenetic risk status , which might be due to mechanistic differences between these drugs . 
although thalidomide and lenalidomide share a similar mechanism of action , recent studies suggest that subtle variations in the chemical structure between the molecules can modulate the range of substrates targeted for degradation by the e3 ubiquitin ligase , leading to different downstream effects.31 in the myeloma xi trial , few patients discontinued because of adverse events or patient preference and there was no evidence of cumulative toxicity . 
the risk of second primary malignancies was increased in patients treated with maintenance lenalidomide , but the 3 - year cumulative incidence of second primary malignancies remained low in both treatment groups . in summary , lenalidomide maintenance improved progression - free survival therapy significantly patients with newly diagnosed multiple myeloma compared with observation , but overall survival was not improved in the intention - to - treat analysis across the whole trial population . 
additionally , prespecified subgroups analyses by cytogenetic risk and transplantation status suggested a progression - free survival benefit across vol 20 january 2019 articles all cytogenetic risk groups , and an overall survival benefit in transplantation - eligible patients . should be directed to the corresponding author in the first instance ; to gain access , data requestors will need to sign a data access agreement . contributors ghj , fed , nhr , and gjm were chief investigators . 
all authors contributed to the review and amendments of the manuscript for important intellectual content and approved this final version for submission . declaration of interests ghj has received consultancy fees , honoraria and speakers bureau fees from roche , amgen , janssen , and merck sharp and dohme ; and consultancy fees , honoraria , travel support , research funding , and speakers bureau fees from celgene corporation and takeda . 
cdw has received honoraria , travel support , and speakers bureau fees from takeda , janssen , and celgene corporation ; honoraria and speakers bureau fees from amgen ; and honoraria from novartis . 
jl has received consultancy fees from janssen ; travel support from novartis and takeda ; consultancy fees and travel support from bristol - myers squibb ; and honoraria and travel support from celgene corporation . 
mwj has received consultancy fees , honoraria , travel support , and research funding from janssen ; consultancy fees , honoraria , and travel support from takeda and amgen ; consultancy fees , honoraria , and research funding from celgene corporation ; and consultancy fees and honoraria from novartis . 
gc has received consultancy fees , honoraria , research funding , and speakers bureau fees from takeda , celgene corporation , janssen , and amgen ; consultancy fees and honoraria from glycomimetics and bristol - myers squibb ; and consultancy fees , honoraria , and speakers bureau fees from sanofi . 
mfk has received consultancy fees and travel support from bristol - myers squibb and takeda ; consultancy fees from chugai ; consultancy fees and honoraria from janssen and amgen ; and consultancy fees , honoraria , and research funding from celgene corporation . 
 gjm has received research funding from janssen ; consultancy fees and honoraria from bristol - myers squibb and takeda ; and consultancy fees , honoraria , and research funding from celgene corporation . data sharing de - identified participant data will be made available when all trial primary and secondary endpoints have been met . 
any requests for trial data and supporting material ( data dictionary , protocol , and statistical analysis plan ) will be reviewed by the trial management group in the first instance . 
we are grateful to the uk national cancer research institute haematological oncology clinical studies group ; uk myeloma research alliance ; and all principal investigators , subinvestigators , and local centre staff for their dedication and commitment to recruiting patients to the study . 
 the support of the clinical trials research unit at the university of leeds ( uk ) was essential to the successful running of the study ; we thank all their staff who have contributed , past and present . 
central laboratory analysis was done at the institute of immunology and immunotherapy , university of birmingham ( uk ) ; the institute of cancer research , london ( uk ) ; and the haematological malignancy diagnostic service , st jamess university hospital , leeds . 
the authors received editorial support from excerpta medica , funded by the university of leeds . correction to lancet oncol 2018 ; 19 : e10212 sundar s , khetrapal - singh p , frampton j , et al . 
 lancet oncol 2018 ; 19 : e10212in this series paper , in the section titled challenges from womens cancer in india , the second sentence of the second paragraph should read despite this initiative , large - scale implementation of cancer prevention and control strategies has yet to take place , and public expenditure on health remains low at 12% of indias gross domestic product . 
this correction has been made to the online version as of may 31 , 2018 . correction to lancet oncol 2018 ; 19 : 72829 correction to lancet oncol 2018 ; 19 : 54961 iarc monographs vol 121 group . 
lancet oncol 2018 ; 19 : 54961in figure 3 of this article ( published online first on feb 20 , 2018 ) , the heatmap in panel a has been replaced to amend display errors . 
this correction has been made to the online version as of may 31 , 2018 . vol 19 june 2018 e283 corrections corrections correction to lancet oncol 2015 ; 16 : 1338 correction to lancet oncol 2015 ; 16 : e434 bagcchi s . 
lancet oncol 2015 ; 16 : e434in this news item , the fourth sentence of the third paragraph should read patients with ccnd1 mutations had worse 2 - year overall survival than those without ( 381% [ 95% ci 14100 ] vs 80% [ 7684 ] ; p = 0005 ) ; similar outcomes were noted with alterations in the dna repair pathways ( tp53 , atm , atr , and znfhx4 mutations )  . 
triage by methylation - marker testing versus cytology in women who test hpvpositive on self - collected cervicovaginal specimens ( prohtect - 3 ) : a randomised controlled non - inferiority trial . 
lancet oncol 2015 ; 16 : 133543in this article , the title of figure 2 should have been kaplan - meier analysis of cumulative incidence of leukaemia for children with or without enterovirus infection after accounting for death as the competing risk . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . correction to lancet oncol 2015 ; 16 : 1289 lokody , i . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the fourth paragraph on liver transplants for patients with high risk hcc has been changed to read : of these , 17 had a liver transplant . 
the 5 - year survival of these patients was superior to those high risk patients that did not have a liver transplant ( 82% vs 38% ; p = 0033 )  . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . vol 16 october 2015 e480 corrections correction to lancet oncol 2015 ; 16 : 1338 correction to lancet oncol 2015 ; 16 : e434 bagcchi s . 
lancet oncol 2015 ; 16 : e434in this news item , the fourth sentence of the third paragraph should read patients with ccnd1 mutations had worse 2 - year overall survival than those without ( 381% [ 95% ci 14100 ] vs 80% [ 7684 ] ; p = 0005 ) ; similar outcomes were noted with alterations in the dna repair pathways ( tp53 , atm , atr , and znfhx4 mutations )  . 
triage by methylation - marker testing versus cytology in women who test hpvpositive on self - collected cervicovaginal specimens ( prohtect - 3 ) : a randomised controlled non - inferiority trial . 
lancet oncol 2015 ; 16 : 133543in this article , the title of figure 2 should have been kaplan - meier analysis of cumulative incidence of leukaemia for children with or without enterovirus infection after accounting for death as the competing risk . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . correction to lancet oncol 2015 ; 16 : 1289 lokody , i . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the fourth paragraph on liver transplants for patients with high risk hcc has been changed to read : of these , 17 had a liver transplant . 
the 5 - year survival of these patients was superior to those high risk patients that did not have a liver transplant ( 82% vs 38% ; p = 0033 )  . 
on the one hand , draft guidelines by the uk national institute for health and care excellence ( nice ) did not recommend the use of axicabtagene ciloleucel ( kite pharma / gilead ) for various types of b - cell lymphoma in adults , a decision contrary to the approval of the drug in the eu and by the us food and drug administration . 
on the other hand , nhs england ( in lieu of a formal nice recommendation ) struck a clandestine deal with novartis via the cancer drugs fund to pay for tisagenlecleucel for children and young adults with b - cell acute lymphoblastic leukaemia . 
the deal , agreed less than 10 days after the european approval of the drug , means that patients in england could be the first in europe to gain access to the treatmenta remarkable prospect for the beleaguered nhs . 
taken alone , these results seem promising , but the lack of control group in both trials and the choice of surrogate primary endpoints make the benefits difficult to discern . 
but these differences are misleading and are a consequence of the scant clinical evidence available currently , and the subjective nature of clinical decision making for these specific treatments . the key driver of the nice and nhs england decisions has been cost . 
axicabtagene ciloleucel is believed to cost more than 50 000 per quality - adjusted life - year ( qaly ) gained , which is at the upper limit of tolerance for cancer treatments . 
the manufacturer has proposed a commercial arrangement that might sway the eventual decision in favour of approval , although at the time of writing , nice has requested the manufacturer find more uk data from which a comparison with the current standard of care can be made . 
tisagenlecleucel , by contrast , which is presumably costing less than the 282 000 list price in the arrangement secured by nhs england , might have a more favourable cost per qaly because children have a longer life expectancy than older patients , provided toxicities are manageable and not debilitating . 
ultimately , more robust evidence is needed to be able to make appropriate decisions , but the high prices set by pharmaceutical companies do make it difficult for universal health - care systems to justify cost - effectiveness and treatment availability . 
 developments the lancet oncology immunotherapy in the vol 19 october 2018 1259 editorial generic drugs : are they the future for affordable medicine ? industriesthe teva pharmaceutical largest manufacturer of generic drugs in the worldis in trouble . 
 this multinational company , which produces a large portfolio of genericsincluding several widely used oncology agents such as cisplatin , docetaxel , letrozole , and gemcitabinehas announced it will be cutting 14 000 jobs ( almost a quarter of its global workforce ) in attempts to salvage its ailing business . 
the move is a drastic response to tevas financial woes : in 2017 , the company lost more than us$20 billion from its market value , its us profits tumbled by 60% , and it is currently saddled with debts of $35 billion . 
the job cuts will be felt most acutely in israel , the location of tevas global headquarters , where it is one of the largest private sector employers andalarminglywhere its shares prop up much of the national pension pot . 
what has gone wrong , and is tevas situation symptomatic of wider issues in the generics industry ? in the past 40 years , teva has emerged as a major global player in the pharmaceutical industry , leading the movement towards the development of cheap generic drugs and biosimilars . 
such financial challenges have , in turn , created new problems , such as shortages of active ingredients or delays in manufacturing leading to decisions to discontinue some drugs altogether . 
the generics drugs market might have become a victim of its own success , as large generics manufacturers are being engulfed by the same market forces the patent - based pharmaceutical companies face . 
generics companies that also manufacture branded drugs suffer a double blow when the patents on their trademarked products run out , opening the door for their competitors to develop copycat versions ; for example , tevas financial woes were compounded in 2017 by the patent expiration of one of its most successful branded drugscopaxone ( glatiramer acetate ) for multiple sclerosis . 
meanwhile , non - generic drug companies are using acquisitions to continue to grow their revenues as quickly as possible , and as such many have bought smaller generics manufacturers to diversify their portfolio . 
instability and vulnerability to economic forces mean that the generic drugs market alone cannot be relied upon to lower drug prices and to ensure the continuous supply of affordable crucial medicines to those who need the what can be done ? better marketplace regulation is needed to maintain appropriate levels of supply and competition and to keep prices low , both by encouraging the development of new generics and protecting major generics manufacturers like teva that are seen as too big to fail . 
new policies to prevent market distortions and to ensure that generics manufacturers do not adopt the same de - stabilising economics of the patentbased pharmaceutical companies that created the need for cheaper generics in the first place are vital . 
 the lancet oncology for more on tevas financial problems and job cuts see com / 2017 / 12 / 27 / business / tevaisrael - layoffs.html for more on the pricing issues faced by generic drugs manufacturers see investors.com / news / technology / generic - drug - makers - facepricing - issues - unlike - otherpharma - companies / for more on generic drugs price increases see washingtonpost.com / business / economy / the - generic - drugindustry - has - brought - hugecost - savings - that - may - bechanging / 2017 / 08 / 01 / ee128d0a - 68cf - 11e7 - 8eb5cbccc2e7bfbf_story.html ? utm_ term = .cf2e80bd3ce4 for more on growth and merging within the generic drugs market see editorial lancet oncol 2015 ; 16 : 595 vol 19 february 2018 editorial kwon m , jang h , kim eh , roh jl . 
efficacy of poly ( adp - ribose ) polymerase inhibitor olaparib against head and neck cancer cells : predictions of drug sensitivity based on par - p53 - nf - b interactions . 
rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
 improving r - chop in diffuse large b - cell lymphoma is still a challenge since the introduction of rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ) as the gold standard for the treatment of diffuse large b - cell lymphoma , clinical investigators have constantly tried to improve its effectiveness by adding new drugs and proposing combinations ( ie , r - chop plus drug x ) .1 this strategy is justified by the great biological heterogeneity of diffuse lymphomas , suggesting that r - chop cannot be a universal treatment but can instead provide a rational basis for personalised therapy . 
as such , for the past decade molecular classification on the basis of the distinction between germinal centre b - cell - like and activated b - cell - like subtypes has largely dominated the debate and focused efforts in terms of targeted therapy and biomarker research.2 large b - cell to show the potential of such a strategy , biologically relevant , reliable , repro ducible biomarkers and a corresponding effective molecule that are likely to improve the efficacy of the r - chop regimen need to be identified . the prospective multicentre phase 3 remodl - b trial , reported in the lancet oncology by andrew davies and colleagues , 3 shows that real - time characterisation of diffuse large b - cell lymphoma is feasible by use of molecular biology with rna extracted from formalinfixed paraffin - embedded ( ffpe ) samples and cdnamediated annealing , selection , extension , and ligation techniques.3 among the 1128 eligible patients in this trial , 918 ( 81% ) were effectively classified according to their cell of origin ( 244 [ 27% ] activated b cell , 475 [ 52% ] germinal centre b cell , and 199 [ 22% ] unclassified )  . 
phenotyped patients were subsequently randomly assigned ( 1 : 1 ) after the first r - chop cycle to receive either r - chop or r - chop with bortezomib ( rb - chop )  . 
the primary outcome analysis showed that the addition of bortezomib does not provide any benefit in terms of progressionin the overall population ( 30 - month free survival progression - free survival 701% [ 95% ci 650747 ] with r - chop vs 743% [ 693787 ] with rb - chop ; adjusted hazard ratio 084 , 95% ci 064111 ; p = 023 ) , with the same conclusion drawn in the secondary outcome analyses in the germinal centre b - cell , activated b - cell , and unclassified subgroups . 
these results support those of a randomised phase 2 trial by leonard and colleagues.4 however , davis and colleagues point out a potential benefit of the combination for patients with double - hit lymphoma or dual - expressor lymphoma ( ie , myc and bcl2 ) , although this benefit was not significant . 
the results show that despite overexpression of the nuclear factor ( nf ) - b pathway and activating mutations of this pathway in activated b - cell diffuse large b - cell lymphoma , the addition of bortezomiba proteasome and nf - b pathway inhibitordoes not provide any benefit over r - chop.3 in diffuse large b - cell how can these ultimately disappointing results be explained ? a relative under - representation of the activated b - cell subtype as compared with previous lymphoma , 5 cohort studies substantially older patients in the activated b - cell subgroup , and the use of bortezomib only from the second cycle onwards , with a relatively low dose , might all have affected the efficacy outcome of the addition of bortezomib . 
a phase 3 randomised study ( phoenix ) 6 that specifically targeted the activated b - cell subtype did not clearly show the value of adding ibrutinib ( an inhibitor of brutons tyrosine kinase ) to r - chop in this setting . 
however , the toxicity of this combination in patients aged 60 years and older is probably partly responsible for the negative conclusion since a benefit in overall survival large b - cell published online april 1 , 2019 s1470 - 2045 ( 19 ) 30021 - x see articles page 649 vol 20 may 2019 comment and progression - free survival was observed for patients younger than 60 years.6 the prognostic effect of the cell - of - origin classification also remains uncertain and has been questioned in two prospective trials.5 data from the cavalli phase 2 trial7 showed a benefit in adding the bh3 ( bcl2 homology 3 ) mimetic venetoclax to r - chop in patients positive for bcl2 , irrespective of whether they had the germinal centre or non - germinal centre b cell subtype of disease , suggesting that a single biomarker ( bcl2 expression quantified by immunohistochemistry ) might be more relevant than cell - of - origin molecular determination for patient selection.7 new classifications that integrate next - generation sequencing , fluorescence in - situ hybridisation , or copy number variation data are now available and might offer other therapeutic or predictive opportunities.810 however , these models are complex , partially overlapping , and relatively difficult to test in a randomised clinical trial or apply in daily practice . 
the selection of diffuse large b - cell lymphoma patients on the basis of biological markers before the first treatment therefore remains a crucial challenge . fabrice jardin department of clinical hematology , centre henri becquerel , inserm u1245 , rouen university , rouen 76038 , france fabrice.jardin@chb.unicancer.fr i have received personal fees from roche , celgene , janssen , gilead , amgen , and servier . copyright 2019 the author ( s )  . 
gene - expression profiling of bortezomib added to standard chemoimmunotherapy for diffuse large b - cell lymphoma ( remodl - b ) : an open - label , randomised , phase 3 trial . 
randomized phase ii study of r - chop with or without bortezomib in previously untreated patients with non - germinal center b - cell - like diffuse large b - cell lymphoma . 
clinical impact of the cell - of - origin classification and the myc / bcl2 dual expresser status in diffuse large b - cell lymphoma treated within prospective clinical trials of the german high - grade non - hodgkins lymphoma study group . 
a global , randomized , placebo - controlled , phase 3 study of ibrutinib plus rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisone ( rchop ) in patients with previously untreated non - germinal center b - cell - like ( gcb ) diffuse large b - cell lymphoma ( dlbcl )  . 
cell 2017 ; 171 : 48194 . adjuvant capecitabine in biliary tract cancer : a standard option ? in the lancet oncology , john primrose and colleagues1 have tackled the question of adjuvant treatment for a rare cancer : biliary tract cancer , an unresolved question to date . 
although a meta - analysis ( of mostly retrospective data ) has suggested improved overall survival with adjuvant treatment ( especially chemotherapy in patients with node - positive disease and adjuvant radiation - based therapy after r1 resection ) , 2 older randomised studies were not sufficiently statistically powered to define a standard of care , 3 , 4 and two recent randomised studies did not show a significant benefit of gemcitabine5 or gemcitabine plus oxaliplatin ( gemox regimen ) .6 randomised , phase 3 , bilcap study , 753 patients were screened across 44 uk centres the between 2006 and 2014 , of whom 447 patients with curatively resected cholangiocarcinoma or muscleinvasive gallbladder cancer and preserved performance status ( eastern cooperative oncology group 0 or 1 ) were randomly assigned to receive oral capecitabine for 24 weeks or observation.1 unfortunately , the study did not meet its primary endpoint : the median overall survival by intention - to - treat was 511 months ( 95% ci 346591 ) in the capecitabine group compared with 364 months ( 297445 ) in the observation group ( hazard ratio [ hr ] 081 , 95% ci 063104 ; p = 0097 )  . should capecitabine be considered as ineffective as gemcitabine5 and gemox6 in the other two recent adjuvant trials ? probably not . 
 we aimed to assess the safety and feasibility of targeted release and enhanced delivery of doxorubicin to solid tumours from thermosensitive liposomes triggered by mild hyperthermia , induced non - invasively by focused ultrasound . methods we did an open - label , single - centre , phase 1 trial in a single uk hospital . 
patients received a single intravenous infusion ( 50 mg / m ) of lyso - thermosensitive liposomal doxorubicin ( ltld ) , followed by extracorporeal focused ultrasound exposure of a single target liver tumour . 
the trial had two parts : in part i , patients had a real - time thermometry device implanted intratumourally , whereas patients in part ii proceeded without thermometry and we used a patient - specific model to predict optimal exposure parameters . 
the primary endpoint was at least a doubling of total intratumoural doxorubicin concentration in at least half of the patients treated , on an intention - to - treat basis . 
this study is registered with clinicaltrials.gov , number nct02181075 , and is now closed to recruitment . findings between march 13 , 2015 , and march 27 , 2017 , ten patients were enrolled in the study ( six patients in part i and four in part ii ) , and received a dose of ltld followed by focused ultrasound exposure . 
the treatment resulted in an average increase of 37 times in intratumoural biopsy doxorubicin concentrations , from an estimate of 234 g / g ( sd 093 ) immediately after drug infusion to 856 g / g ( 569 ) after focused ultrasound . 
no treatment - related deaths occurred . interpretation the combined treatment of ltld and non - invasive focused ultrasound hyperthermia in this study seemed to be clinically feasible , safe , and able to enhance intratumoural drug delivery , providing targeted chemoablative response in human liver tumours that were refractory to standard chemotherapy . funding oxford biomedical research centre , national institute for health research . copyright 2018 the author ( s )  . 
focused ultrasound is the only non - invasive approach capable of generating highly targeted mild hyperthermia at depth within the body and is thus an attractive method for triggered drug release . vol 19 august 2018 1027 research in context evidence before this study achievement of targeted and efficacious drug delivery while avoiding off - target toxicity represents a universal challenge in oncology , especially for the treatment of metastatic cancer . 
 nanotechnology vehicles that passively accumulate or selectively release anticancer agents in solid tumours have shown substantial promise in preclinical studies but have not yet gained widespread adoption because of the absence of demonstrable clinical benefit . 
lyso - thermosensitive liposomal doxorubicin ( ltld ) is a thermally active liposomal drug delivery system capable of selectively releasing its cargo ( doxorubicin ) under conditions of mild hyperthermia . 
however , preclinical studies showed that , by using focused ultrasound to induce mild hyperthermia non - invasively after systemic administration of ltld , the intratumoural delivery and distribution for a given systemic dose of doxorubicin can be greatly enhanced , potentially increasing therapeutic efficacy . 
 because of the small number and heterogeneous nature of preclinical studies and the absence of clinical studies , we did not do a formal meta - analysis of existing literature in ultrasound - mediated targeted drug delivery . added value of this study to our knowledge , this clinical study is the first to investigate the safety and feasibility of extracorporeally triggered drug release in oncology and to quantify the potential benefits of this approach in terms of the drug dose , distribution , and cellular delivery , in addition to radiologically assessing the observed therapeutic response induced by a single systemically administered course of chemotherapy . 
our study showed the safety and feasibility of selectively maintaining non - ablative hyperthermia in tumours with volume up to 100 cm3 in the liver , by use of a clinically approved extracorporeal focused ultrasound device . 
additionally , our study showed quantitative measures of the pharmacokinetics and intratumoural drug accumulation derived from the use of liposomal carriers in several tumour subtypes , both before and after ultrasound exposure , providing much needed clinical data about the value of passive versus active methods of accumulating therapeutic agents in tumours . implications of all the available evidence our study showed the potential to attain a chemo - ablative response in otherwise refractory tumours when using a thermosensitive liposomal drug carrier in combination with non - invasive focused ultrasound . 
building on decades of promising preclinical research , in both therapeutic ultrasound and drug delivery systems , our study highlights the clinical potential of device - based drug delivery approaches in general , and ultrasound in particular , to achieve several - fold enhancements in the delivery and distribution of existing and future therapeutic agents to solid tumours , with potentially transformative implications for their therapeutic effectiveness at a given systemic dose . lyso - thermosensitive unlike non - thermosensitive liposomal doxorubicin ( ntld ) , liposomal doxorubicin ( ltld ; celsion corporation , lawrenceville , nj , usa ) releases its drug payload at temperatures above 395c.6 formulations enhance plasma pharmaliposomal cokinetics of doxorubicin , resulting in a plasma half - life in humans of about 10 h for ntld9 and 1 h for ltld , 10 much longer than that of free doxorubicin , which has a half - life of only minutes.10 the thermosensitive property of ltld has been used clinically , mainly in conjunction with minimally invasive radiofrequency ablation , which is used to thermally ablate the core of the tumour while ltld is circulating systemically , with the intention of improving therapy at the tumour margins.11 ltld was evaluated as part of the heat trial , 12 a pivotal phase 3 study of the use of radiofrequency ablation for the treatment of hepato cellular carcinoma . 
 the primary endpoint of the heat trial was not met ; in the intention - to - treat analysis , the progression - free survival hazard ratio ( hr ) of radio frequency ablation plus ltld versus radiofrequency ablation alone was 096 ( 95% ci 079118 ; p = 071 ) and the overall survival hr was 095 ( 076120 ; p = 067 )  . 
however , in a subgroup of 285 patients with a solitary hepatocellular carcinoma lesion who received a radiofrequency ablation dwell time of at least 45 min , the overall survival hr was 063 ( 041096 ; p < 005 ) in favour of combination therapy . 
the positive findings in this subgroup of the heat study led to the ongoing optima study ( nct02112656 ) , which is a randomised , double - blind , dummy - controlled , phase 3 clinical study of ltld used in combination with standardised radiofrequency ablation for 45 min or longer for solitary hepatocellular carcinoma . 
these radiofrequency ablation studies have shown an acceptable safety profile , but targeted ltld release using extracorporeal focused ultrasound , to our knowledge , has never been assessed in humans . 
therefore , we did a phase 1 trial to assess the safety and feasibility of targeted release and enhanced delivery of doxorubicin from thermosensitive liposomes triggered by mild hyperthermia , induced non - invasively by focused ultrasound . methods study design and participants the tardox study was a phase 1 , single - centre , open - label study , done at churchill hospital ( oxford , uk )  . 
the health research authority national research ethics service , the oxford university hospitals research 1028 vol 19 august 2018 articles see online for appendix and development department , and the uks medicines and healthcare products regulatory agency granted ethics and regulatory approvals . 
the full study protocol is available in the appendix and a detailed account of the protocol design is available elsewhere.13 patients who were considered for this study were aged 18 years or older and had pathologically confirmed incurable solid primary or secondary ( metastatic ) liver tumours , of any histological subtype , who had progressed or were stable on conventional chemotherapy . 
for inclusion , patients were required to have at least one liver tumour ( 1 cm in size ) amenable to ultrasound - guided intervention , a life expectancy of 3 months or longer , a left ventricular ejection fraction of 50% or greater , a who performance status of 1 or lower , and adequate haema tological and biochemical indices . 
patients who had received radiotherapy to the target region in the preceding 12 months or a lifetime dose of doxorubicin greater than 450 mg / m were excluded , as were patients who were pregnant or had hiv - positive status , haemochromatosis , uncontrolled diabetes , ongoing infection , advanced liver disease , or serious illnessincluding congestive heart failure , myocardial infarction , or strokewithin the previous 6 months . 
detailed inclusion and exclusion criteria are provided in the full study protocol ( appendix p 28 ) and the protocol design.13 patients were recruited from the early phase trials clinic at the churchill hospital . 
all patients gave written consent for study participation . procedures participants were assigned to one of two parts of the study , delineated by the presence ( part i ) or absence ( part ii ) of a clinically approved thermometry device temporarily implanted percutaneously in the target tumour during the intervention ( appendix p 4 )  . 
intratumoural drug concentration was estimated by use of tumour biopsies taken before drug infusion ( pre - ltld ) , after infusion ( post - ltld ) , and after ultrasound exposure ( post - ltld plus focused ultrasound ) , through the same co - axial needle used to implant the thermometry device . 
 in addition to assessing safety , feasibility , and efficacy of ultrasound - triggered targeted drug delivery , part i was also designed to capture thermometry data to help predict ultrasound parameters for part ii of the study . part ii of the study was opened subsequently and was designed to assess the feasibility and efficacy of drug delivery without invasive thermometry , to better reflect how this treatment might be ultimately implemented non - invasively in routine clinical practice . 
focused ultrasound treatment parameters were defined by a predictive model to scale the ultrasound power and duty cycle as a function of the treatment depth , to yield a temperature in the range of 39543c on the intended treatment volume . 
clinical data from both parts of the study were used in endpoint analysis , which included quantification of the delivered intratumoural dose of doxorubicin from tumour biopsies . for all study participants , before full study consent , ultrasound planning sessions were done to assess the feasibility of targeting liver lesions with ultrasound , resulting in the selection of a single target tumour for each patient for intervention . 
the treatment was received under a general anaesthetic ( with the use of high - frequency jet ventilation to reduce respiratory motion of the liver ) and involved a single 30 - min intravenous infusion of ltld ( 50 mg / m ) followed by targeted hyperthermia of the selected liver tumour by focused ultrasound . 
in the focused ultrasound treatment , a ce - marked extracorporeal high - intensity focused ultrasound device , certified for oncological treatment ( model jc200 focused ultrasound tumor therapeutic system , chongqing haifu , chongqing , china ) , operating at a frequency of 096 mhz , was used to induce highly targeted mild hyperthermia ( 395c ) within the selected liver tumours . 
for all part i and part ii interventions , the integrated diagnostic b - mode ultrasound probe of the device was used for image guidance through intercostal or subcostal windows . 
extensive preclinical validation of the clinical device for its application in volumetric hyper thermia , using the same thermometry devices that were used in this study , was done before patient inter vention ( lyon pc , unpublished )  . 
the intervention is further detailed in the appendix and protocol design.13 clinical reviews and routine blood tests were done at 2 weeks and 4 weeks post - intervention , coinciding with repeat radiological imaging ( ct and mri scans of the liver and f - fluorodeoxyglucose pet - ct scan )  . 
patients could be removed from the study according to their wishes or clinician decision , if toxic effects or adverse events were deemed unacceptable , if there were substantial protocol deviations or non - compliance , or if there were new exclusion criteria , such as pregnancy . detailed sample analysis methods are outlined in the appendix ( pp 5 , 6 )  . 
in both parts of the study , peripheral vol 19 august 2018 1029 articles blood samples were obtained pre - ltld , post - ltld , and post - ltld plus focused ultra sound for pharmacokinetic analysis , corresponding with part i biopsy timepoints . 
 plasma aliquots and weighed biopsy samples were stored at 80c until sub sequent analysis by high - performance ( hplc ) , with fluorescence liquid chrom atography detection at 480 nm excitation and 560 nm emission , to assess the total doxorubicin concentration within each biopsy and plasma sample , whether liposomal or free . 
plasma aliquots obtained at the same timepoints were also analysed on the same day by a dequenching assay , in an attempt to estimate the degree of encapsulation of doxorubicin in plasma using direct fluorometry ( appendix p 12 )  . 
therefore , for part ii of the study , the mean drug concentration of the part i post - ltld treatment biopsies was used as a comparator to evaluate the number of patients with at least a two - times increase in intra tumoural biopsy drug concentration . the focused ultrasound - targeted tumours were analysed for response by pcl or other members of the radiology team with choi criteria , response evaluation criteria in solid tumors ( recist ) , and pet response criteria in solid tumors ( percist ) , each modified for a single target , by ct , mri , and pet - ct imaging.14 , 15 , 16 additionally , target tumours were also analysed for total lesion glycolysis by pet - ct scan17 ( appendix p 6 )  . 
non - target liver tumours that had received a drug dose but no focused ultrasound exposure were also assessed in isolation in the same manner , with the same scan sequences , to provide timematched radio logical controls . outcomes the primary objective of this study was to assess the feasibility of targeted release of doxorubicin from ltld by use of mild hyperthermia generated non - invasively by focused ultrasound . 
the primary endpoint was defined as at least a doubling of the intratumoural biopsy doxorubicin concentrations , or final concentrations greater than 10 g / g , after focused ultrasound - mediated hyperthermia , in at least half of patients treated . secondary objectives were related to assessment of the safety and optimisation of the ultrasound exposure parameters for targeted liver hyperthermia and drug release . 
therefore , secondary endpoints were defined as the achievement of mild hyperthermia as monitored by the implanted thermometry device for patients in part i ; persistence of cell viability staining after focused ultrasound exposure , to indicate absence of instantaneous thermal ablation ; and adverse events occurring in the 30 days after the intervention relating to either ltld or focused ultrasound procedure , significant bone marrow suppression and liver toxicity . including clinically prespecified exploratory ( tertiary ) objectives investigated alternative methods of quantifying doxorubicin release ( as opposed to estimating intratumoural concentrations ) and the therapeutic effect of the intervention on the target tumours . 
therefore , tertiary endpoints included positive fluorescence in tumour biopsies ( which would be indicative of bioavailable doxorubicin ) , and radiological evidence of response in target tumour volumes up to 30 days after the intervention , according to recist and choi response evaluation criteria based on mri and ct scans , and suvmax using pet - ct , with each criteria modified for a single target . statistical analysis this study tested the hypothesis that higher intratumoural drug concentrations could be achieved when combining ltld with focused ultrasound - induced hyperthermia for targeted tumour delivery , compared with passive accumulation alone . 
this study did not require statistical analysis ; a doubling of total intratumoural doxorubicin concentrations ( post - ltld vs postltld plus focused ultrasound ) in at least half of the evaluable participants was required to meet the primary endpoint . 
after treatment of the first four patients in part i of the study , the trial management group did an interim analysis of the secondary endpoint relating to optimal focused ultrasound exposure parameters , in addition to the remaining secondary endpoints pertaining to safety . 
 because hyperthermia higher than the drug release threshold had been reliably attained in each target liver tumour , and no safety concerns were raised , part ii of the trial was opened in parallel to part i . 
from this point on , allocation to either part was determined on the basis of feasibility ( anatomical location of the potential target tumours ) and study team and patient preference , as detailed in the full study protocol . 
all other analyses were done at the end of the study . this study is registered withclinicaltrials.gov , number nct02181075 , and eudra - ct , number 201400051461 . role of the funding source the funders and sponsor of the study had no role in study design , data collection , data analysis , data inter pretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results of 46 patients who were screened and assessed for eligibility , ten patients satisfied the inclusion criteria and were enrolled between march 13 , 2015 , and march 27 , 2017 . 
of the excluded patients , the majority ( 19 [ 53% ] of 36 ) were excluded on the basis of anatomical location of the tumour , before part ii was open to recruitment , which offered much more flexibility in tumour location . 
there were no treatmentrelated deaths during the study . part i interventions were of long duration ( mean anaesthetic time 3692 min [ sd 384 ] ) because of time localising the target tumour spent simultaneously with diagnostic ultrasound by two different intercostal approaches and optimising the focused ultrasound parameters with thermometry feedback before drug infusion.13 the procedurally simpler part ii interventions , which did not require the insertion of an intratumoural thermometry device and real - time optimisation of focused ultrasound parameters , were expectedly of shorter duration ( mean anaesthetic time 2138 min [ sd 210 ] ) ( appendix p 3 )  . 
for focused ultrasound , we used ultrasound powers in the range of 50140 watts ( corresponding to estimated in - situ peak rarefactional pressures in the range of 5082 mpa ) and duty cycles between 30% and 100% , depending on tumour location ( appendix p 2 )  . in part i of the study ( n = 6 patients ) , the mean intratumoural biopsy doxorubicin concentration postltld plus focused ultrasound was 774 g / g ( sd 409 ) , representing an increase of 33 times compared with the mean post - ltld concentration of 234 g / g ( 093 ; table 2 , appendix pp 7 , 8 )  . 
in all cases , doxorubicin was not detected in tumour samples taken before drug infusion , while higher doxorubicin concentrations were detected in samples taken post - ltld plus focused ultrasound , compared with those of post - ltld samples ( table 2 )  . overall , the mean doxorubicin concentrations in postltld plus focused ultrasound intratumoural biopsy samples from all ten study participants was 856 g / g ( sd 569 ) an increase of 37 times compared with the 46 patients assessed for eligibility 36 patients excluded 19 unsuitable tumour location 10 progressive disease 3 recent radiotherapy to liver 3 declined to participate 1 tumour size too small 10 patients allocated and received intervention 1 patient lost to follow - up 1 patient too fatigued to attend nal follow - up visit ( week 4 ) 10 patients included in intention - to - treat analysis figure 1 : trial profile mean intratumoural biopsy concentrations in part i post - ltld samples ( table 2 , figure 2 )  . 
of the part ii patients , patient ii.03 was the only patient under the two - times increase limit required to satisfy the primary endpoint ( figure 2 )  . 
given that seven ( 70% ) of ten patients showed at least a doubling increase in intratumoural biopsy doxorubicin concentrations after focused ultrasound exposure , with concentrations from biopsies obtained in part ii compared with the mean concentration post - ltld alone from biopsies obtained in part i , our study met its primary endpoint ( table 2 )  . 
 * responses ( ratio of doxorubicin to internal standard ) were significantly lower than the response seen for the plasma lower limit of quantification ( lloq ; 01 g / ml for i.02 and 005 g / ml for i.06 ) ; the values shown are upper - bound estimates ; assuming that the response for these samples would be the same as that for the lloq , the amounts are calculated for the mass of each specific biopsy analysed . 
estimate only , because the internal standard was inadvertently omitted from this sample during processing . table 2 : high - performance liquid chromatography ( hplc ) biopsy results after analysis of chromatograms methods of analysis . 
plasma concentrations calculated with this method were similar for both methods of quantification ; however , the calculated biopsy concentrations were lower when the internal standard was excluded in calculations compared with when it was included . 
therefore , the estimated post - ltld plus focused ultrasound value for intra tumoural doxorubicin in patient i.02 is likely to represent an under estimate of the true concentration . six patients from part i , with prescribed tumour volume range of 105734 cm ( mean 496 cm [ sd 263 ] ) , and four from part ii , with prescribed tumour volume range of 307539 cm ( 438 cm [ 103 ] ) , were exposed to focused ultrasound ( overall mean tumour volume 473 cm [ 207 ] ; appendix p 2 )  . 
sustained and controlled hyperthermia ( > 395c ) was achieved in five ( 83% ) of six part i patients for a mean of 408 min ( sd 157 )  . 
in these six patients , mean intratumoural temperatures of 389415c ( overall mean 401c , sd 09 ) were recorded between 33 min and 79 min ( mean 653 min , 167 ; table 3 , figure 3 , appendix pp 911 )  . 
 in the one patient ( i.03 ) , in whom hyperthermia of 395c or higher was achieved momentarily but not sustained ( appendix p 10 ) , gas introduced around the tip of the co - axial needle on intro duction of the thermometry device ( as visualised on the ultrasound - guidance b - mode imaging system ) might have resulted in underrepresentation of the temperature in the target tumour volume . 
 cumulative equivalent minutes at 43c thermal dose analysis ( table 3 ) is discussed in the appendix p 11 . instantaneous changes consistent with tumour ablation , as is typically seen in high - intensity focused ultrasound thermal ablation , 19 were absent on the diagnostic ultra sound guidance system ( b - mode imaging ) for all inter ventions . 
this absence of thermal ablation was further supported by the day 1 mri findings , cell viability studies , and the predictive model ( gray md , unpublished data )  . 
 serious adverse events were otherwise restricted to selfresolving grade 4 neutropenia in five ( 50% ) of ten patients , an expected adverse event of ltld ( table 4 ) .11 worsening of pre - existing liver function derangements ( grade 3 or lower ) was seen in all patients , except patient i.01 , within the 30 - day follow - up period ( appendix p 3 ) , in keeping with the known adverse event profile of ltld.21 however , it was not possible to distinguish a drug - related cause of liver dysfunction from progressive liver malignancy with certainty in this patient cohort . non - invasive ultrasound - mediated hyperthermia was found to be safe , causing no skin burns , off - target tissue damage , or other clinically significant adverse events , either with or without real - time thermometry ( table 4 )  . at the 2 - week and 4 - week follow - up visits , ct , mri , and pet - ct scans were done . 
 for the remaining nine patients , targeted tumour volumes ( exposed to both ltld and focused ultrasound ) were assessed with recist , choi , and percist criteria modified for a single target tumour and compared with control liver tumours ( exposed to ltld alone )  . 
all other target tumours ( four [ 40% ] of ten ) and control tumours ( 13 [ 81% ] of 16 ) assessed showed either stable or progressive disease according to recist , choi , or percist criteria at 2 weeks or 4 weeks ( appendix pp 2025 )  . 
the four patients with a partial response according to choi criteria showed 364% , 226% , 182% , and 463% reductions in total lesion glycolysis , despite only having partial tumour coverage with focused ultrasound ( appendix p 26 )  . after counterstaining of cell nuclei with 4 ' , 6 - diamidino2 - phenylindole ( dapi ) , tumour biopsies were examined microscopically for evidence of intratumoural ltld release within 2 months of sampling ( appendix p 6 )  . 
tumour samples from patient i.01 were too auto - fluorescent for the doxorubicin signal to be distinguished from background noise in the paraffin - embedded samples , while the postltld plus focused ultrasound tissue sample from patient i.02 was contaminated with blood . 
the presence of nuclear doxorubicin showed bioavailability of intratumoural doxorubicin and thus liposomal release , because doxorubicin must be in its free form to diffuse into the tumour cells.22 in the post - ltld controls , minimal nuclear or extravascular doxorubicin was seen . plasma samples from each patient were assayed for total doxorubicin concentration by hplc . 
polynomial fit was done with least squares fit of fourth order in matlab . table 3 : summary of statistics for the post - drug thermometry analysis for all part i patients , for both raw and polynomial fitted data jc200 treatment parameters : scanning mode = linear mode at 6 mm / s ; power = 115125 w ; duty cycle = 7077% 115 w , 70% duty cycle prescribed volume 909 cm3 125 w , 77% duty cycle prescribed volume 638 cm3 ltld release threshold [ 395c ] 1.05 real - time thermometry ( post - ltld ) polynomial t ( order = 4 ) time ( min ) figure 3 : illustrative controlled hyperthermia by focused ultrasound real - time thermometry data ( trace ) captured after infusion of lyso - thermosensitive liposomal doxorubicin ( ltld ) and during focused ultrasound exposure in moving beam ( linear ) mode for patient i.05. 
from approximately 30 s to 33 min , a 909 cm prescribed target tumour volume was exposed to focused ultrasound at 115 w ( 87 mpa peak rarefactional in situ pressure ) at 70% duty cycle in linear mode . 
although the release threshold was reached within 5 min of focused ultrasound exposure , heating in the first 30 min was deemed slightly suboptimal because of prolonged cooling periods between treatment cycles . 
subsequently , by removing the outermost slices from the prescribed treatment volume , resulting in a smaller 683 cm tumour volume , and increasing power to 125 w ( 90 mpa derated ) and duty cycle to 77% , optimal hyperthermia was achieved for 3580 monce focused ultrasound stopped , the tumour was allowed to cool before the thermocouple was removed from the patient at 85 min , and a tumour biopsy sample was subsequently taken . 
the dotted curve is a fourth order polynomial fit , which is probably more representative of the bulk temperature in the prescribed tumour volume than the rapidly fluctuating point temperature recorded by the sensitive region of the intratumoural thermometry device ( trace )  . the standard curve ; therefore , subsequent plasma samples of the remaining nine patients were diluted before analysis . 
for these patients , mean total plasma doxorubicin concentrations decreased from 263 g / ml ( sd 40 ) post - ltld to 129 g / ml ( 60 ) post - ltld plus focused ultrasound . 
results of the quenched and dequenched fluorometric plasma analysis are available in the appendix ( pp 12 , 13 )  . discussion to our knowledge , our study was the first to attempt noninvasive ultrasound - mediated targeted hyperthermia for vol 19 august 2018 1035 articles grade 1 - 2 grade 3 grade 4 definitely or probably related to ltld : haematological toxic effects neutropenia or neutrophils decreased anaemia urinary tract infection 1 ( 10% ) 1 ( 10% ) 5 ( 50% ) * 1 ( 10% ) definitely or probably related to ltld : non - haematological toxic effects definitely or probably related to the procedure alopecia candida infection fatigue or lethargy nausea vomiting abdominal pain back pain decreased appetite dysphonia erythema fatigue hepatic pain musculoskeletal chest pain musculoskeletal pain or discomfort nausea pain in extremity skin discolouration abdominal pain confusion state constipation decreased appetite fatigue joint swelling malaise nausea peripheral swelling respiratory tract infection vomiting 8 ( 80% ) 1 ( 10% ) 4 ( 40% ) 2 ( 20% ) 2 ( 20% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 2 ( 20% ) 6 ( 60% ) 1 ( 10% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) * 1 ( 10% ) 2 ( 20% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) definitely or probably unrelated or possibly related to ltld or procedure ( indeterminate cause ) no grade 5 adverse events occurred . 
 mean temperatures needed for drug release were safely maintained in clinically relevant tumour volumes by extracorporeal focused ultrasound , for about 1 h , without subsequent radiological or histological evidence of thermal ablation . 
this approach resulted in a substantial increase in the total intratumoural biopsy concentration of doxorubicin , compared with that achieved by passive accumulation alone , with seven of ten patients having at least a doubling and an increase of up to ten times in intratumoural doxorubicin concentrations . 
this increase occurred concurrently with the presence of nuclear doxorubicin , showing liposomal release after focused ultrasound exposure , and localised radiological responses in the target tumour regions exposed to focused ultrasound in several patients . 
overall , these findings suggest that target drug delivery to solid tumours triggered noninvasively by therapeutic ultrasound is clinically safe , feasible , and potentially effective . the non - thermosensitive liposomal formulation of doxorubicin , ntld , is hypothesised to exert its therapeutic effect predominantly by the enhanced permeability and retention effect.23 by contrast , the ltld formulation that we used in this trial is understood to act by rapid diffusion of doxorubicin into the tumour interstitium under conditions of mild hyperthermia , with only a small pro portion of doxorubicin entering the tumour by enhanced permeability and retention . 
these intended delivery mechanisms are reflected in the circulation profiles of the two formulations , with ntld having a half - life of more than 10 h while ltld has a shorter halflife of about 1 h.9 , 10 , 24 , 25 mild hyperthermia has been shown to enhance the perfusion and increase the permeability of tumour vasculature.26 because focused ultrasound exposure begins while blood concentrations of ltld are at their peak11 , 13 ( figure 2 ) and at a timepoint before any substantial enhanced permeability and retention - assisted accumulation could have occurred , it is our understanding that the majority of the intratumoural doxorubicin is released from circulating ltld in the tumour microvasculature , when the tumour reaches the liposomal transition temperature ( 395c )  . 
free ( bio - available ) circulating doxorubicin might then rapidly diffuse into the adjacent or downstream perivascular space , and on to tumour cells at therapeutic concentrations and penetration depths due to a steep concentration gradient , surpassing what could be achieved through passive circulation alone . the post - ltld intratumoural biopsy concentrations of doxorubicin ( after infusion ) were similar to those seen in preclinical tumour models of ltld.5 differences in the measured total doxorubicin concentrations before focused ultrasound exposure were very small across patients . 
in keeping with preclinical studies , 5 , 7 this result strongly suggests that there is little opportunity for passive accumulation of ltld in the first 2 h after administration , but there could still be differences in the leakiness of tumour vascular pores across the different tumour subtypes treated.27 the much greater differences in total doxorubicin concentration observed after focused ultrasound exposure are probably due to a combination of factors , including the differences in tumour leakiness across subtypes , tumour heterogeneity , the percentage of 1036 vol 19 august 2018 articles the ultrasonically treated volume that was adequately vascularised , and the total duration of focused ultrasoundmediated hyperthermia relative to the patient - specific pharmacokinetics of ltld . 
despite the use of a different analytical technique , pharmacokinetic profiles for total doxorubicin were similar to previously published clinical data , 11 in which the same dose of ltld was combined with radiofrequency ablation of liver tumours . magnetic resonance spectroscopy , particularly chemical exchange saturation transfer , was explored as a method of quantifying free doxorubicin preclinically , using phantom and small animal studies ( unpublished )  . 
 in this early study , it remains unclear whether ultrasoundmediated cavitation is involved in the mechanism of delivery , but preclinical data strongly suggest that the microstreaming and shockwaves created by cavitation can be a benefit to the delivery of cancer drugs.29 , 30 although our phase 1 study was , to the best of our knowledge , the first to translate focused ultrasoundtriggered targeted drug delivery to a clinical oncology setting , the study design had inherent limitations . 
first , the prescribed tumour treatment volumes were constrained by the presence of ribs in the acoustic field treatment ( which restricted monitoring and guidance and reduced the focused ultrasound beam intensity ) and by the focused ultrasound system itself ( with restricted scanning capabilities and a nominally small , fixed ultrasonic focus ) , such that , the real - time b - mode typically , only partial sonication of larger tumours could be achieved , usually including tumour borders closest to the ultrasound source . 
custom focused ultrasound devices designed for volumetric hyperthermiafor example , devices using less tightly focused transducers or multi - element systems with beam steering8might allow rapid induction of large volume hyperthermia , facilitating the treatment of larger tumour volumes with this strategy . second , tumours are highly heterogeneous and show great microregional variations , not least in the amount of vascularity and necrosis.31 in this study design , tumour biopsies were intended to provide an estimate of the mean intratumoural drug concentration in the focused ultrasound - exposed tumour volume . 
this design limitation is mitigated , to some extent , by subsequent radiological analysis of the targeted tumours , most crucially by pet - ct scan , a technique that can discriminate metabolically active from necrotic or chemoablated tumours . third , the study design did not include time - matched control biopsies from liver tumours receiving ltld alone , because doing more than three sequential tissue biopsies in more than one location in any one patient was neither ethical nor practical.13 preclinical studies of ltld showed that , in great part because of its short half - life ( 1 h compared with more than 10 h for ntld ) , the additional intratumoural accumulation beyond 30 min after administration is not substantial , and falls well short of the doubling increase in intratumoural concentration that constituted the primary endpoint of our study.6 , 8 radiological follow - up enabled indirect assessment of negligible longer - term passive accumulation of ltld . fourth , although the hplc tumour results were generated by a validated method , worst - case estimations were done in three cases . 
however , since these estimates were worst - case estimates , we are confident that the primary endpoint is not compromised . a fifth limitation was that the introduction of any instrumentation into the target tumour risked contamination of tumour samples with blood products . 
the postltld sample for patient i.04 and the post - ltld plus focused ultrasound sample for patient i.02 were both shown to contain blood contamination on haemotoxylin and eosin staining . 
nevertheless , should be exclusion of these two results from the overall analysis does not alter the outcome of the study , because seven of eight patients still had an increase greater than doubling in drug concentrations and the study still met its primary endpoint . vol 19 august 2018 1037 articles thermography and coregistration with lastly , a magnetic resonance spectroscopy - guided focused ultrasound system would have provided valuable spatial the follow - up mri , facilitating both treatment and response assessment . 
however , the ultrasound - guided focused ultrasound device used made practical issues surrounding the use of high - frequency jet ventilation anaesthesia and the biopsy procedure less challenging because of the absence of a magnetic field . by design , part ii of the study proceeded without invasive thermometry , and this was shown to not adversely affect the efficacy of the intervention ; indeed , the mean post - ltld plus focused ultrasound intratumoural concen tration of doxorubin in part ii was 980 ug / g , compared with 774 ug / g in part i . whether delivering small molecules , antibodies , or viruses , maximising the dose delivered to a tumour while minimising off - target toxicity represents a universal challenge in oncology.32 a major limitation of systemically administered liposomal agents is their low therapeutic index : the dose required to produce a successful antitumour effect is toxic to normal tissues . 
device - targeted drug delivery has undergone decades of preclinical development but could be nearing clinical adoption as a generic tool for overcoming the challenges of delivering existing and emerging therapeutics to solid tumours . 
 mri - based or ultrasound - based treatment monitoring strategiesor detailed predictive treatment planning , as was used in this studyare likely to facilitate clinical adoption for non - invasive targeting . 
preclinical mri studies33 , 34 have combined three - dimensional thermography with sophisticated closed - loop feedback algorithms at high temporal resolutions to reduce microregional temperature fluctuations , and a clinical study involving the use of magnetic resonance - guided high intensity focused ultrasound with ltld is underway for treatment of paediatric solid tumours ( nct02536183 )  . 
by using an ultrasound - guided focused ultrasound device without thermography , our study explored the economically attractive and more easily scalable alternative than mrguided techniques for attaining large - volume bulk hyperthermia with predictive models , with less emphasis on maintaining tight and homogeneous temperature control . overall , this prospective study shows for the first time in a clinical setting the safety , feasibility , and potential for therapeutic benefit of ultrasound - triggered release of ltld in otherwise chemorefractory tumours . 
the small sample size of ten patients reflects that this trial was a proof - of - concept study , for which participation was predominately altruistic , involving only a single cycle of chemotherapy and targeting of a single tumour . 
a demonstrable radiological response in the targeted tumour volume alone is encouraging , given that doxorubicin has been previously shown to have reduced therapeutic value in many of these tumour subtypes.21 , 35 despite its limitations , our study shows for the first time in a clinical setting that it is feasible to safely trigger and enhance intratumoural delivery of a chemotherapeutic agent to a precise anatomical location at depth , by using focused ultrasound applied noninvasively . 
further preclinical and clinical research in focused ultrasound - mediated drug delivery might be warranted , with the intention of reducing toxicity and improving therapeutic outcomes in a broad range of solid tumours , potentially across multiple drug classes . contributors ccc , pcl , rc , mrm , and fvg designed the study and wrote the protocol . 
pcl and ccc wrote the manuscript , and all authors reviewed , commented on , and approved the paper . declaration of interests no author has direct or indirect financial interest in either the clinical device used for the study ( jc200 , chongqing haifu , chongqing , china ) or the drug ( thermodox , celsion corporation , lawrenceville , nj , usa ) used in the study . 
fw does not receive royalties for the manufacture , sale , upkeep , or maintenance of the device used for treatment despite being involved in the original team that filed patents related to the device . 
ccc and rc are founders , shareholders , and consultants for a spinout company from the university of oxford ( oxford , uk ) , oxsonics , specialising in ultrasound - enhanced drug delivery to tumours . 
mrm reports personal fees from amgen , valo therapeutics , and bioline ; grants and personal fees from roche and gsk ; grants from astrazeneca ; personal fees and trial - related payments to institutions from novartis , eisai , rigontec , array biopharma , and bms ; trial - related payments to institutions from astellas , millennium , vertex , regeneron , tcbiopharma , replimune , and pfizer ; non - financial support and trial - related payments to institutions from immunocore ; and personal fees , non - financial support , and trial - related payments to institutions from merck , outside the submitted work . 
all other authors declare no competing interests . acknowledgments the trial was funded by the uks national institute for health research , oxford biomedical research centre , and the research was supported by the oxford centre for drug delivery devices under a programme grant ( ep / l024012 / 1 ) from the engineering and physical sciences research council . 
the views expressed are those of the authors and not necessarily those of the nhs , the nihr , or the department of health . corrections correction to lancet oncol 2016 ; 17 : 429 therapy cristofanilli m , turner nc , bondarenko i , et al . 
fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment o f h o r m o n e r e c e p t o r p o s i t i v e , her2 - negative metastatic breast cancer that progressed on previous endocrine ( paloma - 3 ) : final analysis of the multicentre , double - blind , phase 3 randomised controlled trial . 
lancet oncol 2016 ; 17 : 42539in this article , in the outcomes subsection of the methods , the second sentence should read secondary efficacy endpoints were con rmed objective response , which was defined as complete response or partial response according to recist ; clinical benefit , which was defined as complete response or partial response or stable disease of 24 weeks duration or longer ; tumour tissue biomarkers , including genes ( eg , pik3ca mutations ) , proteins ( eg , quantitiative expression of oestrogen and progesterone receptors ) , and rna expression ; and safety including type , incidence , and severity of adverse events . 
 this correction has been made to the online version as of march 29 , 2016 , and the printed version is correct . vol 17 april 2016 e136 correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
 this correction has been made to the online version as of jan 31 , 2018 . vol 19 february 2018 corrections for more on the study of skin cancer apps see birmingham.ac.uk / news / latest / 2018 / 07 / skin - cancerphone - apps - research.aspx for more on the apple watch emoji study see proc am soc clin oncol 2018 ; 36 ( suppl ) : abstr 6501 digital oncology apps : revolution or evolution ? the uks recent spell of hot and sunny weather serves as a reminder of the need to be cognisant of the association between increased sun exposure and heightened skin cancer risk . 
in a timely study presented at the british association of dermatologists 98th annual meeting ( july 35 , 2018 ; edinburgh , uk ) , researchers evaluated the increasing number of new digital apps to aid in skin cancer diagnosis that are entering the digital oncology market . 
 could such technologies revolutionise the detection and treatment of this disease ? and how much do theyand the rapidly emerging digital health market as a whole add to existing standards of care ? early diagnosis is key in determining outcomes from skin cancer : 5 - year rates can be high with early diagnosis , but as low as 10% if diagnosed at an advanced stage . 
although theoretically these apps could potentially increase selfawareness of skin changes and improve cancer detection rates , the study presented in edinburgh found that some apps were more successful than others at identifying both malignant and benign moles and lesions , with many unable to detect rare or unusual skin cancers . 
 the researchers found that flaws in the computing algorithms and technology and little medical specialist input during development mean that the apps cannot identify suspicious lesions as accurately as a dermatologist could . 
 the range in quality and accuracy of skin cancer detection apps is often a result of hasty development and a lack of high - level evidence from properly conducted trials to show how effectively they work compared with the current standard of care . 
consequently , with the goal of delivering a working product quickly to make money back from the initial investment , the development process can be rushed , without sufficient input from medical experts or rigorous testing . moreover , although these new technologies initially look exciting , careful consideration is needed when comparing them to standard health - care practices . 
 how much clinical value do they truly add ? educational health apps might help to increase awareness about some health conditions , and a recently reported study showed that patients with cancer using an apple watch and emojis to record their quality of life symptoms could be a promising new way to record and track patientreported outcomes . 
indeed , the most successful skin cancer apps are those that involve sending an image directly to a dermatologist for review , showing that medical specialists are still needed to obtain an accurate diagnosis . 
the algorithms on which the technologies are based must undergo thorough peer review and the data ought to be made available in the public doma additionally , digital oncology reporting guidelines should be created , similar to those that already exist for drug trials . 
robust randomised controlled trials comparing these new methods with existing standards of care and head - tohead comparisons of different technologies are needed to provide solid evidence about which ones work and which do not . 
we must not fall into the same commercial traps with digital health technologies as we already have with the pharmaceutical industry in which trials directly comparing competing agents for the same indication are scarce . 
without solid evidence from proper trials to prove the effectiveness of digital health technologies , there is a real danger of compromising public and patient safety , especially when products like the skin cancer apps make bold claims about their ability to detect cancer . 
 as we enter this new world of digital health , we must not allow ourselves to be dazzled by the exciting technologies suddenly on offer and their role in health care needs careful consideration . 
this is a new field , and it needs close scrutiny to ensure that it is appropriate for the health sector , is cost - effective , and , above all , does not compromise patient safety . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections published online may 9 , 2018 s1470 - 2045 ( 18 ) 30289 - 4 see articles page 785 genetic predisposition to medulloblastomas : just follow the tumour genome for a the actual contribution of germline mutations to paediatric cancers has been a major concern for paediatricians , basic researchers , geneticists , epidemiologists , and parents long time . 
 the first notable piece of work1 in this field was produced by researchers from the st jude research hospital the number of germline variants in known cancer genes , assessed using constitutional dna from more than 1000 paediatric patients . 
first , by use of the largest retrospective cohort constituted and validating it on prospectively collected dnas , it aimed to unbiasedly assess the actual incidence of cancer predisposition syndromes in patients with medulloblastoma . 
the authors identified six genes with a significant excess of damaging germline mutations for patients with medulloblastoma : apc , brca2 , palb2 , ptch1 , sufu , and tp53 . 
this study confirms the high prevalence of sufu and ptch1 mutations in infants with shh medulloblastomas , 3 , 4 and also substantiates the overall higher risk for tp53 or ptch1 germline mutations in shh medulloblastomas , whatever the age at onset.5 however , it also highlights that a familial history of cancer is often absent in these cases of shh medulloblastoma . 
 the study shows for the first time the phenotype of the rare ( seven [ 1% ] of 1022 patients ) germline apcrelated medulloblastomas ( five of whom were children in the wnt subgroup who had excellent overall survival of 100% at 36 months ) which , by contrast with shh medulloblastomas , usually occur in a clear familial context , emphasising the need for a careful interview regarding familial history in children with wnt medulloblastomas . 
 the second main finding was the refinement of the potential role of brca2 and palb2 germline mutations in medulloblastoma , so far known only in the context of fanconi anaemia.6 , 7 germline heterozygous brca2 ( seven [ 1% ] of 1022 patients ) and palb2 ( five [ < 1% ] of 1022 ) variants might also be associated with an increased risk of medulloblastoma in childhood . 
the presence of loss of heterozygosity of the wildtype brca2 and palb2 allele in some tumours or the tendency of corresponding tumours to present some signs of homologous recombination repair deficiency ( hrd ) might suggest pathogenicity . 
international collaboration to collect data from more families with brca2 and palb2 mutations with precise evaluation of the frequency of medulloblastomas might help to decipher the actual involvement of these heterozygous mutations in predisposition to medulloblastoma . 
 because chromothripsis medulloblastoma indicates the presence of tp53 mutations and can subsequently induce familial screening , 4 finding insights for hrd and brca2 and palb2 mutations in a child with medulloblastoma might eventually cause the initiation of tumour screening in the relatives . 
since early cancer detection in unaffected individuals is one major goal of genetic counselling , possible familial consequences of broad genetic analyses on tumour dna will need to be explicitly anticipated with parents ; moreover , the medical benefit and psychological effects of such findings on families with no cancer history should be prospectively evaluated . finally , the study does not identify any specific predisposing genes for group 3 and group 4 medulloblastomas , which shows that a young age at cancer 722 vol 19 june 2018 comment onset ( group 3 ) might not indicate a strong probability of predisposing syndrome per se . 
moreover , although many studies have investigated this class of high - penetrance predisposition genes , lowthe penetrance , high - frequency alleles remains unknown and still needs to be investigated through genome - wide association studies for medulloblastoma . 
the study highlights the major interest of somatic molecular criteria , in addition to family history and potential malformative syndrome , to suggest genetic predisposition and hence lead to genetic counselling and germline genetic assessment with a clear prioritisation scheme depending on the type of medulloblastoma . * franck bourdeaut , olivier delattre siredo pediatric cancer center , inserm u830 , institut curie , paris 75005 , france franck.bourdeaut@curie.fr we declare no competing interests . copyright the author ( s )  . 
blood 2004 ; 103 : 255459 . targeting the tumour vasculature in mesothelioma in 2018 , malignant mesothelioma remains a rapidly lethal cancer for which there is no standard second - line therapy . 
the disease represents both an opportunity for drug development and a substantial challenge , as evidenced by recent negative , yet appropriately controlled and powered , phase 3 trials.1 , 2 inter - patient heterogeneity , coupled with an absence of personalised strategies , account for these previous failures , highlighting an unmet need . 
these include the identification of the ezh2 subunit of polycomb in bap1 - mutated repressor complex 2 as a target mesothelioma , which is being explored in a proof - ofconcept phase 2 study ( nct02860286 ) .3 pegylated arginine deiminase has shown efficacy in mesotheliomas that do not express argino succinate synthetase , and a combination strategy is being investigated in the phase 3 atomic trial ( nct02709512 )  . 
checkpoint inhibition shows activity in the context of programmed cell death ligand 1 ( pdl - 1 ) expression ; 4 however , the jury is still out regarding the significance of this potential biomarker for patient selection in treating mesothelioma . 
 in the lancet oncology , vanesa gregorc and colleagues5 report the results of their phase 3 ngr015 trial , in which they tested a novel vascular disrupting agent ( ngr - htnf ) in an unselected population of patients . 
at picomolar concentrations , the endothelial barrier function of the neovasculature impaired , enhancing chemotherapy penetration in murine models.6 in a previous phase 2 trial , 7 ngrhtnf monotherapy showed an arguably modest disease control with 44% of patients achieving disease control , with evidence of partial response ( albeit 2% ) , and a median of 28 months progression - free survival . 
 published online may 9 , 2018 s1470 - 2045 ( 18 ) 30248 - 1 see articles page 799 vol 19 june 2018 comment published online september 12 , 2018 s1470 - 2045 ( 18 ) 30563 - 1 see articles page 1289 cancer trends and disparities in india : data needs for providing equitable cancer care india , with a population close to 13 billion , and growing , is epidemiologically interesting and chal len ging for health - care planners . 
regarding cancer burden , the population demographics , health policies , health - data recording , access to health care , and affordability have all improved substantially during the period between 1990 and 2016 , as reported by the india state - level disease burden initiative cancer collaborators in their global burden of disease paper in the lancet oncology.1 in addition to the heterogeneity in cancer incidence and outcomes between states , significant differences exist within each state , most prominently between urban and rural populations . 
health data availability , access to health care , and affordability are poor and have remained almost static over the entire period in rural areas , while they have improved substantially in urban areas . 
the federal government of india is currently rolling out in a phased manner the national health protection scheme ( nhps , also known as modicare ) .2 if properly implemented , this programme is likely to improve health - care access for the majority of the rural indian population in the next decade . the india state - level disease burden initiative cancer collaborators have used the best possible data - sourcing methods available so far for india . 
the first populationbased cancer registry , based in mumbai ( previously named bombay ) , started in june 1963 , and the first rural population - based cancer registry , based in barshi , in 1987 . 
cancer data maharashtra , was established collection has improved over the years and the indian council of medical research ( icmr ) now has a fully fledged national centre for disease informatics and research ( ncdir )  . 
the federal government of india has made it mandatory for all citizens to possess a unique national identification number ( aadhaar act 2016 ) 3 that currently linked to all financial transactions . 
this number will eventually also be linked to all social security benefits , including modicare , making it an excellent database for future health - services planning in the country . it is heartening to note that the age - standardised incidence of the most common cancers ( except breast cancer ) has remained static over the past two and half decades , despite the assumption of under - reporting in the earlier part of this period . 
the incidence of cancer ( except for cervical cancer , and except for the north - eastern state of mizoram ) is much lower than that in countries that can be said to be in a similar epidemiological transition as india ( brcsbrazil , russia , china , and south africa ) , and substantially lower than in some developed countries with established prevention , screening , and early detection programmes.4 however , the increased incidence of breast cancer in india is worrying and requires serious attention . 
in this context , a comparison between urban and rural populations within states would have been interesting . the federal government of india has taken important towards controlling cancer and policy decisions other non - communicable diseaseseg , cotpa 2003 ( cigarettes and other tobacco products [ prohibition of advertisement and regulation of trade and commerce , production , supply and distribution ] act ) ; 5 however , except for a few successful smokefree city programmes , and graphic package warnings , mechanisms to enforce the act are scarce since enforcement is the responsibility of each state . 
 just like tobacco use in india and most of south asia is different from the rest of the world , mainly due to the high prevalence of smokeless tobacco use , alcohol use ( patterns and disease causation ) are also worthy large proportion of the alcohol consumed by poor people in india is spuriously manufactured , and contaminated with various industrial chemicals . 
 countrywide epidemiological studiesa india has also embarked upon a population - based screening programme for cervical cancer , breast cancer , 1260 vol 19 october 2018 comment and oral cancer . 
however , the techniques chosen for these screening programmes are not optimal ; although there is evidence for visual inspection with acetic acid for cervical cancer , it might be useful to switch to hpv screening as soon as it becomes financially feasible , and evidence for implemented clinical breast examination schedules for breast cancer and oral examinations for oral cancer is weak . 
population - based screening for breast cancer starting at age 35 years will probably be a logistical nightmare , waste of resources , and even cause outright harm to patients . 
 surendra s shastri department of health disparities research , university of texas md anderson cancer center , houston , tx 77030 - 3906 , usa ssshastri@mdanderson.org i declare no competing interests . copyright the author ( s )  . 
 ( accessed aug 9 , 2018 )  . maternal hormonal contraception and childhood leukaemia the treatment of childhood leukaemias has improved in recent years because of additional knowledge of acute leukaemia genetic subtypes , pathogenesis mechanisms , prognosis prediction , and targeted therapies . 
the natural history of this disorder is determined by several interacting factors , including exposure to risk factors , susceptibility , and cell biology orig therefore , data generated by population - based registries are research , health - care indispensable planning , and treatment of childhood leukaemias . 
 for aetiology in the lancet oncology , marie hargreave and colleagues1 present a cohort study that adds value to the set of observational epidemiological data about the impact of maternal use of oestrogenprogesterone contraception on the risk of childhood leukaemia in offspring . 
this nationwide , population - based study shows that maternal hormonal contraceptive use is associated with an increased risk of childhood leukaemia in the offspring ( hazard ratio [ hr ] for recent use of hormonal contraception vs no use 146 , 95% ci 109196 ; p = 0011 ) , particularly of the non - lymphoid leukaemia subtype ( 217 , 122387 ; p = 0008 )  . 
the cohort used in the study has robust statistical value given the well documented population - based dataset and participant linkage in danish registries.2 the findings reported by hargreave and colleagues add oral contraception to the list of established risk factors for childhood leukaemia ( ie , tobacco , pesticides , infectious agents ) and , although the authors highlight this minimal risk in their conclusions , some children may be particularly vulnerable to this new risk factor.3 the design of this nationwide , population - based registry study avoids the recall or selection biases often found in case - control studies . 
it also provides information about molecular profiles of the genetic subtypes of acute lymphoblastic leukaemia , and also about distinct cell subtypes of childhood leukaemia , recurrent genetic abnormalities , and age strata , 3 , 4 enabling sensitivity analyses and stratified analyses according to these factors . 
consequently , the authors are able to report data for the different risk associations for molecularly defined subtypes of acute lymphoblastic leukaemia and acute myeloid leukaemia and for childrens age at diagnosis . 
remarkably , maternal exposure to oestrogen and progestins in combined hormonal contraceptives is associated with a higher risk of acute myeloid leukaemia than of acute lymphoblastic leukaemia ( hrs associated with recent use were 224 leukaemia [ 95% ci 112448 ] for acute leukaemia )  . 
 vs 125 [ 089178 ] for acute myeloid lymphoid published online september 6 , 2018 s1470 - 2045 ( 18 ) 30509 - 6 see articles page 1307 vol 19 october 2018 1261 comment editorial for the macmillan uk report see documents / aboutus / research / richpictures / update / rp - peoplewith - cancer.pdf for the report on use of emergency departments by patients with cancer see j clin oncol 2014 ; published online december 22 . 
furthermore , a report released earlier this month by macmillan uk suggested that there will be 25 million people living with cancer in 2015 and an increasing number of these will be over the age of 65 years . 
moreover , a quarter of people in the uk face poor health or disability after cancer treatment , leaving them dependent on health services for a long period of time after discharge from their specialist . 
furthermore , the new nhs 111 patient hotline , sta ed by medically untrained call - handlers , is directing more patients than its predecessor , nhs direct , to a&e departments . 
the needs of cancer survivorseg , mental health , pain management , and other incapacitating long - term sequelaeare not trivial , and the level of care o ered by an a&e department is unlikely to re ect the more specialised needs of these patients . 
an extended and better integrated health - care network is needed , at the heart of which lies the general practitioner ( gp ) working seamlessly with secondary care , while also o ering greater access via longer practice opening hours , including at the weekend . community support , including home - based care is another key element for e ective management of patients living with cancer . 
for example , a recent study showed that , in ve countries , patients with cancer receiving palliative care ( including home - based care ) were less likely to attend an emergency department compared with those patients not in receipt of dedicated long - term care . 
insu cient home - based care has resulted in an overwhelming number of delayed dischargesie , patients who are medically t to go home remaining in hospital because of an absence of a continued care plan . 
furthermore , hospitals have been forced to reduce the number of available beds , and indeed close whole wards , owing to nancial pressures , including the burden of debts from private nance initiatives . 
collectively , these circumstances cause bottlenecks in the nhs , including overburdening of a&e departments . although laudable that the present uk government has promised an injection of an additional 300 million to the nhs to fund anticipated increased seasonal demand for a&e services , these funds will probably be spent on expensive short - term solutions , such as the hiring of locum doctors or other agency sta  . 
long - term , more sustainable solutions increased recruitment and are needed , retention of full - time a&e doctors and other healthcare professionals , as well as improved upstream and downstream management of potential patients . including for just reserved emergency care , provided by hospital a&e departments , should be that purposeurgent life - threatening conditions needing immediate hospital treatment . 
preventing the use of a&e departments as a stop - gap solution for the management of a growing population of patients with chronic disease such as cancer needs to be a key objective of the next uk government after the general election in may . 
 the lancet oncology vol 16 february 2015 published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
 this correction has been made to the online version as of jan 31 , 2018 . vol 19 february 2018 corrections minimalism in oncology expenses related to cancer treatment can diminish patients quality of life and impede delivery of highquality care . 
thus , it is worrying that , in 2017 , a study showed the price of some common cancer drugs in the usa rose at a rate higher than inflation . 
the us senate has recently started investigating why a 40 - year - old cancer druglomustine , which has no generic competition has increased in price by 1400% since 2013 . 
at the 23rd annual conference of the national comprehensive cancer network ( orlando , fl , usa , march 2224 , 2018 ) , oncologists had a heated debate about the congressional mandate that prohibits the centers for medicaid and medicare services from negotiating drug prices with in the usa . 
although pharmaceutical companies governmental action is needed to regulate the unit price at which cancer drugs are marketed , could the medical oncology community further help alleviate the financial burden placed on patients by rethinking the way oncology is practiced ? optimising treatment dose could be central to the financial toxicity debate . 
for example , a recent trial of abiraterone showed the concentration of drug that enters the bloodstream can be increased by four times if the drug is swallowed with a low - fat meal rather than on an empty stomach . 
this study supports anecdotal evidence that many oncology drugs could be taken at lower doses or for shorter periods without reducing effectiveness , alleviating both physical and financial toxicity to patients . 
another example of successful dose reduction is immunisation against the hpv serotypes 16 and 18 , for which two vaccine doses provide similar protection to the initially recommended three - dose schedule . 
 the condition of life - threatening cancer has traditionally meant that high drug doses , and thereby high toxicity , have generally been considered acceptable if a treatment is effective . 
the presumed understanding that high dose translates into higher anti - tumour activity still drives clinical trial design , with maximumtolerated doses ( mtd ; the highest dose of a treatment that does not cause unacceptable side effects ) being established as the recommended dose for most new oncology drugs . 
although fine - tuning a personalised dose for each patient is neither feasible nor plausible the optimal dose is just an estimation for a particular patient , and optimisation strategies could substantially delay the market entry of new drugsrethinking drug development to aim for a minimum - effective dose ( med ; lowest dose of treatment that provides a clinically meaningful response ) could be a sensible approach to find the balance between oncological effectiveness , and physical and financial toxicity . 
furthermore , in the era of targeted therapies , which differ from cytotoxic chemotherapies in that they follow a non - linear doseresponse saturation curve whereby the addition of more drug does not always improve outcomes , should the way that safety is assessed move away from the traditional pharmacology - driven study designs ? a 2010 pooled analysis of trials of targeted therapy showed that patients treated with low doses ( 25% mtd ) had similar outcomes to those treated with intermediate ( 2575% mtd ) and high doses ( 75% mtd ) in terms of survival , objective responses , and toxicity . 
 additionally , adaptive studies in oncology , such as the keynote - 001 trial ( which led to the accelerated approval of pembrolizumab , following a customised trial design in which no mtd was reached and the recommended phase 2 dose was based on early safety and response assessments that led to the recruitment of several expansion cohorts ) , could serve as a precedent for future oncology trials . 
adopting the minimum - effective dose as a recommended standard and customising trial design , aided by mathematical modelling and simulations for optimal dosage , suggest a new path towards practising minimalism in oncology that could avoid unnecessary financial and physical toxicity and improve patients quality of life . the value in cancer care consortiumwhich plans to initiate trials that explore whether the dose , duration , or type of drug can be optimisedis a first , promising step to tackle financial toxicity . 
 the lancet oncology for more on the study about cancer drug costs increase after launch in the usa see j clin oncol 2018 ; 36 : 31925 for more on the us senators investigation see com / policy / healthcare / 381287senators - launch - probe - intowhy - price - of - cancer - drugincreased - 1400 - percent for more on the debate at the nccn 23rd annual conference see viewarticle / 894498 for the trial on low - dose abiraterone with food see j clin oncol 2018 ; published online march 28 . 
elsewhere , non - clinical grade materials continue to be used in breast implants , despite the 2010 pip scandal in which implants were found to be manufactured with unapproved silicone gel and were prone to rupture . 
although reports have now emerged of an alarming association between textured breast implants and the development of breast large - cell implant - associated anaplastic lymphomaa rare form of t - cell lymphoma that can occur in the fibrous scar capsule that forms around breast the underlying causal mechanisms have yet to be defined , early detection of localised disease and complete removal of the implant and capsule can lead to recovery . 
meanwhile , cases of breast implant - associated anaplastic large - cell lymphoma are increasing : 615 cases have been reported worldwide since the first report in 1997 , including 45 cases in the uk , 72 in australia , and 252 in the usa . 
the concern is so great that the french national agency for medicines and health products has recommended that surgeons switch to smooth implants as the link between textured implants and anaplastic large - cell lymphoma is investigated . for any woman undergoing mastectomy to treat breast cancer , the possibility of developing another cancer because of a medical device must be devastating . 
but , as for any medical procedure , blame cannot , and should not , be apportioned to the patient , especially when risks are not adequately recorded and reported , let alone communicated to the patient . 
data for anaplastic largecell lymphoma are scarce , highlighting a wider concern about the worldwide regulation of medical devices . many countries have systems in places for reporting adverse events associated with medical devices . 
however , such systems do not appear to be compulsoryfor example , the uk registry is not mandatory for clinicians and although large - cell lymphoma as a data item , reporting cases is optional . 
how can clinicians be expected to communicate risks to patients or make clinical decisions without accurate and reliable data ? the existing system of passive monitoring of medical device safety clearly needs to be addressed . include anaplastic it does drug safety monitoring could be a good model for the medical device industry and provide more reassurance to doctors and patients alike . 
reporting of clinical trial data on new drugs has improved , and data from robust trials , including full reporting of adverse events , are essential for any drug approval . 
the same stringent data are not needed for medical devices ; for example , in the european economic area , market approval is granted through ce certification , for which clinical trial data are not mandatory . 
similarly , a new eu regulation on medical devices , due to come into force in 2020 , includes key issues of transparency around medical devices and reinforcement of rules of clinical evidence . the steps taken by the fda and the eu are a good start in a long overdue assessment of medical devices , which undoubtedly hold much promise for many patients . 
 the lancet oncology for the implant files see investigations / implant - files / for safety concerns of breast implants see theguardian.com / society / 2018 / nov / 26 / breast - implants - studyreveals - serious - safety - concerns for more on the pip scandal see pip - implants / for reports on breast implantassociated anaplastic large cell lymphoma see theguardian.com / society / 2018 / nov / 26 / rare - cancer - linkedbreast - implant - used - bymillions - women - lymphoma for the maude database see scripts / cdrh / cfdocs / cfmaude / search.cfm for the australian registry see for the uk registry see information / clinical - audits - andregistries / breast - and - cosmetic - implantregistry for the us action plan see centersoffices / officeofmedical productsandtobacco / cdrh / cdrhreports / ucm604500.htm for the eu regulation see sectors / medical - devices / regulatory - framework_en vol 20 january 2019 editorial published online february 20 , 2019 s1470 - 2045 ( 18 ) 30941 - 0 see articles page 531 sartore - bianchi a , trusolino l , martino c , et al . 
dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - of - concept , multicentre , open - label , phase 2 trial . 
several improved outcomes in childhood cancer have led to an increased focus on the cost of long - term survival : longterm physical , psychological , and financial morbidities that arise as a consequence of cancer therapy or the cancer landmark childhood cancer survivor cohorts have informed our ability to describe , predict , and minimise these late effects.1 , 2 about 80% of adolescents and young adults ( ayas ) with cancer will also achieve long - term cure.3 consequently , late effects are also highly relevant to this population , but very few aya - specific data exist , forcing clinicians to extrapolate from the literature on childhood cancer survivors . 
previous work has shown that survivors of aya cancer have a higher absolute risk of subsequent primary neoplasms than do younger or older populations , which in turn has a substantial impact on overall survival.4 , 5 cohort of more in the lancet oncology , chloe bright and colleagues6 describe the risk of subsequent primary neoplasms than in a population - based 200 000 survivors of aya cancer . 
the large sample size and more than 26 million person - years of follow - up allow the investigators to describe , comprehensively for the first time and in great detail , the risk of specific subsequent primary neoplasms after specific primary cancers . 
 the level of granularity provided in the risk estimates ( eg , by primary cancer , type of subsequent primary neoplasm , and years from diagnosis ) should assist clinicians and policy makers in determining what type of interventions would be of greatest benefit for specific populations of aya cancer survivors . beyond improving risk prediction , several implications of the data are worth highlighting . 
for example , the surprising burden of subsequent lung cancers stands in contrast to the childhood cancer literature.7 in male survivors of hodgkin lymphoma , lung cancer accounted for approximately 40% of the total number of excess subsequent primary neoplasms , with a cumulative incidence of lung neoplasms of 51% at 35 years from diagnosis . 
it is unclear whether this difference compared with childhood cancer survivors is caused by several primary aya cancers being themselves related to smoking history ( eg , cervical cancer ) , a higher probability of smoking after diagnosis , 8 increased use of treatments such as lung radiotherapy , greater attained age , or a combination of these factors . 
irrespective of the mechanism , bright and colleagues results support interventions for survivors and smoking cessation raise the intriguing question of whether lung cancer screening guidelines developed for other high - risk populations may be appropriate.9 a second difference concerns temporal trends . 
the risk of subsequent primary neoplasms in childhood cancer survivors has decreased over consecutive cohorts , largely associated with reductions in radiotherapy doses.2 , 10 in this study , treatment decade was not significantly associated with subsequent primary neoplasm risk , suggesting that no such decline has occurred in the aya survivor population . 
 alternatively , reducing the incidence of subsequent primary neoplasms in survivors of aya cancer might require a stronger focus on lifestyle factors . represents a substantial contribution , several limitations merit note . 
however , a patient with hodgkin lymphoma might receive only two cycles of chemotherapy or might undergo six cycles and radiotherapy , with consequently vastly different risks for subsequent primary neoplas without treatment data , the clinician is still left uncertain on how to counsel an individual patient on his or her personalised risk , or what screening to recommend . 
aya - specific risk prediction models that include treatment exposure are urgently needed . finally , description of risk is only a first step towards the ultimate goal of improving the quantity and quality of life for survivors of aya cancer . 
determining what health - care delivery models maximise uptake of such interventions in a population known to face substantial barriers to access will also be necessary . for decades , paediatricians have insisted that children are not just little adults . 
we must now be equally emphatic in declaring that when it comes to the late effects of cancer and cancer therapy , ayas are not just big children , but instead deserve recognition as their own unique group . sumit gupta division of haematology / oncology , hospital for sick children , toronto , on , m5g 1x8 , canada sumit.gupta@sickkids.ca i declare no competing interests . copyright 2019 the author ( s )  . 
risk of subsequent primary neoplasms in survivors of adolescent and young adult cancer ( teenage and young adult cancer survivor study ) : a population - based , cohort study . 
jama 2017 ; 317 : 81424 . pet oestrogen receptor imaging : ready for the clinic ? oestrogen signalling is a key component of normal mammary gland physiology and mediates breast cancer pathogenesis in most breast cancers.1 drugs targeting oestrogen - mediated growth in breast cancer , termed endocrine therapy , provide a key therapeutic strategy . 
 the presence or absence of oestrogen receptors is a predictor of breast cancer response to endocrine therapy ; documenting oestrogen receptor expression from a biopsy sample before initiating therapy is a well established clinical standard.1 although primary breast tumour biopsy is well developed , safe , and effective , tissue sampling and assays pose challenges in the metastatic setting . 
 consumption of excessive amounts of food and drink containing high levels of sugar can lead to weight gain , and the report states that 10% of 45 year olds , 19% of 1011 year olds , and almost 25% of adults in england are obese ; a substantial proportion of all age groups are overweight . 
the health e ects of being overweight or obese are well - documentedeg , heart disease , diabetes , stroke , and cancersindeed , one in 20 cancers in the uk are related to being overweight . 
 the report o ers a number of recommendations to help cut sugar intake : special promotions in shops should be reduced , and advertising of food and drink to children and adults across all media substantially decreased . 
clear de nitions of high sugar foods are called for , as is the introduction of a programme of gradual reduction in sugar levels in everyday food and drink products , together with reductions in portion size . 
 the introduction of government buying standards for food and catering across the public sector is proposed , as is ensuring that individuals with the opportunity to in uence food choices in the catering , tness , and leisure sectors have appropriate training in diet and health . 
evidence suggests that price increases for high sugar foods and non - alcoholic drinks are likely to reduce the sales of these products , at least in the short tersimilar schemes are already in place in other countries , such as norway , finland , hungary , france , and mexico . 
and indeed , following the introduction of a peso - per - litre tax on sugar sweetened drinks in mexico in october , 2013akin to a 10% increase in pricepreliminary data suggest that there was a reduction of 6% in purchasing of such products in 2014 , with larger reductions noted in more socioeconomically deprived households . 
and perhaps under pressure from the drinks industry , the mexican congress voted on oct 20 , 2015 , to cut the tax in half for drinks with less than 5 mg sugar per 100 ml . 
indeed , whether taxation of unhealthy foods actually works is contentiousfor instance , denmarks fat tax , introduced to wide acclaim in october , 2011 , was abandoned after just 15 months as a result of negative economic effects , little evidence of a reduction in consumption , and the lack of popularity among the public . 
in addition to objections from business owners and trade unions , the tax was widely criticised for making the poor poorer , a situation that could also arise with a sugar tax . 
furthermore , one could foresee a situation in which the food and drinks industry could absorb any potential increase in price in the large and excessive profit margins for their products . thus , taxing the consumer is a blunt weapon and might not be the panacea to tackling sugar consumption on its own . 
the past 3040 years have seen unprecedented changes in the way we interact with food , both in terms of the foods available and in how they are produced , marketed , and advertised . 
 we have become complacent , disconnected with the realities of food production , and the forces of capitalism have allowed the food industry to shirk their ethical responsibility in the pursuit of pro t . 
 public health englands report recognises the need for cultural change and an acknowledgment of individual responsibilities , and proposes the our introduction of a plan to gradually reduce sugar levels in everyday food and drink products . 
however , a recent report from the institute for alcohol studies shows that a voluntary responsibility deal between the uk government and the alcohol industry has failed to implement any meaningful change . 
lancet oncol 2019 ; 20 : 71927 in the summary and methods of this article , the data cutoff date has been updated from dec 31 , 2017 , to june 30 , 2017 . 
this correction has been made to the online version as of april 30 , 2019 , and the printed version is correct . e243 vol 20 may 2019 corrections farewell to four greats as we begin a new year with optimistic anticipation of further achievements in oncology , we must pause to pay tribute to four major innovators and mentors who sadly died at the start of 2019 . on jan 2 , professor waun ki hong , a pioneering physician and scientist at the md anderson cancer center ( houston , tx , usa ) , died aged 76 . 
his work contributed to notable advances in chemoprevention , organ preservation in laryngeal cancer , and personalised targeted therapy . professor bertrand coiffier , who also died on jan 2 , aged 71 , was a leading lymphoma expert , who focused on developing new drug regimens to improve outcomes for aggressive lymphoma . 
he was a professor of hematology at the hospices civils de lyon and the university claude bernard ( lyon , france ) , and was a founding member and president of the groupe detude des lymphomes de ladulte , which later merged with another group to form the world - renowned lymphoma study association . jan 7 , professor john mendelsohn , a former president of the md anderson cancer center , died from glioblastoma , aged 82 . 
he helped to develop the monoclonal antibody cetuximab , which is used to treat colorectal , head and neck , and lung cancers . martin gore , professor of cancer medicine at the institute of cancer research and medical director at the royal marsden hospital ( london , uk ) , died suddenly on jan 10 aged 67 , reportedly after a yellow fever vaccination . 
 he received a cbe in the queens 2016 birthday honours list for services to oncology . as we reflect on the untimely loss of these four inspirational , leading oncologists , this has been a sadand unprecedentedway to start 2019 . 
 the lancet oncology big influences on anti - obesity strategies obesity , the second biggest preventable cause of cancer after tobacco smoking , is a major public health problem worldwide . 
governments must take steps to address this issue ; however , recent reports suggest that chinas antiobesity policies are being influenced by external players . increasingly westernised diets , escalating rural - to - urban migration , and sedentary lifestyles have caused chinas obesity levels to more than double since 1991 . 
in response , the chinese government has launched several public health campaigns , including happy 10 minutes , which encourages schoolchildren to have daily 10 - min breaks for exercise . 
why ? according to recent studies in the bmj and the journal of public health policy , the chinese governments attempts to tackle obesity are being supported by several large multinational food companies , including coca - cola , pepsi - cola , and nestl . 
these companies fund a noninternational life profit research organisation , the sciences institute ( ilsi ) , originally established in the usa in 1978 by a coca - cola executive . 
for several decades , ilsichina has led public health initiatives emphasising the importance of exercise and physical activityrather than nutritionas key to solving the obesity proble by focusing more on physical activity than on a healthy diet , attention is diverted away from highly processed food and calorie - dense snacks and drinks . 
shaping public health policy in this way could help the funding companies to protect sales of their own products and potentially avoid food regulations , advertising rules , and sugar taxes that have been introduced elsewhere . however , diet is clearly crucial . 
governments must not allow their public health strategies to be unduly influenced by powerful multinationals who might be more concerned with protecting their own interests than helping to solve this ongoing health crisis . 
 the lancet oncology vol 20 february 2019 for the bmj report see bmj 2019 ; 364 : k5050 . for the the journal of public health policy study see j public health pol 2019 ; published online jan 9 . 
ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
haematologica 2015 ; 100 : e30206 . lenalidomide as maintenance for every newly diagnosed patient with multiple myeloma in patients with newly diagnosed multiple myeloma , how to maintain the responses achieved after optimal therapeutic strategies was a challenge , and maintenance therapy emerged as an option aiming to extend the duration of the response through continued treatment and thereby improving progression - free survival and overall survival . 
because maintenance treatment is administered as continuous therapy , emphasis is placed on the convenience of administration , tolerability , and toxicity.1 low - dose lenalidomide is the only approved single agent treatment for patients with newly diagnosed multiple myeloma after transplantation.2 in the lancet oncology , graham jackson and colleagues3 confirm the benefit of lenalidomide in terms of progression - free survival . 
 in transplantation - ineligible patients , the findings by jackson and colleagues also support the results reported with lenalidomide as maintenance after induction with melphalan , prednisone , and lenalidomide , and are in line with the use of full - dose lenalidomide and dexamethasone as continuous therapy reported in the first trial.4 , 5 although the debate in this setting has always been whether to use fixed or continuous therapy , the trend now is use of continuous therapy with either lenalidomide or daratumumab after induction with daratumumab in combination with bortezomib plus melphalan and prednisone.6 patient with newly diagnosed multiple myeloma , but new therapies or combinations of drugs are needed to improve overall survival in these patients . the approved dose of lenalidomide is convenient because it is administered orally , and this study did not report any unexpected toxicity data . 
additional studies assessing health - related quality of life through patient - reported outcomes are necessary to know the patients perspective . lenalidomide is 10 mg continuously with the possibility of increasing to 15 mg , but different doses and schedules have been so far used in different trials . 
whether different doses and schedules could potentially result in different outcomes is not known , but the results of this study3 regarding the median progression - free survival of 26 months ( 95% ci 2231 ) in transplantation - ineligible patients is similar to that reported in the first trial , in which lenalidomide was given at full dose combined therefore , with possible to switch to low - dose lenalidomide without dexamethasone in transplantation - ineligible patients after induction therapy ? low - dose dexamethasone . 
 it , lenalidomide maintenance seems to be effective , well tolerated , and convenient , despite the lack of overall survival benefit , because of the influence of rescue therapies in the overall survival . 
lenalidomide is , therefore , a maintenance therapy option for every new agents or combinations of these are being investigated as maintenance therapy in this setting and might result in new standards of care . 
for example , vorinostat was combined with lenalidomide in a subset of patients in this study , and we await the results . published online december 14 , 2018 s1470 - 2045 ( 18 ) 30764 - 2 see articles page 57 vol 20 january 2019 comment the results of this study3 support the benefit of lenalidomide maintenance across different subgroups of patients and highlights the progression - free survival benefit in patients with high - risk cytogenetic abnormalities . 
however , it is important to note that lenalidomide did not overcome the poor prognosis that the presence of high - risk abnormalities confer to patients , and therefore novel treatments to improve the outcomes of these patients are needed . whether all patients need continuous maintenance therapy regardless of the quality of the response achieved with previous treatments remains unclear . 
however , next - generation sequencing and cytometry provide an opportunity to investigate the role of minimal residual disease assessment for tailoring maintenance strategies and would allow physicians to prescribe maintenance therapy and reply to a very common question raised by the patients : how many cycles of treatment does maintenance therapy include ? furthermore , long - term minimal residual disease monitoring could guide preemptive treatment preventing clinical relapses and ensuring durable responses . maintenance with lenalidomide is the standard of care , but the future has to move towards a personalised medicine approach that aims to improve overall survival and quality of life , which means giving the right drug to the right patient at the right time for the optimal duration . * mara - victoria mateos , vernica gonzlez de la calle hematology department , university hospital of salamanca , ibsal , salamanca , spain mvmateos@usal.es m - vm has received honoraria for lectures from janssen , celgene , takeda , and amgen , and for participation in advisory boards from janssen , celgene , takeda , amgen , abbvie , glaxosmithkilne , and pharmamar . 
n engl j med 2018 ; 378 : 51828 . the importance of surgery in colorectal cancer treatment in the lancet oncology , sara benitez majano and colleagues1 have engaged with a very important topic . 
 previous data have indicated poorer treatment results for colorectal cancer in both denmark and england compared with those in similar western countries.2 the continuous audit and assessment of outcomes is important to better understand the reality of cancer care each country and thus , this study is of interest to the public . majano and colleagues identified that an important difference between the countries studied regarding surgery for colorectal cancer was probably not the technique , but rather the frequency of surgical resection . 
 the proportion of patients treated with resectional surgery ranged from 684% in england to 813% in sweden for colon cancer , and from 599% in england to 708% in sweden for rectal cancer ; this range was wider for patients older than 75 years ( colon cancer 597% to 809% ; rectal cancer 457% to 619% )  . 
it is possible that attitudes towards surgery in the older patient population should be altered in england , but the data in this study do not include comorbidity , and the risk for increased perioperative mortality should not be underestimated . 
 preoperative optimisation of patients must be a focus of research , to increase the percentage of patients that are able to undergo resectional surgery in the future . what other factors could be influencing these results ? during the study period , the standardised referral pathway had already been introduced in denmark in 2010 . 
there is scarce vol 20 january 2019 published online december 10 , 2018 s1470 - 2045 ( 18 ) 30679 - x see articles page 74 comment published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections corrections published online march 25 , 2015 s1470 - 2045 ( 14 ) 71115 - 5 correction to lancet oncol 2013 ; 14 : e374 correction to lancet oncol 2015 ; 16 : e163 correction to lancet oncol 2015 ; 16 : 447 , 448 weller m , p ster sm , wick w , hegi me , reifenberger g , stupp r . 
the rst sentence should read : exposure to passive smoke among never smokers does not seem to increase the chances of acquiring somatic mutations in genes linked to non - small - cell lung cancer in smokers , a new study shows . 
 vorinostat in patients with advanced malignant pleural mesothelioma who have progressed on previous chemotherapy ( vantage - 014 ) : a phase 3 , double - blind , randomised , placebocontrolled trial . 
lancet oncol 2015 ; 16 : 44756in the a liation section , p bass should be listed at netherlands in the funding cancer section in the summary and in the a liations , merck & co has been changed to merck & co , inc . 
 lancet oncol 2015 ; 16 : 54149in the key of gure 2 of this article , the boxes should indicate patients who were ct positive for disease , not those who were circulating tumour dna positive for disease . 
this correction has been made to the online version as of april 30 , 2015 , and the printed version is correct . vol 16 may 2015 e199 correction to lancet oncol 2017 ; 18 : 1493501 correction to lancet oncol 2017 ; 18 : 156566 tawbi ha , burgess m , bolejack v , et al . 
 pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
this correction has been made to the online version as of dec 29 , 2017 . vol 19 january 2018 corrections corrections correction to lancet oncol 2012 ; 13 : 817 , 818 , 822 correction to lancet oncol 2014 ; 15 : 1195206 correction to lancet oncol 2015 ; 16 : 52 shen q , fan j , yang x - r , et al . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . vol 16 january 2015 kwon m , jang h , kim eh , roh jl . 
efficacy of poly ( adp - ribose ) polymerase inhibitor olaparib against head and neck cancer cells : predictions of drug sensitivity based on par - p53 - nf - b interactions . 
rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy ( ariel3 ) : a randomised , double - blind , placebo - controlled , phase 3 trial . 
 improving r - chop in diffuse large b - cell lymphoma is still a challenge since the introduction of rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ) as the gold standard for the treatment of diffuse large b - cell lymphoma , clinical investigators have constantly tried to improve its effectiveness by adding new drugs and proposing combinations ( ie , r - chop plus drug x ) .1 this strategy is justified by the great biological heterogeneity of diffuse lymphomas , suggesting that r - chop cannot be a universal treatment but can instead provide a rational basis for personalised therapy . 
as such , for the past decade molecular classification on the basis of the distinction between germinal centre b - cell - like and activated b - cell - like subtypes has largely dominated the debate and focused efforts in terms of targeted therapy and biomarker research.2 large b - cell to show the potential of such a strategy , biologically relevant , reliable , repro ducible biomarkers and a corresponding effective molecule that are likely to improve the efficacy of the r - chop regimen need to be identified . the prospective multicentre phase 3 remodl - b trial , reported in the lancet oncology by andrew davies and colleagues , 3 shows that real - time characterisation of diffuse large b - cell lymphoma is feasible by use of molecular biology with rna extracted from formalinfixed paraffin - embedded ( ffpe ) samples and cdnamediated annealing , selection , extension , and ligation techniques.3 among the 1128 eligible patients in this trial , 918 ( 81% ) were effectively classified according to their cell of origin ( 244 [ 27% ] activated b cell , 475 [ 52% ] germinal centre b cell , and 199 [ 22% ] unclassified )  . 
phenotyped patients were subsequently randomly assigned ( 1 : 1 ) after the first r - chop cycle to receive either r - chop or r - chop with bortezomib ( rb - chop )  . 
the primary outcome analysis showed that the addition of bortezomib does not provide any benefit in terms of progressionin the overall population ( 30 - month free survival progression - free survival 701% [ 95% ci 650747 ] with r - chop vs 743% [ 693787 ] with rb - chop ; adjusted hazard ratio 084 , 95% ci 064111 ; p = 023 ) , with the same conclusion drawn in the secondary outcome analyses in the germinal centre b - cell , activated b - cell , and unclassified subgroups . 
these results support those of a randomised phase 2 trial by leonard and colleagues.4 however , davis and colleagues point out a potential benefit of the combination for patients with double - hit lymphoma or dual - expressor lymphoma ( ie , myc and bcl2 ) , although this benefit was not significant . 
the results show that despite overexpression of the nuclear factor ( nf ) - b pathway and activating mutations of this pathway in activated b - cell diffuse large b - cell lymphoma , the addition of bortezomiba proteasome and nf - b pathway inhibitordoes not provide any benefit over r - chop.3 in diffuse large b - cell how can these ultimately disappointing results be explained ? a relative under - representation of the activated b - cell subtype as compared with previous lymphoma , 5 cohort studies substantially older patients in the activated b - cell subgroup , and the use of bortezomib only from the second cycle onwards , with a relatively low dose , might all have affected the efficacy outcome of the addition of bortezomib . 
a phase 3 randomised study ( phoenix ) 6 that specifically targeted the activated b - cell subtype did not clearly show the value of adding ibrutinib ( an inhibitor of brutons tyrosine kinase ) to r - chop in this setting . 
however , the toxicity of this combination in patients aged 60 years and older is probably partly responsible for the negative conclusion since a benefit in overall survival large b - cell published online april 1 , 2019 s1470 - 2045 ( 19 ) 30021 - x see articles page 649 vol 20 may 2019 comment and progression - free survival was observed for patients younger than 60 years.6 the prognostic effect of the cell - of - origin classification also remains uncertain and has been questioned in two prospective trials.5 data from the cavalli phase 2 trial7 showed a benefit in adding the bh3 ( bcl2 homology 3 ) mimetic venetoclax to r - chop in patients positive for bcl2 , irrespective of whether they had the germinal centre or non - germinal centre b cell subtype of disease , suggesting that a single biomarker ( bcl2 expression quantified by immunohistochemistry ) might be more relevant than cell - of - origin molecular determination for patient selection.7 new classifications that integrate next - generation sequencing , fluorescence in - situ hybridisation , or copy number variation data are now available and might offer other therapeutic or predictive opportunities.810 however , these models are complex , partially overlapping , and relatively difficult to test in a randomised clinical trial or apply in daily practice . 
the selection of diffuse large b - cell lymphoma patients on the basis of biological markers before the first treatment therefore remains a crucial challenge . fabrice jardin department of clinical hematology , centre henri becquerel , inserm u1245 , rouen university , rouen 76038 , france fabrice.jardin@chb.unicancer.fr i have received personal fees from roche , celgene , janssen , gilead , amgen , and servier . copyright 2019 the author ( s )  . 
gene - expression profiling of bortezomib added to standard chemoimmunotherapy for diffuse large b - cell lymphoma ( remodl - b ) : an open - label , randomised , phase 3 trial . 
randomized phase ii study of r - chop with or without bortezomib in previously untreated patients with non - germinal center b - cell - like diffuse large b - cell lymphoma . 
clinical impact of the cell - of - origin classification and the myc / bcl2 dual expresser status in diffuse large b - cell lymphoma treated within prospective clinical trials of the german high - grade non - hodgkins lymphoma study group . 
a global , randomized , placebo - controlled , phase 3 study of ibrutinib plus rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisone ( rchop ) in patients with previously untreated non - germinal center b - cell - like ( gcb ) diffuse large b - cell lymphoma ( dlbcl )  . 
cell 2017 ; 171 : 48194 . adjuvant capecitabine in biliary tract cancer : a standard option ? in the lancet oncology , john primrose and colleagues1 have tackled the question of adjuvant treatment for a rare cancer : biliary tract cancer , an unresolved question to date . 
although a meta - analysis ( of mostly retrospective data ) has suggested improved overall survival with adjuvant treatment ( especially chemotherapy in patients with node - positive disease and adjuvant radiation - based therapy after r1 resection ) , 2 older randomised studies were not sufficiently statistically powered to define a standard of care , 3 , 4 and two recent randomised studies did not show a significant benefit of gemcitabine5 or gemcitabine plus oxaliplatin ( gemox regimen ) .6 randomised , phase 3 , bilcap study , 753 patients were screened across 44 uk centres the between 2006 and 2014 , of whom 447 patients with curatively resected cholangiocarcinoma or muscleinvasive gallbladder cancer and preserved performance status ( eastern cooperative oncology group 0 or 1 ) were randomly assigned to receive oral capecitabine for 24 weeks or observation.1 unfortunately , the study did not meet its primary endpoint : the median overall survival by intention - to - treat was 511 months ( 95% ci 346591 ) in the capecitabine group compared with 364 months ( 297445 ) in the observation group ( hazard ratio [ hr ] 081 , 95% ci 063104 ; p = 0097 )  . should capecitabine be considered as ineffective as gemcitabine5 and gemox6 in the other two recent adjuvant trials ? probably not . 
in fact , despite being vol 20 may 2019 606 published online march 25 , 2019 s1470 - 2045 ( 19 ) 30022 - 1 see articles page 663 comment and advisory board and consulting fees from eli lilly ; has received personal fees and held stock as a member of advisory board from seragon ; has received reimbursement for travel and in - kind items and services from roche , outside the submitted work . 
 s - ai reports grant support from astrazeneca and advisory consultant roles for astrazeneca , eisai , novartis , pfizer , roche / genentech and spectrum , outside the submitted work . 
hi reports grant support and personal fees from novartis during the conduct of the study ; hi was also an uncompensated member of the steering committee of this study ; hi has received personal fees in the form of honoraria and consulting fees from astrazeneca , pfizer , lilly , daiichi - sankyo , and f hoffman la - roche via chugai , outside the submitted work . 
jc reports personal fees from novartis , celgene , cellestia , astrazeneca , biothera pharmaceuticals , merus , seattle genetics , daiichi sankyo , erytech , pfizer , eisai , and samsung ; has received stock , patents , and intellectual property from medsir ; has received personal fees and research funding to his institution from roche , outside the submitted work . 
mdls reports personal fees in the form of speakers honoraria and advisory board honoraria from novartis , roche , lilly , pfizer , eisai , ipsen , and teva , outside the submitted work . 
cla reports personal fees for participation in a steering committee for the clinical trial from novartis , during the conduct of the study ; and personal fees for an expert advisory role from eli lilly , astrazeneca , genentech , millennium , celgene , pfizer , radius , and merck , outside the submitted work . 
sc also reports personal fees received in the form of honoraria for advisory boards from novartis , hoffmann laroche , pfizer , astrazeneca , and genomic health ; and institutional research support from novartis , hoffmann laroche , pfizer , astrazeneca , genomic health , genentech , merck , and bms , outside the submitted work . 
she also reports grant support from ambryx , amgen , bayer , obi pharma , bimarin , cascadian , daiichi sankyo , dignitana , genentech , gsk , lilly , macrogenics , medivation , merrimack , novartis , pfizer , pieris , puma , roche , seattle genetics , and travel support from lilly , novartis , and obi pharma , outside the submitted work . 
 reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
pv reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 15964 wolf a , naylor k , tam m , et al . 
these corrections have been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 17980 massari f , di nunno v . 
lancet oncol 2019 ; 20 ; 17980in this comment , the following sentence has been edited from time to deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab to risk of deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab . 
we aimed to establish the short - term safety of immediate implant - based breast reconstruction performed with and without mesh , to inform the feasibility of undertaking a future randomised clinical trial comparing different breast reconstruction techniques . methods in this prospective , multicentre cohort study , we consecutively recruited women aged 16 years or older who had any type of immediate implant - based breast reconstruction for malignancy or risk reduction , with any technique , at 81 participating breast and plastic surgical units in the uk . 
outcomes of interest were implant loss ( defined as unplanned removal of the expander or implant ) , infection requiring treatment with antibiotics or surgery , unplanned return to theatre , and unplanned re - admission to hospital for complications of reconstructive surgery , up to 3 months after reconstruction and assessed by clinical review or patient self - report . 
the study is registered with the isrctn registry , number isrctn37664281 . findings between feb 1 , 2014 , and june 30 , 2016 , 2108 patients had 2655 mastectomies with immediate implant - based breast reconstruction at 81 units across the uk . 
1376 ( 65% ) patients had reconstruction with biological ( 1133 [ 54% ] ) or synthetic ( 243 [ 12% ] ) mesh , 181 ( 9% ) had non - mesh submuscular or subfascial implants , 440 ( 21% ) had dermal sling implants , 42 ( 2% ) had pre - pectoral implants , and 79 ( 4% ) had other or a combination of implants . 
of these patients , 182 ( 9% , 95% ci 810 ) experienced implant loss , 372 ( 18% , 1620 ) required re - admission to hospital , and 370 ( 18% , 1620 ) required return to theatre for complications within 3 months of their initial surgery . 
the rates of all of these complications are higher than those in the national quality standards ( < 5% for re - operation , re - admission , and implant loss , and < 10% for infection )  . interpretation complications after immediate implant - based breast reconstruction are higher than recommended by national standards . 
a randomised clinical trial is needed to establish the optimal approach to immediate implantbased breast reconstruction . funding national institute for health research , association of breast surgery , and british association of plastic , reconstructive and aesthetic surgeons . copyright 2019 the author ( s )  . 
the mesh is sutured between the lower edge of the pectoralis muscle and the chest wall to create a larger subpectoral pocket that can accommodate a fixed - volume implant at the time of the initial surgery . 
the remaining studies comprised 40 comparative studies and 20 case series , all of which were at high risk of bias . we did another pubmed search in april , 2018 , and identified one small randomised clinical trial that compared standard two - stage expander - implant reconstruction with mesh - assisted , single - stage , direct - to - implant breast reconstruction . 
the frequency of complications in the single - stage , mesh - assisted , direct - to - implant group was significantly higher than that in patients receiving two - stage expander implant reconstruction , and the study was stopped prematurely . 
these studies did not show any differences between products , but were small and underpowered . added value of this study this prospective cohort study of more than 2000 patients having immediate implant - based breast reconstruction in the uk provides high - quality , real - world data regarding the short - term safety outcomes of different implant - based techniques with and without mesh . 
the frequency of key complications , including implant loss , infection , re - admission , and re - operation for complications of reconstructive surgery , was much higher than anticipated ; although adverse outcomes were associated with smoking and increased body - mass index , there was no association with the use or type of mesh in this non - randomised study . 
these findings support the need for a future pragmatic randomised clinical trial to determine the most clinical and cost - effective technique of implant - based breast reconstruction . implications of all the available evidence complications after immediate implant - based reconstruction with and without mesh are high , and patients should be carefully counselled regarding their surgical options . 
 urgent work will also be necessary to determine how the high incidences of complications shown in this study could be reduced . the practice of patients and health - care providers . 
these meshes differ notably in price and , in the absence of comparative evidence , product selection is largely dependent on surgeon preference . immediate implant - based breast reconstruction has evolved further with the introduction techniques.7 these techniques involve wrapping the implant in mesh and placing it on top of , rather than underneath , the pectoralis muscle . 
this pre - pectoral technique might further improve outcomes for patients by reducing postoperative pain and preventing implant animation , the upward movement of the implant seen when the pectoralis muscle contracts.7 so - called muscle - sparing despite the widespread adoption of mesh - assisted techniques into practice , evidence to support the proposed benefits of mesh is lacking.710 a multicentre dutch randomised controlled trial11 showed significantly increased numbers of complications in single - stage , direct - to - implant reconstruction with mesh compared with standard two - stage expander - implant techniques . 
 the study was criticised because the participating surgeons had limited experience with the technique , 12 but further analysis did not identify a learning curve effect.13 however , other large multicentre prospective studies have not shown a significant difference in incidence of com plications or patient - reported outcomes between single - stage direct - to - implant and two - stage techniques , 14 or between two - stage expander - implant reconstruction done with and without acellular dermal matrix.15 although these findings are supportive of the technique , there remains the need for high - quality vol 20 february 2019 articles evidence from a randomised study to support practice . 
 a small randomised clinical trial16 that compared biological single - stage synthetic mesh direct - to - implant reconstruction was underpowered and insufficiently well designed to generate meaningful results . and there is therefore a need for high - quality research to establish the safety and effectiveness of mesh in immediate determine what mesh should be recommended , and , as practice evolves , to determine if the implant should be placed on top of or underneath the pectoralis muscle.7 implant - based breast reconstruction , randomised clinical trials are ideally needed , but randomised clinical trials in breast reconstruction are challenging because of patient and surgeon preference17 and previous trials have closed prematurely because not enough patients were able to be recruited.18 , 19 careful pretrial work is therefore needed to ensure that a future randomised clinical trial is well designed and addresses questions that are important to patients and the reconstructive community . ibra ( implant breast reconstruction evaluation ) 20 is a four - phase study that aims to inform the feasibility , design , and conduct of a future trial in immediate implantbased breast reconstruction . 
results from phase 1 ( a national practice questionnaire to understand current practice ) were previously reported.21 , 22 here we report the primary endpoint for phase 2 , a prospective multicentre national study to determine the short - term clinical outcomes of different approaches to immediate implantbased breast reconstruction in the uk and inform the selection of comparators and sample size for a future randomised clinical trial . implant - based breast recon struction methods study design and participants for this prospective , multicentre ibra study , we invited all uk breast or plastic surgical units performing immediate participate in the study , through the uk trainee collaborative research network and two professional associations , the association of breast surgery and the british association of plastic reconstructive and aesthetic surgeons . 
81 centres participated in the study . women aged 16 years or older , who had a mastectomy and immediate implant - based breast reconstruction using any technique for malignancy or risk reduction at participating centres , were consecutively recruited to the study . 
patients were excluded if they had reconstruction with an implant in combination with a tissue flap ( eg , latissimus dorsi flap and implant ) , had delayed reconstruction , or had revisional surgery . ethics approval was not required , as defined by the hra decision tool . 
 outcomes assessed against each participating centre was required to obtain local audit approvals and register the study before commencing study recruitment , consistent with the methods of previously reported multicentre prospective trainee collaborative studies . 
patient consent was not required for routine clinical data collection , but patients provided written informed consent to receive patient - reported outcome questionnaires , in keeping with the methods employed in the uk national mastectomy and breast reconstruction audit.24 all data were recorded in an anonymised format on a secure web - based database , redcap.25 procedures we prospectively identified eligible patients from clinics , multidisciplinary team meetings , and theatre lists . 
 simple demographic , comorbidity , and operative data were collected for each participant . all patients had skin or nipple - sparing mastectomy followed by immediate implant - based breast reconstruction . 
implants or tissue expanders could be placed under the pectoralis muscle ( subpectoral ) with or without biological or synthetic mesh , or on top of the muscle ( pre - pectoral ) supported by mesh . 
reconstructions were considered to be two - stage if a temporary expander was placed at the time of the initial mastectomy and a second procedure was planned to insert a definitive implant at a later date . precise details of the techniques used varied by surgeon , but broadly , for submuscular reconstructions , a tissue expander was inserted in a pocket created under the pectoralis muscle . 
serratus fascia could be raised to provide complete expander coverage , or the lateral aspect of the expander could be left subcutaneous as per surgeon preference . sub - pectoral reconstruction with mesh involved releasing the lower boarder of the pectoralis muscle from the chest wall and suturing the mesh to the free edge of the muscle . 
a definitive fixed - volume implant , adjustable implant , or tissue expander was then inserted according to surgeon preference and the mesh either sutured at the level of the inframammary fold or tucked under the implant , depending on the product used . 
for dermal sling reconstruction , the pectoralis muscle was detached in a similar way and the lower mastectomy flap de - epithelialised and sutured to the free muscle edge to provide coverage of the lower pole of the for more on redcap see for more on the hra decision tool see decisiontools.org.uk / research 256 vol 20 february 2019 articles implant . 
it is not standard practice to use mesh in this procedure . finally , for pre - pectoral reconstruction , the pectoralis muscle was not disturbed , but a fixed - volume implant , adjustable tissue expander completely or partially wrapped in mesh ( depending on surgeon preference and product selection ) was placed in the mastectomy cavity and sutured into place . implant , or temporary in all cases , perioperative and postoperative antibiotics and drains were used according to local policy or surgeon preference . complication and oncological data were collected by the clinical team at 30 days and 3 months after reconstruction by clinical or case - note review , or both , depending on when the patient returned for follow - up . participants were approached in the clinic or during their hospital stay to obtain consent for patient - reported outcome assessment at 3 months after surgery . 
the patient - reported outcome was a modified version of the 3 - month questionnaire used in the uk national mastectomy and breast reconstruction audit ( nmbra ) and included patient self - report of complications occurring in the 3 months after surgery.24 questionnaires were sent centrally by post or e - mail , depending on patient preference , with a reminder sent 1 month after the initial questionnaire if no response was received . 
 patient satisfaction was also assessed at 18 months after surgery.20 analyses are ongoing and these results will be reported elsewhere . outcomes on the basis of published national quality standards for breast reconstruction derived from the nmbra , 23 we prespecified four key outcomes to assess the short - term safety of different approaches to immediate implantbased breast reconstruction.20 we chose these outcomes because it was anticipated that a safety outcome might be the primary endpoint of a future trial and equivalence in a non - randomised study was important in informing the selection of potential comparators for this study . 
the outcomes were defined implant loss ( the unplanned removal or loss of the implant as a result of infection or other complication ) , infection ( the presence of a hot , red breast requiring treatment with antibiotics , surgery , or both ) , re - admission ( any unplanned re - admission to hospital after discharge for any complication of surgery ) , and reoperation ( any return to the operating theatre for a complication within 3 months of the reconstruction procedure )  . 
any implant loss , infection , re - admission , or re - operation occurring at any timepoint within the first 3 months of the initial reconstruction that was assessed by clinical review or patient self - report was considered an event and included in the analysis . we identified potential risk factors for each of these key outcomes using a prespecified exploratory risk - factor analysis . 
we identified specific variables of interest a priori from the published literature and expert opinion , and included the following patient - related and procedurerelated factors : age , body - mass index ( bmi ) , smoking ( current smokers vs others ) , previous radiotherapy to the ipsilateral breast ( yes vs no ) , receipt of neoadjuvant chemotherapy ( yes vs no ) , bilateral surgery ( yes vs no ) , mastectomy type ( nipple - sparing vs other mas tectomy types ) , type of implant or expander used ( fixed - volume vs adjustable implants or expanders ) , and type of immediate implant - based breast reconstruction performed . 
we classified reconstruction procedures according to the mode of lower pole coverage as being : submuscular or subfascial without mesh ; dermal - sling procedures using the patients own tissue ; biological mesh - assisted ( including acellular dermal matrix and non - dermal biological products ) ; synthetic mesh - assisted ; pre - pectoral if the implant was placed on top of the pectoralis muscle with or without mesh ; and other if a combination of techniques was used ( eg , dermal sling and mesh )  . for quality assurance purposes , the principal investigator at each participating site was asked to independently validate the primary outcomes for all study participants at 3 months and to check complete case ascertainment . statistical analysis because we aimed to inform the design of a future randomised clinical trial , the study was powered to establish parameters required for a sample size calculation and to inform further aspects of trial design , such as entry criteria for the future trial . therefore required at the time of study design , four clinical outcomes ( implant loss , re - admission , re - operation , and infection ) were considered to be potential primary outcomes in a randomised controlled trial , and a wide range of treatment approaches for immediate implant - based breast reconstruction were routinely offered.22 a large sample was to estimate , with reasonable precision , the incidence of the four clinical outcomes of interest ( implant loss , re - admission , reoperation , and infection ) within treatment approaches , and to determine how implant procedures are performed and any variation in patient selection for each of these approaches . 
a sample size of 197 participants would allow a two - sided 95% ci for a single proportion , assumed to be 009 , extending from 005 to 013 , using the large sample normal approximation . 
allowing for the 15% loss to follow - up at 3 months reported in the nmbra , an analysis of implant loss at 3 months required at least 235 patients to be recruited to inform a future trial with implant loss as a primary outcome . 
to determine how implant procedures are performed , centres participating in a national practice questionnaire vol 20 february 2019 articles 2217 patients entered into redcap database 2161 had surgery during study period 56 excluded 34 surgery outside study period 22 operation date not recorded 3 no immediate implant - based breast 53 excluded reconstruction 50 procedure not reported 2108 included in study 181 submuscular or subfascial without mesh 440 dermal sling 1133 biological mesh 243 synthetic mesh 42 pre - pectoral 64 other 15 not known 27 lost to follow - up 2081 with 3 - month follow - up included in 3 - month outcome analysis 180 submuscular or subfascial without mesh 436 dermal sling 1121 biological mesh 236 synthetic mesh 42 pre - pectoral 63 other figure : trial profile for patients with two implant - based reconstructions in which technique differed by breast ( n = 10 ) , these patients are summarised in both groups , depending on the approach used , and once in the total . 
variations of approaches per breast within patient were : biological mesh and dermal sling ( n = 3 ) , biological mesh and synthetic mesh ( n = 1 ) , dermal sling and submuscular or subfascial ( n = 4 ) , other and submuscular or subfascial ( n = 1 ) , and other and synthetic mesh ( n = 1 )  . ( n = 81 ) 21 , 22 were eligible to participate . 
all analyses are based on the number of patients , not the number of implants . we did the analysis according to a prespecified statistical analysis plan approved by the trial steering group . 
we did no formal statistical testing . we established the proportion and 95% ci of patients for each of the four key clinical outcomes to compare our findings against those reported in the nmbra24 and published national quality standards.23 we did a prespecified risk - factor analysis using multivariable logistic regression . 
variables of interest included patient age , bmi , smoking status , previous radiotherapy to the ipsilateral breast , receipt of neoadjuvant chemotherapy , bilateral surgery , nipple - sparing versus other mastectomy types , use of fixed - volume versus adjustable implants or expanders , and type of immediate implant - based breast reconstruction performed . data were considered missing at random ( appendix p 2 ) and therefore no missing data items were imputed . 
we considered this approach as unlikely to lead to bias because all included risk factors were measured once per patient.26 we checked linearity for continuous variables for all four logistic models using locally estimated scatterplot smoothing ( loess ) smoothed - line plots . 
we used sas ( version 9.3 ) for all analyses . this study was registered as an international standard randomised controlled trial , number isrctn37664281 , and the protocol was published in 2016.20 role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to the data in the study and had final responsibility for the decision to submit for publication . results between feb 1 , 2014 , and june 30 , 2016 , 2217 records were entered onto the redcap database . 
of these , 109 ( 5% ) were excluded : 34 patients had surgery outside the study period , 22 records did not include an operation date , 50 records provided no information regarding the type of surgery performed , and three patients did not have an immediate implant - based breast reconstruction . 
further details about unit recruitment are in the appendix ( pp 37 )  . biological mesh - assisted reconstruction was the most commonly performed procedure , with 1133 ( 54% ) of 2108 patients undergoing this technique . 
fewer patients had synthetic mesh - assisted immediate implant - based breast reconstruction ( 243 [ 12% ] ) , and 181 ( 9% ) received traditional subpectoral reconstruction without mesh . 
 subpectoral reconstruction with a dermal sling was done in approximately a fifth of patients ( 440 [ 21% ] ) and prepectoral reconstruction with mesh ( 42 [ 2% ] ) was done in the latter stages of the study . 
 * for patients with two implant - based reconstructions in which technique differed by breast ( n = 10 ) , these patients are summarised in both applicable columns , depending on the method used , and once in the total column . 
variations of approaches per breast within patient were biological mesh and dermal sling ( n = 3 ) , biological mesh and synthetic mesh ( n = 1 ) , dermal sling and submuscular or subfascial ( n = 4 ) , other and submuscular or subfascial ( n = 1 ) , and other and synthetic mesh ( n = 1 )  . 
 * for patients with two implant - based reconstructions in which method differed by breast ( n = 10 ) , these patients are summarised in both applicable columns , depending on the method used , and once in the total column . 
variations of approaches per breast within patient were biological mesh and dermal sling ( n = 3 ) , biological mesh and synthetic mesh ( n = 1 ) , dermal sling and submuscular or subfascial ( n = 4 ) , other and submuscular or subfascial ( n = 1 ) , other and synthetic mesh ( n = 1 )  . 
variable collected on a per - breast basis ; for patients with two implant - based reconstructions , with data for one breast and not the other , that patient is classified according to the non - missing data as indicated in the applicable footnote . 
 * * combinations of type of mastectomy within patients with two implant - based reconstructions with different types per breast were skin - sparing mastectomy and skin and nipple - preserving mastectomy ( n = 15 ) , skin - sparing mastectomy and reduction ( wise ) pattern ( n = 7 ) , skin - sparing mastectomy and other ( n = 3 ) , skin and nipple preserving and reduction ( wise ) pattern ( n = 2 ) , skin and nipple preserving and other ( n = 4 ) , reduction ( wise ) pattern and other ( n = 1 )  . 
combinations of location of incision within patients with two implant - based reconstructions with different types per breast were elliptical removing nac and inframammary ( n = 1 ) , elliptical removing nac and lateral ( n = 4 ) , elliptical removing nac and other ( n = 3 ) , elliptical removing nac and peri - areolar ( nipple preserving ; n = 3 ) , elliptical removing nac and wise - pattern ( n = 1 ) , inframammary and lateral ( n = 1 ) , inframammary and other ( n = 2 ) , inframammary and peri - areolar ( nipple preserving ; n = 1 ) , lateral and peri - areolar ( nipple preserving ; n = 1 ) , other and wise pattern ( n = 2 )  . 
 combinations of breast prosthesis used within patients with two implant - based reconstructions with different types per breast were combined implant ( beckers ) and fixed - volume implant ( n = 1 ) , and fixed - volume implant and temporary expander ( n = 3 )  . 
combinations of axillary surgery within patients with two implant - based reconstructions with different surgeries per breast were axillary clearance and none ( n = 41 ) , axillary clearance and previous staging axillary surgery ( n = 1 ) , axillary clearance and sentinel node biopsy ( n = 10 ) , axillary sample and none ( n = 6 ) , none and previous staging axillary surgery ( n = 32 ) , none and sentinel node biopsy and immediate clearance ( n = 2 ) , none and sentinel node biopsy ( n = 46 ) , and sentinel node biopsy and previous staging axillary surgery ( n = 1 )  . table 2 : operative details , by type of implant - based reconstruction patients , details of the technique were not reported . 
 strattice ( lifecell , brachburg , nj , usa ) or surgimend ( integra lifesciences ) were used in 1215 ( 66% ) of the 1831 mesh - assisted procedures , but in total , 14 different products were used during the course of the study ( artea , biodesign , braxon , cellis , meso biomatrix , native , protexa , silk , strattice , surgimend , tigf , tiloop , veritas , and xcm ) , with an increasing variety of products used as the study progressed ( data not shown )  . the median age of study participants was 49 years ( 4357 ; table 1 )  . 
median bmi was at the upper end of the normal range ( 248 kg / m ; iqr 223282 ) , and was highest overall in patients who had dermal sling reconstruction ( table 1 )  . 
of the 547 ( 26% ) patients having bilateral surgery , 188 ( 34% ) had a contralateral risk - reducing mastectomy at the time of their index cancer operation ( table 2 )  . a one - stage reconstruction was planned in 1650 ( 78% ) patients , and 1239 ( 59% ) had a definitive fixedvolume implant placed at the time of their surgery . 
 tissue expanders or two - stage reconstruction with expandable implants was more common in patients having traditional submuscular procedures without mesh and those having dermal sling reconstruction than in those having other procedure types ( table 2 )  . 
skin and nipple - sparing reconstruction was done in nearly a quarter of cases ( table 2 )  . immediate approximately a third of the 1693 patients having mastectomy and implant - based breast reconstruction for malignancy were recommended chemo therapy or radiotherapy after their reconstruction ( table 3 )  . 
this recommendation did not appear to be related to the type of procedure performed , although more patients having standard subpectoral reconstruction without mesh were recommended for radiotherapy than were patients having other procedure types ( table 3 )  . breast implant - based of the 2108 patients recruited , 2081 ( 99% ) were followed up to 3 months ( median follow - up 3 months , iqr 33 )  . 
 ( 9% ) of loss was experienced by 182 implant 2081 patients followed up at 3 months , which is equivalent to the nmbra published data ( 9% ) but higher ( < 5% )  . 
when two patients have two malignant breasts and there were data about the number of lymph nodes involved for both breasts ( n = 53 ) , the average number of nodes is given . 
when two patients had two malignant breasts with planned axillary clearance data available for one breast , patients are classified according to the breast for which there are data ( n = 12 yes , n = 9 no )  . 
||when both breasts were operated for cancer but only one side needed radiotherapy . table 3 : postoperative data for patients having mastectomy for oncological indications re - admitted for a complication after their reconstruction within 3 months . 
there were 2108 patients with implant - based reconstruction , of whom 2081 ( 99% ) were included in the outcome analysis : complete outcome data ( event data for all four key outcomes ) are available for 2078 patients , who have been included in the analysis 27 ( 1% ) patients have no outcome data and were excluded from the analysis . 
partial outcome data ( event data for three of four outcomes ) are available for three patients , who were included in the analysis and who were assumed to not have had the event for the fourth missing outcome . table 4 : 3 - month outcomes after implant - based breast reconstruction , by procedure type , compared with outcomes in nmbra and uk national quality criteria for breast reconstruction using exploratory multivariable logistic regression , we identified an apparent association between body - mass index and smoking with all four clinical outcomes ( table 5 )  . 
age , neoadjuvant chemotherapy , bilateral surgery , indication for surgery , nipplesparing procedures , insertion of a definitive fixed - volume implant , and type of recon struction performed were not significant risk factors for any of the key safety outcomes ( table 5 )  . 
details of the number of events for each risk factor are shown in the appendix ( p 8 )  . discussion this national , multicentre , prospective cohort study of 2108 patients having immediate implant - based breast reconstruction in 81 centres across the uk shows that the short - term clinical outcomes of immediate implantbased breast reconstruction fall far short of the published aspirational quality standards for immediate breast reconstruction , 23 and have not improved in the 10 years since the nmbra.24 despite recently published evidence showing increased frequency of complications in meshassisted immediate implant - based breast reconstruction , 11 there was no association between type of mesh and shortterm safety outcomes in exploratory regression analyses of this large , non - randomised study . 
to truly answer this important question , a large - scale , pragmatic , randomised controlled trial will be required to identify the most clinically and costeffective approach to immediate implant - based breast reconstruction , and provide information to inform clinical and health policy decisions . despite insufficient high - quality evidence , meshassisted , single - stage , direct - to - implant reconstruction using fixed - volume or adjustable implants has become the most widely used procedure in the uk , 22 with less than 10% of patients undergoing traditional two - stage expander - implant procedures . 
this widespread adoption of mesh suggests that a randomised controlled trial attempting to compare single - stage , direct - to - implant reconstruction with mesh and the standard two - stage techniques would be difficult because of surgeon preference . 
however , our study shows little difference in the short - term clinical outcomes of biological and synthetic mesh - assisted immediate implant - based breast reconstruction , and has highlighted the large number of products in current use . 
pre - pectoral reconstruction was done only in a small number of patients in this study , although it is gaining popularity.7 despite the challenges associated with a randomised clinical trial in breast reconstruction , methods have been developed and successfully used to overcome these issues and support surgeons to recruit patients into trials of very different types of procedures , in which patient and surgeon preferences might be strong.27 although the type of reconstructive technique used does not appear to affect short - term safety outcomes , patient factors such as increased bmi and current smoking seemed to be associated with increased risks of implant loss , infection , re - admission , and reoperation . 
 although this analysis was exploratory in nature , these results highlight the importance of careful patient selection and providing patients at high risk with accurate likelihood of postoperative information about complications , to allow them to make better informed decisions . 
increase in odds for each additional body - mass index unit . table 5 : logistic regression of risk factors for key outcomes the proportion of patients identified in this study who experienced implant loss , re - admission , and infection remain un changed since the 200809 nmbra , whereas the proportion of patients requiring re - operation has more than tripled.24 the reasons for this increase are complex . 
the numbers of immediate implant - based breast recon struction have increased substantially since 200809 , 5 , 22 but there is no evidence to suggest that the indications for implant - based surgery have changed , since the proportions of patients who smoked , had diabetes , had a high bmi , or were american society of anesthesiologists grades iii / iv in our study are largely consistent with the nmbra cohort.24 increased numbers reflect more aggressive management of complications when mesh is used , re - operations could but the use of mesh does not seem to translate into a reduced percentage of implant loss . 
although the proportions of patients with implant loss and return to theatre in this study are much lower than those reported in a 2017 randomised trial , 11 , 13 they are much higher than those reported in other large prospective observational studies14 , 15 , 28 and summarised in recent systematic reviews.8 , 9 this large , multicentre study is likely to reflect real - world outcomes of immediate implant - based breast reconstruction , and highlights the need for improvement in this area . this national prospective study adds substantially to the evidence base in immediate implant - based breast reconstruction , but has several limitations . 
 264 vol 20 february 2019 articles for more on the getting it right first time initiative see co.uk / surgical - specialty / breastsurgery / notably , patients having dermal sling reconstruction had higher bmis than did those in the other groups , but other , subtler , differences might exist between patients having different procedures that were not considered in this study . 
 of particular note was the introduction of implant salvage procedures , whereby fixed - volume implants that were infected or exposed were debrided , washed out , and replaced either with a new implant or a tissue expander . 
we acknowledge that this might have overestimated the occurrence of implant infection , but reported frequencies were consistent those in the nmbra.24 clear , unambiguous definitions of outcomes will therefore be needed for future studies . 
 and previous smoking , bmi , operative radiotherapy were for factors complications in this study , and this potential association might be informative when designing subsequent randomised clinical trials as a basis for balancing randomisation . 
although this study was not powered to establish prognostic factors , and the results should be confirmed in an external validation study , consistency between these results and those in other studies29 , 30 support these findings . 
this approach would not capture complications , such as infection , which developed while patients were receiving chemotherapy or problems developing as a result of adjuvant radiotherapy , for which a longer period of follow - up would be required . identified as risk time , recruitment establish whether the findings of this large , non - randomised study strongly support the need for a randomised controlled trial in immediate implant - based breast reconstruction , and potential trial designs could include biological versus synthetic mesh or pre - pectoral versus subpectoral implant placement . 
the proportion of patients experiencing implant loss and infection and those requiring re - operation and re - admission do not appear to have improved ( ie , decreased ) since nmbra , and do not meet published quality standards . 
these factors are not immediately implant - based breast reconstruction modifiable in the short - term , but neoadjuvant chemotherapy or endocrine therapy could be used as a strategy to provide patients with breast cancer with additional time to lose weight or stop smoking before surgery . 
this approach might not be practical or ethical , and a more appropriate focus could be to develop effective strategies to help patients better understand the potential risks of surgery , to allow them to make fully informed decisions . 
however , it is important that any standardisation of care reflects evidence - based best practice , and further exploratory analysis of the ibra cohort will support this . there remains the need for high - quality evidence from a randomised controlled trial to support the best practice of immediate implant - based breast reconstruction , and the equivalence of different techniques in this nonrandomised study supports a future randomised clinical trial . 
the outcomes of immediate implant - based breast reconstruction in the uk are poor and surgeons need to commit to robust evaluation if outcomes for patients are to be improved . contributors sp , ch , st , js , jmb , ejc , prw , and lw conceived and designed the study and data collection forms . 
all authors reviewed and critically revised the manuscript and approved it before submission . declaration of interests sp , ch , prw , aj , jmb , and lw report grants from nihr research for patient benefit programme ( see below ) during the conduct of the study . 
the other authors have nothing to declare . acknowledgments this work was funded by an nihr research for patient benefit programme grant ( pb - pg - 0214 - 33065 ) and pump - priming funding from the association of breast surgery and the british association of plastic reconstructive and aesthetic surgeons . 
this work was undertaken with the support of the mrc conduct - ii ( collaboration and innovation for difficult and complex randomised controlled trials in invasive procedures ) hub for trials methodology research ( mr / k025643 / 1 ) and the nihr biomedical research centre at university hospitals bristol nhs foundation trust and the university of bristol . 
the views expressed in this publication are those of the authors and not necessarily those of the nhs , the national institute for health research , or the department of health and social care . vol 20 february 2019 articles data sharing individual participant data ( de - identified ) , the data dictionary , and the statistical analysis plan for this study will be available to researchers after methodological review of the proposed analysis plan by the ibra steering group . 
to gain access , data requestors will need to sign a data access agreement . corrections correction to lancet oncol 2015 ; 16 : 133 correction to lancet oncol 2015 ; 16 : 181 , 184 correction to lancet oncol 2015 ; 16 : 237 published online january 29 , 2015 s1470 - 2045 ( 14 ) 70483 - 8 dp . 
 radiotherapy lancet oncol 2015 ; 16 : 23739in this comment , the fth line of the third paragraph should read : by contrast , acute gastrointestinal toxicity was increased with hypofractionation [ 95% ci 372469 ] of ( 420% patients the hypofractionation group had grade 2 adverse events vs 312% [ 266358 ] in the standard fractionation di erence 108% , 90% ci 5251643 ; p = 00015 ) although were similar 3 months after treatment , and non - inferiority was not con rmed . 
these corrections have been made to the online version as of march 2 , 2015 , and have been made to the printed comment . group , cavalli f , atun r . 
lancet oncol 2015 ; 16 : 13334 in this comment , the second sentence should have been : deaths from cancer are projected to increase from the present level of around 8 million a year to more than 13 million by 2030 , with most of the burden being in poorer countries . 
this correction has been made as of jan 29 , 2015 . correction to lancet oncol 2015 ; 16 : 266 ih , williams lj , kunkler jack wjl , cameron da , dixon jm , on behalf of investigators . 
 lancet oncol 2015 ; 16 : 26673in the interpretation section of the summary , the rst sentence should read postoperative whole - breast radiotherapy after breast - conserving surgery and adjuvant endocrine treatment resulted in a signi cant but modest reduction in local recurrence for women aged 65 years or older with early breast cancer 5 years after randomisation . 
this correction has been made to the online version as o f march 2 , 2015 , and to the printed article . thomas a , rajan a , berman a , in patients with et al . 
lancet oncol 2015 ; 16 : 17786 in the key of gure 2a of this article , the text for the red line should read thymic carcinoma ( 16 / 24 failed ) and that for the blue line should read in the thymoma ( 11 / 16 failed )  . 
 key of gure 4b , the text for the red line should read no change / increase ( 0 / 18 failed ) and that for the blue line should read decrease ( 4 / 4 failed )  . 
lancet oncol 2015 ; 16 : 27483in this article , the interpretation should have read : hypofractionated radiotherapy was not non - inferior to standard fractionated radiotherapy in terms of acute genitourinary and gastrofor men with intestinal intermediate - risk high - risk and prostate cancer . 
this correction has been made to the online version as of march 2 , 2015 and to the printed article . toxicity vol 16 march 2015 e105 corrections correction to lancet oncol 2016 ; 17 : 429 therapy cristofanilli m , turner nc , bondarenko i , et al . 
fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment o f h o r m o n e r e c e p t o r p o s i t i v e , her2 - negative metastatic breast cancer that progressed on previous endocrine ( paloma - 3 ) : final analysis of the multicentre , double - blind , phase 3 randomised controlled trial . 
lancet oncol 2016 ; 17 : 42539in this article , in the outcomes subsection of the methods , the second sentence should read secondary efficacy endpoints were con rmed objective response , which was defined as complete response or partial response according to recist ; clinical benefit , which was defined as complete response or partial response or stable disease of 24 weeks duration or longer ; tumour tissue biomarkers , including genes ( eg , pik3ca mutations ) , proteins ( eg , quantitiative expression of oestrogen and progesterone receptors ) , and rna expression ; and safety including type , incidence , and severity of adverse events . 
 the decision was based on interim results of the phase 3 bellini trial , which showed an increased risk of death for patients who were treated with venetoclax and bortezomib compared with placebo ( 41 [ 211% ] deaths in 194 patients in the venetoclax group vs 11 [ 113% ] of 97 in the control group ; hazard ratio 203 [ 95% ci 104394 ] )  . 
the fdas decision raises important questions with respect to the safety of new treatments , their justification in disease settings with existing approved drugs with similar efficacy , and a growing trend in the way innovative therapies are pushed through clinical trials at breakneck speed . in the case of multiple myeloma , drug innovation is at an all - time high . 
these early decisions certainly encourage pharmaceutical innovation and facilitate patient access to new drugs , but they also reflect a worrying trend in which regulators are arguably approving drugs too soon on the basis of early - stage results or uncontrolled phase 2 data for which the efficacy or harm of the new intervention is still too unpredictable . 
additionally , regulators should be more cautious when drugs skip early - phase testing and move straight to a phase 3 trial for diseases in which there are already proven therapies . 
in the case of the bellini trial , researchers justified the investigation of venetoclax for multiple myeloma treatment based on encouraging results of the drug in chronic lymphocytic leukaemia and acute myeloid leukaemia , each of which led to breakthrough designations by the fda . 
but decisions such as these show that different diseases will ultimately respond differently to treatment , even if they show similar disease characteristics or are based on similar trial populations . 
being aware of the ultimate risks and benefits involved is a necessary first step to ensure clinical trials are being done to generate the best possible evidence needed , not to see whether the drug is effective in as many malignancies as possible to maximise commercial opportunity . indeed , involved if the risks in a recent study in enrolling patients experimental clinical trials were apportioned the correct amount of caution , then unwarranted harms such as those seen in the bellini trial might be avoided . 
 jama internal medicine , researchers found that doctors conversations with families about care for critically ill patients failed to take the time to explain the benefits and harms of treatment options and failed to address patients values and preferences . 
when patient preference is so central a concern to deliver optimal cancer care , it is crucial that those responsible for the advent of new trialssuch as funders , ethics approval committees , regulators , doctors , and investigators themselvesaccurately communicate the dangers involved so that overtly risky or futile trials are avoided , whilst still encouraging various treatment avenues that are available to the patient . somehow , the unbridled promotion of new treatments driven by industry - sponsored research , research pressures , and treatment enthusiasm , has fostered a culture in which the promise of miraculous important questions cures overshadows more surrounding the realities of the risks and harms of treatment , the evidence base used to promote their use , and the actual need for new treatment options to be available in any given setting . 
moreover , both regulators should be any and clinicians have a duty of care to ensure risks are communicated as fully and as transparently as possible , and thus ensure that patient care , best practice , and best evidence ultimately comes first . 
 the lancet oncology vol 20 may 2019 editorial corrections published online march 25 , 2015 s1470 - 2045 ( 14 ) 71115 - 5 correction to lancet oncol 2013 ; 14 : e374 correction to lancet oncol 2015 ; 16 : e163 correction to lancet oncol 2015 ; 16 : 447 , 448 weller m , p ster sm , wick w , hegi me , reifenberger g , stupp r . 
the rst sentence should read : exposure to passive smoke among never smokers does not seem to increase the chances of acquiring somatic mutations in genes linked to non - small - cell lung cancer in smokers , a new study shows . 
 vorinostat in patients with advanced malignant pleural mesothelioma who have progressed on previous chemotherapy ( vantage - 014 ) : a phase 3 , double - blind , randomised , placebocontrolled trial . 
lancet oncol 2015 ; 16 : 44756in the a liation section , p bass should be listed at netherlands in the funding cancer section in the summary and in the a liations , merck & co has been changed to merck & co , inc . 
 lancet oncol 2015 ; 16 : 54149in the key of gure 2 of this article , the boxes should indicate patients who were ct positive for disease , not those who were circulating tumour dna positive for disease . 
this correction has been made to the online version as of april 30 , 2015 , and the printed version is correct . vol 16 may 2015 e199 published online august 8 , 2018 s1470 - 2045 ( 18 ) 30498 - 4 see articles page 1159 increasing incidence of cancer in children and competing risks the automated childhood cancer information system ( accis ) has been registering data on cancer occurrence from birth to age 20 years in most european countries since the 1970s . 
in the lancet oncology , eva steliarova - foucher and colleagues1 report the latest accis data analysis trends for the period 19912010 for malignant neoplasms in children aged 014 years and adolescents aged 1519 years . 
first , cancer incidence in children aged 014 years has gradually increased over the 19912010 period.1 increasing incidence was observed for all cancers ( 054% ( 95% ci 044 to 065 ) per year ) , leukaemia ( 066% [ 048 to 084 ] per year ) , lymphoma ( 026% [ 001 to 054 ] per year ) , cns malignant tumours ( 049% [ 020 to 077 ] per year ) , and other cancers ( 056% [ 040 to 072 ] per year )  . 
second , for all five cancer categories investigated , incidence increases were similar in all four regions . remain the accis data reinforce the notion that the slow but steady increase in the incidence of many childhood cancers reported since the 1970s is real , and that it is particularly notable for leukaemia.24 unfortunately , epidemiological studies so far have not identified clear risk factors for childhood cancer . 
however , relating the accis data to the tremendous changes in environmental , living , socioeconomic , and public health conditions in european countries after world war 2 might provide clues as to the nature of these reasons . 
if improvements in medical imaging technology were the reason underlying the increased incidence trends of tumours of the cns , then a lower incidence of these tumours should have been observed in the early 1990s in east europe compared with west europe , with a catch up in incidence afterwards . 
however , incidence and incidence trends observed trends from 1991 to 2010 were about the same in east europe and west europe.1 another contrast across european regions concerns the use of pesticides in agriculture . 
in 2014 , the quantities of pesticide sales per capita were about three times greater in spain , italy , and france than in sweden or the uk.5 if increasing cancer incidence trends were due to pesticides , dissimilarities in incidence trends for leukaemia and lymphoma would be expected between european regions , which was not the case.1 a search for marked changes in health events specific to all european children rapidly identifies the dramatic decreases in mortality of children younger than 15 years after world war 2 . 
for example , infant mortality in europe ranged from 160775 deaths per 1000 newborns in 1960 and dropped to 2398 deaths per 1000 newborns in 2010a decrease of 44% per year on average.5 this phenomenon leads to the hypothesis that the death of some children before they reached a certain age precluded the occurrence of cancer by that age . 
death would represent a competing risk ( or event ) in the sense that cancer can no longer occur after death.6 furthermore , children who would have died could also have been at higher risk of cancer for two possible reasons . 
these hypotheses assume that if a child escapes death either because he or she has been protected against potentially deadly diseases ( eg , by vaccination or improved living conditions ) or has survived its occurrence ( eg , because of efficient therapy ) , then the risk of cancer occurrence would be greater in this child than in other children . 
this hypothesis could explain why the peak incidence of leukaemia has shifted towards younger ages over time.4 , 7 steadily decreasing mortality in the months following birth would increase the number of younger children at higher risk for leukaemia . the competing risk hypothesis essentially rests on ecological observations . 
lancet 2004 ; 364 : 2097105 . bevacizumab therapy for recurrent gliomas : another disappointment ? in their article in the lancet oncology , martin van den bent and colleagues1 report on their clinical trial of bevacizumab in the treatment of recurrent grade ii and iii gliomas , and they report the effects of this treatment on overall survival , progression - free survival , quality of life , toxicity , and neurocognitive function . 
 their study was designed as a phase 2 trial and therefore was not powered to show a definite advantage of bevacizumab in these patients , although a high number of patients ( n = 155 ) were enrolled and randomly allocated to the two treatment groups ( temozolomide plus bevacizumab or temozolomide monotherapy )  . 
 to our knowledge , this is the largest study on the use of bevacizumab , with the highest quality data , in patients with recurrent who grade ii and iii gliomas . bevacizumab was previously regarded as a promising new chemotherapeutic drug for the treatment of gliomas . 
 several large trials that used considerable resources were therefore done , although the findings from the study by van den bent and colleagues is mostly in line with the available data on bevacizumab in the treatment of gliomas . 
the authors found no evidence of improved overall survival with bevacizumab and temozolomide combination therapy versus temo zolomide monotherapy : overall survival at 12 months was achieved by 44 ( 61% [ 80% ci 5369 ] ) of 72 patients in the monotherapy group and 38 ( 55% [ 4769 ] ) of 69 in the combination group . 
the results of the study by van den bent and colleagues are disappointing and continue the pattern of failed clinical trials of bevacizumab , which was thought to be a silver bullet in the treatment of intrinsic brain tumours , but which now seems confirmed to be an ineffective chemotherapeutic drug for this indication.24 validated treatment options for recurrent intrinsic brain tumours are scarce . 
although surgery has become more aggressive in the past 1015 years ( an approach that is not supported by robust evidence ) , potent and effective therapeutic drugs for treatment of recurrent tumours are not available.5 , 6 notably , bevacizumab treatment provided no benefit in the secondary efficacy outcomes of this trial , and side - effects were more common in patients receiving bevacizumab . 
despite its failure to improve overall survival , bevacizumab is still used as an adjunct therapy because of its supposed anti - oedematous effects and reported improvements in progression - free survival of patients with glioblastomas.7 it is of note that these anti - oedematous effects and improvements to progression - free survival were only measured by mri ; however , molecular imaging methods such as aminoacid positron emission tomography scans could reveal different tumour progression or overall response to treatment than is shown by mri alone.8 if bevacizumab has a substantial effect on tumour progression and oedema in patients with glioblastoma that outweighs its side - effects , this effect was not shown in patients with who grade ii and iii gliomas in the study by van den bent and colleagues . 
there are several possible published online august 13 , 2018 s1470 - 2045 ( 18 ) 30601 - 6 see articles page 1170 vol 19 september 2018 1137 comment corrections correction to lancet oncol 2014 ; 15 : 1280 correction to lancet oncol 2014 ; 15 : 310 , 311 boughey jc . 
how do the amaros trial results change practice ? lancet oncol 2014 ; 15 : 128081the last sentence of the fourth paragraph of this comment should read with both the amaros1 and z00112 , 3 studies , the data interpreted should be with caution and should not be extrapolated to patients with three , four , or more positive sentinel lymph nodes . 
this correction has been made to the online version as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e395403 weller m , van den bent m , hopkins k , et al , for the european association for neuro - oncology ( eano ) task force on malignant glioma . 
 lancet oncol 2014 ; 15 : e395403 the appendix of this review was incorrect ; the correct appendix has been uploaded as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e591 furlow b . 
 this correction has been made to the online article as of nov 24 , 2014 . conroy t , galais m - p , raoul j - l , et al , for the fdration francophone de cancrologie digestive and unicancer - gi group . 
de nitive chemo radiotherapy with folfox versus uorouracil and cisplatin in patients with oesophageal cancer ( prodige5 / accord17 ) : final results of a randomised , phase 2 / 3 trial . 
the last sentence of the eighth paragraph in the results section should read an endoscopic complete response at week 15 was achieved in 61 ( 53% ) of 115 patients in the folfox group versus 57 ( 48% ) of 120 patients in the uorouracil plus cisplatin group . 
folfox = uorouracil , leucovorin , and oxaliplat recist = response evaluation criteria in solid tumours.21 * 115 patients assessable in the folfox group and 120 assessable in the uorouracil and cisplatin group . table 2 : tumour response to treatment correction to lancet oncol 2014 ; 15 : 1464 sestak i , singh s , cuzick j , et al . 
changes in bone mineral density at 3 years in postmenopausal women receiving anastrozole and risedronate in the ibis - ii bone substudy : an international , doubleblind , randomised , placebo - controlled trial . 
this correction has been made to the online version as of nov 24 , 2014 , and the printed version is correct . c lumbar spine d total hip 05 10 15 20 25 30 35 40 45 50 12% 40% 18% 40% anastrozole placebo baseline 12 months anastrozole placebo 36 months baseline 12 months 36 months vol 15 december 2014 e587 correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections correction to lancet oncol 2019 ; 20 : 23953 ipilimumab scherpereel a , mazieres j , greillier l , et al . 
nivolumab or nivolumab plus patients with relapsed malignant pleural mesothelioma ( ifct - 1501 maps2 ) : a multicentre , open - label , randomised , non - comparative , phase 2 trial . 
 lancet oncol 2019 ; 20 : 23953in figure 4b of this article , the position of the plotted kaplan - meier curves on the y axis has been corrected , affecting the overall survival readings . 
 this correction has been made to the online version as of march 1 , 2019 correction to lancet oncol 2019 ; 20 : 36170 saad ed , squifflet p , burzykowski t , et al . 
 disease - free survival as a surrogate for overall survival in patients with her2positive , early breast cancer in trials of adjuvant trastuzumab for up to 1 year : a systematic review and meta - analysis . 
 lancet oncology 2019 ; 20 : 36170 in the summary of this article , the fourth sentence of the findings section should read subgroups defined by nodal status and hormone receptor status yielded qualitatively similar results . 
this correction has been made to the online version as of march 1 , 2019 , and the printed article is correct . vol 20 march 2019 e132 corrections corrections correction to lancet oncol 2014 ; 15 : 1324 correction to lancet oncol 2015 ; 16 : 324 correction to lancet oncol 2015 ; 16 : 499508 zapatero a , guerrero a , maldonado x , et al . 
high - dose radiotherapy with shortterm or long - term androgen deprivation in localised prostate cancer ( dart01 / 05 gicor ) : a controlled , randomised , phase 3 trial . 
in the fth paragraph in the results section , the number of patients in the short - term group who died of cancer , but not of the prostate , should read 14 ( 8% ) and the number in the long - term group should read three ( 2% )  . 
ramucirumab versus placebo second - line folfiri in patients with metastatic colorectal carcinoma that progressed during or after rst - line therapy with bevacizumab , uoropyrimidine ( raise ) : a randomised , double - blind , multicentre , phase 3 study . 
 lancet oncol 2014 ; 15 : 131931in gure 3 of the article , the prevalence of hpv type 18 in oral cavity in africa should read 18% , and in oropharynx in oceania hpv type 18 should appear as the second most common type after 16 , and before 35 , with a prevalence of 17% . 
 vol 16 june 2015 e262 published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections editorial for the study of necitumumab in lung cancer see articles page 328 for the study in the journal of the national cancer institute see j natl cancer inst 2014 ; doi : 10.1093 / jnci / dju302 rethinking trial eligibility in the ncd era patient eligibility represents one of the most challenging factors in the design of a clinical trial . 
in this issue of the lancet oncology , a study of necitumumab plus pemetrexed and cisplatin for rst - line treatment of patients with non - small - cell lung cancer lists one of its exclusion criteria as patients having symptomatic brain metastases , despite this being a common occurrence in this setting . 
an article in the november , 2014 , issue of the journal of the national cancer institute reported that up to 18% of patients are not permitted to participate in clinical trials because of previous cancer diagnoses . 
 this bias towards accruing patient populations that maximise the apparent bene ts of a treatment highlights an important issue at the heart of clinical trial design that will become more prevalent as the number of cancer survivors , and people living longer with conditions considered to be chronic diseases , increases . the practice of excluding patients with previous cancer diagnoses is based on the assumption that this population are more likely to be less t , less likely to tolerate or respond to treatment , more prone to develop clinical or radiological changes that may not be attributable to the index disease , carry comorbidities , and have di erent survival rates than those with a rst - time diagnosis of cancer . 
in fact , in the journal of the national cancer institute article , the authors conclude that patient outcomes can be as good asor even better thanthose of patients with no previous cancer diagnosis , possibly because of more intensive clinical and radiographic surveillance during follow - up of the primary cancer , resulting in an earlier diagnosis of the secondary cancer . 
moreover , these exclusions hinder attempts to increase patient participation in oncology clinical trialsparticularly concerning when around one in ve adult cancer trials closes early for reasons unrelated to the safety or e cacy of the intervention , with poor accrual being the most common cause . 
factors such as age , sex , concomitant medication use , and comorbidities ( most notably hiv , and liver and renal diseasewhich are now generally considered to be manageable , chronic conditions ) , are all common barriers to patient enrolment , which could , in turn , prevent fair access to cutting - edge treatments for these groups of patients . 
 but , is exclusion of these patient populations really justi ed ? and is their omission right , ethically ? all trials must have an a - priori protocol and analysis plan in place before patient accrual , and thus theoretically there is no reason why trial designs could not include strati cation factors related to these inclusion and exclusion criteria , and carry out subgroup analyses to take them into account . 
with the ageing population and increasing burden of non - communicable diseases , the validity of extrapolating existing evidence , based on results from younger , healthier populations , becomes increasingly disconnected from the realities in the target population . as treatment outcomes continue to improve for all diseases , not just cancer , it is inevitable that the incidence of patients with chronic diseases will continue to rise . 
if study investigators are able to strike a balance between accruing patient populations that are representative of the general population , and accruing patient populations that will not be prone to major losses or who have comorbidities that might a ect the clinical outcome of their study , then widening lead to improved patient eligibility criteria could patient accrual , higher completion rates , and greater treatment equity . 
 nivolumab monotherapy in recurrent metastatic urothelial carcinoma ( checkmate 032 ) : a multicentre , openlabel , two - stage , multi - arm , phase 1 / 2 trial . 
lancet oncol 2016 ; 17 : 159098 in this article , the declaration of interests should read psh has received fees for advisory board participation for jounce and kite ; fees for consultancy from jounce , kite , bristol - myers squibb , astrazeneca , and amgen ; and stock or stock options from jounce and kite . 
eca reports research grants and / or financial support from boehringer ingelheim , roche / genentech , bristol - myers squibb , novartis , psioxus , nanobiotix janssen , abbvie , pharmamar , puma , sanofi , lilly , pfizer , merck , nektar , amcure , amgen , astrazeneca , principia , bayer , cytomx , h3 , incyte , kura , loxo , macrogenics , menarini , merck serono , merus , millenium , rigontec , tahio , and beugene tesaro ; consultancy fees from janssen - cilag , alkermes ( and travel expenses ) , seattle genetics , pierre fabre , cerulean pharma , eusa , celgene , novartis ( speakers bureau ) , nanobiotix , psioxus therapeutics , abbvie , astrazeneca , guidepoint global , roche / genentech ( and travel expeneses ) , glg , pfizer , servier , amcure , and boehringer ingelheim ; ownership from start ( leadership ) , oncoarts associated and international cancer consultants ; and employment from start and hm hospitals group ( honoraria ) and president and founder of npo foundation intheos ( investigational therapeutics oncological sciences ) , outside the submitted work . 
fdb has received consultancy fees from tiziana life sciences , bristol - myers squibb , msd , servier , eli lilly , merck serono , glaxosmithkline , and novartis , and speaker fees from bristol - myers squibb , eli lilly , roche , and accmed . 
mm has received consultancy fees from etubics and boehringer ingelheim , and speaker fees from genentech , novartis , sanofi , regeneron , lexicon , ipsen , onyx , bayer , taiho , merrimack , and celgene . 
 dj has received consulting fees from definiens , f hoffmann - la roche , curevac , roche pharma , novartis pharma , and novartis oncologynovartis farma , outside the submitted work ; and has a patent issued for intellectual property of infiltrating t - cell density predicting outcome . 
 ech has received grants from bristolmyers squibb and consultancy fees for advisory board participation from emd serono , taiho , bayer , advaxis , amgen , lilly , and castle biosciences . 
jer has received grants for study conduct from novartis ; funds for clinical trial conduct from astellas , seattle genetics , bayer , astrazeneca , mirati therapeutics , oncogenex , and roche / genentech ; has received consultancy fees from roche / genentech , astrazeneca , eli lilly , astellas , seattle genetics , bristol - myers squibb , merck , emd - serono , adicet bio , western oncolytics , pharmacyclics , sensei biotherapeutics , bayer , bioclin therapeutics , qed therapeutics , mirati therapeutics , fortress biotech , inovio ; has gritstone oncology , received honoraria from bristol - myers squibb and chugai ; has held stock in illumina and merck . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2017 ; 18 : 90416 baselga j , im s - a , iwata h , et al . 
buparlisib plus fulvestrant versus placebo plus fulvestrant in postmenopausal , hormone receptor - positive , her2 - negative , advanced breast cancer ( belle - 2 ) : a randomised , double - blind , placebocontrolled , phase 3 trial . 
lancet oncol 2017 ; 18 : 90416in this article , the declaration of interests should read jb has received reimbursement for travel , and advisory board and consulting fees from novartis , during the conduct of the study ; has received personal fees and held stock as a member of the board of directors from aura biosciences ; has received personal fees as a member of the advisory board and held stock as a founder of northern biologics ( f / k / a mosaic biomedicals ) ; has received personal fees and held stock as a member of the board of directors from infinity pharmaceuticals ; held stock as a member of the advisory board from apogen biotechnologies ; has received personal fees and held stock as a member of the advisory board from pmv pharma ; has received personal fees and held stock as a member of the advisory board from juno therapeutics ; has received personal fees and held stock as co - founder from tango ( f / k / a synthetic lethal ) ; has received personal fees and held stock as a member of the scientific advisory board and the board of directors from grail ; has received personal fees and held stock as a member of board of directors from varian medical systems ; held stock as a member of board of directors from foghorn therapeutics ; has received reimbursement for travel , e71 vol 20 february 2019 corrections corrections correction to lancet oncol 2014 ; 15 : 1189 correction to lancet oncol 2014 ; 15 : 1263 dahut wl , madan ra . 
lancet oncol 2014 ; 15 : 118890in this comment , the fourth sentence of the third paragraph should read response in addition assessment was confounded because follow - up imaging was done at the discretion of the treating clinician . 
 this correction has been made to the online version as of oct 27 , 2014 . to safety , cn , prostate castellano sternberg daugaard g , et al , for the abiraterone global eap investigators . 
 pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
this correction has been made to the online version as of dec 29 , 2017 . vol 19 january 2018 corrections correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections corrections published online june 12 , 2015 s1470 - 2045 ( 15 ) 00056 - x correction to lancet oncol 2015 ; 16 : e227 correction to lancet oncol 2015 ; 16 : 738 correction to lancet oncol 2015 ; 16 : 747 schiller jh . 
 antibodies lancet oncol 2015 ; 16 : 73839in this comment , the chemotherapy backbone used in the squire trial was incorrectly referred to as gemcitabine and carboplatin in four instances in the third paragraph ; it should read gemcitabine and cisplat these corrections have been made to the online version as of june 29 , 2015 , and the printed version is correct . torri v , broggini m , garassino mc . 
lancet oncol 2015 ; 16 : 74648the seventh sentence of the nal paragraph of this comment should read : results for leu858arg are still inconclusive because although progression - free survival is higher in patients given all egfr inhibitors versus chemotherapy , overall survival seems to be better with chemotherapy than with afatinib for these patients . 
 this correction has been made to the online version as of june 29 , 2015 , and the printed version is correct . for future lowy dr , herrero r , hildesheim a , for the participants in the iarc / nci workshop on primary endpoints for prophylactic hpv vaccine trial . 
 lancet oncol 2015 ; 16 : e22633 in the panel , in the section on the quadrivalent vaccine for men , the second bullet point should read : approved in the eu by the ema for the prevention of vaccine - type related anal lesions and for the prevention of vaccine - type related genital warts ( ages 9 )  . 
lancet oncol 2015 ; 16 : this news e316in item , the nal two sentences of paragraph 3 read : according to the scale , treatment late - stage egfr - mutated nonsquamous lung cancer with erlotinib provides a gain in progression - free survival ( pfs ) of 85 months ( hazard ratio [ hr ] 016 [ 95% ci 010026 ] ) and an improvement in quality of life compared with carboplatin and gemcitabine , earning an esmo - mcbs score of 4 / 5 . 
in contrast , the same drug when used to treat metas tatic pancreatic cancer provides an overall gain of only 9 days compared with chemotherapy treatment , and had a score of 1 / 5 . 
this correction has been made as of june 12 , 2015 . vol 16 july 2015 e313 correction to lancet oncol 2017 ; 18 : e35463 correction to lancet oncol 2018 ; 19 : 87100 correction to lancet oncol 2018 ; 19 : 25766 oconnor oa , lue jk , sawas a , et al . 
 for lancet oncol 2017 ; 18 : e35463 in this review , the second sentence of the abstract should read additional improvements have been reported in three phase 3 colon cancer trials when oxaliplatin was added to fluoropyrimidines , the effect was mainly on disease - free survival . 
this correction has been made to the online version as of feb 28 , 2018 although women fulvestrant johnston s , lee ks , et di leo a , al . 
buparlisib plus with postmenopausal her2hormone - receptor - positive , negative , advanced breast cancer progressing on or after mtor inhibition ( belle - 3 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
in the results section , the following sentence should have read in the 11 ( 13% ) cases of discordance , a pik3ca wild - type tumour sample and pik3ca - mutated ctdna were reported in three ( 4% ) patients and pik3ca mutations detected in the tumour sample but not in ctdna ( 9% ) patients . 
these corrections have been made to the online version as of feb 28 , 2018 . seven vol 19 march 2018 e137 corrections published online july 9 , 2018 s1470 - 2045 ( 18 ) 30419 - 4 see articles page 1027 non - invasive image - guided targeted drug delivery actively targeted and triggered drug delivery systems to enhance tumour drug uptakesuch as liposomes and other nanoparticleshave been the subject of intensive research for several decades , but so far have not shown therapeutic benefit in clinical trials.1 in the lancet oncology , paul c lyon and colleagues report for the first time in humans the ability to non - invasively enhance drug delivery by triggered chemotherapy release from heat - activated liposomes , while also suggesting a therapeutic response to this enhanced delivery.2 notably , local delivery was triggered non - invasively by focused ultrasound . 
the study used thermosensitive liposomesa type of stimuliresponsive drug delivery system in which release of the encapsulated drug is triggered by mild hyperthermia ( > 395c ) , which was first proposed in the late 1970s.3 since then , several drugs have been encapsulated in thermosensitive liposomes in preclinical studies , with doxorubicin being the most widely used drug.4 combined with an image - guided heating device , thermosensitive liposomes allow targeted drug delivery to a tissue volume defined by medical imaging . lyso - thermosensitive the formulation used in the study by lyon and colleaguestermed liposomal doxorubicin ( ltld ) was developed in the early 2000s.5 this formulation has been the subject of clinical trials as adjuvant radiofrequency in combination with ablation to treat primary and metastatic liver cancer.6 , 7 the first phase 3 trial assessing this combination was unsuccessful , although a post - hoc analysis suggested treatment benefit in a subgroup of patients ; 7 a follow - up trial is ongoing . 
furthermore , tumour drug uptake was not quantified . by contrast , the study by lyon and colleagues exclusively used targeted drug delivery with ltld as therapy , allowing the direct observation of therapeutic response . 
 by quantifying drug uptake in tumour biopsy samples , this study showed for the first time the ability to noninvasively enhance local chemotherapy delivery with thermosensitive liposomes in patients with solid tumours.2 hyperthermia exposure was targeted externally by focused ultrasound.8 image - guided , high - intensity within the past few years , focused ultrasound has become clinically available for high temperature exposures ( thermal ablation ) to treat cancer and other indications , but it is also ideally suited to activate thermosensitive liposomes for targeted drug delivery at lower temperatures ( mild hyperthermia of > 395c )  . 
in the lyon and colleagues study , 19 ( 41% ) of 46 patients had inaccessible tumours , most presumably because of interference by the ribcage ; future focused ultrasound technology advances might expand accessibility . 
 the combination therapy of focused ultrasound liposomes can hyperthermia and thermosensitive facilitate non - invasively targeted and image - guided drug delivery , as shown in numerous preclinical studies , with enhancement of tumour drug uptake in the range of about 520 times.8 by comparison , lyon and colleagues showed that tumour drug uptake was enhanced by 37 - times when focused ultrasound hyperthermia was used , compared with treatment without heating.2 this increase translated into a partial response by modified choi criteria in six ( 67% ) of nine radiologically analysed target tumours , compared with only three ( 19% ) of 16 control tumours . there are areas in which the approach by lyon and colleagues might be further improved . 
in most patients , tumours were only partly exposed to hyperthermia ( and , presumably , to the drug ) , suggesting that an improved hyperthermia device or heating strategy is necessary , especially for larger tumours . 
the large observed variability in drug concentration after hyperthermia is probably partly due to the variability in hyperthermia temperature and duration , because thermosensitive liposome release is 1000 vol 19 august 2018 comment highly sensitive to small temperature changes , 4 whereas temperatures above approximately 44c might reduce perfusion and therefore diminish drug delivery . 
for example , magnetic resonance thermometry is commonly used in combination with focused ultrasound to non - invasively provide real - time temperature maps.8 notably , the duration of hyperthermia required to achieve an optimal clinical response still needs to be established . 
even preclinical studies used widely varying heating durations , from 2 min to 60 min , 4 , 8 and this duration is now known to directly dictate the amount of drug that is delivered.9 nevertheless , lyon and colleagues study represents a first important step towards clinical translation of this elegant targeted drug delivery approach , by locally enhance drug demonstrating the ability to uptake , while showing therapeutic response with a drug that traditionally had low efficacy in liver cancer . 
although the investigators showed the safety , feasibility , and therapeutic potential of ltld in patients with liver cancer , the described focused ultrasound plus ltld approach might be more widely applicable to other solid tumours because doxorubicin is a wide - spectrum antitumour drug . 
in that regard , a recently initiated phase 1 trial of focused ultrasound plus ltld will treat various refractory solid tumours in paediatric patients.10 dieter haemmerich medical university of south carolina , charleston , sc 29425 , usa haemmer@musc.edu dh is a shareholder of medical engineering innovations , has the patent electrode array for tissue ablation licensed to medical engineering innovations , the patent radiofrequency ablation system using multiple prong probes issued , and the patent radio - frequency ablation system using multiple electrodes licensed to medtronic with royalties paid . copyright the author ( s )  . 
safety and feasibility of ultrasound - triggered targeted drug delivery of thermosensitive liposomal doxorubicin in liver tumours ( tardox ) : a single - centre , open - label , phase 1 trial . 
phase 1 trial of lyso - thermosensitive liposomal doxorubicin ( ltld ) and magnetic resonance guided high intensity focused ultrasound ( mr - hifu ) for pediatric refractory solid tumors . 
proc am soc clin oncol 2017 ; 35 ( suppl 15 ) : tps10579 . convection - enhanced delivery : chemosurgery in diffuse intrinsic pontine glioma diffuse intrinsic pontine glioma is a devastating highgrade brain cancer mostly diagnosed in children . 
due to its deep - seated , intrinsic location in the brainstem and the diffusely infiltrating nature of the glioma cells , local disease control by neurosurgical resection is not an option for these patients . 
radiotherapy , often combined with concurrent chemotherapy is palliative , with 1 - year , 2 - year , and 5 - year overall survival of 423% , 96% , and 22% , respectively.1 multiple clinical trials investigating systemic cytotoxic chemotherapy and novel agents have thus far not changed these poor overall survival rates.2 , 3 in most solid cancers , as well as in high - grade gliomas located in other parts of the brain , extensive safe surgery is an essential determinant of disease control , often in combination with adjuvant ( or neoadjuvant ) chemotherapy , radiotherapy , or both . 
in diffuse intrinsic pontine glioma , the presence of vital structures in the pons , such as the cranial nerve nuclei , the pneumotaxic and apneustic ( breathing ) centre , and the passage of corticospinal and corticocerbellar motor tracts impede the possibility of extended resection of the tumour without severely affecting vital functioning . 
currently , the standard treatment for patients with vulval intraepithelial neoplasia is surgery , but this approach does not guarantee cure and can be dis guring , causing physical and psychological problems , particularly in women of reproductive age . 
we aimed to assess the activity , safety , and feasibility of two topical treatments cidofovir and imiquimodas an alternative to surgery in female patients with vulval intraepithelial neoplasia . methods we recruited female patients ( age 16 years or older ) from 32 centres to an open - label , randomised , phase 2 trial . 
we randomly allocated patients to topical treatment with either 1% cidofovir ( supplied as a gel in a 10 g tube , to last 6 weeks ) or 5% imiquimod ( one 250 mg sachet for every application ) , to be self - applied three times a week for a maximum of 24 weeks . 
randomisation ( 1 : 1 ) was done by strati ed minimisation via a central computerised system , with strati cation by hospital , disease focality , and presentation stage . 
the primary endpoint was a histologically con rmed complete response at the post - treatment assessment visit 6 weeks after the end of treatment ( a maximum of 30 weeks after treatment started )  . 
this trial is registered with current controlled trials , isrctn 34420460 . findings between oct 21 , 2009 , and jan 11 , 2013 , 180 participants were enrolled to the study ; 89 patients were randomly allocated cidofovir and 91 were assigned imiquimod . 
at the post - treatment assessment visit , a complete response had been achieved by 41 ( 46% ; 90% ci 370553 ) patients allocated cidofovir and by 42 ( 46% ; 372553 ) patients assigned imiquimod . 
adverse events of grade 3 or higher were reported in 31 ( 37% ) of 84 patients allocated cidofovir and 39 ( 46% ) of 84 patients assigned imiquimod ; the most frequent grade 3 and 4 events were pain in the vulva , pruritus , fatigue , and headache . interpretation cidofovir and imiquimod were active , safe , and feasible for treatment of vulval intraepithelial neoplasia and warrant further investigation in a phase 3 setting . 
open access article distributed under the terms of cc by . introduction vulval intraepithelial neoplasia is a chronic pre malignant disorder that a ects the vulval skthe age - standardised incidence is about one case per 100 000 women per year , with a peak at 3049 years of age , and incidence has been rising over recent decades.1 , 2 vulval intraepithelial neoplasia is graded as 1 , 2 , or 3 according to the proportion of the epithelium containing undi erentiated cells , with grade 3 disease showing full thickness neoplasia.3 symptoms can be severe and include pain , itching , and dyspareunia , with treatment generally needed on these grounds alone.4 the disorder might be related to lichen sclerosus.5 more than 80% of women with vulval intraepithelial neoplasia have lesions associated with high - risk types of human papillomavirus ( hpv ) , most typically hpv type 16 . 
 persistent infection with high - risk types of hpv typically precedes deregulation of viral gene expression , leading to increased amounts of e6 and e7 oncoproteins and resulting in loss of activity of the tumour - suppressor proteins p53 and rb , respectively . 
the rate of progression to invasive disease is di cult to estimate , because most patients undergo surgery to remove lesions , but it can be up to 5% per year , or 12% a year with surgery.6 spontaneous regression happens in 12% of patients and vol 15 november 2014 1361 articles usually takes place within the rst 10 months.6 surgery ( either excision or ablation ) is the standard treatment , but this approach can be associated with substantial morbidity , 4 , 7 and recurrence is high ( 3060% ) .8 alternatives to surgery for vulval intraepithelial neoplasia are needed , and topical drugs and systemic treatments ( eg , photodynamic therapy and immunotherapy ) have been investigated . 
in previous small studies of topical imiquimod ( n15 ) , a complete response was reported in 28 ( 41% ) of 67 women with vulval intraepithelial neoplasia , but with substantial variation among studies ( 073% ) .1116 we aimed to assess the activity , safety , and feasibility of cidofovir and imiquimod in the randomised trial of topical treatment in women with vulval intraepithelial neoplasia ( rtvin ) , an open - label , randomised phase 2 trial developed in the uk on behalf of the uks national cancer research institute . methods study design and patients we did an open - label , randomised phase 2 trial at 32 teaching and general hospitals located in wales and england ( appendix p 3 )  . 
we included female patients who were age 16 years or older , had biopsy - proven vulval intraepithelial neoplasia grade 3 ( including visible perianal disease not extending into the anal canal ) within the past 3 months , and had at least one lesion that could be measured accurately with either a longest diameter of at least 20 mm or an area greater than 120 mm ( ascertained by measurement of two perpendicular dimensions )  . 
 about halfway through recruitment ( sept 28 , 2011 ) , we expanded the inclusion criterion for size of lesion from at least one lesion with longest diameter of at least 20 mm to that described , to allow more patients to be entered into the study while ensuring that all lesions would be of su cient size to allow a biopsy specimen to be taken . 
clinicians with a special interest in vulval intraepithelial neoplasia recruited the participants . we excluded early invasive disease by clinical and vulvoscopic examination ( and , if necessary , biopsy ) , which was done by skilled clinicians . 
we also excluded pregnant women ( by measurement of human chorionic gonadotropin in urine ) and patients with impaired renal function ( de ned as serum creatinine > 133 mol / l )  . 
 moreover , we excluded individuals who had received active treatment for vulval intraepithelial neoplasia within the previous 4 weeks or who had a recorded failure on imiquimod or cidofovir after treatment three times a week for a minimum of 12 weeks . 
we obtained appropriate regulatory approval from the uk medicines and healthcare products regulatory agency ( 21323 / 0020 / 001 - 0001 ) , the o ce for research ethics committees northern ireland ( 08 / nir03 / 82 ) , and nhs research and development departments at participating sites . randomisation and masking we randomly allocated patients in a 1 : 1 ratio to topical treatment with either imiquimod or cidofovir via a vol 15 november 2014 articles central computerised system by strati ed minimisation ( with an 80 : 20 random element )  . 
furthermore , masking was not possible because cidofovir gel has a very di erent appearance from imiquimod . procedures a licensed pharmaceutical unit ( st marys pharmaceutical unit [ smpu ] , cardi & vale university health board ) converted commercially available intravenous cidofovir into 1% topical gel ( the same concentration as used in the pilot study ) , 10 which was supplied to recruiting centres in 10 g tubes . 
we asked patients allocated cidofovir to spread a thin layer of the gel over the whole a ected area three times a week for a maximum of 24 weeks , with every 10 g tube to last about 6 weeks , requiring four tubes in total . 
we asked patients assigned imiquimod to spread the contents of one sachet ( 250 mg ) over the whole a ected area three times a week for a maximum of 24 weeks , requiring 72 sachets in total . 
we advised patients to apply the treatment at night and wash with aqueous cream and water the next day . if the patient was unable to tolerate three applications per week , we allowed them to reduce the dosage by one application a week , then two applications if intolerance continued . 
if new lesions arose during the trial they were also treated , but we did not include them in the assessments . at baseline , we recorded the patients medical history , did a clinical assessment of the lesion with adapted response evaluation criteria in solid tumors ( recist ; appendix pp 12 ) , did a pregnancy test , assessed toxic e ects with the national cancer institutes common terminology criteria for adverse events ( ctcae ) version 3.0 , analysed urine for protein , and did a 4 mm punch biopsy for hpv testing . 
 reporting of serious adverse events was real - time until 30 days after the last participant received their last dose of treatment . we assessed patients at 6 , 12 , 18 , and 24 weeks of treatment . 
 * included if at least one patient had an event of grade 3 or higher , or if grade 12 toxic e ects in more than 10% of the population were present in any column . table 2 : adverse events at baseline cidofovir ( n = 89 ) imiquimod ( n = 91 ) patients meeting 6 - week adherence endpoint 78 ( 88% ) 78 ( 86% ) patients with all four record cards completed * 50 ( 56% ) 37 ( 41% ) 17 ( 1618 ) 16 ( 1418 ) first 6 weeks of the study lost to follow - up withdrew from treatment ( intolerance or patients choice ) incomplete record card number of treatment applications during the 24 - week treatment stage lost to follow - up withdrew from treatment ( intolerance or patients choice ) clinician stopped treatment because of complications stopped early , progression stopped early , complete response incomplete record card number of treatment applications data are number of patients ( % ) or median ( iqr )  . 
 * record cards completed at 6 , 12 , 18 , and 24 weeks . table 3 : treatment adherence and reasons for stopping treatment 675 ( 6471 ) 630 ( 5067 ) ( de ned by adapted recist )  . 
we also took two 4 mm biopsy specimens to assess histological response and for hpv testing , and we obtained blood samples for measurement of haemoglobin , white blood cell count , urea , and electrolytes . 
if more than one lesion was present , we took the biopsy specimen from the same lesion as the original diagnostic biopsy ( and other lesions if judged clinically necessary )  . 
if no lesion was visible at the post - treatment assessment visit , we took a biopsy specimen from the same site as the original diagnostic biopsy . we followed up patients who had a histological complete response at the post - treatment assessment visit every 6 months ( at 6 , 12 , 18 , and 24 months )  . 
we also took blood samples at baseline , at 6 weeks of treatment , and at the post - treatment assessment visit , and we banked these specimens for future translational research . the 24 - week if a participant had a complete response or disease progression ( de ned by adapted recist ) at any time during treatment stage , we stopped treatment and did the post - treatment assessment visit 6 weeks later . 
patients who had stable disease or disease progression ( by adapted recist ) at the post - treatment assessment visit , for whom invasive disease had been ruled out , were eligible for crossover to the alternate treatment for a maximum of 24 weeks . 
subsequent management beyond the post - treatment assessment visit in patients without a complete response was at the discretion of the treating clinician . outcomes the primary endpoint was a histologically con rmed complete response in baseline lesions at the post - treatment assessment visit ( 6 weeks after completion of treatment , a maximum of 30 weeks after the start of treatment )  . 
secondary endpoints were adherence to the dosing regimen at 6 weeks and 24 weeks during the treatment stage ( to assess feasibility ) , toxic e ects during the 24 - week treatment stage and at the post - treatment assessment visit ( to assess safety ) , prediction of response according to hpv status , and the proportion of patients who had a recurrence ( histologically con rmed vulval intraepithelial neoplasia grade 3 ) at 12 months . statistical analysis the primary aim of the rtvin trial was to assess e cacy of cidofovir and imiquimod in terms of the primary endpoint . 
we used a flemings single - stage design in each treatment arm of the study to show e cacy for cidofovir and imiquimod separately ; the study was not formally powered to compare the complete response at 30 weeks between arms . 
if fewer than 30% of patients had had a complete response at 30 weeks in either treatment arm , the treatment would be deemed insu ciently active to warrant further study ; if , however , 45% or more patients had a complete response in either treatment arm , the treatment would be deemed worthy of further investigation . 
with flemings single - stage design , a p1 value of 030 and a p2 value of 045 , an of 005 ( one - sided ) , and 90% power , we calculated that 87 participants needed to be assigned to each treatment group , giving a total of 174 participants . 
 for the primary endpoint , we analysed each treatment arm by both intention to treat ( ie , including all patients randomly allocated to a group ) and per protocol ( ie , including all individuals who continued treat ment until 1364 vol 15 november 2014 articles complete response , disease progression , or 24 weeks )  . 
 we recorded the number of patients with a histologically con rmed complete response at the post - treatment assessment visit in each treatment group and calculated the corresponding proportion ; we used the clopperpearson exact binomial method to calculate the 90% ci for the proportion . 
to look for predictors of response in each treatment group , we did per - protocol subgroup analyses of the primary endpoint for several prede ned variables , using either pearsons test or fishers exact method ( if any cell included fewer than ve patients )  . we assessed adherence to treatment at 6 weeks and 24 weeks in terms of the median ( iqr ) number of applications during each period for all patients completing treatment ( and treatment diary cards ) up to those timepoints . 
we recorded the number of toxic e ects at baseline and in all patients who applied the assigned treatment at least once , in terms of the worst grade reported during treatment and at the post - treatment assessment visit , and we calculated proportions for each treatment group . 
these events were fatigue , pruritus , ulceration , pain in the vulva , headache , muscle pain , and proteinuria ; we reported ndings separately for these adverse events . 
for example , we compared between treatment arms the proportions of expected adverse events and of all toxic e ects of grade 2 or higher recorded during treatment , using pearsons test . 
 also , we assessed the di erence in symptom scores from baseline to the post - treatment assessment visit for pruritus and vulval pain for each treatment arm , using mcnemars test ( and fishers exact method if fewer than ve patients were recorded in any cell )  . 
we also combined data for reported serious adverse events with toxic e ects recorded on crfs . this trial is registered with current controlled trials , isrctn 34420460 . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation of data , or writing of the report . 
 five ( 6% ) of 89 patients assigned cidofovir and seven ( 8% ) of 91 patients allocated imiquimod were lost to follow - up before the rst assessment for toxic e ects and were excluded from this analysis . 
 * response assessed with adapted recist ( appendix pp 12 )  . table 5 : response of patients at the ptav and characteristics of complete responders ( per - protocol population ) results between oct 21 , 2009 , and jan 11 , 2013 , 180 patients were enrolled from 32 hospitals across the uk ( appendix p 3 ) ; 89 were randomly allocated to receive cidofovir and 91 were assigned to receive imiquimod ( gure )  . 
baseline demographics , disease variables , and hpv characteristics were balanced between treatment groups ( table 1 ) , and adverse events at baseline ( de ned by ctcae version 3 ) were also similar ( table 2 )  . five ( 6% ) of 89 patients allocated cidofovir and seven ( 8% ) of 91 assigned imiquimod either withdrew or were lost to follow - up before the rst 6 - week assessment and were regarded as non - compliant with the protocol . 
adherence to treatment was similar in each group at both 6 and 24 weeks , and the median number of treat ment applications by patients did not di er at these timepoints for either cidofovir or imiquimod ( table 3 )  . 
treatment was stopped early because of intolerance in ten ( 11% ; 95% ci 57201 ) of 87 patients allocated cidofovir and 15 ( 17% ; 98263 ) of 89 assigned imiquimod . 
adverse events of grade 2 or individuals allocated higher were less frequent in patients assigned cidofovir imiquimod compared with ( 61 [ 73% ] of 84 patients vs 73 [ 87% ] of 84 patients ; p = 0021 )  . 
the main di erences between treatments with respect to toxic e ects of grade 2 or higher were fatigue , pruritus , and headache , which were all at least 10% more frequent in the imiquimod arm ( table 4 )  . 
 toxic e ects of grade 3 or higher were similar between groups ( 31 [ 37% ] of 84 patients allocated cidofovir vs 39 [ 46% ] of 84 patients assigned imiquimod ; p = 0211 )  . 
 by per - protocol analysis , the propor tion of patients with pruritus grade 2 or higher fell signi cantly between baseline and the post - treatment assessment in both treatment groups ( cidofovir , 14 [ 19% ] of 72 patients vs ve [ 7% ] of 72 patients ; p = 0013 ; imiquimod , 15 [ 22% ] of 69 patients vs ve [ 7% ] of 69 patients ; p = 0008 )  . 
 no di erence in the proportion of patients with grade 2 or higher vulval pain was seen between baseline and the post - treatment assessment ( cidofovir , nine [ 13% ] of 72 patients vs three [ 4% ] of 72 patients ; p = 0109 ; imiquimod , four [ 6% ] of 69 patients vs four [ 6% ] of 69 patients ; p = 1000 )  . 
new lesions arose during the 24 - week treatment stage in 19 ( 21% ) of 87 patients assigned cidofovir and 11 ( 12% ) of 91 patients allocated imiquimod ; however , we do not know whether any of these new lesions arose within the treatment area or not . 
six individuals assigned imiquimod had also been immunocompromised , of whom two responded and four did not . 23 patients crossed over to the alternative treatment ( gure ) , of whom 16 had a post - treatment biopsy sample taken . 
three ( 43% ) of seven patients who received cidofovir after crossover had a complete response compared with four ( 44% ) of nine individuals who were given imiquimod after crossover . ( median is not yet mature follow - up data for the 83 patients who had a complete response follow - up 249 months [ iqr 135312 ] ) , but ndings currently suggest that complete response ( ie , absence of vulval intraepithelial neoplasia ) is maintained at 12 months . 
 at the time of this analysis , 20 ( 87% ) of 23 patients assigned cidofovir still had a complete response at 12 - month follow - up , as did 25 ( 78% ) of 32 individuals allocated imiquimod . 1366 vol 15 november 2014 articles discussion the ndings of the rtvin trial show that both imiquimod and cidofovir are safe , active , and feasible for treatment of vulval intraepithelial neoplasia grade 3 . 
as far as we know , our study is the largest to date to assess topical treatments for vulval intraepithelial neoplasia , with patients recruited from both teaching and general hospitals , supporting the relevance of these ndings to general clinical practice ( panel )  . 
although cidofovir had slightly fewer reported toxic e ects , imiquimod is available for use and is an e ective alternative to surgery that can be o ered to women with vulval intraepithelial neoplasia after exclusion of occult invasive disease . the international society for the study of vulval disease uses morphological criteria to classify vulval intraepithelial neoplasia into usual - type ( hpv - related ) or di erentiated ( non - hpv - related )  . 
in the rtvin trial , we wanted to use a de nition that was familiar to pathologists in the uk , provided a clear threshold for entry into the study , and minimised intra observer variability . 
we considered central histo logical review , but that would have caused substantial logistical di culties in an already challenging trial . table 3 shows that the primary reason for exclusion from the per - protocol analysis was withdrawal from treatment because of intolerance or by patients choice . 
data for adherence to treatment tailed o after the rst 6 weeks of the study ; however , before this timepoint , data collection was good ( around 86% ) and response to treatment did not seem to be related to adherence . 
although the rtvin trial was randomised , the flemings design is not aimed primarily at direct comparison between arms ; thus , the study was not powered to detect a di erence in e cacy between cidofovir and imiquimod . 
more adverse events were noted with panel : research in context systematic review current options for the management of vulval intraepithelial neoplasia are conservative , surgery , or an unlicensed alternative . 
 a cochrane systematic review of medical treatments for vulval intraepithelial neoplasia was done in 2011 , which comprised three randomised controlled trials of imiquimod treatment for vulval intraepithelial neoplasia , but no published studies were included for cidofovir or other topical treatments.18 findings of the three randomised trials showed a combined complete response in 36 ( 58% ) of 62 patients assigned imiquimod compared with none of 42 allocated a placebo.1921 also , two retrospective studies including outcomes after treatment with imiquimod have been published , in which complete responses were reported in 47 ( 76% ) of 62 patients and ten ( 31% ) of 32 patients.22 , 23 to date , no further randomised trials of topical treatment for vulval intraepithelial neoplasia have been completed . 
in addition to our cidofovir pilot study , in which a complete response was seen in four ( 40% ) of ten women completing treatment , 10 one further trial of topical treatment with cidofovir for patients with vulval intraepithelial neoplasia has been completeda phase 2a study in men and women with high - grade anal intraepithelial neoplasia and vulval intraepithelial neoplasia , all of whom were hiv - positive.24 treatment was for 5 days , with a 9 - day treatment gap , repeated for a total of six cycles . 
by intention - to - treat , a complete response was noted in ve ( 15% ) of 33 patients and a partial response was recorded in 12 ( 36% )  . 
an update of the cochrane review awaits publication of data from the rt3vin trial . interpretation allowing for di erences in treatment regimens , the results of previous studies accord with those of the rt3vin trial . 
our study providesto the best of our knowledgethe largest evidence - base so far from which an alternative to surgery can be o ered : either topical imiquimod or cidofovir . 
although more adverse events were noted with imiquimod , most were grade 2 , and imiquimod is already licensed for use on the vulva , is readily available for prescription within hospitals as a topical treatment , and is much cheaper than cidofovir . 
no validated method for measurement of quality of life in patients with vulval intraepithelial neoplasia was available at the start of the rtvin trial ; therefore , we did not gather these data , other than for symptoms and adverse events . 
such a method is now in development , 25 and future trials should include quality - of - life data , along with a health - economic analysis . in view of the complexity of setting up trials in uncommon disorders such as vulval intraepithelial neoplasia , future studies should allow new topical treatments to be assessed alongside existing ones in phase 3 assessments . 
in our trial , cidofovir seemed to be better tolerated than imiquimod ; therefore , in future studies , we might be able to augment complete responses vol 15 november 2014 1367 articles suggest potential predictive by increasing the dose of cidofovir in patients who do not respond initially . 
also , predictive markers for treatment response are needed urgently , because up to now , researchers have been unable to identify patients who are likely to respond to topical treatment . 
 comparing either cidofovir or imiquimod with excisional surgery will be fraught with di culty : the outcomes that are the most important to women are not always easy to measure : methods to assess quality of life will emphasise symptoms that could be associated with one treatment or another . 
in the meantime , a pragmatic approach will most likely have to be taken , whereby we explain to patients the potential bene ts and risks of the available treatment options and take their priorities for treatment into account in this di cult management decision . contributors at , af , gg , cnh , sm , and np designed and developed the study and wrote and reviewed the protocol . 
all authors have seen and approved the nal report . declaration of interests gg has received educational grants from p zer for investigator - initiated clinical trials and has acted as a statistical consultant to p zer . 
all other authors declare no competing interests . acknowledgments the rtvin trial was funded by cancer research uk ( cruk / 06 / 024 ) and cruk core funding to the wales clinical trial unit ( wctu ) at cardi university . 
gilead sciences supported the study by provision of cidofovir at a discounted price , which was funded by a central subvention from the department of health ( england ) and the national institute for social care and health research ( wales )  . 
we thank current and former sta of cardi university and cardi & vale nhs trust for supporting the development and running of this trial ; kim smith , the patients representative on the trial management group ; and members of the independent data monitoring committee and trial steering committee . 
finally , we thank all patients who participated in the trial and the principal investigators ( appendix p 3 ) and their colleagues for recruitment and treatment of patients . corrections correction to lancet oncol 2011 ; 12 : 1051 correction to lancet oncol 2015 ; 16 : 634 , 637 histological sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
 independent lancet oncol 2011 ; 12 : 104552 in the discussion of this article , the second sentence of the fth paragraph should read the proportion of patients a ected by grade 34 fatigue in this study ( 7% ) is similar to that reported for trabectedin ( 78% ) or gemcitabine with docetaxel ( 16% ) .12 , 13 this correction has been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 388 kang hj , loftus s , taylor a , dicristina c , green s , zwaan cm . 
 lancet oncol 2015 ; 16 : 38594 in table 2 of the article , the dose ( mg / kg ) of dexamethasone used in the aprepitant group should read 008 ( 002019 )  . 
this correction has been made to the online version as of aug 31 , 2015 . of medical a airs , from april , 2006 , to december , 2012 , during the design and conduct of the stars trial . 
these cor rections have been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 96778 valle jw , wasan h , lopes a , et al . 
lancet oncol 2015 ; 16 : 96778 in gure 3 of the appendix of this article , parts a and b were mislabelled ; part a shows overall survival data and part b shows progression - free survival data . 
the appendix has been corrected as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 1127 moss sm , wale c , smith r , evans a , cuckle h , duffy sw . 
lancet oncol 2015 ; 16 : 112332in the fourth paragraph of the results section of this article , the absolute mortality reduction in the intervention group should read 003 per 1000 womenyears . 
this correction has been made to the online version as of aug 31 , 2015 and the printed version is correct . chang jy , senan s , paul ma , et al . 
lancet oncol 2015 ; 16 : 63037in this article , the role of the funding source should read : this analysis was designed by the principal and coprincipal investigators of both trials . 
for the stars protocol , accuray speci ed that the cyberknife platform was the sole platform to be used for the study , but did not have a role in any other aspect of the study design . 
beyond providing nancial support , neither funder was in accessing involved the raw data , collection , analysis , or interpretation of the data , or writing of the report . 
dab has received grants from accuray , and is the co - owner of berry consultants , a company that designs clinical trials for pharmaceutical and medical device companies , and international healthcare consortia . 
od was an employee of accuray , as senior vice - president responses vol 16 september 2015 e427 minimalism in oncology expenses related to cancer treatment can diminish patients quality of life and impede delivery of highquality care . 
thus , it is worrying that , in 2017 , a study showed the price of some common cancer drugs in the usa rose at a rate higher than inflation . 
the us senate has recently started investigating why a 40 - year - old cancer druglomustine , which has no generic competition has increased in price by 1400% since 2013 . 
at the 23rd annual conference of the national comprehensive cancer network ( orlando , fl , usa , march 2224 , 2018 ) , oncologists had a heated debate about the congressional mandate that prohibits the centers for medicaid and medicare services from negotiating drug prices with in the usa . 
although pharmaceutical companies governmental action is needed to regulate the unit price at which cancer drugs are marketed , could the medical oncology community further help alleviate the financial burden placed on patients by rethinking the way oncology is practiced ? optimising treatment dose could be central to the financial toxicity debate . 
for example , a recent trial of abiraterone showed the concentration of drug that enters the bloodstream can be increased by four times if the drug is swallowed with a low - fat meal rather than on an empty stomach . 
this study supports anecdotal evidence that many oncology drugs could be taken at lower doses or for shorter periods without reducing effectiveness , alleviating both physical and financial toxicity to patients . 
another example of successful dose reduction is immunisation against the hpv serotypes 16 and 18 , for which two vaccine doses provide similar protection to the initially recommended three - dose schedule . 
 the condition of life - threatening cancer has traditionally meant that high drug doses , and thereby high toxicity , have generally been considered acceptable if a treatment is effective . 
the presumed understanding that high dose translates into higher anti - tumour activity still drives clinical trial design , with maximumtolerated doses ( mtd ; the highest dose of a treatment that does not cause unacceptable side effects ) being established as the recommended dose for most new oncology drugs . 
although fine - tuning a personalised dose for each patient is neither feasible nor plausible the optimal dose is just an estimation for a particular patient , and optimisation strategies could substantially delay the market entry of new drugsrethinking drug development to aim for a minimum - effective dose ( med ; lowest dose of treatment that provides a clinically meaningful response ) could be a sensible approach to find the balance between oncological effectiveness , and physical and financial toxicity . 
furthermore , in the era of targeted therapies , which differ from cytotoxic chemotherapies in that they follow a non - linear doseresponse saturation curve whereby the addition of more drug does not always improve outcomes , should the way that safety is assessed move away from the traditional pharmacology - driven study designs ? a 2010 pooled analysis of trials of targeted therapy showed that patients treated with low doses ( 25% mtd ) had similar outcomes to those treated with intermediate ( 2575% mtd ) and high doses ( 75% mtd ) in terms of survival , objective responses , and toxicity . 
 additionally , adaptive studies in oncology , such as the keynote - 001 trial ( which led to the accelerated approval of pembrolizumab , following a customised trial design in which no mtd was reached and the recommended phase 2 dose was based on early safety and response assessments that led to the recruitment of several expansion cohorts ) , could serve as a precedent for future oncology trials . 
adopting the minimum - effective dose as a recommended standard and customising trial design , aided by mathematical modelling and simulations for optimal dosage , suggest a new path towards practising minimalism in oncology that could avoid unnecessary financial and physical toxicity and improve patients quality of life . the value in cancer care consortiumwhich plans to initiate trials that explore whether the dose , duration , or type of drug can be optimisedis a first , promising step to tackle financial toxicity . 
 the lancet oncology for more on the study about cancer drug costs increase after launch in the usa see j clin oncol 2018 ; 36 : 31925 for more on the us senators investigation see com / policy / healthcare / 381287senators - launch - probe - intowhy - price - of - cancer - drugincreased - 1400 - percent for more on the debate at the nccn 23rd annual conference see viewarticle / 894498 for the trial on low - dose abiraterone with food see j clin oncol 2018 ; published online march 28 . 
how do the amaros trial results change practice ? lancet oncol 2014 ; 15 : 128081the last sentence of the fourth paragraph of this comment should read with both the amaros1 and z00112 , 3 studies , the data interpreted should be with caution and should not be extrapolated to patients with three , four , or more positive sentinel lymph nodes . 
this correction has been made to the online version as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e395403 weller m , van den bent m , hopkins k , et al , for the european association for neuro - oncology ( eano ) task force on malignant glioma . 
 lancet oncol 2014 ; 15 : e395403 the appendix of this review was incorrect ; the correct appendix has been uploaded as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e591 furlow b . 
 this correction has been made to the online article as of nov 24 , 2014 . conroy t , galais m - p , raoul j - l , et al , for the fdration francophone de cancrologie digestive and unicancer - gi group . 
de nitive chemo radiotherapy with folfox versus uorouracil and cisplatin in patients with oesophageal cancer ( prodige5 / accord17 ) : final results of a randomised , phase 2 / 3 trial . 
the last sentence of the eighth paragraph in the results section should read an endoscopic complete response at week 15 was achieved in 61 ( 53% ) of 115 patients in the folfox group versus 57 ( 48% ) of 120 patients in the uorouracil plus cisplatin group . 
folfox = uorouracil , leucovorin , and oxaliplat recist = response evaluation criteria in solid tumours.21 * 115 patients assessable in the folfox group and 120 assessable in the uorouracil and cisplatin group . table 2 : tumour response to treatment correction to lancet oncol 2014 ; 15 : 1464 sestak i , singh s , cuzick j , et al . 
changes in bone mineral density at 3 years in postmenopausal women receiving anastrozole and risedronate in the ibis - ii bone substudy : an international , doubleblind , randomised , placebo - controlled trial . 
this correction has been made to the online version as of nov 24 , 2014 , and the printed version is correct . c lumbar spine d total hip 05 10 15 20 25 30 35 40 45 50 12% 40% 18% 40% anastrozole placebo baseline 12 months anastrozole placebo 36 months baseline 12 months 36 months vol 15 december 2014 e587 corrections correction to lancet oncol 2015 ; 16 : 1045 correction to lancet oncol 2015 ; 16 : 1499 tournigand c , chibaudel b , samson b , et al . 
 this correction has been made to the online version as of nov 29 , 2015 . correction to lancet oncol 2015 ; 16 : 1355 , 1363 hegewisch - becker s , graeven u , lerchenmller ca , et al . 
maintenance strategies after first - line oxaliplatin plus uoropyrimidine plus bevacizumab for patients with metastatic colorectal cancer ( aio 0207 ) : a randomised , noninferiority , open - label phase 3 trial . 
 lancet oncol 2015 ; 16 : 135569the fourth line of the findings section of the summary of this article should read bevacizumab alone was noninferior to standard uoropyrimidine plus bevacizumab ( hazard ratio [ hr ] 108 [ 95% ci 085137 ] ; p = 053 ; upper limit of the one - sided 988% ci 142 ) , whereas no treatment was not ( hr 126 [ 099160 ] ; p = 0056 ; upper limit of the one - sided 988% ci 165 )  . 
 lancet oncol 2015 ; 16 : 14931505in this article , the colours of the curves in both panels of gure 3 were inverted ; the correct version is shown below . 
 these corrections have been made to the online version as of nov 29 , 2015 . events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 49 ( 41 - 57 ) 54 ( 43 - 62 ) stratied hazard ratio 081 ( 066101 ) p = 0059 ( log - rank ) unstratied hazard ratio 078 ( 068096 ) p = 0019 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0023 events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 221 ( 196267 ) 249 ( 214289 ) stratied hazard ratio 079 ( 063099 ) p = 0036 ( log - rank ) unstratied hazard ratio 079 ( 064098 ) p = 0035 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0024 number at risk bevacizumab bevacizumab plus erlotinib time ( months ) number at risk bevacizumab bevacizumab plus erlotinib vol 16 december 2015 e589 for the story on the agreement between pfizer and cipla see com / 2017 / 10 / 07 / health / africacancer - drugs.html for more on glaxosmithklines drug policy in africa see business / 2009 / jul / 14 / glaxosmithkline - aspen - hiv - druglicense and uk / news / health - 35933692 for more on cancer control in africa see j glob oncol 2015 ; 1 : 3036 and thelancet.com / series / cancerhealth - care - systems - in - africa for the study of treatment uptake in cameroon see bmc complement altern med 2017 ; 17 : 209 for evidence on nurse - led cancer prevention programmes see plos med 2011 ; published online may 17 . 
this changing spectrum of disease is altering the continents healthcare needs , but in the absence of insufficient national registries and cancer control plans , many governments have stalled on sustainable cancer management . 
 however , a recent article in the new york times praised an agreement between the american cancer society and two pharmaceutical companies , pfizer and cipla , to provide 16 chemotherapy drugs at a reduced cost to six sub - saharan countries . 
 philanthropic agreements to provide low - cost drugs between governments and major pharmaceutical companies are not new in 2009 , glaxosmithkline put its hiv drug , abacavir , into a patent pool to reduce its price and to improve access . 
this decision included several cancer drugs , and is estimated to have helped 85 countries and more than 2 billion people . there is scepticism towards philanthropy , however , for cancer control : speaking in 2016 , pascal soriot , head of astrazeneca , said , there is no point giving free cancer drugs to africa [ because ] it is not only a question of medicine , it is a question of infrastructure . 
although facilitating drug access is a positive step that should serve as a precedent for other major pharmaceutical companies , the impact of this measure on the treatment of cancer will mainly depend on each countrys capacity to safely and effectively administer these drugs . 
data from the african cancer registry networkan effort to set up a reliable registry on the continenthas shown there are only 102 cancer treatment institutions in africa , including general oncology centres , paediatric , and palliative - care establishments , of which 38 are in south africa . 
moreover , the shortage of medically trained staff , and the absence of appropriate training programmes and country - specific guidelines , complicates adequate provision of treatments and continuity of care . 
across africa , treatment abandonment occurs not only because of financial constraints and limited health - care services , but also because of the predominance of alternative healers and beliefs in traditional medicine . 
in the republic of cameroon , where traditional medicine is recognised by the national health system , 55% of parents of children with burkitts lymphoma consult traditional healers despite this cancer being eminently treatable with conventional medicine . 
finally , international efforts should be used to establish the necessary infrastructure to allow the safe delivery of therapies . african governments will need to cope with the growing number of health challenges as the burden of cardiovascular disease , diabetes , and cancer increases across the continent . 
 rather , governments themselves should take the lead in setting the cancer control agenda by realising the extent of the upcoming crisis and making a concerted effort to provide the requisite measures to meet the needs of their people . 
 the lancet oncology vol 18 november 2017 1423 editorial articles lancet oncol 2015 ; 16 : 106170 published online august 5 , 2015 s1470 - 2045 ( 15 ) 00212 - 0 see comment page 1004 * collaborators listed in appendix p 3 correspondence to : secretariat , cancer epidemiology unit , richard doll building , oxford ox3 7lf , uk collaborations@ceu.ox.ac.uk see online for appendix endometrial cancer and oral contraceptives : an individual participant meta - analysis of 27 276 women with endometrial cancer from 36 epidemiological studies collaborative group on epidemiological studies on endometrial cancer * summary background oral contraceptives are known to reduce the incidence rate of endometrial cancer , but it is uncertain how long this e ect lasts after use ceases , or whether it is modi ed by other factors . methods individual participant datasets were sought from principal investigators and provided centrally for 27 276 women with endometrial cancer ( cases ) and 115 743 without endometrial cancer ( controls ) from 36 epidemiological studies . 
the relative risks ( rrs ) of endometrial cancer associated with oral contraceptive use were estimated using logistic regression , strati ed by study , age , parity , body - mass index , smoking , and use of menopausal hormone therapy . findings the median age of cases was 63 years ( iqr 5768 ) and the median year of cancer diagnosis was 2001 ( iqr 19942005 )  . 
9459 ( 35% ) of 27 276 cases and 45 625 ( 39% ) of 115 743 controls had ever used oral contraceptives , for median durations of 30 years ( iqr 17 ) and 44 years ( iqr 29 ) , respectively . 
the longer that women had used oral contraceptives , the greater the reduction in risk of endometrial cancer ; every 5 years of use was associated with a risk ratio of 076 ( 95% ci 073078 ; p < 00001 )  . 
this reduction in risk persisted for more than 30 years after oral contraceptive use had ceased , with no apparent decrease between the rrs for use during the 1960s , 1970s , and 1980s , despite higher oestrogen doses in pills used in the early years . 
however , the reduction in risk associated with ever having used oral contraceptives di ered by tumour type , being stronger for carcinomas ( rr 069 , 95% ci 066071 ) than sarcomas ( 083 , 067104 ; case - case comparison : p = 002 )  . 
in high - income countries , 10 years use of oral contraceptives was estimated to reduce the absolute risk of endometrial cancer arising before age 75 years from 23 to 13 per 100 women . interpretation use of oral contraceptives confers long - term protection against endometrial cancer . 
these results suggest that , in developed countries , about 400 000 cases of endometrial cancer before the age of 75 years have been prevented over the past 50 years ( 19652014 ) by oral contraceptives , including 200 000 in the past decade ( 200514 )  . funding medical research council , cancer research uk . introduction use of oral contraceptives is known to reduce the incidence of endometrial cancer.1 because endometrial cancer is uncommon in young women but its incidence increases sharply with age , the public health e ects of this inverse association depend mainly on the extent to which the reduced risk of endometrial cancer persists long after use ceases . 
to investigate the association between use of oral contraceptives and the subsequent risk of endometrial cancer , individual participant data from 36 epidemiological studies of endometrial cancer have been brought together and analysed centrally . methods identi cation of studies and collection of data this collaboration was established in 2005 . 
since 2012 , epidemio logical studies were eligible for inclusion if they collected individual data about use of hormonal con traceptives and reproductive history from at least 400 women with endometrial cancer in retrospective studies , and at least 200 women in prospective studies . 
eligible studies were identi ed from review articles , computer - aided literature searches in pubmed and medline ( up to jan 31 , 2012 ) , using combinations of the search terms endometrial cancer risk , endometrium cancer risk , hormon * , oral contraceptive , and oc , plus the additional terms cohort , prospective , women , and cancer risk , and from discussions with colleagues . 
e orts were made to identify all studies that included relevant information , irrespective of whether or not results about oral contraceptives had been published , and principal investigators from each eligible study were invited to participate . cases were de ned as women with invasive cancer of any histological type of the body of the uterus who were without previous cancer ( except non - melanoma skin cancer ) ; controls were women without previous cancer who had an intact uterus . 
prospective studies were incorporated by a nested case - control design , in which up to four controls were selected at random from cohort vol 16 september 2015 1061 articles investigators members , matched for exact year of birth , date of recruitment ( within 6 months ) , duration of follow - up ( at disease onset ) , and , when appropriate , other matching criteria used by ( eg , the principal geographical region )  . 
individual participant data on sociodemographic and repro ductive factors , use of contraceptives , use of hormonal therapies for the menopause , reproductive history , height , weight , consumption of alcohol and tobacco , and family history of breast and endometrial cancer were sought from the principal investi gators of every study . 
for prospective studies , reported information on the use of oral contraceptives was taken from the last record before disease onset , to calculate duration of use and time since last use ( assuming no further use )  . 
 apparent inconsistencies in the data were discussed with the study investigators and if they could not be recti ed , decisions were made about which values to incorporate into the pooled dataset . 
after the records had been checked and corrected , investigators were sent summary analyses of the variables to be used for nal con rmation that their data had been interpreted correctly . 44 eligible studies were identi ed245 of which 36 are included in the current analysis.237 four groups of researchers declined to participate in this collaboration3841 and a further four groups agreed in principle to provide data at a future date.4245 principal individual investigators provided information about whether or not women had ever used hormonal contraceptives ( as de ned by each study ) and most also provided information about the total duration of use and age or calendar year at rst and last use . 
only 13 studies collected information on the type of hormonal contraceptives ; 7 , 17 , 19 , 21 , 2530 , 33 , 35 , 36 women from the remaining 23 studies were assumed to be using combined oral contraceptives ( ie , those containing both oestrogen and progestin ) because more than 95% of hormonal contraceptive users included in studies with such information reported using combined preparations . 
 there were too few women with endometrial cancer exclusively progestin - only oral who had used contraceptives ( 56 cases ) , progestin - only injectable hormonal contraceptives ( 19 cases ) , combined injectable hormonal contraceptives ( three cases ) or sequential oral contraceptives ( 41 cases ) for reliable analysis . statistical analysis statistical analyses were done with stata version 13.0. 
when several groups were compared , with one taken as the reference group with an rr of 1 , the variance of the log risk in the reference group and in each of the other groups was calculated from the variances and covariances of the log rrs in those other groups.47 these group - speci c variances yield the groupspeci c cis for each group ( including the reference group ) that are plotted in the gures . all analyses were strati ed by study , centre ( for multicentre studies ) , age group ( 1619 , 2024 years , and so on up to 7579 , 8084 , and 8589 years ) , parity ( 0 , 1 , 2 , 3 , 4 , 5 , or not known ) , body - mass index ( bmi < 25 , 2530 , 30 kg / m , or not known ) , smoking ( never , ever , or unknown ) and type of menopausal hormone therapy used ( never , oestrogen - only exclusively , combined exclusively , both oestrogen - only and combined , other types , or unknown use )  . 
the e ect on the main ndings of further strati cation by ethnic origin , education , age at rst birth , age at last birth , age at menarche , age at menopause , menopausal status , and family history of endometrial cancer was examined by comparing results before and after strati cation for each variable separately . 
 women with missing information for any of these adjustment factors were assigned to a separate stratum for the relevant variable to conserve total numbers analysed ; sensitivity analyses excluded these women . the rr of endometrial cancer per 5 - year duration of oral contraceptive use was estimated by tting a loglinear trend across categories of duration ( never , < 1 , 1 < 5 , 5 < 10 , 10 < 15 , and 15 years ) , using the median value within each category . the association of endometrial cancer risk and duration of oral contraceptive use was cross - classi ed by time since last use and by mid - calendar - year of use ( grouped as 196069 , 197079 , and 198089 ) to assess the independent e ect , if any , of these factors on risk . 
 although the composition of oral contraceptive pills has varied substantially over time , a strong association exists between calendar year of use and oestrogen dose in the oral contraceptives typically used.4850 in the usa and uk , for example , the oral contraceptives prescribed before 1970 were typically high - dose preparations , often containing 100 g or more of oestrogen ; between 1970 and 1980 prescriptions were typically for medium - dose preparations containing about 50 g of oestrogen ; and by 1980 most prescriptions were for low - dose preparations , containing 35 g or less of oestrogen.49 , 50 thus , in these analyses , decade of use was taken as a correlate of oestrogen dose of oral contraceptives . the classi cation system adopted in each study was used centrally to categorise tumours into three broad histological subtypes : type i ( endometrioid carcinomas ) ; type ii ( non - endometrioid carcinomas ) ; and uterine sarcomas . 
 uterine sarcomas were de ned as sarcoma , not otherwise speci ed ( 88008806 ) , brosarcoma ( 88108833 ) , liposarcoma ( 88508858 ) , myosarcoma ( 88908896 ) , rhabdomyosarcoma ( 89008902 , 89108912 ) , endometrial stromal sarcoma ( 89308931 ) , or cancer coded as sarcoma by study investigators . 
signi cance tests for heterogeneity of the relative risks for oral contraceptive use by tumour subtype compared cases only ( case - case comparisons ) , because controls provide no additional information . 
hence , although they were still strati ed by study ( centre ) and age , to retain su cient statistical information within each stratum they were adjusted rather than strati ed for parity , bmi , smoking , and type of menopausal hormone therapy used . when results are presented in the form of plots , rrs are represented by squares and their corresponding cis or group - speci c cis by horizontal lines . 
the position of the square indicates the point estimate of the rr , and the area of the square is inversely proportional to the variance of the logarithm of the rr ( or , for multigroup analyses , log risk ) , thus providing an indication of the amount of statistical information available for that particular estimate . 
because of the large number of rr estimates presented , 99% cis are generally used in the gures ; however , throughout the text 95% cis are quoted . cumulative incidence rates of endometrial cancer ( up to the age of 75 years ) associated with di erent durations of use of oral contraceptives were estimated by application of rr estimates for endometrial cancer from the present analyses to age - speci c incidence rates for women in 21 high - income countries in western europe , north america , and australasia ( appendix p 8 ) .52 absolute numbers of cancers prevented were estimated from birth cohort - speci c prevalences of oral contraceptive use.53 role of the funding source the funders of the study had no role in the study design , data collection , data analysis , data interpretation , writing of the report , or the decision to submit for publication . 
 the writing committee had full access to all the data , could request any analyses , and had nal responsibility for the decision to submit for publication . results table 1 presents the details of the 36 participating studies . 
the median year of cancer diagnosis was 2001 ( iqr 19942005 ) and the median age at diagnosis was 63 years ( iqr 5768 ) , with 847 ( 3% ) of women diagnosed before 45 years of age , 3743 ( 14% ) at 4554 years , 11 287 ( 41% ) at 5564 years , and 11 399 ( 42% ) at 65 years or older . overall , 9459 ( 35% ) of 27 276 women with endometrial cancer and 45 625 ( 39% ) of 115 743 controls had ever used oral contraceptives , with a median duration of use of 30 years ( iqr 17 ) and 44 years ( 29 ) , respectively . 
the prevalence of ever having used oral contraceptives was substantially lower in controls from asia ( 899 / 11 180 ; 8% ) than in controls from europe and north america ( 39 050 / 86 293 ; 45% )  . figure 1 shows the study - speci c and combined relative risks of endometrial cancer in ever - users compared with never - users of oral contraceptives and , in the ever - users , the rr per 5 years of use . 
studies with a low information content ( de ned as 1 / var [ ln rr ] < 20 ) are included in the other category for each relevant study design . 
overall , the risk of endometrial cancer was signi cantly lower in women who had ever used oral contraceptives than in women who had never used them ( rr 069 , 95% ci 067072 ) , with no signi cant heterogeneity between the three types of study design ( heterogeneity test ; p = 015 )  . duration of use of oral contraceptives ( years ) years of use cases / controls rr ( 99% gsci ) 1595 / 6428 097 ( 088107 ) 1 < 5 3624 / 15 938 081 ( 076086 ) 5 < 10 2096 / 11 070 064 ( 059069 ) 10 < 15 1136 / 6927 052 ( 047058 ) 422 / 3420 032 ( 028038 ) never - users 30 years since last use 1529 years since last use < 15 years since last use duration of use of oral contraceptives ( years ) figure 2 : relative risk of endometrial cancer in users of oral contraceptives compared with never - users , by ( a ) duration of use , and ( b ) duration of use and time since last use of oral contraceptives gsci = group - speci c ci . 
never users in studies with data on time since last use include 15 169 cases and 55 965 controls with relative risk of 100 ( 99% gsci 096104 )  . 
 the longer women had used oral contraceptives for , the lower their risk of endometrial cancer was , with each 5 years of use associated with an rr of 076 ( 95% ci 073078 , p < 00001 ) , based on 8873 cases and 43 783 controls who were ever - users ( gure 1 )  . 
the proportional reduction in risk of endometrial cancer per 5 years of oral contraceptive use varied slightly by age at diagnosis ( heterogeneity test ; p = 0004 ) , with rr 071 ( 95% ci 067075 ) for women diagnosed before 60 years of age and rr 079 ( 075082 ) for women diagnosed at 60 years of age or older . 
the association did not vary by bmi , parity , use of menopausal hormone therapy , menopausal status , smoking status , age at menarche , ethnic origin , or alcohol use ( gure 3 )  . 
the exclusion of women with missing values for any of these strati cation variables also made a negligible di erence to the risk estimates ( making the fully strati ed rr per 5 years use of oral contraceptives 075 , 95% ci 072077 )  . ( median most women with endometrial cancer had stopped using oral contraceptives many years before their cancer diagnosis last use 29 years time since [ iqr 2234 ] )  . 
women who had used oral contraceptives more recently had also , on average , used them for a longer duration ( eg , women who had used oral contraceptives less than 15 years previously had a median duration of use of 47 years [ iqr 1399 ] , whereas women who had last used oral contraceptives 30 years or more previously had a median duration of use of 30 years [ 1053 ] )  . 
for a given duration of use , the reduction in risk was slightly greater in women with more recent use , although a signi cant protective e ect remained more than 30 years after use had ceased ( gure 2b and appendix p 5 )  . in 7452 women with endometrial cancer for whom information about the timing of their oral contraceptive use was available , 3235 ( 43% ) had a mid - year of oral contraceptive use in the 1960s and 371 ( 5% ) had a midyear of use in the 1980s ( appendix p 6 )  . 
the rrs per 5 years duration of use of oral contraceptives in the 1960s , 1970s , and 1980s did not vary signi cantly ( heterogeneity test ; p = 015 , appendix p 6 )  . 
there was also no signi cant heterogeneity in the rr per 5 years of use by age at rst use or age at last use ( appendix p 7 )  . however , there was some evidence that the rr depended on the histological subtype of endometrial cancer ( table 2 )  . 
compared with women who had never used oral contraceptives , ever - users had an rr of 069 ( 95% ci 066071 ) for carcinomas , based on 26 877 cases , which was similar for type i and type ii carcinomas . 
 few cases , ever - use of oral based on relatively contraceptives was not signi cantly associated with the risk of uterine sarcoma ( rr 083 [ 95% ci 067104 ] , based on 399 cases ; heterogeneity , from direct case - case comparison of sarcomas vs carcinomas p = 002 )  . 
analyses were also done in women with information about 50 g per week 1 = 0005 , p = 094 figure 3 : relative risk of endometrial cancer per 5 years use of oral contraceptives , by various lifestyle and reproductive characteristics rr = relative risk . 
 * rr strati ed by study ( centre ) , age , parity , body - mass index , smoking , and type of menopausal hormone therapy used , where appropriate . 
 menopausal hormone replacement similar results were obtained when the analyses were 1066 vol 16 september 2015 articles ever - users never - users relative risk ( 95% ci ) for ever vs never use of oral contraceptives carcinoma type i carcinoma type ii carcinoma sarcoma cases 9280 6096 controls cases controls 45 625 39 191 39 191 40 024 17 597 9921 70 118 56 365 56 365 57 788 069 ( 066071 ) 068 ( 065071 ) 075 ( 066085 ) 083 ( 067104 ) in a case - case comparison of sarcoma vs carcinoma , p = 002 . 
information about histological subtype ( type i , type ii , or uterine sarcoma ) was available for 17 754 ( 65% ) of 27 276 cases ; the remaining cases were classi ed as carcinoma , unspeci ed . 
 table 2 : relative risk of endometrial cancer in ever versus never users of oral contraceptives by histological subtype * duration of oral contraceptive use ( incidence up to 75 years of age ) never users ( risk to age 75 years : 23% ) 5 years use ( risk to age 75 years : 17% ) 10 years use ( risk to age 75 years : 13% ) 15 years use ( risk to age 75 years : 10% ) age ( years ) figure 4 : absolute risk of endometrial cancer incidence per 100 women up to 75 years of age in high - income countries by duration of oral contraceptive use ( population - weighted rates , 200307 , for 21 countries in western europe , north america , and australasia ) endometrial cancer incidence rates are extremely low before the age of 35 years . random errors , and it also avoids the biases that could be produced by undue emphasis on particular studies with extreme results . 
only a third of the eligible studies have published on oral contraceptives and endometrial cancer , 4 , 7 , 8 , 10 , 17 , 18 , 21 , 24 , 2931 , 33 , 35 so a review based solely on these studies could be a ected by publication bias . 
despite extensive e orts to identify all studies with unpublished results , it is impossible to guarantee that others do not exist ; furthermore , it is not possible to have completely up - to - date information from the continuing prospective studies . 
however , the eight eligible studies that were identi ed but did not contribute data to this collaboration together contain only about 12% as many women with endometrial cancer as the included studies . 
only one of these eight studies has published results on oral contraceptives and endometrial cancer , and its reported ndings are broadly similar to ours.39 the 36 included studies were of varied design and were done in di erent settings , with wide duration of oral contraceptive use . 
for carcinoma , the rr per 5 years use of oral contraceptives was 075 ( 95% ci 073077 , based on 8701 cases ) ; for uterine sarcoma , the corresponding rr was 088 ( 95% ci 074103 , based on 172 cases ; heterogeneity , from direct case - case comparison of sarcomas vs carcinoma p = 024 )  . based on the rrs presented in gure 2 and age - speci c rates of endometrial cancer for women in high - income countries , cumulative incidence rates of endometrial cancer were estimated for never - users of oral contraceptives and for women who had used them for di erent durations , beginning at 20 years of age . 
the corresponding cumulative incidence rate for women who had used oral contraceptives for 5 , 10 , and 15 years was estimated to be 17 , 13 , and 10 per 100 users , respectively ( gure 4 )  . 
in this age range , the number of women who were ever - users of oral contraceptives has grown steeply over the past 50 years , from essentially zero in the 1960s to about three - quarters in high - income countries today.53 hence , the annual number of endometrial cancers prevented by ever - use of oral contraceptives has also increased steeply over the past 50 years . 
using birth cohort - speci c in western prevalences of oral contraceptive use developed countries , 53 we estimate that over the past 50 years ( 19652014 ) in 21 countries in western europe , north america , and australasia , oral contraceptive use has prevented a total of about 400 000 endometrial cancers , including 200 000 in the past 10 years ( 200514 ) , at ages 3074 years ( appendix p 8 )  . 
because these results are based on population they automatically allow for the di erent rates of hysterectomy in those populations . incidence rates , discussion this international collaboration has brought together and re - analysed almost all of the available epidemiological evidence on the reduction in endometrial cancer incidence associated with oral contraceptive use , and includes data from 27 000 women with endometrial cancer from 36 studies . 
a protective e ect persists for at least 30 years after use ceases , and does not seem to depend much on the dose of oestrogen in the contraceptive formulations or on personal characteristics such as parity , adiposity , or menopausal status . combining results from many studies has the obvious advantage of yielding a large sample size , which reduces vol 16 september 2015 1067 articles variation in the duration of use and time since last use of oral contraceptives . 
 the main analyses were strati ed simultaneously by study , centre within study , age at diagnosis , parity , bmi , smoking , and use of menopausal hormone therapy . 
it meant that the analyses of the association between oral contraceptive use and risk of endometrial cancer are based on comparisons between women in the same study who were of the same age and who had a similar history of other risk factors for endometrial cancer . although few studies provided information about hormonal constituents of the preparations used , the oral contraceptives of the 1960s would generally have contained much higher doses of oestrogen than those of the 1980s . 
these results show that the amount of oestrogen in the lower - dose pills is still su cient to reduce the incidence of endometrial cancer , which is consistent with ndings from two studies that have assessed the hormonal dosages constituents.41 , 54 the numbers of women who reported using anything other than combined oral contraceptives ( eg , sequential oral or progestin - only oral contraceptives and / or injectable hormonal contraceptives ) were too small for reliable analysis . individual the decline in endometrial cancer risk with increasing duration of use does not seem to vary substantially with parity , bmi , use of menopausal hormone therapy , menopausal status , smoking status , age at menarche , ethnic origin , or alcohol intake . 
the reduction in risk associated with 5 years use of oral contraceptives was slightly greater in women diagnosed before 60 years of age than in women diagnosed at an older age , but given the number of signi cance tests done , this could be due to chance . 
the reduction in endometrial cancer risk with increasing duration of use does not seem to vary much with factors related to the timing of use , such as age of rst or last use , time since last use , or calendar period of use . the e ect of oral contraceptives does , however , seem to vary by histological subtype , with ever - use strongly associated with a reduced risk of type i and probably of type ii endometrial carcinoma , but somewhat less strongly associated with a reduced risk of uterine sarcomaa much rarer type of cancer . 
another pooled analysis that included 15 studies , most of which contributed to the current analysis , also reported a similar reduction in risk of both type i and type ii endometrial carcinoma for ever use of oral contraceptives51 but no signi cant association with uterine sarcoma.55 taken together , it is reasonable to infer that the associations recorded here are causal ( ie , that current or past oral contraceptive use reduces the incidence of the menstrual cycle , endometrial cancer in otherwise similar women )  . 
almost all of the hormonal contraceptive use in these studies is likely to involve combined oral contraceptives , which contain oestrogen plus progest these contraceptives might protect against endometrial cancer by minimising exposure to unopposed oestrogen during the follicular phase of inhibiting oestrogen - induced cell proliferation ; 56 , 57 moreover , the addition of a progestin to menopausal hormone therapy has been shown to reduce the adverse e ects of oestrogen on the risk of endometrial cancer in postmenopausal women.53 , 5860 however , the exact mechanisms by which oral contraceptives cause substantial protection against endometrial cancer many years after cessation of use are still unclear . 
 thereby since the introduction of oral contraception in the early 1960s , about 400 million women have used it in highincome countries alone , 61 often for prolonged periods during early adulthood.53 medium - to - long - term use of oral con traceptives ( eg , for 5 years or longer ) results in a substantial proportional reduction in the incidence of endometrial cancer , the magnitude of which is similar to that seen for ovarian cancer.53 because this reduction in risk persists more than 30 years after use has ceased , and the incidence of endometrial cancer increases steeply with age , the public health e ect of oral contraceptive use on endometrial cancer is most apparent many years after use has stopped . 
the present results , taken together with what what is known about past patterns of use , suggest that in high - income countries oral contraceptives have , over the past 50 years ( 19652014 ) , already prevented a total of about 400 000 endometrial cancers before the age of 75 years , including 200 000 in the past decade ( 200514 )  . 
 contributors na , vb , swk , rs , ss , and toy identi ed studies , received and checked data , did analyses , and had full access to all materials and results . 
na , vb , gr , ss , and rp drafted the report , and all writing committee members helped to revise it before and after circulation to the collaborators for comment . analysis and writing committee clinical trial service unit & epidemiological studies unit , nu eld department of population health , university of oxford , oxford , uk : n allen , r peto . 
department of primary care health sciences , university of oxford , oxford , uk : r stevens . declaration of interests we declare no competing interests . corrections correction to lancet oncol 2014 ; 15 : 1280 correction to lancet oncol 2014 ; 15 : 310 , 311 boughey jc . 
how do the amaros trial results change practice ? lancet oncol 2014 ; 15 : 128081the last sentence of the fourth paragraph of this comment should read with both the amaros1 and z00112 , 3 studies , the data interpreted should be with caution and should not be extrapolated to patients with three , four , or more positive sentinel lymph nodes . 
this correction has been made to the online version as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e395403 weller m , van den bent m , hopkins k , et al , for the european association for neuro - oncology ( eano ) task force on malignant glioma . 
 lancet oncol 2014 ; 15 : e395403 the appendix of this review was incorrect ; the correct appendix has been uploaded as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e591 furlow b . 
 this correction has been made to the online article as of nov 24 , 2014 . conroy t , galais m - p , raoul j - l , et al , for the fdration francophone de cancrologie digestive and unicancer - gi group . 
de nitive chemo radiotherapy with folfox versus uorouracil and cisplatin in patients with oesophageal cancer ( prodige5 / accord17 ) : final results of a randomised , phase 2 / 3 trial . 
the last sentence of the eighth paragraph in the results section should read an endoscopic complete response at week 15 was achieved in 61 ( 53% ) of 115 patients in the folfox group versus 57 ( 48% ) of 120 patients in the uorouracil plus cisplatin group . 
folfox = uorouracil , leucovorin , and oxaliplat recist = response evaluation criteria in solid tumours.21 * 115 patients assessable in the folfox group and 120 assessable in the uorouracil and cisplatin group . table 2 : tumour response to treatment correction to lancet oncol 2014 ; 15 : 1464 sestak i , singh s , cuzick j , et al . 
changes in bone mineral density at 3 years in postmenopausal women receiving anastrozole and risedronate in the ibis - ii bone substudy : an international , doubleblind , randomised , placebo - controlled trial . 
this correction has been made to the online version as of nov 24 , 2014 , and the printed version is correct . c lumbar spine d total hip 05 10 15 20 25 30 35 40 45 50 12% 40% 18% 40% anastrozole placebo baseline 12 months anastrozole placebo 36 months baseline 12 months 36 months vol 15 december 2014 e587 chromatin organisation and cancer prognosis : a pan - cancer study andreas kleppe , fritz albregtsen , ljiljana vlatkovic , manohar pradhan , birgitte nielsen , tarjei s hveem , hanne a askautrud , gunnar b kristensen , arild nesbakken , jone trovik , hkon whre , ian tomlinson , neil a shepherd , marco novelli , david j kerr , hvard e danielsen summary background chromatin organisation affects gene expression and regional mutation frequencies and contributes to carcinogenesis . 
we aimed to define and validate a novel prognostic biomarker for the automatic detection of heterogeneous chromatin organisation . methods machine learning algorithms analysed the chromatin organisation in 461 000 images of tumour cell nuclei stained for dna from 390 patients ( discovery cohort ) treated for stage i or ii colorectal cancer at the aker university hospital ( oslo , norway )  . 
the resulting marker of chromatin heterogeneity , termed nucleotyping , was subsequently independently validated in six patient cohorts : 442 patients with stage i or ii colorectal cancer in the gloucester colorectal cancer study ( uk ) ; 391 patients with stage ii colorectal cancer in the quasar 2 trial ; 246 patients with stage i ovarian carcinoma ; 354 patients with uterine sarcoma ; 307 patients with prostate carcinoma ; and 791 patients with endometrial carcinoma . 
the primary outcome was cancer - specific survival . findings in all patient cohorts , patients with chromatin heterogeneous tumours had worse cancer - specific survival than patients with chromatin homogeneous tumours ( univariable analysis hazard ratio [ hr ] 17 , 95% ci 1225 , in the discovery cohort ; 18 , 1030 , in the gloucester validation cohort ; 22 , 1145 , in the quasar 2 validation cohort ; 31 , 1950 , in the ovarian carcinoma cohort ; 25 , 1834 , in the uterine sarcoma cohort ; 23 , 1246 , in the prostate carcinoma cohort ; and 43 , 2868 , in the endometrial carcinoma cohort )  . 
after adjusting for established prognostic patient characteristics in multivariable analyses , nucleotyping was prognostic in all cohorts except for the prostate carcinoma cohort ( hr 17 , 95% ci 1125 , in the discovery cohort ; 19 , 1132 , in the gloucester validation cohort ; 26 , 1256 , in the quasar 2 cohort ; 18 , 1130 , for ovarian carcinoma ; 16 , 1024 , for uterine sarcoma ; 143 , 068299 , for prostate carcinoma ; and 19 , 1131 , for endometrial carcinoma )  . 
 chromatin heterogeneity was a significant predictor of cancer - specific survival in microsatellite unstable ( hr 29 , 95% ci 1084 ) and microsatellite stable ( 18 , 1227 ) stage ii colorectal cancer , but microsatellite instability was not a significant predictor of outcome in chromatin homogeneous ( 13 , 0724 ) or chromatin heterogeneous ( 08 , 0320 ) stage ii colorectal cancer . interpretation the consistent prognostic prediction of nucleotyping in different biological and technical circumstances suggests that the marker of chromatin heterogeneity can be reliably assessed in routine clinical practice and could be used to objectively assist decision making in a range of clinical settings . 
clinical trials are warranted to evaluate the survival benefit and cost - effectiveness of using nucleotyping to guide treatment decisions in multiple clinical settings . funding the research council of norway , the south - eastern norway regional health authority , the national institute for health research , and the wellcome trust . copyright the author ( s )  . 
we also searched the digital publications collection at the university of oslo ( oslo , norway ) using the terms texture analysis and microscopy images to locate relevant academic theses submitted to the university of oslo in which different methods for detecting chromatin aberrations had been evaluated and compared . attempts to correlate changes in chromatin organisation with cancer diagnosis and prognosis have been made for many decades . 
early findings suggested that accurate identification of disease and patient outcome could be obtained by applying complex image analysis methods on images that depict the chromatin organisation in cell nuclei , but there is an absence of independent validation in external cohorts . we have previously shown that image patterns associated with aberrant chromatin organisation is associated with poor prognosis in many cancers , but none of the developed markers are suitable for validation on external cohorts of different cancer types . added value of this study we have shown that heterogeneous chromatin organisation can be reliably assessed by machine learning algorithms without being adapted for various cancer types or distinct methods and equipment used to prepare the samples and image the nuclei . 
validation of the chromatin heterogeneity marker , termed nucleotyping , in external cohorts shows that chromatin heterogeneity predicts cancer - specific survival of patients with colorectal cancer , ovarian carcinoma , uterine sarcoma , and endometrial cancer independently of established prognostic markers . 
in stage ii colorectal carcinoma , cancer - specific survival was stratified more precisely by chromatin heterogeneity than by microsatellite instability . implications of all the available evidence the generic utility of nucleotyping warrants study of its molecular basis and suggests that it could enhance selection of patients for adjuvant treatment . dna organisation can be described by the texture of cell nuclei stained specifically for dna , and abnormal structure has been linked to poor prognosis in cancer.6 in previous assessments of chromatin aberrations , machine learning algorithms were trained on part of a patient cohort with one specific cancer type and validated on the complementary part of the same cohort . 
the analysed tissue samples were usually prepared and imaged using the same methods and equipment , and attempts to make the assessments of chromatin aberrations robust to moderate technical deviations have rarely been made , which severely limits their applicability , not only in the clinic , but also in research facilities . 
despite obvious limitations , findings from previous studies of this type ( eg , our own studies on ovarian carcinoma , 7 uterine sarcoma , 8 prostate carcinoma , 9 and endometrial carcinoma10 ) suggest that such alterations in chromatin organisation could be a consistent finding in carcinogenesis . 
we hypothesised that generic texture patterns of aberrant chromatin could be detectable in most cancer types and wanted to reliably detect these patterns independently of moderate deviations in preparation methods and imaging equipment . 
to this end , we developed an automated method to robustly identify such patterns and independently validated this marker , termed nucleotyping , in a range of cancer types . methods patient cohorts between 1993 and 2003 , 494 consecutive patients with primary colorectal cancer at aker university hospital ( oslo , norway ) had resection of non - synchronous stage i and ii tumours.11 , 12 390 of these patients were included in our discovery cohort ( figure 1a ; table 1 )  . 
 two ( < 1% ) patients received adjuvant chemotherapy , and 324 ( 83% ) patients did not ; the information was missing for the remaining 64 ( 16% ) patients . 
an experienced pathologist ( as ) did the pathology analyses . the gloucester colorectal cancer validation cohort included 442 of the 467 patients with non - synchronous stage i or ii colorectal cancer from the gloucester colorectal cancer study ( uk ) , who were recruited between 1988 and 1996 ( figure 1b , table 1 ) .13 , 14 data on adjuvant radiotherapy and chemotherapy were available for 310 ( 70% ) patients , of whom 23 ( 7% ) received adjuvant treatment and 287 ( 93% ) did not . 
this study was approved by the gloucestershire local research ethics committee ( number 01 / 21g ) and rek in norway ( number 2015 / 1606 ) , and the pathology analyses were done by an expert pathologist ( nas )  . vol 19 march 2018 articles a 494 patients with stage i or ii colorectal cancer from aker university hospital ( discovery cohort ) 467 patients with stage i or ii colorectal cancer ( gloucester validation cohort ) 441 patients with stage ii colorectal cancer ( quasar 2 validation cohort ) 62 excluded 16 died of postoperative complications 46 unknown cause of death 432 eligible 467 eligible 441 eligible 42 unsuccessful sample preparation 16 no tumour material 26 poor specimen quality 25 unsuccessful sample preparation 19 no tumour material 6 poor specimen quality 50 unsuccessful sample preparation 36 no tumour material 14 poor specimen quality 390 analysed 342 patients with stage i ovarian carcinoma 442 analysed 391 analysed 587 patients with uterine sarcoma 317 patients with prostate carcinoma 39 excluded 2 died of postoperative complications 37 lost to follow - up 197 excluded 29 surgery not performed 9 specimen not received 159 not uterine sarcoma ( reviewed diagnosis ) 3 excluded 1 preoperative radiotherapy 1 died of postoperative complications 1 lost to follow - up 303 eligible 390 eligible 314 eligible 57 unsuccessful sample preparation 3 no tumour material 54 poor specimen quality 36 unsuccessful sample preparation 15 no tumour material 21 poor specimen quality 7 unsuccessful sample preparation 7 no tumour material 354 analysed 307 analysed 246 analysed 1046 patients with endometrial carcinoma 95 excluded 95 lost to follow - up 160 unsuccessful sample preparation 38 no tumour material 122 poor specimen quality 951 eligible 791 analysed figure 1 : consort diagrams showing the origin of each patient cohort ( a ) colorectal cancer discovery cohort . 
 ( g ) endometrial carcinoma cohort . 358 vol 19 march 2018 articles the quasar 2 trial ( isrctn registry number isrctn45133151 ) established a biobank that included formalin - fixed , paraffin - embedded tumour tissue blocks from 441 patients with stage ii colorectal cancer.15 data from 391 patients were available for the second colorectal cancer validation cohort ( figure 1c ; table 1 )  . 
approval for the study was obtained from the west midlands research ethics committee ( number 04 / mre / 11 / 18 ) and rek in norway ( number 2015 / 1607 )  . 
 the pathology assessments were done by pathologists at the participating hospitals in the trial . tertiary 246 patients treated for international federation of gynecology and obstetrics ( figo ) stage i ovarian carcinoma between 1982 and 1989 ( surgery at county hospitals and evaluation of further treatment at the norwegian radium hospital , a referral comprehensive cancer centre in oslo , norway ) were analysed as an ovarian cancer validation cohort ( figure 1d ; appendix p 6 ) .7 all patients provided verbal informed consent , and the study was in accordance with norwegian law . 
a single pathologist ( vma ) masked to patient outcome reviewed the histological sections using who criteria . lymphadenectomy was not we confirmed the diagnosis and obtained adequate tumour material from 354 patients with uterine sarcoma reported to the norwegian cancer registry between 1970 and 2000 to make up the uterine sarcoma validation cohort ( figure 1e ; appendix p 7 ) .8 , 16 all patients in this cohort had a hysterectomy , but records on the precise surgical procedure and additional treatment are not available . 
the study of the total population of uterine sarcoma patients in norway was approved by rek ( number s - 04298 )  . investigator from 1987 to 2005 , 317 consecutive patients underwent the norwegian open retropubic prostatectomy at radium hospital.9 , 17 one ( hw ) was responsible for treatment and follow - up . 
307 patients were included in the prostate cancer validation cohort ( figure 1f ; appendix p 8 ) , and the study was approved by rek ( number s - 07443a )  . 
 * acute surgery was done because of obstruction or perforation of the bowel at presentation in the discovery cohort , and defined as either urgent or emergency surgery in the gloucester validation cohort . table 1 : baseline characteristics of patients with colorectal carcinoma in the discovery and validation cohorts 791 tumour samples from consenting patients with treated between endometrial carcinoma who were 2001 and 2011 in the molecular markers in treatment of endometrial cancer ( momatec ) trial ( nct00598845 ) were included in the endometrial carcinoma validation cohort ( figure 1g ; appendix p 9 ) .10 767 patients had hysterectomy , three patients had tumour reduction , and 21 patients had curettage . 
to account sample preparation and imaging images of cell nuclei were acquired from curettage specimens for patients with endometrial carcinoma and from the surgically resected tumours for all other patients . 
 one of several pathologists selected a representative tumour region for each patient from haematoxylin and eosin - stained sections of the formalin - fixed , paraffinembedded for heterogeneity , 20 three regions ( iqr three to four ) from different tumour blocks were included for prostate carcinoma patients . 
one or more 50 m sections of each selected tumour region was used to obtain isolated nuclei using a modification of hedleys method.21 after rehydration , the sections were enzymatically digested at room temperature at 200 rotations per min ( rpm ) for 70 min ( for colorectal and prostate specimens ) or 60 min ( for other specimens ) with 05 mg / ml protease ( sigma protease type xxiv [ p5380 ] or type viii [ p8038 ] ; sigma chemical , st louis , mo , usa ) to disaggregate the cells . 
 the cell suspension was filtered through a 60 m mesh nylon filter , washed , and cytospun ( 600 rpm for 5 min ) onto a poly - l - lysine - coated slide.22 the nuclei were stained using feulgens method , and slides were incubated in 5 m hcl for 60 min at room temperature for hydrolysis , stained with schiffs solution for 2 h in the dark , rinsed in a fresh solution of 05% sodium metabisulfite in 005 m hydrochloric acid ( three times 10 min ) , dehydrated , and coverslipped.21 , 22 feulgen - stained nuclei were imaged by a zeiss axioplan microscope equipped with a 546 nm green filter and a monochrome high - resolution digital camera ( axiocam mrm , zeiss , jena , germany , or c4742 - 95 , hamamatsu photonics , hamamatsu , japan ) with a depth of field of about 15 in the resulting images , the value of each pixel reflects the dna density at that location and is referred to as the pixel grey level . 
although the sample preparation method and imaging equipment were similar within each cohort except for the prostate carcinoma cohort , methodological and equipment updates were implemented between work on different sample series , and images from the entire set of cohorts thus have notably different technical features ( eg , in image contrast and number of nuclear pixels )  . 
 additionally , a single pathologist selected the tumour regions for all patients in the three colorectal carcinoma cohorts , the ovarian car cinoma cohort , and the uterine sarcoma cohort ( although the pathologist was not the same across these cohorts ) , whereas the selections were done by multiple pathologists in each of two other cohorts . nuclei of interest in the ovarian carcinoma cohort as those that appeared to be whole , isolated , and epithelial.7 in all other cohorts , the ploidy work station ( pws , room4 , sussex , uk ) was applied to automatically discard non - intact nuclei ( eg , cut , folded , and connected ) and to detect cell types . 
the initial method23 was used in the uterine sarcoma cohort , and only non - necrotic , intact nuclei were kept for further analysis.8 the analysis was further restricted to epithelial nuclei in the colorectal , prostate , and endometrial carcinoma cohorts . 
trained personnel verified the automatic nucleus classifications in all cohorts , except in the two colorectal cancer validation cohorts because by then we considered the method in pws to be both robust and accurate enough to allow completely automated identification of nonnecrotic , intact epithelial nuclei . 
43 million images of cell nuclei from the 2921 analysed patients were included in further analysis , giving an average of about 1200 images per tumour region and about 1500 images per patient . 
because images in different cohorts deviated in contrast and size due in sample preparation methods and imaging equipment , the set of images region was single independently normalised using a previously described algorithm that automatically standardises the optical and spatial scales of the images.9 this normalisation method does not depend on external controls and automatically finds internal controls by estimating which nuclei are diploid . 
the resulting images had a physical resolution of about 160 nm / pixel and a pixel depth of ten bits . to differences from each tumour nuclear texture analysis chromatin organisation was quantified by computing the entropy of pixel grey levels in a subregion of a nucleus ( figure 2 )  . 
entropy is a measure of disorder commonly used in thermodynamics but applied here to assess whether the chromatin organisation is disordered in the sense of more interleaved chromatin compartments with different condensations . 
the subregion was taken to be a square region , and the entropy of the region was coupled with the grey level value of the regions centre pixel to integrate measurements of disordered chromatin organisation and dna content . 
the frequency in which each pair of entropy and centre grey level occur throughout a nucleus was stored in a two - way table , known as the grey level entropy matrix ( glem ; figure 2a ) .24 each chromatin pattern ( ie , a subregion with concrete values and arrangement of pixel grey levels ) corresponded to a specific element in the glem . the imaged nuclei were assessed to exclude nonrepresentative cells ( eg , cut or connected nuclei and non - tumour cells )  . 
trained personnel identified the glems stratified on nuclear area ( grouped at 1999 pixels , 10001999 pixels , , 90009999 pixels , and 10 000 pixels or more ) and computed on different scales 360 vol 19 march 2018 articles ( subregions of 3 3 pixels , 5 5 pixels , , 31 31 pixels ) were concatenated to form a four - dimensional expansion of the glem called glem4d.7 each pixel in a nucleus is thus the centre of 15 subregions representing the chromatin organisation near the pixel on different magnifications , and the frequency of these chromatin patterns for all pixels in the nucleus is stored in the glem4d . 
the glem4d was calculated for each of the 461 000 nuclear images in the discovery cohort , and each patient was represented by the average glem4d of the patients nuclei . 
this association was computed for each glem4d element as a constant scaling factor multiplied by the statistic of a two - sample t test that tested for the difference between good and poor prognosis in the specific glem4d element in the discovery cohort . 
the applied adaptive machine learning algorithm25 could then compute the compliance between the glem4d representation of a new patient and the discovered patterns of chromatin aberrations by multiplying each glem4d element with the corresponding scaled t statistic and summing the products . 
 ( 3 ) for each subregion , two quantities are extracted ( the grey level of the centre pixel [ here 22 ] and the entropy of the grey levels in the subregion [ here 32 ] ) ; the entropy h is a variability characteristic of the probability mass function p ( i ) ( ie , the histogram that gives the probability p that grey level i occurs in the subregion )  . 
the occurrence is counted by incrementing the value at the table cell position ( initially , all table cell values are 0 ) , and the computation of the two quantities and incrementation of the corresponding table cell value is performed for every subregion of the nuclear image . 
the resulting table describes the frequency of each pair of centre grey level and surrounding entropy and is normalised by its total count to provide the bivariate probability mass function called the glem . 
the threshold applied to dichotomise the chromatin value was 0044 . vol 19 march 2018 articles see online for video chromatin value , which describes the overall amount of chromatin disorder in a given patient . 
finally , the robust minimum euclidean distance classification method26 , 27 was applied to calculate a fixed threshold with which to dichotomise the chromatin value into a classification of the tumour as either chromatin homogeneous or chromatin hetero geneous . 
the threshold was computed using the discovery cohort ( 0044 ) , but other thresholds provided markers with similar accuracy in the discovery cohort when measured by hazard ratio , although with different abilities to correctly identify patients as good and poor prognosis ( appendix p 23 )  . 
 nucleotyping could subsequently be applied blindly to label new , individual patients as chromatin homogeneous or chromatin heterogeneous on the basis of the glem4ds computed from its nuclear images . in an average chromatin heterogeneous tumour , 63% ( iqr 5273 ) of the nuclei expressed aberrant chromatin patterns . 
the proportion of nuclei required for a tumour to be labelled as chromatin heterogeneous was not fixed because the classification of a tumour sample was based on the average estimated severity of its nuclei ( the scaled t statistic of the chromatin patterns in the nucleus ) , which in turn was calculated as the average severity of all observed chromatin patterns in the nuclear image . 
thus , a relatively small proportion of nuclei ( minimum in the analysed cohorts was 36% ) expressing highly severe chromatin patterns could define the tumour as chromatin heterogeneous , whereas a chromatin homogeneous tumour could have a relatively large proportion of nuclei ( maximum in the analysed cohorts was 57% ) with chromatin patterns associated with mild disorganisation . statistical analysis we measured cancer - specific survival because it was considered the most clinically relevant endpoint that was common to all patient cohorts . 
each analysis included only patients with complete data for the variables in question , but imputation for missing data was subsequently done using multiple imputation by chained equations to assess all patients . 
the clinical and pathological markers included in multivariable analyses were the same as those that had been used in the previous studies of the individual patient cohorts710 , 12 or , in case of the colorectal cancer validation cohorts , were the same prognostic markers as those applied to the discovery cohort . 
 subsequently , number of investigated lymph nodes ( < 12 vs 12 ) and tumour sidedness ( left vs right ) were separately added to the multivariable model . we did sensitivity analyses by repeating analyses without patients who had received neoadjuvant or adjuvant treatment , or both . 
associations were evaluated with spearmans correlation coefficients . a likelihood ratio test was used to assess whether improved the inclusion of chromatin heterogeneity prediction of cancer - specific survival compared with a multivariable model without chromatin heterogeneity . 
the proportion of patients with chromatin heterogeneous tumours who died of their cancer ( positive predictive value ) , the proportion of patients with chromatin homogeneous tumours who did not die of their cancer ( negative predictive value ) , and the proportion of patients who were either both chromatin heterogeneous and died of their cancer or chromatin homogeneous and did not die of their cancer ( correct classification rate ) were computed to quantify how well chromatin heterogeneity corresponded with the final patient outcome . and non - event - net category - free net reclassification improvement can be defined as the sum of the event - net reclassification improvement reclassification improvement.29 event - net reclassification improvement is the probability of the new model to estimate worse cancerspecific survival than the old model in the case of an event , minus the probability of the new model to estimate better cancer - specific survival than the old model in the case of an event . 
non - event - net reclassification improvement is the probability of the new model to estimate better cancerspecific survival than the old model in the case of no event , minus the probability of the new model to estimate worse cancer - specific survival than the old model in the case of no event . 
we used category - free net reclassification improvement to evaluate the reclassification from using only microsatellite stability status to using both nucleotyping and microsatellite stability status to predict the outcome for patients with stage ii colorectal cancer . a two - sided p value of less than 005 was considered statistically significant . 
an had access to the raw data for the discovery cohort , nas for the gloucester validation cohort , djk for the quasar 2 validation cohort , gbk for the ovarian carcinoma and uterine sarcoma cohorts , hw for the prostate carcinoma cohort , and jt for the endometrial carcinoma cohort . 
 articles author had full access to all of the data and the final responsibility to submit for publication . results in the colorectal cancer discovery cohort ( n = 390 ) , 155 ( 40% ) patients had chromatin heterogeneous tumours and 235 ( 60% ) had chromatin homogeneous tumours . 
 patients with chromatin heterogeneous tumours had shorter cancer - specific survival than patients with chromatin homogeneous tumours , both in univariable analysis ( hazard ratio [ hr ] 17 , 95% ci 1225 ) and multivariable analysis ( 17 , 1125 ; figure 3a ; table 2 ; appendix p 10 ) , and when imputing missing data for variables in the multivariable model ( 17 , 1225 )  . 
 adding tumour sidedness ( left vs right ) to the multivariable model did not substantially alter the results ( hr 16 , 95% ci 1124 ) , nor did removing the 11 patients ( all with chromatin homogeneous tumours ) who received neoadjuvant or adjuvant treatment , or both ( 17 , 1226 )  . 
analysis of the gloucester cohort replicated the results from the discovery cohort ( figure 3b ; table 2 ; appendix p 11 ) , and chromatin heterogeneity was also prognostic when imputing missing data ( hr 19 , 95% ci 1133 ) or including number of investigated lymph nodes ( < 12 vs 12 ; 18 , 1032 ) or tumour sidedness ( 19 , 1132 ) in the multivariable model . 
excluding the 29 patients who received neoadjuvant or adjuvant ( 23 patients with chromatin treatment , or both six with tumours and tumours ) , gave similar estimates homo geneous chromatin heterogeneous univariable analysis ( hr 19 , 95% ci 1135 ) and multivariable analysis ( 20 , 1136 )  . 
in patients with stage ii colorectal cancer , 5 - year cancer - specific survival was 85% ( 95% ci 7889 ) for patients with chromatin homogeneous tumours ( 31 [ 12% ] deaths out of 254 patients ) and 72% ( 5981 ) for patients with chromatin heterogeneous tumours ( 22 [ 21% ] deaths out of 105 patients )  . in univariable analysis ; 26 , 12 - 56 in the quasar 2 colorectal cancer validation cohort , 147 ( 38% ) of 391 patients had chromatin heterogeneous tumours and 244 ( 62% ) had chromatin homogeneous tumours . 
cancer - specific survival was shorter in patients with chromatin heterogeneous tumours than in those with chromatin homogeneous tumour ( hr 22 , 95% ci 11 - 45 multivariable analysis ; figure 3c ; table 2 ; appendix p 12 )  . 
the multivariable result was not substantially altered by additionally adjusting for the number of investigated lymph nodes ( hr 27 , 95% ci 1259 ) or tumour sidedness ( 28 , 1363 )  . 
5 - year cancer - specific survival was 94% ( 95% ci 9097 ) for patients with tumours ( 13 [ 5% ] deaths out of 244 patients ) and 88% ( 8092 ) for patients with chromatin heterogeneous tumours ( 16 [ 11% ] deaths out of 147 patients )  . chromatin homogeneous versus in a pooled analysis of all three colorectal cancer cohorts , chromatin heterogeneity was independent of sex , stage ( ii vs i ) , and pathological tumour stage ( t4 vs t3 vs t2 vs t1 ; appendix p 13 )  . 
no association was found for chromatin colon heterogeneity correlated weakly with tumour sidedness ( p = 012 , 95% ci 007018 ; p < 00001 ) and therefore tumour location ( p = 00010 ; appendix p 13 )  . 
 ( p = 048 ) , but rectum colorectal cancer , discovery colorectal cancer , gloucester validation colorectal cancer , quasar 2 validation ovarian carcinoma uterine sarcoma prostate carcinoma endometrial carcinoma univariable analysis multivariable analysis * likelihood ratio test * hr ( 95% ci ) p value hr ( 95% ci ) p value p value 17 ( 1225 ) 18 ( 1030 ) 22 ( 1145 ) 31 ( 1950 ) 25 ( 1834 ) 23 ( 1246 ) 00056 0033 0027 < 00001 < 00001 0012 43 ( 2868 ) < 00001 17 ( 1125 ) 00096 00096 19 ( 1132 ) 26 ( 1256 ) 18 ( 1130 ) 16 ( 1024 ) 14 ( 0730 ) 19 ( 1131 ) 0026 0016 0022 0038 034 0013 0030 0015 0021 0035 035 0014 hr = hazard ratio . 
 * in each colorectal cancer cohort , chromatin heterogeneity was added to the multivariable model consisting of age , stage , histological grade , and surgery type , although stage was not relevant and surgery type data were not available for the quasar 2 validation cohort . 
for the uterine sarcoma cohort , the model consisted of histological subtype , mitotic index , tumour extent , tumour size , tumour margins , cellular atypia , tumour necrosis , hyaline necrosis , and vascular invasion . 
for the prostate cancer cohort , the model consisted of age , preoperative prostate - specific antigen , gleason grade , surgical margins , extracapsular extension , seminal vesicle invasion , and pathological node stage . 
 in a pooled analysis of stage ii colorectal cancer , the hr between patients with chromatin heterogeneous and chromatin homogeneous tumours was similar across subgroups of each patient characteristic ( figure 4 )  . 
 cancer - specific chromatin heterogeneity predicted survival more accurately than micro satellite stability status ( stable vs unstable ) and provided prognostic information for patients with microsatellite unstable and microsatellite stable stage ii colorectal cancer ( figure 5 ; appendix p 14 )  . 
in a multi variable model with microsatellite stability status , cancer - specific survival was shorter in patients with stage ii colorectal cancer with chromatin heterogeneous tumours compared with patients with chromatin homogeneous tumours ( hr 19 , 95% ci 1328 )  . 
the category - free net reclassification improvement of supplementing microsatellite stability status with nucleotyping for prediction of 5 - year cancerspecific survival in stage ii colorectal cancer patients was 311% ( 95% ci 27545 ) ; the event - net reclassification improvement was 75% , and the non - event - net reclassification improvement was 236% . of 246 patients in the ovarian carcinoma cohort , 77 ( 31% ) had chromatin heterogeneous tumours and 169 ( 71% ) had chromatin homogenous tumours . 
5 - year cancer - specific survival was 88% ( 95% ci 8292 ) for patients with chromatin homogeneous tumours ( 21 [ 12% ] deaths out of 169 patients ) and 68% ( 5677 ) for patients with chromatin heterogeneous tumours ( 25 [ 32% ] deaths out of 77 patients )  . ( 43% ) had chromatin heterogeneous of the 354 patients in the uterine sarcoma cohort , 201 ( 57% ) had chromatin homogeneous tumours and tumours . 
 153 chromatin heterogeneity predicted 5 - year cancer - specific survival in univariable analysis ( figure 3e ) , performed consistently across a range of clinicopathological subgroups , and was significant in multivariable analyses ( table 2 ; appendix pp 16 , 25 )  . 
chromatin heterogeneity remained prognostic in both univariable ( hr 24 , 95% ci 1831 ) and multivariable ( 14 , 1020 ) analysis of cancer - specific survival , also when missing data were imputed . 
5 - year cancer - specific survival was 67% ( 95% ci 6174 ) for patients with chromatin homogeneous tumours vol 19 march 2018 articles ( 65 [ 32% ] deaths out of 201 patients ) and 35% ( 2843 ) for patients with tumours ( 97 [ 63% ] deaths out of 153 patients )  . chromatin heterogeneous 55 ( 18% ) of the 307 patients in the prostate carcinoma cohort had chromatin heterogeneous tumours ; the other 252 ( 82% ) patients had chromatin homogeneous tumours . 
in univariable analysis , cancer - specific survival was shorter in patients with chromatin heterogeneous tumours than in patients with chromatin homogeneous tumours , but there was no significant difference in multivariable analysis ( figure 3f ; table 2 ; appendix pp 17 , 26 ) or when performing imputation for missing data ( hr 143 , 95% ci 071290 ; p = 032 )  . 
chromatin homogeneous heterogeneity was prognostic independent of age at surgery and curettage histology classification ( table 2 ; appendix pp 18 , 27 ) , also when imputing missing data ( hr 19 , 95% ci 1232 )  . 
5 - year cancer - specific survival was 90% ( 95% ci 8692 ) for patients with chromatin homogeneous tumours ( 50 [ 7% ] deaths out of 673 patients ) and 62% ( 4972 ) for patients with chromatin heterogeneous tumours ( 32 [ 27% ] deaths out of 118 patients )  . 
exclusion of the 260 patients who received adjuvant treatment ( 192 with chromatin homogeneous tumours and 68 with chromatin heterogeneous the univariable analysis ( hr 109 , 95% ci 48248 ) and multivariable analysis ( 46 , 18113 ; appendix pp 19 , 28 )  . increased tumours ) the hr the negative predictive value exceeded 90% in the two colorectal cancer validation cohorts , the prostate cancer cohort , and the endometrial carcinoma cohort , but the positive predictive value in these cohorts was not higher than 27% ( appendix p 20 )  . 
the positive predictive value was higher in the two remaining validation cohorts ( 47% in the ovarian carcinoma cohort and 63% in the uterine sarcoma cohort ) , but the negative predictive value was 82% and 68% , respectively ( appendix p 20 )  . 
 sensitivity , specificity and correct classification rate for all cohorts are shown in the appendix ( p 20 )  . the chromatin heterogeneity low positive showed correlation with histological grade three gynaecological cancer cohorts and in the prostate cancer cohort , low negative correlation with histological grade in the gloucester validation cohort , and no correlation with histological grade in the discovery cohort or the quasar 2 validation cohort ( appendix p 21 )  . 
the hr of the the multivariable analysis with grade ( appendix p 21 ) was similar to the hr derived in the full multivariable analyses ( table 2 )  . chromatin heterogeneity marker from tumours ; of the 2858 patients with assessable dna ploidy , 1354 ( 47% ) had diploid tumours , of which eight ( < 1% ) had chromatin heterogeneous the remaining 1346 ( > 99% ) patients had chromatin homogeneous tumours . 
in the three colorectal cancer cohorts , chromatin heterogeneity divided the non - diploid tumours into two groups of similar size ( 354 [ 45% ] of 785 patients with chromatin homogeneous tumours and 431 [ 55% ] of 785 patients with chromatin heterogeneous tumours ) and was not associated with tetraploidy versus aneuploidy ( p = 036 )  . 
correspondingly , chromatin homogeneity was detected in 68 ( 47% ) of 144 non - diploid tumours in the ovarian carcinoma cohort , 93 ( 38% ) of 244 non - diploid tumours in the uterine sarcoma cohort , 73 ( 57% ) of 127 in the prostate carcinoma cohort , and 95 ( 47% ) of 204 in the endometrial carcinoma cohort . 
diploid chromatin homogeneous tumours were associated with longer cancer - specific survival than were non - diploid chromatin homogeneous tumours in all cohorts , whereas patients with chromatin heterogeneous tumours consistently had the worst survival ( appendix p 22 )  . irrespective of discussion in all six independent validation cohorts , across a range of tumour types , and in the discovery cohort , chromatin heterogeneity correlated with cancer - specific survival . 
 this suggests that chromatin heterogeneity might be a novel pan - prognostic factor tumour histogenesis , and could add value to the traditional tnm staging syste nucleotyping provided independent prognostic information beyond most conventional markers in multivariable analyses . 
our data permitted more in - depth analysis of stage ii colorectal cancer , for which nucleotyping was found to be weakly associated with other patient characteristics and predicted cancerspecific survival more accurately than microsatellite instability . 
however , much remains to be discovered of the biology underpinning chromatin heterogeneity and whether these descriptive changes are associated with specific drivers and carcinogenic pathways or are reflective of a relatively non - specific burden of accumulated dna damage . recently developed normalisation beside the fundamental biological differences between the analysed cancer types , the images from the various cohorts were acquired using different sample preparation methods and imaging equipment , which cause notable dissimilarities between the images , particularly when using rigid analytical nomograms . 
similarly , the pathologist who selected the tumour region and the bioengineers who prepared the samples differed between cohorts , thus the consistent validation results suggest that the marker is independent of individual human influence . 
 requirement we have begun the process of obtaining iso certification for the nucleotyping procedure . for earlier methods for assessing aberrant chromatin organisation have been reported the ovarian carcinoma , 7 uterine sarcoma , 8 prostate carcinoma , 9 and endometrial carcinoma cohorts.10 the major difference from the present study is that in those studies , a different marker was developed in each cohort , which allowed adaption to the particular cancer type , sample preparation methods , and imaging equipment . 
none of the earlier vol 19 march 2018 articles developed markers are suitable for validation on external cohorts of different cancer types , and they were only validated internally in the same patient series used to develop the marker . 
we therefore find it remarkable that the generic marker developed in this study offered similar prognostic ability in analysis of ovarian and endometrial carcinoma and depicted the prognosis of uterine sarcoma and prostate carcinoma with only slightly less accuracy compared with the pooled analyses of the discovery and internal validation cohorts that were reported in those studies . 
it thus appears that the technical standardisation applied in the generic marker preserves prognostic information and that texture patterns identifying chromatin heterogeneity are essentially identical in most cancer types . the proportion of patients with chromatin homogeneous and heterogeneous tumours who died of their cancer differed between cancer types , suggesting that appropriate use of the chromatin heterogeneity marker in the clinic might differ between clinical settings . 
the role of chromatin heterogeneity , as well as options for treatment and survival benefits , must therefore be investigated in conjunction with disease type and characteristics . in stage ii colorectal cancer , our finding of a somewhat improved survival in the quasar 2 cohort compared with the other two colorectal cancer cohorts perhaps reflects modern advances in chemotherapy and a more consistent application of adjuvant chemotherapy . 
the correlation between nucleotyping and other patient characteristics were either weak or absent , and the similar prognostic ability in univariable and multivariable analysis of each colorectal cancer cohort further indicates that the correlations do not substantially affect nucleotypings ability to predict cancer - specific survival and might therefore be unimportant in practice . 
this could explain why the proportions of patients with chromatin homogeneous and heterogeneous tumours were similar in all three cohorts despite the fact that the quasar 2 series represents a different clinical setting than the discovery and gloucester validation cohorts . the investigators of original quasar trial found that adjuvant chemotherapy reduces the odds of tumour recurrence and death by about 20% in stage ii colorectal cancer , leading to a 5 - year absolute survival advantage of about 4% assuming that the 5 - year mortality without chemotherapy is 20%.30 microsatellite stability status is often used in clinical practice to identify a subgroup of patients with stage ii colorectal cancer for whom adjuvant treatment can be omitted because these patients are at low risk of recurrence and would therefore have a small ( around 2% ) absolute benefit of adjuvant treatment.3133 our data suggest that patients with chromatin heterogeneous tumours have poor cancer - specific survival irrespective of microsatellite stability status , and the slight difference in mortality between microsatellite unstable and microsatellite stable tumours in patients with times chromatin homogeneous tumours was not significant . 
 individually , the chromatin homogeneous subgroup and the microsatellite unstable subgroup were associated with equally good prognosis ( 5 - year cancer - specific survival 89% for chromatin homogeneous tumours and 88% in microsatellite unstable tumours ) , but the chromatin homogeneous subgroup was several larger ( about 60% of patients with stage ii colorectal cancer had chromatin homogeneous tumours vs 1015% of patients who had microsatellite unstable tumours ) , thus allowing substantially more patients to be identified as low risk and with a small absolute benefit of adjuvant chemotherapy . 
 moreover , the patients with chromatin heterogeneous tumours have lower cancer - specific survival than patients with microsatellite stable tumours and could therefore be expected to have a greater absolute survival benefit from adjuvant treatment , assuming , reasonably , that the proportional benefits of chemotherapy remain constant over the different prognostic groups . our findings suggest that heterogeneous chromatin organisation is found in many cancer types and that its presence signifies increased risk of death due to cancer . 
this assay might potentially be cost - effective as it could possibly reduce adjuvant overtreatment of patients who are at relatively low risk of recurrence and death , thus diminishing the burden of toxicity on patients treated unnecessarily and the direct costs of cancer therapy . 
focusing or intensifying adjuvant treatment on those most at risk of death due to cancer is consistent with the wider precision medicine agenda in oncology . the main limitation of this study is that it investigates the prognostic ability of chromatin heterogeneity but not the survival benefit and cost - effectiveness of utilising nucleotyping to guide treatment decisions . 
however , we expect positive findings in this respect because of the preserved or enhanced accuracy of nucleotyping in sensitivity analyses where patients who received adjuvant therapy were excluded , and our experience with the sample preparation method relative to the costs of assessing other markers . 
we also see a potential to improve the cost - benefit ratio by assessing chromatin heterogeneity using routine histological sections with a dna - specific sta another limitation is that tumour heterogeneity was not considered except in prostate cancer where it was partly handled by analysing about three regions from each tumour ; sampling the entire tumour should increase the prognostic accuracy of the marker . in conclusion , our results indicate that chromatin in several human heterogeneity behaves similarly cancers and identifies patients at increased risk of cancer - specific death , independently of established prognostic markers , and could possibly aid clinical decision making around use of adjuvant or neoadjuvant therapy . 368 vol 19 march 2018 articles contributors ak , fa , djk , and hed were involved in study design . 
ak wrote the first draft , and all authors reviewed , contributed to , and approved the manuscript . declaration of interests the university of oxford ( to djk ) received an educational grant from roche to support the quasar 2 trial . 
all other authors declare no competing interests . acknowledgments this study was funded by the research council of norway , through its iktpluss lighthouse program ( 259204 ) and through its centres of excellence funding scheme ( 179571 ) , the south - eastern norway regional health authority ( 2012027 and 2015070 ) , the national institute for health research ( to the oxford nihr comprehensive biomedical research centre ) , and the wellcome trust ( to the wellcome trust centre for human genetics , 090532 / z / 09 / z )  . 
we thank ragnhild a lothe for her contribution to the colorectal cancer dataset from aker university hospital , vera m abeler for pathological review of the uterine sarcoma and ovarian carcinoma cohorts , aud svindland for pathological assessment of the colorectal carcinoma specimens in the discovery cohort , paul callaghan for animating the appendix video , marian seiergren for creating figure 2 and editing figures 35 , wanja kildal , marna lill kjreng , elin ersvr , john arne nesheim , ily kostolomov , rolf anders syvertsen , and the laboratory personnel at the institute for cancer genetics and informatics for assistance , and the reviewers for valuable suggestions . 
we also thank the participating centres in the quasar 2 trial and the momatec trial as well as the staff at aker university hospital , west gloucestershire , and the norwegian radium hospital . 
we sought to establish whether indocyanine green fluorescent dye is non - inferior to isosulfan blue dye in detecting sentinel lymph nodes in women with cervical and uterine cancers . methods in this non - inferiority , within - patient comparison study , patients aged 18 years or older with clinical stage i endometrial or cervical cancer undergoing curative surgery were randomly assigned 1 : 1 to lymphatic mapping with isosulfan blue dye ( visualised by white light ) followed by indocyanine green ( visualised by near - infrared imaging ) , or indocyanine green followed by isosulfan blue dye . 
 the primary outcome was efficacy of intraoperative indocyanine green with near - infrared fluorescence imaging versus that of isosulfan blue dye in the identification of lymph nodes , defined as the number of lymph nodes identified by indocyanine green and isosulfan blue dye , respectively ( and confirmed as lymphoid tissue by histology ) , divided by the number of lymph nodes identified intraoperatively and excised . 
the study had a 5% non - inferiority margin needed to show non - inferiority of the frequency of lymph node detection with indocyanine green to that with isosulfan blue dye with 80% power at a 5% two - sided significance level . 
the trial was registered with clinicaltrials.gov , number nct02209532 , and is completed and closed . findings between dec 21 , 2015 , and june 19 , 2017 , 180 patients were enrolled and randomly assigned to the two groups ( 90 to each group ) ; 176 patients received the intervention and were evaluable ( modified intention - totreat population )  . 
517 sentinel nodes were identified in the per - protocol population ( n = 163 ) , of which 478 ( 92% ) were confirmed to be lymph nodes on pathological processing : 219 ( 92% ) of 238 nodes that were both blue and green , all seven nodes that were blue only , and 252 ( 95% ) of 265 nodes that were green only ( p = 033 )  . 
 in total , 471 ( 97% ) of 485 lymph nodes were identified with the green dye and 226 ( 47% ) with the blue dye ( difference 50% , 95% ci 3962 ; p < 00001 )  . 
in the modified intention - to - treat population ( n = 176 ) , 545 nodes were identified , of which 513 ( 94% ) were confirmed to be lymph nodes on pathological processing : 229 ( 92% ) of 248 nodes that were both blue and green , all nine nodes that were blue only , and 266 ( 95% ) of 279 nodes that were green only ( p = 030 )  . 
the technique of lymphatic mapping and sentinel lymph node biopsy has improved surgeons ability to detect small - volume disease in lymph nodes while greatly reducing intraoperative and postoperative morbidity . 
this technique has been validated and is 1394 vol 19 october 2018 articles research in context evidence before this study before development of the concept for the film study and the production of the subsequent protocol , we reviewed the medical literature to evaluate the off - label use of indocyanine green and near - infrared imaging for lymphatic mapping and sentinel lymph node biopsy in all solid tumours . 
we searched pubmed and clinicaltrials.gov , without date or language restrictions , using the terms indocyanine green , icg , near infrared imaging , lymphatic mapping , and sentinel node . 
we identified several small , single - institution retrospective reports of interstitial injection of indocyanine green for lymphatic mapping in a wide range of solid tumours including breast , uterine , cervical , vulval , lung , kidney , and colon cancers as well as cutaneous melanoma . 
 all these studies showed that use of indocyanine green with near - infrared imaging was feasible and safe for lymphatic mapping in solid tumours and that the technique might potentially improve on substances currently approved by the us food and drug administration for mapping such as patent blue dyes and radiocolloids . 
however , no prospective , controlled studies had compared the use of indocyanine green as a mapping substance with standard of care . added value of this study although the film study was designed as a non - inferiority comparison of the efficacy of intraoperative indocyanine green with near - infrared imaging to blue dye in the identification of lymph nodes , our results showed superiority of the experimental group over standard of care . 
it also identified all sentinel nodes with metastatic disease , whereas isosulfan blue dye missed a large proportion of them . implications of all the available evidence the results of this study will serve as the basis for an application to the food and drug administration for on - label use of interstitial injection of indocyanine green combined with near - infrared imaging for lymphatic mapping . 
if it is approved for on - label use , it will hopefully become the new standard of care for lymphatic mapping and sentinel lymph node biopsy for women with cervical and uterine cancers , and could subsequently be adopted as the mapping substance of choice across multiple subspecialties in surgical oncology . widely accepted as part of the surgical treatment of vulval and breast carcinomas and cutaneous melanoma . 
 gynaecological oncologists are also starting to adopt lymphatic mapping and sentinel node biopsy for women with cervical and uterine cancers.13 in lymphatic mapping for cervical and uterine cancers , mapping agents are most commonly injected into the cervix , a practice that should result in drainage to bilateral sentinel nodes in the pelvis . 
if lymphatic mapping does not identify bilateral sentinel nodes , well accepted algorithms recommend complete pelvic lymphadenectomy on the side with no sentinel nodes detected.4 , 5 because complete pelvic lymphadenectomy increases surgical time and the risks of intraoperative vascular injury and postoperative lower extremity lymphoedema and lymphocyst formation , it is crucial that lymphatic mapping identifies bilateral sentinel nodes . historically , patent blue dye with or without radiocolloid has been the most commonly used agent for lymphatic mapping in women with uterine cancers . 
 however , blue dye alone identifies at least one sentinel node in only 80% of patients and bilateral sentinel nodes in as few as 50% of patients.6 combining blue dye with radiotracer increases the rate of detection of at least one sentinel node to 88% , but the rate of detection of bilateral sentinel nodes to only 51%.6 with either technique , therefore , almost half of women with uterine cancer undergoing lymphatic mapping might require unilateral or bilateral pelvic lymphadenectomy , which increases the risk of surgical complications and long - term morbidity . the fluorescent dye indocyanine green has been explored as an off - label alternative to blue dye for lymphatic mapping in cervical and uterine cancers . 
 small series have shown the potential of interstitial indocyanine green injection to improve frequency of sentinel node detection over that observed with blue dye.79 however , no prospective , randomised studies have compared interstitial blue dye with indocyanine green injections for lymphatic mapping in cervical and uterine cancers . 
we therefore conducted the film ( fluorescence imaging for lymphatic mapping ) trial , which was designed to compare the detection of lymph nodes after interstitial indocyanine green injection versus interstitial isosulfan blue dye injection ( the standard of care ) in women with cervical and uterine cancers . methods study design and participants the film trial was an international , multicentre , randomised , open - label , phase 3 study designed to assess the safety and efficacy of indocyanine green and pinpoint near - infrared fluorescence imaging ( stryker , kalamazoo , mi , usa ) in identification of lymph nodes in women with cervical and uterine malignancies undergoing lymphatic mapping following interstitial vol 19 october 2018 1395 articles see online for appendix cervical injection of coloured dye . 
 comparison we chose this design because it would meet our primary objective and give us reliable results with fewer patients than if we had two separate randomised groups . participating surgeons were required to have completed at least ten lymphatic mapping procedures , including at least three with the pinpoint near - infrared fluorescence imaging system , before the initiation of enrolment . 
 patients were eligible for enrolment if they were 18 years of age or older , diagnosed with international federation of gynecology and obstetrics clinical stage i cervical or uterine cancer ( any histology ) , and were scheduled for curative surgery that included lymph node assessment . 
patients were ineligible if they had previous pelvic dissection or irradiation , advanced cervical or uterine cancer , t3 or t4 lesions , cervical tumour size larger than 2 cm , hepatic dysfunction defined as a model for end - stage liver disease score of 10 or greater , renal dysfunction defined as serum creatinine of 20 mg / dl or greater , or a known allergy to indocyanine green , iodine , iodine dyes , isosulfan blue , or triphenylmethane . the protocol was approved by institutional review boards at each centre , and all patients enrolled gave written informed consent . 
the protocol is available in the appendix ( p 3 )  . randomisation and masking participants were prospectively enrolled into the film trial and underwent random assignment on the day of surgery . 
 participants were randomly assigned on a 1 : 1 basis to either lymph node mapping with isosulfan blue dye followed by lymph node mapping with indocyanine green dye and near - infrared imaging ( pinpoint ) , or lymph node mapping with indocyanine green dye and near - infrared imaging ( pinpoint ) followed by lymph node mapping with isosulfan blue dye . 
randomisation was stratified by study site , with permuted block randomisation within the opportunity for the sequence to be predicted , the block size was variable and randomly chosen from small multiples of two ( ie , two , four , or six )  . 
all participants were masked to their randomisation assignment ( because they were under anaesthesia ) until after the procedure . procedures patients were removed from the study if found to not meet eligibility criteria or if they requested removal at any time before surgery ( patients could request removal at any time during the study )  . 
after general anaesthesia was achieved , the first dye was injected in the cervix deeply and superficially at both 0300 h and 0900 h , followed by the second dye deeply and superficially at both 0300 h and 0900 h , for a total of eight injections . 
for the blue dyeindocyanine green group , the isosulfan blue dye injections were done first , and for the indocyanine greenblue dye group , the indocyanine green injections were done first . 
each blue dye injection consisted of 1 ml of a 10 mg / ml isosulfan blue dye solution ( 1% isosulfan blue ) , for a total dose of 40 mg ; each indocyanine green injection consisted of 1 ml of a 125 mg / ml indocyanine green solution ( novadaq technologies , mississauga , on , canada ) for a total dose of 5 mg . the surgeon identified lymph nodes and lymphatic vessels with white light for isosulfan blue dye ( blue nodes ) or near - infrared imaging with pinpoint for indocyanine green ( green fluorescent nodes ) depending on random isation cohort . 
to minimise the chance that leakage of blue dye or indocyanine green would interfere with mapping , mapping was done first on one side of the pelvis and then on the other side . 
in both patient groups , mapping with the first dye was completed before mapping with the second dye was started , and mapping with both dyes was completed before any lymph nodes were excised . 
mapping with indocyanine green was considered complete when the surgeon identified all green nodes or determined that green nodes could not be identified and the surgeon had scanned the full 360 - degree area within the abdominal cavity . 
 1396 vol 19 october 2018 articles 199 patients screened 19 excluded 180 enrolled and randomly assigned 3 did not receive intervention 1 due to iodine allergy 1 due to negative margins on cone biopsy 1 due to presence of intraperitoneal metastatic disease on laparoscopic exploration 6 protocol violations 2 due to pregnancy test not done on day 0 1 due to incorrect blue dye used 1 due to presence of intraperitoneal metastatic disease on laparoscopic exploration 1 due to no calculation of meld score 1 due to equipment malfunction 90 assigned to blue dyeindocyanine green 90 assigned to indocyanine greenblue dye 87 received intervention and included in mitt analysis 89 received intervention and included in mitt analysis 1 did not receive intervention 1 had excessive bleeding and did not undergo injection of mapping substances 7 protocol violations 3 due to no calculation of meld score 1 due to equipment malfunction 1 due to conversion to open surgery 1 due to incorrect dose of blue and green dye injections 1 due to participation in another trial 81 included in per - protocol analysis 82 included in per - protocol analysis figure : trial profile mitt = modified intention - to - treat . 
 bilateral lymphatic mapping was done according to published national comprehensive cancer network guidelines.4 , 5 all sentinel lymph nodes resected had confirmation of nodal tissue by haematoxylin and eosin staining . 
all participants had standard - ofcare assessments throughout the study according to the hospital or institutions standard procedures , and study - specific visits to monitor occurrence of any adverse events or adverse device effects on postoperative day 1 , the date of discharge , and day 30 ( or within 7 days before or after this date )  . 
 adverse events were characterised as mild , moderate , or severe and assigned relationship ( suspected or not suspected ) to either dyes or device . outcomes the primary endpoint was efficacy of intraoperative indocyanine green with near - infrared fluorescence imaging versus that of blue dye in the identification of lymph nodes , defined as the number of lymph nodes identified by each dye ( and confirmed as lymphoid tissue by histology ) divided by the number of lymph nodes identified intraoperatively and excised . 
secondary end points were the rate of intraoperative detection of at least one sentinel node per patient and the rate of detection of bilateral sentinel nodes with indocyanine green compared with isosulfan blue dye , and the safety of each detection method . 
two other secondary endpoints ( the proportion of lymph nodes identified from following lymphatic channels and the anatomical distribution of lymph nodes ) will be reported in a separate publication . statistical analysis we hypothesised that the use of indocyanine green and near - infrared imaging would be non - inferior to isosulfan blue dye in the detection of sentinel nodes . 
analysis of the primary endpoint was done with a two - sided 95% ci for the difference in proportions using the approach described by nam and kwon for clustered matched - pair data ( the clustering in question being lymph nodes nested within patients ) .11 formal testing for hetero geneity was not completed . 
 results between dec 21 , 2015 , and june 19 , 2017 , 180 patients were enrolled and randomly assigned to the two groups ( 90 to each group ) , of whom 176 received the intervention and were evaluable ( figure )  . 
169 ( 96% ) of 176 patients had uterine cancer and seven ( 4% ) had cervical cancer . after exclusion of 13 patients with major protocol violations ( six in the blue dyeindocyanine green group and seven in the indocyanine greenblue dye group ) , there were 163 in the per - protocol population and primary analytical cohort . 
in this population , 517 nodes were identified intraoperatively and excised , of which 478 ( 92% ) were confirmed to be lymph nodes : 219 ( 92% ) of 238 nodes that were both blue and green , all seven nodes that were blue only , and 252 ( 95% ) of 265 nodes that were green only ( p = 033 ; table 2 )  . 
in total , 471 ( 97% ) of 485 lymph nodes were identified with the green dye and 226 ( 47% ) with the blue dye ( difference 50% , 95% ci 3962 ; p < 00001 )  . 
thus , we were able to conclude that indocyanine green is not inferior to isosulfan blue dye in the identification of nodes . the mean number of nodes per patient in the per - protocol population was 32 ( sd 16 )  . 
at least one node was identified in 159 ( 98% ) of 163 patients with indocyanine green and in 124 ( 76% ) of 163 patients 1398 vol 19 october 2018 articles with isosulfan blue dye ( difference 22% , 95% ci 1732 ; p < 00001 )  . 
bilateral sentinel nodes were identified in 134 ( 82% ) patients , 52 ( 32% ) with isosulfan blue dye and 132 ( 81% ) with indocyanine green ( 49% , 4157 ; p < 00001 )  . 176 evaluable patients received at least one injection of indocyanine green or blue dye and constituted the mitt population . 
545 nodes were identified in total , of which 513 ( 94% ) were confirmed to be lymph nodes : 229 ( 92% ) of 248 nodes that were both blue and green , all nine nodes that were blue only , and 266 ( 95% ) of 279 nodes that were green only ( p = 030 ; table 2 )  . 
thus , we were able to conclude that indo cyanine green is superior to isosulfan blue dye in the identification of nodes . in the mitt population , at least one node was identified in 168 ( 95% ) of 176 patients with indocyanine green and 131 ( 74% ) patients with isosulfan blue dye ( difference 21% , 95% ci 1428 ; p < 00001 )  . 
bilateral sentinel nodes were identified in 54 ( 31% ) of 176 patients with isosulfan blue dye and 138 ( 78% ) of 176 patients with indocyanine green ( 47% , 3056 ; p < 00001 )  . in the 545 nodes ( mean 31 nodes [ sd 17 ] per patient ) identified in the mitt population , isosulfan blue dye identified 257 ( 47% ) sentinel nodes ( mean 15 [ 13 ] per patient ) and indocyanine green identified 527 ( 97% ) sentinel nodes ( mean 30 [ 17 ] per patient ; difference 50% ; 95% ci 3961 ; p < 00001 )  . 
difference estimates and 95% cis indicated that estimates of superiority were consistent throughout all sites ( data not shown )  . randomisation group did not affect the ability of isosulfan blue dye or indocyanine green to detect any or bilateral sentinel nodes in the mitt population . 
in the 87 patients in the blue dyeindocyanine green group , at least one sentinel node was identified in 63 ( 72% ) patients with isosulfan blue dye and in 83 ( 95% ) patients with indocyanine green . 
in the 89 patients in the indocyanine greenblue dye group , at least one sentinel node was identified in 68 ( 76% ) patients with isosulfan blue dye and in 85 ( 96% ) patients with indocyanine green . 
in the indocyanine greenblue dye group , isosulfan blue dye detected a sentinel node in two ( 2% ) patients without a sentinel node detected by indocyanine green . per - protocol population modified intention - to - treat population proportion detected p value p value proportion detected 033 030 219 / 238 229 / 248 indocyanine green only 252 / 265 confirmation of nodal tissue in sentinel lymph node blue dye plus indocyanine green blue dye only identification of one or more sentinel lymph nodes indocyanine green only blue dye only identification of bilateral sentinel lymph nodes indocyanine green only blue dye only 100% 159 / 163 124 / 163 132 / 163 54 / 163 100% 266 / 279 168 / 176 131 / 176 138 / 176 54 / 176 < 00001 < 00001 < 00001 < 00001 table 2 : sentinel lymph node identification by indocyanine green and isosulfan blue dye in the blue dyeindocyanine green group , isosulfan blue dye identified bilateral sentinel nodes in 28 ( 32% ) of 87 patients , indocyanine green identified bilateral sentinel nodes in 67 ( 77% ) patients , and indocyanine green identified bilateral sentinel nodes in 40 ( 46% ) patients without bilateral sentinel nodes identified by isosulfan blue dye . 
in the indocyanine greenblue dye group , isosulfan blue dye identified bilateral sentinel nodes in 26 ( 29% ) of 89 patients , indocyanine green identified bilateral sentinel nodes in 71 patients ( 80% ) , and isosulfan blue dye identified bilateral sentinel nodes in two patients ( 2% ) without bilateral sentinel nodes identified by indocyanine green . as a post - hoc analysis , we assessed metastatic disease . 
macrometastatic disease was found in eight ( 38% ) of 21 sentinel nodes , micro metastatic disease in five ( 24% ) , and isolated tumour cells in eight ( 38% )  . there were no allergic reactions or adverse events attributable to either isosulfan blue dye or indocyanine green . 
most adverse events were related to surgery ( eg , postoperative pain or ileus )  . discussion although this study was designed as a non - inferiority trial , our findings suggest that indocyanine green was superior to isosulfan blue dye in identifying sentinel lymph nodes in women with cervical and uterine cancer because indocyanine green identified sentinel lymph nodes in a much larger proportion of patients than isosulfan blue dye did . 
indocyanine green was also significantly superior to isosulfan blue dye in detecting vol 19 october 2018 1399 articles together does not seem at least one sentinel node and in detecting bilateral sentinel nodes . 
the use of indocyanine green and isosulfan blue dye be necessary , because the addition of isosulfan blue dye to indocyanine green identified few sentinel nodes beyond those identified with indocyanine green alone . 
 finally , interstitial injection of indocyanine green seems to be safe , as we recorded no adverse events related to the compound . our findings that isosulfan blue dye detected at least one sentinel node in 131 ( 74% ) of 176 patients and indocyanine green detected at least one sentinel node in 168 ( 96% ) of 176 patients in the mitt population are similar to what has been previously reported in the literature.6 however , blue dye alone detected bilateral lymph nodes in only 54 ( 31% ) patients in the mitt population , which is lower than the 5560% reported in previous studies.13 , 14 all surgeons participating in our study had attained proficiency in the mapping procedure , so it is difficult to attribute the low rate of detection of bilateral nodes with isosulfan blue dye alone to poor technique or learning curve . 
multiple single - institution studies have found indocyanine green to be superior to blue dye and radiocolloid in detecting bilateral sentinel nodes after a cervical injection , 15 , 16 but a large , multi - institutional retrospective study did not show a difference between the two techniques.17 systematic reviews and meta - analyses also present conflicting results , with some showing combination blue dye and radiocolloid equivalent to indocyanine green in detecting bilateral sentinel nodes18 whereas others show that compared with use of blue dye alone , combined tracers might improve detection of at least one sentinel node but not detection of bilateral nodes.6 although the combination of blue dye and radiocolloid might be better than blue dye alone and equivalent to indocyanine green in detecting sentinel nodes , no studieseither prospective or retrospective have compared the combination of blue dye and radiocolloid with indocyanine green . 
however , the effect was much more pronounced with blue dye alone than with indocyanine green alone.8 because of the high rate of obesity in women with uterine cancer , many gynaecological oncologists have adopted the robotic system to assist in performing hysterectomy and staging , citing as their reason that the robotic system makes it easier to perform the lymphadenectomy portion of the surgery in women with a high bmi.19 , 20 the most commonly used robotic platform , the da vinci surgical system ( intuitive surgical , sunnyvale , ca , usa ) , includes an option for intraoperative near - infrared imaging called the firefly ( originally developed by novadaq technologies )  . 
 the fires trial , 21 a prospective cohort study , showed that indocyanine green and near - infrared imaging in the da vinci system had a sensitivity of 97% in detecting metastatic disease in sentinel nodes . 
the film protocol did not require completion of lymphadenectomy after sentinel node detection , so sensitivity and negative predictive values for the pinpoint system cannot be calculated in our study . 
moreover , the pinpoint technology and image display used in our study differed from that of the firefly , so the results of our study cannot be extrapolated to robotic surgery . 
in the fires study , at least one sentinel node was identified in 293 ( 86% ) of 340 patients , which is lower than the proportion of patients shown to have at least one sentinal node with indocyanine green and the pinpoint system in our study . 
additionally , the indocyanine green used in this study ( ic2000 ) might differ from the indocyanine green used in the fires trial ( no details given in the trial )  . 
 however , we believe lymphatic mapping and sentinel node detection with indocyanine green and near - infrared imaging is probably similar in the two systems , with potential applications of the technique in other cancers , including breast cancer and melanoma . breast cancer , like uterine cancer , has highly predictable lymphatic drainage . 
 consequently , preoperative lymphatic mapping with radiocolloid and dynamic imaging ( eg , lympho scintigraphy or single photon emission ctct [ spect / ct ] ) to establish site of incision is unnecessary for lymphatic mapping in breast cancer . 
for example , a direct comparison showed that indo cyanine green detected a sentinel node in 97100% of patients with breast cancer whereas blue dyes detected a sentinel node in 8889%.22 , 23 additionally , indocyanine green detects more sentinel nodes per patient than does blue dye . 
when compared with radiocolloid , indocyanine green does not appear to detect more sentinel nodes overall but might detect more metastatic sentinel nodes.24 for melanoma , interest in indocyanine green as an alternative to radiocolloid for lymphatic mapping and sentinel node biopsy has been somewhat more tempered . 
lymphatic drainage of melanoma can often be 1400 vol 19 october 2018 articles ambiguous , especially for lesions located on the trunk , head , or neck.25 preoperative lymphatic mapping with dynamic imaging ( lymphoscintigraphy or spect / ct ) is often necessary to identify draining nodal basins and to determine sites for surgical incision and exploration . 
 the penetrance of near - infrared cameras to detect sentinel nodes through the skin is only 23 mm , so the use of indocyanine green as a substitute for radiocolloid is largely ineffective , especially for lesions located in anatomical areas with ambiguous drainage.26 lymphatic mapping and sentinel node biopsy is an image - guided , precision surgical procedure that is increasingly being adopted for the surgical staging of apparent cervical - confined and uterine - confined malignancies . 
as use of indocyanine green for lymphatic mapping in cervical and uterine malignancies becomes more routine , we should also be aware of the potential pitfalls of this new exciting technology . 
this result is likely due to the bright green effect of the imaging with a laser - based near - infrared syste occasionally , dilated lymphatic channels can lead to a very bright signal that leads to the channels being mistaken for nodes and excised . 
mistaken excision of lymphatic trunks or adipose tissue instead of a node is potentially a major pitfall as sentinel node biopsy without complete lymphadenectomy becomes more common ; failure to excise a true node could leave the disease status of an entire hemipelvis unknown . 
if the surgeon has any doubt , it is reasonable to send the presumed nodal tissue for an confirm nodal content . intraoperative pathological consultation a second major potential pitfall of lymphatic mapping and sentinel node biopsy for cervical and uterine malignancies is the removal of multiple bright green nodes that appear to be true sentinel nodes but are in fact second - echelon and third - echelon nodes . 
this pitfall also relates to the bright signal from a laser - based , nearinfrared imaging platfor unlike isosulfan blue dye , which rarely can be seen beyond the first or true sentinel node to secondary - echelon nodes , indocyanine green often produces bright green signal in not only the true sentinel node but also secondary , tertiary , and more distant nodal basins . 
further , the enhanced pathology protocol evaluation should be limited to the true sentinel nodes , which in most studies average about three per patient with uterine malignancy . although the initial capital expenditures needed to incorporate the use of indocyanine green and near - infrared imaging for lymphatic mapping in patients with cervical and uterine cancers might be prohibitively high for some institutions , the near - infrared imaging system could also be used for other purposes , such as evaluating perfusion of bowel or oesophageal anastomoses or delineating anatomy during cholecystectomy.2729 moreover , the alternative to this approach is to continue to use the combination of blue dye and radiocolloid in these patients ( since we have shown that blue dye alone for lymphatic mapping is suboptimal )  . 
although blue dye is quite inexpensive , the use of radiocolloid is not , because its administration requires additional nuclear medicine technicians , nurses , and physicians , and the use of nuclear medicine facilities . 
finally , incorporation of sentinel lymph node biopsy with indocyanine green and near - infrared imaging might be the most cost - effective approach in treating women with gynaecological cancers when compared with complete lymphadenectomy in all patients or lymphatic mapping and sentinel node biopsy with radiocolloid or blue dye.30 this study is limited in its inability to determine the sensitivity , negative predictive value , and oncological outcomes for lymphatic mapping and sentinel node biopsy in women with cervical and uterine cancers . 
 the protocol was designed only to compare indocyanine green and isosulfan blue dye as mapping substances in these patients , and not as a trial to determine the validity the sentinel node concept . 
however , although the combination of blue dye and radiocolloid might have improved detection rates in the standard group , on the basis of the literature , 31 we believe the retrospective data indocyanine green would still be superior in detecting sentinel nodes in women with cervical and uterine cancers . 
surgeons who are new to lymphatic mapping and sentinel lymph node biopsy should perform the procedure followed by complete lymphadenectomy until they are confident that they have achieved proficiency in accurately detecting sentinel nodes . 
finally , as mentioned , the results can only be assumed valid for the specific compound ( ic2000 ) and near - infrared system ( pinpoint ) used in the study . 
however , we believe that studies using other formulations of indocyanine green and other nearinfrared imaging systems will probably yield similar results to our study . the us food and drug administration indications for indocyanine green include only intravenous injection to determine cardiac output , to evaluate perfusion of solid vol 19 october 2018 1401 articles organs , and to perform ophthalmic angiography . 
the manufacturer of ic2000 indocyanine green dye has submitted an application to the food and drug administration on the basis of the results from this study for on - label use of interstitial injection of indocyanine green combined with near - infrared imaging for lymphatic mapping . 
 for women with cervical and uterine cancers , increasing evidence suggests that lymphatic mapping and sentinel node biopsy not only improves detection of disease in regional nodes but also decreases operative morbidity.32 , 33 as lymphatic mapping and sentinel node biopsy become the standard of care in the surgical treatment of cervical and uterine cancers , improving sentinel node detection , particularly detection of bilateral sentinel nodes , will become the focus of research . 
as shown in this study , the incorporation of indocyanine green cervical injection and near - infrared imaging into the mapping improvement over procedure could represent an existing approaches ( ie , blue dye , radiocolloid , or both ) and might in the future become a standard method in these and other solid tumours . contributors mf and nra - r participated in study conception and design , acquisition of data , analysis and interpretation of data , drafting of the report , and critical revision . 
dlu participated in study conception and design , analysis and interpretation of data , and critical revision of the report . declaration of interests mf reports grants from novadaq / stryker , during the conduct of the study , and personal fees from novadaq / stryker , grants from navidea , personal fees from johnson and johnson , and personal fees from genentech , outside the submitted work . 
the other authors declare no competing interests . acknowledgments mf and dlu are supported by the national institutes of health / national cancer institute under award number p30ca016672 . correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections correction to lancet oncol 2017 ; 18 : e31529 correction to lancet oncol 2017 ; 18 : 150211 weller m , van den bent m , tonn jc , et al . 
 lancet oncol 2017 ; 18 : e31529in the panel of this review ( published online first on may 5 , 2017 ) , the dose of bevacizumab should be 10 mg / kg . 
the corrections have been made to the online version as of oct 31 , 2017 , and the printed version is correct . vol 18 november 2017 e642 corrections comment published online october 28 , 2015 s1470 - 2045 ( 15 ) 00364 - 2 see articles page 1605 hypofractionation for prostate cancer and pros radiotherapy study in the non - inferiority chhip trial , 3216 patients underwent for intensity - modulated compared cancer . 
the localised prostate conventional fractionation at a dose of 74 gy in 37 fractions , previously assessed in the rt01 trial , 1 with two moderately hypofractionated schedules : 60 gy in 20 fractions and 57 gy in 19 fractions , with fractions of 3 gy per day . 
the quality - of - life ( qol ) substudy by anna wilkins and colleagues2 describes the patient - reported outcomes ( pros ) of 2100 patients , which were assessed with several qol instruments . 
the incidence of bowel and urinary symptoms were low and similar in the control and hypofractionated groups up to 24 months of follow - up , with no di erences with respect to timeto - event analysis of small or worse overall bowel , urinary , and sexual bother . intensity - modulated radiotherapy is a high - precision external beam radiotherapy approach that is regarded as the gold standard for the treatment of localised prostate cancer.3 intensity modulation has o ered the opportunity to launch phase 3 randomised trials to investigate whether overall treatment times can be reduced by increasing the dose per fraction , without increasing acute and late toxic e ects , and while maintaining quality of life for patients . 
prostate cancer has a low cell renewal rate ; 4 its low / ratio , about 14 , 5 describes the association between the delivered dose and the clinical response . 
 an interim analysis of the chhip trial6 that included 457 patients reported no di erence between treatment groups in the proportion of patients with grade 2 or higher gastrointestinal or bladder toxic e ects . 
the trial had a comprehensive methodology and radiotherapy quality assurance with appropriate dose constraints , and is the rst to report quality of life with pros in such a large population . 
the inclusion of high - risk prostate cancer is controversial because pelvic lymph node irradiation is needed for such strict cases , which might be harmful if delivered by hypofractionation because of the radiosensitivity of the small bowel . 
the dose used in the control group ( 74 gy ) would usually be regarded as an intermediate dose : a high dose would typically fall in the range of 7880 gy . 
high - risk prostate cancer requires a longer duration of androgen deprivation therapy compared with lower risk forms : 23 years rather than 36 months.7 as mentioned by the authors , 2 radiotherapy - related toxic e ects , particularly faecal incontinence , rectal bleeding , and use of urinary pads , were likely to be underestimated because of the use of di erent qol instruments . 
 in both the chhip and rt01 trials , the intensitymodulated schedules show signi cantly fewer adverse gastrointestinal events compared with the 74 gy schedules.8 other phase 3 randomised trials have investigated moderate hypofractionation for localised prostate cancer , but these were done with di erent techniques and sometimes had no comprehensive health - related qol assessments : a systematic review9 of these studies supports the safety of moderate hypofractionation but also emphasises the scarcity of data about long - term e cacy . 
in oncology , treatment choices are based on e cacy , toxic e ects , patient quality of life , and nally treatment costs ( once the other parameters have been met )  . 
before moderate hypofractionation can be recommended in daily practice for low - risk and intermediate - risk prostate cancer , 10 mature data from the chhip trial are needed ( showing the non - inferiority of hypofractionated regimens and 5 - year urinary , bowel , and sexual adverse event data ) , as are results from trials such as the radiation therapy oncology group 0415 trial and the profit trial from the ontario clinical oncology group . 
 intensity - modulated fractionated in the near future , the use of hypofractionation including whether face other challenges , will 1570 vol 16 december 2015 comment published online november 16 , 2015 s1470 - 2045 ( 15 ) 00457 - x see articles page 1617 can be combined moderate hypofractionation with brachytherapy , and the advent of extreme hypofractionation ( 510 gy in four to seven fractions )  . 
 such approaches will have to be managed within the framework of clinical research , with careful estimation of each patients comorbidities and their gastrointestinal and genitourinary function , as assessed with the international prostate symptom recordings . 
hypofractionated radiotherapy versus conventionally fractionated radiotherapy for patients with intermediate - risk localised prostate cancer assessed with patient - reported outcomes : 2 - year follow up of the randomised , non - inferiority , phase 3 chhip trial . 
jama 1998 ; 280 : 96974 . continued role for asct in multiple myeloma in the lancet oncology , francesca gay and colleagues report ndings of an international , multicentre randomised study in patients with newly diagnosed multiple myeloma.1 lenalidomide and dexamethasone were administered as induction treatment , followed by randomisation to either cyclophosphamide , lenalido mide , and dexamethasone or high - dose melphalan and autologous stem - cell transplantation ( asct ) as consolidation , and either lenalidomide and prednisone lenalidomide alone or as maintenance . 
this work builds on a previous study in which induction was followed by randomisation to either oral melphalan , lenalidomide , and prednisone or tandem high - dose melphalan and asct.2 in that report , better progression - free survival and overall survival were reported for asct compared with chemotherapy . 
 lenalidomide gay and colleagues reported that median progressionfree survival was signi cantly longer for melphalan cyclophosphamide , and asct compared with lenalido mide , and dexamethasone ( 433 months [ 95% ci 332522 ] vs 286 months [ 206367 ] ; hazard ratio [ hr ] for the rst 24 months 251 , 95% ci 160394 ; p < 00001 )  . 
4 - year overall survival was signi cantly better for melphalan and asct compared with cyclophosphamide , lenalidomide , and dexamethasone ( 86% [ 95% ci 7992 ] vs 73% [ 6582 ] ; hr 240 , 95% ci 132438 ; p = 0004 )  . 
of note , only 53 ( 43% ) of 124 patients assigned cyclophosphamide , lenalidomide , and dexamethasone received salvage asct after progressive disease , showing that salvage asct after relapse is not always feasible . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections editorial see review page e234 cancer immunotherapy : enthusiasm and reality aligning at last in this issue of the lancet oncology , a review by eliza hawkes and colleagues provides a timely overview of pd - 1 inhibition in lymphoma . 
moreover , since the approval of ipilimumab for use in treatment of metastatic melanoma in 2011 , there has been increased interest , and success , in use of immunotherapies for the treatment of cancer . 
ironically , after several decades without any truly viable treatment options , melanoma has become a proving ground for immunotherapy , revolutionising the standard of care for these patients and paving the way for immunotherapies in other advanced cancers . 
but , we must take care not to allow our enthusiasm for these new treatments to outpace the data . ipilimumab , which targets the ctla - 4 antigen , was the rst immune - modulating antibody to show activity and be approved for cancer treatment rst in metastatic melanoma , and more recently in non - smallcell lung cancer . 
nivolumab and pembrolizumab , which inhibit the interaction between pd - 1 and its ligand , have also been approved for metastatic melanoma , and have activity in bladder cancer , non - small - cell lung cancer , and renal - cell cancer . 
these immunotherapies act by removing a block or checkpoint on t - cell activation , by contrast with earlier drugs like interleukin 2 , which simply stimulated the immune systeother immuneinvestigated , are modulating including antichemokine receptor antibodies , such as mogamulizumab ; therapeutic cancer vaccines , including dendritic cell - based vaccines ; and oncolytic viruses . therapies being in many immunotherapy trials , durable responses and extended long - term survival are seen only in a subset of patients , highlighting the importance of identi cation of distinguishing clinical and molecular characteristics . 
this will not only provide clues about what factors might predict response , but also presents an opportunity to develop immunological or other methods to promote response in refractory patients . 
 recently , the recist guidelines have been amended to include immune - related progression criteria ; however , the adoption of these guidelines is uneven , and the relationship between progression events based on these criteria and overall survival remains unclear . 
in view of the complexity in this area , validated endpoints are needed urgently so that the de nition of tumour response is a reliable surrogate of harder oncological outcomes , and that treatment successes are clear and genuine . another way to in a broad array of patients improve the e ectiveness of immunotherapies to investigate the e ect of combining modalities : what is the e ect of using immunotherapies with chemotherapy , targeted therapy , and even other immunotherapies ? there is some evidence , for example , that combining nivolumab and ipilimumab can result in greater responses in a proportion of patients with metastatic melanoma . 
caution recommended , though , for treatment combinations ; additive and synergistic responses might be expected from our understanding of biological mechanisms , but the complexity of the immune response could result in unexpected serious adverse events . 
the fact that autoimmunity might be linked to a greater proportion of patients achieving a response in some studies is all the more reason to determine optimal dose and scheduling for these drugs before approval and widespread use . immunotherapies hold great promise for patients far beyond what weve already seen , but we must remain aware of the risks associated with modi cation of the immune system , and avoid misinterpretation or overinterpretation of surrogate endpoints when reporting trial results . 
 the lancet oncology vol 16 may 2015 correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
 this correction has been made to the online version as of jan 31 , 2018 . vol 19 february 2018 corrections editorial for the who policy brief see bitstream / 10665 / 179517 / 1 / who_hiv_2015.17_eng. pdf ? ua = 1&ua = 1 for the report of the national transgender discrimination survey see thetaskforce.org / static_html / downloads / reports / reports / ntds_full.pdf for more on transgender health in the usa see world report lancet 2015 ; 386 : 72728 cancer risk in the transgender community for hiv control and care on july 8 , who released a new policy summarising recommendations transgender populations . 
indeed , there is scant information on cancer outcomes for transgender people because of an absence of large - scale prospective studies investigating cancer incidence and mortality in lesbian , gay , bisexual , and transgender people . 
 case reports and anecdotal evidence suggest that transgender people have a disproportionate cancer burden , but without high - level evidence , health - care providers are sti ed in their ability to provide adequate guidance . 
according to a 2011 report by the us national center for transgender equality and the national gay and lesbian task force , transgender people frequently face discrimination by health - care providers . 
this is further underlined by a world report published in the lancet on august 21 , which documents how a lack of provider knowledge about transgender health in the usa might result in intrusive questioning and harassment . 
this can be complicated by the transgender people opting out of cancer screening and examinations because of emotional or physical distress associated with the discordance between their gender and their natal genitalia . disengagement from gender - oriented health care , for any reason , results in missed opportunities for cancer screening and diagnosis , and likely contributes to care disparities in this population . 
the use of oestrogen , progestin , and testosterone , to induce or sustain sex transitions , are often used in excessive doses and continued without medical guidancethe e ect of this on cancer development is unclear . 
additionally , actions considered preventative for certain gynaecological cancers in non - trans women , such as taking the birth control pill , might not be considered by trans men . 
 finally , as reported for lesbians , gay men , and bisexual people , transgender people are also more likely to smoke and drink alcohol , and have a greater chance of contracting hiv and human papillomavirus than the overall population , all of which contribute to an increased cancer risk . cancer care for transgender people is a growing concern and health - care services that are both respectful of this populations di erences , and also relevant to and inclusive of them are needed . 
moreover , research into how cancer a ects the transgender community , as well as how to prevent , screen , and treat cancer in this population , will improve cancer control . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections corrections published online march 25 , 2015 s1470 - 2045 ( 14 ) 71115 - 5 correction to lancet oncol 2013 ; 14 : e374 correction to lancet oncol 2015 ; 16 : e163 correction to lancet oncol 2015 ; 16 : 447 , 448 weller m , p ster sm , wick w , hegi me , reifenberger g , stupp r . 
the rst sentence should read : exposure to passive smoke among never smokers does not seem to increase the chances of acquiring somatic mutations in genes linked to non - small - cell lung cancer in smokers , a new study shows . 
 vorinostat in patients with advanced malignant pleural mesothelioma who have progressed on previous chemotherapy ( vantage - 014 ) : a phase 3 , double - blind , randomised , placebocontrolled trial . 
lancet oncol 2015 ; 16 : 44756in the a liation section , p bass should be listed at netherlands in the funding cancer section in the summary and in the a liations , merck & co has been changed to merck & co , inc . 
 lancet oncol 2015 ; 16 : 54149in the key of gure 2 of this article , the boxes should indicate patients who were ct positive for disease , not those who were circulating tumour dna positive for disease . 
this correction has been made to the online version as of april 30 , 2015 , and the printed version is correct . vol 16 may 2015 e199 correction to lancet oncol 2018 ; 19 : 94052 correction to lancet oncol 2018 ; 19 : 123946 zhu ax , finn rs , edeline j , et al . 
lancet oncol 2018 ; 19 : 94052in this article , the affiliation of dr vittorina zagonel should have been istituto oncologico veneto - istituto di ricovero e cura a carattere scientifico ( iov - irccs )  . 
 apatinib combined with oral etoposide in patients with platinum - resistant or platinum - refractory ovarian cancer ( aeroc ) : a phase 2 , single - arm , prospective study . 
lancet oncol 2018 ; 19 : 123946in this article , the statistical analysis section should have stated that at least three responses were required to continue to the second stage . 
 we aimed to assess the safety and feasibility of targeted release and enhanced delivery of doxorubicin to solid tumours from thermosensitive liposomes triggered by mild hyperthermia , induced non - invasively by focused ultrasound . methods we did an open - label , single - centre , phase 1 trial in a single uk hospital . 
patients received a single intravenous infusion ( 50 mg / m ) of lyso - thermosensitive liposomal doxorubicin ( ltld ) , followed by extracorporeal focused ultrasound exposure of a single target liver tumour . 
the trial had two parts : in part i , patients had a real - time thermometry device implanted intratumourally , whereas patients in part ii proceeded without thermometry and we used a patient - specific model to predict optimal exposure parameters . 
the primary endpoint was at least a doubling of total intratumoural doxorubicin concentration in at least half of the patients treated , on an intention - to - treat basis . 
this study is registered with clinicaltrials.gov , number nct02181075 , and is now closed to recruitment . findings between march 13 , 2015 , and march 27 , 2017 , ten patients were enrolled in the study ( six patients in part i and four in part ii ) , and received a dose of ltld followed by focused ultrasound exposure . 
the treatment resulted in an average increase of 37 times in intratumoural biopsy doxorubicin concentrations , from an estimate of 234 g / g ( sd 093 ) immediately after drug infusion to 856 g / g ( 569 ) after focused ultrasound . 
no treatment - related deaths occurred . interpretation the combined treatment of ltld and non - invasive focused ultrasound hyperthermia in this study seemed to be clinically feasible , safe , and able to enhance intratumoural drug delivery , providing targeted chemoablative response in human liver tumours that were refractory to standard chemotherapy . funding oxford biomedical research centre , national institute for health research . copyright 2018 the author ( s )  . 
focused ultrasound is the only non - invasive approach capable of generating highly targeted mild hyperthermia at depth within the body and is thus an attractive method for triggered drug release . vol 19 august 2018 1027 research in context evidence before this study achievement of targeted and efficacious drug delivery while avoiding off - target toxicity represents a universal challenge in oncology , especially for the treatment of metastatic cancer . 
 nanotechnology vehicles that passively accumulate or selectively release anticancer agents in solid tumours have shown substantial promise in preclinical studies but have not yet gained widespread adoption because of the absence of demonstrable clinical benefit . 
lyso - thermosensitive liposomal doxorubicin ( ltld ) is a thermally active liposomal drug delivery system capable of selectively releasing its cargo ( doxorubicin ) under conditions of mild hyperthermia . 
however , preclinical studies showed that , by using focused ultrasound to induce mild hyperthermia non - invasively after systemic administration of ltld , the intratumoural delivery and distribution for a given systemic dose of doxorubicin can be greatly enhanced , potentially increasing therapeutic efficacy . 
 because of the small number and heterogeneous nature of preclinical studies and the absence of clinical studies , we did not do a formal meta - analysis of existing literature in ultrasound - mediated targeted drug delivery . added value of this study to our knowledge , this clinical study is the first to investigate the safety and feasibility of extracorporeally triggered drug release in oncology and to quantify the potential benefits of this approach in terms of the drug dose , distribution , and cellular delivery , in addition to radiologically assessing the observed therapeutic response induced by a single systemically administered course of chemotherapy . 
our study showed the safety and feasibility of selectively maintaining non - ablative hyperthermia in tumours with volume up to 100 cm3 in the liver , by use of a clinically approved extracorporeal focused ultrasound device . 
additionally , our study showed quantitative measures of the pharmacokinetics and intratumoural drug accumulation derived from the use of liposomal carriers in several tumour subtypes , both before and after ultrasound exposure , providing much needed clinical data about the value of passive versus active methods of accumulating therapeutic agents in tumours . implications of all the available evidence our study showed the potential to attain a chemo - ablative response in otherwise refractory tumours when using a thermosensitive liposomal drug carrier in combination with non - invasive focused ultrasound . 
building on decades of promising preclinical research , in both therapeutic ultrasound and drug delivery systems , our study highlights the clinical potential of device - based drug delivery approaches in general , and ultrasound in particular , to achieve several - fold enhancements in the delivery and distribution of existing and future therapeutic agents to solid tumours , with potentially transformative implications for their therapeutic effectiveness at a given systemic dose . lyso - thermosensitive unlike non - thermosensitive liposomal doxorubicin ( ntld ) , liposomal doxorubicin ( ltld ; celsion corporation , lawrenceville , nj , usa ) releases its drug payload at temperatures above 395c.6 formulations enhance plasma pharmaliposomal cokinetics of doxorubicin , resulting in a plasma half - life in humans of about 10 h for ntld9 and 1 h for ltld , 10 much longer than that of free doxorubicin , which has a half - life of only minutes.10 the thermosensitive property of ltld has been used clinically , mainly in conjunction with minimally invasive radiofrequency ablation , which is used to thermally ablate the core of the tumour while ltld is circulating systemically , with the intention of improving therapy at the tumour margins.11 ltld was evaluated as part of the heat trial , 12 a pivotal phase 3 study of the use of radiofrequency ablation for the treatment of hepato cellular carcinoma . 
 the primary endpoint of the heat trial was not met ; in the intention - to - treat analysis , the progression - free survival hazard ratio ( hr ) of radio frequency ablation plus ltld versus radiofrequency ablation alone was 096 ( 95% ci 079118 ; p = 071 ) and the overall survival hr was 095 ( 076120 ; p = 067 )  . 
however , in a subgroup of 285 patients with a solitary hepatocellular carcinoma lesion who received a radiofrequency ablation dwell time of at least 45 min , the overall survival hr was 063 ( 041096 ; p < 005 ) in favour of combination therapy . 
the positive findings in this subgroup of the heat study led to the ongoing optima study ( nct02112656 ) , which is a randomised , double - blind , dummy - controlled , phase 3 clinical study of ltld used in combination with standardised radiofrequency ablation for 45 min or longer for solitary hepatocellular carcinoma . 
these radiofrequency ablation studies have shown an acceptable safety profile , but targeted ltld release using extracorporeal focused ultrasound , to our knowledge , has never been assessed in humans . 
therefore , we did a phase 1 trial to assess the safety and feasibility of targeted release and enhanced delivery of doxorubicin from thermosensitive liposomes triggered by mild hyperthermia , induced non - invasively by focused ultrasound . methods study design and participants the tardox study was a phase 1 , single - centre , open - label study , done at churchill hospital ( oxford , uk )  . 
the health research authority national research ethics service , the oxford university hospitals research 1028 vol 19 august 2018 articles see online for appendix and development department , and the uks medicines and healthcare products regulatory agency granted ethics and regulatory approvals . 
the full study protocol is available in the appendix and a detailed account of the protocol design is available elsewhere.13 patients who were considered for this study were aged 18 years or older and had pathologically confirmed incurable solid primary or secondary ( metastatic ) liver tumours , of any histological subtype , who had progressed or were stable on conventional chemotherapy . 
for inclusion , patients were required to have at least one liver tumour ( 1 cm in size ) amenable to ultrasound - guided intervention , a life expectancy of 3 months or longer , a left ventricular ejection fraction of 50% or greater , a who performance status of 1 or lower , and adequate haema tological and biochemical indices . 
patients who had received radiotherapy to the target region in the preceding 12 months or a lifetime dose of doxorubicin greater than 450 mg / m were excluded , as were patients who were pregnant or had hiv - positive status , haemochromatosis , uncontrolled diabetes , ongoing infection , advanced liver disease , or serious illnessincluding congestive heart failure , myocardial infarction , or strokewithin the previous 6 months . 
detailed inclusion and exclusion criteria are provided in the full study protocol ( appendix p 28 ) and the protocol design.13 patients were recruited from the early phase trials clinic at the churchill hospital . 
all patients gave written consent for study participation . procedures participants were assigned to one of two parts of the study , delineated by the presence ( part i ) or absence ( part ii ) of a clinically approved thermometry device temporarily implanted percutaneously in the target tumour during the intervention ( appendix p 4 )  . 
intratumoural drug concentration was estimated by use of tumour biopsies taken before drug infusion ( pre - ltld ) , after infusion ( post - ltld ) , and after ultrasound exposure ( post - ltld plus focused ultrasound ) , through the same co - axial needle used to implant the thermometry device . 
 in addition to assessing safety , feasibility , and efficacy of ultrasound - triggered targeted drug delivery , part i was also designed to capture thermometry data to help predict ultrasound parameters for part ii of the study . part ii of the study was opened subsequently and was designed to assess the feasibility and efficacy of drug delivery without invasive thermometry , to better reflect how this treatment might be ultimately implemented non - invasively in routine clinical practice . 
focused ultrasound treatment parameters were defined by a predictive model to scale the ultrasound power and duty cycle as a function of the treatment depth , to yield a temperature in the range of 39543c on the intended treatment volume . 
clinical data from both parts of the study were used in endpoint analysis , which included quantification of the delivered intratumoural dose of doxorubicin from tumour biopsies . for all study participants , before full study consent , ultrasound planning sessions were done to assess the feasibility of targeting liver lesions with ultrasound , resulting in the selection of a single target tumour for each patient for intervention . 
the treatment was received under a general anaesthetic ( with the use of high - frequency jet ventilation to reduce respiratory motion of the liver ) and involved a single 30 - min intravenous infusion of ltld ( 50 mg / m ) followed by targeted hyperthermia of the selected liver tumour by focused ultrasound . 
in the focused ultrasound treatment , a ce - marked extracorporeal high - intensity focused ultrasound device , certified for oncological treatment ( model jc200 focused ultrasound tumor therapeutic system , chongqing haifu , chongqing , china ) , operating at a frequency of 096 mhz , was used to induce highly targeted mild hyperthermia ( 395c ) within the selected liver tumours . 
for all part i and part ii interventions , the integrated diagnostic b - mode ultrasound probe of the device was used for image guidance through intercostal or subcostal windows . 
extensive preclinical validation of the clinical device for its application in volumetric hyper thermia , using the same thermometry devices that were used in this study , was done before patient inter vention ( lyon pc , unpublished )  . 
the intervention is further detailed in the appendix and protocol design.13 clinical reviews and routine blood tests were done at 2 weeks and 4 weeks post - intervention , coinciding with repeat radiological imaging ( ct and mri scans of the liver and f - fluorodeoxyglucose pet - ct scan )  . 
patients could be removed from the study according to their wishes or clinician decision , if toxic effects or adverse events were deemed unacceptable , if there were substantial protocol deviations or non - compliance , or if there were new exclusion criteria , such as pregnancy . detailed sample analysis methods are outlined in the appendix ( pp 5 , 6 )  . 
in both parts of the study , peripheral vol 19 august 2018 1029 articles blood samples were obtained pre - ltld , post - ltld , and post - ltld plus focused ultra sound for pharmacokinetic analysis , corresponding with part i biopsy timepoints . 
 plasma aliquots and weighed biopsy samples were stored at 80c until sub sequent analysis by high - performance ( hplc ) , with fluorescence liquid chrom atography detection at 480 nm excitation and 560 nm emission , to assess the total doxorubicin concentration within each biopsy and plasma sample , whether liposomal or free . 
plasma aliquots obtained at the same timepoints were also analysed on the same day by a dequenching assay , in an attempt to estimate the degree of encapsulation of doxorubicin in plasma using direct fluorometry ( appendix p 12 )  . 
therefore , for part ii of the study , the mean drug concentration of the part i post - ltld treatment biopsies was used as a comparator to evaluate the number of patients with at least a two - times increase in intra tumoural biopsy drug concentration . the focused ultrasound - targeted tumours were analysed for response by pcl or other members of the radiology team with choi criteria , response evaluation criteria in solid tumors ( recist ) , and pet response criteria in solid tumors ( percist ) , each modified for a single target , by ct , mri , and pet - ct imaging.14 , 15 , 16 additionally , target tumours were also analysed for total lesion glycolysis by pet - ct scan17 ( appendix p 6 )  . 
non - target liver tumours that had received a drug dose but no focused ultrasound exposure were also assessed in isolation in the same manner , with the same scan sequences , to provide timematched radio logical controls . outcomes the primary objective of this study was to assess the feasibility of targeted release of doxorubicin from ltld by use of mild hyperthermia generated non - invasively by focused ultrasound . 
the primary endpoint was defined as at least a doubling of the intratumoural biopsy doxorubicin concentrations , or final concentrations greater than 10 g / g , after focused ultrasound - mediated hyperthermia , in at least half of patients treated . secondary objectives were related to assessment of the safety and optimisation of the ultrasound exposure parameters for targeted liver hyperthermia and drug release . 
therefore , secondary endpoints were defined as the achievement of mild hyperthermia as monitored by the implanted thermometry device for patients in part i ; persistence of cell viability staining after focused ultrasound exposure , to indicate absence of instantaneous thermal ablation ; and adverse events occurring in the 30 days after the intervention relating to either ltld or focused ultrasound procedure , significant bone marrow suppression and liver toxicity . including clinically prespecified exploratory ( tertiary ) objectives investigated alternative methods of quantifying doxorubicin release ( as opposed to estimating intratumoural concentrations ) and the therapeutic effect of the intervention on the target tumours . 
therefore , tertiary endpoints included positive fluorescence in tumour biopsies ( which would be indicative of bioavailable doxorubicin ) , and radiological evidence of response in target tumour volumes up to 30 days after the intervention , according to recist and choi response evaluation criteria based on mri and ct scans , and suvmax using pet - ct , with each criteria modified for a single target . statistical analysis this study tested the hypothesis that higher intratumoural drug concentrations could be achieved when combining ltld with focused ultrasound - induced hyperthermia for targeted tumour delivery , compared with passive accumulation alone . 
this study did not require statistical analysis ; a doubling of total intratumoural doxorubicin concentrations ( post - ltld vs postltld plus focused ultrasound ) in at least half of the evaluable participants was required to meet the primary endpoint . 
after treatment of the first four patients in part i of the study , the trial management group did an interim analysis of the secondary endpoint relating to optimal focused ultrasound exposure parameters , in addition to the remaining secondary endpoints pertaining to safety . 
 because hyperthermia higher than the drug release threshold had been reliably attained in each target liver tumour , and no safety concerns were raised , part ii of the trial was opened in parallel to part i . 
from this point on , allocation to either part was determined on the basis of feasibility ( anatomical location of the potential target tumours ) and study team and patient preference , as detailed in the full study protocol . 
all other analyses were done at the end of the study . this study is registered withclinicaltrials.gov , number nct02181075 , and eudra - ct , number 201400051461 . role of the funding source the funders and sponsor of the study had no role in study design , data collection , data analysis , data inter pretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results of 46 patients who were screened and assessed for eligibility , ten patients satisfied the inclusion criteria and were enrolled between march 13 , 2015 , and march 27 , 2017 . 
of the excluded patients , the majority ( 19 [ 53% ] of 36 ) were excluded on the basis of anatomical location of the tumour , before part ii was open to recruitment , which offered much more flexibility in tumour location . 
there were no treatmentrelated deaths during the study . part i interventions were of long duration ( mean anaesthetic time 3692 min [ sd 384 ] ) because of time localising the target tumour spent simultaneously with diagnostic ultrasound by two different intercostal approaches and optimising the focused ultrasound parameters with thermometry feedback before drug infusion.13 the procedurally simpler part ii interventions , which did not require the insertion of an intratumoural thermometry device and real - time optimisation of focused ultrasound parameters , were expectedly of shorter duration ( mean anaesthetic time 2138 min [ sd 210 ] ) ( appendix p 3 )  . 
for focused ultrasound , we used ultrasound powers in the range of 50140 watts ( corresponding to estimated in - situ peak rarefactional pressures in the range of 5082 mpa ) and duty cycles between 30% and 100% , depending on tumour location ( appendix p 2 )  . in part i of the study ( n = 6 patients ) , the mean intratumoural biopsy doxorubicin concentration postltld plus focused ultrasound was 774 g / g ( sd 409 ) , representing an increase of 33 times compared with the mean post - ltld concentration of 234 g / g ( 093 ; table 2 , appendix pp 7 , 8 )  . 
in all cases , doxorubicin was not detected in tumour samples taken before drug infusion , while higher doxorubicin concentrations were detected in samples taken post - ltld plus focused ultrasound , compared with those of post - ltld samples ( table 2 )  . overall , the mean doxorubicin concentrations in postltld plus focused ultrasound intratumoural biopsy samples from all ten study participants was 856 g / g ( sd 569 ) an increase of 37 times compared with the 46 patients assessed for eligibility 36 patients excluded 19 unsuitable tumour location 10 progressive disease 3 recent radiotherapy to liver 3 declined to participate 1 tumour size too small 10 patients allocated and received intervention 1 patient lost to follow - up 1 patient too fatigued to attend nal follow - up visit ( week 4 ) 10 patients included in intention - to - treat analysis figure 1 : trial profile mean intratumoural biopsy concentrations in part i post - ltld samples ( table 2 , figure 2 )  . 
of the part ii patients , patient ii.03 was the only patient under the two - times increase limit required to satisfy the primary endpoint ( figure 2 )  . 
given that seven ( 70% ) of ten patients showed at least a doubling increase in intratumoural biopsy doxorubicin concentrations after focused ultrasound exposure , with concentrations from biopsies obtained in part ii compared with the mean concentration post - ltld alone from biopsies obtained in part i , our study met its primary endpoint ( table 2 )  . 
 * responses ( ratio of doxorubicin to internal standard ) were significantly lower than the response seen for the plasma lower limit of quantification ( lloq ; 01 g / ml for i.02 and 005 g / ml for i.06 ) ; the values shown are upper - bound estimates ; assuming that the response for these samples would be the same as that for the lloq , the amounts are calculated for the mass of each specific biopsy analysed . 
estimate only , because the internal standard was inadvertently omitted from this sample during processing . table 2 : high - performance liquid chromatography ( hplc ) biopsy results after analysis of chromatograms methods of analysis . 
plasma concentrations calculated with this method were similar for both methods of quantification ; however , the calculated biopsy concentrations were lower when the internal standard was excluded in calculations compared with when it was included . 
therefore , the estimated post - ltld plus focused ultrasound value for intra tumoural doxorubicin in patient i.02 is likely to represent an under estimate of the true concentration . six patients from part i , with prescribed tumour volume range of 105734 cm ( mean 496 cm [ sd 263 ] ) , and four from part ii , with prescribed tumour volume range of 307539 cm ( 438 cm [ 103 ] ) , were exposed to focused ultrasound ( overall mean tumour volume 473 cm [ 207 ] ; appendix p 2 )  . 
sustained and controlled hyperthermia ( > 395c ) was achieved in five ( 83% ) of six part i patients for a mean of 408 min ( sd 157 )  . 
in these six patients , mean intratumoural temperatures of 389415c ( overall mean 401c , sd 09 ) were recorded between 33 min and 79 min ( mean 653 min , 167 ; table 3 , figure 3 , appendix pp 911 )  . 
 in the one patient ( i.03 ) , in whom hyperthermia of 395c or higher was achieved momentarily but not sustained ( appendix p 10 ) , gas introduced around the tip of the co - axial needle on intro duction of the thermometry device ( as visualised on the ultrasound - guidance b - mode imaging system ) might have resulted in underrepresentation of the temperature in the target tumour volume . 
 cumulative equivalent minutes at 43c thermal dose analysis ( table 3 ) is discussed in the appendix p 11 . instantaneous changes consistent with tumour ablation , as is typically seen in high - intensity focused ultrasound thermal ablation , 19 were absent on the diagnostic ultra sound guidance system ( b - mode imaging ) for all inter ventions . 
this absence of thermal ablation was further supported by the day 1 mri findings , cell viability studies , and the predictive model ( gray md , unpublished data )  . 
 serious adverse events were otherwise restricted to selfresolving grade 4 neutropenia in five ( 50% ) of ten patients , an expected adverse event of ltld ( table 4 ) .11 worsening of pre - existing liver function derangements ( grade 3 or lower ) was seen in all patients , except patient i.01 , within the 30 - day follow - up period ( appendix p 3 ) , in keeping with the known adverse event profile of ltld.21 however , it was not possible to distinguish a drug - related cause of liver dysfunction from progressive liver malignancy with certainty in this patient cohort . non - invasive ultrasound - mediated hyperthermia was found to be safe , causing no skin burns , off - target tissue damage , or other clinically significant adverse events , either with or without real - time thermometry ( table 4 )  . at the 2 - week and 4 - week follow - up visits , ct , mri , and pet - ct scans were done . 
 for the remaining nine patients , targeted tumour volumes ( exposed to both ltld and focused ultrasound ) were assessed with recist , choi , and percist criteria modified for a single target tumour and compared with control liver tumours ( exposed to ltld alone )  . 
all other target tumours ( four [ 40% ] of ten ) and control tumours ( 13 [ 81% ] of 16 ) assessed showed either stable or progressive disease according to recist , choi , or percist criteria at 2 weeks or 4 weeks ( appendix pp 2025 )  . 
the four patients with a partial response according to choi criteria showed 364% , 226% , 182% , and 463% reductions in total lesion glycolysis , despite only having partial tumour coverage with focused ultrasound ( appendix p 26 )  . after counterstaining of cell nuclei with 4 ' , 6 - diamidino2 - phenylindole ( dapi ) , tumour biopsies were examined microscopically for evidence of intratumoural ltld release within 2 months of sampling ( appendix p 6 )  . 
tumour samples from patient i.01 were too auto - fluorescent for the doxorubicin signal to be distinguished from background noise in the paraffin - embedded samples , while the postltld plus focused ultrasound tissue sample from patient i.02 was contaminated with blood . 
the presence of nuclear doxorubicin showed bioavailability of intratumoural doxorubicin and thus liposomal release , because doxorubicin must be in its free form to diffuse into the tumour cells.22 in the post - ltld controls , minimal nuclear or extravascular doxorubicin was seen . plasma samples from each patient were assayed for total doxorubicin concentration by hplc . 
polynomial fit was done with least squares fit of fourth order in matlab . table 3 : summary of statistics for the post - drug thermometry analysis for all part i patients , for both raw and polynomial fitted data jc200 treatment parameters : scanning mode = linear mode at 6 mm / s ; power = 115125 w ; duty cycle = 7077% 115 w , 70% duty cycle prescribed volume 909 cm3 125 w , 77% duty cycle prescribed volume 638 cm3 ltld release threshold [ 395c ] 1.05 real - time thermometry ( post - ltld ) polynomial t ( order = 4 ) time ( min ) figure 3 : illustrative controlled hyperthermia by focused ultrasound real - time thermometry data ( trace ) captured after infusion of lyso - thermosensitive liposomal doxorubicin ( ltld ) and during focused ultrasound exposure in moving beam ( linear ) mode for patient i.05. 
from approximately 30 s to 33 min , a 909 cm prescribed target tumour volume was exposed to focused ultrasound at 115 w ( 87 mpa peak rarefactional in situ pressure ) at 70% duty cycle in linear mode . 
although the release threshold was reached within 5 min of focused ultrasound exposure , heating in the first 30 min was deemed slightly suboptimal because of prolonged cooling periods between treatment cycles . 
subsequently , by removing the outermost slices from the prescribed treatment volume , resulting in a smaller 683 cm tumour volume , and increasing power to 125 w ( 90 mpa derated ) and duty cycle to 77% , optimal hyperthermia was achieved for 3580 monce focused ultrasound stopped , the tumour was allowed to cool before the thermocouple was removed from the patient at 85 min , and a tumour biopsy sample was subsequently taken . 
the dotted curve is a fourth order polynomial fit , which is probably more representative of the bulk temperature in the prescribed tumour volume than the rapidly fluctuating point temperature recorded by the sensitive region of the intratumoural thermometry device ( trace )  . the standard curve ; therefore , subsequent plasma samples of the remaining nine patients were diluted before analysis . 
for these patients , mean total plasma doxorubicin concentrations decreased from 263 g / ml ( sd 40 ) post - ltld to 129 g / ml ( 60 ) post - ltld plus focused ultrasound . 
results of the quenched and dequenched fluorometric plasma analysis are available in the appendix ( pp 12 , 13 )  . discussion to our knowledge , our study was the first to attempt noninvasive ultrasound - mediated targeted hyperthermia for vol 19 august 2018 1035 articles grade 1 - 2 grade 3 grade 4 definitely or probably related to ltld : haematological toxic effects neutropenia or neutrophils decreased anaemia urinary tract infection 1 ( 10% ) 1 ( 10% ) 5 ( 50% ) * 1 ( 10% ) definitely or probably related to ltld : non - haematological toxic effects definitely or probably related to the procedure alopecia candida infection fatigue or lethargy nausea vomiting abdominal pain back pain decreased appetite dysphonia erythema fatigue hepatic pain musculoskeletal chest pain musculoskeletal pain or discomfort nausea pain in extremity skin discolouration abdominal pain confusion state constipation decreased appetite fatigue joint swelling malaise nausea peripheral swelling respiratory tract infection vomiting 8 ( 80% ) 1 ( 10% ) 4 ( 40% ) 2 ( 20% ) 2 ( 20% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) 2 ( 20% ) 6 ( 60% ) 1 ( 10% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) * 1 ( 10% ) 2 ( 20% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 2 ( 20% ) 1 ( 10% ) 1 ( 10% ) 1 ( 10% ) definitely or probably unrelated or possibly related to ltld or procedure ( indeterminate cause ) no grade 5 adverse events occurred . 
 mean temperatures needed for drug release were safely maintained in clinically relevant tumour volumes by extracorporeal focused ultrasound , for about 1 h , without subsequent radiological or histological evidence of thermal ablation . 
this approach resulted in a substantial increase in the total intratumoural biopsy concentration of doxorubicin , compared with that achieved by passive accumulation alone , with seven of ten patients having at least a doubling and an increase of up to ten times in intratumoural doxorubicin concentrations . 
this increase occurred concurrently with the presence of nuclear doxorubicin , showing liposomal release after focused ultrasound exposure , and localised radiological responses in the target tumour regions exposed to focused ultrasound in several patients . 
overall , these findings suggest that target drug delivery to solid tumours triggered noninvasively by therapeutic ultrasound is clinically safe , feasible , and potentially effective . the non - thermosensitive liposomal formulation of doxorubicin , ntld , is hypothesised to exert its therapeutic effect predominantly by the enhanced permeability and retention effect.23 by contrast , the ltld formulation that we used in this trial is understood to act by rapid diffusion of doxorubicin into the tumour interstitium under conditions of mild hyperthermia , with only a small pro portion of doxorubicin entering the tumour by enhanced permeability and retention . 
these intended delivery mechanisms are reflected in the circulation profiles of the two formulations , with ntld having a half - life of more than 10 h while ltld has a shorter halflife of about 1 h.9 , 10 , 24 , 25 mild hyperthermia has been shown to enhance the perfusion and increase the permeability of tumour vasculature.26 because focused ultrasound exposure begins while blood concentrations of ltld are at their peak11 , 13 ( figure 2 ) and at a timepoint before any substantial enhanced permeability and retention - assisted accumulation could have occurred , it is our understanding that the majority of the intratumoural doxorubicin is released from circulating ltld in the tumour microvasculature , when the tumour reaches the liposomal transition temperature ( 395c )  . 
free ( bio - available ) circulating doxorubicin might then rapidly diffuse into the adjacent or downstream perivascular space , and on to tumour cells at therapeutic concentrations and penetration depths due to a steep concentration gradient , surpassing what could be achieved through passive circulation alone . the post - ltld intratumoural biopsy concentrations of doxorubicin ( after infusion ) were similar to those seen in preclinical tumour models of ltld.5 differences in the measured total doxorubicin concentrations before focused ultrasound exposure were very small across patients . 
in keeping with preclinical studies , 5 , 7 this result strongly suggests that there is little opportunity for passive accumulation of ltld in the first 2 h after administration , but there could still be differences in the leakiness of tumour vascular pores across the different tumour subtypes treated.27 the much greater differences in total doxorubicin concentration observed after focused ultrasound exposure are probably due to a combination of factors , including the differences in tumour leakiness across subtypes , tumour heterogeneity , the percentage of 1036 vol 19 august 2018 articles the ultrasonically treated volume that was adequately vascularised , and the total duration of focused ultrasoundmediated hyperthermia relative to the patient - specific pharmacokinetics of ltld . 
despite the use of a different analytical technique , pharmacokinetic profiles for total doxorubicin were similar to previously published clinical data , 11 in which the same dose of ltld was combined with radiofrequency ablation of liver tumours . magnetic resonance spectroscopy , particularly chemical exchange saturation transfer , was explored as a method of quantifying free doxorubicin preclinically , using phantom and small animal studies ( unpublished )  . 
 in this early study , it remains unclear whether ultrasoundmediated cavitation is involved in the mechanism of delivery , but preclinical data strongly suggest that the microstreaming and shockwaves created by cavitation can be a benefit to the delivery of cancer drugs.29 , 30 although our phase 1 study was , to the best of our knowledge , the first to translate focused ultrasoundtriggered targeted drug delivery to a clinical oncology setting , the study design had inherent limitations . 
first , the prescribed tumour treatment volumes were constrained by the presence of ribs in the acoustic field treatment ( which restricted monitoring and guidance and reduced the focused ultrasound beam intensity ) and by the focused ultrasound system itself ( with restricted scanning capabilities and a nominally small , fixed ultrasonic focus ) , such that , the real - time b - mode typically , only partial sonication of larger tumours could be achieved , usually including tumour borders closest to the ultrasound source . 
custom focused ultrasound devices designed for volumetric hyperthermiafor example , devices using less tightly focused transducers or multi - element systems with beam steering8might allow rapid induction of large volume hyperthermia , facilitating the treatment of larger tumour volumes with this strategy . second , tumours are highly heterogeneous and show great microregional variations , not least in the amount of vascularity and necrosis.31 in this study design , tumour biopsies were intended to provide an estimate of the mean intratumoural drug concentration in the focused ultrasound - exposed tumour volume . 
this design limitation is mitigated , to some extent , by subsequent radiological analysis of the targeted tumours , most crucially by pet - ct scan , a technique that can discriminate metabolically active from necrotic or chemoablated tumours . third , the study design did not include time - matched control biopsies from liver tumours receiving ltld alone , because doing more than three sequential tissue biopsies in more than one location in any one patient was neither ethical nor practical.13 preclinical studies of ltld showed that , in great part because of its short half - life ( 1 h compared with more than 10 h for ntld ) , the additional intratumoural accumulation beyond 30 min after administration is not substantial , and falls well short of the doubling increase in intratumoural concentration that constituted the primary endpoint of our study.6 , 8 radiological follow - up enabled indirect assessment of negligible longer - term passive accumulation of ltld . fourth , although the hplc tumour results were generated by a validated method , worst - case estimations were done in three cases . 
however , since these estimates were worst - case estimates , we are confident that the primary endpoint is not compromised . a fifth limitation was that the introduction of any instrumentation into the target tumour risked contamination of tumour samples with blood products . 
the postltld sample for patient i.04 and the post - ltld plus focused ultrasound sample for patient i.02 were both shown to contain blood contamination on haemotoxylin and eosin staining . 
nevertheless , should be exclusion of these two results from the overall analysis does not alter the outcome of the study , because seven of eight patients still had an increase greater than doubling in drug concentrations and the study still met its primary endpoint . vol 19 august 2018 1037 articles thermography and coregistration with lastly , a magnetic resonance spectroscopy - guided focused ultrasound system would have provided valuable spatial the follow - up mri , facilitating both treatment and response assessment . 
however , the ultrasound - guided focused ultrasound device used made practical issues surrounding the use of high - frequency jet ventilation anaesthesia and the biopsy procedure less challenging because of the absence of a magnetic field . by design , part ii of the study proceeded without invasive thermometry , and this was shown to not adversely affect the efficacy of the intervention ; indeed , the mean post - ltld plus focused ultrasound intratumoural concen tration of doxorubin in part ii was 980 ug / g , compared with 774 ug / g in part i . whether delivering small molecules , antibodies , or viruses , maximising the dose delivered to a tumour while minimising off - target toxicity represents a universal challenge in oncology.32 a major limitation of systemically administered liposomal agents is their low therapeutic index : the dose required to produce a successful antitumour effect is toxic to normal tissues . 
device - targeted drug delivery has undergone decades of preclinical development but could be nearing clinical adoption as a generic tool for overcoming the challenges of delivering existing and emerging therapeutics to solid tumours . 
 mri - based or ultrasound - based treatment monitoring strategiesor detailed predictive treatment planning , as was used in this studyare likely to facilitate clinical adoption for non - invasive targeting . 
preclinical mri studies33 , 34 have combined three - dimensional thermography with sophisticated closed - loop feedback algorithms at high temporal resolutions to reduce microregional temperature fluctuations , and a clinical study involving the use of magnetic resonance - guided high intensity focused ultrasound with ltld is underway for treatment of paediatric solid tumours ( nct02536183 )  . 
by using an ultrasound - guided focused ultrasound device without thermography , our study explored the economically attractive and more easily scalable alternative than mrguided techniques for attaining large - volume bulk hyperthermia with predictive models , with less emphasis on maintaining tight and homogeneous temperature control . overall , this prospective study shows for the first time in a clinical setting the safety , feasibility , and potential for therapeutic benefit of ultrasound - triggered release of ltld in otherwise chemorefractory tumours . 
the small sample size of ten patients reflects that this trial was a proof - of - concept study , for which participation was predominately altruistic , involving only a single cycle of chemotherapy and targeting of a single tumour . 
a demonstrable radiological response in the targeted tumour volume alone is encouraging , given that doxorubicin has been previously shown to have reduced therapeutic value in many of these tumour subtypes.21 , 35 despite its limitations , our study shows for the first time in a clinical setting that it is feasible to safely trigger and enhance intratumoural delivery of a chemotherapeutic agent to a precise anatomical location at depth , by using focused ultrasound applied noninvasively . 
further preclinical and clinical research in focused ultrasound - mediated drug delivery might be warranted , with the intention of reducing toxicity and improving therapeutic outcomes in a broad range of solid tumours , potentially across multiple drug classes . contributors ccc , pcl , rc , mrm , and fvg designed the study and wrote the protocol . 
pcl and ccc wrote the manuscript , and all authors reviewed , commented on , and approved the paper . declaration of interests no author has direct or indirect financial interest in either the clinical device used for the study ( jc200 , chongqing haifu , chongqing , china ) or the drug ( thermodox , celsion corporation , lawrenceville , nj , usa ) used in the study . 
fw does not receive royalties for the manufacture , sale , upkeep , or maintenance of the device used for treatment despite being involved in the original team that filed patents related to the device . 
ccc and rc are founders , shareholders , and consultants for a spinout company from the university of oxford ( oxford , uk ) , oxsonics , specialising in ultrasound - enhanced drug delivery to tumours . 
mrm reports personal fees from amgen , valo therapeutics , and bioline ; grants and personal fees from roche and gsk ; grants from astrazeneca ; personal fees and trial - related payments to institutions from novartis , eisai , rigontec , array biopharma , and bms ; trial - related payments to institutions from astellas , millennium , vertex , regeneron , tcbiopharma , replimune , and pfizer ; non - financial support and trial - related payments to institutions from immunocore ; and personal fees , non - financial support , and trial - related payments to institutions from merck , outside the submitted work . 
all other authors declare no competing interests . acknowledgments the trial was funded by the uks national institute for health research , oxford biomedical research centre , and the research was supported by the oxford centre for drug delivery devices under a programme grant ( ep / l024012 / 1 ) from the engineering and physical sciences research council . 
the views expressed are those of the authors and not necessarily those of the nhs , the nihr , or the department of health . correction to lancet oncol 2018 ; 19 : 58081 grob jj . 
is there any interest in a new brafmek inhibitor combination in melanoma ? lancet oncol 2018 ; 19 : 58081in the title of this comment , braf - mek inhibitor was spelt incorrectly , and in the fourth paragraph one instance of the drug encorafenib was spelt incorrectly and the dose of encorafenib should have been 300 mg . 
 lancet oncol 2018 ; 19 : 70514in the summary , the following statement should have read as follows : cohort 3 was assigned to receive a dose of 100 mg / m twice daily ( maximum 100 mg per dose ) , regardless of age , equating to a maximum of 173% of the recommended adult phase 2 dose . 
we assessed the e cacy and safety of two pembrolizumab doses versus investigator - choice chemotherapy in patients with ipilimumab - refractory melanoma . methods we carried out a randomised phase 2 trial of patients aged 18 years or older from 73 hospitals , clinics , and academic medical centres in 12 countries who had con rmed progressive disease within 24 weeks after two or more ipilimumab doses and , if brafv600 mutant - positive , previous treatment with a braf or mek inhibitor or both . 
patients had to have resolution of all ipilimumab - related adverse events to grade 01 and prednisone 10 mg / day or less for at least 2 weeks , an eastern cooperative oncology group ( ecog ) performance status of 0 or 1 , and at least one measurable lesion to be eligible . 
using a centralised interactive voice response system , we randomly assigned ( 1 : 1 : 1 ) patients in a block size of six to receive intravenous pembrolizumab 2 mg / kg or 10 mg / kg every 3 weeks or investigator - choice chemotherapy ( paclitaxel plus carboplatin , paclitaxel , carboplatin , dacarbazine , or oral temozolomide )  . 
the study is closed to enrolment but continues to follow up and treat patients . findings between nov 30 , 2012 , and nov 13 , 2013 , we enrolled 540 patients : 180 patients were randomly assigned to receive pembrolizumab 2 mg / kg , 181 to receive pembrolizumab 10 mg / kg , and 179 to receive chemotherapy . 
based on 410 progression - free survival events , progression - free survival was improved in patients assigned to pembrolizumab 2 mg / kg ( hr 057 , 95% ci 045073 ; p < 00001 ) and those assigned to pembrolizumab 10 mg / kg ( 050 , 039064 ; p < 00001 ) compared with those assigned to chemotherapy . 
6 - month progression - free survival was 34% ( 95% ci 2741 ) in the pembrolizumab 2 mg / kg group , 38% ( 3145 ) in the 10 mg / kg group , and 16% ( 1022 ) in the chemotherapy group . 
treatment - related grade 34 adverse events occurred in 20 ( 11% ) patients in the pembrolizumab 2 mg / kg group , 25 ( 14% ) in the pembrolizumab 10 mg / kg group , and 45 ( 26% ) in the chemotherapy group . 
the most common treatment - related grade 34 adverse event in the pembrolizumab groups was fatigue ( two [ 1% ] of 178 patients in the 2 mg / kg group and one [ < 1% ] of 179 patients in the 10 mg / kg group , compared with eight [ 5% ] of 171 in the chemotherapy group )  . 
other treatment - related grade 34 adverse events include generalised oedema and myalgia ( each in two [ 1% ] patients ) in those given pembrolizumab 2 mg / kg ; hypopituitarism , colitis , diarrhoea , decreased appetite , hyponatremia , and pneumonitis ( each in two [ 1% ] ) in those given pembrolizumab 10 mg / kg ; and anaemia ( nine [ 5% ] ) , fatigue ( eight [ 5% ] ) , neutropenia ( six [ 4% ] ) , and leucopenia ( six [ 4% ] ) in those assigned to chemotherapy . 
although some studies have shown e cacy for other anti - pd - 1 and pd - l1 inhibitors after ipilimumab , these were not controlled and the sample sizes were small . added value of this study our study is , to the best of our knowledge , the largest reported randomised , controlled trial of an anti - pd - 1 or anti - pd - l1 drug for ipilimumab - refractory melanoma . 
results of this study con rm the e cacy and safety of pembrolizumab and the absence of a signi cant di erence in outcomes between pembrolizumab doses of 2 mg / kg and 10 mg / kg given once every 3 weeks , as observed in an earlier phase 1b study of patients with ipilimumab - refractory melanoma . 
more important , the study shows the superiority of pembrolizumab over cytotoxic chemotherapy , the current standard - of - care therapy , to improve progression - free survival in ipilimumab - refractory melanoma . 
our data are arguably of greater clinical relevance than are the data reported for nivolumab in this population because our study included patients with brafv600 - mutant melanoma and we report progression - free survival and patient - reported outcomes data . implications of all the available evidence overall , these ndings establish pembrolizumab as a new standard of care for melanoma and support the accelerated approval granted by the us food and drug administration for the use of pembrolizumab 2 mg / kg once every 3 weeks by patients with unresectable or metastatic melanoma whose disease progressed after ipilimumab and , if brafv600 mutant - positive , a braf inhibitor . 
we excluded patients with known active brain metastases or carcinomatous meningitis , active autoimmune disease , active infection requiring systemic therapy , known history of hiv infection , active hepatitis b virus or hepatitis c virus infection , a history of grade 4 ipilimumab - related adverse events or grade 3 ipilimumab - related adverse events lasting longer than 12 weeks , or previous treatment with any other anti - pd - 1 or anti - pd - l1 therapy . the study was conducted in accordance with the protocol , good clinical practice standards , and the vol 16 august 2015 articles see online for appendix declaration of helsinki . 
an external data monitoring committee reviewed interim trial results to ensure patient safety and to recommend whether the trial should continue in accordance with the protocol . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to pembrolizumab 2 mg / kg or pembrolizumab 10 mg / kg given intravenously every 3 weeks or investigator - choice chemotherapy ( paclitaxel plus carboplatin , paclitaxel , carboplatin [ eliminated with protocol amendment one ] , dacarbazine , or oral temozolomide )  . 
randomisation was strati ed by ecog performance status ( 0 vs 1 ) , lactate dehydrogenase concentration ( normal vs raised [ ie , 110% upper limit of normal ] ) , and braf status ( wild type vs v600 mutantpositive )  . 
after the second interim analysis , the external data monitoring committee indicated that the progressionfree survival superiority objective had been met and the study for reporting recommended unmasking purposes but continuing the study for overall survival at the nal analysis . 
at the second interim analysis and after the data monitoring committees recommendation , the treatment group was unmasked ; investigators and patients remained masked to the pembrolizumab dose . procedures patients were given their rst dose of study treatment within 3 days of treatment assignment . 
patients in the chemotherapy group with documented and veri ed disease progression at or after week 12 who met the relevant eligibility criteria could cross over to receive pembrolizumab after a washout period of at least 28 days from the last dose of chemotherapy ; patients who crossed over were randomly assigned to one of the two pembrolizumab doses in a double - blind manner . 
if the week 12 scan showed disease progression , patients were allowed to continue treatment until progression was con rmed at a subsequent scan response patterns.14 for atypical for purposes of statistical analysis , progressive disease per recist v1.1 was de ned as the rst documented disease progression , irrespective of con rmation at a second assessment . 
the criteria for removal of a patient from the study and details of permitted interruptions of study treatment are available in the study protocol ( appendix )  . to account tumour assessments were done before starting study treatment ( baseline ) , at week 12 , every 6 weeks through to week 48 , and every 12 weeks thereafter . 
we assessed patient - reported health - related quality of life and disease symptoms using the european organisation for the research and treatment of cancer ( eortc ) quality of life questionnaire c30 ( qlq - c30 )  . outcomes the primary endpoint at the second interim analysis was progression - free survival , the time from randomisation to rst documented disease progression per recist v1.1 by independent central review or death from any cause , whichever occurred rst . 
both progression - free survival assessed per recist v1.1 by investigator review and progression - free assessed per modi ed recist v1.1 ( where con rmation of disease progression on a scan 4 weeks after initial evidence of disease progression was required14 ) by investigator review were done as sensitivity analyses . 
secondary endpoints included the proportion of patients who had an objective response , the proportion of patients who had a complete or partial response as assessed per recist v1.1 by central review ( patients without post - baseline disease assessment were considered to be non - responders ) ; response duration , the time from best overall response of complete or partial response until disease progression ; and safety . 
 we estimated that with 370 events ( deaths ) among a total of 510 patients in the three treatment groups ( 170 patients per group ) , and assuming that the median overall survival in the chemotherapy group is 6 months and the hazard ratio between pembrolizumab and chemotherapy is 065 , the study would have at least 90% power to detect the overall survival di erence least one pembrolizumab group using the hochberg testing procedure15 at a 2% level ( one sided )  . in at before recommendations from the external data monitoring committee to unmask the study treatment allocation , both the rst and second interim analyses were done by an unmasked statistician . 
the rst planned interim analysis on nov 13 , 2013 , focused on detecting whether one pembrolizumab dose was inferior to the other , with the possible decision of discontinuing one pembrolizumab dose , and safety . 
the second interim analysis ( reported here ) was planned to occur after at least 270 progression - free survival events ( about 180 events between one pembrolizumab group and the chemotherapy group ) occurred , at which time 210 deaths were anticipated . 
at the second interim analysis , the study had 92% power to detect a hazard ratio ( hr ) of 055 for progression - free survival at a one - sided of 025% between one pembrolizumab group and the chemotherapy group . 
the study would be considered positive at this interim analysis if the one - sided p value for progression - free or overall survival was lower than 00025 in either pembrolizumab group compared with the chemotherapy group ; based on 270 progression - free survival events , the observed hr that would meet the criterion for a positive trial was 066 . 
because the study completed enrolment 3 months earlier than expected and the death rate was lower than was expected , the timing of the second interim analysis was driven by the targeted number of deaths . 
although overall survival was not the primary endpoint of the second interim analysis , comparisons for each pembrolizumab group compared with the chemotherapy group were tested at an of 025% . 
because the prespeci ed threshold for declaring superiority of pembrolizumab over chemotherapy was met for progression - free but not overall survival , the data monitoring committee recommended that the study could be unmasked but that follow - up should continue as planned . 
 we calculated hrs and associated 95% cis with a strati ed cox proportional hazard model with efrons method of tie handling.16 the strati ed miettinen and nurminen method17 was used to compare the the proportion of patients achieving an objective response between treatment groups . 
the corresponding author had the nal responsibility to submit for publication . results between nov 30 , 2012 , and nov 13 , 2013 , we enrolled 540 patients from 73 sites in 12 countries ( full site list available in the appendix )  . 
we randomly allocated patients to pembrolizumab 2 mg / kg ( n = 180 ) , pem brolizumab 10 mg / kg ( n = 181 ) , or chemotherapy ( n = 179 [ 42 patients to paclitaxel plus carboplatin , 28 to paclitaxel , 13 to carboplatin , 45 to dacarbazine , and 43 to temozolomide ; eight did not receive treatment ] ; gure 1 )  . 
visceral metastases ( stage m1c ) and elevated lactate dehydrogenase concentrations , poor prognostic factors for advanced melanoma , were observed in 446 ( 83% ) and 218 ( 40% ) of the 540 patients , respectively , at baseline . 
most patients received two or more previous lines of including chemotherapy in just under half of the patients ; a quarter of patients had received braf or mek inhibitor ( table 1 )  . 
of the 179 patients allocated to the chemotherapy group , 86 ( 48% ) crossed over to pembrolizumab treatment , with 46 randomly assigned to receive 2 mg / kg and 40 to receive 10 mg / kg . for advanced disease , therapy 912 vol 16 august 2015 articles based on 410 total progression - free survival events the ( recist v1.1 , central review ) , pre - speci ed criteria to show signi cant improvement in progression - free ratios of 057 ( 95% ci 045073 ) for pembrolizumab 2 mg / kg and survival , with hazard the study met 050 ( 95% ci 039064 ) for 10 mg / kg compared with chemotherapy ( p < 00001 for both ; table 2 )  . 
 * a breakdown of progression - free survival events is provided in the appendix.hrs and associated 95% cis were based on cox regression models with treatment as a covariate strati ed by ecog performance status ( 0 vs 1 ) , lactate dehydrogenase concentration ( normal vs raised ) , and brafv600 status ( mutant vs wild type )  . 
||accounts for patients who withdrew consent , were withdrawn by the investigator , died , or started new anticancer therapy before the rst tumour assessment and therefore did not have response evaluated , or patients with tumour assessments , but overall response based on the scans was not evaluable . 
di erence calculated based on miettinen and nurminen method covariate strati ed by ecog performance status ( 0 vs 1 ) , lactate dehydrogenase concentration ( normal vs raised ) , and brafv600 status ( mutant vs wild type )  . 
by 6 months , about a third of patients assigned to pembrolizumab were progression free ( 34% assigned to 2 mg / kg and 38% assigned to 10 mg / kg ) , whereas only 16% assigned to chemotherapy had not progressed ( table 2 )  . 
at 9 months , about a quarter of patients assigned to pembrolizumab were progression pembrolizumab 2 mg / kg pembrolizumab 10 mg / kg chemotherapy number at risk pembrolizumab 2 mg / kg pembrolizumab 10 mg / kg chemotherapy number at risk pembrolizumab 2 mg / kg pembrolizumab 10 mg / kg chemotherapy articles free ( 24% assigned to 2 mg / kg and 29% assigned to 10 mg / kg ) compared with 8% assigned to chemotherapy ( table 2 )  . in a post - hoc analysis , restricted mean progression - free survival time based on the area under the kaplan - meier curve up to 12 months19 was 54 months ( 95% ci 4760 ) for the pembrolizumab 2 mg / kg group , 58 months ( 5164 ) for the pembrolizumab 10 mg / kg group , and 36 months ( 3241 ) for the chemotherapy group . 
 pembrolizumab also signi cantly improved progressionfree survival when assessed by investigator review , with a larger treatment e ect for pembrolizumab ( table 2 ) and a greater separation of the curves ( gure 2b ) , although possible investigator bias in a partly open - label trial such as this might explain the greater e ect size . 
a protocolspeci ed supportive analysis of progression - free survival per investigator review that assessed progression only if it was observed in two consecutive scans also showed a signi cant treatment e ect favouring pembrolizumab ( table 2 , gure 2c )  . 
the superiority of both pembrolizumab doses was evident in all prespeci ed patient subgroups ( gure 3 )  . immature overall survival data , which were evaluated at a small level at this interim analysis , did not meet the prespeci ed 025% superiority threshold for each pembrolizumab dose compared with chemotherapy ( data not shown )  . 
final overall survival will be assessed after 370 deaths . on independent central review , 38 ( 21% ) patients in the pembrolizumab 2 mg / kg group and 46 ( 25% ) in the 10 mg / kg group responded to treatment as per recist v1.1 criteria , compared with eight ( 4% ) in the chemotherapy group ( p < 00001 for each pembrolizumab dose vs chemotherapy )  . 
median time to response was 13 weeks ( iqr 1218 ) in the pembrolizumab 2 mg / kg group , 15 weeks ( 1218 ) in the pembrolizumab 10 mg / kg group , and 13 weeks ( 1218 ) in the chemotherapy group . 
at the time of analysis 35 ( 92% ) of 38 responders in the pembrolizumab 2 mg / kg group , 40 ( 87% ) of 46 responders in the pembrolizumab 10 mg / kg group , and ve ( 63% ) of eight responders in the chemotherapy group remained progression free . 
35 ( 19% ) of 180 patients in the pembrolizumab 2 mg / kg group and 37 ( 20% ) of 181 patients in the pembrolizumab 10 mg / kg group were treated beyond initial evidence of disease progression . of the 540 patients enrolled , 528 received at least one dose of study treatment and were assessed for safety ( gure 1 )  . 
median time on treatment was 113 days ( range 1499 ) in the pembrolizumab 2 mg / kg group , 145 days ( 1505 ) in the pembrolizumab 10 mg / kg group , and number at risk pembrolizumab 2 mg / kg pembrolizumab 10 mg / kg chemotherapy time ( months ) figure 2 : kaplan - meier estimates of progression - free survival assessed in the intention - to - treat population kaplan - meier curves for recist v1.1 - assessed progression by independent central review ( a ) , recist v1.1 , by investigator review ( b ) , and modi ed recist v1.1 , by investigator review ( c )  . 
the day after the rst pembrolizumab dose , the patient presented with a bleeding pelvic mass causing severe pahe was also found to have melaena , possibly from existing small bowel metastases . 
after the analysis cuto date , the causality of this death was changed by the investigator to be unrelated to treatment . incidence of grade 34 treatment - related adverse events was higher in those given chemotherapy ( 45 [ 26% ] of 171 patients ) than in those given pembrolizumab ( 20 [ 11% ] of 178 patients ] in the pembrolizumab 2 mg / kg group and 25 [ 14% ] of 179 patients in the 10 mg / kg group )  . 
 the most common grade 34 treatment - related adverse events in the pembrolizumab 2 mg / kg treatment group were fatigue , generalised oedema , and myalgia ( two [ 1% ] each )  . 
the most common grade 34 treatment - related adverse events observed in those given pembrolizumab 10 mg / kg were hypopituitarism , colitis , diarrhoea , decreased appetite , hyponatraemia , and pneumonitis ( two [ 1% ] each )  . 
the most most common grade 34 treatment - related adverse events observed in patients given chemotherapy were anaemia ( nine [ 5% ] ) , fatigue ( eight [ 5% ] ) , neutropenia ( six [ 4% ] ) , and leucopenia ( six [ 4% ] )  . 
 treatment interruption as a result of treatment - related adverse events was needed in 15 ( 8% ) of 178 patients treated with pembrolizumab 2 mg / kg , 15 ( 8% ) of 179 patients treated with pembrolizumab 10 mg / kg , and 30 ( 18% ) of 171 patients treated with chemotherapy . 
 treatment - related adverse events led to permanent treatment discon tinuation in ve ( 3% ) patients given pembroli zumab 2 mg / kg , 12 ( 7% ) given pembrolizumab 10 mg / kg , and 10 ( 6% ) patients given chemotherapy . 
 the most common serious treatment - related adverse events observed in the combined pembrolizumab treatment groups were diarrhoea and pneumonitis ( three [ 1% ] of 357 patients each )  . 
treatment - related adverse events more common with chemotherapy were alopecia , anaemia , decreased appetite , fatigue , nausea , and vomiting ; those more frequent with pembrolizumab were rash and pruritus ( table 3 )  . 
consistent with previous experience , the adverse event pro les of the 2 mg / kg and 10 mg / kg doses were generally similar.10 , 11 adverse events of a potentially immune - mediated nature were infrequent , and none were of grade 4 or 5 severity ( appendix )  . 
these events were generally manageable 04 06 08 14 16 favours pembrolizumab favours chemotherapy figure 3 : prespeci ed subgroup analysis of progression - free survival progression - free survival assessed by recist v1.1 , by independent central review in the intention - to - treat population ; pembrolizumab 2 mg / kg versus chemotherapy ( a ) and pembrolizumab 10 mg / kg versus chemotherapy ( b )  . 
one additional patient in the pembrolizumab 2 mg / kg treatment group died because of an adverse events considered to be possibly related to treatment at the time of data cuto ( full details provided in text )  . 
one additional patient treated with pembrolizumab 10 mg / kg had arthralgia of unspeci ed severity . table 3 : treatment - related adverse events chemotherapy groups the least squares mean change from baseline to week 12 in the score was 260 ( 95% ci 615 to 096 ) in the pembrolizumab 2 mg / kg group , 255 ( 599 to 089 ) in the 10 mg / kg group , and 913 ( 1286 to 539 ) in the chemotherapy group ( appendix )  . 
the least squares mean change signi cantly di ered between the 2 mg / kg pembrolizumab and ( 653 , the 10 mg / kg 95% ci 1531153 ; p = 0011 ) and ( 657 , and pembrolizumab 1651150 ; p = 0009 )  . 
the global health status quality - of - life score deteriorated by 10 points or more in approximately 7% to 12% fewer patients in the pembrolizumab treatment groups than in the chemotherapy group at week 12 ( 64 [ 38% ] of 167 patients in the chemotherapy group , 56 [ 32% ] of 176 patients in the pembrolizumab 2 mg / kg group , and 47 [ 27% ] of 177 patients in the pembrolizumab 10 mg / kg group ; appendix )  . chemotherapy groups discussion in this population of patients with advanced melanoma that progressed on ipilimumab and , in many cases , on inhibitors , pemchemotherapy or mapk pathway brolizumab reduced the risk of disease progression or death compared with investigator - choice standard - of - care chemotherapy . 
although median progression - free survival values were similar , around the time of the rst scheduled tumour assessment at week 12 in all treatment groups , the kaplan - meier curves separated dramatically thereafter , indicating the treatment e ect . the ability of ipilimumab - refractory disease respond to pembrolizumab is probably a re ection of the di erent mechanisms by which anti - ctla - 4 and anti - pd - 1 therapies stimulate an anti - tumour t - cell response . 
ctla - 4 blockade broadens the immune response , evidenced by an increased t - cell receptor repertoire leading to increased tumour in ltration , 2023 whereas pd - 1 blockade induces intratumoural t - cell 916 vol 16 august 2015 articles proliferation without detectable changes peripheral immune repertoire.12 , 2427 the those assigned five times more patients had an objective response with pembrolizumab than did chemotherapy . 
these results support the food and drug administrations accelerated approval of pembrolizumab in this poorprognosis population . although our study was not powered to assess the equivalence of the two pembrolizumab doses , the results of the two interim analyses do not suggest a signi cant , clinically meaningful , di erence between the doses . 
the absence of a signi cant di erence between the pembrolizumab doses is consistent with ndings in a similar population treated in the keynote - 001 study.10 , 11 taken together , there is no evidence that one pembrolizumab dosing regimen is superior to another . 
therefore , the minimally e ective pembrolizumab dose of 2 mg / kg given every 3 weeks is recommended for further use . hypophysitis , hypothyroidism , pembrolizumab was well tolerated compared with chemotherapy , with treatment - related and fe wer grade 34 adverse events in the pembrolizumab groups despite an approximately two - fold longer duration of exposure . 
potentially immune - mediated adverse events colitis , such pneumonitis , hepatitis , and nephritis were observed with pembrolizumab , although they were infrequent and mostly of grade 1 or 2 severity . 
the bene t of pembrolizumab is further strengthened by the favourable health - related quality - of - life scores compared with chemotherapy . immunosuppressive therapy and two recent studies of nivolumab ( an anti - pd - 1 antibody ) have reported an improvement in objective responses compared with chemotherapy in patients who had previously received ipilimumab28 and improvement in overall survival compared with chemotherapy in patients with brafv600 wild - type melanoma.29 furthermore , pembrolizumab given to patients who were ipilimumab treatment - naive showed improvement in responses , progression - free survival , and overall survival compared with ipilimumab.30 combined with our study ndings , these data support the remarkable activity of pd - 1 blockade in patients with advanced melanoma . 
overall , targeting of the pd - 1 axis is a major advancement in melanoma and establishes pembrolizumab as a new standard treatment after progression on ipilimumab and other therapies . contributors ad , se , ae , spk , jmk , xnl , jl , sjod , ar , cr , and wz conceived , designed , or planned the study . 
all authors revised and reviewed this work and all authors had nal approval of the submitted manuscript . declaration of interests ar reports fees to his institution from merck for serving as an advisory board member . 
rd reports grant support from bristol - myers squibb ( bms ) and advisory board honoraria from bms , glaxosmithkline ( gsk ) , merck sharp & dohme ( msd ) , novartis , and roche . 
ds reports grant support and study fees to his institution from merck ; personal fees for serving as an advisory board , steering committee , and speakers bureau member and for travel and hotel support from bms , merck , novartis , and roche - genentech ; and personal fees for advisory board and speakers bureau membership from amgen and boehringer ingelheioh reports grant support from and personal fees for serving as a speaker for bms and merck . 
fsh reports personal fees , nonnancial support , and clinical trial support to his institution from merck , grant and nonnancial support and clinical trial support to his institution from bms , and clinical trial support to his institution from genentech . 
ldc reports receiving funding to his institution from merck for conduct of clinical trials ; grant support to his institution from bms and genentech ; and serving as a speaker programme member for bms and genentech . 
paa reports grants and personal fees from bms , roche - genentech , and ventana ; personal fees and nonnancial support from msd ; and personal fees from amgen , novartis , and gsk , all outside of the submitted work . 
cl reports personal fees for serving as an advisory board member from amgen , biontech , bms , celgene , msd , and roche ; personal fees for lectures from bms , msd , and roche ; and personal fees for consulting from biontech , celgene , and roche . 
smg reports personal fees and nonnancial support from bms for travel support and providing expert testimony ; from msd for travel support and advisory board membership ; and research funding from the university hospital zurich . 
we thank the patients and their families and caregivers ; all primary investigators and their site personnel ( see appendix ) ; tricia brown and melanie leiby ( the apo group , yardley , pa , usa ) , for assistance with manuscript editing ; james r anderson ( university of nebraska medical center , omaha , ne , usa ) , ronald blum ( albert einstein college of medicine and beth israel medical center , new york , ny , usa ) , janice dutcher ( cancer research foundation , new york , ny , usa ) , and lawrence flaherty ( barbara ann karmanos cancer institute , detroit , mi , usa ) , for serving on the external data monitoring committee ; je maca ( quintiles , morrisville , sc , usa ) , for serving as the unmasked study statistician ; eric rubin and alise reicin ( merck sharp & dohme ) , for critical review of the manuscript and supervision of the study group ; cong chen ( merck ) for critical review of the manuscript and statistical expertise ; and clara benner , linda gammage , claudia geis , klaas koekenbier , amanda mcdonald , kathleen oxberry , lei pang , theodora paraskevopoulos , andrea perrone , kathryn schneck , sigalit segal , sophie vauclair , and jen villetard ( all of merck ) for critical study support . oncology , fake news , and legal liability in trust between the the decline lay public and professional opinion is a major chal lenge . 
at the centre of this crisis , is a collision between personal autonomy , specious journalism , social media , widespread dis infor mation , and political marginalisation , which together undermine the value placed on science and academic endeavour . 
in oncology , this situation manifests itself in numerous waysmost notably through patient selfdiagnosis and demand for specific treatments irrespective of their doctors advice ; escalating numbers of patients using alternative unproven therapies ; and increasing reliance on socalled defensive medicine to fend off lawsuits . institute in 2017 , researchers in a jama oncology study published on july 19 , 2018 , and in an earlier article in the journal of the national cancer investigated the association between the use of complementary and alternative medicine , adherence to conventional treatment , and overall survival in patients with cancer . 
 found that patients using together , the studies complementary medicine are more likely to refuse surgery , radiotherapy , or chemotherapy , and patients using complementary or alternative medicine are more than twice as likely to die than those treated with conventional medicine . 
how has society got to this point , where unproven interventions are being chosen in preference to evidencebased , effective treatments ? unfortunately , disinformation andfranklylies are propagated widely and with the same magnitude as verified evidence due to the ease with which social media , ubiquitous online news platforms , and disreputable marketing exercises can populate information channels , which often do not have sufficient funding to employ subjectspecific journalists to weed out facts from fiction . a further consequence of public distrust in mainstream medicine , spread by socalled fake news , misreporting , or contradictory stories , is a tendency for doctors to overtreat patients to prevent claims of malpractice . 
this number was met with scepticism , but a recent us national bureau of economic research working paper provides some evidence to support the under lying hypothesis that huge sums of money are spent needlessly . 
the article shows the fear of lawsuits increases us healthcare expenditure by about 5% ( equivalent to about $170 billion ) and outcomes for patients who get extra care are no better than in those who do not . 
numerous legal reforms have been suggested to shield doctors from excessive liability , including immunity from malpractice claims , caps on the amount of damages awarded , or the use of administrative courts rather than juries . 
 despite these existential pressures , according to the 2018 medscape oncologist compensation report , twothirds of us oncologists still say the most rewarding part of their job is their relationship with patients , the challenge of making the right diagnosis , or being proud of the job they do . 
however , the report , which surveyed over 20 000 oncologists , also found that 41% were worried about the number of rules and regulations they must comply with , problems associated with dealing with difficult patients , or being sued , all of which emphasises the levels of stress health professionals are exposed to and the constant battle against external factors beyond the satisfaction of their core role . in the current era of fake news and public distrust in the establishment , efforts must be redoubled to better communicate medical advances accurately with the lay public and with patients to ensure genuine knowledge can be separated from false material . 
for example , the uk charity , macmillan cancer support , has recently hired a digital nurse specialist to help debunk fake news via an online questionandanswer service , and the us national institutes of health give detailed tips on how to evaluate health information on the internet . 
 if these challenges are not addressed soon , the great advances in science and medicine that have markedly improved human health worldwide could be easily undone and society will come to regret such inaction and reliance on unreliable sources of information . 
high - dose radiotherapy with shortterm or long - term androgen deprivation in localised prostate cancer ( dart01 / 05 gicor ) : a controlled , randomised , phase 3 trial . 
in the fth paragraph in the results section , the number of patients in the short - term group who died of cancer , but not of the prostate , should read 14 ( 8% ) and the number in the long - term group should read three ( 2% )  . 
ramucirumab versus placebo second - line folfiri in patients with metastatic colorectal carcinoma that progressed during or after rst - line therapy with bevacizumab , uoropyrimidine ( raise ) : a randomised , double - blind , multicentre , phase 3 study . 
 lancet oncol 2014 ; 15 : 131931in gure 3 of the article , the prevalence of hpv type 18 in oral cavity in africa should read 18% , and in oropharynx in oceania hpv type 18 should appear as the second most common type after 16 , and before 35 , with a prevalence of 17% . 
however , given that one in two people will be diagnosed with cancer in their lifetime , and with the prospect of a growing and ageing population , the absolute number of people living with cancer is set to increase substantially in the near future . 
a cancer diagnosis is a serious and potentially life - threatening condition , and there is no desire to trivialise it , but a reluctance to speak about diagnosis , treatment , and supportive care , out of fear or stigma , isolates patients and their carers . 
moreover , this silence prevents survivors from grappling with the more mundane , but crucial , aspects of long - term care and survival , such as reintegration into home and work life after end of treatment , behaviours for long - term wellness , and end - of - life considerations . although online forums , patient support groups , and charity and advocacy groups exist to support those living with cancer , the mainstream media is uniquely positioned to widely disseminate stories and viewpoints of people living with and surviving cancer . 
 such advocacy can simultaneously give a voice to the issues and educate the public about the diversity of people living with cancer and their experiences , as well as reveal the areas where medicine and society could better serve the survivor community as a whole . 
in one such column in the new york times , called living with cancer , susan gubar , a professor emeritus of english at indiana university , in , usa , uses her experience as a survivor of ovarian cancer to discuss the realities , challenges , and hopes of patients with cancer and survivors . 
columns like these serve to inculcate the general public with an understanding , and thereby acceptance of , cancer as a part of life . by contrast , the mainstream media has done less well at illuminating end - of - life care for patients with terminal illness . 
an example that bucks the trend , however , is the emergence of death cafes , as reported recently in the guardian : these meetings are opportunities to discuss the often overlooked and di cult aspects of end - of - life care , such as preparing for death and quality of death . 
shedding light on the issues patients face at this juncture is crucial to improve end - of - life care as well as to break the silence around this di cult topic . 
death cafes o er venues for supportive discussion of the anxieties surrounding death , and their existance highlights both the desire and need for these types of dialogue . mainstream media could go further to raise the pro le of cancer and end - of - life care beyond a few column inches in newspapers and magazines , using more subtle means to capture the experience of patients , carers , and medics . 
inclusion of characters and storylines via the arts ( for example , in the british radio sitcom bad salsa ) that incorporate cancer not as the subject , but simply as one aspect of a story , help us to trans gure the feared and unknown into the familiar and routine fabric of the public consciousness . cancer is becoming an ever - expanding presence in our society , and we would bene t from reconciling its ability to scare and isolate with its ubiquity and c , cancer must longer the big survivability . 
an increasing focus and re ection on cancer in the mainstream media is a good way of destigmatising and desensitising issues among the general public , while also bringing comfort , hope , and perhaps , some useful advice to patients and survivors alike . 
 the lancet oncology vol 17 march 2016 for more on how brexit will affect health services in the uk see lancet 2019 ; 393 : 94958 for the no - deal brexit practical guidance from the rcr see sites / default / files / no_deal_ brexit_planning_guidance_ for_nuclear_medicine_teams_ march_2019.pdf for more on the privatisation of imaging services in the nhs see society / 2019 / mar / 06 / nhscancer - centre - loses - scanningcontract - to - private - firm brexit , radiology , and nhs privatisation : a tragedy for frontline care ? the uks exit from the european union ( eu ) is arguably one of the worst self - inflicted harms any country has done to itself in peace - time . 
in a health policy piece in the lancet in 2017 , and updated in february , 2019 , fahy and colleagues state that brexit will have negative consequences for the uks leadership and governance of health , in both europe and globally . 
an editorial in the lancet on march 2 , 2019 , went further , emphasising : there is no good news for the nhs ( national health service ) ...in all scenarios , depletion of the nhs workforce is inevitable , care for uk nationals living in the eu is uncertain , and access to medicines , vaccines , and devices hangs in the balance . 
indeed , the provision of diagnostic imaging and radiopharmaceuticals for patients with cancer is one key specialty in which the consequences of brexit are multiple and potentially catastrophic . on march 5 , 2019 , the uk royal college of radiologists ( rcr ) , in collaboration with the british nuclear medicine society and the uk radiopharmacy group , issued practical guidance to nuclear medicine physicians on how to manage brexit in a no - deal scenario . 
the advice states that there might be delays to deliveries ; nuclear medicine teams should try to keep their workloads light in the first week postbrexit ; teams should consider the use of alternative radiopharmaceuticals where possible ; and certain patients should be prioritised over others . 
the uk government has stated that , in the event of a no - deal , the uks major radioisotope suppliers have committed to 6 - month air freight contracts as a contingencyrather than run the risk of road transport delays . 
inevitably , this contingency raises major concerns about the increased delivery costs and who will pay for them , and the problems caused by the time of day in which a delivery is made for radiopharmaceuticals that need processing on - site prior to use . the rcr guidance also gives specific advice about radionuclide therapies , and notesrather worryingly that it is only aware of one supplier that is confident of being able to continue to supply therapeutics on a specific schedule after brexit . 
the potential for medical error or waste of radiotracers and radiotherapeutics are therefore manifestly high post - brexit . and , if these challenges in access to essential reagents werent enough to destabilise health care in the uk , new developments in the increasing privatisation of the nhs certainly will . 
an announcement on march 6 , 2019 , stated that the churchill hospital in oxford , uk , will no longer carry out its own pet - ct services ; rather , the tender has been given to inhealth , a private company . 
shockingly , nhs england has invited profit - driven companies to bid against nhs trusts for pet - ct services in 11 different regions across the country , including major teaching hospitals such as kings college hospital in london and the christie hospital in manchester . 
 most importantly , privatisation of frontline patient services necessitates a moment to reflect on whether this is truly in the best interests of patients and what consequences it might have on the safety and quality of care . 
short - term , fragmented , financial gains often do not translate in to long - term advantages in complex health - care systems . patients with cancer in the uk face substantial challenges in accessing the best care . 
despite attempts to reduce such inequities , they persist in the form of geographical limitations , resource allocation , availability of various specialised services , access to cancer medicines , a shortfall in the numbers of consultants and other health - care professionals , and now , two additional barriers to the quality of care : increasing privatisation of frontline services , and a maelstrom of unknowns related to brexit and its impact on all aspects of the nhs . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections prevention , treatment , and profit : an unsustainable alliance world cancer day , on feb 4 , 2019 , had at its core a message of early detection and screening . 
a focus on screening has obvious advantages , but how best to integrate prevention into health services , and the risk of overtreatment , are sources of debate . several strategies have aimed to bring screening to the public more directly , rather than relying on attendance at designated appointments . 
in england , in light of the failure to meet 2018 targets for breast , bowel , and cervical cancer screening , the national health service ( nhs ) has pledged to increase early diagnosis of cancers by 75% over the next 10 years . 
in canada , the screen for life mobile life coach also provides tests for breast , cervical , and colon cancer for individuals near their places of work , with the aim of improving general uptake of these services . 
although any population - based screening increases the chance of overdiagnosis and can be compromised by complex lifestyle and societal factors , precision prevention in high - risk individuals is a useful approach to tackle the cancer burden , while providing a good trade - off between the benefits and harms . 
early diagnosis not only improves outcomes and reduces mortality , it also lessens the reliance on cancer drugs , some with highly debatable clinical benefit , that drain billions of dollars from health - care systems each year . a recent who report shows that even in highincome countries , there are huge disparities in access to , and most notably the pricing of , cancer medicines . 
 the findings , although not surprising , are stark : prices of cancer drugs have continued to increase year on year , sometimes even doubling within 5 years , and with the increasing use of more and more complex immunotherapies , prices are likely to rise further . 
 it is sobering to see , in the who report , not only incurred by pharmaceutical a breakdown of costs companies and the apparent disconnect between cost and profit , but also the huge variation in drug pricing strategies between countries . 
the wholist for cancer drugs endorsed essential medicines is still unaffordable in many places ; in low - income countries , 57% of drugs on the list are available only if patients pay for the full cost of treatment themselves . 
for drug companies , who can reduce their original asking price by as much as 70% , what does this say about the elasticity of their prices ? with an average return of us$1450 on every $1 invested in research and development , there is no doubt room for manoeuvre . 
8 years later , the findings of the who report reiterate that the problem is now even more rampant , and drastic measures are needed to tackle what seems to be gross profiteering by the pharmaceutical industry . agencies regulatory and health - care systems are integral to easing cancer burden . 
in the uk , the national institute for health and care excellence has a firm grip on the introduction of drugs into the nhs and is essential to maintaining cost - effectiveness , but even with this regulation , the nhs still continues to face chronic funding problems . 
 this burden will only be reduced by addressing prevention and profit in paralleland , if profit margins continue to remain out of reach , one of the most effective ways will be to reduce the reliance on these medicines altogether . 
we aimed to identify risk factors for the extent of ovarian damage in women with hodgkins lymphoma treated with different chemotherapy regimens to inform accurate advice on options for fertility preservation . methods we recruited female participants from the randomised phase 3 rathl trial , aged 1845 years , based on availability of participants at recruiting sites in the uk . 
the rathl trial key inclusion criteria were histologically confirmed classic hodgkins lymphoma , stage iibiv or iia with adverse features ( bulky disease or more than two sites of involvement ) , no previous treatments , and a performance status of 03 . 
as part of rathl , participants were treated with two cycles of doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) or avd followed by an interim pet - ct scan . 
participants who had negative interim scans ( pet score of 1 to 3 according to the lugano classification ) were randomly assigned ( 1 : 1 ) by use of minimisation , stratified by interim pet score and study centre , to continue abvd or avd for four more cycles . 
participants with positive scans ( pet score of 4 or 5 ) were escalated to treatment with bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone ( beacopp - 14 or escalated beacopp ) for four cycles . 
for the protocol - driven prospective cohort substudy , ovarian function was assessed before treatment , during chemotherapy , and then annually for 3 years by use of serum antimllerian hormone and follicle - stimulating hormone measurements . 
at 1 year after chemotherapy , antimllerian hormone concentrations recovered to a median of 105 pmol / l ( iqr 43173 ) in the abvd - avd group , but little recovery was seen after beacopp ( median 011 pmol / l [ 007020 ] )  . 
 age also affected the extent of ovarian function recovery , with antimllerian hormone recovery in participants aged 35 years or older in the abvd - avd group to 37% ( sd 10 ) of their before treatment concentrations , compared with full recovery to 127% ( sd 12 ) in those younger than 35 years ( p < 00001 )  . 
follicle - stimulating hormone recovery to less than 25 iu / l occurred for 95% of women younger than 35 years in the abvd - avd group by 2 years and was also dependent on age ( hazard ratio 049 , 95% ci 037065 ; p < 00001 )  . interpretation reduced recovery of ovarian function observed in women older than 35 years treated with abvd or avd compared with younger women indicates that treatment could reduce their reproductive lifespan and supports discussion of fertility preservation before treatment . 
these findings warrant further investigation in large , prospective studies with fertility and reproductive lifespan as outcomes . funding medical research foundation and cancer research uk . copyright 2018 the author ( s )  . 
systemic treatment from chemotherapy regimens based on alkylating agents , which had a high risk of infertility and premature ovarian condition has evolved this for insufficiency in women , to treatment with doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) , which is the current treatment of choice for many adult patients with hodgkins lymphoma . 
both age and ovarian reserves before treatment are predictive of ovarian recovery after chemotherapy with some regimens , but their importance is unknown for treatments for patients with hodgkins lymphoma . added value of this study we found that changes in antimllerian hormone concentration could distinguish between the effects of treatment on ovarian function with doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) or avd , and bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone ( beacopp ) in patients with advanced hodgkins lymphoma , particularly from 3 years of follow - up after chemotherapy . 
treatment with abvd or avd was confirmed to have little gonadotoxcity in female patients with hodgkins lymphoma who were younger than 35 years at diagnosis ; however , in older patients ( 35 years ) recovery of ovarian function was affected by age . 
we found that among older women baseline concentrations of antimllerian hormone did not affect recovery , so reduced hormone recovery in older women was not due to the age - related decline in ovarian reserve . 
little recovery in ovarian function was seen after treatment with beacopp in women of all ages , although a similar number of pregnancies was observed in the two treatment groups . 
due to the small size of the cohorts analysed , these results warrant further confirmation . implication of all the available evidence the absence of detectable ovarian damage after treatment with abvd or avd in younger women with hodgkins lymphoma is reassuring , although longer follow - up is needed in future studies for a full assessment of potential reproductive effects . 
 the finding of reduced ovarian recovery in older women with hodgkins lymphoma treated with chemotherapy indicates that age - specific discussions and consideration of fertility preservation procedures should be considered before treatment . 
these considerations are of growing importance given the increasing age at which women are having children in developed countries . intensification could benefit patients who are at higher risk of relapse , and some clinicians advocate treatment with bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone ( beacopp ) for patients with advanced stage or high - risk early stage disease . 
however , female gonadal toxicity is high with dose - escalated beacopp resulting in amenorrhoea ( a surrogate marker of pre mature ovarian insufficiency ) in about 95% of patients older than 30 years.3 analysis of the effects of cancer therapies on the ovaries requires consideration of both the degree of loss of ovarian function during chemotherapy and changes in ovarian function thereafter . 
the degree of loss of the primordial follicle pool ( the ovarian reserve ) during chemotherapy is the most important effect since it determines the potential for any recovery of ovarian function and fertility , and subsequent age at menopause , although the degree of loss cannot be assessed in vivo . 
the full eligibility criteria for the rathl trial are available in the protocol . for this prospective cohort substudy , women and aged 1845 years ( ie , premenopausal ) were actively recruited from rathl sites in the uk ( appendix pp 35 )  . 
the protocol for the substudy is available online . this cohort substudy received centralised ethical committee approval that covered all sites ( national research ethics service , southampton and south west hampshire ) and all participants gave written informed consent . procedures in the rathl study , after initial staging and a baseline pet - ct scan , participants were treated with two cycles of abvd , intravenously , on days 1 and 15 of a 28 days cycle followed by an interim pet - ct scan ( doses and schedule in the appendix [ p 2 ] )  . 
participants who had negative interim scans by central review ( pet score of 1 to 3 per lugano criteria ) were randomly assigned ( 1 : 1 ) by the cancer research uk and university college london cancer trials centre using minimisation , with stratification according to pet score ( 1 , 2 , or 3 ) and centre , to continue abvd ( intravenously , days 1 and 15 ) or to receive doxorubicin , vinblastine , and dacarbazine ( avd ; intravenously , days 1 and 15 ) for four more cycles . 
participants with positive scans ( pet score of 4 or 5 ) were escalated to either beacopp - 14 for six cycles of 14 days or escalated beacopp for four cycles ( doses and schedule in the appendix [ p 2 ] )  . 
neither patients nor study staff were masked to allocation . ovarian function was assessed by use of serum concentrations of antimllerian hormone in participants enrolled into this substudy and follicle - stimulating hormone concen trations from all eligible participants ( women and aged 1845 years ) from the rathl trial . 
oestradiol measurements are necessary for the identification of women with premature ovarian insufficiency.11 during the rathl trial , blood samples were taken before any treatment , after two cycles of initial abvd treatment , at the end of chemotherapy , and at 1 , 2 , and taken after 3 years after chemotherapy . 
follicle - stimulating hormone measure ments were done locally as part of the rathl trial ; additional samples from participants enrolled in this substudy were taken to measure antimllerian hormone , follicle - stimulating hormone , luteinising hormone , and oestradiol concen trations by use of roche elecsys assays ( automated cobas e 411 1330 vol 19 october 2018 articles analyser , roche , burgess hill , uk )  . 
the substudy samples were sent by post to a central laboratory ( mrc centre for reproductive health , edinburgh ) , where the serum was stored at 20c until analysis . 
the antimllerian hormone assay has a limit of detection of 007 pmol / l , and for all assays the interassay and intra - assay coefficients of variation were below 5% . 
a follicle - stimulating hormone threshold of more than 25 iu / l indicated probable premature ovarian insuffi ciency.11 after recovery from chemotherapy , antimllerian hormone was additionally analysed in association with predictors from before treatment , specifically age and antimllerian hormone concentration . 
the study was not designed to assess fertility , and menstrual bleeding was not recorded since it does not help to distinguish between women with normal ovarian function and those with very depleted ovarian reserves . data on previous pregnancy or use of hormonal contraceptives were only collected from participants enrolled in the ovarian function substudy . 
decisions regarding fertility preservation procedures were between the participant and the local centre , and were not recorded as part of the study . outcomes the primary outcome of this study , specified as an exploratory outcome in the rathl trial , was assessment of gonadal function . 
the prespecified outcomes in this substudy were analysis of acute toxic effects of each treatment regimen on the ovaries , and ovarian function after treatment ( including progression to ovarian failure and recovery of ovarian function )  . 
other prespecified outcomes were the association between fertility after treatment and ovarian function before treatment , degree of acute ovarian toxic effects , which will be reported separately . statistical analysis as a secondary analysis of the rathl trial , the prespecified exploratory analyses presented here are not powered ; we aimed to recruit as many patients as possible while the rathl trial was open . 
we hypo thesised that antimllerian hormone concentrations could show differences between the gonadotoxicity of the chemo therapy regimens in the rathl trial , both during and after treatment , and that concentrations of antimllerian hormone before treatment would be predictive of recovery of ovarian function after treatment . 
we analysed antimllerian hormone and follicle - stimulating hormone concentrations in the ovarian subgroup after log transformation using anova with bonferronis multiple comparisons test for changes during treatment and recovery . 
 * one patient in this group had a missing performance status . table : baseline characteristics 4 ( 2% ) 4 ( 2% ) 4 ( 2% ) concentration of antimllerian hormone against percentage hormone recovery ( calculated as [ concentration at 2 yearsconcentration before treatment ] x 100 ) and against concentration at 2 years . 
we measured time to recovery ( follicle - stimulating hormone concentration of 25 iu / l ) from the end of treatment until the first follicle - stimulating hormone measurement of 25 iu / l or less , or a reported pregnancy ( whichever came first )  . 
patients with follicle - stimulating hormone concentrations of more than 25 iu / l at baseline were excluded , and patients who had neither event were censored at the last reported follicle - stimulating hormone measurement . 
 beacopp = bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisolone . hazards using schoenfeld residuals , and when it did not hold we used restricted mean survival times with a 3 year cutoff . 
all p values are two - sided and a p value of less than 005 was considered statistically significant . data analyses were done in stata ( version 15.1 ) and graphpad prism 7 . 
the corresponding author had final responsibility for the decision to submit for publication . results between dec 13 , 2010 , and dec 19 , 2012 , participants from the rathl trial were recruited for this ovarian function substudy ( figure 1 ; appendix p 3 )  . 
seven ( 10% ) of 74 registered participants were excluded from the substudy and the main trial , six for scan protocol deviations , and one for psychological reasons , leaving 391 ( 94% ) of 415 eligible ( 1845 years ) female rathl participants , of whom 321 ( 82% ) were evaluable for follicle - stimulating hormone analyses , and 67 ( 91% ) were evaluable for substudy analyses . 
of the 67 evaluable participants for the substudy analyses , 24 ( 36% ) had been treated with abvd , 33 ( 49% ) with avd , four ( 6% ) with beacopp - 14 , and six ( 9% ) with escalated beacopp . 
no difference in baseline hormone concentrations were found between treated with abvd versus avd , or partici pants beacopp - 14 versus escalated beacopp ( table ) ; thus these subgroups were combined as abvd - avd ( n = 57 ) and beacopp ( n = 10 ) , respectively , for subsequent analyses . 
the baseline characteristics of the participants who had follicle - stimulating hormone measurements from the rathl trial , and the combined abvd - avd and beacopp subgroups evaluated in this substudy are in the table . for nine participants in the substudy , data at postbaseline timepoints were not available because of disease progression and further treatment ( six in the abvd - avd group , three in the beacopp group ) , and 13 blood samples were missing or taken at incorrect timepoints . 
 eight blood samples taken from eight women during pregnancy in the ovarian subgroup were excluded from analysis . antimllerian hormone concentrations decreased in all participants during chemotherapy treatment with reciprocal increases in follicle - stimulating hormone concentrations ( figure 2 )  . 
in the abvd - avd group , concentrations of antimllerian hormone decreased from a median of 98 pmol / l ( iqr 59181 ) before treatment to 17 pmol / l ( iqr 0443 ) at the end of treatment ( p < 00001 ) , with a small rise between cycle two of initial abvd treatment and the end of treatment ( p < 00001 )  . 
after chemotherapy in the abvd - avd group , concentrations of antimllerian hormone increased to 105 pmol / l ( iqr 43173 ) at 1 year , similar to concentrations before treatment , with no change at later timepoints ( figure 2 )  . 
antimllerian hormone was undetectable in two ( 4% ) of 56 participants at the end of treatment with follicle - stimulating hormone concentration higher than 25 iu / l and low oestradiol insufconcentrations ficiency . 
for one of these participants , antimllerian hormone became detectable during recovery , and for the other , antimllerian hormone showed a transient recovery at 1 year after treatment , becoming undetectable thereafter . indicating premature ovarian 1332 vol 19 october 2018 articles 0 in the beacopp group , concentrations of anti mllerian hormone decreased from a median of 68 pmol / l ( iqr 22128 ) before treatment to 008 pmol / l ( 007024 ) at the end of treatment ( p < 00001 ; figure 2 )  . 
after treatment , by contrast with participants in the abvd - avd group , concentrations of antimllerian hormone showed very little recovery ( median 011 pmol / l [ iqr 007020 ] at 1 year ) and were undetectable in five ( 71% ) of seven participants at 3 years ( figure 2a )  . follicle - stimulating hormone concentrations had generally reciprocal changes compared with concentrations of antimllerian hormone and increased during treatment in both groups ( figure 2b )  . 
 concentrations of luteinising hormone showed the same pattern of changes , increasing from before treatment to the end of treatment in both groups ( both p < 00001 ) and then recovering after treatment to before - treatment concentrations in the abvd - avd group , but remaining significantly increased after treatment in the beacopp group ( data not shown )  . in women both antimllerian hormone concentration 2 years after treatment and follicle - stimulating hormone recovery data provide evidence of the effect of age on ovarian treated with abvd or avd recovery ( figures 3 and 4 )  . 
we saw a correlation between the concentration of antimllerian hormone before treatment and at 2 years after treatment ( r = 089 ; p < 00001 ) but not with antimllerian hormone recovery ( r = 030 ; p = 0051 )  . 
 however , significant and similar negative correlations were seen between age and antimllerian hormone concentrations at 2 years ( r = 040 ; p = 00055 ) and with antimllerian hormone recovery ( r = 040 ; p = 00080 )  . 
analysis of antimllerian hormone concentrations before treatment grouped by whether they were below or above the overall median value ( 977 pmol / l [ iqr 59181 ] ) showed that recovery was similar between the two groups ( below 123% [ sd 21 ] vs above 103% [ sd 9 ] ; p = 085 )  . 
 multiple linear regression analysis also confirmed that age had a significant effect on antimllerian hormone recovery ( = 043 ; p = 0004 ) , but that antimllerian hormone con centrations before treatment did not have an effect on hormone recovery ( = 015 , p = 030 )  . 
 r = 089 ; p < 00001 r = 030 ; p = 0051 antimllerian hormone before treatment ( pmol / l ) antimllerian hormone before treatment ( pmol / l ) r = 040 ; p = 00055 r = 040 ; p = 00080 age ( years ) age ( years ) figure 3 : correlations of antimllerian hormone recovery and before treatment hormone concentrations or age for the abvd - avd group panels show scatter plots of baseline hormone concentration versus concentration at 2 years ( a ) and versus percentage hormone recovery ( b ) , and age versus hormone concentration at 2 years ( c ) and percentage hormone recovery ( d )  . 
each dot shows antimllerian hormone concentration or recovery ; recovery was calculated for each participant as the concentration at 2 years after treatment as a proportion of the concentration before treatment . 
 thus , although overall concentrations of antimllerian hormone after treatment seem to recover to before treatment concentrations , the degree of recovery is restricted by increasing age . we also assessed the degree and timecourse of recovery of ovarian function , as indicated by normalisation of follicle - stimulating hormone concentrations , in the evaluable participants from the rathl trial ( figure 4 )  . 
folliclestimulating hormone measurements after treat ment were available from 321 women in the rathl trial , with a median follow - up ( censoring at recovery ) of 593 months ( iqr 419609 )  . 
follicle - stimulating hormone concentration recovery to 25 iu / l or lower was seen in 270 ( 96% ) of 282 of participants treated with abvd or avd , compared with 26 ( 67% ) of 39 treated with beacopp - 14 or escalated beacopp ( hazard ratio [ hr ] 037 , 95% ci 025056 ; p = 00001 )  . 
evaluable female participants ( n = 391 ) were divided by chemotherapy regimen received : abvd or abvd followed by avd ( abvd - avd group ) , and abvd followed by beacopp - 14 or escalated beacopp ( beacopp group )  . 
 kaplan - meier estimates for participants treated with abvd or avd were 75% ( 95% ci 7080 ) 1 year after treatment and 93% ( 8995 ) 2 years after treatment , whereas the estimates for those treated with beacopp were 33% ( 2052 ) 1 year after treatment and 69% ( 5284 ) 2 years after treatment . 
the relative difference in ovarian function ( between abvd or avd and beacopp ) did not differ when analysed by age ( < 35 years , hr 038 , 95% ci 023062 ; p = 00001 vs 35 years , hr 040 , 019083 ; p = 0011 )  . 
this pattern was also found when analysed by use of restricted mean survival ( recovery ) times ( < 35 years , 1546 days for abvd or avd and 4465 days for beacopp [ difference : 2919 days , 95% ci 16344204 ; p < 00001 ] vs 35 years , 3615 days for for abvd or avd and 6634 days for beacopp [ difference 3019 days , 95% ci 9415097 ; p = 0005 ] )  . 
however , age seemed to affect time to recovery among these participants , with a smaller proportion of those aged 35 years or older showing recovery at both 1 year ( 41 [ 50% ] ) and 2 years ( 64 [ 79% ] ) after treatment than those younger than 35 years did ( 176 [ 79% ] at 1 year and 211 [ 95% ] at 2 years after treatment ; hr 049 , 95% ci 037065 ; p < 00001 )  . 
 thus , the kaplan - meier estimates for follicle - stimulating hormone concentration recovery for those younger than 35 years treated with abvd or avd were 83% ( 95% ci 7788 ) at 1 year and 96% ( 9398 ) at 2 years compared with estimates for those aged 35 years and older of 54% ( 4366 ) at 1 year and 83% ( 7391 ) at 2 years . 
we saw no difference in follicle - stimulating hormone recovery between participants treated with escalated beacopp or beacopp - 14 for all ages ( hr 072 , 95% ci 033156 )  . in the rathl cohort , 64 ( 16% ) of 391 participants were recorded as having 81 pregnancies . 
in the subgroup cohort , antimllerian hormone measurements were available within the follow - up period for six women who became pregnant in the abvd - avd group and two in the beacopp group . 
at 1 year after chemotherapy , con centrations of antimllerian hormone ranged from 074 pmol / l to 269 pmol / l in those who became pregnant in the abvd - avd group , and were 019 pmol / l and 020 pmol / l in those in the beacopp group . 
two women , one in each treatment group , had follicleunde tectable antimllerian hormone , high stimulating hormone , and low oestradiol concentrations after the recorded pregnancy , consistent with development of premature ovarian insufficiency within 3 years of chemotherapy treatment . adverse event data were reported in detail previously , 17 but they did not include any data on ovarian function or fertility . 
 discussion in this prospective cohort study , we have shown that antimllerian hormone concentrations decrease in women with hodgkins lymphoma who are treated with abvd , avd , or beacopp ( beacopp - 14 or escalated beacopp ) , and although antimllerian hormone concentrations recover to baseline concentrations after treatment with abvd or avd , little recovery is seen after treatment with beacopp . 
however , we found 1334 vol 19 october 2018 articles that recovery of ovarian function after treatment with abvd or avd is dependent on age , with full recovery of antimllerian hormone seen in participants younger than 35 years , but not in women aged 35 years or older . 
follicle - stimulating hormone recovery after treatment with abvd or avd was slower in women aged 35 years or older than in those younger than 35 years , and the extent of recovery was much lower for those treated with either beacopp regimen , supporting the increased ovarian toxicity of this drug combination . 
the greater toxicity to other organ systems is also reflected in the higher incidence of febrile neutropenia and thrombocytopenia with beacopp . the potential adverse effect of chemotherapy on ovarian function in women with hodgkins lymphoma is of major concern , affecting fertility , sexual and bone health , and cardiovascular risk . 
potential loss of fertility is a key concern of young women treated for cancer18 and , when appropriate , options for fertility preservation have been established ; thus , the accurate assessment of the is of effect of different chemotherapy regimens substantial importance . 
assessment of ovarian function after treatment via menstrual function and traditional biomarkers such as follicle - stimulating hormone are not of value in detecting ovarian damage that has resulted in incomplete loss of ovarian function . 
measurement of concentrations of antimllerian hormone has emerged as a reliable biomarker to detect partial loss of ovarian function in women after cancer therapy , with the additional advantages of showing little variation across the menstrual cycle.12 although most data are from women after treatment for breast cancer and childhood cancer , 5 , 7 , 8 we have shown the merit of antimllerian hormone measurements in the assessment of ovarian function in adult women with hodgkins lymphoma . 
 specifically , younger women treated with abvd or avd showed full initial recovery of antimllerian hormone after chemotherapy , consistent with previous data2 that indicate that this regimen has little effect on age at menopause , but reduced recovery was seen in women aged 35 years or older at diagnosis . 
by contrast , treatment with beacopp resulted in noticeable and irreversible decreases in antimllerian hormone con centrations , so low in many women that the hormone was undetectable after treatment even with the highly sensitive assay we used . 
participants received either escalated beacopp or beacopp - 14 , a dose - intense version that appears to be similarly gonadotoxic to baseline beacopp.3 our data support this similarity , although the confidence intervals in our estimates were wide . antimllerian hormone concentrations decreased quickly during treatment with both regimens , consistent with both treatments resulting in loss of the growing follicles that are the source of antimllerian hormone . 
this finding is consistent with increased activation of early follicles during chemo therapy resulting from reduced inhibition of growth initiation , which is proposed to be part of the mechanism for chemotherapy - induced premature ovarian insuffi ciency . 
this mechanism has been shown for high toxicity , cyclophosphamide - based regimens , 19 but has not previously been identified for low toxicity regimens such as abvd or avd . the degree of recovery of antimllerian hormone after treatment with abvd or avd in young women could indicate a low toxic effect on the non - growing primordial follicle pool , which constitutes the true ovarian reserve and is the basis for after treatment fertility and the duration of the female reproductive lifespan . 
under physiological conditions , antimllerian hormone con centrations reflect the size of the primordial follicle population , although this population size can be perturbed under circumstances such as a new diagnosis of lymphoma.20 however , the 3 - year follow - up period in this study is likely to have been sufficient for full recovery of ovarian function and therefore restoration of physio logical associations between antimllerian hormone and the ovarian reserve . 
we saw a prominent effect of age on recovery , with substantially lower recovery in women aged 35 years or older than in those younger than 35 years , independent of their antimllerian hormone concentration before treatment . 
 this finding indicates an effect either of age alone or of age in addition to the effects of abvd or avd that result in a substantial decrease in the size of the growing follicle population , and by implication of the non - growing population , after treatment . 
chemotherapy has been shown to affect both the stroma and vasculature of the human ovary , causing fibrosis and hyalinisation of small vessels with loss of primordial follicles within areas of damage.4 changes in ovarian stromal function with age include fibrosis and other hallmarks of chronic inflammation , such as the presence of macrophages , 21 and can impair follicle development.22 these changes could be reversed by gonadotropin suppression , 22 indicating that the increases in concen trations of luteinising hormone and follicle - stimulating hormone during chemotherapy shown here could be of aetiological importance , and the pre - existing more fibrotic stroma in older women could be more susceptible to chemotherapy - induced changes than the stroma in younger women , even with so - called low gonadotoxicity regimens such as abvd or avd . 
these age - associated effects of chemotherapy could have therapeutic implications and be part of the mechanism of action of gonadotropin - releasing hormone agonists to reduce the risk of premature ovarian insufficiency after chemotherapy for breast cancer , 23 , 24 although this effect has not been confirmed for women treated for lymphoma.25 vol 19 october 2018 1335 articles the effect of age on recovery of ovarian function after both regimens , and the different toxic effects of each regimen on the ovaries , is also supported by our analysis of follicle - stimulating hormone recovery in the whole rathl study cohort . 
in this analysis , follicle - stimulating hormone was dichotomised at a value consistent with premature ovarian insufficiency.11 in addition to confirming the effect of age on recovery from treatment with abvd or avd , our analysis showed clear differences in both the speed and extent of recovery between regimens , supporting the antimllerian hormone data . 
folliclestimulating hormone concentrations are affected to a much greater extent than antimllerian hormone concentrations by changes across the menstrual cycle and use of hormonal contraception , but our analysis shows measurement of follicle - stimulating hormone concentrations is of value in large cohorts in which more detailed characterisation is difficult . previous analyses in women with breast cancer have shown that receiving treatment at a young age and high concentrations of anti mllerian hormone before treatment are predictive of recovery of ovarian function after chemotherapy , albeit with variable relative contributions.5 , 9 , 14 , 15 women with breast cancer are generally older ( approximate mean age 40 years5 , 9 , 14 , 15 ) than those with hodgkins lymphoma and treatment involves more gonadotoxic alkylating agent - based regimens , resulting in a high probability of premature loss of ovarian function , particularly in women older than 40 years . 
 these differences emphasise the need for defined populations and treatment regimens to analyse the toxic effects of chemotherapeutic regimens on the ovaries and , particularly , recovery . the data in this study support the paucity of the value of current ovarian reserve markers for the prediction of fertility in the short term , because very low concentrations of antimllerian hormone did not preclude chances of pregnancy . 
the lack of predictive value of anti mllerian hormone measurements for short term fertility has been shown in prospective cohorts of women mostly in their twenties and thirties , 26 , 27 and in women after cancer treatment.28 this study was not designed to assess chances of pregnancy after treatment , and indeed current clinical advice is that women should not attempt to conceive after chemotherapy for around 12 yearsie , most of the duration of follow - up in this study . 
we do not know how many women in each group attempted to conceive , but a similar proportion of pregnancies were seen in women in the beacopp group as in the abvd - avd group within the substudy . 
although these results show that a low concentrations of antimllerian hormone do not preclude pregnancy in the short term , they probably do indicate a reduced interval to menopause and thus a shortened duration of opportunity to achieve pregnancy in the longer term.29 thus , a low concentration of antimllerian hormone after recovery from chemotherapy could identify women who should not unduly postpone pregnancy , and inform individualised discussion ; longer follow - up studies are needed to assess this interpretation . our study had several limitations . 
we also acknowledge the limitations of using follicle - stimulating hormone measurements in isolation without a more robust evidence of premature ovarian insufficiency , which was not possible in the main rathl trial , and data on hormonal contraceptive use during and after treatment were not available . in conclusion , the results of this secondary analysis of the rathl trial indicate the value of antimllerian hormone as a biomarker of toxic effects of chemotherapy on the ovaries during and after different chemo therapy regimens for advanced hodgkins lymphoma . 
we provide additional evidence that treatment with abvd or avd has no detectable effect on gonadal function in young women , although increasing age does restrict ovarian recovery ; confirmation in larger studies is needed to confirm and define this interpretation more precisely , and determine its mechanisby contrast , beacopp shows substantial gonadotoxicity in women of all ages , although some patients might have sufficient ovarian function after to achieve pregnancy . 
concentrations of treatment antimllerian hormone after treatment could be of use in advising women treated for hodgkins lymphoma of their probable reproductive lifespan after treatment . contributors raa and pwmj designed the study ; collected , analysed , and interpreted data ; contributed to manuscript writing ; and approved the manuscript before submission . 
cr recruited patients , collected data , contributed to manuscript writing , and approved the manuscript before submission . declaration of interests raa reports non - financial support from roche diagnostics , and a grant from the medical research foundation . 
all other authors declare no competing interests . acknowledgments the rathl trial was funded by cancer research uk ( reference cruk / 07 / 033 ) , and the ovarian substudy by the medical research foundation ( reference 509909 )  . 
part of this work was done in the mrc centre for reproductive health , university of edinburgh , uk , which is funded by mrc centre grant mr / n022556 / 1 . 
we thank roche diagnostics for the supply of assay reagents , a forbes howie for hormone assays , and all investigators in rathl for their contributions to patient recruitment and management . 1336 vol 19 october 2018 articles 2 correction to lancet oncol 2018 ; 19 : 94052 correction to lancet oncol 2018 ; 19 : 123946 zhu ax , finn rs , edeline j , et al . 
lancet oncol 2018 ; 19 : 94052in this article , the affiliation of dr vittorina zagonel should have been istituto oncologico veneto - istituto di ricovero e cura a carattere scientifico ( iov - irccs )  . 
 apatinib combined with oral etoposide in patients with platinum - resistant or platinum - refractory ovarian cancer ( aeroc ) : a phase 2 , single - arm , prospective study . 
lancet oncol 2018 ; 19 : 123946in this article , the statistical analysis section should have stated that at least three responses were required to continue to the second stage . 
 these corrections have been made to the online version as of aug 30 , 2018 . vol 19 september 2018 e440 corrections correction to lancet oncol 2018 ; 19 : e10212 sundar s , khetrapal - singh p , frampton j , et al . 
 lancet oncol 2018 ; 19 : e10212in this series paper , in the section titled challenges from womens cancer in india , the second sentence of the second paragraph should read despite this initiative , large - scale implementation of cancer prevention and control strategies has yet to take place , and public expenditure on health remains low at 12% of indias gross domestic product . 
this correction has been made to the online version as of may 31 , 2018 . correction to lancet oncol 2018 ; 19 : 72829 correction to lancet oncol 2018 ; 19 : 54961 iarc monographs vol 121 group . 
lancet oncol 2018 ; 19 : 54961in figure 3 of this article ( published online first on feb 20 , 2018 ) , the heatmap in panel a has been replaced to amend display errors . 
this correction has been made to the online version as of may 31 , 2018 . vol 19 june 2018 e283 corrections corrections correction to lancet oncol 2015 ; 16 : 133 correction to lancet oncol 2015 ; 16 : 181 , 184 correction to lancet oncol 2015 ; 16 : 237 published online january 29 , 2015 s1470 - 2045 ( 14 ) 70483 - 8 dp . 
 radiotherapy lancet oncol 2015 ; 16 : 23739in this comment , the fth line of the third paragraph should read : by contrast , acute gastrointestinal toxicity was increased with hypofractionation [ 95% ci 372469 ] of ( 420% patients the hypofractionation group had grade 2 adverse events vs 312% [ 266358 ] in the standard fractionation di erence 108% , 90% ci 5251643 ; p = 00015 ) although were similar 3 months after treatment , and non - inferiority was not con rmed . 
these corrections have been made to the online version as of march 2 , 2015 , and have been made to the printed comment . group , cavalli f , atun r . 
lancet oncol 2015 ; 16 : 13334 in this comment , the second sentence should have been : deaths from cancer are projected to increase from the present level of around 8 million a year to more than 13 million by 2030 , with most of the burden being in poorer countries . 
this correction has been made as of jan 29 , 2015 . correction to lancet oncol 2015 ; 16 : 266 ih , williams lj , kunkler jack wjl , cameron da , dixon jm , on behalf of investigators . 
 lancet oncol 2015 ; 16 : 26673in the interpretation section of the summary , the rst sentence should read postoperative whole - breast radiotherapy after breast - conserving surgery and adjuvant endocrine treatment resulted in a signi cant but modest reduction in local recurrence for women aged 65 years or older with early breast cancer 5 years after randomisation . 
this correction has been made to the online version as o f march 2 , 2015 , and to the printed article . thomas a , rajan a , berman a , in patients with et al . 
lancet oncol 2015 ; 16 : 17786 in the key of gure 2a of this article , the text for the red line should read thymic carcinoma ( 16 / 24 failed ) and that for the blue line should read in the thymoma ( 11 / 16 failed )  . 
 key of gure 4b , the text for the red line should read no change / increase ( 0 / 18 failed ) and that for the blue line should read decrease ( 4 / 4 failed )  . 
lancet oncol 2015 ; 16 : 27483in this article , the interpretation should have read : hypofractionated radiotherapy was not non - inferior to standard fractionated radiotherapy in terms of acute genitourinary and gastrofor men with intestinal intermediate - risk high - risk and prostate cancer . 
this correction has been made to the online version as of march 2 , 2015 and to the printed article . toxicity vol 16 march 2015 e105 corrections correction to lancet oncol 2015 ; 16 : 1045 correction to lancet oncol 2015 ; 16 : 1499 tournigand c , chibaudel b , samson b , et al . 
 this correction has been made to the online version as of nov 29 , 2015 . correction to lancet oncol 2015 ; 16 : 1355 , 1363 hegewisch - becker s , graeven u , lerchenmller ca , et al . 
maintenance strategies after first - line oxaliplatin plus uoropyrimidine plus bevacizumab for patients with metastatic colorectal cancer ( aio 0207 ) : a randomised , noninferiority , open - label phase 3 trial . 
 lancet oncol 2015 ; 16 : 135569the fourth line of the findings section of the summary of this article should read bevacizumab alone was noninferior to standard uoropyrimidine plus bevacizumab ( hazard ratio [ hr ] 108 [ 95% ci 085137 ] ; p = 053 ; upper limit of the one - sided 988% ci 142 ) , whereas no treatment was not ( hr 126 [ 099160 ] ; p = 0056 ; upper limit of the one - sided 988% ci 165 )  . 
 lancet oncol 2015 ; 16 : 14931505in this article , the colours of the curves in both panels of gure 3 were inverted ; the correct version is shown below . 
 these corrections have been made to the online version as of nov 29 , 2015 . events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 49 ( 41 - 57 ) 54 ( 43 - 62 ) stratied hazard ratio 081 ( 066101 ) p = 0059 ( log - rank ) unstratied hazard ratio 078 ( 068096 ) p = 0019 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0023 events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 221 ( 196267 ) 249 ( 214289 ) stratied hazard ratio 079 ( 063099 ) p = 0036 ( log - rank ) unstratied hazard ratio 079 ( 064098 ) p = 0035 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0024 number at risk bevacizumab bevacizumab plus erlotinib time ( months ) number at risk bevacizumab bevacizumab plus erlotinib vol 16 december 2015 e589 editorial to read the lancet oncologys previous editorial on direct - to - consumer advertising see leading edge lancet oncol 2008 ; 9 : 1113 us legislation for direct - to - consumer advertising : paternalism or common sense ? consumers of their own health in the past few decades , the marketing of health - related direct - to - consumer products and services has become ubiquitous . 
simultaneously , a spate of new health - care companies has ushered in a new age of patient - driven , on - demand medicine , in which patients are proactively engaged care . 
 on march 3 , 2016 us senator al franken introduced legislation to end tax breaks for drug manufacturers marketing medicines directly to the consumer , a move that is part of a growing trend in recent months to minimise the prevalence of such advertising in the usa . 
last month , us congresswoman rosa delauro introduced a bill calling for a 3 - year moratorium on advertising newly approved prescription medicines , and in november last year , the american medical association called for an outright ban of such advertising on the grounds that it fuelled escalating drug prices . 
although these moves are welcome in curbing direct - to - consumer advertising , how can we maintain active patient involvement , while simultaneously safeguarding patients from potential harms and misinformation ? and , whose responsibility is it to do so ? in the case of 23andme , a company o ering personal genomic tests , the 2013 decision by the us food and drug administration ( fda ) to stop the sale and marketing of its saliva collection kit was clearly fair and valid . 
the tests were banned on the grounds that the regulator had received no assurances from the company that the personal genome service was analytically or clinically validatedan issue that remains at the heart of concerns facing publically available genetic tests . 
notably , neither consumers nor physicians have the expertise to interpret the tests complex genetic information and due consideration must be given to what consumers could do with their results , especially since many identi able carcinogenic mutations are not actionable . 
an overly reductionist approach to genetic testing may also lead to an over - reliance on such information to determine an individuals risk of developing cancer and their subsequent treatment plan , potentially undermining a more holistic approach to patient care . 
 although con ned to genetic testing , the 23andme story is re ective of a growing concern of the e ects of direct - to - consumer marketing and what steps should be taken to regulate the industry . 
as noted by the american medical association , such advertising can in ate demand for newer , more expensive treatments , even when these drugs might not be appropriate , and in spite of the clinical e cacy of less costly alternatives . 
 there are also issues regarding the scienti c validity of such diagnostic tests and medicineswhich are often based on early - stage researchand an overemphasis of potential bene ts alongside a downplaying of potential harms . 
research has also shown there is a growing trend towards self - diagnosis and self - treatment using illicit online pharmaceuticals as a result of direct - to - consumer marketing online . 
this is evidenced by a recent case of a patient in the usa whoafter being diagnosed with a brain tumour as part of volunteer studyhad amassed nearly 70 gb of personal medical data , partly as a result of direct - to - consumer medical testing . 
although it is unknown how this data was subsequently used , the ease and accessibility of such information , although liberating for an individual who wants to be in command of their health , raises issues of data privacy , should commercial entities wish to use this information in a way which is not compliant with a consumers wishes . 
 although tighter regulation has been seen as the key to tackle direct - to - consumer advertising , several reports have concluded that the fda is insu ciently rigorous to undertake this task , and that it lacks the resources and the authority to regulate safety . 
it is welcome news , therefore , that attempts like the ones from senator franken and congresswoman delauro are now using legislation as a means to balance consumer protection while still fostering scienti c discovery . 
even so , as new information platforms continue to evolve , direct - to - consumer advertising will continue to manifest itself in new ways , even if su cient regulation or legislation is implemented . 
it is therefore vital that we reiterate one of our prior editorials that advocated such advertised services and products are o ered by health professionals alone , and only accessed on the basis of their advice . 
lancet oncol 2016 ; 17 : 26566 in this comment , the second sentence of the sixth paragraph should read the proportion of these patients who achieved a pcr was 36 ( 26% ) of 137 in the solvent - based paclitaxel group versus 67 ( 48% ) of 139 patients in the nab - paclitaxel group . 
these corrections have been made to the online version as of march 1 , 2016 , and the printed version is correct . vol 17 march 2016 correction to lancet oncol 2018 ; 19 : 95364 correction to lancet oncol 2018 ; 19 : 104050 correction to lancet oncol 2018 ; 19 : e386 kramer souweidane mm , pandit - taskar n , et al . 
this correction has been made to the printed article , and to the online version as of aug 1 , 2018 . moreau p , mateos m - v , berenson jr , et al . 
lancet oncol 2018 ; 19 : 95364in the methods section of this article , the exclusion criteria for new york heart association heart failure should have been class iii or iv . 
this correction has been made to the online version as of aug 1 , 2018 . vol 19 aug 2018 e382 corrections malignancies interest group database , 7 5% of patients with thymic carcinomas developed myasthenia gravis ; organotypia is usually mantained in thymic carcinomas and , therefore , confers a small risk of myasthenia gravis relative to thymomas . 
thus , the possibility of heterogeneity of thymoma and thymic carcinoma in one tumour challenges the use of immune checkpoint inhibitors for the treatment of thymic malignancies , both of which are associated with immune - related adverse events . the key limitations of this study will prevent immediate adoption of pembrolizumab versus other treatment for thymic carcinoma . 
first , pd - l1 expression has not been verified to be a reliable biomarker in this or other malignancies , but there are other immune components that might be better biomarkers for response to immune checkpoint inhibitors that have been used in previous studies.810 second , thymic carcinoma comprises histologically different subtypes of cancer . 
notably , the histological subtypes within the tumours of patients in this trial were 48% squamous cell carcinoma and 15% neuroendocrine carcinoma , which does not reflect the typical distribution of histological subtypes in thymic carcinoma . are ongoing although additional trials with immune checkpoint carcinoma , thymic inhibitors important . 
the small number of reproducibility patients in phase 2 trials does not have to be a limitation to achieving treatment advances for rare cancers : replicate sample collection in translational research can counter this shortcoming with demonstrated reproducibility . 
cooperative group collaborations , such as the international thymic malignancies interest group or the thoracic alliance for cancer trials , could be useful to generate sufficient evidence to solve this problem of small patient numbers . approved drugs for rare cancers are scarce , as giaccone and colleagues have mentioned ; the high cost of these drugs , such as sunitinib and pembrolizumab , make it difficult to treat patients with thymic carcinoma worldwide because many countries cannot afford these medicines . 
globally , treatment for recurrent thymic carcinoma is still often single - agent cytotoxic chemotherapy . giaccone and colleagues plan to investigate the combination of pembrolizumab and epacadostat as an immune - combination therapy in a future expansion of this phase 2 study . 
thus , we are facing the next step to develop further therapies for thymic malignancies . yusuke okuma department of thoracic oncology and respiratory medicine , tokyo metropolitan cancer and infectious diseases centre komagome hospital , tokyo 113 - 8677 , japan y - okuma@cick.jp i declare no competing interests . kelly rj , petrini i , rajan a , wang y , giaccone g . 
 clin cancer res 2013 ; 19 : 429596 . next - generation nuclear morphology to grade solid tumours a central task for surgical pathologists diagnosing tumours is to reliably assess tumour aggressiveness from morphologic features . 
typical components of grading systems are tissue architecture , degree of resemblance to the respective benign tissue , mitotic activity , necrosis , and aberrances in nuclear morphology ( ie , nuclear pleomorphism , variations chromatin size , nucleolar prominence , and published online february 2 , 2018 s1470 - 2045 ( 18 ) 30063 - 9 see articles page 356 vol 19 march 2018 comment distribution )  . 
flemming1 coined the term chromatin in 1879 when describing nuclear structures that could be stained with basic dyes in the interphase , whereas waldeyer2 introduced the term chromosome in 1888 when describing mitotic chromat soon after , chromosomal alterations in tumours were described by bovari , 3 who also hypothesised a causal role of unequal chromatin distribution in carcinogenesis . 
the dogma of all morphologists , that function follows form , also applies to chromatin structure , which directly affects genomic activity by activating or silencing genes and gene families . in our contemporary concept , chromatin contains the whole eukaryotic genome , rather densely packaged around histones ( h2a , h2b , h3 , and h4 )  . 
posttranslational modifications of histones ( eg , acetylation , methylation ) also determine chromatin compaction , structure , and dynamics , and it is not surprising that mutations in the genes responsible for these regulatory modifications are often seen in cancer.4 advances in sequencing technologies have massively broadened our knowledge of driver oncogenes and their role during tumour progression and have helped promote the development of therapeutic drugs , but a holistic view that integrates gene expression and higher chromatin regulation is yet to be established . 
 although most pathologists know that chromatin irregularities , especially coarse and clumped chromatin as seen under the light microscope , are typical of higher graded tumours , the diagnostic value of subnuclear morphology has not been unearthed so far . 
 dna cytometry , introduced in 1966 , is a simple approach to compare overall dna content in tumour cells and normal cells.5 this technique gained popularity because aberrant dna content ( aneuploidy ) was more common in more aggressive tumours and neoplastic lesions than in benign , reactive lesions . 
today , most clinicians and pathologists do not use data on dna ploidy in patient care , even though a re - evaluation of this technique might be warranted.6 to classify image analysis chromatin patterns with modern technology is an obvious next step in developing more standardised diagnostic algorithms that could become part of tumour grading in the future . that in the lancet oncology , kleppe and colleagues7 describe nucleotyping , an automated method to reveals determine chromatin heterogeneity relevant prognostic information in various solid tumour types , including colorectal , endometrial , and ovarian carcinoma . 
although the preparatory steps are similar to conventional dna cytometry ( eg , dissection of cells , feulgen stain , multiple images , etc ) , this procedure does not yield overall staining intensity ; instead , it gives a measure of chromatin organisation computed by the entropy of pixel grey levels . 
for all analysed tumour entities , survival times were consistently shorter in patients with chromatin heterogeneous tumours than patients with chromatin homogeneous tumours , and the prognostic value of chromatin heterogeneity was independent of other parameters in a cox analysis . 
 this is an important finding , especially because the technique is applicable to formalin - fixed , paraffinembedded tissue and could easily be added to any routine workflow complement conventional tumour grading . in pathology laboratories however , some questions rema is nucleotyping easily transferable to other academic institutes ? is this biomarker robust enough to perform comparably in a decentralised setting ? how relevant are the trained personnel who identified the nuclei of interest in terms of interobserver variability of the technique ? pending clarification of these questions , this excellent study serves as an example of next - generation morphology that might enrich the pathologists armamentarium in the digital future , which is only just beginning . glen kristiansen institute of pathology , university of bonn , 53127 bonn , germany glen.kristiansen@ukbonn.de i declare no competing interests . copyright the author ( s )  . 
archiv mikrosk anat 1888 ; 32 : 1122 . 276 vol 19 march 2018 comment published online february 8 , 2018 s1470 - 2045 ( 18 ) 30075 - 5 see articles page 370 bovari t . 
 denosumab is not inferior and might even be superior to zoledronic acid in reducing skeletal - related events and improving survival in patients with certain solid tumours.2 however , in a prospective , double - blind study2 comparing denosumab with zoledronic acid in patients with solid tumours ( except breast cancer ) or myeloma ( 10% of the study patients ) , an ad - hoc analysis suggested inferior survival for patients with myeloma treated with denosumab . 
this study had several limitations and zoledronic acid remained the standard of care for patients with myeloma.3 in the lancet oncology , noopur raje and colleagues4 report a large , randomised , double - blind , phase 3 study , in which patients were randomly assigned to either 4 - weekly intravenous zoledronic acid , the present standard of care for myeloma - related bone disease , or 4 - weekly subcutaneous denosumab . 
the study met its primary endpoint of non - inferiority for denosumab versus zoledronic acid regarding the time to first skeletal - related event ( hazard ratio 098 , 95% ci 085114 ; pnon - inferiority = 0010 )  . 
study patients had a high burden of bone disease : 1144 ( 67% ) of the 1718 enrolled patients had already had a skeletalrelated event before enrolment and 376 ( 44% ) of 859 patients in the denosumab group and 383 ( 45% ) of 859 patients in the zoledronic acid group had a first onstudy skeletal - related event . 
however , 60% of first onstudy skeletal - related events occurred during the first 3 months of the study and 81% in the first 6 months , suggesting that even potent osteoclast inhibitors could not prevent skeletal - related events in the short teras such , early identification of patients at risk and timely intervention are crucial to avoid bone complications . 
 in a post - hoc landmark analysis at 15 months , denosumab was associated with fewer skeletal - related events than zoledronic acid , but this analysis has to be interpreted cautiously and cannot confirm superiority of denosumab over zoledronic acid in skeletal - related event prevention . 
 although the study by raje and colleagues4 is the largest placebo - controlled study ever done in patients with myeloma , several questions remaonly patients with myeloma - related bone disease at diagnosis were enrolled and the benefits of denosumab patients without bone disease are uncertaa survival benefit for patients treated with zoledronic acid versus clodronate1 or placebo5 has been shown , but a survival benefit for denosumab over zoledronic acid has not yet been seen , and additional follow - up is needed . 
additionally , rankl is implicated in the growth , survival , and development of drug resistance vol 19 march 2018 comment articles e cacy of fewer than three doses of an hpv - 16 / 18 as04 - adjuvanted vaccine : combined analysis of data from the costa rica vaccine and patricia trials aime r kreimer * , frank struyf * , maria rowena del rosario - raymundo , allan hildesheim , s rachel skinner , sholom wacholder , suzanne m garland , rolando herrero , marie - pierre david , cosette m wheeler , for the costa rica vaccine trial and the patricia study groups summary background there is some evidence to suggest that one or two doses of the hpv vaccine provides similar protection to the three - dose regimen . 
the main aim of the study was to ascertain hpv - 16 / 18 vaccine e cacy in both full and naive cohorts and to explore protection conferred against non - vaccine hpv types , by number of doses received . methods summary data from the costa rica vaccine trial ( cvt ; nct00128661 ) and ~the patricia trial ( nct001226810 ) , two phase 3 , double - blind , randomised controlled clinical trials of the hpv - 16 / 18 as04 - adjuvanted vaccine in young women , were combined in a post - hoc analysis ( glaxosmithkline [ gsk ] e - track number 202142 ) to investigate the e cacy of fewer than three doses of the hpv - 16 / 18 vaccine after 4 years of follow - up . 
after exclusion of women with less than 12 months of follow - up or those who were hpv - 16 / 18 dna - positive at enrolment ( for the hpv - 16 / 18 endpoint ) , we calculated vaccine e cacy against one - time detection of incident hpv infections after three , two , and one dose ( s )  . 
 findings we assessed vaccine e cacy against incident hpv - 16 / 18 infection in the modi ed total vaccinated cohort ( 22 327 received three doses , 1185 two doses , 543 one dose )  . 
vaccine e cacy against incident hpv - 16 / 18 infections for three doses was 770% ( 95% ci 747791 ) , two doses was 760% ( 620853 ) , and one dose was 857% ( 707937 )  . 
 vaccine e cacy against incident hpv - 31 / 33 / 45 infections for three doses was 597% ( 560630 ) , two doses was 377% ( 124559 ) , and one dose was 366% ( 54 to 622 )  . 
vaccine e cacy against incident hpv - 16 / 18 infection for two - dose women who received their second dose at 1 month was 753% ( 542875 ) and 826% ( 423961 ) for those who received the second dose at 6 months ( cvt data only )  . 
vaccine e cacy against hpv - 31 / 33 / 45 for two - dose women who received their second dose at 6 months ( 681% , 270870 ; cvt data only ) , but not those receiving it at one month ( 101% , 420 to 433 ) , was similar to the three - dose group . interpretation 4 years after vaccination of women aged 1525 years , one and two doses of the hpv - 16 / 18 vaccine seem to protect against cervical hpv - 16 / 18 infections , similar to the protection provided by the three - dose schedule . 
these data argue for a direct assessment of one - dose e cacy of the hpv - 16 / 18 vaccine . funding us national cancer institute , national institutes of health o ce of research on womens health , and ministry of health of costa rica ( cvt ) ; glaxosmithkline biologicals sa ( patricia )  . introduction cervical cancer is a leading cause of cancer mortality in women worldwide , although the burden dis proportionately a ects women in low - income countries.1 human papillomavirus ( hpv ) type 16 causes about 50% of cervical cancers , followed by hpv - 18 ( 20% ) , and the remaining 30% are caused mainly by ten other carcinogenic types.2 prevention of hpv infection , especially hpv - 16 and hpv - 18 , could substantially reduce cervical cancer prevalence and subsequent mortality . prophylactic hpv vaccination with three doses given by a prime - prime - boost schedule during a 6 month period of either of the two commercially available vaccines ( hpv - 16 / 18 as04 - adjuvanted vaccine , cervarix [ gsk group of companies , rixensart , belgium ] and and costs hpv - 6 / 11 / 16 / 18 vaccine , gardasil [ merck , whitehouse station , nj , usa ] ) is highly e cacious in prevention of cervical hpv - 16 / 18 infections and related diseases.3 , 4 however , complexities associated with a three - dose programme are barriers to vaccination provision in many world regions.5 on the basis of immunological non - inferiority , two - dose schedules of the hpv - 16 / 18 and hpv - 6 / 11 / 16 / 18 vaccines are now licensed in adolescents ( age 9 years to 13 or 14 years ) in several countries . infrastructure the only published data for e cacy of fewer than three doses comes from a post - hoc analysis6 of the costa rica vaccine trial ( cvt ) in women who did not complete the three - dose regimen . 
women who received fewer than three doses also had strong and stable antibody responses that persisted during this period , although hpv - 16 / 18 antibody titres in recipients of one dose were almost four times lower than in those of two or three doses.7 similar analyses from other studies810 showed stable plateau antibody titres after the immediate decrease in the post - vaccination period after one , two , or three doses . since publication of cvt , new data for reduced - dose protection have come from non - inferiority immunogenicity studies , 810 in which the minimum titre needed for protection remains unknown as a result of the high vaccine e cacy . 
women were additionally excluded if their enrolment cervical status was hpv - 16 and hpv - 18 dna - positive ( or missing ) or if they had fewer than 300 days between rst and last pcr result ; modi ed total vaccinated cohort ( m - tvc ) for assessment of hpv - 16 / 18 - related endpoints . 
 776 vol 16 july 2015 articles with a single dose , or whether the special adjuvant of the hpv - 16 / 18 vaccine is the cause of one - dose e cacy . 
consequently , we focused on only the hpv - 16 / 18 vaccine . in cvt , 12 , 13 7466 young women were enrolled between june 28 , 2004 , and dec 21 , 2005 ; the main eligibility requirements were being aged 1825 years , of good general health , and neither being pregnant nor breastfeeding . 
women were excluded if they had preexisting medical conditions that precluded vaccination , had a history of hepatitis a or previous vaccination against it , or were unwilling to use contraception during the vaccination period . 
 women who reported no more than six lifetime sexual partners before study enrolment ( in some countries this criteria was not considered for women younger than 18 years ) , agreed to adequate contraception ( barrier methods in combination with a spermicide or hormonal contraception ) during the vaccination period , and had an intact cervix were eligible for inclusion . 
main exclusion criteria included a history of hepatitis a or previous vaccination against it , history of colposcopy , pregnancy or breastfeeding , chronic or autoimmune disease , or immunode ciency . investigators from both trials generated study - speci c analyses independently according to a prespeci ed analytical plan ; the summary data were merged to generate the combined analytical estimates . 
patients strati ed by study , number of vaccine doses received , and vaccine group using available data in the total vaccinated cohort in women with 12 or more months of follow - up time ( t - tvc )  . 
in the cvt only , women referred to colposcopy missed the dose if the vaccination window was closed when they returned to regular study visits . the protocols required all women to be observed every 6 months ( patricia ) or annually ( cvt ) during the 4 year follow - up . 
women identi ed to have low - grade squamous intraepithelial neoplasia or carcinogenic hpv - positive atypical squamous cells of undetermined intensi ed follow - up ( ie , repeat testing or referral to colposcopy or both , and , if indicated , biopsy and cervical excision signi cance underwent see online for appendix number of women number of events personyears rate per 100 person - years ( 95% ci ) vaccine e cacy ( 95% ci ) incident one - time detection of hpv - 16 / 18 3 doses ( standard regimen ) 11 110 11 217 2172 43 140 40 682 534 ( 512557 ) 123 ( 112134 ) 770% ( 747791 ) control 2 doses control 1 dose control 3 doses control 2 doses control 1 dose control 3 doses control 2 doses control 1 dose control incident detection of hpv - 16 / 18 that persisted for at least 6 months 11 104 11 209 1000 43 706 41 913 239 ( 224254 ) 026 ( 022031 ) 891% ( 868910 ) 11 104 11 203 2538 2271 1220 2573 2308 1234 1017 43 775 42 589 2576 2324 1234 1021 087 ( 056129 ) 760% ( 620853 ) 361 ( 289446 ) 066 ( 030125 ) 857% ( 707937 ) 458 ( 338608 ) 016 ( 005038 ) 897% ( 733969 ) 152 ( 107209 ) 008 ( 000040 ) 966% ( 817998 ) 236 ( 155346 ) 019 ( 015024 ) 870% ( 837897 ) 147 ( 136159 ) 012 ( 003032 ) 896% ( 689975 ) 112 ( 075162 ) 008 ( 000040 ) 951% ( 732998 ) 167 ( 100261 ) incident detection of hpv - 16 / 18 that persisted for at least 12 months table 2 : dose - strati ed vaccine e cacy against incident hpv - 16 / 18 infection for women in the modi ed total vaccinated cohort ( costa rica vaccine trial and patricia combined ) treatment ) ; missing or inadequate cytology was similarly sent to intensi ed follow - up in cvt . 
secondary endpoints were infections that persisted for at least 6 months ( de ned as two or more type - speci c positive tests at least 150 days apart , with no intervening hpv - negative results ) and at least 12 months ( as for 6 months , but for > 300 days )  . 
the distinction between the endpoints of one - time detection of incident hpv infection and persistent infection is that a case of persistent infection was de ned as a second detection of the hpv type in question occurring within the interval speci ed , without an hpv - negative result ( for the hpv type in question ) occurring between the two positive tests . 
however , this did not mean that a one - time detection of hpv did not also persist , but only that the criteria for an incident event was met when an infection was detected once . 
data safety monitoring groups reviewed safety data during the vaccination phase and as needed during follow - up . balance by arm and dose was assessed in the time total vaccinated cohort ( t - tvc ) , which included all women with at least 12 months of follow - up . 
the number of vaccine study visits ( ie , visits at enrolment , 1 month , and 6 months ) were directly linked to the number of doses a woman received ( ie , women who received only one or two vaccine doses in most instances did not attend the 1 month or 778 vol 16 july 2015 articles 6 month vaccine study visits [ or both of these visits ] and as a result did not receive the full vaccine series )  . 
outcome assessment therefore began at the 12 month study visit ( 301 days after enrolment ) because this visit was the rst study visit potentially attended by women in all dose groups . 
we did not include hpv results between 1 and 300 days after enrolment because of the bias by number of doses in sample availability ( and thus hpv ascertainment ) in this timeframe . 
follow - up ended at the time of an event ( eg , the date of the rst hpv - positive test in the sequence of hpv - positive tests that de ned the event )  . 
for women who did not have an event , follow - up ended on the date of the nal negative test ( including untested visits for virgins ) to ensure parallelism in outcome assessment between women who did and did not have events . for each group , event rates expressed per 100 personyears were calculated as the ratio of number of events to the total follow - up time . 
analyses were done separately on women who received only one dose , two doses irrespective of the schedule , and the full three - dose regimen ( which served as a benchmark to interpret the fewer - dose vaccine e cacy estimates )  . 
additionally , in our exploratory analysis , further strati cation of the twodose vaccine e cacy by time of the second dose ( at 1 month or at 6 months ) was assessed in cvt ; patricia was excluded because only 26 women received two doses on the 06 month schedule . the main analysis estimated di erences in hpv infection rates accumulated over the 4 year follow - up period between the hpv - vaccinated and hav - vaccinated women by number of doses received . 
numbers in the numerators were combined across the two studies , as were the denominators , and these summary counts were used to generate a combined vaccine e cacy by dose for each endpoint . 
vaccine e cacy was de ned as the percentage reduction in endpoint related to vaccine administration , estimated as the complement of the ratio of the attack rates in the hpv and control groups . 
the analysis was conditioned on the total number of events , and the 95% ci around the vaccine e cacy was derived from the ratio of the events in the vaccine group to the total events ; exact con dence limits were calculated using the mid - p exact approach . 
statistical adjustment of vaccine e cacy estimates was not used to account for underlying risk di erences by dose and group because strong di erences were not reported in baseline characteristics . 
exact methods were used in all instances except when they did not work because the sample size was too large ; in those instances , standard asymptotic methods were used to calculate p values . we tested heterogeneity in vaccine e cacy between the two studies using a poisson regression model with an interaction term for vaccination group by trial . 
 role of the funding source the patricia trial was funded by glaxosmithkline biologicals sa , who designed the study in collaboration with investigators , and coordinated collection , analysis , and interpretation of data , and preparation of the manuscript . 
the costa rica hpv vaccine trial was sponsored and funded by the national cancer institute ( nci ) , with funding support from the national institutes of health o ce of research on womens health . 
general characteristics and reasons for not receiving all three vaccine doses are described within dose , group , and study , as are follow - up times from enrolment within each study ( restricted to women with 12 months of follow - up ; t - tvc ; gure 1 )  . in the t - tvc group , the most common reason for missed doses was pregnancy in patricia for all groups and dose categories ( range 53 [ 49% ] of 109 to 143 [ 66% ] of 216 women ) and in cvt for women who received two doses of vaccine ( 150 [ 36% ] of 419 women assigned to hpv vaccine ; 142 [ 37% ] of 379 assigned to control )  . 
for women who received one dose of vaccine in cvt , doses vaccine ecacy ( % ) figure 3 : vaccine e cacy for individual hpv types by dose , for incident hpv infections that were detected one time ( a ) , that persisted for more than 6 months ( b ) , and that persisted for more than 12 months ( c ) in the modi ed total vaccinated cohort 780 vol 16 july 2015 articles were missed mainly because of colposcopy referral ( range 40 [ 22% ] of 185 to 55 [ 29% ] of 192 women ) and the second most common reason for missed doses was pregnancy ( appendix )  . 
mean follow - up was similar between groups and dose categories in cvt and ( table 1 ) ; overall mean follow - up was patricia 476 months ( sd 88 )  . 
the number of non - vaccine study visits was balanced for all dose groups in cvt and for women who received one or two doses in patricia ; women who received three doses in patricia had on average one additional study visit , although mean visits for women who received three doses of vaccine in the hpv and control groups were balanced ( table 1 )  . 
for each study , hpv - 16 / 18 status at enrolment seemed balanced between groups within dose categories , although uctuations were present because of the small number of women in some categories . 
to further show balance in underlying hpv risk by dose group within the hpv and control groups during the 4 year follow - up , we assessed cumulative incident hpv infections for types that the vaccine does not protect against11 as composites of oncogenic and non - oncogenic hpv types . 
similar hpv attack rates were reported in this assessment in both patricia and cvt studies across and within all treatment groups ( one , two , or three vaccine doses ; appendix )  . in the patricia trial , vaccine e cacy against onetime detection of incident hpv - 16 / 18 infection for three doses was 768% ( 95% ci 742792 ) , two doses was 733% ( 404892 ) , and one dose was 722% ( 136924 ) , thereby con rming the original report from cvt of high vaccine e cacy against hpv - 16 / 18 irrespective of dose group . 
in this analysis , we identi ed no evidence for heterogeneity between studies in dose - strati ed vaccine e cacies against hpv - 16 / 18 ( appendix )  . in both trials combined , the analysis in the m - tvc cohort assessing hpv - 16 / 18 - related endpoints included ( for one - time detection ) 22 327 women who received three doses ( 11 110 hpv vs 11 217 control ) , 1185 women who received two doses ( 611 hpv vs 574 control ) , and 543 women who received one dose ( 292 hpv vs 251 control )  . 
this cohort excluded women with inadequate follow - up ( either the women had no visit at 12 months or later or women for whom there were fewer than 300 days between their 12 month or later visit and the last visit ; gure 1 )  . 
in the m - tvc , vaccine e cacy against one - time detection of incident hpv - 16 / 18 infections for three doses was 770% ( 95% ci 747791 ) , two doses was 760% ( 620853 ) , and one dose was 857% ( 707937 ; table 2 ) ; no signi cant di erence was present in vaccine e cacy by dose ( ptrend = 036 )  . 
study - speci c dose - strati ed vaccine e cacies were also similar ( minimum p value = 015 ) , indicating consistency of ( gure 2 ; appendix )  . 
vaccine e cacies for incident hpv - 16 alone and hpv - 18 alone were high irrespective of dose and endpoint ( gure 3 ; appendix )  . the ndings the tvc - naive cohort included 13 296 women who received three doses ( 6634 hpv vs 6662 control ) , 549 women who received two doses ( 273 hpv vs 276 control ) , and 238 women who received a single dose ( 138 hpv vs 100 control )  . 
in this cohort , vaccine e cacy for three doses against one - time detection of incident hpv - 16 / 18 infections was 814% ( 95% ci 787838 ) , for two doses was 812% ( 595923 ) , and for one dose was 875% ( 609971 ; table 3 )  . 
vaccine e cacy against one - time detection of incident hpv - 31 / 33 / 45 infections was 597% ( 95% ci 560630 ) for three doses , 377% ( 124559 ) for two doses , and 366% ( 54 to 622 ) for one dose ( table 4 )  . 
for the 6 month and 12 month persistent hpv - 31 / 33 / 45 infection endpoints , only the three - dose vaccine e cacy was statistically signi cant . 
for individual hpv types for which cross - protection has been reported , 10 vaccine e cacy was signi cant for three doses against hpv - 31 , hpv - 33 , and hpv - 45 , and for two doses for hpv - 31 and hpv - 45 ( appendix )  . there was an absence of heterogeneity in vaccine e cacy by study for all cohorts and endpoints ( minimum p = 015 ) in all analyses except one ( women who received two doses , tvc - naive analysis of hpv - 31 / 33 / 45 infections [ data not shown ] ; p = 0035 )  . in the patricia trial con rm , discussion in an findings independent randomised controlled trial , the original report from cvt that one and two doses of the hpv - 16 / 18 vaccine provide protection against cervical hpv - 16 / 18 infections similar to the protection provided by the three - dose schedule during 4 years of postvaccination follow - up , 6 and extend the ndings to e cacy against hpv types not included in the vaccine ( panel )  . 
further , in analyses combining data from the two trials , the result of high hpv - 16 / 18 vaccine e cacy irrespective of dose was replicated in a cohort of women naive to hpv - 16 / 18 infection at the time of vaccination , which alleviates concerns that the initial ndings might have been due to vaccination boosting of natural immunity in our cohort of older - aged women in cvt ( the original analysis did not have su cient power to create an hpv - naive cohort ) .6 thus , these results are probably relevant to girls in the preferred age range for hpv vaccination ( ie , 1112 years )  . results from cvt two doses of the hpv - 16 / 18 as04 - adjuvanted vaccine protected against a composite endpoint of hpv - 31 / 33 / 45 infection when the second dose was given 6 months after the initial vaccine . 
yet , on the basis of these new data , one dose or two priming doses separated by a short interval ( ie , 1 month ) might not be adequate to induce measurable cross protection . 
follow - up time was equivalent in all groups in both cvt and patricia , and risk of hpv acquisition in the control group was generally similar in the groups who had a similar number of study visits ( ie , all women who received one or two doses of control vaccine , and women in cvt who received three doses of control vaccine )  . 
finally , despite combining of data from two large trials , the number of women who received one dose was small , allowing for assessment of virological endpoints but not histological endpoints . 
most women received their second of only two doses 1 month after the rst , a schedule now recognised as inferior to two doses given 6 months apart.26 continued active surveillance of women who received fewer than three doses after the 4 year study period is essential to ensure long - term duration of protection . post - hoc analyses in two randomised controlled trials independently identi ed similar results for e cacy against cervical hpv - 16 / 18 infections , irrespective of the number of doses , during the 4 year study period . 
by combining summary - level data , we provide further support for the possibility that the bene t of vaccine e cacy against one - time detection of incident infection was our primary endpoint , rather than persistent infection or disease . 
results using this endpoint suggest that , within the limits of the pcr assay , the vaccine conferred sterilising immunity ( de ned as protection not only against clinical disease , but also infection ) for most hpv - 16 / 18 exposures , even for women who received one vaccine dose . 
immunogenicity data from cvt suggest that one - dose vaccination recipients had antibody titres between months 648 that were lower than those elicited with two or three doses , but the titres were stable and several times higher than those identi ed for natural immunity.20 we can now infer that these lower , vaccine - induced antibody titres provide as strong hpv prevention as the titres from two or three doses , at least in the short ter compared with persistent the limitation of including both short - term infection that regresses spontaneously in addition to persistent infections , which have a higher risk of progression to cervical lesions . 
furthermore , some outcomes might have resulted from undetected infections present before vaccination , which explains why e cacy estimates for this endpoint are generally lower than those for persistent infection . 
 additional analysis of e cacy and immuno genicity data from one - dose recipients might also aid in the identi cation of an immune correlate of protection , in view of the absence of e cacy reported against related hpv types ; analyses are being considered and will be the subject of a future report . infection , one - time detection has the priming dose.20 , 2224 furthermore , the structure of the hpv virus - like particles , the key component of hpv prophylactic vaccines , present closely spaced , repetitive epitopes to the immune system that induce highly potent , protective antibody responses , which might reduce or even eliminate the need for doses beyond the immune - stimulatory e ects of a toll - like receptor agonist adjuvant in the hpv - 16 / 18 vaccine might also contribute to the magnitude and durability of the immune response to this vaccine . 
if the protective e ect a orded by one dose is mainly due to the repetitive display of the virus - like particles , this result might be attained for the quadrivalent ( and nonavalent ; both merck ) hpv vaccines as well.25 alternatively , if the protective e ect is mainly due to the adjuvant used ( or di erences in manufacturing of the virus - like particles ) , strong vaccine e cacies in fewer doses could be unique to the hpv - 16 / 18 as04 - adjuvanted vaccine . our data for estimation of the e cacy of fewer than important three doses , summarised here , have limitations . 
the biggest concerns for this post - hoc , nonrandomised study are that women who received one dose of vaccine have the possibility of increasingly greater immune response , and lower risk of infection , which could introduce biases . 
in previously published work vol 16 july 2015 articles panel : research in context systematic review we searched the scienti c literature before this study and found that convincing immunogenicity data now exist that suggest that two doses of the hpv vaccine given to adolescents 6 months apart evokes an immune response similar to that of three doses , for at least 4 years . 
only one study published so far has assessed the e cacy of fewer than three doses of hpv vaccinethe costa rica vaccine trialin a post - hoc analysis nested in this randomised controlled trial . 
its ndings suggested that strong e cacy was provided by the hpv - 16 / 18 vaccine irrespective of the number of doses received . interpretation these new data show similar ndings of protection for 4 years irrespective of the number of doses received in the patricia trial . 
further , by combining the costa rica vaccine trial and patricia trial data , we provide new evidence suggesting that two and one doses of the hpv - 16 / 18 vaccine provide protection against cervical hpv - 16 / 18 infections , similar to the protection provided by the full three - dose schedule for 4 years after vaccination . 
these data strongly argue for a direct assessment of one - dose e cacy of the hpv - 16 / 18 vaccine . heterologous hpv types is retained with two doses given 6 months apart , but perhaps not with administration of one dose or two closely spaced , priming doses . 
because of the non - randomised nature of these analyses , the small sample size in the one - dose group , and the use of incident infection as the primary endpoint of this analysis , an endpoint not accepted by regulators as a surrogate for cervical cancer , policy is unlikely to change to recommend one dose of vaccine in response to this work . 
yet , these new data argue strongly for additional assessments of this question.27 long - term population - e ectiveness studies of girls vaccinated at young ages will be informative , but trials to directly investigate the vaccine e cacy of one dose will be necessary to motivate policy change . 
 if one - dose hpv vaccine administration provides strong protection against hpv - 16 / 18 for the long term , this approach might be what is necessary to overcome the barriers prohibiting vaccine uptake in many world regions . contributors ark , fs , mrdr - r , ah , srs , sw , smg , rh , m - pd , and cmw formed the manuscript core writing teaall authors , including group coauthors listed in the group below , have quali ed for authorship in adherence with the icmje guidelines and have reviewed and commented upon a draft , gave nal approval , and had nal responsibility for the decision to submit for publication . 
cmw received funding to conduct the clinical trial and reimbursement for travel from the gsk group of companies via university of new mexico , and reagents and equipment for hpv genotyping studies were provided to the university of new mexico by roche molecular systems . 
smg reports she was a member of the merck cervical cancer global advisory board , merck scienti c advisory board , and received fare and accommodation related to her participation , grants from the gsk group of companies paid via her institution to perform phase 3 trials of hpv vaccines , a researcher initiated grant from merck sharp & dohme to perform surveillance rrp in australia post - hpv vaccine , and a grant to her institution from csl bio for research on hpv and cancers . 
srs has received , via her institution , grants for clinical trials , travel reimbursements , and honoraria to attend advisory board meetings and to present at educational meetings from the gsk group of companies . 
fxb has received grants for clinical trials and speaker fees from merck sharp & dohme , sano pasteur msd , and the gsk group of companies , and grants from merck sharp & dohme and the gsk group of companies for educational presentations . 
xc has received grants from merck sharp & dohme , sano pasteur msd , and the gsk group of companies , and he has received nonnancial support from sano pasteur msd . 
drl reports that as a part of his us government supported research at the national cancer institute / national institute of health , he is the inventor of technology that underlies the l1 - based prophylactic virus - like particle ( vlp ) hpv vaccine and technology that underlies an l2 - based candidate prophylactic hpv vaccine . 
the nih has licensed the technology for the l1 vlp vaccine to merck , the manufacturer of gardasil , to the gsk group of companies , the manufacturer of cervarix , and indian immunologicals ltd . 
the l2based vaccine technology is the subject of a cooperative research and development agreement between the nci , john hopkins university , and shantha biotech , and has been licensed to shantha , panvax , acambis inc , and the gsk group of companies . 
bro has received grants for clinical trials from merck sharp & dohme and the gsk group of companies and support for travel to meetings for the study or other purposes and consulting fees / honoraria paid via the b romanowski corporation . 
the trial is sponsored and funded by the nci ( contract n01 - cp - 11005 ) , with funding support from the national institutes of health o ce of research on womens health . 
in the usa , we extend our appreciation to the team from information management services responsible for the development and maintenance of the data system used in the trial and who served as the data management centre for this e ort . 
we thank the members of the data and safety monitoring board charged with protecting the safety and interest of participants in our trial ( steve g self , adriana benavides , luis diego calzada , ruth karron , ritu nayar , and nancy roach ) and members of the external scienti c hpv working group who have contributed to the success of our e orts over the years ( joanna m cain , diane d davey , francisco fuster , ann gershon , elizabeth holly , silvia lara , henriette ravents , wasima rida , and luis rosero - bixby )  . 
we acknowledge the work of the central and local study coordinators and sta members of the sites that participated in this study . editorial published online november 28 , 2014 s1470 - 2045 ( 14 ) 71139 - 8 for the medical innovation bill see uk / bills / 2014 - 15 / medicalinnovation.html for the bills second reading in the house of lords see uk / pa / ld201415 / ldhansrd / text / 140627 - 0001 . htm#14062743000565 undermining the hippocratic oath : the medical innovation bill on nov 13 , 2014 , 100 prominent uk oncologists signed a letter to the times stating they neither want nor need the medical innovation bill tabled by lord saatchian unelected individual with no professional medical or scienti c trainingthat is currently making its way through the house of lords . 
as de ned by the bill , acting responsibly includes having obtain [ ed ] the views of one or more appropriately quali ed doctors in relation to the proposed treatment , and taking full account of these views as any responsible doctor would . 
a doctor may only depart from accepted medical treatment if it is with the patients consent , and certainly not for the purposes of research , or for any purpose other than the best interests of the patient . 
its proponents argue that , by allowing doctors to depart from conventional medical treatment without fear of litigation and outside of clinical trials , patients lives could be saved by use of innovative medical practice . 
many oncology drugs are used o - label ( especially towards the end of life ) , and equally , many medicines are only approved for adults and must be used o - label for children . 
while terminal , rare cancers are the medical condition most frequently invoked by the bills proponents , there is no clause stipulating that patients need be untreatable by accepted medicine , nor that they be terminally ill . 
thus , the bill might allow a doctor to depart from accepted practice for no reason other than that he or she , and at least one colleague , does not accept it as best . 
as baroness masham noted in the bills second reading , this legislation would a ect all forms of medical treatment , not only in exceptional circumstances...when all evidence - based treatment options have been exhausted , opening the door to the use of less proven , or unproven , approaches such as complementary or alternative medicine . 
however , provision of these agents on a desperate whim , in an unmonitored environment , could lead to patient har for example , the maximum tolerated dose may be unknown , leading to the dose being subtherapeutic or causing unexpected adverse events . 
even if the drug had advanced to later testing , but is not yet licensed , pharmaceutical companies would be required to disclose data about toxicities to national licensing agencies only . 
not only would this cause otherwise preventable harm to patients ( clearly at odds with the founding tenet of medicine to do no harm ) , but could cause immeasurable psychological pain for doctors who believed they were providing the best care for their patients . 
saatchi and colleagues have often quoted sir austin bradford hill , pioneer of the randomised trial , who wrote that any belief that the control trial is the only way [ to study therapeutic e cacy ] would mean not only the pendulum had swung too far , but that it had come right o its hook . 
in attacking the signatories of the times letter as complacent and self - satis ed in his commentary in the guardian on nov 14 , 2014 , saatchi gave in to precisely the type of emotional response that evidence - based practice seeks to avoid . 
we are all human ; evidence - based medicine provides safeguards against paternalistic , impetuous decisions that may be made with the best of intentions , but without due diligence . 
 the lancet oncology vol 16 january 2015 and advisory board and consulting fees from eli lilly ; has received personal fees and held stock as a member of advisory board from seragon ; has received reimbursement for travel and in - kind items and services from roche , outside the submitted work . 
 s - ai reports grant support from astrazeneca and advisory consultant roles for astrazeneca , eisai , novartis , pfizer , roche / genentech and spectrum , outside the submitted work . 
hi reports grant support and personal fees from novartis during the conduct of the study ; hi was also an uncompensated member of the steering committee of this study ; hi has received personal fees in the form of honoraria and consulting fees from astrazeneca , pfizer , lilly , daiichi - sankyo , and f hoffman la - roche via chugai , outside the submitted work . 
jc reports personal fees from novartis , celgene , cellestia , astrazeneca , biothera pharmaceuticals , merus , seattle genetics , daiichi sankyo , erytech , pfizer , eisai , and samsung ; has received stock , patents , and intellectual property from medsir ; has received personal fees and research funding to his institution from roche , outside the submitted work . 
mdls reports personal fees in the form of speakers honoraria and advisory board honoraria from novartis , roche , lilly , pfizer , eisai , ipsen , and teva , outside the submitted work . 
cla reports personal fees for participation in a steering committee for the clinical trial from novartis , during the conduct of the study ; and personal fees for an expert advisory role from eli lilly , astrazeneca , genentech , millennium , celgene , pfizer , radius , and merck , outside the submitted work . 
sc also reports personal fees received in the form of honoraria for advisory boards from novartis , hoffmann laroche , pfizer , astrazeneca , and genomic health ; and institutional research support from novartis , hoffmann laroche , pfizer , astrazeneca , genomic health , genentech , merck , and bms , outside the submitted work . 
she also reports grant support from ambryx , amgen , bayer , obi pharma , bimarin , cascadian , daiichi sankyo , dignitana , genentech , gsk , lilly , macrogenics , medivation , merrimack , novartis , pfizer , pieris , puma , roche , seattle genetics , and travel support from lilly , novartis , and obi pharma , outside the submitted work . 
 reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
pv reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 15964 wolf a , naylor k , tam m , et al . 
these corrections have been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 17980 massari f , di nunno v . 
lancet oncol 2019 ; 20 ; 17980in this comment , the following sentence has been edited from time to deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab to risk of deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab . 
 this correction has been made to the online version as of feb 1 , 2019 , and the printed version is correct . vol 20 february 2019 corrections for more on the prosper trial see org / record / 157683 / abstract for more on the spartan trial see n engl j med 2018 ; published online feb 8 . 
depending on the stage of disease at diagnosis , prostate cancer can be managed with combinations of active surveillance , surgery , radiotherapy , and androgendeprivation therapy ( adt )  . 
however , some men have aggressive disease , in which rising concentrations of prostate - specific antigen ( psa ) herald biochemical relapse and metastatic disease , even after treatment . 
currently , is available for these men ; no standard treatment however , promising new data from two trials presented at the 2018 asco genitourinary cancers symposium ( feb 810 , 2018 , san francisco , ca , usa ) suggest that this situation might be about to change . 
 the two trials prosper and spartan both treated men with early - stage , castration - resistant m0 disease who were unsuitable for curative treatment , and who were being treated with adt , but continued to have rapidly increasing psa concentrations . 
in spartan , men receiving apalutamide had a median mfs of 405 months compared with 162 months for those receiving placebo ( hazard ratio [ hr ] 028 ; 95% ci 023035 ; p < 0001 )  . 
similarly , in prosper , men receiving enzalutamide had a median mfs of 366 months compared with 147 months with placebo ( hr 029 ; 95% ci 024035 )  . 
apalutamide was subsequently approved by the us food and drug administration on feb 14 , 2018 , under priority review for non - metastatic , castration - resistant prostate cancer on the basis of spartans findingsthe first drug to be approved for this patient population . 
for example , in 20 - year follow - up data from the pivot trial for men diagnosed localised prostate cancer , no significant with early difference was found in either all - cause or prostatecancer specific mortality when comparing men treated with either surgery or observation alone , but men in the surgery group had worse functional outcomes from surgery ( eg , incontinence , erectile dysfunction ) for up to 5 years after treatment . 
 given these outcomes , the impetus for early detection and thus early management of prostate cancer important , making recent news of faster prostate cancer diagnosis in the uk welcome . 
diagnosis in the uk typically requires multiple hospital visits to obtain scans and biopsies ; however , three london hospitals are trialling whether or not patients can be diagnosed within a day . 
 this faster approach hinges on the use of multiparametric mri scans instead of transrectal ultrasound - guided biopsy , allowing all diagnoses to be done through imaging , which is both faster and non - invasive . 
about 5000 men will be tested for prostate cancer at these hospitals over the next 2 years , before a decision can be made as to whether the new system should be rolled out nationally . 
second , it is important to be aware that despite such advances as increased time to distant metastases , the endpoint used in the latest trials do not necessarily also indicate increased survival . 
 for example , in spartan the median time to overall survivala prespecified , albeit unpowered endpointdid not differ significantly between the groups ; comparable data are still awaited for prosper . 
the authors provide the foundation necessary for a call to action for clinicians , policy makers , and researchers focused on reducing the substantial burden that cancer afflicts upon young adults . 
 unfortunately , even in very high - hdi regions , cervical cancer remains one of the top five causes of cancer death in young adults , highlighting the failures of our current policies and approaches . 
 other than cervical cancer , few cases of cancer in young adults can be effectively detected with screening ; one exception being breast cancer screening among women with a known cancer - causing genetic mutation . 
this highlights the importance of primary care providers taking a thorough family history and promptly referring to genetic counselling , as well as potentially testing when appropriate , such that targeted screening regimens for identified cancer predisposition syndromes are initiated appropriately . 
to reduce the incidence of kaposis sarcoma and liver cancer , particularly in africa and parts of asia , there needs to be continued focus on the prevention of hiv and hepatitis c virus ( hcv ) transmission . 
to date , in developing regions of the world , health education around condom use and safer sexual practices , has resulted in reducing the number of new hiv infections . 
 improvements in cure rates for young adults with cancer have lagged behind younger children and older adults.2 many explanations are possible for these worse outcomes , including a smaller proportion of young adult patients on clinical trials , delays in diagnosis , and biological differences in cancers between those in young adults and adults . 
for example , stock and colleagues3 compared the outcomes of young adults treated on paediatric and adult clinical trials for acute lymphoblastic leukaemia ( all ) and noted superior outcomes among those treated on paediatric trials . 
a concerted effort to examine the biology of other 1554 vol 18 december 2017 comment cancers in young adults and to do focused clinical trials among this age group is warranted to improve the outcomes of these patients . 
 lifelong tara o henderson , * kevin c oeffinger department of pediatrics , university of chicago , chicago , il , usa ( toh ) ; and department of medicine , duke university , durham , nc 27705 , usa ( koc ) kevin.oeffinger@duke.edu we declare no competing interests . the author ( s )  . 
what determines the outcomes for adolescents and young adults with acute lymphoblastic leukemia treated on cooperative group protocols ? a comparison of childrens cancer group and cancer and leukemia group b studies . 
crizotinib was approved as frontline therapy based on results showing longer progression - free survival ( 109 months [ 95% ci 83139 ] ) than that seen with platinum - based chemotherapy ( 70 months [ 95% ci 6882 ] ; hazard ratio [ hr ] for progression or death 045 , 95% ci 035060 ; p < 0001 ) .2 however , crizotinib has poor cns penetration , and the cns is the most common site of disease progression in alk - positive patients.3 alectinib has gained favour as frontline therapy after publication of the results of the alex3 and j - alex4 trials in 2017 , which assessed alectinib versus crizotinib treatment in tki - naive patients . 
in alex , 3 median progression - free survival was significantly longer with alectinib than crizotinib ( not reached vs 111 months ; hr 047 , 95% ci 034065 ; p < 00001 )  . 
cns progression was observed more frequently in patients treated with crizotinib ( 12 - month incidence of 414% [ 95% ci 332494 ] ) than alectinib ( 94% [ 54147 ] )  . 
ceritinib has also been shown to confer longer progression - free survival than chemotherapy in the frontline setting , although 78% of patients had grade 3 or 4 toxicity.5 the choice of second - line therapy and beyond is based on previous treatment exposure , presence of an alk resistance mutation , and the tki side - effect profile . 
ceritinib , alectinib , and brigatinib have resulted in progression - free survival of 54 , 6 81 , 7 and 1291 months , respectively , in patients previously treated with crizotinib . 
for patients with measurable cns disease at baseline , intracranial overall responses were achieved by 12 ( 75% ) of 16 patients treated with alectinib7 and 12 ( 67% ) of 18 patients treated with brigatinib.1 notably , responses to ceritinib have been seen in patients with and without resistance mutations.6 however , ceritinib has notable toxicity , including causing increased trans aminases , diarrhoea , nausea , vomiting , and fatigue , which often result in dose reductions . 
 in this clinical context , alice shaw and colleagues8 lorlatinib , report a phase 1 , multicentre study of published online october 23 , 2017 s1470 - 2045 ( 17 ) 30708 - 8 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on november 29 , 2017 see articles page 1590 vol 18 december 2017 1555 comment the results of this study3 support the benefit of lenalidomide maintenance across different subgroups of patients and highlights the progression - free survival benefit in patients with high - risk cytogenetic abnormalities . 
however , it is important to note that lenalidomide did not overcome the poor prognosis that the presence of high - risk abnormalities confer to patients , and therefore novel treatments to improve the outcomes of these patients are needed . whether all patients need continuous maintenance therapy regardless of the quality of the response achieved with previous treatments remains unclear . 
however , next - generation sequencing and cytometry provide an opportunity to investigate the role of minimal residual disease assessment for tailoring maintenance strategies and would allow physicians to prescribe maintenance therapy and reply to a very common question raised by the patients : how many cycles of treatment does maintenance therapy include ? furthermore , long - term minimal residual disease monitoring could guide preemptive treatment preventing clinical relapses and ensuring durable responses . maintenance with lenalidomide is the standard of care , but the future has to move towards a personalised medicine approach that aims to improve overall survival and quality of life , which means giving the right drug to the right patient at the right time for the optimal duration . * mara - victoria mateos , vernica gonzlez de la calle hematology department , university hospital of salamanca , ibsal , salamanca , spain mvmateos@usal.es m - vm has received honoraria for lectures from janssen , celgene , takeda , and amgen , and for participation in advisory boards from janssen , celgene , takeda , amgen , abbvie , glaxosmithkilne , and pharmamar . 
n engl j med 2018 ; 378 : 51828 . the importance of surgery in colorectal cancer treatment in the lancet oncology , sara benitez majano and colleagues1 have engaged with a very important topic . 
 previous data have indicated poorer treatment results for colorectal cancer in both denmark and england compared with those in similar western countries.2 the continuous audit and assessment of outcomes is important to better understand the reality of cancer care each country and thus , this study is of interest to the public . majano and colleagues identified that an important difference between the countries studied regarding surgery for colorectal cancer was probably not the technique , but rather the frequency of surgical resection . 
 the proportion of patients treated with resectional surgery ranged from 684% in england to 813% in sweden for colon cancer , and from 599% in england to 708% in sweden for rectal cancer ; this range was wider for patients older than 75 years ( colon cancer 597% to 809% ; rectal cancer 457% to 619% )  . 
it is possible that attitudes towards surgery in the older patient population should be altered in england , but the data in this study do not include comorbidity , and the risk for increased perioperative mortality should not be underestimated . 
 preoperative optimisation of patients must be a focus of research , to increase the percentage of patients that are able to undergo resectional surgery in the future . what other factors could be influencing these results ? during the study period , the standardised referral pathway had already been introduced in denmark in 2010 . 
there is scarce vol 20 january 2019 published online december 10 , 2018 s1470 - 2045 ( 18 ) 30679 - x see articles page 74 comment scientific evidence that a standardised referral pathway improves survival . introduced another preoperative difference between the countries studied was colorectal cancer screening . 
perhaps the effect of screening was seen in rectal cancer , where diagnoses of stage i to iii disease were more common in england than in the other countries , but , unfortunately , this effect was not reflected in improved survival . benitez majano and colleagues study shows that the previously reported2 poorer treatment results for denmark than those for norway and sweden have improved , particularly for rectal cancer . 
perhaps this change is due to the increased use of surgical resections for rectal cancer , but the authors also suggest that improved results could be partly attributed to laparoscopic surgery , which has been shown to be safe in the long term and confers short - term advantages in the management of colorectal cancer.35 during the study period , laparoscopic surgery for rectal cancer was very differently implemented countries , with denmark having 75% of patients operated with laparoscopic technique compared with about 20% of patients in sweden , according to national quality registry data . 
taken all together , it is unlikely that laparoscopic surgery is the main reason for the improved survival in patients with rectal cancer in denmark shown in this study . four the another surgical difference that was less emphasised in guidelines in england than in recommendations from the other countries in this study was complete mesocolic excision . 
in stockholm , where the technique has been introduced in a structured manner , only about 20% of patients undergoing surgery for colon cancer between 2004 and 2012 had complete mesocolic excision.8 similar data have been published from denmark.9 nonetheless , it is interesting that recommendations for england are less specific than other countries guidelines ; does this in fact result in poorer survival because of unspecified surgical treatment ? future research must focus on including data on patient frailty and comorbidity , which should be added to registry data , as majano and colleagues have suggested . 
 the facilitation of easier interpretation and comparison of data from several national registries must also be a concern for policy makers , because benchmarking of results and making comparisons between countries might help to identify important new areas to improve survival in patients with colorectal cancer . eva angenete department of surgery , institute of clinical sciences , sahlgrenska academy at university of gothenburg , sahlgrenska university hospital / stra , scandinavian surgical outcomes research group , 413 45 gothenburg , sweden eva.angenete@vgregion.se i declare no competing interests . copyright 2018 the author ( s )  . 
lancet oncol 2015 ; 16 : 16168 . vol 20 january 2019 comment correction to lancet oncol 2018 ; 19 : e10212 sundar s , khetrapal - singh p , frampton j , et al . 
 lancet oncol 2018 ; 19 : e10212in this series paper , in the section titled challenges from womens cancer in india , the second sentence of the second paragraph should read despite this initiative , large - scale implementation of cancer prevention and control strategies has yet to take place , and public expenditure on health remains low at 12% of indias gross domestic product . 
this correction has been made to the online version as of may 31 , 2018 . correction to lancet oncol 2018 ; 19 : 72829 correction to lancet oncol 2018 ; 19 : 54961 iarc monographs vol 121 group . 
lancet oncol 2018 ; 19 : 54961in figure 3 of this article ( published online first on feb 20 , 2018 ) , the heatmap in panel a has been replaced to amend display errors . 
this correction has been made to the online version as of may 31 , 2018 . vol 19 june 2018 e283 corrections correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections articles lancet oncol 2015 ; 16 : 112332 published online july 21 , 2015 s1470 - 2045 ( 15 ) 00128 - x this online publication has been corrected . 
 the results of the uk age trial , which compared the e ect of invitation to annual mammographic screening from age 40 years with commencement of screening at age 50 years on breast cancer mortality , have been reported at 10 years of follow - up and showed no signi cant di erence in mortality between the trial groups . 
the primary outcome measures were mortality from breast cancer ( de ned as deaths with breast cancer coded as the underlying cause of death ) and breast cancer incidence , including in - situ , invasive , and total incidence . 
this trial is registered , number isrctn24647151 . findings between oct 14 , 1990 , and sept 25 , 1997 , 160 921 participants were randomly assigned ; 53 883 women in the intervention group and 106 953 assigned to usual medical care were included in this analysis . 
after a median followup of 17 years ( iqr 168188 ) , the rate ratio ( rr ) for breast cancer mortality was 088 ( 95% ci 074104 ) from tumours diagnosed during the intervention phase . 
a signi cant reduction in breast cancer mortality was noted in the intervention group compared with the control group in the rst 10 years after diagnosis ( rr 075 , 058097 ) but not thereafter ( rr 102 , 080130 ) from tumours diagnosed during the intervention phase . 
the overall breast cancer incidence during 17 year follow - up was similar between the intervention group and the control group ( rr 098 , 093104 )  . interpretation our results support an early reduction in mortality from breast cancer with annual mammography screening in women aged 4049 years . 
past funding was received from the medical research council , cancer research uk , the uk department of health , and the us national cancer institute . introduction population - based screening for breast cancer by mammography is well established in many countries , although the target age range for invitation varies and the appropriate age range at which to invite women for screening continues to be an area of debate . 
although some service screening programmes begin o ering screening at age 40 or 45 years , 1 most begin o ering it from age 50 years.1 in england , the lower age limit for invitation is being reduced to 47 years , which means that when this extension is complete , all women will receive their rst invitation before the age of 50 years . 
this change is being made with an experimental design that will allow assessment of its e ect in the service screening environment , 2 but the results will not be available for many years . a recent review3 by the international agency for research on cancer concluded that there was limited evidence for the e cacy of screening women aged 4049 years by mammography . 
however , it has been argued that evidence4 from randomised controlled trials does not provide a strong basis for determining the e ectiveness of mammography in women in their 40s compared with that in older women , and evidence5 , 6 from service screening programmes supports a more optimistic view of the bene ts of mammography in women aged 4049 years . 
although most us organisations recommend annual mammography for vol 16 september 2015 1123 articles see online for appendix research in context evidence before this study several previous randomised trials of mammographic screening included women aged younger than 50 years . 
a meta - analysis including these studies done for the us preventive services task force ( uspstf ) , published in 2009 , identi ed a relative risk reduction in breast cancer mortality of 15% in women , aged 3949 at randomisation , invited for screening , similar to that for older women , but a lower absolute reduction and greater number needed to invite . 
this meta - analysis included the rst mortality results of the uk age trial , and also the results of the canadian trial ( nbss - 1 ) , the only other trial designed to study women younger than 50 years . 
a cochrane review published in 2013 identi ed a 13% reduction in mortality in an analysis of only three of the eight trials included in the uspstf meta - analysis , and a 16% reduction including all eight trials at 13 years of follow - up . 
 evidence from some service screening programmes supports a bene t of mammography in women younger than 50 years . estimates of overdiagnosis as a result of mammographic screening vary widely , largely because of di erences in the methods used . 
as a result , little reliable evidence exists about the extent of overdiagnosis in this age group . added value of this study the uk age trial is the only trial designed speci cally to study the e ect of mammographic screening starting at age 40 years . 
 this study reports breast cancer mortality and incidence at a median of 177 years of follow - up , an increase of 7 years from the previous publication . implications of all the available evidence the evidence supports a reduction in breast cancer mortality as a result of mammographic screening in women younger than 50 years at least in the rst 10 years of follow - up . 
 women in their 40s , in 2009 , the us preventive services task force ( uspstf ) revised its 2002 recommendations that women in their 40s should undergo mammography screening every 12 years , and now recommends against routine screening mammography for women in this age group based mainly on what it judged to be an uncertain balance of bene ts and harms.7 its systematic review8 noted that although the relative risk reductions in women aged 5059 years ( 14% ) and 4049 years ( 15% ) were similar , the absolute risk reduction was greater for women aged 5059 years than for those aged 4049 years , leading to a number needed to invite to screening of 1339 compared with 1904 for the younger age group . included to determine the uspstf meta - analysis7 the rst mortality results from the uk age trial , 9 which were based on breast cancer mortality at a mean of 107 years ( sd 16 ) of follow - up and showed a non - signi cant reduction in women invited to screening ( relative risk 083 , 95% ci 066104 ) , with an absolute risk reduction of 040 per 1000 women invited , equivalent to a number needed to invite of 2512 . 
the uk age trial was a randomised screening trial established in the e ectiveness of annual 1991 mammographic screening commencing at age 40 years compared with the uk national policy at the time , which was to commence from age 50 years . 
the uk age trial is unique in that it included women aged trial of 3941 years at entry and mammography speci cally designed to study the e ectiveness of commencing screening at age 40 years . 
the uninvited control group were unaware of their inclusion in the trial , which was deemed acceptable because this is no di erent to a geographically distinct population that are followed up to monitor cancer and mortality and who are receiving the usual standard of care . 
ethical approval for this study was obtained from london central research ethics committee . informed consent taken randomisation and masking individuals in the uk age trial were randomly assigned ( 1 : 2 ) to either the intervention group or the control group . 
before this , for women in three early centres to join the trial , random numbers generated from the coordinating centre computer were applied to gp lists generated from the health authority . 
 procedures women in the intervention group were invited for screening by the centres up to and including the calendar year of their 48th birthday , although screening ceased 1124 vol 16 september 2015 articles early in three centres because of insu cient resources . 
 women in both groups of the trial became eligible for their rst invitation to screening as part of the nhsbsp between the ages of 50 and 52 years , with invitations every 3 years thereafter . 
additionally , data were obtained from all nhsbsp screening units for the rst nhsbsp invitations for women in the trial , including data for women who had moved outside the trial areas . all women in the trial were followed up through the nhs central register ( nhscr ) to establish breast cancer incidence and mortality , mortality from all causes , and information about emigration . outcomes the primary outcome measures were mortality from breast cancer ( de ned as deaths with breast cancer coded as the underlying cause of death on the death certi cate ) , and breast cancer incidence , including in situ , invasive , and total incidence . 
 statistical analysis we originally designed the trial to recruit 190 000 women to have 80% power to detect a 20% reduction in breast cancer mortality at 10 years of follow - up at the 5% signi cance level . 
later estimates based on a lower expected mortality rate in the control group identi ed a power of 90% to detect a 20% reduction over 14 years.10 the present analysis was based on follow - up to dec 31 , 2011 . the primary analysis compared breast cancer incidence and breast cancer mortality between groups using poisson regression . 
we calculated cumulative hazards using the nelson - aalen method.11 the primary analysis was based on an intent - to - treat principle and included all women assigned to randomised groups who could be traced by the nhscr and who had not died or emigrated before entry . 
we compared all - cause mortality between groups to check randomisation . with increasing time after the end of screening in the trial , the reported e ect on breast cancer mortality will be diluted by the inclusion of breast cancers diagnosed after the end of screening , 12 including those detected by screening from age 50 years in the nhsbsp . 
the primary analysis was therefore restricted to breast cancer deaths in women with breast cancer diagnosed during the intervention phase , during which the intervention group was invited to screening and the control group was not , de ned as the period up to but not including the date of rst nhsbsp invitation . 
breast cancer deaths in women with a date of breast cancer diagnosis before their date of entry to the trial were excluded from the analysis . we did further prespeci ed analyses by period from randomisation , analyses of breast cancer deaths speci c to all periods of diagnosis , and an analysis including all breast cancer deaths irrespective of date of diagnosis . 
we also did a secondary analysis to estimate the e ect of screening in women who accepted their rst invitation , which approximates a per - protocol analysis , with the assumption that the underlying breast cancer mortality in acceptors is equivalent to that in the control group adjusted for the rate in the non - acceptors.13 cumulative breast cancer incidence was analysed for all follow - up and for cancers diagnosed up to the date of rst nhsbsp invitation . 
for women for whom no date of rst nhsbsp invitation was available , we estimated this as the date at which they attained the average age of women at this invitation ( 5103 years [ sd 097 ] )  . 
analyses were done both excluding and including cancers diagnosed at the rst 160 921 women aged 3941 identied from health authorities and randomised ( after checking of pnls ) 53 914 assigned to intervention group ( invited for screening from age 40 years ) 107 007 assigned to control group invited for screening in nhsbsp from age 50 years invited for screening in nhsbsp from age 50 years 31 excluded from analysis 8 not traced by the nhscr 10 deceased before entry 7 emigrated before entry 6 men 54 excluded from analysis 8 not traced by the nhscr 19 deceased before entry 15 emigrated before entry 12 men 53 883 assessed for primary outcome at 10 years 106 953 assessed for primary outcome at 10 years 650 lost to follow - up because of emigration 1183 lost to follow - up because of emigration 53 883 assessed for primary outcome at 17 years 106 953 assessed for primary outcome at 17 years figure 1 : trial pro le pnl = prior noti cation list . 
nhscr = national health service central register . vol 16 september 2015 1125 articles number of women 010 years after randomisation more than 10 years after randomisation womenyears * breast cancer deaths rate per 1000 women - years rate ratio ( 95% ci ) absolute risk reduction per 1000 women ( 95% ci ) womenyears breast cancer deaths rate per 1000 women - years rate ratio ( 95% ci ) absolute risk reduction per 1000 women ( 95% ci ) intervention 53 883 532 747 0156 075 ( 058 to 097 ) 051 ( 008 to 094 ) 408 221 0243 102 ( 080 to 130 ) 003 ( 047 to 041 ) control 106 953 1 058 322 0207 810 395 0238 * calculated from date of randomisation to 10 years after randomisation or end of follow - up , whichever was earliest ; median follow - up of 100 years ( iqr 99100 )  . 
median follow - up of 77 years ( iqr 6989 )  . table 1 : mortality from breast cancers diagnosed during the intervention phase by time since randomisation number of women womenyears * all - cause deaths breast cancer deaths rate per 1000 women - years rate ratio ( 95% ci ) rate per 1000 women - years rate ratio ( 95% ci ) absolute risk reduction per 1000 women ( 95% ci ) intervention 53 883 940 969 2127 226 098 ( 093 to 103 ) 0193 088 ( 074 to 104 ) 047 ( 014 to 109 ) control 106 953 1 868 717 4320 231 0220 rate ratio and absolute risk reduction are for intervention versus control group . * calculated from date of randomisation to end of follow - up ; median follow - up of 177 years ( iqr 168185 )  . 
 table 2 : mortality from all causes and from breast cancer in the intervention and control groups for a 17 year follow - up control group intervention group number at risk control intervention 106 953 53 883 105 864 53 267 years in trial 104 537 52 657 102 678 51 734 5439 2650 figure 2 : nelson - aalen estimate of cumulative breast cancer mortality ( restricted to deaths from breast cancers diagnosed in the intervention phase ) nhsbsp screen ( de ned as cancers recorded as screendetected on the screening centre system , 95% of which occurred within 6 months of the date of screen )  . women - years for analyses of mortality were calculated from date of trial entry to dec 31 , 2011 , or to death or loss to follow - up because of emigration , whichever was earliest . 
 this study is registered , number isrctn24647151 . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results between oct 14 , 1990 , and sept 24 , 1997 , 160 921 women were randomly assigned to the intervention and control groups . 
more than 999% of women were successfully identi ed by the nhscr ; 85 women ( 31 in the intervention group and 54 in the control group ) were excluded from the analysis because they either could not be traced by the nhscr , they had died or emigrated before entry , or were mistakenly identi ed men ( gure 1 )  . 
 four women have been identi ed as having emigrated or died before date of entry since our previous analysis.9 1833 women ( 650 in the intervention group and 1183 in the control group ) were follow - up after randomisation because of emigration . 
3944 ( 3% ) women received their rst nhsbsp invitation after the age of 52 years ( 1245 in the intervention group and 2699 in the control group )  . 
for 11 728 ( 7% ) women , no date of rst nhsbsp lost 1126 vol 16 september 2015 articles intervention control rate ratio ( 95% ci ) absolute reduction per 1000 women - years ( 95% ci ) absolute risk reduction per 1000 women ( 95% ci ) rate per 1000 women - years womenyears rate per 1000 women - years womenyears * 267 864 264 884 261 163 04 years 59 years 1014 years more than 15 years 147 057 total 940 969 0257 010 021 038 041 532 104 526 220 518 223 292 170 1 868 717 013 029 036 037 0276 078 ( 050 to 121 ) 003 ( 002 to 008 ) 014 ( 010 to 039 ) 073 ( 054 to 099 ) 008 ( 0006 to 015 ) 038 ( 003 to 074 ) 105 ( 082 to 134 ) 002 ( 011 to 007 ) 009 ( 054 to 036 ) 111 ( 081 to 152 ) 004 ( 017 to 008 ) 012 ( 047 to 024 ) 093 ( 080 to 109 ) 002 ( 002 to 006 ) 032 ( 038 to 102 ) rate ratio and absolute risk reduction are for intervention versus control group . 
 * women - years in each time period from randomisation . table 3 : breast cancer mortality by period in trial invitation was available ( 4115 in the intervention group and 7613 in the control group )  . of the women randomly assigned to the intervention group , 36 622 ( 68% ) of 53 883 were screened at the prevalent screen ; the mean number of routine screens attended was 48 ( sd 33 )  . 
overall 43 709 ( 81% ) women in the intervention group attended at least one routine screen.14 594 breast cancer deaths occurred from 2684 tumours diagnosed during the intervention phase . 
a signi cant reduction in breast cancer mortality occurred in the rst 10 year period ( rate ratio [ rr ] 075 , 95% ci 058097 ) restricted to deaths in cancers diagnosed in the intervention phase , but not thereafter ( rr 102 , 080130 )  . 
the absolute mortality reduction in the intervention group was 003 per 1000 women - years or 047 per 1000 women , equivalent to a number needed to invite of 2108 , or number needed to screen of 1366 ( based on the average uptake of 65%14 )  . 
figure 2 shows cumulative breast cancer mortality for this analysis estimated by the nelson - aalen method . there were 5761 breast cancer diagnoses ( invasive and in situ ) and 757 breast cancer deaths from cancers diagnosed at any time during follow - up . 
during the rst 10 years after randomisation ( when all but two deaths were from cancers diagnosed intervention phase ) , a the signi cant mortality reduction was noted ( rr 075 [ 95% ci 058096 ] ) , and attenuated with longer followup , similar to that seen in table 1 . including all follow - up , breast cancer mortality per 1000 women - years was 0257 ( 242 of 940 969 ) in the intervention group and 0276 ( 515 of 1 868 717 ) in the control group intervention group number at risk control intervention 106 953 53 883 105 864 53 267 years in trial 104 537 52 657 102 678 51 734 5439 2650 figure 3 : nelson - aalen estimate of cumulative breast cancer mortality ( all dates of diagnosis ) control group giving an rr of 093 ( 080109 )  . 
figure 3 shows a graph of the cumulative breast cancer mortality estimated by the nelson - aalen method . in the rst 10 years of follow - up , breast cancer mortality for women attending their rst round screen was reduced compared with the control group ( rr 064 [ 95% ci 045094 ] )  . 
 figure 4 shows the rr in the intervention group for breast cancer mortality , restricted to deaths in cases diagnosed within di erent number of years from randomisation ; the rr reaches a minimum of 082 ( 95% ci 065102 ) when restricted to deaths in cases diagnosed in the rst 7 years . 
we also did analyses in which deaths from breast cancer were restricted to those in cases diagnosed within 12 , 24 , and 36 months of date of last invitation ( and before rst nhsbsp screen ) , to allow for varying estimates of lead time . 
for women in the control vol 16 september 2015 1127 number of women women years all cause deaths breast cancer deaths rate per 1000 womenyears rate per 1000 womenyears rate ratio ( 95% ci ) attenders versus control group * breast cancer deaths restricted to cancers diagnosed in the intervention phase attenders for screening 36 540 642 865 1130 17 343 298 104 083 ( 065106 ) 176 334 019 020 non - attenders for screening breast cancer deaths restricted to cancer diagnosed in the intervention phase , censored at 10 years of follow - up attenders non - attenders 36 540 17 343 362 952 169 796 114 250 014 020 064 ( 045094 ) * adjusted for rate in those who did not attend screening in the intervention group . 
 table 4 : all cause and breast cancer mortality in attenders and non - attenders at rst screen in the intervention group 95% ci articles upper limit of years of diagnosis included figure 4 : rate ratio of breast cancer mortality in the intervention group , according to period of diagnosis of breast cancer group , the date used was based on the date of last invitation of the participant in the intervention group closest to the same age within the same screening centre . 
the absolute di erences for in - situ and invasive cancer ( table 5 ) are equivalent to an additional 025 in - situ cancers and 093 fewer invasive breast cancers per 1000 women invited for screening . 
for breast cancers diagnosed up to but excluding the rst nhsbsp invitation , a signi cant increase was noted in both in - situ and overall incidence , equivalent to 123 and 028 additional cancers per 1000 women invited ; however , with inclusion of breast cancers diagnosed at the rst nhsbsp screen , only the increase in in - situ disease remained signi cant ( table 5 )  . of those cancers in the intervention group diagnosed in the intervention phase , 171 ( 42% ) of 406 grade 1 and 2 cancers were screen - detected compared with 76 ( 23% ) of 330 grade 3 cancers . discussion the long - term results from the uk age trial presented here show a signi cant reduction in the risk of breast cancer mortality in the intervention group compared with the control group in the rst 10 years , followed by no di erence between the groups thereafter , when analysis was restricted to breast cancers diagnosed during the intervention phase . 
the absolute e ect of mammographic screening in this age group is di cult to assess when we include deaths from cancers diagnosed after the intervention phase of the trial , when both groups are receiving the same care , and at ages older than 50 years , when underlying incidence and mortality are substantially increased . the overall rr was 088 ( 95% ci 074104 ) during a median of 17 years of follow - up and was not signi cant . 
 previous results of this trial showed a non - signi cant rr of 083 ( 066104 ) for breast cancer mortality in the intervention group compared with the control group at a mean of 107 years ( sd 16 ) of follow - up.9 the reported di erence in breast cancer mortality peaked when the analysis was restricted to breast cancers diagnosed up to 7 years of follow - up , despite the fact that at this point in time , there was an excess of breast cancer incidence in the intervention group , which would tend to introduce a bias against screening as some of this excess will be due to the e ect of lead timeie , the analysis includes deaths from cancers in the intervention group whose equivalent in the control group are excluded because they will be diagnosed after the 7 year period . 
 the dilution of e ect seen in gure 4 as breast cancers diagnosed beyond year 7 or 8 are included represents the fact that the two groups have essentially the same screening regimen from this point in time . the di erence between the long - term e ect restricted to deaths from cancers diagnosed in the intervention phase and that reported in table 3 including all cancers irrespective of period of diagnosis shows how a reduction in mortality with screening can be obscured by the inclusion of deaths from cancers diagnosed outside the screening period . 
this observation further casts doubt on some negative results of analyses of published mortality rates include deaths from cancers diagnosed outside the screening periodie , cancers that could not have been a ected by the intervention.15 , 16 that in women who attended screening in response to the rst invitation compared to the control group , the rate ratio for breast cancer mortality was 083 ( 95% ci 065 106 ) overall when restricted to cancers diagnosed in the intervention phase . 
calculated to date of rst nhsbsp screen or end of follow - up if earlier , censored at date of diagnosis of breast cancer ; median follow - up of 106 years ( iqr 98114 )  . 
 table 5 : breast cancer incidence for all follow - up and to date of rst nhsbsp screen reporting a mammogram other than for symptomatic reasons within the previous 3 years . 
although according to the trial protocol , women in the intervention group were invited for screening up to and including the calendar year of their 48th birthday , women who moved to an area not covered by the trial would no longer have been invited for screening . 
as a result , by the seventh screening round less than 55% of women in the intervention group were actually screened.14 the reported e ect at later follow - up will therefore be less than would be observed with population screening . to explore this further , we did analyses in which deaths from breast cancer were restricted to those in cases diagnosed within 12 , 24 , and 36 months of date of last invitation to allow for varying estimates of lead time . 
however , even at 36 months after last invitation , a 15% excess of cancers in the intervention group occurred , which would result in some dilution of the e ect of screening . routinely uses the nhsbsp now two - view mammography at all screens , which has resulted in improved detection , and lower recall , together with a lower incidence of interval cancers.17 , 18 the improved detection rates apply particularly to ductal carcinoma in situ and invasive cancers of size less than 15 muse of two - view mammography in younger women would be likely to result in a similar bene t . 
thus if the uk age trial were done now , the intervention might have a greater e ect because of the improved detection of ductal carcinoma in situ and small invasive tumours . an increased threshold for recall and biopsy of microcalci cations might have contributed to a lower detection of ductal carcinoma in situ than in present screening programmes , in which the detection of ductal carcinoma in situ is generally around three times that reported in this trial . 
an increased detection of ductal carcinoma in situ in this trial might have led to a greater mortality reduction , and those cases of ductal carcinoma in situ leading to death would be more likely to cause death in the long term . we estimated a number needed to screen of around 1400 women to prevent one death during 10 years . 
this contrasts with a number needed to invite of 1904 ( sometimes incorrectly interpreted as number needed to screen ) estimated by the uspstf.7 these results raise the question of why the mortality advantage in the intervention group is reduced after 10 years from entry , even when restricted to cancers diagnosed in the intervention phase of the trial . 
in an analysis of deaths of participants diagnosed in the intervention phase strati ed by histological grade , the intervention group shows lower case fatality in women with grade 1 and 2 cancers in the periods both before and after 10 years from entry , suggesting that the intervention is achieving su ciently early detection of these tumours to a ect long - term prognosis and probably achieving complete cure in a large proportion of these . 
in women with grade 3 cancers , the intervention only confers lower case fatality in the rst 10 years , suggesting that in most of the patients with these tumours , the early detection is postponing rather than completely preventing breast cancer death . 
this notion is consistent with the fact that in the intervention group , 42% of grade 1 and 2 cancers vol 16 september 2015 1129 control group intervention group articles number at risk control intervention 106 953 53 883 105 262 52 916 103 081 51 818 99 967 50 370 5256 2577 number at risk control intervention 106 953 53 883 105 262 52 916 103 081 51 818 99 967 50 370 5256 2577 diagnosed in the intervention phase were screen - detected compared with 23% of grade 3 tumours . we did not collect treatment data for women diagnosed with breast cancer in either group of the trial because these data were not routinely available ; however , any imbalance in treatment between groups would be more likely to have an e ect on long - term follow - up , rather than short - term outcomes that are more dependent on stage at diagnosis.20 in women with grade 3 tumours , prolonging life , even if eventual death is from breast cancer , is a worthwhile achievement . 
 the sensitivity of screening in the national programme has substantially improved since the time of the screening in this trial , with detection rates rising from four to six per 1000 in the 1990s to seven to eight per 1000 today.21 this improvement in detection is likely to be because of the use of two views at each screen ( unlike in this study ) and greater use of double reading . 
also , digital mammography is now in general use , which will confer substantially improved screening sensitivity in this age group who have higher mammographic density than older women.22 , 23 our results di er substantially from those of the canadian national breast screening study ( nbss - 1 ) , which saw no reduction in breast cancer mortality in the mammography group.24 however , participants in the nbss - 1 trial were aged 4049 years at entry , and received an initial breast physical examination and instruction on breast self - examination before randomisation . 
whether cancers detected at this initial screen are included or excluded , the potential to show an e ect of initiation of mammography screening at a younger age will be diluted . 
 this trial was volunteer - based rather than populationbased and reservations have been expressed about adherence to its design , speci cally the unexpectedly high rate of palpable , advanced breast cancers in the invited group in the rst round of screening ; 25 , 26 the authors have responded to these criticisms , for example , by doing analyses excluding cancers diagnosed at the prevalent screen , 24 , 27 which still showed no signi cant mortality reduction . 
results of the swedish trials ( in ostergotland , malmo , and gothenburg ) restricted to women aged 4044 years at randomisation have shown a 15% reduction in breast cancer mortality at an average follow - up of 147 years.28 this long - term follow - up of the swedish trials concluded that , generally , the absolute e ect increased up to 12 years after randomisation , after which it was maintained . an analysis of service screening in sweden comparing women invited to screening at ages 4049 years from 1986 to 2005 with those not invited identi ed an estimated reduction in breast cancer mortality of 26% at an average follow - up of 16 years.5 in this analysis , done figure 5 : cumulative incidence of in - situ and invasive breast cancer ( a ) , in - situ breast cancer alone ( b ) , or invasive breast cancer alone ( c ) number at risk control intervention 106 953 53 883 105 262 52 916 years in trial 103 081 51 818 99 967 50 370 5256 2577 1130 vol 16 september 2015 articles on the basis of re ned mortality in cancers diagnosed at 4049 years , the cumulative mortality from breast cancer continued to diverge between the groups up to 15 years of follow - up . 
in other trials , some evidence exists for an e ect on mortality after 10 years in women aged 4049 years at randomisation , although again this nding is complicated by the fact that these analyses will include cancers diagnosed after age 50 years.29 , 30 in our study , all women will have received their last invitation before reaching age 50 years , thus avoiding this issue . 
 the collective data for epoch of and age at diagnosis might resolve this , by providing greater numbers of participants for long - term follow - up restricted to similar age ranges to ours . correct estimates of overdiagnosis need su cient follow - up to allow time for the compensatory drop after the end of invitation to screening.31 in our trial , estimates of overdiagnosis will be a ected by the fact that women in the control group were invited to screening in the nhsbp starting at ages 5052 years . 
thus , our results provide no evidence that screening in the trial resulted in any overdiagnosis in addition to any occurring as a result of nhsbsp screening , which cannot be assessed because of lead time . 
the absence of a marked excess of invasive cancers in the intervention group at the start of the trial represents the shorter lead time at younger ages , which has also been reported by others.29 at the time of completion of the rst nhsbsp screen , a signi cant excess of in situ disease in the intervention group was noted , balanced by a reduction in invasive disease , which was non - signi cant . 
 the overall excess of breast cancer in the intervention group before the rst nhsbsp screen of 014 per 1000 women - years is as compatible with a small lead time e ect as it is with overdiagnosis . 
no excess incidence was reported in the intervention group at nal follow - up , which is quali ed by the fact that both study and control groups will have been o ered screening in the nhsbsp at this time . 
however , because the intervention group , with 260 638 more screening episodes than the control group , showed no excess incidence after entry to the nhsbsp , it suggests that overdiagnosis is at worst a very minor occurrence . 
figure 5 shows that during the intervention phase when only the intervention group was being screened , the di erence in incidence was small , and even a potential short lead time would rule out substantial overdiagnosis . overall , these results support an early reduction in mortality from breast cancer with annual mammography screening in women aged 4049 years . 
all authors have participated in interpretation of the results and have seen and approved the nal version . declaration of interests smm received funding from the national institute for health research health technology assessment , american cancer society , cancer research uk , department of health , medical research council , and the us national cancer institute , during the conduct of the study . 
all other authors declare no competing interests . acknowledgments the trial is supported by a grant from the national institute for health research health technology assessment programme , and additional funding from the american cancer society . 
the authors would like to acknowledge the role of multidisciplinary teams at participating trial centres , in collection of the large volumes of clerical and clinical information needed for this trial . published online february 12 , 2018 s1470 - 2045 ( 18 ) 30091 - 3 see articles page 295 adjuvant therapy for women with high - risk endometrial carcinoma identification of optimal therapy for patients with highrisk endometrial carcinoma has been frustrated by neardichotomous paradigms of surgical treatment in the international community and a scarcity of level 1 data to inform adjuvant treatment . 
for example , at a meeting of the european society for medical oncologyeuropean society of gynaecological oncologyeuropean society for radiotherapy and oncology endometrial consensus conference working group , 14 recommendations were supported by level 1 or 2 evidence out of 50 nonsurgical treatment topics.1 however , the emergence of successful international cooperatives will accelerate the pace of innovation and learning worldwide , which will be welcome news indeed for both treating clinicians and patients who suffer from endometrial cancer . 
in the lancet oncology , the third successive randomised trial of endometrial cancer treatment is presented by stephanie m de boer and colleagues2 and the portec group on behalf of seven participating countries . 
 the portec - 3 investigators randomly assigned patients with high - risk endometrial cancer to pelvic radiotherapy alone or adjuvant chemotherapy during and after radiotherapy ( chemoradiotherapy ) , a regimen based on the phase 2 rtog - 9708 trial.3 5 - year failurefree survival favoured the chemoradiotherapy group with a 7% difference between the groups . 
analysed separately , patients with stage iii disease obtained the greatest benefit from chemoradiotherapy , with a more than 11% absolute improvement in failure - free survival ( hazard ratio [ hr ] 066 , 95% ci 045097 , p = 0031 ) a clinically relevant finding that exceeds the 10% improvement used to design the trial . 
the 9% improvement in 5 - year overall survival in patients with stage iii disease was smaller than the study was designed to detect ( adjusted p = 0074 )  . 
these results are similar to the pooled results of the nsgo 9501 / eortc 55991 and mango - iliade 3 trials showing improved failure - free survival but non - significantly higher overall survival ( p = 007 ) for patients receiving radiotherapy sequentially with adjuvant chemotherapy compared with radiotherapy alone.4 detailed qualitative data from portec - 3 have been previously published , serving to contextualise these survival improvements.5 treatment - related toxicity was worse in the chemoradiotherapy group , with 60% of patients experiencing grade 3 or worse adverse events compared with 12% in those receiving radiotherapy alone . 
this is an important consideration , recognising that in the usa , patients older than 70 years are 50% less likely than their younger counterparts to receive adjuvant chemotherapy or radiotherapy after surgery.6 although lymph node assessment was not required , it was done in the majority of patients , was not associated with failure - free survival , and rates were identical in both groups . 
the findings of portec - 3 should therefore be relevant to all practices , irrespective of surgical paradigm . by contrast with the benefit conferred to stage iii patients , the addition of chemotherapy did not improve outcomes for stage i or ii patients . 
although portec - 3 might have been underpowered to identify differences in failure - free survival in this subgroup , the small magnitude of benefit does not seem to justify the accompanying increase in adverse events , impairment in long - term quality of life , and longer treatment duration . 
the use of radiotherapy alone is supported by unpublished results of gog - 249 , 7 in which high - risk stage i or ii patients were randomly assigned to radiotherapy or chemotherapy and vaginal brachytherapy . 
chemotherapy did not improve failurefree survival , overall survival , or the incidence of distant recurrences , but resulted in twice the incidence of nodal recurrence and significantly more grade 3 or worse adverse events than did radiotherapy alone . 
the ongoing 268 vol 19 march 2018 comment engot - en2 - dgcg / eortc - 55102 trial evaluating the role of chemotherapy versus observation in patients with high - risk , node - negative endometrial cancer will be pivotal given the conflicting efficacy of chemotherapy observed for uterine serous carcinoma in portec - 3 , the pooled analysis of nsgo - 9501 , eortc - 5599 , and mango - iliade 3 trials , and the gog - 122 trial.2 , 4 , 8 recurrence was most recurrences of endometrial cancer manifested in portec - 3 , and although as distant metastases this type of less common with chemoradiotherapy , the difference did not achieve statistical significance . 
unpublished results of gog - 258 , 9 which randomly assigned patients to the same chemoradiotherapy regimen as that used in portec - 3 or to chemotherapy alone , showed fewer distant recurrences in the chemotherapy group at the expense of more vaginal and nodal recurrences and no difference in failure - free survival or estimated 5 - year overall survival.9 future trials should investigate regimens to maximise the local control advantages of radiotherapy with distant control improvements seen with chemotherapy for patients with high - risk endometrial cancer . 
continued assessment of toxicity , quality of life , and cost will be paramount to define optimal adjuvant therapy . we declare no competing interests . copyright the author ( s )  . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
toxicity and quality of life after adjuvant chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer ( portec - 3 ) : an open - label , multicentre , randomised , phase 3 trial . 
proc am soc clin oncol 2017 ; 35 : abstr 5505 . * sean c dowdy , gretchen e glaser mayo clinic , rochester , mn 55905 , usa dowdy.sean@mayo.edu bmi and outcomes in melanoma : more evidence for the obesity paradox the association between increased body - mass index ( bmi ) and the risk of developing and dying from cancer has been recognised across a broad range of tumour types.1 , 2 the magnitude of this association is so great that in the usa obesity is considered to be the major preventable cause of cancer.3 however , data regarding the effect of obesity on the outcomes of patients undergoing cancer treatment less clear . 
several observational studies in different tumour types have shown that a moderately increased bmi ( compared with an optimal bmi of 225 kg / m2 ) is associated with improved outcomes both around the time of treatment and in later years of follow - up for several cancers.4 however , this protective effect is almost universally reversed as bmi increases to the morbidly obese level , an effect referred to as the obesity paradox.4 many possible explanations have been cited to explain this effect , some of which relate to observational biases and the inadequacy of bmi as an accurate representation of obesity , whereas other suggestions support an underlying biological mechanism in moderately obese patients undergoing cancer treatment that could explain the beneficial effect observed.4 an analysis by jennifer mcquade and colleagues5 in the lancet oncology provides substantial evidence of a biological mechanism , yet to be elucidated , that increased published online february 12 , 2018 s1470 - 2045 ( 18 ) 30077 - 9 see articles page 310 vol 19 march 2018 comment correction to lancet oncol 2017 ; 18 : 67281 j , f o n t a , g a r c a d o n a s prez - valderrama b , et al . 
maintenance therapy with vinflunine plus best supportive care versus best supportive care alone in patients with advanced urothelial carcinoma with a response after first - line chemotherapy ( maja ; sogug 2011 / 02 ) : a multicentre , randomised , controlled , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 67281in this article , the declaration of interests should read jg - d reports personal fees from astellas , janssen ; grants and personal fees from astrazeneca , pfizer , pierre fabre , merck , bioclin , bristol myers squibb , novartis , and msd ; grants , personal fees , and non - financial support from roche ; and grants from gammamabs , outside the submitted work . 
af reports grants from astellas , astrazeneca , pierre - fabre ; personal fees and non - financial support from sanofi , janssen , bayer , and roche , outside the submitted work . 
bp - v reports personal fees from astellas pharma , novartis , pfizer , pierre fabre , bayer , sanofi , bristol - myers squibb , ipsen , and janssen - cilag , during the conduct of the study . 
jaa reports grants and personal fees from glaxosmithkline and novartis ; personal fees and nonfinancial support from jansen cilag ; grants , personal fees and non - financial support from bms ; personal fees from pfizer , roche , and eusa ; grants from sanofi and pierre fabre , outside the submitted work . 
nl reports personal fees from pfizer , sanofi , pierre fabre , roche , ipsen , pharma mar , bms , bayer , astrazeneca , astellas , and msd , outside the submitted work . 
jcv - g reports personal fees from pfizer , astellas , janssen , msd , bayer , roche , bristol , astrazeneca , boehringer , pierre fabre , novartis , ipsen , celgene , lilly , merck , sanofi , and mundipharma , outside the submitted work . 
bm reports personal fees and non - financial support from pfizer and janssen ; personal fees from novartis , astellas oncology , bms , sanofi , ipsen , bayer ; and grants and personal fees from roche , outside the submitted work . 
agda reports advisory board , consultancy and speaker honoraria or travel support from pierre fabre , roche , bristol - myers squibb , msd , pfizer , novartis , bayer , janssen , sanofi , astellas , eusa pharma , and eisai ; and research funding from astellas . 
dc reports personal fees from janssen , roche , astellas , msd , ipsen , pfizer , bms , bayer , astrazeneca , novartis , lilly , sanofi , pierre fabre , and boheringer , outside the submitted work . 
eg reports grants from pierrefabre , during the conduct of the study ; personal fees and non - financial support from janssen , pfizer , bayer , ipsen , novartis , bms , rovi ; personal fees from menarini and leo pharma ; and nonfinancial support from pierre - fabre , outside the submitted work . 
ua reports non - financial support from novartis , pierre fabre , and ipsen ; personal fees from bayer , janssen , astellas , and pfizer ; and personal fees and nonfinancial support from sanofi , roche , and bms , outside the submitted work . 
 xgdm reports personal fees from pfizer , ipsen , bms , roche , lilly , pharmamar , eusapharma , and pierre fabre ; and grants from astrazeneca , outside the submitted work . 
md has participated in advisory boards , consultancy , and speaker bureaus for roche , bristol - myers squibb , msd , pfizer , janssen , sanofi , astellas ; and received travel and accommodations expenses from roche , astellas , janssen , bayer , and lilly . 
jp has received honoraria as a consultant on advisory boards from pfizer , astellas , janssen , msd , bayer , roche , bms , boehringer , astrazeneca , ipsen , novartis , eusa pharma , eisai , and sanofi ; and as speaker from kyowa , pierre - fabre , celgene , lilly , and merck . 
 rm - b has served as a consultant or on advisory and / or speakers bureaus for sanofi aventis , bayer , janssen , astrazeneca , merck sharp & dohme , and asofarma ; and received travel and accommodations expenses from roche , sanofi aventis , astellas , janssen , merck sharp & dohme , bayer , pharmacyclics , clovis oncology , and lilly . 
jlp - g reports non - financial support from pierre fabre , during the conduct of the study ; non - financial support from roche , bms , and msd , outside the submitted work . 
jb reports grants and personal fees from pfizer , merck , bms ; personal fees from genentech , astrazeneca , pierre - fabre ; and grants from takeda , during the conduct of the study . 
 this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1493503 zackrisson s , lng k , rosso a , et al . 
 lancet oncol 2018 ; 19 : 1493503 in this article , in table 1 and table 4 , the age groups should have been listed as follows : 4049 , > 4959 , > 5969 , and > 69 . 
the title and legend of figure 2 should have read as follows : number of false - positive results among participants over the trial period who were recalled only on digital breast tomosynthesis and digital mammography , respectively . 
 these corrections have been made to the online version as of jan 3 , 2019 . vol 20 january 2019 corrections published online may 9 , 2018 s1470 - 2045 ( 18 ) 30289 - 4 see articles page 785 genetic predisposition to medulloblastomas : just follow the tumour genome for a the actual contribution of germline mutations to paediatric cancers has been a major concern for paediatricians , basic researchers , geneticists , epidemiologists , and parents long time . 
 the first notable piece of work1 in this field was produced by researchers from the st jude research hospital the number of germline variants in known cancer genes , assessed using constitutional dna from more than 1000 paediatric patients . 
first , by use of the largest retrospective cohort constituted and validating it on prospectively collected dnas , it aimed to unbiasedly assess the actual incidence of cancer predisposition syndromes in patients with medulloblastoma . 
the authors identified six genes with a significant excess of damaging germline mutations for patients with medulloblastoma : apc , brca2 , palb2 , ptch1 , sufu , and tp53 . 
this study confirms the high prevalence of sufu and ptch1 mutations in infants with shh medulloblastomas , 3 , 4 and also substantiates the overall higher risk for tp53 or ptch1 germline mutations in shh medulloblastomas , whatever the age at onset.5 however , it also highlights that a familial history of cancer is often absent in these cases of shh medulloblastoma . 
 the study shows for the first time the phenotype of the rare ( seven [ 1% ] of 1022 patients ) germline apcrelated medulloblastomas ( five of whom were children in the wnt subgroup who had excellent overall survival of 100% at 36 months ) which , by contrast with shh medulloblastomas , usually occur in a clear familial context , emphasising the need for a careful interview regarding familial history in children with wnt medulloblastomas . 
 the second main finding was the refinement of the potential role of brca2 and palb2 germline mutations in medulloblastoma , so far known only in the context of fanconi anaemia.6 , 7 germline heterozygous brca2 ( seven [ 1% ] of 1022 patients ) and palb2 ( five [ < 1% ] of 1022 ) variants might also be associated with an increased risk of medulloblastoma in childhood . 
the presence of loss of heterozygosity of the wildtype brca2 and palb2 allele in some tumours or the tendency of corresponding tumours to present some signs of homologous recombination repair deficiency ( hrd ) might suggest pathogenicity . 
international collaboration to collect data from more families with brca2 and palb2 mutations with precise evaluation of the frequency of medulloblastomas might help to decipher the actual involvement of these heterozygous mutations in predisposition to medulloblastoma . 
 because chromothripsis medulloblastoma indicates the presence of tp53 mutations and can subsequently induce familial screening , 4 finding insights for hrd and brca2 and palb2 mutations in a child with medulloblastoma might eventually cause the initiation of tumour screening in the relatives . 
since early cancer detection in unaffected individuals is one major goal of genetic counselling , possible familial consequences of broad genetic analyses on tumour dna will need to be explicitly anticipated with parents ; moreover , the medical benefit and psychological effects of such findings on families with no cancer history should be prospectively evaluated . finally , the study does not identify any specific predisposing genes for group 3 and group 4 medulloblastomas , which shows that a young age at cancer 722 vol 19 june 2018 comment onset ( group 3 ) might not indicate a strong probability of predisposing syndrome per se . 
moreover , although many studies have investigated this class of high - penetrance predisposition genes , lowthe penetrance , high - frequency alleles remains unknown and still needs to be investigated through genome - wide association studies for medulloblastoma . 
the study highlights the major interest of somatic molecular criteria , in addition to family history and potential malformative syndrome , to suggest genetic predisposition and hence lead to genetic counselling and germline genetic assessment with a clear prioritisation scheme depending on the type of medulloblastoma . * franck bourdeaut , olivier delattre siredo pediatric cancer center , inserm u830 , institut curie , paris 75005 , france franck.bourdeaut@curie.fr we declare no competing interests . copyright the author ( s )  . 
blood 2004 ; 103 : 255459 . targeting the tumour vasculature in mesothelioma in 2018 , malignant mesothelioma remains a rapidly lethal cancer for which there is no standard second - line therapy . 
the disease represents both an opportunity for drug development and a substantial challenge , as evidenced by recent negative , yet appropriately controlled and powered , phase 3 trials.1 , 2 inter - patient heterogeneity , coupled with an absence of personalised strategies , account for these previous failures , highlighting an unmet need . 
these include the identification of the ezh2 subunit of polycomb in bap1 - mutated repressor complex 2 as a target mesothelioma , which is being explored in a proof - ofconcept phase 2 study ( nct02860286 ) .3 pegylated arginine deiminase has shown efficacy in mesotheliomas that do not express argino succinate synthetase , and a combination strategy is being investigated in the phase 3 atomic trial ( nct02709512 )  . 
checkpoint inhibition shows activity in the context of programmed cell death ligand 1 ( pdl - 1 ) expression ; 4 however , the jury is still out regarding the significance of this potential biomarker for patient selection in treating mesothelioma . 
 in the lancet oncology , vanesa gregorc and colleagues5 report the results of their phase 3 ngr015 trial , in which they tested a novel vascular disrupting agent ( ngr - htnf ) in an unselected population of patients . 
at picomolar concentrations , the endothelial barrier function of the neovasculature impaired , enhancing chemotherapy penetration in murine models.6 in a previous phase 2 trial , 7 ngrhtnf monotherapy showed an arguably modest disease control with 44% of patients achieving disease control , with evidence of partial response ( albeit 2% ) , and a median of 28 months progression - free survival . 
we aimed to assess and define these genes to provide evidence for future screening guidelines . methods in this international , multicentre study , we analysed patients with medulloblastoma from retrospective cohorts ( international cancer genome consortium [ icgc ] pedbrain , medulloblastoma advanced genomics international consortium [ magic ] , and the cefalo series ) and from prospective cohorts from four clinical studies ( sjmb03 , sjmb12 , sjyc07 , and i - hit - med )  . 
dna methylation profiling was done to determine consensus molecular subgroups : wnt ( mbwnt ) , shh ( mbshh ) , group 3 ( mbgroup3 ) , and group 4 ( mbgroup4 )  . 
previously defined somatic mutational signatures were used to further classify medulloblastoma genomes into two groups , a clock - like group ( signatures 1 and 5 ) and a homologous recombination repair deficiency - like group ( signatures 3 and 8 ) , and chromothripsis was investigated using previously established criteria . 
progression - free survival and overall survival were modelled for patients with a genetic predisposition to medulloblastoma . findings we included a total of 1022 patients with medulloblastoma from the retrospective cohorts ( n = 673 ) and the four prospective studies ( n = 349 ) , from whom blood samples ( n = 1022 ) and tumour samples ( n = 800 ) were analysed for germline mutations in 110 cancer predisposition genes . 
in our rare variant burden analysis , we compared these against 53 105 sequenced controls from exac and identified apc , brca2 , palb2 , ptch1 , sufu , and tp53 as consensus medulloblastoma predisposition genes according to our rare variant burden analysis and estimated that germline mutations accounted for 6% of medulloblastoma diagnoses in the retrospective cohort . 
the prevalence of genetic predispositions differed between molecular subgroups in the retrospective cohort and was highest for patients in the mbshh subgroup ( 20% in the retrospective cohort )  . 
these estimates were replicated in the prospective clinical cohort ( germline mutations accounted for 5% of medulloblastoma diagnoses , with the highest prevalence [ 14% ] in the mbshh subgroup )  . 
patients with germline apc mutations developed mbwnt and accounted for most ( five [ 71% ] of seven ) cases of mbwnt that had no somatic ctnnb1 exon 3 mutations . 
germline tp53 mutations presented only in childhood patients in the mbshh subgroup and explained more than half ( eight [ 57% ] of 14 ) of all chromothripsis events in this subgroup . 
 germline mutations in palb2 and brca2 were observed across the mbshh , mbgroup3 , and mbgroup4 molecular subgroups and were associated with mutational signatures typical of homologous recombination repair deficiency . 
 funding german cancer aid ; german federal ministry of education and research ; german childhood cancer foundation ( deutsche kinderkrebsstiftung ) ; european research council ; national institutes of health ; canadian institutes for health research ; german cancer research center ; st jude comprehensive cancer center ; american lebanese syrian associated charities ; swiss national science foundation ; european molecular biology organization ; cancer research uk ; hertie foundation ; alexander and margaret stewart trust ; v foundation for cancer research ; sontag foundation ; musicians against childhood cancer ; bc cancer foundation ; swedish council for health , working life and welfare ; swedish research council ; swedish cancer society ; the swedish radiation protection authority ; danish strategic research council ; swiss federal office of public health ; swiss research foundation on mobile communication ; masaryk university ; ministry of health of the czech republic ; research council of norway ; genome canada ; genome bc ; terry fox research institute ; ontario institute for cancer research ; pediatric oncology group of ontario ; the family of kathleen lorette and the clark h smith brain tumour centre ; montreal childrens hospital foundation ; the hospital for sick children : sonia and arthur labatt brain tumour research centre , chief of research fund , cancer genetics program , garron family cancer centre , mdts garron family endowment ; bc childhood cancer parents association ; cure search foundation ; pediatric brain tumor foundation ; brainchild ; and the government of ontario . copyright 2018 the author ( s )  . 
following the recognition9 of four consensus molecular subgroups ( wnt [ mbwnt ] , shh [ mbshh ] , group 3 [ mbgroup3 ] , and group 4 [ mbgroup4 ] ) with distinct demographics and clinical outcomes , 10 patients with germline tp53 , sufu , and ptch1 mutations have been reported to be predisposed to develop mbshh.11 , 12 although several case studies have reported in patients with fanconi medullo blastomas arising specific anaemia , whether medulloblastoma subgroups , and whether heterozygous germline mutations13 also confer an increased risk of developing medulloblastoma , remain unknown . 
a comprehensive study14 of damaging germline mutations in cancer predisposition genes across a diverse set of paediatric cancers identified variants likely to predispose to the disease in three ( 8% ) of 37 patients with medulloblastomaa cohort size that is too small to allow these predispose these issues to be thoroughly addressed . 
owing to these uncertainties , and since knowledge about germline mutations can be useful for clinical practice , 8 assessment of larger patient series is crucial for the identification of consensus medullo blastoma predisposition genes to estimate the con tribution of genetic predisposition towards consensus molecular sub groups , and investigate whether affected patients have distinct clinical outcomes . 
a comprehensive under standing of molecular alterations in affected patients would further help in the development of clinical screening guidelines for genetic risk assessment in paediatric patients . in this study , we provide a comprehensive description of genetic risk factors across 1022 patients with medulloblastoma based on a retrospective discovery cohort and validation in a prospective clinical cohort . 
additionally , which patients would benefit from genetic counselling in the context of molecular subgroupingnowadays routinely applied in clinical trials and implemented into the revised who classification of cns tumours in 2016and whether genetic predisposition can be recognised based on familial patterns were unclear . 
additionally , several paediatric cancer centres have implemented routine multigene panel analysis and whole - exome analysis of medulloblastomas ; however , these centres encounter several germline mutations with uncertain clinical significance . 
no study has previously aimed to define a consensus set of medulloblastoma predisposition genes or has investigated under which circumstances genetic counselling and testing should be offered to patients with medulloblastoma . added value of this study this study is based on an international cohort of 1022 patients with medulloblastoma , and includes detailed information about medulloblastoma subgroups ( wnt [ mbwnt ] , shh [ mbshh ] , group 3 [ mbgroup3 ] , and group 4 [ mbgroup4 ] ) , somatic mutation landscapes , and clinical outcomes . 
we defined and characterised six consensus , clinically relevant medulloblastoma predisposition genes on the basis of rare variant burden analysis ( apc , brca2 , palb2 , ptch1 , sufu , and tp53 )  . 
half of all patients with damaging germline mutations were not recognised based on familial history of cancer ; however , these patients exhibited distinct phenotypes with respect to age at diagnosis , molecular subgroups , somatic mutation patterns , and clinical outcomes . 
about one in five patients in the mbshh subgroup developed medulloblastoma in the context of a genetic predisposition , underscoring the need for a dedicated genetic screening programme and surveillance programme in this patient group . 
damaging germline mutations in known cancer predisposition genes were rare in paediatric patients in the mbgroup3 and mbgroup4 subgroups , which indicates conservative ordering of genetic tests in these groups . 
we propose clinical guidelines for genetic screening in medulloblastoma based on routinely acquired clinical and molecular tumour phenotypes . implications of all the available evidence a significant prevalence of clinically important germline mutations in two of four molecular subgroups reveals that genetic counselling and testing should be established as a standard - of - care procedure in the management of patients with medulloblastoma . 
we obtained biological samples from all patients , who all provided written informed consent , in accordance with institutional review board guidelines . patient accrual for our retrospective cohort was done from 2003 until 2016 . 
patient accrual for the sjmb03 trial was done from sept 9 , 2003 , until march 7 , 2013 and for the sjyc07 trial was done from dec 17 , 2007 , until march 31 , 2017 . 
the age limit for eligibility in the prospective studies was 5 years or younger ( sjyc07 ) , 321 years ( sjmb03 ) , and 339 years ( sjmb12 )  . 
 patients in the i - hit - med study were excluded if they were registered in another clinical trial for the same diagnosis ( relapse is defined as a second diagnosis ) or if a valid ethical committee approval was lacking . procedures whole - genome and whole - exome sequencing data for germline and tumour samples were generated at the german cancer research centre ( icgc pedbrain ; heidelberg , germany ) , canadas michael smith genome sciences centre ( magic ; vancouver , bc , canada ) , broad institute of massachusetts institute of technology and harvard ( cambridge , ma , usa ) , and st jude childrens research hospital ( pediatric cancer genome project ; memphis , tn , usa )  . to ensure standardisation of genomic data processing , we used the same uniform computational analysis workflows for all germline and tumour samples . 
we used delly for germline genomic structural variant discovery with default settings for whole - genome sequencing samples and a custom read - depth - based copy - number variation ( cnv ) - calling pipeline for whole - exome sequencing samples . 
we based this custom pipeline on read quantification by bedtools in exome capture regions ( maq > 30 ) , followed by variance stabilising transformation of count data with the vst function from the deseq2 r package ( version 1.8.2 ) , unsupervised estimation of hidden confounders using the r package peer ( 30 hidden confounders ) , and copynumber segmentation based on standardised residuals using circular binary segmentation ( r package dnacopy , version 1.50 , default settings )  . 
raw cnv calls were filtered further for size ( to include only those > 10 kb ) , minimum number of exons ( > 2 ) , and cnv signal intensity ( > 4 sds )  . 
 any snv , short indel , and mnv that was observed at low variant allele frequency in blood ( 315% ) and high variant allele frequency in tumours ( > 50% ) was considered a putative mosaic mutation . 
we restricted the analysis to reads with mapping quality of more than 30 ( 10 log10 pr [ mapping position is wrong ] ) , base quality of more than 20 ( 10 log10 pr [ mapping position is wrong ] ) , and sites with more than 30 times sequencing coverage ( ie , number of reads )  . 
we excluded any variant that was present in public genetic archives and discovered in germline genomes of other patients with medulloblastoma . for classification of damaging germline mutations , germline variants were annotated with the ensembl variant effect predictor ( vep ; r81 )  . 
high - impact ( ie , damaging ) germline mutations were defined as frameshift , stop gain , start lost , canonical splice site , exon or gene deletions , known ( clinvar ; accessed feb 16 , 2017 ) damaging non - canonical splice site variants , and somatic mosaic mutations ( defined as mutations present in a subset of normal cells )  . 
putative damaging germline mutations were removed if the estimated minor allele frequency in at least one continental population was more than 01% , which we judged on the basis of 53 105 sequenced individuals that were assigned to known ( control ) populations and without a cancer diagnosis from the exome aggregation consortium ( exac ) resource , the 1000 genomes project , and the national heart , lung , and blood institute go exome sequencing project . 
putative gain - of - function missense variants in tp53 were further evaluated by use of information in the international agency for research on cancer tp53 database and annotated as pathogenic if tp53 mutations were classified as non - functional in experimental transcriptional activity assays . 
we estimated the primary population ancestry ( european , african , east asian , south asian , and native american ) for all patients with medulloblastoma with a supervised decomposition approach20 and ancestry - informative markers that are within exac - defined exome capture target regions . identification of somatic mutations ( snvs , small indels , and copy - number alterations ) was pursued in a standardised manner across all samples ( matched tumour or normal genome as well as exome pairs ) with the german cancer research center ( known as dkfz ) and european molecular biology laboratory cancer genome analysis workflow of the pcawg consortiu somatic snvs and indels were further stringently filtered for germline contamination using information from dbsnp and the 1000 genomes project . 
we used a highstringency structural variant set by additionally filtering somatic structural variants detected in at least 1% of a set of 1105 germline samples from healthy individuals belonging to phase 1 of the 1000 genomes project , and by requiring absence of somatic structural variants in all medulloblastoma germline samples of this study . 
for inference of high - stringency structural variants , we additionally required at least four supporting read pairs21 with a minimum mapping quality of 20 ( 10 log10 pr [ mapping position is wrong ] ) and restricted valid somatic structural variant sizes from 100 bp to 500 mb . we quantified previously defined somatic mutational signatures22 ( termed 1 , 3 , 5 , and 8 ) using tumour - specific somatic point - mutation spectra and published signature probabilities . 
 signatures 1 and 5 ( clock - like signatures ) are associated with ageing ( a clock - like accumulation of mutations ) and occur in normal , non - malignant cells , 22 whereas signatures 3 and 8 are associated with homologous recombination repair deficiency ( hrd ) and have been reported in cancer tissues . 
we used these mutational vol 19 june 2018 articles signatures to further classify medulloblastoma genomes into two groups , a clock - like group ( signatures 1 and 5 ) and a hrd - like group ( signatures 3 and 8 )  . 
somatic mutation spectra were quantified with the r package somaticsignatures ( version 2.6 ) and decomposed into contributions of known mutational signatures based on the lawsonhanson algorithm for non - negative least squares ( nnls version 1.1 , r package )  . 
the quantification error ( residual sum of squares ) was correlated with the total somatic mutation burden ( spearmans r = 074 ; p < 00001 ) and it was highest in tumours with fewer than 100 somatic snvs . 
 medulloblastomas were classified as homo logous recombination repair deficient if most ( > 50% ) somatic snvs were assigned to mutational signatures 3 or 8 . to assess the burden of rare germline snvs and indels in cancer predisposition genes , we performed case control association testing in a subgroup - specific manner as well as across all subgroups based on a collection 110 autosomal cancer predisposition genes8 , 23 ( appendix p 2 )  . 
to ensure comparability with variants found in patients with medulloblastoma , exac germline mutations were normalised with vt normalize , annotated with vep ( r81 ) , and filtered for sites that passed quality controls , as defined by exac . 
moreover , we excluded any germline mutations that were present outside exacdefined target regions to reduce any possible advantages derived from improved variant calling in whole - genome sequences ( eg , exons not being covered in exac )  . 
we assumed equal effect sizes for frameshift , nonsense , splice site , and gain - of - function missense variants , as well as for variants located at any position along a gene . 
allelic relative risks were estimated by the odds ratio ( or ) , which describes the association between medullo blastoma and damaging alleles by comparing the odds of medullo blastoma in an individual carrying a wild - type allele to the odds of medulloblastoma in an individual carrying one damaging allele . 
we assumed that the penetrance of monoallelic germline mutations was lower than that of biallelic germline mutations ( ie , homozygous and compound heterozygous mutations )  . we assessed secondary somatic gene hits in tumours on three levels : point mutations , loss - of - heterozygosity , and allele - specific gene expression . 
loss of heterozygosity was quantified by use of genotyping germline alleles in available tumour genomes or exomes with freebayes and requiring a minimum coverage of ten reads , minimum base quality of 10 ( 10 log10 pr [ base is wrong ] ) , and minimum mapping quality of 10 ( 10 log10 pr [ mapping position is wrong ] )  . 
 allele - specific gene expression was quantified at heterozygous snvs and indels and mrna sequencing data by use of freebayes ( minimum mapping quality of [ 10 log10 pr ( mapping position is wrong ) ] and minimum base quality of 10 [ 10 log10 pr ( base is wrong ) ] ) and was predicted on the basis of binomial tests , an expected ratio of 05 , and p values lower than 005 . 
 when possible , multiple sites within the same gene were phased with paired - end rna sequencing data and individual sites were merged to calculate haplotypespecific expression ratios . investigated chromothripsis using previously established criteria.24 these criteria distinguish chromothripsis from dna rearrangements occurring in a stepwise fashion . 
first , we analysed breakpoint clustering in the entire genome based on highconfidence somatic structural variant calls and did statistical analysis for non - randomness of breakpoint distributions , under the assumption of an exponential distribution ( null hypothesis )  . 
overall survival and progression - free survival were based on definitions consistent with how they were evaluated within each respective patient cohort from each prospective trial : sjmb03 , sjmb12 , and sjyc07 . 
one - sided binomial tests were used for replication analysis with the alternative hypothesis defined as a lower probability of observing germline mutations in the replication cohort . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding authors had full access to all the data and had the final responsibility to submit for publication . tumour genomes were results we analysed germline genome - sequencing and exomesequencing data ( appendix pp 89 ) from 1022 patients with medulloblastoma , of whom 673 were in the retrospective discovery cohort and 349 were in the prospective clinical study cohort ( figure 1a , appendix p 3 )  . 
patientfor matched 800 samples from both cohorts ( n = 451 retrospective and n = 349 prospective ) from whole - genome sequencing ( n = 397 ) and whole - exome sequencing ( n = 403 ; figure 1a )  . 
snvs , mnvs , small ( < 30 bp ) indels , and large structural variants were predicted across 110 paediatric - onset and adult - onset cancer predisposition genes8 , 23 and classified as pathogenic based on stringent criteria . 
most damaging germline mutations have been previously described in the literature ( in 55 [ 71% ] of 77 mutations ) and already classified as ( likely ) pathogenic ( 42 [ 55% ] of 77 ) in public archives ( clinvar , lovd ; appendix pp 1012 )  . 
in total , six genes showed a significant excess of damaging germline mutations for patients with medulloblastoma namely , apc , brca2 , palb2 , ptch1 , sufu , and tp53 ( adjusted p value for multiple testing < 005 ; figure 1b , appendix p 4 )  . 
 however , a single patient in our discovery cohort harboured a heterozygous germline mutation in msh6 ( appendix pp 1012 )  . the overall prevalence of genetic predisposition based on these six genes in the retrospective discovery cohort was 6% ( 40 / 673 ) , with a highest prevalence of 20% ( 28 / 141 ) in patients in the mbshh subgroup ( figure 1c )  . 
key patient characteristics , such as sex , age at diagnosis , and molecular tumour subgroups , were similar between both cohorts ( psex = 068 , page = 017 , psubgroup = 012 ; figure 1a )  . 
the overall prevalence of genetic predisposition in our prospective cohort ( 17 [ 5% ] of 349 ) was consistent with estimates ( p = 024 ; from our retrospective cohort figure 1d , appendix pp 1012 )  . 
notably , patients in the mbwnt subgroup also had an increased prevalence of germline predisposition in both the discovery and replication cohort , albeit more modest than for patients in the mbshh subgroup ( figure 1c , d )  . genes we closely analysed key demographic , clinical , and molecular characteristics of patients with a genetic predisposition in these six genes . 
most patients with available subgroup information developed mbshh ( 41 [ 76% ] of 54 ; figure 2a ) and age at diagnosis also differed significantly between patients with germline mutations in medulloblastoma predisposition ( p < 00001 ; figure 2b )  . 
patients with germline sufu or ptch1 mutations were typically diagnosed as infants at a median age of 20 years ( iqr 1323 ) , whereas patients with apc or tp53 mutations were diagnosed as children at a median age of 98 years ( iqr 8011 )  . 
clinical signs of a genetic predisposition were noted in 16 ( 41% ) of 39 patients and familial history of cancer in 17 ( 46% ) of 37 patients , and both were different between patients with germline mutations in medulloblastoma pre disposition genes ( p = 0017 and p = 0046 , respectively ; figure 2c , 2d )  . 
for example , only one ( 9% ) of all 11 ptch1 and sufu mutation carriers with available medical records had a family history of cancer ; however , eight ( 67% ) of records had 12 patients with available medical clinical symptoms consistent with gorlins syndrome 790 vol 19 june 2018 articles a male ( 63% ) male ( 64% ) medulloblastoma cohort retrospective : n = 673 prospective : n = 349 whole - genome and whole - exome squencing germline : n = 1022 tumour : n = 800 molecular subgroup 844 tumours 110 cancer predisposition genes age at diagnosis molecular subgroup female ( 37% ) female ( 36% ) child ( 70% ) child ( 79% ) infant ( 17% ) adult ( 13% ) infant ( 16% ) adult ( 5% ) group 4 ( 38% ) group 4 ( 40% ) ( 28% ) ( 27% ) group 3 ( 27% ) wnt ( 6% ) group 3 ( 22% ) wnt ( 10% ) sufu ptch1 tp53 palb2 brca2 retrospective cohort prospective cohort 1000 all subgroups of medulloblastoma group 3 group 4 rr ( 95% ci ) n = 349 p = 024 n = 673 group 3 group 4 group 3 group 4 n = 32 20% n = 141 n = 134 n = 189 n = 36 p = 081 14% n = 95 p = 0080 n = 78 p = 048 n = 139 p = 0051 figure 1 : discovery and replication of medulloblastoma predisposition genes ( a ) study design and patient characteristics . 
patients with damaging germline mutations in apc , ptch1 , sufu , tp53 , palb2 , and brca2 . ( eg , macrocephaly , jaw cysts , and frontal bossing ; appendix pp 1012 )  . 
by contrast , all four apc mutation carriers with available medical records had a familial history of familial adenomatous polyposis and associated cancers ( eg , adrenocortical carcinoma )  . 
of note , additional malignancies were observed in six ( 12% ) of 50 patients with medulloblastoma and all were restricted to patients with germline apc ( n = 3 ) or tp53 ( n = 3 ) mutations ( appendix pp 1012 )  . at a median follow - up of 48 months ( iqr 2878 ) , 5 - year progression - free survival for 49 patients with a genetic predisposition who were evaluable for this outcome was 52% ( 95% ci 4069 )  . 
progression - free survival ( logrank p = 00056 ) and overall survival ( log - rank p = 000032 ) differed significantly across patients with germline mutations in different medullo blastoma predisposition genes ( figure 3 )  . germline apc mutations were found in seven ( 1% ) of all 1022 patients with medulloblastoma and included one infant , five children , and one adult patient . 
two of these seven patients harboured partial or full gene deletions ( appendix p 5 ) and the remaining five patients had frameshift and nonsense mutations between codons 554 and 1113 , a region associated with classical familial adenomatous polyposis phenotypes . 
all five wnt - driven medulloblastomas lost the wild - type apc allele and the shhdriven medulloblastoma showed retention of the wild - type allele ( figure 4a )  . 
furthermore , germline apc mutations in mbwnt patients were mutually exclusive with somatic ctnnb1 exon 3 mutations ( p < 00001 ) , the primary26 somatic driver event in mbwnt ( figure 4b )  . 
 overall , germline apc mutations were identified in five ( 71% ) of seven ctnnb1 - wild - type mbwnt cases and , together with somatic ctnnb1 mutations , explained 97% ( 64 / 66 ) of all wnt - driven medulloblastomas . 
by contrast , monosomy 6a frequent somatic chromosome aberration in mbwnt ( in 55 [ 83% ] of 66 cases ) was not mutually exclusive with germline apc mutation status ( p = 019 ) ; although we observed two patients with vol 19 june 2018 articles a group 4 group 3 n = 54 ; p < 00001 patients ( % ) 100% n = 57 ; p < 00001 age at diagnosis ( years ) ( 12 ) ( 23 ) ( 35 ) ( 530 ) ( 410 ) ( 911 ) ( 711 ) brca2 * ptch1 sufu tp53 palb2 brca2 sufu ptch1 brca2 * palb2 brca2 tp53 n = 37 ; p = 0046 n = 39 ; p = 0017 adult ( 18 ) child ( 4 - 17 ) infant ( 3 ) ptch1 sufu tp53 palb2 brca2 brca2 * palb2 tp53 brca2 sufu ptch1 brca2 * figure 2 : clinical characteristics of patients with a genetic predisposition ( a ) molecular tumour subgroups . 
overall and progression - free survival for patients with apc - mbwnt was 100% ( 95% ci 100100 )  . germline tp53 mutations were found in 14 ( 1% ) of all 1022 patients with medulloblastoma and were only present in patients with mbshh ( 13 / 13 ; data missing for one patient )  . 
notably , germline tp53 mutations were identified in 13 ( 8% ) of 170 paediatric mbshh patients and 13 ( 20% ) of 63 children aged between 5 years and 16 years with mbshh . 
most germline tp53 mutations ( 13 / 14 ) clustered within the dna - binding domain ( appendix p 6 ) and somatic inactivation of the wild - type tp53 allele was detected in all 13 available medullo blastoma genomes via loss of heterozygosity ( figure 4a )  . 
all eight whole - genome - sequenced tp53deficient mbshh exhibited complex somatic genomic rearrangements consistent with chromothripsis21 and accounted for eight ( 57% ) of all 14 chromothripsis events in the mbshh subgroup . 
5 - year overall survival for patients with germline tp53 mutations was 27% ( 95% ci 1072 ; figure 3 )  . germline sufu and ptch1 mutations were detected in 20 ( 2% ) of all 1022 patients with medulloblastoma , exclusively the mbshh subgroup ( 19 / 19 ; data missing for one patient ) , and accounted for 11% ( 18 / 170 ) of all paediatric patients with mbshh and 21% ( 17 / 80 ) of all infant patients with mbshh . 
we observed somatic loss of the sufu or ptch1 wild - type allele in all ( n = 18 ) sequenced mbshh that were diagnosed in patients with germline sufu or ptch1 mutations . 
only six of 20 germline sufu and ptch1 mutations have been previously described in the literature ( appendix pp 1012 ) , suggesting either appreciable amounts of de - novo mutagenesis or poor reporting to public archives . 
in support of the de - novo mutagenesis theory , a de - novo germline ptch1 mutation was observed in a patient with mbshh from our retrospective cohort , for whom whole - exome sequences were also available for both parents . 
clinical information was frequency ranged 792 vol 19 june 2018 articles a available for one patient with a mosaic ptch1 mutation , which showed that the patient was clinically diagnosed with gorlins syndrome and the patient had no family history of cancer and no family history of gorlins syndrome . 
moreover , comparison of clinical outcomes between patients with germline mutations in sufu and ptch1 showed no differences in progression - free survival ( p = 050 , 16 patients with germline mutations ) and overall survival ( p = 091 , 17 patients with germline mutations )  . 
notably , patients with germline mutations in either sufu or ptch1 had a better overall survival than progression - free survival ( combined 5 - year progressionfree survival 56% for sufu and ptch1 mutations , 95% ci 3787 ; combined 5 - year overall survival 85% , 95% ci 67100 ; figure 3 )  . germline brca2 mutations were present in 11 ( 1% ) of all 1022 patients with medulloblastoma and included ten paediatric patients and one adult ( survival data not available for all patients with these mutations )  . 
clinical signs of a genetic predisposition or family history of cancer were noted in all four compound heterozygous patients and in four ( 80% ) of five heterozygous patients with available medical records . 
patients with compound heterozygous mutations at brca2 developed exclusively mbshh ( p = 00060 when compared with any other subgroup ; figure 2a ) and exhibited worse progression - free survival ( p = 0025 ) and overall survival ( p = 0022 ) relative to patients with heterozygous germline brca2 mutations ( figure 3 )  . 
when compared with 53 105 controls , the burden of rare germline mutations in brca2 was associated with increased risk of mbshh ( relative risk [ rr ] 138 [ 54294 ] ; p < 00001 ) and mbgroup3 / 4 ( rr 42 [ 14101 ] ; p = 00077 )  . 
 additional details about family history of cancer , parental genetic testing , and somatic mutation profiles heterozygous and compound heterozygous brca2 mutation carriers are provided in the appendix ( p 1 )  . germline palb2 mutations were found in five ( < 1% ) of all 1022 patients with medulloblastoma . 
all five damaging germline mutations were heterozygous in patients affected with medullo blastoma and were previously reported in familial pancreatic and breast cancer studies.27 all five germline mutations were classified as pathogenic according to clinvar ( appendix pp 1012 )  . 
log - rank p values indicate differences across all patient groups . adult - onset cancers ( eg , breast cancer ) , predisposition to paediatric malignancies has so far only been described in the context of fanconi anaemia.28 we excluded the predisposition to fanconi anaemia in all five cases because of an absence of additional rare germline mutations ( including protein - truncating variants , missense mutations , and inframe indels )  . 
analysis of vol 19 june 2018 articles b germline apc mutation somatic ctnnb1 mutation somatic monosomy 6 somatic ctnnb1 mutation germline apc mutation * mbwnt mutant cases wild - type cases 76% 894% 833% n = 66 ; p = 092 age at diagnosis ( years ) tp53 sufu ptch1 palb2 brca2 n = 49 signature 1 associated with ageing seen in healthy cells and tumour cells signature 3 associated with hrd seen in breast cancer signature 5 associated with ageing seen in healthy cells and tumour cells signature 8 associated with hrd seen in medulloblastoma and breast cancer patients ( % ) 100% n = 375 brca2 palb2 wild - type brca2 palb2 wild - type brca2 palb2 wild - type brca2 palb2 wild - type figure 4 : molecular medulloblastoma characteristics for patients with a genetic predisposition ( a ) patterns of somatic inactivation of wild - type alleles for all patients with a germline mutation in one of the consensus medulloblastoma predisposition genes . 
 ( b ) somatic driver events in patients with medulloblastoma in the wnt subgroup ( top panel ) and age at diagnosis for all patients with germline apc mutations and patients in the wnt subgroup with somatic ctnnb1 mutations ( bottom panel )  . 
 ( c ) association between germline palb2 ( n = 5 ) and brca2 ( n = 7 ) mutation status and somatic mutational signatures 1 , 3 , 5 , and 8 . 
additional details about family history of cancer , parental genetic testing , and somatic mutation profiles available for one affected patient are presented in the appendix ( p 1 )  . since the clinical relevance of heterozygous germline mutations in palb2 and brca2 is uncertain , we aimed to corroborate our findings through investigation of somatic mutation patterns ( mutational signatures ) in medulloblastoma genomes . 
quantification of four previously implicated mutational signatures ( signatures 1 , 3 , 5 , and 8 ) across 375 medulloblastoma genomes showed a significant association between both hrd signatures ( signatures 3 and 8 ) and germline brca2 and palb2 mutation status ( figure 4c , appendix p 7 )  . 
moreover , although the overall prevalence of an hrd - like mutation spectrum was modest in medulloblastoma ( 58 [ 15% ] of 375 ) , it was enriched in tumours as brca2 - deficient and palb2 - deficient compared with tumours with other genetic mutations ( or 190 [ 95% ci 45113 ] , p < 00001 )  . 
in total , nine ( 75% ) of 12 brca2 - deficient and palb2 - deficient tumours showed evidence for an hrd - like mutation spectru strikingly , eight ( 89% ) of nine patients with mbshh and an hrd - like mutation spectrum harboured germline mutations in consensus medulloblastoma predisposition genes ( brca2 n = 4 , palb2 n = 2 , and tp53 n = 2 ) , suggesting that hrd might serve as a biomarker for genetic predisposition in this patient group . 
we also observed five patients in the mbwnt subgroup with an hrd - like mutation spectrum and noticed that four ( 89% ) of five cases were diagnosed as adults ( p = 00003 for paediatric vs adult cases )  . 
 the only paediatric patient in the mbwnt subgroup with an hrd - like mutation spectrum harboured a pathogenic heterozygous germline mutation in atm along with somatic inactivation of the wild - type atm allele ( appendix pp 1012 )  . 
finally , we also identified heterozygous germline mutations in fanca ( n = 1 ) and fancq ( n = 1 ) in patients with mbgroup3 and mbgroup4 , respectively , and an hrd - like mutation spectru taken together , these results corroborate our genetic findings and indicate that genetic 794 vol 19 june 2018 articles alteration of homologous recom bination genes is associated with an hrd - like mutation spectrum in medul loblastoma . 
our rare variant burden analyses revealed that genetic predisposition has a major role in the cause of medulloblastoma after accounting for molecular subgroups , with a high prevalence in mbwnt and mbshh patient subgroups . 
recommendations for surveillance and clinical management of individual childhood cancer predisposition syndromes have been summarised in a series of articles29 from the american association for cancer research childhood cancer predisposition workshop . 
 our study complements these recommendations by providing additional diagnostic criteria based on clinical and molecular characteristics . the urgent need here , we identified heterozygous germline apc mutations in 68% of patients in the mbwnt molecular subgroup and showed that genetic cases were indistinguishable from sporadic cases based on age at diagnosis . 
 importantly , all patients with apc - deficient mbwnt did not have the hallmark somatic driver event of mbwntnamely , somatic missense mutations in ctnnb1 ( the gene encoding - catenin )  . 
 in our series , patients with mbwnt and germline apc mutations showed favourable clinical outcomes , which mirrors the favourable outcome for patients with mbwnt with nuclear accumulation of - catenin.30 nevertheless , several patients with germline apc mutations had an additional malignancy , which emphasises the need to provide genetic counselling for patients with mbwnt in the future , irrespective of clinical outcomes . 
additional studies will be needed to assess whether or not germline apc mutations are a genetic risk factor for mbshh . given the particularly high prevalence of damaging germline mutations in patients with mbshh , we recommend that all patients with mbshh should be counselled for genetic testing . 
patients younger medulloblastoma subgroup group 3 group 4 genetic testing of family history of brca - associated cancers , or homologous recombination repair deciency , or both genetic testing of absence of somatic ctnnb1 exon 3 mutation prioritisation of genetic testing based on age or genomic instability , or both sufu , ptch1 tp53 , palb2 , and brca2 palb2 and brca2 figure 5 : proposed clinical guidelines for genetic counselling and testing in medulloblastoma based on clinical and molecular tumour characteristics than 3 years of age should initially be tested for germline mutations in sufu and ptch1 ( especially in view of the high prevalence of sufu mutations in infant patients with mbshh in our study , which is consistent with previous reports31 ) , and children older than 3 years for germline tp53 mutations . 
based on these findings we recommend conservative ordering of genetic tests in these patient groups ( eg , those with familial history of brca - associated cancers or mutational signatures are suggestive of hr deficiency specifically signatures 3 and 8 , the latter of which has previously been reported to be associated with breast cancer ) .32 genetic counselling and testing for germline palb2 and brca2 mutations in paediatric patients has so far been pursued only in case of suspected fanconi anaemia . 
 by use of integrative genomic analyses , we showed that heterozygous mutations in brca2 and palb2 are associated with an increased risk of medulloblastoma and of hr - deficient tumours . 
all identified heterozygous germline mutations are rare in the general population ( minor allele frequency < 001% ) and were classified in most patients as ( likely ) pathogenic in clinvar . 
magnusson and colleagues33 reported that families with germline mutations in brca2 had an increased prevalence of vol 19 june 2018 articles childhood tumours compared with population - based control families . 
for example , it was shown that cells from heterozygous palb2 mutation carriers exhibited an aberrant dna replication stress response and increased amounts of spontaneous genomic instability , 34 and analysis of double - strand break repair outcomes35 revealed a shift towards error - prone dna repair pathways . 
 furthermore , one study36 presented evidence showing that naturally occurring concentrations of formaldehyde , a product of cellular metabolism , can selectively deplete brca2 via proteasomal degradation and induce genomic instability . 
moreover , consequent identification of paediatric patients with heterozygous germline mutations in palb2 and brca2 will be valuable to further evaluate whether hr - deficient tumours show a particularly favourable response to standard platinum - based chemotherapy and whether they might benefit from combination therapies with parp inhibitors . germline mutations in tp53 accounted for the highest proportion of genetic cases among paediatric patients in the mbshh subgroup . 
this finding underscores the need for a dedicated treatment protocol , which is being prepared by the international society of paediatric oncology pnet 5 medulloblastoma study group and by an international registry for this high - risk patient group.37 additionally , clinical surveillance of germline tp53 mutation carriers has been shown to result in earlier detection of tumours and therefore improved long - term survival.38 we also observed rare and damaging germline mutations with potential clinical relevance in additional genes based on loss of heterozygosity analysis and somatic mutation patterns ( eg , atm and pten )  . 
a single patient harboured a heterozygous germline msh6 mutation in our discovery cohort ; however , the meaning of this observation remains uncertain owing to the absence of tumour material for molecular analyses . our study does have some limitations . 
because of the multiple ( and in part heterogeneous ) cohorts used in our study , familial history of cancer could not be obtained in a standardised form for all patients carrying a genetic predisposition . 
 larger cohort sizes in further studies will be necessary to assess the impact of germline mutations on clinical outcomes within molecular subgroups as well as relative to patients who develop sporadic medulloblastoma due to somatic mutations in the same set of genes ( eg , ptch1 , sufu , and tp53 )  . 
 furthermore , we note that our rare variant burden analysis against exac was restricted to regions covered by whole - exome sequencing , was restricted to genes previously in cancer predisposition , and excluded pathogenic germline structural variants . 
 although these steps aimed to reduce potential biases from analysing heterogeneous sequencing cohorts , we cannot rule out that particular classes of germline variation might have been under - represented . 
finally , it is also possible that additional genes are involved in medulloblastoma predisposition , which were not previously associated with hereditary cancer syndromes . involved contributors jok , pan , smp , and smw contributed to manuscript preparation and to study design . 
ag , cb , cdb , cpk , crb , cs , dm , fmdlv , kbg , kwp , and sss contributed to data interpretation . declaration of interests smw reports grants from the european molecular biology organization ( embo ) and from the swiss national science foundation , during the conduct of the study . 
mf reports grants from the swedish research council , the swedish council for health , working life and welfare , the swedish cancer society , the swedish childhood cancer foundation , and the swedish radiation protection authority , during the conduct of the study . 
cdb reports grants from the national institutes of health ( nih ) , during the conduct of the study ; grants from the university of miami , financial activities from the university of chicago ; university of california , los angeles ; hugo ; new york genome center ; university of iowa ; rockefeller university ; alexandria ; fh foundation ; concert genetics ; national autonomous university of 796 vol 19 june 2018 articles mexico ; mexican institute of social security ; colorado state university ; macarthur foundation ; and gordon conference ; and personal fees from cdb consulting ltd , personalis , inc , 23andme roots into the future project , ancestry.com , liberty biosecurity , med - tek , identifygenomics llc , mars inc , etalon inc , fish & richardson pc , eden roc , hypatia , the nicklaus childrens hospital research institute , knox medical , arc bio llc , embark veterinary , digitalis ventures , humancode , web shield , and luna dna , outside the submitted work . 
all other authors declare no competing interests . acknowledgments this project was supported by the pedbrain tumor project contributing to the icgc , funded by german cancer aid ( 109252 ) , the german federal ministry of education and research ( bmbf ; 01ku1201a and 01ku1201c ) , and additionally through bmbf grants biotop ( 01ek1502a and 01ek1502b ) , icgc - data mining ( 01ku1505f ) , medsys ( 0315416c ) and ngfnplus ( 01gs0883 )  . 
pan is the recipient of a roman - herzog postdoctoral fellowship ( hertie foundation ) , v foundation v scholar award , sontag foundation distinguished scientist award , and is a pew - stewart scholar for cancer research ( alexander and margaret stewart trust )  . 
mdt is supported by the garron family chair in childhood cancer research , and grants from the cure search foundation , the national institutes of health ( r01ca148699 and r01ca159859 ) , the pediatric brain tumor foundation , the terry fox research institute , and brainchild . 
tissue banking was supported by funds from the faculty of medicine , masaryk university ( brno , czech republic ) and kz was supported by the project azv 15 - 30657a from the ministry of health of the czech republic . 
the medulloblastoma advanced genomics international consortium ( or magic ) project is financially supported by genome canada , genome bc , terry fox research institute , ontario institute for cancer research , pediatric oncology group ontario , funds from the family of kathleen lorette and the clark h smith brain tumour centre , montreal childrens hospital foundation , hospital for sick children : sonia and arthur labatt brain tumour research centre , chief of research fund , cancer genetics program , garron family cancer centre , brain child , mdts garron family endowment , and bc childhood cancer parents association . 
we thank the dkfz genomics and proteomics core facility , andrea wittmann ( pediatric glioma research group , dkfz , heidelberg , germany ) , laura sieber ( division of pediatric neurooncology , dkfz ) , rolf kabbe ( division of theoretical bioinformatics , dkfz ; department for bioinformatics and functional genomics , institute for pharmacy and molecular biotechnology , and bioquant , heidelberg university , heidelberg , germany ) , matthias bieg ( division of theoretical bioinformatics , heidelberg center for personalised oncology , dkfz ) , matthias schlesner ( bioinformatics and omics data analytics , dkfz ) , and bernd klaus ( genome biology unit , european molecular biology laboratory [ embl ] , heidelberg , germany ) for technical support . 
this work is dedicated to prof dr enno kleihauer , who introduced molecular genetics to the field of neuro - oncology in the early 1980s , and who was one of the most influential paediatric haematologist - oncologists in germany and beyond . corrections correction to lancet oncol 2011 ; 12 : 1051 correction to lancet oncol 2015 ; 16 : 634 , 637 histological sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
 independent lancet oncol 2011 ; 12 : 104552 in the discussion of this article , the second sentence of the fth paragraph should read the proportion of patients a ected by grade 34 fatigue in this study ( 7% ) is similar to that reported for trabectedin ( 78% ) or gemcitabine with docetaxel ( 16% ) .12 , 13 this correction has been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 388 kang hj , loftus s , taylor a , dicristina c , green s , zwaan cm . 
 lancet oncol 2015 ; 16 : 38594 in table 2 of the article , the dose ( mg / kg ) of dexamethasone used in the aprepitant group should read 008 ( 002019 )  . 
this correction has been made to the online version as of aug 31 , 2015 . of medical a airs , from april , 2006 , to december , 2012 , during the design and conduct of the stars trial . 
these cor rections have been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 96778 valle jw , wasan h , lopes a , et al . 
lancet oncol 2015 ; 16 : 96778 in gure 3 of the appendix of this article , parts a and b were mislabelled ; part a shows overall survival data and part b shows progression - free survival data . 
the appendix has been corrected as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 1127 moss sm , wale c , smith r , evans a , cuckle h , duffy sw . 
lancet oncol 2015 ; 16 : 112332in the fourth paragraph of the results section of this article , the absolute mortality reduction in the intervention group should read 003 per 1000 womenyears . 
this correction has been made to the online version as of aug 31 , 2015 and the printed version is correct . chang jy , senan s , paul ma , et al . 
lancet oncol 2015 ; 16 : 63037in this article , the role of the funding source should read : this analysis was designed by the principal and coprincipal investigators of both trials . 
for the stars protocol , accuray speci ed that the cyberknife platform was the sole platform to be used for the study , but did not have a role in any other aspect of the study design . 
beyond providing nancial support , neither funder was in accessing involved the raw data , collection , analysis , or interpretation of the data , or writing of the report . 
dab has received grants from accuray , and is the co - owner of berry consultants , a company that designs clinical trials for pharmaceutical and medical device companies , and international healthcare consortia . 
od was an employee of accuray , as senior vice - president responses vol 16 september 2015 e427 corrections correction to lancet oncol 2012 ; 13 : 817 , 818 , 822 correction to lancet oncol 2014 ; 15 : 1195206 correction to lancet oncol 2015 ; 16 : 52 shen q , fan j , yang x - r , et al . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . vol 16 january 2015 correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections corrections correction to lancet oncol 2016 ; 17 : 109 correction to lancet oncol 2016 ; 17 : 248 , 252 du y sw , dibden a , michalopoulos d , et al . 
lancet oncol 2016 ; 17 : 10914in the findings section of the summary of this article , the second sentence should read the average frequency of dcis detected at screening was 160 per 1000 women screened ( median 150 [ unit range 054356 ] per 1000 women )  . 
 addition of docetaxel or bisphosphonates to standard of care in men with localised or metastatic , hormone - sensitive prostate cancer : a systematic review and meta - analyses of aggregate data . 
 lancet oncol 2016 ; 17 : 24356in the results section , the third sentence of the second paragraph should read in the three remaining trials , 7 , 8 , 10 men aged 3691 years ( median 6366 years ) with a good performance status received androgen deprivation therapy - based treatments ( standard of care ) with or without docetaxel . 
 in figure 3 , the text under parts a and c should have read favours soc + bisphosphonate , and the text under parts b and d should have read favours soc + zoledronic acid . 
 these corrections have been made to the online version as of feb 2 , 2016 , and the printed version is correct . vol 17 february 2016 the burden of cancers and their variations across the states of india : the global burden of disease study 19902016 india state - level disease burden initiative cancer collaborators * summary background previous efforts to report estimates of cancer incidence and mortality in india and its different parts include the national cancer registry programme reports , sample registration system cause of death findings , cancer incidence in five continents series , and globocan . 
we present a comprehensive picture of the patterns and time trends of the burden of total cancer and specific cancer types in each state of india estimated as part of the global burden of diseases , injuries , and risk factors study ( gbd ) 2016 because such a systematic compilation is not readily available . methods we used all accessible data from multiple sources , including 42 population - based cancer registries and the nationwide sample registration system of india , to estimate the incidence of 28 types of cancer in every state of india from 1990 to 2016 and the deaths and disability - adjusted life - years ( dalys ) caused by them , as part of gbd 2016 . 
 we present incidence , dalys , and death rates for all cancers together , and the trends of all types of cancers , highlighting the heterogeneity in the burden of specific types of cancers across the states of india . 
we also present the contribution of major risk factors to cancer dalys in india . findings 83% ( 95% uncertainty interval [ ui ] 7986 ) of the total deaths and 50% ( 4655 ) of the total dalys in india in 2016 were due to cancer , which was double the contribution of cancer in 1990 . 
the ten cancers responsible for the highest proportion of cancer dalys in india in 2016 were stomach ( 90% of the total cancer dalys ) , breast ( 82% ) , lung ( 75% ) , lip and oral cavity ( 72% ) , pharynx other than nasopharynx ( 68% ) , colon and rectum ( 58% ) , leukaemia ( 52% ) , cervical ( 52% ) , oesophageal ( 43% ) , and brain and nervous system ( 35% ) cancer . 
among these cancers , the age - standardised incidence rate of breast cancer increased significantly by 407% ( 95% ui 70856 ) from 1990 to 2016 , whereas it decreased for stomach ( 397% ; 343440 ) , lip and oral cavity ( 64% ; 04186 ) , cervical ( 397% ; 265573 ) , and oesophageal cancer ( 312% ; 279349 ) , and leukaemia ( 161% ; 43242 )  . 
we found substantial inter - state heterogeneity in the age - standardised incidence rate of the different types of cancers in 2016 , with a 33 times to 116 times variation for the four most frequent cancers ( lip and oral , breast , lung , and stomach )  . 
tobacco use was the leading risk factor for cancers in india to which the highest proportion ( 109% ) of cancer dalys could be attributed in 2016 . lancet oncol 2018 ; 19 : 1289306 published online september 12 , 2018 s1470 - 2045 ( 18 ) 30447 - 9 see comment page 1260 see online / comment lancet 2018 ; published online sept 12 . 
 s2214 - 109x ( 18 ) 30387 - 5 , s2214 - 109x ( 18 ) 30407 - 8 , and s2214 - 109x ( 18 ) 30409 - 1 see online / articles lancet public health 2018 ; published online sept 12 . 
 s2468 - 2667 ( 18 ) 30138 - 5 * collaborators listed at the end of the article correspondence to : prof lalit dandona , public health foundation of india , gurugram 122002 , national capital region , india lalit.dandona@phfi.org interpretation the substantial heterogeneity in the state - level incidence rate and health loss trends of the different types of cancer in india over this 26 - year period should be taken into account to strengthen infrastructure and human resources for cancer prevention and control at both the national and state levels . 
these efforts should focus on the ten cancers contributing the highest dalys in india , including cancers of the stomach , lung , pharynx other than nasopharynx , colon and rectum , leukaemia , oesophageal , and brain and nervous system , in addition to breast , lip and oral cavity , and cervical cancer , which are currently the focus of screening and early detection programmes . funding bill & melinda gates foundation ; and indian council of medical research , department of health research , ministry of health and family welfare , government of india . copyright the author ( s )  . 
we found a wide variety of valuable data for cancer distribution in india and several states , but no studies that comprehensively described incidence , prevalence , mortality , and disability - adjusted life - years ( dalys ) for all cancer types in every state of india over a long period of time . added value of this study to our knowledge , this is the first report to produce comprehensive estimates of incidence , prevalence , mortality , and dalys for 28 types of cancers in every state of india over 26 years from 1990 to 2016 . 
this analysis was part of the global burden of diseases , injuries , and risk factors study 2016 that assessed all causes of disease burden , using data from all accessible sources . 
this study estimates that while the agestandardised incidence rate of all cancers considered together has not changed substantially in india during this 26 - year period , the proportion of total disease burden caused by cancers has doubled . 
this study reports the substantial heterogeneity in the incidence , mortality , and dalys of different cancers across the states of india and documents that tobacco use is the highest contributing risk to cancer burden in india . implications of all the available evidence this systematic and comprehensive description of the variations in the distribution and trends of cancer types in different parts of the country can serve as a useful reference for further planning of prevention and management of cancer across india . 
more large - scale collaborative research is needed to understand the reasons behind the changing trends of the different types of cancers in india . types of cancers in each state of india is not readily available . 
this is needed to inform action for cancer control that is commensurate with the need in each state , since delivery of health care is a state subject in india . the united nations sustainable development goals target the reduction of premature mortality from non - communicable diseases , which includes cancer , by one - third by 2030 through prevention and treatment.21 the national cancer registry programme in india was established in 1981 to generate data on the magnitude and patterns of cancer through population - based registries.22 , 23 the number of registries has grown under this programme , and other population - based registries have also been started in recent years.22 however , many populous states have no cancer registries yet , and most registries in india are in urban areas , leading to difficulties in assessing population - level cancer burden trends in all parts of the country . the india state - level disease burden initiative is a collaboration with the global burden of diseases , injuries , and risk factors study ( gbd ) to produce subnational disease burden estimates for india . 
this initiative recently reported the variable health transition across the states of india from 1990 to 2016 based on analysis done as part of gbd 2016.4 , 24 here , we report detailed trends of the incidence and health loss due to each type of cancer in every state of india from 1990 to 2016 . methods overview the india state - level disease burden initiative recently reported the overall trends of diseases , injuries , and risk factors from 1990 to 2016 for every state of india.4 , 24 this analysis was done as part of gbd 2016 , which estimated disease burden due to 333 diseases and injuries and 84 risk factors in all age groups using all accessible data from multiple sources . 
the india state - level disease burden initiative was supported by the efforts of several expert groups and a vast network of collaborators to identify and access all available data sources , assess their scope and quality for inclusion , and participate in the analysis and interpretation of the findings . 
the health ministry screening committee at the indian council of medical research and the ethics committee of the public health foundation of india approved the work of this initiative . estimation of cancer burden a detailed description of methods to estimate cancer mortality , incidence , prevalence , and disability - adjusted life - years ( dalys ) , and the analytical approaches used in gbd 2016 have been reported elsewhere , and are summarised in the appendix ( pp 316 ) .1 , 2529 briefly , the major data inputs to determine cancer mortality in india included the nationwide sample registration system ( srs ) cause of death data , the medically certified cause of death data , and 42 population - based cancer registries ( appendix pp 68 )  . 
srs verbal autopsy cause of death data on 455 460 deaths covering the rural and urban populations of every state of india from 2004 to 2013 were included.4 for states with at least one population - based cancer registry , the incidence data were trans formed to mortality by multiplying incidence data with an independently modelled urban or rural mortality - incidence ( mi ) ratio for the respective states . 
 cancer registry data were used as the gold - standard against which other data sources ( srs or medically see online for appendix 1290 vol 19 october 2018 articles substantially sources differed certified cause of death data ) were compared . 
if the from other data the registry data , they were excluded.1 , 30 because of limitations associated with the medically certified cause of death mortality data , these were used only when the cancer type was not captured by the srs cause of death data . 
 the codcorrect algorithm was used to adjust cancer subtypes to the parent cause and to adjust the sum of predicted deaths from these models for each type of cancers in an agesexstateyear group to be consistent with the results from all - cause mortality estimation . the estimation of cancer incidence was driven by registry data from india . 
the mortality estimates that were derived from transformation of incidence data using the mi ratios , as noted above , were transformed back to incidence after the codem and codcorrect model adjustments.1 10 - year cancer prevalence was estimated by modelling survival using the mi ratio as a surrogate for access to cancer care . 
lifetime prevalence was only estimated for 10 years post incidence1 and for long - term sequelae from procedures ( mastectomy , laryngectomy , stoma , incontinence cystectomy , and prostatectomy )  . 
dalys , a summary measure of total health loss , were computed by adding ylls and ylds for each cancer type for location , year , age and sex.1 , 28 the appendix provides a list of data inputs used for these estimations ( pp 1729 )  . a description of estimation of risk factor exposure and its contribution to disease burden in gbd is available elsewhere.29 briefly , this includes determination of risk exposure and disease outcome pairs based on available evidence and inclusion criteria , assessment of risk exposure from all accessible data sources , and estimation of disease burden attributable to risks based on published relative risks . 
estimates of dalys for specific types of cancers that were attributable to each risk factor were produced by location , age , sex , and year . gbd uses covariates , which are explanatory variables that have a known association with the outcome of interest , to arrive at the best possible estimate of the outcome of interest when data for the outcome are scarce but data for the covariates are available.2529 this approach was part of the estimation process for the findings presented in this report . analysis presented in this paper the findings are reported for 31 geographical units in india : 29 states , union territory of delhi , and the union territories other than delhi ( combining the six smaller union territories of andaman and nicobar islands , chandigarh , dadra and nagar haveli , daman and diu , lakshadweep , and puducherry )  . 
for trends from 1990 onwards , the data for these four new states were disaggregated from their parent states on the basis of data from the districts that now constitute these states . 
 the findings are also presented for four groups of states based on epidemiological transition level ( etl ) as described previously.4 briefly , the etl state groups were defined on the basis of the ratio of dalys from communicable , maternal , neonatal and nutritional diseases to those from non - communicable diseases and injuries combined in 2016 , with a relatively lower ratio indicating higher etl : level etl state group ( ratio 056075 ) , lower - middle etl state group ( 041055 ) , higher - middle etl state group ( 031040 ) , and high etl state group ( less than 031 )  . 
we have reported previously that epidemiological transition ratios of the states of india have a significant inverse relation with the socio - demographic index calculated by the gbd study and based on income , education , and fertility levels , which indicates broad correspondence of etl groups with sociodemographic development levels.4 low we present trends of incidence ( new cases in a year ) , mortality , and dalys due to all cancers together and different types of cancers from 1990 to 2016 for every state of india . 
we regarded dalys as the main metric for disease burden because it includes both mortality and morbidity and is recommended by the national health policy of india for tracking disease burden.31 first , we present the 1990 to 2016 trends for the overall burden from all cancers together in terms of dalys , followed by incidence and deaths . 
we also describe briefly another six cancer types that are among the ten leading incident cancers in females or males in india in 2016 , which are not included in the previous ten cancers causing the highest dalys . 
 we present both crude and age - standardised rates , since crude rates provide the actual situation in each state that vol 19 october 2018 1291 articles 1990 jammu and kashmir ( 691 ) punjab ( 580 ) haryana ( 710 ) himachal pradesh ( 698 ) uttarakhand ( 693 ) delhi ( 646 ) sikkim ( 678 ) arunachal pradesh ( 759 ) rajasthan ( 588 ) uttar pradesh ( 720 ) bihar ( 449 ) assam ( 687 ) nagaland ( 631 ) manipur ( 481 ) mizoram ( 891 ) jharkhand ( 580 ) odisha ( 686 ) meghalaya ( 690 ) tripura ( 529 ) west bengal ( 639 ) chhattisgarh ( 588 ) incidence rate per 100 000 105 901049 75899 60749 45599 449 himachal pradesh ( 916 ) uttarakhand ( 910 ) delhi ( 1029 ) sikkim ( 744 ) arunachal pradesh ( 785 ) rajasthan ( 726 ) uttar pradesh ( 790 ) bihar ( 539 ) assam ( 902 ) nagaland ( 703 ) manipur ( 643 ) mizoram ( 1217 ) jharkhand ( 643 ) odisha ( 836 ) meghalaya ( 814 ) tripura ( 690 ) west bengal ( 854 ) chhattisgarh ( 820 ) gujarat ( 555 ) madhya pradesh ( 694 ) maharashtra ( 620 ) karnataka ( 762 ) telangana ( 549 ) andhra pradesh ( 581 ) ( 525 ) tamil nadu ( 589 ) kerala ( 741 ) 2016 punjab ( 855 ) haryana ( 1033 ) jammu and kashmir ( 792 ) gujarat ( 758 ) madhya pradesh ( 831 ) maharashtra ( 802 ) telangana ( 726 ) andhra pradesh ( 766 ) goa ( 970 ) karnataka ( 1016 ) tamil nadu ( 829 ) kerala ( 1353 ) is preferred by policy makers , and age - standardised rates allow comparisons over time and between states after adjusting for the differences in the age structure of the population . 
 these were based on 1000 runs of the models for each quantity of interest , with the mean considered as the point estimate and the 25th and 975th percentiles considered as the 95% ui ( appendix p 15 ) .2528 role of the funding source some staff of the indian council of medical research are co - authors on this paper as they contributed to various aspects of the study and analysis . 
 the corresponding author had full access to all of the data in the study and had final responsibility for the decision to submit for publication . results all cancers together contributed 50% ( 95% ui 4655 ) of the total dalys and 83% ( 7986 ) of the total deaths in india in 2016 , an increase of 909% and 1128% respectively from 1990 . 
the crude cancer daly rate in india increased by 253% ( 168342 ) from 1990 to 2016 , but the age - standardised cancer daly rate did not change substantially during the same period.32 the agestandardised cancer daly rate had a 26 times variation across the states of india in 2016 ( appendix p 30 )  . 
the highest crude cancer daly rates in 2016 were in the states of mizoram , kerala , assam , haryana , and meghalaya , and the highest age - standardised rates were in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam ( appendix p 30 )  . to 1 069 000 ( 1 043 0001 101 000 ) the estimated number of incident cancer cases in india increased from 548 000 ( 95% ui 520 000576 000 ) in 1990 in 2016 ( appendix p 31 )  . 
the crude cancer incidence rate in india increased by 282% ( 95% ui 199355 ) from 634 per 100 000 in 1990 to 812 per 100 000 in 2016 , but there was no change in the age - standardised incidence rate ( appendix p 32 )  . 
crude cancer incidence rate was highest in kerala and mizoram , followed by haryana , delhi , karnataka , goa , himachal pradesh , uttarakhand , and assam ( figure 1 , appendix p 30 )  . 
age - standardised incidence rates were highest in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam , figure 1 : crude annual incidence rate of all cancers together in the states of india , 1990 and 2016 the states of chhattisgarh , jharkhand , telangana , and uttarakhand did not exist in 1990 , as they were created from existing larger states in 2000 or later . 
crude cancer incidence rate increased substantially from 1990 to 2016 in all etl state groups , with the highest increase in the high etl group ( appendix p 32 )  . the number of deaths due to cancer in india increased from 382 000 ( 95% ui 351 000412 000 ) in 1990 to 813 000 ( 767 000850 000 ) in 2016 ( appendix p 31 )  . 
the crude cancer death rate in india in 2016 was 618 ( 95% ui 583646 ) per 100 000 , as compared with 442 ( 406477 ) in 1990 ( appendix p 32 )  . 
male cancer patients had a 123% ( 95% ui 29233 ) increase in agestandardised death rate over the 26 - year time period , whereas no substantial changes over time were found in female cancer patients ( appendix p 32 )  . 
the crude death rate for both sexes combined was highest in mizoram , kerala , and haryana in 2016 , followed by assam , karnataka , odisha , uttarakhand , meghalaya , and himachal pradesh ( appendix pp 30 , 33 )  . 
the agestandardised death rates were highest in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam ( appendix p 30 )  . the crude cancer mi ratio in india in 2016 was 076 ( 95% ui 072079 )  . 
the mi ratio was higher in low and lower - middle etl state groups than the high and higher - middle etl groups in 2016 ( figure 2 )  . 
the mi ratio for males was more than 080 in all states from the low etl group and most of the lower - middle etl states , with a higher ratio in odisha in low etl , and mizoram and arunachal pradesh in the lower - middle etl state group in 2016 . 
the mi ratio was below 080 for females in most of the states in india in 2016 , except for bihar and meghalaya . the leading types of cancer in india in 2016 , those responsible for more than 5% of the total cancer dalys among both sexes combined , were stomach cancer ( 90% ) , breast cancer ( 82% ) , lung cancer ( 75% ) , lip and oral cavity cancer ( 72% ) , pharynx cancer other than nasopharynx ( 68% ) , colon and rectum cancer ( 58% ) , leukaemia ( 52% ) , and cervical cancer ( 52% ; figure 3 )  . 
the age - standardised daly rate increased significantly in india from 1990 to 2016 for liver cancer ( 512% ; 95% ui 240659 ) , non - hodgkin lymphoma ( 354% ; 207488 ) , ovarian cancer ( 281% ; 151443 ) and myeloma ( 282% ; 56631 )  . 
 age - standardised daly rates from 1990 to 2016 was highest for testicular cancer ( 592% ; 538654 ) and hodgkins lymphoma ( 548% ; 396625 ) , followed by cervical ( 387% ; 230563 ) , nasopharynx ( 335% ; 198461 ) , larynx ( 316% ; 257367 ) , uterine ( 315% ; 178400 ) , and stomach cancer ( 314% ; 237373 )  . 
the highest cancer dalys among males in india in 2016 were due to lung cancer , followed by lip and oral cavity cancer , other pharynx cancer , and stomach cancer ( figure 3 )  . among both boys and girls aged 014 years , leukaemia was responsible for the highest dalys in india in 2016 , followed by brain and nervous system cancer ( figure 5 , appendix pp 3440 )  . 
daly rates for lung cancer and stomach cancer increased in males after the age of 35 years in 2016 , while prostate cancer increased after the age of 50 years . tobacco use , alcohol use , and dietary risks were estimated by gbd to contribute the highest cancer dalys in 2016 ; they were responsible for 109% , 66% and 60% of the total cancer dalys , respectively ( appendix pp 4142 )  . stomach cancer the estimated number of incident stomach cancer cases in india in 2016 was 75 000 ( 95% ui 73 00078 000 ) and the prevalent cases were 112 000 ( 109 000116 000 ; appendix p 31 )  . 
there was a substantial reduction in the age - standardised incidence rate of stomach cancer ( 397% ; 95% ui 343440 ) from 1990 to 2016 in india ( figure 6 )  . 
in 2016 , stomach cancer was the first or second highest cause of cancer deaths in 15 states for females and in 18 states for males ( figure 8 )  . 
only a small proportion of the stomach cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( dietary risks [ 41% ] and smoking [ 35% ] ; appendix pp 4142 )  . breast cancer the estimated number of incident breast cancer cases in india in 2016 was 118 000 ( 95% ui 107 000130 000 ) , 981% of which were in females , and the prevalent cases were 526 000 ( 474 000574 000 ; appendix p 31 )  . 
breast cancer is the leading cancer in indian females , accounting for the largest crude incidence rate and prevalence of any cancer type ( appendix pp 49 , 50 )  . 
over the 26 - year period , the agestandardised incidence rate of breast cancer in females increased by 391% ( 95% ui 51855 ) from 1990 to 2016 , with increase observed in every state of the country ( appendix pp 51 )  . 
the highest crude daly rates for breast cancer were in kerala , punjab , and tamil nadu in the high etl state group , followed by delhi , maharashtra , karnataka , and haryana in the higher - middle etl group . 
only a small proportion of breast cancer dalys in india in 2016 could be attributed to risk factors included [ 49% ] and in gbd ( high fasting plasma glucose secondhand smoke [ 24% ] ; appendix pp 4142 )  . lung cancer we refer to tracheal , bronchus , and lung cancer as lung cancer in this report for simplicity . 
the number of vol 19 october 2018 1295 articles a females b males 8000 7000 6000 5000 4000 3000 2000 1000 8000 7000 6000 5000 4000 3000 2000 1000 bladder cancer brain and nervous system cancer breast cancer cervical cancer colon and rectum cancer gallbladder and biliary tract cancer hodgkins lymphoma kidney cancer larynx cancer leukaemia lip and oral cavity cancer liver cancer lung cancer malignant skin melanoma mesothelioma multiple myeloma nasopharynx cancer non - hodgkin lymphoma non - melanoma skin cancer oesophageal cancer pharynx cancer other than nasopharynx ovarian cancer pancreatic cancer stomach cancer thyroid cancer uterine cancer bladder cancer brain and nervous system cancer breast cancer colon and rectum cancer gallbladder and biliary tract cancer hodgkins lymphoma kidney cancer larynx cancer leukaemia lip and oral cavity cancer liver cancer lung cancer malignant skin melanoma mesothelioma multiple myeloma nasopharynx cancer non - hodgkin lymphoma non - melanoma skin cancer oesophageal cancer pharynx cancer other than nasopharynx pancreatic cancer prostate cancer stomach cancer testicular cancer thyroid cancer 1014 1519 2024 2529 3034 3539 4044 4549 5054 5559 6064 6569 7074 7579 age range ( years ) figure 5 : age - specific dalys for different types of cancers by sex in india , 2016 dalys = disability - adjusted life - years . incident lung cancer cases in india in 2016 was 67 000 ( 95% ui 63 00072 000 ) , 722% of which were in males , and the prevalent cases were 74 000 ( 70 00080 000 ; appendix p 31 )  . 
the crude lung cancer incidence rate in males was highest in kerala and mizoram , and in females was highest in mizoram and manipur ( appendix pp 49 , 50 )  . 
there was a substantial reduction in the age - standardised incidence rate of lip and oral cavity cancer ( 64% ; 95% ui 04186 ) from 1990 to 2016 in india ( figure 6 )  . 
the age - standardised incidence rate for lip and oral cavity cancer varied 51 times among both sexes combined across the states of india in 2016 ( appendix pp 4348 )  . 
smokeless tobacco , alcohol use and smoking were the leading risk factors in gbd for lip and oral cavity cancer in india in 2016 to which 332% , 298% , and 209% of the lip and oral cavity cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . pharynx cancer other than nasopharynx the number of incident pharynx cancer other than nasopharynx cases in india in 2016 was 65 000 ( 95% ui 58 00070 000 ) , 702% of which were in males , and the prevalent cases were 152 000 ( 137 000163 000 ; appendix p 31 )  . 
the age - standardised incidence rate for other pharynx cancer varied 98 times for both sexes combined across the states of india in 2016 ( appendix pp 4348 )  . 
alcohol use was the leading risk factor in gbd for other pharynx cancer in india in 2016 to which 30.1% of the other pharynx cancer dalys could be attributed ( appendix pp 41 , 42 )  . colon and rectum cancer the number of incident colon and rectum cancer cases in india in 2016 was 63 000 ( 95% ui 58 00066 000 ) and the prevalent cases were 185 000 ( 171 000195 000 ; appendix p 31 )  . 
colon and rectum cancer incidence rate in both sexes was higher in the high etl as compared with other etl state groups ( appendix pp 49 , 50 )  . 
dietary risks were the leading risk factor in gbd for colon and rectum cancer in india in 2016 to which 432% of the colon and rectum cancer dalys could be attributed ( appendix pp 41 , 42 )  . leukaemia the number of incident leukaemia cancer cases in india in 2016 was 34 000 ( 95% ui 30 00038 000 ) and the prevalent cases were 105 000 ( 96 000120 000 ; appendix p 31 )  . 
among children aged 014 years , leukaemia was responsible for the highest proportion of the cancer dalys ( 346% ) in india in 2016 , which was similar among boys and girls ( figure 5 , appendix pp 3440 )  . 
in males , leukaemia was the third and fifth leading cause of cancer deaths in delhi and punjab respectively in 2016 , but lower in other states ( figure 8 )  . cervical cancer cervical cancer was the second most common cancer in females in india in 2016 , with 77 000 ( 95% ui 68 00096 000 ) incident cervical cancer cases in india in 2016 and 288 000 ( 247 000342 000 ) prevalent cases ( appendix p 31 )  . 
it is important to note that other unknown risk factors could also be contributing to cervical cancer as the population - attributable fractions of different risks can add up to more than 100% . vol 19 october 2018 1299 articles for rate cancer oesophageal oesophageal cancer the number of incident oesophageal cancer cases in india in 2016 was 37 000 ( 95% ui 36 00038 000 ) , 608% of which were in males , and the prevalent cases were 41 000 ( 39 00042 000 ) ( appendix p 31 )  . 
there was a substantial reduction in the age - standardised incidence rate of oesophageal cancer ( 312% ; 95% ui 279349 ) in india from 1990 to 2016 ( figure 6 )  . 
smokeless tobacco , dietary risks , and smoking were the leading risk factors in gbd for oesophageal cancer in india in 2016 to which 226% , 215% , and 174% of the oesophageal cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . brain and nervous system cancer the number of incident brain and nervous system cancer cases in india in 2016 was 23 000 ( 95% ui 21 00028 000 ) and the prevalent cases were 49 000 ( 44 00057 000 ; appendix p 31 )  . 
among children aged 014 years , brain and nervous system cancer was responsible for the second highest proportion of the cancer dalys ( 16% ) in india in 2016 , which was similar among boys and girls ( figure 5 , appendix pp 3440 )  . 
the daly rate for brain and nervous system cancer was highest in delhi followed by sikki the ranking of deaths due to brain and nervous system cancer was relatively low in all states as compared with the other high burden cancers ( figure 8 )  . 
 prostate cancer prostate cancer had the fifth highest incidence rate among males in india in 2016 ( 48 per 100 000 , 95% ui 3858 ) , with 33 000 ( 26 00040 000 ) incident cases and 112 000 ( 87 000137 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
there were 31 000 ( 95% ui 30 00033 000 ) incident cases in india , of which 835% were in males , and there were 96 000 ( 93 000100 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
the crude incidence rate for larynx cancer in males was highest in kerala in 2016 , followed by delhi , haryana , and assam ( appendix p 50 )  . 
smoking and alcohol use were the leading risk factors in gbd for larynx cancer in india in 2016 to which 379% and 172% of the larynx cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . liver cancer liver cancer had the ninth highest incidence rate among males in 2016 in india ( 31 per 100 000 , 95% ui 29 32 )  . 
 there were 30 000 ( 95% ui 29 00032 000 ) incident cases in india , of which 689% were in males , and 12 000 ( 11 00014 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
the crude incidence rate for liver cancer in males in 2016 was highest in arunachal pradesh , followed by kerala , sikkim , and mizoram ( appendix p 50 )  . 
 to 2016 the sixth highest ovarian cancer ovarian cancer had incidence rate among females in 2016 in india ( 40 per 100 000 , 95% ui 3743 ) , with 26 000 ( 95% ui 24 00027 000 ) incident cases and 76 000 ( 69 00080 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
only a small proportion of the ovarian cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( high fasting plasma glucose [ 55% ] ; appendix pp 41 , 42 )  . gallbladder and biliary tract cancer gallbladder and biliary tract cancer had the ninth highest incidence rate among females in 2016 in india ( 26 per 100 000 , 95% ui 2328 )  . 
there were 26 000 ( 95% ui 23 00029 000 ) incident cases in india , of which 644% were in females , and there were 21 000 ( 18 00023 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
the crude incidence of gallbladder and biliary tract cancer in females 1300 vol 19 october 2018 articles was highest in the states of assam and delhi in 2016 ( appendix p 49 )  . 
91% of the gallbladder and biliary tract cancer dalys in india in 2016 could be attributed to high body - mass index in gbd ( appendix pp 41 , 42 )  . thyroid cancer thyroid cancer had the tenth highest incidence rate among females in 2016 in india ( 25 per 100 000 , 95% ui 2326 )  . 
there were 21 000 ( 95% ui 20 00023 000 ) incident cases in india , of which 743% were in females , and there were 106 000 ( 101 000115 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
the crude incidence rate of thyroid cancer was highest in females in kerala , followed by sikkim , nagaland , and goa in 2016 ( appendix p 49 )  . 
 only a small proportion of the thyroid cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( high body - mass index [ 51% ] ; appendix pp 41 , 42 )  . discussion the number of new cases and deaths due to cancer doubled in india from 1990 to 2016 , as did the proportional contribution of cancers to the total dalys and deaths in the country . 
however , there was no change in the age - standardised rates for both sexes combined , highlighting the contribution of ageing and population growth to the increasing cancer burden of the country . 
 males had higher mi ratios than females in every state of the country . the trends observed in sex - specific and cancer typespecific incidence rates over time in india are likely due to a variety of factors , such as population ageing , changes in cancer literacy , detection , health - care access , and a variety of risk factors . 
the substantial decrease in the age - standardised incidence rate of stomach cancer across the country might be due to lifestyle changes such as reduced consumption of salt - preserved foods , better availability of refrigeration , and increasing fruit con sumption , and to decreases in smoking prevalence.3234 the prevalence of helicobacter pylori remains persistently high in indians , 35 and hence this is an unlikely factor in the decreasing incidence of stomach cancer . 
for breast cancer , a substantial increase in age - standardised incidence rate is consistent with changes in some risk factors over time in india , such as later age at first birth , lower parity , and increase in overweight and obesity.32 , 36 , 37 the substantial decrease in the age - standardised incidence rate of oesophageal cancer might be partly due to the decrease in smoking prevalence over the 26 - year period and in smokeless tobacco use over the past 10 years.32 , 34 the absence of change in the age - standardised incidence rate of lung cancer in india might be related to the mixed trends of its major risk factors , which include decrease in smoking and household air pollution but an increase in ambient air pollution , but also due to the patterns of other unknown risk factors.32 , 34 the small decrease in the age - standardised incidence rate of lip and oral cavity cancer in india could be related to the reduction in use of smokeless tobacco in india during the past decade.32 the decreasing age - standardised incidence rate of cervical cancer could be inversely related to the reproductive risk factors mentioned for breast cancer increase above.36 in the absence of systematic human papilloma virus ( hpv ) testing in india , there is no evidence of changing seroprevalence of hpv and its subtypes over time in india . 
leukaemia has been associated with genetic , infectious , and environmental risks , 38 but the reasons for the substantial reduction in its age - standardised incidence rate in india from 1990 to 2016 are unclear . the interplay of the trends of the two risk factors to which the highest proportion of cancer dalys in india could be attributed , tobacco and alcohol , is interesting in relation to the trends of some of the leading cancers . 
while tobacco use in india has decreased during this period , alcohol use has increased.32 the drop in incidence rate of lip and oral cavity , oesophageal , and larynx cancers could be partly related to a larger influence of tobacco than alcohol on these cancers , and the increase in incidence rate of liver cancer could be partly related to a larger influence of alcohol than tobacco on this cancer , in addition to the trends of yet unknown other risk factors contributing to all of these cancers . 
collaborative multi - institutional research efforts on cancer risk factors can help address such knowledge gaps , as well as lead to a better understanding of the reasons for the substantial decreases or increases in the incidence of different types of cancers in different parts of india . 
detailed decomposition analyses are needed to tease apart the contribution of population structure changes , risk factors , interventions , and other determinants to the trends of leading cancers in india . the heterogeneity of the incidence rate of different types of cancers across india is vast . 
major variations exist even within the same geographical region , such as neighbouring states in the northeastfor example , a 15 times difference in age - standardised incidence rates of naso pharynx cancer between the neighbouring north - eastern states of nagaland and tripura . 
the states in the northeast of vol 19 october 2018 1301 articles india generally have high tobacco use as well as a high incidence of lung , oesophageal , nasopharynx and other pharynx cancers that are associated with tobacco use . 
 there are also unique tobacco consumption patterns in these states , such as use of tobacco - infused water in mizoram.39 , 40 hpv and cervical cancer are both high in dindigul in tamil nadu , 41 consumption of smoked or preserved meats and stomach cancer are high in mizoram , 42 and delayed childbearing and lower parity are high in kerala as is breast cancer.43 the many variations between the states indicate the need for state - specific approaches for cancer control . 
if the reasons for the heterogeneous distribution of the major cancer types in different parts of india are understood better through large - scale collaborative research , this knowledge could help plan more specific efforts to reduce the cancer burden across the states of india . the national cancer control programme was initiated by the government of india in 1975 to equip tertiary care cancer hospitals and institutions to implement systematic , equitable , and evidence - based strategies for prevention , early detection , diagnosis , treatment , and palliation , using available resources.44 state cancer institutes and tertiary care cancer centres have been established under this programme that are responsible for improved cancer awareness and management at the state level.45 despite these attempts , access to critical cancer treatment is low in the country . 
for example , availability of radiotherapy machines is poor , there are delays in treatment , and there is geographic inequity in the distribution of such resources.10 , 11 , 46 with the launch of the national programme for control of cancer , diabetes , cvd and stroke in 2010 in india , the cancer control efforts are now part of this umbrella programme for noncommunicable diseases.47 the national programme aims to tackle cancer by addressing preventable common risk factors through community - level , cost - effective screening for high - burden cancers , which include clinical breast examination for breast cancer , visual inspection with acetic acid for cervical cancer and visual examination for oral cancers.14 however , there are many challenges with these efforts , including difficulties with trained human resources , follow - up of positive tests , timely diagnosis , and well - tracked referral pathways.48 additionally , there are limited population - level screening modalities available for some of the cancers responsible for the highest cancer burden in india , such as stomach and lung cancers . 
for secondary prevention , less invasive tests for h pylori may offer cost - effective first - line tests for referrals to more invasive endoscopic tests for early detection of stomach cancer.49 faecal occult blood testing as a non - invasive , cost - effective approach to screen for colorectal cancer should also be considered.50 ideally , national and state - level efforts should coordinate to facilitate the development of a prevention - to - palliation system of upward referral for early confirmatory diagnosis and prompt treatment of cancers , and downward referral for adequate follow - up , including palliative care and pain relief . 
india pioneered the establishment and expansion of the national cancer registry programme ( ncrp ) under the indian council of medical research through a network of cancer registries during the past 30 years , which now covers 23 states and union territories.23 the gbd methods rely substantially on the ncrp data from india , but they also use data from all accessible data sources , including some registries that are not part of the ncrp , cause of death data from the 1302 vol 19 october 2018 articles srs and other sources , and a variety of covariates to arrive at the best possible estimates for states where registries do not exist . 
accordingly , differences are expected between the gbd estimates and the statistics reported by the ncrp , which are based entirely on population - based registries.23 the objectives and advantages of the gbd and ncrp approaches are complementary . 
while the ncrp adheres to a standardised methodology established by whos international agency for research in cancer , the gbd methodology provides a standardised approach that also incorporates other sources of data for estimations for all states of india , including those where registries do not exist such as the populous states of bihar , chhattisgarh , jharkhand , and uttar pradesh . 
the gbd methodology is integrated into a larger total disease framework estimation process that allows comparison of the cancer burden to that of other diseases , which has helped to highlight the increasing contribution of cancers to the disease burden in india over the past quarter century . 
it has also further highlighted the need to establish cancer registries in large states of north india where none exist , as well as adequate coverage of rural populations . the limitations of the findings in this report include the general limitations of the gbd approach that are described elsewhere.1 , 2528 input data used to generate cancer mortality can be biased in multiple ways.1 a high proportion of ill - defined cancer cases in the registry data or ill - defined causes of death in mortality data sources require redistribution of these cases , which can introduce bias . 
underreporting of cancers that require advanced diagnostic techniques ( eg , leukaemia , brain , pancreatic , and liver cancer ) can be an issue in data from areas where access to these technologies is scarce . 
in addition , risk factors for breast and cervical cancer that are related to reproductive history in women , such as age at first birth and parity , are not yet included in the gbd risk factor assessment . 
a specific limitation for india is an inadequate cause of death reporting as part of the vital registration system , which reports medically certified cause of death only for a small proportion of deaths in india so far , with variable coverage across the states . 
the srs provides cause of death data using verbal autopsy for all states in india , which is a reasonable alternative data source when the cause - specific data are not fully available from vital registration systems.4 however , this situation highlights the need to improve vital registration and improve training to code cause of death across india . 
the absence of population - based registries in major populous states of north india such as bihar and uttar pradesh leaves open questions about the magnitude of some cancers such as gallbladder cancer , which are expected by the india cancer community to be high there , but this cannot be substantiated yet because of the paucity of population - level evidence . 
in cancer datascarce locations , the estimates for the types of cancer were calculated using covariates , which are explanatory variables with a causal relation to cancer incidence and mortality.1 the strengths of the findings presented in this report were the use of standardised gbd methodology and inclusion of all accessible data from multiple sources , and the substantial contribution of a large network of cancer experts from india in the analysis and inter pretation of the findings . in conclusion , the detailed epidemiology of 28 types of cancer in every state of india over a quarter century described the substantial this report highlights variations between the states for the different types of cancer , and can serve as a useful reference for more targeted planning of cancer control that is commensurate with the trends of different cancers in each state of india . 
 the increasing overall contribution of cancer to disease burden in india should motivate more systematic and large - scale approaches to reduce this burden at the population level across the country . 
these efforts should include improved human resources and infrastructure for prevention , screening , treatment , and palliative care for cancers , as well as adequate financial protection for cancer care . 
these approaches should focus at least on the ten cancers that contribute the highest dalys in indiaie , stomach , breast , lung , lip and oral cavity , pharynx other than nasopharynx , colon and rectum , leukaemia , cervical , oesophageal , and brain and nervous system cancers . 
all authors agreed with the final version of the report . declaration of interests pma , an , rm , dks , rsd , tk , rnv , jkc , mc , pd , jm , sp , ksa , kv , and ss are or have been employees of the indian council of medical research , which partly funded this research . 
all other authors declare no competing interests . acknowledgments the research reported in this publication was funded by the bill & melinda gates foundation and the indian council of medical research , department of health research , government of india . 
 the content of this publication is solely the responsibility of the authors and does not necessarily represent the official views of the bill & melinda gates foundation or the government of india . 
 we gratefully acknowledge the ministry of health and family welfare of the government of india for its support and encouragement of the india state - level disease burden initiative , the governments of the states of india for their support of this work , the many institutions across india that contributed valuable data to the national cancer registry programme and to the other cancer registries , the valuable guidance of the advisory board of this initiative , and the large number of staff at the indian council of medical research , public health foundation of india and the institute for health metrics and evaluation for their contribution to various aspects of the work of this initiative . corrections published online june 25 , 2015 s1470 - 2045 ( 15 ) 00119 - 9 correction to lancet oncol 2011 ; 12 : 625 for research baan r , grosse y , lauby - secretan b , et al , on behalf of the who international on cancer agency working monograph group . 
lancet oncol 2011 ; 12 : 62426 the con ict of interest statement for n kuster should read : nk is director and board member of the non - pro t itis foundation that performs research in the eld of exposure assessments for academia , governments , and industry . 
itis has received funding for speci c projects from most mobile phone manufacturers and many service providers , including the mobile manufacturers forum , motorola , ericsson , nokia , samsung , sony , gsm association , arib japan , swisscom , deutsche telekom , and tdc sunrise . 
 nk is president of the board and shareholder of nf technology holding ag , which controls two companies , schmid & partner engineering ag and zmt zurich medtech ag , that develop neareld measurement instruments , simulation software , and medical test equipment . 
this correction has been made to the online version as of june 25 , 2015 . vol 16 august 2015 e379 correction to lancet oncol 2016 ; 17 : 159098 sharma p , callahan mk , bono p , et al . 
 nivolumab monotherapy in recurrent metastatic urothelial carcinoma ( checkmate 032 ) : a multicentre , openlabel , two - stage , multi - arm , phase 1 / 2 trial . 
lancet oncol 2016 ; 17 : 159098 in this article , the declaration of interests should read psh has received fees for advisory board participation for jounce and kite ; fees for consultancy from jounce , kite , bristol - myers squibb , astrazeneca , and amgen ; and stock or stock options from jounce and kite . 
eca reports research grants and / or financial support from boehringer ingelheim , roche / genentech , bristol - myers squibb , novartis , psioxus , nanobiotix janssen , abbvie , pharmamar , puma , sanofi , lilly , pfizer , merck , nektar , amcure , amgen , astrazeneca , principia , bayer , cytomx , h3 , incyte , kura , loxo , macrogenics , menarini , merck serono , merus , millenium , rigontec , tahio , and beugene tesaro ; consultancy fees from janssen - cilag , alkermes ( and travel expenses ) , seattle genetics , pierre fabre , cerulean pharma , eusa , celgene , novartis ( speakers bureau ) , nanobiotix , psioxus therapeutics , abbvie , astrazeneca , guidepoint global , roche / genentech ( and travel expeneses ) , glg , pfizer , servier , amcure , and boehringer ingelheim ; ownership from start ( leadership ) , oncoarts associated and international cancer consultants ; and employment from start and hm hospitals group ( honoraria ) and president and founder of npo foundation intheos ( investigational therapeutics oncological sciences ) , outside the submitted work . 
fdb has received consultancy fees from tiziana life sciences , bristol - myers squibb , msd , servier , eli lilly , merck serono , glaxosmithkline , and novartis , and speaker fees from bristol - myers squibb , eli lilly , roche , and accmed . 
mm has received consultancy fees from etubics and boehringer ingelheim , and speaker fees from genentech , novartis , sanofi , regeneron , lexicon , ipsen , onyx , bayer , taiho , merrimack , and celgene . 
 dj has received consulting fees from definiens , f hoffmann - la roche , curevac , roche pharma , novartis pharma , and novartis oncologynovartis farma , outside the submitted work ; and has a patent issued for intellectual property of infiltrating t - cell density predicting outcome . 
 ech has received grants from bristolmyers squibb and consultancy fees for advisory board participation from emd serono , taiho , bayer , advaxis , amgen , lilly , and castle biosciences . 
jer has received grants for study conduct from novartis ; funds for clinical trial conduct from astellas , seattle genetics , bayer , astrazeneca , mirati therapeutics , oncogenex , and roche / genentech ; has received consultancy fees from roche / genentech , astrazeneca , eli lilly , astellas , seattle genetics , bristol - myers squibb , merck , emd - serono , adicet bio , western oncolytics , pharmacyclics , sensei biotherapeutics , bayer , bioclin therapeutics , qed therapeutics , mirati therapeutics , fortress biotech , inovio ; has gritstone oncology , received honoraria from bristol - myers squibb and chugai ; has held stock in illumina and merck . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2017 ; 18 : 90416 baselga j , im s - a , iwata h , et al . 
buparlisib plus fulvestrant versus placebo plus fulvestrant in postmenopausal , hormone receptor - positive , her2 - negative , advanced breast cancer ( belle - 2 ) : a randomised , double - blind , placebocontrolled , phase 3 trial . 
lancet oncol 2017 ; 18 : 90416in this article , the declaration of interests should read jb has received reimbursement for travel , and advisory board and consulting fees from novartis , during the conduct of the study ; has received personal fees and held stock as a member of the board of directors from aura biosciences ; has received personal fees as a member of the advisory board and held stock as a founder of northern biologics ( f / k / a mosaic biomedicals ) ; has received personal fees and held stock as a member of the board of directors from infinity pharmaceuticals ; held stock as a member of the advisory board from apogen biotechnologies ; has received personal fees and held stock as a member of the advisory board from pmv pharma ; has received personal fees and held stock as a member of the advisory board from juno therapeutics ; has received personal fees and held stock as co - founder from tango ( f / k / a synthetic lethal ) ; has received personal fees and held stock as a member of the scientific advisory board and the board of directors from grail ; has received personal fees and held stock as a member of board of directors from varian medical systems ; held stock as a member of board of directors from foghorn therapeutics ; has received reimbursement for travel , e71 vol 20 february 2019 corrections correction to lancet oncol 2017 ; 18 : 67281 j , f o n t a , g a r c a d o n a s prez - valderrama b , et al . 
maintenance therapy with vinflunine plus best supportive care versus best supportive care alone in patients with advanced urothelial carcinoma with a response after first - line chemotherapy ( maja ; sogug 2011 / 02 ) : a multicentre , randomised , controlled , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 67281in this article , the declaration of interests should read jg - d reports personal fees from astellas , janssen ; grants and personal fees from astrazeneca , pfizer , pierre fabre , merck , bioclin , bristol myers squibb , novartis , and msd ; grants , personal fees , and non - financial support from roche ; and grants from gammamabs , outside the submitted work . 
af reports grants from astellas , astrazeneca , pierre - fabre ; personal fees and non - financial support from sanofi , janssen , bayer , and roche , outside the submitted work . 
bp - v reports personal fees from astellas pharma , novartis , pfizer , pierre fabre , bayer , sanofi , bristol - myers squibb , ipsen , and janssen - cilag , during the conduct of the study . 
jaa reports grants and personal fees from glaxosmithkline and novartis ; personal fees and nonfinancial support from jansen cilag ; grants , personal fees and non - financial support from bms ; personal fees from pfizer , roche , and eusa ; grants from sanofi and pierre fabre , outside the submitted work . 
nl reports personal fees from pfizer , sanofi , pierre fabre , roche , ipsen , pharma mar , bms , bayer , astrazeneca , astellas , and msd , outside the submitted work . 
jcv - g reports personal fees from pfizer , astellas , janssen , msd , bayer , roche , bristol , astrazeneca , boehringer , pierre fabre , novartis , ipsen , celgene , lilly , merck , sanofi , and mundipharma , outside the submitted work . 
bm reports personal fees and non - financial support from pfizer and janssen ; personal fees from novartis , astellas oncology , bms , sanofi , ipsen , bayer ; and grants and personal fees from roche , outside the submitted work . 
agda reports advisory board , consultancy and speaker honoraria or travel support from pierre fabre , roche , bristol - myers squibb , msd , pfizer , novartis , bayer , janssen , sanofi , astellas , eusa pharma , and eisai ; and research funding from astellas . 
dc reports personal fees from janssen , roche , astellas , msd , ipsen , pfizer , bms , bayer , astrazeneca , novartis , lilly , sanofi , pierre fabre , and boheringer , outside the submitted work . 
eg reports grants from pierrefabre , during the conduct of the study ; personal fees and non - financial support from janssen , pfizer , bayer , ipsen , novartis , bms , rovi ; personal fees from menarini and leo pharma ; and nonfinancial support from pierre - fabre , outside the submitted work . 
ua reports non - financial support from novartis , pierre fabre , and ipsen ; personal fees from bayer , janssen , astellas , and pfizer ; and personal fees and nonfinancial support from sanofi , roche , and bms , outside the submitted work . 
 xgdm reports personal fees from pfizer , ipsen , bms , roche , lilly , pharmamar , eusapharma , and pierre fabre ; and grants from astrazeneca , outside the submitted work . 
md has participated in advisory boards , consultancy , and speaker bureaus for roche , bristol - myers squibb , msd , pfizer , janssen , sanofi , astellas ; and received travel and accommodations expenses from roche , astellas , janssen , bayer , and lilly . 
jp has received honoraria as a consultant on advisory boards from pfizer , astellas , janssen , msd , bayer , roche , bms , boehringer , astrazeneca , ipsen , novartis , eusa pharma , eisai , and sanofi ; and as speaker from kyowa , pierre - fabre , celgene , lilly , and merck . 
 rm - b has served as a consultant or on advisory and / or speakers bureaus for sanofi aventis , bayer , janssen , astrazeneca , merck sharp & dohme , and asofarma ; and received travel and accommodations expenses from roche , sanofi aventis , astellas , janssen , merck sharp & dohme , bayer , pharmacyclics , clovis oncology , and lilly . 
jlp - g reports non - financial support from pierre fabre , during the conduct of the study ; non - financial support from roche , bms , and msd , outside the submitted work . 
jb reports grants and personal fees from pfizer , merck , bms ; personal fees from genentech , astrazeneca , pierre - fabre ; and grants from takeda , during the conduct of the study . 
 this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1493503 zackrisson s , lng k , rosso a , et al . 
 lancet oncol 2018 ; 19 : 1493503 in this article , in table 1 and table 4 , the age groups should have been listed as follows : 4049 , > 4959 , > 5969 , and > 69 . 
the title and legend of figure 2 should have read as follows : number of false - positive results among participants over the trial period who were recalled only on digital breast tomosynthesis and digital mammography , respectively . 
 these corrections have been made to the online version as of jan 3 , 2019 . vol 20 january 2019 corrections prevention , treatment , and profit : an unsustainable alliance world cancer day , on feb 4 , 2019 , had at its core a message of early detection and screening . 
a focus on screening has obvious advantages , but how best to integrate prevention into health services , and the risk of overtreatment , are sources of debate . several strategies have aimed to bring screening to the public more directly , rather than relying on attendance at designated appointments . 
in england , in light of the failure to meet 2018 targets for breast , bowel , and cervical cancer screening , the national health service ( nhs ) has pledged to increase early diagnosis of cancers by 75% over the next 10 years . 
in canada , the screen for life mobile life coach also provides tests for breast , cervical , and colon cancer for individuals near their places of work , with the aim of improving general uptake of these services . 
although any population - based screening increases the chance of overdiagnosis and can be compromised by complex lifestyle and societal factors , precision prevention in high - risk individuals is a useful approach to tackle the cancer burden , while providing a good trade - off between the benefits and harms . 
early diagnosis not only improves outcomes and reduces mortality , it also lessens the reliance on cancer drugs , some with highly debatable clinical benefit , that drain billions of dollars from health - care systems each year . a recent who report shows that even in highincome countries , there are huge disparities in access to , and most notably the pricing of , cancer medicines . 
 the findings , although not surprising , are stark : prices of cancer drugs have continued to increase year on year , sometimes even doubling within 5 years , and with the increasing use of more and more complex immunotherapies , prices are likely to rise further . 
 it is sobering to see , in the who report , not only incurred by pharmaceutical a breakdown of costs companies and the apparent disconnect between cost and profit , but also the huge variation in drug pricing strategies between countries . 
the wholist for cancer drugs endorsed essential medicines is still unaffordable in many places ; in low - income countries , 57% of drugs on the list are available only if patients pay for the full cost of treatment themselves . 
for drug companies , who can reduce their original asking price by as much as 70% , what does this say about the elasticity of their prices ? with an average return of us$1450 on every $1 invested in research and development , there is no doubt room for manoeuvre . 
8 years later , the findings of the who report reiterate that the problem is now even more rampant , and drastic measures are needed to tackle what seems to be gross profiteering by the pharmaceutical industry . agencies regulatory and health - care systems are integral to easing cancer burden . 
in the uk , the national institute for health and care excellence has a firm grip on the introduction of drugs into the nhs and is essential to maintaining cost - effectiveness , but even with this regulation , the nhs still continues to face chronic funding problems . 
 this burden will only be reduced by addressing prevention and profit in paralleland , if profit margins continue to remain out of reach , one of the most effective ways will be to reduce the reliance on these medicines altogether . 
 the lancet oncology for more on screening targets not being met see bbc.co.uk / news / health - 47074657 for more on the nhs long - term plan see longtermplan.nhs.uk / areas - ofwork / cancer / for more on the nhs lung cancer screening trucks see society / 2019 / feb / 08 / nhs - toscreen - for - lung - cancer - intrucks - in - supermarket - car - parks for more on the canadian cancer screening bus see story / 7065903 - cancerscreening - at - work - new - mobilecentre - brings - tests - to - patients / for more on precision prevention see thelancet.com / journals / lanonc / article / s1470 - 2045 ( 17 ) 30331 - 5 / fulltext for more on the who technical report see medicines / areas / access / improving - affordabilityeffectiveness - of - cancermedicines / en / for more on the lancet oncology commission see commissions / deliveringaffordable - cancer - care - in - highincome - countries vol 20 march 2019 editorial correction to lancet oncol 2018 ; 19 : 58081 grob jj . 
is there any interest in a new brafmek inhibitor combination in melanoma ? lancet oncol 2018 ; 19 : 58081in the title of this comment , braf - mek inhibitor was spelt incorrectly , and in the fourth paragraph one instance of the drug encorafenib was spelt incorrectly and the dose of encorafenib should have been 300 mg . 
 lancet oncol 2018 ; 19 : 70514in the summary , the following statement should have read as follows : cohort 3 was assigned to receive a dose of 100 mg / m twice daily ( maximum 100 mg per dose ) , regardless of age , equating to a maximum of 173% of the recommended adult phase 2 dose . 
 this correction has been made to the online version as of april 25 , 2018 , and the printed version is correct . vol 19 may 2018 e229 corrections correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections comment published online july 13 , 2015 s1470 - 2045 ( 15 ) 00093 - 5 see articles page 967 chemotherapy and antiangiogenics in biliary tract cancer in the landmark phase 3 abc - 02 trial , valle and colleagues1 established the combination of gemcitabine and cisplatin as the standard of care for rst - line treatment of patients with advanced biliary tract cancer . 
this regimen showed a median overall survival of nearly 1 year , and based on this encouraging result , the combination of gemcitabine and platinum has emerged as the chemotherapy backbone for testing the addition of targeted treatments . 
unfortunately , trials combining an anti - vegf agent or an anti - egfr agent with gemcitabine and platinum have yielded disappointing results , 26 but similar e orts with agents targeting alternative pathways are underway . 
with insu cient e ective second - line systemic regimens in advanced biliary tract cancer , enhancing the e cacy of rst - line treatment is a rational strategy to improve patient outcomes in this aggressive disease . in the lancet oncology , valle and colleagues7 report the results of the abc - 03 trial , a randomised phase 2 trial of gemcitabine and cisplatin with or without cediranib in the rst - line treatment of patients with advanced biliary tract cancer . 
the strategy of simultaneously targeting the tumour microenvironment with antiangiogenic treatment and tumour cells with chemotherapy has improved patient survival in advanced colon , lung , gastric , and ovarian cancers . 
 however , similar to other trials of anti - vegf treatment in advanced biliary tract cancer , the abc - 03 trial was negative and ndings showed no di erence in the primary endpoint , progression free survival , between the two groups ( hr 093 , 95% ci 065135 ; p = 072 )  . 
 why did the addition of cediranib fail in this context ? first , the combination of chemotherapy with kinase inhibitors of vegf pathway have largely been ine ective across disease types and have not matched the e cacy of anti - vegf and anti - vegfr antibodies in a similar setting . 
these ndings might be due to di erential mechanisms of action and increased o - target e ects with kinase inhibitors . second , the lack of validated predictive biomarkers for the identi cation of patients likely to bene t from cediranib led to an unselected study population . 
most including anti - vegf agents previous clinical trials in advanced biliary tract cancer were also done in unselected populations and have not reported analysis of vegf - related biomarkers . 
a randomised phase 2 trial8 of gemcitabine with or without sorafenib showed that pdgfrexpression in tumour stroma was associated with improved progression - free survival , but this result has not been further validated . 
valle and colleagues should be commended for reporting circulating biomarker analysis in the largest cohort of patients with advanced biliary tract cancer in a trial of antiangiogenic treatment so far . 
additional data for outcomes by anatomic location might also yield hypotheses regarding subpopulations likely to bene t from cediranib . third , the toxic e ects of cediranib could have limited drug exposure . 
patients who received cediranib more frequently required at least one dose reduction compared with placebo from the already attenuated dose of 20 mg once a day . fourth , vegf inhibition could have paradoxically fuelled tumour growth and led to chemoresistance . 
several explanations could account for this , including random statistical error , but one explanation could be that cediranib - induced vascular pruning initially led to tumour regression but the ensuing hypoxia ultimately promoted tumour progression . 
increasing evidence has shown that hypoxia can create a hostile environment that promotes tumour growth by inducing angiogenesis , genetic instability , cancer cell invasion , stem - like phenotype , epithelial - to - mesenchymal transition , and resistance to apoptosis.9 the success of antiangiogenic drugs could rest on achieving balance between therapeutic and pathological angiogenesis in which tumour vascular normalisation rather than vascular pruning is the goal . 
in view of the negative results of several anti - vegf agents in advanced biliary tract cancer , future e orts with randomised trials should aim to use alternative strategies ( eg , anti - vegfr antibodies ) , inhibit alternative targets 882 vol 16 august 2015 in angiogenesis , or use a biomarker - driven trial design to select patients likely to bene t from this strategy . two merits of the abc - 03 trial deserve comment . 
with less than 5% of positive phase 2 combination therapy trials eventually improving the standard of care in oncology , 10 aiming for a large e ect size can ultimately save resources and protect patients from receiving ine ective , toxic regimens in futile phase 3 trials . 
 the consortium they have developed in the uk allowed them to accrue 124 patients across 14 centres in 18 months and collect blood for biomarker analysis from many of these patients . 
this structure can serve as a model for other countries to execute e cient trials with generalisable results in advanced biliary tract cancer . in conclusion , gemcitabine and platinum will remain the standard rst - line treatment for patients with advanced biliary tract cancer . 
further e orts to characterise the biology of both the tumour and its microenvironment in advanced biliary tract cancer , coupled with well - designed clinical trials , will hopefully bring us closer to nding the next e ective treatment in this disease . 
 lipika goyal , dawn q chong , dan g duda , * andrew x zhu massachusetts general hospital cancer center , boston , ma 02114 , usa ( lg , dqc , dgd , azx ) ; national cancer centre singapore , singapore ( dqc ) azhu@mgh.harvard.edu we declare no competing interests . 
gemcitabine and oxaliplatin with or without cetuximab in advanced biliary - tract cancer ( bingo ) : a randomised , open - label , non - comparative phase 2 trial . 
e cacy and safety of gemcitabine , oxaliplatin , and bevacizumab in advanced biliary - tract cancers and correlation of changes in 18uorodeoxyglucose pet with clinical outcome : a phase 2 study . 
clin cancer res 2010 ; 16 : 52965302 . is the bene t of oxaliplatin in rectal cancer clinically relevant ? the statement a statistically signi cant gain is not necessarily clinically relevant is accepted by most . 
 statistical signi cance is an objective nding , dependent on the quality of the trial , whereas the assessment of clinical relevance is subjective and open for discussion . in the lancet oncology , claus rdel and colleagues1 report the results of a phase 3 trial examining oxaliplatin added to uorouracil - based preoperative chemoradiotherapy and postoperative chemotherapy in locally advanced rectal cancer . 
the study was a large , well performed trial , meticulously analysed by a group with an excellent track record ; thus , the statistical signi cance favouring the addition of oxaliplatin is likely true . 
to assess its clinical relevance , the design of the study ( eg , inclusion criteria and choice of control treatment ) and the magnitude of the gain must be considered in relation to present knowledge . 
the di erent uoropyrimidine schedules in the experimental and control groups prevent an assessment of the e cacy and toxic e ects of oxaliplatthe lack of any di erence in toxic e ects to the postoperative therapies probably re ects the choice of the toxic mayo clinic schedule as control therapy ; if a proper infusion schedule had been chosen , comment published online july 16 , 2015 s1470 - 2045 ( 15 ) 00018 - 2 see articles page 979 vol 16 august 2015 comment tsc on the endocrine system are not yet understood , 9 and tsc might cause amenorrhea independently . 
mtor are e cacious renal angiomyolipomas and lymphangioleimyomatosis , 10 , 11 and there are continuing and completed studies in patients with tsc to assess oral mtor inhibitors for intractable epilepsy ( exist - 3 ; nct01713946 ) and cognition ( tron ; nct01954693 ) inhibitors for dis guring facial and topical mtor angio bromas ( treatment ; nct01526356 )  . 
with the recent promise shown by mtor inhibitors to help neural connectivity and the fairly minor negative side - e ect pro le , the drugs might soon be prescribed to patients with tsc for indications other than tumour shrinkage . 
the mtor inhibitor revolution rolls on hope northrup division of medical genetics , department of pediatrics , the university of texas medical school at houston , houston , tx 77030 , usa hope.northrup@uth.tmc.edu i declare honoraria and payment of travel expenses from novartis for speaking at the tsc days conference in dublin , ireland ; sept 1213 , 2014 . franz dn , belousova e , sparagana s , et al . 
e cacy and safety of everolimus for subependymal giant cell astrocytomas associated with tuberous sclerosis complex ( exist - 1 ) : a multicenter , randomized , placebo - controlled phase 3 trial . 
 n engl j med 2008 ; 358 : 14051 . 11 mccormack fx , inoue y , moss j , et al , for the national institutes of health rare lung diseases consortium and the miles trial group . 
 chromoplexy and hypoxic microenvironment drives prostate cancer in men with in the lancet oncology , emilie lalonde and colleagues retrospective cohort analysis1 assesses genomics , instability , and hypoxia as predictors of genomic recurrence localised prostate cancer . 
the investigators controlled for pretreatment prostate - speci c antigen , gleason score , and t stage . instability have their results suggest that genomic signatures or independent measures of genomic value in prediction of biochemical ( prostate - speci c antigen ) relapse and clinical metastasis in patients with localised prostate cancer . 
although the mechanisms by which hypoxia leads to radiation resistance can be reasonably assumed , the mechanism for an association between hypoxia in tumour tissue and biochemical recurrence after surgery is far less clear . 
as such , the work in lalonde and colleagues study is novel in that it shows that cancer aggression is driven not only by genome instability and mutations , but also by tissue hypoxia . published online november 13 , 2014 s1470 - 2045 ( 14 ) 71114 - 3 see articles page 1521 vol 15 december 2014 1419 comment the e ectiveness of radiation is very dependent on the oxygen status of the tissue being treated , with tumour sensitivity increased by a factor of about 3 in normoxic compared with hypoxic tumours . 
a rapid increase in radiosensitivity happens as the oxygen concentration reaches 30 mm hg or 05% oxygen.2 studies of patients with cervical cancer and soft - tissue sarcoma treated with radiation have shown that hypoxic tumours are more likely to recur and metastasize than are normoxic tumours.3 , 4 a series of interventions to improve tumour oxygenation have been attempted in order to improve radiotherapy e cacy . 
these interventions are divided into three categories : rst , increased oxygen delivery by the blood ( hyperbaric oxygen , breathing carbogen [ a mixture of oxygen and carbon dioxide ] , nicotinamide , second , transfusions , and erythropoietin ) , blood oxygen mimetics used in the radiochemical process ( nitroimidazoles ) , and , third , destruction of hypoxic cells ( hypoxic cytotoxins and hyperthermia ) .5 in a meta - analysis5 of more than 10 000 patients with solid tumors ( including bladder , uterine cervix , head and neck , brain , lung , oesophagus , and pancreas ) from 86 clinical trials using hyperbaric oxygen , chemical sensitizers , carbogen breathing , and blood transfusions , the investigators reported a signi cant improvement in locoregional control ( odds ratio [ or ] 077 , 95% ci 071086 ) and a signi cant survival bene t ( 087 , 081095 ) with hypoxic modi ers . 
 notably , lalonde and colleagues ndings show that the combination of percentage of genome alteration and hypoxia selects a group of about 25% of low - risk men with prostate cancer who are likely to have biochemical failure before 18 months . 
with validation in an active surveillance population , a socalled quiet genomic or hypoxic subtype could be added to criteria , thus enabling patients who are classi ed as high risk on the basis of genomic categorisation to receive upfront treatment while allowing the quiet group to avoid intervention . 
the potential of the speci c methodology described by lalonde and coleagues will need to be compared with other gene signatures in development and use.6 genomic instability is an evolving concept in clinical cancer . 
chromoplexy , or chromosomal change , in which the prostate cancer tumour genome advances through mutation , translocation , and other interdependent dna rearrangements mediated by post - translational modi cations such as ubiquitination and sumoylation , might be key to a series of essential cancer processes including avoidance of apoptosis , invasion , and metastasis , and therapeutic resistance.7 hence , measures of genomic heterogeneity , instability or change might better characterise the notion of chromoplexy as a measure of cancer cells or clusters to achieve key biological functions needed for tumour progression individual genetic aberrations or compared with disordered pathway signaling . 
much work still needs to be done to formulate the best combination of targeted therapy for the cancer cell and modi cation of the microenvironment to optimise some of our oldest therapies , including radiation . 
of the 552 unique articles citing the bhgi guidelines , 359 ( 65% ) referenced either the guidelines overviews ( 200 [ 36% ] ) or the early detection guidelines ( 159 [ 29% ] )  . 
on the basis of the citation analysis , 375 ( 68% ) cited bhgi guidelines as a breast cancer is the most common cause of cancer deaths for women worldwide.1 the number of women low - income and middlewith breast cancer income regions is increasing over time.2 important advances for e ective breast cancer management have mainly bene ted high - income countries . 
 such countries , evidence - based guidelines outlining optimum approaches for early detection , diagnosis , and treatment of breast cancer have been implemented in national cancer control programmes.3 poor healthresources and poorly organised health - care care systems , however , represent a substantial barrier to the implementation of such practices in low - to - middle income countries ( lmics ) .4 the breast health global initiative ( bhgi ) developed practical guidelines for breast cancer control that are evidence - based , resource strati ed , and culturally appropriate , with the aim of integrating practices in early detection , diagnosis , and treatment for breast cancer into existing health - care systems in lmics . 
 since 2002 , the bhgi has held a series of international summits that have brought together experts from around the world to develop consensus panels to devise appropriate resource - strati ed guidelines for breast cancer care and management . we examined the literature systematically to assess implementation of bhgi guidelines from the creation of knowledge in guideline development , through guideline dissemination in the global health published work , and organisational adoption and implementation of the guidelines . 
of the 776 remaining articles , 224 ( 29% ) were direct products of the bhgi group and 2003 2004 2005 2006 2007 2008 2009 2010 2011 2012 year figure : frequency of articles referencing the breast health global initiative guidelines , by year of publication ( n = 552 ) vol 15 december 2014 1421 correction to lancet oncol 2018 ; 19 : e10212 sundar s , khetrapal - singh p , frampton j , et al . 
 lancet oncol 2018 ; 19 : e10212in this series paper , in the section titled challenges from womens cancer in india , the second sentence of the second paragraph should read despite this initiative , large - scale implementation of cancer prevention and control strategies has yet to take place , and public expenditure on health remains low at 12% of indias gross domestic product . 
this correction has been made to the online version as of may 31 , 2018 . correction to lancet oncol 2018 ; 19 : 72829 correction to lancet oncol 2018 ; 19 : 54961 iarc monographs vol 121 group . 
lancet oncol 2018 ; 19 : 54961in figure 3 of this article ( published online first on feb 20 , 2018 ) , the heatmap in panel a has been replaced to amend display errors . 
this correction has been made to the online version as of may 31 , 2018 . vol 19 june 2018 e283 corrections correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections oncology , fake news , and legal liability in trust between the the decline lay public and professional opinion is a major chal lenge . 
at the centre of this crisis , is a collision between personal autonomy , specious journalism , social media , widespread dis infor mation , and political marginalisation , which together undermine the value placed on science and academic endeavour . 
in oncology , this situation manifests itself in numerous waysmost notably through patient selfdiagnosis and demand for specific treatments irrespective of their doctors advice ; escalating numbers of patients using alternative unproven therapies ; and increasing reliance on socalled defensive medicine to fend off lawsuits . institute in 2017 , researchers in a jama oncology study published on july 19 , 2018 , and in an earlier article in the journal of the national cancer investigated the association between the use of complementary and alternative medicine , adherence to conventional treatment , and overall survival in patients with cancer . 
 found that patients using together , the studies complementary medicine are more likely to refuse surgery , radiotherapy , or chemotherapy , and patients using complementary or alternative medicine are more than twice as likely to die than those treated with conventional medicine . 
how has society got to this point , where unproven interventions are being chosen in preference to evidencebased , effective treatments ? unfortunately , disinformation andfranklylies are propagated widely and with the same magnitude as verified evidence due to the ease with which social media , ubiquitous online news platforms , and disreputable marketing exercises can populate information channels , which often do not have sufficient funding to employ subjectspecific journalists to weed out facts from fiction . a further consequence of public distrust in mainstream medicine , spread by socalled fake news , misreporting , or contradictory stories , is a tendency for doctors to overtreat patients to prevent claims of malpractice . 
this number was met with scepticism , but a recent us national bureau of economic research working paper provides some evidence to support the under lying hypothesis that huge sums of money are spent needlessly . 
the article shows the fear of lawsuits increases us healthcare expenditure by about 5% ( equivalent to about $170 billion ) and outcomes for patients who get extra care are no better than in those who do not . 
numerous legal reforms have been suggested to shield doctors from excessive liability , including immunity from malpractice claims , caps on the amount of damages awarded , or the use of administrative courts rather than juries . 
 despite these existential pressures , according to the 2018 medscape oncologist compensation report , twothirds of us oncologists still say the most rewarding part of their job is their relationship with patients , the challenge of making the right diagnosis , or being proud of the job they do . 
however , the report , which surveyed over 20 000 oncologists , also found that 41% were worried about the number of rules and regulations they must comply with , problems associated with dealing with difficult patients , or being sued , all of which emphasises the levels of stress health professionals are exposed to and the constant battle against external factors beyond the satisfaction of their core role . in the current era of fake news and public distrust in the establishment , efforts must be redoubled to better communicate medical advances accurately with the lay public and with patients to ensure genuine knowledge can be separated from false material . 
for example , the uk charity , macmillan cancer support , has recently hired a digital nurse specialist to help debunk fake news via an online questionandanswer service , and the us national institutes of health give detailed tips on how to evaluate health information on the internet . 
 if these challenges are not addressed soon , the great advances in science and medicine that have markedly improved human health worldwide could be easily undone and society will come to regret such inaction and reliance on unreliable sources of information . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections and advisory board and consulting fees from eli lilly ; has received personal fees and held stock as a member of advisory board from seragon ; has received reimbursement for travel and in - kind items and services from roche , outside the submitted work . 
 s - ai reports grant support from astrazeneca and advisory consultant roles for astrazeneca , eisai , novartis , pfizer , roche / genentech and spectrum , outside the submitted work . 
hi reports grant support and personal fees from novartis during the conduct of the study ; hi was also an uncompensated member of the steering committee of this study ; hi has received personal fees in the form of honoraria and consulting fees from astrazeneca , pfizer , lilly , daiichi - sankyo , and f hoffman la - roche via chugai , outside the submitted work . 
jc reports personal fees from novartis , celgene , cellestia , astrazeneca , biothera pharmaceuticals , merus , seattle genetics , daiichi sankyo , erytech , pfizer , eisai , and samsung ; has received stock , patents , and intellectual property from medsir ; has received personal fees and research funding to his institution from roche , outside the submitted work . 
mdls reports personal fees in the form of speakers honoraria and advisory board honoraria from novartis , roche , lilly , pfizer , eisai , ipsen , and teva , outside the submitted work . 
cla reports personal fees for participation in a steering committee for the clinical trial from novartis , during the conduct of the study ; and personal fees for an expert advisory role from eli lilly , astrazeneca , genentech , millennium , celgene , pfizer , radius , and merck , outside the submitted work . 
sc also reports personal fees received in the form of honoraria for advisory boards from novartis , hoffmann laroche , pfizer , astrazeneca , and genomic health ; and institutional research support from novartis , hoffmann laroche , pfizer , astrazeneca , genomic health , genentech , merck , and bms , outside the submitted work . 
she also reports grant support from ambryx , amgen , bayer , obi pharma , bimarin , cascadian , daiichi sankyo , dignitana , genentech , gsk , lilly , macrogenics , medivation , merrimack , novartis , pfizer , pieris , puma , roche , seattle genetics , and travel support from lilly , novartis , and obi pharma , outside the submitted work . 
 reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
pv reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 15964 wolf a , naylor k , tam m , et al . 
these corrections have been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 17980 massari f , di nunno v . 
lancet oncol 2019 ; 20 ; 17980in this comment , the following sentence has been edited from time to deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab to risk of deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab . 
 this correction has been made to the online version as of feb 1 , 2019 , and the printed version is correct . vol 20 february 2019 corrections correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections treatment pleural personalised mesothelioma , with the potential to improve outcomes and enhance patients quality of life . for malignant in summary , the publication of these two promising studies is an important and encouraging advance for malignant pleural mesothelioma . 
they might do the same for malignant pleural mesothelioma in time ; however , for now all efforts must be directed toward supporting definitive trials , for it is these that have the potential to transform the treatment landscape of malignant pleural mesothelioma . * anna bibby , nick maskell academic respiratory unit , translational health sciences , university of bristol medical school , southmead hospital bristol , bristol bs10 5nb , uk anna.bibby@bristol.ac.uk we declare no competing interests . 1 woolhouse i , bishop l , darlison l , et al . 
nivolumab or nivolumab plus ipilimumab in patients with relapsed malignant pleural mesothelioma ( ifct - 1501 maps2 ) : a multicentre , open - label , randomised , non - comparative , phase 2 trial . 
tremelimumab as second - line or third - line treatment in relapsed malignant mesothelioma ( determine ) : a multicentre , international , randomised , double - blind , placebo - controlled phase 2b trial . 
the dearth of trials results from several methodological challenges , and because of surgeons reluctance to be involved in study design.1 nonetheless , experimental research is crucial to the generation of high - quality data to assess the effects of new procedures or devices before introducing them insufficiency of highinto standard practice . 
despite this technique being the most common surgical procedure for breast reconstruction worldwide , the number of patients involved in randomised trials is very low.2 in the ibra study , shelley potter and colleagues investigated short - term outcomes of immediate implant - based breast reconstruction with or without mesh in a large prospective cohort of 2108 patients ( 2655 reconstructions ) across 81 breast and plastic surgical units in the uk.3 this study was designed to identify key questions and suitable outcomes to be sling trials . 
mesh - based followed by dermal investigated with adequate power in forthcoming randomised reconstruction ( 1376 [ 65% ] patients ) was by far the most common implants method , ( 440 [ 21% ] patients ) and non - mesh submuscular or subfascial implants ( 181 [ 9% ] patients )  . 
the results highlight that the proportion of patients is far higher than proposed with complications standards : nearly a tenth of patients had implant loss , almost a fifth were readmitted or re - operated for complications within 3 months , and a quarter infection.3 , 4 further , these needed treatment for levels of complications have not decreased since the 200809 uk national mastectomy and breast reconstruction audit ( nmbra ) .5 in our opinion , these worrisome conclusions could be a direct consequence of the poor evidence available to inform choices about the best method of reconstruction to use , which generates unreliable and confusing information about indications , risk factors , and outcomes . published online january 9 , 2018 s1470 - 2045 ( 18 ) 30831 - 3 see articles page 254 174 vol 20 february 2019 comment although new trials are awaited , according to the findings of the ibra cohort it is unlikely that they will be based on comparisons between two - stage and one - stage breast reconstruction . 
the latter has gained popularity ( 78% of patients in ibra had a one - stage reconstruction planned ) , probably thanks to the generalised assistance of scaffolds ( 86% of biological meshes and 82% of synthetic devices were implanted in a one - stage procedure ) , which did not produce any significant difference in implant loss , infection , re - operation , or readmission . 
infection , implant loss , readmissions , and re - operation were significantly associated with bodymass index ( bmi ) and smoking , whereas previous radiotherapy was a risk factor only for infection , and operative time only for re - operation . the high incidence of infection shown by the ibra findings is concerning , and we recommend analysis of this outcome according to antibacterial prophylaxis . while despite the fact that all risk factors should be assessed in clinical practice to keep complications under control , we agree with potter and colleagues that the inclusion criteria of further randomised trials should not be too restrictive . 
eliminating subgroups from trials according to potential risk factors ( ie , on the basis of bmi , smoking , previous radiotherapy , or duration of surgery ) might prevent a conclusive and reliable investigation . the surgical community awaits newly designed trials , we wonder how these investigators observations could be translated into safer clinical practice now , to bring the safety outcomes of implantbased reconstructions within the proposed standards . 
this assumption must be supported by data because some studies report that weight increase can be associated with chemotherapy.6 we would suggest instead that pre - operative systemic treatment be used as an option to reduce the numbers of mastectomies.7 clearly , this approach might not reduce the relative number of complications , but it could affect the absolute number of sequelae . that it is interesting to notice that a dutch trial , 8 by contrast with two - stage ibra , concluded reconstructions might be safer than one - stage techniques with acellular dermal matrix , and that one of the risk factors for complications is breast size.9 for this reason , a robust oncoplastic assessment , including standard evaluation of breast morphology , glandular structure , and patterns of vascularity , should be done before selecting the most appropriate reconstructive technique.10 we applaud potter and colleagues for preparing the ground for a future useful randomised controlled trial in implant - based breast reconstruction . 
default - source / commissioning - and - policy / final - oncoplastic - guidelines - - healthcare - professionals.pdf ? sfvrsn = 0 ( accessed dec 28 , 2018 )  . jeevan r , cromwell da , browne jp , et al . 
breast conservation following neoadjuvant therapy for breast cancer in the modern era : are we losing the opportunity ? eur j surg oncol 2016 ; 42 : 178086 . dikmans re , negenborn vl , bouman mb , et al . 
two - stage implant - based breast reconstruction compared with immediate one - stage implant - based breast reconstruction augmented with an acellular dermal matrix : an open - label , phase 4 , multicentre , randomised , controlled trial . 
lancet oncol 2018 ; 19 : e578 . vol 20 february 2019 comment correction to lancet oncol 2018 ; 19 : 95364 correction to lancet oncol 2018 ; 19 : 104050 correction to lancet oncol 2018 ; 19 : e386 kramer souweidane mm , pandit - taskar n , et al . 
this correction has been made to the printed article , and to the online version as of aug 1 , 2018 . moreau p , mateos m - v , berenson jr , et al . 
lancet oncol 2018 ; 19 : 95364in the methods section of this article , the exclusion criteria for new york heart association heart failure should have been class iii or iv . 
this correction has been made to the online version as of aug 1 , 2018 . vol 19 aug 2018 e382 corrections comment published online december 4 , 2015 s1470 - 2045 ( 15 ) 00481 - 7 see articles page 109 future of cancer management , until such strategies become a ordable realities for most patients , the development of high therapeutic index chemotherapy regimens will remain one of the most important goals of academic oncologist societies . 
 tsang - wu liu , * li - tzong chen national institute of cancer research , national health research institutes , tainan 70456 , taiwan ( t - wl , l - tc ) ; department of internal medicine , national cheng kung university hospital , national cheng kung university , tainan , taiwan ( l - tc ) ; department of internal medicine , kaohsiung medical university hospital , kaohsiung medical university , kaohsiung , taiwan ( l - tc ) leochen@nhri.org.tw l - tc has received study medication for a phase 1 trial of sorafenib plus s - 1 from taiho in 2009 , and received study medication for pi - initiated trials and honorarium for scienti c presentations from tty , taiwan , in the past 36 months . 
s - 1 plus leucovorin versus s - 1 plus leucovorin and oxaliplatin versus s - 1 plus cisplatin in patients with advanced gastric cancer : a randomised , multicentre , open - label , phase 2 trial . 
n engl j med 2015 ; 372 : 190919 . detection of dcis and reduced invasive interval cancers when breast screening began in the uk , such was the uncertainty concerning the bene ts and harms of detecting ductal carcinoma in situ ( dcis ) that national guidelines speci ed an upper limit as well as a lower limit for detection by individual screening centres . 
this was only changed when an association was shown between dcis detection and small invasive cancer detection in the national health service breast screening programme.1 nonetheless , controversy regarding the pros and cons of dcis detection at screening has continued to this day . in the lancet oncology , stephen duffy and colleagues2 make a major contribution to the debate concerning the benefits and harms of detecting dcis at mammographic screening . 
it is not clear if the high frequency of screen - detected her2 - positive high - grade dcis leads to a reduction in her2 - positive invasive cancers in particular.6 the results of this study do not mitigate the harms due to overdiagnosis caused by the detection of low - grade dcis , which represents about 15% of screen - detected dcis and 3% of all screen - detected cancer . 
the loris trial continues to be an important vol 17 january 2016 comment study that aims to reduce the harms of detecting and treating low risk dcis.7 other indolent breast cancers detected at screening such as invasive tubular cancer deserve similar attention . it has been argued that recalling for further assessment following screening only those patients with comedo calci cation and not those with granular calci cation might prevent overdiagnosis of low - grade dcis while detecting high - grade dcis . 
 unfortunately , when small , high - grade dcis rarely shows the characteristic comedo calci cations seen in larger areas of high - grade dcis , while a large area of low - grade dcis might show comedo calci cation.8 it is therefore impossible for radiologists to recall small cases of high - grade dcis without also recalling low - grade dcis . 
although this study shows that sites with a high frequency of dcis detection are associated with a higher proportion of low or intermediate grade dcis , the e ect is very small . 
should screening programmes limit their detection of ductal carcinoma in situ ? clin radiol 2002 ; 57 : 108689 . du y sw , dibden a , michalopoulos d , et al . 
the merit of the article by isseki maeda and colleagues2 published in the lancet oncology is to increase the quality of the evidence available regarding the e ect of continuous deep sedation on survival in order to support good clinical practice . 
palliative sedation is de ned in scienti c documents and guidelines as the use of sedatives to reduce a patients level of consciousness with the aim of relieving symptoms due to a terminal illness that cannot be controlled by any other means.3 , 4 inclusion of palliative sedation as an option in end - of - life decision - making processes in a series of articles based on retrospective questionnaires5 answered by family doctors was problematic , because it ( possibly unintentionally ) allowed palliative sedation to be viewed as an alternative to euthanasia , 5 , 6 although other authors have tried to make a clear - cut distinction between these two practices.7 excessive emphasis on ethical discussions drawing on non - empirical evidence followed , and often confused the debate without contributing any clinical data . 
 for palliative despite opinion - based scienti c literature often stating otherwise , clinical experiences in palliative care show that pain is very rarely , if at all , a refractory symptom at the end of life ; instead , the most frequent indications terminal dyspnoea and deliriu additionally , the duration of palliative sedation is rarely longer than 2448 h , 8 , 9 showing that many of the ethical concerns raised are based on fragile foundations . 
we assessed the effects of postmastectomy radiotherapy on quality of life ( qol ) in women with intermediate - risk breast cancer . methods supremo is an open - label , international , parallel - group , randomised , controlled trial . 
women aged 18 years or older with intermediate - risk breast cancer ( defined as pt12n1 ; pt3n0 ; or pt2n0 if also grade iii or with lymphovascular invasion ) who had undergone mastectomy and , if node positive , axillary surgery , were randomly assigned ( 1 : 1 ) to receive chest wall radiotherapy ( 50 gy in 25 fractions or a radiobiologically equivalent dose of 45 gy in 20 fractions or 40 gy in 15 fractions ) or no radiotherapy . 
the qol substudy , open to all uk patients , consists of questionnaires ( european organisation for research and treatment of cancer qlq - c30 and qlq - br23 , body image scale , hospital anxiety and depression scale [ hads ] , and eq - 5d - 3l ) completed before randomisation , and at 1 , 2 , 5 , and 10 years . 
the prespecified primary outcomes within this qol substudy were global qol , fatigue , physical function , chest wall symptoms , shoulder and arm symptoms , body image , and anxiety and depression . 
this trial is registered with the isrctn registry , number isrctn61145589 . findings between aug 4 , 2006 , and april 29 , 2013 , 1688 patients were enrolled internationally and randomly assigned to receive chest wall radiotherapy ( n = 853 ) or not ( n = 835 )  . 
989 ( 79% ) of 1258 patients from 111 uk centres consented to participate in the qol substudy ( 487 in the radiotherapy group and 502 in the no radiotherapy group ) , of whom 947 ( 96% ) returned the baseline questionnaires and were included in the analysis ( radiotherapy , n = 471 ; no radiotherapy , n = 476 )  . 
at up to 2 years , chest wall symptoms were worse in the radiotherapy group than in the no radiotherapy group ( mean score 141 [ sd 158 ] in the radiotherapy group vs 116 [ 146 ] in the no radiotherapy group ; effect estimate 217 , 95% ci 040394 ; p = 0016 ) ; however , there was an improvement in both groups between years 1 and 2 ( visit effect 134 , 95% ci 236 to 031 ; p = 0010 )  . 
the results of some trials investigating selective omission of radio therapy or chemotherapy have recently been reported.2 , 3 although the effects of mastectomy and chemotherapy on quality of life ( qol ) have been well documented , the additional effect of adjuvant radio therapy following mastectomy is unclear . 
chest wall pain , fatigue , anxiety about recurrence , and depressive symptoms can all hold back recovery and return to normal activities of daily living.4 adjuvant chest wall irradiation after mastectomy remains a core and highly effective component of the locoregional management of early breast cancer , reducing locoregional recurrence and breast cancer for the mortality . 
we did not identify any meta - analyses or randomised phase 3 trials comparing qol in patients with breast cancer treated by mastectomy and systemic therapy , with or without adjuvant postoperative chest wall radiotherapy . 
a few studies have investigated patient - reported outcomes , such as symptoms and qol , but most patients in these studies had breast - conserving surgery rather than mastectomy , and none of the studies involved a comparator group randomly assigned to no radiotherapy . added value of this study this substudy of the phase 3 supremo trial investigated the effect of adjuvant postmastectomy radiotherapy on qol in a randomised trial in a large , well characterised population of uk patients with intermediate - risk ( one to three positive lymph nodes ) breast cancer . 
at 2 years , postmastectomy radiotherapy was associated with worse self - reported local chest wall symptoms ( pain , swelling , and skin problems in the area of the affected breast ) compared with no radiotherapy , but the difference between groups was small , unlikely to be of clinical significance , and symptoms improved over time . 
there were no differences between groups in arm and shoulder symptoms , body image , fatigue , overall qol , physical function , or anxiety or depression , or in the secondary qol outcomes of pain , role functioning , social functioning , sexual functioning , and nausea or vomiting . implications of all the available evidence the effect of postmastectomy radiotherapy on 10 - year survival , the primary endpoint of the main supremo trial , in patients with intermediate - risk breast cancer will not be known before 2023 . 
in the meantime , both options of administering or omitting postmastectomy radiotherapy seem to be legitimate in terms of their effects on qol for patients with intermediate - risk disease . 
our data will inform shared decision making ( as recommended in the recent us guidelines on postmastectomy radiotherapy ) and put patients in a better position to make an informed value judgment on what they consider relevant for their situation regarding the data on patient - reported symptoms and qol domains presented in this report . 
both physicians and patients could be helped when weighing up the individual estimates of possible benefits of postmastectomy radiotherapy against its effects on toxicity and qol . more involved axillary nodes is robust , its role in intermediaterisk patients with one to three involved nodes is controversial and practice and guidelines vary.5 results from a metaanalysis in 2014 showed an advantage in overall survival from post mastectomy radiotherapy that included at least the chest wall in the target volume in patients with either one to three positive nodes or four or more positive nodes.6 however , the trials with different generalisability of historical standards of surgery , radiotherapy , and systemic therapy remains uncertain , especially because contem porary survival rates are much higher than those in the studies included in the 2014 metaanalysis . 
potential benefits in survival need to be balanced against the risk of locoregional and cardiopulmonary toxicity , especially when radiotherapy is given in conjunction with poten tially cardiotoxic anthracyclines and trastu zumab . 
the primary and secondary endpoints of the trial have been described previously.9 substudies include transsupremo , which seeks molecular markers of radiosensitivity , a cardiac substudy , andfor uk patients onlyqol and health economics assessments . 
 these substudies will provide an important highquality evidence base about the balance of potential benefits and treatment burden , to support patients and healthcare professionals during shared decision making . the longterm effect of breast cancer and its treatment on everyday life has been identified as a crucial knowledge gap and a key priority for breast cancer research.10 for radiotherapy , little information about treatment impact is available . 
a few trials have investigated selfreported breast , arm , and shoulder symptoms , functional out comes , and qol after radiotherapy , mainly in patients receiving breastconserving therapy.1113 patients usually report transient and shortterm effects of radio therapy , with fairly limited effects on their overall qol.14 , 15 vol 19 november 2018 1517 articles for the trial protocol see supremo%20protocol%20 version29.pdf no comprehensive qol data exist in patients having postmastectomy radiotherapy , and only a few studies have compared patientreported outcomes following breastconserving surgery versus mastectomy with and without reconstruction . 
briefly , eligible patients were women aged 18 years or older who had undergone mastectomy for unilateral breast cancer and , if they had intermediate risk breast cancer , an axillary staging procedure with axillary lymph node dissection . 
patients were eligible if they had intermediaterisk breast cancer ( defined as pt12n1 ; pt3n0 ; or pt2n0 if also grade iii or with lymphovascular invasion on histology )  . 
 exclusion criteria included previous or concurrent malignancy ( apart from nonmelanomatous skin cancer and carcinoma in situ of the cervix ) , ductal carcinoma in situ , bilateral breast cancer , pregnancy at the time of radiotherapy treatment , and male sex . the study was approved by the multicentre research ethics committee , edinburgh ( mrec 05 / 50501 / 106 ) and local research and development offices . 
patients provided written , informed consent before enrolment and had additional options to consent to the substudies , including the qol substudy . randomisation and masking patients were randomly assigned ( 1 : 1 ) postoperatively to either chest wall radiotherapy or no chest wall radiotherapy . 
randomisation was done by permuted blocks , with block length varied randomly to minimise the effect of entry bias , and stratified by treatment centre because of possible betweencentre differences in radiotherapy procedures . 
in 2011 , the eligibility criteria were widened , following a protocol amendment ( version 29 ; aug 30 , 2010 ) approved by the ethics committee , to include the use of neoadjuvant chemotherapy , according to contemporary guidelines . for patients randomly assigned to receive chest wall radiotherapy , radiotherapy was given after chemotherapy ( if administered )  . 
surgery , systemic therapy , and pathology were also subject to prespecified quality assurance . additional recorded data included cardiovascular risk factors , radiotherapy cardiac and lung exposure par ameters , systemic therapy ( type , doses , and dates ) , and any reconstructive surgery ( type , and immediate or delayed )  . 
 patients with gross protocol violations ( eg , margins involved or less than 1 mm margins for invasive cancer or ductal carcinoma in situ ) were to be removed before the final analysis of the main trial . 
serious adverse events were to be reported if they occurred during radiotherapy or within 30 days of the last radiotherapy session ( fraction ) , irrespective of whether or not they were related to the randomly assigned treatment . 
any toxicity assessed as a grade 4 or 5 acute or late morbidity score had to be reported on a serious adverse event or suspected unexpected serious adverse reaction form for the entire followup period of the trial . 
 monitoring ( source data verification ) is being done by the cancer clinical trials team in edinburgh ( edinburgh , uk ) on 10% of the patient data from the main trial , with site visits allowed in the uk . 
higher levels of monitoring by the cancer clinical trials team will be done , if requested by the data monitoring committee , or if specific safety issues ( see protocol ) are identified by the investigators or the trial management group of the trial steering committee . 1518 vol 19 november 2018 articles all patients eligible for supremo from uk centres were invited to participate in the qol substudy . 
if the baseline questionnaire was not returned to the trials office , further questionnaires could not be sent , because the patients name and address were not available to the trial coordinator . 
the european organisation for research and treatment of cancer ( eortc ) qlqc30 ( version 3.0 ) consists of 30 questions addressing five functional scales ( cognitive , emotional , physical , social , and role ) , nine symptom scales ( appetite loss , constipation , diarrhoea , dyspnoea , fatigue , financial difficulties , insomnia , nausea and vomiting , and pain ) , and one global health status qol scale.18 the eortc qlqbr23 ( version 1.0 ) focuses on breast cancerspecific issues and includes 23 questions addressing four functional scales ( body image , future perspective , sexual enjoyment , and sexual functioning ) and four symptom scales ( arm symptoms [ swelling in arm or hand , arm or shoulder pain , and difficulty raising the arm ] , breast or chest wall symptoms [ pain , swelling , oversensitivity , and skin problems in the area of the affected breast ] , systemic therapy sideeffects , and being upset by hair loss ) .19 all scores for the eortc qlqc30 and eortc qlqbr23 were transformed to a scale from 0 to 100 . 
higher scores on the functional scales and global qol scale represent a superior level of functioning and better qol , whereas higher scores in the symptom scales or items represent worse symptoms . the body image scale ( bis ) is a tenitem scale designed specifically for use with cancer patients to assess aspects of attractiveness , sexual attractiveness , and feelings or satisfaction with appearance . 
scores for each scale were graded from 0 to 3 and summed to produce a single score , with a higher score indicating more body image problems ( score range from 0 to 30 ) .20 the hospital anxiety and depression scale ( hads ) is a 14item instrument with two subscales for anxiety and depression.21 scores range from 0 to 21 on each scale , with higher scores indicating more distress . 
a combined score of 19 or higher is considered to be indicative of psychological distress . the eq5d3l questionnaire measures health status across five domains ( mobility , selfcare , usual activities , pain and discomfort , and anxiety and depression )  . 
these eq5d3l health status descriptions are converted into a single summary index ( range from 0 to 1 ) by attaching a value to each of the levels in each dimension . 
according to standard practice , these values were obtained from a large uk population study using a choicebased method of valuation.22 the resulting summary score , or utility value , can then be used directly in a costutility analysis . outcomes the primary endpoint of the supremo trial is 10year overall survival . 
qol is a secondary endpoint alongside chest wall recurrence , regional recurrence , diseasefree survival , acute and late morbidity , costeffectiveness , metastasisfree survival , and cause of death . 
in this qol substudy , we prespecified as primary outcomes global qol ; fatigue ; physical function ; chest wall symptoms ; shoulder and arm symptoms ; body image ; and anxiety and depression . 
secondary outcomes are role , social , and sexual functioning , and pain , nausea , and vomiting . 1688 patients enrolled in supremo trial 853 randomly assigned to radiotherapy group 835 randomly assigned to no radiotherapy group 632 from uk sites 626 from uk sites 145 declined to participate in qol substudy 124 declined to participate in qol substudy 487 ( 77% ) of 632 agreed to participate in qol substudy 502 ( 80% ) of 626 agreed to participate in qol substudy 16 did not complete baseline questionnaire 26 did not complete baseline questionnaire 471 ( 97% ) of 487 completed baseline questionnaire * 476 ( 95% ) of 502 completed baseline questionnaire * 4 died 10 died 388 ( 83% ) of 467 completed year 1 questionnaire 388 ( 83% ) of 466 completed year 1 questionnaire 10 died 3 died 367 ( 80% ) of 457 completed year 2 questionnaire 350 ( 76% ) of 463 completed year 2 questionnaire figure 1 : trial profile of patients participating in the qol substudy qol = quality of life . 
with 200 evaluable patients per group , the proportion of patients with a particular sideeffect or specified degree of morbidity in a qol domain could be estimated with a standard error of 35% or less . 
however , because there is usually substantial attrition over time in qol studies , to have sufficient numbers by 10 years , a target of 800 patients taking part in the qol substudy was set . 
the total sample size of supremo was reduced during the trial , following a protocol amendment approved by the ethics committee , from 3500 to 1600 , but this did not affect the qol substudy sample size . when calculating qol questionnaire or subscale scores , we followed official questionnaire guidelines on handling missing individual items . 
in general , if more than 50% of items were missing , subscale scores ware not calculated ( missing ) ; if less than 50% of items were missing , those were replaced by the mean of the answered items and a score was calculated . 
if no guidance existed , that score was recor ded as missing . to maintain the normality of the residuals , the difference from baseline to each subsequent question naire was calculated for each scale . 
however , as the comparison of radiotherapy versus no radiotherapy is the primary objective of this trial , we will discuss those comparisons if the results have a p value of 005 or lower . 
 because of the large number of models , clinical variables will only be discussed if they exceed the more conservative threshold of p < 001 . the principal analysis modelled the change in score in the prespecified qol primary outcomes ( global qol , fatigue , physical function , chest wall symptoms , shoulder and arm symptoms , body image , and anxiety and depression ) by time ( visit 1 at 12 months or visit 2 at 24 months ) of followup , age group ( < 45 , 4554 , 5569 , 70 years ) , baseline score , and treatment ( with or without radiotherapy )  . because almost all patients received some form of systemic therapy and some underwent breast recon structive surgery , secondary exploratory analyses were done to assess whether or not these treatments affected the qol outcome measures . 
the secondary analysis included a prespecified exploratory analysis of clinical 1520 vol 19 november 2018 articles covariates also considered to have an effect on qol ( extent of axillary surgery , early breast reconstruction , adjuvant chemotherapy , adjuvant hormonal therapy , and use of trastuzumab )  . 
this analysis was done by creating a basic model of age group , time , and baseline score , then adding the clinical variables in turn to create a model of best fit . 
only patients with complete data for all clinical variables were included in this modelling . published data are available for eortc qlqc30 on change scores within groups or scores difference between groups that are clinically significant , but to the best of our knowledge , no such data are available for eortcbr23 scores.23 we opted to present mean scores and sds to allow comparisons with other studies . 
to attempt to explore the clinical significance of any observed statistically significant differences in eortcbr23 scores , we used a generic approach of 05 of the sd to indicate minimally important difference.24 recent guidelines from the us food and drug administration recom mend establishing a meaningful change in patientreported outcome measures at the individual level ( ie , defining a responder ) versus at the treatment group level , 25 with the definition of a responder being a score change in a measure , experienced by an individual patient over a predetermined time period that has been demonstrated in the target population to have a significant treatment benefit . 
26 we calculated proportions of patients whose scores improved ( change score < 05 sd ) between baseline and year 1 , those who remained stable or had no change ( change score 05 sd to + 05 sd ) , and those whose scores worsened ( change score > 05 sd )  . all analyses were done by intention to treat . 
 * only recorded in protocol version 29 ( aug 30 , 2010 ) onwards ; the denominator is the total number of recorded chemotherapy treatments from protocol version 29 onwards ( qol study : radiotherapy , n = 173 ; no radiotherapy , n = 173 ; full trial : radiotherapy , n = 269 ; no radiotherapy , n = 243 )  . 
denominator is the number of recorded answers ( qol study : radiotherapy , n = 460 ; no radiotherapy , n = 454 ; full trial : radiotherapy , n = 806 ; no radiotherapy , n = 782 )  . 
denominator is the total number of recorded neoadjuvant endocrine therapy treatments from protocol version 29 ( aug 30 , 2010 ) onwards ( qol study : radiotherapy , n = 206 ; no radiotherapy , n = 200 ; full trial : radiotherapy , n = 316 ; no radiotherapy , n = 288 )  . 
denominator is number of patients who received adjuvant endocrine therapy . table 1 : patient demographics and clinical characteristics role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author and joint senior authors had full access to all data in the study and had final responsibility for the decision to submit for publication . results between aug 4 , 2006 , and april 29 , 2013 , the trial recruited 1688 patients internationally from 27 eortc centres in nine european countries ( belgium , france , germany , ireland , the netherlands , poland , spain , switzerland , and turkey )  . 
in total , 989 ( 79% ) uk patients consented to participate , of whom 947 ( 96% ) returned the baseline questionnaires ( 471 [ 97% ] of 487 patients in the radio therapy group and 476 [ 95% ] of 502 in the no radiotherapy group )  . 
patients from the uk who declined participation or did not return the baseline questionnaires ( n = 311 ) were older ( mean age vol 19 november 2018 1521 articles 577 years [ sd 119 ] ) than those who consented and returned the baseline questionnaires ( n = 947 ; mean age 561 years [ sd 110 ] )  . 
mean age did not differ between participants in the qol substudy and the remaining 741 participants in the main trial ( ie , uk patients not participating in the substudy and all patients from other countries ; mean age 556 years [ sd 116 ] )  . 
to check further for potential bias in patient selection for the qol substudy , we compared the clinical char acteristics of patients completing the substudy with those of patients in the main trial and found no differences ( table 1 )  . good patient compliance was achieved with the com pletion of qol measures , with slightly better com pliance seen in the radiotherapy group than in the no radiotherapy group at baseline and year 2 ( figure 1 )  . 
eq - 5d - 3l score , range 01 . 074 ( 022 ) 075 ( 024 ) 075 ( 025 ) 1522 vol 19 november 2018 articles clinical characteristics were well balanced between the radiotherapy and no radiotherapy groups ( table 1 )  . 
 a further review of the type of breast reconstruction suggested more frequent autologous reconstructions in the radiotherapy group , whereas there were more recon structions with an implant or expander in the no radio therapy group ( appendix p 2 )  . 
 similar propor tions of patients in the two groups received adjuvant chemotherapy , trastuzumab , and endocrine therapy ( table 1 )  . most patients in the radiotherapy group of the qol substudy received 40 gy radiotherapy in 15 fractions ( 327 [ 68% ] of 478 patients ; seven patients did not receive radiotherapy as per protocol but their participation in the qol study is not known ) , with the remaining patients equally divided between 50 gy in 25 fractions ( 52 [ 11% ] ) , 45 gy in 20 fractions ( 48 [ 10% ] ) , and other or unknown ( 51 [ 11% ] )  . 
in the main trial , 445 ( 52% ) of 853 patients in the radiotherapy group received 40 gy in 15 fractions , 227 ( 27% ) received 50 gy in 25 fractions , 57 ( 7% ) received 45 gy in 20 fractions , and 124 ( 15% ) had other or unknown . 
at baseline , patients reported relative impairment in global qol , with mean scores of 604 and 609 ( 100 on the scale is excellent ) , relative impair ment of role ( mean 630 and 652 ) and social function ( 640 and 655 ) , a high level of fatigue ( mean of 430 and 416 ; 100 is greatest degree of fatigue ) , insomnia ( mean 372 and 362 ; 100 is the worst level of insomnia ) , and a degree of arm symptoms ( mean 212 and 203 ) , chest wall symptoms ( 181 and 173 ) , and pain ( 248 and 226 ; a score of 100 would be the worst symptoms ; table 2 )  . table 3 shows the results from mixedeffects model analysis of the prespecified primary qol outcomes and pain ( a prespecified secondary qol outcome ; data for other prespecified secondary qol outcomes not shown )  . 
such effects were adjuvant chemotherapy and immediate breast recon struction ( table 3 ) , but not extent of axillary surgery , adjuvant endo crine therapy , or trastuzumab ( appendix pp 34 )  . up to 2 years , chest wall symptoms were worse in the radiotherapy group than in the no radiotherapy group ( estimate of effect 217 , 95% ci 040 to 394 ; p = 0016 ; table 3 )  . 
there was an improvement in chest wall symptoms between years 1 and 2 in both groups ( visit effect 134 , 95% ci 236 to 031 ; p = 0010 ) , but the improvement was smaller in the radiotherapy group than in the no radiotherapy group ( table 3 )  . 
to explore the clinical the observed statistically significant significance of difference between the groups for chest wall symptoms , we calculated the sd of the change score for chest wall symptoms from baseline to year 1 in the no radiotherapy group . 
in a responder analysis , we calcu lated proportions of patients whose scores improved ( change score < 865 points ) between baseline and year 1 , those who remained stable or had no change ( change score 865 to 865 ) , and those whose scores worsened ( change score > 865 points )  . 
62 ( 16% ) of 386 patients in the radiotherapy group reported clinically meaningful worse change score ( ie , change score > 865 ) compared with 46 ( 12% ) of 385 patients in the no radiotherapy group ( appendix pp 78 )  . arm and shoulder symptoms did not differ signifi cantly according to treatment ( table 3 , figure 2b )  . 
 however , chemotherapy had an effect , with patients receiving chemotherapy showing less improve ment in arm symptoms over time ( figure 2b , table 3 ) , suggesting that chemotherapy and age were confoun ding variables affecting arm and shoulder symptoms . 
significantly more patients in the younger age groups received chemotherapy than did patients in the older age group ( 130 [ 97% ] of 134 patients aged < 45 years , 318 [ 96% ] of 332 patients aged 4554 years , 305 [ 84% ] of 362 patients aged 5569 years , and 43 [ 36% ] of 119 patients aged 70 years ; p < 00001 for test )  . 
the extent of axillary surgery ( comparison of sentinel node biopsy or node sampling vs sentinel node biopsy plus axillary node clearance vs axillary node clearance ) did not affect arm or shoulder symptom scores ( appendix pp 34 )  . 
furthermore , the extent of axillary surgery did not have an effect on any of the prespecified qol variables , apart from higher hads anxiety scores in patients with sentinel node biopsy plus axillary node clearance ( p = 001 ; appendix pp 34 )  . despite the observed differences in chest wall symptoms , image problems , with patients reported few body improvement in body image scale scores in both treatment groups between years 1 and 2 ( tables 2 , 3 )  . 
some age effect was observed , with patients younger than 45 years reporting more concerns about their body image compared with patients aged 70 years or older ( estimate of effect 196 , 95% ci 053339 ; p = 00074 ; table 3 )  . 
furthermore , improvement in global qol was seen in both groups between baseline and year 1 , with further but smaller improvement by year 2 ( figure 2c )  . 
as expected , there was an age effect 1524 vol 19 november 2018 articles with patients younger than 69 years reporting better overall physical functioning than patients aged 70 years or older ( table 3 )  . patients reported high baseline levels of fatigue , probably because of the preceding surgery . 
women younger than 70 years of age reported higher levels of anxiety ( table 3 ) , with improvement from baseline to year 1 and to year 2 in both groups ( table 3 )  . 
 the mean baseline score for selfreporting of general pain was just over 20 in both groups , but without any improvement from baseline to year 1 or year 2 independent of randomisation group ( tables 2 , 3 )  . 
no effect was found for trastuzumab , chemotherapy , or endocrine therapy ( none vs tamoxifen vs aromatase inhibitors ; data not shown )  . no betweengroup differences were noted for nausea or vomiting , or for sexual , role , and social functions at any timepoint ( table 2 )  . 
we had a good completion rate for the general sexual function questions ( 914 [ 97% ] of 947 ) , but only 253 ( 28% ) of 914 patients completed the conditional sexual enjoyment questions at baseline ( table 2 )  . 
all remaining scales and items did not show any effect of radiotherapy treatment and all showed improvement or stability over time . discussion the main finding of this qol substudy of the supremo trial is that postmastectomy radio therapy was associated with worse selfreported chest wall symptoms ( pain , swelling , oversensitivity , and skin problems in the area of the affected breast ) than no radiotherapy , although these symptoms improved over time . 
the estimated effect is small , with a difference in change scores between the radiotherapy and no radiotherapy groups of 217 points ( 95% ci 040394 ; p = 0016 )  . 
our responder analysis showed that 4% more patients assigned to radiotherapy reported a likely clinically meaningful worsening of their chest wall symptoms than did those in the no radio therapy group . 
the adjusted mean for the individual groups is the mean of the change scores ( defined as change from baseline to year 1 and from baseline to year 2 in each of the treatment groups , adjusted for baseline score , visit , and age )  . 
p values indicate whether each of the means of the change scores within each individual group is significantly different from zero ( ie , improvement or deterioration in scores from baseline )  . 
 table 3 : mixed - effects models ( fixed effects ) for qol outcomes note of caution is appropriate because of the assumptions made in the calculations ( ie , the assumption that an sd of the change score of 865 is likely to indicate a clinically meaningful difference )  . to the best of our knowledge , this is the first study to investigate the effect of adjuvant radiotherapy on qol in a large randomised trial in patients treated by mastectomy for intermediaterisk breast cancer ( including patients undergoing breast reconstruction )  . 
our results show that radiotherapy to the chest wall did not affect arm or shoulder symptoms ( axillary radiotherapy was prohibited in the trial ) , body image , global qol , physical function , fatigue , or symptoms of anxiety or depression . 
in supremo , about a quarter of patients ( those with pn0 [ sn ] tumours ) in the main trial and qol substudy underwent limited axillary surgery ( sentinel node biopsy or nodal sampling )  . 
 this is perhaps an unexpected finding and could be caused by lack of sensitivity of the eortc qlqbr23 scale ( which has three items on pain in arm or shoulder , swollen arm or hand , and difficulty raising your arm )  . 
therefore , our findings are not generalisable to women treated with both an axillary vol 19 november 2018 1525 articles a chest wall symptoms b arm and shoulder symptoms radiotherapy , no chemotherapy radiotherapy , chemotherapy no radiotherapy , no chemotherapy no radiotherapy , chemotherapy c global quality of life no radiotherapy radiotherapy d physical function 05 15 20 25 e fatigue no radiotherapy , no reconstruction radiotherapy , no reconstruction no radiotherapy , reconstruction radiotherapy , reconstruction time since treatment ( years ) time since treatment ( years ) figure 2 : change in qol scores from baseline to years 1 and 2 ( a ) chest wall symptoms . 
global qol ( c ) and functional scores ( d ) range from 0 to 100 with higher score indicating good functioning ; therefore , positive change score indicates improvement . 
this treatment is generally reserved for patients with higher nodal load ( n2 and n3 disease ) than those included in the supremo trial ( pn0 or pn1 )  . neoadjuvant chemotherapy treatment was allowed in a later protocol version ( version 29 ) , but the number of treated patients was too small ( n = 8 ) for valid conclusions and therefore we did not perform any betweengroup comparisons according to this variable . we observed a low frequency of immediate breast reconstruction ( which was done in only 111 patients )  . 
this procedure was associated with higher levels of fatigue and 1526 vol 19 november 2018 articles very compared with no immediate reconstruction , but had no effect on body image or the other qol outcomes . 
the estimated effect of immediate reconstruction on fatigue was 532 , corres ponding to a small clinically meaningful difference.23 however , this was an exploratory analysis and we used generic qol and body image questionnaires , which are likely to be less sensitive to specific outcomes than are breast reconstruction instruments ( such as breastq ) .17 the observed low frequencies ( 11% ) of reconstructive surgery ( either immediate or delayed to year 2 ) should be noted . 
this finding probably reflects the pattern of care in the period of the supremo trial recruitment ( 200613 ) or might be caused by concerns of enrolling patients who had undergone breast reconstruction into a trial of radiotherapy . 
we are collecting further infor mation on delayed ( beyond 2 years ) reconstructions , which will be analysed at 5 years and 10 years to provide valuable information about rates of breast reconstruction across the uk , as well as its effect on patients experiences and satisfaction with body image . 
a direct comparison of conventional versus hypofractionation for chest wall radiotherapy after breast reconstruction is being done in the usa by the alliance for clinical trials in oncology ( nct03414970 )  . 
the trial is ongoing and will complete recruitment in 2021 , with final results expected in august , 2025 . most of the published literature relating to the effect of adjuvant radiotherapy on qol consists of non randomised studies , often of small size , which could be subject to selection bias , and in which neither surgery , radiotherapy , nor systemic treatments were subject to prespecified quality assurance . 
for example , the start trial studied the late effects of different schedules of radiotherapy at 5 years and found that up to a third of women reported moderate or notable pain in the arm and shoulder and more than 10% had arm or hand swelling.12 the trial included a small number of patients who had mastectomy ( about 20% ) and although the qol results are consistent with ours , they are not directly comparable because only 10% of patients had chemotherapy and 20% had regional nodal irradiation in addition to breast or chest wall radiotherapy . 
the experience of breast or arm symptoms over 5 years represents chronic morbidity that has stronger asso ciation longterm qol , making these than cosmesis with important outcomes in clinical trials.28 the moving beyond cancer psychosocial intervention trial27 studied the qol of 558 women with stage 1 and 2 breast cancer treated with surgery alone ( breastconserving surgery or mastectomy ) , surgery with radio therapy , or surgery followed by chemotherapy and radiotherapy over 1 year , using the sf36 questionnaire . 
however , the measures of qol differ from those used in our study and details of chemotherapy regimens and staging were not available in the absence of case record review.27 a similar pattern of improvement in a range of symptoms and qol measures in the first year after diagnosis was observed in a cohort study of 285 women with early breast cancer , treated with surgery ( > 20% of patients had mastectomy ) , adjuvant radiotherapy ( 74% of patients ) , and systemic therapy ( > 30% of patients ) .29 finally , we found that younger women reported worse body image ( if younger than 45 years of age ) and anxiety problems ( if younger than 70 years )  . 
this finding is supported by other breast cancer qol studies , is con cordant with clinical experience , and emphasises the need for targeted psychological in younger women.11 , 30 younger women also reported worse chest wall symptoms ( including pain )  . 
in a populationbased prospective study of more than 3000 patients , 31 persistent pain following breast surgery ( breast conserving or mas tectomy ) was reported by half of the patients and the pain was more common after adjuvant radiotherapy and in younger women . 
the same finding was also reported in a randomised trial of radiotherapy after breastconserving surgery.13 , 31 the wide variation in reports ( 2560% ) might relate to varying definitions of pain , different methods of pain assessment , and mixture of surgery and adjuvant therapy . 
we do not know the reasons for the low rates of patient consent in some centres , but it might be related to availability of local resources ( dedicated clinical research nurses )  . 
furthermore , guidelines on surgery , radiotherapy , and systemic therapy were standardised in the protocol , so any variations in these treatment modalities between treatment groups are unlikely to affect the results . the main limitation of this substudy is not having a true pretreatment baseline qol assessment , because all patients were randomly assigned after mastectomy . 
the low qol scores at the time of randomisation might be explained by the recent breast cancer diagnosis and the surgical procedure , and the subsequent improvement in almost all scores is to be expected . 
we did not record qol scores during or shortly after the allocated radiotherapy treatment , so any differences in acute symptoms between groups , which might predict later toxicity , have not been captured . 
additionally , because the main trial is ongoing and the locoregional control and survival status of the patients in this substudy are not known to us , it is possible that patients who had relapsed or died might have had different patterns of qol than those who survived . notably , a larger proportion of participants in the qol substudy received the dose fractionation schedule as 40 gy in 15 fractions ( 68% ) than in the main trial ( 52% ) , in which a larger proportion received 50 gy in 25 fractions ( 27% in the main trial vs 11% in the substudy )  . 
this difference reflects the variations between standard practice in uk centres versus eortc centres at the time of the trial . in this 2year analysis , we have not investigated any effect of fractionation on the qol outcomes . 
however , because the clinical significance of the increased chest wall symptoms in the radiotherapy group at 2 years might be relatively low , we do not expect a major clinical impact of fractionation at this early timepoint . 
the effects of radiation dose fractionation and technique and radiation dose parameters on organs at risk will be the subject of a more detailed analysis to be performed in the radio therapy group , including assessment of toxicity ( phy sician scoring )  . 
the results will be reported in a separate publication , focusing on the specific technical aspects of the radiotherapy . this report presents a preplanned analysis 2 years after randomisation , with the main qol analysis planned at 5 years and qol data to be collected for 10 years to capture late adverse events . 
the recent us guidelines7 on postmastectomy radiotherapy empha sise the importance of shared decision making between physician and patient in weighing up the benefits and toxicity of treatment in patients with one to three positive nodes undergoing axillary node clearance . 
late radiotherapyinduced toxicity not seen within the first 2 years ( eg , progressive chest wall fibrosis or increased cardiac toxicity due to the com bination of radiotherapy and anthracyclinebased chemotherapy ) might be detected on longerterm followup and should be captured in our 5year and 10year analyses . 
however , we recognise that late cardiac toxicity from radiotherapy could occur beyond 10 years . the effect of postmastectomy radiotherapy on 10year survival , the primary endpoint of the main supremo trial , will not be known before 2023 . 
in the meantime , the decision to administer or omit postmastectomy radiotherapy can be considered preference sensitive for patients in the supremo trial risk category of one to three positive lymph nodes , because both options are legitimate . 
patients will be in a better position to make a value judgment on what they consider relevant for them , given the data on various qol domains presented in this report . 
both physicians and patients could thus be helped when weighing up the individual estimates of possible benefits of radiotherapy against the effect of post mastectomy radiotherapy on toxicity and qol endpoints . in conclusion , chest wall radiotherapy led to more chest wall symptoms up to 2 years after randomisation , but the difference was small and unlikely to be clinically significant . 
however , indications of worse qol scores for anxiety , body image , and chest wall symptoms in younger women irrespective of whether or not they received radiotherapy warrants further investigation . 
longerterm followup at 5 years and 10 years will be needed to see if these early findings in qol are sustained . contributors gv , ljw , sw , jmd , ihk , and nsr were involved in the study design . 
gv , ihk , and nsr gave final approval of the manuscript . declaration of interests gv has received research grants from the national institute of health research ( nihr ) , cancer research uk , and yorkshire cancer research , and personal fees from roche , novartis , and eisai . 
nsr has received research grants from the dutch cancer society and the european 1528 vol 19 november 2018 articles 3 cardoso f , vant veer lj , bogaerts j , et al . 
 we thank the medical research council ( eme 09 / 800 / 31 ) , european organisation for research and treatment of cancer , cancer australia , the dutch cancer society , and the trustees of the hong kong and shanghai banking corporation ( hsbc ) for funding the study . 
 we acknowledge the support of the staff at the information and statistical division at national services scotland and specifically kathleen riddle ( principal trial manager ) ; penelope hopwood ( the christie hospital , manchester , uk ) , initial chief investigator for the quality of life substudy ( who has subsequently retired ) ; the scottish cancer trials breast group , under whose auspices the trial was run ( chair : iain macpherson ) , the trial management group , the trial steering committee ( chair : barry hancock , university of sheffield , sheffield , uk ) , and the data monitoring and ethical committee ( chair : chris frost , london school of hygiene & tropical medicine , london , uk )  . 
we also thank the national institute for health research cancer research networks in england and their equivalent nhs research and developmentfunded networks in scotland , wales , and northern ireland for inkind support . for more on how brexit will affect health services in the uk see lancet 2019 ; 393 : 94958 for the no - deal brexit practical guidance from the rcr see sites / default / files / no_deal_ brexit_planning_guidance_ for_nuclear_medicine_teams_ march_2019.pdf for more on the privatisation of imaging services in the nhs see society / 2019 / mar / 06 / nhscancer - centre - loses - scanningcontract - to - private - firm brexit , radiology , and nhs privatisation : a tragedy for frontline care ? the uks exit from the european union ( eu ) is arguably one of the worst self - inflicted harms any country has done to itself in peace - time . 
in a health policy piece in the lancet in 2017 , and updated in february , 2019 , fahy and colleagues state that brexit will have negative consequences for the uks leadership and governance of health , in both europe and globally . 
an editorial in the lancet on march 2 , 2019 , went further , emphasising : there is no good news for the nhs ( national health service ) ...in all scenarios , depletion of the nhs workforce is inevitable , care for uk nationals living in the eu is uncertain , and access to medicines , vaccines , and devices hangs in the balance . 
indeed , the provision of diagnostic imaging and radiopharmaceuticals for patients with cancer is one key specialty in which the consequences of brexit are multiple and potentially catastrophic . on march 5 , 2019 , the uk royal college of radiologists ( rcr ) , in collaboration with the british nuclear medicine society and the uk radiopharmacy group , issued practical guidance to nuclear medicine physicians on how to manage brexit in a no - deal scenario . 
the advice states that there might be delays to deliveries ; nuclear medicine teams should try to keep their workloads light in the first week postbrexit ; teams should consider the use of alternative radiopharmaceuticals where possible ; and certain patients should be prioritised over others . 
the uk government has stated that , in the event of a no - deal , the uks major radioisotope suppliers have committed to 6 - month air freight contracts as a contingencyrather than run the risk of road transport delays . 
inevitably , this contingency raises major concerns about the increased delivery costs and who will pay for them , and the problems caused by the time of day in which a delivery is made for radiopharmaceuticals that need processing on - site prior to use . the rcr guidance also gives specific advice about radionuclide therapies , and notesrather worryingly that it is only aware of one supplier that is confident of being able to continue to supply therapeutics on a specific schedule after brexit . 
the potential for medical error or waste of radiotracers and radiotherapeutics are therefore manifestly high post - brexit . and , if these challenges in access to essential reagents werent enough to destabilise health care in the uk , new developments in the increasing privatisation of the nhs certainly will . 
an announcement on march 6 , 2019 , stated that the churchill hospital in oxford , uk , will no longer carry out its own pet - ct services ; rather , the tender has been given to inhealth , a private company . 
shockingly , nhs england has invited profit - driven companies to bid against nhs trusts for pet - ct services in 11 different regions across the country , including major teaching hospitals such as kings college hospital in london and the christie hospital in manchester . 
 most importantly , privatisation of frontline patient services necessitates a moment to reflect on whether this is truly in the best interests of patients and what consequences it might have on the safety and quality of care . 
short - term , fragmented , financial gains often do not translate in to long - term advantages in complex health - care systems . patients with cancer in the uk face substantial challenges in accessing the best care . 
despite attempts to reduce such inequities , they persist in the form of geographical limitations , resource allocation , availability of various specialised services , access to cancer medicines , a shortfall in the numbers of consultants and other health - care professionals , and now , two additional barriers to the quality of care : increasing privatisation of frontline services , and a maelstrom of unknowns related to brexit and its impact on all aspects of the nhs . 
 the lancet oncology vol 20 april 2019 editorial correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections k for highlights from asco 2018 see news page 865 for a study on sex differences in immunotherapy responses see articles lancet oncol 2018 ; 19 : 73746 for the study on the effects of antibiotics use during immunotherapy see proc am soc clin oncol 2018 ; 36 ( suppl 15 ) : 3010 for a viewpoint on pulmonary toxicity in cancer immunotherapy see lancet respir med 2018 ; 6 : 47278 for the report of rapid progression of acute adult t - cell leukaemialymphoma see n engl j med 2018 ; 378 : 194748 immunotherapy : hype and hope as the dust settles after a busy week at the 2018 american society of clinical oncology ( asco ) annual meeting ( june 15 , 2018 ; chicago , il , usa ) , there is an opportunity to reflect on the impact of the largest cancer congress of the year . 
among this years highlights were a predictive 21 - gene expression assay that suggests most women with early - stage breast cancer might not need chemotherapy , and findings that pre - operative chemoradiotherapy improves disease - free survival for patients with pancreatic cancer . 
 the most visible recipient of media scrutiny was an account of adoptive transfer of autologous tumourinfiltrating lymphocytes ( targeting somatic mutations ) , which was reported to result in a complete durable regression in a patient with advanced breast cancer with liver metastases , and thus was hailed as a miracle cure by some media outlets , garnering worldwide publicity . 
 equally well - covered was the phase 3 keynote - 042 trial , which showed pembrolizumab was more effective than chemotherapy as a first - line treatment for patients with non - small - cell lung cancer . 
equally , a retrospective study presented at asco 2018 found antibiotic use during treatment with checkpoint inhibitors reduced overall and progression - free survival in patients with advanced cancer , potentially due to changes in microbiota , implicating other important unknown factors in the host response to treatment . 
individual patient immunity undoubtedly leads to variation , but outcomes from a proportion of responders and super - responders can dominate top - line data , potentially masking many other patients with less striking results . 
this individual variance is also reflected in the failed attempts to find and validate predictive markers of response to immunotherapy : pd - 1 or pd - l1 expression , for example , does not seem to correlate with response , despite earlier data suggesting these markers were key targets for checkpoint inhibitors , highlighting just how little we understand the true complexity of the immune system and the mechanisms of action of immunotherapy . 
 cancer immunotherapy has been reported to result immune - related adverse events such as in various opportunistic infection or pulmonary toxicity and , unexpectedly , the rapid progression of disease , such as acute adult t - cell leukaemialymphoma , as well as an array of other side - effects not typically encountered with conventional chemotherapy . 
in view of the varied mechanisms of action , the specific adverse sequelae associated with these drugs warrant further investigation , especially since they are now being used in many disease settings without long - term follow - up data . 
although there is great promise in immunotherapies , we must not let the excitement of such treatments overshadow their potential for har clinicians , researchers , and patients must be wary of the hyperbole associated with certain limitations professionally marketed studies , and the of off - label use of new drugs . 
when the associated media coverage of therapies gives patients unrealistic expectations of outcomes , it is increasingly difficult for clinicians to deny immunotherapy , particularly as a last hope for those patients for whom other treatments have failed ; however , caution must be exercised , with first do no harm being central in decision - making . 
 how can we ensure that hype and promotion do not overshadow the real work at the heart of these large congresses ? it is easy to get swept away by stories of miracle cures and the expanse of shiny stands in the indeed , commercial companies exhibition halls . 
 and some institutionsexcel in the promotion of results of individual drugs or techniques , but the research community must continue to design rigorous investigations that ensure the highest level of reliable , high - quality evidence is generated to inform evidencebased cancer treatment that improves care for all patients , not just specifically selected super - responders . 
 the lancet oncology vol 19 july 2018 editorial infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
han admitted that , while a researcher at iowa state university ( ames , ia , usa ) , he added human antibodies to blood from rabbits that had been injected with an experimental vaccine , which gave the impression that the vaccine worked . 
for example , in 2014 , independent bloggers were key to reporting the inability of researchers to reproduce published data that purported to show that somatic cells could be reverted to a pluripotent state with simple cellular stress - inducing agents such as an acid bath . 
as a result , several papers were retracted , and the researchers involved at the riken center for developmental biology ( kobe , japan ) were charged and found guilty of misconduct . 
however , online commentary can be prone to sensationalism and undisclosed bias , due to lack of coordination , overarching policies , and readily available context . self - monitoring at the research integrity institutional level , monitored by funding bodies and research institutions , with policies and practices as divergent as the countries they reside in the usa , several funding agencies have their own inspectors who have varying levels of power to examine allegations of research misconduct . 
 by contrast , the o ce of research integrity ( ori ) can only oversee investigations initiated by institutions that employ researchers funded by the national institutes of health ( nih ) , but it cannot directly investigate the if misconduct is found , the ori can rescind nih funds or refer the case to the department of justice . 
recent events in the case of duke university ( durham , nc , usa ) researcher anil potti , have shown that this dependence on robust institutional oversight is essential . 
subsequent patients being revelations , such as pottis falsi cation of his credentials , and retraction of several publications , resulted in the broadening of initial investigations of his conduct into a full misconduct review . 
the duke university review into the potti case is still ongoing and the full report of the investigation has not yet been released , nearly 5 years after it began . 
these di erences have been addressed by several bodies issuing global guidelines for research integrity , but the enforcement of these guidelines remains uneven and di cult to implement or monitor . 
 the lancet oncology vol 16 august 2015 corrections published online march 25 , 2015 s1470 - 2045 ( 14 ) 71115 - 5 correction to lancet oncol 2013 ; 14 : e374 correction to lancet oncol 2015 ; 16 : e163 correction to lancet oncol 2015 ; 16 : 447 , 448 weller m , p ster sm , wick w , hegi me , reifenberger g , stupp r . 
the rst sentence should read : exposure to passive smoke among never smokers does not seem to increase the chances of acquiring somatic mutations in genes linked to non - small - cell lung cancer in smokers , a new study shows . 
 vorinostat in patients with advanced malignant pleural mesothelioma who have progressed on previous chemotherapy ( vantage - 014 ) : a phase 3 , double - blind , randomised , placebocontrolled trial . 
lancet oncol 2015 ; 16 : 44756in the a liation section , p bass should be listed at netherlands in the funding cancer section in the summary and in the a liations , merck & co has been changed to merck & co , inc . 
 lancet oncol 2015 ; 16 : 54149in the key of gure 2 of this article , the boxes should indicate patients who were ct positive for disease , not those who were circulating tumour dna positive for disease . 
this correction has been made to the online version as of april 30 , 2015 , and the printed version is correct . vol 16 may 2015 e199 correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
maintenance therapy with vinflunine plus best supportive care versus best supportive care alone in patients with advanced urothelial carcinoma with a response after first - line chemotherapy ( maja ; sogug 2011 / 02 ) : a multicentre , randomised , controlled , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 67281in this article , the declaration of interests should read jg - d reports personal fees from astellas , janssen ; grants and personal fees from astrazeneca , pfizer , pierre fabre , merck , bioclin , bristol myers squibb , novartis , and msd ; grants , personal fees , and non - financial support from roche ; and grants from gammamabs , outside the submitted work . 
af reports grants from astellas , astrazeneca , pierre - fabre ; personal fees and non - financial support from sanofi , janssen , bayer , and roche , outside the submitted work . 
bp - v reports personal fees from astellas pharma , novartis , pfizer , pierre fabre , bayer , sanofi , bristol - myers squibb , ipsen , and janssen - cilag , during the conduct of the study . 
jaa reports grants and personal fees from glaxosmithkline and novartis ; personal fees and nonfinancial support from jansen cilag ; grants , personal fees and non - financial support from bms ; personal fees from pfizer , roche , and eusa ; grants from sanofi and pierre fabre , outside the submitted work . 
nl reports personal fees from pfizer , sanofi , pierre fabre , roche , ipsen , pharma mar , bms , bayer , astrazeneca , astellas , and msd , outside the submitted work . 
jcv - g reports personal fees from pfizer , astellas , janssen , msd , bayer , roche , bristol , astrazeneca , boehringer , pierre fabre , novartis , ipsen , celgene , lilly , merck , sanofi , and mundipharma , outside the submitted work . 
bm reports personal fees and non - financial support from pfizer and janssen ; personal fees from novartis , astellas oncology , bms , sanofi , ipsen , bayer ; and grants and personal fees from roche , outside the submitted work . 
agda reports advisory board , consultancy and speaker honoraria or travel support from pierre fabre , roche , bristol - myers squibb , msd , pfizer , novartis , bayer , janssen , sanofi , astellas , eusa pharma , and eisai ; and research funding from astellas . 
dc reports personal fees from janssen , roche , astellas , msd , ipsen , pfizer , bms , bayer , astrazeneca , novartis , lilly , sanofi , pierre fabre , and boheringer , outside the submitted work . 
eg reports grants from pierrefabre , during the conduct of the study ; personal fees and non - financial support from janssen , pfizer , bayer , ipsen , novartis , bms , rovi ; personal fees from menarini and leo pharma ; and nonfinancial support from pierre - fabre , outside the submitted work . 
ua reports non - financial support from novartis , pierre fabre , and ipsen ; personal fees from bayer , janssen , astellas , and pfizer ; and personal fees and nonfinancial support from sanofi , roche , and bms , outside the submitted work . 
 xgdm reports personal fees from pfizer , ipsen , bms , roche , lilly , pharmamar , eusapharma , and pierre fabre ; and grants from astrazeneca , outside the submitted work . 
md has participated in advisory boards , consultancy , and speaker bureaus for roche , bristol - myers squibb , msd , pfizer , janssen , sanofi , astellas ; and received travel and accommodations expenses from roche , astellas , janssen , bayer , and lilly . 
jp has received honoraria as a consultant on advisory boards from pfizer , astellas , janssen , msd , bayer , roche , bms , boehringer , astrazeneca , ipsen , novartis , eusa pharma , eisai , and sanofi ; and as speaker from kyowa , pierre - fabre , celgene , lilly , and merck . 
 rm - b has served as a consultant or on advisory and / or speakers bureaus for sanofi aventis , bayer , janssen , astrazeneca , merck sharp & dohme , and asofarma ; and received travel and accommodations expenses from roche , sanofi aventis , astellas , janssen , merck sharp & dohme , bayer , pharmacyclics , clovis oncology , and lilly . 
jlp - g reports non - financial support from pierre fabre , during the conduct of the study ; non - financial support from roche , bms , and msd , outside the submitted work . 
jb reports grants and personal fees from pfizer , merck , bms ; personal fees from genentech , astrazeneca , pierre - fabre ; and grants from takeda , during the conduct of the study . 
 this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1493503 zackrisson s , lng k , rosso a , et al . 
 lancet oncol 2018 ; 19 : 1493503 in this article , in table 1 and table 4 , the age groups should have been listed as follows : 4049 , > 4959 , > 5969 , and > 69 . 
the title and legend of figure 2 should have read as follows : number of false - positive results among participants over the trial period who were recalled only on digital breast tomosynthesis and digital mammography , respectively . 
 these corrections have been made to the online version as of jan 3 , 2019 . vol 20 january 2019 corrections corrections correction to lancet oncol 2012 ; 13 : 817 , 818 , 822 correction to lancet oncol 2014 ; 15 : 1195206 correction to lancet oncol 2015 ; 16 : 52 shen q , fan j , yang x - r , et al . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
we aimed to establish the short - term safety of immediate implant - based breast reconstruction performed with and without mesh , to inform the feasibility of undertaking a future randomised clinical trial comparing different breast reconstruction techniques . methods in this prospective , multicentre cohort study , we consecutively recruited women aged 16 years or older who had any type of immediate implant - based breast reconstruction for malignancy or risk reduction , with any technique , at 81 participating breast and plastic surgical units in the uk . 
outcomes of interest were implant loss ( defined as unplanned removal of the expander or implant ) , infection requiring treatment with antibiotics or surgery , unplanned return to theatre , and unplanned re - admission to hospital for complications of reconstructive surgery , up to 3 months after reconstruction and assessed by clinical review or patient self - report . 
the study is registered with the isrctn registry , number isrctn37664281 . findings between feb 1 , 2014 , and june 30 , 2016 , 2108 patients had 2655 mastectomies with immediate implant - based breast reconstruction at 81 units across the uk . 
1376 ( 65% ) patients had reconstruction with biological ( 1133 [ 54% ] ) or synthetic ( 243 [ 12% ] ) mesh , 181 ( 9% ) had non - mesh submuscular or subfascial implants , 440 ( 21% ) had dermal sling implants , 42 ( 2% ) had pre - pectoral implants , and 79 ( 4% ) had other or a combination of implants . 
of these patients , 182 ( 9% , 95% ci 810 ) experienced implant loss , 372 ( 18% , 1620 ) required re - admission to hospital , and 370 ( 18% , 1620 ) required return to theatre for complications within 3 months of their initial surgery . 
the rates of all of these complications are higher than those in the national quality standards ( < 5% for re - operation , re - admission , and implant loss , and < 10% for infection )  . interpretation complications after immediate implant - based breast reconstruction are higher than recommended by national standards . 
a randomised clinical trial is needed to establish the optimal approach to immediate implantbased breast reconstruction . funding national institute for health research , association of breast surgery , and british association of plastic , reconstructive and aesthetic surgeons . copyright 2019 the author ( s )  . 
the mesh is sutured between the lower edge of the pectoralis muscle and the chest wall to create a larger subpectoral pocket that can accommodate a fixed - volume implant at the time of the initial surgery . 
the remaining studies comprised 40 comparative studies and 20 case series , all of which were at high risk of bias . we did another pubmed search in april , 2018 , and identified one small randomised clinical trial that compared standard two - stage expander - implant reconstruction with mesh - assisted , single - stage , direct - to - implant breast reconstruction . 
the frequency of complications in the single - stage , mesh - assisted , direct - to - implant group was significantly higher than that in patients receiving two - stage expander implant reconstruction , and the study was stopped prematurely . 
these studies did not show any differences between products , but were small and underpowered . added value of this study this prospective cohort study of more than 2000 patients having immediate implant - based breast reconstruction in the uk provides high - quality , real - world data regarding the short - term safety outcomes of different implant - based techniques with and without mesh . 
the frequency of key complications , including implant loss , infection , re - admission , and re - operation for complications of reconstructive surgery , was much higher than anticipated ; although adverse outcomes were associated with smoking and increased body - mass index , there was no association with the use or type of mesh in this non - randomised study . 
these findings support the need for a future pragmatic randomised clinical trial to determine the most clinical and cost - effective technique of implant - based breast reconstruction . implications of all the available evidence complications after immediate implant - based reconstruction with and without mesh are high , and patients should be carefully counselled regarding their surgical options . 
 urgent work will also be necessary to determine how the high incidences of complications shown in this study could be reduced . the practice of patients and health - care providers . 
these meshes differ notably in price and , in the absence of comparative evidence , product selection is largely dependent on surgeon preference . immediate implant - based breast reconstruction has evolved further with the introduction techniques.7 these techniques involve wrapping the implant in mesh and placing it on top of , rather than underneath , the pectoralis muscle . 
this pre - pectoral technique might further improve outcomes for patients by reducing postoperative pain and preventing implant animation , the upward movement of the implant seen when the pectoralis muscle contracts.7 so - called muscle - sparing despite the widespread adoption of mesh - assisted techniques into practice , evidence to support the proposed benefits of mesh is lacking.710 a multicentre dutch randomised controlled trial11 showed significantly increased numbers of complications in single - stage , direct - to - implant reconstruction with mesh compared with standard two - stage expander - implant techniques . 
 the study was criticised because the participating surgeons had limited experience with the technique , 12 but further analysis did not identify a learning curve effect.13 however , other large multicentre prospective studies have not shown a significant difference in incidence of com plications or patient - reported outcomes between single - stage direct - to - implant and two - stage techniques , 14 or between two - stage expander - implant reconstruction done with and without acellular dermal matrix.15 although these findings are supportive of the technique , there remains the need for high - quality vol 20 february 2019 articles evidence from a randomised study to support practice . 
 a small randomised clinical trial16 that compared biological single - stage synthetic mesh direct - to - implant reconstruction was underpowered and insufficiently well designed to generate meaningful results . and there is therefore a need for high - quality research to establish the safety and effectiveness of mesh in immediate determine what mesh should be recommended , and , as practice evolves , to determine if the implant should be placed on top of or underneath the pectoralis muscle.7 implant - based breast reconstruction , randomised clinical trials are ideally needed , but randomised clinical trials in breast reconstruction are challenging because of patient and surgeon preference17 and previous trials have closed prematurely because not enough patients were able to be recruited.18 , 19 careful pretrial work is therefore needed to ensure that a future randomised clinical trial is well designed and addresses questions that are important to patients and the reconstructive community . ibra ( implant breast reconstruction evaluation ) 20 is a four - phase study that aims to inform the feasibility , design , and conduct of a future trial in immediate implantbased breast reconstruction . 
results from phase 1 ( a national practice questionnaire to understand current practice ) were previously reported.21 , 22 here we report the primary endpoint for phase 2 , a prospective multicentre national study to determine the short - term clinical outcomes of different approaches to immediate implantbased breast reconstruction in the uk and inform the selection of comparators and sample size for a future randomised clinical trial . implant - based breast recon struction methods study design and participants for this prospective , multicentre ibra study , we invited all uk breast or plastic surgical units performing immediate participate in the study , through the uk trainee collaborative research network and two professional associations , the association of breast surgery and the british association of plastic reconstructive and aesthetic surgeons . 
81 centres participated in the study . women aged 16 years or older , who had a mastectomy and immediate implant - based breast reconstruction using any technique for malignancy or risk reduction at participating centres , were consecutively recruited to the study . 
patients were excluded if they had reconstruction with an implant in combination with a tissue flap ( eg , latissimus dorsi flap and implant ) , had delayed reconstruction , or had revisional surgery . ethics approval was not required , as defined by the hra decision tool . 
 outcomes assessed against each participating centre was required to obtain local audit approvals and register the study before commencing study recruitment , consistent with the methods of previously reported multicentre prospective trainee collaborative studies . 
patient consent was not required for routine clinical data collection , but patients provided written informed consent to receive patient - reported outcome questionnaires , in keeping with the methods employed in the uk national mastectomy and breast reconstruction audit.24 all data were recorded in an anonymised format on a secure web - based database , redcap.25 procedures we prospectively identified eligible patients from clinics , multidisciplinary team meetings , and theatre lists . 
 simple demographic , comorbidity , and operative data were collected for each participant . all patients had skin or nipple - sparing mastectomy followed by immediate implant - based breast reconstruction . 
implants or tissue expanders could be placed under the pectoralis muscle ( subpectoral ) with or without biological or synthetic mesh , or on top of the muscle ( pre - pectoral ) supported by mesh . 
reconstructions were considered to be two - stage if a temporary expander was placed at the time of the initial mastectomy and a second procedure was planned to insert a definitive implant at a later date . precise details of the techniques used varied by surgeon , but broadly , for submuscular reconstructions , a tissue expander was inserted in a pocket created under the pectoralis muscle . 
serratus fascia could be raised to provide complete expander coverage , or the lateral aspect of the expander could be left subcutaneous as per surgeon preference . sub - pectoral reconstruction with mesh involved releasing the lower boarder of the pectoralis muscle from the chest wall and suturing the mesh to the free edge of the muscle . 
a definitive fixed - volume implant , adjustable implant , or tissue expander was then inserted according to surgeon preference and the mesh either sutured at the level of the inframammary fold or tucked under the implant , depending on the product used . 
for dermal sling reconstruction , the pectoralis muscle was detached in a similar way and the lower mastectomy flap de - epithelialised and sutured to the free muscle edge to provide coverage of the lower pole of the for more on redcap see for more on the hra decision tool see decisiontools.org.uk / research 256 vol 20 february 2019 articles implant . 
it is not standard practice to use mesh in this procedure . finally , for pre - pectoral reconstruction , the pectoralis muscle was not disturbed , but a fixed - volume implant , adjustable tissue expander completely or partially wrapped in mesh ( depending on surgeon preference and product selection ) was placed in the mastectomy cavity and sutured into place . implant , or temporary in all cases , perioperative and postoperative antibiotics and drains were used according to local policy or surgeon preference . complication and oncological data were collected by the clinical team at 30 days and 3 months after reconstruction by clinical or case - note review , or both , depending on when the patient returned for follow - up . participants were approached in the clinic or during their hospital stay to obtain consent for patient - reported outcome assessment at 3 months after surgery . 
the patient - reported outcome was a modified version of the 3 - month questionnaire used in the uk national mastectomy and breast reconstruction audit ( nmbra ) and included patient self - report of complications occurring in the 3 months after surgery.24 questionnaires were sent centrally by post or e - mail , depending on patient preference , with a reminder sent 1 month after the initial questionnaire if no response was received . 
 patient satisfaction was also assessed at 18 months after surgery.20 analyses are ongoing and these results will be reported elsewhere . outcomes on the basis of published national quality standards for breast reconstruction derived from the nmbra , 23 we prespecified four key outcomes to assess the short - term safety of different approaches to immediate implantbased breast reconstruction.20 we chose these outcomes because it was anticipated that a safety outcome might be the primary endpoint of a future trial and equivalence in a non - randomised study was important in informing the selection of potential comparators for this study . 
the outcomes were defined implant loss ( the unplanned removal or loss of the implant as a result of infection or other complication ) , infection ( the presence of a hot , red breast requiring treatment with antibiotics , surgery , or both ) , re - admission ( any unplanned re - admission to hospital after discharge for any complication of surgery ) , and reoperation ( any return to the operating theatre for a complication within 3 months of the reconstruction procedure )  . 
any implant loss , infection , re - admission , or re - operation occurring at any timepoint within the first 3 months of the initial reconstruction that was assessed by clinical review or patient self - report was considered an event and included in the analysis . we identified potential risk factors for each of these key outcomes using a prespecified exploratory risk - factor analysis . 
we identified specific variables of interest a priori from the published literature and expert opinion , and included the following patient - related and procedurerelated factors : age , body - mass index ( bmi ) , smoking ( current smokers vs others ) , previous radiotherapy to the ipsilateral breast ( yes vs no ) , receipt of neoadjuvant chemotherapy ( yes vs no ) , bilateral surgery ( yes vs no ) , mastectomy type ( nipple - sparing vs other mas tectomy types ) , type of implant or expander used ( fixed - volume vs adjustable implants or expanders ) , and type of immediate implant - based breast reconstruction performed . 
we classified reconstruction procedures according to the mode of lower pole coverage as being : submuscular or subfascial without mesh ; dermal - sling procedures using the patients own tissue ; biological mesh - assisted ( including acellular dermal matrix and non - dermal biological products ) ; synthetic mesh - assisted ; pre - pectoral if the implant was placed on top of the pectoralis muscle with or without mesh ; and other if a combination of techniques was used ( eg , dermal sling and mesh )  . for quality assurance purposes , the principal investigator at each participating site was asked to independently validate the primary outcomes for all study participants at 3 months and to check complete case ascertainment . statistical analysis because we aimed to inform the design of a future randomised clinical trial , the study was powered to establish parameters required for a sample size calculation and to inform further aspects of trial design , such as entry criteria for the future trial . therefore required at the time of study design , four clinical outcomes ( implant loss , re - admission , re - operation , and infection ) were considered to be potential primary outcomes in a randomised controlled trial , and a wide range of treatment approaches for immediate implant - based breast reconstruction were routinely offered.22 a large sample was to estimate , with reasonable precision , the incidence of the four clinical outcomes of interest ( implant loss , re - admission , reoperation , and infection ) within treatment approaches , and to determine how implant procedures are performed and any variation in patient selection for each of these approaches . 
a sample size of 197 participants would allow a two - sided 95% ci for a single proportion , assumed to be 009 , extending from 005 to 013 , using the large sample normal approximation . 
allowing for the 15% loss to follow - up at 3 months reported in the nmbra , an analysis of implant loss at 3 months required at least 235 patients to be recruited to inform a future trial with implant loss as a primary outcome . 
to determine how implant procedures are performed , centres participating in a national practice questionnaire vol 20 february 2019 articles 2217 patients entered into redcap database 2161 had surgery during study period 56 excluded 34 surgery outside study period 22 operation date not recorded 3 no immediate implant - based breast 53 excluded reconstruction 50 procedure not reported 2108 included in study 181 submuscular or subfascial without mesh 440 dermal sling 1133 biological mesh 243 synthetic mesh 42 pre - pectoral 64 other 15 not known 27 lost to follow - up 2081 with 3 - month follow - up included in 3 - month outcome analysis 180 submuscular or subfascial without mesh 436 dermal sling 1121 biological mesh 236 synthetic mesh 42 pre - pectoral 63 other figure : trial profile for patients with two implant - based reconstructions in which technique differed by breast ( n = 10 ) , these patients are summarised in both groups , depending on the approach used , and once in the total . 
variations of approaches per breast within patient were : biological mesh and dermal sling ( n = 3 ) , biological mesh and synthetic mesh ( n = 1 ) , dermal sling and submuscular or subfascial ( n = 4 ) , other and submuscular or subfascial ( n = 1 ) , and other and synthetic mesh ( n = 1 )  . ( n = 81 ) 21 , 22 were eligible to participate . 
all analyses are based on the number of patients , not the number of implants . we did the analysis according to a prespecified statistical analysis plan approved by the trial steering group . 
we did no formal statistical testing . we established the proportion and 95% ci of patients for each of the four key clinical outcomes to compare our findings against those reported in the nmbra24 and published national quality standards.23 we did a prespecified risk - factor analysis using multivariable logistic regression . 
variables of interest included patient age , bmi , smoking status , previous radiotherapy to the ipsilateral breast , receipt of neoadjuvant chemotherapy , bilateral surgery , nipple - sparing versus other mastectomy types , use of fixed - volume versus adjustable implants or expanders , and type of immediate implant - based breast reconstruction performed . data were considered missing at random ( appendix p 2 ) and therefore no missing data items were imputed . 
we considered this approach as unlikely to lead to bias because all included risk factors were measured once per patient.26 we checked linearity for continuous variables for all four logistic models using locally estimated scatterplot smoothing ( loess ) smoothed - line plots . 
we used sas ( version 9.3 ) for all analyses . this study was registered as an international standard randomised controlled trial , number isrctn37664281 , and the protocol was published in 2016.20 role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to the data in the study and had final responsibility for the decision to submit for publication . results between feb 1 , 2014 , and june 30 , 2016 , 2217 records were entered onto the redcap database . 
of these , 109 ( 5% ) were excluded : 34 patients had surgery outside the study period , 22 records did not include an operation date , 50 records provided no information regarding the type of surgery performed , and three patients did not have an immediate implant - based breast reconstruction . 
further details about unit recruitment are in the appendix ( pp 37 )  . biological mesh - assisted reconstruction was the most commonly performed procedure , with 1133 ( 54% ) of 2108 patients undergoing this technique . 
fewer patients had synthetic mesh - assisted immediate implant - based breast reconstruction ( 243 [ 12% ] ) , and 181 ( 9% ) received traditional subpectoral reconstruction without mesh . 
 subpectoral reconstruction with a dermal sling was done in approximately a fifth of patients ( 440 [ 21% ] ) and prepectoral reconstruction with mesh ( 42 [ 2% ] ) was done in the latter stages of the study . 
 * for patients with two implant - based reconstructions in which technique differed by breast ( n = 10 ) , these patients are summarised in both applicable columns , depending on the method used , and once in the total column . 
variations of approaches per breast within patient were biological mesh and dermal sling ( n = 3 ) , biological mesh and synthetic mesh ( n = 1 ) , dermal sling and submuscular or subfascial ( n = 4 ) , other and submuscular or subfascial ( n = 1 ) , and other and synthetic mesh ( n = 1 )  . 
 * for patients with two implant - based reconstructions in which method differed by breast ( n = 10 ) , these patients are summarised in both applicable columns , depending on the method used , and once in the total column . 
variations of approaches per breast within patient were biological mesh and dermal sling ( n = 3 ) , biological mesh and synthetic mesh ( n = 1 ) , dermal sling and submuscular or subfascial ( n = 4 ) , other and submuscular or subfascial ( n = 1 ) , other and synthetic mesh ( n = 1 )  . 
variable collected on a per - breast basis ; for patients with two implant - based reconstructions , with data for one breast and not the other , that patient is classified according to the non - missing data as indicated in the applicable footnote . 
 * * combinations of type of mastectomy within patients with two implant - based reconstructions with different types per breast were skin - sparing mastectomy and skin and nipple - preserving mastectomy ( n = 15 ) , skin - sparing mastectomy and reduction ( wise ) pattern ( n = 7 ) , skin - sparing mastectomy and other ( n = 3 ) , skin and nipple preserving and reduction ( wise ) pattern ( n = 2 ) , skin and nipple preserving and other ( n = 4 ) , reduction ( wise ) pattern and other ( n = 1 )  . 
combinations of location of incision within patients with two implant - based reconstructions with different types per breast were elliptical removing nac and inframammary ( n = 1 ) , elliptical removing nac and lateral ( n = 4 ) , elliptical removing nac and other ( n = 3 ) , elliptical removing nac and peri - areolar ( nipple preserving ; n = 3 ) , elliptical removing nac and wise - pattern ( n = 1 ) , inframammary and lateral ( n = 1 ) , inframammary and other ( n = 2 ) , inframammary and peri - areolar ( nipple preserving ; n = 1 ) , lateral and peri - areolar ( nipple preserving ; n = 1 ) , other and wise pattern ( n = 2 )  . 
 combinations of breast prosthesis used within patients with two implant - based reconstructions with different types per breast were combined implant ( beckers ) and fixed - volume implant ( n = 1 ) , and fixed - volume implant and temporary expander ( n = 3 )  . 
combinations of axillary surgery within patients with two implant - based reconstructions with different surgeries per breast were axillary clearance and none ( n = 41 ) , axillary clearance and previous staging axillary surgery ( n = 1 ) , axillary clearance and sentinel node biopsy ( n = 10 ) , axillary sample and none ( n = 6 ) , none and previous staging axillary surgery ( n = 32 ) , none and sentinel node biopsy and immediate clearance ( n = 2 ) , none and sentinel node biopsy ( n = 46 ) , and sentinel node biopsy and previous staging axillary surgery ( n = 1 )  . table 2 : operative details , by type of implant - based reconstruction patients , details of the technique were not reported . 
 strattice ( lifecell , brachburg , nj , usa ) or surgimend ( integra lifesciences ) were used in 1215 ( 66% ) of the 1831 mesh - assisted procedures , but in total , 14 different products were used during the course of the study ( artea , biodesign , braxon , cellis , meso biomatrix , native , protexa , silk , strattice , surgimend , tigf , tiloop , veritas , and xcm ) , with an increasing variety of products used as the study progressed ( data not shown )  . the median age of study participants was 49 years ( 4357 ; table 1 )  . 
median bmi was at the upper end of the normal range ( 248 kg / m ; iqr 223282 ) , and was highest overall in patients who had dermal sling reconstruction ( table 1 )  . 
of the 547 ( 26% ) patients having bilateral surgery , 188 ( 34% ) had a contralateral risk - reducing mastectomy at the time of their index cancer operation ( table 2 )  . a one - stage reconstruction was planned in 1650 ( 78% ) patients , and 1239 ( 59% ) had a definitive fixedvolume implant placed at the time of their surgery . 
 tissue expanders or two - stage reconstruction with expandable implants was more common in patients having traditional submuscular procedures without mesh and those having dermal sling reconstruction than in those having other procedure types ( table 2 )  . 
skin and nipple - sparing reconstruction was done in nearly a quarter of cases ( table 2 )  . immediate approximately a third of the 1693 patients having mastectomy and implant - based breast reconstruction for malignancy were recommended chemo therapy or radiotherapy after their reconstruction ( table 3 )  . 
this recommendation did not appear to be related to the type of procedure performed , although more patients having standard subpectoral reconstruction without mesh were recommended for radiotherapy than were patients having other procedure types ( table 3 )  . breast implant - based of the 2108 patients recruited , 2081 ( 99% ) were followed up to 3 months ( median follow - up 3 months , iqr 33 )  . 
 ( 9% ) of loss was experienced by 182 implant 2081 patients followed up at 3 months , which is equivalent to the nmbra published data ( 9% ) but higher ( < 5% )  . 
when two patients have two malignant breasts and there were data about the number of lymph nodes involved for both breasts ( n = 53 ) , the average number of nodes is given . 
when two patients had two malignant breasts with planned axillary clearance data available for one breast , patients are classified according to the breast for which there are data ( n = 12 yes , n = 9 no )  . 
||when both breasts were operated for cancer but only one side needed radiotherapy . table 3 : postoperative data for patients having mastectomy for oncological indications re - admitted for a complication after their reconstruction within 3 months . 
there were 2108 patients with implant - based reconstruction , of whom 2081 ( 99% ) were included in the outcome analysis : complete outcome data ( event data for all four key outcomes ) are available for 2078 patients , who have been included in the analysis 27 ( 1% ) patients have no outcome data and were excluded from the analysis . 
partial outcome data ( event data for three of four outcomes ) are available for three patients , who were included in the analysis and who were assumed to not have had the event for the fourth missing outcome . table 4 : 3 - month outcomes after implant - based breast reconstruction , by procedure type , compared with outcomes in nmbra and uk national quality criteria for breast reconstruction using exploratory multivariable logistic regression , we identified an apparent association between body - mass index and smoking with all four clinical outcomes ( table 5 )  . 
age , neoadjuvant chemotherapy , bilateral surgery , indication for surgery , nipplesparing procedures , insertion of a definitive fixed - volume implant , and type of recon struction performed were not significant risk factors for any of the key safety outcomes ( table 5 )  . 
details of the number of events for each risk factor are shown in the appendix ( p 8 )  . discussion this national , multicentre , prospective cohort study of 2108 patients having immediate implant - based breast reconstruction in 81 centres across the uk shows that the short - term clinical outcomes of immediate implantbased breast reconstruction fall far short of the published aspirational quality standards for immediate breast reconstruction , 23 and have not improved in the 10 years since the nmbra.24 despite recently published evidence showing increased frequency of complications in meshassisted immediate implant - based breast reconstruction , 11 there was no association between type of mesh and shortterm safety outcomes in exploratory regression analyses of this large , non - randomised study . 
to truly answer this important question , a large - scale , pragmatic , randomised controlled trial will be required to identify the most clinically and costeffective approach to immediate implant - based breast reconstruction , and provide information to inform clinical and health policy decisions . despite insufficient high - quality evidence , meshassisted , single - stage , direct - to - implant reconstruction using fixed - volume or adjustable implants has become the most widely used procedure in the uk , 22 with less than 10% of patients undergoing traditional two - stage expander - implant procedures . 
this widespread adoption of mesh suggests that a randomised controlled trial attempting to compare single - stage , direct - to - implant reconstruction with mesh and the standard two - stage techniques would be difficult because of surgeon preference . 
however , our study shows little difference in the short - term clinical outcomes of biological and synthetic mesh - assisted immediate implant - based breast reconstruction , and has highlighted the large number of products in current use . 
pre - pectoral reconstruction was done only in a small number of patients in this study , although it is gaining popularity.7 despite the challenges associated with a randomised clinical trial in breast reconstruction , methods have been developed and successfully used to overcome these issues and support surgeons to recruit patients into trials of very different types of procedures , in which patient and surgeon preferences might be strong.27 although the type of reconstructive technique used does not appear to affect short - term safety outcomes , patient factors such as increased bmi and current smoking seemed to be associated with increased risks of implant loss , infection , re - admission , and reoperation . 
 although this analysis was exploratory in nature , these results highlight the importance of careful patient selection and providing patients at high risk with accurate likelihood of postoperative information about complications , to allow them to make better informed decisions . 
increase in odds for each additional body - mass index unit . table 5 : logistic regression of risk factors for key outcomes the proportion of patients identified in this study who experienced implant loss , re - admission , and infection remain un changed since the 200809 nmbra , whereas the proportion of patients requiring re - operation has more than tripled.24 the reasons for this increase are complex . 
the numbers of immediate implant - based breast recon struction have increased substantially since 200809 , 5 , 22 but there is no evidence to suggest that the indications for implant - based surgery have changed , since the proportions of patients who smoked , had diabetes , had a high bmi , or were american society of anesthesiologists grades iii / iv in our study are largely consistent with the nmbra cohort.24 increased numbers reflect more aggressive management of complications when mesh is used , re - operations could but the use of mesh does not seem to translate into a reduced percentage of implant loss . 
although the proportions of patients with implant loss and return to theatre in this study are much lower than those reported in a 2017 randomised trial , 11 , 13 they are much higher than those reported in other large prospective observational studies14 , 15 , 28 and summarised in recent systematic reviews.8 , 9 this large , multicentre study is likely to reflect real - world outcomes of immediate implant - based breast reconstruction , and highlights the need for improvement in this area . this national prospective study adds substantially to the evidence base in immediate implant - based breast reconstruction , but has several limitations . 
 264 vol 20 february 2019 articles for more on the getting it right first time initiative see co.uk / surgical - specialty / breastsurgery / notably , patients having dermal sling reconstruction had higher bmis than did those in the other groups , but other , subtler , differences might exist between patients having different procedures that were not considered in this study . 
 of particular note was the introduction of implant salvage procedures , whereby fixed - volume implants that were infected or exposed were debrided , washed out , and replaced either with a new implant or a tissue expander . 
we acknowledge that this might have overestimated the occurrence of implant infection , but reported frequencies were consistent those in the nmbra.24 clear , unambiguous definitions of outcomes will therefore be needed for future studies . 
 and previous smoking , bmi , operative radiotherapy were for factors complications in this study , and this potential association might be informative when designing subsequent randomised clinical trials as a basis for balancing randomisation . 
although this study was not powered to establish prognostic factors , and the results should be confirmed in an external validation study , consistency between these results and those in other studies29 , 30 support these findings . 
this approach would not capture complications , such as infection , which developed while patients were receiving chemotherapy or problems developing as a result of adjuvant radiotherapy , for which a longer period of follow - up would be required . identified as risk time , recruitment establish whether the findings of this large , non - randomised study strongly support the need for a randomised controlled trial in immediate implant - based breast reconstruction , and potential trial designs could include biological versus synthetic mesh or pre - pectoral versus subpectoral implant placement . 
the proportion of patients experiencing implant loss and infection and those requiring re - operation and re - admission do not appear to have improved ( ie , decreased ) since nmbra , and do not meet published quality standards . 
these factors are not immediately implant - based breast reconstruction modifiable in the short - term , but neoadjuvant chemotherapy or endocrine therapy could be used as a strategy to provide patients with breast cancer with additional time to lose weight or stop smoking before surgery . 
this approach might not be practical or ethical , and a more appropriate focus could be to develop effective strategies to help patients better understand the potential risks of surgery , to allow them to make fully informed decisions . 
however , it is important that any standardisation of care reflects evidence - based best practice , and further exploratory analysis of the ibra cohort will support this . there remains the need for high - quality evidence from a randomised controlled trial to support the best practice of immediate implant - based breast reconstruction , and the equivalence of different techniques in this nonrandomised study supports a future randomised clinical trial . 
the outcomes of immediate implant - based breast reconstruction in the uk are poor and surgeons need to commit to robust evaluation if outcomes for patients are to be improved . contributors sp , ch , st , js , jmb , ejc , prw , and lw conceived and designed the study and data collection forms . 
all authors reviewed and critically revised the manuscript and approved it before submission . declaration of interests sp , ch , prw , aj , jmb , and lw report grants from nihr research for patient benefit programme ( see below ) during the conduct of the study . 
the other authors have nothing to declare . acknowledgments this work was funded by an nihr research for patient benefit programme grant ( pb - pg - 0214 - 33065 ) and pump - priming funding from the association of breast surgery and the british association of plastic reconstructive and aesthetic surgeons . 
this work was undertaken with the support of the mrc conduct - ii ( collaboration and innovation for difficult and complex randomised controlled trials in invasive procedures ) hub for trials methodology research ( mr / k025643 / 1 ) and the nihr biomedical research centre at university hospitals bristol nhs foundation trust and the university of bristol . 
the views expressed in this publication are those of the authors and not necessarily those of the nhs , the national institute for health research , or the department of health and social care . vol 20 february 2019 articles data sharing individual participant data ( de - identified ) , the data dictionary , and the statistical analysis plan for this study will be available to researchers after methodological review of the proposed analysis plan by the ibra steering group . 
to gain access , data requestors will need to sign a data access agreement . infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
 lancet oncol 2018 ; 19 : e10212in this series paper , in the section titled challenges from womens cancer in india , the second sentence of the second paragraph should read despite this initiative , large - scale implementation of cancer prevention and control strategies has yet to take place , and public expenditure on health remains low at 12% of indias gross domestic product . 
this correction has been made to the online version as of may 31 , 2018 . correction to lancet oncol 2018 ; 19 : 72829 correction to lancet oncol 2018 ; 19 : 54961 iarc monographs vol 121 group . 
lancet oncol 2018 ; 19 : 54961in figure 3 of this article ( published online first on feb 20 , 2018 ) , the heatmap in panel a has been replaced to amend display errors . 
this correction has been made to the online version as of may 31 , 2018 . vol 19 june 2018 e283 corrections e - cigarettesnew product , old tricks tobacco smoking cessation represents one of the most successful public health initiatives in the world , with smoking prevalence at its lowest during the past decade according to recent who estimates . 
however , since the introduction of e - cigarettes in 2003 , marketed as a less harmful alternative to tobacco , what should have simply been an effective tool for tobacco smoking cessation is turning into a new mainstream addiction , with tobacco companies being one of the main beneficiaries and regulators entering the debate with naive tolerance . 
 recent months have seen a substantial increase in public promotion of e - cigarettes , taking advantage of the scarcity of evidence regarding the safety and long - term effects of these products . on oct 3 , 2018 , philip morris international , via prominent branding on ferraris formula 1 racing cars , launched mission winnow , a project in which they boldly claim to want to build a better world for women and men who smoke , using our scientific and engineering expertise to deliver it . 
the promotion of this undertaking as a major corporate responsibility exercise is not only deceptive , but also worrying because it demonstrates the extent to which the tobacco industry aims to shape the scientific evidence to support their commercial strategy of e - cigarettes as harmless smoking . 
the same week , on oct 7 , 2018 , the new york times reported about a cocktail party in geneva , switzerland , that coincidentally occurred at the same time and place as the biannual negotiations of the whos tobacco treaty , which were focused on deciding whether to recommend the introduction of stricter regulations for nicotine - delivery devices . 
in this evening event , cumbersomely named nicotine is not your enemy soire and sponsored by an organisation partly funded by the tobacco industrythe consumer choice center the lack of evidence regarding the long - term safety of e - cigarettes was used to persuade guests , who were enjoying an open bar , free tapas , and e - cigarette samples , to believe that e - cigarettes are harmless . 
this effort by tobacco industry representatives to surreptitiously influence who negotiations is yet another desperate attempt to influence the global public health agenda , and although it shouldnt come as a surprise given the tobacco industrys past activities , it is nevertheless deplorable . although the doors of the who are closed to e - cigarettes lobbying parties , those of the global market are wide open , and subliminal advertising are part of the industrys marketing strategy to promote e - cigarettes as the new smoking alternative . 
at the end of october , 2018 , philip morris international was accused of cynical advertising in the uk after the launch of a series of anti - smoking advertisements while still promoting smoking in other countries . 
altria and juul labs inc also announced that they will stop selling some flavoured vaping products in the usato pre - empt the us food and drug administration crackdownamid concerns of increased underage use of flavoured e - cigarettes . 
 the orchestrated effort and huge investment of the tobacco industry to promote e - cigarettes and alternative nicotine products deserves an equally in august response bold 2018 , an editorial in the lancet covering the uks house of commons science and technology committee report on e - cigarettes concluded that it is naive and premature of the committee to confuse an absence of evidence with an absence of har indeed , although e - cigarettes are unlikely to replicate the link between nicotine addiction and lung cancer caused by tobacco smoking , the absence of long - term evidence about the safety of vaping calls for a more precautionary attitude from policy makers . 
after a century of global inaction against the tobacco epidemic , the 2003 who framework convention on tobacco control provided effective evidence - based recommendations to inform policy and keep countries accountable to global tobacco control targets . 
instead of passively waiting for history itself , non - governmental organisations and governments alike should come together with a united vision to monitor and counter disinformation on e - cigarettes . 
although the long - term effects of e - cigarettes are still unknown , we are aware of their potential to create generations of nicotine addicts , which should be enough to trigger stricter regulations on these products . 
 the lancet oncology industry repeat for more on the who report on the global tobacco epidemic , 2017 see iris / bitstream / handle / 10665 / 255874 / 9789241512824 - eng . pdf ? sequence = 1 for more on mission winnow see com / story / 01 for more on the new york times report see nytimes.com / 2018 / 10 / 07 / health / tobacco - e - cigarettestreaty.html for more on cynical advertising see news / business - 45932048 for more on altrias e - cigarette strategy see washingtonpost.com / health / 2018 / 10 / 25 / marlboromaker - altria - halt - sales - flavorede - cigarettes - amid - concernsabout - youth - vapingsurge / ? noredirect = on&utm_ term = .db5ff0fa4920 the lancet editorial is available at journals / lancet / article / piis0140 - 6736 ( 18 ) 31935 - 4 / fulltext vol 19 december 2018 1543 editorial correction to lancet oncol 2017 ; 18 : e31529 correction to lancet oncol 2017 ; 18 : 150211 weller m , van den bent m , tonn jc , et al . 
 lancet oncol 2017 ; 18 : e31529in the panel of this review ( published online first on may 5 , 2017 ) , the dose of bevacizumab should be 10 mg / kg . 
the corrections have been made to the online version as of oct 31 , 2017 , and the printed version is correct . vol 18 november 2017 e642 corrections correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections published online september 12 , 2018 s1470 - 2045 ( 18 ) 30563 - 1 see articles page 1289 cancer trends and disparities in india : data needs for providing equitable cancer care india , with a population close to 13 billion , and growing , is epidemiologically interesting and chal len ging for health - care planners . 
regarding cancer burden , the population demographics , health policies , health - data recording , access to health care , and affordability have all improved substantially during the period between 1990 and 2016 , as reported by the india state - level disease burden initiative cancer collaborators in their global burden of disease paper in the lancet oncology.1 in addition to the heterogeneity in cancer incidence and outcomes between states , significant differences exist within each state , most prominently between urban and rural populations . 
health data availability , access to health care , and affordability are poor and have remained almost static over the entire period in rural areas , while they have improved substantially in urban areas . 
the federal government of india is currently rolling out in a phased manner the national health protection scheme ( nhps , also known as modicare ) .2 if properly implemented , this programme is likely to improve health - care access for the majority of the rural indian population in the next decade . the india state - level disease burden initiative cancer collaborators have used the best possible data - sourcing methods available so far for india . 
the first populationbased cancer registry , based in mumbai ( previously named bombay ) , started in june 1963 , and the first rural population - based cancer registry , based in barshi , in 1987 . 
cancer data maharashtra , was established collection has improved over the years and the indian council of medical research ( icmr ) now has a fully fledged national centre for disease informatics and research ( ncdir )  . 
the federal government of india has made it mandatory for all citizens to possess a unique national identification number ( aadhaar act 2016 ) 3 that currently linked to all financial transactions . 
this number will eventually also be linked to all social security benefits , including modicare , making it an excellent database for future health - services planning in the country . it is heartening to note that the age - standardised incidence of the most common cancers ( except breast cancer ) has remained static over the past two and half decades , despite the assumption of under - reporting in the earlier part of this period . 
the incidence of cancer ( except for cervical cancer , and except for the north - eastern state of mizoram ) is much lower than that in countries that can be said to be in a similar epidemiological transition as india ( brcsbrazil , russia , china , and south africa ) , and substantially lower than in some developed countries with established prevention , screening , and early detection programmes.4 however , the increased incidence of breast cancer in india is worrying and requires serious attention . 
in this context , a comparison between urban and rural populations within states would have been interesting . the federal government of india has taken important towards controlling cancer and policy decisions other non - communicable diseaseseg , cotpa 2003 ( cigarettes and other tobacco products [ prohibition of advertisement and regulation of trade and commerce , production , supply and distribution ] act ) ; 5 however , except for a few successful smokefree city programmes , and graphic package warnings , mechanisms to enforce the act are scarce since enforcement is the responsibility of each state . 
 just like tobacco use in india and most of south asia is different from the rest of the world , mainly due to the high prevalence of smokeless tobacco use , alcohol use ( patterns and disease causation ) are also worthy large proportion of the alcohol consumed by poor people in india is spuriously manufactured , and contaminated with various industrial chemicals . 
 countrywide epidemiological studiesa india has also embarked upon a population - based screening programme for cervical cancer , breast cancer , 1260 vol 19 october 2018 comment and oral cancer . 
however , the techniques chosen for these screening programmes are not optimal ; although there is evidence for visual inspection with acetic acid for cervical cancer , it might be useful to switch to hpv screening as soon as it becomes financially feasible , and evidence for implemented clinical breast examination schedules for breast cancer and oral examinations for oral cancer is weak . 
population - based screening for breast cancer starting at age 35 years will probably be a logistical nightmare , waste of resources , and even cause outright harm to patients . 
 surendra s shastri department of health disparities research , university of texas md anderson cancer center , houston , tx 77030 - 3906 , usa ssshastri@mdanderson.org i declare no competing interests . copyright the author ( s )  . 
 ( accessed aug 9 , 2018 )  . maternal hormonal contraception and childhood leukaemia the treatment of childhood leukaemias has improved in recent years because of additional knowledge of acute leukaemia genetic subtypes , pathogenesis mechanisms , prognosis prediction , and targeted therapies . 
the natural history of this disorder is determined by several interacting factors , including exposure to risk factors , susceptibility , and cell biology orig therefore , data generated by population - based registries are research , health - care indispensable planning , and treatment of childhood leukaemias . 
 for aetiology in the lancet oncology , marie hargreave and colleagues1 present a cohort study that adds value to the set of observational epidemiological data about the impact of maternal use of oestrogenprogesterone contraception on the risk of childhood leukaemia in offspring . 
this nationwide , population - based study shows that maternal hormonal contraceptive use is associated with an increased risk of childhood leukaemia in the offspring ( hazard ratio [ hr ] for recent use of hormonal contraception vs no use 146 , 95% ci 109196 ; p = 0011 ) , particularly of the non - lymphoid leukaemia subtype ( 217 , 122387 ; p = 0008 )  . 
the cohort used in the study has robust statistical value given the well documented population - based dataset and participant linkage in danish registries.2 the findings reported by hargreave and colleagues add oral contraception to the list of established risk factors for childhood leukaemia ( ie , tobacco , pesticides , infectious agents ) and , although the authors highlight this minimal risk in their conclusions , some children may be particularly vulnerable to this new risk factor.3 the design of this nationwide , population - based registry study avoids the recall or selection biases often found in case - control studies . 
it also provides information about molecular profiles of the genetic subtypes of acute lymphoblastic leukaemia , and also about distinct cell subtypes of childhood leukaemia , recurrent genetic abnormalities , and age strata , 3 , 4 enabling sensitivity analyses and stratified analyses according to these factors . 
consequently , the authors are able to report data for the different risk associations for molecularly defined subtypes of acute lymphoblastic leukaemia and acute myeloid leukaemia and for childrens age at diagnosis . 
remarkably , maternal exposure to oestrogen and progestins in combined hormonal contraceptives is associated with a higher risk of acute myeloid leukaemia than of acute lymphoblastic leukaemia ( hrs associated with recent use were 224 leukaemia [ 95% ci 112448 ] for acute leukaemia )  . 
 vs 125 [ 089178 ] for acute myeloid lymphoid published online september 6 , 2018 s1470 - 2045 ( 18 ) 30509 - 6 see articles page 1307 vol 19 october 2018 1261 comment correction to lancet oncol 2017 ; 18 : 67281 j , f o n t a , g a r c a d o n a s prez - valderrama b , et al . 
maintenance therapy with vinflunine plus best supportive care versus best supportive care alone in patients with advanced urothelial carcinoma with a response after first - line chemotherapy ( maja ; sogug 2011 / 02 ) : a multicentre , randomised , controlled , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 67281in this article , the declaration of interests should read jg - d reports personal fees from astellas , janssen ; grants and personal fees from astrazeneca , pfizer , pierre fabre , merck , bioclin , bristol myers squibb , novartis , and msd ; grants , personal fees , and non - financial support from roche ; and grants from gammamabs , outside the submitted work . 
af reports grants from astellas , astrazeneca , pierre - fabre ; personal fees and non - financial support from sanofi , janssen , bayer , and roche , outside the submitted work . 
bp - v reports personal fees from astellas pharma , novartis , pfizer , pierre fabre , bayer , sanofi , bristol - myers squibb , ipsen , and janssen - cilag , during the conduct of the study . 
jaa reports grants and personal fees from glaxosmithkline and novartis ; personal fees and nonfinancial support from jansen cilag ; grants , personal fees and non - financial support from bms ; personal fees from pfizer , roche , and eusa ; grants from sanofi and pierre fabre , outside the submitted work . 
nl reports personal fees from pfizer , sanofi , pierre fabre , roche , ipsen , pharma mar , bms , bayer , astrazeneca , astellas , and msd , outside the submitted work . 
jcv - g reports personal fees from pfizer , astellas , janssen , msd , bayer , roche , bristol , astrazeneca , boehringer , pierre fabre , novartis , ipsen , celgene , lilly , merck , sanofi , and mundipharma , outside the submitted work . 
bm reports personal fees and non - financial support from pfizer and janssen ; personal fees from novartis , astellas oncology , bms , sanofi , ipsen , bayer ; and grants and personal fees from roche , outside the submitted work . 
agda reports advisory board , consultancy and speaker honoraria or travel support from pierre fabre , roche , bristol - myers squibb , msd , pfizer , novartis , bayer , janssen , sanofi , astellas , eusa pharma , and eisai ; and research funding from astellas . 
dc reports personal fees from janssen , roche , astellas , msd , ipsen , pfizer , bms , bayer , astrazeneca , novartis , lilly , sanofi , pierre fabre , and boheringer , outside the submitted work . 
eg reports grants from pierrefabre , during the conduct of the study ; personal fees and non - financial support from janssen , pfizer , bayer , ipsen , novartis , bms , rovi ; personal fees from menarini and leo pharma ; and nonfinancial support from pierre - fabre , outside the submitted work . 
ua reports non - financial support from novartis , pierre fabre , and ipsen ; personal fees from bayer , janssen , astellas , and pfizer ; and personal fees and nonfinancial support from sanofi , roche , and bms , outside the submitted work . 
 xgdm reports personal fees from pfizer , ipsen , bms , roche , lilly , pharmamar , eusapharma , and pierre fabre ; and grants from astrazeneca , outside the submitted work . 
md has participated in advisory boards , consultancy , and speaker bureaus for roche , bristol - myers squibb , msd , pfizer , janssen , sanofi , astellas ; and received travel and accommodations expenses from roche , astellas , janssen , bayer , and lilly . 
jp has received honoraria as a consultant on advisory boards from pfizer , astellas , janssen , msd , bayer , roche , bms , boehringer , astrazeneca , ipsen , novartis , eusa pharma , eisai , and sanofi ; and as speaker from kyowa , pierre - fabre , celgene , lilly , and merck . 
 rm - b has served as a consultant or on advisory and / or speakers bureaus for sanofi aventis , bayer , janssen , astrazeneca , merck sharp & dohme , and asofarma ; and received travel and accommodations expenses from roche , sanofi aventis , astellas , janssen , merck sharp & dohme , bayer , pharmacyclics , clovis oncology , and lilly . 
jlp - g reports non - financial support from pierre fabre , during the conduct of the study ; non - financial support from roche , bms , and msd , outside the submitted work . 
jb reports grants and personal fees from pfizer , merck , bms ; personal fees from genentech , astrazeneca , pierre - fabre ; and grants from takeda , during the conduct of the study . 
 this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1493503 zackrisson s , lng k , rosso a , et al . 
 lancet oncol 2018 ; 19 : 1493503 in this article , in table 1 and table 4 , the age groups should have been listed as follows : 4049 , > 4959 , > 5969 , and > 69 . 
the title and legend of figure 2 should have read as follows : number of false - positive results among participants over the trial period who were recalled only on digital breast tomosynthesis and digital mammography , respectively . 
 these corrections have been made to the online version as of jan 3 , 2019 . vol 20 january 2019 corrections published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections editorial for public health englands report see government / publications / sugarreduction - from - evidence - intoaction for the institute for alcohol studies report see ias.org.uk / what - we - do / iasreports.aspx sugar : a taxing problem ? on oct 22 , 2015 , public health england published its long - awaited report on the evidence for taking action intake exceeds on sugar reduction . 
 consumption of excessive amounts of food and drink containing high levels of sugar can lead to weight gain , and the report states that 10% of 45 year olds , 19% of 1011 year olds , and almost 25% of adults in england are obese ; a substantial proportion of all age groups are overweight . 
the health e ects of being overweight or obese are well - documentedeg , heart disease , diabetes , stroke , and cancersindeed , one in 20 cancers in the uk are related to being overweight . 
 the report o ers a number of recommendations to help cut sugar intake : special promotions in shops should be reduced , and advertising of food and drink to children and adults across all media substantially decreased . 
clear de nitions of high sugar foods are called for , as is the introduction of a programme of gradual reduction in sugar levels in everyday food and drink products , together with reductions in portion size . 
 the introduction of government buying standards for food and catering across the public sector is proposed , as is ensuring that individuals with the opportunity to in uence food choices in the catering , tness , and leisure sectors have appropriate training in diet and health . 
evidence suggests that price increases for high sugar foods and non - alcoholic drinks are likely to reduce the sales of these products , at least in the short tersimilar schemes are already in place in other countries , such as norway , finland , hungary , france , and mexico . 
and indeed , following the introduction of a peso - per - litre tax on sugar sweetened drinks in mexico in october , 2013akin to a 10% increase in pricepreliminary data suggest that there was a reduction of 6% in purchasing of such products in 2014 , with larger reductions noted in more socioeconomically deprived households . 
and perhaps under pressure from the drinks industry , the mexican congress voted on oct 20 , 2015 , to cut the tax in half for drinks with less than 5 mg sugar per 100 ml . 
indeed , whether taxation of unhealthy foods actually works is contentiousfor instance , denmarks fat tax , introduced to wide acclaim in october , 2011 , was abandoned after just 15 months as a result of negative economic effects , little evidence of a reduction in consumption , and the lack of popularity among the public . 
in addition to objections from business owners and trade unions , the tax was widely criticised for making the poor poorer , a situation that could also arise with a sugar tax . 
furthermore , one could foresee a situation in which the food and drinks industry could absorb any potential increase in price in the large and excessive profit margins for their products . thus , taxing the consumer is a blunt weapon and might not be the panacea to tackling sugar consumption on its own . 
the past 3040 years have seen unprecedented changes in the way we interact with food , both in terms of the foods available and in how they are produced , marketed , and advertised . 
 we have become complacent , disconnected with the realities of food production , and the forces of capitalism have allowed the food industry to shirk their ethical responsibility in the pursuit of pro t . 
 public health englands report recognises the need for cultural change and an acknowledgment of individual responsibilities , and proposes the our introduction of a plan to gradually reduce sugar levels in everyday food and drink products . 
however , a recent report from the institute for alcohol studies shows that a voluntary responsibility deal between the uk government and the alcohol industry has failed to implement any meaningful change . 
nivolumab or nivolumab plus patients with relapsed malignant pleural mesothelioma ( ifct - 1501 maps2 ) : a multicentre , open - label , randomised , non - comparative , phase 2 trial . 
 lancet oncol 2019 ; 20 : 23953in figure 4b of this article , the position of the plotted kaplan - meier curves on the y axis has been corrected , affecting the overall survival readings . 
 this correction has been made to the online version as of march 1 , 2019 correction to lancet oncol 2019 ; 20 : 36170 saad ed , squifflet p , burzykowski t , et al . 
 disease - free survival as a surrogate for overall survival in patients with her2positive , early breast cancer in trials of adjuvant trastuzumab for up to 1 year : a systematic review and meta - analysis . 
 lancet oncology 2019 ; 20 : 36170 in the summary of this article , the fourth sentence of the findings section should read subgroups defined by nodal status and hormone receptor status yielded qualitatively similar results . 
this correction has been made to the online version as of march 1 , 2019 , and the printed article is correct . vol 20 march 2019 e132 corrections addendum to lancet oncol 2005 ; 6 : 75156 hckel m , horn l - c , fritsch the h . 
association between mesenchymal compartment of uterovaginal organogenesis and local tumour spread in stage ibiib cervical carcinoma : a prospective study lancet oncol 2005 ; 6 : 75156the supplemental video accompanying this article has been updated . 
this addendum has been added to the online version as of june 29 , 2018 . correction to lancet oncol 2018 ; 19 : 5164 patel mr , ellerton j , infante jr , et al . 
in figure 4a , the first subheading in the inset on the graph should have referred to median progression - free survival in weeks , not months , and the second subheading in the inset on the graph should have read 6 - month pfs , rate ( 95% ci )  . 
 in the results section , last paragraph , the following sentence should have read as follows : of which infusionrelated reaction , diarrhoea , and pneumonitis were reported in more than one patient ( three , two , and two patients , respectively )  . 
also in the last paragraph of the results section , localised oedema should not have been included in the list of reasons for patients who permanently discontinued avelumab due to a treatment - related adverse event . 
 these corrections have been made to the online version as of june 29 , 2018 . correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
 lancet oncol 2017 ; 18 : 106175 in this article , the following sentence about the safety results in the findings section of the summary should have read : commonly reported treatment - related adverse events were diar rhoea ( 41 [ 16% ] ) , fatigue ( 37 [ 15% ] ) , elevated aspartate aminotrans ferase ( 33 [ 13% ] ) , and elevated alanine aminotrans ferase ( 24 [ 10% ] )  . 
the incidence of serious febrile neutropenia in the summary findings and in the main results ( fourth paragraph , first sentence ) should have been reported as 78 ( 31% )  . 
in table 2 , the percentage values for grade 12 nausea , dizziness , elevated alanine aminotransferase , and thrombocytopenia should have been reported as 19% , 19% , 13% , and 2% , respectively . 
in the results , the second sentence ninth paragraph should have read as follows : of 75 patients who achieved a composite complete remission , two ( 3% ) received the 20 mg / day dose , seven ( 9% ) the 80 mg / day dose , 27 ( 36% ) the 120 mg / day dose , 36 ( 48% ) the 200 mg / day dose , and three ( 4% ) the 300 mg / day dose . 
these corrections have been made to the online version as of june 29 , 2018 . vol 19 july 2018 e335 corrections e for more on the nhs existential crisis see editorial lancet oncol 2018 ; 19 : 1 for more on wilmshursts letter see brit med j 2018 ; 360 : k549 uk national health servicebeyond repair ? in a recent editorial , we highlighted the disconnect between the uk national health service ( nhs ) and its founding philosophy , and the existential crisis facing british health care . 
recent weeks have seen the highest numbers of patients on record not being treated within prescribed waiting times , patients being queued on trolleys in hospital corridors , and urgent surgeries cancelled because of insufficient intensive - care beds . 
 moreover , dangerous , financially - motivated , clinical decisions are being proposed , patients are donating chemotherapy equipment to under - resourced hospitals , and more protest marches by junior doctors and the public alike are happening than ever before . is a failures these extreme pressures on the nhs are leading in cancer care . 
examples of clinical mismanagement have been highlighted in wales , with one patient diagnosed with a liver mass of 5 cm in january , 2017 , having to wait 8 months for treatment , by which point the tumour was 15 cm and incurable . 
far more leaked memo from the churchill concerning hospital in oxford , uk , where the chemotherapy lead allegedly wrote to fellow oncologists suggesting changes in the provision of chemotherapy . 
as a result of having insufficient nurses in the day treatment unit to administer treatment , the specialist suggested delaying initiation of chemotherapy by 4 weeks , and then increasing the length of each cycle while reducing the number . 
 through diarised anecdotes in his candid bestseller , this is going to hurt : secret diaries of a junior doctor , adam kay starkly illustrates the problems that nhs doctors face , including chronic understaffing , lack of cover , a paucity of senior doctors , long hours , stress , and junior doctors left in charge of large caseloads . 
such circumstances underpin the tragic case of 6 - year old jack adcock who died from a cardiac arrest as a result of sepsis whilst under the care of junior paediatrician hadiza bawa - garba at leicester royal infirmary , leicester , uk , in february , 2018 . 
but , was this a fair and proportionate response ? an enlightening piece on sheri browns blog , confessions of a junior doctor , suggests that , whilst the death of jack adcock is an unacceptable tragedy , it was the manifestation of system failure rather than the actions of a single person . 
other doctors have come out in support of bawe - garbeeg , consultant cardiologist peter wilmshurst has called on the general medical council to investigate his own clinical practice , and urges other doctors to do the same . 
wilmshursts aim is to emphasise that clinical errors do occurno one is infalliblebut such tragic failures of care often result from structural problems in the nhs system rather than from malpractice . a free at the point - of - care , universal health service is widely supported in the uk , but a radical rethink is essential . 
a thorough review of other universal health systems in comparable countries , such as germany and france , could yield important insights in to how to make the service more effective and patient - centric . 
equally , a detailed appraisal of the management , organisation , and intersection between primary care , hospitals , and social care ; the degree of safe staffing ; and realistic funding levels are crucial to define effective changes . 
the idea of a ring - fenced tax dedicated specifically to the nhs could potentially solve funding gaps if introduced in tandem with a governance structure that gives the nhs quasiindependence from governments and politicking , and necessary structural reform . the uk can no longer pretend the nhs can be rectified by short - term solutions . 
 delivering world - class cancer care and all other health services is more than humanitarian goodness , it serves an economic necessity to have a healthy working - age , taxpaying nation . 
other countries have patient - centric and adequately resourced universal health systems , so why not the ukthe country that pioneered the welfare state and is one of richest in the world ? the lancet oncology vol 19 march 2018 editorial addendum to lancet oncol 2005 ; 6 : 75156 hckel m , horn l - c , fritsch the h . 
association between mesenchymal compartment of uterovaginal organogenesis and local tumour spread in stage ibiib cervical carcinoma : a prospective study lancet oncol 2005 ; 6 : 75156the supplemental video accompanying this article has been updated . 
this addendum has been added to the online version as of june 29 , 2018 . correction to lancet oncol 2018 ; 19 : 5164 patel mr , ellerton j , infante jr , et al . 
in figure 4a , the first subheading in the inset on the graph should have referred to median progression - free survival in weeks , not months , and the second subheading in the inset on the graph should have read 6 - month pfs , rate ( 95% ci )  . 
 in the results section , last paragraph , the following sentence should have read as follows : of which infusionrelated reaction , diarrhoea , and pneumonitis were reported in more than one patient ( three , two , and two patients , respectively )  . 
also in the last paragraph of the results section , localised oedema should not have been included in the list of reasons for patients who permanently discontinued avelumab due to a treatment - related adverse event . 
 these corrections have been made to the online version as of june 29 , 2018 . correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
 lancet oncol 2017 ; 18 : 106175 in this article , the following sentence about the safety results in the findings section of the summary should have read : commonly reported treatment - related adverse events were diar rhoea ( 41 [ 16% ] ) , fatigue ( 37 [ 15% ] ) , elevated aspartate aminotrans ferase ( 33 [ 13% ] ) , and elevated alanine aminotrans ferase ( 24 [ 10% ] )  . 
the incidence of serious febrile neutropenia in the summary findings and in the main results ( fourth paragraph , first sentence ) should have been reported as 78 ( 31% )  . 
in table 2 , the percentage values for grade 12 nausea , dizziness , elevated alanine aminotransferase , and thrombocytopenia should have been reported as 19% , 19% , 13% , and 2% , respectively . 
in the results , the second sentence ninth paragraph should have read as follows : of 75 patients who achieved a composite complete remission , two ( 3% ) received the 20 mg / day dose , seven ( 9% ) the 80 mg / day dose , 27 ( 36% ) the 120 mg / day dose , 36 ( 48% ) the 200 mg / day dose , and three ( 4% ) the 300 mg / day dose . 
these corrections have been made to the online version as of june 29 , 2018 . vol 19 july 2018 e335 corrections published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections comment published online january 11 , 2016 s1470 - 2045 ( 15 ) 00556 - 2 see articles page 184 excision margins for melanomas : how wide is enough ? the main aim of surgery in treating any cancer is to completely excise the tumour , thereby preventing local recurrence . 
in the case of melanoma , the purpose of a wide excision is to remove local micrometastases and otherwise phenotypically normal tissue that might be harbouring genotypically abnormal cells located in either the surrounding cutis or super cial lymphatics , while at the same time trying to prevent unacceptable functional and cosmetic harm to the patient as a result . in the lancet oncology , andrew hayes and colleagues1 report the long term follow - up data from the uk excision margins trial , 4 which started in 1993 . 
 the latest analysis of the data1 suggests that the narrower excision margin of 1 cm is associated with worse disease - speci c survival , estimated as an absolute di erence of 595% ( 95% ci 054 to 1244 ) at 10 years , compared with that in patients who had the wider 3 cm excision margin at a median follow - up of 88 years : ( unadjusted hazard ratio [ hr ] 124 [ 95% ci 101153 ] , p = 0041 )  . these data are important because they seem to contrast with ndings from ve other randomised trials suggesting that narrow margins around melanomas ( 1 cm or 2 cm ) are just as safe as wide ones ( 3 cm , 4 cm , or 5 cm ) .2 currently , only the uk national guidelines3 continue to recommend 3 cm margins around thicker primary melanomas , compared with guidelines from other countries that recommend 2 cm as the maximum marghayes and colleagues propose that the ndings in their long - term analysis are linked directly to their previous nding of increased locoregional recurrence associated with the narrower 1 cm excision margin compared with the 3 cm excision margin.4 however , in both surgical groups , the incidence of nodal recurrence outweighed the incidence of local recurrence by at least 5 to 1 . 
in view of the ndings of the mslt - 1 study , 5 in which the incidence of sentinel node positivity matched the number of nodal recurrences , especially for thick melanomas , most of these nodal metastases would probably have been detected by sentinel - node biopsy , if it had been done at the time of the intervention . 
 accordingly , a plausible alternative explanation is that the excess nodal disease in the narrow margin group was indicative of poor prognostic disease before the intervention , rather than resulting from the narrow margin intervention itself . the overall recurrence data , including data for in - transit metastases , from the primary analysis4 were remarkably similar between the 1 cm and 3 cm groups ( 57% vs 47% )  . 
however , when analysed as a speci c secondary endpoint , the di erence in local recurrence between the groups was greater , although not signi cantly ( 82% vs 56% ; hr 151 [ 95% ci 091251 ] ; p = 01 ) .4 since 2004 , it has become clear that the presence of microsatellitesrepresenting microscopic , discontiguous , intralymphatic extensions of melanoma directly adjacent to the primary tumour is a poor prognostic indicator for melanoma , and is now classi ed as stage iii disease.6 whether an excess of microsatellites was present in the 1 cm group before or at randomisation in the present study is unclear , because this information was not included in the standard synoptic report at the time . 
data from the recent scandinavian wide excision trial7 is consistent with this notion , because local recurrence was higher in the narrow margin group ( 2 cm ) than in the wide margin group ( 4 cm ) , although this was not signi cant . 
 data from a large , retrospective study investigating risk factors for locoregional recurrences8 have suggested that in - transit metastases and local recurrences are associated with an increased incidence of subsequent regional nodal relapse , despite an initially negative sentinel node . in summary , the implication of hayes and colleagues study is that high - risk melanoma phenotypes might be unmasked by a narrower , 1 cm wide - excision margin around tumours and these risks could manifest as clinically detectable local or regional recurrences ( or both ) in follow - up . 
closer inspection of the data , however , suggests that this subgroup of patients is small and that most patients could be safely managed without creating 46 cm wide excision defects . 
accordingly , clinicians e orts might vol 17 february 2016 comment published online december 7 , 2015 s1470 - 2045 ( 15 ) 00535 - 5 see articles page 193 be supported by the identi cation of biomarkers to recognise the high - risk minority of patients , especially those with a microscopic locoregional extension at the time of diagnosis of their primary melanoma . 
 cancer screening after unprovoked venous thrombosis the risk of an underlying malignant disease is increased in patients presenting with unprovoked venous thromboembolism , particularly with increasing age , with an estimated prevalence of hidden cancer of around 10%.1 , 2 although , at least theoretically , workup for occult cancer in this scenario could lead to early diagnosis and reduce cancer - related mortality , this hypothesis has not yet been con rmed.3 indeed , conducting a randomised trial on this topic is not an easy task , because there are plenty of methodological di culties to face . 
 the recently published some study4 concluded that , in patients with unprovoked venous thromboembolism , routine screening with comprehensive ct of the abdomen and pelvis ( including virtual gastroscopy and colonoscopy ) did not provide a clinical bene t when added to a limited workup , which included complete history taking and physical examination , complete blood counts , liver and kidney function tests , chest radiography , mammography ( for women older than 50 years ) , pap smear testing ( for women 1870 years of age who had ever been sexually active ) , and prostate - speci c antigen test ( for men older than 40 years )  . 
these results , together with other previous studies , havefor nowcooled the enthusiasm for cancer screening in patients with venous thrombosis.5 , 6 but when a door closes , another opens . 
this might be explained by some characteristics of the study population eg , 25% of the patients were younger than 50 years , and 6% of the thrombotic events were associated with oral contraceptives . 
in order to investigate the e ects of these therapies and to respond to emerging evidence , we aimed to systematically review all relevant trials using a framework for adaptive meta - analysis . 
 methods for this systematic review and meta - analysis , we searched medline , embase , lilacs , and the cochrane central register of controlled trials , trial registers , conference proceedings , review articles , and reference lists of trial publications for all relevant randomised controlled trials ( published , unpublished , and ongoing ) comparing either standard of care with or without docetaxel or standard of care with or without bisphosphonates for men with high - risk localised or metastatic hormone - sensitive prostate cancer . 
for each trial , we extracted hazard ratios ( hrs ) of the e ects of docetaxel or bisphosphonates on survival ( time from randomisation until death from any cause ) and failure - free survival ( time from randomisation to biochemical or clinical failure or death from any cause ) from published trial reports or presentations or obtained them directly from trial investigators . 
 results from three ( chaarted , getug - 15 , stampede ) of these trials ( 2992 [ 93% ] of 3206 men randomised ) showed that the addition of docetaxel to standard of care improved survival . 
the hr of 077 ( 95% ci 068087 ; p < 00001 ) translates to an absolute improvement in 4 - year survival of 9% ( 95% ci 514 )  . 
docetaxel in addition to standard of care also improved failure - free survival , with the hr of 064 ( 058070 ; p < 00001 ) translating into a reduction in absolute 4 - year failure rates of 16% ( 95% ci 1219 )  . 
survival results from three ( getug - 12 , rtog 0521 , stampede ) of these trials ( 2121 [ 53% ] of 3978 men ) showed no evidence of a bene t from the addition of docetaxel ( hr 087 [ 95% ci 069109 ] ; p = 0218 ) , whereas failure - free survival data from four ( getug - 12 , rtog 0521 , stampede , tax 3501 ) of these trials ( 2348 [ 59% ] of 3978 men ) showed that docetaxel improved failure - free survival ( 070 [ 061081 ] ; p < 00001 ) , which translates into a reduced absolute 4 - year failure rate of 8% ( 510 )  . 
survival results from three of these trials ( 2740 [ 88% ] of 3109 men ) showed that addition of bisphosphonates improved survival ( 088 [ 079098 ] ; p = 0025 ) , which translates to 5% ( 18 ) absolute improvement , but this result was in uenced by the positive result of one trial of sodium clodronate , and we found no evidence of a bene t from the addition of zoledronic acid ( 094 [ 083107 ] ; p = 0323 ) , which translates to an absolute improvement in survival of 2% ( 3 to 7 )  . 
of 17 trials of bisphosphonates for men with m0 disease , survival results from four trials ( 4079 [ 66% ] of 6220 men ) showed no evidence of bene t from the addition of bisphosphonates ( 103 [ 089118 ] ; p = 0724 ) or zoledronic acid ( 098 [ 082116 ] ; p = 0782 )  . 
failure - free survival de nitions were too inconsistent for formal meta - analyses for the bisphosphonate trials . interpretation the addition of docetaxel to standard of care should be considered standard care for men with m1 hormone - sensitive prostate cancer who are starting treatment for the rst time . 
no evidence exists to suggest that zoledronic acid improves survival in men with m1 or m0 disease , and any potential bene t is probably small . funding medical research council uk . 
open access article distributed under the terms of cc - by . vol 17 february 2016 lancet oncol 2016 ; 17 : 24356 published online december 21 , 2015 s1470 - 2045 ( 15 ) 00489 - 1 this online publication has been corrected . 
with 11 million diagnoses ( 15% of all cancers diagnosed in men ) and 307 000 deaths estimated to have taken the in 2012 , prostate cancer has become place fth leading cause of death from cancer in men worldwide.1 therapy with for many decades , initial ( rst - line ) treatments for both locally advanced and metastatic prostate cancer have been surgical castration by bilateral orchidectomy or androgen deprivation luteinising hormone - releasing hormone agonists or antagonists.2 the aim of these approaches is to reduce testosterone concentrations . 
however , the disease progresses in virtually all patients who have metastatic disease and in many patients with non - metastatic disease.3 , 4 a number treatments , such as bisphosphonates , cytotoxic chemotherapy , new hormone therapies , and radium - 223 , have therefore been assessed in combination with primary androgen deprivation therapy with the aim of reducing progression rates and improving survival . one such treatment , docetaxel ( given with or without estramustine ) , was shown in two pivotal randomised controlled trials5 , 6 to improve survival in men with castrate - resistant prostate cancer that was no longer responsive to testosterone suppression alone . 
this nding led to the international approval by regulatory authorities of docetaxel for this disease setting and a number of randomised controlled trials , in which men with metastatic or high - risk localised prostate cancer , starting long - term androgen deprivation therapy for the rst time , were randomly assigned to receive standard androgen deprivation therapy - based treatment alone or supplemented with docetaxel ( with or without other agents )  . 
in the chaarted7 and stampede8 trials , men with metastatic disease had signi cant improvements in survival with the addition of docetaxel , whereas results of the similar getug - 15 trial9 , 10 showed no evidence of a survival bene t from docetaxel . 
a small number of trials of docetaxel for men with non - metastatic disease have produced promising results for relapse or failure - free survival , but the e ect on survival is unclear . bisphosphonates are a class of drugs that have been shown to have a number of anti - cancer e ects.11 in randomised controlled trials , the rst - generation bisphosphonate , clodronate , delayed time to progression in men with bone metastases when given alongside long - term androgen deprivation therapy . 
some evidence suggests that biphosphonates might improve survival.12 newer ( third - generation ) bisphosphonates , notably zoledronic acid , have been found to reduce the risk of skeletal complications ( eg , fractures ) in patients with bone metastases from breast cancer and castrate - resistant prostate cancer.13 in the wake of these results , a number of randomised controlled trials have been designed to investigate whether men who are commencing long - term androgen deprivation therapy for either metastatic or localised hormone - sensitive prostate cancer bene t from bisphosphonates . as part of the wider systemic treatment options for prostate cancer ( stopcap ) meta - analysis project , we aimed to systematically review all relevant randomised controlled trials that tested the addition of docetaxel or bisphosphonates to standard of care . 
we prospectively planned meta - analyses that would respond and adapt to the emergence of new trial results , while also assessing the potential e ect of trials that are yet to be completed or reported . methods systematic review and framework for adaptive meta - analysis standard systematic reviews of both aggregate and individual participant data can take many years to complete and are usually retrospective , so they cannot always keep pace with therapeutic developments . 
we therefore used a framework for adaptive meta - analysis ( fame ) being developed by the mrc clinical trials unit at ucl ( london , uk ) to rapidly and robustly assess the e ects of therapies and to respond to emerging evidence . 
the key principle is to systematically identify all trials using established methods , then synthesise what is already known about the e ects of therapies from aggregate data , and consider how trials that are ongoing or yet to be reported might a ect these results . 
 thus , we deliberately began the review process before many trials of docetaxel and bisphosphonates had been completed and reported so as to build a picture of how information and evidence of the e ects of these drugs might accumulate . 
this review process allowed us to decide prospectively when we were likely to have su cient results or power , or both , for reliable aggregate data meta - analyses and to interpret our results , taking into account the possible e ect of any as yet unavailable evidence . 
this also helped us determine the potential value of updating meta - analyses , and whether these meta - analyses should be based on aggregate data or individual patient data . study selection and data extraction randomised controlled trials comparing either standard of care versus standard of care plus docetaxel or standard of care versus standard of care plus bisphosphonate ( at a therapeutic dose ) were eligible if they aimed to include men with high - risk localised or metastatic , hormonesensitive ( ie , not castrate - resistant ) prostate cancer . 
we unpublished , with no searched medline , 14 embase , 15 lilacs , 16 and the 244 vol 17 february 2016 articles see online for appendix for the protocol see crd.york.ac.uk / prospero / display_record . asp ? id = crd42015020059 4372 records retrieved from electronic databases searching 1213 from medline 2355 from embase 617 from cochrane central 187 from lilacs 769 records retrieved from clinicaltrials.gov and screened 1191 duplicates removed 738 irrelevant comparison 3181 unique records screened 3132 irrelevant comparison 3 potentially eligible trials identied via conference proceedings 49 assessed for eligibility 34 assessed for eligibility 28 excluded 14 duplicate references to the same trial 14 ineligible after full paper screened 12 not treatment dose 1 crpc 1 not randomised controlled trial 20 excluded 10 duplicate trials already identied via electronic databases 10 ineligible 6 not treatment dose 1 crpc 1 not randomised controlled trial 2 irrelevant comparison 21 eligible trials 14 eligible trials 35 included in systematic review 22 included in meta - analysis of bisphosphonate comparison * 14 included in docetaxel comparison * figure 1 : study ow chart crpc = castrate - resistant prostate cancer . 
search terms used are listed in the appendix . for all eligible trials , we extracted data on : the accrual period , actual or ( if ongoing ) planned number of participants ; whether previous androgen deprivation therapy was allowed ; control group treatments ( eg , type of androgen deprivation therapy used ) ; docetaxel dose and scheduling ; bisphosphonate type ; dose and duration of bisphosphonate treatment ; median patient age ; metastatic status ; performance status ; tnm status ; gleason score ; and median psa concentration at the start of androgen deprivation therapy . 
we also extracted data on methods of sequence generation , allocation concealment , completeness of outcome data reporting , and attrition from trial reports or protocols , or both , to assess the risk of bias of individual trials.17 methods were prespeci ed and are available in an online protocol . outcomes the primary outcome , survival , was de ned as the time from randomisation until death from any cause . 
psa = prostate - speci c antigen . * this value is the mean ( no sd was available ) table 1 : characteristics of studies included in the systematic review and meta - analysis all potential participants , would become available by june , 2015 , with a median follow - up of about 34 years . 
 the typical 4 - year survival reported in trials in this group of men was 40% , which we set as our baseline for predicting the power a meta - analysis of these trials would be likely to provide . 
we estimated that we would have about 70% power to detect an absolute di erence of 5% in 4 - year survival ( hazard ratio [ hr ] 087 ) and more than 99% power to detect a 10% di erence in 4 - year survival ( hr 075 ) ; these are the sort of moderate e ects one might expect in advanced prostate cancer . 
for the bisphosphonate comparison in m1 disease , we predicted that we would have results from trials that included about 85% of all potential participants and , using the same baseline survival , would achieve about 65% power to detect an absolute di erence of 5% in 4 - year survival and more than 99% power to detect a 10% di erence in 4 - year survival . 
these estimates gave us a clear trigger to conduct meta - analyses in the m1 disease setting . we were aware that mature results of trials in m0 disease would lag behind those in the m1 setting owing to a more favourable prognosis , so we expected fewer data for the docetaxel and bisphosphonate comparisons ( around 60% of potential participants )  . 
nevertheless , on the basis of an average baseline 4 - year survival of around 80% in the reported trials , we predicted that we would still have reasonable power ( 60% ) to detect a 5% di erence in 4 - year survival and more than 99% power to detect a 10% di erence in 4 - year survival , allowing us to compare the evidence between the two settings and ascertain if and when further meta - analyses are needed . for each trial , we extracted hrs of the e ects of docetaxel or bisphosphonates on survival and failure - free survival from trial reports , estimated them from published kaplan - meier curves or other summary statistics , 1820 or obtained them directly from trialists . 
for example , we could obtain the hr for the addition of docetaxel to standard of care plus zoledronic acid versus standard of care plus zoledronic acid alone for the stampede trial8 from the ratio of the hrs for the separate comparisons of standard of care with or without zoledronic acid and standard of care with or without zoledronic acid plus docetaxel . 
 we combined the hrs from each of the individual , eligible trials in a meta - analysis using the xed - e ect model ( mantel - haenzsel )  . 
we also used the randome ects model to assess the robustness of the results to the choice of this model for the primary analysis.22 we assessed the heterogeneity in treatment e ects between trials using the i statistic and test . 
we planned to combine all trials and , providing that su cient trials or data were available , preplanned analyses that would compare trials ( or patients within trials ) grouped by metastatic status , use of previous local cancer , planned for prostate radiotherapy as part of the standard of care , type of and length of time on androgen deprivation therapy allowed before randomisation , total planned dose of docetaxel , additional agents in the docetaxel group only , type of bisphosphonate , and dose of zoledronic acid . 
we also planned to investigate whether there were interactions between any the following covariates : age ; performance status ; tnm stage ; gleason score ; whether newly diagnosed or not ; previous androgen deprivation therapy ; and ( for m1 disease only ) the location and volume of all metastases and the volume of bone metastases . 
the interaction hr in each trial was calculated from the ratio of the estimated hrs for each subgroup ( eg , the hr for previous androgen deprivation therapy divided by the hr for no previous androgen deprivation therapy ) ; these hrs were then combined across trials using a xed - e ect meta - analysis.24 we used stata version 13 for all analyses . 
 role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results our searches of bibliographic databases , trial registers , and conference proceedings identi ed 5141 articles and records ( gure 1 )  . 
in total , 35 trials were eligible ; 14 trials were eligible for inclusion in the docetaxel comparison , and 22 the bisphosphonate comparison ( table 1 , table 2 ) .2547 one large multiarm trial ( stampede ) , 8 which incorporates multiple treatment comparisons in men with both m0 and m1 disease , contributes to both the docetaxel and bisphosphonates meta - analyses . trials were eligible for in men with m1 disease . 
one five trials compared standard of care with or without trial docetaxel ( goup 01 / 04 [ nct00796458 ] ) , including 200 men , is still recruiting , and another trial , 32 including 14 men , has yet to report suitable outcome data ( table 2 )  . 
in the three remaining trials , 7 , 8 , 10 men aged 3691 years ( median 6366 years ) with a good performance status received androgen deprivation therapy - based treatments ( standard of care ) with or without docetaxel ( table 1 )  . 
 table 2 : characteristics of studies included in the systematic review that could not be included in the meta - analyses given at a standard dose of 75 mg / m per cycle every 3 weeks for six to nine cycles , and median follow - up ranged from 29 months to 829 months ( table 1 )  . 
 all trials were assessed as being at low risk of bias ( table 3 )  . survival data from these three trials7 , 8 , 10 were available for 2992 ( 93% ) of 3206 men with m1 disease ( table 1 ) , and 1271 deaths had been recorded . 
nhs = national health service . table 3 : assessment of risk of bias 40 patients ( 3% of total randomised ) excluded from analyses ; seven patients were ineligible ; 27 patients withdrew consent ; six patients were lost to follow - up ; exclusions are balanced by group in the primary analysis , no randomised patients were excluded from the analyses ; in the analysis with long - term follow - up , 37 patients were excluded as they had not been agged with the nhs information centre in the primary analysis , no randomised patients were excluded from the analyses ; in the analysis with long - term follow - up , 33 patients were excluded as they had not been agged with the nhs information centre all randomised patients included in the analyses reports survival , but not failure - free survival as de ned in the meta - analysis reports survival , but not failure - free survival as de ned in the meta - analysis reports survival , but not failure - free survival as de ned in the meta - analysis yes , outcomes of interest are reported , including survival and failure - free survival translates to a 9% ( 95% ci 514 ) absolute improvement with standard of care plus docetaxel relative to standard of care alone ( gure 2 )  . 
statistical heterogeneity was very low throughout all analyses , so the estimates generated using a random - e ects model were consistent with those generated with the xed - e ect model . failure - free survival was de ned similarly in all trials . 
 however , in the stampede trial , 8 only prostate cancer speci c deaths were included ( rather than death by any cause ) , and in the chaarted trial7 the most similar reported outcome to our de nition of failure - free survival was time to hormone - refractory disease , which was de ned as the time from randomisation until clinical or serological progression . 
all trials were assessed as being at low risk of bias ( table 3 )  . survival results were available for 2740 ( 88% ) of 3109 men from three trials , and 1365 deaths have been recorded . 
again , we found no evidence of variation between the trial results . we identi ed 11 trials that compared standard of care with or without docetaxel for men with non - metastatic disease ( m0 )  . 
two trials ( can - ncic - pr12 [ nct00651326 ] and 05 - 043 [ nct00116142 ] ) , including 398 men , have nished accrual but have yet to report any results . 
the four remaining trials , 8 , 25 , 27 , 28 all of which have reported survival or failure - free survival , or both , were included in the meta - analysis . 
men of median age 6266 years ( ranges not reported for all trials ) with non - metastatic disease and good performance status were randomly assigned to receive standard of care with or without docetaxel ( table 1 )  . 
docetaxel was given at a standard dose of 75 mg / m per cycle every 3 weeks for six cycles , except in one trial , 25 which used docetaxel 70 mg / m plus estramustine 10 mg / kg on days 15 of each cycle . 
all trials were assessed as being at low risk of bias ( table 3 )  . survival data were available for 2121 ( 53% ) of 3978 men from three of the four trials , 8 , 25 , 28 and 340 deaths have been recorded . 
the meta - analysis hr of 087 ( 95% ci 069109 ; p = 0218 ) translates to a potential absolute improvement of 2% ( 95% ci 2 to 7 ) , assuming a typical baseline 4 - year survival of 80% ( gure 2 ) ; however , the con dence intervals are wide , and the result is not statistically signi cant . 
we found no evidence of variation between the trial results . failure - free survival was de ned consistently in all four trials , 8 , 25 , 27 , 28 but in the stampede trial , 8 only prostate cancer - speci c deaths were included ( rather than death by any cause ) , and the getug - 12 trial26 included time - to - salvage treatment . 
the meta - analysis hr of 070 ( 95% ci 061081 ; p < 00001 ) translates to an absolute improvement of 8% ( 95% ci 510 ) , reducing 4 - year failure rates from 30% to 22% , assuming a baseline 4 - year failure - free survival of 70% ( gure 2 )  . 
again , no evidence exists of variation between the trial results . we identi ed seven trials that compared standard of care with or without bisphosphonates in men with m1 disease . 
the results of one trial ( kyuh - trigu0705 [ nct00685646 ] ) , including 227 men , have yet to be reported , and in three other trials , 37 , 42 , 47 including 142 men , skeletal - related events , changes in bone mineral density , or both were the primary outcomes , and survival was not reported ( table 2 )  . 
in the three remaining trials , 8 , 12 , 30 men of median age 6671 years ( range 4088 ) with good performance status were randomly assigned to receive standard of care with or without either zoledronic acid8 , 30 or sodium clodronate12 ( table 1 )  . 
however , when the analysis was restricted to the two trials ( 1107 deaths among 2462 men ) that compared standard of care with and without zoledronic acid , we found no evidence of a bene t of standard of care plus zoledronic acid ( hr 094 [ 95% ci 083107 ] ; p = 0323 ) , with a potential absolute improvement in survival of 2% ( 95% ci 3 to 7 ; gure 3 ) , although these di erences were not statistically signi cant . 
 in the one trial of sodium clodronate , 12 a clear treatment bene t was reported ( hr 077 [ 95% ci 060098 ] , p = 0032 )  . failure - free survival was only reported in one trial , with other trials reporting a variety of intermediate outcomes ( eg , bone metastases - free survival , time to rst skeletal - related event ) , such that no formal meta - analysis was possible . we identi ed 17 trials that compared standard of care with or without bisphosphonates for men with m0 disease . 
the results of three trials ( cecog [ nct00181584 ] , zenith [ nct00063609 ] , and nu - 02u1 [ nct00058188 ] ) , including 646 men , are unpublished , and ten other trials , 3641 , 4346 including 1494 men , have reported results for outcomes other than survival ( table 2 )  . 
in the four remaining trials8 , 12 , 21 , 29 included in the meta - analysis , men aged 4087 years ( median 6670 years ) with good performance status were randomly assigned to receive standard of care with or without either zoledronic acid8 , 21 , 29 or sodium clodronate12 ( table 1 )  . 
in two of the trials , 21 , 29 zoledronic acid was given at a dose of 4 mg every 3 months for either 18 months or 4 years , whereas in the third trial , 8 zoledronic acid 4 mg was given every 3 weeks for 2 years . 
all trials were assessed as being at low risk of bias ( table 3 )  . follow - up across trials ranged the survival results were available for 4079 ( 66% ) of 6220 men from four trials , and 918 deaths have been recorded . 
assuming a baseline 4 - year survival of 80% , this hr translates to a potential absolute detriment in survival of 1% ( 95% ci 3 to 2 ; gure 3 ) , although this is not statistically signi cant , and we found no evidence of variation between the trial results . 
results were similar when the analysis was restricted to trials that tested standard of care with or without zoledronic acid ( three trials , 637 deaths , 3608 men ; hr 098 [ 082116 ] ; p = 0782 ) , suggesting no potential absolute improvement in survival ( 0% , [ 95% ci 3 to 3 ] ; gure 3 ) , again with no evidence of variation between the trial results . 
failure - free survival was only reported in one trial so no formal meta - analysis was done . for both the docetaxel and bisphosphonate comparisons , far fewer results were available for the m0 disease setting than for the m1 setting , which is why the meta - analyses for the m1 and m0 settings are presented separately . 
moreover , within these meta - analyses , not enough trials have assessed whether any e ect varied by other trial characteristics ( eg , use of radiotherapy plus androgen deprivation therapy )  . 
also , results by patient 252 vol 17 february 2016 articles subgroup were either too sparse , or the de nitions too inconsistent , to allow for meaningful analyses from the available reported data . discussion this meta - analysis provides substantial and reliable evidence that adding docetaxel to standard of care improves the survival of men with m1 disease , with an absolute improvement of around 9% at 4 years . 
for men with m0 disease , evidence to date supports an 8% reduction in absolute failure rates at 4 years with docetaxel , but the evidence is insu cient to reliably assess the e ects on survival . 
although evidence suggests the addition of bisphosphonates to standard of care for men with m1 prostate cancer , this e ect appeared to be largely driven by one trial of the drug sodium clodronate , and our results suggest that any potential bene t of zoledronic acid is small . 
we found no evidence that bisphosphonates improve survival in men with m0 disease . improved survival with cancer the results are reliable and robust for men with m1 hormone - sensitive prostate treated with docetaxel because , although based on three trials only , these results are derived from 93% of all men who were randomly assigned to treatment groups and 1271 deaths . 
although additional results might become available in this setting , from both the goup 01 / 04 and the gentax32 trials , these results are unlikely to materially a ect our ndings . 
importantly , however , in three of the included trials7 , 8 , 10 most of the men who were randomly assigned to treatment groups were newly diagnosed with metastatic disease . 
while we see no reason for why the observed bene t of docetaxel should not be generalisable , the only way to appropriately assess this , or any other remaining questions , is through the collection and re - analysis of individual participant data . 
nevertheless , docetaxel combined with androgen deprivation therapy should be considered a new standard of care for men with metastatic disease starting on long - term androgen deprivation therapy for the rst time who are t to receive chemotherapy and willing to accept these risks . 
future trials in this setting should also consider this as an appropriate control group.48 in men with non - metastatic disease , we found evidence that docetaxel improves failure - free survival ; however , this conclusion is based on data from four trials including just over half of all men who were randomly assigned to treatment groups . 
nevertheless , as the estimate of e ect ( hr 070 ) is in keeping with that for men with metastatic disease ( hr 064 ) and the con dence interval is narrow , this nding provides a clear and early signal of potential bene t . 
for overall survival , however , the available data are less mature , such that the estimate of e ect is based on half of all men who were randomly assigned to treatment groups and 340 deaths , and the con dence interval is wide . 
this meta - analysis will be important to update , to include mature results of unreported trials and long - term followup of those already reported , to reliably assess any e ect of docetaxel on survival . 
we will need to collaborate with trial investigators to determine when these data are likely to emerge so that we can predict when a meta - analysis that includes a much larger proportion of the men randomised in this setting and provides su cient power to detect moderate survival bene ts will be feasible . 
thus , we will also need to examine the e ects of docetaxel on prostate cancer - speci c survival , which will only be possible through our planned international individual participant data meta - analysis . despite the bene ts of bisphosphonates with respect to skeletal - related events and bone pain , 49 , 50 the e ect of bisphosphonates on survival in men with hormonesensitive prostate cancer is less clear . 
in men with m1 disease , although based only on three trials , these results represent 87% of men who were randomly assigned to treatment groups and suggest a small potential survival bene t . 
in the non - metastatic setting , although based on only four of 17 trials , the analysis includes around 65% of randomly assigned men , and we found no evidence of a bene t of bisphosphonates on survival . 
 data from other identi ed trials might provide enough power to detect a small bene t , but our results at present suggest that even a small bene t of zoledronic acid is unlikely . in both the metastatic and non - metastatic disease settings , we are aware of a number of limitations of a meta - analysis based on trials of bisphosphonates , not least that many of the trials identi ed in the systematic review have not reported survival and so could not contribute to the meta - analysis . 
for example , in the stampede trial , 8 treatment was stopped at the time of progression , whereas in the calgb 90202 trial , 30 patients crossed over to receive zoledronic acid when evidence of biochemical failure was found . 
the ongoing icecap the most in men with appropriate hormone - sensitive prostate cancer . initiative51 should help de ne intermediate outcomes the two trials rigorous systematic review methods helped us treatment identify all relevant comparisons , they were irrespective of whether completed or reported . 
this approach allowed us to decide prospectively when we would be likely to have su cient data and power to detect meaningful e ects of docetaxel or bisphosphonates in combination with standard of care , at least in the m1 disease setting . 
 despite knowing that there would be fewer data and less power to assess the e ects of both treatments in the non - metastatic disease setting than in the metastatic disease setting , we have been able to establish early signals of both bene t ( docetaxel ) and no bene t ( bisphosphonates ) , consistency of results with those in metastatic disease , and whether new data are likely to change the results . 
by using an approach that is responsive to the emerging trial results and adaptive to potential future data , we have been able to achieve robust answers to speci c therapeutic questions quickly and determine which meta - analyses will need updating in the future and which will require individual patient data for more reliable and detailed results . in summary , for men with metastatic prostate cancer starting therapy for the rst time , we found strong evidence to support the addition of docetaxel to androgen deprivation therapy as the new standard of care , and this combination should be o ered to men who are t to receive chemotherapy . 
more reliable evidence of the e ect of docetaxel on overall survival and prostate cancer - speci c survival is still needed in the m0 disease setting and will be achieved through our planned collaborative international meta - analysis of individual participant data . 
 although additional trials are yet to be reported , the suggestion from our analyses is that any likely bene t of zoledronic acid will probably be small and not clinically meaningful . contributors sb , clv , lhmr , jft , mrs , and df comprised the project management group and , with the help of la , nwc , kf , gg , ndj , mdm , mkbp , cjs , and bt ( the international advisory group ; appendix p 6 ) , contributed to the conception of the study . 
the international advisory group contributed to the interpretation of the results and various revisions of the article . declaration of interests la has been on advisory boards at amgen and sano  . 
cjs has been a consultant for sano , janssen , astrellas , bind therapeutic , leuchemix , and bayer healthcare , has stock ownership in bind therapeutics and genentech , has patents in parthenolide ( dimethylaminoparthenolide ) as a cancer treatment and a patent pending with exelixis . 
mrs has received educational grants from astrellas , janssen , novartis , p zer , and sano - aventis and has received drug and distribution costs from merck & co . 
clv , sb , lhmr , nwc , df , gg , mkbp , and jft declare no competing interests . acknowledgments the stopcap steering group thanks all patients who participated in the trials and contributed to this research . 
the project management group was funded by the uk medical research council . correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections surgical treatment and survival from colorectal cancer in denmark , england , norway , and sweden : a population - based study sara benitez majano , chiara di girolamo , bernard rachet , camille maringe , marianne grnlie guren , bengt glimelius , lene hjerrild iversen , edrun andrea schnell , kristina lundqvist , jane christensen , melanie morris , michel p coleman , sarah walters summary background survival from colorectal cancer has been shown to be lower in denmark and england than in comparable high - income countries . 
we used data from national colorectal cancer registries to assess whether differences in the proportion of patients receiving resectional surgery could contribute to international differences in colorectal cancer survival . methods in this population - based study , we collected data from all patients aged 1899 years diagnosed with primary , invasive , colorectal adenocarcinoma from jan 1 , 2010 , to dec 31 , 2012 , in denmark , england , norway , and sweden , from national colo rectal cancer registries . 
we used logistic regression to predict the resectional surgery status patients would have had if they had been treated as in the best performing country , given their individual characteristics . findings we extracted registry data for 139 457 adult patients with invasive colorectal adenocarcinoma : 12 958 patients in denmark , 97 466 in england , 11 450 in norway , and 17 583 in sweden . 
3 - year colon cancer survival was lower in england ( 639% , 95% ci 635643 ) and denmark ( 657% , 647668 ) than in norway ( 695% , 684705 ) and sweden ( 721% , 712730 )  . 
rectal cancer survival was lower in england ( 697% , 691703 ) than in the other three countries ( denmark 725% , 711740 ; sweden 741% , 727754 ; and norway 750% , 731768 )  . 
3 - year survival after stage ii or iii rectal cancer and stage iv colon cancer was consistently lower in england ( stage ii rectal cancer 864% , 95% ci 850876 ; stage iii rectal cancer 755% , 742767 ; and stage iv colon cancer 205% , 199211 ) than in norway ( 941% , 915960 ; 834% , 801861 ; and 330% , 310351 ) and sweden ( 929% , 908946 ; 806% , 782827 ; and 237% , 220253 )  . 
3 - year survival after stage ii rectal cancer and stage iv colon cancer was also lower in england than in denmark ( stage ii rectal cancer 912% , 888931 ; and stage iv colon cancer 235% , 219251 )  . 
the total proportion of patients treated with resectional surgery ranged from 47 803 ( 684% ) of 69 867 patients in england to 9582 ( 813% ) of 11 786 in sweden for colon cancer , and from 16 544 ( 599% ) of 27 599 in england to 4106 ( 708% ) of 5797 in sweden for rectal cancer . 
this range was widest for patients older than 75 years ( colon cancer 19 078 [ 597% ] of 31 946 patients in england to 4429 [ 809% ] of 5474 in sweden ; rectal cancer 4663 [ 457% ] of 10 195 in england to 1342 [ 619% ] of 2169 in sweden ) , and the proportion of patients treated with resectional surgery was consistently lowest in england . 
in the hypothetical scenario where all patients were treated as in sweden , given their age , sex , and disease stage , the largest increase in resectional surgery would be for patients with stage iii rectal cancer in england ( increasing from 703% to 882% )  . interpretation survival from colon cancer and rectal cancer in england and colon cancer in denmark was lower than in norway and sweden . 
differences in patient selection for surgery , especially in patients older than 75 years or individuals with advanced disease , might partly explain these differences in international colorectal cancer survival . funding early diagnosis policy research grant from cancer research uk ( c7923 / a18348 )  . copyright 2018 the author ( s )  . 
 analysts who did this research pointed to the need for research into differences in stage - specific treatment between these countries . added value of this study we used national population - based clinical data to compare stage - specific survival of patients diagnosed with primary colorectal adenocarcinoma in denmark , england , norway , and sweden between 2010 and 2012 , and to assess whether the international survival differences could be explained by differences in patient care . 
we showed that net survival up to 3 years after colon cancer was substantially lower in england and denmark than in norway and sweden , and survival from rectal cancer was lower in england than in the other three countries . 
we also found a steep declining age gradient in the probability of receiving resectional surgery in england , which was less noticeable or not evident in the other countries . implications of all the available evidence these findings have important policy implications , showing that the colorectal cancer survival deficit in england can be attributed partly to shortfalls in treatment . 
we highlight the need for more patient data on comorbidities , frailty , and additional therapies to understand these differences better . the primary treatment for colorectal cancer is surgical removal of the main tumour or tumours and affected tissues . 
total mesorectal excision became the standard surgery for rectal cancer in denmark , norway , and sweden in the mid - 1990s68 and some years later in england.9 this technique entails the removal of the rectum and surrounding tissues , including lymph nodes and fascia , 10 and requires particular surgical training and skills to secure good results . 
the surgical principle of resection in the embryological plane , which is used in mesorectal excision , was later applied to colon cancer surgery , with favourable results in terms of recurrences and survival.11 , 12 preoperative ( neo - adjuvant ) or postoperative ( adjuvant ) radiotherapy or chemotherapy can be used to reduce the risk of recurrence and treat micrometastases.13 , 14 the decision to treat patients with colorectal cancer with neo - adjuvant or adjuvant therapy depends on the extent of disease and risk of recurrence . 
in general , clinical guide lines do not recommend additional therapy for early - stage colon tumours or rectal tumours treated with surgery with adequate resection margins.1315 the use of neo - adjuvant or adjuvant therapy for stage ii or iii tumours is variable betweenand within16countries , particularly for rectal tumours.17 we used population - based data from national colorectal cancer registries to estimate stage - specific and age - standardised net survival at 3 years of patients diagnosed with colorectal cancer in denmark , england , norway , and sweden , and to compare the proportions of patients receiving resectional surgery in those countries by patient and tumour characteristics . methods study design and data sources in this population - based study , we included all patients aged 1899 years diagnosed with primary , invasive colorectal adenocarcinomas from jan 1 , 2010 , dec 31 , 2012 . 
patients diagnosed by their death certification alone and patients with records with invalid date sequences were excluded.18 in denmark , england , and norway , we extracted data from population - based national cancer registries . 
by linking individual patient records in denmark to the danish colorectal cancer group database , 19 additional clinical information was available for 11 746 ( 907% ) patients registered with colorectal adenocarcino mas in the danish national cancer registry . 
similarly , 97 185 ( 997% ) english national cancer registry records for patients with colorectal cancer were linked to at least one of the national bowel cancer audit data , hospital episode statistics inpatient and outpatient records , and the cancer waiting times monitoring data set . 
norwegian national cancer registry data are routinely linked to the norwegian colorectal cancer registry , a specialised registry that contains detailed clinical infor mation on all patients with colorectal cancer nationwide.8 the swedish vol 20 january 2019 for more on the danish colorectal cancer group see for the national bowel cancer audit see org.uk / for the hospital episode statistics see digital.nhs.uk / data - andinformation / data - tools - andservices / data - services / hospital - episode - statistics for the cancer waiting times monitoring data set see information / data - collectionsand - data - sets / data - collections / cancerwaitingtimescwt for the norwegian colorectal cancer registry see registries / clinical - registries / colorectal - cancer - registry / articles for more on the swedish colorectal cancer registry see samverkan / cancerdiagnoser / tjocktarm - andtarm - och - anal / tjock - - och - andtarm / kvalitetsregister / see online for appendix colorectal cancer registry provided clinical data on patients with colorectal cancer in sweden ; 7 its coverage for the study period was near complete.20 definitions of clinical variables ( site , stage , or treatment ) were agreed with in - country clinicians and specialised cancer registry staff to reconcile differences in coding between the various data sources . 
some further discussions with clinicians and registry staff were held to understand and reconcile differences in coding and clinical practices in those countries . all patients included in this study were followed up from time of diagnosis until death or until dec 31 , 2014 , whichever occurred first . 
tumours with morphological codes for non - adenocarcinoma were excluded from analyses . we applied consistent quality control measures to all records ( appendix pp 12 ) .18 in cases of multiple tumours diagnosed at the same site within 6 months of each other , we retained the date of diagnosis of the first tumour ; where stage and type of surgery were inconsistent between records ( n = 327 , 023% ) , we selected the most advanced stage and most extensive surgery . 
for all patients with record of more than one surgery , we selected the most extensive surgery . disease extent ( stage ) , as defined by the union for international cancer control tnm classification of malignant tumours , was characterised by applying a hierarchical algorithm previously described.22 priority was given to pathological confirmation of tumour , lymph node extension , and distant metastases ( if positive ) , over clinical tnm components . 
there is broad comparability between the main stage categories among these tnm editions.22 we defined resectional surgery as the surgical removal of the primary tumour , irrespective of the intent and outcome of surgery , done within 9 months of diagnosis . 
in denmark and england , surgical status was categorised as missing when patients were registered in the national cancer registry but were not recorded in the specialised colorectal cancer registry ( or in hospital episode statistics for england )  . 
we calculated the potential range of the proportion of patients that might have had resectional surgery in denmark and england , first assuming that all patients with missing data were treated and then assuming that they were all untreated . 
we then estimated upper and lower limits of the probable distribution of resectional surgery in each of these countries . information regarding radiotherapy and planned chemo therapy within 6 months of diagnosis was extracted from colorectal cancer registry data in denmark , norway , and sweden , and from national bowel cancer audit and cancer waiting times records in england . we hold approvals from the uk health research authority ( reference ecc 304 ( i ) / 2011 ) , the national health service research ethics service ( 11 / lo / 0331 ) , and the london school of hygiene & tropical medicine ( lshtm , 12171 )  . 
we have a data proces sing agreement with the danish cancer society and approval from the danish data protection agency to use data from the danish colorectal cancer group ; a data disclosure agreement with the cancer registry of norway to use the norwegian data ; and ethical approval from the regional ethical committee in uppsala to use the swedish data . 
data were extracted and transferred with a standard data structure protocol and file transmission procedure , in line with the concord programme for the global surveillance of cancer survival.24 outcomes our primary aim was to assess the estimated agestandardised net survival up to 3 years after diagnosis by country and disease stage and the estimated probability of patients receiving resectional surgery by stage and age in each country . 
we also estimated the hypothetical change in the probability of receiving resectional surgery that patients would have had if they had been treated as in the best performing country , given their individual characteristics . statistical analysis we compared the demographic and clinical characteristics of patients with colorectal cancer diagnosed in denmark , england , norway , and sweden , including patients age , sex , and disease stage . 
received within 6 months of diagnosis ; sources and completeness of information on chemotherapy or radiotherapy varied greatly between countries , with a high proportion of missing information in england . 
 table 1 : characteristics of patients diagnosed with colorectal adenocarcinoma , 201012 information on the cause of death , ( background mortality ) and is suitable for use in international comparisons of survival because background mortality differs between countries . 
in the absence of reliable the background mortality hazard was provided by life tables for the general population defined by country , sex , single year of age , and year.26 we used a multivariable modelling approach to estimate the excess mortality hazard ( ie , due to colorectal cancer ) and predict net survival . 
we used a model selection strategy to test for non - linearity and time dependence of the effects of sex and age on the excess mortality hazard and their interactions.27 survival was predicted by age group , defined by the international cancer survival standard . 
we used international cancer survival standard weights to produce a weighted average of the survival estimates ( age - standardisation ) , to allow for differences between countries in the age distribution of the population of patients with cancer.28 we used the stata command strcs to fit flexible parametric survival models on the log - hazard scale.29 we used multivariate logistic regression models to compare the probability of receiving resectional surgery between countries . 
subsequently , we applied the model coefficients of the best performing country to individuals from the other countries , to assess the hypothetical change in the probability of receiving resectional surgery if patients had been treated as in the best performing country , given their observed characteristics . 
the corresponding author had full access to all the data in the study , and the final responsibility for the decision to submit for publication . results we included information from 139 457 patients diagnosed with colorectal adenocarcinoma in england , denmark , norway , and sweden in our analyses . 
in patients with known disease stage , the proportion diagnosed with stage iiii colon cancer was higher in sweden than in england , vol 20 january 2019 articles norway , and denmark ; for rectal cancer , the proportion diagnosed with stage iiii rectal cancer was higher in england than in sweden , denmark , and norway ( table 1 )  . 3 - year age - standardised net survival from colon cancer was higher in sweden and norway than in denmark and england . 
3 - year survival from rectal cancer was generally similar between denmark , norway , and sweden , and lower in england ( table 2 )  . net survival decreased with the increase in disease stage ( table 2 , figure 1 )  . 
3 - year survival for patients with stage ii tumours was about 90% or higher in all countries , although survival for patients with rectal or colon cancer in england and colon cancer in denmark was notably lower than for patients in sweden or norway . 
 although generally higher than 75% , survival for patients with stage iii colon and rectal cancer was lower in england than in norway and sweden up to 3 years after diagnosis , and in denmark 1 year after diagnosis . 
resectional surgery defined as surgery to remove the primary tumour within 9 months of diagnosis , excluding diagnostic and palliative procedures . table 3 : proportion of patients diagnosed with colorectal adenocarcinoma in 201012 that received resectional surgery by age , sex , and disease stage 205% for england and 330% for norway at 3 years . 
for stage iv rectal cancer , survival was lowest in sweden and england ( 267% in sweden and 271% in england ) and highest in norway ( 385% ) at 3 years ( figure 1 )  . the overall proportion of patients who received resectional surgery was higher for colon than for rectal cancer in all countries ( table 1 )  . 
we could not establish the surgical status of some patients in denmark because they were not registered in the danish colorectal cancer group database ( 949 [ 111% ] of 8567 patients with colon cancer and 263 [ 60% ] of 4391 patients with rectal cancer )  . 
patients with colorectal cancer who were not registered in the danish colorectal cancer group database were more likely to have advanced stage disease or missing stage information and be slightly older than patients registered in the database . 
data on surgery were unavailable for 03% of patients with colorectal cancer in england because their national cancer registry records could not be linked to the additional databases ( hospital episode statistics , national bowel cancer audit , or cancer waiting times )  . 
the proportion of patients receiving resectional surgery was highest in sweden and lowest in england , for both types of cancer ( table 1 )  . in younger patients the proportion of patients treated with resectional surgery was lower in individuals aged 75 years or older than in each country , and international differences in resectional surgery use widened with increasing age of patients ( table 3 )  . 
the share of patients aged 75 years or older with colon cancer with evidence of resectional surgery varied from 19 078 ( 597% ) of 31 946 patients in england to 4429 ( 809% ) of 5474 in sweden . 
in patients aged 75 years or older with rectal cancer , the share of those with resectional surgery varied from 4663 ( 457% ) of 10 195 patients in england to 1342 ( 619% ) of 2169 in sweden . 
for rectal cancer , norway and sweden had the highest proportions of resectional surgery for all but the youngest age group , where denmark had the highest proportion of patients treated . 
england had the lowest proportion of patients treated with resectional surgery for rectal cancer in all age groups and for colon cancer in the two oldest age groups ( table 3 )  . to account for differences in disease stage distribution , we examined the proportion of patients treated by stage and age group ( figure 2 )  . 
the proportion of patients with colon cancer with evidence of resectional surgery for each stage and age group was mostly similar between the four countries for stages i and ii and in patients aged 75 years or younger . 
 however , we observed a steep decline in the proportion of patients that had surgical treatment in the older age categories in england for each disease stage and for both types of cancer , which was not evident in the other countries ( figure 2 )  . 
for instance , a higher proportion of patients received resectional surgery for stage i colon tumours in the 7584 age group than in the 85 and older age group in all countries , but the absolute difference between these age groups was 180% in england vol 20 january 2019 articles compared with 2955% in the other countries . 
information on surgery was missing for some patients in denmark and for a small proportion of patients in england : light grey areas represent the proportion of patients with unknown surgical status by stage and age group ; overall height of the bars shows the proportion of patients that would receive surgery if all patients with missing treatment data had surgical treatment . vol 20 january 2019 articles denmark england norway sweden * colon : stage i colon : stage ii colon : stage iii colon : stage iv rectum : stage i rectum : stage ii rectum : stage iii rectum : stage iv being treated with resectional surgery in any of the four countries . 
however , for patients with rectal cancer diagnosed with stage iiiiv disease , the proportion treated was lower in england than in the other countries in our study , particularly in the oldest age groups ( figure 2 )  . 
we observed an age gradient in the proportion of patients receiving resectional surgery with all rectal cancer stages in denmark , england , and sweden , with lower proportions among patients aged 85 years or older than among younger patients . 
for instance , between patients aged 7584 years and those aged 85 years or older , the absolute difference in the proportion of patients who received resectional surgery for stage iii rectal tumours was 296% in england , 209% in sweden , and 128% in denmark . 
we found no age gradient in the proportion of patients treated for rectal cancer in norway , except for patients with stage iv cancer . to assess the validity of our findings and check whether the age differences in the likelihood of patients receiving resectional surgery were driven by differences in the management of patients diagnosed at aged 90 years or older , we repeated the analyses with exclusion of this patient group . 
the patterns we observed persisted in this reanalysis ( appendix pp 3 , 67 )  . overall , sweden had the highest survival for colon and rectal cancer and the highest proportion of patients receiving resectional surgery , compared with those of the other countries ( although outcomes in norway were generally similar , or better in specific strata , to those in sweden )  . 
to highlight any groups of patients who might be at a disadvantage in the likelihood of receiving resectional surgery compared with patients in other countries , we applied the coefficients for sweden to data from the other three countries and interpreted it as the probability of a patient receiving resectional surgery if they had been treated as in sweden , given their observed age , sex , and disease stage . 
the number of events per parameter was above the recommended threshold of ten in all categories , 31 at 100 events per parameter for our most complex model in the category with fewest events ( stage iv rectal cancer )  . in this hypothetical scenario , changes in the proportion of patients with stage i colon or rectal cancer receiving resectional surgery would be minor ( figure 3 )  . 
in england , denmark , and norway there would be a higher proportion treated among patients with stage ii and iii colon and rectal cancer , if treated as in sweden . 
overall , the largest improvements in the proportion of patients receiving resectional surgery would be seen in patients with stage ii ( from 789% to 907% ) or iii ( from 703% to 882% ) rectal cancer in england . 
the proportion of patients receiving resectional surgery for stage iv colon cancer in denmark and england would increase ( from 391% to 511% in denmark and from 400% to 498% in england ) whereas in norway , the proportion would decrease ( from 556% to 499% ) if patients had been figure 3 : predicted probability of receiving resectional surgery by patient characteristics ( age and sex ) and tumour characteristics ( stage at diagnosis ) error bars are 95% ci . 
 * predicted probabilities of patients receiving resectional surgery by applying the coefficients of the swedish logistic model to the cohorts of patients in each country , on the basis of the country - specific distributions of patient characteristics . 
the overall height of the bars shows the proportion we would observe if all patients with missing treatment data had received surgery . among patients younger than 85 years with rectal cancer who were diagnosed with stage i or ii disease , we observed no significant differences in the likelihood of vol 20 january 2019 articles treated as in sweden . 
the hypothetical decrease in the proportion of stage iv patients receiving surgery in norway would be even larger for rectal cancer ( from 474% to 288% )  . patients with missing disease stage were slightly older than the mean age for each country and cancer type ( range 753773 years for colon cancer and 745754 years for rectal cancer )  . 
the proportion of patients with colon cancer without known disease stage who had evidence of having resectional surgery was lower than that of any known stage category in each country and higher in england than in the other three countries ( table 3 )  . 
additionally , survival of these patients was higher than that of patients with known stage iii disease and lower than that of patients with known stage iv disease , in all four countries ( table 2 )  . discussion in this study , to understand the mechanisms underlying international differences in cancer outcomes , we compared the characteristics of patients diagnosed with colorectal adenocarcinoma in denmark , england , norway , and sweden . 
we provide updated figures of up to 3 - year net survival in these countries , and our results support previous findings of lower survival for patients in england and , to a lesser degree , in denmark , than in sweden or norway.25 our results also support findings that denmark seems to be closing the survival gap with sweden and norway , particularly for rectal cancer.4 , 6 , 24 in the stagespecific analyses , we noted no significant differences between countries in survival for patients diagnosed with early stage ( i or ii ) colorectal adenocarcinomas , but wider international survival differences in patients with more advanced disease stages ( iii or iv )  . 
additional information on treatment , available from specialised colorectal cancer registries , helped us to understand these survival differences better . cancer survival is largely determined by receipt of potentially curative treatment , which , in the case of colorectal cancer , is primarily surgery . 
treatment options mainly depend on disease stage and the underlying health status of patients , which is determined by their comorbidities , frailty , and age . clinical guidelines for cancer treatment aim to standardise and assure adequate cancer care for a population . 
 the amount of detail in the national clinical guidelines regarding colorectal cancer management varied , with recom mendations from england being generally less specific than guidelines from denmark , norway , and sweden.14 , 15 , 32 , 33 nonetheless , indications for surgery were largely consistent between these countries , especially for rectal tumours . 
treatment guidelines for colon cancer in denmark , norway , and sweden explicitly recommend the removal of the part of the bowel that contains the tumour and its mesentery ( and en - bloc resection , if the visceral fascia is compromised because of ingrowth of the tumour into neighbouring organs ) .13 , 14 , 32 by contrast , english guidelines recognise mesorectal excision as the standard surgery for most rectal tumours but do not explicitly recommend the corresponding procedure ( dissection in the embryological plane ) for colon tumours.15 none of the guidelines for the countries in our study mentions age as an exclusion criterion for receiving surgical treatment . 
older patients ( aged 75 years or older with stage iiiv rectal cancer or stage iv colon cancer and aged 85 years or older for the other stages of rectal and colon cancer ) in england had a lower probability of receiving resectional surgery than patients of a similar age with similar disease extension in the other three countries , and a lower probability than younger patients in england . 
england had the steepest negative age gradient in the proportion of patients receiving resectional surgery and had a survival deficit in comparison with the other three countries , particularly for rectal cancer . 
conversely , we noted a higher proportion of patients younger than 85 years who were diagnosed with stage i or ii tumours who had evidence of resectional surgery in england than in the other three countries . 
of the countries studied , only england had a colorectal cancer screening programme with national coverage during the study period.34 the diagnosis and treatment of asymptomatic disease through screening might explain the high proportion of patients surgically treated for early stage disease in the eligible age group in england . 
in the other countries in our study , screening was not imple mented at national level during the study period34 and could not have affected the disease stage distribution or population - based survival . although less aggressive treatment for older patients might sometimes be justified because of comorbidity or frailty , concerns have been raised that some of the disparities in age - related cancer care in england arise because of clinical decision making on the basis of chronological age.35 a 2011 report36 showed lower resection rates in older patients with cancer in england during 200406 than those of younger patients , with less than 2% of patients aged 80 years or older having a major resection surgery for six of 13 cancers examined . although an increase in the proportion of patients receiving resectional surgery does not necessarily translate into better short - term survival because aggressive treatment might be associated with high short - term vol 20 january 2019 articles that mortality , our findings suggest international differences in survival are , at least in part , determined by differences in patient selection practices for surgical treatment . 
choices in management of older patients with colorectal cancer might greatly affect populationbased survival because the mean age at diagnosis is about 70 years.37 patients in countries with a greater proportion of patients treated with surgery and better short - term fewer complications survival might also have more access to laparoscopic surgery or better postoperative care than in the other countries . 
although there is conflicting evidence about the long - term benefit of a laparoscopic versus an open surgical approach for rectal cancer , 38 , 39 laparoscopic surgery is associated with lower perioperative mortality and surgery.40 , 41 in denmark , the increasing use of laparoscopic surgery for colorectal cancer has been associated with a reduction in perioperative mortality rates.42 differences between countries in the use of this approach might explain some of the differences in the proportion of patients receiving surgical treatment and , potentially , in survival . 
however , we were not able to account for this information in our analysis because not all datasets had sufficiently complete data for this question . than open our study has some limitations . 
these include core variables that have previously been examined for comparability and validated in these and other european colorectal cancer registries.43 however , some residual data quality issues might affect the comparability of results . 
performance status scales , which are commonly used to assess patients general condition ( such as their degree of independence ) and eligibility for specific treatments , 44 might not be ideal for older patients with cancer , especially those with mul tiple comorbidities.45 although comprehensive geriatric assessment scales have been proposed and validated , 45 they are rarely used , documented , or routinely collected.46 nevertheless , at the population level , the burden of cardiovascular disease the most common contra indication for surgeryis similar in the four countries included in our study.47 population - based all - cause mortality and life expectancy in older ages are also similar in these four countries ( appendix p 4 ) , supporting the validity of the findings in our study . the overall proportion of patients with unknown disease stage is notably higher in england than in denmark , norway , and sweden . 
the reasons for stage information to be missing are likely to differ according to how high or low the proportion of unknown stage is and , therefore , probably differ between countries . 
patients with unknown disease stage had a lower probability of receiving resectional surgery than patients with known stage , and had similar survival to that of patients with advanced disease stages . 
therefore , our complete - case analysis might overestimate stage - specific survival and the proportion of patients receiving resectional surgery in england , and provides a conservative estimate of the disparities between england and the other three countries in our study . in denmark , 93% of patients were not registered in the danish colorectal cancer group database and thus , their treatment status remained undetermined . 
by contrast with the danish national cancer registry , the danish colorectal cancer group database only includes adults with a first - time diagnosis of colorectal adenocarcinoma treated in danish public hospitals who were in contact with a surgical department.19 therefore , we calculated a potential range of the proportion of patients that might have had resectional surgery and estimated upper and lower limits of the probable distribution of resectional surgery in denmark . 
because of the danish colorectal cancer group databases exclusion criteria and the stage distribution of patients without a danish colorectal cancer group database record , it is probable that a substantial number of these patients did not undergo resectional surgery . 
assuming that none of these patients received resectional surgery , the proportion of patients with rectal cancer who received resectional surgery was still higher in denmark than in england and similar to that in sweden for most combinations of age and disease stage . 
nevertheless , these missing data might have masked some age and stage trends in the likelihood of patients undergoing resectional surgery , especially for colon cancer . we were not able to ascertain treatment intent , residual disease status , venous invasion status , or postoperative complications in patients who received resectional surgery . 
systematic differences in the distribution of such patients between these four countries , or differences in their perioperative management , might affect the between - country comparability of these results . 
 further more , patients with non - resectable tumours in better - performing countries might be more likely to be offered other treatment ( such as treatment to prolong life or make tumours amenable to resection ) than patients in worse - performing countries . 
for example , clinical the guidelines importance of neo - adjuvant or conversion treatment of metastatic tumours to render them resectable , 13 , 14 whereas guidelines in england prioritise symptom control and state that initial systemic treatment followed by surgery should be considered only if both primary and metastatic in norway and sweden describe vol 20 january 2019 articles tumours are judged to be resectable.15 moreover , in countries that frequently use neo - adjuvant therapy with delayed surgery for rectal cancer , the resulting downstaging could cause an under estimation of the differences in stage - specific survival when these countries are compared with settings where neo - adjuvant treatment is more variable or followed by immediate surgery . the completeness and granularity of the data collected by the colorectal cancer registries regarding chemotherapy and radiotherapy varied greatly during the study periodfrom complete registration of radiotherapy protocols in norway and sweden to a high proportion of missing information in england . 
adjuvant chemotherapy is associated with improved outcomes in stage iii colon cancer and is used universally , but for stage ii colon cancer and rectal cancer ( in general ) its value and therefore its use have been more variable.4850 neo - adjuvant radiotherapy decreases recur rence rates , but evidence for its effect on survival is conflicting and so use also varies within countries16 , 51 and between countries.17 the use of targeted therapy in com bination with chemotherapy might help to make tumours amenable to resection in some patients with metastatic or locally advanced disease , 52 but no survival benefit has been shown for this combination.53 for patients with metastatic disease treated with non - curative intent , optimal use of systemic therapy contributes to longer survival.52 , 54 variability between countries in the use of these additional therapies , and other differences in oncological care beyond surgery , might also contribute to the observed differences in survival . despite the limitations of the data included in our study , we have identified important international differences in the distribution of resectional surgery by age and disease stage . 
the main data quality issue ( the higher proportion of patients with unknown disease stage in england ) is likely to have led to a conservative estimate of the differences found in stage - specific survival outcomes in england compared with those of other countries . 
we noted that differences in survival between patients with colorectal cancer treated in england , denmark , norway , and sweden tended to increase with time after diagnosis , and it is possible that these differences between countries would widen with longer follow - up . changes in practice during and after the study period are likely to affect future trends . 
over the past two or three decades , colorectal cancer outcomes have improved in all the countries compared in our study.3 , 24 , 55 the centralisation and specialisation of colorectal cancer surgery have been suggested as important drivers of this improvement.4 a 2012 cochrane review56 found a clear association between operative mortality and 5 - year survival with hospital and surgeon caseload and specialisation . 
however , it is likely that centralisation and specialisation vary between the four countries in our study , and these changes in practice are also likely to affect patient survival differently in these countries.4 , 6 expedited referral routes were initiated in england and denmark in the 2000s , in response to low cancer survival related to system delays.57 , 58 similar rapid referral routes were introduced in norway and sweden in 2016 , following the danish experience . 
although diagnostic delays are important factors in cancer care , the effect of these referral routes on cancer survival remains uncertain . in denmark , a nationwide screening programme with a monitoring database was introduced in 2014.59 the norwegian directorate of health is planning to introduce a national colorectal cancer screening programme in norway in 2019 , offering a faecal immunochemical test or colonoscopy to individuals when they turn 55 years.60 similarly , a national colorectal cancer screening programme is due to be implemented in sweden in 2019 , following regional screening programmes.61 in england , a one - off screening test with flexible sigmoidoscopy for people aged 55 years is being rolled out.62 with increases in diagnosis and treatment of asymptomatic disease , it is likely that survival and the proportion of patients treated for early stage disease will increase in the future . since 2013 , surgeon - specific outcomes have been reported annually as quality measures in england.63 it is hoped that this increase in accountability will lead to improvements in patient care . 
the major reorganisation of the nhs in 2013 , 64 alongside sub stantial resource constraints in the nhs65 in the past decade , has had a potentially negative effect on cancer services . 
for instance , the 62 - day treat ment waiting time targetthe aim that a patient should wait no more than 2 months from the date that the hospital receives an urgent referral for suspected cancer to the start of their treatmenthas been missed for several quarters running , showing that services are unable to meet the demands placed on them.66 given the ongoing financial pressures and austerity in the uk and the nhs , the future trends in survival for patients with cancer in england are uncertain . our findings have important policy implications , suggesting that the colorectal cancer survival deficit in england as compared with denmark , norway , and sweden can be attributed partly to shortfalls in provision of surgical treatment . 
we showed that older patients in england , in particular , were less likely to receive resectional surgery than patients with similar characteristics in the other countries in our study . 
we posit that increases in the proportion of patients receiving resectional surgery might translate into better longer - term outcomes in england , provided that adequate postoperative care is also available . improving the capture of information on patients with colorectal cancer in specialised clinical registries , vol 20 january 2019 articles including data from individuals who are not eligible for surgery , would allow a more complete population - based comparison of colorectal cancer outcomes . 
complete and comparable data on comorbidities , frailty , and additional therapies are required to improve understanding of international differences and inequalities in cancer outcomes . contributors sw , br , mpc , and sbm designed the study . 
 jc and lhi ( denmark ) , sbm and cdg ( england ) , eas and mgg ( norway ) , and kl and bg ( sweden ) prepared national datasets according to the protocol . 
all authors had access to results at the data preparation and analysis stages , contributed to the interpretation of the results , revised and critically reviewed the manuscript , and approved the submitted version . 
sbm , cdg , sw , br , and mpc had access to all the data in the study and take responsibility for its integrity and the accuracy of the analyses . declaration of interests br reports grants from the uk department of health , outside the submitted work . 
all other authors declare no competing interests . acknowledgments this study was funded by an early diagnosis policy research grant from cancer research uk to the cancer policy programme at the london school of hygiene & tropical medicine ( lshtm ; award number c7923 / a18348 )  . 
we thank the national colorectal cancer registries in denmark , england , norway , and sweden for their sustained efforts in collecting data for patients with colorectal cancer to the highest quality standards . 
we are grateful for advice received from members of the cancer policy programme scientific advisory group ( peter sasieni , deborah ashby , paul aylin , andrew roddam , and sally vernon )  . 
we gratefully acknowledge the advice and support of members of the lshtm cancer survival group ( csg ) , especially yuki alencar ( csg coordinator ) , francisco javier rubio ( statistician ) , and adrian turculet ( csg data manager )  . farewell to four greats as we begin a new year with optimistic anticipation of further achievements in oncology , we must pause to pay tribute to four major innovators and mentors who sadly died at the start of 2019 . on jan 2 , professor waun ki hong , a pioneering physician and scientist at the md anderson cancer center ( houston , tx , usa ) , died aged 76 . 
his work contributed to notable advances in chemoprevention , organ preservation in laryngeal cancer , and personalised targeted therapy . professor bertrand coiffier , who also died on jan 2 , aged 71 , was a leading lymphoma expert , who focused on developing new drug regimens to improve outcomes for aggressive lymphoma . 
he was a professor of hematology at the hospices civils de lyon and the university claude bernard ( lyon , france ) , and was a founding member and president of the groupe detude des lymphomes de ladulte , which later merged with another group to form the world - renowned lymphoma study association . jan 7 , professor john mendelsohn , a former president of the md anderson cancer center , died from glioblastoma , aged 82 . 
he helped to develop the monoclonal antibody cetuximab , which is used to treat colorectal , head and neck , and lung cancers . martin gore , professor of cancer medicine at the institute of cancer research and medical director at the royal marsden hospital ( london , uk ) , died suddenly on jan 10 aged 67 , reportedly after a yellow fever vaccination . 
 he received a cbe in the queens 2016 birthday honours list for services to oncology . as we reflect on the untimely loss of these four inspirational , leading oncologists , this has been a sadand unprecedentedway to start 2019 . 
 the lancet oncology big influences on anti - obesity strategies obesity , the second biggest preventable cause of cancer after tobacco smoking , is a major public health problem worldwide . 
governments must take steps to address this issue ; however , recent reports suggest that chinas antiobesity policies are being influenced by external players . increasingly westernised diets , escalating rural - to - urban migration , and sedentary lifestyles have caused chinas obesity levels to more than double since 1991 . 
in response , the chinese government has launched several public health campaigns , including happy 10 minutes , which encourages schoolchildren to have daily 10 - min breaks for exercise . 
why ? according to recent studies in the bmj and the journal of public health policy , the chinese governments attempts to tackle obesity are being supported by several large multinational food companies , including coca - cola , pepsi - cola , and nestl . 
these companies fund a noninternational life profit research organisation , the sciences institute ( ilsi ) , originally established in the usa in 1978 by a coca - cola executive . 
for several decades , ilsichina has led public health initiatives emphasising the importance of exercise and physical activityrather than nutritionas key to solving the obesity proble by focusing more on physical activity than on a healthy diet , attention is diverted away from highly processed food and calorie - dense snacks and drinks . 
shaping public health policy in this way could help the funding companies to protect sales of their own products and potentially avoid food regulations , advertising rules , and sugar taxes that have been introduced elsewhere . however , diet is clearly crucial . 
governments must not allow their public health strategies to be unduly influenced by powerful multinationals who might be more concerned with protecting their own interests than helping to solve this ongoing health crisis . 
 the lancet oncology vol 20 february 2019 for the bmj report see bmj 2019 ; 364 : k5050 . for the the journal of public health policy study see j public health pol 2019 ; published online jan 9 . 
within standard - risk medulloblastoma , patients in the wnt subgroup are established as having a favourable prognosis ; however , outcome prediction for the remaining majority of patients is imprecise . 
we assessed the clinical behaviour of the molecularly defined wnt and shh subgroups , and identified novel independent prognostic markers and models for standard - risk patients with non - wnt / non - shh disease . 
because of the scarcity and low quality of available genomic material , we used a mass spectrometry - minimal methylation classifier assay ( ms - mimic ) to assess methylation subgroup and a molecular inversion probe array to detect genome - wide copy number aberrations . 
this cohort of 136 samples consisted of 28 ( 21% ) classified as wnt , 17 ( 13% ) as shh , and 91 ( 67% ) as non - wnt / non - shh ( we considered group3 and group4 medulloblastoma together in our analysis because of their similar molecular and clinical features )  . 
favourable outcomes for wnt tumours were confirmed in patients younger than 16 years , and all relapse events in shh ( four [ 24% ] of 17 ) occurred in patients with tp53 mutation ( tp53mut ) or chromosome 17p loss . 
in patients in the hit - siop pnet4 cohort with non - wnt / non - shh medulloblastoma , with a median follow - up of 67 years ( iqr 5882 ) , 5 - year event - free survival was 100% in the favourable - risk group and 68% ( 95% ci 575827 ; p = 000014 ) in the high - risk group . 
in the validation cohort , with a median follow - up of 56 years ( iqr 3181 ) , 5 - year event - free survival was 947% ( 95% ci 852100 ) in the favourable - risk group and 586% ( 95% ci 451761 ) in the high - risk group ( hazard ratio 941 , 95% ci 1257057 ; p = 0029 )  . 
the remaining subgroups of patients with high - risk medulloblastoma might benefit from more intensive therapies . funding cancer research uk , swedish childhood cancer foundation , french ministry of health / french national cancer institute , and the german childrens cancer foundation . correspondence to : prof steven c clifford , wolfson childhood cancer research centre , northern institute for cancer research , newcastle university , newcastle upon tyne , ne1 7ru , uk steve.clifford@ncl.ac.uk copyright 2018 the author ( s )  . 
 currently , who classification of cns tumours recog nises four distinct genetically defined entities ( wnt , shhtp53wildtype , shhtp53mut , and nonwnt / nonshh ) .1 nonwnt / nonshh medullo blastoma encompasses group3 and group4 , which were defined by epigenetic and mrna expression signatures2 and are considered provisional variants by the 2016 who classification.1 understanding the molecular pathology and clinical relevance of medulloblastoma subtypes provides sub for personalised riskadapted stantial opportunities therapies . discovery and validation of clinically meaningful medullo blastoma features in previous clinical trial cohorts have driven advances in the clinical management of the disease . 
children younger than 16 years of age at diagnosis with wntactivated medulloblastomas have research in context evidence before this study international consensus and the 2016 who classification recognise the following distinct clinico - molecular disease entities in medulloblastoma : wnt , shh - tp53wild - type , shh - tp53mut , and non - wnt / non - shh ( encompassing group3 and group4 )  . 
standard - risk , non - infant disease ( with 7585% 5 - year progression - free survival and affecting 5060% of patients ) represents the largest clinical treatment group of patients . 
application of novel methods to enable assessment of this cohort , and investigation of an independent demographically matched standard - risk medulloblastoma validation cohort , allowed derivation and validation of biomarker - driven , risk - stratification models on the basis of the molecular pathology of standard - risk medulloblastoma , including a novel whole chromosomal cytogenetic aberration signature within standard - risk non - wnt / non - shh medulloblastoma . 
 therefore , findings from this study resolve current patients with standard - risk medulloblastoma into biomarker - defined distinct favourable - risk and high - risk groups , and represent a substantial step in our ability to risk stratify and clinically manage medulloblastoma . implications of all the available evidence the results of this study redefine the concepts of risk stratification in standard - risk medulloblastoma , providing insight into its molecular subtypes , their underpinning biology , and clinical application . 
stratification of standard - risk medulloblastoma by use of the biomarkers and validated schemes we describe could allow assignment of 150200 patients per year in europe into a favourable - risk group , and such patients could benefit from reduction of treatment intensity . 
this group encompasses tumours of all variants except high risk shhtp53mut.6 , 7 diagnosis of favourablerisk , wnt disease ( around 20% of patients with standardrisk medulloblastoma ) provides a clear precedent for therapy deescalation within clinical trials . 
by contrast , patients with nonwnt , standardrisk medullo blastoma have ( 5year eventfree survival heterogeneous outcomes around 75% ) , and further actionable risk groups are yet to be identified or validated to the point of clinical application . 
 the favourable risk of patients with standardrisk , shh tp53wildtype medulloblastoma6 , 7 identified in retrospective series requires validation in clinical trials , and reproducible and clinically significant molecular pathological features with in nonwnt / nonshh tumours remain to be defined . 
trial participants were post operatively staged and randomly assigned to treat ment with standard or hyperfractionated radio therapy , followed by chemo therapy with eight cycles of cisplatin , lomustine , and vincristine . 
this analysis , alongside an independent , demo graphically matched , standardrisk medullo bla stoma validation cohort , enabled the discovery and validation of concerted whole chromosomal aberration signatures with prognostic value for patients with nonwnt / non shh medulloblastoma . 
the study investigated in patients aged 421 years using either hyperfractionated radiotherapy or standard delivery radiotherapy followed by chemo therapy.1 standard delivery radiotherapy comprised 234 gy to the craniospinal axis and 54 gy to the whole posterior fossa , and was given over 42 days in 30 fractions of 18 gy each day for 5 days per week . 
 eight cycles of cisplatin ( 70 mg / m intravenously ) and lomustine ( 75 mg / m ) on day 1 , and vincristine ( 15 mg / m intravenously ) on days 1 , 8 , and 15 , were given with a 6 week interval between each cycle.14 minute remnant material ( cytospinconcentrated cellular nuclei preparations ) or tumour sections , origi nally intended for fish and ihc , 15 were available for analysis ( samples from 147 patients )  . 
we retained tumours from patients with subtotally resected disease18 or categorised as mycnamplified to assess their prognostic value in a clinically controlled cohort.6 , 11 , 15 we excluded myc - amplified tumours because of their established poor prognosis.5 136 tumour samples met these criteria and underwent molecular investigation . 
median year of diagnosis 2006 . table : clinical and molecular characteristics of all cohorts vol 19 december 2018 1605 articles tumour samples ( clinical and molecular cohort ) and their prognostic features were consistent with the whole trial cohort ( table )  . we validated and extended our findings in a second independent , demographically matched , retrospective cohort of patients with nonwnt / nonshh standardrisk medulloblastoma ( n = 70 ) collected at uk childrens cancer and leukaemia group and european society for paediatric oncology ( siope ) associated treatment centres between 1990 and 2014 . 
patients in this cohort received equivalent therapies ( maximal surgical resection [ all patients ] , adjuvant craniospinal radiotherapy [ all patients ; standard radiotherapy in variable doseslow dose : 2427 gy , 39 patients ; high dose : 3539 gy , 27 patients ; hyperfractionated radiotherapy variable doses : 324 gy craniospinal radiotherapy plus 234 gy boost , one patient ; 60 gy hyperfractionated accelerated radiotherapy , one patient ; 31 / 59 gy , one patient ; and 39 / 54 , one patient ] , and chemotherapy [ 65 ( 93% ) of 70 patients ] )  . written informed consent for tumour collection for biological studies was obtained from patients or their parents . 
we analysed mutations in exons 49 of tp53 and exon 3 of ctnnb1 with sanger sequencing as previously described.21 we assessed mutations in apc using a customised next generation dna sequencing panel ( illumina ; san diego , ca , usa ) in samples with ctnnb1wildtype wnt medulloblastoma . 
we used gistic ( genomic identification of significant targets in cancer , v 1.0 ) to identify focal chromosomal aberrations ( appendix pp 1012 ) .22 we analysed the validation cohort samples on the illumina 450k dna methylation micro array ( illumina ; san diego , ca , usa ) , and estimated chromosomal and focal copy number changes by use of the r package conumee v 1.13.0 , as previously described.6 we defined a whole chromosomal aberration group of patients by hier archical clustering of recurrent ( ie , > 15% ) aberrations . eventfree survival was defined as the time from surgery to first event ( progression or relapse ) , or date of last followup . 
after molecular sub grouping , we observed similar cytogenetic changes and eventfree survival between the nonwnt / nonshh medullo blastomas subclassified as group3 and group4 ( appendix p 9 )  . 
because of these results and the emerging evidence of their shared biology , 6 , 12 we considered these groups together in subsequent eventfree survival analyses . to test the null hypothesis that eventfree survival was not associated with clinical , molecular , or patho logical variables in patients with group3 or group4 medullo blastoma , we constructed kaplanmeier curves and compared patient groups with logrank tests . using cox modelling , we tested the prognostic value of clinical markers ( gender , radiotherapy type [ hyper fractionated vs standard ] , resection outcome [ subtotal vs fullyresected disease ] , mycn amplifi cation [ yes vs no ] , histology type [ desmoplastic / nodular vs classic histo logy ] ) , ( recurrent whole chromo somal cytogenetic markers aberration [ presence vs absence ] ) , and cumulative numbers of total whole chromosomal aber rations ( gains vs losses )  . 
we derived pragmatic assignments of patient risk by combining whole chromosomal aberrations that were significantly different in univariate testing to define risk groups and assessed their predictive value by calcu lating total area under the curve ( auc ) , sensitivity , and specificity at 5 years since diagnosis ( appendix p 2 )  . 
residual scores from tests of association are shown ( darker shades of grey indicate stronger enrichment ) alongside p values from fishers exact tests . finally , to better understand the nature of the identified risk groups , we classified the validation cohort according the recently published refinements of epigenetically defined substructures within non wnt / nonshh medullo blastoma.6 , 12 validation cohort samples were assigned to subgroup variants according these published studies and visualised using tdistributed stochastic neighbour embedding ( appendix pp 23 )  . we set the significance threshold at p < 005 for all statistical tests in this study , and twotailed p values are reported . 
we assessed significance of association using fishers exact test , and visualised the strength of asso ciations using test residuals . further detailed methods are provided in the appendix pp 13 . 
event - free survival for patients with non - wnt / non - shh disease ( n = 91 ) grouped as ( e ) patients with mycn amplified vs non - amplified tumours , ( f ) patients with medulloblastomas presenting an i17q or not , and ( g ) patients with medulloblastomas with or without whole chromosomal aberration . 
we found no differences in terms of 5year eventfree survival between the four methylation subgroups ( figure 2 ; wnt 5year eventfree survival 885% , 95% ci 770100 ; group4 5year eventfree survival 816% , 733908 ; group3 5year eventfree survival 800 , 621100 ; shh 5year eventfree survival 753% , 569996 ; wnt vs group4 hr 061 , 95% ci 018212 , p = 044 ; shh vs group4 127 , 042386 , p = 068 ; group3 vs group4 113 , 032394 , p = 085 )  . 
both ctnnb1 wildtype tumours showed a copy neutral loss of vol 19 december 2018 1609 articles heterozygosity within chromosome 5q ( apc ) and we identified apc frameshift deletions ( e1309fs aaaag and q1062fs acaaa )  . 
 a previously reported shh disease risk model ( of chromosome 14 loss and gli2 amplification ) 11 showed significantly worse eventfree survival for patients in this cohort ( p = 000067 ; appendix pp 78 )  . 
as expected , we observed structural cytogenetic ( eg , i17q ) and focal aberrations ( including mycn amplifications , otx2 , ccnd2 , and 18q12 [ tpte2 ] gains or ampli fications , sncaip dupli cations , and 13q1112 [ setbp1 ] loss ; figure 1 ; appendix pp 1112 )  . 
moreover , previously reported prognostic ( mycn amplification , i17q alterations , and sub total resection ) 11 , 18 were not associated with worse eventfree survival ( figure 2 ; appendix p 15 ) , while the observed cohortwide prognostic significance of whole chromosomal aber rations was maintained in this subgroup ( figure 2 )  . factors we next investigated whether the observed mole cular heterogeneity within the 91 nonwnt / nonshh medullo blastoma tumours could inform its biological basis and clinical behaviour . 
the first cytogenetic group was strongly associated with a pattern of i17q in isolation , diploid karyotypes , few recurrent whole chromosomal aberrations , and more relapses ( p = 000084 )  . 
the second cytogenetic group was char acterised by a spectrum of multiple recurrent and co incident whole chromosomal aberrations ( figure 3 ) and aneuploidy ( p < 00001 ; appendix p 13 ) , and was associated with fewer relapses . whole chromosomal aberrations within nonwnt / nonshh medulloblastoma samples were associated with improved 5year eventfree survival ( figure 4 )  . 
 55 ( 60% ) of 91 nonwnt / nonshh tumours had multiple recurrent and coincident whole chromo somal aberrations and showed favourable outcomes compared with those without whole chromosomal aberrations ( hr 016 , 95% ci 005050 ; p = 00015 ; figure 4 )  . 
 when different whole chromosomal aberration numbers were assessed , timedependent auc analysis identified 0 versus 1 or more recurrent whole chromosomal losses as the best discri minator of outcome ( figure 4 ; appendix p 14 )  . 
event - free survival per ( a ) whole chromosomal aberration cytogenetic subgroup and ( b ) recurrent whole chromosomal losses ( 0 vs 1 or more changes )  . 
the standard - risk medulloblastoma validation cohort is indicated by filled and open circles according to risk , with relationship to the schwalbe and colleagues6 and northcott and colleagues12 cohorts shown by t - distributed stochastic neighbour embedding plots . 
the median eventfree survival for these patients was 56 years ( iqr 3181 )  . the characteristics , incidence , and associated event free survival outcomes of the identified whole chromo somal aberrationdefined subgroups were recapitulated ( figure 5 ; appendix p 17 )  . 
the favourablerisk whole chromosomal aberration signature , defined by chromo some 7 gain , chromosome 8 loss , and chromo some 11 loss , was observed within multiple novel methylation subgroups , and was significantly associated with mbgroup4lowrisk 6 and group3 and group4 subtypes vi and vii12 ( p < 00001 , appendix p 18 )  . 
however , patients older than 16 years did not share this good prognosis , consistent with previous reports.15 , 23 together , these data do not support therapy deescalation in patients with wnt medulloblastoma older than 16 years of age . 
these data validate independent previous findings6 , 7 and support the eligibility of these patients for deescalated or targeted therapies ( eg , smo inhibitors ) .24 development of biomarkerdriven treatment strategies for the large remaining group of patients with nonwnt / nonshh disease represents the largest ongoing chal lenge for standardrisk medulloblastoma . 
as described in this article , nonwnt / non shh medulloblastoma tumours have few recurrent mutations , and structural chromosomal abnor malities are the most common genomic features.810 when comparing group4 and group3 tumours , we found around 90% overlap of chromosomal alterations between the two subgroups and equivalent eventfree survival . 
these tumours provide a wider biological context for the poorrisk group of patients with nonwnt disease with chromosome 17p or q defects in a diploid background ( chr17 ( im ) / diploid ( cen ) ) , previously identified by interphase fish in this cohort.15 the second group was large and defined by multiple , cooccurring whole chromosomal aber rations , common polyploidy , and improved relative outcomes . in this whole chromosomal aberration group , using multivariable eventfree survival analysis and risk modelling , we deduced a whole chromosomal aberration signature ( two or more of chromosome 7 gain , chromo some 8 loss , and chromosome 11 loss ) , which best defined patients with nonwnt / nonshh medulloblastoma with 1614 vol 19 december 2018 articles favourable prognosis . 
this whole chromosomal aberration signature was detected within a number of novel methylation subgroups within nonwnt / nonshh medulloblastoma , and associated with the lowrisk mbgroup4lowrisk , 6 and group3 and group4 subtypes vi and vii.12 by contrast , the highrisk isolated i17q diploid group was associated with highrisk mbgroup4 6 and subtype viii.12 these associations suggest highrisk common biological phenotypes and evaluation of their relative contributions to risk stratifi cation could be investigated in future clinically controlled studies . biologically and clinically significant whole chromo somal phenotypes are a notable feature of childhood malignancies other than medulloblastoma . 
characteristic patterns of nonrandom whole chromosomal aberrations in neuroblastoma ( socalled wholechromosomal changes phenotype ; more than two whole chromosomal aber rations ) 25 , 26 and high hyperdiploid acute lymphoblastic leukaemia ( socalled highhyperdiploidy phenotype [ heh ] ; 5165 chromosomes ) 27 define tumour subgroups with favourable prognoses . 
additionally , choroid plexus papil lomas and adult infratentorial ependymomas ( posterior fossa ependymoma type b ) are characterised by multiple whole chromosomal abberations.1 overall , whole chromosomal aberration signatures are associated with a low number of single nucleotide mutations . this common involvement of whole chromosomal aberration signatures provides strong impetus to under stand the underlying molecular pathomechanisms , including errors in mitotic control , chromosome segre gation , and function of the spindle apparatus . 
although beyond the scope of this study , investigation of associated biology ( eg , geneexpression profiles , pathway involve ments , and driver events ) and the involvement of specific chromosomes ( ie , chromosomes 7 , 8 , and 11 ) , is essential to improve understanding and therapeutic targeting . 
for instance , vincristine ( a component of medulloblastoma treatment regimens ) directly targets the spindle apparatus , and the excellent whole chromosomal aberration signature associated outcomes might be explained by high sensitivity to such treatments . 
 combination of these newly defined subtypes with the favourablerisk wnt and shh medulloblastomas validated in our study redistributed around 50% of patients with standardrisk medulloblastoma into a favourablerisk group , who could benefit from reducedintensity therapies aimed at maintaining overall survival while reducing treatmentassociated toxicities and late effects . 
 we thank daniel williamson , rebecca hill , janet lindsey , and simon bailey for their participation in editing of the manuscript . for highlights from asco 2018 see news page 865 for a study on sex differences in immunotherapy responses see articles lancet oncol 2018 ; 19 : 73746 for the study on the effects of antibiotics use during immunotherapy see proc am soc clin oncol 2018 ; 36 ( suppl 15 ) : 3010 for a viewpoint on pulmonary toxicity in cancer immunotherapy see lancet respir med 2018 ; 6 : 47278 for the report of rapid progression of acute adult t - cell leukaemialymphoma see n engl j med 2018 ; 378 : 194748 immunotherapy : hype and hope as the dust settles after a busy week at the 2018 american society of clinical oncology ( asco ) annual meeting ( june 15 , 2018 ; chicago , il , usa ) , there is an opportunity to reflect on the impact of the largest cancer congress of the year . 
among this years highlights were a predictive 21 - gene expression assay that suggests most women with early - stage breast cancer might not need chemotherapy , and findings that pre - operative chemoradiotherapy improves disease - free survival for patients with pancreatic cancer . 
 the most visible recipient of media scrutiny was an account of adoptive transfer of autologous tumourinfiltrating lymphocytes ( targeting somatic mutations ) , which was reported to result in a complete durable regression in a patient with advanced breast cancer with liver metastases , and thus was hailed as a miracle cure by some media outlets , garnering worldwide publicity . 
 equally well - covered was the phase 3 keynote - 042 trial , which showed pembrolizumab was more effective than chemotherapy as a first - line treatment for patients with non - small - cell lung cancer . 
equally , a retrospective study presented at asco 2018 found antibiotic use during treatment with checkpoint inhibitors reduced overall and progression - free survival in patients with advanced cancer , potentially due to changes in microbiota , implicating other important unknown factors in the host response to treatment . 
individual patient immunity undoubtedly leads to variation , but outcomes from a proportion of responders and super - responders can dominate top - line data , potentially masking many other patients with less striking results . 
this individual variance is also reflected in the failed attempts to find and validate predictive markers of response to immunotherapy : pd - 1 or pd - l1 expression , for example , does not seem to correlate with response , despite earlier data suggesting these markers were key targets for checkpoint inhibitors , highlighting just how little we understand the true complexity of the immune system and the mechanisms of action of immunotherapy . 
 cancer immunotherapy has been reported to result immune - related adverse events such as in various opportunistic infection or pulmonary toxicity and , unexpectedly , the rapid progression of disease , such as acute adult t - cell leukaemialymphoma , as well as an array of other side - effects not typically encountered with conventional chemotherapy . 
in view of the varied mechanisms of action , the specific adverse sequelae associated with these drugs warrant further investigation , especially since they are now being used in many disease settings without long - term follow - up data . 
although there is great promise in immunotherapies , we must not let the excitement of such treatments overshadow their potential for har clinicians , researchers , and patients must be wary of the hyperbole associated with certain limitations professionally marketed studies , and the of off - label use of new drugs . 
when the associated media coverage of therapies gives patients unrealistic expectations of outcomes , it is increasingly difficult for clinicians to deny immunotherapy , particularly as a last hope for those patients for whom other treatments have failed ; however , caution must be exercised , with first do no harm being central in decision - making . 
 how can we ensure that hype and promotion do not overshadow the real work at the heart of these large congresses ? it is easy to get swept away by stories of miracle cures and the expanse of shiny stands in the indeed , commercial companies exhibition halls . 
 and some institutionsexcel in the promotion of results of individual drugs or techniques , but the research community must continue to design rigorous investigations that ensure the highest level of reliable , high - quality evidence is generated to inform evidencebased cancer treatment that improves care for all patients , not just specifically selected super - responders . 
 the lancet oncology vol 19 july 2018 editorial editorial for the cancer research uk commission on the health of nhs cancer services see default / les / measuring_up_ health_of_nhs_cancer_services_ sept2014.pdf emotion - based medicine or evidence - based medicine ? the uk national institute for health and care excellence ( nice ) is once again under the microscope because of recent recommendations for various cancer drugs . 
nab - paclitaxel for metastatic pancreatic cancer ( sept 8 , 2014 ) ; trastuzumab emtansine for her2positive breast cancer ( aug 7 , 2014 ) ; and abiraterone for metastatic , hormone - resistant prostate cancer ( aug 14 , 2014 ) have all been rejected on the grounds of insu cient cost - e ectiveness . 
unfortunately , a report commissioned by cancer research uk ( cruk ) published on sept 8 , 2014 , concluded that cancer care by the national health service ( nhs ) in england is at breaking point . 
further reports on sept 16 , 2014 , stated more than half of all hospitals are in de cit and the nhs will end the year with almost 1 billion of debt , adding yet more emotion to the debate surrounding nice decisions . predictably , in response to the criticism of nice , the uks health secretary , jeremy hunt , has engaged in gesture politics . 
on aug 27 , 2014 , hunt ordered a review of the system by which nice approves cancer drugs , and announced an increase in the cancer drugs fund from 200 million to 280 million . 
cancer charities and patient groups have responded positively , but warn that this is a temporary x to a systemic problem in need of major reform to enable long - term sustainability . 
 furthermore , while nice decisions are undermined by the cancer drugs fund in england , their decisions are undone elsewhere in the uk too ; for example , the welsh medicines strategy group has approved nab - paclitaxel for use in wales , creating more fragmentation and further disparities in the level of care available across the uk , the very thing nice was created to eradicate . but , is nice really broken ? and are current circumstances really creating a second - rate cancer service in nhs england , as suggested by the manipulative and emotive language of the mainstream media ? there are no easy answers to these questions . 
on july 22 , 2014 , the institute approved two expensive cancer drugs : ipilimumab for rst - line treatment of advanced malignant melanoma and enzalutamide for progressive prostate cancer . 
 furthermore , the cruk commission shows that , in spite of a 50% increase in the number of cancer referrals from general practitioners in the past 4 years , the health service has managed this substantial increase in cases remarkably wellsurvival is at record highs , and nine out of ten patients say the care they receive is excellent or very good . 
in june , 2014 , a report by the us - based commonwealth fund comparing us health care with that in ten other countries concluded that the uk ranked rst for quality , access , and e ciency of care , and second for health - care equity . 
the uk is also not the only country to restrict access to new medicines on the basis of costeven in the usa increasing numbers of payers are excluding drugs from their formularies for similar reasons ( but without equitable cost - e ectiveness criteria )  . current criticisms of nice and nhs england need to be kept in perspective . 
while it is fair to question whether the qalys used by the institute to determine coste ectiveness are aligned with present - day expectations , it is equally important to recognise the regulator is not fully responsible for the current situation , that nices recommendations are informed by costs and data outside of its control , and that health - care equity can only be achieved by use of consistent algorithms . 
 equally , although the recommendations made by the cruk commission to ensure future sustainability of nhs cancer services are very reasonable given recent reforms , the drive to deliver greater e ciencies in the nhs are also rational . 
 similar counterpoints can be made for all other vested interests in this debate too , but , ultimately rather than point - scoring and in ghting , all parties should work together to deliver the best possible care within the constraints of a world that will , unfortunately , never o er a utopian solution . 
 the lancet oncology vol 15 october 2014 1177 corrections correction to lancet oncol 2014 ; 15 : 856 correction to lancet oncol 2015 ; 16 : 60 , 61 ledermann j , harter p , gourley c , et al . 
lancet oncol 2014 ; 15 : 85261 in this article , the second sentence of the rst paragraph of the results section should read on the basis local germline brca mutation testing reported on case report forms , germline brca mutation status was known for 98 ( 37% ) of 265 patients ( 50 [ 37% ] of 136 in the olaparib group vs 48 [ 37% ] of 129 in the placebo group )  . 
this correction has been made to the online version as of march 30 , 2015 . a multi - centre , topp ms , gckbuget n , stein as , et al . 
lancet oncol 2015 ; 16 : 5766in table 2 of this article , the mrd response during rst two cycles in patients with cr or crh row should not have been indented , and should have been the last row in the table . 
these corrections have been made to the online version as of march 30 , 2015 . after vol 16 april 2015 e158 correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
 this correction has been made to the online version as of jan 31 , 2018 . vol 19 february 2018 corrections comment published online december 11 , 2014 s1470 - 2045 ( 14 ) 71184 - 2 see articles page 67 short duration of e ect . 
several factors should be considered for this approach , including the likelihood of achieving remission , organ toxic e ects , and the time needed to screen , enroll , and treat patients before sct . 
cytokine - release syndrome in patients with b - cell chronic lymphocytic leukemia and high lymphocyte counts after treatment with an anti - cd20 monoclonal antibody ( rituximab , idec - c2b8 )  . 
exp cell res 2011 ; 317 : 125560 . ibis - i tamoxifen update : maturity brings questions the international breast cancer intervention study ( ibis - i ) is a randomised , placebo - controlled chemoprevention clinical trial of the e ects of tamoxifen in a population of women at high risk of developing breast cancer . 
the achievement of such long - term follow - up ( median 16 years ) , especially with more than 74% of participants remaining masked to randomisation , is commendable . an ongoing reduction in the incidence of oestrogen receptor - positive breast cancer through 16 years cumulative median follow - up after 5 years of tamoxifen use results in a very favourable number needed to treat of only 22 ( 95% ci 1926 ) women receiving tamoxifen for 5 years to prevent one case of breast cancer in the next 20 years . 
the ndings have clinical implications because many women could be spared the psychological and physical problems associated with a breast cancer diagnosis and related treatment.2 the results build on those from eight other selective oestrogen receptor modulator chemoprevention trials that showed a reduction in breast cancer risk through 10 years followup.3 however , the slightly higher number of deaths from breast cancer in the tamoxifen group than in the placebo group , which persisted beyond 10 years followup in ibis - i , raises a series of questions . in cuzick and colleagues ibis - i update , 99 fewer breast cancers occurred in the tamoxifen group than in the placebo group ( 251 [ 7% ] in 3579 vs 350 [ 10% ] in 3575 respectively ; hazard ratio [ hr ] 071 [ 95% ci 060083 ] , p < 00001 ) , but surprisingly , there were ve more deaths from breast cancer in the tamoxifen group than in the placebo group ( 31 vs 26 ; odds ratio 119 [ 95% ci 068210 ] , p = 08 )  . 
after 10 years followup , the discordance between the e ect of tamoxifen on breast cancer incidence and deaths from breast cancer was more pronounced ( 18 deaths in the tamoxifen group vs nine with placebo ; odds ratio 200 [ 95% ci 085506 ] , p = 008 ] ) , although it is important to note that this was not signi cantly di erent . 
since endocrine therapy is less e ective in oestrogen receptor - positive , her2positive advanced breast cancer4 than in oestrogen receptor - positive , her2 - negative disease , could a di erential distribution of her2 - positive cases , under the in uence of tamoxifen therapy , have a ected the breast cancer survival ndings ? this important issue needs to be addressed . the ibis - i ndings contrast with those from tamoxifen use in the adjuvant setting where , in women with earlystage oestrogen receptor - positive disease , at 15 years of follow - up after 5 years of tamoxifen use , congruence was recorded between tamoxifens e ect on breast cancer recurrence ( relative risk [ rr ] 053 [ se 003 ] ) and on deaths from the disease ( rr 071 [ se 005 ] ) .5 even in a trial that enrolled and randomly assigned 7154 women , the ndings about deaths from breast cancer could represent the e ect of chance alone in the small sample of 57 deaths that occurred . 
in this regard , although the authors1 cite previous power calculations to indicate that more survival events are needed before de nitive assessment , additional events would be unlikely to appreciably change the results since the trend is in the opposite direction and survival curves that cross are unlikely to become positive . 
although the magnitude and even the existence of breast cancer overdiagnosis by screening remains controversial , 6 , 7 could tamoxifen treatment in ibis - i have been selectively preventing breast cancers with extremely favourable prognoses ? additional follow - up of the other selective oestrogen receptor modulator prevention trials might address this issue . in ibis - i , tamoxifen was less e ective in reducing breast cancer risk in women who used menopausal hormone therapy than in those who did not use hormone therapy.1 menopausal hormone therapy8 and tamoxifen3 , 5 can both a ect breast cancer and other chronic diseases , and their combined e ect on most of these illness is unknown . 
in the womens health initiative randomised trials , oestrogen plus progestin , in the form of conjugated equine oestrogen , increases breast cancer incidence and deaths from breast cancer , reduces breast cancer whereas oestrogen alone overall survival is a reasonable endpoint for advanced breast cancer and adjuvant trials . 
in prevention trials that incorporate analyses after long - term follow - up , an increasingly larger proportion of deaths from other causes occur , years or decades after interventions are stopped . 
 alternative endpoints should be considered for future chemoprevention trials , especially for those that enrol older participants similar to those entered in ibis - i . at present , despite positive ndings in terms of their e ect on breast cancer incidence , the use of selective oestrogen receptor modulators for breast cancer chemoprevention in clinical practice is very infrequent.10 the discordance between tamoxifens e ects on breast cancer incidence and outcome noted in the ibis - i update could merely represent the e ects of chance alone , or alternatively might indicate that tamoxifen mainly decreases the incidence of cancers with a very favourable cancers with unfavourable prognosis , outcomes , or both . 
 lancet 2011 ; 378 : 77184 . vol 16 january 2015 comment published online december 11 , 2014 s1470 - 2045 ( 14 ) 71187 - 8 see articles page 76 bleyer a , welch hg . 
 breast cancer res treat 2012 ; 134 : 87580 . towards e ective adjuvant treatment for urothelial cancer data for the e cacy of adjuvant chemotherapy in urothelial cancer comes from prematurely closed trials with poor accrual that have not yielded de nitive conclusions about bene t . 
in the lancet oncology , cora sternberg and colleagues1 report the results of the eortc 30994 trial , which compared immediate versus deferred cisplatinradical based cystectomy in patients with urothelial carcinoma of the bladder . 
they found no signi cant di erence in the studys primary endpoint of overall survival between immediate and deferred chemotherapy ( hazard ratio [ hr ] 078 , adjusted 95% ci 056108 ; p = 013 ) , but immediate chemotherapy did signi cantly increase 5 - year progression - free survival ( hr 054 , 95% ci 04073 ; p < 00001 )  . 
 chemotherapy after combination some might argue against the relevance of this study , since neoadjuvant chemotherapy with methotrexate , vinblastine , doxorubicin , and cisplatin ( mvac ) is the proven standard for the treatment of muscle - invasive bladder cancer.2 although these recommendations were made more than a decade ago , neoadjuvant inherent therapy remains highly underused . 
the toxicity associated with cisplatin - based therapy in the typical urothelial cancer population of elderly and frail patients ensures that it is unlikely to be given to a substantial proportion of patients . 
therefore , recommendations about adjuvant chemotherapy will remain highly relevant either until a non - toxic curative therapy is discovered , or until the patients who truly bene t from these potentially toxic regimens can be accurately identi ed . 
 e orts to improve chemotherapy for urothelial cancer date back to the 1980s , when adjuvant cisca ( cisplatin , cyclophosphamide , and doxorubicin ) was reported to have cured a higher proportion of patients with bladder cancer than did surgery alone.3 mvac arrived soon after with compelling evidence supporting the use of this combination in patients with pathological t3b or worse disease at surgery , 4 yet insu cient numbers of patients or design aws prevented de nitive con rmation of a survival bene t . 
 additional trials of gemcitabine cisplatin have been limited by similar problems.5 including other chemotherapy combinations for urothelial cancer , those with higher doses of ifosfamide , 6 have been assessed in the perioperative setting , but have not surpassed the outcomes achieved with mvac . 
even high - dose mvac , 7 which is administered every 2 weeks , has not improved survival outcomes , although the improved toxicity pro le has supported its use . 
one potential exception is adjuvant gemcitabine , paclitaxel , and cisplatin , which was reported to improve survival in a recent abstract.8 perhaps nal results from this trial will yield the de nitive conclusions that investigators seek . results of sternberg and colleagues study1 suggest that adjuvant chemotherapy might bene t patients with node - negative disease . 
 clearly , additional studies are needed to con rm this nding . in view of the absence of de nitive success with this trial , and admittedly most other trials of adjuvant chemotherapy for bladder cancer reported so far , it seems unlikely that using a similar framework to design vol 16 january 2015 changing geographical patterns and trends in cancer incidence in children and adolescents in europe , 19912010 ( automated childhood cancer information system ) : a population - based study eva steliarova - foucher , miranda m fidler , murielle colombet , brigitte lacour , peter kaatsch , marion pieros , isabelle soerjomataram , freddie bray , jan willem coebergh , rafael peris - bonet , charles a stiller , on behalf of the accis contributors * summary background a deceleration in the increase in cancer incidence in children and adolescents has been reported in several national and regional studies in europe . 
based on a large database representing 13 billion person - years over the period 19912010 , we provide a consolidated report on cancer incidence trends at ages 019 years . methods we invited all population - based cancer registries operating in european countries to participate in this population - based registry study . 
we requested a listing of individual records of cancer cases , including sex , age , date of birth , date of cancer diagnosis , tumour sequence number , primary site , morphology , behaviour , and the most valid basis of diagnosis . 
we also requested population counts in each calendar year by sex and age for the registration area , from official national sources , and specific information about the covered area and registration practices . 
 incidence rates and the average annual percentage change with 95% cis were reported for all cancers and major diagnostic groups , by region and overall , separately for children ( age 014 years ) and adolescents ( age 1519 years )  . 
 we examined and quantified the stability of the trends with joinpoint analyses . findings for the years 19912010 , 53 registries in 19 countries contributed a total of 180 335 unique cases . 
we excluded 15 162 ( 84% ) of 180 335 cases due to differing practices of registration , and considered the quality indicators for the 165 173 cases included to be satisfactory . 
the average annual age - standardised incidence was 1375 ( 95% ci 13671383 ) per million person - years and incidence increased significantly by 054% ( 044065 ) per year in children ( age 014 years ) with no change in trend . 
in adolescents , the combined european incidence was 1762 ( 17441780 ) per million person - years based on all 35 138 eligible cases and increased significantly by 096% ( 073119 ) per year , although recent changes in rates among adolescents suggest a deceleration in this increasing trend . 
the combined age - standardised incidence of leukaemia based on 48 458 cases in children was 469 ( 465473 ) per million person - years and increased significantly by 066% ( 048084 ) per year . 
the average overall incidence of leukaemia in adolescents was 236 ( 229243 ) per million person - years , based on 4702 cases , and the average annual change was 093% ( 049137 )  . 
this notice should be preserved along with the articles original url . introduction cancer is an important disease burden in children as it is not easily prevented , with known causes explaining only a small proportion of cases . 
evidence from retrieved studies suggested that after a substantial increase in childhood cancer incidence towards the end of the last century , the rate of increase has declined in the 2000s . 
however , the limitations of most of these studies , in terms of number of cases or timeframe , might have hampered the full understanding of the dynamisms behind the observed trends in this population . added value of this study we used all quality data available in europe for the full calendar years in the period 19912010 to evaluate incidence patterns and trends in children and adolescents . 
based on the large scale of all available european data , our findings add an authoritative account on the geographical patterns and temporal trends of cancer in children and adolescents in europe . 
 implications of all the available evidence the increasing trends might have resulted from improvements in cancer diagnosis or registration in this age group , although the influence of other factors cannot be excluded . 
the paucity of evidence of stabilisation of cancer incidence in europe and the variability of the observed trends support the need for continued international monitoring and research into causal mechanisms . the past three decades , incidence increased by about 1% per annum for all cancers combined and this increase affected most major diagnostic groups , including leukaemias , lymphomas , and cns tumours.2 however , in the past decade , incidence appears to have stabilised overall and for the major diagnostic groups in european populations.310 leukaemias , lymphomas , and tumours of the cns represent 70% of all cancers observed in european populations younger than 15 years and half of all cancers in those aged 1519 years1 and therefore contribute considerably to the overall incidence . 
 monitoring these trends is important for planning health - care delivery and for aetiological research . in this study , we documented and interpreted incidence trends in europe for cancers diagnosed at ages 019 years using quality - assured population - based cancer registries . 
 we focused on the 20 - year period 19912010 , assessing the trends separately in children ( aged 014 years ) and adolescents ( aged 1519 years ) , for all cancers combined and for the major diagnostic groups . 
our results update the automated childhood cancer information system ( accis ) studies , extending the previously reported period of observation by over a decade.2 , 11 methods data acquisition invited all population - based cancer registries operating in european countries ( as defined by the un statistics division12 ) and cyprus to participate in this population - based registry study . 
we requested a listing of individual records of cancer cases , and the population in each calendar year by sex and age from official national sources , accompanied by specific information about the geographical and administrative area covered and registration practices . information on cancer cases included coded data on sex , age , date of birth , date of diagnosis , tumour sequence number , primary site , morphology , behaviour , and the most valid basis of diagnosis . 
most registries coded tumours according to the international classification of diseases for oncology , third edition ( icd - o - 313 ) as required , and international classification of diseases for oncology , second edition14 codes were converted to icd - o - 3 codes . 
subsequently , neoplasms were classified according to the international classification of childhood cancer , third edition ( iccc - 3 ) .15 we examined individual records for internal consistency , 16 verifying unlikely combinations of site with morphology , age or sex with tumour type , basis of diagnosis with morphology , and rare tumour entities . 
standardised tables , charts , statistics , lists of selected questioned records , and any relevant information provided by the registry or known from published sources were discussed at meetings of the accis scientific committee , who decided on the inclusion of each dataset in the accis database . 
only datasets with high - quality data were eligible for inclusion in the analyses . the cancers included in the analyses were all malignant tumours diagnosed during the complete calendar years 19912010 , in people younger than 20 years and resident in the contributing registration areas . 
several cancer types were excluded because they were not eligible for registration in all participating registries or during the whole study period : myelodysplasias ( icd - o - 3 m - codes starting with 998 ) , pilocytic astrocytoma ( icd - o - 3 code for more on accis see 1160 vol 19 september 2018 articles m - 9421 ) , non - melanoma skin cancer ( iccc - 3 subgroup xie and xiib with site code c44 ) , and carcinoid tumour of the appendix ( icd - o - 3 site code c18.1 and m - 8240 )  . the data used in this study were submitted and validated during the years 201516 . 
our study design was reviewed and approved by the international agency for research on cancer ( iarc ) ethics committee on june 17 , 2015 . dataset constitution an eligible registry could become a contributor if it provided quality data for all complete calendar years in the 20 - year period 19912010 . 
the paediatric registries collected and provided data for those aged 014 years , and the other cancer registries and the paediatric registry of belarus provided data for the full target age range ( 019 years )  . 
the french national paediatric registry registered haematological malignancies only . some populations in france , germany , italy , spain , switzerland , and the uk were covered by both paediatric and general cancer registries . 
to avoid double counting of cases in two registries while using the maximum number of cases for analyses in these populations , we allocated each registry to one or more datasets ( appendix p 2 )  . 
we built three datasetsone with 39 registries contributing to the analyses of all cancers , cns tumours , and other tumours in ages 014 years , a second with 32 registries contributing to the analyses of leukaemia and lymphoma in ages 014 years , and a third with 45 registries contributing to all the analyses of those aged 1519 years . 
 the first and second datasets ( ages 014 years ) differed only in the contribution from france ; the analyses of all cancers and cns tumours used a dataset that included data from the french general cancer registries , while the leukaemia and lymphoma dataset included data from the french national paediatric registry of haematological malignancies . 
the french national registry increased the person - years by ten times and provided 11 770 more haematological malignancies the combined contribution of the french regional registries . compared with subnational numbers of cases and person - years were pooled to produce national cancer incidence and countries were further pooled into four european regions ( appendix p 2 ) according to un definitions.12 the person - years available in each region are shown in the appendix ( p 3 )  . statistical analysis the number of incident cases in the covered areas of the participating registries during the study period determined our sample size . 
incidence was calculated as the number of cases divided by the number of person - years in the categories of geographical area , sex , age , and diagnostic group for the given 20 - year period and expressed per million person - years . 
as the age distribution of population at risk differs between countries and over time , we adjusted the reported incidence for the age range 014 years vol 19 september 2018 1161 articles a east overall average annual percentage change ( 95% cl ) 050 ( 021079 ) belarus bulgaria czech republic hungary poland overall b north overall average annual percentage change ( 95% cl ) 040 ( 016064 ) estonia iceland norway sweden overall c south overall average annual percentage change ( 95% cl ) 040 ( 007072 ) italy portugal slovenia spain overall d west overall average annual percentage change ( 95% cl ) 070 ( 052088 ) austria france germany netherlands switzerland overall 1990 1995 2000 calendar year 2005 2010 1990 1995 2005 2010 2000 calendar year figure 1 : incidence trends of cancer in children aged 014 years in europe , 19912010 jagged thin lines indicate annual age - standardised rates in countries and smooth red thick lines indicate modelled incidence trends in regions . for age via direct standardisation using weights 12 , 10 , and 9 for the three age groups 04 years , 59 years , and 1014 years , respectively.17 we also calculated 95% cis . 
 as each combination of calendar year , sex , and age group had a positive person - years count , we encountered no missing data . to graphically portray incidence trends for all cancers , we plotted observed incidence against calendar year for each country , and the rates for the four european regions were smoothed using a locally weighted regression18 of the incidence on year . to assess the average annual percentage change , we fit the natural logarithm of the incidence with year using generalised linear regression models adjusting for age group and region , as appropriate . 
we examined incidence trends for changes during the study period using joinpoint regression program ( version 4.1.0 ) applied to the log rates , separately for the age groups 014 years and 1519 years in the total dataset , and in each cancer category , overall and by region . 
where joinpoints were detected , we reported the annual percentage change with corresponding 95% cis for each of the linear segments identified between two significant joinpoints . role of the funding source the funders of the study external to the collaborating institutions had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had final responsibility for the decision to submit for publication . results during the full calendar years of the period 19912010 , the 53 registries contributed 13 billion person - years and 180 335 unique cases . 
in 2010 , the available population at risk represented 532 million ( 466% ) of 1141 million of the european population aged 014 years and 98 million ( 226% ) of 432 million aged 1519 years , with reference to un population estimates.20 in western europe , coverage of the childhood population was almost complete for haematological malignancies ( 279 million [ 933% ] of 299 million ) , and 175 million ( 585% ) of 299 million were covered for the other malignancies , while 21 million ( 201% ) of 106 million adolescents were covered ( appendix p 3 )  . we included all 118 265 eligible cases in patients aged 014 years in our analyses of incidence of all cancers . 
 vol 19 september 2018 1163 articles incidence the average annual age - standardised incidence was 1375 ( 95% ci 13671383 ) per million person - years and increased significantly by 054% ( 044065 ) per year on average ( table 1 ) , with no break in the time trend . 
the large fluctuation of annual incidence in iceland was due to small population size and did not visibly affect the shape of the regional curve ( figure 1 )  . 
the trend in the east was split into two segments , both with nonsignificant trends ( figure 2 )  . the national for we investigated incidence for four diagnostic groups in patients aged 014 years ( table 1 , figure 2 , appendix p 4 ) , and included all eligible cases . 
the combined age - standardised incidence of leukaemia based on 48 458 cases in patients aged 014 years was 469 ( 95% ci 465473 ) per million person - years and increased by 066% ( 048084 ) per year , with no change in slope . 
the overall age - standardised incidence of lymphoma was 158 ( 156160 ) per million person - years ( based on 18 458 cases ) and varied modestly by region . 
the overall agestandardised incidence of malignant cns tumours ( 19 413 cases ) of 222 ( 95% ci 219226 ) per million person - years was observed to rise at 049% ( 020077 ) per annum with no joinpoints ; by region , we observed an increasing trend only in the west , as the rates were stable in the three other regions . in patients aged 014 years , the combined incidence of all 43 706 other cancers increased in europe overall and in all regions except the north . 
in joinpoint analysis , the european trend increased only over the first few years , similar to the trend in the west ( figure 2 )  . in adolescents ( aged 1519 years ) , the combined european incidence was 1762 ( 95% ci 17441780 ) per million person - years based on all 35 138 eligible cases and incidence increased by 096% ( 95% ci 073119 ) per year in the period 19912010 ( table 2 ) , although no significant change in trend was seen in the second decade ( figure 3 )  . 
in addition to large variations due to small numbers of cases for some countries , we observed a large range in incidence ( between around 140 and 240 per million person - years ) for belarus . 
in the east , a decrease was noted over the time segment 19992008 ( figure 3 )  . for adolescents , the overall incidence of leukaemia was 236 ( 95% ci 229243 ) per million person - years ( based on all 4702 eligible cases ) and varied little between regions ( table 2 )  . 
lymphoma ( 9446 cases ) occurred more frequently than did leukaemia ( 4702 cases ) or malignant cns tumours ( 2983 cases ) in adolescents compared with children ( table 2 ) , and the overall incidence of 474 ( 464483 ) per million person - years varied moderately by region . 
changes in this trend were detected in the east and west , where the increase was limited to the second and first half of the study period , respectively ( figure 3 )  . 
incidence was stable overall and in the four defined regions ( figure 3 ) , with no change in the slopes . the overall rate for all other cancers in adolescents ( 18 007 cases ) was 903 per million . 
the pattern of changes in the slopes by region was similar to that observed for all cancers ( figure 3 )  . discussion in this population - based registry study , we reported on cancer incidence trends in the european population of children ( aged 014 years ) and adolescents ( aged 1519 years ) during the full calendar years 19912010 , thus extending the accis study by 10132 , 11 years of observation . 
the overall incidence for children and adolescents increased significantly over this 20 - year period . the increase in incidence was not constant by cancer type , region , or over time , and there was a suggestion of stabilisation in the trend for all cancers in adolescents in the dataset for the whole of europe ( appendix p 6 )  . 
 the most pronounced inter - regional diversities included the decreasing incidence of childhood lymphomas in the east ( compared with stable or increasing incidence in the other regions ) , an increase in the incidence of childhood cns tumours in the west ( compared with little change observed in the other regions ) , and the stable incidence of leukaemia in adolescents in the north ( relative to increasing incidence in the other regions )  . vol 19 september 2018 1165 articles a east b north overall average annual percentage change ( 95% cl ) 123 ( 062184 ) belarus bulgaria czech republic poland overall overall average annual percentage change ( 95% cl ) 062 ( 028096 ) estonia iceland norway sweden overall 1990 c south 1995 2000 2005 2010 1990 1995 2000 2005 2010 overall average annual percentage change ( 95% cl ) 178 ( 136220 ) italy portugal slovenia spain overall d west overall average annual percentage change ( 95% cl ) 108 ( 072143 ) austria france germany netherlands switzerland overall 1990 1995 2000 2005 2010 1990 1995 2000 2005 2010 calendar year calendar year figure 4 : incidence trends of cancer in adolescents aged 1519 years in europe , 19912010 jagged thin lines indicate annual age - specific rates in countries and smooth thick red lines indicate modelled incidence trends in regions . although our results are largely confirmatory and incremental from previous findings , a major strength of our study is its large size , which permits detection of a moderate rate of increase of 05% per year in the age group 014 years . 
data from large paediatric cancer registries helped to increase the coverage and creation of a specific dataset for childhood haematological malignancies enlarged the relevant person - years in the west ( 5838 million ) by 53% compared with data available for other neoplasms ( 3805 million )  . 
we examined the trends separately in children and adolescents to allow for variations in trends between these populations with a different case mix . 1166 vol 19 september 2018 articles we validated the quality and completeness of the data from the included registries during a thorough dataset assessment . 
we consider our results to provide the best available estimates of incidence trends in the european population of children and adolescents for 19912010 . a limitation of our study is the variable coverage of the regions , which might affect the representativeness of the incidence at the national and european regional levels . 
the available data do not allow speculation on what the incidence would be if coverage was complete increase of coverage and quality of registration is required for a full picture of the cancer burden . 
 meanwhile , by use of all quality information available for the study period , our results maximise the number of person - years of comparable data , and provide evidence of changing trends in european populations . we excluded several cancer types that are usually included in reports of childhood cancer incidence from our analyses . 
we plan to examine this assumption in a focused analysis of trends of all cns tumours , by behaviour and diagnostic subgroup , and by considering the differences and changes in coding and their reportability . our reported total incidence was 5% to 15% lower ( depending on the region ) than in another report assessing the period 200110.1 this disparity is explained by the exclusion of several groups of neoplasms from our study and the period starting one decade earlier , which would , in the presence of an increasing trend , result in a lower overall rate . the overall average annual change of 054% in children aged 014 years is lower than the 1% reported by an accis study based on diagnoses in the 1970s through to the 1990s2 or for the period 197897 , 21 and might indicate a deceleration in the increase of cancer incidence , although the registry datasets included differ somewhat between the studies . 
a lower rate of increase could suggest the end of an improvement in reporting , but might also reflect reduced reporting discipline , a change in classification of cancers , or other factors . 
cancer - specific studies might provide more precise interpretation of these trends . studies in european populations of smaller sizes reported stabilising of cancer incidence in children overall and in the three major diagnostic groups.310 by contrast , data collected in the longstanding registries of the surveillance , epidemiology , and end results ( seer ) program suggest continued minor increases in overall childhood cancer incidence over the most recently assessed period 19952014 , 22 consistent with our study . 
in adolescents aged 1519 years , varying incidence trends were observed in different european for leukaemia , populations lymphoma , or cns tumours.3 , 4 , 7 as for the seer data , 22 our study found an increase in overall cancer incidence and leukaemia and lymphoma incidence , but no change in trends for malignant cns tumours . 
we identified changes in overall trends that provide some evidence of a deceleration of time trends during the most recent years of our study , along with varying patterns across age groups , regions , and cancer types , although significant joinpoints should not be taken to imply abrupt changes in underlying trends in risk.19 the variability we found warrants continued monitoring of incidence patterns in large populations over long periods , as trends that are not significant over short intervals might result in significant increases over a longer timeframe , and grouping smaller populations with no trend could yield a significant change in a pooled dataset . 
these considerations might also explain the discrepancy in the measured rate of change between our study and smaller european datasets.310 kroll and colleagues24 have linked the increase in childhood cancer incidence in great britain with advances in diagnostic technology and improved cancer registration , because of the concurrence of a step increase in leukaemia and non - cns solid tumour incidence in 2002 with a registration plan enacted in 2001 . 
although we are not aware of similar studies in other countries , analogous effects on childhood cancer incidence cannot be excluded elsewhere in europe and could have affected our results . the gradual convergence of environmental factors , lifestyle , and health services across europe might have contributed to the similarities in incidence trends across the regions , although such changes will probably have less of an effect on cancer in childhood than in older age . 
nevertheless , some opposing trends ( notably for lymphoma in the east ) suggest caution should be taken in ascribing the slowly increasing trends exclusively to improved detection , at least before further detailed analyses by cancer type , age group , and geographical region are done . overall incidence in children is weighted towards leukaemia , which , in 75% of cases , is the precursor b - cell lymphoid leukaemia . 
with increasing social development over time , this peak shifts towards younger ages and becomes more pronounced.2 , 25 this change is unlikely to be driven by improved registration , which would affect all vol 19 september 2018 1167 articles ages in the same way . 
the deficit of lymphoid leukaemia cases seen in poorer settings can be ascribed in part to underdiagnosis , 26 , 27 but inequalities across social strata might also operate through relevant exposures , such as parental occupation , diet , or reproduction characteristics.28 continuous socioeconomic development and increasing awareness of primary care practitioners might have contributed to the observed increase in leukaemia cases , although reasons for the stabilisation of leukaemia incidence in northern europe are unclear . incidence of lymphoma was relatively high compared with incidence of leukaemia in children in eastern europe . 
furthermore , diagnosis of lymphoma might be delayed until older ages , especially if the decreasing trend in children is accompanied by an increasing trend in adolescents , as seen in the east over the second decade . 
the high incidence in southern europe is consistent with previous reports of possible environmental exposures.30 a further assessment of lymphoma trends by diagnostic subgroups , narrower age groups , and sex could help provide a more specific explanation of the observed temporal changes . the stability of malignant cns tumour incidence in adolescents is encouraging , although drawing firm conclusions should be postponed until incidence trends are examined using data that include non - malignant tumours in the populations in which these are ascertained completely to exclude the possible effect of changes in classification of tumours . 
in children , because of the shown persisting increase in incidence in malignant cns tumours , and the exclusion of non - malignant tumours specifically pilocytic astrocytomafrom our analyses , a further detailed assessment is warranted , especially considering the poor outcome for such tumours . the trends for all other cancers combined show that the overall increase in incidence is not explained solely by changes in the three major groups of childhood and adolescent cancer . 
this fact is especially relevant in adolescents , as many cases are germ cell tumours and carcinomas.1 the candidate explanatory groups for the increase in at least a part of the period are thyroid carcinoma , 31 testicular tumours , 32 and melanoma.33 in particular , the patterns for belarus are probably shaped by the pronounced increase and later waning of thyroid cancer incidence during the study period , reflecting exposure to the radioactive fallout from the chernobyl accident.34 these observations also merit detailed studies . in summary , in this study we aimed to provide an overview of cancer incidence trends in children and adolescents in europe , as an introduction to a detailed investigation of patterns and trends and their possible determinants by diagnostic group and other subcategories in a concerted series of studies . 
the diversity of trends across the regions and tumour groups warrants further monitoring and a more detailed assessment of the high - quality data collected by cancer registries , by specific tumour types and population subgroups . 
whether the observed increase in cancer incidence in children and adolescents is due to enhanced discovery of cases or changing risk factors , the known frequency of cancer in young people should be considered in cancer control programmes . 
without an accurate quantification of the possible causes of this increase , whether real or artifactual , it is prudent to continue aetiological research into the causes of cancer in children and adolescents and to explore possible preventive measures . contributors es - f , bl , pk , jwc , rp - b , and cas designed the study , and contributed to data acquisition and evaluation . 
es - f did the literature search and drafted the manuscript , which was reviewed , modified , and approved by all coauthors . declaration of interests we declare no competing interests . acknowledgments we gratefully acknowledge the cofunders of this study . 
data acquisition was partly supported by the federal ministry of health of the federal german government and the development of infrastructure relevant to this study was enabled through the eus seventh framework programme ( fp7 / 20072013 ) under grant agreement lsshct200821 9453 ( eurocourse )  . 
the required funding was completed by the international agency for research on cancer . and advisory board and consulting fees from eli lilly ; has received personal fees and held stock as a member of advisory board from seragon ; has received reimbursement for travel and in - kind items and services from roche , outside the submitted work . 
 s - ai reports grant support from astrazeneca and advisory consultant roles for astrazeneca , eisai , novartis , pfizer , roche / genentech and spectrum , outside the submitted work . 
hi reports grant support and personal fees from novartis during the conduct of the study ; hi was also an uncompensated member of the steering committee of this study ; hi has received personal fees in the form of honoraria and consulting fees from astrazeneca , pfizer , lilly , daiichi - sankyo , and f hoffman la - roche via chugai , outside the submitted work . 
jc reports personal fees from novartis , celgene , cellestia , astrazeneca , biothera pharmaceuticals , merus , seattle genetics , daiichi sankyo , erytech , pfizer , eisai , and samsung ; has received stock , patents , and intellectual property from medsir ; has received personal fees and research funding to his institution from roche , outside the submitted work . 
mdls reports personal fees in the form of speakers honoraria and advisory board honoraria from novartis , roche , lilly , pfizer , eisai , ipsen , and teva , outside the submitted work . 
cla reports personal fees for participation in a steering committee for the clinical trial from novartis , during the conduct of the study ; and personal fees for an expert advisory role from eli lilly , astrazeneca , genentech , millennium , celgene , pfizer , radius , and merck , outside the submitted work . 
sc also reports personal fees received in the form of honoraria for advisory boards from novartis , hoffmann laroche , pfizer , astrazeneca , and genomic health ; and institutional research support from novartis , hoffmann laroche , pfizer , astrazeneca , genomic health , genentech , merck , and bms , outside the submitted work . 
she also reports grant support from ambryx , amgen , bayer , obi pharma , bimarin , cascadian , daiichi sankyo , dignitana , genentech , gsk , lilly , macrogenics , medivation , merrimack , novartis , pfizer , pieris , puma , roche , seattle genetics , and travel support from lilly , novartis , and obi pharma , outside the submitted work . 
 reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
pv reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 15964 wolf a , naylor k , tam m , et al . 
these corrections have been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 17980 massari f , di nunno v . 
lancet oncol 2019 ; 20 ; 17980in this comment , the following sentence has been edited from time to deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab to risk of deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab . 
we aimed to test combined genomic and microenvironmental indices in prostate cancer to improve risk strati cation and complement clinical prognostic factors . methods we used dna - based indices alone or in combination with intra - prostatic hypoxia measurements to develop four prognostic indices in 126 low - risk to intermediate - risk patients ( toronto cohort ) who will receive image - guided radiotherapy . 
we validated these indices in two independent cohorts of 154 ( memorial sloan kettering cancer center cohort [ mskcc ] cohort ) and 117 ( cambridge cohort ) radical prostatectomy specimens from low - risk to high - risk patients . 
our primary endpoint was the development of a set of prognostic measures capable of stratifying patients for risk of biochemical relapse 5 years after primary treatment . findings biochemical relapse was associated with indices of tumour hypoxia , genomic instability , and genomic subtypes based on multivariate analyses . 
genomic instability is prognostic for relapse in both image - guided radiotherapy ( multivariate analysis hazard ratio [ hr ] 45 [ 95% ci 2198 ] ; p = 000013 ; area under the receiver operator curve [ auc ] 070 [ 95% ci 065076 ] ) and radical prostatectomy ( 40 [ 1697 ] ; p = 00024 ; auc 057 [ 052061 ] ) patients with prostate cancer , and its e ect is magni ed by intratumoral hypoxia ( 38 [ 1212 ] ; p = 0019 ; auc 067 [ 061073 ] )  . 
a novel 100 - loci dna signature accurately classi ed treatment outcome in the mskcc low - risk to intermediate - risk cohort ( multivariate analysis hr 61 [ 95% ci 2019 ] ; p = 00015 ; auc 074 [ 95% ci 065083 ] )  . 
in the independent mskcc and cambridge cohorts , this signature identi ed low - risk to high - risk patients who were most likely to fail treatment within 18 months ( combined cohorts multivariate analysis hr 29 [ 95% ci 1460 ] ; p = 00039 ; auc 068 [ 95% ci 063073 ] ) , and was better at predicting biochemical relapse than 23 previously published rna signatures . interpretation this is the rst study of cancer outcome to integrate dna - based and microenvironment - based failure indices to predict patient outcome . 
by contrast , patients with intermediate risk ( gleason scores of 7 , psa concentrations of 1020 ng / ml , or t2b - c ) and high risk or locally advanced ( gleason scores 8 , prostate speci c antigen concentrations 20 ng / ml , or t3 / 4 ) prostate cancer often undergo radical prostatectomy or image - guided radiotherapy , or receive intensi ed regimens adding adjuvant androgen deprivation therapy or novel systemic drugs to prevent progression to metastatic castration - resistant prostate cancer . 
however , use of treatment intensi cation for individual patients is imprecise : 3050% of patients have biochemical relapse despite radical prostatectomy or image - guided radiotherapy.4 , 5 furthermore , nearly 20% of intermediate - risk patients have biochemical failure within 18 months of primary local therapy ( ie , rapid failure )  . 
such failure might be be due to pre - existing occult metastatic disease , because rapid biochemical failure for prostate - cancer - speci c mortality.6 , 7 the basis of this interpatient clinical heterogeneity has not been clinically resolved.8 , 9 is a surrogate a signature to classify patients as potential responders or non - responders to local therapy would have great clinical use if it was treatment - independent ( ie , e ective both for patients undergoing radical prostatectomy or image - guided radiotherapy ) and could be done on initial diagnostic biopsies . 
such a signature could triage patients at greatest risk of failure into clinical trials for treatment intensi cation and justify potential added toxic e ects.7 , 10 dna copy number alterations in pten , nkx3 - 1 , myc , and star are associated with adverse prognosis , 11 , 12 and rna - based gene signatures might di erentiate indolent and non - indolent , lethal prostate cancer.13 - 15 tmprss2erg fusion status does not predict prognosis after radical prostatectomy or image - guided radiotherapy.16 , 17 importantly , tumour cells exist within a heterogeneous tumour microenvironment with dynamic gradients of hypoxia that have been linked to metastatic potential.9 , 18 indeed , patients with prostate cancer with hypoxic tumours rapidly fail treatment ( eg , within 2 years ) after radical prostatectomy or image - guided radiotherapy.19 , 20 up to now , the interplay of genomic instability and tumour microenvironment in modulation of treatment outcome has been unexplored . 
we therefore aimed to develop clinically relevant prognostic indices , with and microenvironmental indices , to robustly predict patient outcome . tumour dna integrated use signatures methods study design and patients our training ( toronto ) cohort for generation of biopsyconsisted of pre - image - guided based radiotherapy , clinically - staged patients with prostate cancer , who were classi ed as low - risk or intermediaterisk on the basis of national comprehensive cancer network guidelines ( appendix ) .3 to validate our ndings , we used copy number alteration pro les from two cohorts of clinically staged ( ie , similar to pre - imageguided radiotherapy patients ) low - risk to high - risk radical prostatectomy patients ( memorial sloan kettering cancer center cohort [ mskcc ] and cambridge cohorts ; appendix ) .8 the radical prostatectomy cohorts were considered both separately and together . 
second , we used the percentage of a patients genome harbouring copy number alterations ( percent genome alteration ) as a surrogate for genomic instability , and assessed this proportion together with tumour hypoxia . 
third , we undertook supervised machine learning with a random forest21 to develop a statistical model , resulting in a dna signature , which classi ed patients at risk of biochemical relapse on the basis of their copy - number pro les . 
we compared the resulting signature with published rnabased signatures . for and , increase ( de ned as an radiotherapy patients statistical analysis our main aim was the development of a set of prognostic measures capable of stratifying patients for risk of biochemical relapse concentration of prostate - speci c antigen of at least 2 ng / ml above the post - radiation nadir value for imageguided radical prostatectomy patients , as two consecutive concentration values > 02 ng / ml or triggered salvage radiotherapy22 , 23 ) 5 years after primary treatment . 
we modelled indices with univariate and multivariate analyses , with multivariate analyses correcting for gleason score and pre - treatment concentrations of psa ( and clinical t stage during assessment of high - risk patients ; appendix )  . 
all authors had full access to all the data in the study and the corresponding author had nal responsibility for the decision to submit for publication . results we used information derived from 126 pre - imageguided radiotherapy biopsies ( toronto cohort ) and did initial validation with 154 radical prostatectomy specimens ( mskcc cohort )  . 
we focused on clinically - matched validation cohorts containing intermediate - risk patients ( n = 210 ) who might need treatment intensi cation beyond local therapy alone , but also considered all patients with localised disease who might be candidates for intensi cation or de - intensi cation ( full validation cohort n = 271 )  . 
pretreatment psa was prognostic in imageguided radiotherapy patients , whereas pretreatment gleason score , t category , and psa were all prognostic in the full mskcc and cambridge cohorts ( table 1 )  . low - risk and our initial analyses showed that toronto and mskcc cohorts showed extensive genomic heterogeneity , even for patients who were low - risk or intermediate - risk , or had gleason scores of 6 or 7 ( appendix pp 13 , 4043 )  . 
the most recurrent copy number alterations in either cohort were 8p ampli cations and 8q deletions , in addition to deletions of 16q232 and 6q15 ( harbouring maf and map3k7 ; table 2 ) , which have been noted in aggressive tumours.24 we established the frequency of copy number alterations for a set of genes putatively prognostic for adverse outcomes , selected from our previous studies and image - guided radiotherapy biopsies ( appendix p 44 )  . 
we noted this variability across the genome , suggesting that genomically de ned subtypes of prostate cancer might be obtained from biopsies . the toronto literature , the unbiased hierarchical clustering in the toronto cohort ( appendix pp 4546 ) showed four localised prostate cancer subtypes with distinct genomic pro les : subtype 1 ( characterised by gain of chromosome 7 ) , subtype 2 ( deletion of 8p and gain of 8q ) , subtype 3 ( loss of 8p and 16q ) , and subtype 4 ( so - called quiet genomes due to few genomic alterations )  . 
for the toronto - igrt cohort , in which there were only low - risk to intermediate - risk patients , we compared t2t1 patients , whereas for the radical prostatectomy cohorts , we compared t3 patients with t12 patients . 
data are provided for dichotomised and continuous pga in each cohort , on the basis of cox proportional hazard models including only the marker of interest ( univariate ) and models including relevant clinical covariates as shown in the table ( multivariate )  . 
 * genes with most copy number alterations or those with known or putative cancer associations . table 2 : most recurrently aberrant regions | || | ||| || || || || | || || | | || || |||||| | | | || || || subtype 1 subtype 2 subtype 3 subtype 4 number at risk subtype 1 subtype 2 subtype 3 subtype 4 log - rank p < 00001 time ( years ) figure 1 : kaplan - meier analysis of biochemical - relapse free survival for patients strati ed by tumour subtype subtype 2 and 16q deletion in subtype 3 ( appendix p 14 )  . 
 all four subtypes were con rmed in the mskcc radical prostatectomy cohort and were not associated with tmprss2erg fusion , gleason score , or t category ( appendix pp 1517 , 4748 )  . in a pooled analysis of low - risk and intermediate - risk patients ( using the toronto and mskcc cohorts ; 250 patients ) , the four genomic subtypes of localised prostate cancer had signi cantly di erent prognoses , even after adjustment for clinical variables ( gure 1 , appendix pp 1519 , 4349 )  . 
biochemical relapse - free survival at 5 years was 58% ( 95% ci 3792 ) for subtype 1 , 55% ( 3781 ) for subtype 2 , 53% ( 3778 ) for subtype 3 , and 89% ( 8494 ) for subtype 4 . 
with the percentage of the genome showing a copy number alteration as a proxy for genomic instability , we noted interpatient variability in percentage of genome alteration ranging from 052% in the toronto cohort , to 034% in the mskcc cohort , and 028% in the cambridge cohort . 
indeed , individual gleason score - 6 tumours had a higher percentage of genome alteration than did some gleason score 4 + 3 tumours ( gure 2a ) , suggesting that percentage of genome alteration re nes biological description even in tumours of mainly pattern 4 . 
as expected , based on previous ndings , the percentage of genome alteration was increased in patients with prognostic chd1 deletions ( appendix p 50 ) .25 percentage of genome alteration was strongly prognostic , independent of clinical covariates , as previously reported.26 every 1% increase in percentage of alteration led to a 58% decrease in 5 - year biochemical relapse - free survival ( c - index 060072 ; appendix pp 2021 )  . 
to classify the likelihood of clinical failure on the basis of percentage of genome alteration , we set the upper tertile of 749% from the toronto cohort as the lower bound threshold , which e ciently strati ed patients who underwent either image - guided radiotherapy ( multivariate analysis hr for biochemical relapse 45 [ 95% ci 2198 ] ; wald p = 000013 ) or radical prostatectomy ( eg , pooled radical prostatectomy low - risk to intermediate - risk cohort : multivariate analysis hr for biochemical relapse 40 [ 1697 ] ; wald p = 00024 ; gure 3ac )  . 
the hr for the pooled radical prostatectomy full ( ie , low , intermediate , and high - risk ) cohort at 5 years was 27 ( 95% ci 1548 ; p = 00024 ; auc 057 [ 95% ci 052061 ] )  . 
percentage of genome alteration strati es patients at risk of rapid failure consistent with occult metastases , and was increased in 1524 vol 15 december 2014 articles outcome ( biochemical relapse - free survival at 5 years was 93% ) , whereas those with high levels of both measures had the worst ( 49% ; gure 4d )  . 
after the addition of percentage of genome alteration to the multivariate cox proportional hazard model for subtypes , only subtypes 2 and 3 remained prognostic , suggesting that their prognostic ability stems from both speci c genetic aberrations and general genomic instability ( appendix p 18 )  . hypoxia is an important aspect of cancer metabolism and in itself can be prognostic in patients with prostate cancer.19 , 20 we used three hypoxia rna signatures that have been validated in other tumour types to estimate hypoxia within the pooled radical prostatectomy mrna cohorts ( 108 mskcc patients and 110 cambridge patients ; table 3 and gure 4ac ; appendix p 22 ) .2729 none of these signatures were univariately prognostic , nor were they related to gleason score , psa , t category , or percentage of genome alteration ( appendix 5659 )  . 
 however , when we separated patients into four groups on the basis of high versus low percentage of genome alteration and high versus low hypoxia values , we found that hypoxia increased the prognostic accuracy of the percentage genome alteration for risk of biochemical relapse . 
patients with a high percentage of alteration and high hypoxia have the worst prognosis , whereas those with high hypoxia alone ( low percentage of alteration ) responded well after radical prostatectomy ( gure 4ac , appendix pp 2324 , 6061 )  . less to validate this nding , we used the toronto cohort the biobanking of frozen biopsies was because completed with simultaneous and direct assessment of tumour hypoxia at the same intraprostatic locale.20 this cohort therefore contained direct measurements of for hypoxia denoted by patient - speci c values proportion of oxygen measurements than 20 mm hg ( hp20 ; appendix p 25 ) .20 the median hp20 in our cohort was 81% ( range 6493 )  . 
 * the cox proportional hazard model was t with four levels ( percentage of genome alteration status / hypoxia status : + / + , + / , / + , and / , whereby + / + patients had a high percentage of genome alteration and high hypoxia , + / patients had high a high percentage of genome alteration and low hypoxia , etc ) , with / patients used as the baseline group . 
 table 3 : data for patients strati ed by hypoxia percentage of genome alteration and hypoxia ( unadjusted hr for biochemical relapse 38 [ 95% ci 1212 ] ; wald p = 0019 ; appendix pp 2627 ) when used as a combined prognostic index . 
again , patients whose tumour solely showed hypoxia , but not genome alteration , fared better than expected for patients with hypoxic tumours after image - guided radiotherapy , suggesting that cohorts of patients with high hypoxia and a high percentage of genome alteration could bene t from treatment intensi cation . because speci c genes ( gure 1 ) , general genomic instability ( gures 2 , 3 ) , and tumour microenvironment ( gure 4 ) all play a part in determination of patient prognosis , we postulated that a supervised machine learning approach would capture the complex and unknown interactions between genes underlying these events . 
using a random forest21 classi er trained on the toronto cohort , we developed a biopsy - driven prognostic signature that predicts biochemical failure and could guide clinical decisions before , and independent of , treatment ( appendix pp 6667 )  . 
 we rst veri ed the signature in the independent lowrisk and intermediate - risk mskcc cohort , in which it predicted biochemical relapse with an area under the curve of 074 ( 95% ci 065083 )  . 
 58% ( 95% ci 3596 ) of patients in the mskcc low - risk to intermediate - risk groups who were classi ed as poor prognosis were biochemical relapse - free at 5 years , compared with 89% ( 8596 ) for those classi ed as good prognosis , and this di erence remained signi cant after adjustment for clinical covariates ( multivariate analysis hr for biochemical relapse 61 [ 95% ci 2019 ] ; wald p = 00015 ; appendix pp 29 , 70 )  . 
 importantly , our signature e ectively identi ed patients at risk of relapse within 18 months in the full mskcc cohort , despite not including any high - risk patients in the initial training cohort ( 33 [ 1110 ] ; wald p = 0038 )  . 
 we validated this early - failure e ect in a second independent cambridge cohort ( 28 [ 1794 ] ; wald p = 0050 ; appendix pp 30 , 70 )  . 
when genomic instability ( pga ) and hypoxia ( hp20 ) were combined within the same patient , we noted a multiplicative and independent prognostic e ect in image - guided radiotherapy patients ( d )  . 
 importantly , the signature also identi ed patients who go on to develop metastasis ( auc 078 [ 95% ci 063093 ] ; appendix p 76 )  . to underpin the potential use of our dna signature , we noted that the signature had auc and c - index values that were greater than 97% ( 970 000 / 1 000 000 ) of the empirical null distribution from randomly sampled genesets ( appendix p 77 )  . 
furthermore , our signature outperformed 23 previously published rna signatures for prostate cancer biochemical relapse - free survival rates after training of random forests with a cohort of 1299 low - risk to high - risk patients with prostate cancer ( including 293 low - risk to intermediaterisk patients ) with mrna microarray data ( gure 6 )  . 
 application of these trained forests to the 108 mskcc patients with information about both mrna and copy number alteration showed that our dna signature has the highest overall auc ( gure 6a , b ; appendix pp 31 , 78 )  . there is a low alteration rate for most of the genes identi ed in the signature : 154 ( 56% ) of 276 genes had copy - number alterations in zero to 39 patients ( of a total sample size of 397 patients ) , which is less than 10% of the total combined cohorts size ( appendix p 79 )  . 
 vol 15 december 2014 1527 articles ||||| ||| | | ||||| | |||| ||| || | |||||||| | ||||| | | |||| || | | ||||||| || | || | ||||| || ||||| | || |||| | |||| |||| |||| ||| | ||| || | hr 27 ( 95% ci 1264 ) ; p = 0021 signature negative signature positive number at risk signature negative signature positive time ( years ) ||||| | | | ||| || | hr 29 ( 95% ci 1460 ) ; p = 0039 number at risk signature negative signature positive time ( months ) figure 5 : a prognostic dna signature for prostate cancer multivariate cox proportional hazard model adjusting for clinical covariates ( gleason score and pretreatment psa ) in the low - risk and intermediate - risk groups ( a ) and when applied to the full pooled radical prostatectomy cohort ( n = 271 ) the signature for copy number alteration identi es patients who will fail rapidly ( b )  . 
signature negative = patients whose tumour genomics were negative for the dna signature . these results strongly support the use of multigene models , because our biopsy - based dna signature outperformed reported prognostic genes ( appendix p 80 )  . 
notably , genes in these regions relate to lipid metabolism ( appendix p 82 )  . tumours have signi cantly we noted that the signature directly accounts for genomic instability ( appendix pp 8285 )  . 
first , patients lower with subtype - 4 signature risk scores than do those with other subtypes ( median 017 [ iqr 00026032 ] vs 041 [ 031061 ] ; p < 00001 , two - sided mann - whitney u test )  . 
second , percentage of genome alteration di ers signi cantly between the classes predicted by the signature and can be estimated from the gene signature ( spearmans correlation between whole - genome and signatureestimated percentage of genome alteration pga ( cid : 1 ) 073 ; thereby providing similar prognostic p < 00001 ) , information . 
importantly , signature - based estimates of percentage of alteration remain highly prognostic , and the addition of 30 genes ( selected from the toronto cohort ) improves estimates of percentage of alteration in the validation cohorts ( eg , mskcc : spearmans ( cid : 1 ) 073 vs 087 ; p < 00001 ; appendix p 32 )  . 
the hr of percentage of genome alteration as a continous variable estimated from these 306 genes is identical to that of the true percentage of genome alteration in the mskcc cohort and nearly identical to that of the cambridge cohort . 
taken together , these results show that our treatment - independent dna - prognostic signature measures genomic instability in addition to lipid metabolism pathways , suggesting our signature might identify candidates for treatment - intensi cation trials targetting these processes ( appendix pp 8691 )  . discussion our ndings show that combined indices of genomic instability and hypoxia can improve accuracy of prognosis in patients with localised prostate cancer in the context of present clinicopathological variables . 
development of prostate - cancer biomarkers to guide disease management at the time of diagnosis is a di cult but crucial challenge in view of the high rates of overtreatment and clinical relapse.30 initial investigation in the toronto cohort showed striking genomic heterogeneity in the pretreatment biopsies from these patients , and has implications for the discovery of driver mutations in prostate cancer . 
 identify inclusion of additional patients from the independent mskcc cohort of low - risk and intermediate - risk patients mskcc full cohort cambridge full cohort * univariate multivariate univariate multivariate 100 - loci dna signature 40 ( 2081 ; 000011 ) 28 ( 1460 ; 00060 ) 29 ( 1182 ; 0038 ) 29 ( 1082 ; 0050 ) c index 074 ( 068080 ) 084 ( 078089 ) 064 ( 057071 ) 075 ( 068083 ) 070 ( 061080 ) 074 ( 065083 ) 067 ( 054079 ) 073 ( 062085 ) data are hazard ratio ( 95% ci ; p value ) or hazard ratio ( 95% ci )  . 
data are provided for the 100 - loci dna signature in each full validation cohort on the basis of cox proportional hazard models including only the marker of interest ( univariate ) and models including relevant clinical covariates as in the multivariate models in table 1 ( multivariate )  . 
 * data are based on 18 - month biochemical recurrence . table 4 : performance of the 100 - loci dna signature 1528 vol 15 december 2014 articles cna_rf cuzick lapointe saal glinsky genomichealth talantov ramaswamy stephenson clinical singh bismar long varambally bibikova cna_rf glinsky cuzick saal bibikova lapointe bismar genomichealth ramaswamy varambally singh long clinical talantov stephenson led to larger subtype sizes amenable to analyses of biochemical relapse - free survival , showing signi cant di erences in patient outcome according to subtype . 
 patients agged by our copy - number alteration - based signature had biochemical relapse rates that were increased by up to six times , and were at risk of failure within 18 months , all within the clinical context of gleason score , t category , and psa . 
in particular , this signature is highly e ective for low - risk patients , because it can identify those ineligible for active surveillance and provide additional assurance for those who are . 
for instance , if the dna signature was used by clinicians today , of 1000 patients diagnosed with localised disease , 144 patients would be o ered more aggressive treatment ( all signature - positive patients ) and 650 would have the support for active surveillance instead of local treatment ( low - risk signature - negative patients )  . intermediate - risk to an image - guided preclinical experimental work supports hypoxia generating a mutator phenotype ( decreased dna repair leading increased mutation rate and genomic instability ) and selecting for genetically unstable clones , in addition increased capacity for distant metastases.18 this metastatic phenotype occurs independently of local treatment ; hypoxia is associated with both local relapse after image - guided radiotherapy and biochemical failure and distant metastasis in patients receiving radical prostatectomy for prostate cancer.19 , 20 here we have shown that simultaneous measurement of tumour hypoxia and genomic improve the prognostic capability of a pretreatment biopsy by combining the independent biology of cancer genomics with the tumour microenvironment . 
moreover , the poor prognosis previously associated with hypoxia19 , 20 might have been related to genomic instability within a subset of these specimens , because hypoxia itself was not associated with poor prognosis in the absence of a heightened percentage of genome alteration . instability can radiotherapy led cancer - cell metabolism ( increased glycolysis , high lactate , and hypoxia ) is related to oncogene activation and loss of tumour suppressor genes , and increased lipid and fatty acid synthesis have been associated with progression of prostate cancer.31 , 32 therefore it is striking that our supervised machine - learning approach the discovery of a genetic signature enriched for genes involved in lipid biology . 
combined with the nding that constitutive activation of mtorc1 renders hypoxic cells lipids , our dependent on exogenous desaturated signature could represent abnormalities in cancer metabolism amenable to targeting of lipid synthesis.3134 further more , our signature e ciently captures the prognostic e ect of percentage of genome alterationa surrogate for genomic instability . 
because androgen deprivation therapy improves oxygenation35 and reduces dna repair36 in patients with prostate cancer , we speculate that such therapies targeting hypoxia and figure 6 : training and comparison of random forest signatures for 23 previously published rna signatures for biochemical relapse - free survival we trained a clinical model ( in green ) with clinical variables : pretreatment psa , biopsy - based gleason score , and t category . 
we compared our dna - based signature ( cna_rf , shown in red ) with these signatures in the 108 memorial sloan kettering cancer center patients with information about both mrna and cna . 
the dna , rna , and clinical signatures were trained in a cohort of 293 lowrisk to intermediate - risk patients with prostate cancer ( a ) and 1299 low - risk to high - risk patients ( b ) , including some with locally advanced disease . 
patients agged by our signature might intensi cation with bene t androgen deprivation therapy or other systemic therapies from patient - speci c vol 15 december 2014 1529 articles to o set both local and systemic resistance , independent of primary treatment . to our knowledge , this is the rst report of biopsydriven , dna - based indices that predicts prognosis in patients who received either image - guided radiotherapy or radical prostatectomy as primary therapy for patients with prostate cancer ( panel )  . 
dna alterations might be less variable than rna abundance patterns within intraprostatic biopsies from dynamic tumour microenvironments , and more stable ex vivo during formalinxed , para n - embedded protocols . 
because our training cohort was obtained before primary the characterisation of complex indices , showing a priori interpatient heterogeneity , soon after diagnostic mriguided or transurethral ultrasound - guided biopsies . 
 indeed , we have shown that frozen biopsies are amenable to whole - genome sequencing to assess in genomic aberrations intrapatient heterogeneity ( boutros pc , unpublished )  . therapy , our study supports our study has several caveats . 
 nonetheless , our identi cation of patients with metastasis , and can identify patients who will have biochemical relapse before 18 months , which has been shown to be predictive for prostate cancer - speci c mortality.6 , 7 although the cohorts shows promise signature panel : research in context systematic review we reviewed previous studies on the basis of pubmed searches done between jan 1 , 1990 , and dec 31 , 2013 , with the terms : genomics , dna , rna , hypoxia , prognosis , radiotherapy , surgery , radical prostatectomy , acgh , rna expression , arrays , classi er , and biomarker . 
we focused on multigene indices that had been validated in at least one cohort , and noted many previously published rna signatures for prognosis in prostate cancer and for hypoxia in various tissue types . 
to the best of our knowledge , no multigene dna signature exists , and no biomarker assesses genomics and the tumour microenvironment simultaneously . interpretation we propose the use of dna - based and rna - based signatures to measure genomic instability and tumour hypoxia to guide clinical management of patients with primary diagnostic biopsies . 
our 100 - loci dna signature , which measures genomic instability and is enriched for lipid metabolism genes , outperforms previously published rna - based prognostic signatures for prostate cancer . 
once our assays undergo clinical quality assurance protocols within a hospital setting , clinicians can use this assay to divert patients to appropriate clinical trials . di er slightly in the distribution of clinicopathological factors , these di erences changed neither treatment nor survival , making it very unlikely that the di erences a ect the interpretation of our results . 
we will explore this outcome in new cohorts of patients treated with imageguided radiotherapy or radical prostatectomy with or without androgen deprivation therapy , and assess whether the biomarker would become a predictive , rather than a solely prognostic , biomarker . from a technical perspective , despite di erent resolutions between the copy number alteration platforms used for each cohort , the copy number alteration indices developed in the toronto cohort validated in the radical prostatectomy cohorts . 
in future studies we will characterise the dna , rna , and epigenetic pro les of foci within patients who receive oral pimonidazole before treatment to investigate the genomichypoxia prognostic association in ner detail . 
finally , e orts are underway to reduce the signature size without loss of prognostic information related to metabolism or genomic instability , and to improve the sensitivity of our signature with multimodal data sets ( eg , combined dna , rna and epigenetic analyses ) emerging from studies from the international cancer genome consortium and the cancer genome atlas . instability the use of genomic identi cation of the correct patients to treat while avoiding overtreatment in the low - risk to intermediaterisk group remains an important clinical dilemma . 
we and envision microenvironment signatures to divert patients from present clinical risk categories to novel clinical trials of treatment intensi cation , whereby patients with poor prognosis based on these novel biomarkers can be enrolled into trials that add combined local and systemic therapies . 
additionally , low - risk and intermediate - risk patients with low levels of hypoxia and and low percentages of genome alteration could be entered into clinical trials of active surveillance . 
these precision medicine approaches set the stage for novel treatment intensi cation and treatment deintensi cation trials to either increase cure rates by prevention of progression to metastatic castration - resistant prostate cancer or to reduce the burden of overtreatment . contributors el contributed to the bioinformatics analysis , machine learning , the statistical analysis , visualisation , and manuscript preparation . 
rgb contributed to study design , clinical analysis , and manuscript preparation declaration of interest el , pcb , and rgb have a patent biopsy - driven genomic signature for prostate cancer prognosis pending . 
 lll has a patent bladder cancer diagnostics pending , and ed has a patent systems and methods for expression - based discrimination of distinct clinical disease states in prostate cancer pending . 
 acknowledgments we thank study volunteers for their participation , and sta at the wellcome trust clinical research facility , addenbrookes clinical research centre , cambridge , uk for their help in conducting the study . 
 this study was done with the support of movember funds through prostate cancer canada and with the additional support of the ontario institute for cancer research , funded by the government of ontario and by a doctoral fellowship from the canadian institute for health research to el . 
we acknowledge the support of the national institutes of health research cambridge biomedical research centre and the national cancer research prostate cancer : mechanisms of progression and treatment ( prompt ) collaborative ( grant code g0500966 / 75466 ) , which has funded tissue and urine collections in cambridge . 
we acknowledge the support of the university of cambridge , cancer research uk and hutchison whampoa limited , and the support of cancer research uk cambridge institute genomics and bioinformatics core facilities . 
we aimed to investigate whether adding bortezomib to standard therapy could improve outcomes in patients with these subtypes . methods in a randomised evaluation of molecular guided therapy for diffuse large b - cell lymphoma with bortezomib ( remodl - b ) , an open - label , adaptive , randomised controlled , phase 3 superiority trial , participants were recruited from 107 cancer centres in the uk ( n = 94 ) and switzerland ( n = 13 )  . 
eligible patients had previously untreated , histologically confirmed diffuse large b - cell lymphoma with sufficient diagnostic material from initial biopsies for gene - expression profiling and pathology review ; were aged 18 years or older ; had ecog performance status of 2 or less ; had bulky stage i or stage iiiv disease requiring full - course chemotherapy ; had measurable disease ; and had cardiac , lung , renal , and liver function sufficient to tolerate chemotherapy . 
patients initially received one 21 - day cycle of standard rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ; rituximab 375 mg / m , cyclophosphamide 750 mg / m , doxorubicin 50 mg / m , and vincristine 14 mg / m [ to a maximum of 2 mg total dose ] intravenously on day 1 of the cycle , and prednisolone 100 mg orally once daily on days 15 )  . 
during this time , we did gene - expression profiling using whole genome cdna - mediated annealing , selection , extension , and ligation assay of tissue from routine diagnostic biopsy samples to determine the cell - of - origin subtype of each participant ( germinal centre b cell , activated b cell , or unclassified )  . 
patients were then centrally randomly assigned ( 1 : 1 ) via a web - based system , with block randomisation stratified by international prognostic index score and cell - of - origin subtype , to continue r - chop alone ( r - chop group ; control ) , or with bortezomib ( rb - chop group ; experimental ; 13 mg / m intravenously or 16 mg / m subcutaneously ) on days 1 and 8 for cycles two to six . 
 this study was registered at clinicaltrials.gov , number nct01324596 , and recruitment and treatment has completed for all participants , with long - term follow - up ongoing . findings between june 2 , 2011 , and june 10 , 2015 , 1128 eligible patients were registered , of whom 918 ( 81% ) were randomly assigned to receive treatment ( n = 459 to r - chop , n = 459 to rb - chop ) , comprising 244 ( 266% ) with activated b - cell disease , 475 ( 517% ) with germinal centre b cell disease , and 199 ( 217% ) with unclassified disease . 
 at a median follow - up of 297 months ( 95% ci 290320 ) , we saw no evidence for a difference in progression - free survival in the combined germinal centre and activated b - cell population between r - chop and rb - chop ( 30 - month progression - free survival 701% , 95% ci 650747 vs 743% , 693787 ; hazard ratio 086 , 95% ci 065113 ; p = 028 )  . 
the most common grade 3 or worse adverse event was haematological toxicity , reported in 178 ( 398% ) of 447 patients given r - chop and 187 ( 421% ) of 444 given rb - chop . 
however , rb - chop was not associated with increased haematological toxicity and 398 [ 871% ] of 459 participants assigned to receive rb - chop completed six cycles of treatment . 
serious adverse events occurred in 190 ( 425% ) patients given r - chop , including five treatment - related deaths , and 223 ( 502% ) given rb - chop , including four treatment - related deaths . interpretation this is the first large - scale study in diffuse large b - cell lymphoma to use real - time molecular characterisation for prospective stratification , randomisation , and subsequent analysis of biologically distinct subgroups of patients . 
 introduction the combination of rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ) has been considered standard of care for diffuse large b - cell lymphoma for more than 15 years.1 in trials of r - chop , 5 - year progression - free survival has been reported to be 7075% and overall survival 7580% , 2 although unselected population - based studies show lower figures.3 patients with lymphoma that does not respond to r - chop or that recurs have a poor prognosis , with only a third alive at 2 years after diagnosis.4 various approaches have been attempted to improve outcomes for patients with diffuse large b - cell lymphoma , but none has so far increased overall survival . 
the recognised molecular heterogeneity of this aggressive lymphoma contributes to the complexity of this problem.5 gene - expression profiling of diffuse large b - cell lymphoma has been used to define subgroups with distinct pathogenesis . 
cell - of - origin classification recognises those cases with a gene expression similar to that of peripheral blood b cells undergoing in - vitro antigen activation , referred to as the activated b - cell subtype , whereas the germinal centre b - cell subtype resembles b cells in the germinal centre . 
retrospective analyses suggest that the patients with the activated b - cell subtype have worse outcomes , with 40% 3 - year progression - free survival after r - chop compared with 75% in the germinal centre b - cell group.5 the subtypes have distinct genomic characteristics . 
 the activated b - cell subtype shows a higher prevalence of mutations in genes involved in b - cell receptor signalling and regulators of nuclear factor ( nf ) - b ( myd88 , cd79b , tnfaip3 , card11 , traf2 , traf5 , map3k7 , and tnfrsf11a ) than the germinal centre b - cell subtype . 
constitutive nf - b activation down stream of the b - cell receptor is a feature of the activated b - cell subtype of diffuse large b - cell lymphoma . 
genomic , pharmacological , and rna interference screens have shown selective oncogenic addiction of the activated b - cell subtype to activation of this protein complex.6 bortezomib is a proteasome inhibitor and can suppress nf - b activity by preventing proteosomal degradation research in context evidence before this study we searched pubmed for publications of randomised clinical trials in english between jan 1 , 1998 , and dec 1 , 2010 , using the terms diffuse large b - cell lymphoma and cell of origin , and studies involving diffuse - large b - cell lymphoma and bortezomib . 
using gene - expression profiling to characterise patients , several retrospective studies of patients treated with rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ( r - chop ) or chop - like regimens had shown that the activated b - cell subtype was associated with inferior survival compared with the germinal centre b - cell subtype . 
in another phase 2 study , bortezomib in combination with dose - adjusted r - epoch ( rituximab , etoposide , cyclophosphamide , doxorubicin , vincristine , and prednisolone ) had resulted in longer progression - free survival in patients with the activated b - cell subtype than in those with the germinal centre b - cell subtype . 
bortezomib in combination with r - chop had produced similar outcomes in non - germinal centre b - cell diffuse large b - cell lymphoma ( ascertained by immunohistochemistry ) compared with germinal centre b - cell diffuse large b - cell lymphoma in a further phase 2 study . added value of this study to our knowledge , this study is the first to combine prospective gene - expression profiling of lymphoma with a targeted therapy to allow stratification and random assignment of patients to treatment within a phase 3 clinical trial . 
it is the first study to assess a novel agent in diffuse large b - cell lymphoma , prospectively powered to address subtypes defined by gene - expression profiling , and we have shown that the addition of bortezomib to r - chop ( rb - chop ) does not improve survival in the activated b - cell subgroup . 
 extensive characterisation and subgroup analyses suggest that cell - of - origin subtype and nuclear factor ( nf ) - b activating mutations are not associated with improved outcomes with rb - chop , and that bortezomib does not act as an effective inhibitor of the nf - b pathway in this disease . 
 exploratory analyses , however , suggest that different high - risk subgroupsdouble - expressor lymphoma and double - hit lymphomamight benefit from the addition of bortezomib or similar agents to standard immunochemotherapy . implications of all the available evidence the trial design provides a rational framework for future studies in diffuse large b - cell lymphoma , allowing prompt initiation of treatment while molecular characterisation is carried out . 
 we confirm that r - chop is a good standard of care for most patients with diffuse large b - cell lymphoma , but raise the possibility that high - risk subgroups could benefit from the addition of a proteasome inhibitor to standard therapy , which could guide future research . 650 vol 20 may 2019 articles see online for appendix for the tenalea system see alea / login.aspx of the inhibitor ib , thereby keeping nf - b inactive and unable to translocate to the nucleus to mediate transcription . 
when combined with infusional chemotherapy , bortezomib appeared to have preferential activity in relapsed or refractory activated b - cell diffuse large b - cell lymphoma , with a higher response rate and median overall survival than that achieved with infusional chemotherapy alone.7 for diffuse large b - cell the randomised evaluation of molecular guided therapy lymphoma with bortezomib ( remodl - b ) study aimed to investigate the clinical efficacy of r - chop in addition to bortezomib in patients with diffuse large b - cell lymphoma . 
to determine whether the cell - of - origin subtypes respond differently to the combination of bortezomib with r - chop , we used a study design that incorporated prospective randomisation stratified by whole transcriptome gene - expression profiling . 
we also incor porated molecular characterisation into our analysis to assess recognised subgroups distinct from the cell - of - origin subgroups : double - hit ( rearrangements of myc and bcl2 or bcl6 , or both ) and double - expressor lymphomas ( high expression of myc and bcl2 proteins )  . as clinical studies move towards increased application of targeted drugs against molecular phenotype , the feasibility of determining a molecular phenotype in real - time was an important objective of the study . methods study design and participants in this multicentre , open - label , randomised , phase 3 , superiority trial , we compared r - chop with r - chop plus bortezomib ( rb - chop ) in patients with newly diagnosed diffuse large b - cell lymphoma . 
in a collaboration between the uk national cancer research institute group and the schweiz arbeitsgemeinschaft fur klinische krebsforschung in switzerland , patients were recruited from 107 cancer centres in the uk ( n = 94 ) and switzerland ( n = 13 )  . 
patients were eligible for inclusion in the study if they had de novo diffuse large b - cell lymphoma confirmed by an expert haematopathologist ( cb ) with sufficient diagnostic material from previous biopsies for gene - expression profiling and central pathological review ; were aged 18 years or older ; had eastern cooperative oncology group ( ecog ) performance status of 2 or less ; had bulky stage i or stage iiiv disease requiring fullcourse chemo therapy ; had measurable disease ; and had cardiac , lung , renal , and liver function sufficient to tolerate chemo therapy . 
patients with primary mediastinal lymphoma ; clinical cns involvement ; positive serology for hiv , hepatitis b virus , or hepatitis c virus ; active malignancy in the preceding 5 years ; or other conditions precluding administration of study treatment were ineligible . 
the study was carried out according to the principles of the declaration of helsinki , principles of the international conference on harmonisation of technical requirements for registration of pharmaceuticals for human use good clinical practice , and in accordance with uk and swiss regulatory requirements . 
written informed consent was obtained from all patients . randomisation and masking participants were centrally randomly assigned ( 1 : 1 ) with block randomisation of varying block size by tenalea , a web - based system , to receive either r - chop ( control ) or rb - chop ( experimental )  . 
for the purposes of stratification , participants were grouped by their ipi scores as : low ( 01 ) , intermediate ( 23 ) , and high ( 45 ) , and those with an unclassified cell - of - origin sub type were included . 
 in cases of failed rna extraction or insufficient rna yield , participants were not randomly assigned but were given conventional r - chop treatment and followed up with the same assessments as participants in the control group , but analysed as a distinct group . 
participants , investigators , and treating clinicians were unmasked to the treatment allocation ; however , local investigators were not informed which molecular subgroup the participants were in . procedures participants underwent routine staging investigations , including ct scans and bone marrow biopsy , with examination of cerebrospinal fluid as clinically indicated . 
 tumour material was sent to the central laboratory ( haematological malignancy diagnostic service , leeds cancer cancer centre , leeds teaching hospitals , leeds , uk ) for gene - expression profiling and somatic mutation assessment . for cycle one , all participants received the r - chop regimen on a 21 - day schedule . 
the regimen comprised rituximab 375 mg / m intravenously , cyclophosphamide 750 mg / m intravenously , doxorubicin 50 mg / m intravenously , and vincristine 14 mg / m ( maximum total dose 2 mg ) intravenously on day 1 of the cycle , and prednisolone 100 mg orally once daily on days 15 . 
 from cycle 2 onwards , participants were randomly assigned to their treatment groups , either to receive five further cycles of r - chop in the control group , or five cycles of r - chop plus bortezomib ( rb - chop ) on days 1 and 8 ( 13 mg / m intravenously or 16 mg / m vol 20 may 2019 articles subcutan eously ) in the experimental group . 
further cycles were given when neutrophils had recovered to 10 10 per l and platelets to 100 10 per l ; dose reductions of bortezomib in response to neurotoxicity were closely specified according to severity of this toxicity ( appendix pp 4853 )  . on feb 28 , 2014 , we changed the route of bortezomib from intravenous to subcutaneous administration and updated the protocol after publication of data7 that suggested subcutaneous administration was associated with decreased toxicity and similar efficacy at a lower dose , and greater acceptability to patients , as compared with intravenous administration.8 patients who were already being given intraveous bortezomib continued on formulation . 
intrathecal prophylaxis with methotrexate was recommended for patients at high risk of cns relapse for three to six cycles and could be given at any time at investigators discretion at each study site . 
cross - sectional imaging was repeated 1 month after administration of the final dose of chemotherapy to assess disease response using the international working group response criteria for nonhodgkin lymphoma9 and repeated at 12 months . participants were assessed clinically at the beginning of each treatment cycle and after treatment completion every 3 months for 1 year and thereafter every 6 months until 5 years total follow - up . 
progressions were recorded after clinical assessment and imaging , determined by local investigators , according to standard criteria , 9 and at progression trial treatment was discontinued and patients were followed up until data cut off for survival . histological haematoxylin and eosin sections from formalin - fixed paraffin - embedded ( ffpe ) samples taken at diagnosis were reviewed in the central laboratory as a quality check . 
rna was extracted using an ambion recoverall total nucleic acid isolation kit for ffpe ( thermofisher , waltham , ma , usa ) according to the manufacturers protocol , with the exception that two washes in xylene and alcohol were used to remove wax , with extended digestion in proteinase k overnight . during cycle 1 of r - chop , gene - expression profiling was done ( by sb ) using illumina whole genome cdnamediated annealing , selection , extension , and ligation ( dasl ) assay ( illumina , san diego , ca , usa )  . 
patient samples were classified as activated b - cell , germinal centre b - cell , unclassified , or fail ( ie , insufficient quality or quantity of dna or failure of dasl array ) by use of the dasl automated classifier as previously described , 10 with a quality control of a score over 1 to define technical failure . 
the confidence of each sample being one of the three classes was recorded and the final classification was defined as that with the highest confidence score . for tissue micorarrays when possible , we used tissue from the biopsy sample immunohistoto construct chemistry , fluorescence in - situ hybrid isation , and dna extraction . 
specifically , we did immunohistochemistry for myc and bcl2 protein ( dual ) expression using these tissue micorarrays and abcam rabbit monoclonal antibodies ( abcam , cambridge , uk ; clone y69 ) , with a cutoff of 40% or more , and dako anti - bcl - 2 monoclonal antibodies ( agilent , santa clara , usa ; clone 124 ) with a cutoff of 50% or more , scored by two independent assessors according to recognised criteria . 
these cutoff values were used to identify categories of myc and bcl2 gene expression : high or average . dna was extracted from tumour cells enriched by microdissection on ffpe tissue sections and its quality was assessed by pcr of variously sized genomic fragments . 
a panel of 70 genes that are recurrently mutated in aggressive b - cell lymphomas were investigated for mutation by targeted sequencing using haloplexhs target enrichment ( agilent technologies , santa clara , ca , usa ) and illumina hiseq sequencing , as described previously.11 this process was carried out for participants who had dna available of adequate quantity and quality . 
duplicate experiments were done for samples of lower quality , including all those with quality control pcr showing amplification of 300 bp or fewer genomic fragments , and only those mutations that were repro ducible in both experiments were reported . 
variant calling , single nucleotide polymorphisms , and back ground noise filtering were done as previously described.11 in a further 22 samples , mutations in 20 genes ( included in the above panel of 70 genes ) were analysed in duplicate using fluidigm multiplex pcr ( fluidigm , south san francisco , ca , usa ) and illumina miseq sequencing , as described previously , because of evolution of molecular diagnostics during the study period.11 variants detected by use of these targeted sequencing methods were further assessed by use of functional prediction tools . 
as part of a post - hoc analysis , samples were tested for the possible presence of primary mediastinal lymphoma using a bayesian predictor described by the lymphoma molecular profiling project to ensure that no molecular cases of primary mediastinal lymphoma had been included.12 safety was assessed by the recording and grading of adverse events according to the common terminology criteria for adverse event reporting version 4.0 at each study visit , or between visits if notified . 
serious or severe adverse events , including mention of suspected unexpected serious adverse reactions were defined as per the medicines for human use ( clinical trials ) regulations 2004 . outcomes the primary endpoint was 30 - month progression - free survival in the germinal centre and activated b - cell popualtion , defined as time from registration to the date of progression or death from any cause . 
disease progression was determined using the international working group response criteria for non - hodgkin lymphoma.9 participants free from progres sion or death were censored at the date of their last visit . 
secondary outcomes were 30 - month progression - free survival by cell - of - origin subgroup ; the time - to - event variables of overall survival , event - free survival , disease - free survival , and time to progression ; response duration ; complete and overall proportion of patients who achieved a response ; assessment of toxicity ; quality of life ; assess ment of peripheral neuropathy up to 30 days after last treatment ; and safety . 
the proportion of patients who achieved a complete and overall response , duration of response , event - free survival , disease - free survival , time - to - progression , and quality - of - life assessments will be reported elsewhere . 
 statistical analysis we used an adaptive design based on a two - stage approach , with two interim analyses to explore the safety and efficacy in the germinal centre b - cell group treated with rb - chop after a defined number of events . 
if progression - free survival at 12 months was assessed to be below 70% in this subgroup , the trial would stop recruiting into the germinal centre b - cell group . 
the second interim analysis was to take place when 73 patients in the germinal centre b - cell group had been randomly assigned to receive rb - chop and followed up for 1 year . 
 if the progression - free survival at 12 months was assessed to be below 85% in this subgroup , the trial would stop recruiting into the germinal centre b - cell group . the trial was powered to detect an improvement in progression - free survival at 30 months of 10% in the combined activated b - cell and germinal centre b - cell groups , from 75% in the r - chop group to 85% in the rb - chop group ( corresponding to a hazard ratio [ hr ] of 056 ) , on the basis of a log - rank test with a significance level of 5% ( two - sided ) and 90% power , requiring a total of 129 events . 
the intention - to - treat ( itt ) population comprised all patients for whom geneexpression profiling was attempted ( classified as activated b - cell , germinal centre b - cell , or unclassified subgroups , or for whom gene - expression profiling failed )  . 
the safety population was formed of all patients in the itt population who received at least one dose of any study drug . we assessed the primary outcome of 30 - month progression - free survival in a modified itt ( mitt ) population comprising the activated and germinal centre b - cell subgroups who were randomly assigned to receive treatment , using a cox proportional hazards model , adjusted for cell - of - origin subtype and ipi score . secondary outcome analyses included repeating the primary outcome analysis in the activated b - cell itt population alone , the germinal centre b - cell itt population , and the unclassified itt population , adjusting for ipi score only . 
we used summary statistics to describe baseline chara cteristics for participants in the r - chop group , rb - chop group , and patients for whom gene - expression profiling had failed in the itt population , and by cell - of - origin subgroups in the itt population , with formal com parisons between cell - oforigin subgroups using pearson tests . 
 further post - hoc analyses included repeating the primary outcome analysis and adjusting for time from diagnosis to the start of treatment to ascertain whether or not the interval from diagnosis to treatment affected the progression - free survival outcome . 
we also did post - hoc analyses to assess progression - free survival and overall survival by treatment group in the mitt population in the ipi low , intermediate , and high score groups , assessed using a cox proportional hazards model , adjusted for cellof - origin subtype , and also repeated the primary outcome analysis excluding patients who had a dose reduction in any treatment drug . 
rb - chop = rituximab , bortezomib , cyclophosphamide , doxorubicin , vincristine , and prednisolone . com paring double - expressor lymphomas to all other cases , separated by treatment group ; and comparing by treat ment groups in subgroups with mutations in components of the nf - b pathway . we used stata statistical software ( version 15.1 ) for all analyses . 
 the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results between june 2 , 2011 , and june 10 , 2015 , of 3449 patients assessed for eligibility , 1128 ( 327% ) participants were registered to the study ( figure 1 )  . 
of the registered participants , a further 52 who received one cycle of r - chop were excluded for reasons including ineligibility after tumour biopsy ( n = 29 ) and insufficient tumour data 654 vol 20 may 2019 articles ( n = 5 )  . 
158 ( 147% ) of 1076 remaining participants had inadequate sample material for gene - expression profiling and so were excluded from subsequent random assignment to treatment , and instead given r - chop as per the control group . 
918 ( 853% ) of 1076 participants were stratified by cell - of - origin subtype and ipi and randomly assigned to receive r - chop or rb - chop ( figure 1 )  . 
overall , 244 ( 266% ) patients had activated b - cell disease , 475 ( 517% ) had germinal centre b - cell disease , and 199 ( 217% ) had unclassified disease . 
the planned interim analyses and safety assessments by the data monitoring and ethics committee in the germinal centre b - cell group showed the 1 - year progression - free survival to be 70% or above in the germinal centre b - cell subgroup at the first interim analysis and the 1 - year progression - free survival to be 85% or above in the germinal centre b - cell subgroup at the second interim analysis . 
hence , the trial continued to recruit to all groups . baseline characteristics were similar between the control group , experimental group , and non - randomised participants ( table 1 )  . 
for the samples from which sufficient material was extracted , only 1% ( 11 of 1076 ) failed for technical reasons . we observed clinical differences between the molecular subgroups ( table 2 )  . 
median age was higher in the activated b - cell subgroup ( p = 00045 ) and bulky disease occurred more often in the germinal centre b - cell subgroup ( p < 00001 )  . 
no significant difference was seen between the activated and germinal centre b - cell subgroups in the distribution of ipi risk group , serum lactate dehydrogenase ( ldh ) concentration above the upper limit of normal , conventional stage of disease , overall prevalence of extranodal disease , or ecog performance status ( table 2 ; appendix p 6 )  . 
post - hoc testing for the possible presence of primary mediastinal lymphoma identified 19 participants who fulfilled the criteria , 12 of whom 13 ( 68% ) had mediastinal disease . 
of these participants , 14 ( 74% ) had been allocated to the germinal centre b - cell group and five ( 26% ) to the unclassified subgroup . the primary efficacy outcome was analysed when the combined activated and germinal centre b - cell mitt population had been followed up for a median of 30 months , as stipulated in the protocol ( median follow - up 297 months [ 95% ci 290320 ] ; median follow - up of survivors : 294 months [ 286311 ] )  . 
we saw no difference in pro gression - free survival in the combined activated and germinal centre b - cell populations between the r - chop and rb - chop groups ( hr 086 , 95% ci , 95% ci 065113 ; p = 028 ; adjusted hr 084 , 95% ci 064111 ; p = 023 )  . 
after this additional follow - up , the kaplan - meier estimate for 30 - month progression - free survival in the combined activated and germinal centre b - cell mitt population was 706% ( 95% ci 655750 ) for the r - chop group and 752% ( 703794 ) for the rb - chop group . 
we saw no evidence of difference in 30 - month progression - free survival in the mitt population between the r - chop and rb - chop groups ( adjusted hr 082 , 95% ci 063108 ; p = 016 ; figure 2a )  . secondary analysis of subtypes by cell of origin showed that bortezomib did not significantly affect progressionfree survival in either the activated b - cell ( adjusted hr 078 , 95% ci 051121 ; p = 027 ) , germinal centre b - cell ( 085 , 060120 ; p = 035 ) , or unclassifiable participants ( 129 , 95% ci 077216 ; p = 034 ; figure 2 )  . 
 we saw no difference in overall survival by treatment group in the mitt population ( 72 deaths in the r - chop group and 61 in the rb - chop group ; adjusted hr 082 , 95% ci 059116 ; p = 027 ) , and the kaplan - meier estimate of overall survival at 30 months was 816% ( 95% ci 771853 ) in the r - chop group versus 831% ( 787867 ) in the rb - chop group ( appendix p 3 )  . the addition of bortezomib to r - chop was well tolerated ( table 3 )  . 
the most common grade 3 or worse adverse event was haematological toxicity , in 178 ( 398% ) of 447 patients given r - chop and 187 ( 421% ) of 444 given rb - chop . 
however , in a post - hoc analysis of adverse events between groups , we saw no significant increase in the proportion of patients who had grade 3 or worse neutropenia , febrile neutropenia , thrombo cytopenia , or anaemia . 
neuropathy of any grade was more frequent in participants given rb - chop than among those given r - chop ( 252 ( 568% ) rb - chop vs 186 ( 416% ) given r - chop ; p < 00001 ; appendix pp 811 ) but there was no significant difference in the event rate of neuropathy of grade 3 or higher ( 17 ( 38% ) rb - chop vs eight ( 18% ) r - chop ; p = 0070 )  . 
nine suspected unexpected serious adverse reactions were reported : four reactions in four participants in the r - chop group ( haemophagocytic syndrome , leukaemia secondary to chemotherapy , neutropenic sepsis , and fracture ) , and five reactions in four participants in the rb - chop group ( jejunal stricture with small bowel obstruction , bowel perforation , sepsis , and one patient had both renal failure and tumour lysis syndrome )  . 
in the safety population , 73 ( 163% ) of 447 participants in the r - chop group and 68 ( 153% ) of 444 in the rb - chop group died , with most deaths due to progressive lymphoma ( 50 [ 685% ] of 73 in the r - chop group , and 54 [ 794% ] of 68 in the rb - chop group ) ; nine treatment - related deaths were reported ( five [ 68% ] of 73 in the r - chop group , four [ 59% ] of 68 in the rb - chop group ; appendix p 13 )  . in the itt population , fewer participants in the r - chop group had dose reductions in any drug than did those in the rb - chop group ( 158 [ 345% ] of 459 vs 196 [ 429% ] of 459 , not including the non - randomsied participants ; appendix p 12 )  . 
fewer participants discon tinued from trial treatments in the r - chop group than in the rb - chop group ( 43 [ 94% ] vs 60 [ 131% ] ; appendix p 11 )  . 
however , median relative dose intensity for participants in the control and experimental groups was similar for drugs comprising r - chop and a high proportion of participants in both groups success fully completed six cycles of treatment : 418 ( 913% ) of 459 in the r - chop group and 398 ( 871% ) of 459 in the rb - chop group ( appendix p 12 )  . the median time from diagnosis to first treatment was similar between treatment groups ( r - chop 17 days [ iqr 1029 ] ; rb - chop 20 days [ 1032 ] )  . 
post - hoc analyses , repeating the primary analysis and adjusting for the time from diagnosis to first treatment interval also showed no difference in 30 - month progression - free survival in the mitt population between the r - chop and rb - chop groups ( 706% , 95% ci 655750 for r - chop , and 752% , 703794 for rb - chop ; adjusted hr 083 , 95% ci 056124 ; p = 036 )  . 
similarly , post - hoc analyses excluding patients who had a dose reduction in any treatment drug showed no difference in 30 - month progression - free survival the mitt population between the r - chop and rb - chop groups ( 689% , 95% ci 624745 for r - chop and 743% , 658810 for rb - chop ; adjusted hr 080 , 95% ci 054119 ; 656 vol 20 may 2019 articles p = 027 )  . 
post - hoc analysis of progression - free survival and overall survival by ipi score are shown in the appendix ( p 4 )  . the panel of genomic mutations confirmed the known association of different somatic changes with cell - oforigin subtypes , with a bias towards alterations in epigenetic modifier genes in the germinal centre b - cell subgroup and genes of the b - cell receptor signalling pathway in the activated b - cell subgroup ( appendix pp 2 , 6 , 7 )  . 
mutations in ezh2 were seen in 250% ( 53 of 212 ) of germinal centre b - cell biopsy samples but only 42% ( five of 118 ) of activated b - cell samples , and conversely mutations in myd88 were found in 90% ( 19 of 212 ) of germinal centre b - cell and 449% ( 52 or 118 ) of activated b - cell samples tested ( appendix pp 1 , 6 , 7 )  . 
 nf - b target genes were expressed at higher levels in the activated b - cell subgroup compared with the germinal centre b - cell group ( appendix p 2 )  . 417 biopsy samples ( 118 from the activated b - cell subgroup , 212 from the germinal centre b - cell subgroup , and 87 from the unclassified subgroup ) were suitable for construction of tissue microarrays . 
karyotypic double - hit lymphomas were rare in the activated b - cell population and were significantly associated with the germinal centre b - cell subtype ( one [ 04% ] of 244 vs 32 [ 67% ] of 475 ; p < 00001 )  . 
 conversely , the activated b - cell subtype was associated with higher concomitant expression of myc and bcl - 2 proteins ( ie , double - expressor lymphomas ) than the germinal centre b - cell subtype was by immuno histochemistry analysis ( excluding double - hit lymphomas ; 56 [ 549% ] vs 45 [ 26% ] ; p < 00001 ) and mrna ( 109 [ 447% ] vs 87 [ 183% ] ; p < 00001 ; appendix p 13 )  . 395 biopsy samples had sufficient dna of adequate quantity and quality for investigation of mutations via targeted sequencing . 
among the participants given r - chop ( including the non - randomised group ) , myc rearrangement , double - hit lymphoma , and dual high myc and bcl - 2 mrna expression were significantly associated with inferior progression - free survival after controlling for ipi ( data not shown )  . 
rb - chop = rituximab , bortezomib , cyclophosphamide , doxorubicin , vincristine , and prednisolone . table 3 : adverse events in the safety population lymphoma in the same treatment group without these rearrangements ( double - hit lymphoma in the r - chop group : 389% vs 758% , adjusted hr 307 , 95% ci 164576 ; p = 000048 ; and dual - expressor the r - chop group : 615% vs 758% , adjusted hr 181 , 126260 ; p = 00013 ; figure 3 )  . 
high con centrations of myc and bcl - 2 proteins by immunohistochemistry did not appear to have a significant effect on outcomes , although few participants had high concentrations of these proteins , resulting in wide confidence limits ( figure 4 )  . 
the effect of bortezomib on progression - free survival in these high - risk groups is shown in figure 4 . we examined the effect of the addition of bortezomib on survival in patients with mutations known to be associated with activation of nf - b , the putative target of bortezomib ( myd88 , cd79a , cd79b , tnfaip3 , tnfrsf11a ) and found no significant differences for single gene alterations ( appendix p 5 )  . discussion in this trial , we have shown the feasibility of molecular phenotyping in a large multicentre study of rapidly progressive tumours and shown that the addition of bortezomib does not affect treatment outcomes in most patients with diffuse large b - cell lymphoma . 
because patients entering clinical trials are often not representative of the wider population , for prospective testing of a complex biomarker we wished to avoid worsening the problem of generalisability by restricted enrolment and delays to the initiation of therapy . 
such delays were avoided by studying routine ffpe biopsy samples and deferring random assignment to a treatment group until the second cycle of r - chop , thereby allowing treatment to start as soon as staging investigations were completed , with molecular analysis taking place in parallel . 
rb - chop = rituximab , bortezomib , cyclophosphamide , doxorubicin , vincristine , and prednisolone . basis of their molecular phenotype will require real - time outputs , which we have shown to be feasible in this trial . 
 using a central laboratory and the dasl automated classifier , we prospectively assigned cell - of - origin categories within a clinically relevant timeframe , which allowed random assignment to treatment to be stratified by cell - of - origin subtype , with the potential for adaptive design based on interim analyses of molecular subtypes . 
the slight increase in neurotoxicity observed in participants in the rb - chop group compared with the r - chop group suggests that the bortezomib was given at a biologically active dose . 
 bortezomib was administered on days 1 and 8 of cycles 25 , at a dose that has shown efficacy in other lymphoma trials , 19 , 20 but we recognise that more potent proteasome inhibitors are now in use , as are other agents with apparent preferential effects in the activated b - cell subgroup , such as lenalidomide and ibrutinib , trials of which are in pro gress ( nct02285062 , nct01855750 )  . bortezomib did not improve outcomes for participants with the activated b - cell subtype of diffuse large b - cell lymphoma , which was confirmed to be enriched for expression of nf - b target genes , or for patients with somatic mutations associated with nf - b activation . 
 inhibition of nf - b might be insufficient to improve outcomes in addition to r - chop in diffuse large b - cell lymphoma , or bortezomib at the doses given might not have been sufficient to inhibit nf - b adequately for outcomes to improve . 
another study in patients with non - germinal centre b - cell lymphoma , selected by immunohistochemistry , did not show a difference between r - chop and the combination of rituximab , cyclophosphamide , doxorubicin , and prednisone ( r - chp ) with bortezomib given in place of vincristine , supporting our finding.20 studies1820 have shown the difficulty of improving the results of initial therapy in diffuse large b - cell lymphoma by the addition of novel drugs that had promising activity in studies treating recurrent disease with a single 660 vol 20 may 2019 articles treatment group . 
this situation might partly reflect biological selection through treatment failure : in relapsed or refractory lymphomas for which new drugs are investigated , the biology of such disease is likely to be different from that of newly diagnosed lymphomas . 
 thus , most germinal centre b - cell diffuse large b - cell lymphoma can be cured by r - chop , whereas recurrent disease is more common for those with double - hit lymphoma . 
similarly , recurrent activated b - cell diffuse large b - cell lymphoma is enriched for double - expressor lymphomas , which might account for the different results reported in our study compared with the previous studies of bortezomib treatment . 
this observation highlights the need for full molecular char acterisation of the disease being treated , both at diagnosis and in the event of initial treatment failure . in this study , the presence of a small number of participants with double - hit lymphoma in the germinal centre b - cell subgroup lowered the progression - free survival estimate for this subgroup . 
overall , however , the progression - free survival outcome for the patients with double - hit lymphoma appears to be better than that reported in some earlier studies21 and is consistent with more recent analyses.22 , 23 although clearly worse than the non - rearranged group , nearly half of double - hit lymphomas appeared to have not progressed at 30 months . 
the progression - free survival at 30 months in patients with double - hit lymphoma was 389% after r - chop compared with 588% after rb - chop , although this result was from a post - hoc analysis and was not statistically significant ( data not shown )  . this study had several limitations . 
any clinical trial is potentially prone to selective recruitment of those patients with better prognoses , but we endeavoured to minimise this effect by deferring random assignment to treatment until the second cycle of therapy , thereby allowing rapid initiation of treatment at the same time as molecular typing . 
as a result , the median time from diagnosis to initiation of therapy was lower than in similar studies , 24 and the distribution of ipi scores in this study was similar to or worse than recent trials , 2 , 18 with 47% of patients being high - intermediate or high risk . 
we were unable to do a comprehensive central histopathology review on the participants enrolled and we did not assess for the presence of epstein - barr virus in the biopsy samples . 
however , all participants were diagnosed by expert haemato pathologists by use of a procedure with high accuracy for diffuse large b - cell lymphoma ( over 96% in a recent case series from the uk25 ) , and because epstein - barr virus is present in less than 3% of diffuse large b - cell lymphoma in europe , 26 the presence of the virus would be unlikely to affect our results . 
the rb - chop group had a slight excess of vincristine dose reductions compared with the r - chop group , which could potentially have eroded a positive effect from the bortezomib . 
the use of routine ffpe biopsy samples was necessitated by the large number of recruiting centres , but resulted in a failure rate of about 15% for molecular typing and might have resulted in a larger than expected number of unclassified cases for whom poor quality rna resulted in a low probability score in the cell - of - origin classifier . in conclusion , this trial has shown that complex molecular characterisation can be done in real time , with a pragmatic treatment schedule that allows for the allocation of therapy on the basis of the molecular subtype . 
this method is likely to become increasingly relevant as our understanding of the phenotypic diversity of diffuse large b - cell lymphoma expands to encompass not only cell of origin , but also other biologically distinct categories based on genomic alterations.15 , 27 , 28 future trials that use such methods will be important to explore the mechanisms of action of investigational drugs and to redefine the groups in which they are most likely to be effective . 
the poor prognosis of double - hit lymphomas could be seen as a potential opportunity for such an approach . contributors pwmj and ad designed the study , oversaw the study , and contributed to data interpretation , writing and approval of the report . 
tec and gg contributed to data analysis , interpretation , writing of the report , and oversaw work at the southampton clinical trials unit ( southampton , uk )  . 
all authors have reviewed and approved the final version of the report . declaration of interests ad reports grants and personal fees from janssen , bayer , adc therapeutics , roche , celgene , acerta , gilead , and personal fees from kite and morphosys . 
gpc reports grants from celgene , amgen , pfizer , and celleron , and personal fees from takeda , roche , gilead , bristol - myers squibb , and merck sharpe and dohme . 
am reports personal fees from roche , celgene , novartis , bristol - myers squibb , merck sharpe and dohme , sandoz , gilead , janssen , amgen , and takeda , and grants and personal fees from pfizer . 
pwmj reports grants from janssen , bloodwise , and epizyme , and personal fees from takeda , bristol - myers squibb , novartis , celgene , boeringher ingelheim , kite pharmaceuticals , genmab , and incyte . 
individual participant data will be shared that underlie the results reported in this article , after vol 20 may 2019 articles de - identification and normalisation of information ( text , tables , figures , and appendices )  . 
anonymised data will be available beginning 3 months after and ending 5 years after publication of this article to researchers who provide a completed data sharing agreement that describes a methodologically sound proposal for the purpose of the approved proposal . 
data sharing requests are available for 5 years via the southampton clinical trials unit website . acknowledgments the trial was funded by an educational grant from janssen - cilag and endorsed by cancer research uk after independent peer review ( c328 / a12128 )  . 
cm and un are members of the swiss group for clinical cancer research , switzerland correction to lancet oncol 2019 ; 20 : 71927 katzenstein hm , langham mr , malogolowkin mh , et al . 
lancet oncol 2019 ; 20 : 71927 in the summary and methods of this article , the data cutoff date has been updated from dec 31 , 2017 , to june 30 , 2017 . 
we report the nal overall survival results of the trial . methods icon7 was an international , phase 3 , open - label , randomised trial undertaken at 263 centres in 11 countries across europe , canada , australia and new zealand . 
eligible adult women with newly diagnosed ovarian cancer that was either high - risk early - stage disease ( international federation of gynecology and obstetrics [ figo ] stage iiia , grade 3 or clear cell histology ) or more advanced disease ( figo stage iibiv ) , with an eastern cooperative oncology group performance status of 02 , were enrolled and randomly assigned in a 1 : 1 ratio to standard chemotherapy ( six 3 - weekly cycles of intravenous carboplatin [ auc 5 or 6 ] and paclitaxel 175 mg / m of body surface area ) or the same chemotherapy regimen plus bevacizumab 75 mg per kg bodyweight intravenously every 3 weeks , given concurrently and continued with up to 12 further 3 - weekly cycles of maintenance therapy . 
this trial is registered as an international standard randomised controlled trial , number isrctn91273375 . findings between dec 18 , 2006 , and feb 16 , 2009 , 1528 women were enrolled and randomly assigned to receive chemotherapy ( n = 764 ) or chemotherapy plus bevacizumab ( n = 764 )  . 
median follow - up at the end of the trial on march 31 , 2013 , was 489 months ( iqr 266562 ) , at which point 714 patients had died ( 352 in the chemotherapy group and 362 in the bevacizumab group )  . 
no overall survival bene t of bevacizumab was recorded ( restricted mean survival time 446 months [ 95% ci 432459 ] in the standard chemotherapy group vs 455 months [ 442467 ] in the bevacizumab group ; log - rank p = 085 )  . 
in an exploratory analysis of a prede ned subgroup of 502 patients with poor prognosis disease , 332 ( 66% ) died ( 174 in the standard chemotherapy group and 158 in the bevacizumab group ) , and a signi cant di erence in overall survival was noted between women who received bevacizumab plus chemotherapy and those who received chemotherapy alone ( restricted mean survival time 345 months [ 95% ci 320370 ] with standard chemotherapy vs 393 months [ 370417 ] with bevacizumab ; log - rank p = 003 )  . 
during extended follow - up , one further treatment - related grade 3 event ( gastrointestinal stula in a bevacizumab - treated patient ) , three grade 2 treatment - related events ( cardiac failure , sarcoidosis , and foot fracture , all in bevacizumab - treated patients ) , and one grade 1 treatment - related event ( vaginal haemorrhage , in a patient treated with standard chemotherapy ) were reported . interpretation bevacizumab , added to platinum - based chemotherapy , did not increase overall survival in the study population as a whole . 
similar progression - free survival ndings were reported in the gog - 218 trial . added value of this study in a planned mature analysis of overall survival , no di erence in overall survival was noted between those patients who received bevacizumab plus chemotherapy and those who received chemotherapy alone . 
however , in subgroup analyses , improved overall survival was noted in patients at high risk of disease progression who received bevacizumab compared with those who did not . implications of all the available evidence bevacizumab may have a role in the treatment of patients with poor - prognosis ovarian cancer . 
 introduction ovarian cancer is the seventh most common cancer worldwide , with 238 700 new cases and 151 900 deaths in 2012.1 the prognosis of the disease remains poor : the european mean age - standardised 5 - year survival was only 376% for women diagnosed between 2000 and 2007.2 until 2011 , the international standard of care for women with advanced or poor - prognosis early - stage ovarian cancer mainly consisted of debulking surgery followed by chemotherapy with carboplatin and paclitaxel.3 since then , modulation of vegf has moved from a theoretical concept4 to a key component of treatment . 
two large - scale phase 3 randomised trials , gog - 218 and icon7 , both undertaken in rst - line settings , showed that the addition of the anti - vegf monoclonal antibody , bevacizumab , to conventionally administered carboplatin and paclitaxel chemotherapy signi cantly improved progression - free survival.5 , 6 two further randomised trials in recurrent ovarian cancer have shown signi cant improvement in progression - free survival the addition of bevacizumab to conventionally administered carboplatin and gemcitabine chemotherapy both in the platinumsensitive and platinum - resistant relapsed setting.7 , 8 these data were used to support bevacizumab licensing through the european medicines agency for use in the rst - line setting for patients with at least international federation of gynecology and obstetrics ( figo ) stage iiib disease ( according to 1988 staging criteria ) , at rst recurrence for patients with platinum - sensitive disease not previously treated with bevacizumab or other vegf - targeted drugs , and in the setting of platinum - resistant recurrence topotecan , or pegylated combined with paclitaxel , liposomal doxorubicin.9 bevacizumab has also been approved in the platinum - refractory setting by the us food and drug administration.10 through the gog - 218 trial , 5 which enrolled 1873 patients with figo stage iiiiv ovarian cancer with macroscopic residual disease after primary surgery , showed a signi cant improvement in progression - free survival with the addition of bevacizumab ( hazard ratio [ hr ] 072 , 95% ci 063082 ; p < 0001 )  . 
patients received treatment with carboplatin and paclitaxel chemotherapy , and either concurrent bevacizumab 15 mg per kg every 3 weeks followed by up to 16 cycles of maintenance bevacizumab ( at the same dose ) or placebo for the same duration , all administered intravenously . 
the icon7 trial , 6 which was done in a patient population that included those with poor - prognosis , early - stage disease and those with optimally or suboptimally debulked advanced disease , showed improved progression - free survival in patients receiving bevacizumab , with restricted mean progressionfree survival over 36 months of 203 months on standard chemotherapy and 218 months with bevacizumab ( hr 081 , 95% ci 070094 ; p = 0004 )  . 
an increased e ect was noted in patients at high risk of disease progression , a similar group to the gog - 218 study population , with restricted mean progression - free survival after 42 months follow - up of 145 months in the standard chemotherapy group and 181 months in the bevacizumab group ( hr 073 , 95% ci 060093 ; p = 0002 )  . to fully assess a new treatment , the e ect on overall survival as well as progression - free survival must be known . 
at the time of the primary progression - free survival analysis , overall survival data were immature in both icon7 and gog - 218 , and preliminary analyses showed no di erence between treatment groups in either study . 
here , we present the nal analysis of mature overall survival data from icon7 , together with detailed data about the e ect of bevacizumab according to stage and extent of residual disease after primary debulking surgery . methods study design and participants the design of this trial has previously been described in detail.6 in brief , eligible women with ovarian cancer were recruited from 263 centres ( a mixture of general hospitals and specialist centres ) in 11 countries across europe , canada , australia , and new zealand ( appendix pp 15 ) and were randomly assigned 1 : 1 in an open - label study to receive standard chemotherapy or standard chemo therapy with bevacizumab . 
eligible patients were aged 18 years or vol 16 august 2015 articles 1528 women enrolled from 263 sites in 11 countries 764 randomly assigned to receive standard chemotherapy 764 randomly assigned to receive standard chemotherapy plus bevacizumab 30 withdrew consent before disease progression 12 died before progression 208 * did not progress 514 progressed further treatment during follow - up : 62 none 266 one line 186 two or more lines 41 received bevacizumab 340 died after progression 22 withdrew consent before disease progression 12 died before progression 188 did not progress 542 progressed further treatment during follow - up : 81 none 269 one line 192 two or more lines 25 received further bevacizumab 350 died after progression figure 1 : trial pro le * includes 16 patients last seen more than 6 months before the end of the study . 
 includes 11 patients last seen more than 6 months before the end of the study . older ; with newly diagnosed epithelial ovarian , fallopian tube , or primary peritoneal cancer ; an eastern cooperative oncology group ( ecog ) performance status of 02 ; figo 1988 stage iibiv or high - risk ( grade 3 or clear cell histology ) stage iiia disease ; had undergone debulking cytoreductive surgery or , in advanced disease , had a biopsy with no further surgery planned ; and had adequate coagulation parameters and liver , renal , and bone marrow function . 
the exclusion criteria were having other tumour types , previous systemic therapy , planned surgery , and uncontrolled hypertension . the study protocol was compliant with good clinical practice guidelines and the declaration of helsinki . 
 and where required all patients provided written informed consent . randomisation and masking randomisation was done centrally by a computer system based at the medical research council clinical trials unit ( london , uk ) accessed via the web or telephone . 
 randomisation was done using 1 : 1 allocation and a minimisation algorithm , and was strati ed by gynecologic cancer intergroup ( gcig ) group , a combination of figo stage and residual disease ( stage iiii and 1 cm residual disease vs stage iiii and > 1 cm residual disease vs inoperable stage iii and stage iv disease ) and planned interval between surgery and chemo therapy ( 4 weeks or > 4 weeks )  . 
neither patients nor physicians were masked to treatment allocation . procedures patients received either six 3 - weekly cycles of intravenous carboplatin ( auc 5 or 6 ) and paclitaxel ( 175 mg / m of body surface area ) , or the same regimen with intravenous ( 75 mg / kg of bodyweight ) given bevacizumab concurrently and continued for 12 further 3 - weekly cycles ( with a duration of bevacizumab exposure of about 1 year ) , or until disease progression . 
quality of life was assessed with the european organisation for research and treatment of cancer qlq - c30 and qlq - ov28 questionnaires . outcomes the primary outcome of icon7 was progression - free survival , which has been previously reported.6 secondary outcomes were overall survival and safety outcomes of adverse events , laboratory results , and worsened ecog performance status . 
exploratory outcome measures were quality of life , health economics , and translational research . risk groups were de ned at the time of the primary progression - free survival analysis to enable comparison with the gog - 218 study population . 
high risk of progression was de ned as stage iv disease , inoperable stage iii disease , or suboptimally debulked ( > 1 cm ) stage iii disease ( appendix p 10 )  . 
to enable comparison with previous analyses , results are also presented for two other high - risk de nitions : exclusion of inoperable stage iiiiv patients , to match the previous icon7 high - risk group ; and inclusion of patients with 01 cm residual tumour , to match the gog - 218 population ( appendix p 8 )  . 
between the primary progression - free survival analysis and the present analysis , recruiting centres were asked ( following the gcig fourth ovarian cancer consensus conference statement3 ) to reclassify patients with up to 1 cm of residual disease into those with no macroscopic residuum or those with macroscopic residuum measuring 1 cm or less . 
the non - high - risk patients were de ned as those who did not meet the criteria for high - risk disease . 930 vol 16 august 2015 articles three further patient subgroups of particular interest were de ned : patients with clear cell carcinoma ( roughly 10% of patients because of enriched enrolmentie , the use of less restrictive staging criteria , which meant that patients with clear cell carcinoma of any stage were eligible ) ; high - risk low - stage patients , with stage iiia clear cell or grade 3 carcinoma ; and low - grade serous carcinomas ( grade 1 )  . statistical analysis this study was designed and powered to detect di erences in progression - free and overall survival between the treatment groups . 
the analysis of overall survival needed 715 deaths to detect a 10 - month improvement in median survival from 43 to 53 months ( hr 081 ) , with 80% power at a two - sided 5% signi cance level . 
the progression - free survival analysis needed 684 disease progression events to show a 5 - month progression - free survival increase from 18 to 23 months , with 90% power and two - sided 5% signi cance level . analysis followed the principle of intention - to - treat and included all patients randomly assigned to treatment . 
 with evidence of non - proportionality , exible parametric survival models12 were used to smooth survival curves and estimate survival di erences during a 5 - year period , which is the approximate follow - up if patients were enrolled midway through the recruitment period and remained in follow - up at the study end . 
adc and ae had full access to all the raw data , and adc had nal responsibility for the decision to submit for publication . results between dec 18 , 2006 , and feb 16 , 2009 , seven gcig groups recruited 1528 women with ovarian cancer from 263 centres across europe , canada , australia , and new zealand ; these women were enrolled and randomly assigned to receive standard carboplatin and paclitaxel chemotherapy ( n = 764 ) or standard chemo therapy plus bevacizumab ( n = 764 ; gure 1 )  . 
 table 1 : primary analysis of overall survival and updated analysis of progression - free survival vol 16 august 2015 articles bevacizumab standard chemotherapy bevacizumabstandard chemotherapy kaplan - meier dierence smoothed dierence 95% ci , smoothed 12 24 36 36 number at risk bevacizumab standard chemotherapy 764 764 738 707 725 676 618 578 502 476 401 397 10 100 100 36 12 24 36 months since randomisation months since randomisation number at risk bevacizumab standard chemotherapy 248 238 224 254 238 208 180 156 135 101 figure 2 : overall survival ( a ) overall survival in all patients . 
patient baseline characteristics are summarised in appendix p 8 ; the median age of the patients was 57 years ( iqr 5064 ) ; 1415 ( 94% ) of 1501 ( excluding those with unknown performance status ) had an ecog performance status of 0 or 1 ; 1340 ( 89% ) of 1502 ( excluding those with cancer originating from multiple sites ) had cancer of ovarian origin ; 1054 ( 69% ) had disease of serous histology ; 175 ( 11% ) had figo stage iii , iiia , or iiib disease , and 1071 ( 70% ) stage iiic or iv disease . 
 following primary surgery , 395 ( 26% ) patients had residual disease larger than 1 cm , 369 ( 24% ) had visible disease up to 1 cm in diameter , and 734 ( 48% ) had no visible residual disease . 
median follow - up was 486 months ( iqr 243560 ) in the standard chemotherapy group and 488 months ( 282564 ) in the bevacizumab group , with shorter follow - up durations of 290 months ( 141507 ) and 389 months ( 211525 ) , respectively , for high - risk patients . the patient subgroup at high risk of progression consisted of 502 ( 33% ) of 1528 patients . 
their median age was 60 years ( iqr 5266 ) and 60 ( 12% ) had cancer of primary peritoneal origin ( compared with 106 [ 7% ] of all enrolled patients overall )  . 
most of the high - risk patients ( 381 [ 76% ] ) had serous - type ovarian cancer , and the group included 30 ( 6% ) patients who did not undergo debulking surgery . those ( 47% ) of in total , 714 patients ( 47% ) died during the study : 352 ( 46% ) of those in the chemotherapy group and 362 the chemotherapy plus bevacizumab group ( table 1 )  . 
the di erence in overall survival between randomised groups was neither clinically nor statistically signi cant ( log - rank test p = 085 ) , although non - proportionality was evident ( p = 002 )  . 
over time , the largest absolute di erence in survival was less than 5% , occurring around 2 years after enrolment and favouring patients who received bevacizumab ( gure 2b )  . 
restricted mean survival was 446 months ( 95% ci 432459 ) for women in the chemotherapy group and 455 months ( 442467 ) in the chemotherapy plus bevacizumab group ( table 1 )  . of the 502 high - risk patients , 332 ( 66% ) died , including 174 ( 69% ) of 254 in the chemotherapy group and 158 ( 54% ) 932 vol 16 august 2015 articles of 248 in the bevacizumab group ( table 1 )  . 
evidence suggested longer overall survival in those who had received bevacizumab ( p = 003 , gure 2c ) but evidence of non - proportional hazards ( p = 001 ) meant that the hazard ratio was di cult to interpret . 
restricted mean overall survival time was 393 months ( 95% ci 370417 ) for the bevacizumab group and 345 months ( 320370 ) for the chemotherapy group ( log - rank p = 003 ; table 1 )  . 
the absolute di erence in survival exceeded 10% after 2 years , and remained at 44% ( 95% ci 41 to 129 ) at 5 years ( gure 2d )  . 
similar patterns were also noted for progression - free survival ( p = 0014 for stage , p = 0005 for high risk ; appendix p 12 )  . no bene t of bevacizumab was reported for other prede ned poor - prognosis tumour types ( table 2 )  . 
some baseline imbalance was recorded within subgroups , which is most likely a consequence of small numbers and is unlikely to have a ected the results ( appendix p 9 )  . 
 the mortality rate in all three subgroups was lower than in the overall trial population , especially in patients with low - stage high - grade disease ( table 2 )  . 
no evidence of di erence between treatment groups was recorded within these subgroups ( table 2 )  . in our extension of the previously reported quality - oflife analysis , now including data up to the prede ned timepoint of week 76 , in patients without disease progression , global quality of life did not di er between those who received standard chemotherapy and those receiving bevacizumab at week 76 ( p = 043 , appendix p 9 )  . 
 table 2 : overall survival in prede ned subgroups vol 16 august 2015 articles and bene t insigni cant small ( + 43 points , 95% ci 49 to 134 ; p = 036 ) relative to patients not receiving bevacizumab was noted in high - risk patients . 
a sensitivity analysis of missing data suggested that these ndings were robust ( appendix p 9 )  . the primary analysis of progression - free survival was previously reported when 759 patients had experienced disease progression or died ( 392 in the standard chemotherapy group and 367 in the bevacizumab group ) .6 since these primary analyses , a further 321 patients have subsequently progressed or died without progression ( 134 in the standard chemotherapy group and 187 in the bevacizumab group ) for a total of 1080 progression events or deaths . 
however , in highrisk patients , a signi cant bene t remains ( p = 0001 ) with strong evidence of non - proportional hazards ( p < 00001 ) , and longer mean restricted progressionfree survival in the bevacizumab group than in the chemotherapy group ( table 1 )  . most adverse events that occurred in the trial have been previously reported : bevacizumab was associated with an increase in grade 12 mucocutaneous bleeding ( 271 [ 36% ] patients in the bevacizumab group vs 55 [ 7% ] patients in the standard chemotherapy group ) , grade 2 or worse hypertension ( 136 [ 18% ] vs 16 [ 2% ] ) , grade 3 or worse thromboembolic events ( 51 [ 7% ] vs 23 [ 3% ] ) , and grade 3 or worse gastrointestinal perforations ( ten [ 1% ] vs three [ < 1% ] ) .6 during extended follow - up of overall survival , one further treatment - related grade 3 event in a bevacizumab - treated ( gastrointestinal stula patient ) , three grade 2 treatment - related events ( cardiac failure , sarcoidosis , and foot fracture , all in bevacizumabtreated patients ) , and one grade 1 treatment - related event ( vaginal haemorrhage , in a patient treated with standard chemotherapy ) were also reported . the treatment groups was not discussion the results of icon7 show that bevacizumab did not intention - to - treat improve overall survival population of women randomly assigned to receive it in conjunction with chemotherapy , although heterogeneity of bene t was observed dependent on residual disease burden before treatment . 
although the overall di erence statistically between signi cant , non - proportionality was recorded , despite the fact that the magnitude of the change over time was not clinically meaningful . 
however , in a preplanned analysis , women at high risk of disease progression had a signi cant improvement in overall survival with the addition of bevacizumab to standard chemotherapy . 
 a similar improvement in overall survival was also reported in high - risk patients ( > 1 cm residual tumour ) in gog - 218 ( hr 073 in icon7 , hr 086 in gog - 218 ) , with some di erences as expected because of varying treatment strategies , post - progression in particular greater use of bevacizumab ( ie , more participants receiving the drug ) in gog - 218 patients . 
these ndings are relevant since , in practice , bevacizumab use has become focused on the high - risk patient group . in addition to the contrast between high - risk and nonhigh - risk patients , there was a clear association between increasing disease severity and a stronger bene cial e ect of bevacizumab ( gure 3 )  . 
these observations provide a clinical framework for the appropriate use of bevacizumab in ovarian cancer that is consistent with the biological requirement for angiogenesis in growing tumours , and a hypothetical framework to explain this e ect biologically . 
other trials in ovarian cancer have also reported an overt bene t in women with a measurable following recurrence , in both platinum - sensitive7 and platinumresistant settings.8 its e ect on to exert ( higher ) burden disease the debulked suboptimally these nal results complement the ndings of the earlier primary progression - free survival analysis , 6 with a in women with bene t of bevacizumab recorded advanced - stage disease . 
the primary progression - free survival analyses also showed similar outcomes in gog - 218 patients and the high - risk patient group of icon7.5 , 6 the updated progression - free survival analysis reported here showed a reduced overall e ect , with greater elapsed treatment with time bevacizumab , but the earlier results remain the primary pre - speci ed analysis . from our data also identify patients who might not bene t from bevacizumab in the rst - line setting . 
women with early - stage ( figo stage i / ii ) disease , even if judged to be high risk on the basis of grade or clear cell histology , do not seem to bene t . 
it also included 30 patients in whom primary , and subsequent , debulking surgery was regarded as unlikely to be in the patients best interests . three subgroups based on tumour type were also prede ned : clear cell , low - grade serous , and high - risk low - stage cancer . 
this histology was previously thought to confer a substantially worse outcome than other tumour subtypes but these patients did surprisingly well in our trial , with a 72% survival 934 vol 16 august 2015 articles after a median of 51 months follow - up , with no bene t from bevacizumab . 
patients with low - grade serous cancer also did not bene t from the addition of bevacizumab , although a major limitation of this assessment is the absence of central pathology review for these tumours . 
for all three subgroup analyses , the numbers of patients were small and statistical power to detect di erences was low . to re ect on the choice of outcome measures for the icon7 trial is pertinent . 
to assess this outcome measure needed a further 3 years of followup after the primary progression - free survival analysis , but also simpli ed aspects of trial design , such as placebo control and independent masked radiology review , which are essential when progression - free survival is the only outcome measure . 
the primary analysis in 2011 showed a signi cant progression - free survival bene t in the intention - to - treat population , which was most pronounced in women at high risk of progression.6 over time , the e ect closely followed bevacizumab treatment , with the maximum bene t coinciding precisely with duration of treatment ( appendix p 11 )  . 
notably , the overall survival di erence outlasts the duration of bevacizumab exposure and points to a durable bene t in the high - risk group ( gure 2d ) , raising the possibility of additional bene t to high - risk patients from further extension of treatment duration , which is the subject of ongoing research in the ( nct01462890 )  . 
following disease boost progression in icon7 , the pattern of further treatment was similar in both randomised groups , with little use of further bevacizumab in either group . trial questions about the optimum timing of bevacizumab therapy in the trajectory of a womans disease rema should it be considered at initial presentation , time of platinum - sensitive recurrence , or after the development of platinum resistance ? bevacizumab has shown a signi cant progression - free survival bene t in all these settings , 58 and an overall survival bene t in some settings too.6 , 13 , 14 our data strongly support early use of bevacizumab , based on risk and disease burden . 
whether or not bevacizumab can be used beyond progression in this indication , and whether or not treatment can be repeated , remains an intriguing question that is being addressed in the mito16mango2b trial ( nct01802749 ) ; with studies in colorectal cancer15 and breast cancer16 having already provided evidence of bene t . from a societal perspective , there are strong and sometimes opposing views about the costs and cost bene t ratio of bevacizumab . 
the jgog - 316 trial17 reported a similar overall survival bene t without bevacizumab from the use of weekly paclitaxel , whereas gog - 26218 suggests that the e ect of bevacizumab may be attenuated by such a strategy . 
interestingly , the small reduction in quality of life associated with bevacizumab that was reported after 54 weeks19 was smaller still by week 76 and was not statistically signi cant . 
the ability to predict which patients will bene t most is clearly important and could have the power to change the cost - e ectiveness of treatment substantially by not treating patients with little chance of bene t . 
collinson and colleagues20 and backen and colleagues21 have presented biomarker strategies with potentially predictive approaches , whereas gourley and colleagues22 have reported that bevacizumab might disadvantage women with an immunologically active subtype and winterho and coworkers have reported bene t for women with mesenchymal - subtype disease.23 these ndings all need to be validated in independent datasets . the addition of bevacizumab to chemotherapy is an important step forward in integrating biological agents with conventional chemotherapy in ovarian cancer . 
future studies will re ne important questions of biological prediction , duration , and rechallenge . contributors amo , tjp , mkbp , ams , gcj ( translational research ) , and ds ( quality of life ) led and coordinated the study design . 
tjp has received personal fees from novartis and astrazeneca outside the submitted work , and has received other fees from several other pharmaceutical companies and research organisations in connection with the costs of running a broad research portfolio , outside the submitted work . 
amo , jp , ae , jal , gk , msc , mrm , mp , ap , ds , ams , and lf declare no competing interests . acknowledgments we thank the women who participated in the trial and their families . 
roche also undertook regulatory ling of bevacizumab with progression - free survival data , leading to its widespread international use . vol 16 august 2015 articles correction to lancet oncol 2018 ; 19 : 95364 correction to lancet oncol 2018 ; 19 : 104050 correction to lancet oncol 2018 ; 19 : e386 kramer souweidane mm , pandit - taskar n , et al . 
this correction has been made to the printed article , and to the online version as of aug 1 , 2018 . moreau p , mateos m - v , berenson jr , et al . 
lancet oncol 2018 ; 19 : 95364in the methods section of this article , the exclusion criteria for new york heart association heart failure should have been class iii or iv . 
this correction has been made to the online version as of aug 1 , 2018 . vol 19 aug 2018 e382 corrections editorial for more on the bbc report see health - 27894551 for the monitor report see government / publications / closing - the - nhs - funding - gaphow - to - get - better - valuehealthcare - for - patients for the times letter see letters / article4140238.ece nhs privatisation : a step too far according to a recent bbc report , englands national health service ( nhs ) will face a funding shortfall of about 2 billion by 2016 . 
projections in a report by monitor , the sector regulator for health - care services in england , suggest this de cit will rise to around 30 billion by 2021 . 
the e ect that this de cit will have on the nhs has not gone unnoticed : a letter to the times on july 7 , 2014 , signed by leaders from various royal colleges , stated that unless plans for meeting funding gaps were created , the nhs would be unable to cope . 
 clearly , urgent measures need to be taken if the nhs is to continue to be able to provide its mandated services , but worryingly the debate is increasingly looking to privatisation as a means of plugging these funding gaps . 
 this insidious slide towards outsourcing health care is not only a lazy , short - term solution to the immediate problems facing the nhs , but also potentially highly damaging to the provision of health care in the uk . 
 current tenders include catering or provision of health care in prisons ; however , a recent tender proposal by four general practitioner clinical commissioning groups ( ccgs ) in sta ordshire and stoke would see external contractors manage entire clinical cancer - care pathways for patients with bladder , lung , prostate , and breast cancer . 
the proposed removal of an entire care pathway to the private sector is a concerning development , partly because further dismantling of the nhs , and partly because it is indicative of how little thought has gone into the consequences . 
presumably , the contractor will not be expected to run departments peripherally involved in cancer care , or to invest in all of the attendant technologies , and , since the tender is only for 10 years , there would be little nancial incentive to do so . 
these measures will erode the nhs , leading to a failure to invest in sta ng and long - term infrastructureas seen in other sectors that have undergone partial privatisation . 
this scenario will become particularly acute over successive tenders , and especially damaging if winning bids are chosen predominantly on nancial grounds , or if a contractor fails and the government has to step in to handle the costly repercussions . 
for example , if care is outsourced only for patients with speci c types of cancer , what happens to those patients if metastases , comorbidities , or other complications arise ? individual patients risk being caught in a mixed - care model between private and public services for di erent aspects of their treatment , which could lead to disjointed care and unclear accountability . 
it would be unrealistic to not consider some elements of privatisationeg , discrete parts of the nhs that service clinical pathways , and where centralisation could improve consistency and quality . 
but to try to excise an entire clinical care pathway that has several links to other parts of the nhs is an ill - considered x to a complex issue , and will ultimately not serve those for whom the nhs was rst created . 
 the lancet oncology vol 15 august 2014 peri - operative chemotherapy with or without bevacizumab in operable oesophagogastric adenocarcinoma ( uk medical research council st03 ) : primary analysis results of a multicentre , open - label , randomised phase 23 trial david cunningham , sally p stenning , elizabeth c smyth , alicia f okines , william h allum , sam rowley , laura stevenson , heike i grabsch , derek alderson , thomas crosby , s michael griffin , wasat mansoor , fareeda y coxon , stephen j falk , suzanne darby , kate a sumpter , jane m blazeby , ruth e langley summary background peri - operative chemotherapy and surgery is a standard of care for patients with resectable oesophagogastric adenocarcinoma . 
 methods in this multicentre , randomised , open - label phase 23 trial , we recruited patients aged 18 years and older with histologically proven , resectable oesophagogastric adenocarcinoma from 87 uk hospitals and cancer centres . 
patients in the control group ( chemotherapy alone ) received three pre - operative and three post - operative cycles of epirubicin , cisplatin , and capecitabine chemotherapy : 50 mg / m epirubicin and 60 mg / m cisplatin on day 1 and 1250 mg / m oral capecitabine on days 121 . 
patients in the investigational group received the same treatment as the control group plus 75 mg / kg intravenous bevacizumab on day 1 of every cycle of chemotherapy and for six further doses once every 21 days following chemotherapy , as maintenance treatment . 
randomisation was done by means of a telephone call to the medical research council clinical trials unit , where staff used a computer programme that implemented a minimisation algorithm with a random element to establish the allocation for the patient at the point of randomisation . 
the primary outcome for the phase 3 stage of the trial was overall survival ( defined as the time from randomisation until death from any cause ) , analysed in the intention - to - treat population . 
 findings between oct 31 , 2007 , and march 25 , 2014 , 1063 patients were enrolled and randomly assigned to receive chemotherapy alone ( n = 533 ) or chemotherapy plus bevacizumab ( n = 530 )  . 
3 - year overall survival was 503% ( 95% ci 455549 ) in the chemotherapy alone group and 481% ( 432527 ) in the chemotherapy plus bevacizumab group ( hazard ratio [ hr ] 108 , 95% ci 091129 ; p = 036 )  . 
wound healing complications were more prevalent in the bevacizumab group , occurring in 53 ( 12% ) patients in this group compared with 33 ( 7% ) patients in the chemotherapy alone group . 
in patients who underwent oesophagogastrectomy , post - operative anastomotic leak rates were higher in the chemotherapy plus bevacizumab group ( 23 [ 10% ] of 233 in the chemotherapy alone group vs 52 [ 24% ] of 220 in the chemotherapy plus bevacizumab group ) ; therefore , recruitment of patients with lower oesophageal or junctional tumours planned for an oesophagogastric resection was stopped towards the end of the trial . 
serious adverse events for all patients included anastomotic leaks ( 30 events in chemotherapy alone group vs 69 in the chemotherapy plus bevacizumab group ) , and infections with normal neutrophil count ( 42 events vs 53 )  . interpretation the results of this trial do not provide any evidence for the use of bevacizumab in combination with peri - operative epiribicin , cisplatin , and capecitabine chemotherapy for patients with resectable gastric , oesophagogastric junction , or lower oesophageal adenocarcinoma . 
 despite this increase in survival , mortality in patients with this disease remains high , with 5 - year overall survival for localised disease at diagnosis of only about 40%.3 , 4 bevacizumab , a monoclonal antibody that targets vegf , improves responses to chemotherapy and progressionfree survival , but not overall survival , in patients with advanced gastric cancer.5 , 6 in oesophagogastric cancer , a complete surgical resection ( r0 resection ) is an important predictor of long - term survival.7 we postulated that a higher proportion of patients responding to pre - operative chemotherapy would increase the likelihood of an r0 resection and lead to improved survival outcomes.8 therefore , we designed st03 as a phase 23 trial to assess the safety and efficacy of adding bevacizumab to perioperative chemotherapy for patients with resectable oesophagogastric cancer . the initial phase 2 stage of the trial focused on safety and feasibility in the first 200 patients ; these results have been reported previously.9 the addition of bevacizumab was feasible and did not seem to significantly increase toxic effects or the likelihood or severity of surgical complications . 
therefore , the study proceeded to the phase 3 stage . methods study design and participants we recruited patients aged 18 years and older with previously untreated , histologically proven , resectable junction adenocarcinoma of the lower oesophagus , oesophagogastric junction , or stomach from 87 uk hospitals and cancer centres . 
to be eligible , patients were required to have a who performance status of 0 or 1 and adequate cardiac , liver , renal , and bone marrow function to be eligible . 
in 2006 , the magic trial showed an improvement in progression - free survival and overall survival when peri - operative chemotherapy was given in addition to surgery , compared with surgery alone , in patients with resectable oesophagogastric adenocarcinoma . 
in 2011 , the avagast trial in advanced gastric cancer reported an improvement in tumour response and progression - free survival , but not overall survival , when bevacizumab was combined with chemotherapy . added value of this study to the best of our knowledge , this trial is the first study in which bevacizumab was given to patients with resectable oesophagogastric adenocarcinoma in the peri - operative setting ; the results provide no evidence of a benefit of bevacizumab administration in combination with peri - operative chemotherapy in these patients . 
moreover , the safety results indicate that bevacizumab administration might also be associated with impaired wound healing . implications of all the available evidence the results of this trial suggest that there is unlikely to be a role for bevacizumab in the treatment of localised , operable oesophagogastric cancer . 
every participating centre obtained local approvals . cisplatin , epiribicin , peri - operative randomisation and masking eligible patients were randomly assigned ( 1 : 1 ) to receive either and capecitabine chemotherapy or epiribicin , cisplatin , and capecitabine plus bevacizumab , in addition to surgery . 
 treatment allocation was done via a telephone call to the medical research council clinical trials unit at university college london ( normally by the research nurse at the site who was responsible for following up the patient ) , where trial management staff used a computer programme that implemented a minimisation algorithm with a random element and stratification by chemo therapy centre , site of tumour ( lower oesophagus vs oesophagogastric junction type i vs type ii vs type iii vs stomach ) , and tumour stage ( according to tnm 6th edition )  . 
 patients and investigators were not masked to treatment allocation . procedures epirubicin , cisplatin , and capecitabine chemotherapy was given as three pre - operative and three post - operative 21 - day cycles , consisting of 50 mg / m intravenous epirubicin and 60 mg / m cisplatin on day 1 and 1250 mg / m oral capecitabine on days 121 . 
patients in the chemotherapy plus bevacizumab group were given 75 mg / kg bevacizumab as a continuous intravenous infusion on day 1 of each of the chemotherapy cycles ( either before or after the chemotherapy was given )  . 
to maximise any potential treatment effect with an acceptable toxicity profile , patients in the bevacizumab group also received six further infusions of bevacizumab alone ( 75 mg / kg intravenously alone every 21 days ) as maintenance treatment after post - operative chemotherapy . no bevacizumab dose reductions were allowed . 
 bevacizumab was discontinued in the event of any new case of gastrointestinal perforation , arterial thromboembolic events ( including transient ischaemic attack , stroke , myocardial infarction , or new diagnosis of ischaemic heart disease ) , grade 3 or 4 haemorrhage , grade 3 or 4 congestive heart failure or left ventricular dysfunction , grade 4 hypertension , grade 4 proteinuria , tracheoesophageal fistula at any grade or any other fistula deemed to be possibly related to bevacizumab . 
all serious adverse events were reviewed for categorisation and severity by the chief investigator ( dc ) or trial physicians ( ecs , afo )  . surgery was scheduled 56 weeks after the last day of the final pre - operative chemotherapy cycle ; therefore , there were at least 8 weeks between the last pre - operative bevacizumab administration and surgery . 
surgical procedures were specified as follows ; for gastric or siewert type iii oesophagogastric junction tumours either proximal , total , or distal subtotal gastrectomy was recommended with a lymphadenectomy to include as a minimum lymph node stations 17 to ensure at least 15 nodes were excised ; for siewert type ii oesophagogastric junction tumours , either extended gastrectomy or two - field two - phase oesophago - gastrectomy with a lymph adenectomy ; for siewert type i oesophagogastric junction or lower oesophageal tumours , oesophagogastrectomy with either a two phase right thoracoabdominal approach or a left thoracoabdominal approach with a two field lymphadenectomy . 
minimal access procedures were allowed only in centres that had sufficient experience ( at least 20 such procedures done ) after review of outcomes and complication rates by surgeons from the trial management group . 
pathological evaluation of resected tumour specimens followed guidance that was compliant with the royal college of pathologists dataset for oesophagogastric cancer resections . we assessed to pre - operative tumour response chemotherapy with response evaluation criteria in solid tumors ( recist ) criteria ( version 1.0 ; assessed by ct scan , with laparoscopy , endoscopic ultrasound , or pet scans if clinically indicated ) and post - operatively at each centre by pathologists who assessed the resected tumour specimen to establish the extent of resection , margin involvement , extent of lymph node dissection , and mandard tumour regression grade . 
resections were judged to be curative ( r0 ) if the pathologist considered a radical resection had been undertaken and there was no evidence of microscopic residual disease with longitudinal margins ( proximal and distal ) microscopically clear and there were no viable tumour cells present within 1 mm of the oesophageal circumferential resection margins . 
cause of death and disease vol 18 march 2017 articles progression events were reported according to local investigator assessment . analysis of quality of life will be presented in a separate publication . 
 we assessed quality - of - life data with the european organisation for research and treatment of cancer ( eortc ) qlq - c30 and sto22 questionnaires , administered before and after post - operative chemo therapy and twice during the maintenance phase , then every 6 months post - surgery for 3 years and annually thereafter . 
 epiribicin , cisplatin , and capecitabine chemotherapy alone ( n = 533 ) epiribicin , cisplatin , and capecitabine chemotherapy plus bevacizumab ( n = 530 ) 425 ( 80% ) 108 ( 20% ) 434 ( 82% ) 96 ( 18% ) women age ( years ) median ( iqr ) ; range 63 ( 5668 ) ; 3179 64 ( 5669 ) ; 2882 we assessed cardiac function by echocardiogram or multiple gated acquisition scan at baseline and after preoperative and post - operative chemotherapy . 
in february , 2010 , a protocol amendment mandated a nadir neutrophil count on day 10 of the first pre - operative chemotherapy cycle with granulocyte colony stimulating factor ( gcsf ) recommended for all cases of grade 4 neutropenia , and at the investigators discretion for grade 3 cases , during all subsequent chemotherapy cycles . outcomes for the phase 3 analysis , the primary outcome measure from was overall survival defined as randomisation until death . 
stage 4a patients : t2 n1 m1a ( one in the chemotherapy alone group ) ; t3 n0n1 m1a ( two in the chemotherapy alone group and one in the chemotherapy plus bevacizumab group )  . 
these patients were randomly assigned after the inclusion of type ii oesophagogastric junction tumours but before oesophageal tumour staging was added to case report forms and were therefore staged under the gastric staging systestage 4 patients : all t4 n1n2 m0 . ( table 1 continues on next column ) table 1 : baseline characteristics 360 vol 18 march 2017 articles and curative ( r0 ) resection rates . 
all efficacy analyses were done on an intention - to - treat basis . disease - free survival was measured from a landmark point , taken to be 6 months from randomisation to allow for any difference in timing of surgery across all patients , to the first occurrence of disease recurrence or death . 
 patients who had an event before the landmark point and those who had a macroscopically incomplete ( r2 ) resection or no resection were deemed to have had a disease - free survival event at time zero . 
progression - free survival was measured from randomisation to the first occurrence of disease recurrence or death ; unlike disease - free survival , an r2 resection was not considered an event for this outcome measure . 
for the analysis of pathological tumour response , a mandard tumour regression grade of 1 , 2 , or 3 was considered a response and in the intentionto - treat comparison those who did not undergo a resection were included as non - responders . 
 sensitivity analysis of overall survival was repeated on the following pre - defined baseline subgroups : age ( < 60 years ; 6070 years ; > 70 years ) ; sex ; who performance status ; baseline tumour site ; baseline tumour stage ( separately for gastric / type iii oesophagogastric junction tumours and type i / ii oesophagogastric junction / lower oesophageal tumours )  . 
we did not do an analysis by the type of surgery because this was not known at baseline ; instead we analysed tumour site as a baseline surrogate for this variable . statistical analysis 5 - year overall survival in the epiribicin , cisplatin , and capecitabine chemotherapy alone group was estimated to be 40% . 
this estimate was based on the proportion of patients in the peri - operative chemotherapy group of the magic trial who were alive at 5 years ( 36% ) , 1 taking into consideration the possible effect of improvements in surgical technique , staging , and supportive care over time . 
a 10% improvement in survival would have been consistent with the benefit seen when adding bevacizumab in other settings at the time the trial was designed.10 to detect an absolute 10% improvement in 5 - year survival ( corresponding hazard ratio [ hr ] 076 ) , with 80% power and a two - sided 5% significance level , 420 deaths were required . 
on the assumption that the trial would take 34 years to complete recruitment , with 1824 months follow - up , the target sample size was estimated to be between 900 and 1100 patients . 
the accumulating data were monitored by an independent data monitoring committee ( idmc ) , which met 13 times between may , 2008 , and november , 2014 , to review safety data and efficacy analyses . 
analyses of overall survival , disease - free survival , and progression - free survival were based on all randomly assigned patients , whereas analysis of overall survival by resection status and mandard tumour regression grade were based on all randomly assigned patients with available pathological resection status and mandard 1063 patients recruited 533 randomly assigned to epirubicin , cisplatin , and capecitabine 530 randomly assigned to epirubicin , cisplatin , and capecitabine plus bevacizumab 4 did not start chemotherapy 1 ineligible 1 withdrew 2 straight to surgery 5 did not start chemotherapy 2 ineligible 2 withdrew 1 diagnosed with a colon lesion 529 started pre - operative chemotherapy 525 started pre - operative chemotherapy 472 completed three cycles 463 completed three cycles 73 had no resection 87 had no resection 21 found to be inoperable 10 died before surgery due 21 disease progression 2 comorbidity 2 patient refused surgery 8 other reasons 9 reason unknown 30 found to be inoperable 13 died before surgery due 16 disease progression 3 comorbidity 2 patient refused surgery 11 other reasons 12 reason unknown 457 underwent a resection 1 did not start pre - operative chemotherapy 438 underwent a resection 167 had no post - operative 181 had no post - operative chemotherapy 64 change in condition or not t 32 unacceptable toxicity 22 patient choice 15 died before due to start 12 post - operative complications 9 disease progression 8 incomplete resection 5 other or unknown reason chemotherapy 72 change in condition or not t 32 unacceptable toxicity 20 patient choice 15 died before due to start 18 post - operative complications 12 disease progression 5 incomplete resection 7 other or unknown reason 293 started post - operative chemotherapy 257 started post - operative chemotherapy 215 completed all three cycles 197 completed all three cycles 179 started maintenance dosing 119 received six doses 27 received ve doses 12 received four doses 8 received three doses 5 received two doses 8 received one dose figure 1 : trial profile vol 18 march 2017 articles tumour regression grade , respectively . 
 to compare the two groups in terms of the proportions of patients responding to chemotherapy and the proportions in whom curative resection was achieved , we used the test based on all randomly assigned patients who had available data from the relevant assessment . 
 results between oct 31 , 2007 , and march 25 , 2014 , 1063 patients to receive were enrolled and randomly assigned see online for appendix epirubicin , cisplatin , and capecitabine epirubicin , cisplatin , and capecitabine plus bevacizumab hr 108 in favour of the chemotherapy alone group , 95% ci 091129 ; log - rank p = 036 time from randomisation ( months ) 533 ( 11 ) 404 ( 52 ) 271 ( 85 ) 135 ( 59 ) 65 ( 31 ) 30 ( 20 ) 9 ( 8 ) 1 ( 0 ) 0 ( 0 ) 530 ( 11 ) 397 ( 52 ) 254 ( 69 ) 142 ( 71 ) 57 ( 27 ) 26 ( 12 ) 13 ( 13 ) 1 ( 0 ) 0 ( 0 ) number at risk ( number censored ) epirubicin , cisplatin , and capecitabine epirubicin , cisplatin , and capecitabine plus bevacizumab figure 2 : kaplan - meier plot of overall survival hr = hazard ratio . 
the median age of all enrolled patients was 63 years ( iqr 5668 ) , 859 ( 81% ) of 1063 patients were men , and 646 ( 61% ) had stage 3 or 4 disease ( according to tnm 6th edition )  . 
144 ( 14% ) had lower oesophageal tumours , 128 ( 12% ) siewert type i , 199 ( 19% ) siewert type ii , 209 ( 20% ) siewert type iii , and 383 ( 36% ) gastric . 
the proportion of patients undergoing pet scanning as part of staging has increased steadily during the course of the trial ( table 1 ) , but did not appear to differ between the groups . 
 1054 ( 99% ) of 1063 patients ( 529 in the chemotherapy alone group and 525 the chemotherapy plus bevacizumab group ) started chemotherapy after randomisation ( figure 1 )  . 
472 ( 89% ) of 529 patients in the chemotherapy group and 463 ( 88% ) of 525 in the chemo therapy plus bevacizumab group who started chemo therapy received all three pre - operative cycles . 
895 ( 84% ) of 1063 randomly assigned patients ( 457 [ 86% ] of 533 in the chemotherapy alone group vs 438 [ 83% ] of 530 in the chemotherapy plus bevacizumab group ) underwent a resection in the trial . 
 the median time from the start of the last pre - operative cycle to surgery was 62 days ( iqr 5668 ) in the chemotherapy alone group and 62 days ( 5769 ) in the chemotherapy plus bevacizumab group . 
293 ( 55% ) of 533 patients randomly assigned in the chemotherapy group and 257 ( 48% ) of 530 randomly assigned in the chemotherapy plus bevacizumab group re - commenced chemo therapy post - operatively ; 215 ( 73% ) of 293 patients in the chemotherapy group and 197 ( 77% ) of 257 patients in the chemotherapy and bevacizumab group received all three post - operative cycles ( figure 1 )  . 
of all randomly assigned patients , 212 ( 40% ) of 533 in the chemotherapy alone group and 195 ( 37% ) of 530 in the chemotherapy and bevacizumab group received all six scheduled cycles of chemotherapy . 
the appendix provides further details about pre - operative and postoperative chemotherapy , including numbers of patients who discontinued treatment or had dose reductions ( appendix pp 4 , 5 )  . 
 at the time of analysis , we used a reverse kaplan - meier method to calculate median follow - up , which was 384 months ( iqr 275508 ) in the whole population and 362 months ( 274514 ) in the chemotherapy alone group and 391 months ( 276505 ) in the chemotherapy and bevacizumab group . 
508 patients died ( 248 in the chemotherapy group and 260 in the chemotherapy and bevacizumab group ) and 85% of patients in each group 362 vol 18 march 2017 articles ( 451 of 533 given chemotherapy alone and 452 of 530 given chemotherapy and bevacizumab ) had either died or been followed up for at least 2 years . 
3 - year overall survival was similar in the two groups : 503% ( 95% ci 455549 ) in the chemotherapy alone group and 481% ( 432527 ) in the chemotherapy and bevacizumab group ( hr 109 in favour of the chemotherapy alone group , 95% ci 091129 ; log - rank p = 036 ; figure 2 )  . 
 insufficient patients ( n = 56 ) had reached the 5 - year timepoint at the time of analysis to give a reliable estimate of 5 - year overall survival . 
disease recurrence was confirmed in 210 and 192 patients , respectively ( 170 and 159 of whom subsequently died ) , with the remaining events attributable to death before reported recurrence ( 78 in the chemotherapy group and 101 in the chemotherapy plus bevacizumab group ) and a macro scopically incomplete resection ( 12 vs 10 )  . 
for progression - free survival , a macroscopically incomplete resection was not considered an event of interest , so the total number of events was therefore 288 in the chemotherapy alone group and 293 in the chemotherapy plus bevacizumab group . 
there was no evidence of a treatment effect of bevacizumab on either disease - free survival ( hr 104 , 95% ci 089122 ; p = 062 ) or progression - free survival ( hr 105 , 95% ci 089123 ; p = 056 )  . the analysis of recist responses to pre - operative chemotherapy ( partial or complete response vs stable disease , progressive disease , or death before tumour assessment ) is based on 875 patients ( 438 in the chemotherapy alone group and 437 in the chemotherapy plus bevacizumab group ) ; we excluded 188 patients ( 95 in the chemotherapy alone group and 93 the chemotherapy plus bevacizumab group ) with missing response data from the pre - operative tumour assessment . 
 the proportion of patients responding to treatment according to recist were similar in the two groups ( 183 [ 42% ] of 438 patients in the chemotherapy group vs 177 [ 41% ] of 437 in the chemo therapy and bevacizumab tumour group ; p = 070 )  . 
analysis of pathological responses based on mandard tumour regression grade ( grade 13 vs grade 45 or no resection ) includes 895 patients ( 452 chemotherapy alone , 443 chemotherapy plus bevacizumab ) ; those excluded are those who underwent a resection but had unavailable pathological tumour assessment data . 
the proportion of patients achieving pathological tumour responses were also similar between the groups ( 147 [ 33% ] of 452 patients in the chemotherapy alone group vs 135 [ 30% ] of 443 in the chemotherapy plus bevacizumab group ; p = 051 )  . 
percentages are based on all patients with non - missing data ; in the summary of lymph node dissection and mandard tumour regression grade , percentages are based on patients with non - missing data who underwent a resection only . 
includes those patients in which a viable tumour was present either at the circumferential margin or within 1 mm of the circumferential margin ( the above categories combined )  . 
resections were judged to be r0 by local pathologists in 321 ( 64% ) of 505 patients in the chemotherapy alone group and 305 ( 61% ) of 497 in the chemotherapy plus bevacizumab group ( p = 047 )  . 
when the comparison was repeated including only patients who underwent a resection ( r0 vs r1 ) , the proportions of r0 resections were again similar between the groups ( 321 [ 75% ] of 429 patients in the chemotherapy alone group vs 305 [ 75% ] of 405 in the chemotherapy plus bevacizumab group )  . 
 proportion of r0 resections varied by baseline tumour site ; gastric tumours had the highest proportion of r0 resections ( 265 [ 87% ] of 304 resections ) , compared with type iii oesophagogastric junction ( 117 [ 75% ] of 157 ) , type ii oesophagogastric junction ( 106 [ 72% ] of 148 ) , type i oesophagogastric junction ( 62 [ 61% ] of 102 ) , and lower oesophageal ( 76 [ 66% ] of 116 )  . 
circumferential margin involvement was only reported routinely by the pathologist for oesophagogastrectomies ; of 146 r1 oesophagogastrectomies , 72 ( 49% ) had a positive circumferential margin and 132 ( 90% ) were either at or within 1 mm of the circumferential margin . figure 3 shows the results of pre - defined baseline subgroup analyses for overall survival . 
in particular , in patients aged 70 years and older , significantly fewer patients who received chemo therapy alone died compared with those given chemo therapy plus bevacizumab ( figure 3 )  . 
however , in this subgroup , the proportion of deaths that were reported to be non - disease related was higher in the chemotherapy plus bevacizumab group than in the chemotherapy alone group ( 61 [ 30% ] patients given chemotherapy and bevacixumab vs seven [ 19% ] of 36 patients given chemotherapy alone )  . survival beyond the scheduled surgery timepoint assesed post - hoc was significantly longer in patients who had an r0 resection than in those with an r1 resection or no resection ( hr 023 , 95% ci 019028 ; p < 00001 ; figure 4 )  . 
our earlier comparison of the proportion of patients achieving a pathological tumour response categorised patients with a mandard tumour regression grade of 1 , 2 , or 3 as responders . 
however , our data suggest that those patients with a mandard tumour regression grade of 1 or 2 might represent a group with improved post - operative survival ( figure 5 )  . 
when such patients were compared with those with a mandard tumour regression grade of 3 , 4 , or 5 , or no resection post - hoc , post - operative survival was significantly better ( hr 030 , 95% ci 021044 ; p < 00001 ; figure 5 )  . the frequency and severity of adverse events occurring during either pre - operative or post - operative chemotherapy were similar between the groups ( table 3 , table 4 )  . 
neutropenia was the most common grade 3 or worse adverse event , both pre - operatively ( occurring in 145 [ 27% ] of 529 patients in the chemotherapy alone group vs 139 [ 26% ] of 525 patients in the chemotherapy plus bevacizumab group ) and post - operatively ( 95 [ 33% ] of 292 vs 81 [ 32% ] of 254 )  . 
this includes two fatal cases of 364 vol 18 march 2017 articles in the 257 patients infection with neutropenia , one in the chemotherapy in the chemotherapy plus alone group and one bevacizumab group . 
of the chemotherapy plus bevacizumab group who began post - operative chemotherapy , 179 ( 69% ) went on to receive maintenance bevacizumab and 16 ( 9% ) of these 179 patients reported a grade 3 or 4 toxicity during maintenance treatment , the most common of which were neutropenia ( four patients ) , anorexia ( 3 patients ) and lethargy ( 3 patients )  . 
the most commonly reported serious adverse events were gastrointestinal ( 60 events in the chemotherapy alone group vs 63 in the chemotherapy plus bevacizumab group ) , anastomotic leaks ( 30 events vs 69 ) , and infections with normal neutrophil count ( 42 events vs 53 )  . 
causes of death were reported to be mainly disease - related the ( 204 chemotherapy alone group vs 204 [ 78% ] of 260 in the chemotherapy plus bevacizimab group ) ; other deaths were due to chemotherapy - related toxic effects ( six [ 2% ] vs five [ 2% ] ) , or related to resection or reoperations ( 13 [ 5% ] in each group )  . 
other reasons were given for 58 patients ( 23 [ 9% ] in the chemotherapy group vs 35 [ 13% ] in the chemotherapy plus bevacizumab group ; appendix ) and the cause of death was unavailable for the remaining five patients ( two [ < 1% ] vs three [ < 1% ] )  . 
 resection 30 - day post - operative mortality was similar in the two groups ( 14 [ 3% ] of 457 patients who underwent resection in the chemotherapy alone group vs 11 [ 3% ] of 438 who underwent the chemotherapy and bevacizumab group )  . 
21 ( 5% ) of 457 patients in the chemo therapy alone group and 22 ( 5% ) of 438 in the chemotherapy and bevacizumab group died within 90 days of surgery . 
of the patents who underwent a resection , data from the post - operative assessment were available for 446 patients in the chemotherapy alone group and 427 in the chemotherapy plus bevacizumab group . 
the overall incidence of post - operative complications was slightly higher in the chemotherapy plus bevacizumab group , with 215 ( 48% ) of 446 patients in the chemotherapy alone group reporting complications com pared with 243 ( 57% ) of 427 patients in the chemotherapy plus bevacizumab group . 
wound healing complications in particular were more prevalent in the bevacizumab group , occurring in 53 ( 12% ) patients in this group compared with 33 ( 7% ) patients in the chemotherapy alone group . 
however , the overall incidence of complications that were deemed to be life - threatening was similar in both groups , at 8% ( 37 of 446 patients in the chemotherapy alone group and 34 of 427 in the chemotherapy plus bevacizumab group )  . 
 appendix p 6 provides full details of the post - operative complications . an increased incidence of post - operative anastomotic leak in the chemotherapy plus bevacizumab group became apparent towards the end of the trial . 
at a planned idmc review in june , 2013 , leaks were recorded in 30 ( 10% ) of 312 patients in the chemotherapy group and 48 ( 16% ) of 297 in the chemotherapy plus bevacizumab group ( compared with 14 [ 8% ] of 179 and 19 [ 11% ] of 170 , respectively , at the previous idmc review in july , 2012 )  . 
overall post - operative survival times given by the extent of resection , calculated from 6 months post - randomisation until death ( to allow for the difference in timing of surgery between the groups )  . 
overall post - operative survival times given by mandard tumour regression grade , calculated from 6 months post - randomisation until death ( to allow for the difference in timing of surgery between the groups )  . 
 survival curves are unadjusted for covariates and the analysis includes all patients with non - missing mandard tumour regression grade ( 168 patients with missing data are excluded )  . 
in june , 2013 , 12 ( 9% ) of 132 patients in this subgroup who received chemotherapy alone had post - operative anastomotic leak versus 29 ( 24% ) of 123 who received bevacizumab , compared with 18 ( 10% ) of 180 versus 19 ( 11% ) of 174 , respectively , in all other patients . 
no other relevant clinical characteristics were identified that might explain the increased frequency of anastomotic leak , nor was there any evidence of a centre effect ( data not shown )  . 
 * these toxic effects were added to the chemotherapy toxicity assessment case report forms after the trial started and as such , not all participants were asked about these specific toxic effects . table 3 : adverse events reported during pre - operative chemotherapy 366 vol 18 march 2017 articles tumours planned for an oesophagogastric resection , and pre - operative bevacizumab was discontinued in such patients who had already been recruited . at the time of the final analysis ( sept 30 , 2015 ) , in patients undergoing oesophago - gastrectomy , we recorded ( 10% ) of post - operative anastomotic 233 patients in the chemotherapy alone group versus 52 ( 24% ) of 220 in the chemotherapy plus bevacizumab group compared with 20 ( 9% ) of 213 and 23 ( 11% ) of 207 , in 23 leaks respectively , in all other patients . 
overall , most of the 103 cases in which onset dates were available occurred during the period immediately after surgery ( 40 [ 39% ] within 5 days of surgery and 80 [ 78% ] within 10 days )  . 
 leak onset dates were provided on serious adverse event reports and were therefore not available for 15 cases in which the event did not satisfy the criteria for a serious adverse event . 
 * these toxic effects were added to the chemotherapy toxic effect assessment case report forms after the trial started and as such , not all participants were asked about these specific toxic effects . table 4 : adverse events reported during post - operative chemotherapy vol 18 march 2017 articles died within 30 days of the operation versus seven ( 9% ) of 75 in the chemotherapy plus bevacizumab group and revisional operations 22 ( 51% ) of 43 patients in the chemotherapy alone group compared with 24 ( 32% ) of 75 in the chemotherapy plus bevacizumab group . ( appendix ) were required discussion the results of our trial show that the addition of bevacizumab to peri - operative epiribicin , cisplatin , and capecitabine chemotherapy did not improve overall survival resectable in patients with potentially oesophagogastric adenocarcinoma . 
there was no clinical evidence of a differential biological effect on tumour growth ; the proportions of patients responding to preoperative chemotherapy assessed by both radiological recist criteria and mandard tumour regression grade from the resected specimen , as well as r0 resection rates , were similar in both groups . 
 this finding is in contrast to those of one small study ( n = 80 ) , which reported that bevacizumab in combination with docetaxel , oxaliplatin , and fluorouracil increased the proportion of r0 resections achieved in patients with locally advanced gastric cancer , 12 and results from studies in advanced ( unresectable and metastatic ) gastric cancer in which bevacizumab in combination with cisplatin and capecitabine given as first - line treatment increased the proportion of patients achieving a response ( 374% vs 460% ; p = 0032 ) and progression - free survival ( hr 080 ; p = 0037 ) but not overall survival.5 additionally , ramucirumab , a monoclonal antibody against vegf receptor 2 , increases median overall survival compared with placebo from 38 months to 52 months as secondline treatment in advanced disease13 and from 74 to 96 months compared with placebo , in combination with paclitaxel in the same setting.14 although an insufficient number of patients had reached the 5 - year timepoint to give a reliable estimate of 5 - year overall survival , the scarcity of evidence for an effect on tumour growth and overall survival to this point suggest that it is unlikely a treatment effect would emerge with longer follow - up . neoadjuvant bevacizumab has also been assessed in other tumour types and has been associated with increased clinical and pathological responses ; 1517 however , such an effect was not evident in the st03 trial . 
most ( 88% ) patients in the st03 trial received 9 weeks of pre - operative chemotherapy , which has previously been shown to enhance tumour down - staging1 and improve overall survival . 
however , the lack of effect shares similarities with results from studies in other tumour types in which promising results with bevacizumab in the advanced setting have not been replicated in earlier stage disease , although these studies were mainly done in the adjuvant setting , for example in breast18 and colorectal19 , 20 cancer . the finding of an increased anastomotic leak rate in patients who had undergone oesophago - gastrectomy was unexpected . 
this period extends well beyond the reported half - life of bevacizumab ( 20 days ) and was believed to be sufficient to prevent effects on post - operative outcomes . 
the primary outcome measures for the phase 2 component were based on tumour perforation rates , cardiac assessments , and post - operative complications.11 in the phase 2 analysis ( n = 200 ; 101 patients in the chemotherapy alone group , 99 in the chemotherapy plus bevacizumab group ) , the anastomotic leak rate was 4% in both groups ( five cases in each group ) with 107 ( 54% ) patients having gastric tumours , 71 ( 36% ) oesophagogastric junction type iii , and 22 ( 11% ) oesophagogastric junction type ii . 
 these figures compare to 275 ( 32% ) , 141 ( 16% ) , and 175 ( 21% ) , respectively in the subsequent 863 patients , with the remainder having oesophagogastric junction type i ( 128 patients ) and lower oesophageal ( 144 patients ) tumours ( recruited after march , 2011 )  . 
this change in eligibility criteria increased the proportion of patients undergoing oesophago - gastrectomy , potentially explaining why the increased leak rate was not apparent earlier in the trial . the treatment of anastomotic leaks varies across the uk ; however , centres in this study used the same treatment irrespective of which group the patient was surgeons used omentum for anastomosis coverage according to standard practice , although at the time of designing the study , randomised data were not available to support this practice . 
although there is a possibility that this method overdiagnosed even small ( non - clinically significant ) leaks , we do not believe that this had a differential effect on rates in each group . careful review of possible confounding factors including centre and laparoscopic surgical approaches did not provide any clear explanation for the increased leak rate and suggests that there could be a prolonged effect of bevacizumab that impairs wound healing . 
findings of one study21 showed that bevacizumab has sustained effects on vegf inhibition more than 6 weeks after dosing , and findings of several rectal cancer in which bevacizumab was used in conjunction with neoadjuvant chemotherapy or chemoradiotherapy showed increased rates of post - operative complications.2225 tumour and blood specimens were collected at baseline in this trial and will be used to investigate whether patients susceptible to long - term effects of bevacizumab such as impaired wound healing can be identified . trials the potential limitations of our study were the inclusion of both gastric and oesophageal tumours and a generous targeted difference of 10% absolute difference in survival . 
however , in our subgroup analysis we recorded no indication of a differential effect by tumour site , or any evidence of a differential biological effect based on r0 resection rates , disease - free survival , or 368 vol 18 march 2017 articles progression - free survival . 
as with the magic trial1 that compared surgery alone with surgery and peri - operative chemotherapy , about half of patients ( 550 [ 52% ] of 1063 ) started post - operative chemotherapy and only 119 ( 22% ) of 530 in the chemotherapy plus bevacizumab group completed all chemotherapy cycles plus the six cycles of maintenance bevacizumab . our data are consistent with findings that r0 resection is an important predictor of long - term survival . 
in future clinical trials , identification of patients at risk of a positive resection margin might have a role in treatment selection ; careful consideration of the clinicopathological features associated with r1 resection will help to inform these decisions . 
the suggestion from these results that a mandard grade of 1 or 2 predicts a better survival outcome ( as opposed to the usual approach of considering mandard grades 13 as a response and grades 45 as no response ) requires further evaluation ; however , in this trial , patients with a mandard grade 1 or 2 seem to have improved survival compared with those with grade 3 . 
a similar survival advantage for mandard grade 1 and 2 responses was seen in the magic trial26 and in the recently reported mrc oe05 trial27 in which two cycles of neoadjuvant cisplatin and docetaxel , oxaliplatin , and fluorouracil were compared against four cycles of neoadjuvant epirubicin , cisplatin , oesophagogastric junction and oesophageal adeno carcinoma . 
however , as intensification of chemotherapy in the oe05 trial did not lead to improved overall survival for the group of patients treated with chemotherapy as a whole , it is unclear whether mandard tumour regression grade 12 ( or complete pathological response ) is a valid surrogate for overall survival as an endpoint in clinical trials . capecitabine and for in conclusion , the addition of bevacizumab to perioperative chemotherapy for patients with resectable oesophagogastric cancer did not lead to an overall survival benefit ; therefore these results are not practice changing . 
all authors contributed to the interpretation of the data and reviewing of the report . declaration of interests dc holds grants from amgen , astrazeneca , bayer , celgene , merrimack , medimmune , merck serono , and sanofi . 
sps , sr , ls , and rel are employed by the uk medical research council , which received funding from cancer research uk and an educational grant from f hoffmann la - roche limited . 
dc and ecs are funded by the national institute for health research biomedical research centre based at the royal marsden and institute of cancer research . editorial for the astro model policy document see astro.org / uploadedfiles / main_ site / practice_management / reimbursement / astro%20 pbt%20model%20policy%20 final.pdf for the astro emerging technologies committee report see radiother oncol 2012 ; 103 : 811 proton therapy for prostate cancer : time for evidence on june 4 , 2014 , the american society for radiation oncology ( astro ) released its model policy on the use of proton beam therapy . 
while the report states that sound evidence exists for the use of proton therapy in diseases such as ocular cancers , skull - base tumours , some spinal tumours , primary hepatocellular carcinoma , and various paediatric the recommendation on the use of proton therapy for prostate cancer is particularly notableastro states that the evidence for e cacy is not clear cut , and proton therapy is not recommended for the primary treatment of prostate cancer outside of a prospective clinical trial or registry . cancers , in the usa , proton therapy is most commonly used for prostate cancer , despite there being little evidence for its superiority over standard photon - based radiotherapy or brachytherapy in this setting . 
research does suggest that many men who develop prostate cancer do not need any treatment , because their disease is unlikely to progress in a clinically meaningful way during their lifetime . 
however , astros emerging technology committee produced an evidence - based review of proton therapy in 2012 highlighting the fact that there was no sound evidence to support the use of protons in preference to conventional radiotherapy for patients with prostate cancer ; neither technique had been shown to give improved results over the other with respect to disease control or toxicity . 
 so why is prostate cancer the most common indication for proton therapy referrals despite there being no evidence base to support it ? some argue that overtreatment of prostate cancer using proton therapy is being driven by three factors : rst , the high costs of building and running these facilities ( indeed , setting up a new centre can cost up to us$235 million , and the national association for proton therapy states that 14 proton therapy centres are currently in operation in the usa , with another ten under construction ) ; second , patient pressure and the risk of patientinitiated legal action ; and third , the vast pro ts these centres can generateas much as $50 million per year . 
some data show that medicare pays out a median of around $19 000 for a full dose of photon therapy for prostate cancer , but $32 000 for the equivalent proton therapy . 
 the controversy surrounding overuse of proton beam therapy in prostate cancer , and the huge nancial implications of such therapy are thus likely to be the cause of the astro document singling out prostate cancer as the only malignancy of those assessed not to be deemed suitable for proton therapy . 
 certain reforms in the us health - care system have been championed by medicare to drive down costs , but there is little sense in continuing to reimburse almost double for a treatment that has no proven bene t over more economic alternatives . 
advocates of proton therapy say that it will be harder to drive down the costs if its use is restricted , but medicares role is not to fund expensive treatment in the hope that it becomes cheaper in the long run . 
at the second annual conference of the national association for proton therapy in april , 2014 , speakers commented that the proton beam therapy industry must broaden its focus and end its reliance on prostate cancer because of the number of cheaper and equally e ective treatments . now that a leading radiotherapy society has rmly stated the lack of justi cation for promoting proton beam therapy over conventional radiotherapy for prostate cancer , deluding patients with false hopes of much more e ective treatment with vastly reduced side - e ects must stop ; pumping huge sums of money from limited health - care budgets into unnecessarily expensive treatments is morally repugnant . 
astro has called for comparative studies , and resources should now be diverted from indiscriminate use of proton therapy into large , de nitive prospective trials to truly de ne the best settings for this modality . 
 the lancet oncology vol 15 july 2014 articles systemic chemotherapy with or without cetuximab in patients with resectable colorectal liver metastasis : the new epoc randomised controlled trial john primrose , stephen falk , meg finch - jones , juan valle , derek oreilly , ajith siriwardena , joanne hornbuckle , mark peterson , myrddin rees , tim iveson , tamas hickish , rachel butler , louise stanton , elizabeth dixon , louisa little , megan bowers , sin pugh , o james garden , david cunningham , tim maughan , john bridgewater summary background surgery for colorectal liver metastases results in an overall survival of about 40% at 5 years . 
the addition of cetuximab to these chemotherapy regimens results in an overall survival advantage in patients with advanced disease who have the kras exon 2 wild - type tumour genotype . 
we aimed to assess the bene t of addition of cetuximab to standard chemotherapy in patients with resectable colorectal liver metastasis . methods patients with kras exon 2 wild - type resectable or suboptimally resectable colorectal liver metastases were randomised in a 1 : 1 ratio to receive chemotherapy with or without cetuximab before and after liver resection . 
 randomisation was done using minimisation with factors of surgical centre , poor prognostic tumour ( one or more of : 4 metastases , n2 disease , or poor di erentiation of primary tumour ) , and previous adjuvant treatment with oxaliplat chemotherapy consisted of oxaliplatin 85 mg / m intravenously over 2 h and uorouracil bolus 400 mg / m intravenously over 5 min , followed by a 46 h infusion of uorouracil 2400 mg / m repeated every 2 weeks ( regimen one ) or oxaliplatin 130 mg / m intravenously over 2 h and oral capecitabine 1000 mg / m twice daily on days 114 repeated every 3 weeks ( regimen two )  . 
cetuximab was given as an intravenous dose of 500 mg / m every 2 weeks with regimen one and three or a loading dose of 400 mg / m followed by a weekly infusion of 250 mg / m with regimen two . 
this trial is registered , isrctn22944367 . findings 128 kras exon 2 wild - type patients were randomised to chemotherapy alone and 129 to chemotherapy with cetuximab between feb 26 , 2007 , and nov 1 , 2012 . 
the median follow - up was 211 months ( 95% ci 126338 ) in the chemotherapy alone group and 198 months ( 122287 ) in the chemotherapy plus cetuximab group . 
with an overall median follow - up of 207 months ( 95% ci 179256 ) and 123 ( 58% ) of 212 required events observed , progression - free survival was signi cantly shorter in the chemotherapy plus cetuximab group than in the chemotherapy alone group ( 141 months [ 95% ci 118159 ] vs 205 months [ 95% ci 168267 ] , hazard ratio 148 , 95% ci 104212 , p = 0030 )  . 
the most common grade 3 or 4 adverse events were low neutrophil count ( 15 [ 11% ] preoperatively in the chemotherapy alone group vs six [ 4% ] in the chemotherapy plus cetuximab group ; four [ 4% ] vs eight [ 8% ] postoperatively ) , embolic events ( six [ 4% ] vs eight [ 6% ] preoperatively ; two [ 2% ] vs three [ 3% ] postoperatively ) , peripheral neuropathy ( six [ 4% ] vs one [ 1% ] preoperatively ; two [ 2% ] vs four [ 4% ] postoperatively ) , nausea or vomiting ( four [ 3% ] vs six [ 4% ] preoperatively ; four [ 4% ] vs two [ 2% ] postoperatively ) , and skin rash ( two [ 1% ] vs 21 [ 15% ] preoperatively ; 0 vs eight [ 8% ] postoperatively )  . 
there were three deaths in the chemotherapy plus cetuximab group ( one interstitial lung disease and pulmonary embolism , one bronchopneumonia , and one pulmonary embolism ) and one in the chemotherapy alone group ( heart failure ) that might have been treatment related . interpretation addition of cetuximab to chemotherapy and surgery for operable colorectal liver metastases in kras exon 2 wild - type patients results in shorter progression - free survival . 
this bene t was supported by the epoc study , 4 which randomly assigned 364 patients with resectable metastases to surgery alone , or surgery with neoadjuvant chemotherapy , and showed an improvement in 3 - year progression - free survival of vol 15 may 2014 lancet oncol 2014 ; 15 : 60111 published online april 7 , 2014 s1470 - 2045 ( 14 ) 70105 - 6 this online publication has been corrected . 
 in the long - term analysis of this study5 5 - year overall survival was 512% ( 95% ci 436583 ) in the perioperative chemotherapy group versus 478% ( 403550 ) in the surgery - only group . 
although this bene t was small , neoadjuvant therapy was established as a treatment option for patients with operable liver metastasis and formed the basis for this and other studies.6 cetuximab ( merck kgaa , darmstadt , germany ) is a monoclonal antibody to egfr with activity in kras exon 2 wild - type colorectal cancer as a single agent.7 after promising phase 2 data , 8 several studies assessed the bene t of cetuximab and panitumumab , a similar antibody , in combination with chemotherapy.913 in 2005 , the coin trial14 was initiated to investigate the addition of cetuximab to oxaliplatin and uoropyrimidine chemotherapy in rst - line treatment of advanced colorectal cancer . 
the new epoc trial was begun as a rational extension to the coin study , 14 the epoc study , and supportive phase 2 data , 8 using much the same investigational strategies to assess whether the addition of cetuximab to oxaliplatin uoropyrimidine chemotherapy improved outcomes for patients with operable liver metastasis . methods participants eligible patients were 18 years or older with a who performance status of 2 or less , and resectable or suboptimally resectable colorectal liver metastasis without detectable extrahepatic distant metastatic disease . 
after 22 patients had been accrued , data15 supporting a bene t of cetuximab only in kras exon 2 wild - type tumours were presented , leading to a protocol who performance status 0 or 1 128 ( 100% ) 126 ( 98% ) age ( years ) women primary tumour t3 or t4 n1 or n2 poorly di erentiated unresected 13 liver metastases one metastasis > 3 cm synchronous metastases chemotherapy alone ( n = 128 ) chemotherapy plus cetuximab ( n = 129 ) 80 ( 63% ) 48 ( 38% ) 92 ( 71% ) 37 ( 29% ) 107 ( 84% ) 109 ( 84% ) 82 ( 64% ) 10 ( 8% ) 13 ( 10% ) 102 ( 80% ) 64 ( 50% ) 60 ( 47% ) 78 ( 60% ) 15 ( 12% ) 18 ( 14% ) 97 ( 75% ) 73 ( 57% ) 68 ( 53% ) 33 ( 26% ) 6 ( 5% ) carcinoembryonic antigen > 30 ng / l 31 ( 24% ) extrahepatic disease 3 ( 2% ) table 1 : characteristics of randomised patients at baseline in kras exon 2 wild - type patients only amendment on july 8 , 2008 , approved by the trial steering committee , to exclude kras mutated patients . 
two resections were staged in the chemotherapy alone group and four resections were staged in the chemotherapy plus cetuximab group . table 3 : surgical information and postoperative complications in kras exon 2 wild - type patients only correspondence to : prof john primrose , university surgery , southampton general hospital , southampton so16 6yd , uk j.n.primrose@soton.ac.uk ( r0 resection ) , or judged to be resectable . 
previous adjuvant chemotherapy was permitted if completed 6 months or more before trial entry and previous rectal chemo radiotherapy was permitted if completed 1 month or more before trial entry . 
there was no limit to the number of metastases , and patients if they had suboptimally resectable were eligible metastases ( ie , with potentially compromised resection margins , but to be treated with curative intent )  . less a personal or the following patients were excluded : those with any uncontrolled medical comorbidity likely to interfere with treatment or assessment of response ; any psychiatric or neurological disorder a ecting ability to consent or comply with medication ; partial or complete bowel obstruction ; pre - existing peripheral neuropathy of grade 1 or higher according to common toxicity criteria ; those with family history of dihydropyrimidine dehydrogenase de ciency , gilberts syndrome , or other congenital abnormality of biliary transport ; than those with platelet counts 100 10 cells per l , an absolute neutrophil count less than 15 10 cells per l , serum bilirubin greater than one and a quarter times the upper limit of normal ( uln ) , or alkaline phosphatase greater than ve times the uln ; serum aminotransferase ( either aspartate amino transferase or alanine aminotransferase ) greater than two and a half times the uln ; estimated creatinine clearance ( by cockcroft formula ) of less than 50 ml / min , or measured glomerular ltration rate of less than 50 ml / m patients with another previous or current malignant disease which , in the judgement of the treating investigator , was likely to interfere with new epoc treatment or assessment of response were also excluded . 
 written informed consent was obtained from all patients before random assignment . randomisation and masking patients were randomly assigned in a 1 : 1 ratio to chemotherapy alone or chemotherapy plus cetuximab . 
 treatment assignments were made over the telephone by the medical research council clinical trials unit with the use of randomised minimisation factors ( full details are provided in appendix p 8 )  . 
a protocol amendment was then implemented on april 22 , 2009 , to condense the strati cation factors to surgical centre , poor prognostic tumour ( one or more of : 4 metastases , n2 disease , or poor di erentiation of primary tumour ) , and previous treatment with oxaliplatin as adjuvant since it was felt by the trial management group that the initial large number of strati cation factors would be less e ective at achieving balance between the treatment groups , in addition to being logistically complicated . 
there was no masking of either investigators or patients to treatment allocation . procedures patients were randomly assigned to chemotherapy with or without cetuximab for 12 weeks , followed by surgery and 604 vol 15 may 2014 articles to receive then a further 12 weeks of chemotherapy with or without cetuximab . 
the chemotherapy backbone was oxaliplatin ( 85 mg / m intravenously over 2 h ) and uorouracil ( 400 mg / m bolus intravenously over 5 min ) followed by a 46 h infusion of uorouracil 2400 mg / m repeated every 2 weeks ( regimen one ) or oxaliplatin 130 mg / m intravenously over 2 h and oral capecitabine 1000 mg / m twice daily on days 114 repeated every 3 weeks ( regimen two )  . 
patients who had received oxaliplatin irinotecan as adjuvant were permitted 180 mg / m intravenously over 30 min with uorouracil as above instead of oxaliplatin ( regimen three )  . 
cetuximab was given as an intravenous dose of 500 mg / m every 2 weeks with regimen one and three , or a loading dose of 400 mg / m followed by a weekly infusion of 250 mg / m with regimen two as previously described.12 the dose of capecitabine in the regimen two group was reduced to 850 mg / m from 1000 mg / m twice daily after toxicity concerns in the coin study14 , 16 which used an identical schedulethis amendment was made on july 24 , 2007 , and was approved by the trial steering committee . 
 subsequent concerns about poor outcome in the regimen two group in the coin study led to an exclusion of capecitabine in combination with cetuximab in the present study17 on july 28 , 2010 , and this amendment was also approved by the trial steering committee . full details of permitted dose reductions and interruptions are available in the protocol . 
 if further surgery was needed , such as resection of the primary tumour or the second phase of a staged liver resection , it was done before adjuvant chemotherapy and within 24 weeks of rst surgery . 
the planned use of ablative techniques was not allowed , but these techniques could be used if clinically indicated at the time of operation . to verify whether surgery was compliant with the protocol , all les were reviewed to compare sites of disease documented at baseline , and on the surgery forany discrepancies were queried directly with either the operating surgeon , or the lead surgeon for that site . in solid tumors ct or mri scans were done to assess response evaluation criteria ( recist ) version 1.018 before systemic treatment , every 3 months for 2 years , and every 6 months for a further 3 years until progression , or death . 
criteria for treatment to be discontinued were : progression while on illness therapy ; unacceptable preventing further treatment ; withdrawal of consent for intercurrent toxicity ; a progression - free survival hr 148 , 95% ci 104212 , p = 003 chemotherapy alone chemotherapy plus cetuximab number at risk chemotherapy chemotherapy plus cetuximab b overall survival hr 149 , 95% ci 086260 , p = 016 chemotherapy alone chemotherapy plus cetuximab time since randomisation ( months ) number at risk chemotherapy chemotherapy plus cetuximab figure 2 : kaplan - meier curves of progression - free survival ( a ) and overall survival ( b ) by treatment group in kras exon 2 wild - type patients only for the study protocol see protocols / new_epoc_protocol . see online for appendix treatment by the patient ; or any alterations in the patients condition which justi ed the discontinuation of treatment in the investigators opinion . for biomarker analysis , formalinxed , para nembedded tumour samples were sectioned and stained with haematoxylin and eosin to establish the regions of highest tumour nuclei content . 
pcr was done in 25 l reactions using 20 ng dna , megamix - gold bu er ( microzone , haywards heath , uk ) , and 10 pm / l primers . 
thermocycling was done at 95c for 10 min , followed by 3438 cycles of 95c for 30 s , 60c for 30 s , and 72c for 30 s , followed by a nal extension of 72c for 10 m 15 l of each pcr product was used for pyrosequencing . 
the primary analysis was unadjusted and sensitivity analyses were done adjusting the model for the minimisation factors and other prognostic factors . all analyses reported here include data up to nov 1 , 2012 , to match the timeframe presented in the interim report to the data monitoring and ethics committee . 
all analyses , except safety , were done on a modi ed intention - to - treat basis , including all patients with known kras exon 2 wild - type genotype who had reached the timepoint for perioperative assessment of response and recist assessment . 
 jp and sp had full access to the raw data , as did the university of southampton clinical trials unit , and were responsible for all data collection and analysis . 
the corresponding author had nal responsibility for the decision to submit for publication . favours chemotherapy and cetuximab favours chemotherapy alone figure 3 : hrs for progression - free survival with chemotherapy alone versus chemotherapy and cetuximab , according to prespeci ed subgroups the subgroups are based on baseline characteristics . 
an additional 14 patients ( six in the chemotherapy alone group and eight in the chemotherapy plus cetuximab the group ) , who were randomly assigned before amendment necessitating kras testing and were retrospectively shown to be kras mutant or indeterminate , were excluded from all analyses except the safety analyses . 
14 kras exon 2 wild - type patients were excluded from the primary analysis population because they had not reached the timepoint for assessment of preoperative response by nov 1 , 2012 , and three did not have the recist assessment before that date as expected . 
as such , the primary analysis population consisted of 236 patients . the baseline characteristics of most patients received chemotherapy regimen one ( 87 [ 68% ] of 128 patients in the chemotherapy alone group vs 87 [ 67% ] of 129 patients in the chemotherapy plus cetuximab group ) , with smaller numbers receiving regimen two ( 27 [ 21% ] vs 24 [ 19% ] , respectively ) and regimen three ( 11 [ 9% ] vs 15 [ 12% ] , respectively )  . 
93 ( 73% ) of 128 patients in the chemotherapy alone group completed 12 weeks of preoperative chemotherapy compared with 98 ( 76% ) of 129 patients in the chemotherapy plus cetuximab group . 
at the time of analysis , 47 of 100 ( 47% ) patients in the chemotherapy alone group who had surgery and 49 of 98 ( 50% ) patients in the chemotherapy plus cetuximab group who had surgery had completed 12 weeks of postoperative chemotherapy ( appendix pp 14 show details of relative dose intensity [ both preoperative and postoperative ] )  . 
13 of 100 ( 13% ) patients in the chemotherapy alone group and 16 of 98 ( 16% ) in the chemotherapy plus cetuximab group did not complete postoperative chemo therapy . 
198 patients had an operation ; 93 ( 93% ) of 100 patients in the chemotherapy alone group and 85 ( 87% ) of 98 patients in the chemotherapy plus cetuximab group proceeded to resection . 
preoperative chemotherapy period is the start of cycle 1 to the start of the last preoperative cycle , plus 3 weeks for patients receiving chemotherapy regimen 1 or 3 , or plus 4 weeks for patients receiving chemotherapy regimen 2 . 
a fishers exact test showed the di erence in skin rash rates between groups was signi cant : two - sided p = 00017 for preoperative period , p = 00071 for postoperative period . 
||postoperative chemotherapy period is the start of the rst postoperative chemotherapy cycle to the start of the last postoperative cycle , plus 3 weeks for patients receiving chemotherapy regimen 1 or 3 , or plus 4 weeks for patients receiving chemotherapy regimen 2 . table 4 : adverse events according to common toxicity criteria for adverse events , strati ed by time of occurrence ( preoperative vs postoperative chemotherapy period ) and by worst grade experienced group were not resected or ablated because of a nding of progressive disease or a complete response at the time of surgery . 
24 patients , ten ( 9% ) of 110 patients in the chemotherapy alone group and 14 ( 13% ) of 112 patients in the chemotherapy plus cetuximab group did not have surgery . 
there were no signi cant di erences between the groups in terms of the surgical procedures donespeci cally , no fewer resections were done in the cetuximab group because of the numerically greater number of responses in this group . median follow - up was 211 months ( 95% ci 126338 ) in the chemotherapy alone group and 198 months ( 122287 ) in the chemotherapy plus cetuximab group . 
 with an overall median follow - up of 207 months ( 95% ci 179256 ) and 123 ( 58% ) of the required 212 events identi ed ( 56 events in the chemotherapy alone group and 67 events in the chemotherapy plus cetuximab group ) , median progression - free survival was 141 months ( 95% ci 118159 ; gure 2a ) in the group receiving chemotherapy with cetuximab compared with 205 months ( 95% ci 168267 ) in the chemotherapy alone group ( hr 148 , 95% ci 104212 , p = 0030 )  . 
median overall survival ( gure 2b ) was 391 months ( 95% ci 236not reached ) in the chemotherapy plus cetuximab group , but had not been reached in the chemotherapy alone group ( lower limit 320 months , hr 149 , 95% ci 086260 , p = 016 )  . treated with those patients to explore this unexpected nding of detriment with chemotherapy plus cetuximab , subgroup analyses were done on the basis of prede ned characteristics ( gure 3 )  . 
 the adverse e ect of cetuximab was associated with characteristics normally deemed to be good prognostic featuresie , well or moderate di erentiation in the primary tumour , three or fewer metastases , absence of n2 disease , and non - synchronous presentation . 
median progression - free survival in patients showing a tumour response to systemic treatment was 205 months ( 95% ci 112355 ) in the chemotherapy alone group compared with 141 months ( 95251 ) in those receiving cetuximab ( hr 152 95% ci 095244 , p = 0082 ; appendix p 7 ) , suggesting there was a poor association between progression - free survival and response . the di erence the overall incidence of grade 3 and 4 adverse events , both preoperatively and postoperatively , was much the same between the groups with a non - signi cantly higher incidence in the chemotherapy plus cetuximab group ( preoperative 64 of 137 [ 40% ] ; postoperative 29 of 105 [ 28% ] vs 22 of 104 [ 21% ] )  . 
this to skin rash di erence was primarily attributable ( preoperative 21 of 137 [ 1% ] , p = 00017 ; postoperativeeight of 105 ( 8% ) vs none of 104 , p = 00071 ; full toxicity is shown in table 4 )  . 
the number of patients needing at least one dose modi cation was much the chemotherapy alone and the same between [ 15% ] vs two of 134 [ 47% ] vs 54 of 134 608 vol 15 may 2014 articles chemotherapy plus cetuximab groups ( 49 of 128 vs 53 of 129 in the preoperative chemotherapy period and 35 of 100 vs 38 of 98 in the postoperative chemotherapy period , respectively ) and seven patients in the chemotherapy alone group and nine in the chemotherapy plus cetuximab group discontinued treatment because of toxicity . 
there were three deaths from respiratory causes ( one interstitial lung disease and pulmonary embolism , one bronchopneumonia , and one pulmonary embolism ) in the chemotherapy plus cetuximab group that might have been related to treatment . 
in the chemotherapy alone group , there was one death from heart failure that might have been treatment related . discussion this trial examined the bene t of cetuximab in kras exon 2 wild - type patients with colorectal liver metastases treated with curative intent . 
the study demonstrates that the addition of cetuximab to chemotherapy seems to be detrimental , and although only a proportion ( 58% ) of the required events have occurred , further follow - up and more events are unlikely to modify this outcome . 
 indeed , this interim analysis is likely to be the most accurate re ection of the study intervention since all patients in the chemotherapy plus cetuximab group stopped receiving cetuximab as of nov 1 , 2012 . 
systemic the detriment identi ed with the addition of cetuximab is likely to be related to the e ect of egfr inhibition because the two main confounding variables , systemic treatment delivery and surgery , were well balanced between treatment delivery , including cetuximab , was much the same as in similar studies20 , 21 and did not seem to be compromised by overlapping toxicities as previously described ( panel )  . 
possible explanations include interactions between cetuximab and the chemotherapy backbone , further mutations in the egfr pathway conferring insensitivity to egfr inhibition , and upregulation of alternative signalling pathways combination with surgery . 
it has been proposed that the interaction between oxaliplatin and cetuximab potentially negative because cetuximab may protect against free radical damage by platinum drugs.25 in support of this theory , the irinotecan - based9 , 12 , 26 and single - agent studies7 , 27 , 28 are predominantly positive . 
 panel : research in context systematic review liver surgery can result in long - term survival in patients with colorectal liver metastases.1 , 3 a formal systematic review on perioperative chemotherapy in patients with operable colorectal liver metastases was not undertaken because only one adequately powered trial exists.4 this study showed that perioperative chemotherapy improves progression - free survival in patients with operable colorectal liver metastases . 
 egfr inhibition in kras exon 2 wild - type cancer improves response rate , progression - free survival , and overall survival in some13 , 22 , 27 but not all14 , 23 studies in patients with advanced disease . interpretation the negative outcome in this study does not result from overlapping toxicities as previously described , 21 nor di erences in surgical management . 
possible explanations include the need for improved biomarker de nition of patients , 22 chemotherapy interaction , or a modi cation of the biomarker environment after systemic therapy or surgery ; these reasons need further investigation . 
 the use of cetuximab in patients with operable colorectal cancer liver metastases should be deemed contraindicated outside clinical trials , and work to establish a biological explanation for this surprising result is needed . importantly , patients who have a kras mutation and are treated with an egfr inhibitor have an inferior outcome in the oxaliplatin - based studies11 , 22 compared with patients in irinotecan - based studies who had a similar outcome to chemotherapy - only controls.29 the analysis of only the patients in the present study who received an oxaliplatinbased backbone is very similar to the primary study outcome ; however , too few patients received irinotecan to draw any conclusions about this combination . 
a clear understanding of the biological mechanism underlying the detriment identi ed is needed before another neoadjuvant cetuximab study is done in this patient population . it is di cult to extend the outcomes from a neoadjuvant strategy to either adjuvant treatment30 , 31 or treatment in advanced disease13 because of the potential confounding variables inherent in a neoadjuvant strategy ( mainly due to surgery , and the associated treatment interval )  . 
there might also be biological di erences between micrometastatic disease ( the adjuvant studies have been negative30 ) and macroscopic metastatic disease ( most advanced disease studies are positive7 , 12 , 13 ) in terms of response to egfr inhibition . 
biomarker analysis in the petacc - 3 study32 has shown the heterogeneity of patients in terms of their molecular and baseline characteristics , as well as their clinical outcomes . vol 15 may 2014 articles additional mutations in the egfr pathway , namely braf and nras , predict an absence of bene t of cetuximab33 in advanced disease studies27 but are unlikely to explain the inferior progression - free survival of cetuximab patients in the present study who showed a tumour response . 
it is possible that mutations might have arisen after treatment with cetuximab , or that resistance to egfr inhibition might result from activation of parallel pathways such as the met receptor tyrosine kinase , 3437 stimulated after liver surgery . 
translational studies examining these possibilities are in progress . the present study is a reminder that combining biological agents with chemotherapy using a suboptimal selection strategy is overly simplistic , and potentially detrimental for patients . 
it is clear that kras mutated patients were unlikely to bene t from cetuximab but this level of selection was insu cient to demonstrate a cohort who might bene t from cetuximab therapy . 
a so - called one size ts all strategy might have seemed rational when a uoropyrimidine was the only systemic agent available , but fails us when we use targeted agents . 
the nding that patients who have a better prognosis seem to do less well with the addition of cetuximab adds complexity to this trial result . in summary , cetuximab in combination with chemotherapy cannot be recommended for patients with operable colorectal liver metastases . 
further translational studies are needed to establish whether egfr inhibition could have a role in this setting . contributors jp and jb conceived the study , designed the protocol , supervised the conduct and analysis of the trial , and cowrote the report . 
tm designed the protocol with jp and jb and was a member of the trial management group and as such supervised the conduct of the trial ; he commented on all drafts of the report and approved the nal version . 
sf , mf - j , jv , dor , as , jh , mp , mr , ti , and th recruited patients and oversaw the conduct of the trial at participating centres ; they commented on drafts of the report and approved the nal version . 
ojg and dc were members of the trial management group and as such supervised the conduct of the trial ; they commented on all drafts of the report and approved the nal version . declaration of interests jp has attended advisory boards for merck , bayer , and sano - aventis . 
th has received research funding from roche , amgen , sano - aventis , and novartis . acknowledgments this research study was funded by cancer research uk and supported by the national cancer research institute via the national cancer research network . 
jb is funded partly from the national institute for health research biomedical research centres at university college london hospitals and dc is funded partly from the royal marsden and institute of cancer research . articles epirubicin , oxaliplatin , and capecitabine with or without panitumumab for patients with previously untreated advanced oesophagogastric cancer ( real3 ) : a randomised , open - label phase 3 trial tom waddell , ian chau , david cunningham , david gonzalez , alicia frances clare okines , andrew wotherspoon , claire sa ery , gary middleton , jonathan wadsley , david ferry , wasat mansoor , tom crosby , fareeda coxon , david smith , justin waters , timothy iveson , stephen falk , sarah slater , clare peckitt , yolanda barbachano summary background egfr overexpression occurs in 2755% of oesophagogastric adenocarcinomas , and correlates with poor prognosis . 
we aimed to assess addition of the anti - egfr antibody panitumumab to epirubicin , oxaliplatin , and capecitabine ( eoc ) in patients with advanced oesophagogastric adenocarcinoma . methods in this randomised , open - label phase 3 trial ( real3 ) , we enrolled patients with untreated , metastatic , or locally advanced oesophagogastric adenocarcinoma at 63 centres ( tertiary referral centres , teaching hospitals , and district general hospitals ) in the uk . 
eligible patients were randomly allocated ( 1 : 1 ) to receive up to eight 21 - day cycles of open - label eoc ( epirubicin 50 mg / m and oxaliplatin 130 mg / m on day 1 and capecitabine 1250 mg / m per day on days 121 ) or modi ed - dose eoc plus panitumumab ( meoc + p ; epirubicin 50 mg / m and oxaliplatin 100 mg / m on day 1 , capecitabine 1000 mg / m per day on days 121 , and panitumumab 9 mg / kg on day 1 )  . 
median overall survival in 275 patients allocated eoc was 113 months ( 95% ci 96130 ) compared with 88 months ( 7798 ) in 278 patients allocated meoc + p ( hazard ratio [ hr ] 137 , 95% ci 107176 ; p = 0013 )  . 
meoc + p was associated with increased incidence of grade 34 diarrhoea ( 48 [ 17% ] of 276 patients allocated meoc + p vs 29 [ 11% ] of 266 patients allocated eoc ) , rash ( 29 [ 11% ] vs two [ 1% ] ) , mucositis ( 14 [ 5% ] vs none ) , and hypomagnesaemia ( 13 [ 5% ] vs none ) but reduced incidence of haematological toxicity ( grade 3 neutropenia 35 [ 13% ] vs 74 [ 28% ] )  . interpretation addition of panitumumab to eoc chemotherapy does not increase overall survival and cannot be recommended for use in an unselected population with advanced oesophagogastric adenocarcinoma . 
 introduction gastric and oesophageal cancers are among the most common causes of cancer - related mortality , and were responsible for more than 11 million deaths worldwide in 2008.1 combination chemotherapy is bene cial in perioperative and advanced disease settings , although overall survival is poor . 
in patients with metastatic disease , median overall survival with best supportive care is about 3 months , which can be extended to about 10 months with chemotherapy.2 , 3 no inter nationally accepted standard of care regimen exists for advanced oesophagogastric although most adenocarcinoma , centres use doublet or triplet chemo therapy combinations with a platinumuoropyrimidine backbone . 
the real2 non - inferiority study established epirubicin , oxaliplatin , and capecitabine ( eoc ) as a standard rst - line regimen , and noted a median overall survival of 112 months.3 this result compared favourably with the alternative regimens assessed in real2 , including a combination of epirubicin , cisplatin , and uorouracil that had a median overall survival of 99 months . in the past decade , the egfr pathway has been recognised as one of the key proliferative pathways that is dysregulated during tumorigenesis . 
preclinical data con rm that transfection of egfr into human cancer cells is associated with an aggressive phenotype , 4 and several molecular aberrations within this pathway can function as potent oncogenes . 
in oesophagogastric adenocarcinoma , egfr overexpression is reported in 2755% of cases in published literature , 5 , 6 and has been associated with reduced overall survival in some series.5 , 7 ampli cation of egfr , measured by uorescence in - situ vol 14 may 2013 lancet oncol 2013 ; 14 : 48189 published online april 15 , 2013 s1470 - 2045 ( 13 ) 70096 - 2 this online publication has been corrected . 
 methods study design and participants real3 was an open - label , multicentre , phase 3 , randomised controlled trial , undertaken at 63 participating centres ( tertiary referral centres , teaching hospitals , and district general hospitals ) in the uk . 
the meoc + p schedule was established in an unplanned dosending study , 12 which was done because excessive toxicity ( primarily diarrhoea ) was noted when the drugs were initially combined at full dose . 
as reported previously , 12 eligible patients had histologically veri ed , untreated , metastatic or locally advanced inoperable adenocarcinoma or undi erentiated carcinoma of the oesophagus , gastro - oesophageal junction , or stomach . 
other eligibility criteria included who performance status see online for appendix 575 patients enrolled ( phase 13 ) 19 treated in phase 1 excluded from further analyses 3 ineligible 1 squamous - cell carcinoma ( on review ) 1 anaemia despite transfusions 1 cardiac comorbidities 553 included in phase 3 trial ( intention - to - treat population ) 275 randomly allocated eoc 278 randomly allocated meoc + p 4 withdrew after randomisation 5 deteriorated before treatment 1 deteriorated before treatment 1 had not started cycle 1 by trial closure 266 started eoc 276 started meoc + p figure 1 : trial pro le eoc = epirubicin , oxaliplatin , and capecitabine . 
exclusion criteria included previous chemotherapy ( including adjuvant chemo therapy ) , previous anti - egfr therapy , known brain metastases , and clinically signi cant cardiac disease or other signi cant comorbidity . 
recruitment largely oesophagogastric adeno carcinoma and therefore her2 status did not a ect eligibility . routine her2 predated testing the study was done in accordance with good clinical practice guidelines and the declaration of helsinki , and was approved by the north west research ethics committee . 
all patients provided written informed consent before screening investigations . randomisation and masking we randomly allocated patients ( 1 : 1 ) to standard eoc chemotherapy ( intravenous epirubicin 50 mg / m on day 1 , intravenous oxaliplatin 130 mg / m on day 1 , and oral capecitabine 1250 mg / m per day on days 121 ) or modi ed - dose eoc in combination with panitumumab ( meoc + p ; intravenous epirubicin 50 mg / m on day 1 , intravenous oxaliplatin 100 mg / m on day 1 , oral capecitabine 1000 mg / m per day on day 121 , and intravenous panitumumab 9 mg / kg on day 1 ) every 21 days . 
randomisation was done independently at the institute for cancer research clinical trials and statistics unit ( icr - ctsu ) by random permuted blocks ( block sizes of six and eight ) and strati ed by centre region ( locations were divided into 11 regions ) , extent of disease ( locally advanced vs metastatic disease ) , and performance status ( 0 vs 1 vs 2 )  . 
advice regarding dose modi cations for toxic e ects was provided in the protocol ( appendix )  . procedures the primary endpoint was overall survival , de ned as the time from randomisation until death from any cause . 
 secondary endpoints were progression - free survival ( pfs ) , de ned as the time from randomisation until documented disease progression or death from any cause ; response rate according to recist 1.0 criteria ; 13 toxicity graded according to national cancer institute common terminology criteria for adverse events ( nci - ctcae ) version 3.0 ; patient - reported outcomes ; and kras mutation status . 
results from patient - reported outcomes will be reported separately . data for patients recruited at royal marsden hospital were subject to source data veri cation by trust - appointed monitoring sta  . 
for other uk centres , the sponsor deemed it appropriate , in keeping with good clinical practice requirements , to undertake central monitoring and provide sites with training meetings and written guidance to ensure appropriate conduct of the trial . 
 participating centres were required to provide evidence con rming patient eligibility , including blood test results , histopathology reports , and imaging reports to ensure appropriate randomisation and strati cation at trial entry . 
recorded toxicities were cross - referenced against reported serious adverse events to ensure that all toxicities were captured and that all events meeting the criteria for a serious adverse event were reported as such . 
 statistical analysis the trial was powered to detect a 10% improvement in 1 year survival , from 45% for eoc to 55% with meoc + p , equating to a hazard ratio ( hr ) of 0749 . 
to achieve 90% power and a two - sided of 005 , we needed to include 509 events ( deaths from any cause ) and planned a total accrual of 730 patients . 
we also did a preplanned non - comparative interim analysis of response rate with meoc + p after the rst 200 patients were assessable for response ( phase 2 population )  . 
these data were reviewed by the independent data monitoring committee ( idmc ) , and con rmed an acceptable response rate of 52% in the meoc + p group , which exceeded the prede ned futility threshold of 45% . throughout the trial , unmasked data were reviewed by the idmc to examine the safety , scienti c validity , and conduct of the trial . 
at annual review of the data in october , 2011 , the idmc noted a statistically inferior overall survival outcome in the meoc + p group based on the occurrence of 169 events ( hr 153 , p = 00062 )  . 
in discussion with the trial management group , we decided to close the trial to further recruitment with immediate e ect , withdraw panitumumab , and cross all patients over to full - dose eoc . 
meoc + p = modi ed eoc plus panitumumab . table 1 : demographics and baseline characteristics of the intention - to - treat population 105 ( 38% ) 173 ( 62% ) 232 ( 83% ) 118 ( 42% ) 144 ( 52% ) 16 ( 6% ) 106 ( 38% ) 94 ( 34% ) 34 ( 12% ) 244 ( 88% ) 273 ( 98% ) 5 ( 2% ) meoc + p hazard ratio 137 ( 95% ci 107176 ; p = 0013 ) 100 number at risk meoc + p 278 135 130 time from randomisation ( months ) 49 38 12 10 3 2 figure 2 : overall survival in 553 patients in the intention - to - treat population , by treatment group patients still on treatment at the time of trial closure and treatment crossover were censored . 
meoc + p = modi ed eoc plus panitumumab . vol 14 may 2013 oesophagogastric junction 169 127 078207 overall locally advanced metastatic 1 metastatic site > 1 metastatic site stomach oesophagus age < 60 years age 60 years male female performance status 0 performance status 1 performance status 2 kras wild - type kras mutation patients 95% ci 553 494 302 192 167 217 215 338 458 235 287 164 137 107176 125 054288 139 107180 120 085169 179 120268 164 104258 132 090194 137 091207 136 099187 134 101176 152 085272 122 079190 148 107203 195 074513 150 103218 023 005115 articles 100 001 01 favours meoc + p favours eoc figure 3 : forest plot of hazard ratios ( hr ) for overall survival according to baseline characteristics eoc = epirubicin , oxaliplatin , and capecitabine . 
 * 61 patients were excluded because they were still on treatment and had not reached rst response assessment at time of data censoring . table 2 : responses by treatment group in 492 patients * results between june 2 , 2008 , and oct 17 , 2011 , we enrolled 575 patients , three of whom were withdrawn because they did not ful l eligibility criteria . 
additionally , 19 patients randomly allocated during the phase 1 dosending study were excluded from the intention - to - treat analysis.12 we included 553 eligible patients in the phase 3 intention - to - treat population , representing 76% of the planned accrual at the time of trial closure ( gure 1 ; table 1 )  . 
 median follow - up in patients who were alive at the time of analysis was 46 months ( iqr 18101 ) in the eoc group and 53 months ( 2695 ) in the meoc + p group . based on 251 events ( eoc 110 , meoc + p 141 ) at the time of reporting , median overall survival was lower in the meoc + p group than in the eoc group ( hr 137 , 95% ci 107176 , p = 0013 ; gure 2 )  . 
median overall survival was 88 months ( 95% ci 7798 ) in the number at risk meoc + p 275 278 113 100 time from randomisation ( months ) 25 24 6 4 2 0 figure 4 : progression - free survival in 553 patients in the intention - to - treat population , by treatment group patients still on treatment at the time of trial closure and treatment crossover were censored . 
 the funding sources were not involved in collection , analysis , and interpretation of data , writing of the report , or the decision to submit the paper for publication . 
 * p values are for comparison of grade 35 toxicity between the two groups . table 3 : reported toxicities according to treatment group in 542 assessable patients meoc + p group compared with 113 months ( 96130 ) in the eoc group ( gure 2 )  . 
35 ( 13% ) of 278 patients in the meoc + p group and 54 ( 20% ) of 275 patients in the eoc group were on treatment at the time of trial closure and were censored at this timepoint . 
figure 3 shows the forest plot analysis for subgroups tested , with a similar e ect favouring eoc noted between all subgroups . based on 333 events ( eoc 153 , meoc + p 180 ) , pfs did not di er between treatment groups ( hr 122 , 95% ci 098152 , p = 0068 ; gure 4 )  . 
1 - year pfs was 20% ( 95% ci 1426 ) in the meoc + p group compared with 21% ( 1427 ) in the eoc group . 61 patients who were still on treatment ( 37 in the eoc group and 24 in the meoc + p group ) and had not reached their rst response assessment at the time of data censoring were excluded from the response analysis . 
 116 ( 46% ) of 254 patients in the meoc + p group had a complete or partial response compared with 100 ( 42% ) of median relative dose intensity eoc group ( n = 266 ) meoc + p group ( n = 276 ) p value patients with relative dose intensity 80% epirubicin oxaliplatin capecitabine panitumumab epirubicin oxaliplatin capecitabine panitumumab 91% ( 7699 ) 89% ( 7599 ) 88% ( 7797 ) 184 ( 69% ) 177 ( 67% ) 188 ( 71% ) 92% ( 77100 ) 92% ( 78100 ) 88% ( 69100 ) 91% ( 77100 ) 198 ( 72% ) 200 ( 72% ) 175 ( 63% ) 196 ( 71% ) 036 0086 074 051 013 0072 data are median ( iqr ) or n ( % )  . 
 table 4 : relative dose intensity in 542 patients who started chemotherapy 238 patients in the eoc group ( odds ratio 116 , 95% ci 081166 , p = 042 ; table 2 )  . 542 patients received at least one cycle of chemotherapy and were assessed for toxicity ( table 3 )  . 
patients in the eoc group had increased rates of grade 34 peripheral neuropathy , neutropenia , febrile neutropenia , and thrombocytopenia compared with patients in the meoc + p group . 
overall , we noted no signi cant di erence between the two groups in terms of grade 35 toxicity when all toxicities were vol 14 may 2013 articles 100 log - rank p < 00001 median overall survival 43 months number at risk grade 14 rash grade 0 rash 219 17 113 5 34 1 8 0 2 grade 0 rash ( n = 57 ) grade 14 rash ( n = 219 ) median overall survival 103 months four patients died from toxicities regarded as related to meoc + p : one each of septicaemia , neutropenic sepsis , pulmonary embolism , and upper gastrointestinal haemorrhage . 
six patients died from toxicities regarded as related to eoc : one each of pneumonia , diarrhoea and dehydration , pneumonitis , and myocardial infarction , and two cases of neutropenic sepsis . for 542 patients who started treatment , the median number of cycles delivered was ve ( iqr three to eight ) in both trial groups . 
80 ( 30% ) of 266 patients who started eoc received all eight planned cycles of chemotherapy , as did 74 ( 27% ) of 276 patients who started meoc + p . 
 excluding these patients , the median number of cycles delivered was six ( iqr three to eight ) with eoc ( 80 [ 38% ] of 212 patients completed eight cycles ) and ve ( iqr three to eight ) with meoc + p ( 74 [ 31% ] of 241 patients completed eight cycles )  . overall , 1307 cycles of eoc were administered compared with 1375 cycles of meoc + p . 
table 4 shows the median relative dose intensity for each drug according to treatment group and the proportion of patients in each group achieving a relative intensity of at least 80% . in exploratory biomarker analyses of 276 patients treated with meoc + p , development of any grade of rash ( 219 patients ) was associated with signi cantly longer overall survival compared with patients with no rash ( 57 patients ; gure 5 )  . 
median overall survival was 103 months ( 95% ci 89116 ) and median pfs was 68 months ( 5978 ) in patients with grade 14 rash compared with median overall survival of 43 months ( 3354 ) and a median pfs of 37 months ( 2351 ) in patients with grade 0 rash ( p < 00001 for overall survival and pfs )  . however , outcomes in the grade 0 rash population might be negatively skewed by patients with rapid disease progression who received insu cient panitumumab to develop rash . 
 although possibly restricted by the smaller number of patients , in this analysis overall survival did not di er between patients who developed ( median 106 months [ 95% ci 90122 ] ) and those who did not ( 85 months [ 7199 ] ; hr 064 [ 95% ci 037111 ] , p = 011 )  . rash few tissue biomarker analyses have been undertaken to date . 
frequencies of tested biomarkers in the rst 200 patients are shown in table 5 and have been reported elsewhere.14 for ten patients with known kras mutant tumours , we noted a potential association with bene t from meoc + p , although this association was not signi cant ( gure 3 )  . 
further biomarker analyses are ongoing in the full trial cohort . discussion the real3 trial is one of two concurrent randomised phase 3 trials ( the other being the expand trial15 ) assessing the addition of anti - egfr monoclonal antibodies to chemotherapy in rst - line oesophagogastric cancer . 
based on the ndings of real3 , use of panitumumab in combination with eoc cannot be recommended in an unselected population with advanced oesophagogastric adenocarcinoma , and was associated with inferior overall survival and pfs . 
notably , this detrimental outcome in the experimental group was not predicted by the phase 2 endpoint of response rate ( overall response rate 52% with meoc + p )  . 
this trial does , however , con rm the e cacy of the eoc control group in this setting , with median overall survival and pfs results that are consistent with those previously reported in real2 ( 112 months for overall survival and 70 months for pfs ) .3 reported previously , 12 the poor outcome associated with meoc + p in this trial did not seem to be attributable to increased treatment - related deaths , and therefore other potential explanations for our ndings need to be considered . 
 first , combination of panitumumab with full - dose eoc in the initial stages of the trial was associated with unacceptably high rates of grade 3 diarrhoea ( four of the rst ve patients by cycle four )  . 
although doubtedly reduced the frequency of grade 34 diarrhoea with meoc + p ( 17% in phase 3 population ) , they also served to reduce the dose intensity of chemotherapy , which is re ected in the reduced incidence of grade 34 neutropenia and peripheral neuropathy noted in the meoc + p group . 
additionally , the dose intensity data show a reduced proportion of patients achieving at least 80% of the planned capecitabine dose in the experimental group , suggesting that meoc + p was still slightly more di cult to deliver than standard eoc . second , a negative interaction might have occurred between panitumumab and one or more of the eoc components . 
evidence in the setting of colorectal cancer suggests that the chemotherapy partner for anti - egfr therapy might be an important determinant of treatment e cacy , with oxaliplatin - containing regimens yielding inconsistent results . 
the opus16 and prime11 studies provide evidence of improved outcomes with the addition of cetuximab and panitumumab respectively , whereas no bene t was associated with the addition of cetuximab in the coin17 and nordic vii18 studies in the same setting . 
recent cell - line data also suggest that greater synergy might exist between anti - egfr therapy and irinotecan than with oxaliplatin.19 additionally , the coin trial17 results suggest that there might be a di erential bene t the uoropyrimidine partner , with patients receiving oxaliplatin plus uorouracil seemingly deriving increased bene t compared with those treated with oxaliplatin plus capecitabine . 
indeed , the 57% frequency of kras mutation in our population is in keeping with the 310% reported in other studies , 2022 and we did not note any braf mutations in 167 tumour samples tested . 
by contrast , gene copy number alterations ( ampli cations and deletions ) seem to be a relatively frequent nding in oesophagogastric adenocarcinoma and are more likely to represent the key molecular alterations driving carcinogenesis . 
two recent series23 , 24 of detailed genomic analyses in oesophagogastric adenocarcinoma reported that about 37% of tumours harbour copy number aberrations in genes that are deemed to be targetable , including kras , egfr , her2 , and met . 
randomised clinical trials are therefore needed to establish whether targeting of these oncogenic signal transduction pathways can meaningfully improve outcomes for patients . vol 14 may 2013 articles panel : research in context systematic review we designed the real3 trial in an attempt to improve outcomes with systemic therapy in advanced oesophagogastric adenocarcinoma . 
monoclonal antibodies directed against egfr had already been shown to improve outcomes in combination with chemotherapy in advanced colorectal cancer , therefore there was interest in pursuing this combination as a possible therapeutic strategy in upper gastrointestinal malignancy . 
 in preclinical studies , cetuximab can decrease egfr pathway signalling via reduced phosphorylation of egfr and akt in oesophagogastric cancer cell lines.25 in combination with chemotherapy , cetuximab results in synergistic inhibition of cell proliferation and enhanced apoptosis.2527 in hypoxic gastric cancer cell lines the addition of anti - egfr therapy reversed oxaliplatin resistance.26 additionally , a synergistic antitumour e ect of combined cetuximab and s - 1 was apparent in gastric cancer cell lines overexpressing egfr.25 , 27 in colorectal cancer , somatic mutations in codon 12 , 13 , or 61 of the kras oncogene confer resistance to panitumumab therapy.11 , 28 met ampli cation with or without kras mutations might be associated with resistance to cetuximab therapy in gastric cancer cell lines ; 29 however , no validated predictive biomarkers for this setting exist . therapy unfortunately , despite preclinical data suggesting a role for anti - egfr treatment of trial oesophagogastric adenocarcinoma , ndings are supported by two other phase 3 trials assessing anti - egfr therapy in this disease setting . 
the expand trial15 assessed the addition of cetuximab to a in 904 patients with cisplatin - capecitabine doublet previously untreated adenocarcinoma of the stomach the the real3 and gastro - oesophageal junction , and did not meet its primary endpoint of improved pfs ( hr 109 , 95% ci 092129 , p = 032 ) .15 expand also noted no improvement with the addition of cetuximab in either overall survival ( hr 100 , 95% ci 087117 , p = 095 ) or overall response rate ( 30% in the experimental group vs 29% for controls )  . 
the cog trial30 assessed the antiegfr tyrosine - kinase inhibitor ge tinib compared with placebo in the second - line treatment of 450 patients with oesophageal and type iii gastro - oesophageal junction cancers . 
however , improvements in pfs ( hr 0795 , p = 0017 ) and disease control at 8 weeks ( 255% in the experimental group vs 160% in controls , p = 0014 ) were noted , suggesting some activity of ge tinib in a small unde ned subset of patients . cancer trial dataset and taken together , these relatively consistent ndings suggest that the egfr pathway is unlikely to represent an important therapeutic target in most patients with oesophagogastric ( panel )  . 
however , this work is ongoing in the full translational analyses these represent a unique opportunity to further assess the molecular biology of advanced oesophagogastric adenocarcinoma within a randomised trial setting . 
furthermore , the evaluation of genetic aberrations in pathways linked to egfr signalling could still o er the prospect of identi cation of a low - frequency biomarker that identi es a subpopulation of patients bene ting from anti - egfr targeted therapy in this setting . contributors dc and ic were responsible for the initial concept and design of the trial . 
tw and afco were the trial physicians and were delegated responsibility for the day - to - day running of the study and real - time review of data on behalf of dc . 
all authors had input into the data interpretation and preparation of the nal report for publication . con icts of interest dc has received research funding from amgen , roche , sano - aventis , merck - serono , novartis , and celgene , and has had advisory roles ( uncompensated ) with roche and amgen . 
he has advisory roles with merck serono ( uncompensated ) , roche ( compensated ) , and sano - aventis ( compensated ) , and has received honoraria from roche and sano - aventis . 
 acknowledgments we thank all participating patients and sta at real3 trial sites , all uk principal investigators , and the royal marsden hospital research data management and statistics unit for additional statistical support . 
we also wish to acknowledge national health service ( nhs ) support provided through national institute for health research biomedical research centre funding at the royal marsden nhs foundation trust and institute of cancer research . 
 articles surrogate endpoints for overall survival in chemotherapy and radiotherapy trials in operable and locally advanced lung cancer : a re - analysis of meta - analyses of individual patients data audrey mauguen , jean - pierre pignon , sarah burdett , caroline domerg , david fisher , rebecca paulus , samithra j mandrekar , chandra p belani , frances a shepherd , tim eisen , herbert pang , laurence collette , william t sause , suzanne e dahlberg , je rey crawford , mary obrien , steven e schild , mahesh parmar , jayne f tierney , ccile le pechoux , stefan michiels , on behalf of the surrogate lung project collaborative group * summary background the gold standard endpoint in clinical trials of chemotherapy and radiotherapy for lung cancer is overall survival . 
two meta - analyses were of adjuvant chemotherapy in non - small - cell lung cancer , three were of sequential or concurrent chemotherapy , and one was of modi ed radiotherapy in locally advanced lung cancer . 
we investigated disease - free survival ( dfs ) or progression - free survival ( pfs ) , de ned as the time from randomisation to local or distant relapse or death , and locoregional control , de ned as the time to the rst local event , as potential surrogate endpoints . 
at the individual level we calculated the squared correlations between distributions of these three endpoints and overall survival , and at the trial level we calculated the squared correlation between treatment e ects for endpoints . 
 findings in trials of adjuvant chemotherapy , correlations between dfs and overall survival were very good at the individual level ( ( cid : 1 ) = 083 , 95% ci 083083 in trials without radiotherapy , and 087 , 087087 in trials with radiotherapy ) and excellent at trial level ( r = 092 , 95% ci 088095 in trials without radiotherapy and 099 , 098100 in trials with radiotherapy )  . 
in studies of locally advanced disease , correlations between pfs and overall survival were very good at the individual level ( ( cid : 1 ) range 077085 , dependent on the regimen being assessed ) and trial level ( r range 089097 )  . 
in studies with data on locoregional control , individual - level correlations were good ( ( cid : 1 ) = 071 , 95% ci 071071 for concurrent chemotherapy and ( cid : 1 ) = 061 , 061061 for modi ed vs standard radiotherapy ) and trial - level correlations very good ( r = 085 , 95% ci 077092 for concurrent chemotherapy and r = 095 , 091098 for modi ed vs standard radiotherapy )  . interpretation we found a high level of evidence that dfs is a valid surrogate endpoint for overall survival in studies of adjuvant chemotherapy involving patients with non - small - cell lung cancers , and pfs in those of chemotherapy and radiotherapy for patients with locally advanced lung cancers . 
 funding programme hospitalier de recherche clinique , ligue nationale contre le cancer , british medical research council , sano - aventis . introduction worldwide , around 16 million new cases of lung cancer are diagnosed annually , which accounts for 13% of all diagnosed cancers and comprised , with 14 million deaths , 18% of cancer deaths in 2008 . 
lung cancer is the leading cause of cancer deaths in male patients.1 8085% of tumours are non - small - cell lung cancers ( nsclcs ) , 2 which include adenocarcinomas , squamous - cell and large - cell carcinomas . 
estimated 5 - year survival in nsclc is only 16%.3 although surgery is generally viewed as the optimum treatment , only about 30% of patients qualify for potentially curative resection.4 a further 20% , mainly those presenting with locally advanced disease , undergo radical thoracic radiotherapy , with or without chemotherapy . 
the remaining 50% of patients , most of whom have late - stage or metastatic disease , generally receive palliative treatments . the gold standard endpoint in randomised clinical trials of lung cancer is overall survival because it is simple to measure , easy to interpret , and measurement is unbiased . 
some of the disadvantages of this endpoint are the need for long - term follow - up and large numbers of patients , the e ect of successive treatment lines that might prolong survival , and the risk of non - cancer deaths rising with increasing time . 
between december , 1992 , and july , 2010 , the food and drug administration granted accelerated approval for 35 oncology products on the basis of surrogate endpoints , such as disease - free survival ( [ dfs ] eg , anastrozole in breast cancer ) and progression - free survival ( [ pfs ] eg , panitumumab in advanced colon cancer ) .5 in europe in 2009 , the european medicines agency approved ge nitib as rstline treatment in patients with locally advanced or metastatic egfr - mutation - positive nsclc , and extended the licence of erlotinib for this treatment in 2011 , both on the basis of pfs.6 , 7 additionally , multiple second - line treatment options have become available , which encourages use of intermediate endpoints in studies of nsclc.8 to be suitable , surrogate endpoints should predict overall survival , and the e ect of treatments on the surrogate endpoints should predict their e ects on overall survival in meta - analyses of individual patients data.9 we have analysed trial data from ve meta - analyses of individual patients data by the nsclc meta - analyses collaborative group1013 and from one by the mar - lc collaborative group14 to assess the use of dfs , pfs , and locoregional control as surrogate endpoints for overall survival . 
dfs in patients suitable for surgery was de ned as the time from randomisation to the rst event ( locoregional or distant recurrence or death from any cause )  . 
 the rank correlation coe cient ( cid : 1 ) between distributions of the candidate surrogate endpoints and overall survival at the individual level was assessed with a bivariate survival model that takes censoring into account.15 the trial - level correlations between treatment e ects ( log hazard ratios ) on the candidate surrogate endpoints and overall survival were quanti ed linear regression model , 16 weighted by trial size . 
we classi ed squared correlation values higher than 09 as excellent , 19 higher than 075 as very good , higher than 05 as good , higher than 025 as moderate , and equal to or lower than 025 as poor . 
 the surrogate threshold e ect was calculated , and was de ned as the minimum treatment e ect on the surrogate that would be necessary to predict a non - zero e ect on overall survival.20 a future trial would require an upper limit of the ci for the estimated surrogate treatment e ect to fall below the surrogate threshold e ect to predict a non - zero e ect on overall survival . 
the kaplan - meier method was used to calculate curves for dfs and overall survival . for each meta - analysis , we used a leave - one - out crossvalidation approach to assess the prediction accuracy of the surrogate model.18 each trial was left out once and the linear model , weighted by trial size , was rebuilt with the other trials . 
this model was then applied to the left - out trial and a 95% prediction interval was calculated to compare the predicted and observed treatment e ect on overall survival . role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
worse median dfs and overall survival in trials of postoperative radiotherapy and chemotherapy ( table 1 ) re ected the poorer outlook of patients than in trials of chemotherapy alone . 
the studies assessed radiotherapy with or without concurrent ( median follow - up 68 years ) or sequential chemotherapy ( median follow - up 52 years ) , or did a head - to - head vol 14 june 2013 articles adjuvant therapy chemotherapy vs no chemotherapy radiotherapy + chemotherapy vs radiotherapy alone locally advanced disease number of patients ( trials ) dfs or pfs vs overall survival 3 - year dfs or 2 - year pfs vs 5 - year overall survival ( r2 [ 95% ci ] ) individual level ( ( cid : 1 ) 2 [ 95% ci ] ) trial level ( r2 [ 95% ci ] ) 083 ( 083083 ) 092 ( 088095 ) 088 ( 083093 ) 087 ( 087087 ) 099 ( 098100 ) 096 ( 093099 ) 5379 ( 17 ) 2247 ( 7 ) 1458 ( 8 ) 2552 ( 15 ) 1201 ( 6 ) radiotherapy + sequential chemotherapy vs radiotherapy alone 077 ( 077077 ) 096 ( 093099 ) 077 ( 063091 ) radiotherapy + concurrent chemotherapy vs radiotherapy alone 085 ( 085085 ) 097 ( 096099 ) 095 ( 092097 ) radiotherapy + sequential chemotherapy vs radiotherapy + concurrent chemotherapy 083 ( 083083 ) 089 ( 081097 ) 075 ( 058092 ) modi ed radiotherapy vs standard radiotherapy 2685 ( 12 ) 081 ( 081081 ) 096 ( 093098 ) 085 ( 078093 ) dfs = disease - free survival . 
pfs = progression - free survival . table 2 : individual and trial - level correlation coe cients and sensitivity data for dfs and pfs regression line 95% prediction interval comparison of radiotherapy plus sequential chemotherapy versus radiotherapy plus concurrent chemotherapy ( median follow - up 61 years ; table 1 , appendix )  . 
a further 12 trials were assessed in the locally advanced setting that compared standard radiotherapy with hyper fractionated or accelerated ( modi ed ) radiotherapy in 2685 patients ( table 1 , appendix )  . 
 a strong association was noted between dfs and overall survival in patients with nsclc who received adjuvant chemotherapy with or without radiotherapy ( ( cid : 1 ) = 083 , 95% ci 083083 for chemotherapy vs no chemotherapy , and 087 , 087087 for those comparing radiotherapy plus chemotherapy vs radiotherapy alone ; gure 1 , table 2 )  . 
the squared correlations between the treatment e ects on dfs and those on overall survival were excellent ( r = 092 , 95% ci 088095 and 099 , 098100 ; table 2 )  . 
the sensitivity analysis , which aimed to re ect typical trial conditions and treatment e ects estimated on dfs at 3 years with those on overall survival at 5 years , yielded slightly lower r values , but these were still very good to excellent ( 088 , 083093 for chemotherapy vs no chemotherapy and 096 , 093099 for radiotherapy plus chemotherapy vs radiotherapy alone ; table 2 )  . 
an exploratory analysis with earlier cuto times for dfs suggested that to correlate the hazard ratio for disease - free survival figure 2 : correlation between treatment e ects on disease - free and overall survival in the assessment of adjuvant treatment for non - small - cell lung cancers ( a ) chemotherapy compared with no chemotherapy . 
 for survival curves for pfs and overall survival in locally advanced disease for radiotherapy plus concurrent chemotherapy compared with radiotherapy alone , and for modi ed radiotherapy compared with standard radiotherapy are shown in gure 3 . 
in the sensitivity analysis , pfs at 2 years correlated reasonably strongly at the trial level with overall survival ( very good to excellent ; table 2 , appendix )  . 
the surrogate threshold e ects for pfs were 093 for radiotherapy plus sequential chemotherapy compared with radiotherapy alone , concurrent chemotherapy compared with radiotherapy alone , 090 for radiotherapy plus sequential chemo therapy compared with radiotherapy plus concurrent chemotherapy , and 100 for modi ed radiotherapy compared with standard radiotherapy . radiotherapy plus 095 for with respect to locoregional control in the trials of radiotherapy plus concurrent chemotherapy compared with radiotherapy alone and of modi ed radiotherapy compared with squared individual - level correlations with overall survival were good ( ( cid : 1 ) 071 , 95% ci 071071 and 061 , 061061 ) and the squared treatment - e ect correlations were very good ( r 085 , 95% ci 077092 and 095 , 091098 ; appendix )  . radiotherapy , standard the prediction results from the cross - validation analyses showed that for dfs in the adjuvant setting , the hazard ratios for overall survival fell within the 95% prediction intervals in all 17 trials for chemotherapy compared with no chemotherapy and in six of seven trials of radiotherapy plus chemotherapy compared with radiotherapy alone ( gure 5 )  . 
for pfs in the locally advanced setting , the observed hazard ratio for overall survival fell between the limits of the 95% prediction intervals in all eight trials for radiotherapy plus sequential chemotherapy compared with radiotherapy alone , 14 of 15 trials of radiotherapy plus concurrent chemotherapy compared with radiotherapy alone , all six trials for radiotherapy plus sequential chemotherapy compared with radiotherapy plus concurrent chemotherapy , and in 11 of 12 trials of modi ed radiotherapy compared with standard radiotherapy ( gure 5 , appendix )  . 
pfs = progression - free survival . a valid surrogate endpoint for overall survival in studies of adjuvant chemotherapy in patients with nsclc , and that pfs in assessment of chemotherapy and radiotherapy in patients with locally advanced disease . 
dfs and pfs should , therefore , be is a valid surrogate vol 14 june 2013 articles regression line 95% prediction interval hazard ratio for progression - free survival figure 4 : correlation between treatment e ects on progression - free and overall survival in locally advanced disease ( a ) radiotherapy plus concurrent chemotherapy compared with radiotherapy alone in non - small - cell lung cancer . 
correlation values are excellent ( r2 = 097 and r2 = 096 )  . considered chemotherapy and radiotherapy trials ( panel )  . for use as primary endpoints for overall , the correlations for dfs or pfs indicated that almost 8999% of the variation in treatment e ects on overall survival can be explained by e ects on dfs or pfs . 
since the number of events with locoregional control is always lower than for pfs in randomised clinical trials for the same sample size and follow - up , the statistical power for the assessment of locoregional control will also always be lower . 
 the sensitivity analysis strongly suggests that the information on dfs and pfs acquired at 3 years and 2 years , respectively , could be su cient to predict the 5 - year e ect of treatment on overall survival in patients with operable and locally advanced tumours . 
 we used dfs or pfs as de ned by the investigators in the trials , which included patients across a wide time range , but the consistency of the results across the meta - analyses is reassuring . 
the potential gain in the use of pfs as a surrogate in locally advanced lung cancer is probably smaller than that associated with the use of dfs to assess adjuvant treatment because the times from progression to death are shorter . 
the possible gains of using pfs should , therefore , be weighed against the possible risks and the known biases associated with assessing progression21 and the di culties in assessing local relapses after chemotherapy or chemoradiation . 
 use of a similar approach to assess individual patients data has shown that dfs is useful as a surrogate for overall survival in the testing of adjuvant chemotherapy regimens for other cancer types , such as colorectal cancer , trial - level r = 085 ( very good ) .17 the data for pfs , however , have been less consistent , although excellent correlation ( r = 098 ) was seen with overall in assessment of uoropyrimidine - based survival chemotherapy in advanced colorectal cancer.22 a combined dfs and pfs endpoint proved to be an appropriate surrogate for the assessment of various chemotherapy ( r = 087 ) and radiotherapy ( r = 096 ) regimens in locally advanced head and neck cancers.18 pfs alone , however , was not a valid surrogate for overall survival in trials comparing an anthracycline with a taxane for advanced breast cancer ( r = 023 ) .23 few surrogacy assessments based on individual patient data have been done in lung cancer . 
in advanced nsclc , treatment e ects on pfs were moderately correlated with those on overall survival in trials comparing rstline docetaxel with vinorelbine ( r = 038 ) .24 in three trials of patients with extensive sclc , pfs was strongly level associated with overall survival at the trial ( r = 079 ) .25 part of the discrepancy between the nsclc and sclc results could be due to the administration of subsequent lines of therapy that prolong survival in patients with nsclcs . interpretation of outcomes on the basis of surrogate endpoints has several limitations . 
a surrogate endpoint can only be validated for the therapies assessed ; extrapolation to treatments administered by di erent methods or with substantially di erent mechanisms of action might not be warranted . 
additionally , we reassessed data from a generation of trials in which chemotherapy treatments being or radiotherapy were investigated and when few , if any , active agents were the main 624 vol 14 june 2013 articles observed hr predicted hr trial trial figure 5 : internal validation of the prediction of overall survival by treatment e ects on surrogate endpoints ( a ) treatment e ects on disease - free survival for adjuvant chemotherapy compared with no chemotherapy in non - small - cell lung cancer . 
 ( b ) treatment e ects on progression - free survival e ects for radiotherapy plus concurrent chemotherapy compared with radiotherapy alone in non - small - cell lung cancer . 
 ( d ) treatment e ects on progression - free survival for modi ed radiotherapy compared with standard radiotherapy in non - small - cell and small - cell lung cancers . 
predicted hrs for overall survival are calculated from the observed hr on disease - free or progression - free survival of that particular trial and the surrogate model built on all the other trials . 
also , crossover can a ect the power of assessing e ects on overall survival , particularly when an e ective secondline treatment is available.26 , 27 the use of dfs or pfs as primary endpoints in future clinical trials does not reduce the need for long - term follow - up of patients . 
in many cases it remains necessary to con trol for unexpected adverse reactions and to assess overall survival , even when crossover to the experimental therapy from the control arm is permitted . 
the use of validated surrogates , however , would enable earlier assessments of treatment e ects and could lead to conditional approval by regulatory authorities without prema ture discontinuation of followup , which is partic ularly important to assess the potential for long - term late or toxic e ects when a proportion of patients are cured.28 vol 14 june 2013 articles panel : research in context systematic review the gold standard endpoint in randomised clinical trials of lung cancer is overall survival because it is simple to measure , easy to interpret , and measurement is unbiased . 
some of the disadvantages of this endpoint are the need for long - term follow - up and large numbers of patients , the e ect of successive treatment lines that might prolong survival , and the risk of non - cancer deaths rising with increasing time . 
we have analysed trial data from ve meta - analyses of individual patients data by the nsclc meta - analyses collaborative group1013 and from one by the mar - lc collaborative group14 to assess the use of disease - free survival , progression - free survival , and locoregional control as surrogate endpoints for overall survival . 
 interpretation disease - free survival may be used as a primary endpoint in adjuvant chemotherapy trials involving patients with non - small - cell lung cancers , and progression - free survival is suitable for use in trials of chemotherapy and radiotherapy in patients with locally advanced lung cancer . 
these results do not automatically translate to targeted agents . contributors am , j - pp , and sm conceived and coordinated the project , did all analyses , and wrote the report . 
all authors contributed individual patient data from trials and commented on the initial surrogate - endpoint protocol and on drafts of the report . con icts of interests we declare that we have no con icts of interest . acknowledgments this study was sponsored by programme hospitalier de recherche clinique , ligue nationale contre le cancer , british medical research council , and sano - aventis . 
we thank the participating collaborative groups : study group of adjuvant chemotherapy for lung cancer , arbeitsgemeinschaft radioonkologie der deutschen krebsgesellschaft , groupe detude et de traitement des cancers bronchiques , cancer and leukemia group b , eastern cooperative oncology group , european organization for research and treatment of cancer , groupe doncologie thoracique lyon - saint - etiennegroupe franais de pneumo - cancrologie , japan clinical oncology group , japan lung cancer research group , medical research council , north central cancer treatment group , national cancer institute of canada clinical trial group , radiation therapy oncology group , and west japan study group for lung cancer surgery , and the clinical investigators of the trials and the patients . see correspondence page e194 preventable cancer : off - limits for commonwealth meeting ? as the global burden of non - communicable diseases continues to exert its toll , the prevention , screening , and early diagnosis of cancer should be a priority for all countries . 
the letter , cosigned by eminent experts in cancer and population health , demands that issues surrounding cervical cancer and endemic childhood cancers are part of the commonwealth health ministers meeting in may 2017 . 
the signatories also call for screening , early detection , and improved awareness of various childhood cancers , which can be treated successfully if caught early or even prevented through effective control of malnutrition and infectious diseases . 
surely the health of women and children is paramount to achieve such goals ? cost - effective prevention and screening for cancers should be an integral part of any successful uhc agenda . 
the limited reply declares that the prevention , treatment , and care of cancers are a priority , but fails to suggest any amendments to the forthcoming meetings agenda to give these important issues the consideration they deserve . 
a recent report from the american cancer society warns that the incidence of the diseasein which typically 90% of patients are over 50 years of ageis increasing sharply in each generation born since 1950 . 
as national colorectal and bowel cancer awareness months are marked in march and april in the usa and uk , respectively , this timely report rings alarm bells for ominous changes in the aetiology of this disease . despite colorectal cancer being a slow growing disease in which symptoms may not present for many years , survival rates have improved in recent decades , mainly thanks to screening . 
major risk factors ( unhealthy diets , obesity , and sedentary lifestyles ) are becoming more prevalent in successive generations , raising the question of whether these factorsespecially in the early years of lifecould interact with an underlying genetic backdrop to trigger early onset of the disease . screening is the mainstay of colorectal cancer prevention and early detection . 
 furthermore , with the widespread belief that cancer is associated with ageing , family doctors can too easily discount the possibility of colorectal cancer in young patients , even when they present with characteristic symptoms such as blood in the stool and abdominal pain . what can be done ? although whole - population screening is not feasible , cost - effective , or truly warranted , genetic counselling and gene testing for those known to be at high risk because of family history or underlying genetic predisposition could be considered . 
 the lancet oncology vol 18 april 2017 editorial regarding survival and 35 years ( 3045 ) for overall survival ( median follow - up 34 years [ 2943 ] for the sodium thiosulfate group , and 38 years [ 3145 ] for the control group ) ; and localised and sentences disseminated disease should have read localised among participants with disease , 14 events in the sodium thiosulfate group , 13 events in the control group , and six deaths in both the control and sodium thiosulfate groups occurred and in participants with disseminated disease , 12 events and 11 deaths occurred in the sodium thiosulfate group and 11 events and four deaths occurred in the control group . 
these corrections have been made to the online version as of june 2 , 2017 . correction to lancet oncol 2017 ; 18 : 71931 registry international cancer , steliarova - foucher colombet m , ries lag , et al , and the iicc - 3 incidence contributors . 
 lancet oncol 2017 ; 18 : 71931 in this article , the coverage of the population of east asia in table 1 in the age 014 years column should have been 44% , and in the age 1519 years column , 40% . 
 consequently , the fourth sentence in the first paragraph of the results read approximately should have the world population 114% of aged ( contributing years 18 376 710 144 person - years ) was covered by the registries included in our study , ranging from 17% in south asia ( india ) to 994% in north america ( table 1 )  . 
these corrections have been made to the online version as of june 2 , 2017 , and the printed article is correct . 014 correction to lancet oncol 2017 ; 18 : 812 versus gronchi a , ferrari s , quagliuolo v , et al . 
histotype - tailored neoadjuvant chemotherapy standard chemotherapy in patients with high - risk soft - tissue sarcomas ( isg - sts 1001 ) : an international , open - label , randomised , controlled , phase 3 , multicentre trial . 
this correction has been made to the online version as of june 2 , 2017 , and the printed article is correct . correction to lancet oncol 2017 ; 18 : 6374 freyer dr , chen l , krailo md , et al . 
 effects of sodium thiosulfate versus observation on development of cisplatininduced hearing loss in children with cancer ( accl0431 ) : a multicentre , open - label , controlled , randomised , phase 3 trial . 
lancet oncol 2017 ; 18 : 6374in the summary and results of this article , the sentences should regarding adverse events have read the most common grade 34 haematological adverse events reported , irrespective of attribution , were neutropenia ( 117 [ 66% ] of 178 participant cycles in the sodium thiosulfate group vs 145 [ 65% ] of 224 in the control group ) , whereas the most common non - haematological adverse event was hypokalaemia ( 25 [ 17% ] of 149 vs 22 [ 12% ] of 187 )  . 
 in the results , sentences regarding adverse events should have read haematological toxicity was not significantly different between the treatment groups , occurring 137 ( 77% ) of 178 participant cycles in the sodium thiosulfate group and 172 ( 77% ) of 224 participant cycles in the control group ( p = 097 ; table 3 )  . 
aggregate nephrotoxicity was more common in the sodium thiosulfate group , in which 37 ( 25% ) of 149 participant cycles were affected versus 25 ( 13% ) of 187 controls ( p = 00071 ; sentences table 4 ) ; serious adverse events regarding should have read 194 serious adverse events were reported in 26 patients ; of these , 127 were deemed unrelated , 47 unlikely , 20 possibly , and none related to probably or definitely sodium thiosulfate . 
87 were nonhaematological adverse events , of which 45 were deemed unrelated , 28 unlikely , 14 possibly , and none related to probably or definitely sodium sentences thiosulfate ; regarding median follow - up should have read median follow - up was 35 years ( iqr 3045 ) for event - free vol 18 june 2017 e301 corrections articles cixutumumab and temsirolimus for patients with bone and soft - tissue sarcoma : a multicentre , open - label , phase 2 trial gary k schwartz , william d tap , li - xuan qin , michael b livingston , samir d undevia , bartosz chmielowski , mark agulnik , scott m schuetze , damon r reed , scott h okuno , joseph a ludwig , vicki keedy , petra rietschel , andrew s kraft , douglas adkins , brian a van tine , bruce brockstein , vincent yim , christiana bitas , abdul abdullah , cristina r antonescu , mercedes condy , mark a dickson , shyamprasad deraje vasudeva , alan l ho , l austin doyle , helen x chen , robert g maki summary background preclinical studies have shown synergistic antitumour activity by inhibition of insulin - like growth factor - 1 receptor ( igf - 1r ) and mtor . 
we investigated the safety and e cacy of the combination of the igf - 1r antibody cixutumumab and the mtor inhibitor temsirolimus in patients with chemotherapy - refractory bone and soft - tissue sarcomas according to igf - 1r expression by immunohistochemistry . methods we undertook a multicentre , open - label , phase 2 study in 19 cancer centres in the usa . 
patients aged at least 16 years with a histologically con rmed diagnosis of bone or soft - tissue sarcoma were allocated on the basis of igf - 1r expression by immunohistochemistry to one of three treatment groups : igf - 1r - positive soft - tissue sarcoma ( group a ) , igf - 1r - positive bone sarcomas ( group b ) , or igf - 1r - negative bone and soft - tissue sarcoma ( group c )  . 
a simon optimal two - stage design was used for every ar the primary endpoint was progression - free survival ( pfs ) at 12 weeks by intention - to - treat analysis in the rst 54 patients assigned to every treatment aralthough patients still remain on treatment , this trial has completed enrolment and this represents the nal analysis . 
on april 6 , 2011 , the protocol was amended to include three additional patients in the igf - 1r - positive soft - tissue sarcoma group ( total of 57 patients ) and nine more in the igf - 1r - negative group ( total of 63 patients )  . 
the most common grade 34 toxicities in the 174 treated patients were anaemia in 16 ( 9% ) patients , hyperglycaemia in 18 ( 10% ) , hypophosphataemia in 16 ( 9% ) , lymphopenia in 25 ( 14% ) , oral mucositis in 19 ( 11% ) , and thrombocytopenia in 19 ( 11% )  . 
 funding national cancer institute and cycleforsurvival fund , memorial sloan - kettering cancer center . introduction about 13 000 cases of soft - tissue and bone sarcoma are diagnosed annually in the usa.1 the median survival from diagnosis for patients with metastatic disease is about 1018 months.2 in view of the toxicity and limited e cacy of chemotherapy , patients with advanced and metastatic disease are appropriate candidates for investigational treatments . 
insulin - like growth factor - 1 ( igf - 1 ) , igf - 2 , and igf - binding protein ( igf - bp ) are expressed in various sarcoma subtypes , which suggests that igf - 1 receptor ( igf - 1r ) inhibition might be applicable in sarcomas.3 igf - 1r is activated by the growth factor ligands igf - 1 and igf - 2 , resulting in receptor leads to the activation autophosphorylation , which cascades , including signalling of many the pi3kaktmtor pathway . 
we hypothesised that igf - 1r expression by the tumour would be crucial to identify the clinical bene t of this drug combination and would be independent of histological subtype . 
because response to igf - 1r antibody treatment on the basis of histological subtype alone has been scarce , we believed that upfront strati cation by igf - 1r expression would result in an improved clinical bene t . 
therefore , rather than stratify by histological subtype , we assessed clinical bene t according to igf - 1r expression by immuno histochemistry . methods patients we undertook a multicentre , open - label , phase 2 , nonrandomised trial in 19 cancer centres in the usa . 
patients aged at least 16 years were eligible if they had an eastern cooperative oncology group performance status of 0 or 1 , histologically or cytologically con rmed sarcoma of soft tissue or bone , and measurable metastatic or locally advanced disease by response evaluation criteria in solid tumors ( recist ) 1.1 , and if they had received at least one but not more than four previous treatments and had adequate organ function ( de ned by a normal complete blood count [ absolute neutrophil count 15 10 / l , platelet count 100 10 / l ] , liver function tests [ total bilirubin 15 institutional upper limit of normal [ uln ] and aspartate aminotransferase and alanine aminotransferase 3 uln ] , and renal [ serum creatinine 15 uln )  . 
patients with hyper glycaemia , de ned as fasting serum glucose above 666 mmol / l , or those already on oral antidiabetic or insulin treatment were excluded from the study , as were those who received previous igf - 1r or mtor inhibitors . function the study was undertaken in accordance with the declaration of helsinki . 
the institutional review boards of all participating centres reviewed and approved the protocol . procedures all patients had igf - 1r testing on archival tissue by immunohistochemistry at memorial sloan - kettering cancer center ( mskcc ; new york , ny , usa )  . 
im munohistochemistry was done on 4 - m formalinxed para n embedded slides using pre - diluted igf - 1r antibodies ( ventana , ventana medical systems , tucson , az , usa ) according to published methods.18 the scoring for igf1r expression was quantitated on a 03 + scale : 01 + , no staining or faint or weak staining ; 2 + , moderate staining ; and 3 + , strong staining . 
 scoring for igf - 1r expression was done by central pathology review ( cristina antonescu , mskcc ) so as to minimise the inter - patient variability with immunohistochemistry . patients were assigned to one of three groups : those in group a had igf - 1r - positive sarcomas of soft tissue ; those in group b had igf - 1r - positive sarcomas of bone ; and those in group c had igf - 1r - negative sarcomas of bone and soft tissue . 
all patients received weekly treatment with cixutumumab ( 6 mg / kg intravenous ) over 1 h followed 1 h later ( 30 min if the rst two doses were tolerated ) by temsirolimus ( 25 mg intravenous ) in 6 - week cycles . if grade 3 or 4 neutropenia or thrombocytopenia occurred , temsirolimus and cixutumumab were respectively reduced by one ( 20 mg and 5 mg / kg ) or two ( 15 mg and 4 mg / kg ) dose levels . 
for any grade 1 hepatic toxicity ( bilirubin , alanine aminotransferase , or aspartate aminotransferase ) the temsirolimus dose was reduced immediately by two dose levels ( 15 mg )  . 
plasma samples for measurement of igf - 1 and igf - bp3 concentrations by elisa assay ( r&d systems , minneapolis , mn , usa ) were taken before treatment and on weeks 3 and 7 . 
plasma measurements were a requirement at mskcc but were optional at other sites . all patients treated at mskcc were required to undergo tumour biopsies before and after treatment unless deemed clinically inappropriate . 
biopsies were ash frozen in liquid nitrogen before treatment and between weeks 2 and 3 for assessment of total igf - 1r , p - akt , total akt , phosphorylated s6 ( p - s6 ) , and total s6 by western blots according to standard techniques.15 equal 372 vol 14 april 2013 articles loading of protein was con rmed by tubulin and gapdh staining , and relative protein expression was quanti ed by densitometry assessment with imagej . 
a post - hoc analysis was done by histological subtypes on progression - free survival , overall survival , and response . statistical analysis based on historical controls , a pfs of over 40% at 3 months was deemed acceptable for second - line treatment and a pfs of less than 20% was deemed unacceptable.19 we used a simon optimal two - stage design for every arm such that the outcome of the study was assessed by the decision rule of the study design.20 in particular , in stage 1 , 19 patients were to be accrued . 
if at least 16 patients were progression free at 12 weeks among the rst 54 patients , the arm would be judged to have a positive result and the combination therapy would be worthy of further testing . 
 this design had a power of 090 for establishing the treatment e ect for a population 12 - week pfs proportion malignant peripheral nerve sheath tumour 9 ( 82% ) 2 ( 18% ) gastrointestinal stromal tumour chondrosarcoma chordoma clear - cell tumour ewings sarcoma leiomyosarcoma liposarcoma myxo brosarcoma osteosarcoma rhabdomyosarcoma sarcoma , unspeci ed solitary brous tumour spindle - cell tumour synovial sarcoma others undi erentiated pleomorphic sarcoma total igf - 1r positive igf - 1r negative 20 ( 53% ) 18 ( 47% ) 1 ( 17% ) 5 ( 83% ) 5 ( 83% ) 1 ( 17% ) 33 ( 54% ) 28 ( 46% ) 3 ( 25% ) 9 ( 75% ) 26 ( 58% ) 19 ( 42% ) 5 ( 45% ) 6 ( 55% ) 1 ( 17% ) 5 ( 83% ) 33 ( 63% ) 19 ( 37% ) 9 ( 47% ) 10 ( 53% ) 7 ( 70% ) 3 ( 30% ) 7 ( 50% ) 7 ( 50% ) 11 ( 58% ) 8 ( 42% ) 8 ( 47% ) 9 ( 53% ) 14 ( 78% ) 4 ( 22% ) 19 ( 44% ) 24 ( 56% ) of 40% using a type i error of 005 . 
the probability of stopping each arm of the study early was 67% if the population 12 - week pfs proportion was 20% . analyses of e cacy data were done for all patients who had received any study drug ( intention - to - treat )  . 
for every arm , the proportion of patients remaining free of progression at 12 weeks was estimated and a one - sided 95% ci and a two - sided 90% ci were calculated . 
median event - free times for all treated patients were estimated by the kaplanmeier method with a two - sided 95% ci and were compared between groups by the log - rank test with a two - sided p value . 
correlation of plasma biomarkers for igf - 1 and igf - bp3 to pfs at 12 weeks was examined by the wilcoxon rank sum test with a twosided pvalue for absolute levels at baseline , week 3 , or week 7 and for change of levels at week 3 or week 7 from baseline . 
 role of the funding source the sponsor of the study ( national cancer institute ) was involved in study design , data collection , and the decision to submit for publication in conjunction with the authors . 
 388 screened for eligibility 226 excluded 68 study group closed to patient accrual 48 decline in performance status 32 pursued alternative therapy 32 ineligible * 21 withdrew informed consent 25 other 162 eligible 54 assigned to igf - 1r - positive soft - tissue sarcoma and included in analysis of primary endpoint 54 assigned to igf - 1r - positive bone sarcoma and included in analysis of primary endpoint 54 assigned to igf - 1r - negative soft - tissue and bone sarcoma and included in analysis of primary endpoint 3 included after protocol amendment 9 included after protocol amendment 57 included in all ecacy and safety analyses 54 included in all ecacy and safety analyses 63 included in all ecacy and safety analyses 15 gave plasma samples and 9 had tissue biopsies 23 gave plasma samples and 16 had tissue biopsies 17 gave plasma samples and 7 had tissue biopsies data are number ( % )  . 
 table 1 : insulin - like growth factor - 1 receptor status according to histological subtype in at least ve patients for all screened patients figure 1 : trial pro le igf - 1r = insulin - like growth factor - 1 receptor . 
the corresponding author ( gks ) had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results from nov 18 , 2009 , to april 11 , 2012 , 388 patients were screened for igf - 1r expression by immunohistochemistry . 
of these , 211 ( 54% ) were igf - 1r positive and 177 ( 46% ) were igf - 1r negative across many sarcoma subtypes ( table 1 )  . 
the remainder of the screened patients were excluded because the study arm was closed to patient accrual or the patient did not meet protocol eligibility , had poor performance status , withdrew consent , elected to seek hospice or other treatments , or for other reasons ( gure 1 )  . 
on april 6 , 2011 , the protocol was amended to include three additional patients in the igf - 1r - positive soft - tissue sarcoma group and nine in the igf - 1r - negative sarcoma group , giving a total of 57 patients with igf - 1r - positive soft - tissue sarcoma ( group a ) , 54 with igf - 1r - positive bone sar coma ( group b ) , and 63 with igf - 1r - negative sarcoma ( group c )  . 
this protocol amendment was made because of over enrolment into group a ( patients who consented before enrolment was halted ) and on the basis of promising results in rst 54 patients in group c . 
 by intention - to - treat analysis , of the 54 patients in each group in the original cohort ( ie , before the protocol amendment ) , 17 patients ( 31% ; one - sided 95% ci lower bound 21% ; two - sided 90% ci 2143 ) in the igf - 1rpositive soft - tissue sarcoma group , 19 patients ( 35% ; onesided 95% ci lower bound 24% ; two - sided 90% ci 2447 ) the igf - 1r - positive bone sarcoma group , and 21 patients ( 39% ; one - sided 95% ci lower bound 28% ; two - sided 90% ci 2851 ) in the igf - 1r - negative group were progression free at 12 weeks . after the protocol amendment and inclusion of additional patients , 17 of 57 patients ( 30% ; one - sided 95% ci lower bound 20% ; two - sided 90% ci 2041 ) in the igf - 1r - positive soft - tissue sarcoma group and 26 of 63 ( 41% ; one - sided 95% ci lower bound 31% ; two - sided 90% ci 3152 ) in the igf - 1r - negative group were progression free at 12 weeks . 
all deaths were due to disease progression . nine patients achieved a partial response : one ( 2% ) of 57 patients in the igf - 1r - positive soft - tissue sarcoma group , six ( 11% ) of 54 patients in the igf - 1r - positive bone sarcoma group , and two ( 3% ) of 63 patients in the igf - 1rnegative group . 
 all patients with disease progression at week 12 had signi cant increases in plasma biomarkers from baseline to weeks 3 or 7 ( p < 001 appendix )  . 32 patients ( nine in the igf - 1r - positive soft - tissue sarcoma group , 16 in the igf - 1r - positive bone sarcoma group , and seven in the igf - 1r - negative group ) at mskcc had serial tumour biopsies undertaken before treatment and between weeks 2 and 3 of the rst cycle of therapy and analysed by western blot . 
although suppression of igf - 1r and inhibition of both p - s6 and p - akt was noted in individual patients in all treatment arms , semi - quantitative analysis did not suggest any consistent association between the percent decrease in igf - 1r , p - s6 , or p - akt expression and clinical outcome ( table 3 )  . 
all patients in the immunohistochemistryde ned igf - 1r - negative groupin which igf - 1r was assessable by western blot ( ve of the seven ) were igf - 1r positive by western blot ( table 3 )  . in 19 of 2546 adverse events reported , 214 ( 8% ) were grade 34 . 
grade 12 and 34 events that occurred in at least 5% of all patients treated are listed by strati cation groups ( table 4 ) and by histological subtype ( appendix )  . 
the most common grade 34 toxicities in the 174 patients were anaemia in 16 ( 9% ) patients , hyperglycaemia in 18 ( 10% ) patients , hypo phosphataemia in 16 ( 9% ) patients , lymphopenia in 25 ( 14% ) patients , oral mucositis in 19 ( 11% ) patients , and thrombocytopenia ( 11% ) patients . 
of 174 patients treated on the study , 83 ( 48% ) experienced a serious adverse event ; 43 ( 52% ) of these patients had a serious adverse event reported as possibly , probably , or de nitely related to drug therapy . 
among the serious adverse events for which a causal relation to drug therapy was suggested , only oral mucositis ( 12 [ 7% ] ) and thrombocytopenia ( nine [ 5% ] ) occurred in at least 5% of 174 patients treated . 
except for one episode of hypoxia , there were no reports of pneumonitis . 91 ( 52% ) of 174 patients needed either one ( 40 patients [ 23% ] ) or two ( 51 patients [ 29% ] ) dose reductions of temsirolimus . 
the median pfs for the time since start of treatment ( months ) number at risk igf - 1r - positive soft - tissue sarcoma igf - 1r - positive bone sarcoma igf - 1r - negative soft - tissue and bone sarcoma figure 2 : kaplanmeier curves for progression - free survival and overall survival ( a ) progression - free survival and ( b ) overall survival for all treated patients according to igf - 1r expression groups . 
igf - 1r = insulin - like growth factor - 1 receptor . vol 14 april 2013 articles p - akt ( % change from baseline ) p - s6 ( % change from baseline ) igf - 1r ( % change from baseline ) best recist response igf - 1r - positive soft - tissue sarcoma igf - 1r - positive bone sarcoma 66% 90% 60% 99% 20% 100% + 207% 97% 89% 97% + 200% 98% 100% 98% 97% 77% 73% 73% 97% + 111% progressive disease 92% 18% 34% 60% 88% 98% + 171% 40% 92% 27% 94% 65% 57% 98% 97% 99% 97% + 117% 37% 82% 45% 64% stable disease stable disease stable disease stable disease progressive disease progressive disease stable disease progressive disease progressive disease stable disease partial response stable disease stable disease stable disease progressive disease progressive disease stable disease stable disease progressive disease progressive disease stable disease stable disease stable disease stable disease stable disease progressive disease + 127% progressive disease progressive disease + 236% 70% 40% stable disease 97% 99% stable disease igf - 1r - negative soft - tissue and bone sarcoma 75% 20% 33% 50% 88% 90% + 200% 80% + 239% 33% 50% 57% 64% 88% 91% 91% 94% + 200% + 121% 48% 86% 89% + 137% data are shown for each patient ( numbered ) according to their assigned group . 
however , for ewings sarcoma and chondrosarcoma , immuno histochemistry expression had a igf - 1r 129 weeks ( 56469 ) and igf - 1r - negative disease statistically signi cant e ect on median pfs ( gure 3c and d )  . 
for patients with ewings sarcoma , the median pfs was 57 weeks ( 95% ci 43119 ) for those with igf - 1rpositive disease and and 177 weeks ( 90 to nr ) for those with ( p = 0027 , gure 3c )  . 
for patients with chondro sarcoma , the median pfs was 230 weeks ( 110 to nr ) for those with igf - 1r - positive disease and 81 weeks ( 30 to nr ) for those with igf - 1r - negative disease ( p = 0048 , gure 3d )  . 
for the eight patients with solitary brous tumours , the median pfs for the four patients with igf - 1r - positive disease was 896 weeks ( 40 to nr ) and 161 weeks ( 50 to nr ) for those with igf - 1rnegative disease , but this was not statistically signi cantly di erent ( p = 022 )  . 
this analysis included two patients with igf - 1r - positive solitary brous tumours who remained on study for 126 weeks and another who remains on study for 96 weeks . 
 median overall survival was 162 months ( 95% ci 52 to nr ) for ewings sarcoma , 146 months ( 86 to nr ) for leiomyosarcoma , not reached ( 76 to nr ) for osteosarcoma , 136 months ( 106 to nr ) for chondrosarcoma , 155 months ( 85 to nr ) for undi erentiated pleomorphic sarcoma , and 189 months ( 119 to nr ) for others ( gure 3e )  . 
in a post - hoc analysis , patients with igf - 1r - negative ewings sarcoma also had a numerical but not statistically signi cant ( p = 016 ) improvement in median overall survival ( nr , 95% ci 162 to nr ) when compared with those who were igf - 1r positive ( 140 months , 46 to nr )  . 
four of 27 ( 15% ) patients with ewings sarcoma , three of 24 ( 13% ) with osteosarcoma , one of 17 ( 6% ) with chondrosarcoma , and one of eight ( 13% ) with solitary brous tumour ( hemangiopericytoma ) had partial responses . 
of the four patients with a diagnosis of gastrointestinal stromal tumour , one ( igf - 1r positive ) had a 13% decrease in tumour size from baseline as measured by recist . discussion we undertook a phase 2 study to assess the safety and e cacy of an igf - 1r antibody and a mtor inhibitor in combination therapy in bone and soft - tissue sarcomas based on igf - 1r immunohistochemistry status . 
toxicities were consistent with those reported in the phase1 study of this combination.16 the primary endpoint of pfs at 12 weeks ranged from 31% in patients with igf - 1rpositive soft - tissue sarcoma to 39% in patients with igf - 1r - negative sarcoma . 
it has been the primary endpoint of several clinical trials including the single - arm phase 2 study of pazopanib in sarcoma , 21 a drug that is now approved by the us food and drug the administration evidence of stable disease for at least 1 year in two patients with solitary brous tumours and partial responses in patients with ewings sarcoma , osteosarcoma , solitary brous tumour , and chondro sarcoma would support an argument that these drugs could o er disease control to subsets of patients with sarcoma ( panel )  . 
this inability to show an improved outcome across all tumour histological subtypes on the basis of igf - 1r expression does point out potential limitations to using igf - 1r immuno histo chemistry as a screening tool for an igf - 1r - directed treatment . 
therefore , the inability to detect igf - 1r by immunohistochemistry in patients using the ventana antibody , who were otherwise igf - 1r positive by western blot using the cell signaling antibody , suggests that the ventana antibody might not be sensitive enough to detect the low levels of igf - 1r expression . 
by immunohistostandardising our chemistry assay and by having one sarcoma pathologist for central review of all the immunohistochemistry stained slides , we tried to avoid many of the pitfalls associated with immunohistochemistry staining . 
these pitfalls include broad inter - laboratory variability in performance of the assay , discrepancies between laboratories with high - volume versus low - volume throughput , use of di erent antibodies across sites , and deviations from recommended methods in the package insert leading to altered performance characteristics of the assays . 
there are several pitfalls associated with western blotting , especially for the detection of phosphoproteins on tumour tissues , including the handling of the tissues , the time from tumour procurement to ash freezing , the amount of tumour available for analysis , and the speci city of the antibodies used . 
in our study , to minimise several of these issues , we obtained tumour biopsies at only one site ( mskcc ) and all samples were ash frozen almost immediately upon biopsy within the interventional radiology suite . 
for the plasma correlates ( igf - 1 and igf - bp3 by elisa ) , even though they were run at one site ( mskcc ) , they were obtained at multiple cancer centres , leaving us susceptible to some of the same issues mentioned previously for tumour procurement . although there was no overall e ect of igf - 1r expression by immunohistochemistry on outcome , a post - hoc analysis of igf - 1r immunohistochemistry according to speci c sarcoma subtypes did reveal that patients with ewings sarcoma who were igf - 1r negative by immunohistochemistry had better median pfs than those who were igf - 1r positive . 
this nding suggests that in ewings sarcoma , with the present drug dosing ( 6mg / kg ) , low concentrations of igf - 1 receptor might be more easily than higher concentrations . 
alter natively , ewings sarcoma with low igf - 1r immuno histochemistry expression might have saturated vol 14 april 2013 articles 100 osteosarcoma ewings sarcoma chondrosarcoma leiomyosarcoma pleomorphic sarcoma synovial sarcoma others figure 4 : waterfall plot of best change from baseline according to the most common histological subtypes this less aggressive biological e ects . 
the higher incidence of high - grade and dedi erentiated chondrosarcomas in the igf - 1r - positive group suggests that this better outcome was not because of less aggressive histological changes . 
these results , relative to igf - 1r status for speci c sarcoma histological changes , are based on small numbers and should still be considered exploratory . inhibition of igf - 1r pappo and colleagues10 suggested that the moderate clinical bene t noted with the igf - 1r antibody r1507 as a single drug in the treatment of ewings sarcoma could have been because of under dosing of the drug.10 because the minimum dose of cixutumumab needed for is unknown , the dose reductions needed for cixutumumab - related toxicity could have in uenced the outcome of the present study . 
this point is particularly relevant to our study because over 50% of the patients needed a dose reduction of temsirolimus and this also could have had a negative e ect on the primary study outcome . 
therefore , without additional historical data linking the pharmacology of these drugs with pharmaco dynamic changes , especially at low doses , identifying how these dose reductions within the trial a ected median pfs is di cult . 
however , the western blots from our study con rmed pathway inhibition in some patients with downregulation of igf - 1r and inhibition of p - akt and p - s6 in all arms of this study , particularly within the rst cycle of therapy , suggesting a su cient biological e ect to inhibit igf - 1r and mtor signalling at the recommended phase 2 dose of cixutumumab and temsirolimus in the combination therapy . 
one possibility is that there might be other receptor tyrosine kinases that are activated in sarcoma that need to be targeted in concert with mtor to maximise p - akt inhibition.15 however , we do not know whether pathway inhibition was sustained beyond weeks 23 when the matched pair biopsies were obtained , especially at later times in the trial when dose reductions for toxicity were started . 
 we were unsuccessful in obtaining tumour tissue at the time of disease progression , and so assessment of the exact mechanism for drug resistance and tumour progression is di cult . median overall survival was over 14 months for all patients in the study . 
the only comparison that can be made is with 380 vol 14 april 2013 articles panel : research in context systematic review we searched pubmed for original research articles published in english before dec 1 , 2012 with the terms sarcoma , igf - 1r , mtor , and combinations . 
we found two phase 1 combination trials and only one of these included a dose expansion with the combination therapy at the maximally tolerated dose in patients with ewings sarcoma.16 , 17 therefore , we undertook a multicentre phase 2 clinical trial to assess the combination of an inhibitor of insulin - like growth factor - 1 receptor ( igf - 1r ; cixutumumab ) and an inhibitor of mtor ( temsirolimus ) in patients with sarcoma . 
we also examined whether igf - 1r expression by immunohistochemistry could be used to identify patient populations who would most bene t from the combination treatment . interpretation the combination of cixutumumab and temsirolimus achieved an acceptable median progression - free survival at 12 weeks in patients with both igf - 1r - positive and igf - 1r - negative bone and soft - tissue sarcoma . 
this e ect seemed to be greatest in speci c subsets of patients identi ed by immunohistochemistry for igf - 1r expression ( ie , igf - 1r - negative ewings sarcoma and igf - 1r - positive chondrosarcoma )  . 
with r1507 alone in ewings sarcoma , median pfs was 57 weeks , the recist response rate was 10% , and median overall survival was 76 months.10 in the phase 1 , doseexpansion phase of the trial of patients with ewings sarcoma treated with cixutumumab and temsirolimus , there was a 29% response rate and a median overall survival of 126 months ( median pfs not reported ) .16 with cixutumumab and temsirolimus in the present trial , even though the median pfs for the whole group was 60 weeks , the response rate was 15% and the median overall survival was 162 months . 
furthermore , an examination of patients with ewings sarcoma by igf - 1r immunohistochemistry expression suggests that pa tients who were igf - 1r negative had a better median pfs than those who were igf - 1r positive . 
 additionally , although not statistically signi cant , in a post - hoc analysis , patients with igf - 1r - negative ewings sarcoma also had a numerical improvement in median overall survival when compared with those who were igf - 1r positive . 
collectively , these results suggest that the combination therapy should be explored in future clinical studies , especially for speci c sarcoma histological subtypes where igf - 1r immunohistochemistry status might have an e ect on clinical bene t and where signs of clinical response were noted ( ie , ewings sarcoma , chondrosarcoma , and solitary brous tumour )  . contributors gks , wdt , l - xq , cra , mad , alh , lad , hxc , and rgm designed and developed the study . 
all the authors reviewed the article for intellectual content , provided comments , and gave nal approval . con icts of interest gks has received a consultancy fee from p zer and a speaker honorarium from imclone . 
we also acknowledge the funding provided by the national cancer institute under grants rc2 ca148260 ( rgm and gks ) and r01 ca140331 ( gks ) , and cycleforsurvival funding from mskcc . 
we thank noah goodman - davis and jerusa altema ( mskcc ) , who contributed substantially to the preparation of the data for this manuscript . editorial for more on framework convention on tobacco control see editorial lancet 2017 ; 389 : 226 chinas health trajectory in 2017 jan 28 , 2017 , was the start of chinese new yearthe year of the rooster . 
in the coming lunar year , china faces some big challenges that will rely on these characteristics : a rapidly ageing population ; unprecedented pollution manifesting in the highest levels of smog on record ; strained sino - american relations ; and an unusually large government reshu e with ve of seven members of the standing committee retiring and more than half of the central committee standing down . 
all of these events will likely have notable e ects on health care and cancer control policies in the years ahead . chinas position as the worlds most populous state will soon be overtaken by india . 
the communist partys maxim of more people , more power has been undermined by the four - decade social experiment in state - organised population controlmade infamous by the controversial one - child policy implemented in 1978 . 
by 2020 , china is projected to have a population of about 14 billion people , with the demographic then shifting rapidly towards a much older society , similar to that already seen in japan and elsewhere in asia . 
the 2015 abolition of the one - child policy will take many generations to shift the population back to a healthier balance between young and old , male and female , leaving the country in a perilous position in the meantime . 
major non - communicable diseases , such as cancer , diabetes , and heart disease , are mainly seen in older people , but does china have the health - care structure , or future - proof plans , to cope with the challenge of an ageing population ? the solution will lie in a need for much greater levels of screening and prevention coupled to increased provision of acute secondary and tertiary care . 
 chinas decision to increase availability of family doctors , to invest in cancer screening trials , to build 100 specialist lung cancer hospitals , and to train 1000 new lung cancer experts , is a good step forward . 
and with strained relations with the usa , which imports nearly us$500 billion worth of goods from china , any decrease in this trading partnership during the trump administration could inversely a ect the countrys ability to fund these policies . despite important inroads in to controlling lung cancer incidence via the implementation of the framework convention on tobacco control , china remains the largest consumer and producer of tobacco products , and a quarter of the populationabout 300 million peopleare smokers , and more than 730 000 new cases of lung cancer still occur annually . 
in january 2017 , smog in some cities was 40 times higher than the whos recommended safe limits , and these levels will be further exacerbated by a government decision to invest in 200 new coal - burning power plants . 
the revised environment protection law , enacted in 2015 as part of chinas long - running blue skies , green land , and clear running water strategy , introduced harsher punishments for polluters , but the unrelenting downward trends suggest much is still needed to be done . of equal importance in the coming year , china needs to extend measures that rehabilitate the role of doctors in society ; to continue support for evidence - based medicine ; and to eliminate violence against health professionals . 
certainly , government policies of the past , such as the imposition of intrauterine devices as birth control for many women , have not helped public perceptions of doctors , giving them the appearance of government agents of oppression rather than providers of a highly valuable and skilled service for the betterment of society . 
elimination of the one - child policy is a positive step in depoliticising the medical profession , as are recommendations that hospitals hire security guards , a review of doctors salaries , and criminalisation of such violence , but more is needed to eliminate patient dissatisfaction , refocus unrealistic expectations , and recoup out - of - pocket expensesall factors attributed to the increases in violence . 
 many countries face major political upheavals in 2017 , but against these destabilising forces , china must apply some of the characteristics of the rooster : observant of the populations health - care needs , and resourceful and courageous in continuing and expanding its ongoing commitment to health - care reforms , regardless of external events beyond its borders . 
 the lancet oncology vol 18 february 2017 articles gemcitabine - based or capecitabine - based chemoradiotherapy for locally advanced pancreatic cancer ( scalop ) : a multicentre , randomised , phase 2 trial somnath mukherjee * , christopher n hurt * , john bridgewater , stephen falk , sebastian cummins , harpreet wasan , tom crosby , catherine jephcott , rajarshi roy , ganesh radhakrishna , alec mcdonald , ruby ray , george joseph , john sta urth , ross a abrams , gareth gri ths , tim maughan summary background in the uk , chemotherapy is the standard treatment for inoperable , locally advanced , non - metastatic pancreatic cancer . 
we aimed to assess the activity , safety , and feasibility of both gemcitabine - based and capecitabine - based chemoradiotherapy after induction chemotherapy for patients with locally advanced pancreatic cancer . methods in this open - label , randomised , two - arm , phase 2 trial , patients aged 18 years or older with histologically proven , locally advanced pancreatic cancer ( with a tumour diameter of 7 cm or less ) were recruited from 28 uk centres between dec 24 , 2009 and oct 25 , 2011 . 
after 12 weeks of induction gemcitabine and capecitabine chemotherapy ( three cycles of gemcitabine [ 1000 mg / m on days 1 , 8 , 15 of a 28 - day cycle ] and capecitabine [ 830 mg / m twice daily on days 121 of a 28 - day cycle ] ) , patients with stable or responding disease , tumour diameter of 6 cm or less , and who performance status 01 were randomly assigned to receive a further cycle of gemcitabine and capecitabine chemotherapy followed by either gemcitabine ( 300 mg / m once per week ) or capecitabine ( 830 mg / m twice daily , monday to friday only ) , both in combination with radiation ( 504 gy in 28 fractions )  . 
this trial is registered with isrctn , number 96169987 . findings 114 patients were registered and 74 were randomly allocated ( 38 to the gemcitabine group and 36 to the capecitabine group )  . 
after 9 months , 22 of 35 assessable patients ( 629% , 80% ci 506739 ) in the capecitabine group and 18 of 35 assessable patients ( 514% , 394634 ) in the gemcitabine group had not progressed . 
median overall survival was 152 months ( 95% ci 139192 ) in the capecitabine group and 134 months ( 95% ci 110157 ) in the gemcitabine group ( adjusted hazard ratio [ hr ] 039 , 95% ci 018081 ; p = 0012 )  . 
median progression - free survival was 120 months ( 95% ci 102146 ) in the capecitabine group and 104 months ( 95% ci 89125 ) in the gemcitabine group ( adjusted hr 060 , 95% ci 032112 ; p = 011 )  . 
more patients in the gemcitabine group than in the capecitabine group had grade 34 haematological toxic e ects ( seven [ 18% ] vs none , p = 0008 ) and non - haematological toxic e ects ( ten [ 26% ] vs four [ 12% ] , p = 012 ) during chemoradiation treatment ; the most frequent events were leucopenia , neutropenia , and fatigue . 
of the 34 patients in the capecitabine group who received chemoradiotherapy , 25 ( 74% ) received the full protocol dose of radiotherapy , compared with 26 ( 68% ) of 38 patients in the gemcitabine group . 
quality - of - life scores were not signi cantly di erent between the treatment groups . interpretation our results suggest that a capecitabine - based regimen might be preferable to a gemcitabine - based regimen in the context of consolidation chemoradiotherapy after a course of induction chemotherapy for locally advanced pancreatic cancer . 
non - randomised studies that used this method of patient selection have reported overall survival of about 1519 months.9 , 1217 the international , randomised , phase 3 study lap - 07 ( nct00634725 ) , which is comparing chemoradiotherapy with chemotherapy , is expected to be reported in 2013 . intensive both uoropyrimidines and gemcitabine have been used concurrently with radiotherapy in patients with pancreatic cancer . 
fluorouracil is most widely used , but gemcitabine radiosensitisation has been used in some studies because of its systemic activity in pancreatic cancer and potent radiosensitising properties.3 , 18 three randomised , con trolled trials1921 with small numbers of patients have compared uorouracil with gemcitabine chemoradio therapy as primary treatment for locally advanced pan creatic cancer ; one19 showed a signi cant overall survival bene t for gemcitabine - based treatment , but the others20 , 21 did not show a signi cant di erence between the regimens . 
a meta - analysis of these data again suggested a survival advantage of gemcitabine compared with uorouracil chemoradiotherapy , but at the cost of greater toxicity.22 these data are , however , not conclusive enough to de ne practice , because the trials had small numbers of patients ( 1962 per trial )  . 
no study has compared the activity of gemcitabine - based chemoradiotherapy with a chemoradiotherapy regimen that uses the oral uoro uracil prodrug capecitabine for treatment of locally advanced pancreatic cancer . we designed the scalop ( selective chemoradiation in advanced localised pancreatic cancer ) trial to assess the activity , safety , and feasibility of induction chemotherapy followed by chemoradiotherapy and to identify the relative bene ts and toxicities of gemcitabine and capecitabine as concurrent chemotherapy agents . methods study design and patients the scalop trial was a multicentre , open - label , randomised , parallel , two - arm , phase 2 trial . 
patients aged 18 years or older were eligible if they had histologically or cytologically proven , locally advanced , nonmetastatic , and inoperable ( or operable but medically un t for surgery ) pancreatic cancer ; a tumour diameter of 7 cm or less ; who performance status 02 ; and adequate haematological , liver , and renal function ( full inclusion and exclusion criteria are listed in the appendix )  . 
all potential patients were discussed at regional pancreatic multidisciplinary team meetings in the presence of specialist pancreatic surgeons and radiologists for decisions about inoperability , but the exact criteria for inoperability were left to the treating multidisciplinary tea decisions with respect patients deemed medically un t for surgery were taken by the treating clinicians , on the basis of the patients comorbidities and the teams opinion about whether or not they could withstand major pancreatic surgery . response after three cycles of induction gemcitabine and capecitabine chemotherapy was assessed with a ct scan . 
patients were eligible for random allocation if they had responding or stable disease ( according to recist criteria , version 1.1 ) ; a tumour diameter of 6 cm or less ; who performance status 01 ; adequate haematological , liver , and renal function ( as for registration ) ; and no greater than 10% weight loss from baseline ( de ned as weight at registration )  . all patients had to provide written informed consent before registration and the trial protocol was approved by the uk medicines and healthcare products regulatory agency and a multicentre research ethics committee . 
the study protocol is available from the wctu website . randomisation and masking after three cycles of induction chemotherapy , eligible patients were randomly assigned in a 1 : 1 ratio to receive either gemcitabine - based or capecitabine - based chemoradiotherapy , by use of the method of minimisation with a random element ( 80 : 20 )  . 
the study had an openlabel design , so treatment allocation was not masked from patients or investigators . procedures induction chemotherapy consisted of three cycles of gemcitabine ( 1000 mg / m intravenously for 1 h on days 1 , 8 , and 15 of a 28 day cycle ) and capecitabine ( 830 mg / m orally , twice daily on days 121 of a 28 day cycle )  . 
patients eligible for randomisation were allocated to receive a further cycle of gemcitabine and capecitabine chemotherapy at the same doses as were used during induction , followed by radiotherapy in combination with either gemcitabine ( 300 mg / m once per week , total six doses ) or capecitabine ( 830 mg / m twice daily on days of radiotherapy [ monday to friday only ] ) a total dose of 504 gy in 28 daily fractions ( monday to friday only ) was delivered over 55 weeks by use of 3d conformal or intensity - modulated radiotherapy planning . dose modi cations for gemcitabine were made on the basis of neutrophil and platelet counts on the day of ( or day before ) administration , as previously described.23 capecitabine was withheld for grade 2 or higher non - haematological toxic e ects until they resolved to grade 1 ; for recurrent grade 2 toxic e ects , doses were 318 vol 14 april 2013 articles seen . 
treatment after progression was as per institutional practice , and no speci c regimen was recommended . completed subsequent management beyond the trial follow - up period was at the discretion of the treating physician , but outcome data ( death and disease progression ) were collected every 3 months for those patients who had completed the 52 - week assessment until the last patient assessment . 
pan26 results are not reported here ; a detailed quality - of - life anaysis is planned , which will include these results . this statistical analysis the primary endpoint of the trial was progression - free survival at 9 months . 
progression - free survival was chosen in preference to overall survival because , on the basis of the study by huguet and colleagues , 9 we anticipated that activity could be detected earlier and with fewer patients . a flemings single - stage design was assigned to each of the treatment groups to show worthwhile e cacy in each group separatelyie , the study was not formally powered to compare 9 - month progression - free survival between the groups . 
we judged that progression - free survival at 9 months after registration of less than 30% would not be su ciently large to warrant further investigation in a phase 3 setting , but that 50% or higher would warrant investigation . 
using flemings single - stage further 216 assessed for eligibility 114 registered 102 excluded 79 did not meet inclusion criteria 19 declined to participate 4 other reasons 40 excluded 15 progressed 10 excluded by clinician ( because of intolerance , surgery needed for complications , or weight loss ) 9 opted out 5 died 1 should not have been registered 74 randomly allocated sequentially reduced to 75% and then 50% . 
on - trial rttqa consisted of a planning assessment form , which was completed during planning for each patient and reviewed centrally before the start of radiotherapy . fed back assessments in the treatment period and during follow - up consisted of medical history , physical examination , and assessment of who performance status and toxic e ects . 
laboratory tests included haematological and biochemical tests , including tumour marker ( ca19 - 9 ) assessments at stipulated timepoints ( at registration and at 17 , 26 , 39 , and 52 weeks )  . 
contrast - enhanced ct scans of thorax and abdomen to assess response were done at baseline ( registration ) , at 13 weeks ( before randomisation ) , and at weeks 26 , 39 , and 52 . 
patients were clinically reviewed ( including full blood counts and serum renal and liver pro les ) every 4 weeks during induction chemotherapy , every week during chemoradiotherapy , and every 12 weeks thereafter , until the nal follow - up visit at week 52 . 
those not suitable for surgery were kept on trial follow - up and additional chemotherapy was not recom mended unless disease progression was 36 allocated to capecitabine group 38 allocated to gemcitabine group figure 1 : trial pro le vol 14 april 2013 articles design ( p1 = 030 and p2 = 050 , setting = 01 [ 1 - sided ] , 90% power ) , 38 participants needed to be allocated to each arwe estimated that 25% of participants would either withdraw or not be eligible for random allocation at 13 weeks after registration , and that a minimum of 102 participants would therefore need to be recruited . 
 secondary endpoints were median and 12 - month overall survival , median ( including local and distant ) progressionfree survival , toxic e ects ( as per ctcae , version 3.0 ) , objective disease response , treatment compliance , and quality of life . analysis was done with the stata 11 statistical package . 
survival times were calculated from date of registration to that when an event occurred ( ie , progression according to recist criteria or any death for progression - free survival , and any death for overall survival )  . 
event time distributions were estimated by the kaplanmeier method and capecitabine group ( n = 36 ) gemcitabine group ( n = 38 ) patients excluded at randomisation ( n = 40 ) ( hrs ) compared by use of an unadjusted log - rank test and from cox regression , both hazard ratios unadjusted and adjusted for randomisation strati cation factors ( the proportional hazards assumption was tested by use of cox - snell residuals and schoenfelds global test )  . 
e cacy endpoints were analysed according to the intention - to - treat principleie , all randomised patients who met the eligibility criteria were included in the analysis of their allocated groupwhereas the analysis of toxic e ects was restricted to patients who received at least 1 week of treatment . 
objective disease response and 9 - month progression - free survival were only assessed those patients with valid ct assessments , de ned as having been done within 4 weeks of the timepoints stipulated in the protocol ( weeks 26 , 39 , and 52 )  . 
 * two patients in the capecitabine group are excluded because they progressed during the fourth cycle of induction chemotherapy before any chemoradiation treatment could be given . table 1 : patient characteristics table 2 : treatment compliance during chemoradiotherapy 320 vol 14 april 2013 articles 14 ( 37% ) 7 ( 18% ) 5 ( 13% ) 4 ( 11% ) 1 ( 3% ) 1 ( 3% ) 10 ( 26% ) 5 ( 13% ) 4 ( 11% ) 1 ( 3% ) 6 ( 16% ) 3 ( 8% ) 3 ( 8% ) 3 ( 8% ) 2 ( 5% ) 1 ( 3% ) 1 ( 3% ) 3 ( 8% ) 1 ( 3% ) 2 ( 5% ) 3 ( 8% ) chemoradiotherapy induction chemotherapy ( all randomised patients , n = 74 ) capecitabine group ( n = 34 ) * gemcitabine group ( n = 38 ) 4 ( 12% ) role of the funding source cancer research uks clinical trials awards and advisory committee approved the trial design . 
the statistician ( cnh ) had full access to all of the data , and he and the corresponding author ( sm ) had the nal responsibility to submit for publication . results between dec 24 , 2009 , and oct 25 , 2011 , 114 patients were registered into the trial from 28 hospitals across the uk . 
74 patients were eligible induction for randomisation after three cycles of chemotherapy ; 38 were allocated to receive gemcitabinebased chemoradiation and 36 to receive capecitabinebased chemoradiation ( gure 1 )  . the baseline characteristics of age , disease location , and who performance status were well balanced between the groups , but the gemcitabine group had a higher proportion of men than did the capecitabine group ( table 1 )  . 
the median number of days from staging to registration and from registration to start of chemotherapy was low in both groups ; additionally , the median time from registration to start of radiotherapy was the same in both groups ( table 1 )  . 
however , the capecitabine group needed dose reductions or stopped chemotherapy early than did those in the gemcitabine group . fewer patients the main grade 34 toxic e ects that occurred during chemoradiotherapy are summarised in table 3 . 
more patients in the gemcitabine group than in the capecitabine group had any grade 3 or 4 toxic e ects during induction chemotherapy ( 24 [ 67% ] of 36 patients vs 17 [ 45% ] of 38 )  . 
 during chemoradiotherapy , both regi mens were well tolerated , but a smaller proportion of patients in the capecitabine group had haematological and nonhaematological grade 3 or 4 toxic e ects ( haematological : none vs seven [ 18% ] of 38 patients ; = 694 , p = 0008 ; non - haematological : four [ 12% ] of 34 patients vs ten [ 26% ] of 38 patients ; = 243 , p = 012 )  . 
 * two patients in the capecitabine group are excluded because they progressed during the fourth cycle of induction chemotherapy before any chemoradiation treatment could be given . table 3 : grade 34 toxic e ects vol 14 april 2013 articles number at risk capecitabine gemcitabine time ( months ) figure 2 : kaplanmeier estimates of progression - free survival , by treatment group capecitabine gemcitabine group ( unadjusted hr 064 , 95% ci 037109 ; logrank p = 0102 ; adjusted hr 060 , 95% ci 032112 ; p = 011 ; gure 2 )  . 
median local progression - free survival was 146 months ( 95% ci 113186 ) in the capecitabine group and 120 months ( 98140 ) in the gemcitabine survival was group . 
the pattern of disease progres sion at 12 months from registration is shown in table 5 . progres sion - free median overall survival for all registered patients ( n = 114 ) was 127 months ( 95% ci 110145 ) ; 12 - month overall survival was 529% ( 95% ci 429619 )  . 
patients who proceeded to be randomised to chemo radiotherapy ( n = 74 ) had a median overall survival of 146 months ( 95% ci 130158 ) and 12 - month survival of 775% ( 95% ci 658856 ) ; patients who did not proceed to randomisation ( n = 40 ) had a median overall survival of 81 months ( 95% ci 41105 ) and 12 - month survival of 169% ( 95% ci 69307 )  . 
median overall survival was 152 months ( 95% ci 139192 ) in the capecitabine group and 134 months ( 95% ci 110157 ) in the gemcitabine group ( unadjusted hr 050 , 95% ci 027093 ; log - rank p = 0025 ; adjusted hr 039 , 95% ci 018081 ; p = 0012 ; gure 3 )  . 
this di erence was maintained in a sensitivity analysis that included sex and ca19 - 9 concentration ( imbalanced at randomisation ) in the adjusted cox regression ( p = 0003 )  . 
12 - month overall the survival was 792% capecitabine group and 642% ( 95% ci 464775 ) in the gemcitabine group . ( 95% ci 611895 ) we assessed quality of life with the qlq - c30 questionnaire ( gure 4 , appendix )  . 
despite an apparent di erence between the treatment groups , the scores at week 23 ( immediately after completion of chemoradiotherapy ) were not signi cantly di erent ( z = 1492 ; p = 014 ; n = 48 )  . 
nor was the di erence between the changes in score from week 17 ( before chemoradiation treatment ) to week 23 signi cant ( z = 1514 ; p = 013 ; n = 45 )  . 
a detailed quality - of - life analysis is planned . no signi cant di erence in ca19 - 9 concentrations was detected between the capecitabine group and the gemcitabine group , either at baseline ( table 1 ; z = 1500 ; p = 013 ; n = 67 ) or at week 17 , immediately before chemoradiotherapy ( capecitabine median 29 u / ml ( 17170 ) ; gemcitabine median 130 u / ml ( 21251 ) ; z = 1603 ; p = 011 ; n = 58 ) , in randomised patients . 
we divided all patients into groups on the basis of whether or not their ca19 - 9 concentrations at baseline and week 17 were lower than the median , and compared overall survival ( table 6 )  . 
 higher week 17 ca19 - 9 concentrations were highly predictive of worse survival in randomised patients , but the fall in ca19 - 9 between baseline and week 17 was not . 
 22 patients ( 629% , 80% ci 506739 ) in the capecitabine group had not progressed at 9 months , compared with 18 patients ( 514% , 394634 ) in the gemcitabine group . table 4 shows the objective disease response at 26 weeks , 4 weeks after completion of chemo radiotherapy ( when response conventionally reassessed )  . 
five patients ( two from the capecitabine group and three from the gemcitabine group ) underwent resection of the primary tumour after completion of study treatmentfour of these patients ( two from each group ) remained disease free at 52 - week follow - up and one ( from the gemcitabine group ) died from postoperative complications ( appendix )  . 
full histological assessments were done for all of the resected specimens and were reported as ypt1n0 ( n = 1 ) , ypt2n0 ( n = 1 ) , and ypt3n0 ( n = 3 ) ; all had pathologically clear margins . median progression - free survival was 120 months ( 95% ci 102146 ) in the capecitabine group and 104 months ( 95% ci 89125 ) in the gemcitabine 322 vol 14 april 2013 articles capecitabine gemcitabine survival between the capecitabine and gemcitabine groups is more signi cant in patients with high ca19 - 9 at baseline ( hr 030 , 95% ci 011079 ; p = 0014 ) than in those with low baseline ca19 - 9 ( 055 , 017182 ; p = 033 )  . 
 ca19 - 9 measurements at week 17 and 26 ( ie , after chemoradiotherapy ) were available for only 43 ( 58% ) of 74 patients , which limits any further in - depth analysis . discussion our results show that induction chemotherapy followed by gemcitabine - based or capecitabine - based chemoradiotherapy are both active regimens and can be given safely . 
 the capecitabine - based regimen seems to have better safety and e cacy outcomes than the gemcitabine - based regimen , although the di erence in progression - free survival at 9 months was not signi cant ( panel )  . locally advanced pancreatic cancer has a poor prognosis and treatment advances have evolved slowly . 
survival of patients with locally advanced pancreatic cancer who are treated with chemotherapy alone , extracted from studies that combine patients with locally advanced pancreatic cancer and those with metastatic disease , ranges from 99 to 103 months.5 , 23 chemoradiotherapy for inoperable adenocarcinoma of the pancreas has been a standard treatment in the usa since a series of seminal studies from the gastrointestinal studies group in 1981.6 the relative bene t attributed to chemoradiotherapy compared with radiotherapy alone could be due in part to the extended administration of maintenance chemotherapy after chemoradiation in combined modality trial groups , which suggests that additional systemic therapy might confer advantage . 
 this strategy has not been widely used in the uk , partly because of logistical issues , but also because of a paucity of supportive evidence and the perceived toxicity of chemoradiotherapy in patients with such a poor outlook . trials in the past 67 years that have assessed chemoradiotherapy have induction chemotherapy , with chemoradio therapy given as a consolidation regimen for patients who do not develop metastases ( typically 6570% of patients )  . 
this approach enables the initiation of e ective , full - dose systemic therapy followed by intensi ed treatment at the primary site for optimum tumour control and , in some cases , downstaging to enable surgical resection . 
non - randomised trials that have used this approach have reported survival outcomes of 1419 months in this select group of patients , 9 , 13 - 17 , 20 and the results of one non - randomised study suggest that in patients with responding disease , this approach of switching to chemoradiotherapy could have better outcome than continuation of chemotherapy alone ( overall survival of 150 vs 117 months , p = 00009 ) .9 a prospective , phase 3 trial ( lap - 07 ) to assess the additional bene t of immediately after diagnosis , started with number at risk capecitabine gemcitabine time ( months ) figure 3 : kaplanmeier estimates of overall survival , by treatment group capecitabine gemcitabine number at risk capecitabine gemcitabine time ( weeks ) 26 26 figure 4 : quality of life scores scores are from the qlq - c30 questionnaire . 
in this trial , after 3 months of induction chemotherapy , responding patients have been randomly allocated to either continue the same chemotherapy regimen or to switch to a capecitabine - based chemoradiotherapy regimen similar to that used for the capecitabine group in our study . our results suggest that the overall survival with induction chemotherapy followed by consolidation chemoradiotherapy seen here in a multicentre setting accords with the results of previous single - centre studies . 
 40 registered patients did not receive chemoradiotherapy because of death ( n = 5 ) , poor general condition ( n = 10 ) , vol 14 april 2013 articles median ca19 - 9 ( iqr ) , u / ml overall survival in months ( 95% ci ) univariate multivariate * ca19 - 9 less than median ca19 - 9 median or higher hazard ratio ( 95% ci ) p value hazard ratio ( 95% ci ) p value baseline in all patients 3315 ( 751074 ) 157 ( 129165 ) ( n = 53 ) 104 ( 93117 ) ( n = 53 ) 249 ( 153403 ) < 0001 253 ( 153420 ) baseline in randomised patients week 17 in randomised patients percentage fall in ca19 - 9 between baseline and week 17 212 ( 71829 ) 44 ( 19208 ) 163 ( 152207 ) ( n = 33 ) 113 ( 97134 ) ( n = 34 ) 429 ( 214859 ) < 0001 419 ( 209840 ) 163 ( 139192 ) ( n = 29 ) 126 ( 103140 ) ( n = 29 ) 337 ( 167681 ) 0001 384 ( 167880 ) 748% ( 890 to 532 ) 146 ( 103192 ) ( n = 27 ) 140 ( 127160 ) ( n = 27 ) 126 ( 063256 ) 051 112 ( 051244 ) < 0001 < 0001 0002 0780 * for all patients variables include sex , age , and who performance status ; for randomised patients disease location is also included ( centre could not be used because of small numbers )  . table 6 : overall survival by ca19 - 9 concentration at baseline and week 17 progressive disease or ineligibility ( n = 16 ) , or patient choice ( n = 9 ) ; in these patients median survival was only 81 months ( 95% ci 41101 )  . 
however , the overall median survival of all registered patients was 127 months ( 95% 110145 ) , which is better than previous outcomes in chemotherapy - only studies ( roughly 10 months ) .4 , 5 grade 34 toxic e ects were less frequent during consolidation chemoradiotherapy than during induction chemotherapy . 
the selection of tter patients through induction treatment , limitedeld radiotherapy , conformal radiation techniques , and above all , the prospective rttqa programme will all have contributed to this favourable outcome . 
moreover , because all patients received induction chemotherapy that used gemcitabine and capecitabine , potential chemotherapy - related toxic e ects were identi ed and appropriate measures taken , including dose reduction instituted before the start of chemoradiotherapy . of the previous studies that compared gemcitabinebased and uorouracil - based chemoradiotherapy , 1921 at least one study19 and a meta - analysis22 suggested better survival outcomes with gemcitabine . 
our results showed a signi cant advantage for the secondary endpoint of overall survival in the capecitabine group compared with the gemcitabine group , and the di erence is clinically relevant , especially because of the apparently lower toxicity . 
both distant and local progression - free survival seemed to be better in the capecitabine group as well , but the di erences in progression - free survival were not signi cant . clinical the rationale behind the previous studies that compared gemcitabine with uorouracil in a chemo radiotherapy setting was based on the hypothesis that gemcitabine is a more potent radiosensitiser than uorouracil ; however , in the the radiosensitising e ect and the systemic contribution of the chemotherapy is di cult . 
the size of bene t from capecitabine in our study was similar for both distant and local progression - free survival , which might suggest that the systemic e ect accounts for the di erence . setting di eren tiating between an optimum concurrent dose of gemcitabine in conjunction with radiotherapy has not been de ned . 
in phase 12 clinical trials , once - per - week doses of gemcitabine have ranged from 250 mg / m to 1000 mg / m , and the only phase 3 trial7 to use gemcitabine as a radiosensitiser used a dose of 600 mg / that trial , 7 in which patients were randomly assigned to receive either gemcitabine alone or gemcitabine with radiotherapy ( 504 gy in 28 fractions ) , was stopped early because of poor recruitment , with 71 patients entered from eight us centres . 
survival was the chemoradiotherapy group than in the chemotherapyonly group ( 111 vs 92 months , p = 0017 ) , but at the expense of increased grade 45 toxic e ects ( 41% vs 9% )  . 
 phase 12 studies that used full - dose gemcitabine in combination with radical doses of radiotherapy have also been reported.27 , 28 although outcomes from these studies are promising and the toxicities are acceptable , the trials were done in a small number of experienced centres , and the results might not be reproducible in a large multicentre setting . slightly better in our study we used a fairly low dose of gemcitabine ( 300 mg / m once per week )  . 
this reduced dose could possibly account for the di erence in survival outcomes between the gemcitabine and capecitabine groups , since the reduction in dose of systemic therapy in the the gemcitabine group might have compromised therapy was outcome , whereas adequate systemic maintained in the capecitabine group . 
we can speculate that increasing the dose of gemcitabine chemoradiotherapy might have improved the survival outcomes in this group , but doing so would also have increased the frequency of grade 34 toxic e ects . the suggestion that the di erence in outcomes between the treatment groups in our study could have been caused by a reduction in systemic therapy in the gemcitabine group would be consistent with evidence that systemic therapy is important in the management of locally advanced pancreatic cancer , as was shown by chau ert and colleagues , 7 in whose study compromise in the systemic adjuvant chemotherapy after primary uorouracil and cisplatin - based chemoradiotherapy resulted in a poor outcome compared with chemo therapy alone . 
additionally , 324 vol 14 april 2013 articles in a retrospective series29 of 85 patients that compared outcomes in patients who received adjuvant chemotherapy after primary gemcitabine - based chemoradiotherapy with those who did not , 2 - year overall survival was signi cantly better in those who received the adjuvant treatment ( 318% vs 124% , p < 0001 )  . 
the roles of newer chemotherapy regimens such as folfirinox or of the continuation of further systemic treatment after chemoradiotherapy remain to be tested in future randomised studies . our study had several limitations . 
although our results show a clinically relevant di erence in overall survival between capecitabine - based and gemcitabinebased chemoradiotherapy , this nding should be interpreted cautiously since this outcome was not the primary endpoint and the number of patients included in the trial was small . 
data for second - line treatment after disease progression were not obtained and an imbalance between the the groups proportion of patients who received second - line treatment might have a ected the survival outcomes . 
 moreover , although randomised , the flemings design is not ideal for a direct comparison between the groups , and the trial would not have been adequately powered to detect a di erence in overall survival as the primary endpoint . 
we also acknowledge the limitations of progression - free survival as an endpoint for pancreatic cancersince the primary tumour has di use margins , accurate measurement of local progression is di cult . 
 however , nearly 70% of the patients had new - onset metastatic disease at progression . terms of the trial protocol did not specify the criteria for inoperability , with this decision left to the locoregional pancreatic team ( including the surgeon and specialist radiologist ) , in recognition of the variability in surgical practice . 
that few patients ultimately underwent operations suggests that the patients recruited to this trial had truly inoperable disease . despite its limitations , ours is the largest trial so far to report the outcome of consolidation chemoradio therapy panel : research in context systemic review we searched pubmed for research articles published in english before january 15 , 2013 , using the keywords locally advanced pancreatic cancer and chemoradiotherapy , and identi ed 179 articles . 
we identi ed two randomised trials19 , 21 that compared gemcitabine - based with uorouracil - based chemoradiotherapy and one25 that compared gemcitabine - based with paclitaxel - based chemoradiotherapy . 
this meta - analysis included one additional randomised trial26 that was not identi ed in the original pubmed search , and therefore included three randomised trials and one retrospective comparative study , 20 with a total of 229 patients . 
the results showed an overall survival advantage for gemcitabine compared with uorouracil at 12 months from randomisation ( risk ratio 154 , 95% ci 105226 , p = 003 )  . 
severe haematological toxic e ects were more frequent in the gemcitabine group . interpretation the higher toxicity of gemcitabine compared with the uorouracil prodrug capecitabine seen in our study is consistent with previous research . 
although these data should be interpreted with caution , because the di erence in the primary endpoint was non - signi cant and the number of patients small , in the setting of induction chemotherapy , capecitabine - based chemoradiotherapy is safe and e ective and might be preferable to gemcitabine - based chemoradiotherapy for patients with locally advanced pancreatic cancer . after a course of induction chemotherapy . 
 notwith standing the small number of patients in this trial , the good e cacy and toxicity pro le seems to favour capecitabine for combination with radiotherapy in this setting , which suggests that capecitabine could be favoured as a to assess new radiosensitisers or radiotherapy dose escalation . template regimen trials contributors sm , cnh , jb , tm , gg , raa , sf , am , and tc were involved in the design and development of the trial . 
all authors have seen and approved the nal drasm , tc , cj , hw , sc , rro , gr , and jb were principal investigators at centres that recruited more than 5% of patients each . con icts of interest we declare that we have no con icts of interest . acknowledgments the scalop trial was funded by cancer research uk through grant 07 / 040 and core funding at the wales cancer trials unit . 
we thank all the patients who participated in the trial ; the doctors , nurses , pathologists , and other members of the multidisciplinary teams ; and the radiotherapy and research teams from the participating centres . 
additionally , we thank nadim bashir , sarah bridges , bethan tranter , paul morris , and wendy wade for their input on the trial management group . see articles page 1009 a step towards predicting checkpoint inhibitor response in kidney cancer in this issue of the lancet oncology , samra turaljic and colleagues report a heroic undertaking , using wholeexome sequencing data from 5777 patients representing 19 solid tumour types.1 in their series , the presence of frameshift indels across this large pan - cancer cohort was associated with more tumour - specific neoantigens compared with non - synonymous single nucleotide variant ( nssnv ) mutations . 
in renal cell carcinoma , frameshift indels were more prevalent compared with in other tumour types and were associated with enhanced antigen - presenting machinery and t - cell activation . 
their analysis helps to resolve a rather perplexing translational conundrumspecifically , that patients with renal cell carcinoma , a disease with a modest mutational load , show responses to checkpoint inhibitors on par with other diseases with considerably higher mutational loads.2 in non - small - cell lung cancer , melanoma , and other highmutational burden cancers , emerging evidence supports a link between mutational load and clinical outcome.3 , 4 by contrast , results from studies linking mutational load to outcome in renal cell carcinoma are mixed at best.57 the need to identify a predictor of checkpoint inhibitor response in metastatic renal cell carcinoma has never been greater . 
efforts to develop predictive biomarkers have largely failedeg , pd - l1 expression has shown a prognostic role , but did not predict outcome with nivolumab in the phase 3 comparison of this drug to everolimus in metastatic renal clear cell . 
results of the cabosun trial , 8 a randomised , phase 2 study comparing sunitinib and cabozantinib , have shown a significant improvement in progression - free survival in intermediate - risk and poor - risk patients with cabozantinib . 
if multiple studies have positive results , the clinician will need to discern the appropriate patient for either targeted therapy alone ( eg , cabozantinib ) , targeted therapy combined with a checkpoint inhibitor , or immunotherapeutic strategies alone . despite the poor predictive value of pd - l1 in this setting , other biomarkers show early promise . 
atkins and colleagues9 have reported a t - effector gene signature , generated in the context of a randomised , phase 2 study that compared sunitinib , bevacizumab and atezolizumab , and atezolizumab alone . 
 these results suggest a requisite step for turaljic and colleagues , namely , to define the predictive value of frameshift indel load for checkpoint inhibitor response in metastatic renal cell carcinoma . 
without question , they have shown that frameshift indels occur more frequently in the context of renal cell carcinoma , and that frameshift indels are associated with substantial neoantigen immunogenicity compared production with greater with nssnv neoantigens . 
they retrospectively predicate the link between frameshift indel load and checkpoint inhibitor response on four datasets , three including patients with melanoma and one including patients with non - small - cell lung cancer . 
moreover , none of these experiences include randomisation to a non - checkpoint in response assessment and 982 vol 18 august 2017 comment inhibitor control , making it unclear whether frameshift indel load might merely be prognostic rather than predictive . 
supporting this premise , in a previous series of 100 patients with non - small - cell lung cancer treated with a non - checkpoint inhibitor , the authors of this report1 found a higher relapse - free survival in those patients with higher frameshift indel load . 
 with a burgeoning array of clinical trials juxtaposing checkpoint inhibitor combinations against vegf - directed therapies in metastatic renal cell carcinoma , there should be ample opportunity to discern the predictive value of frameshift indel load in metastatic renal cell carcinoma . 
such confirmation is essential because certain frequent frameshift indels in renal cell carcinoma ( eg , vhl , pbrm1 , and kmd5c ) might themselves play a role in predicting response to vegf - directed therapy.10 if validated in randomised trials that compare checkpoint inhibitor interventions with non - checkpoint inhibitor interventions , frameshift indel load could represent a predictive biomarker for immunotherapy benefit that has yet remained elusive in metastatic renal cell carcinoma . 
 manuel caitano maia , eddy s yang , neeraj agarwal , * sumanta k pal department of medical oncology and experimental therapeutics , city of hope comprehensive cancer center , duarte , ca 91010 , usa ( mcm , skp ) ; department of radiation oncology , university of alabama at birmingham comprehensive cancer center , birmingham , al , usa ( esy ) ; hugh kaul precision medicine institute , university of alabama at birmingham school of medicine , birmingham , al , usa ( esy ) ; and division of medical oncology , university of utah huntsman cancer institute , salt lake city , ut , usa ( na ) spal@coh.org skp reports personal fees from pfizer , novartis , ipsen , astellas , bristol - myers squibb , gentech , and roche , outside of the submitted work . 
na reports personal fees from pfizer , exelixis , cerulean pharma , medivation / astellas , eisai , merck , novartis , emd serono , clovis oncology , and genentech / roche , outside of the submitted work . 
immotion150 : a phase ii trial in untreated metastatic renal cell carcinoma ( mrcc ) patients ( pts ) of atezolizumab ( atezo ) and bevacizumab ( bev ) vs and following atezo or sunitinib ( sun )  . 
eur urol 2017 ; 71 : 40514 . all tumours are rare , but some are rarer than others the report from the rarecare consortium1 in the lancet oncology , which updates the estimates of the burden of rare cancers in europe raises questions well beyond its immediate subject matter : what is the purpose of cancer registries ; how important is the quality of their data ; how should we , in the 21st century , classify cancer ? cancer registries have a long and distinguished history . 
subsequently , their role has expanded to include investigations of the causes of cancer , planning the organisation and funding of health services , and comparing outcomes across time and geographies . 
the rarecare initiative has used data from cancer registries across europe to assess the spectrum and combined incidence of rare cancersrare is defined as an annual incidence of less than six cases per 100 000 people . 
they conclude that 24% of all new patients with cancer in the european standard population ( eu28 ) have a rare cancera figure that is almost double the incidence of 13% reported from the usa using an identical definition of rare.2 even within analyses based on data from european registries , discrepancies exist ( figure )  . 
the subject is published online july 4 , 2017 s1470 - 2045 ( 17 ) 30466 - 7 see articles page 1022 vol 18 august 2017 comment editorial fertility preservation and consent less than 5% of adults with cancer choose to protect their future fertility by having samples of their gametes frozen before undergoing treatment . 
on march 6 , 2014 , a widow won a high court case in the uk against the human fertilisation and embryology authority ( hfea ) to preserve her dead husbands sperm for future use beyond the statutory period . 
is this decision to appeal callous or fair ? warren brewer put his sperm into storage in april 2005 , before receiving cranial radiation , and consented for this sample to be kept for the statutory 10 years , which expires on april 18 , 2015 . 
in the case , his widow , elizabeth warren , and her legal team proved that brewers intention for use of the sperm was not limited to 10 years , and that the clinic had failed to make the necessary legal provisions . 
in addition , they argued that given warren was in a state of grief ( she had also lost her brother in a fatal road tra c accident just weeks before her husbands death ) , a life - changing decision on whether to have a child should not be forced on to her by a prescriptive timeframe . 
they further evoked the human rights act 1998 , which protects the right to respect an individuals private and family life that the judge interpreted to include the right for a widow to decide to become a parent by her deceased husband . the hfea argued that consent was only granted for the statutory 10 years , and that given further consent could no longer be obtained , there was no case to extend storage for up to 55 years . 
furthermore , they argued that , because the judge con rmed that legal consent was not in place for storage beyond 10 years , the judgment may have implications for other cases in which the sperm providers wishes are less clear . 
this is clearly a very sensitive case : one where both parties agreed that common sense should prevail , that warrens wishes were reasonable , but they must be achieved in a way that does not set a precedence for future abuse of the regulations , hence hfeas , excessively linguistic and technical approach in the interpretation of the law . the increasing number of people being diagnosed with cancer , and the larger proportions of younger patients , suggests the issues raised in this case are likely to become more commonespecially if this case raises awareness about the availability of fertility preservation and more patients start to make use of the services available . 
a formalised amendment to the human fertilisation and embryology act to take in the speci c circumstances surrounding cancer treatment might now be the best option , rather than allowing provisions to evolve haphazardly via precedence and case law . 
an additional legal solution is needed in the warren case to protect warrens rights to make a decision on her own terms and in her own timeframe , whilst protecting the act from abuse . 
with this in mind , the appeal , albeit unfortunate and insensitive , does seem necessary . fertility preservation cancer is an integral part of comprehensive treatment , and a nice recommendation in the uk , but the legal framework should support all eventualities . 
unfortunately , the hard truth is that many patients still die from their cancer , and if their death is at a young age , it is entirely possible that any frozen gametes might be used by their partners in the time after their death . 
 the lancet oncology vol 15 april 2014 corrections correction to lancet oncol 2013 ; 14 : 1242 correction to lancet oncol 2014 ; 15 : 606 correction to lancet oncol 2014 ; 15 : 621 rst - line metastatic rini bi , melichar b , ueda t , et al . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in figure 1 of this article , the box indicating how many patients received the intervention should have read : 652 patients received intervention . 
 this change has been made to the online version as of may 26 , 2014 . vol 15 june 2014 e253 for the bbc news story see health - 40802527 for the 2013 report on british south asian cancer patients see bmj open 2013 ; 3 : e002650 for more on cervical screening rates in the uk see bbc.co.uk / news / health - 40444170 for more on cervical cancer rates in canada see bmc public health 2016 ; 16 : 868 for the cancer prevention institute of california report see media / press - releases / 2017 / breastcanceramongasians.aspx turning taboos into action as the global burden of cancer continues to rise , disparities in cancer care remain ubiquitous . 
 what can be done to reduce the health care gap ? according to a recent news story , an increasing number of south asian women in the uk are hiding their cancer diagnosis from their relatives and friends . 
the consequences of this lonely experience are not only potentially physically harmful to the patientlate diagnosis and treatment reduces the chance of a good outcomebut also inevitably emotional and psychological . 
according to a 2013 report , british south asian patients with cancer are five - times more likely to suffer severe depression after a cancer diagnosis than their white counterparts . the taboo surrounding cancer remains a stubborn issue in several other cultural groups . 
in the uk , cervical cancer screening prevents 2000 deaths per year , but attendance has been falling ( 757% of eligible women were screened in 2011 vs 727% in 2016 ) and is lowest in ethnic minority and deprived communities . 
in addition to the practical issues voiced by many women who fail to attend screening ( eg , difficulty arranging a convenient appointment ) , women from ethnic minorities might experience several other barriers , including no awareness of the screening programme , not having english as a first language , lack of cancer education , unfamiliar terminology , embarrassment or modesty , and cultural or religious concerns about the intimate nature of the tests . 
 these logistical and emotional barriers are not confined to the uk ( comparable findings have been reported in immigrant groups in other countries , including the usa , canada , norway , and finland ) and are not limited to cervical cancera similar situation exists for breast cancer mammography screening . 
 an increasing incidence of cervical cancer and related mortality has been reported in muslim communities in high - income countries , such as canada , despite an overall decreasing incidence of the disease . 
a recent report from the cancer prevention institute of california showed that by contrast with other ethnic groups , a rising incidence of breast cancer has been reported in asian - americans in the past 15 years , with an increasing prevalence of latestage disease in filipino , south asian , and korean women . 
health communications should be modified to increase awareness of and access improve participation to screening programmes to rates , and screening and treatment options adapted to make them acceptable to specific cultural or religious needs . 
for example , self - sampled cervical testing could provide a suitable alternative to the standard invasive test , alleviating the emotional and cultural barriers that otherwise preclude screening uptake . 
globalised high - income nations could perhaps learn from some of the lowand middle - income countries in which such communities are indigenous , which are taking steps to address these issues locally . ultimately , health - care providers need to be flexible and culturally sensitive to the needs of different ethnic and racial groups , to ensure the provision of equitable cancer care in increasingly diverse communities . 
failure to do so will not only increase the growing cancer burden , but will reinforce health inequity as a social nor the lancet oncology vol 18 september 2017 1137 editorial correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections corrections correction to lancet oncol 2013 ; 14 : 199209 correction to lancet oncol 2014 ; 15 : e241 esserman lj , thompson im , reid b , et al . 
the de nition of mrd low risk in the summary should read ( undetectable mrd at the end of induction [ day 29 ] or detectable mrd [ less than 001% ] at day 29 that became undetectable by week 11 )  . 
in gure 2 and in the rst paragraph of the results section , 1732 patients were clinical standard risk , 989 patients were risk , clinical 405 patients were clinical high risk . 
also in gure 2 , 2721 patients were eligible for mrd strati cation , 820 patients had indeterminate mrd status , 808 had high - risk mrd , 1059 had low - risk mrd , 34 patients had died within 35 days or had never remitted , and 323 patients were identi ed after august , 2009 . 
for the mrd low risk patients in table 1 , the total number of patients should read 1059 , of whom 466 were female , 764 were aged 29 years , 978 were b - lineage , 673 ( 64% ) were standard nci risk , 494 ( 47% ) had a white blood cell count less than 10 109 cells per l , and 177 had a white blood cell count of 1019 109 cells per l . 
the last sentence of the sixth paragraph of the results should read additionally , we noted no di erence between patients with undetectable mrd and those with less than 0005% mrd at day 29 . 
 these corrections have been made to the online version of the article as of june 30 , 2014 . vol 15 july 2014 e308 corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 editorial for the swedish twitter study see bmj open 2013 ; 3 : e002988 for practical guidance for social media use in oncology see j oncol pract 2012 ; 8 : e11424 #trial : clinical research in the age of social media research programmes , data analysis , and conduct of clinical trials have traditionally been the preserve of clinicians and researchers . 
for example , crowdsourcing cancer research : the role of quantitative challenges was a recent topic at the american association for cancer research annual meeting in san diego on april 7 , 2014 . 
indeed , social media is empowering patients in ways that are changing how clinical research is done , but are these changes bene cial or do they undermine integrity ? in some cases , crowdsourcing is being used by researchers to actively solicit patients involvement and input into trials . 
social media can also aid trial enrolment via the action of patient support groupseg , patients of one particular disease - speci c support group on a social network site independently contacted researchers asking for more information about their rare disease . 
 unlike traditional recruitment , the site is not speci cally linked to any particular trial ; instead , it aims to provide the option of trial enrolment for any patient . 
 social networking provides another important function for patients : it gives them with a valuable support network through which they can compare their experiences and ask questions in a safe , accessible , and anonymous environment . 
third , when patients use the same social media outlets to compare information about their experiences , such fora pose a real danger to the integrity of a clinical trial . 
the exchange of personal experiences whilst enrolled in clinical trials can lead to patientsor any researchers on the same social networkto inadvertently unblind themselves , leading to knowledge of treatment allocation . 
an analysis of twitter use by swedish physicians and medical students showed that roughly 2% of tweets were unprofessional , with a small , but important , minority revealing information that could violate patient privacy . 
other clinician - led social media ventures eg , the creation of facebook pages for clinical trials raises further questions about the ownership of data and the importance of tightly restricting access to something that is ultimately hosted in a public doma furthermore , peer - to - peer conversations on social platforms might be read and misinterpreted by patients and other non - experts . 
 enrolment into a clinical trial is the best treatment option if social for patients with cancer , and networking and media can ease this process , its use should be encouraged . 
patients use of social media should be taken into account when designing trials ; patients need education about the use of social media in tandem with protocol - speci ed restrictions on the risks of sharing certain pieces of information . 
clinicians should welcome the bene ts that social media can bring in attracting more patients to trials , but should also be aware of their own use of social media . 
 the lancet oncology vol 15 may 2014 editorial for the nci report on inappropriate treatment see mayo clin proc 2013 ; 88 : 79098 for the march editorial see editorial lancet oncol ; 14 : 177 for the article on shared decision making see br j cancer 2013 ; 109 : 78087 for the perspective see n engl j med 2013 ; 369 : 397400 for the brain metastases reviews see pages e396 and e407 for the prefher trial see articles page 962 keeping patients front and centre in the era of negative results in recent years , a growing emphasis has been placed on evidence - based medicine , and medical development has increased in pace . 
a recent report from the us national cancer institute ( nci ) , published in the mayo clinic proceedings , examined all new england journal of medicine articles published between 2001 and 2010 to identify those reports addressing new or existing therapies and the associated outcomes . 
the authors concluded that a substantial number of new practices or therapies were no betteror sometimes worsethan those they were intended to replace , and many established practices were potentially harmful . 
variation occurs in the experiences of patients treated for the same cancers , the di erent communication approaches taken by doctors and perhaps a need for more standardised approaches . re ecting with widespread screening and more e ective treatments , more patients are being diagnosed with premalignant conditions , and are either surviving or living with cancer as a chronic condition . 
this question is re ected by the increasing emphasis on patientreported outcomes ( pro ) and quality of life ( qol ) data in trial design , which could be yet more patientintegrating new endpoints that have centred by more signi cance for patients , such as therapy - free interval , symptom - free interval , or survival after progression . 
indeed , in this issue of the lancet oncology , two review articles highlight the importance of having prominent pro and qol endpoints in trials of patients with brain metastases , and the prefher trial is a rare example of a pro being a primary endpoint in a trial . 
nevertheless , the rising number of negative and inconclusive studies is a drain on limited research resources and much better means to identify winnersand , more importantly , cull dead endsas soon as possible are increasingly essential if patients needs are to remain foremost in the practice of medicine . 
 the lancet oncology vol 14 september 2013 articles e ects of the addition of gemcitabine , and paclitaxelrst sequencing , in neoadjuvant sequential epirubicin , cyclophosphamide , and paclitaxel for women with high - risk early breast cancer ( neo - tango ) : an open - label , 22 factorial randomised phase 3 trial helena m earl , anne - laure vallier , louise hiller , nicola fenwick , jennie young , mahesh iddawela , jean abraham , luke hughes - davies , ioannis gounaris , karen mcadam , stephen houston , tamas hickish , anthony skene , stephen chan , susan dean , diana ritchie , robert laing , mark harries , christopher gallagher , gordon wishart , janet dunn , elena provenzano , carlos caldas , for the neo - tango investigators summary background anthracyclines and taxanes have been the standard neoadjuvant chemotherapies for breast cancer in the past decade . 
we aimed to assess safety and e cacy of the addition of gemcitabine to accelerated paclitaxel with epirubicin and cyclophosphamide , and also the e ect of sequencing the blocks of epirubicin and cyclophosphamide and paclitaxel ( with or without gemcitabine )  . methods in our randomised , open - label , 22 factorial phase 3 trial ( neo - tango ) , we enrolled women ( aged > 18 years ) with newly diagnosed breast cancer ( tumour size > 20 mm ) at 57 centres in the uk . 
patients were randomly assigned via a central randomisation procedure to epirubicin and cyclophosphamide then paclitaxel ( with or without gemcitabine ) or paclitaxel ( with or without gemcitabine ) then epirubicin and cyclophosphamide . 
207 ( 25% ) patients had in ammatory or locally advanced disease , 169 ( 20% ) patients had tumours larger than 50 mm , 413 ( 50% ) patients had clinical involvement of axillary nodes , 276 ( 33% ) patients had oestrogen receptor ( er ) - negative disease , and 191 ( 27% ) patients had her2 - positive disease . 
addition of gemcitabine did not increase pcr : 70 ( 17% , 95% ci 1421 ) of 404 patients in the epirubicin and cyclophosphamide then paclitaxel group achieved pcr compared with 71 ( 17% , 1421 ) of 408 patients who received additional gemcitabine ( p = 098 )  . 
receipt of a taxane before anthracycline was associated with improved pcr : 82 ( 20% , 95% ci 1624 ) of 406 patients who received paclitaxel with or without gemcitabine followed by epirubicin and cyclophosphamide achieved pcr compared with 59 ( 15% , 1118 ) of 406 patients who received epirubicin and cyclophosphamide rst ( p = 003 )  . 
grade 3 toxicities were reported at expected levels : 173 ( 21% ) of 812 patients who received treatment and had full treatment details had grade 3 neutropenia , 66 ( 8% ) had infection , 41 ( 5% ) had fatigue , 41 ( 5% ) had muscle and joint pains , 37 ( 5% ) had nausea , 36 ( 4% ) had vomiting , 34 ( 4% ) had neuropathy , 23 ( 3% ) had transaminitis , 16 ( 2% ) had acute hypersensitivity , and 20 ( 2% ) had a rash . 
86 ( 11% ) patients had grade 4 neutropenia and 3 ( < 1% ) had grade 4 infection . interpretation although addition of gemcitabine to paclitaxel and epirubicin and cyclophosphamide chemotherapy does not improve pcr , sequencing chemotherapy so that taxanes are received before anthracyclines could improve pcr in standard neoadjuvant chemotherapy for breast cancer . funding cancer research uk , eli lilly , bristol - myers squibb . introduction survival of patients with early breast cancer has improved substantially in the past 20 years.1 however , incidence of breast cancer has increased and continuesto be a major health proble the early breast cancer trialists collaborative group overview analyses , 2 , 3 and individual trial data have shown bene t for adjuvant anthracyclines46 and taxane - containing chemotherapy.79 progress made through large adjuvant randomised treatment trials has been relatively slow . 
follow - up is necessarily prolonged to meet the prespeci ed eventrate criteria for disease - free survival ( dfs ) and overall vol 15 february 2014 lancet oncol 2014 ; 15 : 20112 published online december 19 , 2013 s1470 - 2045 ( 13 ) 70554 - 0 see comment page 131 copyright earl et al . 
tango11 and neo - tango were designed to provide this cross reference , because both trials investigated the addition of gemcitabine to standard chemotherapy , although the sequence of chemotherapy was not addressed in tango . neo - tango was a randomised phase 3 neoadjuvant trial that aimed to assess bene ts of addition of gemcitabine to accelerated paclitaxel with epirubicin and cyclophosphamide , and also the e ect of sequencing of epirubicin and cyclophosphamide , and paclitaxel ( with and without gemcitabine ) blocks . 
gemcitabine is an e ective drug in metastatic disease12 , 13 and other neoadjuvant or adjuvant trials have addressed similar questions for antimetabolites , with gemcitabine14 , 15 or oral capecitabine.16 neo - tango was designed and started before the introduction of adjuvant trastuzumab for her2 - positive disease . methods study design and participants in the neo - tango phase 3 randomised trial , we used a 2 2 factorial design to address both the role of gemcitabine in a sequential neoadjuvant chemotherapy regimen of epirubicin and cyclophosphamide and paclitaxel , and also the sequence of administration of these treatment components , in terms of short - term and long - term outcomes in women presenting with early breast cancer . ipsilateral supraclavicular regarded hormone we enrolled women aged older than 18 years with a histological diagnosis of early invasive breast cancer , with a radiological tumour size of more than 20 mm with or without axillary involvement . 
women with in ammatory cancer , t4 tumours with direct extension to the chest wall or lymph - node skin , and involvement were eligible with any size of primary tumour . 
her2 status was regarded as positive when immunohistochemistry was 3 + , or 2 + with evidence of ampli cation of the her2 gene on uorescence in - situ hybridisation . 
other eligibility criteria were adequate cardiac function , no myocardial infarction during the previous 6 months , adequate bone marrow , hepatic , and renal function , and appropriate ecog performance status ( 02 )  . 
patients provided written informed consent . neo - tango was an investigator designed and led trial , which was granted clinical trials authorisation from the medicines and healthcare products regulatory agency ( mhra ) on june 17 , 2004 , and approved by the multicentre research ethics committee nationally on nov 1 , 2004 , and subsequently the local research ethics committees at all participating centres . 
the study was undertaken by the uk national cancer research institute ( ncri )  . randomisation and masking in our open - label trial , eligible participants were randomly allocated 1 : 1 : 1 : 1 to receive epirubicin and cyclophosphamide followed by paclitaxel , paclitaxel followed by epirubicin and cyclophosphamide , epirubicin and cyclophosphamide followed by paclitaxel and gemcitabine , or paclitaxel and gemcitabine followed by epirubicin and cyclophosphamide . 
strati cation by minimisation was undertaken by age ( 50 years and > 50 years ) , er status ( positive and negative ) , primary tumour size ( 5 cm and > 5 cm ) , clinical involvement of axillary nodes , and in ammatory or locally advanced disease . 
chemotherapy regimens used were epirubicin 90 mg / m and cyclophosphamide 600 mg / m once every 21 days , and paclitaxel 175 mg / m with or without gemcitabine 2000 mg / m once every 14 days . 
 treatment allocations were made by telephoning the cancer research uk trials unit ( birmingham , uk ) , who used their central computerised minimisation procedure to generate the patients random allocation . procedures our primary endpoint was pcr , de ned as absence of invasive breast cancer in the breast and axillary lymph nodes , after neoadjuvant chemotherapy . 
a two - reader review of pathology reports was undertaken , masked to treatment group , by the chief investigator ( hme ) and the study pathologist ( ep ) , for patients who had surgery . 
 a detailed analysis of this review process has been published elsewhere.17 residual non - invasive ductal carcinoma in situ was allowed . secondary endpoints reported here include dfs and overall survival . 
we also recorded use of growth factor support ( usually granulocyte colony stimulating factor [ gcsf ] )  . the maximum permitted dose delay or interruption was 4 weeks to allow recovery from severe toxicity or for unscheduled procedures ( eg , emergency surgery )  . if neutropenic fever or sepsis occurred after a cycle of chemotherapy , the next cycle was delayed until the absolute neutrophil count was at least 10 10 cells per l . 
 following a delay , either dose reduction of all drugs to 202 vol 15 february 2014 articles 80% , or gcsf support with 100% dose were allowed , and all remaining cycles of the same four - cycle block were given at those doses . 
for persistent thrombocytopenia , the next cycle was delayed until patients had at least 100 10 platelets per l and was reduced to 80% , maintaining this dose reduction for subsequent cycles . 
once started , prophylactic gcsf was usually continued into the second phase of chemotherapy at the discretion of the responsible physician . if grade 2 neuropathy occurred during treatment with paclitaxel , remaining doses were reduced to 135 mg / m ( gemcitabine was unchanged )  . 
her2 - negative de ned as immunohistochemistry score of 01 , or 2 , but uorescence in - situ hybridisation ( fish ) negative ; her2 - positive de ned as immunohistochemistry of 3 or 2 and fish positive . 
each tumour could have multiple types and characteristics recorded . table 1 : patient and tumour characteristics at baseline of six cycles in total , at the discretion of the treating consultant . gemcitabine was reduced to 80% in the event of grade 3 hepatic toxicity ( transaminitis ; aspartate aminotransferase or alanine aminotransferase 520 upper limit of normal [ uln ] ) on day of treatment , at clinicians discretion because transaminitis is not known to a ect gemcitabine clearance . 
we were unable to substantiate earlier concerns about gemcitabines potential for clinically signi cant hepatic impairment . cardiac toxicity was not anticipated at the cumulative doses of epirubicin of 360 mg / however , congestive cardiac failure developed , patients were investigated and treated as appropriate , epirubicin was discontinued , and other chemotherapy was given at the discretion of the treating clinician . in the event of gemcitabine - related pulmonary toxicity of ctcae grade 2 or worse , the patient was discontinued from study therapy . paclitaxel infusion was stopped if mild symptoms of skin rash , ushing , and localised pruritus occurred . 
 if severe symptoms occurred , including bronchospasm , generalised urticaria , angio - oedema , hypotension ( systolic blood pressure < 100 mm hg ) , or life - threatening infusion was stopped and anaphylaxis , paclitaxel treatment was given with intramuscular epinephrine 1 ml 1 : 1000 , intravenous steroids , and intravenous antihistamines ; rechallenge was contraindicated . surgery ( breast and axillary ) , radiotherapy , and adjuvant endocrine treatment were given according to local protocols . 
patients will continue to receive the national cancer intelligence network ( ncin ) who will monitor for dfs and overall survival . follow - up through statistical analysis our power calculations assumed that the pcr would be 20% after standard treatment ( epirubicin and cyclophosphamide followed by paclitaxel )  . 
on this basis , we aimed to randomly allocate 200 patients into each of the four treatment groups , yielding combined data for 400 patients into each group for the two questions ( ie , e cacy and safety of the addition of gemcitabine to paclitaxel plus epirubicin and cyclophosphamide treatment [ component analysis ] and order of chemo therapy regimens [ sequencing analysis ] )  . 
this would allow an absolute di erence in the pcr in excess of 10% to be detected at the 5% ( two - sided ) level of signi cance with 85% power . 
all reported p values are two - sided . vol 15 february 2014 articles for the primary analysis , we calculated pcr for all logistic treatment groups and used univariate regression to test the addition of gemcitabine and the role of sequencing . 
we used multivariate logistic regression to calculate p values for both the treatment and scheduling e ects after adjustment for prognostic factors . we calculated dfs from the date of randomisation to the date of rst event ( locoregional relapse , distant relapse , progression on neoadjuvant chemotherapy , or death ) , or to the date of censoring . 
we calculated overall survival from the date of randomisation to the date of death or to the date of each patients last clinic visit ( for women who are not known to have died )  . 
when assessing the association between pathological response and these outcomes , we calculated overall survival and dfs from date of surgery . the neo - tango protocol stated that the rst planned interim analysis of dfs and overall survival would occur when at least 120 events had occurred or when median follow - up was at least 3 years . 
the corresponding authors ( hme and lh ) had full access to all of the data and had nal responsibility for the decision to submit for publication . results between jan 18 , 2005 , and sept 28 , 2007 , we recruited 831 patients at 57 centres ; three patients were found to be ineligible after randomisation , leaving 828 for analysis ( gure 1 ; table 1 )  . 
adjusted for the ve strati cation variables ( age , er status , tumour size , clinical involvement of axillary nodes , and in ammatory or locally advanced disease )  . 
 tumour grade of each patients largest breast tumour at baseline . table 2 : rates of pathological complete response ( pcr ) 206 vol 15 february 2014 articles see online for appendix omission of the nal cycle of chemotherapy , with the patient proceeding straight to surgery . because the neo - tango protocol did not include neoadjuvant trastuzumab , we expected fewer patients with her2 - positive disease to enrol as the trial progressed . 
 107 patients enrolled in 200506 had her2 - positive disease ( 30% of the 357 tested ) compared with 84 in 2007 ( 24% of the 347 tested ; p = 019 )  . all patients had surgery ( breast and axilla ) according to local protocols and the details will form the basis of a future publication . 
all patients with er - positive disease ( 543 [ 67% ] patients were er - positive ) received appropriate adjuvant hormonal treatments and 750 patients ( 91% ) received radiotherapy treatments according to local protocols . 
141 ( 17% ) of these patients had pcr , which was much the same for patients in the epirubicin and cyclophosphamide plus paclitaxel , and the epirubicin and cyclophosphamide plus paclitaxel and gemcitabine groups ( between - group di erence 007% , 95% ci 5 to 5 ; table 2 )  . 
however , signi cantly more patients who received paclitaxel ( with or without gemcitabine ) before epirubicin and cyclophosphamide achieved pcr than did those who received epirubicin and cyclophosphamide rst ( between group di erence 6% , 05 to 11 ; table 2 )  . 
subgroup analysis by her2 status , er status , or tumour grade did not a ect the results ( table 2 , appendix )  . median follow - up was 47 months ( iqr 3751 )  . 
at the time of analysis , 167 ( 20% ) of the 828 eligible patients had died , 227 ( 27% ) had had locoregional or distant relapses , and 236 ( 29% ) had had dfs events . 
702 ( 86% ) of the remaining 812 patients received eight cycles of chemotherapy ; the main reasons for not receiving all eight cycles were toxicity ( 54 [ 49% ] of the 110 patients receiving between one and seven cycles ) , disease progression ( 28 [ 25% ] patients ) , allergic reaction to paclitaxel ( 15 [ 14% ] patients ) , poor response to chemotherapy ( seven [ 6% ] patients ) , or other reasons ( six [ 5% ] patients )  . the median cddi for the 819 patients was 97% ( iqr 9199% )  . 
no di erences between the component groups or the sequencing groups were detected ( p = 056 for component analysis and p = 018 for sequencing analysis )  . dose intensities over individual cycles did not notably deteriorate for any of the four randomised treatment groups ( appendix )  . 
more dose reductions for the fourth cycle of regimens containing paclitaxel ( with or without gemcitabine ) occurred when it was given second compared with prior administration ( 22% vs 10% , respectively ; appendix ) , and similarly for dose delays ( 15% vs 11% , respectively ; appendix )  . overall survival from surgery was longer for patients attaining pcr than it was for those who did not attain pcr ( gure 3 )  . 
grade 3 toxicities included neutropenia , muscle and joint pain , infection , neuropathy , transaminitis , fatigue , nausea and vomiting , rash , and acute hypersensitivity ( table 3 )  . 
one patient in the epirubicin and cyclophosphamide followed by paclitaxel group received only ve cycles of chemotherapy because of fatigue and anaphylaxis and then died 12 weeks later of respiratory failure ( distant recurrence with bilateral pleural e usion and extensive alveolar shadowing )  . 
 = no reported toxic e ects of this grade . table 4 : reported grade 4 severe toxic e ects discussion in our study , provision of a taxane before standard anthracycline chemotherapy was associated with a signi cant improvement in pcr , from 15% to 20% , compared with a standard anthracyclinerst sequence ( p = 003 ; panel )  . 
these ( p < 00001 ) and overall survival improvement ndings con rm the bene t of taxanerst sequencing that was noted in a large retrospective non - randomised study from the md anderson cancer center , tx , usa , 19 which reported data from 1414 patients treated with neoadjuvant chemotherapy and 1596 patients treated with adjuvant chemotherapy between 1994 and 2009 . 
 in addition all major international early breast cancer trials groups were contacted to discuss our proposed design of epirubicin and cyclophosphamide , and dose - dense paclitaxel with or without gemcitabine . 
the nsabp - b38 adjuvant trial had a similar experimental arm with dose - dense doxorubicin and cyclophosphamide , and dose - dense paclitaxel ( 175 mg / m every 2 weeks ) with or without gemcitabine ( 2000 mg / m every 2 weeks )  . 
in addition , neo - tango had a complementary adjuvant trial ( tango ) which also addressed the addition of gemcitabine . interpretation neo - tango con rms the nsabp - b38 , 14 nsabp - b40 , 15 and tango11 results , which show no bene t from the addition of gemcitabine to anthracycline and taxane - based chemotherapy treatments for early breast cancer . 
neo - tango shows a signi cant bene t from taxanerst sequencing , and is the largest randomised trial to con rm this e ect . 314 patients have been included in small randomised phase 2 adjuvant trials2024 and 276 patients have been included in neoadjuvant trials2528 addressing taxane and anthracycline sequencing . 
some of these studies report more dose reductions of taxane when anthracyclines are given rst , 2123 , 25 and one randomised neoadjuvant study showed a non - signi cant increase in incidence of pcr for taxanerst sequencing.27 indirect evidence from neoadjuvant randomised studies for taxanerst sequencing comes compared uorouracil , epirubicin , and cyclophosphamide with docetaxel followed by epirubicin and docetaxel . 
however , the neo - tango analysis showed no sequence - speci c di erence in cddi to explain this taxanerst sequence result . 10994 , 28 which from eortc preclinical and clinical studies have suggested mechanisms to explain the bene t of early receipt of taxanes . 
taghian and colleagues26 drew attention to increases in interstitial uid pressure and improved oxygenation within breast tumours after neoadjuvant paclitaxel , which might allow increased concentrations of anthracyclines to accumulate within tumour tissue when given afterwards . 
in addition , preclinical data show that in breast cancer cells with heat shock protein 27 overexpression , a paclitaxel then doxorubicin sequence is more e ective at cell killing than the more standard doxorubicin then paclitaxel sequence.31 taxanerst sequences allow early treatment with concomitant trastuzumab and bevacizumab , which might provide additional therapeutic advantage , shown for trastuzumab in the finher study.32 both the nsabp - b4015 and artemis33 trials of bevacizumab have adopted taxanerst sequencing for this reason . 
because all patients receive both the taxane and anthracycline components , taxanerst sequencing could be considered in all similar block - sequential adjuvant and neoadjuvant protocols . neo - tango con rms the result of tango11 and shows no signi cant bene t from addition of gemcitabine to a combination that already contains anthracycline , cyclophosphamide , and paclitaxel . 
however , gemcitabine has shown promising results in patients with metastatic disease when added to paclitaxel in the rst - line relapse setting.13 much the same results have already been reported in the adjuvant nsabp - b38 , 14 and neoadjuvant nsabp - b4015 studies . 
 gemcitabine was given at 666 mg / m per week ( compared with 1000 mg / m per week in neotango and nsabp - b38 ) and docetaxel doses were reduced to 75 mg / m , and showed no bene t in terms of pcr . 
in neo - tango , we noted a non - signi cant increase in pcr after the addition of gemcitabine in patients with highgrade disease ( table 2 )  . paclitaxel was delivered every 14 days at 175 mg / m ( with or without gemcitabine 2000 mg / m )  . 
this dose - dense protocol was delivered without any reported delays in 82% of paclitaxel - containing cycles and only 8% of cycles required growth factor support to maintain dose intensity . 
the use of neoadjuvant or adjuvant weekly paclitaxel is now often used as standard at 80 mg / m per week and therefore the taxanerst sequencing bene t seen in neo - tango with paclitaxel at 875 mg / m per week , is close to standard practice across the world . whether pcr in neoadjuvant trials can be a surrogate endpoint for dfs and overall survival has been debated . 
 von minckwitz and colleagues meta - analysis34 of 6377 patients in the german breast group and abobsg neoadjuvant chemotherapy the prognostic value of not achieving a pcr is most dependent on the molecular subtype of the original trials showed that 210 vol 15 february 2014 articles trastuzumab , whereas none of tumour . 
for luminal a subtype , 35 a meta - analysis included 46% of patients in this category with pcr of 89% , whereas neo - tango had 29% luminal a patients with pcr of 35% . 
in addition , 662 ( 50% ) of 1327 patients with her2 - positive disease in the meta - analysis received the neoadjuvant 187 patients with her2 - positive disease in neo - tango did . 
the metaanalysis shows pcr of 358% in 911 patients , although in a recent trial ( gepar quinto ) , 36 663 patients with triplenegative breast cancer had a pcr of 279% , increasing to 393% chemotherapy . 
the pcr for 94 such patients in neotango was 39% with the addition of gemcitabine and 40% with taxanerst sequence . addition of bevacizumab after the in the z1040 - alliance neoadjuvant study , 37 280 patients with her2 - positive breast cancer were randomly allocated to receive standard uorouracil , epirubicin , and cyclophosphamide followed by weekly paclitaxel with trastuzumab ( pcr in the breast 565% ) , and a taxanerst sequence with concurrent weekly trastuzumab throughout ( pcr in the breast 542% )  . 
however in neotango , 187 patients with her2 - positive disease had a pcr for taxanerst sequence of 26% compared with 17% for standard sequence ( p = 003 ; table 2 )  . 
notably , in neotango , in 121 er - positive , her2 - positive women , pcr was 28% for taxanerst sequencing and 9% for anthracyclinerst sequencing , and in 66 er - negative , her2 - positive women pcr was 23% for taxanerst sequencing and 32% for anthracyclinerst sequencing . 
however , the di erences between the neotango results and z1040 could be explained by the absence of neoadjuvant trastuzumab in neo - tango . the association a recent meta - analysis38 by the us food and drug administration ( fda ) con rms the strong correlation between pcr and dfs and overall survival in patients achieving a pcr , and this association was con rmed in neo - tango . 
 the fda proposed that pcr in neoadjuvant trials in highly proliferative breast cancers could now contribute to accelerated drug approval in these types of early breast cancer.39 this proposal is a landmark in neoadjuvant chemotherapy trials for highly proliferative breast cancer , and will facilitate more rapid introduction of new agents for this subtype . 
randomised neoadjuvant trials of chemotherapy in combination with target - directed novel agents will be able to focus on high proliferation molecular subtypes ( er - negative , her2 - positive , high grade , and patients with germline brca mutations ) in which the association between pcr and dfs and overall survival is expected to be correlated . 
 however , indicates the fda meta - analysis also subgroups of breast cancer with lower proliferative potential ( ie , er - positive , her2 - negative , low and intermediate grade ) that have a better prognosis independent of pcr . 
in these groups , the response to chemotherapy is poor and pcr is low but the long - term outcome is good , and survival is in uenced more by subsequent adjuvant hormonal treatment . 
in neotango , patients from all the di erent prognostic groups were included , and therefore the pro le of the trial population will weaken the correlation between pcr and long - term outcomes for the group as a whole . 
for patients with a previously known poor prognosis , who have high pcr incidence , a robust and reliable correlation will probably emerge between pcr and longer - term outcome . contributors hme , a - lv , lh , gw , jd , and cc designed the study and wrote grant applications . 
all authors collected data , revised the report and agreed to submit the paper for publication . con icts of interest this project was funded by cancer research uk ( project grant c57 / a4180 , 2004 - 2009 ) and was supported by the national cancer research network . 
all other authors declare that they have no con icts of interest relevant to this publication . acknowledgments we acknowledge 88 investigators and their teams from 57 participating centres who entered patients in neo - tango . 
we also thank the members of the data and safety monitoring board ( i craig henderson [ university of california , san francisco , ca , usa ] , luca gianni [ unit of new drugs and innovative therapies , department of medical oncology , san ra aele hospital , irccs , milan , italy ] , and mark f brady [ gynecologic oncology group statistical & data center , roswell park cancer institute , bu alo , ny , usa ] ) , and trials unit sta for the phase 3 coordination ( cancer research uk clinical trials unit , birmingham , uk ) , translational coordination ( university of cambridge , addenbrookes hospital , cambridge , uk ) , and statistical analysis ( warwick clinical trials unit , coventry , uk )  . comment lancet oncol 2014 published online april 3 , 2014 s1470 - 2045 ( 14 ) 70137 - 8 see articles page 631 exploring better strategies for egfr antibodies in colon cancer treatment of advanced colon cancer has improved over the past 15 years . 
 the combination of chemotherapy and biological drugs including anti - egfr or anti - vegf antibodiesfor rst - line treatment , as well as the sequencing of di erent active drugs as disease progresses , can signi cantly improve outcomes.1 median survival of patients included in clinical trials is often more than 2 years . 
patients with initially unresectable metastatic disease limited to the liver can become resectable after treatment , with an opportunity for cure.2 nevertheless , despite these advances , the optimal treatment for patients with advanced colorectal cancer in clinical practice is not yet de ned . 
patients with all ras wild - type tumours bene t greatly from treatment with the anti - egfr antibodies cetuximab and panitumumab , whereas these drugs are harmful to patients with mutations in ras.3 , 4 moreover , no validated predictive biomarkers have been identi ed for antiangiogenic drugs . 
 in this setting , harpreet wasan and colleagues5 assessed two cetuximab regimens in combination with intermittent chemotherapy with folfox ( folinic acid and oxaliplatin followed by bolus and infused uorouracil ) as the backbone in a randomised phase 2 trial . 
although oxaliplatin is halted when neurotoxicity occurs , or after 6 months of therapy , uoropyrimidines and biological drugs are usually maintained until disease investigators in the coin - b trial , the progression . 
in the maintenance cetuximab group , after 12 weeks of folfox all patients continued with weekly cetuximab and only on recist progression was folfox reintroduced . the outcomes in each group in coin - b should not be compared , since each group was powered as a separate phase 2 trial . 
the primary outcome was failure - free survival at 10 months among patients who completed 12 weeks of treatment without progression , death , or leaving the trial for other reasons . 
this measure was met for both groups ( 50% for the intermittent cetuximab group and 52% for the continuous cetuximab group ) in patients who had wild - type kras . 
the ideal approach would be to select from all patients with wild - type genes those with tumours that are egfr - driven and which would therefore bene t most from complete inhibition of efgr . 
some attempts at an e ective classi cation have already been made , but further validation in clinical trials is needed.79 another subject for further study is the dynamic process of clonal evolution in tumours . 
under the selection pressure of continuous treatment , emerging ras mutant clones could cause resistance to anti - egfr antibodies.10 intermittent treatment might help to prevent the emergence of such clones . 
liquid biopsies might identify the emergence of mutant clones and might also be useful for designing trials of biological treatments.11 we agree with the coin - b investigators that their results cannot be translated into clinical practice without further validation in randomised phase 3 trials . 
patients with egfr - dependent tumours might need chemotherapy for only a short induction period followed by cetuximab vol 15 may 2014 comment published online march 20 , 2014 s1470 - 2045 ( 14 ) 70116 - 0 see articles page 640 maintenance or reintroduction on progression . 
analysis of kras / nras and braf mutations in fire - 3 : a randomized phase iii study of folfiri plus cetuximab or bevacizumab as rst - line treatment for wild - type ( wt ) kras ( exon 2 ) metastatic colorectal cancer ( mcrc ) patients . 
intermittent chemotherapy plus either intermittent or continuous cetuximab for rst - line treatment of patients with kras wild - type advanced colorectal cancer ( coin - b ) : a randomised phase 2 trial . 
j clin oncol 2014 ; 32 : 57986 . can noah guide us to improved survival in breast cancer ? introduction of adjuvant therapy with the monoclonal antibody trastuzumab has been the most signi cant advance in the management of women with early stage her2 - positive breast cancer , with improvement of disease - free and overall survival in these patients with a biologically aggressive subtype of the disease.14 for patients with large operable or locally advanced breast cancer , induction ( neoadjuvant ) chemotherapy is a standard approach . 
the noah trial5 established for the rst time that , in women with her2 - positive locally advanced or in ammatory breast cancer , addition of trastuzumab to neoadjuvant chemotherapy signi cantly increased the pathological complete response ( pcr ) compared with chemotherapy alone ( 35% vs 15% )  . 
in the lancet oncology , luca gianni and colleagues report the long - term results from noah.6 the updated results show that the bene t from addition of trastuzumab to chemotherapy in achievement of pathological complete response in the neoadjuvant setting translated into a signi cant e ect on the primary endpoint of event - free survival , with an unadjusted hazard ratio for event - free survival between the two randomised her2 - positive treatment groups of 064 ( 95% ci 044093 , p = 0016 )  . 
 furthermore , the investigators report an improvement in overall survival.6 this study has helped to de ne the role of neoadjuvant trials as an appropriate setting for assessment of novel targeted therapies in subsets of early stage breast cancer . the key to the success of this trial was appropriate patient selection for assessment of the targeted therapynamely those with her2 - positive disease . 
 despite the small study size and subsequent crossover after the approval of adjuvant trastuzumab in 2005 that potentially limited the ability of the noah trial to show a bene t on overall survival , a sensitivity analysis to account for the e ect of crossover still showed a signi cant reduction in risk of death with the addition of trastuzumab to chemotherapy . 
patients allocated to neoadjuvant trastuzumab in this trial continued the drug in the adjuvant setting for 1 year , such that improvements in event - free survival and overall survival could have been a ected by trastuzumab given after surgery . 
however , the most relevant nding from this updated analysis is that for those patients who achieved pathological complete response after neoadjuvant therapy , the hr for eventfree survival by treatment group was 029 ( p = 00135 ) , which favours patients given trastuzumab , thus showing the signi cant e ect of neoadjuvant therapy with this 550 vol 15 may 2014 corrections correction to lancet oncol 2014 ; 15 : 38 , 43 , 44 correction to lancet oncol 2014 ; 15 : 11422 gatta g , botta l , rossi s , et al . 
lancet oncol 2014 ; 15 : 11422the last sentence of the findings in the summary should have read : the most common grade 3 or 4 adverse events were fatigue ( 97 [ 14% ] of 697 patients allocated zoledronic acid vs 98 [ 14% ] of 704 allocated ibandronic acid ) , increased bone pain ( 91 [ 13% ] vs 85 [ 12% ] ) , joint should receptor pain ( 41 [ 6% ] vs 38 [ 5% ] ) , infection ( 31 [ 5% ] vs 23 [ 3% ] ) , and nausea or vomiting ( 38 [ 5% ] vs 41 [ 6% ] )  . 
in the per - protocol population in table 1 , in the ibandronic acid group , the number of men should read 11 ( 2% ) , the number of patients the with unknown read status 55 ( 8% ) , the number of patients with unknown pr status should read 283 ( 43% ) , and the number of patients with unknown her2 status should read 212 ( 32% ) ; in the zoledronic acid group , the number of patients with unknown pr status should read 277 ( 41% ) and the number with unknown her2 receptor ( 32% )  . 
 status should read 217 ibandronic acid group ( n = 704 ) zoledronic acid group ( n = 697 ) grade 12 grade 3 grade 4 grade 5 total ( % ) grade 12 grade 3 grade 4 grade 5 total ( % ) any adverse event 674 ( 96% ) 667 ( 96% ) 10% frequency in either group abdominal pain altered taste anaemia anorexia breathlessness constipation diarrhoea dry mouth dyspepsia fatigue fever or in uenzalike symptoms headache hypocalcaemia hypomagnesaemia hypophosphatemia infection joint pain muscle pain oedema other pain nausea or vomiting pins and needles renal impairment increased bone pain other adverse events of interest osteonecrosis of the 199 ( 28% ) 177 ( 25% ) 221 ( 31% ) 177 ( 25% ) 246 ( 35% ) 103 ( 15% ) 121 ( 17% ) 222 ( 32% ) 266 ( 38% ) 248 ( 35% ) 544 ( 77% ) 158 ( 22% ) 80 ( 11% ) 83 ( 12% ) 80 ( 11% ) 435 ( 62% ) 125 ( 18% ) 390 ( 55% ) 301 ( 43% ) 410 ( 58% ) 170 ( 24% ) 170 ( 24% ) 215 ( 31% ) 172 ( 24% ) 5 ( < 1% ) 176 ( 25% ) 236 ( 34% ) 208 ( 30% ) 254 ( 36% ) 104 ( 15% ) 140 ( 20% ) 207 ( 30% ) 265 ( 38% ) 176 ( 25% ) 551 ( 79% ) 280 ( 40% ) 222 ( 32% ) 77 ( 11% ) 80 ( 11% ) 72 ( 10% ) 428 ( 61% ) 136 ( 20% ) 398 ( 57% ) 303 ( 43% ) 417 ( 60% ) 156 ( 22% ) 171 ( 25% ) 202 ( 29% ) 226 ( 32% ) 9 ( 1% ) data are number of patients experiencing the event ( highest grade reported )  . 
toxic e ects include serious adverse events . table 2 : toxic e ects in randomised patients vol 15 february 2014 for more on jeremy hunt and completely unacceptable problems see co.uk / news / health - 38926697 for more on spending on the nhs see news / health - 38887694 for more on the merger of the canadian cancer society and the canadian breast cancer foundation see theglobeandmail.com / news / national / rapid - donation - dropforces - merger - of - canadiancancer - society - breast - cancerfoundation / article33864407 / for more on crowdfunding see health - 38858898 mind the gap : charity and crowdfunding in health care on feb 10 , 2017 , the uks secretary of state for health , jeremy hunt , said the national health service faces completely unacceptable problems , ranging from missed turnaround targets for patients attending accident and emergency departments to delayed operations and soaring costs . 
the burgeoning ageing population means that treating diseases of elderly people , such as cancer , have unique challenges that cannot be overcome solely by increasing health - care budgets . 
given the rising global burden of cancer , how can publicly funded health - care systems address the shortfall in cancer care services ? gaps in public services have often been filled by charities . 
in several countries , cancer charities are federally regulated to prevent mismanagement and exploitation of public funds , and have a tradition of working with governments to support patient care and research . 
for example , in canada , despite the existence of a universal health - care system , cancer charities have propped up cancer care for decades , plugging gaps in home care , travel costs , research funding , and palliative care , as well as helping patients navigate the complexities of the health system itself . 
although several provinces do not have a cancer care plan , the canadian cancer society routinely produces one for each province , in addition to working with several government agencies to create a federal strategy . 
 however , ideally charities should provide extra services and assistance in times of crisis , rather than providing basic services integrated into a health - care syste this overreliance on charity in canada has potentially perilous consequences because of the increasing budgetary strain on charities . 
 these two charities together fund more than 10% of all canadian cancer research , and their combined spending on all services has fallen by can$24 million in the past 4 years . 
the overburdened health - care system is unlikely to be able to pick up the slack , placing the residual financial responsibility on patients themselves . faced with governments struggling to rectify this shortfall in services and finding charities unable to help , patients are increasingly turning to crowdfunding to support their care . 
the online fundraising platform justgiving.com reported a seven - times increase in the number of appeals set up for patients with cancer since 2015 ; more than gb45 million was raised in 2016 , compared with 530 000 in 2015 . 
although fundraising for patients requiring novel , rare , or expensive treatments isnt new , the phenomenon of online crowdfunding is different from that done offline in the past , where money was often raised for prohibitively expensive , but effective , treatments suggested by health - care providers . 
increasingly , patients with more common diseases are taking health care into their own hands , seeking treatments that might not only be unavailable due to cost , but also absent of clinical benefit . 
crowdfunding for cancer care is also completely unregulated , lending the system itself to abuse , both by those creating false cancer claims and by those advertising unsubstantiated therapies . what are reasonable , viable alternatives ? health - care systems need to improve integration with social care to decrease overreliance on emergency care , which in turn will ensure efficient hospital discharge , outpatient management , and longitudinal care . 
moreover , publicly funded health care does not mean free care : the public are paying stakeholders in a large service project and as such are entitled to an efficient , transparent , and effective value - based syste the lancet oncology vol 18 march 2017 editorial articles purged versus non - purged peripheral blood stem - cell transplantation for high - risk neuroblastoma ( cog a3973 ) : a randomised phase 3 trial susan g kreissman , robert c seeger , katherine k matthay , wendy b london , richard sposto , stephan a grupp , daphne a haas - kogan , michael p laquaglia , alice l yu , lisa diller , allen buxton , julie r park , susan l cohn , john m maris , c patrick reynolds , judith g villablanca summary background myeloablative chemoradiotherapy and immunomagnetically purged autologous bone marrow transplantation has been shown to improve outcome for patients with high - risk neuroblastoma . 
we did a randomised study of tumour - selective pbsc purging in stem - cell transplantation for patients with high - risk neuroblastoma . methods between march 16 , 2001 , and feb 24 , 2006 , children and young adults ( < 30 years ) with high - risk neuroblastoma were randomly assigned at diagnosis by a web - based system ( in a 1 : 1 ratio ) to receive either nonpurged or immunomagnetically purged pbsc . 
all patients were treated with six cycles of induction chemotherapy , myeloablative consolidation , and radiation therapy to the primary tumour site plus metaiodobenzylguanidine avid metastases present before myeloablative therapy , followed by oral isotretino pbsc collection was done after two induction cycles . 
pbsc were collected from 229 patients from the purged group and 236 patients from the non - purged group , and 180 patients from the purged group and 192 from the non - purged group received transplant . 
toxic deaths occurred in 15 patients during induction ( eight in the purged group and seven in the non - purged group ) and 12 during consolidation ( eight in the purged group and four in the non - purged group )  . 
the most common adverse event reported was grade 3 or worse stomatitis during both induction ( 87 of 242 patients in the purged group and 93 of 243 patients in the non - purged group ) and consolidation ( 131 of 177 in the purged group vs 145 of 191 in the non - purged group )  . 
serious adverse events during induction were grade 3 or higher decreased cardiac function ( four of 242 in the purged group and ve of 243 in the non - purged group ) and elevated creatinine ( ve of 242 in the purged group and six of 243 non - purged group ) and during consolidation were sinusoidal obstructive syndrome ( 12 of 177 in the purged group and 17 of 191 in the nonpurged group ) , acute vascular leak ( 11 of 177 in the purged group and nine of 191 in the non - purged group ) , and decreased cardiac function ( one of 177 in the purged group and four of 191 in the non - purged group )  . interpretation immunomagnetic purging of pbsc for autologous stem - cell transplantation did not improve outcome , perhaps because of incomplete purging or residual tumour in patients . 
non - purged pbsc are acceptable for support of myeloablative therapy of high - risk neuroblastoma . funding national cancer institute and alexs lemonade stand foundation . introduction high - risk neuroblastoma has a high rate of recurrence , most commonly in bone and bone marrow.1 results from the childrens cancer group ( ccg ) - 3891 trial2 showed that myeloablative chemotherapy with rescue with immunomagnetic bead purged autologous bone marrow improved outcome compared with conventional dose chemotherapy . 
 blood has no or fewer neuroblastoma cells detectable by immunocytology even when bone marrow is positive.5 ( qrtpcr ) can detect quantitative real - time pcr neuroblastoma mrna in pbsc , 68 although the e ect of infusing these pbsc has not been de ned . 
we report the results of the randomised childrens oncology group ( cog ) a3973 trial , which compared outcomes for high - risk neuroblastoma patients who received autologous purged versus non - purged pbsc after myeloablative chemotherapy . 
to our knowledge , this is the rst randomised study in any cancer to evaluate the e ect of tumour - selective pbsc purging . methods study design and participants this phase 3 trial was open from feb 9 , 2001 , to march 31 , 2006 , for children with high - risk neuroblastoma . 
patients or parents or guardians provided written informed consent according to national cancer institute and local institutional review board guidelines . patients were enrolled from 95 cog member institutions in the usa ( 420 ) and canada ( 66 )  . 
eligible patients had high - risk neuroblastoma according to the childrens oncology group ( cog ) criteria , including previously untreated neuroblastoma in patients younger than 1 year with international neuroblastoma staging system9 ( inss ) stage 3 , 4 , or 4s mycn ampli ed tumours and , in children aged 1 year or older , stage 4 tumours , stage 3 tumours with either unfavourable histology or mycn ampli cation , stage 2 tumours with unfavourable histology and mycn ampli cation , and initially low - risk patients treated with surgery only who later progressed with metastatic disease.9 we excluded patients aged 1218 months with stage 4 mycn nonampli ed favourable histology , and hyperdiploid tumours after an amendment in may , 2004.10 additional eligibility criteria included age up to 30 years , no previous history of chemotherapy , registration on companion biology study , ability to tolerate pbsc collection , and adequate cardiac , liver , and renal function . 
 tumours and randomisation and masking patients were randomly assigned to treatment at study enrolment using the cogs online remote data entry system , which assigned treatment group in real - time based on the balance existing at that time , within blocks of size four . 
the method was random until such time as a random assignment exceeded the prespeci ed margin of two within a block , and only then did the method become deterministic . 
patients were randomly assigned ( ratio 1 : 1 ) to receive either purged pbsc or non - purged pbsc at study entry ; patients and treating physicians were not masked to this assignment . 
randomisation was strati ed into blocks by international neuroblastoma staging system ( inss ) stage , 9 age at diagnosis ( < 365 days or 365 days ) , mycn gene status ( ampli ed or nonampli ed ) , and international neuroblastoma pathology classi cation ( inpc ; unfavourable or favourable ) .11 procedures all patients were prescribed identical chemotherapy , radiotherapy , and post - myeloablative isotretinoin ( gure 1 )  . 
 patients without progressive disease and adequate organ function received myeloablative carboplatin , etoposide , and melphalan , 12 with dose adjustment for glomerular ltration rate ( gfr ) lower than 100 ml / min per 173 m.13 after local irradiation , patients could enrol in the cog anbl0032 trial isotretinoin plus chimeric anti - gd2 monoclonal antibody ch14.18 , interleukin 2 , and gm - csf versus isotretinoin alone , 14 with randomisation strati ed by assigned arm of this study . 
we assessed response using the international neuroblastoma criteria.9 we graded adverse events using the national cancer institutes common toxicity criteria , version 2.15 reporting was required for all grade 35 toxic e ects ( non - targeted )  . 
 to monitor safety during the study , the protocol required reporting of all grades of speci c organ function and infectious toxic e ects ( targeted )  . response pbsc were collected after two induction cycles regardless of histological tumour content in the bone marrow . 
requirements to proceed to consolidation were : immunocytology - negative pbsc with minimum of 1510 cd34 cells per kg for non - purged pbsc or minimum of 110 viable cd34 cells per kg for purged pbsc . 
we determined viability on a thawed purged pbsc aliquot using trypan blue.16 patients with insu cient purged pbsc could receive non - purged pbsc ( or purged bone marrow if non - purged pbsc also insu cient ) meeting protocol criteria . 
we de ned neutrophil engraftment as the rst of three consecutive absolute neutrophil counts of more than 500 cells per l ; and platelet engraftment as the rst of three consecutive platelet counts of more than 20 000 without transfusion . institution and transplant the non - purged pbsc were cryopreserved at collecting sites . 
for purged pbsc , heparinised pbsc were transported overnight at ambient temperature to a the day after centralised leukapheresis according to us food and drug administration ( fda ) ide# bb - ide 2259 . 
pbsc were mixed with 200300 mg of carbonyl iron per 10 total laboratory and purged 1000 vol 14 september 2013 articles cells to remove phagocytic cells and decrease the number of immunomagnetic beads required . 
remaining cells were mixed with immunomagnetic beads using ve monoclonal antibodies targeting neuroblastoma cell surface antigens ( 459 , hsan 12 , ba - 1 , hnk - 1 , and 126 - 4 ; appendix )  . 
 magnetic beads and attached cells were removed using samarium cobalt magnets.16 purged samples were suspended in l15 containing human serum albumin 10% volume / volume ( central lab , blood transfusion service , swiss red cross , bern , switzerland ) , hetastarch 15% weight / volume , and dmso 10% volume / volume ( cryoserv , ben venue laboratories inc , bedford , oh , ( baxter - fenwal , usa ) deer eld , nj , usa )  . 
cryopreserved products were shipped to transplant centres in mve ln2 dry shippers with constant temperature monitoring by overnight air delivery . in cryocyte freezing bags to detect neuroblastoma cells in pbsc , immuno cytology and tlda assays were done on a pbsc aliquot from day leukapheresis on all patients before purging . 
immunocytology used monoclonal antibodies against cell surface antigens ( 126 - 4 , 390 , 459 , hsan12 , and bw575 ) .17 , 18 the tlda assay quanti ed chga , dcx , ddc , phox2b , and th mrna expression . 
 we deemed results to be detectable if one or more of the ve genes had a cycle threshold ( ct ) value lower than 40 and to be undetectable if no signal was detected for any genes after 40 cycles ( ct = 40 )  . 
we did a second analysis of the same data using only phox2b and th mrna expression to de ne detectable samples ( appendix )  . statistical analysis analyses were done by intention to treat . 
we targeted an enrolment of 486 patients , which would provide 80% power for a one - sided log - rank test of superiority of the purged group over the non - purged group at a level of 005 , able to detect a 9% improvement in 2 - year eventfree survival ( 38% vs 47% )  . 
 we did an intention - to - treat sequential monitoring of the trial , and considered early stopping if the groups proved19 or would never prove20 to be signi cantly di erent , or if the conditional power fell under 20% . 
we calculated the relative risk as the ratio of non - purged to purged using the planning variables for 2 - year event - free survival , and under the alternative hypothesis , it would equal 133 . 
the fleming - harrington - obrien20 lower ( futility ) boundary induction consolidation ahsct radiotherapy isotretinoin pbsc harvest pbsc infusion at least 48 h after cem induction chemotherapy cycles : 1 , 2 , 4 , 6 cyclophosphamide doxorubicin vincristine cycles : 3 and 5 cisplatin etoposide 21 g / m per day intravenously 2 days 25 mg / m per day intravenously continuous infusion 3 days 067 mg / m per day intravenously continuous infusion 3 days 50 mg / m per day intravenously 4 days 200 mg / m per day intravenously 3 days consolidation chemotherapy ahsct ( cem ) melphalan carboplatin etoposide g - csf 70 mg / m per day intravenously 3 days 425 mg / m per day intravenously 4 days ( if gfr 100 ml / min per 173 m ) adjust dose to auc 41 per day using calvert formula ( if gfr < 100 ml / min per 173 m ) 338 mg / m per day intravenously 4 days ( if gfr 100 ml / min per 173 m ) 200 mg / m per day intravenously 4 days ( if gfr < 100 ml / min per 173 m ) 5 g / kg per day until anc > 2000 l for 3 days fractionated radiotherapy ( 2160 cgy ) given in 12 equal fractions of 180 cgy per fraction to primary site and to all mibg avid metastatic sites at end induction beginning 3045 days after pbsc infusion isotretinoin 80 mg / m per dose orally twice a day 14 days given every 28 days for six courses starting day 60 radiation therapy post - ahsct therapy figure 1 : treatment schema pbsc = peripheral blood stem cells . 
mibg = i or imeta - iodobenzylguanidine . see online for appendix was equivalent to repeated testing of the alternative hypothesis at p = 0005 for a cumulative level of 005 . 
trial e cacy results remained masked until release by the data safety monitoring committee after all patients had completed protocol therapy . the primary endpoint was event - free survival , for which the time to event was calculated from study enrolment and randomisation until rst occurrence of relapse , progressive disease , secondary malignancy , death , or until last contact with the patient if no event occurred . 
we generated kaplan - meier survival curves.21 we report 5 - year point estimates with 95% ci.22 with the exception of the sequential monitoring , we deemed p values lower than 005 signi cant . 
one additional patient who received a transplant was retrospectively ( post - transplant ) determined by the treating institution to have had progressive disease at the end of induction ; thus table 1 presents a total of 38 patients in the purged group with end of induction progressive disease . 
the corresponding author had nal responsibility for the decision to submit for publication . results the trial ended after 495 patients had been enrolled ( patients were enrolled from march 16 , 2001 , to feb 24 , 2006 )  . 
baseline characteristics were much the same in each group and seemed similar to the cog overall high risk cohort ( table 1 ) .2 median age of the patients was 31 years ( range 02291 years )  . 
of the 486 eligible for randomisation , 137 ( 28% ) patients subsequently enrolled in the cog anbl0032 trial after transplantation , and 78 ( 16% ) were assigned to the ch14.18 antibody group ( 36 of 243 in the purged group and 42 of 243 in the non - purged group )  . we obtained pbsc from 465 ( 96% ) of 486 randomised patients : 229 in the purged group and 236 in the nonpurged group . 
reasons patients were not transplanted included progressive disease ( 28 from purged group and 25 from non - purged group ) or death during induction ( eight from purged group and seven from non - purged group ) , organ toxic e ects ( seven from purged group and ve from non - purged group ) , withdrawal from protocol ( three from purged group ) , insu cient pbsc ( ve from purged group and one from non - purged group ) , insu cient response ( two from purged group and four from non - purged group ) , and other ( ten from purged group and nine from non - purged group )  . 
29 patients randomly assigned to purged pbsc could not comply because of insu cient pbsc yield for purging ( 12 patients ) or after purging ( eight patients ) , regulatory or technical issues ( six patients ) , positive microbial culture of pbsc ( one patient ) , and parental refusal ( two patients )  . 
the fth patient , also assigned to receive nonpurged pbsc , had a negative sample from day 1 immunocytology , but the pooled pbsc collection had positive immunocytology before purging . 
we also noted no di erence in event - free survival or overall survival from the time of transplantation between the purged and non - purged groups who completed transplantation ( gure 3c , d )  . 
post - hoc analysis by treatment actually received showed no di erence in event - free survival ( p = 081 ) or overall survival ( p = 089 ) from study enrolment between groups ; similar results were noted when event - free survival ( p = 015 ) and overall survival time of transplantation ( data not shown )  . 
in the 354 patients with stage 4 disease older than 18 months , event - free survival ( p = 032 ) or overall survival ( p = 077 ) from enrolment did not di er between the purged and nonpurged groups . 
outcome was similar for individuals with protocol - de ned low compared with normal gfrs . ( p = 023 ) were measured from although potentially underpowered and done post - hoc , analyses suggested that 5 - year event - free and overall survival for the 270 patients with stage 4 disease with invaded bone marrow at diagnosis did not signi cantly di er between groups ( p = 020 for event - free survival and p = 050 for overall survival )  . 
similarly , for the 120 patients who were stage 4 with invaded bone marrow after two cycles of chemotherapy ( at the time of pbsc collection ) , there was no di erence between groups in terms of 5 - year event - free or overall survival ( p = 022 for event - free survival and p = 052 for overall survival )  . 
 the 245 patients with tlda results from day 1 of leukapheresis ( before purging ) were representative of all 486 patients in terms of clinical and prognostic characteristics ( data not shown )  . 
of these 245 patients , 122 ( 50% ) had detectable tumour mrna by the ve - gene tlda : 68 ( 53% ) of 129 patients in the purged group and 54 ( 47% ) of 116 patients in the non - purged group ( table 1 )  . 
 patients with detectable tlda had lower event - free survival ( at 5 years 29% , 95% ci 2138 ) and overall survival ( at 5 years 41% , 95% ci 3250 ) than did patients with undetectable tlda ( 5 - year event - free survival 51% , 95% ci 4260 ; p = 00003 ; and 5 - year overall survival 62% , 95% ci 5370 ; p = 00017 ; gure 4 )  . 
when we analysed the same data using only expression of th and phox2b , 62 ( 25% ) patients had detectable tlda ( 34 in the purged group and 28 in the non - purged group ) , with lower event - free survival ( at 5 years 26% , 95% ci 1637 ) and overall survival ( at 5 years 35% , 95% ci 2347 ) than those with undetectable tlda ( 5 - year event - free survival 45% , 95% ci 3852 ; p = 0005 ; and 5 - year overall survival 58% , 95% ci 5065 ; p = 001 )  . 
60 ( 33% ) of 183 pbsc with undetectable two - gene tlda ( phox2b and th ; 34 in the purged group and 26 in the non - purged group ) were detectable using ve genes . su cient numbers of cd34 cells per protocol criteria were obtained in 443 of 465 patients : 221 of 229 in the purged group and 222 of 236 in the non - purged group . 
 unknown day 1 immunocytology tlda analysis of pbsc from day 1 of leukapheresis tumour detectable tumour undetectable no tlda specimen obtained or specimen of insu cient quality overall response at the end of induction number proceeding to stem - cell transplantation 180 / 243 ( 74% ) 192 / 243 ( 79% ) number for whom any stem - cell product infused was not the product randomised 35 / 180 ( 19% ) 5 / 192 ( 3% ) number for whom back - up pbsc infusion was given 5 / 180 ( 3% ) 6 / 192 ( 3% ) number receiving post - stem - cell transplantation anti - gd2 antibody 36 / 180 ( 20% ) 42 / 192 ( 22% ) post - induction gfr 100 ml / min per 173 m ( normal gfr ) < 100 ml / min per 173 m ( low gfr ) unknown 163 / 194 ( 84% ) 156 / 201 ( 78% ) 31 / 194 ( 16% ) 45 / 201 ( 22% ) proportions have been calculated excluding patients with unknown values . 
all but two patients without day 1 immunocytological data had immunocytology testing on a separate stem - cell sample before stem cell - infusion for transplantation ; treating physicians chose to infuse non - immunocytology tested products in those two patients . 
percentages calculated on the basis of the number of patients who were harvested and who had a specimen of su cient quality ( 129 purged , 116 non - purged , 245 overall )  . 
one additional patient who received a transplant was retrospectively ( post - transplant ) determined by the treating institution to have had progressive disease at the end of induction . table 1 : patient characteristics vol 14 september 2013 1003 articles p = 077 p = 081 time from study enrolment ( months ) time from study enrolment ( months ) number at risk purged 243 non - purged 243 173 179 119 123 100 20 243 243 203 212 171 175 142 147 124 131 purged pbsc ( n = 180 ) non - purged pbsc ( n = 192 ) purged pbsc ( n = 180 ) non - purged pbsc ( n = 192 ) purged pbsc ( n = 243 ) non - purged pbsc ( n = 243 ) purged pbsc ( n = 243 ) non - purged pbsc ( n = 243 ) 40% ( 95% ci 3346 ) 36% ( 95% ci 3042 ) 49% ( 95% ci 4156 ) 42% ( 95% ci 3448 ) 51% ( 95% ci 4457 ) 50% ( 95% ci 4356 ) 55% ( 95% ci 4762 ) 54% ( 95% ci 4660 ) p = 033 number at risk time from transplantation ( months ) time from transplantation ( months ) purged 180 non - purged 192 126 133 180 192 152 165 133 143 113 125 106 p = 076 figure 3 : event - free survival and overall survival ( a ) event - free survival for intention - to - treat population from time of enrolment or randomisation . 
 ( c ) event - free survival for comparison of patients randomly assigned to purged treatment group versus patients randomly assigned to non - purged treatment group , from time of transplantation . 
 ( d ) overall survival for comparison of patients randomly assigned to purged treatment group versus patients randomly assigned to non - purged treatment group , from time of transplantation . the median number of cd34 cells per kg infused was signi cantly greater for non - purged versus purged pbsc ( 56 [ iqr 37107 ] vs 37 [ 2163 ] million ; p < 00001 )  . 
 patients receiving non - purged pbsc had shorter median time to neutrophil engraftment ( 11 [ iqr 1012 ] vs 12 [ 1013 ] days ; p = 0007 ) and platelet engraftment ( 19 [ 1436 ] vs 28 [ 1640 ] days ; p = 0006 ) than did those receiving purged pbsc , with no evidence of a di erence in infection rates . five patients ( three in the purged group , two in the non - purged group ) required additional pbsc infusions for delayed neutrophil engraftment ; all subsequently engrafted . 
six patients ( two in the purged group , four in the non - purged group ) with initial neutrophil engraftment received additional pbsc infusion because of secondary neutropenia or thrombocytopenia . at the end of induction , 242 ( 51% ) of 477 patients attained an overall complete response or very good partial response ( table 1 ) , 207 ( 53% ) of 388 had a complete response by i or i - meta - iodobenzylguanidine ( mibg ) scan and 349 ( 82% ) of 424 had no tumour detectable in bone marrow by standard morphology ( table 1 )  . 
70 ( 15% ) of 477 patients progressed during induction ( table 1 )  . for brevity , the summary of toxic e ects ( table 2 ) is limited to all protocol - required ( targeted ) toxic e ects and any non - haematological toxic e ects ( non - targeted ) 1004 vol 14 september 2013 articles 62% ( 95% ci 5370 ) 41% ( 95% ci 3250 ) undetectable tlda ( n = 123 ) detectable tlda ( n = 122 ) 51% ( 95% ci 4260 ) 29% ( 95% ci 2138 ) p = 00003 number at risk time from study enrolment ( months ) time from study enrolment ( months ) p = 00017 undetectable 123 detectable 122 123 122 110 109 figure 4 : event - free survival and overall survival by tlda test results ( a ) event - free survival . 
12 ( 7% ) patients in the purged group and 17 ( 9% ) of patients in the non - purged group had sinusoidal obstructive syndrome of grade 3 or higher . 
sinusoidal obstructive syndrome was reported as severe in 15 ( 4% ) patients ( 10 of 177 in the purged group , ve of 191 in the non - purged group ) , life - threatening in 13 ( 3% ) patients ( one of 177 in the purged group , 12 of 191 in the non - purged group ) , or fatal in one ( < 1% ) patient in the purged group . the 15 ( 3% ) deaths that occurred during induction were due to infection ( four in the purged group and one in the non - purged group ) , tumour bleeding ( three in the purged group and one in the non - purged group ) , tumour - related organ compromise ( one in the purged group and two in the non - purged group ) , multi - organ failure ( one death in non - purged group ) , unrelated event ( one death in the non - purged group ) , and central venous line placement ( one death in the purged group )  . 
 infectious deaths were from typhlitis ( one death in the non - purged group ) , or fungal ( two deaths in the purged group ) and viral ( two deaths in the purged group ) causes . 
despite not requiring morphologically tumour - negative bone marrow before pbsc collection , only 1% of pbsc samples had tumour detectable by immunocytology ; therefore , immunocytological testing of pbsc has been eliminated in cog studies . following the proportion of patients who achieved complete or very good partial induction response chemotherapy in this trial was 51% , similar to other groups24 , 25 compared with 875% as originally reported ( with small patient cohort at one institution ) .26 response and progressive disease rates were similar to the less intensive ccg 3891 induction , which had fewer induction deaths.2 this trial escalated carboplatin , etoposide , and melphalan doses from the ccg 3891 regimen and omitted total body radiation ( tbi ) , while maintaining a 5 - year event - free survival similar to that reported in the myeloablative chemotherapy plus isotretinoin group from ccg 3891.2 tbi was replaced with irradiation to the primary tumour site and post - induction mibg avid metastatic sites . 
 table 2 : summary of protocol - required targeted toxic e ects , and non - hematological toxic e ects that occurred in 5% of patients or more sinusoidal obstructive syndrome of grade 3 or higher occurring in roughly the same proportion of patients as with the ccg 3891 cem - tbi regimen , 2 where it led to death in 3% of patients . 
similar results were obtained in a pilot study of tandem high dose chemotherapy using cyclophosphamide and thiotepa followed by cem with pbsc rescue.12 immunomagnetic purging of pbsc did not improve outcome , possibly because of incomplete purging or due to residual tumour in patients . 
in preclinical modelling , immunomagnetic purging removed 34 logs of tumour cells from bone marrow when starting with 1020% tumour cells.16 all ve pbsc products with tumour detected by immunocytology from the sample of day 1 became undetectable after purging , which supports a purging e ect . 
the number of randomised patients achieving complete response were insu cient to resolve the issue of whether residual tumour in patients was a possible cause for the failure of purging to improve outcome . 
this postconsolidation therapy might have eliminated tumour cells infused in the stem - cell product , which could obscure an e ect of purging . low apheresis was planned after cycle two of induction to obtain adequate cd34 cell per kg yield and avoid stemcell exposure to topoisomerases to decrease secondary leukaemia risk.26 results from a previous study5 showed a very immunocytology - detectable tumour in pbsc even when bone marrow contained residual neuroblastoma at the time of pheresis.5 this result was con rmed in our current study , with only 12% of pbsc products having immunocytologydetectable tumour . incidence of we assessed tlda on an aliquot of pbsc from day 1 of leukapheresis to assess the prognostic signi cance of tlda before any manipulation of pbsc for all patients . 
 1006 vol 14 september 2013 articles panel : research in context systematic review we searched pubmed for all publications with the terms neuroblastoma , randomized , transplant , peripheral blood stem cells and purging . 
we identi ed one randomised trial23 of ex - vivo cd34 cell selected or unselected pbsc transplantation in patients with multiple myeloma in which response and progression - free survival did not di er between groups . interpretation in our trial , purging did not improve outcome in high - risk neuroblastoma patients receiving dose intensive induction and consolidation with autologous pbsc transplantation followed by isotretinoin with or without anti - gd2 antibody . 
it will be important to assess the prognostic signi cance of tlda analysis of pbsc products using a multivariable analysis with other prognostic factors . information our analysis showed a detectable signal by ve - gene tlda was associated with a worse outcome . 
we did an additional analysis of our tlda data using only th and phox2b expression to compare with other studies.68 our patients with a detectable signal with either th or phox2b also had signi cantly worse outcome compared with those patients with an undetectable signal . 
a higher number of patients had a detectable signal with the vegene than with the two - gene analysis , providing more sensitive or less speci c , or both , tumour mrna detection . 
 smaller series have shown con icting results regarding the prognostic value of minimum tumour detection in pbsc.68 data from other groups support the prognostic signi cance of qrtpcr detection of neuroblastoma mrna in bone marrow.28 , 29 an international task force is currently assessing qrtpcr methodologies to reach a consensus technology.30 multivariable analysis of signi cance of tlda compared with other prognostic factors is ongoing . 
further analyses that are still in progress include the detection of tumour mrna by ve - gene tlda in bone marrow and peripheral blood and multivariate analysis of tlda , mibg score , bone marrow morphology , and overall clinical response . implementing this for the study was designed to assess the e ect of purging in patients with high - risk neuroblastoma as de ned by the cog . 
although we measured this in a subset of patients , the purging methodology might have caused technical interference with interpretation of the tlda assay , which would prevent accurate quanti cation of the tumour mrna reduction after purging . 
 in conclusion , our results support the use of nonpurged pbsc products following myeloablative therapy of high - risk neuroblastoma . contributors sgk , rcs , kkm , mpl , dah - k , jrp , slc , jmm , cpr , and jgv were involved in the design and development of the study . 
all authors have seen and reviewed the nal manuscript draft . con icts of interest we declare that we have no con icts of interest . acknowledgments this work was supported by u10 - ca98543 cog group chairs grant , cog statistics and data center grants : u10 - ca98413 , u10 - ca37379 , u10ca30969 , and u10 - ca29139 ; r33 - ca152809 - 01 , alexs lemonade stand foundation . 
immunomagnetic bead purging of pbsc was done under a us food and drug administration ( fda ) investigational new device exemption ( ide ) bb - ide 2259 with periodic review done as required by law . 
we thank the childrens hospital of los angeles sta in the hematopoietic stem cell processing / purging laboratory ( carolyn billups , jin - hua min , maybelle sim , and robert torres ) , the immunocytology laboratory ( rich gallego , alfonso parra ) , and the tlda laboratory ( cathy wei yao liu and betty liu ) for their essential contributions , and peter wakamatsu for his statistical and database e orts . 
we also thank the cog sta , cra , nursing and pharmacy committee members for their contributions : dina willis ( cog statistics and data center ) , sally jones ( washington university school of medicine , mo , usa ) , casey hook ( university of minnesota medical center , fairview , mn , usa ) , and john t wiernikowski ( mcmaster university , on , canada ) for providing technical and pharmaceutical assistance . editorial for calls for reformation see jama 2013 ; 309 : 60709 for the lancet oncologys call to support comparative studies see editorial lancet oncol 2010 ; 11 : 499 for the iom report see php ? record_id = 12214 for more on pcori see quality and value in cancer care in these times of stringent nancial cuts , it is more important than ever to ensure excellent value for money in health - care delivery . 
for example , an e ective therapy with a lower adverse event rate is likely to be more economical than is a lower - cost drug that requires more supportive care . 
identifying a biological approach for a cancer treatment inevitably stimulates a race between pharmaceutical companies to bring a drug to market , often resulting in several agents that act against the same target , but with no evidence of their relative e ectiveness . 
this has brought about an increasing cynicism and scepticism towards the pharmaceutical industry , and calls for reformation to restore con dence . the development of the aromatase inhibitors for hormone - dependent breast cancer is a good example of the need for comparative research . 
although the e cacy and toxicity pro les of exemestane , letrozole , and anastrozole have been shown for each drug , only a few studies have compared pairs of these agents with each other and there are no convincing three - way comparisons . comparative e ectiveness research must be done and funded by organisations that are independent of manufacturers , and that therefore do not have a vested interest . 
further proposed funding cuts of 51% at nih in 2013 makes decisions surrounding the rational use of the decreasing budget ever more urgent . the political climate is right for this policy because optimum delivery of quality and value in health care is being widely debated . 
a report by the us institute of medicine ( iom ) in 2011 stated that , in 2009 , nearly us$25 trillion was spent on health care in the usa , but less than 01% of that sum was allocated to discovering what works best . 
comparative e ectiveness research is a central component of the us patient protection and a ordable care act and resulted in the formation of the patient - centered outcomes research institute ( pcori ) , with a remit to produce research based on both systematic reviews and clinical trials . 
however , the act also mandated that representatives from pharmaceutical companies should be represented on the board , and , because pcori is a private non - pro t corporation , there are concerns about independence and the lack of accountability . 
with hindsight , it would perhaps have been better for pcori to have been embedded within the nih to allow full partnering with research divisions such as the national cancer institute . 
in the rst cycle of award funding , pcori approved 25 grants totalling $407 million , which incredibly included only one oncology project , aimed at improving end - of - life care in a single paediatric cancer . 
 this was a missed opportunity to expand comparative e ectiveness research to improve basic cancer treatment and drive down the unsustainable rise in medical costs in the usa , and pcori should be encouraged to have bigger ambitions in its next round of grant approvals . research e ectiveness nih and iom have a role to ensure us citizens have access to the best care based on scienti c knowledge . 
although president obamas administration recognises that this approach is vital for quality and value in health care , cancer health - care professionals must be vigilant to prevent nancial policy makers cutting back on health - care resources irrespective of e ects on clinical outcomes . 
 the lancet oncology vol 14 march 2013 correction to lancet oncol 2017 ; 18 : 895903 the cancer : a shaverdian n , lisberg ae , bornazyan k , et al . 
this correction has been made in the online version as of may 25 , 2017 . toxicities published online may 25 , 2017 s1470 - 2045 ( 17 ) 30409 - 6 vol 18 july 2017 e371 corrections corrections correction to lancet oncol 2014 ; 15 : 38 , 43 , 44 correction to lancet oncol 2014 ; 15 : 11422 gatta g , botta l , rossi s , et al . 
lancet oncol 2014 ; 15 : 11422the last sentence of the findings in the summary should have read : the most common grade 3 or 4 adverse events were fatigue ( 97 [ 14% ] of 697 patients allocated zoledronic acid vs 98 [ 14% ] of 704 allocated ibandronic acid ) , increased bone pain ( 91 [ 13% ] vs 85 [ 12% ] ) , joint should receptor pain ( 41 [ 6% ] vs 38 [ 5% ] ) , infection ( 31 [ 5% ] vs 23 [ 3% ] ) , and nausea or vomiting ( 38 [ 5% ] vs 41 [ 6% ] )  . 
in the per - protocol population in table 1 , in the ibandronic acid group , the number of men should read 11 ( 2% ) , the number of patients the with unknown read status 55 ( 8% ) , the number of patients with unknown pr status should read 283 ( 43% ) , and the number of patients with unknown her2 status should read 212 ( 32% ) ; in the zoledronic acid group , the number of patients with unknown pr status should read 277 ( 41% ) and the number with unknown her2 receptor ( 32% )  . 
 status should read 217 ibandronic acid group ( n = 704 ) zoledronic acid group ( n = 697 ) grade 12 grade 3 grade 4 grade 5 total ( % ) grade 12 grade 3 grade 4 grade 5 total ( % ) any adverse event 674 ( 96% ) 667 ( 96% ) 10% frequency in either group abdominal pain altered taste anaemia anorexia breathlessness constipation diarrhoea dry mouth dyspepsia fatigue fever or in uenzalike symptoms headache hypocalcaemia hypomagnesaemia hypophosphatemia infection joint pain muscle pain oedema other pain nausea or vomiting pins and needles renal impairment increased bone pain other adverse events of interest osteonecrosis of the 199 ( 28% ) 177 ( 25% ) 221 ( 31% ) 177 ( 25% ) 246 ( 35% ) 103 ( 15% ) 121 ( 17% ) 222 ( 32% ) 266 ( 38% ) 248 ( 35% ) 544 ( 77% ) 158 ( 22% ) 80 ( 11% ) 83 ( 12% ) 80 ( 11% ) 435 ( 62% ) 125 ( 18% ) 390 ( 55% ) 301 ( 43% ) 410 ( 58% ) 170 ( 24% ) 170 ( 24% ) 215 ( 31% ) 172 ( 24% ) 5 ( < 1% ) 176 ( 25% ) 236 ( 34% ) 208 ( 30% ) 254 ( 36% ) 104 ( 15% ) 140 ( 20% ) 207 ( 30% ) 265 ( 38% ) 176 ( 25% ) 551 ( 79% ) 280 ( 40% ) 222 ( 32% ) 77 ( 11% ) 80 ( 11% ) 72 ( 10% ) 428 ( 61% ) 136 ( 20% ) 398 ( 57% ) 303 ( 43% ) 417 ( 60% ) 156 ( 22% ) 171 ( 25% ) 202 ( 29% ) 226 ( 32% ) 9 ( 1% ) data are number of patients experiencing the event ( highest grade reported )  . 
toxic e ects include serious adverse events . table 2 : toxic e ects in randomised patients vol 15 february 2014 corrections fever or inuenza - like symptoms renal impairment anaemia headache constipation altered taste fatigue infection joint pain nausea or vomitting anorexia muscle pain osteonecrosis of jaw other pain breathlessness dry mouth abdominal pain hypomagnesaemia hypocalcaemia increased bone pain hypophosphatemia pins and needles oedema diarrhoea dyspepsia risk dierence ( dierence in proportion ) events in ibandronic acid group events in zoledronic group 158 / 704 172 / 704 177 / 704 199 / 704 121 / 704 221 / 704 544 / 704 125 / 704 390 / 704 410 / 704 246 / 704 301 / 704 5 / 704 170 / 704 103 / 704 266 / 704 177 / 704 83 / 704 80 / 704 435 / 704 80 / 704 215 / 704 170 / 704 222 / 704 248 / 704 280 / 697 226 / 697 208 / 697 222 / 697 140 / 697 236 / 697 551 / 697 136 / 697 398 / 697 417 / 697 254 / 697 303 / 697 9 / 697 171 / 697 104 / 697 265 / 697 176 / 697 80 / 697 77 / 697 428 / 697 72 / 697 202 / 697 156 / 697 207 / 697 176 / 697 reporting ( 5% ) patients with 38 pain , 34 ( 4% ) reporting infection , and 20 ( 3% ) reporting vomiting or nausea of the 697 patients in the zoledronic acid group . 
in paragraph six of the results section , the rst sentence should read the primary per - protocol analysis , including any skeletal - related event 21 days apart , included 390 events in 257 ( 38% ) of 672 patients in the zoledronic acid group and 419 events in 253 ( 39% ) of 654 patients in the ibandronic acid ( gure 4a ) , corresponding group to 0435 ( 95% ci 0393 to 0480 ) skeletal - related events per personyear in the zoledronic acid group and 0499 ( 0454 to 0549 ) skeletalrelated events per person - year in the ibandronic acid group . 
and the fourth sentence should read the sensitivity analysis excluding hyper calcaemia skeletal - related events was consistent with the above results , with 312 events in the zoledronic acid group and 330 events in ibandronic acid group ; the log relative risk for ibandronic acid versus zoledronic acid was 0122 ( 95% ci 0069 to 0313 ) , which corresponds to a rate ratio of 1130 ( 0933 to 1367 )  . 
these corrections have been made to the online version as of jan 27 , 2014 . 03 02 01 favours ibandronic acid favours zoledronic acid figure 2 : risk di erence of patients experiencing toxic e ects ( ibandronic acidzoledronic acid ) the results table 2 and gure 2 were incorrect ; corrected versions are shown here . 
this study aimed to provide internationally comparable local data on the incidence of childhood cancer to promote research of causes and implementation of childhood cancer control . methods this population - based registry study , devised by the international agency for research on cancer in collaboration with the international association of cancer registries , collected data on all malignancies and nonmalignant neoplasms of the cns diagnosed before age 20 years in populations covered by high - quality cancer registries with complete data for 200110 . 
incidence rates per million person - years for the 014 years and 019 years age groups were age - adjusted using the world standard population to provide age - standardised incidence rates ( wsrs ) , using the age - specific incidence rates ( asr ) for individual age groups ( 04 years , 59 years , 1014 years , and 1519 years )  . 
the regional wsrs for children aged 014 years were compared with comparable data obtained in the 1980s . findings of 532 invited cancer registries , 153 registries from 62 countries , departments , and territories met quality standards , and contributed data for the entire decade of 200110 . 
the overall wsr was 1406 per million person - years in children aged 014 years ( based on 284 649 cases ) , and the most common cancers were leukaemia ( wsr 464 ) , followed by cns tumours ( wsr 282 ) , and lymphomas ( wsr 152 )  . 
in children aged 1519 years ( based on 100 860 cases ) , the asr was 1853 per million person - years , the most common being lymphomas ( asr 418 ) and the group of epithelial tumours and melanoma ( asr 395 )  . 
since the 1980s , the global wsr of registered cancers in children aged 014 years has increased from 1240 ( 95% ci 12331247 ) to 1406 ( 14011411 ) per million person - years . interpretation this unique global source of childhood cancer incidence will be used for aetiological research and to inform public health policy , potentially contributing towards attaining several targets of the sustainable development goals . 
the observed geographical , racial and ethnic , age , sex , and temporal variations require constant monitoring and research . funding international agency for research on cancer and the union for international cancer control . copyright 2017 world health organization ; licensee elsevier . 
this notice should be preserved along with the articles original url . introduction cancers rarely occur before age 20 years , and when they do , they raise a range of medical , psychological , ethical , and societal concerns . 
furthermore , the extent of the cancer burden in this young population is unknown in many low - income and middle - income countries ( lmics ) , where data on cancer incidence are not collected . 
even in the presence of population - based information about cancer registries , collection of childhood cancers is often neglected because they represent a small proportion of all cancers , additional data sources might be required , and the resulting statistics must be subjected to meticulous quality control because they are more sensitive to imprecision or missing information . since the publication of the international incidence of childhood cancer , volume 1 ( iicc - 1 ) in 19881 and iicc - 2 in 1998 , 2 no internationally comparable data on incidence patterns of childhood cancer have been published . 
 to address this problem , the international agency for research on cancer ( iarc ) , in collaboration with the vol 18 june 2017 lancet oncol 2017 ; 18 : 71931 published online april 11 , 2017 s1470 - 2045 ( 17 ) 30186 - 9 this online publication has been corrected . 
we searched medline and participating registries for studies on the incidence of childhood cancer worldwide , with the search terms childhood cancer , registry , incidence , and population , in february , 2016 , without language or publication date restrictions . 
 we found that no globally comparable data on cancer types affecting children have been published since iicc - 2 , and no comparison of incidence patterns in children aged 1519 years has been attempted on a global scale . 
 added value of this study this study provides an overview of the incidence of cancer in 200110 for children aged 019 years , based on data collected in 153 population - based cancer registries in 62 countries , departments , and territories on five continents . 
in addition to the sex , age , and tumour - specific incidence rates for 19 world regions or populations for 200110 , we report an increase in the incidence of neoplasms since the 1980s in children aged 014 years . 
it comprehensively summarises the most recent and globally comparable data and presents information per sex , age group , geographical region , and tumour type . implications of all the available evidence the wealth of information provided by this study constitutes a solid baseline to assess needs and define priorities in the area of paediatric oncology , supporting sustainable development goal 3 to ensure healthy lives and promote wellbeing for all at all ages . 
the shortage of high - quality local information should stimulate formation of new and more accurate data sources . international association of cancer registries ( iacr ) , has coordinated a study to assess the incidence of childhood cancer worldwide , the complete results of which will be published in iicc - 3 . 
an age range of 019 years was also chosen in previous us and european studies of childhood cancer incidence and survival.3 , 4 from around here we provide an overview of the findings of the iicc - 3 study , based on a selection of quality - assured the world encompassing datasets information for the complete decade of 200110 . 
the objective of this study was to counteract the difficulties in collecting childhood cancer data from relevant data sources and provide globally comparable estimates of cancer occurrence in children to aid further research and adapt policy measures . methods study design and data sources in this epidemiological , population - based registry study , we invited all population - based cancer registries that we identified among the membership of the iacr and from published literature in medline or other published sources , such as annual reports , in any language . 
analyses for the 014 years age group were based on a larger database ( the paediatric dataset ) than those for the 019 years age group ( general dataset ) , because the paediatric dataset included data from the paediatric cancer registries not collecting data in children older than 15 years and these registries tended to have a wider coverage than the cancer registries used in the general dataset ( appendix pp 24 )  . all malignancies and non - malignant tumours of the cns diagnosed before age 20 years ( before age 15 years in most of the paediatric cancer registries ) in the covered populations in 200110 were eligible for inclusion . 
cancer data included individual records of cases with codes for the following : sex ; age ; date of birth ; date of incidence ; and tumour sequence ( ie , the numerical order of occurrence of the neoplasm ) , site , morphology , behaviour , laterality , and most valid basis of diagnosis . 
the 3rd edition of the international classification of diseases for oncology5 was required for coding of the tumour site , morphology , behaviour , multiple primary tumours , and basis of diagnosis . 
non - conforming systems were converted and tumours were classified centrally according to the 3rd edition of the international classification of ( iccc - 3 ) .6 we childhood cancer requested each contributing cancer registry to provide total population coding 720 vol 18 june 2017 articles counts for each ethnic or racial group , calendar year , sex , and year of age in the registration area of their registry . procedures all submitted datasets were processed and assessed individually in a rigorous peer - review process . 
the assessment criteria included a range of indicators , including the following : minimum number of cases ; proportion of cases confirmed from cancer tissue examination ( microscopic verification ) ; proportion of cases registered from death certificate only ; proportion of cases with morphology not otherwise specified ( ie , cases in the unspecified subgroups of iccc - 3 or those coded by unspecified morphology codes such as 8000 , 8800 , 9800 ) ; proportion of cases with an unlikely combination of site and morphology , or an unlikely age and tumour type ; proportion of rare entities ( ie , neoplasms that occurred with a frequency of < 005% in large datasets ) ; proportion of dates of birth and incidence that were incomplete ; proportion of ages that were imprecise ; overall incidence rates ; proportion of cases and incidence by sex , age group , and tumour type ; the stability of rates over time ; proportion of multiple primary diagnoses ; and consistency of population data . 
the improvements included completion of missing information , additional years of data , inclusion of information from missed data sources , correction of coding errors , improvements in calculation of age , inclusion of non - malignant cns tumours , replacement of population data , and explanation of the questioned patterns . statistical analysis we calculated age - specific incidence rates ( asr ) for four 5 - year age groups ( 04 years , 59 years , 1014 years , and 1519 years ) as the quotient of the number of cases and the number of person - years in the respective categories of sex , geographical area , and racial or ethnic group for the applicable time period , expressed per million person - years . 
we defined person - years as the sum of the population counts in a specific geographical area surveyed by a registry in each year from 2001 to 2010 , categorised by sex and age and , if relevant , race or ethnicity . 
in the absence of all required details , we estimated the covered population counts by linear interpolation ( six registries ) or extrapolation ( three registries ) from the data provided by the registries , based on an assumption of regular population growth , before calculating rates . 
the purpose of this study was to make comparisons among regions and time periods , so all reported incidence rates for the 014 years and 019 years age groups were adjusted via direct standardisation . 
we calculated age - standardised rates ( wsrs ) as the weighted average of the three age - specific rates ( to calculate rates for 014 years ) or four age - specific rates ( for 019 years ) , using the weights of the world standard population7 ( appendix p 5 )  . 
 we calculated incidence sex ratios by dividing the incidence in male individuals with that in female individuals . the results are presented for 19 geographical regions or populations and a combined total ; all the defined regions are either un - defined regions8 or an aggregate of un - defined regions , with the exception of north america , for which we present data separately for canada and the usa , and have split data for the usa into five racial or ethnic groups . 
we calculated the proportion of the covered population of the world and each region by dividing the included person - years by the total personyears in 200110 by age group , as estimated by the un in 2015.9 to compare the incidence rates derived from the paediatric dataset for 200110 with those published in iicc - 2 , 2 we assigned iicc - 2 registry data to the same geographical regions as used in this iicc - 3 study . 
although the target period of iicc - 2 was the 1980s , the time periods of the contributing registries differed both in length and starting years , because they either followed on from the iicc - 1 period or they could not provide other years of data . 
the corresponding author had final responsibility for the decision to submit for publication . results of the 532 invited cancer registries , 420 submitted their data and 309 met standard data quality criteria . 
 approximately 114% of the world population aged 014 years ( contributing 18 376 710 144 person - years ) was covered by the registries included in our study , ranging from 17% in south asia ( india ) to 994% in north america ( table 1 )  . 
coverage of the world population within the indicated age group . table 1 : coverage of the world population aged 019 years , person - years , numbers of cancer cases , and quality indicators of data included in the analyses , overall and by region , 200110 paediatric dataset ( age 014 years ) general dataset ( age 019 years ) cases person - years ( millions ) incidence per million cases person - years ( millions ) incidence per million age group , all cases ( asr ) sex ( wsr ) boys girls 04 years 59 years 1014 years 1519 years 019 years 014 years 019 years 156 721 127 917 1072 1023 127 096 74 175 83 378 age group , all cases ( wsr ) 014 years * 284 649 2095 1406 age group , malignant cases only ( wsr ) 274 096 2095 1356 1514 1294 1879 1076 1144 169 531 141 695 1039 93 559 54 370 62 438 100 860 210 367 311 227 206 027 305 233 1481 2025 1481 2025 1632 1436 1971 1116 1203 1853 1472 1558 1443 1528 asr = age - specific rate . 
registration of non - malignant cns tumours differed by registry , and was higher in the paediatric dataset than in the general dataset ( table 1 , 2 )  . 
 the overall wsrs were 1406 per million person - years in children aged 014 years and 1558 per million person - years in those aged 019 years ( table 2 )  . 
the asr in young people aged 1519 years was 1853 per million person - years . incidence rates were slightly higher in boys than in girls ( incidence sex ratio was 117 in the 014 years age group and 114 in the 019 years age - group ) and varied with age , region , and diagnostic group ( table 2 ; appendix p 8 )  . 
across all regions , incidence was higher in boys than in girls ( incidence sex ratio ranged from 11 to 14 in the 019 years age group ; appendix p 8 ) , except for the 1519 years age group of native americans in the usa ( incidence sex ratio of 09 ) and in east asia ( 10 ) , where girls had a higher incidence ( ratios rounded to one decimal place ; appendix p 8 )  . 
sex - specific incidence varied by diagnostic group , with renal tumours and epithelial tumours more common in girls , with variations by age group ( appendix p 8 )  . 
germ cell and gonadal tumours were also more common in girls than in boys in the 014 years age group ( appendix p 8 )  . asrs were higher in children aged 04 years and 1519 years than in those aged 59 years and 1014 years ( table 2 )  . 
 in the 014 years group , overall wsrs varied from less than 100 per million person - years in sub - saharan africa , for native american children in the usa , and in south asia ( india ) , to more than 150 per million person - years in some subpopulations of north america and europe , and in oceania ( figure 1a ; appendix p 6 )  . 
in young people aged 1519 years , the lowest asr was observed in 722 vol 18 june 2017 articles a age 014 years b age 1519 years north africa sub - saharan africa central america and caribbean south america north america east asia south asia * southeast asia west asia eastern europe northern europe southern europe western europe oceania wsr per million person - years highest rate lowest rate overall rate asr per million person - years figure 1 : variation in the overall incidence of childhood cancer by geographical region , 200110 data are for children aged 014 years , from the paediatric dataset ( a ) , and 1519 years , from the general dataset ( b )  . 
 * comprising data from india only . leukaemia lymphoma cns tumours sympathetic nervous system tumours retinoblastoma renal tumours hepatic tumours bone tumours soft tissue sarcomas germ cell and gonadal tumours epithelial tumours and melanoma other and unspecied 04 59 1014 1519 south asia ( india ) , whereas the highest asrs were seen in some predominantly white populations of north america , europe , and oceania ( figure 1b ; appendix p 6 )  . the range of tumour types varied markedly with age group ( figure 2 )  . 
in children aged 04 years , leukaemia represented 361% ( 45 849 of 127 096 ) of all cases ; however , the proportion of leukaemia cases was 154% ( 15 520 of 100 860 ) in young people aged 1519 years . 
conversely , lymphomas represented 53% ( 6766 of 127 096 ) of cases in children aged 04 years , and 225% ( 22 740 of 100 860 ) of cases in those aged 1519 years . 
epithelial tumours and melanoma represented 09% of all cases in children aged 04 years ( 1197 of 127 096 ) , but were the second most common tumour group in young people aged 1519 years ( 21 480 [ 213% ] of 100 860 )  . 
of note is the relatively high sympathetic nervous system tumour wsr of 102 per million person - years in black children in the usa , which contrasts with the wsr of 27 per million person - years in the mostly black population of subsaharan africa ( table 3 )  . 
renal tumours were common in 100% proportion of all cancers figure 2 : proportional distribution of cancer type by age group , 200110 , all regions combined tumours classified by international classification of childhood cancer , volume 3.6 statistics for children younger than 15 years are based on the paediatric dataset and the statistics for those aged 1519 years are based on the general dataset . children aged 04 years ( 11 297 [ 89% ] of 127 096 ) , and their relative frequency decreased in older age groups , to 07% ( 756 of 100 860 ) in young people aged 1519 years ( figure 2 )  . 
soft tissue sarcomas were present in a similar proportion of cases in children aged 014 years and those aged 1519 years in most regions ( table 3 , 4 ; figure 2 ; appendix p 10 )  . 
in sub - saharan africa , 46% ( 579 of 1262 ) of all soft tissue sarcomas in children aged 014 years were kaposis sarcoma compared with 57% ( 119 of 208 ) in those aged 019 years , whereas in all the other regions kaposis sarcoma represented less than 1% of all soft tissue sarcomas in children younger than 15 years and a maximum of 2% ( 14 of 592 ) in black children in the usa ( data for all regions not shown )  . 
germ cell and gonadal tumours were rare in children younger than 15 years ( 10 200 [ 36% ] of 284 649 ; table 3 ) , and more common in those aged 1519 years ( 12 105 [ 120% ] of 100 860 ; table 4 )  . 
the group of epithelial neoplasms and melanoma comprises several specific types of carcinomas ( adrenocortical , thyroid , nasopharyngeal , skin ) , all other types of carcinoma ( except those occurring in kidney , liver , and gonads ) , and melanoma . 
this group constituted 38% ( 10 679 of 284 649 ) of all tumours in children aged 014 years and 213% ( 21 480 of 100 860 ) in those aged 1519 years ( appendix p 10 )  . 
the group of other and unspecified tumours comprised 09% ( 2469 of 284 649 ) of all cases in children aged 014 years and 15% ( 1500 of 100 860 ) of all cases in those aged 1519 years . 
 in 22 registries no tumours were classified in this category ; other and unspecified tumours comprised 5% or more of all tumours in ten registries , including one registry for which 12% ( 68 of 561 ) of all tumours were classified as other and unspecified . in children aged 014 years , the leading cancers in all regions combined were leukaemia , followed by cns tumours , and then lymphomas , and this ranking was 726 vol 18 june 2017 articles all cancers in age 1519 years north africa sub - saharan africa central america and caribbean south america canada usa , native american usa , asian and pacic islander usa , black usa , hispanic white usa , non - hispanic white east asia south asia * southeast asia west asia eastern europe northern europe southern europe western europe oceania observed in most world regions ( table 3 )  . 
the ratios of highest to lowest regional wsr were higher than 50 for cns tumours ( 62 ) , germ cell and gonadal tumours ( 59 ) , neuroblastoma ( 56 ) , epithelial tumours and melanoma ( 55 ) , and leukaemia ( 52 )  . in young people aged 1519 years , lymphomas were the most common cancers in all regions combined , followed by epithelial tumours and melanoma ( table 4 ; figure 4 )  . 
 however , leukaemia was the most common neoplasm in this age group in south america , native american and white hispanic children in the usa , south asia ( india ) , and southeast asia ( table 4 ; figure 4 )  . 
in oceania , white non - hispanic children in the usa , in east asia , and in central america and the caribbean the most common cancer type was the group of epithelial cancers and melanoma ( table 4 ; figure 4 )  . 
geographical variations in incidence , expressed as the ratio of the highest to the lowest asr across regions , were 50 or higher for hepatic tumours ( 78 ) , germ cell tumours ( 64 ) , cns tumours ( 60 ) , lymphomas ( 54 ) , epithelial tumours and melanoma ( 52 ) , and soft tissue sarcomas ( 50 )  . from the 1980s to 200110 , the overall wsr for all tumours in children aged 014 years increased from 1240 per million person - years ( 95% ci 12331247 ) in the 1980s to 1406 per million person - years ( 14011411 ) in 200110 . 
the increase was seen in all regions except sub - saharan africa , and was smallest in central america and the caribbean ( wsr 1253 [ 95% ci 12121294 ] in 198089 ; 1292 [ 95% ci 12591325 ] in 200110 ) and highest in southeast asia ( 920 [ 95% ci 892948 ] ; 1198 [ 95% ci 11731223 ] )  . 
in sub - saharan africa , a decrease was noted between the 1980s ( 810 [ 95% ci 768852 ] ) and 200110 ( 563 [ 95% ci 551575 ] ; figure 5 ; appendix p 7 )  . asr per million person - years leukaemia lymphoma cns tumours sympathetic nervous system tumours retinoblastoma renal tumours hepatic tumours bone tumours soft tissue sarcomas germ cell and gonadal tumours epithelial tumours and melanoma other and unspecied figure 4 : incidence of cancer in young people aged 1519 years , 200110 , by region tumours classified by international classification of childhood cancer , volume 3.6 data are based on the general dataset . 
 * comprising data from india only . discussion using data provided by 153 high - quality cancer registries , we report internationally comparable incidence rates of cancer in children aged 019 years during 200110 . 
the incidence of cancer in children aged 014 years was 1406 per million person - years , and in those aged 019 years was 1558 per million person - years . 
to our knowledge , this report presents the best available information on cancer incidence for the given period and age group . we chose wsr as a relative estimate of cancer burden , but it should not be used for estimating numbers of cases in a population , because the value of wsr depends on the choice of the standard population . 
 although 20% of the cancers occurring in young people aged 1519 years were epithelial tumours ( the most prevalent histology types in adults ) or melanoma , this age group also had high proportions of lymphomas , leukaemias , germ cell tumours , and sarcomas . 
therefore , iccc - 36 seems to be well adapted to reporting incidence in this age group , because the named tumour groups represent the main diagnostic categories in iccc - 3 . 
we found that the incidence of cancer in young people aged 1519 years was 1853 per million person - years , based on 100 860 cases . because not all the contributing paediatric cancer registries could provide data for young people aged 1519 years , the analyses for children aged 014 years were based on a different dataset ( paediatric dataset ) than were the analyses for children aged 019 years or those aged 1519 years ( general dataset )  . 
the two resulting datasets vol 18 june 2017 articles north africa sub - saharan africa central america and caribbean south america north america east asia south asia * southeastern asia west asia eastern europe northern europe southern europe western europe oceania we selected the contributing registries because they provided quality - assured data for the entire decade of 200110 . 
inevitably , the reported rates were influenced by this selection ; however , they provide the best and unique comparable global incidence estimates for the given period because they are not affected by intermittent contributions for parts of the target period . a particular strength of our study comes from separate presentation of the incidence patterns for the five racial and ethnic groups distinguished in the us data , despite the difficulties in classifying the us population into racial and ethnic groups due to population mixing , migration , and self - declaration of ethnicity.11 unfortunately , the ethnic differences within multi - ethnic populations of europe , canada , and some other regions could not be readily studied . 
for the purpose of simplicity these data were not included in this paper ; however , they are available online on the iicc - 3 website . our study improved the overall data quality in all participating cancer registries , particularly in 72 of 153 whose datasets were not acceptable at the beginning of the study . 
the study raised the registries awareness of additional data sources ( haematology , opthalmology , orthopaedics , dermatologicaly , neurology , endocrinology , and paediatric clinics ) and of specific quality control . 
we required a high level of quality and completeness for our study , because small errors or omissions would have had a large impact on the resulting incidence rates . approximately 30 cancer registries dropped out of the study , irrespective of the quality of their data . 
data collected on more than 40 million person - years in 12 cancer registries ( canada [ new brunswick , prince edward island ] , denmark , finland , germany [ berlin , brandenburg , bremen , mecklenburgvorpommern , sachsen - anhalt , and the free states saxony and thuringia ] , and singapore ) could not be used because these registries were bound by requirements of a specific administrative procedure to approve provision of their data . although the cancer registries follow international guidelines , we observed wide variation in registration techniques , access to data sources , case eligibility criteria , application and interpretation of registration standards , and coding systems . 
other practices reduced data quality ( eg , restricted or no access to pathology reports ) , completeness ( eg , restricted or no access to identifiable death certificates ) , or timeliness ( eg , third - party data encryption )  . 
in some registries cases were coded as wsr per million person - years iicc - 2 , published data ( 1980s ) iicc - 3 , selection ( 200110 ) figure 5 : comparison of incidence of neoplasms in children aged 014 years in 198089 and 200110 , by region data from the two time periods were standardised and peer reviewed using similar methods . 
 * comprising data from india only . gave different estimates of incidence for the ( common ) age group of 014 years , and this incidence was 5% lower in the paediatric than in the general dataset . 
this difference can be explained by variations in population coverage between the registries , and possibly distinctive data sources used by the two types of registries ( ie , those that included data for young people aged 1519 years and those that did not ) , as was shown previously in an analysis of data on childhood cancer in europe.4 although the results presented from both datasets are based on the best data available for each age group , they also emphasise the importance of quality assurance , particularly when dealing with a rare disease such as childhood cancer . 728 vol 18 june 2017 articles microscopically verified only if the pathology report could be reviewed by registry staff . 
registries are often under - resourced , and large investments for a small proportion of cases in general cancer registries might not be seen as a priority ; however , these variations highlight the need for support to enable production of high - quality and comparable data . a high proportion of specified diagnoses cannot be ensured without available specialised diagnostic facilities . 
 the category of unspecified morphology might have included misclassified specific cancers , but in the absence of precise documentation it might have also included cases that were not malignant or cancers that did not occur in children . although the differences in sex ratios by diagnostic group and age might have to a large extent reflected true differences in disease occurrence , 12 the differences by geographical region could have more readily reflected sociocultural customs whereby boys are favoured over girls to seek medical attention when sick . 
the potential for such selective treatment in india and in some african populations was supported by our registry contacts in those regions when we inquired about a possibility of inequality in seeking health care . the registries with no access to a national database of all causes of death might not have registered the cancers that were only discovered at the time of death , even though the proportion of missed cases might be low in childhood populations . 
the registries operating in some lmics were particularly affected by missing or infrequent official population estimates , and these data needed to be estimated by interpolation or extrapolation , influencing the reported rates . 
treatment abandonment , common in lmics , 14 might also have led to underregistration if identified patients who refused treatment were not sufficiently well described ( eg , missing dates or place of residence )  . 
under - ascertainment of diagnosed cases might have from administrative resulted restrictions of access to medical files , political or social instability , competing needs , and inadequate political will , causing a dearth of resources , shortage or volatility of registry personnel , loss of perennial expertise , and missing or broken links with relevant data sources . 
 overestimates of incidence might have occurred in areas with superior treatment facilities if the place of permanent residence could not be correctly determined for registered patients , and national coverage would neutralise such artefactual regional differences within a country.15 accurate incidence rates are also difficult to obtain in ethnic minorities , such as the native american population in the usa , possibly because of imprecise classification of the at - risk population , as well as patients with cancer.16 cancer statistics in high - income countries might be influenced by overdiagnosis of some cancers detected by non - invasive imaging and screening tests , including neuroblastoma , thyroid cancer , melanoma , and kidney cancer.17 is certainly influenced by although a complete assessment of time trends in incidence falls outside the scope of this report , our data showed that the overall incidence of registered neoplasms in childhood increased between the 1980s and the 2000s . 
 our comparison the composition of the two data pools ( different registries have contributed to the two compared periods ) ; however , the increase in the overall rates is clear . 
future detailed analyses of time trends by tumour group and subpopulations will bring more clarity to the interpretation of these secular changes . the reduction of cancer incidence in sub - saharan africa probably had two main causes . 
first , this iicc - 3 study included data from the national childhood cancer registry of south africa , which contributed 70% of all cases for this region and reported very low incidence rates . 
of the five datasets classified as sub - saharan african in iicc - 2 , only one ( from namibia ) reported a lower overall incidence rate than the south african registry in iicc - 3 . 
the possible reasons for the low rates in south africa are discussed elsewhere.18 second , the implementation of antiretroviral therapy in some areas affected by hiv19 has contributed to a decrease in incidence of kaposis sarcoma . 
this cancer type represented more than a third of the total cancer incidence in kampala , uganda , in the iicc - 2 ( wsr 1827 per million person - years )  . 
the incidence of kaposis sarcoma in kampala halved between the iicc - 2 and this iicc - 3 study , and a decreasing trend between the 1990s and the 2000s was also noted in a kampala registry study.20 leukaemia , the most common cancer in children worldwide , had the largest impact on total cancer incidence . 
even though strong underdiagnosis of leukaemia is suspected in sub - saharan africa , 21 less commonly diagnosed in black children in the usa than in the other us ethnic groups ; however , whether leukaemia was also vol 18 june 2017 articles leukaemia might be underdiagnosed as a result of reduced access to health care associated with lower economic status in this group is unclear.22 in children aged 014 years , the highest leukaemia rates were in hispanic white children in the usa ( 40% of total incidence )  . 
the native american component of hispanic ancestry was a presumed risk factor , based on the observations that known risk alleles at loci identified in genome - wide association studies of european - ancestry populations in cdkn2a , pip4k2a , cebpe , and arid5b were all significantly associated with native american ancestry.23 comparatively high incidence rates and the largest proportion of leukaemia among all cancers were reported in southeast asia . 
a link to the massive use of pesticides in this world region24 to protect crops and increase yields should be examined in specific studies , since exposure to pesticides has been associated with leukaemia risk.25 , 26 the male predominance among patients with lymphoma is probably a result of innate sex differences in susceptibility , but with increasing age other factors might play a role , such as the increased risk of hiv infection in boys compared with girls.27 the highest incidence of lymphomas worldwide has been reported in the mediterranean region ( as shown in our study and others28 ) , and in hiv - infected populations , 29 with b - cell non - hodgkin lymphoma an aids - defining malignancy . burkitts lymphoma is endemic and common in some sub - saharan african childhood populations , 30 in which hiv infection can further accentuate its incidence.2 , 31 hodgkins lymphoma is rarer in populations of south and east asia than in other parts of the world ; the undergoing socioeconomic changes might gradually result in a similarly high incidence to that observed in western populations.32 , 33 rates in lmics most probably the highest incidence of all cns tumours was noted in high - income countries , which is clearly related to the wide availability of diagnostic facilities . 
the lower incidence ( and proportionately ) reflect poor access to neuroimaging facilities ( eg , low number of ct or mri scans , long waiting lists , and prohibitive costs of diagnostics tests ) .34 , 35 this poor access causes delay in diagnosis and possibly underdiagnosis of brain tumours.36 comparability of incidence of cns tumours across the continents would be greatly improved if all registries attempted to collect information on non - malignant cns tumours , at least in children . this study describes the global cancer incidence patterns in children younger than 20 years for 200110 , providing an update to comparable information that is now almost 20 years old.2 despite possible artefacts influencing data availability , quality , and comparability , the size of the studied populations and the observed differences in our study suggest that our data are sufficiently robust for international comparisons of childhood cancer occurrence , and provide useful pointers for further studies . 
the collected data can be used for further research , including continued development of childhood - specific registration standards and guidelines , detailed studies in subpopulations and by tumour subtype , and global estimates of cancer indicators . 
to secure data availability and quality , constant support of cancer registration is required at local , national , and international levels . contributors es - f , lagr , fm , ph , hys , and cas designed the study . 
es - f drafted the manuscript , which was reviewed , modified , and approved by es - f , lagr , fm , ad , fb , ph , hys , and cas . declaration of interests we declare no competing interests . acknowledgments international incidence of childhood cancer , volume 3 is supported by the international agency for research on cancer and the union for international cancer control . 
the cooperation of all cancer registries and members of the international association of cancer registries is gratefully acknowledged . editorial see comment page 578 for the letter from the royal colleges see rcplondon.ac.uk / press - releases / royal - colleges - join - forcesaustralian - counterparts - callstandard - packs for the lancets series on tobacco control see thelancet.com / themed / tobaccocontrol uk government panders to tobacco industry and lacks social conscience one of the most important roles of any government is to protect its citizens . 
however , on may 8 , 2013 , the uk government condemned 150 000 children per year to a lifetime of addiction , poor health , and for many , premature death . 
in the days running up to the annual state opening of parliament , speculation had been made about the contents of the queens speech , in which the government detailed legislative measures it wishes to pass through parliament over the next 12 months . 
 last year , the former uk health secretary andrew lansley declared smoking should no longer be an acceptable part of normal life , smoking was the largest avoidable cause of early mortality , and government was committed to act against the habit . 
 indeed , anne milton , a former uk health minister , is also on record as saying just last year that , we cannot ignore the fact that young people are recruited into smoking by colourful , eye - catching , cigarette displays . 
the roy castle lung cancer foundation remarked on may 8 , 2013 , that , packaging of tobacco products remains the last form of tobacco promotion legislated in the uk and is produced to attract [ consumers with ] colourful and targeted eyecatching designs . 
it is also absurd that the governments own systematic review backing the introduction of standardised packaging , public health minister anna soubrys public support for plain packaging , and opinion polls showing 62% of adults in england favour the use of standardised packaging , have all been conveniently forgotten . it is also curious that senior department of health o cials are reported to have held meetings earlier this year with imperial tobacco , british american tobacco , philip morris international , and japan tobacco international . 
why the uk government felt the need to entertain representatives from these companies is hard to comprehend given none would likely say anything that wasnt biased and self - serving . 
equally , recent election successes by the right - winged uk independence party , which aligns itself with smokers , leads to suspicions that the conservative partythe dominant force in the current coalition governmentdoes not want to be seen as overtly anti - smoking in the run - up to the 2015 general election because of the possible loss of potential votes . 
 australia , by contrast , have stayed resolute on the issue and have seen o the cynical arguments put forward by the tobacco industry , and those of the pro - tobacco lobbying of lynton crosbys company , crosby textor , to become the rst country to implement legislation restricting tobacco products to plain packagingan initiative quite - rightly referred to as brave and groundbreaking in a letter published on may 3 , 2013 , in the uk newspaper , the independent , and written by the presidents of uk royal college of physicians , the uk royal college of paediatrics and child health , and the royal australasian college of physicians . 
these three colleges all make a strong plea in their letter for jeremy hunt to pursue similar legislation as soon as possible and condemn the uk government for delaying its plans in this regard . 
interestingly , in the rst 6 months of packaging legislation in australia , none of the calamitous predictions made by the tobacco industry about the negative e ects on the economy , loss of jobs , and increased illicit trade , have come to pass . the uk has a strong record on implementation of tobacco - control policies , and is ranked as one of the leaders among european countries ; however , conservative party interests within the current government undermine progress by pandering to the tobacco lobby and by letting self - interests weaken health policy . 
ironic , too , that a government so obsessed with austerity does not see the cost bene t to the national health service of eliminating the scourge of tobacco usage from the health of a nation . 
we randomly assigned patients ( by minimisation ) to receive either intravenous mitomycin ( one dose of 12 mg / m on day 1 ) or intravenous cisplatin ( one dose of 60 mg / m on days 1 and 29 ) , with intravenous fluorouracil ( one dose of 1000 mg / m per day on days 14 and 2932 ) and radiotherapy ( 504 gy in 28 daily fractions ) ; and also did a second randomisation after initial therapy to maintenance chemotherapy ( fluorouracil and cisplatin ) or no maintenance chemotherapy . 
the primary outcome was complete clinical response ( the absence of primary and nodal tumour by clinical examination ) , in addition to overall survival and progression - free survival from time of randomisation . 
in this post - hoc analysis , we analysed complete clinical response at three timepoints : 11 weeks from the start of chemoradiotherapy ( assessment 1 ) , 18 weeks from the start of chemoradiotherapy ( assessment 2 ) , and 26 weeks from the start of chemoradiotherapy ( assessment 3 ) as well as the overall and progression - free survival estimates of patients with complete clinical response or without complete clinical response at each assessment . 
complete clinical response was achieved in 492 ( 52% ) of 940 patients at assessment 1 ( 11 weeks ) , 665 ( 71% ) of patients at assessment 2 ( 18 weeks ) , and 730 ( 78% ) of patients at assessment 3 ( 26 weeks )  . 
691 patients attended all three assessments and in this subgroup , complete clinical response was reported in 441 ( 64% ) patients at assessment 1 , 556 ( 80% ) at assessment 2 , and 590 ( 85% ) at assessments 3 . 
in the overall trial population of 940 patients , 5 year overall survival in patients who had a clinical response at assessments 1 , 2 , 3 was 83% ( 95% ci 7986 ) , 84% ( 8187 ) , and 87% ( 8489 ) , respectively and was 72% ( 6678 ) , 59% ( 4967 ) , and 46% ( 3755 ) for patients who did not have a complete clinical response at assessments 1 , 2 , 3 , respectively . 
in the subgroup of 691 patients , 5 year overall survival in patients who had a clinical response at assessment 1 , 2 , 3 was 85% ( 8188 ) , 86% ( 8288 ) , and 87% ( 8490 ) , respectively , and was 75% ( 6880 ) , 61% ( 5070 ) , and 48% ( 3658 ) for patients who did not have a complete clinical response at assessment 1 , 2 , 3 , respectively . 
similarly , progression - free survival in both the overall trial population and the subgroup was longer in patients who had a complete clinical response , compared with patients who did not have a complete clinical response , at all three assessments . interpretation many patients who do not have a complete clinical response when assessed at 11 weeks after commencing chemoradiotherapy do in fact respond by 26 weeks , and the earlier assessment could lead to some patients having unnecessary surgery . 
our data suggests that the optimum time for assessment of complete clinical response after chemoradiotherapy for patients with squamous cell carcinoma of the anus is 26 weeks from starting chemoradiotherapy . 
however , present guidelines offer discordant advice on how often and when biopsy should be done and offer uncertainty over the optimum timing of response . added value of this study our post - hoc analysis of our trial data shows that tumour assessment at 26 weeks from the start of chemoradiotherapy is most strongly associated with progression and mortality compared with any earlier assessment . 
patients were randomised to one of four groups to receive mitomycin ( 12 mg / m on day 1 ) or cisplatin ( 60 mg / m on days 1 and 29 ) with fluorouracil ( 1000 mg / m per day on days 14 and 2932 ) and radiotherapy ( 504 gy in 28 day fractions ) ; with or without two courses of maintenance chemotherapy ( fluorouracil and cisplatin at weeks 11 and 14 )  . 
the full trial methods and results have been reported previously.7 participants patients were eligible if they had newly diagnosed , histologically confirmed squamous cell carcinoma basaloid or cloacogenic carcinoma of the anal canal or margin , without metastatic disease , and considered fit for trial treatment ; a glomerular filtration rate of 50 ml / min or more ; acceptable haematological para meters ( haemoglobin > 100 g per l , platelets > 100 10 per l , white blood cells > 3 10 per l ) ; liver function tests within twice normal range ; and function . 
exclusion other major malignancies likely to compromise life expectancy or completion of trial therapy , comorbidity including hiv - positive status and cardiac diseases , previous complete local excision , and previous radiotherapy to the pelvis . 
 procedures briefly , all patients received 504 gy delivered in 28 daily fractions over 38 days with fluorouracil on days 14 and 2932 by continuous intravenous infusion and either mitomycin as bolus on day 1 only or cisplatin by infusion on days 1 and 29.7 patients randomly allocated to receive maintenance were given two additional courses of fluorouracil and cisplatin on days 7174 and 9295 after the start of chemoradiotherapyie , weeks 11 and 14 . 
 before treatment , patients were staged according to the uicc 1990 staging system.12 abdominopelvic ct scans and chest radiographs or thoracic ct scans were mandated , but not mri or pet . to maintenance treatment started there were three primary tumour assessments ( figure 1 ) , made by the patients clinician ( single clinical oncologist review )  . 
 assessment 2 was at 18 weeks from the start of chemoradiotherapy ( 4 weeks after completion of maintenance therapy for those receiving it ) to assess the effect of maintenance therapy . 
assessment 3 was at 26 weeks from the start of chemoradiotherapy in case of treatment delay and this timepoint has been used in other squamous cell cancers to allow for tumours that relapse or progress early.13 information about examination under anaesthetic was not collected during the trial and biopsies were not routinely done unless there was a high suspicion of residual disease because of anxieties from the radiation oncologist regarding healing in an irradiated area ( according to uk practice )  . 
 patients who did not have a complete clinical response ( those with partial response , stable disease , or progressive disease who did not have salvage surgery before week 26 ) at either assessment 1 or 2 could have subsequent assessments and delay interventions at the time ( to determine slow responders )  . 
residual or recurrent disease was confirmed by biopsy before further therapy if results from other evaluations were ambiguous . patients were classified into two groups at each assessment : patients with a complete clinical response or patient without a complete clinical response ( ie , patients with a partial response , stable disease , or disease progression )  . 
patients who attended the assessments with insufficient response data were classified as unknown whereas those who either did not attend assessments or whose data were not reported were classified as missing . 
this post - hoc analysis investigated complete clinical response at all three assessments ( 11 weeks , 18 weeks , and 26 weeks from the start of chemoradiotherapy ) as well as progression - free survival and overall survival measured from the time of randomisation . 
 tumour factors and statistical analysis response and the association between progression - free survival or overall survival at each timepoint was examined by kaplan - meier curves and cox regression models . 
time - to - event endpoints were measured from the date of randomisation , and patients without the event of interest were censored at date of last follow - up . 
sensitivity analyses were done to check the effect of extrapolating nodal status when missing on the proportion of patients with a complete response . trial to ensure that the analyses were not biased by the inclusion of patients who died before assessment 3 , progression - free survival and overall survival were analysed both in all randomised patients using complete clinical response status where known , and those patients who attended clinic at all three timepoints and did not have salvage treatment before assessment 3 . two sensitivity analyses of progression - free survival and overall survival was done using two extreme assumptions . 
 the first was done on all ran domised patients , and where response status was unknown it was assumed to be complete clinical response , and the second was done on all ran domised patients , and where response status was unknown it was assumed to be notcomplete clinical response . 
analyses other than overall survival and progression - free survival were based on those patients who had tumour assessment data at all timepoints excluding those patients who had salvage treatment , to have a uniform dataset for these analyses , unaffected by missing tumour response data . 
this study is registered as at isrctn , number 26715889 . role of the funding source the funder had no role in study design , report writing , or collecting , analysing , or interpretation of the data . 
all authors made the decision to submit the report for publication and gave final approval for submission . results 940 patients were enrolled from june 4 , 2001 , until dec 16 , 2008 . 
the baseline characteristics of all individuals enrolled in the trial have been reported previously.7 overall , the median age was 58 years , 486 ( 52% ) of 940 had a primary tumour of 5 cm or smaller ( t1 or t2 ) , 430 ( 46% ) of 940 had a primary tumour larger than 5 cm or invasion to neighbouring organs ( t3 or t4 ) , 305 ( 32% ) of 940 had positive lymph nodes , 787 ( 84% ) of 940 had a tumour in the anal canal , and 132 ( 14% ) of 940 had a tumour in the anal marg of the 940 patients , 249 were excluded for subgroup tumour analysis : 241 patients did not attend all assessments , or had results where it was not possible to determine response status , and eight patients had salvage treatment before the third assessment . 
the baseline characteristics of these 691 remaining patients who were analysed in this subgroup analysis were similar to both the entire trial population 940 patients ( appendix p 1 ) , and the 249 patients who were excluded ( appendix p 2 )  . 
 the proportions of patients with primary tumour response data at all three assessments were similar in the two treatment groups ( 345 [ 73% ] of 472 patients who received mitomycin vs 346 ( 74% ) of 468 patients who received cisplatin ; appendix p 3 )  . 
eight of 19 patients with confirmed early progressive disease at assessments 1 or 2 had a potentially curative resection before week 26 and therefore had a complete clinical response at the third assessment ( week 26 )  . 
excluding these patients in the analysis had a negligible effect on the results . the median follow - up , censoring deaths , was 51 years ( iqr 3969 ) for all 940 patients and 52 years ( 4068 ) for the 691 patients who attended all three assessments . 
12 patients died before assessment 1 ( six from chemotherapy - related adverse events , two from anal cancer , three from reasons unrelated to cancer , and one from an unknown cause )  . 
no difference in the proportion of patients with a complete response is expected between patients with and without maintenance therapy at assessment 1 because maintenance treatment would only start after this time . 
the p values shown were calculated with tests . table 1 : complete clinical response at all three assessments in patients with primary tumour response data at all three assessments 940 trial patients.7 the median overall treatment time was 38 days ( iqr 3839 days ) in both the mitomycin and cisplatin groups . in our subgroup analysis of the 691 patients with response data at all three timepoints , the proportion of patients with complete clinical response increased over time : 441 ( 64% , 95% ci 6167 ) of 691 patients had a complete clinical response at assessment 1 , 556 ( 81% , 7888 ) at assessment 2 , and 590 ( 85% , 8388 ) at assessment 3 ( table 1 , 2 )  . 
421 ( 95% ) of 441 patients who had a complete clinical response at assessment 1 maintained this complete clinical response at assessment 2 and 411 ( 93% ) of 441 still had a complete clinical response at assessment 3 ( table 3 )  . 
the remaining 30 ( 7% ) of 441 patients either had a suspected relapse at assessment 2 or 3 ( n = 25 ) or they were missing data for nodal status ( n = 5 )  . 
complete clinical response was achieved in 492 ( 52% ) of 940 patients at assessment 1 ( 11 weeks ) , 665 ( 71% ) of patients at assessment 2 ( 18 weeks ) , and 730 ( 78% ) of patients at assessment 3 ( 26 weeks )  . 
however , 151 ( 72% ) of 209 patients who were not in complete clinical response at assessment 1 achieved complete clinical response by assessment 3 , and 115 ( 76% ) of 151 were alive and disease - free on last follow - up after treatment . 
therefore , 115 ( 55% ) of 209 patients who did not have a complete clinical response at assessment 1 could be considered slow responders . these 119 , of the overall trial population , 119 ( 13% ) of 940 patients did not have a complete clinical response at assessment 3 ( table 3 )  . 
of ( 2% ) patients had defunctioning stomas for side - effects of radiotherapy , 27 ( 23% ) had salvage surgery ( abdominoperineal excision of rectum or anorectal excision ) , and three had other types of surgery ( all done after 26 weeks )  . 
disease was pathologically confirmed before radical surgery . two the difference in the population of patients achieving a complete clinical response between patients in the cisplatin and mitomycin groups or between patients in the groups that received or did not receive maintenance was not significant at any assessment ( table 1 )  . 
the proportion of patients with a complete clinical response at patients with complete clinical response patients without complete clinical response patients with unknown response data * assessment 1 assessment 2 assessment 3 * patients classified as unknown attended the assessment but had response data that were inconclusive . 
some patients did not attend for more than one assessment or had missing response data for more than one assessment so it is not possible to sum these numbers over all three timepoints . table 2 : distribution of patients and tumour response for patients who attended all three assessments ( n = 691 ) patients with complete clinical response patients without complete clinical response patients with unknown response data * patients with missing data assessment 1 assessment 2 assessment 3 * patients classified as unknown attended the assessment but had response data that were inconclusive . 
some patients did not attend for more than one assessment or had missing response data for more than one assessment so it is not possible to sum these numbers over all three timepoints . table 3 : distribution of patients and tumour response for all patients in the trial ( n = 940 ) assessment 3 ( disregarding nodal status ) , was 311 ( 90% ) of 345 for mitomycin and 313 ( 91% ) of 346 for cisplatin ( appendix p 3 ) , similar to those among all 940 patients as previously reported ( 391 [ 91% ] of 432 patients treated with mitomycin and 386 [ 90% ] of 431 patients treated with cisplatin ) .7 when nodal status was included at assessment 3 ( 26 weeks ) , the results were similar , with 290 ( 84% ) of 345 patients in the mitomycin group achieving a complete clinical response compared with 294 ( 85% ) of 346 patients in the cisplatin group ( appendix p 3 )  . regardless of when patients were assessed , clinical complete response was affected by patients tumour size and nodal stage ( appendix p 5 )  . 
the 5 year overall survival for patients with complete clinical response and patients without a complete clinical response groups were : 83% ( 7986 ) and 72% ( 6678 ) at assessment 1 ; 84% ( 8187 ) and 59% ( 4967 ) at assessment 2 ; and 87% ( 8489 ) and 46% ( 3755 ) at assessment 3 . 
the overall survival for the subgroup of 691 patients who had tumour assessments at all three timepoints was also assessed ( appendix p 8 ) and was similar to that found in the overall trial population ( table 4 )  . 
the 5 year overall survival in this subgroup for patients with a complete clinical response and patients without a complete clinical response group was 85% ( 95% ci 8188 ) and 75% ( 6880 ) at assessment 1 , 86% ( 8288 ) and 61% ( 5070 ) at assessment 2 , and 87% ( 8490 ) and 48% ( 3658 ) at assessment 3 . progression - free survival for the overall trial population and the subgroup of patients with a response at all timepoints was also analysed ( table 4 , figure 3 , appendix p 9 )  . 
the 5 year progression - free survival in patients who had a complete clinical response compared with those who did not have a complete clinical response was 75% versus 63% at assessments 1 , 75% versus 53% at assessment 2 , and 80% versus 33% at assessment 3 . 
there was no difference in progression - free survival events in patients who had a complete clinical response at assessment 1 ( 105 events in 441 patients ) and those who had a complete clinical response only at assessment 3 ( nine events in 43 patients ) ( absolute difference 29 [ 95% ci 99 to 157 ] , p = 067 )  . we did several analyses for overall survival and progression - free survival to check for consistency in the results because 241 of 940 patients had missing tumour assess ments at one or more timepoints ( where the complete clinical response status was unavailable : unknown or missing ) and eight patients who had available data were excluded because they had salvage treatment . 
sensitivity analyses on the basis of imputing data for missing tumour response ( with assumptions ) and those who did not attend assessments ( which includes those for which response data were not reported ) provided similar results for both overall survival and progression - free survival as the main analysis ( table 4 , appendix pp 1013 ) ; as well as for imputation for missing nodal status , assumed to be either positive or negative ( appendix p 6 )  . 
 * adjusted for potential confounding factors : age , sex , site of primary , tumour differentiation , histology , baseline white blood cell count , baseline platelets , baseline haemoglobin , tumour size , nodal stage , and trial treatment . 
excluding eight patients who had salvage surgery . table 4 : association between overall survival or progression - free survival and tumour response at three different assessment timepoints after excluding 23 deaths occurring before assessment 3 ( which would otherwise bias the group of patients with missing data ) , there was no difference in overall survival between patients who attended , patients who did not attend this assessment , or those with data not reported ( table 3 )  . 
at 1 year the overall survival was 96% ( 95% 9598 ) for 809 patients who attended assessment 1 versus 91% ( 8495 ) for patients who either did not attend or had data unreported at assessment 1 . 
1 year overall survival at assessment 2 was 97% ( 9598 ) for the 852 patients who attended compared with 90% ( 8095 ) for 73 patients who did not attend or had data not reported , and 1 year overall survival at assessment 3 was 98% ( 9699 ) for the 871 patients who attended versus 84% ( 7092 ) for the 46 patients who did not attend or data not reported at assessment 3 ( data not shown )  . the sensitivity ( ie the number of patients with a complete response who are alive relative to the total number of patient alive ) of complete clinical response to predict overall survival was analysed at all three timepoints ( appendix p 7 )  . 
sensitivity of complete clinical response to predict overall survival at 1 year was the highest at assessment 3 ( 88% ) compared with at assessment 2 ( 85% ) or assessment 1 ( 68% )  . 
the probability of a false - positive at 1 year was also the lowest at assessment 3 ( 20% ) compared with assessment 2 ( 32% ) and assessment 1 ( 50% )  . discussion our results show that the proportion of those with a complete clinical response at 26 weeks ( assessment 3 ) is the informative more two earlier than either of assessments , and that it is acceptable to monitor partial responders carefully up to the 26 week assessment . 
this extended period with careful monitoring has not been international practice to date , and there are patients who have salvage surgery because of residual tumour found shortly after completing chemoradiotherapy . 
therefore it is important for patients and clinicians to establish the best time to assess tumour response , and we have done so with data from our clinical trial . there was no evidence that maintenance therapy acted as a confounding factor for the association between complete clinical response status and overall survival and progression - free survival , as maintenance therapy did not influence whether a patient had complete clinical response . 
moreover , maintenance treatment started only after assessment 1 , there was no difference in the complete clinical response rates between patients with and without maintenance therapy ( table 1 ) , and there was no effect of maintenance therapy on either progressionfree survival or overall survival , as detailed in our original report on this trial.7 since the median overall treatment time was the same in both the mitomycin and cisplatin groups ( 38 days [ iqr 3839 days ] ) the timing of assessment of complete clinical response was probably not confounded by variations in treatment duration . 
 there was a substantial increase in the proportion of patients with a complete clinical response at 26 weeks ( assessment 3 ) from the start of chemoradiotherapy compared with earlier assessments ( table 1 )  . 
our findings are also consistent with those previously described in a series of sequential chemoradiotherapy studies with mitomycin , 15 which showed that some patients with squamous cell carcinoma of the anus required 912 months to achieve a complete clinical ( defined as complete resolution of all clinical signs of the primary cancer for a duration of 2 months ; if not , the tumour was scored as residual )  . response a limitation of our analysis is that the group which achieved a complete clinical response at assessment 3 ( week 26 ) does not truly represent all responders to chemoradiotherapy because it also includes patients who have had an early and sustained response and those who have a late response , but not patients who had a complete clinical response at assessment 1 but subsequently relapsed or did not have a complete clinical response by assessment 3 . eventual outcomes ( overall survival and progression - free survival ) were independent of the timing that complete clinical response was achieved . 
the hrs from both the overall survival and progression - free survival curves suggest that assessment 3 ( 26 weeks from the start of treatment ) gives the most widely discriminating effect on survival outcomes , and suggests this is the optimum timepoint for assessment . 
tumour assessment ( including nodal status ) at week 26 should therefore be explored as a surrogate endpoint for progression - free survival and overall survival in future trials . these findings challenge guidelines8 , 9 for the posttreatment follow - up of patients with anal cancer , which include serial digital rectal examination , with biopsy of clinically suspicious lesions recommended at weeks 46 , 68 , and 812 after chemoradiotherapy completion , respectively . 
to address whether substantial bias could have arisen we made extreme assumptions about unknown status in two sensitivity analyses , and both produced the same conclusions irrespective of whether we considered the whole trial population or only those who attended all three assessmentsie , that the strongest association between complete clinical response 354 vol 18 march 2017 articles status and either overall survival or progression - free survival is at assessment 3 . anal cancers can regress slowly after completion of chemo radiotherapy treatment . 
clinical groups recommended salvage surgery should only be considered after at least 12 weeks because complete resolution might take 36 months.1 the ideal method and timing of response evaluation and when maximum response occurs after chemoradiotherapy is unclear . 
retrospective reports suggested initial early clinical response is an independent survival.1618 randomised studies have done clinical assessments of the tumour between 6 weeks and 12 weeks after completion of chemoradiotherapy.16 prognostic factor for the mainstay of clinical evaluation has relied on digital rectal examination and careful examination of the inguinal regions . 
the limitations of this approach include the subjectivity of the clinical examination and the absence of treatment response information for any more deeply sited , non - palpable disease , including the pelvic lymph nodes . 
severe skin reactions , oedema , residual fibrosis , or scar tissue can be difficult to distinguish from persistent , active , or recurrent disease.19 , 20 the risk of radionecrosis should also be kept in mind when considering biopsy . 
a significant correlation has also been observed between high - grade acute toxicity in terms of skin reactions , cystitis , proctitis , or enteritis ( national cancer institute common toxicity criteria grade 3 or worse ) during chemoradiotherapy and overall survival , loco regional control , and stoma - free survival.21 imaging in terms of endoanal ultrasound or mri has an established role in initial locoregional staging of the primary and pelvic lymph nodes , 8 , 10 but their ability to assess response accurately is less welldefined.22 it can take 1620 weeks to allow sufficient time for resolution of oedema to enable accurate classification of treatment response by ultrasound.23 mri complements clinical assessment but can assign a worse stage prognosis to a patient , particularly lymph node status because enlarged lymph nodes can be recorded as node positive although many do not contain tumours . 
metabolic and functional imaging techniques , such as diffusion - weighted mri , 24 or pet with f - fluorodeoxyglucose , 2527 might offer an alternative option to assess response at an early timepoint without the potential morbidity of a biopsy , but large prospective studies are required . the reported 5 year overall survival with salvage locally abdominoperineal resection for persistent or recurrent anal cancer was only 2464% ; 28 , 29 hence , the rationale for proactive follow - up . 
for surgeons , there is always a tension between doing an early biopsy to define an early recurrence with limited locoregional disease , when surgical salvage is likely to be effective , and the risk of provoking necrosis from a biopsy after chemoradiotherapy . 
 209 ( 30% ) of 691 patients were not in complete clinical response 4 weeks after chemoradiotherapy ( assessment 1 ) ; however , 115 remained disease - free at later follow - up , hence , early surgical salvage would not have been appropriate for these patients . the rtog - 8704 trial mandated biopsy of the primary tumour at 46 weeks after a dose of 45 gy to confirm complete pathological response in clinically residual disease , 1 but routine biopsy is controversial in the monitoring of response to treatment , with some clinicians supporting random biopsies at a 3 month interval , while others support a biopsy only when there is a suspicious lesion.30 our results suggest that early response assessments might not be reliable by failing to account for patients who are slow to respond to treatment . 
the consistency of the overall treatment time ( median 38 days ) makes the validity of our data for timing of complete clinical response assessment even stronger . although we would advise careful monitoring from completion of treatment to facilitate timely surgical salvage therapy for progressive disease , it seems safe to observe a resolving tumour up to 26 weeks after the start of chemoradiotherapy , and some patients could thus avoid unnecessary surgery . 
it might even be safe to extend evaluation beyond this timepoint , as some studies suggest a few patients might require more than 10 months for complete regression , but prospective data are required to confirm this timeline . 
we propose guidelines should be revised , and that the assessment of response at 26 weeks be used in future trials and explored as a surrogate endpoint for overall survival and progression - free survival . contributors rg - j , ds - m , dc , lk , ah , hmm contributed to the design of this substudy , the figures , data collection , data interpretation , and writing . 
all authors reviewed iterations of the manuscript and gave final approval . vol 18 march 2017 articles declaration of interests dc has received research funding from amgen , astrazeneca , bayer , celgene , merrimack medimmune , merck , and sanofi and rg - j has received grant funding and personal fees from merck and roche , and personal fees from eisai , amgen , and servier . 
we thank all those who participated in this trial , clinicians and their staff , and patients . articles characterisation of retinoblastomas without rb1 mutations : genomic , gene expression , and clinical studies diane e rushlow , berber m mol , * jennifer y kennett , * stephanie yee , * sanja pajovic , brigitte l thriault , nadia l prigoda - lee , clarellen spencer , helen dimaras , timothy w corson , rene pang , christine massey , roseline godbout , zhe jiang , eldad zacksenhaus , katherine paton , annette c moll , claude houdayer , anthony raizis , william halliday , wan l lam , paul c boutros , dietmar lohmann , josephine c dorsman , brenda l gallie summary background retinoblastoma is the childhood retinal cancer that de ned tumour - suppressor genes . 
we aimed to characterise non - familial retinoblastoma tumours with no detectable rb1 mutations . methods of 1068 unilateral non - familial retinoblastoma tumours , we compared those with no evidence of rb1 mutations ( rb1 + / + ) with tumours carrying a mutation in both alleles ( rb1 / )  . 
we analysed genomic copy number , rb1 gene expression and protein function , retinal gene expression , histological features , and clinical data . findings no rb1 mutations ( rb1 + / + ) were reported in 29 ( 27% ) of 1068 unilateral retinoblastoma tumours . 
15 of the 29 rb1 + / + tumours had high - level mycn oncogene ampli cation ( 28121 copies ; rb1 + / + mycna ) , whereas none of 93 rb1 / primary tumours tested showed mycn ampli cation ( p < 00001 )  . 
rb1 + / + mycna tumours expressed functional rb1 protein , had fewer overall genomic copy - number changes in genes characteristic of retinoblastoma than did rb1 / tumours , and showed distinct aggressive histological features . 
median age at diagnosis of the 17 children with rb1 + / + mycna tumours was 45 months ( iqr 3510 ) , compared with 24 months ( 1537 ) for 79 children with nonfamilial unilateral rb1 / retinoblastoma . interpretation ampli cation of the mycn oncogene might initiate retinoblastoma in the presence of non - mutated rb1 genes . 
these unilateral rb1 + / + mycna retinoblastomas are characterised by distinct histological features , only a few of the genomic copy - number changes that are characteristic of retinoblastoma , and very early age of diagnosis . funding national cancer institutenational institutes of health , canadian institutes of health research , german research foundation , canadian retinoblastoma society , hyland foundation , toronto netralaya and doctors lions clubs , ontario ministry of health and long term care , uk - essen , and foundations avanti - str and kika . that predisposes introduction retinoblastoma set the paradigm for tumour - suppressor genes , with knudsons classic hypothesis predicting that two rate - limiting hits initiate this childhood eye cancer.1 the two hits were later attributed to the retinoblastoma gene ( rb1 ) .2 40% of children with retinoblastoma have bilateral disease . 
accepted dogma is that disruption of both rb1 alleles ( rb1 / ) initiates all cases of retinoblastoma.24 the mutant rb1 allele is identi able in blood samples of 95% of bilaterally a ected patients . 
low - level mosaicism can account for the remaining 5% of blood samples in which no mutation is found.5 previously , we have identi ed mutations in both rb1 alleles ( or promoter methylation ) in more than 95% of tumours from unilateral probands with no known family history.5 , 6 in 34% of tumours , we iden ti ed only one rb1 mutation , and in 2% we saw no disruption to rb1 . 
we obtained tissue samples and clinical data for identi cation of rb1 mutations from children in clinical care at these labora tories , and laboratory contributed both local and international families . 
we did either qm - pcr ( toronto ) or mlpa or snp analyses ( amsterdam ) to measure genomic copy numbers of ve genes known to be commonly altered in rb1 / retinoblastomas ( kif14 , dek , e2f3 , cdh11 , and mycn )  . 
we used sub - megabase resolution array comparative genomic hybridisation ( acgh ) or snp array to assess overall genomic copy numbers and nontumour cell contamination ( appendix p 3 )  . we placed three primary rb1 + / + mycna tumours in the same culture conditions that support growth of rb1 / cell lines , and we developed these into cell lines ( appendix p 4 )  . 
we stained para n - embedded sections of retinoblastomas and adjacent normal retinas for fulllength rb1 protein ( antibodies targeted n - terminal and c - terminal rb1 protein ) and mycn protein.8 we did western blots on rb1 + / + mycna and rb1 / primary tumours and cell lines , control rb1 + / + human fetal and adult retina , and lines lymphoblastoid and neuroblastoma cell ( appendix pp 34 )  . 
we did western blotting to assess the function of rb1 protein , using phospho - speci c anti - rb1 and coimmunoprecipitation of rb1 and its major e ector molecule e2f1 . 
we used endpoint reverse transcriptase pcr ( rt - pcr ) or quantitative real - time pcr to measure expression of rb1 , mycn , and genes re ecting the proliferative status and retinal derivation of tumours . statistical analysis to assess the likelihood that rb1 + / + tumours originated from two undetected rb1 mutations , we did the goodness - oft test , using default probabilities of p1 = 00025 for rb1 + / + and p2 = 09975 for rb1 / samples ( appendix pp 45 )  . 
to compare the proportion of rb1 + / + unilateral tumours at every study site and frequencies of speci c genomic copy - number changes of tumours with di erent rb1 statuses , we used fishers exact test ( appendix p 13 ) .9 we used the t test with welchs adjustment to compare the total number of bp altered per region between rb1 + / + mycna and rb1 / tumours ( appendix p 5 )  . 
 we processed normalised intensity values with the circular binary segmentation algorithm , with data ltered identify only high quality ( greater than three con rmatory probes ) and suitably sized ( > 25 kbp ) regions of clear di erential signal relative to normal ( |meansignal| > 01 )  . 
we used a contrast matrix to identify the number of di erentially abundant probes relative to normal sam ples with an empirical bayes moderation of se and a false - discovery rate adjustment 328 vol 14 april 2013 articles for multiple testing . 
to ascertain if ages at diagnosis were from a one - hit or two - hit distribution , 1 we estimated the parameter k in the equation ln s = kt ( in which s is the proportion of cases not yet diagnosed and t is age at diagnosis ) through a simple linear nointercept regres sion analysis . 
we regressed the empirical values of s on age at diagnosis , 1 assuming an exponential distribution ( one - hit ) , and in the equation ln s = kt , assuming a weibull distribution with shape parameter of two ( two - hit )  . 
to compare the relative t of these data to the two assumptions , we plotted data points for rb1 / and rb1 + / + mycna cases and the besttting curves . 
we used sas version 9.3 ( ts level 1m1 ) for analyses of number of events to initiate retinoblastoma . role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
all authors had full access to all data in the study ; the corresponding author ( blg ) had nal responsibility for the decision to submit for publication . results during clinical work in toronto , we found seven ( 16% ) of 441 unilateral retinoblastoma tumours with no rb1 mutations , no promoter methylation , and no rb1 loss of heterozygosity ( rb1 + / + )  . 
we used qm - pcr to measure , in rb1 + / + tumours , copy numbers of genes at 6p , 1q , 16q , and 2p that are characteristically gained or lost in rb1 / retinoblastoma tumours.10 unexpectedly , ve of seven rb1 + / + tumours showed striking ampli cation of the mycn oncogene ( mycna )  . 
we combined our data on 1068 primary unilateral non - familial retinoblastoma tumours after statistical analysis showed that frequencies did not di er by much ( p = 008 ) between the ve laboratories ( table 1 )  . 
 laboratories the standard sensitivity for nding the rb1 mutation in blood samples of bilaterally a ected individuals is greater than 95%.57 the probability of nding no rb1 mutations in a tumour with no rb1 loss of hetero zygosity is equivalent two independent rb1 mutations in one sample ( 005005 ) or 025% . 
qm - pcr = quantitative multiplex pcr . non - familial tumours , we identi ed 29 ( 27% ) rb1 + / + tumours , tenfold more than expected ( p < 00001 ; table 1 )  . 
 subsequently , a new patient was predicted clinically and pathologically to have an rb1 + / + mycna tumour ( t101 ) , con rmed by mycn copy number ; thus , 30 rb1 + / + retinoblastomas were included in further analyses ( appendix p 6 )  . to characterise copy numbers of genes commonly gained or lost in retinoblastomas , 10 we used qm - pcr ( toronto ) or mlpa and snp ( amsterdam ) analyses . 
except for mycn copy number , acgh ( gure 2a ) con rmed a reduced frequency in rb1 + / + mycna retino blastomas of the speci c genomic copy - number changes characteristic of rb1 / retinoblastomas ( gure 1 ; appendix p 13 ) .10 also , rb1 + / + mycna retino blastomas showed signi cantly fewer altered bp and acgh clones overall than did rb1 / retinoblastomas ( p = 0033 ; gure 2a ; appendix pp 31 , 1428 )  . we used acgh11 or snp analysis3 to study mycn ampli cations in 14 rb1 + / + mycna retinoblastomas , one rb1 + / tumour ( t33 , with 73 mycn copies ) , and one rb1 / primary tumour ( rb381 , with 92 copies of mycn )  . 
of the 35 remaining unilateral tumours tested by acgh ( ten rb1 / , 13 rb1 / + , and 12 rb1 + / + ) , 24 showed no gain or loss at mycn , and 11 had moderate gain spanning a broad region of at least 28 mbp of chromosome 2p , too large to meet the de nition of ampli cation.13 amplicon de ned by three of 14 rb1 + / + mycna tumours showed 17q213 - qter or 17q243 - qter gain ; two showed 11q loss . 
both regions are commonly altered in neuroblastoma , 14 , 15 but changes are rare in rb1 / retinoblastoma.16 , 17 other changes in rb1 + / + mycna retinoblastomas not typically seen in rb1 / retinoblastoma were gains at 14q and 18q and losses at 11p ( gure 2a ; appendix pp 1420 , 33 )  . retinoblastoma t33 ( rb1 + / ) showed high - level mycn ampli cation and loss of one copy of most of 13q , including rb1 ; we suspect that ampli cation of mycn initiated proliferation , followed by 13q deletion . 
since t33 showed several characteristics of rb1 + / + mycna tumours , we included t33 with mycna retinoblastomas in clinical analyses ( gure 2 , gure 3a ; appendix pp 32 , 34 )  . rb1 + / + mycna retinoblastomas and retinal cell types ( ganglion cells , speci c inner nuclear cells , and cone photoreceptors ) 18 expressed functional rb1 protein and showed nuclear staining for c - terminal ( gure 4a ; appendix p 34 ) and n - terminal ( data not shown ) epitopes , whereas rb1 / and rb1 + / tumours were negative or stained weakly , depending on their rb1 mutations . 
 western blots and three rb1 + / + mycna cell lines ( a3 , rb522 , and t101 ) derived from rb1 + / + mycna primary retinoblastomas showed functional , nuclear , full - length rb1 protein ( appendix pp 3435 ) , normally hypophosphorylated and hyperphosphorylated ( gure 4b ; appendix p 35 ) , and bound to e2f1 ( gure 4c ) , which is the major target of rb1 protein and controls the cell cycle.19 full - length 28 kbp rb1 transcripts were detected by endpoint and real - time immunoprecipitation age at diagnosis ( months ) rb1 / rb1 + / + mycna age at diagnosis ( months ) figure 3 : clinical features of children with retinoblastomas ( a ) age at diagnosis of children with retinoblastomas . 
 ( b ) knudson one - hit and two - hit plots for children with rb1 / or rb1 + / + mycna tumours , comparing proportion not yet diagnosed with age at diagnosis , using birth as a surrogate for initiation . 
scatterplot does not distinguish children of identical ages . children with rb1 + / + mycna tumours , dna from available blood samples showed two mycn copies . tumours showed a the 16 rb1 + / + mycna lower frequency of copy - number changes in four other genes characteristic of retinoblastoma , compared with rb1 / retinoblastoma : gain of oncogenes kif14 ( three of 16 [ 19% ] vs 55 of 89 [ 62% ] ; p = 0002 ) , dek ( one of 16 [ 6% ] vs 50 of 87 [ 57% ] ; p = 00002 ) , and e2f3 ( one of 16 [ 6% ] vs 52 of 90 [ 58% ] ; p = 00002 ) ; and loss of tumour - suppressor gene cdh11 ( two of 16 [ 13% ] vs 50 of 90 [ 56% ] ; p = 0002 ; gure 1 ; appendix pp 613 )  . 
snp analysis indicated that level of non - tumour cell contamination the rb1 + / + mycna tumours was low and similar to rb1 / tumours ( appendix p 3 )  . to probe for other genomic gains or losses , we studied dna from 48 unilateral retinoblastomas by acgh11 ( 11 rb1 + / + mycna , 12 rb1 + / + , 14 rb1 / , and 11 rb1 + / in samples from canada , germany , france , and new zealand ) and three rb1 + / + mycna tumours by snp analysis ( netherlands ; gure 2a ; appendix pp 612 , 1428 , 33 )  . 
 none of the rb1 + / + mycna retino blastomas showed any evidence of copy - number changes or translocations12 at the 330 vol 14 april 2013 articles rt - pcr in three rb1 + / + mycna primary retinoblastomas for which mrna was available ( appendix pp 29 , 36 )  . 
 by contrast , four primary rb1 / retinoblastomas expressed low rb1 transcript levels relative to fetal and adult retina . rb1 + / + mycna primary retinoblastomas ( gure 4a ) and three derived cell lines ( data not shown ) stained strongly for mycn prote mycn and ki67 transcripts ( indicative of proliferation ) were found at low levels in adult retina , at higher levels in fetal retina and in rb1 / retinoblastomas without mycn ampli cation , and at very high levels in primary rb1 + / + mycna retinoblastoma and rb1 / cell lines with mycn ampli cation ( appendix pp 29 , 36 )  . 
rb1 + / + mycna tumours showed reduced expression of the oncogene kif14 , 10 by contrast with healthy fetal retina and rb1 / primary retinoblastomas , which overexpressed kif14 ( appendix pp 29 , 36 )  . rb1 + / + mycna tumours expressed embryonic cell markers consistent with a retinal origmrna of cone cell marker x - arrestin20 and crx ( a marker of retinal and pineal lineage in rb1 / tumours , which retinoblastoma but not in neuroblastoma ) 21 were expressed in fetal retina , human adult retina , and rb1 + / + mycna and rb1 / primary retinoblastomas ( appendix p 36 )  . is strongly expressed children with rb1 + / + mycna retinoblastomas were much younger at diagnosis than were those with uni lateral rb1 / retinoblastomas . 
we estimated that 18% of children diagnosed with non - familial unilateral retinoblastoma at age 6 months or younger will have rb1 + / + mycna retino blastoma ( appendix p 5 )  . analysis of age at diagnosis versus proportion not yet diagnosed led knudson to propose his two - hit model for initiation of retinoblastoma.1 our data for 79 unilaterally a ected rb1 / patients accorded with knudsons model and t a two - hit curve , representative of two independent mutational events in a tumour - suppressor gene ( gure 3b )  . 
 similar analysis of rb1 + / + mycna tumours was inconclusive : although datapoints for 12 children diagnosed before age 10 months approximated the calculated one - hit curve , ages for older children deviated ( gure 3b )  . rb1 + / + mycna tumours had distinctive histological features , comprising undi erentiated cells with large , prominent , multiple nucleoli , and necrosis , apoptosis , and little calci cation . 
flexnerwintersteiner rosettes23 and nuclear moulding , which are characteristic of prototypic rb1 / retinoblastoma ( gure 5b ) , were absent . mycn 60 m 60 m 60 m specimen total prb1 e2f1 60 m e2f1 e2f1 e2f1 immunoprecipitate e2f1 immunoprecipitate e2f1 e2f1 e2f1 e2f1 e2f1 figure 4 : expression of rb1 and mycn ( a ) staining of adjacent retinal tissue and rb1 + / + mycna or rb1 mutant retinoblastoma for mycn protein and rb1 protein ( c - terminus antibody )  . 
 ( b ) western blots with anti - rb1 that recognises both hypophosphorylated and hyperphosphorylated rb1 protein ( total rb1 ) , phospho - rb1 ( ser795 ) antibody ( prb1 ) , and anti - e2f1 . 
 ( c ) cell lysates immunoprecipitated with antibodies against mouse igg ( negative control ) , rb1 protein , and e2f1 , and western blots done with antibodies to rb1 and e2f . clinically , rb1 + / + mycna retinoblastomas were large and invasive , in view of the young age of a ected children ( gure 5c ; appendix p 37 )  . 
 ( c ) rb1 + / + mycna retinoblastoma in an 11 - month - old child ( a2 ) with extraocular extension into the optic nerve ( triple arrows ; haemoxylin and eosin staining )  . 
 ( d ) 35 - month - old child with a small , heritable , rb1 / retinoblastoma present in the inner nuclear layer of the retina on optical coherence tomography ( oct )  . mutation of which is widely assumed to initiate all retinoblastoma ( panel )  . 
in this report , we have described a previously unrecognised form of retinoblastoma that has no evidence of rb1 muta tions , displays functional protein , and is probably initiated by ampli cation of the mycn oncogene . 1068 unilateral non - familial retinoblastomas , identi ed a distinct rb1 + / + mycna subtype that constituted 14% of the sample ( n = 15 )  . 
despite the low frequency of rb1 + / + mycna retinoblastoma , this tumour subtype was discovered and characterised independently in two laboratories ( toronto and amsterdam ) , using di erent cohorts and technologies . 
 statistical analyses show that although rare , rb1 + / + mycna retinoblastomas a ect an im portant subset of patients . rb1 + / + mycna retinoblastomas , but we did not have enough rb1 + / + tumour samples for gene expression or protein studies . 
although rb1 + / + mycna retinoblastomas have not been recognised previously as a distinct subtype , they resemble large nucleolar neuro blastomas with mycn ampli cation and poor out come.22 similar to mycn - ampli ed neuroblastomas , 15 rb1 + / + mycna tumours have less complex alterations of genomic copy number than do tumours without mycn ampli cation , suggesting that mycna could be the important driver of malignancy . 
loss of rb1 to genomic time less are rb1 + / + mycna tumours truly retinoblastomas ? these malignant subtypes arise in and express markers of embryonic retina , meeting the de nition of retinoblastoma as a blast - cell tumour arising from the retina.20 , 21 , 29 we showed intact rb1 genes in primary rb1 + / + mycna retinoblastomas with strong nuclear rb1 antibody staining . 
three rb1 + / + mycna cell lines expressed full - length rb1 mrna and inactive hyperphosphorylated and active hypophosphorylated rb1 protein that coimmunoprecipitated with e2f1 , indicating normal functional rb1 protein.19 the possibility that nonmalignant cell contamination could be masking rb1 mutations in rb1 + / + mycna tumours is ruled out because three rb1 + / + mycna cell lines grew rapidly from the primary tumours , unlike rb1 / retinoblastoma , and maintained the rb1 + / + mycna genotype of the primary tumours . although next - generation dna sequencing is a powerful discovery technique , its clinical application has not yet achieved sensitivity to match rb1 mutation technologies . 
if an rb1 mutation were detection identi ed by the next - generation enhanced read depth approach , that variant would represent convergent evolution to knockout rb1 protein with cancer progression , common in many cancers , rather than an initiating rb1 mutation . 
based on the cell - line genotypes , the mycn ampli cation would still be the event common to all cells and , thereby , the probable initiating event . we also identi ed 14 rb1 + / + retinoblastomas without mycn ampli cation . 
acgh showed genomic gains and losses that were distinct from either rb1 / or the very early presentation of rb1 + / + mycna retinoblastomas , absence of rb1 mutations , functional rb1 protein , and high mycn ampli cation in a genome with a 332 vol 14 april 2013 articles fairly stable copy number suggests that these tumours arise by somatic mycn oncogene ampli cation in a retinal progenitor cell . 
this idea is supported by the nding of one rb1 + / + mycna tumour in which mycn ampli cation was the only identi ed genomic copy - number change . 
the method by which mycn ampli cation is initiated , and whether mycn ampli cation alone is su cient to initiate retinoblastoma , remains to be shown formally . treatment , which in retinal development , the mycn protein can sup port cell division without activation of the e2f family of transcription factors ; presumably , unregu lated mycn expression associated with high - level gene ampli cation in rb1 + / + mycna tumours promotes cell division by indirect inactivation of rb1 protein.30 the relative genomic stability of rb1 + / + mycna retino blastomas could result in less resistance in rb1 / retinoblastoma associated with progressive genomic rearrangements . 
we predict that , worldwide , infants younger than 1 year24 with extraocular retinoblastoma could have rb1 + / + mycna tumours and might bene t from anti - mycn treatment.31 this idea accords with an anecdotal observation by one of us ( blg ) during review of retinoblastoma pathology slides in kenya , of rb1 + / + mycna histological ndings in an orbital recurrence , later con rmed to have 40 mycn copies . is seen the young age at diagnosis of unilateral retinoblastoma is interpreted frequently as an indication of heritable disease and is cited as a reason to try to cure the cancer without enucleation . 
although we predict that 18% of children diagnosed with non - familial unilateral retinoblastoma at age 6 months or younger will have rb1 + / + mycna retinoblastoma ( appendix p 5 ) , if tumour size is also considered , rb1 + / + mycna tumours might be clinically predictable , facilitating prompt removal of these eyes with good outcomes for children . including invasion standard care for unilateral non - familial retinoblastoma is identi cation of the rb1 mutant alleles in the tumour and examination of blood to ascertain whether either mutant allele is germline . 
diagnosis panel : research in context systematic review we systematically searched pubmed with the terms : retinoblastoma , initiation , and genetics ; retinoblastoma tumour genetics ; retinoblastoma development ; and retinoblastoma initiation . 
we identi ed no data to challenge knudsons 1971 conclusion that two rate - limiting events , 1 later shown to be loss of both rb1 gene alleles , 25 , 7 are essential , but not necessarily su cient , for development of retinoblastoma . 
we found no data to suggest other forms of retinoblastoma . interpretation with our collaborative studies , we identi ed a previously unrecognised disease : retinoblastoma with normal rb1 genes , apparently driven by mycn oncogene ampli cation . 
attempts to salvage the eye on the assumption of heritable disease in young children could incur high treatment morbidity and failure to cure these aggressive oncogene - driven retinoblastomas . rb1 status rb1 protein expression mycn copy number mycn mrna expression histological characteristics classic rb1 ( cid : 8 ) / ( cid : 8 ) novel rb1 / mycna / rare moderate rosettes full - length , nuclear , phosphorylated , binds e2f1 high multiple nucleoli and blast cells speci c and general genomic gains and losses common uncommon 29 copies , wide region 28121 copies , narrow amplicon median ( iqr ) age at diagnosis ( months ) 24 ( 1537 ) 45 ( 3510 ) table 2 : di erences between classic rb1 ( cid : 8 ) / ( cid : 8 ) tumours and novel rb1 / mycna unilateral non - familial retinoblastoma of rb1 + / + mycna retinoblastoma strongly suggests nonhereditary disease , with normal population risks for retinoblastomas in the other eye and for other cancers throughout life , and no familial risks . our ndings challenge the longstanding dogma that all retinoblastomas are initiated by rb1 gene mutations . 
 rb1 + / + mycna retinoblastoma di ers from classic retinoblastoma in terms of both genetics and clinical characteristics ( table 2 ) , with immediate relevance to patients . contributors der recognised the initial connection between mycn ampli cation and rb1 mutation status , did the literature search and qm - pcr analysis , supervised rb1 mutation analysis , coordinated collaborations with the other sites , and made a major contribution to preparation of the report . 
hd and twc did the vol 14 april 2013 articles literature search , assisted with data analysis and ideas for the discussion , and contributed to preparation of gures and the report . 
rg discovered and characterised the rst tumour with mycn ampli cation and normal rb1 protein ( rb522 ; now rb1 + / + mycna ) and provided the cell line and western blot showing multiple bands of rb1 protezj and ez did western blots speci c to phosphorylated rb1 protekp and acm provided and interpreted clinical data and images . 
all authors contributed ideas and helped to write the report . con icts of interest blg was part - owner of solutions by sequence and was a board member of retinoblastoma solutions ( now impact genetics , of which blg is medical director )  . 
all other authors declare that they have no con icts of interest . acknowledgments we thank the sponsors of the study : the national cancer institute national institutes of health ( grant 5r01ca118830 - 05 [ blg ] ) ; canadian institutes for health research ( grants mop - 86731 , mop - 77903 , and mop - 110949 [ wll ] , and mop - 77710 [ ez ] ) ; the canadian retinoblastoma society ; hyland foundation ; toronto netralaya and doctors lions clubs ; the alcon research institute ; the ontario ministry of health and long term care ; retinoblastoma solutions and solutions by sequence ( now impact genetics ) ; the german research foundation ( grant lo 530 / 6 - 2 ) ; uk - essen ; avanti - str ( jcd , j cloos , and acm ) ; kika ( jcd , h te riele , j cloos , acm ) ; vu university medical center ; ontario institute for cancer research and the government of ontario ( pcb ) ; cca / v - ici / avanti - str ( bmm ) ; the vision science research program of the university health network and the university of toronto ( sy ) ; and queens university school of medicine ( great west life studentship [ rp ] )  . 
we thank : irsan kooi ( vu university medical center ) for assessment of normal - cell contamination by snp data ; leslie mackeen for the collage of retcam images in gure 3b ; valerie white ( university of british columbia ) for clinical and pathological details and images ; cynthia vandenhoven for clinical images in gure 5 ; members of the vu university medical center / the netherlands cancer institute , institut curie , institut fr humangenetik , toronto retinoblastoma teams , and other colleagues for useful discussions ; and the children and families who donated tissues for these studies . 
 corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
 the corrected version rst appeared at thelancet.com / oncology on sept 4 , 2014 see articles lancet oncol 2014 ; 15 : 68999 see editorial lancet oncol 2014 ; 15 : 667 patient priority in the era of patent expiries on aug 8 , 2014 , the uk national institute for health and care excellence ( nice ) ruled that trastuzumab emtansine is not cost e ective for routine use for patients with her2 - positive breast cancer in englands national health service . 
 using clinical data from the emilia and th3resa trials , roche valued the drug at just over 90 000 per patient more than twice the price of trastuzumab alonedespite a lack of head - to - head evidence showing trastuzumab emtansines greater e cacy compared with trastuzumab to justify the higher price . 
on july 28 , 2014only 11 days before nice issued their press releasethe patent for trastuzumab ( which earnt the company us$59 billion in 2011 alone ) expired in the european union ( eu )  . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy investment in research and development . 
despite the deal falling through , the attempted acquisition may be representative of pharmaceutical companies responses in recent years to try to recoup losses from a series of drugs that have simultaneously gone o patent . 
 this phenomenonthe so - called patent cli has been extensively reported since one of the rst blockbusters , atorvastatin , a cholesterol - lowering drug that had estimated global sales in excess of 64 billion a year , went o patent in 2011 . 
since then , and in light of an unprecedented number of blockbuster drugs coming o or soon to come o patent , a urry of mergers and acquisitions by pharmaceutical companies has taken place in an attempt to revive pro ts , most notably in diversifying their portfolio in to low - risk revenue streams ( eg , animal health , medical devices , and generic drugs ) as well as expanding their pipelines to include biological agents . 
despite the number of legitimate steps taken to extend patent licences , there have also been a series of morally dubious legal strategies used by patent proprietors to extend their patents . 
in addition to applying for supplementary protection certi cates ( allowing the patent to be extended up to 5 years in the eu ) , and 6 - month paediatric exclusivity licences , both of which are common practices to extend patent protection , pharmaceutical companies have explored other ways to gain extensions to their existing patents , such as new approvals in di erent medical settings to the original application . but where is the line between legitimate patentable development , and abusive extension of patent rights ? in 2001 , glaxosmithkline accumulated 5 years of 30 - month stay approval from the us food and drug administrationan automatic period granted to originator companies if threatened by patent infringementfor the drug paroxetine . 
although lawful , this example does raise the question as to whether these strategies are a violation of patients rights of access to a ordable , e ective medicines , especially considering the unsustainable nancial burdens faced by health - care systems worldwide . 
in a bid to maintain income , it is worrying that the pharmaceutical industry might opt to prioritise loopholes in legislation , undertake litigation , and consider mergers and acquisitions as a more rewarding primary focus to secure revenue , as opposed to competitive income from the development of new medicinal products . 
it is crucial , therefore , that appropriate legislation is in place to encourage strike a balance pharmaceutical between their own pro t ability and upholding a contemporary social and ethical responsibility to allow a ordable access to medicines to those most in need . 
 the lancet oncology companies vol 15 september 2014 1039 novel molecular subgroups for clinical classification and outcome prediction in childhood medulloblastoma : a cohort study edward c schwalbe , janet c lindsey , sirintra nakjang , stephen crosier , amanda j smith , debbie hicks , gholamreza rafiee , rebecca m hill , alice iliasova , thomas stone , barry pizer , antony michalski , abhijit joshi , stephen b wharton , thomas s jacques , simon bailey , daniel williamson , steven c clifford summary background international consensus recognises four medulloblastoma molecular subgroups : wnt ( mbwnt ) , shh ( mbshh ) , group 3 ( mbgrp3 ) , and group 4 ( mbgrp4 ) , each defined by their characteristic genome - wide transcriptomic and dna methylomic profiles . 
we aimed to investigate whether additional molecular subgroups exist within childhood medulloblastoma and whether these could be used to improve disease subclassification and prognosis predictions . methods in this retrospective cohort study , we assessed 428 primary medulloblastoma samples collected from uk childrens cancer and leukaemia group ( cclg ) treatment centres ( uk ) , collaborating european institutions , and the ukccsg - siop - pnet3 european clinical trial . 
we did comprehensive molecular profiling , including dna methylation microarray analysis , and did unsupervised class discovery of test and validation cohorts to identify consensus primary molecular subgroups and characterise their clinical and biological significance . 
we modelled survival of patients aged 316 years in patients ( n = 215 ) who had craniospinal irradiation and had been treated with a curative intent . findings seven robust and reproducible primary molecular subgroups of childhood medulloblastoma were identified . 
mbshh was split into agedependent subgroups corresponding to infant ( < 43 years ; mbshh - infant ; n = 65 ) and childhood patients ( 43 years ; mbshh - child ; n = 38 )  . 
cross - validated subgroup - dependent survival models , incorporating these novel subgroups along with secondary clinicopathological and molecular features and established disease risk - factors , outperformed existing disease risk - stratification schemes . 
these subgroupdependent models stratified patients into four clinical risk groups for 5 - year progression - free survival : favourable risk ( 54 [ 25% ] of 215 patients ; 91% survival [ 95% ci 82100 ] ) ; standard risk ( 50 [ 23% ] patients ; 81% survival [ 7094 ] ) ; highrisk ( 82 [ 38% ] patients ; 42% survival [ 3156 ] ) ; and very high - risk ( 29 [ 13% ] patients ; 28% survival [ 1456 ] )  . interpretation the discovery of seven novel , clinically significant subgroups improves disease risk - stratification and could inform treatment decisions . 
these data provide a new foundation for future research and clinical investigations . funding cancer research uk , the tom grahame trust , star for harris , action medical research , sparks , the jgw patterson foundation , the instinct network ( co - funded by the brain tumour charity , great ormond street childrens charity , and children with cancer uk )  . copyright the author ( s )  . 
 profiling and class discovery studies published to date in medulloblastoma are based on cohorts typically with sample sizes less than 200 patients and , even within the consensus subgroups , significant heterogeneity of clinical and molecular features remains and many relationships to disease outcome are unresolved . 
evidence from the component studies and reviews undertaken in the international consensus definition and the 2016 who classification , alongside our own reviews of the current literature , formed the foundation for the present study ; no systematic reviews were carried out . added value of this study we defined and characterised seven robust , reproducible , clinically significant , primary molecular subgroups within childhood medulloblastoma ( in children aged up to 16 years at diagnosis ) , each with distinct clinicomolecular features . 
we propose a cross - validated , subgroup - dependent survival model that incorporates these novel subgroups , alongside established disease features and risk - factors and outperforms the disease risk - stratification schemes in current clinical use . 
redistribution of disease risk using this scheme identifies substantial proportions of favourable - risk non - infant patients ( > 90% 5 - year survival in 11% of patients ) outside the mbwnt subgroup ( equivalent to approximately 70 patients per year in the european union [ eu ] ) who would be suitable for consideration of reduced intensity of therapy , and very - high - risk non - infant patients ( < 40% survival , 13% of patients , about 80 eu patients per year ) for whom new treatment strategies should be prioritised . implications of all the available evidence these data provide a step - change in our understanding and characterisation of molecular subgroups within medulloblastoma , with potential application to future disease subclassification , risk - stratification , and subgroup - dependent translational research . integral subgrouping the 2016 who medulloblastoma classification , 13 and is used to direct treatment strategies aimed at improving cure rates ( 5 - year survival across all four subgroups is 6570% ) , and reducing long - term intellectual and neuroendocrine impairments associated with existing multimodality therapies . 
 clinically methods study design and participants in this retrospective cohort study , we assessed 428 centrally reviewed , clinically annotated primary medulloblastomas from patients aged 016 years at diagnosis , collected from uk childrens cancer and leukaemia group ( cclg ) treatment centres ( uk ; 366 [ 86% ] ) , collaborating european institutions in budapest ( hungary ; 20 [ 5% ] ) and warsaw ( poland ; 15 [ 4% ] ) , and samples from the european ukccsg - siop - pnet3 clinical trial ( 27 [ 6% ] )  . 
108 ( 26% ) of 408 patient samples used were collected in 201014 , 192 ( 47% ) in 200010 , 85 ( 21% ) in 19902000 , and the remaining 23 ( 6% ) were collected before 1990 ( 18 were from the 1980s , four from the 1970s , and one was from 1968 )  . 
tumour investigations were done with vol 18 july 2017 articles see online for appendix approval from newcastle north tyneside research ethics committee ( study reference 07 / q0905 / 71 ) ; all tumour material was collected in accordance with this approval . 
18 post - mortem cerebellar samples were collected from the newcastle brain tissue resource and used as controls in some analyses ; all samples were collected with written , informed consent . procedures we tested medulloblastoma samples with the illumina humanmethylation450k dna methylation array ( illumina , san diego , ca , usa )  . 
the gene expression omnibus accession number for 450k dna methylation array profiles we used for the determination of human medulloblastoma molecular subgroup status is gse93646 . to identify methylation - dependent subgroups , we did unsupervised class discovery by nmf - metagene and k - means clustering , testing all combinations of 310 metagenes and clusters for reproducibility using bootstrapped resampling methods ( 250 iterations ) as described previously.7 this analysis identified metagenes ( a single score that reflects the methylation status of several cpg loci ) representing the main biological effects present in the genome - wide dataset . 
we assessed cluster stability using the cophenetic index , a shorthand measure of the robustness of sample clustering as determined by consensus non - negative matrix factorisation ( appendix p 3 )  . 
we visualised clusters with t - sne.22 we assigned samples classified with less than 80% confidence ( by ( nc ; resampling procedures ) appendix pp 23 )  . as non - classifiable we projected metagenes derived from our discovery cohort onto the validation cohort . 
additionally , we combined the discovery and validation cohorts to do equivalent consensus clustering . we assessed established medulloblastoma clinical , pathological , and molecular features as described previously.7 briefly , we defined histopathological variants according to the who 2016 guidelines.13 we assigned metastatic status ( m + ) based on changs criteria ( appendix p 3 )  . 
tumours were designated as r + if their residuum after surgical excision exceeded 15 c pathology was centrally reviewed by three experienced neuropathologists for 380 ( 89% ) of 428 samples , and clinical data were collated from contributing centres and reviewed centrally ( appendix p 3 )  . 
we identified gfi1 mutations from rna - seq data ( appendix p 4 )  . mbshh mutation data were obtained from a previous study.26 although 450k methylation data for mbshh subgroup assignment were not available for this sample cohort , the tightly defined age cutoff that we defined between the molecularly determined mbshh - infant and mbshh - child subgroups enabled us to infer subgroups for this sequencing cohort ( appendix p 4 ) .26 we tested recurrent mbshh mutations ( tp53 , sufu , ptch1 , smo , and tert ) and gene amplifications ( mycn and gli2 ) identified by whole genome sequencing , for association with the age - defined mbshh - child or mbshh - infant subgroups using fishers exact test ( appendix p 4 )  . statistical analysis we did survival analyses ( overall survival and progressionfree survival ) on samples from patients aged 316 years within our discovery cohort , who received maximal surgical resection and craniospinal irradiation with curative intent . 
overall survival was defined as the time from date of surgery to death or date of last follow - up and progression - free survival as the time from date of surgery to first event ( progression or relapse ) or date of last follow - up . 
patients with follow - up time that exceeded 10 years were right - censored at 10 years . ( n = 55 ) , the tightly defined age cutoff between the molecularly determined mbshh - infant and mbshh - child subgroups enabled us to assess an expanded survival cohort of mbshh - child including additional samples with disease insufficient dna for methylation array analysis , classified as mbshh - child on the basis of their age ( appendix p 4 )  . 
in this group , we assessed the prognostic potential of currently used clinical and molecular risk markers ( m + disease , r + disease , lca pathology , sex , mycn amplification , tert mutation , and tp53 mutation [ appendix pp 45 ] )  . 
as a consequence , we report only overall survival in this group . in this group of patients we created univariate and cross - validated multivariate cox models based on subgroups , established risk factors , and cytogenetic changes . 
prognostic markers in the multivariate analysis were identified by performing 100 rounds of 10 - fold cross - validation , evaluating the performance of markers by measuring area under the curve ( auc ) at 5 years for progression - free survival in the left out fold , and calculating the overall mean auc over all rounds ( appendix p 5 )  . 
 960 vol 18 july 2017 articles consensus , 1 whereas the second ( six metagenes , seven clusters ) revealed further clusters within the established subgroups ( figure 1a , appendix pp 1011 )  . discovery cohort ( n = 428 ) validation cohort ( n = 276 ) mbshh - child survival cohort ( n = 55 ) mbgrp3 / 4 survival cohort ( n = 175 ) 174 ( 63% ) 102 ( 37% ) 17 : 1 32 ( 58% ) 23 ( 42% ) 14 : 1 124 ( 71% ) 51 ( 29% ) 24 : 1 median ( range ) 634 ( 0241597 ) 750 ( 00180 ) 1086 ( 351554 ) 733 ( 341597 ) 30 ( 11% ) 244 ( 89% ) 55 ( 100% ) 175 ( 100% ) changes , mbgrp3 membership , because mbgrp3 and mbgrp4 shared a metagene ( v1 ) , which defined a low - risk outcome and implied shared biology , we considered mbgrp3 / 4 as a single entity , and mbgrp3 and mbgrp4 separately for creation of survival models . 
ixdition to currently understood clinical and molecular risk markers in these groups ( m + disease , r + disease , lca pathology , gender , myc / mycn amplification , and i17q [ isochromosome 17q ] ) , we additionally tested for recurrent cytogenetic and membership of the high - risk methylomic group composed of members from both mbgrp3 and mbgrp4 , defined by metagene v1 ( appendix pp 56 )  . 
we categorised identified independent prognostic markers into risk - stratification schemes ( favourable - risk , > 90% survival ; standard - risk , > 7590% survival ; high - risk , 4075% survival ; very highrisk , < 40% survival ) and survival - dependent roc analysis of progression - free survival at 5 years , to assess performance27 by comparison with previously reported classification schemes ( appendix pp 56 ) .16 , 28 we constructed kaplan - meier curves and compared patient groups with log - rank tests . 
we implemented array processing , normalisation , quality - control checks , and copy - number estimation , relative to a panel of 18 normal cerebella with the r packages minfi29 and conumee ( appendix p 2 )  . the significance threshold was set at p < 005 for all statistical tests in this study , unless otherwise stated . 
the corresponding author had full access to all of the data and had the final responsibility to submit for publication . and molecular results clinicopathological diagnostic characteristics of 428 patients younger than 16 years who had primary childhood medulloblastoma ( discovery cohort ) are shown in table 1 . 
 wnt = wnt / wingless . table 1 : demographics and clinicopathological characteristics of all cohorts loss split into age - dependent mbwnt tumours formed a single subgroup ( n = 33 ) characterised by ctnnb1 mutations , chromosome 6 , and an expected favourable prognosis ( 5 - year overall survival : 93% [ 95% ci 82100 ] ; figure 1b )  . 
 mbshh was subgroups corresponding to infant ( < 43 years ; mbshh - infant ; n = 65 ) and childhood patients ( 43 years ; mbshh - child ; n = 38 ) by the respective absence or presence of metagene v4 . 
both have intermediate prognoses ( 5 - year overall survival mbshh - child : 58% [ 95% ci 4182 ] ; mbshh - infant : 62% [ 5077 ] ; figure 1b )  . 
the subdivision of mbgrp3 and mbgrp4 distinguishes patients with a superior stratification ( 5 - year overall survival auc 0649 [ mbgrp3 / 4 combined with low - risk or high - risk subdivision ] ) compared with the current consensus mbgrp3 and mbgrp4 subgroups ( auc 0610 )  . 
moreover , in the patients aged 316 years at diagnosis and receiving craniospinal irradiation , the high - risk or low - risk subdivision of mbgrp3 / 4 stratifies this group into standard ( mbgrp3 - lr 81% [ 95% ci 60100% ] ; mbgrp4 - lr 81% [ 7193% ] ) and high - risk ( mbgrp3 - hr 35% [ 2355% ] ; mbgrp4 - hr 47% [ 3466% ] ) 5 - year progressionfree survival outcomes , by contrast with the current consensus mbgrp3 / 4 intermediate outcomes ( figure 1c , 1d )  . designations , which show clinicopathological and biological features were nonrandomly distributed in all seven subgroups ( figure 1a , appendix pp 1215 )  . 
patients in the mbshh - infant subgroup had significantly enriched desmoplastic or nodular pathology compared with all other subgroups ( p < 00001 ) , and tp53 mutation ( p < 00001 ) and mycn amplifications ( p < 00001 ) were significantly more frequent in mbshh - child than in all other subgroups . 
patients in the mbgrp3 - hr frequently had lca subgroup significantly more pathology ( p < 00001 ) and myc amplification ( p < 00001 ) , than all other subgroups . 
although patients in the mbgrp3 - hr and mbgrp4 - hr subgroups had similar 10 - year overall survival ( 22% [ 95% ci 1046 ] vs 36% [ 2259 ] ; figure 1b ) , patients in the mbgrp4 - hr subgroup died later of their disease ( ten [ 36% ] of 28 deaths in the mbgrp4 - hr subgroup occurred more than 5 years after diagnosis ) than did those in the mbgrp3 - hr subgroup ( 33 [ 92% ] of 36 deaths occurred within 5 years of diagnosis ; appendix p 26 )  . validation by projection of six metagenes onto an independent cohort8 of 276 patients ( table 1 ) confirmed their existence ( appendix pp 1011 )  . 
moreover , reapplying consensus clustering the combined cohort of 704 patients confirmed a seven subgroup model as optimal , giving 100% concordance to the classifications derived separately from our discovery cohort ( appendix pp 1011 )  . age distributions differed between the two mbshh subgroups ; age distributions are log - normally distributed and intersect at 43 years ( figure 2a )  . 
the two peak incidences of age at diagnosis in infants and in older children for mbshh disease , 26 when observed as a whole , are resolved by their classification into distinct mbshh - infant and mbshh - child subgroups ( appendix pp 1213 )  . 
lca pathology ( p = 000050 ) , mycn amplification ( p < 00001 ) , and mutations of tp53 ( p < 00001 ) and tert ( p = 00015 ) were all significantly enriched in the mbshh - child subgroup compared with the mbshh - infant subgroup ; whereas gender , m + disease status , and r + disease status were not significantly different between groups ( figure 2b ; appendix pp 1213 )  . 
mutational data from an independent mbshh cohort26 showed that sufu mutation was significantly associated with mbshh - infant , whereas ptch1 mutations were observed in both mbshh subgroups ( figure 2c )  . 
residuals from tests indicate where subgroup - enrichment has occurred ( darker shades of grey indicate stronger relationships ) , p values are from tests of enrichment ; scale bar for residuals ( 2 to 2 ) is shown . 
methylation - derived metagene levels ( v1v6 ) , which define subgroup membership , are also shown ( red indicates high metagene levels , blue indicates low levels )  . 
 ( c ) progression - free survival of patients in the consensus four subgroups of medulloblastoma in discovery cohort patients receiving craniospinal irradiation and aged 316 years at diagnosis ( n = 250 )  . 
 ( d ) progression - free survival of patients in the seven identified subgroups of medulloblastoma in patients receiving craniospinal irradiation and aged 316 years at diagnosis ( n = 239 )  . 
discrepancy in the numbers of patients in ( c ) and ( d ) is due to consensus clustering ; certain samples could not be confidently classified for the seven subgroup model or the four subgroup model , and were omitted from the figures . 
r + = residual disease . ( predominantly hypermethylation ) , at both individual cpg loci and at the gene level ( figure 2b ; appendix pp 1213 ) , frequently involving developmental genes ( 79 [ 14% ] of 584 genes with gene ontology term embryonic morphogenesis had aberrant hypermethylation )  . 
residuals from tests indicate where subgroup - enrichment has occurred ( darker shades of grey indicate stronger relationships ) ; scale bar for residuals ( 4 to 4 ) is shown . 
 patients in the mbgrp3 - lr and mbgrp3 - hr subgroups were younger at diagnosis than those in the mbgrp4 - lr and mbgrp4 - hr subgroups ( appendix pp 1415 )  . 
residuals from tests indicate where subgroup - enrichment has occurred ( darker shades of grey indicate stronger relationships ) ; scale bar for residuals ( 6 to 6 ) is shown . 
mbgrp3 - hr tumours were strongly associated with lca pathology ( 20 [ 35% ] of 57 ) and gfi1 mutations ( nine [ 29% ] of 31 ; figure 3a , appendix pp 1415 )  . 
mbgrp3 - hr was characterised by the greatest number of significantly differentially methylated cpgs compared with other subgroups , commonly hypomethylated cpg loci ( figure 3b ; appendix pp 1415 )  . 
notably , the low - risk subgroups were defined primarily by hypermethylation with respect to normal cerebellum , whereas the high - risk univariate ( n = 55 ) cross - validated multivariate ( n = 42 ) hr ( 95% ci ) p value hr ( 95% ci ) p value mycn amplification vs no amplification 447 ( 165121 ) 00032 283 ( 087922 ) 0084 m + vs m disease 569 ( 201160 ) 00011 459 ( 128164 ) 0019 tp53 mutation vs no mutation 347 ( 129930 ) 0014 344 ( 115102 ) 0027 lca pathology vs non - lca pathology 288 ( 115724 ) 0025 tert wild - type vs tert mutation r + vs r disease male vs female 221 ( 078625 ) 013 345 ( 130919 ) 0013 113 ( 045282 ) 079 p values are from cox proportional hazards analyses . 
r = no residual disease ( gross total resection )  . table 2 : identification of prognostic survival markers in mbshh - child cohort univariate ( n = 175 ) cross - validated multivariate ( n = 133 ) hr ( 95% ci ) p value hr ( 95% ci ) p value 175 373 ( 194718 ) < 00001 321 ( 159651 ) 00012 high - risk methylation group vs low - risk methylation group myc amplification vs no amplification 173 294 ( 106813 ) 184 ( 501677 ) < 00001 loss of chromosome 13 vs no loss 158 010 ( 001074 ) 006 ( 001049 ) 00090 mbgrp3 vs mbgrp4 m + vs m disease i17q vs no i17q male vs female mycn amplification vs no amplification 175 204 ( 123340 ) 177 ( 103305 ) 158 171 ( 099295 ) 175 156 ( 086284 ) 173 072 ( 023229 ) lca pathology vs non - lca pathology 108 ( 049239 ) r + vs r disease 122 ( 072209 ) 0038 0024 0006 0039 0056 0144 0576 0848 0464 identification of prognostic survival markers in combined childhood non - mbshh and non - mbwnt survival cohort ( aged 30160 years , receiving craniospinal irradiation , with survival information )  . 
r = no residual disease ( gross total resection )  . table 3 : identification of prognostic survival markers in mbgrp3 and mbgrp4 cohorts subgroups were defined by hypomethylation ( figure 3b ; appendix pp 1415 )  . 
 these distinguishing cytogenetic features were validated in an independent cohort ( appendix pp 1415 )  . survival we did survival analyses in an mbshh - child cohort that included 31 additional shh cases unsuitable for 450k array analysis and classified as mbshh - child on the basis of age ( appendix pp 45 )  . 
tp53 mutation was significantly associated with mycn amplification ( p = 0022 ) and lca pathology ( p = 00033 ) , mycn amplification was associated with lca pathology ( p < 00001 ) , and lca pathology and mycn amplification were never observed with tert mutations ( p = 000079 for lca and p = 00090 for mycn amplification )  . 
there was no significant association between metastatic ( m + ) disease and tp53 mutation ( p = 1 ) , mycn amplification ( p = 0.15 ) , or lca pathology ( p = 067 ) , or an association between subtotally resected ( r + ) disease and tp53 mutation ( p = 1 ) , mycn amplification ( p = 1 ) or lca pathology ( p = 041 )  . 
 univariate survival analysis of clinicobiological features ( including risk features established in disease - wide studies16 ) in this cohort showed significantly shorter progression - free associated with mycn amplification tp53 mutation , lca pathology , m + disease , and r + disease , but no associations with tert mutation status or sex ( table 2 ; appendix pp 1819 )  . 
multivariate cox modelling , showed that mycn amplification , tp53 mutation , and m + disease are independent risk factors for progression - free survival ( table 2 )  . 
the disease - wide risk - stratification scheme currently in use for the hit - siop - pnet5 - mb clinical trial , 16 which deems mycn amplification , lca pathology , m + disease , and r + disease as high - risk factors , outperformed the mbshh - child subgroup stratification in auc this analysis hit - siop - pnet5 - mb stratification scheme as the basis of a combined risk - stratification model for mbshh - child ( appendix pp 1617 ) , classifying patients with any one of these risk factors as very high risk . 
additionally , in multivariate analysis , myc amplification was identified as an independently prognostic high - risk factor , and chromosome 13 loss was associated with an improved outcome ( table 3 )  . 966 vol 18 july 2017 articles a favourable standard high very high time since diagnosis ( years ) false positive mbgrp3 / grp4 mbgrp3 and mbgrp4 cytogenetic current ( pnet5 ) 0678 0656 0639 0538 number at risk ( number censored ) favourable standard high very high 16 ( 0 ) 50 ( 0 ) 82 ( 0 ) 5 ( 0 ) 14 ( 2 ) 34 ( 11 ) 41 ( 19 ) 0 ( 2 ) 10 ( 5 ) 24 ( 18 ) 26 ( 23 ) 7 ( 8 ) 16 ( 26 ) 15 ( 29 ) 6 ( 9 ) 8 ( 34 ) 7 ( 36 ) 2 ( 13 ) 5 ( 37 ) 3 ( 40 ) favourable vs standard ; hr 032 ( 95% ci 004256 ) , p = 026 high vs standard ; hr 348 ( 95% ci 162749 ) , p = 000032 very high vs standard ; hr 577 ( 95% ci 547609 ) , p < 00001 figure 4 : novel risk stratification scheme for mbgrp3 and mbgrp4 medulloblastoma ( a ) progression - free survival plots for identified risk subgroups ( n = 156 ) defined in table 3 and the appendix ( p 20 )  . 
 ( b ) time - dependent roc curves at 5 years are shown for this novel risk stratification alongside a published cytogenetic stratification scheme28 ( mbgrp4 with chromosome 11 loss or chromosome 17 gain , low risk ; mbgrp4 with m disease , standard risk ; mbgrp4 with m + disease , high risk ; mbgrp3 with myc amplification , i17q , or m + disease , high risk ; mbgrp3 without myc amplification , i17q , or m + disease , standard risk ) , and the pnet5 risk stratification ( patients positive for one or more of lca pathology , m + disease , r + disease , myc ( n ) amplification are high risk ; patients absent for all high - risk features , standard risk ) , as well as the stratification derived from considering mbgrp3 and mbgrp4 as separate entities ( appendix p 22 )  . 
roc = receiver operating characteristic . a stratification model was developed that divided mbgrp3 / 4 into different risk groups for 5 - year progressionfree survival : favourable risk ( chromosome 13 loss and no myc amplification ; 16 [ 10% ] of 153 patients ; 92% [ 95% ci 79100 ] ) ; standard risk ( mbgrp4 - lr or mbgrp3 - lr with no myc amplification ; 50 [ 33% ] patients ; 81% [ 7094 ] ) ; high risk ( mbgrp4 - hr or mbgrp3 - hr with no myc amplification ; 82 [ 54% ] patients ; 42% [ 3156 ] ) ; and very high risk ( mbgrp3 with myc amplification ; five [ 3% ] patients ; 0% ; figure 4a ; appendix pp 2021 )  . 
156 patients had information for chromosome 13 loss and myc amplification , of which three were classed as unassignable because they were mbgrp4 with myc amplification ( appendix pp 2021 )  . 
this stratification riskscheme outperformed stratification models ( figure 4b )  . current for comparison , we developed equivalent separate survival stratification schemes for mbgrp3 and mbgrp4 ( appendix pp 2223 )  . 
risk factors identified were broadly consistent with the factors identified in the combined scheme , although the combined scheme was a better predictor of progression - free survival than when mbgrp3 and mbgrp4 were considered separately ( figure 4b )  . 
taking mbgrp4 patients in isolation , in univariate analysis , a designation of mbgrp4 - hr , chromosome 7q status , m + disease , and male sex were associated with poor progression - free survival , whereas mycn amplification , r + disease , and lca pathology were not ( appendix pp 2223 )  . 
a 5 - year variate analysis progression - free survival model incorporating chromosome 7q gain and m + disease defined standard - risk ( 35 [ 32% ] of 110 patients ; 87% [ 95% ci 76100 ] ) and highrisk groups ( 75 [ 68 ] ; 49% [ 3766 ] ) , and outperformed other published models by auc analysis ( appendix pp 2223 )  . taking patients with mbgrp3 isolation , myc amplification was the only risk factor significantly associated with progression - free survival in multivariate analysis , and outcomes were poor for these very high - risk patients ( appendix pp 2223 )  . 
patients in the mbgrp3 with non - myc amplified tumours were at high risk , with progression - free survival similar to that for the mbgrp4 - hr subgroup ( 51 [ 91% ] of 56 patients ; 46% [ 95% ci 3364 ] for mbgrp3 with non - myc amplified tumours vs 41% [ 2860 ] for mbgrp4 - hr )  . 
 * comparisons of cytogenetic , gene expression , and dna methylation changes are made with respect to their counterpart subgroup , except for mbwnt cases , which were compared with normal cerebella if data were available . 
for probe - level comparisons , kyoto encyclopedia of genes and genomes pathway enrichment of demethylated loci was investigated , after correcting for multiple probes mapping to the same gene ( data summarised in appendix pp 2731 )  . 
lca = large - cell anaplastic . gfi1 i17q 16q myc amplication pvt1 , trap1 , nmral1 , cntln ribosome biogenesis genes pi3k - akt signalling pathway vs mbgrp3 - lr , cb galnt9 , mir662 significant seven clinically the clinicopathological and molecular features of the subgroups are new summarised in figure 5 . 
patients are stratified into four clinical risk groups for 5 - year progression - free survival : favourable risk ( comprising mbwnt , mbshh - child with no high - risk features , and non - myc amplified mbgrp3 / grp4 with chromosome 13 loss ; 54 [ 25% ] of 215 patients ; 91% [ 95% ci 82100 ] ) ; standard risk ( comprising non - myc amplified mbgrp3 - lr / grp4 - lr subgroups ; 50 [ 23% ] patients ; 81% [ 7094 ] ) ; high - risk ( comprising non - myc amplified mbgrp3 - hr / grp4 - hr subgroups ; 82 [ 38% ] patients ; 42% [ 3156 ] ) ; and very high - risk ( comprising mbshh - child with high - risk features and myc - amplified mbgrp3 ; 29 [ 13% ] patients ; 28% [ 1456 ] ; figure 6b )  . 
the auc from our proposed childhood medulloblastoma outperforms current and proposed cytogenetic risk stratifications ( figure 6c ) .28 we note that stratification of to create m + disease status is a strong risk factor for poor progression - free survival in mbgrp4 . 
incorporation of m + disease status into mbgrp4 - lr and non - myc amplified mbgrp3 - lr survival modelling does not affect model performance , but potentially allows redistribution of larger favourable standard - risk patients ( 90 [ 41% ] of 218 patients ) and high - risk groups ( 99 [ 45% ] of 218 patients ; figure 6a , c ; appendix pp 2425 ) , which could be considered as an alternative stratification scheme . 
mbgrp3 / 4 : mbgrp3 and mbgrp4 considered as a single entity ; mbgrp3 / 4 plus m + : mbgrp3 and mbgrp4 considered as a single entity with mbgrp4 - lr and non - myc amplified mbgrp3 - lr further stratified by m + disease status ; mbgrp3 and mbgrp4 : mbgrp3 and mbgrp4 stratified separately ; cytogenetic : cytogenetically defined scheme ; 28 pnet5 : scheme employed by hit - siop - pnet5 - mb clinical trial . 
notably , these subgroups were not identifiable in a previously published dataset , which analysis , and are included fewer samples and , specifically , fewer infant patients.8 our seven subgroups reveal a biological overlap between mbgrp3 and mbgrp4 . 
they share a biological signature , defined by a common metagene , indicating a clinicobiological overlap , which might suggest a common origin . these primary subgroups may be further subdivided by the presence or absence of secondary molecular characteristics , many of which , in turn , have subgroupspecific clinical and prognostic significance ( eg , myc vol 18 july 2017 articles in mbgrp3 or tp53 mutation , mycn amplification amplification , lca pathology , m + disease , and r + disease in mbshh - child )  . 
some of these secondary features have been described and assigned clinical significance in previous studies ; in this article , their association with specific novel subgroups ( eg , chromosome 11 loss and chromosome 17 gain in mbgrp4 - lr 28 ) has revealed the underlying biological basis of these subgroup - specific biomarkers . 
moreover , re - evaluation of currently used high - risk factors derived from cohort - wide studies that did not consider subgroup shows that their importance is either low ( eg , lca pathology , m + disease , or r + disease in mbgrp3 ; mycn in mbgrp4 ) or high ( mycn amplification , lca pathology , tp53 mutation , and m + disease in mbshh - child ; myc in mbgrp3 ; m + in mbgrp4 ) when considered in the context of our new subgroups . 
 finally , the biological definition of mbshh - infant ( < 43 years ) is at odds with current clinical definitions of infant disease ( < 3 years ) and this should prompt consideration in the future as to whether infant treatment protocols are appropriate for mbshh - infant patients older than 3 years.16 survival modelling in children younger than 3 years is qualitatively different from analysis in those over 3 years of age , because of the heterogeneity of treatment of infant disease . 
the overall survival at 5 years that we observed in mbshh - infant disease ( 62% , 95% ci 5077 ) is lower than previously reported in an international meta - analysis of the mbshh subgroup in age - defined infants ( < 4 years at diagnosis ; 77% ) , 30 but these patients were not molecularly defined and , as such , are not directly comparable . our survival analysis focused on the 316 - year - old clinical group who received current conventional therapies : surgical resection followed by adjuvant radiotherapy with or without chemotherapy at diagnosis with curative intent . 
combined risk - modelling across all patients in the non - mbwnt or non - mbshh subgroups identified myc amplification , high - risk methylation subgroup membership , and loss of chromosome 13 as independent risk factors . 
survival models incorporating these factors outperformed the clinical risk - stratification used in current clinical trials ( hit - siop - pnet5 - mb16 ) and stratification schemes.28 subgroup - dependent cytogenetic we have defined a risk - stratification of childhood medulloblastoma that allows patients to be assigned into four overarching risk groups . 
very high - risk patients , typically refractory to conventional therapies ( eg , amplified mycn , mutated tp53 , lca pathology , and m + disease in mbshh and amplified myc in mbgrp3 ) should be prioritised for alternative upfront treatment strategies . 
the priority for high - risk patients , comprising the novel mbgrp4 - hr and patients with non - amplified myc in the mbgrp3 - hr subgroup , and a standard - risk group , comprising all other patients , should be optimisation of current therapies and the application of novel , biologically targeted agents . cohorts , who retrospective patient treatments . 
notwithstanding we note the limitations of developing survival models received heterogeneous that models were developed using patients aged 316 years , who all received maximal surgical resection and craniospinal irradiation with curative intent , caution should be applied to their clinical implementation . 
a small number of samples ( < 5 samples ) from this study were used to assist with four - subgroup classification the creation of consensus.5 similarly , our own publication that described four methylation - dependent subgroups of medulloblastoma7 contained 87 samples that overlapped with this study , although the previously published study contained fewer samples ( discovery cohort size of 100 and validation cohort size of 130 patients ) and dna methylation profiling was at much lower resolution ( 1505 vs > 400 000 cpg loci )  . the the existence of novel primary medulloblastoma subgroups , coupled with the characterisation of secondary prognostic features within each group , represents a significant advance in our understanding of medulloblastoma biology and its application in clinical management and future trials design . 
we provide clear evidence of the shared biology between mbgrp3 and mbgrp4 , which affects clinical behaviour and has significant implications for understanding disease biology , developmental origins , and experimental modelling . 
 these investigations constitute a blueprint for a new consensus in medulloblastoma molecular subclassification with important implications for future molecular diagnostics and clinical management . contributors ecs , dw , sb , and scc designed the study and wrote the manuscript . 
all authors contributed to and approved the final manuscript . declaration of interests we declare no competing interests . 970 vol 18 july 2017 articles acknowledgments this study was funded by cancer research uk ( c8464 / a13457 ) , the tom grahame trust , star for harris , action medical research , sparks , the jgw patterson foundation , and the instinct network ( co - funded by the brain tumour charity , great ormond street childrens charity , and children with cancer uk )  . 
tsj is supported by the national institute for health research and a great ormond street hospital ucl biomedical research centre award . corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 corrections correction to lancet oncol 2014 ; 15 : 38 , 43 , 44 correction to lancet oncol 2014 ; 15 : 11422 gatta g , botta l , rossi s , et al . 
lancet oncol 2014 ; 15 : 11422the last sentence of the findings in the summary should have read : the most common grade 3 or 4 adverse events were fatigue ( 97 [ 14% ] of 697 patients allocated zoledronic acid vs 98 [ 14% ] of 704 allocated ibandronic acid ) , increased bone pain ( 91 [ 13% ] vs 85 [ 12% ] ) , joint should receptor pain ( 41 [ 6% ] vs 38 [ 5% ] ) , infection ( 31 [ 5% ] vs 23 [ 3% ] ) , and nausea or vomiting ( 38 [ 5% ] vs 41 [ 6% ] )  . 
in the per - protocol population in table 1 , in the ibandronic acid group , the number of men should read 11 ( 2% ) , the number of patients the with unknown read status 55 ( 8% ) , the number of patients with unknown pr status should read 283 ( 43% ) , and the number of patients with unknown her2 status should read 212 ( 32% ) ; in the zoledronic acid group , the number of patients with unknown pr status should read 277 ( 41% ) and the number with unknown her2 receptor ( 32% )  . 
 status should read 217 ibandronic acid group ( n = 704 ) zoledronic acid group ( n = 697 ) grade 12 grade 3 grade 4 grade 5 total ( % ) grade 12 grade 3 grade 4 grade 5 total ( % ) any adverse event 674 ( 96% ) 667 ( 96% ) 10% frequency in either group abdominal pain altered taste anaemia anorexia breathlessness constipation diarrhoea dry mouth dyspepsia fatigue fever or in uenzalike symptoms headache hypocalcaemia hypomagnesaemia hypophosphatemia infection joint pain muscle pain oedema other pain nausea or vomiting pins and needles renal impairment increased bone pain other adverse events of interest osteonecrosis of the 199 ( 28% ) 177 ( 25% ) 221 ( 31% ) 177 ( 25% ) 246 ( 35% ) 103 ( 15% ) 121 ( 17% ) 222 ( 32% ) 266 ( 38% ) 248 ( 35% ) 544 ( 77% ) 158 ( 22% ) 80 ( 11% ) 83 ( 12% ) 80 ( 11% ) 435 ( 62% ) 125 ( 18% ) 390 ( 55% ) 301 ( 43% ) 410 ( 58% ) 170 ( 24% ) 170 ( 24% ) 215 ( 31% ) 172 ( 24% ) 5 ( < 1% ) 176 ( 25% ) 236 ( 34% ) 208 ( 30% ) 254 ( 36% ) 104 ( 15% ) 140 ( 20% ) 207 ( 30% ) 265 ( 38% ) 176 ( 25% ) 551 ( 79% ) 280 ( 40% ) 222 ( 32% ) 77 ( 11% ) 80 ( 11% ) 72 ( 10% ) 428 ( 61% ) 136 ( 20% ) 398 ( 57% ) 303 ( 43% ) 417 ( 60% ) 156 ( 22% ) 171 ( 25% ) 202 ( 29% ) 226 ( 32% ) 9 ( 1% ) data are number of patients experiencing the event ( highest grade reported )  . 
toxic e ects include serious adverse events . table 2 : toxic e ects in randomised patients vol 15 february 2014 corrections correction to lancet oncol 2013 ; 14 : 678 montemurro f , aglietta m . 
lancet oncol 2013 ; 14 : 67879 in this comment , the fth sentence of the fourth paragraph should read where speci cally analysed , rates of pathological complete her2 - positive and hormone - receptorpositive tumours were lower than those for their hormone - receptor - negative counterparts.5 , 8 this correction has been made to the online version as of july 26 , 2013 . response vol 14 august 2013 e342 editorial for the swedish twitter study see bmj open 2013 ; 3 : e002988 for practical guidance for social media use in oncology see j oncol pract 2012 ; 8 : e11424 #trial : clinical research in the age of social media research programmes , data analysis , and conduct of clinical trials have traditionally been the preserve of clinicians and researchers . 
for example , crowdsourcing cancer research : the role of quantitative challenges was a recent topic at the american association for cancer research annual meeting in san diego on april 7 , 2014 . 
indeed , social media is empowering patients in ways that are changing how clinical research is done , but are these changes bene cial or do they undermine integrity ? in some cases , crowdsourcing is being used by researchers to actively solicit patients involvement and input into trials . 
social media can also aid trial enrolment via the action of patient support groupseg , patients of one particular disease - speci c support group on a social network site independently contacted researchers asking for more information about their rare disease . 
 unlike traditional recruitment , the site is not speci cally linked to any particular trial ; instead , it aims to provide the option of trial enrolment for any patient . 
 social networking provides another important function for patients : it gives them with a valuable support network through which they can compare their experiences and ask questions in a safe , accessible , and anonymous environment . 
third , when patients use the same social media outlets to compare information about their experiences , such fora pose a real danger to the integrity of a clinical trial . 
the exchange of personal experiences whilst enrolled in clinical trials can lead to patientsor any researchers on the same social networkto inadvertently unblind themselves , leading to knowledge of treatment allocation . 
an analysis of twitter use by swedish physicians and medical students showed that roughly 2% of tweets were unprofessional , with a small , but important , minority revealing information that could violate patient privacy . 
other clinician - led social media ventures eg , the creation of facebook pages for clinical trials raises further questions about the ownership of data and the importance of tightly restricting access to something that is ultimately hosted in a public doma furthermore , peer - to - peer conversations on social platforms might be read and misinterpreted by patients and other non - experts . 
 enrolment into a clinical trial is the best treatment option if social for patients with cancer , and networking and media can ease this process , its use should be encouraged . 
patients use of social media should be taken into account when designing trials ; patients need education about the use of social media in tandem with protocol - speci ed restrictions on the risks of sharing certain pieces of information . 
clinicians should welcome the bene ts that social media can bring in attracting more patients to trials , but should also be aware of their own use of social media . 
 the lancet oncology vol 15 may 2014 published online august 3 , 2017 s1470 - 2045 ( 17 ) 30589 - 2 see articles page 1159 selective internal radiotherapy in advanced colorectal cancer : only for right - sided tumours ? colorectal cancer is a biologically unique tumour entity ; in 3040% of patients , metastases are confined exclusively to the liver , lung , or both , with or without minor additional lymph node involvement . 
different from all other tumour types , r0 - resection of these lesions is not always followed by systemic relapse in other regions , therefore this local approach isdespite systemic spread of the diseaseleads to a potentially curative resection in up to 61% of patients.1 , 2 therefore , locoregional treatment of metastases is of key importance . ( transarterial chemoembolisation if surgery alone is not appropriate , other locoregional modalities can be given , 3 such as hepatic arterial infusion of floxuridine , mitomycin , and oxaliplatin ; addition of starch microspheres or application of drug - coated glass beads ( eg , irinotecan beads ) for prolonged arterial drug chemoexposure ; embol ization ; tace ) ; ablation - techniques ( eg , radiofrequency , ultrasound , laser - ablation , heat - ablation , or cryoablation , radio surgery , and brachytherapy [ yttrium - 90 resin microspheres ; selective internal radiotherapy ; sirt ] )  . 
 however , randomised trials testing the individual value of any one treatment are rare ; only radiofrequency ablation with or without surgical resection plus chemotherapy has been prospectively proven effective for superior overall survival versus chemotherapy alone ( phase 3 clocc trial4 )  . 
 beyond this , sirt also showed clinically relevant efficacy on liver metastases in three small randomised in patients refractory to standard systemic trials chemotherapy ; therefore , a broad first - line therapy was justified . 
in the lancet oncology , harpreet wasan and colleagues5 report the results of a combined analysis of three trials of first - line folfox ( leucovorin , fluorouracil , and oxaliplatin ) chemotherapy with or without sirt . 
eligibility criteria used in the three trials were more or less comparable , including patients with unresectable , but limited , liver metastases , with or without lung metastases , and with or without lymph node metastases.6 as expected , the local effect of sirt is clear , with an improved proportion of patients achieving an overall response and liver - only progression . 
however , this locoregional effect did not translate into improved overall progression - free survival or overall survival , even in those patients with metastases restricted to the liver investigation ( one third of the patients )  . 
 why does this proven effective locoregional approach not alter the overall course of disease , even in liver - only disease ? several potential contributing factors that caused imbalance between the groups might have been involved , including different eligibility criteria in each of the three trials , different oxaliplatin dose between treatment groups ( 29% less in the folfox plus sirt group in cycles 13 than in the folfox alone group ) , lower dose of bevacizumab starting 23 months later in the folfox plus sirt group , fewer patients who had bevacizumab in the folfox plus sirt group compared with the folfox alone group ( 197 [ 36% ] vs 256 [ 47% ] ) , less salvage treatment in the folfox plus sirt group , and heterogeneity of the sirt dose between patients , centres , and treatment times . 
more relevant factors might be the fact 47 ( 8% ) of 554 patients randomly assigned to sirt did not receive sirt , that 41 ( 7% ) patients only had unilobar application , and 18 ( 3% ) patients crossed over from folfox alone to folfox plus sirt . 
however , even if those patients are eliminated from the analysis , the overall outcome would not change substantially . another relevant factor might be the short overall survival of patients in all three trials , which was shorter than that of other trials with comparable patient populations but that included treatment with one or two targeted drugs ( bevacizumab and egfr inhibitors ) .7 in the foxfire trials , egfr inhibitors were not used and vegf inhibitors were used in only one third of patients . 
this difference is mainly due to the enrolment and treatment era of the largest trial included in the analysis , sirflox ( 200613 ) and also the fact that patients were treated in countries without routine access to the targeted drugs . 
however , if systemic treatment is weak as in this case , shouldnt sirt have a bigger effect on overall survival ? this is obviously not the case , because , beyond the local treatment only , complete metastases resection after optimal and highly active chemotherapy can improve the long term outcome.4 1138 vol 18 september 2017 comment furthermore , although the local sirt approach improved frequency of resection , it only marginally increased the depth of response , the most important prerequisite for complete secondary resection . 
therefore , the frequency of secondary resection of liver ( and lung ) metastases was not sufficiently increased to improve survival . however , in an important subgroup analysis , 8 sirt was shown to significantly improve overall survival ( p = 0007 ) and progression - free survival ( p = 0053 ) in one third of patients with right - sided primary tumours , known to be much less sensitive to all types of systemic treatment versus left sided tumours , but had no effect in patients with left - sided primary tumours.sirt , which is not affected by chemoresistance in the same way , appears to overcome the intrinsic chemoresistance of liver metastases of right - sided primary tumours . 
this is an important message from wasan and colleagues study , the hr for overall survival in patients with right - sided tumours was 067 ( 048092 ) versus nonsignificant for left - sided tumours , which could have an impact on further clinical research , to improve the poor outcome of patients who have right - sided tumours . 
first - line selective internal radiotherapy plus chemotherapy versus chemotherapy alone in patients with liver metastases from colorectal cancer ( foxfire , sirflox , and foxfire - global ) : a combined analysis of three multicentre , randomised , phase 3 trials . 
protocol for combined analysis of foxfire , sirflox , and foxfire - global randomized phase iii trials of chemotherapy + / selective internal radiation therapy as first - line treatment for patients with metastatic colorectal cancer . 
phosphorylated trifluridine concentration and tumour growth inhibition are increased with the combination of tas - 102 and bevacizumab compared with either drug alone.4 the available clinical data5 suggest that the real benefit of tas - 102 monotherapy is small , therefore strategies to extend this benefit are urgently needed . 
 authors planned to enrol 25 patients , with at least 21 patients needed to have 80% power to reject the null hypothesis of 25% of patients free of progression at 16 weeks by central review . 
this design highlights two points of strength of this study : first , in this setting , 25% progression - free survival after four cycles is clinically relevant ; and second , independent review of response , which is uncommon in phase 2 studies , grants reliability to the results . 
the original hypothesis required at least nine ( 43% ) of the 21 patients included in the primary efficacy analysis to be free of progression at 16 weeksindeed , exactly nine patients achieved such a result . 
from a methodological perspective , this result shifts the attention to the level of the study , published online july 28 , 2017 s1470 - 2045 ( 17 ) 30574 - 0 see articles page 1172 vol 18 september 2017 1139 comment articles preferences for cancer investigation : a vignette - based study of primary - care attendees jonathan banks , sandra hollinghurst , lin bigwood , tim j peters , fiona m walter , willie hamilton lancet oncol 2014 ; 15 : 23240 published online january 14 , 2014 s1470 - 2045 ( 13 ) 70588 - 6 see comment page 136 copyright banks et al . 
we investigated preferences for diagnostic testing for colorectal , lung , and pancreatic cancers in primary - care attendees . methods in a vignette - based study , researchers recruited individuals aged at least 40 years attending 26 general practices in three areas of england between dec 6 , 2011 , and aug 1 , 2012 . 
the vignettes outlined a set of symptoms , the risk that these symptoms might indicate cancer ( 1% , 2% , 5% , or 10% ) , the relevant testing process , probable treatment , possible alternative diagnoses , and prognosis if cancer were identi ed . 
we recorded no strong evidence that participants were more likely to opt for investigation with a 1% increase in risk of cancer ( odds ratio [ or ] 102 , 95% ci 099106 ; p = 0189 ) , although the association between risk and opting for investigation was strong when colorectal cancer was analysed alone ( 108 , 103113 ; p = 00001 )  . 
in multivariable analysis , age had an e ect in all three cancer models : participants aged 6069 years were signi cantly more likely to opt for investigation than were those aged 4059 years , and those aged 70 years or older were less likely . 
other variables associated with increased likelihood of opting for investigation were shorter travel times to testing centre ( colorectal and lung cancers ) , a family history of cancer ( colorectal and lung cancers ) , and higher household income ( colorectal and pancreatic cancers )  . interpretation participants in our sample expressed a clear preference for diagnostic testing at all risk levels , and individuals want to be tested at risk levels well below those stipulated by uk guidelines . 
the public engagement with our study should encourage general practitioners to involve patients in referral decision making . funding the national institute for health research programme grants for applied research programme . introduction more than one in three people in the uk will develop cancer during their lifetime.1 although cancer mortality in the uk has improved in the past 15 years , 2 it is still worse than the average across europe.3 several initiatives have been introduced in the uk to address this issue , such as the cancer reform strategy and the national awareness and early diagnosis initiative.4 earlier diagnosis is thought to be one of the main ways to improve survival , mainly by improved selection of patients for further investigation.5 almost 90% of patients with cancer are diagnosed after experiencing symptoms , most of whom present to primary - care facilities.6 selection of patients for further is not straightforward : overinvestigation has clinical and nancial costs , and underinvestigation risks a delay in diagnosis and therefore has clinical and medicolegal costs . 
however , other groups have a legitimate interest in this decision : providers of cancer investigation diagnostic services , govern ments , taxpayers , insurers , andmost import antlypatients . most common symptoms of cancer can also represent benign disease . 
when deciding whether to investigate for possible cancer , general practitioners use their experience and national guidelines , especially the uk national institute for health and care excellence ( nice ) guidance that was issued in 2005.7 this guidance also underpins the provision of 2 - week - wait clinics , in which patients are guaranteed to be seen within 2 weeks . 
by implication , when investigation is recommended by the guidance , the likelihood of the patient having cancer is high enough to justify it , although no explicit risk threshold warranting investigation for cancer has been reported in the uk or any other national guidance.8 the percentage of patients referred to 2 - week - wait clinics who are subsequently shown to have cancer varies between cancer sites , geographical areas , and general practitioners.9 however , 232 vol 15 february 2014 articles only a quarter of cancers in the uk are diagnosed in 2 - week - wait clinics , with other patients presenting as emergencies or referred to other specialist services.10 , 11 research in primary care has provided estimates of the risk of cancer for many symptoms , with several symptoms recommended by nice as indicating a high likelihood of cancer : few of the nice recommendations equate to risks of less than 5%.12 , 13 investigation , 16 or nice referral guidance strongly recommends that the patient participate in decisions about testing , 7 although little research has been done into diagnostic preferences of patients . 
previous research has focused on treatment or follow - up options , 14 preferences for screening , 15 predictive the sharing of risk information.17 patients certainly fear cancermore so than they do knife crime , alzheimers disease , and job loss18but how likely they are to choose investigation for cancer when provided with the relevant information about cancer risk , the details of investigation , and possible outcomes is unknown . 
we aimed to establish the likelihood that individuals would choose to be tested for cancer at various levels of risk . methods study design and participants in a vignette - based study , we recruited 26 general practices in three areas of england ( bristol and south gloucestershire , devon , and the east of england ) to include a broad range of urban and rural locations and varying levels of socioeconomic status ( number of practices and speci c practices not prespeci ed )  . 
we compared mean practice size and index of multiple deprivation score with overall means from the national public health observatory , and ethnic origin of patients with 2009 means from the o ce of national statistics . in these general practices , researchers recruited attendees aged at least 40 years in waiting areas at di erent times of the day and week between dec 6 , 2011 , and aug 1 , 2012 . 
we did a testretest exercise in one additional practice , with 48 volunteers ( of a recruitment target of 50 ; same inclusion criteria ) who agreed to return 2 weeks later , to complete identical vignettes to their rst exercise . 
these participants were o ered 10 shopping vouchers . we obtained ethics approval from the south west ( southmead ) national research ethics service committee ( ref 11 / sw / 0055 )  . 
participants provided oral informed consent . procedures we chose to compare colorectal , lung , and pancreatic cancers , because they di er in terms of symptoms , type of test , treatment , and prognosis . 
we developed 12 separate vignettes ( ie , descriptions of hypothetical situations ) , with four for each of the three cancers ( table 1 full shows description of vignettes )  . 
the content of the vignettes symptoms extracts ; appendix shows was informed by nice guidelines , qualitative interviews with patients referred for diagnostic tests for the three cancers , 19 and clinical experience.2022 each vignette contained a description of symptoms , the risk that these symptoms might indicate cancer ( both numerically and pictorially ) , information about the relevant diagnostic test , probable treatment , possible alternative diagnoses , and an indication of the prognosis if cancer were identi ed . 
the vignette culminated in a brief summary of information and asked the respondent whether they would choose diagnostic testing at that point , or would not want to be tested ( the exact wording being yesi would choose to be tested or noi would not want to be tested now )  . 
after this choice , participants were asked for the main reason for their decision with a list of options that were informed by qualitative interviews , 19 questionnaires previously used in cancer research , 23 and the cognitive interviewing phase . we re ned the vignettes in two rounds of cognitive the verbal probing method24 interviewing using with 18 members of patient groups from three general practices . 
we recorded responses systematically and collated the after redesign , we tested the questionnaire again on ve additional participants followed by 1 week of piloting in which the questionnaire was administered as per protocol in a general practice waiting room to check recruitment method , functionality of equipment , and data recording . participants could complete up to three vignettes , which were delivered on an electronic touchscreen tablet computer . 
the software developed for the survey selected the rst vignette randomly from all 12 possibilities , the second ( eight possibilities ) , and the third from the remaining cancer ( four possibilities )  . 
 table 2 : characteristics of participants statistical analysis we estimated that 80% of participants given a 10% risk vignette would opt for investigation , and 60% of those given 1% risk would do so . 
with a two - sided 5% alpha and 90% power , we estimated that we would need 119 participants in each group , or 1428 overall . in addition to descriptive statistics , we used logistic regression for the main question ( ie , whether or not to be tested ) , with opting for investigation as the outcome variable . 
the explanatory variables were cancer site , risk level ( as a continuous variable ) , age group , sex , ethnic origin , income band , education , employment , previous diagnosis of cancer , cancer diagnosis in a family member or close friend , convenience of hospital , and travel time to hospital . 
in this analysis , we used only the rst completed vignette from each participant because data were available for all participants , thus avoiding possible di erential selection bias for subsequent vignettes . we then developed separate models for each cancer , using all ( rst , second , or third ) responses for that cancer . 
 because participants who completed more than one vignette always had a di erent cancer for the later vignettes , concerns about selection bias in the analysis of each cancer separately were eliminated . 
initially , we entered every possible explanatory variable into univariable analysis to establish the strength of the association between it and opting for investigation , and those with a p value of less than 02 were retained for multivariable analysis . 
the rst multivariable model contained only variables with a univariable p value of less than 005 ; we then added the other variables sequentially , repeating the process until only variables with p values of less than 005 after adjustment for all other variables in the model were present . a supplementary analysis used k - fold cross validation with risk level as the only predictor variable in the base model and four other explanatory variables as additional predictors . 
we also considered the e ect of missing data on the regression models by omitting any variable with more than 5% of missing data and examining the change in results . 
our nal validation check was to use intracluster correlation coe cients to investigate the degree of clustering of the outcome variable across the 26 practices and the six researchers involved in data collection . 
we did the testretest analysis on the rst vignettes and used percentage comparisons for participant characteristics and statistics for the vignette components . role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all data in the study and had nal responsibility for the decision to submit for publication . 234 vol 15 february 2014 articles colorectal cancer lung cancer pancreatic cancer all three cancers ( rst vignette only ) responses responses responses responses choose to be tested 462 ( 81% ) 485 ( 85% ) 496 ( 86% ) 508 ( 89% ) choose to be tested 533 ( 92% ) 531 ( 93% ) 543 ( 92% ) 537 ( 92% ) choose to be tested 525 ( 90% ) 527 ( 91% ) 526 ( 92% ) 529 ( 91% ) choose to be tested 782 ( 87% ) 738 ( 88% ) 764 ( 88% ) 768 ( 89% ) 1951 ( 85% ) 2323 2144 ( 92% ) 2316 2107 ( 91% ) 3469 3052 ( 88% ) 2291 table 3 : number of participants who would choose to be investigated , by cancer and risk level travel time to hospital ( h ) 00004 00032 risk age ( years ) 4059 * 6069 < 05 * 051 yes * household income < 10 000 * 10 00025 000 > 25 000 family member or close friend previously diagnosed with cancer colorectal cancer or ( 95% ci ) 108 ( 103113 ) 129 ( 092182 ) 081 ( 059111 ) 078 ( 059103 ) 039 ( 022068 ) 131 ( 095181 ) 185 ( 126271 ) p value 00001 00347 or = odds ratio . 
1415 individuals declined to participate . the age and sex pro les of our sample ( table 2 ) were similar to that of the consulting population in england.27 however , the proportion of men aged 4059 years in our study population ( 589 [ 17% ] ) was lower than in the overall population of england ( 27% ) and the proportion of women aged 6069 years ( 526 [ 15% ] ) was higher than in the overall population ( 11% ) .28 the proportion of participants aged 70 years or more in our study population ( 28% ; table 2 ) was also higher than in the overall population ( 24% ) .28 the respondents were largely of white british ethnic origin and nearly half were retired ( table 2 )  . 
15% had previously been diagnosed with cancer ( table 2 ) , which is higher than the estimate of 13% for individuals older than 65 years in the uk ( owing to scarce data on this subject , this age group represents the most meaningful comparison available ) .29 for most characteristics , only a small proportion of data was missing ( table 2 )  . overall , 88% of participants opted for investigation in the rst vignette ( table 3 )  . 
the proportion was slightly lower in the lowest risk group and higher in the highest risk group ( table 3 ) , but the di erence was small and could largely be explained by a risk gradient for colorectal cancer ( table 3 )  . 
compared with colorectal cancer , after adjustment for risk , participants were more likely to opt for investigation for lung cancer ( 266 , 95% ci 199356 , p < 00001 ) and pancreatic cancer ( 196 , 148260 , p < 00001 )  . 
however , when the types of cancers were analysed separately , risk did have an e ect on whether investigation was chosen for colorectal cancer ( table 4 )  . age had an e ect in all three cancer models : participants aged 6069 years were more likely to opt for investigation for all three cancers than were those aged 4059 years , and those in the oldest group ( 70 years ) were least likely to opt for investigation ( table 4 )  . 
further investigation into whether attitude to risk was a ected by age showed weak evidence of an e ect overall ( pinteraction = 010 ) , with substantial variation across the di erent cancers . 
other variables associated with increased likelihood of opting for investigation were shorter travel times to testing centre ( colorectal and lung cancers ) , a family member or close friend previously diagnosed with cancer ( colorectal and lung cancers ) , and higher household income ( colorectal and pancreatic cancers ; table 4 )  . identi ed the k - fold cross validation results for all three cancer sites produced nal models including the same variables as those in the original models , with almost identical regression coe cients ( data not shown )  . 
we the variable examined the potential bias of missing data in relation to income by omitting the variable from the two nal models for colorectal and pancreatic cancers in table 4 , with almost identical results for risk level and the other variables ( ie , omission of this variable from the models made no di erence to the models themselves )  . 
we noted negligible intracluster correlation of the preference for investigation by general practice and by researcher who enrolled the individual for all vignettes , and for each cancer site separately ( data not shown )  . the main reasons cited by participants opting for investigation in the rst vignette were peace of mind , early detection , and a family history of cancer , with little variation across the three cancers ( table 6 )  . 
reasons for opting for no investigation varied between the three cancers ( table 6 ) eg , much higher proportions cited an unpleasant test or harmful test for colorectal cancer than for lung and pancreatic cancers . the primary research question of whether the participant chose to undergo diagnostic tests for cancer showed excellent testretest consistency , with a statistic of 0878 ( > 075 is deemed excellent )  . 
participants reasons for their choice produced statistics of 0584 for those who would opt for investigation and 0667 for those who would not opt for investigation , which are both in the fair to good range ( 04075 ) .30 the social and economic status data showed reliable testretest consistency : six of ten questions returned higher than 90% agreement , three were between 80% and 89% , and one ( hospital travel time ) was 69% . discussion to our knowledge , ours is the rst study of public preferences for cancer investigation ( panel )  . 
88% of participants would opt for investigation when given a realistic scenario of symptoms that could indicate cancer , along with the risk of cancer these symptoms posed , plus a description of the relevant investigation and likely outcomes . 
 although this risk gradient was identi ed in the analysis incorporating all three cancers , it was primarily driven by the ndings for colorectal cancer , for which participants seemed to make a trade - o between the invasiveness of the colonoscopy and the risk of cancer . 
age also seemed to a ect responses , with the preference for investigation highest in individuals aged 6069 years and lowest in those aged at least 70 years . the willingness for testing shown in our study far exceeds what is actually being o ered by the national health service . 
participants in our study might have simply opted for a free test , an idea which is supported by the fact that the proportion opting for investigation did not vary by risk for lung and pancreatic cancer . 
however , the di erences by risk level for colorectal cancer and by age group suggest that participants considered their responses . the four vignettes for colorectal cancer were all in line with nice guidance for urgent referral ( because of the 6 weeks of diarrhoea ) , although many symptoms with a low risk of cancer ( 15% ) are not included in nice guidance.12 , 13 for lung cancer , a chest radiograph is recommended by nice when a patient has a persistent cough ( de ned as lasting at least 3 weeks )  . 
only in the case of colorectal cancer , with its invasive method of testing , did we record clear evidence of an association between a preference for testing and risk level , but even at the lowest risks , the proportion who would choose testing was more than 80% . 
our study emphasises how the public and patients should be allowed to contribute directly to the continuing redesign of diagnostic pathways into and out of primary care for cancer in the uk . 
no threshold level of risk warranting urgent investigation of cancer has been published , although the concept of a threshold is implicit in all uk guidanceand must be in excess of 1% . 
as well as giving referral guidance , nice guidelines emphasise the value and importance of including the patient in the decision - making process for referral and diagnostic testing for cancer ; e ective communication is a key dimension of an appropriate referral.33 the way that participants engaged with our study , the subtle variations in participant preferences , and the high participant numbers suggest that general practitioners should be able to con dently engage in a dialogue with patients about the meaning of symptoms and the risk of cancer . 
general practitioners can underestimate the degree to which patients want information and to be involved in decision making , 34 and decisions are sometimes made on the basis of a perception of what patients prefer , 35 but our data and experience show that a substantial proportion of the population are willing to think about what symptoms mean , personal risk , and the possibility of cancer . 
much of the debate around their use centres on the degree to which responses can be used as accurate measures of views and behaviour , with the correlation between vignette response and actual behaviour being questioned.36 conversely , several studieseg , peabody and colleagues investigation37have shown that vignette responses are useful indicators of behaviour and compare favourably with other methods of assessments of preferences and intentions . 
the method has been widely used in the investigation of medical choice and judgment , such as by jiwa and colleagues.38 many participants in our study had not experienced referral for cancer testing and the vignettes provided a way to elicit preferences in the absence of direct experience . any questionnaire survey is only useful if the questions are realistic and the responses considered . 
we tried to ensure the vignettes were as realistic as possible and to make the percentage risk understandable by presenting it numerically and pictorially ( see appendix for example ) , on the basis of suggestions from our two rounds of cognitive interviewing . 
we cannot know whether the overall high proportion of participants who would opt for investigation was driven by the symptom burden ( which worsened with high risk levels ) or by the risk level itself , or by a combination , although the last of these interpretations seems to be closest to clinical reality . 
we were realistic in our description of the three rst - line investigations ( colonoscopy , chest radiograph , and ct scanning ) , including their requirements and possible hazards ( largely relevant to colonoscopy with its need for bowel preparation and the small risk of perforation )  . 
 since our study began , the ndings of the siggar study39 have suggested that ct colonography could be as accurate as colonoscopy ; a higher proportion of participants in our study might have opted for investigation had this test been available . 
we made it clear that early diagnosis might not reduce the chance of death from lung and pancreatic cancers , emphasising that most patients would die of their disease , although prompt diagnosis could allow bene t from palliative care . 
we would also point to the reasons given for responses , which suggested that participants responded re ectively ; the subtle variations around the type of test , risk , and the age of respondents showed an engagement with the di ering components of the vignette . that ours was a large study , in which participants were recruited from urban , rural , wealthy , and deprived locations . 
although our target population was the general uk population susceptible to cancer ( adults aged 40 years ) , we made a pragmatic decision to recruit from waiting areas of general practices as opposed to other community settings . 
the proportion with a past history of cancer in our sample ( 15% ) is similar to the estimated proportion in the uk population of individuals older than 65 years ( 13% )  . 
 the small number of non - white individuals in our study means that the e ect of any ethnic variation is beyond the scope of this study . nice recommendations and national health service provision seem to di er greatly from preferences of patients in terms of cancer diagnostic pathways . 
if more patients can be drawn into a full dialogue about preference , risk , and decision making with their general practitioner , a more e ective referral pathway from primary care could be created . contributors all authors contributed to study design , study conduct , and study management . 
his contribution to this article is in a personal capacity , and should not be interpreted as representing the view of the guideline development group , or of nice itself . 
the other authors declare that they have no con icts of interest . acknowledgments this report presents independent research funded by the national institute for health research programme grants for applied research programme ( rp - pg - 0608 - 10045 )  . 
the views expressed are those of the authors and not necessarily those of the national health service , the national institute for health research , or the department of health . 
we thank the discovery programme steering committee ( roger jones [ chair ] , clare bankhead , alison clutterbuck , jon emery , ardiana gjini , joanne hartland , maire justice , jenny knowles , helen morris , richard neal , peter rose , greg rubin ) ; catherine stabb and the east of england primary care research network , who recruited participants outside of bristol ; helen morris who coordinated researcher training and project documentation in the east of england ; katie mills and nicky hall who collected qualitative data that informed vignette development ; and bristol software partners who developed the software for the application used to collect data . corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2017 ; 18 : e142 correction to lancet oncol 2017 ; 18 : e81 , e82 , e86 burki tk . 
this correction has been made to the online version as of march 2 , 2017 . published online march 2 , 2017 s1470 - 2045 ( 17 ) 30173 - 0 published online march 2 , 2017 s1470 - 2045 ( 17 ) 30175 - 4 rl , cancer cancer and survivors : childhood adolescent , r , mulder al . 
recommendations kremer skinner for lc , in male gonadotoxicity surveillance young childhood , report adult international late effects from the guideline harmonization group in collaboration with the pancaresurfup consortiu lancet oncol 2017 ; 18 : e7590in this review , the sixth paragraph under the who needs surveillance ? heading should have read there is probably no increased risk after treatment with cyclophosphamide , busulfan or cyclophosphamide or fludarabine and melphalan , hsct conditioning , and ifosfamide , and mechlorethamine , cisplat additionally , the key for figure 2 should have been light orange for moderate recommendation to do and dark orange for weak recommendation do . 
these corrections have been made to the online version as of march 29 , 2017 . procarbazine vol 18 april 2017 e196 corrections corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 preventing prevention : indian politics and public health clash recent move by the largest indian government , in a the countrys independent public health organisation , the public health foundation of india ( phfi ) , has been barred from receiving foreign funding , including donations from the bill & melinda gates foundation . 
the phfi , which helps to support central and local governments by promoting breast cancer awareness campaigns , developing population - based cancer registries , and promoting universal health care , will lose roughly 45% of its funding from foreign investment over concerns regarding alleged lobbying with parliamentarians and media on anti - tobacco messages , and the misuse of funds and bank accounts that were allegedly not disclosed to the home ministry . 
 this suspension is part of a wider move in recent years by the indian government to cancel foreign contribution ( regulation ) act licenses , which regulate the flow of funds from foreign donors , from which some 20 000 indian non - governmental organisations benefit . 
while some have seen these cancellations as part of a wider effort to appease affiliate groups to the government who have accused philanthropic organisations of pushing corporate interests , others believe that the government is trying to promote a wholly nationalistic agenda in a bid to retain power in the 2019 elections . the recent move to cut funds to the phfi comes at a time when public health is a growing concern in india . 
earlier this month , the indian government announced that it will miss its deadline of december 2017 to reduce coal emissions and airborne particulate matter by two - thirds , declaring instead that developed countries should be responsible for tackling global pollution levels . 
although indias per capita emissions are only 159 metric tonnes per year compared with 755 for china and 1639 for the usa , india is still the worlds third - biggest emitter of greenhouse gases in absolute terms , and has notable levels of air pollution , which killed nearly 11 million of its residents in 2015 alone . 
such an open and defiant attitude by the indian government about their failure to meet coal emission targets , and their dismissive attempt to shift the responsibility to other countries , is a careless and harmful attitude to adopt , but an understandable attitude at a time when the us government dismantling its own environmental protection agency and backtracking on former president barack obamas clean power plan . 
by failing to address such chronic causes of illness , the indian government stands to exacerbate the growing pressure the current public health system upon which a large proportion of indias working class and unemployed rely . 
as a result , indias public health - care system has wholly inadequate financial resources to sufficiently train , staff , equip , or sometimes even run , health facilities nationally an infrastructure that is sure to worsen as one of the countrys largest public health organisations loses a substantial portion of their funding from overseas . although aligning public health targets with a political agenda is certainly nothing new , these drastic steps taken by the current government will inevitably affect public health programmes and initiatives . 
cancer is an emerging health problem in india , and already causes 6% of all adult deaths every year , with the number of cancer deaths set to increase to nearly 1 million in 2025 . 
 this means increasing , not reducing , the availability of funds to help to promote public health campaigns that encourage healthy lifestyles , reduce tobacco use , improve cancer registries , and increase the availability of cancer screening . 
it is worrying that at a time when health care in india is most in need , the government has opted to push for a wholly political and nationalistic agenda at the cost of public health , which clearly needs foreign investment to realistically meet the growing burden of non - communicable diseases across the country . 
that the indian government openly makes moves to undermine public health goals is somewhat paradoxical to a vision of india as an emerging social and economic superpower , and will erode the true social and democratic value that improved health holds for the country . 
the primary aim of this study was to establish how cetuximab might be safely and e ectively added to intermittent chemotherapy . methods coin - b was an open - label , multicentre , randomised , exploratory phase 2 trial done at 30 hospitals in the uk and one in cyprus . 
patients in both groups received folfox and weekly cetuximab for 12 weeks , then either had a planned interruption ( those taking intermittent cetuximab ) or planned maintenance by continuing on weekly cetuximab ( continuous cetuximab )  . 
 10 - month failure - free survival was 50% ( lower bound of 95% ci 39 ) in the intermittent group versus 52% ( lower bound of 95% ci 41 ) in the continuous group ; median failure - free survival was 122 months ( 95% ci 88156 ) and 143 months ( 107204 ) , respectively . 
the most common grade 34 adverse events were skin rash ( 21 [ 27% ] of 77 patients vs 20 [ 22% ] of 92 patients ) , neutropenia ( 22 [ 29% ] vs 30 [ 33% ] ) , diarrhoea ( 14 [ 18% ] vs 23 [ 25% ] ) , and lethargy ( 20 [ 26% ] vs 19 [ 21% ] )  . interpretation cetuximab was safely incorporated in two rst - line intermittent chemotherapy strategies . 
maintenance of biological monotherapy , with less cytotoxic chemotherapy within the rst 6 months , in molecularly selected patients is promising and should be validated in phase 3 trials . funding uk medical research council , merck kgaa . 
open access article distributed under the terms of cc by . introduction the discovery of predictive biomarkers for advanced colorectal cancer and the development of new targeted treatments has led to the combination of cytotoxic drugs with targeted treatments as the international standard of care . 
however , these combinations have failed to improve outcomes in several phase 3 trials.14 toxic e ects caused by drug combinations have also confounded assessments of e cacy.2 , 3 intermittent treatment and maintenance biological treatment have been explored in several trials to address this shortcoming.311 palliative treatment of cancer should address both quantity and quality of life . 
 minimising the time spent taking cytotoxic drugs and introducing chemotherapy - free intervals or complete treatment holidays ( ie , planned interruptions ) might help to meet both these goals . 
de - escalation of components of treatment for maintenance in patients vol 15 may 2014 articles for the study protocol see plugins / studydisplay / protocols / coin - b%20combined%20 protocol%20with%20crfs.pdf who have not progressed is increasingly done in practice and a clinical bene t has been shown in a trial of capecitabine and bevacizumab maintenance treatment.8 however , the best strategy to use for di erent clinically or molecularly de ned cohorts has yet to be established . the coin trial1 , 6 was designed to assess whether intermittent chemotherapy was as e ective as continuous chemotherapy and whether the addition of cetuximab to continuous chemotherapy was associated with additional bene t . 
in the coin - b trialdone as an adjunct to coinwe sought to establish how cetuximab might be safely and e ectively added to intermittent chemotherapy . methods study design and participants we did this open - label , multicentre , randomised , exploratory phase 2 trial at 30 hospitals in the uk and one in cyprus . 
eligibility criteria were age 18 years or older , colorectal adenocarcinoma , inoperable metastatic or locoregional measurable disease according to recist ( version 1.1 ) , no previous chemotherapy for metastases , who per formance status 02 , and good organ function ( baseline require ments were : 15 10 neutrophils per l , 100 10 platelets per l , serum bilirubin 125 upper limit of normal , serum aminotransferases 25 upper limit of normal , alkaline phosphatase 5 upper limit of normal , and estimated creatinine clearance or measured glomerular ltration rate 50 ml / min )  . 
 patients were excluded if they had had any previous likely to cancer , uncontrolled medical comorbidity interfere with coin - b treatment or response assessment , or known brain metastases . the trial was designed before kras mutations were identi ed as predictors of resistance to egfr monoclonal antibody treatment.12 coin - b was suspended in may , intermittent chemotherapy and intermittent cetuximab randomisation intermittent chemotherapy and continuous cetuximab cetuximab maintenance cetuximab maintenance folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks figure 1 : trial design treatment cycles continued until progressive disease ( pd ) with maximally tolerated treatment , or patient choice . 
 folfox = folinic acid and oxaliplatin followed by bolus and infused uorouracil . 2008 , and on restarting ( january 2009 ) it included prospective kras mutation analysis before ran domisation . 
coin - b was approved by the south west research ethics committee and the medicines and healthcare regulatory agency in the uk and the national bioethics and the pharmaceutical services of the ministry of health in cyprus . randomisation and masking the mrc clinical trials unit did the randomisation by telephone , using the method of minimisation with a random element . 
rb established the mutational status of braf ( codon 600 ) and nras ( codons 12 , 13 , and 61 ) retrospectively for kras wild - type patients who consented to future bowel cancer research . 
when cetuximab was given in combination with chemotherapy ( day 1 ) , cetuximab was given rst ( see protocol for full details of the treatment regimens )  . patients in both groups received treatment for 12 weeks and those with stable or responding disease started a chemotherapy - free interval ( ie , no folfox )  . 
on recist 632 vol 15 may 2014 119 patients registered before protocol amendment 59 assigned to intermittent cetuximab 60 assigned to continuous cetuximab 282 patients registered after protocol amendment 57 excluded 18 no tumour block or analysis 39 kras mutations failed articles 9 had abnormal laboratory 133 had kras mutation 175 excluded test results 1 scan out of date 1 performance status > 2 1 previous oxaliplatin 1 resectable metastases 1 unusual histology 9 kras analysis failed 7 too ill 2 died 9 withdrew consent 1 chemoradiation within 1 month 62 kras wild - type 25 assigned to intermittent cetuximab 37 assigned to continuous cetuximab 107 kras wild - type 169 eligible and randomly assigned 78 assigned to intermittent cetuximab 91 assigned to continuous cituximab 14 did not complete initial 12 weeks of chemotherapy and cetuximab 25 did not complete initial 12 weeks of chemotherapy and cetuximab 64 included in primary analysis 66 included in primary analysis 20 did not restart trial study treatment after rst chemotherapy - free interval 9 early progression or death 4 patient or doctor choice 3 complete response or liver surgery 2 toxic eects 1 intercurrent illness 1 lost to follow - up and censored 33 did not restart trial study treatment after rst chemotherapy - free interval 5 early progression or death 15 patient or doctor choice 5 complete response or liver surgery 4 toxic eects 2 intercurrent illness 2 lost to follow - up and censored 44 restarted study treatment after rst chemotherapy - free interval 33 restarted study treatment after rst chemotherapy - free interval figure 2 : trial pro le we designed coin - b as two separately powered phase 2 trials , using aherns single - stage design15 to distinguish between a 10 - month failure - free survival of 50% ( implying that the treatment would be worth pursuing in a phase 3 trial , feasibility and toxic e ects permitting ) and of 35% ( implying that the treatment would not be worth pursuing )  . 
serious adverse events and deathstogether with an assessment of causalitywere con tinuously reported ; and were reassessed by an experienced oncologist ( rst by am , then the trial management group ) on behalf of the medical research council . a baseline ct scan was done within 4 weeks before the start of treatment and then at least once every 12 weeks and evaluated with recist criteria . 
data were collected via remote data capture , except for reports of serious adverse events , which were submitted by fax . outcomes the primary outcome was failure - free survival at 10 months . 
secondary objectives were : safety assessment of cetuximab reintroduction , overall survival , progression - free survival , response rates , toxic e ects , disease control at 24 weeks ( complete response , progressive disease , and stable disease ) , and quality of life . time from randomisation ( week 0 ) was used for the analysis of failure - free survival and overall survival . 
at the time of analysis , survivors were censored at the date they were last known to be alive . the primary and main secondary outcomes ( overall survival and progression - free survival in the interval ) were retrospectively analysed for patients who were triple wild - type ( for kras , braf , and nras )  . 
data from phase 2 studies14 suggested that 50% failure - free survival at 10 months would be a suitable primary outcome for the addition of cetuximab . vol 15 may 2014 articles women site of primary tumour right or transverse colon status of primary tumour left colon or rsj rectum resected unresected local recurrence distribution of metastases liver only non - liver liver and elsewhere data missing [ a : ok ? ] number of metastatic sites none three adjuvant chemotherapy 16 months ago > 6 months ago suspension , interim data from coin and coin - b suggested that attrition before 12 weeks was 16% because of toxic e ects or absence of bene t . 
as a result , we changed the target enrolment so that 158 patients with kras wild - type would be included , of whom we expected 136 to be assessable for the primary outcome . we used the kaplan - meier method to assess failurefree survival , overall survival , and progression - free survival . 
we used stata ( version 11.1 ) for all statistical analyses . the trial is registered as an international standard randomised controlled trial , number isrctn38375681 . role of the funding source the mrc was the overall sponsor of the trial . 
the corresponding author had full access to the data and had nal responsibility for the decision to submit for publication . results between july 13 , 2007 , and march 6 , 2010 , 401 patients were registered and 226 patients were enrolled . 
the continuous cetuximab group had more elderly patients ( age > 75 years ) , more with a who performance score of 2 , more with braf mutations , and more with primary colon cancers ( vs rectal ) than did the intermittent cetuximab group ( tables 1 , 2 )  . 24 patients had braf mutations and 15 had nras mutations ( table 2 )  . 
it has not since been validated and our analysis con rms that it is not informative ( data not shown )  . at the time of analysis ( april 24 , 2012 ) , median duration of follow - up in the kras wild - type intention - to - treat population was 328 months ( iqr 229458 ) in the intermittent cetuximab group and 342 months ( iqr 273504 months ) in continuous cetuximab group . seven patients did not start protocol treatment : two in the intermittent cetuximab group and ve in the continuous cetuximab group . 
most patients required a treatment delay , 68 ( 87% ) of 78 patients in the intermittent cetuximab group and 74 ( 81% ) of 91 in the continuous cetuximab group . 
dose modi cations occurred in similar proportions in each group ; for cetuximab , modi cations were made for 57 ( 73% ) of 78 patients taking intermittent cetuximab versus 70 ( 77% ) of 91 taking continuous cetuximab , oxaliplatin was modi ed for 40 ( 51% ) versus 43 ( 47% ) patients , and uorouracil was modi ed for 49 ( 63% ) versus 51 ( 56% )  . 
treatment was discontinued because of drug - related toxic e ects for nine ( 12% ) of 78 patients in the intermittent group versus 11 ( 12% ) of 91 in the continuous group . the primary analysis included 64 patients in the intermittent cetuximab group and 66 in the continuous cetuximab group . 
patients were excluded for progressive disease ( one in the intermittent cetuximab group vs four in the continuous cetuximab group ) , death ( four vs 14 ) , and failure of treatment in the rst 12 weeks ( nine vs seven )  . 
the greater dropout from the continuous cetuximab group could be a result of di erences in baseline characteristics combined with the greater proportion of patients with a braf mutation ( table 1 , appendix )  . 
in the primary analysis population , at least 50% of patients were failure - free at 10 months in both groups : 32 ( 50% ) of 64 in the intermittent cetuximab group and 34 ( 52% ) of 66 in the continuous cetuximab group . 
median failure - free survival was 122 months ( 95% ci 88156 ) in the intermittent cetuximab group and 143 months ( 107204 ) in the continuous cetuximab group ( gure 3a )  . 
in an intentionto - treat analysis ( n = 169 ) , median failure - free survival was 121 months ( 95% ci 78147 ) versus 120 months ( 87145 ; appendix )  . 
median failure - free survival was greater for patients with all wild - type alleles than for those with kras wild - type only in both treatment groups , in both the primary analysis cohort and the intention - to - treat population ( gure 3b ; appendix )  . in the primary analysis cohort , median overall survival was 168 months ( 95% ci 145226 ) in the intermittent cetuximab group versus 222 months ( 184289 ) in the continuous cetuximab group ( gure 4a )  . 
the di erence in median overall survival was smaller in the intentionto - treat population ( 160 months , 95% ci 133204 vs 175 months , 137217 ; appendix )  . 
median overall survival was greater for patients with all wild - type alleles than for those with kras wild - type only in both treatment groups in both the primary analysis cohort and the intention - to - treat population ( gure 4b ; appendix )  . from week in the primary analysis cohort , median progressionfree survival 12 was 31 months ( 95% ci 2847 ) in the intermittent cetuximab group and 58 months ( 4986 ) with continuous cetuximab ( gure 5a )  . 
as with the other survival endpoints , median progression - free survival was greater for patients with all wild - type alleles than for those with kras wild - type , for both treatment groups ( gure 5b )  . 54 ( 32% ) of 78 patients died in the intermittent cetuximab group versus 67 ( 40% ) of 91 in the continuous cetuximab group . 
112 ( 93% ) deaths were caused by colorectal cancer ( 49 vs 63 ) , three ( 2% ) were related to treatment ( one vs two ) , and six ( 5% ) were the result of other causes ( four vs two )  . only 77 patients restarted trial treatment after a intermittent interval , 44 chemotherapy - free cetuximab and 33 taking continuous cetuximab . 
for patients who survived at least 24 weeks , greater disease control ( ie , complete response , partial response , or stable disease ) was noted in those assigned to continuous cetuximab ( n = 29 , 32% ) than in those assigned to intermittent cetuximab the imbalances . ( n = 17 , 22% ) , despite patients with mutations in kras , nras , and braf had a worse prognosis than patients with wild - type for overall survival and failure - free survival in the intention - to - treat population ( p < 00001 for both outcomes ; appendix )  . toxic e ects and adverse events were similar in each treatment group . 
three patients in the intermittent cetuximab group reported grade 3 or higher hyper sensitivity events with only one on reintroduction of cetuximab ( table 3 )  . both the coin and coin - b trials contained a quality - oflife substudy . 
although not statistically compared , maintenance cetuximab with inter mittent chemotherapy seemed to be slightly more active than intermittent cetuximab with intermittent chemotherapy . coin - b is one of a series of trials of patients with noncurable advanced colorectal cancer to explore strategies to improve the combinations and sequences of cytotoxic treatments , planned targeted chemotherapy , newer maintenance , and planned interruptions ; all with a focus on reducing toxic e ects and improving quality of life without reducing survival . 
in some trials , part or all of the rst - line chemotherapy is discontinued in the investigational group and compared with continuation of the full rst - line treatment.4 , 7 , 11 , 16 in others , planned maintenance is compared with a planned interruption5 , 8 , 9 or an additional maintenance treatment is introduced when chemotherapy is discontinued.10 in all these studies , the conventional surrogate endpoint of progression - free survival is inappropriate because it does the subsequent bene t of planned not consider reintroduction of full rst - line treatment on progression . 
 other outcome measures have therefore been used ( duration of disease control and failure - free survival ) .5 however , the best measure of how maintenance treatment a ects the course of disease is progressionfree survival in the interval . the coin trial adds to preliminary data from cr06 and optimox - 1 , 11 , 16 which suggested that interruption or de - escalation of treatment was safe and potentially bene cial . 
the results of adams and colleagues6 could not exclude the possibility of a very small negative e ect on overall survival of a treatment holiday after 3 months of cytotoxic chemotherapy . 
the upper limits of the twosided 80% cis for the hazard ratios ( hrs ) in both the per - protocol and intention - to - treat analyses were greater than the prede ned non - inferiority boundary of 1162 . 
 the hr in the intention - to - treat population ( n = 1630 ) was 1084 ( 80% ci 10081165 ) and in the per - protocol population ( n = 978 ) it was 1087 ( 09861198 ) .6 planned subgroup analyses showed that patients with normal baseline platelet counts could gain the bene ts of intermittent chemotherapy without harming survival . 
 this nding suggests that a planned interruption might not be detrimental to most patients and warrants further study with clinical or molecular predictive markers . coin - b was designed as an exploratory , hypothesisgenerating study to complement coin . 
at randomisation , only infusional uorouracil in com bination with oxaliplatin and cetuximab was allowed , which removed the confounding e ect and possible negative interaction reported in coin and other studies when capecitabine was the partner uoropyrimidine.17 in coin - b , planned maintenance with cetuximab ( ie , continuous cetuximab ) was associated with a greater failure - free survival , greater progression - free survival , greater overall survival , improved disease control at 24 weeks , and a longer chemotherapy - free intermittent cetuximab . 
such an imbalance might be considered a limitation of a small study such as coin - b ; however , the main reason for the imbalance between groups was discovered after the change in the population of interest from all patients with advanced than was interval vol 15 may 2014 articles panel : research in context systematic review at the time of study inception , very few randomised trials had been done of cetuximab and chemotherapy , all of which were reviewed to help power the study , and choose the outcome measures . 
stopping and restarting cetuximab could in theory increase the risk of hypersensitivity , so establishing safety was a main aiwe designed coin - b to complement the coin trial.1 , 6 coin rst tested the non - inferiority of intermittent chemotherapy compared with continuous chemotherapy and second , the addition of cetuximab to continuous chemotherapy for superiority . 
this nding needs to be validated in phase 3 trials , such as the upcoming focus 4 study , 20 in which novel targeted treatments will be assessed in biomarker - enriched populations . colorectal cancer to those who had kras wild - type tumours . 
119 patients were enrolled before the introduction of kras screening , 62 of whom were subsequently found to be kras wild - type and included in the primary outcome analysis . 
this nding is consistent with data for egfr inhibitors as rst - line treatment.18 , 19 other studies comparing planned maintenance interruption have shown treatment with planned evidence of a bene t of maintenance treatment . 
in optimox - 2 , planned maintenance with infusions of uorouracil and leucovorin prolonged disease control compared with a planned interruption although it had no signi cant e ect on overall survival ( 238 months vs 195 months , hr 085 ; p = 042 ) .5 in cairo - 3 , 8 planned maintenance with bevacizumab and capecitabine was compared with a planned interruption , after 4 months of induction treatment with capecitabine , oxaliplatin , and improved probevacizumab . 
planned maintenance gression - free survival in the interval ( 41 months vs 85 months , hr 044 , 95% ci 037054 ; p < 00001 ) and overall survival ( 179 months vs 217 months , hr 077 , 95% ci 062096 ; p = 002 )  . 
median time to progression was 179 weeks ( 95% ci 133234 ) for bevacizumab continuation and 126 weeks ( 120164 ) for no continuation ( hr 072 , 95% ci 056092 )  . 
coin - b is the rst trial to enrol patients with kras wild - type to di erent intermittent treatment schedules and therefore show the e ect of planned maintentance with a in a molecularly selected subgroup . targeted monotherapy two other studies have tested egfr inhibition as planned maintenance treatment . 
progression - free survival in the interval was improved from 48 months with bevacizumab alone to 59 months with bevacizumab and erlotinib ( hr 076 , 95% ci 061094 ; p = 001 )  . 
thus , the best strategies by which integrate bevacizumab and cetuximab into treatment are di erent , because no predictive biomarker has been discovered for bevacizumab . the nordic - vii trial4 investigated the e cacy of cetuximab when added to bolus uorouracil with folinic acid and oxaliplatin ( nordic flox ) in patients with previously untreated metastatic colorectal cancer . 
the investigators did not compare planned maintenance with cetuximab with a planned interruption and had no mandated criteria for chemotherapy reintroduction ; however , the similarity in overall survival between groups suggests that maintenance cetuximab might be an alternative strategy to continuing chemotherapy until progression . the life expectancy of patients with advanced colorectal cancer is increasing , raising questions of duration and intensity of treatment required . 
for inhibitors , greater re nement of biomarker egfr selection suggests maintenance monotherapy might be a favourable continuation strategy ( panel )  . the molecular evolution of panitumumab resistance has been elegantly shown in patients who were initially diagnosed as kras wild - type but soon developed detectable mutations in kras in their sera ( three of whom developed several di erent kras mutations ) .21 the appearance of these mutations consistently occurred 56 months after the start of treatment , which coincides with the clinical bene t noted with egfr inhibitors used 638 vol 15 may 2014 articles as monotherapy . 
the hypothesis that minimal residual disease in cancer is controlled , but rarely eradicated , implies that ono strategies with drugs might be a rational way to regulate clonal selection favourably in palliative care . 
other studies concur with coin - b with respect to the bene t of planned maintenance , although both induction chemotherapy and the bene t of continuing maintenance cytotoxic drugs to achieve maximal clinical bene t , are unknown . 
further clinical trials are warranted to investigate these points . the best duration of contributors hw was chief investigator , chaired the trial management group , cowrote the report , and enrolled patients . 
all authors reviewed the data and commented on the report . declaration of interests hw has taken part in advisory boards and educational meetings as faculty and speaker for merck kgaa during this study . 
 amm , df , cp , bs , rk , am , rb , and cl declare that they have no competing interests . acknowledgments merck kgaa provided an educational grant . 
we thank all of the patients and their families who agreed to participate in coin - b . correction to lancet oncol 2017 ; 18 : 132737 correction to lancet oncol 2017 ; 18 : 133847 correction to lancet oncol 2017 ; 18 : e564 dimopoulos ma , goldschmidt h , niesvizky r , et al . 
 lancet oncol 2017 ; 18 : 132737in the results section of this article , the data presented for any - grade adverse diarrhoea events should read diarrhoea ( 168 [ 36% ] vs 185 [ 41% ] )  . 
 these corrections have been made to the online version as of sept 27 , 2017 , and the printed article is correct . myelodysplastic in patients with platzbecker u , germing u , gtze ks , et al . 
luspatercept for the treatment of anaemia lowerrisk syndromes ( pace - mds ) : a multicentre , openlabel phase 2 dose - finding study with long - term extension study . 
 18 : e564in the second paragraph of brian samuels affiliation , the sentence in parentheses should have read ( summit cancer centers , post falls , id , usa )  . 
in the third paragraph , the sentence and quote from brian samuels as should have samuels summarised , we decided to recapitulate the original phase 2 study in liposarcomas pazopanib is active in the treatment of liposarcomas , just as it is for other subtypes of sarcoma . 
 these corrections has been made to the online version as of sept 27 , 2017 . vol 18 october 2017 e562 corrections correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections bjrn - ole juhnke , martin mynarek , * stefan rutkowski department of pediatric hematology and oncology , university medical center hamburg - eppendorf , 20251 hamburg , germany s.rutkowski@uke.de sr is a member of the paediatric oncology advisory board for novartis germany , and has received financial support from riemser pharma , as part of the hit - med trial group . 
molecular subgroups of medulloblastoma : an international meta - analysis of transcriptome , genetic aberrations , and clinical data of wnt , shh , group 3 , and group 4 medulloblastomas . 
2045 ( 17 ) 30243 - 7 . mammography screening : please dont be vague , tell me when i should come ! in the lancet oncology , prue allgood and colleagues1 report the results of a large population - based trial of second timed appointments for non - attenders of breast cancer screening in england . 
their findings show that this policy is effective in improving participation compared with an invitation letter with a telephone number to call to book a new appointment ( 2861 [ 22% ] of 12 807 women in the intervention group participated in breast cancer screening within 90 days of the first offered appointment compared with 1632 [ 12% ] of 13 247 women in the control group ; relative risk 181 [ 95% ci 170193 ] , p < 00001 )  . this kind of research is not often published in the lancet oncology or other high - impact factor scientific journals with a multidisciplinary audience , probably because research on health behaviours and compliance with public health initiatives is often context specific and not generalisable . 
a timed appointment for screening seems to be an exception : results are consistent across countries , type of screening , cultures , and time periods.2 , 3 allgood and colleagues findings suggest that timed appointments also have positive effects on participation at second timed appointments . 
 furthermore , the potential consequences on health of an intervention capable of increasing mammography screening uptake by 34% is probably higher than the impact of some new oncology drugs , tested in trials published in top - ranking according to the estimates of one death prevented and 17 life - years gained out of 180 participating women over a 20 - year period of screening , 4 increasing the average screening participation from 72% to 76% in about 8 million women ( ie , the target population in england ) could save the lives of about 90 women per year and 1500 life - years . 
this postulation can only be made if all women , at any age , with a new diagnosis of stage iv breast cancer receive and tolerate the treatment , which is clearly an implausible situation . 
 this example has been adapted from a study recently published in this journal.6 a prescheduled in the never - ending controversy about mammography screening , those opposed to screening maintain that appointment undermines the option of not participating.7 whether or not this effect actually happens is not clear , but if so , it depends on what information is conveyed to women . 
screening programmes are committed to maximising the number of women who , after having received comprehensive information about screening , decide to participate because they are published online may 15 , 2017 s1470 - 2045 ( 17 ) 30344 - 3 see articles page 972 848 vol 18 july 2017 comment conscious of both the screening benefits and harms ( informed choice to participate ) and women who decide not to participate because , according to their values , the screening benefits do not outweigh the harms ( informed choice to not participate )  . 
similarly , screening programmes should minimise the number of women who do not participate because they did not receive appropriate information or because of organisational barriers ( disinformed or involuntary non - participation ) and the number of women who agree to participate but would not have done so if they had received a clear outline of screening benefits and harms ( disinformed participation )  . through information the only way to go forward in this direction is by delivering accurate , understandable , and comthe most appropriate plete communication methods . 
although messages conveyed through an invitation letter might be transparent , they can never be neutral , because screening professionals are duty - bound to set up initiatives that are effective , and breast cancer screening programmes are established on this basis.1 nevertheless , screening programmes must remove organisational barriers as much as possible , because they could interfere with a womans decision - making process . 
with these premises , trust in public health services has a relevant role in how women decide about screening ; trust in such a common good as public health services is something that has been constructed over years of care , competence , expertise , empathy , honesty , and commitment shown by public health operators both as individuals and as an organisation . 
a timed appointment is an implicit demonstration of the accountability of the screening programmes regarding their position on the balance of screening benefits and harms . * paolo giorgi rossi , livia giordano inter - institutional epidemiology unit , ausl reggio emilia , 42122 , reggio emilia , italy ( pgr ) ; arcispedale santa maria nuova , irccs , reggio emilia , italy ( pgr ) ; and aou citt della salute e della scienza , unit of epidemiology , cpo piemonte , turin , italy ( lg ) paolo.giorgirossi@ausl.re.it pgr was a member of the steering committee of the national centre for screening monitoring . 
lg works in the epidemiology unit of the cpo piemonte that is in charge of the breast cancer screening evaluation and implementation in piedmont . the author ( s )  . 
breast cancer survival and stage at diagnosis in australia , canada , denmark , norway , sweden and the uk , 2000 - 2007 : a population - based study . 
utidelone plus capecitabine versus capecitabine alone for heavily pretreated metastatic breast cancer refractory to anthracyclines and taxanes : a multicentre , open - label , superiority , phase 3 , randomised controlled trial . 
bmj 2006 ; 332 : 53841 . the tnm classification of malignant tumourstowards common understanding and reasonable expectations clarity and precision about the anatomical extent of disease in cancer is essential for prognostication , research , and cancer - control activities . 
although the addition of predictive markers , molecular and genomic profiling , and imaging data has contributed important advances to the care of cancer patients , it has also complicated the clarity of the purpose and mission of cancer staging . 
we believe that communication of the core purpose of the tumour , node , metastasis ( tnm ) classification to different audiences , to address uncertainty about its application and to articulate the future of this system to permit ongoing study of factors that underpin most cancer discoveries , is urgently needed . 
it is an integral part of the cancer language ; 1 , 2 vol 18 july 2017 comment corrections published online november 22 , 2013 s1470 - 2045 ( 13 ) 70328 - 0 correction to lancet oncol 2013 ; 14 : 1279 , 1283 , 1285 correction to lancet oncol 2013 ; 14 : 1330 , 1333 , 1335 yamada y , takahari d , matsumoto h , et al . 
 leucovorin , fluorouracil , and oxaliplatin plus bevacizumab versus s - 1 and oxaliplatin plus bevacizumab in patients with metastatic colorectal cancer ( soft ) : an open - label , non - inferiority , randomised phase 3 trial . 
this has been corrected online as of dec 30 , 2013 . correction to lancet oncol 2013 ; 14 : 1295306 zhang j - x , song w , chen z - h , et al . 
 docetaxel or pemetrexed with or without cetuximab in recurrent or progressive non - small - cell lung cancer after platinum - based therapy : a phase 3 , open - label , randomised trial . 
 lancet oncol 2013 ; 14 : 132636in the online first version of this article ( published online nov 12 ) , in table 3 , all entries of ( > 1% ) should have read ( < 1% ) , and the rst two sentences of the third paragraph on page 1335 should state : a subsequent analysis of flex showed a signi cant association between egfr expression by immunohistochemistry and improved outcomes , with high egfr expression ( h - score 200 or higher ) being associated with improved overall survival , time - to - treatment failure , and a greater proportion of patients achieving objective responses when treated with cetuximab than when treated with cisplatin plus vinorelbine alone.13 there was no improvement in outcomes in the low h - score group ( h - score lower than 200 ) .13 these corrections were made to the print version of the article in the december issue of the journal , and have been made online as of nov 22 , 2013 . 
in table 1 , the entry for adenocarcinoma in the cetuximab and pemetrexed group should have read 161 ( 53% ) and the entry for all other diagnoses in the pemetrexed group should have read 41 ( 13% )  . 
in table 3 , in the cetuximab plus pemetrexed group , the entry for patients with one or more ctcae grades 12 should have read 89 ( 30% ) , that for grade 3 anaemia 16 ( 5% ) , for grade 4 infusion related reactions 5 ( 2% ) , and grade 3 lung infection 16 ( 5% )  . 
 in the pemetrexed group in the same table , the entry for patients with one or more grade 4 ctcae should have read 36 ( 12% ) and one or more grade 5 ctcae 10 ( 3% ) ; the entry for grade 12 diarrhoea should have read 36 ( 12% ) , that for grade 12 hyperglycaemia 10 ( 3% ) , and grade 12 maculopapular rash 39 ( 13% )  . 
 vol 15 january 2014 correction to lancet oncol 2017 ; 18 : 132737 correction to lancet oncol 2017 ; 18 : 133847 correction to lancet oncol 2017 ; 18 : e564 dimopoulos ma , goldschmidt h , niesvizky r , et al . 
 lancet oncol 2017 ; 18 : 132737in the results section of this article , the data presented for any - grade adverse diarrhoea events should read diarrhoea ( 168 [ 36% ] vs 185 [ 41% ] )  . 
 these corrections have been made to the online version as of sept 27 , 2017 , and the printed article is correct . myelodysplastic in patients with platzbecker u , germing u , gtze ks , et al . 
luspatercept for the treatment of anaemia lowerrisk syndromes ( pace - mds ) : a multicentre , openlabel phase 2 dose - finding study with long - term extension study . 
 18 : e564in the second paragraph of brian samuels affiliation , the sentence in parentheses should have read ( summit cancer centers , post falls , id , usa )  . 
in the third paragraph , the sentence and quote from brian samuels as should have samuels summarised , we decided to recapitulate the original phase 2 study in liposarcomas pazopanib is active in the treatment of liposarcomas , just as it is for other subtypes of sarcoma . 
 these corrections has been made to the online version as of sept 27 , 2017 . vol 18 october 2017 e562 corrections corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
we assessed whether the addition of docetaxel to active symptom control alone can improve survival and hrqol for patients . methods for this open - labelled , multicentre trial , we recruited patients aged 18 years or older from 30 uk centres . 
 patients were eligible if they had an advanced , histologically con rmed adenocarcinoma of the oesophagus , oesophagogastric junction , or stomach that had progressed on or within 6 months of treatment with a platinumuoropyrimidine combination . 
we randomly assigned patients using a central , computerised minimisation procedure to receive docetaxel plus active symptom control , or active symptom control alone ( 1 : 1 ; strati ed by disease status , disease site , duration of response to previous chemotherapy , and performance status )  . 
this study is an international standardised randomised controlled trial , number isrctn13366390 . findings between april 21 , 2008 , and april 26 , 2012 , we recruited 168 patients , allocating 84 to each treatment group . 
docetaxel was associated with higher incidence of grade 34 neutropenia ( 12 [ 15% ] patients vs no patients ) , infection ( 15 [ 19% ] patients vs two [ 3% ] patients ) , and febrile neutropenia ( six [ 7% ] patients vs no patients )  . 
 even after combination treatment including surgery , more than half of patients in western populations relapse.2 when relapse or progression occurs after rstline treatment , median overall survival with supportive care is only 34 months.3 the high global incidence of oesophago gastric cancer , the high relapse rate , and the short survival after relapse or progression indicate an urgent need for e ective second - line treatment . when we planned this trial , we knew of no randomised data indicating any bene t to second - line chemotherapy . 
 the best evidence consisted of small ( fewer than 50 patients ) phase 2 trials , ndings from which had suggested tumour responses with di erent chemo therapy agents including irinotecan4 and docetaxel.5 the largest series reported 154 patients treated with docetaxel 75 mg / m of body surface area every 3 weeks after failure of a platinum and uoropyrimidine combination , with a response rate of 14% and median overall survival of 72 months.6 however , potential for toxicity from chemo therapy is high in this group of patients with a poor prognosis , and there was no evidence that chemotherapy improved either survival or health - related quality of life ( hrqol )  . vol 15 january 2014 articles we therefore aimed to assess the bene ts of secondline docetaxel in patients whose disease had progressed within 6 months of previous chemotherapy . 
in particular , we aimed to nd out whether any survival bene t came with an improvement in hrqol . con rmed adenocarcinoma of methods study design and patients this multicentre , open - label , randomised , controlled phase 3 trial was designed by the cougar - 02 trial management group under the auspices of the upper gastrointestinal cancer clinical studies group of the uk national cancer research institute . 
patients at least 18 years old with the histologically oesophagus , oeso phago gastric junction , or stomach were eligible for inclusion if they had advanced disease and documented disease progression during or within 6 months of treatment with platinum and uoropyrimidine - based treatment ( which could have been given as adjuvant or neoadjuvant therapy , or for advanced disease )  . 
patients with disease - free intervals longer than 6 months were not eligible because the most common uk practice is that patients with a treatment - free interval of more than 6 months with chemotherapy would be either re - challenged with the original chemotherapy or o ered second - line chemo therapy . 
all aspects of the study were done in accordance with the declaration of helsinki including all of its relevant amendments , the guidelines for good clinical practice harmonization , and all relevant uk and european laws and directives . 
we randomly allocated patients in a 1 : 1 ratio to either docetaxel plus active symptom control ( docetaxel group ) or active symptom control alone using a central computerised minimisation procedure generated at the warwick clinical trials unit . 
 trial allocations were strati ed by disease status ( locally advanced vs metastatic disease ) , disease site ( oesophagus vs oesophagogastric junction vs gastric ) , duration of response to previous chemotherapy ( no response vs response duration < 3 months vs response duration 36 months ) , and performance status ( 01 vs 2 )  . 
because this was an open - label study , participants , investigators , and trials sta were aware of treatment allocations . each administration treatment active symptom control was o ered to all patients participating in the trial , and was delivered according to local pathways within each participating hospital and included community and hospice care . 
docetaxel was given at a dose of 75 mg / m of body - surface area by intravenous infusion over 1 h every 3 weeks for up to six cycles , which was the standard dose and schedule in the uk at the time of the study . 
we gave patients dexamethasone 8 mg orally , two times a day for three doses before docetaxelie , dexamethasone treatment starting 1 day before docetaxel administration ( morning and evening ) and about 1 h before docetaxel administration . 
we stipulated in the protocol that steroids were also given after treatment ( ie , 8 mg orally , two times a day for three doses ) , but local protocols were accepted . 
if the absolute neutrophil count ( anc ) was greater than 15 10 cells per l or platelet count was above 100 10 per l then treatment was continued at full dose . 
subsequent treatments were given at full dose unless there was lengthy grade 4 neutropenia ( anc less than 05 10 cells per l for more than 7 days ) or febrile neutropenia , in which case the dose of docetaxel was reduced to 55 mg / m of body - surface area for subsequent cycles . 
 subsequent treatments were given at full dose unless the platelet count had fallen to less than 50 10 per l , in which to greater vol 15 january 2014 articles case the dose of docetaxel was reduced to 55 mg / m of body - surface area for subsequent cycles . 
in the event of hepatic toxicity , de ned as bilirubin greater than upper limit of normal , alanine aminotransferase or aspartate aminotransferase greater than 15 times the upper limit of normal , alkaline phosphatase greater than 25 times the upper limit of normal in the absence of liver metastases , or alkaline phosphatase greater than 5 times the upper limit of normal in the presence of liver metastases , then treatment was delayed until recovery and the dose of docetaxel was reduced to 55 mg / m of body - surface area for subsequent cycles . 
for grade 2 toxicity subsequent treatments were given at full dose , whereas in the event of grade 3 or 4 toxicity , the dose of docetaxel was reduced to 55 mg / m of body - surface area for subsequent cycles . 
for all other grade 34 non - haematological toxicities , treatment was interrupted until resolution and the dose of docetaxel was reduced to 55 mg / m of bodysurface area for subsequent cycles . see online for appendix enrolment 356 assessed for eligibility 188 excluded 77 did not meet inclusion criteria 71 declined to participate 40 other reasons 168 randomised 84 allocated to docetaxel active symptom control 77 received allocated intervention 7 did not receive allocated intervention 3 died 1 refused treatment 1 withdrew 1 delay > 21 days 1 patient admitted for another disorder 84 allocated to active symptom control 78 received allocated intervention 6 did not receive allocated intervention 4 withdrew 1 entered another trial 1 had progressive disease allocation outcome 48 discontinued intervention 32 died 6 entered phase i trial 4 patient decision ( wanted chemotherapy ) 2 followed up at dierent hospital 2 declined further assessments 1 progressive disease 1 withdrew 84 analysed for primary survival outcome 57 health - related quality of life 74 adverse events analysis 58 discontinued intervention 26 progressive disease 20 unacceptable toxicity 7 died 4 delay > 21 days 1 poor performance status 84 analysed for primary survival outcome 69 health - related quality of life 81 adverse events 56 response assessment 84 time to progression figure 1 : trial pro le docetaxel was discontinued on completion of six cycles , delay of treatment for more than 21 days , disease progression , unacceptable toxicity , or patient request . we reviewed patients on active symptom control alone every 3 weeks for the 18 - week treatment period . 
at baseline and at each study visit a patients status was assessed by medical history , physical examination including performance status and weight , full blood count , and biochemical serum analysis . 
we needed a sample size of 320 patients to detect a median overall survival gain from 4 months to 6 months , assuming patients were recruited over a 2 year period and were followed up for a minimum of 6 months , with 90% power and two - sided alpha of 005 . 
while the study was underway , a randomised trial was published that suggested a survival advantage for chemotherapy and a poorer overall survival for patients given active symptom control than we had assumed.12 we recalculated the sample size on the recommendation of the rst independent data monitoring and ethics committee in june , 2010 , on the basis of poorer recruitment than expected and assuming a lower overall survival in the control group . 
a revised minimum total of 164 patients was therefore needed to detect a hazard ratio of 064 , assuming 35 years recruitment , a two - sided alpha of 005 , and 80% power , but was su cient to accommodate a range of potential outcomes ( appendix ) .13 secondary endpoints were best response to docetaxel , time to documented disease progression ( for the docetaxel group ) , toxicity , and hrqol . 
important hrqol endpoints identi ed before we started the study were physical and social function and fatigue ( qlq - c30 ) and eating restrictions and dysphagia ( qlq - sto22 )  . we did all analyses on an intention - to - treat basis . 
we calculated time to documented disease progression within 24 weeks from date of randomisation until date of progression , or death from disease without recorded progression if within 24 weeks . 
we constructed survival curves using the kaplan - meier method.14 we vol 15 january 2014 articles compared survival di erences using a cox proportional hazard model and calculated hazard ratios with 95% cis.15 we did a planned multivariate cox - regression analysis for overall survival to adjust the treatment e ect for the strati cation variables . 
we calculated hazard ratios for prognostic subgroups and constructed a hazard ratio plot.16 the delivered dose intensity for docetaxel was calculated as the ratio of actual dose received per week to the expected dose averaged over the number of cycles administered . we analysed hrqol data with a standardised area under the curve analysis and compared them using wilcoxon rank sum tests.17 we handled missing questionnaire data by calculating the scale score if at least half of items were answered.18 we did sensitivity analyses adjusting for dropouts due to death using a qualityadjusted survival analysis for the global hrqol score.19 reported p values are two sided and are considered statistically signi cant at a value of less than 005 . 
we used sas ( version 9.2 ) for all statistical analyses . this study is registered as an international standard randomised controlled trial , number isrctn 13366390 . role of the funding source neither the funders or sponsors of the trial participated in study design , in data accrual or analysis , or in the preparation of this paper . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results between april 21 , 2008 , and april 26 , 2012 , we recruited 168 patients ( appendix ) , allocating 84 patients to each trial group ( gure 1 )  . 
 after randomisation , eight patients ( four in each group ) were deemed ineligible because they did not have documented disease progression within 6 months of previous chemotherapy ( n = 3 ) or unsatisfactory blood results ( n = 5 )  . 
these patients all went on to receive the allocated treatment and were included in the analyses on an intention - to - treat basis . 255 the treatment cycles were administered 84 patients in the docetaxel group , with a median of three treatment cycles ( iqr 15 ) per patient . 
in the docetaxel group , 19 ( 23% ) of these 84 patients completed all six cycles of treatment , 17 ( 20% ) received only one cycle , and seven ( 8% ) had no docetaxel . 
of the 65 patients who did not complete all six cycles , the three main reasons for early discontinuation of treatment were progressive disease in 26 ( 40% ) patients , unacceptable toxicity in 20 ( 31% ) patients , and death in ten ( 15% ) patients . 
 treatment delays were infrequent ( occurring in 29 [ 11% ] of 255 cycles ) and were mainly due to toxicity ( in ten [ 34% ] cycles ) , administrative decisions ( in eight [ 28% ] ) , clinical decision ( in six [ 21% ] ) , or patient request ( in three [ 10% ] )  . 
the overall median course dose intensity was 46% ( iqr 1974 )  . in the active symptom control group , 30 ( 36% ) of 84 patients completed at least 18 weeks of follow - up . 
the main reason for early discontinuation of follow - up was death ( in 32 [ 59% ] patients )  . individuals older than 70 years 23 ( 27% ) 16 ( 19% ) eastern cooperative oncology group performance status male female age in years disease status locally advanced metastatic disease site of primary disease oesophagus oesophagogastric junction stomach during treatment within 3 months 36 months docetaxel ( n = 84 ) active symptom control ( n = 84 ) 69 ( 82% ) 15 ( 18% ) 67 ( 80% ) 17 ( 20% ) 65 ( 2884 ) 66 ( 3684 ) 24 ( 28% ) 46 ( 55% ) 14 ( 17% ) 11 ( 13% ) 73 ( 87% ) 18 ( 22% ) 27 ( 32% ) 39 ( 46% ) 36 ( 43% ) 27 ( 32% ) 21 ( 25% ) 22 ( 26% ) 50 ( 60% ) 12 ( 14% ) 10 ( 12% ) 74 ( 88% ) 15 ( 18% ) 32 ( 38% ) 37 ( 44% ) 36 ( 43% ) 22 ( 26% ) 26 * ( 31% ) time between end of previous chemotherapy and documented disease progression data are n ( % ) or median ( range )  . 
 table 1 : baseline characteristics docetaxel active symptom control hazard ratio = 067 ( 95% ci 049092 ) ; p = 001 time from randomisation ( months ) number at risk docetaxel 84 active symptom 84 control figure 2 : kaplan - meier plot of overall survival vol 15 january 2014 articles 16 patients in the active symptom control group went on to have further systemic cancer treatment : 11 entered early phase clinical studies and ve had conventional chemotherapy . 
seven patients in the docetaxel group went on to have further systemic cancer treatment : three entered early phase clinical trials and four received conventional chemotherapy . at the time of the planned nal analysis , 6 months after we allocated the nal patient to treatment , 161 ( 96% ) patients had died ( 80 patients [ 95% ] in the docetaxel group and 81 [ 96% ] in the active symptom control group )  . 
median overall survival for patients allocated to docetaxel was 52 months ( 95% ci 4159 ) compared with 36 months ( 3344 ) for patients in the control group ( hazard ratio 067 , 95% ci 049092 , p = 001 ; gure 2 )  . 
overall survival in the docetaxel group was 82% ( 95% ci 7289 ) at 2 months and 39% ( 2950 ) at 6 months , and in the control group was 84% ( 7591 ) at 2 months and 23% ( 1534 ) at 6 months . 
we estimated the number of patients needed to treat at 6 months to be seven ( 95% ci 39348 ) ie , seven patients would be needed to be treated with docetaxel to lead to one extra survivor at 6 months . a multivariate cox proportional hazard model showed that performance status ( p = 0001 ) and disease status ( locally advanced better than metastatic disease , hazard ratio 207 , 95% ci 123350 ; p = 0006 ) were predictors of overall survival ( appendix )  . 
patients with a performance status of 0 had better overall survival than those with a performance status of 1 ( hazard ratio 200 , 95% ci 135296 ) or two ( 216 , 127366 )  . 
the treatment e ect remained statistically signi cant in the multivariate analysis after adjustment for strati cation variables ( p = 003 )  . we detected a bene t of docetaxel treatment after stratifying by performance status , disease status , site of disease , and time between end of previous chemotherapy and documented disease progression ( gure 3 )  . 
 progression - free survival at 6 weeks was 88% ( 7993 ) and at 24 weeks was 29% ( 1938 )  . for patients ten deaths ( seven in the docetaxel group and three in the active supportive care group ) occurred within 30 days of randomisation . 
 hence , ve ( 6% ) deaths were within 30 days of receiving any docetaxel , but none was attributed to chemotherapy . more patients in the docetaxel group had one or more grade 4 toxicity compared with those in the control group ( 17 [ 21% ] patients vs three [ 4% ] patients )  . 
 haemorrhage and pain were more common in the control group than in the docetaxel group ( table 2 )  . 560 ( 69% ) of 812 hrqol forms were returned : 318 ( 72% ) of 442 in the docetaxel group and 242 ( 65% ) of 370 in the active supportive care group ( appendix )  . 
the the absent main reasons for non - completion of 242 on - study hrqol forms were : administration error ( 75 [ 31% ] of 242 patients ) , patient unwell ( 50 [ 21% ] of 242 patients ) , or patient refused or did not attend ( 48 [ 20% ] of 242 patients )  . 
by 24 weeks , 118 ( 70% ) patients had died or were o study and no longer participating in hrqol ( 51 [ 61% ] patients in the docetaxel group , and 67 [ 80% ] patients in the active supportive care group )  . baseline qlq - c30 and qlq - sto22 scores were similar in both groups . 
bene ts for docetaxel were seen in all pre - speci ed important domains , of which dysphagia was statistically signi cant ( p = 002 ) , and for several exploratory domains ( gure 4 )  . patients in the docetaxel group reported less general pain ( p = 00008 ) , abdominal pain ( p = 001 ) , nausea and vomiting ( p = 002 ) , and constipation ( p = 002 ) than those in the control group , but similar global hrqol ( p = 053 ; appendix )  . 
the ndings of a phase 3 trial of the mtor inhibitor everolimus showed no bene t compared with 43 months ; survival 54 placebo ( overall p = 012 ) .23 targeting of angiogenesis might be a more productive avenue of investigation . 
findings from a study of 355 patients with gastrooesophageal adenocarcinoma treated in the second - line setting with either placebo or with ramucirumab , an inhibitor of vegfr - 2 , showed a survival advantage for ramucirumab with median overall survival of 52 months versus 38 months ( hazard ratio 078 [ 95% ci 060100 ] ; p = 0047 ) .24 another group have reported the results of a randomised phase 2 trial comparing apatinib ( yn968d1 ; another vegfr - 2 inhibitor ) 850 mg given either as a single or divided dose with placebo.25 patients treated with either schedule of apatinib had better overall survival ( 483 months and 427 months , respectively , vs 25 months for placebo ; p < 0001 and p = 00017 , respectively ) .25 we believe that our ndings add several important factors to the present evidence base . 
the largest previously published trial of chemotherapy was done in an asian population with gastric cancer only.3 therefore , the ndings of that trial are not ideally suited to guide treat ment outside of asia because evidence exists that tumour biology di ers between people of asian origin and those of white patients.2 , 26 we know of no other trial that included patients with oesophageal adenocarcinoma in addition to those with oesophagogastric junction and gastric adenocarcinoma . 
 the median age of 65 years in our study was more representative of the population seen in clinical practice than in other studies in which the median age was less than 60 years.3 , 12 we also included patients with an ecog performance status of 02 . 
the only other trial we know of that included any patients with a performance status of 2 had only four such patients in the treatment group.12 the slight survival bene t achieved by administration of toxic chemotherapy necessitates careful assessment of hrqol , toxicity , and disease - speci c symptoms . 
hrqol data are important to inform clinical decision making , and to provide patients with information about likely e ects of functional aspects of health and treatment on symptoms.27 studies that have measured hrqol in gastric cancer often have incomplete datasets or poor reporting , which limits their application . 
this nding is in keeping with other research showing the predictive value of self - reported pain and survival in oesophagogastric cancer.29 unfortunately , however , the health of this population of patients deteriorates rapidly , meaning that questionnaire return is often problematicour study was no exception , with only 57% of questionnaires returned in vol 15 january 2014 articles the active symptom control group at 6 weeks . 
such low questionnaire return is a limitation of the study , and might in part explain why dysphagia was the only prespeci ed endpoint to show a bene t in favour of docetaxel . 
 undertaking home visits might be the only way to improve response to hrqol surveys in such trials.30 we did not measure time to progression in the active symptom control group . 
in a population with known progressive disease at study entry the value of measuring time to progression in a population not receiving cancer treatment is questionable , and we felt that it was not appropriate to subject these patients to additional unnecessary investigations . 
patients in both arms of the trial were allowed to receive other treatments after study completion , and a greater number did so in the control group ( 16 patients ) than the docetaxel group ( seven patients )  . 
if anything , this disparity might be expected to improve outcomes in the control group , and reduce the recorded bene t of docetaxel . there are areas of possible bias in this trial , principally the open - label design without placebo control ( which was felt to be unavoidable given the very obvious toxicities of docetaxel such as alopecia and the ethical di culty associated with a placebo infusion )  . 
the sex ratio in the trial ( 81% male ) is higher than would be expected for the uk oesophagogastric cancer population , generally , in which where the male - to - female ratio is about 65 men to 35 women . 
the reasons for this high proportion of men are not clear . patients in the docetaxel group received steroids with each infusion , which has some potential to bias the hrqol scores , as does the rate of non - completion of questionnaires . 
additionally , although active symptom control was provided for all patients in the trial , and included access to community palliative care and hospice services , we could not standardise the type of active supportive care fully , which is another potential source of bias . 
this possible bias was mitigated by the fact that patients continued to have regular review at the treating centre , with only one patient in the control group lost to follow - up . the evidence for improvement in hrqol with docetaxel , particularly reduced pain , and the survival gain are both consistent with a bene cial e ect from chemotherapy . 
 future trials , which should include hrqol outcome measures , should focus on optimising chemotherapy and the addition of relevant biological agents . panel : research in context systematic review we identi ed a systematic review of second - line chemotherapy versus supportive cancer treatment in advanced gastric cancers21 that searched the cochrane central register of controlled trials ( central , issue 1 , 2013 ) , medline ( 1950 to march week 4 , 2013 ) , and embase ( 1980 to 2013 , week 13 ) for articles that included the following terms gastric or gastroesophageal or gastroesophagus or esophagogastric or stomach , cancer or neoplasm or carcinoma or malignant or malignancy , second line or salvage or supportive care , chemotherapy or chemotherapeutic or antineoplastic agent , and randomized or randomised , controlled trial or randomised , and searched the reference lists of relevant articles and reviews and used the related articles feature in pubmed to identify additional articles . 
clinical trials that met the following criteria were included in the meta - analysis : trials comparing second - line or salvage treatment chemotherapy with best supportive care , and prospective phase 3 randomised trials . 
the investigators21 did a meta - analysis of the three high - quality randomised trials identi ed ( including the initial report of our trial , presented at the american society of clinical oncology annual meeting in chicago , il , usa , held on may 31 to june 4 , 2013 ) , and reported a reduction in the risk of death with second - line chemotherapy with no di erences in treatment e ect between docetaxel and irinotecan . 
 however , the ndings are lent support by another trial that reported no di erence between outcomes for patients treated with either paclitaxel or irinotecan22 and are the best available assessment of the evidence in this subject area . interpretation the results of our trial and others provide level a evidence that second - line chemotherapy can provide both survival and quality - of - life bene ts to selected patients who have progressed after rst - line treatment for oesophagogastric adenocarcinoma . 
docetaxel , paclitaxel , and irinotecan have all shown activity and can be regarded as appropriate for use as second - line treatment , with this study providing new evidence of quality - of - life bene t with docetaxel . 
in practice , patients who have received a taxane as part of their primary treatment are likely to be treated with irinotecan , whereas those who have not could be considered for either second - line irinotecan or taxane therapy . 
the role of biological agents such as ramucirumab and apatinib will depend on the results of future trials and regulatory approval , but addition of these agents could prove to add bene t to that already seen with chemotherapy . on the basis of our ndings , we believe that chemotherapy should be o ered to t patients for the second - line treatment of oesophagogastric adenocarcinoma , and that treatment with docetaxel can improve some aspects of quality of life for patients . 
am was the trial statistician and did the trial design , preparation of study reports , and preparation of paper including gures , and was a member of trial management group and trial steering committee . 
 the trial was sponsored by cambridge university hospitals nhs foundation trust ( cambridge , uk ) and funded by cancer research uk [ grant number c21276 / a12372 ] , clinical trial number cruk / 07 / 013 . 
 dc is funded by the nihr biomedical centre at the royal marsden hospital and institute of cancer research . articles lancet oncol 2013 ; 14 : 199209 published online february 7 , 2013 s1470 - 2045 ( 12 ) 70600 - 9 this online publication has been corrected . 
the corrected version rst appeared at thelancet.com / oncology on june 30 , 2014 see comment page 178 she eld childrens hospital , she eld , uk ( prof a vora frcpath ) ; great ormond street hospital , london , uk ( n goulden phd ) ; clinical trial service unit , university of oxford , oxford , uk ( r wade msc , s richards dphil ) ; john radcli e hospital , oxford , uk ( c mitchell frcpch ) ; north bristol nhs trust , bristol , uk ( j hancock phd ) ; university college hospital , london , uk ( r hough md ) ; and university hospital of wales , cardi , uk ( c rowntree phd ) correspondence to : prof ajay vora , department of haematology , she eld childrens hospital , she eld s10 2th , uk ajay.vora@sch.nhs.uk treatment reduction for children and young adults with low - risk acute lymphoblastic leukaemia de ned by minimal residual disease ( ukall 2003 ) : a randomised controlled trial ajay vora , nick goulden , rachel wade , chris mitchell , jeremy hancock , rachael hough , clare rowntree , sue richards summary background minimal residual disease ( mrd ) is the most sensitive and speci c predictor of relapse risk in children with acute lymphoblastic leukaemia ( all ) during remission . 
we assessed whether treatment intensity could be adjusted for children and young adults according to mrd risk strati cation . methods between oct 1 , 2003 and june 30 , 2011 , consecutive children and young adults ( aged 124 years ) with all from the uk and ireland were recruited . 
eligible patients were categorised into clinical standard , intermediate , and high risk groups on the basis of a combination of national cancer institute ( nci ) criteria , cytogenetics , and early response to induction therapy , which was assessed by bone marrow blast counts taken at days 8 ( nci high - risk patients ) and 15 ( nci standard - risk patients ) after induction began . 
those classi ed as mrd low risk ( undetectable mrd at the end of induction [ day 29 ] or detectable mrd [ less than 001% ] at day 29 that became undetectable by week 11 ) were randomly assigned to receive one or two delayed intensi cation courses . 
delayed intensi cation consisted of pegylated asparaginase on day 4 ; vincristine , dexamethasone ( alternate weeks ) , and doxorubicin for 3 weeks ; and 4 weeks of cyclophosphamide and cytarabine . 
 this trial is registered , number isrctn07355119 . findings of 3207 patients registered in the trial overall , 521 mrd low - risk patients were randomly assigned to receive one ( n = 260 ) or two ( n = 261 ) delayed intensi cation courses . 
we recorded no signi cant di erence in efs between the group given one delayed intensi cation ( 944% at 5 years , 95% ci 911977 ) and that given two delayed intensi cations ( 955% , 928982 ; unadjusted odds ratio 100 , 95% ci 043231 ; two - sided p = 099 )  . 
11 patients ( actuarial relapse at 5 years 56% , 95% ci 2389 ) given one delayed intensi cation and six ( 24% , 0246 ) given two delayed intensi cations relapsed ( p = 023 )  . 
three patients ( 12% , 026 ) given two delayed intensi cations died of treatment - related causes compared with none in the group given one delayed intensi cation ( p = 008 )  . 
we recorded no signi cant di erence between groups for serious adverse events and grade 3 or 4 toxic e ects ; however , the second delayed intensi cation course was associated with one ( < 1% ) treatment - related death , and 74 episodes of grade 3 or 4 toxic e ects in 45 patients ( 17% )  . interpretation treatment reduction is feasible for children and young adults with all who are predicted to have a low risk of relapse on the basis of rapid clearance of mrd by the end of induction therapy . funding medical research council and leukaemia and lymphoma research . introduction several step changes in outcomes for children with acute lymphoblastic leukaemia ( all ) were made in the last three decades of the 20th century ; at the start of the 21st century , 80% of patients could expect to survive without relapse after rst - line treatment.14 the challenges for clinical trials at that time were to sustain that rate of improvement without new drugs and to address the problem of immediate and long - term toxic e ects of treatment . 
 historically , the intensity of treatment received by a patient with all was based on risk of relapse , which was predicted by a combination of clinical , cytogenetic , and morphological early response criteria.1 , 3 , 4 however , risk groups identi ed by these variables are fairly non - speci c , because most relapses arise in medium - risk and low - risk groups.1 , 3 , 4 monitoring of minimal residual disease ( mrd ) has been shown to be the most sensitive and speci c predictor of relapse risk in several large studies.5 , 6 these studies established that the positive and negative predictive vol 14 march 2013 articles for trial protocol see mega - trials / leukaemia - trials / ukall - 2003 value of a speci c mrd result depends on the sensitivity of the technique used to measure it , the point at which it is measured , and the treatment received by the patient before and after the point of assessment . 
 patients who have undetectable mrd by the end of induction therapy have a negligible risk of relapse , whereas those who have more than 001% mrd at that timepoint have a relapse risk of more than 20% . 
hence , mrd monitoring has been used in several clinical trials1 , 79 to better predict the risk of relapse for an individual . we tested whether adjustment of treatment intensity according to mrd risk strati cation was feasible . 
 patients with philadelphia - chromosome - positive all were transferred to other protocols such as the european study for philadelphia - chromosome - positive all ( esphall ) 11 or ukall xii12 once their philadelphiachromosome status was known . 
 the upper age limit of entry was 18 years at the start of the trial , but was increased to 20 years in february , 2006 , and to 24 years from august , 2007 , because retrospective studies showed that young adults obtained an improved outcome when treated with paediatric protocols . 
the overall treatment intensity for patients with downs syndrome had to be reduced after june , 2008 , because of excess treatment - related mortality ; from that time , patients with downs syndrome were registered on the trial but did not undergo randomisation and were treated as clinical standard - risk patients , with adjustment of postinduction treatment according to response to induction therapy . patients were strati ed according to initial clinical risk of relapse , on the basis of three metrics : the national cancer institute ( nci ) risk criteria ( nci standard risk : patients younger than 10 years with a white blood cell count of less than 5010 per l ; nci high risk : patients aged 10 years or older and those with a white blood cell count of at least 5010 per l ) , leukaemia cytogenetics ( all patients with a cytogenetic abnormality involving rearrangement of the mll gene , hypodiploidy [ < 45 chromosomes ] , or intrachromosomal ampli cation of chromosome 21 were classi ed as clinical high risk ) , and early response to induction therapy as assessed by bone - marrow morphology on day 8 and 15 of treatment in patients younger than 16 years . 
patients who had more than 25% of the marrow made up of blast cells at day 8 ( nci high risk ) or 15 ( nci standard risk ) were reclassi ed to the clinical high risk group irrespective of initial classi cation and were not eligible for mrd strati cation and randomisation . 
nci standard - risk patients had to have an early response of less than 25% marrow blasts at the day 15 assessment ( reclassi ed as clinical standard risk ) and nci high - risk patients who had less than 25% marrow blasts at day 8 were reclassi ed as clinical intermediate risk to be eligible for randomisation . 
all patients who were 16 years or older were treated as clinical intermediate risk irrespective of day 8 or 15 bone - marrow response and were eligible for mrd strati cation and randomisation . we strati ed clinical standard and intermediate risk groups by bone - marrow mrd at the end of induction and recovery from consolidation ( before start of interim maintenance )  . 
the quantitative range of the assay was 10 , which was done within four laboratories in the uk in a european quality - assurance that participated scheme.13 , 14 all mrd results were centrally reviewed . 
 patients with undetectable mrd after induction ( day 29 ) and before interim maintenance were classi ed as mrd low risk , as were those with detectable ( less than 001% ) mrd at the end of induction but undetectable mrd before the start of interim maintenance . 
patients in whom mrd could not be measured because no or poor - quality samples were available and those with persistent disease which was less than 001% mrd before the start of interim maintenance were classi ed as mrd indeterminate . 
the trial was monitored by an independent data monitoring committee , which reviewed safety and e cacy data annually . randomisation and masking mrd low - risk patients were randomly assigned ( 1 : 1 ) to receive one ( reduced treatment ) or two ( standard treatment ) delayed intensi cations and mrd high - risk patients were randomly assigned ( 1 : 1 ) to standard treatment or an intensive schedule . 
treatment allocation in both groups was obtained by telephone call to the central trials unit , where computer randomisation was done , with strati cation by mrd result and balancing for sex , age ( < 10 years vs 10 years ) and white blood cell count at diagnosis ( < 50 10 per l vs 50 10 per l ) by method of minimisation . 
patients , clinicians , and data analysts were not masked to treatment allocation . 200 vol 14 march 2013 articles see online for appendix procedures patients received one of three escalating - intensity treatment regimens depending on their clinical risk grouping ( gure 1 ; full regimen details are provided in the appendix )  . 
all patients received two doses of intrathecal methotrexate in induction , and their cerebrospinal uid at diagnosis received an additional two doses at day 15 and 21 . those who had blasts during consolidation , clinical standard - risk patients received daily oral mercaptopurine and four doses of weekly intrathecal methotrexate . 
clinical high - risk patients received an additional four doses of vincristine and two doses of pegylated asparaginase during the bfm consolidation course . clinical standard - risk and intermediate - risk patients received the same interim maintenance courses for 8 weeks : daily oral mercaptopurine and weekly methotrexate with monthly vincristine and steroid pulses . 
clinical highrisk patients received escalating doses of intravenous methotrexate without folinic acid rescue , and vincristine and pegylated asparaginase as interim maintenance . clinical standard - risk and inter mediate - risk patients assigned to standard treatment received two delayed intensi cation courses separated by interim maintenance courses ( gure 1 ) , and those assigned to reduced treatment received only one delayed intensi cation course followed therapy . 
clinical standard - risk and by continuing intermediate - risk patients received the same delayed intensi cation courses : one dose of pegylated asparaginase on day 4 ; vincristine , dexamethasone ( alternate weeks ) , and doxorubicin for 3 weeks ; and then 4 weeks of cyclophosphamide and cytarabine as during the bfm consolidation course . 
male patients received treatment for 3 years and female patients for 2 years from the start of interim maintenance . all patients received 6 mg / m oral dexamethasone daily during induction and maintenance courses , with a maximum dose of 10 mg . 
mrd high - risk patients assigned to the intensive schedule transferred to clinical high - risk regimen after induction . vol 14 march 2013 articles 3207 patients registered in the trial 3126 eligible for analysis 81 excluded 3 had been registered twice 7 withdrew consent 12 had been misdiagnosed * 59 philadelphia - chromosomepositive 1732 clinical standard risk 989 clinical intermediate risk 405 clinical high risk 2721 eligible for mrd stratication 820 indeterminate mrd status 808 high - risk mrd 1059 low - risk mrd 34 died within 35 days or never remitted 736 identied before august , 2009 323 identied after august , 2009 215 not randomly assigned 97 refused 7 had downs syndrome 4 because of toxic eects 28 other reason 79 unknown 521 randomly assigned 261 assigned to two delayed intensications 260 assigned to one delayed intensication figure 2 : trial pro le mrd = minimal residual disease . 
 * one patient had burkitts lymphoma , one t - cell lymphoma , one t non - hodgkin lymphoma , one mature b - cell acute lymphoblastic leukaemia , two acute myeloid leukaemia , ve mixed - phenotype acute leukaemia , and one precursor b non - hodgkin lymphoma . 
 patients with traumatic lumbar puncture and blasts in the cerebrospinal uid , and those with fewer than ve blasts per l also received an extra two doses of intrathecal methotrexate during induction . 
clinical highrisk patients received capizzi intravenous methotrexate at doses of less than 500 mg / m without folinic acid rescue during interim maintenance . patients whose bone marrow consisted of more than 25% blasts at day 29 of induction , or those with a high - risk karyotype whose bone marrow consisted of more than 5% blasts at that timepoint were eligible for allogeneic haemopoietic stem - cell transplantation in the rst complete remission . 
additionally , patients with an intrachromosomal ampli cation of chromosome 21 and a morphological slow early response at day 8 or 15 , or mrd high - risk status at day 29 were eligible for allogeneic transplant in rst complete remission . 
 statistical analysis we anticipated that total accrual to the trial in a 6 - year period would be 2500 patients , of whom we expected about 400 to be eligible for the randomisation of the mrd low - risk group . 
in view of the few relapses expected in this group , and with a one - sided p value , we would have 80% power to detect a reduction in 5 - year efs in the group given one delayed intensi cation course from 95% to 88% . 
 however , the proportion of patients in the low - risk group was higher than had been originally anticipated and , because of a shortfall in recruitment to the high - risk group , the trial was kept open after its original closing date of oct 31 , 2009 . 
therefore , the data monitoring committee recommended an increase in sample size in the low - risk group to narrow the con dence intervals of the di erences in outcome between groups . 
randomisation of mrd lowrisk patients ended on aug 24 , 2009 , and randomisation of mrd high - risk patients on june 30 , 2011 , after the target number of patients had been recruited . we compared categorical variables with standard tests . 
we counted only rst events , censoring at competing eventseg , time to bone - marrow relapse included censoring at non - bone marrow relapse or death in remission for patients with these events as their rst . 
we used cox 202 vol 14 march 2013 articles regression multivariate analyses to test whether e ects of prognostic factors were independent , with additional interaction tests and tests of proportional hazards using an interaction with time variable for signi cant factors . 
 this trial is registered , number isrctn07355119 . role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results of 3207 patients registered in the trial ( gure 2 ) , 59 were philadelphia chromosome positive : 52 were transferred to esphall and seven to ukall xii . 
on the basis of cytogenetics and early bonemarrow response , 1732 patients were reclassi ed as clinical standard risk , 989 clinical intermediate risk , and 405 clinical high risk ( gure 2 )  . 
all eligible trial patients , with the exception of those who died within 35 days or never achieved remission ( n = 34 ) , were tested for mrd status after interim maintenance , but clinical high - risk patients were not eligible for mrd strati cation and randomisation . 
mrd status was low risk in 1090 ( 35% ) of 3092 patients tested for mrd status , high risk in 1030 ( 33% ) , and indeterminate risk in 972 ( 31% )  . 
 table 1 : baseline characteristics in the trial overall vol 14 march 2013 articles overall survival event - free survival relapse rate number at risk overall survival event - free survival relapse 3126 3126 3092 time ( years ) 2755 2743 2743 2284 2243 2247 1838 1786 1789 1412 1345 1348 1041 figure 3 : event - free survival , relapse , and overall survival in the trial overall number of events actuarial percentage at 5 years ( 95% ci ) induction failure isolated cns relapse any cns relapse non - cns relapse any bone marrow relapse non - bone marrow relapse relapse secondary tumour death in remission * any event death 11% ( 0715 ) 19% ( 1325 ) 30% ( 2238 ) 59% ( 4771 ) 66% ( 5478 ) 23% ( 1729 ) 88% ( 76100 ) 06% ( 0210 ) 27% ( 2133 ) 872% ( 858886 ) 915% ( 903927 ) with censoring at competing events . 
the proportion of patients with an informative mrd result who were mrd low risk or high risk varied by age , white blood cell count , and immunophenotype ( data not shown )  . 
follow - up continued to oct 31 , 2011 , with a median follow - up of 46 months ( iqr 2570 ) for the trial overall and 57 months ( 4272 ) low - risk for randomisation , because this randomisation ceased 2 years before the high - risk randomisation . 
the results of the high - risk randomisation will be reported elsewhere once there has been su cient time for follow - up . patients who underwent of the 3126 patients who were eligible for analyses in the trial overall , a small proportion experienced any event or died in the rst 6 years of follow - up . 
the risk of isolated cns relapse was 18% ( 95% ci 1224 ) for patients with b - lineage all and 32% ( 1252 ) for those with t - lineage all . 
the only subgroup with a fairly high risk of isolated cns relapse was patients with t - lineage all and a white blood cell count of greater than 200 10 per l ( 121% , 95% ci 05237 ) , but only four cns events occurred in 55 such patients . 
secondary tumours occurred in 16 patients ( ve had acute myeloid leukaemia [ one post - relapse ] , one myelodysplasia , two second all , one t - cell lymphoma , one neuroblastoma , two histiocytic sarcoma , one epstein barr virus lymphoma , one ewings sarcoma , one lymphoblastic lymphoma , and one low - grade glioma ) , of whom eight died . 
of the 47 patients who received an allogeneic haemopoietic transplantation , 30 ( 64% ) were alive and relapse free as of oct 31 , 2011 . stem - cell analysis of outcome by leukaemia cytogenetics is in progress and will be reported separately . 
of other prognostic factors , mrd risk status was the single most important determinant of outcome ( appendix ) , with a 5 - year cumulative relapse rate of 40% ( 95% ci 245.6 ) in mrd low - risk patients versus 150% ( 123177 ) in high - risk patients ( log - rank p < 00001 )  . 
older age , high white blood cell count , and t - cell immunophenotype were signi cantly associated with mrd high - risk status ( data not shown )  . 
multivariate cox analyses showed that age , white blood cell count , and mrd risk group were independently associated with relapse - free survival ( table 3 , appendix )  . 
in cox analyses , the e ects of age ( pinteraction = 001 ) and white blood cell count ( pinteraction = 0001 ) , but not mrd ( pinteraction = 009 ) , varied signi cantly during follow - up . 
after 2 years , only mrd was signi cant ( 336 , 197573 ; p < 00001 ) , although more follow - up is needed . we recorded no di erence in efs or relapse risk between mrd low - risk patients whose mrd had become undetectable at day 29 and those with less than 001% mrd at day 29 but became undetectable by week 11 . 
within the mrd high - risk group , 5 - year efs was lower in nci high - risk patients ( 728% , 95% ci 679777 ) than in nci standard - risk patients ( 858% , 821895 ; p < 00001 ; appendix )  . 
 on the basis of review by the chief investigator , 17 deaths were classi ed as having been caused by 204 vol 14 march 2013 articles univariate log rank * univariate cox regression * multivariate ( cox regression ) hazard ratio ( 95% ci ) p value hazard ratio ( 95% ci ) p value hazard ratio ( 95% ci ) p value sex ( female vs male ) 065 ( 049086 ) 0003 064 ( 047086 ) 0003 078 ( 054113 ) 018 age white blood cell count mrd risk ( high vs low ) 184 ( 148230 ) 136 ( 122150 ) 383 ( 272539 ) nci risk group ( high vs standard ) 206 ( 154275 ) immunophenotype ( t vs b ) 247 ( 158384 ) < 00001 < 00001 < 00001 < 00001 00002 109 ( 106111 ) 132 ( 120145 ) 469 ( 304726 ) 201 ( 151268 ) 201 ( 142 285 ) < 00001 < 00001 < 00001 < 00001 < 00001 110 ( 105115 ) 135 ( 117156 ) 402 ( 259625 ) 083 ( 049140 ) 061 ( 034102 ) < 00001 < 00001 < 00001 048 006 mrd = minimal residual disease . 
logarithm of white blood cell count as a continuous variable in cox analyses , with groups of < 1010 per l , 101910 per l , 204910 per l , 509910 per l , 10010 per l . table 3 : prognostic factors for relapse - free survival in the trial overall induction therapy despite having occurred after day 35 , because the onset of the causative event was before that timepoint . 
34 ( 2% ) of 1578 patients who received four drugs during induction ( clinical intermediate or high risk ) died compared with 12 ( 1% ) of 1548 patients who received three drugs ( clinical standard risk ; p = 0001 )  . 
the number of deaths in remission did not di er by clinical risk group ( 21 [ 1% ] of 1536 standard - risk patients , 19 [ 2% ] of 885 intermediate - risk patients , and 11 [ 1% ] of 659 high - risk patients ; p = 035 )  . 
 that were clinical high - risk patients experienced more toxic asparaginase e ects attributable ( hypersensitivity and pancreatitis ) as a result of higher cumulative doses of asparaginase than did standard - risk and intermediate - risk patients ( table 5 , appendix )  . 
the di erence in 5 - year efs was 11% ( 95% ci 56 to 25 ) , which means the primary endpoint of the randomisation ( to rule out a 7% reduction in efs ) was achieved . 
5 - year overall survival the group given one delayed intensi cation ( 979% , 95% ci 9571000 ) and that given two delayed intensi cations ( 985% , 9691000 ) did not di er signi cantly ( or 067 , 95% ci 019230 ; p = 053 )  . 
in the reduced - treatment group , 11 of 260 patients relapsed ( three isolated marrow , four isolated cns , two combined marrow and cns , one testes , and one isolated cervical lymph node )  . 
siadh = syndrome of inappropriate antidiuretic hormone secretion . table 5 : number of speci c toxic e ects by clinical risk groups < 00001 080 091 < 00001 073 < 00001 < 00001 058 045 092 046 035 023 < 00001 002 they received one course of delayed intensi cation . 
the outcome for these patients is included in that reported for the overall mrd low - risk group ( appendix ) , because their follow - up is too short to be analysed separately . 
 discussion the results of our trial show that a reduction of postremission treatment is feasible for children and young adults with all predicted to have a low risk of relapse on the basis of rapid clearance of mrd by the end of induction therapy . 
we have reported a 5 - year efs in the trial overall that is comparable with the benchmark of 856% established in a study of 498 patients.8 a reduction in relapse risk in this study has resulted in a 72% improvement in 5 - year efs compared with our previous trial ( ukall 99 ) , 1 in which only patients aged 18 years or younger were recruited . 
combined with a signi cant reduction in treatment - related mortality , the improved efs resulted in a 4% improvement in 5 - year overall survival to 923% for that age group compared with ukall 99.16 although the improvement was recorded in all risk groups , higher - risk patients bene ted the most , with a 12% improvement in 5 - year efs for nci high - risk patients and an 115% improvement in patients with t - lineage all , 16 leading to a signi cant increase in overall survival for these groups compared with ukall 99.1 the low frequency of isolated and any cns relapse within 5 years is reassuring , and was equivalent to that reported in studies2 , 3 in which a signi cantly higher proportion of patients received cranial irradiation than in our trial . 
 restricted use of cranial radiotherapy combined with a small proportion of patients who received an allogeneic haemopoietic stem - cell transplantation relative to other trials and the absence of etoposide from our treatment one delayed intensication : event - free survival two delayed intensications : event - free survival one delayed intensication : relapse two delayed intensications : relapse number at risk one delayed intensication two delayed intensications time ( years ) figure 4 : event - free survival and relapse in mrd low - risk patients mrd = minimal residual disease . criteria for adverse events grade 3 or 4 toxic e ects in patients given reduced treatment and those given standard treatment did not di er signi cantly ( table 7 )  . 
 however , the second delayed intensi cation course was associated with one ( < 1% ) treatment - related death and 74 episodes of grade 3 or 4 toxic e ects in 45 patients ( 17% ) given standard treatment , of whom 21 had at least one grade 3 or 4 infection . 347 mrd low - risk patients were registered after closure of the low - risk randomisation in august , 2009 ( gure 2 )  . 
 206 vol 14 march 2013 articles one delayed intensi cation ( n = 260 ) two delayed intensi cations ( n = 261 ) number of events actuarial percentage at 5 years ( 95% ci ) number of events actuarial percentage at 5 years ( 95% ci ) unadjusted analyses adjusted analyses * two - sided p value unadjusted odds ratio for group given two delayed intensi cations ( 95% ci ) any event relapse 56% ( 2389 ) 45% ( 1872 ) 100 ( 043231 ) 56% ( 2389 ) 24% ( 0246 ) 055 ( 021143 ) remission death 12% ( 026 ) 740 ( 0777104 ) any death 21% ( 043 ) 15% ( 031 ) 067 ( 019230 ) 099 023 008 053 two - sided p value adjusted odds ratio for group given two delayed intensi cations ( 95% ci ) 109 ( 047253 ) 060 ( 023157 ) 839 ( 0868161 ) 071 ( 021248 ) 084 030 006 061 mrd = minimal residual disease . 
 * adjusted for variables upon which randomisation was balanced : age ( < 10 years vs 10 years ) , sex ( males vs female ) , white blood cell count ( < 5010 per l vs 5010 per l )  . 
 table 6 : events in mrd low - risk patients who underwent randomisation regimens should hopefully reduce the risk of treatmentrelated cancers.17 , 18 the overall outcomes reported here and in other recent trials19 , 20 have been obtained even though no new drugs for treatment of all have been introduced in the past 30 years ; targeted drugs , such as monoclonal antibodies and protein kinase inhibitors , were not available for testing when our trial opened . 
several large randomised clinical trials have shown that dexamethasone has a better e cacy in prevention of systemic and cns relapse than does prednisolone.2123 pegylated asparaginase has better pharmacokinetic24 , 25 and pharmacodynamic properties , 26 and a lower risk of hypersensitivity reactions on reexposure27 than does the native formulation . 
deaths caused by toxic e ects amount to half the deaths reported in our trial so far , although the proportion will diminish with longer follow - up as more patients relapse . 
in a recently concluded european study , aieop - bfm 2000 , 23 twice as many patients in the group given dexamethasone died during the group given than prednisolone ; other studies28 , 29 have had similar results . 
 additionally , dexamethasone might be associated with a higher risk of osteonecrosis than is prednisolone , 29 but that has not been a universal experience.22 , 30 dexamethasone a ects quality of life more than prednisolone does , 31 although the e ect does not persist in the long term.32 dose , scheduling , and interaction with anthracyclines are important determinants of the risk of steroid - associated induction one delayed intensi cation ( n = 260 ) two delayed intensi cations ( n = 261 ) relative risk for group given two delayed intensi cations ( 95% ci ) two - sided p value grade 34 toxic e ect * 189 ( 73% ) 200 ( 77% ) 105 ( 095116 ) serious adverse event 70 ( 27% ) 82 ( 31% ) 117 ( 089153 ) cumulative toxicity 195 ( 75% ) 204 ( 78% ) 104 ( 095115 ) 030 026 039 mrd = minimal residual disease . 
de ned as remission death , grade 34 toxic e ect , or serious adverse event . table 7 : toxic e ects in mrd low - risk patients who underwent randomisation toxic e ects , and we are testing novel schedules of dexamethasone in our next trial in an attempt to reduce the toxic e ects while retaining the e cacy of this drug . 
studies of native escherichia coli asparaginase26 , 33 have reported a frequency of 2040% of hypersensitivity reactions associated with asparaginase intensi cation courses . in view of these toxic e ects , we were pleased to note that treatment reduction is feasible in a substantial subgroup of patients with a low risk of relapse ( panel )  . 
 mrd strati cation identi ed 4050% of patients ( depending on age ) whoirrespective of conventional risk factorshave a chance of surviving to 5 years relapse free of about 95% . 
 whether they also have decreased risk of late cardiac toxic e ects and secondary cancers due to reduced exposure to anthracyclines and alkylating agents ( appendix ) will become apparent only after longer follow - up . 
 after ukall 2003 opened , two us trials34 , 35 also reported no bene t of a second intensi cation course for nci standard - risk and high - risk patients . 
however , treatment was not strati ed by mrd in either trial and the overall vol 14 march 2013 articles panel : research in context systematic review we did not do a formal systematic review when planning this trial . 
the need for the trial and the questions to be answered were determined by a combination of non - systematic literature review , discussions in the national childhood and adult leukaemia clinical study groups and clinician networks , and consultation with experts from the us childrens oncology group and european childhood leukaemia study groups ( eg , french acute lymphoblastic leukaemia group , nordic society of paediatric haematology and oncology , dutch childhood oncology group , associazione italiana ematologia oncologia , and pediatrica - berlin - franklin - munster )  . 
during planning , the evidence base indicated that on - treatment monitoring and detection of submicroscopic levels of leukaemia ( minimal residual disease [ mrd ] ) was the best predictor of relapse risk in children with acute lymphoblastic leukaemia ( all ) , but whether treatment could be modi ed on the basis of mrd response was not known . 
we aimed to establish whether treatment for childhood all could be strati ed by risk of relapse predicted by mrd response . interpretation we have reported an improved outcome for children and young adults with all overall and have shown that postremission therapy can be reduced for a subgroup of patients with rapid clearance of mrd during induction therapy without compromising the cure frequency . 
mrd monitoring should allow clinicians to select patients who have a chance of being cured and might bene t from treatment deescalation to reduce their exposure to the side - e ects of intensive therapy . intensity of treatment di ers signi cantly from our trial . 
 the conclusion of the us trials34 , 35 was that intensi ed interim maintenance with one delayed intensi cation course was the optimum therapy for nci standard - risk and high - risk patients with a rapid morphological early response . 
our trial has extended the previous ndings by establishing that molecular mrd monitoring identi es a large group of patients with a rapid morphological early response who do not require a second delayed intensi cation course or intensi ed interim maintenance treatment to achieve a high chance of event - free survival to 5 years . 
additionally , a small proportion of patients can be identi ed as low risk by karyotype and mrd response by the childrens oncology group criteria ; the remaining subgroups interim maintenance and delayed intensi cation therapy than was used in our protocol . 
an international trial , aieop - bfm 2000 , 7 , 14 has also treatment reduction and intensi cation interventions for mrd high - risk and standard - risk groups , but the results are yet to be reported . 
 we note three main limitations of our study : an informative mrd result was not available for a third of receive more intensive tested can patients enrolled ; median follow - up of mrd low - risk patients was fairly short ; and the reduction in treatment achieved by omitting the second delayed intensi cation is fairly modest . 
we are reasonably con dent that the efs for mrd low - risk patients will remain stable during extended follow - up , because no late relapses in the mrd low - risk group have been reported in the bfm 90 study6 or our retrospective study of all ( unpublished )  . 
 improvements in the quality of samples and ability to nd mrd markers have meant that an informative mrd result is available for 92% of patients in our successor trial ukall 2011 ( isrctn64515327 ) , which opened in april , 2012 , and is testing ways to further reduce risk of treatment - related toxic e ects . 
in future , new drugs36 , 37 designed to target leukaemia - speci c receptors and proteins could replace elements of conventional chemotherapy regimens that are the cause of some of the major toxic e ects , thereby reducing toxicity while retaining overall treatment e cacy . 
 finally , translation of advances in understanding of the molecular biology of all and its e ect on phenotype and clinical outcome3840 will help to de ne speci c subgroups that might bene t from such an approach . 
ng , cm , rh , and cr collected data , analysed data , helped to address queries from local investigators , dealt with treatment di culties , and contributed to the writing of the report . 
rw and sr collected and analysed data and contributed to the writing of the report . con icts of interest we declare that we have no con icts of interest . acknowledgments this trial was supported by grants from leukaemia and lymphoma research ( uk ) and the medical research council ( uk )  . 
we thank the patients and their families who participated in these trials and the study pharmacists , nurses , and clinicians who supported thewe also thank all the laboratory sta for providing timely and accurate minimal residual disease results for patients . 
 articles systemic chemotherapy with or without cetuximab in patients with resectable colorectal liver metastasis : the new epoc randomised controlled trial john primrose , stephen falk , meg finch - jones , juan valle , derek oreilly , ajith siriwardena , joanne hornbuckle , mark peterson , myrddin rees , tim iveson , tamas hickish , rachel butler , louise stanton , elizabeth dixon , louisa little , megan bowers , sin pugh , o james garden , david cunningham , tim maughan , john bridgewater summary background surgery for colorectal liver metastases results in an overall survival of about 40% at 5 years . 
the addition of cetuximab to these chemotherapy regimens results in an overall survival advantage in patients with advanced disease who have the kras exon 2 wild - type tumour genotype . 
we aimed to assess the bene t of addition of cetuximab to standard chemotherapy in patients with resectable colorectal liver metastasis . methods patients with kras exon 2 wild - type resectable or suboptimally resectable colorectal liver metastases were randomised in a 1 : 1 ratio to receive chemotherapy with or without cetuximab before and after liver resection . 
 randomisation was done using minimisation with factors of surgical centre , poor prognostic tumour ( one or more of : 4 metastases , n2 disease , or poor di erentiation of primary tumour ) , and previous adjuvant treatment with oxaliplat chemotherapy consisted of oxaliplatin 85 mg / m intravenously over 2 h and uorouracil bolus 400 mg / m intravenously over 5 min , followed by a 46 h infusion of uorouracil 2400 mg / m repeated every 2 weeks ( regimen one ) or oxaliplatin 130 mg / m intravenously over 2 h and oral capecitabine 1000 mg / m twice daily on days 114 repeated every 3 weeks ( regimen two )  . 
cetuximab was given as an intravenous dose of 500 mg / m every 2 weeks with regimen one and three or a loading dose of 400 mg / m followed by a weekly infusion of 250 mg / m with regimen two . 
this trial is registered , isrctn22944367 . findings 128 kras exon 2 wild - type patients were randomised to chemotherapy alone and 129 to chemotherapy with cetuximab between feb 26 , 2007 , and nov 1 , 2012 . 
the median follow - up was 211 months ( 95% ci 126338 ) in the chemotherapy alone group and 198 months ( 122287 ) in the chemotherapy plus cetuximab group . 
with an overall median follow - up of 207 months ( 95% ci 179256 ) and 123 ( 58% ) of 212 required events observed , progression - free survival was signi cantly shorter in the chemotherapy plus cetuximab group than in the chemotherapy alone group ( 141 months [ 95% ci 118159 ] vs 205 months [ 95% ci 168267 ] , hazard ratio 148 , 95% ci 104212 , p = 0030 )  . 
the most common grade 3 or 4 adverse events were low neutrophil count ( 15 [ 11% ] preoperatively in the chemotherapy alone group vs six [ 4% ] in the chemotherapy plus cetuximab group ; four [ 4% ] vs eight [ 8% ] postoperatively ) , embolic events ( six [ 4% ] vs eight [ 6% ] preoperatively ; two [ 2% ] vs three [ 3% ] postoperatively ) , peripheral neuropathy ( six [ 4% ] vs one [ 1% ] preoperatively ; two [ 2% ] vs four [ 4% ] postoperatively ) , nausea or vomiting ( four [ 3% ] vs six [ 4% ] preoperatively ; four [ 4% ] vs two [ 2% ] postoperatively ) , and skin rash ( two [ 1% ] vs 21 [ 15% ] preoperatively ; 0 vs eight [ 8% ] postoperatively )  . 
there were three deaths in the chemotherapy plus cetuximab group ( one interstitial lung disease and pulmonary embolism , one bronchopneumonia , and one pulmonary embolism ) and one in the chemotherapy alone group ( heart failure ) that might have been treatment related . interpretation addition of cetuximab to chemotherapy and surgery for operable colorectal liver metastases in kras exon 2 wild - type patients results in shorter progression - free survival . 
this bene t was supported by the epoc study , 4 which randomly assigned 364 patients with resectable metastases to surgery alone , or surgery with neoadjuvant chemotherapy , and showed an improvement in 3 - year progression - free survival of vol 15 may 2014 lancet oncol 2014 ; 15 : 60111 published online april 7 , 2014 s1470 - 2045 ( 14 ) 70105 - 6 this online publication has been corrected . 
 in the long - term analysis of this study5 5 - year overall survival was 512% ( 95% ci 436583 ) in the perioperative chemotherapy group versus 478% ( 403550 ) in the surgery - only group . 
although this bene t was small , neoadjuvant therapy was established as a treatment option for patients with operable liver metastasis and formed the basis for this and other studies.6 cetuximab ( merck kgaa , darmstadt , germany ) is a monoclonal antibody to egfr with activity in kras exon 2 wild - type colorectal cancer as a single agent.7 after promising phase 2 data , 8 several studies assessed the bene t of cetuximab and panitumumab , a similar antibody , in combination with chemotherapy.913 in 2005 , the coin trial14 was initiated to investigate the addition of cetuximab to oxaliplatin and uoropyrimidine chemotherapy in rst - line treatment of advanced colorectal cancer . 
the new epoc trial was begun as a rational extension to the coin study , 14 the epoc study , and supportive phase 2 data , 8 using much the same investigational strategies to assess whether the addition of cetuximab to oxaliplatin uoropyrimidine chemotherapy improved outcomes for patients with operable liver metastasis . methods participants eligible patients were 18 years or older with a who performance status of 2 or less , and resectable or suboptimally resectable colorectal liver metastasis without detectable extrahepatic distant metastatic disease . 
after 22 patients had been accrued , data15 supporting a bene t of cetuximab only in kras exon 2 wild - type tumours were presented , leading to a protocol who performance status 0 or 1 128 ( 100% ) 126 ( 98% ) age ( years ) women primary tumour t3 or t4 n1 or n2 poorly di erentiated unresected 13 liver metastases one metastasis > 3 cm synchronous metastases chemotherapy alone ( n = 128 ) chemotherapy plus cetuximab ( n = 129 ) 80 ( 63% ) 48 ( 38% ) 92 ( 71% ) 37 ( 29% ) 107 ( 84% ) 109 ( 84% ) 82 ( 64% ) 10 ( 8% ) 13 ( 10% ) 102 ( 80% ) 64 ( 50% ) 60 ( 47% ) 78 ( 60% ) 15 ( 12% ) 18 ( 14% ) 97 ( 75% ) 73 ( 57% ) 68 ( 53% ) 33 ( 26% ) 6 ( 5% ) carcinoembryonic antigen > 30 ng / l 31 ( 24% ) extrahepatic disease 3 ( 2% ) table 1 : characteristics of randomised patients at baseline in kras exon 2 wild - type patients only amendment on july 8 , 2008 , approved by the trial steering committee , to exclude kras mutated patients . 
two resections were staged in the chemotherapy alone group and four resections were staged in the chemotherapy plus cetuximab group . table 3 : surgical information and postoperative complications in kras exon 2 wild - type patients only correspondence to : prof john primrose , university surgery , southampton general hospital , southampton so16 6yd , uk j.n.primrose@soton.ac.uk ( r0 resection ) , or judged to be resectable . 
previous adjuvant chemotherapy was permitted if completed 6 months or more before trial entry and previous rectal chemo radiotherapy was permitted if completed 1 month or more before trial entry . 
there was no limit to the number of metastases , and patients if they had suboptimally resectable were eligible metastases ( ie , with potentially compromised resection margins , but to be treated with curative intent )  . less a personal or the following patients were excluded : those with any uncontrolled medical comorbidity likely to interfere with treatment or assessment of response ; any psychiatric or neurological disorder a ecting ability to consent or comply with medication ; partial or complete bowel obstruction ; pre - existing peripheral neuropathy of grade 1 or higher according to common toxicity criteria ; those with family history of dihydropyrimidine dehydrogenase de ciency , gilberts syndrome , or other congenital abnormality of biliary transport ; than those with platelet counts 100 10 cells per l , an absolute neutrophil count less than 15 10 cells per l , serum bilirubin greater than one and a quarter times the upper limit of normal ( uln ) , or alkaline phosphatase greater than ve times the uln ; serum aminotransferase ( either aspartate amino transferase or alanine aminotransferase ) greater than two and a half times the uln ; estimated creatinine clearance ( by cockcroft formula ) of less than 50 ml / min , or measured glomerular ltration rate of less than 50 ml / m patients with another previous or current malignant disease which , in the judgement of the treating investigator , was likely to interfere with new epoc treatment or assessment of response were also excluded . 
 written informed consent was obtained from all patients before random assignment . randomisation and masking patients were randomly assigned in a 1 : 1 ratio to chemotherapy alone or chemotherapy plus cetuximab . 
 treatment assignments were made over the telephone by the medical research council clinical trials unit with the use of randomised minimisation factors ( full details are provided in appendix p 8 )  . 
a protocol amendment was then implemented on april 22 , 2009 , to condense the strati cation factors to surgical centre , poor prognostic tumour ( one or more of : 4 metastases , n2 disease , or poor di erentiation of primary tumour ) , and previous treatment with oxaliplatin as adjuvant since it was felt by the trial management group that the initial large number of strati cation factors would be less e ective at achieving balance between the treatment groups , in addition to being logistically complicated . 
there was no masking of either investigators or patients to treatment allocation . procedures patients were randomly assigned to chemotherapy with or without cetuximab for 12 weeks , followed by surgery and 604 vol 15 may 2014 articles to receive then a further 12 weeks of chemotherapy with or without cetuximab . 
the chemotherapy backbone was oxaliplatin ( 85 mg / m intravenously over 2 h ) and uorouracil ( 400 mg / m bolus intravenously over 5 min ) followed by a 46 h infusion of uorouracil 2400 mg / m repeated every 2 weeks ( regimen one ) or oxaliplatin 130 mg / m intravenously over 2 h and oral capecitabine 1000 mg / m twice daily on days 114 repeated every 3 weeks ( regimen two )  . 
patients who had received oxaliplatin irinotecan as adjuvant were permitted 180 mg / m intravenously over 30 min with uorouracil as above instead of oxaliplatin ( regimen three )  . 
cetuximab was given as an intravenous dose of 500 mg / m every 2 weeks with regimen one and three , or a loading dose of 400 mg / m followed by a weekly infusion of 250 mg / m with regimen two as previously described.12 the dose of capecitabine in the regimen two group was reduced to 850 mg / m from 1000 mg / m twice daily after toxicity concerns in the coin study14 , 16 which used an identical schedulethis amendment was made on july 24 , 2007 , and was approved by the trial steering committee . 
 subsequent concerns about poor outcome in the regimen two group in the coin study led to an exclusion of capecitabine in combination with cetuximab in the present study17 on july 28 , 2010 , and this amendment was also approved by the trial steering committee . full details of permitted dose reductions and interruptions are available in the protocol . 
 if further surgery was needed , such as resection of the primary tumour or the second phase of a staged liver resection , it was done before adjuvant chemotherapy and within 24 weeks of rst surgery . 
the planned use of ablative techniques was not allowed , but these techniques could be used if clinically indicated at the time of operation . to verify whether surgery was compliant with the protocol , all les were reviewed to compare sites of disease documented at baseline , and on the surgery forany discrepancies were queried directly with either the operating surgeon , or the lead surgeon for that site . in solid tumors ct or mri scans were done to assess response evaluation criteria ( recist ) version 1.018 before systemic treatment , every 3 months for 2 years , and every 6 months for a further 3 years until progression , or death . 
criteria for treatment to be discontinued were : progression while on illness therapy ; unacceptable preventing further treatment ; withdrawal of consent for intercurrent toxicity ; a progression - free survival hr 148 , 95% ci 104212 , p = 003 chemotherapy alone chemotherapy plus cetuximab number at risk chemotherapy chemotherapy plus cetuximab b overall survival hr 149 , 95% ci 086260 , p = 016 chemotherapy alone chemotherapy plus cetuximab time since randomisation ( months ) number at risk chemotherapy chemotherapy plus cetuximab figure 2 : kaplan - meier curves of progression - free survival ( a ) and overall survival ( b ) by treatment group in kras exon 2 wild - type patients only for the study protocol see protocols / new_epoc_protocol . see online for appendix treatment by the patient ; or any alterations in the patients condition which justi ed the discontinuation of treatment in the investigators opinion . for biomarker analysis , formalinxed , para nembedded tumour samples were sectioned and stained with haematoxylin and eosin to establish the regions of highest tumour nuclei content . 
pcr was done in 25 l reactions using 20 ng dna , megamix - gold bu er ( microzone , haywards heath , uk ) , and 10 pm / l primers . 
thermocycling was done at 95c for 10 min , followed by 3438 cycles of 95c for 30 s , 60c for 30 s , and 72c for 30 s , followed by a nal extension of 72c for 10 m 15 l of each pcr product was used for pyrosequencing . 
the primary analysis was unadjusted and sensitivity analyses were done adjusting the model for the minimisation factors and other prognostic factors . all analyses reported here include data up to nov 1 , 2012 , to match the timeframe presented in the interim report to the data monitoring and ethics committee . 
all analyses , except safety , were done on a modi ed intention - to - treat basis , including all patients with known kras exon 2 wild - type genotype who had reached the timepoint for perioperative assessment of response and recist assessment . 
 jp and sp had full access to the raw data , as did the university of southampton clinical trials unit , and were responsible for all data collection and analysis . 
the corresponding author had nal responsibility for the decision to submit for publication . favours chemotherapy and cetuximab favours chemotherapy alone figure 3 : hrs for progression - free survival with chemotherapy alone versus chemotherapy and cetuximab , according to prespeci ed subgroups the subgroups are based on baseline characteristics . 
an additional 14 patients ( six in the chemotherapy alone group and eight in the chemotherapy plus cetuximab the group ) , who were randomly assigned before amendment necessitating kras testing and were retrospectively shown to be kras mutant or indeterminate , were excluded from all analyses except the safety analyses . 
14 kras exon 2 wild - type patients were excluded from the primary analysis population because they had not reached the timepoint for assessment of preoperative response by nov 1 , 2012 , and three did not have the recist assessment before that date as expected . 
as such , the primary analysis population consisted of 236 patients . the baseline characteristics of most patients received chemotherapy regimen one ( 87 [ 68% ] of 128 patients in the chemotherapy alone group vs 87 [ 67% ] of 129 patients in the chemotherapy plus cetuximab group ) , with smaller numbers receiving regimen two ( 27 [ 21% ] vs 24 [ 19% ] , respectively ) and regimen three ( 11 [ 9% ] vs 15 [ 12% ] , respectively )  . 
93 ( 73% ) of 128 patients in the chemotherapy alone group completed 12 weeks of preoperative chemotherapy compared with 98 ( 76% ) of 129 patients in the chemotherapy plus cetuximab group . 
at the time of analysis , 47 of 100 ( 47% ) patients in the chemotherapy alone group who had surgery and 49 of 98 ( 50% ) patients in the chemotherapy plus cetuximab group who had surgery had completed 12 weeks of postoperative chemotherapy ( appendix pp 14 show details of relative dose intensity [ both preoperative and postoperative ] )  . 
13 of 100 ( 13% ) patients in the chemotherapy alone group and 16 of 98 ( 16% ) in the chemotherapy plus cetuximab group did not complete postoperative chemo therapy . 
198 patients had an operation ; 93 ( 93% ) of 100 patients in the chemotherapy alone group and 85 ( 87% ) of 98 patients in the chemotherapy plus cetuximab group proceeded to resection . 
preoperative chemotherapy period is the start of cycle 1 to the start of the last preoperative cycle , plus 3 weeks for patients receiving chemotherapy regimen 1 or 3 , or plus 4 weeks for patients receiving chemotherapy regimen 2 . 
a fishers exact test showed the di erence in skin rash rates between groups was signi cant : two - sided p = 00017 for preoperative period , p = 00071 for postoperative period . 
||postoperative chemotherapy period is the start of the rst postoperative chemotherapy cycle to the start of the last postoperative cycle , plus 3 weeks for patients receiving chemotherapy regimen 1 or 3 , or plus 4 weeks for patients receiving chemotherapy regimen 2 . table 4 : adverse events according to common toxicity criteria for adverse events , strati ed by time of occurrence ( preoperative vs postoperative chemotherapy period ) and by worst grade experienced group were not resected or ablated because of a nding of progressive disease or a complete response at the time of surgery . 
24 patients , ten ( 9% ) of 110 patients in the chemotherapy alone group and 14 ( 13% ) of 112 patients in the chemotherapy plus cetuximab group did not have surgery . 
there were no signi cant di erences between the groups in terms of the surgical procedures donespeci cally , no fewer resections were done in the cetuximab group because of the numerically greater number of responses in this group . median follow - up was 211 months ( 95% ci 126338 ) in the chemotherapy alone group and 198 months ( 122287 ) in the chemotherapy plus cetuximab group . 
 with an overall median follow - up of 207 months ( 95% ci 179256 ) and 123 ( 58% ) of the required 212 events identi ed ( 56 events in the chemotherapy alone group and 67 events in the chemotherapy plus cetuximab group ) , median progression - free survival was 141 months ( 95% ci 118159 ; gure 2a ) in the group receiving chemotherapy with cetuximab compared with 205 months ( 95% ci 168267 ) in the chemotherapy alone group ( hr 148 , 95% ci 104212 , p = 0030 )  . 
median overall survival ( gure 2b ) was 391 months ( 95% ci 236not reached ) in the chemotherapy plus cetuximab group , but had not been reached in the chemotherapy alone group ( lower limit 320 months , hr 149 , 95% ci 086260 , p = 016 )  . treated with those patients to explore this unexpected nding of detriment with chemotherapy plus cetuximab , subgroup analyses were done on the basis of prede ned characteristics ( gure 3 )  . 
 the adverse e ect of cetuximab was associated with characteristics normally deemed to be good prognostic featuresie , well or moderate di erentiation in the primary tumour , three or fewer metastases , absence of n2 disease , and non - synchronous presentation . 
median progression - free survival in patients showing a tumour response to systemic treatment was 205 months ( 95% ci 112355 ) in the chemotherapy alone group compared with 141 months ( 95251 ) in those receiving cetuximab ( hr 152 95% ci 095244 , p = 0082 ; appendix p 7 ) , suggesting there was a poor association between progression - free survival and response . the di erence the overall incidence of grade 3 and 4 adverse events , both preoperatively and postoperatively , was much the same between the groups with a non - signi cantly higher incidence in the chemotherapy plus cetuximab group ( preoperative 64 of 137 [ 40% ] ; postoperative 29 of 105 [ 28% ] vs 22 of 104 [ 21% ] )  . 
this to skin rash di erence was primarily attributable ( preoperative 21 of 137 [ 1% ] , p = 00017 ; postoperativeeight of 105 ( 8% ) vs none of 104 , p = 00071 ; full toxicity is shown in table 4 )  . 
the number of patients needing at least one dose modi cation was much the chemotherapy alone and the same between [ 15% ] vs two of 134 [ 47% ] vs 54 of 134 608 vol 15 may 2014 articles chemotherapy plus cetuximab groups ( 49 of 128 vs 53 of 129 in the preoperative chemotherapy period and 35 of 100 vs 38 of 98 in the postoperative chemotherapy period , respectively ) and seven patients in the chemotherapy alone group and nine in the chemotherapy plus cetuximab group discontinued treatment because of toxicity . 
there were three deaths from respiratory causes ( one interstitial lung disease and pulmonary embolism , one bronchopneumonia , and one pulmonary embolism ) in the chemotherapy plus cetuximab group that might have been related to treatment . 
in the chemotherapy alone group , there was one death from heart failure that might have been treatment related . discussion this trial examined the bene t of cetuximab in kras exon 2 wild - type patients with colorectal liver metastases treated with curative intent . 
the study demonstrates that the addition of cetuximab to chemotherapy seems to be detrimental , and although only a proportion ( 58% ) of the required events have occurred , further follow - up and more events are unlikely to modify this outcome . 
 indeed , this interim analysis is likely to be the most accurate re ection of the study intervention since all patients in the chemotherapy plus cetuximab group stopped receiving cetuximab as of nov 1 , 2012 . 
systemic the detriment identi ed with the addition of cetuximab is likely to be related to the e ect of egfr inhibition because the two main confounding variables , systemic treatment delivery and surgery , were well balanced between treatment delivery , including cetuximab , was much the same as in similar studies20 , 21 and did not seem to be compromised by overlapping toxicities as previously described ( panel )  . 
possible explanations include interactions between cetuximab and the chemotherapy backbone , further mutations in the egfr pathway conferring insensitivity to egfr inhibition , and upregulation of alternative signalling pathways combination with surgery . 
it has been proposed that the interaction between oxaliplatin and cetuximab potentially negative because cetuximab may protect against free radical damage by platinum drugs.25 in support of this theory , the irinotecan - based9 , 12 , 26 and single - agent studies7 , 27 , 28 are predominantly positive . 
 panel : research in context systematic review liver surgery can result in long - term survival in patients with colorectal liver metastases.1 , 3 a formal systematic review on perioperative chemotherapy in patients with operable colorectal liver metastases was not undertaken because only one adequately powered trial exists.4 this study showed that perioperative chemotherapy improves progression - free survival in patients with operable colorectal liver metastases . 
 egfr inhibition in kras exon 2 wild - type cancer improves response rate , progression - free survival , and overall survival in some13 , 22 , 27 but not all14 , 23 studies in patients with advanced disease . interpretation the negative outcome in this study does not result from overlapping toxicities as previously described , 21 nor di erences in surgical management . 
possible explanations include the need for improved biomarker de nition of patients , 22 chemotherapy interaction , or a modi cation of the biomarker environment after systemic therapy or surgery ; these reasons need further investigation . 
 the use of cetuximab in patients with operable colorectal cancer liver metastases should be deemed contraindicated outside clinical trials , and work to establish a biological explanation for this surprising result is needed . importantly , patients who have a kras mutation and are treated with an egfr inhibitor have an inferior outcome in the oxaliplatin - based studies11 , 22 compared with patients in irinotecan - based studies who had a similar outcome to chemotherapy - only controls.29 the analysis of only the patients in the present study who received an oxaliplatinbased backbone is very similar to the primary study outcome ; however , too few patients received irinotecan to draw any conclusions about this combination . 
a clear understanding of the biological mechanism underlying the detriment identi ed is needed before another neoadjuvant cetuximab study is done in this patient population . it is di cult to extend the outcomes from a neoadjuvant strategy to either adjuvant treatment30 , 31 or treatment in advanced disease13 because of the potential confounding variables inherent in a neoadjuvant strategy ( mainly due to surgery , and the associated treatment interval )  . 
there might also be biological di erences between micrometastatic disease ( the adjuvant studies have been negative30 ) and macroscopic metastatic disease ( most advanced disease studies are positive7 , 12 , 13 ) in terms of response to egfr inhibition . 
biomarker analysis in the petacc - 3 study32 has shown the heterogeneity of patients in terms of their molecular and baseline characteristics , as well as their clinical outcomes . vol 15 may 2014 articles additional mutations in the egfr pathway , namely braf and nras , predict an absence of bene t of cetuximab33 in advanced disease studies27 but are unlikely to explain the inferior progression - free survival of cetuximab patients in the present study who showed a tumour response . 
it is possible that mutations might have arisen after treatment with cetuximab , or that resistance to egfr inhibition might result from activation of parallel pathways such as the met receptor tyrosine kinase , 3437 stimulated after liver surgery . 
translational studies examining these possibilities are in progress . the present study is a reminder that combining biological agents with chemotherapy using a suboptimal selection strategy is overly simplistic , and potentially detrimental for patients . 
it is clear that kras mutated patients were unlikely to bene t from cetuximab but this level of selection was insu cient to demonstrate a cohort who might bene t from cetuximab therapy . 
a so - called one size ts all strategy might have seemed rational when a uoropyrimidine was the only systemic agent available , but fails us when we use targeted agents . 
the nding that patients who have a better prognosis seem to do less well with the addition of cetuximab adds complexity to this trial result . in summary , cetuximab in combination with chemotherapy cannot be recommended for patients with operable colorectal liver metastases . 
further translational studies are needed to establish whether egfr inhibition could have a role in this setting . contributors jp and jb conceived the study , designed the protocol , supervised the conduct and analysis of the trial , and cowrote the report . 
tm designed the protocol with jp and jb and was a member of the trial management group and as such supervised the conduct of the trial ; he commented on all drafts of the report and approved the nal version . 
sf , mf - j , jv , dor , as , jh , mp , mr , ti , and th recruited patients and oversaw the conduct of the trial at participating centres ; they commented on drafts of the report and approved the nal version . 
ojg and dc were members of the trial management group and as such supervised the conduct of the trial ; they commented on all drafts of the report and approved the nal version . declaration of interests jp has attended advisory boards for merck , bayer , and sano - aventis . 
th has received research funding from roche , amgen , sano - aventis , and novartis . acknowledgments this research study was funded by cancer research uk and supported by the national cancer research institute via the national cancer research network . 
jb is funded partly from the national institute for health research biomedical research centres at university college london hospitals and dc is funded partly from the royal marsden and institute of cancer research . correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections comment published online april 16 , 2014 s1470 - 2045 ( 14 ) 70177 - 9 see articles page 620 time will show whether the results reported by zhu and colleagues2 can be achieved in other centres and whether this technique will become an accepted palliative treatment option . 
regional di erences in infrastructure , expertise , and health - care economics will continue to be essential factors as clinicians tailor appropriate therapy for patients with advanced oesophageal cancer . russell e white tenwek hospital , box 39 , bomet , 20400 , kenya russ.white@wgm.org i declare that i have no competing interests . 
health economic evaluation of stent or endoluminal brachytherapy as a palliative strategy in patients with incurable cancer of the oesophagus or gastro - oesophageal junction : results of a randomized clinical trial . 
eur j gastroenterol hepatol 2005 ; 17 : 136977 . setting the bar for adjuvant treatment of melanoma there is universal agreement about the need to improve adjuvant treatment for patients who have melanoma and are at high risk of disease recurrence after surgery.1 , 2 medical management of metastatic melanoma has improved greatly , with the approval of four new drugs that have shown clear survival bene ts phase 3 randomised trials , beginning with the approvals of ipilimumab and vemurafenib in 2011 . 
the american society of clinical oncology has published guidance that aims to improve the standard of clinical trials in metastatic breast , colon , lung , and pancreatic cancers by setting where a higher bar for treatment expectations.3 should the bar then be set for clinical trials of adjuvant treatment in patients with melanoma ? how do the results of the avast - m trial , 4 which assessed the role of bevacizumab as adjuvant treatment for patients with stage iii melanoma at high risk of recurrence , help inform our deliberations ? the availability of new drugs with clear e ects on metastatic melanoma provides a strong rationale for their investigation in adjuvant trials . 
 avast - m began before the approval of ipilimumab and vemurafenib , but even today there is little evidence from trials in metastatic disease to suggest that adjuvant bevacizumab would be bene cial in patients with melanoma . 
 moreover , adjuvant use of bevacizumab has not improved survival in patients with any other tumour type to date.6 dosage is also an important consideration : the avast - m investigators studied bevacizumab given at a dose of 75 mg / kg whereas other studies have assessed bevacizumab given at a dose of 1015 mg / kg , which could have a ected the results . 
future adjuvant trials in patients with melanoma need a strong rationale and design , but whether known e cacy of the agent in in metastatic melanoma is an absolute requirement for successful adjuvant therapy remains to be de ned . the choice of overall survival as the primary endpoint of the avast - m study was clearly an appropriate one , with no signi cant di erence noted between patients in the bevacizumab group and those in the observation group ( hazard ratio [ hr ] 097 , 95% ci 078122 ; p = 076 )  . 
the suitability of relapse - free survival as the primary endpoint in melanoma adjuvant trials bears further scrutiny : does having drugs that improve overall survival in patients with stage iv melanoma negate the value of relapse - free survival in the adjuvant setting , or might rapidly evolving and improving treatment vol 15 may 2014 comment importance of strategies actually accentuate the delaying recurrence ? when relapse - free survival is used as a primary or key secondary endpoint , the investigational agent should be compared with the standard already set by interferon . 
previous studies7 , 8 of adjuvant interferon have shown improvements in relapse - free survival in the range of 1338% , and results for relapse - free survival from the ipilimumab adjuvant trials ( clinicaltrials.gov , numbers nct00636168 and nct01274338 ) are eagerly awaited . 
 in the avast - m trial , disease - free interval was in the bevacizumab group in patients improved compared with those in the observation group ( hr 083 , 95% ci 070098 ; p = 003 )  . 
disease - free interval is subtly di erent from relapse - free survival because deaths due to non - melanoma causes are not included in its calculation ; as such , relapse - free survival should remain the standard relapse endpoint for trials of adjuvant melanoma . 
even if we assume that relapsefree survival was improved by the same amount as disease - free interval in the avast - m trial , and that this improvement was statistically signi cant , bevacizumab does not surpass the e ectiveness of interferon su ciently enough to justify its use in clinical practice . in the preplanned interim analysis of avast - m , patients in the bevacizumab group with braf mutant melanoma had a longer disease - free interval than did those in the observation group , whereas no di erence was noted between groups for patients with braf wild - type melanoma . 
enthusiasm for this observation should be tempered by the nding that the test for interaction between treatment and braf status was not signi cant ( p = 010 ) .4 furthermore , a phase 2 study of bevacizumab plus temozolomide chemotherapy in patients with metastatic melanoma showed the opposite resultbetter survival for braf wild - type melanoma.9 either way , the rationale for improved outcomes for patients given bevacizumab in mutationde ned subsets is not well elucidated , and would need further study in prospective trials prior to acceptance as established fact . 
 interferon is the only approved adjuvant treatment for resected melanoma , with several studies showing improvement in relapse - free survival7 , 8 and meta - analyses showing small improvements in overall survival , 2 thus setting the bar for future adjuvant trials . 
adjuvant bevacizumab has not yet improved overall survival , and although disease - free interval is statistically improved in the avast - m trial , its bene ts seem to be , at best , similar to the relapse - free - survival bene t of interferon . 
other variables should also be considered , such as patient selection and toxic e ects ( of note , only 361 [ 54% ] of 652 patients completed the planned treatment , with unacceptable toxic e ects nearly as common as disease recurrence as a reason for discontinuation ) , and balanced with the observed e cacy . 
adjuvant interferon in melanoma : is duration of therapy important ? j clin oncol 2014 ; 32 : 17173 . 2 mocellin s , lens mb , pasquali s , et al . 
adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomized controlled phase 3 study . 
ann oncol 2011 ; 23 : 53136 . 548 vol 15 may 2014 correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections articles docetaxel and atrasentan versus docetaxel and placebo for men with advanced castration - resistant prostate cancer ( swog s0421 ) : a randomised phase 3 trial david i quinn , catherine m tangen , maha hussain , primo n lara jr , amir goldkorn , carol m moinpour , mark g garzotto , philip c mack , michael a carducci , j paul monk , przemyslaw w twardowski , peter j van veldhuizen , neeraj agarwal , celestia s higano , nicholas j vogelzang , ian m thompson jr summary background the endothelin pathway has a role in bone metastases , which are characteristic of advanced prostate cancer . 
we therefore assessed its e ect on survival in patients with castration - resistant prostate cancer with bone metastases . methods in a double - blind phase 3 trial , men with metastatic castration - resistant prostate cancer , strati ed for progression type ( prostate - speci c antigen or radiological ) , baseline pain , extraskeletal metastases , and bisphosphonate use , were randomly assigned in a 1 : 1 ratio to docetaxel ( 75 mg / m every 21 days , intravenously ) with atrasentan ( 10 mg / day , orally ) or placebo for up to 12 cycles and treated until disease progression or unacceptable toxicity . 
median pfs was 92 months ( 95% ci 8599 ) in the atrasentan group and 91 months ( 84102 ) in the placebo group ( hazard ratio 102 , 089116 ; p = 081 )  . 
median overall survival was 178 months ( 164198 ) in the atrasentan group versus 176 months ( 164201 ) in the placebo group ( 104 , 090119 ; p = 064 )  . 
278 ( 57% ) of 492 patients in the atrasentan group had grade 3 and greater toxicity compared with 294 ( 60% ) of 486 in the placebo group ( p = 022 )  . 
three deaths in the atrasentan group and seven in the placebo group were judged to be possibly or probably due to protocol treatment . interpretation atrasentan , when added to docetaxel , does not improve overall survival or pfs in men with castrationresistant prostate cancer and bone metastases ; therefore , single - agent docetaxel should remain as one of the standard treatments . funded national cancer institute , sano - aventis , and abbott laboratories . introduction prostate cancer is an androgen - dependent disease . 
subsequent treatment with docetaxel prolonged overall survival without a reduction in quality of life compared with palliative mitoxantrone in two studies of patients with castration - resistant prostate cancer , 2 , 3 resulting in docetaxel becoming the standard of care for this cancer . in addition to the characteristic androgen dependence , prostate cancer has other distinguishing features . 
more than 90% of men with fatal prostate cancer have bone metastases.4 the endothelin pathway was delineated as being crucial for the initiation and maintenance of bone metastases from prostate cancer.5 , 6 increased endothelinreceptor a expression was also noted with advanced tumour stage and grade in primary and metastatic prostate cancer.5 endothelin 1 and endothelin receptor a interaction is crucial for stimulation by prostate cancer cells of osteoblast proliferation and migration and production of osteoblastic metastases.7 subsequently , small molecule inhibitors of this interaction were developed and showed inhibition of the development and progression of metastases in preclinical models.8 results from single agent trials of orally bioavailable small molecule inhibitors , such as atrasentan and zibotentan , suggested activity against prostate cancer , particularly in patients with bone metastases . 
patients were eligible if they had pathologically con rmed prostate adeno carcinoma with evidence of bone metastases on a bone scan , judged to be unresponsive or refractory to hormone treatment ( despite androgen deprivation and antiandrogen withdrawal ) according to one or more of the following criteria : progression of one - dimensionally measurable disease that was assessed within 28 days before registration ; progression of evaluable but not measurable disease ( ie , bone scan ) assessed within 42 days before registration ; rising psa concentration , de ned as at least two consecutive increases relative to a reference value ( measurement 1 )  . 
the patient had to have a psa concentration of at least 5 g / l ( 5 ng / ml ) in addition to increasing concentrations of psa to be eligible . no minimum psa concentration was required for patients with progression according to measurable or non - psa - evaluable disease . 
if the bone scan result was judged to be equivocal then mri was used to discriminate between malignant and other causes of bone scan abnormality . patients were required to have undergone surgical or medical castration with a serum testo sterone concentration of less than 17 nmol / l ( 50 ng / ml ) before enrolment . 
if luteinising hormone - releasing hormone ( lhrh ) agonists were used for the chemically induced castration , then the patient should be willing to continue the use of lhrh agonists . 
if non - steroidal antiandrogens ( utamide , bicalutamide , nilutamide , or ketoconazole ) were used , the drugs had to be stopped at least 28 days before the patient was enrolled . 
one previous systemic treatment ( vaccine or biological ) was allowed and at least 28 days had to have elapsed since completion of treatment and the patient recovered from all side - e ects . 
completion of a baseline quality - of - life questionnaire for men who could complete it in english or spanish was a requirement , and patients were o ered the opportunity to participate in correlative studies . exclusion criteria included brain metastases , active infection , and clinically signi cant ascites or pleural e usions . all patients provided written informed consent . 
 the study protocol was approved by the institutional review board or the national cancer institute central institutional review board , or both . type factorsprogression randomisation and masking patients were randomly assigned in a ratio of 1 : 1 to either atrasentan ( 10 mg / day , orally ) or matching placebo at the swog statistical center , seattle , wa , usa . 
the randomisation was dynamically balanced for four strati cation ( psa or radiological ) , baseline pain , extraskeletal metastases , and bisphosphonate usewith the method of pocock and simon.14 the department of veterans a airs cooperative studies program clinical research pharmacy coordinating center , albuquerque , nm , usa , was in charge of drug distribution . 
patients , local research team ( treating physician , research team , and pharmacist ) , data coordinator and study coordinator ( ie , those assessing outcomes ) , but not the study statistician , were masked to treatment assignment . 
no formal assessment of the adequacy of the masking was undertaken . serotonin treatment all patients received docetaxel ( 75 mg / m every 21 days , intravenously ) with dexamethasone ( per institutional guidelines ) , ( 5ht3 ) - receptor antagonist antiemetic treatment , and prednisone ( 5 mg twice daily , orally )  . 
progression con rmed by bone scan required development of de nitive new lesions on a bone scan , with the development of further new lesions on a subsequent bone scan undertaken not less than 6 weeks after the rst scan . 
pain progression was de ned as a two - point increase15 in the brief pain inventory scale for worst pain score , 16 or increased opioid analgesia score on a pain medication log , 17 or both on the day of chemotherapy . 
patients were not deemed to have progressed or to be removed from study for increased serum psa concentration alone although the level was measured with each cycle and available to the clinician and the patient . 
if there was grade 4 afebrile neutropenia for more than 7 days , grade 3 and greater febrile neutropenia or stomatitis , or grade 4 thrombocytopenia , a 20% dose reduction was required for docetaxel . 
it was withheld in the event of grade 3 or greater non - haematological toxicity until resolution to grade 2 and at the physicians discretion to grade 1 toxicity for up to 3 weeks . 
patients stopped chemotherapy for grade 4 hypersensitivity , grade 3 neurotoxicity , and grade 2 diarrhoea that was unresponsive to standard supportive therapy , or if there was a delay in administration of the scheduled dose by more than 3 weeks . 
patients who completed 12 cycles of docetaxel or who stopped docetaxel because of toxicity were permitted to continue atrasentan or placebo for a total of up to 52 weeks from commencement . 
patients did not receive routine prophylactic colony - stimulating factors to prevent neutropenia , but were permitted to have such treatment as per the national risk guidelines18 during the study . 
the planned follow up was a maximum of 3 years . statistical analysis the coprimary endpoints were progression - free survival ( pfs ) and overall survival following the addition of atrasentan or matching placebo to standard docetaxel chemotherapy with prednisone . 
pfs was de ned as any one of the following criteria for progressionincreased pain or analgesia or both , soft tissue disease as per recist ( version 1.0 ) , or the development of new lesions on the technetium - 99m bone scan , con rmed with further lesions on another bone scan not less than 6 weeks later or death from any cause . 
 if the larger of the two nal p values was less than 0025 ( pfs ) or 0022 ( overall survival , to account for interim testing ) , both null hypotheses would be rejected . 
 assuming a 4 year accrual , 25 years of follow - up , and 930 eligible patients , the study was designed to have 87% power to detect a 25% increase from 60 months to 75 months in median pfs and from 180 months to 225 months in median overall survival with a one - sided log rank with of 00125 . three formal the study was overseen by the swog data safety monitoring committee ( dsmc ) on a twice a year basis . 
 additionally , interim analyses were planned after half the patients were enrolled , after 75% accrual ( 698 of 930 ) and 40% ( 307 of 768 ) of the predicted deaths had occurred , and after completion of accrual ( n = 930 )  . 
an evaluation of the alternative hypothesis of a 25% improvement in survival was tested at the one - sided 0005 level and the null hypothesis of no survival di erence between groups was tested at the one - sided 0001 level at each interim analysis timepoint . 
the recommendation to terminate accrual and report early fell to the dsmc , based on progression , 1038 patients randomly assigned 518 allocated to docetaxel and placebo 520 allocated docetaxel and atrasentan 22 ineligible 20 ineligible 496 eligible for docetaxel and placebo 500 eligible for docetaxel and atrasentan 2 withdrew consent before receiving any protocol treatment 496 discontinued trial treatment 498 discontinued trial treatment 169 completed treatment as planned 327 did not complete treatment 171 progression or death 81 adverse events or side - eects 20 refused further trial treatment 6 could not be ascertained 49 other ( not protocol specied ) 185 completed treatment as planned 313 did not complete treatment 171 progression or death 67 adverse events or side - eects 3 could not be ascertained 19 refused further trial treatment 53 other ( not protocol specied ) 496 included in intention - to - treat analysis 498 included in intention - to - treat analysis figure 1 : trial pro le vol 14 august 2013 toxicities , and other factors in addition to overall survival . 
 a comprehensive quality - of - life assess ment was done in swog s0421 ; these results will be reported separately . the graphical and numerical methods of lin and colleagues19 were used to check the adequacy of the cox regression model . 
 table 1 : demographic characteristics of 994 eligible patients docetaxel + atrasentan docetaxel + placebo role of the funding source sano - aventis or abbott laboratories had no role in the study design , data collection , analysis or inter pretation , or the writing of the report . 
the corresponding author had full access to all the data and the nal responsibility to submit for publication . results between august , 2006 , and may , 2010 , 1038 patients were enrolled by swog , cancer and leukemia group b ( calgb ) , and eastern cooperative oncology group ( ecog )  . 
table 1 shows that the characteristics of the 994 eligible patients ( two patients who withdrew all consent immediately after randomisation are not included in this analysis ) were well balanced between the two groups . 
notably , 801 ( 81% ) of 994 patients had progressed with measurable or evaluable disease by the time they entered the trial , whereas 193 ( 19% ) of 994 were eligible with psa increase alone in the presence of metastatic disease . 
at randomisation , 609 ( 61% ) of 994 patients were already on bisphosphonate therapy , 585 ( 59% ) had extraskeletal metastases in addition to bone involvement , 423 ( 43% ) had a score of at least 4 on the brief pain inventory scale and 313 ( 31% ) had previous prostatectomy . 
the median number of cycles of docetaxel administered was nine , and 169 ( 34% ) of 496 patients in the placebo group and 185 ( 37% ) of 498 in the atrasentan group completed all 12 cycles of chemotherapy . 
260 ( 52% ) of 496 patients in the placebo group and 258 ( 52% ) of 498 in the atrasentan group required dose modi cation or delay , and 81 ( 16% ) of 496 and 67 ( 13% ) of 498 patients , respectively , stopped protocol treatment because of adverse events or side - e ects . 
the trial was released to the investigators for reporting 1 year earlier than the scheduled nal analysis . median pfs was 91 months ( 95% ci 84102 ) in the placebo group and 92 months ( 8599 ) in the atrasentan group ( hazard ratio [ hr ] 102 , 089116 ; p = 081 ; gure 2 )  . 
156 ( 31% ) of 498 patients in the atrasentan group and 159 ( 32% ) of 496 in the placebo group had not progressed or died at 1 year ( gure 2 )  . 
55 ( 15% ) of 367 patients in the atrasentan group and 53 ( 16% ) of 331 in the placebo group had not number at risk docetaxel + atrasentan 498 docetaxel + placebo 496 156 159 months from randomisation figure 2 : kaplan - meier curves of composite progression - free survival 896 vol 14 august 2013 articles docetaxel + atrasentan docetaxel + placebo progressed or died at 2 years . 
249 ( 50% ) of 498 patients in the atrasentan group and 243 ( 49% ) of 496 in the placebo group had a fall in psa concentrations to below 50% of the baseline ( p = 075 )  . 
14% of 450 patients had partial responses ( 31 in the placebo group and 32 in the atrasentan group ; p = 097 ) , although slightly more patients in the atrasentan group than in the placebo group had uncon rmed partial responses ( 61 [ 27% ] vs 49 [ 22% ] , respectively , p = 019 )  . 
 overall median survival was 178 months ( 95% ci 164198 ) in the atrasentan group compared with 176 months ( 164201 ) in the placebo group ( hr 104 , 090119 ; p = 064 ; gure 3 )  . 
a multivariable proportional hazards analysis was used to assess the e ect of treatment after adjustment for strati cation factors and other characteristics of patients and disease ( table 2 )  . 
hrs for the risk factors were in the direction expected with worse overall survival for patients with radiological disease progression , worse pain , and extraskeletal disease at study entry ( table 2 )  . 
after adjustment for these factors , the hr for atrasentan versus placebo remained virtually unchanged ( 103 , 089120 ; p = 067 )  . treatment table 3 shows the grade 4 or higher adverse events . 
 278 ( 57% ) of 492 patients in the atrasentan group had grade 3 or greater toxicity compared with 294 ( 60% ) of 486 in the placebo group ( p = 022 )  . 
other secondary objectives including serum bone markers and circulating tumour cell number will be reported elsewhere . we also assessed interactions with strati cation factors and risk factors to evaluate any trend in di erential treatment with respect to overall survival within subsets of patients . 
interactions of atrasentan with psa , performance status , gleason score , ethnic origin , type of progression at study entry , bisphosphonate use , bone pain , and disease involving lymph nodes or other visceral sites provided no evidence of di erential treatment e ect ( all p > 010 )  . 
the proportional hazards assumption was not violated for either the univariate or multivariable models with outcomes of overall survival ( univariate , p = 088 ; multivariable , p = 032 ) or pfs ( univariate , p = 075 ; multivariable , p = 061 )  . 370 patients completed or stopped chemotherapy because of adverse e ects and were registered to continue their assigned masked treatment ( atrasentan or placebo ) for a total of 52 weeks . 
there was no di erence between groups in post - chemotherapy overall survival for patients who continued masked study drug after stopping chemotherapy ( hr 108 , 083142 ; p = 056 )  . number at risk docetaxel + atrasentan 498 docetaxel + placebo 496 338 342 171 176 figure 3 : kaplan - meier curves of overall survival months from randomisation overall survival progression - free survival hazard ratio ( 95% ci ) p value hazard ratio ( 95% ci ) p value 0001 00006 log ( psa ) 121 ( 115128 ) < 00001 107 ( 103112 ) performance status 23 vs 01 206 ( 157270 ) < 00001 159 ( 122207 ) gleason score 7 vs 56 810 vs 56 africanamerican vs other ethnic origin 076 ( 061095 ) measurable or evaluable vs psa - only progression bisphosphonate use at study entry ( yes vs no ) 097 ( 074126 ) 110 ( 086141 ) 087 ( 068111 ) 104 ( 083131 ) 087 ( 071107 ) 026 073 018 080 044 0017 0032 123 ( 102149 ) 120 ( 101144 ) 0043 102 ( 088119 ) 079 109 ( 095126 ) 023 worst pain at study entry ( > 4 vs 4 ) 16 176 ( 151204 ) < 00001 143 ( 124165 ) < 00001 positive lymph nodes 109 ( 089134 ) 039 109 ( 090132 ) extraskeletal disease vs none 126 ( 103153 ) 0024 130 ( 108157 ) previous radical prostatectomy atrasentan vs placebo 093 ( 078110 ) 103 ( 089 120 ) 037 067 089 ( 077104 ) 099 ( 086113 ) 037 0005 014 087 psa = prostate - speci c antigen . table 2 : multivariable analysis of strati cation and other risk factors and atrasentan with overall survival and progression - free survival results of our discussion the intergroup placebo - controlled phase 3 study of atrasentan with standard docetaxel chemotherapy and prednisone were negative for the two primary endpoints : composite pfs and overall survival . 
the study was designed for patients with bone metastases to test the hypothesis that inhibition of the endothelin pathway , predominantly in osteoblasts , would slow disease progression and improve survival . 
 * possibly , probably , or de nitely treatment related . table 3 : adverse events ( at least one grade 4 ) in patients who received any protocol treatment * panel : research in context systematic review we searched pubmed , american society of clinical oncology , and european society for medical oncology websites on feb 28 , 2005 , and dec 30 , 2012 , with the search terms phase iii trials , docetaxel , and prostate cancer , restricting the search to clinical trials ( reviews were excluded )  . 
after completion of our trial , the second assessment with the same parameters identi ed three trials on pubmed ( of bevacizumab , high - dose vitamin d , and estramustine ) and ve on american society of clinical oncology and european society for medical oncology sites ( a ibercept , a gm - csf gene vaccine , lenalidomide , zibotentan , and dasatinib )  . 
the results of these trials were negative for the primary endpoint overall survival , whereas two trials with curtisen and 89sr have been completed but the data are not reported yet . 
 in our double - blind swog s0421 trial , we assessed the combination of atrasentan plus docetaxel in patients with castration - resistant prostate cancer and skeletal metastasis compared with docetaxel plus placebo . interpretation our ndings provide de nitive evidence for the lack of any bene t from endothelin receptor a blockade with atrasentan in patients with castration - resistant prostate cancer with bone metastases . 
this negative result emphasises the challenges of adding novel agents to standard treatments for castration - resistant prostate cancer , particularly docetaxel , even in the context of a good biological rationale and supportive early phase clinical data . 
docetaxel as a single agent remains the standard of care in metastatic castration - resistant prostate cancer . phase 3 studies of the newer endothelin antagonist ( zibotentan ) in patients with advanced prostate cancer were also negative ; therefore , inhibitors of the endothelin pathway seem to be ine ective in this disease setting ( panel ) .10 , 11 , 2022 are the osteoblast and its interaction with the prostate cancer cell in bone metastasis valid targets for prostate cancer treatments ? in our study , we noted that patients with substantially elevated markers of bone turnover did seem to bene t from atrasentan compared with placebo ( lara pn , unpublished )  . 
this di erence suggests that it might be possible to design a more stringent study of only patients with bone metastases and worse serum bone turnover parameters , and exclusion of any clinically signi cant visceral involvement . 
the solution would be to restrict inclusion to less than 3% of the accrued patients with castration - resistant prostate cancer , but it would leave questions about practicality and generalisability unaddressed . completion of swog s0421 was contemporaneous with several other events in drug development for castration - resistant prostate cancer . 
first was the reporting of several negative studies in which a targeted agent had been used with docetaxel in a randomised phase 2 or 3 trial to improve outcomes for patients with castration - resistant prostate cancer . 
these agents included high - dose calcitriol ( dn - 101 ) , bevacizumab , a ibercept , vandetanib , zibotentan , lenalidomide , a gm - csf gene vaccine , imatinib , oblimersen , and at101.11 , 2330 second , was the reporting of an e ective treatment ( ra ) to target the osteoblast and its environment in a randomised phase 3 trial.31 ra had a large palliative bene t and improved overall survival in patients with symptomatic castration - resistant prostate cancer with osseous but not visceral metastases , who were ineligible for or declined participation , or were previously exposed to docetaxel ; the ndings suggested that bone turnover markers , particularly serum alkaline phosphatase , were good surrogate measures of tumour control . 
however , the interpretation of this nding , when taken with data from swog s0421 and other trials , is that small molecule targeting of the endothelin receptor is either too selective or simply not su ciently e ective to change outcome . 
third , we have several novel treatments that improve survival , including novel immunotherapy with sipuleucel - t , androgen receptor pathway blockade with acetate or enzalutamide , and chemotherapy with cabazitaxel for patients after docetaxel chemotherapy.3234 these new agents are likely to be used for the earlier treatment of advanced prostate cancer.35 together these drug developments mean more options for clinicians and patients for the treatment of metastatic prostate cancer ; abiraterone 898 vol 14 august 2013 articles however , docetaxel - containing chemo therapy is still regarded as a key treatment for men with castrationresistant prostate cancer . in conclusion , in our intergroup phase 3 trial in patients with metastatic castrate - resistant prostate cancer , atrasentan did not improve pfs or overall survival when added to docetaxel plus prednisone . 
the osteoblastprostate cancer interface remains a potential target based on the results of the bone marker studies , subset analyses , and , most importantly , the successful treatment with ra . 
based on our ndings and those of more than ten other randomised trials of the addition targeted agents , standard - of - care , single - agent docetaxel remains one of the standard options for castrate - resistant prostate cancer ; endothelin inhibitors do not have an established role in advanced prostate cancer.2330 contributors diq , cmt , mh , pnl , ag , cmm , mgg , pcm , mac , jpm , csh , njv , and imt designed the study . 
diq , cmt , mh , pnl , ag , cmm , mgg , pcm , mac , jpm , pwt , pjvv , na , csh , njv , and imt wrote and edited the report . con icts of interest diq has been a consultant for novartis , bayer , algeta , teva , dendreon , oncogenex , medivation , amgen , and astellas ; and has received payment for expert testimony from medivation and teva . 
cm has received a tenth of the full - time equivalent salary support from abbott in support of her role as coordinator for the quality - of - life analysis associated with s0421 . 
the other authors declare that they have no con icts of interest . acknowledgments the investigation was supported , partly , by the following public health service cooperative agreement grant numbers awarded by the national cancer institute , department of health and human services : ca32102 , ca38926 , ca46368 , ca46441 , ca58882 , ca58861 , ca12644 , ca22433 , ca46282 , ca27057 , ca58416 , ca45807 , ca45808 , ca45450 , ca42777 , ca35281 , ca20319 , ca35090 , ca76429 , ca14028 , ca67575 , ca45377 , ca68183 , ca63848 , ca74647 , ca16385 , ca35192 , ca63844 , ca11083 , ca63845 , ca76447 , ca35128 , ca13612 , ca35431 , ca76448 , ca35178 , ca35176 , ca35119 , ca35421 , ca128567 , ca04919 , ca68183 , ca45560 , ca37981 , ca58723 , ca21115 , ca16116 , and ca31949 ; and , partly , by sano - aventis and abbott laboratories . 
the authors report on behalf of a large team and would like to acknowledge the contribution of clinicians , research teams , patients , and their families through ecog , calgb , and the clinical trials support unit in completing swog s0421 . regarding survival and 35 years ( 3045 ) for overall survival ( median follow - up 34 years [ 2943 ] for the sodium thiosulfate group , and 38 years [ 3145 ] for the control group ) ; and localised and sentences disseminated disease should have read localised among participants with disease , 14 events in the sodium thiosulfate group , 13 events in the control group , and six deaths in both the control and sodium thiosulfate groups occurred and in participants with disseminated disease , 12 events and 11 deaths occurred in the sodium thiosulfate group and 11 events and four deaths occurred in the control group . 
these corrections have been made to the online version as of june 2 , 2017 . correction to lancet oncol 2017 ; 18 : 71931 registry international cancer , steliarova - foucher colombet m , ries lag , et al , and the iicc - 3 incidence contributors . 
 lancet oncol 2017 ; 18 : 71931 in this article , the coverage of the population of east asia in table 1 in the age 014 years column should have been 44% , and in the age 1519 years column , 40% . 
 consequently , the fourth sentence in the first paragraph of the results read approximately should have the world population 114% of aged ( contributing years 18 376 710 144 person - years ) was covered by the registries included in our study , ranging from 17% in south asia ( india ) to 994% in north america ( table 1 )  . 
these corrections have been made to the online version as of june 2 , 2017 , and the printed article is correct . 014 correction to lancet oncol 2017 ; 18 : 812 versus gronchi a , ferrari s , quagliuolo v , et al . 
histotype - tailored neoadjuvant chemotherapy standard chemotherapy in patients with high - risk soft - tissue sarcomas ( isg - sts 1001 ) : an international , open - label , randomised , controlled , phase 3 , multicentre trial . 
this correction has been made to the online version as of june 2 , 2017 , and the printed article is correct . correction to lancet oncol 2017 ; 18 : 6374 freyer dr , chen l , krailo md , et al . 
 effects of sodium thiosulfate versus observation on development of cisplatininduced hearing loss in children with cancer ( accl0431 ) : a multicentre , open - label , controlled , randomised , phase 3 trial . 
lancet oncol 2017 ; 18 : 6374in the summary and results of this article , the sentences should regarding adverse events have read the most common grade 34 haematological adverse events reported , irrespective of attribution , were neutropenia ( 117 [ 66% ] of 178 participant cycles in the sodium thiosulfate group vs 145 [ 65% ] of 224 in the control group ) , whereas the most common non - haematological adverse event was hypokalaemia ( 25 [ 17% ] of 149 vs 22 [ 12% ] of 187 )  . 
 in the results , sentences regarding adverse events should have read haematological toxicity was not significantly different between the treatment groups , occurring 137 ( 77% ) of 178 participant cycles in the sodium thiosulfate group and 172 ( 77% ) of 224 participant cycles in the control group ( p = 097 ; table 3 )  . 
aggregate nephrotoxicity was more common in the sodium thiosulfate group , in which 37 ( 25% ) of 149 participant cycles were affected versus 25 ( 13% ) of 187 controls ( p = 00071 ; sentences table 4 ) ; serious adverse events regarding should have read 194 serious adverse events were reported in 26 patients ; of these , 127 were deemed unrelated , 47 unlikely , 20 possibly , and none related to probably or definitely sodium thiosulfate . 
87 were nonhaematological adverse events , of which 45 were deemed unrelated , 28 unlikely , 14 possibly , and none related to probably or definitely sodium sentences thiosulfate ; regarding median follow - up should have read median follow - up was 35 years ( iqr 3045 ) for event - free vol 18 june 2017 e301 corrections editorial for more on the bbc report see health - 27894551 for the monitor report see government / publications / closing - the - nhs - funding - gaphow - to - get - better - valuehealthcare - for - patients for the times letter see letters / article4140238.ece nhs privatisation : a step too far according to a recent bbc report , englands national health service ( nhs ) will face a funding shortfall of about 2 billion by 2016 . 
projections in a report by monitor , the sector regulator for health - care services in england , suggest this de cit will rise to around 30 billion by 2021 . 
the e ect that this de cit will have on the nhs has not gone unnoticed : a letter to the times on july 7 , 2014 , signed by leaders from various royal colleges , stated that unless plans for meeting funding gaps were created , the nhs would be unable to cope . 
 clearly , urgent measures need to be taken if the nhs is to continue to be able to provide its mandated services , but worryingly the debate is increasingly looking to privatisation as a means of plugging these funding gaps . 
 this insidious slide towards outsourcing health care is not only a lazy , short - term solution to the immediate problems facing the nhs , but also potentially highly damaging to the provision of health care in the uk . 
 current tenders include catering or provision of health care in prisons ; however , a recent tender proposal by four general practitioner clinical commissioning groups ( ccgs ) in sta ordshire and stoke would see external contractors manage entire clinical cancer - care pathways for patients with bladder , lung , prostate , and breast cancer . 
the proposed removal of an entire care pathway to the private sector is a concerning development , partly because further dismantling of the nhs , and partly because it is indicative of how little thought has gone into the consequences . 
presumably , the contractor will not be expected to run departments peripherally involved in cancer care , or to invest in all of the attendant technologies , and , since the tender is only for 10 years , there would be little nancial incentive to do so . 
these measures will erode the nhs , leading to a failure to invest in sta ng and long - term infrastructureas seen in other sectors that have undergone partial privatisation . 
this scenario will become particularly acute over successive tenders , and especially damaging if winning bids are chosen predominantly on nancial grounds , or if a contractor fails and the government has to step in to handle the costly repercussions . 
for example , if care is outsourced only for patients with speci c types of cancer , what happens to those patients if metastases , comorbidities , or other complications arise ? individual patients risk being caught in a mixed - care model between private and public services for di erent aspects of their treatment , which could lead to disjointed care and unclear accountability . 
it would be unrealistic to not consider some elements of privatisationeg , discrete parts of the nhs that service clinical pathways , and where centralisation could improve consistency and quality . 
but to try to excise an entire clinical care pathway that has several links to other parts of the nhs is an ill - considered x to a complex issue , and will ultimately not serve those for whom the nhs was rst created . 
 the lancet oncology vol 15 august 2014 correction to lancet oncol 2016 ; 17 : 23442 correction to lancet oncol 2016 ; 17 : e506 shaw at , gandhi l , gadgeel s , et al , on behalf of the study investigators . 
 lancet oncol 2016 ; 17 : e50209the fourth sentence of the biosimilar monoclonal antibodies in oncology section should have read , the primary endpoint , overall response rate , at week 24 was equivalent between groups ( 70% for myl - 1401o vs 64% for trastuzumab ) , and the risk ratio was 109 ( 90% ci 097121 )  . 
this correction has been made to the online version as of march 1 , 2017 . vol 18 march 2017 e134 corrections correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2017 ; 18 : e142 correction to lancet oncol 2017 ; 18 : e81 , e82 , e86 burki tk . 
this correction has been made to the online version as of march 2 , 2017 . published online march 2 , 2017 s1470 - 2045 ( 17 ) 30173 - 0 published online march 2 , 2017 s1470 - 2045 ( 17 ) 30175 - 4 rl , cancer cancer and survivors : childhood adolescent , r , mulder al . 
recommendations kremer skinner for lc , in male gonadotoxicity surveillance young childhood , report adult international late effects from the guideline harmonization group in collaboration with the pancaresurfup consortiu lancet oncol 2017 ; 18 : e7590in this review , the sixth paragraph under the who needs surveillance ? heading should have read there is probably no increased risk after treatment with cyclophosphamide , busulfan or cyclophosphamide or fludarabine and melphalan , hsct conditioning , and ifosfamide , and mechlorethamine , cisplat additionally , the key for figure 2 should have been light orange for moderate recommendation to do and dark orange for weak recommendation do . 
these corrections have been made to the online version as of march 29 , 2017 . procarbazine vol 18 april 2017 e196 corrections corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 published online august 3 , 2017 s1470 - 2045 ( 17 ) 30589 - 2 see articles page 1159 selective internal radiotherapy in advanced colorectal cancer : only for right - sided tumours ? colorectal cancer is a biologically unique tumour entity ; in 3040% of patients , metastases are confined exclusively to the liver , lung , or both , with or without minor additional lymph node involvement . 
different from all other tumour types , r0 - resection of these lesions is not always followed by systemic relapse in other regions , therefore this local approach isdespite systemic spread of the diseaseleads to a potentially curative resection in up to 61% of patients.1 , 2 therefore , locoregional treatment of metastases is of key importance . ( transarterial chemoembolisation if surgery alone is not appropriate , other locoregional modalities can be given , 3 such as hepatic arterial infusion of floxuridine , mitomycin , and oxaliplatin ; addition of starch microspheres or application of drug - coated glass beads ( eg , irinotecan beads ) for prolonged arterial drug chemoexposure ; embol ization ; tace ) ; ablation - techniques ( eg , radiofrequency , ultrasound , laser - ablation , heat - ablation , or cryoablation , radio surgery , and brachytherapy [ yttrium - 90 resin microspheres ; selective internal radiotherapy ; sirt ] )  . 
 however , randomised trials testing the individual value of any one treatment are rare ; only radiofrequency ablation with or without surgical resection plus chemotherapy has been prospectively proven effective for superior overall survival versus chemotherapy alone ( phase 3 clocc trial4 )  . 
 beyond this , sirt also showed clinically relevant efficacy on liver metastases in three small randomised in patients refractory to standard systemic trials chemotherapy ; therefore , a broad first - line therapy was justified . 
in the lancet oncology , harpreet wasan and colleagues5 report the results of a combined analysis of three trials of first - line folfox ( leucovorin , fluorouracil , and oxaliplatin ) chemotherapy with or without sirt . 
eligibility criteria used in the three trials were more or less comparable , including patients with unresectable , but limited , liver metastases , with or without lung metastases , and with or without lymph node metastases.6 as expected , the local effect of sirt is clear , with an improved proportion of patients achieving an overall response and liver - only progression . 
however , this locoregional effect did not translate into improved overall progression - free survival or overall survival , even in those patients with metastases restricted to the liver investigation ( one third of the patients )  . 
 why does this proven effective locoregional approach not alter the overall course of disease , even in liver - only disease ? several potential contributing factors that caused imbalance between the groups might have been involved , including different eligibility criteria in each of the three trials , different oxaliplatin dose between treatment groups ( 29% less in the folfox plus sirt group in cycles 13 than in the folfox alone group ) , lower dose of bevacizumab starting 23 months later in the folfox plus sirt group , fewer patients who had bevacizumab in the folfox plus sirt group compared with the folfox alone group ( 197 [ 36% ] vs 256 [ 47% ] ) , less salvage treatment in the folfox plus sirt group , and heterogeneity of the sirt dose between patients , centres , and treatment times . 
more relevant factors might be the fact 47 ( 8% ) of 554 patients randomly assigned to sirt did not receive sirt , that 41 ( 7% ) patients only had unilobar application , and 18 ( 3% ) patients crossed over from folfox alone to folfox plus sirt . 
however , even if those patients are eliminated from the analysis , the overall outcome would not change substantially . another relevant factor might be the short overall survival of patients in all three trials , which was shorter than that of other trials with comparable patient populations but that included treatment with one or two targeted drugs ( bevacizumab and egfr inhibitors ) .7 in the foxfire trials , egfr inhibitors were not used and vegf inhibitors were used in only one third of patients . 
this difference is mainly due to the enrolment and treatment era of the largest trial included in the analysis , sirflox ( 200613 ) and also the fact that patients were treated in countries without routine access to the targeted drugs . 
however , if systemic treatment is weak as in this case , shouldnt sirt have a bigger effect on overall survival ? this is obviously not the case , because , beyond the local treatment only , complete metastases resection after optimal and highly active chemotherapy can improve the long term outcome.4 1138 vol 18 september 2017 comment furthermore , although the local sirt approach improved frequency of resection , it only marginally increased the depth of response , the most important prerequisite for complete secondary resection . 
therefore , the frequency of secondary resection of liver ( and lung ) metastases was not sufficiently increased to improve survival . however , in an important subgroup analysis , 8 sirt was shown to significantly improve overall survival ( p = 0007 ) and progression - free survival ( p = 0053 ) in one third of patients with right - sided primary tumours , known to be much less sensitive to all types of systemic treatment versus left sided tumours , but had no effect in patients with left - sided primary tumours.sirt , which is not affected by chemoresistance in the same way , appears to overcome the intrinsic chemoresistance of liver metastases of right - sided primary tumours . 
this is an important message from wasan and colleagues study , the hr for overall survival in patients with right - sided tumours was 067 ( 048092 ) versus nonsignificant for left - sided tumours , which could have an impact on further clinical research , to improve the poor outcome of patients who have right - sided tumours . 
first - line selective internal radiotherapy plus chemotherapy versus chemotherapy alone in patients with liver metastases from colorectal cancer ( foxfire , sirflox , and foxfire - global ) : a combined analysis of three multicentre , randomised , phase 3 trials . 
protocol for combined analysis of foxfire , sirflox , and foxfire - global randomized phase iii trials of chemotherapy + / selective internal radiation therapy as first - line treatment for patients with metastatic colorectal cancer . 
phosphorylated trifluridine concentration and tumour growth inhibition are increased with the combination of tas - 102 and bevacizumab compared with either drug alone.4 the available clinical data5 suggest that the real benefit of tas - 102 monotherapy is small , therefore strategies to extend this benefit are urgently needed . 
 authors planned to enrol 25 patients , with at least 21 patients needed to have 80% power to reject the null hypothesis of 25% of patients free of progression at 16 weeks by central review . 
this design highlights two points of strength of this study : first , in this setting , 25% progression - free survival after four cycles is clinically relevant ; and second , independent review of response , which is uncommon in phase 2 studies , grants reliability to the results . 
the original hypothesis required at least nine ( 43% ) of the 21 patients included in the primary efficacy analysis to be free of progression at 16 weeksindeed , exactly nine patients achieved such a result . 
from a methodological perspective , this result shifts the attention to the level of the study , published online july 28 , 2017 s1470 - 2045 ( 17 ) 30574 - 0 see articles page 1172 vol 18 september 2017 1139 comment editorial uk pharmaceutical industry under threat on may 2 , 2014 , p zerthe worlds largest pharmaceutical companymade a second attempt to purchase the rival rm astrazeneca . 
these events happened soon after an asset swap between glaxosmithkline ( gsk ) and novartis , in which novartis sold its vaccines division to gsk , who in turn sold its oncology portfolio to novartis ; the two companies are also to merge their consumer health divisions . 
the sale of gsks oncology portfolio in particular is surprising , because the company stated on record last year that they wanted to become one of the top ve players in oncology . 
 inevitably , concerns have been raised in the uk , where astrazenecas headquarters are based , that the potential merger with p zer will cost the country jobs and vital income . 
p zer has a bad reputation in this area ; for instance , it sold its uk research facilities in sandwich , kent , in 2011 , in the process making 1500 highly skilled people redundant . 
clearly aware of these negative perceptions , p zers chief executive has written to the uks prime minister , david cameron , to promise to complete work on astrazenecas research and development ( r&d ) hub in cambridge , and to pledge to employ at least 20% of the combined companys r&d workforce in the uk and locate some of the companys manufacturing plants in brita however , these guarantees are only for 5 years and do not go far enough . 
 additional concerns are that pharmaceutical mergers will not only negatively a ect the economy , but that they could also sti e innovation and the development of new drugs , further threatening the hard - won reputation of the uk as a world leader in medical r&d . 
indeed , a f ormer head of research at p zer recently informed the independent that he fears drug discovery programmes in their early stages are likely to be disrupted or abandoned , and highlighted astrazenecas oncology portfolio as being particularly vulnerable . 
innovation could also be sti ed in the gsknovartis deal , which means gsk has an e ective monopoly on vaccine development , and the subsequent loss of competition could deter further innovation . 
the mergers could also increase the onus on academia and small biotechnology companies to do more early - stage discovery and r&d work , bringing with it increased nancial pressures . it is therefore vital that the uk government does all it can to encourage companies to retain their drug discovery divisions within the uk . 
the introduction of the patent box in 2013 , which allows companies to apply for lower corporation tax on earnings from patented inventions , should encourage innovative companies to remain in the uk . 
as a last resort , the government could consider a golden share option ( akin to past deals with rolls royce and bae systems ) to prevent a foreign takeover , or using its public interest test powers , which can block takeovers if they could damage national interestuk business secretary vince cable has said he would not rule out this latter option , and states that the government sees the uk as a knowledge economy , not a tax haven . 
an announcement in april this year from the uks exam regulator , ofqual , that stated practical work would cease to contribute to the overall grade of a levelsthe quali cations that determine university entrance in the ukis a major retrograde step and disconnected from the realities of science . 
 although mergers and acquisitions are an everyday part of business for companies that compete in a global market , sometimes national interests need to be put ahead of markets and pro t , and every e ort must be made to ensure that researchers and innovators are not hampered in the pursuit of better outcomes for patients . 
 the lancet oncology vol 15 june 2014 in view of the poor outcome of patients with highrisk , localised soft - tissue sarcomas , how can these data be incorporated and built upon ? this trial suggests that patients with high - risk extremity and trunk sarcomas could be considered for neoadjuvant anthracycline and ifosfamide , accounting for patient age , performance status , and comorbidities . 
these data should not be a justification for the routine use of adjuvant or neoadjuvant chemotherapy in other histological subtypes not included in this trial . with many sarcoma centres routinely administering neoadjuvant radiation , the optimum preoperative treatment sequence for localised soft - tissue sarcomas remains to be defined because this trial was not designed to answer this question . 
the provisional thoughtful interpretation because of the initial onesided testing , short follow - up , limited number of events , and relatively young patient age ( median 489 years )  . 
rlj is a consultant for pharmamar , lilly , merck , eisai , diachii , immundesign , adaptimmune , blueprint , and deciphera . gronchi a , ferrari s , quagliuolo v , et al . 
histotype - tailored neoadjuvant chemotherapy versus standard chemotherapy in patients with high - risk soft - tissue sarcomas ( isg - sts 1001 ) : an international , open - label , randomised , controlled , phase 3 , multicentre trial . 
evaluation of response after neoadjuvant treatment in soft tissue sarcomas ; the european organization for research and treatment of cancer - soft tissue and bone sarcoma group ( eortc - stbsg ) recommendations for pathological examination and reporting . 
a further shift towards recommended vol 18 june 2017 published online april 27 , 2017 s1470 - 2045 ( 17 ) 30305 - 4 see articles page 823 comment intensive surveillance was adopted in the 2008 usmstf guidelines , which recommended a 510 year interval for low - risk patients.1 guidelines were also developed by other organisations and in other countries . 
european union ( eu ) and uk guidelines are consistent with the us guidelines with one exception.4 the low - risk and highrisk groups are classified as low - risk and intermediaterisk and a third group is defined : a high - risk group of patients with five or more adenomas . 
 with knowledge of the slow growth of the adenomatous polyp before it develops into colorectal cancer , guidelines have evolved to take a more conservative approach to surveillance , with increasingly longer intervals between examinations . 
the goal of surveillance is to reduce the risk of colorectal cancer and mortality in the group of patients at increased risk while minimising procedure risk , cost , and burden on medical resources . 
 in the lancet oncology , atkin and colleagues5 report a retrospective analysis of a large multicentre cohort in which 11 944 patients with adenomas study , deemed to be of intermediate risk according to the uk classification ( us high - risk group ) were followed up for a median of 79 years ( iqr 56111 )  . 
a subset of these patients had an incidence of colorectal cancer that was significantly less than that of the general uk population not undergoing surveillance ( standardised incidence ratio 051 , 95% ci 029084 )  . 
 the study by atkin and colleagues is excellent , but has the limitations of a retrospective study , including the absences of bowel preparation reporting in line with current standardised criteria , central review of baseline pathology , information about the training , rate of the expertise , and adenoma detection endoscopists , criteria for a complete colonoscopy , and pathology of the proximal polyps . 
prospective studies can address many of these limitations and can further examine the question of whether some patients really need surveillance and whether further lengthening of intervals can be recommended in others . 
for example , in the eu and uk guidelines , can the lower - risk subgroup defined by atkin and colleagues within the intermediaterisk group be relegated to receiving no surveillance , as they suggest ? how can this approach be put into practice with clear terminology so that clinicians can easily separate out a lower - risk subgroup from this intermediate - risk group ? should the lower - risk subgroup be included in the original low - risk group ? in the us guidelines , the recommendations for lowrisk patients are for exams every 510 years . 
could this recommendation be more definitively made 10 years ? can a subset of the us low - risk group be relegated to no surveillance ? can the intervals in us high - risk patients be lengthened to 5 years or could this group be further risk stratified ? within this context , much more information is needed on the natural history and follow - up of sessile serrated adenomas and polyps.6 crucial given new studies are being planned to address these that postquestions , which are polypectomy surveillance colonoscopies have become an increasing burden on endoscopy units , patients , the economy , and medical resources.7 available colonoscopy resources might be better used if shifted to initial highquality screening and diagnosis and will continue to be the driving force in the decrease in colorectal cancer incidence and mortality that has been ongoing since 1975.8 this will take on more urgency as worldwide colorectal cancer screening continues to accelerate , as has happened in the eu , the usa , 8 , 9 and elsewhere . 
 * sidney j winawer , ann g zauber gastroenterology and nutrition service , department of medicine ( sjw ) and department of epidemiology and biostatistics ( agz ) , memorial sloan kettering cancer center , new york 10065 - 6007 , ny , usa winawers@mskcc.org we declare no competing interests . 
this publication was mainly funded by the national cancer institute with grants p30 ca008748 , u01ca152959 , r01 ca026852 , r01 ca079572 , and with additional support from the cantor colon cancer fund to sjw and agz . 
annual report to the nation on the status of cancer , 19752006 , featuring colorectal cancer trends and impact of interventions ( risk factors , screening , and treatment ) to reduce future rates . 
cancer 2015 ; 121 : 228185 . improving childhood cancer care in latin america and the caribbean : a paho childhood cancer working group position statement most children with cancer live and die in low - income and middle - income countries ( lmics )  . 
medical and health system advances have brought cure to more than 80% of children with cancer in high - income countries ( hics ) , 1 but such advances have eluded children in most lmics , where inequities can yield cure percentages anywhere from 5% to 60%.2 multiple factors contribute to the inadequate care of childhood cancers in lmics , including resource scarcity , health system fragility , limited provider awareness , and absence of political attention.3 these conditions are abetted by a lack of sustained political attention to childhood cancer at the international level . 
 despite a growing global burden of non - communicable diseases ( ncds ) , calls by global health governance institutions to address ncds have largely failed to address the plight of children with cancer in lmics . 
 a longstanding commitment by childhood cancer professionals and advocates in latin america and the caribbean has contributed to substantial , if variable , progress towards understanding the burden of childhood cancer and improving childhood cancer services in the region.4 past and present lancet oncology commissions have underscored the challenges and opportunities that cancer presents in the context of strengthening health systems in latin america.5 recent work6 suggests opportunities to bring such efforts to scale through a strengthening of the policy and system dimensions of childhood cancer care . 
the union for international cancer control ( uicc ) convened an international policy dialogue on childhood cancer in latin america , identifying integrated elements necessary to improve childhood cancer outcomes in the region . 
this correction has been made to the online version as of march 2 , 2017 . published online march 2 , 2017 s1470 - 2045 ( 17 ) 30173 - 0 published online march 2 , 2017 s1470 - 2045 ( 17 ) 30175 - 4 rl , cancer cancer and survivors : childhood adolescent , r , mulder al . 
recommendations kremer skinner for lc , in male gonadotoxicity surveillance young childhood , report adult international late effects from the guideline harmonization group in collaboration with the pancaresurfup consortiu lancet oncol 2017 ; 18 : e7590in this review , the sixth paragraph under the who needs surveillance ? heading should have read there is probably no increased risk after treatment with cyclophosphamide , busulfan or cyclophosphamide or fludarabine and melphalan , hsct conditioning , and ifosfamide , and mechlorethamine , cisplat additionally , the key for figure 2 should have been light orange for moderate recommendation to do and dark orange for weak recommendation do . 
these corrections have been made to the online version as of march 29 , 2017 . procarbazine vol 18 april 2017 e196 corrections articles adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study pippa g corrie , andrea marshall , janet a dunn , mark r middleton , paul d nathan , martin gore , neville davidson , steve nicholson , charles g kelly , maria marples , sarah j danson , ernest marshall , stephen j houston , ruth e board , ashita m waterston , jenny p nobes , mark harries , satish kumar , gemma young , paul lorigan summary background bevacizumab , a monoclonal antibody that targets vegf , has shown restricted activity in patients with advanced melanoma . 
we report results from the preplanned interim analysis . methods we did a multicentre , open - label , randomised controlled phase 3 trial at 48 centres in the uk between july 18 , 2007 , and march 29 , 2012 . 
patients aged 16 years or older with american joint committee on cancer stage ( ajcc ) stage iib , iic , and iii cutaneous melanoma were randomly allocated ( 1 : 1 ) , via a central , computer - based minimisation procedure , to receive intravenous bevacizumab 75 mg / kg , every 3 weeks for 1 year , or to observation . 
this trial is registered as an international standardised randomised controlled trial , number isrctn81261306 . findings 1343 patients were randomised to either the bevacizumab group ( n = 671 ) or the observation group ( n = 672 )  . 
at the time of interim analysis , 286 ( 21% ) of 1343 enrolled patients had died : 140 ( 21% ) of 671 patients in the bevacizumab group , and 146 ( 22% ) of 672 patients in the observation group . 
we noted no signi cant di erence in overall survival between treatment groups ( hazard ratio [ hr ] 097 , 95% ci 078122 ; p = 076 ) ; this nding persisted after adjustment for strati cation variables ( hr 103 ; 95% ci 081129 ; p = 083 )  . 
180 grade 3 or 4 adverse events were recorded in 101 ( 15% ) of 671 patients in the bevacizumab group , and 36 ( 5% ) of 672 patients in the observation group . 
there was an improvement in disease - free interval for patients in the bevacizumab group compared with those in the observation group ( hr 083 , 95% ci 070098 , p = 003 ) , but no signi cant di erence between groups for distant - metastasis - free interval ( hr 088 , 95% ci 073106 , p = 018 )  . 
no signi cant di erences were noted between treatment groups in the standardised area under the curve for any of the quality - of - life scales over 36 months . 
three adverse drug reactions were regarded as both serious and unexpected : one patient had optic neuritis after the rst bevacizumab infusion , a second patient had persistent erectile dysfunction , and a third patient died of a haemopericardium after receiving two bevacizumab infusions and was later identi ed to have had signi cant predisposing cardiovascular risk factors . interpretation bevacizumab has promising tolerability . 
fewer than 50% of patients with resected locoregional melanoma survive to 5 years.1 adjuvant trials assessing interferon alfa have shown that the drug delays melanoma recurrence , but has only a small overall survival bene t.2 the low survival bene t and high treatment - related toxic e ects associated with interferon alfa mean that no internationally agreed standard adjuvant treatment is available for patients with high - risk melanoma . vol 15 may 2014 lancet oncol 2014 ; 15 : 62030 published online april 16 , 2014 s1470 - 2045 ( 14 ) 70110 - x this online publication has been corrected . 
eligible patients were at least 16 years old , with histological con rmation of completely resected american joint committee on cancer stage iib ( t3bn0m0 and t4an0m0 ) , iic ( t4bn0m0 ) , or iii ( txn13m0 ) cutaneous melanoma . 
inclusion criteria were an eastern cooperative oncology group ( ecog ) performance status of 01 ; a life expectancy of 6 months or more ; and adequate haematological , liver , and renal function . 
exclusion criteria were evidence of distant or non - regional lymph - node metastases ( established by ct or mri scanning of the body and head within 8 weeks of randomisation ) , incomplete resection of melanoma , or adjuvant radiotherapy that was ongoing at randomisation . 
 treatment assignment could not take place within 4 weeks of surgery or in the presence of unhealed wounds , but had to be within 12 weeks of a patients latest surgery for melanoma . 
because this interim analysis was preplanned , and in view of the absence of an international standard adjuvant therapy for melanoma , the independent data monitoring committee supported publication of these results in advance of the nal analysis anticipated in 2017 . randomisation and masking eligible patients were randomly assigned centrally in a 1 : 1 ratio using a computer - based minimisation algo rithm , to receive either adjuvant bevacizumab or standard observation . 
randomisation was strati ed by breslow thickness of the primary tumour , n stage according to ajcc staging criteria , 1 ulceration of the primary tumour ( absent , present , or unknown ) , and patient sex . 
this was an openlabelled trial and therefore participants , investigators , and trial sta were not masked to group allocation . procedures for patients randomly assigned to bevacizumab , 75 mg / kg was given via 30 min intravenous infusion once every 3 weeks for 1 calendar year ( maximum 17 infusions ) , or until disease recurred . 
if a patient required any further dose interruptions , treatment was discontinued . department , royal preston hospital , preston , uk ( re board phd ) ; clinical trials unit , beatson west of scotland cancer centre , glasgow , uk ( am waterston phd ) ; clinical oncology , norfolk and norwich university hospital , norwich , uk ( jp nobes frcr ) ; guys and st thomas hospital , london , uk ( m harries phd ) ; velindre cancer centre , cardi , uk ( s kumar md ) ; cambridge cancer trials centre / cambridge clinical trials unitcancer theme , addenbrookes hospital , cambridge , uk ( g young mphil ) ; and deptartment of medical oncology , christie hospital , manchester , uk ( p lorigan md ) correspondence to : dr pippa g corrie , oncology centre , cambridge university hospitals nhs foundation trust 3394 participants assessed for eligibility 2051 excluded 1357 did not meet inclusion criteria 694 declined to participate 1343 randomised 671 assigned to bevacizumab 672 assigned to observation 652 received intervention 1 local recurrence 4 wound healing complications or surgical 19 did not receive intervention 10 because of patient choice intervention 1 case of cellulitis 1 case of thrombus 1 case of hypertension 1 diagnosis of central retinal vein occlusion 119 because of recurrence 112 because of unacceptable toxic eects 28 because of patient choice 1 patient died 291 discontinued early 10 cases of unacceptable dose interruption due to surgical intervention or investigation 7 wound healing complications 12 unplanned discontinuations 2 had a new second malignancy 671 included in primary analysis 592 analysed for health - related quality of life * 672 included in primary analysis 623 analysed for health - related quality of life * figure 1 : trial pro le hr = hazard ratio . 
adverse events reported during the rst year by patients in the observation group and for 28 days after the last bevacizumab infusion for those the bevacizumab group were recorded according to the national cancer institute common terminology criteria for adverse events ( ctcae ) , version 3.0. 
treatment options therapy ; surgery ; radiotherapy , dependent on type of recurrence ; and patient choice . included systemic we ascertained braf mutation status in archived tumour tissue with a cobas4800 ( roche diagnostics , west sussex , uk ) test or by pyrosequencing . 
nras status was not established for braf mutant tumours , because nras and braf mutations are generally mutually exclusive . outcomes the primary endpoint of the trial was overall survival , which we de ned as the time from date of randomisation until date of death from any cause , or censored at the last known date alive . 
disease - free interval was de ned as the time from the date of randomisation until the date of rst ( including distant and locoregional recurrence ) , or date of death due to melanoma . 
distant - metastasis - free interval was de ned as the time from the date of randomisation until the date of rst distant recurrent disease , or date of death due to melanoma . recurrence tumour statistical analysis patients who withdrew consent for further follow - up were included in the analysis , but censored at the time of withdrawal . 
a sample size of 1320 patients ( 660 patients per group ) was needed to detect an absolute increase in 5 year overall survival from 40% to 48% , with 85% power and a 5% signi cance level , which equates to a hazard ratio ( hr ) of 080 . 
hrs were calculated for prognostic subgroups and a hr plot constructed.16 multivariable cox - regression models were used to adjust the treatment e ect for strati cation variables , to assess the independent predictors of overall survival and disease - free interval , and to assess treatment interaction with tumour mutation status and whether hypertension , tted as a time - dependent covariate , a ected disease - free interval . 
quality - of - life data were analysed by standardised and compared across trial groups with wilcoxon rank - sum tests . area - under - the - curve analysis18 reported p values are two - sided . 
this trial is registered as an international standardised randomised controlled trial , number isrctn 81261306 . results 1343 patients were randomly assigned to either the bevacizumab group ( n = 671 ) or the observation group ( n = 672 ; gure 1 )  . 
975 ( 73% ) patients had resected ajcc stage iii melanoma , 515 ( 38% ) patients had an ulcerated primary tumour , and 440 ( 32% ) patients underwent sentinel lymph - node biopsy . 
368 ( 27% ) patients had no known nodal involvement ( n0 and nx ) , 281 ( 21% ) had microscopic lymph - node involvement ( n1a and n2a ) , and 694 ( 52% ) had macroscopic lymphnode involvement . 
we subsequently identi ed 11 ( 1% ) of enrolled patients as ineligible ; three in the bevacizumab group and eight in the observation group : ve had metastatic disease , ve had incomplete surgery , and one had stage iia melanoma . 
am had full access to all the data in the study and the corresponding author had nal responsibility for the decision to submit for publication . number at risk bevacizumab observation hr 097 , 95% ci 078122 ; p = 076 articles e ect causing treatment discontinuation was hypertension in 36 ( 5% ) patients . 
the main reasons for delay were for planned drug holidays or toxic e ects ( data not shown )  . 286 ( 21% ) of 1343 enrolled patients had died at the time of the interim analysis ( 140 [ 21% ] of 671 patients in the bevacizumab group and 146 [ 22% ] of 672 patients in the observation group )  . 
we noted no signi cant di erence in overall survival between treatment groups ( gure 2 ) ; this nding persisted after adjustment for strati cation variables ( hr 103 ; 95% ci 081129 ; p = 083 )  . 
multivariable analysis identi ed disease stage , ecog performance status , and primary melanoma ulceration as independent overall survival disease stage iii ( n1a and n2a ) iii ( other n ) ecog performance status ulceration unknown disease - free interval disease stage iii ( n1a and n2a ) iii ( other n ) breslow thickness ( mm ) 20 > 24 unknown trial group treatment observation ecog performance status n ( % ; n = 1343 ) number of events ( % ) hazard ratio ( 95% ci ) p value 368 ( 27% ) 281 ( 21% ) 694 ( 52% ) 45 ( 12% ) 39 ( 14% ) 100 142 ( 091221 ) 202 ( 29% ) 305 ( 216432 ) 1194 ( 89% ) 235 ( 20% ) 054 ( 039073 ) 147 ( 11% ) 50 ( 34% ) 100 515 ( 38% ) 632 ( 47% ) 196 ( 15% ) 109 ( 21% ) 121 ( 19% ) 100 068 ( 052089 ) 56 ( 29% ) 075 ( 053106 ) 368 ( 27% ) 281 ( 21% ) 694 ( 52% ) 399 ( 30% ) 407 ( 30% ) 437 ( 33% ) 100 ( 7% ) 118 ( 32% ) 76 ( 27% ) 370 ( 53% ) 100 112 ( 082152 ) 278 ( 220351 ) 160 ( 40% ) 100 165 ( 41% ) 200 ( 46% ) 125 ( 101157 ) 174 ( 138220 ) 39 ( 39% ) 084 ( 059119 ) 671 ( 50% ) 672 ( 50% ) 264 ( 39% ) 300 ( 45% ) 083 ( 070098 ) 100 1194 ( 89% ) 490 ( 41% ) 130 ( 102167 ) 147 ( 11% ) 73 ( 50% ) 100 < 00001 < 00001 002 < 00001 < 00001 003 004 ecog = eastern cooperative oncology group . table 2 : results from the multivariate analyses for overall survival and disease - free interval predictors of overall survival ( table 2 )  . 
the treatment e ect remained non - signi cant for overall survival after adjustment for the three prognostic variables ( hr 102 , 95% 081128 ; p = 089 )  . we recorded an improvement in disease - free interval for patients in the bevacizumab group compared with those in the observation group ( gure 3 )  . 
multivariable analysis identi ed disease stage , breslow the primary melanoma , trial group , and ecog performance status as independent predictors of disease - free interval ( table 2 )  . 
results from the analysis of disease - free interval were unchanged in a sensitivity analysis excluding the ineligible patients . thickness of braf status was available for 645 ( 48% ) patients ( table 1 )  . 
su cient material remained to undertake nras testing 239 ( 68% ) of 354 patients with braf wild - type ; 106 ( 44% ) of these patients had a mutation at codon 61 . 
the interaction between treatment and braf status was not signi cant ( p = 010 ) ; however , in patients with braf mutant tumours , we noted an improvement in the disease - free interval in those given bevacizumab ( gure 3 )  . 
diseasefree interval did not di er signi cantly between treatment groups in the wild - type braf population ( gure 3 )  . 180 grade 3 or 4 adverse events were recorded in 101 ( 15% ) of 671 patients in the bevacizumab group and 36 ( 5% ) of 672 patients in the observation group . 
 216 ( 32% ) patients had hypertension in the bevacizumab the disorder was generally group manageable ; we recorded grade 3 or 4 hypertension in 41 ( 6% ) patients ( table 4 )  . 
hypertension did not signi cantly a ect disease - free interval ( hr 085 , 95% ci 067109 ; p = 020 ) after adjustment for trial group . ( table 4 ) , but three adverse drug reactions were regarded as both serious and unexpected . 
 1215 ( 90% ) of 1343 patients returned at least two forms 624 vol 15 may 2014 articles bevacizumab observation and were included in the analyses : 592 ( 88% ) of 671 patients in the bevacizumab group and 623 ( 93% ) of 672 patients in the observation group . 
after bonferroni adjustment for multiple testing , no signi cant di erences were noted between treatment groups in the standardised area under the curve for any of the quality - of - life scales over 36 months ( table 5 )  . discussion our ndings show an improvement in disease - free interval with bevacizumab in patients with resected melanoma at high risk of recurrence as compared with observation alone . 
clearly , it will be important to ascertain whether this treatment e ect ultimately translates into a bene t in overall survival at nal analysis , which is follow - up driven and planned for when all patients have been on study for a minimum of 5 years , at which time 736 events are anticipated . 
the conditional power for futility of the primary outcome of overall survival at this interim analysis was 35% . to our knowledge , avast - m is one of the largest adjuvant melanoma trials and the largest bevacizumab monotherapy study ever undertaken ( panel )  . 
 patients and regulatory agencies increasingly value relapse - free survival as a primary endpoint in this setting , which is justi ed now that systemic therapies have been shown to improve overall survival in advanced disease.1921 however , when we started avast - m bevacizumab was a new drug with signi cant toxic e ects ( albeit reported mainly in combination with cytotoxic chemotherapy ) , and so we felt that a bene t in overall survival would need to be shown to change clinical practice . 
however , diseasefree interval in this trial could be indiciative of relapsefree survival , because only seven additional deaths from other causes without recurrence would have been included in an analysis of relapse - free survival ; these inclusions would not have changed the results from those reported for disease - free interval . identify the most frequently used adjuvant melanoma treatment worldwide is interferon alfa . 
 trials assessing di erent doses and formulations of interferon alfa have not identi ed the optimum adjuvant regimen this treatment is recognised to be associated with substantial toxic e ects , including liver dysfunction , fatigue , and depression.22 , 23 other immunotherapeutic strategies , including several vaccines , have been rigorously tested in patients with melanoma , with disappointing results overall.24 this outcome is exempli ed by the results of the derma randomised trial , in which a mage a3 vaccine did not improve relapse - free survival ( its rst coprimary endpoint ) in patients with resected stage iii melanoma expressing the mage a3 antigen.25 our results suggest that the extent of patient bene t o ered with bevacizumab might be similar to that with interferon alfa for the endpoint of relapse - free survival ( hr for interferon alfa 082 , 95% ci 077087 ) , but the overall survival bene t ( 089 , 082096 ) on ifterferon alfa was not noted with bevacizumab.2 at this interim analysis , few patients had received immunotherapy or targeted therapy at relapse , and the most common intervention was surgery . 
this nding is consistent with the high rate of locoregional recurrence as a result of the fairly low use of sentinel node biopsy and the inclusion of high risk primary tumours , together with the scarcity of active systemic therapy options 626 vol 15 may 2014 articles available until more recently . 
the e ect of subsequent treatments at relapse on overall survival is likely to be small at this time point , but will be of greater importance in the future . 
even so , the delay in melanoma recurrence noted with adjuvant bevacizumab in this trial might be clinically relevant . bevacizumab monotherapy seems to be well tolerated : grade 3 or 4 adverse events associated with bevacizumab were interferon , depending on the dose used , although cross - trial comparisons should be made with caution.22 , 23 those reported with fewer than interruptions around surgical there was no obvious safety signal associated with surgical interventions or haemorrhage to account for patients early discontinuation . 
the protocol speci ed interventions , dose requiring 28 days free from drug administration either side of any procedure , and preventing drug administration in the presence of any unhealed wound . 
drugassociated complications in wound healing seem to be negligible , and only a few patients failed to complete planned treatment due to unacceptable delays in wound healing , suggesting that , in routine clinical practice , withholding treatment in such circumstances need not be so stringent . 
withdrawal rates will be a ected by the duration of intended treatment , but low - level chronic side - e ects in an otherwise t population might account for patients electing to stop prematurely and this should be considered in future adjuvant trial designs . 
a placebocontrolled trial might have improved patient willingness to remain on treatment for longer , but the additional cost of a placebo would have been prohibitive in this charityfunded trial . multivariate analyses of disease - free interval and overall survival were undertaken to explore whether some subsets of patients were more likely to bene t from therapy than others . 
disease stage and breslow thickness were the most signi cant predictors of disease - free interval ; disease stage and ecog performance status were the most signi cant predictors of overall survival . 
a tenth of patients had an ecog performance status score of 1 on trial entry ; the reason for their poor outcome is not apparent , but will be assessed fully in the nal analysis . avast - m includes a prespeci ed translational study , aimed at identifying predictive and prognostic biomarkers . 
firm conclusions about whether bevacizumab might result in a longer disease - free interval for the subgroup of patients with braf mutant tumours cannot yet be made , but further analysis will be including multivariate analyses undertaken at the nal analysis . 
investigation into the biological basis for this initially unexpected nding is ongoing , but it is consistent with emerging evidence of the map kinase pathway playing a role in the control of vegf expression . 
 * an additional three patients ( one in the bevacizumab group and two in the observation group ) who died of melanoma before details of their recurrence being reported are included in the analyses of disease - free interval . 
adverse events are recorded for all patients who had an event of grade 3 or 4 severity and include any other adverse events that were recorded in 10% or more patients . 
if this mechanism applies to melanomas in human beings , it would provide a basis for the selection of patients for bevacizumab therapy , and a rationale for future potential combination regimens . trials three testing adjuvant bevacizumab combination with chemotherapy have been reported in patients with colon27 , 28 and breast cancer.29 all three trials had disease - free survival as the primary endpoint , and none identi ed any improvement . 
both immunological and angiogenic biomarkers are now being explored with tumour and blood samples collected from most patients recruited to the avast - m trial . 813 ( 681896 ) 819 ( 688911 ) 026 data are median ( iqr ) , unless otherwise indicated . 
p values less than 0003 would be signi cant after adjustment with bonferroni correction for multiple testing . table 5 : quality of life standardised area - under - curve analyse 628 vol 15 may 2014 articles panel : research in context systematic review an international standard adjuvant therapy for patients at risk of melanoma recurrence has not yet been established . 
 we searched pubmed for clinical trials published in english between jan 1 , 2000 and feb 1 , 2014 , assessing systemic therapy speci cally in melanoma , with the search terms melanoma and adjuvant . 
inhibition of angiogenesis as an adjuvant strategy has not previously been tested in melanoma patients . interpretation to our knowledge , avast - m is the rst phase 3 trial assessing bevacizumab as adjuvant therapy for melanoma and the largest bevacizumab monotherapy every undertaken . 
longer follow - up is needed to identify the e ect of bevacizumab on overall survival at 5 years . e ective treatment to prevent melanoma relapse remains an unmet need . 
the results of these trials , alongside the nal results of the avast - m trial , will have a key role in identifying future adjuvant strategies for this disease . contributors pc was the chief investigator , responsible for the trial design , trial management , data interpretation , and preparation of the manuscript . 
 am was the trial statistician who analysed the data , created the tables and gures , and contributed to the trial design , trial management , data interpretation , and preparation of the manuscript . 
all authors participated in the revision and nalisation of the manuscript . declaration of interests pc has received nonnancial support from f ho man la roche , grants from cancer research uk during the study , and personal fees and nonnancial support from f ho man la roche outside the submitted work . 
 mrm has received grants from cancer research uk during the study , personal fees from amgen , grants and personal fees from f ho man la roche , grants from astrazeneca , grants and personal fees from glaxosmithkline , institution study fees from novartis , institution study fees from astellas , institution study fees from millenium , institution study fees from immunocore , personal fees and institution study fees from bristol myers squibb , institution study fees from vertex , personal fees and institution study fees from eisai , institution study fees from abbott , institution study fees from clovis , institution study fees from p zer , institution study fees from merck , outside the submitted work . 
pl reports being a remunerated consultant to f ho man la roche for unrelated product and support for travel from f ho man la roche , outside the submitted work . 
all other authors declare that they have no competing interests . acknowledgments we thank all the patients who participated in the avast - m trial ; all investigators and their research teams ; colleagues working in regional cancer networks responsible for referring patients ; and the avast - m trial coordination team and the national cancer research institute melanoma clinical studies group for their adoption of the trial and support . 
national institutes for health research funding to the national clinical research network , biomedical research centres and experimental cancer medicine centres contributed to the undertaking of this trial in various sites . 
 bevacizumab was provided free of charge by f ho man la roche , basel , switzerland . articles e ects of the addition of gemcitabine , and paclitaxelrst sequencing , in neoadjuvant sequential epirubicin , cyclophosphamide , and paclitaxel for women with high - risk early breast cancer ( neo - tango ) : an open - label , 22 factorial randomised phase 3 trial helena m earl , anne - laure vallier , louise hiller , nicola fenwick , jennie young , mahesh iddawela , jean abraham , luke hughes - davies , ioannis gounaris , karen mcadam , stephen houston , tamas hickish , anthony skene , stephen chan , susan dean , diana ritchie , robert laing , mark harries , christopher gallagher , gordon wishart , janet dunn , elena provenzano , carlos caldas , for the neo - tango investigators summary background anthracyclines and taxanes have been the standard neoadjuvant chemotherapies for breast cancer in the past decade . 
we aimed to assess safety and e cacy of the addition of gemcitabine to accelerated paclitaxel with epirubicin and cyclophosphamide , and also the e ect of sequencing the blocks of epirubicin and cyclophosphamide and paclitaxel ( with or without gemcitabine )  . methods in our randomised , open - label , 22 factorial phase 3 trial ( neo - tango ) , we enrolled women ( aged > 18 years ) with newly diagnosed breast cancer ( tumour size > 20 mm ) at 57 centres in the uk . 
patients were randomly assigned via a central randomisation procedure to epirubicin and cyclophosphamide then paclitaxel ( with or without gemcitabine ) or paclitaxel ( with or without gemcitabine ) then epirubicin and cyclophosphamide . 
207 ( 25% ) patients had in ammatory or locally advanced disease , 169 ( 20% ) patients had tumours larger than 50 mm , 413 ( 50% ) patients had clinical involvement of axillary nodes , 276 ( 33% ) patients had oestrogen receptor ( er ) - negative disease , and 191 ( 27% ) patients had her2 - positive disease . 
addition of gemcitabine did not increase pcr : 70 ( 17% , 95% ci 1421 ) of 404 patients in the epirubicin and cyclophosphamide then paclitaxel group achieved pcr compared with 71 ( 17% , 1421 ) of 408 patients who received additional gemcitabine ( p = 098 )  . 
receipt of a taxane before anthracycline was associated with improved pcr : 82 ( 20% , 95% ci 1624 ) of 406 patients who received paclitaxel with or without gemcitabine followed by epirubicin and cyclophosphamide achieved pcr compared with 59 ( 15% , 1118 ) of 406 patients who received epirubicin and cyclophosphamide rst ( p = 003 )  . 
grade 3 toxicities were reported at expected levels : 173 ( 21% ) of 812 patients who received treatment and had full treatment details had grade 3 neutropenia , 66 ( 8% ) had infection , 41 ( 5% ) had fatigue , 41 ( 5% ) had muscle and joint pains , 37 ( 5% ) had nausea , 36 ( 4% ) had vomiting , 34 ( 4% ) had neuropathy , 23 ( 3% ) had transaminitis , 16 ( 2% ) had acute hypersensitivity , and 20 ( 2% ) had a rash . 
86 ( 11% ) patients had grade 4 neutropenia and 3 ( < 1% ) had grade 4 infection . interpretation although addition of gemcitabine to paclitaxel and epirubicin and cyclophosphamide chemotherapy does not improve pcr , sequencing chemotherapy so that taxanes are received before anthracyclines could improve pcr in standard neoadjuvant chemotherapy for breast cancer . funding cancer research uk , eli lilly , bristol - myers squibb . introduction survival of patients with early breast cancer has improved substantially in the past 20 years.1 however , incidence of breast cancer has increased and continuesto be a major health proble the early breast cancer trialists collaborative group overview analyses , 2 , 3 and individual trial data have shown bene t for adjuvant anthracyclines46 and taxane - containing chemotherapy.79 progress made through large adjuvant randomised treatment trials has been relatively slow . 
follow - up is necessarily prolonged to meet the prespeci ed eventrate criteria for disease - free survival ( dfs ) and overall vol 15 february 2014 lancet oncol 2014 ; 15 : 20112 published online december 19 , 2013 s1470 - 2045 ( 13 ) 70554 - 0 see comment page 131 copyright earl et al . 
tango11 and neo - tango were designed to provide this cross reference , because both trials investigated the addition of gemcitabine to standard chemotherapy , although the sequence of chemotherapy was not addressed in tango . neo - tango was a randomised phase 3 neoadjuvant trial that aimed to assess bene ts of addition of gemcitabine to accelerated paclitaxel with epirubicin and cyclophosphamide , and also the e ect of sequencing of epirubicin and cyclophosphamide , and paclitaxel ( with and without gemcitabine ) blocks . 
gemcitabine is an e ective drug in metastatic disease12 , 13 and other neoadjuvant or adjuvant trials have addressed similar questions for antimetabolites , with gemcitabine14 , 15 or oral capecitabine.16 neo - tango was designed and started before the introduction of adjuvant trastuzumab for her2 - positive disease . methods study design and participants in the neo - tango phase 3 randomised trial , we used a 2 2 factorial design to address both the role of gemcitabine in a sequential neoadjuvant chemotherapy regimen of epirubicin and cyclophosphamide and paclitaxel , and also the sequence of administration of these treatment components , in terms of short - term and long - term outcomes in women presenting with early breast cancer . ipsilateral supraclavicular regarded hormone we enrolled women aged older than 18 years with a histological diagnosis of early invasive breast cancer , with a radiological tumour size of more than 20 mm with or without axillary involvement . 
women with in ammatory cancer , t4 tumours with direct extension to the chest wall or lymph - node skin , and involvement were eligible with any size of primary tumour . 
her2 status was regarded as positive when immunohistochemistry was 3 + , or 2 + with evidence of ampli cation of the her2 gene on uorescence in - situ hybridisation . 
other eligibility criteria were adequate cardiac function , no myocardial infarction during the previous 6 months , adequate bone marrow , hepatic , and renal function , and appropriate ecog performance status ( 02 )  . 
patients provided written informed consent . neo - tango was an investigator designed and led trial , which was granted clinical trials authorisation from the medicines and healthcare products regulatory agency ( mhra ) on june 17 , 2004 , and approved by the multicentre research ethics committee nationally on nov 1 , 2004 , and subsequently the local research ethics committees at all participating centres . 
the study was undertaken by the uk national cancer research institute ( ncri )  . randomisation and masking in our open - label trial , eligible participants were randomly allocated 1 : 1 : 1 : 1 to receive epirubicin and cyclophosphamide followed by paclitaxel , paclitaxel followed by epirubicin and cyclophosphamide , epirubicin and cyclophosphamide followed by paclitaxel and gemcitabine , or paclitaxel and gemcitabine followed by epirubicin and cyclophosphamide . 
strati cation by minimisation was undertaken by age ( 50 years and > 50 years ) , er status ( positive and negative ) , primary tumour size ( 5 cm and > 5 cm ) , clinical involvement of axillary nodes , and in ammatory or locally advanced disease . 
chemotherapy regimens used were epirubicin 90 mg / m and cyclophosphamide 600 mg / m once every 21 days , and paclitaxel 175 mg / m with or without gemcitabine 2000 mg / m once every 14 days . 
 treatment allocations were made by telephoning the cancer research uk trials unit ( birmingham , uk ) , who used their central computerised minimisation procedure to generate the patients random allocation . procedures our primary endpoint was pcr , de ned as absence of invasive breast cancer in the breast and axillary lymph nodes , after neoadjuvant chemotherapy . 
a two - reader review of pathology reports was undertaken , masked to treatment group , by the chief investigator ( hme ) and the study pathologist ( ep ) , for patients who had surgery . 
 a detailed analysis of this review process has been published elsewhere.17 residual non - invasive ductal carcinoma in situ was allowed . secondary endpoints reported here include dfs and overall survival . 
we also recorded use of growth factor support ( usually granulocyte colony stimulating factor [ gcsf ] )  . the maximum permitted dose delay or interruption was 4 weeks to allow recovery from severe toxicity or for unscheduled procedures ( eg , emergency surgery )  . if neutropenic fever or sepsis occurred after a cycle of chemotherapy , the next cycle was delayed until the absolute neutrophil count was at least 10 10 cells per l . 
 following a delay , either dose reduction of all drugs to 202 vol 15 february 2014 articles 80% , or gcsf support with 100% dose were allowed , and all remaining cycles of the same four - cycle block were given at those doses . 
for persistent thrombocytopenia , the next cycle was delayed until patients had at least 100 10 platelets per l and was reduced to 80% , maintaining this dose reduction for subsequent cycles . 
once started , prophylactic gcsf was usually continued into the second phase of chemotherapy at the discretion of the responsible physician . if grade 2 neuropathy occurred during treatment with paclitaxel , remaining doses were reduced to 135 mg / m ( gemcitabine was unchanged )  . 
her2 - negative de ned as immunohistochemistry score of 01 , or 2 , but uorescence in - situ hybridisation ( fish ) negative ; her2 - positive de ned as immunohistochemistry of 3 or 2 and fish positive . 
each tumour could have multiple types and characteristics recorded . table 1 : patient and tumour characteristics at baseline of six cycles in total , at the discretion of the treating consultant . gemcitabine was reduced to 80% in the event of grade 3 hepatic toxicity ( transaminitis ; aspartate aminotransferase or alanine aminotransferase 520 upper limit of normal [ uln ] ) on day of treatment , at clinicians discretion because transaminitis is not known to a ect gemcitabine clearance . 
we were unable to substantiate earlier concerns about gemcitabines potential for clinically signi cant hepatic impairment . cardiac toxicity was not anticipated at the cumulative doses of epirubicin of 360 mg / however , congestive cardiac failure developed , patients were investigated and treated as appropriate , epirubicin was discontinued , and other chemotherapy was given at the discretion of the treating clinician . in the event of gemcitabine - related pulmonary toxicity of ctcae grade 2 or worse , the patient was discontinued from study therapy . paclitaxel infusion was stopped if mild symptoms of skin rash , ushing , and localised pruritus occurred . 
 if severe symptoms occurred , including bronchospasm , generalised urticaria , angio - oedema , hypotension ( systolic blood pressure < 100 mm hg ) , or life - threatening infusion was stopped and anaphylaxis , paclitaxel treatment was given with intramuscular epinephrine 1 ml 1 : 1000 , intravenous steroids , and intravenous antihistamines ; rechallenge was contraindicated . surgery ( breast and axillary ) , radiotherapy , and adjuvant endocrine treatment were given according to local protocols . 
patients will continue to receive the national cancer intelligence network ( ncin ) who will monitor for dfs and overall survival . follow - up through statistical analysis our power calculations assumed that the pcr would be 20% after standard treatment ( epirubicin and cyclophosphamide followed by paclitaxel )  . 
on this basis , we aimed to randomly allocate 200 patients into each of the four treatment groups , yielding combined data for 400 patients into each group for the two questions ( ie , e cacy and safety of the addition of gemcitabine to paclitaxel plus epirubicin and cyclophosphamide treatment [ component analysis ] and order of chemo therapy regimens [ sequencing analysis ] )  . 
this would allow an absolute di erence in the pcr in excess of 10% to be detected at the 5% ( two - sided ) level of signi cance with 85% power . 
all reported p values are two - sided . vol 15 february 2014 articles for the primary analysis , we calculated pcr for all logistic treatment groups and used univariate regression to test the addition of gemcitabine and the role of sequencing . 
we used multivariate logistic regression to calculate p values for both the treatment and scheduling e ects after adjustment for prognostic factors . we calculated dfs from the date of randomisation to the date of rst event ( locoregional relapse , distant relapse , progression on neoadjuvant chemotherapy , or death ) , or to the date of censoring . 
we calculated overall survival from the date of randomisation to the date of death or to the date of each patients last clinic visit ( for women who are not known to have died )  . 
when assessing the association between pathological response and these outcomes , we calculated overall survival and dfs from date of surgery . the neo - tango protocol stated that the rst planned interim analysis of dfs and overall survival would occur when at least 120 events had occurred or when median follow - up was at least 3 years . 
the corresponding authors ( hme and lh ) had full access to all of the data and had nal responsibility for the decision to submit for publication . results between jan 18 , 2005 , and sept 28 , 2007 , we recruited 831 patients at 57 centres ; three patients were found to be ineligible after randomisation , leaving 828 for analysis ( gure 1 ; table 1 )  . 
adjusted for the ve strati cation variables ( age , er status , tumour size , clinical involvement of axillary nodes , and in ammatory or locally advanced disease )  . 
 tumour grade of each patients largest breast tumour at baseline . table 2 : rates of pathological complete response ( pcr ) 206 vol 15 february 2014 articles see online for appendix omission of the nal cycle of chemotherapy , with the patient proceeding straight to surgery . because the neo - tango protocol did not include neoadjuvant trastuzumab , we expected fewer patients with her2 - positive disease to enrol as the trial progressed . 
 107 patients enrolled in 200506 had her2 - positive disease ( 30% of the 357 tested ) compared with 84 in 2007 ( 24% of the 347 tested ; p = 019 )  . all patients had surgery ( breast and axilla ) according to local protocols and the details will form the basis of a future publication . 
all patients with er - positive disease ( 543 [ 67% ] patients were er - positive ) received appropriate adjuvant hormonal treatments and 750 patients ( 91% ) received radiotherapy treatments according to local protocols . 
141 ( 17% ) of these patients had pcr , which was much the same for patients in the epirubicin and cyclophosphamide plus paclitaxel , and the epirubicin and cyclophosphamide plus paclitaxel and gemcitabine groups ( between - group di erence 007% , 95% ci 5 to 5 ; table 2 )  . 
however , signi cantly more patients who received paclitaxel ( with or without gemcitabine ) before epirubicin and cyclophosphamide achieved pcr than did those who received epirubicin and cyclophosphamide rst ( between group di erence 6% , 05 to 11 ; table 2 )  . 
subgroup analysis by her2 status , er status , or tumour grade did not a ect the results ( table 2 , appendix )  . median follow - up was 47 months ( iqr 3751 )  . 
at the time of analysis , 167 ( 20% ) of the 828 eligible patients had died , 227 ( 27% ) had had locoregional or distant relapses , and 236 ( 29% ) had had dfs events . 
702 ( 86% ) of the remaining 812 patients received eight cycles of chemotherapy ; the main reasons for not receiving all eight cycles were toxicity ( 54 [ 49% ] of the 110 patients receiving between one and seven cycles ) , disease progression ( 28 [ 25% ] patients ) , allergic reaction to paclitaxel ( 15 [ 14% ] patients ) , poor response to chemotherapy ( seven [ 6% ] patients ) , or other reasons ( six [ 5% ] patients )  . the median cddi for the 819 patients was 97% ( iqr 9199% )  . 
no di erences between the component groups or the sequencing groups were detected ( p = 056 for component analysis and p = 018 for sequencing analysis )  . dose intensities over individual cycles did not notably deteriorate for any of the four randomised treatment groups ( appendix )  . 
more dose reductions for the fourth cycle of regimens containing paclitaxel ( with or without gemcitabine ) occurred when it was given second compared with prior administration ( 22% vs 10% , respectively ; appendix ) , and similarly for dose delays ( 15% vs 11% , respectively ; appendix )  . overall survival from surgery was longer for patients attaining pcr than it was for those who did not attain pcr ( gure 3 )  . 
grade 3 toxicities included neutropenia , muscle and joint pain , infection , neuropathy , transaminitis , fatigue , nausea and vomiting , rash , and acute hypersensitivity ( table 3 )  . 
one patient in the epirubicin and cyclophosphamide followed by paclitaxel group received only ve cycles of chemotherapy because of fatigue and anaphylaxis and then died 12 weeks later of respiratory failure ( distant recurrence with bilateral pleural e usion and extensive alveolar shadowing )  . 
 = no reported toxic e ects of this grade . table 4 : reported grade 4 severe toxic e ects discussion in our study , provision of a taxane before standard anthracycline chemotherapy was associated with a signi cant improvement in pcr , from 15% to 20% , compared with a standard anthracyclinerst sequence ( p = 003 ; panel )  . 
these ( p < 00001 ) and overall survival improvement ndings con rm the bene t of taxanerst sequencing that was noted in a large retrospective non - randomised study from the md anderson cancer center , tx , usa , 19 which reported data from 1414 patients treated with neoadjuvant chemotherapy and 1596 patients treated with adjuvant chemotherapy between 1994 and 2009 . 
 in addition all major international early breast cancer trials groups were contacted to discuss our proposed design of epirubicin and cyclophosphamide , and dose - dense paclitaxel with or without gemcitabine . 
the nsabp - b38 adjuvant trial had a similar experimental arm with dose - dense doxorubicin and cyclophosphamide , and dose - dense paclitaxel ( 175 mg / m every 2 weeks ) with or without gemcitabine ( 2000 mg / m every 2 weeks )  . 
in addition , neo - tango had a complementary adjuvant trial ( tango ) which also addressed the addition of gemcitabine . interpretation neo - tango con rms the nsabp - b38 , 14 nsabp - b40 , 15 and tango11 results , which show no bene t from the addition of gemcitabine to anthracycline and taxane - based chemotherapy treatments for early breast cancer . 
neo - tango shows a signi cant bene t from taxanerst sequencing , and is the largest randomised trial to con rm this e ect . 314 patients have been included in small randomised phase 2 adjuvant trials2024 and 276 patients have been included in neoadjuvant trials2528 addressing taxane and anthracycline sequencing . 
some of these studies report more dose reductions of taxane when anthracyclines are given rst , 2123 , 25 and one randomised neoadjuvant study showed a non - signi cant increase in incidence of pcr for taxanerst sequencing.27 indirect evidence from neoadjuvant randomised studies for taxanerst sequencing comes compared uorouracil , epirubicin , and cyclophosphamide with docetaxel followed by epirubicin and docetaxel . 
however , the neo - tango analysis showed no sequence - speci c di erence in cddi to explain this taxanerst sequence result . 10994 , 28 which from eortc preclinical and clinical studies have suggested mechanisms to explain the bene t of early receipt of taxanes . 
taghian and colleagues26 drew attention to increases in interstitial uid pressure and improved oxygenation within breast tumours after neoadjuvant paclitaxel , which might allow increased concentrations of anthracyclines to accumulate within tumour tissue when given afterwards . 
in addition , preclinical data show that in breast cancer cells with heat shock protein 27 overexpression , a paclitaxel then doxorubicin sequence is more e ective at cell killing than the more standard doxorubicin then paclitaxel sequence.31 taxanerst sequences allow early treatment with concomitant trastuzumab and bevacizumab , which might provide additional therapeutic advantage , shown for trastuzumab in the finher study.32 both the nsabp - b4015 and artemis33 trials of bevacizumab have adopted taxanerst sequencing for this reason . 
because all patients receive both the taxane and anthracycline components , taxanerst sequencing could be considered in all similar block - sequential adjuvant and neoadjuvant protocols . neo - tango con rms the result of tango11 and shows no signi cant bene t from addition of gemcitabine to a combination that already contains anthracycline , cyclophosphamide , and paclitaxel . 
however , gemcitabine has shown promising results in patients with metastatic disease when added to paclitaxel in the rst - line relapse setting.13 much the same results have already been reported in the adjuvant nsabp - b38 , 14 and neoadjuvant nsabp - b4015 studies . 
 gemcitabine was given at 666 mg / m per week ( compared with 1000 mg / m per week in neotango and nsabp - b38 ) and docetaxel doses were reduced to 75 mg / m , and showed no bene t in terms of pcr . 
in neo - tango , we noted a non - signi cant increase in pcr after the addition of gemcitabine in patients with highgrade disease ( table 2 )  . paclitaxel was delivered every 14 days at 175 mg / m ( with or without gemcitabine 2000 mg / m )  . 
this dose - dense protocol was delivered without any reported delays in 82% of paclitaxel - containing cycles and only 8% of cycles required growth factor support to maintain dose intensity . 
the use of neoadjuvant or adjuvant weekly paclitaxel is now often used as standard at 80 mg / m per week and therefore the taxanerst sequencing bene t seen in neo - tango with paclitaxel at 875 mg / m per week , is close to standard practice across the world . whether pcr in neoadjuvant trials can be a surrogate endpoint for dfs and overall survival has been debated . 
 von minckwitz and colleagues meta - analysis34 of 6377 patients in the german breast group and abobsg neoadjuvant chemotherapy the prognostic value of not achieving a pcr is most dependent on the molecular subtype of the original trials showed that 210 vol 15 february 2014 articles trastuzumab , whereas none of tumour . 
for luminal a subtype , 35 a meta - analysis included 46% of patients in this category with pcr of 89% , whereas neo - tango had 29% luminal a patients with pcr of 35% . 
in addition , 662 ( 50% ) of 1327 patients with her2 - positive disease in the meta - analysis received the neoadjuvant 187 patients with her2 - positive disease in neo - tango did . 
the metaanalysis shows pcr of 358% in 911 patients , although in a recent trial ( gepar quinto ) , 36 663 patients with triplenegative breast cancer had a pcr of 279% , increasing to 393% chemotherapy . 
the pcr for 94 such patients in neotango was 39% with the addition of gemcitabine and 40% with taxanerst sequence . addition of bevacizumab after the in the z1040 - alliance neoadjuvant study , 37 280 patients with her2 - positive breast cancer were randomly allocated to receive standard uorouracil , epirubicin , and cyclophosphamide followed by weekly paclitaxel with trastuzumab ( pcr in the breast 565% ) , and a taxanerst sequence with concurrent weekly trastuzumab throughout ( pcr in the breast 542% )  . 
however in neotango , 187 patients with her2 - positive disease had a pcr for taxanerst sequence of 26% compared with 17% for standard sequence ( p = 003 ; table 2 )  . 
notably , in neotango , in 121 er - positive , her2 - positive women , pcr was 28% for taxanerst sequencing and 9% for anthracyclinerst sequencing , and in 66 er - negative , her2 - positive women pcr was 23% for taxanerst sequencing and 32% for anthracyclinerst sequencing . 
however , the di erences between the neotango results and z1040 could be explained by the absence of neoadjuvant trastuzumab in neo - tango . the association a recent meta - analysis38 by the us food and drug administration ( fda ) con rms the strong correlation between pcr and dfs and overall survival in patients achieving a pcr , and this association was con rmed in neo - tango . 
 the fda proposed that pcr in neoadjuvant trials in highly proliferative breast cancers could now contribute to accelerated drug approval in these types of early breast cancer.39 this proposal is a landmark in neoadjuvant chemotherapy trials for highly proliferative breast cancer , and will facilitate more rapid introduction of new agents for this subtype . 
randomised neoadjuvant trials of chemotherapy in combination with target - directed novel agents will be able to focus on high proliferation molecular subtypes ( er - negative , her2 - positive , high grade , and patients with germline brca mutations ) in which the association between pcr and dfs and overall survival is expected to be correlated . 
 however , indicates the fda meta - analysis also subgroups of breast cancer with lower proliferative potential ( ie , er - positive , her2 - negative , low and intermediate grade ) that have a better prognosis independent of pcr . 
in these groups , the response to chemotherapy is poor and pcr is low but the long - term outcome is good , and survival is in uenced more by subsequent adjuvant hormonal treatment . 
in neotango , patients from all the di erent prognostic groups were included , and therefore the pro le of the trial population will weaken the correlation between pcr and long - term outcomes for the group as a whole . 
for patients with a previously known poor prognosis , who have high pcr incidence , a robust and reliable correlation will probably emerge between pcr and longer - term outcome . contributors hme , a - lv , lh , gw , jd , and cc designed the study and wrote grant applications . 
all authors collected data , revised the report and agreed to submit the paper for publication . con icts of interest this project was funded by cancer research uk ( project grant c57 / a4180 , 2004 - 2009 ) and was supported by the national cancer research network . 
all other authors declare that they have no con icts of interest relevant to this publication . acknowledgments we acknowledge 88 investigators and their teams from 57 participating centres who entered patients in neo - tango . 
we also thank the members of the data and safety monitoring board ( i craig henderson [ university of california , san francisco , ca , usa ] , luca gianni [ unit of new drugs and innovative therapies , department of medical oncology , san ra aele hospital , irccs , milan , italy ] , and mark f brady [ gynecologic oncology group statistical & data center , roswell park cancer institute , bu alo , ny , usa ] ) , and trials unit sta for the phase 3 coordination ( cancer research uk clinical trials unit , birmingham , uk ) , translational coordination ( university of cambridge , addenbrookes hospital , cambridge , uk ) , and statistical analysis ( warwick clinical trials unit , coventry , uk )  . correction to lancet oncol 2017 ; 18 : 132737 correction to lancet oncol 2017 ; 18 : 133847 correction to lancet oncol 2017 ; 18 : e564 dimopoulos ma , goldschmidt h , niesvizky r , et al . 
 lancet oncol 2017 ; 18 : 132737in the results section of this article , the data presented for any - grade adverse diarrhoea events should read diarrhoea ( 168 [ 36% ] vs 185 [ 41% ] )  . 
 these corrections have been made to the online version as of sept 27 , 2017 , and the printed article is correct . myelodysplastic in patients with platzbecker u , germing u , gtze ks , et al . 
luspatercept for the treatment of anaemia lowerrisk syndromes ( pace - mds ) : a multicentre , openlabel phase 2 dose - finding study with long - term extension study . 
 18 : e564in the second paragraph of brian samuels affiliation , the sentence in parentheses should have read ( summit cancer centers , post falls , id , usa )  . 
in the third paragraph , the sentence and quote from brian samuels as should have samuels summarised , we decided to recapitulate the original phase 2 study in liposarcomas pazopanib is active in the treatment of liposarcomas , just as it is for other subtypes of sarcoma . 
 these corrections has been made to the online version as of sept 27 , 2017 . vol 18 october 2017 e562 corrections correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 chemoradiotherapy with or without cetuximab in patients with oesophageal cancer ( scope1 ) : a multicentre , phase 2 / 3 randomised trial thomas crosby * , christopher n hurt * , stephen falk , simon gollins , somnath mukherjee , john sta urth , ruby ray , nadim bashir , john a bridgewater , j ian geh , david cunningham , jane blazeby , rajarshi roy , tim maughan , gareth gri ths summary background de nitive chemoradiotherapy ( crt ) is an alternative to surgery for the curative treatment of oesophageal carcinoma . 
the scope1 trial aimed to investigate the addition of cetuximab to cisplatin and uoropyrimidine - based de nitive crt in patients with localised oesophageal squamous - cell cancer and adenocarcinomas to assess activity , safety , and feasibility of use . methods in this multicentre , randomised , open - label , phase 2 / 3 trial , we recruited patients aged 18 years and older from uk radiotherapy centres who had non - metastatic , histologically con rmed carcinoma of the oesophagus ( adenocarcinoma , squamous - cell , or undi erentiated ; who status 01 ; stage iiii disease ) and been selected to receive de nitive crt . 
patients were randomly assigned ( 1 : 1 ) via a central computerised system using strati ed minimisation ( with an 80 : 20 random element ) to receive crt alone or crt with cetuximab ( 400 mg / m on day 1 followed by 250 mg / m weekly ) , strati ed by recruiting hospital , primary reason for not having surgery , tumour histology , and tumour stage . 
crt consisted of cisplatin 60 mg / m ( day 1 ) and capecitabine 625 mg / m twice daily ( days 121 ) for four cycles ; cycles three and four were given concurrently with 50 gy in 25 fractions of radiotherapy . 
 the primary endpoint was the proportion of patients who were treatment failure free at week 24 for the phase 2 trial and overall survival for the phase 3 trial , both measured from randomisation . 
 this trial is an international standard randomised controlled trial , number 47718479 . findings 258 patients ( 129 assigned to each treatment group ) from 36 uk centres were recruited between feb 7 , 2008 , and feb 22 , 2012 . 
recruitment was stopped without continuation to phase 3 because the trial met criteria for futility , but we continued to follow - up recruited patients until all had reached at least 24 - week follow - up ( median follow - up of patients who survived was 168 months [ iqr 112245 ] )  . 
fewer patients were treatment failure free at 24 weeks in the crt plus cetuximab group ( 79 of 119 patients [ 664% , 90% ci 586736 ] ) than in the crt only group ( 93 of 121 patients [ 769% , 697830 ] )  . 
the crt plus cetuximab group also had shorter median overall survival ( 221 months [ 95% ci 151245 ] vs 254 months [ 205379 ] ; adjusted hr 153 [ 95% ci 103227 ] ; p = 0035 )  . 
patients who received crt plus cetuximab had more non - haematological grade 3 or 4 toxicities ( 102 [ 79% ] of 129 patients vs 81 [ 63% ] of 129 patients ; p = 0004 )  . 
less often , patients or clinicians will opt for this strategy.8 increasingly , de nitive chemoradiotherapy is being considered as a standard of care in patients with oesophageal because evidence suggests that outcomes are similar to those of surgical treatment.3 , 6 , 9 by contrast , for adenocarcinomas , de nitive evi dence chemoradiotherapy is less strong and is restricted to studies of chemo radiotherapy in patients who are unsuitable for surgery . squamous - cell carcinoma , the use support concurrent chemoradiotherapy regimens have been based on cisplatin and uorouracil . 
both drugs have good single - agent activity in oesophageal malignant disease and are two of the best radiosensitisers in tumour models.10 , 11 the regimen used most frequently in the uk consists of conformal external beam radio therapy ( 50 gy in 25 fractions for 5 weeks ) with two cycles of cisplatin and uorouracil given concurrently , with or without a further two cycles of the same chemo therapy , given in a neoadjuvant phase . 
this neoadjuvant phase , as well as delivering additional systemic therapy , allows time for careful radiotherapy planning , frequently improves patients dysphagia , and debulks the tumour before radiotherapy . 
capecitabine has been shown to be as e ective as uorouracil in locally advanced and metastatic oesophagogastric cancer.7 encouraging outcomes with de nitive chemoradiotherapy regimens were reported in single - centre series , 8 , 12 but whether the ndings could be replicated in a prospective , multicentre trial was unclear . although de nitive chemoradiotherapy in patients with a poor outlook can lead to useful long - term disease control , most patients still succumb to the disease . 
the pattern of treatment failure di ers from that after surgery , with a higher rate of locoregional recurrence.6 , 8 , 9 , 12 improvements to both the systemic and locoregional components of this treatment strategy are therefore urgently needed . egfr is overexpressed in up to 55% of oesophagogastric cancers and is associated with poor prognosis.13 cetuximab , a monoclonal egfr antagonist , improved outcomes when given in combination with chemo therapy tumourseg , advanced colorectal adenoin other carcinomas14 and squamous - cell head and neck cancer.15 more importantly , preclinical studies have shown that cetuximab can overcome an important mechanism of radioresistance , 16 and results of a phase 3 trial by bonner and colleagues17 in squamous - cell carcinoma of the head and neck showed that cetuximab in combination with radiotherapy can improve local control and overall survival compared with therefore postulated that cetuximab in combination with conventional de nitive chemoradiotherapy might improve radiotherapy alone . 
on behalf of the uk national cancer research institute ( ncri ) upper gi clinical studies group we designed ( study of chemoradiotherapy in oesophageal cancer with erbitux ) to test this hypothesis . 
 the scope1 trial methods study design and patients in this multicentre , randomised , open - label , parallel , two - arm , phase 2 / 3 trial , we recruited patients from radiotherapy centres in the uk who had the following key eligibility criteria ( for full inclusion and exclusion criteria see appendix ) : non - metastatic , histologically con rmed carcinoma of the oesophagus ( adenocarcinoma , squamous - cell , or undi erentiated carcinoma ) or gastro - oesophageal junction ( siewert type 1 or 2 with < 2 cm extension into the stomach ) ; selected for de nitive chemoradiotherapy by a designated multidisciplinary team ; aged 18 years or older ; who performance status 0 or 1 ; stage iiii disease ( tnm stage 6 ) ; and disease length of less than 10 cm de ned by endoscopic ultrasound . 
the protocol for the study has been published elsewhere18 and the trial was coordinated by the wales cancer trials unit ( wctu )  . patients were required to have staging investigations that consisted of endoscopic ultrasound and contrastenhanced spiral ct scan of the thorax and abdomen . 
 patients were physiologically assessed to identify those with eligible lung function ( forced expiratory volume in 1 s > 10 ) , cardiac function ( left ventricular ejection fraction > 40% on echocardiogram or multigated acquisition scan ) , renal function ( edta glomerular ltration rate [ gfr ] > 40 ml / min , or estimated by cockcroft - gault formula to be > 60 ml / min ) , ( serum bilirubin liver function 15upper limit of normal [ uln ] , aspartate aminotransferase to alanine aminotransferase ratio 25uln , alkaline phosphatase 3uln ) and haematological assessment ( haemoglobin > 100 g / l , white blood cells > 310 / l , absolute neutrophil count [ anc ] > 1510 / l , platelet count > 10010 / l )  . 
all treatment and assessments were done in uk radiotherapy centres . all patients had to provide written informed consent before registration and the trial protocol was approved the uk medicines and healthcare products regulatory agency and a multicentre research ethics committee . 
cancer research uks clinical trials awards and advisory committee ( ctaac ) approved the trial design . 628 vol 14 june 2013 articles for the trial protocol see php ? trial = scope1 randomisation and masking eligible patients were randomly assigned ( 1 : 1 ) to chemoradiotherapy with cetuximab ( crt plus cetuximab ) or chemoradiotherapy without cetuximab ( crt only ) by strati ed minimisation with a random element ( 80 : 20 )  . 
to conceal the sequence until interventions were assigned , research nurses ( who recruited the patients ) telephoned the wctu where the random allocation sequence was generated by a trial or data manager interacting with a computerised syste the study had an open - label design . 
participants , those administering the interventions , and those assessing the outcomes were aware of which treatment had been allocated . procedures both study groups received the same chemotherapy , which consisted of four 3 - weekly cycles of cisplatin ( 60 mg / m intravenously on day 1 ) and capecitabine ( 625 mg / m orally twice daily from day 1 to day 21 ) ; cycles one and two were given as neoadjuvant treatment . 
patients randomly assigned to the crt plus cetuximab group also received intravenous cetuximab 400 mg / m on day 1 of chemotherapy and 250 mg / m weekly for the 12 weeks of treatment . 
if patients were unable to swallow capecitabine , investi gators could use a protracted intravenous infusion of uorouracil at a rate of 225 mg / m per day from day 1 to day 21 of each cycle . 
 full details of protocol treatment and dose reductions are detailed in the trial protocol . dose modi cation for haematological toxicity was based on a full blood counts taken within the 3 days before the start of each cycle of chemotherapy . 
for anc 0510 / l to less than 110 / l or a platelet count 5010 / l to less than 7510 / l , chemotherapy was stopped until recovery of counts and restarted with a 25% dose reduction of cisplatin and capecitabine . 
 cisplatin was given at a 75% dose reduction to patients with gfr of 4050 ml / min , and replaced by carboplatin ( at a concentration to achieve an area under the concentrationtime curve of 5 ) if gfr was below 40 ml / m capecitabine was given at a 75% dose reduction if gfr was below 50 ml / min , a 50% dose reduction if gfr was below 40 ml / min , and omitted if gfr was below 30 ml / m for other non - haematological toxicities of grade 2 or higher , chemotherapy was withheld until resolution to grade 01 . 
sequential dose reduction of cetuximab to 200 mg / m and 150 mg / m was advised for second and third occurrences of grade 3 skin rash , respectively ; it was permanently discontinued after a fourth appearance . the radiotherapy protocol and planning guidance document mandated the use of intravenous contrast ct simulation with minimum 3 - mm ct slices . 
50 gy in 25 fractions , prescribed according to recommendations by the inter national commission on radiation units and measure ments ( icru - 50 / 62 ) , was delivered monday to friday as a three - dimensional ( 3d ) conformally planned single - phase treatment , usually with four radiotherapy elds to achieve the following normal organ dose constraints : less than 30% of the heart volume to receive at least 40 gy , less than 25% of the lung volume to receive at least 20 gy , and a maximum dose in the spinal cord of less than 40 gy . 
elective nodal irradiation was not done . all potential principal investigators and radiotherapy centres received a cd - rom containing the detailed radio therapy planning radiotherapy protocol , guidance document , and example planning cases . 
all principal investigators had to outline a benchmark case 540 patients were assessed for eligibility 282 excluded 213 did not meet inclusion criteria 66 refused 3 other reasons 258 were randomly assigned 129 were assigned to chemoradiotherapy plus cetuximab 129 assigned to chemoradiotherapy only figure 1 : trial pro le vol 14 june 2013 articles radiotherapy and radiotherapy centres then planned the same case , which had to pass central review before patient recruitment.19 on - trial trials quality assurance ( rttqa ) consisted of all principal investigators rst plans , 10% of all subsequent plans , and trial - speci c planning assessment forms for each patient submitted for central review that outlined and assessed the 3d dose distribution before treatment . 
blood and biopsy samples were obtained at both baseline and week 24 , but the processing of these samples is still in progress , and correlations with treatment response will be the subject of a future paper . follow - up was at 24 weeks , then every 3 months after that during the rst year , every 4 months during the second year , and yearly thereafter for a minimum of 5 years from randomisation . 
we postulated that scores for physical and role function , fatigue , dysphagia , and eating restrictions would be better over time in the crt plus cetuximab group than in the crt only group . 
 a patient was deemed treatment failure free if they were still alive with no evidence of residual malignancy in the endoscopic biopsy sample , and no evidence of disease progression outside the radiotherapy eld on ct scan . 
using a flemings single - stage design ( p1 = 060 ; p2 = 075 ; = 005 ; 90% power ; 10% loss to follow up ) , we needed to recruit 90 patients in the crt plus cetuximab group ( 180 patients overall )  . 
subject to the independent data monitoring committees review of the phase 2 analysis , the study would proceed to phase 3 with a primary endpoint of overall survival from date of randomisation . 
for the phase 3 trial , we needed to recruit 420 patients ( 269 events ) to detect an improvement in 2 - year overall survival from 35% to 475% ( hazard ratio [ hr ] 071 ) in patients assigned to crt plus cetuximab , with 80% power at 5% signi cance . data were analysed with the stata 11 statistical package according to intention to treat . 
analyses of the proportion of patients who were treatment failure free were done using the number of patients who died or progressed before 24 weeks , or those with a valid 24 - week assess ment , as the denominator . 
detailed quality - of - life analyses , health economic analyses , and correl ation of outcomes with radiotherapy treatment delivery will be presented in future reports . this trial is an international standard randomised controlled trial , number 47718479 . role of funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the statistician ( ch ) had full access to all the data and the corresponding author ( tc ) and statistician ( ch ) had nal responsibility for the decision to submit for publication . 
merck serono provided the cetuximab free of charge but had no role in study design , data collection , data analysis , data interpretation or writing of the report . results 258 patients were recruited from 36 of the 56 radiotherapy centres in the uk between feb 7 , 2008 , and feb 22 , 2012 ( gure 1 )  . 
in february , 2012 , the independent data monitoring committee undertook a preplanned analysis of the rst 180 patients recruited who had completed 24 weeks of follow up , and recommended stopping recruitment because the trial had met predetermined criteria for futility . 
when making this decision , they also took into account toxicity , treatment compliance , and overall survival , and recommended completion of treatment and follow - up of all recruited patients . 
the data presented here are those from all 258 patients ( 129 patients allocated to each treatment group ) who were recruited up until the independent data monitoring committees decision , analysed after the last patient had undergone assessment at week 24 . 
the median length of follow - up for patients who had survived by the time of analysis was 168 months ( iqr 112245 )  . patient and tumour baseline characteristics were well balanced between groups ( table 1 )  . 
patients who were assigned to receive crt plus cetuximab were less likely to com plete standard protocol treatment than were those assigned to the crt only group ( table 2 )  . 
the com pliance di erence between groups was signi cant for completion ( at full or reduced dose ) of four planned cycles of cisplatin ( p = 0005 ) , completion of four cycles of capecitabine ( p = 0002 ) , and delivery of any radiotherapy ( 104 [ 81% ] of 129 patients in the crt plus cetuximab group vs 119 [ 92% ] of 129 patients in the crt only group ; p = 0006 ; table 2 )  . 
 the number of patients whose cisplatin dose was reduced ( or stopped ) was similar in each group ( 56 [ 43% ] in the crt plus cetuximab group vs 60 ( 47% ) in the crt only group )  . 
the number of patients whose capecitabine dose was reduced was higher in the crt plus cetuximab group than in the crt only group ( 97 [ 75% ] vs 85 [ 66% ] )  . 
 more patients in the crt plus cetuximab group stopped both cisplatin and capecitabine treatment early because 632 vol 14 june 2013 articles crt plus cetuximab crt only of toxicity or illness than did those in the crt only group ( cisplatin stopped , 26 [ 20% ] vs 12 [ 9% ] ; capecitabine stopped , 36 [ 28% ] vs 19 [ 15% ] )  . all ctcae grade 3 or 4 toxicities ( including serious adverse reactions and suspected unexpected serious adverse reactions ) reported during treatment are shown in table 3 . 
these toxicities were mainly dermatological , biochemical ( metabolic or laboratory tests ) , and cardiac disorders ( table 3 )  . the proportion of patients who were treatment failure free at 24 weeks was lower in the crt plus cetuximab group than in the crt only group ( 79 of 119 patients [ 664% , 90% ci 586736 ] vs 93 of 121 patients [ 769% , 697830 ] )  . 
patients who were failure free at 24 weeks had signi cantly better median overall survival than did those who were not failure free ( 83 months [ 95% ci 67125 ] vs 267 months [ 245427 ] )  . 
of those patients who were failure free at 24 weeks , 107 ( 62% ) of 172 were still alive without progression at the end of the study follow - up , whereas 40 ( 23% ) were alive with progression and 25 ( 15% ) had died . 
of patients who died before 24 weeks , more were recorded as having oesophageal cancer as the cause of death in the crt plus cetuximab group than in the crt only group ( table 4 )  . 
29 patients are known to have had further treatment during the 12 months after randomisation ( table 4 )  . overall survival was signi cantly worse in the crt plus cetuximab group than in the crt only group ( unadjusted hr 145 [ 95% ci 101209 ] , log - rank p = 0043 ; adjusted hr 153 [ 103227 ] , p = 0035 ; gure 2 )  . 
2 - year overall sur vival was also lower in the crt plus cetuximab group than in the crt only group ( 413% [ 95% ci 309514 ] vs 560% [ 451656 ] ) , as well as median progression - free survival , but not signi cantly so ( 159 months [ 95% ci 110211 ] vs 216 months [ 162278 ] ; un adjusted hr 126 [ 95% ci 090177 ] , 129 [ 089185 ] , p = 018 ) , median distant progression - free survival ( 184 months [ 133232 ] vs 254 months [ 184293 ] ) , survival local progression - free ( 159 months [ 110211 ] vs 216 [ 162278 ] )  . log - rank p = 017 ; adjusted hr and figures 4 and 5 show the results of the quality - of - life analysis . 
 a completion rate of 69% or above was maintained at week 13 ( 184 [ 71% ] completed qlq - c30 and 178 [ 69% ] completed qlq - oes18 ) ; the major reason for loss to follow - up was attrition . 
the change in the fol lowing number at risk crt plus cetuximab crt only months from randomisation figure 2 : kaplan - meier curves of overall survival by treatment group crt = chemoradiotherapy . reason for no surgery local extent of disease patient choice comorbidity / poor performance status tumour type adenocarcinoma squamous cell other stage deaths survival ( months ) 222 ( 161254 ) 247 ( 200303 ) 232 ( 128nc ) 197 ( 147258 ) 240 ( 205278 ) 303 ( 197nc ) 207 ( 169247 ) favours crt + cetuximab favours crt only figure 3 : hazard ratio plots for overall survival , by baseline characteristics survival data are median number of months ( 95% ci ) in all patients . 
positions of squares show hazard ratio of death in the crt plus cetuximab group compared with death in the crt only group ; the area of each square represents the amount of information ( ie , the number of patients ) in each category . 
full quality - of - life data will be reported elsewhere . discussion as the result of a preplanned assessment , the independent data monitoring committee reported that the primary endpoint of the phase 2 stage of the scope1 trial had not been met and recommended closing the vol 14 june 2013 articles crt plus cetuximab crt only the outcome of scope1 is consistent with recent results from other randomised trials comparing the addition of anti - egfr therapy to standard treatment across several tumour sites ( panel )  . 
patients who received the monoclonal antibody received a lower protocol dose of capecitabine and oxaliplat despite this prespeci ed dose modication , patients in the chemotherapy plus panitumumab group received a lower median number of cycles than did the control group ( ve vs six ) , a lower median dose intensity of capecitabine , and had worse overall survival ( 88 months vs 113 months ; hr 137 ; p = 001 )  . 
the radiation therapy oncology group ( rtog ) 0522 trial24 sought to build on the results of bonner and colleagues study17 by adding cetuximab to cisplatin or uoropyrimidine - based chemoradiation in a similar patient population with squamous - cell head and neck cancer . 
 once again , no bene t was reported in terms of progression - free survival or overall survival , although an increased rate of mucositis was noted in the patients treated with cetuximab.24 in the coin trial , 25 which randomly assigned 2445 patients with metastatic colorectal cancer to oxaliplatin uoropyrimidine ( uorouracil or capecitabine ) chemotherapy with or without cetuximab , a higher than anticipated incidence of grade 3 or 4 diarrhoea ( 30% ) in the experimental group resulted in a dose modi cation of capecitabine during the course of the trial . 
in the scope1 trial , the real3 trial , 23 and for most patients in the coin trial , 25 a capecitabine backbone was used and the resultant reduction in doses of standard therapy might have contributed to the worse outcome in the cetuximab groups of these trials . 
as seen in the real3 study , 23 patients receiving cetuximab had a lower rate of haematological toxicity , possibly as a result of the lower chemotherapy dose intensity delivered . perhaps more importantlywith respect to this study of an investigational drug in de nitive treatment of oesophageal cancerwas the e ect on the dose of radiotherapy delivered . 
more than twice the number of patients in the crt plus cetuximab group than in the crt only group did not receive any radiotherapy ( 25 vs 10 )  . 
as systemic therapies move from palliative , through to adjuvant , to de nitive treatment protocols , evidencebased treatment regimens should be vigilantly protected , especially if such treatments are intensi ed . another explanation for these results , independent of dose intensity , is the possible occurrence of a negative interaction between cetuximab and chemoradiotherapy . 
 the proin ammatory and antitumour proliferative e ects of cetuximab have been proposed as the cause of number of patients crt plus cetuximab crt only weeks from randomisation figure 4 : physical functioning score from qlq - c30 in each treatment group at ve timepoints over 52 weeks the number of patients shows the amount who completed qlq - c30 at each timepoint . 
qlq - c30 = european organisation for research and treatment of cancers quality of life questionnaire c30 . crt plus cetuximab crt only number of patients crt plus cetuximab crt only weeks from randomisation figure 5 : eating restrictions score from qlq - oes18 in each treatment group at ve timepoints over 52 weeks the number of patients shows the amount who completed qlq - oes18 at each timepoint . 
the addition of cetuximab to chemoradiotherapy resulted in more toxicity , less protocol treatment being delivered , and worse overall survival than with chemoradiotherapy alone , although quality of life was not reduced compared with chemoradiotherapy alone . 
therefore , the addition of cetuximab to standard de nitive chemoradiotherapy cannot be recommended . 634 vol 14 june 2013 articles reduced e cacy in combination with chemoradiation in rectal cancer.27 a similar interaction between oxaliplatin and cetuximab has been proposed , speci cally that cetuximab might protect against free - radical damage by platinum drugs , 28 and again could explain the negative outcome in this and other studies.25 , 29 despite this reduction in survival , however , and increased toxicity , we did not record an e ect on quality of life according to standard eortc generic and disease - speci c measures . the egfr pathway seems to be important in the carcinogenesis of oesophagogastric malignancy30 and a bene t of anti - egfr therapy has been shown in head and neck cancer in combination with radiotherapy17 and in advanced disease.15 the negative outcome in this study therefore seems to be a result of tumour - speci c interactions and biology that are not fully understood , or overlapping toxicities that preclude the delivery of e ective standard treatment . an understanding of why the overall survival in this trial was better than anticipated will be important ; 2 - year overall survival was predicted to be 35% in the crt only group in the phase 3 design . 
despite the fact that most patients had stage iii disease , 38% of patients were older than 70 years , and 15% of patients had comorbidities that precluded surgery , the 2 - year overall survival in all patients was 49% , and was 56% in those receiving crt only . 
indeed , the overall survival in the crt only group exceeded that which was hoped to be seen by the addition of cetuximab and was better than that seen in the us and uk studies exploring the role of the addition of neoadjuvant chemotherapy to surgery.3 although one of the lead authors in our investigation ( tc ) has previously published encouraging out comes of single centre , retrospective series , 8 , 12 whether these outcomes could be reproduced in a multicentre , prospective study was unclear . 
before this trial , concerns had been raised about the quality of radiotherapy delivered in multicentre uk studies of radiotherapy in upper gastrointestinal cancers.31 such studies did not have detailed radiotherapy treatment protocols and had near - absent radiotherapy quality assurance . 
 we developed a detailed protocol mandating the use of endoscopic ultrasound and intravenous contrast to aid localisation of target volume and used a single - phase conformal treatment plan.33 this plan , together with a comprehensive radiotherapy planning protocol and test cases , was sent to all principal investigators and radiotherapy centres before patients were recruited.19 we propose that this protocol , together with the on - trial quality assurance programme providing a positive dialogue between recruiting units and the rttqa central team , was a crucial component to the successful outcomes seen in the crt only group . 
the bene t of rttqa has been reported in other studies.34 to the best of our know ledge , this trial is the largest prospective panel : research in context systematic review we identi ed a systematic review22 on combined modality radiotherapy and chemotherapy in non - surgical management of localised carcinoma of the oesophagus that searched medline ( 19962001 ) , cancerlit ( 19832001 ) , cochrane library databases ( 2001 ) , and abstracts published in the american society of clinical oncology and the american society for therapeutic radiology and oncology ( 19992001 ) for articles published in any language . 
the review reported the bene ts of chemoradiotherapy ( crt ) compared with radiotherapy alone ; however , it also showed that most patients still relapse with locoregional or metastatic disease . 
we also identi ed studies that reported that cetuximab , a monoclonal egfr antagonist , improved outcomes when given in combination with : chemotherapy in advanced colorectal adenocarcinomas and squamous - cell head and neck cancer ; and radiotherapy in squamous - cell head and neck cancer . 
the results of our study do , however , support the use of chemoradiation alone as a standard of care in patients with non - metastatic squamous - cell carcinoma of the oesophagus and in patients with non - metastatic adenocarcinoma who are not suitable for surgery . 
indeed , the outcomes of this study would support the increased use of this treatment in patients who have a higher risk of failure of surgical treatment , either due to the existence of comorbidities or where surgical excision is likely to be incomplete . 
a randomised trial to compare surgical and radiotherapy - based treatments in patients with oesophageal cancer with a better outlook is warranted . study with a comprehensive assessment of quality of life with disease and cancer - speci c questionnaires patients under going de nitive chemoradiotherapy . 
 scores achieved in patients surviving for 2 years in our study are compatible with that achieved by surgical - based treatments.5 other factors that could have contributed to improved outcomes in this study are patient selection and organisation of cancer services throughout the uk . 
pet has been shown to both exclude patients with metastatic disease not otherwise seen with endoscopic ultrasound and ct scan35 and be useful in radiotherapy planning.36 substantial reconguration of oesophagogastric cancer treatment ser vices in the uk has also taken place in the past decade.37 , 38 although the changes have mainly been in centralisation of surgical services , they have led to the development of regional specialist multidisciplinary teams , which has vol 14 june 2013 articles undoubtedly added rigour to treatment decisions and patient selection . 
the 2012 annual report of the uk national oesophago - gastric cancer audit38 has showed an improvement in outcomes for patients undergoing surgery , with 45% of patients surviving for 3 years . 
both of these areas have scope for further development , namely the incorporation of ct - pet more directly into radiotherapy planning and assessment of caseload , with outcomes in specialist non - surgical services . how can we build further on the encouraging clinical outcomes reported in the crt only group of this study ? clearly , as patients continue to relapse with both metastatic and locoregional disease , systemic and local components of this treatment strategy need to be improved and intensi ed . 
the overexpression of her2 ( also known as erbb2 ) predicts whether the addition of trastuzumab will bene t patients with advanced oesophagogastric cancer.40 the safety and e cacy of anti - her2 therapy should be tested as part of chemoradiotherapy treatment in this patient population . a radiotherapy doseresponse e ect in patients with oesophageal cancer has been known for some time.41 however , a study designed to test the bene t of a higher radiation dose given concurrently with cisplatin and uoropyrimidine chemotherapy was prematurely stopped for futility as a result of an excess of treatmentrelated deaths occurring in the high - dose treatment group.9 we believe , however , that by using newer radiotherapy techniques , such as intensity - modulated and imageguided radiotherapy , we can now safely deliver a higher dose of radiation to a highly conformal target volume within the context of a high - quality rttqa programme . this trial was a phase 2 / 3 study that ended on completion of phase 2 . 
additionally , although the study strati ed patients according to tumour histology , it was not powered to assess with certainty the bene t of cetuximab in each of the two main histological variants of this disease . this trial has not shown that the addition of cetuximab to standard de nitive chemoradiotherapy bene ts patients with locally advanced oesophageal cancer . 
in fact , the addition of cetuximab increased toxicity , reduced delivery of all components of standard chemoradiotherapy , and was associated with a signi cant reduction in overall survival . 
however , the very encouraging outcomes seen with de nitive chemoradiotherapy alone should provide an excellent platform to test more targeted therapeutic approaches , incorporating biomarker - driven systemic therapies and newer radiotherapy technologies to safely intensify treatment , including increases to radiotherapy doses . contributors tc , cnh , sf , sg , js , jab , jig , jb , tm , and gg were involved in the design and development of the trial and the writing and review of the protocol . 
all authors have contributed to , seen , and approved the nal dratc , sf , sg , rro , jig , and dc were principal investigators at centres recruiting more than 5% of patients . 
a full list of all scope1 study investigators is listed in the appendix . con icts of interest we declare that we have no con icts of interest . acknowledgments the scope1 trial was sponsored by velindre nhs trust , funded by cancer research uk ( cruk ) , and cruk core funding at the wales cancer trials unit ( wctu )  . 
the radiotherapy trials quality assurance ( rttqa ) was funded by cruk and the cardi national cancer research institute rttqa centre at velindre nhs trust which are funded by the national institute of social care and health research ( nischr ; wales ) and department of health ( england )  . 
we thank all the patients who participated in the trial , the doctors , nurses , pathologists , other members of the multidisciplinary teams , radiotherapy team , and research team from the participating centres . 
we also thank lisette nixon ( wctu trial manager ) , bethan tranter ( trial pharmacist ) , david kirby ( patient representative ) , wendy wade ( research nurse ) , and ashley roberts ( radiologist ) for their input into the trial management group . editorial uk pharmaceutical industry under threat on may 2 , 2014 , p zerthe worlds largest pharmaceutical companymade a second attempt to purchase the rival rm astrazeneca . 
these events happened soon after an asset swap between glaxosmithkline ( gsk ) and novartis , in which novartis sold its vaccines division to gsk , who in turn sold its oncology portfolio to novartis ; the two companies are also to merge their consumer health divisions . 
the sale of gsks oncology portfolio in particular is surprising , because the company stated on record last year that they wanted to become one of the top ve players in oncology . 
 inevitably , concerns have been raised in the uk , where astrazenecas headquarters are based , that the potential merger with p zer will cost the country jobs and vital income . 
p zer has a bad reputation in this area ; for instance , it sold its uk research facilities in sandwich , kent , in 2011 , in the process making 1500 highly skilled people redundant . 
clearly aware of these negative perceptions , p zers chief executive has written to the uks prime minister , david cameron , to promise to complete work on astrazenecas research and development ( r&d ) hub in cambridge , and to pledge to employ at least 20% of the combined companys r&d workforce in the uk and locate some of the companys manufacturing plants in brita however , these guarantees are only for 5 years and do not go far enough . 
 additional concerns are that pharmaceutical mergers will not only negatively a ect the economy , but that they could also sti e innovation and the development of new drugs , further threatening the hard - won reputation of the uk as a world leader in medical r&d . 
indeed , a f ormer head of research at p zer recently informed the independent that he fears drug discovery programmes in their early stages are likely to be disrupted or abandoned , and highlighted astrazenecas oncology portfolio as being particularly vulnerable . 
innovation could also be sti ed in the gsknovartis deal , which means gsk has an e ective monopoly on vaccine development , and the subsequent loss of competition could deter further innovation . 
the mergers could also increase the onus on academia and small biotechnology companies to do more early - stage discovery and r&d work , bringing with it increased nancial pressures . it is therefore vital that the uk government does all it can to encourage companies to retain their drug discovery divisions within the uk . 
the introduction of the patent box in 2013 , which allows companies to apply for lower corporation tax on earnings from patented inventions , should encourage innovative companies to remain in the uk . 
as a last resort , the government could consider a golden share option ( akin to past deals with rolls royce and bae systems ) to prevent a foreign takeover , or using its public interest test powers , which can block takeovers if they could damage national interestuk business secretary vince cable has said he would not rule out this latter option , and states that the government sees the uk as a knowledge economy , not a tax haven . 
an announcement in april this year from the uks exam regulator , ofqual , that stated practical work would cease to contribute to the overall grade of a levelsthe quali cations that determine university entrance in the ukis a major retrograde step and disconnected from the realities of science . 
 although mergers and acquisitions are an everyday part of business for companies that compete in a global market , sometimes national interests need to be put ahead of markets and pro t , and every e ort must be made to ensure that researchers and innovators are not hampered in the pursuit of better outcomes for patients . 
 the lancet oncology vol 15 june 2014 editorial pancreatic cancer in the spotlight in february , 2014 , an advertising campaign launched in the uk by the charity pancreatic cancer action generated a storm of criticism , depicting patients with pancreatic cancer stating that they wished they had other forms of the disease , speci cally testicular and breast cancer . 
although few would argue against raising awareness of an invariably fatal disease , the comparison with other cancersand especially the idea that having one cancer is better than having another prompted objections from several sources , including charities breakthrough breast cancer and breast cancer care . 
 furthermore , other charities ( such as macmillian cancer support ) have backed the campaign , which now continues with a focus on the types of symptoms associated with the disease . while is understandable why the campaign provoked a reaction , it must be acknowledged that , although charities are not - for - pro t organisations , there is heavy competition for limited resources within the philanthropic sector . 
with less money to go around , individuals and corporations are more selective about where they give , and with so many causes seeking attention , donation fatigue is a serious concern . 
in the uk , for example , there are at least three charities that focus on pancreatic cancer , which begs the question as to whether a collaborative or combined approach would be greater than the sum of all parts . 
funding for pancreatic cancer research is very low compared with other cancer types , and as a result , there are currently 81 clinical trials for breast cancer recruiting in the uk , but only eight for pancreatic cancer . 
unlike breast cancer , which lends itself to self - diagnosis and for which there are well established screening programmes in place , pancreatic cancer presents with di use symptoms and often at a late stage . 
more research is therefore desperately needed to understand the basic biology of the disease and to develop appropriate screening programmes . more than 330 000 people are diagnosed with pancreatic cancer annually worldwide , and prognosis remains poorjust under 4% are expected to survive for 5 years after their diagnosis . 
in doing so , patients with rarer or di cultto - treat cancers would no longer be forgotten and governments in turn might make more e ective use of limited research budgets . 
we assessed whether dose intensi cation of doxorubicin with ifosfamide improves survival of patients with advanced soft - tissue sarcoma compared with doxorubicin alone . methods we did this phase 3 randomised controlled trial ( eortc 62012 ) at 38 hospitals in ten countries . 
we included patients with locally advanced , unresectable , or metastatic high - grade soft - tissue sarcoma , age 1860 years with a who performance status of 0 or 1 . 
they were randomly assigned ( 1 : 1 ) by the minimisation method to either doxorubicin ( 75 mg / m by intravenous bolus on day 1 or 72 h continuous intravenous infusion ) or intensi ed doxorubicin ( 75 mg / m ; 25 mg / m per day , days 13 ) plus ifosfamide ( 10 g / m over 4 days with mesna and peg lgrastim ) as rst - line treatment . 
randomisation was strati ed by centre , performance status ( 0 vs 1 ) , age ( < 50 vs 50 years ) , presence of liver metastases , and histopathological grade ( 2 vs 3 )  . 
there was no signi cant di erence in overall survival between groups ( median overall survival 128 months [ 955% ci 105143 ] in the doxorubicin group vs 143 months [ 125165 ] in the doxorubicin and ifosfamide group ; hazard ratio [ hr ] 083 [ 955% ci 067103 ] ; strati ed logrank test p = 0076 )  . 
median progression - free survival was signi cantly higher for the doxorubicin and ifosfamide group ( 74 months [ 95% ci 6683 ] ) than for the doxorubicin group ( 46 months [ 2956 ] ; hr 074 [ 95% ci 060090 ] , strati ed log - rank test p = 0003 )  . 
more patients in the doxorubicin and ifosfamide group than in the doxorubicin group had an overall response ( 60 [ 26% ] of 227 patients vs 31 [ 14% ] of 228 ; p < 00006 )  . 
for a few sarcomasnotably , targeted gastrointestinal stromal treatment is available.1 however , although translocations or ampli cations have been associated with an increasing number of sarcoma subtypes , these ndings have led to innovative treatment for only a minority of cases.24 for most advanced sarcomas , clinicians rely on conventional tumourse ective chemotherapy for palliation , which is somewhat e ective , few patients achieve an objective response.5 but histological diagnosis can be used to guide treatment for some sarcomaseg , taxanes for angiosarcoma , 6 , 7 or gemcitabine - containing treatment for leiomyosarcoma and un di erentiated pleomorphic sarcoma.8 , 9 nevertheless , doxorubicin and ifosfamidewhich have been used to treat soft - tissue sarcoma for more than 30 yearsstill have an important role . 
 ifosfamide has a clear doseresponse relationship , with 9 g / m fractionated over 3 days producing a higher proportion of responses than 5 g / m given as a 24 h infusion.10 responses in as many as 5060% of patients have been reported for various regimens of anthracycline plus ifosfamide1113 but these ndings have not been replicated in randomised trials . 
in the palliative setting , disease control can delay deterioration of symptoms , therefore progression - free survival might be equally important as overall survival , although improved overall survival is still a key goal of treatment.14 we assessed whether the addition of ifosfamide to doxorubicin improved the survival of patients with locally advanced unresectable or metastatic soft - tissue sarcoma . 
 to establish the true value of the combination , we used a dose of ifosfamide used in previous phase 2 trials to enable direct comparison and the doxorubicin dose was identical in the two groups both to maximise dose intensi cation and to test the e ect of adding ifosfamide . methods study design and participants we did this phase 3 , randomised controlled trial ( eortc 62012 ) at 38 hospitals in ten countries ( belgium , canada , denmark , france , germany , netherlands , slovakia , spain , switzerland , uk ; appendix )  . 
patients had to be age 1860 years , with a who performance status17 of 0 or 1 , absolute neutrophil count more than 2 10 cells per l , more than 100 10 platelets per l , serum creatinine of 120 mol / l or less or calculated creatinine clearance ( cockroft and gault method ) more than 65 ml / min , two functioning kidneys , bilirubin 30 mol / l or less , and albumin more than 25 g / l . 
patients also had to have a normal ( according to local assessments ) left ventricular ejection fraction by multiple gated acquisition scan or echocardiogra liposarcoma , pleomorphic synovial women of child - bearing potential had to take adequate contraceptive measures and have a negative pregnancy test within 7 days of study entry . 
we excluded patients with : gastrointestinal stromal tumour , mixed mesodermal tumour , chondrosarcoma , malignant mesothelioma , neuroblastoma , osteosarcoma , ewings sarcoma , desmoplastic small round cell tumour , embryonal rhabdomyosarcoma , and alveolar soft part sarcoma . 
additional exclusion criteria were other severe illness ( eg , psychosis or previous history of cardiovascular disease ) , symptomatic or known cns metastases , previous or concurrent second primary malignant tumours ( except adequately treated insitu carcinoma of cervix or basal cell carcinoma )  . 
we also excluded patients who had had radiotherapy to the sole available lesion or those who had received chemotherapy for advanced disease , although previous adjuvant chemotherapy ( preoperative or postoperative ) was allowed if disease progression had not occurred within 6 months of completion . index the study protocol is available online . 
randomisation was strati ed by centre , performance status ( 0 vs 1 ) , age ( < 50 years vs 50 years ) , liver metastases ( present vs absent ) , and histological grade ( 2 vs 3 )  . 
neither patients nor investigators were masked to treatment allocation . procedures patients assigned to receive doxorubicin alone were given doxorubicin 75 mg / m by intravenous bolus on day 1 or 72 h continuous intravenous infusion . 
those assigned to receive intensi ed doxorubicin and ifosfamide received doxorubicin 25 mg / m per day on days 13 and ifosfamide ( 25 g / m per day , days 14 ) plus mesna ( 05 g / m by intravenous bolus before ifosfamide , 15 g / m concurrent with ifosfamide , and 1 g / m orally 2 h and 6 h after completion of ifosfamide infusion ) , followed by peg lgrastim ( 6 mg subcutaneously , day 5 ; appendix )  . 
clinical assessments of safety , including physical examination , performance status , blood chemistry , and urinalysis ( with dipstick ) were done at baseline and before each cycle of treatment . 
doxorubicin causes cumulative cardiotoxicity and ifosfamide can cause cumulative renal impairment , bladder toxic e ects , and central encephalopathy . disease was assessed after every two cycles of treatment with chest radiography and either ct or mri scans . 
for patients with complete response , partial response , or stable disease at the end of treatment ( assessed with recist 1.0 ) , assessments were continued every 6 weeks . 
for stable disease , a minimum of 6 weeks was speci ed . statistical analysis the trial was powered to detect a hazard ratio ( hr ) of 0737 at most . 
the choice of 50% as comparator was based on an analysis of more than 2000 patients with sarcoma treated with rst - line anthracycline - containing chemotherapy , survival was for whom median 12 months.19 366 events were needed to detect such a di erence with a two - sided strati ed log - rank test ( = 005 , power = 80% )  . 
we did two interim analyses : one futility analysis after 52 events ( progression or death ) to assess if progression - free survival at 6 months was signi cantly greater in the doxorubicin and the doxorubicin group ( target hr 05 , = 005 ) and one based on overall survival after 188 deaths ( using an error spending function with a boundary parameter of 02 )  . 
 we used a stopping rule for toxic e ects , with ongoing analyses once every 6 months , such that if febrile neutropenia occurred in more than 30% of cycles of treatment with doxorubicin and ifosfamide , the study would be stopped . ifosfamide group than overall survival was computed from the date of randomisation to the date of death from any cause . 
patients alive and progression - free at the time of analysis were censored at the date of last follow - up . we estimated overall survival and progression - free survival with the kaplan - meier method and compared treatment groups with a two - sided log - rank test . 
we used a signi cance level of 00451 ( adjusted for interim analysis , associated cis are 955% ) for the analysis of overall survival , whereas we used 005 for the other endpoints . we did the primary e cacy analyses for the intentionto - treat populationie , all randomly assigned patients ( including those retrospectively found to be ineligible ) according to their allocated treatment . 
we did sensitivity e cacy analyses for the per - protocol populationie , all randomly assigned patients who satis ed the eligibility criteria and started their allocated treatment . 455 patients randomly assigned 228 assigned to doxorubicin only 227 assigned to doxorubicin and ifosfamide 8 ineligible according to study coordinator ( ij ) review * 7 ineligible according to study coordinator ( ij ) review 3 refused treatment 3 did not start treatment 1 refused 1 performance status worsened 1 clinical progressive disease 2 started treatment , but did not follow the allocated approach 1 by mistake 1 reason unknown before rst cycle 217 eligible and started allocated treatment 215 eligible and started allocated treatment 94 relapsed or died because of 45 relapsed or died because of 117 discontinued progressive disease 5 had toxic eects 4 refused 4 intercurrent deaths 10 for other reasons progressive disease 103 discontinued 36 had toxic eects 10 refused 1 intercurrent death 11 for other reasons 228 included in intention - to - treat ecacy analyses 223 included in safety analyses 217 included in per - protocol analyses 227 included in intention - to - treat ecacy analyses 224 included in safety analyses 215 included in per - protocol analyses figure 1 : trial pro le * one of whom started treatment but did not follow the allocated approach . vol 15 april 2014 articles the clinical cuto date was july 5 , 2012 . 
the corresponding author had the nal responsibility for the decision to submit for publication . results we enrolled 455 patients between april 30 , 2003 , and may 25 , 2010 . 
although information about degree of di erentiation and necrosis was available , missing data for mitotic count for ten patients precluded accurate distinction between intermediate and high grade ; thus , they were strati ed as high grade for randomisation . 
15 patients were deemed ineligible by the study coordinator ( ij ; gure 1 ) , reasons were : inappropriate histological results on central review ( n = 9 ) , treatment started before randomisation ( n = 1 ) , previous treatment ( n = 1 ) , too old ( n = 2 ) , impaired renal function ( n = 1 ) , only one kidney because of previous kidney cancer ( n = 1 ) , and poor performance status ( n = 2 )  . 
as a result , the safety population consisted of 447 patients and the per - protocol population of 432 patients ( gure 1 )  . median follow - up was 56 months ( iqr 3177 ) for the doxorubicin group versus 59 months ( iqr 3672 ) for the doxorubicin and ifosfamide group . 
most patients died as a result of progressive disease ( table 2 ) ; 30 patients ( 13 vs 17 ) were still alive and progression - free at the cuto date . there was no signi cant di erence between groups in terms of overall survival ( gure 2a )  . 
median overall survival was 128 months ( 955% ci 105143 ) in the doxorubicin group versus 143 months ( 125165 ) in the doxorubicin and ifosfamide group ( hr 083 , 955% ci 067103 ; strati ed log - rank test p = 0076 )  . 
 overall survival at 1 year was 51% ( 955% ci 4458 ) in the doxorubicin alone group versus 60% ( 5366 ) in the doxorubicin and ifosfamide group , whereas at 2 years it was 28% ( 2234 ) and 31% ( 2538 ) , respectively . 
no signi cant di erence was noted between the groups in the per - protocol analysis ( p = 0057 )  . the doxorubicin and median progression - free survival was signi cantly higher ifosfamide group ( 74 months , 95% ci 6683 ) than in the doxorubicin group ( 46 months , 95% ci 2956 ; hr 074 , 955% ci 060090 , strati ed log - rank test p = 0003 ; gure 2b )  . 
figure 3 also shows a bene t of combination treatment for patients aged 4049 years , which might have been a result of statistical imbalances for this age groupboth for performance status and the tumour gradewhich combination treatment group ( data not shown )  . 
best overall response to treatment di ered signi cantly between the two groups in favour of doxorubicin and ifosfamide ( 31 [ 14% ] of patients in the doxorubicin group and 60 [ 26% ] in the doxorubicin and ifosfamide group had an overall response ; test , p = 00006 )  . the occurrence of toxic e ects di ered between treatment groups . 
roughly half of all patients completed six cycles of treatment , 102 ( 45% ) of 228 patients with doxorubicin and 115 ( 51% ) of 227 with doxorubicin and ifosfamide . 
those taking doxorubicin and ifosfamide were more likely than those taking doxorubicin only to need a dose reduction ( 71 [ 32% ] of 224 patients vs 20 [ 9% ] of 223 had a reduction of doxorubicin ; 84 [ 38% ] of 224 had a reduction of ifosfamide )  . 
likewise , treatment interruptions were more common in patients taking the combination compared with the single drug treatment ( 15 [ 7% ] of 224 vs ve [ 2% ] of 223 needed interruption of doxorubicin , 17 [ 8% ] of 224 required interruption of ifosfamide )  . 
 however , treatment discontinuation because of disease progression occurred more often in those who received doxorubicin only than in those who received doxorubicin and ifosfamide ( table 4 )  . than grade 34 adverse events were signi cantly more prevalent in patients treated with doxorubicin and ifosfamide than in those treated with doxorubicin only ( table 5 , appendix lists all grades )  . 
 likewise , grade 2 and grade 3 vomiting was more common in the doxorubicin and ifosfamide group ( 53 [ 24% ] and 13 [ 5% ] , respectively ) compared with the doxorubicin group ( 32 [ 14% ] and six [ 3% ] , respectively )  . 
despite the toxic e ects associated with doxorubicin and ifosfamide , toxic deaths occurred in much the same proportion in each group ( table 2 )  . hr 083 , 955% ci 067103 ; p = 0076 228 227 170 197 113 130 number at risk doxorubicin doxorubicin and ifosfamide hr 074 , 955% ci 060090 ; p = 0003 time ( months ) number at risk doxorubicin doxorubicin and ifosfamide 228 227 104 149 figure 2 : kaplan - meier curves for overall survival ( a ) and progression - free survival ( b ) hr = hazard ratio . post - protocol treatment did not di er substantially between groups other than that patients treated with doxorubicin were more likely to receive subsequent ifosfamide than were those who received doxorubicin and ifosfamide ( table 6 )  . 
once patients progressed while taking study treatment , investigators were required to collect only survival data . discussion we found no improvement in overall survival from the administration of intensi ed combination chemotherapy ifosfamide compared with with doxorubicin plus doxorubicin alone . 
most data for high - dose combinations come from single - centre phase 2 studies of highly selected groups of patients.1214 few randomised studies have been done , mostly with a dose of dose of 5 g / m , none of which have shown a survival advantage ( panel )  . 
 doxorubicin , for example , a randomised trial20 done by the eortc soft tissue and bone sarcoma group compared doxorubicin alone with a combination of doxorubicin and ifosfamide 5 g / m or a four - drug regimen of cyclophosphamide , and vincristine , dacarbazine . 
the combination treatments did not signi cantly increase the proportion of patients who responsed , progression - free survival , or overall survival and were signi cantly more toxic than the single drug treatment.20 a phase 3 study comparing single - agent doxorubicin with a combination of doxorubicin with either ifosfamide 75 g / m , or mitomycin and cisplatin showed a greater proportion of responses with combination treatment but no di erence in survival.21 similarly , a comparing doxorubicin plus dacarbazine with or without ifosfamide , for treatment of soft - tissue sarcoma and bone sarcoma also showed a signi cantly greater proportion of responses and longer progression - free survival , but no survival advantage , for the ifosfamide - containing regimen than for the regimen without ifosfamide . trial22 other studies have investigated the role of dose intensi cation . 
for example , a randomised phase 2 trial of ifosfamide 6 g / m versus 12 g / m with doxorubicin showed no advantage for disease - free survival or overall survival for the higher dose.23 dose intensi cation of the 420 vol 15 april 2014 articles progression of disease or death caused by progressive disease 95 ( 42% ) toxic e ect ( including toxic death ) toxic death patients refusal ( not related to toxic e ects ) intercurrent death ( not related to malignant disease or toxic e ects ) other data are n ( % )  . table 4 : reasons for discontinuation of treatment doxorubicin group ( n = 228 ) doxorubicin and ifosfamide group ( n = 227 ) 6 ( 3% ) 5 ( 2% ) 4 ( 2% ) 4 ( 2% ) 12 ( 5% ) 47 ( 21% ) 40 ( 18% ) 2 ( 1% ) 10 ( 4% ) 1 ( < 1% ) 11 ( 5% ) doxorubicin , ifosfamide , and dacarbazine regimen originally developed in the late 1980sproduced no improvement in responses , progression - free survival , or overall survival compared with the standard dose regimen.24 a phase 3 trial of dose intensi cation of doxorubicin ( 75 mg / m vs 50 mg / m ) with ifosfamide 5 g / m showed no improvement in responses or overall survival , but did show a longer progression - free survival for patients taking the higher dose of doxorubicin.25 other studies of dose intensi cation showed no advantage compared with doxorubicin alone.26 , 27 two meta - analyses of dose - intensive chemotherapy and ifosfamide - based chemotherapy have combination provided the same conclusion.28 , 29 in this context , our study was uniquely powered for overall survival as the primary endpoint . 
however , we did note a signi cant 28 month improvement in median progression - free survival with the dose - intensi ed regimen , and a greater proportion of patients responded to the combination therapy than to doxorubicin alone . intravenous the study was not masked , which might have biased the assessment of response and disease progression . 
as in most previous studies , combination treatment was signi cantly more toxic than the single - drug regimen , but there was no excess of toxic deaths . the proportion of patients who had a response in both groups was lower than reported in somebut not all previous eortc studies , 10 , 11 and lower for the combination than that reported in single - centre studies.1214 eligible patients had to have high grade disease and progression within 6 weeks of study entry ; thus , the prognosis for participants was poor . 
however , the high proportion of patients with synovial sarcoma suggests that such a bias did not have a major role . how can these data be used to guide clinical practice ? if palliative chemotherapy is being given to control metastatictypically pulmonarydisease , rather than to relieve acute symptoms , then sequential single - drug chemotherapy will probably be less toxic without signi cantly impairing survival . 
conversely , if acute symptoms are best relieved by tumour shrinkage , the use of combination treatment would be justi ed ; likewise , if is being given before surgery or chemotherapy doxorubicin group ( n = 223 ) doxorubicin and ifosfamide group ( n = 224 ) 83 ( 37% ) 40 ( 18% ) 30 ( 13% ) 10 ( 4% ) 1 ( < 1% ) 93 ( 42% ) 97 ( 43% ) 103 ( 46% ) 78 ( 35% ) 75 ( 33% ) neutropenia leucopenia febrile neutropenia anaemia thrombocytopenia data are n ( % )  . 
clinical situations might also exist for which delaying disease progression for as long as possible is the priority ; for example , if adjacent critical structures such as nerves are involved . 
although some older patients can vol 15 april 2014 articles panel : research in context systematic review we searched pubmed for reports published in english from jan 1 , 1983 , to jan 1 , 2014 , for all randomised trials assessing dose intensi cation for treatment of soft - tissue sarcoma with the terms : randomis ( z ) ed , trial ( s ) , advanced , soft tissue , sarcoma ( s ) , ifosfamide , and doxorubicwe found eight randomised trials2027 and two metaanalyses.28 , 29 our search also returned single group and randomised phase 2 trials of higher dose treatment . 
combination treatment has been shown to improve the proportion of patients who responded and progression - free survival but not overall survival in some , but not all trials.22 , 25 , 26 interpretation in our study both doxorubicin and ifosfamide doses were higher than those used in previous randomised trials . 
if the goal of treatment is disease control , doxorubicin alone remains an appropriate treatment but combination treatment can be justi ed if tumour shrinkage is desired , either to relieve symptoms or before another intervention . 
the lack of improvement in overall survival shows the need for better treatments for advanced soft tissue sarcoma . tolerate intensive combination treatment , the regimen we used is very myelosuppressive , therefore our data cannot be extrapolated to patients older than 60 years . these data should also be considered in the context of the diversi cation of chemotherapy and other systemic treatment that is taking place in the management of softtissue sarcoma . 
pazopanib has recently been approved for the treatment of soft - tissue sarcoma on the basis of its e ect on progression - free survival.32 nevertheless , an urgent need still exists for treatment that improves survival in patients with advanced disease . contributors ij wrote the protocol , reviewed all the case record forms for eligibility and protocol violations , recruited patients , and wrote and edited the report with sl . 
all authors reviewed the nal version of the report . declaration of interests we have no competing interests . acknowledgments we thank anne kirkpatrick and the other sta at eortc headquarters who contributed to the success of the trial . 
we acknowledge nhs funding to the royal marsden / icr national institute for health research biomedical research centre and researchers at the nihr university college london hospitals biomedical research centre . 
the eortc received nancial support from amgen for the cost of peg lgrastithe contribution of ncic clinical trials group was supported by the canadian cancer society research institute ( grant 021039 )  . corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
we investigated whether replacing mitomycin with cisplatin in chemoradiation improves response , and whether maintenance chemotherapy after chemoradiation improves survival . methods in this 22 factorial trial , we enrolled patients with histologically con rmed squamous - cell carcinoma of the anus without metastatic disease from 59 centres in the uk . 
patients were randomly assigned to one of four groups , to receive either mitomycin ( 12 mg / m on day 1 ) or cisplatin ( 60 mg / m on days 1 and 29 ) , with uorouracil ( 1000 mg / m per day on days 14 and 2932 ) and radiotherapy ( 504 gy in 28 daily fractions ) ; with or without two courses of maintenance chemotherapy ( uorouracil and cisplatin at weeks 11 and 14 )  . 
391 of 432 ( 905% ) patients in the mitomycin group versus 386 of 431 ( 896% ) in the cisplatin group had a complete response at 26 weeks ( di erence 09% , 95% ci 49 to 31 ; p = 064 )  . 
overall , toxic e ects were similar in each group ( 334 / 472 [ 71% ] for mitomycin vs 337 / 468 [ 72% ] for cisplatin )  . 
3 - year progression - free survival was 74% ( 95% ci 6977 ; maintenance ) versus 73% ( 95% ci 6877 ; no maintenance ; hazard ratio 095 , 95% ci 075121 ; p = 070 )  . 
chemoradiation became the standard of care for treatment of squamous - cell cancer of the anus after three phase 3 trials35 showed that radiotherapy with concurrent uorouracil and mitomycin resulted in better local control and recurrence - free or progression - free survival than did radiotherapy alone , or radiotherapy with uorouracil . 
the rationale for comparing 516 vol 14 may 2013 articles for the ucl clinical trials centre see patients , clinicians ( including those assessing patients ) , and investigators analysing data were not masked to treatment allocation . 
minimisation was used and strati ed according to primary site ( canal vs margin ) , t stage , n stage , age ( < 65 years vs 65 years ) , sex , and glomerular ltration rate ( < 60 ml / min vs 60 ml / min )  . 
 phase 1 delivered 306 gy in 17 daily fractions to the international commission of radiological units and measurements ( icru ) intersection point , as determined following the guidelines in icru report 50 , 13 using nonconformal rectangular parallel - opposed elds aiming to treat all pelvic nodes ( except the common iliac ) to a dose of 306 gy . 
phase 2 was conformally planned using ct images to deliver 198 gy to the icru intersection point in 11 daily fractions over 15 days ( weekends excluded ) treating the primary tumour and the whole anal canal with a 3 cm margin around all macroscopic tumours de ning the eld size ( for further details see protocol , available from the ucl clinical trials centre website )  . 
 the quality assurance of this trial will be reported elsewhere . patients received uorouracil 1000 mg / m per day on days 14 ( week 1 ) and 2932 ( week 5 ) by continuous 24 h intravenous infusion with radiotherapy , and either 12 mg / m of mitomycin as an intravenous bolus on day 1 only ( maximum single dose 20 mg ) or 60 mg / m of cisplatin by intravenous infusion on days 1 and 29 ( up to a maximum surface area of 20 m , therefore maximum single dose was 120 mg )  . 
maintenance chemotherapy 940 patients randomly assigned 246 assigned to cisplatin and no maintenance * 222 assigned to 246 assigned to 226 assigned to cisplatin and maintenance mitomycin and no maintenance * mitomycin and maintenance 246 in intention - to - treat analysis 222 in intention - to - treat analysis 246 in intention - to - treat analysis 226 in intention - to - treat analysis figure 1 : trial pro le four patients assigned to cisplatin received mitomycin : two treated o trial , one administrative error , one had an inadequate glomerular ltration rate ; two patients assigned to mitomycin received cisplatin during week 5 of chemoradiation : one treated o trial , one because of toxic e ects ( see appendix for details of compliance )  . 
 * 23 patients assigned to the cisplatin group and 23 assigned to the mitomycin group were not eligible for maintenance randomisation and were excluded from the analysis of progression - free survival for the maintenance endpoint . 
 cisplatin instead of mitomycin with uorouracil - based chemoradiation was based on seemingly higher complete response rates with cisplatin , 79 and acceptable acute toxic e ects in phase 2 trials . 
patients were eligible if they had histologically con rmed invasive squamous cell , basaloid or cloacogenic carcinoma of the anal canal and margin that was deemed t for investigated treatment ; a glomerular ltration rate of more than 50 ml / min ; acceptable blood test results ( haemoglobin > 100 g / l , > 1 10 platelets per l , > 3 10 white blood cells per l ) ; liver function tests within two times the normal range ; and adequate cardiac function . 
exclusion criteria were metastatic disease , other major malignancy likely to compromise life expectancy or completion of trial treatment , comorbidity including being hiv - positive and cardiac diseases , previous complete local excision , and previous radiotherapy to the pelvis . 
the study was approved by local research ethics committees , and all patients provided written informed consent . randomisation and masking patients were randomly assigned before starting initial treatment to one of four treatment groups . 
patients were assessed for tumour response by digital examination using the response evaluation criteria in solid tumors ( recist ) 15 at 11 , 18 , and 26 weeks from the start of treatment . 
routine biopsies were not recommended because of the risk of radionecrosis but the 26 - week assessment included imaging ( abdominopelvic ct and radiography and whole body ct ) as at baseline . 
haematological toxic e ects were assessed at week 11 for all patients , and for those receiving maintenance treatment , haematological toxic e ects were checked before the rst and second cycles of maintenance treatment and non - haematological toxic e ects were checked weekly until 30 days after the last dose of study drug . 
 after the assessment at week 26 , patients were reassessed once every 2 months in the rst year , once every 3 months in the second year , once every 6 months until the fth year , and yearly thereafter . 
abdominopelvic ct was done at 12 and 24 months after the start of treatment and afterwards only when clinically indicated or if the patient had signs or symptoms of recurrence . for the comparison of mitomycin with cisplatin the primary endpoints were complete response ( complete disappearance of clinically or radiologically overt disease ) at 26 weeks from start of chemoradiation , and grade 3 or 4 acute toxic e ects for 4 weeks after chemoradiation ( haematological , gastrointestinal , and genitourinary )  . 
for the comparison of maintenance with no maintenance treatment the primary endpoint was progression - free survival . secondary endpoints included colostomy - free survival ( including pretreatment colostomies not reversed within 8 months after starting treatment , or any colostomies after treatment ) ; ineld recurrence rate ; cause - speci c survival ; and overall survival ( death from any cause )  . 
we also analysed progression - free survival by treatment during chemoradiation ; by disease stage ( t1 or t2 and t3 or t4 ) ; and by node status ( node positive and node negative disease )  . statistical analysis we calculated a target sample size of 950 patients based on detecting an improvement in 3 - year progression - free survival from 750% to 825% ( for the maintenance comparison )  . 
this sample size would enable us to detect an increase in the number of patients with complete response from 90% to 95% for cisplatin versus mitomycboth comparisons had 80% power and twosided 5% statistical signi cance . 
the sample size was increased in march , 2007 , from 600 to 950 patients , on the recommendation of the independent data monitoring committee because fewer progression - free survival events occurred than expected . events included in progression - free survival were progressive disease , local recurrence ( with or without metastatic disease ) , metastases , or death from any cause , but new tumours were not included . 
colostomy - free survival events were all post - treatment colostomies , hr 095 ( 95% ci 075121 ; p = 070 ) number at risk no maintenance maintenance mitomycin , no maintenance cisplatin , no maintenance mitomycin , maintenance cisplatin , maintenance time since randomisation ( years ) number at risk mitomycin , no maintenance cisplatin , no maintenance mitomycin , maintenance cisplatin , maintenance figure 2 : progression - free survival comparing the maintenance versus no maintenance groups ( a ) , and all four groups ( b )  . 
the four curves in b overlap , providing no evidence for an interaction between chemoradiotherapy regimen and maintenance ( p = 094 )  . vol 14 may 2013 articles see online for appendix pretreatment colostomies not reversed within 8 months from the start of treatment , and death from any cause . 
 all survival endpoints were measured from the date of randomisation , and patients who did not have the event of interest were censored at the date of last follow - up . 
 role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
of the 46 patients assigned to mitomycin or cisplatin , but not randomly assigned to a maintenance group , ten died : seven from anal cancer , one related to surgery , one from another cancer , and one not related to cancer . 
one case of neutropenic sepsis in the mitomycin , no maintenance group ; one acute myocardial infarction in the cisplatin , no maintenance group ; one case of pancolitis in the mitomycin , maintenance group ; and one bowel perforation in the cisplatin , maintenance group . 
these patients were excluded from the analysis of progression - free survival for the maintenance endpoint . total compliance to radiotherapy was good with few patients failing to complete the planned dose of 504 gy in either group ( 37 of 472 [ 8% ] in the mitomycin group and 44 of 468 [ 9% ] in the cisplatin group )  . 
370 of 472 patients ( 78% ) in the mitomycin group versus 352 of 468 ( 75% ) in the cisplatin group completed radiotherapy as planned ( ie , with no treatment gap or dose reduction ; appendix )  . 
 only 18 patientsnine in the mitomycin group and nine cisplatin grouphad interruptions to treatment for 8 days or more . 862 of 940 ( 92% ) patients received the full rst course of uorouracil with mitomycin or cisplatin without delays or dose reductions ( 433 of 472 in the mitomycin group , 429 of 468 in the cisplatin group , appendix )  . 
703 of 940 patients ( 75% ) completed the entire chemotherapy regimen during chemoradiation without delays or dose reductions ( 365 of 472 in the mitomycin group , 338 of 468 in the cisplatin group )  . 
of the 237 who did not , 222 ( 94% ) had either dose delays , reductions , or both in line with protocol recommendations or to prevent toxic e ects . 
only two ( < 1% ) were not given any chemotherapy during chemoradiation ( one died and did not have radiotherapy , and one withdrew from the study , both in the cisplatin group ; not excluded from the intention - totreat analysis ) ; and data were missing for six patients in the cisplatin group and seven in the mitomycin group . 
 the main reasons for non - completion were toxic e ects ( 66 patients in the mitomycin group and 78 in the cisplatin group )  . 357 of 448 to receive maintenance chemotherapy started treatment . 
286 ( 64% ) completed the rst course of treatment according to schedule , and 196 ( 44% ) completed both courses without any delay or dose reduction ( 105 of 226 [ 46% ] in the mitomycin group and 91 of 222 [ 41% ] assigned to cisplatin ; appendix )  . 
119 patients had dose modi cation because of maintenance did not receive it , 41 of the 91 ( 45% ) choosing not to receive any maintenance chemotherapy ( appendix )  . 
386 ( 896% ) in the cisplatin group and 391 ( 905% ) in the mitomycin group had a complete response at 26 weeks ; absolute di erence 09% ( 95 ci 49 to 31 ; p = 064 ; table 2 )  . 
 we assessed progression - free survival in 223 patients in the cisplatin , no maintenance group ; 222 in the cisplatin , maintenance group ; 223 in the mitomycin , no maintenance group ; and 226 in the mitomycin , maintenance group . 
3 - year progression - free survival was 74% ( 95% ci 6977 ) in the maintenance group and 73% ( 6877 ) in the no maintenance group ( hr 095 , 95% ci 075121 ; p = 070 ; gure 2 )  . 
 progression - free survival did not di er signi cantly between patients who took mitomycin and cisplatin during chemoradiation ( hr 095 , 95% ci 075119 ; p = 063 ; appendix )  . 
3 - year progression - free survival of patients without maintenance treatment was 73% ( 95% ci 6778 ) in the mitomycin group versus 72% ( 6678 ) in the cisplatin group ; for those who were given maintenance treatment , it was 73% ( 6678 ) versus 74% ( 6880 )  . 
 3 - year progression - free survival of patients with stage t1 or t2 disease was 80% ( 95% ci 7484 ) for patients taking maintenance treatment , 84% ( 7888 ) for those not taking maintenance treatment , 80% ( 7484 ) for those taking mitomycin , and 83% ( 7887 ) for those taking cisplat the respective progression - free survivals for t3 or t4 disease were 67% ( 6073 ) , 62% ( 5568 ) , 65% ( 5971 ) , and 62% ( 5569 )  . 
overall progression - free survival was 68% ( 6273 ) for node - positive patients and 76% ( 7279 ) for node - negative patients ; with similar rates for the treatment groups ( 67% [ 5974 ] with mitomycin vs 69% [ 6176 ] with cisplatin for nodepositive disease ; 76% [ 7080 ] vs 76% [ 7181 ] for nodenegative disease )  . 
the overlapping curves in gure 2b suggest no interaction between the two treatment strategies ( p = 094 )  . 211 patients died , 155 from anal cancer ( including treatment - related deaths ; table 3 )  . 
the hr for cisplatin versus mitomycin was 105 ( 95% ci 080138 ; p = 070 ) ; and for maintenance versus no maintenance the hr was 107 ( 081141 ; p = 065 )  . 
 3 - year anal cancer survival rates were also much the same for each treatment group ( appendix )  . 118 of 884 ( 13% ) assessable patients had colostomies at randomisation ( appendix )  . 
3 - year colostomy - free survival was 73% ( 95% ci 6779 ) in the mitomycin , main tenance group , 75% ( 6880 ) in the cisplatin , maintenance group , 75% ( 6880 ) in the mitomycin , no maintenance group , and 72% ( 6677 ) in the cisplatin , no maintenance group ( appendix )  . 
 table 5 : reported grade 34 adverse events during maintenance treatment with t1 or t2 disease and 61% ( 5666 ) for patients with t3 or t4 disease . toxic e ects during chemoradiation were as expected for this population and were much the same in the mitomycin and cisplatin treatment groups ( table 4 )  . 
the proportion of patients who had a maximum grade 12 adverse event was 133 of 472 ( 28% ) in the mitomycin group versus 126 of 468 ( 27% ) in the cisplatin group and the proportion of patients who had grade 34 adverse events was 334 of 472 ( 71% ) versus 337 of 468 ( 72% ; table 4 ) , although more patients had grade 3 haematological toxic e ects in the mitomycin group than in the cisplatin group ( 26% vs 16% ; p < 0001 )  . 
grade 3 or 4 toxic e ects were generally uncommon , and occurred in similar proportions in patients who had previously taken mitomycin ( 39 / 226 ; 17% ) and those who had previously taken cisplatin ( 39 / 222 ; 18% ; table 5 )  . 
treatment - related mortality was less than 1% ( n = 8 , four died during or up to 4 weeks after chemoradiation , three died 58 weeks after chemoradiation , and one died shortly after maintenance ; table 3 )  . 
subgroup analyses according to baseline characteristics did not show signi cant di erences in progression - free survival for any comparison ( appendix ) , or overall survival ( data not shown )  . discussion our results show no evidence of any improvement in the complete response rate or 3 - year progression - free survival , and similar acute grade 34 toxic e ects , when uorouracil plus cisplatin chemoradiation is compared with uorouracil plus mitomycin chemoradiation . 
our 22 randomisation enables us to examine complete response to chemoradiation with either concurrent mitomycin or cisplatin in a straightforward and simple manner , and also to test the bene t of adding further maintenance chemotherapy after initial chemoradiation to assess whether it enhances the chemoradiation response , or improves progression - free survival . 
preliminary results from our trial have already been used to guide practice.17 also , maintenance chemotherapy with uorouracil and cisplatinwhich had been used in some placescould now be stopped , and future patients can avoid unnecessary treatment ( as well as reducing nancial costs )  . 
 although grade 34 haematological toxic e ects were less common with uorouracil plus cisplatin ( 26% vs 16% ) patients , these were almost entirely related to white blood cells but were not su cient to increase neutropenic sepsis . 
this marginal bene t is likely to be outweighed by the extra resources needed to administer cisplatintwo courses of either all day or overnight intravenous treatment with hydration , compared with only a single dose of mitomycin delivered over 10 m cisplatin contraindicated ; however , this situation is rare . could be used when mitomycin survival maintenance chemotherapy using two cycles of uorouracil plus cisplatin did not improve progressionfree compared with no maintenance chemotherapy . 
exploratory subset analyses ( appendix ) show no evidence of any bene t for maintenance chemotherapy in any subgroups including patients with a high rate of relapse ( t3 or t4 and n + disease )  . 
these ndings accord with the rtog - 98 and accord - 03 trials , 10 , 11 , 16 which used neoadjuvant cisplatin - based chemotherapy before chemoradiation . our ndings are based on a 22 factorial trial design in which no evidence exists of an interaction between the chemoradiation and maintenance chemotherapy comparisons . 
fluorouracil and mitomycin chemoradiation should remain the standard of care for anal cancer because of similar e cacy and toxic e ects , fewer cycles of chemotherapy , fewer non - chemotherapy drugs , less time in the chemotherapy suite , less expense , and no risk of neuropathy compared with cisplatin , and the addition of maintenance chemotherapy in routine clinical practice is not justi ed . the high complete response rate ( 90% ) , similar 3 - year progression - free survival in the mitomycin and cisplatin groups , an overall 3 - year colostomy - free survival of 74% , and the very few ( 14 of 844 patients ) colostomies done for 522 vol 14 may 2013 articles ascribe late treatment e ects compares favourably with the results of other phase 3 trials.10 , 11 , 16 75% of patients had local control with organ preservation and avoided colostomy . these outcomes e cient radiobiological schedule . 
the two main achievements of our trial were the ability to maintain high compliance with 504 gy and the ability to give concurrent chemotherapy over a short overall treatment time by avoiding a planned gap in treatment.18 , 19 the median overall treatment time in the rtog 8704 trial was 49 days and in the rtog 9811 trial it was 42 days.5 , 11 , 20 a shorter overall treatment time is clinically important because a longer overall duration of radiation treatment adversely a ects local control in anal cancer.21 , 22 in the ecog e4292 phase 2 study using cisplatin - based chemoradiotherapy , 23 the clinical complete response rates were higher in patients who did not get a planned radiotherapy treatment break compared with those who did ( 12 / 13 vs 13 / 19 ; 92% vs 68% )  . 
possible strategies for improvement include the use of a non - cross - resistant induction chemotherapy ( eg , a taxane , 24 as used in head and neck cancer ) , the integration of biological agents ( eg , an egfr inhibitor25 ) , or dose - escalation above 504 gy enabled by intensity - modulated radiotherapy , which should be tested in appropriately designed clinical trials . intensiveness of our study has several limitations . 
we did not collect quality - of - life data ( patient - reported outcomes ) to investigate the pattern and severity of late radiotherapy - related toxic e ects . 
because of the the chemoradiation , maintenance treatment was di cult to deliver at full doses because of cumulative toxicity and low compliance , although most dose reductions were according to protocol . 
additionally , 41 maintenance patients chose not to start treatment and investigators might not have encouraged full complianceespecially at the start of the trialsince the e ectiveness of maintenance treatments is unproven . 
finally , panel : research in context systematic review we searched pubmed , medline , and cancerlit and abstracts of asco / astro / estro meetings with the terms anal cancer , squamous cell carcinoma , complete clinical response , local recurrence , survival , concurrent , chemotherapy , cisplatin , mitomycin c , radiotherapy , chemoradiation , radiochemotherapy , and combined modality . 
we found two other phase 3 trials in progress testing additional neoadjuvant cisplatin - based chemotherapy ( accord 03 and rtog 9811 ) , 10 , 11 , 16 but found no studies testing additional maintenance chemotherapy . interpretation in our trial , uorouracil and cisplatin had the same e ect on complete response rate , progression - free survival , and colostomy - free survival compared with uorouracil and mitomycnor did we see any improvement in progressionfree survival when additional maintenance chemotherapy was used . 
the low dose of elective nodal irradiation and a continuous radiotherapy schedule might have contributed to the good long - term outcomes . in conclusion , large phase 3 trials of primary anal cancer are feasible , even though this disease is uncommon ( we recruited roughly 25% of the uk incident cases )  . 
neither of the two strategies investigatedchemo radiation with cisplatin , and further maintenance chemotherapy using uorouracil and cisplatinis more e ective than standard care with mitomycin for achieving complete response , progression - free survival , or overall survival . 
 con icts of interest we declare that we have no con icts of interest . acknowledgments preliminary results of this trial were presented at the american society of clinical oncology meeting chicago in 2009 . 
the trial management group when the trial was designed were : roger d james ( chairman ) , david cunningham , rob glynne - jones , jonathan ledermann , helen m meadows , john northover , david sebag - monte ore , and maurice slevdc receives funding from biomedical research centre at royal marsden hospital ( uk ) and institute of cancer research ( uk )  . 
 we thank all those who participated in this trial , clinicians , their sta and patients , neil balderson and susan wan for study coordination , allan hackshaw and mark jitlal for comments on the report , and rubina begum for data management . 
we also thank the independent data vol 14 may 2013 articles monitoring committee ( richard gray , adrian crellin , and john shepherd ) and the independent trial steering committee ( peter hoskin , nicholas reed , and john tidy )  . corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 articles ge tinib for oesophageal cancer progressing after chemotherapy ( cog ) : a phase 3 , multicentre , double - blind , placebo - controlled randomised trial susan j dutton , david r ferry , jane m blazeby , haider abbas , asa dahle - smith , wasat mansoor , joyce thompson , mark harrison , anirban chatterjee , stephen falk , angel garcia - alonso , david w fyfe , richard a hubner , tina gamble , lynnda peachey , mina davoudianfar , sarah r pearson , patrick julier , janusz jankowski , rachel kerr , russell d petty summary background evidence is scarce for the e ectiveness of therapies for oesophageal cancer progressing after chemotherapy , and no randomised trials have been reported . 
we aimed to compare ge tinib with placebo in previously treated advanced oesophageal cancer . methods for this phase 3 , parallel , randomised , placebo - controlled trial , eligible patients were adults with advanced oesophageal cancer or type i / ii siewert junctional tumours , histologically con rmed squamous - cell carcinoma or adenocarcinoma , who had progressed after chemotherapy , with who performance status 02 , and with measurable or evaluable disease on ct scan . 
participants were recruited from 48 uk centres and randomly assigned ( 1 : 1 ) to ge tinib ( 500 mg ) or matching placebo by simple randomisation with no strati cation factors . 
this trial is registered , number isrctn29580179 . findings between march 30 , 2009 , and nov 18 , 2011 , 450 patients were randomly assigned to treatment groups ( one patient withdrew consent ; 224 patients allocated ge tinib and 225 allocated placebo included in analyses )  . 
overall survival did not di er between groups ( median 373 months , 95% ci 323450 , for ge tinib vs 367 months , 95% ci 297437 , for placebo ; hazard ratio [ hr ] 090 , 95% ci 074109 , p = 029 )  . 
among the prespeci ed patientreported outcomes ( 110 patients on ge tinib and 121 on placebo completed both baseline and 4 week questionnaires and were included in analyses ) , odynophagia was signi cantly better in the ge tinib group ( adjusted mean di erence 861 , 95% ci 1449 to 273 ; n = 227 ; p = 0004 ) , whereas the other outcomes were not signi cantly improved compared with placebo : global quality of life ( 269 , 95% ci 233 to 772 , n = 231 , p = 0293 ) , dysphagia ( 318 , 95% ci 836 to 200 , n = 231 , p = 0228 ) , and eating ( 411 , 95% ci 996 to 175 , n = 229 , p = 0168 )  . 
median progression - free survival was marginally longer with ge tinib than it was with placebo ( 157 months , 95% ci 123190 in the ge tinib group vs 117 months , 95% ci 107137 in the placebo group ; hr 080 , 95% ci 066096 , p = 0020 )  . 
the most common toxicities were diarrhoea ( 36 [ 16% ] of 224 patients on ge tinib vs six [ 3% ] of 225 on placebo ) and skin toxicity ( 46 [ 21% ] vs two [ 1% ] ) , both mostly grade 2 . 
54 ( 24% ) of patients in the ge tinib group achieved disease control at 8 weeks , as did 35 ( 16% ) of patients on placebo ( p = 0023 )  . interpretation the use of ge tinib as a second - line treatment in oesophageal cancer in unselected patients does not improve overall survival , but has palliative bene ts in a subgroup of these di cult - to - treat patients with short life expectancy . 
symptom scales or single items : high score = high level of symptoms or problems . table 1 : baseline clinical characteristics and patient - reported outcomes reported outcomes , the latter to explore the e ect of ge tinib on generic and disease - speci c aspects of health - related quality of life . 
to the best of our knowledge , cog the rst randomised trial of systemic therapy in this indication . ( cancer oesophagus ge tinib ) methods patients and study design for this phase 3 randomised trial , patients were recruited from 48 uk centres . 
eligible patients were adults ( 18 years ) with histologically con rmed adenocarcinoma , squamous - cell carcinoma , or poorly di erentiated oesophageal cancer or type i / ii siewert junctional tumours , had up to two previous chemotherapy and one regimens , who performance chemoradiotherapy status 02 , ability to swallow tablets , no contraindications to ge tinib , and either measurable or evaluable disease on ct . 
patients receiving cytotoxic chemotherapy , immunotherapy or hormonal therapy , radiotherapy to site of measurable or evaluable disease within the previous 4 weeks , or who had evidence of clinically active interstitial lung disease or abnormal blood results by prede ned criteria ( serum bilirubin 3 times upper limit of reference range , aspartate or alanine aminotransferase 25 times the upper limit of normal if no demonstrable liver disease ) were excluded . written informed consent was obtained . 
the study was undertaken in accordance with the protocol , good clinical practice , and the declaration of helsinki , and was approved by national research ethics service committee ( rec reference : 08 / h0505 / 127 )  . 
toxicities of grade 25 were collected for skin toxicity and diarrhoea only , and grade 35 for all other toxicities , as per the protocol . an independent data safety monitoring committee did safety reviews twice a year . randomisation and masking patients were randomly assigned ( 1 : 1 ) to oral ge tinib 500 mg / day or matching placebo , as two 250 mg tablets taken orally per day . 
6 months after completion of recruitment the masking was broken for patients remaining on trial treatment and patients on ge tinib were allowed to continue on ge tinib . centre and procedures all patients received best supportive care , de ned in the study protocol and delivered according to local pathways within each participating including community and hospice care . 
best supportive care included all symptomatic supportive measures deemed appropriate and indicated by local investigators including endoscopic stenting , specialist palliative care services , pain management , blood transfusions , and nutritional support , but excluding cytotoxic chemotherapy , immunotherapy , hormonal therapy ( excluding contraceptives and replacement steroids ) , or experimental medicines while patients were on trial drug . 
the protocol provided detailed guidelines for dose interruption ( maximum of 14 days ) or single dose reduction to 250 mg / day for adverse events . patients had a baseline ct scan of chest , abdomen , and pelvis , repeated at 4 and 8 weeks and then every 8 weeks until disease progression . 
patients with progressive disease , or stable disease with symptom deterioration , discontinued randomised treatment . outcomes the primary outcome was overall survival , de ned as time from randomisation until death from any cause with censoring for patients still alive at the end of the study . 
 progression - free survival was de ned as time from randomisation until radiological or clinical progression or death from any cause if progression was not previously reported , with censoring for patients alive and progression free at the end of the study . 
safety was measured by assessment of adverse reactions and toxicities of grade 25 for skin toxicity and diarrhoea ( known side - e ects of ge tinib ) and grade 35 for all other toxicities , with common terminology criteria for adverse events ( version 4.0 ) , monitored continuously throughout treatment and up to 30 days after treatment completion . health - related quality of life was assessed with the for research and generic european organisation treatment of cancer ( eortc ) qlq - c30 , 17 and the vol 15 july 2014 articles 100 075 050 025 100 075 050 025 100 075 050 025 placebo , median 367 months getinib , median 373 months hr 0901 ( 95% ci 07431094 ) log - rank test p = 0293 ps0 , median 607 months ps1 , median 393 months ps2 , median 197 months ps0 , hr 100 ps1 , hr 141 ( 95% ci 111179 ) ps2 , hr 298 ( 95% ci 223399 ) log - rank test p < 00001 placebo , median 117 months getinib , median 157 months hr 0797 ( 95% ci 06590964 ) log - rank test p = 0020 disease control was de ned as complete or partial response and stable disease observed at 4 weeks with response sustained for at least a further 4 weeks , con rmed at the 8 week scan , with all other patients assumed to not have achieved disease control . statistical analysis the sample size of 450 was estimated to detect an improvement from 10% 1 - year survival , as reported by previous phase 2 trials9 , 14 to 18% with a power of 825% , two - sided 5% signi cance allowing for a 10% loss to follow - up ( hazard ratio [ hr ] 0745 , 389 events )  . a statistical analysis plan was nalised before masking was broken and analysis undertaken . 
sensitivity analyses of overall and progression - free survival were done in the per - protocol population , de ned as all patients randomly assigned to treatment groups , excluding those who did not start treatment , or who had major protocol deviation ( no previous treatment , treatment breaks of > 14 days )  . 
an intention - to - treat analysis for survival used kaplan - meier survival curves and the log - rank test , with cox proportional hazards modelling to estimate hrs and 95% cis . 
binary outcomes were compared with the test . to reduce errors from multiple testing , four patientreported outcomes were prespeci ed as of particular importance : global quality of life , dysphagia , eating restrictions , and odynophagia . 
patient - reported outcomes were compared with ancova at 4 weeks adjusted for baseline values , therefore only patients completing both baseline and 4 week questionnaires were included in the intention - to - treat analysis . 
this analysis was repeated at 8 and 12 weeks , again when baseline values were available for adjustment . response for patients with measurable lesions was assessed by comparison of the percentage change ( from baseline to 4 weeks ) in longest diameter of the target lesions and presented as a waterfall plot . 
 protocol analyses were done with stata version 12.0. this trial is registered , number isrctn29580179 . role of the funding source the funding and sponsoring parties had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 results from march 30 , 2009 , to nov 18 , 2011 , 450 patients were enrolled and randomly assigned to receive ge tinib ( n = 225 ) or placebo ( n = 225 ) and followed up until death number at risk getinib placebo number at risk getinib placebo months from randomisation figure 2 : survival kaplan - meier plots of overall survival by ( a ) treatment and ( b ) performance status , and ( c ) progression - free survival by treatment . 
a di erence of eight points was deemed to be of clinical importance . 898 vol 15 july 2014 articles hazard ratio ( 95% ci ) 067 ( 046098 ) 083 ( 064108 ) 081 ( 054123 ) 081 ( 065101 ) 072 ( 048108 ) 080 ( 064099 ) 073 ( 048109 ) 079 ( 062101 ) 082 ( 060111 ) 082 ( 067101 ) 070 ( 044112 ) at the end of the study , 417 ( 93% ) of 449 patients had died and 432 ( 96% ) had disease progression . 
patients reported high levels of symptoms for eating restrictions , fatigue , pain , insomnia , appetite loss , anxiety , and weight loss and poor global quality of life . median duration of treatment was 44 days ( range 0680 ) on ge tinib versus 35 days ( 0371 ) for placebo . 
210 serious adverse events occurred in 150 patients : 101 ( 45% ) of 225 patients on placebo and 109 ( 49% ) of 224 on ge tinib ( p = 074 )  . 
30 ( 7% ) of 449 patients had fatal serious adverse events , of which three were judged to be related to drug toxicity ( two in the placebo group and one in the ge tinib group )  . 
grade 25 toxicities reported in more than 10% of patients in the ge tinib group were diarrhoea ( 36 [ 16% ] of 224 patients ) , skin toxicity ( 46 [ 21% ] patients ) , and fatigue ( 24 [ 11% ] patients ; table 2 )  . 
most of the excess toxicities were grade 2 , with grade 3 diarrhoea reported in 13 ( 6% ) of 224 patients and skin rash in ve ( 2% ) ; no grade 4 or 5 diarrhoea or skin toxicity was reported . 
 dose reduction from 500 mg to 250 mg occurred in only 12 ( 3% ) of 449 patients ( ten [ 4% ] of 224 on ge tinib )  . getinib placebo ( e / n ) ( e / n ) 45 / 57 107 / 117 50 / 50 diagnosis adenocarcinoma squamous cell 160 / 173 41 / 50 52 / 56 120 / 125 44 / 44 162 / 168 53 / 56 disease site oesophageal junctional i / ii 152 / 171 50 / 53 173 / 181 43 / 44 previous treatment 123 / 137 79 / 87 131 / 137 84 / 87 male female 167 / 183 35 / 41 182 / 189 34 / 36 050 075 favours getinib favours placebo figure 3 : hazard ratio plot of the treatment e ect by prognostic factors for progression - free survival placebo progressive disease progressive disease getinib 100 stable disease partial response stable disease partial response figure 4 : waterfall plots for patients with measurable disease at baseline and 4 weeks , response con rmed at 8 weeks green = recorded as progressed by 8 weeks , might have been new lesions . 
54 ( 24% ) of 224 patients in the ge tinib group had disease control at 8 weeks ( 48 stable disease and six partial response ) as did 35 ( 16% ) of 225 patients in the placebo group ( 34 stable disease and one partial response ) ( p = 0023 )  . 
40 ( 23% ) of 170 patients with adenocarcinoma treated with ge tinib had disease control at 8 weeks as did 14 ( 28% ) of 50 patients with squamous - cell carcinoma treated with ge tinib ( p = 0478 )  . 
only 98 ( 22% ) of 449 patients had further therapy once they came o study treatment , with no di erences in patients receiving further therapy between the two groups . 
44 ( 10% ) of 449 patients received further chemotherapy ( 23 [ 10% ] of 225 on placebo and 21 [ 9% ] of 224 on ge tinib ) ; 43 ( 10% ) of 449 patients were treated with palliative radiotherapy ( 24 [ 11% ] of 225 on placebo and 19 [ 8% ] of 224 on ge tinib ) ; 30 ( 7% ) of 449 patients were treated with stents ( 17 [ 8% ] of 225 on placebo and 13 [ 6% ] of 224 on ge tinib ) and 13 ( 3% ) of 449 with other treatments . compliance for patient - reported outcomes at baseline was 94% ( 423 of 449 patients ) and remained high at 79% ( 245 / 312 ) , 74% ( 133 / 180 ) , and 66% ( 84 / 127 ) at 4 , 8 , and 12 weeks , respectively . 
1321 ( 3% ) of 48 675 individual items were missing from the questionnaires and these were imputed according to eortc guidelines.19 4 weeks after the start of treatment , 312 ( 69% ) of 449 patients ( 154 [ 68% ] of 225 in the placebo group and 158 [ 71% ] of 224 in the ge tinib group ) were still alive and progression free and available to complete the 4 - week questionnaire . 
 figure 5 shows the mean raw scores for the prespeci ed patient - reported outcomes over the four timepoints . in total , 231 patients ( 121 placebo , 110 ge tinib ) completed both baseline and 4 week questionnaires and could be included in the primary analysis of patientreported outcomes . 
di erences between the ge tinib and placebo groups in the prespeci ed domains of global quality of life , dysphagia , and eating restrictions at 4 weeks compared with baseline were not signi cant ; however odynophagia , the fourth prespeci ed domain , worsened from baseline to 4 weeks for patients on placebo and signi cantly for patients on ge tinib ( table 3 )  . 
other exploratory patient - reported ( or not functions and symptoms were worsened ) for patients on ge tinib compared with those on placebo : patients on ge tinib had less deterioration in social functioning and fewer problems with pain , constipation , cough , and speech , than did patients on placebo , but reported more diarrhoea ( table 3 )  . 
moreover , repeated improved improved baseline 4 weeks 8 weeks 12 weeks number of patients per timepoint placebo : baseline 214 ; 4 weeks 127 ; 8 weeks 60 ; 12 weeks 33 getinib : baseline 209 ; 4 weeks 118 ; 8 weeks 73 ; 12 weeks 51 figure 5 : mean raw scores for prespeci ed patient - reported outcomes at all timepoints higher score equates to better quality of life or more symptoms . all patients in the trial were analysed ( not separated by treatment ) , median overall survival of those with performance status 0 was 61 months ( 95% ci 4974 ) , status 1 was 39 months ( 3244 ) , and status 2 was 20 ( 1624 ) months ( p < 00001 ; gure 2b )  . progression - free survival was marginally better with ge tinib than it was with placebo ( median 157 months , 95% ci 123190 , with ge tinib vs 117 months , 107137 , with placebo ; hr 080 , 95% ci 066096 ; log - rank test , p = 0020 ; gure 2c )  . 
for the symptom scores a negative adjusted mean di erences implies that patients on ge tinib has less deterioration or even improvement of symptoms compared with those on placebo , whereas a positive di erence implies that the symptoms have worsened more for those on ge tinib . 
 table 3 : treatment e ect at 4 weeks for patient - reported outcomes measures over time did not detect any statistical di erences in the four prespeci ed domains . discussion cog is the rst randomised trial of systemic therapy in patients with oesophageal cancer progressing after chemotherapy ( panel )  . 
 cog showed no overall survival bene t for ge tinib over placebo , but a small bene t in progression - free survival and some aspects of health - related quality of life were observed , including an improvement in a prespeci ed patient - reported outcome , odynophagia . 
the toxicity pro le observed in the current study was generally consistent with that previously observed for ge tinib in in other tumour types20 with no new safety signals identi ed . a suggestion of progression - free survival bene t for ge tinib was observed across most subgroups , including adenocarcinoma , squamous - cell cancers , and oesophagus and junctional cancers , although not all di erences were signi cant . 
although the biological di erences between adenocarcinoma and squamous - cell vol 15 july 2014 articles global quality of life cognitive physical emotional role social constipation hair loss speech cough odynophagia pain dyspnoea anxiety sleep saliva reux eating pain and discomfort appetite choking dysphagia eating with others taste finance fatigue nausea / vomiting body image weight loss dry mouth diarrhoea than combination with chemotherapy as well as tkis , oesophagogastric cancers have also been treated with anti - egfr antibodies . 
single agent activity is low22 and investigators have focused on combination with chemotherapy.23 , 24 however , in phase 3 trials combining anti - egfr monoclonal antibodies with chemotherapy in the rst - line setting , overall survival was lower with targeted agents such as panitumumab and cetuximab than with chemotherapy.23 , 24 one explanation is that anti - egfr therapies are not clinically active in oesophagogastric cancer . 
however a similar absence of bene t in molecularly unselected patients has also been reported when egfr tkis or anti - egfr antibodies are combined with platinum - based chemotherapy in several studies in various other malignancies , notably in non - small - cell lung cancer25 and colorectal cancer.26 monotherapy with egfr tkis and anti - egfr antibodies after chemotherapy has proven useful in nonsmall - cell lung cancer and colorectal cancer.27 , 28 our nding of anti - tumour activity for ge tinib in a subgroup of responsive patients in the cog trial similarly suggests that single agent anti - egfr therapy might be more e ective oesophageal cancer . 
in oesophageal cancer a predictive biomarker that identi es a ge tinib - responsive subgroup might also be useful for other anti - egfr therapies , such as monoclonal antibodies , in this disease type . study has including detailed strengths , examination of the e ect of treatment on patient - reported outcomes , and it is the rst multicentre randomised trial in oesophageal cancer that has included a well - designed comprehensive assessment of patient - reported outcomes . 
for example , only patients who had not had disease progression at 4 weeks were asked to complete the patient - reported outcome questionnaires and are included in the analysis . 
this approach might have a ected the results and patients with disease progression at this timepoint might have had a di erent outcome pro le because treatment might have been withdrawn earlier because of general deterioration . 
skin toxicity is a known side - e ect of ge tinib and was not directly measured with the patient - reported outcomes , although the global quality - of - life score re ects problems with skin toxicity , and this outcome did not vary between groups . our in conclusion , the phase 3 cog study did not meet its primary endpoint of a signi cant overall survival bene t for ge tinib compared with placebo in unselected mean dierence between groups getinib better placebo better figure 6 : mean change in health - related quality - of - life outcomes from baseline to 4 weeks positive values on the functioning scale and negative values on the symptom scale denote bene t from ge tinib compared with placebo . carcinoma are increasingly characterised , 21 these data were not available at the time of study design and there was no consistent indication from phase 2 trials of ge tinib or erlotinib that histological subtypes of oesophageal cancer responded di erently . 
in the context of the rst randomised trial in the second - line setting in oesophageal cancer , we believe that this observation is clinically signi cant . the increased disease control , bene t in some patient - reported outcomes , and progression - free survival might suggest the existence of a ge tinibresponsive subgroup of patients with oesophageal cancer . 
we are undertaking tumour specimens from cog to identify predictive biomarkers for ge tinib ( transcog study )  . translational research 902 vol 15 july 2014 articles see online for appendix panel : research in context systematic review pubmed was searched for clinical trials ( published in english only ) assessing second - line therapies in patients with oesophageal cancer progressing after chemotherapy . 
the search terms used were oesophageal or esophageal , cancer or neoplasm or malignancy or malignant , second - line or salvage or supportive care or advanced , randomised or randomized , with no publication date parameter . 
evidence is scarce and no phase 3 trials have been done to support use of second - line therapies in this setting , and very few data exist for the e ect of treatments on health - related quality of life , which is important in clinical decision making in such situations when life expectancy is poor . 
because of biological di erences between gastric and oesophageal cancers , extrapolation of data from phase 3 trials in gastric cancer to oesophageal cancer is likely to result in suboptimum outcomes for patients . 
a systematic review of the use of egfr tyrosine - kinase inhibitors in oesophageal cancer showed that in a series of phase 2 trials , objective responses to ge tinib or erlotinib were observed in patients who had disease progression after previous chemotherapy and the toxicity of treatment was mild.9 to the best of our knowledge , cog was established as the rst phase 3 study in oesophageal cancer to investigate both survival and patient - reported outcomes in the second - line setting with patients randomly assigned to treatment with ge tinib or placebo . interpretation we noted no signi cant di erence between ge tinib and placebo for the primary outcome , overall survival ; however , ge tinib was well tolerated and improved progression - free survival , disease control , and patient - reported outcomes . 
the data also suggest that a subgroup of patients might gain clinically signi cant bene ts from this treatment and identi cation of a predictive biomarker for this ge tinib - responsive subgroup of patients is important . patients with oesophageal cancer progressing after previous systemic chemotherapy . 
 together with the observation of rapid and durable responses and prolonged disease control in a few patients treated with ge tinib , this nding suggests antipossible tumour activity in an as yet unidenti ed small ge tinib - responsive subgroup . 
the data presented are valuable for clinical practice and decision making , indicating that without biomarker strati cation , ge tinib has marginal clinical bene ts in advanced oesophageal cancer ; however , patient - reported outcomes suggest some useful palliation of symptoms . 
 identi cation of a predictive biomarker to identify any of patients with subgroup ge tinib - responsive oesophageal cancer would greatly increase clinical usefulness and is the priority for ongoing work . speci c contributors drf was chief investigator for the trial . 
jmb was the quality - of - life adviser for the trial and was involved in the study design , data analysis , and the interpretation and writing of this paper . 
all authors have contributed to , seen , and approved the nal draa full list of all cog study investigators is shown in the appendix . declaration of interests drf received a grant from astrazeneca to continue with ongoing research into frgr inhibitor azd4547 and money for an educational dvd on egfr mutation analysis . 
jmb is supported by the mrc conduct - ii hub for trials methodology research acknowledgments the study was funded by cancer research uk and jointly sponsored by the university of oxford and the royal wolverhampton hospitals nhs trust . 
we thank the patients who participated in the cog trial ; the investigators , the research nurses , clinical sta from the individual trial centres and sta members from the oncology clinical trials o ce ( octo ) at the university of oxford who provided ongoing support . 
we thank the members of the trial steering committee ( tom crosby [ velindre cancer centre ] , christopher poole [ university of warwick ] , and helen marshall [ university of leeds ] ) , and the independent data and safety monitoring committee ( matthew sydes [ mrc clinical trials unit ] , mark saunders [ christie hospital nhs foundation trust ] , and nicola levitt [ john radcli e hospital ] )  . comment published online july 29 , 2013 s1470 - 2045 ( 13 ) 70364 - 4 see articles page 989 copyright buzdar . 
 the tailor study will contribute to more rational use of chemotherapy and egfr tyrosine kinase inhibitors in the treatment of nsclc , based on its molecular pro le . * jacek jassem , rafa dziadziuszko department of oncology and radiotherapy , medical university of gdask , 80 211 gdask , poland jjassem@gumed.edu.pl we declare that we have no con icts of interest . shepherd fa , rodrigues pereira j , ciuleanu t , et al . 
erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
ge tinib versus cisplatin plus docetaxel in patients with non - small - cell lung cancer harbouring mutations of the epidermal growth factor receptor ( wjtog3405 ) : an open label , randomised phase 3 trial . 
erlotinib versus chemotherapy as rst - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
a randomised trial of erlotinib versus docetaxel as second - line treatment of patients with advanced non - small cell lung cancer and wild - type epidermal growth factor receptor ( tailor )  . 
 combination endocrine treatments unproven in breast cancer and although ovarian ablation , which was introduced more than 100 years ago , was the rst endocrine treatment for advanced breast cancer , followed by adrenalectomy and hypophysectomy . 
these ablative therapies have since been replaced by antioestrogen treatments , luteinisinghormone - releasing hormone agonists , and aromatase inhibitors.1 other endocrine treatments with di erent mechanisms of action have also become available for breast cancer : oestrogens , progestins , androgens , antiandrogens , selective oestrogen - receptor downregulators . 
 the combinations of superiority of chemotherapeutic agents with di erent mechanisms of action to single agents has been established in the treatment of early and advanced breast cancer , 2 that of combinations of endocrine treatments has not been shown.1 several combinations of hormonal agents have been assessed in patients with advanced breast cancer , with no consistent improvement in either time to progression of disease or survival.3 additionally , the combination of an antioestrogen treatment ( tamoxifen ) and ovarian suppression with luteinising - hormone - releasing hormone agonist does not lead to improvements in disease - free or overall survival when compared with antioestrogen treatment alone in premenopausal women with early breast cancer.4 a large , prospective , double - blind trial5 comparing tamoxifen with an aromatase inhibitor ( anastrozole ) and tamoxifen or anastrozole alone as adjuvant treatment for breast cancer showed that the combination did not improve either disease - free or overall survival . 
indeed , the group who received the combination was discontinued after initial analysis of the data.5 suggested aromatase that inhibitor because preclinical data6 the and combination of fulvestranta member of the newest class of hormonal agents , selective oestrogen receptor downregulators was superior to either agent alone against breast tumours in mice , three prospective studies79 have assessed this approach in postmenopausal women with advanced breast cancer . 
in the lancet oncology , stephen johnston and colleagues report results of a phase 3 , european , multicentre trial.7 postmenopausal women with hormone - receptor - positive breast cancer who had relapsed or progressed while receiving a nonsteroidal aromatase inhibitor were randomly assigned to receive fulvestrant plus anastrozole , fulvestrant plus vol 14 september 2013 comment anastrozole - matched placebo , or the steroidal aromatase inhibitor exemestane . 
no improvement in progressionfree survival was recorded in the group who received fulvestrant plus anastrozole ( median 44 months , 95% ci 3454 ) compared with fulvestrant plus placebo ( 48 months , 3655 ; hazard ratio [ hr ] 100 , 95% ci 083121 ; log - rank p = 098 ) , or in the group given fulvestrant plus placebo compared with exemestane ( 34 months , 3046 ; hr 095 , 079114 ; log - rank p = 056 )  . 
 another phase 3 study8 comparing the combination of anastrozole and fulvestrant as rst - line treatment in postmenopausal patients with hormone - receptorpositive advanced breast cancer also showed no advantages in terms of clinical e cacy for the combination compared with anastrozole alone . 
 by contrast , a phase 3 trial from north america9 compared the combination of anastrozole and fulvestrant with anastrozole alone as rst - line treatment in postmenopausal women with hormonereceptor - positive advanced breast cancer , and showed increased control of disease and survival with the combination of fulvestrant and anastrozole . 
however , as understanding of the mechanisms of resistance to endocrine treatment has improved , targeting of some pathways has resulted in new approaches that o er hope for disease control . 
 for example , postmenopausal patients with hormoneadvanced breast receptor - positive , her2 - positive cancer given endocrine and anti - her2 treatments have had longer control of disease than have those given endocrine treatment alone.1 indeed , a combination of an aromatase inhibitor with an anti - her2 treatment has been approved by the us food and drug administration for the management of postmenopausal patients with hormone - receptor - positive , her2 - positive advanced breast cancer.1 another e ective approach has been the combination of an mtor inhibitor ( everolimus ) with exemestane.10 the combination of exemestane with a histone deacetylase inhibitor ( entinostat ) has also had encouraging results.11 in conclusion , a combination of endocrine agents with di erent mechanisms of action will probably not result in a meaningful improvement in outcomes for patients with breast cancer . 
however , understanding of the mechanisms of resistance to hormonal agents continues to advance , and combinations of endocrine treatment with targeted agents that block resistance pathways should improve the outlook for patients with breast cancer that is resistant to endocrine treatment . aman u buzdar department of breast medical oncology , university of texas md anderson cancer center , houston , tx 77030 , usa abuzdar@mdanderson.org i declare that i have no con icts of interest . barrios c , forbes jf , jonat w , et al . 
use of luteinisinghormone - releasing hormone agonists as adjuvant treatment in premenopausal patients with hormone - receptor - positive breast cancer : a meta - analysis of individual patient data from randomised adjuvant trials . 
fulvestrant plus anastrozole or placebo versus exemestane alone after progression on non - steroidal aromatase inhibitors in postmenopausal patients with hormonereceptor - positive locally advanced or metastatic breast cancer ( sofea ) : a composite , multicentre , phase 3 randomised trial . 
fact : an open - label randomized phase iii study of fulvestrant and anastrozole in combination compared with anastrozole alone as rst - line therapy for patients with receptorpositive postmenopausal breast cancer . 
randomized phase ii , double - blind , placebo - controlled study of exemestane with or without entinostat in postmenopausal women with locally recurrent or metastatic estrogen receptor - positive breast cancer progressing on treatment with a nonsteroidal aromatase inhibitor . 
j clin oncol 2013 ; 31 : 212835 . 918 vol 14 september 2013 comment published online august 20 , 2014 s1470 - 2045 ( 14 ) 70198 - 6 this online publication has been corrected . 
the corrected version rst appeared at thelancet.com / oncology on september 29 , 2014 see articles page 1109 the protect trial : what can we expect ? profound changes in the detection of prostate cancer have occurred since prostate - speci c antigen ( psa ) introduced as a biomarker test for prostate was cancer . 
instead of the disease being detected at an advanced stage when symptoms caused by invasive growth emergedwith palliative treatment the main optionprostate cancer is diagnosed early on in the disease course . 
 largest randomised screening trial showed that psa testing , with its concomitant early treatment , substantially reduced the development of metastatic disease and prevented prostate cancer deaths.1 , 2 however , not only were potentially lethal tumours detected at an early , treatable stage , but also many non - lethal tumours were diagnosed.2 this over - diagnosis leads to substantial overtreatment with its associated side - e ects.3 therefore , whether treatment of early detected , localised cancers will result in a bene t or mainly cause harm is unclear . 
 furthermore , with many treatment options to choose from , evidence of one being most bene cial is needed . indeed , results of the several researchers have attempted to compare the e ectiveness of di erent curative treatment options ( including no or no initial radical treatment ) for early , psa - detected , localised prostate cancer . 
however , most failed because of di culties in recruiting men willing to leave their cancer treatment to chance.4 in the lancet oncology , j athene lane and colleagues5 present the data for the recruitment phase of the prostate testing for cancer and treatment ( protect ) trial . 
the group of investigators should already be commended for this careful work , which will result in a unique and highly informative dataset . in addition to the primary analysis , an interesting topic will be the very detailed assessment of quality of life , which is measured at recruitment ( before the diagnosis of prostate cancer ) , rst biopsy , and during follow - up for at least 10 years . 
a detailed assessment of the e ect of di erent treatment modalities on quality of life might become crucial if the primary analysis shows a bene t in prostate cancer mortality for early active intervention . 
active surveillance protocols advise men to switch to active treatment much sooner.6 additionally , some men ( and most likely their doctors ) might switch to active treatment because of anxiety or other nonprotocol - based reasons ( eg , high absolute psa value ) .7 however , the strict protocol and visits to a dedicated study nurse might reduce this number . 
 the limitations of the design are clearly emphasised , being often a direct result of the inevitable , relatively long duration of the trial and the rapid evolvement in curative treatment modalities . 
a limitation that might a ect the ability of drawing de nite conclusions about the e ectiveness of the three conventional treatment options for localised prostate cancer is the expected prostate cancer mortality at 10 years of follow - up . 
pairwise signi cance tests ( ie , comparing active monitoring with radical prostatectomy , active monitoring with radiation therapy , and radical prostatectomy with radiation therapy ) are done only if the overall test yields a signi cant p value ( < 005 )  . 
initial estimates projected a 15% prostate cancer mortality in the active monitoring group at a median 10 - year follow - up , which was later adjusted to a 10% prostate cancer mortality , based on more recent mortality data . 
with 10% prostate cancer mortality in the active monitoring group , sample size was calculated to be able to show a 46% absolute mortality di erence ( the percentage point di erence ) , or hazard ratio of 054 , compared with radical treatment with a power of 80% . 1046 vol 15 september 2014 comment but is this 10% prostate cancer mortality estimate , based on 2008 uk mortality statistics , realistic ? as suggested by the investigators , opportunistic testing in the uk was and still is relatively rare , which implies that these uk mortality statistics are most likely not applicable to the psa - based screen - detected cohort of protect . 
this theory is supported by data from the rotterdam section of the european randomized study of screening for prostate cancer.8 of all 1071 patients with psa - based screen - detected prostate cancer at the initial screening visit ( including advanced and metastatic disease ) , 78 ( 73% ) died of prostate cancer after a median follow - up of 13 years . 
in the pivot trial at a median follow - up of 10 years , 31 ( 84% ) of 367 prostate cancer deaths were reported in the observation group and 21 ( 58% ) of 364 in the radical prostatectomy group ( hr 063 [ 95% ci 036109 ] ) .9 as lane and colleagues5 point out correctly , the protect trial included men with much lower psa values , lower age , and fewer high - stage cancers , and men in the active monitoring group were o ered radical treatment if progression occurred ; all factors that will most likely decrease the expected prostate cancer mortality . 
in fact , the 10 - year prostate cancer survival reported by active surveillance cohorts , with more similar tumour characteristics , ranges from 96100%.10 although a 46% absolute mortality di erence between active monitoring and radical treatment might be expected , the calculated 80% power will decrease substantially if fewer events occur than expected . 
if , however , the expected 10% prostate cancer mortality in the active monitoring group turns out to be realistic , the causes of this discrepancy with the earlier mentioned observations will be interesting to explore . 
impact of a multi - disciplinary patient education session on accrual to a di cult clinical trial : the toronto experience with the surgical prostatectomy versus interstitial radiation intervention trial . 
 j surg oncol 2014 ; 109 : 83035 . future of alk inhibition in non - small - cell lung cancer progress in de ning molecular targets of oncogenesis and drugs to inhibit cancer growth in speci c populations has led to augmented outcomes for patients and new expectations in the development of treatments . 
 the eml4alk fusion protein was identi ed in patients lung cancer ( nsclc ) in 2007.1 with non - small - cell rearrangements in the alk gene lead to constitutive signalling , triggering transforming properties . 
it has an objective response of 61% and results in median progression - free survival of 97 months.2 crizotinib was superior to chemotherapy as second - line treatment published online august 19 , 2014 s1470 - 2045 ( 14 ) 70390 - 0 this online publication has been corrected . 
the corrected version rst appeared at thelancet.com / oncology on september 29 , 2014 see articles page 1119 vol 15 september 2014 1047 editorial this online publication has been corrected . 
 the corrected version rst appeared at thelancet.com / oncology on sept 4 , 2014 see articles lancet oncol 2014 ; 15 : 68999 see editorial lancet oncol 2014 ; 15 : 667 patient priority in the era of patent expiries on aug 8 , 2014 , the uk national institute for health and care excellence ( nice ) ruled that trastuzumab emtansine is not cost e ective for routine use for patients with her2 - positive breast cancer in englands national health service . 
 using clinical data from the emilia and th3resa trials , roche valued the drug at just over 90 000 per patient more than twice the price of trastuzumab alonedespite a lack of head - to - head evidence showing trastuzumab emtansines greater e cacy compared with trastuzumab to justify the higher price . 
on july 28 , 2014only 11 days before nice issued their press releasethe patent for trastuzumab ( which earnt the company us$59 billion in 2011 alone ) expired in the european union ( eu )  . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy investment in research and development . 
despite the deal falling through , the attempted acquisition may be representative of pharmaceutical companies responses in recent years to try to recoup losses from a series of drugs that have simultaneously gone o patent . 
 this phenomenonthe so - called patent cli has been extensively reported since one of the rst blockbusters , atorvastatin , a cholesterol - lowering drug that had estimated global sales in excess of 64 billion a year , went o patent in 2011 . 
since then , and in light of an unprecedented number of blockbuster drugs coming o or soon to come o patent , a urry of mergers and acquisitions by pharmaceutical companies has taken place in an attempt to revive pro ts , most notably in diversifying their portfolio in to low - risk revenue streams ( eg , animal health , medical devices , and generic drugs ) as well as expanding their pipelines to include biological agents . 
despite the number of legitimate steps taken to extend patent licences , there have also been a series of morally dubious legal strategies used by patent proprietors to extend their patents . 
in addition to applying for supplementary protection certi cates ( allowing the patent to be extended up to 5 years in the eu ) , and 6 - month paediatric exclusivity licences , both of which are common practices to extend patent protection , pharmaceutical companies have explored other ways to gain extensions to their existing patents , such as new approvals in di erent medical settings to the original application . but where is the line between legitimate patentable development , and abusive extension of patent rights ? in 2001 , glaxosmithkline accumulated 5 years of 30 - month stay approval from the us food and drug administrationan automatic period granted to originator companies if threatened by patent infringementfor the drug paroxetine . 
although lawful , this example does raise the question as to whether these strategies are a violation of patients rights of access to a ordable , e ective medicines , especially considering the unsustainable nancial burdens faced by health - care systems worldwide . 
in a bid to maintain income , it is worrying that the pharmaceutical industry might opt to prioritise loopholes in legislation , undertake litigation , and consider mergers and acquisitions as a more rewarding primary focus to secure revenue , as opposed to competitive income from the development of new medicinal products . 
it is crucial , therefore , that appropriate legislation is in place to encourage strike a balance pharmaceutical between their own pro t ability and upholding a contemporary social and ethical responsibility to allow a ordable access to medicines to those most in need . 
 the lancet oncology companies vol 15 september 2014 1039 correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections adenoma surveillance and colorectal cancer incidence : a retrospective , multicentre , cohort study wendy atkin , kate wooldrage , amy brenner , jessica martin , urvi shah , sajith perera , fiona lucas , jeremy p brown , ines kralj - hans , paul greliak , kevin pack , jill wood , ann thomson , andrew veitch , stephen w duffy , amanda j cross summary background removal of adenomas reduces colorectal cancer incidence and mortality ; however , the benefit of surveillance colonoscopy on colorectal cancer risk remains unclear . 
we examined heterogeneity in colorectal cancer incidence in intermediate - risk patients and the effect of surveillance on colorectal cancer incidence . methods we did this retrospective , multicentre , cohort study using routine lower gastrointestinal endoscopy and pathology data from patients who , after baseline colonoscopy and polypectomy , were diagnosed with intermediaterisk adenomas mostly ( > 99% ) between jan 1 , 1990 , and dec 31 , 2010 , at 17 hospitals in the uk . 
patients were followed up through to dec 31 , 2014 . we assessed the effect of surveillance on colorectal cancer incidence using cox regression with adjustment for patient , procedural , and polyp characteristics . 
this trial is registered , number isrctn15213649 . findings 253 798 patients who underwent colonic endoscopy were identified , of whom 11 944 with intermediate - risk adenomas were included in this analysis . 
compared to no surveillance , one or two surveillance visits were associated with a significant reduction in colorectal cancer incidence rate ( adjusted hazard ratio 057 , 95% ci 040080 for one visit ; 051 , 031084 for two visits )  . 
without surveillance , colorectal cancer incidence in patients with a suboptimal quality colonoscopy , proximal polyps , or a high - grade or large adenoma ( 20 mm ) at baseline ( 8865 [ 74% ] patients ) was significantly higher than in the general population ( sir 130 , 95% ci 106157 )  . 
by contrast , in patients without these features , colorectal cancer incidence was lower than that of the general population ( sir 051 , 95% ci 029084 )  . interpretation colonoscopy surveillance benefits most patients with intermediate - risk adenomas . 
however , some patients are already at low risk after baseline colonoscopy and the value of surveillance for them is unclear . funding national institute for health research health technology assessment , cancer research uk . copyright the author ( s )  . 
a 3 year surveillance interval was indicated for those at intermediate risk on the basis of evidence from a randomised trial that compared different surveillance intervals for the detection of advanced adenomas at follow - up . 
the results of the study showed a clear benefit from surveillance in patients with one or more advanced adenomas , whereas in those with only non - advanced adenomas , the benefit was less marked . 
evidence suggests that the quality of colonoscopy has improved and that the number of missed or incompletely removed lesions has decreased since the publication of a uk national colonoscopy audit in 2001 , leading to implementation of national training standards and quality assessments . 
no study has yet assessed the effect of surveillance on long - term colorectal cancer risk among patients offered 3 - yearly surveillance , who represent most patients offered surveillance . added value of this study our study assessed colorectal cancer risk in patients considered to be at intermediate risk . 
across 8 years of follow - up , our data identified risk factors for colorectal cancer at baseline colonoscopy that permitted further stratification of these patients into lower - risk and higher - risk subgroups . 
patients with an incomplete colonoscopy , poor bowel preparation , proximal polyps , or a high - grade or large adenoma ( 20 mm ) at baseline were at increased risk , and the first surveillance colonoscopy significantly reduced colorectal cancer risk . 
 by contrast , in patients without these baseline colonoscopy findings , future risk of colorectal cancer was already lower than that in the general population before any surveillance . implications of all the available evidence our results show that most patients who are currently offered 3 - yearly surveillance colonoscopy benefit substantially from attending at least one surveillance visit . 
evidence from this study will be important in informing future adenoma surveillance guidelines and will help to minimise the costs and risks associated with unnecessary colonoscopies . two consecutive negative colonoscopies ( appendix p 1 ) , whereas in the usa , there are no recommended criteria for stopping other than older age . the main aim of adenoma surveillance is to reduce the incidence of colorectal cancer , but very few studies have used long - term colorectal cancer incidence after adenoma removal to define risk groups and need for surveillance12 , 19 , 20 and none have looked at predictive factors for long - term colorectal cancer incidence in patients who are currently offered surveillance . 
 in this study , we estimated colorectal cancer incidence after baseline colonoscopy in patients who are recommended 3 - yearly surveillance , and assessed the effect of surveillance on colorectal cancer incidence . 
 we hypothesised that a subgroup of patients exists in whom surveillance colonoscopy could be stopped earlier , or for whom surveillance is not necessary , on the basis of their colorectal cancer incidence . methods study design and participants we did this retrospective , multicentre , cohort study using information from 17 uk hospitals with electronic records of lower gastrointestinal endoscopy and pathology data recorded for at least 6 years before the start of the study in 2006 ( appendix p 2 )  . 
the size of the catchment population for the 17 hospitals was estimated to be more than 65 million people.23 , 24 patients were eligible for inclusion in the study if they had a baseline colonoscopy and newly diagnosed intermediate - risk adenomas according to uk guidelines , defined as one - to - two large ( 10 mm ) adenomas , or threeto - four small adenomas ( appendix p 1 )  . 
we excluded patients with a history of bowel resection , colorectal cancer , inflammatory bowel disease , a family history of colorectal cancer , or any endoscopies without a date . we searched gastrointestinal endoscopy databases to identify patients who underwent colonic examination before dec 31 , 2010 , then we searched pathology databases for reports of colorectal lesions , using systematised nomenclature of medicine ( snomed ) codes ( versions 2 and 3 ) , systematized nomenclature of pathology ( snop ) codes , keywords , or multiple search terms . 
endoscopy see online for appendix 824 vol 18 june 2017 articles and pathology reports were linked and pseudonymised before being entered into an oracle ( 11g enterprise edition ) database . 
further details on hospital data collection and standard operating procedures are available in the appendices of our national institute for health research ( nihr ) health technology assessment ( hta ) report.25 we divided endoscopic examinations into visits ( ie , one or more examinations made in close succession to complete a full examination of the colon and remove detected lesions )  . 
we used a hierarchy of rules to assign a summary value for the size , histology , and location of lesions seen at multiple examinations.25 completeness of colonoscopy , and quality of bowel preparation26 were defined by the most complete examination and the best bowel preparation during the baseline visit . 
bowel preparation quality and completeness of colonoscopy , as assessed by the endoscopist , were obtained from endoscopy reports when not included as a separate field in the endoscopy database . patient , procedural , and polyp characteristics at baseline assessed as a - priori risk factors and confounders included age at first adenoma detection , sex , completeness of colonoscopy , quality of bowel preparation ( graded as excellent , good , adequate or satisfactory , and poor ) , 26 year of entry ( year first adenoma detected ) , and adenoma number ( total number recorded at baseline ) , size ( largest at baseline ) , histology and grade of dysplasia ( worst at baseline ) , and polyp location . 
 data on lifestyle factors , such as smoking and alcohol consumption , were not available . we ascertained the presence of colorectal cancers from hospital pathology reports and from national health service ( nhs ) digital , the nhs central register ( nhscr ) , and national services scotland ( nss )  . 
mortality data were provided by nhs digital , nhscr , and nss . ethics approval was granted by the royal free research ethics committee ( reference 06 / q0501 / 45 )  . 
approval for use of patient information without consent was granted by the patient information advisory group under section 60 of the health and social care act 2001 ( piag 105 [ e ] / 2006 )  . 
 identified at baseline had been incompletely resected if baseline examinations showed that they were left intact or partly removed , were in the same or adjacent segment of the colon , and had similar histology ; such cancers were excluded from the analysis . our sample size calculations stipulated that estimates of the colorectal cancer incidence rate have a coefficient of variation of about 30% ( ie , the standard error of the estimate would be 30% of the actual estimate )  . 
assuming conservatively a rate of two colorectal cancers per 1000 person - years , 20 , 27 , 28 approximate poisson distribution of incidence , and a simple univariate estimate of the rate , then nine colorectal cancer events and 4500 person - years in any given subgroup would give a coefficient of variation of 33% . 
assuming a smallest subgroup of interest of 15% of the cohort , we required at least 30 000 person - years ( 4500 divided by 015 ) and 60 colorectal cancers , or a total cohort of 6000 patients with at least 5 years of follow - up . 
because inclusion of covariates might increase standard errors , we aimed to include at least 10 000 patients . we censored time - to - event data at first colorectal cancer diagnosis , death , emigration , or december 31 , 2014 , for 253 798 patients with a lower gastrointestinal endoscopy for the protocol see ac.uk / programmes / hta / 043301 223 539 excluded 45 717 colorectal cancer or other colonic conditions * 16 081 colorectal cancer at baseline 6798 resection at or before baseline 30 555 inammatory bowel disease , crohns disease , colitis , or radiation proctitis or colitis 1745 polyposis , juvenile polyps , hamartomatous polyps 264 hereditary non - polyposis colorectal cancer or family history of adenomatous polyposis 14 volvulus 2752 no baseline colonoscopy 92 missing examination dates 174 978 no adenomas 18 264 not at intermediate risk 1033 not classiable 14 522 at low risk ( one or two adenomas , both small [ < 10 mm ] ) 2709 at high risk ( 5 small adenomas or 3 adenomas , at least one of which is large [ 10 mm ] ) 30 259 eligible patients with adenomas 11 995 intermediate - risk patients ( three or four small adenomas or one or two adenomas , at least one of which is large [ 10 mm ] ) 51 lost to follow - up statistical analysis the primary outcome was incident adenocarcinoma of the colorectu this outcome excluded in - situ cancer . 
p values calculated with test to compare patients with and without surveillance visits . table 1 : baseline patient , procedural , and polyp characteristics by surveillance visit attendance and exposure to successive surveillance visits started at the last procedure in each visit . 
some analyses divided each patients follow - up time into three distinct periods ; without surveillance ( from start of time at risk , censored at any first surveillance ) ; after first surveillance ( from first surveillance , censored at any second surveillance ) ; and after second surveillance ( from second surveillance to final date of censoring )  . we compared baseline characteristics in patients with and without surveillance visits using tests . 
 we did not use multiple imputation or inverse probability weighting to deal with missing data . we used one minus the kaplan - meier estimator of the survival function to show time to cancer diagnosis and to estimate the cumulative incidence of cancer with 95% cis at 3 , 5 , and 10 years ; we used the log - rank test to compare subgroups . 
we examined the effects of surveillance and patient , procedural , and polyp characteristics at baseline on long - term colorectal cancer incidence using cox proportional hazards models . we used univariable models to estimate unadjusted hazard ratios ( hr ) and 95% cis . 
we identified independent predictors of colorectal cancer incidence in a multivariable model , using backward stepwise selection with a p value less than 005 in the likelihood ratio test as the criterion for retention of variables . 
the number of surveillance visits was included as a time - varying covariate and was constrained to be included in the multivariable model . using baseline polyp and procedural risk factors identified from the multivariable model , we stratified the intermediate - risk cohort into lower - risk and higher - risk subgroups . 
we did not include age as a factor in defining the higher - risk subgroup in our study because risks of adverse events increase with age coincidental with general decline in health , and older age is associated with worse colonoscopy quality.29 , 30 we calculated expected numbers of colorectal cancers by multiplying the observed sex and 5 - year age - group - specific person - years by the corresponding incidence in the general population of england in 2007.31 we report the ratio of observed to expected cases as a standardised incidence ratio ( sir ) and 95% cis assumed an exact poisson distribution . we did all analyses with stata / ic 13.1. 
this study is registered with isrctn , number isrctn15213649 . role of the funding source the funders of the study had no role in the study design , data collection , data analysis , data interpretation , or the writing of the report . 
kw , us , and wa had full access to all the data and wa had final responsibility for the decision to submit for publication . results we identified 253 798 consecutive patients who underwent ( > 99% ) lower gastrointestinal endoscopies mostly 826 vol 18 june 2017 articles between jan 1 , 1990 , and dec 31 , 2010 . 
we excluded 223 539 patients : 174 978 with no adenomas , 45 717 with colorectal cancer or other conditions associated with increased colorectal cancer risk , 2752 with no colonoscopy , and 92 with missing procedure dates . 
of the remaining 30 259 patients with a histologically confirmed adenoma at baseline , ( 40% ) were diagnosed with intermediate - risk adenomas , of whom 51 could not be traced in national data sources and had no surveillance , leaving 11 944 patients for analysis ( figure 1 )  . 11 995 the median age of 11 944 intermediate - risk patients was 667 years ( iqr 584740 ) and 6625 ( 55% ) were men ( table 1 )  . 
a lower proportion of patients who attended at least one surveillance visit had an incomplete colonoscopy or poor bowel preparation than did patients who did not attend any visits ( table 1 )  . 
the multivariable hr and associated p value reported for sex , adenoma histology , and year of entry ( variables not included in the final multivariable model ) , were for if the variable was added as an additional variable to the final multivariable model . 
 * number of surveillance visits was included in the models as a time - varying covariate ; if a patient had any surveillance visits , they contributed person - years to more than one category of number of surveillance visits . 
no multivariable hazard ratio and p value was reported for number of adenomas because of multicollinearity with largest adenoma size ( largest size < 10 mm perfectly predicts 3 adenomas )  . table 2 : long - term colorectal cancer incidence by baseline risk factors and number of surveillance visits ( 95% ci 182238 ; table 2 )  . 
of the 5019 patients who did not attend surveillance , 2326 ( 46% ) died and 121 ( 2% ) were diagnosed with cancer , whereas of the 6925 patients who attended one or more surveillance visits , 1455 ( 21% ) died and 89 ( 1% ) were diagnosed with cancer . 
after adjustment for baseline risk factors , compared with no surveillance , one or two surveillance visits were associated with a significant reduction in colorectal cancer incidence rate ( hr 057 , 95% ci 040080 for one visit ; 051 , 031084 for two visits ) ; a similar reduction in incidence rate was seen with three or more surveillance examinations ( hr 054 , 95% ci 029099 ; table 2 )  . baseline characteristics independently associated with increased colorectal cancer incidence included older age , adenomas of 20 mm or larger , adenomas with high - grade dysplasia , polyps in the proximal colon , a colonoscopy that was incomplete or of unknown completeness , and poor quality bowel preparation ( table 2 )  . 
other baseline variables not included in the multivariable model are listed in the appendix ( p 3 )  . on the basis of the polyp and procedural characteristics identified as colorectal cancer risk factors ( but not older age ) , we divided the cohort into lower - risk ( 3079 [ 26% ] ( 8865 patients ) and higher - risk [ 74% ] ) subgroups . 
 the higher - risk subgroup consisted of patients who , at baseline , had a large adenoma ( 20 mm ) , high - grade dysplasia , proximal polyps , or a suboptimal colonoscopy . 
colorectal cancer incidence was 247 cancers per 100 000 person - years ( 95% ci 214285 ) in the higher - risk subgroup versus 93 cancers per 100 000 person - years ( 95% ci 63139 ) in the lower - risk subgroup ( table 3 )  . patients in the higher - risk subgroup were older , had entered the study earlier , and had significantly more surveillance visits than those in the lower - risk subgroup ( appendix p 4 )  . 
however , median follow - up times were similar ( 80 years [ iqr 55113 ] in the higher - risk subgroup vs 78 years [ 57106 ] in the lower - risk subgroup )  . 
among higher - risk patients , number of surveillance visits was inversely associated with colorectal cancer incidence ; by contrast , in the lower - risk subgroup , the number of surveillance visits was not associated with colorectal cancer incidence ; however , statistical power was limited because of the low number of cancers ( n = 24 in total ; table 3 )  . 
 * number of surveillance visits was included in the models as a time - varying covariate ; if a patient had any surveillance visits , they contributed person - years to more than one category of number of surveillance visits . 
the higher - risk subgroup included patients with any of the following risk factors at baseline : suboptimal quality examination ( defined as incomplete colonoscopy , unknown completeness , or poor bowel preparation ) , high - risk polyps ( defined as proximal polyps or a high - grade or large [ 20mm or larger ] adenoma ) , or both ; the lower - risk subgroup included patients without any of these risk factors . 
 table 3 : incidence of colorectal cancer and unadjusted effect of surveillance on incidence of colorectal cancer by number of visits incidence was 33% without surveillance , colorectal cancer incidence at 10 years was 27% ( 95% ci 2134 ; 114 cancers ) in the ( 2642 ; cohort overall ; 101 cancers ) in the higher - risk subgroup and 11% ( 0523 ; 13 cancers ) in the lower - risk subgroup ( table 4 )  . 
colorectal cancer incidence in the whole cohort was not significantly different from that of the general population ( sir 109 , 95% ci 091130 ) ; however , colorectal cancer incidence was significantly higher in the higher - risk subgroup ( sir 130 , 106157 ) and significantly lower in the lower - risk subgroup ( sir 051 , 029084 ) than in the general population ( table 4 ; figure 2a and b )  . after a single surveillance visit , colorectal cancer incidence at 10 years was 23% ( 95% ci 1633 ; in the cohort overall , 28% ( 1941 ; 47 cancers ) 42 cancers ) in the higher - risk subgroup , and 07% ( 0217 ; five cancers ) in the lower - risk subgroup ( table 4 )  . 
 compared with the general population , the sir for colorectal cancer was 080 ( 95% ci 059105 ) in the overall cohort , 042 ( 95% ci 016092 ) in the lower - risk subgroup , and 090 ( 95% ci 066121 ) in the higher - risk subgroup ( table 4 ; figure 2c and d )  . 
following a second surveillance visit , colorectal cancer incidence at 10 years was 20% ( 1431 ; 29 cancers ) overall and 22% ( 1534 ; 26 cancers ) in the higher - risk subgroup ; the lower - risk vol 18 june 2017 articles n 830 vol 18 june 2017 articles b higher - risk subgroup ( 95% ci ) lower - risk subgroup ( 95% ci ) higher - risk subgroup ( 95% ci ) lower - risk subgroup ( 95% ci ) time from baseline ( years ) time from baseline ( years ) number at risk 11 944 8430 4820 3079 1752 number at risk higher - risk lower - risk 8865 3079 5998 2432 3388 1432 2131 1238 95% ci 95% ci number at risk 6925 5430 2695 1429 time from rst surveillance visit ( years ) time from rst surveillance visit ( years ) number at risk higher - risk lower - risk 5257 1668 4082 1348 2056 1107 figure 2 : cumulative colorectal cancer incidence after baseline cumulative colorectal cancer incidence with no surveillance ( ie , censoring at first follow - up ) for the whole cohort ( a ) and for the risk subgroups ( b )  . 
cumulative colorectal cancer incidence after one surveillance visit ( ie , censoring at the second follow - up ) for the whole cohort ( c ) and for the risk subgroups ( d )  . 
95% cis are shown for each curve . subgroup analyses were underpowered because only three colorectal cancers had been diagnosed by 10 years ( table 4 )  . discussion in this retrospective , multicentre , cohort study , colonoscopy surveillance was associated with a substantially reduced these incidence of colorectal cancer intermediate - risk patients , who are currently offered surveillance colonoscopy at 3 - year intervals . 
the first surveillance visit seemed to confer the most benefit and was associated with a significantly reduced colorectal cancer incidence rate compared with no surveillance ; this incidence reduction was maintained in patients who attended subsequent visits . 
in the uk , about 20% of colonoscopies are done for the purpose of surveillance.21 in our dataset 80% of patients undergoing adenoma surveillance were at intermediate risk ( figure 1 ) .21 we identified a subgroup of patients at higher risk of colorectal cancer , which included roughly three - quarters of this intermediate - risk cohort . 
this subgroup consisted of patients who had a suboptimal quality colonoscopy ( incomplete , of unknown completeness , or poor bowel preparation ) , a large adenoma ( 20 mm ) , an adenoma with high - grade dysplasia , or proximal polyps detected at baseline ; surveillance was highly effective in this subgroup and was associated with a significant reduction in the incidence of colorectal cancer . 
by contrast , in patients without these baseline findings , the benefit of surveillance was unclear because only a few cancers were subsequently diagnosed . patients with intermediate - risk adenoma are offered surveillance at 3 - year intervals because they are perceived to be at increased risk of colorectal cancer compared with the general population . 
this perception is based on high detection rates of advanced neoplasia in those who attend surveillance1114 and on follow - up of patients diagnosed in the 1980s and 1990s ; 12 , 19 , 20 colorectal cancer risk has not previously been quantified by use of data in an era of higher quality colonoscopies . 
we found that colorectal cancer incidence in the absence of surveillance was similar to that expected in the general population , vol 18 june 2017 articles suggesting that intensive surveillance might not be appropriate for all intermediate - risk patients . 
however , in the higher - risk subgroup , colorectal cancer incidence without surveillance was significantly higher than that of the general population ; therefore , individuals in this subgroup might benefit from at least one surveillance visit . 
by contrast , in the lower - risk subgroup , the colorectal cancer incidence was already lower than that of the general population after baseline colonoscopy , with a 10 - year cumulative incidence of only 11% . 
this low baseline incidence raises uncertainty as to whether any surveillance is warranted for these individuals . some of the independent risk factors for colorectal cancer that we identified within this intermediate - risk group have been described as risk factors for detection of advanced neoplasia at follow - up colonoscopy , including larger adenoma size , older patient age , and having only a suboptimal quality baseline colonoscopy.1116 a less well documented risk factor was the presence of polyps in the proximal colon , which in our study was associated with an increased incidence of colorectal cancer . 
this finding corroborates data from two previous studies reporting that patients with proximal polyps had an 80% increased risk of advanced neoplasia at follow - up colonoscopy.14 , 32 this evidence suggests that proximal polyps could be regarded as a colorectal cancer risk factor in future iterations of surveillance guidelines . 
however , results from a large pooled analysis of 9167 men and women showed that body - mass index , smoking , and family history , which are often important epidemiological risk factors , are not major predictors of metachronous advanced neoplasia at surveillance after adjustment for the baseline adenoma characteristics.14 our results emphasise the importance of achieving a complete colonoscopy with good quality bowel preparation . 
since the national colonoscopy audit in 2001 , 33 there has been heightened awareness of colonoscopy standards and implementation of national quality assessments and training programmes , 21 , 34 , 35 resulting in substantial improvements in endoscopy quality and leading to nearly 30% fewer cancers arising from missed or incompletely removed lesions within 3 years of colonoscopy in 2007 than in 2001.36 patient factors , such as older age , female sex , having prior abdominal or pelvic surgery , and obesity might also affect the quality of a bowel preparation or colonoscopy.3742 in the english bowel cancer screening programme ( bcsp ) , examinations to complete an investigation of the colon and remove detected lesions are regarded as part of the initial work - up , with surveillance only considered when baseline examinations have been completed ; this would be a good policy to adopt for patients diagnosed with adenomas outside of the bcsp . 
for individuals in whom colonoscopy is problematic , the clinician should establish on a case - by - case basis whether it is appropriate to recommend colonoscopy surveillance . in our study , 42% of patients did not attend surveillance . 
other factors that we were unable to assess but which are likely to affect attendance for surveillance include the health status of the patient , administrative problems in scheduling an appointment 3 years in advance , and patient choice , especially if they had either a bad experience with the index colonoscopy or the reasons for surveillance were not well explained . the main strengths of this study are the generation of a high - quality detailed dataset by use of a large nationwide sample of routinely collected clinical endoscopy and pathology data on colonoscopies for consecutive patients with adenomas across 17 uk hospitals , which serve a combined population of more than 65 million people.23 follow - up for cancer and death was complete for almost all patients and , apart from data on bowel preparation quality , very few data were missing . 
finally , we studied incidence in a large number of patients with intermediaterisk adenomas , about 84% of whom had their baseline colonoscopy after the implementation of national quality improvement programmes beginning in 2000 . the main limitation of this study is that it is an observational study and therefore we cannot assume a causal association between surveillance and colorectal cancer incidence . 
this difference was only substantial for the bowel preparation and colonoscopy completeness variables , suggesting that when a future surveillance visit was planned , there was less of a tendency to record the quality of the initial examination . 
 a further limitation is that conclusions were based on a median of 79 years of follow - up and longer - term followup is needed to substantiate our findings , especially in the lower - risk subgroup without surveillance . 
finally , although follow - up examinations were assumed to be for surveillance , some might have been for symptomatic purposes . we conclude from our results that patients diagnosed with intermediate - risk adenomas are at only a small increased risk of developing colorectal cancer after their baseline colonoscopy and polypectomy compared with the general population , especially if they have had a good 832 vol 18 june 2017 articles quality baseline colonoscopy ; therefore , it is unclear whether all of these intermediate - risk patients need the currently recommended 3 - yearly surveillance by colonoscopy . 
among patients in the lower - risk subgroup , surveillance might not be warranted at all if baseline colonoscopy is complete , with good visibility of the bowel mucosa and all lesions completely excised . 
additionally , future research should aim to define the subgroup of intermediate - risk patients for whom the risk of colorectal cancer after first surveillance is so low that they can stop surveillance altogether . contributors wa and ik - h were responsible for trial design and organisation . 
all authors edited the paper and gave final approval on the version to be published . trial staff , collaborators , and data providers cancer screening and prevention research group staffiain stenson ( data acquisition and cleaning ) , eilidh macrae ( trial manager ) , bhavita patel ( senior data clerk ) , joanne monger ( data clerk ) , laura j turner and paula kirby ( projects managers ) , rosemary howe and elizabeth coles ( project administrators )  . trial steering committeematt rutter , chris todd , allan hackshaw , marco novelli , sue moss , and lynn faulds wood and helen watson ( patient representatives )  . participating hospitalswe are grateful to the people listed for their involvement in this project . 
royal sussex county hospital , brighton : stuart cairns * , lena king , sam goode , nigel loaring , and mark harris ; cumberland infirmary , carlisle : denis burke * , fergus young , and ian pearson ; charing cross hospital , hammersmith hospital and st marys hospital , london : paul ziprin * , geoff smith * , bola makinwa , patrizia cohen , rob goldin , david peston , and andrew hay ; glasgow royal infirmary , glasgow : john anderson * , gordon reid , and craig napier , jane hair , julie macdonell , and marion flood ; leicester general hospital , leicester : john de caestecker * , and angus mcgregor ; royal liverpool university hospital , liverpool : anthony morris * , martin lombard , steve bradburn ; institute of translational medicine , university of liverpool : michael burkitt * ; new cross hospital , wolverhampton : sarah jewes , roy cooper ; university hospital of north tees , stockton - on - tees : matt rutter * , sharron pooley , and danielle mead ; queen elizabeth hospital , woolwich , london : alistair mcnair * , matthew foxton , thelma pinto ; queen marys hospital , sidcup , kent : howard curtis * ; dartford and gravesham nhs trust , kent : guy sisson * , angela christopher , and diane gambrell ; royal shrewsbury hospital , shropshire : mark smith * ; st georges hospital , tooting , london : roger leicester * caroline finlayson ; st marks hospital , harrow , london : brian saunders , john northover , david smith ; royal surrey county hospital , surrey : john stebbing * , vanessa bollons , and tasmin patel ; torbay district general hospital , devon : mark feeney * , brett hardwell , and kirsty james ; yeovil district hospital , somerset : sue bulley * , jill burt , garry sweet , edwin cooper , and fiona wulf ; norfolk & norwich university hospital : richard tighe * and virginia sams . 
all rights reserved ; nhs central register ( nhscr ) ; and national services scotland ( nss )  . declaration of interests wa , as principal investigator , was the recipient of all of the funding . 
all other authors declare no competing interests . acknowledgments this study was fully funded by the national institute for health research ( nihr ) health technology assessment programme ( hta project number 04 / 33 / 01 )  . 
the work of the cancer screening and prevention research group ( csprg ) at imperial college is also supported by the bobby moore fund for cancer research uk ( c8171 / a16894 )  . 
we assessed whether rituximab use could delay the need for chemotherapy or radiotherapy compared with watchful waiting and the e ect of this strategy on quality of life ( qol )  . methods asymptomatic patients ( aged 18 years ) with low - tumour - burden follicular lymphoma ( grades 1 , 2 , and 3a ) were randomly assigned centrally ( 1 : 1 : 1 ) , by the minimisation approach strati ed by institution , grade , stage , and age , to watchful waiting , rituximab 375 mg / m weekly for 4 weeks ( rituximab induction ) , or rituximab induction followed by a maintenance schedule of 12 further infusions given at 2 - monthly intervals for 2 years ( maintenance rituximab )  . 
there was a signi cant di erence in the time to start of new treatment , with 46% ( 95% ci 3953 ) of patients in the watchful waiting group not needing treatment at 3 years compared with 88% ( 8392 ) in the maintenance rituximab group ( hazard ratio [ hr ] 021 , 95% ci 014031 ; p < 00001 )  . 
78% ( 95% ci 6987 ) of patients in the rituximab induction group did not need treatment at 3 years , which was signi cantly more than in the watchful waiting group ( hr 035 , 95% ci 022056 ; p < 00001 ) , but no di erent compared with the maintenance rituximab group ( 075 , 041134 ; p = 033 )  . 
compared with the watchful waiting group , patients in the maintenance rituximab group had signi cant improvements in the mental adjustment to cancer scale score ( p = 00004 ) , and illness coping style score ( p = 00012 ) between baseline and month 7 . 
 there were 18 serious adverse events reported in the rituximab groups ( four in the rituximab induction group and 14 in the maintenance rituximab group ) , 12 of which were grade 3 or 4 ( ve infections , three allergic reactions , and four cases of neutropenia ) , all of which fully resolved . interpretation rituximab monotherapy should be considered as a treatment option for patients with asymptomatic , advanced - stage , low - tumour - burden follicular lymphoma . funding cancer research uk , lymphoma research trust , lymphoma association , and roche . low - grade introduction findings from retrospective analyses of asymptomatic lymphoma patients with advanced - stage , showed no reduction in overall survival when systemic treatment was deferred until development of symptoms or organ failure , 1 , 2 which generally occurred about 30 months after diagnosis . 
these ndings were subsequently con rmed in three randomised trials.35 in the largest of these trials , 3 309 patients were randomly assigned to either watchful waiting or an intensive chlorambucil regimen . 
at a median follow - up of 16 years , there was no survival advantage to early start of treatment , and at 10 years , 19% of patients still did not need advanced - stage , chemotherapy . 
these trial data support the widely practised strategy of watch and wait in asymptomatic low - tumour - burden patients with follicular lymphoma , which is based on the assumption that the delay in exposure to chemotherapy and its attendant side - e ects would result in an improved quality of life ( qol )  . 
this assumption has not been formally assessed , and there is anecdotal evidence that in some patients this strategy can lead to a worse qol because patients nd being diagnosed with a malignant disorder without receiving treatment psychologically demanding . rituximab is a chimeric monoclonal antibody directed against cd20 . 
low tumour burden was de ned as normal lactate dehydrogenase , largest nodal or extranodal mass less than 7 cm , up to three nodal sites containing nodes with a diameter greater than 3 cm , no clinically signi cant serous e usions detectable by physical examination or ct scan , and spleen enlargement up to 16 cm by ct . this trial was overseen by an independent trial steering committee and independent data monitoring committee . 
 the protocol was approved by the uk medicines and articles of sydney , sydney , nsw , australia ( prof k bradstock phd ) correspondence to : dr kirit m ardeshna , department of haematology , university college hospital , 250 euston road , london nw1 2pg , uk kirit.ardeshna@uclh.nhs.uk for the trial protocol see trialprotocols.aspx 484 patients enrolled 21 excluded 8 reasons unknown 7 not eligible 1 stage 1 disease 5 high tumour burden 1 reason not stated 3 physician started treatment 1 second malignancy discovered 1 consent withdrawn 1 diagnosis revised to mantle - cell lymphoma 463 patients randomly assigned 187 patients assigned to watch and wait * 84 patients assigned to rituximab induction 192 patients assigned to maintenance rituximab * 2 stopped early because of toxicity 1 missing information 1 missing information 81 received four infusions 191 received four induction infusions 36 stopped early 156 received 12 maintenance infusions 187 included in intention - to - treat population 84 included in intention - to - treat population 192 included in intention - to - treat population figure 1 : trial pro le on sept 30 , 2007 , recruitment into the rituximab induction group was closed and the study was amended to a two - arm study . 
 * inclusive of the patients enrolled in the three - arm study ( 83 in the watch and wait group and 85 in the maintenance rituximab group )  . vol 15 april 2014 articles healthcare products regulatory agency and cambridge south research ethics committee , and was done in accordance with the declaration of helsinki and the eu clinical trials directive . 
all patients provided written informed consent before enrolment . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to be carefully observed until treatment was needed ( watchful waiting ) , to receive rituximab induction , or to receive maintenance rituximab . 
some percentages do not total 100% because of rounding . table 1 : demographics and baseline characteristics procedures patients randomly assigned to the rituximab induction group received intravenous rituximab ( 375 mg / m ) every week for 4 weeks ( rituximab induction ) , while those in the maintenance rituximab group received the same rituximab induction followed by 12 infusions of rituximab given at 2 - monthly intervals for 2 years . 
no dose reductions were recommended . clinical assessments including full blood count and renal and liver function tests were done at baseline , 1 month , and then every 2 months for 2 years or until start of treatment . 
a bone marrow trephine biopsy was taken for restaging only if patients were in complete remission or uncon rmed complete remission on radiological assessment at month 7 , 13 , or 25 , or before starting rst chemotherapy or radiotherapy . safety data were collected while patients in the rituximab induction and maintenance groups were on treatment with rituximab and for up to 30 days afterwards unless a late complication of rituximab was reported . qol was assessed at baseline ( before randomisation ) , after randomisation ( within 1 week and before treatment ) , at each clinic visit during the rst 2 years , and then every 6 months for 2 years . 
the questionnaires used were the functional assessment of cancer therapygeneral ( fact - g ) , hospital anxiety and depression scale ( hads ) , impact of event scalerevised , and questions from the illness coping style , illness impact bank , and mental adjustment to cancer scale together with four additional questions relating to lymphoma ( appendix )  . and scales summary subscales or emotional wellbeing , for each qol questionnaire were derived according to their score manuals . 
there are four subscales of the fact - g questionnaire : physical wellbeing , social or family wellbeing , functional wellbeing , each scored 0100 , with higher scores suggesting better qol . 
the hads is summarised by anxiety and depression subscales , which are classi ed as normal ( score 07 ) , borderline ( score 810 ) , and case ( score 1114 )  . 
there are 27 items in the impact of event scalerevised questionnaire , which are summarised as avoidance , intrusions , and hyperarousal subscales ; scores of all subscales are scaled as 0100 , with higher scores suggesting better qol . 
one summary measure each is derived from the illness coping style , the illness impact bank , and the mental adjustment to cancer 426 vol 15 april 2014 articles scale questionnaires ; scores of each are scaled as 0100 , with higher scores suggesting better qol . outcomes the primary outcome measures were the time to start of new treatment and qol at month 7 ( 6 months after completion of induction treatment )  . 
progression - free survival and time to histological transformation were analysed post hoc . time to start of new treatment was calculated from the date of randomisation to the date of starting new systemic chemotherapy or radiotherapy . 
 we recognised that de ning clearly when disease progression is su cient to warrant the start of chemotherapy or radiotherapy is di cult and so we provided a detailed guidance ( appendix )  . 
standard criteria for response assess ment were used.8 survival was de ned as time from random isation to death from any cause ( overall survival ) or progression or death from any cause ( progression - free survival )  . 
 statistical analysis with an estimated median time to start of new treatment of 30 months in the watchful waiting arm , the original three - arm trial was designed to detect an improvement in the median time to start of new treatment in each of the rituximab groups of 18 months ( from 30 to 48 months ) with a 25% signi cance level ( allowing for the multiple comparisons ) and 90% power . 
recruitment of 600 patients was planned . on sept 30 , 2007 , about 3 years after the start of enrolment , recruitment into the rituximab induction group was closed because of a low recruitment rate and because other studies had shown a bene t of maintenance rituximab compared with watchful waiting after induction with rituximab with or without chemotherapy , 9 , 10 although in only one of these studies was the rituximab induction administered as a monotherapy . 
this change was approved by the independent trial steering committee , independent data monitoring committee , and regulatory and ethics committees . for the two - arm trial , the study was redesigned to detect an improvement in the median time to start of new treatment in the maintenance rituximab arm of 18 months ( from 30 to 48 months ) with a 5% signi cance level and 90% power . 
recruitment of 360 patients was planned . the primary analysis was done using an unstrati ed log - rank test for the di erence in the distribution of time to start of new treatment between the di erent groups . 
interaction analyses were done to assess the di erence in the size of treatment e ects in subgroups classi ed according to age , sex , stage , follicular lymphoma international prognostic index , 11 and 2 microglobulin concentration . 
however , on march 26 , 2010 , the independent data monitoring committee concluded that the data regarding the clinical primary outcome measure were mature and suitable for full analysis and publication . 
this decision was approved by the independent trial steering committee . watch and wait overall remission spontaneous complete remission spontaneous partial remission uncon rmed complete response no change disease progression rituximab induction overall response complete response partial response no change disease progression maintenance rituximab overall response complete response partial response no change disease progression data are n / n ( % )  . 
 the change in qol from baseline to month 7 within each arm was also compared between the arms and this was judged to be the most important comparison . except for anxiety or depression subscales , a change of 5 points for a subscale was regarded as the minimum clinically signi cant di erence . 
statistical analyses were done using sas version 9.2. this study is registered with clinicaltrials.gov , nct00112931 , and eudract , 2004 - 001621 - 16 . role of the funding source the trial sponsor ( university college london ) was responsible for randomisation , data collection , entry , and validation ; monitoring procedures ; reporting of serious adverse events ; organisation of central pathological review ; liaison with investigators ; data analysis ; and writing of the report . 
roche , the lymphoma association , and the lymphoma research trust had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between oct 15 , 2004 , and march 25 , 2009 , 463 patients were randomly assigned from 118 centres in the uk , australia , new zealand , turkey , and poland . 
252 patients were randomly assigned in the original three - arm study ( 83 to the watchful waiting group , 84 to the rituximab induction group , and 85 to the maintenance rituximab group )  . 
in the two - arm study , 379 patients were randomly assigned between the watchful waiting group ( n = 187 ) and the maintenance rituximab group ( n = 192 ; gure 1 )  . 
 a time to start of new treatment b progression - free survival watch and wait maintenance rituximab hr 021 ( 95% ci 014031 ) log - rank p < 00001 number at risk watch and wait maintenance rituximab hr 023 ( 95% ci 016032 ) log - rank p < 00001 c overall survival d time to histological transformation hr 073 ( 95% ci 034154 ) log - rank p = 040 number at risk watch and wait maintenance rituximab hr 062 ( 95% ci 031126 ) log - rank p = 019 years from randomisation years from randomisation figure 2 : kaplan - meier curves for the two - arm study ( a ) time to start of new treatment , ( b ) progression - free survival , ( c ) overall survival , and ( d ) time to histological transformation . 
 428 vol 15 april 2014 articles a time to start of new treatment b progression - free survival watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 035 ( 95% ci 022056 ) ; log - rank p < 00001 maintenance rituximab vs rituximab induction hr 075 ( 95% ci 041134 ) ; log - rank p = 033 number at risk watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 055 ( 95% ci 037083 ) ; log - rank p = 00034 maintenance rituximab vs rituximab induction hr 053 ( 95% ci 032087 ) ; log - rank p = 0011 c overall survival d time to histological transformation rituximab induction vs watch and wait hr 104 ( 95% ci 039280 ) ; log - rank p = 093 maintenance rituximab vs rituximab induction hr 112 ( 95% ci 043290 ) ; log - rank p = 082 years from randomisation number at risk watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 034 ( 95% ci 011106 ) ; log - rank p = 0052 maintenance rituximab vs rituximab induction hr 147 ( 95% ci 042522 ) ; log - rank p = 055 years from randomisation figure 3 : kaplan - meier curves for the 252 patients randomly assigned in the initial three - arm study ( a ) time to start of new treatment , ( b ) progression - free survival , ( c ) overall survival , and ( d ) time to histological transformation . 
 the 4 - week rituximab induction was administered to all patients except for two patients in the rituximab induction group who only received one and three infusions , respectively , because of toxicity . 
 maintenance was stopped because of progressive disease or new treatment ( n = 13 ) ; other illness taking priority or resulting in death ( n = 5 ) ; infection ( n = 3 ) ; patient choice ( n = 6 ) ; reclassi cation as di use large b - cell lymphoma ( n = 1 ) ; neutropenia ( n = 3 ) ; or uncertain reasons ( n = 2 )  . 
there were no dose reductions . 18 serious adverse events occurred in the two rituximabcontaining groups , which were considered possibly , probably , or de nitely related to the rituximab : nine infections ( induction group n = 1 , maintenance group n = 8 ) , ve allergies ( induction group n = 3 , maintenance group n = 2 ) , and four neutropenia ( all in the maintenance group )  . 
there were ve grade 3 infections in the maintenance rituximab group ( two pneumonia , one viral meningitis , one de - novo hepatitis b infection , and one urinary tract infection )  . 
 vol 15 april 2014 articles the fourth patient developed grade 3 neutropenic sepsis 5 months after randomisation and was treated with antibiotics and granulocyte colony - stimulating factor and the rituximab was stopped . 
there were no other grade 3 or 4 adverse events . the rate of spontaneous remissions in the watchful waiting group was low : by month 25 , only 15 ( 12% ) of 128 patients had shown radiological regressions over 50% ( ie , overall remission ) , with only eight ( 6% ) patients having a spontaneous complete remission or uncon rmed spontaneous complete remission . 
162 ( 88% ) of 184 patients in the maintenance rituximab group had had a response at 7 months , as had 144 ( 83% ) of 173 at 25 months . 
 radiologically identi ed complete responses , or un conrmed complete responses , were noted in 109 ( 59% ) of 184 patients at month 7 and in 130 ( 75% ) of 173 patients at month25 ( table 2 )  . analysis of the 252 patients recruited to the three - arm study showed that there were signi cantly more overall responses in the maintenance rituximab group than in the rituximab induction group at both month 7 ( 77 / 85 [ 91% ] vs 62 / 81 [ 77% ] ; p = 0043 ) and month 25 ( 67 / 80 [ 84% ] vs 43 / 75 [ 57% ] ; p = 0001 ; appendix )  . 
 investigator compliance with bone marrow examination when a radiological complete remission or uncon rmed complete remission was achieved was suboptimum ; incorporation of these ndings underestimated rates of complete remission or uncon rmed complete remission ( appendix )  . 
 in the two - arm study , 105 ( 56% ) of 187 patients in the watchful waiting group and 33 ( 17% ) of 192 patients in the maintenance rituximab group needed new treatment ; the reason for starting new treatment was disease progression except for six ( 4% ) patients ( three watch and wait ( n = 187 ) rituximab induction ( n = 84 ) maintenance rituximab ( n = 192 ) total breast lung colorectal squamous cell stomach prostate basal - cell carcinoma melanoma pancreas unknown primary hodgkins lymphoma total table 3 : list of second malignancies patient choice in the watchful waiting group , one clinician choice in the watchful waiting group , and one in each group reclassi ed as di use large b - cell lymphoma )  . 
 the estimated median time to start of new treatment was 311 months ( 95% ci 255460 ) in the watchful waiting group and has not been reached in the maintenance rituximab group . 
at 3 years , the estimated percentage of patients not needing new treatment was 46% ( 95% ci 3953 ) in the watchful waiting group , and 88% ( 8392 ) in the maintenance rituximab group ( hr 021 , 95% ci 014031 ; p < 00001 ; gure 2a )  . 
all prespeci ed patient subgroups showed prolongation of time to start of new treatment with maintenance rituximab . in the three - arm study , 97 of 252 patients randomly assigned into the three - arm study needed to start new treatment : 52 ( 63% ) of 83 in the watchful waiting group , 25 ( 30% ) of 84 in the rituximab induction group , and 20 ( 24% ) of 85 in the maintenance rituximab group . 
for patients randomly assigned to the rituximab induction group , the median time to start of new treatment has not been reached and new treatment had not been started in 78% ( 95% ci 6987 ) of patients at 3 years . 
the hr was 035 ( 95% ci 022056 ; p < 00001 ) for rituximab induction versus watchful waiting and was 075 ( 041134 ; p = 033 ) for maintenance rituximab versus rituximab induction ( gure 3a )  . 
exploratory analyses of patient subgroups are summarised in the appendix . in the two - arm study , 121 ( 65% ) of 187 patients in the watchful waiting group and 43 ( 22% ) of 192 patients in the maintenance rituximab group had either developed progressive disease or died . 
median progression - free survival was 241 months ( 95% ci 171253 ) in the watchful waiting group , but has not yet been reached in the maintenance rituximab group . 
3 - year progression - free survival was 36% ( 95% ci 2943 ) in the watchful waiting group and 82% ( 7788 ) in the maintenance rituximab group ( hr 023 , 95% ci 016032 ; p < 00001 ; gure 2b )  . in the three - arm study , 41 ( 49% ) of 84 patients in the rituximab induction group had either developed progressive disease or died . 
3 - year progression - free survival was 60% ( 95% ci 4971 ) in the rituximab induction group , which was signi cantly di erent from the other two arms : hr 053 ( 95% ci 032087 ; p = 0011 ) for the comparison between maintenance rituximab and rituximab induction and hr 055 ( 037083 ; p = 00034 ) for the comparison between rituximab induction and watchful waiting ( gure 3b ; appendix )  . in the two - arm study , 28 ( 7% ) of 379 patients had died : 16 ( 9% ) of 187 in the watchful waiting group and 12 ( 6% ) of 192 in the maintenance rituximab group . 
eight patients died in the rituximab induction group , giving a 3 - year overall survival of 96% ( 95% ci 92100 ) , with no di erence between the three groups ( gure 3c ; appendix )  . 
six second malignancies occurred in the rituximab induction group , two were fatal ( table 3 )  . by data cuto ( sept 8 , 2012 ) , 33 patients had had biopsy - proven transformation in the two - arm study ( 20 [ 11% ] of 187 in the watchful waiting group and 13 [ 7% ] of 192 in the maintenance rituximab group )  . 
a further four patients have had biopsyproven transformation in the rituximab induction group , with no evidence of di erences between the rituximab group and the other groups in the three - arm study ( gure 3d ; appendix )  . time table 4 summarises the qol results for the two - arm study at month 7 . 
there was a signi cant improvement in the mental adjustment to cancer scale score from baseline to month 7 in the maintenance rituximab group ( p = 00001 ) that did not occur in the watchful waiting group ( p = 019 )  . 
compared with baseline , scores at month 7 for the illness coping style were much the same in the maintenance rituximab group ( p = 0072 ) and deteriorated in the watchful waiting group ( p = 00063 )  . 
 patients in the maintenance rituximab group were also signi cantly less worried about the need for treatment or more treatment than patients in the watchful waiting group by month 7 compared with baseline ( p = 00037 )  . 
 there were no other clinically signi cant di erences between the two arms in all other qol measures between baseline and month 7 ; all measures either improved or remained unchanged between baseline and month 7 ( table 4 )  . this di erence was signi cant in the three - arm study , there was no evidence of di erence in qol between baseline and month 7 when the rituximab induction group was compared with the watchful waiting group . 
in accordance with these data , more patients in the watchful waiting group had started new treatment compared with those in the rituximab induction group , and also compared with those in the maintenance rituximab group . 
the nding that the administration of rituximab delayed progression and time to start of new treatment is not surprising , but the magnitude of remarkable , with more than three times fewer patients needing treatment by 3 years in the maintenance rituximab group than in the watchful waiting group . 
the di erence between the time to start of new treatment in the rituximab induction and maintenance groups was not signi cant , but the start of new treatment lags behind progression and once the trial was amended to two arms , the trial was underpowered for the comparison of the two rituximab groups . this e ect longer follow - up is needed to ascertain the median time to progression and time until new treatment becomes necessary in the rituximab - containing groups , but three other studies are relevant to this issue . 
colombat and colleagues6 updated the results of their phase 2 study in patients with previously untreated low - tumour - burden follicular lymphoma who received infusions of rituximab induction without maintenance every 4 weeks . 
in the sakk 35 / 98 study , 9 , 10 standard rituximab induction was administered and patients were randomly assigned to observation or four further doses of rituximab given at 2 - monthly intervals . 
in the subgroup of previously untreated patients ( not all asymptomatic or with low tumour burden ) who responded to induction , 22% remained event free without maintenance at 8 years compared with 45% in the maintenance group . 
similarly , in the resort study , 12 the proportion of patients remaining free of cytotoxic treatment at 3 years was signi cantly greater receiving extended maintenance rituximab than in those receiving rituximab re - treatment upon progression . those in the present study , we chose time to start of new treatment rather than progression - free survival as the primary endpoint . 
we acknowledge that there is some subjectivity as to when treatment is needed , even when guidance is provided , but oncologists are familiar with making this decision in routine clinical practice and this pragmatic endpoint is of greatest relevance to the patient . 
 the de nition of progression covers a wide spectrum of clinical scenarios , some of which would not warrant the start of treatmenteg , the appearance of a new small nodethus reducing its utility in patients with indolent lymphoma . 
 * worsened or stayed as very much , quite a bit , or somewhat . table 4 : quality of life at baseline and month 7 from randomisation duration after rst new treatment as well as time to second new treatment . 
preliminary data from the us lymphocare study14 suggest that the time to second systemic treatment is signi cantly longer in patients who received rituximab monotherapy than in those who were initially on watchful waiting . 
the estimated 5 - year overall survival in the watchful waiting arm in the present study is over 90% , which compares favourably with the 58% in our previous study.35 this di erence , in the space of fewer than two decades , is substantial and probably due in baseline patient characteristics between the two studies and newer treatment options that have become available . 
for example , in our initial study , bulk disease per se was not an exclusion criterion , there was no requirement for a to di erences treatment in the watchful waiting group was very close to that reported in previous studies1 , 35 further shows the reproducibility of this endpoint . findings from this trial also show that rituximab induction can be delivered without a reduction in qol : patients receiving maintenance rituximab actually had an improvement in some aspects of their qol when compared with those on watchful waiting . 
at month 7 , patients in the maintenance rituximab group were signi cantly more likely to feel in control of their situation than those in the rituximab induction group and the watchful waiting group , as shown by the mental adjustment to cancer scores . 
conversely , patients in the watchful waiting group were signi cantly more likely to avoid learning or thinking about their illness and to have unpleasant connotations with their clinic visits , as shown by the illness coping style scores , and to be worrying about the need for treatment than those in the maintenance rituximab group . 
therefore , the administration of rituximab does not seem to negatively a ect patients qol and patients who receive a maintenance schedule seem to feel more empowered and better adjusted to their diagnosis . 
this nding might be because these patients felt that something active was being done to combat their lymphoma , and many of them would have noticed physical evidence such as lymph nodes shrinking to suggest that this was the case . rituximab monotherapy seems to be well tolerated , with only eight cases of grade 3 infection or allergy . 
this nding might be a result of the fact that patients included in the study were well at the outset , had low tumour burden , and had not received treatment previously . 
follow - up is short so far and long - term sequelae of rituximab might appear ; however , rituximab has been in use for 15 years and the follow - up of patients treated in other trials with rituximab is extensive . so far there is no overall survival di erence between the three groups , and much longer follow - up will be needed to assess the e ect of this strategy on overall survival . 
we have extended the follow - up of this study to collect information regarding response and response vol 15 april 2014 articles panel : research in context systematic review we searched pubmed from january , 1987 , until august , 2013 , for randomised trials published in english with the terms lymphoma and watchful waiting or observation or delayed treatment . 
we found three randomised studies , 35 each of which showed no survival bene t when systemic treatment was started immediately in patients with advanced - stage asymptomatic low - tumourburden low - grade lymphoma compared with a watchful waiting approach in which treatment was deferred until disease progression . 
there were no other studies comparing watchful waiting with the administration of rituximab monotherapy in this patient group . interpretation in this study , we show that rituximab monotherapy is e ective at deferring disease progression and the need for chemotherapy or radiotherapy in patients with asymptomatic low - tumour - burden follicular lymphoma , and when administered as a maintenance schedule it can be delivered with minimum toxicity and results in improved quality of life compared with watchful waiting . 
however , probably the most important reason for the improvement in overall survival is the routine therapeutic use of monoclonal antibodies . with a median follow - up of nearly 4 years , there was no di erence in the incidence of histological transformation between the three groups . 
previous retrospective studies have di ered as to whether a watchful waiting approach increased the risk of transformation ; that a di erence will emerge is not inconceivable and further follow - up is clearly necessary.15 , 16 we found that maintenance rituximab compared with rituximab induction had a numerically greater e ect on time to initiation of new treatment in women than in men . 
although the heterogeneity of to sex was not signi cant , response with regard gisselbrecht and colleagues17 also found that maintenance rituximab improved overall survival when compared with observation in women , but not in men , when administered after autologous stem - cell transplantation for relapsed refractory di use large b - cell lymphoma . 
the reason for this nding is unclear , but might relate to the di erential clearance of rituximab from the serum between the sexes.18 management options for patients with low - tumourlymphoma burden are varied and include watchful waiting , immediate asymptomatic follicular that rituximab time . 
in this study we show induction alone can delay chemotherapy and is not signi cantly less e ective than a m aintenance schedule ; however , the number of responses was lower and the rate of progression after induction alone was signi cantly higher than that after maintenance . 
thus , a di erence in time to start of new treatment will probably emerge between these two the cost approaches with associated with the administration of maintenance rituximab over 2 years and that the use of rituximab induction alone was attractive in terms of reduced number of hospital visits for administration of rituximab and cost , but the improvements in qol that occurred with the maintenance schedule did not occur for rituximab induction alone . 
this absence in improvement of qol might have been because the amended study was not powered su ciently to show a qol di erence between the rituximab induction group and the watchful waiting group . 
however , despite this factor , patients receiving maintenance rituximab still had a signi cant improvement in their mental adjustment to cancer score between baseline and month 7 compared with those receiving rituximab induction alone , suggesting a qol bene t of the maintenance approach between randomisation and month 7 . watchful waiting might still be appropriate for some patients . 
we have previously shown that 40% of patients over 70 years of age will never need any treatment and will not die of their lymphoma ; 3 however , this nding must be balanced against the improved qol achieved with maintenance rituximab . 
 furthermore , by administering rituximab to the whole group of patients older than 70 years , an even larger cohort might never need chemotherapy , which would be advantageous in view of the comorbidities and the reduced ability to withstand the side - e ects of treatment in this age group . 
if watchful waiting is used , clinicians will need to be alert to whether the patient is anxious that no treatment is experiencing feelings of is being administered , helplessness , or is having di culty adjusting to their diagnosis . 
if these are substantial concerns then the treatment approach should be reconsidered . in conclusion , our results suggest that rituximab monotherapy should be regarded as a standard approach in the management of many patients with asymptomatic , low - tumour - burden follicular lymphoma . 
the full results of other studies that address the optimum schedule of rituximab monotherapy administration , such as the resort study , 12 are awaited with interest . 434 vol 15 april 2014 articles contributors kma and dcl designed the study , interpreted data , and wrote and approved the report . 
all authors have reviewed and approved the nal version of the report . declaration of interests kma has received funding from roche for being an advisory board member , speaker , and data manager , and for travel and accommodation at international conferences . 
dcl has been chair of an oversight committee for cellmedica , adviser for cellectsis , an advisory board member and speaker for roche and chugai , and an advisory board member for millenniuwq , ps , nb , ll , pp , jwar , ls , fm , rs , bf , and kb declare that they have no competing interests . acknowledgments roche provided rituximab free of charge . 
dc recieves funding from the national institute for health research biomedical centre at the royal marsden hospital . editorial for the chief medical o cer annual report , volume 2 see category / publications / reportspublications / for information on antimicrobial resistance from the who see int / drugresistance / en / cancer treatment and antimicrobial resistance on march 11 , 2013 , englands chief medical o cer ( cmo ) , prof dame sally davies , published the second volume of her annual report . 
the focus of this publication was the growing threat of antimicrobial resistance , and came with a stark warning about the potential apocalyptic scenario that could arise if steps are not taken now to prevent widespread resistance . 
 additionally , in a world of antimicrobial resistance , techniques such as bone marrow transplantation would bring risk not only to cancer patients , but also to bone marrow donors . 
davies makes seventeen speci c recommendations in her report and calls for antimicrobial resistance to be added to the uk national security risk assessment register and for the implementation of a cross - government antimicrobial strategy , which will champion the responsible use of antibiotics , strengthen surveillance , and encourage development of new diagnostics , therapeutics , and antibiotics . resistance as highlighted in the cmo report and by who , it is not enough for individual countries to take measures ; there needs to be a global e ort to combat this problem , to improve monitoring of outbreaks , and to prevent the inappropriate use of antibiotics . 
in many developing countries , antibiotics are available over - the - counter and individuals are able to self - medicate , often taking the drugs inappropriately , either as an incorrect dose or to treat a non - bacterial ailment . 
 even in the uk , which should have adequate resources for disease diagnosis and access to the appropriate drugs , there remains substantial variation in prescription of antibiotics , both clinically and geographically . 
davies highlights the need for biomarkers to guide antibiotic prescriptions , with the aim to target therapy , rather than use broad - spectrum antibiotics , which can contribute to resistance . besides the use of antibiotics in a medical setting leading to antimicrobial resistance , there are also concerns over antimicrobial use in agriculture and household products . 
although there are tight regulations over use of antibiotics in food production in europe , in many other countries the use of antibiotics in agriculture far exceeds that used in medicine . 
the recent increase in marketing antibacterial soaps and gels to consumers has also raised debate , particularly as there is very little , if any , evidence of there being any health bene t . 
steps are being taken to combat this ; recently the european commission did not approve an application for the addition of triclosan to plastics for food packaging , and the safety of this drug in household products is currently under review by regulators in canada . 
greater regulation should be put in place for use of antimicrobials in agriculture and consumer products , and better education of the public on actual risks and bene ts would go a long way to removing these potential sources of antimicrobial resistance . the spread of antimicrobial antimicrobial drugs are a unique class of medicines because they are prescribed by all doctors , not just those who specialise in infectious diseases . 
the provision of cancer care has traditionally been multidisciplinary in nature , and it would not be di cult to incorporate an additional voice to the tea after all the gains that have been made in recent years to improve survival outcomes for patients with cancer through targeted therapies , better surgical techniques , and improved radiotherapy , we must now work to ensure that infection will not once again become the killer it was a century ago . 
 the lancet oncology vol 14 april 2013 corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 corrections published online december 21 , 2016 s1470 - 2045 ( 16 ) 30686 - 6 correction to lancet oncol 2017 ; 18 : 205 , 206 , 208 , ( d ) low jg , berglund a , schell mj , scott et al . 
in gure 1 , the footnote should have read pie charts show dose assignments for patients in gard score groups : ( b ) high ( 8941100 percentile ) ; ( c ) middle ( 3041894 percentile ) ; and ( 0304 percentile )  . 
in the second paragraph of the results , the third sentence should have read however , although 1456 ( 58% ) of 2517 patients assigned to 45 gy were in the low gard group , 1023 ( 21% ) of 4877 patients in the middle gard group and 38 ( 4% ) of 887 patients in the high gard group were assigned to 45 gy ( gure 1 )  . 
the fth sentence in this paragraph should have read similarly , although most patients assigned to 70 gy were in the high gard group , 588 ( 11% ) of 4877 patients in the middle gard group were assigned to 70 gy ( gure 1 )  . 
in the fth paragraph of the discussion , the start of the eighth sentence should have read : finally , while we use the gene - expressionbased a backbone for our analyses , the calculation of gard could use other measures of radiosensitivity or be expanded to include other biological parameters including hypoxia , dna repair , proliferation , and the immune systethese corrections were made to the online version as of dec 21 , 2016 , and printed article is correct . radiosensitivity index vol 18 february 2017 * krzysztof bujko , rafa sopyo i department of radiotherapy ( kb ) and department of surgery ( rs ) , m skodowska - curie memorial cancer centre , 02 781 warsaw , poland ( kb ) bujko@coi.waw.pl we declare no competing interests . ngan sy , burmeister b , fisher rj , et al . 
randomized trial of short - course radiotherapy versus long - course chemoradiation comparing rates of local recurrence in patients with t3 rectal cancer : trans - tasman radiation oncology group trial 01.04. 
effect of interval ( 7 or 11 weeks ) between neoadjuvant radiochemotherapy and surgery on complete pathologic response in rectal cancer : a multicenter , randomized , controlled trial ( greccar - 6 )  . 
 although this advice seems reasonable , the stockholm iii trial does not support this because 30 - day and 90 - day postoperative mortality was not decreased after delaying surgery ; 3 , 5 however , only a fourth of patients in this trial were older than 75 years . 
 one small prospective trial reported acute toxicity in 27% of patients in the short - course radiotherapy with delayed surgery group and in 64% of patients in the chemoradiation group ( p = 0001 ) .8 other trials investigating short - course radiotherapy with delayed surgery also reported lower frequencies of acute radiation toxicity compared with that usually observed after chemoradiation.3 , 6 , 9 of note , about 1% mortality due to chemoradiation toxicity has usually been reported , whereas to our knowledge , no mortality attributed to short - course radiotherapy has ever been described . 
simple digital rectal examination became the sole method for the assessment of response among these patients 276 vol 18 march 2017 comment without the requirement for complex , elaborate , or expensive studies to rule out the presence of microscopic disease . 
despite the inherent differences between anal and rectal cancers , this approach was considered years later to be applicable to patients with very distal rectal adenocarcinomas that had a complete clinical response after being treated with a chemoradiotherapy regimen similar to that used for anal cancer.4 however , nigros original findings and observational treatment approach endured slower acceptance in the clinical rectal oncology community . 
 these rectal cancers are located centimetres away from the anus and have been only recently more widely considered for an organ - preserving strategy without immediate radical surgery after a complete clinical response.5 , 6 the understanding of in the lancet oncology , robert glynne - jones important and colleagues , 7 , 8 provide an additional contribution in - vivo kinetics of anal tumour response to neoadjuvant chemoradiotherapy . 
the observation that the ideal interval to assess tumour response is 26 weeks is remarkable and a leap forward in clinical practice for the management of these patients , especially considering that this interval was formerly only 8 weeks.9 besides the issue of timing of assessment , the present study draws attention to a very interesting observation . 
 not only were patients unharmed by rather long periods of time without a definitive conclusion ( complete versus incomplete response ) , but were not prematurely given unnecessary surgical resection . 
ultimately , the inherent subjectivity of clinical response assessment and the variation in examiners and specific tools for assessment of response incorrectly might have accounted for some complete clinical responses being incomplete clinical response in the early intervals . 
furthermore , these results and the kinetics of tumour regression after neoadjuvant chemoradiotherapy and the accuracy of clinical assessment might not be unique to anal carcinoma and might again apply , at least to some extent , to rectal adenocarcinoma after neoadjuvant chemoradiotherapy . 
 * angelita habr - gama , guilherme pagin so julio , rodrigo oliva perez colorectal surgery division , university of so paulo , so paulo , brazil ( ah - g ) ; and gastroenterology department , angelita and joaquim gama institute , so paulo 04001 - 005 , brazil ( ah - g , gpsj , rop ) we declare no competing interests . the author ( s )  . 
 int j radiat oncol biol phys 2003 ; 56 : 125973 . vol 18 march 2017 comment correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections corrections correction to lancet oncol 2013 ; 14 : 84 correction to lancet oncol 2013 ; 14 : 99 schutz fab , pomerantz mm , gray kp , et al . 
lancet oncol 2013 ; 14 : 8187in the key and the number at risk rows in the gure ( page 84 ) , aa or gg should have read aa or ag . 
bevacizumab in breast cancer : fundamental questions rema lancet oncol 2013 ; 14 : 99101in this comment , the third sentence the second paragraph should have read the investigators chose a non - inferiority study design with a boundary of 133 for hazard ratio ( hr ) survivalie , an increased risk of death of 33% or less over the duration of the study for the capecitabine - containing regimen would be regarded as non - inferior . 
 this correction has been made as of feb 25 , 2013 . for overall vol 14 march 2013 corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections for more on human mismanagement of the planet see the lancet planetary health journals / lanplh / issue / current for more on developments in us air pollution policies see editorial lancet resp med 2017 ; 5 : 361 for the global burden of disease attributable to ambient air pollution see articles lancet 2017 ; published online april 10 . 
this years annual meeting of the american association for cancer research ( aacr ) in washington , dc , usa ( april 15 , 2017 ) was no exception , and last years meeting saw the launch of the ambitious cancer moonshot programme , which laid out plans to accelerate two - fold the transition of genetic and immunological findings from laboratories to the clinica goal formally recognised when the us senate approved dedicated funding via the 21st century cures act . 
but can this insatiable desire to enhance our fundamental understanding of tumour biology overshadow the health gains that could be secured by improved environmental protection ? many genetic loci associated with increased risk of developing cancer have been discovered , and some can lead to preventive actions . 
 on march 14 , 2017 , the us department of veteran affairs amended a ruling regarding payments to army personnel who had resided at marine corps base camp lejeune ( jacksonville , nc , usa ) for 30 days or longer between aug 1 , 1953 , and dec 31 , 1987all veterans , former reservists , and former national guard members who had been stationed there during this time , and had subsequently been diagnosed with one of several types of cancer , would be entitled to veteran disability benefits . 
 the allowance was made because those who had served at the camp , and their families , had spent the duration of their stay drinking and bathing in water contaminated with an estimated 70 organic volatile compounds known to be carcinogenic . 
since the town changed its water supply in april , 2014 , from lake huron to the flint river , residents noted that their tapwater had become yellow and cloudy . 
after declaring an emergency and enlisting the help of the national guard in 2016 , flint river water was re - declared as unsafe , and work began on replacing lead - contaminated pipes . 
 the consequences of 3 years worth of exposure to lead - contaminated water for flints residentsand especially their growing childrenare unknown , but in view of leads classification as probably carcinogenic to humans in a recent iarc monograph , they are likely to be at an increased risk of developing cancer in the future . 
in view of the precedent set by camp lejeune , where the total settlement has now reached around us$2 billion , this incident will plague and cost residents and regulators alike for decades to come . 
such incidents of neglect inevitably occur elsewhere too : a british water utility company , thames water , was fined a record 203 million on march 22 , 2017 , for a series of leaks of untreated sewage during 201314 into the river thames ( which indirectly supplies londons drinking water ) , its tributaries , and the adjacent land . 
and , contaminated water supplies in china have been long documented . a large - scale economic inefficiency clearly exists , with financial resources being divided into both the science of cancer prevention and also into efforts to help those who have developed cancer as a direct result of human mismanagement of the planet . 
 paradoxically , recent moves by the us government to reduce the funding of the environmental protection agency , to increase coal production , and to review corporate average fuel economy standards will probably increase the populations exposure to carcinogenic pollutants , while at the same time the moonshot programme aims to counter the adverse consequences . 
 outside the usa , the european commission issued a final warning to the uk on feb 15 , 2017 , regarding its repeated breaches of legal air pollution limits , and globally , 42 million deaths in 2015 have been attributed to ambient particulate matter . 
to eradicate cancer , governments need to both identify and act not only on increased risk susceptibility , but also ensure that people are not exposed to carcinogenic materials through gross environmental mismanagement . 
 the lancet oncology vol 18 may 2017 editorial articles the sex hormone system in carriers of brca1 / 2 mutations : a case - control study martin widschwendter * , adam n rosenthal * , sue philpott , ivana rizzuto , lindsay fraser , jane hayward , maria p intermaggio , christopher k edlund , susan j ramus , simon a gayther , louis dubeau , evangelia ourania fourkala , alexey zaikin , usha menon , ian j jacobs summary background penetrance for breast cancer , ovarian cancer , or both in carriers of brca1 / brca2 mutations is disproportionately high . 
 follicular and luteal oestradiol and progesterone serum titres were grouped into quartiles and odds ratios were calculated with logistic regression . findings follicular phase endometrial thickness of carriers of the mutations adjusted for age and day of the menstrual cycle was higher ( odds ratio [ or ] 111 , 95% ci 103120 ; p = 00063 ) and luteal phase endometrial thickness lower ( 090 , 083098 ; p = 0027 ) than for women negative for the mutations . 
median luteal phase titres of progesterone were 121% higher ( p = 000037 ) in carriers than in women negative for the mutations , and for oestradiol were 33% higher ( p = 0007 ) ie , 59% of carriers had concentrations of serum progesterone that would have been in the top quartile of concentrations in the control group ( or 80 , 95% ci 215257 ; p = 0008 )  . interpretation carriers of brca1 / brca2 mutations are exposed to higher titres of oestradiol and progesterone known risk - factors for breast cancer . 
our ndings could not be explained by di erential contraceptive pill use . funding eve appeal , european union , cancer research uk , and us national institutes of health . introduction in all inherited cancer syndromes the germline mutation is thought to have a so - called local e ect in an organ that is predisposed to the development of cancer , because these mutations do not cause cancers in all organs . 
for example , the increased cancer risk in carriers of the brca1 and brca2 mutations is predominantly that of breast cancer , ovarian cancer , or both.1 these mutations are thought to cause cancer via a defect in dna damage response or in the dna repair pathway.2 however , this defect does not explain the organ - speci c cancer penetrance . 
that removal of both ovaries and fallopian tubes reduces not only the risk of ovarian but also breast cancer3 implicates a systemic dysregulation of hormone production in carriers of the mutation , which a ects both the mllerian epithelium , as the cell of origin for ovarian cancer , 4 and breast epitheliuevidence from preclinical models suggests that both hormone production and hormone sensitivity of end organs is altered in carriers of the brca1 mutation . 
studies in animals57 showed that mice carrying a brca1 mutation in the steroid - hormoneproducing granulosa cells had a longer pro - oestrus phase , corresponding with the oestrogen - dominant follicular phase of the human menstrual cycle . 
also , the insulin - like growth factor system has a fundamental role endometrial biology , acting via autocrine and paracrine mechanisms.8 there are strong interactions between the factor and brca1 signalling insulin - like growth pathways , which also involve oestrogen signalling ; 9 hence , it is possible that the endometrium of carriers of the brca1 mutation has altered sensitivity to hormones . cyclical change in oestradiol and progesterone titres alters endometrial thickness and menstrual bleeding in premenopausal women . 
because many women in the study had undergone clinical genetic for brca1 / 2 mutations , we had a cohort of women known to carry the mutation and a cohort known to be negative for the mutation to compare . 
 to establish the mutation status of these women , highthroughput next generation sequencing provided the fastest and most cost - e ective method of rapidly detecting carriers of the mutations , albeit with potentially lower sensitivity than clinical testing , which in the uk uses a combination of sanger sequencing ( including limited ashkenazi mutation screening where appropriate ) and multiplex ligation probe ampli cation . methods participants after ethical approval ( eastern mrec 97 / 5 / 007 ) , ukfocss recruited from 44 uk regional centres . 
 between june , 2002 , and september , 2010 , women older than 35 years , at an estimated minimum 10% lifetime risk of ovarian cancer based on family history or predisposing germline gene mutations ( appendix ) were recruited and screening data and outcomes were collected prospectively . 
so far , about 25% of the study population have undergone clinically initiated testing for brca1 and brca2 mutations ( either before or after recruitment )  . after ethical approval ( joint university college london / university college london hospital ethics committee , ref 06 / q0505 / 102 ) , we selected all premenopausal ukfocss participants with no previous or subsequent history of cancer ( to avoid including women on hormonal therapy or women with a subclinical cancer , which could have triggered an altered hormonal environment and which could have confounded our analyses ) and no intrauterine device . procedures ovarian cancer screening was done with transvaginal sonography to assess ovarian morphology and serum ca125 tumour marker measurement . 
all centres scanned study participants and all scans were done by sonographers , radiologists , or gynaecologists approved by the uks national health service ( nhs ) , employed by the local hospital for gynaecological scanning , and subject to local nhs quality control . 
participants were included if they matched our inclusion criteria and had provided a dna sample . oestradiol and progesterone were measured with automated immunoassays on the elecsys 2010 analyser ( roche diagnostics gmbh , mannheim , germany )  . 
the progesterone intra - assay cv is 1527% and interassay cv is 3754% . statistical analysis endometrial thickness for each group was averaged for each day of menstrual cycle and smoothed using the averaging running window of 5 days . 
on start and end days of the menstrual cycle the dependencies were prolongedeg , for day 1 , endometrial thickness was averaged over days 30 , 31 , 1 , 2 , and 3 . 
to quantify di erences we focused on days 1014 and days 2126 ( because these were the times in the cycle when di erences were most pronounced ) , and calculated the area under the curve ( auc )  . 
to construct the distributions for aucs , the endometrial thickness values were bootstrapped : for each cycle day the thickness value was sampled with replacement , then the obtained dependence was averaged using a window of 5 days and the auc was calculated for the obtained dependence between days 1014 and 2126 . 
the odds ratios ( ors ) for brca status were obtained for endometrial thickness , treated as a continuous predictor variable , and adjusted in the logistic regression for age and the speci c menstrual cycle day as continuous variables . follicular and luteal oestradiol and progesterone serum titres were grouped into quartiles and ors were calculated with logistic regression . 
therefore the only di erence between b and a is that the former would have had a lower a - priori risk of being mutation carriersthis explains the lower prevalence of mutations recorded in b versus a . 
 however , there was no di erence in ultrasound methods , data collection , sample collection , or storage for these women , so this is not a source of bias . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results 2808 endometrial - thickness measurements and associated last menstrual period dates were available from 1460 eligible women , including 1573 endometrial thickness measurements in women negative for both mutations , 203 in carriers of bcra1 , and 190 in carriers of brca2 ( baseline data shown in the appendix )  . 
in view of this statistically similar endometrial thickness pattern in carriers of the mutations , we combined these groups , and noted clear di erences between the combined carrier group and the group negative for mutations ( gure 2 and table 2 )  . 
in the follicular phase , the carrier groups endometrial thickness was signi cantly higher , whereas thickness was signi cantly lower than that of non - carriers , even after using logistic regression analysis and adjusting for age and menstrual cycle day . 
to assess whether a womans knowledge of her mutation status might a ect the results ( eg , by changing her lifestyle in an attempt to minimise her cancer risk ) , we separately analysed the 728 women in the next generation sequencing group who did not know their mutation status during the trial . 
to be certain that the endometrial thickness di erences were not due to di erential oral contraceptive pill use , we analysed the 1318 endometrial thickness scans for which the women had reported no oral contraceptive pill use in the decade the scan was done ( table 1 )  . 
again , we noted the same endometrial thickness patterns as before ( appendix ) , with higher follicular phase endometrial thickness and lower luteal phase endometrial thickness in carriers of the mutations than for women negative for the mutations . luteal phase endometrial the 1228 vol 14 november 2013 articles brca1 and 2 negative brca1 mutation brca2 mutation brca1 and 2 negative brca1 and 2 mutation the di erences in endometrial thickness between carriers and those negative for the mutations could be a consequence of di erent hormonal sensitivity of the target tissue ( ie , the endometrium ) in carriers of the mutations , triggered by di erent titres of the steroid hormones known to regulate endometrial biology , or a combination of the two . 
although it is di cult to assess hormonal sensitivity directly , to assess the triggering threshold we analysed oestradiol and progesterone in stored serum samples from all premenopausal carriers of the mutations who provided samples between days 1014 ( follicular phase ) and 2126 ( luteal phase ; n = 59 , mean age 406 years , 70 samples ) , and all women negative for the mutations ( n = 283 , mean age 435 years , 339 samples )  . 
 progesterone titres during day 1014 were not measured in all women because pilot data in 38 carriers and 44 controls showed such low titres ( median 127 nmol / l in carriers and controls ) that no signi cant di erences would become apparent on testing all available samples . 
 median luteal phase titres of progesterone were 121% higher ( p = 000034 ) in carriers than in women negative for the mutations , and oestradiol titres were 33% higher ( p = 0007 ) ie , 59% of carriers had concentrations of serum progesterone that would have been in the top quartile of concentrations in the control group ( or 80 , 95% ci 215257 ; p = 0008 ; appendix , gure 3 )  . discussion in cyclical our ndings show clear di erences endometrial thickness in carriers of brca1 / 2 mutations compared with wild - type controls . 
our cohort of well matched premenopausal carriers and controls with combined endometrial thickness information , and serum samples with known menstrual cycle data , was ideal for testing the hypothesis that the organspeci c cancer penetrance in carriers is due to hormonal dysregulation . 
 we speculate that the high luteal phase oestradiol we recorded in carriers triggers increased expression of progesterone receptors , 11 thus potentiating any possible mutagenic e ect of the higher luteal progesterone . 
our ndings support those from studies in mice carrying a brca1 mutation in ovarian granulosa cells.6 , 7 although data on endogenous premenopausal progesterone exposure or = 111 * ( 95% ci 103120 ) p = 00063 or = 090 * ( 95% ci 083098 ) p = 0027 menstrual cycle ( days ) figure 2 : endometrial thickness as a function of the menstrual cycle ( a ) endometrial thickness calculated from 1573 transvaginal ultrasound scans from 754 women negative for both mutations , 203 scans from 116 carriers of the brca1 mutation , and 190 scans from 112 carriers of the brca2 mutation . 
 ( b ) endometrial thickness in 754 women negative for both mutations ( 1573 scans ) and the combined 228 women who were carriers of either mutation ( 393 scans )  . 
 * adjusted for menstrual cycle day and age . and cancer risk is less extensive and less conclusive , 12 postmenopausal exogenous progesterone exposure is a well established risk factor for breast cancer.11 , 1315 we were recently part of a collaborative report suggesting that progestogens cause breast cancer by inducing expression of the receptor activator of nf - b ligand ( rankl ) , and that deleting the receptor for this ligand delays the onset of progestogen - driven breast cancers.16 there is already an vol 14 november 2013 1229 articles area under curve p value panel : research in context days 1014 of cycle days 2126 of cycle < 00001 < 00001 separate brca analysis brca1 mutation brca2 mutation brca1 / 2 negative combined brca analysis brca1 / 2 mutated brca1 / 2 negative auc = area under curve . 
n = number of volunteers . table 2 : endometrial thickness as a function of menstrual cycle in women by brca1 and brca2 mutation status p = 00074 1000 p = 000034 systematic review we searched pubmed for studies on brca mutation and alterations in the female premenopausal reproductive hormone system published in english between sept 1 , 1993 , and feb 28 , 2013 . 
we established that studies in animals showed aberrant hormonal regulation upon loss of brca1 in granulosa cells and that premenopausal surgical resection of the ovaries in women carrying the brca1 or brca2 mutation led to a substantial reduction in the risk of breast cancer.3 systemic endocrine e ects of brca1 or brca2 mutations have not previously been assessed in humans . interpretation our ndings suggest that brca1 / 2 germline mutations are driving carcinogenesis only in part via altered molecular pathways ( eg , those involved in dna repair ) in the organ at risk , and that brca1 / 2 - associated changes in the endocrine system are additional factors . 
potential agents for these trials include selective oestrogen or progesterone receptor modulators , and the anti - rankl ( receptor activator of nf - b ligand ) antibody denosumab ( currently used for osteoporosis treatment , but known to block the downstream carcinogenic e ects of progestogens )  . negative brca1 / 2 mutation negative brca1 / 2 mutation figure 3 : serum progesterone and oestradiol analysis during luteal phase of the menstrual cycle boxplots with horizontal line show 25% , 50% , and 75% quartiles . 
in conjunction with data that show the potential of a progesterone antagonist to prevent brca1 - mediated mammary tumorigenesis in mice , 17 our ndings provide an additional rationale for treatment that interferes with progesterone signalling to prevent breast cancer in carriers of brca1 / brca2 mutations . 
this nding suggests that the endometrium of carriers might be more sensitive to oestrogen - receptor agonists . for ovarian cancer , oestrogen replacement usage21 and obesity ( a hyperoestrogenic state ) 22 are established epidemiological risk implicating hormonal factors dysregulation in its pathogenesis . 
our data , suggesting higher oestradiol titres in the luteal phase of the menstrual cycle in women who are carriers of the brca1 / 2 mutations compared with women negative for the mutations supports this hypothesis . 
we speculate that the higher titres of progesterone with concordant reduced endometrial thickness recorded in the luteal phase in the carrier group compared with the control group might explain why the penetrance for the third triggered cancernamely endometrial hormonally cancerin carriers is much lower than that for ovarian and breast cancer ; it is well recognised that progestogens suppress endometrial proliferation , 23 resulting in a thinner endometrial thickness and lower lifetime risk of endometrial cancer.24 1230 vol 14 november 2013 articles our study has certain limitations . 
furthermore , in view of the age of the cohort ( all were > 35 years ) and their known increased risk of breast cancer , it is probable the proportion using the contraceptive pill at the time of sample donation would have been even lower than the data above . 
most importantly , excluding women with unreported pill use and those known to have taken the pill in the same decade as the scan did not reduce the statistical signi cance of the endometrial thickness di erences between carriers and controls . the control group could have included participants that carry brca1 / 2 mutations who were missed using our next generation sequencing mutation - detection methods ( eg , mutations in regions of low sequence coverage or large genomic rearrangements )  . 
although it is not possible to estimate the frequency of missed mutations , the individuals screened were una ected and therefore had at most a 50% chance of inheriting a germline mutation even if it were present in their family . 
any mutation carriers in the screen - negative group would bias our nding towards the null , suggesting that our study has underestimated rather than overestimated the strength of the recorded e ects . we had insu cient numbers of scans with last menstrual period dates of a cycle length greater than 28 days to draw any conclusions about whether carriers of brca1 / brca2 mutations might have a longer menstrual cycle than women negative for the mutations , as was evident in the previously described mouse model.57 if this were the case , then we speculate that longer cumulative exposure , and the observed higher absolute titres of progesterone and to a lesser extent oestradiol , might contribute to the excess breast cancer risk of carriers of the mutations . our study cannot address whether endometrial thickness and hormone titres are respectively a marker and e ector of breast cancer risk within a brca1 / 2mutant population . 
as a result addressing the question as to whether altered endometrial thickness and steroid hormone titres in premenopausal women are markers for subsequent breast cancer risk or not would be di cult to do . 
it would need a substantial prospective long - term study of pre menopausal brcacarriers who were unwilling to undergo risk - reducing surgery but willing to be followed up for decades . 
our ndings suggest that sex steroids are one of the major drivers for development of breast cancer in this population . we deliberately excluded patients who had a previous diagnosis of breast or ovarian cancer because they could have been on antiendocrine therapy or chemotherapy , which would have altered their ovarian function and biased our ndings . 
it is well known that sex steroids are locally produced within invasive but also within non - invasive breast carcinoma , 25 which might not have been clinically apparent at the time of sample donation . 
hence we decided a priori not to include women with a diagnosis of breast or ovarian cancer subsequent to sample donation to avoid any bias that would favour the hypothesis of an aberrant endocrine system being associated with cancer development in high - risk women . 
however , despite this , we have noted hormonal changes that would be expected to increase breast cancer risk ( ie , raised oestradiol and progesterone in carriers vs controls )  . 
 furthermore , because of the young age of the study group ( all were premenopausal ) , most have not yet reached the age at which their breast cancer would be likely to occur , so most of the excess breast cancer risk of the study population has yet to accrue . 
excluding the small number of women who we know developed breast cancer subsequent to sample donation would be likely to minimise di erences between carriers and controls , making our ndings more compelling . to improve statistical power , we combined carriers of brca1 and brca2 mutations into a single study group . 
 although we acknowledge that it is possible that there are biological di erences between these groups relevant to our investigation , we did not identify statistical di erences between them with respect to endometrial thickness or hormone titres ( appendix )  . 
furthermore , gure 2 clearly shows that both groups have a similar pattern of higher follicular phase endometrial thickness and lower luteal phase endometrial thickness compared with women negative for the mutations . although we have in e ect analysed multiple crosssectional data rather than longitudinal data , we have still identi ed statistically signi cant di erences between carriers and controls . 
we feel such a study would be logistically challenging and recruitment for it would be extremely di cult . carriers and controls , vol 14 november 2013 1231 articles for more on the eve appeal see the control group was not a random sample from the general population , but rather was deliberately selected for high familial risk of ovarian cancer ( to minimise any di erences between mutation carriers and controls )  . 
however , their shared increased ovarian cancer risk makes them the most appropriate control group to compare with carriers of brca1 / brca2 mutations . in conclusion , our ndings provide novel insights into the high penetrance for breast cancer ( via higher progesterone and oestrogen titres ) and also possibly ovarian cancer ( via higher oestrogen titres and potentially lower titres of anti - mllerian hormone26 ) in carriers of brca1 / brca2 mutations . 
 con icts of interest we declare that we have no con icts of interest . acknowledgments this work was funded by the eve appeal and the european unions seventh framework programme ( fp7 / 2007 - 2013 ) under grant agreement number 305428 ( project epifemcare ) and done at uclh / ucl , which received a proportion of its funding from the department of health nihr biomedical research centres ( brc ) funding scheme . 
 we thank david conti for his help in the bioinformatic analysis of next generation sequencing data . corrections correction to lancet oncol 2014 ; 15 : 38 , 43 , 44 correction to lancet oncol 2014 ; 15 : 11422 gatta g , botta l , rossi s , et al . 
lancet oncol 2014 ; 15 : 11422the last sentence of the findings in the summary should have read : the most common grade 3 or 4 adverse events were fatigue ( 97 [ 14% ] of 697 patients allocated zoledronic acid vs 98 [ 14% ] of 704 allocated ibandronic acid ) , increased bone pain ( 91 [ 13% ] vs 85 [ 12% ] ) , joint should receptor pain ( 41 [ 6% ] vs 38 [ 5% ] ) , infection ( 31 [ 5% ] vs 23 [ 3% ] ) , and nausea or vomiting ( 38 [ 5% ] vs 41 [ 6% ] )  . 
in the per - protocol population in table 1 , in the ibandronic acid group , the number of men should read 11 ( 2% ) , the number of patients the with unknown read status 55 ( 8% ) , the number of patients with unknown pr status should read 283 ( 43% ) , and the number of patients with unknown her2 status should read 212 ( 32% ) ; in the zoledronic acid group , the number of patients with unknown pr status should read 277 ( 41% ) and the number with unknown her2 receptor ( 32% )  . 
 status should read 217 ibandronic acid group ( n = 704 ) zoledronic acid group ( n = 697 ) grade 12 grade 3 grade 4 grade 5 total ( % ) grade 12 grade 3 grade 4 grade 5 total ( % ) any adverse event 674 ( 96% ) 667 ( 96% ) 10% frequency in either group abdominal pain altered taste anaemia anorexia breathlessness constipation diarrhoea dry mouth dyspepsia fatigue fever or in uenzalike symptoms headache hypocalcaemia hypomagnesaemia hypophosphatemia infection joint pain muscle pain oedema other pain nausea or vomiting pins and needles renal impairment increased bone pain other adverse events of interest osteonecrosis of the 199 ( 28% ) 177 ( 25% ) 221 ( 31% ) 177 ( 25% ) 246 ( 35% ) 103 ( 15% ) 121 ( 17% ) 222 ( 32% ) 266 ( 38% ) 248 ( 35% ) 544 ( 77% ) 158 ( 22% ) 80 ( 11% ) 83 ( 12% ) 80 ( 11% ) 435 ( 62% ) 125 ( 18% ) 390 ( 55% ) 301 ( 43% ) 410 ( 58% ) 170 ( 24% ) 170 ( 24% ) 215 ( 31% ) 172 ( 24% ) 5 ( < 1% ) 176 ( 25% ) 236 ( 34% ) 208 ( 30% ) 254 ( 36% ) 104 ( 15% ) 140 ( 20% ) 207 ( 30% ) 265 ( 38% ) 176 ( 25% ) 551 ( 79% ) 280 ( 40% ) 222 ( 32% ) 77 ( 11% ) 80 ( 11% ) 72 ( 10% ) 428 ( 61% ) 136 ( 20% ) 398 ( 57% ) 303 ( 43% ) 417 ( 60% ) 156 ( 22% ) 171 ( 25% ) 202 ( 29% ) 226 ( 32% ) 9 ( 1% ) data are number of patients experiencing the event ( highest grade reported )  . 
toxic e ects include serious adverse events . table 2 : toxic e ects in randomised patients vol 15 february 2014 corrections fever or inuenza - like symptoms renal impairment anaemia headache constipation altered taste fatigue infection joint pain nausea or vomitting anorexia muscle pain osteonecrosis of jaw other pain breathlessness dry mouth abdominal pain hypomagnesaemia hypocalcaemia increased bone pain hypophosphatemia pins and needles oedema diarrhoea dyspepsia risk dierence ( dierence in proportion ) events in ibandronic acid group events in zoledronic group 158 / 704 172 / 704 177 / 704 199 / 704 121 / 704 221 / 704 544 / 704 125 / 704 390 / 704 410 / 704 246 / 704 301 / 704 5 / 704 170 / 704 103 / 704 266 / 704 177 / 704 83 / 704 80 / 704 435 / 704 80 / 704 215 / 704 170 / 704 222 / 704 248 / 704 280 / 697 226 / 697 208 / 697 222 / 697 140 / 697 236 / 697 551 / 697 136 / 697 398 / 697 417 / 697 254 / 697 303 / 697 9 / 697 171 / 697 104 / 697 265 / 697 176 / 697 80 / 697 77 / 697 428 / 697 72 / 697 202 / 697 156 / 697 207 / 697 176 / 697 reporting ( 5% ) patients with 38 pain , 34 ( 4% ) reporting infection , and 20 ( 3% ) reporting vomiting or nausea of the 697 patients in the zoledronic acid group . 
in paragraph six of the results section , the rst sentence should read the primary per - protocol analysis , including any skeletal - related event 21 days apart , included 390 events in 257 ( 38% ) of 672 patients in the zoledronic acid group and 419 events in 253 ( 39% ) of 654 patients in the ibandronic acid ( gure 4a ) , corresponding group to 0435 ( 95% ci 0393 to 0480 ) skeletal - related events per personyear in the zoledronic acid group and 0499 ( 0454 to 0549 ) skeletalrelated events per person - year in the ibandronic acid group . 
and the fourth sentence should read the sensitivity analysis excluding hyper calcaemia skeletal - related events was consistent with the above results , with 312 events in the zoledronic acid group and 330 events in ibandronic acid group ; the log relative risk for ibandronic acid versus zoledronic acid was 0122 ( 95% ci 0069 to 0313 ) , which corresponds to a rate ratio of 1130 ( 0933 to 1367 )  . 
these corrections have been made to the online version as of jan 27 , 2014 . 03 02 01 favours ibandronic acid favours zoledronic acid figure 2 : risk di erence of patients experiencing toxic e ects ( ibandronic acidzoledronic acid ) the results table 2 and gure 2 were incorrect ; corrected versions are shown here . 
 sentence nine of paragraph four should read the most reported serious adverse events were pain , commonly section , infection , and vomiting or nausea , reporting with 43 ( 6% ) patients pain , 15 ( 2% ) reporting infection , and 16 ( 2% ) reporting vomiting or nausea of the 704 patients in the ibandronic acid group , compared e53 vol 15 february 2014 correction to lancet oncol 2017 ; 18 : e186 addeo a , gyawali b . 
this has been corrected online as of may 2 , 2017 . vol 18 may 2017 e245 corrections corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 see correspondence page e194 preventable cancer : off - limits for commonwealth meeting ? as the global burden of non - communicable diseases continues to exert its toll , the prevention , screening , and early diagnosis of cancer should be a priority for all countries . 
the letter , cosigned by eminent experts in cancer and population health , demands that issues surrounding cervical cancer and endemic childhood cancers are part of the commonwealth health ministers meeting in may 2017 . 
the signatories also call for screening , early detection , and improved awareness of various childhood cancers , which can be treated successfully if caught early or even prevented through effective control of malnutrition and infectious diseases . 
surely the health of women and children is paramount to achieve such goals ? cost - effective prevention and screening for cancers should be an integral part of any successful uhc agenda . 
the limited reply declares that the prevention , treatment , and care of cancers are a priority , but fails to suggest any amendments to the forthcoming meetings agenda to give these important issues the consideration they deserve . 
a recent report from the american cancer society warns that the incidence of the diseasein which typically 90% of patients are over 50 years of ageis increasing sharply in each generation born since 1950 . 
as national colorectal and bowel cancer awareness months are marked in march and april in the usa and uk , respectively , this timely report rings alarm bells for ominous changes in the aetiology of this disease . despite colorectal cancer being a slow growing disease in which symptoms may not present for many years , survival rates have improved in recent decades , mainly thanks to screening . 
major risk factors ( unhealthy diets , obesity , and sedentary lifestyles ) are becoming more prevalent in successive generations , raising the question of whether these factorsespecially in the early years of lifecould interact with an underlying genetic backdrop to trigger early onset of the disease . screening is the mainstay of colorectal cancer prevention and early detection . 
 furthermore , with the widespread belief that cancer is associated with ageing , family doctors can too easily discount the possibility of colorectal cancer in young patients , even when they present with characteristic symptoms such as blood in the stool and abdominal pain . what can be done ? although whole - population screening is not feasible , cost - effective , or truly warranted , genetic counselling and gene testing for those known to be at high risk because of family history or underlying genetic predisposition could be considered . 
this study aimed to provide internationally comparable local data on the incidence of childhood cancer to promote research of causes and implementation of childhood cancer control . methods this population - based registry study , devised by the international agency for research on cancer in collaboration with the international association of cancer registries , collected data on all malignancies and nonmalignant neoplasms of the cns diagnosed before age 20 years in populations covered by high - quality cancer registries with complete data for 200110 . 
incidence rates per million person - years for the 014 years and 019 years age groups were age - adjusted using the world standard population to provide age - standardised incidence rates ( wsrs ) , using the age - specific incidence rates ( asr ) for individual age groups ( 04 years , 59 years , 1014 years , and 1519 years )  . 
the regional wsrs for children aged 014 years were compared with comparable data obtained in the 1980s . findings of 532 invited cancer registries , 153 registries from 62 countries , departments , and territories met quality standards , and contributed data for the entire decade of 200110 . 
the overall wsr was 1406 per million person - years in children aged 014 years ( based on 284 649 cases ) , and the most common cancers were leukaemia ( wsr 464 ) , followed by cns tumours ( wsr 282 ) , and lymphomas ( wsr 152 )  . 
in children aged 1519 years ( based on 100 860 cases ) , the asr was 1853 per million person - years , the most common being lymphomas ( asr 418 ) and the group of epithelial tumours and melanoma ( asr 395 )  . 
since the 1980s , the global wsr of registered cancers in children aged 014 years has increased from 1240 ( 95% ci 12331247 ) to 1406 ( 14011411 ) per million person - years . interpretation this unique global source of childhood cancer incidence will be used for aetiological research and to inform public health policy , potentially contributing towards attaining several targets of the sustainable development goals . 
the observed geographical , racial and ethnic , age , sex , and temporal variations require constant monitoring and research . funding international agency for research on cancer and the union for international cancer control . copyright 2017 world health organization ; licensee elsevier . 
this notice should be preserved along with the articles original url . introduction cancers rarely occur before age 20 years , and when they do , they raise a range of medical , psychological , ethical , and societal concerns . 
furthermore , the extent of the cancer burden in this young population is unknown in many low - income and middle - income countries ( lmics ) , where data on cancer incidence are not collected . 
even in the presence of population - based information about cancer registries , collection of childhood cancers is often neglected because they represent a small proportion of all cancers , additional data sources might be required , and the resulting statistics must be subjected to meticulous quality control because they are more sensitive to imprecision or missing information . since the publication of the international incidence of childhood cancer , volume 1 ( iicc - 1 ) in 19881 and iicc - 2 in 1998 , 2 no internationally comparable data on incidence patterns of childhood cancer have been published . 
 to address this problem , the international agency for research on cancer ( iarc ) , in collaboration with the vol 18 june 2017 lancet oncol 2017 ; 18 : 71931 published online april 11 , 2017 s1470 - 2045 ( 17 ) 30186 - 9 this online publication has been corrected . 
we searched medline and participating registries for studies on the incidence of childhood cancer worldwide , with the search terms childhood cancer , registry , incidence , and population , in february , 2016 , without language or publication date restrictions . 
 we found that no globally comparable data on cancer types affecting children have been published since iicc - 2 , and no comparison of incidence patterns in children aged 1519 years has been attempted on a global scale . 
 added value of this study this study provides an overview of the incidence of cancer in 200110 for children aged 019 years , based on data collected in 153 population - based cancer registries in 62 countries , departments , and territories on five continents . 
in addition to the sex , age , and tumour - specific incidence rates for 19 world regions or populations for 200110 , we report an increase in the incidence of neoplasms since the 1980s in children aged 014 years . 
it comprehensively summarises the most recent and globally comparable data and presents information per sex , age group , geographical region , and tumour type . implications of all the available evidence the wealth of information provided by this study constitutes a solid baseline to assess needs and define priorities in the area of paediatric oncology , supporting sustainable development goal 3 to ensure healthy lives and promote wellbeing for all at all ages . 
the shortage of high - quality local information should stimulate formation of new and more accurate data sources . international association of cancer registries ( iacr ) , has coordinated a study to assess the incidence of childhood cancer worldwide , the complete results of which will be published in iicc - 3 . 
an age range of 019 years was also chosen in previous us and european studies of childhood cancer incidence and survival.3 , 4 from around here we provide an overview of the findings of the iicc - 3 study , based on a selection of quality - assured the world encompassing datasets information for the complete decade of 200110 . 
the objective of this study was to counteract the difficulties in collecting childhood cancer data from relevant data sources and provide globally comparable estimates of cancer occurrence in children to aid further research and adapt policy measures . methods study design and data sources in this epidemiological , population - based registry study , we invited all population - based cancer registries that we identified among the membership of the iacr and from published literature in medline or other published sources , such as annual reports , in any language . 
analyses for the 014 years age group were based on a larger database ( the paediatric dataset ) than those for the 019 years age group ( general dataset ) , because the paediatric dataset included data from the paediatric cancer registries not collecting data in children older than 15 years and these registries tended to have a wider coverage than the cancer registries used in the general dataset ( appendix pp 24 )  . all malignancies and non - malignant tumours of the cns diagnosed before age 20 years ( before age 15 years in most of the paediatric cancer registries ) in the covered populations in 200110 were eligible for inclusion . 
cancer data included individual records of cases with codes for the following : sex ; age ; date of birth ; date of incidence ; and tumour sequence ( ie , the numerical order of occurrence of the neoplasm ) , site , morphology , behaviour , laterality , and most valid basis of diagnosis . 
the 3rd edition of the international classification of diseases for oncology5 was required for coding of the tumour site , morphology , behaviour , multiple primary tumours , and basis of diagnosis . 
non - conforming systems were converted and tumours were classified centrally according to the 3rd edition of the international classification of ( iccc - 3 ) .6 we childhood cancer requested each contributing cancer registry to provide total population coding 720 vol 18 june 2017 articles counts for each ethnic or racial group , calendar year , sex , and year of age in the registration area of their registry . procedures all submitted datasets were processed and assessed individually in a rigorous peer - review process . 
the assessment criteria included a range of indicators , including the following : minimum number of cases ; proportion of cases confirmed from cancer tissue examination ( microscopic verification ) ; proportion of cases registered from death certificate only ; proportion of cases with morphology not otherwise specified ( ie , cases in the unspecified subgroups of iccc - 3 or those coded by unspecified morphology codes such as 8000 , 8800 , 9800 ) ; proportion of cases with an unlikely combination of site and morphology , or an unlikely age and tumour type ; proportion of rare entities ( ie , neoplasms that occurred with a frequency of < 005% in large datasets ) ; proportion of dates of birth and incidence that were incomplete ; proportion of ages that were imprecise ; overall incidence rates ; proportion of cases and incidence by sex , age group , and tumour type ; the stability of rates over time ; proportion of multiple primary diagnoses ; and consistency of population data . 
the improvements included completion of missing information , additional years of data , inclusion of information from missed data sources , correction of coding errors , improvements in calculation of age , inclusion of non - malignant cns tumours , replacement of population data , and explanation of the questioned patterns . statistical analysis we calculated age - specific incidence rates ( asr ) for four 5 - year age groups ( 04 years , 59 years , 1014 years , and 1519 years ) as the quotient of the number of cases and the number of person - years in the respective categories of sex , geographical area , and racial or ethnic group for the applicable time period , expressed per million person - years . 
we defined person - years as the sum of the population counts in a specific geographical area surveyed by a registry in each year from 2001 to 2010 , categorised by sex and age and , if relevant , race or ethnicity . 
in the absence of all required details , we estimated the covered population counts by linear interpolation ( six registries ) or extrapolation ( three registries ) from the data provided by the registries , based on an assumption of regular population growth , before calculating rates . 
the purpose of this study was to make comparisons among regions and time periods , so all reported incidence rates for the 014 years and 019 years age groups were adjusted via direct standardisation . 
we calculated age - standardised rates ( wsrs ) as the weighted average of the three age - specific rates ( to calculate rates for 014 years ) or four age - specific rates ( for 019 years ) , using the weights of the world standard population7 ( appendix p 5 )  . 
 we calculated incidence sex ratios by dividing the incidence in male individuals with that in female individuals . the results are presented for 19 geographical regions or populations and a combined total ; all the defined regions are either un - defined regions8 or an aggregate of un - defined regions , with the exception of north america , for which we present data separately for canada and the usa , and have split data for the usa into five racial or ethnic groups . 
we calculated the proportion of the covered population of the world and each region by dividing the included person - years by the total personyears in 200110 by age group , as estimated by the un in 2015.9 to compare the incidence rates derived from the paediatric dataset for 200110 with those published in iicc - 2 , 2 we assigned iicc - 2 registry data to the same geographical regions as used in this iicc - 3 study . 
although the target period of iicc - 2 was the 1980s , the time periods of the contributing registries differed both in length and starting years , because they either followed on from the iicc - 1 period or they could not provide other years of data . 
the corresponding author had final responsibility for the decision to submit for publication . results of the 532 invited cancer registries , 420 submitted their data and 309 met standard data quality criteria . 
 approximately 114% of the world population aged 014 years ( contributing 18 376 710 144 person - years ) was covered by the registries included in our study , ranging from 17% in south asia ( india ) to 994% in north america ( table 1 )  . 
coverage of the world population within the indicated age group . table 1 : coverage of the world population aged 019 years , person - years , numbers of cancer cases , and quality indicators of data included in the analyses , overall and by region , 200110 paediatric dataset ( age 014 years ) general dataset ( age 019 years ) cases person - years ( millions ) incidence per million cases person - years ( millions ) incidence per million age group , all cases ( asr ) sex ( wsr ) boys girls 04 years 59 years 1014 years 1519 years 019 years 014 years 019 years 156 721 127 917 1072 1023 127 096 74 175 83 378 age group , all cases ( wsr ) 014 years * 284 649 2095 1406 age group , malignant cases only ( wsr ) 274 096 2095 1356 1514 1294 1879 1076 1144 169 531 141 695 1039 93 559 54 370 62 438 100 860 210 367 311 227 206 027 305 233 1481 2025 1481 2025 1632 1436 1971 1116 1203 1853 1472 1558 1443 1528 asr = age - specific rate . 
registration of non - malignant cns tumours differed by registry , and was higher in the paediatric dataset than in the general dataset ( table 1 , 2 )  . 
 the overall wsrs were 1406 per million person - years in children aged 014 years and 1558 per million person - years in those aged 019 years ( table 2 )  . 
the asr in young people aged 1519 years was 1853 per million person - years . incidence rates were slightly higher in boys than in girls ( incidence sex ratio was 117 in the 014 years age group and 114 in the 019 years age - group ) and varied with age , region , and diagnostic group ( table 2 ; appendix p 8 )  . 
across all regions , incidence was higher in boys than in girls ( incidence sex ratio ranged from 11 to 14 in the 019 years age group ; appendix p 8 ) , except for the 1519 years age group of native americans in the usa ( incidence sex ratio of 09 ) and in east asia ( 10 ) , where girls had a higher incidence ( ratios rounded to one decimal place ; appendix p 8 )  . 
sex - specific incidence varied by diagnostic group , with renal tumours and epithelial tumours more common in girls , with variations by age group ( appendix p 8 )  . 
germ cell and gonadal tumours were also more common in girls than in boys in the 014 years age group ( appendix p 8 )  . asrs were higher in children aged 04 years and 1519 years than in those aged 59 years and 1014 years ( table 2 )  . 
 in the 014 years group , overall wsrs varied from less than 100 per million person - years in sub - saharan africa , for native american children in the usa , and in south asia ( india ) , to more than 150 per million person - years in some subpopulations of north america and europe , and in oceania ( figure 1a ; appendix p 6 )  . 
in young people aged 1519 years , the lowest asr was observed in 722 vol 18 june 2017 articles a age 014 years b age 1519 years north africa sub - saharan africa central america and caribbean south america north america east asia south asia * southeast asia west asia eastern europe northern europe southern europe western europe oceania wsr per million person - years highest rate lowest rate overall rate asr per million person - years figure 1 : variation in the overall incidence of childhood cancer by geographical region , 200110 data are for children aged 014 years , from the paediatric dataset ( a ) , and 1519 years , from the general dataset ( b )  . 
 * comprising data from india only . leukaemia lymphoma cns tumours sympathetic nervous system tumours retinoblastoma renal tumours hepatic tumours bone tumours soft tissue sarcomas germ cell and gonadal tumours epithelial tumours and melanoma other and unspecied 04 59 1014 1519 south asia ( india ) , whereas the highest asrs were seen in some predominantly white populations of north america , europe , and oceania ( figure 1b ; appendix p 6 )  . the range of tumour types varied markedly with age group ( figure 2 )  . 
in children aged 04 years , leukaemia represented 361% ( 45 849 of 127 096 ) of all cases ; however , the proportion of leukaemia cases was 154% ( 15 520 of 100 860 ) in young people aged 1519 years . 
conversely , lymphomas represented 53% ( 6766 of 127 096 ) of cases in children aged 04 years , and 225% ( 22 740 of 100 860 ) of cases in those aged 1519 years . 
epithelial tumours and melanoma represented 09% of all cases in children aged 04 years ( 1197 of 127 096 ) , but were the second most common tumour group in young people aged 1519 years ( 21 480 [ 213% ] of 100 860 )  . 
of note is the relatively high sympathetic nervous system tumour wsr of 102 per million person - years in black children in the usa , which contrasts with the wsr of 27 per million person - years in the mostly black population of subsaharan africa ( table 3 )  . 
renal tumours were common in 100% proportion of all cancers figure 2 : proportional distribution of cancer type by age group , 200110 , all regions combined tumours classified by international classification of childhood cancer , volume 3.6 statistics for children younger than 15 years are based on the paediatric dataset and the statistics for those aged 1519 years are based on the general dataset . children aged 04 years ( 11 297 [ 89% ] of 127 096 ) , and their relative frequency decreased in older age groups , to 07% ( 756 of 100 860 ) in young people aged 1519 years ( figure 2 )  . 
soft tissue sarcomas were present in a similar proportion of cases in children aged 014 years and those aged 1519 years in most regions ( table 3 , 4 ; figure 2 ; appendix p 10 )  . 
in sub - saharan africa , 46% ( 579 of 1262 ) of all soft tissue sarcomas in children aged 014 years were kaposis sarcoma compared with 57% ( 119 of 208 ) in those aged 019 years , whereas in all the other regions kaposis sarcoma represented less than 1% of all soft tissue sarcomas in children younger than 15 years and a maximum of 2% ( 14 of 592 ) in black children in the usa ( data for all regions not shown )  . 
germ cell and gonadal tumours were rare in children younger than 15 years ( 10 200 [ 36% ] of 284 649 ; table 3 ) , and more common in those aged 1519 years ( 12 105 [ 120% ] of 100 860 ; table 4 )  . 
the group of epithelial neoplasms and melanoma comprises several specific types of carcinomas ( adrenocortical , thyroid , nasopharyngeal , skin ) , all other types of carcinoma ( except those occurring in kidney , liver , and gonads ) , and melanoma . 
this group constituted 38% ( 10 679 of 284 649 ) of all tumours in children aged 014 years and 213% ( 21 480 of 100 860 ) in those aged 1519 years ( appendix p 10 )  . 
the group of other and unspecified tumours comprised 09% ( 2469 of 284 649 ) of all cases in children aged 014 years and 15% ( 1500 of 100 860 ) of all cases in those aged 1519 years . 
 in 22 registries no tumours were classified in this category ; other and unspecified tumours comprised 5% or more of all tumours in ten registries , including one registry for which 12% ( 68 of 561 ) of all tumours were classified as other and unspecified . in children aged 014 years , the leading cancers in all regions combined were leukaemia , followed by cns tumours , and then lymphomas , and this ranking was 726 vol 18 june 2017 articles all cancers in age 1519 years north africa sub - saharan africa central america and caribbean south america canada usa , native american usa , asian and pacic islander usa , black usa , hispanic white usa , non - hispanic white east asia south asia * southeast asia west asia eastern europe northern europe southern europe western europe oceania observed in most world regions ( table 3 )  . 
the ratios of highest to lowest regional wsr were higher than 50 for cns tumours ( 62 ) , germ cell and gonadal tumours ( 59 ) , neuroblastoma ( 56 ) , epithelial tumours and melanoma ( 55 ) , and leukaemia ( 52 )  . in young people aged 1519 years , lymphomas were the most common cancers in all regions combined , followed by epithelial tumours and melanoma ( table 4 ; figure 4 )  . 
 however , leukaemia was the most common neoplasm in this age group in south america , native american and white hispanic children in the usa , south asia ( india ) , and southeast asia ( table 4 ; figure 4 )  . 
in oceania , white non - hispanic children in the usa , in east asia , and in central america and the caribbean the most common cancer type was the group of epithelial cancers and melanoma ( table 4 ; figure 4 )  . 
geographical variations in incidence , expressed as the ratio of the highest to the lowest asr across regions , were 50 or higher for hepatic tumours ( 78 ) , germ cell tumours ( 64 ) , cns tumours ( 60 ) , lymphomas ( 54 ) , epithelial tumours and melanoma ( 52 ) , and soft tissue sarcomas ( 50 )  . from the 1980s to 200110 , the overall wsr for all tumours in children aged 014 years increased from 1240 per million person - years ( 95% ci 12331247 ) in the 1980s to 1406 per million person - years ( 14011411 ) in 200110 . 
the increase was seen in all regions except sub - saharan africa , and was smallest in central america and the caribbean ( wsr 1253 [ 95% ci 12121294 ] in 198089 ; 1292 [ 95% ci 12591325 ] in 200110 ) and highest in southeast asia ( 920 [ 95% ci 892948 ] ; 1198 [ 95% ci 11731223 ] )  . 
in sub - saharan africa , a decrease was noted between the 1980s ( 810 [ 95% ci 768852 ] ) and 200110 ( 563 [ 95% ci 551575 ] ; figure 5 ; appendix p 7 )  . asr per million person - years leukaemia lymphoma cns tumours sympathetic nervous system tumours retinoblastoma renal tumours hepatic tumours bone tumours soft tissue sarcomas germ cell and gonadal tumours epithelial tumours and melanoma other and unspecied figure 4 : incidence of cancer in young people aged 1519 years , 200110 , by region tumours classified by international classification of childhood cancer , volume 3.6 data are based on the general dataset . 
 * comprising data from india only . discussion using data provided by 153 high - quality cancer registries , we report internationally comparable incidence rates of cancer in children aged 019 years during 200110 . 
the incidence of cancer in children aged 014 years was 1406 per million person - years , and in those aged 019 years was 1558 per million person - years . 
to our knowledge , this report presents the best available information on cancer incidence for the given period and age group . we chose wsr as a relative estimate of cancer burden , but it should not be used for estimating numbers of cases in a population , because the value of wsr depends on the choice of the standard population . 
 although 20% of the cancers occurring in young people aged 1519 years were epithelial tumours ( the most prevalent histology types in adults ) or melanoma , this age group also had high proportions of lymphomas , leukaemias , germ cell tumours , and sarcomas . 
therefore , iccc - 36 seems to be well adapted to reporting incidence in this age group , because the named tumour groups represent the main diagnostic categories in iccc - 3 . 
we found that the incidence of cancer in young people aged 1519 years was 1853 per million person - years , based on 100 860 cases . because not all the contributing paediatric cancer registries could provide data for young people aged 1519 years , the analyses for children aged 014 years were based on a different dataset ( paediatric dataset ) than were the analyses for children aged 019 years or those aged 1519 years ( general dataset )  . 
the two resulting datasets vol 18 june 2017 articles north africa sub - saharan africa central america and caribbean south america north america east asia south asia * southeastern asia west asia eastern europe northern europe southern europe western europe oceania we selected the contributing registries because they provided quality - assured data for the entire decade of 200110 . 
inevitably , the reported rates were influenced by this selection ; however , they provide the best and unique comparable global incidence estimates for the given period because they are not affected by intermittent contributions for parts of the target period . a particular strength of our study comes from separate presentation of the incidence patterns for the five racial and ethnic groups distinguished in the us data , despite the difficulties in classifying the us population into racial and ethnic groups due to population mixing , migration , and self - declaration of ethnicity.11 unfortunately , the ethnic differences within multi - ethnic populations of europe , canada , and some other regions could not be readily studied . 
for the purpose of simplicity these data were not included in this paper ; however , they are available online on the iicc - 3 website . our study improved the overall data quality in all participating cancer registries , particularly in 72 of 153 whose datasets were not acceptable at the beginning of the study . 
the study raised the registries awareness of additional data sources ( haematology , opthalmology , orthopaedics , dermatologicaly , neurology , endocrinology , and paediatric clinics ) and of specific quality control . 
we required a high level of quality and completeness for our study , because small errors or omissions would have had a large impact on the resulting incidence rates . approximately 30 cancer registries dropped out of the study , irrespective of the quality of their data . 
data collected on more than 40 million person - years in 12 cancer registries ( canada [ new brunswick , prince edward island ] , denmark , finland , germany [ berlin , brandenburg , bremen , mecklenburgvorpommern , sachsen - anhalt , and the free states saxony and thuringia ] , and singapore ) could not be used because these registries were bound by requirements of a specific administrative procedure to approve provision of their data . although the cancer registries follow international guidelines , we observed wide variation in registration techniques , access to data sources , case eligibility criteria , application and interpretation of registration standards , and coding systems . 
other practices reduced data quality ( eg , restricted or no access to pathology reports ) , completeness ( eg , restricted or no access to identifiable death certificates ) , or timeliness ( eg , third - party data encryption )  . 
in some registries cases were coded as wsr per million person - years iicc - 2 , published data ( 1980s ) iicc - 3 , selection ( 200110 ) figure 5 : comparison of incidence of neoplasms in children aged 014 years in 198089 and 200110 , by region data from the two time periods were standardised and peer reviewed using similar methods . 
 * comprising data from india only . gave different estimates of incidence for the ( common ) age group of 014 years , and this incidence was 5% lower in the paediatric than in the general dataset . 
this difference can be explained by variations in population coverage between the registries , and possibly distinctive data sources used by the two types of registries ( ie , those that included data for young people aged 1519 years and those that did not ) , as was shown previously in an analysis of data on childhood cancer in europe.4 although the results presented from both datasets are based on the best data available for each age group , they also emphasise the importance of quality assurance , particularly when dealing with a rare disease such as childhood cancer . 728 vol 18 june 2017 articles microscopically verified only if the pathology report could be reviewed by registry staff . 
registries are often under - resourced , and large investments for a small proportion of cases in general cancer registries might not be seen as a priority ; however , these variations highlight the need for support to enable production of high - quality and comparable data . a high proportion of specified diagnoses cannot be ensured without available specialised diagnostic facilities . 
 the category of unspecified morphology might have included misclassified specific cancers , but in the absence of precise documentation it might have also included cases that were not malignant or cancers that did not occur in children . although the differences in sex ratios by diagnostic group and age might have to a large extent reflected true differences in disease occurrence , 12 the differences by geographical region could have more readily reflected sociocultural customs whereby boys are favoured over girls to seek medical attention when sick . 
the potential for such selective treatment in india and in some african populations was supported by our registry contacts in those regions when we inquired about a possibility of inequality in seeking health care . the registries with no access to a national database of all causes of death might not have registered the cancers that were only discovered at the time of death , even though the proportion of missed cases might be low in childhood populations . 
the registries operating in some lmics were particularly affected by missing or infrequent official population estimates , and these data needed to be estimated by interpolation or extrapolation , influencing the reported rates . 
treatment abandonment , common in lmics , 14 might also have led to underregistration if identified patients who refused treatment were not sufficiently well described ( eg , missing dates or place of residence )  . 
under - ascertainment of diagnosed cases might have from administrative resulted restrictions of access to medical files , political or social instability , competing needs , and inadequate political will , causing a dearth of resources , shortage or volatility of registry personnel , loss of perennial expertise , and missing or broken links with relevant data sources . 
 overestimates of incidence might have occurred in areas with superior treatment facilities if the place of permanent residence could not be correctly determined for registered patients , and national coverage would neutralise such artefactual regional differences within a country.15 accurate incidence rates are also difficult to obtain in ethnic minorities , such as the native american population in the usa , possibly because of imprecise classification of the at - risk population , as well as patients with cancer.16 cancer statistics in high - income countries might be influenced by overdiagnosis of some cancers detected by non - invasive imaging and screening tests , including neuroblastoma , thyroid cancer , melanoma , and kidney cancer.17 is certainly influenced by although a complete assessment of time trends in incidence falls outside the scope of this report , our data showed that the overall incidence of registered neoplasms in childhood increased between the 1980s and the 2000s . 
 our comparison the composition of the two data pools ( different registries have contributed to the two compared periods ) ; however , the increase in the overall rates is clear . 
future detailed analyses of time trends by tumour group and subpopulations will bring more clarity to the interpretation of these secular changes . the reduction of cancer incidence in sub - saharan africa probably had two main causes . 
first , this iicc - 3 study included data from the national childhood cancer registry of south africa , which contributed 70% of all cases for this region and reported very low incidence rates . 
of the five datasets classified as sub - saharan african in iicc - 2 , only one ( from namibia ) reported a lower overall incidence rate than the south african registry in iicc - 3 . 
the possible reasons for the low rates in south africa are discussed elsewhere.18 second , the implementation of antiretroviral therapy in some areas affected by hiv19 has contributed to a decrease in incidence of kaposis sarcoma . 
this cancer type represented more than a third of the total cancer incidence in kampala , uganda , in the iicc - 2 ( wsr 1827 per million person - years )  . 
the incidence of kaposis sarcoma in kampala halved between the iicc - 2 and this iicc - 3 study , and a decreasing trend between the 1990s and the 2000s was also noted in a kampala registry study.20 leukaemia , the most common cancer in children worldwide , had the largest impact on total cancer incidence . 
even though strong underdiagnosis of leukaemia is suspected in sub - saharan africa , 21 less commonly diagnosed in black children in the usa than in the other us ethnic groups ; however , whether leukaemia was also vol 18 june 2017 articles leukaemia might be underdiagnosed as a result of reduced access to health care associated with lower economic status in this group is unclear.22 in children aged 014 years , the highest leukaemia rates were in hispanic white children in the usa ( 40% of total incidence )  . 
the native american component of hispanic ancestry was a presumed risk factor , based on the observations that known risk alleles at loci identified in genome - wide association studies of european - ancestry populations in cdkn2a , pip4k2a , cebpe , and arid5b were all significantly associated with native american ancestry.23 comparatively high incidence rates and the largest proportion of leukaemia among all cancers were reported in southeast asia . 
a link to the massive use of pesticides in this world region24 to protect crops and increase yields should be examined in specific studies , since exposure to pesticides has been associated with leukaemia risk.25 , 26 the male predominance among patients with lymphoma is probably a result of innate sex differences in susceptibility , but with increasing age other factors might play a role , such as the increased risk of hiv infection in boys compared with girls.27 the highest incidence of lymphomas worldwide has been reported in the mediterranean region ( as shown in our study and others28 ) , and in hiv - infected populations , 29 with b - cell non - hodgkin lymphoma an aids - defining malignancy . burkitts lymphoma is endemic and common in some sub - saharan african childhood populations , 30 in which hiv infection can further accentuate its incidence.2 , 31 hodgkins lymphoma is rarer in populations of south and east asia than in other parts of the world ; the undergoing socioeconomic changes might gradually result in a similarly high incidence to that observed in western populations.32 , 33 rates in lmics most probably the highest incidence of all cns tumours was noted in high - income countries , which is clearly related to the wide availability of diagnostic facilities . 
the lower incidence ( and proportionately ) reflect poor access to neuroimaging facilities ( eg , low number of ct or mri scans , long waiting lists , and prohibitive costs of diagnostics tests ) .34 , 35 this poor access causes delay in diagnosis and possibly underdiagnosis of brain tumours.36 comparability of incidence of cns tumours across the continents would be greatly improved if all registries attempted to collect information on non - malignant cns tumours , at least in children . this study describes the global cancer incidence patterns in children younger than 20 years for 200110 , providing an update to comparable information that is now almost 20 years old.2 despite possible artefacts influencing data availability , quality , and comparability , the size of the studied populations and the observed differences in our study suggest that our data are sufficiently robust for international comparisons of childhood cancer occurrence , and provide useful pointers for further studies . 
the collected data can be used for further research , including continued development of childhood - specific registration standards and guidelines , detailed studies in subpopulations and by tumour subtype , and global estimates of cancer indicators . 
to secure data availability and quality , constant support of cancer registration is required at local , national , and international levels . contributors es - f , lagr , fm , ph , hys , and cas designed the study . 
es - f drafted the manuscript , which was reviewed , modified , and approved by es - f , lagr , fm , ad , fb , ph , hys , and cas . declaration of interests we declare no competing interests . acknowledgments international incidence of childhood cancer , volume 3 is supported by the international agency for research on cancer and the union for international cancer control . 
the cooperation of all cancer registries and members of the international association of cancer registries is gratefully acknowledged . see correspondence page e194 preventable cancer : off - limits for commonwealth meeting ? as the global burden of non - communicable diseases continues to exert its toll , the prevention , screening , and early diagnosis of cancer should be a priority for all countries . 
the letter , cosigned by eminent experts in cancer and population health , demands that issues surrounding cervical cancer and endemic childhood cancers are part of the commonwealth health ministers meeting in may 2017 . 
the signatories also call for screening , early detection , and improved awareness of various childhood cancers , which can be treated successfully if caught early or even prevented through effective control of malnutrition and infectious diseases . 
surely the health of women and children is paramount to achieve such goals ? cost - effective prevention and screening for cancers should be an integral part of any successful uhc agenda . 
the limited reply declares that the prevention , treatment , and care of cancers are a priority , but fails to suggest any amendments to the forthcoming meetings agenda to give these important issues the consideration they deserve . 
a recent report from the american cancer society warns that the incidence of the diseasein which typically 90% of patients are over 50 years of ageis increasing sharply in each generation born since 1950 . 
as national colorectal and bowel cancer awareness months are marked in march and april in the usa and uk , respectively , this timely report rings alarm bells for ominous changes in the aetiology of this disease . despite colorectal cancer being a slow growing disease in which symptoms may not present for many years , survival rates have improved in recent decades , mainly thanks to screening . 
major risk factors ( unhealthy diets , obesity , and sedentary lifestyles ) are becoming more prevalent in successive generations , raising the question of whether these factorsespecially in the early years of lifecould interact with an underlying genetic backdrop to trigger early onset of the disease . screening is the mainstay of colorectal cancer prevention and early detection . 
 furthermore , with the widespread belief that cancer is associated with ageing , family doctors can too easily discount the possibility of colorectal cancer in young patients , even when they present with characteristic symptoms such as blood in the stool and abdominal pain . what can be done ? although whole - population screening is not feasible , cost - effective , or truly warranted , genetic counselling and gene testing for those known to be at high risk because of family history or underlying genetic predisposition could be considered . 
 the lancet oncology vol 18 april 2017 editorial correction to lancet oncol 2017 ; 18 : 132737 correction to lancet oncol 2017 ; 18 : 133847 correction to lancet oncol 2017 ; 18 : e564 dimopoulos ma , goldschmidt h , niesvizky r , et al . 
 lancet oncol 2017 ; 18 : 132737in the results section of this article , the data presented for any - grade adverse diarrhoea events should read diarrhoea ( 168 [ 36% ] vs 185 [ 41% ] )  . 
 these corrections have been made to the online version as of sept 27 , 2017 , and the printed article is correct . myelodysplastic in patients with platzbecker u , germing u , gtze ks , et al . 
luspatercept for the treatment of anaemia lowerrisk syndromes ( pace - mds ) : a multicentre , openlabel phase 2 dose - finding study with long - term extension study . 
 18 : e564in the second paragraph of brian samuels affiliation , the sentence in parentheses should have read ( summit cancer centers , post falls , id , usa )  . 
in the third paragraph , the sentence and quote from brian samuels as should have samuels summarised , we decided to recapitulate the original phase 2 study in liposarcomas pazopanib is active in the treatment of liposarcomas , just as it is for other subtypes of sarcoma . 
 these corrections has been made to the online version as of sept 27 , 2017 . vol 18 october 2017 e562 corrections corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
we assessed the effect on participation of sending invitations for breast screening with a timed appointment to women who did not attend their first offered appointment within the nhs breast screening programme ( nhsbsp )  . methods in this open , randomised controlled trial , women in six centres in the nhsbsp in england who were invited for routine breast cancer screening were randomly assigned ( 1 : 1 ) to receive an invitation to a second appointment with fixed date and time ( intervention ) or an invitation letter with a telephone number to call to book their new screening appointment ( control ) in the event of non - attendance at the first offered appointment . 
 randomisation was by sx number , a sequential unique identifier of each woman within the nhsbsp , and at the beginning of the study a coin toss decided whether women with odd or even sx numbers would be allocated to the intervention group . 
the primary endpoint was participation ( ie , attendance at breast cancer screening ) within 90 days of the date of the first offered appointment ; we used poisson regression to compare the proportion of women who participated in screening in the study groups . 
this trial is registered with barts health , number 009304qm . findings we obtained 33 146 records of women invited for breast cancer screening at the six centres between june 2 , 2014 , and sept 30 , 2015 , who did not attend their first offered appointment . 
participation within 90 days of the first offered appointment was significantly higher in the intervention group ( 2861 [ 22% ] of 12 807 ) than in the control group ( 1632 [ 12% ] of 13 247 ) ; relative risk of participation 181 ( 95% ci 170193 ; p < 00001 )  . 
this strategy can be easily implemented by the screening sites and , if combined with simple interventions , could further increase participation and ensure an upward shift in the participation trend nationally . 
whether the policy should vary by time since last attended screen will have to be considered . funding national health service cancer screening programmes and department of health policy research programme . copyright the author ( s )  . 
 introduction an important indicator of the public health impact of the national health service breast screening programme ( nhsbsp ) in the uk is the participation rate , defined as the percentage of women invited for screening who are screened adequately within 180 days of invitation ( usually referred to as uptake in official reports )  . 
in england , participation following routine invitation fell from 744% in 200405 to 713% in 201415 , 1 and we are seeing a decline for the fourth consecutive year in a row , approaching the national minimum standard of 70% . 
 in particular , participation among women invited for their prevalent ( first ) round of screening has decreased by an even greater amount ( from 701% in 200405 to 633% in 201415 ) .1 participation in breast cancer screening also tends to be lower in areas of socioeconomic deprivation than in wealthier areas.2 , 3 the nhsbsp invites women aged 5070 years to mammographic screening every 3 years . 
an age eligibility extension to invite women aged between 47 years and 73 years is currently being for non - attenders of the first offered appointment is to send trialled.4 the usual practice 972 vol 18 july 2017 articles research in context evidence before this study we searched the pubmed database with the keywords breast cancer , breast screening , appointment , and non - attenders for articles in english published between jan 1 , 1990 , and dec 31 , 2016 . 
in 1998 , stead and colleagues compared second appointments with fixed date and time versus open second invitations for non - attenders of breast cancer screening in a randomised controlled trial in one breast screening centre in england , finding an increased participation rate with second timed appointments . 
 although the quality of the trial was good , its findings might not apply to current practice and target populations for screening since these have changed in terms of age and might have changed in terms of social support and employment status . 
in 2016 , hudson and colleagues reported the results of an observational study in north london comparing timed and non - timed second appointments , showing increased participation with timed appointments . 
we identified no trials of second timed appointments for non - attenders from outside the uk breast screening programme . added value of this study our randomised controlled trial assessed the effects of sending invitations for breast cancer screening with a second timed appointment to women who did not attend their first offered appointment . 
we could therefore analyse the efficacy of the intervention depending on a womans location and level of socioeconomic deprivation since the sites in the study covered a wide range of socioeconomic status levels . implications of all the available evidence our findings show the positive effects of second timed appointments on attendance for breast cancer screenings . 
 the results are of policy interest for early detection of breast cancer , because a simple change in the procedure of addressing non - attenders of breast cancer screening invitations could result in more women being screened . them a second invitation letter , which can vary : some centres supply open invitations , asking women to telephone to make an alternative appointment ; whereas others routinely offer second timed appointments , with date , time , and place stipulated . 
the department of health has advised nhs england that the approach with second timed appointments should be used.5 second timed appointments are nhsbsp policy , although this approach is not universally followed . although some women might not attend their screening appointment because they have made an informed choice not to do so , some of them will not attend for other reasons . 
these women might find a second timed appointment more beneficial than an open invitation because it does not require any effort to book a new appointment with the screening centre . 
 previous findings suggest that participation is greater when a second non - attenders , 6 , 7 but further investigations are needed to identify the women who would be most and least likely to respond to the second invitation . 
for example , someone who has not attended their last three screening appointments might not attend whatever the form of the second invitation . timed appointment is given in a randomised trial published in 1998 , stead and colleagues6 found that the effect of second timed appointments declined with increasing time since last screen , and in a more recent observational study , hudson and colleagues7 noted the same association , at least in absolute terms , in north london . 
therefore , we did a randomised trial of second timed appointments versus open invitations for non - attenders within the nhsbsp , powered to obtain significant results within subgroups of time since last screen . methods study design and participants this open , two - arm , randomised controlled trial was done in six screening sites in england ( derby , hull , plymouth , sheffield , southeast london , and west london ) for different time lengths between june 2 , 2014 , and sept 30 , 2015 . 
the date a batch was set up ( ie , the list of women to be invited was compiled ) , was defined as the date the screening episode was opened for each woman in that list . 
 batches of women invited to routine breast cancer screening were randomly assigned ( 1 : 1 ) to be sent either a second appointment with a fixed date and time ( intervention ) or an open invitation ( control ) in the event of non - attendance at the first offered appointment . 
women who self - referred for screening , women on an early recall protocol , and women who were invited because of a high risk of breast cancer were not randomised . 
for these women , the first invitation date was used for reference and participation was based on the first attendance date ( if any ) ie , only one of the multiple records was kept . 
other exclusions that were judged to be necessary were women invited to screening outside the study period of the screening sites ; observations with previous screening appointment more recent than the first offered appointment or date of the screening episode being opened ; and observations with a date on the invitation letter for a previous round of screening more recent than the date on the current invitation letter . 
we also excluded women who participated but had missing dates of attendance , because in those cases it was not possible to determine whether they had attended within 90 days of their first offered appointment or within 180 days of their episode being opened ( or neither )  . women were not informed of the study or asked to give consent for three reasons . 
the study was approved by the london bloomsbury research ethics committee . randomisation and masking within each screening centre , every invited woman was allocated a unique number , known as the sx number . 
at the beginning of the study , a coin toss by the chief investigator ( swd ) decided that women with an odd sx number would be allocated to the intervention group ( second timed appointment ) , whereas women with an even sx number would be allocated to the control group ( open second invitation )  . 
women who received their group assignment ( eg , women randomly assigned to the control group who received a second timed appointment letter by administrative error ) were marked with an error code but were still included in analysis . intervention the wrong for procedures women who did not attend their first offered appointment were flagged as such by staff at that clinic on the national breast screening system ( nbss )  . 
differences between the two letters were kept to a minimum so that women receiving second timed appointment letters did not feel pressurised into attending their screening appointment if they had made the decision not to participate . 
second timed appointments had to be allocated to non - attenders within 90 days of the missed appointment . because many practices already used second timed appointments for non - attenders of breast cancer screening , this study merely represented a minor variation in routine practice . 
data were pseudonymised , removing identifying data items such as month and day of birth and postcode , before being sent to the centre for cancer prevention ( wolfson institute of preventive medicine , queen mary university of london ) , where analyses were done . outcomes the primary endpoint was participation ( ie , attendance ) within 90 days of the first offered appointment . 
the key secondary endpoint was participation within 180 days of the screening episode being opened , used formally in the programme as a measure for calculating participation rates ( usually referred to as uptake in reports )  . 
other secondary endpoints were subgroup analyses by prevalent ( first ) or incident ( subsequent ) screen status , by time since last attended screen , and by index of multiple deprivation and age . 
 statistical analysis on the assumption that 40% of women who received their first invitation letter would not attend their screening appointment , we required 90% power for a difference of 20% ( intervention group ) versus 15% ( control group ) of those re - invited participating within 90 days . 
we also assumed that 20% of invitees would be non - attenders at their last routine screening ; that 15% would not have attended for three screening episodes or more ; and that 10% would not have attended for four episodes or more . 
 these proportions were approximations derived from offman and colleagues study8 and from the 10% neverattenders observed in the west midlands screening histories project.9 we required 80% power in all the subgroups for a difference of 14% ( intervention ) versus 10% ( control ) in non - attenders at their last routine screening , of 10% versus 7% in those who had not attended for three screening episodes or more , and of 2% versus 1% in those who had not attended for four screening episodes or more . 
these proportions corresponded to requirements 974 vol 18 july 2017 articles of 1252 , 1085 , 1422 , and 2515 individuals per group in each of the four categories , respectively . 
thus , we required at least 10 060 non - attenders per group in total ( corresponding to approximately 50 300 women invited to first screening appointment in the two groups )  . 
we asked participating centres to recruit substantially more women than this number as a failsafe measure . the difference in participation between the two groups was compared with poisson regression for the primary and key secondary endpoints , offset by the total numbers of invitees . 
we also did prespecified subgroup analyses by prevalent or incident screen status , by time since last attended screen , and by the 2010 index of multiple deprivation ( imd , based on a womans postcode ) .10 national quintiles of imd were used . 
primary analysis and subgroup analyses were by intention to treat , so that women who received the wrong type of letter for their trial group were retained in the analysis as if they had received the correct letter . 
other women who were potentially excludable but were kept in the intention - to - treat analysis were those who were being screened at the time of extraction of the dataset , who were permanently or temporarily under care , who died , who moved away , who were not known at their recorded address , who attended for screening but for some reason were not screened , who had been recently screened , or whose reason for attendance or nonattendance was missing or coded as other . 
these potentially excludable women were more likely to be identified in the intervention group than in the control group , since the offer of a timed appointment was more likely to prompt the invitee to inform the service that she had moved away or had already been recently screened . 
this trial is registered with barts health , number 009304qm . role of the funding source the department of health policy research programme was given the opportunity to comment on this report before submission for publication . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results the dataset received from the six screening centres had 33 146 records of women invited for screening at different times between june 2 , 2014 , and sept 30 , 2015 , who did not attend their first appointment ( see appendix p 3 for details of recruitment by centre )  . 
women were followed up for more than 180 days after their episode in the current round of screening was opened , and the trial was ended when we estimated that the number of women recruited was larger than the one required by our power calculations . 
7092 ( 21% ) of the 33 146 records were excluded after randomisation because of the reasons stated in the methodseg , ineligible age or date of invitation , missing attendance record , or multiple records for the same woman ( 3520 in the intervention group vs 3572 in the control group ; figure )  . 
 of the remaining 26 054 women , 12 807 ( 49% ) had been randomly assigned to receive the intervention of a second timed appointment letter , and 13 247 ( 51% ) to receive an open invitation letter . 
most women in both groups were younger than 60 years of age and came from more deprived socioeconomic areas ( imd quintiles 1 and 2 ; table 1 )  . 586 ( 5% ) of 12 807 women in the intervention group and 52 ( < 1% ) of 13 247 women in the control group received the incorrect invitation letter for their group but were still included in the intention - to - treat analysis as if they had received the correct letter . 
455 ( 4% ) women in the intervention group and 119 ( < 1% ) women in the control group were judged to be potentially excludable , because of the nature of the intervention ( as noted in the methods section )  . 
the majority of these women were either recently screened and so invited in error ( 121 [ 21% ] for non - attendance of 574 ) , had missing reason 33 146 records of non - attenders receiving second invitation letters 16 327 records of women with odd sx numbers randomly assigned to timed appointment ( intervention ) 16 819 records of women with even sx numbers randomly assigned to an open invitation letter ( control ) 2482 outside screening range 2551 outside screening range 110 duplicates for the same 146 duplicates for the same ( 5070 years ) woman 3520 records excluded * attendance dates 147 duplicates for the same woman in the same batch 867 outside study period 34 with incongruences in ( 5070 years ) woman 3572 records excluded * attendance dates 54 duplicates for the same woman in the same batch 958 outside study period 8 with incongruences in 44 with missing date of 24 with missing date of 12 807 women analysed 13 247 women analysed figure : trial profile sx = a sequential unique identifier of each woman within the nhs breast screening programme . 
 * 2010 index of multiple deprivation ( imd ) from most deprived to most affluent . table 1 : characteristics of study groups intervention group ( n = 12 807 ) control group ( n = 13 247 ) absolute difference in attendance rr ( 95% ci ) p value 2861 ( 22% ) 1632 ( 12% ) 181 ( 170193 ) < 00001 3054 ( 24% ) 1784 ( 13% ) 177 ( 167188 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened data are number who participated ( % ) unless otherwise stated . 
percentages have been rounded up . table 2 : participation at second invitation for all women in the trial ( 162 [ 28% ] ) , or were not known to be or no longer living at the address held ( 194 [ 34% ] )  . 
these women were also retained in our intention - to - treat analyses . the in total , 4493 ( 17% ) of 26 054 women participated in breast cancer screening within 90 days of the date of their first offered appointment . 
a significantly higher intervention group proportion of women participated within 90 days than did women in the control group ( 2861 [ 22% ] of 12 807 vs 1632 [ 12% ] of 13 247 ; rr 181 [ 95% ci 170193 ] , p < 00001 ; table 2 )  . 
a higher proportion of women in the intervention group than in the control group also met the secondary endpoint of participation within 180 days of the screening episode being opened ( rr 177 [ 95% ci 167188 ] , p < 00001 )  . 
 similar results were obtained in a post - hoc per - protocol analysis and an analysis excluding the women deemed potentially excludable ( data not shown )  . overall , 12 817 ( 49% ) of 26 054 women were offered a prevalent screen ( 6300 in the intervention group vs 6517 in the control group ) and 13 237 ( 51% ) women were offered an incident screen ( 6507 in the intervention group vs 6730 in the control group )  . 
to take into account the fact that the prevalent screen includes women who have been invited before but have never attended , we first analysed younger women in the prevalent round ( ie , those aged 5052 years )  . 
in this subgroup , participation within 90 days of the first offered appointment was significantly greater for women in the intervention group than in the control group ( table 3 ) ; participation within 180 days of the episode being opened supported this result . 
although numbers were small , participation at second invitation was still significantly higher in the intervention group than in the control group ( table 3 )  . participation data for incident screen women aged 5370 years who had attended any time previously are shown in table 4 by time since last attended screen before the date of the first offered appointment for this screening episode . 
age intervals were adjusted accordingly ( eg , only women aged 5670 years were included in the group who last attended their screening 69 years before their first offered appointment )  . 
despite numbers of women participating diminishing with increasing time since last attendance , all results were significantly in favour of the intervention , even for women who had attended previously but 9 years or more before their first offered appointment ( table 4 )  . 
for women who had last attended 13 years previously , the expected proportion of women participating in screening within 180 days in the intervention group if there had been no effect of the intervention is 32% ( attendance in the control group ) of 2853 ( number invited in the intervention group , n = 912 )  . 
 therefore , the effect of 2853 second timed appointments was generating 495 ( ie , 1407 [ the number of attendees in the intervention group ] 912 [ the number expected of attendees ] ) attended screens . 
 the timed appointments required per additional participant are six , 15 , and 26 for women whose last attendance was 36 years , 69 years , and 9 or more years before their current first offered appointment , respectively , calculated as for those attending 13 years previously . corresponding numbers of second formal tests for heterogeneity of the effect of the intervention by prevalent or incident status were significant ( p < 00001 for participation within 90 days of the first offered appointment and within 180 days of the episode being opened )  . 
although the relative effects are larger in the prevalent screen women , the absolute differences in participation are larger in the incident screen women ( tables 3 and 4 )  . 976 vol 18 july 2017 articles intervention group control group rr ( 95% ci ) p value absolute difference in attendance 5052 years number invited participation in screening 5370 years number invited participation in screening 2017 2072 4283 4445 within 90 days of first offered appointment within 180 days of episode opened 347 ( 17% ) 369 ( 18% ) 147 ( 7% ) 163 ( 8% ) 242 ( 199295 ) 233 ( 193280 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 283 ( 7% ) 307 ( 7% ) 82 ( 2% ) 97 ( 2% ) 358 ( 280458 ) 328 ( 261413 ) < 00001 < 00001 data are number who participated ( % ) unless otherwise stated . 
percentages for the difference in attendance have been rounded up . table 3 : participation at second invitation for prevalent screen women , by age group intervention group attendance control group absolute difference in rr ( 95% ci ) p value attended any time previously number invited participation in screening 6507 6730 aged 5170 years who attended 1 to < 3 years previously number invited participation in screening 2853 2992 aged 5370 years who attended 3 to < 6 years previously number invited participation in screening 1633 1638 aged 5670 years who attended 6 to < 9 years previously number invited participation in screening aged 5970 years who attended 9 years previously number invited participation in screening within 90 days of first offered appointment 2231 ( 34% ) 1403 ( 21% ) within 180 days of episode opened 2378 ( 37% ) 1524 ( 23% ) 164 ( 153178 ) < 00001 161 ( 151173 ) < 00001 within 90 days of first offered appointment 1307 ( 46% ) 876 ( 29% ) within 180 days of episode opened 1407 ( 49% ) 956 ( 32% ) 156 ( 143171 ) < 00001 154 ( 142168 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened 568 ( 35% ) 590 ( 36% ) 306 ( 19% ) 327 ( 20% ) 186 ( 162214 ) < 00001 181 ( 158208 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened 71 ( 13% ) 76 ( 14% ) 39 ( 7% ) 45 ( 8% ) 200 ( 135297 ) < 00001 186 ( 128269 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened 35 ( 7% ) 37 ( 8% ) 16 ( 4% ) 18 ( 4% ) 210 ( 116381 ) 198 ( 112348 ) 001 002 data are number who participated ( % ) unless otherwise stated . 
percentages for the difference in attendance have been rounded up . table 4 : participation at second invitation for incident screen women , overall and by time since last attendance results did not vary substantially by age group ( data not shown )  . 
the first two quintiles ( 1 and 2 ) , corresponding to the most deprived populations , have higher rrs than the other quintiles for participation within 90 days of the first offered appointment and participation within 180 days of the episode being opened . 
results were highly significant in all quintiles ( p < 00001 in all cases )  . vol 18 july 2017 articles intervention group control group rr ( 95% ci ) p value absolute difference in attendance imd quintile 1 ( most deprived ) number invited participation in screening 3395 3623 within 90 days of first offered appointment within 180 days of episode opened 639 ( 19% ) 682 ( 20% ) 353 ( 10% ) 386 ( 11% ) 193 ( 169220 ) 189 ( 166214 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 768 ( 21% ) 825 ( 23% ) 398 ( 11% ) 434 ( 12% ) 196 ( 173222 ) 193 ( 171217 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 686 ( 24% ) 734 ( 26% ) 402 ( 13% ) 442 ( 15% ) 177 ( 156201 ) 173 ( 153195 ) < 00001 < 00001 imd quintile 2 number invited participation in screening imd quintile 3 number invited participation in screening imd quintile 4 number invited participation in screening within 90 days of first offered appointment within 180 days of episode opened imd quintile 5 ( least deprived ) number invited participation in screening 3645 3703 2864 2978 1946 2028 488 ( 25% ) 519 ( 27% ) 297 ( 15% ) 324 ( 16% ) 171 ( 148198 ) 167 ( 145192 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 277 ( 29% ) 290 ( 31% ) 178 ( 20% ) 194 ( 22% ) 148 ( 122179 ) 142 ( 118171 ) < 00001 < 00001 data are number who participated ( % ) unless otherwise stated . 
percentages fhave been rounded up . table 5 : participation at second invitation for all national imd quintiles ( from most to least deprived ) in our post - hoc exploratory analyses , the intervention significantly increased participation at all study sites ( p < 00001 in all centres ; appendix p 2 ) compared with that in the control group . 
the effect of the intervention was highest in southeast london ( rr for participation within 90 days of the first offered appointment 227 [ 95% ci 190272 ] ) , which had the highest proportion of women in the two most deprived imd quintiles ( 3249 [ 87% ] of 3738 ) , and only 53 ( 1% ) women in the two most affluent quintiles . 
by contrast , the effect of the intervention was smallest in plymouth ( rr 155 [ 95% ci 136177 ] ) , where 3595 ( 50% ) of 7190 women were in the two most deprived imd quintiles and 1706 ( 24% ) were in the two most affluent quintiles . discussion in this study , the intervention of inviting non - attenders of breast cancer screening to a second appointment with a fixed date and time caused an absolute increase in participation of 103% compared with an open invitation , which would translate to an increase in participation of 3% , since around 30% of invitees to a first appointment were non - attenders.1 most women included in our analysis were younger than 60 years of age and came from more deprived socioeconomic areas . a limitation of this study was that more than 20% of women were excluded after randomisation . 
we have been unable to identify a systematic factor or staff action that could have caused this imbalance , although centres with more error codes for the sending of the wrong letter were also those with the larger imbalances between the 978 vol 18 july 2017 articles sizes of the two groups . 
although nearly twice as many women in the intervention group than the control group participated in screening at second intention - to - treat analysis led to more diluted results than less statistically cautious approaches , the improvement in participation in the intervention group was still substantial , as shown by our primary analysis . 
the greater effect at prevalent screen than incident screen is important , since a stronger decline in participation over time has been reported at first invitation than at subsequent invitations.1 the universal adoption of second timed appointments for non - attenders at first invitation could go some way to rectifying this trend . the practice of second evidence at the ecological and individual level from europe and north america suggests that socioeconomic deprivation , often in conjunction with specific ethnicity , is strongly associated with non - participation in breast cancer screening.1116 transport issues and difficulties in getting to the screening appointment are cited as reasons for non - participation.12 , 14 further detailed surveys of nonparticipants are needed to improve our understanding of the barriers to participation . 
thus , timed appointments for non - attenders could address in part the the breast socioeconomic gradient screening service.2 , 3 at the very least , this practice should not exacerbate the proble this gradient needs to be addressed because the clinical stage of presentation tends to be later for women of lower socioeconomic status than for women of higher status , and is a factor that contributes to worse treatment outcomes.11 arguably , a key factor responsible for women not attending their breast screening invitation might be car ownership , which is strongly correlated with socioeconomic status and positively associated with breast screening coverage.12 a comparison of car ownership within the same imd quintile between women who responded to their second timed appointment letter and women who did not could be interesting . in delivery of the greatest effect of the intervention was seen in southeast london , which had the highest proportion of women in the two lowest imd quintiles . 
in view of our findings , and the internationally observed socioeconomic gradient in participation in breast cancer screening , 1416 our results could have relevance to other countries with organised screening programmes . in all time - interval categories into which women were divided , the proportions of women who participated in screening increased in the intervention group versus the control by around the same relative factor for second timed appointments and there did not seem to be a trend between time since last screen and efficacy of the intervention , by contrast with findings reported by stead and colleagues.6 however , the absolute effect declined with time since last attended screen , as has been reported previously , and reflecting generally similar or larger relative effects but smaller absolute effects in those with a lower baseline participation . 
the number of second timed appointment letters that need to be offered per additional participant increases for women whose last attendance at breast cancer screening was more than 6 years before their current first offered appointment . 
of course , fewer second timed appointment letters have to be issued than open letters per participant ; however , reservation of the appointment time is the call on resources . the economic implications of compulsorily extending the intervention to all women in the breast cancer screening programme will have to be examined before such a change in policy is made , because allocating time slots for fixed timed appointments has a cost in terms of resources . 
in most cases , overbooking for screening appointments is advised to minimise the waste from unused slots ; our results suggest that increasing the overbooking ratio for second timed appointments for previous non - attenders would be safe . 
however , with the higher variability of the likelihood of participation in the second timed appointments , it would be prudent to mix small numbers of these within sessions with a majority of first offered appointments . 
 offering second timed appointments only to those who have attended in the 6 years previous to their first offered appointment might be a cost - effective approach , since it leads to fewer wasted appointments than in those who have not attended for a longer period . 
this strategy , however , raises questions of ethics and equity and should be considered further by the department of health and public health england to determine the appropriate policy for the programme . 
scope also exists for qualitative research into the public acceptability of the policy of second timed appointments . in other countries , such as italy , 17 , 18 fixed appointments rather than open invitations have been associated with improved participation in screening in general , not only for non - attenders . 
other methods that can successfully increase participation in breast cancer screening are text message , 19 , 20 postal , 21 and telephone reminders ; 22 general practitioner endorsement ; 23 , 24 and the possibility to change appointments to out - of - office hours.8 second for non - attenders could be timed appointments implemented with these methods ( eg , with the second vol 18 july 2017 articles timed appointment letter offering the opportunity to change to an out - of - hours time slot , or having primary care endorsement ) and other interventions to improve delivery to all eligible women , with the ultimate goal of improving early detection of breast cancer in england and worldwide . contributors pca contributed to study design , data analysis , data interpretation , and drafting the report . 
he was responsible jointly with jp for study concept and design , supervised the statistical analysis and data interpretation , and contributed to drafting the report . declaration of interests we declare no competing interests . acknowledgments we thank all the staff who worked at the screening centres that took part to this project . 
swd and rm contributed to this study as part of the programme of the policy research unit in cancer awareness , screening and early diagnosis , which receives funding for a research programme from the department of health policy research programme . 
this programme is a collaboration between researchers from seven institutions ( queen mary university of london , university college london , kings college london , london school of hygiene & tropical medicine , hull york medical school , durham university , and peninsula medical school )  . articles adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study pippa g corrie , andrea marshall , janet a dunn , mark r middleton , paul d nathan , martin gore , neville davidson , steve nicholson , charles g kelly , maria marples , sarah j danson , ernest marshall , stephen j houston , ruth e board , ashita m waterston , jenny p nobes , mark harries , satish kumar , gemma young , paul lorigan summary background bevacizumab , a monoclonal antibody that targets vegf , has shown restricted activity in patients with advanced melanoma . 
we report results from the preplanned interim analysis . methods we did a multicentre , open - label , randomised controlled phase 3 trial at 48 centres in the uk between july 18 , 2007 , and march 29 , 2012 . 
patients aged 16 years or older with american joint committee on cancer stage ( ajcc ) stage iib , iic , and iii cutaneous melanoma were randomly allocated ( 1 : 1 ) , via a central , computer - based minimisation procedure , to receive intravenous bevacizumab 75 mg / kg , every 3 weeks for 1 year , or to observation . 
this trial is registered as an international standardised randomised controlled trial , number isrctn81261306 . findings 1343 patients were randomised to either the bevacizumab group ( n = 671 ) or the observation group ( n = 672 )  . 
at the time of interim analysis , 286 ( 21% ) of 1343 enrolled patients had died : 140 ( 21% ) of 671 patients in the bevacizumab group , and 146 ( 22% ) of 672 patients in the observation group . 
we noted no signi cant di erence in overall survival between treatment groups ( hazard ratio [ hr ] 097 , 95% ci 078122 ; p = 076 ) ; this nding persisted after adjustment for strati cation variables ( hr 103 ; 95% ci 081129 ; p = 083 )  . 
180 grade 3 or 4 adverse events were recorded in 101 ( 15% ) of 671 patients in the bevacizumab group , and 36 ( 5% ) of 672 patients in the observation group . 
there was an improvement in disease - free interval for patients in the bevacizumab group compared with those in the observation group ( hr 083 , 95% ci 070098 , p = 003 ) , but no signi cant di erence between groups for distant - metastasis - free interval ( hr 088 , 95% ci 073106 , p = 018 )  . 
no signi cant di erences were noted between treatment groups in the standardised area under the curve for any of the quality - of - life scales over 36 months . 
three adverse drug reactions were regarded as both serious and unexpected : one patient had optic neuritis after the rst bevacizumab infusion , a second patient had persistent erectile dysfunction , and a third patient died of a haemopericardium after receiving two bevacizumab infusions and was later identi ed to have had signi cant predisposing cardiovascular risk factors . interpretation bevacizumab has promising tolerability . 
fewer than 50% of patients with resected locoregional melanoma survive to 5 years.1 adjuvant trials assessing interferon alfa have shown that the drug delays melanoma recurrence , but has only a small overall survival bene t.2 the low survival bene t and high treatment - related toxic e ects associated with interferon alfa mean that no internationally agreed standard adjuvant treatment is available for patients with high - risk melanoma . vol 15 may 2014 lancet oncol 2014 ; 15 : 62030 published online april 16 , 2014 s1470 - 2045 ( 14 ) 70110 - x this online publication has been corrected . 
eligible patients were at least 16 years old , with histological con rmation of completely resected american joint committee on cancer stage iib ( t3bn0m0 and t4an0m0 ) , iic ( t4bn0m0 ) , or iii ( txn13m0 ) cutaneous melanoma . 
inclusion criteria were an eastern cooperative oncology group ( ecog ) performance status of 01 ; a life expectancy of 6 months or more ; and adequate haematological , liver , and renal function . 
exclusion criteria were evidence of distant or non - regional lymph - node metastases ( established by ct or mri scanning of the body and head within 8 weeks of randomisation ) , incomplete resection of melanoma , or adjuvant radiotherapy that was ongoing at randomisation . 
 treatment assignment could not take place within 4 weeks of surgery or in the presence of unhealed wounds , but had to be within 12 weeks of a patients latest surgery for melanoma . 
because this interim analysis was preplanned , and in view of the absence of an international standard adjuvant therapy for melanoma , the independent data monitoring committee supported publication of these results in advance of the nal analysis anticipated in 2017 . randomisation and masking eligible patients were randomly assigned centrally in a 1 : 1 ratio using a computer - based minimisation algo rithm , to receive either adjuvant bevacizumab or standard observation . 
randomisation was strati ed by breslow thickness of the primary tumour , n stage according to ajcc staging criteria , 1 ulceration of the primary tumour ( absent , present , or unknown ) , and patient sex . 
this was an openlabelled trial and therefore participants , investigators , and trial sta were not masked to group allocation . procedures for patients randomly assigned to bevacizumab , 75 mg / kg was given via 30 min intravenous infusion once every 3 weeks for 1 calendar year ( maximum 17 infusions ) , or until disease recurred . 
if a patient required any further dose interruptions , treatment was discontinued . department , royal preston hospital , preston , uk ( re board phd ) ; clinical trials unit , beatson west of scotland cancer centre , glasgow , uk ( am waterston phd ) ; clinical oncology , norfolk and norwich university hospital , norwich , uk ( jp nobes frcr ) ; guys and st thomas hospital , london , uk ( m harries phd ) ; velindre cancer centre , cardi , uk ( s kumar md ) ; cambridge cancer trials centre / cambridge clinical trials unitcancer theme , addenbrookes hospital , cambridge , uk ( g young mphil ) ; and deptartment of medical oncology , christie hospital , manchester , uk ( p lorigan md ) correspondence to : dr pippa g corrie , oncology centre , cambridge university hospitals nhs foundation trust 3394 participants assessed for eligibility 2051 excluded 1357 did not meet inclusion criteria 694 declined to participate 1343 randomised 671 assigned to bevacizumab 672 assigned to observation 652 received intervention 1 local recurrence 4 wound healing complications or surgical 19 did not receive intervention 10 because of patient choice intervention 1 case of cellulitis 1 case of thrombus 1 case of hypertension 1 diagnosis of central retinal vein occlusion 119 because of recurrence 112 because of unacceptable toxic eects 28 because of patient choice 1 patient died 291 discontinued early 10 cases of unacceptable dose interruption due to surgical intervention or investigation 7 wound healing complications 12 unplanned discontinuations 2 had a new second malignancy 671 included in primary analysis 592 analysed for health - related quality of life * 672 included in primary analysis 623 analysed for health - related quality of life * figure 1 : trial pro le hr = hazard ratio . 
adverse events reported during the rst year by patients in the observation group and for 28 days after the last bevacizumab infusion for those the bevacizumab group were recorded according to the national cancer institute common terminology criteria for adverse events ( ctcae ) , version 3.0. 
treatment options therapy ; surgery ; radiotherapy , dependent on type of recurrence ; and patient choice . included systemic we ascertained braf mutation status in archived tumour tissue with a cobas4800 ( roche diagnostics , west sussex , uk ) test or by pyrosequencing . 
nras status was not established for braf mutant tumours , because nras and braf mutations are generally mutually exclusive . outcomes the primary endpoint of the trial was overall survival , which we de ned as the time from date of randomisation until date of death from any cause , or censored at the last known date alive . 
disease - free interval was de ned as the time from the date of randomisation until the date of rst ( including distant and locoregional recurrence ) , or date of death due to melanoma . 
distant - metastasis - free interval was de ned as the time from the date of randomisation until the date of rst distant recurrent disease , or date of death due to melanoma . recurrence tumour statistical analysis patients who withdrew consent for further follow - up were included in the analysis , but censored at the time of withdrawal . 
a sample size of 1320 patients ( 660 patients per group ) was needed to detect an absolute increase in 5 year overall survival from 40% to 48% , with 85% power and a 5% signi cance level , which equates to a hazard ratio ( hr ) of 080 . 
hrs were calculated for prognostic subgroups and a hr plot constructed.16 multivariable cox - regression models were used to adjust the treatment e ect for strati cation variables , to assess the independent predictors of overall survival and disease - free interval , and to assess treatment interaction with tumour mutation status and whether hypertension , tted as a time - dependent covariate , a ected disease - free interval . 
quality - of - life data were analysed by standardised and compared across trial groups with wilcoxon rank - sum tests . area - under - the - curve analysis18 reported p values are two - sided . 
this trial is registered as an international standardised randomised controlled trial , number isrctn 81261306 . results 1343 patients were randomly assigned to either the bevacizumab group ( n = 671 ) or the observation group ( n = 672 ; gure 1 )  . 
975 ( 73% ) patients had resected ajcc stage iii melanoma , 515 ( 38% ) patients had an ulcerated primary tumour , and 440 ( 32% ) patients underwent sentinel lymph - node biopsy . 
368 ( 27% ) patients had no known nodal involvement ( n0 and nx ) , 281 ( 21% ) had microscopic lymph - node involvement ( n1a and n2a ) , and 694 ( 52% ) had macroscopic lymphnode involvement . 
we subsequently identi ed 11 ( 1% ) of enrolled patients as ineligible ; three in the bevacizumab group and eight in the observation group : ve had metastatic disease , ve had incomplete surgery , and one had stage iia melanoma . 
am had full access to all the data in the study and the corresponding author had nal responsibility for the decision to submit for publication . number at risk bevacizumab observation hr 097 , 95% ci 078122 ; p = 076 articles e ect causing treatment discontinuation was hypertension in 36 ( 5% ) patients . 
the main reasons for delay were for planned drug holidays or toxic e ects ( data not shown )  . 286 ( 21% ) of 1343 enrolled patients had died at the time of the interim analysis ( 140 [ 21% ] of 671 patients in the bevacizumab group and 146 [ 22% ] of 672 patients in the observation group )  . 
we noted no signi cant di erence in overall survival between treatment groups ( gure 2 ) ; this nding persisted after adjustment for strati cation variables ( hr 103 ; 95% ci 081129 ; p = 083 )  . 
multivariable analysis identi ed disease stage , ecog performance status , and primary melanoma ulceration as independent overall survival disease stage iii ( n1a and n2a ) iii ( other n ) ecog performance status ulceration unknown disease - free interval disease stage iii ( n1a and n2a ) iii ( other n ) breslow thickness ( mm ) 20 > 24 unknown trial group treatment observation ecog performance status n ( % ; n = 1343 ) number of events ( % ) hazard ratio ( 95% ci ) p value 368 ( 27% ) 281 ( 21% ) 694 ( 52% ) 45 ( 12% ) 39 ( 14% ) 100 142 ( 091221 ) 202 ( 29% ) 305 ( 216432 ) 1194 ( 89% ) 235 ( 20% ) 054 ( 039073 ) 147 ( 11% ) 50 ( 34% ) 100 515 ( 38% ) 632 ( 47% ) 196 ( 15% ) 109 ( 21% ) 121 ( 19% ) 100 068 ( 052089 ) 56 ( 29% ) 075 ( 053106 ) 368 ( 27% ) 281 ( 21% ) 694 ( 52% ) 399 ( 30% ) 407 ( 30% ) 437 ( 33% ) 100 ( 7% ) 118 ( 32% ) 76 ( 27% ) 370 ( 53% ) 100 112 ( 082152 ) 278 ( 220351 ) 160 ( 40% ) 100 165 ( 41% ) 200 ( 46% ) 125 ( 101157 ) 174 ( 138220 ) 39 ( 39% ) 084 ( 059119 ) 671 ( 50% ) 672 ( 50% ) 264 ( 39% ) 300 ( 45% ) 083 ( 070098 ) 100 1194 ( 89% ) 490 ( 41% ) 130 ( 102167 ) 147 ( 11% ) 73 ( 50% ) 100 < 00001 < 00001 002 < 00001 < 00001 003 004 ecog = eastern cooperative oncology group . table 2 : results from the multivariate analyses for overall survival and disease - free interval predictors of overall survival ( table 2 )  . 
the treatment e ect remained non - signi cant for overall survival after adjustment for the three prognostic variables ( hr 102 , 95% 081128 ; p = 089 )  . we recorded an improvement in disease - free interval for patients in the bevacizumab group compared with those in the observation group ( gure 3 )  . 
multivariable analysis identi ed disease stage , breslow the primary melanoma , trial group , and ecog performance status as independent predictors of disease - free interval ( table 2 )  . 
results from the analysis of disease - free interval were unchanged in a sensitivity analysis excluding the ineligible patients . thickness of braf status was available for 645 ( 48% ) patients ( table 1 )  . 
su cient material remained to undertake nras testing 239 ( 68% ) of 354 patients with braf wild - type ; 106 ( 44% ) of these patients had a mutation at codon 61 . 
the interaction between treatment and braf status was not signi cant ( p = 010 ) ; however , in patients with braf mutant tumours , we noted an improvement in the disease - free interval in those given bevacizumab ( gure 3 )  . 
diseasefree interval did not di er signi cantly between treatment groups in the wild - type braf population ( gure 3 )  . 180 grade 3 or 4 adverse events were recorded in 101 ( 15% ) of 671 patients in the bevacizumab group and 36 ( 5% ) of 672 patients in the observation group . 
 216 ( 32% ) patients had hypertension in the bevacizumab the disorder was generally group manageable ; we recorded grade 3 or 4 hypertension in 41 ( 6% ) patients ( table 4 )  . 
hypertension did not signi cantly a ect disease - free interval ( hr 085 , 95% ci 067109 ; p = 020 ) after adjustment for trial group . ( table 4 ) , but three adverse drug reactions were regarded as both serious and unexpected . 
 1215 ( 90% ) of 1343 patients returned at least two forms 624 vol 15 may 2014 articles bevacizumab observation and were included in the analyses : 592 ( 88% ) of 671 patients in the bevacizumab group and 623 ( 93% ) of 672 patients in the observation group . 
after bonferroni adjustment for multiple testing , no signi cant di erences were noted between treatment groups in the standardised area under the curve for any of the quality - of - life scales over 36 months ( table 5 )  . discussion our ndings show an improvement in disease - free interval with bevacizumab in patients with resected melanoma at high risk of recurrence as compared with observation alone . 
clearly , it will be important to ascertain whether this treatment e ect ultimately translates into a bene t in overall survival at nal analysis , which is follow - up driven and planned for when all patients have been on study for a minimum of 5 years , at which time 736 events are anticipated . 
the conditional power for futility of the primary outcome of overall survival at this interim analysis was 35% . to our knowledge , avast - m is one of the largest adjuvant melanoma trials and the largest bevacizumab monotherapy study ever undertaken ( panel )  . 
 patients and regulatory agencies increasingly value relapse - free survival as a primary endpoint in this setting , which is justi ed now that systemic therapies have been shown to improve overall survival in advanced disease.1921 however , when we started avast - m bevacizumab was a new drug with signi cant toxic e ects ( albeit reported mainly in combination with cytotoxic chemotherapy ) , and so we felt that a bene t in overall survival would need to be shown to change clinical practice . 
however , diseasefree interval in this trial could be indiciative of relapsefree survival , because only seven additional deaths from other causes without recurrence would have been included in an analysis of relapse - free survival ; these inclusions would not have changed the results from those reported for disease - free interval . identify the most frequently used adjuvant melanoma treatment worldwide is interferon alfa . 
 trials assessing di erent doses and formulations of interferon alfa have not identi ed the optimum adjuvant regimen this treatment is recognised to be associated with substantial toxic e ects , including liver dysfunction , fatigue , and depression.22 , 23 other immunotherapeutic strategies , including several vaccines , have been rigorously tested in patients with melanoma , with disappointing results overall.24 this outcome is exempli ed by the results of the derma randomised trial , in which a mage a3 vaccine did not improve relapse - free survival ( its rst coprimary endpoint ) in patients with resected stage iii melanoma expressing the mage a3 antigen.25 our results suggest that the extent of patient bene t o ered with bevacizumab might be similar to that with interferon alfa for the endpoint of relapse - free survival ( hr for interferon alfa 082 , 95% ci 077087 ) , but the overall survival bene t ( 089 , 082096 ) on ifterferon alfa was not noted with bevacizumab.2 at this interim analysis , few patients had received immunotherapy or targeted therapy at relapse , and the most common intervention was surgery . 
this nding is consistent with the high rate of locoregional recurrence as a result of the fairly low use of sentinel node biopsy and the inclusion of high risk primary tumours , together with the scarcity of active systemic therapy options 626 vol 15 may 2014 articles available until more recently . 
the e ect of subsequent treatments at relapse on overall survival is likely to be small at this time point , but will be of greater importance in the future . 
even so , the delay in melanoma recurrence noted with adjuvant bevacizumab in this trial might be clinically relevant . bevacizumab monotherapy seems to be well tolerated : grade 3 or 4 adverse events associated with bevacizumab were interferon , depending on the dose used , although cross - trial comparisons should be made with caution.22 , 23 those reported with fewer than interruptions around surgical there was no obvious safety signal associated with surgical interventions or haemorrhage to account for patients early discontinuation . 
the protocol speci ed interventions , dose requiring 28 days free from drug administration either side of any procedure , and preventing drug administration in the presence of any unhealed wound . 
drugassociated complications in wound healing seem to be negligible , and only a few patients failed to complete planned treatment due to unacceptable delays in wound healing , suggesting that , in routine clinical practice , withholding treatment in such circumstances need not be so stringent . 
withdrawal rates will be a ected by the duration of intended treatment , but low - level chronic side - e ects in an otherwise t population might account for patients electing to stop prematurely and this should be considered in future adjuvant trial designs . 
a placebocontrolled trial might have improved patient willingness to remain on treatment for longer , but the additional cost of a placebo would have been prohibitive in this charityfunded trial . multivariate analyses of disease - free interval and overall survival were undertaken to explore whether some subsets of patients were more likely to bene t from therapy than others . 
disease stage and breslow thickness were the most signi cant predictors of disease - free interval ; disease stage and ecog performance status were the most signi cant predictors of overall survival . 
a tenth of patients had an ecog performance status score of 1 on trial entry ; the reason for their poor outcome is not apparent , but will be assessed fully in the nal analysis . avast - m includes a prespeci ed translational study , aimed at identifying predictive and prognostic biomarkers . 
firm conclusions about whether bevacizumab might result in a longer disease - free interval for the subgroup of patients with braf mutant tumours cannot yet be made , but further analysis will be including multivariate analyses undertaken at the nal analysis . 
investigation into the biological basis for this initially unexpected nding is ongoing , but it is consistent with emerging evidence of the map kinase pathway playing a role in the control of vegf expression . 
 * an additional three patients ( one in the bevacizumab group and two in the observation group ) who died of melanoma before details of their recurrence being reported are included in the analyses of disease - free interval . 
adverse events are recorded for all patients who had an event of grade 3 or 4 severity and include any other adverse events that were recorded in 10% or more patients . 
if this mechanism applies to melanomas in human beings , it would provide a basis for the selection of patients for bevacizumab therapy , and a rationale for future potential combination regimens . trials three testing adjuvant bevacizumab combination with chemotherapy have been reported in patients with colon27 , 28 and breast cancer.29 all three trials had disease - free survival as the primary endpoint , and none identi ed any improvement . 
both immunological and angiogenic biomarkers are now being explored with tumour and blood samples collected from most patients recruited to the avast - m trial . 813 ( 681896 ) 819 ( 688911 ) 026 data are median ( iqr ) , unless otherwise indicated . 
p values less than 0003 would be signi cant after adjustment with bonferroni correction for multiple testing . table 5 : quality of life standardised area - under - curve analyse 628 vol 15 may 2014 articles panel : research in context systematic review an international standard adjuvant therapy for patients at risk of melanoma recurrence has not yet been established . 
 we searched pubmed for clinical trials published in english between jan 1 , 2000 and feb 1 , 2014 , assessing systemic therapy speci cally in melanoma , with the search terms melanoma and adjuvant . 
inhibition of angiogenesis as an adjuvant strategy has not previously been tested in melanoma patients . interpretation to our knowledge , avast - m is the rst phase 3 trial assessing bevacizumab as adjuvant therapy for melanoma and the largest bevacizumab monotherapy every undertaken . 
longer follow - up is needed to identify the e ect of bevacizumab on overall survival at 5 years . e ective treatment to prevent melanoma relapse remains an unmet need . 
the results of these trials , alongside the nal results of the avast - m trial , will have a key role in identifying future adjuvant strategies for this disease . contributors pc was the chief investigator , responsible for the trial design , trial management , data interpretation , and preparation of the manuscript . 
 am was the trial statistician who analysed the data , created the tables and gures , and contributed to the trial design , trial management , data interpretation , and preparation of the manuscript . 
all authors participated in the revision and nalisation of the manuscript . declaration of interests pc has received nonnancial support from f ho man la roche , grants from cancer research uk during the study , and personal fees and nonnancial support from f ho man la roche outside the submitted work . 
 mrm has received grants from cancer research uk during the study , personal fees from amgen , grants and personal fees from f ho man la roche , grants from astrazeneca , grants and personal fees from glaxosmithkline , institution study fees from novartis , institution study fees from astellas , institution study fees from millenium , institution study fees from immunocore , personal fees and institution study fees from bristol myers squibb , institution study fees from vertex , personal fees and institution study fees from eisai , institution study fees from abbott , institution study fees from clovis , institution study fees from p zer , institution study fees from merck , outside the submitted work . 
pl reports being a remunerated consultant to f ho man la roche for unrelated product and support for travel from f ho man la roche , outside the submitted work . 
all other authors declare that they have no competing interests . acknowledgments we thank all the patients who participated in the avast - m trial ; all investigators and their research teams ; colleagues working in regional cancer networks responsible for referring patients ; and the avast - m trial coordination team and the national cancer research institute melanoma clinical studies group for their adoption of the trial and support . 
national institutes for health research funding to the national clinical research network , biomedical research centres and experimental cancer medicine centres contributed to the undertaking of this trial in various sites . 
 bevacizumab was provided free of charge by f ho man la roche , basel , switzerland . editorial for our earlier editorial on direct - to - consumer genetic testing see lancet oncol 2008 ; 9 : 1113 black - box warning : direct - to - consumer marketing on nov 22 , 2013 , the us food and drug administration ( fda ) ordered the company 23andme to immediately discontinue sale and marketing of its saliva collection kit and personal genome service , stating that it was being marketed without fda approval . 
23andme had recently begun a series of television adverts to market their test , which is billed as providing data on 254 diseases and conditions , including data on carrier status , health risk , and responses to drugs . 
the warning letter stated that the fda had received no assurances from the company that the personal genome service was analytically or clinically validated for its intended uses , and that the tests could put patients at risk when decisions are made on false positive or negative assessments for high - risk indications . 
for instance , the letter highlighted that a false positive result for a brcarelated risk assessment could lead a patient to undergo intensive prophylactic screening , or other morbidity - inducing actions , while a false negative result could result in a patient failing to recognise an actual risk that might exist . 
in response , 23andme have suspended marketing the product , and halted the provision of health - related results to new customers , although ancestry - related information and raw genetic data will still be provided . chemoprevention , surgery , these concerns are the crux of the issue with publicly available genetic tests . 
while genetic testing has a role in the clinic , the provision of complex genetic data to lay individuals , especially without access to expert genetic counselling , is a risky business . 
 further , it is premature to believe that we understand the overall genetic complexity of common diseases to the extent that we can accurately predict whether or not an individual will succumb to that condition in the long run . one must also consider what a consumer can actually do with the results of their genetic tests . 
although in a handful of situationseg , testing positive for brca1 / 2 with a strong family history of brca - related cancerradical steps can be taken to prevent or treat the disease , many conditions do not have such obvious courses of action . 
most frequently , the only possible recommendation for a patient would be to modify diet and lifestyle , but one could argue that this should be done by many people , irrespective of knowledge of their genetics . 
and would knowledge of the risk of an untreatable condition cause long - lasting anxiety , the adoption of a fatalistic attitude to bad news , or use of unproven interventions , perhaps at great personal expense ? as we have noted previously , is the ready availability of such information ethical , when little can be done with it , and could be the source of distress ? is also an instance , 23andmes database currently contains data for 400 000 people . 
 what guarantees does an individual have that this information will not nd its way to health insurers , resulting in in ated premiums or the refusal to grant coverage ? in an unauthorised data protection information issuefor to use inherent many of the fears raised by this particular issue are common to other direct - to - consumer marketed health products . 
 or is it perhaps time to ban outright product - speci c adverts of health - care products aimed directly at the consumer ? the lancet oncology vol 15 january 2014 editorial fertility preservation and consent less than 5% of adults with cancer choose to protect their future fertility by having samples of their gametes frozen before undergoing treatment . 
on march 6 , 2014 , a widow won a high court case in the uk against the human fertilisation and embryology authority ( hfea ) to preserve her dead husbands sperm for future use beyond the statutory period . 
is this decision to appeal callous or fair ? warren brewer put his sperm into storage in april 2005 , before receiving cranial radiation , and consented for this sample to be kept for the statutory 10 years , which expires on april 18 , 2015 . 
in the case , his widow , elizabeth warren , and her legal team proved that brewers intention for use of the sperm was not limited to 10 years , and that the clinic had failed to make the necessary legal provisions . 
in addition , they argued that given warren was in a state of grief ( she had also lost her brother in a fatal road tra c accident just weeks before her husbands death ) , a life - changing decision on whether to have a child should not be forced on to her by a prescriptive timeframe . 
they further evoked the human rights act 1998 , which protects the right to respect an individuals private and family life that the judge interpreted to include the right for a widow to decide to become a parent by her deceased husband . the hfea argued that consent was only granted for the statutory 10 years , and that given further consent could no longer be obtained , there was no case to extend storage for up to 55 years . 
furthermore , they argued that , because the judge con rmed that legal consent was not in place for storage beyond 10 years , the judgment may have implications for other cases in which the sperm providers wishes are less clear . 
this is clearly a very sensitive case : one where both parties agreed that common sense should prevail , that warrens wishes were reasonable , but they must be achieved in a way that does not set a precedence for future abuse of the regulations , hence hfeas , excessively linguistic and technical approach in the interpretation of the law . the increasing number of people being diagnosed with cancer , and the larger proportions of younger patients , suggests the issues raised in this case are likely to become more commonespecially if this case raises awareness about the availability of fertility preservation and more patients start to make use of the services available . 
a formalised amendment to the human fertilisation and embryology act to take in the speci c circumstances surrounding cancer treatment might now be the best option , rather than allowing provisions to evolve haphazardly via precedence and case law . 
an additional legal solution is needed in the warren case to protect warrens rights to make a decision on her own terms and in her own timeframe , whilst protecting the act from abuse . 
with this in mind , the appeal , albeit unfortunate and insensitive , does seem necessary . fertility preservation cancer is an integral part of comprehensive treatment , and a nice recommendation in the uk , but the legal framework should support all eventualities . 
unfortunately , the hard truth is that many patients still die from their cancer , and if their death is at a young age , it is entirely possible that any frozen gametes might be used by their partners in the time after their death . 
 the lancet oncology vol 15 april 2014 correction to lancet oncol 2016 ; 17 : 23442 correction to lancet oncol 2016 ; 17 : e506 shaw at , gandhi l , gadgeel s , et al , on behalf of the study investigators . 
 lancet oncol 2016 ; 17 : e50209the fourth sentence of the biosimilar monoclonal antibodies in oncology section should have read , the primary endpoint , overall response rate , at week 24 was equivalent between groups ( 70% for myl - 1401o vs 64% for trastuzumab ) , and the risk ratio was 109 ( 90% ci 097121 )  . 
this correction has been made to the online version as of march 1 , 2017 . vol 18 march 2017 e134 corrections correction to lancet oncol 2017 ; 18 : e186 addeo a , gyawali b . 
we aimed to compare high - dose melphalan plus salvage asct with cyclophosphamide in patients with relapsed multiple myeloma who had previously undergone asct . methods this multicentre , randomised , open - label , phase 3 study recruited patients aged at least 18 years with multiple myeloma who needed treatment for rst progressive or relapsed disease at least 18 months after a previous asct from 51 centres across the uk . 
before randomisation , eligible patients received bortezomib , doxorubicin , and dexamethasone ( pad ) induction therapy and then underwent peripheral blood stem - cell mobilisation and harvesting if applicable . 
eligible patients ( with adequate stem - cell harvest ) were randomly assigned ( 1 : 1 ) , using an automated telephone randomisation line , to either high - dose melphalan 200 mg / m plus salvage asct or oral cyclophosphamide ( 400mg / m per week for 12 weeks )  . 
 this trial is registered with clinicaltrials.gov , number nct00747877 , and eudract , number 2006 - 005890 - 24 . findings between april 16 , 2008 , and nov 19 , 2012 , 297 patients were registered , of whom 293 received pad reinduction therapy . 
between aug 26 , 2008 , and nov 16 , 2012 , 174 patients with su cient pbscs were randomised to salvage asct ( n = 89 ) or cyclophosphamide ( n = 85 )  . 
after a median follow - up of 31 months ( iqr 1942 ) , median time to progression was signi cantly longer in the salvage asct than in the cyclophosphamide group ( 19 months [ 95% ci 1625 ] vs 11 months [ 912 ] ; hazard ratio 036 [ 95% ci 025053 ] ; p < 00001 )  . 
results of randomised trials comparing high - dose therapy plus asct with conventional chemotherapy have shown that transplantation improves progression - free and overall survival.1 , 2 as a result , the procedure is regarded as the standard of care for patients with newly diagnosed multiple myeloma up to about age 6570 years without substantial comorbidities.35 the incorporation of thalidomide , bortezomib , and lenalidomide into the rst - line management strategy during induction , consolidation , or maintenance therapy has further improved patient outcomes.613 however , for most patients , a cure remains elusive and the disease will eventually relapse . 
thalidomide , bortezomib , and lenalidomide form the mainstay of treatment in combination with steroids and conventional chemotherapy . the use of asct at relapse ( salvage asct ) is an appealing option because of the potential for long - term vol 15 july 2014 lancet oncol 2014 ; 15 : 87485 published online june 17 , 2014 s1470 - 2045 ( 14 ) 70245 - 1 this online publication has been corrected . 
results of several retrospective , registrybased or single - centre analyses investigating the use of salvage asct in the relapse setting after a previous asct have been published , and all suggest a bene t for the repeated use of the procedure.1421 a review22 of available retrospective studies suggests that salvage asct can lead to objective responses in about 65% of patients , with progression - free survival and overall survival reaching 12 months and 32 months , respectively . 
 furthermore , using asct in the relapse setting seems to be associated with an overall treatment - related mortality of less than 5%.14 analyses to identify reasons for the success of salvage asct suggest that the duration of response to the rst asct is crucial.1421 taken together , these analyses point to an important role for salvage asct ; however , until now , a prospective assessment had not been done . on behalf of the uk myeloma forum and the british society of blood and marrow transplantation , we designed the national cancer research institute myeloma x relapse ( intensive ) trial to compare highdose melphalan asct with cyclophosphamide in patients with relapsed multiple myeloma who had previously undergone asct in the rst - line setting . 
the choice of cyclophosphamide as post - induction consolidation for patients in the control group represented an accepted standard of care in the absence of a global standard of care in this setting . 
 salvage plus methods study design and patients in this randomised , multicentre , open - label , parallelgroup , phase 3 trial with an initial single - intervention recruited patients with registration phase , we symptomatic , measurable multiple myeloma from 51 national health service hospitals in england , wales , scotland , and northern ireland . 
patients were eligible for registration if they needed treatment for rst progressive or relapsed disease at least 18 months after a previous asct ( reduced to 12 months in 2011 after the publication of expected bene t14 ) ; needed therapy for relapsed disease ( as de ned by the international myeloma working group [ imwg ] criteria23 ) ; were deemed t by the treating physician to undergo an intensive therapeutic protocol ; and were older than 18 years ( no predetermined upper age limit )  . 
patients who had a complete ( immuno xationnegative ) response therapy but who to rst - line subsequently became immuno xation - positive had to have a greater than 5 g / l absolute increase in paraprotein to be eligible . 
laboratory assessments to establish trialentry eligibility were done within 14 days of registration , with the following tolerance limits : adequate full blood count ( platelet count 350 10 cells per l and absolute neutrophil count 331 10 cells per l ) ; adequate renal function ( creatinine clearance 330 ml / min ) ; adequate hepatobiliary function ( total bilirubin < 2 upper limit of normal [ uln ] and an aspartate aminotransferase alanine aminotransferase ratio of < 25 uln ) ; adequate pulmonary function ( no evidence of a history of pulmonary disease , and carbon monoxide transfer coe cient or di using capacity of the lung for carbon monoxide ( cid : 98 ) of 50% ) ; and adequate cardiac function within 12 weeks before registration ( left ventricular ejection fraction 40% )  . patients were excluded if they had received therapy for their relapsed disease , had an eastern cooperative oncology group performance status of 34 , grade 2 peripheral neuropathy , known resistance to combined bortezomib , doxorubicin , and dexamethasone ( pad ) therapy , or any comorbidity that would preclude highdose chemotherapy . all patients gave written informed consent . 
the study was approved by the national ethics review board ( multicentre research ethics committee , uk ) , institutional review boards of the participating centres , and the competent regulatory authority ( medicines and healthcare products regulatory agency , uk ) , and was undertaken according to the declaration of helsinki and the principles of good clinical practice as espoused in ( clinical trials ) for human use the medicines regulations . 
the trial management group , chaired by gc , veri ed the accuracy and completeness of the data reported and the adherence of the study to the protocol , and jmb vouches for the statistical accuracy of the manuscript . pre - randomisation procedures before randomisation , all eligible patients received reinduction chemotherapy , which consisted of intravenous bortezomib 13 mg / m per day on days 1 , 4 , 8 , and 11 , intravenous doxorubicin 9 mg / m per day on days 14 , and oral dexamethasone 40 mg per day on days 14 , 811 , and 1518 during cycle 1 and days 14 during cycles 24 ( pad )  . 
patients were eligible to progress to next stage if they had received 24 cycles of pad re - induction chemotherapy according to the protocol and had a complete response , partial response , or stable disease following re - induction chemotherapy . patients then underwent peripheral blood stem cell ( pbsc ) mobilisation and harvesting ; however , su cient pbscs were available from their rst - line asct , this procedure was not compulsory . 
the response and time of progression were de ned using the imwg criteria , as per protocol . bone marrow aspirate samples at trial entry and at disease progression were cd138 + selected ( automacs , miltenyi biotec , cologne , germany ) and plasma cell strati ed permuted randomisation and masking eligible patients were randomly assigned on a 1 : 1 basis to receive either high - dose melphalan plus salvage asct or cyclophosphamide . 
a block randomisation was used to ensure treatment groups were well balanced for length of rst remission or plateau ( < 18 months vs 1824 months vs > 24 months ) and response to pad re - induction therapy ( stable disease vs partial or complete response )  . 
randomisation was done centrally at the clinical trials research unit ( leeds , uk ) using a 24 - h automated telephone randomisation line according to randomisation lists produced by the trial statistician under the supervision of jmb . 
 assessment of outcomes was also unblinded , apart from nal con rmation of central response and progression , which was done by an independent myeloma physician masked to treatment allocation . 
 procedures patients received consolidation therapy consisting of a single infusion of intravenous melphalan 200 mg / m followed by asct after 2448 h , or oral cyclophosphamide 400 mg / m per week for 12 weeks . 
 response and disease progression were assessed according to the imwg uniform response criteria for multiple myeloma ( appendix ) using blood and urine samples , unless progression of myeloma occurred as an isolated bone lesion , growth of a plasmacytoma , or an increase in plasma cells in the bone marrow without a change in m - protein , in which case tissue histological and disease examination was done . 
response progression were con rmed by a central laboratory using sequential samples of blood and urine and bone marrow aspirates taken at baseline , after re - induction treatment , 100 days after asct or 30 days after the end of cyclophosphamide treatment , every year after randomisation , and at disease progression . 
 table 1 : demographic and baseline characteristics of registered patients and randomly assigned patients , per treatment group vol 15 july 2014 articles suspensions were xed in carnoys solution and stored at in - situ hybridisation 20c . 
interphase uorescence ( ifish ) , was done with commercial probes , scored and image - captured using an axioplan microscope ( zeiss , jena , germany ) with metasystems isis software ( altluheim , germany )  . 
cd138 - puri ed plasma cells were tested with probes to identify deletion of chromosome 17p , tp53 [ ch17p deletion ] , igh , and myc gene rearrangements , and for the presence of fgfr3 / igh [ t ( 4 ; 14 ) ] and maf / igh [ t ( 14 ; 16 ) ] fusion genes , among other abnormalities . 
for the detection of a tp53 deletion , a cuto of 20% plasma - cell involvement was used , and for fusion gene detection the reporting was absolute ( present vs absent )  . 
overall survival was de ned as the time from randomisation to death from any cause , and progressionfree survival was de ned as the time from randomisation to rst documented assessment showing disease progression or death from any cause . 
we determined response in accordance with imwg criteria.23 toxicity and safety were assessed after each cycle of protocol treatment according to adverse events , graded by the national cancer institute common terminology criteria ( ctcae ) version 3.0 during routine clinical assessments at each centre.24 pain and quality - of - life results will be reported separately . for adverse events statistical analysis we planned to register 460 patients with the aim of randomly assigning 320 to a treatment group . 
the sample size was based on a 4 - year recruitment period and 2 - year follow - up , 80% power , a 5% signi cance level , and a median time to progression of 14 months in the cyclophosphamide group to detect a 30% reduction in hazard ratio [ hr ] in the asct group compared with the cyclophosphamide group , equating to a 6 - month improvement in median time to progression . 
on the basis of these assumptions , which we based on published retrospective study outcomes and an early phase trial of bortezomib in a similar population , 25 249 events were required . 
we allowed for 5% of patients to drop out . the trial closed to recruitment in november , 2012 , after an interim analysis of the primary endpoint done at the request of the independent medical research council leukaemia data monitoring and ethics committee ( dmec ) showed that the prespeci ed boundary ( de ned as a guideline as p < 0001 ) representing overwhelming evidence had been met . 
 the dmec reviewed all the information that they requested about statistical signi cance and the estimated treatment e ects to come to a decision , and on the basis of the dmec review , the chair of the leukaemia trials steering committee recommended that the trial be closed and the results unmasked . 
centres were instructed to complete treatment as per protocol for those patients receiving treatment , and attending physicians were to administer treatment at their discretion to patients not yet receiving treatment . 
followup data is being obtained regarding the nature of the treatments that were given to patients who had progressive disease after the trial closed , and durability of responses to this next line of therapy . the cuto date for the nal analysis was july 9 , 2013 , and all data entered into the database up to that timepoint were incorporated in the nal analysis . 
time to progression , objective response , progression - free survival , and overall survival endpoints related to consolidation treatment ( ie , after randomisation ) were analysed in all patients who were randomly assigned to a treatment group . 
toxicity and safety endpoints were assessed in the safety population , which consisted of all patients who received at least one dose of study treatment . we used cox regression to analyse time to progression , accounting for strati cation factors ( length of rst remission or plateau and response to pad re - induction therapy ) and whether or not mobilisation therapy was received . 
response rates ( appendix ) were compared with ordinal logistic regression analysis accounting for the strati cation factors and whether or not mobilisation therapy was received . we did sensitivity analyses to account for deviations from trial protocol for patients who had not completed study treatment at the time of trial closure by censoring these patients at the time of closure . 
 878 vol 15 july 2014 articles gc had nal responsibility for the decision to submit for publication in agreement with all the investigators participating in the trial . the median time from the original myeloma diagnosis to randomisation was 41 years ( range 22136 ) in the salvage asct group and 37 years ( 24132 ) in the a time to progression cyclophosphamide melphalan plus asct results between april 16 , 2008 , and nov 19 , 2012 , 297 patients were registered ( gure 1 )  . 
293 ( 99% ) of 297 registered patients induction received 967 cycles of pad chemotherapy , of whom 281 ( 96% ) had the protocolde ned two to four cycles and 162 ( 55% ) completed four cycles . 
between aug 26 , 2008 , and nov 16 , 2012 , 174 patients with newly mobilised pbscs or su cient pbscs stored from their rst transplant ( or both ) were randomly assigned to receive high - dose melphalan followed by asct ( n = 89 ) or oral cyclophosphamide ( n = 85 ; gure 1 )  . baseline demographic and disease characteristics were well balanced between the treatment groups ( table 1 ) , except that a higher proportion of patients had international staging system ( iss ) stage 3 multiple myeloma in the asct group than in the cyclophosphamide group . 
280 ( 94% ) of 297 registered patients were bortezomib - naive ; induction therapy before rst - line asct had consisted of thalidomide - based combinations in 182 ( 61% ) of 297 vincristine plus doxorubicin plus patients and dexamethasone - like combinations in 84 ( 28% ) , with only 50 ( 17% ) having received thalidomide maintenance after the transplant . 
no patients had received lenalidomide as a rst - line therapy . initial cytogenetic data by ifish at trial registration were available for 149 ( 50% ) of 297 registered patients and for 88 ( 51% ) of 174 randomly assigned patients ( table 1 )  . 
 cytogenetic abnormalities were collated into a cytogenetic risk pro le , which resulted in 13 ( 15% ) randomly assigned patients ( table 1 ) having an adverse risk pro le ( de ned by the presence of any one of the following : t [ 4 ; 14 ] , t [ 14 ; 16 ] , or del17p ) and 75 ( 85% ) randomly assigned patients having a standard risk pro le ( absence of adverse genetic risk factors , but including the presence of hyperdiploidy , t [ 11 ; 14 ] , del13q , and igh rearrangement with no de ned translocation partner )  . figure 2 : progression and survival outcomes in the intention - to - treat population kaplan - meier curves were plotted for time to progression ( a ) , de ned as time from randomisation to the rst assessment showing disease progression ( deaths not due to disease progression were censored ) ; progression - free survival ( b ) , de ned as time from randomisation to rst assessment showing disease progression or death from any cause ; and overall survival ( c ) , de ned as the time from randomisation to death from any cause . 
 number at risk cyclophosphamide melphalan plus asct log - rank p < 00001 b progression - free survival number at risk cyclophosphamide melphalan plus asct log - rank p < 00001 c overall survival log - rank p = 02332 number at risk cyclophosphamide melphalan plus asct time from randomisation ( months ) vol 15 july 2014 articles time cyclophosphamide group . 
the median from previous asct to rst progression or relapse was 27 years ( range 10124 ) in the salvage asct group and 25 years ( 0765 ) in the cyclophosphamide group and the median time from the previous asct to the rst required treatment ( ie , pad induction therapy ) was 28 years ( range 11124 ) in the salvage asct group and 26 years ( 1283 ) in the cyclophosphamide group . 
finally , the median time from registration to randomisation was 38 years ( range 1697 ) in the salvage asct group and 36 years ( 1674 ) in the cyclophosphamide group . 
the reasons for registered patients not proceeding randomisation , and the status of patients at trial closure , are summarised in the appendix . ( 2531 ) at the cuto date for the nal analysis ( july 9 , 2013 ) , the median follow - up was 31 months ( iqr 1942 ) in the whole population : 34 months ( iqr 1948 ) in the salvage asct group and 23 months the cyclophosphamide group . 
at data cuto , 125 progression events had occurred in the intention - to - treat population ( 57 [ 64% ] of 89 patients in the salvage asct group had con rmed disease progression vs 68 [ 80% ] of 85 patients in the cyclophosphamide group )  . 
time to progression was signi cantly longer in the salvage asct group than in the cyclophosphamide group ( median 19 months [ 95% ci 1625 ] vs 11 months [ 912 ] ; hr 036 [ 95% ci 025053 ] ; p < 00001 ; gure 2 )  . 
 overall survival did not di er signi cantly between randomised groups ( hr 062 [ 95% ci 03127 ] ; p value for treatment e ect in the cox proportional hazards regression model = 019 )  . 
3 - year overall survival was 803% ( 95% ci 693912 ) in the salvage asct group and 629% ( 466792 ) in the cyclophosphamide group ( gure 2 )  . 
the main causes of death randomised patients were progressive disease ( in eight [ 9% ] of 89 patients in the salvage asct group vs nine [ 11% ] of 85 patients in the cyclophosphamide group ) , peripheral vascular disease ( none vs one [ 1% ] ) , myelodysplastic syndrome ( one [ 1% ] vs none ) , pneumonia ( none vs one [ 1% ] ) , haemorrhage ( none vs one [ 1% ] ) , and subarachnoid haemorrhage ( none vs one [ 1% ] )  . 
cause of death was not reported in six [ 7% ] patients in the salvage the asct group and cyclophosphamide group . [ 5% ] patients four after pad induction therapy , 49 ( 16% ; 95% ci 125212 ) of 297 patients achieved a stringent complete response or complete response , 186 ( 63% ; 569682 ) had a very good partial response or partial response , and 44 ( 15% ; 110194 ) had stable disease ( table 2 )  . 
thus , the proportion of patients achieving a very good partial response or better was 37% ( 111 of 297 ; 319429 ) , and the proportion of patients achieving an overall response was 79% ( 745837 ; table 2 )  . 
after randomisation , a stringent complete response or complete response was reported in 35 ( 39% ; 95% ci 291503 ) of 89 patients in the salvage asct group compared with 19 ( 22% ; 143327 ) of 85 patients in the cyclophosphamide group ( odds ratio [ or ] 224 , 111465 ; p = 0021 )  . 
39 ( 44% ; 335541 ) patients in the salvage asct group and 45 ( 53% ; 423636 ) in the cyclophosphamide group had a very good partial response or partial response . 
the proportion of patients with a very good partial response or better was 60% ( 53 of 89 ; 494697 ) after salvage asct versus 47% ( 40 of 85 ; 364577 ) after cyclophosphamide ( or 038 , 95% ci 0207 ; p = 00036 )  . an analysis of responses to initial and salvage asct revealed that the proportion of patients who achieved an objective response after rst - line asct was 96% ( 85 of 89 ) , whereas it was 83% ( 74 of 89 ) after salvage asct . 
of the 52 ( 58% ) of 89 patients who achieved a stringent complete response or complete response after rst - line asct , 28 ( 54% ) reached a stringent complete response or complete response after salvage asct , whereas 15 ( 29% ) achieved a very good partial response or partial response ( appendix )  . 
additionally , of the 33 ( 37% ) of 89 patients who had a very good partial response or partial response after rst - line asct , ve ( 15% ) achieved a stringent complete response or complete response after salvage asct , whereas 22 ( 67% ) achieved a very good partial response or partial response . 880 vol 15 july 2014 articles hr ( 95%ci ) 005 ( 00060419 ) 044 ( 02870672 ) 0086 ( 00090831 ) 0288 ( 01740478 ) 0590 ( 02871209 ) 0200 ( 01030390 ) 2410 ( 039614662 ) 0362 ( 02460534 ) response at end of pad scr or cr ( n = 54 ) vgpr or pr ( n = 84 ) sd ( n = 6 ) 2 microglobulin at registration < 35 mg / l ( n = 112 ) > 35 mg / l ( n = 47 ) ifish cytogenetic risk * favourable ( n = 75 ) unfavourable ( n = 13 ) overall ( n = 174 ) 001 010 020 050 100 200 500 1000 favours melphalan plus asct favours cyclophosphamide figure 3 : subgroup analysis of time to progression hrs for risk of disease progression in the melphalan plus salvage asct group compared with the cyclophosphamide group . 
 * adverse risk was de ned by the presence of a t ( 4 ; 14 ) translocation , t ( 14 ; 16 ) translocation , or tp53 deletion ; standard risk was de ned by the absence of adverse markers . 
second primary malignancies were reported in three patients at a median of 334 months ( range 199383 ) after trial registration : one patient was diagnosed with prostatic cancer in the asct group , with one patient diagnosed with squamouscell cancer and one patient diagnosed with breast cancer in the cyclophosphamide group . discussion this phase 3 study , which was stopped early because it crossed a stopping boundary for e cacy at an interim analysis , assessed the application of salvage asct in patients with recurrence of multiple myeloma after previous asct . 
the use of high - dose melphalan plus asct at relapse signi cantly prolonged progression compared with cyclophosphamide therapy . time until now , only retrospective single - centre and registry studies had examined the role of salvage asct , all concluding a bene cial e ect , although with varied results for durability of response ( panel ) .1421 our randomised study provides clear evidence for the bene t of high - dose melphalan plus salvage asct by showing that patients assigned to this treatment achieved a durable response after re - induction therapy with bortezomib , doxorubicin , and dexamethasone . 
few phase 3 trials have focused on treatment for rst relapse in multiple myeloma , and although cross - trial comparisons are problematic , our results compare favourably with those achieved with combination therapy incorporating novel response to pad re - induction the time - to - progression bene t associated with salvage asct was consistent across subgroups of patients de ned therapy and 2 - microglobulin concentration at registration , but not for those with an adverse cytogenetic risk by ifish ( gure 3 )  . 
for the 64 ( 72% ) of 89 patients in the salvage asct group and 64 ( 75% ) of 85 in the cyclophosphamide group who had a rst response lasting longer than 24 months , median time to progression was 24 months ( 95% ci 1827 ) versus 11 months ( 1012 ) , respectively ( hr 035 , 95% ci 022054 ; p < 00001 from cox proportional hazards regression model )  . 
for the 25 ( 28% ) patients in the salvage asct group and 21 the cyclophosphamide group who had a rst response of 24 months or less , median time to progression was 13 months ( 95% ci 1020 ) and 9 months ( 812 ) , respectively ( hr 037 , 95% ci 019074 ; p < 00037 from cox proportional hazards regression model )  . ( 25% ) results of sensitivity analyses for time to progression , progression - free survival , and overall survival that censored patients who had not completed study treatment at the time of trial closure were similar to those of the intention - to - treat analyses ( data not shown )  . all patients who received at least one dose of study treatment were assessed for adverse events . 
during pad induction therapy , 131 ( 45% ) of 293 patients reported at least one serious adverse event , with 120 ( 60% ) of 131 reported serious adverse events suspected to be related to the study medication . 
the most frequent ctcae grade 34 adverse events were haematological ( table 3 ) : 125 ( 43% ) of 293 patients who had pad induction therapy had grade 34 neutropenia , and 150 ( 51% ) had grade 34 thrombocytopenia , whereas grade 34 neuropathy ( sensory plus motor ) occurred in 35 ( 12% ) patients . 
gastrointestinal grade 34 toxicity was infrequent during pad induction therapy ( 28 [ 10% ] of 293 patients ) , as were grade 34 infections ( 25 [ 9% ] patients )  . 
during induction , 184 ( 63% ) of patients had a treatment delay , most frequently around cycle 3 , which occurred in 101 ( 34% ) , mainly due to cytopenias . 
154 ( 52% ) of 293 patients needed a dose modi cation , with g - csf support being administered to 49 ( 16% ) patients to support pad therapy , most frequently in cycle 4 ( n = 22 needed g - csf support in cycle 4 )  . the received randomly 167 patients assigned consolidation therapy ( 83 in the asct group and 84 in the cyclophosphamide group )  . 
the dose of intravenous melphalan was reduced from 200 mg / m to 140 mg / m in two ( 2% ) patients owing to reduced creatinine clearance and in four ( 5% ) patients for other reasons . 
a greater proportion of patients in the melphalan plus asct group than in the cyclophosphamide group had grade 34 adverse events related to neutropenia ( 63 [ 76% ] of 83 in the melphalan plus asct group vs 11 [ 13% ] of 84 in the cyclophosphamide group ) , thrombocytopenia vol 15 july 2014 articles ( biological ) agents . 
in one phase 3 trial , 26 time to progression after the triple combination of bortezomib , thalidomide , and dexamethasone ( vtd ) was 195 months in patients who had relapsed after rst - line asct , and the proportion of patients who received vtd who were alive at 2 years was 71% . 
in our study , 803% of patients in the salvage asct group were alive at 3 years compared with 629% in the cyclophosphamide group . results of the prede ned subgroup analysis in our study suggested that melphalan plus salvage asct was better than weekly cyclophosphamide , irrespective of the quality of response to pad re - induction and the concentration of 2 - microglobulin at registration . 
 furthermore , melphalan plus salvage asct was better than weekly cyclophosphamide irrespective of the response duration to the initial asct , although time to progression seemed to be longer in patients with a response lasting longer than 24 months after their rst asct than in those with a response of 24 months or less . 
however , the small number of patients with an adverse cytogenetic risk pro le makes the interpretation of this result di cult ; therefore , we cannot rmly recommend that salvage asct should be avoided in patients with adverse cytogenetics at rst relapse . randomised controlled trials that are stopped early for e cacy have been suggested to overestimate the e ect size.27 however , when a stringent and prede ned stopping rule is in place28 and greater than 50% of the required events have been reported , 29 stopping early has been suggested to have a negligible impact on estimated e ect sizes . 
this interim analysis was subsequently brought forward at the request of the independent dmec , but a stringent ad - hoc rule was included for early interim analyses as described above and in the statistical analysis plan . 
the primary endpoint analysis was undertaken when 125 ( 50% ) of the required 249 events had been reported , suggesting that the estimated e ect could be at most minimally in ated . although salvage asct also extended progression - free survival compared with cyclophosphamide , as yet , overall survival does not signi cantly di er between the treatment groups . 
the e ect of therapy after progression , particularly because the trial closed early , might confound the survival analysis , especially if a signi cant proportion of patients in the cyclophosphamide group received high - dose melphalan plus salvage asct at progression in this study , as retrospective studies have shown an overall survival advantage when salvage asct has been used.14 , 16 , 17 , 21 longterm follow - up analysis for overall survival will be undertaken in the future , at which point the primary endpoint analysis will also be updated . our trial further shows that the quality of responses after salvage asct is similar to that after rst - line asct . 
 we reported a stringent complete response or complete 882 vol 15 july 2014 articles response in 39% of patients after salvage asct , whereas 49% of patients had this response after the rst asct ( appendix )  . 
a partial response or very good partial response was reported in 44% of patients after salvage asct and in 34% after the rst asct . the response to pad re - induction therapy in this broadly bortezomib - naive population was similar to that seen in front - line trials of pad therapy.30 the proportion of patients with an overall response in our trial after four cycles of pad was 79% , with 17% of patients reaching a complete response or a stringent complete response and 38% achieving a very good partial response or better . 
in a randomised trial comparing pad with vincristine , adriamycin , and dexamethasone , 12 7% of patients had achieved a complete response after three cycles of pad , with 4% achieving a near - complete response and 42% achieving a very good partial response or better . 
depth of response is an important prognostic factor in the front - line transplant setting , 3133 and the results of our study suggest that the depth of response to re - induction translates longer time to progression , but this was not con rmed in our prede ned subgroup analysis . into a ( imid ) - based our trial was designed to incorporate a proteasome inhibitor - based re - induction regimen rather than an immune - modulatory drug regimen because of the high level of imid exposure in the rstline setting for trial registrants , and also because of access restrictions to treatment with any novel agents across many health - care systems . 
as such , we used a bortezomib - containing regimen as re - induction therapy to obtain a high extent of tumour control to help to assess which consolidation strategy o ered the better balance of e cacy and toxicity . 
however , when the trial was designed in 2006 , no worldwide standard of care was evident for post re - induction consolidation , although weekly cyclophosphamide was used as a standard of care in the uk in earlier medical research council trials that showed e cacy for cyclophosphamide in the nontransplant setting.34 our trial design permitted the comparison of the e ect on durability of response by alkylating - agent dose comparison . 
time to progression with cyclophosphamide in our study ( 11 months from randomisation plus a median of 38 months from requiring treatment to randomisation ) is similar to that of the control group in a study by garderet and colleagues26 and received dexamethasone ( 138 months )  . 
furthermore , no maintenance therapy was included as part of the treatments in our trial , because the role of maintenance therapy after salvage asct has not been established , even in retrospective studies . 
nevertheless , having thalidomide that shown that salvage asct has a better durability of response than does cyclophosphamide , and after studies have shown the bene t of consolidation or maintenance strategies in the front - line transplant setting , 6 , 8 , 9 , 12 , 35 further investigation of therapy after asct in the relapse setting is warranted , and we will seek to address this question in a new study . 
failure to mobilise stem cells resulted in 30 ( 11% ) of 266 patients not being eligible for randomisation ; however , the study design was powered to accommodate a stem - cell mobilisation failure rate of 30% . 
however , this study had 123 patients who had an adequate amount of stored cells , which suggests that it can be possible to mobilise enough stem cells at rstline asct for a second , salvage asct , thus making salvage asct an option for a third of patients who would be eligible for the procedure , but who might not mobilise a su cient number of stem cells at relapse . 
there was no di erence in response or outcome for patients who had their salvage asct from newly mobilised cells versus stored cells . as expected , salvage asct was associated with more grade 34 haematological and gastrointestinal adverse events than was weekly cyclophosphamide . 
the proportion of patients with grade 34 peripheral neuropathy after pad induction was 12% , which is lower panel : research in context systematic review the management of relapsed multiple myeloma after a previous autologous stem - cell transplant ( asct ) has evolved over the past 1015 years with the advent of strategies containing new agents . 
we undertook a systematic review , with no date or language restrictions ( pubmed search for salvage autologous transplant , second autologous transplant , and relapsed myeloma ) , in 2006 and found seven published studies that were suitable for consideration . 
both scienti c literature reviews showed that the evidence to support salvage asct was based on retrospective registry or single - centre studies only , mainly without the incorporation of new agents in the re - induction phase . 
because the published results were limited by their retrospective and non - comparative nature , and were largely done in an era when new anti - myeloma agents were not available , randomised , multicentre data was clearly needed that delineated the true potential for salvage asct in relapsed disease , as evidence for clinical decision making and thus practice - changing research . interpretation we show that high - dose melphalan plus salvage asct administered at rst relapse signi cantly prolongs time to progression compared with conventional , low - dose alkylating agent ( cyclophosphamide ) consolidation , after the use of a re - induction regimen containing a new agent . 
the data provide the necessary prospective evidence not only substantiating the previous retrospective studies in an up - to - date clinical treatment scenario , but also showing the clinical usefulness of salvage asct in myeloma at rst relapse . 
our results might aid the decision - making process for both physicians and patients with myeloma at rst relapse . vol 15 july 2014 articles that than that reported in a trial by sonneveld and colleagues13 after pad induction ( 24% ) .13 in our trial , bortezomib was administered intravenously . 
moreau and colleagues36 showed the subcutaneous administration of bortezomib results in improved tolerability , particularly a reduction in peripheral neuropathy , while retaining the e cacy reported with the intravenous application of the agent , 36 suggesting that the subcutaneous route might be preferable in future studies . in conclusion , to our knowledge , this trial is the rst randomised study to show that salvage asct is better than weekly cylcophosphamide in consolidating the response obtained from new - agent re - induction therapy . 
 the clear demonstration of e ect on durability of response in the relapse setting provides evidence for salvage asct to be considered as a standard of care for eligible patients , although this approach to the clinical management of relapsed myeloma is widely practised in some countries . 
although the e ect on overall survival remains to be clari ed , these results show that salvage asct should be routinely considered in eligible patients at rst relapse , o ering evidence for informed decision making regarding the choice of asct for clinicians and patients alike . contributors authorship was determined in accordance with a pre - determined trial management group policy delineated in the protocol . 
gc wrote the article and cw , jmb , dac , jcaven , jas , aja , mf , cp , ky , jcavet , hh , jmb , ac , soc , mtd , and tcmm obtained the data , revised the article , and gave nal approval . declaration of interests gc and jas have received honoraria , research funding , and speakers bureau fees from janssen . 
 acknowledgments the study was designed by gc and the trial management group , on behalf of the uk myeloma forum ( ukmf ) and the british society of blood and marrow transplantation ( bsbmt )  . 
 correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
we aimed to assess the use of the edinburgh selection criteria for ovarian tissue cryopreservation in girls and young women with cancer to determine whether we are o ering this invasive procedure to the patients who are most at risk of premature ovarian insu ciency . methods cryopreservation of ovarian tissue has been selectively o ered to girls and young women with cancer who met the edinburgh selection criteria since 1996 . 
between jan 1 , 1996 , and june 30 , 2012 , 410 female patients younger than 18 years at diagnosis were treated for cancer ( including leukaemia and brain tumours ) at the edinburgh childrens cancer centre , which serves the whole south east of scotland region . 
we determined the ovarian status of these patients from review of clinical records and classi ed them as having premature ovarian insu ciency or not , or as unable to be determined . 
patients younger than 12 years at time of data cuto ( jan 31 , 2013 ) were excluded from the analysis . findings 34 ( 8% ) of the 410 patients met the edinburgh selection criteria and were o ered ovarian tissue cryopreservation before starting cancer treatment . 
of the 14 assessable patients who had successfully undergone ovarian cryopreservation , six had developed premature ovarian insu ciency at a median age of 134 years ( iqr 125146 ) , one of whom also had a natural pregnancy . 
the cumulative probability of developing premature ovarian insu ciency after treatment was completed was signi cantly higher for patients who met the criteria for ovarian tissue cryopreservation than for those who did not ( 15 - year probability 35% [ 95% ci 1053 ] vs 1% [ 02 ] ; p < 00001 ; hazard ratio 568 [ 95% ci 625216 ] at 10 years )  . interpretation the results of this analysis show that the edinburgh selection criteria accurately identify the few girls and young women who will develop premature ovarian insu ciency , and validate their use for selection of patients for ovarian tissue cryopreservation . 
about 80% of children with cancer will be alive 5 years after diagnosis and about 70% will be alive and cured of their original cancer 10 years after diagnosis.1 however , some cancer treatments can compromise ovarian in children.24 the function increasing life expectancy of children with cancer has led to a growing population of girls and young women who are at risk of developing premature ovarian insu ciency . 
most girls and young women treated for cancer will retain a window of opportunity for fertility ; however , for those at high risk of premature ovarian insu ciency the options for fertility preservation are few and experimental . is an ovarian tissue cryopreservation important development for fertility preservation in girls and young women at risk of premature ovarian insu ciency as a result of treatment for cancer.58 at least 30 pregnancies after orthotopic reimplantation of frozenthawed ovarian cortex have been reported worldwide , 5 showing that this approach is viable in adults , although the success rate is vol 15 september 2014 1129 articles unclear because the total number of women in whom frozenthawed ovarian tissue has been reimplanted is unknown . 
the procedure remains unproven and experimental in girls and young women . evidence from case series and reviews9 , 10 has suggested that the collection of ovarian tissue for freezing by laparoscopy under a general anaesthetic is safe and feasible in prepubertal girls as well as in adult women . 
 the procedure is invasive , and can carry an unacceptable operative risk in some children with cancer who might be immunocompromised and pancytopenic and are therefore at increased risk of bleeding and infection . 
these uncertainties , and e ectiveness of the procedure for the restoration of fertility , dictate that it should only be o ered to girls and young women who are at high risk of premature ovarian insu ciency and who will have a substantially reduced opportunity for fertility . 
accurate identi cation of these patients requires that the risk of premature ovarian insu ciency , which is determined by the nature of the treatment to be delivered and not the disease itself , can be assessed at the time of diagnosis.4 however , in children , the full consequences of treatment with respect to reproductive function are not fully known and will take several decades to be fully realised.13 , 14 thus an accurate fertility prognosis cannot always be obtained before the start of treatment . 
on the basis of these considerations , we have previously proposed that factors that a ect the assessment of an individual patient for invasive fertility preservation techniques can be usefully grouped as intrinsic ( ie , related to the patient herself and her present state of health ) and extrinsic ( ie , related largely to the anticipated treatment and the availability of appropriate expertise for the techniques proposed ) .15 with the now proven success of ovarian tissue cryopreservation in adult women , 5 it is important to establish if this experimental technique is being o ered to the correct young patientsie , those who are at high risk for the development of premature ovarian insu ciency , can safely undergo laparoscopic surgery , and have a good long - term prognosis . 
the edinburgh selection criteria for panel 1 : the edinburgh selection criteria age younger than 35 years no previous chemotherapy or radiotherapy if aged 15 years or older at diagnosis , but mild , non - gonadotoxic chemotherapy acceptable if younger than 15 years a realistic chance of surviving for 5 years a high risk of premature ovarian insu ciency ( > 50% ) informed consent ( from parents and , where possible , patient ) negative serology results for hiv , syphilis , and hepatitis b not pregnant and no existing children ovarian tissue cryopreservation have been previously reported , 4 , 9 having been developed after multidisciplinary discussion in 1996 and slightly revised in 2000 . 
the aim of this study is to assess the accuracy of patient selection for ovarian tissue cryopreservation in a single centre that has o ered this experimental procedure ( as part of this approved study ) to selected children and teenagers with cancer since 1996 , by comparing the prevalence of premature ovarian insu ciency in those who were and were not o ered the procedure . methods study design and participants the study cohort consisted of all female patients treated for cancer ( including leukaemia and brain tumours ) at the edinburgh childrens cancer centre who were younger than 18 years at diagnosis between jan 1 , 1996 , and june 30 , 2012 . 
we aimed to assess the relation between whether or not patients had been o ered ovarian tissue cryo preservation and whether they had premature ovarian insu ciency at the time of their most recent assessment . 
 a risk assessment for fertility preservation was made for all patients before the start of treatment , 15 and cryopreservation of ovarian tissue was o ered to those patients who met the edinburgh selection criteria ( panel 1 )  . 
we used knowledge of the relevant scienti c literature and our own experience to make an initial assessment at diagnosis of whether an individual patient with a new diagnosis of cancer had a greater than 50% risk of premature ovarian insu ciency . 
most of the patients identi ed as being at high risk of premature ovarian insu ciency were planned to be treated with high - dose alkylating agent - based regimens or radiotherapy to a eld that would include the ovaries . 
we obtained written informed consent from parents and , where possible , patients for ovarian tissue cryopreservation . this study was done with the approval of the lothian research ethics committee . procedures in those patients who consented to the procedure , ovarian laparoscopically under general tissue was obtained anaesthetic and cryopreserved . 
generally , three to ve ovarian cortical strips from one ovary were dissected with scissors , without diathermy , with the aim of removing roughly 70% of the ovarian cortex . 
thin strips ( not more than 15 mm thick ) were collected into liebovitz medium and cryopreserved as previously described.16 a whole ovary could be obtained from very young patients for whom the cortex could not be dissected . 
biopsy samples are stored in the vapour phase of liquid nitrogen at the scottish national blood transfusion service tissue establishment ( edinburgh , uk ) under licence from the uk human tissue authority and , for part of the time period reported , the human fertilisation and embryology authority . ovarian status was recorded for the whole surviving cohort who were aged 12 years or older on jan 31 , 2013 , from review of their medical notes from diagnosis and when they attended routine follow - up assessments . 
premature ovarian insu ciency was de ned as the documented presence of at least two of three identifying features : amenorrhoea for at least 4 months ; serum follicle stimulating hormone greater than 25 iu / l on at least two occasions ; and low ( < 150 pmol / l ) serum oestradiol concomitant with raised ( > 25 iu / l ) follicle stimulating hormone . 
the absence of premature ovarian insu ciency was con rmed by one or more of three identifying features : premenarcheal , but progressing normally through puberty ; having regular menses while not taking hormonal contraception ; or normal concentrations of gonadotropins and oestradiol . 
 ovarian status could not be determined in children younger than 12 years , because the measurement of gonadotropins and oestradiol in girls younger than 12 years is not a reliable measure of ovarian function , or in individuals taking hormonal contraception . statistical analysis we used the kaplan - meier method17 with premature ovarian insu ciency as the de ned event . 
since patient classi cation into the premature ovarian insu ciency group occurred after the actual date of onset of premature ovarian insu ciency , we discretised the 15 years after diagnosis into calendar years , and recorded each assessment of premature ovarian insu ciency occurring in the year after diagnosis as a premature ovarian insu ciency event in that year . 
we then calculated life tables for the patients who were o ered ovarian tissue cryopreservation ( the o ered group ) and those who were not o ered the procedure ( the noto ered group ) as cumulative event - free probabilities for each year of follow - up after diagnosis . we derived p values to test the null hypothesis that the frequency of premature ovarian insu ciency occurrences were distributed evenly between the two groups . 
the hr for each year was calculated as the ratio of observed - to - expected occurrences of premature ovarian insu ciency in the o ered group in that year , divided by the ratio of observed - to - expected occurrences of premature ovarian insu ciency in the not - o ered group in that year , with the observed and expected values taken from the intermediate calculations used to derive the kaplanmeier cumulative probabilities . we calculated hrs using microsoft excel for mac ( version 14.3.7 ) and did the kaplan - meier analyses , including calculation of cis and p values , using the kmsurv version 0.1 - 5 package for r version 2.15.3. role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
at the time of data censoring ( jan 31 , 2013 ) , an additional four patients who had not been o ered ovarian tissue cryopreservation were still receiving cancer treatment , and we were unable to classify ovarian function in a further 42 patients in the same group because of incomplete information in their medical records . 
median follow - up for the assessable patients who were o ered and underwent ovarian tissue cryopreservation ( n = 14 ) was 60 years ( iqr 35149 ) ; for those who were o ered the procedure but declined ( n = 6 ) it was 109 years ( 74137 ) and for those who were not o ered the procedure ( n = 141 ) it was 107 years ( 61138 )  . ovarian tissue cryopreservation was o ered 34 patients , of whom 21 underwent the procedure and 13 declined . 
 the median age of the cohort of patients who were o ered cryopreservation and were assessable ( n = 20 , gure 1 ) was 169 years ( iqr 155218 ) at data cuto for this analysis ; the median age of assessable patients in the not - o ered group ( n = 141 ) was 179 years ( 156220 )  . 
of the patients who underwent ovarian cryopreservation , a whole ovary was obtained in the two youngest patients ( table ) ; the other patients had ovarian cortical strips taken from one ovary . of the 20 patients in the o ered group who had ovarian tissue successfully cryopreserved , four were younger than 12 years at the time of last follow - up , one had died , and one was using hormonal contraception ; 14 patients were aged 12 years or older and available for assessment of ovarian function . 
of these 14 , six had developed premature ovarian insu ciency at a median age of 134 years ( iqr 125146 ) , after a median interval since vol 15 september 2014 1131 articles 410 female cancer patients aged younger than 18 years at diagnosis 34 were oered cryopreservation 376 were not oered cryopreservation 20 had tissue cryopreserved 13 declined procedure 1 procedure unsuccessful ( patient later died , unrelated to procedure ) 1 declined because of poor communication 1 declined because of a uterine factor * 2 declined because of parental choice 9 declined because patient was too unwell 1 died 4 younger than 12 years 1 on cocp 1 younger than 12 years 3 died 2 younger than 12 years 1 lost to follow - up 81 died 91 younger than 12 years 17 on cocp 4 were still on cancer treatment 42 had insucient follow - up information 14 available for assessment of ovarian function 6 available for assessment of ovarian function 141 available for assessment of ovarian function figure 1 : study pro le cocp = combined oral contraceptive pill . 
 * treatment plan meant that there was a high chance that the patient would receive radiation to her pelvis and uterus at a very young age . diagnosis of 17 years ( 0824 ) , and eight had normal ovarian function at a median age of 219 years ( 162277 )  . 
one patient who developed premature ovarian insu ciency subsequently had a successful natural pregnancy , as reported previously.18 of the 13 patients who were o ered cryopreservation but declined the procedure ( gure 1 ) , three were deceased and three were younger than 12 years at the time of last follow - up ; one was lost to follow - up . 
thus premature ovarian insu ciency was identi ed in a total of seven ( 35% ) of 20 assessable patients in the group o ered ovarian cryopreservation . the 376 o ered ovarian patients not cryopreservation , 81 were deceased at the time of assessment , 91 were younger than 12 years , 17 were using hormonal con traception , four were still receiving cancer treatment , and information about ovarian status was incomplete for 42 ( gure 1 )  . 
of the 141 who were not o ered cryopreservation and for whom ovarian function is known , 140 did not have premature ovarian insu ciency at a median age 179 years ( iqr 156220 )  . 
 these , 112 had achieved menarche , 17 were premenarchal but aged 12 years or older and were progressing normally through puberty , and 11 had hypogonadotropic hypogonadism as a result of cranial irradiation treatment for brain tumours . 
premature ovarian insu ciency was con rmed in only one patient in this group , who developed premature ovarian insu ciency at age 150 years ( 29 years after diagnosis ) after a successful allogeneic bone marrow transplantation for relapsed acute myeloid leukaemia with busulfan and cyclophosphamide conditioning . 
she was not o ered cryopreservation of ovarian tissue at the time of original diagnosis because she did not meet the criteria ( low risk of premature ovarian insu ciency ) , nor at relapse because of the urgency of the need for further treatment , when she was believed to be too unwell to undergo a laparoscopic procedure . last premature ovarian therefore , by 9 years from diagnosis ( the interval to the insu ciency event ) , seven ( 35% ) of 20 patients o ered ovarian tissue cryopreservation had developed premature ovarian insu ciency , compared with one ( 1% ) of 141 of those not o ered ovarian tissue cryopreservation . 
the cumulative probability of developing premature ovarian treatment was completed was insu ciency after signi cantly higher for the patients o ered ovarian tissue cryopreservation than for those who were not o ered ovarian ( 15 - year probability 35% [ 95% ci 1053 ] vs 1% [ 02 ] ; p < 00001 ; hr 568 [ 95% ci 625216 ] at 10 years ; gure 2 )  . cryopreservation tissue in addition to the assessed risk of premature ovarian insu ciency as a result of the planned treatment , another of the edinburgh selection criteria is that the patient has to have a realistic chance of surviving for 5 years ( panel 1 )  . 
in our cohort , four ( 12% ) of 34 patients 1132 vol 15 september 2014 articles poi ( plus one child ) ovarian function not poi deceased not poi not poi on cocp not poi not poi deceased not assessed not poi not assessed not assessed not poi not poi not assessed age at cryopreservation ( years ) method of ovarian tissue collection complications from procedure duration since cryopreservation ( years ) age at last assessment ( years ) diagnosis hodgkins lymphoma * ewings sarcoma ewings sarcoma ( pubic bone ) sacral ependymoma hodgkins lymphoma hodgkins lymphoma chronic granulocytic leukaemia rhabdomyosarcoma ewings sarcoma ( pelvic ) uterine cervix rhabdomyosarcoma hodgkins lymphoma ewings sarcoma hodgkins lymphoma metastatic medulloblastoma hodgkins lymphoma alveolar rhabdomyosarcoma embryonal rhabdomyosarcoma ewings sarcoma undi erentiated sarcoma wilms tumour abdominal embryonal rhabdomyosarcoma 149 149 113 137 110 164 140 121 127 152 105 120 123 laparoscopic cortical strip procedure failed laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip laparoscopic cortical strip oophorectomy laparoscopic cortical strip laparoscopic cortical strip oophorectomy none none none none none none none none none none none none none none none none none none none none none 158 166 158 156 147 122 302 256 245 289 217 131 156 175 172 152 143 169 135 134 all tissue was collected before chemotherapy ( with or without radiotherapy ) were given , apart from patients 1 and 11 . 
metastatic deposits identi ed on cortical strip . table : characteristics and ovarian function for patients who underwent laparoscopy for fertility preservation , by patient number in the o ered group ( or one [ 5% ] of 20 who had their ovarian tissue cryopreserved ) were deceased at the time of analysis , compared with 81 ( 22% ) of 376 in the noto ered group ; thus , overall this criterion was met . 13 patients declined the o er of ovarian tissue cryopreservation . 
the most common reason for this decision ( in nine cases ) was that both the medical team and the patients parents believed that she was too unwell to undergo an additional laparoscopic procedure . 
 for the remaining patient , who had a vaginal rhabdomyosarcoma , the parents decided against the procedure because there was a high chance that their daughter would receive radiation to her pelvis and uterus at a very young age , making it highly unlikely that she would be able to carry a pregnancy successfully in the future . not oered ovarian cryopreservation oered ovarian cryopreservation years since diagnosis number at risk oered group not oered group figure 2 : cumulative probabilities of not having premature ovarian insu ciency discussion the results of our analysis show that the edinburgh selection criteria accurately predict which girls and young women will or will not develop premature ovarian insu ciency . 
these ndings validate the use of these criteria cryopreservation before the start of cancer treatment . for patient selection for ovarian tissue high survival following childhood cancer has led to an increased focus on the late e ects of treatment , 19 , 20 and the e ect of cancer treatment on fertility is a prime concern to vol 15 september 2014 1133 articles panel 2 : research in context systematic review for prepubertal girls and young women with cancer who are unwilling to delay the start of chemotherapy , cryopreservation of ovarian tissue is the only fertility preservation option available . 
most girls and young women treated for cancer will retain a window of opportunity for fertility in the future once they have survived their original cancer , dependent on the nature of the patients planned treatment ( which might change dependent on their response ) .4 the identi cation of those patients who are at the highest risk of loss of fertility , thus justifying the use of an invasive experimental approach , is crucial . 
no previous study has addressed the accuracy and safety with which this procedure can be o ered to girls and adolescents with cancer who are at highest risk of developing premature ovarian insu ciency . 
 interpretation we have shown that the edinburgh selection criteria predict which young female patients with cancer are more likely to develop premature ovarian insu ciency and are therefore most likely to bene t from ovarian tissue cryopreservation . 
a minority of girls and young women with cancer are at high risk of premature ovarian insu ciency and , because this approach remains experimental , 7 it is necessary to limit ovarian tissue cryopreservation to those patients at high risk of premature ovarian insu ciency . 
through the application of our criteria , we have o ered ovarian tissue cryopreservation to all but one of our patients who have gone on develop premature ovarian insu ciency so far . 
we believe that the edinburgh selection criteria provide a solid scienti c basis for the identi cation of patients at risk of premature ovarian insu ciency and to whom this invasive procedure may be o ered ( panel 2 )  . some girls and young women treated for cancer are at risk of premature ovarian insu ciency and infertility . 
 overall , data from the childhood cancer survivor study14 suggest that the relative risk of premature ovarian insu ciency is roughly 13 by age 40 years , compared with sibling controls , although 92% of survivors did not have premature ovarian insu ciency by that age.22 however , survivors who have not developed premature ovarian insu ciency are still at increased risk of infertility , 14 as are women treated for cancer in adulthood.23 accurate identi cation of girls and young women at high risk of premature ovarian insu ciency is important so as to allow the application of an experimental technique to those patients most likely to bene t in the long term . we have o ered ovarian tissue cryopreservation for more than 15 years to selected female patients at our regional childrens cancer centre . 
the key selection criteria are the expected e ect of proposed treatment on ovarian function , and the likelihood of survival , as well as surgical considerations with respect to the safety of the procedure . 
the e ect of treatment can be classi ed by risk , 24 with high - risk treatment involving high doses of alkylating agent - based treatment or abdominopelvic irradiation . 
development of the treatment plan in all cases allowed a decision about the risk of premature ovarian insu ciency , but disease response or relapse will often require the treatment plan to be revised . 
this issue is exempli ed by the single patient in the group not o ered cryopreservation who developed premature ovarian insu ciency : she did not meet the criteria for ovarian tissue cryopreservation at the time of original diagnosis , but when she presented with a relapse she was believed to be too unwell to justify the surgical intervention needed . 
the ovarian tissue cryopreservation procedure was done successfully , but shortly after the procedure the diagnosis was changed to mllerian adenosarcoma , and she did not need any potentially gonadotoxic treatment . 
 this patient was therefore not at high risk of premature ovarian insu ciency , but she is nevertheless included in this analysis because the initial assessment was made on the basis of the initial ( later revised ) diagnosis ; the key issue is that the assessment has to be based on the intended treatment plan . although the duration of follow - up in the present analysis is up to 166 years , for many of the patients the duration is much less ( as little as a few months ) , so additional young women survivors might develop premature ovarian insu ciency with time . 
continued follow - up is therefore necessary to test whether the substantial di erence in prevalence of premature ovarian 1134 vol 15 september 2014 articles insu ciency between the group o ered cryopreservation and that not o ered it at this point persists , or perhaps widens further , and to allow assessment of other outcomes such as fertility . although the diagnosis of premature ovarian insu ciency used in our analysis is robust , the data are limited by the large number of patients for whom ovarian function could not be determined ( because some patients were still at a prepubertal age , some were using hormonal contraception , and some did not have information about ovarian function in their medical records )  . 
anti - mllerian hormone is not established as part of the diagnosis of premature ovarian insu ciency , but might become a useful biomarker in children because it is measurable in girls of all ages and shows a progressive rise through childhood.25 the concentration of anti - mllerian hormone falls during cancer treatment in prepubertal and adolescent girls13 as it does in adults , 26 with clearly divergent patterns of recovery after treatment completion in accordance with gonadotoxicity risk.13 , 27 measurement of anti - mllerian hormone even in prepubertal cancer survivors might thus be of diagnostic value for the identi cation of individuals with premature ovarian insu ciency in whom early sex steroid treatment can be introduced for induction of puberty . the inability to con rm or refute premature ovarian insu ciency in some women might have biased our analysis . 
all women taking hormonal contraception were taking it to prevent pregnancy rather than as hormone replacement , although premature ovarian insu ciency might have developed after the start of oral contraceptive use in some individuals , and therefore gone undetected in our analysis . 
thus , although the group not o ered some cryopreservation ( prepubertal , oral contraceptive users , or those with information about ovarian function ) might have premature ovarian insu ciency that we were unable to identify , identi cation of these cases would be very unlikely to give a similar prevalence of premature ovarian insu ciency to that in the group who were o ered the procedure . individuals within incomplete reimplantation of ovarian tissue has resulted in successful pregnancies in some adult women , con rming the potential of this approach.5 no cases have been reported of pregnancy after ovarian tissue cryopreservation in childhood or adolescence . 
however , ndings from a recent study in an ovine model28 have shown that grafting immature ovarian tissue can restore spontaneous puberty and fertility , 28 and a mature oocyte at metaphase ii has been derived from a prepubertal ovarian biopsy sample xenografted into a mouse.29 in our study population , none of the young women has yet requested use of their stored tissue , nor are we aware of such use for fertility elsewhere . 
the authors of two case reports30 , 31 have described the replacement of ovarian tissue in adolescents for the purpose of oestrogen production for pubertal induction ; 30 , 31 we do not believe that the use of such a scarce resource is appropriate for this purpose.32 the evidence of successful ( if short - lived ) hormone production by the ovarian autografts in those reports does , however , suggest that follicular development is possible , potentially allowing for oocyte maturation , ovulation , and fertility . in conclusion , our data show that speci c selection criteria can be applied at diagnosis to girls and young women with cancer to identify the fairly small proportion of patients who are likely to survive but are at high risk of premature ovarian insu ciency . 
whether ovarian tissue cryopreservation can give an opportunity for fertility in the future for these patients still needs to be determined . contributors whbw contributed to study design , data analysis , and the drafting and revision of the report . 
 raa contributed to study design , data analysis , and the drafting and revision of the report . declaration of interests we declare no competing interests . acknowledgments this study was partly funded by the uk medical research council grant g1100357 ( to raa )  . 
we thank andrew jd wallace and andrea bischof - renner for their help with data collection , louise bath and fraser munro for the care of and provision of fertility preservation to the patients in the study , and george galea for the safe storage of ovarian tissue . correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
we assessed whether rituximab use could delay the need for chemotherapy or radiotherapy compared with watchful waiting and the e ect of this strategy on quality of life ( qol )  . methods asymptomatic patients ( aged 18 years ) with low - tumour - burden follicular lymphoma ( grades 1 , 2 , and 3a ) were randomly assigned centrally ( 1 : 1 : 1 ) , by the minimisation approach strati ed by institution , grade , stage , and age , to watchful waiting , rituximab 375 mg / m weekly for 4 weeks ( rituximab induction ) , or rituximab induction followed by a maintenance schedule of 12 further infusions given at 2 - monthly intervals for 2 years ( maintenance rituximab )  . 
there was a signi cant di erence in the time to start of new treatment , with 46% ( 95% ci 3953 ) of patients in the watchful waiting group not needing treatment at 3 years compared with 88% ( 8392 ) in the maintenance rituximab group ( hazard ratio [ hr ] 021 , 95% ci 014031 ; p < 00001 )  . 
78% ( 95% ci 6987 ) of patients in the rituximab induction group did not need treatment at 3 years , which was signi cantly more than in the watchful waiting group ( hr 035 , 95% ci 022056 ; p < 00001 ) , but no di erent compared with the maintenance rituximab group ( 075 , 041134 ; p = 033 )  . 
compared with the watchful waiting group , patients in the maintenance rituximab group had signi cant improvements in the mental adjustment to cancer scale score ( p = 00004 ) , and illness coping style score ( p = 00012 ) between baseline and month 7 . 
 there were 18 serious adverse events reported in the rituximab groups ( four in the rituximab induction group and 14 in the maintenance rituximab group ) , 12 of which were grade 3 or 4 ( ve infections , three allergic reactions , and four cases of neutropenia ) , all of which fully resolved . interpretation rituximab monotherapy should be considered as a treatment option for patients with asymptomatic , advanced - stage , low - tumour - burden follicular lymphoma . funding cancer research uk , lymphoma research trust , lymphoma association , and roche . low - grade introduction findings from retrospective analyses of asymptomatic lymphoma patients with advanced - stage , showed no reduction in overall survival when systemic treatment was deferred until development of symptoms or organ failure , 1 , 2 which generally occurred about 30 months after diagnosis . 
these ndings were subsequently con rmed in three randomised trials.35 in the largest of these trials , 3 309 patients were randomly assigned to either watchful waiting or an intensive chlorambucil regimen . 
at a median follow - up of 16 years , there was no survival advantage to early start of treatment , and at 10 years , 19% of patients still did not need advanced - stage , chemotherapy . 
these trial data support the widely practised strategy of watch and wait in asymptomatic low - tumour - burden patients with follicular lymphoma , which is based on the assumption that the delay in exposure to chemotherapy and its attendant side - e ects would result in an improved quality of life ( qol )  . 
this assumption has not been formally assessed , and there is anecdotal evidence that in some patients this strategy can lead to a worse qol because patients nd being diagnosed with a malignant disorder without receiving treatment psychologically demanding . rituximab is a chimeric monoclonal antibody directed against cd20 . 
low tumour burden was de ned as normal lactate dehydrogenase , largest nodal or extranodal mass less than 7 cm , up to three nodal sites containing nodes with a diameter greater than 3 cm , no clinically signi cant serous e usions detectable by physical examination or ct scan , and spleen enlargement up to 16 cm by ct . this trial was overseen by an independent trial steering committee and independent data monitoring committee . 
 the protocol was approved by the uk medicines and articles of sydney , sydney , nsw , australia ( prof k bradstock phd ) correspondence to : dr kirit m ardeshna , department of haematology , university college hospital , 250 euston road , london nw1 2pg , uk kirit.ardeshna@uclh.nhs.uk for the trial protocol see trialprotocols.aspx 484 patients enrolled 21 excluded 8 reasons unknown 7 not eligible 1 stage 1 disease 5 high tumour burden 1 reason not stated 3 physician started treatment 1 second malignancy discovered 1 consent withdrawn 1 diagnosis revised to mantle - cell lymphoma 463 patients randomly assigned 187 patients assigned to watch and wait * 84 patients assigned to rituximab induction 192 patients assigned to maintenance rituximab * 2 stopped early because of toxicity 1 missing information 1 missing information 81 received four infusions 191 received four induction infusions 36 stopped early 156 received 12 maintenance infusions 187 included in intention - to - treat population 84 included in intention - to - treat population 192 included in intention - to - treat population figure 1 : trial pro le on sept 30 , 2007 , recruitment into the rituximab induction group was closed and the study was amended to a two - arm study . 
 * inclusive of the patients enrolled in the three - arm study ( 83 in the watch and wait group and 85 in the maintenance rituximab group )  . vol 15 april 2014 articles healthcare products regulatory agency and cambridge south research ethics committee , and was done in accordance with the declaration of helsinki and the eu clinical trials directive . 
all patients provided written informed consent before enrolment . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to be carefully observed until treatment was needed ( watchful waiting ) , to receive rituximab induction , or to receive maintenance rituximab . 
some percentages do not total 100% because of rounding . table 1 : demographics and baseline characteristics procedures patients randomly assigned to the rituximab induction group received intravenous rituximab ( 375 mg / m ) every week for 4 weeks ( rituximab induction ) , while those in the maintenance rituximab group received the same rituximab induction followed by 12 infusions of rituximab given at 2 - monthly intervals for 2 years . 
no dose reductions were recommended . clinical assessments including full blood count and renal and liver function tests were done at baseline , 1 month , and then every 2 months for 2 years or until start of treatment . 
a bone marrow trephine biopsy was taken for restaging only if patients were in complete remission or uncon rmed complete remission on radiological assessment at month 7 , 13 , or 25 , or before starting rst chemotherapy or radiotherapy . safety data were collected while patients in the rituximab induction and maintenance groups were on treatment with rituximab and for up to 30 days afterwards unless a late complication of rituximab was reported . qol was assessed at baseline ( before randomisation ) , after randomisation ( within 1 week and before treatment ) , at each clinic visit during the rst 2 years , and then every 6 months for 2 years . 
the questionnaires used were the functional assessment of cancer therapygeneral ( fact - g ) , hospital anxiety and depression scale ( hads ) , impact of event scalerevised , and questions from the illness coping style , illness impact bank , and mental adjustment to cancer scale together with four additional questions relating to lymphoma ( appendix )  . and scales summary subscales or emotional wellbeing , for each qol questionnaire were derived according to their score manuals . 
there are four subscales of the fact - g questionnaire : physical wellbeing , social or family wellbeing , functional wellbeing , each scored 0100 , with higher scores suggesting better qol . 
the hads is summarised by anxiety and depression subscales , which are classi ed as normal ( score 07 ) , borderline ( score 810 ) , and case ( score 1114 )  . 
there are 27 items in the impact of event scalerevised questionnaire , which are summarised as avoidance , intrusions , and hyperarousal subscales ; scores of all subscales are scaled as 0100 , with higher scores suggesting better qol . 
one summary measure each is derived from the illness coping style , the illness impact bank , and the mental adjustment to cancer 426 vol 15 april 2014 articles scale questionnaires ; scores of each are scaled as 0100 , with higher scores suggesting better qol . outcomes the primary outcome measures were the time to start of new treatment and qol at month 7 ( 6 months after completion of induction treatment )  . 
progression - free survival and time to histological transformation were analysed post hoc . time to start of new treatment was calculated from the date of randomisation to the date of starting new systemic chemotherapy or radiotherapy . 
 we recognised that de ning clearly when disease progression is su cient to warrant the start of chemotherapy or radiotherapy is di cult and so we provided a detailed guidance ( appendix )  . 
standard criteria for response assess ment were used.8 survival was de ned as time from random isation to death from any cause ( overall survival ) or progression or death from any cause ( progression - free survival )  . 
 statistical analysis with an estimated median time to start of new treatment of 30 months in the watchful waiting arm , the original three - arm trial was designed to detect an improvement in the median time to start of new treatment in each of the rituximab groups of 18 months ( from 30 to 48 months ) with a 25% signi cance level ( allowing for the multiple comparisons ) and 90% power . 
recruitment of 600 patients was planned . on sept 30 , 2007 , about 3 years after the start of enrolment , recruitment into the rituximab induction group was closed because of a low recruitment rate and because other studies had shown a bene t of maintenance rituximab compared with watchful waiting after induction with rituximab with or without chemotherapy , 9 , 10 although in only one of these studies was the rituximab induction administered as a monotherapy . 
this change was approved by the independent trial steering committee , independent data monitoring committee , and regulatory and ethics committees . for the two - arm trial , the study was redesigned to detect an improvement in the median time to start of new treatment in the maintenance rituximab arm of 18 months ( from 30 to 48 months ) with a 5% signi cance level and 90% power . 
recruitment of 360 patients was planned . the primary analysis was done using an unstrati ed log - rank test for the di erence in the distribution of time to start of new treatment between the di erent groups . 
interaction analyses were done to assess the di erence in the size of treatment e ects in subgroups classi ed according to age , sex , stage , follicular lymphoma international prognostic index , 11 and 2 microglobulin concentration . 
however , on march 26 , 2010 , the independent data monitoring committee concluded that the data regarding the clinical primary outcome measure were mature and suitable for full analysis and publication . 
this decision was approved by the independent trial steering committee . watch and wait overall remission spontaneous complete remission spontaneous partial remission uncon rmed complete response no change disease progression rituximab induction overall response complete response partial response no change disease progression maintenance rituximab overall response complete response partial response no change disease progression data are n / n ( % )  . 
 the change in qol from baseline to month 7 within each arm was also compared between the arms and this was judged to be the most important comparison . except for anxiety or depression subscales , a change of 5 points for a subscale was regarded as the minimum clinically signi cant di erence . 
statistical analyses were done using sas version 9.2. this study is registered with clinicaltrials.gov , nct00112931 , and eudract , 2004 - 001621 - 16 . role of the funding source the trial sponsor ( university college london ) was responsible for randomisation , data collection , entry , and validation ; monitoring procedures ; reporting of serious adverse events ; organisation of central pathological review ; liaison with investigators ; data analysis ; and writing of the report . 
roche , the lymphoma association , and the lymphoma research trust had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between oct 15 , 2004 , and march 25 , 2009 , 463 patients were randomly assigned from 118 centres in the uk , australia , new zealand , turkey , and poland . 
252 patients were randomly assigned in the original three - arm study ( 83 to the watchful waiting group , 84 to the rituximab induction group , and 85 to the maintenance rituximab group )  . 
in the two - arm study , 379 patients were randomly assigned between the watchful waiting group ( n = 187 ) and the maintenance rituximab group ( n = 192 ; gure 1 )  . 
 a time to start of new treatment b progression - free survival watch and wait maintenance rituximab hr 021 ( 95% ci 014031 ) log - rank p < 00001 number at risk watch and wait maintenance rituximab hr 023 ( 95% ci 016032 ) log - rank p < 00001 c overall survival d time to histological transformation hr 073 ( 95% ci 034154 ) log - rank p = 040 number at risk watch and wait maintenance rituximab hr 062 ( 95% ci 031126 ) log - rank p = 019 years from randomisation years from randomisation figure 2 : kaplan - meier curves for the two - arm study ( a ) time to start of new treatment , ( b ) progression - free survival , ( c ) overall survival , and ( d ) time to histological transformation . 
 428 vol 15 april 2014 articles a time to start of new treatment b progression - free survival watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 035 ( 95% ci 022056 ) ; log - rank p < 00001 maintenance rituximab vs rituximab induction hr 075 ( 95% ci 041134 ) ; log - rank p = 033 number at risk watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 055 ( 95% ci 037083 ) ; log - rank p = 00034 maintenance rituximab vs rituximab induction hr 053 ( 95% ci 032087 ) ; log - rank p = 0011 c overall survival d time to histological transformation rituximab induction vs watch and wait hr 104 ( 95% ci 039280 ) ; log - rank p = 093 maintenance rituximab vs rituximab induction hr 112 ( 95% ci 043290 ) ; log - rank p = 082 years from randomisation number at risk watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 034 ( 95% ci 011106 ) ; log - rank p = 0052 maintenance rituximab vs rituximab induction hr 147 ( 95% ci 042522 ) ; log - rank p = 055 years from randomisation figure 3 : kaplan - meier curves for the 252 patients randomly assigned in the initial three - arm study ( a ) time to start of new treatment , ( b ) progression - free survival , ( c ) overall survival , and ( d ) time to histological transformation . 
 the 4 - week rituximab induction was administered to all patients except for two patients in the rituximab induction group who only received one and three infusions , respectively , because of toxicity . 
 maintenance was stopped because of progressive disease or new treatment ( n = 13 ) ; other illness taking priority or resulting in death ( n = 5 ) ; infection ( n = 3 ) ; patient choice ( n = 6 ) ; reclassi cation as di use large b - cell lymphoma ( n = 1 ) ; neutropenia ( n = 3 ) ; or uncertain reasons ( n = 2 )  . 
there were no dose reductions . 18 serious adverse events occurred in the two rituximabcontaining groups , which were considered possibly , probably , or de nitely related to the rituximab : nine infections ( induction group n = 1 , maintenance group n = 8 ) , ve allergies ( induction group n = 3 , maintenance group n = 2 ) , and four neutropenia ( all in the maintenance group )  . 
there were ve grade 3 infections in the maintenance rituximab group ( two pneumonia , one viral meningitis , one de - novo hepatitis b infection , and one urinary tract infection )  . 
 vol 15 april 2014 articles the fourth patient developed grade 3 neutropenic sepsis 5 months after randomisation and was treated with antibiotics and granulocyte colony - stimulating factor and the rituximab was stopped . 
there were no other grade 3 or 4 adverse events . the rate of spontaneous remissions in the watchful waiting group was low : by month 25 , only 15 ( 12% ) of 128 patients had shown radiological regressions over 50% ( ie , overall remission ) , with only eight ( 6% ) patients having a spontaneous complete remission or uncon rmed spontaneous complete remission . 
162 ( 88% ) of 184 patients in the maintenance rituximab group had had a response at 7 months , as had 144 ( 83% ) of 173 at 25 months . 
 radiologically identi ed complete responses , or un conrmed complete responses , were noted in 109 ( 59% ) of 184 patients at month 7 and in 130 ( 75% ) of 173 patients at month25 ( table 2 )  . analysis of the 252 patients recruited to the three - arm study showed that there were signi cantly more overall responses in the maintenance rituximab group than in the rituximab induction group at both month 7 ( 77 / 85 [ 91% ] vs 62 / 81 [ 77% ] ; p = 0043 ) and month 25 ( 67 / 80 [ 84% ] vs 43 / 75 [ 57% ] ; p = 0001 ; appendix )  . 
 investigator compliance with bone marrow examination when a radiological complete remission or uncon rmed complete remission was achieved was suboptimum ; incorporation of these ndings underestimated rates of complete remission or uncon rmed complete remission ( appendix )  . 
 in the two - arm study , 105 ( 56% ) of 187 patients in the watchful waiting group and 33 ( 17% ) of 192 patients in the maintenance rituximab group needed new treatment ; the reason for starting new treatment was disease progression except for six ( 4% ) patients ( three watch and wait ( n = 187 ) rituximab induction ( n = 84 ) maintenance rituximab ( n = 192 ) total breast lung colorectal squamous cell stomach prostate basal - cell carcinoma melanoma pancreas unknown primary hodgkins lymphoma total table 3 : list of second malignancies patient choice in the watchful waiting group , one clinician choice in the watchful waiting group , and one in each group reclassi ed as di use large b - cell lymphoma )  . 
 the estimated median time to start of new treatment was 311 months ( 95% ci 255460 ) in the watchful waiting group and has not been reached in the maintenance rituximab group . 
at 3 years , the estimated percentage of patients not needing new treatment was 46% ( 95% ci 3953 ) in the watchful waiting group , and 88% ( 8392 ) in the maintenance rituximab group ( hr 021 , 95% ci 014031 ; p < 00001 ; gure 2a )  . 
all prespeci ed patient subgroups showed prolongation of time to start of new treatment with maintenance rituximab . in the three - arm study , 97 of 252 patients randomly assigned into the three - arm study needed to start new treatment : 52 ( 63% ) of 83 in the watchful waiting group , 25 ( 30% ) of 84 in the rituximab induction group , and 20 ( 24% ) of 85 in the maintenance rituximab group . 
for patients randomly assigned to the rituximab induction group , the median time to start of new treatment has not been reached and new treatment had not been started in 78% ( 95% ci 6987 ) of patients at 3 years . 
the hr was 035 ( 95% ci 022056 ; p < 00001 ) for rituximab induction versus watchful waiting and was 075 ( 041134 ; p = 033 ) for maintenance rituximab versus rituximab induction ( gure 3a )  . 
exploratory analyses of patient subgroups are summarised in the appendix . in the two - arm study , 121 ( 65% ) of 187 patients in the watchful waiting group and 43 ( 22% ) of 192 patients in the maintenance rituximab group had either developed progressive disease or died . 
median progression - free survival was 241 months ( 95% ci 171253 ) in the watchful waiting group , but has not yet been reached in the maintenance rituximab group . 
3 - year progression - free survival was 36% ( 95% ci 2943 ) in the watchful waiting group and 82% ( 7788 ) in the maintenance rituximab group ( hr 023 , 95% ci 016032 ; p < 00001 ; gure 2b )  . in the three - arm study , 41 ( 49% ) of 84 patients in the rituximab induction group had either developed progressive disease or died . 
3 - year progression - free survival was 60% ( 95% ci 4971 ) in the rituximab induction group , which was signi cantly di erent from the other two arms : hr 053 ( 95% ci 032087 ; p = 0011 ) for the comparison between maintenance rituximab and rituximab induction and hr 055 ( 037083 ; p = 00034 ) for the comparison between rituximab induction and watchful waiting ( gure 3b ; appendix )  . in the two - arm study , 28 ( 7% ) of 379 patients had died : 16 ( 9% ) of 187 in the watchful waiting group and 12 ( 6% ) of 192 in the maintenance rituximab group . 
eight patients died in the rituximab induction group , giving a 3 - year overall survival of 96% ( 95% ci 92100 ) , with no di erence between the three groups ( gure 3c ; appendix )  . 
six second malignancies occurred in the rituximab induction group , two were fatal ( table 3 )  . by data cuto ( sept 8 , 2012 ) , 33 patients had had biopsy - proven transformation in the two - arm study ( 20 [ 11% ] of 187 in the watchful waiting group and 13 [ 7% ] of 192 in the maintenance rituximab group )  . 
a further four patients have had biopsyproven transformation in the rituximab induction group , with no evidence of di erences between the rituximab group and the other groups in the three - arm study ( gure 3d ; appendix )  . time table 4 summarises the qol results for the two - arm study at month 7 . 
there was a signi cant improvement in the mental adjustment to cancer scale score from baseline to month 7 in the maintenance rituximab group ( p = 00001 ) that did not occur in the watchful waiting group ( p = 019 )  . 
compared with baseline , scores at month 7 for the illness coping style were much the same in the maintenance rituximab group ( p = 0072 ) and deteriorated in the watchful waiting group ( p = 00063 )  . 
 patients in the maintenance rituximab group were also signi cantly less worried about the need for treatment or more treatment than patients in the watchful waiting group by month 7 compared with baseline ( p = 00037 )  . 
 there were no other clinically signi cant di erences between the two arms in all other qol measures between baseline and month 7 ; all measures either improved or remained unchanged between baseline and month 7 ( table 4 )  . this di erence was signi cant in the three - arm study , there was no evidence of di erence in qol between baseline and month 7 when the rituximab induction group was compared with the watchful waiting group . 
in accordance with these data , more patients in the watchful waiting group had started new treatment compared with those in the rituximab induction group , and also compared with those in the maintenance rituximab group . 
the nding that the administration of rituximab delayed progression and time to start of new treatment is not surprising , but the magnitude of remarkable , with more than three times fewer patients needing treatment by 3 years in the maintenance rituximab group than in the watchful waiting group . 
the di erence between the time to start of new treatment in the rituximab induction and maintenance groups was not signi cant , but the start of new treatment lags behind progression and once the trial was amended to two arms , the trial was underpowered for the comparison of the two rituximab groups . this e ect longer follow - up is needed to ascertain the median time to progression and time until new treatment becomes necessary in the rituximab - containing groups , but three other studies are relevant to this issue . 
colombat and colleagues6 updated the results of their phase 2 study in patients with previously untreated low - tumour - burden follicular lymphoma who received infusions of rituximab induction without maintenance every 4 weeks . 
in the sakk 35 / 98 study , 9 , 10 standard rituximab induction was administered and patients were randomly assigned to observation or four further doses of rituximab given at 2 - monthly intervals . 
in the subgroup of previously untreated patients ( not all asymptomatic or with low tumour burden ) who responded to induction , 22% remained event free without maintenance at 8 years compared with 45% in the maintenance group . 
similarly , in the resort study , 12 the proportion of patients remaining free of cytotoxic treatment at 3 years was signi cantly greater receiving extended maintenance rituximab than in those receiving rituximab re - treatment upon progression . those in the present study , we chose time to start of new treatment rather than progression - free survival as the primary endpoint . 
we acknowledge that there is some subjectivity as to when treatment is needed , even when guidance is provided , but oncologists are familiar with making this decision in routine clinical practice and this pragmatic endpoint is of greatest relevance to the patient . 
 the de nition of progression covers a wide spectrum of clinical scenarios , some of which would not warrant the start of treatmenteg , the appearance of a new small nodethus reducing its utility in patients with indolent lymphoma . 
 * worsened or stayed as very much , quite a bit , or somewhat . table 4 : quality of life at baseline and month 7 from randomisation duration after rst new treatment as well as time to second new treatment . 
preliminary data from the us lymphocare study14 suggest that the time to second systemic treatment is signi cantly longer in patients who received rituximab monotherapy than in those who were initially on watchful waiting . 
the estimated 5 - year overall survival in the watchful waiting arm in the present study is over 90% , which compares favourably with the 58% in our previous study.35 this di erence , in the space of fewer than two decades , is substantial and probably due in baseline patient characteristics between the two studies and newer treatment options that have become available . 
for example , in our initial study , bulk disease per se was not an exclusion criterion , there was no requirement for a to di erences treatment in the watchful waiting group was very close to that reported in previous studies1 , 35 further shows the reproducibility of this endpoint . findings from this trial also show that rituximab induction can be delivered without a reduction in qol : patients receiving maintenance rituximab actually had an improvement in some aspects of their qol when compared with those on watchful waiting . 
at month 7 , patients in the maintenance rituximab group were signi cantly more likely to feel in control of their situation than those in the rituximab induction group and the watchful waiting group , as shown by the mental adjustment to cancer scores . 
conversely , patients in the watchful waiting group were signi cantly more likely to avoid learning or thinking about their illness and to have unpleasant connotations with their clinic visits , as shown by the illness coping style scores , and to be worrying about the need for treatment than those in the maintenance rituximab group . 
therefore , the administration of rituximab does not seem to negatively a ect patients qol and patients who receive a maintenance schedule seem to feel more empowered and better adjusted to their diagnosis . 
this nding might be because these patients felt that something active was being done to combat their lymphoma , and many of them would have noticed physical evidence such as lymph nodes shrinking to suggest that this was the case . rituximab monotherapy seems to be well tolerated , with only eight cases of grade 3 infection or allergy . 
this nding might be a result of the fact that patients included in the study were well at the outset , had low tumour burden , and had not received treatment previously . 
follow - up is short so far and long - term sequelae of rituximab might appear ; however , rituximab has been in use for 15 years and the follow - up of patients treated in other trials with rituximab is extensive . so far there is no overall survival di erence between the three groups , and much longer follow - up will be needed to assess the e ect of this strategy on overall survival . 
we have extended the follow - up of this study to collect information regarding response and response vol 15 april 2014 articles panel : research in context systematic review we searched pubmed from january , 1987 , until august , 2013 , for randomised trials published in english with the terms lymphoma and watchful waiting or observation or delayed treatment . 
we found three randomised studies , 35 each of which showed no survival bene t when systemic treatment was started immediately in patients with advanced - stage asymptomatic low - tumourburden low - grade lymphoma compared with a watchful waiting approach in which treatment was deferred until disease progression . 
there were no other studies comparing watchful waiting with the administration of rituximab monotherapy in this patient group . interpretation in this study , we show that rituximab monotherapy is e ective at deferring disease progression and the need for chemotherapy or radiotherapy in patients with asymptomatic low - tumour - burden follicular lymphoma , and when administered as a maintenance schedule it can be delivered with minimum toxicity and results in improved quality of life compared with watchful waiting . 
however , probably the most important reason for the improvement in overall survival is the routine therapeutic use of monoclonal antibodies . with a median follow - up of nearly 4 years , there was no di erence in the incidence of histological transformation between the three groups . 
previous retrospective studies have di ered as to whether a watchful waiting approach increased the risk of transformation ; that a di erence will emerge is not inconceivable and further follow - up is clearly necessary.15 , 16 we found that maintenance rituximab compared with rituximab induction had a numerically greater e ect on time to initiation of new treatment in women than in men . 
although the heterogeneity of to sex was not signi cant , response with regard gisselbrecht and colleagues17 also found that maintenance rituximab improved overall survival when compared with observation in women , but not in men , when administered after autologous stem - cell transplantation for relapsed refractory di use large b - cell lymphoma . 
the reason for this nding is unclear , but might relate to the di erential clearance of rituximab from the serum between the sexes.18 management options for patients with low - tumourlymphoma burden are varied and include watchful waiting , immediate asymptomatic follicular that rituximab time . 
in this study we show induction alone can delay chemotherapy and is not signi cantly less e ective than a m aintenance schedule ; however , the number of responses was lower and the rate of progression after induction alone was signi cantly higher than that after maintenance . 
thus , a di erence in time to start of new treatment will probably emerge between these two the cost approaches with associated with the administration of maintenance rituximab over 2 years and that the use of rituximab induction alone was attractive in terms of reduced number of hospital visits for administration of rituximab and cost , but the improvements in qol that occurred with the maintenance schedule did not occur for rituximab induction alone . 
this absence in improvement of qol might have been because the amended study was not powered su ciently to show a qol di erence between the rituximab induction group and the watchful waiting group . 
however , despite this factor , patients receiving maintenance rituximab still had a signi cant improvement in their mental adjustment to cancer score between baseline and month 7 compared with those receiving rituximab induction alone , suggesting a qol bene t of the maintenance approach between randomisation and month 7 . watchful waiting might still be appropriate for some patients . 
we have previously shown that 40% of patients over 70 years of age will never need any treatment and will not die of their lymphoma ; 3 however , this nding must be balanced against the improved qol achieved with maintenance rituximab . 
 furthermore , by administering rituximab to the whole group of patients older than 70 years , an even larger cohort might never need chemotherapy , which would be advantageous in view of the comorbidities and the reduced ability to withstand the side - e ects of treatment in this age group . 
if watchful waiting is used , clinicians will need to be alert to whether the patient is anxious that no treatment is experiencing feelings of is being administered , helplessness , or is having di culty adjusting to their diagnosis . 
if these are substantial concerns then the treatment approach should be reconsidered . in conclusion , our results suggest that rituximab monotherapy should be regarded as a standard approach in the management of many patients with asymptomatic , low - tumour - burden follicular lymphoma . 
the full results of other studies that address the optimum schedule of rituximab monotherapy administration , such as the resort study , 12 are awaited with interest . 434 vol 15 april 2014 articles contributors kma and dcl designed the study , interpreted data , and wrote and approved the report . 
all authors have reviewed and approved the nal version of the report . declaration of interests kma has received funding from roche for being an advisory board member , speaker , and data manager , and for travel and accommodation at international conferences . 
dcl has been chair of an oversight committee for cellmedica , adviser for cellectsis , an advisory board member and speaker for roche and chugai , and an advisory board member for millenniuwq , ps , nb , ll , pp , jwar , ls , fm , rs , bf , and kb declare that they have no competing interests . acknowledgments roche provided rituximab free of charge . 
dc recieves funding from the national institute for health research biomedical centre at the royal marsden hospital . corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 corrections correction to lancet oncol 2013 ; 14 : 1242 correction to lancet oncol 2014 ; 15 : 606 correction to lancet oncol 2014 ; 15 : 621 rst - line metastatic rini bi , melichar b , ueda t , et al . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in figure 1 of this article , the box indicating how many patients received the intervention should have read : 652 patients received intervention . 
 this change has been made to the online version as of may 26 , 2014 . vol 15 june 2014 e253 corrections correction to lancet oncol 2013 ; 14 : 1242 correction to lancet oncol 2014 ; 15 : 606 correction to lancet oncol 2014 ; 15 : 621 rst - line metastatic rini bi , melichar b , ueda t , et al . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in figure 1 of this article , the box indicating how many patients received the intervention should have read : 652 patients received intervention . 
 this change has been made to the online version as of may 26 , 2014 . vol 15 june 2014 e253 correction to lancet oncol 2016 ; 17 : 23442 correction to lancet oncol 2016 ; 17 : e506 shaw at , gandhi l , gadgeel s , et al , on behalf of the study investigators . 
 lancet oncol 2016 ; 17 : e50209the fourth sentence of the biosimilar monoclonal antibodies in oncology section should have read , the primary endpoint , overall response rate , at week 24 was equivalent between groups ( 70% for myl - 1401o vs 64% for trastuzumab ) , and the risk ratio was 109 ( 90% ci 097121 )  . 
this correction has been made to the online version as of march 1 , 2017 . vol 18 march 2017 e134 corrections corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2017 ; 18 : e142 correction to lancet oncol 2017 ; 18 : e81 , e82 , e86 burki tk . 
this correction has been made to the online version as of march 2 , 2017 . published online march 2 , 2017 s1470 - 2045 ( 17 ) 30173 - 0 published online march 2 , 2017 s1470 - 2045 ( 17 ) 30175 - 4 rl , cancer cancer and survivors : childhood adolescent , r , mulder al . 
recommendations kremer skinner for lc , in male gonadotoxicity surveillance young childhood , report adult international late effects from the guideline harmonization group in collaboration with the pancaresurfup consortiu lancet oncol 2017 ; 18 : e7590in this review , the sixth paragraph under the who needs surveillance ? heading should have read there is probably no increased risk after treatment with cyclophosphamide , busulfan or cyclophosphamide or fludarabine and melphalan , hsct conditioning , and ifosfamide , and mechlorethamine , cisplat additionally , the key for figure 2 should have been light orange for moderate recommendation to do and dark orange for weak recommendation do . 
these corrections have been made to the online version as of march 29 , 2017 . procarbazine vol 18 april 2017 e196 corrections editorial see cancer and society page 812 see articles page 813 see articles lancet 2013 ; published online july 20 . 
 s0140 - 6736 ( 13 ) 61167 - 8 see news lancet respir med 2013 ; 1 : 12 see news lancet respir med 2013 ; published online july 4 . 
 s2213 - 2600 ( 13 ) 70141 - 3 cleaning our polluted skies in this issue of the lancet oncology , ole raaschou - nielsen and colleagues report data from the european study of cohorts for air pollution e ects ( escape ) , a collaboration of more than 30 european cohort studies including almost 1 million participants , which aims to quantify the health risks of air pollution . 
the researchers noted a higher risk of lung cancer , especially adenocarcinoma , with increasing exposure to coarse particulate matter ( less than 10 m in diameter ; pm10 ) , and evidence of a raised risk with increasing exposure to ne particulate matter ( less than 25 m in diameter ; pm25 )  . 
however , perhaps most alarmingly , their data suggest that the risk of lung cancer remains increased even at particulate matter concentrations below current european union ( eu ) limits , challenging existing regulations on air quality . air pollution is a major environmental problem that a ects everyone , with health e ects reaching far beyond lung cancer alone ; indeed , the escape project is also examining the e ects of air pollution on respiratory and cardiovascular diseases , and also on all - cause mortality . 
 of the six most common pollutantsparticulate matter , ground - level ozone , carbon monoxide , sulphur oxides , nitrogen oxides , and leadparticulate matter and ozone represent the greatest risk to health , particularly ne particulate matter , which can penetrate the lungs and bloodstreaa great deal of air pollution results from anthropogenic activity , with the burning of various fuels high on the list of culpritsin industry ( eg , power plants , factories , waste incinerators ) , generated by furnaces and stoves ( ie , use of traditional biomass ) , from motor vehicles , and from agricultural practices ( eg , controlled burns )  . 
 although the 2005 who air quality guidelines were designed to establish global criteria for reducing the health e ects of air pollution , there is wide variation in uptake and adherence . 
at present eu standards , for instance , are more stringent than who guidelines for both ne and coarse particulate matter ; by contrast , concentrations in the us environmental protection agencys december , 2012 , revision of the national ambient air quality standards are more liberal than those recommended by who . 
nevertheless , legislation to limit emissions from industry and transport is in place in both regions , and measures to reduce long - range pollution across country borders have been adopted . 
 for instance , china only began to monitor pm25 concentrations in beijing in october , 20122 years after the us embassy in beijing reported air quality index levels of 755 , a gure more than 20 times higher than safe limits according to who criteria . 
furthermore , it took until june this year for the chinese government to announce ten new measures to improve air quality , including plans to reduce emissions from key industries by 30% by 2017 and to monitor pollution levels in 116 other cities . 
given that recent data suggest that pollution has reduced life expectancy in northern china by as much as 55 years , these initiativesalthough conceived a little too latemust not be allowed to fail . elsewhere , political lobbying stands in the way of progress . 
for instance , burning of the rainforest by farmers to clear land in indonesia for production of palm oil resulted in concentrations of air pollutants in singapore , malaysia , and southern thailand climbing to record levels in june , 2013 . 
although indonesia has a no - burn policy , it is rarely enforced , and the country remains the only member state of the association of southeast asian nations not to have signed up to the groups agreement on transboundary haze pollution . 
 despite measures and recommendations currently in place , escape shows that the risk of lung cancer remains increased even at particulate matter concentrations below levels that are currently deemed to be safe . 
existing e orts , including new energy sources , increased legislation for industry and farming , carbon caps and o setting , and encouraging the use of greener transport and e orts to reduce the need to travel , are undoubtedly part of the solution . 
 however , new solutions are needed that are both pragmatic and e ective , and free from the in uence of competing interestsan ambition that unfortunately still eludes even the most creative ideas to date . 
 the lancet oncology vol 14 august 2013 editorial for the society of gynecological oncologys position statement see newsroom / positionstatements - 2 / morcellation / patient safety must be a priority in all aspects of care in december , 2013 , the society of gynecologic oncology ( sgo ) released a position statement regarding intracorporeal morcellation , a technique by which tissues excised during minimally invasive surgery are cut up to facilitate removal through small excisions , which might increase the risk of disseminating tumour cells . 
the statement follows the case of a harvard anaesthetist who had a hysterectomy involving intracorporeal morcellation at brigham and womens hospital , boston , ma , usa , to treat presumed benign broids , and was subsequently found to have leiomyosarcoma ; the patient is now being treated for stage iv disease . 
subsequent to this case and another similar incident at the same hospital , the chair of obstetrics and gynaecology issued a note to medical sta warning that morcellation of an occult tumour may occur in between one in 400 and one in 1000 women who have this procedurea risk at least ten times higher than previously assumed . 
in view of the strong risk of developing high - grade cancer following the procedure , this advice is prudent , but does it go far enough ? minimally invasive surgery does , of course , have major advantages and the advent of these techniques has heralded an era of shorter hospital stays , lower infection risk , quicker recovery times , reduced use of donor blood , and less scarring . 
in most areas of life , new technologies are received with an implied assumption that they are better than the device or procedure they are intended to replace , and so seems to be the case in medicine . 
 however , contrary to the situation with new drugs , medical devices do not have to undergo such rigorous testing and safety pro ling before they are propelled into everyday clinical practice by the manufacturers extensive , unregulated marketing . 
it is not practical to subject every new surgical procedure to the same trial processes as new drugs , but nevertheless structured follow - up and full reporting of adverse events should be the minimum standards . 
guidelines should err on the side of caution where hazards are reported , as has been the case with intracorporeal morcellationthe risk of disseminating malignant cells by morcellation has been shown numerous times over the past couple of decades . 
for instance , the patient information website for one manufacturers minimally invasive system extols the bene ts of the system in hysterectomy for a range of conditionsincluding cancerbut fails to mention that morcellation could spread cancer cells . 
this problem needs urgent attention , not only because hysterectomy is extremely common and a one in 400 risk of morcellating an occult tumour is unacceptable , but also because these techniques are used in a wide range of settings . 
 the lancet oncology vol 15 february 2014 corrections correction to lancet oncol 2013 ; 14 : 1242 correction to lancet oncol 2014 ; 15 : 606 correction to lancet oncol 2014 ; 15 : 621 rst - line metastatic rini bi , melichar b , ueda t , et al . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in figure 1 of this article , the box indicating how many patients received the intervention should have read : 652 patients received intervention . 
 this change has been made to the online version as of may 26 , 2014 . vol 15 june 2014 e253 corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 comment published online february 26 , 2014 s1470 - 2045 ( 14 ) 70081 - 6 see articles page 464 illidge t , specht l , yahalom j , et al . 
 clin lymphoma myeloma 2008 ; 8 : 24145 . the value of randomised trials for prostate cancer management in the lancet oncology , david dearnley and colleagues1 report the long - term outcomes of the medical research council ( mrc ) rt01 studya randomised study of 64 gy versus 74 gy of conformal radiotherapy given with 36 months of neoadjuvant or concomitant androgen deprivation therapy ( adt )  . 
in sum , an additional week of radiotherapy improves biochemical control by about 18%.2 in this trial with 843 participants , the 10 - year absolute di erence in biochemical progression - free survival was 12% ( 43% [ 95% ci 3848 ] in the standarddose group vs 55% [ 5061 ] ; hazard ratio [ hr ] 069 [ 95% ci 056084 ] ; p < 00001 ) with no signi cant di erence in overall survival ( 71% [ 95% ci 6675 ] in both groups ; hr 099 [ 95% ci 077128 ] ; p = 096 )  . although overall survival is the gold - standard outcome to improve , it is exceptionally di cult to show in localised disease diagnosed in a screendetected era when median overall survival approaches 20 years . 
notably , the swog 8794 study3 did not show an overall survival advantage when it reported its 106 year median follow - up results , despite having a high - risk postoperative population , and doing the trial early in the prostatespeci c antigen ( psa ) screening era . 
although psa is not a perfect surrogate for overall recurrence survival , clinical experience suggests that higher psa control means that more patients feel good about their disease status , and are free of next - line treatment interventions with their attendant side - e ects and costs . and as the mrc rt01 study constitutes another piece of level 1 evidence , it is likely that dose - escalated radiotherapy with short - term adt ( at least compared with lower dose radiotherapy ) will be listed as one of the options that should be o ered to men with localised prostate cancer when guidelines about management of localised prostate cancer are updated . 
 we can add this to the list of recommendations in localised prostate cancer : long - term versus shortterm or no adt for high - risk disease ; radiotherapy plus adt versus radiotherapy or adt alone for high - risk disease ; adjuvant postoperative radiotherapy versus delayed or no postoperative radiotherapy for margin - positive or extracapsular disease . 
the problem is that much of what clinicians can o er is not based on level 1 evidence , despite many attempts to design appropriate trialseg , early detection and screening ; active surveillance ; radical prostatectomy ( in screened populations ) ; robotic - assisted laparoscopic prostatectomy ( in any population ) ; low dose rate ( ldr ) brachytherapy ; high dose rate ( hdr ) brachytherapy ( compared with intensity modulated dose - escalated radiotherapy ) ; radiotherapy ; radiotherapy ; stereotactic ablative cryotherapy ; high intensity focused ultra sound ; and focal ablative therapy . 
second , and arguably more importantly , there has to be a balance of interests to do a randomised trialthe patient and supervising physician have to be uncertain as to the best treatment , unbiased ( particularly nancially ) about which treatment might be better , and for the patient , be willing to enter into the study and subject themselves to random allocation of treatment . 
third , are clinicians willing to stop innovating while they wait 20 years to design , enrol , and mature the results of each randomised controlled trial ? and predictive factors , illustrates radiotherapy the debate over ldr brachytherapy versus dosethese points . 
long - term results for ldr have shown 10 - year failure ranging from 6% ( ldr monotherapy for low and intermediate risk disease , n = 1006 ) 4 to 10% ( ldr boost for highrisk disease , n = 473 ) .5 with the same patient risk distribution as rt01 , the expected occurrence of overall biochemical failure would be 77% with ldr . 
since ldr is cheaper ( at least in canada ) , more convenient for patients , more e cient for the health - care system , and has equivalent or better quality of life , 6 is it ethical to do a randomised trial of these two options ? we need more studies like the one reported by dearnley and colleagues . 
all other treatments would need to prove ( through randomised trials ) that they are of equal or better value than those to be publicly funded . andrew loblaw odette cancer centre , sunnybrook health sciences centre , toronto , on m4n 3m5 , canada ; department of radiation oncology , and department of health policy , university of toronto , toronto , on , canada andrew.loblaw@sunnybrook.ca i have received research support from sano and paladin and honoraria from astrazeneca , elekta , ge healthcare , sano , and paladi have served on advisory boards for astellas and sano  . 
can urol assoc j 2013 ; 7 : 46370 . the bone substudy of ma.27 : does bone make a di erence ? oestrogen suppression using aromatase inhibitors is the cornerstone of adjuvant treatment for postmenopausal women with hormone receptor - positive early breast cancer.1 both non - steroidal ( anastrozole and letrozole ) and steroidal inhibitors are more e cacious than is tamoxifen for reduction of recurrence of breast cancer.24 the investigators ( exemestane ) aromatase of ma.27in which exemestane was compared with anastrozolereported no di erence for breast cancer - related outcomes between the two drugs.5 generic versions of all three aromatase inhibitors are available and are used interchangeably for adjuvant treatment of hormone - dependent early breast cancer in postmenopausal women . published online march 11 , 2014 s1470 - 2045 ( 14 ) 70050 - 6 see articles page 474 vol 15 april 2014 corrections correction to lancet oncol 2013 ; 14 : 1242 correction to lancet oncol 2014 ; 15 : 606 correction to lancet oncol 2014 ; 15 : 621 rst - line metastatic rini bi , melichar b , ueda t , et al . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in figure 1 of this article , the box indicating how many patients received the intervention should have read : 652 patients received intervention . 
 this change has been made to the online version as of may 26 , 2014 . vol 15 june 2014 e253 corrections correction to lancet oncol 2013 ; 14 : 84 correction to lancet oncol 2013 ; 14 : 99 schutz fab , pomerantz mm , gray kp , et al . 
lancet oncol 2013 ; 14 : 8187in the key and the number at risk rows in the gure ( page 84 ) , aa or gg should have read aa or ag . 
bevacizumab in breast cancer : fundamental questions rema lancet oncol 2013 ; 14 : 99101in this comment , the third sentence the second paragraph should have read the investigators chose a non - inferiority study design with a boundary of 133 for hazard ratio ( hr ) survivalie , an increased risk of death of 33% or less over the duration of the study for the capecitabine - containing regimen would be regarded as non - inferior . 
 this correction has been made as of feb 25 , 2013 . for overall vol 14 march 2013 comment available and the future place of these drugs is di cult to comprehend but future treatments of patients with indolent lymphomas will probably involve less chemotherapy and more biological agents and , for lymphomas , the combination of these aggressive new agents with chemotherapy might decrease the refractoriness to therapy identi ed in some patients . altogether , the results of westin and colleagues strongly support the restoration of an antitumour response that is directly mediated by anti - pd1 antibodies . 
 however , interplay between the micro environment and tumour cells in follicular lymphoma is highly complex and alternative pathways could not be de nitely ruled out by the correlative analyses . 
disabling immune tolerance by programmed death - 1 blockade with pidilizumab after autologous hematopoietic stem - cell transplantation for di use large b - cell lymphoma : results of an international phase ii trial . 
safety and activity of pd1 blockade by pidilizumab in combination with rituximab in patients with relapsed follicular lymphoma : a single - group , open - label , phase 2 trial . 
expert rev hematol 2013 ; 6 : 191202 . second - line chemotherapy for patients with oesophagogastric adenocarcinoma during the past two decades , there have been major advancements in cancer treatment , such as the incorporation of newer cytotoxic , molecularly targeted , and other biological agents to traditional chemotherapy . 
unfortunately , clinical trials involving novel agents have had little success in the treatment of oesophagogastric adenocarcinoma , which is one of the main causes of cancer - related deaths worldwide . 
 initial reports of chemotherapy regimens that include uoropyrimidines , anthracyclines , or cisplatin provided evidence of a survival bene t , and , at present , 20 years worth of clinical trials have indicated uoropyrimidines ( uorouracil or its oral pro - drugs ) and platinum combination , with or without the addition of anthracyclines , as the standard for rst - line treatment . 
a small subset of patients with her2 - positive disease might bene t from trastuzumab , 1 but more than half of patients do not respond to rst - line chemotherapy , and even in those who respond , the duration of response is as short as a few months . 
due to the absence of evidence associated with the bene t of second - line chemotherapy , and the potential for toxicity from such treatment , the proportion of patients o ered further therapy varies from 20% to 50% , depending on the region.2 in the past 4 years , the results of three multicentre phase 3 trials assessing the role of second - line in patients with oesophagogastric chemotherapy reported.35 findings adenocarcinoma have been from all three trials showed signi cant reductions in the risk of deathreductions in all three trials were of a similar magnitude , which gives an indication vol 15 january 2014 published online december 10 , 2013 s1470 - 2045 ( 13 ) 70580 - 1 see articles page 78 copyright park . 
the rst trial included 40 pretreated patients who received either irinotecan ( in the experimental group ) or best supportive care ( in the control group ) .3 the second trial compared salvage chemotherapy with best supportive care in 202 korean patients with gastric cancer.4 the study was designed to include patients who were pretreated with not one but two prior chemotherapy regimens , a factor that might have diluted the results . 
 investigators reported a signi cant survival the bene t with chemotherapy versus best supportive care ( 53 months with chemotherapy vs 38 months with best supportive care ; hazard ratio [ hr ] 0657 , 95% ci 04850891 )  . researchers the rst - line in the lancet oncology , hugo ford and colleagues5 present ndings from the third of these trials , the cougar - 02 trial . 
 patients , who had an eastern cooperative oncology group performance score of 02 , were randomly allocated to receive docetaxel 75 mg / m every 3 weeks plus active symptom control ( n = 84 ) , or active symptom control alone ( n = 84 )  . 
the results showed that second - line docetaxel improved median overall survival compared with active symptom control alone ( 52 months [ 95% ci 4159 ] vs 36 months [ 3344 ] ; hr 067 , 95% ci 049092 ; p = 001 )  . 
global healthrelated quality of life was similar in the two groups , and disease - speci c health - related quality - of - life measures also showed that second - line treatment reduced dysphagia and abdominal pain . we should consider several issues raised by the results of cougar - 02 and previous trials . 
obviously , patients who failed or were refractory to rst - line chemotherapy with uoropyrimidines and platinum should receive second - line treatment , with best supportive care reserved for those with a poor performance status . 
while seeking the answers to these questions , we should remember that the role of chemotherapy in this setting remains strictly palliative , in terms of its ability to substantially improve overall survival and to maintain patients quality of life . 
 despite the failures of several clinical trials involving molecularly targeted agents , the phase 3 regard trial of ramucirumab , a monoclonal antibody against vegfr , was successful.6 in this trial , pretreated patients with oesophagogastric adenocarcinoma were randomly allocated to receive ramucirumab or placebo as second - line treatment . 
surprisingly , the survival bene t achieved with ramucirumab ( 38 months with placebo vs 52 months with ramucirumab ; hr 0776 , 06030998 ) was similar to that seen in the cougar - 02 trial . 
the results of the more clinically relevant rainbow trial ( nct001170663 ) , which assessed the addition of ramucirumab to paclitaxel versus paclitaxel alone for second - line therapy , are expected in the near future . the should cougar - 02 investigators commended for doing this trialtheir ndings seem to end the debate about the bene ts of secondline chemotherapy in patients with advanced oesophago gastric adenocarcinoma . 
however , in the real worldoutside of the strict enrolment criteria of a clinical trialmany patients develop peritoneal carcinomatosis during the course of their disease , leading to a rapid symptomatic deterioration and chemotherapy intolerance.2 data from cougar - 02 and other trials should be interpreted carefully because of the potential selection biasonly a small subset of patients continue to have a good performance status after rst - line failure and are still physically t enough to be o ered second - line chemotherapy . 
better molecular characterisation of cancer has brought hope for more successful treatment , 1 , 6 including the use of trastuzumab for patients with her2 - positive disease and hopefully ramucirumab in the second - line setting . 
experience with other types of vol 15 january 2014 comment published online november 30 , 2013 s1470 - 2045 ( 13 ) 70537 - 0 see articles page 87 cancer has taught us that a substantial improvement in the treatment of oesophagogastric adenocarcinoma individualised treatment might be achieved with strategies , identi cation of genetic including the alterations and studying of the molecular biology of therapeutic agents . se hoon park division of hematology - oncology , department of medicine , sungkyunkwan university samsung medical center , seoul , korea hematoma@skku.edu i declare that i have no con icts of interest . bang yj , van cutsem e , feyereislova a , et al . 
trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of her2 - positive advanced gastric or gastro - oesophageal junction cancer ( toga ) : a phase 3 , open - label , randomised controlled trial . 
survival advantage for irinotecan versus best supportive care as second - line chemotherapy in gastric cancer - - a randomised phase iii study of the arbeitsgemeinschaft internistische onkologie ( aio )  . 
ramucirumab monotherapy for previously treated advanced gastric or gastro - oesophageal junction adenocarcinoma ( regard ) : an international , randomised , multicentre , placebo - controlled , phase 3 trial . 
 e ects of histone deacetylase inhibitors on alloresponses inhibition of histone deacetylases ( hdacs ) can have important antineoplastic e ects through cytotoxic and pro apoptotic mechanisms , and it can prevent cell pro liferation and promote cell di erentiation . 
 the researchers added vorinostat to a standard regimen of tacrolimus and mycophenolate mofetil for pro phylaxis of acute graft - versus - host disease ( gvhd ) in patients receiving reduced - intensity conditioning and an allogeneic haemopoietic stem - cell transplant . 
the results raise several questions : what mechanisms are involved ? how might this therapeutic approach be optimised further ? what steps will be necessary for wider clinical application ? acute gvhd is dependent on activation and proliferation of alloreactive t cells . 
hdac inhibitors such as vorinostat have inhibitory e ects on t - cell activation , di erentiation , and e ector functions , but the e ects on normal t - cell development are much diminished . 
in a fully mhcmismatched model of gvhd , 3 vorinostat reduced in ammation and gvhd - dependent mortality by targeting activated allospeci c t cells but did not a ect broad donor t - cell expansion and immune in a murine model , reconstitution.3 likewise , vorinostat lowered the incidence and severity of gvhd while preserving the graft - versus - leukaemia e ect.4 the study by choi and colleagues is notable because the data show the ability of hdac inhibitors to dampen undesired t - cell alloreactivity after transplantation without haemopoietic stem - cell a ecting engraftment or promoting relapse or increased rates of fungal or other infections . 
 and although immunosuppressive the precise mechanisms underlying the anti - in ammatory actions of hdac inhibitors might vary by cell type and context , one unifying theme that has arisen from experimental and in - vitro studies with human cells is that inhibition of hdac activity can promote development and suppressive functions of foxp3 + t - regulatory ( treg ) cells.5 after 2 weeks of treatment vol 15 january 2014 editorial pancreatic cancer in the spotlight in february , 2014 , an advertising campaign launched in the uk by the charity pancreatic cancer action generated a storm of criticism , depicting patients with pancreatic cancer stating that they wished they had other forms of the disease , speci cally testicular and breast cancer . 
although few would argue against raising awareness of an invariably fatal disease , the comparison with other cancersand especially the idea that having one cancer is better than having another prompted objections from several sources , including charities breakthrough breast cancer and breast cancer care . 
 furthermore , other charities ( such as macmillian cancer support ) have backed the campaign , which now continues with a focus on the types of symptoms associated with the disease . while is understandable why the campaign provoked a reaction , it must be acknowledged that , although charities are not - for - pro t organisations , there is heavy competition for limited resources within the philanthropic sector . 
with less money to go around , individuals and corporations are more selective about where they give , and with so many causes seeking attention , donation fatigue is a serious concern . 
in the uk , for example , there are at least three charities that focus on pancreatic cancer , which begs the question as to whether a collaborative or combined approach would be greater than the sum of all parts . 
funding for pancreatic cancer research is very low compared with other cancer types , and as a result , there are currently 81 clinical trials for breast cancer recruiting in the uk , but only eight for pancreatic cancer . 
unlike breast cancer , which lends itself to self - diagnosis and for which there are well established screening programmes in place , pancreatic cancer presents with di use symptoms and often at a late stage . 
more research is therefore desperately needed to understand the basic biology of the disease and to develop appropriate screening programmes . more than 330 000 people are diagnosed with pancreatic cancer annually worldwide , and prognosis remains poorjust under 4% are expected to survive for 5 years after their diagnosis . 
in doing so , patients with rarer or di cultto - treat cancers would no longer be forgotten and governments in turn might make more e ective use of limited research budgets . 
 the lancet oncology vol 15 march 2014 for more on human mismanagement of the planet see the lancet planetary health journals / lanplh / issue / current for more on developments in us air pollution policies see editorial lancet resp med 2017 ; 5 : 361 for the global burden of disease attributable to ambient air pollution see articles lancet 2017 ; published online april 10 . 
this years annual meeting of the american association for cancer research ( aacr ) in washington , dc , usa ( april 15 , 2017 ) was no exception , and last years meeting saw the launch of the ambitious cancer moonshot programme , which laid out plans to accelerate two - fold the transition of genetic and immunological findings from laboratories to the clinica goal formally recognised when the us senate approved dedicated funding via the 21st century cures act . 
but can this insatiable desire to enhance our fundamental understanding of tumour biology overshadow the health gains that could be secured by improved environmental protection ? many genetic loci associated with increased risk of developing cancer have been discovered , and some can lead to preventive actions . 
 on march 14 , 2017 , the us department of veteran affairs amended a ruling regarding payments to army personnel who had resided at marine corps base camp lejeune ( jacksonville , nc , usa ) for 30 days or longer between aug 1 , 1953 , and dec 31 , 1987all veterans , former reservists , and former national guard members who had been stationed there during this time , and had subsequently been diagnosed with one of several types of cancer , would be entitled to veteran disability benefits . 
 the allowance was made because those who had served at the camp , and their families , had spent the duration of their stay drinking and bathing in water contaminated with an estimated 70 organic volatile compounds known to be carcinogenic . 
since the town changed its water supply in april , 2014 , from lake huron to the flint river , residents noted that their tapwater had become yellow and cloudy . 
after declaring an emergency and enlisting the help of the national guard in 2016 , flint river water was re - declared as unsafe , and work began on replacing lead - contaminated pipes . 
 the consequences of 3 years worth of exposure to lead - contaminated water for flints residentsand especially their growing childrenare unknown , but in view of leads classification as probably carcinogenic to humans in a recent iarc monograph , they are likely to be at an increased risk of developing cancer in the future . 
in view of the precedent set by camp lejeune , where the total settlement has now reached around us$2 billion , this incident will plague and cost residents and regulators alike for decades to come . 
such incidents of neglect inevitably occur elsewhere too : a british water utility company , thames water , was fined a record 203 million on march 22 , 2017 , for a series of leaks of untreated sewage during 201314 into the river thames ( which indirectly supplies londons drinking water ) , its tributaries , and the adjacent land . 
and , contaminated water supplies in china have been long documented . a large - scale economic inefficiency clearly exists , with financial resources being divided into both the science of cancer prevention and also into efforts to help those who have developed cancer as a direct result of human mismanagement of the planet . 
 paradoxically , recent moves by the us government to reduce the funding of the environmental protection agency , to increase coal production , and to review corporate average fuel economy standards will probably increase the populations exposure to carcinogenic pollutants , while at the same time the moonshot programme aims to counter the adverse consequences . 
 outside the usa , the european commission issued a final warning to the uk on feb 15 , 2017 , regarding its repeated breaches of legal air pollution limits , and globally , 42 million deaths in 2015 have been attributed to ambient particulate matter . 
to eradicate cancer , governments need to both identify and act not only on increased risk susceptibility , but also ensure that people are not exposed to carcinogenic materials through gross environmental mismanagement . 
 the lancet oncology vol 18 may 2017 editorial bjrn - ole juhnke , martin mynarek , * stefan rutkowski department of pediatric hematology and oncology , university medical center hamburg - eppendorf , 20251 hamburg , germany s.rutkowski@uke.de sr is a member of the paediatric oncology advisory board for novartis germany , and has received financial support from riemser pharma , as part of the hit - med trial group . 
molecular subgroups of medulloblastoma : an international meta - analysis of transcriptome , genetic aberrations , and clinical data of wnt , shh , group 3 , and group 4 medulloblastomas . 
2045 ( 17 ) 30243 - 7 . mammography screening : please dont be vague , tell me when i should come ! in the lancet oncology , prue allgood and colleagues1 report the results of a large population - based trial of second timed appointments for non - attenders of breast cancer screening in england . 
their findings show that this policy is effective in improving participation compared with an invitation letter with a telephone number to call to book a new appointment ( 2861 [ 22% ] of 12 807 women in the intervention group participated in breast cancer screening within 90 days of the first offered appointment compared with 1632 [ 12% ] of 13 247 women in the control group ; relative risk 181 [ 95% ci 170193 ] , p < 00001 )  . this kind of research is not often published in the lancet oncology or other high - impact factor scientific journals with a multidisciplinary audience , probably because research on health behaviours and compliance with public health initiatives is often context specific and not generalisable . 
a timed appointment for screening seems to be an exception : results are consistent across countries , type of screening , cultures , and time periods.2 , 3 allgood and colleagues findings suggest that timed appointments also have positive effects on participation at second timed appointments . 
 furthermore , the potential consequences on health of an intervention capable of increasing mammography screening uptake by 34% is probably higher than the impact of some new oncology drugs , tested in trials published in top - ranking according to the estimates of one death prevented and 17 life - years gained out of 180 participating women over a 20 - year period of screening , 4 increasing the average screening participation from 72% to 76% in about 8 million women ( ie , the target population in england ) could save the lives of about 90 women per year and 1500 life - years . 
this postulation can only be made if all women , at any age , with a new diagnosis of stage iv breast cancer receive and tolerate the treatment , which is clearly an implausible situation . 
 this example has been adapted from a study recently published in this journal.6 a prescheduled in the never - ending controversy about mammography screening , those opposed to screening maintain that appointment undermines the option of not participating.7 whether or not this effect actually happens is not clear , but if so , it depends on what information is conveyed to women . 
screening programmes are committed to maximising the number of women who , after having received comprehensive information about screening , decide to participate because they are published online may 15 , 2017 s1470 - 2045 ( 17 ) 30344 - 3 see articles page 972 848 vol 18 july 2017 comment conscious of both the screening benefits and harms ( informed choice to participate ) and women who decide not to participate because , according to their values , the screening benefits do not outweigh the harms ( informed choice to not participate )  . 
similarly , screening programmes should minimise the number of women who do not participate because they did not receive appropriate information or because of organisational barriers ( disinformed or involuntary non - participation ) and the number of women who agree to participate but would not have done so if they had received a clear outline of screening benefits and harms ( disinformed participation )  . through information the only way to go forward in this direction is by delivering accurate , understandable , and comthe most appropriate plete communication methods . 
although messages conveyed through an invitation letter might be transparent , they can never be neutral , because screening professionals are duty - bound to set up initiatives that are effective , and breast cancer screening programmes are established on this basis.1 nevertheless , screening programmes must remove organisational barriers as much as possible , because they could interfere with a womans decision - making process . 
with these premises , trust in public health services has a relevant role in how women decide about screening ; trust in such a common good as public health services is something that has been constructed over years of care , competence , expertise , empathy , honesty , and commitment shown by public health operators both as individuals and as an organisation . 
a timed appointment is an implicit demonstration of the accountability of the screening programmes regarding their position on the balance of screening benefits and harms . * paolo giorgi rossi , livia giordano inter - institutional epidemiology unit , ausl reggio emilia , 42122 , reggio emilia , italy ( pgr ) ; arcispedale santa maria nuova , irccs , reggio emilia , italy ( pgr ) ; and aou citt della salute e della scienza , unit of epidemiology , cpo piemonte , turin , italy ( lg ) paolo.giorgirossi@ausl.re.it pgr was a member of the steering committee of the national centre for screening monitoring . 
lg works in the epidemiology unit of the cpo piemonte that is in charge of the breast cancer screening evaluation and implementation in piedmont . the author ( s )  . 
breast cancer survival and stage at diagnosis in australia , canada , denmark , norway , sweden and the uk , 2000 - 2007 : a population - based study . 
utidelone plus capecitabine versus capecitabine alone for heavily pretreated metastatic breast cancer refractory to anthracyclines and taxanes : a multicentre , open - label , superiority , phase 3 , randomised controlled trial . 
bmj 2006 ; 332 : 53841 . the tnm classification of malignant tumourstowards common understanding and reasonable expectations clarity and precision about the anatomical extent of disease in cancer is essential for prognostication , research , and cancer - control activities . 
although the addition of predictive markers , molecular and genomic profiling , and imaging data has contributed important advances to the care of cancer patients , it has also complicated the clarity of the purpose and mission of cancer staging . 
we believe that communication of the core purpose of the tumour , node , metastasis ( tnm ) classification to different audiences , to address uncertainty about its application and to articulate the future of this system to permit ongoing study of factors that underpin most cancer discoveries , is urgently needed . 
it is an integral part of the cancer language ; 1 , 2 vol 18 july 2017 comment adenoma surveillance and colorectal cancer incidence : a retrospective , multicentre , cohort study wendy atkin , kate wooldrage , amy brenner , jessica martin , urvi shah , sajith perera , fiona lucas , jeremy p brown , ines kralj - hans , paul greliak , kevin pack , jill wood , ann thomson , andrew veitch , stephen w duffy , amanda j cross summary background removal of adenomas reduces colorectal cancer incidence and mortality ; however , the benefit of surveillance colonoscopy on colorectal cancer risk remains unclear . 
we examined heterogeneity in colorectal cancer incidence in intermediate - risk patients and the effect of surveillance on colorectal cancer incidence . methods we did this retrospective , multicentre , cohort study using routine lower gastrointestinal endoscopy and pathology data from patients who , after baseline colonoscopy and polypectomy , were diagnosed with intermediaterisk adenomas mostly ( > 99% ) between jan 1 , 1990 , and dec 31 , 2010 , at 17 hospitals in the uk . 
patients were followed up through to dec 31 , 2014 . we assessed the effect of surveillance on colorectal cancer incidence using cox regression with adjustment for patient , procedural , and polyp characteristics . 
this trial is registered , number isrctn15213649 . findings 253 798 patients who underwent colonic endoscopy were identified , of whom 11 944 with intermediate - risk adenomas were included in this analysis . 
compared to no surveillance , one or two surveillance visits were associated with a significant reduction in colorectal cancer incidence rate ( adjusted hazard ratio 057 , 95% ci 040080 for one visit ; 051 , 031084 for two visits )  . 
without surveillance , colorectal cancer incidence in patients with a suboptimal quality colonoscopy , proximal polyps , or a high - grade or large adenoma ( 20 mm ) at baseline ( 8865 [ 74% ] patients ) was significantly higher than in the general population ( sir 130 , 95% ci 106157 )  . 
by contrast , in patients without these features , colorectal cancer incidence was lower than that of the general population ( sir 051 , 95% ci 029084 )  . interpretation colonoscopy surveillance benefits most patients with intermediate - risk adenomas . 
however , some patients are already at low risk after baseline colonoscopy and the value of surveillance for them is unclear . funding national institute for health research health technology assessment , cancer research uk . copyright the author ( s )  . 
a 3 year surveillance interval was indicated for those at intermediate risk on the basis of evidence from a randomised trial that compared different surveillance intervals for the detection of advanced adenomas at follow - up . 
the results of the study showed a clear benefit from surveillance in patients with one or more advanced adenomas , whereas in those with only non - advanced adenomas , the benefit was less marked . 
evidence suggests that the quality of colonoscopy has improved and that the number of missed or incompletely removed lesions has decreased since the publication of a uk national colonoscopy audit in 2001 , leading to implementation of national training standards and quality assessments . 
no study has yet assessed the effect of surveillance on long - term colorectal cancer risk among patients offered 3 - yearly surveillance , who represent most patients offered surveillance . added value of this study our study assessed colorectal cancer risk in patients considered to be at intermediate risk . 
across 8 years of follow - up , our data identified risk factors for colorectal cancer at baseline colonoscopy that permitted further stratification of these patients into lower - risk and higher - risk subgroups . 
patients with an incomplete colonoscopy , poor bowel preparation , proximal polyps , or a high - grade or large adenoma ( 20 mm ) at baseline were at increased risk , and the first surveillance colonoscopy significantly reduced colorectal cancer risk . 
 by contrast , in patients without these baseline colonoscopy findings , future risk of colorectal cancer was already lower than that in the general population before any surveillance . implications of all the available evidence our results show that most patients who are currently offered 3 - yearly surveillance colonoscopy benefit substantially from attending at least one surveillance visit . 
evidence from this study will be important in informing future adenoma surveillance guidelines and will help to minimise the costs and risks associated with unnecessary colonoscopies . two consecutive negative colonoscopies ( appendix p 1 ) , whereas in the usa , there are no recommended criteria for stopping other than older age . the main aim of adenoma surveillance is to reduce the incidence of colorectal cancer , but very few studies have used long - term colorectal cancer incidence after adenoma removal to define risk groups and need for surveillance12 , 19 , 20 and none have looked at predictive factors for long - term colorectal cancer incidence in patients who are currently offered surveillance . 
 in this study , we estimated colorectal cancer incidence after baseline colonoscopy in patients who are recommended 3 - yearly surveillance , and assessed the effect of surveillance on colorectal cancer incidence . 
 we hypothesised that a subgroup of patients exists in whom surveillance colonoscopy could be stopped earlier , or for whom surveillance is not necessary , on the basis of their colorectal cancer incidence . methods study design and participants we did this retrospective , multicentre , cohort study using information from 17 uk hospitals with electronic records of lower gastrointestinal endoscopy and pathology data recorded for at least 6 years before the start of the study in 2006 ( appendix p 2 )  . 
the size of the catchment population for the 17 hospitals was estimated to be more than 65 million people.23 , 24 patients were eligible for inclusion in the study if they had a baseline colonoscopy and newly diagnosed intermediate - risk adenomas according to uk guidelines , defined as one - to - two large ( 10 mm ) adenomas , or threeto - four small adenomas ( appendix p 1 )  . 
we excluded patients with a history of bowel resection , colorectal cancer , inflammatory bowel disease , a family history of colorectal cancer , or any endoscopies without a date . we searched gastrointestinal endoscopy databases to identify patients who underwent colonic examination before dec 31 , 2010 , then we searched pathology databases for reports of colorectal lesions , using systematised nomenclature of medicine ( snomed ) codes ( versions 2 and 3 ) , systematized nomenclature of pathology ( snop ) codes , keywords , or multiple search terms . 
endoscopy see online for appendix 824 vol 18 june 2017 articles and pathology reports were linked and pseudonymised before being entered into an oracle ( 11g enterprise edition ) database . 
further details on hospital data collection and standard operating procedures are available in the appendices of our national institute for health research ( nihr ) health technology assessment ( hta ) report.25 we divided endoscopic examinations into visits ( ie , one or more examinations made in close succession to complete a full examination of the colon and remove detected lesions )  . 
we used a hierarchy of rules to assign a summary value for the size , histology , and location of lesions seen at multiple examinations.25 completeness of colonoscopy , and quality of bowel preparation26 were defined by the most complete examination and the best bowel preparation during the baseline visit . 
bowel preparation quality and completeness of colonoscopy , as assessed by the endoscopist , were obtained from endoscopy reports when not included as a separate field in the endoscopy database . patient , procedural , and polyp characteristics at baseline assessed as a - priori risk factors and confounders included age at first adenoma detection , sex , completeness of colonoscopy , quality of bowel preparation ( graded as excellent , good , adequate or satisfactory , and poor ) , 26 year of entry ( year first adenoma detected ) , and adenoma number ( total number recorded at baseline ) , size ( largest at baseline ) , histology and grade of dysplasia ( worst at baseline ) , and polyp location . 
 data on lifestyle factors , such as smoking and alcohol consumption , were not available . we ascertained the presence of colorectal cancers from hospital pathology reports and from national health service ( nhs ) digital , the nhs central register ( nhscr ) , and national services scotland ( nss )  . 
mortality data were provided by nhs digital , nhscr , and nss . ethics approval was granted by the royal free research ethics committee ( reference 06 / q0501 / 45 )  . 
approval for use of patient information without consent was granted by the patient information advisory group under section 60 of the health and social care act 2001 ( piag 105 [ e ] / 2006 )  . 
 identified at baseline had been incompletely resected if baseline examinations showed that they were left intact or partly removed , were in the same or adjacent segment of the colon , and had similar histology ; such cancers were excluded from the analysis . our sample size calculations stipulated that estimates of the colorectal cancer incidence rate have a coefficient of variation of about 30% ( ie , the standard error of the estimate would be 30% of the actual estimate )  . 
assuming conservatively a rate of two colorectal cancers per 1000 person - years , 20 , 27 , 28 approximate poisson distribution of incidence , and a simple univariate estimate of the rate , then nine colorectal cancer events and 4500 person - years in any given subgroup would give a coefficient of variation of 33% . 
assuming a smallest subgroup of interest of 15% of the cohort , we required at least 30 000 person - years ( 4500 divided by 015 ) and 60 colorectal cancers , or a total cohort of 6000 patients with at least 5 years of follow - up . 
because inclusion of covariates might increase standard errors , we aimed to include at least 10 000 patients . we censored time - to - event data at first colorectal cancer diagnosis , death , emigration , or december 31 , 2014 , for 253 798 patients with a lower gastrointestinal endoscopy for the protocol see ac.uk / programmes / hta / 043301 223 539 excluded 45 717 colorectal cancer or other colonic conditions * 16 081 colorectal cancer at baseline 6798 resection at or before baseline 30 555 inammatory bowel disease , crohns disease , colitis , or radiation proctitis or colitis 1745 polyposis , juvenile polyps , hamartomatous polyps 264 hereditary non - polyposis colorectal cancer or family history of adenomatous polyposis 14 volvulus 2752 no baseline colonoscopy 92 missing examination dates 174 978 no adenomas 18 264 not at intermediate risk 1033 not classiable 14 522 at low risk ( one or two adenomas , both small [ < 10 mm ] ) 2709 at high risk ( 5 small adenomas or 3 adenomas , at least one of which is large [ 10 mm ] ) 30 259 eligible patients with adenomas 11 995 intermediate - risk patients ( three or four small adenomas or one or two adenomas , at least one of which is large [ 10 mm ] ) 51 lost to follow - up statistical analysis the primary outcome was incident adenocarcinoma of the colorectu this outcome excluded in - situ cancer . 
p values calculated with test to compare patients with and without surveillance visits . table 1 : baseline patient , procedural , and polyp characteristics by surveillance visit attendance and exposure to successive surveillance visits started at the last procedure in each visit . 
some analyses divided each patients follow - up time into three distinct periods ; without surveillance ( from start of time at risk , censored at any first surveillance ) ; after first surveillance ( from first surveillance , censored at any second surveillance ) ; and after second surveillance ( from second surveillance to final date of censoring )  . we compared baseline characteristics in patients with and without surveillance visits using tests . 
 we did not use multiple imputation or inverse probability weighting to deal with missing data . we used one minus the kaplan - meier estimator of the survival function to show time to cancer diagnosis and to estimate the cumulative incidence of cancer with 95% cis at 3 , 5 , and 10 years ; we used the log - rank test to compare subgroups . 
we examined the effects of surveillance and patient , procedural , and polyp characteristics at baseline on long - term colorectal cancer incidence using cox proportional hazards models . we used univariable models to estimate unadjusted hazard ratios ( hr ) and 95% cis . 
we identified independent predictors of colorectal cancer incidence in a multivariable model , using backward stepwise selection with a p value less than 005 in the likelihood ratio test as the criterion for retention of variables . 
the number of surveillance visits was included as a time - varying covariate and was constrained to be included in the multivariable model . using baseline polyp and procedural risk factors identified from the multivariable model , we stratified the intermediate - risk cohort into lower - risk and higher - risk subgroups . 
we did not include age as a factor in defining the higher - risk subgroup in our study because risks of adverse events increase with age coincidental with general decline in health , and older age is associated with worse colonoscopy quality.29 , 30 we calculated expected numbers of colorectal cancers by multiplying the observed sex and 5 - year age - group - specific person - years by the corresponding incidence in the general population of england in 2007.31 we report the ratio of observed to expected cases as a standardised incidence ratio ( sir ) and 95% cis assumed an exact poisson distribution . we did all analyses with stata / ic 13.1. 
this study is registered with isrctn , number isrctn15213649 . role of the funding source the funders of the study had no role in the study design , data collection , data analysis , data interpretation , or the writing of the report . 
kw , us , and wa had full access to all the data and wa had final responsibility for the decision to submit for publication . results we identified 253 798 consecutive patients who underwent ( > 99% ) lower gastrointestinal endoscopies mostly 826 vol 18 june 2017 articles between jan 1 , 1990 , and dec 31 , 2010 . 
we excluded 223 539 patients : 174 978 with no adenomas , 45 717 with colorectal cancer or other conditions associated with increased colorectal cancer risk , 2752 with no colonoscopy , and 92 with missing procedure dates . 
of the remaining 30 259 patients with a histologically confirmed adenoma at baseline , ( 40% ) were diagnosed with intermediate - risk adenomas , of whom 51 could not be traced in national data sources and had no surveillance , leaving 11 944 patients for analysis ( figure 1 )  . 11 995 the median age of 11 944 intermediate - risk patients was 667 years ( iqr 584740 ) and 6625 ( 55% ) were men ( table 1 )  . 
a lower proportion of patients who attended at least one surveillance visit had an incomplete colonoscopy or poor bowel preparation than did patients who did not attend any visits ( table 1 )  . 
the multivariable hr and associated p value reported for sex , adenoma histology , and year of entry ( variables not included in the final multivariable model ) , were for if the variable was added as an additional variable to the final multivariable model . 
 * number of surveillance visits was included in the models as a time - varying covariate ; if a patient had any surveillance visits , they contributed person - years to more than one category of number of surveillance visits . 
no multivariable hazard ratio and p value was reported for number of adenomas because of multicollinearity with largest adenoma size ( largest size < 10 mm perfectly predicts 3 adenomas )  . table 2 : long - term colorectal cancer incidence by baseline risk factors and number of surveillance visits ( 95% ci 182238 ; table 2 )  . 
of the 5019 patients who did not attend surveillance , 2326 ( 46% ) died and 121 ( 2% ) were diagnosed with cancer , whereas of the 6925 patients who attended one or more surveillance visits , 1455 ( 21% ) died and 89 ( 1% ) were diagnosed with cancer . 
after adjustment for baseline risk factors , compared with no surveillance , one or two surveillance visits were associated with a significant reduction in colorectal cancer incidence rate ( hr 057 , 95% ci 040080 for one visit ; 051 , 031084 for two visits ) ; a similar reduction in incidence rate was seen with three or more surveillance examinations ( hr 054 , 95% ci 029099 ; table 2 )  . baseline characteristics independently associated with increased colorectal cancer incidence included older age , adenomas of 20 mm or larger , adenomas with high - grade dysplasia , polyps in the proximal colon , a colonoscopy that was incomplete or of unknown completeness , and poor quality bowel preparation ( table 2 )  . 
other baseline variables not included in the multivariable model are listed in the appendix ( p 3 )  . on the basis of the polyp and procedural characteristics identified as colorectal cancer risk factors ( but not older age ) , we divided the cohort into lower - risk ( 3079 [ 26% ] ( 8865 patients ) and higher - risk [ 74% ] ) subgroups . 
 the higher - risk subgroup consisted of patients who , at baseline , had a large adenoma ( 20 mm ) , high - grade dysplasia , proximal polyps , or a suboptimal colonoscopy . 
colorectal cancer incidence was 247 cancers per 100 000 person - years ( 95% ci 214285 ) in the higher - risk subgroup versus 93 cancers per 100 000 person - years ( 95% ci 63139 ) in the lower - risk subgroup ( table 3 )  . patients in the higher - risk subgroup were older , had entered the study earlier , and had significantly more surveillance visits than those in the lower - risk subgroup ( appendix p 4 )  . 
however , median follow - up times were similar ( 80 years [ iqr 55113 ] in the higher - risk subgroup vs 78 years [ 57106 ] in the lower - risk subgroup )  . 
among higher - risk patients , number of surveillance visits was inversely associated with colorectal cancer incidence ; by contrast , in the lower - risk subgroup , the number of surveillance visits was not associated with colorectal cancer incidence ; however , statistical power was limited because of the low number of cancers ( n = 24 in total ; table 3 )  . 
 * number of surveillance visits was included in the models as a time - varying covariate ; if a patient had any surveillance visits , they contributed person - years to more than one category of number of surveillance visits . 
the higher - risk subgroup included patients with any of the following risk factors at baseline : suboptimal quality examination ( defined as incomplete colonoscopy , unknown completeness , or poor bowel preparation ) , high - risk polyps ( defined as proximal polyps or a high - grade or large [ 20mm or larger ] adenoma ) , or both ; the lower - risk subgroup included patients without any of these risk factors . 
 table 3 : incidence of colorectal cancer and unadjusted effect of surveillance on incidence of colorectal cancer by number of visits incidence was 33% without surveillance , colorectal cancer incidence at 10 years was 27% ( 95% ci 2134 ; 114 cancers ) in the ( 2642 ; cohort overall ; 101 cancers ) in the higher - risk subgroup and 11% ( 0523 ; 13 cancers ) in the lower - risk subgroup ( table 4 )  . 
colorectal cancer incidence in the whole cohort was not significantly different from that of the general population ( sir 109 , 95% ci 091130 ) ; however , colorectal cancer incidence was significantly higher in the higher - risk subgroup ( sir 130 , 106157 ) and significantly lower in the lower - risk subgroup ( sir 051 , 029084 ) than in the general population ( table 4 ; figure 2a and b )  . after a single surveillance visit , colorectal cancer incidence at 10 years was 23% ( 95% ci 1633 ; in the cohort overall , 28% ( 1941 ; 47 cancers ) 42 cancers ) in the higher - risk subgroup , and 07% ( 0217 ; five cancers ) in the lower - risk subgroup ( table 4 )  . 
 compared with the general population , the sir for colorectal cancer was 080 ( 95% ci 059105 ) in the overall cohort , 042 ( 95% ci 016092 ) in the lower - risk subgroup , and 090 ( 95% ci 066121 ) in the higher - risk subgroup ( table 4 ; figure 2c and d )  . 
following a second surveillance visit , colorectal cancer incidence at 10 years was 20% ( 1431 ; 29 cancers ) overall and 22% ( 1534 ; 26 cancers ) in the higher - risk subgroup ; the lower - risk vol 18 june 2017 articles n 830 vol 18 june 2017 articles b higher - risk subgroup ( 95% ci ) lower - risk subgroup ( 95% ci ) higher - risk subgroup ( 95% ci ) lower - risk subgroup ( 95% ci ) time from baseline ( years ) time from baseline ( years ) number at risk 11 944 8430 4820 3079 1752 number at risk higher - risk lower - risk 8865 3079 5998 2432 3388 1432 2131 1238 95% ci 95% ci number at risk 6925 5430 2695 1429 time from rst surveillance visit ( years ) time from rst surveillance visit ( years ) number at risk higher - risk lower - risk 5257 1668 4082 1348 2056 1107 figure 2 : cumulative colorectal cancer incidence after baseline cumulative colorectal cancer incidence with no surveillance ( ie , censoring at first follow - up ) for the whole cohort ( a ) and for the risk subgroups ( b )  . 
cumulative colorectal cancer incidence after one surveillance visit ( ie , censoring at the second follow - up ) for the whole cohort ( c ) and for the risk subgroups ( d )  . 
95% cis are shown for each curve . subgroup analyses were underpowered because only three colorectal cancers had been diagnosed by 10 years ( table 4 )  . discussion in this retrospective , multicentre , cohort study , colonoscopy surveillance was associated with a substantially reduced these incidence of colorectal cancer intermediate - risk patients , who are currently offered surveillance colonoscopy at 3 - year intervals . 
the first surveillance visit seemed to confer the most benefit and was associated with a significantly reduced colorectal cancer incidence rate compared with no surveillance ; this incidence reduction was maintained in patients who attended subsequent visits . 
in the uk , about 20% of colonoscopies are done for the purpose of surveillance.21 in our dataset 80% of patients undergoing adenoma surveillance were at intermediate risk ( figure 1 ) .21 we identified a subgroup of patients at higher risk of colorectal cancer , which included roughly three - quarters of this intermediate - risk cohort . 
this subgroup consisted of patients who had a suboptimal quality colonoscopy ( incomplete , of unknown completeness , or poor bowel preparation ) , a large adenoma ( 20 mm ) , an adenoma with high - grade dysplasia , or proximal polyps detected at baseline ; surveillance was highly effective in this subgroup and was associated with a significant reduction in the incidence of colorectal cancer . 
by contrast , in patients without these baseline findings , the benefit of surveillance was unclear because only a few cancers were subsequently diagnosed . patients with intermediate - risk adenoma are offered surveillance at 3 - year intervals because they are perceived to be at increased risk of colorectal cancer compared with the general population . 
this perception is based on high detection rates of advanced neoplasia in those who attend surveillance1114 and on follow - up of patients diagnosed in the 1980s and 1990s ; 12 , 19 , 20 colorectal cancer risk has not previously been quantified by use of data in an era of higher quality colonoscopies . 
we found that colorectal cancer incidence in the absence of surveillance was similar to that expected in the general population , vol 18 june 2017 articles suggesting that intensive surveillance might not be appropriate for all intermediate - risk patients . 
however , in the higher - risk subgroup , colorectal cancer incidence without surveillance was significantly higher than that of the general population ; therefore , individuals in this subgroup might benefit from at least one surveillance visit . 
by contrast , in the lower - risk subgroup , the colorectal cancer incidence was already lower than that of the general population after baseline colonoscopy , with a 10 - year cumulative incidence of only 11% . 
this low baseline incidence raises uncertainty as to whether any surveillance is warranted for these individuals . some of the independent risk factors for colorectal cancer that we identified within this intermediate - risk group have been described as risk factors for detection of advanced neoplasia at follow - up colonoscopy , including larger adenoma size , older patient age , and having only a suboptimal quality baseline colonoscopy.1116 a less well documented risk factor was the presence of polyps in the proximal colon , which in our study was associated with an increased incidence of colorectal cancer . 
this finding corroborates data from two previous studies reporting that patients with proximal polyps had an 80% increased risk of advanced neoplasia at follow - up colonoscopy.14 , 32 this evidence suggests that proximal polyps could be regarded as a colorectal cancer risk factor in future iterations of surveillance guidelines . 
however , results from a large pooled analysis of 9167 men and women showed that body - mass index , smoking , and family history , which are often important epidemiological risk factors , are not major predictors of metachronous advanced neoplasia at surveillance after adjustment for the baseline adenoma characteristics.14 our results emphasise the importance of achieving a complete colonoscopy with good quality bowel preparation . 
since the national colonoscopy audit in 2001 , 33 there has been heightened awareness of colonoscopy standards and implementation of national quality assessments and training programmes , 21 , 34 , 35 resulting in substantial improvements in endoscopy quality and leading to nearly 30% fewer cancers arising from missed or incompletely removed lesions within 3 years of colonoscopy in 2007 than in 2001.36 patient factors , such as older age , female sex , having prior abdominal or pelvic surgery , and obesity might also affect the quality of a bowel preparation or colonoscopy.3742 in the english bowel cancer screening programme ( bcsp ) , examinations to complete an investigation of the colon and remove detected lesions are regarded as part of the initial work - up , with surveillance only considered when baseline examinations have been completed ; this would be a good policy to adopt for patients diagnosed with adenomas outside of the bcsp . 
for individuals in whom colonoscopy is problematic , the clinician should establish on a case - by - case basis whether it is appropriate to recommend colonoscopy surveillance . in our study , 42% of patients did not attend surveillance . 
other factors that we were unable to assess but which are likely to affect attendance for surveillance include the health status of the patient , administrative problems in scheduling an appointment 3 years in advance , and patient choice , especially if they had either a bad experience with the index colonoscopy or the reasons for surveillance were not well explained . the main strengths of this study are the generation of a high - quality detailed dataset by use of a large nationwide sample of routinely collected clinical endoscopy and pathology data on colonoscopies for consecutive patients with adenomas across 17 uk hospitals , which serve a combined population of more than 65 million people.23 follow - up for cancer and death was complete for almost all patients and , apart from data on bowel preparation quality , very few data were missing . 
finally , we studied incidence in a large number of patients with intermediaterisk adenomas , about 84% of whom had their baseline colonoscopy after the implementation of national quality improvement programmes beginning in 2000 . the main limitation of this study is that it is an observational study and therefore we cannot assume a causal association between surveillance and colorectal cancer incidence . 
this difference was only substantial for the bowel preparation and colonoscopy completeness variables , suggesting that when a future surveillance visit was planned , there was less of a tendency to record the quality of the initial examination . 
 a further limitation is that conclusions were based on a median of 79 years of follow - up and longer - term followup is needed to substantiate our findings , especially in the lower - risk subgroup without surveillance . 
finally , although follow - up examinations were assumed to be for surveillance , some might have been for symptomatic purposes . we conclude from our results that patients diagnosed with intermediate - risk adenomas are at only a small increased risk of developing colorectal cancer after their baseline colonoscopy and polypectomy compared with the general population , especially if they have had a good 832 vol 18 june 2017 articles quality baseline colonoscopy ; therefore , it is unclear whether all of these intermediate - risk patients need the currently recommended 3 - yearly surveillance by colonoscopy . 
among patients in the lower - risk subgroup , surveillance might not be warranted at all if baseline colonoscopy is complete , with good visibility of the bowel mucosa and all lesions completely excised . 
additionally , future research should aim to define the subgroup of intermediate - risk patients for whom the risk of colorectal cancer after first surveillance is so low that they can stop surveillance altogether . contributors wa and ik - h were responsible for trial design and organisation . 
all authors edited the paper and gave final approval on the version to be published . trial staff , collaborators , and data providers cancer screening and prevention research group staffiain stenson ( data acquisition and cleaning ) , eilidh macrae ( trial manager ) , bhavita patel ( senior data clerk ) , joanne monger ( data clerk ) , laura j turner and paula kirby ( projects managers ) , rosemary howe and elizabeth coles ( project administrators )  . trial steering committeematt rutter , chris todd , allan hackshaw , marco novelli , sue moss , and lynn faulds wood and helen watson ( patient representatives )  . participating hospitalswe are grateful to the people listed for their involvement in this project . 
royal sussex county hospital , brighton : stuart cairns * , lena king , sam goode , nigel loaring , and mark harris ; cumberland infirmary , carlisle : denis burke * , fergus young , and ian pearson ; charing cross hospital , hammersmith hospital and st marys hospital , london : paul ziprin * , geoff smith * , bola makinwa , patrizia cohen , rob goldin , david peston , and andrew hay ; glasgow royal infirmary , glasgow : john anderson * , gordon reid , and craig napier , jane hair , julie macdonell , and marion flood ; leicester general hospital , leicester : john de caestecker * , and angus mcgregor ; royal liverpool university hospital , liverpool : anthony morris * , martin lombard , steve bradburn ; institute of translational medicine , university of liverpool : michael burkitt * ; new cross hospital , wolverhampton : sarah jewes , roy cooper ; university hospital of north tees , stockton - on - tees : matt rutter * , sharron pooley , and danielle mead ; queen elizabeth hospital , woolwich , london : alistair mcnair * , matthew foxton , thelma pinto ; queen marys hospital , sidcup , kent : howard curtis * ; dartford and gravesham nhs trust , kent : guy sisson * , angela christopher , and diane gambrell ; royal shrewsbury hospital , shropshire : mark smith * ; st georges hospital , tooting , london : roger leicester * caroline finlayson ; st marks hospital , harrow , london : brian saunders , john northover , david smith ; royal surrey county hospital , surrey : john stebbing * , vanessa bollons , and tasmin patel ; torbay district general hospital , devon : mark feeney * , brett hardwell , and kirsty james ; yeovil district hospital , somerset : sue bulley * , jill burt , garry sweet , edwin cooper , and fiona wulf ; norfolk & norwich university hospital : richard tighe * and virginia sams . 
all rights reserved ; nhs central register ( nhscr ) ; and national services scotland ( nss )  . declaration of interests wa , as principal investigator , was the recipient of all of the funding . 
all other authors declare no competing interests . acknowledgments this study was fully funded by the national institute for health research ( nihr ) health technology assessment programme ( hta project number 04 / 33 / 01 )  . 
the work of the cancer screening and prevention research group ( csprg ) at imperial college is also supported by the bobby moore fund for cancer research uk ( c8171 / a16894 )  . 
the views and opinions expressed by the authors in this publication are those of the authors and do not necessarily reflect those of the nihr , the hta , the department of health , the nhs , or cancer research uk . first - line selective internal radiotherapy plus chemotherapy versus chemotherapy alone in patients with liver metastases from colorectal cancer ( foxfire , sirflox , and foxfire - global ) : a combined analysis of three multicentre , randomised , phase 3 trials harpreet s wasan * , peter gibbs * , navesh k sharma , julien taieb , volker heinemann , jens ricke , marc peeters , michael findlay , andrew weaver , jamie mills , charles wilson , richard adams , anne francis , joanna moschandreas , pradeep s virdee , peter dutton , sharon love , val gebski , alastair gray , foxfire trial investigators , sirflox trial investigators , foxfire - global trial investigators , guy van hazel * , ricky a sharma * summary background data suggest selective internal radiotherapy ( sirt ) in third - line or subsequent therapy for metastatic colorectal cancer has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . 
the foxfire , sirflox , and foxfire - global randomised studies evaluated the efficacy of combining first - line chemotherapy with sirt using yttrium - 90 resin microspheres in patients with metastatic colorectal cancer with liver metastases . 
the studies were designed for combined analysis of overall survival . methods foxfire , sirflox , and foxfire - global were randomised , phase 3 trials done in hospitals and specialist liver centres in 14 countries worldwide ( australia , belgium , france , germany , israel , italy , new zealand , portugal , south korea , singapore , spain , taiwan , the uk , and the usa )  . 
chemotherapy - naive patients with metastatic colorectal cancer ( who performance status 0 or 1 ) with liver metastases not suitable for curative resection or ablation were randomly assigned ( 1 : 1 ) to either oxaliplatin - based chemotherapy ( folfox : leucovorin , fluorouracil , and oxaliplatin ) or folfox plus single treatment sirt concurrent with cycle 1 or 2 of chemotherapy . 
in foxfire , folfox chemotherapy was oxmdg ( oxaliplatin modified de gramont chemotherapy ; 85 mg / m oxaliplatin infusion over 2 h , l - leucovorin 175 mg or d , l - leucovorin 350 mg infusion over 2 h , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
in sirflox and foxfire - global , folfox chemotherapy was modified folfox6 ( 85 mg / m oxaliplatin infusion over 2 h , 200 mg leucovorin , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
randomisation was done by central minimisation with four factors : presence of extrahepatic metastases , tumour involvement of the liver , planned use of a biological agent , and investigational centre . 
the primary endpoint was overall survival , analysed in the intention - to - treat population , using a two - stage meta - analysis of pooled individual patient data . 
sirflox and foxfire - global are registered with clinicaltrials.gov , numbers nct00724503 ( sirflox ) and nct01721954 ( foxfire - global )  . findings between oct 11 , 2006 , and dec 23 , 2014 , 549 patients were randomly assigned to folfox alone and 554 patients were assigned folfox plus sirt . 
there were 411 ( 75% ) deaths in 549 patients in the folfox alone group and 433 ( 78% ) deaths in 554 patients in the folfox plus sirt group . 
the median survival time in the folfox plus sirt group was 226 months ( 95% ci 210245 ) compared with 233 months ( 218247 ) in the folfox alone group . 
in the safety population containing patients who received at least one dose of study treatment , as treated , the most common grade 34 adverse event was neutropenia ( 137 [ 24% ] of 571 patients receiving folfox alone vs 186 ( 37% ) of 507 patients receiving folfox plus sirt )  . 
serious adverse events of any grade occurred in 244 ( 43% ) of 571 patients receiving folfox alone and 274 ( 54% ) of 507 patients receiving folfox plus sirt . 
10 patients in the folfox plus sirt group and 11 patients in the folfox alone group died due to an adverse event ; eight treatment - related deaths occurred in the folfox plus sirt group and three treatment - related deaths occurred in the folfox alone group . interpretation addition of sirt to first - line folfox chemotherapy for patients with liver - only and liver - dominant metastatic colorectal cancer did not improve overall survival compared with that for folfox alone . 
after complete resection of liver metastases from metastatic colorectal cancer , approximately 3540% of patients survive for 5 years.5 the european organisation for research and treatment of cancer ( eortc ) intergroup clocc 400046 randomised study of the addition of radiofrequency ablation with or without surgery to chemotherapy in 119 patients with up to nine colorectal liver metastases , a significant effect on progression - free survival did translate into a significant overall survival benefit . is a at present , the proportion of patients eligible for surgical resection is only 20%.7 among the liver - directed therapies that might improve local control and increase downsizing of tumours to operability , selective internal leading technology.8 radiation therapy ( sirt ) sir - spheres y - 90 resin microspheres ( sirtex medical limited ; sydney , nsw , australia ) containing the - emitter yttrium - 90 ( y - 90 ) are delivered into the arterial supply of the liver under fluoroscopic guidance . 
the delivery of the resin microspheres into branches of the hepatic artery , which supplies the majority of blood to liver tumours , results in selective targeting by high - dose radiotherapy because the healthy liver is supplied predominantly by the portal venous system and therefore relatively spared from radiation exposure.9 research in context evidence before this study metastatic disease affects up to 50% of the more than one million patients diagnosed with colorectal cancer worldwide every year . 
the efficacy of sirt in third - line or subsequent therapy for metastatic colorectal cancer has been evaluated and there are data to suggest that sirt has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . 
we previously published a phase 1 / 2 trial that established the maximum tolerated dose of oxaliplatin - fluorouracil ( folfox ) chemotherapy to combine as concomitant radiosensitising chemotherapy with sirt . 
at the time of planning our studies in 2006 , we searched pubmed and web of science for articles published between jan 1 , 1980 , and may 31 , 2006 , with the search terms : colorectal cancer , colon cancer , rectal cancer , oxaliplatin chemotherapy , 5 - fluourouracil chemotherapy , fluoropyrimidine , selective internal radiotherapy , yttrium - 90 microsphere , radio - embolization , radio - embolisation , trans - arterial radio - embolization , liver metastasis , and hepatic metastasis original articles and review articles , published in english , were reviewed . 
no meta - analyses of sirt treatment of liver metastasis were identified at the time of protocol writing in 2006 . added value of this study the foxfire , sirflox , and foxfire - global , randomised clinical trials were designed to study whether sirt in combination with folfox chemotherapy as first - line therapy for metastatic colorectal cancer can improve overall survival compared with folfox alone . 
to our knowledge , the combined study represents the largest , randomised analysis performed in the field of interventional oncology to address the question of whether improved local control of colorectal liver metastases impacts on overall survival . 
despite higher proportions of patients achieving a response and improved liver - specific progression - free survival , the addition of sirt to first - line oxaliplatin - fluorouracil chemotherapy for patients with liver - only and liver - dominant metastatic colorectal cancer did not improve overall survival or progression - free survival . 
 additionally , to our knowledge , this study provides the most comprehensive account of the risk of adverse events which can occur secondary to sirt when it is used in combination with folfox chemotherapy . implications of all the available evidence because of the absence of overall survival benefit , early use of sirt in combination with first - line , oxaliplatin - fluorouracil - based chemotherapy in unselected patients with metastatic colorectal cancer cannot be recommended . 
careful patient selection and studies investigating the role of sirt as a post - chemotherapy consolidation therapy are required to define the role of sirt in treating metastatic colorectal cancer . 1160 vol 18 september 2017 articles chemotherapy with sirt , 10 building on our phase 1 / 2 trial , in which we established the maximum tolerated dose of oxaliplatin - fluorouracil ( folfox ) chemotherapy to combine as concomitant radiosensitising the foxfire , sirflox , and foxfire - global clinical trials were designed to study sirt in combination with folfox chemotherapy compared with folfox alone as first - line therapy for metastatic colorectal cancer.11 , 12 eligibility criteria and trial designs were pre - planned to be similar so that the three trials could be prospectively combined for analysis of overall survival and secondary endpoints . 
we previously reported that the combination of sirt with folfox in sirflox13 increased liverspecific progression - free compared with folfox chemotherapy alone , but there was no effect on overall progression - free survival . 
in this combined study , we sought to address the question of whether improved local control of colorectal liver metastases impacts on overall survival . survival methods study design and participants the foxfire , sirflox , and foxfire - global randomised , phase 3 trials were done in 14 countries ( australia , belgium , france , germany , israel , italy , new zealand , portugal , south korea , singapore , spain , taiwan , the uk , and the usa ) : in 28 hospitals and specialist liver centres for foxfire , 87 hospitals or centres for sirflox , and 69 hospitals or centres for foxfire - global ( appendix pp 2834 )  . 
two complementary trials were originally planned ( foxfire and sirflox ) , but the foxfire study took longer than anticipated to set up and recruit , so a third study ( foxfire - global ) was added as an independent trial . 
 liver - only or patients had to be eligible for systemic chemotherapy as first - line treatment for metastatic colorectal cancer.1114 eligibility criteria were similar between the three trials , but not identical . 
similarities and differences are highlighted in the combined study protocol paper.14 inclusion criteria included histologically confirmed colorectal cancer with liver - dominant metastases with or without the primary tumour in situ , who performance status of 0 or 1 , limited extrahepatic disease , age of 18 years or older , and life expectancy 3 months or longer . 
exclusion criteria included ascites , cirrhosis , or portal hypertension ( all established by clinical or radiological assessment ) ; thrombosis of the main portal vein ; and peripheral neuropathy grade 1 or worse . 
the protocols for foxfire and sirlox trials and for this combined study have previously been published.11 , 12 , 14 randomisation and masking in all three trials , patients were randomly assigned ( 1 : 1 ) to either folfox chemotherapy alone or folfox plus sirt with minimisation , based on the strata metastasis site ( liver - only vs liver plus extrahepatic metastases ) , extent of tumour involvement of the liver ( 25% vs > 25% measured objectively on baseline ct scan ) , planned use of a biological agent , and investigational centre . in foxfire , patients were allocated using minimisation with a probability of 08 to the treatment that most reduced the imbalance of the above factors . 
the first 30 treatments were allocated using ( simple ) block randomisation ( using variable block sizes of 2 , 4 , and 6 in a ratio of 1 : 2 : 1 )  . 
in sirflox and foxfire - global , an imbalance window of 5 was used ; if the treatment imbalance between the two groups was less than 5 , the treatment was randomly allocated . 
while the trial was in progress , access to the full randomisation lists was restricted to the database development manager at octo and the trial statistician at the centre for statistics in medicine ( csm ; oxford , uk )  . 
in sirflox and foxfire - global , randomisation was done centrally at the national health and medical research council clinical trials centre ( camperdown , nsw , australia ) via an interactive voice response syste participants were enrolled by the investigators in all three trials . 
as none of the trials were masked , once patients were allocated to treatment , participants , all members of the trial team , and treating medical staff knew the treatment allocation . procedures in foxfire , systemic folfox chemotherapy consisted of oxmdg ( oxaliplatin modified de gramont chemo therapy ; 85 mg / m oxaliplatin infusion over 2 h , l - leucovorin 175 mg or d , l - leucovorin 350 mg infusion over 2 h , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
systemic folfox chemotherapy in sirflox and foxfire - global consisted of modified folfox6 ( 85 mg / m oxaliplatin infusion over 2 h , 200 mg leucovorin , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
 in foxfire , protocol chemotherapy was 12 cycles ; in sirflox and foxfire - global , protocol chemotherapy continued until disease progression or dose - limiting see online for appendix vol 18 september 2017 1161 articles toxicity . 
the oxaliplatin dose was reduced from 85 mg / m to 60 mg / m for three cycles from the cycle coinciding with sirt administration and for two cycles thereafter , based on phase 1 / 2 data.10 dose modifications were permitted in line with standard care ( appendix pp 38 )  . 
we used the patients body surface area , percentage of tumour involvement , and magnitude of liver - to - lung shunting to establish the activity ( gbq ) per dosing chart.12 planned sirt was done on cycle 1 day 3 or 4 or cycle 2 day 3 or 4.10 in foxfire , patients could receive anti - vegf ( eg , bevacizumab ) or anti - egfr ( eg , cetuximab ) from cycle 1 in the folfox alone group and from cycle 7 onwards in the folfox plus sirt group . 
the addition of anti - vegf or anti - egfr treatments to protocol therapy was at the discretion of the treating physician and doses prescribed were according to local policy at the treating centre . foxfire - global , patients could we assessed patients by ct scan every 812 weeks until hepatic progression . 
follow - up assessments included clinical assessment ; ct of chest , abdomen , and pelvis ; and health related quality - of - life ( hrqol ) assessment.11 , 12 , 14 scans were independently reviewed by pharmtrace ( berlin , germany ) for overall and hepatic progression in foxfire using response evaluation criteria in solid tumors ( recist ; version 1.0 ) and in sirflox with recist ( version 1.0 ) with minor modifications.13 independent reviews were not done in foxfire - global . 
all patients were followed up until death or for a minimum of 2 years . health - related quality of life was assessed with the euroqol - 5d three - level questionnaire ( eq - 5d - 3l ) , a generic hrqol instrument15 measuring health in five dimensions ( mobility , self - care , usual activities , pain or discomfort , and anxiety or depression ) , which summarised as a utility score.16 the eq - 5d - 3l was administered during clinic visits at baseline , between the second and the third months after randomisation , at 6 months , at 12 months , and once per year until 60 months from the start of protocol treatment . 
grading of adverse events used the national cancer institute common terminology criteria for adverse events ( version 3 )  . outcomes the primary outcome of this analysis was overall survival , defined as the time from randomisation to death from any cause , with patients who were still alive censored at their last known follow - up date . 
the proportion of patients achieving an objective response in each treatment group was defined as the number of patients achieving a complete or partial response at any point during the trial , up to their first occurrence of hepatic resection , over the number randomised in that group ( early deaths by any cause and unknown responses were included in the demominator )  . 
 the percentage resected in each group was defined as the number of patients who underwent a hepatic resection divided by the number randomly assigned to that group . for progression - free survival or liver - specific progression - free statistical analysis for the primary combined overall survival analysis , a sample size of 810 was originally calculated , but subsequently updated to 1075 patients ( 710 deaths ) using a protocol - specified hazard ratio ( hr ) of 08 , with a control group median overall survival of 197 months and sirt group median overall survival of 246 months , two - sided 5% significance , 80% power , and allowing for 5% noncompliance.14 the updated sample size allowed for a higher median overall survival , the addition of biological agents to protocol chemotherapy ( planned use added as a stratification factor to the randomisation in may , 2011 , for foxfire and sirflox , and incorporated in foxfireglobal since set - up ) and crossover in both directions . 
the study also had 80% power to detect a 6 - month overall survival benefit in the subgroup of patients with metastatic disease restricted to the liver : 708 patients ( 463 deaths ) were needed . 
the cutoff for analysis was chosen such that there was a minimum of 710 deaths overall and 463 deaths in the liver - only subgroup ( assuming a 6 - month increase in overall survival in the sirt - treated , liver - metastasisonly patients ) and a minimum follow - up of 2 years since 1162 vol 18 september 2017 articles the last patient was randomly assigned to treatment . 
 we did two interim toxicity and safety analyses with the combined data from the foxfire and sirflox trials 8 months after at least 80 patients were randomly assigned ( 40 patients per trial ) and 8 months after 300 were randomly assigned ( minimum of 120 patients per trial ) ; foxfire - global was not included in the interim analyses on the combined data . we calculated median follow - up time using the reverse kaplan - meier method . 
we did all efficacy analyses on an intention - to - treat basis per the published statistical analysis plan.14 we estimated overall survival and progression - free survival for each trial using kaplan - meier survival curves , unadjusted log - rank tests , and cox proportional hazards the proportionality survival models . 
hrs for overall survival and progression - free survival from the individual trials were combined using a two - stage , fixed - effect , inverse - variance weighted individual participant data meta - analysis approach.17 the i statistic indicates the proportion of variation in the treatment effect that is due to heterogeneity rather than chance . 
we also estimated causespecific hazards.19 for overall survival , progression - free survival , and liver - specific progression - free survival , we investigated the potential treatment benefit in patients presenting with disease confined to the liver using survival models stratified by trial ( prespecified subgroup analysis )  . 
 the odds of patients having a resection or achieving a response ( overall and liver - specific ) were compared between treatment groups by pooling individual trial odds ratios ( or ) using two - stage individual participant data meta - analysis . 
 a minimum clinically significant difference in eq - 5d scores of 008 has been suggested across all cancers.20 we used analysis of covariance to analyse differences in eq - 5d - 3l utility scores between the two treatment groups , adjusted for eq - 5d - 3l baseline values . 
we made post - hoc comparisons between treatment groups of treatment received after protocol therapy using the mantel - haenszel test , stratifying by trial . we did safety analyses on patients who received at least one dose of chemotherapy in either group and on an astreated basis . 
we included adverse events reported up to 28 days after the end of trial treatment or 7 months after foxfire 1282 discussed at mdt meeting or screened sirflox 561 screened foxfire - global 240 screened 31 failed screening 31 failed screening 918 excluded 712 did not meet inclusion or exclusion criteria 110 patient refusal 96 other reason 364 randomly assigned 530 randomly assigned 209 randomly assigned 182 assigned oxmdg 263 assigned mfolfox6 104 assigned mfolfox6 267 assigned mfolfox6 plus sirt 105 assigned mfolfox6 plus sirt 182 assigned oxmdg plus sirt 179 started folfox chemotherapy 180 started folfox chemotherapy 167 sirt given 252 started folfox chemotherapy 263 started folfox chemotherapy 247 sirt given 102 started folfox chemotherapy 102 started folfox chemotherapy 93 sirt given 1103 included in individual participant data analysis * 549 folfox chemotherapy group 554 folfox chemotherapy plus sirt group figure 1 : trial profile oxmdg and mfolfox6 are equivalent oxaliplatin - fluorouracil - based folfox chemotherapy regimens . 
discontinuation data were available for patients in foxfire and for a subset of patients in sirflox , but were not available for patients in foxfire - global . vol 18 september 2017 1163 articles folfox alone ( n = 549 ) folfox plus sirt ( n = 554 ) folfox alone ( n = 549 ) folfox plus sirt ( n = 554 ) age at randomisation ( years ) 627 ( 231890 ) 634 ( 284896 ) ( continued from previous column ) 14 ( 0923 ) 14 ( 0923 ) extrahepatic metastases status 12 ( 0818 ) 12 ( 0718 ) extent of liver involvement time since diagnosis of primary tumour to randomisation ( months ) time since diagnosis of liver metastases to randomisation ( months ) who performance status primary tumour site not categorisable * primary tumour in situ male female missing missing colon rectum missing missing 361 ( 66% ) 187 ( 34% ) 1 ( < 1% ) 347 ( 63% ) 200 ( 36% ) 2 ( < 1% ) 392 ( 71% ) 137 ( 25% ) 8 ( 1% ) 12 ( 2% ) 302 ( 55% ) 246 ( 45% ) 1 ( < 1% ) 363 ( 66% ) 191 ( 34% ) 354 ( 64% ) 198 ( 36% ) 2 ( < 1% ) 421 ( 76% ) 116 ( 21% ) 5 ( 1% ) 12 ( 2% ) 278 ( 50% ) 275 ( 50% ) 1 ( < 1% ) previous adjuvant chemotherapy 28 ( 5% ) 31 ( 6% ) 520 ( 95% ) 523 ( 94% ) missing 1 ( < 1% ) metastases present at initial diagnosis yes ( synchronous ) no ( metachronous ) missing 475 ( 87% ) 71 ( 13% ) 3 ( 1% ) 483 ( 87% ) 68 ( 12% ) 3 ( 1% ) ( table 1 continues in next column ) randomisation , whichever was earlier ( deemed the safety window )  . 
 * site of primary tumour recorded as both colon and rectum ; the only options in foxfire were colon or rectu minimisation factors ; treating site was also a minimisation factor . 
extrahepatic disease permitted as per trial protocols were foxfire : no more than five metastases in the lung and metastases should have been , in the opinion of either the local multidisciplinary team meeting or after central review of scans arranged via the trials office , amenable to future definitive local therapy , in addition to lung metastases , a single site of other extrahepatic disease was permitted ( eg , multiple lymph nodes in one lymph node region ) after approval by the trials office ; for sirflox and foxfire - global : limited extrahepatic metastases in the lung , lymph nodes , or both were permitted , no more than five nodules in the metastases in the lung were allowed , which were no more than 1 cm in diameter or up to 17 cm in diameter per single lesion ; involvement of lymph nodes in one single anatomic area ( pelvis , abdomen , or chest ) was permitted provided their longest diameter measured less than 2 cintention to treat with a biological agent was not a minimisation factor for these patients because it was introduced after these patients entered the study . table 1 : baseline characteristics of participants in the combined study nct00724503 ( foxfire - global )  . ( sirflox ) and nct01721954 role of the funding source the sponsor had no role in the foxfire study design , data collection , or data analysis . 
jmo , pd , psv , and sl had full access to all of the data in the study and the corresponding author had final responsibility for the decision to submit for publication . results between oct 11 , 2006 , and dec 23 , 2014 , 1103 patients were enrolled and randomly assigned to either folfox chemotherapy ( n = 549 ) or folfox plus single treatment sirt ( n = 554 ) ( figure 1 )  . 
end of follow - up was oct 31 , 2016 , for foxfire , june 1 , 2016 , for sirflox , and nov 30 , 2016 , for foxfire - global , ensuring 2 years of follow - up after the last patient was enrolled ( appendix p 13 )  . 
median followup was 433 months ( iqr 316584 )  . in the first 12 cycles of treatment , 3193 ( 59% of 5369 ) oxaliplatin cycles in the folfox plus sirt group and 3608 ( 68% ) of 5344 cycles in the folfox alone group were at full protocol dose . 
the median number of cycles of folfox treatment was 12 ( iqr 713 ) in the folfox plus sirt group and 12 ( 715 ) in the folfox alone group . 
 in foxfire , 13 ( 4% ) of 364 patients received cetuximab ( four in the folfox plus sirt group and nine in the to 197 folfox group )  . 
after finishing protocol therapy , fewer patients in the folxfox plus sirt group were given irinotecan , fluoropyrimidine , anti - vegf , or anti - egfr systemic therapies upon progression than were patients in the folfox alone group ( appendix p 16 )  . 
66 ( 12% ) of 549 patients randomly assigned to the folfox alone group received sirt in a later course of therapy , whereas 47 ( 8% ) of 554 patients randomly assigned to sirt did not receive sirt . there were 844 ( 77% ) deaths in 1103 patients in the intention - to - treat population over the follow - up period : 296 ( 81% ) deaths in 364 patients in foxfire , 424 ( 80% ) in 530 patients in sirflox , and 124 ( 59% ) in 209 patients in foxfire - global . 
 the median survival time in the folfox plus sirt group was 226 months ( 95% ci 210245 ) compared with 233 months ( 218247 ) in the folfox alone group ; the pooled hr was 104 ( 95% ci 090119 , p = 061 ; figure 2a , c )  . 
sirt = selective internal radiotherapy . ( 261 [ 73% ] of 358 patients in the folfox group , median overall survival 246 months , 95% ci 221264 ; 264 [ 74% ] of 355 patients in the folfox plus sirt group , 245 months , 223263 ; pooled hr 100 , 95% ci 085119 , p = 096 )  . 
in a sensitivity analysis of overall [ 11% ] of survival excluding ineligible patients ( 62 549 patients in the folfox group and 60 [ 11% ] of 554 patients in the folfox plus sirt group were ineligible ; reasons for ineligibility not reported ) , there were 360 deaths ( 74% ) in 487 patients in the folfox group and 382 deaths ( 77% ) in 494 patients in the folfox plus sirt group . 
median overall survival was 239 months ( 95% ci 218250 ) in the folfox group and 234 months ( 218252 ) in the folfox plus sirt group ; pooled hr was 101 ( 95% ci 088117 , p = 086 )  . 
 subgroup comparisons for overall survival of the prespecified subgroups metastatic site , liver involvement , age , sex , who performance status , and tumour in situ , and the post - hoc subgroups primary tumour site , bevacizumab administration , and timing of metastasis are shown in figure 3 . 941 ( 85% ) of 1103 patients had an observed radiological progression or died before progression : 304 ( 84% ) of 364 patients in foxfire , 452 ( 85% ) of 530 patients in sirflox , and 185 ( 89% ) of 209 patients in foxfireglobal . 
progression - free survival was not significantly different between treatment groups ( pooled hr 090 , 95% ci 079102 , p = 011 ; figure 2b , d )  . 
the median progression - free survival in the folfox plus sirt group was 110 months ( 95% ci 102118 ) compared with 103 months ( 97109 ) in the folfox alone group . 
similar results were found in the pre specified subgroup analysis restricted to patients with liver - only metastatic colorectal cancer at baseline ; 297 ( 83% ) of 358 patients in the folfox group had progressed or died in the liver - only subgroup analysis ( median progressionfree survival 111 months , 95% ci 100121 ) ; 292 ( 82% ) of 355 patients in the folfox plus sirt group had progressed or died ( 119 months , 110138 ; hr 086 , 95% ci 073101 , p = 0066 )  . 
the results of a prespecified sensitivity analysis using radiological scan data as reported by sites from all three trials were consistent with the analysis of the centrally reviewed data ( hr 091 , 95% ci 080103 , p = 015 )  . in 271 ( 49% ) of 549 patients in the folfox and 173 ( 31% ) of 554 patients in the folfox plus sirt group , first progression events were radiologically observed in the liver ( figure 4a )  . 
the cumulative incidence of first progression in the liver was lower in the folfox plus sirt group than the folfox alone group ( figure 4a ; appendix p 17 )  . 
the cumulative incidence of progression within the liver in the first 12 months of follow - up was 22% ( 95% ci 1926 ) in the folfox plus sirt group and 39% ( 3543 ) in the folfox alone group . 
in 196 ( 36% ) of 549 patients in the folfox group and 301 ( 54% ) of 554 patients in the folfox plus sirt group , first progression was extrahepatic or death occurred before recorded radiological progression ( figure 4b , appendix p 17 )  . 
table shows grade 3 or worse haematological events occurring in at least 5% of patients , grade 3 or worse non - haematological events occurring in at least 5% of patients , and all sirt - associated adverse events . 
sirt = selective internal radiotherapy . table 2 : adverse events reported in each treatment group sirt group than in the folfox alone group ( figure 4b ; appendix p 17 )  . 
the cumulative incidence of progression outside the liver or death before recorded radiological progression in 12 months of follow - up was 33% ( 95% ci 2937 ) in the folfox plus sirt group and 19% ( 1623 ) in the folfox alone group . 
cause - specific hrs were in the same direction as , and of similar magnitudes to , the subdistribution hrs ( appendix p 17 )  . an objective ( complete or partial ) response over the study duration was achieved in 746 ( 68% ) of 1103 patients ; 400 ( 72% ) of 554 in the folfox plus sirt group and 346 ( 63% ) of 549 in the folfox alone group ( pooled or 152 , 95% ci 118196 , p = 00012 ; appendix pp 10 , 17 )  . 
an objective response was observed in more patients in the folfox plus sirt group than in the folfox alone group in each of the individual trials ( appendix p 17 )  . 
the odds of achieving an objective response in the liver were also higher in the folfox plus sirt group than in the folfox alone group ( pooled or 178 , 95% ci 137231 , p < 00001 ; appendix p 18 )  . vol 18 september 2017 1167 articles over the follow - up period , 182 ( 17% ) of 1103 patients had at least one hepatic resection . 
overall , 94 ( 17% ) of 554 patients in the folfox plus sirt group and 88 ( 16% ) of 549 patients in the folfox alone group had a resection . 
the odds of undergoing a resection were not significantly different between treatment groups ( pooled or 107 , 95% ci 078148 , p = 067 ; appendix p 11 )  . the proportion of patients who had a grade 3 or worse adverse event at each treatment cycle by treatment group , overall and for haematological adverse events , non - haematological adverse events , and neutropenia are shown in the appendix ( p 12 )  . 
of 1078 patients who received at least one dose of study treatment in the astreated population , 755 ( 70% ) had a grade 3 or worse adverse event ( up to 28 days after the end of protocol chemotherapy or the first 7 months after randomisation , whichever was earlier ) ; 375 ( 74% ) of 507 patients in the folfox plus sirt group and 380 ( 67% ) of 571 patients in the folfox alone group ( table 2 )  . 
the odds of a patient having a grade 3 or worse adverse event were higher in the folfox plus sirt group than in the folfox alone group ( pooled or 142 , 95% ci 109185 , p = 00089 , appendix p 13 )  . 
 of 507 patients who received sirt , 231 ( 46% ) had a haematological grade 3 or worse adverse event , whereas 165 ( 29% ) of the 571 patients who did not have sirt had a haematological grade 3 or worse adverse event , the most frequent being neutropenia ( 186 [ 37% ] in the folfox plus sirt group vs 138 [ 24% ] in the folfox alone group ; table 2 )  . 
adverse events of grade 1 or 2 occurring in 10% of patients or more and all grade 3 or worse events are shown in the appendix ( pp 1826 )  . 
 in foxfire , 15 ( 8% ) of 182 patients in the folfox group and 25 ( 14% ) of 182 patients in the folfox plus sirt group discontinued treatment because of an adverse event or serious adverse event ; data were not fully available for sirflox and not available for foxfire - global . 
serious adverse events of any grade occurred in 244 ( 43% ) of 571 patients receiving folfox alone and 274 ( 54% ) of 507 patients receiving folfox plus sirt ( appendix p 27 )  . 
10 patients in the folfox plus sirt group and 11 patients in the folfox alone group died due to an adverse event during the main safety window ( appendix p 26 )  . 
of the eight treatment - related deaths in the folfox plus sirt group , three deaths due to radiation - induced complications of surgery , one due to liver failure , one due to drug - induced pneumonitis , and one due to offtarget delivery of microspheres . 
there were three treatment - related deaths in the folfox alone group : one due to complications of surgery , one due to neutropenic sepsis , and one due to bowel perforation . 
average unadjusted eq - 5d - 3l utility scores were not significantly different between treatment groups at any time point except at 23 months ( appendix p 27 ) ; however , this difference would not be deemed clinically meaningful . discussion the foxfire , sirflox , and foxfire - global randomised studies designed to definitively assess the combination of sirt with folfox versus folfox alone for colorectal liver metastases in the first - line setting have not shown a benefit of adding sirt on overall survival . 
the combined analysis of these three randomised clinical that a global , multidisciplinary trial involving a complex liver - directed therapy can be done with adequate power to answer an important clinical question . trials shows the efficacy of sirt in third - line or subsequent therapy for metastatic colorectal cancer ( ie , salvage therapy of chemotherapy - refractory disease ) has previously been evaluated.21 a randomised trial22 of salvage in patients with metastatic colorectal cancer with liver - confined disease showed a significant benefit of chemotherapy plus sirt versus chemotherapy alone in time to progression . 
these data suggest that sirt has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . in our study , metastatic colorectal cancer in which the liver is the only site of disease occurs frequently in a subset of patients ; some of these patients can be resected with long - term cures.23 the significant improvement in liver disease control assessed by competing risk analyses did not translate to a benefit in overall survival . 
the absence of benefit of the addition of sirt to folfox on progression - free survival and overall survival in our combined study could be partly explained by the high proportion of patients who developed first progression at an extrahepatic site , independently of whether the metastases were liver - only at baseline or whether there were extrahepatic metastases or primary tumour in situ at baseline . 
despite the better liver control in the folfox plus sirt group compared with the folfox alone group , this observation of extrahepatic progression might also explain the absence of a 1168 vol 18 september 2017 articles in the groups significant difference between the frequency of surgical resection of the liver metastases being done during or after protocol therapy . 
to avoid possible ascertainment bias in interpreting responses and difficulties differentiating disease progression from radiation reaction of the hepatic parenchyma in patients undergoing liver interventional procedure , scans were centrally reviewed by independent readers . 
the absence of an overall survival benefit suggests that early use of sirt in combination with firstline recommended in unselected patients with metastatic colorectal cancer . oxaliplatin - based chemotherapy radiotherapy cannot the in our study , the sirt - treated patients had a similar quality of life to the patients who had chemotherapy only . 
in the as - treated population in the folfox plus sirt group ( n = 507 patients ) , hepatic failure resulted in death of one patient during the main safety window and death of a further two patients during extended follow - up . 
this study provides the most comprehensive account of the risk of adverse events that might occur secondary to sirt when used in combination with folfox chemotherapy . one possible limitation of our study is that significant changes to the management of metastatic colorectal cancer occurred during the 8 - year recruitment period with the introduction of bevacizumab and egfr inhibitors as first - line standards of care , and increased use of liver interventions such as surgery and ablation . 
the non - identical design of the individual trials might also be considered a limitation , but is accounted for by the use of appropriate statistical methods . little progress has been reported in improving overall survival in molecularly unselected populations since the crystal , prime , and tribe studies.2427 in our study , crossover was anticipated and 12% of patients randomised to folfox alone received sirt with a later line of therapy . 
furthermore , 8% of patients assigned to sirt did not receive sirt , a proportion consistent with our previously published data in patients with metastatic colorectal cancer.13 the difference in exposure to posttrial treatments between the two treatment groups might have affected the primary endpoint . 
it is possible that the improved liver disease control observed in the folfox plus sirt group might have influenced physicians to bias towards intensive subsequent treatment , particularly as so - called treatment - holiday strategies were evolving during the recruitment and follow - up periods of less these trials . 
alternatively , it could be postulated that the reduced use of irinotecan after protocol therapy might have been related to increased or prolonged toxicities in the patients in the folfox plus sirt group , including the risk of myelosuppression . 
our analysis of these toxicities for both groups over time showed an apparent increase of grade 3 or worse adverse events in the folfox plus sirt group , particularly haematological events , with the curves gradually converging after 6 months of protocol therapy . in the past decade , the focus of clinical trials has been on improving outcomes for selected biological subtypes in metastatic colorectal cancer with predefined molecular criteria ( eg , mutant ras or braf )  . 
several studies from the past 2 years have reported that patients with rightsided primary tumours have worse survival outcomes and it is possible that these patients benefit less from standard therapies.2830 molecular subtypes in our study are not currently available , but in the dataset available , 179 ( 25% ) of 718 patients had right sided - tumours . 
further analyses are underway to investigate this exploratory finding , with specific scrutiny of ras mutation , braf mutation , and tumour location in study populations who have received sirt in clinical trials . 
 further studies designed to define the potential benefit of sirt to treat colorectal liver metastases from rightsided primaries are warranted . improved radiological response , in conclusion , despite better liver - specific disease control and the foxfire prospective trials did not show a benefitof the combination of sirt with folfox for progression - free survival or overall survival . 
further studies are needed to study the role of sirt in carefully selected patient populations and as a consolidation therapy after chemotherapy . contributors hsw , pg , sl , vg , ag , gvh , and ras designed the study and wrote the protocol . 
hsw , pg , nks , jt , vh , jr , mp , mf , aw , jmi , cw , ra , af , jmo , psv , pd , sl , vg , ag , gvh , and ras interpreted the data , wrote the manuscript , and approved the paper . declaration of interests hsw reports grants , personal fees , non - financial support , and other uncompensated work from sirtex medical and merck serono ; personal fees and non - financial support from celgene ; grants and non - financial support from pfizer ; personal fees and non - financial support from roche and lily outside the submitted work . 
pg reports personal fees from sirtex ; grants and personal fees from roche , amgen , pfizer , merck , bayer , and servier , during the conduct of the study . 
vh vol 18 september 2017 1169 articles reports grants , personal fees , and non - financial support from sirtex medical , merck , and roche , during the conduct of the study ; involvement in a scientific project on radiological imaging from sirtex medical ; grants , personal fees , and non - financial support from merck and roche ; grants and non - financial support from amgen ; grants and personal fees from sanofi ; grants from pfizer and boehringer ingelheim ; and personal fees from bristol - myers squibb , msd , and novartis , outside the submitted work . 
jmi reports personal fees from sirtex medical , during the conduct of the study ; grants from sirtex medical ; and personal fees from sirtex medical , astellas , jannessen , lily , and roche , outside the submitted work . 
jmo reports grants from cancer research uk and sirtex medical , during the conduct of the study ; and non - financial support from sirtex medical , outside the submitted work . 
pd reports grants from cancer research uk and sirtex medical , during the conduct of the study ; and non - financial support from sirtex medical , outside the submitted work . 
gvh reports personal fees and non - financial support from sirtex medical , during the conduct of the study ; and personal fees and non - financial support from sirtex medical , outside the submitted work . 
ras is a consultant for and reports grants and personal fees from sirtex medical and btg , during the conduct of the study ; and reports personal fees from affidea , astrazeneca , boston scientific , cancer research technology , eisai , terumo , and varian , outside the submitted work . 
aw declares no competing interests . acknowledgments the foxfire study design was reviewed and endorsed by the clinical trials awards and advisory committee of cancer research uk , was approved by the national research ethics service committee south central - berkshire ( research ethics committee reference 09 / h0505 / 1 ) , was developed by the national cancer research institute colorectal clinical study group and the national institute for health research clinical research network and equivalents in devolved nations , and was sponsored by the university of oxford . 
we thank georgie perry for secretarial support . 4 gy versus 24 gy radiotherapy for patients with indolent lymphoma ( fort ) : a randomised phase 3 non - inferiority trial peter j hoskin , amy a kirkwood , bilyana popova , paul smith , martin robinson , eve gallop - evans , stewart coltart , timothy illidge , krishnaswamy madhavan , caroline brammer , patricia diez , andrew jack , isabel syndikus summary background follicular lymphoma has been shown to be highly radiosensitive with responses to doses as low as 4 gy in two fractions . 
this trial was designed to explore the dose response for follicular lymphoma comparing 4 gy in two fractions with 24 gy in 12 fractions methods fort is a prospective randomised , unblinded , phase 3 non - inferiority study comparing radiotherapy given as 4 gy in two fractions with a standard dose of 24 gy in 12 fractions . 
entry criteria included all patients aged over 18 years , having local radiotherapy for radical or palliative local control , with follicular lymphoma or marginal zone lymphoma , who had received no previous treatment for at least 1 month before . 
radiotherapy target sites were randomised ( 1 : 1 ) with minimisation strati ed by histology ( follicular lymphoma vs marginal zone lymphoma ) , treatment intent ( palliative or curative ) and centre . 
after a median follow - up of 26 months ( range 039754 ) , 91 local progressions had been recorded ( 21 in the 24 gy group and 70 in the 4 gy group )  . 
mucositis was the most common event in the 24 gy group ( two patients with acute mucositis and two with late mucositis ; all grade 3 ) and was not reported in the 4 gy group . 
 the most common acute e ect was pain at the site of irradiation ( two patients in the 4 gy group , one patient in the 24 gy group ; all grade 3 ) , and the most common late e ect was fatigue ( two patients in the 4 gy group , one patient in the 24 gy group ; all grade 3 )  . interpretation 24 gy in 12 fractions is the more e ective radiation schedule for indolent lymphoma and should be regarded as the standard of care . 
a large randomised study1 con rmed that a dose of 24 gy in 12 fractions was as e ective for local control as 40 gy in 20 fractions in terms of overall response and within eld progression . evidence for the e cacy of even lower doses has been reported over many years with the exquisite sensitivity of follicular lymphoma described using doses as low as 075 gy given as total body irradiation.2 an initial report3 of the use of 4 gy in two fractions in advanced indolent lymphoma was published in 1994 , with 89% of patients having a response . 
since then , several centres have reported similarly impressive high responses.4 the largest of these series comes from a study5 in the netherlands in which 96 patients with follicular lymphoma received 4 gy in two fractions . 
this study5 reported that 92% of patients had a response , with 61% achieving a complete response , and a median duration of complete remission of 42 months . against this background of an increasing number of studies con rming that 4 gy in two fractions was an e ective dose in the local treatment of follicular lymphoma , we did a randomised trial in patients receiving local external beam radiotherapy for control of follicular lymphoma , with the aim of showing that a lower dose of 4 gy in two fractions ( easier to give with hopefully fewer toxic e ects ) is as e ective in terms of local control as the standard 24 gy in 12 fractions . methods participants and study design the protocol for this study can be found online . 
the aim of the trial was to demonstrate that low - dose radiotherapy ( 4 gy ) is as e ective as conventional dose radiotherapy ( 24 gy ) in terms of tumour progression within the irradiated eld . 
as progression was to be assessed locally , it was decided that radiotherapy target sites would be randomised rather than patients , therefore individual patients could be randomly assigned more than once . treatment for control of patients were eligible for this study if they had a histologically con rmed diagnosis of follicular lymphoma and were to receive local radiotherapy with the aim of local control . 
initially , this trial was open only to patients local receiving palliative symptoms , but subsequently , protocol amendments allowed patients having radiotherapy for early stage localised disease in a curative setting to be included as well as those with marginal zone lymphoma . 
we excluded patients with histology results other than follicular lymphoma ( and later marginal zone lymphoma ) , those who had chemotherapy within 4 weeks of radiotherapy and a predicted prognosis of less than 3 months . the east of englandcambridge south research ethics committee reviewed the study and all patients provided written informed consent . randomisation and masking central randomisation was through the cancer research uk and university college london cancer trials centre using the minim6 progra sites were randomly assigned ( 1 : 1 ) to either 4 gy or 24 gy radiotherapy using minimisation strati ed by histology ( follicular lymphoma vs marginal zone lymphoma ) , treatment intent ( palliative vs curative ) and centre . 
we used no blinding since sham radiotherapy was not considered appropriate and followup was undertaken by the treating clinicians . procedures we delivered treatment using external megavoltage x - ray beams unless the lesion was super cial , when electrons or kilovoltage x - rays were allowed . 
 we treated some patients with ap - pa elds using orthogonal x - ray localisation whereas we treated most patients using 3d ct - based volume de nition and conformal beam arrangements . 
treatment was delivered using 2 gy per fraction , treating daily monday to friday . we monitored patients for acute toxic e ects before and during radiotherapy , and at 4 weeks after radiotherapy . 
 * flipi score was calculated using the stage ( worst seen at randomisation ) , baseline lactate dehydrogenase concentration , baseline hb , and number of nodal sites ( total seen , including earlier randomisations )  . 
 quality of life was recorded at each follow - up using the equation 5d ( eq - 5d ) health questionnaire . outcomes the primary outcome was time to local progression and was analysed on an intention - to - treat basis with all radiotherapy sites included . 
secondary endpoints were overall survival , response , toxic e ects , and quality of life . statistical analysis the study was designed as a non - inferiority trial to reliably exclude the chance that 4 gy might increase the rate of local progression at 2 years by more than 10% , which translates to the hr of 137 . at 2 years , we assumed that 60% of radiotherapy sites would be progression - free and using a one - sided 5% signi cance level and 90% power this requires 364 events ( a sample size of 650 target sites )  . we randomly selected the radiotherapy target site used in the analysis of overall survival ( each patient included only once ) before analyses were done . 
we used a cox proportional hazards model to estimate the hazard ratio ( hr ) between the the proportionality assumption using the schoenfeld residuals.7 all analyses were done with stata version 12.1. 
ph had full access to all of the data and the nal responsibility to submit for publication . results we randomly assigned 614 sites from 548 patients in 43 uk centres ( listed in the appendix ) to treatment groups vol 15 april 2014 299 allocated to radiotherapy 24 gy 315 allocated to radiotherapy 4 gy 3 did not receive trial radiotherapy 1 clinicians decision 1 treatment sites would overlap 1 patient too unwell 614 sites randomised 6 did not receive trial radiotherapy 1 emergency radiotherapy needed 1 patient refusal 1 did not want 24 gy 1 patient wanted a lower dose 1 surgery given , radiotherapy no 1 unknown ( missing treatment longer needed form ) 293 received trial radiotherapy 312 received trial radiotherapy 1 did not complete treatment ( patients choice after 6 gy ) 4 did not receive randomised dose 1 error ( received 8 gy ) 3 trial stopped , advised to switch groups 292 completed full protocol treatment 308 completed full protocol treatment 299 available for analysis * 315 available for analysis * 3 withdrew after treatment 296 available for follow - up 315 available for follow - up figure 1 : trial pro le all numbers refer to randomised sites , not patients . 
 * all radiotherapy target sites are included in the analysis of local progression ( the primary endpoint )  . the committee between april 7 , 2006 , and june 8 , 2011 , when the independent data monitoring ( idmc ) trial . 
although 94% of recommended halting recruitment had been completed , the idmc felt that the study question had been answered and patients should not be randomly assigned to a treatment believed to be inferior . 299 sites were randomly assigned to receive 24 gy and 315 sites to receive 4 gy . 
the medians seemed to di er between the two groups , with patients in the 24 gy group having longer times between diagnosis and randomisation than those in the 4 gy group ( 116 months vs 70 months ) , however , when we compared the distribution of the times further , we did not feel there was an imbalance . because of the sometimes lengthy periods between diagnosis and randomisation , patients had often received other treatments . 
151 ( 25% ) had received previous radiotherapy and 207 ( 34% ) previous chemotherapy ; these were also well balanced between the treatment groups ( table 1 )  . see online for appendix articles 482 tumour biopsies were reviewed centrally ; diagnoses could not be con rmed for 67 ( 14% ) of these samples ( 48 had insu cient material , 11 were reported to show no clear evidence of lymphoma , and another eight showed reactive changes only )  . 
of the 415 for which diagnoses were given , 386 ( 93% ) were follicular lymphoma and 46 ( 11% ) were marginal zone lymphoma ( table 1 )  . compliance with radiotherapy was very good ( gure 1 )  . 
 nine patients ( nine target sites ) were withdrawn before treatment started ; of target sites , 292 ( > 99% ) of the 293 sites in the 24 gy group and 308 ( 99% ) of the 312 sites in the 4 gy group received the complete , randomised dose . 
 the remaining stable disease ( including < 30% regression ) 22 ( 8% ) partial regression ( > 30% ) 53 ( 23% ) stable disease ( including < 30% regression ) 19 ( 8% ) 78 ( 32% ) 40 ( 16% ) all patients * complete regression partial regression ( > 30% ) progression total follicular lymphoma complete regression progression total marginal zone lymphoma complete regression partial regression ( > 30% ) stable disease progression total 24 gy 4 gy 176 ( 68% ) 137 ( 49% ) 60 ( 23% ) 90 ( 32% ) 44 ( 16% ) 2 ( < 1% ) 10 ( 4% ) 152 ( 67% ) 116 ( 48% ) 2 ( < 1% ) 9 ( 4% ) 24 ( 71% ) 7 ( 21% ) 3 ( 1 % ) 21 ( 55% ) 12 ( 32% ) 4 ( 11% ) 1 ( 3% ) data are number of sites ( % )  . 
 * patients who withdrew before treatment or with missing treatment data have been excluded , as have the three patients who switched from 4 gy to 24 gy after the trial was closed . 
there were also 43 ( 20 in the 24 gy group and 23 in the 4 gy group ) with no measurable disease at baseline and 17 ( 13 in the 24 gy group and four in the 4 gy group ) with missing response data . 
the exclusion of sites without measurable disease at baseline and those with missing response data showed that 236 ( 91% ) of 260 sites in the 24 gy group and 227 ( 81% ) of 281 in the 4 gy group had a complete or partial response ( p = 000095 )  . 
progressive disease was noted in more target sites in the 4 gy group than in the 24 gy group , but numbers in both groups were small ( two [ < 1% ] in the 24 gy group vs 10 [ 4% ] in the 4 gy group )  . 
although the marginal zone group was small ( and the di erence between 24 gy and 4 gy not signi cant , p = 071 ) the responses showed a similar pattern ( table 2 )  . we also looked at the subgroups of patients with early stage disease and those treated with curative intent . 
 although there were more responses , the di erence between the groups was slightly larger and remained statistically signi cant ( table 3 )  . after a median follow - up of 26 months ( 039754 ) , 91 local progressions had been recorded ( 21 in the 24 gy group and 70 in the 4 gy group ) giving an hr for time to local progression of 342 ( 95% ci 210557 , p < 00001 , gure 2a )  . 
although this is well below the 364 events required in the sample size calculation , it is not expected that longer follow - up will reduce the hr to a level that would meet the non - inferiority margin ( di erence in local progression - free interval at 3 years currently 198% ; 95% ci 278 to 134 )  . to explore the e ect of multiple randomisations within a patient , we did a sensitivity analysis using just one observation from each patient ( appendix )  . 
the hr was just below 1 in all samples , therefore there is currently no evidence to suggest that 4 gy has a negative e ect on overall survival . as patients often had more than one site of disease , many received additional anti - cancer therapies before local progression . 
this treatment was systemic therapy or radiotherapy either given to the target site for residual disease ( 12 patients ) or more often due to overlap with an adjacent site receiving radiation . 
this analysis reduced the number of events by seven , but the hr remained similar ( 373 ; 95% ci 223622 , p < 00001 )  . we did subgroup analyses for baseline size , treatment intent , karnofsky score , stage , time from diagnosis , and follicular lymphoma international prognostic index ( flipi ) score . 
we did not note any evidence of a di erence in treatment e ect within any of the subgroups ( appendix )  . we also tested the group of patients with con rmed follicular lymphoma treated with curative intent . 
this was a small group of only 134 patients ( 16 events ) but 4 gy remained inferior in terms of local progression ( hr 637 , 95% ci 1442818 , p = 00051 )  . toxic e ects were low , with just eight ( 3% ) sites in the 24 gy group and four ( 1% ) in the 4 gy group having grade 3 or 4 acute toxic e ects . 
a similar pattern was seen in late e ects with 105 sites ( 37% ) in the 24 gy group and 71 sites ( 23% ) in the 4 gy group a ected . we recorded quality of life using the eq - 5d form at 7 set timepoints and yearly thereafter , only patients with a single randomisation ( 228 in the 24 gy group and 239 in the 4 gy group ) were included in the analysis . 
we did not note any di erence between the two treatments ( p = 092 ; appendix )  . indolent b - cell non - hodgkin discussion our data suggest that , although 4 gy is an e ective dose local progression - free survival is inferior to a higher dose of 24 gy in 12 fractions . 
we noted no di erence in overall survival between groups ; however , these data are relatively lymphoma , 24 gy 4 gy number at risk 24 gy 4 gy time since randomisation ( months ) number at risk 24 gy 4 gy figure 2 : progression - free survival for all sites ( a ) and overall survival for one site per patient ( b ) immature , and we will re - analyse these data as further follow - up data are obtained and more events recorded . in our previous study1 of 24 gy compared with 40 gy in indolent lymphoma , 92% of patients had a response , similar to the 91% seen in this cohort , despite di erences in the populations : 62% of patients in the earlier study were treated with radical intent for stage one disease whereas in the current study , 60% of patients were treated with palliative intent and only 40% radically . 
while this is similar to the 91% in the 24 gy group , a striking , much larger , di erence is apparent in vol 15 april 2014 articles 24 gy 4 gy panel : research in context acute toxic e ects diarrhoea mucositis fatigue pain in target dry mouth oral candidiasis cerebrovascular ischaemia total late toxic e ects mucositis fatigue pressure sore constipation pharyngitis dry mouth total neutropenia and thrombocytopenia 1 * ( 04% ) any ( each patient only counted once ) 4 ( 13% ) 1 ( 04% ) 2 ( 07% ) 2 ( 07% ) 1 ( 04% ) 1 ( 04% ) 1 ( 04% ) 8 ( 28% ) 2 ( 07% ) 1 ( 04% ) 1 ( 04% ) 1 ( 04% ) 1 ( 03% ) 2 ( 07% ) 1 ( 03% ) 2 ( 06% ) 1 ( 03% ) 1 ( 03% ) 4 ( 13% ) any ( each patient only counted once ) 4 ( 14% ) all events were grade 3 , except where indicated . 
at the time of developing the protocol in 2004 , we did a formal literature search using medline and search terms follicular lymphoma , lymphoma , indolent lymphoma , low grade lymphoma , and radiotherapy . 
we identi ed no relevant randomised trials in the cochrane central register of controlled trials . interpretation the results of this trial con rm that 4 gy is e ective in many patients but that it is inferior to 24 gy in terms of time to local progression in both the radical and palliative setting when treating follicular lymphoma . 
4 gy has , however , a potential role as a simpler , shorter , and more pragmatic schedule in patients being treated for local control in the palliative setting , in which durable response might be less important . 
the proportion of patients with a complete response in previously published series of 4 gy in follicular lymphoma varied from 36% to 84% with a median value of 46% , 4 which is remarkably similar to that achieved in this study . 
it would seem reasonable therefore to propose that the di erence we noted between 4 gy and 24 gy regimens is real and that on balance , 24 gy in 12 fractions should be deemed the standard in this setting ( panel )  . both radical early stage and more advanced stage palliative patients were included in this study . 
however , in some patients with advanced disease and limited life span 4 gy is a very convenient and pragmatic alternative . the inclusion of marginal zone lymphoma in the latter part of the trial was a re ection of slow accrual at the time and was successful in signi cantly increasing the rate of patient entry . 
although it is di cult to draw any de nitive conclusions for marginal zone lymphoma as a distinct subgroup , the overall pattern of response was similar to that seen in follicular lymphoma and it would seem reasonable to conclude that 24 gy is better than 4 gy in this group as well , and should be considered the standard . the design of this trial allowed multiple sequential randomisations in one patient , which has been criticised in the past . 
however , we applied strict criteria to this approach ensuring response and toxic e ects were speci c to every site , and the results of the sensitivity analysis provide further reassurance that this feature did not compromise the results as presented here . 
premature closure of a trial is always a concern , however , the recommendation by the idmc in this case was as a result of mature data , the trial having been running for more than 5 years at the time of the decision and at the time of closure 94% of the planned accrual had been reached . despite the results of this trial , that a dose as low as 4 gy can achieve responses in a signi cant proportion of the population remains remarkable , and , indeed , more than 40% of sites were in complete remission after this dose . 
these events include apoptosis with inactivation of bcl - 2 overexpression , which is a characteristic of follicular lymphoma.8 this inactivation might result in overexpression of p53 and caspase - 8 and caspase - 9 . 
macrophage activation might also be upregulated.9 with such potent biological e ects within the cell , it is therefore tempting to suggest that a dose in excess of 4 gy , but much lower than 24 gy , could be optimum and further studies exploring intermediate doses might be of biological interest . toxic e ects with such low radiation doses are not a dose - limiting issue , unlike the situation in the radical treatment of epithelial cancers . 
however , we noted about half the incidence of acute grade 3 or higher toxic e ects in the 4 gy group compared with that in the 24 gy group . 
 this does not detract from the recommendation that 24 gy should be the standard treatment for indolent b - cell lymphoma , but supports the use of 4 gy for palliative treatment of patients with poor performance status . 
combination therapy using low - dose radiotherapy and other drugs that might similarly induce apoptosis , such as rituximab , could be of interest.10 in - vitro evidence suggests rituximab can enhance radiation - induced apoptosis in lymphoma cells and combination schedules with low - dose radiotherapy might therefore result in both optimum local control and carry the advantage of systemic e ects for more widespread disease control . contributors ph was chief investigator and lead author . 
ph , is , mr , eg - e , km , and cb were members of the trial management group and local principal investigators responsible for trial design , data collection , and interpretation . 
the oe05 trial assessed whether increasing the duration and intensity of neoadjuvant chemotherapy further improved survival compared with the current standard regimen . methods oe05 was an open - label , phase 3 , randomised clinical trial . 
 eligibility criteria included who performance status 0 or 1 , adequate respiratory , cardiac , and liver function , white blood cell count at least 3 10 cells per l , platelet count at least 100 10 platelets per l , and a glomerular filtration rate at least 60 ml / mparticipants were randomly allocated ( 1 : 1 ) using a computerised minimisation program with a random element and stratified by centre and tumour stage , to receive two cycles of cisplatin and fluorouracil ( cf ; two 3 - weekly cycles of cisplatin [ 80 mg / m intravenously on day 1 ] and fluorouracil [ 1 g / m per day intravenously on days 14 ] ) or four cycles of epirubicin , cisplatin , and capecitabine ( ecx ; four 3 - weekly cycles of epirubicin [ 50 mg / m ] and cisplatin [ 60 mg / m ] intravenously on day 1 , and capecitabine [ 1250 mg / m ] daily throughout the four cycles ) before surgery , stratified according to centre and clinical disease stage . 
this trial is registered with the isrctn registry ( number 01852072 ) and clinicaltrials.gov ( nct00041262 ) , and is completed . findings between jan 13 , 2005 , and oct 31 , 2011 , 897 patients were recruited and 451 were assigned to the cf group and 446 to the ecx group . 
no unexpected chemotherapy toxicity was seen , and neutropenia was the most commonly reported event ( grade 3 or 4 neutropenia : 74 [ 17% ] of 446 patients in the cf group vs 101 [ 23% ] of 441 people in the ecx group )  . 
the proportions of patients with postoperative complications ( 224 [ 56% ] of 398 people for whom data were available in the cf group and 233 [ 62% ] of 374 in the ecx group ; p = 0089 ) were similar between the two groups . 
one patient in the ecx group died of suspected treatment - related neutropenic sepsis . interpretation four cycles of neoadjuvant ecx compared with two cycles of cf did not increase survival , and cannot be considered standard of care . 
our study involved a large number of centres and detailed protocol with comprehensive prospective assessment of health - related quality of life in a patient population confined to people with adenocarcinomas of the oesophagus and gastro - oesophageal junction ( siewert types 1 and 2 )  . 
alternative chemotherapy regimens and neoadjuvant chemoradiation are being investigated to improve outcomes for patients with oesophageal carcinoma . funding cancer research uk and medical research council clinical trials unit at university college london . copyright the author ( s )  . 
these meta - analyses showed a significant survival benefit after treatment with neoadjuvant chemotherapy , both overall and for the subset of patients with adenocarcinoma who were considered in this study . 
these meta - analyses were unable to assess the benefits of different neoadjuvant chemotherapy regimens , and we can identify no phase 3 randomised trials that have directly compared different regimens . added value of this study to our knowledge , this is the largest randomised trial investigating whether an alternative neoadjuvant chemotherapy regimen might offer a survival benefit over the standard of two cycles of cisplatin and fluorouracil ( cf )  . 
this trial showed that giving four cycles of epirubicin , cisplatin , and capecitabine ( ecx ) neoadjuvantly might increase the level of tumour regression , but does not lead to any survival benefit . implications of all available evidence for patients with oesophageal adenocarcinoma , two cycles of cf should remain the standard choice of neoadjuvant chemotherapy regimen . 
further research is ongoing into the use of neoadjuvant chemoradiotherapy , but little evidence exists that directly compares it to neoadjuvant chemotherapy . studies were specifically powered to detect any such difference . 
few studies have been done only in patients with oesophageal adenocarcinoma.2124 high - quality data on the effect of neoadjuvant chemotherapy or chemoradiotherapy on health - related quality of life ( hrql ) are scarce ; more information is needed for clinical decision making , where small survival benefits might only be achieved with detrimental effects on many aspects of hrql . the results of the previous medical research council ( mrc ) oe02 randomised clinical trial19 showed a survival advantage at 2 years with neoadjuvant chemotherapy and surgery over surgery alone ( 43% vs 34% ; 9% increase [ 95% ci 314 ] ) , with a hazard ratio ( hr ) of 079 ( 95% ci 067093 ) , so two - cycle cisplatin with fluorouracil was used for the control group in this study . 
the results showed a 5 - year survival of 36% ( 95% ci 3043 ) for perioperative chemotherapy and surgery compared with 23% ( 1729 ) for surgery alone ( overall survival hr 075 , 95% ci 060093 ) .25 because 45% of participants in the magic trial ( 34% of people who had surgery ) did not receive postoperative treatment ( a similar pattern was also seen in the ffcd - fnclcc 9703 trial22 ) , we concluded that further assessment of perioperative chemotherapy would be challenging and increased it was decided neoadjuvant therapy would be the best strategy . 
oral capecitabine is readily available and has been shown to be equivalent to intravenous fluorouracil in colorectal cancer , 26 so we decided to investigate four cycles of neoadjuvant epirubicin , cisplatin , and capecitabine ( ecx ) as the investigational group without postoperative chemotherapy . 
given the results of the magic trial , that increasing the duration of neoadjuvant chemotherapy from two cycles to four cycles and adding anthracycline to the established doublet regimen was considered the most promising strategy for improving outcomes in patients with oesophageal adenocarcinoma in this study . 
participants were of any age with surgically resectable histologically verified adenocarcinoma of the oesophagus ( including siewert types 1 and 2 gastro - oesophageal junction tumours ) stage ct1n1 , ct2n1 , ct3n0 / n1 , or ct4n0 / n1 where invasion was thought to be confined to diaphragm , crura , or mediastinal pleura and surgically resectable ( union for international cancer control [ uicc ] tnm staging28 )  . 
additionally , patients had to meet the following criteria : who performance status 0 or 1 and adequate respiratory and cardiac function ( forced expiratory volume in 1 sec of > 15 l and cardiac ejection fraction of 50% on echocardiography or multigated acquisition scan ) within 4 weeks of randomisation . 
 within 1 week of randomisation , liver function tests needed to be at most 15 - times normal , white blood cell count at least 3 10 cells per l , platelet counts at least 100 10 platelets per l , and the calculated or measured glomerular filtration rate at least 60 ml / min . 1250 vol 18 september 2017 articles assessment of disease stage required a contrastenhanced multislice ct scan from neck to pelvis and endo scopic ultrasonography within 4 weeks of randomisation . 
the final staging of patients ( and siewert classification ) was done on the basis of a multidisciplinary team discussion following endoscopy , endoscopic ultrasonography , ct , and laparoscopy if appropriate . ( radiologically patients were ineligible if investigations indicated blood - borne metastases assessed ) , peritoneal dissemination , local invasion involving the tracheobronchial tree , aorta , pericardium or lung , or abdominal para - aortic lymphadenopathy greater than 1 cm in diameter on ct scan or more than 6 mm in diameter on endoscopic ultrasonography . 
patients were also excluded if they had received any previous treatment for oesophageal cancer , had siewert type 3 cancer , a medical condition that was likely to compromise the proposed trial treatment . 
uncontrolled angina pectoris , myocardial infarction in the 6 months before entry into the trial , heart failure , clinically significant uncontrolled cardiac arrhythmias , or any patient with a clinically significant abnormal ecg , as well as patients with abnormal left ventricular ejection fraction ( lvef ) diagnosed on muga scan or echocardiography , including areas of abnormal contractility , were excluded . 
 patients with positive serology for hiv or hepatitis c , active hepatitis b , or were pregnant were also excluded . participating centres were considered eligible if they had a multidisciplinary team structure , had experience of twophase oesophagectomy with two - field lymphadenectomy ( unproctored surgeons were recommended to have done a minimum of 12 such operations before joining the trial ) , access to multislice ct and endoscopic ultrasonography equipment , and had pathologists who were experienced in reporting oesophageal cancer . the protocol was approved by the south west multicentre research ethics committee ( 04 / 6 / 005 ) and all patients gave written consent for participation in the study . 
the protocol had five amendments during the course of the trial , predominantly for administrative reasons or to add clarity ; amendments did not affect the eligibility or treatment of patients . 
the most recent version of the protocol ( version 6.0 ) is available online . randomisation and masking eligible patients were enrolled by staff at participating centres who then called the randomisation line at the mrc clinical trials unit at ucl ( london , uk )  . 
no masking to treatment allocation was done because of the difference in the number of chemotherapy cycles in the two groups . chemotherapy control group procedures the regimen was two 3 - weekly cycles of cisplatin and fluorouracil . 
cisplatin ( 80 mg / m ) was infused intravenously on day 1 and fluorouracil ( 1 g / m per day ) was administered intravenously on days 14 ( total 4 g / m )  . the investigational chemotherapy was four 3 - weekly cycles of ecx . 
epirubicin ( 50 mg / m ) and cisplatin ( 60 mg / m ) were given intravenously on day 1 and capecitabine ( 1250 mg / m daily ) was given orally continuously over all four cycles ( for a total of 12 weeks )  . protocols for chemotherapy dose modifications were provided for haematological , renal , neurological , and hepatic toxicities , and for palmarplantar erythema , stomatitis , diarrhoea , nausea , and vomiting . 
 centres were allowed to use a minimal access surgery approach after providing evidence that complication rates and lymph node yields were similar to an open surgery approach from at least 20 patients who had had minimal access oesophagectomy . the stomach was the preferred conduit for reconstruction based on the right gastric and right gastroepiploic vessels . 
lymph node clearance in the abdomen was at the origin of the left gastric artery and along the hepatic and splenic arteries , the upper lesser curve , and at the right and left cardiac lymph node stations . 
dissection at the diaphragm was used to minimise a positive radial or circumferential resection margin by inclusion of sufficient crural fibres and a cuff of diaphragm based on endoscopic ultrasonography and intraoperative appearances . 
the extent of proximal lymphadenectomy for the upper paraoesophageal nodes was determined by the extent of division of the oesophagus ( ie , the length of oesophagus remaining after resection )  . reconstruction was recommended above the aortic arch for the right - sided approach and just below it for the left , and preferably within 5 cm of the thoracic inlet . 
trans - hiatal surgery was not permitted . postoperative complications , described as none , present but not life threatening , or life threatening , were for the oe05 clinical trial protocol version 6.0 see research / documents / cancer_ protocols / oe05_protocol_ version_6_23_dec_09.pdf vol 18 september 2017 1251 articles recorded for each patient . 
these complications were reviewed clinically , and assigned to categories . processing of the surgical resection specimens and histopathological assessment of all materials were done according to the recommendations of the royal college of pathologists : 30 r0 , no tumour cells remaining within 1 mm of any resection margin ; r1 , microscopically visible positive margin indicating the presence of tumour cells at or within 1 mm of a longitudinal or radial or circumferential resection margin ; and r2 , macroscopically visible tumour remaining . 
for patients not listed in above , cause of death was reported as sepsis - related multiple organ failure in one patient and oesophageal cancer in the remaining two patients . 
 in terms of both interobserver agreement ( ie , likelihood of two pathologists concluding the same grading by their independent assessments ) and prognostic ability.32 , 33 pathology data were collected from local pathologists at each centre , and used for the primary analyses of all pathology data . 
the hrql protocol prespecified four domains of hrql to be examined in the primary analyses and full details of all scales and items assessed in the questionnaires will be reported subsequently . 
clinical follow - up involved the same schedule with the use of tests to establish recurrent disease at the discretion of individual centres . outcomes the primary outcome measure of the trial was overall survival . 
secondary outcomes were disease - free survival , effects on the primary tumour ( as assessed by mandard trg ) , hrql , and morbidity related to chemotherapy and surgery . 
exploratory outcomes were progression - free survival ( where a progression - free survival event was defined as the first confirmed local or distant recurrence , or death from any cause ) , and an analysis of mandard trg using an amended responder definition . statistical analysis the sample size calculations were based on the primary outcome measure of overall survival . 
on the basis of the oe02 trial results , 19 which showed an absolute survival difference of 8% at 3 years , we thought it unlikely that any greater difference would be seen in this study . 
with a 5% two - sided significance level , this sample would provide 90% power to detect an 8% difference ( or 1252 vol 18 september 2017 articles 80% power to detect a 7% difference ) in 3 - year survival , from 30% in the cf group . 
in 2007 , following a period of lower than expected recruitment , the sample size was reassessed to ensure that an adequately powered study would still be achieved in a given timeframe . 
the updated sample size calculations required 842 patients with 677 events over 6 years with a minimum follow - up of 2 years before analysis , to provide at least 82% power to detect an 8% difference ( and 70% to detect a 7% difference ) at 3 years with a two - sided significance level of 5% . although we anticipated that the required events would be obtained 2 years after the final patient was randomly assigned , they accrued far more slowly than expected . 
 3 years after the final randomisation , a conditional survival analysis was done to assess the probability that continuing to wait for the full number of events would lead to a different trial conclusion . 
after discussion with the independent data monitoring committee and trial steering committee , a decision was reached that the current data were sufficiently robust for full analysis and dissemination , because the chance of obtaining a different conclusion with more events was less than 5% . all safety and primary analyses were done on an intention - to - treat basis . 
 patients either lost to follow - up or still alive at the time of analysis were censored at the date they were last known to be alive . because patients can only be deemed disease free after surgery , and to account for the different durations of preoperative chemotherapy , disease - free survival was analysed using a landmark analysis.36 rather than the date of randomisation , the time 1 week after the last patient had surgery was used as the start point , up to a maximum of 6 months from group assignment . 
patients who had an event before this point , who did not have surgery , or who were not macroscopically disease free at surgery , were said to have had an event on day 1 . 
 disease - free survival was calculated as the time from this modified origin until the first date of confirmed local recurrence , distant metastases , or death from any cause . 
 patients who had no evidence of relapse were censored on the last date they were known to be disease free . progression - free survival was calculated from random assignment to the date of the event or , in event - free patients , the date last known to be alive and free from recurrence . 
 specific site of t4 invasion is mediastinal pleura for eight patients ( four in the cisplatin and fluorouracil group vs four in the epirubicin , cisplatin , and capecitabine group ) , crura for 14 patients ( nine vs five ) , and diaphragm for five patients ( two vs three )  . table 1 : baseline characteristics grambsch - therneau test . 
the heterogeneity of treatment effects across levels of prespecified patient characteristics ( sex , age , performance status , clinical t - stage , and clinical n - stage ) were explored using cox proportional hazard models . to analyse tumour regression , the original five - point into responders mandard scale was dichotomised ( mandard trg 13 ) and non - responders ( mandard trg 45 )  . 
a second , unplanned analysis was also done because emerging evidence suggested that a more appropriate dichotomisation was mandard trg 12 as responders and grades 35 as non - responders . formal comparisons and summaries of hrql function and symptom scales were restricted to a number of prespecified outcome measures . 
global hrql and the effects of prespecified symptoms related chemotherapy and surgery ( appetite loss , dysphagia , pain , and reflux ) were compared immediately before surgery , and 3 , 12 , and 24 months after surgery , using an anova with adjustment for baseline score . 
these timepoints were considered separately , rather than using a repeated measures method of analysis . between comparisons toxicities , surgical complications , tumour regression , and resection were done using a test or fishers exact test , as appropriate . 
the corresponding author had final responsibility for the decision to submit for publication . results between jan 13 , 2005 , and oct 31 , 2011 , 897 patients were recruited from 72 uk hospitals and randomly allocated to the cf group ( n = 451 ) or the ecx group ( n = 446 ; figure 1 )  . 
the median number of patients per centre cisplatin and fluorouracil ( n = 451 ) epirubicin , cisplatin , and capecitabine ( n = 446 ) 411 ( 91% ) 387 ( 87% ) 40 ( 9% ) 59 ( 13% ) 3 ( 8% ) 11 ( 19% ) 6 ( 10% ) 4 ( 10% ) 4 ( 7% ) 6 ( 15% ) 2 ( 5% ) 1 ( 3% ) 9 ( 15% ) 7 ( 12% ) 8 ( 14% ) reason for no surgery * ct evidence of disease progression 13 ( 33% ) clinical evidence of disease progression laparoscopic evidence of disease progression surgery done comorbidity patient choice patient died resection done patient otherwise deemed inoperable 11 ( 28% ) 14 ( 24% ) surgical approach abdomen and right chest open abdomen ( laparoscopic ) and right chest open left thoracoabdominal incision totally laparoscopic other missing location mid - oesophagus siewert type 1 siewert type 2 missing 192 ( 50% ) 108 ( 28% ) 187 ( 51% ) 101 ( 28% ) 28 ( 7% ) 9 ( 2% ) 43 ( 11% ) 7 ( 2% ) 24 ( 7% ) 9 ( 2% ) 35 ( 10% ) 8 ( 2% ) 72 ( 19% ) 56 ( 15% ) 227 ( 59% ) 208 ( 57% ) 76 ( 20% ) 12 ( 3% ) 89 ( 24% ) 11 ( 3% ) data are n ( % )  . 
an open - close operation was deemed as one in which no resection was done , or the reason given on the case report form for not having surgery was that the patient was found to be inoperable at laparotomy or thoracotomy . 
after was eight chemotherapy , following retrospective review of the baseline ct scan , one patient was found to be ineligible because of adrenal metastases so did not have surgery , but was included in all summaries and analyses . 
the median age was 62 years ( iqr 5667 ; range 2781 ) , 810 ( 90% ) of 897 patients were male , 603 ( 67% ) had a who performance status of 0 , and 576 ( 64% ) had stage t3n1 cancer ( table 1 ; appendix pp 45 )  . three ( 4% ) of 72 recruiting centres did not take part in the hrql aspect of the trial for any of their patients , and hrql assessment data were omitted at baseline for the [ 4% ] of the total patients from these centres ( 37 897 patients )  . 
baseline hrql was also well balanced see online for appendix 1254 vol 18 september 2017 articles ( 1834 ) , appetite ( 2405 ) , pain 203 between the two groups . 
mean values ( sd ) for the five prespecified domains of interest were : global hrql ( 2798 ) , 760 reflux 173 ( 2050 ) , and dysphagia 739 ( 257 ) ; data per treatment group are in the appendix ( pp 810 )  . 
a higher score indicates better hrql for the global score and dysphagia , but worse hrql for the symptom scales . loss 374 details of the chemotherapy received are shown in table 2 . 
four patients ( < 1% ; two in the cf group and two in the ecx group ) of 897 withdrew consent before starting chemotherapy and five ( 1% ; one cf , four ecx ) died during chemotherapy . 
the number of patients who completed their allocated treatment was greater in the cf group than in the ecx group ( 435 [ 96% ] of 451 vs 363 [ 81% ] of 446 ; p < 00001 ) , although a similar number of patients in the cf ( 435 [ 96% ] of 451 ) and ecx ( 432 [ 97% ] of 446 ) groups received at least two cycles . 
of the 451 patients in the cf group , eight ( 2% ) stopped chemotherapy because of toxicity and one ( < 1% ) died , whereas in the ecx group , 46 ( 10% ) of 446 patients stopped because of toxicity , and five ( 1% ) died , one of which was thought to be related to chemotherapy toxicity ( figure 1 )  . 
the number of patients requiring dose reduction to any drug was smaller in the cf than in the ecx group ( 88 [ 20% ] of 451 vs 187 [ 42% ] of 446 ; p < 00001 ) , although the number receiving cisplatin dose reductions was similar between the groups ( 61 [ 14% ] of 451 in the cf group and 53 [ 12% ] of 446 in the ecx group )  . the median time from randomisation to surgery was 71 days ( iqr 6680 ) in the cf group and 127 days ( 119137 ) in the ecx group . 
the median time of surgery from the start of the last preoperative chemotherapy cycle was 44 days ( 3952 ) for patients in the cf group and 57 days ( 5264 ) for patients in the ecx group . 
of the 99 who did not have surgery , 41 ( 41% ) were because of disease progression , nine ( 9% ) died before surgery , nine ( 9% ) decided not to have surgery , that ( 15% ) developed significant comorbidities precluded surgery , and 25 ( 25% ) were deemed otherwise unsuitable for surgery . 
in total , 411 ( 91% ) of 451 patients in the cf group and 387 ( 87% ) of 446 patients in the ecx group proceeded to surgery ( figure 1 )  . 751 ( 84% ) of 897 people had resection and reconstruction , whereas 47 ( 5% ) of 897 patients were found to have progressive disease or to be inoperable during surgery ( table 3 )  . 
588 ( 78% ) of 751 resections were done via the abdomen and right chest using open surgery throughout ( ivor - lewis resection ) or as hybrid with a laparoscopic abdominal approach . 
the median follow - up of the surviving patients was 64 years ( iqr 4882 ) , and 250 ( 93% ) of 268 patients had at least 3 years of follow - up assessments . 
median overall survival was estimated to be 234 months ( 95% ci 206263 ) in the cf group and 261 months ( 225297 ) in the ecx group , with an hr of 090 ( 95% ci 077105 , p = 019 )  . 
no evidence indicated that the proportional hazards assumption was violated . figure 3 shows prespecified subgroup analyses of overall survival were done , considering sex , age group ( < 60 years , 6069 years , and 70 years ) , who performance status , clinical t - stage , and clinical n - stage ( appendix p 11 )  . median disease - free survival ( 347 events in the cf group vs 316 events in the ecx group , based on a 6 - month landmark analysis ; appendix p 13 ) was 116 months ( 95% ci 89133 ) in the cf group and 144 months ( 117165 ) in the ecx group , with an hr of 086 ( 95% ci 074100 , p = 0051 )  . chemotherapy toxicity data were not provided by three patients in each group and two in each group did not receive any chemotherapy . 
p values for heterogeneity of treatment effect are 069 for sex , 005 for age , 046 for who performance status , 011 for t - stage , and 0028 for n - stage . 
one patient in the epirubicin , cisplatin , and capecitabine group died of cerebrovascular incident ( reported as other toxicity )  . table 4 : chemotherapy toxicity group ( 0 , p < 00001 )  . 
 in patients for whom data were reported , no difference was seen in the overall prevalence of surgical complications between the two treatment groups ( 224 [ 56% ] of 398 people in the cf group and 233 [ 62% ] of 374 in the ecx group ; p = 0089 ) , although more people in the ecx group had respiratory complications ( 125 [ 33% ] of 374 ) than in the cf group ( 107 [ 27% ] of 398 ; p = 0048 ; appendix p 7 )  . 
at 30 days after surgery , ten ( 2% ) of 411 patients in the cf group and 11 ( 3% ) of 387 people in the ecx group had died , and at 90 days , 21 ( 5% ) people in the cf group and 23 ( 6% ) people in the ecx group had died . in the local pathologist review ( table 5 ) , the primary tumour was classified as mandard trg 13 in 44 ( 15% ) of the 288 specimens with available results from the cf group and 93 ( 32% ) of the 289 specimens from the ecx group ( p < 00001 )  . 
mandard primary tumour regression data were also available from central pathology review of 656 patients ( 87% of patients who had a resection ) and a total of 24 625 slides were received , with a median of 34 ( iqr 2445 ) slides per person . 
the proportions of patients who achieved r0 , r1 , and r2 were similar in both groups . no statistically and clinically relevant differences were seen between the treatment groups in terms of hrql ( appendix pp 810 ) in any of the prespecified domains ( global quality of life , pain , reflux , appetite loss , or dysphagia ) or at nearly all timepoints ( preoperatively and 3 , 12 , and 24 months postoperatively )  . 
r0 = no tumour cells within 1 mm of any resection margr1 = presence of tumour cells at or within 1 mm of a longitudinal or radial or circumferential resection marg r2 = macroscopically visible tumour left behind during surgery . 
the proportion of surviving patients who time , completed hrql assessments declined over with 725 ( 84% ) of 860 patients completing an assessment at randomisation , 339 ( 57% ) of 595 at 3 months after surgery , 208 ( 45% ) of 467 at 12 months , and 142 ( 44% ) of 322 at 24 months . when the trial and analyses were planned , we felt that mandard trg 1 , 2 , or 3 was the most suitable definition of good response to treatment . 
exploratory analyses ( appendix p 14 ) in patients who had available specimens suggested that postoperative survival of patients with tumours considered to be mandard trg 1 or 2 was significantly different ( appendix p 14 ) to survival in those with tumours considered to be mandard trg 3 , 4 , or 5 , so mandard trg 1 or 2 appeared to denote significant tumour regression . 
applying this definition to the locally collected histopathological data , 18 ( 6% ) of 288 patients in the cf group and 48 ( 17% ) of 289 patients in the ecx group regression ( p < 00001 )  . 
similarly , using the central review data , 12 ( 4% ) of 339 patients in the cf group and 37 ( 12% ) of 317 patients in the ecx group achieved notable tumour regression ( p < 00001 )  . significant achieved tumour in the exploratory analysis of progression - free survival , median progression - free survival ( 343 events in the cf group vs 313 in the ecx group ; appendix p 13 ) was vol 18 september 2017 1257 articles 184 months ( 95% ci 152205 ) in the cf group and 214 months ( 194240 ) in the ecx group , with an hr of 084 ( 95% ci 072098 , p = 0033 )  . 
the contributing progression - free survival event was either local recurrence ( 60 [ 17% ] of 343 patients in the cf group vs 46 [ 15% ] of 313 in the ecx group ) , distant metastases ( 94 [ 27% ] of 343 people vs 78 [ 25% ] of 313 ) , local recurrence and distant metastases ( 87 [ 25% ] of 343 vs 59 [ 19% ] of 313 ) , or death without confirmed progression ( 102 [ 30% ] of 343 vs 130 [ 42% ] of 313 )  . an exploratory analysis highlighted that the overall survival hr did not remain constant over time , and a strong interaction with year of randomisation was seen ( p = 00004 ; appendix p 12 )  . 
patients randomly assigned early in the trial ( 200507 ) had some survival benefit in the ecx group compared with those in the cf group , whereas those assigned in later years ( 2008 onwards ) did not . 
the use of pet scans increased greatly over the course of the trial , and so a further exploratory subgroup analysis was done looking at the effect of receiving a pet scan . 
 patients who did not have a pet scan had longer overall survival in the ecx group , whereas for patients who did receive a pet scan , ecx gave no survival advantage . discussion this study showed that more intensive neoadjuvant chemotherapy with four cycles of ecx provided no overall or disease - free survival advantage over two cycles of cf in 897 patients with oesophageal adenocarcinoma . 
chemotherapy toxicity and serious adverse events were reported more often with ecxas can be expected from four cycles of a triplet regimen compared with two cycles of a doublet regimen . 
these adverse events contributed to a greater number of patients completing their planned chemotherapy and undergoing surgery in the cf group than in the ecx group , although surgical resection , postoperative complications , and postoperative mortality were similar between the groups . 
in a post - hoc exploratory analysis , improved progression - free survival was shown with ecx treatment compared with cf treatment . more patients in the ecx group had a good pathological response to chemotherapy ( mandard trg 1 or 2 ) , and consequently more were staged as ypt0 or 1 or ypn0 after surgery , than were those in the cf group . 
results from the mrc gastro - oesophageal st0338 study showed that mandard trg 1 or 2 after chemotherapy was associated with improved survival compared with mandard trg 3 , 4 , or 5 . 
however , the absolute numbers of specimens assessed that were classified as mandard trg 1 or 2 ( 48 [ 17% ] of 289 in the ecx group vs 18 [ 6% ] of 288 in the cf group ) were low , and so this difference did not translate into an overall survival benefit . the results of this trial raise the question of the optimal number of preoperative chemotherapy cycles . 
in the current absence of a reliable biomarker that enables prediction of responses either before or midway through preoperative treatment , the extent of preoperative chemotherapy relies on the judgement of the clinician after discussion with the patient , to balance the possibility of achieving a good response against the risk of not being able to proceed to surgery . 
 however , two cycles of cf preoperatively has not been the perioperative approach directly compared with assessed in the magic trial , 25 which studied three cycles of ecx given preoperatively and post operatively . 
given the increased proportion of patients who achieved a response with ecx treatment in our study , a smaller number of preoperative cycles ( two or three ) with a triplet regimen combined with the selective use of postoperative chemotherapy for responding patients might be a better approach than either four cycles of ecx or two cycles of cf . oe05 showed an improvement in overall survival of patients in the cf group ( recruited 200511 ) compared with the same regimen in oe02 ( recruited 199298 ) , in which the median survival was 14 years compared with 20 years in oe05 . a number of potential factors could explain why the survival of patients with oesophageal cancer who were treated with cf improved with time . 
changes in referral patterns , moves towards centralisation of surgical services , the introduction of endoscopic ultrasonography , and the development of multidisciplinary teams are all events that occurred towards the end of recruitment to the oe02 study , and these changes might have led to better patient selection for attempted curative treatment by the time of this oe05 study . 
post - hoc analyses indicated that ecx offered a survival benefit in the early years of the study when pet scans were rarely used , but offered no benefit during the later years when pet was used for nearly all patients . 
patients with this type of disease are now usually identified and would have been ineligible for participation in the study . neoadjuvant chemoradiotherapy has also improved survival compared with surgery alone for patients with oesophageal adenocarcinoma and squamous cell cancers , with a median survival of 486 months ( 95% ci 321651 ) with adjuvant therapy compared with led 1258 vol 18 september 2017 articles 240 months ( 95% ci 142337 ) with surgery alone in the cross trial.39 the hrs for comparison with surgery alone are similar with chemoradiotherapy in cross ( 073 [ 95% ci 055088 ] in patients with adeno carcinoma ) and with chemotherapy in magic ( 075 [ 060093 ] ) , suggesting trials studied slightly different that although populations , the size of benefit might be similar . 
trials comparing these two approaches directly20 , 23 , 24 have shown an increased response with chemo radiotherapy , but without any subsequent improvement in overall survival . the the present study has a number of advantages over other oesophageal cancer trials . 
this study was confined to patients with adenocarcinomas of the oesophagus and gastro - oesophageal junction ( siewert type 1 and 2 ) , specifically excluding squamous cell cancers and siewert type 3 ( gastric cancer )  . 
to our knowledge , our study is the only prospective randomised trial in neoadjuvant treatment and surgery for oesophageal cancer to have included a comprehensive prospective assessment of hrql using validated generic and specific measures . 
 although no differences between trial groups were observed in hrql , the data confirm findings from much smaller cohort studies.40 neoadjuvant chemotherapy and surgery are associated with reduced hrql that persists for more than 6 months after surgery , and some features such as appetite loss persist for at least 12 months . 
 these hrql results should be accepted as the standard that can be achieved with current platinum - based or fluoropyrimidine - based neoadjuvant chemotherapy and surgery , and communicated to patients during shared decision making before surgery , along with the likely median survival data of the combined interventions . 
 limitations of this study include the changing use of pet scanning through the course of this trial as we have discussed and its potential effect on the prognosis of patients who entered the trial over time . 
additional limitations are the fact that postoperative chemotherapy was not assessed , and the challenge of interpreting and implementing these results in the face of the evolving role of chemoradiation in the management of oesophagogastric adenocarcinomas . data published in 2017 show a survival advantage for patients treated with docetaxel , oxaliplatin , and fluorouracil compared with epirubicin , cisplatin , and fluorouracil or ecx given perioperatively for junctional and gastric tumours , with a 3 - year overall survival of 57% for the docetaxel - containing regimen compared with 48% with epirubicin , cisplatin , and fluorouracil or ecx ( hr 077 , 95% ci 063094 ) .41 though an improvement in overall survival for biomarker - unselected patients , these results highlight that further improvements in outcomes are still needed for these patients . 
alternative neoadjuvant approaches such as chemoradiation are also being investigated.42 , 43 additional correlative science projects are planned for this trial with the aim of identifying subsets of patients who might specifically benefit from ecx neoadjuvant chemotherapy . contributors da and dc were joint chief investigators . 
all authors were involved in data interpretation , manuscript review , and approval of the final manuscript . declaration of interests dc reports grants from amgen , astrazeneca , bayer , celgene , merrimack , medimmune , merck serono , sanofi , and the national institute of health biomedical centre at the institute of research and royal marsden hospital . 
lancet oncol 2013 ; 14 : e436in this correspondence , the authors names should read athanassios kyrgidis , thrasivoulos - george tzellos , anastasia trigoni , stefanos triaridis and their a liations as 1st department of otolaryngologyhead & neck surgery ( ak , st ) and department of clinical pharmacology ( tgt ) , aristotle university of thessaloniki , thessaloniki , greece ; hospital for skin and venereal diseases , thessaloniki , greece ( at )  . 
 these corrections have been made as of oct 28 , 2013 . vol 14 november 2013 e493 effect of patient choice and hospital competition on service configuration and technology adoption within cancer surgery : a national , population - based study ajay aggarwal , daniel lewis , malcolm mason , arnie purushotham , richard sullivan , jan van der meulen summary background there is a scarcity of evidence about the role of patient choice and hospital competition policies on surgical cancer services . 
in this national , population - based study we investigated the effect of patient mobility and hospital competition on service configuration and technology adoption in the national health service ( nhs ) in england , using prostate cancer surgery as a model . methods we mapped all patients in england who underwent radical prostatectomy between jan 1 , 2010 , and dec 31 , 2014 , according to place of residence and treatment location . 
for each radical prostatectomy centre we analysed the effect of hospital competition ( measured by use of a spatial competition index [ sci ] , with a score of 0 indicating weakest competition and 1 indicating strongest competition ) and the effect of being an established robotic radical prostatectomy centre at the start of 2010 on net gains or losses of patients ( difference between number of patients treated in a centre and number expected based on their residence ) , and the likelihood of closing their radical prostatectomy service . findings between jan 1 , 2010 , and dec 31 , 2014 , 19 256 patients underwent radical prostatectomy at an nhs provider in england . 
37 ( 57% ) of the 65 centres had a significant net loss of patients , of which two ( 5% ) were established robotic centres and ten ( 27% ) closed their radical prostatectomy service during the study period . 
radical prostatectomy centres that closed were more likely to be located in areas with stronger competition ( highest sci quartile [ 087092 ] ; p = 00081 ) than in areas with weaker competition . 
the number of centres performing robotic surgery increased from 12 ( 18% ) of the 65 centres at the beginning of 2010 to 39 ( 71% ) of 55 centres open at the end of 2014 . interpretation competitive factors , in addition to policies advocating centralisation and the requirement to do minimum numbers of surgical procedures , have contributed to large - scale investment in equipment for robotic surgery without evidence of superior outcomes and contributed to the closure of cancer surgery units . 
if quality performance and outcome indicators are not available to guide patient choice , these policies could threaten health services ability to deliver equitable and affordable cancer care . lancet oncol 2017 ; 18 : 144553 published online october 3 , 2017 s1470 - 2045 ( 17 ) 30572 - 7 see comment page 1424 department of health services research & policy ( a aggarwal md , prof j van der meulen phd ) and department of social and environment health research ( d lewis phd ) , london school of hygiene & tropical medicine , london , uk ; clinical effectiveness unit , royal college of surgeons of england , london , uk ( a aggarwal , prof j van der meulen ) ; school of medicine , cardiff university , cardiff , uk ( prof m mason md ) ; and division of cancer studies ( prof a purushotham md ) and institute of cancer policy ( prof r sullivan md ) , kings college london , london , uk correspondence to : dr ajay aggarwal , department of health services research & policy , london school of hygiene & tropical medicine , london wc1h 9sh , uk ajay.aggarwal@lshtm.ac.uk funding national institute for health research . copyright the author ( s )  . 
in health - care systems where hospitals compete on quality and not on price , competition is also in others8with expected to incentivise improvements in the quality of hospital services to attract patients.9 choice and competition , as well as centralisation , attempt to achieve improvements in patient outcomes , but they require different health - system configurations and provider incentives to operate effectively . 
finding the right balance between choice and competition on the one hand and centralisation on the other is therefore key , but there is little evidence to guide how best to achieve this.10 the uk national health service ( nhs ) is an example of a health system that remains committed to choice and competition as a health - care reform model since the inception of this model in 2006.11 the cost of providing vol 18 november 2017 1445 articles research in context evidence before this study several countries have introduced policies that allow patients to choose a specific health - care provider , with the aim of improving the quality of care . 
we did a systematic review to assess the evidence that patients with cancer are willing to travel beyond ( bypass ) their nearest hospital for cancer surgery , and to assess the effect of competition on outcomes of surgery . 
there was significant heterogeneity in the design of empirical studies , including differences in data quality , the geographical unit of analysis , and limited control for the influence of price competition . 
no studies had looked at the effect of competition on outcomes of cancer . added value of this study to our knowledge , this is the first national evaluation of the effect of choice and competition policies on the patterns of service configuration and technology adoption for cancer surgery . 
 the mobility of men to alternative , more distant centres resulted in substantial changes in market share for individual surgical centres , which were most marked in areas of highest competition . 
we found that , between 2010 and 2017 , there has been large - scale adoption of robot - assisted radical prostatectomy , increasing by three times , from 12 centres at the start of 2010 to 42 by 2017 . 
during the same time period , 16 of the 65 nhs radical prostatectomy centres in england closed their prostate cancer surgery unit . implications of all the available evidence patients with cancer respond to policies that enable them to choose a surgical provider of their choice . 
in the absence of appropriate information about quality of care , policies based on patient choice and hospital competition could create incentives for adoption of new technologies without evidence of superior outcomes as hospitals look to retain and attract new patients . 
 the resulting changes in market share for individual hospitals could threaten the viability of their surgical services . services is fixed under a national rate tariff scheme12 and hospitals are expected to compete for patients on the basis of quality . 
receiving care incurs no additional user charges at the point of access and patients have the right to choose and travel to any hospital that best meets their needs . additionally , national policy in the uk continues to advocate centralisation of specialist cancer services such as prostate and oesophagogastric surgery.1316 not only does this serve to reduce the number of hospitals that patients with cancer can choose from , but it is also expected that patients will receive care at their nearest ( local ) centre on the basis of established secondary care referral pathways for specialist cancer surgery.17 however , our 2017 analysis18 found that not all patients are following the expected referral patterns for specialised cancer surgery . 
one in three men who had a radical prostatectomy for prostate cancer between 2010 and 2014 in the nhs travelled beyond or bypassed their nearest prostate cancer surgery centre , in many cases across regional boundaries . 
in the absence of indicators that accurately reflect the quality of prostate cancer surgery , men were attracted to centres offering robot - assisted radical prostatectomy or centres that employed surgeons with a national reputation for prostate cancer surgery . there is little evidence about what effect patient mobility and hospital competition have had on the configuration of specialist cancer services and the introduction of new surgical technologies into clinical practice . 
we used patient - level data and geographical information system modelling to analyse the effect of patient mobility for cancer surgery and hospital competition on service configuration and technology adoption within the nhs , using prostate cancer as a model . 
in light of our findings , we appraised the international evidence exploring the role of choice and competition policies on the delivery of cancer surgery services and considered opportunities for developing the empirical research base in this area . methods patient population for this national , population - based study we obtained individual patient - level data from the national cancer registration and analysis service ( ncras ) for all men who were diagnosed with prostate cancer and underwent a radical prostatectomy in the nhs in england between jan 1 , 2010 , and dec 31 , 2014 . 
these data were linked at the individual patient level to hospital episode statistics ( hes ) , the administrative database of all hospital episodes in nhs hospitals in england.19 the study was exempt from nhs research ethics committee approval because it involved analysis of an for service existing dataset of anonymised data evaluation . see online for appendix for more on hospital episode statistics see digital.nhs.uk / hes 1446 vol 18 november 2017 articles study design to define each individual patients residence , we used the population - weighted centroids of small geographical areas termed lower super output areas ( lsoas )  . 
there are 34 753 of these small geographical areas ( ie , lsoas ) in england , with an average population of about 1600.20 both the lsoas and full postcodes for the hospitals where the surgery was done were inputted into a geographical information system ( esri arcgis 10.3 ) to calculate travel times according to the fastest route by car to all surgical centres in england ( calculated by use of the ordnance survey mastermap integrated transport network )  . 
those who did not receive care at their nearest surgical centre were classified as bypassers . for each surgical centre , we identified the number of leaverspatients for whom that centre was nearest but who had their treatment at an nhs centre further away . 
a centre was identified as being a winner ( ie , having a net gain of patients ) or loser ( ie , having a net loss of patients ) if the difference between leavers and arrivers was statistically significant based on the conditional method for testing a difference between two poisson means.21 for each surgical centre we calculated a spatial competition index ( sci ) as a measure of external competition.22 , 23 the sci provides a uniform metric that can be used across all surgical centres and that represents the demand for services and the availability of alternative hospitals . 
 conversely , london is 1572 km in size ( and the largest urbanised region in europe ) and had ten surgical centres at the start of the study period.24 ( one of nine english regions ) data analysis in this analysis , the sci for a surgical centre was calculated on the basis of both the number of eligible patients within a 60 - min drive and the number of surgical centres within a 60 - min drive for each eligible patient ; in the equation shown , the surgical centre i has n eligible patients within a 60 - min drive , and patient j in centre i has k surgical centres within a 60 - min drive : scii = 1 1 ji = 1 the sci ranges theoretically from 0 for centres in a monopoly environment to a value close to 1 for centres in the most competitive environment . at the start of the study period ( january , 2010 ) there were 65 prostate cancer surgical centres in england , of which 12 centres routinely performed robot - assisted radical prostatectomy procedures . 
an analysis of hes data , in addition to an organisational survey produced as part of the national prostate cancer audit , 17 was used to evaluate the change in configuration of prostate cancer surgical units across england and the availability of robotic surgery from 2010 onwards . 
all analyses were done with stata , version 14 , to assess the effect of competition , as measured by the sci , on changes in service configuration ( expressed as net gains or losses of patients as defined above ) and adoption of robotic surgery in the nhs . role of the funding source the funder of the study , national institute for health research , had no role in study design , data collection , data analysis , data interpretation , writing of the report , or the decision to submit for publication . 
aa and jvdm had full access to all the data in the study , take responsibility for the integrity of the data and the accuracy of the data analysis , and had final responsibility for the decision to submit for publication . results we identified 19 518 men who were diagnosed with prostate cancer and underwent radical prostatectomy in 19 518 men with hes - linked cancer repository records received radical prostatectomy from 2010 to 2014 19 365 men living in england received radical prostatectomy at an nhs provider in england 153 men excluded who lived outside england : scotland ( n = 8 ) , isle of wight ( n = 67 ) , wales ( n = 78 ) 109 men excluded as the treatment provider was not a recognised nhs provider or the provider was not operational on the date when the surgery was done 19 256 men matched to 65 providers of prostate cancer surgery 19 256 men included in nal cohort figure 1 : flowchart of men included in the study hes = hospital episode statistics . 
nhs = uk national health service . vol 18 november 2017 1447 articles a 50 km 25 km patient origins core users arrivers leavers radical prostatectomy centre 1 dot = 1 patient 100 km 100 km figure 2 : mobility patterns of patients receiving radical prostate cancer surgery at two selected nhs cancer centres maps of the uk , illustrating the mobility pattern of patients who received radical prostate cancer surgery at two selected national health service ( nhs ) cancer centres ( indicated with a + symbol in the area of core users ) located in the east of england ( a ) and southwest england ( b ) that had a net gain of patients from outside their local area ( ie , more arrivers than leavers )  . 
contains national statistics data , crown copyright and database right 2017 ; nhs research scotland ( nrs ) data , crown copyright and database right 2017 ; ordnance survey data crown copyright and database right 2017 ; and northern ireland statistics and research agency data . 
 of these 19 518 men , 262 ( 13% ) were excluded because they either lived outside england or could not be assigned to a particular hospital ; 19 256 were eligible for inclusion in the study ( figure 1 )  . figure 2 shows the places of residence for patients who had their prostate cancer surgery at two selected surgical centres located in the east of england ( figure 2a ) and southwest england ( figure 2b ) , both of which were classified as winners . 
conversely , some of the losers were doing approximately 200 fewer procedures than expected ( and 400 fewer in the case of one centre )  . figure 3 also shows the relationship between , on the one hand , radical prostatectomy centres having a net gain or net loss of patients and , on the other hand , being an established robotic centre or a centre that closed during the study period . 
centres with a net gain were 13 15 19 21 43 45 49 51 55 57 61 63 31 33 25 27 radical prostatectomy centre 37 39 figure 3 : net gains and losses of patients for each radical prostatectomy centre ( n = 65 ) during the study period established robotic radical prostatectomy centres ( n = 12 ) shown in green and centres that closed during the 201014 study period ( n = 10 ) shown in red . 
centres in blue are centres that were neither robotic radical prostectomy centres nor centres that closed during the study period . 1448 vol 18 november 2017 articles s 100 200 300 400 500 more likely to be established robotic centres ( ten [ 43% ] of the 23 winners were robotic centres , compared with two [ 5% ] of the 37 centres with a net loss ; p = 00043 )  . 
 conversely , ten ( 27% ) of the 37 centres with a net loss of patients closed down during the study period . centres with the largest net gains or losses were predominantly located in the most competitive areas ( figure 4 )  . 
seven ( 41% ) of the 17 centres in the highest sci quartile were established robotic centres compared with five ( 10% ) of the 48 other centres in the three other quartiles ( p = 00050 )  . 
similarly , for centre closures , six ( 35% ) of the 17 centres in the highest sci quartile closed compared with four ( 8% ) of the 48 other centres ( p = 00081 )  . 
 both the analysis of hes and the results of the national organisational survey showed profound changes in the organisation and practices of prostate cancer surgical care that continued beyond the end of the study period ( figure 5 )  . 
between 2010 and 2017 , there has been large - scale adoption of robotic surgery , increasing by three times , from 12 ( 18% ) of 65 centres open at the start of 2010 to 39 ( 71% ) of 55 centres open in 2014 to 42 ( 86% ) of 49 in 2017 . 
both the closures and the rapid and widespread adoption of robotic surgery have been unforeseen , effectively rendering commissioning guidelinespublished only in 2015 and recommending phased introduction of robotics for prostate cancer surgery within the nhsobsolete.25 discussion our results suggest that , during the study period analysed , patient choice and hospital competition , rather than a coordinated policy towards centralisation , have been drivers in the changing configuration of surgical cancer services . 
the proportion of patients who bypassed their nearest hospital to have prostate cancer surgery elsewhere has been far larger than the 510% considered to be necessary in the health economics literature to incentivise improvements in hospital quality.26 in the absence of data on outcomes , the mobility of patients has been driven by factors such as availability of advanced surgical technology and the reputation of individual hospitals and clinicians.18 the resulting competition between hospitals has contributed to the closure of radical prostatectomy centres in the nhs in england and widespread adoption of robot - assisted radical prostatectomy as centres have had to respond to potential changes in their market share , which threatened both their income and their ability to meet minimum procedure volume requirements . 
this finding indicates that patient choice and hospital competition , although rarely considered in redesign of cancer services , are potentially powerful drivers of service change , even spatial competition index figure 4 : effect of competition on the net gain or loss of patients for each radical prostatectomy centre during the study period the size of the circles corresponds to the number of men expected to have surgery at the centre . 
 robotic centres total surgical centres 2009 2010 2011 2012 2014 2015 2016 2017 2013 year figure 5 : changes in the number of robotic centres and total number of centres in the nhs in england ( 200917 ) within publicly funded systems . 
it is unlikely that these findings are limited to the nhs in england or to prostate cancer surgery alone . from a wider system perspective , the geographical layout of cancer services means that not all centres face the same competitive pressures and , in turn , will respond differently to choice and competition policies as mechanisms for quality improvement . 
however , we found that patients were prepared to travel substantial distances for treatment , in some cases bypassing several surgical units , which means that even centres within less competitive areas face some level of external competition for patients and subsequently become late adopters of technology to retain local patients.27 vol 18 november 2017 1449 articles attempts to coordinate cancer care services through centralisation and regionalisation have largely ignored the fact that patients are prepared to bypass their local services for treatment . 
this occurrence is partly due to the paucity of empirical evidence about the extent of patient mobility.2830 additionally , cancer care plans have exerted limited control of the available services and technology at the individual hospital level ( eg , introduction of new devices and practices of care ) , which can serve as proxy measures of quality in the absence of quality indicators.31 substantial levels of patient mobility mean that centres need to compete with other providers to meet minimum procedure volume thresholds as set down by national policy.16 in england , each prostate cancer surgery centre is expected to do a specified number of operations per year or face the threat of closure.15 , 32 competition policies have therefore stimulated a form of centralisation through natural selection , as centres act to protect their status as a cancer surgery centre , rather than through a coordinated process based on valid indicators of quality . 
 similar effects have been observed in the us health - care market , where both acute and non - acute care services have closed in response to competition.33 , 34 it is unclear whether these effects have improved the quality of care . none of the centres that closed during the study period did so because of explicit evidence of poor quality . 
further research is required to establish what effect the observed pattern of closures has had on travel times , outcomes , and equity in access to surgical services for the most vulnerable groups , given their decreased ability to travel.28 , 35 the patterns of patient mobility observed occurred at a time when comparative outcome measures for prostate cancer surgery were not available . 
this observation highlights that providers of cancer services , just like any other industry , will consider the use of alternative incentives to attract or retain patients.3638 patients will gravitate to places that make themselves attractive and by doing so they will create centres that treat large numbers of patients , which itself will attract further patients.39 patients with prostate cancer were more likely to travel to centres that were early adopters of robot - assisted radical prostatectomy , showing the powerful effect of advanced technology on perceptions of quality . 
the result of this travel pattern has been that other centres have invested in costly robotic surgery to avoid losing their patients to other centres and to maintain their market share to preserve their cancer centre status , despite a scarcity of evidence for the superiority of this surgical procedure with respect to functional and oncological outcomes.40 , 41 notably , none of the centres that adopted robotic surgery closed down . 
similar patterns have been observed in other health - care markets across the usa and europe , with cancer centres adopting robotic surgery to increase their market share.36 , 4244 our previous systematic review of the literature on patient choice and competition28 identified five empirical studies in high - income settings showing that patients with several tumour types , including breast , bladder , gastric , colorectal , and thoracic cancers , were prepared to bypass their nearest surgical centre.4550 the availability of advanced surgical techniques , procedure volume , and both surgeon and hospital reputation were identified as key drivers for patient mobility . 
patients of advanced age and from low socioeconomic backgrounds were less likely to consider alternatives than those who were younger and more affluent . hospital competition , rather than the pursuit of better quality care by itself , is also cited as a major factor influencing the adoption of new technologies and diversifying individual practices of care for both cancer surgery and radiotherapy.51 there is growing evidence of rapid adoption of technology for cancer surgery across a range of cancer types , beyond prostate cancer , such as renal , colorectal , and gynaecological cancer surgery.36 , 5255 for radiotherapy , where one would expect potentially less patient mobility than is normally observed for services because of the protracted duration of radiotherapy regimens , the past decade has also seen a substantial increase in the use of an array of high - cost technologies.41 these technologies have included intensity - modulated radiotherapy , and proton - beam therapy , with providers trying to gain a competitive advantage over others.51 stereotactic - beam radiotherapy , the question as to whether competition can stimulate improvements in outcomes of cancer surgery remains unanswered . 
two studies have analysed the effect of hospital competition on the pricing of pancreatic cancer56 and colon cancer57 surgery , and one study assessed the effect of such competition on the efficiency of cancer care delivery across tumour types in the us cancer health - care market.58 studies across other specialties have shown mixed results for the effect of fixed - price markets on improvements in health - care quality . 
8 , 23 , 5966 the dearth of studies on patient mobility in both high - income and emerging economies is a major limitation for evidenced - based policy making to decide how best to balance patient choice and top - down policy approaches to service coordination in cancer care . 
we have highlighted potential approaches for management of this health system challenge . for patients , having choice over their treatment or how a specific treatment is given might be more important than having a choice over the actual service provider.67 therefore , differences in availability of technology at the local level , even within a system that publishes validated outcome measures , can contribute to shifts in market share.28 investment in medical devices for cancer care51 seems to be driven predominantly by individual clinicians and clinical departments , possibly because the regulatory hurdles for adoption of new devices are relatively low compared with those of medicines.31 , 68 1450 vol 18 november 2017 articles the use of health technology assessment processes or value frameworks for all new technologies across the cancer care spectrum ( ie , medicines , radio therapy , and surgery ) would act as a meaningful first step towards providing stronger guidance on which inter ventions are likely to deliver the greatest value to patients and society.69 , 70 other options for coordination of technology adoption include coverage with evidence development schemes or establishment of nationally designated research centres to trial new technologies before considering reimbursement.71 however , a significant time lag remains before functional and oncological outcomes will be available inform national implementation , especially for conditions with a lengthy disease coursesuch as prostate cancer . competition between hospitals will continue irrespective of attempts to centralise cancer services . 
 whether public reporting of performance indicators could help to achieve improvements in care quality through competition is debatable.72 it might never be feasible to develop meaningful indicators for some tumour types . 
for example , the appropriateness of many available indicators is problematic because they can only be published after a long lag period ( eg , side - effects and survival rates at 1 and 5 years ) , during which clinical practice can change substantially.73 additionally , there is little evidence to suggest that individuals are more likely to use published performance indicators than proxies for quality , such as a hospitals or clinicians reputation.74 , 75 however , in the absence of any indicator , hospitals will try to differentiate themselves to attract new users , and patients will continue to be reliant on lay sources of industry marketing.76 this information , observation strengthens the need to develop and provide access to performance indicators across different tumour types to inform patients decision making . 
performance indicators are publicly available for oesophageal and bowel cancer surgery in the nhs.77 , 78 additionally , the national prostate cancer audit has completed a national patient reported outcome measures ( proms ) collection exercise for men following radical surgery or radiotherapy , with the aim of reporting risk - adjusted outcomes at the individual hospital level.79 public reporting of outcomes would mean improvement could be stimulated through hospitals competing for market share or aiming to avoid reputational losses.80 , 81 that quality including finally , the configuration of cancer services needs to account for existing patterns of patient mobility , hospital capacity , catchment areas , and clinical quality . 
to this end , location - allocation modelling provides a rigorous empirical approach to optimising the configuration of health - care services ( including decisions about service centralisation ) .82 , 83 for example , it can guide which centres should close to maximise outcomes , or minimise travel distances for those individuals who face difficulties in accessing services because of financial and physical constraints.82 , 84 a limitation of our study is that we used centroids of the lsoas as the representation of the patients residence . 
it is likely that this noise has attenuated rather than enhanced the observed relationships between spatial competition and technology adoption on the one hand and patient mobility on the other . influence on in conclusion , we show that patient choice and hospital competition can have a major the configuration of cancer services . 
all authors were involved in revising the work critically and approved the final version . declaration of interests jvdm reports grants from healthcare quality improvement partnership during the conduct of the study . 
the views expressed in this publication are those of the authors and not necessarily those of the nhs , the national institute for health research , or the department of health . 
we thank graham davies for his valuable comments and insights during the drafting of the manuscript . articles dose - dense cisplatin - based chemotherapy and surgery for children with high - risk hepatoblastoma ( siopel - 4 ) : a prospective , single - arm , feasibility study jzsef zsiros , laurence brugieres , penelope brock , derek roebuck , rudolf maibach , arthur zimmermann , margaret childs , daniele pariente , veronique laithier , jean - bernard otte , sophie branchereau , daniel aronson , arun rangaswami , milind ronghe , michela casanova , michael sullivan , bruce morland , piotr czauderna , giorgio perilongo , for the international childhood liver tumours strategy group ( siopel ) * summary background the objective of this study was to establish the e cacy and safety of a new treatment regimen consisting of dose - dense cisplatin - based chemotherapy and radical surgery in children with high - risk hepatoblastoma . methods siopel - 4 was a prospective single - arm feasibility study . 
patients aged 18 years or younger with newly diagnosed hepatoblastoma with either metastatic disease , tumour in all liver segments , abdominal extrahepatic disease , major vascular invasion , low fetoprotein , or tumour rupture were eligible . 
treatment consisted of preoperative chemotherapy ( cycles a1a3 : cisplatin 80 mg / m per day intravenous in 24 h on day 1 ; cisplatin 70 mg / m per day intravenous in 24 h on days 8 , 15 , 29 , 36 , 43 , 57 , and 64 ; and doxorubicin 30 mg / m per day intravenous in 24 h on days 8 , 9 , 36 , 37 , 57 , and 58 ) followed by surgical removal of all remaining tumour lesions if feasible ( including liver transplantation and metastasectomy , if needed )  . 
patients whose tumour remained unresectable received additional preoperative chemotherapy ( cycle b : doxorubicin 25 mg / m per day in 24 h on days 13 and 2224 , and carboplatin area under the curve [ auc ] 106 mg / ml per min per day intravenous in 1 h on days 1 and 22 ) before surgery was attempted . 
with a median follow - up of 52 months , 3 - year event - free survival was 76% ( 95% ci 6587 ) and 3 - year overall survival was 83% ( 7393 )  . 
60 ( 97% ) patients had grade 34 haematological toxicity ( anaemia , neutropenia , or thrombocytopenia ) and 44 ( 71% ) had at least one episode of febrile neutropenia . 
other main grade 3 or 4 toxicities were documented infections ( 17 patients , 27% ) , anorexia ( 22 , 35% ) , and mucositis ( seven , 11% )  . 
18 serious adverse events ( including two deaths ) re ecting the observed side - e ects were reported in the trial ( the most common was ototoxicity in ve patients )  . interpretation the siopel - 4 treatment regimen is feasible and e cacious for complete remission at the end of treatment for patients with high - risk hepatoblastoma . funding cancer research uk and cancer research switzerland / oncosuisse . introduction despite important progress in the cure of children with localised hepatoblastoma , the prognosis of patients with metastatic disease remains poor , with 5 - year event - free survival of 2128% and 5 - year overall survival of 2757%.114 only the most recently published study of the international childhood liver tumours strategy group ( siopel - 3 ) , 15 which used intensive multiagent chemotherapy and aggressive surgery , managed to achieve a better outcome for these children ( 3 - year eventfree survival 56% , 3 - year overall survival 62% )  . 
to further improve the number of children cured with high risk , in particular metastatic hepatoblastoma , new and therapeutic approaches are needed that can increase treatment e cacy without excessive toxicity . data from earlier studies suggest that cisplatin is the key chemotherapeutic drug in the treatment of hepatoblastoma , but its optimum schedule and dose in this setting is not yet established . 
 according to these results , high risk was de ned as involving all four hepatic sections ( pretumour treatment extent of disease [ pretext ] - iv23 , 24 ) , or presence of distant metastases , or tumour extension into the vena cava or all three hepatic veins , or into the main or both branches of the portal vein , or extrahepatic intraabdominal disease , or serum fetoprotein ( afp ) less than 100 g / l at diagnosis , or tumour rupture . 
tumour extension was assessed by pretreatment imaging ( ultrasound , ct , and mri ) according to the pretext system.23 , 24 for the purposes of eligibility for this trial , pulmonary lesions were judged to be metastases if there was one nodule more than 10 mm or several nodules with at least one more than 5 mbiopsy and histological evaluation of the primary tumour was mandatory for all children . chemotherapy was given as procedures treatment consisted of three cycles of preoperative chemotherapy ( cycles a1a3 ) followed by surgical removal of all remaining tumour lesions if feasible ( including liver transplantation and metastasectomy if needed ) followed by postoperative chemotherapy ( cycle c )  . 
for infants and children with bodyweight less than 10 kg and in case of delay in chemotherapy because of toxicity , dose reduction was recommended by the protocol ( appendix )  . 
to assist optimum treatment decisions by the treating centres , the protocol provided detailed guidelines tumour assessment and surgery including the issue of di cult or extreme resection , liver transplantation , and metastasectomy ( appendix )  . 
ca * = carboplatin area under the curve ( auc ) 106 mg / ml per min per day intravenous infusion in 1 h ; on days 1 and 22 in cycle b . 
empty circle = assessment of response and resectability . vol 14 august 2013 articles which is a good surrogate for event - free survival and was thought to be an adequate outcome measure for this trial . 
tumour response and resectability were assessed by imaging and serum afp concentration after each chemotherapy cycle according to the following criteria : complete response , 67 patients enrolled 62 eligible 5 misdiagnosis 1 primary surgery 60 complete or partial response after preoperative chemotherapy 1 stable disease after preoperative chemotherapy , withdrawn before surgery * 2 death before surgery 1 withdrawn before surgery 1 no documentation of surgery 1 unresectable disease 2 surgical death 6 liver resection in the presence of residual lung lesions ( small lesions ) , no metastasectomy 1 liver resection in the presence of residual lung lesions ( unresectable ) , no metastasectomy 46 complete surgical resection of all remaining lesions after preoperative chemotherapy 4 no complete remission 49 in complete remission at the end of treatment figure 2 : enrolment , treatment , and outcome of patients * withdrawn after second preoperative chemotherapy cycle ( a2 ) because of grade 3 ototoxicity . 
unresectable because of multiple lung lesions , no surgery attempted . de ned as no evidence of disease and normal afp ( for age ) ; partial response , de ned as any tumour volume shrinkage and a decrease of afp greater than 1 log below the original measurement ; stable disease , de ned as no tumour volume change and no change or less than 1 log fall of afp ; progressive disease , de ned as unequivocal increase of tumour size in one or more dimensions or any unequivocal increase of the afp concentration , or both ; complete surgical resection , de ned as total macroscopic removal of all tumour lesions ; and complete remission , de ned as no evidence of tumour on imaging and normal ( for age ) serum afp . 
toxicity was graded according to the national cancer institute common toxicity criteria for adverse events version 3.0 and the brock grading for ototoxicity.25 the trial was monitored for excessive toxicity by regular evaluation of severe adverse event reports and toxicity data . 
 these data were reported to an independent data monitoring committee that assessed and judged observed toxicity at least once a year and made recommendations for amendments or closing of the study if necessary . 
 statistical analysis we used simons two - stage optimal design with a probability of complete remission in 60% of patients or less ( from the siopel - 3hr study ) as the null hypothesis and a probability of 80% of patients or higher as the alternative hypothesis . 
the sample size was n1 = 19 for stage 1 and n2 = 34 for stage 2 , resulting in a maximum sample size of 53 if the trial was not stopped after stage 1 analysis . 
the stage 1 evaluation was done on the rst 19 treated patients in february , 2007 , and concluded that early stopping criteria were not met and the trial could be continued . 
a stopping rule for safety was devised on the basis of the number of patients in whom possible treatment - related severe adverse events developed , including death and grade 4 toxic e ects . 
the corresponding author had full access to all data in the study and had nal responsibility for the decision to submit for publication . 836 vol 14 august 2013 articles results between jan 1 , 2005 , and aug 31 , 2009 , 67 patients were enrolled in the trial from 18 countries worldwide ( gure 2 )  . 
no children were excluded because of abnormal cardiac , renal , or liver function or pre - existing hearing loss . table 1 shows the number of chemotherapy cycles given in total and per patient . 
the cumulative delay in the administration of the second and third cycles of preoperative therapy ( a2 and a3 ) because of toxicity ranged from 4 to 63 days ( median 7 days , mean 10 days ) ; reasons for early start of the next cycle of chemotherapy in some patients were good haematological recovery and clinical condition . 
two patients who withdrew from the study received some non - protocol chemotherapy after withdrawal . 60 ( 98% , 95% ci 91100 ) of 61 evaluable patients ( one child underwent primary hepatectomy ) had a partial response to preoperative chemotherapy . 
of the 39 patients with initial lung metastases , a complete response of the lung lesions was achieved in 20 patients and partial response in 18 patients , with preoperative chemotherapy alone ( 97% patients responded )  . 
in one patient no evaluation of the lung lesions was done . in 53 ( 85% ) of the 62 patients , complete macroscopic resection of the primary tumour was achieved with partial hepatectomy ( n = 37 ) or liver transplantation ( n = 16 )  . 
in ve patients , no surgery was attempted because of unresectable disease ( one patient ) , early death ( two ) , or withdrawal before surgery ( two )  . 
 in seven patients with residual lung lesions after chemotherapy , the liver tumour was resected but no metastasectomy was done ( gure 2 )  . 16 patients were transplanted , eight with pretext - iv , ve with pretext - iii , and three with pretext - ii tumour . 
none of these seven patients had a ( pulmonary ) relapse . given according of the 46 patients with complete resection of all tumour lesions , one developed recurrent lung lesions before the end of treatment . 
 conversely , six patients with small residual pulmonary lesions after liver surgery who did not undergo metastasectomy achieved complete remission with postsurgical chemotherapy total 49 ( 79% , 95% ci 6788 ) of 62 patients were in complete remission at the end of therapy , including the one who underwent primary hepatectomy , close to the prespeci ed goal of 80% . 
one patient died of postoperative complications , in one no reported toxicity in cycles a1a3 number of patients with reported toxicity in cycle b number of patients with reported toxicity in cycle c number of patients number of cycles ( continued from previous page ) ( one , fungal infection in profound neutropenia ) , surgical compli cations ( two , one intra operative bleeding and shock ; one , lethal postoperative wound infection ) , or tumour bleeding ( one , spontaneous intratumour bleeding with irreversible haemorrhagic shock before the second cycle of chemo therapy )  . 
the kaplan - meier estimate of 3 - year eventfree survival was 76% ( 95% ci 6587 ) and of overall survival was 83% ( 95% ci 7393 ) for the whole group ( gure 3 )  . 
 the relapses occurred 548 months after the end of treatment at the following sites : locoregional ( three ) , lungs ( one ) , unknown ( one )  . 
two of the ve patients died of their cancer , the other three had a second complete remission . 19 of the 20 patients with metastatic disease with complete response in the lungs were in complete remission at the end of treatment . 
in two of the 18 children the lung lesions remained unresectable ; in one the liver tumour was resected but no metastasectomy was done , and in the other no surgery was attempted . 
of the remaining ten patients , six did not achieve complete remission because of residual pulmonary disease : in one patient lung lesions disappeared with preoperative chemotherapy but recurred after liver surgery ; in two patients pulmonary lesions were diminished , but remained unresectable ; and in three patients no visible tumour was left , but afp remained slightly raised at the end of treatment . 
3 - year eventfree survival was 77% ( 95% ci 6390 ) and 3 - year overall survival was 79% ( 95% ci 6692 ) for the 39 patients with metastasis . 
in an exploratory analysis , 27 ( 78% ) of 37 patients with metastatic disease and afp higher than 100 g / l had achieved continuous complete remission at the end of therapy . 
 in 11 of the 16 patients with initial pretext - iv tumour , chemotherapy led to downstaging of the liver mass to category iii in six , category ii in four , and category i in one patient as assessed preoperatively . 
cycles a1a3 were given to 62 patients ( in total 182 cycles ) , additional preoperative chemotherapy ( cycle b ) to 13 patients , and postoperative chemotherapy ( cycle c ) to 37 patients . 
 table 2 : short - term toxicity in the siopel - 4 trial vol 14 august 2013 articles surgery was attempted because of unresectable lung disease , and two patients were withdrawn before surgery . 
3 - year event - free survival was 73% ( 95% ci 5196 ) and overall survival was 80% ( 95% ci 60100 ) for the 16 patients with pretext - iv tumours , including the seven with lung metastases . 
of the nine patients who did not have metastatic disease at diagnosis , eight ( 89% ) had a complete resection and eight ( 89% ) achieved complete remission . 60 ( 97% ) patients had grade 34 haematological toxicity after at least one of the cycles . 
the highest frequency of neutropenia and thrombocytopenia was after additional preoperative chemotherapy ( cycle b ; 12 [ 92% ] and 11 [ 85% ] , respectively ) , which was given only to 13 patients . 
one patient died of fungal infection in profound neutropenia . of the 61 children who received at least two preoperative cycles , ototoxicity was evaluated and documented in 54 , with at least two measurements , both done after at least two cycles or during follow - up . 
in seven patients ( 10% ) ototoxicity was not su ciently documented . panel : research in context systematic review we searched pubmed on jan 20 , 2004 , for clinical trials published in english before jan 1 , 2004 , using the keywords hepatoblastoma , metastatic , or high risk , or locally advanced or unresectable hepatoblastoma and identi ed 11 articles that provided prospective survival data for at least one of these patient groups . 
four more relevant articles were identi ed , one of which showed improved resultscompared with the previous datain high - risk hepatoblastoma ( 3 year event - free survival 65% , overall survival 69% ; 56% and 62% for the metastatic subgroup )  . 
systematic search for publications on the use of ( high ) dose - dense or weekly cisplatin in childhood cancer retrieved no articles . interpretation our study used a novel and unique design of dose - dense ( weekly ) cisplatin in the treatment of patients with high - risk hepatoblastoma and provides rm evidence for the feasibility and e cacy of this approach . 
the reported outcome , in particular for those with metastatic disease , is higher than ever before achieved for children with high - risk hepatoblastoma and denotes an important improvement in the prognosis of these children . 
although further evaluation of the long - term toxicity is needed , the presented treatment strategy could be now regarded as rst choice in the treatment of patients with metastatic or very high - risk hepatoblastoma . 18 serious adverse events , including two deaths , were reported ( appendix )  . 
on the basis of the observed toxicity , the independent data monitoring committee did not recommend any changes or amendment to the protocol during the trial . discussion the siopel - 4 trial addressed the question of whether increased dose density of cisplatin in the preoperative phase can improve the prognosis of children with highrisk , in particular metastatic , hepatoblastoma ( panel )  . 
the proportion of patients with complete remission and the 3 - year eventfree and overall survival compare favourably with results of previous studies and suggest an improvement in the prognosis of children with high - risk hepatoblastoma . in view of the rarity of high - risk hepatoblastoma , a randomised controlled study to directly prove the superiority of the study treatment was not deemed feasible within an acceptable timeframe . 
instead , a single - arm study was designed with complete remission at the end of trial treatment as the primary endpoint , which is an objective and relevant outcome measure and allows analysis shortly after the study is closed . 
siopel - 4 aimed to achieve an improvement in proportion of patients with complete remission of 20% or more ( from 60% [ in siopel - 3hr ] to 80% ) , which is regarded as a clinically relevant and signi cant improvement . since tumour - free status at the end of treatment is a prerequisite for cure and the relapse rate in high - risk hepatoblastoma is low , complete remission is thought to be a good surrogate for overall and event - free survival . 
 additionally , to produce robust survival data that can be adequately compared with previously published results , patients were followed up for a median of 52 months ( table 3 )  . 
on the basis of these data the current follow - up seems largely su cient for a good estimate of the long - term e cacy of the regimen and gives a good basis for comparison with other studies . although we acknowledge that comparison with historical controls does not provide the highest level of evidence , we are convinced that in this context the use of historical controls is the best available option to indicate improvement . 
we believe that the high similarities in patient populations , inclusion and exclusion criteria , and trial design , conduct , and analysis make the comparison with previous siopel studies appropriate . 840 vol 14 august 2013 articles the most important progress has been achieved in the cure of children with metastases . 
the complete response in the lungs achieved in this way appears stable , since 19 ( 95% ) of the 20 patients remained in continuous complete remission , including the six who underwent liver transplantation . 
25 of the 39 patients had complete remission without pulmonary surgery and two additional patients had no viable tumour cells in their metastasectomy specimens , emphasising the e cacy of the applied chemotherapy . 
additionally , two of the six children who did not have complete remission because of pulmonary disease had low initial afp and scud histology , both features known as bad prognostic factors.26 , 27 the outcome of patients with metastatic disease achieved in this study appears to be better than the results of all previously published studies , including siopel3hr , and denotes a major improvement in the cure of these children ( table 3 )  . the excellent response of lung metastases to preoperative chemotherapy in this study is in line with the promising results of the previous siopel study ( 3hr ) , which seem to be further improved by the highly e ective siopel - 4 regimen . 
 surgery remains important in patients whose lung lesions are not cleared by chemotherapy alone . the presented results for patients with pretext - iv tumour con rm the fairly good prognosis of this subgroup and might suggest a slight improvement in overall survival compared with previous siopel studies ( table 3 )  . 
 because of an excellent response to chemotherapy , the tumour extent decreased signi cantly in most patients and partial hepatectomy became feasible in four children who otherwise would have needed liver transplantation . 
this study con rms that transplantation is a safe and potentially curative option for patients whose primary tumour remains unresectable with partial hepatectomy.2830 these results also emphasise that the presence of lung metastases at diagnosis is not a contraindication to liver transplantation , provided that e ective preoperative chemotherapy is given , the lung lesions respond to chemotherapy , and are completely cleared before transplantation by chemotherapy and metastasectomy ( if needed )  . we believe that the most important explanation for the improved results is the increased preoperative dose density of cisplatin used in this treatment regimen ( 475 mg / m per week vs 229 mg / m per week in siopel - 3hr ) , in the context of the previously established multidisciplinary approach . 
our results encourage exploration of the role of dose - dense cisplatin - based regimens in the treatment of other paediatric tumours . as expected , the main toxicity was haematological , leading to profound neutropenia in most children . 
however , because of the young age of most patients , follow - up audiology investigations will be needed to establish the incidence and severity of long - term ototoxicity after this regimen . in conclusion , the siopel - 4 treatment regimen with dose - dense administration of cisplatin and radical surgery is a feasible and e ective treatment and improves the prognosis of children with high - risk hepatoblastoma , in particular of those with metastatic disease . contributors jz , lb , pb , dr , rm , az , mch , j - bo , da , ms , pc , and gp were involved in the design and concept of the study and in writing of the protocol . 
all authors have participated in drafting and nalising the report and have approved the nal draft . con icts of interest we declare that we have no con icts of interest . acknowledgments this study was partly supported by cancer research uk and cancer research switzerland / oncosuisse grants to the siopel group . 
we thank the participating siopel members and institutions ( appendix )  . corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
based on the sample size calculation , we planned to analyse overall survival when 190 deaths occurred ; this target has now been reached , after a median 10 years of follow - up . methods rt01 was a phase 3 , open - label , international , randomised controlled trial enrolling men with histologically con rmed t1bt3a , n0 , m0 prostate cancer with prostate speci c antigen of less than 50 ng / ml . 
patients were randomly assigned centrally in a 1 : 1 ratio , using a computer - based minimisation algorithm stratifying by risk of seminal vesicle invasion and centre to either the control group ( 64 gy in 32 fractions , the standard dose at the time the trial was designed ) or the escalated - dose group ( 74 gy in 37 fractions )  . 
this trial is registered , number isrctn47772397 . findings between jan 7 , 1998 , and dec 20 , 2001 , 862 men were registered and 843 subsequently randomly assigned : 422 to the escalated - dose group and 421 to the control group . 
biochemical progression or progressive disease occurred in 391 patients ( 221 [ 57% ] in the control group and 170 [ 43% ] in the escalated - dose group )  . 
at 10 years , biochemical progression - free survival was 43% ( 95% ci 3848 ) in the control group and 55% ( 5061 ) in the escalated - dose group ( hr 069 , 95% ci 056084 ; p = 00003 )  . interpretation at a median follow - up of 10 years , escalated - dose conformal radiotherapy with neoadjuvant androgen deprivation therapy showed an advantage in biochemical progression - free survival , but this advantage did not translate into an improvement in overall survival . 
open access article distributed under the terms of cc by . introduction external beam radiotherapy is one of the standard curative options for men with localised prostate cancer and is particularly appropriate for men with intermediate - risk or high - risk disease.1 , 2 improved radiotherapy techniques , such as conformal radiotherapy , allow high treatment doses to be given safely3 , 4 and several phase 3 randomised controlled trials of dose escalation have reported improved biochemical progression - free survival.510 the medical research council ( mrc ) rt01 trial is the largest of these trials to have reported results , and since its initial report of results dose - escalated conformal radiotherapy has been the standard of care in the uk since 2008.1 the trial mandated the use of short - course neoadjuvant androgen deprivation therapy ( adt ) ; neoadjuvant adt has since been shown to improve overall and cancer - speci c survival in patients with advanced localised disease.1114 overall the aim of the rt01 trial was to assess the e ect of survival , biochemical dose - escalation progression - free survival , and toxicity , by comparing doses of 74 gy and 64 gy delivered by use of conformal radiotherapy techniques . 
64 gy in 32 fractions was chosen as the radiotherapy schedule for the control group in our randomised trial , because that was the standard 464 vol 15 april 2014 articles 862 assessed for eligibility 19 excluded 8 intercurrent illness 6 patients preference 3 hospital error 2 disease progression 843 randomised 4 received more than planned dose 421 patients assigned to control group ( 64 gy in 32 fractions ) 2 had less than planned dose 4 did not receive radiotherapy 1 dose information not available 410 received planned dose 422 patients assigned to escalated - dose group ( 74 gy in 37 fractions ) 14 received less than planned dose 7 did not receive radiotherapy 401 received planned dose 421 patients analysed 422 patients analysed figure 1 : trial pro le age ( years ) median ( range ) t stage t1b / t1c t2a / t2b t3a / t3b not known gleason score * 6 or lower 8 or higher not known median ( iqr ) mean ( sd ) moderate nccn risk group * high intermediate unobtainable control group ( n = 421 ) escalated - dose group ( n = 422 ) 67 ( 4680 ) 67 ( 4880 ) 106 ( 26% ) 236 ( 57% ) 71 ( 17% ) 103 ( 25% ) 239 ( 57% ) 76 ( 18% ) 261 ( 62% ) 105 ( 25% ) 52 ( 12% ) 249 ( 59% ) 117 ( 28% ) 54 ( 13% ) 128 ( 84200 ) 128 ( 78202 ) 156 ( 100 ) 152 ( 96 ) 137 ( 33% ) 284 ( 67% ) 138 ( 33% ) 284 ( 67% ) 79 ( 19% ) 159 ( 38% ) 178 ( 43% ) 81 ( 19% ) 152 ( 36% ) 184 ( 44% ) prehormone psa ( ng / ml ) risk group for involvement of seminal vesicles data are n ( % ) unless otherwise speci ed . 
 * if gleason score was missing , who di erentiation was used in the following way : well , moderate , or poor di erentiation is classi ed as gleason score of 6 , 7 , or 8 , respectively . 
we initially reported ndings of the trial with a 5 - year median followup and now update these results with a median follow - up of 10 years , because the target number of deaths for analysis of overall survival has been reached . 
treatmentrelated side - e ects have been reported previously.7 , 15 , 16 methods study design and participants rt01 was a phase 3 , open - label , international , randomised controlled trial comparing dose - escalated conformal radiotherapy with control - dose conformal radiotherapy . 
it was preceded by a pilot study at the royal marsden hospital.5 patients were registered , initiated on neoadjuvant adt , and then randomly assigned to receive either control or escalated radiotherapy using conformal radiotherapy techniques . 
men 18 years or older with histologically con rmed t1bt3a , n0 , m0 prostate cancer and prostate - speci c antigen ( psa ) of less than 50 ng per ml , with no contraindications for radical radiotherapy were included in the trial . 
this study was done in compliance with the declaration of helsinki , and the protocol was approved by the appropriate research ethics committees . randomisation and masking consenting patients were randomly assigned in a 1 : 1 ratio to control or escalated - dose conformal radiotherapy centrally at the mrc clinical trials unit ( ctu ) using a computer - based minimisation algorithm , stratifying for risk of seminal vesicle invasion and centre . 
the random allocation list was created by the mrc ctu . injections of procedures as reported previously , androgen deprivation was achieved using luteinising - hormonereleasing hormone agonists every 4 weeks and was accompanied by antiandrogen therapy to prevent are events.7 neoadjuvant adt was given for 36 months before commencement of conformal radiotherapy and continued until the end of conformal radiotherapy . men were randomised to receive either a control - dose schedule ( 64 gy in 32 fractions ; control group ) schedule , or an escalated - dose schedule ( 74 gy in 37 fractions )  . 
all radiotherapy treatments used three - dimensional conformal techniques as previously described.7 , 11 , 17 the radiotherapy phase 1 target volume included the prostate and all or part of the seminal vesicles , depending on the vol 15 april 2014 articles risk of seminal vesicle invasion.18 all patients were treated to a dose of 64 gy in 32 fractions over 65 weeks using a standard threeeld plan ( anterior eld and left and right lateral or posterior oblique elds ) with a 10 cm marg patients randomised to the escalated - dose group had a phase 2 boost to the prostate alone using a sixeld technique ( left and right anterior oblique , left and right posterior oblique , and left and right lateral elds ) with no margin added . 
veri cation was with daily and then weekly port lms and images . men were followed - up throughout radiotherapy at 6 monthly intervals up to 2 years , and annually thereafter . 
 acute and late treatment - related side - e ects were collected using radiation therapy oncology group19 and late e ects of normal tissues - subjective objective management analytic scales20 and timed from the start of radiotherapy . 
the design , objectives , eligibility criteria for patients , treatment methods , and statistical considerations are detailed elsewhere.7 , 17 outcomes the coprimary outcome measures were overall survival and biochemical progression - free survival . 
overall 020 015 010 005 005 010 015 020 020 015 010 005 005 010 015 020 control group by kaplan - meier control group by exible parametric model escalated - dose group by kaplan - meier escalated - dose group by exible parametric model number at risk control group escalated - dose group 95% ci overall survival by exible parametric model control group by kaplan - meier control group by exible parametric model escalated - dose group by kaplan - meier escalated - dose group by exible parametric model time from randomisation ( years ) number at risk control group escalated - dose group 95% ci biochemical progression - free survival by exible parametric model time from randomisation ( years ) figure 2 : primary analysis of overall survival and biochemical progression - free survival ( a ) overall survival , predicted from kaplan - meier function and exible parametric model . 
 ( d ) absolute di erence in biochemical progression - free survival , from exible parametric model . 466 vol 15 april 2014 articles hr ( 95% ci ) 096 ( 054170 ) 101 ( 076134 ) 077 ( 032187 ) 113 ( 073174 ) 095 ( 068134 ) 080 ( 054118 ) 066 ( 052083 ) 061 ( 034109 ) 084 ( 059119 ) 060 ( 046079 ) with cox models , adjusted for seminal vesicle risk group.18 we applied the restricted mean survival time method to overall survival and biochemical progressionfree survival , as an additional method of estimating di erence between the treatments , with the restriction time being 10 years . 
 all comparisons are expressed relative to the control group ; therefore , an hr of less than 10 indicates a decreased risk in the escalated - dose group . we did a competing - risk analysis for prostate cancer death because the number of deaths from causes other than prostate cancer exceeded the prespeci ed level of 20% . 
for this analysis , time to prostate cancer death is presented with cumulative incidence function rather than survival function ; sub - hr is presented with 95% ci and p value . 
cause - speci c hrs are presented for both prostate cancer and non - prostate - cancer deaths . we did pre - planned , exploratory subgroup analyses to examine consistency of e ect across seminal vesicle risk group ( low vs moderate ) and national comprehensive cancer network ( nccn ) risk group ( low vs intermediate vs high ) .2 this analysis uses tests for heterogeneity of interaction or trend when appropriate , and examines overall survival and biochemical progression - free survival . 
this trial is registered , number isrctn47772397 . low risk intermediate risk test for heterogeneity : p = 089 low risk intermediate risk high risk test for heterogeneity : p = 070 low - risk intermediate - risk test for heterogeneity : p = 042 low risk intermediate risk high risk test for heterogeneity : p = 032 survival was de ned as time from randomisation to death from any cause or censoring at date of last contact . 
 biochemical progression - free survival was de ned as time from randomisation to biochemical failure , death from prostate cancer , or development of local , nodal , or metastatic disease , whichever occurred rst . additional outcome measures were biochemical failure ( an increase in psa concentration to 50% above nadir and above 2 ng / ml 6 months or more after the start of radiotherapy ) ; progression - free survival ( excluding psa failure ) ; initiation of long - term salvage adt ; development of metastases ; death from prostate cancer ; and metastasesfree survival ( time to development of any metastases or death from prostate cancer )  . 
cause of death was reviewed by pairs of clinicians from a panel of ve individuals who were masked to treatment allocation . the original protocol speci ed ve primary outcome measures survival ( biochemical progression - free [ named as biochemical control in the protocol , local progression , metastases free freedom from survival , overall survival , and late toxicity ) ; with sample size calculations included for local control and overall survival . 
during the course of the trial , the trial management group , independent data monitoring committee , and trial steering committee agreed from external evidence that biochemical progression - free survival was a more important outcome measure than local control . 
all outcome measures are reported . statistical analysis we estimated that inclusion of about 800 patients would meet the targets for the numbers of patients in the subgroups at low - risk and intermediate - risk of seminal vesicle involvement.17 we assumed that survival at 5 years would be 50% in patients in the control group , and the trial aimed to achieve a 15% increase in survival at 5 years in the escalated - dose group . 
with 90% power and a 5% two - sided signi cance level , we established that about 194 deaths were needed for this analysis of overall survival . we did all analyses on an intention - to - treat basis , with patients analysed according to allocated treatment group . 
 all analysed outcome measures are presented in this report . we used standard survival analysis methods to investigate time from randomisation to the rst reported event for each outcome measure , except for time to death from prostate cancer . 
hazard ratios ( hr ) were estimated favours escalated - dose favours control figure 3 : subgroup analyses of overall survival and biochemical progression - free survival ( a ) overall survival and risk of seminal vesicle involvement . 
 results between jan 7 , 1998 , and dec 20 , 2001 , 862 men were registered and 843 subsequently randomised : 422 to the escalated - dose group and 421 to the control group ( gure 1 )  . table 1 shows characteristics of the patients at baseline ; the groups were balanced . 
209 ( 25% ) of 831 patients had t1 stage cancers , 475 ( 57% ) had t2 stage , and 147 ( 18% ) had t3 cancers ; t stage was unavailable for 12 patients . 
 analyses of biopsy specimens were reported by local histopathologists , and showed gleason scores of 6 or lower in 510 ( 61% ) of the 838 enrolled patients , a score of 7 in 222 ( 26% ) of patients , and a score 8 of or higher in 13% ( 106 ) of patients ; gleason score was not available for ve patients . 
160 ( 19% ) of 833 patients had low - risk disease according to nccn criteria , 311 ( 37% ) had intermediate - risk disease , and 362 ( 43% ) had high - risk disease ; unavailability of t - stage or histological grading precluded ascertainment of risk group in ten patients . 
overall , 117 patients were alive at 11 years and 30 at 12 years . as of aug 2 , 2011 , 236 deaths had been reported , 118 in each group , triggering the overall survival analysis . 
there was no di erence in 10 year overall survival between groups : 10 year overall survival was 71% ( 95% ci 6675 ) in both groups ( hr 099 , 95% ci 077128 , p = 096 , gure 2 )  . 
mean overall survival , using the exible parametric model and when restricted to 10 years , was 930 years ( 95% ci 908952 ) for the control group and 928 years ( 906950 ) for the escalated - dose group . 
there was no evidence of a di erence between restricted mean survival : 002 years ( 95% ci 034 to 029 ; p = 088 )  . for patients who had not yet reported a biochemical progression event , adherence to psa testing was 90% complete at 5 years and 76% complete at 10 years . 
 biochemical progression - free survival was better in the escalated - dose group , being 43% at 10 years ( 95% ci 3848 ) in the control group and 55% ( 5061 ) in the escalated - dose group ( hr 069 , 95% ci 056084 ; p = 00003 , gure 2 )  . 
mean biochemical progressionfree survival , when time of analysis was restricted to 10 years , was 733 years ( 95% ci 687780 ) in the control group and 801 years ( 760840 ) in the escalated - dose group , leading to an improvement in restricted mean survival of 069 years with escalateddose radiotherapy ( 95% ci 008130 ; p = 003 )  . 
||cause - speci c hr . table 2 : outcome measures 468 vol 15 april 2014 articles 020 015 010 005 control group escalated - dose group number at risk control group escalated - dose group control groups , pc death control groups , non - pc death escalated - dose groups , pc death escalated - dose groups , non - pc death number at risk control group escalated - dose group time from randomisation ( years ) time from randomisation ( years ) figure 4 : additional outcome measures ( a ) progression - free survival , kaplan - meier plot . 
progression - free survival , biochemical failure , and delayed commencement of salvage adt were all signi cantly better the escalated - dose group compared to the control group ( table 2 , gure 4 )  . 
of patients who had biochemical progression , a lower proportion ( 67 [ 30% ] of 221 patients ) in the control group had metastases , or died from prostate cancer compared to the escalated - dose group ( 65 [ 38% ] of 170 patients )  . 
notably , of the 391 patients who developed psa failure or progressive disease , only 220 ( 56% ) reported commencing long - term salvage adt ( 123 in the control group , 97 in the escalated - dose group )  . 
of 268 men who had clinical evidence of progressive disease , 132 ( 49% ) developed metastases or died from prostate cancer ( 67 in the control group , 65 in the escalated - dose group )  . according to the central , blinded review of deaths , 91 of 236 ( 39% ) deaths were from prostate cancer ( 44 in the control group , 47 in the escalated - dose group ) , 132 ( 56% ) were from other causes ( 68 in the control group vs 64 in the escalated - dose group ) , and for 13 ( 6% ) patients there were insu cient data for the reviewers to assign cause of death ( six control vs seven escalated dose ) : for ten , the investigator de ned causality as not prostate cancer ( which was accepted ) , and for the other three , no evidence of recurrent prostate cancer had been recorded . 
 we did a competing - risk analysis for prostate cancer death because 145 ( 61% ) of 236 deaths were from causes other the than prostate cancer , which exceeded prespeci ed level of 20% . 
the sub - hr for the comparison of cumulative incidences is 107 ( 95% ci 071161 ; p = 075 ) in favour of the control group with a cause - speci c hr for prostate cancer deaths of 106 ( 95% ci 070160 ; p = 079 ) and for other deaths of 096 ( 069132 ; p = 078 )  . nccn risk group was available for 90 of the 91 patients who died from prostate cancer . 
only one of 160 ( 1% ) men with low - risk disease died from prostate cancer compared with 21 of 311 ( 7% ) with intermediate - risk disease and 68 of 362 ( 19% ) with high - risk disease . 
as a proportion of total deaths , for lowrisk disease , one ( control group ) of 20 ( 5% ) were from prostate cancer compared with 21 ( nine control vs 12 escalated - dose ) of 81 ( 26% ) for intermediate - risk disease and 68 ( 34 control vs 34 escalated - dose ) of 133 ( 51% ) for high - risk disease . 
we identi ed no evidence of heterogeneity of e ect of dose escalation between these subgroups . discussion the previously reported advantage of escalated - dose conformal radiotherapy treatment compared to controldose conformal radiotherapy in biochemical progressionfree survival after a median follow - up of about 5 years was maintained in the present study with more mature data and a median follow - up of 10 years . 
this improvement in biochemical control of disease has not translated into an advantage for metastases - free survival , prostate - cancer - speci c survival , or overall survival . 
we identi ed no evidence of heterogeneity of treatment e ect between low , intermediate , and highrisk groups . we recorded a signi cant delay in the reported time to initiation of long - term , salvage adt in the escalated - dose group ; using the hr there was an absolute improvement of 7% ( 95% ci 012 ) at 10 years from 45% . 
this advantage of reducing or delaying the initiation of long - term adt , which is associated with well - documented andropausal side - e ects , 22 must be balanced against the known small increase in bowel side - e ects from the ve extra treatments in the escalated - dose group , which we and others have reported.5 , 6 , 8 , 10 , 16 , 23 why has the di erence in psa control not translated into an advantage for metastasis - free survival and prostate - cancer - speci c survival ? several factors might be involved . 
first , it is likely that there were more indolent recurrences con ned to the prostate in the control group : a lower proportion of patients in the control group had metastases or died from prostate cancer than those in the escalated - dose group . 
moreover , of patients who developed psa failure or progressive disease , only 56% reported commencing long - term salvage adt , and only 49% of patients who had clinical evidence of progressive disease developed metastases or died from prostate cancer . 
we now know that some men with indolent local disease do not necessarily need treatment , for example men with low - risk disease or older than 65 years do not bene t from radical prostatectomy , 24 , 25 and active surveillance has become a standard of care for patients with a favourable outlook.26 second , there is a long time from commencement of salvage adt to death . 
in an international trial of intermittent or continuous salvage androgen suppression , 22 time from salvage adt to death was estimated at about 9 years , but with only about 17% of patients dying of prostate cancer after 7 years . 
in the control group of rt01 , 25% of patients had a biochemical progression - free survival event by 26 years after randomisation , but it was 57 years from randomisation before 25% of patients had reported initiation of salvage adt ; median times for these outcome measures have not been reached . 
moreover , our results clearly show that nccn risk group was related to the probability of dying from prostate cancer . the lower bound of the 95% ci for overall survival was 077 , and therefore our results cannot rule out some improvement in overall survival . 
 after 14 years of follow - up , the small pilot study ( n = 126 ) which recruited before the start of rt01 suggested an overall survival advantage for the escalated - dose group ( 74 gy ) with hr 059 , but with only 19 prostate cancer deaths the 95% cis were wide ( 023149 ) .5 the phoenix de nition27 our trial was designed in 1997 and launched in 1998 before for biochemical recurrence became established , but our chosen de nition of psa failure with 2 ng / ml has much the same speci city and sensitivity.28 our results are in alignment with reported data from other studies of dose - escalated external beam radiotherapy ( table 3 ) , which have shown absolute advantages in psa failure - free survival of 619% for dose - escalated treatments . even in trials with a high proportion of patients with poor prognostic factors and long follow - up , none have yet reported prostate - cancer - speci c mortality of greater than 15% . 
a meta - analysis with the other randomised trials would provide a larger number of events from patients with high - risk disease to assess the e ect of dose - escalation on death from prostate cancer . our ndings draw attention to two issues for future trials . 
 survival - based outcome measures must remain of paramount importance , but there are implications for recruiting centres , trials units , and funding bodies in collecting long - term data . 
 * freedom from biochemical ( psa ) or clinical failure . table 3 : data from randomised controlled trials of dose - escalated external beam radiotherapy for prostate cancer absolute reduction in psa failure in dose escalated group ( 10 year ) ( 10 year ) ( 10 year ) 19% * ( 8 year ) ( 12 year ) 85% ( 5 year ) ( 10 year ) ( 10 year ) ( ns ) ( 8 year ) about ( 14 year ) ( ns ) outcome data needs to be explored . 
we have previously reported our comparative side - e ect data , which we planned to collect only to 5 years , 7 , 15 , 16 and a limitation of the present report is that no 10 - year patient - reported outcome data are available . by contrast with the dose - escalation trials , phase 3 studies assessing the addition of neoadjuvant adt to radical prostate radiotherapy have shown clear evidence of improved overall survival and cause - speci c survival in meta - analysis.29 , 30 review of additional trial results1114 shows that survival bene ts become apparent about 35 years after randomisation . 
one interpretation is that , in addition to short - course adt having an e ect on local control of disease , 11 6 months of adt also has a direct e ect on eradication of micrometastatic disease . 
 these trials have been in patients given modest doses of radiotherapy by present standards ( equivalent to 70 gy or lower ) but large institutional us series have suggested much the same bene ts of neoadjuvant adt in patients given doses of 7681 gy.31 , 32 either what are the relative merits of dose escalation and combined modality treatment with neoadjuvant adt ? dose escalation leads to excellent local disease control using brachytherapy33 in lower risk disease . 
by use of a biopsy sample obtained 2 years after treatment as a gold radiotherapy external beam panel : research in context systematic review radiotherapy dose is limited by treatment - related side - e ects . 
advancing radiotherapy techniques using conformal radiotherapy had been shown to reduce the occurrence of side - e ects.3 dose - escalation therefore became feasible with the hypothesis that higher radiation doses would lead to improved outcomes.5 , 3739 interpretation as far as we are aware , this study is the largest dose - escalation trial to have reported long - term e cacy results . 
 however , none of these trials have convincingly shown a positive e ect on overall or prostate - cancer - speci c survival after 10 years of follow - up . 
dose escalation improves intermediate disease outcomes and reduces the use of salvage hormonal treatment , but at the cost of a modest increase in treatment - related side - e ects . 
further improvements in radiotherapy techniques have been shown to reduce the e ect of dose - escalation on side - e ects4 , 40 , 41 and should be used to maintain the reported advantages of dose - escalation while minimising treatment sequelae . 
 standard method34 to detect local recurrence , a 3 - month period of neoadjuvant adt given with modest - dose or high - dose radiotherapy reduced positive biopsy ndings from 46% to 10%.35 in a preplanned substudy of the rt01 trial , only six ( 6% ) of 97 men in the escalated - dose group who agreed to have a biopsy 2 years after treatment had positive histology ( unpublished )  . 
the use of neoadjuvant adt , however , must be balanced against the usually short - lasting increase in morbidity from vol 15 april 2014 articles short - term adt.36 clinical trials that are in progress , including eortc study 22991 ( nct00021450 ) , will more completely de ne the role of combined modality treatment and high - dose radiotherapy . and since we designed our trial using conformal radiotherapy methods , technology advances have led to the widespread introduction of intensity - modulated , image - directed , techniques image - guided including the combined use of external beam radiotherapy with high - dose or low - dose rate brachytherapy , which have enabled high - dose treat ment to be given with a reduced prevalence of side - e ects using conventional or hypofractionated schedules ( panel ) .4 , 40 , 41 high - quality treatments are essential to maintain the potential advantages of dose - escalated treatment in improving disease control and avoiding salvage therapy , while maintaining low levels of treatmentrelated side - e ects . in conclusion , we have shown a clear and maintained advantage in biochemical ( psa ) assessment of disease control , which has translated into a modest reduction in salvage adt , but no evidence of a bene t in survivalbased outcome measures with a median follow - up of 10 years . 
all authors were involved in data interpretation , manuscript review , and approval of the nal manuscript . declaration of interests mrs , mkbp , gj , cm are employees of the sponsor at the medical research council , clinical trials unit at ucl , london , uk . 
randomized trial comparing conventional - dose with high - dose conformal radiation therapy in early - stage adenocarcinoma of the prostate : long - term results from proton radiation oncology group / american college of radiology 95 - 09 . 
the early toxicity of escalated versus standard dose conformal radiotherapy with neo - adjuvant androgen suppression for patients with localised prostate cancer : results from the mrc rt01 trial ( isrctn47772397 )  . 
implementing the uk medical research council ( mrc ) rt01 trial ( isrctn 47772397 ) : methods and practicalities of a randomised controlled trial of conformal radiotherapy in men with localised prostate cancer . 
j natl cancer inst monogr 2012 ; 45 : 23441 . 472 vol 15 april 2014 articles 27 roach m 3rd , hanks g , thames h jr , et al . 
is androgen deprivation therapy necessary in all intermediate - risk prostate cancer patients treated in the dose escalation era ? int j radiat oncol biol phys 2013 ; 85 : 69399 . 33 morris wj , keyes m , spadinger i , et al . 
int j radiat oncol biol phys 1998 ; 41 : 491500 . 36 stephens rj , dearnaley dp , cowan r , sydes m , naylor s , fallow eld l . 
 cancer treat rev 2014 ; 40 : 41425 . vol 15 april 2014 preventing prevention : indian politics and public health clash recent move by the largest indian government , in a the countrys independent public health organisation , the public health foundation of india ( phfi ) , has been barred from receiving foreign funding , including donations from the bill & melinda gates foundation . 
the phfi , which helps to support central and local governments by promoting breast cancer awareness campaigns , developing population - based cancer registries , and promoting universal health care , will lose roughly 45% of its funding from foreign investment over concerns regarding alleged lobbying with parliamentarians and media on anti - tobacco messages , and the misuse of funds and bank accounts that were allegedly not disclosed to the home ministry . 
 this suspension is part of a wider move in recent years by the indian government to cancel foreign contribution ( regulation ) act licenses , which regulate the flow of funds from foreign donors , from which some 20 000 indian non - governmental organisations benefit . 
while some have seen these cancellations as part of a wider effort to appease affiliate groups to the government who have accused philanthropic organisations of pushing corporate interests , others believe that the government is trying to promote a wholly nationalistic agenda in a bid to retain power in the 2019 elections . the recent move to cut funds to the phfi comes at a time when public health is a growing concern in india . 
earlier this month , the indian government announced that it will miss its deadline of december 2017 to reduce coal emissions and airborne particulate matter by two - thirds , declaring instead that developed countries should be responsible for tackling global pollution levels . 
although indias per capita emissions are only 159 metric tonnes per year compared with 755 for china and 1639 for the usa , india is still the worlds third - biggest emitter of greenhouse gases in absolute terms , and has notable levels of air pollution , which killed nearly 11 million of its residents in 2015 alone . 
such an open and defiant attitude by the indian government about their failure to meet coal emission targets , and their dismissive attempt to shift the responsibility to other countries , is a careless and harmful attitude to adopt , but an understandable attitude at a time when the us government dismantling its own environmental protection agency and backtracking on former president barack obamas clean power plan . 
by failing to address such chronic causes of illness , the indian government stands to exacerbate the growing pressure the current public health system upon which a large proportion of indias working class and unemployed rely . 
as a result , indias public health - care system has wholly inadequate financial resources to sufficiently train , staff , equip , or sometimes even run , health facilities nationally an infrastructure that is sure to worsen as one of the countrys largest public health organisations loses a substantial portion of their funding from overseas . although aligning public health targets with a political agenda is certainly nothing new , these drastic steps taken by the current government will inevitably affect public health programmes and initiatives . 
cancer is an emerging health problem in india , and already causes 6% of all adult deaths every year , with the number of cancer deaths set to increase to nearly 1 million in 2025 . 
 this means increasing , not reducing , the availability of funds to help to promote public health campaigns that encourage healthy lifestyles , reduce tobacco use , improve cancer registries , and increase the availability of cancer screening . 
it is worrying that at a time when health care in india is most in need , the government has opted to push for a wholly political and nationalistic agenda at the cost of public health , which clearly needs foreign investment to realistically meet the growing burden of non - communicable diseases across the country . 
that the indian government openly makes moves to undermine public health goals is somewhat paradoxical to a vision of india as an emerging social and economic superpower , and will erode the true social and democratic value that improved health holds for the country . 
 the lancet oncology vol 18 june 2017 editorial correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2017 ; 18 : e142 correction to lancet oncol 2017 ; 18 : e81 , e82 , e86 burki tk . 
this correction has been made to the online version as of march 2 , 2017 . published online march 2 , 2017 s1470 - 2045 ( 17 ) 30173 - 0 published online march 2 , 2017 s1470 - 2045 ( 17 ) 30175 - 4 rl , cancer cancer and survivors : childhood adolescent , r , mulder al . 
recommendations kremer skinner for lc , in male gonadotoxicity surveillance young childhood , report adult international late effects from the guideline harmonization group in collaboration with the pancaresurfup consortiu lancet oncol 2017 ; 18 : e7590in this review , the sixth paragraph under the who needs surveillance ? heading should have read there is probably no increased risk after treatment with cyclophosphamide , busulfan or cyclophosphamide or fludarabine and melphalan , hsct conditioning , and ifosfamide , and mechlorethamine , cisplat additionally , the key for figure 2 should have been light orange for moderate recommendation to do and dark orange for weak recommendation do . 
the oe05 trial assessed whether increasing the duration and intensity of neoadjuvant chemotherapy further improved survival compared with the current standard regimen . methods oe05 was an open - label , phase 3 , randomised clinical trial . 
 eligibility criteria included who performance status 0 or 1 , adequate respiratory , cardiac , and liver function , white blood cell count at least 3 10 cells per l , platelet count at least 100 10 platelets per l , and a glomerular filtration rate at least 60 ml / mparticipants were randomly allocated ( 1 : 1 ) using a computerised minimisation program with a random element and stratified by centre and tumour stage , to receive two cycles of cisplatin and fluorouracil ( cf ; two 3 - weekly cycles of cisplatin [ 80 mg / m intravenously on day 1 ] and fluorouracil [ 1 g / m per day intravenously on days 14 ] ) or four cycles of epirubicin , cisplatin , and capecitabine ( ecx ; four 3 - weekly cycles of epirubicin [ 50 mg / m ] and cisplatin [ 60 mg / m ] intravenously on day 1 , and capecitabine [ 1250 mg / m ] daily throughout the four cycles ) before surgery , stratified according to centre and clinical disease stage . 
this trial is registered with the isrctn registry ( number 01852072 ) and clinicaltrials.gov ( nct00041262 ) , and is completed . findings between jan 13 , 2005 , and oct 31 , 2011 , 897 patients were recruited and 451 were assigned to the cf group and 446 to the ecx group . 
no unexpected chemotherapy toxicity was seen , and neutropenia was the most commonly reported event ( grade 3 or 4 neutropenia : 74 [ 17% ] of 446 patients in the cf group vs 101 [ 23% ] of 441 people in the ecx group )  . 
the proportions of patients with postoperative complications ( 224 [ 56% ] of 398 people for whom data were available in the cf group and 233 [ 62% ] of 374 in the ecx group ; p = 0089 ) were similar between the two groups . 
one patient in the ecx group died of suspected treatment - related neutropenic sepsis . interpretation four cycles of neoadjuvant ecx compared with two cycles of cf did not increase survival , and cannot be considered standard of care . 
our study involved a large number of centres and detailed protocol with comprehensive prospective assessment of health - related quality of life in a patient population confined to people with adenocarcinomas of the oesophagus and gastro - oesophageal junction ( siewert types 1 and 2 )  . 
alternative chemotherapy regimens and neoadjuvant chemoradiation are being investigated to improve outcomes for patients with oesophageal carcinoma . funding cancer research uk and medical research council clinical trials unit at university college london . copyright the author ( s )  . 
these meta - analyses showed a significant survival benefit after treatment with neoadjuvant chemotherapy , both overall and for the subset of patients with adenocarcinoma who were considered in this study . 
these meta - analyses were unable to assess the benefits of different neoadjuvant chemotherapy regimens , and we can identify no phase 3 randomised trials that have directly compared different regimens . added value of this study to our knowledge , this is the largest randomised trial investigating whether an alternative neoadjuvant chemotherapy regimen might offer a survival benefit over the standard of two cycles of cisplatin and fluorouracil ( cf )  . 
this trial showed that giving four cycles of epirubicin , cisplatin , and capecitabine ( ecx ) neoadjuvantly might increase the level of tumour regression , but does not lead to any survival benefit . implications of all available evidence for patients with oesophageal adenocarcinoma , two cycles of cf should remain the standard choice of neoadjuvant chemotherapy regimen . 
further research is ongoing into the use of neoadjuvant chemoradiotherapy , but little evidence exists that directly compares it to neoadjuvant chemotherapy . studies were specifically powered to detect any such difference . 
few studies have been done only in patients with oesophageal adenocarcinoma.2124 high - quality data on the effect of neoadjuvant chemotherapy or chemoradiotherapy on health - related quality of life ( hrql ) are scarce ; more information is needed for clinical decision making , where small survival benefits might only be achieved with detrimental effects on many aspects of hrql . the results of the previous medical research council ( mrc ) oe02 randomised clinical trial19 showed a survival advantage at 2 years with neoadjuvant chemotherapy and surgery over surgery alone ( 43% vs 34% ; 9% increase [ 95% ci 314 ] ) , with a hazard ratio ( hr ) of 079 ( 95% ci 067093 ) , so two - cycle cisplatin with fluorouracil was used for the control group in this study . 
the results showed a 5 - year survival of 36% ( 95% ci 3043 ) for perioperative chemotherapy and surgery compared with 23% ( 1729 ) for surgery alone ( overall survival hr 075 , 95% ci 060093 ) .25 because 45% of participants in the magic trial ( 34% of people who had surgery ) did not receive postoperative treatment ( a similar pattern was also seen in the ffcd - fnclcc 9703 trial22 ) , we concluded that further assessment of perioperative chemotherapy would be challenging and increased it was decided neoadjuvant therapy would be the best strategy . 
oral capecitabine is readily available and has been shown to be equivalent to intravenous fluorouracil in colorectal cancer , 26 so we decided to investigate four cycles of neoadjuvant epirubicin , cisplatin , and capecitabine ( ecx ) as the investigational group without postoperative chemotherapy . 
given the results of the magic trial , that increasing the duration of neoadjuvant chemotherapy from two cycles to four cycles and adding anthracycline to the established doublet regimen was considered the most promising strategy for improving outcomes in patients with oesophageal adenocarcinoma in this study . 
participants were of any age with surgically resectable histologically verified adenocarcinoma of the oesophagus ( including siewert types 1 and 2 gastro - oesophageal junction tumours ) stage ct1n1 , ct2n1 , ct3n0 / n1 , or ct4n0 / n1 where invasion was thought to be confined to diaphragm , crura , or mediastinal pleura and surgically resectable ( union for international cancer control [ uicc ] tnm staging28 )  . 
additionally , patients had to meet the following criteria : who performance status 0 or 1 and adequate respiratory and cardiac function ( forced expiratory volume in 1 sec of > 15 l and cardiac ejection fraction of 50% on echocardiography or multigated acquisition scan ) within 4 weeks of randomisation . 
 within 1 week of randomisation , liver function tests needed to be at most 15 - times normal , white blood cell count at least 3 10 cells per l , platelet counts at least 100 10 platelets per l , and the calculated or measured glomerular filtration rate at least 60 ml / min . 1250 vol 18 september 2017 articles assessment of disease stage required a contrastenhanced multislice ct scan from neck to pelvis and endo scopic ultrasonography within 4 weeks of randomisation . 
the final staging of patients ( and siewert classification ) was done on the basis of a multidisciplinary team discussion following endoscopy , endoscopic ultrasonography , ct , and laparoscopy if appropriate . ( radiologically patients were ineligible if investigations indicated blood - borne metastases assessed ) , peritoneal dissemination , local invasion involving the tracheobronchial tree , aorta , pericardium or lung , or abdominal para - aortic lymphadenopathy greater than 1 cm in diameter on ct scan or more than 6 mm in diameter on endoscopic ultrasonography . 
patients were also excluded if they had received any previous treatment for oesophageal cancer , had siewert type 3 cancer , a medical condition that was likely to compromise the proposed trial treatment . 
uncontrolled angina pectoris , myocardial infarction in the 6 months before entry into the trial , heart failure , clinically significant uncontrolled cardiac arrhythmias , or any patient with a clinically significant abnormal ecg , as well as patients with abnormal left ventricular ejection fraction ( lvef ) diagnosed on muga scan or echocardiography , including areas of abnormal contractility , were excluded . 
 patients with positive serology for hiv or hepatitis c , active hepatitis b , or were pregnant were also excluded . participating centres were considered eligible if they had a multidisciplinary team structure , had experience of twophase oesophagectomy with two - field lymphadenectomy ( unproctored surgeons were recommended to have done a minimum of 12 such operations before joining the trial ) , access to multislice ct and endoscopic ultrasonography equipment , and had pathologists who were experienced in reporting oesophageal cancer . the protocol was approved by the south west multicentre research ethics committee ( 04 / 6 / 005 ) and all patients gave written consent for participation in the study . 
the protocol had five amendments during the course of the trial , predominantly for administrative reasons or to add clarity ; amendments did not affect the eligibility or treatment of patients . 
the most recent version of the protocol ( version 6.0 ) is available online . randomisation and masking eligible patients were enrolled by staff at participating centres who then called the randomisation line at the mrc clinical trials unit at ucl ( london , uk )  . 
no masking to treatment allocation was done because of the difference in the number of chemotherapy cycles in the two groups . chemotherapy control group procedures the regimen was two 3 - weekly cycles of cisplatin and fluorouracil . 
cisplatin ( 80 mg / m ) was infused intravenously on day 1 and fluorouracil ( 1 g / m per day ) was administered intravenously on days 14 ( total 4 g / m )  . the investigational chemotherapy was four 3 - weekly cycles of ecx . 
epirubicin ( 50 mg / m ) and cisplatin ( 60 mg / m ) were given intravenously on day 1 and capecitabine ( 1250 mg / m daily ) was given orally continuously over all four cycles ( for a total of 12 weeks )  . protocols for chemotherapy dose modifications were provided for haematological , renal , neurological , and hepatic toxicities , and for palmarplantar erythema , stomatitis , diarrhoea , nausea , and vomiting . 
 centres were allowed to use a minimal access surgery approach after providing evidence that complication rates and lymph node yields were similar to an open surgery approach from at least 20 patients who had had minimal access oesophagectomy . the stomach was the preferred conduit for reconstruction based on the right gastric and right gastroepiploic vessels . 
lymph node clearance in the abdomen was at the origin of the left gastric artery and along the hepatic and splenic arteries , the upper lesser curve , and at the right and left cardiac lymph node stations . 
dissection at the diaphragm was used to minimise a positive radial or circumferential resection margin by inclusion of sufficient crural fibres and a cuff of diaphragm based on endoscopic ultrasonography and intraoperative appearances . 
the extent of proximal lymphadenectomy for the upper paraoesophageal nodes was determined by the extent of division of the oesophagus ( ie , the length of oesophagus remaining after resection )  . reconstruction was recommended above the aortic arch for the right - sided approach and just below it for the left , and preferably within 5 cm of the thoracic inlet . 
trans - hiatal surgery was not permitted . postoperative complications , described as none , present but not life threatening , or life threatening , were for the oe05 clinical trial protocol version 6.0 see research / documents / cancer_ protocols / oe05_protocol_ version_6_23_dec_09.pdf vol 18 september 2017 1251 articles recorded for each patient . 
these complications were reviewed clinically , and assigned to categories . processing of the surgical resection specimens and histopathological assessment of all materials were done according to the recommendations of the royal college of pathologists : 30 r0 , no tumour cells remaining within 1 mm of any resection margin ; r1 , microscopically visible positive margin indicating the presence of tumour cells at or within 1 mm of a longitudinal or radial or circumferential resection margin ; and r2 , macroscopically visible tumour remaining . 
for patients not listed in above , cause of death was reported as sepsis - related multiple organ failure in one patient and oesophageal cancer in the remaining two patients . 
 in terms of both interobserver agreement ( ie , likelihood of two pathologists concluding the same grading by their independent assessments ) and prognostic ability.32 , 33 pathology data were collected from local pathologists at each centre , and used for the primary analyses of all pathology data . 
the hrql protocol prespecified four domains of hrql to be examined in the primary analyses and full details of all scales and items assessed in the questionnaires will be reported subsequently . 
clinical follow - up involved the same schedule with the use of tests to establish recurrent disease at the discretion of individual centres . outcomes the primary outcome measure of the trial was overall survival . 
secondary outcomes were disease - free survival , effects on the primary tumour ( as assessed by mandard trg ) , hrql , and morbidity related to chemotherapy and surgery . 
exploratory outcomes were progression - free survival ( where a progression - free survival event was defined as the first confirmed local or distant recurrence , or death from any cause ) , and an analysis of mandard trg using an amended responder definition . statistical analysis the sample size calculations were based on the primary outcome measure of overall survival . 
on the basis of the oe02 trial results , 19 which showed an absolute survival difference of 8% at 3 years , we thought it unlikely that any greater difference would be seen in this study . 
with a 5% two - sided significance level , this sample would provide 90% power to detect an 8% difference ( or 1252 vol 18 september 2017 articles 80% power to detect a 7% difference ) in 3 - year survival , from 30% in the cf group . 
in 2007 , following a period of lower than expected recruitment , the sample size was reassessed to ensure that an adequately powered study would still be achieved in a given timeframe . 
the updated sample size calculations required 842 patients with 677 events over 6 years with a minimum follow - up of 2 years before analysis , to provide at least 82% power to detect an 8% difference ( and 70% to detect a 7% difference ) at 3 years with a two - sided significance level of 5% . although we anticipated that the required events would be obtained 2 years after the final patient was randomly assigned , they accrued far more slowly than expected . 
 3 years after the final randomisation , a conditional survival analysis was done to assess the probability that continuing to wait for the full number of events would lead to a different trial conclusion . 
after discussion with the independent data monitoring committee and trial steering committee , a decision was reached that the current data were sufficiently robust for full analysis and dissemination , because the chance of obtaining a different conclusion with more events was less than 5% . all safety and primary analyses were done on an intention - to - treat basis . 
 patients either lost to follow - up or still alive at the time of analysis were censored at the date they were last known to be alive . because patients can only be deemed disease free after surgery , and to account for the different durations of preoperative chemotherapy , disease - free survival was analysed using a landmark analysis.36 rather than the date of randomisation , the time 1 week after the last patient had surgery was used as the start point , up to a maximum of 6 months from group assignment . 
patients who had an event before this point , who did not have surgery , or who were not macroscopically disease free at surgery , were said to have had an event on day 1 . 
 disease - free survival was calculated as the time from this modified origin until the first date of confirmed local recurrence , distant metastases , or death from any cause . 
 patients who had no evidence of relapse were censored on the last date they were known to be disease free . progression - free survival was calculated from random assignment to the date of the event or , in event - free patients , the date last known to be alive and free from recurrence . 
 specific site of t4 invasion is mediastinal pleura for eight patients ( four in the cisplatin and fluorouracil group vs four in the epirubicin , cisplatin , and capecitabine group ) , crura for 14 patients ( nine vs five ) , and diaphragm for five patients ( two vs three )  . table 1 : baseline characteristics grambsch - therneau test . 
the heterogeneity of treatment effects across levels of prespecified patient characteristics ( sex , age , performance status , clinical t - stage , and clinical n - stage ) were explored using cox proportional hazard models . to analyse tumour regression , the original five - point into responders mandard scale was dichotomised ( mandard trg 13 ) and non - responders ( mandard trg 45 )  . 
a second , unplanned analysis was also done because emerging evidence suggested that a more appropriate dichotomisation was mandard trg 12 as responders and grades 35 as non - responders . formal comparisons and summaries of hrql function and symptom scales were restricted to a number of prespecified outcome measures . 
global hrql and the effects of prespecified symptoms related chemotherapy and surgery ( appetite loss , dysphagia , pain , and reflux ) were compared immediately before surgery , and 3 , 12 , and 24 months after surgery , using an anova with adjustment for baseline score . 
these timepoints were considered separately , rather than using a repeated measures method of analysis . between comparisons toxicities , surgical complications , tumour regression , and resection were done using a test or fishers exact test , as appropriate . 
the corresponding author had final responsibility for the decision to submit for publication . results between jan 13 , 2005 , and oct 31 , 2011 , 897 patients were recruited from 72 uk hospitals and randomly allocated to the cf group ( n = 451 ) or the ecx group ( n = 446 ; figure 1 )  . 
the median number of patients per centre cisplatin and fluorouracil ( n = 451 ) epirubicin , cisplatin , and capecitabine ( n = 446 ) 411 ( 91% ) 387 ( 87% ) 40 ( 9% ) 59 ( 13% ) 3 ( 8% ) 11 ( 19% ) 6 ( 10% ) 4 ( 10% ) 4 ( 7% ) 6 ( 15% ) 2 ( 5% ) 1 ( 3% ) 9 ( 15% ) 7 ( 12% ) 8 ( 14% ) reason for no surgery * ct evidence of disease progression 13 ( 33% ) clinical evidence of disease progression laparoscopic evidence of disease progression surgery done comorbidity patient choice patient died resection done patient otherwise deemed inoperable 11 ( 28% ) 14 ( 24% ) surgical approach abdomen and right chest open abdomen ( laparoscopic ) and right chest open left thoracoabdominal incision totally laparoscopic other missing location mid - oesophagus siewert type 1 siewert type 2 missing 192 ( 50% ) 108 ( 28% ) 187 ( 51% ) 101 ( 28% ) 28 ( 7% ) 9 ( 2% ) 43 ( 11% ) 7 ( 2% ) 24 ( 7% ) 9 ( 2% ) 35 ( 10% ) 8 ( 2% ) 72 ( 19% ) 56 ( 15% ) 227 ( 59% ) 208 ( 57% ) 76 ( 20% ) 12 ( 3% ) 89 ( 24% ) 11 ( 3% ) data are n ( % )  . 
an open - close operation was deemed as one in which no resection was done , or the reason given on the case report form for not having surgery was that the patient was found to be inoperable at laparotomy or thoracotomy . 
after was eight chemotherapy , following retrospective review of the baseline ct scan , one patient was found to be ineligible because of adrenal metastases so did not have surgery , but was included in all summaries and analyses . 
the median age was 62 years ( iqr 5667 ; range 2781 ) , 810 ( 90% ) of 897 patients were male , 603 ( 67% ) had a who performance status of 0 , and 576 ( 64% ) had stage t3n1 cancer ( table 1 ; appendix pp 45 )  . three ( 4% ) of 72 recruiting centres did not take part in the hrql aspect of the trial for any of their patients , and hrql assessment data were omitted at baseline for the [ 4% ] of the total patients from these centres ( 37 897 patients )  . 
baseline hrql was also well balanced see online for appendix 1254 vol 18 september 2017 articles ( 1834 ) , appetite ( 2405 ) , pain 203 between the two groups . 
mean values ( sd ) for the five prespecified domains of interest were : global hrql ( 2798 ) , 760 reflux 173 ( 2050 ) , and dysphagia 739 ( 257 ) ; data per treatment group are in the appendix ( pp 810 )  . 
a higher score indicates better hrql for the global score and dysphagia , but worse hrql for the symptom scales . loss 374 details of the chemotherapy received are shown in table 2 . 
four patients ( < 1% ; two in the cf group and two in the ecx group ) of 897 withdrew consent before starting chemotherapy and five ( 1% ; one cf , four ecx ) died during chemotherapy . 
the number of patients who completed their allocated treatment was greater in the cf group than in the ecx group ( 435 [ 96% ] of 451 vs 363 [ 81% ] of 446 ; p < 00001 ) , although a similar number of patients in the cf ( 435 [ 96% ] of 451 ) and ecx ( 432 [ 97% ] of 446 ) groups received at least two cycles . 
of the 451 patients in the cf group , eight ( 2% ) stopped chemotherapy because of toxicity and one ( < 1% ) died , whereas in the ecx group , 46 ( 10% ) of 446 patients stopped because of toxicity , and five ( 1% ) died , one of which was thought to be related to chemotherapy toxicity ( figure 1 )  . 
the number of patients requiring dose reduction to any drug was smaller in the cf than in the ecx group ( 88 [ 20% ] of 451 vs 187 [ 42% ] of 446 ; p < 00001 ) , although the number receiving cisplatin dose reductions was similar between the groups ( 61 [ 14% ] of 451 in the cf group and 53 [ 12% ] of 446 in the ecx group )  . the median time from randomisation to surgery was 71 days ( iqr 6680 ) in the cf group and 127 days ( 119137 ) in the ecx group . 
the median time of surgery from the start of the last preoperative chemotherapy cycle was 44 days ( 3952 ) for patients in the cf group and 57 days ( 5264 ) for patients in the ecx group . 
of the 99 who did not have surgery , 41 ( 41% ) were because of disease progression , nine ( 9% ) died before surgery , nine ( 9% ) decided not to have surgery , that ( 15% ) developed significant comorbidities precluded surgery , and 25 ( 25% ) were deemed otherwise unsuitable for surgery . 
in total , 411 ( 91% ) of 451 patients in the cf group and 387 ( 87% ) of 446 patients in the ecx group proceeded to surgery ( figure 1 )  . 751 ( 84% ) of 897 people had resection and reconstruction , whereas 47 ( 5% ) of 897 patients were found to have progressive disease or to be inoperable during surgery ( table 3 )  . 
588 ( 78% ) of 751 resections were done via the abdomen and right chest using open surgery throughout ( ivor - lewis resection ) or as hybrid with a laparoscopic abdominal approach . 
the median follow - up of the surviving patients was 64 years ( iqr 4882 ) , and 250 ( 93% ) of 268 patients had at least 3 years of follow - up assessments . 
median overall survival was estimated to be 234 months ( 95% ci 206263 ) in the cf group and 261 months ( 225297 ) in the ecx group , with an hr of 090 ( 95% ci 077105 , p = 019 )  . 
no evidence indicated that the proportional hazards assumption was violated . figure 3 shows prespecified subgroup analyses of overall survival were done , considering sex , age group ( < 60 years , 6069 years , and 70 years ) , who performance status , clinical t - stage , and clinical n - stage ( appendix p 11 )  . median disease - free survival ( 347 events in the cf group vs 316 events in the ecx group , based on a 6 - month landmark analysis ; appendix p 13 ) was 116 months ( 95% ci 89133 ) in the cf group and 144 months ( 117165 ) in the ecx group , with an hr of 086 ( 95% ci 074100 , p = 0051 )  . chemotherapy toxicity data were not provided by three patients in each group and two in each group did not receive any chemotherapy . 
p values for heterogeneity of treatment effect are 069 for sex , 005 for age , 046 for who performance status , 011 for t - stage , and 0028 for n - stage . 
one patient in the epirubicin , cisplatin , and capecitabine group died of cerebrovascular incident ( reported as other toxicity )  . table 4 : chemotherapy toxicity group ( 0 , p < 00001 )  . 
 in patients for whom data were reported , no difference was seen in the overall prevalence of surgical complications between the two treatment groups ( 224 [ 56% ] of 398 people in the cf group and 233 [ 62% ] of 374 in the ecx group ; p = 0089 ) , although more people in the ecx group had respiratory complications ( 125 [ 33% ] of 374 ) than in the cf group ( 107 [ 27% ] of 398 ; p = 0048 ; appendix p 7 )  . 
at 30 days after surgery , ten ( 2% ) of 411 patients in the cf group and 11 ( 3% ) of 387 people in the ecx group had died , and at 90 days , 21 ( 5% ) people in the cf group and 23 ( 6% ) people in the ecx group had died . in the local pathologist review ( table 5 ) , the primary tumour was classified as mandard trg 13 in 44 ( 15% ) of the 288 specimens with available results from the cf group and 93 ( 32% ) of the 289 specimens from the ecx group ( p < 00001 )  . 
mandard primary tumour regression data were also available from central pathology review of 656 patients ( 87% of patients who had a resection ) and a total of 24 625 slides were received , with a median of 34 ( iqr 2445 ) slides per person . 
the proportions of patients who achieved r0 , r1 , and r2 were similar in both groups . no statistically and clinically relevant differences were seen between the treatment groups in terms of hrql ( appendix pp 810 ) in any of the prespecified domains ( global quality of life , pain , reflux , appetite loss , or dysphagia ) or at nearly all timepoints ( preoperatively and 3 , 12 , and 24 months postoperatively )  . 
r0 = no tumour cells within 1 mm of any resection margr1 = presence of tumour cells at or within 1 mm of a longitudinal or radial or circumferential resection marg r2 = macroscopically visible tumour left behind during surgery . 
the proportion of surviving patients who time , completed hrql assessments declined over with 725 ( 84% ) of 860 patients completing an assessment at randomisation , 339 ( 57% ) of 595 at 3 months after surgery , 208 ( 45% ) of 467 at 12 months , and 142 ( 44% ) of 322 at 24 months . when the trial and analyses were planned , we felt that mandard trg 1 , 2 , or 3 was the most suitable definition of good response to treatment . 
exploratory analyses ( appendix p 14 ) in patients who had available specimens suggested that postoperative survival of patients with tumours considered to be mandard trg 1 or 2 was significantly different ( appendix p 14 ) to survival in those with tumours considered to be mandard trg 3 , 4 , or 5 , so mandard trg 1 or 2 appeared to denote significant tumour regression . 
applying this definition to the locally collected histopathological data , 18 ( 6% ) of 288 patients in the cf group and 48 ( 17% ) of 289 patients in the ecx group regression ( p < 00001 )  . 
similarly , using the central review data , 12 ( 4% ) of 339 patients in the cf group and 37 ( 12% ) of 317 patients in the ecx group achieved notable tumour regression ( p < 00001 )  . significant achieved tumour in the exploratory analysis of progression - free survival , median progression - free survival ( 343 events in the cf group vs 313 in the ecx group ; appendix p 13 ) was vol 18 september 2017 1257 articles 184 months ( 95% ci 152205 ) in the cf group and 214 months ( 194240 ) in the ecx group , with an hr of 084 ( 95% ci 072098 , p = 0033 )  . 
the contributing progression - free survival event was either local recurrence ( 60 [ 17% ] of 343 patients in the cf group vs 46 [ 15% ] of 313 in the ecx group ) , distant metastases ( 94 [ 27% ] of 343 people vs 78 [ 25% ] of 313 ) , local recurrence and distant metastases ( 87 [ 25% ] of 343 vs 59 [ 19% ] of 313 ) , or death without confirmed progression ( 102 [ 30% ] of 343 vs 130 [ 42% ] of 313 )  . an exploratory analysis highlighted that the overall survival hr did not remain constant over time , and a strong interaction with year of randomisation was seen ( p = 00004 ; appendix p 12 )  . 
patients randomly assigned early in the trial ( 200507 ) had some survival benefit in the ecx group compared with those in the cf group , whereas those assigned in later years ( 2008 onwards ) did not . 
the use of pet scans increased greatly over the course of the trial , and so a further exploratory subgroup analysis was done looking at the effect of receiving a pet scan . 
 patients who did not have a pet scan had longer overall survival in the ecx group , whereas for patients who did receive a pet scan , ecx gave no survival advantage . discussion this study showed that more intensive neoadjuvant chemotherapy with four cycles of ecx provided no overall or disease - free survival advantage over two cycles of cf in 897 patients with oesophageal adenocarcinoma . 
chemotherapy toxicity and serious adverse events were reported more often with ecxas can be expected from four cycles of a triplet regimen compared with two cycles of a doublet regimen . 
these adverse events contributed to a greater number of patients completing their planned chemotherapy and undergoing surgery in the cf group than in the ecx group , although surgical resection , postoperative complications , and postoperative mortality were similar between the groups . 
in a post - hoc exploratory analysis , improved progression - free survival was shown with ecx treatment compared with cf treatment . more patients in the ecx group had a good pathological response to chemotherapy ( mandard trg 1 or 2 ) , and consequently more were staged as ypt0 or 1 or ypn0 after surgery , than were those in the cf group . 
results from the mrc gastro - oesophageal st0338 study showed that mandard trg 1 or 2 after chemotherapy was associated with improved survival compared with mandard trg 3 , 4 , or 5 . 
however , the absolute numbers of specimens assessed that were classified as mandard trg 1 or 2 ( 48 [ 17% ] of 289 in the ecx group vs 18 [ 6% ] of 288 in the cf group ) were low , and so this difference did not translate into an overall survival benefit . the results of this trial raise the question of the optimal number of preoperative chemotherapy cycles . 
in the current absence of a reliable biomarker that enables prediction of responses either before or midway through preoperative treatment , the extent of preoperative chemotherapy relies on the judgement of the clinician after discussion with the patient , to balance the possibility of achieving a good response against the risk of not being able to proceed to surgery . 
 however , two cycles of cf preoperatively has not been the perioperative approach directly compared with assessed in the magic trial , 25 which studied three cycles of ecx given preoperatively and post operatively . 
given the increased proportion of patients who achieved a response with ecx treatment in our study , a smaller number of preoperative cycles ( two or three ) with a triplet regimen combined with the selective use of postoperative chemotherapy for responding patients might be a better approach than either four cycles of ecx or two cycles of cf . oe05 showed an improvement in overall survival of patients in the cf group ( recruited 200511 ) compared with the same regimen in oe02 ( recruited 199298 ) , in which the median survival was 14 years compared with 20 years in oe05 . a number of potential factors could explain why the survival of patients with oesophageal cancer who were treated with cf improved with time . 
changes in referral patterns , moves towards centralisation of surgical services , the introduction of endoscopic ultrasonography , and the development of multidisciplinary teams are all events that occurred towards the end of recruitment to the oe02 study , and these changes might have led to better patient selection for attempted curative treatment by the time of this oe05 study . 
post - hoc analyses indicated that ecx offered a survival benefit in the early years of the study when pet scans were rarely used , but offered no benefit during the later years when pet was used for nearly all patients . 
patients with this type of disease are now usually identified and would have been ineligible for participation in the study . neoadjuvant chemoradiotherapy has also improved survival compared with surgery alone for patients with oesophageal adenocarcinoma and squamous cell cancers , with a median survival of 486 months ( 95% ci 321651 ) with adjuvant therapy compared with led 1258 vol 18 september 2017 articles 240 months ( 95% ci 142337 ) with surgery alone in the cross trial.39 the hrs for comparison with surgery alone are similar with chemoradiotherapy in cross ( 073 [ 95% ci 055088 ] in patients with adeno carcinoma ) and with chemotherapy in magic ( 075 [ 060093 ] ) , suggesting trials studied slightly different that although populations , the size of benefit might be similar . 
trials comparing these two approaches directly20 , 23 , 24 have shown an increased response with chemo radiotherapy , but without any subsequent improvement in overall survival . the the present study has a number of advantages over other oesophageal cancer trials . 
this study was confined to patients with adenocarcinomas of the oesophagus and gastro - oesophageal junction ( siewert type 1 and 2 ) , specifically excluding squamous cell cancers and siewert type 3 ( gastric cancer )  . 
to our knowledge , our study is the only prospective randomised trial in neoadjuvant treatment and surgery for oesophageal cancer to have included a comprehensive prospective assessment of hrql using validated generic and specific measures . 
 although no differences between trial groups were observed in hrql , the data confirm findings from much smaller cohort studies.40 neoadjuvant chemotherapy and surgery are associated with reduced hrql that persists for more than 6 months after surgery , and some features such as appetite loss persist for at least 12 months . 
 these hrql results should be accepted as the standard that can be achieved with current platinum - based or fluoropyrimidine - based neoadjuvant chemotherapy and surgery , and communicated to patients during shared decision making before surgery , along with the likely median survival data of the combined interventions . 
 limitations of this study include the changing use of pet scanning through the course of this trial as we have discussed and its potential effect on the prognosis of patients who entered the trial over time . 
additional limitations are the fact that postoperative chemotherapy was not assessed , and the challenge of interpreting and implementing these results in the face of the evolving role of chemoradiation in the management of oesophagogastric adenocarcinomas . data published in 2017 show a survival advantage for patients treated with docetaxel , oxaliplatin , and fluorouracil compared with epirubicin , cisplatin , and fluorouracil or ecx given perioperatively for junctional and gastric tumours , with a 3 - year overall survival of 57% for the docetaxel - containing regimen compared with 48% with epirubicin , cisplatin , and fluorouracil or ecx ( hr 077 , 95% ci 063094 ) .41 though an improvement in overall survival for biomarker - unselected patients , these results highlight that further improvements in outcomes are still needed for these patients . 
alternative neoadjuvant approaches such as chemoradiation are also being investigated.42 , 43 additional correlative science projects are planned for this trial with the aim of identifying subsets of patients who might specifically benefit from ecx neoadjuvant chemotherapy . contributors da and dc were joint chief investigators . 
all authors were involved in data interpretation , manuscript review , and approval of the final manuscript . declaration of interests dc reports grants from amgen , astrazeneca , bayer , celgene , merrimack , medimmune , merck serono , sanofi , and the national institute of health biomedical centre at the institute of research and royal marsden hospital . 
 leucovorin , fluorouracil , and oxaliplatin plus bevacizumab versus s - 1 and oxaliplatin plus bevacizumab in patients with metastatic colorectal cancer ( soft ) : an open - label , non - inferiority , randomised phase 3 trial . 
this has been corrected online as of dec 30 , 2013 . correction to lancet oncol 2013 ; 14 : 1295306 zhang j - x , song w , chen z - h , et al . 
 docetaxel or pemetrexed with or without cetuximab in recurrent or progressive non - small - cell lung cancer after platinum - based therapy : a phase 3 , open - label , randomised trial . 
 lancet oncol 2013 ; 14 : 132636in the online first version of this article ( published online nov 12 ) , in table 3 , all entries of ( > 1% ) should have read ( < 1% ) , and the rst two sentences of the third paragraph on page 1335 should state : a subsequent analysis of flex showed a signi cant association between egfr expression by immunohistochemistry and improved outcomes , with high egfr expression ( h - score 200 or higher ) being associated with improved overall survival , time - to - treatment failure , and a greater proportion of patients achieving objective responses when treated with cetuximab than when treated with cisplatin plus vinorelbine alone.13 there was no improvement in outcomes in the low h - score group ( h - score lower than 200 ) .13 these corrections were made to the print version of the article in the december issue of the journal , and have been made online as of nov 22 , 2013 . 
in table 1 , the entry for adenocarcinoma in the cetuximab and pemetrexed group should have read 161 ( 53% ) and the entry for all other diagnoses in the pemetrexed group should have read 41 ( 13% )  . 
in table 3 , in the cetuximab plus pemetrexed group , the entry for patients with one or more ctcae grades 12 should have read 89 ( 30% ) , that for grade 3 anaemia 16 ( 5% ) , for grade 4 infusion related reactions 5 ( 2% ) , and grade 3 lung infection 16 ( 5% )  . 
 in the pemetrexed group in the same table , the entry for patients with one or more grade 4 ctcae should have read 36 ( 12% ) and one or more grade 5 ctcae 10 ( 3% ) ; the entry for grade 12 diarrhoea should have read 36 ( 12% ) , that for grade 12 hyperglycaemia 10 ( 3% ) , and grade 12 maculopapular rash 39 ( 13% )  . 
 vol 15 january 2014 gemcitabine and docetaxel versus doxorubicin as first - line treatment in previously untreated advanced unresectable or metastatic soft - tissue sarcomas ( geddis ) : a randomised controlled phase 3 trial beatrice seddon , sandra j strauss , jeremy whelan , michael leahy , penella j woll , fiona cowie , christian rothermundt , zoe wood , charlotte benson , nasim ali , maria marples , gareth j veal , david jamieson , katja kver , roberto tirabosco , sharon forsyth , stephen nash , hakim - moulay dehbi , sandy beare summary background for many years , first - line treatment for locally advanced or metastatic soft - tissue sarcoma has been doxorubicthis study compared gemcitabine and docetaxel versus doxorubicin as first - line treatment for advanced or metastatic soft - tissue sarcoma . methods the geddis trial was a randomised controlled phase 3 trial done in 24 uk hospitals and one swiss group for clinical cancer research ( sakk ) hospital . 
eligible patients had histologically confirmed locally advanced or metastatic soft - tissue sarcoma of trojani grade 2 or 3 , disease progression before enrolment , and no previous chemotherapy for sarcoma or previous doxorubicin for any cancer . 
patients were randomly assigned 1 : 1 to receive six cycles of intravenous doxorubicin 75 mg / m on day 1 every 3 weeks , or intravenous gemcitabine 675 mg / m on days 1 and 8 and intravenous docetaxel 75 mg / m on day 8 every 3 weeks . 
the trial was registered with the european clinical trials ( eudract ) database ( no 200901490729 ) and with the international standard randomised controlled trial registry ( isrctn07742377 ) , and is now closed to patient entry . findings between dec 3 , 2010 , and jan 20 , 2014 , 257 patients were enrolled and randomly assigned to the two treatment groups ( 129 to doxorubicin and 128 to gemcitabine and docetaxel )  . 
 the proportion of patients alive and progression free at 24 weeks did not differ between those who received doxorubicin versus those who received gemcitabine and docetaxel ( 463% [ 95% ci 375546 ] vs 464% [ 375548 ] ) ; median progression - free survival ( 233 weeks [ 95% ci 196304 ] vs 237 weeks [ 181200 ] ; hazard ratio [ hr ] for progressionfree survival 128 , 95% ci 099165 , p = 006 )  . 
the most common grade 3 and 4 adverse events were neutropenia ( 32 [ 25% ] of 128 patients who received doxorubicin and 25 [ 20% ] of 126 patients who received gemcitabine and docetaxel ) , febrile neutropenia ( 26 [ 20% ] and 15 [ 12% ] ) , fatigue ( eight [ 6% ] and 17 [ 14% ] ) , oral mucositis ( 18 [ 14% ] and two [ 2% ] ) , and pain ( ten [ 8% ] and 13 [ 10% ] )  . 
154 ( 60% ) of 257 patients died in the intention - to - treat population : 74 ( 57% ) of 129 patients in the doxorubicin group and 80 ( 63% ) of 128 in the gemcitabine and docetaxel group . 
no deaths were related to the treatment , but two deaths were due to a combination of disease progression and treatment . interpretation doxorubicin should remain the standard first - line treatment for most patients with advanced softtissue sarcoma . 
these results provide evidence for clinicians to consider with their patients when selecting first - line treatment for locally advanced or metastatic soft - tissue sarcoma . funding cancer research uk , sarcoma uk , and clinical trial unit kantonsspital st gallen . copyright the author ( s )  . 
we identified six published randomised controlled trials , none of which showed a survival advantage for any schedule over single - agent doxorubicwe identified a further randomised controlled study comparing single - agent doxorubicin versus doxorubicin and ifosfamide chemotherapy , which was recruiting at that time , and which has since been published in 2014 , showing an advantage for the combination for progression - free survival but not overall survival . 
 although we identified three phase 2 studies ( one of which was a randomised phase 2 study comparing gemcitabine versus gemcitabine and docetaxel ) , we were unable to find any phase 3 trials comparing this combination with doxorubicin . added value of this study to our knowledge , this is the first randomised controlled trial that compares two commonly used treatmentsdoxorubicin versus gemcitabine and docetaxelas first - line treatment in advanced soft - tissue sarcoma . 
furthermore , planned subgroup analyses have not identified any subgroup for which gemcitabine and docetaxel was superior , and in particular we did not observe superiority for either leiomyosarcoma or uterine leiomyosarcoma , for which gemcitabine and docetaxel has previously been believed to be particularly active . 
we found worse treatment adherence with gemcitabine and docetaxel compared with doxorubicin , with more dose delays , lower dose intensity , and more patients stopping treatment early due to toxicity , and lower quality - of - life scores . implications of all the available evidence these results provide evidence for clinicians to consider with patients when selecting first - line treatment for advanced soft - tissue sarcoma . 
although the observed similar progression - free survival and overall survival of gemcitabine and docetaxel and doxorubicin might support a conclusion that either schedule can be used according to patient or clinician preference , our results indicate the need for caution with such an approach given the greater difficulty in delivery and toxicity of gemcitabine and docetaxel , and indeed the higher cost of this combination regimen . 
the data support the conclusion that doxorubicin should remain standard of care as first - line treatment for most patients with advanced soft - tissue sarcoma , and that there is no subgroup of patients for whom gemcitabine and docetaxel should be routinely recommended . introduction soft - tissue sarcoma comprises a number of rare malignancies , with 3298 patients newly diagnosed with the disease in the uk in 2010.1 surgery with radiotherapy is the most common treatment for localised disease , with associated 5 - year overall survival of 55% in 200610.1 survival outcomes for locally advanced or metastatic softtissue sarcoma are poor , with a median overall survival of 128143 months after diagnosis.2 , 3 doxorubicin has been used as first - line treatment for locally advanced or metastatic soft - tissue sarcoma for more than 40 years . 
a trial2 comparing randomised controlled phase 3 combination doxorubicin versus doxorubicin alone showed a significant increase in progression - free survival in the combination treatment group , but with no increase in overall survival . 
toxicity was predictably higher in the combination group , and the authors concluded their results do not support the use of intensified doxorubicin and ifosfamide for palliation of advanced soft - tissue sarcoma unless the specific goal is tumour shrinkage . 
subsequently , two first - line phase 3 trials4 , 5 have combined doxorubicin with novel agents ( doxorubicin and palifosfamide compared with doxorubicin and placebo , 4 and doxorubicin and evofosfamide compared with doxorubicin alone5 ) , and neither study ifosfamide and was able to show improved progression - free survival or overall survival for the combination treatments . 
thus , no regimen has proved to be unequivocally superior to doxorubicin as first - line treatment for locally advanced or metastatic soft - tissue sarcoma . gemcitabine and docetaxel was first reported as a treatment for locally advanced or metastatic soft - tissue sarcoma in 2002 . 
this study also compared plasma levels of gemcitabine achieved with a 90 - min infusion versus a 30 - min infusion , and showed that the 90 - min infusion was associated with a longer duration of plasma gemcitabine concentrations above 10 mol / l , which is the threshold for saturation of intracellular accumulation of the active form of the drug , gemcitabine triphosphate . 
a further retrospective review of gemcitabine and docetaxel in patients with locally advanced or metastatic disease included an in - vitro study to investigate the dosing sequence of gemcitabine and docetaxel , finding that gemcitabine followed by docetaxel was synergistic , whereas docetaxel followed by gemcitabine was antagonistic.7 hence , the currently used schedule of gemcitabine and docetaxel in locally advanced or metastatic soft - tissue sarcoma was established . 
subsequently , several 1398 vol 18 october 2017 articles retrospective studies and phase 2 studies , in both leiomyosarcoma811 and unselected soft - tissue sarcoma , 7 , 12 , 13 have all showed activity of the combination . 
the observed responsiveness of leiomyosarcoma in particular has led to some clinicians adopting gemcitabine and docetaxel as a first - line treatment option for locally advanced or metastatic leiomyosarcoma , in the absence of evidence from phase 3 trials . 
with increasing use of the combination in both leiomyosarcoma and locally advanced or metastatic softtissue sarcoma , robust evidence is needed to establish the roles of gemcitabine and docetaxel and doxorubicin as firstline treatments for this disease . the geddis trial aimed to compare the efficacy of gemcitabine and docetaxel versus doxorubicin in the firstline setting for locally advanced or metastatic soft - tissue sarcoma . 
a pharmacogenomics study was also done to investigate the influence of single - nucleotide polymorphisms ( snps ) on treatment efficacy and toxicity . methods study design and participants geddis was a multicentre , randomised , phase 3 trial , which recruited patients from 24 uk hospitals , and one swiss group for clinical cancer research ( sakk ) hospital in switzerland ( appendix p 1 )  . 
patients were required to have adequate organ function ( absolute neutrophil count 10 10 per l ; platelet count 100 10 per l ; bilirubin 15 upper limit of normal [ uln ] ; aspartate transaminase , alanine transaminase , or both 30 uln ; alkaline phosphatase 30 uln [ patients were eligible with a higher alkaline phosphatase concentration if this was shown to be due to bone isoenzyme ] ; measured or calculated creatinine clearance 30 ml / min ; and cardiac ejection fraction within local normal limits )  . 
tumour tissue was required to be available for central review . treatment delays patients were excluded from the trial if they had alveolar soft part sarcoma , gastrointestinal stromal tumour , ewings dermatofibrosarcoma sarcoma , alveolar or embryonal rhabdomyosarcoma , desmo plastic small round cell tumour , extraskeletal myxoid chondrosarcoma , protuberans , malignant mixed mesodermal tumour or carcinosarcoma of the uterus , smooth muscle tumours of uncertain malignant potential of uterus , known active or uncontrolled brain metastases , active uncontrolled infection , or grade 3 or 4 peripheral neuropathy . 
pregnant or lactating women were excluded , as were patients with a history of malignancy other than sarcoma ( exceptions included basal or squamous cell carcinoma of the skin and carcinoma in situ of the cervix , breast , or prostate ) within 3 years before enrolment . samples of formalin - fixed , paraffin - embedded tumour tissue and haematoxylin and eosin - stained slides were submitted for central review for confirmation of sarcoma diagnosis and histological subtype , although patients were enrolled on the basis of the local pathology report . 
all samples were reviewed by a single histopathologist ( rt )  . the trial was approved by the national research ethics service committee : london , bloomsbury ( 10 / h0713 / 54 ) , the medicines and healthcare products regulatory agency ( clinical trials authorisation number 20363 / 0285 / 001 0001 ) , and by the research and development department of each participating nhs trust . 
gemcitabine was administered over 90 min and docetaxel was administered over 60 mdose capping according to sites local policy and dose banding to within plus or minus 5% of the calculated dose were permitted . 
in both groups , patients completed up to six cycles of treatment in the absence of disease progression , intolerable side - effects , or withdrawal of consent . laboratory monitoring ( blood count and biochemistry ) was done within 72 h of day 1 of each cycle , with additional monitoring on day 8 ( blood count only ) for gemcitabine and docetaxel treatment . 
to proceed with treatment on day 1 of each cycle ( both groups ) the following were required : absolute neutrophil count of at least 10 10 per l , platelet count of at least 100 10 per l , bilirubin of up to 15 uln , and aspartate transaminase , alanine trans aminase , or both of up to 30 uln . 
for administration of treatment on day 8 ( in the gemcitabine and docetaxel group ) the following were required : absolute neutrophil count of at least 10 10 per l and platelets of at least 75 10 per l . 
dose modifications for adverse events were made according to prespecified criteria : dose reductions of 20% ( first occurrence ) nd then 33% ( second occurrence ) were permitted for doxorubicin ( in the case of grade 3 or worse febrile neutropenia ) and gemcitabine and docetaxel ( for grade 3 or worse febrile neutropenia , grade 2 neuropathy , or any grade pulmonary toxicity ) ; a third occurrence required the patient to be withdrawn from treatment . 
 dose delays of up to 2 weeks for haematological toxicity and up to 3 weeks for non - haematological toxicity were allowed ; delays longer than this required the patient to be withdrawn from treatment . 
for doxorubicin , patients were advised to be withdrawn from treatment if left ventricular ejection fraction was less than 45% or reduced by 20% from baseline ( cardiotoxicity monitoring was done according to local institutional policies )  . 
for gemcitabine and docetaxel , patients were withdrawn for the following events : grade 3 pulmonary fibrosis , any grade 4 pulmonary toxicity , grade 3 or 4 hypersensitivity reactions ( docetaxel only ) , or grade 3 weight gain . adverse events were assessed according to the national cancer institute common terminology criteria for adverse events ( ctcae ) version 4.03 , from informed consent until 30 days after last trial treatment administration . 
serious adverse events were reported from informed consent until 30 days after last trial treatment administration , or later if the investigator felt that an event was related to trial treatment . disease status was assessed by ct scan , mri scan , or both at baseline , 12 and 24 weeks after randomisation , and then every 12 weeks until disease progression ( including patients who discontinued treatment for any reason other than disease progression )  . 
 for the pharmacogenomics analyses , dna was extracted from 4 ml whole blood using a qiaamp dna blood maxi kit ( qiagen , manchester , uk ) , according to the manufacturers instructions . 
individual candidate snps the pharmacology of the three drugs were identified from relevant published literature , 1521 and taqman assay on demand probes ( applied biosystems , paisley , uk ) were used to genotype the samples . in genes associated with outcomes the primary endpoint was the proportion of patients alive and progression free at 24 weeks after the date of randomisation . 
secondary endpoints were the proportion of patients alive and progression free at 12 weeks after the date of randomisation , progression - free survival ( time from randomisation to date of progression or death from any cause , whichever occurred first ) , and overall survival ( time from randomisation to date of death from any cause ) , the proportion of patients achieving an objective response by recist 1.1 , the proportion of patients achieving an objective response by choi criteria ( retrospective analysis ) , assessment of adverse events , quality of life , and health economics evaluation . 
time to progression , proportion of patients achieving an objective response as assessed by choi criteria , the health economics assessment , and the planned sensitivity analyses will all be published separately at a later date . 
 statistical analysis under the assumption of a hazard ratio ( hr ) of 063 , 250 patients ( and 148 progressions or deaths ) were required to achieve 80% power with a two - sided of 5% . 
 we assumed a median progression - free survival of 35 months for doxorubicin22 ( corresponding with 30% of patients achieving 24 - week progression - free survival ) and a median progression - free survival of 5 months 1400 vol 18 october 2017 articles ( corresponding with 47% of patients achieving 24 - week progression - free survival ) for gemcitabine and docetaxel.6 , 13 we did the efficacy analysis in the intention - to - treat population of all randomised patients . 
we plotted kaplan - meier curves for progression - free survival and overall survival ; treatment effect hrs ( with 95% cis and p values ) were obtained from cox proportional hazards regression models , adjusted for randomisation stratification factors . 
these analyses were exploratory by nature , and were performed using tests for interaction . we presented adverse events as the worst grade per patient per event , and comparison between groups was done using a test of proportions . we assessed quality of life at the 12 - week postrandomisation visit . 
we used ancova and fitted a linear regression model adjusting for baseline score , stratification factors , and actual time between baseline and 12 - week assessments ( to allow for variation in the timings of assessments )  . 
we prospectively actual planned in our statistical analysis plan to use 99% cis to account for multiple comparisons within the different scales of quality of life , which is a robust approach when the risk of a type 1 error is inflated by making multiple comparisons . to assess the effect of snps on efficacy and toxicity within treatment groups , we used cox proportional hazards regressions on overall survival and progressionfree survival and logistic regressions on any grade 3 or 4 adverse events . we calculated dose intensity relative to the total planned dose using a formula that incorporated delays and dose reductions.23 we used stata version 14.2 for all statistical analyses . an external independent data monitoring committee oversaw the trial and assessed the safety and efficacy approximately annually . 
this study is registered with the european clinical trials ( eudract ) database ( no 2009 01490729 ) and as an international standard randomised controlled trial , number isrctn07742377 . role of the funding source the trial was sponsored by university college london ( ucl ) and coordinated centrally by cancer research uk and ucl ctc . 
the corresponding author had full access to all the data and the final responsibility to submit for publication . associated with raw data the results between dec 3 , 2010 , and jan 20 , 2014 , 257 patients from 24 uk hospitals and one swiss hospital ( appendix p 1 ) were enrolled and randomly assigned to receive doxorubicin ( 129 patients ) or gemcitabine and docetaxel ( 128 patients ; figure 1 )  . 
two randomised patients ( one in each group ) were later found to be ineligible ( figure 1 ) ; however , both are included in the intention - totreat analysis and received treatment . 
our safety population included 254 of the 257 randomised patients , 497 patients assessed for eligibility 240 excluded 91 did not meet inclusion criteria 96 declined to participate 53 other reasons * 257 patients enrolled and randomly assigned 129 allocated to doxorubicin 128 allocated to gemcitabine and docetaxel 1 did not start treatment 2 did not start treatment 128 received allocated intervention ( including 126 received allocated intervention ( including 1 ineligible patient ) 1 ineligible patient ) 3 lost to follow - up 58 discontinued intervention|| 1 lost to follow - up 79 discontinued intervention|| 129 included in intention - to - treat population 128 included in safety population 128 included in intention - to - treat population 126 included in safety population figure 1 : trial profile * other reasons were : 43 multidisciplinary team decision not to approach patient , five deaths , three referred to or treated at other hospital , one patient did not fully understand trial , one trial closed before patient finished radiotherapy . 
histology review reclassified as ineligible histological subtypes ( one gastrointestinal tumour in the doxorubicin group and one extra - skeletal myxoid chondrosarcoma in the gemcitabine and docetaxel group )  . 
||see appendix p 6 for a breakdown of reasons for treatment discontinuation . vol 18 october 2017 1401 articles because one patient who was assigned to doxorubicin and two patients who were assigned to gemcitabine and docetaxel did not receive at least one dose of their allocated treatment ( figure 1 )  . patient characteristics were similar in the two treatment groups at baseline ( table 1 )  . 
the analysis is based on the dataset in its version of sept 8 , 2015 ; at this point , the estimated median follow - up for all patients was 22 months ( iqr 157293 )  . of the 257 randomised patients , 244 ( 95% ) had central histopathology review done . 
51 ( 21% ) of 244 reports differed between the local histology report and the central review report , with 36 ( 14% ) major discrepancies resulting in reclassification of histology , and 15 ( 6% ) minor discrepancies ( eg , high - grade spindle cell sarcoma being reclassified as pleomorphic sarcoma )  . 
of the 13 ( 5% ) of 257 patients whose histology was not reviewed , six samples were never received , one patient had no tissue available , and for six patients there was no tumour tissue in the submitted blocks . more patients in the doxorubicin group ( 71 [ 56% ] of 128 patients ) received the full six cycles of chemotherapy than those in the gemcitabine and docetaxel group ( 49 [ 39% ] of 126 patients )  . 
mean dose intensity23 ( incorporating dose delays and reductions ) was 937% ( sd 009 ) in the doxorubicin group and 834% ( sd 020 ) in the gemcitabine and docetaxel group . 
 more patients in the gemcitabine and docetaxel group experienced dose delays ( 71 [ 56% ] of 126 patients ) than in the doxorubicin group ( 59 [ 46% ] of 128 patients )  . 
the main reasons for dose delays in both groups were febrile neutropenia ( seven [ 12% ] of 59 reasons in the doxorubicin group vs six [ 4% ] of 155 reasons in the gemcitabine and docetaxel group ) , other haematological toxicities ( 16 [ 27% ] vs 44 [ 28% ] ) , non - haematological toxicities ( five [ 8% ] vs seven [ 5% ] ) , other adverse events ( 14 [ 24% ] vs 29 [ 18% ] ) , and other practical or social reasons ( 11 [ 19% ] vs 32 [ 21% ] )  . 
 more patients had dose reductions in the doxorubicin group ( 34 [ 27% ] of 128 patients ) than in the gemcitabine and docetaxel group ( 23 [ 18% ] of 126 ; appendix p 17 ) ; the main reasons for dose reductions were febrile neutropenia ( eight [ 20% ] of 41 reasons in the doxorubicin group vs one [ 1% ] of 89 reasons in the gemcitabine and docetaxel group ) and other haematological toxicities ( seven [ 17% ] of 41 vs 26 [ 29% ] of 89 )  . 
one ( 1% ) of 128 patients in the doxorubicin group and 13 ( 10% ) of 126 in the gemcitabine and docetaxel group stopped treatment early because of toxicity ( appendix p 6 )  . at the time of data analysis , 223 ( 87% ) of 257 patients in the intention - to - treat population had experienced disease progression ; 106 ( 82% ) of 129 patients in the doxorubicin group and 117 ( 91% ) of 128 patients in the gemcitabine and docetaxel group . 
154 ( 60% ) of 257 patients died in the intention - to - treat population ; 74 ( 57% ) of 129 patients in the doxorubicin group and 80 ( 63% ) of 128 patients in the gemcitabine and docetaxel group . 
no deaths were related to the treatment , but two deaths were due to a combination of disease progression and treatment ( see appendix p 10 for the breakdown of causes of death by treatment group )  . 
no discrepancies were noted between the hospitals and the central review for any patients . progression - free survival at 24 weeks did not differ between the treatment groups ( 463% [ 95% ci 375546 ] in the doxorubicin group vs 464% [ 375548 ] in the gemcitabine and docetaxel group ; figure 2 )  . 
the unadjusted hr was 128 ( 95% ci 099165 ; p = 006 ) ; after adjusting for 1402 vol 18 october 2017 articles histological subtype , the hr was 126 ( 097163 ; p = 008 ) in favour of doxorubic although the kaplan - meier curves did not violate the proportional hazards assumption ( p = 046 for the adjusted model ) , they initially overlapped , and then separated after 24 weeks . overall survival did not significantly differ between the two groups . 
overall survival at 24 weeks was 868% ( 95% ci 796916 ) in the doxorubicin group and 826% ( 748882 ) in the gemcitabine and docetaxel group ( figure 3 )  . 
median overall survival was 763 weeks ( 95% ci 600913 ) in the doxorubicin group and 673 weeks ( 531831 ) in the gemcitabine and docetaxel group ( unadjusted hr 114 , 95% ci 083157 ; p = 041 )  . the proportion of patients achieving an objective response by recist 1.1 ( complete or partial response ) was similar in the two groups : 25 ( 19% ) of 129 patients in the doxorubicin group and 25 ( 20% ) of 128 in the gemcitabine and docetaxel group ( table 2 )  . 
 in our prospectively planned exploratory subgroup analysis , no evidence of a differential treatment effect by histological subtype was recorded ( p = 024 ; appendix p 11 )  . 
further subgroup analyses were done comparing leiomyosarcoma versus other sarcomas ( p = 014 ) , and uterine leiomyosarcoma versus other sarcomas ( p = 038 ) , but again no differential effect was evident between the two treatment groups . 
 the most common low - grade non - haematological adverse event was grade 1 and 2 alopecia , which occurred in 110 ( 86% ) of 128 patients in the doxorubicin group and 95 ( 75% ) of 126 patients in the gemcitabine and docetaxel group ( table 3 )  . 
the most common low - grade haematological adverse event was anaemia ( grade 12 in 91 [ 71% ] patients in the doxorubicin group vs 104 [ 83% ] in the gemcitabine and docetaxel group )  . 
the three most common serious adverse events , accounting for 111 ( 39% ) of all 285 serious adverse events , were febrile neutropenia ( 27 [ 17% ] of 155 serious adverse events in the doxorubicin group vs 15 [ 12% ] of 130 in the gemcitabine and docetaxel group ) , fever ( 18 [ 12% ] vs 19 [ 15% ] ) , and neutropenia ( 22 [ 14% ] vs ten [ 8% ] ; appendix pp 79 )  . we compared quality of life between the groups at 12 weeks postrandomisation . 
insufficient questionnaires were returned to be able to assess quality of life at 18 weeks and 24 weeks ( 83 [ 32% ] of 257 questionnaires were returned at both 18 weeks and 24 weeks , compared with 132 [ 51% ] of 257 at 12 weeks )  . 
however , the mean global health status score at 12 weeks was 638 ( sd 225 ) in the doxorubicin group ( based on 64 [ 50% ] of 129 patients ) and 591 ( sd 218 ) in the gemcitabine and docetaxel group doxorubicin gemcitabine and docetaxel hr 128 ( 95% ci 099165 ) ; p = 006 time since randomisation ( weeks ) 129 ( 0 ) 128 ( 0 ) 60 ( 1 ) 60 ( 2 ) 28 ( 6 ) 12 ( 4 ) 11 ( 10 ) 5 ( 6 ) 3 ( 11 ) 3 ( 6 ) number at risk ( number censored ) doxorubicin gemcitabine and docetaxel figure 2 : progression - free survival hr = hazard ratio . doxorubicin gemcitabine and docetaxel hr 114 ( 95% ci 083157 ) ; p = 041 time since randomisation ( weeks ) 129 ( 0 ) 128 ( 0 ) 108 ( 4 ) 104 ( 3 ) 80 ( 12 ) 74 ( 13 ) 47 ( 27 ) 44 ( 20 ) 20 ( 42 ) 24 ( 31 ) number at risk ( number censored ) doxorubicin gemcitabine and docetaxel figure 3 : overall survival hr = hazard ratio . complete response partial response stable disease progressive disease not evaluable data are n ( % )  . table 2 : objective responses doxorubicin ( n = 129 ) gemcitabine and docetaxel ( n = 128 ) 2 ( 2% ) 23 ( 18% ) 60 ( 47% ) 25 ( 19% ) 19 ( 15% ) 25 ( 20% ) 50 ( 39% ) 27 ( 21% ) 26 ( 20% ) ( based on 63 [ 49% ] of 128 patients )  . 
myocardial infarction ( grade 5 ) recorded in one patient who received doxorubicsudden death not otherwise specified ( grade 5 ) recorded in one patient who received gemcitabine and docetaxel . 
higher scores are associated with better quality of life ; a positive number indicates better functioning and quality of life on gemcitabine and docetaxel than on doxorubic lower scores are associated with better quality of life ; a positive number indicates worse symptoms on gemcitabine and docetaxel than on doxorubicc30 = eortc core quality - of - life questionnaire . 
 table 4 : difference in quality - of - life outcomes at 12 weeks after randomisation for the pharmacogenomics analysis in our translational from total dna was successfully extracted study , 240 patients : 119 in the doxorubicin group and 121 in the gemcitabine and docetaxel group . 
within the doxorubicin group , three of the four snps in the slc22a16 gene , all in linkage disequilibrium with each other , were associated with a worse progression - free survival ( appendix pp 12 , 15 ) , as was the minor allele of the slc29a1 snp ( rs9394992 , in both heterozygotes and homozygotes ; appendix p 14 )  . 
by contrast , the prdx4 snp ( rs518329 ) minor allele was associated with improved overall survival in the doxorubicin group in both heterozygotes and homozygotes ( appendix p 13 )  . 
analysis of the gemcitabine and docetaxel treatment group indicated a possible association of the abcb1 rs1045642 minor allele with worse progression - free survival in both heterozygotes and homozygotes ( appendix p 12 ) ; the cda rs2072671 snp was associated with worse overall survival ( appendix p 14 ) , and the cmpk1 rs4492666 snp was associated with improved overall survival in both heterozygotes and homozygotes ( appendix p 14 )  . 
the slc22a16 rs723685 minor allele was associated with a reduced frequency of grade 34 adverse events compared with wild type ( ten [ 48% ] of 21 patients vs 69 [ 71% ] of 97 patients ) in the doxorubicin treatment group but not in the gemcitabine and docetaxel group . 
 after completion of treatment within the trial , 58 ( 23% ) of 254 patients in the safety population ( 28 [ 22% ] of 128 patients receiving doxorubicin and 30 ( 24% ) of 126 receiving gemcitabine and docetaxel ) did not receive any additional treatment . 
the remaining 196 ( 77% ) patients received at least one additional treatment : chemotherapy for 139 ( 71% ) of 196 patients ( 62 [ 62% ] of 100 patients in the doxorubicin group and 77 [ 80% ] of 96 patients in the gemcitabine and docetaxel group ) , and local therapies for 57 ( 29% ) of 196 patients ( 38 [ 38% ] and 19 [ 20% ] )  . 
soft - tissue sarcoma is recognised to be a very heterogeneous disease with a large number of histological subtypes , and indeed our trial included 22 different subtypes , with very small numbers of patients with many of these subtypes . 
this heterogeneity is an inevitable feature of most large soft - tissue sarcoma trials , and as such we believe that the geddis trial population is representative of the general population with advanced soft - tissue sarcoma . the activity of combination gemcitabine and docetaxel has been used in locally advanced or metastatic soft - tissue sarcoma since 2002 , and has been investigated in several small studies , which have shown therapy.69 , 11 , 12 a randomised phase 2 study compared gemcitabine and docetaxel with gemcitabine alone in 122 patients with advanced soft - tissue sarcoma who had received between zero and three previous chemotherapy regimens , and reported superior median progression - free survival for gemcitabine and docetaxel compared with gemcitabine alone ( 62 months vs 30 months ) and overall survival ( 179 months vs 115 months ) .13 a subsequent randomised phase 2 study compared gemcitabine and docetaxel versus gemcitabine alone as second - line treatment in 90 patients with leiomyosarcoma , reporting that both schedules were effective second - line therapies , with similar proportions of patients achieving a response.10 gemcitabine and docetaxel has therefore become an accepted in metastatic soft - tissue sarcoma after first - line therapy.24 subsequent phase 1b / 2 studies have combined gemcitabine and docetaxel with bevacizumab showing feasibility and activity , 25 , 26 and also with pazopanib , 27 although that trial closed early because of slow accrual and substantial toxicity . 
a placebo - controlled phase 3 trial28 of gemcitabine and docetaxel in combination with bevacizumab in metastatic uterine leiomyosarcoma for first - line treatment did not show a benefit for progression - free survival or overall survival . treatment option since the first published study6 of gemcitabine and docetaxel , which was confined to patients with leiomyosarcoma , some clinicians have assumed that the combination is more active in leiomyosarcoma and uterine leiomyosarcoma than in other histological subtypes . 
 treatment eect favours doxorubicin favours gemicitabine and docetaxel figure 4 : quality - of - life outcomes at 12 weeks post - randomisation the plotted points represent the mean treatment effect between the groups ( a positive number for the treatment effect indicates a better quality of life on gemcitabine and docetaxel than doxorubicin )  . 
however , the results of the geddis trial refute these claims of superior activity in particular histological subtypes of locally advanced or metastatic softtissue sarcoma versus others , since our results show no evidence influenced by treatment effect was histological subtype . 
we did planned subgroup analyses to investigate whether patients with either leiomyosarcoma or uterine leiomyosarcoma responded better to gemcitabine and docetaxel than other soft - tissue sarcoma histological subtypes , but found no indication of a superior response to gemcitabine and docetaxel in either of these subgroups . that we chose 13 years as the minimum age for the trial , specifically to try to increase participation of the teenage and young adult population , because clinical trial recruitment of this age group is recognised to be poor.29 however , only one patient younger than 18 years of age was recruited , which we believe reflects the differing approaches to treatment of advanced soft - tissue sarcoma by uk paediatric and adult oncologistswith paediatric oncologists using more intensive chemotherapy regimens than those used in this trial . 
additionally , competing paediatric trials in this population were running in the uk at the time of recruitment to geddis , such that we believe that younger patients were preferentially recruited to those paediatric trials . why did gemcitabine and docetaxel fail to show superiority to doxorubicin ? this outcome might have been vol 18 october 2017 1407 articles partly due to the choice of lower dose and fewer cycles of treatment ; the 2002 study by hensley and colleagues6 delivered more cycles ( eight vs six ) , at higher doses ( gemcitabine 900 mg / m and docetaxel 100 mg / m vs gemcitabine 675 mg / m and docetaxel 75 mg / m ) than in geddis . 
our regimen was chosen on the basis of the randomised phase 2 study of maki and colleagues , 13 which had used the higher dose schedule , and had reported high frequency ( 46% ) of dose reductions for gemcitabine and docetaxel , lower dose intensity than gemcitabine , and more than 40% of patients on gemcitabine and docetaxel stopping within 6 months of starting therapy , for nonhaematological toxicities such as fatigue and myalgias , despite dose reductions . 
 additionally , a previous phase 2 study11 that the geddis chief investigator had led using this schedule had found that quite substantial toxicity was experienced in the uk population , such that eight ( 18% ) of 45 patients stopped treatment early due to toxicity , and only ten ( 20% ) patients received the full eight cycles . 
the lower doses used are reflected by the absence of grade 34 thrombocytopenia recorded ( no patients on gemcitabine and docetaxel experienced this toxicity ) compared with a 40% frequency in the previous randomised phase 2 study.13 it might be suggested that the gemcitabine and docetaxel doses we selected were too low . 
 however , despite modifying the gemcitabine and docetaxel schedule for the geddis trial , our results were similar for gemcitabine and docetaxel to those of maki and colleagues study , 13 with median progression - free survival of 55 months versus 62 months , and median overall survival of 155 months versus 179 months , respectively . receiving suitable for an additional factor in the lack of superiority of gemcitabine and docetaxel over doxorubicin at least for overall survival might be the lower overall exposure of patients to gemcitabine and docetaxel , as first - line and second - line treatments combined . 
of 96 patients in the gemcitabine and docetaxel group receiving a subsequent received doxorubicin , whereas of treatment , 60 100 patients in the doxorubicin group receiving a subsequent treatment , only 18 received gemcitabine and docetaxel . 
this difference is because for many uk hospitals at the time of the geddis trial , the combination of gemcitabine and docetaxel was not funded and thus unavailable to clinicians . despite the use of a modified gemcitabine and docetaxel schedule in our study , treatment adherence to gemcitabine and docetaxel was inferior to that for doxorubicpatients in the gemcitabine and docetaxel group experienced more dose delays and lower dose intensity than those in the doxorubicin group , with fewer patients in the gemcitabine and docetaxel group receiving all six cycles of chemotherapy and more patients stopping treatment early due to toxicity . 
docetaxel was omitted at these points according to protocol criteria for low neutrophils or platelets , or toxicity leading to a clinical decision to omit docetaxel ( notably , the most common non - haematological grade 34 toxicity in the gemcitabine and docetaxel group was fatigue )  . 
the excess of patients stopping gemcitabine and docetaxel early might also have reflected a bias in clinicians to stop treatment earlier in the experimental group , in the knowledge that patients could go on to receive standard doxorubicin - based treatment . 
it could be argued that the gemcitabine and docetaxel doses that were delayed or missed represent undertreatment in this group , which could explain the separation of the progression - free survival curves in figure 2 . although no significant difference was seen in any of the individual quality - of - life parameters between the treatment groups , the global health status was numerically lower for gemcitabine and docetaxel than in the doxorubicin group . 
 potential contributing factors are that gemcitabine and docetaxel requires an additional visit to hospital in each 3 - week cycle , and gemcitabine and docetaxel takes longer to deliver than doxorubicin , prolonging each hospital visit and resulting in an added burden on patients with incurable disease receiving palliative chemotherapy . 
the implication of these results is that gemcitabine and docetaxel was more difficult to deliver ( lower dose intensity , more treatment delays , and more patients stopping early due to toxicity ) , and was associated with a worse global health status than doxorubicthus , there does seem to be a disadvantage to patients in receiving gemcitabine and docetaxel as first - line treatment . 
furthermore , there are economic , as well as personal , disadvantages gemcitabine and docetaxel because it is a more expensive treatment regimen than doxorubicin because of higher drug costs , more frequent and longer hospital visits are needed for treatment , and increased requirements for supportive medications ( data not shown )  . importantly , the results of the current study are consistent with two other first - line studies in locally advanced or metastatic soft - tissue sarcoma that included doxorubicin as the control group , with the median progression - free survival of 233 weeks the doxorubicin group in the current study similar to the 225 weeks4 and 26 weeks5 reported in the other studies . 
 this is also true of median overall survival , which was 763 weeks in the doxorubicin group in the current study , compared with 732 weeks4 and 823 weeks5 with doxorubicin in the other studies . 
interestingly , all three studies showed an improvement in progressionfree survival and overall survival compared with the preceding published trial of judson and colleagues2 ( progression - free survival of 199 weeks and overall survival of 554 weeks ) , which had recruited patients several years earlier , suggesting that outcomes have improved for patients with locally advanced or metastatic 1408 vol 18 october 2017 articles soft - tissue sarcoma in recent years . 
clinicians might be better at selecting patients most likely to benefit from palliative chemotherapy for advanced soft - tissue sarcoma , and are treating patients more aggressively in terms of minimising dose reductions and treatment delays , with greater use of supportive medications such as growth factors . 
a further factor might be increasing use of local therapies such as radiotherapy and surgery for patients with metastatic disease , which has been associated with longer overall survival than for patients not receiving such therapies.30 indeed , 57 patients on the geddis trial went on to receive surgery or radiotherapy after completing study treatment . the pharmacogenomics data obtained in the current study suggest that snps in the organic cation transporter slc22a16 are associated with reduced efficacy and decreased toxicity following doxorubicin treatment . 
 these findings are in keeping with previously published data from a breast cancer patient cohort and are consistent with a loss of function in the transporter that results in reduced intracellular influx of doxorubicin.20 validation of these effects in an independent cohort of sarcoma patients would be valuable to ascertain the potential for this snp to influence clinical decisionmaking . 
two other snps , slc29a1 rs9394992 and prdx4 rs518329 , were also associated with outcomes in the doxorubicin group ; however , these genes are not known to be involved in the pharmacology of doxorubicin , so further investigation is required to understand these effects . 
there were indications that three snps predicted to affect gemcitabine pharmacokinetics were associated with an effect on overall survival , most notably the cda rs2072671 snp , which was associated with reduced overall survival in the gemcitabine and docetaxel group , with worse survival in patients homozygous ( rather than heterozygous ) for the minor allele ( this is referred to as a gene - dose effect )  . 
however , the same snp was not associated with a difference in progression - free survival , and insufficient evidence is currently available to advocate routine testing of these snps to influence clinical decision - making . limitations of the current study include the fact that we used a gemcitabine and docetaxel schedule that used fewer cycles and lower doses than in the originally published schedule , 6 which is widely used in other countries . 
 although we had a clear rationale for this decision , nevertheless we acknowledge that some might conclude that this limits the applicability of the trial results to the wider population of patients with advanced soft - tissue sarcoma beyond our trial . 
additionally , more patients stopped treatment early on gemcitabine and docetaxel than doxorubicin , which might have reflected the fact that clinicians knew that patients could go on to receive doxorubicin , whereas the reverse was not true due to the limited availability of gemcitabine and docetaxel in the uk at that time outside of clinical trials . how should these results inform our discussions with patients with advanced soft - tissue sarcoma ? the data do not support superiority for gemcitabine and docetaxel over doxorubicin on survival outcomes . 
although the similar progression - free survival and overall survival of gemcitabine and docetaxel and doxorubicin might support a conclusion that either schedule can be used according to patient or clinician preference , our results indicate the need for caution with such an approach , in that gemcitabine and docetaxel is more difficult to deliver than doxorubicin , and patients find it more toxic than doxorubicin , with some effects on quality of life . 
thus , the overall clinical conclusion should be that doxorubicin remains standard of care as first - line treatment for locally advanced or metastatic softtissue sarcoma , and that gemcitabine and docetaxel is not recommended as routine first - line treatment . 
there might of course be occasions when different choices are made depending on patient factors and preferences , such as using combination doxorubicin and ifosfamide for selected patients who need to optimise chances of tumour shrinkage , or using gemcitabine and docetaxel in patients with cardiac dysfunction that contraindicates use of doxorubichowever , for most patients , these results will hopefully provide evidence for clinicians to consider with their patients when selecting first - line treatment for advanced soft - tissue sarcoma . 
the study also highlights the importance of doing randomised trials in rare cancers to rigorously compare new treatments with established standard treatments , rather than extrapolating promising results from smaller non - comparative trials . contributors geddis was developed through and supported by the uk national cancer research institute sarcoma clinical studies group and was led by the trial management group ( composed of bs , sjs , jw , ml , pjw , fc , cr , zw , sf , and sb )  . 
sf and sb were responsible for the conduct of the trial , ensuring all required approvals were in place , and for collection and verification of the integrity of the data . 
all authors gave final approval of the version to be published . declaration of interests bs has received honoraria and travel grants from novartis , pharmamar , ariad , clinigen , daiichi , and lilly . 
 jw , ml , fc , zw , cb , gjv , dj , kk , rt , sf , sn , and h - md declare no competing interests . acknowledgments we thank all patients participating in geddis and their families . 
 the geddis trial was funded by cancer research uk ( c2921 / a11561 ) , with separate funding obtained from sarcoma uk ( suk16.2015 ) to support the pharmacogenomics studies described . 
we thank ian judson ( royal marsden hospital , london , uk ; retired ) for his review of the manuscript and shonit punwani ( university college london , london , uk ) for his input into the central ct scan review . 
 crs work on the trial was supported at the kantonsspital st gallen by a grant of the clinical trials unit commission , ctu 12 / 14 . editorial for our earlier editorial on direct - to - consumer genetic testing see lancet oncol 2008 ; 9 : 1113 black - box warning : direct - to - consumer marketing on nov 22 , 2013 , the us food and drug administration ( fda ) ordered the company 23andme to immediately discontinue sale and marketing of its saliva collection kit and personal genome service , stating that it was being marketed without fda approval . 
23andme had recently begun a series of television adverts to market their test , which is billed as providing data on 254 diseases and conditions , including data on carrier status , health risk , and responses to drugs . 
the warning letter stated that the fda had received no assurances from the company that the personal genome service was analytically or clinically validated for its intended uses , and that the tests could put patients at risk when decisions are made on false positive or negative assessments for high - risk indications . 
for instance , the letter highlighted that a false positive result for a brcarelated risk assessment could lead a patient to undergo intensive prophylactic screening , or other morbidity - inducing actions , while a false negative result could result in a patient failing to recognise an actual risk that might exist . 
in response , 23andme have suspended marketing the product , and halted the provision of health - related results to new customers , although ancestry - related information and raw genetic data will still be provided . chemoprevention , surgery , these concerns are the crux of the issue with publicly available genetic tests . 
while genetic testing has a role in the clinic , the provision of complex genetic data to lay individuals , especially without access to expert genetic counselling , is a risky business . 
 further , it is premature to believe that we understand the overall genetic complexity of common diseases to the extent that we can accurately predict whether or not an individual will succumb to that condition in the long run . one must also consider what a consumer can actually do with the results of their genetic tests . 
although in a handful of situationseg , testing positive for brca1 / 2 with a strong family history of brca - related cancerradical steps can be taken to prevent or treat the disease , many conditions do not have such obvious courses of action . 
most frequently , the only possible recommendation for a patient would be to modify diet and lifestyle , but one could argue that this should be done by many people , irrespective of knowledge of their genetics . 
and would knowledge of the risk of an untreatable condition cause long - lasting anxiety , the adoption of a fatalistic attitude to bad news , or use of unproven interventions , perhaps at great personal expense ? as we have noted previously , is the ready availability of such information ethical , when little can be done with it , and could be the source of distress ? is also an instance , 23andmes database currently contains data for 400 000 people . 
 what guarantees does an individual have that this information will not nd its way to health insurers , resulting in in ated premiums or the refusal to grant coverage ? in an unauthorised data protection information issuefor to use inherent many of the fears raised by this particular issue are common to other direct - to - consumer marketed health products . 
 or is it perhaps time to ban outright product - speci c adverts of health - care products aimed directly at the consumer ? the lancet oncology vol 15 january 2014 corrections published online november 22 , 2013 s1470 - 2045 ( 13 ) 70328 - 0 correction to lancet oncol 2013 ; 14 : 1279 , 1283 , 1285 correction to lancet oncol 2013 ; 14 : 1330 , 1333 , 1335 yamada y , takahari d , matsumoto h , et al . 
 leucovorin , fluorouracil , and oxaliplatin plus bevacizumab versus s - 1 and oxaliplatin plus bevacizumab in patients with metastatic colorectal cancer ( soft ) : an open - label , non - inferiority , randomised phase 3 trial . 
this has been corrected online as of dec 30 , 2013 . correction to lancet oncol 2013 ; 14 : 1295306 zhang j - x , song w , chen z - h , et al . 
 docetaxel or pemetrexed with or without cetuximab in recurrent or progressive non - small - cell lung cancer after platinum - based therapy : a phase 3 , open - label , randomised trial . 
 lancet oncol 2013 ; 14 : 132636in the online first version of this article ( published online nov 12 ) , in table 3 , all entries of ( > 1% ) should have read ( < 1% ) , and the rst two sentences of the third paragraph on page 1335 should state : a subsequent analysis of flex showed a signi cant association between egfr expression by immunohistochemistry and improved outcomes , with high egfr expression ( h - score 200 or higher ) being associated with improved overall survival , time - to - treatment failure , and a greater proportion of patients achieving objective responses when treated with cetuximab than when treated with cisplatin plus vinorelbine alone.13 there was no improvement in outcomes in the low h - score group ( h - score lower than 200 ) .13 these corrections were made to the print version of the article in the december issue of the journal , and have been made online as of nov 22 , 2013 . 
in table 1 , the entry for adenocarcinoma in the cetuximab and pemetrexed group should have read 161 ( 53% ) and the entry for all other diagnoses in the pemetrexed group should have read 41 ( 13% )  . 
in table 3 , in the cetuximab plus pemetrexed group , the entry for patients with one or more ctcae grades 12 should have read 89 ( 30% ) , that for grade 3 anaemia 16 ( 5% ) , for grade 4 infusion related reactions 5 ( 2% ) , and grade 3 lung infection 16 ( 5% )  . 
 in the pemetrexed group in the same table , the entry for patients with one or more grade 4 ctcae should have read 36 ( 12% ) and one or more grade 5 ctcae 10 ( 3% ) ; the entry for grade 12 diarrhoea should have read 36 ( 12% ) , that for grade 12 hyperglycaemia 10 ( 3% ) , and grade 12 maculopapular rash 39 ( 13% )  . 
use of parenteral oestrogen could avoid the long - term complications associated with lhrha and the thromboembolic complications associated with oral oestrogen . methods in this multicentre , open - label , randomised , phase 2 trial , we enrolled men with locally advanced or metastatic prostate cancer scheduled to start inde nite hormone therapy . 
randomisation was by minimisation , in a 2 : 1 ratio , to four self - administered oestrogen patches ( 100 g per 24 h ) changed twice weekly or lhrha given according to local practice . 
the primary outcome , cardiovascular morbidity and mortality , was analysed by modi ed intention to treat and by therapy at the time of the event to account for treatment crossover in cases of disease progression . 
after a median follow - up of 19 months ( iqr 1231 ) , 24 cardiovascular events were reported , six events in six ( 71% ) men in the lhrha group ( 95% ci 27149 ) and 18 events in 17 ( 101% ) men in the oestrogen - patch group ( 60156 )  . 
mean 12 - month changes in fasting glucose concentrations were 033 mmol / l ( 55% ) in the lhrha group and 016 mmol / l ( 24% ) in the oestrogen - patch group ( p = 0004 ) , and for fasting cholesterol were 020 mmol / l ( 41% ) and 023 mmol / l ( 33% ) , respectively ( p < 00001 )  . 
other adverse events reported by 6 months included gynaecomastia ( 15 [ 19% ] of 78 patients in the lhrha group vs 104 [ 75% ] of 138 in the oestrogen - patch group ) , hot ushes ( 44 [ 56% ] vs 35 [ 25% ] ) , and dermatological problems ( 10 [ 13% ] vs 58 [ 42% ] )  . interpretation parenteral oestrogen could be a potential alternative to lhrha in management of prostate cancer if e cacy is con rmed . 
on the basis of our ndings , enrolment in the patch trial has been extended , with a primary outcome of progression - free survival . funding cancer research uk , mrc clinical trials unit . introduction around 900 000 men worldwide are diagnosed as having prostate cancer every year , 1 and more than 40% receive androgen - deprivation therapy ( adt ) within 6 months of diagnosis.2 adt is the standard treatment for metastatic disease , but is also used at earlier stages as adjuvant and neoadjuvant therapy in men who require radical treatment for localised disease and for those with rising concentrations of prostate - speci c antigen ( psa ) who are at high risk of distant metastases.3 the immediate e ects of castration are loss of male secondary sexual characteristics , impotence , muscle weakness , and changes in body composition.4 this leads treatment these drugs are associated with long - term toxic e ects , including de creased bone - mineral density , 5 , 6 osteoporotic fractures , 710 adverse metabolic changes , 11 and diabetes.10 , 12 , 13 whether cardio vascular complications is unclear because evidence is inconsistent . 
includes a small number of individuals ( maximum 3 ) who had been assumed not to be receiving treatment at an earlier time ( eg , owing to low oestradiol concentrations , reported di culty in using op , or missed appointments )  . 
oral oestrogen ( eg , diethylstilbestrol ) was used for adt before the development of lhrha , but is no longer used routinely because it is associated with an increased risk of thrombotic complications15 attributed to the e ects of rst - pass hepatic metabolism on coagulation lipids.16 administration of oestrogen proteins and parenterally ( intravenously , transcutaneously ) avoids rst - pass hepatic metabolism and , therefore , is not expected to be associated with the same thrombotic complications as oral oestrogen.16 , 17 parenteral oestrogen could , therefore , be a potential intramuscularly , therapeutic alternative to lhrha . 
we did the prostate adenocar cinoma : transcutaneous hormones versus luteinising agonists ( patch ) ran domised , phase 2 trial to assess the safety and activity of transdermal oestrogen patches in the treatment of prostate cancer . hormone - releasing hormone methods patients eligible men had locally advanced or metastatic prostate cancer ( including those previously treated with radical intent with rising concentrations of psa ) and scheduled to start continuous inde nite hormone therapy at multiple hospitals in the uk . 
other baseline investigations were physical examinations ( including blood pressure ) , bone scans , ct or mri at the discretion of the physician , and blood including measurement of psa concentration . 
cardiovascular exclusion criteria were stroke or transient ischaemic attack within the previous 2 years ; radiologically con rmed deep - vein thrombosis or tests , pul monary embolism at any time ; myocardial infarction in the 6 months before the study or more than 6 months previously with evidence of q - wave infarction on electrocardiography at screening ; angina ( new york heart association grade iii or higher ) in the previous year ; symptoms of heart failure ( new york heart association grade iii or higher ) ; pulmonary oedema evident on chest radiography at screening ; left - ventricular ejection fraction of 40% or lower in patients with a history of ischaemic heart disease or heart failure ; and systolic blood pressure of 160 mmhg or higher and , diastolic blood pressure of 100 mmhg or higher , or both , in men . 
other exclusion criteria were previous systemic therapy or previous or current malignant disease or cardiovascular disease thought likely to compromise the patients ability to tolerate therapy or a ect assessment . the protocol was approved by national regulatory and ethics committees and participating hospitals obtained the appropriate local approvals . 
randomisation was done centrally at the trials unit , according to a computer - based minimisation algorithm with a random element ( 80% ) balanced for the following factors : disease stage , age , smoking status , personal or family history of heart disease , and which lhrha agent was to be used . 
the trial was open - label , but reviewed by an primary outcome events were that was independent endpoint review committee unaware of treatment allocation . procedures initially , patients in the oestrogen - patch group received three patches ( 100 g per 24 h ) to be self - administered and changed twice weekly for 4 weeks . 
the number of patches was reduced to two twice weekly if castrate testosterone concentrations in serum of 17 nmol / l or lower were achieved ( regimen one )  . 
this biweekly regimen was based on previous data18 and was intended to be practical and to achieve castrate testosterone concentrations quickly and maintain thethe rst review by the independent data monitoring oestradiol concentrations were lower and testosterone responses were less frequent than anticipated . 
the regimen was changed , therefore , to four patches to be changed twice weekly for 4 weeks , followed by use of three patches twice weekly when the target castrate testos terone concentration in serum was reached ( regimen two ) .19 patients with testosterone concentrations higher than castrate levels at 4 weeks remained on the induction regimen and had testosterone checked every 2 weeks . 
lhrha was prescribed according to local practice and could be accompanied by a short course of antiandrogens to treat committee showed that 308 vol 14 april 2013 articles intention - to - treat analysis * treatment at time of event lhrha ( n = 84 ) op ( n = 169 ) lhrha 18 ( 5 ) 17 ( 10% ) 15 ( 4 ) 15 9 ( 2 ) 3 ( 1 ) 6 ( 1 ) 4 ( 1 ) 1 ( 1 ) 4 ( 1 ) 107 3 ( 1 ) 5 ( 2 ) 2 ( 0 ) 5 ( 1 ) 3 ( 0 ) 3 ( 1 ) 1 ( 1 ) 2 ( 0 ) 71% ( 27149 ) 101% ( 60156 ) cardiovascular events number of events ( fatal events ) number of patients type of event ( fatal events ) heart failure acute coronary syndrome thromboembolic stroke other arterial embolic events venous thromboembolism rate of events per 100 patients proportion ( exact binomial 95% ci ) of patients with events ( % ) total reviewed events that did not satisfy outcome de nitions 6 ( 1 ) 6 ( 7% ) 2 ( 1 ) 1 ( 0 ) 3 ( 0 ) lhrha = luteinising - hormone - releasing - hormone agonists . 
 * in the modi ed intention - to - treat population , patients were included in the op group if they had been treated with op at any point ; patients were included in the lhrha group if they had been treated with an lhrha and had not received op at any point . 
a sample size of 200 patients , of whom 133 would be randomised to receive oestrogen patches , was calculated to be large enough to estimate the cardiovascular event rate in the oestrogen - patch group with reasonable precision . 
if strong evidence of a 15% or higher cardiovascular - event rate in the oestrogenpatch arm was seen ( based on the lower limit of a 95% ci ) , an early review by the independent data monitoring committee would be triggered and trial closure could be considered . 
the numbers of events required to trigger a review were ten or more in the rst 33 patients assigned oestrogen patches , 17 in 67 patients , 23 in 100 patients , and 29 in 133 patients . the primary cardiovascular analysis was based on modi ed intention - to - treat principles : patients were assessed in the oestrogen - patch group if they had been treated with patches at any point , and assessed in the lhrha group if they had received lhrha but not patches at any point ; patients who received no treatment at all were excluded . 
in cases of disease progression , patients could be given second - line therapy at the discretion of the treating clinician , including changing to the non - assigned study treatment . the primary outcome measure was cardiovascular morbidity and mortality , according to the following prespeci ed de nitions : new symptoms or clinical signs of decompensated cardiac failure , supported by chest radiography , echocardiography , or a rise in concentration of brain natriuretic peptide ; acute coronary syndrome ( including unstable angina , non - st - segment - elevation myocardial infarction , and myocardial infarction ) presenting as new - onset cardiac chest pain , collapse , or shortness of breath , and con rmed as ischaemic in origin by electrocardiography , troponin rise , coronary angiography , or a combination of these tests ; new neurological symptoms and signs of a cerebrovascular accident , con rmed by brain ct or mri or by clinical diagnosis and carotid duplex scanning for transient ischaemic attacks , with evidence of pre - existing or new , persistent or paroxysmal atrial brillation ; new clinical symptoms supported by radiological evidence of other thromboembolism arterial embolic events ; venous con rmed by ultra sonography , venography , or both , or pulmonary em bolism con rmed by ct pulmonary angiogram , ventilation - perfusion scans , or angi ography ; and other relevant events ( deaths attributed to one of these cardiovascular causes without supporting documentation , or events that did not meet the exact de nitions but were judged appropriate for inclusion by the independent reviewers )  . cardiac events were reported by investigators at 3 and 6 months and 6 - monthly thereafter on a speci cally designed form or identi ed from reports of serious adverse events and routinely collected data on toxic e ects . 
two independent reviewers unaware of original treatment allocation or current treatment being received reviewed original documentation and decided which events met the primary outcome de nitions and whether or not they were related to hormone therapy . 
discrepancies in classi cation were resolved by discussion , assessment of further clinical information , or both . events , adverse changes including secondary outcomes were hormone responses and other cardiovascular risk factors ( concentrations of fasting glucose , fasting total cholesterol , and hdl cholesterol , weight , and blood pressure ) and other toxic e ects . 
owing to distribution , data are presented as median ( 5th and 95th percentiles ) at baseline and 6 months , median change ( range ) , and median percentage change . 
 log - transformed values were used for the ancova model . table 3 : cardiovascular risk factors in men who remained on randomised treatment without additional therapy patients who experienced an event is reported with exact binomial 95% cis . 
as crossover was allowed in the case of disease progression , we did a planned sensitivity analysis in which we included numbers of events according to treatment being taken at the time of ( or within 30 days before ) the events . 
analysis of the primary outcome was planned for 3 months after the last randomisation to enable a prompt decision regarding continuation of the study , whereas assessment of the secondary outcomes were done 15 months after the last randomisation to enable assessment of changes over time . 
men with oestradiol concentrations of 250 pmol / l or lower , or who were reported to have stopped using patches ( where oestradiol data were not available ) were not assessed . 
all analyses were done with stata statistical software ( version 12 )  . 310 vol 14 april 2013 articles in this study , we report data from the preplanned the rst analysis of cardiovascular outcomes 254patients . 
on the basis of recommendations from the independent data monitoring committee , the study was extended to assess progression - free survival in 660 men ( including this initial cohort )  . 
rel , fhc , scf , and rcj had access to the raw data , and processed data released by the independent data monitoring committee were available to all authors . 
rel , fhc , and pda were jointly responsible for the decision to submit for publication . treatment results between april 7 , 2006 , and april 28 , 2010 , 254 patients from 27 uk centres were enrolled , 169 into the oestrogenpatch group ( 33 regimen one , 136 regimen two ) and 85 into the lhrha group . 
median age was 74 years ( iqr 6979 ) , 91 ( 36% ) patients had metastatic disease , 236 ( 93% ) had who performance status scores of 0 or 1 , 142 ( 56% ) were current or previous smokers , and 70 ( 28% ) were longterm regular aspirin users . 
five ( 2% ) men had undergone radical radiotherapy ( three in the oestrogen - patches group and two in the lhrha group )  . at 3 months , among men who were still receiving their allocated treatment without additional therapy , 70 ( 93% ) of 75 with data available in the lhrha group and 111 ( 92% ) of 121 receiving oestrogen patches under regimen two had testosterone concentrations of 17 nmol / l or less . 
the castration rate in the lhrha group did not di er by agonist used ( 28 [ 93% ] of 30 for leuprorelin , 41 [ 93% ] of 44 for goserelin , and one [ 100% ] of one for triptorelin )  . 
testosterone concentrations of 11 mmol / l or lower were seen in 53 ( 71% ) of 75 , 94 ( 78% ) of 121 , and 14 ( 48% ) of 29 men who received lhrha , oestrogen - patch regimen two , and oestrogenpatch regimen one , respectively , and concentrations of 07 nmol / l or lower were seen in 44 ( 59% ) of 75 , 75 ( 62% ) of 121 , and nine ( 31% ) of 29 . at 6 months , 68 ( 88% ) of 77 patients with available data had testosterone concentrations of 17 nmol / l or lower in the lhrha group , compared with 106 ( 95% ) of 112 in the oestrogen - patch group receiving regimen two lhrha ( n = 55 ) ( n = 107 ) lhrha ( n = 54 ) ( n = 95 ) lhrha ( n = 59 ) ( n = 119 ) lhrha ( n = 55 ) ( n = 101 ) 6 months 12 months 6 months 12 months time time figure 2 : changes in fasting glucose ( a ) and total cholesterol ( b ) concentrations in patients still receiving treatment at 6 and 12 months patients were not receiving additional therapy . 
 testosterone breakthrough was seen at 6 months in six ( 9% ) of 68 in the lhrha group and four ( 4% ) of 104 in the oestrogen - patch group ( regimen two ) who had had castrate concentrations at 3 months . 
oestradiol concentrations higher than 250 pmol / l indicated that adherence to treatment with oestrogen patches was generally good , and at 3 months most ( 117 [ 96% ] of 122 ) men randomised to receive oestrogen - patch regimen two had changed to the maintenance regimen of three patches ; two ( 2% ) were using two patches and three ( 2% ) were using four patches . median follow - up for cardiovascular events was 19 months ( iqr 1231 , minimum 3 months )  . 
55 potential events were identi ed among patients in the modi ed intention - to - treat cohort , of which 24 met the outcome de nitions ( table 2 )  . 
the number of patients with an event in the lhrha group was six ( 71% ) of 84 ( 95% ci 27149 , six events ) and in the oestrogen - patches group was 17 ( 101% ) of 169 ( 60156 , 18 events )  . 
13 ( 72% ) of the 18 events in the oestrogen - patch group and four ( 67% ) of the six in the lhrha group were deemed possibly related to the allocated trial treatment by one or both independent reviewers . 
 in the oestrogen - patch group , 13 of the 18 cardiovascular events occurred in 12 men who were receiving regimen two . six ( 25% ) of the 24 cardiovascular events were fatal , of which three were thought to be possibly related to the study treatment by the independent reviewers : a thromboembolic stroke in a man assigned to oestrogen patches and using them at the time of the event ( 36 months ) ; a myocardial infarction in a man assigned to lhrha and receiving it at the time of the event ( 2 months ) ; and a pulmonary embolism in a man assigned to oestrogen patches who had switched to lhrha 16 months before death . 
one further death potentially related to treatment was reported up to july , 2011an acute myocardial infarction in a patient who was assigned to lhrha and had continued to take that treatment until death ( 33 months )  . 31 events were deemed not to meet the primaryoutcome de nitions : non - cardiac chest pain or investigation for a silent myocardial infarction that was not con rmed ( n = 6 ) ; symptoms that might indicate congestive cardiac failure or venous thromboembolism , such as dyspnoea or leg swelling , but for which the causes were not con rmed ( n = 5 ) ; other cardiac events , including atrial brillation , hypotension , hypertension , ( continued from previous column ) chest pain other lhrha ( n = 78 * ) op regimen one ( n = 26 ) op regimen two ( n = 112 ) 73 ( 94% ) 26 ( 100% ) 110 ( 98% ) 4 ( 5% ) 1 ( 1% ) 55 ( 71% ) 21 ( 27% ) 2 ( 3% ) ( palpitations , hyperglycaemia ) 1 ( 1% ) 1 ( 1% ) 18 ( 69% ) 7 ( 27% ) 1 ( 4% ) ( urinary retention ) 89 ( 79% ) 22 ( 20% ) 1 ( 1% ) ( angioplasty ) lhrha = luteinising - hormone - releasing - hormone agonists . 
 table 4 : toxic e ects reported up to 6 months in men who remained on assigned treatment without additional therapy and non - embolic peripheral vascular disease ( n = 11 ) ; other medical events ( n = 4 ) ; and symptoms associated with an outcome event that did not constitute a separate event ( n = 5 )  . in men who were still receiving the allocated treatment without additional therapy at 6 months , mean fasting glucose had increased in the lhrha group and decreased in the oestrogen - patches group , which led to a signi cant di erence between groups ( table 3 , gure 2 )  . 
 in men who remained on assigned treatments at 12 months , fasting glucose concentrations increased further in the lhrha arm but remained similar in the oestrogen - patches group , with the mean changes from baseline being 033 mmol / l ( 55% ) and 016 mmol / l ( 24% ) , respectively ( p = 0004 )  . mean fasting cholesterol concentration increased in the lhrha group at 6 months , compared with a small decrease in recipients of oestrogen patches ( table 3 , gure 2 )  . 
at 12 months , the mean value was similar to that at 6 months in the lhrha group ( 531 mmol / l ) , but had decreased further in the oestrogen - patches group ( 456 mmol / l )  . 
by contrast , hdl cholesterol concentrations had in creased to a similar degree in the two groups at 6 months and 12 months ( table 3 )  . changes mean weight had increased by similar amounts in the two treatment groups at 6 months ( table 3 ) and 12 months . 
diastolic blood pressure had increased in the lhrha group at 6 months and decreased in the oestrogen - patches group , but changes were small , as were changes in systolic blood pressure ( table 3 )  . 
these data were supported by those for adverse e ects , with only a few reports being made of substantial changes in weight or blood pressure ( table 4 )  . 
values for cardiovascular risk factors were similar after exclusion of patients randomised to regimen one of the oestrogen patches . other adverse events were largely as expected , and were generally mild in the two treatment groups ( table 4 )  . 
 as anticipated , the most frequently reported symptoms at 6 months in men still receiving their allocated treatment were related to sexual function , and , in some cases were severe ( table 4 )  . 
gynaecomastia was reported on both treatments , but was more frequently reported in the oestrogen - patch group than in the lhrha group , and in a small number of cases was symptomatic . 
minor dermatological problems associated with use of oestrogen patches were reported for 58 ( 42% ) of 138 men , compared with ten ( 13% ) of 78 in the lhrha group . 
in the two groups all reported symptoms were grade 12 and included pruritis , erythema , in skin pigmentation eczema , urticaria , change ( oestrogen - patches group only ) , and hair changes vol 14 april 2013 articles panel : research in context systematic review in a systematic review , 20 randomised controlled trials of parenteral oestrogen in patients with prostate cancer were identi ed from electronic databases , including medline , embase , and the cochrane central register of controlled trials , with no restrictions on language or publication date.27 relevant published papers and internet resources , such as trial and national drug registries , were also searched . 
the review found no consistent evidence that parenteral oestrogen given at doses su cient to produce castrate testosterone concentrations di ered from luteinisinghormone - releasing - hormone agonists in terms of prostatecancer , cardiovascular , or overall mortality . 
transdermal oestrogen patches had shown promise in terms of activity and toxic - e ect pro les in the treatment of locally advanced or metastatic prostate cancer in a single - arm pilot study.21 interpretation our study provides evidence that castrate testosterone concentrations similar to those seen in patients taking luteinising - hormone - releasing - hormone agonists can be achieved with transdermal oestrogen . 
rates of cardiovascular toxic e ects were similar with the two treatments and were lower than those seen with oral oestrogen.15 the study also provides data on metabolic changes associated with the two treatments . 
some men reported more than one symptono grade 4 or 5 adverse events had been reported by 6 months and , with the exception of the cardiovascular events noted above , no other potentially treatment - related deaths had been reported in this cohort to july , 2011 . discussion our results show that parenteral oestrogen administered via patches can lead to castrate testosterone concentrations similar to those achieved with lhrha in men with locally advanced and metastatic prostate cancer . 
 these ndings con rm the results of a small pilot study.21 in our study , which excluded patients with high baseline risks of cardiovascular events , the rate of cardiovascular complications in men receiving oestrogen patches was similar to that in men receiving lhrha . 
additionally , it was lower than rates observed with oral oestrogen by the veterans admin istration cooperative urological research group.15 , 22 our modi ed intention - to - treat analysis of cardiovascular events seems to have been conservative , because several events attributed to the oestrogen - patches group occurred in men who had received oestrogen therapy for only a short period , or who had stopped treatment for a long time before the event occurred , or both . 
data on disease progression and survival are not yet available because e cacy will be assessed in the extended trial . an important strength of this study is the independent , masked review of cardiovascular events . 
several large population - based studies have reported associations between treatment with lhrha and increased incidence of fatal and non - fatal cardiovascular events , 12 , 13 , 23 , 24 but other studies have shown no such relation.10 , 25 a meta - analysis of eight randomised trials involving 4141 patients with median follow - up durations of 76132 years compared im mediate versus no or delayed lhrha treatment in men with non - metastatic prostate cancer . 
cardiovascular mortality of 11% was reported and did not di er between groups ( relative risk 093 , 95% ci 079110 ) .26 data were extracted from inconsistencies in de nitions of events and assessment procedures . 
e ects on non - fatal events , time to cardiovascular death , and potential di erences relating to pre - existing cardiovascular disease were not assessed . trial reports and were subject use of parenteral oestrogens to treat prostate cancer has been reviewed previously ( panel ) .27 parenteral oestrogen administration should avoid the venous thrombotic risk associated with oral administration while providing the arterial bene ts attributed to oestrogen.28 a series of trials in scandinavia intramuscular assessed use polyoestradiol . 
biochemical progression , cancer - speci c survival , cardiac mortality , and overall mortality did not di er between treatment groups.29 men were excluded on the basis of cardiovascular risk only if they had had myocardial or cerebral infarction within the preceding month . 
cardiovascular morbidity was higher in both groups among those who had a history of major cardiovascular disease than in those who did not , but the di erence was greater in the polyoestradiol group.30 we did not assess di erences by pre - existing cardiovascular risk , but such analysis will be possible in the larger cohort of the extended trial . the other important nding in the polyoestradiol study was , as predicted , a protective e ect of oestrogen on bone health : 18 serious skeletal events were reported in the group undergoing combined androgen deprivation versus none in the polyoestradiol group ( p = 0001 ) .29 osteoporosis and associated events are important and costly side - e ects of lhrha.7 , 9 strategies to mitigate lhrha - induced bisphosphonates , targeting of rankl ( with , for example , denosumab ) , and use of selective oestrogen - receptor modulators . 
all these ap proaches , however , are expensive , but would potentially be unwarranted if an e ective method of achieving androgen deprivation without associated bone loss were available . 
the extended patch trial will investigate the e ects of lhrha and oestrogen patches on bone health by assessment of fractures and bone - mineral density . include bone loss use 314 vol 14 april 2013 articles see online for appendix increases our ndings that fasting total cholesterol , hdl cholesterol , and fasting glucose con centrations in serum increased in patients receiving lhrha are in keeping with previous reports.11 , 31 during the rst year of treatment with lhrha , increases of total cholesterol concentrations by 510% and of hdl cholesterol by 612% have been reported in several small studies.3134 observed increases in fasting glucose concentrations by 12% have also been seen in short - term ( 12 - week ) studies , 35 , 36 and larger changes have been seen in one longer - term study.34 these results are again consistent with our ndings ( increases of 2% and 6% in fasting glucose concentrations at 6 and 12 months , respectively )  . 
the metabolic abnormalities associated with use of lhrha have similarities to those in in obesity and the metabolic syndrome : concentrations of total and ldl cholesterol and triglycerides , and decreases in lean mass and insulin sensitivity.11 the e ects with lhrha , however , also include increases in hdl cholesterol concentrations and subcutaneous fat , but no e ect on blood pressure is seen.37 the changes we noted in lipid pro les in the oestrogenpatches group are in keeping with the known bene cial arterial e ects of oral and parenteral oestrogen therapy , 28 , 38 and the decrease in glucose concentrations is consistent with the bene cial e ects of oestradiol on pancreatic - cell function.39 a limitation of our analysis , however , is that data on triglycerides and ldl cholesterol were not collected . 
changes in concomitant medication that might a ect lipid pro les were also not recorded , but , as this was a randomised study , it is likely that these e ects would have been balanced across the arms . 
as the trial was not powered to compare changes in metabolic factors , results should be con rmed in future trials . other adverse e ects with the two treatments were largely as expected and were generally mild . 
thus , e ects on wider features , such as cognition and quality of life in particular , require more detailed investigation . oestrogen patches seem to be a potential alternative to lhrha for men with prostate cancer . 
patches o er a low - cost , single therapy that can be self - administered , and which might avoid some of the side - e ects associated with lhrha . 
for individual patients treatment decisions will need to be balanced and take into account antitumour e ects , risks of cardiovascular events , e ects on bone health , quality of life , including sexual dysfunction , and possible glucose fasting either negative e ects on cognition . 
overall , though , the need to prioritise the assessment of a potential method of androgen deprivation that could avoid the toxic e ects associated with standard therapy , and to avoid the addition of new and expensive agents to counteract them , is clear . contributors rel , mkbp , and pda developed the trial and oversaw study conduct . 
rel , aaa , rk , nwc , hgk , and pda provided clinical advice and oversight , sdr provided advice on cardiovascular features , and ifg provided advice on endocrine features . 
all authors reviewed and approved the nal version . con icts of interest hgk has received a speaker fee ( honorarium ) from takeda uk for a presentation at the british association of urological surgeons annual meeting , which was unrelated to the patch trial . 
the other authors declare that they have no con icts of interest . acknowledgments the patch trial is sponsored by imperial college london and funded by cancer research uk ( cruk / 06 / 001 , c17093 / a5343 ) , with additional support from the medical research council clinical trials unit . 
 we also thank the trial steering committee ( david guthrie [ chair ] , john chester , richard cowan , and john schole eld ) , the data monitoring committee ( peter hoskin [ chair ] , philip smith , and laurence collette ) , and the endpoint review committee ( alastair ritchie and adam de belder )  . correction to lancet oncol 2016 ; 17 : 23442 correction to lancet oncol 2016 ; 17 : e506 shaw at , gandhi l , gadgeel s , et al , on behalf of the study investigators . 
 lancet oncol 2016 ; 17 : e50209the fourth sentence of the biosimilar monoclonal antibodies in oncology section should have read , the primary endpoint , overall response rate , at week 24 was equivalent between groups ( 70% for myl - 1401o vs 64% for trastuzumab ) , and the risk ratio was 109 ( 90% ci 097121 )  . 
this correction has been made to the online version as of march 1 , 2017 . vol 18 march 2017 e134 corrections corrections correction to lancet oncol 2013 ; 14 : e337 correction to lancet oncol 2013 ; 14 : e436 soares m , salluh jif . 
lancet oncol 2013 ; 14 : e436in this correspondence , the authors names should read athanassios kyrgidis , thrasivoulos - george tzellos , anastasia trigoni , stefanos triaridis and their a liations as 1st department of otolaryngologyhead & neck surgery ( ak , st ) and department of clinical pharmacology ( tgt ) , aristotle university of thessaloniki , thessaloniki , greece ; hospital for skin and venereal diseases , thessaloniki , greece ( at )  . 
 these corrections have been made as of oct 28 , 2013 . vol 14 november 2013 e493 corrections correction to lancet oncol 2013 ; 14 : 1205 oncol remke lancet ramaswamy bou et e , et al . 
 2013 ; 14 : 120007in table 3 of this article ( published online first on oct 17 , 2013 ) , the data in the mixed and metastatic columns for group 4 patients in cohort 2 were reversed ; the data for mixed recurrence should have been 2 ( 8% ) and for metastatic recurrence should have been 19 ( 76% )  . 
additionally , in table 4 , the data in the mixed and metastatic columns for group 4 patients were also reversed ; in patients who received chemotherapy the data for mixed recurrence should have been 2 ( 25% ) and for metastatic recurrence should have been 3 ( 38% ) , and in patients who received csi with or without chemotherapy , the data for mixed recurrence should have been 12 ( 20% ) and for metastatic recurrence should have been 43 ( 73% )  . 
 vol 15 april 2014 e154 articles lancet oncol 2014 ; 15 : 11422 published online december 11 , 2013 s1470 - 2045 ( 13 ) 70539 - 4 this online publication has been corrected . 
the corrected version rst appeared at thelancet.com / oncology on january 27 , 201 see comment page 15 * these authors contributed equally these authors contributed equally velindre cancer centre , velindre hospital , cardi , uk ( prof p barrett - lee md , j abraham frcr ) ; wales cancer trials unit ( a casbard msc , h timmins bsc , g griths phd ) and south east wales trials unit ( prof k hood phd ) , cardi university , cardi , uk ; cancer research uk / yorkshire cancer research she eld cancer research centre , weston park hospital , she eld , uk ( prof r coleman md ) ; cancer research uk clinical unit , southampton general hospital , southampton , uk ( p simmonds fracp ) ; royal cornwall hospitals nhs trust , truro , uk ( d wheatley frcr ) ; arden cancer centre , university hospitals coventry & warwickshire , coventry , uk ( r grieve frcr ) ; and royal adelaide hospital , adelaide , sa , australia ( n murray dphil ) correspondence to : angela casbard , wales cancer trials unit , college of biomedical and life sciences , cardi university , neuadd meirionnydd , heath park , cardi cf14 4ys , uk casbardac@cardi .ac.uk oral ibandronic acid versus intravenous zoledronic acid in treatment of bone metastases from breast cancer : a randomised , open label , non - inferiority phase 3 trial peter barrett - lee * , angela casbard * , jacinta abraham , kerenza hood , robert coleman , peter simmonds , hayley timmins , duncan wheatley , robert grieve , gareth gri ths , nick murray summary background bisphosphonates are routinely used in the treatment of metastatic bone disease from breast cancer to reduce pain and bone destruction . 
in the zice trial , we compared oral ibandronic acid with intravenous zoledronic acid for the treatment of metastatic breast cancer to bone . methods this phase 3 , open - label , parallel group active - controlled , multicentre , randomised , non - inferiority phase 3 study was done in 99 uk hospitals . 
patients with ecog performance status 0 to 2 and clinical decision to treat with bisphosphonates within 3 months of randomisation were randomly assigned to receive 96 weeks of treatment with either intravenous zoledronic acid at 4 mg every 34 weeks or oral ibandronic acid 50 mg daily . 
randomisation was strati ed on whether patients had current or planned treatment with chemotherapy ; current or planned treatment with hormone therapy ; and whether they had a previous skeletal - related event within the last 3 months or had planned radiotherapy treatment to the bone or planned orthopaedic surgery due to bone metastases . 
annual rates of skeletal - related events were 0499 ( 95% ci 04540549 ) with ibandronic acid and 0435 ( 03930480 ) with zoledronic acid ; the rate ratio for skeletal - related events was 1148 ( 95% ci 09671362 )  . 
the upper ci was greater than the margin of non - inferiority of 108 ; therefore , we could not reject the null hypothesis that ibandronic acid was inferior to zoledronic acid . 
more patients in the zoledronic acid group had renal toxic e ects than in the ibandronic acid group ( 226 [ 32% ] of 697 vs 172 [ 24% ] of 704 ) but rates of osteonecrosis of the jaw were low in both groups ( nine [ 1% ] of 697 vs ve [ < 1% ] of 704 )  . 
the most common grade 3 or 4 adverse events were fatigue ( 97 [ 14% ] of 697 patients allocated zoledronic acid vs 98 [ 14% ] of 704 allocated ibandronic acid ) , increased bone pain ( 91 [ 13% ] vs 85 [ 12% ] ) , joint pain ( 41 [ 6% ] vs 38 [ 5% ] ) , infection ( 31 [ 5% ] vs 23 [ 3% ] ) , and nausea or vomiting ( 38 [ 5% ] vs 41 [ 6% ] )  . interpretation our results suggest that zoledronic acid is preferable to ibandronic acid in preventing skeletal - related events caused by bone metastases . 
however , both drugs have acceptable side - e ect pro les and the oral formulation is more convenient , and could still be considered if the patient has a strong preference or if di culties occur with intravenous infusions . funding roche products ltd ( educational grant ) , supported by national institute for health research cancer network , following endorsement by cancer research uk ( cruke / 04 / 022 )  . introduction bone metastases cause major morbidity in metastatic breast cancer . 
introduction of bisphosphonate therapy has led to a substantial reduction in the incidence of skeletal - related events in metastatic breast cancer.1 the third - generation bisphosphonate , zoledronic acid , given by 4 weekly intravenous infusion , has been shown to be better than intravenous pamidronate , lowering the skeletal morbidity rate ( smr , number of skeletal - related events per year ) by 25% , and the risk of skeletal complications by 16% in a multiple - event analysis ( a composite measure of both rate and frequency of skeletal - related events ) .2 during the past decade bisphosphonates , mainly zoledronic acid , have been widely used in the uk health system for the prevention of skeletal - related events in patients with metastatic 114 vol 15 january 2014 articles breast cancer to bone , and , despite the superior e cacy and convenience of the new drug denosumab , 3 are still in use today . alternative third - generation bisphosphonate ibandronic acid , is licensed in the uk for the prevention of skeletal - related events in patients with breast cancer and bone metastases and is available in both intravenous and oral formulations . 
monthly intravenous treatment is inconvenient for patients not otherwise needing to attend hospital , and imposes substantial health - care costs compared with a self - administered oral medication such as ibandronic acid . 
although ibandronic acid has been shown to be superior to placebo in the treatment of metastatic breast cancer to bone , 4 , 5 there had previously been no direct comparison of ibandronic acid with the standard of care , zoledronic acid . we report here the rst results of the zice trial , a randomised phase 3 trial designed to assess the noninferiority of oral ibandronic acid compared with intravenous zoledronic acid in preventing skeletal - related events in an unselected uk population of patients with breast cancer metastatic to bone . methods study design and patients in this open - label , multicentre , parallel group , noninferiority , randomised phase 3 trial , we enrolled patients with the following key eligibility criteria : male or female ; 18 years or older ; at least one radiologically con rmed bone metastasis from a histologically con rmed breast cancer ; clinical decision to treat with bisphosphonates within the 3 months before randomisation ; eastern cooperative oncology group ( ecog ) performance status ( ps ) 02 ; and written informed consent . 
key exclusion criteria included : cns metastases ; current active dental problems ; known active peptic ulcer ; pregnant or lactating ; creatinine clearance lower than 30 ml / min ( cockcroftgault ) ; serum bilirubin higher than 15 upper limit of normal ( uln ) or aspartate aminotransferase / alanine aminotransferase higher than 30 uln ; bisphosphonate therapy in the previous 6 months ; or history of bisphosphonate hypersensitivity . 
we originally designed the trial include patients diagnosed with multiple bone metastases within the 3 months before randomisation , but this criterion was later changed ( in august 2007 ) to include those with one metastasis and a decision to treat with bisphosphonates within 3 monthsthis change was to include all patients who would usually be treated with bisphosphonates and to include those that had a treatment delay caused by dental work . 
this patient group was similar to those recruited in previous trials assessing zoledronic acid and ibandronic acid . all patients gave written informed consent before study entry and the trial protocol was approved by the uk medicines and health - care products regulatory agency and a multi - centre research ethics committee . 
the full trial protocol can be accessed online . randomisation and masking eligible patients were randomly assigned ( 1 : 1 ratio ) to intravenous zoledronic acid or oral receive either ibandronic acid by use of a computer - generated randomisation list at the wales cancer trials unit ( wctu )  . 
randomisation was strati ed , within blocks of size four , according to whether the patient was currently receiving chemotherapy , hormone therapy , or had had a previous skeletal - related event within the last 3 months or had planned radiotherapy . 
concealed allocation was achieved by research nurses ( who recruited the patients ) the wctu , where randomisation and telephoning treatment allocation was done by a trial / data manager 1404 patients randomised for the trial protocol see zice / zice . 705 randomly assigned to ibandronic acid 699 randomly assigned to zoledronic acid 1 withdrew on same day as randomisation 2 withdrew on same day as randomisation 704 included in itt analysis 697 included in itt analysis 50 did not start treatment 37 withdrew 11 died 2 in follow - up 13 withdrew 25 did not start treatment 11 died 1 in follow - up 654 included in pp analysis 672 included in pp analysis during 96 week treatment : 199 discontinued ( 3 later found ineligible , 107 later died , 66 later withdrew consent , 23 remained in follow - up ) 65 intolerant * 67 patients choice * 113 clinicians decision * 27 non - compliance * 173 died before discontinuing during 96 week treatment : 180 discontinued ( 66 later died , 75 later withdrew consent , 39 remained in follow - up ) 51 intolerant * 57 patients choice * 98 clinicians decision * 19 non - compliance * 200 died before discontinuing 282 nished 96 week treatment 292 nished 96 week treatment after 96 week treatment : 7 discontinued ( 2 died , 2 withdrew consent , 3 remained in follow - up ) 130 died before discontinuing ( 1 later found ineligible ) 1 intolerant 1 patients choice 2 clinicians decision 1 non - compliance after 96 week treatment : 7 discontinued ( 1 died , 5 withdrew consent , 1 remained in follow - up ) 2 patients choice 2 clinicians decision 115 died before discontinuing 145 remained in follow - up 170 remained in follow - up figure 1 : trial pro le itt = intention to treat . 
 * not all patients gave a reason and more than one reason could be given . vol 15 january 2014 articles for the summaries of product characteristics see medicines.org.uk / emc / interacting with a computerised systethe study had an open - label design . procedures patients randomly assigned to zoledronic acid received 4 mg intravenously over a minimum of 15 min in at least 100 ml of saline every 4 weeks for 96 weeks . 
 patients with bone pain or hypercalcaemia at study entry , or during treatment , could receive one treatment with ibandronic acid 6 mg or three times 2 mg intravenously instead of the 50 mg daily tablet , if needed . 
oral vitamin d ( at least 400 iu ) and calcium ( at least 500 mg ) daily was strongly recommended for the duration of bisphosphonate treatment . in each group , dose modi cations for renal impairment ( creatinine clearance < 60 ml / min ) were made according to the then current summaries of product characteristics . 
 trial medication could be withheld for any reason for up to 4 weeks , but participants delaying treatment for more than 4 weeks other than for dental infection or treatment were deemed withdrawn from protocol treatment . osteonecrosis of the jaw is a known side - e ect of bisphos phonates . 
 we deemed cases of osteonecrosis of the jaw to be serious adverse events , and the study site con rmed those cases after being diagnosed by a dental or ear , nose , and throat surgeon . we did study assessments at baseline , at 34 week intervals up to week 12 , and every 12 weeks to 96 weeks . 
these included medical assessment , ecog status , full blood count and bio chemistry tests ( with cockcroft - gault creatinine clearance estimation ) , quality - of - life assessment ( qlq - c30 ) and pain score ( bried pain inventory [ bpi ] ) .6 plain radiographs of the thoracolumbar spine were obtained at baseline and 96 weeks . 
we also obtained previous details of breast cancer diagnosis and treatment , hormone - receptor status , her2 status , distribution of metastatic disease , and previous skeletalrelated events . the primary endpoint for non - inferiority was frequency and timing of skeletal - related events over 96 weeks . 
a skeletal - related event was a composite event de ned as one of : requirement for orthopaedic surgery , vertebroplasty , or radiotherapy to bone ; symptomatic vertebral fracture ; pathological non - vertebral fracture ; spinal - cord compression ; and hypercalcaemia of malignancy . 
this primary endpoint is similar to that used in previous trials , 116 vol 15 january 2014 articles although other trials included asymptomatic fractures identi ed on serial radiographs done at regular 34 monthly intervals but did not consider the e ect of repeated events . 
 secondary outcomes were time to rst skeletal - related event , percentage of participants with any skeletal - related event , pain or analgesic scores over 96 weeks , toxic e ects reported over 96 weeks , quality of life over 96 weeks ( ie , every 12 - week visit ) , overall survival at 96 weeks and 5 years , safety , and health resource use at 48 weeks and 96 weeks . 
an independent data monitoring committee reviewed trial progress , safety data , and completeness of data collection on at least a yearly basis . statistical analysis the primary aim of this study was to show that oral ibandronic acid was non - inferior to intravenous zoledronic acid in reducing the number and frequency of skeletalrelated events , and incorporated all skeletal - related events experienced by participants over the treatment period using an anderson - gill multiple - event analysis.7 this analysis adjusts for non - independent multiple events within the same patient in the 96 - week treatment period , which is achieved by applying a robust covariance matrix to construct the ci for the relative risk of multiple skeletalrelated event events . 
we aimed to show that oral ibandronic acid maintained at least 67% of the lower limit of the e ect of zoledronic acid versus placebo ( relative risk of placebo versus zoledronic acid 1275 and a log relative risk of 0243 ) , 8 based on the two - ci approach.9 the margin for non - inferiority was ( 1 067 ) 0243 = 008 , therefore equivalent to a maximum rate ratio for ibandronic acid - tozoledronic acid of 108 . 
we assumed that there was no di erential e ect on survival , 55% of patients survive 2 years , and a ( conservative ) annual event rate of 07 on zoledronic acid . 
1400 participants were required to allow for a dropout rate of up to 5% . ibandronic acid group ( n = 704 ) zoledronic acid group ( n = 697 ) any adverse event 674 ( 96% ) 667 ( 96% ) grade 12 grade 3 grade 4 grade 5 total ( % ) grade 12 grade 3 grade 4 grade 5 total ( % ) 10% frequency in either group fever or in uenza - like symptoms abdominal pain altered taste anaemia anorexia breathlessness constipation diarrhoea dry mouth dyspepsia fatigue headache hypocalcaemia hypomagnesaemia hypophosphatemia increased bone pain infection joint pain muscle pain oedema other pain nausea or vomiting pins and needles renal impairment 177 ( 25% ) 221 ( 31% ) 177 ( 25% ) 246 ( 35% ) 103 ( 15% ) 121 ( 17% ) 222 ( 32% ) 266 ( 38% ) 248 ( 35% ) 544 ( 77% ) 158 ( 22% ) 199 ( 28% ) 80 ( 11% ) 83 ( 12% ) 80 ( 11% ) 435 ( 62% ) 125 ( 18% ) 390 ( 55% ) 301 ( 43% ) 410 ( 58% ) 170 ( 24% ) 170 ( 24% ) 215 ( 31% ) 172 ( 24% ) 5 ( < 1% ) other adverse events of interest osteonecrosis of the jaw table 2 : toxic e ects in randomised patients data are number of patients experiencing the event ( highest grade reported )  . 
multiple events occurring within the same 21 day time period counted as one event , to ensure that linked events ( eg , surgery to repair a fracture ) were not counted as separate events ; this was in line with the statistical methods of the trial comparing zoledronic acid versus pamidronate10 and the denosumab trial.3 we used both a per - protocol analysis and an intention - to - treat analysis . 
the per - protocol analysis was the primary analysis and only included patients who started treatment by the 12 - week visit , and included events occurring up until the time of protocol treatment withdrawal ( plus 21 days ) or death . 
as a sensitivity analysis , we did the analysis excluding hypercalcaemia events , because hyper calcaemia is not always deemed to be a true bone - related event.11 risk dierence ( dierence in proportion ) events in ibandronic acid group events in zoledronic group fever or inuenza - like symptoms renal impairment anaemia headache constipation altered taste fatigue infection joint pain nausea or vomitting anorexia muscle pain osteonecrosis of jaw other pain breathlessness dry mouth abdominal pain hypomagnesaemia hypocalcaemia increased bone pain hypophosphatemia pins and needles oedema diarrhoea dyspepsia 158 / 704 172 / 704 177 / 704 199 / 704 121 / 704 221 / 704 544 / 704 125 / 704 390 / 704 410 / 704 246 / 704 301 / 704 5 / 704 170 / 704 103 / 704 266 / 704 177 / 704 83 / 704 80 / 704 435 / 704 80 / 704 215 / 704 170 / 704 222 / 704 248 / 704 280 / 697 226 / 697 208 / 697 222 / 697 140 / 697 236 / 697 551 / 697 136 / 697 398 / 697 417 / 697 254 / 697 303 / 697 9 / 697 171 / 697 104 / 697 265 / 697 176 / 697 80 / 697 77 / 697 428 / 697 72 / 697 202 / 697 156 / 697 207 / 697 176 / 697 we used cumulative incidence curves , kaplan - meier curves , and a log - rank test to do the secondary analyses of the di erences in time to rst skeletal - related event and overall survival between treatment groups . 
we compared the proportion of patients with renal dysfunction and osteonecrosis of the jaw using a test . we summarised toxic e ects noted in at least 10% of patients by ctcae grade ; we calculated and plotted the risk di erence and 95% ci in the proportion of patients experiencing these toxic e ects in the ibandronic acid group compared with the zoledronic acid group . this trial is registered with clinicaltrials.gov , number nct00326820 , and international standard randomised controlled trial number isrctn13914201 . role of the funding source the zice trial was an independent , national cancer research institute ( ncri ) academic trial , funded by an educational grant and provision of oral ibandronic acid from roche products ltd and cancer research uk core funding at wctu . 
the trial was endorsed by cancer research uk ( cruke / 04 / 022 ) enabling approval by the national institute for health research cancer research network ( ncrn ) to access service support costs . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results between jan 13 , 2006 , and oct 4 , 2010 , 1404 patients were randomly assigned into the trial from 99 hospitals across the uk ( gure 1 ) , with 699 patients allocated to receive zoledronic acid and 705 to receive ibandronic acid . 
all patients have been followed up for a minimum of 96 weeks ( unless died or withdrawn ) with a median follow - up of 91 weeks ( iqr 40132 ) for the zoledronic acid group and 92 weeks ( iqr 42130 ) for the ibandronic acid group . 
84% ( 1172 of 1401 ) were oestrogen - receptor ( er ) positive , 39% ( 553 of 1401 ) 03 02 01 favours ibandronic acid favours zoledronic acid figure 2 : risk di erence of patients experiencing toxic e ects ( ibandronic acidzoledronic acid ) 118 vol 15 january 2014 articles a pain severity score ( bpi ) ibandronic acid zoledronic acid progesterone - receptor ( pr ) positive , and 15% ( 209 of 1401 ) her2 - positive ( table 1 )  . 
previous treatment was also balanced : around fourfths of patients had received recent hormone therapy , just under a half had had adjuvant chemotherapy , and a minority had had adjuvant trastuzumab ( table 1 )  . 
median time from randomisation to start of treatment was 6 days ( iqr 111 ) in the zoledronic acid group and 3 days ( 17 ) in the ibandronic acid group . in the zoledronic acid group 96% ( 672 of 699 ) of patients started treatment with a median time on treatment of 75 weeks ( iqr 3596 )  . 
in the ibandronic acid group , 93% ( 654 of 705 ) of patients started treatment with a median time on treatment of 75 weeks ( iqr 3196 )  . 
the appendix shows treatment compliance over the 96 weeks ; compliance in the zoledronic acid group decreased over time , and compliance in both groups was about 80% by the end of the protocol treatment . table 2 and gure 2 show the main toxic e ects in patients undergoing each treatment over the 96 weeks . 
any grade renal toxic e ects were more common in the zoledronic acid group than in the ibandronic acid group ( = 109 , p = 0001 ) , although grade 34 renal adverse events occurred in similar numbers of patients in each group ( table 2 )  . 
figure 2 shows that the known side - e ects of zoledronic acid , such as fever and u symptoms , anaemia , and headache , were more common in the zoledronic acid group , whereas dyspepsia , a common sidee ect of ibandronic acid , was more common in the ibandronic acid group . 
pain scores showed a reduction from baseline at 12 weeks which seemed to be maintained over 96 weeks , with no di erence between the two groups ( gure 3 )  . 
 in the ibandronic acid group , 318 toxic e ects in 204 patients were reported as serious adverse events , and in the zoledronic acid arm 272 toxic e ects in 179 patients were reported as serious adverse events . 
the most commonly reported serious adverse events were pain , infection , and vomiting or nausea , with 43 ( 6% ) patients reporting pain , 15 ( 2% ) reporting infection , and 16 ( 2% ) reporting vomiting or nausea of the 704 patients in the ibandronic acid group , compared with 38 ( 5% ) patients reporting pain , 34 ( 4% ) reporting infection , and 20 ( 3% ) reporting vomiting or nausea of the 697 patients in the zoledronic acid group . 
 during the 96 - week treatment period , 65 ( 10% ) of 654 patients in the ibandronic acid group and 51 ( 8% ) of 672 patients in the zoledronic acid group withdrew from treatment because of intolerance . 
 for the primary analysis , we noted 647 skeletal - related events of any type in 284 ( 41% ) of 697 patients in the 666 536 469 441 401 357 325 305 253 645 540 487 423 382 341 300 273 251 ibandronic acid opioid non - opioid zoledronic acid weeks 704 630 581 537 497 450 412 374 333 weeks 697 643 602 543 490 450 418 371 332 figure 3 : pain severity ( a ) and use of analgesics ( b ) during the study period mean pain severity scores measured using the brief pain inventory ( bpi )  . 
opioid use represents the percentage of patients reporting use of opioid and non - opioid analgesics at each visit , with 95% cis . ibandronic acid zoledronic acid number of events number of patients ( % ) number of events number of patients 100 / 704 ( 14% ) 210 / 704 ( 30% ) 75 / 704 ( 11% ) 41 / 704 ( 6% ) 20 / 704 ( 3% ) 91 / 697 ( 13% ) 188 / 697 ( 27% ) 65 / 697 ( 9% ) 30 / 697 ( 4% ) 23 / 697 ( 3% ) fractures radiotherapy to bone hypercalcaemia orthopaedic surgery spinal cord compression sre = skeletal - related event . table 3 : sres over 96 weeks in the intention - to - treat population zoledronic acid group and 787 of any type in 293 ( 42% ) of 704 patients in the ibandronic acid group . 
table 3 shows the number and type of skeletal - related event occurring in each group over the 96 weeks in the intention - to - treat see online for appendix vol 15 january 2014 ibandronic acid ( n = 654 , 419 sres ) zoledronic acid ( n = 672 , 390 sres ) articles number at risk zoledronic acid 672 ibandronic acid 654 632 588 571 522 501 473 447 418 396 373 351 332 315 292 ibandronic acid ( n = 654 ) zoledronic acid ( n = 672 ) number at risk zoledronic acid 672 ibandronic acid 654 time ( months ) 564 521 462 423 376 349 320 296 271 256 227 222 198 184 figure 4 : cumulative incidence of skeletal - related events ( a ) and of rst skeletal - related event ( b ) in the per - protocol population population , with radiotherapy to the bone being the most common skeletal - related event ( see appendix for perprotocol population )  . 
 the primary per - protocol analysis , including any skeletal - related event 21 days apart , included 390 events in 257 ( 38% ) of 672 patients in the zoledronic acid group and 419 events in 253 ( 39% ) of 654 patients in the ibandronic acid group ( gure 4a ) , corresponding to 0435 ( 95% ci 0393 to 0480 ) skeletal - related events per person - year in the zoledronic acid group and 0499 ( 0454 to 0549 ) skeletal - related events per person - year in the ibandronic acid group . 
the log relative risk for ibandronic acid versus zoledronic acid was 0138 ( 95% ci 0033 to 0309 ) , corresponding to a rate ratio of 1148 ( 95% ci 0967 to 1362 , p = 011 )  . 
 the sensitivity analysis excluding hyper calcaemia skeletal - related events was consistent with the above results , with 312 events in the zoledronic acid group and 330 events in ibandronic acid group ; the log relative risk for ibandronic acid versus zoledronic acid was 0122 ( 95% ci 0069 to 0313 ) , which corresponds to a rate ratio of 1130 ( 0933 to 1367 )  . the intention - to - treat analysis , including any skeletalrelated event 21 days apart , included 415 skeletal - related events in 271 ( 39% ) of patients in the zoledronic acid group and 490 skeletal - related events in 284 ( 40% ) of patients in the ibandronic acid group ( gure 5 ) , corresponding to 0507 ( 95% ci 04640554 ) skeletal - related events per person - year in the ibandronic acid group and 0425 ( 03870469 ) skeletal - related events per person - year in the zoledronic acid group . 
this nding supports the result of the per - protocol analysis , with the upper ci exceeding the margin of non - inferiority . in the per - protocol population , median time to rst skeletal - related event was 970 weeks ( 95% ci 929not reached ) in the ibandronic acid group , and 99 weeks ( 95% ci 936not reached ) in the zoledronic acid group ; however , the hazard ratio ( hr ; ibandronic acid vs zoledronic acid ) was 1034 ( 95% ci 08731226 ; log - rank test p = 070 ) , indicating little di erence in time to rst event ( gure 4b )  . for the intention - to - treat analysis of overall survival , 831 patients died , 395 ( 57% ) of 697 patients in the zoledronic acid group and 436 ( 62% ) of 704 patients in the ibandronic acid group . 
we noted no di erence between groups , with an hr of 1086 ( 95% ci 09481245 , logrank test p = 024 ; gure 6 )  . discussion this large randomised phase 3 trial showed that daily oral medication with ibandronic acid 50 mg was inferior to 34 weekly intravenous infusion of zoledronic acid 4 mg in reducing the frequency of skeletal - related events in patients with breast cancer metastatic to bone . 
 however , the times to rst on - study skeletal - related event were similar in both groups ; an explanation for this inconsistency could be that the multiple - event analysis is a more sensitive analysis , which is less a ected by baseline risks for skeletal - related events that the structural bene ts of a might occur before bisphosphonate can accrue . 
this result was also seen in 120 vol 15 january 2014 articles ibandronic acid ( n = 704 , 490 sres ) zoledronic acid ( n = 697 , 415 sres ) the bismark trial , 12 which was a biomarker directed trial of zoledronic acid . those with pre - existing as expected , overall survival was very similar between groups . 
renal toxic e ects occurred less frequently with ibandronic acid than with zoledronic acid , which might have advantages for patients receiving concomitant chemotherapy or renal insu ciency , in view of the known incidence of renal adverse events associated with intravenous zoledronic acid . 
the prevalence of osteonecrosis of the jaw was low in both groups , similar in frequency to that noted in other large prospective trials , 3 re ecting modern management with pretreatment assessment of dentition and general awareness of the issue . overall compliance with ibandronic acid was 83% , compared with 86% with zoledronic acid . 
compliance with any oral therapy will be expected to be lower than a scheduled hospital - based intravenous treatment , and might be one factor underlying the reduced overall e cacy . 
the incidence of hypocalcaemia was similar between groups , and grade 34 hyopocalcaemia was very infrequent . oral ibandronic acid is licensed and widely used in the uk and in europe for the prevention of skeletal - related events in patients with breast cancer and bone metastases . 
the zice trial is the only large - scale randomised comparison of these two bisphosphonates in patients with bone metastases ( panel ) , and our overall nding that daily oral ibandronic acid cannot be regarded as non - inferior to zoledronic acid in terms of reducing the frequency of skeletal - related events in patients with metastatic breast cancer to bone should help inform its future use . 
 physicians and patients regarding additionally substudy , 14 explored the patient experience of trial - related processes in a subsample of zice participants , which might also help inform the choice of bisphosphonate . the qualzice qualitative more recently , a better understanding of the biology of bone resorption in the context of bone metastases , and the identi cation of the receptor activator of nuclear factor b ligand ( rankl ) as the key mediator of osteoclast activation , has led to the discovery of denosumab . 
this fully human monoclonal igg2 monoclonal antibody speci cally binds to human rankl profoundly inhibiting osteoclast activity and was assessed in a large randomised study3 comparing subcutaneous denosumab with intravenous zoledronic acid both every 4 weeks . 
denosumab is now licensed for the prevention of skeletal - related events number at risk zoledronic acid 697 ibandronic acid 704 time ( months ) 646 639 599 588 535 541 488 492 453 448 414 411 377 368 figure 5 : cumulative incidence of skeletal - related events in the intention - to - treat population ibandronic acid ( n = 704 ) zoledronic acid ( n = 697 ) number at risk zoledronic acid 704 ibandronic acid 697 study month 580 592 483 477 400 396 242 234 175 178 108 101 figure 6 : overall survival in the intention - to - treat population ( pathological fracture , radiation to bone , spinal cord compression or surgery to bone ) in adults with bone metastases from solid tumours and provides another , possibly better option for patients with this common complication of metastatic cancer . one of the limitations of this pragmatic large study was that serial imaging was not done routinely to detect asymptomatic skeletal - related events such as vertebral fractures . 
 another limitation is that compliance with oral ibandronic vol 15 january 2014 articles panel : research in context systematic review we combined the evidence from a contemporary cochrane review of bisphosphonate trials in advanced breast cancer published in 2002 , 13 together with information from the pharmaceutical companies , and particularly roche products ltd , the holder of the licence for ibandronic acid , who informed us that no large - scale randomised trials collecting skeletalrelated event information as the primary endpoint of ibandronic acid against zoledronic acid were being carried out worldwide . interpretation this study provides a direct comparison , in a large randomised trial , of the e cacy and side - e ect pro le of oral ibandronic acid versus the gold standard of zoledronic acid . 
we conclude that clinicians should consider alternative treatment for bone metastases in their breast cancer patients , such as zoledronic acid or denosumab , since they seem to be more e ective in skeletal - related event prevention than oral ibandronic acid . acid was only assessed by checking compliance with the patient or patient - reported discontinuation of use . 
a further limitation relates to the open label nature of the trial , which meant that pain assessments were not masked with respect to allocated therapy to either the patient or the study investigator , and thus the possibility of bias cannot be excluded . 
further limitations included that we did not obtain data for progression at other sites , nor did we obtain data for dose reductions for renal toxic e ects or dose delays for dental problems , and we did not take into account modi cations to anticancer therapies in the analysis . 
a future analysis could be done to examine the association between adverse events and concurrent anticancer treatment . the results of this study are generalisable to the population of patients with metastatic breast cancer to bone for which bisphosphonate therapy is indicated . 
 although oral ibandronic acid remains a licensed option for these patients and has some advantages in convenience in terms of administration , it would seem to be slightly less e ective in clinical practice in preventing skeletalrelated events . 
however , physicians and patients might need to select treatment by balancing the inconvenience and costs of intravenous administration . in e cacy against the di erence contributors pb - l , nm , rc , ps , ja , kh , and gg were involved in the design and development of the trial and the writing and review of the protocol . 
all authors have seen and approved the nal dradw and rg were principal investigators at centres recruiting more than 5% of patients . con icts of interest we declare that we have no con icts of interest . acknowledgments the zice trial was sponsored by velindre nhs trust , funded by an educational grant from roche products ltd and cruk core funding at the wales cancer trials unit ( wctu )  . 
we also thank robert cowles , sue rees , and helen philips ( wctu trial managers ) , athena tsonis , hala jundi , and becca lloyd ( wctu data managers ) , loys richards and liz merri eld ( wctu safety o cers ) , debbie wright ( pharmacist ) , clare boobier and debbie fenlon ( research nurses ) , bernadette fuge and catherine roberts ( patient representatives )  . 
we would like to thank all the principal investigators and their colleagues responsible for recruiting and treating patients ( appendix )  . access to opioids : a balance of harms opioid overdose killed 64 070 americans between 201617 to become the leading cause of mortality in the usa for people younger than 50 years . 
this recommendation is in stark contrast to this administrations aim of cutting the government health budget , and trump has refused to declare the current situation a national emergency , an action that would increase national impetus to act . 
what is causing this devastating increase in opioid abuse in the usa , and what implications will failure to act have on provision of legitimate opioid access ? opioid analgesics are essential for the relief of in patients with cancer . 
 moderate - to - severe pain in recognition of this fact , morphine , a naturallyoccurring opiate , was added to the who model list of essential medicines in 2015 . 
nonetheless , because of the long and chequered history of the recreational use of opiates , access is still limited worldwide , with approximately 80% of the worlds population estimated to have insufficient access to analgesics for pain relief . 
 a 2016 paper by the international narcotics control board found that the use of opioid analgesics remained low in africa , asia , central and south america , the caribbean , and eastern and southeastern europe . 
when compared with cancer incidence in these areas , there is a clear disparity between the level of need ( especially in regions where cancers are more likely to be diagnosed at advanced stages ) and analgesic provision , with barriers including inadequate medical training medical training , fear of addiction , inadequate financial resources , cultural attitudes towards treatment of pain , fear of criminal prosecution , and onerous regulatory frameworks for prescription of medical narcotics . 
 countries , in high - income the pendulum has arguably swung the other way , with prescriptions for opioid analgesics tripling between 1991 and 2013 in the usa , and doubling between 2000 and 2015 in the uk . 
beginning with recently deceased ted stanleys discovery that fentanyl ( a synthetic opioid analgesic between 50100 times more potent than heroin ) could be combined with sugar to make a palatable , quick - acting analgesic lollipop , synthetic opioids are now readily available in easily ingestible formulations , including delayed - release and oral spray formulations . 
part of the unprecedented increase in prescriptions has been driven through unscrupulous pharmaceutical marketing strategies of these easyto - ingest formulations to physicians ; in 2007 , purdue pharma executives pleaded guilty to criminal charges of misbranding oxycontin ( a timed - release formulation of the opioid oxycodone ) as less addictive and less prone to substance abuse than other formulations . 
although purdue pharma was fined us$634 million , such aggressive product marketing continues , with insys therapeutics currently under investigation for insurance fraud for approval of their oral fentanyl spray subsys . 
in the absence of a care network to address and help with addiction rehabilitation , patients who are addicted are driven to find new sources of opioids , including cheaper , and more readily - available , black market sources of opioids of unknown quality and strength , thus leading to frequent accidental overdose . 
the who access to controlled medications programme defines balance as the dual obligation of a government to enable adequate availability of controlled substances for medical need while simultaneously preventing abuse . 
in the usa at least , multiple steps to address the situation must be taken , including provision of adequate rehabilitation facilities and a legislative end to overprescription and unethical marketing of opioids . 
we investigated whether the frameshift nature of indel mutations , which create novel open reading frames and a large quantity of mutagenic peptides highly distinct from self , might contribute to the immunogenic phenotype . methods we analysed whole - exome sequencing data from 5777 solid tumours , spanning 19 cancer types from the cancer genome atlas . 
we assessed in - silico tumour - specific neoantigen predictions by mutation type with pan - cancer analysis , together with rnaseq profiling in renal clear cell carcinoma cases ( n = 392 ) , to compare immune gene expression across patient subgroups . 
associations between indel burden and treatment response were assessed across four checkpoint inhibitor datasets . findings we observed renal cell carcinomas to have the highest proportion ( 012 ) and number of indel mutations across the pan - cancer cohort ( p < 22 10 ) , more than double the median proportion of indel mutations in all other cancer types examined . 
immune gene expression analysis in the renal clear cell carcinoma cohort showed that the presence of mutant - specific neoantigens was associated with upregulation of antigen presentation genes , which correlated ( r = 078 ) with t - cell activation as measured by cd8 - positive expression . 
finally , analysis of checkpoint inhibitor response data revealed frameshift indel count to be significantly associated with checkpoint inhibitor response across three separate melanoma cohorts ( p = 47 10 )  . interpretation renal cell carcinomas have the highest pan - cancer proportion and number of indel mutations . 
 evidence suggests indels are a highly immunogenic mutational class , which can trigger an increased abundance of neoantigens and greater mutant - binding specificity . funding cancer research uk , uk national institute for health research ( nihr ) at the royal marsden hospital national health service foundation trust , institute of cancer research and university college london hospitals biomedical research centres , the uk medical research council , the rosetrees trust , novo nordisk foundation , the prostate cancer foundation , the breast cancer research foundation , the european research council . copyright the author ( s )  . 
the data have also been scrutinised for mutations that might play a role in the recognition of cancer cells by the immune syste the focus of these analyses to a large extent is on the single nucleotide variants ( snvs ) , on account of the relative simplicity and reliability of calling sequence changes of one base pair ( bp ) fixed length . 
as a consequence , the effect of small scale insertion and deletion mutations ( indels ) on antitumour immunity has been poorly characterised despite the clear link of such mutations to oncogenesis3 and their potential to generate highly immunogenic peptides . inhibitor the notion the success of checkpoint therapies underlines tumour - specific t - cell that responses pre - exist in some patients and are kept under tight control via immune modulatory mechanisms . 
the predominant focus of existing literature was on single nucleotide variation ( snv ) mutations , with no previous study done of insertion and deletion ( indel ) mutations on a pan - cancer basis . 
regarding the association between somatic mutations and upregulation of antitumour immunity via checkpoint inhibition , several previous studies reported a link between high snv load and improved response to checkpoint inhibition . 
no previous pan - cancer study has investigated the difference between snv and indel - derived neoantigens , despite the propensity of indels to generate highly mutagenic peptides via creation of a shifted novel open reading frame . added value of this study we did a pan - cancer assessment of indel load across 5777 tumour samples spanning 19 cancer types . 
kidney tumours were observed to have the highest proportion and absolute count of indel mutations on a pan - cancer basis , a result which was replicated in two further independent datasets . 
finally , we assessed the association between indel load and checkpoint inhibitor response in three melanoma cohorts , which showed indel load to be more strongly associated with response than non - synonymous ( ns ) snv load . implications of all the available evidence our data highlight the importance of frameshift neoantigens alongside nssnv neoantigens as determinants of immunotherapy efficacy and potentially crucial targets for vaccine and cell therapy interventions . 
t cells reactive to tumour - specific mutant antigens ( neoantigens ) have been detected epithelial malignancies4 and neoantigens are increasingly shown to be the target of checkpoint inhibitor - induced t - cell responses5 , 6 and adoptively transferred t cells.79 many investigators are leveraging whole - exome sequencing and rna sequencing , focusing on non - synonymous snvs ( nssnvs ) , to predict expressed mutated peptides that bind mhc class i molecules ( snv - neoantigens )  . 
 neoantigen burden is closely related to the nssnv burden , which varies significantly across cancer types , from one nssnv in paediatric tumours to more than 1500 nssnvs in tumours associated with microsatellite instability.10 however , less than 1% of the nssnvs in expressed genes lead to detectable cd4 - positive11 or cd8 - positive t - cell7 reactivities in tumour - infiltrating lymphocytes . 
accordingly , efficacy of checkpoint inhibitors is most marked in tumour types with a high nssnv lung adenocarcinoma , lung squamous cell carcinoma , head and neck squamous cell carcinoma , and carcinoma of the bladder , 10 which reflects a higher probability of creating a neoantigen that will be presented to and recognised by t cells . 
furthermore , within these tumour types , nssnv and neoantigen burdens correlate with response to checkpoint inhibitors.1216 a notable outlier is renal clear cell carcinoma , which has a relatively low nssnv burden ( around ten times lower than melanoma )  . 
 including melanoma , burden , renal clear cell carcinoma is characterised by a high level of tumour - infiltrating immune cells17 and has been interferon - , high - dose shown interleukin 2 , 18 , 19 and , more recently , checkpoint inhibitors , 20 , 21 but the mutational and antigenic determinants of these responses are unknown . respond from self indel mutations that cause a frameshift ( frameshift indels ) create a novel open reading frame and could produce a large quantity of neoantigenic peptides highly distinct ( appendix p 5 )  . 
it has been hypothesised22 that novel open reading frames might be an ideal source of tumour - derived neoantigens and so induce multiple neoantigen reactive t cells , because of both an increased number of mutant peptides and reduced susceptibility to self - tolerance mechanisms . 
on this basis , we aimed to characterise the pattern of indel mutations with pan - cancer analysis and investigate their association with antitumour immune response and outcome following checkpoint blockade . methods study design and participants pan - cancer somatic mutational data were obtained from the cancer genome atlas ( tcga ) for whole - exome sequencing data of 5777 solid tumours , across 19 cancer types : bladder urothelial carcinoma , invasive breast carcinoma , cervical and endocervical cancers , colorectal adenocarcinoma , glioma , head and neck squamous cell carcinoma , chromophobe renal cell carcinoma , renal clear cell carcinoma , renal papillary cell carcinoma , liver hepatocellular carcinoma , lung adenocarcinoma , serous lung carcinoma , ovarian squamous cell 1010 vol 18 august 2017 articles pancreatic cystadenocarcinoma , adenocarcinoma , prostate adeno carcinoma , skin cutaneous melanoma , stomach adenocarcinoma , thyroid carcinoma , and uterine carcinosarcoma . 
we performed replication analyses in two additional cohorts of patients with renal clear cell carcinoma : a whole - exome sequencing study of 106 patients with renal clear cell carcinomas reported by sato and colleagues23 and a whole - exome sequencing study of ten patients with renal clear cell carcinomas reported by gerlinger and colleagues.24 we obtained final post - quality control patient - level mutation annotation files for each study . to further test for an association between nssnvs or indel loads and patient response to checkpoint inhibitor therapy we used four patient cohorts . 
the first dataset consisted of 38 patients with melanoma treated with anti - pd - 1 therapy , as reported by hugo and colleagues.25 we obtained final post - quality control mutation annotation files and clinical outcome data , and 34 patients were retained for analysis after exclusion of cases in which dna had been extracted from patientderived cell lines and patients in whom tissue tumor purity was below 20% . 
four samples from hugo and colleagues25 were taken after a short period on treatment , which raises the possibility that checkpoint inhibitor therapy itself might have affected mutational frequencies through possible elimination of immunogenic tumour clones . 
to be consistent with the original study , these samples were not excluded ; however , we note the frameshift indel association presented becomes more significant with these cases removed . 
the second checkpoint inhibitor cohort comprised of 62 patients with melanoma treated with anti - ctla - 4 therapy , as reported by snyder and colleagues.13 all patients samples were taken from fresh snap frozen tumour tissue with tumour purity of more than 20% so , accordingly , all 62 cases were retained for analysis . 
the snyder and colleagues cohort also contained a number of samples taken on treatment ; these samples have been retained for consistency ; however , we note again the significance of results strengthens if they are removed . 
 the third checkpoint inhibitor cohort comprised of 100 patients with melanoma treated with anti - ctla - 4 therapy , as reported by van allen and colleagues ; 12 one patient ( pat21 ) was excluded because of a tumour purity of less than 20% . 
the final checkpoint inhibitor cohort comprised of 31 patients with non - small - cell lung cancer treated with anti - pd - 1 therapy , as reported by rizvi and colleagues ; 14 all patients were eligible for inclusion . 
for these four cohorts , 1214 final mutation annotation files , including indel mutations , were not available , so we obtained raw bam files and undertook variant calling using a standardised bioinformatics pipeline . 
to assess for a general association between nssnvs or indel loads and patient overall survival we used a final cohort of 100 patients with non - small - cell lung cancer , as reported by jamal - hanjani and colleagues.26 we obtained final post - quality control mutation annotation files and clinical outcome data , and 88 patients were retained for analysis after exclusion of non - smokers . 
we used picard tools , gatk ( version 2.8.1 ) , and fastqc ( version 0.10.1 ) to produce quality samtools mpileup ( version 0.1.19 ) 29 was used to locate non - reference positions in tumour and germline samples . 
 following completion , variants called by mutect were filtered according to the filter parameter pass . in the pan - cancer cohort , snv and indel mutation counts were computed per case , considering all variant types . 
we estimated the extent of nmd for all indel and snv mutations ( with snv mutations used as a benchmark comparator ) by comparing mrna expression in samples with a mutation to the median mrna expression of the same transcript across all other tumour samples in which the mutation was absent . 
specifically , mrna expression of every mutation - bearing transcript was divided by the median mrna expression of that transcript in non - mutated samples , to give an nmd index . 
tumour purity in the renal clear cell carcinoma cohort was 054 , 32 quantified by histological assessment , and assuming constant expression in the remaining 046 normal cellular content , that would yield an adjusted 14% drop in expression in indel - mutationbearing cancer cells . 
if we assume that tumour mutations are clonal , of heterozygote genotype , in a diploid genomic region , and wild - type allele expression in mutated cancer cells remains constant , a purity - adjusted reduction of 05 would be expected under a model of fully effective nmd . 
these data are presented as a global approximation of nmd efficiency , using methods in line with previous publications.33 nmd index values were log indicating no mrna degradation and plotted for indel or snv mutations . transformed , with 0 we used pyclone34 and ascat35 to determine the clonal status of variants in the cohorts by snyder and colleagues13 and van allen and colleagues.12 for each case variant calls were integrated with local allele - specific copy number ( obtained from ascat ) , tumour purity ( also obtained from ascat ) , and variant allele frequency . 
for a number of tumours the reliable copy number , mutation , and purity estimations could not be clonal architecture analysis extracted , rendering and colleagues in snyder intractable and these tumours were omitted from the analysis . 
a strong binding threshold was used for wild - type alleles to ensure fair comparison between snv - derived and indel - derived neoantigens , in view of the high incidence of wild - type non - binders for indels . 
we excluded ( from the pancancer neoantigen analyses ) cancers that were associated with a high level of viral genome integration , including cervical ( > 80% rate of human papillomavirus integration ) and hepatocellular carcinoma ( > 50% rate of hepatitis b integration ) , but not head and neck squamous cell ( < 15% rate of human papillomavirus carcinoma integration )  . 
no tcga dataset was available for merkel cell carcinoma . immune gene signature data were obtained from rooney and colleagues , 40 with gene sets defined as stated in the appendix ( p 3 )  . 
a high burden of frameshift indel high - affinity neoantigens was defined as more than 10 per case ( n = 32 ) , and the percentage difference in expression was compared between the high indel neoantigen group and all other patients across each immune signature . 
the same analysis was repeated for a high burden of snv - derived high - affinity 1012 vol 18 august 2017 articles neoantigens , with a threshold of more than 17 snv neoantigens selected to size match the high burden groups ( equal number of patients ; n = 32 across all highload groups ) across mutational types . 
 we did correlation analysis within the high - frameshift indel neoantigen group ( n = 32 patients with renal clear cell carcinoma )  . outcomes across the four cohorts of patients treated with checkpoint inhibitors , we tested nssnv , all - coding indel , and frameshift indel variant counts for an association with patient response to therapy . 
 for snyder and colleagues cohort , 13 long - term clinical benefit was defined as radiographic evidence of freedom from disease , evidence of a stable disease , or decreased volume of disease for more than 6 months . 
no long - term clinical benefit was defined as tumour growth on every ct scan after the initiation of treatment ( no benefit ) or a clinical benefit lasting 6 months or less ( minimal benefit )  . 
for hugo and colleagues cohort , 25 responding tumours were complete response , partial response , and stable disease , and non - responding tumours were defined as disease progression . 
for van allen and colleagues cohort , 12 clinical benefit was defined as complete response , partial response , or stable disease , and no clinical benefit was progressive disease or stable disease with overall survival less than 1 year . 
for rizvi and colleagues cohort , 14 durable clinical benefit was defined as partial response or stable disease lasting longer than 6 months , and no durable benefit was progressive disease less than 6 months from beginning of therapy . 
 multivariate cox regression was done with relapse - free survival versus indel load with stage , adjuvant therapy ( yes or no ) , age , and histology included in the model . we compared indel burden and proportion measures between renal cell carcinomas and all other non - kidney cancers with a two - sided mann - whitney u test . 
in the checkpoint inhibitor response analysis , nssnv , exonic indel , and frameshift indel counts were each compared to patient response outcome using a two - sided mannwhitney u test . 
we carried out statistical analyses using r ( version 3.0.2 ) and considered a p value of 005 or less ( two - sided ) as being statistically significant . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results we observed a median indel proportion value of 005 and a median indel count of 4 , cohort - wide . 
across all tumour types , renal clear cell carcinoma was found to have the highest proportion of coding indels , 012 ( p < 22 10 ; figure 1 ) , a 24 times increase when compared with the pan - cancer average . 
this result was replicated in two further independent cohorts , with median observed indel proportions of 010 in sato and colleagues study23 and 012 in gerlinger and colleagues study24 ( figure 1 )  . 
renal papillary cell carcinoma and chromophobe renal cell carcinoma had the second and third highest indel proportion , suggesting a possible tissue - specific mutational process contributing to the acquisition of indels in renal cancers . 
renal papillary cell carcinoma ( median indel number of 10 [ 95% ci 911 ] ) and chromophobe renal cell carcinoma ( 8 [ 710 ] ) had the highest absolute indel count across all tumour types , closely followed by renal clear cell carcinoma ( 7 [ 68 ] )  . 
 renal clear cell carcinoma is characterised by loss - offunction mutations in one or more tumour - suppressor genes : vhl , pbrm1 , setd2 , bap1 , and kdm5c , 32 which can be inactivated by nssnv or indel mutations . 
 to exclude the possibility that these hallmark mutations were distorting the results , we recalculated renal clear cell carcinoma indel proportion excluding these genes ; the revised indel proportion remained at 012 . 
when we used previously published multiregion whole - exome sequencing data24 from ten cases of renal clear cell carcinoma to assess the clonal nature of indel mutations , 53 ( 48% ) of 110 frameshifting indels were clonal in nature ( present in all tumour regions )  . the overall effect of nmd on the expression of indelmutated genes was estimated to be 14% ( 7% drop divided by 054 tumour purity ) , suggesting it operates on a subset of transcripts ( appendix p 6 )  . next we sought to investigate the potential immunogenicity of nssnv and indel mutations through analysis of mhc class i - associated tumour - specific neoantigen binding predictions in the pan - cancer tcga cohort . 
the last two boxplots are additional independent renal clear cell carcinoma replication datasets from sato and colleagues23 and gerlinger and colleagues.24 statistical comparison is renal clear cell carcinoma cohort compared with all other non - kidney tcga samples . 
 mutations ( n ) neoantigens ( n ) * mutant - specific neoantigens ( n ) neoantigens per mutation mutant - specific neoantigens per mutation nssnvs fs - indels 335 594 19 849 214 882 39 768 75 224 39 608 enrichment 064 200 313 022 200 894 nssnvs = non - synonymous single nucleotide variants . 
in a similar manner , predictions were made on 19 849 frameshift indel mutations , resulting in 39 768 high - affinity binders with a rate of 200 neoantigens per frameshift mutation ( frameshift neoantigens ; table )  . 
thus on a per mutation basis , frameshift indels could generate around three times more high - affinity neoantigen binders than nssnvs ( table ) , consistent with the prediction in a recent analysis of a colorectal cancer cohort.41 when both wild - type and mutant peptides are predicted to bind , central immune tolerance mechanisms might delete cells with the reactive t - cell receptor.42 therefore , we repeated a pancancer analysis restricting the neoantigens to mutantspecific binders ( ie , where the wild - type peptide is not predicted to be a strong binder ) , and showed that frameshift indels were nine times enriched for mutantallele - only binders ( table )  . of particular interest were genes that are frequently altered via frameshift mutations and with high propensity for mhc binding . 
in a pan - cancer analysis , these genes were enriched for classic tumour - suppressor genes , including tp53 , arid1a , pten , kmt2d , kmt2c , apc , and vhl ( figure 2 )  . 
collectively , the top 15 genes with the highest number of frameshift mutations were mutated in more than 500 samples ( approximately 10% of the cohort with 5777 samples ) with more than 2400 highaffinity neoantigens predicted . 
 furthermore , by virtue of being founder events , many alterations in tumour - suppressor genes are clonal , present in all cancer cells , rendering them compelling targets for immunotherapy.43 we next considered the clinical effect of indel mutations the association between neoantigen by assessing enrichment and therapeutic benefit . 
consistent with a potential role of frameshifts in the generation of neoantigens , those tumour types approved for the use of checkpoint inhibitors were all found to harbour an above average number of frameshift neoantigens , despite substantial differences in the total snv or indel mutational burdeneg , renal cell carcinoma ( figure 3 )  . 
 overall , the number of frameshift neoantigens were significantly higher in the checkpoint inhibitor - approved tumour types versus those that have not been approved to date ( p < 22 10 )  . 
however , the potential presence of frameshift neoantigens alone does not imply that they induce t - cell responses , and hence we tested their effect on checkpoint inhibitor efficacy . 
 although nssnvs ( p = 027 ) and in - frame ( 3n ) indels from an anti - pd - 1 study25 1014 vol 18 august 2017 articles ( p = 019 ) had no association with response to treatment , frameshift indel mutations were significantly associated with anti - pd - 1 response ( p = 0023 ; figure 4a )  . 
the upper quartile of patients with the highest burden of frameshift indels had an 88% ( seven of eight cases ) response to antipd - 1 therapy , compared with 43% ( 11 of 26 cases ) for the lower three quartiles ( odds ratio 95 [ 95% ci 1028923 ] ; figure 4b )  . 
to confirm the reproducibility of this association , further checkpoint inhibitor response data were obtained from two additional melanoma cohorts : snyder and colleagues cohort13 ( n = 62 , anti - ctla - 4 treated ) and van allen and colleagues cohort12 ( n = 100 , anti - ctla - 4 treated )  . 
we did the same analysis in each cohort and frameshift indel burden was significantly associated with checkpoint inhibitor response in both datasets ( hr 34 [ 95% ci 1051127 ] ; p = 00074 for snyder and colleagues cohort and 29 [ 115755 ] ; p = 0032 for van allen and colleagues cohort ; figure 4a )  . 
 an overall meta - analysis across the three cohorts confirmed frameshift indel count to be associated with checkpoint inhibitor response ( p = 47 10 ) , and with a more significant association than nssnv count ( p = 48 10 )  . 
the effect of clonality was additionally assessed , and clonal frameshift indels were found to have a further significantly predictive advantage beyond all frameshift indels ( clonal and subclonal ; appendix p 7 ) , supporting previous work reported by our group.43 overall survival analysis was not different between high and low frameshift indel groups , possibly because of the effect of subsequent therapies on the overall survival ( or 243 [ 95% ci 077773 ] ; p = 0228 for hugo and colleagues cohort25 ; appendix p 8 )  . 
we assessed the association between frameshift indel load and checkpoint inhibitor response in another tumour type by using data obtained from rizvi and colleagues small cohort14 of 31 patients with non - small - cell lung cancer treated with anti - pd - 1 therapy ; no difference was observed ( p = 023 )  . 
 to further investigate the importance of frameshift indels in non - small - cell lung cancer , we did additional analysis using data from jamal - hanjani and colleagues cohort26 of 100 cases , none of whom received treatment with checkpoint inhibitors . 
consistent with our previous findings , 43 we observed lung adenocarcinoma whose tumour 's harboured a high clonal neoantigen burden ( higher than upper quartile of cohort ) survival compared with the bottom three quartiles ( p = 0026 )  . 
 however , across all histological subtypes of non - smallcell lung cancer , survival was found to be significantly improved for patients with a high load of frameshift indels ( vs low load : hr 025 [ 95% ci 006108 ] ; p = 0045 ) ; by contrast , nssnv load was not formally associated ( 036 [ 011121 ] ; p = 0084 ; appendix p 9 )  . 
 of note , the strongest prognostic predictor was for patients in the patients with a high load of both nssnvs and frameshift indels , with elevated levels of both frameshift indels and nssnvs , with no events in this that patients with relapse - free improved exhibited arid1a mll3 mll2 tp53 vps13c map3k1 flna fat1 notch1 pten number of samples mutated figure 2 : recurrent genes with frameshift indel neoantigens data are from all patients in the cancer genome atlas pan - cancer cohort . 
the graph shows the number of unique samples containing a frameshift indel neoantigen and the number of unique neoantigens ( ie , each mutation can generate multiple neoantigens )  . 
multivariate analysis showed some evidence of correlation between variables ( appendix p 2 ) , so further investigation of nssnvs and frameshift indels as predictors in larger patient cohort will be required to draw definitive conclusions . analyses of the indel load and proportion of response achieved from phase 2 studies for the tumour types not approved for checkpoint inhibition were limited by the small sample size and variable patient inclusion criteria such as pdl - 1 immunohistochemistry ( appendix p 4 )  . 
 nevertheless , the proportion of patients achieving a response was higher in triple - negative breast cancer44 compared with other invasive breast carcinoma molecular subtypes , and triple - negative invasive breast carcinoma has a higher burden of frameshift and mutant - specific neoantigens ( figure 3 )  . 
furthermore , mutational burden has been reported as higher in brca1 - mutated triplenegative breast cancer compared with brca - wild - type triple - negative breast cancer , 45 and we specifically observed a higher indel load in these cases ( appendix p 10 )  . 
 however , this outcome did not correlate with tumourinfiltrating lymphocyte density ( appendix p 10 ) , possibly because of the small sample size , absence of indel immunogenicity in this tissue type , or additional factors that modulate tumour - infiltrating lymphocyte density . finally , although genomic data are not available to correlate with checkpoint inhibitor response in renal clear cell carcinoma , we analysed the association between frameshift neoantigen load and immune responses within the tumour using rnaseq gene expression data . 
a high load of frameshift neoantigens was associated with upregulation of immune signatures classically linked to immune activation , including mhc class i antigen and presen tation , cd8 - positive t - cell increased cytolytic activity , a pattern not observed in the high snv - neoantigen group ( figure 5 )  . 
furthermore , correlation analysis within the high frameshift neoantigen group showed that cd8 - positive t - cell signature was correlated with both mhc class i antigen presentation genes ( r = 078 ) and cytolytic activity ( r = 083 ; figure 5 )  . activation , discussion in this study , we analysed the pattern of indel mutations across 19 solid tumour types and found that renal clear cell carcinoma , renal papillary cell carcinoma , and chromophobe renal cell carcinoma have the highest indel rate as a proportion of their total mutational burden and the highest overall indel count and are enriched for mutant - specific neoantigens . 
we also observed that indel number is significantly associated with checkpoint inhibitor response in melanoma . in non - smoking non - small - cell indels are thought to occur as a result of dna strand slippage during dna synthesis46 and their frequency is higher in repetitive sequences , especially those that are at - rich . 
indels are also generated through mutagen exposure , with a higher number observed in smoking than lung cancer ( lung adenocarcinoma ) 40 and higher in uv - exposed ( cutaneous ) versus uv - protected ( mucosal ) melanomas.47 less is known about the repair of indels than snvs ; however , the role of the mismatch repair mechanism instability - high phenotype , characterised by excess indels in repetitive sequences as seen in patients with lynch syndrome . 
 although renal clear cell carcinoma has been reported in patients with lynch syndrome , 48 this cannot account for the overall pattern of indel rates across renal clear cell the microsatellite illustrated by figure 3 : tumour - specific neoantigen counts by cancer type count of snv - derived neoantigens ( a ) , frameshift indel - derived neoantigens ( b ) , and mutant - only neoantigen binders ( c ) , and proportion of neoantigens derived from snvs and indels ( d ) and neoantigens in which mutant allele - only binds ( e )  . 
most renal clear cell carcinomas have loss of chromosome 3p , which encodes the mismatch repair gene mlh1 , but the remaining allele is rarely mutated in sporadic renal clear cell carcinoma . 
another relevant gene encoded on 3p is fhit , and its deficiency has been linked with indel accumulation in knockout mouse models , but the consequences of the heterozygous knockout ( whether haploinsufficient ) are unknown.49 however , as loss of 3p is an infrequent event in renal papillary cell carcinoma and chromophobe renal cell carcinoma and indels are also elevated in both these tumour types , other tissuespecific phenomena are likely to contribute to the increased indel burden across all renal carcinoma subtypes.50 renal clear cell carcinoma and renal papillary in the proximal tubule and cell carcinoma arise chromophobe renal cell carcinoma in the distal tubule of the nephron , and this shared tissue context might be important , even if the three subtypes are molecularly distinct.32 , 50 , 51 the nephron , and the proximal tubule in particular , play a crucial role in the reabsorption of vast volumes of renal filtrate and elimination of waste products of metabolism and toxins , with the effects of toxin elimination evident in the increased incidence of renal clear cell carcinoma in those individuals exposed to aristolochic acid.52 ochratoxin a , a mycotoxin , induces renal tumours in rodents by causing double - strand breaks.53 poly morphisms in genes involved in the repair of double - strand breaks are associated with an increased risk of renal clear cell carcinoma.54 double - strand breaks are mostly repaired by non - homologous end - joining , which is error - prone and can increase the rate of small indels ( 110 bp )  . 
therefore , it is possible that an environmental toxin causes an excess of double - strand vol 18 august 2017 1017 articles a co - inhibition_apc type_ii_ifn_response cytolytic_activity co - inhibition_t_cell co - stimulation_apc pdcs mhc_class_i cd8_t_cells r = 078 mhc class i if - indel - m utations fs - indel - neoatgs ns - snv - neoatgs r = 083 cytolytic activity figure 5 : immune gene signatures in patients with renal clear cell carcinoma ( a ) percentage change in median gene signature expression is shown between high and low groups for each metric on the x - axis as labelled . 
 ( b ) correlation analysis within the high fs - indel - neoatgs group showed the cd8 + t - cell signature was correlated with both mhc class i antigen presentation genes and cytolytic activity . 
brca1 has been shown to inhibit error prone non - homologous endjoining.55 however , we did not observe a correlation between indel load and tumour - infiltrating leucocytes density invasive breast carcinoma . 
 triple - negative in brca1 we observed that indels , which alter the reading frame , generate three times as many predicted neoantigens as nssnvs and nine times as many strong mutant - binding neoantigens where the wild - type sequence is not predicted to strongly bind the hla molecule ( ic50 > 50 nm )  . 
in keeping with this notion , microsatellite instability - high colorectal cancer cd8 - positive leucocytes density correlates positively with the total number of frameshift mutations.56 with the exception of polyomavirus - positive merkel cell carcinoma and hodgkins lymphoma , renal clear cell carcinoma is the only tumour type with a relatively low nssnv burden among the tumour types for which checkpoint inhibitors have been approved for tumour - infiltrating its clinical use . 
however , owing to a comparable frameshift level of mutant - specific high - affinity burden neoantigens is similar to that observed in non - small - cell lung cancer and melanoma , and the same is true of renal papillary cell carcinoma and chromophobe renal the cell carcinoma . 
although immunogenicity of renal papillary cell carcinoma is sparse , complete responses have been noted with the use of both high - dose interleukin 257 and anti - pd - 1 therapy.58 , 59 therapeutic data in chromophobe renal cell carcinoma are limited . the evidence for inhibitor drugs , efforts given the differential benefit across patients , the spectrum of immune - related adverse events , and the cost of checkpoint identify biomarkers of response are ongoing . 
mutational and neoantigen burdens have been shown to correlate with clinical outcomes from checkpoint inhibitor therapy in patients with advanced melanoma , colorectal cancer , and nonsmall - cell lung cancer.13 , 14 , 16 however , some patients with cutaneous melanoma with a low nssnv burden still derive benefit from checkpoint inhibitors , as do some patients with uv - protected mucosal melanomas , 60 which have a characteristically low nssnv burden.61 we analysed three melanoma datasets for which both response and mutational data were available . 
in two of the three studies , 13 , 14 comprising a total of 96 patients treated with either anti - pd - 1 or anti - ctla - 4 therapy , frameshift indel burden was a better predictor of response than nssnv burden . 
in the third study12 of 100 patients treated with anti - ctla - 4 therapy , the nssnv burden and frameshift burden were both significantly associated with checkpoint inhibitor response . 
we note that most of the patients in van allen and colleagues cohort12 were pretreated and therefore any mutational biomarker assessment in this group might be less reliable . although nssnvs contribute greatly towards tumour immunogenicity in heavily mutated tumours , our analyses suggest that frameshift mutations also make a significant contribution relative to their overall low number . 
the contribution of frameshift indels in low nssnv burden tumours might be of greater importance still , as illustrated by the fact that frameshift mutations contribute over a third of the neoantigen load in renal clear cell carcinoma . 
mutational and checkpoint inhibitor response data were not available for renal clear cell carcinoma , hence we could not establish a direct association between frameshift indels and positive checkpoint inhibitor response . 
in terms of indirect evidence in renal clear cell carcinoma , we observed an association between the frameshift neoantigens and upregulation of machinery necessary for antigen presentation by the mhc complex and t - cell activation . 
 furthermore , the cd8 - positive t - cell signature in the frameshift neoantigen - high group was closely related to cytolytic activity , suggesting the presence of antitumour 1018 vol 18 august 2017 articles effectors that could confer sensitivity to immunotherapy . 
 however , no definitive conclusions can be drawn until checkpoint inhibitor response and indel load is directly investigated in a sufficiently powered series of renal clear cell carcinoma cases . lead to the for frameshift neoantigens to contribute to antitumour immunity the mutant peptides must be expressed . 
published analyses62 of germline samples show that premature loss of termination codons frequently expression of the variant allele , but that some mutant transcripts escape nmd on the basis of the exact location of the frameshift within a gene . 
combined analyses of than mutational and expression data 10 000 cancer samples showed that nmd is triggered with variable efficacy , and even when effective might not alter expression because of factors such as short mrna halflife.33 rnaseq analysis in renal clear cell carcinoma cases showed a minimal change in mrna transcript levels for frameshift indel - mutated tumours , suggesting nmd is operating on a subset of transcripts , as expected . 
in this context , the strongly hypoxic microenvironment that characterises renal clear cell carcinomas might be a contributing factor , with evidence showing nmd inhibition in cells subject to hypoxia and other perturbed microenvironmental conditions.63 from more clonal frameshift mutations could be an important source of tumour - specific antigens for personalised immunotherapy strategies , including peptide vaccines and adoptive cell therapy . 
tumour - reactive t cells recognising a frameshifted product of the cdkn2a tumour - suppressor gene were reported to mediate a potent in - vivo response in melanoma.64 in microsatellite instability - high colorectal cancer , frameshift neopeptidespecific cytotoxic t - cell responses were observed in patients harbouring those mutations.65 cytotoxic t - lymphocyte responses to frameshifted proteins have been detected in healthy hereditary non - polyposis colorectal cancer - mutation carriers , raising the possibility of protective immunosurveillance in this population.66 frameshift neoantigens are particularly pertinent in the context of mismatch repair - deficiency , which is a pancancer event , and crucially , frameshifts commonly occurring in microsatellite instability - high colorectal carcinomas have been shown to generate nmd - resistant transcripts.67 in support of this , in a study68 of pd - 1 blockade in patients with microsatellite instability - high tumours from various cancer subtypes , functional analyses in - vivo in a responding patient showed expansion of frameshift neoantigen - specific t - cell clones . frameshift neoantigens provide a unique opportunity to target common tumour - suppressor genes , such as such as tp53 and bap1 , 69 and their founder status also enriches for clonal neoantigens . 
neoantigens derived from driver mutations elicit profound t - cell exhaustion via chronic antigen stimulation , generating t - cell pools refractory to immune therapy.70 thus , early administration of checkpoint blockade might further improve clinical benefit in cancers with particularly antigenic mutations such as renal clear cell carcinoma . 
it is also noteworthy that a high differential affinity between wild - type and mutant peptides is indicative of enhanced tumour protection in vivo.71 the enrichment of mutant - only binders by nine times in neoantigens derived from frameshift mutations relative to nssnvs might therefore partly explain the predictive power of frameshift neoantigens in checkpoint inhibitor responses . a widely recognised challenge in bioinformatics is indel variant calling , due to the inherent nature of shortread sequencing technology ; however , accurate indel calling can be achieved within both a research and clinical context with strict quality control procedures.72 while strict quality control procedures can ensure a low false - positive rate , as a consequence the true rate of indel mutations might be underestimated . in conclusion , we report that kidney cancers carry the indel mutations . 
 highest pan - cancer burden of futhermore , our data suggest that frameshift indels are a highly immunogenic mutational class ; triggering an increased quantity of neoantigens and greater mutant binding specificity . 
collectively , these data might reconcile the outlier nature of immunotherapy responses in renal clear cell carcinoma , highlighting frameshift indels as a potential biomarker of checkpoint inhibitor response and supporting targeting of clonal frameshift indels by both vaccine and cell therapy approaches . the contributors st , kl , and cs designed the study and wrote the manuscript . 
all authors interpreted the data . declaration of interests st reports grants from ventana , outside the submitted work ; and has a patent on indel burden and checkpoint inhibitor response pending , and a patent on targeting of frameshift neoantigens for personalised immunotherapy pending . 
 nm reports personal fees from achilles therapeutics , outside of the submitted work ; and has two patents pending ( pct / ep2016 / 059401 and pct / ep2016 / 071471 )  . 
 jl reports personal fees from eisai , glaxosmithkline , kymab , roche / genentech , secarna , pierre fabre , and eusa pharma ; and grants and personal fees from bristol - myers squibb , merck sharp & dohme , pfizer , and novartis , outside of the submitted work . 
cs reports personal fees from janssen , boehringer ingelheim , ventana , novartis , roche , sequenom , natera , achilles therapeutics , and sarah cannon research institute , and personal fees and other from apogen biotechnologies , epic sciences , and grail , outside of the submitted work ; and has a patent on indel burden and checkpoint inhibitor response pending and a patent on targeting of frameshift neoantigens for personalised immunotherapy pending . 
all other authors declare no competing interests . vol 18 august 2017 1019 articles acknowledgments st is funded by cancer research uk ( grant reference number c50947 / a )  . 
tc , st , mg , and jl are funded by the national institute for health research ( nihr ) biomedical research centre at the royal marsden hospital national health service foundation trust ( st grant reference number a109 )  . 
cs is funded by cancer research uk ( tracerx ) , the rosetrees trust , novonordisk foundation ( id 16584 ) , eu fp7 ( projects predict and responsify , id number 259303 ) , the prostate cancer foundation , the breast cancer research foundation , the european research council ( theseus ) , and national institute for health research university college london hospitals biomedical research centre . 
we thank levi garraway , eli van allen , alexandra snyder , matthew hellman , naiyer rizvi , and timothy chan for kindly allowing access to their checkpoint inhibitor datasets . 
 we aimed to assess the e ectiveness of imiquimod cream versus surgical excision in patients with low - risk basal - cell carcinoma . methods we did a multicentre , parallel - group , pragmatic , non - inferiority , randomised controlled trial at 12 centres in the uk , in which patients were recruited between june 19 , 2003 , and feb 22 , 2007 , with 3 year follow - up from june 26 , 2006 , to may 26 , 2010 . 
participants were randomly assigned ( 1 : 1 ) via computer - generated blocked randomisation , strati ed by centre and tumour type , to receive either imiquimod 5% cream once daily for 6 weeks ( super cial ) or 12 weeks ( nodular ) , or surgical excision with a 4 mm margthe randomisation sequence was concealed from study investigators . 
the primary outcome was the proportion of participants with clinical success , de ned as absence of initial treatment failure or signs of recurrence at 3 years from start of treatment . 
at 3 years , 178 ( 84% ) of 213 participants in the imiquimod group were treated successfully compared with 185 ( 98% ) of 188 participants in the surgery group ( rr 084 , 98% ci 078091 ; p < 00001 )  . 
we recorded serious adverse events in 99 ( 40% ) of 249 participants in the imiquimod group and 97 ( 42% ) of 229 in the surgery group had serious adverse events , but none were regarded as related to treatment . 
12 ( 5% ) participants in the imiquimod group withdrew because of adverse events compared with four ( 2% ) in the surgery group . interpretation imiquimod was inferior to surgery according to our prede ned non - inferiority criterion . 
the incidence of basal - cell carcinoma is increasing worldwide by up to 10% per year , 1 and is also increasing in young people.24 skin cancer is a growing health problem and puts a substantial burden on the resources of health - care systems.5 , 6 although various treatment options are available for patients with low - risk basal - cell carcinoma , surgery is regarded as the gold standard.7 surgical largely done by treatment dermatologists and plastic surgeons , although treatment of low - risk disease can be undertaken by other healthcare professionals with additional skills in skin cancer eg , by family doctors or by professionals at local community hospital or treatment centres.8 studies identi ed in our previous systematic review7 have reported successful treatment with imiquimod cream ; with 8788% of patients with super cial basalcell carcinoma , using a once - daily regimen for 6 weeks being successfully treated , and 76% of patients with nodular disease following once - daily treatment for vol 15 january 2014 articles 12 weeks.7 , 9 however , none of these studies compared imiquimod with surgery . 
the medicine is licensed in a cream form to be applied by patients for the treatment of external genital warts , super cial basal - cell carcinoma , and actinic keratoses in adults.1012 we postulated that topical imiquimod , although inferior to surgery , could still be an acceptable alternative because it might result in a better cosmetic appearance , especially for patients with low - risk basal - cell carcinomas of the face and neck , and because of the convenience of home application , plus possible cost and service savings . 
in this randomised study , we assessed whether imiquimod cream was noninferior to surgical excision for treatment of low - risk basal - cell carcinoma . methods study design and patients this multicentre , parallel - group , we undertook pragmatic , randomised , non - inferiority trial , in which patients were recruited between june 19 , 2003 , and feb 22 , 2007 , with 3 year follow - up in clinic from june 26 , 2006 , to may 26 , 2010 , and longer follow - up from patients notes from the last trial visit until up to 5 years and 4 weeks after the start of treatment . 
the study protocol has been previously published.13 eligible participants of any age had histologically con rmed , primary , previously untreated , nodular or super cial basal - cell carcinoma not arising at sites at high risk for subclinical tumour spread , including the nose , ear , eyelid , eyebrow , and temple.14 we excluded patients with morphoeic or recurrent basal - cell carcinoma and those with gorlin syndrome . the study had full ethics approval from the nottingham research ethics committee 2 ; all other sites had ethics approval . 
all participants gave written informed consent . randomisation and masking participants were randomly assigned ( 1 : 1 ) via computergenerated blocked randomisation to receive topical imiquimod 5% cream or surgical excision with a 4 mm marg the allocation sequence was prepared by the trent research and development support unit ( rdsu ; nottingham , uk ) and randomisation was strati ed by centre and type of basal - cell carcinoma . 
the trent rdsu recorded the name of the next participant to be recruited and logged the date of the telephone call against the participants identi cation number before specifying the 947 participants assessed for eligibility * 314 excluded at screening 446 not randomised * 44 did not meet inclusion criteria 265 declined to participate 4 not suitable 1 too frail 132 excluded just before randomisation 501 randomised 5 did not begin treatment 5 had lesions that were not basal - cell carcinomas 7 died 6 were non - contactable or had 31 lost to follow - up 10 unwilling or unable to attend moved 5 had adverse events 2 had possibly treatment - related adverse events|| 1 had previously treated basal - cell carcinoma 11 did not begin treatment 7 did not accept treatment 2 for whom treatment was considered unsuitable by doctor 1 was too ill 1 was confused about dates 41 lost to follow - up 20 unwilling to continue 9 had lesions that were not basal - cell carcinomas 7 died 5 were non - contactable or had moved 254 assigned to imiquimod 247 assigned to surgery 249 received allocated intervention 236 received allocated intervention 218 at 3 year follow - up 195 at 3 year follow - up 5 not analysed 5 had a missing primary endpoint 7 not analysed 2 had a missing primary endpoint 5 had had the wrong procedure done by mistake * * 213 analysed 188 analysed figure : trial pro le * numbers who saw the nurse were not available from some smaller centres ; an unknown greater number saw a doctor in clinic before assessment ; potential participants were directed to the nurse who explained the study . 
because of unsuitable histology , death , poor health , regression of basal - cell carcinoma , participant was no longer available for follow - up or was unable to reach . 
i = pale skin , burns very easily and rarely tans ; ii = fair skin that usually burns , but can gradually tan ; iii = skin that burns with long or intense exposure to the sun , but generally tans quite easily ; iv = olive - coloured skin that always tans easily , but could possibly burn with lengthy exposures to intense sunshine ; v = naturally brown skin , with brown eyes and dark hair ; skin darkens easily with sun exposure and only burns with excessive exposure to the sun ; vi = black skin with dark brown eyes and black hair ; skin very easily darkens further on exposure to sun and would very rarely , if ever , burn . 
three ( 1% ) patients with other skin cancers in the imiquimod group , and seven ( 3% ) with other cancers in the surgery group had a previous history of invasive melanoma . table 1 : baseline and demographic characteristics procedures treatment duration and frequency of dosing for imiquimod 5% cream were based on results from previous studies.15 after the start of this study , imiquimod was licensed for treatment of super cial basal - cell carcinoma , with a 5 days per week dosing regimen . 
for patients with nodular disease , total application time was for 12 weeks . participants received an instruction sheet for how to apply the cream ( separate sheets for nodular and super cial tumours )  . 
if a participant could not tolerate the cream because of sidee ects , they were advised to stop treatment for a week and then restart at a frequency of 5 days a week . 
if this schedule was tolerated , the participant could go back to 7 days a week ; if not , or if 7 days a week was not tolerated , a second time , they could go back to 5 days a week after a further rest period of 1 week . 
 we chose the 3 year timepoint for the primary endpoint because it was the last planned face - to - face visit that would enable measurement of clinical response in a way that would match clinical practice , and because 67% of recurrences of basal - cell carcinoma happen within the rst 3 years after treatment.16 secondary outcomes were clinical success at years 1 , 2 , and 5 ( 5 year data are not yet available ) ; time to rst failure ( as strati ed into within 1 year , between 12 years , and between 23 years ) ; cosmetic appearance of lesion site as rated by the participant and dermatologist assessor ; pain during treatment and in the 16 weeks of follow - up ; the number of days the participant had moderate or severe pain during treatment and in the 16 week follow - up ; and cost - e ectiveness of imiquimod versus surgery . statistical analysis the original sample size for non - inferiority was based on a prestudy survey of uk dermatologists ( unpublished data ) , which suggested that imiquimod needed to have roughly a 90% minimum chance of clinical success to vol 15 january 2014 articles change practice , compared with a success rate of 97% for surgery . 
we explored how the lower boundary of the ci varied for a range of sample sizes whereas all other assumptions used in the original calculation of sample size remained the same . 
this calculation showed that with a total sample size of 500 , the lower limit of the con dence boundary of the imiquimod response rate would be 83% , and the additional gain in power from increasing the sample size to 550 and then to 600 was small . 
the precision of the response rate estimate for imiquimod would be within 10 percentage points of the actual imiquimod success rate for a sample size of 500 , which was deemed acceptable to change practice . 
the noninferiority margin based on these gures is a relative risk of 087 ( lower boundary of a 98% ci for the relative di erence in e ect expressed as a relative risk ) , and only applies to the primary outcome . 
the sample size and choice of non - inferiority margin are fully reported in the study protocol.13 all analyses were done according to the protocolspeci ed statistical analysis plan , apart from the coste ectiveness analysis , which we did with a di erent method to that originally planned because the rst method was no longer appropriate . 
we did a modi ed intentionto - treat analysis on the full dataset , de ned as all randomised participants with a histologically con rmed basal - cell carcinoma lesion who met the inclusion criteria and received at least one application of imiquimod cream or surgery , and for whom the outcome being analysed was available . 
this analysis started with the modi ed intention - to - treat population , with additional exclusion of patients who did not comply with the protocol procedures : those who received insu cient imiquimod ( less than two - thirds of required dosing ) , those who had surgery by mistake after imiquimod , those who had additional surgery for early failure , and those who had complete curettage plus cryosurgery instead of biopsy for presumed treatment failure ( histology negative )  . we did sensitivity analyses for missing data for two measures : ( 1 ) the primary outcome measure ( assuming the worst - case scenario of all participants with missing data having recurrence or treatment failure and the bestcase scenario of all participants with missing data having been successfully treated ) ; and ( 2 ) time to failure ( assuming the worst - case scenario with missing data replaced with the earliest time and the best - case scenario with missing data replaced with the latest time )  . 
in tumour , and subgroup analyses for the primary outcome we assessed whether the intervention e ect varied by tumour type ( super cial vs nodular ) , tumour site ( head and neck vs other sites ) , and tumour size ( 15 mm vs > 15 mm diameters ) , by incorporation of an interaction term between treatment group and the covariate of interest in the regression models.17 for the primary outcome , we calculated the number and proportion of participants successfully treated at 3 years in each group , and the absolute di erence in percentages between groups together with corresponding 98% cis . 
we used poisson regression with a robust error variance to estimate the treatment e ect as a relative risk.18 we analysed secondary outcome measures with the same method as that for the primary outcome variable . 
we rated the cosmetic outcome as excellent , good , fair , poor , very poor , and unable to see lesion , and we classed evaluable lesions as a success if they had an excellent or good appearance . 
we assessed pain daily on a scale consisting of no pain , and mild , mild to moderate , moderate , moderate to severe , and severe pain ; we took pain during treatment to mean at least moderate pain on any one of the days during treatment . 
one less participant because the time category of failure was unknown for that participant ; this individual is included in the sensitivity analyses . table 3 : patients who failed treatement as strati ed by timepoints , by type of basal - cell carcinoma and treatment group ( modi ed intention - to - treat analysis ) ( one of ve between - assessment time intervals ) was analysed with a continuation ratio model with a complementary log - log link to estimate hazard ratios ( hrs ) , and we used descriptive statistics to summarise the pain outcomes . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit it for publication . results the gure shows the trial pro le . 
five ( 2% ) participants did not receive the intervention in the imiquimod group and 18 ( 7% ) did not receive the intervention in the surgery group ( gure 1 )  . 
seven ( 39% ) of these 18 participants in the surgery group had a di erent surgical procedure done by mistake : two of these were lost to follow - up , but the remaining ve were followed up to year 3 and excluded from the modi ed intention - to - treat analysis ( gure 1 )  . 
 five ( 31% ) of these 16 patients in the surgery group had a di erent surgical procedure done by mistake but were followed up to year 3 and excluded from the modi ed intention - to - treat analysis ( gure 1 )  . 
31 ( 12% ) participants in the imiquimod group and 41 ( 17% ) in the surgery group were ( 2% ) further participants in the imiquimod group and two ( < 1% ) in the surgery group had a missing end point , leaving 401 ( 80% ) patients for the modi ed intention - to - treat analysis at year 3 ( gure 1 )  . to follow - up ; ve lost enrolled ( table 1 )  . 
two - thirds of participants did not previously have basal - cell carcinoma ( table 1 )  . at 3 years in the modi ed intention - to - treat population of 213 patients in the imiquimod group , and 188 patients in the surgery group , signi cantly fewer participants were successfully treated in the imiquimod group than in the surgery group ( table 2 )  . 
the lower limit of the 98% ci for successful treatment at 3 years ( 078 ) was less than the prespeci ed non - inferiority margin ( 087 ) , and the upper limit was less than 10 ( table 2 ) ; therefore , imiquimod was inferior to surgery . 
 similar results were shown in the per - protocol analysis of 202 patients in the imquimod group and 187 patients in the surgery group ( table 2 ) and results were unchanged in sensitivity analyses for missing data ( data not shown )  . the type of basal - cell carcinoma did not a ect the di erence in outcome between those treated with imiquimod and surgery . 
 our planned subgroup analysis showed clinical response rates of 92% ( 138 / 150 patients ) for super cial lesions of 15 mm or less versus 89% ( 55 / 62 ) for lesions of more than 15 mcorresponding values for nodular lesions were 90% ( 138 / 153 ) and 89% ( 32 / 36 ) , respectively . 
after 1 and 2 years of followup , fewer patients , for whom the outcome data were available , were successfully treated in the imiquimod group than in the surgery group ( table 2 )  . in the 3 - year modi ed intention - to - treat population , signi cantly more tumours recurred or did not go away in patients in the imiquimod group in the rst year of follow - up from start of treatment than in those in the surgery group ( table 3 )  . 
participants in the imiquimod group had a shorter time to failure than did those in the surgery group ( hr 008 , 98% ci 002032 , table 3 )  . baseline characteristics were similar between the two groups ( table 1 )  . 
median age of the participants was 68 years ( range 3092 ) and more men than woman were data for participant - rated cosmetic appearance ( at all sites ) did not di er signi cantly between groups at 6 months and 3 years ( appendix )  . 
 table 4 : cosmetic appearance of lesion ( excellent or good ) at 6 months and 3 years as rated by two independent dermatologists 117 patients in the imiquimod group and 109 patients in the surgery group , at 6 months , and in 160 imiquimod treated patients and 166 surgery patients at 3 years ; data were missing because patients could not see the lesion sites , and at 6 months for some participants because we changed the scale we used . 
pictures were available for independent review for 213 patients treated with imquimod and 195 patients treated with surgery at 6 months , and 170 and 174 patients , respectively , at 3 years . 
cosmetic appearance at all sites di ered signi cantly between treatment groups in favour of imiquimod , as rated by two independent dermatologists using digital images , at 6 months and 3 years ( table 4 )  . data for pain during treatment were available for 242 patients treated with imiquimod and 201 patients treated with surgery . 
proportions for some events have not been provided if we deemed them unuseful ( eg , number of adverse events in the rst 6 months compared with those at 3 years , when criteria changed for collection of such events after 1 year )  . 
adr = possibly treatment related adverse event . table 6 : number of participants who had adverse events and number of adverse events ( safety dataset ) withdrew because of adverse events ( ve [ 42% ] of these events were treatment related , three [ 25% ] were part of treatment failure , and two [ 17% ] were non - related events leading to death as reason for withdrawal )  . 
four ( 2% ) of 229 participants withdrew because of adverse events in the surgery group ( all non - related events , three [ 75% ] of which led to death )  . 
 15 ( 6% ) of 249 patients were assessed to have received insu cient imiquimod from compliance diaries , sachet returns , and dose reductions ( appendix )  . the appendix shows results of the cost - e ectiveness analysis . discussion our ndings show that imiquimod is inferior to surgery for treatment of basal - cell carcinoma because it failed to reach our prede ned non - inferiority margin after 3 years of follow - up . 
slightly more participants in the imiquimod group reported pain on treatment than in the surgical group , although direct comparisons were di cult because treatment times di ered substantially and pain relief was often given routinely after surgery . 
more patients had adverse events when treated with the cream than those in the surgery group ; however , more patients who underwent surgery had adverse events in the followup period . 
the total costs between treatment methods were not signi cantly di erent . the proportion of patients who had successful treatment with topical imiquimod for super cial basalcell carcinoma at 1 year in our study is similar to those ( 8788% ) reported in our cochrane review , 7 and in a subsequent review that included non - randomised trials , which reported a pooled estimate of 862% ( 95% ci 8290 ) for the proportion of patients with a complete response.9 834% of patients with super cial basal - cell carcinoma treated with topical imiquimod used ve times per week responded to treatment as assessed after 12 months in a recent study from the netherlands , treated with compared with 728% of patients photodynamic therapy and 801% of patients treated with uorouracil cream.19 findings from another study suggested that thicker lesions ( > 04 mm thickness ) might be much more likely to recur than thin lesions.20 in our study , where patients were treated with imiquimod daily , more patients with nodular basal - cell carcinoma were successfully treated at 1 year compared with another study that used imiquimod three times a week for either 8 weeks or 12 weeks and reported a successful treatment of 64% of patients , 21 and with a review that suggested a 76% treatment response for nodular tumours.7 an open - label study of imiquimod ( used once daily for 6 weeks ) for super cial basal - cell carcinoma reported a 10% cumulative recurrence at 3 years.22 another open label study23 of imiquimod ( ve times a week for 6 weeks ) for super cial basal - cell carcinoma showed a cumulative recurrence of 86% at 3 years . we did not rebiopsy patients with basal - cell carcinoma given topical imiquimod to con rm tumour clearance because this population would not be routinely biopsied if the lesion were regarded as clinically clear . 
furthermore , a biopsy scar would have a ected the cosmetic result for 102 vol 15 january 2014 articles imiquimod ( n = 249 ) surgery ( n = 229 ) panel : research in context patients who had higher frequency mild or moderate adverse events * cold or u - type symptoms or feeling of unwell 53 ( 21% ) 21 ( 9% ) itching at tumour site weeping at tumour site new basal - cell carcinoma erythema or redness at tumour site small spots or pimples close to trial tumour headache scab on tumour site soreness of tumour site bleeding at tumour site pain at tumour site swelling at tumour site 211 ( 85% ) 129 ( 56% ) 160 ( 64% ) 81 ( 35% ) 64 ( 26% ) 55 ( 24% ) 56 ( 22% ) 9 ( 4% ) 39 ( 16% ) 38 ( 17% ) 33 ( 13% ) 30 ( 12% ) 1 ( < 1% ) 5 ( 2% ) 24 ( 10% ) 16 ( 7% ) 21 ( 8% ) 12 ( 5% ) 10 ( 4% ) 8 ( 3% ) 17 ( 7% ) 19 ( 8% ) patients who had higher frequency severe , life - threatening , or disabling events cold or u - type symptoms in ammatory reaction to treatment heart attack or heart failure pneumonia 7 ( 3% ) 4 ( 2% ) 3 ( 1% ) 1 ( < 1% ) 4 ( 2% ) 4 ( 2% ) data are n ( % ) , unless otherwise indicated . 
 > 1% in either group table 7 : number of participants who had higher frequency mild or moderate or severe , life - threatening , or disabling adverse events of all types ( safety dataset ) imiquimod , which was an important outcome to measure in this study . topical imiquimod treatment versus few studies have compared the cost - e ectiveness of for surgical super cial basal - cell carcinoma . 
one study24 estimated the mean cost per patient given imiquimod 5% cream to be lower than that of a patient assigned surgery for a super cial basal - cell carcinoma ( 621 vs 676 euros ) , but costs associated with treatment of initial treatment failures or recurrences were not addressed . 
another study25 compared the cost of imiquimod with surgery and reported imiquimod to be more cost e ective in the short term but more expensive in the long ter one study26 compared the cost - e ectiveness of imiquimod with that of a range of other treatments and showed the cost of imiquimod to be higher . 
future studies might compare other treatments used for low - risk basal - cell carcinomas , such as electrodesiccation and curettage , with topical imiquimod or photodynamic therapy . to our knowledge this study is the rst large , independent , pragmatic study comparing imiquimod with surgery in a wide range of patients who might typically be considered for such treatment in primary care ( panel )  . 
selection bias was unlikely due to strong concealment of the allocation sequence , and the modi ed intention - to - treat analysis shows similar results to our per - protocol analysis . 
there were few missing data for the risk factors we adjusted for , so this systematic review we did a cochrane systematic review of interventions for basal - cell carcinoma when planning our study in 2002 , which we then updated in 2007.7 in the cochrane review we searched six databases and contacted companies and identi ed 27 randomised controlled trials of mainly poor quality as judged by method of randomisation , allocation concealment , blinding , and whether an intention - to - treat analysis and unit of analysis issues were considered . 
nine short - term studies combined using a random - e ects model suggested a success rate of 87% for imiquimod in the treatment of super cial basal - cell carcinoma with a once - daily regimen for 6 weeks , and a 76% treatment response with treatment of nodular basal - cell carcinoma for 12 weeks , when measured histologically . 
we then searched pubmed and central from january , 2006 , to june , 2013 , with the same terms as used in our cochrane review , to identify new relevant studies of interventions for basal - cell carcinoma . 
 none of the newly identi ed studies directly compared topical imiquimod with excisional surgery . interpretation to our knowledge this study is the rst large , independent , pragmatic study comparing imiquimod with surgery in patients who might typically be considered for such treatment in primary care . 
the study provides a useful estimate of response rates for topical imiquimod in clinical practice for both low - risk super cial and nodular basal - cell carcinoma at 3 years . 
topical imiquimod might still be a useful treatment option for people with low - risk basal - cell carcinomas who have more than one super cial basal - cell carcinoma , those treated in primary care where success rates for excisional surgery can be considerably lower than in secondary care , and for those who prefer to use a cream at home , especially since recurrences are usually easy to identify and deal with surgically . 
however , none of these treatments have been assessed long term , except for photodynamic therapy , 27 which has shown similar long - term response rates to those reported for imiquimod in this study . issue had little e ect on the number of participants on which our regression models were based . 
additionally , some of the surgeons were trained in advanced surgery vol 15 january 2014 articles and were therefore not typical primary - care or secondarycare professionals , which means that the surgical results in this study might have been better than what would be observed in general practice . 
 in terms of external validity , the study could have favoured slightly younger people with basal - cell carcinoma who were more mobile than some of the older and more frail patients who declined to participate ; the study were furthermore , motivated about topical imiquimod , which was not licensed for basal - cell carcinoma at the start of the study . the prospect of use of individuals entering for leads imiquimod cream although our study showed imiquimod to be inferior to surgery according to our prede ned non - inferiority margin , others might consider the overall success rate at 3 years still clinically useful , especially because low - risk recurrences of basal - cell carcinoma can be treated . 
in other words , some policy makers might consider use of topical imiquimod as part of a sequential treatment approach that treats most people with low - risk lesions successfully at home and those who fail with surgery . 
mo was the study coordinator and was on the trial management group ; updated the protocol as necessary ; obtained ethics amendment approvals ; supervised the study nurses ; designed the data capture forms ; wrote instruction documents as needed ; built and maintained the database ; ensured data quality , including double data entry and 100% checks ; prepared datasets for analysis , interpretation , and tabulation of the results , and contributed to writing of the nal report . 
 sa was the trial statistician and a member of the trial management group , participated in the design of the study , commented on revisions of the protocol , wrote the study analysis plan , did the statistical analysis , and contributed to the drafting of this manuscript and the interpretation of the results . 
hw contributed to the funding proposal , the main protocol , was chief investigator , and contributed to trial delivery , interpretation of the results , and writing of the nal report ; wp recruited patients , was on the trial management group , and contributed to interpretation of results and approval of the nal report ; gc recruited patients , was on the trial management group , and contributed to interpretation of results and approval of the nal report . 
pm contributed to the funding proposal and the main protocol , was study health economist , designed and implemented the cost - e ectiveness analyses , and contributed to the drafting of this manuscript . con icts of interest we declare that we have no con icts of interest . acknowledgments the study was nanced by cancer research uk . 
we investigated infertility and time to pregnancy in female childhood cancer survivors , and analysed treatment characteristics associated with infertility and subsequent pregnancy . methods the childhood cancer survivor study ( ccss ) is a cohort study including 5 year cancer survivors from 26 canadian and us institutions who were younger than 21 years at the time of diagnosis between jan 1 , 1970 , and dec 31 , 1986 , and a sibling control group . 
self - reported infertility , medical treatment for infertility , time to rst pregnancy in survivors and siblings , and the risk of infertility in survivors by demographic , disease , and treatment variables were analysed . findings 3531 survivors and 1366 female sibling controls who enrolled between nov 3 , 1992 , and april 4 , 2004 , were included . 
compared with their siblings , survivors had an increased risk ( relative risk [ rr ] 148 [ 95% ci 123178 ] ; p < 00001 ) of clinical infertility ( ie , > 1 year of attempts at conception without success ) , which was most pronounced at early reproductive ages ( rr 292 [ 95% ci 118720 ] , p = 0020 , in participants 24 years ; 161 [ 105248 ] , p = 0029 , in those aged 2529 years ; and 137 [ 111169 ] , p = 00035 , in those aged 3040 years )  . 
despite being equally likely to seek treatment for infertility , survivors were less likely than were their siblings to be prescribed drugs for treatment of infertility ( 057 [ 95% ci 046070 ] , p < 00001 )  . 
although survivors had an increased time to pregnancy compared with their siblings ( p = 0032 ) , 292 ( 64% ) of 455 participants with self - reported clinical infertility achieved a pregnancy . interpretation a more comprehensive understanding of infertility after cancer is crucial for counselling and decision making about future conception attempts and fertility preservation . funding national cancer institute , american lebanese syrian associated charities , swim across america . introduction substantial improvements in cancer treatment have greatly increased 5 year survival for childhood cancers , which now exceeds 80% in the usa.1 infertility is reported as a major concern about the long - term e ects of female cancer survivors.2 , 3 treatment , especially menstruation is not a sensitive way to identify the gonadotoxic e ects of treatment and many survivors of childhood cancer are at risk of unrecognised infertility.4 the risk of non - surgical premature menopause in childhood cancer survivors is increased compared with that in their siblings , with a cumulative incidence of 8% by age 40 years.5 furthermore , childhood cancer survivors are less likely to become pregnant than are their siblings.6 , 7 likelihood of pregnancy as a measure of fertility does not take into account individual desires for childbearing or attempts at pregnancy and thus does not assess infertility . 
therefore , previous studies might the prevalence of have underestimated the risk of infertility in survivors of childhood cancer . we quanti ed the risk of infertility in survivors of childhood cancer on the basis of clinical de nitions of infertility and treatment characteristics in childhood cancer that increase the risk of infertility . 
additionally , we assessed if the length of time to pregnancy is longer in survivors of childhood cancer than in their siblings who have conceived . identi ed disease and methods study design and participants details of design , cohort characteristics , and baseline data collection of the childhood cancer survivor study ( ccss ) have been published previously.8 , 9 brie y , ccss is a collaborative study at 26 clinical centres in canada and the usa in which a cohort of 5 year cancer survivors who were diagnosed with an eligible malignancy before age 21 years between jan 1 , 1970 , and dec 31 , 1986 , was assembled . 
eligible malignancies were leukaemia , cns cancer , hodgkins lymphoma , vol 14 august 2013 articles lymphoma , wilms non - hodgkin tumour , neuroblastoma , soft - tissue sarcoma , and bone tumours . 
the next - of - kin ( usually parents or spouse ) of patients who had survived at least 5 years but subsequently died was contacted . participants in the ccss are required to complete a baseline questionnaire when they join the study . 
for our study , we included women who were aged 1839 years when they completed the baseline questionnaire between nov 3 , 1992 , and april 4 , 2004 , who reported they had ever been sexually active . previously published ccss data8 show no di erences in clinical or demographic characteristics between participants in the study and non - participants , other than a high rate of non - participation in the next - of - kin of patients who had died and a somewhat low proportion of male participants . 
written institution approved consent was obtained from all participants . procedures data about disease and treatment characteristics ( type and dose of chemotherapeutic drugs ; radiation eld size , 20 690 eligible survivors 17 632 available survivors 14 358 completed baseline questionnaire 3058 lost to follow - up after tracing 3274 chose not to participate 3962 were < 18 years or 10 827 were excluded active * 40 years at contact 5618 were male 1247 were never sexually 3531 women aged 1839 years who reported ever being sexually active comprised the study population figure 1 : flowchart of cancer survivor cohort included in infertility analyses * includes uncertain or incomplete data . site , and dose ) were gathered by medical record abstraction at each collaborating institution.5 the total exposure to alkylating agents was quanti ed with the alkylating agent score , which accounted for the number of alkylating agents given and the doses of each individual agent ( total dose per m of body surface area )  . 
distribution of doses of each alkylating agent was determined and each patient was assigned a score of 0 to 3 for each drug ( 0 represents no exposure and 1 , 2 , and 3 represent the lower , middle , and upper tertile of doses of that drug , respectively )  . 
doses of individual alkylating agents used to derive the score have been previously published.6 individual drug scores for each patient were summed , and an overall score of 0 to 3 was assigned.10 individual chemotherapeutic drugs , bone marrow transplantation , history of relapse , and history of second malignancy before completion of the baseline questionnaire were deemed additional exposures . 
doses of radiation therapy to the ovaries , uterus , and hypothalamus pituitary were estimated as previously described by stovall and colleagues.11 , 12 to become pregnant , without we used two de nitions of infertility . 
the rst , clinical the commonly accepted infertility , was based on de nition for infertility and included anyone who responded yes to the question , was there ever a period in your life when you and a partner tried for 1 year or more success ? .13 the second de nition , total infertility , included clinically infertile women and those who reported ovarian failure , which was de ned as never having had a menstrual period or menstrual periods stopping 5 years or more before the baseline questionnaire . 
patients were asked to recall any instance of infertility that occurred up to the time of the baseline questionnaire . participants who reported at least one pregnancy at any point after their cancer diagnosis were asked to complete a pregnancy questionnaire , which included questions about whether the pregnancy was planned , and , if so , how many months the participant tried to get pregnant for . 
we did not ask patients when they began trying to become pregnant or when they experienced infertility , and therefore could not account for individual di erences in follow - up time . 
inclusion of covariates in the multivariate models was based on clinical judgment and examination of the univariate estimates . 874 vol 14 august 2013 articles analyses subsequent risk of total infertility and clinical infertility were rst assessed in a model comparing survivors and siblings . 
potential factors for inclusion in multivariate models were age at baseline questionnaire , race , education level , smoking status , and body - mass index ( bmi )  . 
we postulated that the risk of infertility would increase with age and that the relative risk of infertility in survivors versus siblings would fall with age at time of baseline questionnaire . 
in view of the high correlation between these variables , we could not t a multivariate model included both uterine that radiotherapy dose and maximum ovarian radiotherapy dose , and thus uterine dose is reported in this study to exposure . 
 we used a modi ed poission regression with robust variance estimates for all relative risk ( rr ) estimates and 95% cis.14 and gonadal from and on the basis of data from the supplemental pregnancy questionnaire , we compared time to rst conception between survivors and siblings , who were included if they reported at least one planned pregnancy . 
to describe di erences between groups de ned by survivor status ( ie , survivor vs sibling ) , or among survivors between treatment exposures , we examined empirical cumulative distribution plots and used wilcoxon rank - sum or kruskal - wallis tests . 
we used sas ( version 9.2 ) for all statistical analyses . role of the funding source the study sponsors had no role in study design ; collection , analysis , or interpretation of data ; writing of the article ; or the decision to submit for publication . 
jsn and wml had full access to raw data , and the corresponding author had full access to all the data and the nal responsibility to submit for publication . results 20 690 survivors were eligible for inclusion , 3058 ( 15% ) of whom could not be located after intensive tracing e orts . 
4775 eligible siblings were contacted and 4023 ( 84% ) participated . 14 358 of the 17 632 ( 81% ) survivors contacted provided a baseline questionnaire ( gure 1 ) and 3531 were eligible for inclusion . 
n = 208 in the survivor group and 75 in the sibling group . table 2 : comparison of infertility and use of medical services for infertility between survivors and their siblings group . 
2894 of 3531 ( 82% ) survivors and 1186 of 1366 ( 87% ) siblings were still menstruating at the time of the baseline questionnaire . compared with their siblings , cancer survivors had an increased risk of both clinical and total infertility . 
 after adjustment for known sociodemographic and behavioural risk factors , the rr of clinical infertility in survivors siblings was 148 ( 95% ci 123178 ; p < 00001 )  . 
this adjusted risk was more pronounced at younger ages at study participation ( rr 292 [ 95% ci 118720 ] , p = 0020 , in participants 24 years ; 161 [ 105248 ] , p = 0029 , in those aged 2529 years ; and 137 [ 111169 ] , p = 00035 , in those aged 3040 years )  . compared with their the likelihood of visiting a doctor for infertility did not di er between survivors and siblings who reported clinical infertility , neither did the likelihood of the doctor nding a reason for infertility ( table 2 )  . 
however , survivors were signi cantly less likely than were their siblings to receive drugs to help them become pregnant ( rr 057 [ 95% ci 046070 ] , p < 00001 ; table 2 )  . 
 we noted signi cant unadjusted increases in risk of infertility in female cancer survivors who were older at childhood cancer diagnosis , older at study entry , currently or previously married , or current smokers and those with high bmis or lower educational attainment ( table 3 )  . 
in adjusted models , only associations with older age ( ie , > 29 years vs 2429 years ) at the time of the baseline questionnaire ( rr 168 [ 95% ci 126224 ] ; p = 00004 ) , marital status ( currently married vs never married ; 791 [ 4581368 ] ; p < 00001 ) , and bmi ( > 30 kg / m vs 185 < 250 ; 171 [ 130226 ] ; p = 00002 ) remained signi cant . 
a signi cant association between age at primary diagnosis and infertility was not recorded after adjustment . in unadjusted models , cancer survivors with a history of lymphoma or who received any radiotherapy , total body irradiation , or radiotherapy to the abdomen or pelvis had an increased risk of infertility ( table 3 )  . 
 additionally , increasing doses of uterine radiotherapy , exposure to high cumulative doses of alkylating agents ( ie , an alkylating agent score of 3 ) , and pituitary radiation doses of 130 gy signi cantly increased the risk of infertility ( table 3 )  . 
in adjusted models , compared with no uterine radiotherapy , uterine radiotherapy doses of greater than 5 gy ( rr 248 [ 95% ci 154401 ] , p = 00002 , for 51100 gy ; 202 [ 127323 ] , p = 00032 , for 101200 gy ; and 195 [ 95% ci 119319 ] , p = 00080 , for > 200 gy ) signi cantly increased the risk of infertility , as did an alkylating agent score of 3 compared with a score of 0 ( 148 [ 110199 ] , p = 00093 )  . 704 participants reported a planned rst pregnancy . 
time to pregnancy did not di er signi cantly on the basis of alkylating agent score ( gure 2d )  . took signi cantly longer nearly two - thirds ( 292 of 455 [ 64% ] ) of survivors with self - reported clinical infertility achieved a pregnancy . 
 in adjusted analyses , infertile survivors who received more than 10 gy of uterine radiotherapy were signi cantly less likely to become pregnant than were those who were not exposed ( rr 033 for 10120 gy ; [ 95% ci 014075 ] , p = 00087 , 021 [ 008060 ] , p = 00023 for > 20 gy )  . 
referent. table 3 : unadjusted relative risk of clinical infertility by demographic , disease , and treatment characteristics in survivors of childhood cancer 878 vol 14 august 2013 articles p = 0032 p = 0045 sibling ( n = 253 ) survivor ( n = 423 ) no abdominal radiotherapy ( n = 284 ) any abdominal radiotherapy ( n = 94 ) p = 0091 p = 0088 no brain or head radiotherapy ( n = 287 ) any brain or head radiotherapy ( n = 90 ) time ( months ) time ( months ) figure 2 : time to rst pregnancy among survivors and siblings by group ( a ) , abdominal radiotherapy ( b ) , brain or head radiotherapy ( c ) , and alkylating score ( d ) for presentation purposes , plots were truncated at 40 months . 
however , all available data were used in estimations of distributions and group comparisons . score = 0 ( n = 138 ) score = 1 ( n = 49 ) score = 2 ( n = 37 ) score = 3 ( n = 27 ) discussion our data show an increased risk of infertility in childhood cancer survivors starting at a very young reproductive age . 
 however , nearly two - thirds of survivors with clinical infertility reported a pregnancy . than were infertility function , and counselling about treatment for childhood cancer has variable e ects on the reproductive likelihood of fertility in survivors remains challenging . 
 previous studies have characterised risk factors for childlessness or pregnancy , but did not assess a group of women who desired pregnancy and reported an inability to conceive within a year . 
to our knowledge , ours is the rst large study of female childhood cancer survivors to quantify the risk of infertility that is based on a clinical de nition and characterises the use and success of infertility treatments in this setting ( panel )  . survivors who had received radiotherapy to the brain had a signi cantly shorter time to pregnancy than did other survivors . 
survivors who receive high doses of brain radiotherapy might have substantial neurocognitive impairments and be less likely to partner or attempt pregnancy.16 the shortened time to pregnancy in this survivor group in our study is probably a result of selection bias for a good prognosis group that received low dose radiotherapy that did not a ect ovarian reserve . survivors were roughly half as likely to be medically treated for infertility as were their siblings , which is a cause for concern . 
 alternatively , reproductive medicine providers might have been uncomfortable with perceived medical comorbidities . take drugs after previous extensive vol 14 august 2013 articles panel : research in context systematic review we were familiar with previous childhood cancer survivor study work6 about the relative risk of pregnancy in childhood cancer survivors compared with their siblings . 
to our knowledge , no previous studies that included childhood cancer survivors have included direct measures of infertility . interpretation our data support earlier work showing that cancer therapies have negative gonadal e ects on young female cancer survivors , leading to an increased risk of infertility and childlessness . 
our data di er from those from other studies , which suggest that earlier age at cancer diagnosis is protective against the development of infertility , probably because our multivariate models were adjusted for treatment - related factors ( and sociodemographic variables associated with infertility )  . 
we noted an increased risk of infertility in cancer survivors at very young ages , even though most young female cancer survivors resume menstruation ( more than 50% of our cohort was aged < 30 years when they answered questions about infertility ) , showing that menstrual function does not equate to normal fecundity . 
clinicians should alert cancer survivors with ovarian function of the risk of infertility , and refer to reproductive specialists for possible fertility preservation if they are not ready to attempt conception . 
small uterine volumes , impaired blood ow , and endometrial damage might have roles in infertility or adverse pregnancy outcomes ( increased frequency of low birthweights and miscarriage , and fewer livebirths ) in survivors who received uterine radiotherapy.1720 independently of to our knowledge , our study is the most comprehensive investigation into infertility in childhood cancer survivors so far . 
importantly , previous ccss work did not show an overall higher risk of miscarriage or stillbirth in survivors than in their siblings , despite a lower rate of livebirths in survivors . 
additionally , previous reports19 have shown an increased rate of elective terminations in young survivors ( aged 2125 years ) , which lowers the livebirth rate but is not associated with fertility potential . 
women with ovarian failure were not included in the analysis of likelihood of pregnancy , and the proportion of infertile survivors achieving pregnancy would have been lower if that group had been included . 
because of the young age of our cohort ( median 276 years ) and the lower marriage rate in survivors than in their siblings , we might be underestimating the overall burden of infertility in their lifespan . 
previous reports2123 about childhood cancer survivors have shown diminished ovarian reserve even with regular menstruation and timely puberty , and studies15 , 24 of adult cancer survivors have shown that infertility . 
similarly , amenorrhoea underestimates survivors might be at risk for secondary infertility if they want more than one child . another important limitation of these data is that participants answered infertility questions starting in 1992 , when use of assisted reproduction such as in - vitro fertilisation was less common and less successful than it is now . 
 finally , antineoplastic treatments have evolved towards gonad - sparing regimens in some cases , and the late reproductive e ects of such regimens might be less pronounced than those of older regimens . 
however , alkylating agents and pelvic radiation are still used , which emphasises the importance of our analysis , especially in view of advances in reproductive technology . increased reproductive medicine o ers options for fertility preservation before cancer treatment . 
 the american society of clinical oncology recommends that oncologists should refer interested and appropriate patients to reproductive specialists as soon as possible.25 because assisted reproductive outcomes after cancer treatment seem poor , fertility preservation interventions are preferred at diagnosis when possible.26 fertility preservation techniques before ( or early in ) cancer treatment include oophoropexy and cryopreservation of oocytes , ovarian tissue , or embryos , and depend on demographic and clinical factors and resource availability . 
 importantly , multiple livebirths have been reported from ovarian freezing.2729 collaboration between oncologists and reproductive medicine providers might increase timely access to fertility preservation for patients in need and prevent provider bias when treating cancer survivors for infertility . modern tissue 880 vol 14 august 2013 articles contributors seb , jsn , esg , wml , ms , cas , llr , and ld had roles in design and conduct of the study ; collection , management , analysis , and interpretation of data ; and preparation , review , or approval of the article . 
 rew had roles in collection , management , analysis , and interpretation of data and preparation , review , or approval of the article . con icts of interest we declare that we have no con icts of interest . acknowledgments this study was funded by grant u24 ca55727 ( awarded to llr , the principal investigator ) from the us national cancer institute , support to st jude childrens research hospital from the american lebanese syrian associated charities , and support to ld from swim across america . correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections corrections published online november 22 , 2013 s1470 - 2045 ( 13 ) 70328 - 0 correction to lancet oncol 2013 ; 14 : 1279 , 1283 , 1285 correction to lancet oncol 2013 ; 14 : 1330 , 1333 , 1335 yamada y , takahari d , matsumoto h , et al . 
 leucovorin , fluorouracil , and oxaliplatin plus bevacizumab versus s - 1 and oxaliplatin plus bevacizumab in patients with metastatic colorectal cancer ( soft ) : an open - label , non - inferiority , randomised phase 3 trial . 
this has been corrected online as of dec 30 , 2013 . correction to lancet oncol 2013 ; 14 : 1295306 zhang j - x , song w , chen z - h , et al . 
 docetaxel or pemetrexed with or without cetuximab in recurrent or progressive non - small - cell lung cancer after platinum - based therapy : a phase 3 , open - label , randomised trial . 
 lancet oncol 2013 ; 14 : 132636in the online first version of this article ( published online nov 12 ) , in table 3 , all entries of ( > 1% ) should have read ( < 1% ) , and the rst two sentences of the third paragraph on page 1335 should state : a subsequent analysis of flex showed a signi cant association between egfr expression by immunohistochemistry and improved outcomes , with high egfr expression ( h - score 200 or higher ) being associated with improved overall survival , time - to - treatment failure , and a greater proportion of patients achieving objective responses when treated with cetuximab than when treated with cisplatin plus vinorelbine alone.13 there was no improvement in outcomes in the low h - score group ( h - score lower than 200 ) .13 these corrections were made to the print version of the article in the december issue of the journal , and have been made online as of nov 22 , 2013 . 
in table 1 , the entry for adenocarcinoma in the cetuximab and pemetrexed group should have read 161 ( 53% ) and the entry for all other diagnoses in the pemetrexed group should have read 41 ( 13% )  . 
in table 3 , in the cetuximab plus pemetrexed group , the entry for patients with one or more ctcae grades 12 should have read 89 ( 30% ) , that for grade 3 anaemia 16 ( 5% ) , for grade 4 infusion related reactions 5 ( 2% ) , and grade 3 lung infection 16 ( 5% )  . 
 in the pemetrexed group in the same table , the entry for patients with one or more grade 4 ctcae should have read 36 ( 12% ) and one or more grade 5 ctcae 10 ( 3% ) ; the entry for grade 12 diarrhoea should have read 36 ( 12% ) , that for grade 12 hyperglycaemia 10 ( 3% ) , and grade 12 maculopapular rash 39 ( 13% )  . 
 vol 15 january 2014 for the fda press release see newsevents / newsroom / pressannouncements / ucm560167.htm making precision oncology the standard of care on may 23 , 2017 , the us food and drug administration ( fda ) granted accelerated approval for pembrolizumab to treat adults and children with unresectable or metastatic solid tumours with high microsatellite instability ( msi - h ) or mismatch - repair deficiency ( dmmr )  . 
what is remarkable about this latest decision is that it is the first time the fdaor indeed any regulatory agencyhas approved a cancer drug on the basis of a molecular target rather than on the tissue of origin the wake of this decision , specific questions remain to be answered : why does pembrolizumab work so well in people with msi - h and dmmr ? will overall survival reflect the promising results from the interim endpoints ? will resistance develop , and in what form ? which toxicities will occur and what management will they need ? irrespective of these uncertainties , this action represents a major shift in thinking by the fda , and anticipates a potential transformation in the way clinical trials are designed and oncology is routinely practiced . 
despite the advent of molecularly targeted small - molecule inhibitors and antibodies , regulatory agencies have continued to approve drugs on the basis of tumour site , thus leaving patients who are often excluded from organ - specific clinical trials ( eg , those with rare cancers ) with few or no approved treatment options . 
various cancer hospitals have started to address this gap by using precision oncology tumour boards , in which difficult cases are discussed and triaged to appropriate clinical trials or to an application for an investigational new drug licence for off - label use . 
these tumour board reviews currently operate in parallel with conventional ( pathology - based ) tumour boards , but one can imagine their integration into a single multidisciplinary team meeting in the near future , in which cases are considered from both a genetic and histological perspective , and ideally at an early disease stage , when better outcomes can be expected . although approvals like the one for pembrolizumab can potentially enhance access to efficacious new drugs for patients with rare or otherwise difficult - totreat cancers , they can only do so if genetic testing is also part of standard care . 
indeed , many institutions are developing in - house testing at a fraction of the cost so that all patients are tested , and their results easily integrated into clinical services . 
the hurdle of securing affordable access to genetic testing is crucial ; drug approval without the means to identify those who will benefit undermines the gains made by approving the drug in the first place . interpretation , especially lower the fda moreover , frequently , increasingly approving treatments on the accelerated approval level of evidence when pathway , using a considering drugs for serious conditions with unmet medical need . 
while accelerated approval is a worthy goal , improving access to novel therapies sooner , it is not unknown for promising drugs in phase 1 and 2 trials to profoundly disappoint at later stages . 
therefore , continued evidence gathering is crucialand the uncertainty of benefit , despite approval , should be communicated to patients . clinical medicine has been embracing a precision perspective for years , but the latest decision by the fda might herald a new era of regulatory processes that will encourage hospitals to adopt a fully integrated precision oncology service , rather than running parallel processes with the attendant duplication in time and cost . 
the fdas shift in philosophy will hopefully have a profound effect on the provision of oncology services and increase the potential to improve outcomes for a far greater number of patients than ever before as another hurdle is removed in the quest towards precision oncology truly becoming the standard of care . 
 2013 ; 14 : 120007in table 3 of this article ( published online first on oct 17 , 2013 ) , the data in the mixed and metastatic columns for group 4 patients in cohort 2 were reversed ; the data for mixed recurrence should have been 2 ( 8% ) and for metastatic recurrence should have been 19 ( 76% )  . 
additionally , in table 4 , the data in the mixed and metastatic columns for group 4 patients were also reversed ; in patients who received chemotherapy the data for mixed recurrence should have been 2 ( 25% ) and for metastatic recurrence should have been 3 ( 38% ) , and in patients who received csi with or without chemotherapy , the data for mixed recurrence should have been 12 ( 20% ) and for metastatic recurrence should have been 43 ( 73% )  . 
 vol 15 april 2014 e154 correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
we assessed the effect on participation of sending invitations for breast screening with a timed appointment to women who did not attend their first offered appointment within the nhs breast screening programme ( nhsbsp )  . methods in this open , randomised controlled trial , women in six centres in the nhsbsp in england who were invited for routine breast cancer screening were randomly assigned ( 1 : 1 ) to receive an invitation to a second appointment with fixed date and time ( intervention ) or an invitation letter with a telephone number to call to book their new screening appointment ( control ) in the event of non - attendance at the first offered appointment . 
 randomisation was by sx number , a sequential unique identifier of each woman within the nhsbsp , and at the beginning of the study a coin toss decided whether women with odd or even sx numbers would be allocated to the intervention group . 
the primary endpoint was participation ( ie , attendance at breast cancer screening ) within 90 days of the date of the first offered appointment ; we used poisson regression to compare the proportion of women who participated in screening in the study groups . 
this trial is registered with barts health , number 009304qm . findings we obtained 33 146 records of women invited for breast cancer screening at the six centres between june 2 , 2014 , and sept 30 , 2015 , who did not attend their first offered appointment . 
participation within 90 days of the first offered appointment was significantly higher in the intervention group ( 2861 [ 22% ] of 12 807 ) than in the control group ( 1632 [ 12% ] of 13 247 ) ; relative risk of participation 181 ( 95% ci 170193 ; p < 00001 )  . 
this strategy can be easily implemented by the screening sites and , if combined with simple interventions , could further increase participation and ensure an upward shift in the participation trend nationally . 
whether the policy should vary by time since last attended screen will have to be considered . funding national health service cancer screening programmes and department of health policy research programme . copyright the author ( s )  . 
 introduction an important indicator of the public health impact of the national health service breast screening programme ( nhsbsp ) in the uk is the participation rate , defined as the percentage of women invited for screening who are screened adequately within 180 days of invitation ( usually referred to as uptake in official reports )  . 
in england , participation following routine invitation fell from 744% in 200405 to 713% in 201415 , 1 and we are seeing a decline for the fourth consecutive year in a row , approaching the national minimum standard of 70% . 
 in particular , participation among women invited for their prevalent ( first ) round of screening has decreased by an even greater amount ( from 701% in 200405 to 633% in 201415 ) .1 participation in breast cancer screening also tends to be lower in areas of socioeconomic deprivation than in wealthier areas.2 , 3 the nhsbsp invites women aged 5070 years to mammographic screening every 3 years . 
an age eligibility extension to invite women aged between 47 years and 73 years is currently being for non - attenders of the first offered appointment is to send trialled.4 the usual practice 972 vol 18 july 2017 articles research in context evidence before this study we searched the pubmed database with the keywords breast cancer , breast screening , appointment , and non - attenders for articles in english published between jan 1 , 1990 , and dec 31 , 2016 . 
in 1998 , stead and colleagues compared second appointments with fixed date and time versus open second invitations for non - attenders of breast cancer screening in a randomised controlled trial in one breast screening centre in england , finding an increased participation rate with second timed appointments . 
 although the quality of the trial was good , its findings might not apply to current practice and target populations for screening since these have changed in terms of age and might have changed in terms of social support and employment status . 
in 2016 , hudson and colleagues reported the results of an observational study in north london comparing timed and non - timed second appointments , showing increased participation with timed appointments . 
we identified no trials of second timed appointments for non - attenders from outside the uk breast screening programme . added value of this study our randomised controlled trial assessed the effects of sending invitations for breast cancer screening with a second timed appointment to women who did not attend their first offered appointment . 
we could therefore analyse the efficacy of the intervention depending on a womans location and level of socioeconomic deprivation since the sites in the study covered a wide range of socioeconomic status levels . implications of all the available evidence our findings show the positive effects of second timed appointments on attendance for breast cancer screenings . 
 the results are of policy interest for early detection of breast cancer , because a simple change in the procedure of addressing non - attenders of breast cancer screening invitations could result in more women being screened . them a second invitation letter , which can vary : some centres supply open invitations , asking women to telephone to make an alternative appointment ; whereas others routinely offer second timed appointments , with date , time , and place stipulated . 
the department of health has advised nhs england that the approach with second timed appointments should be used.5 second timed appointments are nhsbsp policy , although this approach is not universally followed . although some women might not attend their screening appointment because they have made an informed choice not to do so , some of them will not attend for other reasons . 
these women might find a second timed appointment more beneficial than an open invitation because it does not require any effort to book a new appointment with the screening centre . 
 previous findings suggest that participation is greater when a second non - attenders , 6 , 7 but further investigations are needed to identify the women who would be most and least likely to respond to the second invitation . 
for example , someone who has not attended their last three screening appointments might not attend whatever the form of the second invitation . timed appointment is given in a randomised trial published in 1998 , stead and colleagues6 found that the effect of second timed appointments declined with increasing time since last screen , and in a more recent observational study , hudson and colleagues7 noted the same association , at least in absolute terms , in north london . 
therefore , we did a randomised trial of second timed appointments versus open invitations for non - attenders within the nhsbsp , powered to obtain significant results within subgroups of time since last screen . methods study design and participants this open , two - arm , randomised controlled trial was done in six screening sites in england ( derby , hull , plymouth , sheffield , southeast london , and west london ) for different time lengths between june 2 , 2014 , and sept 30 , 2015 . 
the date a batch was set up ( ie , the list of women to be invited was compiled ) , was defined as the date the screening episode was opened for each woman in that list . 
 batches of women invited to routine breast cancer screening were randomly assigned ( 1 : 1 ) to be sent either a second appointment with a fixed date and time ( intervention ) or an open invitation ( control ) in the event of non - attendance at the first offered appointment . 
women who self - referred for screening , women on an early recall protocol , and women who were invited because of a high risk of breast cancer were not randomised . 
for these women , the first invitation date was used for reference and participation was based on the first attendance date ( if any ) ie , only one of the multiple records was kept . 
other exclusions that were judged to be necessary were women invited to screening outside the study period of the screening sites ; observations with previous screening appointment more recent than the first offered appointment or date of the screening episode being opened ; and observations with a date on the invitation letter for a previous round of screening more recent than the date on the current invitation letter . 
we also excluded women who participated but had missing dates of attendance , because in those cases it was not possible to determine whether they had attended within 90 days of their first offered appointment or within 180 days of their episode being opened ( or neither )  . women were not informed of the study or asked to give consent for three reasons . 
the study was approved by the london bloomsbury research ethics committee . randomisation and masking within each screening centre , every invited woman was allocated a unique number , known as the sx number . 
at the beginning of the study , a coin toss by the chief investigator ( swd ) decided that women with an odd sx number would be allocated to the intervention group ( second timed appointment ) , whereas women with an even sx number would be allocated to the control group ( open second invitation )  . 
women who received their group assignment ( eg , women randomly assigned to the control group who received a second timed appointment letter by administrative error ) were marked with an error code but were still included in analysis . intervention the wrong for procedures women who did not attend their first offered appointment were flagged as such by staff at that clinic on the national breast screening system ( nbss )  . 
differences between the two letters were kept to a minimum so that women receiving second timed appointment letters did not feel pressurised into attending their screening appointment if they had made the decision not to participate . 
second timed appointments had to be allocated to non - attenders within 90 days of the missed appointment . because many practices already used second timed appointments for non - attenders of breast cancer screening , this study merely represented a minor variation in routine practice . 
data were pseudonymised , removing identifying data items such as month and day of birth and postcode , before being sent to the centre for cancer prevention ( wolfson institute of preventive medicine , queen mary university of london ) , where analyses were done . outcomes the primary endpoint was participation ( ie , attendance ) within 90 days of the first offered appointment . 
the key secondary endpoint was participation within 180 days of the screening episode being opened , used formally in the programme as a measure for calculating participation rates ( usually referred to as uptake in reports )  . 
other secondary endpoints were subgroup analyses by prevalent ( first ) or incident ( subsequent ) screen status , by time since last attended screen , and by index of multiple deprivation and age . 
 statistical analysis on the assumption that 40% of women who received their first invitation letter would not attend their screening appointment , we required 90% power for a difference of 20% ( intervention group ) versus 15% ( control group ) of those re - invited participating within 90 days . 
we also assumed that 20% of invitees would be non - attenders at their last routine screening ; that 15% would not have attended for three screening episodes or more ; and that 10% would not have attended for four episodes or more . 
 these proportions were approximations derived from offman and colleagues study8 and from the 10% neverattenders observed in the west midlands screening histories project.9 we required 80% power in all the subgroups for a difference of 14% ( intervention ) versus 10% ( control ) in non - attenders at their last routine screening , of 10% versus 7% in those who had not attended for three screening episodes or more , and of 2% versus 1% in those who had not attended for four screening episodes or more . 
these proportions corresponded to requirements 974 vol 18 july 2017 articles of 1252 , 1085 , 1422 , and 2515 individuals per group in each of the four categories , respectively . 
thus , we required at least 10 060 non - attenders per group in total ( corresponding to approximately 50 300 women invited to first screening appointment in the two groups )  . 
we asked participating centres to recruit substantially more women than this number as a failsafe measure . the difference in participation between the two groups was compared with poisson regression for the primary and key secondary endpoints , offset by the total numbers of invitees . 
we also did prespecified subgroup analyses by prevalent or incident screen status , by time since last attended screen , and by the 2010 index of multiple deprivation ( imd , based on a womans postcode ) .10 national quintiles of imd were used . 
primary analysis and subgroup analyses were by intention to treat , so that women who received the wrong type of letter for their trial group were retained in the analysis as if they had received the correct letter . 
other women who were potentially excludable but were kept in the intention - to - treat analysis were those who were being screened at the time of extraction of the dataset , who were permanently or temporarily under care , who died , who moved away , who were not known at their recorded address , who attended for screening but for some reason were not screened , who had been recently screened , or whose reason for attendance or nonattendance was missing or coded as other . 
these potentially excludable women were more likely to be identified in the intervention group than in the control group , since the offer of a timed appointment was more likely to prompt the invitee to inform the service that she had moved away or had already been recently screened . 
this trial is registered with barts health , number 009304qm . role of the funding source the department of health policy research programme was given the opportunity to comment on this report before submission for publication . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results the dataset received from the six screening centres had 33 146 records of women invited for screening at different times between june 2 , 2014 , and sept 30 , 2015 , who did not attend their first appointment ( see appendix p 3 for details of recruitment by centre )  . 
women were followed up for more than 180 days after their episode in the current round of screening was opened , and the trial was ended when we estimated that the number of women recruited was larger than the one required by our power calculations . 
7092 ( 21% ) of the 33 146 records were excluded after randomisation because of the reasons stated in the methodseg , ineligible age or date of invitation , missing attendance record , or multiple records for the same woman ( 3520 in the intervention group vs 3572 in the control group ; figure )  . 
 of the remaining 26 054 women , 12 807 ( 49% ) had been randomly assigned to receive the intervention of a second timed appointment letter , and 13 247 ( 51% ) to receive an open invitation letter . 
most women in both groups were younger than 60 years of age and came from more deprived socioeconomic areas ( imd quintiles 1 and 2 ; table 1 )  . 586 ( 5% ) of 12 807 women in the intervention group and 52 ( < 1% ) of 13 247 women in the control group received the incorrect invitation letter for their group but were still included in the intention - to - treat analysis as if they had received the correct letter . 
455 ( 4% ) women in the intervention group and 119 ( < 1% ) women in the control group were judged to be potentially excludable , because of the nature of the intervention ( as noted in the methods section )  . 
the majority of these women were either recently screened and so invited in error ( 121 [ 21% ] for non - attendance of 574 ) , had missing reason 33 146 records of non - attenders receiving second invitation letters 16 327 records of women with odd sx numbers randomly assigned to timed appointment ( intervention ) 16 819 records of women with even sx numbers randomly assigned to an open invitation letter ( control ) 2482 outside screening range 2551 outside screening range 110 duplicates for the same 146 duplicates for the same ( 5070 years ) woman 3520 records excluded * attendance dates 147 duplicates for the same woman in the same batch 867 outside study period 34 with incongruences in ( 5070 years ) woman 3572 records excluded * attendance dates 54 duplicates for the same woman in the same batch 958 outside study period 8 with incongruences in 44 with missing date of 24 with missing date of 12 807 women analysed 13 247 women analysed figure : trial profile sx = a sequential unique identifier of each woman within the nhs breast screening programme . 
 * 2010 index of multiple deprivation ( imd ) from most deprived to most affluent . table 1 : characteristics of study groups intervention group ( n = 12 807 ) control group ( n = 13 247 ) absolute difference in attendance rr ( 95% ci ) p value 2861 ( 22% ) 1632 ( 12% ) 181 ( 170193 ) < 00001 3054 ( 24% ) 1784 ( 13% ) 177 ( 167188 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened data are number who participated ( % ) unless otherwise stated . 
percentages have been rounded up . table 2 : participation at second invitation for all women in the trial ( 162 [ 28% ] ) , or were not known to be or no longer living at the address held ( 194 [ 34% ] )  . 
these women were also retained in our intention - to - treat analyses . the in total , 4493 ( 17% ) of 26 054 women participated in breast cancer screening within 90 days of the date of their first offered appointment . 
a significantly higher intervention group proportion of women participated within 90 days than did women in the control group ( 2861 [ 22% ] of 12 807 vs 1632 [ 12% ] of 13 247 ; rr 181 [ 95% ci 170193 ] , p < 00001 ; table 2 )  . 
a higher proportion of women in the intervention group than in the control group also met the secondary endpoint of participation within 180 days of the screening episode being opened ( rr 177 [ 95% ci 167188 ] , p < 00001 )  . 
 similar results were obtained in a post - hoc per - protocol analysis and an analysis excluding the women deemed potentially excludable ( data not shown )  . overall , 12 817 ( 49% ) of 26 054 women were offered a prevalent screen ( 6300 in the intervention group vs 6517 in the control group ) and 13 237 ( 51% ) women were offered an incident screen ( 6507 in the intervention group vs 6730 in the control group )  . 
to take into account the fact that the prevalent screen includes women who have been invited before but have never attended , we first analysed younger women in the prevalent round ( ie , those aged 5052 years )  . 
in this subgroup , participation within 90 days of the first offered appointment was significantly greater for women in the intervention group than in the control group ( table 3 ) ; participation within 180 days of the episode being opened supported this result . 
although numbers were small , participation at second invitation was still significantly higher in the intervention group than in the control group ( table 3 )  . participation data for incident screen women aged 5370 years who had attended any time previously are shown in table 4 by time since last attended screen before the date of the first offered appointment for this screening episode . 
age intervals were adjusted accordingly ( eg , only women aged 5670 years were included in the group who last attended their screening 69 years before their first offered appointment )  . 
despite numbers of women participating diminishing with increasing time since last attendance , all results were significantly in favour of the intervention , even for women who had attended previously but 9 years or more before their first offered appointment ( table 4 )  . 
for women who had last attended 13 years previously , the expected proportion of women participating in screening within 180 days in the intervention group if there had been no effect of the intervention is 32% ( attendance in the control group ) of 2853 ( number invited in the intervention group , n = 912 )  . 
 therefore , the effect of 2853 second timed appointments was generating 495 ( ie , 1407 [ the number of attendees in the intervention group ] 912 [ the number expected of attendees ] ) attended screens . 
 the timed appointments required per additional participant are six , 15 , and 26 for women whose last attendance was 36 years , 69 years , and 9 or more years before their current first offered appointment , respectively , calculated as for those attending 13 years previously . corresponding numbers of second formal tests for heterogeneity of the effect of the intervention by prevalent or incident status were significant ( p < 00001 for participation within 90 days of the first offered appointment and within 180 days of the episode being opened )  . 
although the relative effects are larger in the prevalent screen women , the absolute differences in participation are larger in the incident screen women ( tables 3 and 4 )  . 976 vol 18 july 2017 articles intervention group control group rr ( 95% ci ) p value absolute difference in attendance 5052 years number invited participation in screening 5370 years number invited participation in screening 2017 2072 4283 4445 within 90 days of first offered appointment within 180 days of episode opened 347 ( 17% ) 369 ( 18% ) 147 ( 7% ) 163 ( 8% ) 242 ( 199295 ) 233 ( 193280 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 283 ( 7% ) 307 ( 7% ) 82 ( 2% ) 97 ( 2% ) 358 ( 280458 ) 328 ( 261413 ) < 00001 < 00001 data are number who participated ( % ) unless otherwise stated . 
percentages for the difference in attendance have been rounded up . table 3 : participation at second invitation for prevalent screen women , by age group intervention group attendance control group absolute difference in rr ( 95% ci ) p value attended any time previously number invited participation in screening 6507 6730 aged 5170 years who attended 1 to < 3 years previously number invited participation in screening 2853 2992 aged 5370 years who attended 3 to < 6 years previously number invited participation in screening 1633 1638 aged 5670 years who attended 6 to < 9 years previously number invited participation in screening aged 5970 years who attended 9 years previously number invited participation in screening within 90 days of first offered appointment 2231 ( 34% ) 1403 ( 21% ) within 180 days of episode opened 2378 ( 37% ) 1524 ( 23% ) 164 ( 153178 ) < 00001 161 ( 151173 ) < 00001 within 90 days of first offered appointment 1307 ( 46% ) 876 ( 29% ) within 180 days of episode opened 1407 ( 49% ) 956 ( 32% ) 156 ( 143171 ) < 00001 154 ( 142168 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened 568 ( 35% ) 590 ( 36% ) 306 ( 19% ) 327 ( 20% ) 186 ( 162214 ) < 00001 181 ( 158208 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened 71 ( 13% ) 76 ( 14% ) 39 ( 7% ) 45 ( 8% ) 200 ( 135297 ) < 00001 186 ( 128269 ) < 00001 within 90 days of first offered appointment within 180 days of episode opened 35 ( 7% ) 37 ( 8% ) 16 ( 4% ) 18 ( 4% ) 210 ( 116381 ) 198 ( 112348 ) 001 002 data are number who participated ( % ) unless otherwise stated . 
percentages for the difference in attendance have been rounded up . table 4 : participation at second invitation for incident screen women , overall and by time since last attendance results did not vary substantially by age group ( data not shown )  . 
the first two quintiles ( 1 and 2 ) , corresponding to the most deprived populations , have higher rrs than the other quintiles for participation within 90 days of the first offered appointment and participation within 180 days of the episode being opened . 
results were highly significant in all quintiles ( p < 00001 in all cases )  . vol 18 july 2017 articles intervention group control group rr ( 95% ci ) p value absolute difference in attendance imd quintile 1 ( most deprived ) number invited participation in screening 3395 3623 within 90 days of first offered appointment within 180 days of episode opened 639 ( 19% ) 682 ( 20% ) 353 ( 10% ) 386 ( 11% ) 193 ( 169220 ) 189 ( 166214 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 768 ( 21% ) 825 ( 23% ) 398 ( 11% ) 434 ( 12% ) 196 ( 173222 ) 193 ( 171217 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 686 ( 24% ) 734 ( 26% ) 402 ( 13% ) 442 ( 15% ) 177 ( 156201 ) 173 ( 153195 ) < 00001 < 00001 imd quintile 2 number invited participation in screening imd quintile 3 number invited participation in screening imd quintile 4 number invited participation in screening within 90 days of first offered appointment within 180 days of episode opened imd quintile 5 ( least deprived ) number invited participation in screening 3645 3703 2864 2978 1946 2028 488 ( 25% ) 519 ( 27% ) 297 ( 15% ) 324 ( 16% ) 171 ( 148198 ) 167 ( 145192 ) < 00001 < 00001 within 90 days of first offered appointment within 180 days of episode opened 277 ( 29% ) 290 ( 31% ) 178 ( 20% ) 194 ( 22% ) 148 ( 122179 ) 142 ( 118171 ) < 00001 < 00001 data are number who participated ( % ) unless otherwise stated . 
percentages fhave been rounded up . table 5 : participation at second invitation for all national imd quintiles ( from most to least deprived ) in our post - hoc exploratory analyses , the intervention significantly increased participation at all study sites ( p < 00001 in all centres ; appendix p 2 ) compared with that in the control group . 
the effect of the intervention was highest in southeast london ( rr for participation within 90 days of the first offered appointment 227 [ 95% ci 190272 ] ) , which had the highest proportion of women in the two most deprived imd quintiles ( 3249 [ 87% ] of 3738 ) , and only 53 ( 1% ) women in the two most affluent quintiles . 
by contrast , the effect of the intervention was smallest in plymouth ( rr 155 [ 95% ci 136177 ] ) , where 3595 ( 50% ) of 7190 women were in the two most deprived imd quintiles and 1706 ( 24% ) were in the two most affluent quintiles . discussion in this study , the intervention of inviting non - attenders of breast cancer screening to a second appointment with a fixed date and time caused an absolute increase in participation of 103% compared with an open invitation , which would translate to an increase in participation of 3% , since around 30% of invitees to a first appointment were non - attenders.1 most women included in our analysis were younger than 60 years of age and came from more deprived socioeconomic areas . a limitation of this study was that more than 20% of women were excluded after randomisation . 
we have been unable to identify a systematic factor or staff action that could have caused this imbalance , although centres with more error codes for the sending of the wrong letter were also those with the larger imbalances between the 978 vol 18 july 2017 articles sizes of the two groups . 
although nearly twice as many women in the intervention group than the control group participated in screening at second intention - to - treat analysis led to more diluted results than less statistically cautious approaches , the improvement in participation in the intervention group was still substantial , as shown by our primary analysis . 
the greater effect at prevalent screen than incident screen is important , since a stronger decline in participation over time has been reported at first invitation than at subsequent invitations.1 the universal adoption of second timed appointments for non - attenders at first invitation could go some way to rectifying this trend . the practice of second evidence at the ecological and individual level from europe and north america suggests that socioeconomic deprivation , often in conjunction with specific ethnicity , is strongly associated with non - participation in breast cancer screening.1116 transport issues and difficulties in getting to the screening appointment are cited as reasons for non - participation.12 , 14 further detailed surveys of nonparticipants are needed to improve our understanding of the barriers to participation . 
thus , timed appointments for non - attenders could address in part the the breast socioeconomic gradient screening service.2 , 3 at the very least , this practice should not exacerbate the proble this gradient needs to be addressed because the clinical stage of presentation tends to be later for women of lower socioeconomic status than for women of higher status , and is a factor that contributes to worse treatment outcomes.11 arguably , a key factor responsible for women not attending their breast screening invitation might be car ownership , which is strongly correlated with socioeconomic status and positively associated with breast screening coverage.12 a comparison of car ownership within the same imd quintile between women who responded to their second timed appointment letter and women who did not could be interesting . in delivery of the greatest effect of the intervention was seen in southeast london , which had the highest proportion of women in the two lowest imd quintiles . 
in view of our findings , and the internationally observed socioeconomic gradient in participation in breast cancer screening , 1416 our results could have relevance to other countries with organised screening programmes . in all time - interval categories into which women were divided , the proportions of women who participated in screening increased in the intervention group versus the control by around the same relative factor for second timed appointments and there did not seem to be a trend between time since last screen and efficacy of the intervention , by contrast with findings reported by stead and colleagues.6 however , the absolute effect declined with time since last attended screen , as has been reported previously , and reflecting generally similar or larger relative effects but smaller absolute effects in those with a lower baseline participation . 
the number of second timed appointment letters that need to be offered per additional participant increases for women whose last attendance at breast cancer screening was more than 6 years before their current first offered appointment . 
of course , fewer second timed appointment letters have to be issued than open letters per participant ; however , reservation of the appointment time is the call on resources . the economic implications of compulsorily extending the intervention to all women in the breast cancer screening programme will have to be examined before such a change in policy is made , because allocating time slots for fixed timed appointments has a cost in terms of resources . 
in most cases , overbooking for screening appointments is advised to minimise the waste from unused slots ; our results suggest that increasing the overbooking ratio for second timed appointments for previous non - attenders would be safe . 
however , with the higher variability of the likelihood of participation in the second timed appointments , it would be prudent to mix small numbers of these within sessions with a majority of first offered appointments . 
 offering second timed appointments only to those who have attended in the 6 years previous to their first offered appointment might be a cost - effective approach , since it leads to fewer wasted appointments than in those who have not attended for a longer period . 
this strategy , however , raises questions of ethics and equity and should be considered further by the department of health and public health england to determine the appropriate policy for the programme . 
scope also exists for qualitative research into the public acceptability of the policy of second timed appointments . in other countries , such as italy , 17 , 18 fixed appointments rather than open invitations have been associated with improved participation in screening in general , not only for non - attenders . 
other methods that can successfully increase participation in breast cancer screening are text message , 19 , 20 postal , 21 and telephone reminders ; 22 general practitioner endorsement ; 23 , 24 and the possibility to change appointments to out - of - office hours.8 second for non - attenders could be timed appointments implemented with these methods ( eg , with the second vol 18 july 2017 articles timed appointment letter offering the opportunity to change to an out - of - hours time slot , or having primary care endorsement ) and other interventions to improve delivery to all eligible women , with the ultimate goal of improving early detection of breast cancer in england and worldwide . contributors pca contributed to study design , data analysis , data interpretation , and drafting the report . 
he was responsible jointly with jp for study concept and design , supervised the statistical analysis and data interpretation , and contributed to drafting the report . declaration of interests we declare no competing interests . acknowledgments we thank all the staff who worked at the screening centres that took part to this project . 
swd and rm contributed to this study as part of the programme of the policy research unit in cancer awareness , screening and early diagnosis , which receives funding for a research programme from the department of health policy research programme . 
this programme is a collaboration between researchers from seven institutions ( queen mary university of london , university college london , kings college london , london school of hygiene & tropical medicine , hull york medical school , durham university , and peninsula medical school )  . articles the uk standardisation of breast radiotherapy ( start ) trials of radiotherapy hypofractionation for treatment of early breast cancer : 10 - year follow - up results of two randomised controlled trials joanne s haviland , j roger owen , john a dewar , rajiv k agrawal , jane barrett , peter j barrett - lee , h jane dobbs , penelope hopwood , pat a lawton , brian j magee , judith mills , sandra simmons , mark a sydenham , karen venables , judith m bliss * , john r yarnold * , on behalf of the start trialists group summary background 5 - year results of the uk standardisation of breast radiotherapy ( start ) trials suggested that lower total doses of radiotherapy delivered in fewer , larger doses ( fractions ) are at least as safe and e ective as the historical standard regimen ( 50 gy in 25 fractions ) for women after primary surgery for early breast cancer . 
in this prespeci ed analysis , we report the 10 - year follow - up of the start trials testing 13 fraction and 15 fraction regimens . methods from 1999 to 2002 , women with completely excised invasive breast cancer ( pt13a , pn01 , m0 ) were enrolled from 35 uk radiotherapy centres . 
in start - a , a regimen of 50 gy in 25 fractions over 5 weeks was compared with 416 gy or 39 gy in 13 fractions over 5 weeks . 
in start - a , moderate or marked breast induration , telangiectasia , and breast oedema were signi cantly less common normal tissue e ects in the 39 gy group than in the 50 gy group . 
the proportion of patients with local - regional relapse at 10 years did not di er signi cantly between the 40 gy group ( 43% , 95% ci 3259 ) and the 50 gy group ( 55% , 95% ci 4272 ; hr 077 , 95% ci 051116 ; p = 021 )  . 
in start - b , breast shrinkage , telangiectasia , and breast oedema were signi cantly less common normal tissue e ects in the 40 gy group than in the 50 gy group . 
the results support the continued use of 40 gy in 15 fractions , which has already been adopted by most uk centres as the standard of care for women requiring adjuvant radiotherapy for invasive early breast cancer . funding cancer research uk , uk medical research council , uk department of health . introduction the local cancer control and overall survival bene ts of adjuvant radiotherapy for women with early breast cancer have been established by a systematic review of 17 randomised trials involving more than 10 000 patients.1 in most studies , a total dose of 50 gy was delivered in 25 fractions of 2 gy over 5 weeks . 
5 - year results for local tumour control and late - occurring normal tissue e ects assessed by patients and from photographs were consistent with the hypothesis that breast cancer tissue and the doselimiting normal tissues are similarly sensitive to fraction size.8 , 9 start - b had a pragmatic design , with 5 - year results suggesting that local tumour control and safety of normal tissue e ects are as good after 40 gy in 15 fractions over 3 weeks ( used in the uk and canada for decades ) as with 50 gy in 25 fractions over 5 weeks.9 , 10 the 5 - year results of the start trials had a large e ect on breast cancer radiotherapy practice both in the uk and worldwide . 
start results have subsequently informed national institute for health and care excellence ( nice ) and american society for radiation oncology ( astro ) guidelines for breast radiotherapy fractionation.11 , 12 a 2010 cochrane review concluded that hypofractionation did not seem to compromise safety and e cacy , but that longer follow - up was needed for a more complete assessment.13 we here present a 10 - year update of start - a and start - b , including assessment of long - term e cacy and adverse e ects . interval was required before methods study design and participants the start trials were two randomised , unmasked trials of women recruited between 1999 and 2002 , from uk radiotherapy centres17 centres for start - a and 23 for start - b . 
patients in start - a were randomly assigned to either 50 gy in 25 fractions ( control group ) or 416 gy in 13 fractions or 39 gy in 13 fractions over 5 weeks , and start - b patients to either 50 gy in 25 fractions ( control group ) over 5 weeks or 40 gy in 15 fractions over 3 weeks . 
 randomisation method was computer - generated , and strati ed by centre , type of primary surgery ( breastconservation surgery or mastectomy ) , and tumour bed boost trials permitted prescription of a sequential tumour bed boost dose of 10 gy in ve fractions , which needed to be planned before randomisation to ensure that the independent e ect of tumour bed boost radiotherapy on adverse e ects did not a ect the comparisons of fractionation schedules . 
both start and details of the radiotherapy planning , delivery , and veri cation protocols have been previously reported.810 the start trials were approved by the south thames multi - research ethics committee in september , 1998 , and by the local ethics committees of all participating centres . 
 written informed consent was obtained for all patients . the principal endpoints were local - regional relapse de ned as relapse in breast or chest wall , ipsilateral axilla , or supraclavicular fossa within an irradiated target volumeand late normal tissue e ects . 
physician assessments of normal tissue e ects in the treated breast compared with the contralateral breast were scored on a four - point scale ( none , a little , quite a bit , or very much )  . 
 table 1 : relapse and mortality according to fractionation schedule in start - a vol 14 october 2013 1087 statistical analysis we predicted a 5 - year local - regional tumour relapse rate of 10% in the 50 gy schedule group ( control ) , on the basis of the start pilot trial.7 start - a had a target sample size of 2000 patients to provide 80% power to detect a di erence of 5% in the local - regional relapse rate between the control and each test schedule ( two - sided = 005 )  . 
start - b had a target of 1840 patients to provide 95% power to exclude an increase of 5% in the localregional relapse rate in the 40 gy schedule compared with control ( one - sided = 0025 )  . we used survival analysis methods to compare endpoint occurrences between fractionation schedules . 
 both one - sided and two - sided 95% cis were calculated for the absolute di erence in local - regional relapse rates because the upper limit is of greater clinical interest , in view of concern about a possible excess risk caused by hypofractionated schedules . 
we plotted kaplan - meier survival curves and cumulative hazard rates according to fractionation schedule , censoring at the median length of follow - up . we obtained direct estimates of the / value for breast cancer and the dose - limiting normal tissues from cox proportional hazards regression models containing terms for total dose , and total dose multiplied by dose per fraction as well as known prognostic factors ( appendix )  . 
 the / value is derived from an empirical model that describes sensitivity of a normal or malignant tissue to fraction size ; / values less than 10 gy indicate relative sensitivity to fraction size . 
we carried out meta - analyses of start - a , start - b , and the start pilot trial by tting the cox proportional hazards regression models to all individual patient data from the three trials . 
analyses were done with spss ( version 19 ) and stata ( version 9 )  . the trial is registered as an international standard randomised controlled trial , number isrctn59368779 . role of the funding source the funders of the study provided peer - reviewed approval for the trials and had no role other than as representatives ( as observers ) on the trial steering committee . 
the corresponding author had full access to all the data , and had nal responsibility for the decision to submit for publication . results 2236 women were recruited into start - a between jan 20 , 1999 , and dec 20 , 2002 ; median age was 57 years ( range 2585 ) ( appendix )  . 
1900 ( 85% ) had received breast - conserving surgery , 1138 ( 51% ) had tumours smaller than 2 cm , 643 ( 29% ) had positive lymph nodes , 1572 ( 70% ) had grade 1 or 2 disease , 793 ( 35% ) received adjuvant chemotherapy , 1758 ( 79% ) received tamoxifen , and 318 ( 14% ) received lymphatic radiotherapy . 
at a median follow - up in survivors of 93 years ( iqr 80100 , maximum 124 years ) , 1700 of 2236 patients ( 760% ) were alive and without relapse , 57 ( 25% ) were 40 gy vs 50 gy hr 077 , 95% ci 051116 ; p = 021 time from randomisation ( years ) 1077 1085 1047 1055 1002 1016 number at risk 50 gy 40 gy 1105 1110 figure 1 : cumulative risk of local - regional tumour relapse in start - a ( a ) and start - b ( b )  . 1088 vol 14 october 2013 articles 50 gy 416 gy 39 gy 50 gy 40 gy alive with local - regional relapse ( without distant relapse ) , 78 ( 35% ) were alive with distant relapse ( including 16 with local - regional relapse ) , 392 ( 175% ) had died ( including 66 with local - regional relapse ) , and nine ( 04% ) had had no follow - up . at the time of analysis ( feb 20 , 2012 ) , 139 of 2236 ( 62% ) patients in start - a had local - regional tumour relapse . 
the hrs for local - regional relapse relative to the 50 gy schedule were 091 ( 95% ci 059138 ) for the 416 gy schedule and 118 ( 079176 ) for the 39 gy schedule ( table 1 )  . 
the estimated absolute di erences in the proportion of patients with local - regional relapses at 10 years compared with 50 gy were 06% ( 95% ci 30 to 27 ) for 416 gy and 13% ( 15 to 52 ) for 39 gy . 
the upper limits of the one - sided 95% ci for the absolute di erence in 10 - year local - regional relapse rates indicated an estimated maximum 20% excess risk with 416 gy and 45% with 39 gy compared with 50 gy . 
the estimated / value for local - regional relapse in start - a was 4 gy ( 95% ci 0089 ) , adjusting for age , tumour size , type of primary surgery , use of adjuvant chemotherapy , use of tamoxifen , lymphatic radiotherapy , and tumour bed boost radiotherapy . 
15 ( 577% ) of the 26 deaths from cardiac disease in start - a were in women with left - sided primary tumours ( four of seven with 50 gy , ten of 13 with 416 gy , and one of six with 39 gy )  . 
distant relapses , disease - free survival , and overall survival were not signi cantly di erent between schedules start - a , with no evidence of a clinically signi cant detriment for either of the hypofractionated schedules compared with 50 gy ( table 1 , gure 2 )  . breast shrinkage and induration were the most common normal tissue e ects at 10 years in start - a ( table 2 )  . 
moderate or marked breast induration , telangiectasia , and breast oedema were signi cantly less common in the 39 gy regimen patients group than in the 50 gy regimen group ( table 2 , gure 3 )  . 
 / estimates for normal tissue endpoints in start - a ( adjusting for age , breast size , surgical de cit , lymphatic radiotherapy , and tumour bed boost radiotherapy ) were 35 gy ( 95% ci 0764 ) for breast shrinkage , 416 gy vs 50 gy hr 094 , 95% ci 075117 ; p = 057 39 gy vs 50 gy hr 108 , 95% ci 087135 ; p = 048 number at risk 50 gy 416 gy 39 gy 40 gy vs 50 gy hr 079 , 95% ci 065097 ; p = 0022 number at risk 50 gy 40 gy 1105 1110 time from randomisation ( years ) 1064 1080 1021 1040 figure 2 : kaplan - meier analysis of disease - free survival in start - a ( a ) and start - b ( b )  . 4 gy ( 2356 ) for breast induration , 38 gy ( 1857 ) for telangiectasia , and 47 gy ( 2470 ) for breast oedema . 
 ischaemic heart disease , symptomatic rib fracture , and symptomatic lung brosis were rare at 10 years ( table 3 ) and occurred in much the same proportions with each treatment schedule . 2215 women were recruited into start - b between jan 4 , 1999 , and oct 12 , 2001 . 
2038 of 2215 ( 92% ) patients had received breastconserving surgery , 1412 ( 64% ) had tumours smaller than 2 cm , 504 ( 23% ) had positive lymph nodes , 1667 ( 75% ) had grade 1 or 2 disease , 491 ( 22% ) received adjuvant chemotherapy , 1928 ( 87% ) received tamoxifen , and 161 ( 7% ) received lymphatic radiotherapy ( appendix )  . 
restricted to women who received lymphatic radiotherapy ( to axilla or supraclavicular fossa )  . table 2 : physician - assessed normal tissue e ects by fractionation schedule in start - a alive with local - regional relapse ( without distant relapse ) , 63 ( 28% ) were alive with distant relapse ( including ten with local - regional relapse ) , 351 ( 158% ) had died ( including 35 with local - regional relapse ) , and 19 ( 09% ) had no follow - up . at the time of the analysis , 95 of 2215 ( 43% ) patients in start - b had had local - regional tumour relapse , a lower proportion than in start - a , which is probably a result of the slightly better prognosis of patients recruited into start - b compared with start - a . 
the estimated absolute di erence in the proportion of patients with 10 - year local - regional relapse for 40 gy compared with 50 gy was 12% ( 95% ci 26% to 10% )  . 
the upper limit of the one - sided 95% ci for the absolute di erence in 10 - year local - regional relapse rates suggested an estimated 04% excess risk associated with the 15 fraction schedule . 
the kaplanmeier and cumulative hazard rate plots for local - regional relapse according to fractionation schedule ( gure 1 , appendix ) show the low number of recurrences in both randomised groups in start - b . 236 of 351 ( 672% ) deaths in start - b were from breast cancer ( 130 with 50 gy and 106 with 40 gy ) , 17 ( 48% ) were related to cardiac disease only ( 12 with 50 gy and ve with 40 gy ) , 48 ( 137% ) were from other cancers ( 25 with 50 gy and 23 with 40 gy ) , 40 ( 114% ) were from other noncancer causes ( 21 with 50 gy and 19 with 40 gy ) , and ten ( 28% ) were from unknown cause ( four with 50 gy and six with 40 gy )  . 
11 ( 647% ) of the 17 deaths from cardiac disease were in women with left - sided primary tumours ( eight of 12 with 50 gy and three of ve with 40 gy )  . 
 * reported cases include seven after trauma ( ve in start - a , two in start - b ) , and ten after metastases ( ve in starta and ve in start - b )  . 
 hazard ratio ( 95% ci ) table 3 : incidence of other late adverse e ects according to fractionation schedule 20 30 40 favours 40 gy favours 50 gy local - regional relapse figure 3 : late normal tissue e ects in start - a ( a ) and start - b ( b )  . 
moderate or marked breast shrinkage , telangiectasia , and breast oedema were signi cantly lower with 40 gy than with 50 gy ( gure 3 , table 5 )  . 
 ischaemic heart disease , symptomatic rib fracture , and symptomatic lung brosis were rare and occurred in much the same proportions with each treatment schedule ( table 3 )  . post - hoc subgroup analyses of the combined hypofractionated regimens versus the control groups for localregional relapse in start - a , start - b , and the pilot trial ( n = 5861 ) showed that the treatment e ect was not signi cantly di erent irrespective of age , type of primary surgery , axillary node status , tumour grade , adjuvant chemotherapy use , or use of tumour bed boost radiotherapy ( gure 4 )  . 
in a post - hoc analysis , the incidence of any moderate or marked physician - assessed normal tissue e ects in the breast ( shrinkage , induration , oedema , or telangiectasia ) for the 4660 women with data available from start - a , start - b , and the pilot trial showed that the treatment e ect was similar irrespective of age , breast size , use of tumour bed boost radiotherapy , adjuvant chemotherapy , or tamoxifen ( gure 5 )  . local relapse 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy events ( n / patients ; % ) estimated proportion of patients with event by 5 years ( % ; 95% ci ) estimated proportion of patients with event by 10 years ( % ; 95% ci ) crude hazard ratio ( 95% ci ) value * 50 / 1105 ( 45% ) 33% ( 2446 ) 52% ( 3969 ) 100 36 / 1110 ( 32% ) 19% ( 1230 ) 38% ( 2752 ) 070 ( 046107 ) 010 53 / 1105 ( 48% ) 35% ( 2548 ) 55% ( 4272 ) 100 42 / 1110 ( 38% ) 23% ( 1534 ) 43% ( 3259 ) 077 ( 051116 ) 021 158 / 1105 ( 143% ) 105% ( 88125 ) 160% ( 138185 ) 100 121 / 1110 ( 109% ) 75% ( 6092 ) 123% ( 103146 ) 074 ( 059094 ) 0014 any breast cancer - related event all - cause mortality 222 / 1105 ( 201% ) 143% ( 123165 ) 222% ( 197250 ) 100 182 / 1110 ( 164% ) 104% ( 87124 ) 183% ( 160209 ) 079 ( 065097 ) 0022 192 / 1105 ( 174% ) 109% ( 91129 ) 192% ( 168219 ) 100 159 / 1110 ( 143% ) 79% ( 6496 ) 159% ( 137184 ) 080 ( 065099 ) 0042 * assessed with log - rank test compared with 50 gy . 
 table 4 : relapse and mortality according to fractionation schedule in start - b time , the relative di erences between discussion although the absolute numbers of events have increased over the hypofractionated and control schedules at 10 years remain similar to those at 5 years , con rming that appropriately dosed hypofractionated radiotherapy for women with early breast cancer is safe and e ective.810 in start - a , 416 gy in 13 fractions over 5 weeks remains a safe and e ective alternative to 50 gy in 25 fractions the two regimens have much the same anti - tumour and adverse e ects . 
 restricted to women who received lymphatic radiotherapy ( to axilla or supraclavicular fossa )  . table 5 : physician - assessed normal tissue e ects by fractionation schedule in start - b number of events / patients age ( years ) 4049 5059 primary surgery axillary nodes ( pn ) negative positive tumour grade breast conservation surgery 409 / 5348 mastectomy 35 / 513 60 / 343 116 / 1046 154 / 2226 114 / 2246 289 / 4318 149 / 1421 41 / 1213 108 / 2398 114 / 1272 199 / 2749 241 / 3071 303 / 4346 139 / 1480 tumour bed boost radiotherapy adjuvant chemotherapy 1092 12 14 16 18 20 favours fraction sizes > 20 gy favours fraction size 20 gy figure 4 : meta - analysis of local - regional relapse comparing hypofractionated regimens versus 50 gy in 25 fractions includes 5861 patients from the start pilot trial , start - a , and start - b . average treatment groups enabled an unconfounded test of sensitivity to fraction size . 
the cis around the / estimate for breast cancer become narrower as more data are collected , and the low value is supported by the evidence from the combined hypofractionation trials.14 an underlying estimate describes the distribution of / that can be narrow or broad : its characterisation is a challenge for correlative research . 
 the 10 - year results of start - b con rm that 40 gy in 15 fractions over 3 weeks is at least as safe and e ective as 50 gy in 25 fractions over 5 weeks . 
application of an / value of 35 gy for breast shrinkageas obtained from start - aand assuming no e ect of treatment time on late normal tissue e ects , 40 gy in 15 fractions corresponds to 45 gy in 2 gy equivalents . 
the 15 fraction regimen is less harmful to normal tissues , and there is no suggestion that it is less e ective in treating the cancer . the data from the start trials are consistent with the 10 - year results of the ontario trial , which reported that local tumour control and breast cosmesis were no worse with a regimen of 425 gy in 16 fractions over 32 weeks compared with 50 gy in 25 fractions over 5 weeks.5 the start pilot trial , ontario trial , and start - a and start - b trials , considered together , present robust evidence that hypofractionation is a safe and e ective approach to breast cancer radiotherapy ( panel ) .15 the corollary is that the continued use of small ( 2 gy ) fractions spares the cancer as much as the normal tissues , thereby bringing no bene t to patients . 
the proportion of patients who had distant metastases di ered after the rst few years of follow - up , which translated into an overall survival bene t ( table 4 )  . 
this e ect did not occur in start - a and it occurs too early to be a result of better local control , in which case the survival bene t would not be apparent until after 15 years . 
similarly , it is unlikely to be caused by baseline di erences in patient and treatment characteristics , which were well balanced between schedules , and unknown factors are unlikely to be imbalanced in randomised trials of this size . 
following publication of the start trials 5 - year results , most uk centres pragmatically adopted the 15 fraction schedule as standard of care , as recommended by nice guidelines in 2009.11 the 15 fraction schedule was already in widespread use in the uk and elsewhere before the start trials , but had not been formally tested in a randomised controlled setting . controversy remains about generalising trial ndings to all patients satisfying the eligibility criteria of the start trials.12 to address this concern , we did unplanned subgroup meta - analyses of the start - a and start - b trial comparing all trials and the start pilot vol 14 october 2013 hazard ratio ( 95% ci ) 079 ( 047134 ) 088 ( 060128 ) 103 ( 074144 ) 111 ( 075163 ) 097 ( 080119 ) 091 ( 046181 ) 110 ( 086140 ) 080 ( 057111 ) 096 ( 051182 ) 107 ( 072159 ) 086 ( 059125 ) 099 ( 074132 ) 099 ( 076129 ) 109 ( 086138 ) 081 ( 057114 ) articles hazard ratio ( 95% ci ) 085 ( 056128 ) 109 ( 086137 ) 078 ( 068091 ) 080 ( 069092 ) 096 ( 065142 ) 077 ( 068087 ) 091 ( 072115 ) 080 ( 069092 ) 086 ( 076096 ) 083 ( 075091 ) 088 ( 071108 ) 083 ( 068102 ) 084 ( 076093 ) hypofractionated schedules combined versus the control schedules . 
although direct comparisons of results across the di erent trials are inadvisable because of the di erent patient populations , our subgroup analyses lend no support to a conservative approach with respect to patient age , breast size , tumour grade , axillary node status , type of surgery , cytotoxic chemotherapy , tumour bed boost radiotherapy , and lymphatic radiotherapy , although numbers are small in some groups . 
along with other investigators , 16 we have found no suggestion of a detrimental e ect of hypofractionated radiotherapy on risk of local relapse in grade 3 tumours , which does not support a subgroup analysis of the ontario trial.5 whether or not a tumour bed boost radiotherapy was given did not alter the e ect of hypofractionation on risk of late normal tissue e ects , and tumour bed boost radiotherapy could not have a confounding e ect because it was prescribed before randomisation and was given to similar proportions of patients in each treatment schedule group . 
one exclusion criterion from the start trials was immediate breast reconstruction , and a conservative approach might be to defer from using a 15 fraction regimen in such patients , despite the very high likelihood , in our opinion , that the 15 fraction schedule would reduce normal tissue e ects and provide equivalent local - regional control . 
finally , concerns have been raised about doses to the heart with hypofractionated schedules.12 our results showed that although follow - up was still short for cardiac events , there was no major di erence between the schedules for the number of cases of heart disease in women with left - sided primary tumours . 
some research suggests that hypofractionated breast radiotherapy might be safer for the heart than are conventional regimens.18 although such ndings are reassuring , the heart is sensitive to radiation whatever fractionation is used , with no lower dose threshold for adverse e ects.19 thus , the heart should be protected irrespective of the dose fractionation regimen used . other ongoing or planned trials of hypofractionation for whole breast radiotherapy aim to validate the ndings from the start trials in di erent popu lations . 
 * assessed from baseline photographs . panel : research in context systematic review the start trials began with the pilot study in 1986 , at which time there was no evidence available from randomised trials comparing alternative fractionation schedules for breast cancer radiotherapy . 
alternative shorter fractionation schedules were in use at some uk centres and in canada , but the only evidence available for these schedules was from case series and cohort studies . 
5 - year results of the start trials were published in 2008 , and in 2002 for the ontario trial , which suggested that the hypofractionated regimens were as safe and e ective as the historical standard control schedule of 50 gy in 25 fractions . 
10 - year follow - up results of the ontario trial were published in 2010 , and an updated cochrane systematic review was published in 2010 . interpretation following publication of 5 - year results from the ontario and start trials , long - term follow - up was needed to con rm the safety and e cacy of the hypofractionated schedules . 
the 10 - year start trial results presented here , together with the long - term results of the ontario trial , con rm the earlier ndings and strengthen the evidence in favour of using hypofractionated schedules for breast cancer radiotherapy . 
they support the continued use of 40 gy in 15 fractions as the uk standard of care as recommended by the national institute for health and care excellence , and contribute further to the worldwide debate about breast cancer radiotherapy hypofractionation . vol 14 october 2013 1093 articles informed by the results of the pilot fast trial ( n = 915 ) .20 in conclusion , long - term follow - up of the start trials con rms that appropriately dosed hypofractionated radiotherapy is safe and e ective for patients with early breast cancer . contributors jry was chief investigator and chair of the trial management group . 
 rka , jb , pjb - l , hjd , pal , and bjm contributed to trial design , trial management , data interpretation , and commented on the report . con icts of interest we declare that we have no con icts of interest . 
we thank cancer research uk , the uk medical research council , and the uk department of health for providing the funds to undertake this research ( grant g9600656 )  . 
the start trialists group consists of the trial management group ( appendix ) , consumers , trial steering committee , independent data monitoring committee , and the principal and main co - investigators at the participating centres ( published previously ) .8 , 10 corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 comment with colorectal cancer ? there are some arguments against this opinion . 
first , the results of the focus2 trial6 supported the use of rst - line oxaliplatin - based combination chemotherapy rather than uoropyrimidine monotherapy in elderly or frail patients with advanced colorectal cancer , although the primary endpoint of progression - free survival did not di er signi cantly . 
 second , pooled analyses7 , 8 of elderly patients randomised studies showed a bene t of oxaliplatinbased or irinotecan - based combination chemotherapy in patients aged 70 years and older similar to that in younger patients . 
finally , a pooled analysis9 showed that upfront combination chemotherapy ( compared with uoropyrimidine monotherapy ) showed a slightly higher in patients with a performance status of 2 than in those with a performance status of 01 , 9 which suggests that e ective rst - line combination chemotherapy is necessary for preventing early cancer - related death in some elderly patients without comorbidities , but with heavy tumour load . 
 stefan kubicka cancer center reutlingen , 72764 reutlingen , germany kubicka_s@klin - rt.de i am a scienti c advisor to , and have received honoraria from , merck , amgen , sano - aventis , and roche . kopetz s , chang gj , overman mj , et al . 
ann oncol 2012 ; 23 : 153136 . seymour mt , thompson lc , wasan hs , et al , on behalf of the focus2 investigators and the national cancer research institute colorectal cancer clinical studies group . 
irinotecan / uorouracil combination in rst - line therapy of older and younger patients with metastatic colorectal cancer : combined analysis of 2 , 691 patients in randomized controlled trials . 
pooled safety and e cacy analysis examining the e ect of performance status on outcomes in nine rst - line treatment trials using individual data from patients with metastatic colorectal cancer . 
j clin oncol 2013 ; 31 : 146470 . see articles page 1086 hypofractionated breast radiation : preferred standard of care ? in the lancet oncology , joanne haviland and colleagues1 report important 10 - year outcomes of the uk standardisation of breast radiotherapy ( start ) - a and start - b trials.2 , 3 these trials examined whether a shorter hypofractionation radiation schedule was as safe and e ective as the standard 5 week fractionation schedule for the treatment of breast cancer . 
coupled with long - term results from a similar randomised trial led by the ontario clinical oncology group , 4 these ndings provide robust evidence that most patients with breast cancer can receive a hypofractionated schedule that remains bene cial whilst decreasing treatment duration . 
of these two studies , the 1032 vol 14 october 2013 comment start - b trial is more clinically relevant because this study contracted the overall treatment time from 5 to 3 weeks , which provides clear socioeconomic bene ts for both patients and health systems . 
start - b compared the standard treatment of 50 gy given in 25 fractions over 5 weeks with or without a 1 week tumour bed boost with a schedule of 40 gy in 15 fractions over 3 weeks ( hypofractionation ) with or without a 1 week tumour bed boost . 
they found that the two schedules led to similar numbers of patients having local - regional relapse at 10 years ( 55% , 95% ci 4272 vs 43% , 3259 ; hazard ratio [ hr ] 077 , 95% ci 051116 ; p = 021 )  . 
 should these ndings lead to abandonment of the 56 week standard for all patients with breast cancer ? because only a minority of patients ( 116 [ 7% ] of 2215 ) in start - b received regional lymphatic radiation , a more conservative approach might be to continue to use the standard regimen in patients who receive regional nodal irradiation after lumpectomy or mastectomy . 
however , the investigators reported no evidence of increased normal tissue e ects of the brachial plexus , arm oedema , or shoulder sti ness with hypofractionation in patients who did receive lymphatic treatment . 
these clinical outcomes are also consistent with theoretical modelling of normal tissue e ects , which predicts that 40 gy in 15 fractions should be as safe as 50 gy in 25 fractions for all normal tissues.5 thus , we agree with haviland and colleagues that hypofractionation is a reasonable approach even when treating the regional lymph nodes . 
 however , we also understand why many physicians might choose a more conservative approach as far more data are available about the standard regimen for treatment of regional lymph nodes . 
we also concur with the authors that techniques used to protect the heart are important for both radiotherapy schedules and the choice of fractionation should not be a ected by whether the tumour is in the right or left breast . 
 another subject of controversy is whether patients treated with the hypofractionated schedule could subsequently be treated with a tumour bed boost , as is often done for patients treated with the standard radiotherapy regimen . 
although use of a tumour bed boost was optional in the start trials , it was common : 1152 ( 61% ) of 1900 patients who had breast - conserving surgery had tumour bed boost radiotherapy in start - a , as did 868 ( 43% ) of 2038 patients in start - b . 
however , as tumour control and normal tissue outcomes did not di er signi cantly between patients who received tumour bed boost and those who did not , we therefore agree with the authors that the use of a boost with a hypofractionated schedule seems to be safe and e ective . 
 breast cancers are molecularly heterogeneous and tumours with di erent oestrogen , progesterone , and her2 statuses respond di erently to treatment.6 most patients in both the start trials and the ontario study had oestrogen receptor - positive , her2 - negative tumours , therefore the analyses were underpowered to measure the e ect of breast cancer subtype on e cacy of the hypofractionated schedule . 
tumour grade did not have an e ect in the start trials2 , 3 whereas in the ontario trial4 patients with high grade disease had better outcomes with standard radiotherapy . 
 vol 14 october 2013 1033 comment published online september 12 , 2013 s1470 - 2045 ( 13 ) 70403 - 0 see articles page 1095 * bruce g ha ty , thomas a buchholz department of radiation oncology , rutgers - cancer institute of new jersey , robert wood johnson medical school and new jersey medical school , new brunswick , nj 08903 , usa ( bgh ) ; and division of radiation oncology , university of texas , md anderson cancer center , houston , tx , usa ( tab ) ha tybg@cinj.rutgers.edu we declare that we have no con icts of interest . 1 haviland js , owen jr , dewar ja , et al . 
the uk standardisation of breast radiotherapy ( start ) trials of radiotherapy hypofractionation for treatment of early breast cancer : 10 - year follow - up results of two randomised controlled trials . 
jama 2012 ; 308 : 163536 . bayesian analysis unravels pancreas - cancer adjuvant therapy of all the recent advances being made in pancreatic cancer , the three - times improvement in long - term survival from the use of adjuvant chemotherapy after pancreas - cancer resection is the most striking . this notion was rst introduced by the gastrointestinal tumor study group in the usa in the 1970s in a randomised controlled trial comparing a combination of adjuvant chemoradiation with uorouracil with subsequent maintenance chemotherapy , also with uorouracil , with a control group of post - resection observation.1 the target was 150 patients , but this trial was closed after 8 years with just 43 patients recruited , in part because of substantial concerns over toxic e ects . 
 however , there was still a signi cant survival advantage for the adjuvant chemoradiation and maintenance uorouracil group compared to the control group.1 this regimen became common practice in the usa , but the strength of evidence was thought too weak to greatly alter clinical practice elsewhere . 
 that was until the adjuvant european study for pancreatic cancer ( espac ) 1 trial provided strong evidence for improved survival using just maintenance chemotherapy ( using uorouracil and folinic acid ) but , perhaps surprisingly at the time , there was no evidence from the trial data that adjuvant chemoradiation provided any survival bene t.2 , 3 controversially , the factorial design of espac 1 , which aimed to answer the two main questions on adjuvant therapywhether and whether chemotherapy chemoradiotherapy improved survivalwas heavily criticised by some us radiation oncologists and there were also claims of poor radiotherapy quality control.4 however , an eortc trial of adjuvant chemoradiation improved survival follow - on maintenance ( without chemotherapy ) 5 was promoted as supporting evidence for chemoradiotherapy , but was said to be underpowered because there was no signi cant survival advantage compared to the control observation group.4 it was not until 2008 that the rst major us adjuvant trial was published by the radiation therapy oncology group ( rtog ; 9704 trial ) , in which 538 patients were randomised to receive either gemcitabine before ( with uorouracil ) or and after chemoradiation uorouracil before and after chemoradiation.6 there was no di erence in median survival in the 451 patients analysed ( 167 and 18.8 months respectively ) and median survival was actually less than in the espac - 1 chemoradiotherapy group . 
although the rtog 9704 investigators reported the lowest local recurrence rate reported so far ( 23% ) , metastatic spread to the liver and elsewhere was still very high ( 70% ) suggesting relative lack of systemic e cacy in the combination used.6 despite the mounting evidence supporting chemotherapy , now in the form of gemcitabine7 as well as uorouracil plus folinic acid , adjuvant chemoradiation was still being promoted . 
 the simmering controversy led to a strong editorial by renee twombly8 in the journal of the national cancer institute , calling for more data to inform the debate on the use of adjuvant chemoradiation . 
despite further randomised trials supporting adjuvant chemotherapy , adjuvant chemoradiation is still recommended in the usa . in the lancet oncology , a study by wei - chih liao and colleagues9 now pulls together nine controlled trials with a total of 3033 patients randomised to receive 1034 vol 14 october 2013 corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
we investigated whether the frameshift nature of indel mutations , which create novel open reading frames and a large quantity of mutagenic peptides highly distinct from self , might contribute to the immunogenic phenotype . methods we analysed whole - exome sequencing data from 5777 solid tumours , spanning 19 cancer types from the cancer genome atlas . 
we assessed in - silico tumour - specific neoantigen predictions by mutation type with pan - cancer analysis , together with rnaseq profiling in renal clear cell carcinoma cases ( n = 392 ) , to compare immune gene expression across patient subgroups . 
associations between indel burden and treatment response were assessed across four checkpoint inhibitor datasets . findings we observed renal cell carcinomas to have the highest proportion ( 012 ) and number of indel mutations across the pan - cancer cohort ( p < 22 10 ) , more than double the median proportion of indel mutations in all other cancer types examined . 
immune gene expression analysis in the renal clear cell carcinoma cohort showed that the presence of mutant - specific neoantigens was associated with upregulation of antigen presentation genes , which correlated ( r = 078 ) with t - cell activation as measured by cd8 - positive expression . 
finally , analysis of checkpoint inhibitor response data revealed frameshift indel count to be significantly associated with checkpoint inhibitor response across three separate melanoma cohorts ( p = 47 10 )  . interpretation renal cell carcinomas have the highest pan - cancer proportion and number of indel mutations . 
 evidence suggests indels are a highly immunogenic mutational class , which can trigger an increased abundance of neoantigens and greater mutant - binding specificity . funding cancer research uk , uk national institute for health research ( nihr ) at the royal marsden hospital national health service foundation trust , institute of cancer research and university college london hospitals biomedical research centres , the uk medical research council , the rosetrees trust , novo nordisk foundation , the prostate cancer foundation , the breast cancer research foundation , the european research council . copyright the author ( s )  . 
the data have also been scrutinised for mutations that might play a role in the recognition of cancer cells by the immune syste the focus of these analyses to a large extent is on the single nucleotide variants ( snvs ) , on account of the relative simplicity and reliability of calling sequence changes of one base pair ( bp ) fixed length . 
as a consequence , the effect of small scale insertion and deletion mutations ( indels ) on antitumour immunity has been poorly characterised despite the clear link of such mutations to oncogenesis3 and their potential to generate highly immunogenic peptides . inhibitor the notion the success of checkpoint therapies underlines tumour - specific t - cell that responses pre - exist in some patients and are kept under tight control via immune modulatory mechanisms . 
the predominant focus of existing literature was on single nucleotide variation ( snv ) mutations , with no previous study done of insertion and deletion ( indel ) mutations on a pan - cancer basis . 
regarding the association between somatic mutations and upregulation of antitumour immunity via checkpoint inhibition , several previous studies reported a link between high snv load and improved response to checkpoint inhibition . 
no previous pan - cancer study has investigated the difference between snv and indel - derived neoantigens , despite the propensity of indels to generate highly mutagenic peptides via creation of a shifted novel open reading frame . added value of this study we did a pan - cancer assessment of indel load across 5777 tumour samples spanning 19 cancer types . 
kidney tumours were observed to have the highest proportion and absolute count of indel mutations on a pan - cancer basis , a result which was replicated in two further independent datasets . 
finally , we assessed the association between indel load and checkpoint inhibitor response in three melanoma cohorts , which showed indel load to be more strongly associated with response than non - synonymous ( ns ) snv load . implications of all the available evidence our data highlight the importance of frameshift neoantigens alongside nssnv neoantigens as determinants of immunotherapy efficacy and potentially crucial targets for vaccine and cell therapy interventions . 
t cells reactive to tumour - specific mutant antigens ( neoantigens ) have been detected epithelial malignancies4 and neoantigens are increasingly shown to be the target of checkpoint inhibitor - induced t - cell responses5 , 6 and adoptively transferred t cells.79 many investigators are leveraging whole - exome sequencing and rna sequencing , focusing on non - synonymous snvs ( nssnvs ) , to predict expressed mutated peptides that bind mhc class i molecules ( snv - neoantigens )  . 
 neoantigen burden is closely related to the nssnv burden , which varies significantly across cancer types , from one nssnv in paediatric tumours to more than 1500 nssnvs in tumours associated with microsatellite instability.10 however , less than 1% of the nssnvs in expressed genes lead to detectable cd4 - positive11 or cd8 - positive t - cell7 reactivities in tumour - infiltrating lymphocytes . 
accordingly , efficacy of checkpoint inhibitors is most marked in tumour types with a high nssnv lung adenocarcinoma , lung squamous cell carcinoma , head and neck squamous cell carcinoma , and carcinoma of the bladder , 10 which reflects a higher probability of creating a neoantigen that will be presented to and recognised by t cells . 
furthermore , within these tumour types , nssnv and neoantigen burdens correlate with response to checkpoint inhibitors.1216 a notable outlier is renal clear cell carcinoma , which has a relatively low nssnv burden ( around ten times lower than melanoma )  . 
 including melanoma , burden , renal clear cell carcinoma is characterised by a high level of tumour - infiltrating immune cells17 and has been interferon - , high - dose shown interleukin 2 , 18 , 19 and , more recently , checkpoint inhibitors , 20 , 21 but the mutational and antigenic determinants of these responses are unknown . respond from self indel mutations that cause a frameshift ( frameshift indels ) create a novel open reading frame and could produce a large quantity of neoantigenic peptides highly distinct ( appendix p 5 )  . 
it has been hypothesised22 that novel open reading frames might be an ideal source of tumour - derived neoantigens and so induce multiple neoantigen reactive t cells , because of both an increased number of mutant peptides and reduced susceptibility to self - tolerance mechanisms . 
on this basis , we aimed to characterise the pattern of indel mutations with pan - cancer analysis and investigate their association with antitumour immune response and outcome following checkpoint blockade . methods study design and participants pan - cancer somatic mutational data were obtained from the cancer genome atlas ( tcga ) for whole - exome sequencing data of 5777 solid tumours , across 19 cancer types : bladder urothelial carcinoma , invasive breast carcinoma , cervical and endocervical cancers , colorectal adenocarcinoma , glioma , head and neck squamous cell carcinoma , chromophobe renal cell carcinoma , renal clear cell carcinoma , renal papillary cell carcinoma , liver hepatocellular carcinoma , lung adenocarcinoma , serous lung carcinoma , ovarian squamous cell 1010 vol 18 august 2017 articles pancreatic cystadenocarcinoma , adenocarcinoma , prostate adeno carcinoma , skin cutaneous melanoma , stomach adenocarcinoma , thyroid carcinoma , and uterine carcinosarcoma . 
we performed replication analyses in two additional cohorts of patients with renal clear cell carcinoma : a whole - exome sequencing study of 106 patients with renal clear cell carcinomas reported by sato and colleagues23 and a whole - exome sequencing study of ten patients with renal clear cell carcinomas reported by gerlinger and colleagues.24 we obtained final post - quality control patient - level mutation annotation files for each study . to further test for an association between nssnvs or indel loads and patient response to checkpoint inhibitor therapy we used four patient cohorts . 
the first dataset consisted of 38 patients with melanoma treated with anti - pd - 1 therapy , as reported by hugo and colleagues.25 we obtained final post - quality control mutation annotation files and clinical outcome data , and 34 patients were retained for analysis after exclusion of cases in which dna had been extracted from patientderived cell lines and patients in whom tissue tumor purity was below 20% . 
four samples from hugo and colleagues25 were taken after a short period on treatment , which raises the possibility that checkpoint inhibitor therapy itself might have affected mutational frequencies through possible elimination of immunogenic tumour clones . 
to be consistent with the original study , these samples were not excluded ; however , we note the frameshift indel association presented becomes more significant with these cases removed . 
the second checkpoint inhibitor cohort comprised of 62 patients with melanoma treated with anti - ctla - 4 therapy , as reported by snyder and colleagues.13 all patients samples were taken from fresh snap frozen tumour tissue with tumour purity of more than 20% so , accordingly , all 62 cases were retained for analysis . 
the snyder and colleagues cohort also contained a number of samples taken on treatment ; these samples have been retained for consistency ; however , we note again the significance of results strengthens if they are removed . 
 the third checkpoint inhibitor cohort comprised of 100 patients with melanoma treated with anti - ctla - 4 therapy , as reported by van allen and colleagues ; 12 one patient ( pat21 ) was excluded because of a tumour purity of less than 20% . 
the final checkpoint inhibitor cohort comprised of 31 patients with non - small - cell lung cancer treated with anti - pd - 1 therapy , as reported by rizvi and colleagues ; 14 all patients were eligible for inclusion . 
for these four cohorts , 1214 final mutation annotation files , including indel mutations , were not available , so we obtained raw bam files and undertook variant calling using a standardised bioinformatics pipeline . 
to assess for a general association between nssnvs or indel loads and patient overall survival we used a final cohort of 100 patients with non - small - cell lung cancer , as reported by jamal - hanjani and colleagues.26 we obtained final post - quality control mutation annotation files and clinical outcome data , and 88 patients were retained for analysis after exclusion of non - smokers . 
we used picard tools , gatk ( version 2.8.1 ) , and fastqc ( version 0.10.1 ) to produce quality samtools mpileup ( version 0.1.19 ) 29 was used to locate non - reference positions in tumour and germline samples . 
 following completion , variants called by mutect were filtered according to the filter parameter pass . in the pan - cancer cohort , snv and indel mutation counts were computed per case , considering all variant types . 
we estimated the extent of nmd for all indel and snv mutations ( with snv mutations used as a benchmark comparator ) by comparing mrna expression in samples with a mutation to the median mrna expression of the same transcript across all other tumour samples in which the mutation was absent . 
specifically , mrna expression of every mutation - bearing transcript was divided by the median mrna expression of that transcript in non - mutated samples , to give an nmd index . 
tumour purity in the renal clear cell carcinoma cohort was 054 , 32 quantified by histological assessment , and assuming constant expression in the remaining 046 normal cellular content , that would yield an adjusted 14% drop in expression in indel - mutationbearing cancer cells . 
if we assume that tumour mutations are clonal , of heterozygote genotype , in a diploid genomic region , and wild - type allele expression in mutated cancer cells remains constant , a purity - adjusted reduction of 05 would be expected under a model of fully effective nmd . 
these data are presented as a global approximation of nmd efficiency , using methods in line with previous publications.33 nmd index values were log indicating no mrna degradation and plotted for indel or snv mutations . transformed , with 0 we used pyclone34 and ascat35 to determine the clonal status of variants in the cohorts by snyder and colleagues13 and van allen and colleagues.12 for each case variant calls were integrated with local allele - specific copy number ( obtained from ascat ) , tumour purity ( also obtained from ascat ) , and variant allele frequency . 
for a number of tumours the reliable copy number , mutation , and purity estimations could not be clonal architecture analysis extracted , rendering and colleagues in snyder intractable and these tumours were omitted from the analysis . 
a strong binding threshold was used for wild - type alleles to ensure fair comparison between snv - derived and indel - derived neoantigens , in view of the high incidence of wild - type non - binders for indels . 
we excluded ( from the pancancer neoantigen analyses ) cancers that were associated with a high level of viral genome integration , including cervical ( > 80% rate of human papillomavirus integration ) and hepatocellular carcinoma ( > 50% rate of hepatitis b integration ) , but not head and neck squamous cell ( < 15% rate of human papillomavirus carcinoma integration )  . 
no tcga dataset was available for merkel cell carcinoma . immune gene signature data were obtained from rooney and colleagues , 40 with gene sets defined as stated in the appendix ( p 3 )  . 
a high burden of frameshift indel high - affinity neoantigens was defined as more than 10 per case ( n = 32 ) , and the percentage difference in expression was compared between the high indel neoantigen group and all other patients across each immune signature . 
the same analysis was repeated for a high burden of snv - derived high - affinity 1012 vol 18 august 2017 articles neoantigens , with a threshold of more than 17 snv neoantigens selected to size match the high burden groups ( equal number of patients ; n = 32 across all highload groups ) across mutational types . 
 we did correlation analysis within the high - frameshift indel neoantigen group ( n = 32 patients with renal clear cell carcinoma )  . outcomes across the four cohorts of patients treated with checkpoint inhibitors , we tested nssnv , all - coding indel , and frameshift indel variant counts for an association with patient response to therapy . 
 for snyder and colleagues cohort , 13 long - term clinical benefit was defined as radiographic evidence of freedom from disease , evidence of a stable disease , or decreased volume of disease for more than 6 months . 
no long - term clinical benefit was defined as tumour growth on every ct scan after the initiation of treatment ( no benefit ) or a clinical benefit lasting 6 months or less ( minimal benefit )  . 
for hugo and colleagues cohort , 25 responding tumours were complete response , partial response , and stable disease , and non - responding tumours were defined as disease progression . 
for van allen and colleagues cohort , 12 clinical benefit was defined as complete response , partial response , or stable disease , and no clinical benefit was progressive disease or stable disease with overall survival less than 1 year . 
for rizvi and colleagues cohort , 14 durable clinical benefit was defined as partial response or stable disease lasting longer than 6 months , and no durable benefit was progressive disease less than 6 months from beginning of therapy . 
 multivariate cox regression was done with relapse - free survival versus indel load with stage , adjuvant therapy ( yes or no ) , age , and histology included in the model . we compared indel burden and proportion measures between renal cell carcinomas and all other non - kidney cancers with a two - sided mann - whitney u test . 
in the checkpoint inhibitor response analysis , nssnv , exonic indel , and frameshift indel counts were each compared to patient response outcome using a two - sided mannwhitney u test . 
we carried out statistical analyses using r ( version 3.0.2 ) and considered a p value of 005 or less ( two - sided ) as being statistically significant . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results we observed a median indel proportion value of 005 and a median indel count of 4 , cohort - wide . 
across all tumour types , renal clear cell carcinoma was found to have the highest proportion of coding indels , 012 ( p < 22 10 ; figure 1 ) , a 24 times increase when compared with the pan - cancer average . 
this result was replicated in two further independent cohorts , with median observed indel proportions of 010 in sato and colleagues study23 and 012 in gerlinger and colleagues study24 ( figure 1 )  . 
renal papillary cell carcinoma and chromophobe renal cell carcinoma had the second and third highest indel proportion , suggesting a possible tissue - specific mutational process contributing to the acquisition of indels in renal cancers . 
renal papillary cell carcinoma ( median indel number of 10 [ 95% ci 911 ] ) and chromophobe renal cell carcinoma ( 8 [ 710 ] ) had the highest absolute indel count across all tumour types , closely followed by renal clear cell carcinoma ( 7 [ 68 ] )  . 
 renal clear cell carcinoma is characterised by loss - offunction mutations in one or more tumour - suppressor genes : vhl , pbrm1 , setd2 , bap1 , and kdm5c , 32 which can be inactivated by nssnv or indel mutations . 
 to exclude the possibility that these hallmark mutations were distorting the results , we recalculated renal clear cell carcinoma indel proportion excluding these genes ; the revised indel proportion remained at 012 . 
when we used previously published multiregion whole - exome sequencing data24 from ten cases of renal clear cell carcinoma to assess the clonal nature of indel mutations , 53 ( 48% ) of 110 frameshifting indels were clonal in nature ( present in all tumour regions )  . the overall effect of nmd on the expression of indelmutated genes was estimated to be 14% ( 7% drop divided by 054 tumour purity ) , suggesting it operates on a subset of transcripts ( appendix p 6 )  . next we sought to investigate the potential immunogenicity of nssnv and indel mutations through analysis of mhc class i - associated tumour - specific neoantigen binding predictions in the pan - cancer tcga cohort . 
the last two boxplots are additional independent renal clear cell carcinoma replication datasets from sato and colleagues23 and gerlinger and colleagues.24 statistical comparison is renal clear cell carcinoma cohort compared with all other non - kidney tcga samples . 
 mutations ( n ) neoantigens ( n ) * mutant - specific neoantigens ( n ) neoantigens per mutation mutant - specific neoantigens per mutation nssnvs fs - indels 335 594 19 849 214 882 39 768 75 224 39 608 enrichment 064 200 313 022 200 894 nssnvs = non - synonymous single nucleotide variants . 
in a similar manner , predictions were made on 19 849 frameshift indel mutations , resulting in 39 768 high - affinity binders with a rate of 200 neoantigens per frameshift mutation ( frameshift neoantigens ; table )  . 
thus on a per mutation basis , frameshift indels could generate around three times more high - affinity neoantigen binders than nssnvs ( table ) , consistent with the prediction in a recent analysis of a colorectal cancer cohort.41 when both wild - type and mutant peptides are predicted to bind , central immune tolerance mechanisms might delete cells with the reactive t - cell receptor.42 therefore , we repeated a pancancer analysis restricting the neoantigens to mutantspecific binders ( ie , where the wild - type peptide is not predicted to be a strong binder ) , and showed that frameshift indels were nine times enriched for mutantallele - only binders ( table )  . of particular interest were genes that are frequently altered via frameshift mutations and with high propensity for mhc binding . 
in a pan - cancer analysis , these genes were enriched for classic tumour - suppressor genes , including tp53 , arid1a , pten , kmt2d , kmt2c , apc , and vhl ( figure 2 )  . 
collectively , the top 15 genes with the highest number of frameshift mutations were mutated in more than 500 samples ( approximately 10% of the cohort with 5777 samples ) with more than 2400 highaffinity neoantigens predicted . 
 furthermore , by virtue of being founder events , many alterations in tumour - suppressor genes are clonal , present in all cancer cells , rendering them compelling targets for immunotherapy.43 we next considered the clinical effect of indel mutations the association between neoantigen by assessing enrichment and therapeutic benefit . 
consistent with a potential role of frameshifts in the generation of neoantigens , those tumour types approved for the use of checkpoint inhibitors were all found to harbour an above average number of frameshift neoantigens , despite substantial differences in the total snv or indel mutational burdeneg , renal cell carcinoma ( figure 3 )  . 
 overall , the number of frameshift neoantigens were significantly higher in the checkpoint inhibitor - approved tumour types versus those that have not been approved to date ( p < 22 10 )  . 
however , the potential presence of frameshift neoantigens alone does not imply that they induce t - cell responses , and hence we tested their effect on checkpoint inhibitor efficacy . 
 although nssnvs ( p = 027 ) and in - frame ( 3n ) indels from an anti - pd - 1 study25 1014 vol 18 august 2017 articles ( p = 019 ) had no association with response to treatment , frameshift indel mutations were significantly associated with anti - pd - 1 response ( p = 0023 ; figure 4a )  . 
the upper quartile of patients with the highest burden of frameshift indels had an 88% ( seven of eight cases ) response to antipd - 1 therapy , compared with 43% ( 11 of 26 cases ) for the lower three quartiles ( odds ratio 95 [ 95% ci 1028923 ] ; figure 4b )  . 
to confirm the reproducibility of this association , further checkpoint inhibitor response data were obtained from two additional melanoma cohorts : snyder and colleagues cohort13 ( n = 62 , anti - ctla - 4 treated ) and van allen and colleagues cohort12 ( n = 100 , anti - ctla - 4 treated )  . 
we did the same analysis in each cohort and frameshift indel burden was significantly associated with checkpoint inhibitor response in both datasets ( hr 34 [ 95% ci 1051127 ] ; p = 00074 for snyder and colleagues cohort and 29 [ 115755 ] ; p = 0032 for van allen and colleagues cohort ; figure 4a )  . 
 an overall meta - analysis across the three cohorts confirmed frameshift indel count to be associated with checkpoint inhibitor response ( p = 47 10 ) , and with a more significant association than nssnv count ( p = 48 10 )  . 
the effect of clonality was additionally assessed , and clonal frameshift indels were found to have a further significantly predictive advantage beyond all frameshift indels ( clonal and subclonal ; appendix p 7 ) , supporting previous work reported by our group.43 overall survival analysis was not different between high and low frameshift indel groups , possibly because of the effect of subsequent therapies on the overall survival ( or 243 [ 95% ci 077773 ] ; p = 0228 for hugo and colleagues cohort25 ; appendix p 8 )  . 
we assessed the association between frameshift indel load and checkpoint inhibitor response in another tumour type by using data obtained from rizvi and colleagues small cohort14 of 31 patients with non - small - cell lung cancer treated with anti - pd - 1 therapy ; no difference was observed ( p = 023 )  . 
 to further investigate the importance of frameshift indels in non - small - cell lung cancer , we did additional analysis using data from jamal - hanjani and colleagues cohort26 of 100 cases , none of whom received treatment with checkpoint inhibitors . 
consistent with our previous findings , 43 we observed lung adenocarcinoma whose tumour 's harboured a high clonal neoantigen burden ( higher than upper quartile of cohort ) survival compared with the bottom three quartiles ( p = 0026 )  . 
 however , across all histological subtypes of non - smallcell lung cancer , survival was found to be significantly improved for patients with a high load of frameshift indels ( vs low load : hr 025 [ 95% ci 006108 ] ; p = 0045 ) ; by contrast , nssnv load was not formally associated ( 036 [ 011121 ] ; p = 0084 ; appendix p 9 )  . 
 of note , the strongest prognostic predictor was for patients in the patients with a high load of both nssnvs and frameshift indels , with elevated levels of both frameshift indels and nssnvs , with no events in this that patients with relapse - free improved exhibited arid1a mll3 mll2 tp53 vps13c map3k1 flna fat1 notch1 pten number of samples mutated figure 2 : recurrent genes with frameshift indel neoantigens data are from all patients in the cancer genome atlas pan - cancer cohort . 
the graph shows the number of unique samples containing a frameshift indel neoantigen and the number of unique neoantigens ( ie , each mutation can generate multiple neoantigens )  . 
multivariate analysis showed some evidence of correlation between variables ( appendix p 2 ) , so further investigation of nssnvs and frameshift indels as predictors in larger patient cohort will be required to draw definitive conclusions . analyses of the indel load and proportion of response achieved from phase 2 studies for the tumour types not approved for checkpoint inhibition were limited by the small sample size and variable patient inclusion criteria such as pdl - 1 immunohistochemistry ( appendix p 4 )  . 
 nevertheless , the proportion of patients achieving a response was higher in triple - negative breast cancer44 compared with other invasive breast carcinoma molecular subtypes , and triple - negative invasive breast carcinoma has a higher burden of frameshift and mutant - specific neoantigens ( figure 3 )  . 
furthermore , mutational burden has been reported as higher in brca1 - mutated triplenegative breast cancer compared with brca - wild - type triple - negative breast cancer , 45 and we specifically observed a higher indel load in these cases ( appendix p 10 )  . 
 however , this outcome did not correlate with tumourinfiltrating lymphocyte density ( appendix p 10 ) , possibly because of the small sample size , absence of indel immunogenicity in this tissue type , or additional factors that modulate tumour - infiltrating lymphocyte density . finally , although genomic data are not available to correlate with checkpoint inhibitor response in renal clear cell carcinoma , we analysed the association between frameshift neoantigen load and immune responses within the tumour using rnaseq gene expression data . 
a high load of frameshift neoantigens was associated with upregulation of immune signatures classically linked to immune activation , including mhc class i antigen and presen tation , cd8 - positive t - cell increased cytolytic activity , a pattern not observed in the high snv - neoantigen group ( figure 5 )  . 
furthermore , correlation analysis within the high frameshift neoantigen group showed that cd8 - positive t - cell signature was correlated with both mhc class i antigen presentation genes ( r = 078 ) and cytolytic activity ( r = 083 ; figure 5 )  . activation , discussion in this study , we analysed the pattern of indel mutations across 19 solid tumour types and found that renal clear cell carcinoma , renal papillary cell carcinoma , and chromophobe renal cell carcinoma have the highest indel rate as a proportion of their total mutational burden and the highest overall indel count and are enriched for mutant - specific neoantigens . 
we also observed that indel number is significantly associated with checkpoint inhibitor response in melanoma . in non - smoking non - small - cell indels are thought to occur as a result of dna strand slippage during dna synthesis46 and their frequency is higher in repetitive sequences , especially those that are at - rich . 
indels are also generated through mutagen exposure , with a higher number observed in smoking than lung cancer ( lung adenocarcinoma ) 40 and higher in uv - exposed ( cutaneous ) versus uv - protected ( mucosal ) melanomas.47 less is known about the repair of indels than snvs ; however , the role of the mismatch repair mechanism instability - high phenotype , characterised by excess indels in repetitive sequences as seen in patients with lynch syndrome . 
 although renal clear cell carcinoma has been reported in patients with lynch syndrome , 48 this cannot account for the overall pattern of indel rates across renal clear cell the microsatellite illustrated by figure 3 : tumour - specific neoantigen counts by cancer type count of snv - derived neoantigens ( a ) , frameshift indel - derived neoantigens ( b ) , and mutant - only neoantigen binders ( c ) , and proportion of neoantigens derived from snvs and indels ( d ) and neoantigens in which mutant allele - only binds ( e )  . 
most renal clear cell carcinomas have loss of chromosome 3p , which encodes the mismatch repair gene mlh1 , but the remaining allele is rarely mutated in sporadic renal clear cell carcinoma . 
another relevant gene encoded on 3p is fhit , and its deficiency has been linked with indel accumulation in knockout mouse models , but the consequences of the heterozygous knockout ( whether haploinsufficient ) are unknown.49 however , as loss of 3p is an infrequent event in renal papillary cell carcinoma and chromophobe renal cell carcinoma and indels are also elevated in both these tumour types , other tissuespecific phenomena are likely to contribute to the increased indel burden across all renal carcinoma subtypes.50 renal clear cell carcinoma and renal papillary in the proximal tubule and cell carcinoma arise chromophobe renal cell carcinoma in the distal tubule of the nephron , and this shared tissue context might be important , even if the three subtypes are molecularly distinct.32 , 50 , 51 the nephron , and the proximal tubule in particular , play a crucial role in the reabsorption of vast volumes of renal filtrate and elimination of waste products of metabolism and toxins , with the effects of toxin elimination evident in the increased incidence of renal clear cell carcinoma in those individuals exposed to aristolochic acid.52 ochratoxin a , a mycotoxin , induces renal tumours in rodents by causing double - strand breaks.53 poly morphisms in genes involved in the repair of double - strand breaks are associated with an increased risk of renal clear cell carcinoma.54 double - strand breaks are mostly repaired by non - homologous end - joining , which is error - prone and can increase the rate of small indels ( 110 bp )  . 
therefore , it is possible that an environmental toxin causes an excess of double - strand vol 18 august 2017 1017 articles a co - inhibition_apc type_ii_ifn_response cytolytic_activity co - inhibition_t_cell co - stimulation_apc pdcs mhc_class_i cd8_t_cells r = 078 mhc class i if - indel - m utations fs - indel - neoatgs ns - snv - neoatgs r = 083 cytolytic activity figure 5 : immune gene signatures in patients with renal clear cell carcinoma ( a ) percentage change in median gene signature expression is shown between high and low groups for each metric on the x - axis as labelled . 
 ( b ) correlation analysis within the high fs - indel - neoatgs group showed the cd8 + t - cell signature was correlated with both mhc class i antigen presentation genes and cytolytic activity . 
brca1 has been shown to inhibit error prone non - homologous endjoining.55 however , we did not observe a correlation between indel load and tumour - infiltrating leucocytes density invasive breast carcinoma . 
 triple - negative in brca1 we observed that indels , which alter the reading frame , generate three times as many predicted neoantigens as nssnvs and nine times as many strong mutant - binding neoantigens where the wild - type sequence is not predicted to strongly bind the hla molecule ( ic50 > 50 nm )  . 
in keeping with this notion , microsatellite instability - high colorectal cancer cd8 - positive leucocytes density correlates positively with the total number of frameshift mutations.56 with the exception of polyomavirus - positive merkel cell carcinoma and hodgkins lymphoma , renal clear cell carcinoma is the only tumour type with a relatively low nssnv burden among the tumour types for which checkpoint inhibitors have been approved for tumour - infiltrating its clinical use . 
however , owing to a comparable frameshift level of mutant - specific high - affinity burden neoantigens is similar to that observed in non - small - cell lung cancer and melanoma , and the same is true of renal papillary cell carcinoma and chromophobe renal the cell carcinoma . 
although immunogenicity of renal papillary cell carcinoma is sparse , complete responses have been noted with the use of both high - dose interleukin 257 and anti - pd - 1 therapy.58 , 59 therapeutic data in chromophobe renal cell carcinoma are limited . the evidence for inhibitor drugs , efforts given the differential benefit across patients , the spectrum of immune - related adverse events , and the cost of checkpoint identify biomarkers of response are ongoing . 
mutational and neoantigen burdens have been shown to correlate with clinical outcomes from checkpoint inhibitor therapy in patients with advanced melanoma , colorectal cancer , and nonsmall - cell lung cancer.13 , 14 , 16 however , some patients with cutaneous melanoma with a low nssnv burden still derive benefit from checkpoint inhibitors , as do some patients with uv - protected mucosal melanomas , 60 which have a characteristically low nssnv burden.61 we analysed three melanoma datasets for which both response and mutational data were available . 
in two of the three studies , 13 , 14 comprising a total of 96 patients treated with either anti - pd - 1 or anti - ctla - 4 therapy , frameshift indel burden was a better predictor of response than nssnv burden . 
in the third study12 of 100 patients treated with anti - ctla - 4 therapy , the nssnv burden and frameshift burden were both significantly associated with checkpoint inhibitor response . 
we note that most of the patients in van allen and colleagues cohort12 were pretreated and therefore any mutational biomarker assessment in this group might be less reliable . although nssnvs contribute greatly towards tumour immunogenicity in heavily mutated tumours , our analyses suggest that frameshift mutations also make a significant contribution relative to their overall low number . 
the contribution of frameshift indels in low nssnv burden tumours might be of greater importance still , as illustrated by the fact that frameshift mutations contribute over a third of the neoantigen load in renal clear cell carcinoma . 
mutational and checkpoint inhibitor response data were not available for renal clear cell carcinoma , hence we could not establish a direct association between frameshift indels and positive checkpoint inhibitor response . 
in terms of indirect evidence in renal clear cell carcinoma , we observed an association between the frameshift neoantigens and upregulation of machinery necessary for antigen presentation by the mhc complex and t - cell activation . 
 furthermore , the cd8 - positive t - cell signature in the frameshift neoantigen - high group was closely related to cytolytic activity , suggesting the presence of antitumour 1018 vol 18 august 2017 articles effectors that could confer sensitivity to immunotherapy . 
 however , no definitive conclusions can be drawn until checkpoint inhibitor response and indel load is directly investigated in a sufficiently powered series of renal clear cell carcinoma cases . lead to the for frameshift neoantigens to contribute to antitumour immunity the mutant peptides must be expressed . 
published analyses62 of germline samples show that premature loss of termination codons frequently expression of the variant allele , but that some mutant transcripts escape nmd on the basis of the exact location of the frameshift within a gene . 
combined analyses of than mutational and expression data 10 000 cancer samples showed that nmd is triggered with variable efficacy , and even when effective might not alter expression because of factors such as short mrna halflife.33 rnaseq analysis in renal clear cell carcinoma cases showed a minimal change in mrna transcript levels for frameshift indel - mutated tumours , suggesting nmd is operating on a subset of transcripts , as expected . 
in this context , the strongly hypoxic microenvironment that characterises renal clear cell carcinomas might be a contributing factor , with evidence showing nmd inhibition in cells subject to hypoxia and other perturbed microenvironmental conditions.63 from more clonal frameshift mutations could be an important source of tumour - specific antigens for personalised immunotherapy strategies , including peptide vaccines and adoptive cell therapy . 
tumour - reactive t cells recognising a frameshifted product of the cdkn2a tumour - suppressor gene were reported to mediate a potent in - vivo response in melanoma.64 in microsatellite instability - high colorectal cancer , frameshift neopeptidespecific cytotoxic t - cell responses were observed in patients harbouring those mutations.65 cytotoxic t - lymphocyte responses to frameshifted proteins have been detected in healthy hereditary non - polyposis colorectal cancer - mutation carriers , raising the possibility of protective immunosurveillance in this population.66 frameshift neoantigens are particularly pertinent in the context of mismatch repair - deficiency , which is a pancancer event , and crucially , frameshifts commonly occurring in microsatellite instability - high colorectal carcinomas have been shown to generate nmd - resistant transcripts.67 in support of this , in a study68 of pd - 1 blockade in patients with microsatellite instability - high tumours from various cancer subtypes , functional analyses in - vivo in a responding patient showed expansion of frameshift neoantigen - specific t - cell clones . frameshift neoantigens provide a unique opportunity to target common tumour - suppressor genes , such as such as tp53 and bap1 , 69 and their founder status also enriches for clonal neoantigens . 
neoantigens derived from driver mutations elicit profound t - cell exhaustion via chronic antigen stimulation , generating t - cell pools refractory to immune therapy.70 thus , early administration of checkpoint blockade might further improve clinical benefit in cancers with particularly antigenic mutations such as renal clear cell carcinoma . 
it is also noteworthy that a high differential affinity between wild - type and mutant peptides is indicative of enhanced tumour protection in vivo.71 the enrichment of mutant - only binders by nine times in neoantigens derived from frameshift mutations relative to nssnvs might therefore partly explain the predictive power of frameshift neoantigens in checkpoint inhibitor responses . a widely recognised challenge in bioinformatics is indel variant calling , due to the inherent nature of shortread sequencing technology ; however , accurate indel calling can be achieved within both a research and clinical context with strict quality control procedures.72 while strict quality control procedures can ensure a low false - positive rate , as a consequence the true rate of indel mutations might be underestimated . in conclusion , we report that kidney cancers carry the indel mutations . 
 highest pan - cancer burden of futhermore , our data suggest that frameshift indels are a highly immunogenic mutational class ; triggering an increased quantity of neoantigens and greater mutant binding specificity . 
collectively , these data might reconcile the outlier nature of immunotherapy responses in renal clear cell carcinoma , highlighting frameshift indels as a potential biomarker of checkpoint inhibitor response and supporting targeting of clonal frameshift indels by both vaccine and cell therapy approaches . the contributors st , kl , and cs designed the study and wrote the manuscript . 
all authors interpreted the data . declaration of interests st reports grants from ventana , outside the submitted work ; and has a patent on indel burden and checkpoint inhibitor response pending , and a patent on targeting of frameshift neoantigens for personalised immunotherapy pending . 
 nm reports personal fees from achilles therapeutics , outside of the submitted work ; and has two patents pending ( pct / ep2016 / 059401 and pct / ep2016 / 071471 )  . 
 jl reports personal fees from eisai , glaxosmithkline , kymab , roche / genentech , secarna , pierre fabre , and eusa pharma ; and grants and personal fees from bristol - myers squibb , merck sharp & dohme , pfizer , and novartis , outside of the submitted work . 
cs reports personal fees from janssen , boehringer ingelheim , ventana , novartis , roche , sequenom , natera , achilles therapeutics , and sarah cannon research institute , and personal fees and other from apogen biotechnologies , epic sciences , and grail , outside of the submitted work ; and has a patent on indel burden and checkpoint inhibitor response pending and a patent on targeting of frameshift neoantigens for personalised immunotherapy pending . 
all other authors declare no competing interests . vol 18 august 2017 1019 articles acknowledgments st is funded by cancer research uk ( grant reference number c50947 / a )  . 
tc , st , mg , and jl are funded by the national institute for health research ( nihr ) biomedical research centre at the royal marsden hospital national health service foundation trust ( st grant reference number a109 )  . 
cs is funded by cancer research uk ( tracerx ) , the rosetrees trust , novonordisk foundation ( id 16584 ) , eu fp7 ( projects predict and responsify , id number 259303 ) , the prostate cancer foundation , the breast cancer research foundation , the european research council ( theseus ) , and national institute for health research university college london hospitals biomedical research centre . 
we thank levi garraway , eli van allen , alexandra snyder , matthew hellman , naiyer rizvi , and timothy chan for kindly allowing access to their checkpoint inhibitor datasets . 
the results published here are in part based on data generated by the cancer genome atlas research network . corrections correction to lancet oncol 2013 ; 14 : 790 correction to lancet oncol 2013 ; 14 : 989 vandendriessche chuah mk . 
 fulvestrant placebo versus exemestane alone after progression on non - steroidal aromatase inhibitors in postmenopausal patients with hormone - receptor - positive locally advanced or metastatic breast cancer ( sofea ) : a composite , multicentre , phase 3 randomised trial . 
lancet oncol 2013 ; 14 : 98998in the methods section of the summary of this article , the rst part of the third sentence should have read participants were randomly assigned ( 1 : 1 : 1 ) to receive intramuscular fulvestrant ( 500 mg injection on day 1 , followed by 250 mg doses on days 15 and 29 , and then every 28 days )  . 
 vol 14 september 2013 e391 corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 articles preferences for cancer investigation : a vignette - based study of primary - care attendees jonathan banks , sandra hollinghurst , lin bigwood , tim j peters , fiona m walter , willie hamilton lancet oncol 2014 ; 15 : 23240 published online january 14 , 2014 s1470 - 2045 ( 13 ) 70588 - 6 see comment page 136 copyright banks et al . 
we investigated preferences for diagnostic testing for colorectal , lung , and pancreatic cancers in primary - care attendees . methods in a vignette - based study , researchers recruited individuals aged at least 40 years attending 26 general practices in three areas of england between dec 6 , 2011 , and aug 1 , 2012 . 
the vignettes outlined a set of symptoms , the risk that these symptoms might indicate cancer ( 1% , 2% , 5% , or 10% ) , the relevant testing process , probable treatment , possible alternative diagnoses , and prognosis if cancer were identi ed . 
we recorded no strong evidence that participants were more likely to opt for investigation with a 1% increase in risk of cancer ( odds ratio [ or ] 102 , 95% ci 099106 ; p = 0189 ) , although the association between risk and opting for investigation was strong when colorectal cancer was analysed alone ( 108 , 103113 ; p = 00001 )  . 
in multivariable analysis , age had an e ect in all three cancer models : participants aged 6069 years were signi cantly more likely to opt for investigation than were those aged 4059 years , and those aged 70 years or older were less likely . 
other variables associated with increased likelihood of opting for investigation were shorter travel times to testing centre ( colorectal and lung cancers ) , a family history of cancer ( colorectal and lung cancers ) , and higher household income ( colorectal and pancreatic cancers )  . interpretation participants in our sample expressed a clear preference for diagnostic testing at all risk levels , and individuals want to be tested at risk levels well below those stipulated by uk guidelines . 
the public engagement with our study should encourage general practitioners to involve patients in referral decision making . funding the national institute for health research programme grants for applied research programme . introduction more than one in three people in the uk will develop cancer during their lifetime.1 although cancer mortality in the uk has improved in the past 15 years , 2 it is still worse than the average across europe.3 several initiatives have been introduced in the uk to address this issue , such as the cancer reform strategy and the national awareness and early diagnosis initiative.4 earlier diagnosis is thought to be one of the main ways to improve survival , mainly by improved selection of patients for further investigation.5 almost 90% of patients with cancer are diagnosed after experiencing symptoms , most of whom present to primary - care facilities.6 selection of patients for further is not straightforward : overinvestigation has clinical and nancial costs , and underinvestigation risks a delay in diagnosis and therefore has clinical and medicolegal costs . 
however , other groups have a legitimate interest in this decision : providers of cancer investigation diagnostic services , govern ments , taxpayers , insurers , andmost import antlypatients . most common symptoms of cancer can also represent benign disease . 
when deciding whether to investigate for possible cancer , general practitioners use their experience and national guidelines , especially the uk national institute for health and care excellence ( nice ) guidance that was issued in 2005.7 this guidance also underpins the provision of 2 - week - wait clinics , in which patients are guaranteed to be seen within 2 weeks . 
by implication , when investigation is recommended by the guidance , the likelihood of the patient having cancer is high enough to justify it , although no explicit risk threshold warranting investigation for cancer has been reported in the uk or any other national guidance.8 the percentage of patients referred to 2 - week - wait clinics who are subsequently shown to have cancer varies between cancer sites , geographical areas , and general practitioners.9 however , 232 vol 15 february 2014 articles only a quarter of cancers in the uk are diagnosed in 2 - week - wait clinics , with other patients presenting as emergencies or referred to other specialist services.10 , 11 research in primary care has provided estimates of the risk of cancer for many symptoms , with several symptoms recommended by nice as indicating a high likelihood of cancer : few of the nice recommendations equate to risks of less than 5%.12 , 13 investigation , 16 or nice referral guidance strongly recommends that the patient participate in decisions about testing , 7 although little research has been done into diagnostic preferences of patients . 
previous research has focused on treatment or follow - up options , 14 preferences for screening , 15 predictive the sharing of risk information.17 patients certainly fear cancermore so than they do knife crime , alzheimers disease , and job loss18but how likely they are to choose investigation for cancer when provided with the relevant information about cancer risk , the details of investigation , and possible outcomes is unknown . 
we aimed to establish the likelihood that individuals would choose to be tested for cancer at various levels of risk . methods study design and participants in a vignette - based study , we recruited 26 general practices in three areas of england ( bristol and south gloucestershire , devon , and the east of england ) to include a broad range of urban and rural locations and varying levels of socioeconomic status ( number of practices and speci c practices not prespeci ed )  . 
we compared mean practice size and index of multiple deprivation score with overall means from the national public health observatory , and ethnic origin of patients with 2009 means from the o ce of national statistics . in these general practices , researchers recruited attendees aged at least 40 years in waiting areas at di erent times of the day and week between dec 6 , 2011 , and aug 1 , 2012 . 
we did a testretest exercise in one additional practice , with 48 volunteers ( of a recruitment target of 50 ; same inclusion criteria ) who agreed to return 2 weeks later , to complete identical vignettes to their rst exercise . 
these participants were o ered 10 shopping vouchers . we obtained ethics approval from the south west ( southmead ) national research ethics service committee ( ref 11 / sw / 0055 )  . 
participants provided oral informed consent . procedures we chose to compare colorectal , lung , and pancreatic cancers , because they di er in terms of symptoms , type of test , treatment , and prognosis . 
we developed 12 separate vignettes ( ie , descriptions of hypothetical situations ) , with four for each of the three cancers ( table 1 full shows description of vignettes )  . 
the content of the vignettes symptoms extracts ; appendix shows was informed by nice guidelines , qualitative interviews with patients referred for diagnostic tests for the three cancers , 19 and clinical experience.2022 each vignette contained a description of symptoms , the risk that these symptoms might indicate cancer ( both numerically and pictorially ) , information about the relevant diagnostic test , probable treatment , possible alternative diagnoses , and an indication of the prognosis if cancer were identi ed . 
the vignette culminated in a brief summary of information and asked the respondent whether they would choose diagnostic testing at that point , or would not want to be tested ( the exact wording being yesi would choose to be tested or noi would not want to be tested now )  . 
after this choice , participants were asked for the main reason for their decision with a list of options that were informed by qualitative interviews , 19 questionnaires previously used in cancer research , 23 and the cognitive interviewing phase . we re ned the vignettes in two rounds of cognitive the verbal probing method24 interviewing using with 18 members of patient groups from three general practices . 
we recorded responses systematically and collated the after redesign , we tested the questionnaire again on ve additional participants followed by 1 week of piloting in which the questionnaire was administered as per protocol in a general practice waiting room to check recruitment method , functionality of equipment , and data recording . participants could complete up to three vignettes , which were delivered on an electronic touchscreen tablet computer . 
the software developed for the survey selected the rst vignette randomly from all 12 possibilities , the second ( eight possibilities ) , and the third from the remaining cancer ( four possibilities )  . 
 table 2 : characteristics of participants statistical analysis we estimated that 80% of participants given a 10% risk vignette would opt for investigation , and 60% of those given 1% risk would do so . 
with a two - sided 5% alpha and 90% power , we estimated that we would need 119 participants in each group , or 1428 overall . in addition to descriptive statistics , we used logistic regression for the main question ( ie , whether or not to be tested ) , with opting for investigation as the outcome variable . 
the explanatory variables were cancer site , risk level ( as a continuous variable ) , age group , sex , ethnic origin , income band , education , employment , previous diagnosis of cancer , cancer diagnosis in a family member or close friend , convenience of hospital , and travel time to hospital . 
in this analysis , we used only the rst completed vignette from each participant because data were available for all participants , thus avoiding possible di erential selection bias for subsequent vignettes . we then developed separate models for each cancer , using all ( rst , second , or third ) responses for that cancer . 
 because participants who completed more than one vignette always had a di erent cancer for the later vignettes , concerns about selection bias in the analysis of each cancer separately were eliminated . 
initially , we entered every possible explanatory variable into univariable analysis to establish the strength of the association between it and opting for investigation , and those with a p value of less than 02 were retained for multivariable analysis . 
the rst multivariable model contained only variables with a univariable p value of less than 005 ; we then added the other variables sequentially , repeating the process until only variables with p values of less than 005 after adjustment for all other variables in the model were present . a supplementary analysis used k - fold cross validation with risk level as the only predictor variable in the base model and four other explanatory variables as additional predictors . 
we also considered the e ect of missing data on the regression models by omitting any variable with more than 5% of missing data and examining the change in results . 
our nal validation check was to use intracluster correlation coe cients to investigate the degree of clustering of the outcome variable across the 26 practices and the six researchers involved in data collection . 
we did the testretest analysis on the rst vignettes and used percentage comparisons for participant characteristics and statistics for the vignette components . role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all data in the study and had nal responsibility for the decision to submit for publication . 234 vol 15 february 2014 articles colorectal cancer lung cancer pancreatic cancer all three cancers ( rst vignette only ) responses responses responses responses choose to be tested 462 ( 81% ) 485 ( 85% ) 496 ( 86% ) 508 ( 89% ) choose to be tested 533 ( 92% ) 531 ( 93% ) 543 ( 92% ) 537 ( 92% ) choose to be tested 525 ( 90% ) 527 ( 91% ) 526 ( 92% ) 529 ( 91% ) choose to be tested 782 ( 87% ) 738 ( 88% ) 764 ( 88% ) 768 ( 89% ) 1951 ( 85% ) 2323 2144 ( 92% ) 2316 2107 ( 91% ) 3469 3052 ( 88% ) 2291 table 3 : number of participants who would choose to be investigated , by cancer and risk level travel time to hospital ( h ) 00004 00032 risk age ( years ) 4059 * 6069 < 05 * 051 yes * household income < 10 000 * 10 00025 000 > 25 000 family member or close friend previously diagnosed with cancer colorectal cancer or ( 95% ci ) 108 ( 103113 ) 129 ( 092182 ) 081 ( 059111 ) 078 ( 059103 ) 039 ( 022068 ) 131 ( 095181 ) 185 ( 126271 ) p value 00001 00347 or = odds ratio . 
1415 individuals declined to participate . the age and sex pro les of our sample ( table 2 ) were similar to that of the consulting population in england.27 however , the proportion of men aged 4059 years in our study population ( 589 [ 17% ] ) was lower than in the overall population of england ( 27% ) and the proportion of women aged 6069 years ( 526 [ 15% ] ) was higher than in the overall population ( 11% ) .28 the proportion of participants aged 70 years or more in our study population ( 28% ; table 2 ) was also higher than in the overall population ( 24% ) .28 the respondents were largely of white british ethnic origin and nearly half were retired ( table 2 )  . 
15% had previously been diagnosed with cancer ( table 2 ) , which is higher than the estimate of 13% for individuals older than 65 years in the uk ( owing to scarce data on this subject , this age group represents the most meaningful comparison available ) .29 for most characteristics , only a small proportion of data was missing ( table 2 )  . overall , 88% of participants opted for investigation in the rst vignette ( table 3 )  . 
the proportion was slightly lower in the lowest risk group and higher in the highest risk group ( table 3 ) , but the di erence was small and could largely be explained by a risk gradient for colorectal cancer ( table 3 )  . 
compared with colorectal cancer , after adjustment for risk , participants were more likely to opt for investigation for lung cancer ( 266 , 95% ci 199356 , p < 00001 ) and pancreatic cancer ( 196 , 148260 , p < 00001 )  . 
however , when the types of cancers were analysed separately , risk did have an e ect on whether investigation was chosen for colorectal cancer ( table 4 )  . age had an e ect in all three cancer models : participants aged 6069 years were more likely to opt for investigation for all three cancers than were those aged 4059 years , and those in the oldest group ( 70 years ) were least likely to opt for investigation ( table 4 )  . 
further investigation into whether attitude to risk was a ected by age showed weak evidence of an e ect overall ( pinteraction = 010 ) , with substantial variation across the di erent cancers . 
other variables associated with increased likelihood of opting for investigation were shorter travel times to testing centre ( colorectal and lung cancers ) , a family member or close friend previously diagnosed with cancer ( colorectal and lung cancers ) , and higher household income ( colorectal and pancreatic cancers ; table 4 )  . identi ed the k - fold cross validation results for all three cancer sites produced nal models including the same variables as those in the original models , with almost identical regression coe cients ( data not shown )  . 
we the variable examined the potential bias of missing data in relation to income by omitting the variable from the two nal models for colorectal and pancreatic cancers in table 4 , with almost identical results for risk level and the other variables ( ie , omission of this variable from the models made no di erence to the models themselves )  . 
we noted negligible intracluster correlation of the preference for investigation by general practice and by researcher who enrolled the individual for all vignettes , and for each cancer site separately ( data not shown )  . the main reasons cited by participants opting for investigation in the rst vignette were peace of mind , early detection , and a family history of cancer , with little variation across the three cancers ( table 6 )  . 
reasons for opting for no investigation varied between the three cancers ( table 6 ) eg , much higher proportions cited an unpleasant test or harmful test for colorectal cancer than for lung and pancreatic cancers . the primary research question of whether the participant chose to undergo diagnostic tests for cancer showed excellent testretest consistency , with a statistic of 0878 ( > 075 is deemed excellent )  . 
participants reasons for their choice produced statistics of 0584 for those who would opt for investigation and 0667 for those who would not opt for investigation , which are both in the fair to good range ( 04075 ) .30 the social and economic status data showed reliable testretest consistency : six of ten questions returned higher than 90% agreement , three were between 80% and 89% , and one ( hospital travel time ) was 69% . discussion to our knowledge , ours is the rst study of public preferences for cancer investigation ( panel )  . 
88% of participants would opt for investigation when given a realistic scenario of symptoms that could indicate cancer , along with the risk of cancer these symptoms posed , plus a description of the relevant investigation and likely outcomes . 
 although this risk gradient was identi ed in the analysis incorporating all three cancers , it was primarily driven by the ndings for colorectal cancer , for which participants seemed to make a trade - o between the invasiveness of the colonoscopy and the risk of cancer . 
age also seemed to a ect responses , with the preference for investigation highest in individuals aged 6069 years and lowest in those aged at least 70 years . the willingness for testing shown in our study far exceeds what is actually being o ered by the national health service . 
participants in our study might have simply opted for a free test , an idea which is supported by the fact that the proportion opting for investigation did not vary by risk for lung and pancreatic cancer . 
however , the di erences by risk level for colorectal cancer and by age group suggest that participants considered their responses . the four vignettes for colorectal cancer were all in line with nice guidance for urgent referral ( because of the 6 weeks of diarrhoea ) , although many symptoms with a low risk of cancer ( 15% ) are not included in nice guidance.12 , 13 for lung cancer , a chest radiograph is recommended by nice when a patient has a persistent cough ( de ned as lasting at least 3 weeks )  . 
only in the case of colorectal cancer , with its invasive method of testing , did we record clear evidence of an association between a preference for testing and risk level , but even at the lowest risks , the proportion who would choose testing was more than 80% . 
our study emphasises how the public and patients should be allowed to contribute directly to the continuing redesign of diagnostic pathways into and out of primary care for cancer in the uk . 
no threshold level of risk warranting urgent investigation of cancer has been published , although the concept of a threshold is implicit in all uk guidanceand must be in excess of 1% . 
as well as giving referral guidance , nice guidelines emphasise the value and importance of including the patient in the decision - making process for referral and diagnostic testing for cancer ; e ective communication is a key dimension of an appropriate referral.33 the way that participants engaged with our study , the subtle variations in participant preferences , and the high participant numbers suggest that general practitioners should be able to con dently engage in a dialogue with patients about the meaning of symptoms and the risk of cancer . 
general practitioners can underestimate the degree to which patients want information and to be involved in decision making , 34 and decisions are sometimes made on the basis of a perception of what patients prefer , 35 but our data and experience show that a substantial proportion of the population are willing to think about what symptoms mean , personal risk , and the possibility of cancer . 
much of the debate around their use centres on the degree to which responses can be used as accurate measures of views and behaviour , with the correlation between vignette response and actual behaviour being questioned.36 conversely , several studieseg , peabody and colleagues investigation37have shown that vignette responses are useful indicators of behaviour and compare favourably with other methods of assessments of preferences and intentions . 
the method has been widely used in the investigation of medical choice and judgment , such as by jiwa and colleagues.38 many participants in our study had not experienced referral for cancer testing and the vignettes provided a way to elicit preferences in the absence of direct experience . any questionnaire survey is only useful if the questions are realistic and the responses considered . 
we tried to ensure the vignettes were as realistic as possible and to make the percentage risk understandable by presenting it numerically and pictorially ( see appendix for example ) , on the basis of suggestions from our two rounds of cognitive interviewing . 
we cannot know whether the overall high proportion of participants who would opt for investigation was driven by the symptom burden ( which worsened with high risk levels ) or by the risk level itself , or by a combination , although the last of these interpretations seems to be closest to clinical reality . 
we were realistic in our description of the three rst - line investigations ( colonoscopy , chest radiograph , and ct scanning ) , including their requirements and possible hazards ( largely relevant to colonoscopy with its need for bowel preparation and the small risk of perforation )  . 
 since our study began , the ndings of the siggar study39 have suggested that ct colonography could be as accurate as colonoscopy ; a higher proportion of participants in our study might have opted for investigation had this test been available . 
we made it clear that early diagnosis might not reduce the chance of death from lung and pancreatic cancers , emphasising that most patients would die of their disease , although prompt diagnosis could allow bene t from palliative care . 
we would also point to the reasons given for responses , which suggested that participants responded re ectively ; the subtle variations around the type of test , risk , and the age of respondents showed an engagement with the di ering components of the vignette . that ours was a large study , in which participants were recruited from urban , rural , wealthy , and deprived locations . 
although our target population was the general uk population susceptible to cancer ( adults aged 40 years ) , we made a pragmatic decision to recruit from waiting areas of general practices as opposed to other community settings . 
the proportion with a past history of cancer in our sample ( 15% ) is similar to the estimated proportion in the uk population of individuals older than 65 years ( 13% )  . 
 the small number of non - white individuals in our study means that the e ect of any ethnic variation is beyond the scope of this study . nice recommendations and national health service provision seem to di er greatly from preferences of patients in terms of cancer diagnostic pathways . 
if more patients can be drawn into a full dialogue about preference , risk , and decision making with their general practitioner , a more e ective referral pathway from primary care could be created . contributors all authors contributed to study design , study conduct , and study management . 
his contribution to this article is in a personal capacity , and should not be interpreted as representing the view of the guideline development group , or of nice itself . 
the other authors declare that they have no con icts of interest . acknowledgments this report presents independent research funded by the national institute for health research programme grants for applied research programme ( rp - pg - 0608 - 10045 )  . 
the views expressed are those of the authors and not necessarily those of the national health service , the national institute for health research , or the department of health . 
we thank the discovery programme steering committee ( roger jones [ chair ] , clare bankhead , alison clutterbuck , jon emery , ardiana gjini , joanne hartland , maire justice , jenny knowles , helen morris , richard neal , peter rose , greg rubin ) ; catherine stabb and the east of england primary care research network , who recruited participants outside of bristol ; helen morris who coordinated researcher training and project documentation in the east of england ; katie mills and nicky hall who collected qualitative data that informed vignette development ; and bristol software partners who developed the software for the application used to collect data . corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 comment published online december 19 , 2013 s1470 - 2045 ( 13 ) 70584 - 9 see articles page 201 copyright colleoni et al . 
if the patient had preoperative chemoradiotherapy , irrespective of response , we are as uncertain as other oncologists about what to recommend . geerard l beets , bengt l glimelius department of surgery , maastricht university medical center , po box 5800 , 6202az maastricht , netherlands ( glb ) ; and department of radiology , oncology and radiation science , uppsala university , uppsala , sweden ( blg ) g.beets@mumc.nl we declare that we have no con icts of interest . engelen sm , maas m , lahaye mj , et al . 
eurecca colorectal : multidisciplinary management : european consensus conference colon and rectueur j cancer 2014 ; 50 : 1 ; e1e34 . bosset j - f , calais g , mineur l , et al , for the eortc radiation oncology group . 
ann oncol 2013 ; 24 ( suppl 4 ) : iv18 . neoadjuvant chemotherapy for breast cancer : any progress ? neoadjuvant chemotherapy is a well established approach to treatment of locally advanced breast cancer . 
preoperative therapy allows breast - conserving surgery in many patients and provides prognostic information that could guide the choice of treatments to maximise the degree of response ( ie , towards pathological complete remission [ pcr ] ) .1 at present , about 20% of patients achieve pcr after an appropriate neoadjuvant chemotherapy regimen , including a taxane and an anthracycline , and an antiher2 drug for her2 - positive disease.2 improved pcr is reported in subgroups of patients ( eg , patients with triple - negative and her2 - positive disease ) and in the presence of targeted therapies.3 is a suitable scenario the next step is to improve these results . 
the strategy was highlighted recently by regulatory agencies that might grant accelerated approval of new drugs on the basis of an endpoint such as pcr , which is reasonably likely to predict survival bene t.4 in the neo - tango study , 5 helena earl and colleagues addressed the value of addition of gemcitabine to paclitaxel , and the sequencing of epirubicin and cyclophosphamide and paclitaxel ( with or without gemcitabine ) blocks . 
the investigators concluded that no advantage was provided in terms of pcr rate by addition of gemcitabine : 70 ( 17% ) of 404 patients given epirubicin and cyclophosphamide then paclitaxel had pcr compared with 71 ( 17% ) of 408 patients ( p = 098 )  . 
 who conversely , improved pcr was seen with taxanerst sequencing for neoadjuvant chemotherapy : 82 ( 20% ) of 406 patients given paclitaxel with or without gemcitabine followed by epirubicin and cyclophosphamide achieved pcr compared with 59 ( 15% ) of 406 patients who received epirubicin and cyclophosphamide rst ( p = 003 )  . received additional gemcitabine the absence of a signi cant e ect for addition of gemcitabine is not surprising and is in line with results already reported in large phase 3 randomised studies in the neoadjuvant setting.6 these results however con rm the value of neoadjuvant trials for anticipation vol 15 february 2014 comment of results of large adjuvant trials , which yielded much the same outcomes.7 the improved pcr reported in neo - tango5 with the taxanerst sequence did not translate into improved disease - free survival and overall survival . 
 the overall low pcr ( 17% ) was possibly related to the heterogeneous population , which included patients with in ammatory breast cancer . interpretation of e cacy of neoadjuvant treatments might be improved by a selective focus on speci c subtypes of breast cancer . 
the neo - tango study , 5 as is the case with most studies done in the neoadjuvant setting in the past few years , took no account of potential heterogeneity of tumour biology , which has been widely studied since such studies began.2 the magnitude of the therapeutic e ect on pcr in patients with favourable and unfavourable prognosis might di er according to the intrinsic breast cancer subtype . 
von minckwitz and colleagues3 explored , according to selected subtypes , the value of pcr in 6377 patients with primary breast cancer who received neoadjuvant chemotherapy with an anthracycline and a taxane in seven randomised trials . 
they concluded that pcr is a good surrogate endpoint for patients with triple negative , luminal b ( her2 - negative ) , and non - luminal ( her2 - positive ) disease , but not for patients with luminal a and luminal b / her2 - positive disease . pcr according to subtypes should be taken into consideration when results of earl and colleagues trial are interpreted . 
although results were adjusted for her2 and oestrogen receptor status , information on the taxanerst sequence was restricted in some subgroups ( eg , her2 - positive disease )  . 
the regimen used in the study cannot be regarded as a present standard for patients with her2 - positive disease , because no targeted anti - her2 agent was used . 
pcr rates obtained in breast or nodes did not di er between two regimens in the analysis of anthracyclines followed by taxane plus trastuzumab compared with taxanes plus trastuzumab followed by anthracyclines plus trastuzumab . overall , a taxanerst sequence can be regarded as a reasonable option in neoadjuvant chemotherapy for locally advanced breast cancer . 
the results of earl and colleagues study5 reinforce available evidence on the e cacy of this sequence.9 in future trials , breast cancer should be regarded as a homogeneous disease until new evidence supports a di erent approach . 
 this strategy will be key for progress to be made in the treatment of individual patients with locally advanced breast cancer . * marco colleoni , aron goldhirsch international breast cancer study group and division of medical senology ( mc ) and international breast cancer study group and breast health program ( ag ) , european institute of oncology , via ripamonti 435 , 20141 , milan , italy marco.colleoni@ieo.it we declare that we have no con icts of interest . 
 neoadjuvant sequential epirubicin , cyclophosphamide , and paclitaxel , with or without gemcitabine , for women with high - risk early breast cancer ( neo - tango ) : an open - label , factorial , randomised phase 3 trial . 
tango : a randomised phase iii trial of gemcitabine ( gem ) in paclitaxel - containing , epirubicin / cyclophosphamide - based , adjuvant chemotherapy ( ct ) for women with early stage breast cancer ( ebc )  . 
fluorouracil , epirubicin , and cyclophosphamide ( fec - 75 ) followed by paclitaxel plus trastuzumab versus paclitaxel plus trastuzumab followed by fec - 75 plus trastuzumab as neoadjuvant treatment for patients with her2 - positive breast cancer ( z1041 ) : a randomised , controlled , phase 3 trial . 
the poor survival must be partly a result of presentation with ambiguous symptoms , which means that many patients need three or more primary - care consultations before the diagnosis is reached , as shown by data from england for 200910 , 2 when the principles of the nhs cancer plan were well established . 
analysis of previous eurocare data3 , 4 showed that the poor survival in the uk and ireland when compared with other european countries is most explained by a high number of deaths in the rst year after diagnosis . 
the reliance on primary - care gatekeeping to control access to diagnostic services in primary care in the uk and ireland is probably highly important ; other countries allow patients to have direct access to specialists . 
 denmark also has poorer survival than do norway , sweden , and finland , which is associated with a similar reliance on primary care.1 against this background , it is disconcerting that a strategy of several consultations and their associated delays has been proposed as a viable option to control and protect expensive secondary care resources from excessive demand.5 in the lancet oncology , jonathan banks and colleagues6 present results of a study in which they explored potential patients acceptance of diagnostic investigation in response to vignettes describing patterns of symptoms that carry a risk of a neoplasms of as little as 1% or 2% . 
the vignettes and the ascribed risks of cancer were derived from careful observational studies in uk primary care and are a re ection of the reality of early symptomatic diagnosis of cancer.7 investigation of a clinical presentation with a 2% risk of an underlying cancer needs 50 patients to be assessed for every patient for whom the diagnosis is made . 
publicity encourages people who have the sort of ambiguous symptoms that can indicate common cancers to seek the advice of a pharmacist whose bias must be towards sales of medicine . 
additionally , individuals who do seek an appointment with a general practitioner are increasingly asked to have a telephone discussion with a member of the practice to ascertain if a personal consultation is justi ed.8 in the uks national health service , diagnosis and treatment have no direct costs to patients . 
banks and colleagues showed that higher household income was associated with an increased likelihood of opting for investigation for colorectal and pancreatic cancers.6 a family history of cancer was also associated with an increased likelihood of opting for investigation for colorectal and lung cancers . 
distance from the investigating facility could be an inhibitory factor.6 similar considerations most probably apply to the decision to make the rst contact with a family doctor or to initiate a further contact after initial reassurance . 
the application of this rule has been explored in child protection : the urgent needs of the child being neglected or abused are not recognised by health and education agencies.10 the same pattern could exist in the diagnosis of new or indeed recurrent cancer ; general practitioners would 136 vol 15 february 2014 comment prefer their patients not to have cancer and are therefore reluctant to give the possibility priority . 
if such thinking derives from a preference not to burden the patient with investigation for the small probability that a malignancy exists , the clear message from banks and colleagues is that patients would prefer to have diagnostic testing . 
 s michael crawford airedale general hospital , steeton , keighley bd20 6td , uk michael.crawford@anhst.nhs.uk i declare that i have no con icts of interest . de angelis r , sant m , coleman mp , et al . 
cancer survival in england and the in uence of early diagnosis : what can we learn from recent eurocare results ? br j cancer 2009 ; 101 ( suppl 2 ) : 10209 . 4 mller h , linklater km , robinson d . 
case - reviews - 2009 - 2010 ( accessed jan 8 , 2014 )  . vol 15 february 2014 corrections published online december 21 , 2016 s1470 - 2045 ( 16 ) 30686 - 6 correction to lancet oncol 2017 ; 18 : 205 , 206 , 208 , ( d ) low jg , berglund a , schell mj , scott et al . 
in gure 1 , the footnote should have read pie charts show dose assignments for patients in gard score groups : ( b ) high ( 8941100 percentile ) ; ( c ) middle ( 3041894 percentile ) ; and ( 0304 percentile )  . 
in the second paragraph of the results , the third sentence should have read however , although 1456 ( 58% ) of 2517 patients assigned to 45 gy were in the low gard group , 1023 ( 21% ) of 4877 patients in the middle gard group and 38 ( 4% ) of 887 patients in the high gard group were assigned to 45 gy ( gure 1 )  . 
the fth sentence in this paragraph should have read similarly , although most patients assigned to 70 gy were in the high gard group , 588 ( 11% ) of 4877 patients in the middle gard group were assigned to 70 gy ( gure 1 )  . 
in the fth paragraph of the discussion , the start of the eighth sentence should have read : finally , while we use the gene - expressionbased a backbone for our analyses , the calculation of gard could use other measures of radiosensitivity or be expanded to include other biological parameters including hypoxia , dna repair , proliferation , and the immune systethese corrections were made to the online version as of dec 21 , 2016 , and printed article is correct . radiosensitivity index vol 18 february 2017 articles accelerated versus standard epirubicin followed by cyclophosphamide , methotrexate , and fluorouracil or capecitabine as adjuvant therapy for breast cancer in the randomised uk tact2 trial ( cruk / 05 / 19 ) : a multicentre , phase 3 , open - label , randomised , controlled trial david cameron , james p morden , peter canney , galina velikova , robert coleman , john bartlett , rajiv agrawal , jane banerji , gianfilippo bertelli , david bloomfield , a murray brunt , helena earl , paul ellis , claire gaunt , alexa gillman , nicholas hearfield , robert laing , nicholas murray , niki couper , robert c stein , mark verrill , andrew wardley , peter barrett - lee , judith m bliss , on behalf of the tact2 investigators summary background adjuvant chemotherapy for early breast cancer has improved outcomes but causes toxicity . 
the uk tact2 trial used a 2 2 factorial design to test two hypotheses : whether use of accelerated epirubicin would improve time to tumour recurrence ( ttr ) ; and whether use of oral capecitabine instead of cyclophosphamide would be non - inferior in terms of patients outcomes and would improve toxicity , quality of life , or both . methods in this multicentre , phase 3 , randomised , controlled trial , we enrolled patients aged 18 years or older from 129 uk centres who had histologically confirmed node - positive or high - risk node - negative operable breast cancer , had undergone complete excision , and were due to receive adjuvant chemotherapy . 
patients were randomly assigned to receive four cycles of 100 mg / m epirubicin either every 3 weeks ( standard epirubicin ) or every 2 weeks with 6 mg pegfilgrastim on day 2 of each cycle ( accelerated epirubicin ) , followed by four 4 - week cycles of either classic cyclophosphamide , methotrexate , and fluorouracil ( cmf ; 600 mg / m cyclophosphamide intravenously on days 1 and 8 or 100 mg / m orally on days 114 ; 40 mg / m methotrexate intravenously on days 1 and 8 ; and 600 mg / m fluorouracil intravenously on days 1 and 8 of each cycle ) or four 3 - week cycles of 2500 mg / m capecitabine ( 1250 mg / m given twice daily on days 114 of each cycle )  . 
the randomisation schedule was computer generated in random permuted blocks , stratified by centre , number of nodes involved ( none vs one to three vs four or more ) , age ( 50 years vs > 50 years ) , and planned endocrine treatment ( yes vs no )  . 
the primary endpoint was ttr , defined as time from randomisation to first invasive relapse or breast cancer death , with intention - to - treat analysis of standard versus accelerated epirubicin and per - protocol analysis of cmf versus capecitabine . 
at a median followup of 856 months ( iqr 806959 ) no significant difference was seen in the proportions of patients free from ttr events between the accelerated and standard epirubicin groups ( overall hazard ratio [ hr ] 094 , 95% ci 081109 ; stratified p = 042 )  . 
at 5 years , 859% ( 95% ci 843873 ) of patients receiving standard epirubicin and 871% ( 856884 ) of those receiving accelerated epirubicin were free from ttr events . 
4358 patients were included in the per - protocol analysis , and no difference was seen in the proportions of patients free from ttr events between the cmf and capecitabine groups ( hr 098 , 95% ci 0851.14 ; stratified p = 000092 for non - inferiority )  . 
compared with baseline , significantly more patients taking cmf than those taking capecitabine had clinically relevant worsening of quality of life at end of treatment ( 255 [ 58% ] of 441 vs 235 [ 50% ] of 475 ; p = 0011 ) and at 12 months ( 114 [ 34% ] of 334 vs 89 [ 22% ] of 401 ; p < 0001 at 12 months ) and had worse quality of life over time ( p < 00001 )  . 
the most common grade 3 or higher adverse events in cycles 14 were neutropenia ( 175 [ 16% ] ) and fatigue ( 56 [ 5% ] ) of the 1070 patients treated with standard epirubicin , and fatigue ( 63 [ 6% ] ) and infection ( 34 [ 3% ] ) of the 1045 patients treated with accelerated epirubicin cycles 58 , the most common grade 3 or higher adverse events were neutropenia ( 321 [ 31% ] ) and fatigue ( 109 [ 11% ] ) in the patients treated with cmf , and hand - foot syndrome ( 129 [ 12% ] ) and diarrhoea ( 67 [ 6% ] ) in the 1044 patients treated with capcitabine . interpretation we found no benefit from increasing the dose density of the anthracycline component of chemotherapy . 
 however , capecitabine could be used in place of cmf without significant loss of efficacy and with improved quality of life . funding cancer research uk , amgen , pfizer , and roche . copyright the author ( s )  . 
no optimum regimen had been established and , although the benefits of adding taxanes to the previously established standard anthracycline - based chemotherapy regimens had been shown , the absolute benefit for patients varied . 
this approach was called accelerated chemotherapy , and was becoming the standard of care in parts of the world , but the designs of the trials on which use was based did not make it clear whether the benefits were due to the accelerated regimen alone . 
 toxicity of adjuvant chemotherapy was , and remains , an important issue for patients , and in particular for one of the standard uk regimens , epirubicin followed by cyclophosphamide , methotrexate , and fluorouracil ( cmf ) , it was observed in an analysis of two trials that all treatmentrelated deaths occurred while patients were taking cmf . 
we designed tact2 to investigate whether use of accelerated epirubicin chemotherapy would improve time to tumour recurrence and whether using oral capecitabine instead of cmf would be non - inferior for efficacy but superior for toxicity , quality of life , or both . 
 furthermore , detailed analysis of the toxicity and tolerability of accelerated chemotherapy showed that accelerated epirubicin was not associated with fewer hospital admissions than standard epirubicin , as had been hoped , nor with better quality of life from the patients perspective . 
use of capecitabine instead of cmf after epirubicin was not associated with inferior disease outcomes , and was , as hypothesised , associated with a different and generally better tolerated toxicity profile . 
a notable effect was that fewer women receiving capecitabine became permanently menopausal than those taking cmf . implications of all the available evidence several studies have indicated benefits or otherwise with accelerated chemotherapy in early breast cancer , but the regimens and schedules assessed have differed . 
 our observations on the lack of subjective benefit on quality of life with accelerated epirubicin will be important to form part of any discussion between patients and doctors about the possible benefits and risks of using an accelerated chemotherapy regimen . 
furthermore , for premenopausal women concerned about retaining ovarian function , epirubicin followed by capecitabine seemed to reduce the risk of permanent chemotherapy - induced menopause . introduction current outcomes for patients with early breast cancer reflect advances in diagnosis and therapy , including the standardisation of adjuvant systemic therapy.1 chemotherapy is administered to many patients with early breast cancer , and the use of anthracyclines has improved efficacy2 compared with older non - anthracycline regimens . 
 although the addition of taxanes to anthracycline - based regimens has shown modest benefits , the growing recognition of breast cancer as a heterogeneous disease has prompted post - hoc analyses which suggest that benefits with different regimens , with or without taxanes , could be restricted to specific subgroups.35 from the early 2000s , when little advantage to patients was expected from the addition of taxanes , block - sequential epirubicin and cyclophosphamide , methotrexate , and fluorouracil ( cmf ) was the anthracycline regimen of choice in many uk hospitals.6 however , in an analysis of two similar trials involving 2391 women who received epirubicin followed by cmf or cmf alone , all 20 treatment - related deaths occurred during treatment with cmf ( six among those receiving epirubicin followed by cmf and 14 among those receiving cmf alone ) .6 a less toxic but equally effective alternative to cmf was , therefore , needed . 
the oral chemotherapy agent capecitabine was equally efficacious to , and less toxic than , cmf in the metastatic setting , 7 which made it an obvious choice for testing as adjuvant therapy in the tact2 trial as a substitution for cmf after an anthracycline . further improvements in chemotherapy efficacy were sought by shortening the interval between cycles from the standard 21 days , a concept that was termed accelerated chemotherapy . 
the calgb 9741 trial3 showed a significant advantage with doxorubicin and cyclophosphamide 930 vol 18 july 2017 articles followed by paclitaxel every 2 weeks compared with the standard of every 3 weeks . 
a clear advantage has also been reported for paclitaxel given once per week.3 , 8 , 9 the relative contributions of the accelerated anthracycline regimen versus the use of paclitaxel to the advantage , however , were unclear . we designed the tact2 trial to investigate two questions using standard epirubicin followed by cmf : whether efficacy could be improved without increasing toxicity when the pure anthracycline chemotherapy component was accelerated ; and whether capecitabine instead of cmf would improve tolerability without loss of efficacy . 
we used a pragmatic 2 2 factorial study design , which allowed tact2 to run throughout the national institute for health research ( nihr ) - funded national cancer research network in england and affiliated research networks supported by the departments of health in other parts of the uk permitting recruitment of breast cancer patients from both teaching and district general hospitals across the uk . methods study design and patients tact2 is a multicentre , phase 3 , randomised , controlled trial with a 2 2 factorial design testing two hypotheses : first that accelerated epirubicin regimen will be superior in terms of time to tumour recurrence ; and , second , that substituting cmf with the oral prodrug capecitabine will not worsen patients outcomes and will offer advantages in terms of toxicity , quality of life , or both ( appendix pp 4299 )  . 
eligible patients were women or men aged 18 years or older with histologically confirmed invasive primary breast carcinoma ( t03 , n02 , m0 ) 10 who had undergone complete excision and were due to receive adjuvant chemotherapy . 
exclusion criteria ( appendix p 10 ) included malignant disease in the previous 10 years , except ductal carcinoma in situ , basalcell carcinoma , and cervical carcinoma in situ , locally advanced or distant disease , surgical margins involved at any tumour site in the final operative resection , and severe cardiac or renal disorders . the study was approved by the scotland multi - research ethics committee ( mrec 04 / mre00 / 88 ) and local research and development offices . 
the clinical trials and statistics unit at the institute of cancer ( icr - ctsu ) , had overall research , london , uk responsibility for trial coordination with three collaborating clinical trials units ( cancer clinical trials unit , scotland , edinburgh , uk ; leeds clinical trials research unit , leeds , uk ; and cancer research uk clinical trials unit , birmingham , uk ) that were responsible for randomisation independent data monitoring and data management of patients within their geographical regions . 
icr - ctsu did all central statistical monitoring and the interim and final analyses . randomisation and masking the randomisation schedule was generated by computer at icr - ctsu in permuted blocks with sizes of eight and 12 . 
patients were assigned in a 1 : 1 : 1 : 1 ratio to receive standard epirubicin followed by cmf , accelerated epirubicin followed by cmf , standard epirubicin followed by capecitabine , or accelerated epirubicin followed by capecitabine . 
 patients were stratified by centre , number of nodes involved ( none vs one to three vs four or more ) , age ( 50 years vs > 50 years ) , and planned endocrine treatment ( yes vs no )  . 
tact2 was open label because the different treatment schedules made a double - blind design impractical . procedures patients assigned to the standard epirubicin group received four treatment cycles with 100 mg / m epirubicin delivered every 3 weeks , and those assigned to the accelerated epirubicin group received four cycles with 100 mg / m epirubicin delivered every 2 weeks plus 6 mg pegfilgrastim given on day 2 of each cycle . 
patients subsequently received four 4 - week cycles of cmf ( 600 mg / m cyclophosphamide intravenously on days 1 and 8 or 100 mg / m orally on days 114 ; 40 mg / m methotrexate intravenously on days 1 and 8 ; and 600 mg / m fluorouracil intravenously on days 1 and 8 of each cycle ) or four 3 - week cycles of 2500 mg / m capecitabine per day ( 1250 mg / m given twice daily on days 114 of each cycle )  . clinical , haematological , and biochemical assessments were done before the start of each cycle . 
the protocol stressed the need to maintain the interval between cycles , such that during standard epirubicin and cmf chemotherapy , any delay of longer than 7 days required a 20% dose reduction to minimise the risk of further dose delays ( appendix pp 45 )  . after chemotherapy , standard radiotherapy , endocrine therapy , and 1 year of trastuzumab treatment were given according to local and national guidelines , and patients were permitted to enter further selected trials of adjuvant therapy provided these did not compromise the aims of tact2 ( appendix p 6 )  . see online for appendix vol 18 july 2017 articles patients were followed up at 12 , 18 , and 24 months and then yearly for at least 10 years after randomisation , according to local practice for patients in trials of early breast cancer . 
imaging of the breasts ( eg , by mammography or mri ) was done every 1 or 2 years for at least 10 years , in accordance with local practice . 
 patients in selected centres participated in a quality - oflife and toxicity substudy , for which data were obtained via questionnaires completed by patients and by collection of detailed information by clinicians . 
due to logistical issues , collection of quality - of - life data was temporarily suspended part way through the trial and , therefore , lower numbers of patients are available for this analysis than that for acute toxicity . 
we used the european organisation for research and treatment of cancer ( eortc ) qlq - c30 - br23 , 11 , 12 hospital anxiety and depression scale ( hads ) , wu cancer fatigue scale , fatigue symptoms inventory ( fsi ) , and the eq5d , and included tact2 - treatment - specific questions on toxicities during the treatment period ( appendix pp 3233 )  . 
adverse events were assessed by clinicians after each chemotherapy cycle and graded with the national cancer institute common toxicity criteria for adverse events ( version 3.0 ) and coded by use of the medical dictionary for regulatory activities ( version 10 ) , with central clinical review done by dc , pc , and pb - l when needed . 
data on use of national health service ( nhs ) resources , including hospital admissions , were collected after each chemotherapy cycle and at each clinical follow - up visit for up to 5 years after treatment . 
data on ovarian function in women who were premenopausal at the start of chemotherapy were collected 18 months after randomisation . outcomes the primary endpoint was time to tumour recurrence ( ttr ) , defined as the time from randomisation to first invasive relapse or breast cancer death . 
patients who remained free from ttr events , including those who died from other causes in the absence of breast cancer relapse , were censored at their date of last follow - up or death . 
the primary analysis of standard versus accelerated epirubicin was by intention to treat and the analysis of cmf versus capecitabine was per protocol . statistical analysis we assumed the 5 - year proportion of patients free from ttr events would be 80% after standard epirubicin followed by cmf . 
to test whether accelerated epirubicin was superior to standard epirubicin , we calculated that 3876 patients would be needed to detect a 4% absolute improvement from 80% to 84% ( hazard ratio [ hr ] 078 ) with 5% two - sided significance and 90% power . 
to test the second hypothesis that capecitabine would be noninferior to cmf , we calculated that 4400 patients would be needed to provide 80% probability that the lower 90% ci for the difference between the regimens would exclude 3% if the groups were truly equivalent . 
therefore , a target accrual of 4400 patients was chosen , giving approximately 92% power for the comparison of standard versus accelerated epirubicin ( appendix p 7 )  . for survival - related endpoints , we plotted kaplan - meier curves and compared treatment groups with the log - rank test . 
the non - inferiority analysis and additional sensitivity analyses of the primary endpoint were done per protocol ( ie , including all patients who received at least one cycle of allocated treatment )  . 
we did further analyses in a priori defined subgroups : companion randomisation regimen , oestrogen - receptor status , her2 status , nodal status , age , tumour grade , tumour size , and vascular invasion . 
we also did exploratory subgroup analyses by menopausal status and molecular subtype ( local oestrogen - receptor , progesterone - receptor , and her2 status )  . for the standard epirubicin versus accelerated epirubicin comparison , we calculated the actual fraction of the intended dose density for epirubicin , defined as the observed dose density divided by the protocol planned dose density for standard epirubicin , with the mean expected to be 15 times higher than that in patients who received standard epirubicfor cmf and capecitabine , 932 vol 18 july 2017 articles we calculated relative dose intensities ( separately for each drug ) , defined as the observed dose intensity divided by protocol planned dose intensity . 
for both comparisons , for each chemotherapy cycle not received a relative dose intensity of zero was assumed . reported 12 months or the acute safety analysis population included all patients in the quality - of - life and toxicity substudy who received at least one cycle of allocated chemotherapy . 
 longitudinally across all in addition to randomised treatment , generalised estimating equations models included baseline score , time follow - up questionnaire completion , component of quality - of - life study ( before or after suspension ) , and age at randomisation . 
proportions of patients reporting each score were compared across treatment groups with a trend test . from baseline timepoint , analyses presented here are based on a database frozen on aug 25 , 2015 . 
 results between dec 16 , 2005 , to dec 5 , 2008 , 4391 patients from 129 hospitals were enrolled , with 2221 patients allocated to receive standard epirubicin ( 1116 followed by cmf and 1105 followed by capecitabine ) and 2170 to receive accelerated epirubicin ( 1086 followed by cmf and 1084 followed by capecitabine ; figure 1 )  . 
of 4391 patients , 2711 ( 62% ) were postmenopausal women and 20 ( < 1% ) were men , 2337 ( 53% ) were node positive , 2520 ( 57% ) had grade 3 disease , 3196 ( 73% ) had oestrogen - receptor - positive and / or progesterone - receptor - positive tumours , and 831 ( 19% ) had her2 - positive tumours based on local assessments . 3735 ( 85% ) of 4391 patients received all eight cycles of allocated treatment , with proportions being similar in the standard and accelerated epirubicin groups ( appendix pp 89 , figure 1 )  . 
the mean actual fraction of the intended dose density for standard epirubicin over the first four cycles of treatment was 995% ( iqr 9501000 ) and for accelerated epirubicin was 1494% ( 14191503 ) , giving a ratio between treatment groups of 151 ( 95% ci 149152 , appendix p 10 )  . 
the median relative dose intensity across treatment cycles five for cyclophosphamide , 966% ( 824999 ) for methotrexate , 962% for fluorouracil , and 942% ( 759994 ) for capecitabine . 
use of other adjuvant therapies was similar across the two epirubicin groups ( appendix pp 1112 )  . to eight was 947% ( iqr 804997 ) ( 829997 ) median follow - up in patients was 856 months ( iqr 806959 ) , with 3193 ( 85% ) of 3748 known to be alive without withdrawing consent followed up within the previous 15 - month period . 
ttr events were reported in 724 ( 17% ) of 4391 patients in the intention - totreat population and in 716 ( 16% ) of 4358 in the perprotocol population ( table 2 )  . 
there was no significant difference in ttr between the two epirubicin groups ( 377 [ 17% ] of 2221 patients in the standard epirubicin group had ttr events , compared with 347 [ 16% ] of 2170 patients in the accelerated epirubicin group , overall hr 094 , 95% ci 081109 , stratified log - rank test p = 042 ; figure 2 )  . 
there was also no significant difference in ttr between the cmf and capecitabine groups ( 362 [ 17% ] of 2178 patients in the cmf group had ttr events compared with 354 [ 16% ] of 2180 patients in the capecitabine alone group , overall hr 098 , upper 9578% ci limit 112 ; 95% ci 085114 , p = 000092 for non - inferiority and stratified log - rank test p = 081 for superiority of capecitabine compared with cmf ; figure 2 )  . 
tumour grade not known for six patients ( two in the standard epirubicin followed by capecitabine group , one in the accelerated epirubicin followed by cmf group , and three in the accelerated epirubicin followed by capecitabine group )  . 
excludes 25 patients with her2 status borderline or unknown ( five in the standard epirubicin followed by cmf group , five in the standard epirubicin followed by capecitabine group , six in the accelerated epirubicin followed by cmf group , and nine in the accelerated epirubicin followed by capecitabine group )  . 
||includes 58 patients with oestrogen - receptor and her2 - negative tumours but unknown progesterone - receptor status ( 14 in the standard epirubicin followed by cmf group , 13 in the standard epirubicin followed by capecitabine group , 14 in the in the accelerated epirubicin followed by cmf group , and 17 in the accelerated epirubicin followed by capecitabine group )  . 
includes six deaths from other causes after distant disease recurrence : infective endocarditis ( n = 1 in the standard epirubicin followed by cmf group ) , metabolic acidosis and sepsis from bronchopneumonia ( n = 1 in the standard epirubicin followed by cmf group ) , pancreatic cancer ( n = 1 standard epirubicin followed by capecitabine group and n = 1 in the accelerated epirubicin followed by cmf group ) , a fall ( n = 1 in the accelerated epirubicin followed by capecitabine group ) , and ovarian cancer ( n = 1 in the accelerated epirubicin followed by capecitabine group )  . 
includes one death of unknown cause in the standard epirubicin followed by cmf group . table 2 : events contributing to analyses of time to tumour recurrence and numbers of distant relapses , second cancers , and deaths the cmf group versus 912% ( 900923 ) in the capecitabine group . 
the proportions of patients free from ttr events at 5 years were 859% ( 95% ci 843873 ) for the standard epirubicin group versus 871% ( 856884 ) for the accelerated epirubicin group , and 865% ( 850879 ) for the cmf group versus 867% ( 852881 ) for the capecitabine group . 
when the hr for ttr events was adjusted for factors known to affect prognosis ( age , vascular invasion , oestrogen - receptor status , her2 status , nodal status , tumour grade , and tumour size ) the value for accelerated epirubicin compared with standard epirubicin was 095 ( 95% ci 082110 ; p = 048 )  . 
after adjustment for randomisation stratification factors and allocation to either standard or accelerated epirubicin , the hr for capecitabine compared with cmf was 101 ( 95% ci 087117 , p = 088 )  . 
no evidence of heterogeneity in treatment effect was seen by previous treatment with standard or accelerated epirubicin or clinical subgroups ( figure 3 )  . 601 ( 14% ) patients died ( table 2 ; figure 2 )  . 
nine deaths were reported to be due to infection related to chemotherapy ( cmf n = 8 , capecitabine n = 1 ) , but none of these occurred during epirubicin treatment . 
results for other secondary clinical outcome endpoints , such as invasive - disease - free survival and time to distant tumour recurrence , were consistent with those presented for ttr ( data not shown )  . 
overall survival at 3 years was 955% ( 95% ci 945962 ) in the standard epirubicin groups versus 944% ( 934953 ) in the accelerated epirubicin groups , and 952% ( 943961 ) in the cmf groups versus 947% ( 936955 ) in the capecitabine groups . 
at 5 years , overall survival was 907% ( 95% ci 894918 ) in the standard epirubicin groups versus 897% ( 883909 ) in the accelerated epirubicin groups , and 902% ( 889914 ) in the cmf groups versus 901% ( 888913 ) in the capecitabine groups . of the 1399 premenopausal women with data available on ovarian function , disruption or discontinuation of periods during chemotherapy was significantly higher with accelerated epirubicin than standard epirubicin ( 558 [ 83% ] of 672 vs 556 [ 76% ] of 728 ; p = 00020 ) and with cmf than capecitabine ( 593 [ 86% ] of 687 vs 520 [ 73% ] of 712 ; p < 00001 )  . 
ttr = time to tumour recurrence . ( standard epirubicin 345 [ 49% ] of 710 and accelerated epirubicin 305 [ 47% ] of 651 ; p = 052 )  . 
between the cmf and capecitabine groups , however , the proportions of patients with permanently discontinued periods at 18 months remained significantly different ( cmf 499 [ 75% ] of 667 and capecitabine 294 [ 42% ] of 695 ; absolute difference in proportions 325% , 95% ci 275374 , p < 00001 ) , as did those for patients receiving adjuvant ovarian suppression ( 67 [ 10% ] of 687 and 133 [ 19% ] of 713 ; 89% , 53125 , p < 00001 )  . the quality - of - life and included 2121 patients , 2115 ( 997% ) of whom received at least one cycle of allocated chemotherapy ( table 3 , appendix pp 1319 )  . 
 the proportion of completed quality - of - life questionnaires toxicity substudy received at 12 months from those who consented to particpate in the quality - of - life substudy was 172 ( 53% ) of 326 patients in the standard epirubicin and cmf group , 181 ( 58% ) of 314 in the accelerated epirubicin and cmf group , 206 ( 65% ) of 319 in the standard epirubicin and capecitabine group , and 208 ( 65% ) of 322 in the accelerated epirubicin and capecitabine group . 
during cycles one to four of chemotherapy , the numbers of adverse events of grade 3 or worse were lower in the accelerated epirubicin group for leucopenia , neutropenia , febrile neutropenia ( table 3 )  . 
the number of hospital admissions for neutropenic sepsis during chemotherapy cycles one to four was higher among patients receiving standard epirubicin than among those receiving accelerated epirubicin ( appendix p 20 )  . the toxicity and quality - of - life substudy patients , 2074 ( 98% ) of 2121 patients received at least one cycle of allocated cmf or capecitabine chemo therapy ( table 4 , appendix pp 2127 )  . 
during cycles five to eight of chemotherapy , the proportion of patients who had grade 3 or worse adverse events was significantly greater nausea , mucositis / stomatitis , thrombosis / embolism , infection , anaemia , leucopenia , neutropenia , thrombo cytopenia , and febrile neutropenia than in the capecitabine group , whereas grade 3 or worse handfoot syndrome was more prevalent in the capecitabine group . the end of epirubicin treatment , accelerated epirubicin was associated with significantly worse selfreported tingling , numb , or sore hands and feet ( consistent with clinician - reported acute adverse events ) than standard epirubic by contrast , patients receiving standard epirubicin reported more weight gain ( appendix pp 3440 )  . 
these differences did not persist over time ( at 12 months , 724762 vs 736 , 717755 ; at 24 months , 743 , 723762 vs 769 , 750788 , figure 4 )  . 
her2 - negative phenotype includes patients with borderline her2 results and without fluorescence in situ hybridisation ( n = 10 ) and patients with no her2 results ( n = 15 in luminal and triple negative subgroups )  . 
her2 - negative phenotype group includes patients with borderline her2 results and without fluorescence in situ hybridisation ( n = 10 ) and patients with no her2 result ( n = 15 in luminal and triple negative subgroups )  . 
events are shown that meet at least one one of the following criteria : difference in proportion of patients reporting an event of any grade is > 1% between the epirubicin groups ; the proportion of patients experiencing an event of any grade is > 10% in either the standard epirubicin or the accelerated epirubicin group ; and the difference between epirubicin groups in the proportion of patients experiencing an event of any grade is significant ( p < 001 )  . 
events are shown that meet at least one of the following criteria : difference in proportion of patients reporting an event of any grade is > 1% between the cmf and capecitabine groups ; the proportion of patients experiencing an event of any grade is > 10% in either the cmf or capecitabine group ; and the difference between the cmf and capecitabine groups in the proportion of patients experiencing an event of any grade is significant ( p < 001 )  . 
free - text preferred terms of medical dictionary for regulatory activities version 10 are used . table 4 : adverse events during cycles five to eight of chemotherapy among patients in the quality - of - life and toxicity substudy 940 vol 18 july 2017 articles and dry , flaky , or sensitive skin and tingling , numb , or sore hands and feet were worse in the capecitabine group ( appendix pp 3440 )  . 
patients receiving cmf had significantly worse pain in muscles , bones , and joints at 12 months and worse tiredness at 24 months than those in the capecitabine group ( appendix pp 3440 )  . 
longitudinal analysis with generalised estimating equations models confirmed that patients receiving cmf had a significantly worse quality of life over time ( p < 00001 , appendix p 41 )  . 
no significant interaction was found between the previous epirubicin regimen and cmf or capecitabine treatment ( appendix p 41 )  . the proportions of patients with grade 3 or worse late adverse events 12 months or later after randomisation did not differ significantly between the standard and accelerated epirubicin groups , irrespective of whether or not events were prespecified ( table 5 , appendix pp 2829 )  . 
 likewise , we found no significant differences in the proportion of patients who had late grade 3 or worse adverse events between the cmf and capecitabine groups ( table 6 , appendix pp 3031 )  . 
p value from ancova analysis of e versus ae and for cmf versus x , adjusted for baseline subscale score . discussion in the tact2 trial , despite achieving the intended 50% increase in epirubicin dose density , our findings did not support the hypothesis that this would lead to significant improvements in breast cancer outcomes . 
the two treatment groups were well balanced for standard clinicopathological factors likely to influence outcomes , and we found no evidence of heterogeneity of effect by breast cancer subtype or nodal status . 
by contrast , our results support the second hypothesis , that capecitabine can be safely substituted for cmf , when given after singleagent epirubicin , without loss of efficacy and with improvements in toxicity profile and overall quality of life . 
 randomly assigned for diarrhoea , which is a known side - effect of capecitabine , patients self - reported severity did not differ significantly between the cmf and capecitabine treatment groups . patients in all groups had 5 - year overall survival of around 90% with no unexpected adverse events . 
fatal adverse events were rare and occurred at similar frequencies in all groups , although numerically more deaths due to infection were seen among patients receiving cmf and more vascular deaths were seen among patients receiving capecitabine . 
thus , although even with an improved toxicity profile , use of capecitabine did not prevent all treatment - related deaths . the results of our analysis of accelerated versus standard epirubicin might seem to be at odds with those from other studies . 
however , a meta - analysis of 3418 patients in four trials that included the calgb 9741 study showed an vol 18 july 2017 articles standard epirubicin ( n = 2193 ) accelerated epirubicin ( n = 2155 ) p value for trend * p value for events grade 3 grade 12 grade 3 grade 4 grade 12 grade 3 grade 4 events prespecified on case - report form other adverse events fatigue 773 ( 35% ) 26 ( 1% ) 3 ( < 05% ) 764 ( 36% ) 15 ( 1% ) 2 ( < 05% ) 063 010 anxiety arthralgia hot flush 25 ( 1% ) 229 ( 10% ) 250 ( 11% ) 1 ( < 05% ) 11 ( 1% ) 12 ( 1% ) 1 ( < 05% ) 7 ( < 05% ) 234 ( 11% ) 212 ( 10% ) 1 ( < 05% ) 8 ( < 05% ) 6 ( < 05% ) 1 ( < 05% ) 00029 081 0066 > 099 050 036 analysis of late safety compared all signs and symptoms reported at or after 12 months from randomisation and included all patients who were randomly assigned treatment , followed up for at least 9 months , and received at least one cycle of allocated chemotherapy . 
events are shown that meet at least one of the following criteria : difference in proportion of patients reporting an event is > 1% between epirubicin groups ; the proportion of patients experiencing the event is > 10% in either group ; the difference between epirubicin groups in the proportion experiencing an event is significant ( p < 001 )  . 
free - text preferred terms of medical dictionary for regulatory activities version 10 are used . table 5 : late adverse events by epirubicin regimen cmf ( n = 2176 ) capecitabine ( n = 2172 ) p value for trend * p value for events grade 3 grade 12 grade 3 grade 4 grade 12 grade 3 grade 4 fatigue 781 ( 36% ) 21 ( 1% ) 2 ( < 05% ) 758 ( 35% ) 20 ( 1% ) 3 ( < 05 ) 014 handfoot syndrome 89 ( 4% ) 1 ( < 05% ) 208 ( 10% ) 3 ( < 05% ) < 00001 events prespecified on case - report form other adverse events arthralgia hot flush joint stiffness nail disorder onychoclasis 263 ( 12% ) 253 ( 12% ) 50 ( 2% ) 24 ( 1% ) 7 ( < 05% ) 13 ( 1% ) 7 ( < 05% ) 200 ( 9% ) 6 ( < 05% ) 1 ( < 05% ) 00010 209 ( 10% ) 11 ( < 05% ) 1 ( < 1% ) 28 ( 1% ) 72 ( 3% ) 21 ( 1% ) 0066 0016 < 00001 00079 > 099 037 026 026 analysis of late safety compared all signs and symptoms reported at or after 12 months from randomisation and included all patients randomly assigned treatment , followed up for at least 9 months , and received at least one cycle of allocated chemotherapy . 
events are shown that meet at least one of the following criteria : difference in proportion of patients reporting event is > 1% between cmf and capecitabine groups ; the proportion of patients experiencing an event of any grade is > 10% in either the cmf or capecitabine group ; and the difference between the cmf and capecitabine groups in the proportion experiencing an event is significant ( p < 001 )  . 
free - text preferred terms of medical dictionary for regulatory activities version 10 are used . table 6 : late adverse events by cmf or capecitabine group therapy , but overall significant benefit in terms of survival free from invasive disease for accelerated chemotherapy ( hr 085 , 95% ci 073095 ) , 14 an estimate consistent with the data reported in tact2 , which assessed a larger population than these four trials combined . 
the calgb 9840 study has further shown inferiority of paclitaxel given every 3 weeks compared with when given once per week.16 in both of these studies , however , how much of the reported benefits were due to the altered paclitaxel schedule and how much to the accelerated administration of the anthracycline and in contrast to tact2 , cyclophosphamide - based components remains unclear . 
 the tact2 data indicate that acceleration of only the anthracycline component alone provides little benefit to patients . the tact2 population differs from the populations in other trials in several ways . 
the benefits seen in the calgb 9741 and gim2 studies , therefore , might have been driven by the inclusion of higher - risk populations , and particularly patients with extensive nodal involvement . 
this possibility is supported by data from the ago - etc trial , 17 in which the hr at 5 years for a dose - dense schedule was 064 among patients with ten or more involved nodes , compared with 942 vol 18 july 2017 articles 079 for patients with four to nine involved nodes , although the difference was not significant . 
however , despite what other studies have suggested , we saw no benefit from dose - dense chemotherapy in patients with more than ten involved nodes ( hr 082 , 95% ci 051131 )  . 
this difference between findings highlights the need for a meta - analysis of individual patients data to determine whether or not traditional prognostic factors , such as extent of nodal involvement , identify subgroups of patients who will gain increased benefit from accelerated chemotherapy ( table 7 )  . in tact2 , patients with her2 - positive tumours had access to routine treatment with trastuzumab upon completion of their chemotherapy , which was given to 761 ( 92% ) of 831 atients with known her2 - positive disease . 
of the other studies , gim2 was the only one to be done in the trastuzumab era , but only 130 ( 27% ) of 480 patients with her2 - positive disease received this drug , which constituted 6% of the overall trial population ( compared with 17% in our study ) , and in this small group no benefit was associated with accelerated chemotherapy.15 this difference alone , however , cannot explain from accelerated chemotherapy in tact2 . the absence of benefit we had anticipated that epirubicin given every 2 weeks in our accelerated regimen would be associated with reduced risk of toxicity because of the use of primary prophylactic granulocyte - colony - stimulating factor . 
apart from the expected significant reduction in neutropenia and febrile neutropenia , patients in the accelerated epirubicin group had more adverse events , particularly low - grade events , than those in the standard epirubicin group . 
the overall quality of life was worse during accelerated epirubicin treatment than during standard epirubicin treatment , although this difference did not persist after this treatment ended . and capecitabine although other studies have tested the efficacy of additional capecitabine in early breast cancer ( finxx18 , gbg geparquattro19 , create - x20 ) , only one other study of which we are aware , the calgb 49907 study , 21 has compared cmf adjuvant chemotherapy for breast cancer , and that trial showed inferior outcomes for patients assigned capecitabine . 
 older women at increased risk of recurrence were assigned to receive standard chemotherapy ( a choice of four cycles of cyclophosphamide and doxorubicin or six cycles of cmf ) or single - agent capecitabine at a reduced dose of 2000 mg / m per day . 
the study was stopped early due to inferiority of capecitabine when just over 600 patients had been enrolled , of whom less than half of the standard chemotherapy group had opted for cmf . 
an updated analysis suggested that the difference in efficacy between the two groups had reduced , and might only be significant in tact2 gim215 * ago etc17 node negative 13 nodes > 3 nodes 100 ( 078128 ) 087 ( 069109 ) 097 ( 072130 ) 088 ( 067111 ) 068 ( 054086 ) 072 ( 059087 ) data are hazard ratios ( 95% ci ) for the primary endpoint ( recurrence ) by nodal subgroups . 
 table 7 : risk of disease recurrence by nodal status in trials of dose - dense chemotherapy patients with hormone - receptor - negative tumours.22 in the tact2 trial , we used capecitabine after anthracycline chemotherapy , which might explain further the difference between our results and those in the calgb 49997 study . we conducted the acute substudy in only a large subset of patients since both regimens were well characterised clinically and the number needed to assess patientreported outcomes and adverse events was not as large as that required for assessing the efficacy endpoint . 
 defining whether a toxicity profile is better for one treatment than another from the patients perspective is not as straightforward as assessing relative efficacy with one disease - based endpoint , such as ttr . 
patients , nurses , and doctors might classify the relevance of toxicity differently , and the inclusion of patient - reported adverse events is recommended to supplement clinician reporting.2325 from a medical perspective , of the 12 adverse events for which the frequency of grade 3 or 4 events differed significantly between the cmf and capecitabine groups only two were more frequent with capecitabine ( table 4 )  . 
the differences are what would be expected from these therapies , with fatigue , nausea / vomiting , gastrointestinal and bone marrow events , and thromboembolism all being more frequent in patients receiving cmf , whereas only diarrhoea and handfoot syndrome were more frequent in patients receiving capecitabine . 
 how to synthesise from a patients perspective a shift in toxicity profile between two similarly effective regimens is a conundrufor some patients , although toxicities were numerically fewer with capecitabine , experiencing grade 34 diarrhoea while taking this drug might be less acceptable than , for example , experiencing grade 34 nausea , fatigue , and asymptomatic neutropenia while taking cmf . quality - of - life scales are designed to measure overall burden on patients , globally and within various subdomains . 
our hypothesis that capecitabine would have better tolerability than cmf is confirmed by the main quality - of - life outcome , which showed worse selfreported global quality of life at the end of cmf treatment than at the end of capecitabine treatment , and this difference persisted at 12 and 24 months . 
although the vol 18 july 2017 articles numbers of patients who completed quality - of - life questionnaires differed between groups , additional analyses suggested that at 12 months these differences were not associated with physician - reported adverse events at the same timepoint ( data not shown )  . an important difference in the toxicity profiles of capecitabine and cmf was the recovery of menstrual function in women who were premenopausal at enrolment . 
evidence suggests that recovery of function could have resulted in a slightly less active endocrine regimen , 26 but our findings do not allow us to draw conclusions on the relation between this and diseaserelated outcome . 
importantly , recovery of menstrual function might be of benefit to younger women , given the increasing age at which many are starting families , with increasing numbers of women with early breast cancer requiring chemotherapy but also wishing to preserve their fertility . 
although we do not know the numbers of women in this study who maintained fertility , the increased frequency of return of menses among those receiving capecitabine seems to offer this as an option to try and preserve ovarian function . 
this regimen , along with fluorouracil , epirubicin , and cyclophosphamide chemotherapy , was compared in the tact trial4 with an anthracycline and taxane regimen , against which there was no evidence of inferiority . 
for the adjuvant treatment of early breast cancer , in patients in whom taxanes are not indicated or contraindicated , treatment with epirubicin followed by capecitabine in 3 - week cycles is an effective , safe , and well tolerated option . the dose density of increasing that contributors dc , pc , gv , jbar , amb , he , pe , rcs , aw , pb - l , and jmb were involved in the study design . 
pc , gv , ra , gb , amb , he , cg , ag , nm , mv , and aw reviewed the drafts , pe was involved in manuscript development , and dc gave final approval of the paper . declaration of interests dc has received funding from amgen , pfizer , and roche . 
we thank cancer research uk for funding the study , amgen , pfizer , and roche , for unrestricted educational grants , and the national institute for health research cancer research networks in england and their equivalent nhs r&d - funded networks in scotland , wales , and northern ireland for in - kind support . 
finally , we thank the members of the independent data monitoring committee and the clinical trials and statistics unit at the institute of cancer research overarching trials steering committee , and the two co - sponsoring organisations , the institute of cancer research and nhs lothian . 
the pharmaceutical company partners had the opportunity to review the manuscript to ensure any proprietary information was correct . comment published online april 16 , 2014 s1470 - 2045 ( 14 ) 70177 - 9 see articles page 620 time will show whether the results reported by zhu and colleagues2 can be achieved in other centres and whether this technique will become an accepted palliative treatment option . 
regional di erences in infrastructure , expertise , and health - care economics will continue to be essential factors as clinicians tailor appropriate therapy for patients with advanced oesophageal cancer . russell e white tenwek hospital , box 39 , bomet , 20400 , kenya russ.white@wgm.org i declare that i have no competing interests . 
health economic evaluation of stent or endoluminal brachytherapy as a palliative strategy in patients with incurable cancer of the oesophagus or gastro - oesophageal junction : results of a randomized clinical trial . 
eur j gastroenterol hepatol 2005 ; 17 : 136977 . setting the bar for adjuvant treatment of melanoma there is universal agreement about the need to improve adjuvant treatment for patients who have melanoma and are at high risk of disease recurrence after surgery.1 , 2 medical management of metastatic melanoma has improved greatly , with the approval of four new drugs that have shown clear survival bene ts phase 3 randomised trials , beginning with the approvals of ipilimumab and vemurafenib in 2011 . 
the american society of clinical oncology has published guidance that aims to improve the standard of clinical trials in metastatic breast , colon , lung , and pancreatic cancers by setting where a higher bar for treatment expectations.3 should the bar then be set for clinical trials of adjuvant treatment in patients with melanoma ? how do the results of the avast - m trial , 4 which assessed the role of bevacizumab as adjuvant treatment for patients with stage iii melanoma at high risk of recurrence , help inform our deliberations ? the availability of new drugs with clear e ects on metastatic melanoma provides a strong rationale for their investigation in adjuvant trials . 
 avast - m began before the approval of ipilimumab and vemurafenib , but even today there is little evidence from trials in metastatic disease to suggest that adjuvant bevacizumab would be bene cial in patients with melanoma . 
 moreover , adjuvant use of bevacizumab has not improved survival in patients with any other tumour type to date.6 dosage is also an important consideration : the avast - m investigators studied bevacizumab given at a dose of 75 mg / kg whereas other studies have assessed bevacizumab given at a dose of 1015 mg / kg , which could have a ected the results . 
future adjuvant trials in patients with melanoma need a strong rationale and design , but whether known e cacy of the agent in in metastatic melanoma is an absolute requirement for successful adjuvant therapy remains to be de ned . the choice of overall survival as the primary endpoint of the avast - m study was clearly an appropriate one , with no signi cant di erence noted between patients in the bevacizumab group and those in the observation group ( hazard ratio [ hr ] 097 , 95% ci 078122 ; p = 076 )  . 
the suitability of relapse - free survival as the primary endpoint in melanoma adjuvant trials bears further scrutiny : does having drugs that improve overall survival in patients with stage iv melanoma negate the value of relapse - free survival in the adjuvant setting , or might rapidly evolving and improving treatment vol 15 may 2014 comment importance of strategies actually accentuate the delaying recurrence ? when relapse - free survival is used as a primary or key secondary endpoint , the investigational agent should be compared with the standard already set by interferon . 
previous studies7 , 8 of adjuvant interferon have shown improvements in relapse - free survival in the range of 1338% , and results for relapse - free survival from the ipilimumab adjuvant trials ( clinicaltrials.gov , numbers nct00636168 and nct01274338 ) are eagerly awaited . 
 in the avast - m trial , disease - free interval was in the bevacizumab group in patients improved compared with those in the observation group ( hr 083 , 95% ci 070098 ; p = 003 )  . 
disease - free interval is subtly di erent from relapse - free survival because deaths due to non - melanoma causes are not included in its calculation ; as such , relapse - free survival should remain the standard relapse endpoint for trials of adjuvant melanoma . 
even if we assume that relapsefree survival was improved by the same amount as disease - free interval in the avast - m trial , and that this improvement was statistically signi cant , bevacizumab does not surpass the e ectiveness of interferon su ciently enough to justify its use in clinical practice . in the preplanned interim analysis of avast - m , patients in the bevacizumab group with braf mutant melanoma had a longer disease - free interval than did those in the observation group , whereas no di erence was noted between groups for patients with braf wild - type melanoma . 
enthusiasm for this observation should be tempered by the nding that the test for interaction between treatment and braf status was not signi cant ( p = 010 ) .4 furthermore , a phase 2 study of bevacizumab plus temozolomide chemotherapy in patients with metastatic melanoma showed the opposite resultbetter survival for braf wild - type melanoma.9 either way , the rationale for improved outcomes for patients given bevacizumab in mutationde ned subsets is not well elucidated , and would need further study in prospective trials prior to acceptance as established fact . 
 interferon is the only approved adjuvant treatment for resected melanoma , with several studies showing improvement in relapse - free survival7 , 8 and meta - analyses showing small improvements in overall survival , 2 thus setting the bar for future adjuvant trials . 
adjuvant bevacizumab has not yet improved overall survival , and although disease - free interval is statistically improved in the avast - m trial , its bene ts seem to be , at best , similar to the relapse - free - survival bene t of interferon . 
other variables should also be considered , such as patient selection and toxic e ects ( of note , only 361 [ 54% ] of 652 patients completed the planned treatment , with unacceptable toxic e ects nearly as common as disease recurrence as a reason for discontinuation ) , and balanced with the observed e cacy . 
adjuvant interferon in melanoma : is duration of therapy important ? j clin oncol 2014 ; 32 : 17173 . 2 mocellin s , lens mb , pasquali s , et al . 
adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomized controlled phase 3 study . 
ann oncol 2011 ; 23 : 53136 . 548 vol 15 may 2014 in view of the poor outcome of patients with highrisk , localised soft - tissue sarcomas , how can these data be incorporated and built upon ? this trial suggests that patients with high - risk extremity and trunk sarcomas could be considered for neoadjuvant anthracycline and ifosfamide , accounting for patient age , performance status , and comorbidities . 
these data should not be a justification for the routine use of adjuvant or neoadjuvant chemotherapy in other histological subtypes not included in this trial . with many sarcoma centres routinely administering neoadjuvant radiation , the optimum preoperative treatment sequence for localised soft - tissue sarcomas remains to be defined because this trial was not designed to answer this question . 
the provisional thoughtful interpretation because of the initial onesided testing , short follow - up , limited number of events , and relatively young patient age ( median 489 years )  . 
rlj is a consultant for pharmamar , lilly , merck , eisai , diachii , immundesign , adaptimmune , blueprint , and deciphera . gronchi a , ferrari s , quagliuolo v , et al . 
histotype - tailored neoadjuvant chemotherapy versus standard chemotherapy in patients with high - risk soft - tissue sarcomas ( isg - sts 1001 ) : an international , open - label , randomised , controlled , phase 3 , multicentre trial . 
evaluation of response after neoadjuvant treatment in soft tissue sarcomas ; the european organization for research and treatment of cancer - soft tissue and bone sarcoma group ( eortc - stbsg ) recommendations for pathological examination and reporting . 
a further shift towards recommended vol 18 june 2017 published online april 27 , 2017 s1470 - 2045 ( 17 ) 30305 - 4 see articles page 823 comment intensive surveillance was adopted in the 2008 usmstf guidelines , which recommended a 510 year interval for low - risk patients.1 guidelines were also developed by other organisations and in other countries . 
european union ( eu ) and uk guidelines are consistent with the us guidelines with one exception.4 the low - risk and highrisk groups are classified as low - risk and intermediaterisk and a third group is defined : a high - risk group of patients with five or more adenomas . 
 with knowledge of the slow growth of the adenomatous polyp before it develops into colorectal cancer , guidelines have evolved to take a more conservative approach to surveillance , with increasingly longer intervals between examinations . 
the goal of surveillance is to reduce the risk of colorectal cancer and mortality in the group of patients at increased risk while minimising procedure risk , cost , and burden on medical resources . 
 in the lancet oncology , atkin and colleagues5 report a retrospective analysis of a large multicentre cohort in which 11 944 patients with adenomas study , deemed to be of intermediate risk according to the uk classification ( us high - risk group ) were followed up for a median of 79 years ( iqr 56111 )  . 
a subset of these patients had an incidence of colorectal cancer that was significantly less than that of the general uk population not undergoing surveillance ( standardised incidence ratio 051 , 95% ci 029084 )  . 
 the study by atkin and colleagues is excellent , but has the limitations of a retrospective study , including the absences of bowel preparation reporting in line with current standardised criteria , central review of baseline pathology , information about the training , rate of the expertise , and adenoma detection endoscopists , criteria for a complete colonoscopy , and pathology of the proximal polyps . 
prospective studies can address many of these limitations and can further examine the question of whether some patients really need surveillance and whether further lengthening of intervals can be recommended in others . 
for example , in the eu and uk guidelines , can the lower - risk subgroup defined by atkin and colleagues within the intermediaterisk group be relegated to receiving no surveillance , as they suggest ? how can this approach be put into practice with clear terminology so that clinicians can easily separate out a lower - risk subgroup from this intermediate - risk group ? should the lower - risk subgroup be included in the original low - risk group ? in the us guidelines , the recommendations for lowrisk patients are for exams every 510 years . 
could this recommendation be more definitively made 10 years ? can a subset of the us low - risk group be relegated to no surveillance ? can the intervals in us high - risk patients be lengthened to 5 years or could this group be further risk stratified ? within this context , much more information is needed on the natural history and follow - up of sessile serrated adenomas and polyps.6 crucial given new studies are being planned to address these that postquestions , which are polypectomy surveillance colonoscopies have become an increasing burden on endoscopy units , patients , the economy , and medical resources.7 available colonoscopy resources might be better used if shifted to initial highquality screening and diagnosis and will continue to be the driving force in the decrease in colorectal cancer incidence and mortality that has been ongoing since 1975.8 this will take on more urgency as worldwide colorectal cancer screening continues to accelerate , as has happened in the eu , the usa , 8 , 9 and elsewhere . 
 * sidney j winawer , ann g zauber gastroenterology and nutrition service , department of medicine ( sjw ) and department of epidemiology and biostatistics ( agz ) , memorial sloan kettering cancer center , new york 10065 - 6007 , ny , usa winawers@mskcc.org we declare no competing interests . 
this publication was mainly funded by the national cancer institute with grants p30 ca008748 , u01ca152959 , r01 ca026852 , r01 ca079572 , and with additional support from the cantor colon cancer fund to sjw and agz . 
annual report to the nation on the status of cancer , 19752006 , featuring colorectal cancer trends and impact of interventions ( risk factors , screening , and treatment ) to reduce future rates . 
cancer 2015 ; 121 : 228185 . improving childhood cancer care in latin america and the caribbean : a paho childhood cancer working group position statement most children with cancer live and die in low - income and middle - income countries ( lmics )  . 
medical and health system advances have brought cure to more than 80% of children with cancer in high - income countries ( hics ) , 1 but such advances have eluded children in most lmics , where inequities can yield cure percentages anywhere from 5% to 60%.2 multiple factors contribute to the inadequate care of childhood cancers in lmics , including resource scarcity , health system fragility , limited provider awareness , and absence of political attention.3 these conditions are abetted by a lack of sustained political attention to childhood cancer at the international level . 
 despite a growing global burden of non - communicable diseases ( ncds ) , calls by global health governance institutions to address ncds have largely failed to address the plight of children with cancer in lmics . 
 a longstanding commitment by childhood cancer professionals and advocates in latin america and the caribbean has contributed to substantial , if variable , progress towards understanding the burden of childhood cancer and improving childhood cancer services in the region.4 past and present lancet oncology commissions have underscored the challenges and opportunities that cancer presents in the context of strengthening health systems in latin america.5 recent work6 suggests opportunities to bring such efforts to scale through a strengthening of the policy and system dimensions of childhood cancer care . 
the union for international cancer control ( uicc ) convened an international policy dialogue on childhood cancer in latin america , identifying integrated elements necessary to improve childhood cancer outcomes in the region . 
these corrections have been made to the online version as of june 2 , 2017 . correction to lancet oncol 2017 ; 18 : 71931 registry international cancer , steliarova - foucher colombet m , ries lag , et al , and the iicc - 3 incidence contributors . 
 lancet oncol 2017 ; 18 : 71931 in this article , the coverage of the population of east asia in table 1 in the age 014 years column should have been 44% , and in the age 1519 years column , 40% . 
 consequently , the fourth sentence in the first paragraph of the results read approximately should have the world population 114% of aged ( contributing years 18 376 710 144 person - years ) was covered by the registries included in our study , ranging from 17% in south asia ( india ) to 994% in north america ( table 1 )  . 
these corrections have been made to the online version as of june 2 , 2017 , and the printed article is correct . 014 correction to lancet oncol 2017 ; 18 : 812 versus gronchi a , ferrari s , quagliuolo v , et al . 
histotype - tailored neoadjuvant chemotherapy standard chemotherapy in patients with high - risk soft - tissue sarcomas ( isg - sts 1001 ) : an international , open - label , randomised , controlled , phase 3 , multicentre trial . 
this correction has been made to the online version as of june 2 , 2017 , and the printed article is correct . correction to lancet oncol 2017 ; 18 : 6374 freyer dr , chen l , krailo md , et al . 
 effects of sodium thiosulfate versus observation on development of cisplatininduced hearing loss in children with cancer ( accl0431 ) : a multicentre , open - label , controlled , randomised , phase 3 trial . 
lancet oncol 2017 ; 18 : 6374in the summary and results of this article , the sentences should regarding adverse events have read the most common grade 34 haematological adverse events reported , irrespective of attribution , were neutropenia ( 117 [ 66% ] of 178 participant cycles in the sodium thiosulfate group vs 145 [ 65% ] of 224 in the control group ) , whereas the most common non - haematological adverse event was hypokalaemia ( 25 [ 17% ] of 149 vs 22 [ 12% ] of 187 )  . 
 in the results , sentences regarding adverse events should have read haematological toxicity was not significantly different between the treatment groups , occurring 137 ( 77% ) of 178 participant cycles in the sodium thiosulfate group and 172 ( 77% ) of 224 participant cycles in the control group ( p = 097 ; table 3 )  . 
aggregate nephrotoxicity was more common in the sodium thiosulfate group , in which 37 ( 25% ) of 149 participant cycles were affected versus 25 ( 13% ) of 187 controls ( p = 00071 ; sentences table 4 ) ; serious adverse events regarding should have read 194 serious adverse events were reported in 26 patients ; of these , 127 were deemed unrelated , 47 unlikely , 20 possibly , and none related to probably or definitely sodium thiosulfate . 
87 were nonhaematological adverse events , of which 45 were deemed unrelated , 28 unlikely , 14 possibly , and none related to probably or definitely sodium sentences thiosulfate ; regarding median follow - up should have read median follow - up was 35 years ( iqr 3045 ) for event - free vol 18 june 2017 e301 corrections corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 editorial published online october 11 , 2013 s1470 - 2045 ( 13 ) 70462 - 5 for more on the us shutdown and the a ordable care act see editorial lancet 2013 ; 382 : 1153 us shutdown : not all services are non - essential on the eve of sept 30 , 2013 , the worlds eyes looked towards the usa with a sense of dj vu . 
would political the grandstanding and bloody - mindedness hold american people to ransom again ? at 10 minutes to midnight , that realisation came to pass : orders were made to shutdown government , and force tens of thousands of federal workers in to an indeterminable length of unpaid leave . 
the shutdown brought with it a number of less foreseen consequences , not least , the inability to start new government - sponsored clinical trials at the national institutes of health ( nih ) clinical center , meaning hundreds of patients are left without treatment . 
ironically , this latest round of political brinkmanship is caused by the lack of acceptance by right - wing republican extremists of a basic human rightthat they undoubtedly enjoy themselvesaccess to a ordable health care . in the aftermath of the shutdown , stories of individual patients due to enroll on to new clinical trials , but now unable to do so , played out across many us newspapers and television stationspatients for whom options are fast running out . 
plus , the food and drug administration , centers for disease control and prevention , and agency for healthcare research and quality are running reduced programmes , and , if the shutdown continues for several weeks , the centers for medicare and medicaid services might be unable to pay health providers . at the heart of this is a titanic battle over the a ordable care act ( aca ) , a statute to over haul healthcare provision in the usa by increasing competition between insurers and extending medicaid to 41 million uninsured americans . 
the republicans have failed 42 times since the legislation was passed in 2010 to either repeal it or strip it of its funding despite the law being upheld by the supreme court in 2012 and being a central issue in the 2012 presidential election , which obama won convincingly . 
 however , this bill ( and all others ) has been blocked by the senate , with obama dismissing a piecemeal approach to budgeting as not a serious or responsible way to run the united states government . luckily for the politicians , their personal circumstances are likely una ected by these events : their in ated salaries being exempt from the shutdown rationing . 
 mean while , for the thousands of unpaid federal workers , how many will be driven in to debt ? equally , while nih sta are on enforced leave , research grant applications go unprocessed , conference attendance suspended , training of graduate students and postdoctoral fellows stopped , and international collaborations adversely a ected . 
and what of the untold damage this will have on future research ? plus , this comes after years of stringent cuts in research funding during the global economic crisis . 
 these actions are not simply causing the temporary closure of non - essential services ; they are much more profound and widely in uential . urgent resolution to the shutdown is needed to prevent long - term damage to peoples lives , clinical research , and the global economy . 
in the longer term , however , the us government needs to assess whether the current model of decision - making is truly democratic , since the american people are being badly let down by their elected representatives . 
 the lancet oncology vol 14 november 2013 1141 access to opioids : a balance of harms opioid overdose killed 64 070 americans between 201617 to become the leading cause of mortality in the usa for people younger than 50 years . 
this recommendation is in stark contrast to this administrations aim of cutting the government health budget , and trump has refused to declare the current situation a national emergency , an action that would increase national impetus to act . 
what is causing this devastating increase in opioid abuse in the usa , and what implications will failure to act have on provision of legitimate opioid access ? opioid analgesics are essential for the relief of in patients with cancer . 
 moderate - to - severe pain in recognition of this fact , morphine , a naturallyoccurring opiate , was added to the who model list of essential medicines in 2015 . 
nonetheless , because of the long and chequered history of the recreational use of opiates , access is still limited worldwide , with approximately 80% of the worlds population estimated to have insufficient access to analgesics for pain relief . 
 a 2016 paper by the international narcotics control board found that the use of opioid analgesics remained low in africa , asia , central and south america , the caribbean , and eastern and southeastern europe . 
when compared with cancer incidence in these areas , there is a clear disparity between the level of need ( especially in regions where cancers are more likely to be diagnosed at advanced stages ) and analgesic provision , with barriers including inadequate medical training medical training , fear of addiction , inadequate financial resources , cultural attitudes towards treatment of pain , fear of criminal prosecution , and onerous regulatory frameworks for prescription of medical narcotics . 
 countries , in high - income the pendulum has arguably swung the other way , with prescriptions for opioid analgesics tripling between 1991 and 2013 in the usa , and doubling between 2000 and 2015 in the uk . 
beginning with recently deceased ted stanleys discovery that fentanyl ( a synthetic opioid analgesic between 50100 times more potent than heroin ) could be combined with sugar to make a palatable , quick - acting analgesic lollipop , synthetic opioids are now readily available in easily ingestible formulations , including delayed - release and oral spray formulations . 
part of the unprecedented increase in prescriptions has been driven through unscrupulous pharmaceutical marketing strategies of these easyto - ingest formulations to physicians ; in 2007 , purdue pharma executives pleaded guilty to criminal charges of misbranding oxycontin ( a timed - release formulation of the opioid oxycodone ) as less addictive and less prone to substance abuse than other formulations . 
although purdue pharma was fined us$634 million , such aggressive product marketing continues , with insys therapeutics currently under investigation for insurance fraud for approval of their oral fentanyl spray subsys . 
in the absence of a care network to address and help with addiction rehabilitation , patients who are addicted are driven to find new sources of opioids , including cheaper , and more readily - available , black market sources of opioids of unknown quality and strength , thus leading to frequent accidental overdose . 
the who access to controlled medications programme defines balance as the dual obligation of a government to enable adequate availability of controlled substances for medical need while simultaneously preventing abuse . 
in the usa at least , multiple steps to address the situation must be taken , including provision of adequate rehabilitation facilities and a legislative end to overprescription and unethical marketing of opioids . 
 the lancet oncology for more on the opioid crisis in the usa see nytimes.com / interactive / 2017 / 09 / 02 / upshot / fentanyl - drugoverdose - deaths.html for more on opioid access worldwide see articles lancet 2016 ; 387 : 164456 for more on the uk opioid use see health - 41201397 for more on the insys therapeutics report see com / 2017 / 09 / 06 / politics / insyscancer - drug - company - fakedcancer - patients - to - sell - drug / index.html ? utm_ content = buffer01f8b&utm_ medium = social&utm_ source = twitter . com&utm_campaign = buffer for more on the balance in opioid provision see publications / 2011 / 9789241564175_eng.pdf vol 18 october 2017 1285 editorial corrections correction to lancet oncol 2013 ; 14 : 199209 correction to lancet oncol 2014 ; 15 : e241 esserman lj , thompson im , reid b , et al . 
the de nition of mrd low risk in the summary should read ( undetectable mrd at the end of induction [ day 29 ] or detectable mrd [ less than 001% ] at day 29 that became undetectable by week 11 )  . 
in gure 2 and in the rst paragraph of the results section , 1732 patients were clinical standard risk , 989 patients were risk , clinical 405 patients were clinical high risk . 
also in gure 2 , 2721 patients were eligible for mrd strati cation , 820 patients had indeterminate mrd status , 808 had high - risk mrd , 1059 had low - risk mrd , 34 patients had died within 35 days or had never remitted , and 323 patients were identi ed after august , 2009 . 
for the mrd low risk patients in table 1 , the total number of patients should read 1059 , of whom 466 were female , 764 were aged 29 years , 978 were b - lineage , 673 ( 64% ) were standard nci risk , 494 ( 47% ) had a white blood cell count less than 10 109 cells per l , and 177 had a white blood cell count of 1019 109 cells per l . 
the last sentence of the sixth paragraph of the results should read additionally , we noted no di erence between patients with undetectable mrd and those with less than 0005% mrd at day 29 . 
 these corrections have been made to the online version of the article as of june 30 , 2014 . vol 15 july 2014 e308 corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 articles lancet oncol 2014 ; 15 : 110918 published online august 20 , 2014 s1470 - 2045 ( 14 ) 70361 - 4 this online publication has been corrected . 
we report the study design , participant sociodemographic and clinical characteristics , and the initial results of the testing and diagnostic phase of the prostate testing for cancer and treatment ( protect ) trial , which aims to investigate the e ectiveness of treatments for localised prostate cancer . methods in this randomised phase 3 trial , men aged 5069 years registered at 337 primary care centres in nine uk cities were invited to attend a specialist nurse appointment for a serum prostate - speci c antigen ( psa ) test . 
consenting participants with clinically localised prostate cancer were randomly assigned to active monitoring ( surveillance strategy ) , radical prostatectomy , or three - dimensional conformal external - beam radiotherapy by a computer - generated allocation syste randomisation was strati ed by site ( minimised for di erences in participant age , psa results , and gleason score )  . 
 the primary endpoint is prostate cancer mortality at a median 10 - year follow - up , ascertained by an independent committee , which will be analysed by intention to treat in 2016 . 
this trial is registered with clinicaltrials.gov , number nct02044172 , and as an international standard randomised controlled trial , number isrctn20141297 . findings between oct 1 , 2001 , and jan 20 , 2009 , 228 966 men were invited to attend an appointment with a specialist nurse . 
2896 men were diagnosed with prostate cancer ( 4% of tested men and 39% of those who had a biopsy ) , of whom 2417 ( 83% ) had clinically localised disease ( mostly t1c , gleason score 6 )  . 
with the addition of 247 pilot study participants recruited between 1999 and 2001 , 2664 men were eligible for the treatment trial and 1643 ( 62% ) agreed to be randomly assigned ( 545 to active monitoring , 545 to radiotherapy , and 553 to radical prostatectomy )  . 
clinical and sociodemographic characteristics of randomly assigned participants were balanced across treatment groups . interpretation the protect trial randomly assigned 1643 men with localised prostate cancer to active monitoring , radiotherapy , or surgery . 
open access article distributed under the terms of cc by . introduction prostate cancer is the most frequently diagnosed cancer in men in developed countries , with an estimated 241 740 new cases and 28 171 deaths caused by the disease every year in the usa alone.1 in the uk , it is the second most common cause of cancer deaths in men ( 13% ) with 41 763 new cases diagnosed and 10 793 deaths caused by the disease in 2011.2 the disease can be detected early by prostate - speci c antigen ( psa ) measurement followed by prostate biopsy . 
however , most screen - detected cancers are at low risk of progression , and potential harm could be caused by unnecessary diagnosis and treatment . the publication of two population - based randomised controlled trials3 , 4 of screening has not resolved this dilemma . 
the european randomized study of screening for prostate cancer ( erspc ) 3 reported a clear but relatively small disease - speci c survival bene t from screening compared with no active intervention at 8 years and 13 years follow - up , with a larger e ect reported in a smaller scandinavian cohort at 14 years after diagnosis.4 by contrast , the us - based prostate , lung , colorectal , and ovarian ( plco ) trial5 reported no bene t from screening with a similar length of follow - up , but was limited by substantial contamination from previous psa testing in the control group in more than 50% of the unscreened men . most men diagnosed with psa - detected prostate cancer tend to undergo radical treatment . 
the us - based prostate cancer intervention versus observation trial ( pivot ) 6 reported no overall mortality bene t from surgery in patients with psa - detected cancer , whereas the scandinavian prostate cancer group 4 trial ( spcg - 4 ) 7 showed a clear diseasespeci c and overall survival bene t for surgery in patients presenting clinically , as well as a reduction in progression to metastatic disease . androgen the prostate testing for cancer and treatment ( protect ) randomised trial was designed to assess the e ectiveness and cost - e ectiveness of active monitoring ( a surveillance protocol ) , external beam conformal radiotherapy with neoadjuvant radical prostatectomy for men with psa - detected clinically localised prostate cancer . 
the recruitment was undertaken in two stages : a feasibility pilot in three english cities ( in 24 primary care centres linked to three university hospitals ) from june , 1999 , to september , 2001 ( isrctn08435261 ) , and the main trial from october , 2001 , to january , 2009 , in nine cities ( seven in england , one in scotland , and one in wales ) .8 also in 2001 , the cap trial ( cluster randomised trial of psa testing for prostate cancer ; isrctn92187251 ) commenced , which is an extension to the protect trial . 
 the cap trial randomly assigned primary care centres to undertake either the protect trial or standard uk national health service ( nhs ) management ( no routine psa testing ; gure 1 ) , to assess population - based screening in addition to treatment e ectiveness of clinically localised disease identi ed in protect.9 further details of the cap trial design and randomisation have been published previously.10 a written invitation was sent by 337 primary care centres assigned to undertake the protect trial to registered men aged 5069 years , excluding those with a previous malignancy ( apart from skin cancer ) , renal transplant or on renal dialysis , major cardiovascular or respiratory comorbidities , bilateral hip replacement , or an estimated life expectancy of less 10 years . 
men who responded received a protect patient information sheet and an appointment with a specialist nurse who explained the complexities of psa testing , assessed trial eligibility , and sought written informed consent . 
participants with a psa concentration of at least 30 g / l were invited to attend secondary care centres within the nine participating cities for a physical and digital rectal examination and standardised transrectalultrasound - guided prostate biopsies . 
participants with an initial psa concentration at least 200 g / l at diagnosis were excluded because of the high likelihood that they had more advanced cancer . ten - core individual received a protect patients were staged using a combination of digital rectal examination , psa concentration , transrectal ultrasound - guided biopsies , and isotope bone scanning ( if psa was 10 g / l )  . 
men with a psa concentration of 10 g / l or higher or a gleason score of greater than 7 points underwent an isotope bone scan to exclude metastatic disease . 
men with a benign rst biopsy sample and a free - to - total psa ratio below 11% , or atypical small acinar proliferation or 1110 vol 15 september 2014 articles for the study protocol see projects / hta / 962099 high - grade prostatic intraepithelial neoplasia , were o ered further biopsies ; if these repeat biopsy samples were benign , these men were managed in primary care and excluded from the trial . 
no further trial follow - up occurred after the one round of psa testing or identi cation of cancers after referral to the nhs . approval was obtained from the uk trent multicentre research ethics committee ( 01 / 4 / 025 )  . 
study training programmes and on - site monitoring visits were used to standardise trial conduct.11 , 12 randomisation and masking men discussed treatment options with the specialist nurses , and if they agreed to the three - group randomisation ( 1 : 1 : 1 ) , the nurse telephoned a central system in the bristol trials o ce ( bristol , uk ) and logged participant details . 
 allocations were computer - generated as required for each participant , originally using microsoft excel functions , and subsequently in c + + , strati ed by site with stochastic minimisation to improve the balance across the groups in relation to age at primary care patient identi cation date , gleason sum score ( < 7 , 7 , or 810 points ) and mean of baseline and rst biopsy psa results ( < 60 , 6099 , or > 99 g / l )  . 
eligible participants were o ered the choice of a two - group randomisation ( radical prostatectomy or radiotherapy ) , or a three - group randomisation ( with the addition of active monitoring to the two treatment groups )  . 
in 2003 , the independent data monitoring committee ( dmc ) terminated the two - group option because of limited uptake , and the only option for participants who consented was three - group randomisation throughout the remaining period of recruitment . 
men who declined randomisation were o ered identical follow - up and formed a comprehensive cohort within the study design . the procedures participant sociodemographic characteristics , family history of cancer , and previous psa tests were obtained at recruitment . 
 imaging of the skeleton was recommended if serum psa reached 10 g / l , using isotope bone scintigraphy , plain radiographs , and mri as necessary . in patients randomly assigned to active monitoring , the protocol aim was to avoid immediate radical treatment while assessing the disease over time , with radical treatment o ered if disease progression was evident . 
the specialist nurses also met with participants yearly to assess their overall health , and discuss graphical displays of psa results and any concerns raised , overseen by each centres local clinical investigator . 
if the psa concentrations were persistently raised , or the patient had any other concerns , a review appointment was made with the centre urologist for discussion of further tests including re - biopsy and all relevant management options . in patients randomly assigned to receive external beam 3d conformal radiotherapy , neoadjuvant androgen suppression was given for 36 months before and concomitantly with 3d - conformal radiotherapy delivered at 74 gy in 37 fractions.13 quality assurance followed the rt01 trial procedures.14 , 15 psa concentrations were measured every 6 months for the rst year and then yearly . 
the study oncologist held a review appointment with participants if the psa concentrations rose by at least 20 g / l post - nadir or concerns were raised about disease progression.16 management options were discussed , including continued monitoring , further tests , salvage , radical , or palliative treatments as indicated . in patients randomly assigned to receive radical prostatectomy , the predominant approach was open retropubic radical prostatectomy with individual - level quality assurance according to minimum standards.17 participants with a baseline psa concen tration of at least 10 g / l or a biopsy gleason score of at least 7 points received bilateral lymph adenectomy . 
the centre urologist held a review appointment their postoperative psa conwith participants centrations reached 02 g / l or higher to discuss adjuvant radiotherapy . linked translational study obtained biological specimens and epidemiological data.9 outcomes outcome measures were selected for relevance to patients and health - care providers . 
the primary outcome was de ned as de nite or probable prostate cancer mortality , including intervention - related deaths , at a median of 10 years follow - up . 
the process used to assess cause of death was adapted from the plco algorithm5 and erspc process3 and then combined to vol 15 september 2014 1111 articles assess deaths in both the cap and protect studies . 
a full list of all prespeci ed outcomes can be found in our study protocol . for statistical analysis before the start of the trial , a sample - size target of 1434 randomly assigned men ( 478 in each group ) was identi ed as su cient to estimate the absolute di erence in mortality probability between two treatment groups with a 95% ci of 0045 , on the basis of an assumed mortality rate of 15% , consistent with prostate cancerspeci c mortality in men aged 5569 years with clinically detected disease managed conservatively at that time and a di erence that would be deemed clinically signi cant by the nhs . 
 however , more recent data10 suggested that diseasespeci c mortality with non - radical treatment was likely to be closer to 10% at 10 years , because of improvements in disease management . 
as a result , the dmc advised in 2008 that recruitment should continue to the planned end date , with 1590 men ( 530 per group ) expected to be randomly allocated by that point . 
this sample size would enable a 46% reduction in prostate cancer mortality to be detected with 80% power at a 5% signi cance level for a pairwise comparison of a radical treatment with active monitoring . 
this calculation assumes a 10% prostate cancer - speci c mortality at 10 years with active monitoring , and hence a 54% risk with radical treatmentan absolute di erence very similar to the margin of error speci ed in the rst calculation . 
these sample size targets are based on di erences in and ratios of risk rather than the hazard ratios planned for the primary analysis , because the resulting calculations are simpler and more exible . 
when a median of 10 years of follow - up has accumulated ( november , 2015 ) , the primary outcome measure of prostate cancer mortality will be compared between ( cox treatment groups using a survival analysis proportional hazards regression model ) adjusted for strati cation and minimisation variables . 
hazard ratios are interpreted in the same way as rate ratios ; the advantage of hazard ratios and coxs proportional hazards model for this study is the accommodation of variation in the underlying rate of prostate cancer mortality during follow - up . 
 pairwise signi cance tests will only be done if a test of an equal 10 - year disease - speci c mortality risk across all three groups yields a p value of less than 005.26 this approach will be used for event - based secondary outcomesie , grouped analyses of de nite , probable , or possible prostate cancer , all - cause mortality , and metastatic disease . pairwise comparisons of symptom burden will use multilevel models for repeated measures to estimate the average treatment e ect over the median 10 - year followup . 
prespeci ed subgroup analyses will investigate whether treatment e ectiveness in the reduction of prostate cancer - speci c mortality is modi ed by baseline clinical stage , gleason grade , age , or psa concentration using strati ed analyses for descriptive statistics and by formally including interaction terms in the relevant regression models . 
secondary analyses will estimate the e cacy of radical treatment versus active monitoring in the reduction of prostate cancer mortality in individuals who complied with their allocated treatment , by using a method to derive an unbiased estimate in parallel with the per - protocol analysis originally speci ed in the trial protocol.27 , 28 an analysis of primary and secondary outcome measures by trial group is reported yearly to the dmc . 
the dmc recommends changes to the trial steering committee if clear evidence ( of the order of p < 0001 ) of a positive or negative balance of risks and bene ts emerges for one intervention in comparison with the others . data from the recruitment , diagnostic , and randomisation phases are presented , and categorisation of continuous variables is either based on clinical thresholds ( eg , for psa ) or the aim of equal group sizes ( other measures )  . 
129 men were 49 years of age when the primary care list was generated , 120 of whom were 50 years old by recruitment ; 25 men were 70 years or older at generation of the primary care list , of whom four were 71 years of age and one was 72 years of age ; at the time of recruitment , all men who were enrolled tted the stated inclusion criteria as per protocol . 
based on resident area - based material and social deprivation scoreseg , percentage of social housing . table 1 : demographic and clinical characteristics according to diagnosis of prostate cancer in patients recruited into the main protect trial 228 966 men aged 5069 years were invited to participate 106 464 did not respond 122 502 responded 100 444 attended appointment 82 429 were recruited 8566 had an eligible psa result 7414 received prostate biopsies 5468 single biopsy 1946 more than one biopsies 18 015 not recruited 7665 ineligible 10 350 declined to participate 73 863 ineligible psa results 73 538 < 30 g / l 279 200 g / l 46 results not given 1152 did not receive biopsy 3504 biopsy negative or mild 4518 biopsy negative or other 756 high grade pin 255 asap atypia 3 inadequate specimen 479 ineligible 270 advanced disease 209 localised but excluded 2896 had a positive biopsy result for prostate cancer 2417 eligible for randomisation ( localised prostate cancer ) figure 2 : flow diagram of the diagnostic phase of the main protect trial results are from one round of psa testing . 
jal , fch , jld , and den had full access to all the data for this analysis ( full outcome data will become accessible to them from nov 15 , 2015 ) and had nal responsibility for the decision to submit for publication . results between oct 1 , 2001 , and jan 20 , 2009 , 228 966 men were invited to participate in the protect study , of whom 122 502 ( 54% ) responded , although 5954 ( 5% ) of respondents declined to participate and 16 104 ( 13% ) did not attend the appointment with the specialist nurse ( gure 2 )  . 
of the men who attended their appointment , 10 350 ( 10% ) did not enrol or return their second consent form and 7665 ( 8% ) were deemed ineligible . 73 538 ( 89% ) of the 82429 recruited participants had a psa concentration that was below the biopsy cuto point . 
date of birth could not be obtained or age was out of eligible range for 130 recruited participants ; age was out of eligible range for two participants invited for biopsy ; two participants who received biopsy ; and one participant who was diagnosed with prostate cancer . 
 table 2 : psa distribution , biopsy , and prostate cancer diagnosis by age and psa concentration in the main protect trial 2664 participants were eligible 2417 recruited in main trial 247 recruited in pilot study 1643 participants were randomly assigned 1497 from main trial 146 from pilot study 1021 were not randomly assigned 997 selected treatment 24 were randomly assigned to two groups 545 allocated to active monitoring 545 allocated to radiotherapy 553 allocated to surgery figure 3 : flow diagram of the randomisation phase of th e protect trial biopsies were o ered to the 2357 ( 32% ) men without a de nitive diagnosis ; 1563 those o ered underwent the repeat procedure , with a further 322 ( 14% ) receiving a repeat biopsy after advice from a urologist . ( 66% ) of 2896 men were diagnosed with prostate cancer ( 4% of those recruited ; 39% of those who had a biopsy )  . 
additionally , of men with a positive biopsy result , 270 ( 9% ) were ineligible for locally advanced , randomisation because they had advanced , or metastatic disease , and 209 ( 7% ) were excluded because of comorbidity . predominantly , recruited protect participants were white and married or living with a partner , and 4082 ( 5% ) reported a family history of prostate cancer ( table 1 )  . 
 median age was 58 years ( range 5069 ) in the total cohort , with slightly more men younger than 60 years recruited than older men ( table 2 ) , and 11 011 ( 13% ) men had received a previous psa test . 
the relation between higher psa concentrations and prostate cancer diagnosis was unchanged by adjustment for age , whereas the relation between the proportion of recruited patients diagnosed with prostate cancer and increased age was attenuated by adjustment for psa concentration ( unadjusted odds ratio [ or ] data not shown ; table 2 )  . 
ethnic origin , married or partnership status , and extent of material deprivation did not di er between participants diagnosed with cancer and those without cancer ( table 1 )  . ( 62% ) of these eligible patients agreed 2417 men recruited to the main protect trial were eligible , as were 247 from the feasibility pilot phase.8 1643 randomisation ( gure 3 )  . 
the median follow - up is currently 86 years ( iqr 71104 ) and we have obtained vital status ( primary outcome ) info for 99% of patients , and secondary outcomes have been measured in 93% . of the 997 men who declined to be randomly assigned and expressed a preference for a particular treatment , 529 ( 53% ) opted for active monitoring , 273 ( 27% ) for radical prostatectomy , 133 ( 13% ) for radiotherapy , 50 ( 5% ) for brachytherapy , and 12 ( 1% ) selected other treatments . 
 1114 vol 15 september 2014 articles these participants had similar clinical and sociodemographic characteristics to those who were randomly assigned ( table 4 ) , except that they were less likely to reside in an area of material deprivation ( or of increased deprivation in randomised versus non - randomised participants of 074 [ 95% ci 058094 ] )  . discussion the protect trial recruited and tested more than 82 000 community - based men aged 5069 years . 
more than 8000 men had a psa concentration of 30 g / l or more , and of those , 87% received a biopsy , resulting in nearly 3000 men diagnosed with prostate cancer ( 4% of those recruited )  . 
in this initial report , median 8 - year follow - up is more than 93% for all endpoints ( 99% for the primary outcome )  . to active monitoring , the ndings the robustness of the including three conventional the the protect trial was designed to address key issues in the management of clinically localised prostate cancer , speci cally the comparative e ectiveness and coste ectiveness of treatment trade - o between early modalities , diagnosis with psa testing and the risks of over - detection and over - treatment . 
trial design features that will enhance include standardised diagnostic , treatment , and follow - up protocols ; internal and external quality assurance processes ; allocation concealment ; high compliance with follow - up ; extensive secondary outcomes ; and an independent , masked primary endpoint committee . 
the recruitment process was based on psa testing , which is known to over - detect prostate cancer , and has the potential to be superseded by newer diagnostic modalities such as pre - biopsy imaging . 
 additionally , the long natural history of the disease means that the study will have taken more than 15 years to report , from rst patient participation in 1999 to the planned analysis of primary outcome after a median 10 - year follow - up in november , 2015 . 
furthermore , during the past decade radical surgery has evolved with the introduction of robot - assisted and laparoscopic techniques , but few of these new approaches were undertaken in this trial . 
other treatments have also changed : brachytherapy , dose escalation , and intensitymodulated radiotherapy are not being assessed in protect , and active surveillance cohorts now tend to focus on men with a gleason score of 6 points and use scheduled prostate biopsieseg , prias ( prostate cancer research international active surveillance ) .29 another limitation is that the lack of ethnic diversity in the study population might limit the applicability of the protect ndings to non - white populations . 
one patient from the feasibility study had a serum psa concentration of 209 g / l at the specialist nurse visit ; the concentration fell to 176 g / l on repeat measurement and he became eligible for recruitment . table 3 : participant and clinical characteristics at randomisation in the protect trial randomised ( n = 1643 ) non - randomised ( n = 997 ) p value 62 ( 4969 ) 62 ( 5069 ) married or living with partner 1375 ( 84% ) living in area of deprivation 239 ( 15% ) family history of prostate cancer 119 ( 7% ) 1606 ( 98% ) 10 ( < 1% ) 37 ( 2% ) 58 ( 30 ) 1266 ( 77% ) 339 ( 21% ) 37 ( 2% ) 1 ( < 1% ) 1249 ( 76% ) 394 ( 24% ) 984 ( 99% ) 2 ( < 1% ) 11 ( 1% ) 841 ( 84% ) 111 ( 11% ) 83 ( 8% ) 58 ( 31 ) 755 ( 76% ) 218 ( 22% ) 24 ( 2% ) 758 ( 76% ) 239 ( 24% ) 060 031 072 0015 028 067 042 096 4954 5559 6064 6569 psa ( g / l ) 3059 6099 100 gleason score 810 missing clinical stage age ( years ) * ethnic origin white other african - caribbean psa ( g / l ) gleason score 810 missing clinical stage data are median ( range ) or number ( % )  . 
 * 24 patients are classi ed as non - randomised because they were part of the early study with randomisation only between radical treatments ( not active monitoring )  . 
based on resident area - based material and social deprivation scores using several indicators of income and living conditionseg , percentage of social housing . table 4 : demographic and clinical characteristics at randomisation according to randomisation status in the protect trial vol 15 september 2014 1115 articles were men with a psa concentration of 20 g / l or higher because they were likely to harbour non - localised cancer and an increased risk of lymph node metastasis , as shown by joniau and colleagues.30 although we acknowledge that recent advances in imaging techniques would have improved staging in these patients , only 279 ( 03% ) of 82 429 participants in our tested cohort had a psa concentration of 20 g / l or higher . additionally , the recruited population could be generally healthier than the overall population , as often occurs in screening trials , but this does not a ect the compara tive e ectiveness analyses of treat ments.3 , 5 furthermore , uk statistics in 2008 suggested that prostate cancer mortality in the active monitoring group would be around 10% after 10 yearslower than expected at the trial outset . 
 therefore the mortality risk di erence of 46% , upon which the original sample size was based , roughly corresponds to a hazard ratio of 054 in the revised calculationa substantial bene t of radical compared with conservative management . 
should results from this trial support early active intervention , evidence will be needed that bene ts are su ciently large to outweigh the well recognised complications of radical treatments . 
 the primary analysis will be highly informative for clinicians , patients , and decision makers because the trial has been designed to consider mortality , resource use , and quality - of - life outcomes . 
and , as with the other treatment trials , the ndings will continue to be of interest as the data mature over time . treatment options the studys limitations need to be balanced against a number of strengths that ensure that the protect trial will be of pivotal importance in establishing the comparative e ectiveness of the three most frequently used in psa - detected clinically localised prostate cancer . 
it is the largest ongoing randomised controlled trial of prostate cancer treatments worldwide , with standardised protocols for diagnosis , treatment , and follow - up and enabling an assessment of screening through the linked cap trial . 
high levels of generalisability are assured by embedding protect within the cap randomised control trial of population - based psa testing involving about 15% of all uk men aged 5069 years recruited from randomly selected primary care centres . 
 participants with intermediate and some high - risk disease features were included and will help to establish whether active monitoring protocols can o er an alternative to immediate radical intervention in these patients . 
the planned subgroup analyses of treatment erspc ( europe ) 3 plco ( usa ) 5 protect ( uk ) pivot ( usa ) 6 spcg - 4 ( sweden ) 7 screening vs control screening vs control am vs rp vs rt 19932001 19992009 rp vs ww 19942002 rp vs ww 198999 199399 30 / 40 68 896 variable 38 350 228 966 100 444 psa tested ( % of attendees ) * 56 064 ( 2991% ) 34 244 ( 89% ) 82 559 ( 82% ) interventions recruitment period psa biopsy threshold ( g / l ) number of biopsy cores men invited men attended raised psa results biopsy uptake diagnosed with prostate cancer randomly assigned to treatment white ethnic origin mean psa , g / l clinical stage * not recorded gleason score * 26 ( erspc 27 ) * * 710 ( erspc 810 ) * * not recorded 27% 101 130 16% 05% 04% 35% 1643 ( 62% ) 5069 ( 61 ) age range , years ( mean age ) 5569 ( 6063 ) 5575 ( 60 ) 731 ( 15% ) < 75 ( 67 ) 695 ( nk ) < 75 ( 65 ) am = active monitoring . 
 * * erspc gleason grades 24 ( 15% ) and 57 ( 76% ) have been combined ; 810 ( 6% )  . table 5 : design , and participant and clinical characteristics , of the principal screening and treatment trials in clinically localised prostate cancer 1116 vol 15 september 2014 articles panel : research in context systematic review a systematic review of the evidence was done before the design of the trial and informed our protocol development . 
 the review was commissioned by the health technology assessment programme of the national institute for health research in the uk.36 the following search terms were used for a text search within the title , abstract , and keywords : prostate cancer and related terms , and therapy ( speci cally radiotherapy and prostatectomy )  . 
the systematic review concluded that there was insu cient evidence to establish the e ectiveness or cost - e ectiveness of screening or treatments for localised prostate cancer because of the shortage of robust randomised evidence at the time . interpretation the protect trial is , to our knowledge , the largest contemporary randomised controlled trial investigating the e ectiveness of conventional treatment options in men with clinically localised prostate cancer detected after psa testing . 
 the protect trial clearly di ers from two previously published treatment trials6 , 7 that compared surgery with watchful waiting ( a passive observational option ) in men with clinically detected disease ( spcg - 4 ) 7 and older veterans administration men with psa - detected disease ( pivot ) .6 in the protect trial , these baseline results show that we successfully recruited men aged 5069 years after community - based psa testing and a high proportion agreed to be randomly assigned between the three major conventional contemporary options ( surveillance , surgery , and radiotherapy ) , and have achieved high levels of follow - up . 
in 2016 , the trial will publish its outcome data . e ectiveness by stage and grade will investigate this aspect and assist comparison with spcg - 4 and pivot treatment trial patients . 
furthermore , the assessment of a radiotherapy and neoadjuvant regimen will be relevant for patients with higher risk disease because good evidence already exists for endocrine therapy combined with radiotherapy for advanced disease.31 protect detected more prostate cancer in the rst round of testing than did the erspc and plco trials , probably because of protects lower psa threshold combined with the minimum ten - core biopsy protocol in a population previously unexposed to routine psa testing . 
the clinical characteristics of the participants cancers in the protect trial are similar to those of other unscreened populations.32 cancer was generally detected at a lower stage and grade in protect participants than in a uk cohort of patients with clinically detected prostate cancer in the early 2000s.33 however , this reduction in stage and grade would have been mitigated by the upward grade migration reported in gleason scoring in nhs practice between 2000 and 2010.34 nevertheless , the mean proportion of uk men whose psa concentration has been tested remains low by international standards at 6% ( range 29 ) in primary care centres in the mid2000s . 
compared with the pivot6 and spcg - 47 treatment trials , protect participants had the lowest psa concentration , age , and included fewer higher stage cancers at the point of randomisation ( table 5 )  . 
 randomisation of eligible participants was higher in protect ( 62% ) than in pivot ( 15% ) , and other similar trials did not complete recruitment ( eg , start , spirit )  . 
 the acceptability of randomisation in the protect trial was enhanced by integrated qualitative research.35 most notably , protect participants received active monitoring , not watchful waiting as in pivot6 and spcg - 4.7 current active surveillance protocols have more restrictive entry criteria and rely more on scheduled re - biopsy than in protect , but protect trial results will provide , to our knowledge , for a monitoring strategy that includes the option of radical treatment ( panel )  . the rst randomised evidence in 2016 , the protect trial will provide data for the comparative e ectiveness and cost - e ectiveness of active monitoring , radical prostatectomy , and radiotherapy in men diagnosed with localised prostate cancer after psa testing with a median 10 - year follow - up . 
the major ndings will provide key information needed to underpin the management of clinically localised prostate cancer , including the crucial trade - o between survival gains and potential harm caused by over - detection and unnecessary radical treatment in psa - detected prostate cancer . contributors fch , jld , and den designed the protect trial and obtained the funding . 
jal , fch , jld , and den are the guarantors of the manuscript . declaration of interests jld reports grants from the uk national institute for health research ( nihr )  . 
all other authors declare no competing interests . acknowledgments the protect trial is funded by the uk national institute for health research ( nihr ) health technology assessment programme ( projects 96 / 20 / 06 , 96 / 20 / 99 ) with the university of oxford ( oxford , uk ) as vol 15 september 2014 1117 articles sponsor . 
we acknowledge the tremendous contribution of all the protect study participants , investigators , researchers , data monitoring committee , and trial steering comittee ( chair : michael baum )  . 
we acknowledge the support from the oxford nihr biomedical research centre through the surgical innovation and evaluation theme and the surgical interventional trials unit , and cancer research uk through the oxford cancer research centre . 
we are grateful to joke snoeck for her assistance in the preparation of this manuscript . correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections gemcitabine and docetaxel versus doxorubicin as first - line treatment in previously untreated advanced unresectable or metastatic soft - tissue sarcomas ( geddis ) : a randomised controlled phase 3 trial beatrice seddon , sandra j strauss , jeremy whelan , michael leahy , penella j woll , fiona cowie , christian rothermundt , zoe wood , charlotte benson , nasim ali , maria marples , gareth j veal , david jamieson , katja kver , roberto tirabosco , sharon forsyth , stephen nash , hakim - moulay dehbi , sandy beare summary background for many years , first - line treatment for locally advanced or metastatic soft - tissue sarcoma has been doxorubicthis study compared gemcitabine and docetaxel versus doxorubicin as first - line treatment for advanced or metastatic soft - tissue sarcoma . methods the geddis trial was a randomised controlled phase 3 trial done in 24 uk hospitals and one swiss group for clinical cancer research ( sakk ) hospital . 
eligible patients had histologically confirmed locally advanced or metastatic soft - tissue sarcoma of trojani grade 2 or 3 , disease progression before enrolment , and no previous chemotherapy for sarcoma or previous doxorubicin for any cancer . 
patients were randomly assigned 1 : 1 to receive six cycles of intravenous doxorubicin 75 mg / m on day 1 every 3 weeks , or intravenous gemcitabine 675 mg / m on days 1 and 8 and intravenous docetaxel 75 mg / m on day 8 every 3 weeks . 
the trial was registered with the european clinical trials ( eudract ) database ( no 200901490729 ) and with the international standard randomised controlled trial registry ( isrctn07742377 ) , and is now closed to patient entry . findings between dec 3 , 2010 , and jan 20 , 2014 , 257 patients were enrolled and randomly assigned to the two treatment groups ( 129 to doxorubicin and 128 to gemcitabine and docetaxel )  . 
 the proportion of patients alive and progression free at 24 weeks did not differ between those who received doxorubicin versus those who received gemcitabine and docetaxel ( 463% [ 95% ci 375546 ] vs 464% [ 375548 ] ) ; median progression - free survival ( 233 weeks [ 95% ci 196304 ] vs 237 weeks [ 181200 ] ; hazard ratio [ hr ] for progressionfree survival 128 , 95% ci 099165 , p = 006 )  . 
the most common grade 3 and 4 adverse events were neutropenia ( 32 [ 25% ] of 128 patients who received doxorubicin and 25 [ 20% ] of 126 patients who received gemcitabine and docetaxel ) , febrile neutropenia ( 26 [ 20% ] and 15 [ 12% ] ) , fatigue ( eight [ 6% ] and 17 [ 14% ] ) , oral mucositis ( 18 [ 14% ] and two [ 2% ] ) , and pain ( ten [ 8% ] and 13 [ 10% ] )  . 
154 ( 60% ) of 257 patients died in the intention - to - treat population : 74 ( 57% ) of 129 patients in the doxorubicin group and 80 ( 63% ) of 128 in the gemcitabine and docetaxel group . 
no deaths were related to the treatment , but two deaths were due to a combination of disease progression and treatment . interpretation doxorubicin should remain the standard first - line treatment for most patients with advanced softtissue sarcoma . 
these results provide evidence for clinicians to consider with their patients when selecting first - line treatment for locally advanced or metastatic soft - tissue sarcoma . funding cancer research uk , sarcoma uk , and clinical trial unit kantonsspital st gallen . copyright the author ( s )  . 
we identified six published randomised controlled trials , none of which showed a survival advantage for any schedule over single - agent doxorubicwe identified a further randomised controlled study comparing single - agent doxorubicin versus doxorubicin and ifosfamide chemotherapy , which was recruiting at that time , and which has since been published in 2014 , showing an advantage for the combination for progression - free survival but not overall survival . 
 although we identified three phase 2 studies ( one of which was a randomised phase 2 study comparing gemcitabine versus gemcitabine and docetaxel ) , we were unable to find any phase 3 trials comparing this combination with doxorubicin . added value of this study to our knowledge , this is the first randomised controlled trial that compares two commonly used treatmentsdoxorubicin versus gemcitabine and docetaxelas first - line treatment in advanced soft - tissue sarcoma . 
furthermore , planned subgroup analyses have not identified any subgroup for which gemcitabine and docetaxel was superior , and in particular we did not observe superiority for either leiomyosarcoma or uterine leiomyosarcoma , for which gemcitabine and docetaxel has previously been believed to be particularly active . 
we found worse treatment adherence with gemcitabine and docetaxel compared with doxorubicin , with more dose delays , lower dose intensity , and more patients stopping treatment early due to toxicity , and lower quality - of - life scores . implications of all the available evidence these results provide evidence for clinicians to consider with patients when selecting first - line treatment for advanced soft - tissue sarcoma . 
although the observed similar progression - free survival and overall survival of gemcitabine and docetaxel and doxorubicin might support a conclusion that either schedule can be used according to patient or clinician preference , our results indicate the need for caution with such an approach given the greater difficulty in delivery and toxicity of gemcitabine and docetaxel , and indeed the higher cost of this combination regimen . 
the data support the conclusion that doxorubicin should remain standard of care as first - line treatment for most patients with advanced soft - tissue sarcoma , and that there is no subgroup of patients for whom gemcitabine and docetaxel should be routinely recommended . introduction soft - tissue sarcoma comprises a number of rare malignancies , with 3298 patients newly diagnosed with the disease in the uk in 2010.1 surgery with radiotherapy is the most common treatment for localised disease , with associated 5 - year overall survival of 55% in 200610.1 survival outcomes for locally advanced or metastatic softtissue sarcoma are poor , with a median overall survival of 128143 months after diagnosis.2 , 3 doxorubicin has been used as first - line treatment for locally advanced or metastatic soft - tissue sarcoma for more than 40 years . 
a trial2 comparing randomised controlled phase 3 combination doxorubicin versus doxorubicin alone showed a significant increase in progression - free survival in the combination treatment group , but with no increase in overall survival . 
toxicity was predictably higher in the combination group , and the authors concluded their results do not support the use of intensified doxorubicin and ifosfamide for palliation of advanced soft - tissue sarcoma unless the specific goal is tumour shrinkage . 
subsequently , two first - line phase 3 trials4 , 5 have combined doxorubicin with novel agents ( doxorubicin and palifosfamide compared with doxorubicin and placebo , 4 and doxorubicin and evofosfamide compared with doxorubicin alone5 ) , and neither study ifosfamide and was able to show improved progression - free survival or overall survival for the combination treatments . 
thus , no regimen has proved to be unequivocally superior to doxorubicin as first - line treatment for locally advanced or metastatic soft - tissue sarcoma . gemcitabine and docetaxel was first reported as a treatment for locally advanced or metastatic soft - tissue sarcoma in 2002 . 
this study also compared plasma levels of gemcitabine achieved with a 90 - min infusion versus a 30 - min infusion , and showed that the 90 - min infusion was associated with a longer duration of plasma gemcitabine concentrations above 10 mol / l , which is the threshold for saturation of intracellular accumulation of the active form of the drug , gemcitabine triphosphate . 
a further retrospective review of gemcitabine and docetaxel in patients with locally advanced or metastatic disease included an in - vitro study to investigate the dosing sequence of gemcitabine and docetaxel , finding that gemcitabine followed by docetaxel was synergistic , whereas docetaxel followed by gemcitabine was antagonistic.7 hence , the currently used schedule of gemcitabine and docetaxel in locally advanced or metastatic soft - tissue sarcoma was established . 
subsequently , several 1398 vol 18 october 2017 articles retrospective studies and phase 2 studies , in both leiomyosarcoma811 and unselected soft - tissue sarcoma , 7 , 12 , 13 have all showed activity of the combination . 
the observed responsiveness of leiomyosarcoma in particular has led to some clinicians adopting gemcitabine and docetaxel as a first - line treatment option for locally advanced or metastatic leiomyosarcoma , in the absence of evidence from phase 3 trials . 
with increasing use of the combination in both leiomyosarcoma and locally advanced or metastatic softtissue sarcoma , robust evidence is needed to establish the roles of gemcitabine and docetaxel and doxorubicin as firstline treatments for this disease . the geddis trial aimed to compare the efficacy of gemcitabine and docetaxel versus doxorubicin in the firstline setting for locally advanced or metastatic soft - tissue sarcoma . 
a pharmacogenomics study was also done to investigate the influence of single - nucleotide polymorphisms ( snps ) on treatment efficacy and toxicity . methods study design and participants geddis was a multicentre , randomised , phase 3 trial , which recruited patients from 24 uk hospitals , and one swiss group for clinical cancer research ( sakk ) hospital in switzerland ( appendix p 1 )  . 
patients were required to have adequate organ function ( absolute neutrophil count 10 10 per l ; platelet count 100 10 per l ; bilirubin 15 upper limit of normal [ uln ] ; aspartate transaminase , alanine transaminase , or both 30 uln ; alkaline phosphatase 30 uln [ patients were eligible with a higher alkaline phosphatase concentration if this was shown to be due to bone isoenzyme ] ; measured or calculated creatinine clearance 30 ml / min ; and cardiac ejection fraction within local normal limits )  . 
tumour tissue was required to be available for central review . treatment delays patients were excluded from the trial if they had alveolar soft part sarcoma , gastrointestinal stromal tumour , ewings dermatofibrosarcoma sarcoma , alveolar or embryonal rhabdomyosarcoma , desmo plastic small round cell tumour , extraskeletal myxoid chondrosarcoma , protuberans , malignant mixed mesodermal tumour or carcinosarcoma of the uterus , smooth muscle tumours of uncertain malignant potential of uterus , known active or uncontrolled brain metastases , active uncontrolled infection , or grade 3 or 4 peripheral neuropathy . 
pregnant or lactating women were excluded , as were patients with a history of malignancy other than sarcoma ( exceptions included basal or squamous cell carcinoma of the skin and carcinoma in situ of the cervix , breast , or prostate ) within 3 years before enrolment . samples of formalin - fixed , paraffin - embedded tumour tissue and haematoxylin and eosin - stained slides were submitted for central review for confirmation of sarcoma diagnosis and histological subtype , although patients were enrolled on the basis of the local pathology report . 
all samples were reviewed by a single histopathologist ( rt )  . the trial was approved by the national research ethics service committee : london , bloomsbury ( 10 / h0713 / 54 ) , the medicines and healthcare products regulatory agency ( clinical trials authorisation number 20363 / 0285 / 001 0001 ) , and by the research and development department of each participating nhs trust . 
gemcitabine was administered over 90 min and docetaxel was administered over 60 mdose capping according to sites local policy and dose banding to within plus or minus 5% of the calculated dose were permitted . 
in both groups , patients completed up to six cycles of treatment in the absence of disease progression , intolerable side - effects , or withdrawal of consent . laboratory monitoring ( blood count and biochemistry ) was done within 72 h of day 1 of each cycle , with additional monitoring on day 8 ( blood count only ) for gemcitabine and docetaxel treatment . 
to proceed with treatment on day 1 of each cycle ( both groups ) the following were required : absolute neutrophil count of at least 10 10 per l , platelet count of at least 100 10 per l , bilirubin of up to 15 uln , and aspartate transaminase , alanine trans aminase , or both of up to 30 uln . 
for administration of treatment on day 8 ( in the gemcitabine and docetaxel group ) the following were required : absolute neutrophil count of at least 10 10 per l and platelets of at least 75 10 per l . 
dose modifications for adverse events were made according to prespecified criteria : dose reductions of 20% ( first occurrence ) nd then 33% ( second occurrence ) were permitted for doxorubicin ( in the case of grade 3 or worse febrile neutropenia ) and gemcitabine and docetaxel ( for grade 3 or worse febrile neutropenia , grade 2 neuropathy , or any grade pulmonary toxicity ) ; a third occurrence required the patient to be withdrawn from treatment . 
 dose delays of up to 2 weeks for haematological toxicity and up to 3 weeks for non - haematological toxicity were allowed ; delays longer than this required the patient to be withdrawn from treatment . 
for doxorubicin , patients were advised to be withdrawn from treatment if left ventricular ejection fraction was less than 45% or reduced by 20% from baseline ( cardiotoxicity monitoring was done according to local institutional policies )  . 
for gemcitabine and docetaxel , patients were withdrawn for the following events : grade 3 pulmonary fibrosis , any grade 4 pulmonary toxicity , grade 3 or 4 hypersensitivity reactions ( docetaxel only ) , or grade 3 weight gain . adverse events were assessed according to the national cancer institute common terminology criteria for adverse events ( ctcae ) version 4.03 , from informed consent until 30 days after last trial treatment administration . 
serious adverse events were reported from informed consent until 30 days after last trial treatment administration , or later if the investigator felt that an event was related to trial treatment . disease status was assessed by ct scan , mri scan , or both at baseline , 12 and 24 weeks after randomisation , and then every 12 weeks until disease progression ( including patients who discontinued treatment for any reason other than disease progression )  . 
 for the pharmacogenomics analyses , dna was extracted from 4 ml whole blood using a qiaamp dna blood maxi kit ( qiagen , manchester , uk ) , according to the manufacturers instructions . 
individual candidate snps the pharmacology of the three drugs were identified from relevant published literature , 1521 and taqman assay on demand probes ( applied biosystems , paisley , uk ) were used to genotype the samples . in genes associated with outcomes the primary endpoint was the proportion of patients alive and progression free at 24 weeks after the date of randomisation . 
secondary endpoints were the proportion of patients alive and progression free at 12 weeks after the date of randomisation , progression - free survival ( time from randomisation to date of progression or death from any cause , whichever occurred first ) , and overall survival ( time from randomisation to date of death from any cause ) , the proportion of patients achieving an objective response by recist 1.1 , the proportion of patients achieving an objective response by choi criteria ( retrospective analysis ) , assessment of adverse events , quality of life , and health economics evaluation . 
time to progression , proportion of patients achieving an objective response as assessed by choi criteria , the health economics assessment , and the planned sensitivity analyses will all be published separately at a later date . 
 statistical analysis under the assumption of a hazard ratio ( hr ) of 063 , 250 patients ( and 148 progressions or deaths ) were required to achieve 80% power with a two - sided of 5% . 
 we assumed a median progression - free survival of 35 months for doxorubicin22 ( corresponding with 30% of patients achieving 24 - week progression - free survival ) and a median progression - free survival of 5 months 1400 vol 18 october 2017 articles ( corresponding with 47% of patients achieving 24 - week progression - free survival ) for gemcitabine and docetaxel.6 , 13 we did the efficacy analysis in the intention - to - treat population of all randomised patients . 
we plotted kaplan - meier curves for progression - free survival and overall survival ; treatment effect hrs ( with 95% cis and p values ) were obtained from cox proportional hazards regression models , adjusted for randomisation stratification factors . 
these analyses were exploratory by nature , and were performed using tests for interaction . we presented adverse events as the worst grade per patient per event , and comparison between groups was done using a test of proportions . we assessed quality of life at the 12 - week postrandomisation visit . 
we used ancova and fitted a linear regression model adjusting for baseline score , stratification factors , and actual time between baseline and 12 - week assessments ( to allow for variation in the timings of assessments )  . 
we prospectively actual planned in our statistical analysis plan to use 99% cis to account for multiple comparisons within the different scales of quality of life , which is a robust approach when the risk of a type 1 error is inflated by making multiple comparisons . to assess the effect of snps on efficacy and toxicity within treatment groups , we used cox proportional hazards regressions on overall survival and progressionfree survival and logistic regressions on any grade 3 or 4 adverse events . we calculated dose intensity relative to the total planned dose using a formula that incorporated delays and dose reductions.23 we used stata version 14.2 for all statistical analyses . an external independent data monitoring committee oversaw the trial and assessed the safety and efficacy approximately annually . 
this study is registered with the european clinical trials ( eudract ) database ( no 2009 01490729 ) and as an international standard randomised controlled trial , number isrctn07742377 . role of the funding source the trial was sponsored by university college london ( ucl ) and coordinated centrally by cancer research uk and ucl ctc . 
the corresponding author had full access to all the data and the final responsibility to submit for publication . associated with raw data the results between dec 3 , 2010 , and jan 20 , 2014 , 257 patients from 24 uk hospitals and one swiss hospital ( appendix p 1 ) were enrolled and randomly assigned to receive doxorubicin ( 129 patients ) or gemcitabine and docetaxel ( 128 patients ; figure 1 )  . 
two randomised patients ( one in each group ) were later found to be ineligible ( figure 1 ) ; however , both are included in the intention - totreat analysis and received treatment . 
our safety population included 254 of the 257 randomised patients , 497 patients assessed for eligibility 240 excluded 91 did not meet inclusion criteria 96 declined to participate 53 other reasons * 257 patients enrolled and randomly assigned 129 allocated to doxorubicin 128 allocated to gemcitabine and docetaxel 1 did not start treatment 2 did not start treatment 128 received allocated intervention ( including 126 received allocated intervention ( including 1 ineligible patient ) 1 ineligible patient ) 3 lost to follow - up 58 discontinued intervention|| 1 lost to follow - up 79 discontinued intervention|| 129 included in intention - to - treat population 128 included in safety population 128 included in intention - to - treat population 126 included in safety population figure 1 : trial profile * other reasons were : 43 multidisciplinary team decision not to approach patient , five deaths , three referred to or treated at other hospital , one patient did not fully understand trial , one trial closed before patient finished radiotherapy . 
histology review reclassified as ineligible histological subtypes ( one gastrointestinal tumour in the doxorubicin group and one extra - skeletal myxoid chondrosarcoma in the gemcitabine and docetaxel group )  . 
||see appendix p 6 for a breakdown of reasons for treatment discontinuation . vol 18 october 2017 1401 articles because one patient who was assigned to doxorubicin and two patients who were assigned to gemcitabine and docetaxel did not receive at least one dose of their allocated treatment ( figure 1 )  . patient characteristics were similar in the two treatment groups at baseline ( table 1 )  . 
the analysis is based on the dataset in its version of sept 8 , 2015 ; at this point , the estimated median follow - up for all patients was 22 months ( iqr 157293 )  . of the 257 randomised patients , 244 ( 95% ) had central histopathology review done . 
51 ( 21% ) of 244 reports differed between the local histology report and the central review report , with 36 ( 14% ) major discrepancies resulting in reclassification of histology , and 15 ( 6% ) minor discrepancies ( eg , high - grade spindle cell sarcoma being reclassified as pleomorphic sarcoma )  . 
of the 13 ( 5% ) of 257 patients whose histology was not reviewed , six samples were never received , one patient had no tissue available , and for six patients there was no tumour tissue in the submitted blocks . more patients in the doxorubicin group ( 71 [ 56% ] of 128 patients ) received the full six cycles of chemotherapy than those in the gemcitabine and docetaxel group ( 49 [ 39% ] of 126 patients )  . 
mean dose intensity23 ( incorporating dose delays and reductions ) was 937% ( sd 009 ) in the doxorubicin group and 834% ( sd 020 ) in the gemcitabine and docetaxel group . 
 more patients in the gemcitabine and docetaxel group experienced dose delays ( 71 [ 56% ] of 126 patients ) than in the doxorubicin group ( 59 [ 46% ] of 128 patients )  . 
the main reasons for dose delays in both groups were febrile neutropenia ( seven [ 12% ] of 59 reasons in the doxorubicin group vs six [ 4% ] of 155 reasons in the gemcitabine and docetaxel group ) , other haematological toxicities ( 16 [ 27% ] vs 44 [ 28% ] ) , non - haematological toxicities ( five [ 8% ] vs seven [ 5% ] ) , other adverse events ( 14 [ 24% ] vs 29 [ 18% ] ) , and other practical or social reasons ( 11 [ 19% ] vs 32 [ 21% ] )  . 
 more patients had dose reductions in the doxorubicin group ( 34 [ 27% ] of 128 patients ) than in the gemcitabine and docetaxel group ( 23 [ 18% ] of 126 ; appendix p 17 ) ; the main reasons for dose reductions were febrile neutropenia ( eight [ 20% ] of 41 reasons in the doxorubicin group vs one [ 1% ] of 89 reasons in the gemcitabine and docetaxel group ) and other haematological toxicities ( seven [ 17% ] of 41 vs 26 [ 29% ] of 89 )  . 
one ( 1% ) of 128 patients in the doxorubicin group and 13 ( 10% ) of 126 in the gemcitabine and docetaxel group stopped treatment early because of toxicity ( appendix p 6 )  . at the time of data analysis , 223 ( 87% ) of 257 patients in the intention - to - treat population had experienced disease progression ; 106 ( 82% ) of 129 patients in the doxorubicin group and 117 ( 91% ) of 128 patients in the gemcitabine and docetaxel group . 
154 ( 60% ) of 257 patients died in the intention - to - treat population ; 74 ( 57% ) of 129 patients in the doxorubicin group and 80 ( 63% ) of 128 patients in the gemcitabine and docetaxel group . 
no deaths were related to the treatment , but two deaths were due to a combination of disease progression and treatment ( see appendix p 10 for the breakdown of causes of death by treatment group )  . 
no discrepancies were noted between the hospitals and the central review for any patients . progression - free survival at 24 weeks did not differ between the treatment groups ( 463% [ 95% ci 375546 ] in the doxorubicin group vs 464% [ 375548 ] in the gemcitabine and docetaxel group ; figure 2 )  . 
the unadjusted hr was 128 ( 95% ci 099165 ; p = 006 ) ; after adjusting for 1402 vol 18 october 2017 articles histological subtype , the hr was 126 ( 097163 ; p = 008 ) in favour of doxorubic although the kaplan - meier curves did not violate the proportional hazards assumption ( p = 046 for the adjusted model ) , they initially overlapped , and then separated after 24 weeks . overall survival did not significantly differ between the two groups . 
overall survival at 24 weeks was 868% ( 95% ci 796916 ) in the doxorubicin group and 826% ( 748882 ) in the gemcitabine and docetaxel group ( figure 3 )  . 
median overall survival was 763 weeks ( 95% ci 600913 ) in the doxorubicin group and 673 weeks ( 531831 ) in the gemcitabine and docetaxel group ( unadjusted hr 114 , 95% ci 083157 ; p = 041 )  . the proportion of patients achieving an objective response by recist 1.1 ( complete or partial response ) was similar in the two groups : 25 ( 19% ) of 129 patients in the doxorubicin group and 25 ( 20% ) of 128 in the gemcitabine and docetaxel group ( table 2 )  . 
 in our prospectively planned exploratory subgroup analysis , no evidence of a differential treatment effect by histological subtype was recorded ( p = 024 ; appendix p 11 )  . 
further subgroup analyses were done comparing leiomyosarcoma versus other sarcomas ( p = 014 ) , and uterine leiomyosarcoma versus other sarcomas ( p = 038 ) , but again no differential effect was evident between the two treatment groups . 
 the most common low - grade non - haematological adverse event was grade 1 and 2 alopecia , which occurred in 110 ( 86% ) of 128 patients in the doxorubicin group and 95 ( 75% ) of 126 patients in the gemcitabine and docetaxel group ( table 3 )  . 
the most common low - grade haematological adverse event was anaemia ( grade 12 in 91 [ 71% ] patients in the doxorubicin group vs 104 [ 83% ] in the gemcitabine and docetaxel group )  . 
the three most common serious adverse events , accounting for 111 ( 39% ) of all 285 serious adverse events , were febrile neutropenia ( 27 [ 17% ] of 155 serious adverse events in the doxorubicin group vs 15 [ 12% ] of 130 in the gemcitabine and docetaxel group ) , fever ( 18 [ 12% ] vs 19 [ 15% ] ) , and neutropenia ( 22 [ 14% ] vs ten [ 8% ] ; appendix pp 79 )  . we compared quality of life between the groups at 12 weeks postrandomisation . 
insufficient questionnaires were returned to be able to assess quality of life at 18 weeks and 24 weeks ( 83 [ 32% ] of 257 questionnaires were returned at both 18 weeks and 24 weeks , compared with 132 [ 51% ] of 257 at 12 weeks )  . 
however , the mean global health status score at 12 weeks was 638 ( sd 225 ) in the doxorubicin group ( based on 64 [ 50% ] of 129 patients ) and 591 ( sd 218 ) in the gemcitabine and docetaxel group doxorubicin gemcitabine and docetaxel hr 128 ( 95% ci 099165 ) ; p = 006 time since randomisation ( weeks ) 129 ( 0 ) 128 ( 0 ) 60 ( 1 ) 60 ( 2 ) 28 ( 6 ) 12 ( 4 ) 11 ( 10 ) 5 ( 6 ) 3 ( 11 ) 3 ( 6 ) number at risk ( number censored ) doxorubicin gemcitabine and docetaxel figure 2 : progression - free survival hr = hazard ratio . doxorubicin gemcitabine and docetaxel hr 114 ( 95% ci 083157 ) ; p = 041 time since randomisation ( weeks ) 129 ( 0 ) 128 ( 0 ) 108 ( 4 ) 104 ( 3 ) 80 ( 12 ) 74 ( 13 ) 47 ( 27 ) 44 ( 20 ) 20 ( 42 ) 24 ( 31 ) number at risk ( number censored ) doxorubicin gemcitabine and docetaxel figure 3 : overall survival hr = hazard ratio . complete response partial response stable disease progressive disease not evaluable data are n ( % )  . table 2 : objective responses doxorubicin ( n = 129 ) gemcitabine and docetaxel ( n = 128 ) 2 ( 2% ) 23 ( 18% ) 60 ( 47% ) 25 ( 19% ) 19 ( 15% ) 25 ( 20% ) 50 ( 39% ) 27 ( 21% ) 26 ( 20% ) ( based on 63 [ 49% ] of 128 patients )  . 
myocardial infarction ( grade 5 ) recorded in one patient who received doxorubicsudden death not otherwise specified ( grade 5 ) recorded in one patient who received gemcitabine and docetaxel . 
higher scores are associated with better quality of life ; a positive number indicates better functioning and quality of life on gemcitabine and docetaxel than on doxorubic lower scores are associated with better quality of life ; a positive number indicates worse symptoms on gemcitabine and docetaxel than on doxorubicc30 = eortc core quality - of - life questionnaire . 
 table 4 : difference in quality - of - life outcomes at 12 weeks after randomisation for the pharmacogenomics analysis in our translational from total dna was successfully extracted study , 240 patients : 119 in the doxorubicin group and 121 in the gemcitabine and docetaxel group . 
within the doxorubicin group , three of the four snps in the slc22a16 gene , all in linkage disequilibrium with each other , were associated with a worse progression - free survival ( appendix pp 12 , 15 ) , as was the minor allele of the slc29a1 snp ( rs9394992 , in both heterozygotes and homozygotes ; appendix p 14 )  . 
by contrast , the prdx4 snp ( rs518329 ) minor allele was associated with improved overall survival in the doxorubicin group in both heterozygotes and homozygotes ( appendix p 13 )  . 
analysis of the gemcitabine and docetaxel treatment group indicated a possible association of the abcb1 rs1045642 minor allele with worse progression - free survival in both heterozygotes and homozygotes ( appendix p 12 ) ; the cda rs2072671 snp was associated with worse overall survival ( appendix p 14 ) , and the cmpk1 rs4492666 snp was associated with improved overall survival in both heterozygotes and homozygotes ( appendix p 14 )  . 
the slc22a16 rs723685 minor allele was associated with a reduced frequency of grade 34 adverse events compared with wild type ( ten [ 48% ] of 21 patients vs 69 [ 71% ] of 97 patients ) in the doxorubicin treatment group but not in the gemcitabine and docetaxel group . 
 after completion of treatment within the trial , 58 ( 23% ) of 254 patients in the safety population ( 28 [ 22% ] of 128 patients receiving doxorubicin and 30 ( 24% ) of 126 receiving gemcitabine and docetaxel ) did not receive any additional treatment . 
the remaining 196 ( 77% ) patients received at least one additional treatment : chemotherapy for 139 ( 71% ) of 196 patients ( 62 [ 62% ] of 100 patients in the doxorubicin group and 77 [ 80% ] of 96 patients in the gemcitabine and docetaxel group ) , and local therapies for 57 ( 29% ) of 196 patients ( 38 [ 38% ] and 19 [ 20% ] )  . 
soft - tissue sarcoma is recognised to be a very heterogeneous disease with a large number of histological subtypes , and indeed our trial included 22 different subtypes , with very small numbers of patients with many of these subtypes . 
this heterogeneity is an inevitable feature of most large soft - tissue sarcoma trials , and as such we believe that the geddis trial population is representative of the general population with advanced soft - tissue sarcoma . the activity of combination gemcitabine and docetaxel has been used in locally advanced or metastatic soft - tissue sarcoma since 2002 , and has been investigated in several small studies , which have shown therapy.69 , 11 , 12 a randomised phase 2 study compared gemcitabine and docetaxel with gemcitabine alone in 122 patients with advanced soft - tissue sarcoma who had received between zero and three previous chemotherapy regimens , and reported superior median progression - free survival for gemcitabine and docetaxel compared with gemcitabine alone ( 62 months vs 30 months ) and overall survival ( 179 months vs 115 months ) .13 a subsequent randomised phase 2 study compared gemcitabine and docetaxel versus gemcitabine alone as second - line treatment in 90 patients with leiomyosarcoma , reporting that both schedules were effective second - line therapies , with similar proportions of patients achieving a response.10 gemcitabine and docetaxel has therefore become an accepted in metastatic soft - tissue sarcoma after first - line therapy.24 subsequent phase 1b / 2 studies have combined gemcitabine and docetaxel with bevacizumab showing feasibility and activity , 25 , 26 and also with pazopanib , 27 although that trial closed early because of slow accrual and substantial toxicity . 
a placebo - controlled phase 3 trial28 of gemcitabine and docetaxel in combination with bevacizumab in metastatic uterine leiomyosarcoma for first - line treatment did not show a benefit for progression - free survival or overall survival . treatment option since the first published study6 of gemcitabine and docetaxel , which was confined to patients with leiomyosarcoma , some clinicians have assumed that the combination is more active in leiomyosarcoma and uterine leiomyosarcoma than in other histological subtypes . 
 treatment eect favours doxorubicin favours gemicitabine and docetaxel figure 4 : quality - of - life outcomes at 12 weeks post - randomisation the plotted points represent the mean treatment effect between the groups ( a positive number for the treatment effect indicates a better quality of life on gemcitabine and docetaxel than doxorubicin )  . 
however , the results of the geddis trial refute these claims of superior activity in particular histological subtypes of locally advanced or metastatic softtissue sarcoma versus others , since our results show no evidence influenced by treatment effect was histological subtype . 
we did planned subgroup analyses to investigate whether patients with either leiomyosarcoma or uterine leiomyosarcoma responded better to gemcitabine and docetaxel than other soft - tissue sarcoma histological subtypes , but found no indication of a superior response to gemcitabine and docetaxel in either of these subgroups . that we chose 13 years as the minimum age for the trial , specifically to try to increase participation of the teenage and young adult population , because clinical trial recruitment of this age group is recognised to be poor.29 however , only one patient younger than 18 years of age was recruited , which we believe reflects the differing approaches to treatment of advanced soft - tissue sarcoma by uk paediatric and adult oncologistswith paediatric oncologists using more intensive chemotherapy regimens than those used in this trial . 
additionally , competing paediatric trials in this population were running in the uk at the time of recruitment to geddis , such that we believe that younger patients were preferentially recruited to those paediatric trials . why did gemcitabine and docetaxel fail to show superiority to doxorubicin ? this outcome might have been vol 18 october 2017 1407 articles partly due to the choice of lower dose and fewer cycles of treatment ; the 2002 study by hensley and colleagues6 delivered more cycles ( eight vs six ) , at higher doses ( gemcitabine 900 mg / m and docetaxel 100 mg / m vs gemcitabine 675 mg / m and docetaxel 75 mg / m ) than in geddis . 
our regimen was chosen on the basis of the randomised phase 2 study of maki and colleagues , 13 which had used the higher dose schedule , and had reported high frequency ( 46% ) of dose reductions for gemcitabine and docetaxel , lower dose intensity than gemcitabine , and more than 40% of patients on gemcitabine and docetaxel stopping within 6 months of starting therapy , for nonhaematological toxicities such as fatigue and myalgias , despite dose reductions . 
 additionally , a previous phase 2 study11 that the geddis chief investigator had led using this schedule had found that quite substantial toxicity was experienced in the uk population , such that eight ( 18% ) of 45 patients stopped treatment early due to toxicity , and only ten ( 20% ) patients received the full eight cycles . 
the lower doses used are reflected by the absence of grade 34 thrombocytopenia recorded ( no patients on gemcitabine and docetaxel experienced this toxicity ) compared with a 40% frequency in the previous randomised phase 2 study.13 it might be suggested that the gemcitabine and docetaxel doses we selected were too low . 
 however , despite modifying the gemcitabine and docetaxel schedule for the geddis trial , our results were similar for gemcitabine and docetaxel to those of maki and colleagues study , 13 with median progression - free survival of 55 months versus 62 months , and median overall survival of 155 months versus 179 months , respectively . receiving suitable for an additional factor in the lack of superiority of gemcitabine and docetaxel over doxorubicin at least for overall survival might be the lower overall exposure of patients to gemcitabine and docetaxel , as first - line and second - line treatments combined . 
of 96 patients in the gemcitabine and docetaxel group receiving a subsequent received doxorubicin , whereas of treatment , 60 100 patients in the doxorubicin group receiving a subsequent treatment , only 18 received gemcitabine and docetaxel . 
this difference is because for many uk hospitals at the time of the geddis trial , the combination of gemcitabine and docetaxel was not funded and thus unavailable to clinicians . despite the use of a modified gemcitabine and docetaxel schedule in our study , treatment adherence to gemcitabine and docetaxel was inferior to that for doxorubicpatients in the gemcitabine and docetaxel group experienced more dose delays and lower dose intensity than those in the doxorubicin group , with fewer patients in the gemcitabine and docetaxel group receiving all six cycles of chemotherapy and more patients stopping treatment early due to toxicity . 
docetaxel was omitted at these points according to protocol criteria for low neutrophils or platelets , or toxicity leading to a clinical decision to omit docetaxel ( notably , the most common non - haematological grade 34 toxicity in the gemcitabine and docetaxel group was fatigue )  . 
the excess of patients stopping gemcitabine and docetaxel early might also have reflected a bias in clinicians to stop treatment earlier in the experimental group , in the knowledge that patients could go on to receive standard doxorubicin - based treatment . 
it could be argued that the gemcitabine and docetaxel doses that were delayed or missed represent undertreatment in this group , which could explain the separation of the progression - free survival curves in figure 2 . although no significant difference was seen in any of the individual quality - of - life parameters between the treatment groups , the global health status was numerically lower for gemcitabine and docetaxel than in the doxorubicin group . 
 potential contributing factors are that gemcitabine and docetaxel requires an additional visit to hospital in each 3 - week cycle , and gemcitabine and docetaxel takes longer to deliver than doxorubicin , prolonging each hospital visit and resulting in an added burden on patients with incurable disease receiving palliative chemotherapy . 
the implication of these results is that gemcitabine and docetaxel was more difficult to deliver ( lower dose intensity , more treatment delays , and more patients stopping early due to toxicity ) , and was associated with a worse global health status than doxorubicthus , there does seem to be a disadvantage to patients in receiving gemcitabine and docetaxel as first - line treatment . 
furthermore , there are economic , as well as personal , disadvantages gemcitabine and docetaxel because it is a more expensive treatment regimen than doxorubicin because of higher drug costs , more frequent and longer hospital visits are needed for treatment , and increased requirements for supportive medications ( data not shown )  . importantly , the results of the current study are consistent with two other first - line studies in locally advanced or metastatic soft - tissue sarcoma that included doxorubicin as the control group , with the median progression - free survival of 233 weeks the doxorubicin group in the current study similar to the 225 weeks4 and 26 weeks5 reported in the other studies . 
 this is also true of median overall survival , which was 763 weeks in the doxorubicin group in the current study , compared with 732 weeks4 and 823 weeks5 with doxorubicin in the other studies . 
interestingly , all three studies showed an improvement in progressionfree survival and overall survival compared with the preceding published trial of judson and colleagues2 ( progression - free survival of 199 weeks and overall survival of 554 weeks ) , which had recruited patients several years earlier , suggesting that outcomes have improved for patients with locally advanced or metastatic 1408 vol 18 october 2017 articles soft - tissue sarcoma in recent years . 
clinicians might be better at selecting patients most likely to benefit from palliative chemotherapy for advanced soft - tissue sarcoma , and are treating patients more aggressively in terms of minimising dose reductions and treatment delays , with greater use of supportive medications such as growth factors . 
a further factor might be increasing use of local therapies such as radiotherapy and surgery for patients with metastatic disease , which has been associated with longer overall survival than for patients not receiving such therapies.30 indeed , 57 patients on the geddis trial went on to receive surgery or radiotherapy after completing study treatment . the pharmacogenomics data obtained in the current study suggest that snps in the organic cation transporter slc22a16 are associated with reduced efficacy and decreased toxicity following doxorubicin treatment . 
 these findings are in keeping with previously published data from a breast cancer patient cohort and are consistent with a loss of function in the transporter that results in reduced intracellular influx of doxorubicin.20 validation of these effects in an independent cohort of sarcoma patients would be valuable to ascertain the potential for this snp to influence clinical decisionmaking . 
two other snps , slc29a1 rs9394992 and prdx4 rs518329 , were also associated with outcomes in the doxorubicin group ; however , these genes are not known to be involved in the pharmacology of doxorubicin , so further investigation is required to understand these effects . 
there were indications that three snps predicted to affect gemcitabine pharmacokinetics were associated with an effect on overall survival , most notably the cda rs2072671 snp , which was associated with reduced overall survival in the gemcitabine and docetaxel group , with worse survival in patients homozygous ( rather than heterozygous ) for the minor allele ( this is referred to as a gene - dose effect )  . 
however , the same snp was not associated with a difference in progression - free survival , and insufficient evidence is currently available to advocate routine testing of these snps to influence clinical decision - making . limitations of the current study include the fact that we used a gemcitabine and docetaxel schedule that used fewer cycles and lower doses than in the originally published schedule , 6 which is widely used in other countries . 
 although we had a clear rationale for this decision , nevertheless we acknowledge that some might conclude that this limits the applicability of the trial results to the wider population of patients with advanced soft - tissue sarcoma beyond our trial . 
additionally , more patients stopped treatment early on gemcitabine and docetaxel than doxorubicin , which might have reflected the fact that clinicians knew that patients could go on to receive doxorubicin , whereas the reverse was not true due to the limited availability of gemcitabine and docetaxel in the uk at that time outside of clinical trials . how should these results inform our discussions with patients with advanced soft - tissue sarcoma ? the data do not support superiority for gemcitabine and docetaxel over doxorubicin on survival outcomes . 
although the similar progression - free survival and overall survival of gemcitabine and docetaxel and doxorubicin might support a conclusion that either schedule can be used according to patient or clinician preference , our results indicate the need for caution with such an approach , in that gemcitabine and docetaxel is more difficult to deliver than doxorubicin , and patients find it more toxic than doxorubicin , with some effects on quality of life . 
thus , the overall clinical conclusion should be that doxorubicin remains standard of care as first - line treatment for locally advanced or metastatic softtissue sarcoma , and that gemcitabine and docetaxel is not recommended as routine first - line treatment . 
there might of course be occasions when different choices are made depending on patient factors and preferences , such as using combination doxorubicin and ifosfamide for selected patients who need to optimise chances of tumour shrinkage , or using gemcitabine and docetaxel in patients with cardiac dysfunction that contraindicates use of doxorubichowever , for most patients , these results will hopefully provide evidence for clinicians to consider with their patients when selecting first - line treatment for advanced soft - tissue sarcoma . 
the study also highlights the importance of doing randomised trials in rare cancers to rigorously compare new treatments with established standard treatments , rather than extrapolating promising results from smaller non - comparative trials . contributors geddis was developed through and supported by the uk national cancer research institute sarcoma clinical studies group and was led by the trial management group ( composed of bs , sjs , jw , ml , pjw , fc , cr , zw , sf , and sb )  . 
sf and sb were responsible for the conduct of the trial , ensuring all required approvals were in place , and for collection and verification of the integrity of the data . 
all authors gave final approval of the version to be published . declaration of interests bs has received honoraria and travel grants from novartis , pharmamar , ariad , clinigen , daiichi , and lilly . 
 jw , ml , fc , zw , cb , gjv , dj , kk , rt , sf , sn , and h - md declare no competing interests . acknowledgments we thank all patients participating in geddis and their families . 
 the geddis trial was funded by cancer research uk ( c2921 / a11561 ) , with separate funding obtained from sarcoma uk ( suk16.2015 ) to support the pharmacogenomics studies described . 
we thank ian judson ( royal marsden hospital , london , uk ; retired ) for his review of the manuscript and shonit punwani ( university college london , london , uk ) for his input into the central ct scan review . 
 crs work on the trial was supported at the kantonsspital st gallen by a grant of the clinical trials unit commission , ctu 12 / 14 . correction to lancet oncol 2017 ; 18 : 132737 correction to lancet oncol 2017 ; 18 : 133847 correction to lancet oncol 2017 ; 18 : e564 dimopoulos ma , goldschmidt h , niesvizky r , et al . 
 lancet oncol 2017 ; 18 : 132737in the results section of this article , the data presented for any - grade adverse diarrhoea events should read diarrhoea ( 168 [ 36% ] vs 185 [ 41% ] )  . 
 these corrections have been made to the online version as of sept 27 , 2017 , and the printed article is correct . myelodysplastic in patients with platzbecker u , germing u , gtze ks , et al . 
luspatercept for the treatment of anaemia lowerrisk syndromes ( pace - mds ) : a multicentre , openlabel phase 2 dose - finding study with long - term extension study . 
 18 : e564in the second paragraph of brian samuels affiliation , the sentence in parentheses should have read ( summit cancer centers , post falls , id , usa )  . 
in the third paragraph , the sentence and quote from brian samuels as should have samuels summarised , we decided to recapitulate the original phase 2 study in liposarcomas pazopanib is active in the treatment of liposarcomas , just as it is for other subtypes of sarcoma . 
we aimed to compare high - dose melphalan plus salvage asct with cyclophosphamide in patients with relapsed multiple myeloma who had previously undergone asct . methods this multicentre , randomised , open - label , phase 3 study recruited patients aged at least 18 years with multiple myeloma who needed treatment for rst progressive or relapsed disease at least 18 months after a previous asct from 51 centres across the uk . 
before randomisation , eligible patients received bortezomib , doxorubicin , and dexamethasone ( pad ) induction therapy and then underwent peripheral blood stem - cell mobilisation and harvesting if applicable . 
eligible patients ( with adequate stem - cell harvest ) were randomly assigned ( 1 : 1 ) , using an automated telephone randomisation line , to either high - dose melphalan 200 mg / m plus salvage asct or oral cyclophosphamide ( 400mg / m per week for 12 weeks )  . 
 this trial is registered with clinicaltrials.gov , number nct00747877 , and eudract , number 2006 - 005890 - 24 . findings between april 16 , 2008 , and nov 19 , 2012 , 297 patients were registered , of whom 293 received pad reinduction therapy . 
between aug 26 , 2008 , and nov 16 , 2012 , 174 patients with su cient pbscs were randomised to salvage asct ( n = 89 ) or cyclophosphamide ( n = 85 )  . 
after a median follow - up of 31 months ( iqr 1942 ) , median time to progression was signi cantly longer in the salvage asct than in the cyclophosphamide group ( 19 months [ 95% ci 1625 ] vs 11 months [ 912 ] ; hazard ratio 036 [ 95% ci 025053 ] ; p < 00001 )  . 
results of randomised trials comparing high - dose therapy plus asct with conventional chemotherapy have shown that transplantation improves progression - free and overall survival.1 , 2 as a result , the procedure is regarded as the standard of care for patients with newly diagnosed multiple myeloma up to about age 6570 years without substantial comorbidities.35 the incorporation of thalidomide , bortezomib , and lenalidomide into the rst - line management strategy during induction , consolidation , or maintenance therapy has further improved patient outcomes.613 however , for most patients , a cure remains elusive and the disease will eventually relapse . 
thalidomide , bortezomib , and lenalidomide form the mainstay of treatment in combination with steroids and conventional chemotherapy . the use of asct at relapse ( salvage asct ) is an appealing option because of the potential for long - term vol 15 july 2014 lancet oncol 2014 ; 15 : 87485 published online june 17 , 2014 s1470 - 2045 ( 14 ) 70245 - 1 this online publication has been corrected . 
results of several retrospective , registrybased or single - centre analyses investigating the use of salvage asct in the relapse setting after a previous asct have been published , and all suggest a bene t for the repeated use of the procedure.1421 a review22 of available retrospective studies suggests that salvage asct can lead to objective responses in about 65% of patients , with progression - free survival and overall survival reaching 12 months and 32 months , respectively . 
 furthermore , using asct in the relapse setting seems to be associated with an overall treatment - related mortality of less than 5%.14 analyses to identify reasons for the success of salvage asct suggest that the duration of response to the rst asct is crucial.1421 taken together , these analyses point to an important role for salvage asct ; however , until now , a prospective assessment had not been done . on behalf of the uk myeloma forum and the british society of blood and marrow transplantation , we designed the national cancer research institute myeloma x relapse ( intensive ) trial to compare highdose melphalan asct with cyclophosphamide in patients with relapsed multiple myeloma who had previously undergone asct in the rst - line setting . 
the choice of cyclophosphamide as post - induction consolidation for patients in the control group represented an accepted standard of care in the absence of a global standard of care in this setting . 
 salvage plus methods study design and patients in this randomised , multicentre , open - label , parallelgroup , phase 3 trial with an initial single - intervention recruited patients with registration phase , we symptomatic , measurable multiple myeloma from 51 national health service hospitals in england , wales , scotland , and northern ireland . 
patients were eligible for registration if they needed treatment for rst progressive or relapsed disease at least 18 months after a previous asct ( reduced to 12 months in 2011 after the publication of expected bene t14 ) ; needed therapy for relapsed disease ( as de ned by the international myeloma working group [ imwg ] criteria23 ) ; were deemed t by the treating physician to undergo an intensive therapeutic protocol ; and were older than 18 years ( no predetermined upper age limit )  . 
patients who had a complete ( immuno xationnegative ) response therapy but who to rst - line subsequently became immuno xation - positive had to have a greater than 5 g / l absolute increase in paraprotein to be eligible . 
laboratory assessments to establish trialentry eligibility were done within 14 days of registration , with the following tolerance limits : adequate full blood count ( platelet count 350 10 cells per l and absolute neutrophil count 331 10 cells per l ) ; adequate renal function ( creatinine clearance 330 ml / min ) ; adequate hepatobiliary function ( total bilirubin < 2 upper limit of normal [ uln ] and an aspartate aminotransferase alanine aminotransferase ratio of < 25 uln ) ; adequate pulmonary function ( no evidence of a history of pulmonary disease , and carbon monoxide transfer coe cient or di using capacity of the lung for carbon monoxide ( cid : 98 ) of 50% ) ; and adequate cardiac function within 12 weeks before registration ( left ventricular ejection fraction 40% )  . patients were excluded if they had received therapy for their relapsed disease , had an eastern cooperative oncology group performance status of 34 , grade 2 peripheral neuropathy , known resistance to combined bortezomib , doxorubicin , and dexamethasone ( pad ) therapy , or any comorbidity that would preclude highdose chemotherapy . all patients gave written informed consent . 
the study was approved by the national ethics review board ( multicentre research ethics committee , uk ) , institutional review boards of the participating centres , and the competent regulatory authority ( medicines and healthcare products regulatory agency , uk ) , and was undertaken according to the declaration of helsinki and the principles of good clinical practice as espoused in ( clinical trials ) for human use the medicines regulations . 
the trial management group , chaired by gc , veri ed the accuracy and completeness of the data reported and the adherence of the study to the protocol , and jmb vouches for the statistical accuracy of the manuscript . pre - randomisation procedures before randomisation , all eligible patients received reinduction chemotherapy , which consisted of intravenous bortezomib 13 mg / m per day on days 1 , 4 , 8 , and 11 , intravenous doxorubicin 9 mg / m per day on days 14 , and oral dexamethasone 40 mg per day on days 14 , 811 , and 1518 during cycle 1 and days 14 during cycles 24 ( pad )  . 
patients were eligible to progress to next stage if they had received 24 cycles of pad re - induction chemotherapy according to the protocol and had a complete response , partial response , or stable disease following re - induction chemotherapy . patients then underwent peripheral blood stem cell ( pbsc ) mobilisation and harvesting ; however , su cient pbscs were available from their rst - line asct , this procedure was not compulsory . 
the response and time of progression were de ned using the imwg criteria , as per protocol . bone marrow aspirate samples at trial entry and at disease progression were cd138 + selected ( automacs , miltenyi biotec , cologne , germany ) and plasma cell strati ed permuted randomisation and masking eligible patients were randomly assigned on a 1 : 1 basis to receive either high - dose melphalan plus salvage asct or cyclophosphamide . 
a block randomisation was used to ensure treatment groups were well balanced for length of rst remission or plateau ( < 18 months vs 1824 months vs > 24 months ) and response to pad re - induction therapy ( stable disease vs partial or complete response )  . 
randomisation was done centrally at the clinical trials research unit ( leeds , uk ) using a 24 - h automated telephone randomisation line according to randomisation lists produced by the trial statistician under the supervision of jmb . 
 assessment of outcomes was also unblinded , apart from nal con rmation of central response and progression , which was done by an independent myeloma physician masked to treatment allocation . 
 procedures patients received consolidation therapy consisting of a single infusion of intravenous melphalan 200 mg / m followed by asct after 2448 h , or oral cyclophosphamide 400 mg / m per week for 12 weeks . 
 response and disease progression were assessed according to the imwg uniform response criteria for multiple myeloma ( appendix ) using blood and urine samples , unless progression of myeloma occurred as an isolated bone lesion , growth of a plasmacytoma , or an increase in plasma cells in the bone marrow without a change in m - protein , in which case tissue histological and disease examination was done . 
response progression were con rmed by a central laboratory using sequential samples of blood and urine and bone marrow aspirates taken at baseline , after re - induction treatment , 100 days after asct or 30 days after the end of cyclophosphamide treatment , every year after randomisation , and at disease progression . 
 table 1 : demographic and baseline characteristics of registered patients and randomly assigned patients , per treatment group vol 15 july 2014 articles suspensions were xed in carnoys solution and stored at in - situ hybridisation 20c . 
interphase uorescence ( ifish ) , was done with commercial probes , scored and image - captured using an axioplan microscope ( zeiss , jena , germany ) with metasystems isis software ( altluheim , germany )  . 
cd138 - puri ed plasma cells were tested with probes to identify deletion of chromosome 17p , tp53 [ ch17p deletion ] , igh , and myc gene rearrangements , and for the presence of fgfr3 / igh [ t ( 4 ; 14 ) ] and maf / igh [ t ( 14 ; 16 ) ] fusion genes , among other abnormalities . 
for the detection of a tp53 deletion , a cuto of 20% plasma - cell involvement was used , and for fusion gene detection the reporting was absolute ( present vs absent )  . 
overall survival was de ned as the time from randomisation to death from any cause , and progressionfree survival was de ned as the time from randomisation to rst documented assessment showing disease progression or death from any cause . 
we determined response in accordance with imwg criteria.23 toxicity and safety were assessed after each cycle of protocol treatment according to adverse events , graded by the national cancer institute common terminology criteria ( ctcae ) version 3.0 during routine clinical assessments at each centre.24 pain and quality - of - life results will be reported separately . for adverse events statistical analysis we planned to register 460 patients with the aim of randomly assigning 320 to a treatment group . 
the sample size was based on a 4 - year recruitment period and 2 - year follow - up , 80% power , a 5% signi cance level , and a median time to progression of 14 months in the cyclophosphamide group to detect a 30% reduction in hazard ratio [ hr ] in the asct group compared with the cyclophosphamide group , equating to a 6 - month improvement in median time to progression . 
on the basis of these assumptions , which we based on published retrospective study outcomes and an early phase trial of bortezomib in a similar population , 25 249 events were required . 
we allowed for 5% of patients to drop out . the trial closed to recruitment in november , 2012 , after an interim analysis of the primary endpoint done at the request of the independent medical research council leukaemia data monitoring and ethics committee ( dmec ) showed that the prespeci ed boundary ( de ned as a guideline as p < 0001 ) representing overwhelming evidence had been met . 
 the dmec reviewed all the information that they requested about statistical signi cance and the estimated treatment e ects to come to a decision , and on the basis of the dmec review , the chair of the leukaemia trials steering committee recommended that the trial be closed and the results unmasked . 
centres were instructed to complete treatment as per protocol for those patients receiving treatment , and attending physicians were to administer treatment at their discretion to patients not yet receiving treatment . 
followup data is being obtained regarding the nature of the treatments that were given to patients who had progressive disease after the trial closed , and durability of responses to this next line of therapy . the cuto date for the nal analysis was july 9 , 2013 , and all data entered into the database up to that timepoint were incorporated in the nal analysis . 
time to progression , objective response , progression - free survival , and overall survival endpoints related to consolidation treatment ( ie , after randomisation ) were analysed in all patients who were randomly assigned to a treatment group . 
toxicity and safety endpoints were assessed in the safety population , which consisted of all patients who received at least one dose of study treatment . we used cox regression to analyse time to progression , accounting for strati cation factors ( length of rst remission or plateau and response to pad re - induction therapy ) and whether or not mobilisation therapy was received . 
response rates ( appendix ) were compared with ordinal logistic regression analysis accounting for the strati cation factors and whether or not mobilisation therapy was received . we did sensitivity analyses to account for deviations from trial protocol for patients who had not completed study treatment at the time of trial closure by censoring these patients at the time of closure . 
 878 vol 15 july 2014 articles gc had nal responsibility for the decision to submit for publication in agreement with all the investigators participating in the trial . the median time from the original myeloma diagnosis to randomisation was 41 years ( range 22136 ) in the salvage asct group and 37 years ( 24132 ) in the a time to progression cyclophosphamide melphalan plus asct results between april 16 , 2008 , and nov 19 , 2012 , 297 patients were registered ( gure 1 )  . 
293 ( 99% ) of 297 registered patients induction received 967 cycles of pad chemotherapy , of whom 281 ( 96% ) had the protocolde ned two to four cycles and 162 ( 55% ) completed four cycles . 
between aug 26 , 2008 , and nov 16 , 2012 , 174 patients with newly mobilised pbscs or su cient pbscs stored from their rst transplant ( or both ) were randomly assigned to receive high - dose melphalan followed by asct ( n = 89 ) or oral cyclophosphamide ( n = 85 ; gure 1 )  . baseline demographic and disease characteristics were well balanced between the treatment groups ( table 1 ) , except that a higher proportion of patients had international staging system ( iss ) stage 3 multiple myeloma in the asct group than in the cyclophosphamide group . 
280 ( 94% ) of 297 registered patients were bortezomib - naive ; induction therapy before rst - line asct had consisted of thalidomide - based combinations in 182 ( 61% ) of 297 vincristine plus doxorubicin plus patients and dexamethasone - like combinations in 84 ( 28% ) , with only 50 ( 17% ) having received thalidomide maintenance after the transplant . 
no patients had received lenalidomide as a rst - line therapy . initial cytogenetic data by ifish at trial registration were available for 149 ( 50% ) of 297 registered patients and for 88 ( 51% ) of 174 randomly assigned patients ( table 1 )  . 
 cytogenetic abnormalities were collated into a cytogenetic risk pro le , which resulted in 13 ( 15% ) randomly assigned patients ( table 1 ) having an adverse risk pro le ( de ned by the presence of any one of the following : t [ 4 ; 14 ] , t [ 14 ; 16 ] , or del17p ) and 75 ( 85% ) randomly assigned patients having a standard risk pro le ( absence of adverse genetic risk factors , but including the presence of hyperdiploidy , t [ 11 ; 14 ] , del13q , and igh rearrangement with no de ned translocation partner )  . figure 2 : progression and survival outcomes in the intention - to - treat population kaplan - meier curves were plotted for time to progression ( a ) , de ned as time from randomisation to the rst assessment showing disease progression ( deaths not due to disease progression were censored ) ; progression - free survival ( b ) , de ned as time from randomisation to rst assessment showing disease progression or death from any cause ; and overall survival ( c ) , de ned as the time from randomisation to death from any cause . 
 number at risk cyclophosphamide melphalan plus asct log - rank p < 00001 b progression - free survival number at risk cyclophosphamide melphalan plus asct log - rank p < 00001 c overall survival log - rank p = 02332 number at risk cyclophosphamide melphalan plus asct time from randomisation ( months ) vol 15 july 2014 articles time cyclophosphamide group . 
the median from previous asct to rst progression or relapse was 27 years ( range 10124 ) in the salvage asct group and 25 years ( 0765 ) in the cyclophosphamide group and the median time from the previous asct to the rst required treatment ( ie , pad induction therapy ) was 28 years ( range 11124 ) in the salvage asct group and 26 years ( 1283 ) in the cyclophosphamide group . 
finally , the median time from registration to randomisation was 38 years ( range 1697 ) in the salvage asct group and 36 years ( 1674 ) in the cyclophosphamide group . 
the reasons for registered patients not proceeding randomisation , and the status of patients at trial closure , are summarised in the appendix . ( 2531 ) at the cuto date for the nal analysis ( july 9 , 2013 ) , the median follow - up was 31 months ( iqr 1942 ) in the whole population : 34 months ( iqr 1948 ) in the salvage asct group and 23 months the cyclophosphamide group . 
at data cuto , 125 progression events had occurred in the intention - to - treat population ( 57 [ 64% ] of 89 patients in the salvage asct group had con rmed disease progression vs 68 [ 80% ] of 85 patients in the cyclophosphamide group )  . 
time to progression was signi cantly longer in the salvage asct group than in the cyclophosphamide group ( median 19 months [ 95% ci 1625 ] vs 11 months [ 912 ] ; hr 036 [ 95% ci 025053 ] ; p < 00001 ; gure 2 )  . 
 overall survival did not di er signi cantly between randomised groups ( hr 062 [ 95% ci 03127 ] ; p value for treatment e ect in the cox proportional hazards regression model = 019 )  . 
3 - year overall survival was 803% ( 95% ci 693912 ) in the salvage asct group and 629% ( 466792 ) in the cyclophosphamide group ( gure 2 )  . 
the main causes of death randomised patients were progressive disease ( in eight [ 9% ] of 89 patients in the salvage asct group vs nine [ 11% ] of 85 patients in the cyclophosphamide group ) , peripheral vascular disease ( none vs one [ 1% ] ) , myelodysplastic syndrome ( one [ 1% ] vs none ) , pneumonia ( none vs one [ 1% ] ) , haemorrhage ( none vs one [ 1% ] ) , and subarachnoid haemorrhage ( none vs one [ 1% ] )  . 
cause of death was not reported in six [ 7% ] patients in the salvage the asct group and cyclophosphamide group . [ 5% ] patients four after pad induction therapy , 49 ( 16% ; 95% ci 125212 ) of 297 patients achieved a stringent complete response or complete response , 186 ( 63% ; 569682 ) had a very good partial response or partial response , and 44 ( 15% ; 110194 ) had stable disease ( table 2 )  . 
thus , the proportion of patients achieving a very good partial response or better was 37% ( 111 of 297 ; 319429 ) , and the proportion of patients achieving an overall response was 79% ( 745837 ; table 2 )  . 
after randomisation , a stringent complete response or complete response was reported in 35 ( 39% ; 95% ci 291503 ) of 89 patients in the salvage asct group compared with 19 ( 22% ; 143327 ) of 85 patients in the cyclophosphamide group ( odds ratio [ or ] 224 , 111465 ; p = 0021 )  . 
39 ( 44% ; 335541 ) patients in the salvage asct group and 45 ( 53% ; 423636 ) in the cyclophosphamide group had a very good partial response or partial response . 
the proportion of patients with a very good partial response or better was 60% ( 53 of 89 ; 494697 ) after salvage asct versus 47% ( 40 of 85 ; 364577 ) after cyclophosphamide ( or 038 , 95% ci 0207 ; p = 00036 )  . an analysis of responses to initial and salvage asct revealed that the proportion of patients who achieved an objective response after rst - line asct was 96% ( 85 of 89 ) , whereas it was 83% ( 74 of 89 ) after salvage asct . 
of the 52 ( 58% ) of 89 patients who achieved a stringent complete response or complete response after rst - line asct , 28 ( 54% ) reached a stringent complete response or complete response after salvage asct , whereas 15 ( 29% ) achieved a very good partial response or partial response ( appendix )  . 
additionally , of the 33 ( 37% ) of 89 patients who had a very good partial response or partial response after rst - line asct , ve ( 15% ) achieved a stringent complete response or complete response after salvage asct , whereas 22 ( 67% ) achieved a very good partial response or partial response . 880 vol 15 july 2014 articles hr ( 95%ci ) 005 ( 00060419 ) 044 ( 02870672 ) 0086 ( 00090831 ) 0288 ( 01740478 ) 0590 ( 02871209 ) 0200 ( 01030390 ) 2410 ( 039614662 ) 0362 ( 02460534 ) response at end of pad scr or cr ( n = 54 ) vgpr or pr ( n = 84 ) sd ( n = 6 ) 2 microglobulin at registration < 35 mg / l ( n = 112 ) > 35 mg / l ( n = 47 ) ifish cytogenetic risk * favourable ( n = 75 ) unfavourable ( n = 13 ) overall ( n = 174 ) 001 010 020 050 100 200 500 1000 favours melphalan plus asct favours cyclophosphamide figure 3 : subgroup analysis of time to progression hrs for risk of disease progression in the melphalan plus salvage asct group compared with the cyclophosphamide group . 
 * adverse risk was de ned by the presence of a t ( 4 ; 14 ) translocation , t ( 14 ; 16 ) translocation , or tp53 deletion ; standard risk was de ned by the absence of adverse markers . 
second primary malignancies were reported in three patients at a median of 334 months ( range 199383 ) after trial registration : one patient was diagnosed with prostatic cancer in the asct group , with one patient diagnosed with squamouscell cancer and one patient diagnosed with breast cancer in the cyclophosphamide group . discussion this phase 3 study , which was stopped early because it crossed a stopping boundary for e cacy at an interim analysis , assessed the application of salvage asct in patients with recurrence of multiple myeloma after previous asct . 
the use of high - dose melphalan plus asct at relapse signi cantly prolonged progression compared with cyclophosphamide therapy . time until now , only retrospective single - centre and registry studies had examined the role of salvage asct , all concluding a bene cial e ect , although with varied results for durability of response ( panel ) .1421 our randomised study provides clear evidence for the bene t of high - dose melphalan plus salvage asct by showing that patients assigned to this treatment achieved a durable response after re - induction therapy with bortezomib , doxorubicin , and dexamethasone . 
few phase 3 trials have focused on treatment for rst relapse in multiple myeloma , and although cross - trial comparisons are problematic , our results compare favourably with those achieved with combination therapy incorporating novel response to pad re - induction the time - to - progression bene t associated with salvage asct was consistent across subgroups of patients de ned therapy and 2 - microglobulin concentration at registration , but not for those with an adverse cytogenetic risk by ifish ( gure 3 )  . 
for the 64 ( 72% ) of 89 patients in the salvage asct group and 64 ( 75% ) of 85 in the cyclophosphamide group who had a rst response lasting longer than 24 months , median time to progression was 24 months ( 95% ci 1827 ) versus 11 months ( 1012 ) , respectively ( hr 035 , 95% ci 022054 ; p < 00001 from cox proportional hazards regression model )  . 
for the 25 ( 28% ) patients in the salvage asct group and 21 the cyclophosphamide group who had a rst response of 24 months or less , median time to progression was 13 months ( 95% ci 1020 ) and 9 months ( 812 ) , respectively ( hr 037 , 95% ci 019074 ; p < 00037 from cox proportional hazards regression model )  . ( 25% ) results of sensitivity analyses for time to progression , progression - free survival , and overall survival that censored patients who had not completed study treatment at the time of trial closure were similar to those of the intention - to - treat analyses ( data not shown )  . all patients who received at least one dose of study treatment were assessed for adverse events . 
during pad induction therapy , 131 ( 45% ) of 293 patients reported at least one serious adverse event , with 120 ( 60% ) of 131 reported serious adverse events suspected to be related to the study medication . 
the most frequent ctcae grade 34 adverse events were haematological ( table 3 ) : 125 ( 43% ) of 293 patients who had pad induction therapy had grade 34 neutropenia , and 150 ( 51% ) had grade 34 thrombocytopenia , whereas grade 34 neuropathy ( sensory plus motor ) occurred in 35 ( 12% ) patients . 
gastrointestinal grade 34 toxicity was infrequent during pad induction therapy ( 28 [ 10% ] of 293 patients ) , as were grade 34 infections ( 25 [ 9% ] patients )  . 
during induction , 184 ( 63% ) of patients had a treatment delay , most frequently around cycle 3 , which occurred in 101 ( 34% ) , mainly due to cytopenias . 
154 ( 52% ) of 293 patients needed a dose modi cation , with g - csf support being administered to 49 ( 16% ) patients to support pad therapy , most frequently in cycle 4 ( n = 22 needed g - csf support in cycle 4 )  . the received randomly 167 patients assigned consolidation therapy ( 83 in the asct group and 84 in the cyclophosphamide group )  . 
the dose of intravenous melphalan was reduced from 200 mg / m to 140 mg / m in two ( 2% ) patients owing to reduced creatinine clearance and in four ( 5% ) patients for other reasons . 
a greater proportion of patients in the melphalan plus asct group than in the cyclophosphamide group had grade 34 adverse events related to neutropenia ( 63 [ 76% ] of 83 in the melphalan plus asct group vs 11 [ 13% ] of 84 in the cyclophosphamide group ) , thrombocytopenia vol 15 july 2014 articles ( biological ) agents . 
in one phase 3 trial , 26 time to progression after the triple combination of bortezomib , thalidomide , and dexamethasone ( vtd ) was 195 months in patients who had relapsed after rst - line asct , and the proportion of patients who received vtd who were alive at 2 years was 71% . 
in our study , 803% of patients in the salvage asct group were alive at 3 years compared with 629% in the cyclophosphamide group . results of the prede ned subgroup analysis in our study suggested that melphalan plus salvage asct was better than weekly cyclophosphamide , irrespective of the quality of response to pad re - induction and the concentration of 2 - microglobulin at registration . 
 furthermore , melphalan plus salvage asct was better than weekly cyclophosphamide irrespective of the response duration to the initial asct , although time to progression seemed to be longer in patients with a response lasting longer than 24 months after their rst asct than in those with a response of 24 months or less . 
however , the small number of patients with an adverse cytogenetic risk pro le makes the interpretation of this result di cult ; therefore , we cannot rmly recommend that salvage asct should be avoided in patients with adverse cytogenetics at rst relapse . randomised controlled trials that are stopped early for e cacy have been suggested to overestimate the e ect size.27 however , when a stringent and prede ned stopping rule is in place28 and greater than 50% of the required events have been reported , 29 stopping early has been suggested to have a negligible impact on estimated e ect sizes . 
this interim analysis was subsequently brought forward at the request of the independent dmec , but a stringent ad - hoc rule was included for early interim analyses as described above and in the statistical analysis plan . 
the primary endpoint analysis was undertaken when 125 ( 50% ) of the required 249 events had been reported , suggesting that the estimated e ect could be at most minimally in ated . although salvage asct also extended progression - free survival compared with cyclophosphamide , as yet , overall survival does not signi cantly di er between the treatment groups . 
the e ect of therapy after progression , particularly because the trial closed early , might confound the survival analysis , especially if a signi cant proportion of patients in the cyclophosphamide group received high - dose melphalan plus salvage asct at progression in this study , as retrospective studies have shown an overall survival advantage when salvage asct has been used.14 , 16 , 17 , 21 longterm follow - up analysis for overall survival will be undertaken in the future , at which point the primary endpoint analysis will also be updated . our trial further shows that the quality of responses after salvage asct is similar to that after rst - line asct . 
 we reported a stringent complete response or complete 882 vol 15 july 2014 articles response in 39% of patients after salvage asct , whereas 49% of patients had this response after the rst asct ( appendix )  . 
a partial response or very good partial response was reported in 44% of patients after salvage asct and in 34% after the rst asct . the response to pad re - induction therapy in this broadly bortezomib - naive population was similar to that seen in front - line trials of pad therapy.30 the proportion of patients with an overall response in our trial after four cycles of pad was 79% , with 17% of patients reaching a complete response or a stringent complete response and 38% achieving a very good partial response or better . 
in a randomised trial comparing pad with vincristine , adriamycin , and dexamethasone , 12 7% of patients had achieved a complete response after three cycles of pad , with 4% achieving a near - complete response and 42% achieving a very good partial response or better . 
depth of response is an important prognostic factor in the front - line transplant setting , 3133 and the results of our study suggest that the depth of response to re - induction translates longer time to progression , but this was not con rmed in our prede ned subgroup analysis . into a ( imid ) - based our trial was designed to incorporate a proteasome inhibitor - based re - induction regimen rather than an immune - modulatory drug regimen because of the high level of imid exposure in the rstline setting for trial registrants , and also because of access restrictions to treatment with any novel agents across many health - care systems . 
as such , we used a bortezomib - containing regimen as re - induction therapy to obtain a high extent of tumour control to help to assess which consolidation strategy o ered the better balance of e cacy and toxicity . 
however , when the trial was designed in 2006 , no worldwide standard of care was evident for post re - induction consolidation , although weekly cyclophosphamide was used as a standard of care in the uk in earlier medical research council trials that showed e cacy for cyclophosphamide in the nontransplant setting.34 our trial design permitted the comparison of the e ect on durability of response by alkylating - agent dose comparison . 
time to progression with cyclophosphamide in our study ( 11 months from randomisation plus a median of 38 months from requiring treatment to randomisation ) is similar to that of the control group in a study by garderet and colleagues26 and received dexamethasone ( 138 months )  . 
furthermore , no maintenance therapy was included as part of the treatments in our trial , because the role of maintenance therapy after salvage asct has not been established , even in retrospective studies . 
nevertheless , having thalidomide that shown that salvage asct has a better durability of response than does cyclophosphamide , and after studies have shown the bene t of consolidation or maintenance strategies in the front - line transplant setting , 6 , 8 , 9 , 12 , 35 further investigation of therapy after asct in the relapse setting is warranted , and we will seek to address this question in a new study . 
failure to mobilise stem cells resulted in 30 ( 11% ) of 266 patients not being eligible for randomisation ; however , the study design was powered to accommodate a stem - cell mobilisation failure rate of 30% . 
however , this study had 123 patients who had an adequate amount of stored cells , which suggests that it can be possible to mobilise enough stem cells at rstline asct for a second , salvage asct , thus making salvage asct an option for a third of patients who would be eligible for the procedure , but who might not mobilise a su cient number of stem cells at relapse . 
there was no di erence in response or outcome for patients who had their salvage asct from newly mobilised cells versus stored cells . as expected , salvage asct was associated with more grade 34 haematological and gastrointestinal adverse events than was weekly cyclophosphamide . 
the proportion of patients with grade 34 peripheral neuropathy after pad induction was 12% , which is lower panel : research in context systematic review the management of relapsed multiple myeloma after a previous autologous stem - cell transplant ( asct ) has evolved over the past 1015 years with the advent of strategies containing new agents . 
we undertook a systematic review , with no date or language restrictions ( pubmed search for salvage autologous transplant , second autologous transplant , and relapsed myeloma ) , in 2006 and found seven published studies that were suitable for consideration . 
both scienti c literature reviews showed that the evidence to support salvage asct was based on retrospective registry or single - centre studies only , mainly without the incorporation of new agents in the re - induction phase . 
because the published results were limited by their retrospective and non - comparative nature , and were largely done in an era when new anti - myeloma agents were not available , randomised , multicentre data was clearly needed that delineated the true potential for salvage asct in relapsed disease , as evidence for clinical decision making and thus practice - changing research . interpretation we show that high - dose melphalan plus salvage asct administered at rst relapse signi cantly prolongs time to progression compared with conventional , low - dose alkylating agent ( cyclophosphamide ) consolidation , after the use of a re - induction regimen containing a new agent . 
the data provide the necessary prospective evidence not only substantiating the previous retrospective studies in an up - to - date clinical treatment scenario , but also showing the clinical usefulness of salvage asct in myeloma at rst relapse . 
our results might aid the decision - making process for both physicians and patients with myeloma at rst relapse . vol 15 july 2014 articles that than that reported in a trial by sonneveld and colleagues13 after pad induction ( 24% ) .13 in our trial , bortezomib was administered intravenously . 
moreau and colleagues36 showed the subcutaneous administration of bortezomib results in improved tolerability , particularly a reduction in peripheral neuropathy , while retaining the e cacy reported with the intravenous application of the agent , 36 suggesting that the subcutaneous route might be preferable in future studies . in conclusion , to our knowledge , this trial is the rst randomised study to show that salvage asct is better than weekly cylcophosphamide in consolidating the response obtained from new - agent re - induction therapy . 
 the clear demonstration of e ect on durability of response in the relapse setting provides evidence for salvage asct to be considered as a standard of care for eligible patients , although this approach to the clinical management of relapsed myeloma is widely practised in some countries . 
although the e ect on overall survival remains to be clari ed , these results show that salvage asct should be routinely considered in eligible patients at rst relapse , o ering evidence for informed decision making regarding the choice of asct for clinicians and patients alike . contributors authorship was determined in accordance with a pre - determined trial management group policy delineated in the protocol . 
gc wrote the article and cw , jmb , dac , jcaven , jas , aja , mf , cp , ky , jcavet , hh , jmb , ac , soc , mtd , and tcmm obtained the data , revised the article , and gave nal approval . declaration of interests gc and jas have received honoraria , research funding , and speakers bureau fees from janssen . 
 acknowledgments the study was designed by gc and the trial management group , on behalf of the uk myeloma forum ( ukmf ) and the british society of blood and marrow transplantation ( bsbmt )  . 
 regarding survival and 35 years ( 3045 ) for overall survival ( median follow - up 34 years [ 2943 ] for the sodium thiosulfate group , and 38 years [ 3145 ] for the control group ) ; and localised and sentences disseminated disease should have read localised among participants with disease , 14 events in the sodium thiosulfate group , 13 events in the control group , and six deaths in both the control and sodium thiosulfate groups occurred and in participants with disseminated disease , 12 events and 11 deaths occurred in the sodium thiosulfate group and 11 events and four deaths occurred in the control group . 
these corrections have been made to the online version as of june 2 , 2017 . correction to lancet oncol 2017 ; 18 : 71931 registry international cancer , steliarova - foucher colombet m , ries lag , et al , and the iicc - 3 incidence contributors . 
 lancet oncol 2017 ; 18 : 71931 in this article , the coverage of the population of east asia in table 1 in the age 014 years column should have been 44% , and in the age 1519 years column , 40% . 
 consequently , the fourth sentence in the first paragraph of the results read approximately should have the world population 114% of aged ( contributing years 18 376 710 144 person - years ) was covered by the registries included in our study , ranging from 17% in south asia ( india ) to 994% in north america ( table 1 )  . 
these corrections have been made to the online version as of june 2 , 2017 , and the printed article is correct . 014 correction to lancet oncol 2017 ; 18 : 812 versus gronchi a , ferrari s , quagliuolo v , et al . 
histotype - tailored neoadjuvant chemotherapy standard chemotherapy in patients with high - risk soft - tissue sarcomas ( isg - sts 1001 ) : an international , open - label , randomised , controlled , phase 3 , multicentre trial . 
this correction has been made to the online version as of june 2 , 2017 , and the printed article is correct . correction to lancet oncol 2017 ; 18 : 6374 freyer dr , chen l , krailo md , et al . 
 effects of sodium thiosulfate versus observation on development of cisplatininduced hearing loss in children with cancer ( accl0431 ) : a multicentre , open - label , controlled , randomised , phase 3 trial . 
lancet oncol 2017 ; 18 : 6374in the summary and results of this article , the sentences should regarding adverse events have read the most common grade 34 haematological adverse events reported , irrespective of attribution , were neutropenia ( 117 [ 66% ] of 178 participant cycles in the sodium thiosulfate group vs 145 [ 65% ] of 224 in the control group ) , whereas the most common non - haematological adverse event was hypokalaemia ( 25 [ 17% ] of 149 vs 22 [ 12% ] of 187 )  . 
 in the results , sentences regarding adverse events should have read haematological toxicity was not significantly different between the treatment groups , occurring 137 ( 77% ) of 178 participant cycles in the sodium thiosulfate group and 172 ( 77% ) of 224 participant cycles in the control group ( p = 097 ; table 3 )  . 
aggregate nephrotoxicity was more common in the sodium thiosulfate group , in which 37 ( 25% ) of 149 participant cycles were affected versus 25 ( 13% ) of 187 controls ( p = 00071 ; sentences table 4 ) ; serious adverse events regarding should have read 194 serious adverse events were reported in 26 patients ; of these , 127 were deemed unrelated , 47 unlikely , 20 possibly , and none related to probably or definitely sodium thiosulfate . 
87 were nonhaematological adverse events , of which 45 were deemed unrelated , 28 unlikely , 14 possibly , and none related to probably or definitely sodium sentences thiosulfate ; regarding median follow - up should have read median follow - up was 35 years ( iqr 3045 ) for event - free vol 18 june 2017 e301 corrections for the bbc news story see health - 40802527 for the 2013 report on british south asian cancer patients see bmj open 2013 ; 3 : e002650 for more on cervical screening rates in the uk see bbc.co.uk / news / health - 40444170 for more on cervical cancer rates in canada see bmc public health 2016 ; 16 : 868 for the cancer prevention institute of california report see media / press - releases / 2017 / breastcanceramongasians.aspx turning taboos into action as the global burden of cancer continues to rise , disparities in cancer care remain ubiquitous . 
 what can be done to reduce the health care gap ? according to a recent news story , an increasing number of south asian women in the uk are hiding their cancer diagnosis from their relatives and friends . 
the consequences of this lonely experience are not only potentially physically harmful to the patientlate diagnosis and treatment reduces the chance of a good outcomebut also inevitably emotional and psychological . 
according to a 2013 report , british south asian patients with cancer are five - times more likely to suffer severe depression after a cancer diagnosis than their white counterparts . the taboo surrounding cancer remains a stubborn issue in several other cultural groups . 
in the uk , cervical cancer screening prevents 2000 deaths per year , but attendance has been falling ( 757% of eligible women were screened in 2011 vs 727% in 2016 ) and is lowest in ethnic minority and deprived communities . 
in addition to the practical issues voiced by many women who fail to attend screening ( eg , difficulty arranging a convenient appointment ) , women from ethnic minorities might experience several other barriers , including no awareness of the screening programme , not having english as a first language , lack of cancer education , unfamiliar terminology , embarrassment or modesty , and cultural or religious concerns about the intimate nature of the tests . 
 these logistical and emotional barriers are not confined to the uk ( comparable findings have been reported in immigrant groups in other countries , including the usa , canada , norway , and finland ) and are not limited to cervical cancera similar situation exists for breast cancer mammography screening . 
 an increasing incidence of cervical cancer and related mortality has been reported in muslim communities in high - income countries , such as canada , despite an overall decreasing incidence of the disease . 
a recent report from the cancer prevention institute of california showed that by contrast with other ethnic groups , a rising incidence of breast cancer has been reported in asian - americans in the past 15 years , with an increasing prevalence of latestage disease in filipino , south asian , and korean women . 
health communications should be modified to increase awareness of and access improve participation to screening programmes to rates , and screening and treatment options adapted to make them acceptable to specific cultural or religious needs . 
for example , self - sampled cervical testing could provide a suitable alternative to the standard invasive test , alleviating the emotional and cultural barriers that otherwise preclude screening uptake . 
globalised high - income nations could perhaps learn from some of the lowand middle - income countries in which such communities are indigenous , which are taking steps to address these issues locally . ultimately , health - care providers need to be flexible and culturally sensitive to the needs of different ethnic and racial groups , to ensure the provision of equitable cancer care in increasingly diverse communities . 
failure to do so will not only increase the growing cancer burden , but will reinforce health inequity as a social nor the lancet oncology vol 18 september 2017 1137 editorial corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 comment published online august 15 , 2014 s1470 - 2045 ( 14 ) 70378 - x see articles page 1129 seto t , kiura k , nishio m , et al . 
ch5424802 ( ro5424802 ) for patients with alk - rearranged advanced non - small - cell lung cancer ( af - 001jp study ) : a single - arm , open - label , phase 12 study . 
safety and activity of alectinib against systemic disease and brain metastases in patients with crizotinib - resistant alk - rearranged non - small - cell lung cancer ( af - 002jg ) : results from the dosending portion of a phase 1 / 2 study . 
j clin oncol 2014 ; 32 : 141218 . ovarian tissue cryopreservation in children with cancer ovarian tissue cryopreservation is now a major part of the strategies used to preserve fertility in prepubertal children given gonadotoxic treatments for cancer . 
unlike post - pubertal patients , oocyte or embryo cryobanking is not appropriate for children and cryopreservation of ovarian tissue remains the only therapeutic option in most of the cases . 
restoration of ovarian function after reimplantation of frozenthawed mature ovarian cortex and reports of subsequent pregnancies were the basis of the rationale that guided the development of this approach in the treatment of childhood cancer . 
however , the success rate of the procedure in adult women is unknown , and the potency of cryopreserved immature gonads to restore fertility in adult survivors of childhood cancer has not yet been assessed . 
nevertheless , recent data suggest that immature ovaries are able to restore hormonal function in prepubertal children , in the same way that mature ovaries can in adults.1 , 2 additionally , immature ovaries have been used to restore fertility in experimental models.3 , 4 although the conditions of tissue harvesting , conditioning , and storing are well supervised by national biomedical and bioethical frameworks , patient selection criteria are mainly left to the discretion local multidisciplinary committees , resulting substantial heterogeneity of inclusion criteria , not only worldwide , but also within individual countries . 
 the authors retrospectively compared the occurrence of premature ovarian insu ciency over 15 years in a population - based study of children treated for cancer , who were or not o ered this procedure . 
they report that the cumulative probability of developing premature ovarian insu ciency after treatment was completed was signi cantly higher for patients o ered ovarian tissue cryopreservation than for those who were not o ered ovarian tissue cryopreservation ( 15 - year probability 35% [ 95% ci 1053 ] vs 1% [ 02 ] ; p < 00001 ; hazard ratio 568 [ 95% ci 625216 ] at 10 years ) , suggesting that the edinburgh selection criteria accurately predicted which patients would or would not develop premature ovarian insu ciency . 
although the small number of assessable patients who had successfully undergone ovarian cryopreservation ( 14 , compared with 141 assessable patients in the not - o ered group ) weakened the comparison , this is the rst report that aimed to assess selection criteria for ovarian cryopreservation in children with cancer . 
 the o er of ovarian tissue cryopreservation in the paediatric context is especially sensitive because the delay between the procedure and the potential use of the ovarian cortex could reach decades ( the median age at diagnosis for childhood cancer is about 51 years ) .6 parents are asked to plan for a future they cannot yet imagine , and , at the same time this request suggests the possibility of recovery , and so could be perceived as a message of hope . 
in this context , the selection criteria and follow - up protocol for paediatric ovarian tissue cryopreservation , as with any treatment protocol for children with cancer , should undergo evidence - based standardisation . 
in view of the small size of population of childhood cancer patients who could bene t from the procedure , national or international studies will be necessary to properly assess the validity of these selection criteria . 
because of the di erent sensitivity of gonads to toxic treatment at di erent ages , 7 and the report of spontaneous recovery of hormonal function after premature menopause as vol 15 september 2014 1049 comment published online august 15 , 2014 s1470 - 2045 ( 14 ) 70342 - 0 see articles page 1137 a result of treatment , 8 the de nition of high - risk for premature ovarian insu ciency and of premature ovarian insu ciency itself , as well as the modalities of follow - up , should be key points of discussion in a process of harmonisation . 
other means to preserve fertility , such as ovarian transposition in case of pelvic radiotherapy , 9 should also be assessed either as an alternative or as a combined approach . almost two decades have passed since the rst ovarian tissue cryopreservation was o ered to children submitted to gonadotoxic treatment . 
it should take into account the risk of reseeding cancer , which is particularly high in blood - borne cancers ( the most common types of cancer in childhood )  . 
generation of oocytes by in - vitro culture of primordial follicles to avoid this risk is an option , but such studies are still underway and clinically relevant data are not yet available.10 the indication for reimplantation is also still debated , and many authors , including wallace and colleagues , 5 recommend that the procedure be limited to fertility use only ( rejecting its use for induction of puberty , which can be done with synthetic hormonal substitution ) , because of the limited lifespan of the ovary linked to ischaemia - related follicle depletion . 
3 , 4 the nal step of a story that began many years ago for the adult survivor of childhood cancer will therefore be taken by adult specialists ( eg , assisted reproduction physicians and surgeons ) , who are not always familiar with childhood cancers . 
int j dev biol 2012 ; 56 : 90107 . dual targeting of her2 with lapatinib and trastuzumab drugs targeting her2 are central to the treatment of patients with her2 - positive breast cancer , and dual targeting of her2 with two drugs has gained much attention since 2010.1 patients with metastatic her2positive breast cancer have better overall survival when treated with docetaxel and the two anti - her2 monoclonal antibodies ( trastuzumab and pertuzumab , which bind to di erent extracellular domains of the her2 kinase ) , than do patients treated only with docetaxel and trastuzumab.2 dual targeting of her2 is also supported by neoadjuvant studies . 
in these trials , a greater proportion of patients who were treated with chemotherapy , trastuzumab , and lapatinib ( a her1 and her2 inhibitor ) , 35 or with chemotherapy , trastuzumab , and pertuzumab6 achieved pathological complete response than did those treated with chemotherapy plus trastuzumab alone . the phase 3 , three - group neoaltto trial7 is one of the key studies to assess dual targeting of her2 . 
 in neoaltto , investigators compared trastuzumab , lapatinib , and their combination as neoadjuvant and adjuvant treatment in a population of 455 patients with early her2 - positive breast cancer . 
the anti - her2directed therapies were rst administered alone for 1050 vol 15 september 2014 see articles page 1009 a step towards predicting checkpoint inhibitor response in kidney cancer in this issue of the lancet oncology , samra turaljic and colleagues report a heroic undertaking , using wholeexome sequencing data from 5777 patients representing 19 solid tumour types.1 in their series , the presence of frameshift indels across this large pan - cancer cohort was associated with more tumour - specific neoantigens compared with non - synonymous single nucleotide variant ( nssnv ) mutations . 
in renal cell carcinoma , frameshift indels were more prevalent compared with in other tumour types and were associated with enhanced antigen - presenting machinery and t - cell activation . 
their analysis helps to resolve a rather perplexing translational conundrumspecifically , that patients with renal cell carcinoma , a disease with a modest mutational load , show responses to checkpoint inhibitors on par with other diseases with considerably higher mutational loads.2 in non - small - cell lung cancer , melanoma , and other highmutational burden cancers , emerging evidence supports a link between mutational load and clinical outcome.3 , 4 by contrast , results from studies linking mutational load to outcome in renal cell carcinoma are mixed at best.57 the need to identify a predictor of checkpoint inhibitor response in metastatic renal cell carcinoma has never been greater . 
efforts to develop predictive biomarkers have largely failedeg , pd - l1 expression has shown a prognostic role , but did not predict outcome with nivolumab in the phase 3 comparison of this drug to everolimus in metastatic renal clear cell . 
results of the cabosun trial , 8 a randomised , phase 2 study comparing sunitinib and cabozantinib , have shown a significant improvement in progression - free survival in intermediate - risk and poor - risk patients with cabozantinib . 
if multiple studies have positive results , the clinician will need to discern the appropriate patient for either targeted therapy alone ( eg , cabozantinib ) , targeted therapy combined with a checkpoint inhibitor , or immunotherapeutic strategies alone . despite the poor predictive value of pd - l1 in this setting , other biomarkers show early promise . 
atkins and colleagues9 have reported a t - effector gene signature , generated in the context of a randomised , phase 2 study that compared sunitinib , bevacizumab and atezolizumab , and atezolizumab alone . 
 these results suggest a requisite step for turaljic and colleagues , namely , to define the predictive value of frameshift indel load for checkpoint inhibitor response in metastatic renal cell carcinoma . 
without question , they have shown that frameshift indels occur more frequently in the context of renal cell carcinoma , and that frameshift indels are associated with substantial neoantigen immunogenicity compared production with greater with nssnv neoantigens . 
they retrospectively predicate the link between frameshift indel load and checkpoint inhibitor response on four datasets , three including patients with melanoma and one including patients with non - small - cell lung cancer . 
moreover , none of these experiences include randomisation to a non - checkpoint in response assessment and 982 vol 18 august 2017 comment inhibitor control , making it unclear whether frameshift indel load might merely be prognostic rather than predictive . 
supporting this premise , in a previous series of 100 patients with non - small - cell lung cancer treated with a non - checkpoint inhibitor , the authors of this report1 found a higher relapse - free survival in those patients with higher frameshift indel load . 
 with a burgeoning array of clinical trials juxtaposing checkpoint inhibitor combinations against vegf - directed therapies in metastatic renal cell carcinoma , there should be ample opportunity to discern the predictive value of frameshift indel load in metastatic renal cell carcinoma . 
such confirmation is essential because certain frequent frameshift indels in renal cell carcinoma ( eg , vhl , pbrm1 , and kmd5c ) might themselves play a role in predicting response to vegf - directed therapy.10 if validated in randomised trials that compare checkpoint inhibitor interventions with non - checkpoint inhibitor interventions , frameshift indel load could represent a predictive biomarker for immunotherapy benefit that has yet remained elusive in metastatic renal cell carcinoma . 
 manuel caitano maia , eddy s yang , neeraj agarwal , * sumanta k pal department of medical oncology and experimental therapeutics , city of hope comprehensive cancer center , duarte , ca 91010 , usa ( mcm , skp ) ; department of radiation oncology , university of alabama at birmingham comprehensive cancer center , birmingham , al , usa ( esy ) ; hugh kaul precision medicine institute , university of alabama at birmingham school of medicine , birmingham , al , usa ( esy ) ; and division of medical oncology , university of utah huntsman cancer institute , salt lake city , ut , usa ( na ) spal@coh.org skp reports personal fees from pfizer , novartis , ipsen , astellas , bristol - myers squibb , gentech , and roche , outside of the submitted work . 
na reports personal fees from pfizer , exelixis , cerulean pharma , medivation / astellas , eisai , merck , novartis , emd serono , clovis oncology , and genentech / roche , outside of the submitted work . 
immotion150 : a phase ii trial in untreated metastatic renal cell carcinoma ( mrcc ) patients ( pts ) of atezolizumab ( atezo ) and bevacizumab ( bev ) vs and following atezo or sunitinib ( sun )  . 
eur urol 2017 ; 71 : 40514 . all tumours are rare , but some are rarer than others the report from the rarecare consortium1 in the lancet oncology , which updates the estimates of the burden of rare cancers in europe raises questions well beyond its immediate subject matter : what is the purpose of cancer registries ; how important is the quality of their data ; how should we , in the 21st century , classify cancer ? cancer registries have a long and distinguished history . 
subsequently , their role has expanded to include investigations of the causes of cancer , planning the organisation and funding of health services , and comparing outcomes across time and geographies . 
the rarecare initiative has used data from cancer registries across europe to assess the spectrum and combined incidence of rare cancersrare is defined as an annual incidence of less than six cases per 100 000 people . 
they conclude that 24% of all new patients with cancer in the european standard population ( eu28 ) have a rare cancera figure that is almost double the incidence of 13% reported from the usa using an identical definition of rare.2 even within analyses based on data from european registries , discrepancies exist ( figure )  . 
the subject is published online july 4 , 2017 s1470 - 2045 ( 17 ) 30466 - 7 see articles page 1022 vol 18 august 2017 comment comment lancet oncol 2014 published online april 3 , 2014 s1470 - 2045 ( 14 ) 70137 - 8 see articles page 631 exploring better strategies for egfr antibodies in colon cancer treatment of advanced colon cancer has improved over the past 15 years . 
 the combination of chemotherapy and biological drugs including anti - egfr or anti - vegf antibodiesfor rst - line treatment , as well as the sequencing of di erent active drugs as disease progresses , can signi cantly improve outcomes.1 median survival of patients included in clinical trials is often more than 2 years . 
patients with initially unresectable metastatic disease limited to the liver can become resectable after treatment , with an opportunity for cure.2 nevertheless , despite these advances , the optimal treatment for patients with advanced colorectal cancer in clinical practice is not yet de ned . 
patients with all ras wild - type tumours bene t greatly from treatment with the anti - egfr antibodies cetuximab and panitumumab , whereas these drugs are harmful to patients with mutations in ras.3 , 4 moreover , no validated predictive biomarkers have been identi ed for antiangiogenic drugs . 
 in this setting , harpreet wasan and colleagues5 assessed two cetuximab regimens in combination with intermittent chemotherapy with folfox ( folinic acid and oxaliplatin followed by bolus and infused uorouracil ) as the backbone in a randomised phase 2 trial . 
although oxaliplatin is halted when neurotoxicity occurs , or after 6 months of therapy , uoropyrimidines and biological drugs are usually maintained until disease investigators in the coin - b trial , the progression . 
in the maintenance cetuximab group , after 12 weeks of folfox all patients continued with weekly cetuximab and only on recist progression was folfox reintroduced . the outcomes in each group in coin - b should not be compared , since each group was powered as a separate phase 2 trial . 
the primary outcome was failure - free survival at 10 months among patients who completed 12 weeks of treatment without progression , death , or leaving the trial for other reasons . 
this measure was met for both groups ( 50% for the intermittent cetuximab group and 52% for the continuous cetuximab group ) in patients who had wild - type kras . 
the ideal approach would be to select from all patients with wild - type genes those with tumours that are egfr - driven and which would therefore bene t most from complete inhibition of efgr . 
some attempts at an e ective classi cation have already been made , but further validation in clinical trials is needed.79 another subject for further study is the dynamic process of clonal evolution in tumours . 
under the selection pressure of continuous treatment , emerging ras mutant clones could cause resistance to anti - egfr antibodies.10 intermittent treatment might help to prevent the emergence of such clones . 
liquid biopsies might identify the emergence of mutant clones and might also be useful for designing trials of biological treatments.11 we agree with the coin - b investigators that their results cannot be translated into clinical practice without further validation in randomised phase 3 trials . 
patients with egfr - dependent tumours might need chemotherapy for only a short induction period followed by cetuximab vol 15 may 2014 comment published online march 20 , 2014 s1470 - 2045 ( 14 ) 70116 - 0 see articles page 640 maintenance or reintroduction on progression . 
analysis of kras / nras and braf mutations in fire - 3 : a randomized phase iii study of folfiri plus cetuximab or bevacizumab as rst - line treatment for wild - type ( wt ) kras ( exon 2 ) metastatic colorectal cancer ( mcrc ) patients . 
intermittent chemotherapy plus either intermittent or continuous cetuximab for rst - line treatment of patients with kras wild - type advanced colorectal cancer ( coin - b ) : a randomised phase 2 trial . 
j clin oncol 2014 ; 32 : 57986 . can noah guide us to improved survival in breast cancer ? introduction of adjuvant therapy with the monoclonal antibody trastuzumab has been the most signi cant advance in the management of women with early stage her2 - positive breast cancer , with improvement of disease - free and overall survival in these patients with a biologically aggressive subtype of the disease.14 for patients with large operable or locally advanced breast cancer , induction ( neoadjuvant ) chemotherapy is a standard approach . 
the noah trial5 established for the rst time that , in women with her2 - positive locally advanced or in ammatory breast cancer , addition of trastuzumab to neoadjuvant chemotherapy signi cantly increased the pathological complete response ( pcr ) compared with chemotherapy alone ( 35% vs 15% )  . 
in the lancet oncology , luca gianni and colleagues report the long - term results from noah.6 the updated results show that the bene t from addition of trastuzumab to chemotherapy in achievement of pathological complete response in the neoadjuvant setting translated into a signi cant e ect on the primary endpoint of event - free survival , with an unadjusted hazard ratio for event - free survival between the two randomised her2 - positive treatment groups of 064 ( 95% ci 044093 , p = 0016 )  . 
 furthermore , the investigators report an improvement in overall survival.6 this study has helped to de ne the role of neoadjuvant trials as an appropriate setting for assessment of novel targeted therapies in subsets of early stage breast cancer . the key to the success of this trial was appropriate patient selection for assessment of the targeted therapynamely those with her2 - positive disease . 
 despite the small study size and subsequent crossover after the approval of adjuvant trastuzumab in 2005 that potentially limited the ability of the noah trial to show a bene t on overall survival , a sensitivity analysis to account for the e ect of crossover still showed a signi cant reduction in risk of death with the addition of trastuzumab to chemotherapy . 
patients allocated to neoadjuvant trastuzumab in this trial continued the drug in the adjuvant setting for 1 year , such that improvements in event - free survival and overall survival could have been a ected by trastuzumab given after surgery . 
however , the most relevant nding from this updated analysis is that for those patients who achieved pathological complete response after neoadjuvant therapy , the hr for eventfree survival by treatment group was 029 ( p = 00135 ) , which favours patients given trastuzumab , thus showing the signi cant e ect of neoadjuvant therapy with this 550 vol 15 may 2014 expression . 
for example , mir - 193a - 3p edv minicells have been identified as apoptosis inducers via mcl1 silencing , with evidence of growth inhibition in mesothelioma xenografts.4 in the past few years , the range of promising molecular targets being investigated in mesotheliomaincluding gen etic or epigenetically stratified synthetic lethal approaches , 7 , 8 pd - 1 - targeted immune checkpoint blockade , 9 and mesothelin - directed antibody - directed conjugate therapy10has expanded rapidly . 
mir - 16 targomirs can be added to this growing list , each member of which has the potential to improve outcomes and transform a setting of unmet clinical need . dean fennell leicester cancer research centre , university of leicester & university hospitals of leicester , nhs trust , hodgkin building , lancaster road , leicester , le1 9hn , uk df132@le.ac.uk i have received grants from bayer and astex , personal fees from bayer , boehringer ingelheim , and msd , and have been a consultant for bms , msd , boehringer ingelheim , and roche , all of which were outside the submitted work . bueno r , stawiski ew , goldstein ld , et al . 
safety and activity of micrornaloaded minicells in patients with recurrent malignant pleural mesothelioma : a first - in - man , phase 1 , open - label , dose - escalation study . 
clinical safety and activity of pembrolizumab in patients with malignant pleural mesothelioma ( keynote - 028 ) : preliminary results from a non - randomised , open - label , phase 1b trial . 
sci transl med 2013 ; 5 : 208ra147 . geddis : insight into frontline therapy in soft tissue sarcoma gemcitabine has known activity in sarcoma ; although its exact role , indication , or best combination is still debated . 
the combination of gemcitabine and docetaxel gained favour in the usa after efficacy was noted in uterine leiomyosarcoma1 , 2 and later in sarcoma , generally with superiority over gemcitabine alone.3 however , this combination is used to a lesser extent in europe , partly due to more equivocal data in leiomyosarcoma , 4 noted efficacy of other gemcitabine - based regimens , 5 and potential issues of access as described in the geddis6 trial in the lancet oncology.6 recently , several phase 3 studies have provided substantial insight into the use of anthracyclines and alkylators as first - line treatments for patients with advanced sarcoma.79 the geddis6 trial iis the first to shed comparative light on the efficacy of gemcitabine and docetaxel versus doxorubicin alone in this setting . 
 the primary endpoint of the trialprogression - free survival at 24 weeksdid not differ between the two treatment groups ( 463% [ 95% ci 375546 ] in the doxorubicin group vs 464% [ 375548 ] in the gemcitabine and docetaxel group )  . 
the geddis trial investigators concluded that the combination should not be recommended as routine , while doxorubicin should remain standard of care , in the first - line setting for patients with advanced soft - tissue sarcoma . 
the results of the geddis trial should allow individual clinicians to determine how to position and in what clinical context to use gemcitabine and docetaxel for the care of their patients . 
 published online september 4 , 2017 s1470 - 2045 ( 17 ) 30672 - 1 see articles page 1397 vol 18 october 2017 1297 comment the main confounder in the trial is the starting dose and overall usage pattern of the combination . 
in conventional practice , gemcitabine and docetaxel is routinely administered with gemcitabine 900 mg / m2 given at a 10 mg / m per min infusion rate on days 1 and 8 and docetaxel 75 mg / m on day 8 of a 21 - day cycle . 
the docetaxel dose is lower than the 100 mg / m used in early trials to help mitigate toxicity.13 the regimen is generally considered well tolerated with predictable and manageable toxicity . 
in the geddis trial , patients received gemcitabine 675 mg / m at a 75 mg / m per min infusion rate on days 1 and 8 and docetaxel 75 mg / m on day 8 of a 21 - day cycle . 
the dose , infusion rate , and number of cycles of gemcitabine is relevant to the results and calls into question how the combination was perceived in trial design and used by investigators . 
the overall lack of grade 3 or 4 thrombocytopenia ( 0% ) in the combination group , at least compared with previous studies , 3 , 4 suggests that gemcitabine might have been underdosed and underused in geddis . 
 the proportion of patients who received the full treatment regimen ( ie , all six cycles ) of gemcitabine and docetaxel ( 39% vs 56% doxorubicin ) is also of interest , even with its lower starting dose , the need for fewer dose reductions ( 18% gemcitabine and docetaxel vs 27% doxorubicin ) , a significantly lower incidence of cytopenias , and a similar grade 34 adverse event profile . 
finally , it is curious that more patients in the combination group went on to receive doxorubicin as a second - line therapy after disease progression , whereas very few patients in the doxorubicin group went on to receive the combination ( 42% vs 13% )  . 
are these all signs of a preconceived investigator bias in this open - label study ? does the fact that the combination performed as well as it did under these circumstances suggest that it does have activity as a first - line treatment ? considering that no statistically significant benefit was noted in the proportion of patients achieving an objective response ( 19% doxorubicin vs 20% gemcitabine and docetaxel ) , progression - free survival ( hazard ratio [ hr ] 128 , 95% ci 099165 , p = 006 ) , and overall survival ( hr 114 , 95% ci 083157 , p = 041 ) , one could prudently conclude that neither regimen is superior . 
 this concept would allow clinicians to choose the regimen they feel is most appropriate for the patient based on their clinical scenario , comorbidities , performance status , and sarcoma subtype . 
it also argues for equipoise in consideration for either doxorubicin or gemcitabine and docetaxel as a first - line treatment for patients with softtissue sarcomas including leiomyosarcoma . the authors should be congratulated for not only publishing the results of this trial with such transparency and completeness , but also for having the foresight to design and the ability to perform and complete this very important trial . 
even though the outcome of the trial was negative based on pre - study statistical assumptions , the results should guide many clinicians as they practice medicine and hopefully make gemcitabine and docetaxel more widely available to patients in countries that still have issues of access . 
 william d tap memorial sloan kettering cancer institute , new york , ny 10065 , usa tapw@mskcc.org i have received personal fees from eli lilly , emd serono , novartis , eisai , janssen , immune design , adaptimmune , ariad , daiichi sankyo , plexxikon , morphotek , advaxis , and tracon , outside of the submitted work . 
additionally , i have a patent using atrx as a companion diagnostic for cdk4 inhibitors pending , and a patent for methods for drug discovery pending . the author ( s )  . 
randomized phase ii study of gemcitabine and docetaxel compared with gemcitabine alone in patients with metastatic soft tissue sarcomas : results of sarcoma alliance for research through collaboration study 002 [ corrected ]  . 
randomized multicenter and stratified phase ii study of gemcitabine alone versus gemcitabine and docetaxel in patients with metastatic or relapsed leiomyosarcomas : a federation nationale des centres de lutte contre le cancer ( fnclcc ) french sarcoma group study ( taxogem study )  . 
oncologist 2012 ; 17 : 121320 . 1298 vol 18 october 2017 comment 5 garcia - del - muro x , lpez - pousa a , maurel j , et al . 
gemcitabine and docetaxel versus doxorubicin as first - line treatment in previously untreated advanced unresectable or metastatic soft - tissue sarcomas ( geddis ) : a randomised controlled phase 3 trial . 
lancet oncol 2017 ; 18 : 1089103 . maintaining quality of life for patients with neuroendocrine tumours ideally , new treatments should either improve overall survival or the health - related quality of life ( hrqol ) of patients , or both , and should have a favourable costto - benefit ratio . 
for instance , folfirinox ( leucovorin , fluorouracil , irinotecan , and oxaliplatin ) significantly improves progression - free survival , overall survival , and hrqol compared with gemcitabine in patients with metastatic pancreatic adenocarcinoma , even though it causes substantially more side - effects.1 , 2 after publication of the radiant - 3 and radiant - 4 randomised , placebocontrolled , phase 3 studies , everolimus was approved for all non - functional , advanced , neuroendocrine tumours ( nets ) , including those of the pancreas , 3 lung , and gastrointestinal tract , 4 and sunitinib has been approved for pancreatic nets ( pnets ) .5 everolimus did not improve overall survival compared with placebo but was approved on the basis of a significant improvement versus placebo in progression - free survival.3 , 4 findings of randomised trials have not shown that progression - free survival is a good surrogate marker of long - term overall survival in nets , which could be because of the long natural history of nets , use of a cross - over design , or off - study use of the drug under investigation . 
however , ter - minassian and reported significant correlations colleagues6 have between progression - free survival and overall survival in two observational cohorts of patients receiving somatostatin analogues or everolimus . 
 in the lancet oncology , marianne pavel and colleagues report hrqol endpoints of the radiant - 4 trial , as measured by the time to definitive deterioration in total the first hypothesis score on the functional assessment of cancer therapy general ( fact - g ) questionnaire by at least 7 points.7 previously in radiant - 4 , compared with placebo , everolimus delayed disease progression in advanced lung or gastrointestinal nets.4 pavel and colleagues now report that disease progression was associated with a decline in hrqol , with a decline in fact - g total score of 491 ( 95% ci 371611 ) after disease progression . 
 however , no difference in time to definitive deterioration of hrqol between patients receiving everolimus and placebo was reported , with a median time to definitive deterioration in fact - g score of 1127 months ( 95% ci 9271935 ) with everolimus and 923 months ( 552 not estimable ) with placebo ( adjusted hazard ratio 081 , 95% ci 055121 ; p = 031 ) .7 what does this finding mean ? is that the toxic effects of everolimus are counterbalanced perfectly by its higher efficacy and potentially fewer disease - related symptoms than are reported with placebo . 
on one hand , everolimus was associated with a reduction in the risk of progression lung or gastrointestinal in patients with advanced nets.4 this benefit was noted in all subgroups , with the exception of 71 patients with ileal nets , 8 probably because these patients have less aggressive disease.9 on the other hand , and as with almost all effective drugs , everolimus causes side - effects : twice as many adverse events were reported with everolimus than with placebo ( grade 34 , 140 [ 69% ] of 205 vs 28 [ 29% ] of 97 ) , and more dose reductions or temporary treatment interruptions were noted ( 135 [ 67% ] of 202 vs 29 [ 30% ] of 98 ) .4 moreover , deaths ( four vs one ) and adverse events ( 59 [ 29% ] vs seven [ 7% ] ) were more frequently the primary reason for treatment discontinuation among those receiving published online august 21 , 2017 s1470 - 2045 ( 17 ) 30618 - 6 see articles page 1411 vol 18 october 2017 1299 comment corrections correction to lancet oncol 2013 ; 14 : 790 correction to lancet oncol 2013 ; 14 : 989 vandendriessche chuah mk . 
 fulvestrant placebo versus exemestane alone after progression on non - steroidal aromatase inhibitors in postmenopausal patients with hormone - receptor - positive locally advanced or metastatic breast cancer ( sofea ) : a composite , multicentre , phase 3 randomised trial . 
lancet oncol 2013 ; 14 : 98998in the methods section of the summary of this article , the rst part of the third sentence should have read participants were randomly assigned ( 1 : 1 : 1 ) to receive intramuscular fulvestrant ( 500 mg injection on day 1 , followed by 250 mg doses on days 15 and 29 , and then every 28 days )  . 
 vol 14 september 2013 e391 corrections correction to lancet oncol 2013 ; 14 : 297 correction to lancet oncol 2013 ; 14 : 481 correction to lancet oncol 2013 ; 14 : 557 motzer rj , escudier b , tomczak p , et al . 
this correction has been made to the online version as of may 28 , 2013 . galimberti v , cole bf , zurrida s , et al , for the international breast cancer study group trial 2301 investigators . 
 lancet oncol 2013 ; 14 : 297305in the summary of this article , the fourth sentence of the findings section should read : breast cancer - related events were recorded in 48 patients in the axillary dissection group and 47 in the no axillary dissection group ( ten local recurrences in the axillary dissection group and eight in the no axillary dissection group ; three and nine contralateral breast cancers ; one and ve regional recurrences ; and 34 and 25 distant relapses )  . 
 this correction has been made to the online version as of may 28 , 2013 . tom waddell , oesophagogastric randomised , waddell t , chau i , cunningham d , et al . 
lancet oncol 2013 ; 14 : 48189in this article , list of authors should have the read : ian chau , david cunningham , david gonzalez , alicia frances clare okines , andrew wotherspoon , claire sa ery , gary middleton , jonathan wadsley , david ferry , wasat mansoor , tom crosby , fareeda coxon , david smith , justin waters , timothy iveson , stephen falk , sarah slater , clare peckitt , yolanda barbachano . 
this correction has been made to the online version as of may 28 , 2013 . vol 14 june 2013 e254 4 gy versus 24 gy radiotherapy for patients with indolent lymphoma ( fort ) : a randomised phase 3 non - inferiority trial peter j hoskin , amy a kirkwood , bilyana popova , paul smith , martin robinson , eve gallop - evans , stewart coltart , timothy illidge , krishnaswamy madhavan , caroline brammer , patricia diez , andrew jack , isabel syndikus summary background follicular lymphoma has been shown to be highly radiosensitive with responses to doses as low as 4 gy in two fractions . 
this trial was designed to explore the dose response for follicular lymphoma comparing 4 gy in two fractions with 24 gy in 12 fractions methods fort is a prospective randomised , unblinded , phase 3 non - inferiority study comparing radiotherapy given as 4 gy in two fractions with a standard dose of 24 gy in 12 fractions . 
entry criteria included all patients aged over 18 years , having local radiotherapy for radical or palliative local control , with follicular lymphoma or marginal zone lymphoma , who had received no previous treatment for at least 1 month before . 
radiotherapy target sites were randomised ( 1 : 1 ) with minimisation strati ed by histology ( follicular lymphoma vs marginal zone lymphoma ) , treatment intent ( palliative or curative ) and centre . 
after a median follow - up of 26 months ( range 039754 ) , 91 local progressions had been recorded ( 21 in the 24 gy group and 70 in the 4 gy group )  . 
mucositis was the most common event in the 24 gy group ( two patients with acute mucositis and two with late mucositis ; all grade 3 ) and was not reported in the 4 gy group . 
 the most common acute e ect was pain at the site of irradiation ( two patients in the 4 gy group , one patient in the 24 gy group ; all grade 3 ) , and the most common late e ect was fatigue ( two patients in the 4 gy group , one patient in the 24 gy group ; all grade 3 )  . interpretation 24 gy in 12 fractions is the more e ective radiation schedule for indolent lymphoma and should be regarded as the standard of care . 
a large randomised study1 con rmed that a dose of 24 gy in 12 fractions was as e ective for local control as 40 gy in 20 fractions in terms of overall response and within eld progression . evidence for the e cacy of even lower doses has been reported over many years with the exquisite sensitivity of follicular lymphoma described using doses as low as 075 gy given as total body irradiation.2 an initial report3 of the use of 4 gy in two fractions in advanced indolent lymphoma was published in 1994 , with 89% of patients having a response . 
since then , several centres have reported similarly impressive high responses.4 the largest of these series comes from a study5 in the netherlands in which 96 patients with follicular lymphoma received 4 gy in two fractions . 
this study5 reported that 92% of patients had a response , with 61% achieving a complete response , and a median duration of complete remission of 42 months . against this background of an increasing number of studies con rming that 4 gy in two fractions was an e ective dose in the local treatment of follicular lymphoma , we did a randomised trial in patients receiving local external beam radiotherapy for control of follicular lymphoma , with the aim of showing that a lower dose of 4 gy in two fractions ( easier to give with hopefully fewer toxic e ects ) is as e ective in terms of local control as the standard 24 gy in 12 fractions . methods participants and study design the protocol for this study can be found online . 
the aim of the trial was to demonstrate that low - dose radiotherapy ( 4 gy ) is as e ective as conventional dose radiotherapy ( 24 gy ) in terms of tumour progression within the irradiated eld . 
as progression was to be assessed locally , it was decided that radiotherapy target sites would be randomised rather than patients , therefore individual patients could be randomly assigned more than once . treatment for control of patients were eligible for this study if they had a histologically con rmed diagnosis of follicular lymphoma and were to receive local radiotherapy with the aim of local control . 
initially , this trial was open only to patients local receiving palliative symptoms , but subsequently , protocol amendments allowed patients having radiotherapy for early stage localised disease in a curative setting to be included as well as those with marginal zone lymphoma . 
we excluded patients with histology results other than follicular lymphoma ( and later marginal zone lymphoma ) , those who had chemotherapy within 4 weeks of radiotherapy and a predicted prognosis of less than 3 months . the east of englandcambridge south research ethics committee reviewed the study and all patients provided written informed consent . randomisation and masking central randomisation was through the cancer research uk and university college london cancer trials centre using the minim6 progra sites were randomly assigned ( 1 : 1 ) to either 4 gy or 24 gy radiotherapy using minimisation strati ed by histology ( follicular lymphoma vs marginal zone lymphoma ) , treatment intent ( palliative vs curative ) and centre . 
we used no blinding since sham radiotherapy was not considered appropriate and followup was undertaken by the treating clinicians . procedures we delivered treatment using external megavoltage x - ray beams unless the lesion was super cial , when electrons or kilovoltage x - rays were allowed . 
 we treated some patients with ap - pa elds using orthogonal x - ray localisation whereas we treated most patients using 3d ct - based volume de nition and conformal beam arrangements . 
treatment was delivered using 2 gy per fraction , treating daily monday to friday . we monitored patients for acute toxic e ects before and during radiotherapy , and at 4 weeks after radiotherapy . 
 * flipi score was calculated using the stage ( worst seen at randomisation ) , baseline lactate dehydrogenase concentration , baseline hb , and number of nodal sites ( total seen , including earlier randomisations )  . 
 quality of life was recorded at each follow - up using the equation 5d ( eq - 5d ) health questionnaire . outcomes the primary outcome was time to local progression and was analysed on an intention - to - treat basis with all radiotherapy sites included . 
secondary endpoints were overall survival , response , toxic e ects , and quality of life . statistical analysis the study was designed as a non - inferiority trial to reliably exclude the chance that 4 gy might increase the rate of local progression at 2 years by more than 10% , which translates to the hr of 137 . at 2 years , we assumed that 60% of radiotherapy sites would be progression - free and using a one - sided 5% signi cance level and 90% power this requires 364 events ( a sample size of 650 target sites )  . we randomly selected the radiotherapy target site used in the analysis of overall survival ( each patient included only once ) before analyses were done . 
we used a cox proportional hazards model to estimate the hazard ratio ( hr ) between the the proportionality assumption using the schoenfeld residuals.7 all analyses were done with stata version 12.1. 
ph had full access to all of the data and the nal responsibility to submit for publication . results we randomly assigned 614 sites from 548 patients in 43 uk centres ( listed in the appendix ) to treatment groups vol 15 april 2014 299 allocated to radiotherapy 24 gy 315 allocated to radiotherapy 4 gy 3 did not receive trial radiotherapy 1 clinicians decision 1 treatment sites would overlap 1 patient too unwell 614 sites randomised 6 did not receive trial radiotherapy 1 emergency radiotherapy needed 1 patient refusal 1 did not want 24 gy 1 patient wanted a lower dose 1 surgery given , radiotherapy no 1 unknown ( missing treatment longer needed form ) 293 received trial radiotherapy 312 received trial radiotherapy 1 did not complete treatment ( patients choice after 6 gy ) 4 did not receive randomised dose 1 error ( received 8 gy ) 3 trial stopped , advised to switch groups 292 completed full protocol treatment 308 completed full protocol treatment 299 available for analysis * 315 available for analysis * 3 withdrew after treatment 296 available for follow - up 315 available for follow - up figure 1 : trial pro le all numbers refer to randomised sites , not patients . 
 * all radiotherapy target sites are included in the analysis of local progression ( the primary endpoint )  . the committee between april 7 , 2006 , and june 8 , 2011 , when the independent data monitoring ( idmc ) trial . 
although 94% of recommended halting recruitment had been completed , the idmc felt that the study question had been answered and patients should not be randomly assigned to a treatment believed to be inferior . 299 sites were randomly assigned to receive 24 gy and 315 sites to receive 4 gy . 
the medians seemed to di er between the two groups , with patients in the 24 gy group having longer times between diagnosis and randomisation than those in the 4 gy group ( 116 months vs 70 months ) , however , when we compared the distribution of the times further , we did not feel there was an imbalance . because of the sometimes lengthy periods between diagnosis and randomisation , patients had often received other treatments . 
151 ( 25% ) had received previous radiotherapy and 207 ( 34% ) previous chemotherapy ; these were also well balanced between the treatment groups ( table 1 )  . see online for appendix articles 482 tumour biopsies were reviewed centrally ; diagnoses could not be con rmed for 67 ( 14% ) of these samples ( 48 had insu cient material , 11 were reported to show no clear evidence of lymphoma , and another eight showed reactive changes only )  . 
of the 415 for which diagnoses were given , 386 ( 93% ) were follicular lymphoma and 46 ( 11% ) were marginal zone lymphoma ( table 1 )  . compliance with radiotherapy was very good ( gure 1 )  . 
 nine patients ( nine target sites ) were withdrawn before treatment started ; of target sites , 292 ( > 99% ) of the 293 sites in the 24 gy group and 308 ( 99% ) of the 312 sites in the 4 gy group received the complete , randomised dose . 
 the remaining stable disease ( including < 30% regression ) 22 ( 8% ) partial regression ( > 30% ) 53 ( 23% ) stable disease ( including < 30% regression ) 19 ( 8% ) 78 ( 32% ) 40 ( 16% ) all patients * complete regression partial regression ( > 30% ) progression total follicular lymphoma complete regression progression total marginal zone lymphoma complete regression partial regression ( > 30% ) stable disease progression total 24 gy 4 gy 176 ( 68% ) 137 ( 49% ) 60 ( 23% ) 90 ( 32% ) 44 ( 16% ) 2 ( < 1% ) 10 ( 4% ) 152 ( 67% ) 116 ( 48% ) 2 ( < 1% ) 9 ( 4% ) 24 ( 71% ) 7 ( 21% ) 3 ( 1 % ) 21 ( 55% ) 12 ( 32% ) 4 ( 11% ) 1 ( 3% ) data are number of sites ( % )  . 
 * patients who withdrew before treatment or with missing treatment data have been excluded , as have the three patients who switched from 4 gy to 24 gy after the trial was closed . 
there were also 43 ( 20 in the 24 gy group and 23 in the 4 gy group ) with no measurable disease at baseline and 17 ( 13 in the 24 gy group and four in the 4 gy group ) with missing response data . 
the exclusion of sites without measurable disease at baseline and those with missing response data showed that 236 ( 91% ) of 260 sites in the 24 gy group and 227 ( 81% ) of 281 in the 4 gy group had a complete or partial response ( p = 000095 )  . 
progressive disease was noted in more target sites in the 4 gy group than in the 24 gy group , but numbers in both groups were small ( two [ < 1% ] in the 24 gy group vs 10 [ 4% ] in the 4 gy group )  . 
although the marginal zone group was small ( and the di erence between 24 gy and 4 gy not signi cant , p = 071 ) the responses showed a similar pattern ( table 2 )  . we also looked at the subgroups of patients with early stage disease and those treated with curative intent . 
 although there were more responses , the di erence between the groups was slightly larger and remained statistically signi cant ( table 3 )  . after a median follow - up of 26 months ( 039754 ) , 91 local progressions had been recorded ( 21 in the 24 gy group and 70 in the 4 gy group ) giving an hr for time to local progression of 342 ( 95% ci 210557 , p < 00001 , gure 2a )  . 
although this is well below the 364 events required in the sample size calculation , it is not expected that longer follow - up will reduce the hr to a level that would meet the non - inferiority margin ( di erence in local progression - free interval at 3 years currently 198% ; 95% ci 278 to 134 )  . to explore the e ect of multiple randomisations within a patient , we did a sensitivity analysis using just one observation from each patient ( appendix )  . 
the hr was just below 1 in all samples , therefore there is currently no evidence to suggest that 4 gy has a negative e ect on overall survival . as patients often had more than one site of disease , many received additional anti - cancer therapies before local progression . 
this treatment was systemic therapy or radiotherapy either given to the target site for residual disease ( 12 patients ) or more often due to overlap with an adjacent site receiving radiation . 
this analysis reduced the number of events by seven , but the hr remained similar ( 373 ; 95% ci 223622 , p < 00001 )  . we did subgroup analyses for baseline size , treatment intent , karnofsky score , stage , time from diagnosis , and follicular lymphoma international prognostic index ( flipi ) score . 
we did not note any evidence of a di erence in treatment e ect within any of the subgroups ( appendix )  . we also tested the group of patients with con rmed follicular lymphoma treated with curative intent . 
this was a small group of only 134 patients ( 16 events ) but 4 gy remained inferior in terms of local progression ( hr 637 , 95% ci 1442818 , p = 00051 )  . toxic e ects were low , with just eight ( 3% ) sites in the 24 gy group and four ( 1% ) in the 4 gy group having grade 3 or 4 acute toxic e ects . 
a similar pattern was seen in late e ects with 105 sites ( 37% ) in the 24 gy group and 71 sites ( 23% ) in the 4 gy group a ected . we recorded quality of life using the eq - 5d form at 7 set timepoints and yearly thereafter , only patients with a single randomisation ( 228 in the 24 gy group and 239 in the 4 gy group ) were included in the analysis . 
we did not note any di erence between the two treatments ( p = 092 ; appendix )  . indolent b - cell non - hodgkin discussion our data suggest that , although 4 gy is an e ective dose local progression - free survival is inferior to a higher dose of 24 gy in 12 fractions . 
we noted no di erence in overall survival between groups ; however , these data are relatively lymphoma , 24 gy 4 gy number at risk 24 gy 4 gy time since randomisation ( months ) number at risk 24 gy 4 gy figure 2 : progression - free survival for all sites ( a ) and overall survival for one site per patient ( b ) immature , and we will re - analyse these data as further follow - up data are obtained and more events recorded . in our previous study1 of 24 gy compared with 40 gy in indolent lymphoma , 92% of patients had a response , similar to the 91% seen in this cohort , despite di erences in the populations : 62% of patients in the earlier study were treated with radical intent for stage one disease whereas in the current study , 60% of patients were treated with palliative intent and only 40% radically . 
while this is similar to the 91% in the 24 gy group , a striking , much larger , di erence is apparent in vol 15 april 2014 articles 24 gy 4 gy panel : research in context acute toxic e ects diarrhoea mucositis fatigue pain in target dry mouth oral candidiasis cerebrovascular ischaemia total late toxic e ects mucositis fatigue pressure sore constipation pharyngitis dry mouth total neutropenia and thrombocytopenia 1 * ( 04% ) any ( each patient only counted once ) 4 ( 13% ) 1 ( 04% ) 2 ( 07% ) 2 ( 07% ) 1 ( 04% ) 1 ( 04% ) 1 ( 04% ) 8 ( 28% ) 2 ( 07% ) 1 ( 04% ) 1 ( 04% ) 1 ( 04% ) 1 ( 03% ) 2 ( 07% ) 1 ( 03% ) 2 ( 06% ) 1 ( 03% ) 1 ( 03% ) 4 ( 13% ) any ( each patient only counted once ) 4 ( 14% ) all events were grade 3 , except where indicated . 
at the time of developing the protocol in 2004 , we did a formal literature search using medline and search terms follicular lymphoma , lymphoma , indolent lymphoma , low grade lymphoma , and radiotherapy . 
we identi ed no relevant randomised trials in the cochrane central register of controlled trials . interpretation the results of this trial con rm that 4 gy is e ective in many patients but that it is inferior to 24 gy in terms of time to local progression in both the radical and palliative setting when treating follicular lymphoma . 
4 gy has , however , a potential role as a simpler , shorter , and more pragmatic schedule in patients being treated for local control in the palliative setting , in which durable response might be less important . 
the proportion of patients with a complete response in previously published series of 4 gy in follicular lymphoma varied from 36% to 84% with a median value of 46% , 4 which is remarkably similar to that achieved in this study . 
it would seem reasonable therefore to propose that the di erence we noted between 4 gy and 24 gy regimens is real and that on balance , 24 gy in 12 fractions should be deemed the standard in this setting ( panel )  . both radical early stage and more advanced stage palliative patients were included in this study . 
however , in some patients with advanced disease and limited life span 4 gy is a very convenient and pragmatic alternative . the inclusion of marginal zone lymphoma in the latter part of the trial was a re ection of slow accrual at the time and was successful in signi cantly increasing the rate of patient entry . 
although it is di cult to draw any de nitive conclusions for marginal zone lymphoma as a distinct subgroup , the overall pattern of response was similar to that seen in follicular lymphoma and it would seem reasonable to conclude that 24 gy is better than 4 gy in this group as well , and should be considered the standard . the design of this trial allowed multiple sequential randomisations in one patient , which has been criticised in the past . 
however , we applied strict criteria to this approach ensuring response and toxic e ects were speci c to every site , and the results of the sensitivity analysis provide further reassurance that this feature did not compromise the results as presented here . 
premature closure of a trial is always a concern , however , the recommendation by the idmc in this case was as a result of mature data , the trial having been running for more than 5 years at the time of the decision and at the time of closure 94% of the planned accrual had been reached . despite the results of this trial , that a dose as low as 4 gy can achieve responses in a signi cant proportion of the population remains remarkable , and , indeed , more than 40% of sites were in complete remission after this dose . 
these events include apoptosis with inactivation of bcl - 2 overexpression , which is a characteristic of follicular lymphoma.8 this inactivation might result in overexpression of p53 and caspase - 8 and caspase - 9 . 
macrophage activation might also be upregulated.9 with such potent biological e ects within the cell , it is therefore tempting to suggest that a dose in excess of 4 gy , but much lower than 24 gy , could be optimum and further studies exploring intermediate doses might be of biological interest . toxic e ects with such low radiation doses are not a dose - limiting issue , unlike the situation in the radical treatment of epithelial cancers . 
however , we noted about half the incidence of acute grade 3 or higher toxic e ects in the 4 gy group compared with that in the 24 gy group . 
 this does not detract from the recommendation that 24 gy should be the standard treatment for indolent b - cell lymphoma , but supports the use of 4 gy for palliative treatment of patients with poor performance status . 
combination therapy using low - dose radiotherapy and other drugs that might similarly induce apoptosis , such as rituximab , could be of interest.10 in - vitro evidence suggests rituximab can enhance radiation - induced apoptosis in lymphoma cells and combination schedules with low - dose radiotherapy might therefore result in both optimum local control and carry the advantage of systemic e ects for more widespread disease control . contributors ph was chief investigator and lead author . 
ph , is , mr , eg - e , km , and cb were members of the trial management group and local principal investigators responsible for trial design , data collection , and interpretation . 
ti and sc were principal investigators , major contributors of data , and involved in interpretation , writing , and approval of report . declaration of interests we declare that we have no competing interests . acknowledgments we thank all patients , participating centres and sta , the lymphoma research trust , and members of the trials steering committee and independent data monitoring committee . this trial was funded by cancer research uk ( cruk / 05 / 015 ) and conducted by the cancer rresearch uk and ucl cancer trials centre . editorial see review page e321 for more on the childhood cancer survivor study see for the long - term health outcomes for childhood cancer survivors see jama 2013 ; 309 : 237181 for the childhood oncology group survivorship guidelines see survivorshipguidelines.org / for the study on mri monitoring of heart disease see j cardiovasc magn reson 2013 ; 15 : 48 for more on depression and anxiety in long - term cancer survivors see articles page 721 for more on improving cancer care for children and young people see thelancet.com / series / childhoodcancer it doesnt stop at cure : monitoring childhood cancer survivors on june 1213 , 2013 , the investigators of the childhood cancer survivors study met for their annual meeting in memphis , tn , usa . 
 the study included more than 1700 adults , with a median time from diagnosis of childhood cancer of 25 years , and showed that almost all participants had at least one chronic disease , including abnormal lung function , heart disease , and secondary malignancies . 
the investigators concluded that their ndings highlight the importance of monitoring survivors of childhood cancer for long - term health problems , but are current health systems and care pathways t for this purpose ? treatment in paediatric oncology has improved remarkably over the past half century . 
but , although measures are being taken to reduce long - term health risks at treatment stage , with less aggressive chemotherapy regimens and careful use of radiotherapy , there will probably always be some price to pay for cancer treatment . 
robust and regular monitoring of survivors could do much to help lessen the additional social , economic , and health burdens that many will face in the years after their treatment . 
 although there are initiatives taken to ensure survivors of childhood cancer are monitored and o ered support , these are generally institutional and regional e orts , with much of the onus put on the patient to use the resources provided , rather than health - care systems o ering them proactive support . 
the childhood oncology group have published a series of guidelines for clinicians who provide ongoing health care to survivors of childhood cancer , and recommends at least annual follow - up checks covering a range of conditions , such as growth , fertility , and secondary malignancies . 
although this is a start , there are two clear areas where monitoring of childhood cancer survivors could be improved . first , robust methods for monitoring should be developed , to ensure that medical interventions can be provided as early as possible . 
 furthermore , personalised screening programmes , such a breast - cancer screening for children who received chest irradiation , would be of further help to identify secondary malignancies early . regular second , improvements can be made receive in ensuring patients follow - up appointments . 
 although this seems obvious , as childhood cancer survivors grow up and move on with their lives , it may not be as straightforward as visiting a family doctor once a year . 
standardised record keeping and an easy way for survivors to be in control of their medical records , or improved mechanisms of ensuring records follow patients as they move from one health - care jurisdiction to another , can help prevent gaps in care over the years after cure . 
the establishment of specialist late - e ects clinics as part of a national cancer plan can also help to ensure regular monitoring is available no matter where a childhood cancer survivor ends up . 
furthermore , such clinics could ensure that those who are monitoring the survivors are highly trained and aware of the health risks that might a ect cancer survivors . besides monitoring the physical wellbeing of childhood cancer survivors , it is also important that their mental health is also attended to . 
 personalised , web - accessible survivorship programmes may o er a way to aid in this respect , allowing an easy way to document emotions and struggles on a regular basis , rather than as a single snapshot at an annual appointment . childhood cancer survivors are at long - term risk of substantial adverse events . 
follow - up should be centred on the individual , and information should be provided to survivors to help them understand how regular checkups can improve their long - term wellbeing and quality of life . 
 the lancet oncology vol 14 july 2013 correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections first - line selective internal radiotherapy plus chemotherapy versus chemotherapy alone in patients with liver metastases from colorectal cancer ( foxfire , sirflox , and foxfire - global ) : a combined analysis of three multicentre , randomised , phase 3 trials harpreet s wasan * , peter gibbs * , navesh k sharma , julien taieb , volker heinemann , jens ricke , marc peeters , michael findlay , andrew weaver , jamie mills , charles wilson , richard adams , anne francis , joanna moschandreas , pradeep s virdee , peter dutton , sharon love , val gebski , alastair gray , foxfire trial investigators , sirflox trial investigators , foxfire - global trial investigators , guy van hazel * , ricky a sharma * summary background data suggest selective internal radiotherapy ( sirt ) in third - line or subsequent therapy for metastatic colorectal cancer has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . 
the foxfire , sirflox , and foxfire - global randomised studies evaluated the efficacy of combining first - line chemotherapy with sirt using yttrium - 90 resin microspheres in patients with metastatic colorectal cancer with liver metastases . 
the studies were designed for combined analysis of overall survival . methods foxfire , sirflox , and foxfire - global were randomised , phase 3 trials done in hospitals and specialist liver centres in 14 countries worldwide ( australia , belgium , france , germany , israel , italy , new zealand , portugal , south korea , singapore , spain , taiwan , the uk , and the usa )  . 
chemotherapy - naive patients with metastatic colorectal cancer ( who performance status 0 or 1 ) with liver metastases not suitable for curative resection or ablation were randomly assigned ( 1 : 1 ) to either oxaliplatin - based chemotherapy ( folfox : leucovorin , fluorouracil , and oxaliplatin ) or folfox plus single treatment sirt concurrent with cycle 1 or 2 of chemotherapy . 
in foxfire , folfox chemotherapy was oxmdg ( oxaliplatin modified de gramont chemotherapy ; 85 mg / m oxaliplatin infusion over 2 h , l - leucovorin 175 mg or d , l - leucovorin 350 mg infusion over 2 h , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
in sirflox and foxfire - global , folfox chemotherapy was modified folfox6 ( 85 mg / m oxaliplatin infusion over 2 h , 200 mg leucovorin , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
randomisation was done by central minimisation with four factors : presence of extrahepatic metastases , tumour involvement of the liver , planned use of a biological agent , and investigational centre . 
the primary endpoint was overall survival , analysed in the intention - to - treat population , using a two - stage meta - analysis of pooled individual patient data . 
sirflox and foxfire - global are registered with clinicaltrials.gov , numbers nct00724503 ( sirflox ) and nct01721954 ( foxfire - global )  . findings between oct 11 , 2006 , and dec 23 , 2014 , 549 patients were randomly assigned to folfox alone and 554 patients were assigned folfox plus sirt . 
there were 411 ( 75% ) deaths in 549 patients in the folfox alone group and 433 ( 78% ) deaths in 554 patients in the folfox plus sirt group . 
the median survival time in the folfox plus sirt group was 226 months ( 95% ci 210245 ) compared with 233 months ( 218247 ) in the folfox alone group . 
in the safety population containing patients who received at least one dose of study treatment , as treated , the most common grade 34 adverse event was neutropenia ( 137 [ 24% ] of 571 patients receiving folfox alone vs 186 ( 37% ) of 507 patients receiving folfox plus sirt )  . 
serious adverse events of any grade occurred in 244 ( 43% ) of 571 patients receiving folfox alone and 274 ( 54% ) of 507 patients receiving folfox plus sirt . 
10 patients in the folfox plus sirt group and 11 patients in the folfox alone group died due to an adverse event ; eight treatment - related deaths occurred in the folfox plus sirt group and three treatment - related deaths occurred in the folfox alone group . interpretation addition of sirt to first - line folfox chemotherapy for patients with liver - only and liver - dominant metastatic colorectal cancer did not improve overall survival compared with that for folfox alone . 
after complete resection of liver metastases from metastatic colorectal cancer , approximately 3540% of patients survive for 5 years.5 the european organisation for research and treatment of cancer ( eortc ) intergroup clocc 400046 randomised study of the addition of radiofrequency ablation with or without surgery to chemotherapy in 119 patients with up to nine colorectal liver metastases , a significant effect on progression - free survival did translate into a significant overall survival benefit . is a at present , the proportion of patients eligible for surgical resection is only 20%.7 among the liver - directed therapies that might improve local control and increase downsizing of tumours to operability , selective internal leading technology.8 radiation therapy ( sirt ) sir - spheres y - 90 resin microspheres ( sirtex medical limited ; sydney , nsw , australia ) containing the - emitter yttrium - 90 ( y - 90 ) are delivered into the arterial supply of the liver under fluoroscopic guidance . 
the delivery of the resin microspheres into branches of the hepatic artery , which supplies the majority of blood to liver tumours , results in selective targeting by high - dose radiotherapy because the healthy liver is supplied predominantly by the portal venous system and therefore relatively spared from radiation exposure.9 research in context evidence before this study metastatic disease affects up to 50% of the more than one million patients diagnosed with colorectal cancer worldwide every year . 
the efficacy of sirt in third - line or subsequent therapy for metastatic colorectal cancer has been evaluated and there are data to suggest that sirt has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . 
we previously published a phase 1 / 2 trial that established the maximum tolerated dose of oxaliplatin - fluorouracil ( folfox ) chemotherapy to combine as concomitant radiosensitising chemotherapy with sirt . 
at the time of planning our studies in 2006 , we searched pubmed and web of science for articles published between jan 1 , 1980 , and may 31 , 2006 , with the search terms : colorectal cancer , colon cancer , rectal cancer , oxaliplatin chemotherapy , 5 - fluourouracil chemotherapy , fluoropyrimidine , selective internal radiotherapy , yttrium - 90 microsphere , radio - embolization , radio - embolisation , trans - arterial radio - embolization , liver metastasis , and hepatic metastasis original articles and review articles , published in english , were reviewed . 
no meta - analyses of sirt treatment of liver metastasis were identified at the time of protocol writing in 2006 . added value of this study the foxfire , sirflox , and foxfire - global , randomised clinical trials were designed to study whether sirt in combination with folfox chemotherapy as first - line therapy for metastatic colorectal cancer can improve overall survival compared with folfox alone . 
to our knowledge , the combined study represents the largest , randomised analysis performed in the field of interventional oncology to address the question of whether improved local control of colorectal liver metastases impacts on overall survival . 
despite higher proportions of patients achieving a response and improved liver - specific progression - free survival , the addition of sirt to first - line oxaliplatin - fluorouracil chemotherapy for patients with liver - only and liver - dominant metastatic colorectal cancer did not improve overall survival or progression - free survival . 
 additionally , to our knowledge , this study provides the most comprehensive account of the risk of adverse events which can occur secondary to sirt when it is used in combination with folfox chemotherapy . implications of all the available evidence because of the absence of overall survival benefit , early use of sirt in combination with first - line , oxaliplatin - fluorouracil - based chemotherapy in unselected patients with metastatic colorectal cancer cannot be recommended . 
careful patient selection and studies investigating the role of sirt as a post - chemotherapy consolidation therapy are required to define the role of sirt in treating metastatic colorectal cancer . 1160 vol 18 september 2017 articles chemotherapy with sirt , 10 building on our phase 1 / 2 trial , in which we established the maximum tolerated dose of oxaliplatin - fluorouracil ( folfox ) chemotherapy to combine as concomitant radiosensitising the foxfire , sirflox , and foxfire - global clinical trials were designed to study sirt in combination with folfox chemotherapy compared with folfox alone as first - line therapy for metastatic colorectal cancer.11 , 12 eligibility criteria and trial designs were pre - planned to be similar so that the three trials could be prospectively combined for analysis of overall survival and secondary endpoints . 
we previously reported that the combination of sirt with folfox in sirflox13 increased liverspecific progression - free compared with folfox chemotherapy alone , but there was no effect on overall progression - free survival . 
in this combined study , we sought to address the question of whether improved local control of colorectal liver metastases impacts on overall survival . survival methods study design and participants the foxfire , sirflox , and foxfire - global randomised , phase 3 trials were done in 14 countries ( australia , belgium , france , germany , israel , italy , new zealand , portugal , south korea , singapore , spain , taiwan , the uk , and the usa ) : in 28 hospitals and specialist liver centres for foxfire , 87 hospitals or centres for sirflox , and 69 hospitals or centres for foxfire - global ( appendix pp 2834 )  . 
two complementary trials were originally planned ( foxfire and sirflox ) , but the foxfire study took longer than anticipated to set up and recruit , so a third study ( foxfire - global ) was added as an independent trial . 
 liver - only or patients had to be eligible for systemic chemotherapy as first - line treatment for metastatic colorectal cancer.1114 eligibility criteria were similar between the three trials , but not identical . 
similarities and differences are highlighted in the combined study protocol paper.14 inclusion criteria included histologically confirmed colorectal cancer with liver - dominant metastases with or without the primary tumour in situ , who performance status of 0 or 1 , limited extrahepatic disease , age of 18 years or older , and life expectancy 3 months or longer . 
exclusion criteria included ascites , cirrhosis , or portal hypertension ( all established by clinical or radiological assessment ) ; thrombosis of the main portal vein ; and peripheral neuropathy grade 1 or worse . 
the protocols for foxfire and sirlox trials and for this combined study have previously been published.11 , 12 , 14 randomisation and masking in all three trials , patients were randomly assigned ( 1 : 1 ) to either folfox chemotherapy alone or folfox plus sirt with minimisation , based on the strata metastasis site ( liver - only vs liver plus extrahepatic metastases ) , extent of tumour involvement of the liver ( 25% vs > 25% measured objectively on baseline ct scan ) , planned use of a biological agent , and investigational centre . in foxfire , patients were allocated using minimisation with a probability of 08 to the treatment that most reduced the imbalance of the above factors . 
the first 30 treatments were allocated using ( simple ) block randomisation ( using variable block sizes of 2 , 4 , and 6 in a ratio of 1 : 2 : 1 )  . 
in sirflox and foxfire - global , an imbalance window of 5 was used ; if the treatment imbalance between the two groups was less than 5 , the treatment was randomly allocated . 
while the trial was in progress , access to the full randomisation lists was restricted to the database development manager at octo and the trial statistician at the centre for statistics in medicine ( csm ; oxford , uk )  . 
in sirflox and foxfire - global , randomisation was done centrally at the national health and medical research council clinical trials centre ( camperdown , nsw , australia ) via an interactive voice response syste participants were enrolled by the investigators in all three trials . 
as none of the trials were masked , once patients were allocated to treatment , participants , all members of the trial team , and treating medical staff knew the treatment allocation . procedures in foxfire , systemic folfox chemotherapy consisted of oxmdg ( oxaliplatin modified de gramont chemo therapy ; 85 mg / m oxaliplatin infusion over 2 h , l - leucovorin 175 mg or d , l - leucovorin 350 mg infusion over 2 h , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
systemic folfox chemotherapy in sirflox and foxfire - global consisted of modified folfox6 ( 85 mg / m oxaliplatin infusion over 2 h , 200 mg leucovorin , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
 in foxfire , protocol chemotherapy was 12 cycles ; in sirflox and foxfire - global , protocol chemotherapy continued until disease progression or dose - limiting see online for appendix vol 18 september 2017 1161 articles toxicity . 
the oxaliplatin dose was reduced from 85 mg / m to 60 mg / m for three cycles from the cycle coinciding with sirt administration and for two cycles thereafter , based on phase 1 / 2 data.10 dose modifications were permitted in line with standard care ( appendix pp 38 )  . 
we used the patients body surface area , percentage of tumour involvement , and magnitude of liver - to - lung shunting to establish the activity ( gbq ) per dosing chart.12 planned sirt was done on cycle 1 day 3 or 4 or cycle 2 day 3 or 4.10 in foxfire , patients could receive anti - vegf ( eg , bevacizumab ) or anti - egfr ( eg , cetuximab ) from cycle 1 in the folfox alone group and from cycle 7 onwards in the folfox plus sirt group . 
the addition of anti - vegf or anti - egfr treatments to protocol therapy was at the discretion of the treating physician and doses prescribed were according to local policy at the treating centre . foxfire - global , patients could we assessed patients by ct scan every 812 weeks until hepatic progression . 
follow - up assessments included clinical assessment ; ct of chest , abdomen , and pelvis ; and health related quality - of - life ( hrqol ) assessment.11 , 12 , 14 scans were independently reviewed by pharmtrace ( berlin , germany ) for overall and hepatic progression in foxfire using response evaluation criteria in solid tumors ( recist ; version 1.0 ) and in sirflox with recist ( version 1.0 ) with minor modifications.13 independent reviews were not done in foxfire - global . 
all patients were followed up until death or for a minimum of 2 years . health - related quality of life was assessed with the euroqol - 5d three - level questionnaire ( eq - 5d - 3l ) , a generic hrqol instrument15 measuring health in five dimensions ( mobility , self - care , usual activities , pain or discomfort , and anxiety or depression ) , which summarised as a utility score.16 the eq - 5d - 3l was administered during clinic visits at baseline , between the second and the third months after randomisation , at 6 months , at 12 months , and once per year until 60 months from the start of protocol treatment . 
grading of adverse events used the national cancer institute common terminology criteria for adverse events ( version 3 )  . outcomes the primary outcome of this analysis was overall survival , defined as the time from randomisation to death from any cause , with patients who were still alive censored at their last known follow - up date . 
the proportion of patients achieving an objective response in each treatment group was defined as the number of patients achieving a complete or partial response at any point during the trial , up to their first occurrence of hepatic resection , over the number randomised in that group ( early deaths by any cause and unknown responses were included in the demominator )  . 
 the percentage resected in each group was defined as the number of patients who underwent a hepatic resection divided by the number randomly assigned to that group . for progression - free survival or liver - specific progression - free statistical analysis for the primary combined overall survival analysis , a sample size of 810 was originally calculated , but subsequently updated to 1075 patients ( 710 deaths ) using a protocol - specified hazard ratio ( hr ) of 08 , with a control group median overall survival of 197 months and sirt group median overall survival of 246 months , two - sided 5% significance , 80% power , and allowing for 5% noncompliance.14 the updated sample size allowed for a higher median overall survival , the addition of biological agents to protocol chemotherapy ( planned use added as a stratification factor to the randomisation in may , 2011 , for foxfire and sirflox , and incorporated in foxfireglobal since set - up ) and crossover in both directions . 
the study also had 80% power to detect a 6 - month overall survival benefit in the subgroup of patients with metastatic disease restricted to the liver : 708 patients ( 463 deaths ) were needed . 
the cutoff for analysis was chosen such that there was a minimum of 710 deaths overall and 463 deaths in the liver - only subgroup ( assuming a 6 - month increase in overall survival in the sirt - treated , liver - metastasisonly patients ) and a minimum follow - up of 2 years since 1162 vol 18 september 2017 articles the last patient was randomly assigned to treatment . 
 we did two interim toxicity and safety analyses with the combined data from the foxfire and sirflox trials 8 months after at least 80 patients were randomly assigned ( 40 patients per trial ) and 8 months after 300 were randomly assigned ( minimum of 120 patients per trial ) ; foxfire - global was not included in the interim analyses on the combined data . we calculated median follow - up time using the reverse kaplan - meier method . 
we did all efficacy analyses on an intention - to - treat basis per the published statistical analysis plan.14 we estimated overall survival and progression - free survival for each trial using kaplan - meier survival curves , unadjusted log - rank tests , and cox proportional hazards the proportionality survival models . 
hrs for overall survival and progression - free survival from the individual trials were combined using a two - stage , fixed - effect , inverse - variance weighted individual participant data meta - analysis approach.17 the i statistic indicates the proportion of variation in the treatment effect that is due to heterogeneity rather than chance . 
we also estimated causespecific hazards.19 for overall survival , progression - free survival , and liver - specific progression - free survival , we investigated the potential treatment benefit in patients presenting with disease confined to the liver using survival models stratified by trial ( prespecified subgroup analysis )  . 
 the odds of patients having a resection or achieving a response ( overall and liver - specific ) were compared between treatment groups by pooling individual trial odds ratios ( or ) using two - stage individual participant data meta - analysis . 
 a minimum clinically significant difference in eq - 5d scores of 008 has been suggested across all cancers.20 we used analysis of covariance to analyse differences in eq - 5d - 3l utility scores between the two treatment groups , adjusted for eq - 5d - 3l baseline values . 
we made post - hoc comparisons between treatment groups of treatment received after protocol therapy using the mantel - haenszel test , stratifying by trial . we did safety analyses on patients who received at least one dose of chemotherapy in either group and on an astreated basis . 
we included adverse events reported up to 28 days after the end of trial treatment or 7 months after foxfire 1282 discussed at mdt meeting or screened sirflox 561 screened foxfire - global 240 screened 31 failed screening 31 failed screening 918 excluded 712 did not meet inclusion or exclusion criteria 110 patient refusal 96 other reason 364 randomly assigned 530 randomly assigned 209 randomly assigned 182 assigned oxmdg 263 assigned mfolfox6 104 assigned mfolfox6 267 assigned mfolfox6 plus sirt 105 assigned mfolfox6 plus sirt 182 assigned oxmdg plus sirt 179 started folfox chemotherapy 180 started folfox chemotherapy 167 sirt given 252 started folfox chemotherapy 263 started folfox chemotherapy 247 sirt given 102 started folfox chemotherapy 102 started folfox chemotherapy 93 sirt given 1103 included in individual participant data analysis * 549 folfox chemotherapy group 554 folfox chemotherapy plus sirt group figure 1 : trial profile oxmdg and mfolfox6 are equivalent oxaliplatin - fluorouracil - based folfox chemotherapy regimens . 
discontinuation data were available for patients in foxfire and for a subset of patients in sirflox , but were not available for patients in foxfire - global . vol 18 september 2017 1163 articles folfox alone ( n = 549 ) folfox plus sirt ( n = 554 ) folfox alone ( n = 549 ) folfox plus sirt ( n = 554 ) age at randomisation ( years ) 627 ( 231890 ) 634 ( 284896 ) ( continued from previous column ) 14 ( 0923 ) 14 ( 0923 ) extrahepatic metastases status 12 ( 0818 ) 12 ( 0718 ) extent of liver involvement time since diagnosis of primary tumour to randomisation ( months ) time since diagnosis of liver metastases to randomisation ( months ) who performance status primary tumour site not categorisable * primary tumour in situ male female missing missing colon rectum missing missing 361 ( 66% ) 187 ( 34% ) 1 ( < 1% ) 347 ( 63% ) 200 ( 36% ) 2 ( < 1% ) 392 ( 71% ) 137 ( 25% ) 8 ( 1% ) 12 ( 2% ) 302 ( 55% ) 246 ( 45% ) 1 ( < 1% ) 363 ( 66% ) 191 ( 34% ) 354 ( 64% ) 198 ( 36% ) 2 ( < 1% ) 421 ( 76% ) 116 ( 21% ) 5 ( 1% ) 12 ( 2% ) 278 ( 50% ) 275 ( 50% ) 1 ( < 1% ) previous adjuvant chemotherapy 28 ( 5% ) 31 ( 6% ) 520 ( 95% ) 523 ( 94% ) missing 1 ( < 1% ) metastases present at initial diagnosis yes ( synchronous ) no ( metachronous ) missing 475 ( 87% ) 71 ( 13% ) 3 ( 1% ) 483 ( 87% ) 68 ( 12% ) 3 ( 1% ) ( table 1 continues in next column ) randomisation , whichever was earlier ( deemed the safety window )  . 
 * site of primary tumour recorded as both colon and rectum ; the only options in foxfire were colon or rectu minimisation factors ; treating site was also a minimisation factor . 
extrahepatic disease permitted as per trial protocols were foxfire : no more than five metastases in the lung and metastases should have been , in the opinion of either the local multidisciplinary team meeting or after central review of scans arranged via the trials office , amenable to future definitive local therapy , in addition to lung metastases , a single site of other extrahepatic disease was permitted ( eg , multiple lymph nodes in one lymph node region ) after approval by the trials office ; for sirflox and foxfire - global : limited extrahepatic metastases in the lung , lymph nodes , or both were permitted , no more than five nodules in the metastases in the lung were allowed , which were no more than 1 cm in diameter or up to 17 cm in diameter per single lesion ; involvement of lymph nodes in one single anatomic area ( pelvis , abdomen , or chest ) was permitted provided their longest diameter measured less than 2 cintention to treat with a biological agent was not a minimisation factor for these patients because it was introduced after these patients entered the study . table 1 : baseline characteristics of participants in the combined study nct00724503 ( foxfire - global )  . ( sirflox ) and nct01721954 role of the funding source the sponsor had no role in the foxfire study design , data collection , or data analysis . 
jmo , pd , psv , and sl had full access to all of the data in the study and the corresponding author had final responsibility for the decision to submit for publication . results between oct 11 , 2006 , and dec 23 , 2014 , 1103 patients were enrolled and randomly assigned to either folfox chemotherapy ( n = 549 ) or folfox plus single treatment sirt ( n = 554 ) ( figure 1 )  . 
end of follow - up was oct 31 , 2016 , for foxfire , june 1 , 2016 , for sirflox , and nov 30 , 2016 , for foxfire - global , ensuring 2 years of follow - up after the last patient was enrolled ( appendix p 13 )  . 
median followup was 433 months ( iqr 316584 )  . in the first 12 cycles of treatment , 3193 ( 59% of 5369 ) oxaliplatin cycles in the folfox plus sirt group and 3608 ( 68% ) of 5344 cycles in the folfox alone group were at full protocol dose . 
the median number of cycles of folfox treatment was 12 ( iqr 713 ) in the folfox plus sirt group and 12 ( 715 ) in the folfox alone group . 
 in foxfire , 13 ( 4% ) of 364 patients received cetuximab ( four in the folfox plus sirt group and nine in the to 197 folfox group )  . 
after finishing protocol therapy , fewer patients in the folxfox plus sirt group were given irinotecan , fluoropyrimidine , anti - vegf , or anti - egfr systemic therapies upon progression than were patients in the folfox alone group ( appendix p 16 )  . 
66 ( 12% ) of 549 patients randomly assigned to the folfox alone group received sirt in a later course of therapy , whereas 47 ( 8% ) of 554 patients randomly assigned to sirt did not receive sirt . there were 844 ( 77% ) deaths in 1103 patients in the intention - to - treat population over the follow - up period : 296 ( 81% ) deaths in 364 patients in foxfire , 424 ( 80% ) in 530 patients in sirflox , and 124 ( 59% ) in 209 patients in foxfire - global . 
 the median survival time in the folfox plus sirt group was 226 months ( 95% ci 210245 ) compared with 233 months ( 218247 ) in the folfox alone group ; the pooled hr was 104 ( 95% ci 090119 , p = 061 ; figure 2a , c )  . 
sirt = selective internal radiotherapy . ( 261 [ 73% ] of 358 patients in the folfox group , median overall survival 246 months , 95% ci 221264 ; 264 [ 74% ] of 355 patients in the folfox plus sirt group , 245 months , 223263 ; pooled hr 100 , 95% ci 085119 , p = 096 )  . 
in a sensitivity analysis of overall [ 11% ] of survival excluding ineligible patients ( 62 549 patients in the folfox group and 60 [ 11% ] of 554 patients in the folfox plus sirt group were ineligible ; reasons for ineligibility not reported ) , there were 360 deaths ( 74% ) in 487 patients in the folfox group and 382 deaths ( 77% ) in 494 patients in the folfox plus sirt group . 
median overall survival was 239 months ( 95% ci 218250 ) in the folfox group and 234 months ( 218252 ) in the folfox plus sirt group ; pooled hr was 101 ( 95% ci 088117 , p = 086 )  . 
 subgroup comparisons for overall survival of the prespecified subgroups metastatic site , liver involvement , age , sex , who performance status , and tumour in situ , and the post - hoc subgroups primary tumour site , bevacizumab administration , and timing of metastasis are shown in figure 3 . 941 ( 85% ) of 1103 patients had an observed radiological progression or died before progression : 304 ( 84% ) of 364 patients in foxfire , 452 ( 85% ) of 530 patients in sirflox , and 185 ( 89% ) of 209 patients in foxfireglobal . 
progression - free survival was not significantly different between treatment groups ( pooled hr 090 , 95% ci 079102 , p = 011 ; figure 2b , d )  . 
the median progression - free survival in the folfox plus sirt group was 110 months ( 95% ci 102118 ) compared with 103 months ( 97109 ) in the folfox alone group . 
similar results were found in the pre specified subgroup analysis restricted to patients with liver - only metastatic colorectal cancer at baseline ; 297 ( 83% ) of 358 patients in the folfox group had progressed or died in the liver - only subgroup analysis ( median progressionfree survival 111 months , 95% ci 100121 ) ; 292 ( 82% ) of 355 patients in the folfox plus sirt group had progressed or died ( 119 months , 110138 ; hr 086 , 95% ci 073101 , p = 0066 )  . 
the results of a prespecified sensitivity analysis using radiological scan data as reported by sites from all three trials were consistent with the analysis of the centrally reviewed data ( hr 091 , 95% ci 080103 , p = 015 )  . in 271 ( 49% ) of 549 patients in the folfox and 173 ( 31% ) of 554 patients in the folfox plus sirt group , first progression events were radiologically observed in the liver ( figure 4a )  . 
the cumulative incidence of first progression in the liver was lower in the folfox plus sirt group than the folfox alone group ( figure 4a ; appendix p 17 )  . 
the cumulative incidence of progression within the liver in the first 12 months of follow - up was 22% ( 95% ci 1926 ) in the folfox plus sirt group and 39% ( 3543 ) in the folfox alone group . 
in 196 ( 36% ) of 549 patients in the folfox group and 301 ( 54% ) of 554 patients in the folfox plus sirt group , first progression was extrahepatic or death occurred before recorded radiological progression ( figure 4b , appendix p 17 )  . 
table shows grade 3 or worse haematological events occurring in at least 5% of patients , grade 3 or worse non - haematological events occurring in at least 5% of patients , and all sirt - associated adverse events . 
sirt = selective internal radiotherapy . table 2 : adverse events reported in each treatment group sirt group than in the folfox alone group ( figure 4b ; appendix p 17 )  . 
the cumulative incidence of progression outside the liver or death before recorded radiological progression in 12 months of follow - up was 33% ( 95% ci 2937 ) in the folfox plus sirt group and 19% ( 1623 ) in the folfox alone group . 
cause - specific hrs were in the same direction as , and of similar magnitudes to , the subdistribution hrs ( appendix p 17 )  . an objective ( complete or partial ) response over the study duration was achieved in 746 ( 68% ) of 1103 patients ; 400 ( 72% ) of 554 in the folfox plus sirt group and 346 ( 63% ) of 549 in the folfox alone group ( pooled or 152 , 95% ci 118196 , p = 00012 ; appendix pp 10 , 17 )  . 
an objective response was observed in more patients in the folfox plus sirt group than in the folfox alone group in each of the individual trials ( appendix p 17 )  . 
the odds of achieving an objective response in the liver were also higher in the folfox plus sirt group than in the folfox alone group ( pooled or 178 , 95% ci 137231 , p < 00001 ; appendix p 18 )  . vol 18 september 2017 1167 articles over the follow - up period , 182 ( 17% ) of 1103 patients had at least one hepatic resection . 
overall , 94 ( 17% ) of 554 patients in the folfox plus sirt group and 88 ( 16% ) of 549 patients in the folfox alone group had a resection . 
the odds of undergoing a resection were not significantly different between treatment groups ( pooled or 107 , 95% ci 078148 , p = 067 ; appendix p 11 )  . the proportion of patients who had a grade 3 or worse adverse event at each treatment cycle by treatment group , overall and for haematological adverse events , non - haematological adverse events , and neutropenia are shown in the appendix ( p 12 )  . 
of 1078 patients who received at least one dose of study treatment in the astreated population , 755 ( 70% ) had a grade 3 or worse adverse event ( up to 28 days after the end of protocol chemotherapy or the first 7 months after randomisation , whichever was earlier ) ; 375 ( 74% ) of 507 patients in the folfox plus sirt group and 380 ( 67% ) of 571 patients in the folfox alone group ( table 2 )  . 
the odds of a patient having a grade 3 or worse adverse event were higher in the folfox plus sirt group than in the folfox alone group ( pooled or 142 , 95% ci 109185 , p = 00089 , appendix p 13 )  . 
 of 507 patients who received sirt , 231 ( 46% ) had a haematological grade 3 or worse adverse event , whereas 165 ( 29% ) of the 571 patients who did not have sirt had a haematological grade 3 or worse adverse event , the most frequent being neutropenia ( 186 [ 37% ] in the folfox plus sirt group vs 138 [ 24% ] in the folfox alone group ; table 2 )  . 
adverse events of grade 1 or 2 occurring in 10% of patients or more and all grade 3 or worse events are shown in the appendix ( pp 1826 )  . 
 in foxfire , 15 ( 8% ) of 182 patients in the folfox group and 25 ( 14% ) of 182 patients in the folfox plus sirt group discontinued treatment because of an adverse event or serious adverse event ; data were not fully available for sirflox and not available for foxfire - global . 
serious adverse events of any grade occurred in 244 ( 43% ) of 571 patients receiving folfox alone and 274 ( 54% ) of 507 patients receiving folfox plus sirt ( appendix p 27 )  . 
10 patients in the folfox plus sirt group and 11 patients in the folfox alone group died due to an adverse event during the main safety window ( appendix p 26 )  . 
of the eight treatment - related deaths in the folfox plus sirt group , three deaths due to radiation - induced complications of surgery , one due to liver failure , one due to drug - induced pneumonitis , and one due to offtarget delivery of microspheres . 
there were three treatment - related deaths in the folfox alone group : one due to complications of surgery , one due to neutropenic sepsis , and one due to bowel perforation . 
average unadjusted eq - 5d - 3l utility scores were not significantly different between treatment groups at any time point except at 23 months ( appendix p 27 ) ; however , this difference would not be deemed clinically meaningful . discussion the foxfire , sirflox , and foxfire - global randomised studies designed to definitively assess the combination of sirt with folfox versus folfox alone for colorectal liver metastases in the first - line setting have not shown a benefit of adding sirt on overall survival . 
the combined analysis of these three randomised clinical that a global , multidisciplinary trial involving a complex liver - directed therapy can be done with adequate power to answer an important clinical question . trials shows the efficacy of sirt in third - line or subsequent therapy for metastatic colorectal cancer ( ie , salvage therapy of chemotherapy - refractory disease ) has previously been evaluated.21 a randomised trial22 of salvage in patients with metastatic colorectal cancer with liver - confined disease showed a significant benefit of chemotherapy plus sirt versus chemotherapy alone in time to progression . 
these data suggest that sirt has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . in our study , metastatic colorectal cancer in which the liver is the only site of disease occurs frequently in a subset of patients ; some of these patients can be resected with long - term cures.23 the significant improvement in liver disease control assessed by competing risk analyses did not translate to a benefit in overall survival . 
the absence of benefit of the addition of sirt to folfox on progression - free survival and overall survival in our combined study could be partly explained by the high proportion of patients who developed first progression at an extrahepatic site , independently of whether the metastases were liver - only at baseline or whether there were extrahepatic metastases or primary tumour in situ at baseline . 
despite the better liver control in the folfox plus sirt group compared with the folfox alone group , this observation of extrahepatic progression might also explain the absence of a 1168 vol 18 september 2017 articles in the groups significant difference between the frequency of surgical resection of the liver metastases being done during or after protocol therapy . 
to avoid possible ascertainment bias in interpreting responses and difficulties differentiating disease progression from radiation reaction of the hepatic parenchyma in patients undergoing liver interventional procedure , scans were centrally reviewed by independent readers . 
the absence of an overall survival benefit suggests that early use of sirt in combination with firstline recommended in unselected patients with metastatic colorectal cancer . oxaliplatin - based chemotherapy radiotherapy cannot the in our study , the sirt - treated patients had a similar quality of life to the patients who had chemotherapy only . 
in the as - treated population in the folfox plus sirt group ( n = 507 patients ) , hepatic failure resulted in death of one patient during the main safety window and death of a further two patients during extended follow - up . 
this study provides the most comprehensive account of the risk of adverse events that might occur secondary to sirt when used in combination with folfox chemotherapy . one possible limitation of our study is that significant changes to the management of metastatic colorectal cancer occurred during the 8 - year recruitment period with the introduction of bevacizumab and egfr inhibitors as first - line standards of care , and increased use of liver interventions such as surgery and ablation . 
the non - identical design of the individual trials might also be considered a limitation , but is accounted for by the use of appropriate statistical methods . little progress has been reported in improving overall survival in molecularly unselected populations since the crystal , prime , and tribe studies.2427 in our study , crossover was anticipated and 12% of patients randomised to folfox alone received sirt with a later line of therapy . 
furthermore , 8% of patients assigned to sirt did not receive sirt , a proportion consistent with our previously published data in patients with metastatic colorectal cancer.13 the difference in exposure to posttrial treatments between the two treatment groups might have affected the primary endpoint . 
it is possible that the improved liver disease control observed in the folfox plus sirt group might have influenced physicians to bias towards intensive subsequent treatment , particularly as so - called treatment - holiday strategies were evolving during the recruitment and follow - up periods of less these trials . 
alternatively , it could be postulated that the reduced use of irinotecan after protocol therapy might have been related to increased or prolonged toxicities in the patients in the folfox plus sirt group , including the risk of myelosuppression . 
our analysis of these toxicities for both groups over time showed an apparent increase of grade 3 or worse adverse events in the folfox plus sirt group , particularly haematological events , with the curves gradually converging after 6 months of protocol therapy . in the past decade , the focus of clinical trials has been on improving outcomes for selected biological subtypes in metastatic colorectal cancer with predefined molecular criteria ( eg , mutant ras or braf )  . 
several studies from the past 2 years have reported that patients with rightsided primary tumours have worse survival outcomes and it is possible that these patients benefit less from standard therapies.2830 molecular subtypes in our study are not currently available , but in the dataset available , 179 ( 25% ) of 718 patients had right sided - tumours . 
further analyses are underway to investigate this exploratory finding , with specific scrutiny of ras mutation , braf mutation , and tumour location in study populations who have received sirt in clinical trials . 
 further studies designed to define the potential benefit of sirt to treat colorectal liver metastases from rightsided primaries are warranted . improved radiological response , in conclusion , despite better liver - specific disease control and the foxfire prospective trials did not show a benefitof the combination of sirt with folfox for progression - free survival or overall survival . 
further studies are needed to study the role of sirt in carefully selected patient populations and as a consolidation therapy after chemotherapy . contributors hsw , pg , sl , vg , ag , gvh , and ras designed the study and wrote the protocol . 
hsw , pg , nks , jt , vh , jr , mp , mf , aw , jmi , cw , ra , af , jmo , psv , pd , sl , vg , ag , gvh , and ras interpreted the data , wrote the manuscript , and approved the paper . declaration of interests hsw reports grants , personal fees , non - financial support , and other uncompensated work from sirtex medical and merck serono ; personal fees and non - financial support from celgene ; grants and non - financial support from pfizer ; personal fees and non - financial support from roche and lily outside the submitted work . 
pg reports personal fees from sirtex ; grants and personal fees from roche , amgen , pfizer , merck , bayer , and servier , during the conduct of the study . 
vh vol 18 september 2017 1169 articles reports grants , personal fees , and non - financial support from sirtex medical , merck , and roche , during the conduct of the study ; involvement in a scientific project on radiological imaging from sirtex medical ; grants , personal fees , and non - financial support from merck and roche ; grants and non - financial support from amgen ; grants and personal fees from sanofi ; grants from pfizer and boehringer ingelheim ; and personal fees from bristol - myers squibb , msd , and novartis , outside the submitted work . 
jmi reports personal fees from sirtex medical , during the conduct of the study ; grants from sirtex medical ; and personal fees from sirtex medical , astellas , jannessen , lily , and roche , outside the submitted work . 
jmo reports grants from cancer research uk and sirtex medical , during the conduct of the study ; and non - financial support from sirtex medical , outside the submitted work . 
pd reports grants from cancer research uk and sirtex medical , during the conduct of the study ; and non - financial support from sirtex medical , outside the submitted work . 
gvh reports personal fees and non - financial support from sirtex medical , during the conduct of the study ; and personal fees and non - financial support from sirtex medical , outside the submitted work . 
ras is a consultant for and reports grants and personal fees from sirtex medical and btg , during the conduct of the study ; and reports personal fees from affidea , astrazeneca , boston scientific , cancer research technology , eisai , terumo , and varian , outside the submitted work . 
aw declares no competing interests . acknowledgments the foxfire study design was reviewed and endorsed by the clinical trials awards and advisory committee of cancer research uk , was approved by the national research ethics service committee south central - berkshire ( research ethics committee reference 09 / h0505 / 1 ) , was developed by the national cancer research institute colorectal clinical study group and the national institute for health research clinical research network and equivalents in devolved nations , and was sponsored by the university of oxford . 
we thank georgie perry for secretarial support . editorial for more on framework convention on tobacco control see editorial lancet 2017 ; 389 : 226 chinas health trajectory in 2017 jan 28 , 2017 , was the start of chinese new yearthe year of the rooster . 
in the coming lunar year , china faces some big challenges that will rely on these characteristics : a rapidly ageing population ; unprecedented pollution manifesting in the highest levels of smog on record ; strained sino - american relations ; and an unusually large government reshu e with ve of seven members of the standing committee retiring and more than half of the central committee standing down . 
all of these events will likely have notable e ects on health care and cancer control policies in the years ahead . chinas position as the worlds most populous state will soon be overtaken by india . 
the communist partys maxim of more people , more power has been undermined by the four - decade social experiment in state - organised population controlmade infamous by the controversial one - child policy implemented in 1978 . 
by 2020 , china is projected to have a population of about 14 billion people , with the demographic then shifting rapidly towards a much older society , similar to that already seen in japan and elsewhere in asia . 
the 2015 abolition of the one - child policy will take many generations to shift the population back to a healthier balance between young and old , male and female , leaving the country in a perilous position in the meantime . 
major non - communicable diseases , such as cancer , diabetes , and heart disease , are mainly seen in older people , but does china have the health - care structure , or future - proof plans , to cope with the challenge of an ageing population ? the solution will lie in a need for much greater levels of screening and prevention coupled to increased provision of acute secondary and tertiary care . 
 chinas decision to increase availability of family doctors , to invest in cancer screening trials , to build 100 specialist lung cancer hospitals , and to train 1000 new lung cancer experts , is a good step forward . 
and with strained relations with the usa , which imports nearly us$500 billion worth of goods from china , any decrease in this trading partnership during the trump administration could inversely a ect the countrys ability to fund these policies . despite important inroads in to controlling lung cancer incidence via the implementation of the framework convention on tobacco control , china remains the largest consumer and producer of tobacco products , and a quarter of the populationabout 300 million peopleare smokers , and more than 730 000 new cases of lung cancer still occur annually . 
in january 2017 , smog in some cities was 40 times higher than the whos recommended safe limits , and these levels will be further exacerbated by a government decision to invest in 200 new coal - burning power plants . 
the revised environment protection law , enacted in 2015 as part of chinas long - running blue skies , green land , and clear running water strategy , introduced harsher punishments for polluters , but the unrelenting downward trends suggest much is still needed to be done . of equal importance in the coming year , china needs to extend measures that rehabilitate the role of doctors in society ; to continue support for evidence - based medicine ; and to eliminate violence against health professionals . 
certainly , government policies of the past , such as the imposition of intrauterine devices as birth control for many women , have not helped public perceptions of doctors , giving them the appearance of government agents of oppression rather than providers of a highly valuable and skilled service for the betterment of society . 
elimination of the one - child policy is a positive step in depoliticising the medical profession , as are recommendations that hospitals hire security guards , a review of doctors salaries , and criminalisation of such violence , but more is needed to eliminate patient dissatisfaction , refocus unrealistic expectations , and recoup out - of - pocket expensesall factors attributed to the increases in violence . 
 many countries face major political upheavals in 2017 , but against these destabilising forces , china must apply some of the characteristics of the rooster : observant of the populations health - care needs , and resourceful and courageous in continuing and expanding its ongoing commitment to health - care reforms , regardless of external events beyond its borders . 
 the lancet oncology vol 18 february 2017 regarding survival and 35 years ( 3045 ) for overall survival ( median follow - up 34 years [ 2943 ] for the sodium thiosulfate group , and 38 years [ 3145 ] for the control group ) ; and localised and sentences disseminated disease should have read localised among participants with disease , 14 events in the sodium thiosulfate group , 13 events in the control group , and six deaths in both the control and sodium thiosulfate groups occurred and in participants with disseminated disease , 12 events and 11 deaths occurred in the sodium thiosulfate group and 11 events and four deaths occurred in the control group . 
these corrections have been made to the online version as of june 2 , 2017 . correction to lancet oncol 2017 ; 18 : 71931 registry international cancer , steliarova - foucher colombet m , ries lag , et al , and the iicc - 3 incidence contributors . 
 lancet oncol 2017 ; 18 : 71931 in this article , the coverage of the population of east asia in table 1 in the age 014 years column should have been 44% , and in the age 1519 years column , 40% . 
 consequently , the fourth sentence in the first paragraph of the results read approximately should have the world population 114% of aged ( contributing years 18 376 710 144 person - years ) was covered by the registries included in our study , ranging from 17% in south asia ( india ) to 994% in north america ( table 1 )  . 
these corrections have been made to the online version as of june 2 , 2017 , and the printed article is correct . 014 correction to lancet oncol 2017 ; 18 : 812 versus gronchi a , ferrari s , quagliuolo v , et al . 
histotype - tailored neoadjuvant chemotherapy standard chemotherapy in patients with high - risk soft - tissue sarcomas ( isg - sts 1001 ) : an international , open - label , randomised , controlled , phase 3 , multicentre trial . 
this correction has been made to the online version as of june 2 , 2017 , and the printed article is correct . correction to lancet oncol 2017 ; 18 : 6374 freyer dr , chen l , krailo md , et al . 
 effects of sodium thiosulfate versus observation on development of cisplatininduced hearing loss in children with cancer ( accl0431 ) : a multicentre , open - label , controlled , randomised , phase 3 trial . 
lancet oncol 2017 ; 18 : 6374in the summary and results of this article , the sentences should regarding adverse events have read the most common grade 34 haematological adverse events reported , irrespective of attribution , were neutropenia ( 117 [ 66% ] of 178 participant cycles in the sodium thiosulfate group vs 145 [ 65% ] of 224 in the control group ) , whereas the most common non - haematological adverse event was hypokalaemia ( 25 [ 17% ] of 149 vs 22 [ 12% ] of 187 )  . 
 in the results , sentences regarding adverse events should have read haematological toxicity was not significantly different between the treatment groups , occurring 137 ( 77% ) of 178 participant cycles in the sodium thiosulfate group and 172 ( 77% ) of 224 participant cycles in the control group ( p = 097 ; table 3 )  . 
aggregate nephrotoxicity was more common in the sodium thiosulfate group , in which 37 ( 25% ) of 149 participant cycles were affected versus 25 ( 13% ) of 187 controls ( p = 00071 ; sentences table 4 ) ; serious adverse events regarding should have read 194 serious adverse events were reported in 26 patients ; of these , 127 were deemed unrelated , 47 unlikely , 20 possibly , and none related to probably or definitely sodium thiosulfate . 
87 were nonhaematological adverse events , of which 45 were deemed unrelated , 28 unlikely , 14 possibly , and none related to probably or definitely sodium sentences thiosulfate ; regarding median follow - up should have read median follow - up was 35 years ( iqr 3045 ) for event - free vol 18 june 2017 e301 corrections concurrent once - daily versus twice - daily chemoradiotherapy in patients with limited - stage small - cell lung cancer ( convert ) : an open - label , phase 3 , randomised , superiority trial corinne faivre - finn , michael snee , linda ashcroft , wiebke appel , fabrice barlesi , adityanarayan bhatnagar , andrea bezjak , felipe cardenal , pierre fournel , susan harden , cecile le pechoux , rhona mcmenemin , nazia mohammed , mary obrien , jason pantarotto , veerle surmont , jan p van meerbeeck , penella j woll , paul lorigan , fiona blackhall , for the convert study team summary background concurrent chemoradiotherapy is the standard of care in limited - stage small - cell lung cancer , but the optimal radiotherapy schedule and dose remains controversial . 
the aim of this study was to establish a standard chemoradiotherapy treatment regimen in limited - stage small - cell lung cancer . methods the convert trial was an open - label , phase 3 , randomised superiority trial . 
we enrolled adult patients ( aged 18 years ) who had cytologically or histologically confirmed limited - stage small - cell lung cancer , eastern cooperative oncology group performance status of 02 , and adequate pulmonary function . 
patients were randomly assigned to receive either 45 gy radiotherapy in 30 twicedaily fractions of 15 gy over 19 days , or 66 gy in 33 once - daily fractions of 2 gy over 45 days , starting on day 22 after commencing cisplatinetoposide chemotherapy ( given as four to six cycles every 3 weeks in both groups )  . 
a 12% higher overall survival at 2 years in the once - daily group versus the twice - daily group was considered to be clinically significant to show superiority of the once - daily regimen . 
the study is registered with clinicaltrials . gov ( nct00433563 ) and is currently in follow - up . findings between april 7 , 2008 , and nov 29 , 2013 , 547 patients were enrolled and randomly assigned to receive twice - daily concurrent chemoradiotherapy ( 274 patients ) or once - daily concurrent chemoradiotherapy ( 273 patients )  . 
 four patients ( one in the twice - daily group and three in the once - daily group ) did not return their case report forms and were lost to follow - up ; these patients were not included in our analyses . 
at a median follow - up of 45 months ( iqr 3558 ) , median overall survival was 30 months ( 95% ci 2434 ) in the twice - daily group versus 25 months ( 2131 ) in the once - daily group ( hazard ratio for death in the once daily group 118 [ 95% ci 095145 ] ; p = 014 )  . 
 2 - year overall survival was 56% ( 95% ci 5062 ) in the twice - daily group and 51% ( 4557 ) in the once - daily group ( absolute difference between the treatment groups 53% [ 95% ci 32% to 137% ] )  . 
the most common grade 34 adverse event in patients evaluated for chemotherapy toxicity was neutropenia ( 197 [ 74% ] of 266 patients in the twice - daily group vs 170 [ 65% ] of 263 in the once - daily group )  . 
most toxicities were similar between the groups , except there was significantly more grade 4 neutropenia with twice - daily radiotherapy ( 129 [ 49% ] vs 101 [ 38% ] ; p = 005 )  . 
in patients assessed for radiotherapy toxicity , was no difference in grade 34 oesophagitis between the groups ( 47 [ 19% ] of 254 patients in the twice - daily group vs 47 [ 19% ] of 246 in the once - daily group ; p = 085 ) and grade 34 radiation pneumonitis ( 4 [ 3% ] of 254 vs 4 [ 2% ] of 246 ; p = 070 )  . 
11 patients died from treatment - related causes ( three in the twice - daily group and eight in the once - daily group )  . interpretation survival outcomes did not differ between twice - daily and once - daily concurrent chemoradiotherapy in patients with limited - stage small - cell lung cancer , and toxicity was similar and lower than expected with both regimens . 
since the trial was designed to show superiority of once - daily radiotherapy and was not powered to show equivalence , the implication is that twice - daily radiotherapy should continue to be considered the standard of care in this setting . funding cancer research uk ( clinical trials awards and advisory committee ) , french ministry of health , canadian cancer society research institute , european organisation for research and treatment of cancer ( cancer research fund , lung cancer , and radiation oncology groups )  . copyright the author ( s )  . 
we searched pubmed and the abstracts of major conferences ( such as the american society of clinical oncology ) with the terms small cell lung cancer , limited - stage , radiotherapy ( or irradiation ) , and chemotherapy , with no constraints imposed on the timeframe for the search , for randomised evidence to support this practice . 
we found only one relevant randomised clinical trial comparing once - daily and twice - daily radiotherapy . added value of this study although twice - daily radiotherapy has produced the best outcomes in these patients so far , concerns about its toxicity , logistical issues in the delivery of twice - daily radiotherapy , and the low radiation dose used in the control group of the intergroup 0096 study have resulted in the poor adoption of this regimen and no consensus on the standard treatment to use in the routine setting . 
 furthermore , the results of this study show that in the era of modern radiotherapy techniques , the frequency and severity of acute and late radiation toxicities are lower than previously reported . implications of all the available evidence results from this study showed that twice - daily radiotherapy should be considered standard - of - care in patients with limitedstage small - cell lung cancer . 
this article provides updated information on expected treatment toxicity that clinicians can relay to their patients . introduction small - cell lung cancer is characterised by its rapid tumour doubling time , early dissemination , and high response rate to both chemotherapy and radiotherapy . 
of the 42 000 patients in the uk and 225 000 in the usa diagnosed with lung cancer every year , 15% have small - cell lung cancer and 30% of those have limited - stage disease that can be encompassed within a tolerable radiotherapy field.1 even in this early - stage disease , outcomes are poor , with median survival of 1624 months after curative intent treatment and 2 - year survival of less than 50%.24 combined chemotherapy and thoracic radiotherapy is the standard treatment for limited - stage small - cell lung cancer . 
subsequently , metaanalyses of clinical trials investigating the optimal timing and sequencing of chemoradiotherapy have shown an advantage for early concurrent thoracic radiotherapy.711 furthermore , twice - daily radiotherapy was superior to once - daily radiotherapy in the landmark intergroup 0096 study.4 in that study , patients were randomly assigned to receive either 45 gy once - daily ( 18 gy per fraction ) for 5 weeks or 45 gy twice - daily ( 15 gy per fraction ) for 3 weeks . 
 twice - daily radiotherapy significantly improved 5 - year overall survival compared with once - daily radiotherapy ( 26% vs 16% ) and reduced the risk of thoracic relapse ( 36% vs 52% ) but at the cost of increased severe radiation oesophagitis ( 32% vs 16% )  . 
consequently , twice - daily radiotherapy concurrently with chemotherapy was adopted as a standard of care for limited - stage small - cell lung cancer.12 however , it is unclear whether twice - daily radiotherapy resulted in better outcomes because of the increase in the biologically effective dose of radiation or because of shorter overall treatment time , which is rapidly proliferating disease . 
 important radiotherapy the techniques have evolved intergroup 0096 study was designed in the late 1980s ; specifically , the use of ct - planned conformal treatment and the omission of elective nodal irradiation to reduce normal toxicity , particularly oesophagitis . tissue exposure and since this although twice - daily radiotherapy concurrently with chemotherapy has produced the best outcomes so far , concerns about its toxicity , logistical issues in its delivery , and the low radiation dose in the control group of the intergroup 0096 study , resulting in a very high ( 52% ) local failure rate , have resulted in the poor adoption of this regimen and no consensus on the standard treatment to use in the routine setting.13 the authors of one study14 suggested that the local control could be improved with a higher dose of once - daily radiotherapy . 
the convert trial was therefore designed as a superiority trial to improve on the standard of care for limited - stage smallcell lung cancer by comparing twice - daily radiotherapy to a higher dose of radiotherapy delivered once daily , given concurrently with chemotherapy . methods study design and participants the convert trial was an international , multicentre , open - label , randomised phase 3 superiority trial . 
details of the trial design have been published previously.15 patients were recruited at 73 centres in eight countries vol 18 august 2017 1117 articles see online for appendix ( belgium , canada , france , netherlands , poland , slovenia , spain , and the uk ; appendix pp 12 )  . eligible patients were aged 18 years or older ; had histologically or cytologically confirmed small - cell lung cancer with limited disease ( as defined by the veterans administration lung cancer study groupie , patients whose disease can be encompassed within a radical radiation portal ) ; 16 had an eastern cooperative oncology group performance status of 0117 or performance status of 2 due to disease - related symptoms and not comorbidities ( since small - cell lung cancer is characterised by rapid doubling time and central disease location , which can be associated with a sudden change in performance status ) ; had no malignant pleural or pericardial effusions ; and had acceptable radiotherapy target volume ( according to the local radiotherapist )  . 
eligible patients had a maximum of one adverse biochemical factor ( concentrations of serum alkaline phosphatase > 15 - times the upper limit of normal , serum sodium < lower limit of normal , and serum lactate dehydrogenase > the upper limit of normal ) , forced expiratory volume in 1 s greater than 1 l or 40% predicted value , and transfer factor for carbon monoxide greater than 40% predicted value . 
patients with a previous history of malignancy in the past 5 years ( except for non - melanomatous skin or insitu cervix carcinoma ) and those with previous or concomitant illness or treatment that , in the opinion of the investigator , would interfere with the trial treatments or comparisons were excluded . participants gave written informed consent and the study was done according to the declaration of helsinki and good clinical practice guidelines . 
the trial was reviewed in the uk by the national research ethics service committee north westgreater manchester central , which granted ethics approval for the study on dec 21 , 2007 ( rec reference : 07 / h1008 / 229 )  . 
the protocol was also approved by the institutional review board or research ethics committee in each country and at each study centre . randomisation and masking patients were randomly assigned ( 1 : 1 ) to one of the two treatment groups ( twice - daily vs once - daily radiotherapy )  . 
 the factors controlled for in the allocation were institution , planned number of chemotherapy cycles ( four vs six ) , and performance status ( 01 vs 2 )  . 
 investigators were not masked procedures at baseline , all patients underwent baseline investigations , which included physical examination , chest radiograph , ct scan of the thorax and upper abdomen , ct or mri of the brain , full blood count , biochemical profile , and lung function tests . 
staging was done using the union for international cancer control / american joint committee on cancer classification system.18 patients were randomly assigned to receive radiotherapy either twice - daily ( 45 gy in 30 twice - daily fractions of 15 gy , with a minimum of 6 h between fractions , over 19 days , on 5 consecutive days a week ) or once - daily ( 66 gy in 33 daily fractions of 2 gy over 45 days , on 5 consecutive days a week ) , concurrently with chemo therapy . 
chemotherapy was started within 4 weeks of randomisation and consisted of four to six cycles of cisplatin and etoposide every 3 weeks in both groups ( etoposide 100 mg / m intravenously on days 13 and cisplatin 75 mg / m intravenously on day 1 , or etoposide 100 mg / m intravenously on days 13 and cisplatin 25 mg / m intravenously on days 13 )  . 
no later than 6 weeks after the last cycle of chemotherapy , patients without evidence of progressive disease on the ct scan and with no clinical evidence of brain metastases were offered prophylactic cranial irradiation . radiotherapy commenced on day 22 of cycle one of chemotherapy , coinciding with cycle two of chemotherapy in patients not experiencing chemotherapy delay due to toxicity . 
however , we recommended a chemotherapy treatment delay of more than 7 days for grade 4 febrile neutropenia , grade 4 thrombocytopenia requiring medical intervention , or grade 2 or worse bleeding with thrombocytopenia ; for the first episode of such an event , we recommended full - dose chemotherapy and granulocyte colony - stimulating factor support , or a 20% dose reduction . 
 a radiotherapy quality assurance programme was set up to ensure the robustness of the radiotherapy procedures , and the details of the programme have been reported previously.15 the programme was managed by the uk national cancer research institute radiotherapy trials quality assurance team . 1118 vol 18 august 2017 articles 274 allocated to receive twice - daily concurrent chemoradiotherapy 273 allocated to receive once - daily concurrent chemoradiotherapy 547 patients randomly assigned 7 progressive disease or died 25 did not receive concurrent chemoradiotherapy ( 20 no radiotherapy and 5 received sequential chemoradiotherapy ) 5 tumour volume too large 4 randomisation error 4 patient withdrawal or lost to follow - up 3 chemotherapy toxicity 2 oncologist decision 10 progressive disease or died 33 did not receive concurrent chemoradiotherapy ( 26 no radiotherapy , 6 received sequential chemoradiotherapy , and 1 unknown ) 7 oncologist decision 7 tumour volume too large 5 patient withdrawal or lost to follow - up 3 randomisation error 1 unknown 249 received concurrent chemoradiotherapy 1 received once - daily chemoradiotherapy 240 received concurrent chemoradiotherapy 6 received twice - daily chemoradiotherapy 1 lost to follow - up ( did not return case report form ) 3 lost to follow - up ( did not return case report form ) 273 included in survival analysis 254 included in radiotherapy toxicity analysis ( concurrent and sequential chemoradiotherapy ) 266 included in chemotherapy toxicity analysis 270 included in survival analysis 246 included in radiotherapy toxicity analysis ( concurrent and sequential chemoradiotherapy ) 263 included in chemotherapy toxicity analysis figure 1 : trial profile * one patient withdrew consent for twice - daily radiotherapy . 
 on completion of study treatment , patients were followed up weekly until the resolution of acute sideeffects , then every 3 months until 1 year , and every 6 months for 5 years . 
subsequently , during followup at 6 and 12 months after randomisation , investigations included physical evaluation , reporting of adverse events , and a ct scan of the thorax and abdomen . 
follow - up investigations were done according to local policy . outcomes the primary outcome of the study was overall survival , defined as time from randomisation until death from any cause . 
secondary outcomes included compliance with chemotherapy and radiotherapy ( defined as dose intensity delivered ) , acute toxicity ( defined as toxicity occurring between the start of treatment and up to 3 months after completion of treatment , and assessed according to the common terminology criteria for adverse events [ version 3.0 ] ) , late toxicity ( according to the common terminology criteria for adverse events [ version 3.0 ] ) , 19 local and metastatic progression - free survival and ( calculated from date of randomisation to date of first clinical or radiological evidence of progressive disease at the primary site or distant sites )  . 
all serious adverse events were reported to the trial coordinating centre and were assessed for causality and expectedness , both locally by the principal investigator and centrally by the chief investigator . statistical analysis our hypothesis was that overall survival in the once - daily chemoradiotherapy group would be superior to that of the twice - daily group . 
a 12% higher overall survival at 2 years in the once - daily group versus the twice - daily group was considered to be clinically significant to show superiority of the once - daily regimen . 
overall and the progression - free survival were estimated with kaplan - meier method , and between - group comparisons vol 18 august 2017 1119 articles evaluated by the log - rank test with stratification for institution , planned number of chemotherapy cycles ( four vs six ) , and performance status ( 01 vs 2 )  . 
the number of events required to detect a hazard ratio ( hr ) for death of 07 with an level ( two - sided ) of 005 and 80% power ( ie , an increase in 2 - year survival from 44% in the twice - daily radiotherapy group to 56% in the oncedaily radiotherapy group ) was 247 . 
 * eastern cooperative oncology group performance status was not recorded on the source documentation and case report form in three cases at baseline ; in all three cases , the performance score was recorded as 01 on the randomisation fornever smokers defined as adults who have never smoked a cigarette or who smoked fewer than 100 cigarettes in their entire lifetime ; former smokers defined as adults who have smoked at least 100 cigarettes in their lifetime but say they currently do not smoke ; current smokers defined as adults who have smoked 100 cigarettes in their lifetime and currently smoke cigarettes every day ( daily ) or on some days ( non - daily )  . table 1 : baseline characteristics added to the sample size of 506 patients to allow for ineligible patients , giving a total recruitment target of 532 patients . 
the primary survival outcome was analysed using the modified intention - to - treat principle , because four cases provided no follow - up data and hence were censored at time zero . 
further details about the statistical analysis are available in the protocol.15 all randomly assigned patients who were treated with at least one study dose of chemotherapy and who were alive at the time of the first toxicity assessment were included in the safety analysis . 
 the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results between april 7 , 2008 , and nov 29 , 2013 , we recruited 547 patients from 73 centres in eight countries . 
the median age at randomisation was 62 years ( iqr 2984 ) in the twice - daily group and 63 years ( 3481 ) in the once - daily group , with 83 ( 15% ) of 547 patients being older than 70 years ( 32 [ 12% ] in the twice - daily group and 51 [ 19% ] in the once - daily group )  . 
less than 2% of patients were never smokers , almost two - thirds were former smokers , and just over a third were current smokers ( table 1 )  . 
312 ( 57% ) of 547 patients were staged with pet / ct , and 426 ( 78% ) of 547 were stage iii according to the union for international cancer control classification ( table 1 )  . the number of planned cycles of chemotherapy was four for most patients ( table 1 )  . 
 1120 vol 18 august 2017 articles 164 ( 60% ) of 273 patients in the twice - daily group had died , compared with 176 ( 65% ) of 270 patients in the once - daily group . in our survival analysis ( which included 273 patients in the twice - daily group and 270 in the once - daily group ) , median overall survival was 30 months ( 95% ci 2434 ) in the twice - daily group and 25 months ( 2131 ) in the oncedaily group ( hazard ratio 118 [ 95% ci 095145 ] ; p = 014 ; figure 2a )  . 
2 - year overall survival was 56% ( 95% ci 5062 ) in the twice - daily group and 51% ( 4557 ) in the once - daily group ( absolute difference between the treatment groups 53% [ 95% ci 32% to 137% ] )  . 
5 - year overall survival was 34% ( 95% ci 2741 ) in the twice - daily group and 31% ( 2537 ) in the once - daily group ( absolute difference 28% [ 95% ci 64% to 120% ] )  . 
in the twice - daily group versus the once - daily group , causes of death were lung cancer ( 152 vs 146 ) , intercurrent deaths ( six vs 14 ) , treatmentrelated ( three vs eight ) , and cardiovascular ( three vs eight ) ; causes of the 12 treatment - related deaths were radiation pneumonitis ( one vs two ) , dementia possibly related to prophylactic cranial irradiation ( none vs one ) , neutropenic sepsis ( one vs three ) , septic shock ( one vs none ) , bronchial pneumonia ( none vs two ) , and peripheral vascalar ischaemia ( one vs none )  . 
 intensity - modulated 25 ( 9% ) of 273 patients in the twice - daily radiotherapy group and 33 ( 12% ) of 270 in the once - daily radiotherapy group did not receive concurrent chemoradiotherapy ( figure 1 ) , giving compliance rates of 91% in the twicedaily group and 88% in the once - daily group . 
less than 10% of patients did not receive any radiotherapy ( 20 [ 7% ] in the twice - daily group and 26 [ 10% ] in the once - daily group ; figure 1 , table 2 )  . 
of the patients who received radiotherapy was radiotherapy , delivered to 40 ( 16% ) of 254 participants in the twice - daily group versus 43 ( 17% ) of 247 participants in the once - daily group . 
 more patients received the full dose of radiotherapy in the twice - daily group than in the once - daily group ( p < 00001 ; table 3 )  . 
the optimal number of fractions , as defined in the protocol , 15 ( 30 fractions in the twice daily group and 33 in the once daily group ) were delivered in 213 ( 86% ) of 249 patients in the twice - daily group and 192 ( 80% ) of 240 patients ( p = 010 )  . 
 radiotherapy was delivered over the planned overall treatment time of 19 days in 158 ( 63% ) of 249 patients in the twice - daily group and over the planned overall treatment time of 45 days in 114 ( 48% ) of 240 patients in the once - daily group ( p = 00004 )  . 
protocol deviations and violations were mainly due to logistical reasons , such as public holidays . the once - daily group at the time of analysis , 181 ( 66% ) of 273 patients in the twice - daily group and 189 ( 70% ) of 270 patients in the once - daily group had disease progression ( p = 026 )  . 
median local progression - free survival was 207 months ( 95% ci 161279 ) in the twice - daily group versus 179 months ( 153217 ) in the once daily group ( figure 2b ) and median metastatic progression - free survival was 202 months ( 95% ci 159253 ) versus 166 months ( 137218 )  . 
 the difference between groups for local progressionfree survival ( p = 020 ) and metastatic progression - free survival ( p = 024 ) was not significant ( figure 2 )  . 
there was no notable difference between groups in treatment received at the time of progression ( appendix p 4 )  . chemotherapy toxicity was assessed in 266 ( 97% ) of 273 patients in the twice - daily group and 263 ( 97% ) of 270 patients in the once - daily group , who had received at least one cycle of chemotherapy and who were alive at the time of the first toxicity assessment ( figure 1 , table 4 )  . 
the frequencies of most adverse events recorded were similar in both groups , with the exception that significantly more grade 4 neutropenia was recorded in the twice - daily group than in the once - daily group ( 129 [ 49% ] vs 101 [ 38% ] ; p = 005 )  . 
acute radiotherapy toxicity was similar in both groups : grade 34 oesophagitis was reported in 47 ( 18% ) of 254 patients in the twice - daily group and 47 ( 19% ) of 246 patients in the once - daily group . 
 11 patients developed grade 35 radiation pneumonitis ( five in the twice daily group and six in the once daily group ) , of whom three patients died within 3 months of radiotherapy ( two in the once - daily group and one in the twice - daily group , one of whom received sequential rather than concurrent radiotherapy ; table 4 , appendix p 3 )  . 
six patients in each group developed grade 34 pneumonitis , and five patients ( three in the twice - daily group and two in the once - daily group ) developed grade 3 pulmonary fibrosis ( table 5 )  . discussion our results show that once - daily radiotherapy did not improve overall survival in patients with limited - stage small - cell lung cancer and good performance status , compared with twice - daily radiotherapy , when given concurrently with chemotherapy . 
 however , although results are unable to show superiority of the once - daily radiotherapy regimen , the convert trial should have a major effect on the standardisation of chemoradiotherapy in this disease groupa treatment that has been the subject of controversy since the publication of the intergroup 0096 study.4 , 13 overall survival with both regimens were higher than the survival results reported in the intergroup 0096 study . 
in convert , 2 - year survival for twice - daily and once - daily radiotherapy was 56% and 51% , versus 47% and 41% in the intergroup 0096 study.4 convert was not an equivalence study ( and was not powered for equivalence ) so it cannot be concluded that the two regimens have the same efficacy . 
 furthermore , the 2 - year survival of 56% achieved in the control group with twice - daily radiotherapy is the same survival that was projected for the experimental group . 
the radiotherapy toxicity population was used to analyse the prevalence of these adverse events because it would not be possible to report radiotherapy - related toxicity in patients who did not receive radiotherapy . 
two deaths ( peripheral arterial ischaemia [ n = 1 ] in the twice - daily group and dementia possibly related to prophylactic cranial irradiation [ n = 1 ] in the once - daily group )  . 
 table 4 : acute adverse events ( 3 months after completion of study treatment ) groups might be explained by several changes in the management of small - cell lung cancer since the publication of the intergroup study , including pet / ct staging in more than half of patients , the use of modern and precise radiotherapy techniques , and improvements in supportive care . 
these results , together with several meta - analyses and systematic overviews , support the use of short overall radiotherapy treatment time to avoid early cancer cell repopulation.711 one of the systematic overviews also identified that time from the start of any treatment to completion of radiotherapy is a key variable in predicting outcome.20 although not significant , 2 - year overall survival was slightly higher in the twice - daily group than in the once - daily group , which could possibly be a result of improved delivery of treatment in the twice - daily group ( n = 248 ) once - daily group ( n = 233 ) p value * grade 12 grade 3 grade 4 grade 12 grade 3 grade 4 dermatitis oesophagitis oesophageal stricture or fistula 15 ( 6% ) 29 ( 12% ) 8 ( 3% ) 17 ( 7% ) 39 ( 17% ) 4 ( 2% ) 6 ( 3% ) 1 ( < 1% ) 2 ( 1% ) 5 ( 2% ) 006 048 > 099 078 pulmonary fibrosis 119 ( 48% ) 3 ( 1% ) 106 ( 46% ) pneumonitis 71 ( 29% ) 5 ( 2% ) 1 ( < 1% ) 70 ( 30% ) 1 ( < 1% ) 090 myelitis other 1 ( < 1% ) 8 ( 3% ) 131 ( 53% ) 20 ( 8% ) 3 ( 1% ) 113 ( 49% ) 18 ( 8% ) 2 ( 1% ) data are n ( % )  . 
 table 5 : late adverse events ( > 3 months after study treatment ) vol 18 august 2017 1123 articles twice - daily group , with more patients receiving full - dose radiotherapy , the optimal planned number of fractions , and treatment delivered over the optimal treatment time . 
another reason why treatment delivery was superior in the twice - daily group is because of the lower overall dose of radiotherapy in this group , which meant it was possible to achieve the protocol dose constraints for organs at risk , such as lung and spinal cord , in a greater proportion of patients than in the once - daily group . 
a further advantage of the twice - daily regime is that it halves the radiotherapy treatment time ( from 45 days to 19 days ) and reduces the number of fractions ( from 33 to 30 ) compared with the once - daily regimen . 
 although no formal health economic analysis has been done as part of this study , the delivery of twice - daily radiotherapy could lead to cost savings , especially if patients require hospital transport to attend radiotherapy appointments . overall , the frequency and severity of acute and late radiation toxicities were lower than expected , probably because of the use of modern radiotherapy techniques , including 3d radiotherapy or intensity - modulated radiotherapy , and treatment of involved fields with regard to nodal disease . 
in the intergroup 0096 trial , 4 patients were treated with outdated radiotherapy techniques including elective nodal irradiation , which would have resulted in higher radiation exposure of normal tissues than in this trial . 
indeed , the high rate of severe acute oesophagitis ( 32% with twice - daily radiotherapy ) in the intergroup study has been cited as the main reason for poor adoption of twice - daily radiotherapy.13 by contrast , less than 20% of patients had severe oesophagitis in the convert study and only one patient developed an oesophageal stricture requiring intervention . 
radiation pneumonitis was not specifically reported in the intergroup 0096 study , but in this trial very few ( < 3% ) patients had severe radiation pneumonitis or severe pulmonary fibrosis . 
the lower than anticipated toxicity rates and rates of local failure reported in this study suggest that radiotherapy treatment delivered concurrently with chemotherapy could be intensified furtherfor example , by means of dose escalation or hypofractionation . a limitation of this study is that although we did not mandate an upper age limitwith the aim to gather much needed evidence about the outcome of elderly patients treated with concurrent chemoradiotherapy only 15% of the patients included were older than 70 years . 
data for patients older than 70 years participating in convert was presented at the international association for the study of lung cancer 17th world conference on lung cancer in vienna , austria , in 2016 , and the results of this analysis will be presented in a separate report . 
elderly patients have been reported to be less likely to receive concurrent chemoradiotherapy than their younger counterparts , which is mainly due to insufficient high - quality evidence to support the use of this potentially toxic treatment.21 another limitation is that the majority of patients enrolled in both groups were white , and therefore the results of the study might not be applicable to other ethnicities . to our knowledge , convert is the largest study completed investigating thoracic radiotherapy in limitedstage small - cell lung cancer , and the first clinical trial in this group of patients to report on the outcome of patients treated with modern radiotherapy techniques incorporating a quality assurance programme . 
furthermore , by contrast with us practice , concurrent chemoradiotherapy is not always adopted as the standard of care for limited - stage smallcell lung cancer in europe , and the study provided an incentive for centres to adopt and set up concurrent treatment protocols . given the importance of keeping overall treatment time as short as possible , future studies could investigate doseescalated twice - daily or hypofractionated radio therapy concurrently with chemotherapy . 
further data for the outcome of patients treated with high - dose 2 gy per fraction treatment will be provided by the ongoing calgb 30610 / rtog 0538 study ( nct00632853 )  . 
the upcoming analysis of the convert translational studies , including the prognostic role of baseline circulating tumour cells , could provide data for relevant biological stratification factors that can be used prospectively in future studies . in conclusion , the results of convert show that there were no significant differences in survival and no major differences in toxicity between twice - daily and once - daily radiotherapy . 
however , since the trial was designed to show superiority of once - daily radiotherapy and not powered to show equivalence , twice - daily to be considered radiotherapy should continue standard - of - care . 
from a pragmatic perspective , oncedaily radiotherapy could be considered when delivery of twice - daily radiotherapy is impossible because of departmental logistics or patient choice . contributors cf - f , la , pl , ms , fbl , rm , nm , and pjw conceived the study and initiated the study design . 
the authors designed the trial , analysed the data , wrote the manuscript ( with the first draft written by the first author ) , made the decision to submit the manuscript for publication , and assured the completeness and accuracy of the data and analysis and of the fidelity of this report to the trial protocol . 
all authors approved the final manuscript . declaration of interests cf - f , la , pl , and fbl report grants from cancer research uk during the conduct of this study . 
the other authors declare no completing interests . 1124 vol 18 august 2017 articles acknowledgments this study was funded by the cancer research uk clinical trials awards and advisory committee ( grant reference number c17052 / a8154 ) , frenchministry of health , programme hospitalier de recherch clinique ( grant reference number nat 2007 - 28 - 01 ) , canadian cancer society research institute ( grant reference number 021039 ) , and the european organisation for the research and treatment of cancer ( cancer research fund , lung cancer , and radiation oncology groups )  . 
 the authors would like to acknowledge the support of the national cancer research institute radiotherapy trials quality assurance team ( nicki groom and elena wilson ) ; the manchester academic health science centre clinical trials unit ; sally falk and amy bossons ( convert trial coordinators ) ; david ryder ( manchester academic health science centre trials co - ordination unit statistician ) ; the national institute for health research ( nihr ) christie clinical research facility ; david girling , steve roberts , christian manegold , and robert huddart ( independent data monitoring committee members ) ; and dirk de ruysscher and jason lester ( independent members of the trial steering committee )  . 
the views expressed are those of the authors and not necessarily those of the nhs , nihr , or the department of health . articles panitumumab and irinotecan versus irinotecan alone for patients with kras wild - type , uorouracil - resistant advanced colorectal cancer ( piccolo ) : a prospectively strati ed randomised trial matthew t seymour , sarah r brown , gary middleton , timothy maughan , susan richman , stephen gwyther , catherine lowe , jennifer f seligmann , jonathan wadsley , nick maisey , ian chau , mark hill , lesley dawson , stephen falk , ann ocallaghan , kim benstead , philip chambers , alfred oliver , helen marshall , vicky napp , phil quirke summary background therapeutic antibodies targeting egfr have activity in advanced colorectal cancer , but results from clinical trials are inconsistent and the population in which most bene t is derived is uncertaour aim was to assess the addition of panitumumab to irinotecan in pretreated advanced colorectal cancer . 
 methods in this open - label , randomised trial , we enrolled patients who had advanced colorectal cancer progressing after uoropyrimidine treatment with or without oxaliplatin from 60 centres in the uk . 
from december , 2006 until june , 2008 , molecularly unselected patients were recruited to a three - arm design including irinotecan ( control ) , irinotecan plus ciclosporin , and irinotecan plus panitumumab ( irpan ) groups . 
from june 10 , 2008 , in response to new data , the trial was amended to a prospectively strati ed design , restricting panitumumab randomisation to patients with kras wild - type tumours ; the results of the comparison between the irinotcan and irpan groups are reported here . 
we used a computergenerated randomisation sequence ( strati ed by previous egfr targeted therapy and then minimised by centre , who performance status , previous oxaliplatin , previous bevacizumab , previous dose modi cations , and best previous response ) to randomly allocate patients to either irinotecan or irpan . 
patients in both groups received 350 mg / m intravenous irinotecan every 3 weeks ( 300 mg / m if aged 70 years or a performance status of 2 ) ; patients in the irpan group also received intravenous panitumumab 9 mg / kg every 3 weeks . 
tumour dna was pyrosequenced for krasc.146 , braf , nras , and pik3ca mutations , and prede ned molecular subgroups were analysed for interaction with the e ect of panitumumab . 
this study is registered , number isrctn93248876 . results between dec 4 , 2006 , and aug 31 , 2010 , 1198 patients were enrolled , of whom 460 were included in the primary population of patients with krasc.1213 , 61 wild - type tumours and no previous egfr targeted therapy . 
there was no di erence in overall survival between groups ( hr 101 , 95% ci 083123 ; p = 091 ) , but individuals in the irpan group had longer progressionfree survival ( 078 , 064095 ; p = 0015 ) and a greater number of responses ( 79 [ 34% ] patients vs 27 [ 12% ] ; p < 00001 ) than did individuals in the irinotecan group . 
we recorded ve treatment - related deaths , two in the irpan group and three in the irinotecan group . interpretation adding panitumumab to irinotecan did not improve the overall survival of patients with wild - type kras tumours . 
in december , 2006 , the uk colorectal clinical studies group launched a randomised trial in uorouracil - resistant advanced colorectal cancer , called the panitumumab , irinotecan , and ciclosporin in colorectal cancer ( piccolo ) trial . 
 we selected patients using conventional clinico pathological criteria and allocated them randomly in equal distributions to one of three groups : irinotecan alone , irinotecan plus irinotecan plus ciclosporin , or panitumumab ( irpan )  . 
 in april , 2008 , kras mutation was reported to be a negative predictive biomarker targeted therapyretrospective analysis of a randomised trial1 of panitumumab versus supportive care showed that panitumumab bene t was con ned to patients with tumours wild - type at kras codons 1213 ( p < 00001 )  . 
30 patients were randomised to irinotecan under the irinotecan vs ircs comparison only during this time , and are not included in the summaries of patients forming the irinotecan vs irpan comparison . 
the trial management group ( including patients representatives ) and an independent data monitoring and ethics committee agreed that continued randomisation of patients with kras mutations to panitumumab would not be bene cial to the patients nor would it provide useful data . 
the aim of the trial was therefore amended : evaluation of panitumumab would now focus on patients with kras wild - type tumours , with quanti cation of treatment bene t and evaluation of further biomarkers this selected population , rather than in an unselected population . 
on june 10 , 2008 , 1 week after announcement of the cetuximab data , a safety amendment was introduced to exclude patients with kras - mutated tumours from randomisation to the irpan group ; within 3 months piccolo was reopened as a prospectively strati ed trial : patients with kras wild - type tumours were randomly allocated to irinotecan or irpan while those with kras mutations ( or unknown kras status ) were randomly allocated to irinotecan or irinotecan plus ciclosporwe present here the nal results of the irinotecan versus irpan comparison for patients with kras wild - type tumours who had not received previous anti - egfr therapy ; ndings from the irinotecan versus irinotecan plus ciclosporin comparison will be reported elsewhere.4 methods study design and patients piccolo was a multicentre , randomised controlled trial in chemoresistant advanced colorectal cancer . 
recruitment of molecularly unselected patients started on dec 4 , 2006 ; panitumumab randomisation was restricted to known kras - wild type patients from june 10 , 2008 ; it was then relaunched with full prospective molecular strati cation recruitment on aug 31 , 2010 . 
 eligible patients were aged 18 years or older , had histologically con rmed colorectal cancer , inoperable advanced disease , and had progressed during or after uoro pyrimidine - containing chemotherapy . 
other eligibility criteria were as follows : response evaluation criteria in solid tumors ( recist ) measurable disease ; 5 who per for mance status 02 ; haemoglobin concentration of 100 g / l or greater ; white blood cell count of greater than or equal to 30 10 cells per l ; a platelet count of greater than or equal to 100 10 per l ; estimated glomerular ltration rate of greater than or equal to 50 ml min ; bilirubin concentration less than or equal to 25 mol / l ; and alkaline phosphatase concentrations of ve times the upper limit of normal or lower and aminotransferase concentrations of 25 times upper limit of normal or lower . 
before enrolment , patients provided written consent participate , and for the molecular studies . randomisation and masking from dec 4 , 2006 , to june 9 , 2008 , patients were allocated equally to irinotecan alone , irinotecan plus ciclosporin , or irpan . 
randomisation was done with an automated telephonic system at the clinical trials research unit , university of leeds , uk , using a computer - generated minimisation algorithm including a random element , rst strati ed by previous treatment with egfr monoclonal antibodies , then minimised within each of the following strata : centre , who performance status , previous oxaliplatin , previous bevacizumab , previous dose modi cations , and best previous response . 
 on june 10 , 2008 , a temporary safety measure was applied that restricted the allocation of patients with unknown or mutated kras status to the irinotecan or irinotecan plus ciclosporin groups only . 
under the new protocol , patients were pre - registered ( either when piccolo therapy was indicated or pre - emptively during rst - line therapy ) and stored resection or biopsy tumour material was retrieved and tested for krasc.12 , 13 , 61 . 
to reduce the possibility of patients in the control group ( irinotecan only ) being discontinued from treatment prematurely , and after consultation with the patient representative on the trial management group , patients and their clinicians were not routinely made aware of patients kras status , but the information was available on request . 
randomisation occurred immediately before starting treatment . in the amended protocol , randomisation was strati ed by kras status : patients with kras wild - type tumours were randomised in a one - to - one ratio to irinotecan or irpan . 
if kras was mutated or unknown , randomisation was one - to - one to irinotecan or irinotecan plus ciclospor 173 not conrmed wild - type kras c.12 - 13 , 61 kras mutant c.12 - 13 , 61 prior anti - egfr - mab therapy kras - undetermined 696 patients randomised to irinotecan versus irpan 523 conrmed kras wild - type c.12 - 13 , 61 460 primary population : kras wild - type , no prior anti - egfr mab c.12 - 13 , 61 323 all wild - type braf mutant nras mutant pik3ca mutant mutant kras c.146 prior anti - egfr therapy figure 2 : molecular characterisation irpan = irinotecan plus panitumumab . 
in the irinotecan versus irpan comparison , patients were rst strati ed by previous egfr targeted therapy , with minimisation done separately within each stratu this was an open - label trial , so patients and clinicians were not masked to treatment allocation . procedures the full protocol is available online . 
brie y , a 1 - week delay was given for unresolved non - haematological toxicities of grade 2 or higher ; patients who had toxicities of grade 3 or higher , or a toxicity requiring two dose delays , had a 20% dose reduction . 
after 12 weeks ( four cycles ) patients with stable or responding disease could , at the clinicians discretion , be o ered a planned break from irinotecan of up to two cycles ; patients on irpan continued panitumumab alone during irinotecan breaks . 
there was no within - protocol crossover , but post - trial treatment was not restricted . recist5 response was assessed every 12 weeks with ct scans , scored locally , and quality - assured by central review in more than a third of patients . 
anticipated median overall survival with irinotecan was 9 months , 11 with a targeted improvement to 12 months with the addition of panitumumab , resulting in a sample size of 720 patients and at least 380 deaths . 
 in the amended design , we anticipated an increased treatment bene t with irpan in the re ned primary population of krasc.12 , 13 , 61 wild - type patients not pretreated with egfr monoclonal antibodies . 
we have previously assessed kras as a prognostic and predictive marker in patients treated with cytotoxic chemotherapy alone , 10 and on the basis of these data , we made no change to the predicted overall survival of 9 months for kras wild - type patients in the irinotecan alone group . 
however , in the new design we aimed to detect a 30% reduction in hazard rate , corresponding to a median overall survival of 129 months with the addition of panitumumab . 
 an interim analysis was planned to address inferiority or superiority of irinotecan plus panitumumab compared with irinotecan alone , with a stringent p value of 0001 , therefore no adjustment was required in the nal signi cance included progression - free survival ( pfs ) , the proportion of patients level.12 secondary endpoints who achieved a recist response , quality of life , and toxicity . 
post - hoc statistical comparisons were made between the rates of grade 3 or higher events in the two groups , using univariate tests ( or fishers exact test for ve or fewer events ) at the 5% signi cance level . 
in planning these analyses , molecular subgroups were prede ned to determine treatment interaction with mutation status , with the pre - existing hypothesis that krasc.12 , 13 , 61 wild - type patients with a mutation at one of the other loci would have less bene t from panitumumab than would patients with no mutations . 
patients were grouped as having any mutation ( a mutation at any other one of the assessed loci ) or as all wild - type ( no mutations at the loci tested )  . 
in the analysis , missing data for an individual gene was imputed as wild - type , but we did a sensitivity analysis in which only patients con rmed to be wild - type at all 12 loci were classed as all wild - type . 
 for individual rare mutations occurring in less than 10% of patients , piccolo provides only minimal power ( about 10% ) to detect clinically signi cant treatment e ects ( eg , reduction in hazard rate of 30% )  . 
coxs proportional hazards irinotecan irpan events / patients 208 / 230 211 / 230 irinotecan irpan events / patients 206 / 230 193 / 230 hr 101 ( 95%ci 083123 ) , p = 091 hr 078 ( 95%ci 064095 ) , p = 0015 number at risk irinotecan irpan months months figure 3 : kaplan - meier curves of ( a ) overall survival and ( b ) progression - free survival , at nal analysis irpan = irinotecan plus panitumumab . vol 14 july 2013 articles modelling , adjusting for minimisation factors , was prespeci ed for overall survival and pfs . 
on recommendation from the data monitoring and ethics committee , we also planned a nal updated analysis of overall survival when at least 2 years had passed since all patients were allocated to treatment . 
we also report the secondary endpoints and nal analysis of overall survival , in the primary population , its planned molecular subgroups , and in the exploratory population of patients with mutations at krasc.12 , 13 , 61 . 
results in patients previously treated with an anti - egfr monoclonal antibody will be reported elsewhere , as will results for the comparison of irinotecan versus irinotecan plus ciclospor we used sas ( version 9.2 ) for all statistical analyses . this study is registered as an international standard randomised controlled trial , number isrctn93248876 . role of the funding source cancer research uk provided independent peer review and feedback on the original and revised protocols , but had no other involvement in the trial . 
 * the population for adverse event reporting is patients who received at least one dose of the allocated treatment , and for whom at least one case record form was received to provide adverse event or serious adverse event data . 
post - hoc univariate 2 test ( fishers exact test when number of events is ve or fewer ) of di erence in proportion of grade 35 events , not adjusting for multiple testing . 
 non - haematological nausea vomiting constipation abdominal pain skin toxicity nail toxicity alopecia lethargy headache dizziness haematological neutropenia thrombocytopenia anaemia any haematological table 3 : adverse events 754 vol 14 july 2013 p value grade 3 irpan vs irinotecan 021 099 069 050 069 < 00001 0061 00063 100 073 00072 00082 006 013 0012 articles results in december , 2006 , 1198 patients were starting recruited to the piccolo trial : 494 to the initial threearm design ( dec 4 , 2006june 9 , 2008 ) , 78 to the total ( n ) irinotecan hazard ratio ( 95% ci ) for overall survival comparison vs wild - type in irinotecan group all wild - type any mutation braf mutation nras mutation krasc.146 mutation pik3ca mutation 136 ( 100183 ) ; p = 0049 156 ( 103237 ) ; p = 0035 115 ( 060221 ) ; p = 067 177 ( 085369 ) ; p = 013 111 ( 068180 ) ; p = 069 a hazard ratio greater than one indicates worse survival for patients in mutation group compared with all wild - type patients . 
 table 4 : prognostic analysis temporary safety protocol excluding patients with mutated or unknown kras status from the irpan group ( june 10aug 31 , 2008 ) and 626 to the fully prospectively strati ed design ( sept 1 , 2008aug 31 , 2010 )  . 
in all , 460 patients with kras wild - type tumours who had not previously received egfr therapy were randomly allocated to irinotecan ( 230 patients ) or irpan ( 230 patients ) , and these form our primary population for this report ( gures 1 and 2 ; appendix )  . 
13 ( 6% ) patients in the irinotecan group and one ( < 05% ) patient in the irpan group received an anti - egfr irinotecan irpan events / patients 145 / 163 141 / 160 irinotecan irpan events / patients 145 / 163 131 / 160 number at risk irinotecan irpan irinotecan irpan events / patients 63 / 67 70 / 70 irinotecan irpan events / patients 61 / 67 62 / 70 number at risk irinotecan irpan months months figure 4 : key e cacy endpoints , by mutation status ( a ) overall survival in patients with no mutations . 
 * patients randomised before the protocol amendment in june 10 , 2008 , and genotyped retrospectively . monoclonal antibody as salvage therapy within 3 months of nishing trial treatment . the primary analysis of overall survival was triggered after 246 deaths , although when the database was locked for analysis , 312 ( 68% ) of 460 patients had died . 
the analysis was presented in full at an international conference in 2011 : 13 in brief , median overall survival was 105 months ( 95% ci 95124 ) in the irinotecan group and 104 months ( 87122 ) in the irpan group ( hazard ratio [ hr ] 091 , 95% ci 073114 ; p = 044 )  . 
at nal analysis , 419 ( 91% ) of 460 patients in the primary population had died , and median follow - up of those patients still alive ( n = 41 ) was 254 months ( iqr 225308 )  . 
at nal analysis , we recorded no di erence in overall survival between the groups : median survival was 109 months ( 95% ci 95125 ) in the irinotecan group and 104 months ( 89122 ) in the irpan group ( hr 101 , 95% ci 083123 ; p = 091 ; gure 3 )  . 
more patients had a recist - de ned response in the irpan group than in the irinotecan group ( table 2 ) , with a multivariate odds ratio of 412 ( 95% ci 252676 ; p < 00001 )  . 
brie y , the toxicity of the two regimens was consistent with summaries of product characteristics for irinotecan and panitumumab , and in line with previous trials of antiegfr monoclonal antibodies . 
in terms of events that were grade 3 or higher , diarrhoea , lethargy , skin toxicity , infection , and neutropenia were all more common in the irpan group than in the irinotecan group , as were any haematological , any non - haematological , or a grade 3 or higher toxicity of any type . 
however , there was no increase in the number of deaths attributed wholly or partly to treatment ( three patients with irinotecan , two patients with irpan ) , or in 60 - day all - cause mortality ( 12 patients with irinotecan , 14 patients with irpan )  . 13 patients did not receive any trial treatment ( seven allocated to irinotecan , six to irpan )  . 
of those who did , 66 ( 30% ) of 223 patients on irinotecan and 89 ( 40% ) of 224 patients on irpan needed an irinotecan dose modi cation during cycles 14 ; panitumumab dose modi cations were required for 60 ( 27% ) of 224 patients during cycles 14 . 
by contrast with the global scores , and in keeping with the clinician - reported adverse events ( table 3 ) , quality - of - life symptom scores were worse with irpan ( data not shown )  . of the 460 patients in the primary population , 137 ( 30% ) were classi ed as having any mutation and 323 ( 70% ) were all wild type ( table 1 and gure 2 )  . 
when corrected for prognostic variables ( minimisation factors ) , patients in the any mutation group had inferior survival to all wild - type patients ( p = 0049 )  . 
however , the numbers of patients in these subgroup analyses is small and these exploratory results should be interpreted with caution . we then assessed mutation status as a predictive biomarker of the e ect of panitumumab treatment on 756 vol 14 july 2013 articles survival overall survival , pfs , and response rate , using tests of interaction with mutation status ( any mutation vs all wildtype ) , corrected for prognostic variables . 
the interaction test was positive for all three outcome measures : ( p = 0028 , overall gures 4 and 5a ) , progression - free survival ( p = 0018 , gure 5b ) and response rate ( p = 00095 , appendix )  . 
in patients with all - wild - type tumours , those in the irpan group had better pfs and response rate than did those in the irinotecan groups ( gures 4b and 5b , appendix ) , but we detected no between - group di erence in terms of overall survival ( gure 5 )  . 
by contrast with this nding , in patients with any mutation , panitumumab had no e ect on pfs or response rate ( gure 5b , and appendix ) and an adverse e ect on overall survival ( gures 4c and 5a )  . 
for the small numbers provide individual mutations , insu cient power to con dently detect or refute interactions between treatment e ect and mutation status , so results are exploratory . 
the e ect of panitumumab on pfs and response rate in the individual mutation subgroups gave less consistent results than for overall survival ( gure 5b , appendix )  . 
 a sensitivity analysis including only patients with a full set of data in the all - wild - type group gave similar hrs and e ect sizes to those for the whole all - wild - type population for all endpoints ( appendix )  . 
post - progression survival was reduced in patients in the irpan group , and this di erence was more pronounced in the any - mutation population ( appendix )  . 
103 ( 39% ; 53 in the irinotecan group , 50 in the irpan ) had a krasc.12 , 13 , 61 mutation ( including 17 patients with gly13asp mutations ; ten in the irinotecan group , seven in the irpan group )  . 
we detected no bene t of panitumumab in the gly13asp mutation subgroup ( data not shown )  . discussion in our trial , the addition of panitumumab to irinotecan for patients with kras wild - type tumours had no e ect on overall survival , which was our primary endpoint . 
our ndings are in keeping with the emerging pattern of clinical e ect of anti - egfr monoclonal antibody therapy in patients with kras wild - type colorectal cancer ( panel )  . to the best of our knowledge , piccolo is the rst randomised trial in advanced colorectal cancer to have introduced prospective testing of mutation status to determine patients randomisation and treatment . 
in addition to prospective strati cation by krasc.12 , 13 , 61 status , piccolo included a prospectively planned , retrospective analysis of other candidate mutations in the mek / akt activation pathway . 
 determination of the e ect of less common mutations is challenging , because any randomised trial powered for a common group ( eg , kras wild - type ) inevitably underpowered to detect or exclude potentially clinically important e ects in rarer subgroups ( eg , braf mutation )  . 
 in piccolo , we grouped several candidate mutations in the egfr signalling pathway , allowing a higher - powered comparison of any mutation versus all - wild - type than would be possible for individual mutations . 
this approach panel : research in context systematic review we searched medline using ovidsp for published randomised clinical trials in advanced colorectal cancer involving an anti - egfr monoclonal antibody . 
we identi ed 12 trials that included randomisation to standard treatment plus or minus anti - egfr monoclonal antibodies.13 , 17 , 18 , 2329 in none was kras status determined before randomisation , but for ten trials results have been published by kras status ( usually con ned to codons 1213 ) either within the primary analysis or as a secondary report . 
two useful meta - analyses of these ten trials have been done , drawing attention to a lack of consistency in outcomes , especially among patients with kras wild - type tumours.16 , 30 unexplained antagonistic interactions with other cancer drugs have been proposed : combinations with bevacizumab , capecitabine , or oxaliplatin have produced poor results , whereas single - agent therapy or combinations with irinotecan or uorouracil have had more success . 
another trend , also unexplained , is toward worsening outcomes with earlier stage disease : clear bene t in the third - line setting , lesser bene t in second line , mixed results in rst - line , and negative results in two large surgical adjuvant trials.31 , 32 interpretation our ndings for krasc.12 , 13 , 61 wild - type patients show that prospective molecular strati cation is feasible and gives outcomes consistent with these previous retrospective analyses . 
as in the two previous second - line studies of panitumumab , 24 , 25 we saw improved response rate and progression - free survival , but with no e ect on overall survival . 
for example , randomised trials have shown small , but statistically signi cant , improvements in survival when either bevacizumab33 or a ibercept34 is added to chemotherapy in the second - line setting . 
thus , only if further re nement of molecular selection resulted in a substantial survival bene t from therapeutic antibodies targeting egfr would they become the preferred option in this clinical setting . vol 14 july 2013 articles does not mean that every mutation selected is individually important , nor that the list is exhaustive ; it does , however , provide evidence that interactions exist . 
the choice of mutations was based on their roles as oncogenes in egfr signal transduction , coupled with data from grouped retrospective analyses of non - randomised patients suggesting clinical relevance.15 , 16 least certain is the relevance of pik3ca , where non - randomised data has implicated exon 20 , but not exon 9 , as a negative biomarker.15 the small number of patients with mutations at pik3ca in piccolo precludes rm conclusions ; however , patients with mutations at exon 9 did not bene t from panitumumab , and the sensitivity analysis excluding pik3ca from the list did not alter that nding ( appendix )  . an inconsistent , but nonetheless worrying , nding in trials of anti - egfr monoclonal antibodies is that patients who do not bene t from treatment are potentially harmed . 
 findings of a meta - analysis including ten randomised controlled trials in advanced colorectal cancer showed , although not statistically signi cant , a trend towards worse pfs in patients with kras mutations ( hr 111 , 95% ci 097127 ) ; 17 three of the ten trials showed a statistically signi cant detrimental e ect.3 , 18 , 19 druginteractions with oxaliplatin and speci c adverse bevacizumab have been inferred , although on no basis and with no mechanism proposed , and this has led to a supposition that anti - egfr monoclonal antibodies are better paired with irinotecan than with other drugs.16 that we have now shown in this prospective randomised trial , including irinotecan , but neither oxaliplatin nor bevacizumab , the kras wild - type population contains subpopulations for whom anti - egfr monoclonal antibodies are similarly detrimental . 
the all wild - type population of patients bene ted from panitumumab , with a high response rate ( 70 [ 44% ] of 160 patients ) and improved pfs ( hr 068 ; 95% ci 053086 ) ; but we saw no statistically signi cant di erence in overall survival between the two groups ( gures 4 and 5 )  . 
by contrast with these ndings , in patients with any mutation , we detected a potential detrimental e ect of panitumumab in terms of pfs and of overall survival ( gures 4 and 5 )  . this disparity between e ects on pfs and overall survival is substantiated by our ndings that suggested shorter survival after progression following irinotecan and panitumumab , especially in the any - mutation population ( appendix )  . 
imbalanced post - trial treatment with more e ective salvage of patients in the control group is unlikely to have been a major factor : the use of anti - egfr monoclonal carefully monitored , but these drugs were not funded in the uk at the time of the trial and were received by only 13 ( 6% ) patients in the control group in the 3 months after progression . 
although the fact that full data were not collected for other salvage treatments is a weakness of this study , there is no reason to believe that these would have been imbalanced . 
ascertainment biasa lower antibodies was threshold for diagnosing progression in patients in the control groupis also unlikely , because there was a higher rate of con rmed radiological progression in the control group than in the experimental group ( appendix )  . 
urgent clari cation of subpopulations at risk of harm is important , but positive biomarkers are also needed , to allow a change to a selectin strategy , using anti - egfr monoclonal antibodies in only well - de ned molecular groups with proven e cacy . 
 potential , although not validated , positive biomarkers include egfr ligands20 and egfr copy number.21 , 22 for the individual mutations tested in piccolo , the numbers of patients were insu cient to provide clear results . 
the exception was in patients with mutations in braf , the most common mutation , in whom we detected a detrimental e ect of panitumumab on overall survival ( hr 184 , 95% ci 110308 )  . 
large , but non - randomised , series suggest that anti - egfr monoclonal antibodies are inactive in braf - mutated cancers ; 14 , 15 , 17 however , retrospective analysis of braf status in two randomised trials , although showing a low response rate in patients with braf mutations , showed no evidence of a negative interaction on pfs.2 the data presented here substantiate the activity of anti - egfr monoclonal antibodies in advanced colorectal cancer , but also show the need for selection strategies beyond the current reliance on kras . 
urgent re nement of both negative and positive selection biomarkers using preclinical studies and both retrospective and prospective clinical trial analysis are needed if best use is to be made of an e ective targeted therapy for the bene t of patients . contributors mts was chief investigator of the trial , cowrote the protocol , chaired the trial management group , and cowrote the reports . 
all authors reviewed and approved the nal paper . 758 vol 14 july 2013 articles con icts of interest we declare that we have no con icts of interest . acknowledgments for a list of institutions and principal investigators who contributed patients see the appendix . 
this trial was developed through the national cancer research institute colorectal clinical studies group , funded by cancer research uk and supported by an unrestricted educational grant from amgen inc . 
we also thank the independent trial steering committee ( malcolm mason , chris parker , robin rudd , mahesh parmar , peter johnson , and jeremy whelan ) and data monitoring and ethics committee ( robert coleman , dion morton , john schole eld , and sally stenning ) for their important contributions . corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 corrections correction to lancet oncol 2013 ; 14 : 199209 correction to lancet oncol 2014 ; 15 : e241 esserman lj , thompson im , reid b , et al . 
the de nition of mrd low risk in the summary should read ( undetectable mrd at the end of induction [ day 29 ] or detectable mrd [ less than 001% ] at day 29 that became undetectable by week 11 )  . 
in gure 2 and in the rst paragraph of the results section , 1732 patients were clinical standard risk , 989 patients were risk , clinical 405 patients were clinical high risk . 
also in gure 2 , 2721 patients were eligible for mrd strati cation , 820 patients had indeterminate mrd status , 808 had high - risk mrd , 1059 had low - risk mrd , 34 patients had died within 35 days or had never remitted , and 323 patients were identi ed after august , 2009 . 
for the mrd low risk patients in table 1 , the total number of patients should read 1059 , of whom 466 were female , 764 were aged 29 years , 978 were b - lineage , 673 ( 64% ) were standard nci risk , 494 ( 47% ) had a white blood cell count less than 10 109 cells per l , and 177 had a white blood cell count of 1019 109 cells per l . 
the last sentence of the sixth paragraph of the results should read additionally , we noted no di erence between patients with undetectable mrd and those with less than 0005% mrd at day 29 . 
 these corrections have been made to the online version of the article as of june 30 , 2014 . vol 15 july 2014 e308 correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections concurrent once - daily versus twice - daily chemoradiotherapy in patients with limited - stage small - cell lung cancer ( convert ) : an open - label , phase 3 , randomised , superiority trial corinne faivre - finn , michael snee , linda ashcroft , wiebke appel , fabrice barlesi , adityanarayan bhatnagar , andrea bezjak , felipe cardenal , pierre fournel , susan harden , cecile le pechoux , rhona mcmenemin , nazia mohammed , mary obrien , jason pantarotto , veerle surmont , jan p van meerbeeck , penella j woll , paul lorigan , fiona blackhall , for the convert study team summary background concurrent chemoradiotherapy is the standard of care in limited - stage small - cell lung cancer , but the optimal radiotherapy schedule and dose remains controversial . 
the aim of this study was to establish a standard chemoradiotherapy treatment regimen in limited - stage small - cell lung cancer . methods the convert trial was an open - label , phase 3 , randomised superiority trial . 
we enrolled adult patients ( aged 18 years ) who had cytologically or histologically confirmed limited - stage small - cell lung cancer , eastern cooperative oncology group performance status of 02 , and adequate pulmonary function . 
patients were randomly assigned to receive either 45 gy radiotherapy in 30 twicedaily fractions of 15 gy over 19 days , or 66 gy in 33 once - daily fractions of 2 gy over 45 days , starting on day 22 after commencing cisplatinetoposide chemotherapy ( given as four to six cycles every 3 weeks in both groups )  . 
a 12% higher overall survival at 2 years in the once - daily group versus the twice - daily group was considered to be clinically significant to show superiority of the once - daily regimen . 
the study is registered with clinicaltrials . gov ( nct00433563 ) and is currently in follow - up . findings between april 7 , 2008 , and nov 29 , 2013 , 547 patients were enrolled and randomly assigned to receive twice - daily concurrent chemoradiotherapy ( 274 patients ) or once - daily concurrent chemoradiotherapy ( 273 patients )  . 
 four patients ( one in the twice - daily group and three in the once - daily group ) did not return their case report forms and were lost to follow - up ; these patients were not included in our analyses . 
at a median follow - up of 45 months ( iqr 3558 ) , median overall survival was 30 months ( 95% ci 2434 ) in the twice - daily group versus 25 months ( 2131 ) in the once - daily group ( hazard ratio for death in the once daily group 118 [ 95% ci 095145 ] ; p = 014 )  . 
 2 - year overall survival was 56% ( 95% ci 5062 ) in the twice - daily group and 51% ( 4557 ) in the once - daily group ( absolute difference between the treatment groups 53% [ 95% ci 32% to 137% ] )  . 
the most common grade 34 adverse event in patients evaluated for chemotherapy toxicity was neutropenia ( 197 [ 74% ] of 266 patients in the twice - daily group vs 170 [ 65% ] of 263 in the once - daily group )  . 
most toxicities were similar between the groups , except there was significantly more grade 4 neutropenia with twice - daily radiotherapy ( 129 [ 49% ] vs 101 [ 38% ] ; p = 005 )  . 
in patients assessed for radiotherapy toxicity , was no difference in grade 34 oesophagitis between the groups ( 47 [ 19% ] of 254 patients in the twice - daily group vs 47 [ 19% ] of 246 in the once - daily group ; p = 085 ) and grade 34 radiation pneumonitis ( 4 [ 3% ] of 254 vs 4 [ 2% ] of 246 ; p = 070 )  . 
11 patients died from treatment - related causes ( three in the twice - daily group and eight in the once - daily group )  . interpretation survival outcomes did not differ between twice - daily and once - daily concurrent chemoradiotherapy in patients with limited - stage small - cell lung cancer , and toxicity was similar and lower than expected with both regimens . 
since the trial was designed to show superiority of once - daily radiotherapy and was not powered to show equivalence , the implication is that twice - daily radiotherapy should continue to be considered the standard of care in this setting . funding cancer research uk ( clinical trials awards and advisory committee ) , french ministry of health , canadian cancer society research institute , european organisation for research and treatment of cancer ( cancer research fund , lung cancer , and radiation oncology groups )  . copyright the author ( s )  . 
we searched pubmed and the abstracts of major conferences ( such as the american society of clinical oncology ) with the terms small cell lung cancer , limited - stage , radiotherapy ( or irradiation ) , and chemotherapy , with no constraints imposed on the timeframe for the search , for randomised evidence to support this practice . 
we found only one relevant randomised clinical trial comparing once - daily and twice - daily radiotherapy . added value of this study although twice - daily radiotherapy has produced the best outcomes in these patients so far , concerns about its toxicity , logistical issues in the delivery of twice - daily radiotherapy , and the low radiation dose used in the control group of the intergroup 0096 study have resulted in the poor adoption of this regimen and no consensus on the standard treatment to use in the routine setting . 
 furthermore , the results of this study show that in the era of modern radiotherapy techniques , the frequency and severity of acute and late radiation toxicities are lower than previously reported . implications of all the available evidence results from this study showed that twice - daily radiotherapy should be considered standard - of - care in patients with limitedstage small - cell lung cancer . 
this article provides updated information on expected treatment toxicity that clinicians can relay to their patients . introduction small - cell lung cancer is characterised by its rapid tumour doubling time , early dissemination , and high response rate to both chemotherapy and radiotherapy . 
of the 42 000 patients in the uk and 225 000 in the usa diagnosed with lung cancer every year , 15% have small - cell lung cancer and 30% of those have limited - stage disease that can be encompassed within a tolerable radiotherapy field.1 even in this early - stage disease , outcomes are poor , with median survival of 1624 months after curative intent treatment and 2 - year survival of less than 50%.24 combined chemotherapy and thoracic radiotherapy is the standard treatment for limited - stage small - cell lung cancer . 
subsequently , metaanalyses of clinical trials investigating the optimal timing and sequencing of chemoradiotherapy have shown an advantage for early concurrent thoracic radiotherapy.711 furthermore , twice - daily radiotherapy was superior to once - daily radiotherapy in the landmark intergroup 0096 study.4 in that study , patients were randomly assigned to receive either 45 gy once - daily ( 18 gy per fraction ) for 5 weeks or 45 gy twice - daily ( 15 gy per fraction ) for 3 weeks . 
 twice - daily radiotherapy significantly improved 5 - year overall survival compared with once - daily radiotherapy ( 26% vs 16% ) and reduced the risk of thoracic relapse ( 36% vs 52% ) but at the cost of increased severe radiation oesophagitis ( 32% vs 16% )  . 
consequently , twice - daily radiotherapy concurrently with chemotherapy was adopted as a standard of care for limited - stage small - cell lung cancer.12 however , it is unclear whether twice - daily radiotherapy resulted in better outcomes because of the increase in the biologically effective dose of radiation or because of shorter overall treatment time , which is rapidly proliferating disease . 
 important radiotherapy the techniques have evolved intergroup 0096 study was designed in the late 1980s ; specifically , the use of ct - planned conformal treatment and the omission of elective nodal irradiation to reduce normal toxicity , particularly oesophagitis . tissue exposure and since this although twice - daily radiotherapy concurrently with chemotherapy has produced the best outcomes so far , concerns about its toxicity , logistical issues in its delivery , and the low radiation dose in the control group of the intergroup 0096 study , resulting in a very high ( 52% ) local failure rate , have resulted in the poor adoption of this regimen and no consensus on the standard treatment to use in the routine setting.13 the authors of one study14 suggested that the local control could be improved with a higher dose of once - daily radiotherapy . 
the convert trial was therefore designed as a superiority trial to improve on the standard of care for limited - stage smallcell lung cancer by comparing twice - daily radiotherapy to a higher dose of radiotherapy delivered once daily , given concurrently with chemotherapy . methods study design and participants the convert trial was an international , multicentre , open - label , randomised phase 3 superiority trial . 
details of the trial design have been published previously.15 patients were recruited at 73 centres in eight countries vol 18 august 2017 1117 articles see online for appendix ( belgium , canada , france , netherlands , poland , slovenia , spain , and the uk ; appendix pp 12 )  . eligible patients were aged 18 years or older ; had histologically or cytologically confirmed small - cell lung cancer with limited disease ( as defined by the veterans administration lung cancer study groupie , patients whose disease can be encompassed within a radical radiation portal ) ; 16 had an eastern cooperative oncology group performance status of 0117 or performance status of 2 due to disease - related symptoms and not comorbidities ( since small - cell lung cancer is characterised by rapid doubling time and central disease location , which can be associated with a sudden change in performance status ) ; had no malignant pleural or pericardial effusions ; and had acceptable radiotherapy target volume ( according to the local radiotherapist )  . 
eligible patients had a maximum of one adverse biochemical factor ( concentrations of serum alkaline phosphatase > 15 - times the upper limit of normal , serum sodium < lower limit of normal , and serum lactate dehydrogenase > the upper limit of normal ) , forced expiratory volume in 1 s greater than 1 l or 40% predicted value , and transfer factor for carbon monoxide greater than 40% predicted value . 
patients with a previous history of malignancy in the past 5 years ( except for non - melanomatous skin or insitu cervix carcinoma ) and those with previous or concomitant illness or treatment that , in the opinion of the investigator , would interfere with the trial treatments or comparisons were excluded . participants gave written informed consent and the study was done according to the declaration of helsinki and good clinical practice guidelines . 
the trial was reviewed in the uk by the national research ethics service committee north westgreater manchester central , which granted ethics approval for the study on dec 21 , 2007 ( rec reference : 07 / h1008 / 229 )  . 
the protocol was also approved by the institutional review board or research ethics committee in each country and at each study centre . randomisation and masking patients were randomly assigned ( 1 : 1 ) to one of the two treatment groups ( twice - daily vs once - daily radiotherapy )  . 
 the factors controlled for in the allocation were institution , planned number of chemotherapy cycles ( four vs six ) , and performance status ( 01 vs 2 )  . 
 investigators were not masked procedures at baseline , all patients underwent baseline investigations , which included physical examination , chest radiograph , ct scan of the thorax and upper abdomen , ct or mri of the brain , full blood count , biochemical profile , and lung function tests . 
staging was done using the union for international cancer control / american joint committee on cancer classification system.18 patients were randomly assigned to receive radiotherapy either twice - daily ( 45 gy in 30 twice - daily fractions of 15 gy , with a minimum of 6 h between fractions , over 19 days , on 5 consecutive days a week ) or once - daily ( 66 gy in 33 daily fractions of 2 gy over 45 days , on 5 consecutive days a week ) , concurrently with chemo therapy . 
chemotherapy was started within 4 weeks of randomisation and consisted of four to six cycles of cisplatin and etoposide every 3 weeks in both groups ( etoposide 100 mg / m intravenously on days 13 and cisplatin 75 mg / m intravenously on day 1 , or etoposide 100 mg / m intravenously on days 13 and cisplatin 25 mg / m intravenously on days 13 )  . 
no later than 6 weeks after the last cycle of chemotherapy , patients without evidence of progressive disease on the ct scan and with no clinical evidence of brain metastases were offered prophylactic cranial irradiation . radiotherapy commenced on day 22 of cycle one of chemotherapy , coinciding with cycle two of chemotherapy in patients not experiencing chemotherapy delay due to toxicity . 
however , we recommended a chemotherapy treatment delay of more than 7 days for grade 4 febrile neutropenia , grade 4 thrombocytopenia requiring medical intervention , or grade 2 or worse bleeding with thrombocytopenia ; for the first episode of such an event , we recommended full - dose chemotherapy and granulocyte colony - stimulating factor support , or a 20% dose reduction . 
 a radiotherapy quality assurance programme was set up to ensure the robustness of the radiotherapy procedures , and the details of the programme have been reported previously.15 the programme was managed by the uk national cancer research institute radiotherapy trials quality assurance team . 1118 vol 18 august 2017 articles 274 allocated to receive twice - daily concurrent chemoradiotherapy 273 allocated to receive once - daily concurrent chemoradiotherapy 547 patients randomly assigned 7 progressive disease or died 25 did not receive concurrent chemoradiotherapy ( 20 no radiotherapy and 5 received sequential chemoradiotherapy ) 5 tumour volume too large 4 randomisation error 4 patient withdrawal or lost to follow - up 3 chemotherapy toxicity 2 oncologist decision 10 progressive disease or died 33 did not receive concurrent chemoradiotherapy ( 26 no radiotherapy , 6 received sequential chemoradiotherapy , and 1 unknown ) 7 oncologist decision 7 tumour volume too large 5 patient withdrawal or lost to follow - up 3 randomisation error 1 unknown 249 received concurrent chemoradiotherapy 1 received once - daily chemoradiotherapy 240 received concurrent chemoradiotherapy 6 received twice - daily chemoradiotherapy 1 lost to follow - up ( did not return case report form ) 3 lost to follow - up ( did not return case report form ) 273 included in survival analysis 254 included in radiotherapy toxicity analysis ( concurrent and sequential chemoradiotherapy ) 266 included in chemotherapy toxicity analysis 270 included in survival analysis 246 included in radiotherapy toxicity analysis ( concurrent and sequential chemoradiotherapy ) 263 included in chemotherapy toxicity analysis figure 1 : trial profile * one patient withdrew consent for twice - daily radiotherapy . 
 on completion of study treatment , patients were followed up weekly until the resolution of acute sideeffects , then every 3 months until 1 year , and every 6 months for 5 years . 
subsequently , during followup at 6 and 12 months after randomisation , investigations included physical evaluation , reporting of adverse events , and a ct scan of the thorax and abdomen . 
follow - up investigations were done according to local policy . outcomes the primary outcome of the study was overall survival , defined as time from randomisation until death from any cause . 
secondary outcomes included compliance with chemotherapy and radiotherapy ( defined as dose intensity delivered ) , acute toxicity ( defined as toxicity occurring between the start of treatment and up to 3 months after completion of treatment , and assessed according to the common terminology criteria for adverse events [ version 3.0 ] ) , late toxicity ( according to the common terminology criteria for adverse events [ version 3.0 ] ) , 19 local and metastatic progression - free survival and ( calculated from date of randomisation to date of first clinical or radiological evidence of progressive disease at the primary site or distant sites )  . 
all serious adverse events were reported to the trial coordinating centre and were assessed for causality and expectedness , both locally by the principal investigator and centrally by the chief investigator . statistical analysis our hypothesis was that overall survival in the once - daily chemoradiotherapy group would be superior to that of the twice - daily group . 
a 12% higher overall survival at 2 years in the once - daily group versus the twice - daily group was considered to be clinically significant to show superiority of the once - daily regimen . 
overall and the progression - free survival were estimated with kaplan - meier method , and between - group comparisons vol 18 august 2017 1119 articles evaluated by the log - rank test with stratification for institution , planned number of chemotherapy cycles ( four vs six ) , and performance status ( 01 vs 2 )  . 
the number of events required to detect a hazard ratio ( hr ) for death of 07 with an level ( two - sided ) of 005 and 80% power ( ie , an increase in 2 - year survival from 44% in the twice - daily radiotherapy group to 56% in the oncedaily radiotherapy group ) was 247 . 
 * eastern cooperative oncology group performance status was not recorded on the source documentation and case report form in three cases at baseline ; in all three cases , the performance score was recorded as 01 on the randomisation fornever smokers defined as adults who have never smoked a cigarette or who smoked fewer than 100 cigarettes in their entire lifetime ; former smokers defined as adults who have smoked at least 100 cigarettes in their lifetime but say they currently do not smoke ; current smokers defined as adults who have smoked 100 cigarettes in their lifetime and currently smoke cigarettes every day ( daily ) or on some days ( non - daily )  . table 1 : baseline characteristics added to the sample size of 506 patients to allow for ineligible patients , giving a total recruitment target of 532 patients . 
the primary survival outcome was analysed using the modified intention - to - treat principle , because four cases provided no follow - up data and hence were censored at time zero . 
further details about the statistical analysis are available in the protocol.15 all randomly assigned patients who were treated with at least one study dose of chemotherapy and who were alive at the time of the first toxicity assessment were included in the safety analysis . 
 the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results between april 7 , 2008 , and nov 29 , 2013 , we recruited 547 patients from 73 centres in eight countries . 
the median age at randomisation was 62 years ( iqr 2984 ) in the twice - daily group and 63 years ( 3481 ) in the once - daily group , with 83 ( 15% ) of 547 patients being older than 70 years ( 32 [ 12% ] in the twice - daily group and 51 [ 19% ] in the once - daily group )  . 
less than 2% of patients were never smokers , almost two - thirds were former smokers , and just over a third were current smokers ( table 1 )  . 
312 ( 57% ) of 547 patients were staged with pet / ct , and 426 ( 78% ) of 547 were stage iii according to the union for international cancer control classification ( table 1 )  . the number of planned cycles of chemotherapy was four for most patients ( table 1 )  . 
 1120 vol 18 august 2017 articles 164 ( 60% ) of 273 patients in the twice - daily group had died , compared with 176 ( 65% ) of 270 patients in the once - daily group . in our survival analysis ( which included 273 patients in the twice - daily group and 270 in the once - daily group ) , median overall survival was 30 months ( 95% ci 2434 ) in the twice - daily group and 25 months ( 2131 ) in the oncedaily group ( hazard ratio 118 [ 95% ci 095145 ] ; p = 014 ; figure 2a )  . 
2 - year overall survival was 56% ( 95% ci 5062 ) in the twice - daily group and 51% ( 4557 ) in the once - daily group ( absolute difference between the treatment groups 53% [ 95% ci 32% to 137% ] )  . 
5 - year overall survival was 34% ( 95% ci 2741 ) in the twice - daily group and 31% ( 2537 ) in the once - daily group ( absolute difference 28% [ 95% ci 64% to 120% ] )  . 
in the twice - daily group versus the once - daily group , causes of death were lung cancer ( 152 vs 146 ) , intercurrent deaths ( six vs 14 ) , treatmentrelated ( three vs eight ) , and cardiovascular ( three vs eight ) ; causes of the 12 treatment - related deaths were radiation pneumonitis ( one vs two ) , dementia possibly related to prophylactic cranial irradiation ( none vs one ) , neutropenic sepsis ( one vs three ) , septic shock ( one vs none ) , bronchial pneumonia ( none vs two ) , and peripheral vascalar ischaemia ( one vs none )  . 
 intensity - modulated 25 ( 9% ) of 273 patients in the twice - daily radiotherapy group and 33 ( 12% ) of 270 in the once - daily radiotherapy group did not receive concurrent chemoradiotherapy ( figure 1 ) , giving compliance rates of 91% in the twicedaily group and 88% in the once - daily group . 
less than 10% of patients did not receive any radiotherapy ( 20 [ 7% ] in the twice - daily group and 26 [ 10% ] in the once - daily group ; figure 1 , table 2 )  . 
of the patients who received radiotherapy was radiotherapy , delivered to 40 ( 16% ) of 254 participants in the twice - daily group versus 43 ( 17% ) of 247 participants in the once - daily group . 
 more patients received the full dose of radiotherapy in the twice - daily group than in the once - daily group ( p < 00001 ; table 3 )  . 
the optimal number of fractions , as defined in the protocol , 15 ( 30 fractions in the twice daily group and 33 in the once daily group ) were delivered in 213 ( 86% ) of 249 patients in the twice - daily group and 192 ( 80% ) of 240 patients ( p = 010 )  . 
 radiotherapy was delivered over the planned overall treatment time of 19 days in 158 ( 63% ) of 249 patients in the twice - daily group and over the planned overall treatment time of 45 days in 114 ( 48% ) of 240 patients in the once - daily group ( p = 00004 )  . 
protocol deviations and violations were mainly due to logistical reasons , such as public holidays . the once - daily group at the time of analysis , 181 ( 66% ) of 273 patients in the twice - daily group and 189 ( 70% ) of 270 patients in the once - daily group had disease progression ( p = 026 )  . 
median local progression - free survival was 207 months ( 95% ci 161279 ) in the twice - daily group versus 179 months ( 153217 ) in the once daily group ( figure 2b ) and median metastatic progression - free survival was 202 months ( 95% ci 159253 ) versus 166 months ( 137218 )  . 
 the difference between groups for local progressionfree survival ( p = 020 ) and metastatic progression - free survival ( p = 024 ) was not significant ( figure 2 )  . 
there was no notable difference between groups in treatment received at the time of progression ( appendix p 4 )  . chemotherapy toxicity was assessed in 266 ( 97% ) of 273 patients in the twice - daily group and 263 ( 97% ) of 270 patients in the once - daily group , who had received at least one cycle of chemotherapy and who were alive at the time of the first toxicity assessment ( figure 1 , table 4 )  . 
the frequencies of most adverse events recorded were similar in both groups , with the exception that significantly more grade 4 neutropenia was recorded in the twice - daily group than in the once - daily group ( 129 [ 49% ] vs 101 [ 38% ] ; p = 005 )  . 
acute radiotherapy toxicity was similar in both groups : grade 34 oesophagitis was reported in 47 ( 18% ) of 254 patients in the twice - daily group and 47 ( 19% ) of 246 patients in the once - daily group . 
 11 patients developed grade 35 radiation pneumonitis ( five in the twice daily group and six in the once daily group ) , of whom three patients died within 3 months of radiotherapy ( two in the once - daily group and one in the twice - daily group , one of whom received sequential rather than concurrent radiotherapy ; table 4 , appendix p 3 )  . 
six patients in each group developed grade 34 pneumonitis , and five patients ( three in the twice - daily group and two in the once - daily group ) developed grade 3 pulmonary fibrosis ( table 5 )  . discussion our results show that once - daily radiotherapy did not improve overall survival in patients with limited - stage small - cell lung cancer and good performance status , compared with twice - daily radiotherapy , when given concurrently with chemotherapy . 
 however , although results are unable to show superiority of the once - daily radiotherapy regimen , the convert trial should have a major effect on the standardisation of chemoradiotherapy in this disease groupa treatment that has been the subject of controversy since the publication of the intergroup 0096 study.4 , 13 overall survival with both regimens were higher than the survival results reported in the intergroup 0096 study . 
in convert , 2 - year survival for twice - daily and once - daily radiotherapy was 56% and 51% , versus 47% and 41% in the intergroup 0096 study.4 convert was not an equivalence study ( and was not powered for equivalence ) so it cannot be concluded that the two regimens have the same efficacy . 
 furthermore , the 2 - year survival of 56% achieved in the control group with twice - daily radiotherapy is the same survival that was projected for the experimental group . 
the radiotherapy toxicity population was used to analyse the prevalence of these adverse events because it would not be possible to report radiotherapy - related toxicity in patients who did not receive radiotherapy . 
two deaths ( peripheral arterial ischaemia [ n = 1 ] in the twice - daily group and dementia possibly related to prophylactic cranial irradiation [ n = 1 ] in the once - daily group )  . 
 table 4 : acute adverse events ( 3 months after completion of study treatment ) groups might be explained by several changes in the management of small - cell lung cancer since the publication of the intergroup study , including pet / ct staging in more than half of patients , the use of modern and precise radiotherapy techniques , and improvements in supportive care . 
these results , together with several meta - analyses and systematic overviews , support the use of short overall radiotherapy treatment time to avoid early cancer cell repopulation.711 one of the systematic overviews also identified that time from the start of any treatment to completion of radiotherapy is a key variable in predicting outcome.20 although not significant , 2 - year overall survival was slightly higher in the twice - daily group than in the once - daily group , which could possibly be a result of improved delivery of treatment in the twice - daily group ( n = 248 ) once - daily group ( n = 233 ) p value * grade 12 grade 3 grade 4 grade 12 grade 3 grade 4 dermatitis oesophagitis oesophageal stricture or fistula 15 ( 6% ) 29 ( 12% ) 8 ( 3% ) 17 ( 7% ) 39 ( 17% ) 4 ( 2% ) 6 ( 3% ) 1 ( < 1% ) 2 ( 1% ) 5 ( 2% ) 006 048 > 099 078 pulmonary fibrosis 119 ( 48% ) 3 ( 1% ) 106 ( 46% ) pneumonitis 71 ( 29% ) 5 ( 2% ) 1 ( < 1% ) 70 ( 30% ) 1 ( < 1% ) 090 myelitis other 1 ( < 1% ) 8 ( 3% ) 131 ( 53% ) 20 ( 8% ) 3 ( 1% ) 113 ( 49% ) 18 ( 8% ) 2 ( 1% ) data are n ( % )  . 
 table 5 : late adverse events ( > 3 months after study treatment ) vol 18 august 2017 1123 articles twice - daily group , with more patients receiving full - dose radiotherapy , the optimal planned number of fractions , and treatment delivered over the optimal treatment time . 
another reason why treatment delivery was superior in the twice - daily group is because of the lower overall dose of radiotherapy in this group , which meant it was possible to achieve the protocol dose constraints for organs at risk , such as lung and spinal cord , in a greater proportion of patients than in the once - daily group . 
a further advantage of the twice - daily regime is that it halves the radiotherapy treatment time ( from 45 days to 19 days ) and reduces the number of fractions ( from 33 to 30 ) compared with the once - daily regimen . 
 although no formal health economic analysis has been done as part of this study , the delivery of twice - daily radiotherapy could lead to cost savings , especially if patients require hospital transport to attend radiotherapy appointments . overall , the frequency and severity of acute and late radiation toxicities were lower than expected , probably because of the use of modern radiotherapy techniques , including 3d radiotherapy or intensity - modulated radiotherapy , and treatment of involved fields with regard to nodal disease . 
in the intergroup 0096 trial , 4 patients were treated with outdated radiotherapy techniques including elective nodal irradiation , which would have resulted in higher radiation exposure of normal tissues than in this trial . 
indeed , the high rate of severe acute oesophagitis ( 32% with twice - daily radiotherapy ) in the intergroup study has been cited as the main reason for poor adoption of twice - daily radiotherapy.13 by contrast , less than 20% of patients had severe oesophagitis in the convert study and only one patient developed an oesophageal stricture requiring intervention . 
radiation pneumonitis was not specifically reported in the intergroup 0096 study , but in this trial very few ( < 3% ) patients had severe radiation pneumonitis or severe pulmonary fibrosis . 
the lower than anticipated toxicity rates and rates of local failure reported in this study suggest that radiotherapy treatment delivered concurrently with chemotherapy could be intensified furtherfor example , by means of dose escalation or hypofractionation . a limitation of this study is that although we did not mandate an upper age limitwith the aim to gather much needed evidence about the outcome of elderly patients treated with concurrent chemoradiotherapy only 15% of the patients included were older than 70 years . 
data for patients older than 70 years participating in convert was presented at the international association for the study of lung cancer 17th world conference on lung cancer in vienna , austria , in 2016 , and the results of this analysis will be presented in a separate report . 
elderly patients have been reported to be less likely to receive concurrent chemoradiotherapy than their younger counterparts , which is mainly due to insufficient high - quality evidence to support the use of this potentially toxic treatment.21 another limitation is that the majority of patients enrolled in both groups were white , and therefore the results of the study might not be applicable to other ethnicities . to our knowledge , convert is the largest study completed investigating thoracic radiotherapy in limitedstage small - cell lung cancer , and the first clinical trial in this group of patients to report on the outcome of patients treated with modern radiotherapy techniques incorporating a quality assurance programme . 
furthermore , by contrast with us practice , concurrent chemoradiotherapy is not always adopted as the standard of care for limited - stage smallcell lung cancer in europe , and the study provided an incentive for centres to adopt and set up concurrent treatment protocols . given the importance of keeping overall treatment time as short as possible , future studies could investigate doseescalated twice - daily or hypofractionated radio therapy concurrently with chemotherapy . 
further data for the outcome of patients treated with high - dose 2 gy per fraction treatment will be provided by the ongoing calgb 30610 / rtog 0538 study ( nct00632853 )  . 
the upcoming analysis of the convert translational studies , including the prognostic role of baseline circulating tumour cells , could provide data for relevant biological stratification factors that can be used prospectively in future studies . in conclusion , the results of convert show that there were no significant differences in survival and no major differences in toxicity between twice - daily and once - daily radiotherapy . 
however , since the trial was designed to show superiority of once - daily radiotherapy and not powered to show equivalence , twice - daily to be considered radiotherapy should continue standard - of - care . 
from a pragmatic perspective , oncedaily radiotherapy could be considered when delivery of twice - daily radiotherapy is impossible because of departmental logistics or patient choice . contributors cf - f , la , pl , ms , fbl , rm , nm , and pjw conceived the study and initiated the study design . 
the authors designed the trial , analysed the data , wrote the manuscript ( with the first draft written by the first author ) , made the decision to submit the manuscript for publication , and assured the completeness and accuracy of the data and analysis and of the fidelity of this report to the trial protocol . 
all authors approved the final manuscript . declaration of interests cf - f , la , pl , and fbl report grants from cancer research uk during the conduct of this study . 
the other authors declare no completing interests . 1124 vol 18 august 2017 articles acknowledgments this study was funded by the cancer research uk clinical trials awards and advisory committee ( grant reference number c17052 / a8154 ) , frenchministry of health , programme hospitalier de recherch clinique ( grant reference number nat 2007 - 28 - 01 ) , canadian cancer society research institute ( grant reference number 021039 ) , and the european organisation for the research and treatment of cancer ( cancer research fund , lung cancer , and radiation oncology groups )  . 
 the authors would like to acknowledge the support of the national cancer research institute radiotherapy trials quality assurance team ( nicki groom and elena wilson ) ; the manchester academic health science centre clinical trials unit ; sally falk and amy bossons ( convert trial coordinators ) ; david ryder ( manchester academic health science centre trials co - ordination unit statistician ) ; the national institute for health research ( nihr ) christie clinical research facility ; david girling , steve roberts , christian manegold , and robert huddart ( independent data monitoring committee members ) ; and dirk de ruysscher and jason lester ( independent members of the trial steering committee )  . 
the views expressed are those of the authors and not necessarily those of the nhs , nihr , or the department of health . articles gemcitabine and capecitabine with or without telomerase peptide vaccine gv1001 in patients with locally advanced or metastatic pancreatic cancer ( telovac ) : an open - label , randomised , phase 3 trial gary middleton , paul silcocks , trevor cox , juan valle , jonathan wadsley , david propper , fareeda coxon , paul ross , srinivasan madhusudan , tom roques , david cunningham , stephen falk , nick wadd , mark harrison , pippa corrie , tim iveson , angus robinson , karen mcadam , martin eatock , je evans , caroline archer , tamas hickish , angel garcia - alonso , marianne nicolson , william steward , alan anthoney , william greenhalf , victoria shaw , eithne costello , dean naisbitt , charlotte rawcli e , gemma nanson , john neoptolemos summary background we aimed to assess the e cacy and safety of sequential or simultaneous telomerase vaccination ( gv1001 ) in combination with chemotherapy in patients with locally advanced or metastatic pancreatic cancer . methods telovac was a three - group , open - label , randomised phase 3 trial . 
 eligible patients were treatment naive , aged older than 18 years , with locally advanced or metastatic pancreatic ductal adenocarcinoma , and eastern cooperative oncology group performance status of 02 . 
patients were randomly assigned ( 1 : 1 : 1 ) to receive either chemotherapy alone , chemotherapy with sequential gv1001 ( sequential chemoimmunotherapy ) , or chemotherapy with concurrent gv1001 ( concurrent chemoimmunotherapy )  . 
chemotherapy included six cycles of gemcitabine ( 1000 mg / m , 30 min intravenous infusion , at days 1 , 8 , and 15 ) and capecitabine ( 830 mg / m orally twice daily for 21 days , repeated every 28 days )  . 
sequential chemoimmunotherapy included two cycles of combination chemotherapy , then an intradermal lower abdominal injection of granulocyte - macrophage colony - stimulating factor ( gm - csf ; 75 g ) and gv1001 ( 056 mg ; days 1 , 3 , and 5 , once on weeks 24 , and six monthly thereafter )  . 
this study is registered as an international standard randomised controlled trial , number isrctn4382138 . findings the rst patient was randomly assigned to treatment on march 29 , 2007 , and the trial was terminated on march 27 , 2011 . 
of 1572 patients screened , 1062 were randomly assigned to treatment ( 358 patients were allocated to the chemotherapy group , 350 to the sequential chemoimmunotherapy group , and 354 to the concurrent chemoimmunotherapy group )  . 
median overall survival was not signi cantly di erent in the chemotherapy group than in the sequential chemoimmunotherapy group ( 79 months [ 95% ci 7188 ] vs 69 months [ 6476 ] ; hazard ratio [ hr ] 119 , 9825% ci 097148 , p = 005 ) , or in the concurrent chemoimmunotherapy group ( 84 months [ 95% ci 7397 ] , hr 105 , 9825% ci 085129 , p = 064 ; overall log - rank of 2df = 43 ; p = 011 )  . 
results from studies in other patients with cancer have shown that gv1001 induces the expression of cd8 cytotoxic t cells and can initiate epitope spreading.1013 although cytotoxic drugs are generally regarded as immunosuppressive , some chemotherapy regimens might potentiate the e ect of cancer vaccines.1419 gemcitabine and uorouracil induce apoptosis of cancer cells leading to the release of antigens that can be taken up by professional antigen - presenting cells , and cross - presented to prime cytotoxic t cells.14 , 20 ligation of cd40 on antigen - presenting cells with cd40l present on activated cd4 cells determines the generation of cytotoxic t cells . 
gv1001 vaccination was expected to generate telomerase - speci c t - helper cells to activate several antigen - presenting cells loaded with diverse antigens , to prime and activate cytotoxic t cells with a broad repertoire . 
synergy between cd40 ligation and gemcitabine is highest when gemcitabine is given before cd40 ligation.21 chemotherapy delivered after immuno therapy can enhance the e ect of immunotherapy by delivering a bolus of tumour antigens and immuno stimulatory signals.15 thus from preclinical studies showed synergy between gemcitabine and both cd40 agonism and vaccines in vitro and in mice.14 , 15 , 21 results the combination of gemcitabine and capecitabine ( an orally active uorouracil pro - drug ) is a standard of care for patients with pancreatic cancer , with improved objective response and time to progression compared with gemcitabine monotherapy.22 the design of the telovac study was based on the clear clinical evidence of immunogenicity of gv1001 in patients with pancreatic cancer , the available preclinical data showing the synergy of gemcitabine with cancer vaccines and the other positive immunomodulatory e ects of gemcitabine and uoropyrimidines . 
thus the telovac study aimed to exploit the positive immunomodulatory e ects of these agents and tested the e ect of combining them with gv1001 with granulocyte - macrophage colony - stimulating factor ( gm - csf ) as an adjuvant.23 methods study design and participants telovac was a multicentre , three - group , open - label , phase 3 randomised controlled trial done at 51 uk hospitals . 
the protocol can be viewed online . eligible patients were treatment naive , aged older than 18 years , with histologically or cytologically con rmed locally advanced or metastatic pancreatic ductal adenocarcinoma , an eastern cooperative oncology group ( ecog ) performance status of 02 , and adequate end organ function . 
other speci c inclusion criteria were locally advanced or metastatic disease precluding curative surgical resection or patients who had relapsed following previously resected pancreatic cancer ; contrast enhanced ct scan of the thorax , abdomen , and pelvis within 28 days before commencing treatment ; uni dimensionally measurable disease on ct in accordance with the response evaluation criteria in solid tumors ( recist 1.0 ) guidelines ; platelet count equal or higher than 100 10 cells per l , white blood cell count ( wbc ) equal or higher than 3 10 cells per l , and neutrophil count equal or higher than 15 10 cells per l at entry ; serum bilirubin equal or lower than 35 mol / l ; calculated creatinine clearance higher than 50 ml / min ( cockcroft and gualt ) ; and a life expectancy longer than 3 months . 
the estimated median survival of eligible patients was 71 months ( 95% ci 6278 ) .22 we excluded patients if they had had radiotherapy within the last 4 weeks before start of study treatment ; no other pre - treatment information on radiotherapy was obtained as radiotherapy was not used in the uk for locally advanced pancreatic cancer . 
speci c exclusion criteria were medical or psychiatric conditions compromising informed consent ; intracerebral metastases or meningeal carcinomatosis ; clinically signi cant serious disease or organ system disease not currently controlled on present therapy ; uncontrolled angina pectoris ; pregnancy or breastfeeding ; previous chemotherapy for locally advanced and metastatic disease ; concurrent malignancies or invasive cancers diagnosed within the past 5 years apart from adequately treated basal - cell carcinoma of the skin , in - situ carcinoma of the uterine cervix , or resected pancreatic cancer ; known malabsorption syndromes ; hyper sensitivity to any of the investigational products or patients with a dihydropyrimidine dehydrogenase de ciency ; medi cation that might a ect immuno competence such as long - term steroids or other immunosuppressants for an unrelated condition ; men or women of reproductive potential , unless using at least two contraceptive precautions , one of which must be a condom . the trial conformed the international conference on harmonisation on good the principles of 830 vol 15 july 2014 articles for the protocol see asp ? id = 42&tgcode = 4&menuid = 43 see online for appendix clinical practice , and was undertaken by the cancer research uk liverpool cancer trials unit ; pharmacovigilance was subcontracted to orion clinical services ltd ( slough , uk )  . 
all participants provided written , informed consent before randomisation . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to receive either chemotherapy alone , chemotherapy with sequential gv1001 ( sequential chemoimmunotherapy group ) , or chemotherapy with concurrent gv1001 ( concurrent chemo immunotherapy group )  . 
the allocation sequence was generated by the then trial statistician and was held centrally with access restricted to the senior statistician , the senior trial co - ordinator , and the data managers . 
all patients and investigators were aware of the treatment allocation . procedures patients randomly assigned to the chemotherapy group received gemcitabine ( 1000 mg / m , 30 min intravenous infusion on days 1 , 8 , and 15 ) and capecitabine ( 830 mg / m orally twice daily for 21 days ) repeated every 28 days for six cycles , or until disease progression , development of cumulative toxic e ects or patient discontinuation ( appendix ) .22 patients randomly assigned to sequential chemoimmunotherapy received two cycles of combination chemotherapy as above , and were subsequently immunised with an intradermal injection of recombinant gm - csf ( 75 g ) into the lower abdomen , and 1015 min later , with an intradermal injection at the same site of 056 mg of gv1001 ( 200 ml of 28 mg / ml ) .10 immunisation was undertaken on days 1 , 3 , and 5 during week 1 , then once on weeks 2 , 3 , 4 , and 6 and then monthly . 
if disease progression occurred , as measured by ct scan , gv1001 was stopped and gemcitabine and capecitabine was restarted . patients randomly assigned to concurrent chemoimmunotherapy received combination chemo therapy as in the chemotherapy alone group for six cycles with gm - csf and gv1001 from day 1 of therapy as in the sequential chemoimmunotherapy group and then received just immunotherapy at the end of cycle six . 
capecitabine interrupted following the rst doses were to be appearance of any grade 2 non - haematological adverse events ( the most frequent side - e ects were gastrointestinal disorders , especially diarrhoea , nausea , vomiting and stomatitis , and hand - foot syndrome ) until resolved to grade 01 , and to maintain normal dose level subsequent for the next cycle . 
if any grade 2 non - haematological adverse events appeared for a second time , capecitabine was to be interrupted and reduced to 75% with prophylaxis in the next cycle ; and if any events appeared for a third time , capecitabine was to be interrupted and reduced to 50% in the next cycle . 
the occurrence of any grade 3 adverse events followed the same discontinuation rules for capecitabine for their rst and second appearances , but capecitabine was discontinued permanently after the third appearance of a grade 3 nonhaematological adverse event . 
if patients had an episode of any - grade febrile neutropenia , or had a neutrophil count lower than 05 10 cells per l , or a platelet count lower than 50 10 cells per l , then capecitabine was withheld and omitted until resolved to grade 01 toxic e ects , at which point patients could restart capecitabine at a 75% dose . patients could withdraw by deciding to discontinue the trial , because of disease progression according to recist , or due to intolerable adverse e ects . 
patients had to withdraw because of pregnancy ; recurrent grade 3 or 4 drug - related toxic e ects despite dose modi cation , serious systemic allergic reaction to any of the study drugs eg , angio - oedema or anaphylaxis , intercurrent , unrelated conditions requiring long - term use of steroids ; missing two consecutive gv1001 administrations , or three gv1001 the entire non - consecutive administrations during treatment course ; or missing two consecutive cycles of gemcitabine and capecitabine administrations or three non - consecutive cycles during the entire treatment course . 
 we used the national cancer institute common toxicity criteria for adverse events version 3 to record toxic e ects . we tested for delayed - type hypersensitivity in the chemoimmunotherapy groups by giving a second intradermal injection of 0105 mg of gv1001 simultaneously at the contralateral site on the lower abdomen without concomitant gm - csf . 
we continued testing for delayed - type hypersensitivity until the result was positive , or the vaccine therapy discontinued . we assessed t - cell proliferation in a subset of patients ( from volunteer sites that had the facilities to collect and immediately process samples )  . 
we seeded thawed peripheral blood mononuclear cells ( pbmcs ) in 48 - well plates ( thermofisher scienti c , usa ) at 2 10 cells per well in x - vivo 15 ( lonza , uk ) with 10% pooled human serum ( innovative research , usa ) and 20 g / ml of gv1001 peptide . 
on day 11 , we harvested the gv1001 - enriched cells and placed them in a round bottom 96 - well plate ( 50 l , 1 10 cells per well )  . 
to the pre - stimulated cells , we added irradiated ( 45 gy ) autologous pbmcs ( 50 l , 1 10 cells per well ) to act as antigen - presenting cells . 
we tested for gv1001 - speci c 832 vol 15 july 2014 articles number of patients number of deaths median survival in months ( 95% ci ) 12 - month survival ( 95% ci ) hazard ratio * ( 9825% ci ) log - rank rank test , p value * chemotherapy alone group 245 ( 68% ) 79 ( 7188 ) 337% ( 282392 ) sequential chemoimmunotherapy group 268 ( 77% ) 69 ( 6476 ) 253% ( 202305 ) concurrent chemoimmunotherapy 259 ( 73% ) 84 ( 7397 ) 323% ( 268378 ) 12 ( 1.015 ) 105 ( 0813 ) 00466 06378 ecog = eastern cooperative oncology group . 
 table 2 : overall survival proliferation by adding 100 l of either : control media , 20 g / ml of gv1001 , or 5 g / ml of phytohaemagglutinin ( pha ) as a control . 
we de ned a positive total immune response as a positive test for delayed - type hypersensitivity or a positive proliferation assay , or both . outcomes the primary endpoint was overall survival . 
the secondary endpoints were safety , time to progression , objective tumour response , quality of life , changes in ca19 - 9 concentration over time , and immunogenicity ( measured as delayed type hyper sensitivity and t - cell proliferation )  . statistical analysis to detect a 10% improvement in 1 - year survival for either experimental group ( above the 25% survival expected in the chemotherapy group ) , an enrolment of 1110 patients , with 780 deaths expected , was required . 
a two - sided of 0025 ( corresponding to a 975% ci ) was set for each primary response comparison of chemoimmunotherapy versus standard chemotherapy , with a total 005 level of signi cance and at least 80% power for the trial as a whole . 
the sample size additionally adjusted for four formal interim and one nal analysis on the primary endpoint ( obrienfleming type boundaries based on the lan - demets - spending function )  . 
in practice , as the trial terminated early , we applied 9825% cis ( signi cance of 00175 ) to all analyses of the primary including comparison between treatment endpoint groups . the nal analysis was done on the intention - to - treat population , consisting of all patients randomly assigned to treatment , except for patients who withdrew consent between randomisation and the start of therapy , and patients who were withdrawn from the study after randomisation because of irregularities with the consent process . 
 * ca19 - 9 not available for 47 patients . table 3 : survival factors by univariate analysis the chief primary endpoint , investigator reviewed deviations to identify protocol deviations that would a ect the outcome . 
sensitivity vol 15 july 2014 articles local , ecog 0 local , ecog 1 local , ecog 2 metatastic , ecog 0 metatastic , ecog 1 metatastic , ecog 2 overall ( i2 = 00% , p = 0895 ) local , ecog 0 local , ecog 1 local , ecog 2 metatastic , ecog 0 metatastic , ecog 1 metatastic , ecog 2 overall ( i2 = 00% , p = 0920 ) analyses included testing the proportional hazards assumption , additional strati cation for ca19 - 9 concentration , allowance for random centre e ect , and testing for interaction between treatment and centre . 
 overall survival and time to progression were estimated by the kaplan - meier method , with hazard ratios ( hrs ) and con dence intervals obtained from a strati ed cox model and p values the corresponding strati ed log - rank test ( strata as de ned for the randomisation )  . 
for other pre - speci ed outcomes ( including time to progression ) , for descriptive analyses including only one group , and for unplanned from chemotherapy alone sequential chemoimunotherapy concurrent chemoimmunotherapy number at risk chemotherapy alone sequential chemoimmunotherapy concurrent chemoimmunotherapy time from randomisation ( months ) 0196 100 511 favours sequential chemoimmunotherapy favours standard chemotherapy weight ( % ) hr ( 95% ci ) p value 881% 1708% 225% 1872% 4349% 964% 10000% 120 ( 059246 ) 052 094 ( 061158 ) 080 124 ( 038513 ) 100 118 ( 078192 ) 039 131 ( 100181 ) 006 124 ( 070246 ) 038 weight ( % ) hr ( 95% ci ) p value 855% 1804% 270% 1798% 4337% 936% 10000% 085 ( 041176 ) 062 107 ( 065177 ) 078 084 ( 023307 ) 082 105 ( 064174 ) 084 103 ( 075143 ) 083 137 ( 068275 ) 032 analyses , we used a conventional 95% two - sided ci with no correction . 
this trial is registered as an international standard randomised controlled trial , number isrctn4382138 . role of the funding source neither the sponsors nor funders had any role in the design and conduct of the study ; the collection , management , analysis , and interpretation of the data ; the the preparation , review , or approval of nor presentation . 
the academic chief investigator gm and the principal grant holder jn had full access to all the data in the study , and take full responsibility for the integrity of the data and the accuracy of the data analysis.the corresponding author had nal responsibility to submit for publication . results the rst patient was randomly assigned to treatment on march 29 , 2007 , and the trial was terminated slightly ahead of target , on march 27 , 2011 , because of unfavourable survival in the sequential chemo immunotherapy group . 
 to receive 358 patients were randomly assigned gemcitabine and capecitabine alone ( chemotherapy group ) , 350 to gemcitabine and capecitabine and then sequential gv1001 ( sequential chemoimmunotherapy group ) , and 354 to gemcitabine and capecitabine and concurrent gv1001 ( concurrent chemoimmunotherapy group ; gure 1 )  . 
baseline characteristics were well balanced across all three groups ( table 1 )  . 772 patients died during the study ; the 290 patients still alive were followed up for a median of 60 months ( iqr 24122 )  . 
median overall survival was 76 months ( 95% ci 7181 ) with 12 - month survival of 304% ( 95% ci 273336 ) , and 24 - month survival of 94% ( 72120 ) ( table 2 )  . 
baseline clinical stage , blood ca19 - 9 levels , and ecog performance status were all associated with survival ( p < 00001 for each factor on univariate analysis ; table 3 )  . 
 patients on sequential chemoimmunotherapy with a positive delayed - type hypersensitivity response had a median survival of 75 months ( 95% ci 3595 ) those with a negative response a median and overall survival of 58 months ( 3971 , hr 095 ; 95% ci 049184 ; 1df = 0036 , p = 085 ; gure 4 )  . 
 median survival in patients on concurrent chemoimmuno therapy with a positive delayed - type hypersensitivity response was 90 months ( 95% ci 61109 ) and 80 months ( 6687 ) for those with a negative response ( hr 098 , 060159 ; 1df = 0015 , p = 090 ; gure 4 )  . there was no signi cant di erence in t - cell proliferation between chemoimmunotherapy groups ; t - cell proliferation was positive in ten ( 31% ) of 32 patients given sequential chemoimmunotherapy and ten ( 15% ) of 68 patients given concurrent chemoimmunotherapy ( p = 0065 )  . 
12 ( 38% ) of 32 patients on sequential immunotherapy ( 40% of the 30 patients without any missing values ) had a total immune response , as did 25 ( 37% ) of 68 patients on concurrent chemo immuno therapy ( 40% of the 63 without missing values )  . 
median survival ( from week 18 ) in patients on sequential immunotherapy group with a positive total immune response was 84 months ( 95% ci , 70na ) and 73 months ( 95% ci 30292 ) with a negative response ( hr 028 , 95% ci , 005153 ; 1df = 2368 , p = 012 )  . 
median survival ( from week 10 ) in patients randomly assigned to concurrent chemoimmunotherapy was 106 months ( 95% ci 62137 ) and 122 months ( 72166 ) respectively ( hr 157 , 95% ci 071349 ; 1df = 1241 , p = 027 ; appendix )  . 
 the per - protocol analysis was undertaken after removing 62 patients who deviated from the protocol ( 21 patients in the chemotherapy group alone , 21 in the sequential chemo immunotherapy group , and 20 in the concurrent chemo immunotherapy )  . 
the lack of treatment e ect on survival was consistent between tumour stages ( global likelihoodratio test for treatment stage interaction , 2df = 273 , p = 026 )  . 
patients assigned to either sequential or concurrent chemo immunotherapy with a lower tumour burden ( locally advanced disease ) or a good performance status ( ecog 0 ) had no survival bene t when compared with those assigned to chemotherapy alone ( gure 2b , c )  . 
 an unplanned post - hoc analysis showed that the overall survival of the 84 patients who were randomly assigned to sequential chemo immunotherapy , and subsequently returned to standard chemotherapy following progression on vaccination therapy , and were alive at 18 weeks , did not di er from that of patients alive at 18 weeks randomly assigned to standard chemotherapy ( hr 084 ; 95% ci 058123 ; p = 028 ; appendix )  . we assessed the possibility that treatment e ects might di er according to tumour stage , ecog performance status , and ca19 - 9 concentration by a likelihood ratio test nesting a main - e ects - only model within one including interactions between treatment group and each of the other factors , but this analysis showed no di erence ( 12df = 1376 , p = 032 )  . median time to progression was not signi cantly di erent in the chemotherapy group compared to the sequential chemoimmunotherapy group ( 64 months [ 95% ci 4871 ] vs 45 months [ 4346 ] ; hr 150 , 95% ci 126178 , p < 00001 ) , nor the concurrent chemoimmunotherapy group ( 66 [ 5073 ] , hr 10 , 95% ci 084119 ; p = 099 ; overall log - rank 2df = 295 ; p < 00001 ; gure 3 )  . ( 7% ) of 350 patients a partial or complete tumour response was noted at 8 weeks in 36 ( 10% ) of 358 patients in the chemotherapy the alone group , 25 sequential chemo immunotherapy group , and 29 ( 8% ) of 354 patients in the concurrent chemoimmunotherapy group ; there was no signi cant di erence between the three groups . 
an overall response ( complete plus partial response at any time ) was noted in 63 ( 18% ) of 358 patients in the chemotherapy alone group , 31 ( 9% ) of 350 patients in the sequential chemoimmunotherapy group , and 55 ( 16% ) of 354 patients in the concurrent chemoimmunotherapy the sequential chemoimmunotherapy group achieved signi cantly fewer overall responses than those in the chemotherapy alone group ( p = 0001 )  . group ; patients the proportion of delayed - type hypersensitivitypositive patients did not di er between immunochemotherapy groups ; 19 ( 12% ) of 154 patients assigned vol 15 july 2014 articles number at risk dth negative dth positive number at risk dth negative dth positive dth negative dth positive time from randomisation ( months ) positive total immune response was 115 ( 95% ci 056238 ; 1df = 3208 , p = 0073 )  . from e ects sequential the standard chemotherapy regimen was well tolerated and there was no evidence of any additional toxic concurrent chemoimmunotherapy ( table 4 )  . 
there were 32 ( 3% ) patients altogether who withdrew because of toxic e ects , 15 ( 4% ) patients from the standard chemotherapy group , four ( 1% ) from the sequential chemo immunotherapy group , and 13 ( 4% ) from the concurrent chemoimmunotherapy group ( 2df = 64 ; p = 004 )  . 
there were four ( 1% ) deaths due to drugrelated toxic e ects in the standard chemotherapy group , ve ( 1% ) in the sequential chemoimmunotherapy group , and six ( 2% ) in the concurrent chemo immunotherapy group ( p = 081 )  . patients randomly assigned to sequential immunotherapy had a signi cantly higher pain score than did patients randomly assigned to standard chemotherapy at 20 weeks ( table 5 )  . discussion our ndings showed that the addition of the gv1001 vaccine to gemcitabine and capecitabine did not improve survival in patients with advanced pancreatic cancer . 
the total immune response in the phase 2 study compared with that seen in the current study is consistent with the reduction in response rates generally noted in the transition from phase 2 to phase 3 studies ( 12 of 17 [ 71% ] patients in the phase 2 study vs 12 of 32 and 25 of 68 [ 37% overall ] in the phase 3 study ; panel ) .10 for a cancer vaccine to be e ective , an active immune response is needed , which is dependent on a su cient period of time for this response to develop . 
the characteristic early metastasising and rapidly progressive nature of pancreatic cancer might partly explain the absence of clinical e cacy , but other complex immunological and stromal factors also need to be overcome.25 , 28 , 30 a dense stromal reaction has been shown to impede the penetration of cytotoxics into pancreatic tumours , thus restricting the synergistic potential of chemotherapy and gv1001 vaccination intended to achieve cd40 activation and generate telomerase - speci c t - helper cells.25 direct cd40 activation ( using the agonist cp - 870 , 893 ) with gemcitabine chemotherapy has recently been shown to cause a partial tumour response in four of 21 patients with advanced pancreatic cancer , but this e ect was surprisingly due to stroma - in ltrating macrophages rather than t cells.28 an e ective active immune response might also depend on a lower tumour burden and good performance status , but recent studies from other tumour types do not seem to support this . 
in a randomised phase 2 trial of prostate cancer including prostvac - vf ( consisting of two prostate speci c antigen [ psa ] encoding viral vectors , and the b71 , icam - 1 , and lfa - 3 co - stimulatory molecules ) and gm - csf , no survival improvement was noted in men with fewer bony metastases or an ecog performance status of zero.31 similar ndings were noted in the impact phase 3 trial in men treated with sipuleucel - t , which is a form of active cellular immunotherapy ( autologous pbmcs activated with the recombinant pa2024 protein composed of a prostate antigen and prostatic acid phosphatase , fused to gm - csf ) .32 in the telovac trial , we noted no e ect of gv1001 vaccination on survival by either stage of disease or performance status . identi cation of robust immunotherapy response signatures in human cancer studies remains challenging across tumour types . 
in the prostvac - vf trial , 31 no antibody response to psa was noted , and although all patients generated titres to one or both viral vectors , no association with survival was noted . 
in the impact trial , 32 although there was a t - cell proliferation response to pa2024 in 46 ( 73% ) of 63 patients given sipuleucel - t , only 15 ( 27% ) of 55 patients had a t - cell response against the target antigen prostatic acid phosphatase . 
the scarce immunotherapeutic figure 4 : overall survival according to a positive or negative delayed - type hypersensitivity response in patients assigned to chemoimmunotherapy ( a ) patients randomly assigned to sequential chemoimmunotherapy , conditional on reaching week 18 . 
in a trial30 of an anti - pd - l1 antibody ( bms - 936559 ) 207 patients , objective responses were reported in malignant melanoma , renal - cell cancer , non - small - cell lung cancer , and ovarian cancer but none in 14 patients with advanced pancreatic cancer . 
the relative absence of immuno therapy e cacy in pancreatic cancer might also to speci c carcinoma - associated partly be related broblasts ( expressing broblast activation protein ) , which secrete cxcl12 and thus stop t cells from accessing cancer cell regions in the stroma . 
in a genetically engineered mouse model of pancreatic cancer blocking the receptor of cxcl12 , induced rapid t - cell accumulation and synergised with - pd - l1 in cancer cell killing.29 there have been concerns raised about the use of gmcsf as adjuvant based on the induction of myeloid derived suppressor cells ( mdscs ) by low - dose gmcsf , 35 but we have shown that the concentrations of mdscs were reduced in patients treated with gv1001 , gm - csf , and concomitant chemotherapy compared with chemotherapy alone.36 there was a shorter time to progression observed after the administration of two cycles of chemotherapy in the sequential chemoimmunotherapy group than the other two groups . 
a post - hoc analysis showed that the overall survival in this group of patients who returned to standard chemotherapy following progression on vaccination therapy was not di erent from similar patients randomly assigned to standard chemotherapy . 
 these ndings suggest that treatment until progression is the appropriate approach in pancreatic cancer and is consistent with recent ndings that a minimum of six cycles of chemotherapy is necessary for optimum survival bene t in the adjuvant setting.37 the telovac study has shown the challenges for immunotherapy study design when immunotherapy is combined with standard therapy in the rst - line setting and highlights the uncertainties in extrapolating treatment scheduling from experimental models to the clinical setting . 
one option that had been considered was vaccination after 838 vol 15 july 2014 articles panel : research in context systematic review in trial set up for the treatment of locally advanced and metastatic pancreatic cancer , two systematic reviews were undertaken.24 , 25 medline , oldmedline , cancerlit , embase , and isi web of science , isi science and technology proceedings , current contents databases , trial registries , and conference proceedings were searched , and results identi ed included randomised controlled trials involving patients with advanced pancreatic cancer of chemotherapy , novel agents , radiotherapy , chemoradiotherapy , and best supportive care . 
 we searched pubmed for any clinical trial and experimental work for telomerase , immunotherapy , vaccines , cancer , pancreatic cancer , and gv1001 , with no restrictions.26 the reviews showed that chemoradiation followed by chemotherapy did not show any survival advantage over chemotherapy alone . 
the combination of gemcitabine with capecitabine was chosen as this could potentiate the vaccine e ects , and was also associated with signi cantly improved objective responses compared with gemcitabine alone.22 , 24 , 25 interpretation we noted no survival bene t from the addition of the gv1001 vaccine to gemcitabine and capecitabine in patients with advanced pancreatic cancer . 
during the course of the trial there has been a major development in clinically relevant genetically engineered models that has signi cantly contributed to the deeper understanding of the biological mechanisms that undermine the e ective treatment of pancreatic cancer.2729 these can now be countered and could be deployed in multimodality strategies to overcome the key biological constraints to e ective treatment . 
 six cycles of chemotherapy rather than two cycles but it was important to test the institution of vaccination after initial stabilisation of disease before progression , and at a time when apoptosis was likely to be still high . 
in this study , the median time to progression on chemotherapy alone was 64 months ( 95% ci 95% ci 4871 ) ; therefore 50% of patients would have progressed at this point . 
for future immunotherapy trials , randomised phase 2 studies using adaptive trial designs should be seriously considered to explore di erent scheduling regimens that do not compromise standard treatment . the telovac trial has shown that vaccination to htert can elicit immune responses during chemotherapy but without clinical e cacy . 
there are presently a number of di erent approaches being used to target telomerase in cancer including small - molecule telomerase inhibitors that might be more e ective in tumours with shorter telomeres.38 , 39 opportunities to uncloak the mechanism of action of vaccines such as gv1001 using multimodality strategies that are directed against the stroma and check point inhibition as well as direct cd40 activation should be explored . contributors development of the study design was supported and conducted through national cancer research institute ( ncri ) of the uk pancreatic cancer sub - group and the cruk liverpool cancer trials unit ( of the liverpool clinical trials unit ) and was led by the telovac working party composed of gm , jn , dc , tc , ps , jv , jw , dp , fc , pr , sm , tr , and pc . 
the results were interpreted by the telovac working party , which prepared the initial draft and were responsible for collating changes proposed by all of the authors into the nal draft paper before nal approval by all participants telovac study group . 
the specialists who also contributed to the recruitment , treatment , and follow - up of patients as trial site principle investigators , along with sites and number of patients recruited are shown in the appendix . declaration of interests jw reports personal fees from astra zeneca , celgene , and novartis outside the submitted work . 
pr reports personal fees from roche ; grants and personal fees from merck serono , sano aventis ; personal fees from cellgene , bayer , novartis , bristol - myers squibb , and sirtex , outside the submitted work . 
jn reports grants from cancer research uk ; grants and personal fees from kael gemvax , during the conduct of the study ; and personal fees from oxford biomedica ( uk ) ltd , pzifer novartis , astellas , and novartis pharma ag , outside the submitted work . 
ec , tc , wg , dn , gn , cr , ps , and vs report grants from cancer research uk ; and grants and personal fees from kael gemvax , during the conduct of the study . 
we thank the independent data and safety monitoring committee which consisted of chris russell ( university college london , london , uk ) , roger ahern ( institute of cancer research , sutton , uk ) , and david chao ( the royal free hospital , london , uk )  . 
we report the study design , participant sociodemographic and clinical characteristics , and the initial results of the testing and diagnostic phase of the prostate testing for cancer and treatment ( protect ) trial , which aims to investigate the e ectiveness of treatments for localised prostate cancer . methods in this randomised phase 3 trial , men aged 5069 years registered at 337 primary care centres in nine uk cities were invited to attend a specialist nurse appointment for a serum prostate - speci c antigen ( psa ) test . 
consenting participants with clinically localised prostate cancer were randomly assigned to active monitoring ( surveillance strategy ) , radical prostatectomy , or three - dimensional conformal external - beam radiotherapy by a computer - generated allocation syste randomisation was strati ed by site ( minimised for di erences in participant age , psa results , and gleason score )  . 
 the primary endpoint is prostate cancer mortality at a median 10 - year follow - up , ascertained by an independent committee , which will be analysed by intention to treat in 2016 . 
this trial is registered with clinicaltrials.gov , number nct02044172 , and as an international standard randomised controlled trial , number isrctn20141297 . findings between oct 1 , 2001 , and jan 20 , 2009 , 228 966 men were invited to attend an appointment with a specialist nurse . 
2896 men were diagnosed with prostate cancer ( 4% of tested men and 39% of those who had a biopsy ) , of whom 2417 ( 83% ) had clinically localised disease ( mostly t1c , gleason score 6 )  . 
with the addition of 247 pilot study participants recruited between 1999 and 2001 , 2664 men were eligible for the treatment trial and 1643 ( 62% ) agreed to be randomly assigned ( 545 to active monitoring , 545 to radiotherapy , and 553 to radical prostatectomy )  . 
clinical and sociodemographic characteristics of randomly assigned participants were balanced across treatment groups . interpretation the protect trial randomly assigned 1643 men with localised prostate cancer to active monitoring , radiotherapy , or surgery . 
open access article distributed under the terms of cc by . introduction prostate cancer is the most frequently diagnosed cancer in men in developed countries , with an estimated 241 740 new cases and 28 171 deaths caused by the disease every year in the usa alone.1 in the uk , it is the second most common cause of cancer deaths in men ( 13% ) with 41 763 new cases diagnosed and 10 793 deaths caused by the disease in 2011.2 the disease can be detected early by prostate - speci c antigen ( psa ) measurement followed by prostate biopsy . 
however , most screen - detected cancers are at low risk of progression , and potential harm could be caused by unnecessary diagnosis and treatment . the publication of two population - based randomised controlled trials3 , 4 of screening has not resolved this dilemma . 
the european randomized study of screening for prostate cancer ( erspc ) 3 reported a clear but relatively small disease - speci c survival bene t from screening compared with no active intervention at 8 years and 13 years follow - up , with a larger e ect reported in a smaller scandinavian cohort at 14 years after diagnosis.4 by contrast , the us - based prostate , lung , colorectal , and ovarian ( plco ) trial5 reported no bene t from screening with a similar length of follow - up , but was limited by substantial contamination from previous psa testing in the control group in more than 50% of the unscreened men . most men diagnosed with psa - detected prostate cancer tend to undergo radical treatment . 
the us - based prostate cancer intervention versus observation trial ( pivot ) 6 reported no overall mortality bene t from surgery in patients with psa - detected cancer , whereas the scandinavian prostate cancer group 4 trial ( spcg - 4 ) 7 showed a clear diseasespeci c and overall survival bene t for surgery in patients presenting clinically , as well as a reduction in progression to metastatic disease . androgen the prostate testing for cancer and treatment ( protect ) randomised trial was designed to assess the e ectiveness and cost - e ectiveness of active monitoring ( a surveillance protocol ) , external beam conformal radiotherapy with neoadjuvant radical prostatectomy for men with psa - detected clinically localised prostate cancer . 
the recruitment was undertaken in two stages : a feasibility pilot in three english cities ( in 24 primary care centres linked to three university hospitals ) from june , 1999 , to september , 2001 ( isrctn08435261 ) , and the main trial from october , 2001 , to january , 2009 , in nine cities ( seven in england , one in scotland , and one in wales ) .8 also in 2001 , the cap trial ( cluster randomised trial of psa testing for prostate cancer ; isrctn92187251 ) commenced , which is an extension to the protect trial . 
 the cap trial randomly assigned primary care centres to undertake either the protect trial or standard uk national health service ( nhs ) management ( no routine psa testing ; gure 1 ) , to assess population - based screening in addition to treatment e ectiveness of clinically localised disease identi ed in protect.9 further details of the cap trial design and randomisation have been published previously.10 a written invitation was sent by 337 primary care centres assigned to undertake the protect trial to registered men aged 5069 years , excluding those with a previous malignancy ( apart from skin cancer ) , renal transplant or on renal dialysis , major cardiovascular or respiratory comorbidities , bilateral hip replacement , or an estimated life expectancy of less 10 years . 
men who responded received a protect patient information sheet and an appointment with a specialist nurse who explained the complexities of psa testing , assessed trial eligibility , and sought written informed consent . 
participants with a psa concentration of at least 30 g / l were invited to attend secondary care centres within the nine participating cities for a physical and digital rectal examination and standardised transrectalultrasound - guided prostate biopsies . 
participants with an initial psa concentration at least 200 g / l at diagnosis were excluded because of the high likelihood that they had more advanced cancer . ten - core individual received a protect patients were staged using a combination of digital rectal examination , psa concentration , transrectal ultrasound - guided biopsies , and isotope bone scanning ( if psa was 10 g / l )  . 
men with a psa concentration of 10 g / l or higher or a gleason score of greater than 7 points underwent an isotope bone scan to exclude metastatic disease . 
men with a benign rst biopsy sample and a free - to - total psa ratio below 11% , or atypical small acinar proliferation or 1110 vol 15 september 2014 articles for the study protocol see projects / hta / 962099 high - grade prostatic intraepithelial neoplasia , were o ered further biopsies ; if these repeat biopsy samples were benign , these men were managed in primary care and excluded from the trial . 
no further trial follow - up occurred after the one round of psa testing or identi cation of cancers after referral to the nhs . approval was obtained from the uk trent multicentre research ethics committee ( 01 / 4 / 025 )  . 
study training programmes and on - site monitoring visits were used to standardise trial conduct.11 , 12 randomisation and masking men discussed treatment options with the specialist nurses , and if they agreed to the three - group randomisation ( 1 : 1 : 1 ) , the nurse telephoned a central system in the bristol trials o ce ( bristol , uk ) and logged participant details . 
 allocations were computer - generated as required for each participant , originally using microsoft excel functions , and subsequently in c + + , strati ed by site with stochastic minimisation to improve the balance across the groups in relation to age at primary care patient identi cation date , gleason sum score ( < 7 , 7 , or 810 points ) and mean of baseline and rst biopsy psa results ( < 60 , 6099 , or > 99 g / l )  . 
eligible participants were o ered the choice of a two - group randomisation ( radical prostatectomy or radiotherapy ) , or a three - group randomisation ( with the addition of active monitoring to the two treatment groups )  . 
in 2003 , the independent data monitoring committee ( dmc ) terminated the two - group option because of limited uptake , and the only option for participants who consented was three - group randomisation throughout the remaining period of recruitment . 
men who declined randomisation were o ered identical follow - up and formed a comprehensive cohort within the study design . the procedures participant sociodemographic characteristics , family history of cancer , and previous psa tests were obtained at recruitment . 
 imaging of the skeleton was recommended if serum psa reached 10 g / l , using isotope bone scintigraphy , plain radiographs , and mri as necessary . in patients randomly assigned to active monitoring , the protocol aim was to avoid immediate radical treatment while assessing the disease over time , with radical treatment o ered if disease progression was evident . 
the specialist nurses also met with participants yearly to assess their overall health , and discuss graphical displays of psa results and any concerns raised , overseen by each centres local clinical investigator . 
if the psa concentrations were persistently raised , or the patient had any other concerns , a review appointment was made with the centre urologist for discussion of further tests including re - biopsy and all relevant management options . in patients randomly assigned to receive external beam 3d conformal radiotherapy , neoadjuvant androgen suppression was given for 36 months before and concomitantly with 3d - conformal radiotherapy delivered at 74 gy in 37 fractions.13 quality assurance followed the rt01 trial procedures.14 , 15 psa concentrations were measured every 6 months for the rst year and then yearly . 
the study oncologist held a review appointment with participants if the psa concentrations rose by at least 20 g / l post - nadir or concerns were raised about disease progression.16 management options were discussed , including continued monitoring , further tests , salvage , radical , or palliative treatments as indicated . in patients randomly assigned to receive radical prostatectomy , the predominant approach was open retropubic radical prostatectomy with individual - level quality assurance according to minimum standards.17 participants with a baseline psa concen tration of at least 10 g / l or a biopsy gleason score of at least 7 points received bilateral lymph adenectomy . 
the centre urologist held a review appointment their postoperative psa conwith participants centrations reached 02 g / l or higher to discuss adjuvant radiotherapy . linked translational study obtained biological specimens and epidemiological data.9 outcomes outcome measures were selected for relevance to patients and health - care providers . 
the primary outcome was de ned as de nite or probable prostate cancer mortality , including intervention - related deaths , at a median of 10 years follow - up . 
the process used to assess cause of death was adapted from the plco algorithm5 and erspc process3 and then combined to vol 15 september 2014 1111 articles assess deaths in both the cap and protect studies . 
a full list of all prespeci ed outcomes can be found in our study protocol . for statistical analysis before the start of the trial , a sample - size target of 1434 randomly assigned men ( 478 in each group ) was identi ed as su cient to estimate the absolute di erence in mortality probability between two treatment groups with a 95% ci of 0045 , on the basis of an assumed mortality rate of 15% , consistent with prostate cancerspeci c mortality in men aged 5569 years with clinically detected disease managed conservatively at that time and a di erence that would be deemed clinically signi cant by the nhs . 
 however , more recent data10 suggested that diseasespeci c mortality with non - radical treatment was likely to be closer to 10% at 10 years , because of improvements in disease management . 
as a result , the dmc advised in 2008 that recruitment should continue to the planned end date , with 1590 men ( 530 per group ) expected to be randomly allocated by that point . 
this sample size would enable a 46% reduction in prostate cancer mortality to be detected with 80% power at a 5% signi cance level for a pairwise comparison of a radical treatment with active monitoring . 
this calculation assumes a 10% prostate cancer - speci c mortality at 10 years with active monitoring , and hence a 54% risk with radical treatmentan absolute di erence very similar to the margin of error speci ed in the rst calculation . 
these sample size targets are based on di erences in and ratios of risk rather than the hazard ratios planned for the primary analysis , because the resulting calculations are simpler and more exible . 
when a median of 10 years of follow - up has accumulated ( november , 2015 ) , the primary outcome measure of prostate cancer mortality will be compared between ( cox treatment groups using a survival analysis proportional hazards regression model ) adjusted for strati cation and minimisation variables . 
hazard ratios are interpreted in the same way as rate ratios ; the advantage of hazard ratios and coxs proportional hazards model for this study is the accommodation of variation in the underlying rate of prostate cancer mortality during follow - up . 
 pairwise signi cance tests will only be done if a test of an equal 10 - year disease - speci c mortality risk across all three groups yields a p value of less than 005.26 this approach will be used for event - based secondary outcomesie , grouped analyses of de nite , probable , or possible prostate cancer , all - cause mortality , and metastatic disease . pairwise comparisons of symptom burden will use multilevel models for repeated measures to estimate the average treatment e ect over the median 10 - year followup . 
prespeci ed subgroup analyses will investigate whether treatment e ectiveness in the reduction of prostate cancer - speci c mortality is modi ed by baseline clinical stage , gleason grade , age , or psa concentration using strati ed analyses for descriptive statistics and by formally including interaction terms in the relevant regression models . 
secondary analyses will estimate the e cacy of radical treatment versus active monitoring in the reduction of prostate cancer mortality in individuals who complied with their allocated treatment , by using a method to derive an unbiased estimate in parallel with the per - protocol analysis originally speci ed in the trial protocol.27 , 28 an analysis of primary and secondary outcome measures by trial group is reported yearly to the dmc . 
the dmc recommends changes to the trial steering committee if clear evidence ( of the order of p < 0001 ) of a positive or negative balance of risks and bene ts emerges for one intervention in comparison with the others . data from the recruitment , diagnostic , and randomisation phases are presented , and categorisation of continuous variables is either based on clinical thresholds ( eg , for psa ) or the aim of equal group sizes ( other measures )  . 
129 men were 49 years of age when the primary care list was generated , 120 of whom were 50 years old by recruitment ; 25 men were 70 years or older at generation of the primary care list , of whom four were 71 years of age and one was 72 years of age ; at the time of recruitment , all men who were enrolled tted the stated inclusion criteria as per protocol . 
based on resident area - based material and social deprivation scoreseg , percentage of social housing . table 1 : demographic and clinical characteristics according to diagnosis of prostate cancer in patients recruited into the main protect trial 228 966 men aged 5069 years were invited to participate 106 464 did not respond 122 502 responded 100 444 attended appointment 82 429 were recruited 8566 had an eligible psa result 7414 received prostate biopsies 5468 single biopsy 1946 more than one biopsies 18 015 not recruited 7665 ineligible 10 350 declined to participate 73 863 ineligible psa results 73 538 < 30 g / l 279 200 g / l 46 results not given 1152 did not receive biopsy 3504 biopsy negative or mild 4518 biopsy negative or other 756 high grade pin 255 asap atypia 3 inadequate specimen 479 ineligible 270 advanced disease 209 localised but excluded 2896 had a positive biopsy result for prostate cancer 2417 eligible for randomisation ( localised prostate cancer ) figure 2 : flow diagram of the diagnostic phase of the main protect trial results are from one round of psa testing . 
jal , fch , jld , and den had full access to all the data for this analysis ( full outcome data will become accessible to them from nov 15 , 2015 ) and had nal responsibility for the decision to submit for publication . results between oct 1 , 2001 , and jan 20 , 2009 , 228 966 men were invited to participate in the protect study , of whom 122 502 ( 54% ) responded , although 5954 ( 5% ) of respondents declined to participate and 16 104 ( 13% ) did not attend the appointment with the specialist nurse ( gure 2 )  . 
of the men who attended their appointment , 10 350 ( 10% ) did not enrol or return their second consent form and 7665 ( 8% ) were deemed ineligible . 73 538 ( 89% ) of the 82429 recruited participants had a psa concentration that was below the biopsy cuto point . 
date of birth could not be obtained or age was out of eligible range for 130 recruited participants ; age was out of eligible range for two participants invited for biopsy ; two participants who received biopsy ; and one participant who was diagnosed with prostate cancer . 
 table 2 : psa distribution , biopsy , and prostate cancer diagnosis by age and psa concentration in the main protect trial 2664 participants were eligible 2417 recruited in main trial 247 recruited in pilot study 1643 participants were randomly assigned 1497 from main trial 146 from pilot study 1021 were not randomly assigned 997 selected treatment 24 were randomly assigned to two groups 545 allocated to active monitoring 545 allocated to radiotherapy 553 allocated to surgery figure 3 : flow diagram of the randomisation phase of th e protect trial biopsies were o ered to the 2357 ( 32% ) men without a de nitive diagnosis ; 1563 those o ered underwent the repeat procedure , with a further 322 ( 14% ) receiving a repeat biopsy after advice from a urologist . ( 66% ) of 2896 men were diagnosed with prostate cancer ( 4% of those recruited ; 39% of those who had a biopsy )  . 
additionally , of men with a positive biopsy result , 270 ( 9% ) were ineligible for locally advanced , randomisation because they had advanced , or metastatic disease , and 209 ( 7% ) were excluded because of comorbidity . predominantly , recruited protect participants were white and married or living with a partner , and 4082 ( 5% ) reported a family history of prostate cancer ( table 1 )  . 
 median age was 58 years ( range 5069 ) in the total cohort , with slightly more men younger than 60 years recruited than older men ( table 2 ) , and 11 011 ( 13% ) men had received a previous psa test . 
the relation between higher psa concentrations and prostate cancer diagnosis was unchanged by adjustment for age , whereas the relation between the proportion of recruited patients diagnosed with prostate cancer and increased age was attenuated by adjustment for psa concentration ( unadjusted odds ratio [ or ] data not shown ; table 2 )  . 
ethnic origin , married or partnership status , and extent of material deprivation did not di er between participants diagnosed with cancer and those without cancer ( table 1 )  . ( 62% ) of these eligible patients agreed 2417 men recruited to the main protect trial were eligible , as were 247 from the feasibility pilot phase.8 1643 randomisation ( gure 3 )  . 
the median follow - up is currently 86 years ( iqr 71104 ) and we have obtained vital status ( primary outcome ) info for 99% of patients , and secondary outcomes have been measured in 93% . of the 997 men who declined to be randomly assigned and expressed a preference for a particular treatment , 529 ( 53% ) opted for active monitoring , 273 ( 27% ) for radical prostatectomy , 133 ( 13% ) for radiotherapy , 50 ( 5% ) for brachytherapy , and 12 ( 1% ) selected other treatments . 
 1114 vol 15 september 2014 articles these participants had similar clinical and sociodemographic characteristics to those who were randomly assigned ( table 4 ) , except that they were less likely to reside in an area of material deprivation ( or of increased deprivation in randomised versus non - randomised participants of 074 [ 95% ci 058094 ] )  . discussion the protect trial recruited and tested more than 82 000 community - based men aged 5069 years . 
more than 8000 men had a psa concentration of 30 g / l or more , and of those , 87% received a biopsy , resulting in nearly 3000 men diagnosed with prostate cancer ( 4% of those recruited )  . 
in this initial report , median 8 - year follow - up is more than 93% for all endpoints ( 99% for the primary outcome )  . to active monitoring , the ndings the robustness of the including three conventional the the protect trial was designed to address key issues in the management of clinically localised prostate cancer , speci cally the comparative e ectiveness and coste ectiveness of treatment trade - o between early modalities , diagnosis with psa testing and the risks of over - detection and over - treatment . 
trial design features that will enhance include standardised diagnostic , treatment , and follow - up protocols ; internal and external quality assurance processes ; allocation concealment ; high compliance with follow - up ; extensive secondary outcomes ; and an independent , masked primary endpoint committee . 
the recruitment process was based on psa testing , which is known to over - detect prostate cancer , and has the potential to be superseded by newer diagnostic modalities such as pre - biopsy imaging . 
 additionally , the long natural history of the disease means that the study will have taken more than 15 years to report , from rst patient participation in 1999 to the planned analysis of primary outcome after a median 10 - year follow - up in november , 2015 . 
furthermore , during the past decade radical surgery has evolved with the introduction of robot - assisted and laparoscopic techniques , but few of these new approaches were undertaken in this trial . 
other treatments have also changed : brachytherapy , dose escalation , and intensitymodulated radiotherapy are not being assessed in protect , and active surveillance cohorts now tend to focus on men with a gleason score of 6 points and use scheduled prostate biopsieseg , prias ( prostate cancer research international active surveillance ) .29 another limitation is that the lack of ethnic diversity in the study population might limit the applicability of the protect ndings to non - white populations . 
one patient from the feasibility study had a serum psa concentration of 209 g / l at the specialist nurse visit ; the concentration fell to 176 g / l on repeat measurement and he became eligible for recruitment . table 3 : participant and clinical characteristics at randomisation in the protect trial randomised ( n = 1643 ) non - randomised ( n = 997 ) p value 62 ( 4969 ) 62 ( 5069 ) married or living with partner 1375 ( 84% ) living in area of deprivation 239 ( 15% ) family history of prostate cancer 119 ( 7% ) 1606 ( 98% ) 10 ( < 1% ) 37 ( 2% ) 58 ( 30 ) 1266 ( 77% ) 339 ( 21% ) 37 ( 2% ) 1 ( < 1% ) 1249 ( 76% ) 394 ( 24% ) 984 ( 99% ) 2 ( < 1% ) 11 ( 1% ) 841 ( 84% ) 111 ( 11% ) 83 ( 8% ) 58 ( 31 ) 755 ( 76% ) 218 ( 22% ) 24 ( 2% ) 758 ( 76% ) 239 ( 24% ) 060 031 072 0015 028 067 042 096 4954 5559 6064 6569 psa ( g / l ) 3059 6099 100 gleason score 810 missing clinical stage age ( years ) * ethnic origin white other african - caribbean psa ( g / l ) gleason score 810 missing clinical stage data are median ( range ) or number ( % )  . 
 * 24 patients are classi ed as non - randomised because they were part of the early study with randomisation only between radical treatments ( not active monitoring )  . 
based on resident area - based material and social deprivation scores using several indicators of income and living conditionseg , percentage of social housing . table 4 : demographic and clinical characteristics at randomisation according to randomisation status in the protect trial vol 15 september 2014 1115 articles were men with a psa concentration of 20 g / l or higher because they were likely to harbour non - localised cancer and an increased risk of lymph node metastasis , as shown by joniau and colleagues.30 although we acknowledge that recent advances in imaging techniques would have improved staging in these patients , only 279 ( 03% ) of 82 429 participants in our tested cohort had a psa concentration of 20 g / l or higher . additionally , the recruited population could be generally healthier than the overall population , as often occurs in screening trials , but this does not a ect the compara tive e ectiveness analyses of treat ments.3 , 5 furthermore , uk statistics in 2008 suggested that prostate cancer mortality in the active monitoring group would be around 10% after 10 yearslower than expected at the trial outset . 
 therefore the mortality risk di erence of 46% , upon which the original sample size was based , roughly corresponds to a hazard ratio of 054 in the revised calculationa substantial bene t of radical compared with conservative management . 
should results from this trial support early active intervention , evidence will be needed that bene ts are su ciently large to outweigh the well recognised complications of radical treatments . 
 the primary analysis will be highly informative for clinicians , patients , and decision makers because the trial has been designed to consider mortality , resource use , and quality - of - life outcomes . 
and , as with the other treatment trials , the ndings will continue to be of interest as the data mature over time . treatment options the studys limitations need to be balanced against a number of strengths that ensure that the protect trial will be of pivotal importance in establishing the comparative e ectiveness of the three most frequently used in psa - detected clinically localised prostate cancer . 
it is the largest ongoing randomised controlled trial of prostate cancer treatments worldwide , with standardised protocols for diagnosis , treatment , and follow - up and enabling an assessment of screening through the linked cap trial . 
high levels of generalisability are assured by embedding protect within the cap randomised control trial of population - based psa testing involving about 15% of all uk men aged 5069 years recruited from randomly selected primary care centres . 
 participants with intermediate and some high - risk disease features were included and will help to establish whether active monitoring protocols can o er an alternative to immediate radical intervention in these patients . 
the planned subgroup analyses of treatment erspc ( europe ) 3 plco ( usa ) 5 protect ( uk ) pivot ( usa ) 6 spcg - 4 ( sweden ) 7 screening vs control screening vs control am vs rp vs rt 19932001 19992009 rp vs ww 19942002 rp vs ww 198999 199399 30 / 40 68 896 variable 38 350 228 966 100 444 psa tested ( % of attendees ) * 56 064 ( 2991% ) 34 244 ( 89% ) 82 559 ( 82% ) interventions recruitment period psa biopsy threshold ( g / l ) number of biopsy cores men invited men attended raised psa results biopsy uptake diagnosed with prostate cancer randomly assigned to treatment white ethnic origin mean psa , g / l clinical stage * not recorded gleason score * 26 ( erspc 27 ) * * 710 ( erspc 810 ) * * not recorded 27% 101 130 16% 05% 04% 35% 1643 ( 62% ) 5069 ( 61 ) age range , years ( mean age ) 5569 ( 6063 ) 5575 ( 60 ) 731 ( 15% ) < 75 ( 67 ) 695 ( nk ) < 75 ( 65 ) am = active monitoring . 
 * * erspc gleason grades 24 ( 15% ) and 57 ( 76% ) have been combined ; 810 ( 6% )  . table 5 : design , and participant and clinical characteristics , of the principal screening and treatment trials in clinically localised prostate cancer 1116 vol 15 september 2014 articles panel : research in context systematic review a systematic review of the evidence was done before the design of the trial and informed our protocol development . 
 the review was commissioned by the health technology assessment programme of the national institute for health research in the uk.36 the following search terms were used for a text search within the title , abstract , and keywords : prostate cancer and related terms , and therapy ( speci cally radiotherapy and prostatectomy )  . 
the systematic review concluded that there was insu cient evidence to establish the e ectiveness or cost - e ectiveness of screening or treatments for localised prostate cancer because of the shortage of robust randomised evidence at the time . interpretation the protect trial is , to our knowledge , the largest contemporary randomised controlled trial investigating the e ectiveness of conventional treatment options in men with clinically localised prostate cancer detected after psa testing . 
 the protect trial clearly di ers from two previously published treatment trials6 , 7 that compared surgery with watchful waiting ( a passive observational option ) in men with clinically detected disease ( spcg - 4 ) 7 and older veterans administration men with psa - detected disease ( pivot ) .6 in the protect trial , these baseline results show that we successfully recruited men aged 5069 years after community - based psa testing and a high proportion agreed to be randomly assigned between the three major conventional contemporary options ( surveillance , surgery , and radiotherapy ) , and have achieved high levels of follow - up . 
in 2016 , the trial will publish its outcome data . e ectiveness by stage and grade will investigate this aspect and assist comparison with spcg - 4 and pivot treatment trial patients . 
furthermore , the assessment of a radiotherapy and neoadjuvant regimen will be relevant for patients with higher risk disease because good evidence already exists for endocrine therapy combined with radiotherapy for advanced disease.31 protect detected more prostate cancer in the rst round of testing than did the erspc and plco trials , probably because of protects lower psa threshold combined with the minimum ten - core biopsy protocol in a population previously unexposed to routine psa testing . 
the clinical characteristics of the participants cancers in the protect trial are similar to those of other unscreened populations.32 cancer was generally detected at a lower stage and grade in protect participants than in a uk cohort of patients with clinically detected prostate cancer in the early 2000s.33 however , this reduction in stage and grade would have been mitigated by the upward grade migration reported in gleason scoring in nhs practice between 2000 and 2010.34 nevertheless , the mean proportion of uk men whose psa concentration has been tested remains low by international standards at 6% ( range 29 ) in primary care centres in the mid2000s . 
compared with the pivot6 and spcg - 47 treatment trials , protect participants had the lowest psa concentration , age , and included fewer higher stage cancers at the point of randomisation ( table 5 )  . 
 randomisation of eligible participants was higher in protect ( 62% ) than in pivot ( 15% ) , and other similar trials did not complete recruitment ( eg , start , spirit )  . 
 the acceptability of randomisation in the protect trial was enhanced by integrated qualitative research.35 most notably , protect participants received active monitoring , not watchful waiting as in pivot6 and spcg - 4.7 current active surveillance protocols have more restrictive entry criteria and rely more on scheduled re - biopsy than in protect , but protect trial results will provide , to our knowledge , for a monitoring strategy that includes the option of radical treatment ( panel )  . the rst randomised evidence in 2016 , the protect trial will provide data for the comparative e ectiveness and cost - e ectiveness of active monitoring , radical prostatectomy , and radiotherapy in men diagnosed with localised prostate cancer after psa testing with a median 10 - year follow - up . 
the major ndings will provide key information needed to underpin the management of clinically localised prostate cancer , including the crucial trade - o between survival gains and potential harm caused by over - detection and unnecessary radical treatment in psa - detected prostate cancer . contributors fch , jld , and den designed the protect trial and obtained the funding . 
jal , fch , jld , and den are the guarantors of the manuscript . declaration of interests jld reports grants from the uk national institute for health research ( nihr )  . 
all other authors declare no competing interests . acknowledgments the protect trial is funded by the uk national institute for health research ( nihr ) health technology assessment programme ( projects 96 / 20 / 06 , 96 / 20 / 99 ) with the university of oxford ( oxford , uk ) as vol 15 september 2014 1117 articles sponsor . 
we acknowledge the tremendous contribution of all the protect study participants , investigators , researchers , data monitoring committee , and trial steering comittee ( chair : michael baum )  . 
we acknowledge the support from the oxford nihr biomedical research centre through the surgical innovation and evaluation theme and the surgical interventional trials unit , and cancer research uk through the oxford cancer research centre . 
we are grateful to joke snoeck for her assistance in the preparation of this manuscript . articles gemcitabine and capecitabine with or without telomerase peptide vaccine gv1001 in patients with locally advanced or metastatic pancreatic cancer ( telovac ) : an open - label , randomised , phase 3 trial gary middleton , paul silcocks , trevor cox , juan valle , jonathan wadsley , david propper , fareeda coxon , paul ross , srinivasan madhusudan , tom roques , david cunningham , stephen falk , nick wadd , mark harrison , pippa corrie , tim iveson , angus robinson , karen mcadam , martin eatock , je evans , caroline archer , tamas hickish , angel garcia - alonso , marianne nicolson , william steward , alan anthoney , william greenhalf , victoria shaw , eithne costello , dean naisbitt , charlotte rawcli e , gemma nanson , john neoptolemos summary background we aimed to assess the e cacy and safety of sequential or simultaneous telomerase vaccination ( gv1001 ) in combination with chemotherapy in patients with locally advanced or metastatic pancreatic cancer . methods telovac was a three - group , open - label , randomised phase 3 trial . 
 eligible patients were treatment naive , aged older than 18 years , with locally advanced or metastatic pancreatic ductal adenocarcinoma , and eastern cooperative oncology group performance status of 02 . 
patients were randomly assigned ( 1 : 1 : 1 ) to receive either chemotherapy alone , chemotherapy with sequential gv1001 ( sequential chemoimmunotherapy ) , or chemotherapy with concurrent gv1001 ( concurrent chemoimmunotherapy )  . 
chemotherapy included six cycles of gemcitabine ( 1000 mg / m , 30 min intravenous infusion , at days 1 , 8 , and 15 ) and capecitabine ( 830 mg / m orally twice daily for 21 days , repeated every 28 days )  . 
sequential chemoimmunotherapy included two cycles of combination chemotherapy , then an intradermal lower abdominal injection of granulocyte - macrophage colony - stimulating factor ( gm - csf ; 75 g ) and gv1001 ( 056 mg ; days 1 , 3 , and 5 , once on weeks 24 , and six monthly thereafter )  . 
this study is registered as an international standard randomised controlled trial , number isrctn4382138 . findings the rst patient was randomly assigned to treatment on march 29 , 2007 , and the trial was terminated on march 27 , 2011 . 
of 1572 patients screened , 1062 were randomly assigned to treatment ( 358 patients were allocated to the chemotherapy group , 350 to the sequential chemoimmunotherapy group , and 354 to the concurrent chemoimmunotherapy group )  . 
median overall survival was not signi cantly di erent in the chemotherapy group than in the sequential chemoimmunotherapy group ( 79 months [ 95% ci 7188 ] vs 69 months [ 6476 ] ; hazard ratio [ hr ] 119 , 9825% ci 097148 , p = 005 ) , or in the concurrent chemoimmunotherapy group ( 84 months [ 95% ci 7397 ] , hr 105 , 9825% ci 085129 , p = 064 ; overall log - rank of 2df = 43 ; p = 011 )  . 
results from studies in other patients with cancer have shown that gv1001 induces the expression of cd8 cytotoxic t cells and can initiate epitope spreading.1013 although cytotoxic drugs are generally regarded as immunosuppressive , some chemotherapy regimens might potentiate the e ect of cancer vaccines.1419 gemcitabine and uorouracil induce apoptosis of cancer cells leading to the release of antigens that can be taken up by professional antigen - presenting cells , and cross - presented to prime cytotoxic t cells.14 , 20 ligation of cd40 on antigen - presenting cells with cd40l present on activated cd4 cells determines the generation of cytotoxic t cells . 
gv1001 vaccination was expected to generate telomerase - speci c t - helper cells to activate several antigen - presenting cells loaded with diverse antigens , to prime and activate cytotoxic t cells with a broad repertoire . 
synergy between cd40 ligation and gemcitabine is highest when gemcitabine is given before cd40 ligation.21 chemotherapy delivered after immuno therapy can enhance the e ect of immunotherapy by delivering a bolus of tumour antigens and immuno stimulatory signals.15 thus from preclinical studies showed synergy between gemcitabine and both cd40 agonism and vaccines in vitro and in mice.14 , 15 , 21 results the combination of gemcitabine and capecitabine ( an orally active uorouracil pro - drug ) is a standard of care for patients with pancreatic cancer , with improved objective response and time to progression compared with gemcitabine monotherapy.22 the design of the telovac study was based on the clear clinical evidence of immunogenicity of gv1001 in patients with pancreatic cancer , the available preclinical data showing the synergy of gemcitabine with cancer vaccines and the other positive immunomodulatory e ects of gemcitabine and uoropyrimidines . 
thus the telovac study aimed to exploit the positive immunomodulatory e ects of these agents and tested the e ect of combining them with gv1001 with granulocyte - macrophage colony - stimulating factor ( gm - csf ) as an adjuvant.23 methods study design and participants telovac was a multicentre , three - group , open - label , phase 3 randomised controlled trial done at 51 uk hospitals . 
the protocol can be viewed online . eligible patients were treatment naive , aged older than 18 years , with histologically or cytologically con rmed locally advanced or metastatic pancreatic ductal adenocarcinoma , an eastern cooperative oncology group ( ecog ) performance status of 02 , and adequate end organ function . 
other speci c inclusion criteria were locally advanced or metastatic disease precluding curative surgical resection or patients who had relapsed following previously resected pancreatic cancer ; contrast enhanced ct scan of the thorax , abdomen , and pelvis within 28 days before commencing treatment ; uni dimensionally measurable disease on ct in accordance with the response evaluation criteria in solid tumors ( recist 1.0 ) guidelines ; platelet count equal or higher than 100 10 cells per l , white blood cell count ( wbc ) equal or higher than 3 10 cells per l , and neutrophil count equal or higher than 15 10 cells per l at entry ; serum bilirubin equal or lower than 35 mol / l ; calculated creatinine clearance higher than 50 ml / min ( cockcroft and gualt ) ; and a life expectancy longer than 3 months . 
the estimated median survival of eligible patients was 71 months ( 95% ci 6278 ) .22 we excluded patients if they had had radiotherapy within the last 4 weeks before start of study treatment ; no other pre - treatment information on radiotherapy was obtained as radiotherapy was not used in the uk for locally advanced pancreatic cancer . 
speci c exclusion criteria were medical or psychiatric conditions compromising informed consent ; intracerebral metastases or meningeal carcinomatosis ; clinically signi cant serious disease or organ system disease not currently controlled on present therapy ; uncontrolled angina pectoris ; pregnancy or breastfeeding ; previous chemotherapy for locally advanced and metastatic disease ; concurrent malignancies or invasive cancers diagnosed within the past 5 years apart from adequately treated basal - cell carcinoma of the skin , in - situ carcinoma of the uterine cervix , or resected pancreatic cancer ; known malabsorption syndromes ; hyper sensitivity to any of the investigational products or patients with a dihydropyrimidine dehydrogenase de ciency ; medi cation that might a ect immuno competence such as long - term steroids or other immunosuppressants for an unrelated condition ; men or women of reproductive potential , unless using at least two contraceptive precautions , one of which must be a condom . the trial conformed the international conference on harmonisation on good the principles of 830 vol 15 july 2014 articles for the protocol see asp ? id = 42&tgcode = 4&menuid = 43 see online for appendix clinical practice , and was undertaken by the cancer research uk liverpool cancer trials unit ; pharmacovigilance was subcontracted to orion clinical services ltd ( slough , uk )  . 
all participants provided written , informed consent before randomisation . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to receive either chemotherapy alone , chemotherapy with sequential gv1001 ( sequential chemoimmunotherapy group ) , or chemotherapy with concurrent gv1001 ( concurrent chemo immunotherapy group )  . 
the allocation sequence was generated by the then trial statistician and was held centrally with access restricted to the senior statistician , the senior trial co - ordinator , and the data managers . 
all patients and investigators were aware of the treatment allocation . procedures patients randomly assigned to the chemotherapy group received gemcitabine ( 1000 mg / m , 30 min intravenous infusion on days 1 , 8 , and 15 ) and capecitabine ( 830 mg / m orally twice daily for 21 days ) repeated every 28 days for six cycles , or until disease progression , development of cumulative toxic e ects or patient discontinuation ( appendix ) .22 patients randomly assigned to sequential chemoimmunotherapy received two cycles of combination chemotherapy as above , and were subsequently immunised with an intradermal injection of recombinant gm - csf ( 75 g ) into the lower abdomen , and 1015 min later , with an intradermal injection at the same site of 056 mg of gv1001 ( 200 ml of 28 mg / ml ) .10 immunisation was undertaken on days 1 , 3 , and 5 during week 1 , then once on weeks 2 , 3 , 4 , and 6 and then monthly . 
if disease progression occurred , as measured by ct scan , gv1001 was stopped and gemcitabine and capecitabine was restarted . patients randomly assigned to concurrent chemoimmunotherapy received combination chemo therapy as in the chemotherapy alone group for six cycles with gm - csf and gv1001 from day 1 of therapy as in the sequential chemoimmunotherapy group and then received just immunotherapy at the end of cycle six . 
capecitabine interrupted following the rst doses were to be appearance of any grade 2 non - haematological adverse events ( the most frequent side - e ects were gastrointestinal disorders , especially diarrhoea , nausea , vomiting and stomatitis , and hand - foot syndrome ) until resolved to grade 01 , and to maintain normal dose level subsequent for the next cycle . 
if any grade 2 non - haematological adverse events appeared for a second time , capecitabine was to be interrupted and reduced to 75% with prophylaxis in the next cycle ; and if any events appeared for a third time , capecitabine was to be interrupted and reduced to 50% in the next cycle . 
the occurrence of any grade 3 adverse events followed the same discontinuation rules for capecitabine for their rst and second appearances , but capecitabine was discontinued permanently after the third appearance of a grade 3 nonhaematological adverse event . 
if patients had an episode of any - grade febrile neutropenia , or had a neutrophil count lower than 05 10 cells per l , or a platelet count lower than 50 10 cells per l , then capecitabine was withheld and omitted until resolved to grade 01 toxic e ects , at which point patients could restart capecitabine at a 75% dose . patients could withdraw by deciding to discontinue the trial , because of disease progression according to recist , or due to intolerable adverse e ects . 
patients had to withdraw because of pregnancy ; recurrent grade 3 or 4 drug - related toxic e ects despite dose modi cation , serious systemic allergic reaction to any of the study drugs eg , angio - oedema or anaphylaxis , intercurrent , unrelated conditions requiring long - term use of steroids ; missing two consecutive gv1001 administrations , or three gv1001 the entire non - consecutive administrations during treatment course ; or missing two consecutive cycles of gemcitabine and capecitabine administrations or three non - consecutive cycles during the entire treatment course . 
 we used the national cancer institute common toxicity criteria for adverse events version 3 to record toxic e ects . we tested for delayed - type hypersensitivity in the chemoimmunotherapy groups by giving a second intradermal injection of 0105 mg of gv1001 simultaneously at the contralateral site on the lower abdomen without concomitant gm - csf . 
we continued testing for delayed - type hypersensitivity until the result was positive , or the vaccine therapy discontinued . we assessed t - cell proliferation in a subset of patients ( from volunteer sites that had the facilities to collect and immediately process samples )  . 
we seeded thawed peripheral blood mononuclear cells ( pbmcs ) in 48 - well plates ( thermofisher scienti c , usa ) at 2 10 cells per well in x - vivo 15 ( lonza , uk ) with 10% pooled human serum ( innovative research , usa ) and 20 g / ml of gv1001 peptide . 
on day 11 , we harvested the gv1001 - enriched cells and placed them in a round bottom 96 - well plate ( 50 l , 1 10 cells per well )  . 
to the pre - stimulated cells , we added irradiated ( 45 gy ) autologous pbmcs ( 50 l , 1 10 cells per well ) to act as antigen - presenting cells . 
we tested for gv1001 - speci c 832 vol 15 july 2014 articles number of patients number of deaths median survival in months ( 95% ci ) 12 - month survival ( 95% ci ) hazard ratio * ( 9825% ci ) log - rank rank test , p value * chemotherapy alone group 245 ( 68% ) 79 ( 7188 ) 337% ( 282392 ) sequential chemoimmunotherapy group 268 ( 77% ) 69 ( 6476 ) 253% ( 202305 ) concurrent chemoimmunotherapy 259 ( 73% ) 84 ( 7397 ) 323% ( 268378 ) 12 ( 1.015 ) 105 ( 0813 ) 00466 06378 ecog = eastern cooperative oncology group . 
 table 2 : overall survival proliferation by adding 100 l of either : control media , 20 g / ml of gv1001 , or 5 g / ml of phytohaemagglutinin ( pha ) as a control . 
we de ned a positive total immune response as a positive test for delayed - type hypersensitivity or a positive proliferation assay , or both . outcomes the primary endpoint was overall survival . 
the secondary endpoints were safety , time to progression , objective tumour response , quality of life , changes in ca19 - 9 concentration over time , and immunogenicity ( measured as delayed type hyper sensitivity and t - cell proliferation )  . statistical analysis to detect a 10% improvement in 1 - year survival for either experimental group ( above the 25% survival expected in the chemotherapy group ) , an enrolment of 1110 patients , with 780 deaths expected , was required . 
a two - sided of 0025 ( corresponding to a 975% ci ) was set for each primary response comparison of chemoimmunotherapy versus standard chemotherapy , with a total 005 level of signi cance and at least 80% power for the trial as a whole . 
the sample size additionally adjusted for four formal interim and one nal analysis on the primary endpoint ( obrienfleming type boundaries based on the lan - demets - spending function )  . 
in practice , as the trial terminated early , we applied 9825% cis ( signi cance of 00175 ) to all analyses of the primary including comparison between treatment endpoint groups . the nal analysis was done on the intention - to - treat population , consisting of all patients randomly assigned to treatment , except for patients who withdrew consent between randomisation and the start of therapy , and patients who were withdrawn from the study after randomisation because of irregularities with the consent process . 
 * ca19 - 9 not available for 47 patients . table 3 : survival factors by univariate analysis the chief primary endpoint , investigator reviewed deviations to identify protocol deviations that would a ect the outcome . 
sensitivity vol 15 july 2014 articles local , ecog 0 local , ecog 1 local , ecog 2 metatastic , ecog 0 metatastic , ecog 1 metatastic , ecog 2 overall ( i2 = 00% , p = 0895 ) local , ecog 0 local , ecog 1 local , ecog 2 metatastic , ecog 0 metatastic , ecog 1 metatastic , ecog 2 overall ( i2 = 00% , p = 0920 ) analyses included testing the proportional hazards assumption , additional strati cation for ca19 - 9 concentration , allowance for random centre e ect , and testing for interaction between treatment and centre . 
 overall survival and time to progression were estimated by the kaplan - meier method , with hazard ratios ( hrs ) and con dence intervals obtained from a strati ed cox model and p values the corresponding strati ed log - rank test ( strata as de ned for the randomisation )  . 
for other pre - speci ed outcomes ( including time to progression ) , for descriptive analyses including only one group , and for unplanned from chemotherapy alone sequential chemoimunotherapy concurrent chemoimmunotherapy number at risk chemotherapy alone sequential chemoimmunotherapy concurrent chemoimmunotherapy time from randomisation ( months ) 0196 100 511 favours sequential chemoimmunotherapy favours standard chemotherapy weight ( % ) hr ( 95% ci ) p value 881% 1708% 225% 1872% 4349% 964% 10000% 120 ( 059246 ) 052 094 ( 061158 ) 080 124 ( 038513 ) 100 118 ( 078192 ) 039 131 ( 100181 ) 006 124 ( 070246 ) 038 weight ( % ) hr ( 95% ci ) p value 855% 1804% 270% 1798% 4337% 936% 10000% 085 ( 041176 ) 062 107 ( 065177 ) 078 084 ( 023307 ) 082 105 ( 064174 ) 084 103 ( 075143 ) 083 137 ( 068275 ) 032 analyses , we used a conventional 95% two - sided ci with no correction . 
this trial is registered as an international standard randomised controlled trial , number isrctn4382138 . role of the funding source neither the sponsors nor funders had any role in the design and conduct of the study ; the collection , management , analysis , and interpretation of the data ; the the preparation , review , or approval of nor presentation . 
the academic chief investigator gm and the principal grant holder jn had full access to all the data in the study , and take full responsibility for the integrity of the data and the accuracy of the data analysis.the corresponding author had nal responsibility to submit for publication . results the rst patient was randomly assigned to treatment on march 29 , 2007 , and the trial was terminated slightly ahead of target , on march 27 , 2011 , because of unfavourable survival in the sequential chemo immunotherapy group . 
 to receive 358 patients were randomly assigned gemcitabine and capecitabine alone ( chemotherapy group ) , 350 to gemcitabine and capecitabine and then sequential gv1001 ( sequential chemoimmunotherapy group ) , and 354 to gemcitabine and capecitabine and concurrent gv1001 ( concurrent chemoimmunotherapy group ; gure 1 )  . 
baseline characteristics were well balanced across all three groups ( table 1 )  . 772 patients died during the study ; the 290 patients still alive were followed up for a median of 60 months ( iqr 24122 )  . 
median overall survival was 76 months ( 95% ci 7181 ) with 12 - month survival of 304% ( 95% ci 273336 ) , and 24 - month survival of 94% ( 72120 ) ( table 2 )  . 
baseline clinical stage , blood ca19 - 9 levels , and ecog performance status were all associated with survival ( p < 00001 for each factor on univariate analysis ; table 3 )  . 
 patients on sequential chemoimmunotherapy with a positive delayed - type hypersensitivity response had a median survival of 75 months ( 95% ci 3595 ) those with a negative response a median and overall survival of 58 months ( 3971 , hr 095 ; 95% ci 049184 ; 1df = 0036 , p = 085 ; gure 4 )  . 
 median survival in patients on concurrent chemoimmuno therapy with a positive delayed - type hypersensitivity response was 90 months ( 95% ci 61109 ) and 80 months ( 6687 ) for those with a negative response ( hr 098 , 060159 ; 1df = 0015 , p = 090 ; gure 4 )  . there was no signi cant di erence in t - cell proliferation between chemoimmunotherapy groups ; t - cell proliferation was positive in ten ( 31% ) of 32 patients given sequential chemoimmunotherapy and ten ( 15% ) of 68 patients given concurrent chemoimmunotherapy ( p = 0065 )  . 
12 ( 38% ) of 32 patients on sequential immunotherapy ( 40% of the 30 patients without any missing values ) had a total immune response , as did 25 ( 37% ) of 68 patients on concurrent chemo immuno therapy ( 40% of the 63 without missing values )  . 
median survival ( from week 18 ) in patients on sequential immunotherapy group with a positive total immune response was 84 months ( 95% ci , 70na ) and 73 months ( 95% ci 30292 ) with a negative response ( hr 028 , 95% ci , 005153 ; 1df = 2368 , p = 012 )  . 
median survival ( from week 10 ) in patients randomly assigned to concurrent chemoimmunotherapy was 106 months ( 95% ci 62137 ) and 122 months ( 72166 ) respectively ( hr 157 , 95% ci 071349 ; 1df = 1241 , p = 027 ; appendix )  . 
 the per - protocol analysis was undertaken after removing 62 patients who deviated from the protocol ( 21 patients in the chemotherapy group alone , 21 in the sequential chemo immunotherapy group , and 20 in the concurrent chemo immunotherapy )  . 
the lack of treatment e ect on survival was consistent between tumour stages ( global likelihoodratio test for treatment stage interaction , 2df = 273 , p = 026 )  . 
patients assigned to either sequential or concurrent chemo immunotherapy with a lower tumour burden ( locally advanced disease ) or a good performance status ( ecog 0 ) had no survival bene t when compared with those assigned to chemotherapy alone ( gure 2b , c )  . 
 an unplanned post - hoc analysis showed that the overall survival of the 84 patients who were randomly assigned to sequential chemo immunotherapy , and subsequently returned to standard chemotherapy following progression on vaccination therapy , and were alive at 18 weeks , did not di er from that of patients alive at 18 weeks randomly assigned to standard chemotherapy ( hr 084 ; 95% ci 058123 ; p = 028 ; appendix )  . we assessed the possibility that treatment e ects might di er according to tumour stage , ecog performance status , and ca19 - 9 concentration by a likelihood ratio test nesting a main - e ects - only model within one including interactions between treatment group and each of the other factors , but this analysis showed no di erence ( 12df = 1376 , p = 032 )  . median time to progression was not signi cantly di erent in the chemotherapy group compared to the sequential chemoimmunotherapy group ( 64 months [ 95% ci 4871 ] vs 45 months [ 4346 ] ; hr 150 , 95% ci 126178 , p < 00001 ) , nor the concurrent chemoimmunotherapy group ( 66 [ 5073 ] , hr 10 , 95% ci 084119 ; p = 099 ; overall log - rank 2df = 295 ; p < 00001 ; gure 3 )  . ( 7% ) of 350 patients a partial or complete tumour response was noted at 8 weeks in 36 ( 10% ) of 358 patients in the chemotherapy the alone group , 25 sequential chemo immunotherapy group , and 29 ( 8% ) of 354 patients in the concurrent chemoimmunotherapy group ; there was no signi cant di erence between the three groups . 
an overall response ( complete plus partial response at any time ) was noted in 63 ( 18% ) of 358 patients in the chemotherapy alone group , 31 ( 9% ) of 350 patients in the sequential chemoimmunotherapy group , and 55 ( 16% ) of 354 patients in the concurrent chemoimmunotherapy the sequential chemoimmunotherapy group achieved signi cantly fewer overall responses than those in the chemotherapy alone group ( p = 0001 )  . group ; patients the proportion of delayed - type hypersensitivitypositive patients did not di er between immunochemotherapy groups ; 19 ( 12% ) of 154 patients assigned vol 15 july 2014 articles number at risk dth negative dth positive number at risk dth negative dth positive dth negative dth positive time from randomisation ( months ) positive total immune response was 115 ( 95% ci 056238 ; 1df = 3208 , p = 0073 )  . from e ects sequential the standard chemotherapy regimen was well tolerated and there was no evidence of any additional toxic concurrent chemoimmunotherapy ( table 4 )  . 
there were 32 ( 3% ) patients altogether who withdrew because of toxic e ects , 15 ( 4% ) patients from the standard chemotherapy group , four ( 1% ) from the sequential chemo immunotherapy group , and 13 ( 4% ) from the concurrent chemoimmunotherapy group ( 2df = 64 ; p = 004 )  . 
there were four ( 1% ) deaths due to drugrelated toxic e ects in the standard chemotherapy group , ve ( 1% ) in the sequential chemoimmunotherapy group , and six ( 2% ) in the concurrent chemo immunotherapy group ( p = 081 )  . patients randomly assigned to sequential immunotherapy had a signi cantly higher pain score than did patients randomly assigned to standard chemotherapy at 20 weeks ( table 5 )  . discussion our ndings showed that the addition of the gv1001 vaccine to gemcitabine and capecitabine did not improve survival in patients with advanced pancreatic cancer . 
the total immune response in the phase 2 study compared with that seen in the current study is consistent with the reduction in response rates generally noted in the transition from phase 2 to phase 3 studies ( 12 of 17 [ 71% ] patients in the phase 2 study vs 12 of 32 and 25 of 68 [ 37% overall ] in the phase 3 study ; panel ) .10 for a cancer vaccine to be e ective , an active immune response is needed , which is dependent on a su cient period of time for this response to develop . 
the characteristic early metastasising and rapidly progressive nature of pancreatic cancer might partly explain the absence of clinical e cacy , but other complex immunological and stromal factors also need to be overcome.25 , 28 , 30 a dense stromal reaction has been shown to impede the penetration of cytotoxics into pancreatic tumours , thus restricting the synergistic potential of chemotherapy and gv1001 vaccination intended to achieve cd40 activation and generate telomerase - speci c t - helper cells.25 direct cd40 activation ( using the agonist cp - 870 , 893 ) with gemcitabine chemotherapy has recently been shown to cause a partial tumour response in four of 21 patients with advanced pancreatic cancer , but this e ect was surprisingly due to stroma - in ltrating macrophages rather than t cells.28 an e ective active immune response might also depend on a lower tumour burden and good performance status , but recent studies from other tumour types do not seem to support this . 
in a randomised phase 2 trial of prostate cancer including prostvac - vf ( consisting of two prostate speci c antigen [ psa ] encoding viral vectors , and the b71 , icam - 1 , and lfa - 3 co - stimulatory molecules ) and gm - csf , no survival improvement was noted in men with fewer bony metastases or an ecog performance status of zero.31 similar ndings were noted in the impact phase 3 trial in men treated with sipuleucel - t , which is a form of active cellular immunotherapy ( autologous pbmcs activated with the recombinant pa2024 protein composed of a prostate antigen and prostatic acid phosphatase , fused to gm - csf ) .32 in the telovac trial , we noted no e ect of gv1001 vaccination on survival by either stage of disease or performance status . identi cation of robust immunotherapy response signatures in human cancer studies remains challenging across tumour types . 
in the prostvac - vf trial , 31 no antibody response to psa was noted , and although all patients generated titres to one or both viral vectors , no association with survival was noted . 
in the impact trial , 32 although there was a t - cell proliferation response to pa2024 in 46 ( 73% ) of 63 patients given sipuleucel - t , only 15 ( 27% ) of 55 patients had a t - cell response against the target antigen prostatic acid phosphatase . 
the scarce immunotherapeutic figure 4 : overall survival according to a positive or negative delayed - type hypersensitivity response in patients assigned to chemoimmunotherapy ( a ) patients randomly assigned to sequential chemoimmunotherapy , conditional on reaching week 18 . 
in a trial30 of an anti - pd - l1 antibody ( bms - 936559 ) 207 patients , objective responses were reported in malignant melanoma , renal - cell cancer , non - small - cell lung cancer , and ovarian cancer but none in 14 patients with advanced pancreatic cancer . 
the relative absence of immuno therapy e cacy in pancreatic cancer might also to speci c carcinoma - associated partly be related broblasts ( expressing broblast activation protein ) , which secrete cxcl12 and thus stop t cells from accessing cancer cell regions in the stroma . 
in a genetically engineered mouse model of pancreatic cancer blocking the receptor of cxcl12 , induced rapid t - cell accumulation and synergised with - pd - l1 in cancer cell killing.29 there have been concerns raised about the use of gmcsf as adjuvant based on the induction of myeloid derived suppressor cells ( mdscs ) by low - dose gmcsf , 35 but we have shown that the concentrations of mdscs were reduced in patients treated with gv1001 , gm - csf , and concomitant chemotherapy compared with chemotherapy alone.36 there was a shorter time to progression observed after the administration of two cycles of chemotherapy in the sequential chemoimmunotherapy group than the other two groups . 
a post - hoc analysis showed that the overall survival in this group of patients who returned to standard chemotherapy following progression on vaccination therapy was not di erent from similar patients randomly assigned to standard chemotherapy . 
 these ndings suggest that treatment until progression is the appropriate approach in pancreatic cancer and is consistent with recent ndings that a minimum of six cycles of chemotherapy is necessary for optimum survival bene t in the adjuvant setting.37 the telovac study has shown the challenges for immunotherapy study design when immunotherapy is combined with standard therapy in the rst - line setting and highlights the uncertainties in extrapolating treatment scheduling from experimental models to the clinical setting . 
one option that had been considered was vaccination after 838 vol 15 july 2014 articles panel : research in context systematic review in trial set up for the treatment of locally advanced and metastatic pancreatic cancer , two systematic reviews were undertaken.24 , 25 medline , oldmedline , cancerlit , embase , and isi web of science , isi science and technology proceedings , current contents databases , trial registries , and conference proceedings were searched , and results identi ed included randomised controlled trials involving patients with advanced pancreatic cancer of chemotherapy , novel agents , radiotherapy , chemoradiotherapy , and best supportive care . 
 we searched pubmed for any clinical trial and experimental work for telomerase , immunotherapy , vaccines , cancer , pancreatic cancer , and gv1001 , with no restrictions.26 the reviews showed that chemoradiation followed by chemotherapy did not show any survival advantage over chemotherapy alone . 
the combination of gemcitabine with capecitabine was chosen as this could potentiate the vaccine e ects , and was also associated with signi cantly improved objective responses compared with gemcitabine alone.22 , 24 , 25 interpretation we noted no survival bene t from the addition of the gv1001 vaccine to gemcitabine and capecitabine in patients with advanced pancreatic cancer . 
during the course of the trial there has been a major development in clinically relevant genetically engineered models that has signi cantly contributed to the deeper understanding of the biological mechanisms that undermine the e ective treatment of pancreatic cancer.2729 these can now be countered and could be deployed in multimodality strategies to overcome the key biological constraints to e ective treatment . 
 six cycles of chemotherapy rather than two cycles but it was important to test the institution of vaccination after initial stabilisation of disease before progression , and at a time when apoptosis was likely to be still high . 
in this study , the median time to progression on chemotherapy alone was 64 months ( 95% ci 95% ci 4871 ) ; therefore 50% of patients would have progressed at this point . 
for future immunotherapy trials , randomised phase 2 studies using adaptive trial designs should be seriously considered to explore di erent scheduling regimens that do not compromise standard treatment . the telovac trial has shown that vaccination to htert can elicit immune responses during chemotherapy but without clinical e cacy . 
there are presently a number of di erent approaches being used to target telomerase in cancer including small - molecule telomerase inhibitors that might be more e ective in tumours with shorter telomeres.38 , 39 opportunities to uncloak the mechanism of action of vaccines such as gv1001 using multimodality strategies that are directed against the stroma and check point inhibition as well as direct cd40 activation should be explored . contributors development of the study design was supported and conducted through national cancer research institute ( ncri ) of the uk pancreatic cancer sub - group and the cruk liverpool cancer trials unit ( of the liverpool clinical trials unit ) and was led by the telovac working party composed of gm , jn , dc , tc , ps , jv , jw , dp , fc , pr , sm , tr , and pc . 
the results were interpreted by the telovac working party , which prepared the initial draft and were responsible for collating changes proposed by all of the authors into the nal draft paper before nal approval by all participants telovac study group . 
the specialists who also contributed to the recruitment , treatment , and follow - up of patients as trial site principle investigators , along with sites and number of patients recruited are shown in the appendix . declaration of interests jw reports personal fees from astra zeneca , celgene , and novartis outside the submitted work . 
pr reports personal fees from roche ; grants and personal fees from merck serono , sano aventis ; personal fees from cellgene , bayer , novartis , bristol - myers squibb , and sirtex , outside the submitted work . 
jn reports grants from cancer research uk ; grants and personal fees from kael gemvax , during the conduct of the study ; and personal fees from oxford biomedica ( uk ) ltd , pzifer novartis , astellas , and novartis pharma ag , outside the submitted work . 
ec , tc , wg , dn , gn , cr , ps , and vs report grants from cancer research uk ; and grants and personal fees from kael gemvax , during the conduct of the study . 
we thank the independent data and safety monitoring committee which consisted of chris russell ( university college london , london , uk ) , roger ahern ( institute of cancer research , sutton , uk ) , and david chao ( the royal free hospital , london , uk )  . 
 novel molecular subgroups for clinical classification and outcome prediction in childhood medulloblastoma : a cohort study edward c schwalbe , janet c lindsey , sirintra nakjang , stephen crosier , amanda j smith , debbie hicks , gholamreza rafiee , rebecca m hill , alice iliasova , thomas stone , barry pizer , antony michalski , abhijit joshi , stephen b wharton , thomas s jacques , simon bailey , daniel williamson , steven c clifford summary background international consensus recognises four medulloblastoma molecular subgroups : wnt ( mbwnt ) , shh ( mbshh ) , group 3 ( mbgrp3 ) , and group 4 ( mbgrp4 ) , each defined by their characteristic genome - wide transcriptomic and dna methylomic profiles . 
we aimed to investigate whether additional molecular subgroups exist within childhood medulloblastoma and whether these could be used to improve disease subclassification and prognosis predictions . methods in this retrospective cohort study , we assessed 428 primary medulloblastoma samples collected from uk childrens cancer and leukaemia group ( cclg ) treatment centres ( uk ) , collaborating european institutions , and the ukccsg - siop - pnet3 european clinical trial . 
we did comprehensive molecular profiling , including dna methylation microarray analysis , and did unsupervised class discovery of test and validation cohorts to identify consensus primary molecular subgroups and characterise their clinical and biological significance . 
we modelled survival of patients aged 316 years in patients ( n = 215 ) who had craniospinal irradiation and had been treated with a curative intent . findings seven robust and reproducible primary molecular subgroups of childhood medulloblastoma were identified . 
mbshh was split into agedependent subgroups corresponding to infant ( < 43 years ; mbshh - infant ; n = 65 ) and childhood patients ( 43 years ; mbshh - child ; n = 38 )  . 
cross - validated subgroup - dependent survival models , incorporating these novel subgroups along with secondary clinicopathological and molecular features and established disease risk - factors , outperformed existing disease risk - stratification schemes . 
these subgroupdependent models stratified patients into four clinical risk groups for 5 - year progression - free survival : favourable risk ( 54 [ 25% ] of 215 patients ; 91% survival [ 95% ci 82100 ] ) ; standard risk ( 50 [ 23% ] patients ; 81% survival [ 7094 ] ) ; highrisk ( 82 [ 38% ] patients ; 42% survival [ 3156 ] ) ; and very high - risk ( 29 [ 13% ] patients ; 28% survival [ 1456 ] )  . interpretation the discovery of seven novel , clinically significant subgroups improves disease risk - stratification and could inform treatment decisions . 
these data provide a new foundation for future research and clinical investigations . funding cancer research uk , the tom grahame trust , star for harris , action medical research , sparks , the jgw patterson foundation , the instinct network ( co - funded by the brain tumour charity , great ormond street childrens charity , and children with cancer uk )  . copyright the author ( s )  . 
 profiling and class discovery studies published to date in medulloblastoma are based on cohorts typically with sample sizes less than 200 patients and , even within the consensus subgroups , significant heterogeneity of clinical and molecular features remains and many relationships to disease outcome are unresolved . 
evidence from the component studies and reviews undertaken in the international consensus definition and the 2016 who classification , alongside our own reviews of the current literature , formed the foundation for the present study ; no systematic reviews were carried out . added value of this study we defined and characterised seven robust , reproducible , clinically significant , primary molecular subgroups within childhood medulloblastoma ( in children aged up to 16 years at diagnosis ) , each with distinct clinicomolecular features . 
we propose a cross - validated , subgroup - dependent survival model that incorporates these novel subgroups , alongside established disease features and risk - factors and outperforms the disease risk - stratification schemes in current clinical use . 
redistribution of disease risk using this scheme identifies substantial proportions of favourable - risk non - infant patients ( > 90% 5 - year survival in 11% of patients ) outside the mbwnt subgroup ( equivalent to approximately 70 patients per year in the european union [ eu ] ) who would be suitable for consideration of reduced intensity of therapy , and very - high - risk non - infant patients ( < 40% survival , 13% of patients , about 80 eu patients per year ) for whom new treatment strategies should be prioritised . implications of all the available evidence these data provide a step - change in our understanding and characterisation of molecular subgroups within medulloblastoma , with potential application to future disease subclassification , risk - stratification , and subgroup - dependent translational research . integral subgrouping the 2016 who medulloblastoma classification , 13 and is used to direct treatment strategies aimed at improving cure rates ( 5 - year survival across all four subgroups is 6570% ) , and reducing long - term intellectual and neuroendocrine impairments associated with existing multimodality therapies . 
 clinically methods study design and participants in this retrospective cohort study , we assessed 428 centrally reviewed , clinically annotated primary medulloblastomas from patients aged 016 years at diagnosis , collected from uk childrens cancer and leukaemia group ( cclg ) treatment centres ( uk ; 366 [ 86% ] ) , collaborating european institutions in budapest ( hungary ; 20 [ 5% ] ) and warsaw ( poland ; 15 [ 4% ] ) , and samples from the european ukccsg - siop - pnet3 clinical trial ( 27 [ 6% ] )  . 
108 ( 26% ) of 408 patient samples used were collected in 201014 , 192 ( 47% ) in 200010 , 85 ( 21% ) in 19902000 , and the remaining 23 ( 6% ) were collected before 1990 ( 18 were from the 1980s , four from the 1970s , and one was from 1968 )  . 
tumour investigations were done with vol 18 july 2017 articles see online for appendix approval from newcastle north tyneside research ethics committee ( study reference 07 / q0905 / 71 ) ; all tumour material was collected in accordance with this approval . 
18 post - mortem cerebellar samples were collected from the newcastle brain tissue resource and used as controls in some analyses ; all samples were collected with written , informed consent . procedures we tested medulloblastoma samples with the illumina humanmethylation450k dna methylation array ( illumina , san diego , ca , usa )  . 
the gene expression omnibus accession number for 450k dna methylation array profiles we used for the determination of human medulloblastoma molecular subgroup status is gse93646 . to identify methylation - dependent subgroups , we did unsupervised class discovery by nmf - metagene and k - means clustering , testing all combinations of 310 metagenes and clusters for reproducibility using bootstrapped resampling methods ( 250 iterations ) as described previously.7 this analysis identified metagenes ( a single score that reflects the methylation status of several cpg loci ) representing the main biological effects present in the genome - wide dataset . 
we assessed cluster stability using the cophenetic index , a shorthand measure of the robustness of sample clustering as determined by consensus non - negative matrix factorisation ( appendix p 3 )  . 
we visualised clusters with t - sne.22 we assigned samples classified with less than 80% confidence ( by ( nc ; resampling procedures ) appendix pp 23 )  . as non - classifiable we projected metagenes derived from our discovery cohort onto the validation cohort . 
additionally , we combined the discovery and validation cohorts to do equivalent consensus clustering . we assessed established medulloblastoma clinical , pathological , and molecular features as described previously.7 briefly , we defined histopathological variants according to the who 2016 guidelines.13 we assigned metastatic status ( m + ) based on changs criteria ( appendix p 3 )  . 
tumours were designated as r + if their residuum after surgical excision exceeded 15 c pathology was centrally reviewed by three experienced neuropathologists for 380 ( 89% ) of 428 samples , and clinical data were collated from contributing centres and reviewed centrally ( appendix p 3 )  . 
we identified gfi1 mutations from rna - seq data ( appendix p 4 )  . mbshh mutation data were obtained from a previous study.26 although 450k methylation data for mbshh subgroup assignment were not available for this sample cohort , the tightly defined age cutoff that we defined between the molecularly determined mbshh - infant and mbshh - child subgroups enabled us to infer subgroups for this sequencing cohort ( appendix p 4 ) .26 we tested recurrent mbshh mutations ( tp53 , sufu , ptch1 , smo , and tert ) and gene amplifications ( mycn and gli2 ) identified by whole genome sequencing , for association with the age - defined mbshh - child or mbshh - infant subgroups using fishers exact test ( appendix p 4 )  . statistical analysis we did survival analyses ( overall survival and progressionfree survival ) on samples from patients aged 316 years within our discovery cohort , who received maximal surgical resection and craniospinal irradiation with curative intent . 
overall survival was defined as the time from date of surgery to death or date of last follow - up and progression - free survival as the time from date of surgery to first event ( progression or relapse ) or date of last follow - up . 
patients with follow - up time that exceeded 10 years were right - censored at 10 years . ( n = 55 ) , the tightly defined age cutoff between the molecularly determined mbshh - infant and mbshh - child subgroups enabled us to assess an expanded survival cohort of mbshh - child including additional samples with disease insufficient dna for methylation array analysis , classified as mbshh - child on the basis of their age ( appendix p 4 )  . 
in this group , we assessed the prognostic potential of currently used clinical and molecular risk markers ( m + disease , r + disease , lca pathology , sex , mycn amplification , tert mutation , and tp53 mutation [ appendix pp 45 ] )  . 
as a consequence , we report only overall survival in this group . in this group of patients we created univariate and cross - validated multivariate cox models based on subgroups , established risk factors , and cytogenetic changes . 
prognostic markers in the multivariate analysis were identified by performing 100 rounds of 10 - fold cross - validation , evaluating the performance of markers by measuring area under the curve ( auc ) at 5 years for progression - free survival in the left out fold , and calculating the overall mean auc over all rounds ( appendix p 5 )  . 
 960 vol 18 july 2017 articles consensus , 1 whereas the second ( six metagenes , seven clusters ) revealed further clusters within the established subgroups ( figure 1a , appendix pp 1011 )  . discovery cohort ( n = 428 ) validation cohort ( n = 276 ) mbshh - child survival cohort ( n = 55 ) mbgrp3 / 4 survival cohort ( n = 175 ) 174 ( 63% ) 102 ( 37% ) 17 : 1 32 ( 58% ) 23 ( 42% ) 14 : 1 124 ( 71% ) 51 ( 29% ) 24 : 1 median ( range ) 634 ( 0241597 ) 750 ( 00180 ) 1086 ( 351554 ) 733 ( 341597 ) 30 ( 11% ) 244 ( 89% ) 55 ( 100% ) 175 ( 100% ) changes , mbgrp3 membership , because mbgrp3 and mbgrp4 shared a metagene ( v1 ) , which defined a low - risk outcome and implied shared biology , we considered mbgrp3 / 4 as a single entity , and mbgrp3 and mbgrp4 separately for creation of survival models . 
ixdition to currently understood clinical and molecular risk markers in these groups ( m + disease , r + disease , lca pathology , gender , myc / mycn amplification , and i17q [ isochromosome 17q ] ) , we additionally tested for recurrent cytogenetic and membership of the high - risk methylomic group composed of members from both mbgrp3 and mbgrp4 , defined by metagene v1 ( appendix pp 56 )  . 
we categorised identified independent prognostic markers into risk - stratification schemes ( favourable - risk , > 90% survival ; standard - risk , > 7590% survival ; high - risk , 4075% survival ; very highrisk , < 40% survival ) and survival - dependent roc analysis of progression - free survival at 5 years , to assess performance27 by comparison with previously reported classification schemes ( appendix pp 56 ) .16 , 28 we constructed kaplan - meier curves and compared patient groups with log - rank tests . 
we implemented array processing , normalisation , quality - control checks , and copy - number estimation , relative to a panel of 18 normal cerebella with the r packages minfi29 and conumee ( appendix p 2 )  . the significance threshold was set at p < 005 for all statistical tests in this study , unless otherwise stated . 
the corresponding author had full access to all of the data and had the final responsibility to submit for publication . and molecular results clinicopathological diagnostic characteristics of 428 patients younger than 16 years who had primary childhood medulloblastoma ( discovery cohort ) are shown in table 1 . 
 wnt = wnt / wingless . table 1 : demographics and clinicopathological characteristics of all cohorts loss split into age - dependent mbwnt tumours formed a single subgroup ( n = 33 ) characterised by ctnnb1 mutations , chromosome 6 , and an expected favourable prognosis ( 5 - year overall survival : 93% [ 95% ci 82100 ] ; figure 1b )  . 
 mbshh was subgroups corresponding to infant ( < 43 years ; mbshh - infant ; n = 65 ) and childhood patients ( 43 years ; mbshh - child ; n = 38 ) by the respective absence or presence of metagene v4 . 
both have intermediate prognoses ( 5 - year overall survival mbshh - child : 58% [ 95% ci 4182 ] ; mbshh - infant : 62% [ 5077 ] ; figure 1b )  . 
the subdivision of mbgrp3 and mbgrp4 distinguishes patients with a superior stratification ( 5 - year overall survival auc 0649 [ mbgrp3 / 4 combined with low - risk or high - risk subdivision ] ) compared with the current consensus mbgrp3 and mbgrp4 subgroups ( auc 0610 )  . 
moreover , in the patients aged 316 years at diagnosis and receiving craniospinal irradiation , the high - risk or low - risk subdivision of mbgrp3 / 4 stratifies this group into standard ( mbgrp3 - lr 81% [ 95% ci 60100% ] ; mbgrp4 - lr 81% [ 7193% ] ) and high - risk ( mbgrp3 - hr 35% [ 2355% ] ; mbgrp4 - hr 47% [ 3466% ] ) 5 - year progressionfree survival outcomes , by contrast with the current consensus mbgrp3 / 4 intermediate outcomes ( figure 1c , 1d )  . designations , which show clinicopathological and biological features were nonrandomly distributed in all seven subgroups ( figure 1a , appendix pp 1215 )  . 
patients in the mbshh - infant subgroup had significantly enriched desmoplastic or nodular pathology compared with all other subgroups ( p < 00001 ) , and tp53 mutation ( p < 00001 ) and mycn amplifications ( p < 00001 ) were significantly more frequent in mbshh - child than in all other subgroups . 
patients in the mbgrp3 - hr frequently had lca subgroup significantly more pathology ( p < 00001 ) and myc amplification ( p < 00001 ) , than all other subgroups . 
although patients in the mbgrp3 - hr and mbgrp4 - hr subgroups had similar 10 - year overall survival ( 22% [ 95% ci 1046 ] vs 36% [ 2259 ] ; figure 1b ) , patients in the mbgrp4 - hr subgroup died later of their disease ( ten [ 36% ] of 28 deaths in the mbgrp4 - hr subgroup occurred more than 5 years after diagnosis ) than did those in the mbgrp3 - hr subgroup ( 33 [ 92% ] of 36 deaths occurred within 5 years of diagnosis ; appendix p 26 )  . validation by projection of six metagenes onto an independent cohort8 of 276 patients ( table 1 ) confirmed their existence ( appendix pp 1011 )  . 
moreover , reapplying consensus clustering the combined cohort of 704 patients confirmed a seven subgroup model as optimal , giving 100% concordance to the classifications derived separately from our discovery cohort ( appendix pp 1011 )  . age distributions differed between the two mbshh subgroups ; age distributions are log - normally distributed and intersect at 43 years ( figure 2a )  . 
the two peak incidences of age at diagnosis in infants and in older children for mbshh disease , 26 when observed as a whole , are resolved by their classification into distinct mbshh - infant and mbshh - child subgroups ( appendix pp 1213 )  . 
lca pathology ( p = 000050 ) , mycn amplification ( p < 00001 ) , and mutations of tp53 ( p < 00001 ) and tert ( p = 00015 ) were all significantly enriched in the mbshh - child subgroup compared with the mbshh - infant subgroup ; whereas gender , m + disease status , and r + disease status were not significantly different between groups ( figure 2b ; appendix pp 1213 )  . 
mutational data from an independent mbshh cohort26 showed that sufu mutation was significantly associated with mbshh - infant , whereas ptch1 mutations were observed in both mbshh subgroups ( figure 2c )  . 
residuals from tests indicate where subgroup - enrichment has occurred ( darker shades of grey indicate stronger relationships ) , p values are from tests of enrichment ; scale bar for residuals ( 2 to 2 ) is shown . 
methylation - derived metagene levels ( v1v6 ) , which define subgroup membership , are also shown ( red indicates high metagene levels , blue indicates low levels )  . 
 ( c ) progression - free survival of patients in the consensus four subgroups of medulloblastoma in discovery cohort patients receiving craniospinal irradiation and aged 316 years at diagnosis ( n = 250 )  . 
 ( d ) progression - free survival of patients in the seven identified subgroups of medulloblastoma in patients receiving craniospinal irradiation and aged 316 years at diagnosis ( n = 239 )  . 
discrepancy in the numbers of patients in ( c ) and ( d ) is due to consensus clustering ; certain samples could not be confidently classified for the seven subgroup model or the four subgroup model , and were omitted from the figures . 
r + = residual disease . ( predominantly hypermethylation ) , at both individual cpg loci and at the gene level ( figure 2b ; appendix pp 1213 ) , frequently involving developmental genes ( 79 [ 14% ] of 584 genes with gene ontology term embryonic morphogenesis had aberrant hypermethylation )  . 
residuals from tests indicate where subgroup - enrichment has occurred ( darker shades of grey indicate stronger relationships ) ; scale bar for residuals ( 4 to 4 ) is shown . 
 patients in the mbgrp3 - lr and mbgrp3 - hr subgroups were younger at diagnosis than those in the mbgrp4 - lr and mbgrp4 - hr subgroups ( appendix pp 1415 )  . 
residuals from tests indicate where subgroup - enrichment has occurred ( darker shades of grey indicate stronger relationships ) ; scale bar for residuals ( 6 to 6 ) is shown . 
mbgrp3 - hr tumours were strongly associated with lca pathology ( 20 [ 35% ] of 57 ) and gfi1 mutations ( nine [ 29% ] of 31 ; figure 3a , appendix pp 1415 )  . 
mbgrp3 - hr was characterised by the greatest number of significantly differentially methylated cpgs compared with other subgroups , commonly hypomethylated cpg loci ( figure 3b ; appendix pp 1415 )  . 
notably , the low - risk subgroups were defined primarily by hypermethylation with respect to normal cerebellum , whereas the high - risk univariate ( n = 55 ) cross - validated multivariate ( n = 42 ) hr ( 95% ci ) p value hr ( 95% ci ) p value mycn amplification vs no amplification 447 ( 165121 ) 00032 283 ( 087922 ) 0084 m + vs m disease 569 ( 201160 ) 00011 459 ( 128164 ) 0019 tp53 mutation vs no mutation 347 ( 129930 ) 0014 344 ( 115102 ) 0027 lca pathology vs non - lca pathology 288 ( 115724 ) 0025 tert wild - type vs tert mutation r + vs r disease male vs female 221 ( 078625 ) 013 345 ( 130919 ) 0013 113 ( 045282 ) 079 p values are from cox proportional hazards analyses . 
r = no residual disease ( gross total resection )  . table 2 : identification of prognostic survival markers in mbshh - child cohort univariate ( n = 175 ) cross - validated multivariate ( n = 133 ) hr ( 95% ci ) p value hr ( 95% ci ) p value 175 373 ( 194718 ) < 00001 321 ( 159651 ) 00012 high - risk methylation group vs low - risk methylation group myc amplification vs no amplification 173 294 ( 106813 ) 184 ( 501677 ) < 00001 loss of chromosome 13 vs no loss 158 010 ( 001074 ) 006 ( 001049 ) 00090 mbgrp3 vs mbgrp4 m + vs m disease i17q vs no i17q male vs female mycn amplification vs no amplification 175 204 ( 123340 ) 177 ( 103305 ) 158 171 ( 099295 ) 175 156 ( 086284 ) 173 072 ( 023229 ) lca pathology vs non - lca pathology 108 ( 049239 ) r + vs r disease 122 ( 072209 ) 0038 0024 0006 0039 0056 0144 0576 0848 0464 identification of prognostic survival markers in combined childhood non - mbshh and non - mbwnt survival cohort ( aged 30160 years , receiving craniospinal irradiation , with survival information )  . 
r = no residual disease ( gross total resection )  . table 3 : identification of prognostic survival markers in mbgrp3 and mbgrp4 cohorts subgroups were defined by hypomethylation ( figure 3b ; appendix pp 1415 )  . 
 these distinguishing cytogenetic features were validated in an independent cohort ( appendix pp 1415 )  . survival we did survival analyses in an mbshh - child cohort that included 31 additional shh cases unsuitable for 450k array analysis and classified as mbshh - child on the basis of age ( appendix pp 45 )  . 
tp53 mutation was significantly associated with mycn amplification ( p = 0022 ) and lca pathology ( p = 00033 ) , mycn amplification was associated with lca pathology ( p < 00001 ) , and lca pathology and mycn amplification were never observed with tert mutations ( p = 000079 for lca and p = 00090 for mycn amplification )  . 
there was no significant association between metastatic ( m + ) disease and tp53 mutation ( p = 1 ) , mycn amplification ( p = 0.15 ) , or lca pathology ( p = 067 ) , or an association between subtotally resected ( r + ) disease and tp53 mutation ( p = 1 ) , mycn amplification ( p = 1 ) or lca pathology ( p = 041 )  . 
 univariate survival analysis of clinicobiological features ( including risk features established in disease - wide studies16 ) in this cohort showed significantly shorter progression - free associated with mycn amplification tp53 mutation , lca pathology , m + disease , and r + disease , but no associations with tert mutation status or sex ( table 2 ; appendix pp 1819 )  . 
multivariate cox modelling , showed that mycn amplification , tp53 mutation , and m + disease are independent risk factors for progression - free survival ( table 2 )  . 
the disease - wide risk - stratification scheme currently in use for the hit - siop - pnet5 - mb clinical trial , 16 which deems mycn amplification , lca pathology , m + disease , and r + disease as high - risk factors , outperformed the mbshh - child subgroup stratification in auc this analysis hit - siop - pnet5 - mb stratification scheme as the basis of a combined risk - stratification model for mbshh - child ( appendix pp 1617 ) , classifying patients with any one of these risk factors as very high risk . 
additionally , in multivariate analysis , myc amplification was identified as an independently prognostic high - risk factor , and chromosome 13 loss was associated with an improved outcome ( table 3 )  . 966 vol 18 july 2017 articles a favourable standard high very high time since diagnosis ( years ) false positive mbgrp3 / grp4 mbgrp3 and mbgrp4 cytogenetic current ( pnet5 ) 0678 0656 0639 0538 number at risk ( number censored ) favourable standard high very high 16 ( 0 ) 50 ( 0 ) 82 ( 0 ) 5 ( 0 ) 14 ( 2 ) 34 ( 11 ) 41 ( 19 ) 0 ( 2 ) 10 ( 5 ) 24 ( 18 ) 26 ( 23 ) 7 ( 8 ) 16 ( 26 ) 15 ( 29 ) 6 ( 9 ) 8 ( 34 ) 7 ( 36 ) 2 ( 13 ) 5 ( 37 ) 3 ( 40 ) favourable vs standard ; hr 032 ( 95% ci 004256 ) , p = 026 high vs standard ; hr 348 ( 95% ci 162749 ) , p = 000032 very high vs standard ; hr 577 ( 95% ci 547609 ) , p < 00001 figure 4 : novel risk stratification scheme for mbgrp3 and mbgrp4 medulloblastoma ( a ) progression - free survival plots for identified risk subgroups ( n = 156 ) defined in table 3 and the appendix ( p 20 )  . 
 ( b ) time - dependent roc curves at 5 years are shown for this novel risk stratification alongside a published cytogenetic stratification scheme28 ( mbgrp4 with chromosome 11 loss or chromosome 17 gain , low risk ; mbgrp4 with m disease , standard risk ; mbgrp4 with m + disease , high risk ; mbgrp3 with myc amplification , i17q , or m + disease , high risk ; mbgrp3 without myc amplification , i17q , or m + disease , standard risk ) , and the pnet5 risk stratification ( patients positive for one or more of lca pathology , m + disease , r + disease , myc ( n ) amplification are high risk ; patients absent for all high - risk features , standard risk ) , as well as the stratification derived from considering mbgrp3 and mbgrp4 as separate entities ( appendix p 22 )  . 
roc = receiver operating characteristic . a stratification model was developed that divided mbgrp3 / 4 into different risk groups for 5 - year progressionfree survival : favourable risk ( chromosome 13 loss and no myc amplification ; 16 [ 10% ] of 153 patients ; 92% [ 95% ci 79100 ] ) ; standard risk ( mbgrp4 - lr or mbgrp3 - lr with no myc amplification ; 50 [ 33% ] patients ; 81% [ 7094 ] ) ; high risk ( mbgrp4 - hr or mbgrp3 - hr with no myc amplification ; 82 [ 54% ] patients ; 42% [ 3156 ] ) ; and very high risk ( mbgrp3 with myc amplification ; five [ 3% ] patients ; 0% ; figure 4a ; appendix pp 2021 )  . 
156 patients had information for chromosome 13 loss and myc amplification , of which three were classed as unassignable because they were mbgrp4 with myc amplification ( appendix pp 2021 )  . 
this stratification riskscheme outperformed stratification models ( figure 4b )  . current for comparison , we developed equivalent separate survival stratification schemes for mbgrp3 and mbgrp4 ( appendix pp 2223 )  . 
risk factors identified were broadly consistent with the factors identified in the combined scheme , although the combined scheme was a better predictor of progression - free survival than when mbgrp3 and mbgrp4 were considered separately ( figure 4b )  . 
taking mbgrp4 patients in isolation , in univariate analysis , a designation of mbgrp4 - hr , chromosome 7q status , m + disease , and male sex were associated with poor progression - free survival , whereas mycn amplification , r + disease , and lca pathology were not ( appendix pp 2223 )  . 
a 5 - year variate analysis progression - free survival model incorporating chromosome 7q gain and m + disease defined standard - risk ( 35 [ 32% ] of 110 patients ; 87% [ 95% ci 76100 ] ) and highrisk groups ( 75 [ 68 ] ; 49% [ 3766 ] ) , and outperformed other published models by auc analysis ( appendix pp 2223 )  . taking patients with mbgrp3 isolation , myc amplification was the only risk factor significantly associated with progression - free survival in multivariate analysis , and outcomes were poor for these very high - risk patients ( appendix pp 2223 )  . 
patients in the mbgrp3 with non - myc amplified tumours were at high risk , with progression - free survival similar to that for the mbgrp4 - hr subgroup ( 51 [ 91% ] of 56 patients ; 46% [ 95% ci 3364 ] for mbgrp3 with non - myc amplified tumours vs 41% [ 2860 ] for mbgrp4 - hr )  . 
 * comparisons of cytogenetic , gene expression , and dna methylation changes are made with respect to their counterpart subgroup , except for mbwnt cases , which were compared with normal cerebella if data were available . 
for probe - level comparisons , kyoto encyclopedia of genes and genomes pathway enrichment of demethylated loci was investigated , after correcting for multiple probes mapping to the same gene ( data summarised in appendix pp 2731 )  . 
lca = large - cell anaplastic . gfi1 i17q 16q myc amplication pvt1 , trap1 , nmral1 , cntln ribosome biogenesis genes pi3k - akt signalling pathway vs mbgrp3 - lr , cb galnt9 , mir662 significant seven clinically the clinicopathological and molecular features of the subgroups are new summarised in figure 5 . 
patients are stratified into four clinical risk groups for 5 - year progression - free survival : favourable risk ( comprising mbwnt , mbshh - child with no high - risk features , and non - myc amplified mbgrp3 / grp4 with chromosome 13 loss ; 54 [ 25% ] of 215 patients ; 91% [ 95% ci 82100 ] ) ; standard risk ( comprising non - myc amplified mbgrp3 - lr / grp4 - lr subgroups ; 50 [ 23% ] patients ; 81% [ 7094 ] ) ; high - risk ( comprising non - myc amplified mbgrp3 - hr / grp4 - hr subgroups ; 82 [ 38% ] patients ; 42% [ 3156 ] ) ; and very high - risk ( comprising mbshh - child with high - risk features and myc - amplified mbgrp3 ; 29 [ 13% ] patients ; 28% [ 1456 ] ; figure 6b )  . 
the auc from our proposed childhood medulloblastoma outperforms current and proposed cytogenetic risk stratifications ( figure 6c ) .28 we note that stratification of to create m + disease status is a strong risk factor for poor progression - free survival in mbgrp4 . 
incorporation of m + disease status into mbgrp4 - lr and non - myc amplified mbgrp3 - lr survival modelling does not affect model performance , but potentially allows redistribution of larger favourable standard - risk patients ( 90 [ 41% ] of 218 patients ) and high - risk groups ( 99 [ 45% ] of 218 patients ; figure 6a , c ; appendix pp 2425 ) , which could be considered as an alternative stratification scheme . 
mbgrp3 / 4 : mbgrp3 and mbgrp4 considered as a single entity ; mbgrp3 / 4 plus m + : mbgrp3 and mbgrp4 considered as a single entity with mbgrp4 - lr and non - myc amplified mbgrp3 - lr further stratified by m + disease status ; mbgrp3 and mbgrp4 : mbgrp3 and mbgrp4 stratified separately ; cytogenetic : cytogenetically defined scheme ; 28 pnet5 : scheme employed by hit - siop - pnet5 - mb clinical trial . 
notably , these subgroups were not identifiable in a previously published dataset , which analysis , and are included fewer samples and , specifically , fewer infant patients.8 our seven subgroups reveal a biological overlap between mbgrp3 and mbgrp4 . 
they share a biological signature , defined by a common metagene , indicating a clinicobiological overlap , which might suggest a common origin . these primary subgroups may be further subdivided by the presence or absence of secondary molecular characteristics , many of which , in turn , have subgroupspecific clinical and prognostic significance ( eg , myc vol 18 july 2017 articles in mbgrp3 or tp53 mutation , mycn amplification amplification , lca pathology , m + disease , and r + disease in mbshh - child )  . 
some of these secondary features have been described and assigned clinical significance in previous studies ; in this article , their association with specific novel subgroups ( eg , chromosome 11 loss and chromosome 17 gain in mbgrp4 - lr 28 ) has revealed the underlying biological basis of these subgroup - specific biomarkers . 
moreover , re - evaluation of currently used high - risk factors derived from cohort - wide studies that did not consider subgroup shows that their importance is either low ( eg , lca pathology , m + disease , or r + disease in mbgrp3 ; mycn in mbgrp4 ) or high ( mycn amplification , lca pathology , tp53 mutation , and m + disease in mbshh - child ; myc in mbgrp3 ; m + in mbgrp4 ) when considered in the context of our new subgroups . 
 finally , the biological definition of mbshh - infant ( < 43 years ) is at odds with current clinical definitions of infant disease ( < 3 years ) and this should prompt consideration in the future as to whether infant treatment protocols are appropriate for mbshh - infant patients older than 3 years.16 survival modelling in children younger than 3 years is qualitatively different from analysis in those over 3 years of age , because of the heterogeneity of treatment of infant disease . 
the overall survival at 5 years that we observed in mbshh - infant disease ( 62% , 95% ci 5077 ) is lower than previously reported in an international meta - analysis of the mbshh subgroup in age - defined infants ( < 4 years at diagnosis ; 77% ) , 30 but these patients were not molecularly defined and , as such , are not directly comparable . our survival analysis focused on the 316 - year - old clinical group who received current conventional therapies : surgical resection followed by adjuvant radiotherapy with or without chemotherapy at diagnosis with curative intent . 
combined risk - modelling across all patients in the non - mbwnt or non - mbshh subgroups identified myc amplification , high - risk methylation subgroup membership , and loss of chromosome 13 as independent risk factors . 
survival models incorporating these factors outperformed the clinical risk - stratification used in current clinical trials ( hit - siop - pnet5 - mb16 ) and stratification schemes.28 subgroup - dependent cytogenetic we have defined a risk - stratification of childhood medulloblastoma that allows patients to be assigned into four overarching risk groups . 
very high - risk patients , typically refractory to conventional therapies ( eg , amplified mycn , mutated tp53 , lca pathology , and m + disease in mbshh and amplified myc in mbgrp3 ) should be prioritised for alternative upfront treatment strategies . 
the priority for high - risk patients , comprising the novel mbgrp4 - hr and patients with non - amplified myc in the mbgrp3 - hr subgroup , and a standard - risk group , comprising all other patients , should be optimisation of current therapies and the application of novel , biologically targeted agents . cohorts , who retrospective patient treatments . 
notwithstanding we note the limitations of developing survival models received heterogeneous that models were developed using patients aged 316 years , who all received maximal surgical resection and craniospinal irradiation with curative intent , caution should be applied to their clinical implementation . 
a small number of samples ( < 5 samples ) from this study were used to assist with four - subgroup classification the creation of consensus.5 similarly , our own publication that described four methylation - dependent subgroups of medulloblastoma7 contained 87 samples that overlapped with this study , although the previously published study contained fewer samples ( discovery cohort size of 100 and validation cohort size of 130 patients ) and dna methylation profiling was at much lower resolution ( 1505 vs > 400 000 cpg loci )  . the the existence of novel primary medulloblastoma subgroups , coupled with the characterisation of secondary prognostic features within each group , represents a significant advance in our understanding of medulloblastoma biology and its application in clinical management and future trials design . 
we provide clear evidence of the shared biology between mbgrp3 and mbgrp4 , which affects clinical behaviour and has significant implications for understanding disease biology , developmental origins , and experimental modelling . 
 these investigations constitute a blueprint for a new consensus in medulloblastoma molecular subclassification with important implications for future molecular diagnostics and clinical management . contributors ecs , dw , sb , and scc designed the study and wrote the manuscript . 
all authors contributed to and approved the final manuscript . declaration of interests we declare no competing interests . 970 vol 18 july 2017 articles acknowledgments this study was funded by cancer research uk ( c8464 / a13457 ) , the tom grahame trust , star for harris , action medical research , sparks , the jgw patterson foundation , and the instinct network ( co - funded by the brain tumour charity , great ormond street childrens charity , and children with cancer uk )  . 
based on the sample size calculation , we planned to analyse overall survival when 190 deaths occurred ; this target has now been reached , after a median 10 years of follow - up . methods rt01 was a phase 3 , open - label , international , randomised controlled trial enrolling men with histologically con rmed t1bt3a , n0 , m0 prostate cancer with prostate speci c antigen of less than 50 ng / ml . 
patients were randomly assigned centrally in a 1 : 1 ratio , using a computer - based minimisation algorithm stratifying by risk of seminal vesicle invasion and centre to either the control group ( 64 gy in 32 fractions , the standard dose at the time the trial was designed ) or the escalated - dose group ( 74 gy in 37 fractions )  . 
this trial is registered , number isrctn47772397 . findings between jan 7 , 1998 , and dec 20 , 2001 , 862 men were registered and 843 subsequently randomly assigned : 422 to the escalated - dose group and 421 to the control group . 
biochemical progression or progressive disease occurred in 391 patients ( 221 [ 57% ] in the control group and 170 [ 43% ] in the escalated - dose group )  . 
at 10 years , biochemical progression - free survival was 43% ( 95% ci 3848 ) in the control group and 55% ( 5061 ) in the escalated - dose group ( hr 069 , 95% ci 056084 ; p = 00003 )  . interpretation at a median follow - up of 10 years , escalated - dose conformal radiotherapy with neoadjuvant androgen deprivation therapy showed an advantage in biochemical progression - free survival , but this advantage did not translate into an improvement in overall survival . 
open access article distributed under the terms of cc by . introduction external beam radiotherapy is one of the standard curative options for men with localised prostate cancer and is particularly appropriate for men with intermediate - risk or high - risk disease.1 , 2 improved radiotherapy techniques , such as conformal radiotherapy , allow high treatment doses to be given safely3 , 4 and several phase 3 randomised controlled trials of dose escalation have reported improved biochemical progression - free survival.510 the medical research council ( mrc ) rt01 trial is the largest of these trials to have reported results , and since its initial report of results dose - escalated conformal radiotherapy has been the standard of care in the uk since 2008.1 the trial mandated the use of short - course neoadjuvant androgen deprivation therapy ( adt ) ; neoadjuvant adt has since been shown to improve overall and cancer - speci c survival in patients with advanced localised disease.1114 overall the aim of the rt01 trial was to assess the e ect of survival , biochemical dose - escalation progression - free survival , and toxicity , by comparing doses of 74 gy and 64 gy delivered by use of conformal radiotherapy techniques . 
64 gy in 32 fractions was chosen as the radiotherapy schedule for the control group in our randomised trial , because that was the standard 464 vol 15 april 2014 articles 862 assessed for eligibility 19 excluded 8 intercurrent illness 6 patients preference 3 hospital error 2 disease progression 843 randomised 4 received more than planned dose 421 patients assigned to control group ( 64 gy in 32 fractions ) 2 had less than planned dose 4 did not receive radiotherapy 1 dose information not available 410 received planned dose 422 patients assigned to escalated - dose group ( 74 gy in 37 fractions ) 14 received less than planned dose 7 did not receive radiotherapy 401 received planned dose 421 patients analysed 422 patients analysed figure 1 : trial pro le age ( years ) median ( range ) t stage t1b / t1c t2a / t2b t3a / t3b not known gleason score * 6 or lower 8 or higher not known median ( iqr ) mean ( sd ) moderate nccn risk group * high intermediate unobtainable control group ( n = 421 ) escalated - dose group ( n = 422 ) 67 ( 4680 ) 67 ( 4880 ) 106 ( 26% ) 236 ( 57% ) 71 ( 17% ) 103 ( 25% ) 239 ( 57% ) 76 ( 18% ) 261 ( 62% ) 105 ( 25% ) 52 ( 12% ) 249 ( 59% ) 117 ( 28% ) 54 ( 13% ) 128 ( 84200 ) 128 ( 78202 ) 156 ( 100 ) 152 ( 96 ) 137 ( 33% ) 284 ( 67% ) 138 ( 33% ) 284 ( 67% ) 79 ( 19% ) 159 ( 38% ) 178 ( 43% ) 81 ( 19% ) 152 ( 36% ) 184 ( 44% ) prehormone psa ( ng / ml ) risk group for involvement of seminal vesicles data are n ( % ) unless otherwise speci ed . 
 * if gleason score was missing , who di erentiation was used in the following way : well , moderate , or poor di erentiation is classi ed as gleason score of 6 , 7 , or 8 , respectively . 
we initially reported ndings of the trial with a 5 - year median followup and now update these results with a median follow - up of 10 years , because the target number of deaths for analysis of overall survival has been reached . 
treatmentrelated side - e ects have been reported previously.7 , 15 , 16 methods study design and participants rt01 was a phase 3 , open - label , international , randomised controlled trial comparing dose - escalated conformal radiotherapy with control - dose conformal radiotherapy . 
it was preceded by a pilot study at the royal marsden hospital.5 patients were registered , initiated on neoadjuvant adt , and then randomly assigned to receive either control or escalated radiotherapy using conformal radiotherapy techniques . 
men 18 years or older with histologically con rmed t1bt3a , n0 , m0 prostate cancer and prostate - speci c antigen ( psa ) of less than 50 ng per ml , with no contraindications for radical radiotherapy were included in the trial . 
this study was done in compliance with the declaration of helsinki , and the protocol was approved by the appropriate research ethics committees . randomisation and masking consenting patients were randomly assigned in a 1 : 1 ratio to control or escalated - dose conformal radiotherapy centrally at the mrc clinical trials unit ( ctu ) using a computer - based minimisation algorithm , stratifying for risk of seminal vesicle invasion and centre . 
the random allocation list was created by the mrc ctu . injections of procedures as reported previously , androgen deprivation was achieved using luteinising - hormonereleasing hormone agonists every 4 weeks and was accompanied by antiandrogen therapy to prevent are events.7 neoadjuvant adt was given for 36 months before commencement of conformal radiotherapy and continued until the end of conformal radiotherapy . men were randomised to receive either a control - dose schedule ( 64 gy in 32 fractions ; control group ) schedule , or an escalated - dose schedule ( 74 gy in 37 fractions )  . 
all radiotherapy treatments used three - dimensional conformal techniques as previously described.7 , 11 , 17 the radiotherapy phase 1 target volume included the prostate and all or part of the seminal vesicles , depending on the vol 15 april 2014 articles risk of seminal vesicle invasion.18 all patients were treated to a dose of 64 gy in 32 fractions over 65 weeks using a standard threeeld plan ( anterior eld and left and right lateral or posterior oblique elds ) with a 10 cm marg patients randomised to the escalated - dose group had a phase 2 boost to the prostate alone using a sixeld technique ( left and right anterior oblique , left and right posterior oblique , and left and right lateral elds ) with no margin added . 
veri cation was with daily and then weekly port lms and images . men were followed - up throughout radiotherapy at 6 monthly intervals up to 2 years , and annually thereafter . 
 acute and late treatment - related side - e ects were collected using radiation therapy oncology group19 and late e ects of normal tissues - subjective objective management analytic scales20 and timed from the start of radiotherapy . 
the design , objectives , eligibility criteria for patients , treatment methods , and statistical considerations are detailed elsewhere.7 , 17 outcomes the coprimary outcome measures were overall survival and biochemical progression - free survival . 
overall 020 015 010 005 005 010 015 020 020 015 010 005 005 010 015 020 control group by kaplan - meier control group by exible parametric model escalated - dose group by kaplan - meier escalated - dose group by exible parametric model number at risk control group escalated - dose group 95% ci overall survival by exible parametric model control group by kaplan - meier control group by exible parametric model escalated - dose group by kaplan - meier escalated - dose group by exible parametric model time from randomisation ( years ) number at risk control group escalated - dose group 95% ci biochemical progression - free survival by exible parametric model time from randomisation ( years ) figure 2 : primary analysis of overall survival and biochemical progression - free survival ( a ) overall survival , predicted from kaplan - meier function and exible parametric model . 
 ( d ) absolute di erence in biochemical progression - free survival , from exible parametric model . 466 vol 15 april 2014 articles hr ( 95% ci ) 096 ( 054170 ) 101 ( 076134 ) 077 ( 032187 ) 113 ( 073174 ) 095 ( 068134 ) 080 ( 054118 ) 066 ( 052083 ) 061 ( 034109 ) 084 ( 059119 ) 060 ( 046079 ) with cox models , adjusted for seminal vesicle risk group.18 we applied the restricted mean survival time method to overall survival and biochemical progressionfree survival , as an additional method of estimating di erence between the treatments , with the restriction time being 10 years . 
 all comparisons are expressed relative to the control group ; therefore , an hr of less than 10 indicates a decreased risk in the escalated - dose group . we did a competing - risk analysis for prostate cancer death because the number of deaths from causes other than prostate cancer exceeded the prespeci ed level of 20% . 
for this analysis , time to prostate cancer death is presented with cumulative incidence function rather than survival function ; sub - hr is presented with 95% ci and p value . 
cause - speci c hrs are presented for both prostate cancer and non - prostate - cancer deaths . we did pre - planned , exploratory subgroup analyses to examine consistency of e ect across seminal vesicle risk group ( low vs moderate ) and national comprehensive cancer network ( nccn ) risk group ( low vs intermediate vs high ) .2 this analysis uses tests for heterogeneity of interaction or trend when appropriate , and examines overall survival and biochemical progression - free survival . 
this trial is registered , number isrctn47772397 . low risk intermediate risk test for heterogeneity : p = 089 low risk intermediate risk high risk test for heterogeneity : p = 070 low - risk intermediate - risk test for heterogeneity : p = 042 low risk intermediate risk high risk test for heterogeneity : p = 032 survival was de ned as time from randomisation to death from any cause or censoring at date of last contact . 
 biochemical progression - free survival was de ned as time from randomisation to biochemical failure , death from prostate cancer , or development of local , nodal , or metastatic disease , whichever occurred rst . additional outcome measures were biochemical failure ( an increase in psa concentration to 50% above nadir and above 2 ng / ml 6 months or more after the start of radiotherapy ) ; progression - free survival ( excluding psa failure ) ; initiation of long - term salvage adt ; development of metastases ; death from prostate cancer ; and metastasesfree survival ( time to development of any metastases or death from prostate cancer )  . 
cause of death was reviewed by pairs of clinicians from a panel of ve individuals who were masked to treatment allocation . the original protocol speci ed ve primary outcome measures survival ( biochemical progression - free [ named as biochemical control in the protocol , local progression , metastases free freedom from survival , overall survival , and late toxicity ) ; with sample size calculations included for local control and overall survival . 
during the course of the trial , the trial management group , independent data monitoring committee , and trial steering committee agreed from external evidence that biochemical progression - free survival was a more important outcome measure than local control . 
all outcome measures are reported . statistical analysis we estimated that inclusion of about 800 patients would meet the targets for the numbers of patients in the subgroups at low - risk and intermediate - risk of seminal vesicle involvement.17 we assumed that survival at 5 years would be 50% in patients in the control group , and the trial aimed to achieve a 15% increase in survival at 5 years in the escalated - dose group . 
with 90% power and a 5% two - sided signi cance level , we established that about 194 deaths were needed for this analysis of overall survival . we did all analyses on an intention - to - treat basis , with patients analysed according to allocated treatment group . 
 all analysed outcome measures are presented in this report . we used standard survival analysis methods to investigate time from randomisation to the rst reported event for each outcome measure , except for time to death from prostate cancer . 
hazard ratios ( hr ) were estimated favours escalated - dose favours control figure 3 : subgroup analyses of overall survival and biochemical progression - free survival ( a ) overall survival and risk of seminal vesicle involvement . 
 results between jan 7 , 1998 , and dec 20 , 2001 , 862 men were registered and 843 subsequently randomised : 422 to the escalated - dose group and 421 to the control group ( gure 1 )  . table 1 shows characteristics of the patients at baseline ; the groups were balanced . 
209 ( 25% ) of 831 patients had t1 stage cancers , 475 ( 57% ) had t2 stage , and 147 ( 18% ) had t3 cancers ; t stage was unavailable for 12 patients . 
 analyses of biopsy specimens were reported by local histopathologists , and showed gleason scores of 6 or lower in 510 ( 61% ) of the 838 enrolled patients , a score of 7 in 222 ( 26% ) of patients , and a score 8 of or higher in 13% ( 106 ) of patients ; gleason score was not available for ve patients . 
160 ( 19% ) of 833 patients had low - risk disease according to nccn criteria , 311 ( 37% ) had intermediate - risk disease , and 362 ( 43% ) had high - risk disease ; unavailability of t - stage or histological grading precluded ascertainment of risk group in ten patients . 
overall , 117 patients were alive at 11 years and 30 at 12 years . as of aug 2 , 2011 , 236 deaths had been reported , 118 in each group , triggering the overall survival analysis . 
there was no di erence in 10 year overall survival between groups : 10 year overall survival was 71% ( 95% ci 6675 ) in both groups ( hr 099 , 95% ci 077128 , p = 096 , gure 2 )  . 
mean overall survival , using the exible parametric model and when restricted to 10 years , was 930 years ( 95% ci 908952 ) for the control group and 928 years ( 906950 ) for the escalated - dose group . 
there was no evidence of a di erence between restricted mean survival : 002 years ( 95% ci 034 to 029 ; p = 088 )  . for patients who had not yet reported a biochemical progression event , adherence to psa testing was 90% complete at 5 years and 76% complete at 10 years . 
 biochemical progression - free survival was better in the escalated - dose group , being 43% at 10 years ( 95% ci 3848 ) in the control group and 55% ( 5061 ) in the escalated - dose group ( hr 069 , 95% ci 056084 ; p = 00003 , gure 2 )  . 
mean biochemical progressionfree survival , when time of analysis was restricted to 10 years , was 733 years ( 95% ci 687780 ) in the control group and 801 years ( 760840 ) in the escalated - dose group , leading to an improvement in restricted mean survival of 069 years with escalateddose radiotherapy ( 95% ci 008130 ; p = 003 )  . 
||cause - speci c hr . table 2 : outcome measures 468 vol 15 april 2014 articles 020 015 010 005 control group escalated - dose group number at risk control group escalated - dose group control groups , pc death control groups , non - pc death escalated - dose groups , pc death escalated - dose groups , non - pc death number at risk control group escalated - dose group time from randomisation ( years ) time from randomisation ( years ) figure 4 : additional outcome measures ( a ) progression - free survival , kaplan - meier plot . 
progression - free survival , biochemical failure , and delayed commencement of salvage adt were all signi cantly better the escalated - dose group compared to the control group ( table 2 , gure 4 )  . 
of patients who had biochemical progression , a lower proportion ( 67 [ 30% ] of 221 patients ) in the control group had metastases , or died from prostate cancer compared to the escalated - dose group ( 65 [ 38% ] of 170 patients )  . 
notably , of the 391 patients who developed psa failure or progressive disease , only 220 ( 56% ) reported commencing long - term salvage adt ( 123 in the control group , 97 in the escalated - dose group )  . 
of 268 men who had clinical evidence of progressive disease , 132 ( 49% ) developed metastases or died from prostate cancer ( 67 in the control group , 65 in the escalated - dose group )  . according to the central , blinded review of deaths , 91 of 236 ( 39% ) deaths were from prostate cancer ( 44 in the control group , 47 in the escalated - dose group ) , 132 ( 56% ) were from other causes ( 68 in the control group vs 64 in the escalated - dose group ) , and for 13 ( 6% ) patients there were insu cient data for the reviewers to assign cause of death ( six control vs seven escalated dose ) : for ten , the investigator de ned causality as not prostate cancer ( which was accepted ) , and for the other three , no evidence of recurrent prostate cancer had been recorded . 
 we did a competing - risk analysis for prostate cancer death because 145 ( 61% ) of 236 deaths were from causes other the than prostate cancer , which exceeded prespeci ed level of 20% . 
the sub - hr for the comparison of cumulative incidences is 107 ( 95% ci 071161 ; p = 075 ) in favour of the control group with a cause - speci c hr for prostate cancer deaths of 106 ( 95% ci 070160 ; p = 079 ) and for other deaths of 096 ( 069132 ; p = 078 )  . nccn risk group was available for 90 of the 91 patients who died from prostate cancer . 
only one of 160 ( 1% ) men with low - risk disease died from prostate cancer compared with 21 of 311 ( 7% ) with intermediate - risk disease and 68 of 362 ( 19% ) with high - risk disease . 
as a proportion of total deaths , for lowrisk disease , one ( control group ) of 20 ( 5% ) were from prostate cancer compared with 21 ( nine control vs 12 escalated - dose ) of 81 ( 26% ) for intermediate - risk disease and 68 ( 34 control vs 34 escalated - dose ) of 133 ( 51% ) for high - risk disease . 
we identi ed no evidence of heterogeneity of e ect of dose escalation between these subgroups . discussion the previously reported advantage of escalated - dose conformal radiotherapy treatment compared to controldose conformal radiotherapy in biochemical progressionfree survival after a median follow - up of about 5 years was maintained in the present study with more mature data and a median follow - up of 10 years . 
this improvement in biochemical control of disease has not translated into an advantage for metastases - free survival , prostate - cancer - speci c survival , or overall survival . 
we identi ed no evidence of heterogeneity of treatment e ect between low , intermediate , and highrisk groups . we recorded a signi cant delay in the reported time to initiation of long - term , salvage adt in the escalated - dose group ; using the hr there was an absolute improvement of 7% ( 95% ci 012 ) at 10 years from 45% . 
this advantage of reducing or delaying the initiation of long - term adt , which is associated with well - documented andropausal side - e ects , 22 must be balanced against the known small increase in bowel side - e ects from the ve extra treatments in the escalated - dose group , which we and others have reported.5 , 6 , 8 , 10 , 16 , 23 why has the di erence in psa control not translated into an advantage for metastasis - free survival and prostate - cancer - speci c survival ? several factors might be involved . 
first , it is likely that there were more indolent recurrences con ned to the prostate in the control group : a lower proportion of patients in the control group had metastases or died from prostate cancer than those in the escalated - dose group . 
moreover , of patients who developed psa failure or progressive disease , only 56% reported commencing long - term salvage adt , and only 49% of patients who had clinical evidence of progressive disease developed metastases or died from prostate cancer . 
we now know that some men with indolent local disease do not necessarily need treatment , for example men with low - risk disease or older than 65 years do not bene t from radical prostatectomy , 24 , 25 and active surveillance has become a standard of care for patients with a favourable outlook.26 second , there is a long time from commencement of salvage adt to death . 
in an international trial of intermittent or continuous salvage androgen suppression , 22 time from salvage adt to death was estimated at about 9 years , but with only about 17% of patients dying of prostate cancer after 7 years . 
in the control group of rt01 , 25% of patients had a biochemical progression - free survival event by 26 years after randomisation , but it was 57 years from randomisation before 25% of patients had reported initiation of salvage adt ; median times for these outcome measures have not been reached . 
moreover , our results clearly show that nccn risk group was related to the probability of dying from prostate cancer . the lower bound of the 95% ci for overall survival was 077 , and therefore our results cannot rule out some improvement in overall survival . 
 after 14 years of follow - up , the small pilot study ( n = 126 ) which recruited before the start of rt01 suggested an overall survival advantage for the escalated - dose group ( 74 gy ) with hr 059 , but with only 19 prostate cancer deaths the 95% cis were wide ( 023149 ) .5 the phoenix de nition27 our trial was designed in 1997 and launched in 1998 before for biochemical recurrence became established , but our chosen de nition of psa failure with 2 ng / ml has much the same speci city and sensitivity.28 our results are in alignment with reported data from other studies of dose - escalated external beam radiotherapy ( table 3 ) , which have shown absolute advantages in psa failure - free survival of 619% for dose - escalated treatments . even in trials with a high proportion of patients with poor prognostic factors and long follow - up , none have yet reported prostate - cancer - speci c mortality of greater than 15% . 
a meta - analysis with the other randomised trials would provide a larger number of events from patients with high - risk disease to assess the e ect of dose - escalation on death from prostate cancer . our ndings draw attention to two issues for future trials . 
 survival - based outcome measures must remain of paramount importance , but there are implications for recruiting centres , trials units , and funding bodies in collecting long - term data . 
 * freedom from biochemical ( psa ) or clinical failure . table 3 : data from randomised controlled trials of dose - escalated external beam radiotherapy for prostate cancer absolute reduction in psa failure in dose escalated group ( 10 year ) ( 10 year ) ( 10 year ) 19% * ( 8 year ) ( 12 year ) 85% ( 5 year ) ( 10 year ) ( 10 year ) ( ns ) ( 8 year ) about ( 14 year ) ( ns ) outcome data needs to be explored . 
we have previously reported our comparative side - e ect data , which we planned to collect only to 5 years , 7 , 15 , 16 and a limitation of the present report is that no 10 - year patient - reported outcome data are available . by contrast with the dose - escalation trials , phase 3 studies assessing the addition of neoadjuvant adt to radical prostate radiotherapy have shown clear evidence of improved overall survival and cause - speci c survival in meta - analysis.29 , 30 review of additional trial results1114 shows that survival bene ts become apparent about 35 years after randomisation . 
one interpretation is that , in addition to short - course adt having an e ect on local control of disease , 11 6 months of adt also has a direct e ect on eradication of micrometastatic disease . 
 these trials have been in patients given modest doses of radiotherapy by present standards ( equivalent to 70 gy or lower ) but large institutional us series have suggested much the same bene ts of neoadjuvant adt in patients given doses of 7681 gy.31 , 32 either what are the relative merits of dose escalation and combined modality treatment with neoadjuvant adt ? dose escalation leads to excellent local disease control using brachytherapy33 in lower risk disease . 
by use of a biopsy sample obtained 2 years after treatment as a gold radiotherapy external beam panel : research in context systematic review radiotherapy dose is limited by treatment - related side - e ects . 
advancing radiotherapy techniques using conformal radiotherapy had been shown to reduce the occurrence of side - e ects.3 dose - escalation therefore became feasible with the hypothesis that higher radiation doses would lead to improved outcomes.5 , 3739 interpretation as far as we are aware , this study is the largest dose - escalation trial to have reported long - term e cacy results . 
 however , none of these trials have convincingly shown a positive e ect on overall or prostate - cancer - speci c survival after 10 years of follow - up . 
dose escalation improves intermediate disease outcomes and reduces the use of salvage hormonal treatment , but at the cost of a modest increase in treatment - related side - e ects . 
further improvements in radiotherapy techniques have been shown to reduce the e ect of dose - escalation on side - e ects4 , 40 , 41 and should be used to maintain the reported advantages of dose - escalation while minimising treatment sequelae . 
 standard method34 to detect local recurrence , a 3 - month period of neoadjuvant adt given with modest - dose or high - dose radiotherapy reduced positive biopsy ndings from 46% to 10%.35 in a preplanned substudy of the rt01 trial , only six ( 6% ) of 97 men in the escalated - dose group who agreed to have a biopsy 2 years after treatment had positive histology ( unpublished )  . 
the use of neoadjuvant adt , however , must be balanced against the usually short - lasting increase in morbidity from vol 15 april 2014 articles short - term adt.36 clinical trials that are in progress , including eortc study 22991 ( nct00021450 ) , will more completely de ne the role of combined modality treatment and high - dose radiotherapy . and since we designed our trial using conformal radiotherapy methods , technology advances have led to the widespread introduction of intensity - modulated , image - directed , techniques image - guided including the combined use of external beam radiotherapy with high - dose or low - dose rate brachytherapy , which have enabled high - dose treat ment to be given with a reduced prevalence of side - e ects using conventional or hypofractionated schedules ( panel ) .4 , 40 , 41 high - quality treatments are essential to maintain the potential advantages of dose - escalated treatment in improving disease control and avoiding salvage therapy , while maintaining low levels of treatmentrelated side - e ects . in conclusion , we have shown a clear and maintained advantage in biochemical ( psa ) assessment of disease control , which has translated into a modest reduction in salvage adt , but no evidence of a bene t in survivalbased outcome measures with a median follow - up of 10 years . 
all authors were involved in data interpretation , manuscript review , and approval of the nal manuscript . declaration of interests mrs , mkbp , gj , cm are employees of the sponsor at the medical research council , clinical trials unit at ucl , london , uk . 
randomized trial comparing conventional - dose with high - dose conformal radiation therapy in early - stage adenocarcinoma of the prostate : long - term results from proton radiation oncology group / american college of radiology 95 - 09 . 
the early toxicity of escalated versus standard dose conformal radiotherapy with neo - adjuvant androgen suppression for patients with localised prostate cancer : results from the mrc rt01 trial ( isrctn47772397 )  . 
implementing the uk medical research council ( mrc ) rt01 trial ( isrctn 47772397 ) : methods and practicalities of a randomised controlled trial of conformal radiotherapy in men with localised prostate cancer . 
j natl cancer inst monogr 2012 ; 45 : 23441 . 472 vol 15 april 2014 articles 27 roach m 3rd , hanks g , thames h jr , et al . 
is androgen deprivation therapy necessary in all intermediate - risk prostate cancer patients treated in the dose escalation era ? int j radiat oncol biol phys 2013 ; 85 : 69399 . 33 morris wj , keyes m , spadinger i , et al . 
int j radiat oncol biol phys 1998 ; 41 : 491500 . 36 stephens rj , dearnaley dp , cowan r , sydes m , naylor s , fallow eld l . 
 cancer treat rev 2014 ; 40 : 41425 . vol 15 april 2014 correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections * krzysztof bujko , rafa sopyo i department of radiotherapy ( kb ) and department of surgery ( rs ) , m skodowska - curie memorial cancer centre , 02 781 warsaw , poland ( kb ) bujko@coi.waw.pl we declare no competing interests . ngan sy , burmeister b , fisher rj , et al . 
randomized trial of short - course radiotherapy versus long - course chemoradiation comparing rates of local recurrence in patients with t3 rectal cancer : trans - tasman radiation oncology group trial 01.04. 
effect of interval ( 7 or 11 weeks ) between neoadjuvant radiochemotherapy and surgery on complete pathologic response in rectal cancer : a multicenter , randomized , controlled trial ( greccar - 6 )  . 
 although this advice seems reasonable , the stockholm iii trial does not support this because 30 - day and 90 - day postoperative mortality was not decreased after delaying surgery ; 3 , 5 however , only a fourth of patients in this trial were older than 75 years . 
 one small prospective trial reported acute toxicity in 27% of patients in the short - course radiotherapy with delayed surgery group and in 64% of patients in the chemoradiation group ( p = 0001 ) .8 other trials investigating short - course radiotherapy with delayed surgery also reported lower frequencies of acute radiation toxicity compared with that usually observed after chemoradiation.3 , 6 , 9 of note , about 1% mortality due to chemoradiation toxicity has usually been reported , whereas to our knowledge , no mortality attributed to short - course radiotherapy has ever been described . 
simple digital rectal examination became the sole method for the assessment of response among these patients 276 vol 18 march 2017 comment without the requirement for complex , elaborate , or expensive studies to rule out the presence of microscopic disease . 
despite the inherent differences between anal and rectal cancers , this approach was considered years later to be applicable to patients with very distal rectal adenocarcinomas that had a complete clinical response after being treated with a chemoradiotherapy regimen similar to that used for anal cancer.4 however , nigros original findings and observational treatment approach endured slower acceptance in the clinical rectal oncology community . 
 these rectal cancers are located centimetres away from the anus and have been only recently more widely considered for an organ - preserving strategy without immediate radical surgery after a complete clinical response.5 , 6 the understanding of in the lancet oncology , robert glynne - jones important and colleagues , 7 , 8 provide an additional contribution in - vivo kinetics of anal tumour response to neoadjuvant chemoradiotherapy . 
the observation that the ideal interval to assess tumour response is 26 weeks is remarkable and a leap forward in clinical practice for the management of these patients , especially considering that this interval was formerly only 8 weeks.9 besides the issue of timing of assessment , the present study draws attention to a very interesting observation . 
 not only were patients unharmed by rather long periods of time without a definitive conclusion ( complete versus incomplete response ) , but were not prematurely given unnecessary surgical resection . 
ultimately , the inherent subjectivity of clinical response assessment and the variation in examiners and specific tools for assessment of response incorrectly might have accounted for some complete clinical responses being incomplete clinical response in the early intervals . 
furthermore , these results and the kinetics of tumour regression after neoadjuvant chemoradiotherapy and the accuracy of clinical assessment might not be unique to anal carcinoma and might again apply , at least to some extent , to rectal adenocarcinoma after neoadjuvant chemoradiotherapy . 
 * angelita habr - gama , guilherme pagin so julio , rodrigo oliva perez colorectal surgery division , university of so paulo , so paulo , brazil ( ah - g ) ; and gastroenterology department , angelita and joaquim gama institute , so paulo 04001 - 005 , brazil ( ah - g , gpsj , rop ) we declare no competing interests . the author ( s )  . 
 int j radiat oncol biol phys 2003 ; 56 : 125973 . vol 18 march 2017 comment see correspondence page e194 preventable cancer : off - limits for commonwealth meeting ? as the global burden of non - communicable diseases continues to exert its toll , the prevention , screening , and early diagnosis of cancer should be a priority for all countries . 
the letter , cosigned by eminent experts in cancer and population health , demands that issues surrounding cervical cancer and endemic childhood cancers are part of the commonwealth health ministers meeting in may 2017 . 
the signatories also call for screening , early detection , and improved awareness of various childhood cancers , which can be treated successfully if caught early or even prevented through effective control of malnutrition and infectious diseases . 
surely the health of women and children is paramount to achieve such goals ? cost - effective prevention and screening for cancers should be an integral part of any successful uhc agenda . 
the limited reply declares that the prevention , treatment , and care of cancers are a priority , but fails to suggest any amendments to the forthcoming meetings agenda to give these important issues the consideration they deserve . 
a recent report from the american cancer society warns that the incidence of the diseasein which typically 90% of patients are over 50 years of ageis increasing sharply in each generation born since 1950 . 
as national colorectal and bowel cancer awareness months are marked in march and april in the usa and uk , respectively , this timely report rings alarm bells for ominous changes in the aetiology of this disease . despite colorectal cancer being a slow growing disease in which symptoms may not present for many years , survival rates have improved in recent decades , mainly thanks to screening . 
major risk factors ( unhealthy diets , obesity , and sedentary lifestyles ) are becoming more prevalent in successive generations , raising the question of whether these factorsespecially in the early years of lifecould interact with an underlying genetic backdrop to trigger early onset of the disease . screening is the mainstay of colorectal cancer prevention and early detection . 
 furthermore , with the widespread belief that cancer is associated with ageing , family doctors can too easily discount the possibility of colorectal cancer in young patients , even when they present with characteristic symptoms such as blood in the stool and abdominal pain . what can be done ? although whole - population screening is not feasible , cost - effective , or truly warranted , genetic counselling and gene testing for those known to be at high risk because of family history or underlying genetic predisposition could be considered . 
 the lancet oncology vol 18 april 2017 editorial editorial for more on the debate surrounding the harms and bene ts of e - cigarettes see comment lancet respir med 2013 ; 1 : 42931 and 43133 for more on the e ectiveness of e - cigarettes to help quit smoking see articles lancet 2013 ; published online sept 9 . 
most importantly , new evidence released by the us centers for disease control and prevention ( cdc ) on sept 6 , 2013 , shows that use of e - cigarettes by children and teenagers has more than doubled in the past 2 years . 
there is a real danger of the devices becoming a gateway product , attracting more young people to begin smoking , undoing years of public awareness campaigning on the dangers of smoking . 
 however , in the usa , a legal case between sottera ( an importer and distributor of e - cigarettes ) and the us food and drug administration ruled that e - cigarettes should be regulated as tobacco products unless explicitly marketed for therapeutic purposes . 
in the usa , blu ecigs sponsor an indycar team , while in the uk , merthyr town football club has renamed its stadium the cigg - e stadium in light of a sponsorship deal , and e - lites have gone into partnership with scottish football team celtic . 
further , e - cigarette companies are actively soliciting their consumers to become brand managers to promote their products through social mediaa cynical attempt to appeal to a younger target audience . 
many teens who start with e - cigarettes may be condemned to struggling with a lifelong addiction to nicotine and conventional cigarettes . the addictive nature of nicotine is where the inherent aw in e - cigarette advocacy lies . 
irrespective of the safety of the delivery mechanism , regular use of addictive substances causes users to become acclimatised to their current dosage and seek other ways to increase it . 
for example , according to the 2012 annual report of us tobacco rm lorillard , blu ecigs accounted for most of their 42% growth last year , and british american tobacco recently acquired e - cigarette company vype to expand their portfolio of products . 
given that most e - cigarettes are designed to mimic cigarettes in as many ways as possible , being around people lighting upelectronically or otherwisewill once again become socially acceptable . 
such regulation would prevent tobacco companies from adopting their usual cynical and devious tactics to hook young people to a product that serves as a gateway to their main business interestthe sale of regular cigarettes . 
the primary aim of this study was to establish how cetuximab might be safely and e ectively added to intermittent chemotherapy . methods coin - b was an open - label , multicentre , randomised , exploratory phase 2 trial done at 30 hospitals in the uk and one in cyprus . 
patients in both groups received folfox and weekly cetuximab for 12 weeks , then either had a planned interruption ( those taking intermittent cetuximab ) or planned maintenance by continuing on weekly cetuximab ( continuous cetuximab )  . 
 10 - month failure - free survival was 50% ( lower bound of 95% ci 39 ) in the intermittent group versus 52% ( lower bound of 95% ci 41 ) in the continuous group ; median failure - free survival was 122 months ( 95% ci 88156 ) and 143 months ( 107204 ) , respectively . 
the most common grade 34 adverse events were skin rash ( 21 [ 27% ] of 77 patients vs 20 [ 22% ] of 92 patients ) , neutropenia ( 22 [ 29% ] vs 30 [ 33% ] ) , diarrhoea ( 14 [ 18% ] vs 23 [ 25% ] ) , and lethargy ( 20 [ 26% ] vs 19 [ 21% ] )  . interpretation cetuximab was safely incorporated in two rst - line intermittent chemotherapy strategies . 
maintenance of biological monotherapy , with less cytotoxic chemotherapy within the rst 6 months , in molecularly selected patients is promising and should be validated in phase 3 trials . funding uk medical research council , merck kgaa . 
open access article distributed under the terms of cc by . introduction the discovery of predictive biomarkers for advanced colorectal cancer and the development of new targeted treatments has led to the combination of cytotoxic drugs with targeted treatments as the international standard of care . 
however , these combinations have failed to improve outcomes in several phase 3 trials.14 toxic e ects caused by drug combinations have also confounded assessments of e cacy.2 , 3 intermittent treatment and maintenance biological treatment have been explored in several trials to address this shortcoming.311 palliative treatment of cancer should address both quantity and quality of life . 
 minimising the time spent taking cytotoxic drugs and introducing chemotherapy - free intervals or complete treatment holidays ( ie , planned interruptions ) might help to meet both these goals . 
de - escalation of components of treatment for maintenance in patients vol 15 may 2014 articles for the study protocol see plugins / studydisplay / protocols / coin - b%20combined%20 protocol%20with%20crfs.pdf who have not progressed is increasingly done in practice and a clinical bene t has been shown in a trial of capecitabine and bevacizumab maintenance treatment.8 however , the best strategy to use for di erent clinically or molecularly de ned cohorts has yet to be established . the coin trial1 , 6 was designed to assess whether intermittent chemotherapy was as e ective as continuous chemotherapy and whether the addition of cetuximab to continuous chemotherapy was associated with additional bene t . 
in the coin - b trialdone as an adjunct to coinwe sought to establish how cetuximab might be safely and e ectively added to intermittent chemotherapy . methods study design and participants we did this open - label , multicentre , randomised , exploratory phase 2 trial at 30 hospitals in the uk and one in cyprus . 
eligibility criteria were age 18 years or older , colorectal adenocarcinoma , inoperable metastatic or locoregional measurable disease according to recist ( version 1.1 ) , no previous chemotherapy for metastases , who per formance status 02 , and good organ function ( baseline require ments were : 15 10 neutrophils per l , 100 10 platelets per l , serum bilirubin 125 upper limit of normal , serum aminotransferases 25 upper limit of normal , alkaline phosphatase 5 upper limit of normal , and estimated creatinine clearance or measured glomerular ltration rate 50 ml / min )  . 
 patients were excluded if they had had any previous likely to cancer , uncontrolled medical comorbidity interfere with coin - b treatment or response assessment , or known brain metastases . the trial was designed before kras mutations were identi ed as predictors of resistance to egfr monoclonal antibody treatment.12 coin - b was suspended in may , intermittent chemotherapy and intermittent cetuximab randomisation intermittent chemotherapy and continuous cetuximab cetuximab maintenance cetuximab maintenance folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks folfox cetuximab 12 weeks figure 1 : trial design treatment cycles continued until progressive disease ( pd ) with maximally tolerated treatment , or patient choice . 
 folfox = folinic acid and oxaliplatin followed by bolus and infused uorouracil . 2008 , and on restarting ( january 2009 ) it included prospective kras mutation analysis before ran domisation . 
coin - b was approved by the south west research ethics committee and the medicines and healthcare regulatory agency in the uk and the national bioethics and the pharmaceutical services of the ministry of health in cyprus . randomisation and masking the mrc clinical trials unit did the randomisation by telephone , using the method of minimisation with a random element . 
rb established the mutational status of braf ( codon 600 ) and nras ( codons 12 , 13 , and 61 ) retrospectively for kras wild - type patients who consented to future bowel cancer research . 
when cetuximab was given in combination with chemotherapy ( day 1 ) , cetuximab was given rst ( see protocol for full details of the treatment regimens )  . patients in both groups received treatment for 12 weeks and those with stable or responding disease started a chemotherapy - free interval ( ie , no folfox )  . 
on recist 632 vol 15 may 2014 119 patients registered before protocol amendment 59 assigned to intermittent cetuximab 60 assigned to continuous cetuximab 282 patients registered after protocol amendment 57 excluded 18 no tumour block or analysis 39 kras mutations failed articles 9 had abnormal laboratory 133 had kras mutation 175 excluded test results 1 scan out of date 1 performance status > 2 1 previous oxaliplatin 1 resectable metastases 1 unusual histology 9 kras analysis failed 7 too ill 2 died 9 withdrew consent 1 chemoradiation within 1 month 62 kras wild - type 25 assigned to intermittent cetuximab 37 assigned to continuous cetuximab 107 kras wild - type 169 eligible and randomly assigned 78 assigned to intermittent cetuximab 91 assigned to continuous cituximab 14 did not complete initial 12 weeks of chemotherapy and cetuximab 25 did not complete initial 12 weeks of chemotherapy and cetuximab 64 included in primary analysis 66 included in primary analysis 20 did not restart trial study treatment after rst chemotherapy - free interval 9 early progression or death 4 patient or doctor choice 3 complete response or liver surgery 2 toxic eects 1 intercurrent illness 1 lost to follow - up and censored 33 did not restart trial study treatment after rst chemotherapy - free interval 5 early progression or death 15 patient or doctor choice 5 complete response or liver surgery 4 toxic eects 2 intercurrent illness 2 lost to follow - up and censored 44 restarted study treatment after rst chemotherapy - free interval 33 restarted study treatment after rst chemotherapy - free interval figure 2 : trial pro le we designed coin - b as two separately powered phase 2 trials , using aherns single - stage design15 to distinguish between a 10 - month failure - free survival of 50% ( implying that the treatment would be worth pursuing in a phase 3 trial , feasibility and toxic e ects permitting ) and of 35% ( implying that the treatment would not be worth pursuing )  . 
serious adverse events and deathstogether with an assessment of causalitywere con tinuously reported ; and were reassessed by an experienced oncologist ( rst by am , then the trial management group ) on behalf of the medical research council . a baseline ct scan was done within 4 weeks before the start of treatment and then at least once every 12 weeks and evaluated with recist criteria . 
data were collected via remote data capture , except for reports of serious adverse events , which were submitted by fax . outcomes the primary outcome was failure - free survival at 10 months . 
secondary objectives were : safety assessment of cetuximab reintroduction , overall survival , progression - free survival , response rates , toxic e ects , disease control at 24 weeks ( complete response , progressive disease , and stable disease ) , and quality of life . time from randomisation ( week 0 ) was used for the analysis of failure - free survival and overall survival . 
at the time of analysis , survivors were censored at the date they were last known to be alive . the primary and main secondary outcomes ( overall survival and progression - free survival in the interval ) were retrospectively analysed for patients who were triple wild - type ( for kras , braf , and nras )  . 
data from phase 2 studies14 suggested that 50% failure - free survival at 10 months would be a suitable primary outcome for the addition of cetuximab . vol 15 may 2014 articles women site of primary tumour right or transverse colon status of primary tumour left colon or rsj rectum resected unresected local recurrence distribution of metastases liver only non - liver liver and elsewhere data missing [ a : ok ? ] number of metastatic sites none three adjuvant chemotherapy 16 months ago > 6 months ago suspension , interim data from coin and coin - b suggested that attrition before 12 weeks was 16% because of toxic e ects or absence of bene t . 
as a result , we changed the target enrolment so that 158 patients with kras wild - type would be included , of whom we expected 136 to be assessable for the primary outcome . we used the kaplan - meier method to assess failurefree survival , overall survival , and progression - free survival . 
we used stata ( version 11.1 ) for all statistical analyses . the trial is registered as an international standard randomised controlled trial , number isrctn38375681 . role of the funding source the mrc was the overall sponsor of the trial . 
the corresponding author had full access to the data and had nal responsibility for the decision to submit for publication . results between july 13 , 2007 , and march 6 , 2010 , 401 patients were registered and 226 patients were enrolled . 
the continuous cetuximab group had more elderly patients ( age > 75 years ) , more with a who performance score of 2 , more with braf mutations , and more with primary colon cancers ( vs rectal ) than did the intermittent cetuximab group ( tables 1 , 2 )  . 24 patients had braf mutations and 15 had nras mutations ( table 2 )  . 
it has not since been validated and our analysis con rms that it is not informative ( data not shown )  . at the time of analysis ( april 24 , 2012 ) , median duration of follow - up in the kras wild - type intention - to - treat population was 328 months ( iqr 229458 ) in the intermittent cetuximab group and 342 months ( iqr 273504 months ) in continuous cetuximab group . seven patients did not start protocol treatment : two in the intermittent cetuximab group and ve in the continuous cetuximab group . 
most patients required a treatment delay , 68 ( 87% ) of 78 patients in the intermittent cetuximab group and 74 ( 81% ) of 91 in the continuous cetuximab group . 
dose modi cations occurred in similar proportions in each group ; for cetuximab , modi cations were made for 57 ( 73% ) of 78 patients taking intermittent cetuximab versus 70 ( 77% ) of 91 taking continuous cetuximab , oxaliplatin was modi ed for 40 ( 51% ) versus 43 ( 47% ) patients , and uorouracil was modi ed for 49 ( 63% ) versus 51 ( 56% )  . 
treatment was discontinued because of drug - related toxic e ects for nine ( 12% ) of 78 patients in the intermittent group versus 11 ( 12% ) of 91 in the continuous group . the primary analysis included 64 patients in the intermittent cetuximab group and 66 in the continuous cetuximab group . 
patients were excluded for progressive disease ( one in the intermittent cetuximab group vs four in the continuous cetuximab group ) , death ( four vs 14 ) , and failure of treatment in the rst 12 weeks ( nine vs seven )  . 
the greater dropout from the continuous cetuximab group could be a result of di erences in baseline characteristics combined with the greater proportion of patients with a braf mutation ( table 1 , appendix )  . 
in the primary analysis population , at least 50% of patients were failure - free at 10 months in both groups : 32 ( 50% ) of 64 in the intermittent cetuximab group and 34 ( 52% ) of 66 in the continuous cetuximab group . 
median failure - free survival was 122 months ( 95% ci 88156 ) in the intermittent cetuximab group and 143 months ( 107204 ) in the continuous cetuximab group ( gure 3a )  . 
in an intentionto - treat analysis ( n = 169 ) , median failure - free survival was 121 months ( 95% ci 78147 ) versus 120 months ( 87145 ; appendix )  . 
median failure - free survival was greater for patients with all wild - type alleles than for those with kras wild - type only in both treatment groups , in both the primary analysis cohort and the intention - to - treat population ( gure 3b ; appendix )  . in the primary analysis cohort , median overall survival was 168 months ( 95% ci 145226 ) in the intermittent cetuximab group versus 222 months ( 184289 ) in the continuous cetuximab group ( gure 4a )  . 
the di erence in median overall survival was smaller in the intentionto - treat population ( 160 months , 95% ci 133204 vs 175 months , 137217 ; appendix )  . 
median overall survival was greater for patients with all wild - type alleles than for those with kras wild - type only in both treatment groups in both the primary analysis cohort and the intention - to - treat population ( gure 4b ; appendix )  . from week in the primary analysis cohort , median progressionfree survival 12 was 31 months ( 95% ci 2847 ) in the intermittent cetuximab group and 58 months ( 4986 ) with continuous cetuximab ( gure 5a )  . 
as with the other survival endpoints , median progression - free survival was greater for patients with all wild - type alleles than for those with kras wild - type , for both treatment groups ( gure 5b )  . 54 ( 32% ) of 78 patients died in the intermittent cetuximab group versus 67 ( 40% ) of 91 in the continuous cetuximab group . 
112 ( 93% ) deaths were caused by colorectal cancer ( 49 vs 63 ) , three ( 2% ) were related to treatment ( one vs two ) , and six ( 5% ) were the result of other causes ( four vs two )  . only 77 patients restarted trial treatment after a intermittent interval , 44 chemotherapy - free cetuximab and 33 taking continuous cetuximab . 
for patients who survived at least 24 weeks , greater disease control ( ie , complete response , partial response , or stable disease ) was noted in those assigned to continuous cetuximab ( n = 29 , 32% ) than in those assigned to intermittent cetuximab the imbalances . ( n = 17 , 22% ) , despite patients with mutations in kras , nras , and braf had a worse prognosis than patients with wild - type for overall survival and failure - free survival in the intention - to - treat population ( p < 00001 for both outcomes ; appendix )  . toxic e ects and adverse events were similar in each treatment group . 
three patients in the intermittent cetuximab group reported grade 3 or higher hyper sensitivity events with only one on reintroduction of cetuximab ( table 3 )  . both the coin and coin - b trials contained a quality - oflife substudy . 
although not statistically compared , maintenance cetuximab with inter mittent chemotherapy seemed to be slightly more active than intermittent cetuximab with intermittent chemotherapy . coin - b is one of a series of trials of patients with noncurable advanced colorectal cancer to explore strategies to improve the combinations and sequences of cytotoxic treatments , planned targeted chemotherapy , newer maintenance , and planned interruptions ; all with a focus on reducing toxic e ects and improving quality of life without reducing survival . 
in some trials , part or all of the rst - line chemotherapy is discontinued in the investigational group and compared with continuation of the full rst - line treatment.4 , 7 , 11 , 16 in others , planned maintenance is compared with a planned interruption5 , 8 , 9 or an additional maintenance treatment is introduced when chemotherapy is discontinued.10 in all these studies , the conventional surrogate endpoint of progression - free survival is inappropriate because it does the subsequent bene t of planned not consider reintroduction of full rst - line treatment on progression . 
 other outcome measures have therefore been used ( duration of disease control and failure - free survival ) .5 however , the best measure of how maintenance treatment a ects the course of disease is progressionfree survival in the interval . the coin trial adds to preliminary data from cr06 and optimox - 1 , 11 , 16 which suggested that interruption or de - escalation of treatment was safe and potentially bene cial . 
the results of adams and colleagues6 could not exclude the possibility of a very small negative e ect on overall survival of a treatment holiday after 3 months of cytotoxic chemotherapy . 
the upper limits of the twosided 80% cis for the hazard ratios ( hrs ) in both the per - protocol and intention - to - treat analyses were greater than the prede ned non - inferiority boundary of 1162 . 
 the hr in the intention - to - treat population ( n = 1630 ) was 1084 ( 80% ci 10081165 ) and in the per - protocol population ( n = 978 ) it was 1087 ( 09861198 ) .6 planned subgroup analyses showed that patients with normal baseline platelet counts could gain the bene ts of intermittent chemotherapy without harming survival . 
 this nding suggests that a planned interruption might not be detrimental to most patients and warrants further study with clinical or molecular predictive markers . coin - b was designed as an exploratory , hypothesisgenerating study to complement coin . 
at randomisation , only infusional uorouracil in com bination with oxaliplatin and cetuximab was allowed , which removed the confounding e ect and possible negative interaction reported in coin and other studies when capecitabine was the partner uoropyrimidine.17 in coin - b , planned maintenance with cetuximab ( ie , continuous cetuximab ) was associated with a greater failure - free survival , greater progression - free survival , greater overall survival , improved disease control at 24 weeks , and a longer chemotherapy - free intermittent cetuximab . 
such an imbalance might be considered a limitation of a small study such as coin - b ; however , the main reason for the imbalance between groups was discovered after the change in the population of interest from all patients with advanced than was interval vol 15 may 2014 articles panel : research in context systematic review at the time of study inception , very few randomised trials had been done of cetuximab and chemotherapy , all of which were reviewed to help power the study , and choose the outcome measures . 
stopping and restarting cetuximab could in theory increase the risk of hypersensitivity , so establishing safety was a main aiwe designed coin - b to complement the coin trial.1 , 6 coin rst tested the non - inferiority of intermittent chemotherapy compared with continuous chemotherapy and second , the addition of cetuximab to continuous chemotherapy for superiority . 
this nding needs to be validated in phase 3 trials , such as the upcoming focus 4 study , 20 in which novel targeted treatments will be assessed in biomarker - enriched populations . colorectal cancer to those who had kras wild - type tumours . 
119 patients were enrolled before the introduction of kras screening , 62 of whom were subsequently found to be kras wild - type and included in the primary outcome analysis . 
this nding is consistent with data for egfr inhibitors as rst - line treatment.18 , 19 other studies comparing planned maintenance interruption have shown treatment with planned evidence of a bene t of maintenance treatment . 
in optimox - 2 , planned maintenance with infusions of uorouracil and leucovorin prolonged disease control compared with a planned interruption although it had no signi cant e ect on overall survival ( 238 months vs 195 months , hr 085 ; p = 042 ) .5 in cairo - 3 , 8 planned maintenance with bevacizumab and capecitabine was compared with a planned interruption , after 4 months of induction treatment with capecitabine , oxaliplatin , and improved probevacizumab . 
planned maintenance gression - free survival in the interval ( 41 months vs 85 months , hr 044 , 95% ci 037054 ; p < 00001 ) and overall survival ( 179 months vs 217 months , hr 077 , 95% ci 062096 ; p = 002 )  . 
median time to progression was 179 weeks ( 95% ci 133234 ) for bevacizumab continuation and 126 weeks ( 120164 ) for no continuation ( hr 072 , 95% ci 056092 )  . 
coin - b is the rst trial to enrol patients with kras wild - type to di erent intermittent treatment schedules and therefore show the e ect of planned maintentance with a in a molecularly selected subgroup . targeted monotherapy two other studies have tested egfr inhibition as planned maintenance treatment . 
progression - free survival in the interval was improved from 48 months with bevacizumab alone to 59 months with bevacizumab and erlotinib ( hr 076 , 95% ci 061094 ; p = 001 )  . 
thus , the best strategies by which integrate bevacizumab and cetuximab into treatment are di erent , because no predictive biomarker has been discovered for bevacizumab . the nordic - vii trial4 investigated the e cacy of cetuximab when added to bolus uorouracil with folinic acid and oxaliplatin ( nordic flox ) in patients with previously untreated metastatic colorectal cancer . 
the investigators did not compare planned maintenance with cetuximab with a planned interruption and had no mandated criteria for chemotherapy reintroduction ; however , the similarity in overall survival between groups suggests that maintenance cetuximab might be an alternative strategy to continuing chemotherapy until progression . the life expectancy of patients with advanced colorectal cancer is increasing , raising questions of duration and intensity of treatment required . 
for inhibitors , greater re nement of biomarker egfr selection suggests maintenance monotherapy might be a favourable continuation strategy ( panel )  . the molecular evolution of panitumumab resistance has been elegantly shown in patients who were initially diagnosed as kras wild - type but soon developed detectable mutations in kras in their sera ( three of whom developed several di erent kras mutations ) .21 the appearance of these mutations consistently occurred 56 months after the start of treatment , which coincides with the clinical bene t noted with egfr inhibitors used 638 vol 15 may 2014 articles as monotherapy . 
the hypothesis that minimal residual disease in cancer is controlled , but rarely eradicated , implies that ono strategies with drugs might be a rational way to regulate clonal selection favourably in palliative care . 
other studies concur with coin - b with respect to the bene t of planned maintenance , although both induction chemotherapy and the bene t of continuing maintenance cytotoxic drugs to achieve maximal clinical bene t , are unknown . 
further clinical trials are warranted to investigate these points . the best duration of contributors hw was chief investigator , chaired the trial management group , cowrote the report , and enrolled patients . 
all authors reviewed the data and commented on the report . declaration of interests hw has taken part in advisory boards and educational meetings as faculty and speaker for merck kgaa during this study . 
 amm , df , cp , bs , rk , am , rb , and cl declare that they have no competing interests . acknowledgments merck kgaa provided an educational grant . 
we thank all of the patients and their families who agreed to participate in coin - b . correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections corrections correction to lancet oncol 2013 ; 14 : 297 correction to lancet oncol 2013 ; 14 : 481 correction to lancet oncol 2013 ; 14 : 557 motzer rj , escudier b , tomczak p , et al . 
this correction has been made to the online version as of may 28 , 2013 . galimberti v , cole bf , zurrida s , et al , for the international breast cancer study group trial 2301 investigators . 
 lancet oncol 2013 ; 14 : 297305in the summary of this article , the fourth sentence of the findings section should read : breast cancer - related events were recorded in 48 patients in the axillary dissection group and 47 in the no axillary dissection group ( ten local recurrences in the axillary dissection group and eight in the no axillary dissection group ; three and nine contralateral breast cancers ; one and ve regional recurrences ; and 34 and 25 distant relapses )  . 
 this correction has been made to the online version as of may 28 , 2013 . tom waddell , oesophagogastric randomised , waddell t , chau i , cunningham d , et al . 
lancet oncol 2013 ; 14 : 48189in this article , list of authors should have the read : ian chau , david cunningham , david gonzalez , alicia frances clare okines , andrew wotherspoon , claire sa ery , gary middleton , jonathan wadsley , david ferry , wasat mansoor , tom crosby , fareeda coxon , david smith , justin waters , timothy iveson , stephen falk , sarah slater , clare peckitt , yolanda barbachano . 
this correction has been made to the online version as of may 28 , 2013 . vol 14 june 2013 e254 correction to lancet oncol 2017 ; 18 : 895903 the cancer : a shaverdian n , lisberg ae , bornazyan k , et al . 
this correction has been made in the online version as of may 25 , 2017 . toxicities published online may 25 , 2017 s1470 - 2045 ( 17 ) 30409 - 6 vol 18 july 2017 e371 corrections for more on the pharmaceutical industrys interest in immunotherapy see financial times july 2 , 2017 . 
 business / 2017 / 06 / 25 / behindbig - pharmas - race - develop - nextwave - cancer - therapy / for more on the ca184 - 024 trial see j clin oncol 2015 ; 33 : 119196 for more on the reproducibility of preclinical studies see plos biol 2017 ; 15 : e2002212 calling time on the immunotherapy gold rush at the 2008 annual meeting of the american society of clinical oncology , results from an early phase trial of ipilimumab heralded a remarkable turnaround in fortunes for immunotherapyan intervention previously considered to be a dead end , limited to underwhelming outcomes with interleukin - 2 . 
results from the pivotal ca184 - 024 phase 3 trial on the same drug 3 years later proved beyond any doubt that targeting the immune system was both possible and efficacious . 
however , fastforward to 2017 , and with about 800 immunotherapy clinical trials in the usa involving over 100 000 patients ( financial times , july 2 , 2017 ) , some opinion leaders are now calling for a halt in the number of studies being done . 
many argue that this gold rush , which has seen most pharmaceutical companies aspiring for their own versions of is suffocating immune - targeting drugs , research , is leading to trials being done in haste without sufficient preclinical investigation , and is an inefficient use of funds spent on research and development . from a commercial perspective , the stakes are high . 
indeed , up to 50 immune checkpoint inhibitors are thought to be in development by pharmaceutical companies worldwide , but , just a small number of effective drugs in any one class are truly necessary clinically to allow healthy competition to drive down costs for patients and health systems , and to allow alternative treatments for patients developing resistance to any one drug . 
although the present level of interest in immunotherapy seems unprecedented , it is useful to remember that it is not uniquea similar bubble occurred around the potential of egfr and vegf inhibitors also leading to far too many me too versions of these drugs . 
although competition is an effective means to reach a goal quickly , too much can lead to developments delivering diminishing returns and patients losing out through inefficient use of limited resources . a fundamental problem with the current speed of development is the lack of time and research invested into understanding the reasons why a trial failed or , for that matter , why it succeeded . 
furthermore , because the reproducibility of preclinical studies and their translatable the clinic are often overestimated , findings more thorough translational research with independent validation is needed to ensure robust understanding and clinical correlation . 
the complexity of the immune system far exceeds our existing knowledge , and many of the combinatorial approaches being tested in trials are based on outmoded philosophies that were more appropriate for cytotoxic chemotherapies . 
lessons can be learned from some of the egfr and vegf inhibitor trials , which have resulted in many failures because the biology wasnt given sufficient forethought when these specific agents were combined with conventional cytotoxic drugs . a further reason for caution in the rapid pace at which immunotherapy trials are being undertaken is the nature of adverse events . 
many of the oldest trials , now with at least 5 years of follow - up , are uncovering a range of unusual side - effects that require different supportive interventions . 
these findings emphasise the importance of accruing sufficient data before launching another trial , especially if the new study combines multiple immune - targeting drugs each with unknown safety profiles . 
such findings also emphasise the need to ensure trials include many assessment criteria , such as patient - reported outcomes in addition to regular oncologic endpoints , to evaluate clinically meaningful responses . 
and finally , while tumour responses to these latest generation immune - targeted agents can be extraordinary , long - term data show that most patients still ultimately succumb to their disease ; for example , 5 - year survival in the ca184 - 024 trial in which previously untreated patients with advanced melanoma received ipilimumab plus dacarbazine was just 182% . 
 although this survival was statistically superior to the control group ( 88% for patients treated with placebo plus dacarbazine ) , it nonetheless clearly highlights that about 80% of patients treated with ipilimumab do not acheive good long - term outcomes . while heralding an enticing treatment opportunity , it is essential to bear in mind that the current generation of immunotherapies merely extends life expectancy for a small proportion of patients . 
this important observation must serve to temper the degree of offlabel use fostering false hope , and the amount of investment in this single line of investigation when other less funded research avenues , also with potential to improve cancer outcomes , remain underexploited . 
 the lancet oncology vol 18 august 2017 editorial editorial for the uk national bereavement survey 2012 see subnational - health1 / nationalbereavement - survey - voices - / 2012 / stb - - - national - bereavementsurvey - 2012.html for more on the macmillan report see macmillan.org.uk / aboutus / news / latest_news / 36 , 000cancerpatientsdenied theirlastwishtodieathome.aspx for the neuberger lcp report see government / uploads / system / uploads / attachment_data / le / 212450 / liverpool_care_ pathway.pdf for the randomised lcp study see articles lancet 2013 ; published online october 16 . 
 s0140 - 6736 ( 13 ) 61725 - 0 dignity in death : the triumph of politics over evidence with high - income countries facing ageing populations , and an increasing number of people with terminal illnesses such as cancer , the number of people dying in care settings will continue to increase . 
yet , according to the uk national bereavement survey 2012 , only 37% of relatives found the quality of care given to a deceased family member in a hospital during the end of life to be excellent or outstanding , compared with 63% of those whose relatives died at home . 
furthermore , on oct 28 , 2013 , macmillan ( a uk cancer - support charity ) estimated 36 000 patients with cancer would have preferred to die at home . 
however , despite this need , the uk government is phasing out the liverpool care pathway ( lcp ) the only set of guidelines issued for end - of - life care in general clinical practicewithout plans for any alternative . 
 the lcp was originally developed as a palliative instrument for patients with cancer by the marie curie palliative care institute liverpool ; its successful use in hospices led to its adoption in other medical settings . 
 a set of prompting guidelines , the lcp was designed to help those attending the dying consider multiple facets of care including spiritual wellbeing , pain relief , and the appropriateness of continuing to medicate for the prolongation of life . 
however , in response to media reports of harmful or negligent clinical implementation , baronness julia neuberger was commissioned in 2012 to write a report examining the wide spread use of the lcp . 
 the main critique of the lcp highlighted by the neuberger report was that where care was already substandard , poor implementation of the lcp led to more harhowever , the important question of whether or not poor care given at the end of life without the lcp would be just as damaging was not addressed . 
taken in conjunction with the reports ndings on its e ectiveness when used properly , there does not seem to be a rationale for lcps removal : it is the translation from the hospice to the hospital that has failed , not the pathway itself . 
it is these experts we need to turn to for guidance : the uk has long been at the forefront of the hospice movement , and hospices have consistently been shown to provide superior end - of - life care . 
but how can we hope to have rational debate when the palliative sectors contributions are so readily dismissed ? as a recent comment about the italian lcp study in the lancet remarked : increasingly , clinicians are asked to justify their practice against the best possible evidence . 
 and where do these debates leave the dying ? writing in the lancet oncology , nigel sykes ( st christophers hospice , london , uk ) noted recently : the lcp was meant to help non - expert sta  . 
with the withdrawal of the lcp there is now no due process for patients at the end of life , necessitating urgent evidence gathering and reasoned debate unencumbered by politicised media , lead by palliative specialists to develop more appropriate and adaptable end - of - life pathways . 
 business / 2017 / 06 / 25 / behindbig - pharmas - race - develop - nextwave - cancer - therapy / for more on the ca184 - 024 trial see j clin oncol 2015 ; 33 : 119196 for more on the reproducibility of preclinical studies see plos biol 2017 ; 15 : e2002212 calling time on the immunotherapy gold rush at the 2008 annual meeting of the american society of clinical oncology , results from an early phase trial of ipilimumab heralded a remarkable turnaround in fortunes for immunotherapyan intervention previously considered to be a dead end , limited to underwhelming outcomes with interleukin - 2 . 
results from the pivotal ca184 - 024 phase 3 trial on the same drug 3 years later proved beyond any doubt that targeting the immune system was both possible and efficacious . 
however , fastforward to 2017 , and with about 800 immunotherapy clinical trials in the usa involving over 100 000 patients ( financial times , july 2 , 2017 ) , some opinion leaders are now calling for a halt in the number of studies being done . 
many argue that this gold rush , which has seen most pharmaceutical companies aspiring for their own versions of is suffocating immune - targeting drugs , research , is leading to trials being done in haste without sufficient preclinical investigation , and is an inefficient use of funds spent on research and development . from a commercial perspective , the stakes are high . 
indeed , up to 50 immune checkpoint inhibitors are thought to be in development by pharmaceutical companies worldwide , but , just a small number of effective drugs in any one class are truly necessary clinically to allow healthy competition to drive down costs for patients and health systems , and to allow alternative treatments for patients developing resistance to any one drug . 
although the present level of interest in immunotherapy seems unprecedented , it is useful to remember that it is not uniquea similar bubble occurred around the potential of egfr and vegf inhibitors also leading to far too many me too versions of these drugs . 
although competition is an effective means to reach a goal quickly , too much can lead to developments delivering diminishing returns and patients losing out through inefficient use of limited resources . a fundamental problem with the current speed of development is the lack of time and research invested into understanding the reasons why a trial failed or , for that matter , why it succeeded . 
furthermore , because the reproducibility of preclinical studies and their translatable the clinic are often overestimated , findings more thorough translational research with independent validation is needed to ensure robust understanding and clinical correlation . 
the complexity of the immune system far exceeds our existing knowledge , and many of the combinatorial approaches being tested in trials are based on outmoded philosophies that were more appropriate for cytotoxic chemotherapies . 
lessons can be learned from some of the egfr and vegf inhibitor trials , which have resulted in many failures because the biology wasnt given sufficient forethought when these specific agents were combined with conventional cytotoxic drugs . a further reason for caution in the rapid pace at which immunotherapy trials are being undertaken is the nature of adverse events . 
many of the oldest trials , now with at least 5 years of follow - up , are uncovering a range of unusual side - effects that require different supportive interventions . 
these findings emphasise the importance of accruing sufficient data before launching another trial , especially if the new study combines multiple immune - targeting drugs each with unknown safety profiles . 
such findings also emphasise the need to ensure trials include many assessment criteria , such as patient - reported outcomes in addition to regular oncologic endpoints , to evaluate clinically meaningful responses . 
and finally , while tumour responses to these latest generation immune - targeted agents can be extraordinary , long - term data show that most patients still ultimately succumb to their disease ; for example , 5 - year survival in the ca184 - 024 trial in which previously untreated patients with advanced melanoma received ipilimumab plus dacarbazine was just 182% . 
 although this survival was statistically superior to the control group ( 88% for patients treated with placebo plus dacarbazine ) , it nonetheless clearly highlights that about 80% of patients treated with ipilimumab do not acheive good long - term outcomes . while heralding an enticing treatment opportunity , it is essential to bear in mind that the current generation of immunotherapies merely extends life expectancy for a small proportion of patients . 
this important observation must serve to temper the degree of offlabel use fostering false hope , and the amount of investment in this single line of investigation when other less funded research avenues , also with potential to improve cancer outcomes , remain underexploited . 
for example , mir - 193a - 3p edv minicells have been identified as apoptosis inducers via mcl1 silencing , with evidence of growth inhibition in mesothelioma xenografts.4 in the past few years , the range of promising molecular targets being investigated in mesotheliomaincluding gen etic or epigenetically stratified synthetic lethal approaches , 7 , 8 pd - 1 - targeted immune checkpoint blockade , 9 and mesothelin - directed antibody - directed conjugate therapy10has expanded rapidly . 
mir - 16 targomirs can be added to this growing list , each member of which has the potential to improve outcomes and transform a setting of unmet clinical need . dean fennell leicester cancer research centre , university of leicester & university hospitals of leicester , nhs trust , hodgkin building , lancaster road , leicester , le1 9hn , uk df132@le.ac.uk i have received grants from bayer and astex , personal fees from bayer , boehringer ingelheim , and msd , and have been a consultant for bms , msd , boehringer ingelheim , and roche , all of which were outside the submitted work . bueno r , stawiski ew , goldstein ld , et al . 
safety and activity of micrornaloaded minicells in patients with recurrent malignant pleural mesothelioma : a first - in - man , phase 1 , open - label , dose - escalation study . 
clinical safety and activity of pembrolizumab in patients with malignant pleural mesothelioma ( keynote - 028 ) : preliminary results from a non - randomised , open - label , phase 1b trial . 
sci transl med 2013 ; 5 : 208ra147 . geddis : insight into frontline therapy in soft tissue sarcoma gemcitabine has known activity in sarcoma ; although its exact role , indication , or best combination is still debated . 
the combination of gemcitabine and docetaxel gained favour in the usa after efficacy was noted in uterine leiomyosarcoma1 , 2 and later in sarcoma , generally with superiority over gemcitabine alone.3 however , this combination is used to a lesser extent in europe , partly due to more equivocal data in leiomyosarcoma , 4 noted efficacy of other gemcitabine - based regimens , 5 and potential issues of access as described in the geddis6 trial in the lancet oncology.6 recently , several phase 3 studies have provided substantial insight into the use of anthracyclines and alkylators as first - line treatments for patients with advanced sarcoma.79 the geddis6 trial iis the first to shed comparative light on the efficacy of gemcitabine and docetaxel versus doxorubicin alone in this setting . 
 the primary endpoint of the trialprogression - free survival at 24 weeksdid not differ between the two treatment groups ( 463% [ 95% ci 375546 ] in the doxorubicin group vs 464% [ 375548 ] in the gemcitabine and docetaxel group )  . 
the geddis trial investigators concluded that the combination should not be recommended as routine , while doxorubicin should remain standard of care , in the first - line setting for patients with advanced soft - tissue sarcoma . 
the results of the geddis trial should allow individual clinicians to determine how to position and in what clinical context to use gemcitabine and docetaxel for the care of their patients . 
 published online september 4 , 2017 s1470 - 2045 ( 17 ) 30672 - 1 see articles page 1397 vol 18 october 2017 1297 comment the main confounder in the trial is the starting dose and overall usage pattern of the combination . 
in conventional practice , gemcitabine and docetaxel is routinely administered with gemcitabine 900 mg / m2 given at a 10 mg / m per min infusion rate on days 1 and 8 and docetaxel 75 mg / m on day 8 of a 21 - day cycle . 
the docetaxel dose is lower than the 100 mg / m used in early trials to help mitigate toxicity.13 the regimen is generally considered well tolerated with predictable and manageable toxicity . 
in the geddis trial , patients received gemcitabine 675 mg / m at a 75 mg / m per min infusion rate on days 1 and 8 and docetaxel 75 mg / m on day 8 of a 21 - day cycle . 
the dose , infusion rate , and number of cycles of gemcitabine is relevant to the results and calls into question how the combination was perceived in trial design and used by investigators . 
the overall lack of grade 3 or 4 thrombocytopenia ( 0% ) in the combination group , at least compared with previous studies , 3 , 4 suggests that gemcitabine might have been underdosed and underused in geddis . 
 the proportion of patients who received the full treatment regimen ( ie , all six cycles ) of gemcitabine and docetaxel ( 39% vs 56% doxorubicin ) is also of interest , even with its lower starting dose , the need for fewer dose reductions ( 18% gemcitabine and docetaxel vs 27% doxorubicin ) , a significantly lower incidence of cytopenias , and a similar grade 34 adverse event profile . 
finally , it is curious that more patients in the combination group went on to receive doxorubicin as a second - line therapy after disease progression , whereas very few patients in the doxorubicin group went on to receive the combination ( 42% vs 13% )  . 
are these all signs of a preconceived investigator bias in this open - label study ? does the fact that the combination performed as well as it did under these circumstances suggest that it does have activity as a first - line treatment ? considering that no statistically significant benefit was noted in the proportion of patients achieving an objective response ( 19% doxorubicin vs 20% gemcitabine and docetaxel ) , progression - free survival ( hazard ratio [ hr ] 128 , 95% ci 099165 , p = 006 ) , and overall survival ( hr 114 , 95% ci 083157 , p = 041 ) , one could prudently conclude that neither regimen is superior . 
 this concept would allow clinicians to choose the regimen they feel is most appropriate for the patient based on their clinical scenario , comorbidities , performance status , and sarcoma subtype . 
it also argues for equipoise in consideration for either doxorubicin or gemcitabine and docetaxel as a first - line treatment for patients with softtissue sarcomas including leiomyosarcoma . the authors should be congratulated for not only publishing the results of this trial with such transparency and completeness , but also for having the foresight to design and the ability to perform and complete this very important trial . 
even though the outcome of the trial was negative based on pre - study statistical assumptions , the results should guide many clinicians as they practice medicine and hopefully make gemcitabine and docetaxel more widely available to patients in countries that still have issues of access . 
 william d tap memorial sloan kettering cancer institute , new york , ny 10065 , usa tapw@mskcc.org i have received personal fees from eli lilly , emd serono , novartis , eisai , janssen , immune design , adaptimmune , ariad , daiichi sankyo , plexxikon , morphotek , advaxis , and tracon , outside of the submitted work . 
additionally , i have a patent using atrx as a companion diagnostic for cdk4 inhibitors pending , and a patent for methods for drug discovery pending . the author ( s )  . 
randomized phase ii study of gemcitabine and docetaxel compared with gemcitabine alone in patients with metastatic soft tissue sarcomas : results of sarcoma alliance for research through collaboration study 002 [ corrected ]  . 
randomized multicenter and stratified phase ii study of gemcitabine alone versus gemcitabine and docetaxel in patients with metastatic or relapsed leiomyosarcomas : a federation nationale des centres de lutte contre le cancer ( fnclcc ) french sarcoma group study ( taxogem study )  . 
oncologist 2012 ; 17 : 121320 . 1298 vol 18 october 2017 comment 5 garcia - del - muro x , lpez - pousa a , maurel j , et al . 
gemcitabine and docetaxel versus doxorubicin as first - line treatment in previously untreated advanced unresectable or metastatic soft - tissue sarcomas ( geddis ) : a randomised controlled phase 3 trial . 
lancet oncol 2017 ; 18 : 1089103 . maintaining quality of life for patients with neuroendocrine tumours ideally , new treatments should either improve overall survival or the health - related quality of life ( hrqol ) of patients , or both , and should have a favourable costto - benefit ratio . 
for instance , folfirinox ( leucovorin , fluorouracil , irinotecan , and oxaliplatin ) significantly improves progression - free survival , overall survival , and hrqol compared with gemcitabine in patients with metastatic pancreatic adenocarcinoma , even though it causes substantially more side - effects.1 , 2 after publication of the radiant - 3 and radiant - 4 randomised , placebocontrolled , phase 3 studies , everolimus was approved for all non - functional , advanced , neuroendocrine tumours ( nets ) , including those of the pancreas , 3 lung , and gastrointestinal tract , 4 and sunitinib has been approved for pancreatic nets ( pnets ) .5 everolimus did not improve overall survival compared with placebo but was approved on the basis of a significant improvement versus placebo in progression - free survival.3 , 4 findings of randomised trials have not shown that progression - free survival is a good surrogate marker of long - term overall survival in nets , which could be because of the long natural history of nets , use of a cross - over design , or off - study use of the drug under investigation . 
however , ter - minassian and reported significant correlations colleagues6 have between progression - free survival and overall survival in two observational cohorts of patients receiving somatostatin analogues or everolimus . 
 in the lancet oncology , marianne pavel and colleagues report hrqol endpoints of the radiant - 4 trial , as measured by the time to definitive deterioration in total the first hypothesis score on the functional assessment of cancer therapy general ( fact - g ) questionnaire by at least 7 points.7 previously in radiant - 4 , compared with placebo , everolimus delayed disease progression in advanced lung or gastrointestinal nets.4 pavel and colleagues now report that disease progression was associated with a decline in hrqol , with a decline in fact - g total score of 491 ( 95% ci 371611 ) after disease progression . 
 however , no difference in time to definitive deterioration of hrqol between patients receiving everolimus and placebo was reported , with a median time to definitive deterioration in fact - g score of 1127 months ( 95% ci 9271935 ) with everolimus and 923 months ( 552 not estimable ) with placebo ( adjusted hazard ratio 081 , 95% ci 055121 ; p = 031 ) .7 what does this finding mean ? is that the toxic effects of everolimus are counterbalanced perfectly by its higher efficacy and potentially fewer disease - related symptoms than are reported with placebo . 
on one hand , everolimus was associated with a reduction in the risk of progression lung or gastrointestinal in patients with advanced nets.4 this benefit was noted in all subgroups , with the exception of 71 patients with ileal nets , 8 probably because these patients have less aggressive disease.9 on the other hand , and as with almost all effective drugs , everolimus causes side - effects : twice as many adverse events were reported with everolimus than with placebo ( grade 34 , 140 [ 69% ] of 205 vs 28 [ 29% ] of 97 ) , and more dose reductions or temporary treatment interruptions were noted ( 135 [ 67% ] of 202 vs 29 [ 30% ] of 98 ) .4 moreover , deaths ( four vs one ) and adverse events ( 59 [ 29% ] vs seven [ 7% ] ) were more frequently the primary reason for treatment discontinuation among those receiving published online august 21 , 2017 s1470 - 2045 ( 17 ) 30618 - 6 see articles page 1411 vol 18 october 2017 1299 comment comment published online august 15 , 2014 s1470 - 2045 ( 14 ) 70378 - x see articles page 1129 seto t , kiura k , nishio m , et al . 
ch5424802 ( ro5424802 ) for patients with alk - rearranged advanced non - small - cell lung cancer ( af - 001jp study ) : a single - arm , open - label , phase 12 study . 
safety and activity of alectinib against systemic disease and brain metastases in patients with crizotinib - resistant alk - rearranged non - small - cell lung cancer ( af - 002jg ) : results from the dosending portion of a phase 1 / 2 study . 
j clin oncol 2014 ; 32 : 141218 . ovarian tissue cryopreservation in children with cancer ovarian tissue cryopreservation is now a major part of the strategies used to preserve fertility in prepubertal children given gonadotoxic treatments for cancer . 
unlike post - pubertal patients , oocyte or embryo cryobanking is not appropriate for children and cryopreservation of ovarian tissue remains the only therapeutic option in most of the cases . 
restoration of ovarian function after reimplantation of frozenthawed mature ovarian cortex and reports of subsequent pregnancies were the basis of the rationale that guided the development of this approach in the treatment of childhood cancer . 
however , the success rate of the procedure in adult women is unknown , and the potency of cryopreserved immature gonads to restore fertility in adult survivors of childhood cancer has not yet been assessed . 
nevertheless , recent data suggest that immature ovaries are able to restore hormonal function in prepubertal children , in the same way that mature ovaries can in adults.1 , 2 additionally , immature ovaries have been used to restore fertility in experimental models.3 , 4 although the conditions of tissue harvesting , conditioning , and storing are well supervised by national biomedical and bioethical frameworks , patient selection criteria are mainly left to the discretion local multidisciplinary committees , resulting substantial heterogeneity of inclusion criteria , not only worldwide , but also within individual countries . 
 the authors retrospectively compared the occurrence of premature ovarian insu ciency over 15 years in a population - based study of children treated for cancer , who were or not o ered this procedure . 
they report that the cumulative probability of developing premature ovarian insu ciency after treatment was completed was signi cantly higher for patients o ered ovarian tissue cryopreservation than for those who were not o ered ovarian tissue cryopreservation ( 15 - year probability 35% [ 95% ci 1053 ] vs 1% [ 02 ] ; p < 00001 ; hazard ratio 568 [ 95% ci 625216 ] at 10 years ) , suggesting that the edinburgh selection criteria accurately predicted which patients would or would not develop premature ovarian insu ciency . 
although the small number of assessable patients who had successfully undergone ovarian cryopreservation ( 14 , compared with 141 assessable patients in the not - o ered group ) weakened the comparison , this is the rst report that aimed to assess selection criteria for ovarian cryopreservation in children with cancer . 
 the o er of ovarian tissue cryopreservation in the paediatric context is especially sensitive because the delay between the procedure and the potential use of the ovarian cortex could reach decades ( the median age at diagnosis for childhood cancer is about 51 years ) .6 parents are asked to plan for a future they cannot yet imagine , and , at the same time this request suggests the possibility of recovery , and so could be perceived as a message of hope . 
in this context , the selection criteria and follow - up protocol for paediatric ovarian tissue cryopreservation , as with any treatment protocol for children with cancer , should undergo evidence - based standardisation . 
in view of the small size of population of childhood cancer patients who could bene t from the procedure , national or international studies will be necessary to properly assess the validity of these selection criteria . 
because of the di erent sensitivity of gonads to toxic treatment at di erent ages , 7 and the report of spontaneous recovery of hormonal function after premature menopause as vol 15 september 2014 1049 comment published online august 15 , 2014 s1470 - 2045 ( 14 ) 70342 - 0 see articles page 1137 a result of treatment , 8 the de nition of high - risk for premature ovarian insu ciency and of premature ovarian insu ciency itself , as well as the modalities of follow - up , should be key points of discussion in a process of harmonisation . 
other means to preserve fertility , such as ovarian transposition in case of pelvic radiotherapy , 9 should also be assessed either as an alternative or as a combined approach . almost two decades have passed since the rst ovarian tissue cryopreservation was o ered to children submitted to gonadotoxic treatment . 
it should take into account the risk of reseeding cancer , which is particularly high in blood - borne cancers ( the most common types of cancer in childhood )  . 
generation of oocytes by in - vitro culture of primordial follicles to avoid this risk is an option , but such studies are still underway and clinically relevant data are not yet available.10 the indication for reimplantation is also still debated , and many authors , including wallace and colleagues , 5 recommend that the procedure be limited to fertility use only ( rejecting its use for induction of puberty , which can be done with synthetic hormonal substitution ) , because of the limited lifespan of the ovary linked to ischaemia - related follicle depletion . 
3 , 4 the nal step of a story that began many years ago for the adult survivor of childhood cancer will therefore be taken by adult specialists ( eg , assisted reproduction physicians and surgeons ) , who are not always familiar with childhood cancers . 
int j dev biol 2012 ; 56 : 90107 . dual targeting of her2 with lapatinib and trastuzumab drugs targeting her2 are central to the treatment of patients with her2 - positive breast cancer , and dual targeting of her2 with two drugs has gained much attention since 2010.1 patients with metastatic her2positive breast cancer have better overall survival when treated with docetaxel and the two anti - her2 monoclonal antibodies ( trastuzumab and pertuzumab , which bind to di erent extracellular domains of the her2 kinase ) , than do patients treated only with docetaxel and trastuzumab.2 dual targeting of her2 is also supported by neoadjuvant studies . 
in these trials , a greater proportion of patients who were treated with chemotherapy , trastuzumab , and lapatinib ( a her1 and her2 inhibitor ) , 35 or with chemotherapy , trastuzumab , and pertuzumab6 achieved pathological complete response than did those treated with chemotherapy plus trastuzumab alone . the phase 3 , three - group neoaltto trial7 is one of the key studies to assess dual targeting of her2 . 
 in neoaltto , investigators compared trastuzumab , lapatinib , and their combination as neoadjuvant and adjuvant treatment in a population of 455 patients with early her2 - positive breast cancer . 
the anti - her2directed therapies were rst administered alone for 1050 vol 15 september 2014 corrections correction to lancet oncol 2013 ; 14 : e337 correction to lancet oncol 2013 ; 14 : e436 soares m , salluh jif . 
lancet oncol 2013 ; 14 : e436in this correspondence , the authors names should read athanassios kyrgidis , thrasivoulos - george tzellos , anastasia trigoni , stefanos triaridis and their a liations as 1st department of otolaryngologyhead & neck surgery ( ak , st ) and department of clinical pharmacology ( tgt ) , aristotle university of thessaloniki , thessaloniki , greece ; hospital for skin and venereal diseases , thessaloniki , greece ( at )  . 
 these corrections have been made as of oct 28 , 2013 . vol 14 november 2013 e493 published online july 29 , 2019 s1470 - 2045 ( 19 ) 30424 - 3 see articles page 1211 for cancer today see global burden of childhood cancer : growing , but controllable there are many facets to the burden of childhood and adolescent cancer . 
in those countries , cancer is largely a disease of older adults , with well under 2% of cases diagnosed in the first 20 years of life ( data from the cancer today database )  . 
more than half a century of progress in therapy and supportive care for children with cancer has resulted in impressive gains in survival and corresponding reductions in population mortality rates in high - income countries . 
however , this success has come at the price of increased long - term morbidity and mortality among survivors compared with the general population , which must also be counted as part of the cancer burden.1 , 2 in their article in the lancet oncology , lisa force and colleagues3 estimate , for the first time , the global burden of childhood cancer in disability - adjusted life - years ( dalys ) , taking into account loss of healthy life - years to ill health and disability in addition to death . the overwhelming majority of cases of cancer in children and adolescents ( those aged younger than 20 years ) occur in low - income and middle - income countries , which thus bear a correspondingly large part of the global cancer burden for this age group.4 , 5 a notable feature of the study by force and colleagues is its stark demonstration of the absolute and relative scale of the burden in lower - resource countries and how it contrasts with that in high - income countries . 
 high and high - middle socio - demographic index ( sdi ) countries account for 35% of global childhood and adolescent cancer incidence , but only 18% of dalys , whereas low - middle and low sdi countries , with 38% of global incidence , account for 60% of dalys . 
worldwide , years of life lost represent 973% ( 95% uncertainty interval 973973 ) of dalys and years lived with disability only 27% ( 2727 ) , but the contribution of years lived with disability to total dalys ranges from almost 9% ( 99 ) in high and high - middle sdi countries to less than 1% ( 11 ) in low - middle and low sdi countries . 
force and colleagues note that their estimates probably understate the global burden of years lived with disability , and therefore of dalys , because consideration of disability was limited to the first decade after cancer diagnosis rather than the entire remainder of the life course . how can the global burden of childhood and adolescent cancer be expected to evolve in the future , and what can be done to mitigate or even reduce it ? as the population at risk increasesmainly in lowincome to middle - income countriesthe number of incident cases will also increase , and the total and proportional burden of childhood and adolescent cancer on lower - resource countries will become even larger . 
immunisation against hepatitis b where it is endemic has resulted in a reduced incidence of liver cancer , 6 but most of the effect will be seen in adults , and liver cancer accounts for less than 2% of the global burden of childhood and adolescent cancer . 
in sub - saharan africa , the waning of the hiv epidemic should lead to a reduction in kaposi sarcoma and progress against malaria could reduce the burden of burkitts lymphoma . 
the only feasible target was neuroblastoma , but screening led to overdiagnosis of cases that would have regressed without symptoms and had no effect on mortality from the more aggressive forms of this cancer.7 earlier diagnosis through greater public and clinical awareness could bring a short - term rise in global burden for children and adolescents because fewer cancers with onset before the age of 20 years would actually be diagnosed after that age ; this change would particularly affect cancers that can have a relatively protracted natural history , such as hodgkin lymphoma and thyroid carcinoma . 
although gains from early diagnosis should be greatest in lower - resource countries , where too many cases are diagnosed at a late stage , they should be felt even in affluent countries , notably for people with low - grade brain tumours , survivors of which bear a considerable burden of disability.8 for the benefits of early diagnosis to be fully realised worldwide , 1184 vol 20 september 201 comment it must be accompanied by improved diagnostic and treatment facilities with universal access . 
international collaboration will be an essential component of the necessary capacity building.9 it is to be hoped that the present study will help to stimulate the necessary improvements , and future iterations can monitor their success . charles a stiller national cancer registration and analysis service , public health england , london se1 8ug , uk charles.stiller@phe.gov.uk i declare no competing interests . 
the author alone is responsible for the views expressed in this comment and they do not necessarily represent the decisions , policy , or views of public health england . copyright 2019 the author ( s )  . 
a new clinical guideline from the royal college of paediatrics and child health with a national awareness campaign accelerates brain tumor diagnosis in uk childrenheadsmart : be brain tumour aware . 
 pediatr blood cancer 2016 ; 63 : 38791 . overcoming endocrine resistance in neoadjuvant endocrine therapy for early breast cancer endocrine therapy is the mainstay of treatment for oestrogen receptor - positive breast cancer , now classified as either the luminal a ( her2 - negative with low levels of ki67 ) or luminal b ( her2 positive or negative , with high levels of ki67 ) phenotype . 
historically , endocrine therapy has included the approach of targeting the oestrogen receptor itself , either by means of selective oestrogen receptor modulators such as tamoxifen , or fulvestrant , a selective oestrogen receptor degrader . 
this is the mode of action of aromatase inhibitors , which block the aromatase enzyme and lower oestrogen levels in postmenopausal women ; whereas in premenopausal women , luteinising hormone - releasing hormone agonists reduce oestrogen production in the ovaries by interacting via the regulatory axis from the pituitary gland to the ovary . 
since the 1990s , data have suggested that aromatase inhibitors might be the optimal neoadjuvant endocrine therapy treatment approach in postmenopausal women with breast cancer , resulting in better overall responses , improved increased pathological breast conservation at surgery.1 more empirically , a responses , and complete 3 - month period for neoadjuvant endocrine therapy was introduced as the standard of care in postmenopausal women with breast cancer in the mid - 1990s . 
however , compared with neoadjuvant chemotherapy , neoadjuvant endocrine therapy has always yielded inferior results in terms of pathological complete responses.2 once in the metastatic breast cancer setting , combinations of endocrine therapy plus mtor inhibitors or cdk4 / 6 inhibitors instantly changed the standard treatment approach . 
however , resistance and disease progression while on treatment have occurred in both the adjuvant and metastatic settings.3 introduced apart from oestrogen expression , receptor levels , and to some extent a decrease in ki67 levels , no biomarker has been identified as a prognostic marker for the benefit of neoadjuvant endocrine therapy . 
the phosphatidylinositol 3 - kinase ( pi3k ) pathway is frequently altered in oestrogen receptor - positive breast cancer and has been implicated in resistance to endocrine therapies.4 furthermore , pik3ca , which encodes the pi3k p110 isoform , is mutated in approximately 40% of oestrogen receptor - positive breast cancers.5 oestrogen - independent breast cancer cell growth can be inhibited by adding pi3k inhibitors to anti - oestrogens . 
 published online august 8 , 2019 s1470 - 2045 ( 19 ) 30500 - 5 see articles page 1226 vol 20 september 201 9 1185 comment guidelines , and the country - specific covid - 19 case burden will dictate our actions , most likely negatively . in west africa , covid - 19 protocols are defined by individual institutions . 
patients with a fever are referred to the emergency roo a minimum number of essential staff ( in protective gear when available ) will be rotated , prescriptions refilled remotely , and second - line and third - line palliative chemotherapy halted . 
of particular concern is the large population infected by hiv , which includes approximately 8 million people.6 while public hospitals prepare for the first wave of covid - 19 patients , oncology services at this point are still aiming to deliver full service when follow - up outpatient services possible , although have been severely curtailed . 
staff will be divided into teams consisting of core personnel . in sudan , despite the low covid - 19 burden , cancer centres have established a contingency plan by deferring new referrals except for emergency surgery , non - urgent intravenous cases . 
 medical teams and core support staff work as divided teams after having attended mandatory covid - 19 training sessions . oncologists in africa , in the absence of centralised and resource - appropriate covid - 19 guidelines , are pragmatically safeguarding patients and the workforce while providing essential cancer care . 
korle bu teaching hospital , accra gqqf + 6r , ghana ( vv ) ; the national cancer institute , university of gezira , wad madani , sudan ( mmae ) ; and stellenbosch university , stellenbosch , south africa ( hs ) yu j , ouyang w , chua mlk , xie c . 
countries / southafrica ( accessed march 29 , 2020 )  . the uk coronavirus cancer monitoring project : protecting patients with cancer in the era of covid - 19 published online april 15 , 2020 s1470 - 2045 ( 20 ) 30230 - 8 the uk coronavirus cancer monitoring project ( ukccmp ) aims to collect , analyse , and disseminate in real time data from the uk cancer centres about severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection rates in patients with cancer , and their outcomes in terms of coronavirus disease 2019 ( covid - 19 )  . 
this approach will enable oncologists to gain crucial insights to inform decision making . 622 vol 21 may 2020 comment s for more on the uk coronavirus cancer monitoring project see ukcoronaviruscancermonitoring . identified in december , 2019 , several cases of acute respiratory syndrome in hubei province , china were identified ; these were the first described cases of covid - 19 . 
 the causative virus , sars - cov - 2 , is a new strain of betacoronavirus previously not humans and thought to be of zoonotic origin.1 the presentation of covid - 19 varies from no or minor symptoms akin to the common cold , to severe acute respiratory distress syndrome , resulting in severely impaired respiratory function.1 sars - cov - 2 is highly contagious through direct transfer of respiratory droplets during coughing and sneezing or indirect fomite spread via contaminated surfaces.2 this simple transmission , coupled with international travel , has enabled rapid spread of the virus with more than 870 000 cases and 43 000 deaths reported worldwide as of april 1 , 2020.3 approximately 25 million individuals live with , or have a history of , cancer in the uk , with 1000 new diagnoses each day.4 of these patients , a substantial proportion require , are undergoing , or are recovering from surgery and complex treatments . 
patients with cancer potentially have increased susceptibility to sars - cov - 2 infection and have more serious sequelae , resulting from impaired immune function due to cancer itself , cancer treatment , or both.5 , 6 wenhua liang and colleagues6 reported their identification of 18 patients with cancer in a cohort of 1590 patients with covid - 19 in china , indicating an increased incidence of covid - 19 in patients with cancer compared with the general chinese population ( 113% vs 029% )  . 
the incidence of covid - 19 in patients with cancer ( 12 [ 079% ] of 1524 patients ) was higher than in the general wuhan population ( 037% )  . patients with specific types of cancer might be at an increased risk of covid - 19 , with both these reports highlighting the high proportion of patients with lung cancer with confirmed diagnoses of covid - 19 ( five of 18 patients in liang et al , 6 and seven of 12 in yu et al7 )  . 
severe infection with sars - cov - 2 is associated with cytokine storm and increased concentrations of c - reactive protein and il - 6 pneumonitis , severe adverse events that are also lymphocyte associated with immune checkpoint inhibitor therapy.8 consequently , patients on immunotherapy could be at increased risk from covid - 19 . 
therefore , sars - cov - 2 inflammatory infection is highly unlikely to affect all patients with cancer equally . little effect on populations , the european society of medical oncology has published guidelines on how to mitigate the effect of covid - 19 on patients with cancer , by prioritisation of cancer treatment in patients expected to derive a substantial absolute survival benefit , reducing hospital visits , and converting from intravenous to oral regimens.9 however , these guidelines take a broad approach for a very heterogenous population . 
policies , including self - isolation and social distancing , are widely acknowledged to be required to suppress viral spread , both in the general and at - risk populations , thereby reducing pressure on already stretched healthreallocation care of resources away from cancer care services could potentially have unintended cancer - related implications , including increased morbidity and mortality . 
a local emergency response reporting group has been created at each uk cancer centre to ensure continued updating of the ukccmp live clinical data dissemination systethe project will collect data on patients with cancer who are positive for sars - cov - 2 infection , including tumour type and stage , patient age , present cancer treatment , and clinical outcomes , with the aim to enable oncologists to gain crucial insights to inform decision making . 
 data collection , analysis , and dissemination coordinated by the centre for computational biology at the university of birmingham , ( birmingham , uk ) through a dedicated workflow hosted by the compute and storage for life science infrastructure as part of vol 21 may 2020 comment the birmingham environment for academic research local cloud.10 ukccmp delivers meaningful real - time data to all uk cancer centres and clinicians to allow more personalised approaches to individual patient care and inform clinical decision making . 
this initiative will improve cancer care in the uk and beyond at this time of unprecedented global turmoil and reliance on health - care resources . we declare no other competing interests . 
the university of birmingham initiated this process , with the pro - vice - chancellor dedicating the computational and human resources of the universitys centre for computational biology , the institute of translational medicine , and scientists from the institute of cancer and genomic sciences . 
other academic institutions dedicating time and staff to the project include the university of oxford , university of leeds , university college london , edinburgh cancer centre , clatterbridge cancer centre , and kings college london . the uk coronavirus cancer monitoring project team lennard.lee@nhs.net huang c , wang y , li x , et al . 
 joint - mission - on - covid - 19 - final - report.pdf ( accessed april 9 , 2020 )  . coronavirus covid - 19 global cases by the center for systems science and engineering at johns hopkins university ( jhu )  . 
castles ( compute and storage for the life sciences ) : a collection of compute and storage resources for supporting research at the university of birminghabirmingham : birmingham environment for academic research , june 20 , 2019 . 
 ( accessed april 7 , 2020 )  . recommendations from national regulatory agencies for ongoing cancer trials during the covid - 19 pandemic clinical research has transformed cancer care and is often integrated seamlessly into routine oncology clinics , offering eligible patients additional treatment options or lines of therapy . 
typically , and particularly for diseases with poor prognoses or when trials entail biomarker - directed personalised treatment , clinical trial enrolment can be preferred ( by both doctors and patients ) over standard care.1 however , many barriers already preclude patients participation in clinical trials , with only a small proportion enrolled in interventional trials.2 the coronavirus disease 2019 ( covid - 19 ) pandemic presents an additional major barrier to patients enrolment and ongoing participation in clinical trials . 
institutions are adapting their oncology practice , considering alternative treat ment strategies to appropriately balance risks and benefits , despite the absolute individual risk increases from covid - 19 for patients being currently unknown.3 the us food and drug administration ( fda ) and other international bodies have released guidance for sponsors and study sites to ensure the safety of trial participants while maintaining compliance with good clinical practice and minimising risks to study integrity . 
this guidance is summarised in the panel.410 although this guidance is very welcome and helpful , specific considerations must be made for each trial , in view of the wide variety of study types , relative complexities , and perceived risks and benefits . 
many study sites and sponsors have already stopped study enrolment , and it is not clear when these studies will reopen because of the probable prolonged effects of the covid - 19 pandemic . 
for patients on study treatment , the difficult decision to stop or carry on with the investigational medical product or other study treatments should be discussed between see online for appendix members of the uk coronavirus cancer monitoring project team are listed in the appendix ( p 1 )  . 
a worldwide collaboration to harmonize guidelines for the long - term follow - up of childhood and young adult cancer survivors : a report from the international late effects of childhood cancer guideline harmonization group . 
eur j cancer 2007 ; 43 : 1778 - 80 . interrogating molecular data for medulloblastoma risk stratification medulloblastoma is the most common malignant paediatric brain tumour , with an incidence between 234 and 596 per million population.1 early studies on medulloblastoma biology were largely inconclusive because of its molecular heterogeneity and the small size of the cohorts analysed . 
 indeed , on the basis of gene expression , genetic aberrations , and dna methylation , medulloblastoma is now classified into several molecular subgroups.25 the 2016 who classification of tumors of the central nervous system6 combines molecular and histological features for an innovative integrated diagnosis , thus allowing stratification of patients into four prognostic risk categories : favourable , standard , high , and very high risk.3 heterogeneous , comprising 5060% of patients with medulloblastoma and encompassing shh - activated tp53wild - type and groups 3 and 4 , in the absence of highrisk features ( ie , myc amplification , anaplastic histology , or metastasis at diagnosis )  . 
 micrornas and long non - coding rnas have been shown to be important regulators of medulloblastoma biology , and could represent valuable biomarkers for risk stratification and targeted therapy.10 in conclusion , this study8 provides a tool for immediate clinical application . 
although these results require validation in a controlled multicentre study , they set the foundation that is needed to improve genomic patient characterisation for more accurate risk stratification in routine clinical settings . * elisabetta ferretti , agnese po department of experimental medicine ( ef ) and department of molecular medicine ( ap ) , sapienza university of rome , rome 00161 , italy ; and irccs neuromed mediterranean neurological institute , pozzilli , italy ( ef ) elisabetta.ferretti@uniroma1.it we declare no competing interests . copyright 2018 the author ( s )  . 
nearly half of patients at diagnosis have metastases , with a 5 - year overall survival of only 50% , despite therapeutic advances.1 initial improvements to outcome were achieved by the introduction of consolidation with myeloablative chemotherapy and autologous haemopoietic stemisotretinoin , a cell transplantation , followed by targeted therapy with differentiating agent used to treat minimal residual disease.2 next , anti - glycolipid disialoganglioside ( gd2 ) monoclonal antibodies was tested in resistant tumours . 
gd2 is highly expressed on the surface of neuroblastoma cells , with normal tissue expression restricted to neurons , sensory nerve fibres , and melanocytes , thus creating an attractive target for published online november 12 , 2018 s1470 - 2045 ( 18 ) 30627 - 2 see articles page 1617 vol 19 december 2018 1549 comment editorial see review page e321 for more on the childhood cancer survivor study see for the long - term health outcomes for childhood cancer survivors see jama 2013 ; 309 : 237181 for the childhood oncology group survivorship guidelines see survivorshipguidelines.org / for the study on mri monitoring of heart disease see j cardiovasc magn reson 2013 ; 15 : 48 for more on depression and anxiety in long - term cancer survivors see articles page 721 for more on improving cancer care for children and young people see thelancet.com / series / childhoodcancer it doesnt stop at cure : monitoring childhood cancer survivors on june 1213 , 2013 , the investigators of the childhood cancer survivors study met for their annual meeting in memphis , tn , usa . 
 the study included more than 1700 adults , with a median time from diagnosis of childhood cancer of 25 years , and showed that almost all participants had at least one chronic disease , including abnormal lung function , heart disease , and secondary malignancies . 
the investigators concluded that their ndings highlight the importance of monitoring survivors of childhood cancer for long - term health problems , but are current health systems and care pathways t for this purpose ? treatment in paediatric oncology has improved remarkably over the past half century . 
but , although measures are being taken to reduce long - term health risks at treatment stage , with less aggressive chemotherapy regimens and careful use of radiotherapy , there will probably always be some price to pay for cancer treatment . 
robust and regular monitoring of survivors could do much to help lessen the additional social , economic , and health burdens that many will face in the years after their treatment . 
 although there are initiatives taken to ensure survivors of childhood cancer are monitored and o ered support , these are generally institutional and regional e orts , with much of the onus put on the patient to use the resources provided , rather than health - care systems o ering them proactive support . 
the childhood oncology group have published a series of guidelines for clinicians who provide ongoing health care to survivors of childhood cancer , and recommends at least annual follow - up checks covering a range of conditions , such as growth , fertility , and secondary malignancies . 
although this is a start , there are two clear areas where monitoring of childhood cancer survivors could be improved . first , robust methods for monitoring should be developed , to ensure that medical interventions can be provided as early as possible . 
 furthermore , personalised screening programmes , such a breast - cancer screening for children who received chest irradiation , would be of further help to identify secondary malignancies early . regular second , improvements can be made receive in ensuring patients follow - up appointments . 
 although this seems obvious , as childhood cancer survivors grow up and move on with their lives , it may not be as straightforward as visiting a family doctor once a year . 
standardised record keeping and an easy way for survivors to be in control of their medical records , or improved mechanisms of ensuring records follow patients as they move from one health - care jurisdiction to another , can help prevent gaps in care over the years after cure . 
the establishment of specialist late - e ects clinics as part of a national cancer plan can also help to ensure regular monitoring is available no matter where a childhood cancer survivor ends up . 
furthermore , such clinics could ensure that those who are monitoring the survivors are highly trained and aware of the health risks that might a ect cancer survivors . besides monitoring the physical wellbeing of childhood cancer survivors , it is also important that their mental health is also attended to . 
 personalised , web - accessible survivorship programmes may o er a way to aid in this respect , allowing an easy way to document emotions and struggles on a regular basis , rather than as a single snapshot at an annual appointment . childhood cancer survivors are at long - term risk of substantial adverse events . 
follow - up should be centred on the individual , and information should be provided to survivors to help them understand how regular checkups can improve their long - term wellbeing and quality of life . 
 the lancet oncology vol 14 july 2013 published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
 n a d o f a r a g e n e k u l k a r n i firadenovec : a new gold standard for bcg - unresponsive bladder cancer ? lancet oncol 2021 ; 22 : 89in this comment , the declaration of interests statement was incorrect and should have read as follows : i report personal fees from merck , ferring , biosyent , tersera , abbvie , roche , theralase , and janssen , outside the submitted work . 
 this correction has been made to the online version as of dec 30 , 2020 , and the printed version is correct . maringe c , spicer j , morris m , et al . 
 the impact of the covid - 19 pandemic on cancer deaths due to delays in diagnosis in england , uk : a national , population - based , modelling study . 
lancet oncol 2020 ; 21 : 154950in this comment , on the second and eleventh lines of paragraph two , the drug name has been corrected to gx - 188e . 
durvalumab alone and durvalumab plus tremelimumab versus chemotherapy in previously untreated locally patients with unresectable , advanced or metastatic urothelial carcinoma ( danube ) : a randomised , open - label , multicentre , phase 3 trial . 
 lancet oncol 2020 ; 21 : 157488 in this article , the affiliation for ignacio duran should have been hospital universitario virgen del roco , seville , spathis correction has been made to the online version as of dec 30 , 2020 . correction to lancet oncol 2020 ; 21 : 160210 pm , welt ens poortmans fortpied c , et al . 
internal mammary and medial supraclavicular lymph node chain irradiation in stage iiii breast cancer ( eortc 22922 / 10925 ) : 15 - year results of a randomised , phase 3 trial . 
 lancet oncol 2020 ; 21 : 160210 in this article , the funders of the study should have been ligue nationale contre le cancer and kwf kankerbestrijding in the funding and acknowledgments sections . 
this correction has been made to the online version as of dec 30 , 20202 . vol 22 january 2021 corrections chemoradiotherapy with or without cetuximab in patients with oesophageal cancer ( scope1 ) : a multicentre , phase 2 / 3 randomised trial thomas crosby * , christopher n hurt * , stephen falk , simon gollins , somnath mukherjee , john sta urth , ruby ray , nadim bashir , john a bridgewater , j ian geh , david cunningham , jane blazeby , rajarshi roy , tim maughan , gareth gri ths summary background de nitive chemoradiotherapy ( crt ) is an alternative to surgery for the curative treatment of oesophageal carcinoma . 
the scope1 trial aimed to investigate the addition of cetuximab to cisplatin and uoropyrimidine - based de nitive crt in patients with localised oesophageal squamous - cell cancer and adenocarcinomas to assess activity , safety , and feasibility of use . methods in this multicentre , randomised , open - label , phase 2 / 3 trial , we recruited patients aged 18 years and older from uk radiotherapy centres who had non - metastatic , histologically con rmed carcinoma of the oesophagus ( adenocarcinoma , squamous - cell , or undi erentiated ; who status 01 ; stage iiii disease ) and been selected to receive de nitive crt . 
patients were randomly assigned ( 1 : 1 ) via a central computerised system using strati ed minimisation ( with an 80 : 20 random element ) to receive crt alone or crt with cetuximab ( 400 mg / m on day 1 followed by 250 mg / m weekly ) , strati ed by recruiting hospital , primary reason for not having surgery , tumour histology , and tumour stage . 
crt consisted of cisplatin 60 mg / m ( day 1 ) and capecitabine 625 mg / m twice daily ( days 121 ) for four cycles ; cycles three and four were given concurrently with 50 gy in 25 fractions of radiotherapy . 
 the primary endpoint was the proportion of patients who were treatment failure free at week 24 for the phase 2 trial and overall survival for the phase 3 trial , both measured from randomisation . 
 this trial is an international standard randomised controlled trial , number 47718479 . findings 258 patients ( 129 assigned to each treatment group ) from 36 uk centres were recruited between feb 7 , 2008 , and feb 22 , 2012 . 
recruitment was stopped without continuation to phase 3 because the trial met criteria for futility , but we continued to follow - up recruited patients until all had reached at least 24 - week follow - up ( median follow - up of patients who survived was 168 months [ iqr 112245 ] )  . 
fewer patients were treatment failure free at 24 weeks in the crt plus cetuximab group ( 79 of 119 patients [ 664% , 90% ci 586736 ] ) than in the crt only group ( 93 of 121 patients [ 769% , 697830 ] )  . 
the crt plus cetuximab group also had shorter median overall survival ( 221 months [ 95% ci 151245 ] vs 254 months [ 205379 ] ; adjusted hr 153 [ 95% ci 103227 ] ; p = 0035 )  . 
patients who received crt plus cetuximab had more non - haematological grade 3 or 4 toxicities ( 102 [ 79% ] of 129 patients vs 81 [ 63% ] of 129 patients ; p = 0004 )  . 
less often , patients or clinicians will opt for this strategy.8 increasingly , de nitive chemoradiotherapy is being considered as a standard of care in patients with oesophageal because evidence suggests that outcomes are similar to those of surgical treatment.3 , 6 , 9 by contrast , for adenocarcinomas , de nitive evi dence chemoradiotherapy is less strong and is restricted to studies of chemo radiotherapy in patients who are unsuitable for surgery . squamous - cell carcinoma , the use support concurrent chemoradiotherapy regimens have been based on cisplatin and uorouracil . 
both drugs have good single - agent activity in oesophageal malignant disease and are two of the best radiosensitisers in tumour models.10 , 11 the regimen used most frequently in the uk consists of conformal external beam radio therapy ( 50 gy in 25 fractions for 5 weeks ) with two cycles of cisplatin and uorouracil given concurrently , with or without a further two cycles of the same chemo therapy , given in a neoadjuvant phase . 
this neoadjuvant phase , as well as delivering additional systemic therapy , allows time for careful radiotherapy planning , frequently improves patients dysphagia , and debulks the tumour before radiotherapy . 
capecitabine has been shown to be as e ective as uorouracil in locally advanced and metastatic oesophagogastric cancer.7 encouraging outcomes with de nitive chemoradiotherapy regimens were reported in single - centre series , 8 , 12 but whether the ndings could be replicated in a prospective , multicentre trial was unclear . although de nitive chemoradiotherapy in patients with a poor outlook can lead to useful long - term disease control , most patients still succumb to the disease . 
the pattern of treatment failure di ers from that after surgery , with a higher rate of locoregional recurrence.6 , 8 , 9 , 12 improvements to both the systemic and locoregional components of this treatment strategy are therefore urgently needed . egfr is overexpressed in up to 55% of oesophagogastric cancers and is associated with poor prognosis.13 cetuximab , a monoclonal egfr antagonist , improved outcomes when given in combination with chemo therapy tumourseg , advanced colorectal adenoin other carcinomas14 and squamous - cell head and neck cancer.15 more importantly , preclinical studies have shown that cetuximab can overcome an important mechanism of radioresistance , 16 and results of a phase 3 trial by bonner and colleagues17 in squamous - cell carcinoma of the head and neck showed that cetuximab in combination with radiotherapy can improve local control and overall survival compared with therefore postulated that cetuximab in combination with conventional de nitive chemoradiotherapy might improve radiotherapy alone . 
on behalf of the uk national cancer research institute ( ncri ) upper gi clinical studies group we designed ( study of chemoradiotherapy in oesophageal cancer with erbitux ) to test this hypothesis . 
 the scope1 trial methods study design and patients in this multicentre , randomised , open - label , parallel , two - arm , phase 2 / 3 trial , we recruited patients from radiotherapy centres in the uk who had the following key eligibility criteria ( for full inclusion and exclusion criteria see appendix ) : non - metastatic , histologically con rmed carcinoma of the oesophagus ( adenocarcinoma , squamous - cell , or undi erentiated carcinoma ) or gastro - oesophageal junction ( siewert type 1 or 2 with < 2 cm extension into the stomach ) ; selected for de nitive chemoradiotherapy by a designated multidisciplinary team ; aged 18 years or older ; who performance status 0 or 1 ; stage iiii disease ( tnm stage 6 ) ; and disease length of less than 10 cm de ned by endoscopic ultrasound . 
the protocol for the study has been published elsewhere18 and the trial was coordinated by the wales cancer trials unit ( wctu )  . patients were required to have staging investigations that consisted of endoscopic ultrasound and contrastenhanced spiral ct scan of the thorax and abdomen . 
 patients were physiologically assessed to identify those with eligible lung function ( forced expiratory volume in 1 s > 10 ) , cardiac function ( left ventricular ejection fraction > 40% on echocardiogram or multigated acquisition scan ) , renal function ( edta glomerular ltration rate [ gfr ] > 40 ml / min , or estimated by cockcroft - gault formula to be > 60 ml / min ) , ( serum bilirubin liver function 15upper limit of normal [ uln ] , aspartate aminotransferase to alanine aminotransferase ratio 25uln , alkaline phosphatase 3uln ) and haematological assessment ( haemoglobin > 100 g / l , white blood cells > 310 / l , absolute neutrophil count [ anc ] > 1510 / l , platelet count > 10010 / l )  . 
all treatment and assessments were done in uk radiotherapy centres . all patients had to provide written informed consent before registration and the trial protocol was approved the uk medicines and healthcare products regulatory agency and a multicentre research ethics committee . 
cancer research uks clinical trials awards and advisory committee ( ctaac ) approved the trial design . 628 vol 14 june 2013 articles for the trial protocol see php ? trial = scope1 randomisation and masking eligible patients were randomly assigned ( 1 : 1 ) to chemoradiotherapy with cetuximab ( crt plus cetuximab ) or chemoradiotherapy without cetuximab ( crt only ) by strati ed minimisation with a random element ( 80 : 20 )  . 
to conceal the sequence until interventions were assigned , research nurses ( who recruited the patients ) telephoned the wctu where the random allocation sequence was generated by a trial or data manager interacting with a computerised syste the study had an open - label design . 
participants , those administering the interventions , and those assessing the outcomes were aware of which treatment had been allocated . procedures both study groups received the same chemotherapy , which consisted of four 3 - weekly cycles of cisplatin ( 60 mg / m intravenously on day 1 ) and capecitabine ( 625 mg / m orally twice daily from day 1 to day 21 ) ; cycles one and two were given as neoadjuvant treatment . 
patients randomly assigned to the crt plus cetuximab group also received intravenous cetuximab 400 mg / m on day 1 of chemotherapy and 250 mg / m weekly for the 12 weeks of treatment . 
if patients were unable to swallow capecitabine , investi gators could use a protracted intravenous infusion of uorouracil at a rate of 225 mg / m per day from day 1 to day 21 of each cycle . 
 full details of protocol treatment and dose reductions are detailed in the trial protocol . dose modi cation for haematological toxicity was based on a full blood counts taken within the 3 days before the start of each cycle of chemotherapy . 
for anc 0510 / l to less than 110 / l or a platelet count 5010 / l to less than 7510 / l , chemotherapy was stopped until recovery of counts and restarted with a 25% dose reduction of cisplatin and capecitabine . 
 cisplatin was given at a 75% dose reduction to patients with gfr of 4050 ml / min , and replaced by carboplatin ( at a concentration to achieve an area under the concentrationtime curve of 5 ) if gfr was below 40 ml / m capecitabine was given at a 75% dose reduction if gfr was below 50 ml / min , a 50% dose reduction if gfr was below 40 ml / min , and omitted if gfr was below 30 ml / m for other non - haematological toxicities of grade 2 or higher , chemotherapy was withheld until resolution to grade 01 . 
sequential dose reduction of cetuximab to 200 mg / m and 150 mg / m was advised for second and third occurrences of grade 3 skin rash , respectively ; it was permanently discontinued after a fourth appearance . the radiotherapy protocol and planning guidance document mandated the use of intravenous contrast ct simulation with minimum 3 - mm ct slices . 
50 gy in 25 fractions , prescribed according to recommendations by the inter national commission on radiation units and measure ments ( icru - 50 / 62 ) , was delivered monday to friday as a three - dimensional ( 3d ) conformally planned single - phase treatment , usually with four radiotherapy elds to achieve the following normal organ dose constraints : less than 30% of the heart volume to receive at least 40 gy , less than 25% of the lung volume to receive at least 20 gy , and a maximum dose in the spinal cord of less than 40 gy . 
elective nodal irradiation was not done . all potential principal investigators and radiotherapy centres received a cd - rom containing the detailed radio therapy planning radiotherapy protocol , guidance document , and example planning cases . 
all principal investigators had to outline a benchmark case 540 patients were assessed for eligibility 282 excluded 213 did not meet inclusion criteria 66 refused 3 other reasons 258 were randomly assigned 129 were assigned to chemoradiotherapy plus cetuximab 129 assigned to chemoradiotherapy only figure 1 : trial pro le vol 14 june 2013 articles radiotherapy and radiotherapy centres then planned the same case , which had to pass central review before patient recruitment.19 on - trial trials quality assurance ( rttqa ) consisted of all principal investigators rst plans , 10% of all subsequent plans , and trial - speci c planning assessment forms for each patient submitted for central review that outlined and assessed the 3d dose distribution before treatment . 
blood and biopsy samples were obtained at both baseline and week 24 , but the processing of these samples is still in progress , and correlations with treatment response will be the subject of a future paper . follow - up was at 24 weeks , then every 3 months after that during the rst year , every 4 months during the second year , and yearly thereafter for a minimum of 5 years from randomisation . 
we postulated that scores for physical and role function , fatigue , dysphagia , and eating restrictions would be better over time in the crt plus cetuximab group than in the crt only group . 
 a patient was deemed treatment failure free if they were still alive with no evidence of residual malignancy in the endoscopic biopsy sample , and no evidence of disease progression outside the radiotherapy eld on ct scan . 
using a flemings single - stage design ( p1 = 060 ; p2 = 075 ; = 005 ; 90% power ; 10% loss to follow up ) , we needed to recruit 90 patients in the crt plus cetuximab group ( 180 patients overall )  . 
subject to the independent data monitoring committees review of the phase 2 analysis , the study would proceed to phase 3 with a primary endpoint of overall survival from date of randomisation . 
for the phase 3 trial , we needed to recruit 420 patients ( 269 events ) to detect an improvement in 2 - year overall survival from 35% to 475% ( hazard ratio [ hr ] 071 ) in patients assigned to crt plus cetuximab , with 80% power at 5% signi cance . data were analysed with the stata 11 statistical package according to intention to treat . 
analyses of the proportion of patients who were treatment failure free were done using the number of patients who died or progressed before 24 weeks , or those with a valid 24 - week assess ment , as the denominator . 
detailed quality - of - life analyses , health economic analyses , and correl ation of outcomes with radiotherapy treatment delivery will be presented in future reports . this trial is an international standard randomised controlled trial , number 47718479 . role of funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the statistician ( ch ) had full access to all the data and the corresponding author ( tc ) and statistician ( ch ) had nal responsibility for the decision to submit for publication . 
merck serono provided the cetuximab free of charge but had no role in study design , data collection , data analysis , data interpretation or writing of the report . results 258 patients were recruited from 36 of the 56 radiotherapy centres in the uk between feb 7 , 2008 , and feb 22 , 2012 ( gure 1 )  . 
in february , 2012 , the independent data monitoring committee undertook a preplanned analysis of the rst 180 patients recruited who had completed 24 weeks of follow up , and recommended stopping recruitment because the trial had met predetermined criteria for futility . 
when making this decision , they also took into account toxicity , treatment compliance , and overall survival , and recommended completion of treatment and follow - up of all recruited patients . 
the data presented here are those from all 258 patients ( 129 patients allocated to each treatment group ) who were recruited up until the independent data monitoring committees decision , analysed after the last patient had undergone assessment at week 24 . 
the median length of follow - up for patients who had survived by the time of analysis was 168 months ( iqr 112245 )  . patient and tumour baseline characteristics were well balanced between groups ( table 1 )  . 
patients who were assigned to receive crt plus cetuximab were less likely to com plete standard protocol treatment than were those assigned to the crt only group ( table 2 )  . 
the com pliance di erence between groups was signi cant for completion ( at full or reduced dose ) of four planned cycles of cisplatin ( p = 0005 ) , completion of four cycles of capecitabine ( p = 0002 ) , and delivery of any radiotherapy ( 104 [ 81% ] of 129 patients in the crt plus cetuximab group vs 119 [ 92% ] of 129 patients in the crt only group ; p = 0006 ; table 2 )  . 
 the number of patients whose cisplatin dose was reduced ( or stopped ) was similar in each group ( 56 [ 43% ] in the crt plus cetuximab group vs 60 ( 47% ) in the crt only group )  . 
the number of patients whose capecitabine dose was reduced was higher in the crt plus cetuximab group than in the crt only group ( 97 [ 75% ] vs 85 [ 66% ] )  . 
 more patients in the crt plus cetuximab group stopped both cisplatin and capecitabine treatment early because 632 vol 14 june 2013 articles crt plus cetuximab crt only of toxicity or illness than did those in the crt only group ( cisplatin stopped , 26 [ 20% ] vs 12 [ 9% ] ; capecitabine stopped , 36 [ 28% ] vs 19 [ 15% ] )  . all ctcae grade 3 or 4 toxicities ( including serious adverse reactions and suspected unexpected serious adverse reactions ) reported during treatment are shown in table 3 . 
these toxicities were mainly dermatological , biochemical ( metabolic or laboratory tests ) , and cardiac disorders ( table 3 )  . the proportion of patients who were treatment failure free at 24 weeks was lower in the crt plus cetuximab group than in the crt only group ( 79 of 119 patients [ 664% , 90% ci 586736 ] vs 93 of 121 patients [ 769% , 697830 ] )  . 
patients who were failure free at 24 weeks had signi cantly better median overall survival than did those who were not failure free ( 83 months [ 95% ci 67125 ] vs 267 months [ 245427 ] )  . 
of those patients who were failure free at 24 weeks , 107 ( 62% ) of 172 were still alive without progression at the end of the study follow - up , whereas 40 ( 23% ) were alive with progression and 25 ( 15% ) had died . 
of patients who died before 24 weeks , more were recorded as having oesophageal cancer as the cause of death in the crt plus cetuximab group than in the crt only group ( table 4 )  . 
29 patients are known to have had further treatment during the 12 months after randomisation ( table 4 )  . overall survival was signi cantly worse in the crt plus cetuximab group than in the crt only group ( unadjusted hr 145 [ 95% ci 101209 ] , log - rank p = 0043 ; adjusted hr 153 [ 103227 ] , p = 0035 ; gure 2 )  . 
2 - year overall sur vival was also lower in the crt plus cetuximab group than in the crt only group ( 413% [ 95% ci 309514 ] vs 560% [ 451656 ] ) , as well as median progression - free survival , but not signi cantly so ( 159 months [ 95% ci 110211 ] vs 216 months [ 162278 ] ; un adjusted hr 126 [ 95% ci 090177 ] , 129 [ 089185 ] , p = 018 ) , median distant progression - free survival ( 184 months [ 133232 ] vs 254 months [ 184293 ] ) , survival local progression - free ( 159 months [ 110211 ] vs 216 [ 162278 ] )  . log - rank p = 017 ; adjusted hr and figures 4 and 5 show the results of the quality - of - life analysis . 
 a completion rate of 69% or above was maintained at week 13 ( 184 [ 71% ] completed qlq - c30 and 178 [ 69% ] completed qlq - oes18 ) ; the major reason for loss to follow - up was attrition . 
the change in the fol lowing number at risk crt plus cetuximab crt only months from randomisation figure 2 : kaplan - meier curves of overall survival by treatment group crt = chemoradiotherapy . reason for no surgery local extent of disease patient choice comorbidity / poor performance status tumour type adenocarcinoma squamous cell other stage deaths survival ( months ) 222 ( 161254 ) 247 ( 200303 ) 232 ( 128nc ) 197 ( 147258 ) 240 ( 205278 ) 303 ( 197nc ) 207 ( 169247 ) favours crt + cetuximab favours crt only figure 3 : hazard ratio plots for overall survival , by baseline characteristics survival data are median number of months ( 95% ci ) in all patients . 
positions of squares show hazard ratio of death in the crt plus cetuximab group compared with death in the crt only group ; the area of each square represents the amount of information ( ie , the number of patients ) in each category . 
full quality - of - life data will be reported elsewhere . discussion as the result of a preplanned assessment , the independent data monitoring committee reported that the primary endpoint of the phase 2 stage of the scope1 trial had not been met and recommended closing the vol 14 june 2013 articles crt plus cetuximab crt only the outcome of scope1 is consistent with recent results from other randomised trials comparing the addition of anti - egfr therapy to standard treatment across several tumour sites ( panel )  . 
patients who received the monoclonal antibody received a lower protocol dose of capecitabine and oxaliplat despite this prespeci ed dose modication , patients in the chemotherapy plus panitumumab group received a lower median number of cycles than did the control group ( ve vs six ) , a lower median dose intensity of capecitabine , and had worse overall survival ( 88 months vs 113 months ; hr 137 ; p = 001 )  . 
the radiation therapy oncology group ( rtog ) 0522 trial24 sought to build on the results of bonner and colleagues study17 by adding cetuximab to cisplatin or uoropyrimidine - based chemoradiation in a similar patient population with squamous - cell head and neck cancer . 
 once again , no bene t was reported in terms of progression - free survival or overall survival , although an increased rate of mucositis was noted in the patients treated with cetuximab.24 in the coin trial , 25 which randomly assigned 2445 patients with metastatic colorectal cancer to oxaliplatin uoropyrimidine ( uorouracil or capecitabine ) chemotherapy with or without cetuximab , a higher than anticipated incidence of grade 3 or 4 diarrhoea ( 30% ) in the experimental group resulted in a dose modi cation of capecitabine during the course of the trial . 
in the scope1 trial , the real3 trial , 23 and for most patients in the coin trial , 25 a capecitabine backbone was used and the resultant reduction in doses of standard therapy might have contributed to the worse outcome in the cetuximab groups of these trials . 
as seen in the real3 study , 23 patients receiving cetuximab had a lower rate of haematological toxicity , possibly as a result of the lower chemotherapy dose intensity delivered . perhaps more importantlywith respect to this study of an investigational drug in de nitive treatment of oesophageal cancerwas the e ect on the dose of radiotherapy delivered . 
more than twice the number of patients in the crt plus cetuximab group than in the crt only group did not receive any radiotherapy ( 25 vs 10 )  . 
as systemic therapies move from palliative , through to adjuvant , to de nitive treatment protocols , evidencebased treatment regimens should be vigilantly protected , especially if such treatments are intensi ed . another explanation for these results , independent of dose intensity , is the possible occurrence of a negative interaction between cetuximab and chemoradiotherapy . 
 the proin ammatory and antitumour proliferative e ects of cetuximab have been proposed as the cause of number of patients crt plus cetuximab crt only weeks from randomisation figure 4 : physical functioning score from qlq - c30 in each treatment group at ve timepoints over 52 weeks the number of patients shows the amount who completed qlq - c30 at each timepoint . 
qlq - c30 = european organisation for research and treatment of cancers quality of life questionnaire c30 . crt plus cetuximab crt only number of patients crt plus cetuximab crt only weeks from randomisation figure 5 : eating restrictions score from qlq - oes18 in each treatment group at ve timepoints over 52 weeks the number of patients shows the amount who completed qlq - oes18 at each timepoint . 
the addition of cetuximab to chemoradiotherapy resulted in more toxicity , less protocol treatment being delivered , and worse overall survival than with chemoradiotherapy alone , although quality of life was not reduced compared with chemoradiotherapy alone . 
therefore , the addition of cetuximab to standard de nitive chemoradiotherapy cannot be recommended . 634 vol 14 june 2013 articles reduced e cacy in combination with chemoradiation in rectal cancer.27 a similar interaction between oxaliplatin and cetuximab has been proposed , speci cally that cetuximab might protect against free - radical damage by platinum drugs , 28 and again could explain the negative outcome in this and other studies.25 , 29 despite this reduction in survival , however , and increased toxicity , we did not record an e ect on quality of life according to standard eortc generic and disease - speci c measures . the egfr pathway seems to be important in the carcinogenesis of oesophagogastric malignancy30 and a bene t of anti - egfr therapy has been shown in head and neck cancer in combination with radiotherapy17 and in advanced disease.15 the negative outcome in this study therefore seems to be a result of tumour - speci c interactions and biology that are not fully understood , or overlapping toxicities that preclude the delivery of e ective standard treatment . an understanding of why the overall survival in this trial was better than anticipated will be important ; 2 - year overall survival was predicted to be 35% in the crt only group in the phase 3 design . 
despite the fact that most patients had stage iii disease , 38% of patients were older than 70 years , and 15% of patients had comorbidities that precluded surgery , the 2 - year overall survival in all patients was 49% , and was 56% in those receiving crt only . 
indeed , the overall survival in the crt only group exceeded that which was hoped to be seen by the addition of cetuximab and was better than that seen in the us and uk studies exploring the role of the addition of neoadjuvant chemotherapy to surgery.3 although one of the lead authors in our investigation ( tc ) has previously published encouraging out comes of single centre , retrospective series , 8 , 12 whether these outcomes could be reproduced in a multicentre , prospective study was unclear . 
before this trial , concerns had been raised about the quality of radiotherapy delivered in multicentre uk studies of radiotherapy in upper gastrointestinal cancers.31 such studies did not have detailed radiotherapy treatment protocols and had near - absent radiotherapy quality assurance . 
 we developed a detailed protocol mandating the use of endoscopic ultrasound and intravenous contrast to aid localisation of target volume and used a single - phase conformal treatment plan.33 this plan , together with a comprehensive radiotherapy planning protocol and test cases , was sent to all principal investigators and radiotherapy centres before patients were recruited.19 we propose that this protocol , together with the on - trial quality assurance programme providing a positive dialogue between recruiting units and the rttqa central team , was a crucial component to the successful outcomes seen in the crt only group . 
the bene t of rttqa has been reported in other studies.34 to the best of our know ledge , this trial is the largest prospective panel : research in context systematic review we identi ed a systematic review22 on combined modality radiotherapy and chemotherapy in non - surgical management of localised carcinoma of the oesophagus that searched medline ( 19962001 ) , cancerlit ( 19832001 ) , cochrane library databases ( 2001 ) , and abstracts published in the american society of clinical oncology and the american society for therapeutic radiology and oncology ( 19992001 ) for articles published in any language . 
the review reported the bene ts of chemoradiotherapy ( crt ) compared with radiotherapy alone ; however , it also showed that most patients still relapse with locoregional or metastatic disease . 
we also identi ed studies that reported that cetuximab , a monoclonal egfr antagonist , improved outcomes when given in combination with : chemotherapy in advanced colorectal adenocarcinomas and squamous - cell head and neck cancer ; and radiotherapy in squamous - cell head and neck cancer . 
the results of our study do , however , support the use of chemoradiation alone as a standard of care in patients with non - metastatic squamous - cell carcinoma of the oesophagus and in patients with non - metastatic adenocarcinoma who are not suitable for surgery . 
indeed , the outcomes of this study would support the increased use of this treatment in patients who have a higher risk of failure of surgical treatment , either due to the existence of comorbidities or where surgical excision is likely to be incomplete . 
a randomised trial to compare surgical and radiotherapy - based treatments in patients with oesophageal cancer with a better outlook is warranted . study with a comprehensive assessment of quality of life with disease and cancer - speci c questionnaires patients under going de nitive chemoradiotherapy . 
 scores achieved in patients surviving for 2 years in our study are compatible with that achieved by surgical - based treatments.5 other factors that could have contributed to improved outcomes in this study are patient selection and organisation of cancer services throughout the uk . 
pet has been shown to both exclude patients with metastatic disease not otherwise seen with endoscopic ultrasound and ct scan35 and be useful in radiotherapy planning.36 substantial reconguration of oesophagogastric cancer treatment ser vices in the uk has also taken place in the past decade.37 , 38 although the changes have mainly been in centralisation of surgical services , they have led to the development of regional specialist multidisciplinary teams , which has vol 14 june 2013 articles undoubtedly added rigour to treatment decisions and patient selection . 
the 2012 annual report of the uk national oesophago - gastric cancer audit38 has showed an improvement in outcomes for patients undergoing surgery , with 45% of patients surviving for 3 years . 
both of these areas have scope for further development , namely the incorporation of ct - pet more directly into radiotherapy planning and assessment of caseload , with outcomes in specialist non - surgical services . how can we build further on the encouraging clinical outcomes reported in the crt only group of this study ? clearly , as patients continue to relapse with both metastatic and locoregional disease , systemic and local components of this treatment strategy need to be improved and intensi ed . 
the overexpression of her2 ( also known as erbb2 ) predicts whether the addition of trastuzumab will bene t patients with advanced oesophagogastric cancer.40 the safety and e cacy of anti - her2 therapy should be tested as part of chemoradiotherapy treatment in this patient population . a radiotherapy doseresponse e ect in patients with oesophageal cancer has been known for some time.41 however , a study designed to test the bene t of a higher radiation dose given concurrently with cisplatin and uoropyrimidine chemotherapy was prematurely stopped for futility as a result of an excess of treatmentrelated deaths occurring in the high - dose treatment group.9 we believe , however , that by using newer radiotherapy techniques , such as intensity - modulated and imageguided radiotherapy , we can now safely deliver a higher dose of radiation to a highly conformal target volume within the context of a high - quality rttqa programme . this trial was a phase 2 / 3 study that ended on completion of phase 2 . 
additionally , although the study strati ed patients according to tumour histology , it was not powered to assess with certainty the bene t of cetuximab in each of the two main histological variants of this disease . this trial has not shown that the addition of cetuximab to standard de nitive chemoradiotherapy bene ts patients with locally advanced oesophageal cancer . 
in fact , the addition of cetuximab increased toxicity , reduced delivery of all components of standard chemoradiotherapy , and was associated with a signi cant reduction in overall survival . 
however , the very encouraging outcomes seen with de nitive chemoradiotherapy alone should provide an excellent platform to test more targeted therapeutic approaches , incorporating biomarker - driven systemic therapies and newer radiotherapy technologies to safely intensify treatment , including increases to radiotherapy doses . contributors tc , cnh , sf , sg , js , jab , jig , jb , tm , and gg were involved in the design and development of the trial and the writing and review of the protocol . 
all authors have contributed to , seen , and approved the nal dratc , sf , sg , rro , jig , and dc were principal investigators at centres recruiting more than 5% of patients . 
a full list of all scope1 study investigators is listed in the appendix . con icts of interest we declare that we have no con icts of interest . acknowledgments the scope1 trial was sponsored by velindre nhs trust , funded by cancer research uk ( cruk ) , and cruk core funding at the wales cancer trials unit ( wctu )  . 
the radiotherapy trials quality assurance ( rttqa ) was funded by cruk and the cardi national cancer research institute rttqa centre at velindre nhs trust which are funded by the national institute of social care and health research ( nischr ; wales ) and department of health ( england )  . 
we thank all the patients who participated in the trial , the doctors , nurses , pathologists , other members of the multidisciplinary teams , radiotherapy team , and research team from the participating centres . 
we also thank lisette nixon ( wctu trial manager ) , bethan tranter ( trial pharmacist ) , david kirby ( patient representative ) , wendy wade ( research nurse ) , and ashley roberts ( radiologist ) for their input into the trial management group . articles e cacy of neoadjuvant bevacizumab added to docetaxel followed by uorouracil , epirubicin , and cyclophosphamide , for women with her2 - negative early breast cancer ( artemis ) : an open - label , randomised , phase 3 trial helena m earl , louise hiller , janet a dunn , clare blenkinsop , louise grybowicz , anne - laure vallier , jean abraham , jeremy thomas , elena provenzano , luke hughes - davies , ioannis gounaris , karen mcadam , stephen chan , rizvana ahmad , tamas hickish , stephen houston , daniel rea , john bartlett , carlos caldas , david a cameron , larry hayward , for the artemis investigators summary background the artemis trial was developed to assess the e cacy and safety of adding bevacizumab to standard neoadjuvant chemotherapy in her2 - negative early breast cancer . methods in this randomised , open - label , phase 3 trial , we enrolled women ( 18 years ) with newly diagnosed her2negative early invasive breast cancer ( radiological tumour size > 20 mm , with or without axillary involvement ) , at 66 centres in the uk . 
patients were randomly assigned via a central computerised minimisation procedure to three cycles of docetaxel ( 100 mg / m once every 21 days ) followed by three cycles of uorouracil ( 500 mg / m ) , epirubicin ( 100 mg / m ) , and cyclophosphamide ( 500 mg / m ) once every 21 days ( d - fec ) , without or with four cycles of bevacizumab ( 15 mg / kg ) ( bev + d - fec )  . 
signi cantly more patients in the bevacizumab group achieved a pathological complete response compared with those treated with chemotherapy alone : 87 ( 22% , 95% ci 1827 ) of 388 patients in the bev + d - fec group compared with 66 ( 17% , 1321 ) of 393 patients in the d - fec group ( p = 003 )  . 
grade 3 and 4 toxicities were reported at expected levels in both groups , although more patients had grade 4 neutropenia in the bev + d - fec group than in the d - fec group ( 85 [ 22% ] vs 68 [ 17% ] )  . interpretation addition of four cycles of bevacizumab to d - fec in her2 - negative early breast cancer signi cantly improved pathological complete response . 
however , the incidence of breast cancer has increased and continues to represent a major health problem worldwide.1 both the early breast cancer trialists collaborative group ( ebctcg ) overview analyses , 2 , 3 and individual trial data have shown bene t for adjuvant anthracycline46 and taxane - containing chemotherapy.79 although considerable progress has been made in early breast cancer through large adjuvant randomised these advances have been relatively slow . 
follow - up is prolonged in order to meet the prespeci ed event rate criteria for disease - free survival and overall survival analyses , as treatment trials , de ned in the statistical analysis plans.10 neoadjuvant trials in breast cancer have become increasingly common over the past 10 years , and the primary endpoint of pathological complete response can be reported more rapidly than in their adjuvant counterparts . trial and looked at neo - tango was our previous randomised phase 3 neoadjuvant the addition of gemcitabine to an anthracycline - based chemotherapy followed by taxane sequential combination , 11 and also the e cacy of giving paclitaxel rst in the treatment sequence . 
individual trials and the early breast cancer trialists collaborative group overviews had shown bene t for taxane and anthracycline chemotherapy , but intensi cation had failed to yield further rapid progress . 
neoadjuvant trials in breast cancer have been increasingly pursued with the early primary endpoint of pathological complete response as a surrogate for activity and improvement in long - term outcomes . 
in 2008 there was great interest in the role of the anti - angiogenic monoclonal antibody bevacizumab because phase 3 trials of bevacizumab had reported bene t in the metastatic setting . 
we developed the artemis uk multicentre trial to test the hypothesis that the combination of bevacizumab with neoadjuvant taxane and anthracycline containing chemotherapy might improve the proportion of patients achieving a pathological complete response in her2 - negative breast cancer , with acceptable toxicity . 
the artemis trial also collected tumour and blood from participants for future translational studies seeking molecular characteristics predicting bene t from bevacizumab , a key to optimising coste ectiveness in future . 
 added value of this study this report presents the primary endpoint of pathological complete response in artemis , showing a signi cant improvement in the proportion of patients achieving a pathological complete response with the addition of bevacizumab to neoadjuvant chemotherapy . 
we postulate that known variations between the trials in er status de nition might have resulted in varying distribution of er weakly positive patients across the dichotomised er positive and negative categories , thus explaining the apparently divergent results . 
we also hypothesise that molecular characteristics of individual tumours , similar to those recently observed in ovarian cancer trials of bevacizumab , might correlate with er status and underlie the variations in individual patient bene t observed . 
we developed the artemis randomised trial to test the hypothesis that the combination of bevacizumab with neoadjuvant anthracycline and taxane - based chemotherapy might improve the proportion of patients achieving a pathological complete response in breast cancer with acceptable toxicity . 
this study presents the results of the primary endpoint analysis . methods study design and participants the artemis phase 3 randomised trial aimed to assess the bene t of the addition of neoadjuvant bevacizumab to chemotherapy in terms of short - term and long - term outcomes in women presenting with early breast cancer . 
 we enrolled women aged 18 years or older with a histological diagnosis of early invasive breast cancer , and a radiological tumour size of more than 20 mm with or without axillary involvement . 
 patients with in ammatory cancer , t4 tumours with direct extension to the chest wall or skin , and ipsilateral supraclavicular lymph node involvement were eligible with any size of primary tumour . 
we regarded hormone oestrogen receptor ( er ) status as negative when allred score was 02 / 8 ; er weakly positive was 35 / 8 ; and er strongly positive was 68 / 8 . 
these er categories were based on those already used by our group in the tango trial14 and subsequently con rmed by petit and colleagues15 to be predictive of neoadjuvant chemotherapy response ( pathological complete response ) in er - positive tumours . 
 all patients were her2 negative , de ned immunohistochemistry of 0 / 1 + , or if 2 + , uorescence insitu hybridisation showed no evidence of ampli cation of the her2 gene . 
other eligibility criteria were adequate cardiac function ( left ventricular ejection fraction within the normal institutional range , as assessed by multiplegated acquisition scan or echocardiogram ) , adequate bone marrow , hepatic , and renal function , and appropriate ( ecog ) eastern cooperative oncology group performance status ( 02 )  . 
in view of potential side - e ects from bevacizumab , patients had to have no previous diagnosis of ischaemic heart disease , cerebrovascular disease , peripheral vascular disease , arterial or venous thromboembolic disease , cardiac failure , gastroduodenal vol 16 june 2015 articles 401 assigned to d - fec 399 assigned to bev + d - fec 800 participants randomly assigned 1 did not undergo surgery 1 protocol violator refused surgery 1 did not have lymph node examination after chemotherapy 6 withdrew consent for further follow - up before surgery that was her2 - positive 6 were ineligible 4 with tumours 20 mm or less 1 with a second breast tumour 1 with liver metastases 8 had baseline blood pressure measurements outside of the protocol stated limits 4 did not undergo surgery 3 withdrew from the trial due to early disease progression or inadequate response to chemotherapy 1 had inammatory disease after neoadjuvant chemotherapy 7 withdrew consent for further follow - up before surgery 1 ineligible because of bone metastases 6 had baseline blood pressure measurements outside of the protocol stated limits 393 included in the primary endpoint analysis 388 included in the primary endpoint analysis figure 1 : trial pro le d - fec = docetaxel 100 mg / m once every 21 days , followed by uorouracil 500 mg / m , epirubicin 100 mg / m , and cyclophosphamide 500 mg / m once every 21 days . 
bev + d - fec = bevacizumab 15 mg / kg given every 3 weeks with the rst four cycles of chemotherapy ( d - fec )  . for the trial protocol see warwick.ac.uk / go / artemis ulcer , symptomatic diverticulitis , or in ammatory bowel disease . 
additionally , no uncon trolled hypertension , de ned by a systolic pressure greater than 150 mm hg or diastolic pressure greater than 90 mm hg , with or without antihypertensive medication was allowed . 
 patients with initial increases in blood pressure were eligible if initiation or adjustment of antihypertensive medication lowered pressure to meet entry criteria . no previous exposure to chemotherapy , radiotherapy , or endocrine therapy as treatment for breast cancer was allowed . 
full eligibility criteria can be found in the trial protocol . artemis was an investigator designed and led trial , granted a clinical trials authorisation ( cta ) from the medicines and healthcare products regulatory agency ( mhra ) on feb 25 , 2009 , approved by the multi - centre research ethics committee nationally on march 26 , 2009 , and subsequently by the local research ethics committees at all participating centres . 
treatment allocations were made by telephone to the warwick clinical trials unit , where a central computerised minimisation procedure was used to ( 1 : 1 ) generate the patients random allocation . 
strati cation by minimisation was done by age ( 50 years vs > 50 years ) , er status ( negative vs weakly positive vs strongly positive ) , total tumour size ( 5 cm vs > 5 cm ) , clinical involvement of axillary lymph nodes ( yes vs no ) , and disease type ( in ammatory or locally advanced or both vs neither )  . 
the trial was open label . procedures chemotherapy regimens used were docetaxel 100 mg / m once every 21 days for three cycles , followed by uorouracil 500 mg / m , epirubicin 100 mg / m , with cyclophosphamide 500 mg / m once every 21 days for three cycles ( d - fec )  . 
bevacizumab 15 mg / kg ( genentech , south san francisco and vacaville , ca , usa ) was given every 3 weeks with the rst four cycles of chemotherapy in the experimental group ( bev + d - fec )  . we assessed adverse events for each chemotherapy cycle by grade according to common terminology criteria for adverse events ( ctcae ) version 3 . 
if neutropenic fever or sepsis occurred after a cycle of chemotherapy , the next cycle was delayed until the absolute neutrophil count was at least 10 10 cells per l . 
after a delay , either dose reduction of all drugs to 80% , or gcsf support with 100% dose were allowed , and all remaining cycles of the same three - cycle block were given at those doses . 
for persistent thrombocytopenia , the next cycle was delayed until platelets had recovered to at least 100 10 cells per l and chemotherapy doses were reduced to 80% , maintaining this dose reduction for subsequent cycles . 
however , once started , prophylactic gcsf was usually continued into the second phase of chemotherapy at the discretion of the responsible physician . if grade 2 neuropathy occurred during treatment with docetaxel , remaining doses were reduced to 75 mg / if grade 3 neuropathy occurred , docetaxel was stopped . 
if fewer than three cycles of docetaxel had been given , additional fec cycles were allowed up to a maximum of six cycles in total , at the discretion of the treating consultant . cardiac toxicity was checked by left ventricular ejection fraction before treatment started and after four cycles of chemotherapy with or without bevacizumab . 
if severe allergic symptoms occurred , including bronchospasm , angio - oedema , hypotension generalised urticaria , ( systolic blood pressure < 100 mm hg ) , or life - threatening anaphylaxis , docetaxel infusion was stopped and treatment was given with intramuscular epinephrine ( 1 ml , 1 : 1000 ) , intravenous steroids , and intravenous antihistamines ; rechallenge was contraindicated . surgery ( breast and axillary ) , radiotherapy , and adjuvant endocrine treatment were done according to local protocols . 
patients will continue to receive follow - up through the national cancer intelligence network ( ncin ) with monitoring of disease - free survival and overall survival . similar to other recent and the reporting of pathological complete response and minimal residual disease was by an independent , central , two - reader masked review of all anonymised local surgical histopathology reports undertaken by the cochief investigators ( hme and lha )  . 
a quality assurance comparison ( using a statistic ) has been done in cases reviewed to date , between central pathological review of the haematoxylin and eosin slides ( all cases done by jt ) and the local histopathology reports for the primary endpoint of pathological complete response . outcomes our primary endpoint was pathological complete response , de ned as absence of invasive breast cancer in ductal carcinoma in situ associated with tumour data are n ( % )  . 
each measurable breast tumours longest single diameter is summed within each breast for each patient , and labelled as tumour bulk ; for each patients breast with maximum tumour bulk , tumour characteristics are presented . 
 * adjusted for the ve strati cation variables ( age [ 50 years , > 50 years ] , er status [ negative , weakly positive , strongly positive ] , tumour size [ 50 mm , > 50 mm ] , clinical involvement of axillary nodes [ no , yes ] , and inammatory or locally advanced disease [ no , yes ] )  . 
tumour grade of each patients largest breast tumour at baseline . table 2 : pathological complete response and minimal residual disease in d - fec and bev + d - fec groups less of original tumour burden remaining at surgery , and has previously been reported as a potentially useful secondary endpoint in neoadjuvant studies.16 other protocol - de ned secondary endpointsthat are not reported hereinclude disease - free survival and overall survival . 
these will be analysed in early 2016 when it is anticipated that median follow - up will be at least 36 months or 120 disease - free survival events will have occurred . statistical analysis the power calculations assume a 70 to 30 split in the trial sample between er - positive and er - negative tumours , respectively . 
the proportion of patients achieving a pathological complete response with the standard treatment ( d - fec ) was estimated as about 10% for erpositive tumours and 25% for er - negative tumours . 
on this basis , a trial randomly assigning 400 patients into each of the two treatment groups would allow an absolute di erence in the proportion of patients achieving a pathological complete response in excess of 10% to be detected at the 5% ( two - sided ) level of signi cance with an 85% power . 
a 10% di erence in the proportion of patients who achieve a pathological complete response is the most widely accepted in neoadjuvant chemotherapy trials and was used in this groups previously reported neo - tango trial.11 the proportion of patients achieving pathological complete response was calculated for all patients known to have had surgery . 
 multivariate logistic regression provided p values for the treatment e ect after adjustment for strati cation factors . as a secondary analysis , the proportion of patients achieving pathological complete response in the breast alone was assessed along with those achieving pathological complete response or minimal residual disease , and comparisons across treatment groups were logistic regression with made using multivariate adjustment for prognostic factors . the sample size of our study is too small to permit multiple subgroup analyses , and so we chose not to do tests for statistical signi cance in each er subgroup separately . the methods for dose intensity calculations have been described previously.17 chemotherapy course delivered dose intensities were compared across treatment groups using wilcoxon rank - sum tests and fishers exact tests . common toxicity criteria ( ctc ) grades were recorded for each chemotherapy cycle and growth factor support ( usually gcsf ) was also recorded . 
the reports of grade 3 and 4 toxicities were examined in detail . statistical analysis was done on an intention - to - treat basis and therefore all patients who were ineligible , or whose treatment violated the trial protocol , were analysed within their randomised treatment groups . 
pathological complete response di ered signi cantly across both er status ( negative 41% [ 95% ci 3548 ] , weakly positive 49% [ 3861 ] , strongly positive 8% [ 611 ] ; p < 00001 ) and tumour grade ( grade 1 / 2 9% [ 613 ] , grade 3 32% [ 2837 ] ; p < 00001 )  . 
similarly , the proportion of patients who obtained a pathological complete response or minimal residual disease was signi cantly better in the bev + dfec group than in the d - fec group ( di erence 7% [ 95% ci 01132 ] ; p = 003 after adjustment for strati cation factors ; table 2 )  . 
the proportion of patients who obtained a pathological complete response or minimal residual disease di ered signi cantly across both er status ( negative 51% [ 95% ci 4558 ] , weakly positive 60% [ 4871 ] , strongly positive 18% [ 1522 ] ; p < 00001 ) and tumour grade ( grade 1 / 2 16% [ 1221 ] , grade 3 44% [ 3949 ] ; p < 00001 )  . 
hme , lhi , and lha had full access to all of the data and had nal responsibility for the decision to submit for publication with the agreement of all the authors and the data monitoring and safety committee . results 800 patients were recruited at 66 uk centres ( between may 7 , 2009 , and jan 9 , 2013 ) and randomly assigned to either d - fec ( 401 patients ) or bev + d - fec regimens ( 399 patients ; gure 1 )  . 
we subsequently identi ed seven patients as ineligible ; six in the d - fec group ( four with tumours 20 mm or less , one with a second breast tumour that was her2 - positive , and one with liver metastases ) ; and one in the bev + d - fec group ( with bone metastases )  . 
additionally , 14 patients ( eight in the d - fec group and six in the bev + d - fec group ) had baseline blood pressure measurements outside of the protocol stated limits . 
153 ( 20% ) of all 781 patients achieved a pathological complete response : 66 ( 17% , 95% ci 1321 ) in the d - fec group and 87 ( 22% , 1827 ) in the bev + d - fec group ( di erence 6% , 01112 ; p = 003 after adjustment for strati cation factors , p = 006 for the unadjusted analysis ; table 2 and gure 2 )  . 
er negative , er weakly positive , and grade 3 patients appeared to bene t from the addition of bevacizumab whereas er strongly positive and grade 1 / 2 patients did not appear to bene t from the addition of bevacizumab ( table 2 )  . 
an analysis of bene t for bevacizumab for each level of allred score ( er status ) , con rmed that our categories of er weakly positive ( allred 35 / 8 ) and er strongly positive ( allred 68 / 8 ) were the correct cut points both for pathological complete response rate and bene t for bevacizumab ( appendix )  . 
 table 4 : chemotherapy modi cations in the 4418 cycles number not given as per protocol number of treatment delays cycle 1 cycle 2 cycle 3 cycle 4 data are n ( % )  . 
four patients in the bev + d - fec group received no treatment cycles for the following reasons : diagnosis of colitis and patient proceeded to mastectomy with axillary surgery ; patient chose to withdraw from trial before any treatment was given ; allergic reaction and no chemotherapy given ; diagnosis of metastatic disease during the trial screening phase . 695 ( 90% ) of 775 patients ( 352 [ 90% ] of 391 patients in the d - fec group and 343 [ 89% ] of 384 in the bev + d - fec group ) who started treatment received six cycles of chemotherapy ; the main reasons for receiving fewer cycles being patient withdrawal , allergic reaction to drugs , and chemotherapy toxicities . 
no di erences in chemotherapy course delivered dose intensity between the treatment groups were detected ( d - fec 98% [ 95% ci 92100 ] vs bev + d - fec 97% [ 91100 ] ; p = 024 )  . 
665 ( 85% ) patients received a chemotherapy course delivered dose intensity of at least 85% ( d - fec 86% [ 95% ci 8289 ] vs bev + dfec 85% [ 8188 ] ; p = 058 )  . 
 the main reason for switching early was allergy to docetaxel ( 19 [ 83% ] of 23 patients ; 11 [ 79% ] of 14 d - fec patients , eight [ 89% ] of nine bev + d - dfec patients )  . 331 ( 86% ) of 384 bev + d - fec patients who started treatment received four cycles of bevacizumab . 
85% ( 95% ci 8188% ) of bev + d - fec patients received a bevacizumab course delivered dose intensity of at least 85% . the intensities both individual cycle dose for chemotherapy and bevacizumab did not show substantial attrition over time ( appendix )  . 
of the 386 ( 9% ) reports of chemotherapy dose reductions from 4418 chemotherapy cycles , dose reductions were most commonly reported in cycles 2 and 3 and again in cycles 5 and 6 , in both treatment groups ( table 4 )  . 
 reports of modi cations to bevacizumab administration were infrequent throughout the four cycles ( table 5 )  . gcsf was used in 2744 ( 62% ) of 4418 cycles with slightly higher rates in the bev + d - fec group in all treatment cycles ( appendix )  . 
full treatment details were available for 4418 cycles delivered to 775 patients ( 2234 cycles in 391 d - fec patients and 2184 cycles in 384 bev + d - fec patients )  . 
more patients receiving bevacizumab with d - fec had grade 3 infections than those receiving d - fec alone ( 68 [ 18% ] vs 40 [ 10% ] )  . 
allergies were reported separately : 43 ( 5% ) of 800 patients ( 26 d - fec patients , 17 bev + d - fec patients ) had grade 3 and 4 allergic reactions attributable to docetaxel and only one patient had grade 3 allergy attributable to bevacizumab . 
both regimens appear tolerable and deliverable . full surgery details were available for 764 ( 98% ) of 781 patients ( 378 d - fec patients , 386 bev + d - fec patients ) analysed for pathological complete response by local report review . 
the geparquinto results are supported by those of calgb 40603 , which enrolled triple - negative patients only.20 in this smaller study , the addition of bevacizumab signi cantly the proportion of patients achieving a pathological complete response ( de ned as absence of invasive disease in breast only [ ypt0 / tis ] ) in the bevacizumab group compared with the chemotherapy alone group ( 59% vs 48% ; p = 0009 )  . 
the results of these two studies are very similar to our study , in which a greater proportion of patients treated with bevacizumab achieved a pathological complete response ( de ned as no invasive disease in breast or axilla [ ypt0 / tis ypn0 ] ) than those treated with chemotherapy alone ( 22% vs 17% in the overall study population and 44% vs 32% in er / her2 - negative patients )  . 
as an example , in calgb 40603 , the signi cantly lower proportions of patients having mastectomy compared with the d - fec group ( 48% vs 51% ; p = 047 ; appendix )  . 
however , overall , signi cantly fewer patients who achieved a pathological complete response had a mastectomy compared with those who did not achieve a pathological complete response ( 42 / 146 [ 29% ] vs 335 / 618 [ 54% ] ; p < 00001 ; appendix )  . 
having a pathological complete response or minimal residual disease in the breast also signi cantly lowered the frequency of mastectomy compared with those patients who achieved neither ( 90 / 243 [ 37% ] vs 287 / 522 [ 55% ] p < 00001 ; appendix )  . discussion in the artemis study , the addition of short course bevacizumab to standard neoadjuvant anthracycline and taxane - based chemotherapy in her2 - negative , early breast cancer , was associated with a signi cant improvement in the proportion of patients achieving a pathological complete response . 
a greater proportion of er - negative ( allred 02 ) and er weakly positive ( allred 35 ) patients achieved pathological complete response compared with the er strongly positive ( allred 68 ) patients . 
the bene t of bevacizumab for er - negative and weakly positive patients is in marked contrast to the er strongly positive group in which low proportions of patients achieved pathological complete response and there was also an apparent lack of bene t from bevacizumab . 
the artemis treatment protocol was deliverable for both chemotherapy and bevacizumab , and toxicity from chemotherapy was as expected for d - fec , although there was an increase in grade 4 neutropenia in patients given bev + d - fec , as reported previously.18 the observed di erences in pathological complete response were statistically signi cant in the group as a whole . 
however , the clinical signi cance of the addition of bevacizumab appears to be most compelling within the er - negative subgroup . three other randomised studies have reported on the addition of bevacizumab to neoadjuvant chemotherapy in her2 - negative breast cancer1922 ( appendix )  . 
 in our trial , er weakly positive patients ( although a small strati ed subgroup ; n = 75 ) showed similar chemotherapy response and bene t from bevacizumab to the er - negative group . 
we believe that a meta - analysis of all four studies with uniform de nitions of hormone receptor and pathological complete response is needed to identify a subgroup of patients in whom bevacizumab increases pathological complete response . 
with that in mind , and acknowledging that the sample size of our study is too small for subgroup analyses , we chose not to do tests for statistical signi cance in each er subgroup separately ( table 2 )  . the use of pathological complete response as a trial endpoint is to some extent dependent on its role as a surrogate for meaningful clinical outcomes such as disease - free survival , distant relapse - free interval , breast cancer speci c survival , and overall survival . 
some of these have very recently been reported the geparquinto study24 and show no di erence for the addition of bevacizumab at 3 years for either disease - free for that explanation survival ( hr 103 , 95% ci 084125 ) or overall survival ( 097 , 075126 )  . 
results might be confounded because no bevacizumab was given after surgery and patients who were not responding on ultrasound assessment , at the midpoint of their neoadjuvant treatment , were o ered randomisation into a novel treatment group with everolimus . 
whereas an increased incidence of pathological complete response occurs in the well - developed primary tumour , which is angiogenesis - dependent , there might be no such advantage in terms of increased eradication of eventually lethal distant micrometastatic bone marrow disease . 
hatzis and colleagues29 have explored this in depth , and have 664 vol 16 june 2015 articles improved event - free modelled data from neoadjuvant trials and made two conclusions . 
first , that in high - risk breast cancer the design of neoadjuvant trials could increase the numbers of patients to a level that would make a positive correlation between the primary endpoint ( proportion of patients achieving pathological complete response ) and longer term outcomes more likely . 
in the ctneobc analysis of 12 trials and 11 955 patients , the coe cient of determination ( r ) was only 003 for eventfree survival and 024 for overall survival , meaning that only 3% and 24% of the variability in event - free survival and overall survival , respectively , between trial groups can be explained by di ering proportions of patients achieving a pathological complete response . 
the translational artemis group plan to explore , using samples from the artemis trial biobank , whether the same angiogenic signature in breast cancer could provide a predictive biomarker of response to bevacizumab . contributors hme and lha were responsible for the conception , design , recruitment , interpretation of the data , and drafting of the manuscript . 
lha received funding through the university of cambridge ( as sponsors of the trial ) from cancer research uk , roche , and sano - aventis , and disbursed the proportion due to nhs lotian for work on the trial ; and personal fees from roche for attendance at advisory board and international meetings . 
a - lv , ja , lh - d , ra , ig , sc , th , jt , ep , cc , and sh declare no competing interests . acknowledgments the trial was funded by cancer research uk ( cruk / 08 / 037 for trial coordination ) , roche ( provision of free study drug bevacizumab and unrestricted educational grant for trial coordination ) , and sano - aventis ( unrestricted educational grant for trial coordination )  . 
we thank the data and safety monitoring committee members : i craig henderson ( university of california , san francisco , ca , usa ) , luca gianni ( ospedale san ra aele , milan , italy ) , mark f brady ( gynecologic oncology group statistical & data center , roswell park cancer institute , bu alo , ny , usa ) , and xavier pivot ( centre hospitalier rgional universitaire et institut rgional fdratif de cancrologie , besanon , france )  . 
we thank the trials unit sta : phase 3 coordination at warwick clinical trials unit , coventry , uk ; translational coordination at university of cambridge , addenbrookes hospital , cambridge , uk and university of edinburgh department of oncology ( biobank ) ; and statistical analysis at warwick clinical trials unit , uk . risk of subsequent primary neoplasms in survivors of adolescent and young adult cancer ( teenage and young adult cancer survivor study ) : a population - based , cohort study chloe j bright , raoul c reulen , david l winter , daniel p stark , martin g mccabe , angela b edgar , clare frobisher , michael m hawkins summary background few studies have investigated the risks of subsequent primary neoplasms after adolescent and young adult ( aya ) cancer . 
we investigated the risks of specific subsequent primary neoplasms after each of 16 types of aya cancer . methods the teenage and young adult cancer survivor study is a population - based cohort of 200 945 survivors of cancer diagnosed when aged 1539 years in england and wales from jan 1 , 1971 , to dec 31 , 2006 . 
in this analysis , we focus on the risk of specific subsequent primary neoplasms after 16 types of aya cancer : breast ; cervical ; testicular ; hodgkin lymphoma ( female ) ; hodgkin lymphoma ( male ) ; melanoma ; cns ( intracranial ) ; colorectal ; non - hodgkin lymphoma ; thyroid ; soft - tissue sarcoma ; ovarian ; bladder ; other female genital ; leukaemia ; and head and neck cancer . 
we report absolute excess risks ( aers ; per 10 000 person - years ) and cumulative incidence of specific types of subsequent primary neoplasm after each type of aya cancer . findings during the 2 631 326 person - years of follow - up ( median follow - up 168 years , iqr 105252 ) , 12 321 subsequent primary neoplasms were diagnosed in 11 565 survivors , most frequently among survivors of breast cancer , cervical cancer , testicular cancer , and hodgkin lymphoma . 
aers of any subsequent primary neoplasms were 195 per 10 000 person - years ( 95% ci 174215 ) in survivors of breast cancer , 102 ( 80124 ) in survivors of cervical cancer , 189 ( 166211 ) in survivors of testicular cancer , 557 ( 504611 ) in female survivors of hodgkin lymphoma , and 299 ( 263336 ) in male survivors of hodgkin lymphoma . 
the cumulative incidence of all subsequent primary neoplasms 35 years after diagnosis was 119% ( 95% ci 113126 ) in survivors of breast cancer , 158% ( 148167 ) in survivors of cervical cancer , 202% ( 189215 ) in survivors of testicular cancer , 266% ( 247286 ) in female survivors of hodgkin lymphoma , and 165% ( 152180 ) in male survivors of hodgkin lymphoma . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma in women , breast cancer , and hodgkin lymphoma in men , we identified a small number of specific subsequent primary neoplasms that account for 82% , 61% , 58% , 45% , and 41% of the total excess number of neoplasms , respectively . 
lung cancer accounted for a notable proportion of the excess number of neoplasms across all aya groups investigated . interpretation our finding that a small number of specific subsequent primary neoplasms account for a large percentage of the total excess number of neoplasms in long - term survivors of cervical , breast , and testicular cancer , and hodgkin lymphoma provides an evidence base to inform priorities for clinical long - term follow - up . 
the prominence of lung cancer after each of these aya cancers indicates the need for further work aimed at preventing and reducing the burden of this cancer in future survivors of aya cancer . funding cancer research uk , national institute for health research , academy of medical sciences , and children with cancer uk . copyright 2019 the author ( s )  . 
 we searched pubmed without any language or date restrictions using the keywords teenage and young adult cancer or adolescent and young adult cancer and survivor or long - term and second cancer or subsequent cancer on feb 16 , 2016 , for articles describing subsequent primary neoplasms in this population . 
a more focused search using each specific aya cancer as keywords ( eg , hodgkin lymphoma ) in place of teenage and young adult cancer or adolescent and young adult cancer was also done . 
we identified only one study that investigated the risk of subsequent primary neoplasms after the entire spectrum of aya cancers diagnosed at 1539 years of age . added value of this study to our knowledge , this is the largest study to investigate the risks of subsequent primary neoplasm after each specific aya cancer and the first to provide excess risks of specific types of subsequent primary neoplasm after each of 16 types of aya cancer . 
unlike previous studies , which focused on the multiplicative risk , we concentrated on the absolute excess riskie , the excess number of subsequent primary neoplasms beyond those expected from the general population , which is directly interpretable in terms of adverse health impact on survivors . 
additionally , we identified a small number of specific subsequent primary neoplasms that account for a substantial proportion of the total excess number of neoplasms in survivors of breast cancer , cervical cancer , testicular cancer , and hodgkin lymphoma . implications of all the available evidence our findings advance previous knowledge on the risks of subsequent neoplasms after aya cancer and provide an evidence base for identifying priorities for clinical follow - up of survivors of aya cancer . 
because lung cancer accounted for a notable proportion of the excess number of neoplasms across all aya groups investigated , there is need for work aimed at reducing this burden among future survivors . primary breast cancer and primary hodgkin lymphoma had the highest absolute excess risk ( 544 and 486 per 10 000 person - years , respectively )  . 
however , the study did not investigate the risks of specific subsequent primary neoplasms after each specific type of aya cancer . evidence from previous studies of childhood cancer survivors suggests that the principal factors determining risks of subsequent primary neoplasms relate to aspects of treatments received for the original cancer.1416 treatment of aya cancer varies greatly by cancer type and therefore , in the absence of detailed treatment information , it is essential to stratify risks by specific types of aya cancer ; such risk stratification provides an evidence base for clinical follow - up . the aims of this large - scale population - based study were to calculate risks of all and specific subsequent primary neoplasms after each type of aya cancer and to explore variation in these risks in relation to years from diagnosis , age at diagnosis , decade of diagnosis , and sex . methods study design and participants the teenage and young adult cancer survivor study ( tyacss ) was established using cancer registrations relating to neoplasms diagnosed between jan 1 , 1971 , and dec 31 , 2006 , in individuals aged 1539 years inclusive , which were obtained from the office for national statistics for english cancer registrations , and the welsh cancer intelligence and surveillance unit , public health wales , for welsh cancer registrations . 
both tumourrelated ( eg , tumour site , morphology , date of diagnosis ) and patient - related ( eg , sex , date of birth , national health service [ nhs ] number , and unique patient identifier ) information were obtained . 
the cancer registrations were checked for any errors , such as missing data in essential variables ( including sex , date of birth , date of diagnosis , tumour site , and tumour histology ) and incorrect chronology of events ( birth , cancer , death )  . 
 cancer registrations were excluded if the neoplasm was not malignant ( apart from intracranial , intraspinal , and bladder neoplasms where any behaviour was allowed ) , the histological type was not in the international classification of diseases for oncology classification , the histological type was a non - melanoma skin cancer ( these are underascertained by cancer registries ) , or if they were duplicate registrations . 
we also excluded individuals who had a previous childhood cancer included in the british childhood cancer survivor study.17 if an individual had multiple neoplasms diagnosed as an aya cancer , then the first was regarded as the index cancer for the cohort . 
ethical approval was provided by the national research ethics service and permission to process information without individual consent by the national information governance board for health and social care . see online for appendix 532 vol 20 april 2019 articles procedures information on cancer diagnosis , sex , age at cancer diagnosis , decade of cancer diagnosis , and years since diagnosis were derived from the cancer registration information . 
first primary neoplasms were grouped according to the internationally acknowledged classification scheme for tumours diagnosed in adolescence and young adulthood.18 carcinomas and germ cell tumours were further subdivided by anatomical site because of the implications of radiotherapy site for the risk of subsequent primary neoplasm ( appendix pp 35 )  . 
 we aimed to produce risk estimates after each specific first primary neoplasm ; therefore , survivors of cancers categorised as other cancers were not included ( appendix pp 2 , 6 )  . 
we focused on the risk of specific subsequent primary neoplasms after 16 types of aya cancer : breast ; cervical ; testicular ; hodgkin lymphoma ( female ) ; hodgkin lymphoma ( male ) ; melanoma ; cns ( intracranial ) ; lymphoma ; colorectal ; non - hodgkin thyroid ; soft - tissue sarcoma ; ovarian ; bladder ; other female genital ; leukaemia ; and head and neck cancer . 
 decade of diagnosis was divided into 197179 , 198089 , and 19902006 , in order to broadly describe differences in treatment given in these periods ( early chemotherapy , chemotherapy , and modern treatment era )  . 
years since diagnosis were classified using 10 - year bands following diagnosis . individual patient record linkage to national cancer registries enabled data to be obtained indicating when an individual in the cohort had a subsequent cancer registration . 
subsequent cancer registrations were classified as a subsequent primary neoplasm according to the international association of cancer registries ( iacr ) and international agency for research on cancer ( iarc ) rules for determining multiple primary tumours using the iacr / iarc tools software . 
 to reduce the likelihood of a local spread of the original aya cancer being classified as a subsequent primary neoplasm , potential subsequent primary neoplasms occurring in anatomical sites close to the first primary neoplasm were excluded ( appendix pp 78 )  . 
consequently , reported risk estimates are inevitably conservative . statistical analysis individuals were followed from 5 - year survival until the first occurrence of death , emigration , or study end date ( dec 31 , 2012 )  . 
absolute excess risks ( aers ) were calculated as the observed minus expected number of neoplasms , divided by the person - years at risk and multiplied by 10 000 . 
the expected number of neoplasms was derived by multiplying the number of person - years accrued , stratified by sex , attained age ( 5 - year bands ) , and calendar year ( 1 - year bands ) by the corresponding cancer rate in the general population of england and wales , 19 and summing appropriately . 
for aya cancers with 200 or more observed subsequent primary neoplasms , sirs are reported by specific type of subsequent primary neoplas we restrict attention to first primary neoplasm / subsequent primary neoplasm combinations with at least 100 subsequent primary neoplasms and a statistically significant sir . 
 we considered aers to be statistically significant at the 5% level ( two - tailed test ) if the 95% ci did not include 0 . incorporating aers were stratified by years from diagnosis , age at diagnosis , decade of diagnosis , and sex where there were at least 100 subsequent primary neoplasms . 
to explore the simultaneous effect of these explanatory factors , the multivariable poisson regression expected number of events was used to derive relative excess risks ( rers ) .20 rers can be interpreted as the ratio of aers adjusted for other potential explanatory factors included within the statistical model . 
aers by an explanatory factor are reported if both the univariable and multivariable tests for linear trend in the aers were each significant and the difference in the aers between the lowest and highest level of the risk factor was at least nine excess subsequent primary neoplasms . 
a likelihood ratio test was used to test for linear trend in a factor by comparing the log - likelihood of a model including the variable of interest with the log - likelihood of a model without the variable of interest . 
in deciding the percentage of the total aer attributable to specific subsequent primary neoplasms in relation to years from diagnosis , we ignored negative values for the aer and focused only on the positive values . 
thus , the total aer ( for the purposes of calculating percentages ) after each specific first primary neoplasm is the sum of the positive values for the contributing subsequent primary neoplasms . cumulative incidence was calculated treating death as a competing risk . 
other aya cancers were not included in the analysis of subsequent primary neoplasms . table 1 : cohort characteristics we did sensitivity analyses in which subsequent leukaemia was included among survivors of aya hodgkin lymphoma , leukaemia , and non - hodgkin lymphoma , and subsequent sarcoma was included among survivors of soft - tissue sarcoma and bone tumours . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results the tyacss cohort comprises 200 945 5 - year survivors of cancer diagnosed when aged 1539 years , between jan 1 , 1971 , and dec 31 , 2006 , in england and wales . 
during the 2 631 326 person - years of follow - up ( median follow - up 168 years , iqr 105252 ) , 12 321 subsequent primary neoplasms were diagnosed in 11 565 ( 6% ) of the 197 827 survivors included in the analysis . 
subsequent primary neoplasms were most frequently seen in survivors of breast cancer ( 1877 [ 15% ] of 12 321 subsequent primary neoplasms ) , cervical cancer ( 1675 [ 14% ] ) , hodgkin lymphoma ( 1606 [ 13% ] ) , and testicular cancer ( 1435 [ 12% ] ; table 1 )  . 
median follow - up was 143 years ( iqr 91223 ) in survivors of breast cancer , 202 years ( 128272 ) in survivors of cervical cancer , 177 years ( 117253 ) in survivors of testicular cancer , 193 years ( 123270 ) in female survivors of hodgkin lymphoma , and 196 years ( 121275 ) in male survivors of hodgkin lymphoma . 
investigation of all first primary neoplasm / subsequent primary neoplasm combinations with at least 100 subsequent primary neoplasms showed that neither age at diagnosis nor decade of diagnosis was systematically associated with aers , apart from age at diagnosis for breast cancer after female hodgkin lymphoma and decade of diagnosis for lung cancer after male hodgkin lymphoma ( appendix p 9 )  . 
 consequently , in this report we consider only variation of aers with years from diagnosis and sex . female survivors of breast cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 20 excess subsequent primary neoplasms per 10 000 person - years ( sir 18 , 95% ci 1718 ; aer 195 per 10 000 person - years , 95% ci 174215 ; table 2 )  . 
 sirs for subsequent primary cancers of ovarian , lung , corpus uteri , other genital , melanoma , and colorectal sites were statistically significantly increased ( table 3 )  . 
 the total aer of developing any subsequent primary neoplasm increased statistically significantly with time from breast cancer diagnosis to an aer of 256 per 10 000 person - years ( 95% ci 104408 ) subsequent to 30 years from diagnosis ( p < 00001 ; table 4 )  . 
consists of 80 small intestine , 62 gallbladder , 77 retroperitoneum and peritoneum , and 31 other or unspecified . table 3 : risk of specific subsequent primary neoplasms ( row headings ) after specific aya cancers * ( column headings ) with at least 200 subsequent primary neoplasms observed in total neoplasms ( total aer 289 per 10 000 person - years when negative aers are excluded )  . 
the total aer of developing any subsequent primary neoplasm increased with time from cervical cancer diagnosis to an aer of 323 per 10 000 person - years ( 95% ci 154491 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing lung , colorectal , and bladder cancer ( each vol 20 april 2019 articles 538 vol 20 april 2019 articles for the aers lung cancer p < 00001 ; table 4 )  . 
in patients who had survived at least ( 172 per 30 years , 10 000 person - years , 95% ci 88256 ) , colorectal cancer ( 107 , 35179 ) , and bladder cancer ( 101 , 45157 ) accounted for 37% , 23% , and 22% of the total number of excess neoplasms , respectively ( total aer 465 per 10 000 person - years when negative aers are excluded )  . 
 the cumulative lung , colorectal , and bladder neoplasms at 35 years from diagnosis were 36% ( 95% ci 3242 ) , 26% ( 2230 ) , and 13% ( 1016 ) , whereas incidences of 16% , 14% , and 04% were expected , respectively ( figure , table 5 )  . incidences of subsequent survivors of testicular cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 19 excess subsequent primary neoplasms per 10 000 person - years ( sir 18 , 95% ci 1719 ; aer 189 per 10 000 person - years , 95% ci 166211 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from testicular cancer diagnosis to an aer of 1270 per 10 000 person - years ( 95% ci 10001540 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing bladder , colorectal , lung , and prostate cancer ( each p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aers for prostate cancer ( 253 per 10 000 person - years , 95% ci 121386 ) , bladder cancer ( 228 , 130327 ) , colorectal cancer ( 196 , 92299 ) , and lung cancer ( 95 , 01188 ) accounted for 20% , 18% , 15% , and 8% of the total number of excess neoplasms , respectively . 
 incidences of subsequent primary the cumulative neoplasms at 35 years from diagnosis were 37% ( 95% ci 3144 ) for prostate , 29% ( 95% ci 2436 ) for bladder , 30% ( 2536 ) for colorectal , and 27% ( 2232 ) for lung , whereas incidences of 29% , 11% , 18% , and 20% were expected , respectively ( figure , table 5 )  . female survivors of hodgkin lymphoma had an excess risk of developing any subsequent primary neoplasm corresponding to 56 excess subsequent primary neoplasms per 10 000 person - years ( sir 31 , 95% ci 2933 ; aer 557 per 10 000 person - years , 95% ci 504611 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from hodgkin lymphoma diagnosis to an aer of 1686 per 10 000 person - years ( 95% ci 12952078 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing breast and lung cancer ( each p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aers for breast cancer ( 718 per 10 000 person - years , 95% ci 464972 ) and lung cancer ( 260 , 112408 ) accounted for 43% and 15% of the total number of excess neoplasms , respectively . 
the total aer of developing any subsequent primary neoplasm increased with time from hodgkin lymphoma diagnosis to an aer of 1219 per 10 000 person - years ( 95% ci 9131524 ) subsequent to 30 years from diagnosis ( p < 00001 ) , as did the aer for developing lung cancer ( p < 00001 ; table 4 )  . 
in patients who had survived at least 30 years , the aer for lung cancer ( 502 per 10 000 person - years , 95% ci 330673 ) accounted for 41% of the total number of excess neoplasms . 
the cumulative incidence of lung neoplasms in male survivors of hodgkin lymphoma was 51% ( 95% ci 4360 ) at 35 years from diagnosis , whereas an incidence of 14% was expected ( figure , table 5 )  . female survivors of thyroid cancer had an excess risk of developing any subsequent primary neoplasm corresponding to 13 excess subsequent primary neoplasms per 10 000 person - years ( sir 14 , 95% ci 1215 ; aer 131 per 10 000 person - years , 95% ci 84178 ; table 2 )  . 
the total aer of developing any subsequent primary neoplasm increased with time from thyroid cancer diagnosis to an aer of 219 per 10 000 person - years ( 95% ci 109 to 547 ) subsequent to 30 years from diagnosis , ( p = 003 ; table 4 )  . 
 the cumulative incidence of all subsequent primary neoplasms in female survivors of thyroid cancer was 182% ( 95% ci 161205 ) at 35 years from diagnosis ( table 5 ) , whereas an incidence of 136% was expected . 
the cumulative risks for the specific subsequent primary neoplasms add up to more than the overall cumulative risk because survivors can develop more than one subsequent primary neoplas * all subsequent primary neoplasms in female survivors excluding subsequent primary neoplasms of the breast . 
||all subsequent primary neoplasms in female survivors excluding subsequent primary neoplasms of the thyroid . table 5 : cumulative incidence of specific subsequent primary neoplasms after specific first primary neoplasms by years from diagnosis to 12 excess subsequent primary corresponding neoplasms per 10 000 person - years ( sir 14 , 95% ci 1215 ; aer 123 per 10 000 person - years , 95% ci 75171 ; table 2 )  . 
the cumulative incidence of all subsequent primary neoplasms was 139% ( 95% ci 122157 ) at 35 years from diagnosis ( table 2 ) , whereas an incidence of 123% was expected . both male and female survivors of cns tumours had an excess risk of developing any subsequent primary vol 20 april 2019 articles neoplasm corresponding to 15 and 11 excess neoplasms , respectively ( male survivors : sir 17 [ 95% ci 1519 ] ; aer 148 per 10 000 person - years [ 95% ci 107190 ] ; [ 1215 ] ; female survivors : sir 13 aer 111 [ 70152 ] )  . 
a statistically significant reduction in the sir for the development of a subsequent primary breast cancer was found ( sir 07 , 95% ci 0608 ; table 3 )  . 
the cumulative incidence of all subsequent primary neoplasms was 119% ( 95% ci 106133 ) in female survivors of cns tumours and 100% ( 87114 ) in male survivors of cns tumours at 35 years from diagnosis ( table 2 ) , whereas an incidence of 94% was expected . sensitivity analyses showed that inclusion of leukaemia after aya hodgkin lymphoma , non - hodgkin lymphoma , and leukaemia had little effect on the sirs and aers ( appendix p 10 )  . 
inclusion of sarcomas after aya softtissue sarcoma and bone tumour increased the aers , but there was substantial overlap in confidence intervals ( appendix p 10 )  . discussion we show that the excess number of subsequent primary neoplasms observed increases with increased period of follow - up from diagnosis after each aya cancer investigated . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma in women , breast cancer , and hodgkin lymphoma in men , we identified just a small number of specific subsequent primary neoplasms that account for 82% , 61% , 58% , 45% , and 41% of the total excess number of neoplasms , respectively . 
one study has previously addressed the risk of all subsequent primary neoplasms combined after each aya cancer , 3 but no study has previously considered specific subsequent primary neoplasms . in our study , the burden of the excess number of neoplasms beyond 30 years from diagnosis accounted for by lung cancer was substantial and apparent across all aya cancers investigated ( breast , cervical , testicular , and hodgkin lymphoma in males and females )  . 
additionally , smoking increases the risk of developing subsequent primary neoplasms , particularly oral or pharyngeal , oesophageal , stomach , lung , and haematological malignancies.21 kaul and colleagues22 reported that 33% of survivors of aya cancer were current smokers compared with 22% in a non - cancer comparison group matched on age , sex , and other factors . 
 although this decrease could be caused by a number of factors , it might be related to a change in smoking habits in more recent decades ( ie , a reduction in male smokers )  . 
 the evidence presented in our study , along with previous literature on smoking in cancer survivors , clearly suggests that clinical follow - up of survivors of aya cancer , particularly survivors of breast cancer , cervical cancer , and hodgkin lymphoma , should focus on subsequent lung cancer and provision of smoking cessation advice . generally , it is difficult to compare risks of subsequent primary neoplasms between survivors of aya and childhood cancer because there are so many important confounding influences . 
however , lung cancer as a subsequent primary neoplasm is an exception to this general rule in that from our population - based national cohort of survivors of childhood cancer in britain , we reported that in survivors aged 40 years and older , lung cancer was associated with an aer of only 29 per 10 000 person - years ( 95% ci 0455 ) , which accounted for just 9% of the total aer.28 by contrast , in the present analysis , the aer for lung cancer after at least 30 years from diagnosis of aya cancer was substantially higher and accounted for a much greater proportion of the total aer . 
notably , by contrast with survivors of aya cancer , the odds ratio for being a current regular smoker among survivors of childhood cancer in britain was 051 compared with the general population of britain.29 in female survivors of breast cancer , the sirs reported in our study were broadly consistent with those reported in previous literature.57 the increased risk of ovarian cancer could relate to shared hormonal and genetic ( eg , brca1 and brca2 mutations ) risk factors.30 the increased risk of uterine cancers might relate to partial oestrogen agonists used to treat the breast cancera previous large case - control study found that risk of uterine cancer increases with duration of tamoxifen treatment.31 of the six anatomical sites at which an excess of subsequent primary neoplasms was observed , only the lungs would be directly exposed if external - beam radiotherapy was used to treat the breast cancer . 
a previous large case - control study showed a dose - response relation between radiotherapy and risk of lung cancer in breast cancer survivors diagnosed at any age ( not aya - specific ) .26 existing literature suggests that chest 542 vol 20 april 2019 articles radiotherapy and smoking are both likely contributors to the substantial number of excess neoplasms accounted for by lung cancer . the bladder and bowel would be directly exposed if external - beam radiotherapy was used to treat cervical cancer . 
a large case - control study showed a doseresponse relation between radiotherapy and the risk of both bladder and rectal cancers in cervical cancer survivors.32 existing that pelvic irradiation and smoking are likely contributors to the number of excess neoplasms accounted for by lung , colorectal , and bladder cancer . 
clinical follow - up of survivors of aya cervical cancer , particularly where pelvic irradiation is used , should focus on lung , bowel , and bladder cancers . literature suggests treatment for testicular cancer can involve irradiating the para - aortic lymph nodes , which might explain the excess of subsequent primary neoplasms seen abdominal sites ( prostate , bladder , and colorectal )  . 
the excess of subsequent primary neoplasms observed in the abdomen is consistent with international studies of testicular cancer survivors.8 the excess of lung subsequent primary neoplasms might be caused by radiotherapy to the lungs , since previous studies have reported an increased risk of lung cancer in survivors of testicular cancer who were given chest radiotherapy.8 clinical follow - up of survivors of aya testicular cancer should focus on prostate , bladder , colorectal , and lung cancers . the lungs would be directly exposed if external - beam radiotherapy was used to treat hodgkin lymphoma ; previous studies of hodgkin lymphoma survivors have provided evidence of a dose - dependent increase in lung cancer risk with radiotherapy with or without chemotherapy.27 our findings are consistent with previous large - scale studies of female survivors of hodgkin lymphoma , for which a substantial amount of literature already exists , and by contrast with other aya cancers considered here , we have little to add.911 our findings support the decrease in lung cancer risk with more recent calendar period of diagnosis that was reported in a dutch study of hodgkin lymphoma survivors.9 this decrease might be due to a latency effect , where more recently diagnosed survivors simply have not had enough time to develop a lung subsequent primary neoplasm , or it might be caused by changes in treatment for hodgkin lymphoma during recent decades , including withholding the delivery of radiotherapy or radiotherapy resulting in less damage to healthy tissue than in previous decades.33 however , because a decrease in lung cancer risk was not seen after hodgkin lymphoma in women , it is possible that the decrease in lung cancer in men is caused by other environmental influences , such as changes in smoking habits . 
previous studies have reported an increase in the number of excess lung cancers with increasing years from diagnosis ; 9 , 10 however , to our knowledge , our study is the first to report the number of excess lung cancers in male and female improvements survivors separately . 
existing literature suggests that treatment ( radiotherapy and chemotherapy ) , in addition to smoking , could contribute to the number of excess neoplasms accounted for by lung cancer.9 clinical followup of male survivors of aya hodgkin lymphoma should focus on lung cancer and provision of smoking cessation advice . younger age at radiation exposure is a risk factor for the development of breast cancer in many populations exposed to radiation , including atomic bomb survivors , patients with tuberculosis monitored with x - rays , and children with benign disorders treated with radiotherapy.34 thus , the effect of age at diagnosis ( closely related to age at radiotherapy ) of hodgkin lymphoma on the risk of breast cancer in our cohort is not surprising . knowledge of late effects of cancer treatment has resulted in lower radiation exposures for treatments of good prognosis cancers in recent years ; 35 however , the multivariable regression showed the risk of developing a subsequent primary neoplasm did not vary with decade of diagnosis of aya cancer apart from lung cancer after hodgkin lymphoma in males . 
therefore , currently there is little evidence of a detectable impact . that until recently , no internationally agreed clinical guidelines existed regarding surveillance for specific types of neoplasm after aya cancer , but this is now being addressed by the international late effects of childhood cancer guideline harmonization group.36 so far , two such guidelines have been published.37 , 38 there are also guidelines in development relating to second primary cns tumours and second primary bowel cancers . strengths of our cohort study relate to its large scale and population - based design , with the inclusion of all 5 - year survivors of aya cancer in england and wales . 
our study had much greater statistical power than the only comparable previous study by lee and colleagues , 3 because we report almost double the number of subsequent primary neoplasms and an additional million person - years of follow - up . 
most previous studies investigating the risk of subsequent primary neoplasms with years from diagnosis have mainly focused on the sir , a measure of multiplicative risk that relates to an unspecified baseline risk and is therefore difficult to interpret . 
we concentrated on the aer , which is the excess number of subsequent primary neoplasms beyond those expected from the general population , and so is directly interpretable in terms of adverse health impact on survivors . 
to our knowledge , our study is the first to report aers by years from diagnosis for each specific aya cancer . a limitation of using cancer registration data is the absence of detailed treatment information . 
treatment for aya cancer varies greatly by cancer type ; therefore , in the absence of treatment data , we chose to determine risks in relation to specific cancer types . 
however , inevitably vol 20 april 2019 articles there is variation in the intensity of treatment given for a specific type of cancer , depending on the stage at diagnosis and whether the disease recurs or relapses after initial treatment . 
crude treatment information is inherent in cohort studies based on cancer registry data ; however , we are planning to conduct case - control studies with detailed treatment dosimetry , questionnaires for lifestyle and other relevant factors , and saliva collection for genotypic factors . 
a potential limitation of our study is that our results might not be generalisable to populations outside of england and wales . another limitation is the possibility that recurrence or metastases of the aya cancer could have been mistaken for a subsequent primary neoplas however , we used the iacr / iarc rules to define multiple primary cancers and further excluded any additional neoplasms close to the aya cancer site . 
thus , our estimate of the risk of specific subsequent primary neoplasms after specific aya cancers is probably conservative , and although many of the estimates we report are substantial , they are likely to be an underestimate of the true risk . in conclusion , our data show that the excess number of subsequent primary neoplasms observed increases with increased period of follow - up from diagnosis after each aya cancer investigated . 
in patients who had survived at least 30 years from diagnosis of cervical cancer , testicular cancer , hodgkin lymphoma , and breast cancer , we identified just a small number of specific subsequent primary neoplasms that account for high proportions of the total excess number of neoplasms . 
a notable finding was the excess number of neoplasms accounted for by lung cancer across all aya groups investigated in detail , in addition to subsequent primary neoplasms occurring in potentially irradiated sites . 
our findings provide an evidence base for clinical follow - up relating specifically to the aya population . contributors cjb did the literature search and data analysis , created the figure , and drafted the report . 
cjb , rcr , dlw , mmh , cf , dps , mgm , and abe interpreted the data , and reviewed and finalised the report . declaration of interests dps reports grants from teenage cancer trust , outside the submitted work . 
other funding was provided by a post - doctoral fellowship to rcr from the national institute for health research ( pdf - 2012 - 05 - 280 ) , and by the academy of medical sciences ( springboard health of the public 2040 ) and children with cancer uk . 
 study collaborators include sarah darby ( university of oxford ) ; richard feltbower ( university of leeds ) ; lorna anne fern ( university college london ) ; diana greenfield ( sheffield teaching hospital nhs foundation trust ) ; helen alexandra spoudeas ( university college london hospitals nhs foundation trust ) ; william hamish wallace ( royal hospital for sick children , edinburgh ) ; and jeremy whelan ( university college london hospitals nhs foundation trust )  . 
this report is independent research and the views expressed in this article are those of the author ( s ) and not necessarily those of nhs digital , cancer research uk , the national institute for health research , the office for national statistics , or the welsh cancer registry . editorial for more on the bbc report see health - 27894551 for the monitor report see government / publications / closing - the - nhs - funding - gaphow - to - get - better - valuehealthcare - for - patients for the times letter see letters / article4140238.ece nhs privatisation : a step too far according to a recent bbc report , englands national health service ( nhs ) will face a funding shortfall of about 2 billion by 2016 . 
projections in a report by monitor , the sector regulator for health - care services in england , suggest this de cit will rise to around 30 billion by 2021 . 
the e ect that this de cit will have on the nhs has not gone unnoticed : a letter to the times on july 7 , 2014 , signed by leaders from various royal colleges , stated that unless plans for meeting funding gaps were created , the nhs would be unable to cope . 
 clearly , urgent measures need to be taken if the nhs is to continue to be able to provide its mandated services , but worryingly the debate is increasingly looking to privatisation as a means of plugging these funding gaps . 
 this insidious slide towards outsourcing health care is not only a lazy , short - term solution to the immediate problems facing the nhs , but also potentially highly damaging to the provision of health care in the uk . 
 current tenders include catering or provision of health care in prisons ; however , a recent tender proposal by four general practitioner clinical commissioning groups ( ccgs ) in sta ordshire and stoke would see external contractors manage entire clinical cancer - care pathways for patients with bladder , lung , prostate , and breast cancer . 
the proposed removal of an entire care pathway to the private sector is a concerning development , partly because further dismantling of the nhs , and partly because it is indicative of how little thought has gone into the consequences . 
presumably , the contractor will not be expected to run departments peripherally involved in cancer care , or to invest in all of the attendant technologies , and , since the tender is only for 10 years , there would be little nancial incentive to do so . 
these measures will erode the nhs , leading to a failure to invest in sta ng and long - term infrastructureas seen in other sectors that have undergone partial privatisation . 
this scenario will become particularly acute over successive tenders , and especially damaging if winning bids are chosen predominantly on nancial grounds , or if a contractor fails and the government has to step in to handle the costly repercussions . 
for example , if care is outsourced only for patients with speci c types of cancer , what happens to those patients if metastases , comorbidities , or other complications arise ? individual patients risk being caught in a mixed - care model between private and public services for di erent aspects of their treatment , which could lead to disjointed care and unclear accountability . 
it would be unrealistic to not consider some elements of privatisationeg , discrete parts of the nhs that service clinical pathways , and where centralisation could improve consistency and quality . 
but to try to excise an entire clinical care pathway that has several links to other parts of the nhs is an ill - considered x to a complex issue , and will ultimately not serve those for whom the nhs was rst created . 
 the lancet oncology vol 15 august 2014 venetoclax in combination with cytarabine with or without idarubicin in children with relapsed or refractory acute myeloid leukaemia : a phase 1 , dose - escalation study seth e karol , thomas b alexander , amit budhraja , stanley b pounds , kristin canavera , lei wang , joshua wolf , jeffery m klco , paul e mead , soumyasri das gupta , su y kim , ahmed hamed salem , tammy palenski , norman j lacayo , ching - hon pui , joseph t opferman , jeffrey e rubnitz summary background outcomes for children with relapsed or refractory acute myeloid leukaemia remain poor . 
the bcl - 2 inhibitor , venetoclax , has shown promising activity in combination with hypomethylating agents and low - dose cytarabine in older adults for whom chemotherapy is not suitable with newly diagnosed acute myeloid leukaemia . 
we aimed to determine the safety and explore the activity of venetoclax in combination with standard and high - dose chemotherapy in paediatric patients with relapsed or refractory acute myeloid leukaemia . methods we did a phase 1 , dose - escalation study at three research hospitals in the usa . 
during dose escalation , participants received venetoclax orally once per day in continuous 28 - day cycles at either 240 mg / m or 360 mg / m , in combination with cytarabine received intravenously every 12 h at either 100 mg / m for 20 doses or 1000 mg / m for eight doses , with or without intravenous idarubicin ( 12 mg / m ) as a single dose , using a rolling - 6 accrual strategy . 
the primary endpoint was the recommended phase 2 dose of venetoclax plus chemotherapy and the secondary endpoint was the proportion of patients treated at the recommended phase 2 dose who achieved complete remission or complete remission with incomplete haematological recovery . 
the study is registered with clinicaltrials.gov ( nct03194932 ) and is now enrolling to address secondary and exploratory objectives . findings between july 1 , 2017 , and july 2 , 2019 , 38 patients were enrolled ( aged 322 years ; median 10 [ iqr 713 ] ) , 36 of whom received combination therapy with dose escalation , with a median follow - up of 71 months ( iqr 51112 )  . 
 the recommended phase 2 dose of venetoclax was found to be 360 mg / m ( maximum 600 mg ) combined with cytarabine ( 1000 mg / m per dose for eight doses ) , with or without idarubicin ( 12 mg / m as a single dose )  . 
among the 20 patients treated at the recommended phase 2 dose , 14 ( 70% , 95% ci 4688 ) showed complete response with or without complete haematological recovery , and two ( 10% ) showed partial response . 
the most common grade 34 adverse events were febrile neutropenia ( 22 [ 66% ] ) , bloodstream infections ( six [ 16% ] ) , and invasive fungal infections ( six [ 16% ] )  . 
overexpression of the anti - apoptotic bcl - 2 family of proteins is a documented mechanism of resistance in acute myeloid leukaemia and other malignancies.46 preclinical data show that inhibitors of bcl - 2 have activity against acute lines and patient - derived myeloid samples.4 , 6 , 7 encouraging results observed in older leukaemia cell patients for whom chemotherapy was not suitable , with newly diagnosed acute myeloid leukaemia , treated with the specific bcl - 2 inhibitor venetoclax in combination with hypomethylating agents8 or low - dose cytarabine , 9 led to recent approval of these combinations . 
published literature on acute myeloid leukaemia indicate that venetoclax in combination with low - dose cytarabine ( 20 mg / m per day ) or the hypomethylating agents decitabine and azacitidine have activity in adults who were treatment naive or had relapsed acute myeloid leukaemia . 
we found no published reports of the use of venetoclax alone or in combination with conventional acute myeloid leukaemia regimens in paediatric patients . added value of this study our results indicate that the specific bcl - 2 inhibitor , venetoclax , is safe and active in combination with conventional intensive chemotherapy in paediatric patients with relapsed acute myeloid leukaemia . 
the combination of venetoclax with highdose cytarabine with or without idarubicin in adults showed excellent activity in this heavily pretreated population , which was higher than in published data using venetoclax in alternative combinations ( with low - dose cytarabine or hypomethylating agents )  . 
to our knowledge , this is the first report of combination therapy with bcl - 2 inhibition and intensive chemotherapy in paediatric patients with acute myeloid leukaemia . implications of all the available evidence the results of this study support further evaluation of venetoclax in combination with intensive chemotherapy in paediatric patients with acute myeloid leukaemia . of acute myeloid leukaemia blasts , response to window therapy with venetoclax , leukaemic mutational pattern , and the clinical response to the combination of venetoclax and conventional high - dose chemotherapy . methods study design and participants in this phase 1 , dose - escalation study , patients were enrolled at three research hospitals in the usa , coordinated by st jude childrens research hospital , memphis , tn , usa ( appendix p 4 )  . 
patients were required to have greater than 5% bone marrow blasts , adequate organ function , and a performance status ( lanksy for patients aged 16 years , karnofsky for patients > 16 years ) of at least 50 , and to have recovered from previous therapy . 
patients low - dose cytarabine could receive hydroxyurea or ( 100 mg / m per day ) up to 24 h before the start of therapy but had to be 14 days from prior myelosuppressive therapy or gemtuzumab ozogamic patients were eligible to receive idarubicin if they had previously received less than 300 mg / m of doxorubicin equivalents ( using conversion ratios of 05 : 1 for daunorubicin , 5 : 1 for idarubicin , and 4 : 1 for mitoxantrone )  . 
further details are available in the protocol ( appendix pp 1153 )  . procedures we explored the safety of two dose levels of venetoclax ( abbvie ; north chicago , il , usa ) and two regimens of cytarabine with or without idarubicin using a rolling - 6 accrual strategy : 12 two to six participants could be concurrently enrolled onto a dose level , depending on the number of participants enrolled at that dose level , the number of participants who had intensity - limiting toxicity at the current dose level , and the number of participants enrolled at that dose level but with tolerability data pending . 
venetoclax was given orally once daily on days 128 , with a first dose level of 240 mg / m ( maximum 400 mg ) at dose levels 1 and 2b and escalated to 360 mg / m ( maximum 600 mg ) at dose levels 2a , 3 , and 4 . 
conventional chemotherapy began on day 8 , starting with intermediate - dose cytarabine ( 100 mg / m per dose every 12 h for 20 doses ) given intravenously at dose levels 1 and 2a , escalated to high - dose cytarabine ( 1000 mg / m per dose every 12 h for 8 doses ) given intravenously at dose levels 2b , 3 , and 4 . using the rolling - 6 design , six evaluable patients were enrolled before it was deemed that level 1 was tolerable . 
 after dose level 1 was deemed tolerable , new patients were enrolled in alternating fashion on dose levels 2a and 2b to evaluate the toxicity of increasing doses of either venetoclax ( dose level 2a ) or cytarabine ( dose level 2b )  . 
dose level 4 also included intravenous idarubicin ( 12 mg / m ) as a single dose and was opened to patients with limited prior anthra cycline exposure after dose level 3 was determined to be tolerated ( appendix pp 10 , 54 )  . 
at all dose levels , see online for appendix 552 vol 21 april 2020 articles 50% of the planned venetoclax dose was given on day 1 to mitigate potential tumour lysis syndrome . 
patients were admitted for monitoring during the first 2 days of therapy and then were monitored at least twice weekly with laboratory and clinical evaluations for toxicity until the completion of cycle 1 . intrathecal therapy with methotrexate , hydrocortisone , and cytarabine during diagnostic evaluation . 
the use of azole antifungals and other potent inhibitors of cyp3a4 was prohibited during treatment with venetoclax . institutional guidelines and patients received triple criteria for removing patients from trial therapy included the development of a dose - limiting toxicity ( determined by the treating physician ) , no response to therapy , relapse , second malignancy , and completion of the protocol therapy and evaluation period . toxicities were graded according to the common terminology criteria for adverse events version 4.03. 
any grade 3 or higher non - haematological event that was attributable to venetoclax was considered a dose - limiting toxicity , with the exception of grade 3 or 4 infection , grade 3 or 4 nausea , vomiting , or diarrhoea manageable with supportive care , or grade 3 or 4 electrolyte disturbance resolving to grade 2 or less within 7 days . 
 failure to recover an absolute neutrophil count of more than 300 per l or platelet count of 30 000 per l by day 50 was also deemed a dose - limiting toxicity unless it was attributable to underlying leukaemia or infection . 
 invasive fungal infection was categorised according to european organisation for research and treatment of cancer ( eortc ) consensus criteria with the addition of the category of suspected invasive fungal infection , comprising diagnosed invasive fungal infection with imaging findings consistent with the condition but not meeting eortc criteria.13 response was determined by bone marrow evaluation between days 35 and 49 . 
complete response was defined as the minimal residual disease being less than 5% with haematological recovery ( absolute neutrophil count 500 per l and platelets 75 000 per l ) , complete response with incomplete haematological recovery was when the minimal residual disease was less than 5% without haematological recovery , and partial response was a minimal residual disease of 525% with a greater than 50% decrease in leukaemic blast percentage . 
minimal residual disease testing and response evaluations were done in the department of pathology at st jude childrens research hospital , memphis , tn , usa . response to single - agent venetoclax was assessed by comparing absolute peripheral blood leukaemic blast counts on days 1 and 8 as determined by a flow cytometric - based minimal residual disease assay . 
in patients whose minimal residual disease was not evaluable in peripheral blood , single - agent response to venetoclax was evaluated using optional day 8 bone marrow evaluation ( n = 4 ) by comparing minimal residual disease in bone marrow before therapy and on day 8 . for bh3 profiling , cryopreserved blood or bone marrow cells were stained with leukaemia - specific antibodies and made permeable ( appendix p 1 )  . 
bad , hrk , and noxa peptides were tested for induction of cytochrome c loss from the mitochondria of leukaemic blasts that were made permeable to digiton dependence on bcl - 2 , bcl - xl , and mcl - 1 were determined by the relative release of cytochrome c due to the mitochondrial outer membrane becoming permeable in the presence of these agents as measured by multi colour flow - cytometry . blood samples were collected 2 , 4 , and 6 h after dose administration on days 1 and 2 , and before dosing ( 0 h ) and at 2 , 4 , and 6 h after dosing on day 8 to characterise venetoclax pharmacokinetics . 
the estimated pharmacokinetic parameters included the maximum plasma concentration ( cmax ) , the time to maximum concentration ( tmax ) , the area under the concentrationtime curve ( auc ) from time 0 to 6 h after dosing ( auc6 ) , and the area under the concentration time curve during the 24 - h dose interval ( auc24 )  . 
the pre - dose ( 0 h ) concentration was used as the 24 - h postdose concentration value at steady state on that same day vol 21 april 2020 articles previous therapies since last complete response 1 died of colitis and sepsis before response evaluation age in years , median ( iqr ) 10 ( 713 ) patients ( n = 38 ) 38 participants enrolled 2 did not receive combination therapy 1 viral infection during venetoclax window 1 rapid disease progression after 1 day ( half dose ) venetoclax female male previous complete response previous transplantation favourable genetics runx1 - runx1t1 cbfb / myh11 cebpa mutations neutral genetics tp53 monosomy 7 21 ( 55% ) 17 ( 45% ) 4 ( 11% ) 21 ( 55% ) 13 ( 34% ) 16 ( 42% ) 9 ( 24% ) 7 ( 18% ) 6 ( 16% ) 20 ( 53% ) 9 ( 24% ) 9 ( 24% ) 4 ( 11% ) 2 ( 5% ) 2 ( 5% ) 3 ( 8% ) 2 ( 5% ) 4 ( 11% ) 5 ( 13% ) 2 ( 5% ) 1 ( 3% ) kmt2a rearrangements 12 ( 32% ) adverse genetics flt3 internal tandem duplication flt3 point mutations bone marrow leukaemic burden at study entry , median ( iqr ) 33% ( 1868 ) data are in n ( % ) unless specified otherwise . table 1 : baseline characteristics in order to calculate auc24 . 
dose - normalised exposures were calculated using the dose received . patient - reported quality of life and hope measures were administered at baseline before the start of treatment , during the first week of therapy , and after completion of one cycle of venetoclax therapy . 
physical , emotional , and social health were assessed directly in patients aged 817 years , and in those aged 57 years using parent proxies with the 37 - item patient reported outcomes measurement information system ( promis ) pediatric profile.15 participants responded on the basis of their experience during the past 7 days , and raw scores were converted into age - normalised t - scores in each doma hopefulness and optimism were assessed using the herth hope index ( hhi ) 16 in adolescents and young adults ( aged 13 years ) and their parents.17 36 received combination therapy 35 evaluable participants figure : trial profile identification of outcomes the primary endpoint was the recommended phase 2 dose and was defined as the highest dose level at which six participants were treated with at most one experiencing a dose - limiting toxicity . 
prespecified exploratory objectives included bh3 profiling , pharmacokinetics , and quality of life assessments . statistical analysis statistical analysis was done using stata 15.1 ( statacorp ; college station , tx , usa ) using data available on aug 24 , 2019 . 
for the primary endpoint , the rolling - 6 design resulted in a minimum possible sample size of two patients if the first two patients each experienced a dose - limiting toxicity and a maximum sample size of 54 patients . 
participants without dose - limiting toxicities who received at least 21 of the planned 28 doses of venetoclax and at least 80% of the planned chemotherapy were also considered evaluable for toxicity . post - hoc analyses included the estimation of overall survival , analysis of associations between response to single - agent venetoclax ( including identification of an optimal threshold to define a good window response ) and overall response to combination therapy , and description of severe infection . 
overall survival was defined as the time from study enrolment to death , with living patients censored at the last follow - up , and was estimated by the kaplan - meier method . 
fishers exact test was used to compare the proportion of patients who achieved complete response or complete response with incomplete haematological recovery among patients who had good response to the window therapy with patients who had a poor response , and the kruksall - wallis test was also used . 
jer was responsible for the decision to submit the manuscript for publication . results between july 1 , 2017 , and july 2 , 2019 , 38 patients were enrolled , including four patients with primary refractory acute myeloid leukaemia , 33 patients with relapsed acute myeloid leukaemia , and one patient with relapsed mixedphenotypic acute leukaemia ( appendix p 2 )  . 
the median follow - up time was 71 months ( iqr 51112 ) and the median age was 10 years ( iqr 713 ) at enrolment ( table 1 )  . 
previous attempts of salvage therapy had been made in 18 relapsed patients , nine of whom had received at least two previous salvage attempts . two patients did not receive combination therapy because one had rapid disease progression and one had an infection precluding ongoing therapy ; both were excluded from further analyses ( figure )  . 
although the protocol allowed early initiation of chemotherapy in patients with disease progression during the venetoclax window , disease - induced organ dysfunction precluded ongoing therapy after the half - dose of venetoclax on day 1 , precluding evaluation of treatment - related toxicity or activity in the patient with rapid disease progression . 
 patients received one 28 - day cycle ( n = 30 ) , two cycles ( n = 5 ) , or four cycles ( n = 1 ) of treatment . all dose levels were tolerated , with only one doselimiting toxicity observed ( prolonged haemopoietic recovery in one patient at dose level 1 )  . 
there was one on - therapy death due to colitis and sepsis in a patient who had relapsed , was refractory to three previous courses of therapy , and had colitis during his previous course of therapy . 
the recommended phase 2 dose was therefore venetoclax 360 mg / m ( maximum 600 mg ) combined with cytarabine 1000 mg / m per dose with or without idarubicin 12 mg / m ( dose levels 3 and 4 ; table 2 )  . patients had a median of two ( iqr 03 ) grade 3 or higher toxicities during the first cycle of therapy , with infectious toxicities accounting for 42 ( 65% ) of 65 toxicities ( table 3 )  . 
tumour lysis syndrome was observed in one patient with rapidly progressive disease during the venetoclax window , who was taken off the study after one half - dose of venetoclax because of disease - induced multisystem organ dysfunction before combi nation therapy . 
 febrile neutropenia was common , with 43 episodes in 25 ( 66% ) of the 38 study participants ; 14 ( 33% ) of these episodes were associated with clinically or microbiologically documented infection . 
there were eight episodes of bloodstream infection in six ( 16% ) study participants during cycle 1 of therapy ; sepsis requiring urgent intervention occurred in six ( 75% ) of these eight episodes , severe sepsis in three ( 38% ) , and septic shock in two episodes ( 25% )  . 
data are in n ( % )  . table 3 : patients with encing non - haematological toxicities during cycle 1 of therapy response ( table 2 ; appendix p 5 )  . 
the median time to haematological recovery in patients achieving a complete response was 38 days ( iqr 3539 ) to an absolute neutrophil count greater than 300 per l and 385 days ( 3243 ) to more than 30 000 platelets per l . 
among the 12 evaluable patients who received intermediate - dose cytarabine ( dose levels 1 and 2a ) , four ( 33% , 95% ci 1065 ) had complete response with or without complete haematological recovery and two had a partial response , making the overall response rate 50% ( 2179 ; table 2 )  . 
among the 23 patients who received high - dose cytarabine with or without idarubicin ( dose levels 2b , 3 , and 4 ) , 16 ( 70% , 4787 ) had a complete response with or without complete haematological recovery and two had a partial response , making the overall response rate 78% ( 5693 ; table 2 )  . 
among the 20 evaluable patients who were the recommended phase 2 dose ( levels 3 and 4 ) , 14 ( 70% ; 95% ci 4688 ) had a complete response with or without complete haematological recovery and two had a partial response , so that the overall response rate was 80% treated at 556 vol 21 april 2020 articles ( 95% ci 5694 )  . 
of the 22 patients who were refractory to previous therapy ( including four primary refractory and 18 relapsed or refractory patients ) , six had a complete response and four had a complete response with incomplete haematological recovery , giving a combined complete response rate of 45% ; responses were seen in patients refractory to one ( n = 6 ) , two ( n = 3 ) , and four ( n = 1 ) previous regimens . 
in a post - hoc analysis , better response to the window was associated with achieving a complete response ( with or without complete haematological recovery ) at the end of cycle 1 ( kruskalwallis p = 0045 )  . 
a receiver operating curve identified an optimal cut - off of at least a 50% reduction in blasts to identify patients likely to achieve a complete response with or without complete haematological recovery . 
this cut - off correctly classified 74% with a sensitivity of 84% and a specificity of 57% ( appendix p 7 )  . in post - hoc analyses , 16 ( 73% , 95% ci 5089 ) of the 22 patients who had a good response to the venetoclax window ( > 50% blast reduction ) had complete response with or without complete haematological recovery ( 13 had complete response and three had complete response with incomplete haematological recovery ) ; by contrast , three ( 27% , 661 ) of the 11 patients with a poor response to the window therapy had a complete response ( p = 0017 by fishers exact test ; appendix pp 3 , 8 )  . 
 ten ( 45% ) of the 22 patients with a good window response were minimal residual disease negative after cycle 1 , compared with only two ( 18% ) of the 11 patients with poor response ( p = 025 )  . 
when analysis was restricted to patients treated at the recommended phase 2 dose ( dose level 3 or 4 ) , 12 ( 86% , 95% ci 5798 ) of the 14 patients with a good window response had a complete response ( 11 had complete response , one had complete response with incomplete haematological recovery , and nine were minimal residual disease negative ) , whereas two ( 40% , 585 ) of the five patients with a poor window response had a complete response ( one was minimum residual disease negative ) , giving a p value of 0084 for complete response and a p value of 014 for being minimal residual disease negative . ( kmt2a rearrangements ) , runx1 - runx1t1 fusions , nf1 mutations , and biallelic cebpa , ptpn11 , dnm2 , and nras mutations ( table 1 ; appendix pp 2 , 5 )  . 
among the 12 patients with neutral genetic alterations four had a complete response , one had complete response with incomplete haematological recovery , one had partial response , and five patients had no response . 
in the patients with adverse genetic alterations , the four patients with tp53 mutations showed two complete responses , one complete response with incomplete haematological recovery , and one partial response , and none of the five patients with flt3 alterations responded . the venetoclax bh3 dependency profiling prior to protocol therapy was available for 19 patients . 
no patients had leukaemia primarily dependent on mcl - 1 , although one patient who was more dependent on bcl - xl or bcl - 2 also showed some dependence on mcl - 1 . 
the nine patients with bcl - 2 dependence included five patients with complete response and one with complete response with incomplete haematological recovery ( combined complete response rate of 67% ) , one with partial response , and two with no response . 
 of the two patients who had not responded by the end of the cycle , one showed a poor response to window therapy and profiling following cycle 1 , and showed a switch to bcl - xl dependence . 
of the five patients with bcl - xl dependence , one had complete response , one had complete response with incomplete haematological recovery ( combined complete response rate of 40% ) , one had partial response , and two showed no response . 
patients with minimal or no in vitro bh3 dependence included one with complete response and one with partial response ( both showing minimal response to bcl - 2 ) , and three with no response ( appendix p 3 )  . recurrent genetic lesions in this relapsed population included flt3 alterations , kmt2a rearrangements , tp53 mutations , wt1 mutations , cbf / myh11 , and pharmacokinetic data was available for ten patients , including six patients on dose level 3 and four patients on dose level 4 . 
the median time to maximal venetoclax vol 21 april 2020 articles concentration was 6 h ( iqr 66 ) , with maximal concentrations increasing across each day measured : 07 g / ml ( sd 07 ) on day 1 , 14 g / ml ( sd 09 ) on day 2 , and 22 g / ml ( sd 14 ) on day 8 . 
pharmacokinetic parameters were similar across age groups ; day 8 aucs24 were 219 g * h / ml and 343 g * h / ml in two children younger than 6 years , 535 g * h / ml ( sd 407 ) in five children aged 712 years , and 419 g * h / ml ( sd 197 ) in three children aged 13 years or more . 
pharmacokinetic parameters were also similar across weight groups and with and without idarubicin ( appendix p 9 )  . quality of life scores were within the average range for nearly all domains at baseline ( appendix pp 34 ) , although mobility concerns were higher at baseline per parent report . 
 descriptive statistics suggested that parents and adolescent patients endorsed hopefulness at all timepoints ( appendix pp 34 )  . discussion to our knowledge , this is the first study of venetoclax in children and young adults with relapsed acute myeloid leukaemia . 
we found that the combination of venetoclax and high - dose cytarabine with or without idarubicin was well tolerated and active , with 14 ( 70% ) of the 20 evaluable patients who were treated at the recommended phase 2 dose showing complete response with or without complete haematological recovery after one cycle of therapy . 
the overall response rate of patients treated at the recommended phase 2 dose ( 80% ) was similar to that observed in the aml 2001 / 01 study20 ( using fludarabine , cytarabine , and g - csf with or without liposomal daunorubicin ) of patients in first relapse ( 75% ) , despite the greater prior therapy burden in our population . 
additionally , the proportion of patients who had complete response ( with complete haematological recovery ) after one cycle of therapy at the recommended phase 2 dose ( 65% ) in this study was similar to that obtained after two cycles of intensive therapy in aml 2001 / 01 ( 59% ) .20 this complete response estimate also compared favourably to that reported in aaml1421 ( using cpx - 351 ) after one cycle of therapy ( 57% ) .21 the low availability of patients with relapsed acute myeloid leukaemia for randomised trials makes direct prospective comparisons between retrieval therapies impractical . 
the haematological parameters used to define count recovery in our study have been used in previous studies by our group.22 although differences between these parameters and those used by other groups might result in slight differences in the definitions of response , the ability of patients to proceed to trans plantation following attainment of a complete response ( with or without complete haematological recovery ) on therapy suggests that the definitions used within the trial adequately identified patients whose response enabled more definitive therapy . included febrile neutropenia despite our patient population being heavily pretreated , the side - effect profile of the combination was consistent with toxicities seen with intensive chemotherapy in this in a population and proportion of patients that is similar to previous studies at our institution in patients with relapsed acute myeloid leukaemia.22 , 23 one ( 3% ) of 38 patients died due to infectious complications , which is a proportion similar to that seen in studies of patients with first relapse of acute myeloid leukaemia.20 in addition to the objective tolerability of the regimen , survey results from patients and parents indicated that the therapy did not adversely affect quality of life . 
patients and their parents also maintained normal herth hope index scores throughout the first cycle , suggesting that the adverse effects did not diminish either hope or quality of life . a similar proportion of patients in this study had grade 3 or 4 infections to those reported in previous relapsed acute myeloid leukaemia trials ( 289% vs 194% ) .20 the overall number of invasive fungal infections ( six patients ; 16% ) was similar to that in other paediatric patients with relapsed leukaemia.24 however , the impact of each infection was high ; three of the six participants with invasive fungal infection discontinued venetoclax therapy because of the infection . 
notably , the prohibition on azole use during the study precluded both azole prophylaxis and treatment of invasive fungal infection ; the use of azoles in future studies ( combined with lower doses of venetoclax due to interactions via cytochrome p450 3a4 ) 25 might address this issue . than with our data suggest that complete responses might be more frequent when venetoclax is combined with highdose chemotherapy intermediate - dose cytarabine . 
this finding is consistent with data from studies of venetoclax in adults with relapsed acute myeloid leukaemia.10 in that retrospective cohort , objective responses were seen in only 21% of patients treated with combinations of venetoclax and either hypomethylating agents or low - dose cytarabine . 
our data are also consistent with preclinical data showing synergy between venetoclax , cytarabine , and idarubicin , with greater synergy observed with higher doses of chemotherapy.26 despite the responses being encouraging overall , discreet subsets of patients experienced poor responses . 
this finding is consistent with previous reports in which flt3 - activated samples were resistant to venetoclax.27 combining venetoclax with flt3 inhibitors is an attractive therapeutic approach for these patients.28 additional previously proposed mechanisms of resistance to venetoclax were also observed in our patients , with exclusively bcl - xl dependent samples having poor responses to therapy and one patient converting from bcl - 2 dependence to 558 vol 21 april 2020 articles bcl - xl dependence after one cycle of therapy . 
 this finding aligns with preclinical data , in which resistance to bcl - 2 inhibition often occurred through family transition members.7 , 29 , 30 to reliance on other bh3 the body surface area - based dosing of venetoclax in this study resulted in similar venetoclax concentrations across different age and weight groups . 
in addition , the venetoclax concentrations in this study were similar to those observed in the adult acute myeloid leukaemia subjects.9 this finding indicates that body surface areabased dosing adequately accounts for the developmental pharmacokinetics of venetoclax . 
idarubicin showed no effect on venetoclax pharmacokinetics in this study . the limitations of this study include the hetero geneous patient population in terms of previous therapy , genetics , and bh3 dependency , as well as the small number of patients treated at each dose level . 
future studies should evaluate not only the activity of such combinations , but should also seek to validate leukaemic blast reduction and bh3 dependencies as biomarkers of response to combination therapy . contributors sek participated in the design of the trial , took care of patients on the trial , analysed data , and wrote the manuscript . 
tba , jw , njl , and c - hp participated in the design of the trial , took care of patients on the trial , and reviewed the manuscript . 
ab , jmk , pem , sdg , and jto participated in the design of the trial , performed laboratory studies associated with the trial , and reviewed the manuscript . 
 jer was the principal investigator of the trial , took care of patients on the trial , analysed data , and reviewed the manuscript . declaration of interests tba received travel funds from abbvie . 
jto and jer report research funding from abbvie and gateway for cancer research during the conduct of the study , and jto received additional funding from abbvie outside the submitted work . 
the data used to generate this article will be made available at the time of article publication ; investigators who seek access to individual level de - identified data should contact the computing team in the department of biostatistics at st jude childrens research hospital ( clintrialdatarequest@stjude.org ) who will respond to the data request . acknowledgments this study was funded by the cancer center support from the national institutes of health ( grant p30 ca021765 ) , the american lebanese syrian associated charities ( alsac ) , abbvie , and gateway for cancer research . 
we thank lauren wheeler and christie daniels for data collection and management . global elimination of cervical cancer is achievablewith commitment on sept 6 , 2019 , who called on countries in the southeast asia region to accelerate their efforts towards cervical cancer elimination . 
improvements in screening , diagnosis , and treatment are urgently needed , but widespread vaccination against human papillomavirus ( hpv ) will have the largest effect towards eliminating the disease . a modelling study published in the lancet oncology showed that if hpv vaccination and screening are quickly implemented in low - income and middle - income countries ( lmics ) , 125134 million cervical cancer cases could be avoided by 2069 . 
in the lancet public health , researchers showed how a national immunisation scheme with early adoption and high coverage , along with a national hpv screening programme , was on track to eliminate cervical cancer in australia ( < 4 cases per 100 000 by 2028 and < 1 case per 100 000 by 2066 )  . 
 crucially , long - term maintenance of these programmes , with support from the government and communities , would be required to sustain low cervical cancer incidence and mortality . among countries in south - east asia , bhutan , maldives , sri lanka , and thailand have introduced national hpv vaccination ; however , one glaring omission is india , which has the largest population in the region . 
in this issue of the lancet oncology , rengaswamy sankaranarayanan and colleagues highlight barriers to implementing a national hpv vaccination programme in india and the status of prevention efforts there . 
although the hpv vaccine was licensed in india in 2008 , state government - sponsored vaccination pro grammes in the states of andhra pradesh and gujarat and a clinical trial were suspended in 2010 after the deaths of several girls who were vaccinated . 
 despite evidence refuting a causal link between the deaths and the vaccine , and against recommendations from the indian national technical advisory group on immunisation , availability and uptake of the hpv vaccine has been severely hindered since then . 
moreover , because cervical cancer incidence has fallen in parts of india , arguments have been inappropriately made that vaccination and screening are not needed . similar to hpv vaccination , in south - east asia , only bhutan , indonesia , maldives , sri lanka , and thailand have widespread or national cervical cancer screening programmes . 
bangladesh is a lowresource country and this plan is an encouraging start , but whether it is ambitious enough to achieve cervical cancer control remains to be seen . reported even with high screening and vaccination coverage , cervical cancer elimination will take time , and substantial numbers of women will require treatment for the disease ; thus , improvements here are also needed . 
for example , to overcome costs of the hpv vaccine itself , both indian and chinese pharmaceutical companies are trialling generic hpv vaccines to provide more affordable alternatives to currently available formulations . national , publicly funded hpv vaccination programmes , high uptake of vaccination and screening , and access to high - quality diagnosis and treatment , are essential to tackle the global burden of cervical cancer . 
we were completely oversubscribed ; i was astonished to see the need out there , he said . those in the early stages of their career are particularly susceptible to budget cuts . 
that is a cost of the pandemic that we cannot begin to put a value on . talha khan burki cuts in cancer research funding due to covid - 19 on dec 8 , 2020 , cancer research uk ( cruk ) announced cuts of 45 million to its research budget . 
 the charity has been badly affected by the covid - 19 pandemic , which forced the cancellation of fundraising events and the suspension of trading at the 600 cruk shops across the country . 
we are planning for a managed decrease in spending on research from pre - covid levels of 400450 million to somewhere around 250 million , said iain foulkes , cruks executive director of research and innovation . 
cruk is responsible for roughly half of publicly funded research into cancer in the uk . the latest round of cuts amount to 12 fewer fellowships , 24 fewer 5 - year research programmes , and 68 fewer projects , which are typically 3 - year programmes . 
it is hard to imagine a scenario in which these measures do not have serious consequences . in the short - term , we are going to see an impact on patient outcomes because of the reduced number of trials ; in the long - term , because we will not be able to fund as much discovery science , we are going to see our ability to develop new drugs diminish , foulkes told the lancet oncology . 
he raised the prospect of a lost generation of cancer researchersmen and women deprived of the opportunity to make the breakthroughs that drive the field forward . the association of medical research charities predicts that it will take more than 4 years for spending in the sector to return to pre - pandemic levels , and a decade to rebuild lost capacity and capability . 
although the medical research council ( mrc ) might be able to make up some of the shortfall caused by the contraction at cruk , given that the mrcs total research expenditure in 201718 was 814 million , it is unlikely to be able to cover the 150 million of research funding that cruk expects to cut . the situation is similar outside the uk . 
the canadian cancer society has predicted that the pandemic will cost them ca$100 million in lost donations during the ongoing financial year , which amounts to more than half their budget . 
the charity has cut its expenditure on new research from $100 million to $50 million . government funding contributes a larger proportion of total expenditure on medical research in the usa than in the uk . 
the nih has been something of a backstop ; they even provided supplemental awards to people who had lost fellowships , said ross levine , who runs a laboratory focusing on myeloid malignancies at memorial sloan kettering cancer center ( new york , ny , usa )  . 
 nonetheless , covid - 19 has put severe pressure on the academic sector . many institutions are not hiring new faculty this year ; after last years freezes , that makes at least 2 years in which there has been a significant decline in recruitment , said levine . 
i am also hearing a lot of stories about young investigators vol 22 january 2021 news corrections correction to lancet oncol 2012 ; 13 : 817 , 818 , 822 correction to lancet oncol 2014 ; 15 : 1195206 correction to lancet oncol 2015 ; 16 : 52 shen q , fan j , yang x - r , et al . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . vol 16 january 2015 corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 corrections correction to lancet oncol 2014 ; 16 : 767 correction to lancet oncol 2016 ; 17 : 431 , 434 , 435 correction to lancet oncol 2016 ; 17 : 953 weber js , geo gibney , sullivan rj , et al . 
 sequential administration of nivolumab and ipilimumab with a planned switch in patients with advanced melanoma ( checkmate 064 ) : an open - label , randomised , phase 2 trial . 
lancet oncol 2016 ; 17 : 94355in gure 5 , under the headings nivolumab followed by ipilimumab and ipilimumab followed by nivolumab , the text should have read number of events / number of patients . 
this correction has been made to the online version as of june 28 , 2016 , and the printed version is correct . correction to lancet oncol 2016 ; 17 : 995 , 1002 cella d , grnwald v , nathan p , et al . 
 quality of life in patients with advanced renal cell carcinoma given nivolumab versus everolimus in checkmate 025 : a randomised , open - label , phase 3 trial lancet oncol 2016 ; 17 : 9941003in this article , the order of references 711 has been corrected and the fourth sentence of the second paragraph of the introduction has been corrected to read furthermore , an analysis of hrqol scores according to the functional assessment of cancer therapy - kidney symptom index - disease related symptoms ( fksi - drs ) questionnaire ( a subscale of the 15 - item fksi - 15 ) showed that median change from baseline increased over time with nivolumab treatment . 
these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . jeong s - y , park jw , nam bh , et al . 
open versus laparoscopic surgery for mid - rectal or low - rectal cancer after neoadjuvant chemoradiotherapy ( corean trial ) : survival outcomes of an open - label , non - inferiority , randomised controlled trial . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2015 ; 16 : 1479 motzer rj , hutson te , glen h , et al . 
lancet oncol 2015 ; 16 : 147382in table 3 of this article , the number of patients in the lenvatinib plus everolimus group with grade 3 constipation should be 0 . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 351 untch m , jackisch c , schneeweiss a , et al . 
 lancet oncol 2016 ; 17 : 34556in this article , the data in the second sentence of the third paragraph of the results section should have read in multivariable logistic regression analysis , nab - paclitaxel remained an independent predictor for achievement of pathological complete response after adjustment for baseline and minimisation factors ( or 159 ; 95% ci 120211 ; p = 00013 )  . 
fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment o f h o r m o n e r e c e p t o r p o s i t i v e , her2 - negative metastatic breast cancer that progressed on previous endocrine therapy ( paloma - 3 ) : final analysis of the multicentre , doubleblind , phase 3 randomised controlled trial . 
lancet oncol 2016 ; 17 : 42539 in figures 2a , 5a , 5b , and 5c , the kaplan - meier curves should have intersected with the y - axis at the 100% mark . 
these corrections have been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 888 , 890 , 892 cancer antonia sj , lpez - martin ja , bendell j , et al . 
 lancet oncol 2016 ; 17 : 88395in this article , the rst line in the third paragraph of the results , blinded independent central review should have been investigator - assessed recist . 
in the seventh paragraph of the results , the number of patients in the nivolumab 3 mg / kg plus ipilimumab 1 mg / kg cohort who had diarrhoea as a serious adverse event should have been two ( 4% ) , not four ( 7% )  . 
 these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . vol 17 july 2016 e270 3 versus 6 months of adjuvant oxaliplatin - fluoropyrimidine combination therapy for colorectal cancer ( scot ) : an international , randomised , phase 3 , non - inferiority trial timothy j iveson * , rachel s kerr * , mark p saunders , jim cassidy , niels henrik hollander , josep tabernero , andrew haydon , bengt glimelius , andrea harkin , karen allan , john mcqueen , claire scudder , kathleen anne boyd , andrew briggs , ashita waterston , louise medley , charles wilson , richard ellis , sharadah essapen , amandeep s dhadda , mark harrison , stephen falk , sherif raouf , charlotte rees , rene k olesen , david propper , john bridgewater , ashraf azzabi , david farrugia , andrew webb , david cunningham , tamas hickish , andrew weaver , simon gollins , harpreet s wasan , james paul summary background 6 months of oxaliplatin - containing chemotherapy is usually given as adjuvant treatment for stage 3 colorectal cancer . 
we investigated whether 3 months of oxaliplatin - containing chemotherapy would be non - inferior to the usual 6 months of treatment . methods the scot study was an international , randomised , phase 3 , non - inferiority trial done at 244 centres . 
 patients aged 18 years or older with high - risk stage ii and stage iii colorectal cancer underwent central randomisation with minimisation for centre , choice of regimen , sex , disease site , n stage , t stage , and the starting dose of capecitabine . 
this trial is registered with isrctn , number isrctn59757862 , and follow - up is continuing . findings 6088 patients underwent randomisation between march 27 , 2008 , and nov 29 , 2013 . 
nine patients in the 3 month group and 14 patients in the 6 month group did not consent for their data to be used , leaving 3035 patients in the 3 month group and 3030 patients in the 6 month group for the intention - to - treat analyses . 
at the cutoff date for analysis , there had been 1482 disease - free survival events , with 740 in the 3 month group and 742 in the 6 month group . 
3 year disease - free survival was 767% ( 95% ci 751782 ) for the 3 month group and 771% ( 756786 ) for the 6 month group , giving a hazard ratio of 1006 ( 09091114 , test for non - inferiority p = 0012 ) , significantly below the non - inferiority marg peripheral neuropathy of grade 2 or worse was more common in the 6 month group ( 237 [ 58% ] of 409 patients for the subset with safety data ) than in the 3 month group ( 103 [ 25% ] of 420 ) and was long - lasting and associated with worse quality of life . 
1098 serious adverse events were reported ( 492 reports in the 3 month group and 606 reports in the 6 month group ) and 32 treatment - related deaths occurred ( 16 in each group )  . interpretation in the whole study population , 3 months of oxaliplatin - containing adjuvant chemotherapy was noninferior to 6 months of the same therapy for patients with high - risk stage ii and stage iii colorectal cancer and was associated with reduced toxicity and improved quality of life . 
despite the fact the study was underpowered , these data suggest that a shorter duration leads to similar survival outcomes with better quality of life and thus might represent a new standard of care . 
the scot study was designed to test for the non - inferiority of 3 months of treatment compared with the standard 6 month duration . added value of this study worldwide , six studies have addressed this research question , of which scot is the largest . 
peripheral neuropathy was significantly worse in the 6 month group and reducing the treatment duration to 3 months more than halved the number of grade 3 or 4 peripheral neuropathy events reported . 
moreover those patients who were most severely affected by peripheral neuropathy also had a significant reduction in quality of life . implications of all the available evidence in view of the results of the scot study and the meta - analysis of all six worldwide studies conducted by the idea collaboration , 3 months of adjuvant chemotherapy will become the new global standard of adjuvant treatment for most patients who are suitable for treatment with capox , particularly those patients with t13 , n1 disease . the major cumulative chronic toxic effect of oxaliplatincontaining chemotherapy is sensory peripheral neuropathy , which can be disabling . 
this effect is recognised to be dependent on dose and duration and can be long - lasting.8 , 9 as most patients undergoing adjuvant chemotherapy are cured and will survive , long - term , irreversible peripheral neuropathy is a significant issue . the current standard duration of adjuvant chemo therapy for colorectal cancer is 6 months . 
a shorter duration of adjuvant chemotherapy would be expected to result in less chronic peripheral neuropathy , but it has been hitherto unknown to what , if any , extent cutting duration would compromise its efficacy . 
the results of one study10 using fluoropyrimidine alone , which was not powered for non - inferiority , suggested that 3 months of infused fluoropyrimidine was similar to 6 months of bolus fluoropyrimidine treatment in terms of disease - free survival.10 the scot study was designed as a stand - alone international phase 3 non - inferiority study to investigate whether 3 months of oxaliplatin - based adjuvant chemotherapy for colorectal cancer is non - inferior to 6 months of treatment with the same regimen . 
here we report the final efficacy results of disease - free survival and the toxicity and quality - of - life ( qol ) results . methods study design and participants the scot study is an international , randomised , nonblinded , non - inferiority , phase 3 trial comparing 6 months versus 3 months of oxaliplatin and fluoropyrimidine adjuvant chemotherapy in patients with high - risk stage ii or stage iii colorectal cancer . 
patients were recruited from 244 centres in six countries ( the uk , denmark , spain , sweden , australia , and new zealand )  . patients were eligible if they were aged 18 years or older and had undergone a curative resection for stage iii or high - risk stage ii ( defined as having one or more of t4 disease , tumour obstruction with or without perforation of the primary tumour preoperatively , fewer than ten lymph nodes harvested , poorly differentiated histology , perineural invasion , or extramural venous or lymphatic vascular invasion ) adenocarcinoma of the colon or rectupatients were enrolled within 11 weeks of surgery and started treatment on their allocated study group within 2 weeks of randomisation . 
other eligibility inclusion requirements included who performance status 0 or 1 , adequate organ function , and life expectancy of greater than 5 years with reference to noncancer related diseases . 
patients had to have a normal ct scan of the chest , abdomen , and pelvis before study enrolment and carcinoembryonic antigen less than 12 times the local upper limit of normal ( uln ) within 1 week before randomisation . 
exclusion criteria included chemotherapy ( except chemotherapy administered with curative intent that was completed > 5 years ago and from which there were no residual complications ) , previous long - course chemo radiotherapy ( preoperative short - course radiotherapy alone was allowed ) , moderate or severe renal impair ment ( glomerular filtration rate or creatinine clearance < 30 ml / min , as calculated with the cockcroftgault equation ) , haemoglobin less than 9 g / dl , absolute neutrophil count less than 15 10 cells per l , platelet count less than 100 10 cells per l , and aspartate aminotransferase or alanine aminotransferase greater than 25 times the uln . 
this study was approved by the west glasgow research ethics committee ( version 1.1 of the protocol ) on jan 21 , 2008 , and all subsequent amendments approved by the committee , where required ( rec reference number 07 / s0703 / 136 )  . 
 randomisation and masking by use of a minimisation algorithm incorporating a random component , patients were centrally randomly assigned ( 1 : 1 ) , to receive either 3 months or 6 months of treatment . 
the minimisation factors were centre , choice of regimen , sex , disease site ( colon vs rectum ) , n stage ( x , 0 , 1 , or 2 ) and t stage ( x , 0 , 1 , 2 , 3 , or 4 ) and , if the patient was going to receive the capox ( capecitabine and oxaliplatin ) regimen , the starting dose of capecitabine ( from feb 1 , 2010 )  . initially some participating centres were randomly allocated to randomise patients after completion of the first 3 months of treatment to either receive a further 3 months treatment or to stop treatment . 
this approach was stopped because of a poorer randomisation rate ( ie , fewer patients randomised per month ) compared with centres that randomised patients before the start of treatment.11 participants were enrolled by authorised clinicians , after obtaining patient consent , by contacting the cancer research uk clinical trials unit in glasgow , uk , to check eligibility and request an allocation . 
 the study was open - label for patients , clinicians , and those doing the data analysis . procedures patients were assigned to receive oxaliplatin - containing adjuvant treatment for either 3 months or 6 months . 
 the chemotherapy regimen , which could be folfox ( bolus and infused fluorouracil with oxaliplatin ) or capox , was chosen by the physician and patient and was not randomised . for patients receiving folfox , treatment was given every 2 weeks with the intention of delivering six cycles to patients assigned 3 months of therapy and 12 cycles to patients assigned 6 months of therapy . 
intravenous oxaliplatin 85 mg / m was given over 2 h on day one concurrently with l - folinic acid 175 mg or folinic acid ( leucovorin ) 350 mg . 
this was followed by an intravenous bolus injection of fluorouracil 400 mg / m over 5 min , then a continuous intravenous infusion of fluorouracil 2400 mg / m over 46 h . 
at the investigators discretion , patients receiving folfox who were older than 70 years could start on the bolus and continuous infusion of fluorouracil at 75% of the starting dose , if clinically indicated . for patients receiving capox , treatment was given every 3 weeks with an intention of delivering four cycles to patients assigned 3 months of therapy and eight cycles to patients assigned 6 months of therapy . 
patients older than 70 years could be considered for treatment with capecitabine at 75% of the full dose , but the decision to reduce dose was left to the discretion of the investigator , depending on the fitness of the individual patient . 
if the clinician felt that any other patient required a - priori dose reduction because of any other comorbidity , that patient could be started on a minimum starting dose of oral capecitabine 800 mg / m twice per day . 
 toxicity was assessed by the investigators after each cycle of chemotherapy treatment and graded by use of national cancer institute common terminology criteria for adverse events ( ctcae ) version three . 
for capox , if more than one delay or a delay of at least 2 weeks occurred , capecitabine and oxaliplatin doses were reduced by 25% and , if further delays occurred due to myelotoxicity , further dose reductions were allowed at the investigators discretion . 
for folfox , if more than one delay or a delay of at least 2 weeks occurred , doses of oxaliplatin and infused fluorouracil were maintained , but the bolus fluorouracil was omitted and , if further delays occurred due to myelotoxicity , the oxaliplatin and infusional fluorouracil doses were reduced by 25% . 
 also for folfox , if after the first cycle neutrophils were less than 10 10 cells per l , the bolus fluorouracil was omitted and the oxaliplatin and infused fluorouracil doses were reduced by 25% . 
patients were followed up for 8 years with full blood count , urea and electrolyte , liver function , and carcinoembryonic antigen tested at months 9 , 12 , 18 , 24 , and 36 , then 564 vol 19 april 2018 articles annually . 
ct of the chest , abdomen , and pelvis was done at months 6 , 12 , 18 , 24 and 36 . qol was assessed with the european organisation for research and treatment of cancer ( eortc ) qlq - c30 and qlq - cr29 and eq - 5d - 3l ( visual analogue scale and health index ) , with uk value sets.12 neuropathy was assessed with the fact / gog - ntx4 questionnaire . the qol questionnaires were administered at baseline and before each treatment cycle . 
subsequent assessments were made at months 9 and 12 for the eortc questionnaires and months 9 , 12 , 18 , and 24 , then annually for eq - 5d - 3l . neuropathy assessments with fact / gog - ntx4 were initially completed up to 12 months , as were the eortc questionnaires in patients who underwent randomisation before feb 16 , 2011 , from sites that opted to participate in this substudy . 
an amendment introduced in version 3.0 of the protocol on march 20 , 2012 , extended the requirement for the neuropathy questionnaire to be completed for patients who completed it at baseline to the follow - up visits at months 18 and 24 . 
a further amendment ( version 4.0 on dec 20 , 2012 ) extended the requirement for the neuropathy questionnaire to be completed to every follow - up visit ( to a maximum of 8 years ) for all new patients and existing patients already participating in the substudy . 
these amendments were made as a result of recommendations by the independent data monitoring committee . outcomes the primary study endpoint was disease - free survival , defined as the time from randomisation ( or trial registration for those randomised after 3 months of therapy ) to relapse , development of a new colorectal cancer , or death from any cause . 
assuming that the study would recruit over a period of 5 years with a subsequent minimum follow - up of 2 years , this design required 8600 patients to undergo randomisation and 2750 events ( relapses , deaths , or new colorectal cancers ) to be observed . 
to allow for losses to follow - up , our target recruitment was 9500 patients . from the outset , we recognised that reliable conclusions based on safety and qol data would not require information on all 9500 patients . 
for safety outcomes , the plan was that 700 patients ( 350 in each group ) would be sufficient to detect ( with 80% power and two - sided significance level of 5% ) a halving in the proportion of patients with grade 3 or 4 toxic effects from 12% to 6% ( 12% being the rate at which grade 3 or 4 paraesthesia the most frequent non - haematological grade 3 or 4 toxic effectoccurred in the oxaliplatin group in the mosaic trial ) .3 this same sample size would allow small changes in global qol to be detected ( assuming a difference of magnitude of 75313 and a standard deviation of 234 ) 14 with 95% power at the 1% significance level . 
this more stringent level of significance was used to allow for multiple testing across the various qol scales . we collected information on these toxicity and qol endpoints from all patients recruited until the number required was exceeded and the decision to stop was endorsed by the independent data monitoring committee and trial steering committee . 
the data monitoring committee had access to summary plots of eortc qol data , eq - 5d health status , and fact / gog - ntx4 neuropathy data by study group and study timepoints and following a committee meeting on may 28 , 2010 ( based on 1047 randomised patients ) , recommended that the collection of qol and fact / gog - ntx4 data be continued because they were concerned that the amount of missing data might undermine the comparisons at later timepoints if the original sample size estimates were used . 
they also recommended that the collection of fact / gog - ntx4 data should be extended beyond 12 months for new patients and , where possible , for patients already on the study . 
at their next meeting on the data monitoring committee nov 23 , 2010 , recommended the collection of qol and fact / gog - ntx4 data should stop once 1800 patients had been recruited . 
delays in the amendment of the protocol to implement the collection of the fact / gogntx4 beyond 12 months led to patient recruitment beyond this recommendation to ensure sufficient numbers of patients at these later timepoints . 
these extensions to data collection were made to compensate for missing data and no formal power calculations were made for these changes . that the efficacy analyses of disease - free survival and overall survival included all randomly assigned patients far as possible . 
 ( intention - to - treat population ) as vol 19 april 2018 articles kaplan - meier techniques were used to plot both disease - free survival and overall survival . 
the analysis of treatment delivery and safety was based on patients who started study treatment . the comparison of disease - free survival and overall survival between the treatment groups was based on a cox regression model incorporating the minimisation factors as covariates . 
the p value for testing the null hypothesis that the hr of 3 months versus 6 months was greater than or equal to 113 was derived from this model by comparing the log - likelihood of the fitted model with the log - likelihood of a model where the hr between the groups is set to 113 by use of a likelihood ratio test . 
the proportional hazards assumption implicit in these analyses was examined graphically via a log - minus log plot of the survival function against log time and via a test of the interaction between the treatment group and time ( logged ) obtained from a cox model time - varying covariate . incorporating an appropriate the components of the forest plot ( estimated hr for the comparison between groups and associated 95% ci ) were derived from a cox model that included separate terms for the effect of duration within each category of the relevant stratification factor or other factor being examined . 
patients could have more than one reason . 566 vol 19 april 2018 articles the impact of treatment duration varied across important patient subgroups . multiple imputation analysis15 was used to fill in the missing data and questionnaires in the qol and neuropathy scales . 
 the standardised adjusted auc was calculated for the five imputed datasets and compared between the randomised treatment groups via a generalised linear model ( with study group as an independent factor and study minimisation factors as covariates )  . 
the test statistics associated with study group from each of the five imputations were finally combined to provide an overall p value that takes into account the extent of the missing data . 
to allow for the number of scales being examined , an adjustment for multiple comparisons ( separately for the eortc and eq - 5d questionnaires ) was made with the sharpened hochberg procedure.17 the p value threshold for statistical significance was 5% after adjustment . 
comparisons of these scales at individual timepoints also made use of multiple imputation and generalised linear models . the mann - whitney u test was used for the comparison of ordered categorical variables for toxicity grade . 
 fishers exact test was used to compare the incidence of grade 35 toxic effects and the odds ratio and associated confidence interval for the incidence of grade 35 toxicity was estimated using logistic regression . about issues the study data were reviewed by the data monitoring committee approximately once per year to assess safety and efficacy from an ethical viewpoint . 
 the conditional power for disease - free survival was presented at the fifth ( june 26 , 2012 ) , sixth ( jan 7 , 2013 ) , and seventh ( oct 2 , 2013 ) meetings of the data monitoring committee . 
the data monitoring committee also had access to interim disease - free survival results from an italian study tosca ( nct00646607 ) , which was addressing the same question and had more mature data at the time . 
 table 1 : baseline patient characteristics recorded at randomisation by study group role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the study did not meet its recruitment target of 9500 patients because accrual was not as rapid as originally forecast and recruitment needed to stop to allow sufficiently complete follow - up on current patients within the available funding . 
 by increasing the recruitment period by 6 months and extending minimum follow - up to 3 years ( 88% patients were followed up for 3 year disease - free survival by the reverse kaplan - meier method , allowing for a 2 month deviation from the assessment time ) , 1482 disease - free survival events were observed , giving the study 66% power rather than the originally planned 90% power for rejecting the null hypothesis . 
results from previous adjuvant studies have shown that most disease - free survival events occur within the first 3 years of starting treatment.3 , 19 the analysis time was prespecified in the protocol and therefore no bias would be introduced as might be the case if we had allowed the timing of the analysis to be guided by the data at hand . the data cutoff for this analysis was dec 1 , 2016 . 
787 patients had died at the time of analysis . 568 vol 19 april 2018 articles the baseline demographics , stage , and site of disease for each group were balanced across the trial population ( table 1 )  . 
the largest difference between the overall population and the subgroups assessed for safety and qol was a 9% increase in the incidence of patients with performance status 1 in the ctcae safety cohort ; all other differences in individual characteristics were within 5% . at the time of the disease - free survival analysis there had been 740 events in the 3 month group and 742 events in the 6 month group . 
3 year disease - free survival was 767% ( 95% ci 751782 ) in the 3 month group and 771% ( 756786 ) in the 6 month group , giving an hr of 1006 ( 09091114 , p = 0012 ) which met the criteria for non - inferiority ( figure 2 )  . 3 year overall survival is shown in figure 2 . 
the appendix contains a breakdown of causes of death ( p 10 ) and further details of deaths related to protocol treatment ( p 11 )  . in a prespecified sensitivity analysis , we also examined the difference between the study groups according to the actual duration of treatment on the two randomised groups ( appendix p 1 )  . 
for eligible patients who received the actual assigned study duration of 3 and 6 months , the observed hr was 1158 ( 95% ci 10181317 , p = 0641 )  . forest plots by stratification factors and randomisation timepoint are shown in figure 3 . 
the most marked heterogeneity was for the dependence of the duration effect on the initial choice of regimen ( p = 0069 ) , so we did a post - hoc analysis of disease - free survival for the two durations of therapy for capox and folfox regimens ( figure 4 )  . 
 among patients with available chemotherapy duration data , 2521 ( 83% ) of 3024 of patients assigned to 3 months of treatment actually received 3 months of treatment , including 845 ( 86% ) of 980 receiving folfox and 1676 ( 82% ) of the 2044 receiving capox . 
1773 ( 59% ) of 3013 patients assigned to receive 6 months of treatment actually received 6 months of treatment , which was similar for those receiving folfox ( 585 [ 59% ] of 985 ) and capox ( 1188 [ 59% ] of 2028 )  . 
 * these estimates differ slightly because the underlying multivariable cox model on which they are based includes parameters for other minimisation variables , as well as those factors relating to stage ; the increased flexibility in the expanded stage model allows the influence of these parameters on the high risk stage ii estimates to modify . 
 see online for appendix receive 3 months ( 425 [ 14% ] of 3024 ) and 6 months ( 417 [ 14% ] of 3013 ) of treatment . 244 patients in the 3 month group and 576 patients in the 6 month group cited adverse events as the reason for stopping treatment early . 
in the 6 month group , both diarrhoea ( 150 patients ) and peripheral neuropathy ( 156 patients ) were commonly cited as reasons for stopping . figure 5 shows the dose delivery for fluoropyrimidine and oxaliplat the median percentage of full fluoropyrimidine dose delivered was 953% ( iqr 831998 ) in the 3 month group and 832% ( 567957 ) in the 6 month group . 
the number of patients who had recorded fluorouracil or prescribed capecitabine dose reductions in the 3 month group were 788 ( 26% ) of 3009 compared with 1286 ( 43% ) of 3013 in the 6 month group . 
for oxaliplatin , the corresponding figures were 906 ( 30% ) of 3009 and 1869 ( 62% ) of 3013 . given previous trial data , 20 it is known that there is a marked difference in risk of relapse between patients with n1 colorectal cancer compared with those with n2 pathology , so we did a post - hoc analysis comparing t13 , n1 colorectal cancer against t4 and n2 pathology ( figure 6 ) , and analysed these different prognostic groups according to the chemotherapy regimen they received ( folfox or capox ; appendix p 5 )  . 
for those patients with t1 - 3 / n1 disease the test for non - inferiority in this post - hoc analysis was statistically significant ( p = 0012 )  . safety was assessed by the investigators in 868 patients , 434 ( 50% ) in each group . 
sensory neuropathy , diarrhoea , neutropenia , fatigue , pain , nausea , and hand - foot syndrome were the most common grade 35 adverse events ( table 2 )  . 
the frequency of grade 35 diarrhoea ( p = 0033 ) , neutropenia ( p = 0014 ) , hand - foot syndrome ( p = 0031 ) , and sensory neuropathy ( p < 00001 ) was significantly higher in the 6 month group than in the 3 month group . 
the only side - effect for which the percentage of patients with adverse events ( p = 0031 ) , pain 570 vol 19 april 2018 articles during months 9 and 12 after patients in the 6 month group had stopped treatment . 
overall , grade 35 adverse events were reported by 150 ( 36% ) of 420 patients in the 3 month group and 243 ( 59% ) of 409 patients in the 6 month group ( p < 00001 )  . 
we compared the results from the fact / gog - ntx4 questionnaire for patients receiving 3 months of chemotherapy with those receiving 6 months of chemotherapy ( figure 7 )  . 
the neuropathy standardised adjusted auc differed significantly between the two study groups ( p < 00001 ) , with clear differences appearing at month 4 and persisting until at least 5 years ( p < 00001 )  . 
the maximum difference in means was generally seen at 6 months and , in accordance with the categories of osoba and colleagues , 13 these mean differences in functional and global health status scales represented moderate changes ( values between 1020 ) for global health status , role functioning , and social function and a ( values between 510 ) for physical little change functioning , and cognitive functioning , emotional functioning . 
thereafter , the mean values converged 3 months of treatment 6 months of treatment study group figure 5 : treatment delivery by selected adjuvant regimen box and whisker plots indicate median and iqr ( boxes ) and range ( whiskers )  . 
the standardised adjusted aucs differed significantly for both the eq - 5d self - rated visual analogue scale ( p = 000081 ) and the eq - 5d - 3l health index ( p = 000081 ; appendix p 15 )  . 
 plotting the eq - 5d scales showed that the differences between the two groups of the study were restricted to months 4 , 5 , and 6 , the period when patients in the 6 month group were still receiving treatment and those in the 3 month group had stopped . 
the maximum difference in means was at 6 months and these differences were consistent with clinically important differences ( appendix p 15 ) .21 this pattern was also noticeable for the eq - 5d selfrated visual analogue scale ; patients in the 6 month group had significantly lower qol than those in the 3 month group during months 4 , 5 , and 6 , but after this point , there were no overall clinically important differences up to the 6 year follow - up ( appendix p 3 )  . to investigate the potential effects of missing data on the results from the fact / gog - ntx4 , eortc , and eq - 5d assessments , the reasons for missing questionnaires were recorded ( appendix p 16 )  . 
similarly , an analysis of missingness according to baseline factors indicated that the patients who completed the questionnaires were representative of the patients who participated in this aspect of the study , with any associations between a questionnaire being missing and 572 vol 19 april 2018 articles l vol 19 april 2018 articles 6 months 3 months baseline 1 month 2 month 3 month 4 month 5 month 6 month 9 month 1 year 18 months 2 years 3 years 4 years 5 years 6 years assessment timepoint baseline month 1 month 2 month 3 month 4 month 5 month 6 month 9 year 1 month 18 * year 2 * year 3 * year 4 year 5 year 6 3 months treatment questionnaires completed questionnaires expected proportion of expected questionnaires received 859 1445 59% 6 months treatment questionnaires completed questionnaires expected proportion of expected questionnaires received 865 1426 61% 817 1433 57% 782 1426 55% 527 1421 37% 639 1416 45% 639 1416 45% 606 1400 43% 733 1386 53% 721 1266 53% 172 1312 13% 169 1202 14% 22% 796 1406 57% 782 1395 56% 701 1389 50% 679 1384 49% 679 1382 45% 268 1375 19% 665 1366 49% 721 1346 54% 182 1308 13% 174 1195 15% 22% 48% 42% 62% 54% figure 7 : peripheral neuropathy by study group patients reported peripheral neuropathy with the gog ntx4 questionnaire . 
 * the low completion rates at these timepoints reflect the fact that , initially , neurotoxicity data were only collected up to 12 months and there was a delay before an amendment extended the collection to the whole study period . 
low return rate because patients were assessed at the start of last cycle rather than 6 months ( which corresponds to end of cycle )  . baseline characteristics being small ( appendix p 17 )  . 
 finally , we did a sensitivity analysis to compare the primary imputed results with the results based on observed data only or the imputed results for patients who completed baseline questionnaires only . 
the results of these analyses were all very similar to the findings of the main study ( appendix p 18 )  . we did an exploratory analysis to examine the differences in qol scales between patients whose worst responses to the questions on the gogntx4 questionnaire about whether they had numbness , tingling , or discomfort in their hands or feet were quite a bit or very much and those whose worst responses were somewhat , a little bit , or not at all ( appendix p 4 )  . 
this analysis identified statistically and clinically significant poorer qol between these patient groups at 1 year , 3 years , and 5 years , apart from eq - 5d visual analogue scale at 1 year , for which the difference was not clinically significant . 
the proportion of patients recording neuropathy symptoms as being present quite a bit or very much was significantly higher in the 6 month group than in the 3 month group at each timepoint ( 248 [ 34% ] of 721 vs 99 [ 14% ] of 721 , p < 00001 at 1 year ; 63 [ 32% ] of 199 vs 30 [ 15% ] of 198 , p < 00001 at 3 years ; 49 [ 29% ] of 170 vs 30 [ 16% ] of 193 , p = 00032 at 5 years )  . discussion our results show the non - inferiority of 3 months of adjuvant oxaliplatin - containing chemotherapy treatment compared with 6 months of treatment for patients with high - risk stage ii and stage iii cancer of the colon and rectu the shorter treatment duration was also associated with reduced toxicity and less deterioration in qol . 
because this study recruited 6088 patients with conventionally defined high - risk stage ii and stage iii colorectal cancer from a large number of centres and countries and made use of standard chemotherapy regimens , the study findings are applicable to a typical patient with colorectal cancer needing adjuvant chemotherapy treatment . 
the non - inferiority boundary was set to exclude a maximum 25% fall in 3 year disease - free survival in patients in the 3 month group compared with those in the 6 month group , whichas estimated on the basis of results from previous trials would yield a predicted 3 year disease - free survival of 78% . 
this threshold of 25% was chosen because it was half the difference seen in 3 year disease - free survival between patients in the oxaliplatin - containing group and those in the fluoropyrimidine only group in the mosaic study . 
it was felt by clinicians commonly treating 574 vol 19 april 2018 articles colorectal cancer that this small difference would be an acceptable payoff to bring about a significant reduction in long - term neuropathy and potential improvement in qol to patients who achieve a long - term cure . 
this difference corresponds to an hr of 113 , which we aimed to detect with 90% power at the 25% one - sided level of statistical significance . initial ( rather than our because 6088 patients were recruited and 1482 events were recorded target of 9500 patients with 2750 events ) , the power was reduced to 66% . 
however , we were still able to show the noninferiority of 3 months of treatment compared with 6 months of treatment ( p = 0012 ) across the trial population as a whole ( stage iii and high risk stage ii disease ; colon and rectal cancer ) , with 3 year disease - free survival of 771% ( 95% ci 756 to 786 ) for patients in the 6 month group and 767% ( 751 to 782 ) for those in the 3 month group ( hr 1006 , 0909 to 1114 )  . 
patients in the 6 month group had similar 3 year disease - free survival to that seen with 6 months of oxaliplatin - containing adjuvant chemotherapy in the mosaic study ( 782% ) and nsabp c07 studies ( 761% ) , suggesting that the outcome observed in our control group was similar to that previously seen.3 , 4 however , it is important to note that in the scot trial , only 1096 ( 18% ) of 6088 patients had highrisk stage ii disease , whereas in mosaic and nsabp - c07 , 40% and 30% of patients had all - risk stage ii disease . 
at the time scot was initiated , less data were available on adjuvant chemotherapy for rectal cancer because many adjuvant studies have excluded these patients , and patients with rectal cancer were eligible to participate if they had received no preoperative chemotherapy ( short - course radiotherapy alone was allowed ) and had undergone total mesorectal excision with an r0 resection . 
the only adjuvant chemotherapy these patients received was within this study and randomised for the duration of treatment . we did comparisons of disease - free survival based on the actual duration of treatment received in the study groups , as well as the primary intention - to - treat analyses . 
 these subanalyses did not show non - inferiority , but are inherently biased by the differential exclusion of patients not able to receive prolonged therapy because of the different target treatment durations in the study groups . 
 in a setting such as this where differential compliance is intrinsic to the treatments being compared , our view is that the intention - to - treat analysis is a more accurate reflection of the impact of the intervention on actual clinical practice . in terms of our analyses of smaller subgroups , we have not been able to draw solid conclusions about the effect of treatment duration on specific patient populations such as those with high - risk stage ii disease or patients with rectal cancer because the numbers in these subgroups were relatively small and few events occurred . 
however , the forest plots did not show any differences in the effect of the duration of adjuvant chemotherapy between patients with high - risk stage 2 disease and those with stage iii disease and between those with rectal cancer and those with colon cancer . 
in clinical practice in many parts of the world , a substantial proportion of patients with high - risk stage ii disease or stage iii disease ( especially if older than 70 years of age ) receive only single - agent fluoropyrimidine for 6 months because the addition of oxaliplatin to fluoropyrimidine has not been shown to improve survival in these patients.22 other factors to consider in terms of prognosis and prediction of response to treatment include the sidedness of the cancer ( right vs left ) , ras and braf status , which affect prognosis in metastatic disease , and microsatellite instability status , which affects the outcome of adjuvant treatment.23 these questions cannot yet be answered by the results of scot , but there is a translational research substudythe transscot study , which is ongoing that will look at these factors . it is more difficult to give 6 months of treatment than 3 months of treatment . 
in the scot study , 2521 ( 83% ) of 3024 patients assigned to 3 months received 3 months of treatment , whereas only 1773 ( 59% ) of 3013 patients assigned to 6 months received 6 months of treatment . 
however , the median percentage of the full expected dose of fluoropyrimidine received varied between 94% and 98% for the 3 month group and 82% and 85% for the 6 month group , depending on regimen choice . 
given that the median fluoropyrimidine and oxaliplatin doses received were similar between the two regimens ( figure 5 ) , compliance to treatment is unlikely to explain the difference seen between the two regimens . our results showed that 6 months of adjuvant chemotherapy was significantly more toxic than 3 months of treatment . 
this difference was most marked for peripheral neuropathy , with 237 ( 58% ) of 409 patients in the 6 month group reporting grade 2 or worse neuropathy compared with 103 ( 25% ) of 420 patients in the 3 month group . 
peripheral neuropathy , as reported via a patient questionnaire , was significantly worse in the 6 month group and persisted for at least 5 years ( figure 7 )  . 
however , the vol 19 april 2018 articles effects are large , as are the significance levels , and there is no evidence that these comparisons are biased between the groups , qol , as measured by qlq - c30 global health status and eq - 5d - 3l , declined while patients were receiving chemotherapy . 
 in peripheral neuropathy , with more patients in the 6 month group reporting quite a bit or very much numbness , tingling , or discomfort in their hands or feet in the fact / gog - ntx4 questionnaire , which correlated with significantly worse qol at 1 year , 3 years , and 5 years . 
when we looked at the effect of duration for each regimen separately , capox showed non - inferiority in terms of disease - free survival for 3 months versus 6 months of treatment , but this was not the case for patients receiving folfox . 
the choice of chemotherapy regimen was not randomised but instead chosen by the physician and patient and the reasons why specific regimens were chosen for individual patients are not known . also important to note for capecitabine , an oral drug that is self - administered at home , is that we only know that we might overestimate the prescribed dose and do not have detailed compliance the data , meaning fluoropyrimidine dose intensity for patients receiving capox . 
however , in our experience , except in instances where clinicians curtail or modify doses according to intracycle toxicity , compliance with oral chemotherapy drugs is high . since the difference in the impact of treatment duration between the capox and folfox regimens does not seem to be easily explained by compliance with treatment or differences in the overall percentage of standard drug doses that were delivered , we perhaps need to consider other potential reasons for this finding . 
in the capox regimen , the dose of oxaliplatin given with each cycle is higher than that given in folfox , and therefore we presume that higher peak doses of oxaliplatin are achieved . 
additionally , although the peak dose of fluoropyrimidine will be lower with capox ( capecitabine is given twice daily orally for two out of three weeks ) than with folfox ( where the fluoropyrimidine is given as a bolus , then infused over 2 days every 2 weeks ) , the duration and continuity of exposure is greater . 
could the micrometastatic disease be rendered more sensitive by one or both of these differences ? if each of the cells in this micrometastatic setting are cycling through s phase only sporadically , does the continuity of exposure of the fluoropyrimidine in the form of capecitabine mean that there is a greater overall chance that these cells will be exposed to fluoropyrimidine at the critical part of the cell cycle , compared with fluorouracil given as bolus , then over 2 days every 2 weeks . 
this notion is supported by data from two previous adjuvant studies.10 , 28 in terms of oxaliplatin , a drug that is nearly always given over 24 h , does the peak concentration have more of an effect than the frequency , giving an advantage to the capox regimen and less attrition to efficacy when the overall duration of therapy is shortened ? additionally , a higher dose of oxaliplatin is given in the first 4 weeks of treatment with capox ( 260 mg / m ) than with folfox ( 170 mg / m )  . 
it is very difficult to prove these speculative theories without developing appropriate adjuvant models of malignancy , but the results seen will certainly be a focus of strong debate over the coming months and years . stage iii colorectal cancer is a heterogeneous disease and data from the idea collaboration and from multiple adjuvant trials have shown that patients with t13 , n1 pathology have much better outcomes than those with either t4 or n2 features.27 this has led to the evolution of the concept of a high - risk stage iii patient population , with either t4 or n2 disease , as opposed to the lower risk stage iii population ( t13 , n1 ) ; we might need to consider whether patients with high - risk stage iii disease need to be treated in a slightly different way to those with lower risk stage iii disease . similarly , our results have shown that patients with t13 , n1 disease have a much better 3 year disease - free survival than those with either t4 or n2 pathology . 
 576 vol 19 april 2018 articles we found that , in patients with t13 , n1 colorectal cancer , 3 months of treatment was non - inferior to 6 months ( hr 0908 , 95% ci 0751098 )  . 
the hr for disease - free survival is greater than 1 for the 3 months duration compared to 6 months , suggesting that there could be some small loss of efficacy , but the confidence intervals are wide , making this difference difficult to interpret with certainty . 
notably , the observed absolute deficit in 3 year disease - free survival between the 3 months and 6 months of treatment for the high - risk group ( t4 or n2 disease ) is 18% , which has to be balanced against the increased toxicity seen with 6 months of treatment . 
this is particularly important because the worsened peripheral neuropathy persists for at least 5 years after treatment and results in worse qol outcomes . for patients with t4 or n2 pathology , the absolute increase in 3 year disease - free survival with 6 months versus 3 months of treatment was 27% ( 95% ci 41 to 96 ) for folfox and 13% ( 95% ci 37 to 62 ) for capox ( appendix p 5 )  . 
in view of the difference in toxicity seen with longer treatment , many patients will accept a small reduction in disease - free survival in exchange for reduced toxicity and this is especially true if they are able to receive capox . 
there is less evidence to support a shorter duration of adjuvant treatment if it is decided that the patient needs to receive folfox or has t4 disease . across the whole trial population , scot met the criteria for non - inferiority with a difference in 3 year disease - free survival of 04% ( 95% ci 26 to 18 ) between 3 months and 6 months of treatment . 
while the study was underpowered , the 95% ci for the hr lies below the noninferiority boundary and the results are consistent with those of other individual studies by the idea group , taking into account how the duration effect depended on regimen and risk group . 
the concept that underpowered studies are more likely to produce false - positives ( ignoring the factor of publication bias , which does not apply to a large scale enterprise such as scot ) is disputed.29 as noted , the results differed with the ( non - randomised ) choice of chemotherapy regimens and we can recom mend a 3 month duration of adjuvant chemotherapy for patients with t13 , n1 disease ( 2677 [ 44% ] of the 6088 patients in the scot study ) if the patient is felt to be suitable for the capox regimen . 
we have not been able to show with any statistical certainty that 3 months of treatment was non - inferior to 6 months for patients receiving folfox , for whom there was an absolute increase in 3 year diseasefree survival with 6 months versus 3 months of treatment of 29% ( 95% ci 67 to 08 )  . despite the studys size , there are limitations to the reliability of conclusions that can be drawn for some subgroups . 
high - risk stage iii disease includes either t4 or n2 disease ( or both ) and this study has not been able to the effect of duration of adjuvant show whether chemotherapy is the same for t4 and n2 disease . 
the final decision on treatment duration and regimen used for each individual will depend on a careful discussion between the clinician and patient , taking into account the risk of recurrence , the likely absolute difference in diseasefree survival and risk of long - term toxicity , and the strength of evidence for that particular setting available both from scot and the wider idea analysis . scot is , to our knowledge , the largest single randomised study on the adjuvant treatment of colorectal cancer to date . 
 the study achieved its primary endpoint of showing that 3 months of oxaliplatin - containing adjuvant chemotherapy is non - inferior to 6 months of the same treatment in the overall trial population . 
tji , rsk , mps , ahar , ka , jm , cs , kab , ab , and jp wrote the manuscript and all authors contributed to the review of the manuscript . declaration of interests tji reports receiving honoraria from eli lilly ; serving on advisory boards for servier , roche , and celgene and receiving travel expenses from bayer and servier . 
jt reports support for being on advisory boards from amgen , bayer , boehringer ingelheim , celgene , chugai , lilly , msd , merck serono , novartis , pfizer , roche , sanofi , symphogen , taiho , and takeda . 
awa reports belonging to an institution involved in research that is funded by drug companies that provide the drugs for this study ; and has been coinvestigator in trials funded by roche which provided the capecitabine used in this study . 
all other authors declare no competing interests . acknowledgments this research was supported by the medical research council ( transferred to netsccefficacy and mechanism evaluation ; grant reference g0601705 ) , swedish cancer society , and cancer research uk vol 19 april 2018 articles core clinical trials unit funding ( funding ref : c6716 / a9894 )  . 
we also thank all international collaborative groups who led the trial in their countries ( the danish colorectal oncology group , vhio , agitg , and swedish society of gastrointestinal oncology ) , the independent trial data monitoring committee members ( hilary calvert [ chair ] , allan hackshaw , robin kennedy , and kees punt ) , and the trial steering committee members ( stan kaye , janet dunn , and alberto sobrero )  . articles hypofractionated radiotherapy versus conventionally fractionated radiotherapy for patients with intermediate - risk localised prostate cancer : 2 - year patient - reported outcomes of the randomised , non - inferiority , phase 3 chhip trial anna wilkins , helen mossop , isabel syndikus , vincent khoo , david bloom eld , chris parker , john logue , christopher scrase , helen patterson , alison birtle , john sta urth , zafar malik , miguel panades , chinnamani eswar , john graham , martin russell , peter kirkbride , joe m osullivan , annie gao , clare cruickshank , clare gri n , david dearnaley * , emma hall * summary background patient - reported outcomes ( pros ) might detect more toxic e ects of radiotherapy than do clinicianreported outcomes . 
we did a quality of life ( qol ) substudy to assess pros up to 24 months after conventionally fractionated or hypofractionated radiotherapy in the conventional or hypofractionated high dose intensity modulated radiotherapy in prostate cancer ( chhip ) trial . methods the chhip trial is a randomised , non - inferiority phase 3 trial done in 71 centres , of which 57 uk hospitals took part in the qol substudy . 
men with localised prostate cancer who were undergoing radiotherapy were eligible for trial entry if they had histologically con rmed t1bt3an0m0 prostate cancer , an estimated risk of seminal vesicle involvement less than 30% , prostate - speci c antigen concentration less than 30 ng / ml , and a who performance status of 0 or 1 . 
participants were randomly assigned ( 1 : 1 : 1 ) to receive a standard fractionation schedule of 74 gy in 37 fractions or one of two hypofractionated schedules : 60 gy in 20 fractions or 57 gy in 19 fractions . 
ucla prostate cancer index ( ucla - pci ) , including short form ( sf ) - 36 and functional assessment of cancer therapy - prostate ( fact - p ) , or expanded prostate cancer index composite ( epic ) and sf - 12 quality - of - life questionnaires were completed at baseline , pre - radiotherapy , 10 weeks post - radiotherapy , and 6 , 12 , 18 , and 24 months post - radiotherapy . 
the chhip trial is registered with isrctn registry , number isrctn97182923 . findings 2100 participants in the chhip trial consented to be included in the qol substudy : 696 assigned to the 74 gy schedule , 698 assigned to the 60 gy schedule , and 706 assigned to the 57 gy schedule . 
median follow - up was 500 months ( iqr 384642 ) on april 9 , 2014 , which was the most recent follow - up measurement of all data collected before the qol data were analysed in september , 2014 . 
 we saw no di erences between treatment groups in change of bowel bother score from baseline or pre - radiotherapy to 24 months . interpretation the incidence of patient - reported bowel symptoms was low and similar between patients in the 74 gy control group and the hypofractionated groups up to 24 months after radiotherapy . 
these studies have not usually included health - related quality of life or patient - reported outcomes ( pros ) , which detect more side - e ects than do clinician - reported outcomes . 
we searched pubmed using the terms patient - reported outcomes or quality of life and hypofractionated or hypofractionation and prostate up to oct 1 , 2002 , and retrieved eight articles . 
of these articles , none reported pros from randomised trials of conventional versus hypofractionated radiotherapy . added value of this study to our knowledge , this study is the largest randomised trial of moderately hypofractionated versus conventionally fractionated radiotherapy using modern radiotherapy techniques , and the rst to report pros up to 2 years after treatment , showing both early and late developing side - e ects . 
 other randomised trials that have included pros and have been reported since this study began used older radiotherapy techniques , or only included follow - up to 3 months after radiotherapy , therefore assessing early rather than late treatment e ects , which are usually dose - limiting . implications of all the available evidence if e cacy outcomes from chhip show non - inferiority for hypofractionated treatments , the absence of any di erence in pros between trial groups adds to the growing evidence for moderately hypofractionated radiotherapy schedules becoming the standard treatment for localised prostate cancer . 
 introduction prostate cancer is the most common cancer in men in the uk , with 41 700 patients diagnosed in 2011.1 for patients diagnosed with localised disease , external beam radiotherapy , radical prostatectomy , and brachytherapy are conventional treatments with similar control rates for organ - con ned tumours . 
patient - reported outcomes ( pros ) detect treatment side - e ects more reliably than do clinician - reported measures and might better guide treatment decisions.2 , 3 the conventional or hypofractionated high dose intensity modulated radiotherapy in prostate cancer ( chhip ) trial ( cruk / 06 / 016 ) randomly assigned men with localised prostate cancer who were undergoing radiotherapy to a standard fractionation schedule or to one of two hypofractionated regimens . 
quality of life ( qol ) was assessed in a substudy within the main trial , in which we aimed to assess whether pros di ered between patients receiving conventionally fractionated versus hypofractionated radiotherapy up to 24 months after radiotherapy . methods study design and participants chhip was a randomised , non - inferiority phase 3 trial done in three seamless stages . 
 initially , men with a prostate - speci c antigen ( psa ) concentration of less than 40 ng / ml and risk of lymph node involvement less than 30% were eligible ; on aug 1 , 2006 , these criteria were revised and a psa concentration less than 30 ng / ml and a risk of seminal vesicle involvement less than 30% were needed . 
full details of trial design , eligibility , and treatment have been reported previously.4 the study was approved by the london multi - centre research ethics committee ( 04 / mre02 / 10 )  . 
the institute of cancer research clinical trials and statistics unit ( icr - ctsu ; sutton , uk ) coordinated the study and carried out central statistical data monitoring and all analyses . 
neither treatment allocation nor ( control ) or one of 1606 vol 16 december 2015 articles clinical assessment were masked because sham radiotherapy was not given . androgen suppression short - course procedures men with nccn intermediate - risk or high - risk disease for received 36 months before and during radiotherapy ; this was optional for patients with low - risk disease . 
individuals assigned the control group received standard radiotherapy with 2 gy daily fractions ( monday to friday treatment ) for 74 weeks , to give a total dose of 74 gy in 37 fractions . 
individuals in the experimental groups received hypofractionated treatment with 3 gy daily fractions to a total dose of either 60 gy in 20 fractions in 40 weeks or 57 gy in 19 fractions in 38 weeks . 
for the hypofractionated schedules , the protocol stated that the overall duration of treatment should be at least 28 days for the 20 - fraction schedule and at least 27 days for the 19 - fraction schedule . 
further details of treatment and quality assurance have been reported previously.4 men consenting to participate in the qol substudy were eligible to complete questionnaires at trial entry if they had not already started endocrine treatment , to minimise the e ect of toxicity of hormone deprivation on qol at this timepoint . 
all men were eligible to complete further questionnaires pre - radiotherapy , and at 10 weeks and 6 , 12 , 18 , and 24 months after the start of radiotherapy . 
 from trial entry to 6 months after radiotherapy , questionnaires were administered in the clinic , and subsequent questionnaires were posted to patients from the icr - ctsu after local veri cation of their current health status . 
all qol questionnaires were selfadministered . in patients during the planning stages of the chhip trial , the university of california , los angeles prostate cancer index ( ucla - pci ) was an important qol instrument available for use in patients with localised prostate cancer.5 subsequently it became apparent that this instrument needed augmentation to better capture the broad range of urinary , bowel , sexual , and hormonal symptoms receiving external beam radiotherapy or brachytherapy , or undergoing radical prostatectomy . 
consequently the expanded prostate cancer index composite ( epic ) qol instrument was developed that had item content that better represented typical symptoms after radiotherapy.6 to maximise the sensitivity of the pros , the qol instruments were updated during the trial to include the epic instrument . 
 therefore from trial initiation to early 2009 , the ucla - pci , including the short form 36 ( sf - 36 ) and functional assessment of cancer therapy - prostate ( fact - p ) qol instruments were used.7 following a protocol amendment on march 12 , 2009 , the epic and short form 12 ( sf - 12 ) qol instruments replaced uclasome old pci , sf - 36 , and fact - p , although questionnaires were received back from participants after this date.8 epic - 50 was used for bowel and urinary domains and epic - 26 for sexual and hormonal domains.9 ucla - pci consists of 20 items organised into six domains , including bowel function ( four items ) , bowel bother ( one item ) , urinary function ( ve items ) , urinary bother ( one item ) , sexual function ( eight items ) , and sexual bother ( one item )  . 
epic - 50 includes a bowel function domain ( seven items ) and a bowel bother domain ( seven items ) , which together form the bowel summary domain , and a urinary function domain ( ve items ) and a urinary bother domain ( seven items ) , which together form a urinary summary doma epic - 26 includes a sexual function domain ( ve items ) and a sexual bother domain ( one item ) , which are combined to form a sexual summary domain ; there is also a hormonal domain ( ve items )  . 
items in the ucla - pci and epic qol instruments di ered : for example , the epic bowel function domain included rectal bleeding , faecal incontinence , and daily bowel movements , which were absent from ucla - pci , the whereas bowel distress was represented ucla - pci bowel function domain and absent from epic - 50 . 
all qol instrument scores range from 0 to 100 and a higher score represents better qol . health - related qol was assessed using the fact - p and sf - 36 instruments ( with ucla - pci ) or the sf - 12 instrument ( with epic )  . 
fact - p consists of physical , social , functional , and emotional wellbeing domains ; each domain has seven items , and scores per domain range from 0 to 28 , except for emotional wellbeing , which ranges from 0 to 24 . 
the sf - 36 instrument includes eight domains of physical functioning , social functioning , vitality , role limitations ( physical ) , role limitations ( emotional ) , mental health , general health , and bodily pain , and each domain score ranges from 0 to 100 . 
sf - 12 consists of a physical composite score ( pcs ) and mental composite score ( mcs ) , each of which have six items , and scores range from 0 to 100 . 
all questionnaires were scored in accordance with scoring manuals.1014 not all the respondents answered all questions ; all available data points were used in analyses . recommended separate qol analyses were planned after 2 and 5 years of follow - up , and this report describes pros up to 2 years . 
 outcomes the primary endpoint was the single item overall how much of a problem have your bowels been for you during the last 4 weeks ( overall bowel bother )  . 
this question vol 16 december 2015 1607 articles was chosen because it gives a good overall measure of bowel - associated morbidity and is common to both the ucla - pci and epic instruments , so was reported by all patients . 
additional secondary endpoints were individual bowel , urinary , and sexual items and domain scores assessed within epic and ucla - pci and the general health - related qol domain scores in fact - p , sf - 36 , and sf - 12 . statistical analysis for all endpoints , the control group was compared with each of the experimental groups , as per the statistical analysis plan of the main trial . 
after this analysis , a post - hoc pragmatic comparison was done between the 60 gy and 57 gy experimental schedules to support clinical management choices if both hypofractionated schedules were shown to be non - inferior to standard fractionation for disease control . 
with 443 patients per experimental group , this substudy would have 80% power and 25% two - sided signi cance to detect changes in the proportion of patients with overall bowel bother scores as follows : from 65% in the standard fractionation group to 60% in an experimental hypofractionation group for scores of 1 ( no bother ) , from 22% to 20% for scores of 2 ( very small bother ) , from 7% to 10% for scores of 3 ( small bother ) , and from 6% to 10% for scores of 4 or 5 ( moderate or severe bother )  . 
power calculations were based on comparisons of two independent groups of ordered categorical data , with constant odds ratios computed across all categories , and assumed complete data would be available for 70% of patients ( 1330 individuals ) at 2 years . 
patients were excluded from the xed timepoint analyses if their qol assessments were dated outside prespeci ed acceptable time intervals : after 1 month of endocrine treatment or after randomisation for baseline ; before 3 months or after 1 week of starting radiotherapy for pre - radiotherapy ; outside 2 weeks from the expected date of completion for 10 weeks ; and outside of 3 months from the expected date of completion for later timepoints . 
qol = quality of life . 1608 vol 16 december 2015 articles were used , guided by a bonferroni adjustment , to make some allowance for multiple testing . we did cross - sectional , time - to - event , and change - frombaseline analyses . 
cross - sectional analysis was done at each timepoint , with formal comparisons between treatment groups at 24 months via the test for trend and the mann - whitney u test . 
we did time - to - event analysis using kaplan - meier methods and the log - rank test to assess time to small or worse , and moderate or worse events for individual items . 
this analysis aimed to detect di erences in late radiation toxic e ects between treatment groups and therefore did not include the 10 - week post - radiotherapy assessment , which assessed acute symptoms . 
patients who reached the relevant endpoint at trial entry or pre - radiotherapy were excluded from that speci c time - to - event analysis . we assessed change from baseline ( post - radiotherapy score minus baseline score ) to account for di erences in pre - existing comorbidity between groups . 
for bowel and urinary items and domain scores , we used the preradiotherapy score as a surrogate baseline score unless it was missing , in which case the baseline score was used . 
 a sensitivity analysis was also done to con rm the robustness of including the baseline assessments of patients receiving less than 1 month of endocrine treatment which involved repeating analyses using baseline assessments of patients receiving no endocrine therapy beforehand . we modelled the odds of any speci c change from baseline or pre - radiotherapy to 24 months using ordinal logistic regression after checking the validity of the proportional odds assumption.15 odds ratios less than one favour the relevant experimental group . 
for the ordinal logistic regression models , the dependent variable is the post - radiotherapy score minus the baseline or preradiotherapy score , taking values of 4 , 3 , 2 , 1 , 0 , 1 , 2 , 3 , or 4 , where negative numbers represent an improvement in qol and positive numbers represent worsening qol . 
patients were excluded from the xed timepoint analyses if their qol assessments were dated outside prespeci ed acceptable time intervals , as outlined in gure 1 . no imputation of missing pro data was done . 
for absent whole instruments , the e ect of these missing data was assessed by comparison of the baseline characteristics of patients present in the analysis versus , rst , those who consented but were missing entirely , and second , those who consented but were missing at 24 months , when formal statistical testing was done . analysis was on an intention - to - treat basis and all analyses were done with stata version 13.1. 
the chhip international standard trial randomised controlled trial , number isrctn97182923 . is registered as an role of the funding source the funders provided peer - reviewed approval for the study concept but had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 table 1 : baseline characteristics and clinical history results between oct 18 , 2002 , and nov 1 , 2009 , 2100 patients were recruited from 57 centres in the uk ( gure 1 and appendix p 14 ) into the qol substudy of the chhip trial ; subsequently , the substudy closed to accrual . 
696 patients were assigned to the standard 74 gy schedule , 698 were assigned to the 60 gy schedule , and 706 were assigned to the 57 gy schedule . median follow - up was 500 months ( iqr 384642 ) on april 9 , 2014 , which was the most recent follow - up measurement of all data collected before the qol data snapshot for this analysis in september , 2014 . 
 questionnaires were returned by 1659 ( 79% ) patients pre - radiotherapy , 1470 ( 70% ) patients at 10 weeks , 1597 ( 76% ) patients at 6 months , 1551 ( 74% ) patients at 12 months , 1456 ( 69% ) patients at 18 months , and 1444 ( 69% ) patients at 24 months . baseline characteristics of patients were balanced between treatment groups except for an imbalance in t stage between the 74 gy and 60 gy groups ( table 1 )  . 
 intermediate nccn risk 1490 ( 71% ) patients had disease.16 for 46 patients reported to have consented to enter the substudy , no qol assessments were received by the icr - ctsu . 
the only signi cant di erence in baseline characteristics between groups with and without 24 - month pro data was that patients with missing questionnaires were more likely to have high nccn risk disease at trial entry than were patients who provided data ( appendix p 2 )  . 
of patients with data from at least one qol assessment , 665 ( 98% ) of 676 in the 74 gy treatment group , 674 ( 98% ) of 686 in the 60 gy treatment group , and 677 ( 98% ) of 692 in the 57 gy treatment group received endocrine therapy . 
cross - sectional analysis at 24 months showed no signi cant di erences in overall bowel bother between the treatment groups ( 74 gy vs 60 gy , ptrend = 064 ; 74 gy vs 57 gy , ptrend = 059 ; appendix p 3 )  . 
 a temporary increase in any bowel bother was seen at 10 weeks ( a change from 413 [ 27% ] of 1509 patients preradiotherapy to 745 [ 57% ] of 1309 patients at 10 weeks )  . 
at 6 months , any bowel bother had decreased ( 581 [ 38% ] of 1519 patients ) , and remained around this level to 24 months , when any overall bowel bother was reported by 441 ( 35% ) of 1258 patients . 
a sensitivity analysis showed that using pre - radiotherapy scores as a surrogate for baseline scores at trial entry for some patients was valid ( appendix p 1112 )  . 
because 252 men completed baseline questionnaires endocrine treatment , a sensitivity analysis was done , which con rmed the robustness of including patients receiving less than 1 month of endocrine treatment at baseline ( appendix p 13 )  . starting after the pattern in overall urinary bother was similar to that for overall bowel bother ( gure 2 , appendix p 4 ) and crosssectional analysis at 24 months showed no signi cant di erences in overall urinary bother between treatment groups ( appendix p 4 )  . 
the baseline incidence of overall sexual bother was higher than that for bowel or urinary bother , with 412 ( 57% ) of 719 patients having any bother at baseline , which increased to 975 ( 68% ) of 1440 patients pre - radiotherapy and improved from 6 months to 24 months ( gure 2 , appendix p 4 )  . 
bowel , urinary , and sexual domain scores assessed within ucla - pci or epic qol instruments also showed no di erence between treatments at 24 months ( table 2 )  . time - to - event analysis of small or worse overall bowel , urinary , and sexual bother showed no signi cant di erences between treatment groups for any endpoints ( gure 2 )  . 
the appendix contains absolute numbers of cumulative small or worse and moderate or worse events , the prevalence of the relevant bowel , urinary , and sexual symptoms before radiotherapy , and the hazard ratios for the time - to - event analysis time from start of radiotherapy to small or worse and moderate or worse events for all individual items in all treatment groups ( appendix pp 5 and 6 )  . 
the number of patients reporting symptoms that were represented only in epic ( faecal incontinence , rectal bleeding , daily bowel movements , dysuria , and haematuria ) was considerably lower than that for other endpoints , so these analyses were underpowered . including incontinence , although we saw no signi cant di erences between treatment groups , the cumulative incidence of some rectal faecal symptoms , bleeding , and use of urinary pads , was higher in patients treated with hypofractionated radiation than in those treated with standard fractionation ( appendix p 5 )  . 
 however , at 24 months , di erences in the prevalence of these symptoms between groups were smaller ( appendix pp 34 )  . figure 3 shows change from baseline for ucla - pci domain scores and epic domain summary scores ; additional epic domain scores are shown in the appendix ( p 10 )  . 
for all urinary and bowel items and domain scores , to maximise numbers , the preradiotherapy score was used as a surrogate baseline score unless missing , in which case the baseline score was used ; exact numbers are : 749 pre - radiotherapy plus 65 baseline for change in ucla - pci bowel function to 24 months ; 146 plus 14 for change in epic bowel summary to 24 months ; 751 plus 64 for change in uclapci urinary function to 24 months ; and 139 plus 16 for change in epic urinary summary to 24 months ( numbers per treatment group shown in appendix p 14 )  . 
 figure 3 also shows change from baseline in scores for the individual items of overall bowel bother , overall urinary bother , and overall sexual bother ; all other endpoints are shown in the appendix ( p 8 )  . 
most patients had no change in score from baseline and we noted no signi cant di erences between treatment groups in change from baseline to 24 months for any individual items . 
compared to the 74 gy control group , the odds of a one - point increase in overall bowel bother were reduced , although not signi cantly , in the 60 gy treatment group ( odds ratio [ or ] 085 [ 99% ci 057126 ] ; p = 029 ) and the 57 gy treatment group ( or 084 [ 057124 ] ; p = 025 )  . 
for some endpoints , the odds of a patient developing sidee ects were slightly increased for the 60 gy group compared with the 57 gy group , but none of these increases were signi cant ( appendix p 8 )  . 
for all urinary and bowel items and domain scores , to maximise numbers , the pre - radiotherapy score was used as a surrogate baseline score unless missing , in which case the baseline score was used . and sf - 36 between treatment groups at 24 months ( appendix p 9 )  . 
however , for domains of vitality , physical role functioning , and social wellbeing , we noted a reduction of more than 10 points between the median domain score at baseline and at 10 weeks after the start of radiotherapy in all treatment groups . 
by 6 months , median scores had increased to within 10 points of the median scores at baseline for all three measures . discussion in this qol substudy of the chhip trial , pros were not signi cantly di erent between treatment groups for any of the endpoints assessed . 
both cross - sectional analysis at 24 months and time - to - event analysis suggest an overall pattern of low incidence of bowel and urinary toxic e ects in all treatment groups . 
these acute toxic e ects had a small and short - lived e ect on general healthrelated qol , especially the sf - 36 domains of vitality , vol 16 december 2015 1613 articles important physical role functioning , and social wellbeing . 
overall , changes from baseline to 24 months for urinary , bowel , and most general health - related qol domains ( except role limitations [ physical ] ) , were less than previously reported minimally from longitudinal anchor - based methods.17 although further development of toxic e ects is possible after 2 years , recent studies have reported minimal change in late radiotherapy side - e ects after 2 years following external beam radiation therapy.18 this suggests that 2 years is an appropriate endpoint for initial pro reporting . di erences derived to our knowledge , this is the rst large randomised trial of hypofractionated radiotherapy that used modern radiotherapy techniques to report pros with follow - up to 24 months . 
radiotherapy doses were higher in hypro ( standard fractionation of 39 fractions of 2 gy in 8 weeks vs hypofractionation with 19 fractions of 34 gy in 65 weeks ) than in chhip . 
a small ( 124 patients ) randomised study of moderate hypofractionation ( 63 gy in 20 fractions ) versus conventional fractionation ( 76 gy in 38 fractions ) reported no di erence in epic scores between treatment groups up to 3 months after radiotherapy.20 the pros in this study are broadly consistent with preliminary data for clinician - reported outcomes in the chhip trial , 4 and the clinician - reported outcomes of a small ( 168 patients ) phase 3 trial in italy.21 results from another randomised trial that included 203 patients showed a non - signi cant numerical increase in clinicianreported toxic e ects with hypofractionation.22 however , the radiotherapy dose schedules used in these studies21 , 22 di er substantially from those in chhip . late gastrointestinal and hypofractionated so far , randomised trials2125 reporting the e ects of hypofractionation versus conventional fractionation have reported inconsistent results for side - e ects and do not clearly show a di erence in the rate of increase of genitourinary or gastrointestinal toxic e ects between conventional radiotherapy treatments.26 these ndings emphasise the need for outcome data from large trials of hypofractionation that use modern radiotherapy techniques . 
such studies to compare hypofractionated radiotherapy with standard fractionation , the clinician - reported outcomes from chhip , will help to con rm whether faecal incontinence , rectal bleeding , or use of urinary pads are more common at a dose of 3 gy per fraction . together with findings from a trial of hypofractionation25 that included 303 patients raised concerns about increased urinary toxic e ects after hypofractionated treatment in patients who had compromised urinary function before enrolment , as assessed by clinician - reported lent and rtog scores . 
a formal comparison restricted to patients with baseline dysfunction has not been done in our study , partly because obstructive and irritative symptoms , and consequently overall urinary dysfunction , are not well represented in the ucla - pci instrument . 
furthermore , overall urinary bother seems to decrease during the 2 years after radiotherapy , which is consistent with ndings from the rt01 dose escalation trial.27 comparison of bowel bother and distress assessed using the ucla - pci instrument in both the 74 gy group of chhip and the 74 gy group of the rt01 trial , 27 in which conventional radiotherapy planning techniques were used , suggests that patients bene t substantially from improved treatment methods that use intensitymodulated radiotherapy and the dose constraints used in chhip . 
in rt01 , 27 ( 9% ) of 289 patients reported moderate bowel bother and nine ( 3% ) patients reported severe bother in the 74 gy group at 24 months.28 this compares with 19 ( 5% ) of 410 patients reporting moderate bother and four ( < 1% ) patients reporting severe bother in the 74 gy group in chhip at 24 months . 
similarly , at 24 months , 34 ( 12% ) of 288 patients in rt0128 versus 13 ( 4% ) of 312 patients in chhip reported moderate bowel distress , and two ( < 1% ) patients in rt0128 versus none in chhip reported severe bowel distress . strengths of our study include the wide age range and large number of patients recruited from di erent parts of the uk . 
the use of di erent qol instruments was a limitation of the analysis , because it meant that fewer patients reported some important radiotherapy - related toxic e ects , including rectal bleeding and faecal incontinence , which were only represented in epic . 
to our knowledge , minimally clinically important di erences have not been published for epic - 50 , but will be a valuable addition when available . patients might acclimatise to symptoms over time and therefore the most subjective endpoints , such as overall bowel , urinary , and sexual bother , might under - represent the actual toxicity at later timepoints . 
however , more objective pros , including rectal bleeding , dysuria , and quality of erections showed similar patterns of toxic e ects over time compared with overall bother items , suggesting reliable representation of patient experience . 
bother items might incorporate a psychosocial component as well as actual that overall bother gives a 1614 vol 16 december 2015 articles functional change , but we believe that overall perception of toxic e ects is a comprehensive and comprehensible endpoint in a randomised comparison of pros . patients with missing data at 24 months were more likely to be in a higher nccn risk group than were those patients with data present . 
both nccn risk group and numbers of patients with missing data did not di er between treatment groups , therefore missing data are unlikely to have substantially biased the randomised comparisons . to complete pros at 5 years will be important to con rm our ndings . 
so far , our results show that the bowel and urinary side - e ects of moderate hypofractionation for prostate cancer delivered with modern radiotherapy techniques are low and similar to those of standard fractionation . contributors aw did statistical analyses , data interpretation and wrote the report . 
dd , eh , is , js , vk , cs , hp , jg , cc , and cg are members of the chhip trial management group responsible for the design and day - to - day oversight of the study and contributed to data interpretation . 
vk reports advisory and educational fees and nonnancial support from astellas , educational fees from bayer , nonnancial educational support from janssen , advisory and educational fees and nonnancial support from ipsen , and educational fees from tolmar . 
 acknowledgments this work was supported by cancer research uk ( cruk / 06 / 16 , c8262 / a7253 , c1491 / a9895 , c1491 / a15955 , sp2312 / 021 ) , the department of health , the national institute for health research cancer research network , and nhs funding to the nihr biomedical research centre at the royal marsden nhs foundation trust and the institute of cancer research , london . 
we would also like to thank the chhip trial management group members , past and present , and the independent data monitoring and trial steering committees for overseeing the trial . 
 helen patterson died in 2012 shortly after completion of recruitment to the trial and remains greatly missed by her colleagues . articles parotid - sparing intensity modulated versus conventional radiotherapy in head and neck cancer ( parsport ) : a phase 3 multicentre randomised controlled trial christopher m nutting , james p morden , kevin j harrington , teresa guerrero urbano , shreerang a bhide , catharine clark , elizabeth a miles , aisha b miah , kate newbold , maryanne tanay , fawzi adab , sarah j je eries , christopher scrase , beng k yap , roger p ahern , mark a sydenham , marie emson , emma hall , on behalf of the parsport trial management group * summary background xerostomia is the most common late side - e ect of radiotherapy to the head and neck . 
we assessed the hypothesis that parotid - sparing imrt reduces the incidence of severe xerostomia . methods we undertook a randomised controlled trial between jan 21 , 2003 , and dec 7 , 2007 , that compared conventional radiotherapy ( control ) with parotid - sparing imrt . 
we randomly assigned patients with histologically con rmed pharyngeal squamous - cell carcinoma ( t14 , n03 , m0 ) at six uk radiotherapy centres between the two radiotherapy techniques ( 1 : 1 ratio )  . 
 this study is registered with the international standard randomised controlled trial register , number isrctn48243537 . findings 47 patients were assigned to each treatment armedian follow - up was 440 months ( iqr 300597 )  . 
at 12 months xerostomia side - e ects were reported in 73 of 82 alive patients ; grade 2 or worse xerostomia at 12 months was signi cantly lower in the imrt group than in the conventional radiotherapy group ( 25 [ 74% ; 95% ci 5687 ] of 34 patients given conventional radiotherapy vs 15 [ 38% ; 2355 ] of 39 given imrt , p = 00027 )  . 
the only recorded acute adverse event of grade 2 or worse that di ered signi cantly between the treatment groups was fatigue , which was more prevalent in the imrt group ( 18 [ 41% ; 99% ci 2361 ] of 44 patients given conventional radiotherapy vs 35 [ 74% ; 5589 ] of 47 given imrt , p = 00015 )  . 
at 24 months , grade 2 or worse xerostomia was signi cantly less common with imrt than with conventional radiotherapy ( 20 [ 83% ; 95% ci 6395 ] of 24 patients given conventional radiotherapy vs nine [ 29% ; 1448 ] of 31 given imrt ; p < 00001 )  . 
at 12 and 24 months , signi cant bene ts were seen in recovery of saliva secretion with imrt compared with conventional radiotherapy , as were clinically signi cant improvements in dry - mouth - speci c and global quality of life scores . 
at 24 months , no signi cant di erences were seen between randomised groups in non - xerostomia late toxicities , locoregional control , or overall survival . interpretation sparing the parotid glands with imrt signi cantly reduces the incidence of xerostomia and leads to recovery of saliva secretion and improvements in associated quality of life , and thus strongly supports a role for imrt in squamous - cell carcinoma of the head and neck . funding cancer research uk ( cruk / 03 / 005 )  . introduction radiotherapy is the main non - surgical treatment for squamous - cell carcinoma of the head and neck ( hnscc ) .1 high rates of local tumour control can be achieved with 5 - year survival greater than 80% for stage 1 and 2 and 6070% for stage 3 and 4 tumours ; 2 however , long - term late sequelae of radiotherapy are highly prevalent and have severe adverse e ects on quality of life ( qol ) .3 , 4 radiation - induced xerostomia is the most commonly reported late side - e ect of radiotherapy to the head and neck . 
lack of saliva a ects speech and swallowing and can accelerate dental caries.5 ( imrt ) radiotherapy intensity - modulated conformal radiotherapy technique that can spare the major salivary glands . 
patients were required to attend regular follow - up , undergo salivary ow measurements , and complete self - assessed qol questionnaires . they were exclusion criteria included previous head or neck radiotherapy ; previous malignancy except non - melanoma skin cancer ; pre - existing salivary gland disease ; tumour involvement of the parotid glands ; or previous or concurrent illness that would compromise completion of treatment or follow - up . 
patients who had received neoadjuvant chemotherapy were eligible . 94 patients recruited 47 randomly assigned to conventional 47 randomly assigned to imrt radiotherapy 6 died before 12 months 6 died before 12 months 41 alive at 12 months 41 alive at 12 months 7 not assessed at 12 months 3 withdrew consent 2 did not attend 1 reason unknown 1 deviated and withdrew ( treated with chemoradiation ) 2 not assessed at 12 months 1 did not attend 1 not done because of disease recurrence at 8 months 34 evaluable for primary endpoint 39 evaluable for primary endpoint at 12 months 33 received treatment as per protocol 1 deviation ( imrt given , unable to cover target volume adequately ) at 12 months 37 received treatment as per protocol 2 deviations ( radiotherapy gap because of rectal bleeding , concomitant chemotherapy ) 29 alive and disease free 12 months after completion of radiotherapy 5 alive with recurrence or progressive disease 29 alive and disease free 24 months after completion of radiotherapy 5 died figure 1 : study pro le imrt = intensity - modulated radiotherapy . 37 alive and disease free 12 months after completion of radiotherapy 2 alive with recurrence 29 alive and disease free 24 months after completion of radiotherapy 7 alive with recurrence or progressive 3 died disease all patients provided written informed consent . 
 the parsport ( cruk / 03 / 005 ) was approved by national south - west multicentre research ethics committee ( mrec 03 / 6 / 79 ) and local ethics committees of all participating centres . 
our trial was sponsored by the royal marsden nhs foundation trust and undertaken in accordance with the principles of good clinical practice . the randomisation and masking patients were randomly assigned in a 1 : 1 ratio to parotidsparing imrt or conventional radiotherapy ( control )  . 
treatment allocation was not masked ; however , the patient was not informed of the treatment until they had completed the baseline qol questionnaires . procedures staging investigations included examination under anaesthetic , tumour biopsy , diagnostic ct or mri of head and neck , chest radiograph , full blood count , and biochemistry . 
in postoperative patients , histology reports that documented the extent of surgical resection were required . the protocol for target volume de nition and treatment planning has been previously described.9 all patients underwent ct - planned radiotherapy with either threedimensional conformal radiotherapy with parallel opposed lateral elds ( conventional radiotherapy ) or parotid - sparing imrt . 
nodal groups at risk of harbouring occult metastatic disease received a biologically equivalent dose of either 50 gy in 25 daily fractions ( conventional radiotherapy ) or 54 gy in 30 fractions ( imrt )  . 
for imrt patients a planning constraint of less than 24 gy to the whole contralateral parotid gland was used.9 , 10 for quality assurance , plans were assessed from all centres for protocol compliance and dosimetric consistency.10 , 11 acute side - e ects were graded weekly with national cancer institute common toxicity criteria ( version 3 ) 12 during radiotherapy and until 8 weeks after treatment . 
salivary ow 128 vol 12 february 2011 articles december , 2007 , both committees approved closure of recruitment after 94 patients had been randomly assigned to the study groups with the expectation that this would provide su cient evaluable patients to allow robust statistical analysis . 
our trial was not powered to reliably assess small di erences in locoregional pfs or overall survival , although these are reported for completeness . our analysis was done on an intention - to - treat basis , with all patients who had a 12 - month xerostomia assessment included . 
mann - whitney test p < 00001 . table 1 : baseline characteristics and treatment details measurements were done before radiotherapy , at week 4 of radiotherapy , and at 2 weeks , 3 , 6 , 12 , 18 , and 24 months after radiotherapy . 
unstimulated and sodium - citratestimulated parotid saliva from each parotid duct ori ce and oor of mouth saliva were collected by standard methods.7 , 8 after treatment , clinical follow - up was monthly in year 1 , every 8 weeks in year 2 , then every 36 months until the end of year 5 . 
assessments were not blinded to treatment allocation . patient - reported qol was collected with questionnaire booklets that contained the european organization for research and treatment of cancer ( eortc ) qlqc30 quality - of - life instrument16 ( which measures generic cancer - related qol ) , the associated head and neck speci c module hn35 , 17 xerostomia questionnaire.8 patients completed the baseline booklet in the clinic before randomisation . 
follow - up booklets were sent directly to the patients homes at 2 weeks , 3 , 6 , 12 , 18 , and 24 months after radiotherapy . the modi ed and our primary objective was to assess late side - e ects . 
this endpoint was chosen because it assesses an abnormal symptom ( ie , partial but persistent or complete dryness or worse ) measured by a reliable and sensitive method for scoring late side - e ects in hnscc.18 we decided on 12 months a priori as a clinically appropriate time at which to make a valid assessment of late e ects . xerostomia secondary endpoints were the proportion of patients with any measurable salivary ow after radiotherapy , acute and other late radiation side - e ects , qol that included xerostomia - related qol as measured by the modi ed locoregional progression - free survival ( pfs ) , and overall survival . 
in march , 2007 , the independent data monitoring committee and the trial steering committee approved an increase in the target sample size to 84 evaluable patients ( ie , alive 1 year after the end of radiotherapy ) that was anticipated to be achievable with 100 randomly assigned patients . 
in vol 12 february 2011 conventional radiotherapy imrt p = 0061 p = 00096 p = 00027 p = 00029 p < 00001 number at risk conventional radiotherapy imrt p = 0028 p = 000068 p = 0025 p < 00001 p < 00001 articles not presented these sensitivity analyses because they gave similar results to the main analysis . 
we present unadjusted odds ratios ( ors ) and ors adjusted for tumour site ( oropharynx or hypopharynx ) , stage of disease ( 1 and 2 or 3 and 4 ) , and radiotherapy indication ( radical or postoperative )  . 
all other analyses are unadjusted . we compared the proportions of patients with any measurable saliva ow and proportions ever reporting grade 2 or worse acute and late side - e ects between treatment groups with fishers exact tests . 
to make some adjustment for multiple testing we used a signi cance level of 1% for all secondary side - e ects , sialometry , and qol endpoints and accordingly we provide 99% cis . 
acute and late side - e ects in our report were those where sidee ects of grade 2 or worse were experienced by at least 20% of patients in either group or those where proportions were signi cantly di erent between treatment groups . we calculated qol scores with standard algorithms with a higher score suggesting poorer qol on all scales except eortc global health status , where a higher score suggests better qol.24 we deemed di erences in eortc qol scores of 10 points or more clinically signi cant in line with eortc guidelines.25 the primary qol analysis included all completed questionnaires . 
we compared in eortc qol and xerostomia mean changes questionnaire item scores from baseline between groups by two - sample t tests . we used generalised estimating equations ( gee ) , adjusting for the correlations in multiple measurements from the same patient ( with an exchangeable correlation matrix ) to account for the longitudinal nature of the xerostomia and qol data . 
a pragmatic approach to modelling was taken , with treatment - by - time interaction terms included if they were identi ed in advance as clinically relevant or they were statistically signi cant . 
qol gee models also included terms for baseline score for the item of interest . for survival - related endpoints , alive and disease - free patients were censored at date of last follow - up . 
rtog = radiation therapy oncology group . censored 1 month before any disease recurrence , in case recurrence could adversely a ect salivary ow , and by excluding patients whose side - e ect assessment was not within 2 months either side of its expected date . 
we have 130 vol 12 february 2011 articles our analyses were based on a database snapshot frozen on may 14 , 2010 , and were done in stata version 10 . 
 this study is registered as an international standard randomised controlled trial , number isrctn48243537 . role of the funding source the funding source provided peer - reviewed approval for the trial but had no other role in study design , collection , analysis , interpretation of data , or writing of the report . 
one patient assigned to the conventional radiotherapy group was deemed ineligible because they were due to be treated with chemoradiation ( no follow - up data are available for this patient )  . 
 * * worst of subjective ( pain , dysphagia , taste alteration ) , objective ( mucosal integrity , weight ) , and management ( pain , ulcer , dysphagia , taste alteration ) grades . 
worst of subjective ( dysphagia , pain ) , objective ( weight loss , stricture , ulceration , bleeding , anaemia ) , and management ( dysphagia / stricture , weight loss , pain / ulceration , bleeding ) grades . 
worst of subjective ( roughness , sensation ) , objective ( oedema , alopecia , pigmentation change , ulcer / necrosis , telangiectasia , brosis / scar , atrophy / contraction ) , and management ( dryness , sensation , ulcer , oedema , brosis / scar ) grades . 
worst of subjective ( pain , voice hoarseness , breathing ) , objective ( oedema , mucosal integrity , respiration ) , and management ( pain , hoarseness , respiration ) grades . 
worst of subjective ( pain , mastication , denture use , trismus ) , objective ( exposed bone , trismus ) , and management ( pain , bone , trismus / mastication ) grades . 
||||worst of subjective ( pain , tinnitus , hearing ) , objective ( skin , hearing ) , and management ( pain , skin , hearing loss ) grades . table 2 : maximum acute and late side - e ect grades by treatment group vol 12 february 2011 conventional radiotherapy imrt no measurable salivary ow * ( n = 25 ) measurable salivary ow ( n = 0 ) no measurable salivary ow ( n = 18 ) measurable salivary ow ( n = 16 ) subjective xerostomia better than grade 2 6 ( 24% ) subjective xerostomia grade 2 or worse 19 ( 76% ) 10 ( 56% ) 8 ( 44% ) 12 ( 75% ) 4 ( 25% ) fishers exact test for association ( treatment groups combined ) p = 0018 . 
eortc hn35 = european organization for research and treatment of cancer head and neck speci c module hn35 . contralateral parotid was signi cantly less in the imrt group ( p < 00001 ; table 1 )  . 
45 of 47 patients randomly allocated to receive conventional radiotherapy and 45 of 47 randomly assigned to receive imrt completed radiotherapy as per protocol ; 33 of the 34 patients evaluable for the primary outcome in the conventional radiotherapy group and 37 of 39 patients evaluable for the primary endpoint in the imrt group completed radiotherapy as per protocol ( gure 1 )  . 
at 12 months , there were signi cantly fewer cases of xerostomia in the imrt group ( 25 [ 74% , 95% ci 56 to 87 ] of 34 in the conventional radiotherapy group vs 15 [ 38% , 23 to 55 ] of 39 in the imrt group ) , and the absolute reduction was 35% ( 95% ci 14 to 56 ; p = 00027 )  . 
 at 24 months , 20 ( 83% , 63 to 95 ) of 24 patients in the conventional radiotherapy group reported xerostomia versus nine ( 29% , 14 to 48 ) of 31 in the imrt group , and the absolute reduction was 54% ( 32 to 76 ; p < 00001 )  . 
the proportion of patients that reported grade 2 or worse xerostomia at 12 months did not di er by tumour site , radiotherapy indication ( primary vs postoperative ) , stage of disease , or use of neoadjuvant chemotherapy ( data not shown )  . 
a similar pattern was seen over time and between treatment groups when xerostomia was scored with the rtog scale ( gure 2 )  . 132 vol 12 february 2011 articles conventional radiotherapy imrt the only recorded acute adverse event of grade 2 or worse to di er between treatment groups ( at the 1% signi cance level ) was fatigue ( table 2 ) : 18 ( 41% ; 99% ci 23 to 61 ) of 44 patients in the conventional radiotherapy group versus 35 ( 74% ; 55 to 89 ) of 47 in the imrt group ( p = 00015 )  . 
of note , at 12 months , grade 3 or worse dysphagia was reported by two ( 5% ) of 40 patients in the conventional radiotherapy group and four ( 9% ) of 46 in the imrt group . we recorded baseline sialometry in 80 patients , all of whom had measurable salivary ow . 
at 12 months unstimulated saliva ow from the contralateral parotid gland was noted in 16 ( 47% ) of 34 patients in the imrt group compared with none of 25 in the conventional radiotherapy group ( p < 00001 )  . 
corresponding data at 24 months were seven ( 44% ) of 16 in the imrt group versus none of 15 in the conventional radiotherapy group ( p = 00068 )  . 
strong concordance was noted between measurable contralateral saliva ow and grade 2 or worse xerostomia ( table 3 )  . mean changes in global health status from baseline to 12 months were 11 ( 99% ci 99 to 121 ) for conventional radiotherapy versus 30 ( 119 to 179 ; p = 078 ) for imrt . 
 changes at 24 months were 28 ( 171 to 116 ) for conventional radiotherapy versus 83 ( 66 to 232 ) for imrt , corresponding to a between group di erence in change scores of 111 ( 90 to 312 ; p = 014 )  . 
no in change from statistically signi cant di erences baseline between groups were noted for any qlqc30 subscale scores ( data not shown )  . in both study groups , hn35 subscale scores for dry mouth , senses , and sticky saliva were signi cantly worse than baseline at 12 months . 
mean increases from baseline at 12 months in the dry mouth subscale were 565 ( 99% ci 365 to 765 ; p < 00001 ) for conventional radiotherapy and 480 ( 318 to 642 ; p < 00001 ) for imrt . 
mean increases at 24 months were 593 ( 378 to 807 ; p < 00001 ) for conventional radiotherapy and 348 ( 138 to 559 ; p < 00001 ) for imrt . 
at both time points , smaller score changes were noted in the imrt group than in the conventional radiotherapy group , although these were not signi cant at the 1% level . in the gee model for dry mouth the main treatment coe cient was 66 ( 99% ci 215 to 83 ; p = 025 ) with a treatment - by - time interaction term of 003 ( 006 to 000 ; p = 0017 ) , suggesting the di erence in dry mouth between treatment groups increases over time . 
censoring at recurrence had a negligible e ect on qol results , although the interaction term from the gee analysis 0 / 47 0 / 47 number of events / at risk conventional radiotherapy imrt time from randomisation ( months ) 1 / 42 2 / 44 5 / 34 4 / 39 1 / 30 4 / 31 1 / 29 0 / 28 0 / 23 2 / 22 0 / 19 0 / 18 0 / 15 1 / 15 0 / 11 figure 4 : kaplan - meier plot of locoregional progression - free survival by treatment group hazard ratio 153 ( 95% ci 063 to 370 )  . 
2 - year locoregional progression - free survival estimates for conventional radiotherapy 80% ( 95% ci 65 to 90 ) and for imrt 78% ( 62 to 87 ) ; absolute di erence 3% ( 15 to 20 )  . 
 became less statistically signi cant ( coe cient 002 ; p = 0080 )  . the xerostomia questionnaire was only completed by 39 patients at baseline and 12 months and by 33 patients at baseline and 24 months ( compared with 73 reporting the primary endpoint at 12 months and 55 at 24 months )  . 
 in both treatment groups all eight xerostomia questionnaire items were signi cantly worse at 12 and 24 months than at baseline and although the changes were smaller in the imrt group , no statistically signi cant di erences between group changes were noted ( webappendix p 1 )  . overall , there were seven locoregional recurrences in the conventional radiotherapy group : ve in the highdose volume and two in both the high - dose volume and electively irradiated neck . 
2 - year locoregional pfs was 80% ( 95% ci 65 to 90 ) in the conventional radiotherapy group and 78% ( 62 to 87 ) in the imrt group ( absolute di erence 3% , 95% ci 15 to 20 ; hr 153 , 95% ci 063 to 370 ; log - rank p = 034 ; gure 4 )  . 32 deaths have been reported so far ( 18 in the conventional radiotherapy group vs 14 in the imrt group ; hr for overall survival 068 , 95% ci 034 to 137 )  . 
of these deaths , 20 were due to head and neck cancer ( ten in the conventional radiotherapy group vs ten in the imrt see online for webappendix vol 12 february 2011 articles group )  . 
other causes of death in the conventional radiotherapy group were second ( non - head - and - neck ) primary cancer ( four patients ) , cardiac ( two ) , gastrointestinal complications ( one ) , and suicide ( one ) ; and in the imrt group were infection ( two ) , second primary cancer ( one ) , and gastrointestinal complications ( one )  . 
a consistently higher qlqc30 global and hn35 dry mouth qol score was reported in patients who received imrt ; between group di erences at 24 months were clinically but not statistically signi cant . 
xerostomia questionnaire results showed changes in favour of imrt in all eight questions but these di erences were not large enough to reach statistical signi cance , probably because of the small number of patients that completed this questionnaire . 
we postulate that this could be because of di erences in patient perception of the xerostomia symptom or because of other factors such as submandibular gland or oral cavity dose or comorbidity . 
before the design of our randomised trial , a few small single centre experiences had been published and a review of the published work on imrt had been done.26 no randomised trials were identi ed . 
during the recruitment period of the parsport trial two smaller randomised trials were reported in nasopharyngeal cancer from centres in asia , and several other single institutional experiences were reported.27 , 28 interpretation our trial is the largest randomised trial of imrt in head and neck cancer , and the only trial addressing squamous - cell carcinoma , the predominant form seen worldwide . 
our trial shows that imrt reduces patient - reported xerostomia , allows recovery of salivary ow , and improves quality of life after treatment compared with conventional radiotherapy . detailed analyses of the distribution of dose to the salivary tissue including parotid glands and other minor salivary glands , and its correlation with clinical outcomes are ongoing . 
initial results suggest that there is no correlation between submandibular gland dose and xerostomia . a limitation of our trial was that it was not possible to mask the treatments from patients or clinicians because of di erences in treatment delivery . 
however , results that relate to multiple secondary endpoints support the primary analysis and the size of the observed e ect is unlikely to be due entirely to assessment or reporting bias . 
after our trial was designed , several small nonrandomised studies2935 and one case - control study36 of parotid - sparing imrt have been published with a range of endpoints including saliva ow rate , patient - reported symptoms , and qol . 
 qol was assessed with eortc qlqc30 , hn35 , and the sf36 health survey and although qol scores for some domains were better for imrt patients , no improvements in patient - reported dry mouth symptoms on the hn35 questionnaire were noted . 
kam and colleagues38 reported a reduction in observer - rated severe xerostomia ( rtog grade 2 or worse ) with imrt ( 39% vs 82% ; p = 0001 ) in 60 patients with early - stage nasopharyngeal cancer . 
the results of the parsport trial are thus likely to be generalisable to all head and neck tumours for which conventional radiotherapy is used . in our study , fewer cases of acute dermatitis were recorded in patients treated with imrt than in those treated with conventional radiotherapy , although di erences were not statistically signi cant at the 1% level , probably because of reduced dose to skthe proportions of patients that reported grade 2 or worse acute xerostomia and grade 2 or worse salivary gland changes also showed reductions , albeit not statistically signi cant ( table 2 )  . 
 in an unplanned dosimetry review in a subset of patients , mean radiation doses to the posterior fossa were 2030 gy in the patients treated with imrt compared with about 6 gy in patients treated with conventional 134 vol 12 february 2011 articles radiotherapy , which could account for the recorded di erence in acute radiation fatigue . 
apart from salivary gland changes and radiation - induced xerostomia , other late side - e ects of conventional radiotherapy were not altered by imrt . our trial was too small to detect small di erences in , or conclude non - inferiority of , locoregional pfs or overall survival . 
although patients continue to be followed up for long - term survival , to show non - inferiority in overall survival to no more than 5% at 2 years ( 80% power , onesided 5% signi cance ) would need a randomised controlled trial of more than 900 patients . 
 recurrences have not been noted in the spared parotid tissue in patients treated with imrt or surgery , 21 , 39 suggesting that a large study to show non - inferiority in this tumour type is probably both impractical and inappropriate . 
our trial has shown a clinically and statistically signi cant reduction in xerostomia , improved salivary ow , and improved qol , and thus strongly supports a role for imrt in hnscc . contributors cmn and eh were responsible for the trial design , trial management , data interpretation , and writing of the report . 
cc and eam were responsible for the design and conduct of the quality assurance programme and contributed to the trial management , data interpretation , and writing of the report . 
all authors reviewed and approved the nal version of the paper . con icts of interest the authors declared no con icts of interest . acknowledgments parsport was supported by cancer research uk ( grant numbers c8996 / a8684 , trial reference number cruk / 03 / 005 )  . 
on the one hand , draft guidelines by the uk national institute for health and care excellence ( nice ) did not recommend the use of axicabtagene ciloleucel ( kite pharma / gilead ) for various types of b - cell lymphoma in adults , a decision contrary to the approval of the drug in the eu and by the us food and drug administration . 
on the other hand , nhs england ( in lieu of a formal nice recommendation ) struck a clandestine deal with novartis via the cancer drugs fund to pay for tisagenlecleucel for children and young adults with b - cell acute lymphoblastic leukaemia . 
the deal , agreed less than 10 days after the european approval of the drug , means that patients in england could be the first in europe to gain access to the treatmenta remarkable prospect for the beleaguered nhs . 
taken alone , these results seem promising , but the lack of control group in both trials and the choice of surrogate primary endpoints make the benefits difficult to discern . 
but these differences are misleading and are a consequence of the scant clinical evidence available currently , and the subjective nature of clinical decision making for these specific treatments . the key driver of the nice and nhs england decisions has been cost . 
axicabtagene ciloleucel is believed to cost more than 50 000 per quality - adjusted life - year ( qaly ) gained , which is at the upper limit of tolerance for cancer treatments . 
the manufacturer has proposed a commercial arrangement that might sway the eventual decision in favour of approval , although at the time of writing , nice has requested the manufacturer find more uk data from which a comparison with the current standard of care can be made . 
tisagenlecleucel , by contrast , which is presumably costing less than the 282 000 list price in the arrangement secured by nhs england , might have a more favourable cost per qaly because children have a longer life expectancy than older patients , provided toxicities are manageable and not debilitating . 
ultimately , more robust evidence is needed to be able to make appropriate decisions , but the high prices set by pharmaceutical companies do make it difficult for universal health - care systems to justify cost - effectiveness and treatment availability . 
we investigated whether erlotinib improves clinical outcome in these patients . methods topical was a double - blind , randomised , placebo - controlled , phase 3 trial , done at 78 centres in the uk . 
 eligibility criteria were newly diagnosed , pathologically con rmed nsclc ; stage iiib or iv ; chemotherapy naive ; no symptomatic brain metastases ; deemed unsuitable for chemotherapy because of poor ( 2 ) eastern cooperative oncology group performance status or presence of several comorbidities , or both ; and estimated life expectancy of at least 8 weeks . 
patients were randomly assigned ( by phone call , in a 1 : 1 ratio , strati ed by disease stage , performance status , smoking history , and centre , block size 10 ) to receive oral placebo or erlotinib ( 150 mg per day ) until disease progression or unacceptable toxicity . 
this study is registered , number isrctn 77383050 . findings between april 14 , 2005 , and april 1 , 2009 , we randomly assigned 350 patients to receive erlotinib and 320 to receive placebo . 
657 patients died ; median overall survival did not di er between groups ( erlotinib , 37 months , 95% ci 3242 , vs placebo , 36 months , 3239 ; unadjusted hazard ratio [ hr ] 094 , 95% ci 081110 , p = 046 )  . 
59% ( 178 of 302 ) of patients assigned erlotinib and who were assessable at 1 month developed rst - cycle rash , which was the only independent factor associated with overall survival . 
 compared with placebo , overall survival seemed to be worse in the group that did not develop rst - cycle rash ( 130 , 105161 , p = 0017 )  . 
grade 3 or 4 diarrhoea was more common with erlotinib than placebo ( 8% [ 28 of 334 ] vs 1% [ four of 313 ] , p = 00001 ) , as was high - grade rash ( 23% [ 79 of 334 ] vs 2% [ ve of 313 ] , p < 00001 ) ; other adverse events were much the same between groups . interpretation patients with nsclc who are deemed unsuitable for chemotherapy could be given erlotinib . 
patients who develop a rst - cycle rash should continue to receive erlotinib , whereas those who do not have a rash after 28 days should discontinue erlotinib , because of the possibility of decreased survival . fundingcancer research uk , roche . introduction lung cancer , the main cause of cancer - related death , accounts for nearly 14 million deaths worldwide every year , and has an annual incidence of more than 41 000 in the uk ( age standardised incidence of 48 per 100 000 ) .1 mortality from lung cancer accounts for more than 452 000 deaths in china , 342 000 in europe , and 162 000 in the usa.1 the number of lung - cancer deaths in developing countries is expected to increase during the next few decades such that by 2030 about 70% of tobacco - related deaths will occur in these countries . 
however , most patients with advanced or metastatic nsclc are elderly ( median age 72 years2 ) and many receive only active supportive care , including palliative radiotherapy , because of physician choice , poor performance status , or presence of several comorbidities.2 , 3 therefore , despite the recom mendation to treat these patients with platinum - based chemo therapy , only about 25% of elderly ( age > 65 years ) us patients3 and 29% of newly diagnosed uk patients2 currently receive any cytotoxic treatment . erlotinib is an oral egfr inhibitor that is associated with a signi cant survival bene t among patients with nsclc when used as maintenance monotherapy after rst - line chemotherapy or as second - line or third - line monotherapy.46 in chemotherapy - naive patients with vol 13 november 2012 1161 articles activating egfr mutations , erlotinib signi cantly improved progression - free survival compared with chemotherapy.7 , 8 we did a large randomised trial to determine whether erlotinib monotherapy would be bene cial as rst - line therapy in unselected patients with advanced nsclc deemed unsuitable for chemotherapy . methods study design and participants topical was a superiority phase 3 , double - blind , randomised , placebo - controlled trial . 
eligibility criteria were newly diagnosed , pathologically con rmed nsclc ; stage iiib or iv disease ; chemotherapy naive ; no symptomatic brain metastases ; deemed unsuitable for chemotherapy because of poor eastern cooperative oncology group ( ecog ) performance status ( ps 2 ) or presence of several comorbidities ( including impaired renal function with creatinine clearance < 60 ml / min ) , or both ; and estimated life expectancy of at least 8 weeks . 
other inclusion criteria were age older than 18 years , diagnosis within the past 62 days , able to take oral medication , and using e ective contraception if appropriate . 
exclusion criteria were previous treatment with any biological anticancer therapy ; previous palliative radiotherapy ( except to bone metastases , within the previous 2 weeks ) ; pregnant or lactating women ; evidence of signi cant laboratory nding or concurrent uncontrolled medical illness judged to 670 patients randomised 350 patients assigned erlotinib 329 received erlotinib 16 did not start study treatment 5 missing data * 320 patients assigned placebo 311 received placebo 7 did not start study treatment 2 missing data * 39 ineligible 1 ecog 0 / 1 with crcl > 60 ml / min 38 > 62 days of diagnosis 40 ineligible 4 ecog 0 / 1 with crcl > 60 ml / min 36 > 62 days of diagnosis 350 analysed by intention to treat 320 analysed by intention to treat reasons for stopping 2 still on study drug at end of follow - up 14 completed 12 months 40 protocol toxicity 20 non - protocol toxicity 16 clinical morbidity 21 voluntary withdrawals ( not toxicity ) 84 progressive disease 126 died 6 other 16 never started study drug 5 missing data reasons for stopping 0 still on study drug at end of follow - up 6 completed 12 months 12 protocol toxicity 13 non - protocol toxicity 2 clinical morbidity 26 voluntary withdrawals ( not toxicity ) 119 progressive disease 119 died 1 unavailable 13 other 7 never started study drug 2 missing data figure 1 : trial pro le * patients with no recorded start date of study drug or dosing details . 
patients were randomised in a 1 : 1 ratio to either once daily oral erlotinib ( 150 mg tablets ) or matching placebo , with a computer generated sequence , strati ed by disease stage ( iiib , iv ) , performance status ( 01 , 2 , 3 ) , smoking history ( never , current / former ) , and centre ( 78 sites ) , with a block size of 10 . 
patients continued to receive active supportive care , including palliative radiotherapy , at the discretion of their clinician . the primary endpoint was overall survival , measured from the date of randomisation until death from any cause . 
secondary endpoints were progression - free survival ( time until progression or death from any cause ) , tumour response ( according to response evaluation criteria in solid tumours ) , adverse events , and quality of life . 
 within 4 weeks before randomisation patients had a physical examination , assessment of comorbidities with the charlson comorbidity index ( cci ) , blood count and biochemistry , chest radiograph , and ct of the chest and abdomen . 
 presence of several comorbidities was de ned as cci of 3 or more . clinicians did physical examinations , including assessment of performance status , development of rash , and adverse events ( with national cancer institute of canada common toxicity criteria for adverse events , version 3.0 ) , and a chest radiograph every month for the rst 12 months , and every 2 months thereafter . 
we graded rash with the criteria : erythema alone ( a ) , erythema with papules ( b ) , erythema with papules and pustules ( c ) , and erythema with papules 1162 vol 13 november 2012 and con uent pustules ( d )  . 
puri cation and assessment of quality and quantity of tumour dna were done with wizard genomic dna puri cation kit ( promega , madison , wi , erlotinib ( n = 350 ) placebo ( n = 320 ) age at randomisation median ( years ) 75 years 77 ( 7282 ) 220 ( 63% ) 77 ( 7281 ) 203 ( 63% ) usa )  . 
 * all patients with a performance score of 01 had comorbidities , ie , 92% ( 98 of 106 ) had cci scores of 3 , 95% ( 101 of 106 ) had creatinine clearance < 60 ml / min , and a median age of 81 years with 81% ( 86 of 106 ) aged > 75 years old . 
we calculated compliance to study treatment by dividing the total number of tablets taken ( equivalent to number of days on study drug ) by the number of days from randomisation to death , progression , or when treatment was stopped early , and expressed results as a percentage . 
preplanned subgroup analyses included sex , histological examination , activating egfr or kras mutation , stage , smoking status , ecog score , and development of rst - cycle rash . this study is registered , number isrctn 77383050 . role of the funding source the trial was funded by cancer research uk ( c1438 / a4147 ) , with an educational grant from roche for the translational studies , but neither were involved in trial design , data analyses or interpretation , or writing of this report . 
additional support came from the university college london and university college london hospital biomedical research centre , who had no role in study design , data collection , analysis , or interpretation , or writing of the report . 
the corresponding author had the nal responsibility for the decision to submit for publication . results we recruited 670 patients from 78 centres from the uk national cancer research network between april 14 , 2005 , and april 1 , 2009 . 
our randomisation procedure gave 936 cells and by chance the rst allocation in each cell for several centres was erlotinib , producing an imbalance in the number randomised to each group ; 350 participants were as signed to receive erlotinib and 320 placebo ( gure 1 )  . 
compliance to study treatment ( de ned as patients who took their tablets for 75% of the time that they were in the trial , until they died or stopped treatment early ) , was 58% ( 204 of 350 ) for erlotinib and 63% ( 203 of 320 ) for placebo ( median compliance was 88% [ iqr 098 ] for erlotinib and 86% [ 096 ] for placebo , appendix p 4 )  . 
 after discontinuation of study treatment , the most common subsequent therapy was palliative radiotherapy , which was given to 34% ( 119 of 350 ) of patients assigned erlotinib and 36% ( 114 of 320 ) of those assigned placebo . 
 only 2% ( 12 of 670 ) of patients received a tyrosinekinase inhibitor ( n = 3 ) or chemotherapy ( n = 9 ) after disease progression , seven in the placebo group and ve in the erlotinib group . 
the only tyrosine - kinase inhibitor used was erlotinib . 657 patients died ; 314 in the placebo group and 343 in the erlotinib group , with 93% ( 608 of 657 ) of deaths attributed to progressive disease . 
we identi ed no di erence in overall survival 1164 vol 13 november 2012 articles among all patients ; median overall survival was 37 months ( 95% ci 3242 ) in the erlotinib group versus 36 months ( 3239 ) in the placebo group ( unadjusted hr 094 , 95% ci 081110 , p = 046 ; adjusted hr 092 , 078107 , p = 031 )  . 
1 year overall survival was 14% ( 95% ci 1018 ) with placebo versus 15% ( 1219 ) with erlotinib . we identi ed a signi cant improvement in progression - free survival with erlotinib ( unadjusted hr 083 , 95% ci 071097 , p = 0019 ; adjusted hr 080 , 068093 , p = 00054 ) ; median progression - free survival was 28 months ( 95% ci 2630 ) with erlotinib versus 26 months ( 2429 ) with placebo ( gure 2b )  . 
tumour response rates are shown in the appendix ( p 5 ) ; 4% ( 15 of 350 ) of patients in the erlotinib group and 2% ( seven of 320 ) of those in the placebo group had a complete or partial tumour response . among the 647 patients who started study treatment , the occurrence of any grade 34 adverse event was 75% ( 252 of 334 ) with erlotinib and 70% ( 219 of 313 ) with placebo ( p = 012 , table 2 )  . 
more patients assigned erlotinib had rash at any time and of any grade than did those assigned placebo ( 56% [ 188 of 334 ] vs 15% [ 46 of 313 ] p < 00001 )  . 
 21% ( 69 of 334 ) of patients assigned erlotinib had diarrhoea of grade 12 versus 8% ( 24 of 313 ) for placebo ( p < 00001 ) , and rash and diarrhoea mainly occurred within the rst month of treatment . 
we recorded increased diarrhoea ( mean di erence 151 ) , hair loss ( 126 ) , sore mouth ( 64 ) , and decreased constipation ( 94 ) more frequently in patients assigned erlotinib than in those assigned placebo . [ p < 00001 ] , in prespeci ed subgroup analyses , rst - cycle rash among patients assigned erlotinib was the only signi cant independent factor ( hr 024 , 95% ci 016035 , p < 00001 ; table 3 ) associated with overall survival , from a stepwise selection multivariate analysis containing rash , sex , histological examination , ecog score , stage , and smoking status . 
patients were classi ed as having rst - cycle rash ( any grade ) when the rash occurred within the rst 28 days , which was when we made the rst assessment of rash . 
of the 647 patients who started study treatment , predictor variables for overall survival * rash women vs men ecog 01 vs 23 stage iiib vs iv ex - smoker vs smoker never smoker vs smoker hazard ratio ( 95% ci ) p value 024 ( 016035 ) < 00001 081 ( 059101 ) 087 ( 053140 ) 084 ( 061110 ) 092 ( 071118 ) 064 ( 036114 ) adenocarcinoma vs non - adenocarcinoma 092 ( 066129 ) predictor variables for progression - free survival rash women vs men 041 ( 027060 ) < 00001 074 ( 044103 ) 0058 adenocarcinoma vs non - adenocarcinoma 099 ( 071137 ) ecog 01 vs 23 stage iiib vs iv ex - smoker vs smoker never smoker vs smoker 091 ( 056148 ) 083 ( 059109 ) 098 ( 076127 ) 062 ( 035110 ) * for overall survival , p values from overall tests were p = 017 for sex , p = 062 for ecog , p = 084 for histological examination , p = 023 for stage , and p = 035 for smoking status . 
for progression - free survival , p values from overall tests were p = 006 for sex , p = 086 for ecog , p = 079 for histological examination , p = 021 for stage , and p = 028 for smoking status . 
result after a stepwise selection ; rash remained the only signi cant variable in the model for overall survival and progression - free survival . table 3 : summary of multivariate analysis for overall survival and progression - free survival 017 064 055 023 051 013 095 070 021 088 010 67 who died before this assessment were excluded from this subgroup analysis , to avoid bias by classi cation of them as not having rash . 
59% ( 178 of 302 ) of patients assigned erlotinib developed rst - cycle rash ( compared with 5% [ 15 of 278 ] assigned placebo ) , and we recorded a positive correlation between overall survival ( p < 00001 ) and progression - free survival ( p < 00001 ) with in creasing rash severity . among patients assigned erlotinib who developed rash ( compared with all those assigned placebo ) , overall survival was signi cantly longer ( hr 076 , 95% ci 063092 , p = 00058 ) , as was progression - free survival ( 066 , 054080 , p < 00001 )  . 
hazard ratios for patients assigned erlotinib who did not develop rash , compared with placebo , were 130 ( 95% ci 105161 , p = 0017 ) for overall survival , and 109 ( 089136 , p = 039 ) for progression - free survival , neither of which overlapped the corresponding intervals for patients who were treated with erlotinib and developed rash , indicating that they were signi cantly di erent ( ie , evidence for an interaction )  . 
 median overall survival was 62 months ( 95% ci 4872 ) for the erlotinib and rash group , 29 months ( 2337 ) for the erlotinib without rash group , and 41 months ( 3746 ) for placebo . 
1 year overall survival was 24% ( 95% ci 1729 ) for erlotinib and rash , 10% ( 516 ) for erlotinib without rash , and 18% ( 1221 ) for placebo . 
for erlotinib and rash compared with placebo , the number needed to treat to save one life at 6 months was seven and vol 13 november 2012 1165 articles erlotininb , no rash ( events 120 ) erlotininb , rash ( events 175 ) placebo ( events 272 ) erlotinib , no rash vs placebo hr 130 ( 95% ci 105161 ) p = 0017 erlotinib , rash vs placebo hr 076 ( 95% ci 063092 ) p = 00058 number at risk erlotinib , no rash erlotinib , rash placebo erlotininb , no rash ( events 122 ) erlotininb , rash ( events 173 ) placebo ( events 278 ) erlotinib , no rash vs placebo hr 109 ( 95% ci 089136 ) p = 039 erlotinib , rash vs placebo hr 066 ( 95% ci 054080 ) p < 00001 number at risk erlotinib , no rash erlotinib , rash placebo time since randomisation ( months ) figure 3 : overall survival and progression - free survival according to whether patients on erlotinib developed rst - cycle rash or not hr = hazard ratio . 
median progression - free survival was 34 months ( 95% ci 3140 ) for erlotinib and rash , 25 months ( 2228 ) for erlotinib without rash , and 29 months ( 2732 ) for placebo . we identi ed overall survival bene ts in patients who developed rst - cycle rash in all subgroups including those with the worst characteristics : ecog performance status 3 , overall survival hr 058 ( 95% ci 038089 , p = 0012 ) and progression - free survival hr 041 ( 026065 , p < 00001 ) ; stage iv , overall survival hr 066 ( 052084 , p < 00001 ) and progression - free survival hr 056 ( 044072 , p = 00009 ) ; and age 75 years or older , overall survival hr 077 ( 061097 , p = 0028 ) and progression - free survival hr 071 ( 056089 , p = 00032 )  . 
 kaplan - meier curves for overall survival were much the same for patients assigned placebo who did or did not develop rash ( p = 035 , data not shown )  . patients assigned erlotinib who developed rst - cycle rash had a higher occurrence of fatigue and diarrhoea than did those assigned erlotinib who did not develop rash ( appendix p 7 )  . 
the proportions with grade 34 fatigue were 30% ( 53 of 178 ) for erlotinib and rash , 19% ( 24 of 124 ) for erlotinib without rash , and 26% ( 72 of 278 ) for placebo . 
for grade 34 diarrhoea , the proportions were 11% ( 20 of 178 ) for erlotinib and rash , 6% ( eight of 124 ) for erlotinib without rash , and 1% ( four of 278 ) for placebo . 
when we excluded rst - cycle rash , the proportion of patients reporting at least four grade 34 adverse events was 47% ( 84 of 178 ) for erlotinib and rash , 19% ( 23 of 124 ) for erlotinib without rash , and 36% ( 99 of 278 ) for placebo ( appendix p 8 )  . 
among patients assigned erlotinib who developed rash , we recorded much the same e ects on quality of life as we did in the main analysis , with dyspnoea ( 93 ) and chest pain ( 67 ) signi cantly improved compared with patients without rash ( appendix p 9 )  . appendix p 2 shows the results of the other prespeci ed subgroup analyses , according to the presence or absence of rash in participants assigned erlotinib . 
among patients without rash , we identi ed no evidence of bene t , and overall survival might be worse for some subgroups , such as men ( hr 152 , 95% ci 113204 , p = 00046 ) , or ecog performance status 3 ( 169 , 111258 , p = 0014 )  . 
 patients assigned erlotinib who developed rash had longer overall survival and progression - free survival than did those assigned erlotinib who did not develop rash irrespective of baseline charac teristics , although some subgroups , including women ( overall survival hr 066 , 95% ci 048090 , p = 00090 ) and patients with adenocarcinoma ( 055 , 039077 , p = 000049 ) seemed to have a greater bene t than did other subgroups . 
 median overall survival for erlotinib and rash versus placebo was 81 months ( 95% ci 62104 ) versus 45 months ( 3956 ) for women , and 49 months ( 4163 ) versus 38 months ( 3344 ) for men . 
 however , the interaction test between sex and treatment was not signi cant ( p = 029 ) , and some of this di erence might be explained by a higher compliance to erlotinib in women ( 68% , 81 of 119 ) than in men ( 52% , 101 of 195 )  . 
 appendix p 10 shows further results for overall survival and progression - free survival according to sex and histological examination . in our biological substudy , dna was available for 390 patients out of 398 ( 58% of total study population ) who provided material . 
of the 28 egfr mutation - positive samples , 11 had exon 19 deletions , ten had a mutation at exon 21 ( 858leuarg ) , and seven had other mutations . 
in these patients , median overall survival was 104 months ( 95% ci 55151 ) for erlotinib ( n = 17 ) versus 37 months ( 03493 ) for pla cebo ( n = 11 )  . 
 among patients with wild - type egfr who were assigned erlotinib and developed rash ( n = 94 ) , hr for overall survival was 086 ( 95% ci 066112 , p = 027 ) and for progression - free survival was 069 ( 053090 , p = 00070 ; appendix p 2 )  . 
hr for those assigned erlotinib who did not develop rash ( n = 67 ) was 128 ( 095172 , p = 010 ) for overall survival and 105 ( 078141 , p = 074 ) for progression - free survival . kras mutation - positivity was not associated with overall survival or progression - free survival . 
among those who were kras mutation - positive , median overall survival was 42 months ( 95% ci 1862 ) for erlotinib ( n = 35 ) versus 36 months ( 1944 ) for placebo ( n = 38 ) ; median progression - free survival was 35 months ( 1748 ) versus 27 months ( 1839 )  . 
patients with wild - type kras had median overall survival of 37 months ( 2842 ) for erlotinib ( n = 210 ) versus 34 months ( 2743 ) for placebo ( n = 180 ) ; median progression - free survival was 27 months ( 2229 ) for erlotinib and 26 months ( 2329 ) for placebo . 
the presence or absence of rst - cycle rash did not a ect the results ( data not shown )  . discussion first - line treatment with erlotinib did not improve overall survival in all unselected patients with advanced nsclc deemed unsuitable for chemotherapy treatment , who usually have a poor prognosis ( about 34 months median overall survival10 )  . 
additionally , in prespeci ed subgroup analyses , com pared with placebo , erlotinib signi cantly improved both overall survival and progression - free survival for patients who developed a rst - cycle rash ; median overall survival in this group increased by 21 months , from 41 months to 62 months . 
however , few patients assigned placebo developed rst - cycle rash ( 5% compared with 59% assigned erlotinib ) , and we identi ed no di erence in survival in patients assigned placebo who had rash compared with those who did not . 
few patients were lost to follow - up because survival is short and patients with lung cancer in the uk are seen regularly and remain under the care of a hospital physician . a limitation of our study was that the incidence of egfr mutation was only 7% and a quarter of them were uncommon mutations . 
most egfr mutation studies focus on so - called hot spot analysis , looking only for common alterations , short deletions in exon 19 , or the 858leuarg point mutation in exon 21 . 
our population were mostly elderly , white , present or exsmokers , and such groups might have a di erent mutation spectrum pro le , which further studies could examine . 
never theless , although analyses were based on only 28 patients , overall survival and progressionfree survival were improved in patients with an egfr mutation who were assigned erlotinib , consistent with ge tinib in patients with poor performance status.13 however , patients with tumours showing wild - type egfr also showed bene t when they developed an erlotinib - related rash . 
in the ipass study , 14 only 56% ( 683 ) of patients provided samples with egfr mutation data available in 36% ( 437 ) of the 1217 patients randomised . 
this proportion was much the same as in our trial where samples from 58% of patients had su cient dna for analysis . another limitation of our study is that we did routine ct scans at 3 and 6 months , whereas some other studies have used ct scans every 68 weeks , so our schedule might be deemed suboptimum for assessment of progression - free survival . 
also , we included patients of performance status 2 , for whom , on the basis of evidence reported in 2005 , 15 chemotherapy could improve survival , and a phase 2 study16 has shown that doublet chemotherapy has a better survival than single agent chemotherapy . 
however , when topical was designed , provision of chemotherapy to such patients was not routine practice because many studies with second and third generation chemotherapy had not shown survival bene t , and many of these patients had serious adverse events.17 , 18 a limitation of many of the more recent chemotherapy trials is that median age of patients of performance status 2 is 65 years or younger , median survival is much the same as for patients of performance status 01 , and many go on to receive second - line treatment , suggesting that they are a highly selected group . 
by contrast , in topical median age was 77 years , 90% of participants had several comorbidities , and less than 2% were given second - line treatment , which is indicative of the real - world scenario that lung cancer is a disease of elderly people with comorbidities , and many of these patients still continue to be treated with best supportive care worldwide , including palliative radiotherapy.19 when topical was designed some evidence already suggested that development of a rash during erlotinib vol 13 november 2012 1167 articles panel : research in context systematic review we did not do a systematic review of scienti c literature before designing the topical trial ( in 2002 ) , because at the time there were no other studies of rst - line egfr inhibitors in patients with advanced non - small - cell lung cancer ( nsclc ) who were elderly or had poor performance status . 
these patients are often excluded from rst - line chemotherapy trials . lung cancer is predominantly a disease of elderly people , and elderly patients with advanced nsclc deemed unsuitable for chemotherapy with poor performance status ( 2 and 3 ) or several comorbidities , or both , remain a major challenge . 
since topical , no phase 3 trials of rst - line monotherapy for this group have been reported . interpretation the ndings of topical and other trials58 show that erlotinib is an important treatment for patients with nsclc in various clinical settings , including as maintenance after rst - line chemotherapy , as second - line or third - line monotherapy in unselected patients with advanced nsclc , and in chemotherapy - naive patients with activating egfr mutations . 
however , unlike the topical patients , most of the patients in other studies had good performance status . the clinical implications of the topical trial are that patients who are deemed unsuitable for chemotherapy could be given erlotinib . 
those who have egfr mutation - positive tumours could receive continuous erlotinib ; whereas those who have wild - type tumours should discontinue erlotinib after about 28 days if they do not develop a rash because of the possibility of decreased survival . therapy could be associated with improved outcomes across several cancers including nsclc.20 with this knowledge , we developed a scoring system for rash as part of the topical protocol , and speci ed a preplanned subgroup analysis . 
furthermore , retrospective analyses of two phase 3 nsclc trials show a positive correlation between rash and treatment e ect on survival : the br.21 trial12 of erlotinib and the flex trial11 of cetuximab , an anti - egfr antibody , when added to rst - line chemotherapy . 
researchers have recorded much the same ndings in trials of pancreatic cancer , locally advanced head and neck cancer , and metastatic colorectal cancer.12 , 21 , 22 currently no clear biological explanations link erlotinib activity with rash , but rash probably represents greater uptake of the drug . 
smokers have a lower plasma concentration of erlotinib than do non - smokers.23 , 24 smokers also have a lower incidence of skin rash and have less clinical bene t from egfr inhibitors compared with non - smokers.23 , 24 this nding was con rmed in topical because present smokers in the erlotinib group were less likely to develop rash when compared with former smokers ( odds ratio 029 , 95% ci 018048 ) or never - smokers ( 020 , 006066 )  . 
 increased occurrence of skin rash has been identi ed in a phase 2 dose escalation study of erlotinib , although another study suggested that dose - escalation does not improve incidence or out come.25 , 26 alternatively , skin rash might be a surrogate marker of patients able to mount antitumour immune response . 
data increasingly suggest the importance of the host immune system in control of cancer cell growth after tyrosine - kinase inhibitor treatments.27 , 28 as reported with other tyrosinekinase inhibitors , erlotinib could enhance cytotoxic t - cell in ltration . drug uptake and cytotoxic t - cell in ltration could be linked , with increased uptake of drug causing increased egfr blockade and cell killing , resulting in improved host immune response . 
future studies could examine whether combining erlotinib and immunomodulatory agents can further fuel a more robust immunological response , increase the severity and incidence of skin rash , and potentially further improve durability of response , progression - free survival , and overall survival in this group of patients who are deemed not suitable for chemotherapy . a phase 2 study10 of ge tinib ( n = 201 ) compared with placebo ( instep ) in a group of patients with similar characteristics to those in topical showed no statistical di erence in survival with a hr of 084 ( 95% ci 062115 ) , but we identi ed a suggestion of a bene t among patients with high egfr gene copy number determined by uorescence in - situ hybridisation ( hr 044 , 95% ci 017112 )  . 
the dose of ge tinib might have been sub therapeutic in patients with wild - type egfr tumours , and this notion is supported by the lower than expected proportion who developed rash . 
 another phase 2 trial29 of only patients of performance status 2 ( n = 103 ) with a median age of less than 70 years compared erlotinib with carboplatin and paclitaxel , and showed that progression - free survival was better with chemotherapy than with erlotinib but progression - free survival did not di er between patients assigned erlotinib who developed rash compared with those who were assigned chemotherapy ( hr 094 , 95% ci 056159 )  . 
in topical , erlotinib seemed to have a greater e ect in some subgroups than in others ( eg , median overall survival was improved by 36 months for women with rash and 11 months for men with rash )  . 
previous studies have also reported sextreatment interactions with tyrosine - kinase inhibitors and other chemotherapies , where female patients bene ted more than men.30 diarrhoea , hair loss , and fatigue were expected adverse events associated with erlotinib , and their severity was usually mild to moderate . 
overall , occur rence and severity of adverse events in topical were much the same as those in the saturn and br.21 trials despite our population being predominantly elderly patients with poor performance status ( ecog 23 ) .5 , 6 taking erlotinib tablets at home should be more convenient to patients compared with treatments that require administration in hospital . 
we believe that patients with poor performance status and activating egfr mutation tumours should 1168 vol 13 november 2012 articles receive erlotinib or ge tinib , in line with the established evidence in patients with good per formance status , and supported by the nding that the small number of these patients in topical all developed rash.7 , 8 , 14 our data suggest patients with egfr wild - type or unknown egfr status tumours could start erlotinib but they should discontinue if they do not develop rash within 28 days , because these patients had no bene t in overall survival or progression - free survival , and in some subgroups overall survival could be reduced if erlotinib were taken continuously ( panel )  . 
the reasons for this nding are unknown but for some of our patients ( especially men and those with ecog performance status of 3 ) , the disease might be so advanced that any toxic treatment could accelerate deaths . 
researchers have recorded deleterious e ects of anti - egfr in some patients treated with erlotinib or cetuximab.31 , 32 a strategy of use of rst - cycle erlotinib - induced rash to select patients with poor performance status for continued treatment could substantially improve cost e ectiveness . 
second and third line erlotinib is marginally cost - e ective compared with best supportive care , therefore rst - line erlotinib could be more cost - e ective.33 egfr testing has now become standard of care to select patients who are egfr mutation - positive for treatment with tyrosine - kinase inhibitors . 
if erlotinib is to become a standard therapy for patients who have egfr wild - type tumours and are unsuitable for chemotherapy ( 93% in our trial ) it should be in a selected population . 
prospective studies are needed to increase our understanding of the biological mechanism linking rash and erlotinib bene t , including dose - escalation studies or studies of the relation between rash and tumour egfr copy number.34 further translational research with our biological samples might identify candidate markers for erlotinib - induced rash that can preselect patients for treatment with a marker measured at baseline , without having to treat all patients for 4 weeks , and then discontinue those without rash . contributors sml had the initial trial concept ; sml , cb , rr , and ah designed the trial ; sml , su , cl , sf , gs , em , pjw , mh , rl , rj , et , dc , gm , and sb were centre investigators , and recruited and treated patients ; sml , ik , yn , and ah were involved in trial conduct ; sml , ik , cb , and ah analysed and interpreted the data ; ik did the statistical analyses ; sml , cb , and ah wrote the report . 
all authors reviewed and approved the nal report . con icts of interest cl , et , dc , gm , and sml have received travel grants and honoraria from roche uk for serving on advisory boards . 
all other authors declare that they have no con icts of interest . acknowledgments the trial was funded by cancer research uk ( c1438 / a4147 ) , with an educational grant from roche for the translational studies , and support from the university college london and university college london hospital biomedical research centre ( who part - fund sml )  . 
we thank the independent data monitoring committee for their helpful advice and comments throughout the trial , gerard kingdon for secretarial assistance , rachel partridge , nicole gower , sumrana ali ( trial coordination and data management ) , and nirali patel ( tissue collections )  . correction to lancet oncol 2016 ; 17 : 74756 correction to lancet oncol 2018 ; 19 : 153042 correction to lancet oncol 2019 ; 20 : 81626 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
lancet oncol 2016 ; 17 : 74756in results , median overall survival should have been median time of death ( after randomisation ) in eleven patients who died from progressive disease . 
prognostic value of end - of - induction pet response after first - line immunochemotherapy for ( gallium ) : follicular secondary analysis of a randomised , phase 3 trial . 
 lancet oncol 2019 ; 20 : 81626 the appendix of this article has been updated as of may 10 , 2019 . published online april 29 , 2019 s1470 - 2045 ( 19 ) 30280 - 3 published online may 10 , 2019 s1470 - 2045 ( 19 ) 30292 - x published online may 10 , 2019 s1470 - 2045 ( 19 ) 30293 - 1 correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
this correction has been made to the online version as of may 29 , 2019 . correction to lancet oncol 2019 ; 20 : 82736 shitara k , iwata h , takahashi s , et al . 
lancet oncol 2019 ; 20 : 82736the appendix of this article has been updated as of may 10 , 2019 . correction to lancet oncol 2019 ; 20 : 84961 eng c , kim tw , bendell j , et al . 
 atezolizumab with or without cobimetinib versus regorafenib previously treated metastatic colorectal cancer ( imblaze370 ) : a multicentre , open - label , phase 3 , randomised , controlled trial . 
this correction has been made to the online version as of may 29 , 2019 and the printed article is correct . correction to lancet oncol 2019 ; 20 : e26273 ngiam ky , khor iw . 
lancet oncol 2019 ; 20 : e26273tables 1 and 2 in this article have been corrected as of april 29 , 2019 . correction to lancet oncol 2019 ; 20 : 297310 cella d , grnwald v , escudier b , et al . 
this update has been made online as of may 29 , 2019 . vol 20 june 2019 e293 corrections corrections correction to lancet oncol 2007 ; 8 : 1099 correction to lancet oncol 2013 ; 14 : 1245 correction to lancet oncol 2014 ; 15 : 133 oncol lancet xue f , michels kb . 
 2007 ; 8 : 1088100in this article , the con icts of interest statement should have read kbm has provided expert testimony on diethylstilbestrol and infertility and adverse pregnancy outcomes . 
afatinib for lung cancer : let there be light ? lancet oncol 2014 ; 15 : 13334in this comment , the sixth sentence of the fourth paragraph should begin furthermore , for progressionthe derived hr free survival of patients with rare mutations.... 
lancet oncol third 2013 ; sentence of this comment should read the comparz trial , 2 comparing in 1110 sunitinib with pazopanib showed pazopanib was patients , non - inferior sunitinib , with median progression - free survival of 84 months and a response in 31% of patients in the pazopanib group compared with a median progressionfree survival of 95 months and a response in 25% of patients in the sunitinib group , thereby con rming both drugs as reasonable rst - line options . 
this correction has been made to the online version as of march 3 , 2014 . vol 15 march 2014 e106 articles purged versus non - purged peripheral blood stem - cell transplantation for high - risk neuroblastoma ( cog a3973 ) : a randomised phase 3 trial susan g kreissman , robert c seeger , katherine k matthay , wendy b london , richard sposto , stephan a grupp , daphne a haas - kogan , michael p laquaglia , alice l yu , lisa diller , allen buxton , julie r park , susan l cohn , john m maris , c patrick reynolds , judith g villablanca summary background myeloablative chemoradiotherapy and immunomagnetically purged autologous bone marrow transplantation has been shown to improve outcome for patients with high - risk neuroblastoma . 
we did a randomised study of tumour - selective pbsc purging in stem - cell transplantation for patients with high - risk neuroblastoma . methods between march 16 , 2001 , and feb 24 , 2006 , children and young adults ( < 30 years ) with high - risk neuroblastoma were randomly assigned at diagnosis by a web - based system ( in a 1 : 1 ratio ) to receive either nonpurged or immunomagnetically purged pbsc . 
all patients were treated with six cycles of induction chemotherapy , myeloablative consolidation , and radiation therapy to the primary tumour site plus metaiodobenzylguanidine avid metastases present before myeloablative therapy , followed by oral isotretino pbsc collection was done after two induction cycles . 
pbsc were collected from 229 patients from the purged group and 236 patients from the non - purged group , and 180 patients from the purged group and 192 from the non - purged group received transplant . 
toxic deaths occurred in 15 patients during induction ( eight in the purged group and seven in the non - purged group ) and 12 during consolidation ( eight in the purged group and four in the non - purged group )  . 
the most common adverse event reported was grade 3 or worse stomatitis during both induction ( 87 of 242 patients in the purged group and 93 of 243 patients in the non - purged group ) and consolidation ( 131 of 177 in the purged group vs 145 of 191 in the non - purged group )  . 
serious adverse events during induction were grade 3 or higher decreased cardiac function ( four of 242 in the purged group and ve of 243 in the non - purged group ) and elevated creatinine ( ve of 242 in the purged group and six of 243 non - purged group ) and during consolidation were sinusoidal obstructive syndrome ( 12 of 177 in the purged group and 17 of 191 in the nonpurged group ) , acute vascular leak ( 11 of 177 in the purged group and nine of 191 in the non - purged group ) , and decreased cardiac function ( one of 177 in the purged group and four of 191 in the non - purged group )  . interpretation immunomagnetic purging of pbsc for autologous stem - cell transplantation did not improve outcome , perhaps because of incomplete purging or residual tumour in patients . 
non - purged pbsc are acceptable for support of myeloablative therapy of high - risk neuroblastoma . funding national cancer institute and alexs lemonade stand foundation . introduction high - risk neuroblastoma has a high rate of recurrence , most commonly in bone and bone marrow.1 results from the childrens cancer group ( ccg ) - 3891 trial2 showed that myeloablative chemotherapy with rescue with immunomagnetic bead purged autologous bone marrow improved outcome compared with conventional dose chemotherapy . 
 blood has no or fewer neuroblastoma cells detectable by immunocytology even when bone marrow is positive.5 ( qrtpcr ) can detect quantitative real - time pcr neuroblastoma mrna in pbsc , 68 although the e ect of infusing these pbsc has not been de ned . 
we report the results of the randomised childrens oncology group ( cog ) a3973 trial , which compared outcomes for high - risk neuroblastoma patients who received autologous purged versus non - purged pbsc after myeloablative chemotherapy . 
to our knowledge , this is the rst randomised study in any cancer to evaluate the e ect of tumour - selective pbsc purging . methods study design and participants this phase 3 trial was open from feb 9 , 2001 , to march 31 , 2006 , for children with high - risk neuroblastoma . 
patients or parents or guardians provided written informed consent according to national cancer institute and local institutional review board guidelines . patients were enrolled from 95 cog member institutions in the usa ( 420 ) and canada ( 66 )  . 
eligible patients had high - risk neuroblastoma according to the childrens oncology group ( cog ) criteria , including previously untreated neuroblastoma in patients younger than 1 year with international neuroblastoma staging system9 ( inss ) stage 3 , 4 , or 4s mycn ampli ed tumours and , in children aged 1 year or older , stage 4 tumours , stage 3 tumours with either unfavourable histology or mycn ampli cation , stage 2 tumours with unfavourable histology and mycn ampli cation , and initially low - risk patients treated with surgery only who later progressed with metastatic disease.9 we excluded patients aged 1218 months with stage 4 mycn nonampli ed favourable histology , and hyperdiploid tumours after an amendment in may , 2004.10 additional eligibility criteria included age up to 30 years , no previous history of chemotherapy , registration on companion biology study , ability to tolerate pbsc collection , and adequate cardiac , liver , and renal function . 
 tumours and randomisation and masking patients were randomly assigned to treatment at study enrolment using the cogs online remote data entry system , which assigned treatment group in real - time based on the balance existing at that time , within blocks of size four . 
the method was random until such time as a random assignment exceeded the prespeci ed margin of two within a block , and only then did the method become deterministic . 
patients were randomly assigned ( ratio 1 : 1 ) to receive either purged pbsc or non - purged pbsc at study entry ; patients and treating physicians were not masked to this assignment . 
randomisation was strati ed into blocks by international neuroblastoma staging system ( inss ) stage , 9 age at diagnosis ( < 365 days or 365 days ) , mycn gene status ( ampli ed or nonampli ed ) , and international neuroblastoma pathology classi cation ( inpc ; unfavourable or favourable ) .11 procedures all patients were prescribed identical chemotherapy , radiotherapy , and post - myeloablative isotretinoin ( gure 1 )  . 
 patients without progressive disease and adequate organ function received myeloablative carboplatin , etoposide , and melphalan , 12 with dose adjustment for glomerular ltration rate ( gfr ) lower than 100 ml / min per 173 m.13 after local irradiation , patients could enrol in the cog anbl0032 trial isotretinoin plus chimeric anti - gd2 monoclonal antibody ch14.18 , interleukin 2 , and gm - csf versus isotretinoin alone , 14 with randomisation strati ed by assigned arm of this study . 
we assessed response using the international neuroblastoma criteria.9 we graded adverse events using the national cancer institutes common toxicity criteria , version 2.15 reporting was required for all grade 35 toxic e ects ( non - targeted )  . 
 to monitor safety during the study , the protocol required reporting of all grades of speci c organ function and infectious toxic e ects ( targeted )  . response pbsc were collected after two induction cycles regardless of histological tumour content in the bone marrow . 
requirements to proceed to consolidation were : immunocytology - negative pbsc with minimum of 1510 cd34 cells per kg for non - purged pbsc or minimum of 110 viable cd34 cells per kg for purged pbsc . 
we determined viability on a thawed purged pbsc aliquot using trypan blue.16 patients with insu cient purged pbsc could receive non - purged pbsc ( or purged bone marrow if non - purged pbsc also insu cient ) meeting protocol criteria . 
we de ned neutrophil engraftment as the rst of three consecutive absolute neutrophil counts of more than 500 cells per l ; and platelet engraftment as the rst of three consecutive platelet counts of more than 20 000 without transfusion . institution and transplant the non - purged pbsc were cryopreserved at collecting sites . 
for purged pbsc , heparinised pbsc were transported overnight at ambient temperature to a the day after centralised leukapheresis according to us food and drug administration ( fda ) ide# bb - ide 2259 . 
pbsc were mixed with 200300 mg of carbonyl iron per 10 total laboratory and purged 1000 vol 14 september 2013 articles cells to remove phagocytic cells and decrease the number of immunomagnetic beads required . 
remaining cells were mixed with immunomagnetic beads using ve monoclonal antibodies targeting neuroblastoma cell surface antigens ( 459 , hsan 12 , ba - 1 , hnk - 1 , and 126 - 4 ; appendix )  . 
 magnetic beads and attached cells were removed using samarium cobalt magnets.16 purged samples were suspended in l15 containing human serum albumin 10% volume / volume ( central lab , blood transfusion service , swiss red cross , bern , switzerland ) , hetastarch 15% weight / volume , and dmso 10% volume / volume ( cryoserv , ben venue laboratories inc , bedford , oh , ( baxter - fenwal , usa ) deer eld , nj , usa )  . 
cryopreserved products were shipped to transplant centres in mve ln2 dry shippers with constant temperature monitoring by overnight air delivery . in cryocyte freezing bags to detect neuroblastoma cells in pbsc , immuno cytology and tlda assays were done on a pbsc aliquot from day leukapheresis on all patients before purging . 
immunocytology used monoclonal antibodies against cell surface antigens ( 126 - 4 , 390 , 459 , hsan12 , and bw575 ) .17 , 18 the tlda assay quanti ed chga , dcx , ddc , phox2b , and th mrna expression . 
 we deemed results to be detectable if one or more of the ve genes had a cycle threshold ( ct ) value lower than 40 and to be undetectable if no signal was detected for any genes after 40 cycles ( ct = 40 )  . 
we did a second analysis of the same data using only phox2b and th mrna expression to de ne detectable samples ( appendix )  . statistical analysis analyses were done by intention to treat . 
we targeted an enrolment of 486 patients , which would provide 80% power for a one - sided log - rank test of superiority of the purged group over the non - purged group at a level of 005 , able to detect a 9% improvement in 2 - year eventfree survival ( 38% vs 47% )  . 
 we did an intention - to - treat sequential monitoring of the trial , and considered early stopping if the groups proved19 or would never prove20 to be signi cantly di erent , or if the conditional power fell under 20% . 
we calculated the relative risk as the ratio of non - purged to purged using the planning variables for 2 - year event - free survival , and under the alternative hypothesis , it would equal 133 . 
the fleming - harrington - obrien20 lower ( futility ) boundary induction consolidation ahsct radiotherapy isotretinoin pbsc harvest pbsc infusion at least 48 h after cem induction chemotherapy cycles : 1 , 2 , 4 , 6 cyclophosphamide doxorubicin vincristine cycles : 3 and 5 cisplatin etoposide 21 g / m per day intravenously 2 days 25 mg / m per day intravenously continuous infusion 3 days 067 mg / m per day intravenously continuous infusion 3 days 50 mg / m per day intravenously 4 days 200 mg / m per day intravenously 3 days consolidation chemotherapy ahsct ( cem ) melphalan carboplatin etoposide g - csf 70 mg / m per day intravenously 3 days 425 mg / m per day intravenously 4 days ( if gfr 100 ml / min per 173 m ) adjust dose to auc 41 per day using calvert formula ( if gfr < 100 ml / min per 173 m ) 338 mg / m per day intravenously 4 days ( if gfr 100 ml / min per 173 m ) 200 mg / m per day intravenously 4 days ( if gfr < 100 ml / min per 173 m ) 5 g / kg per day until anc > 2000 l for 3 days fractionated radiotherapy ( 2160 cgy ) given in 12 equal fractions of 180 cgy per fraction to primary site and to all mibg avid metastatic sites at end induction beginning 3045 days after pbsc infusion isotretinoin 80 mg / m per dose orally twice a day 14 days given every 28 days for six courses starting day 60 radiation therapy post - ahsct therapy figure 1 : treatment schema pbsc = peripheral blood stem cells . 
mibg = i or imeta - iodobenzylguanidine . see online for appendix was equivalent to repeated testing of the alternative hypothesis at p = 0005 for a cumulative level of 005 . 
trial e cacy results remained masked until release by the data safety monitoring committee after all patients had completed protocol therapy . the primary endpoint was event - free survival , for which the time to event was calculated from study enrolment and randomisation until rst occurrence of relapse , progressive disease , secondary malignancy , death , or until last contact with the patient if no event occurred . 
we generated kaplan - meier survival curves.21 we report 5 - year point estimates with 95% ci.22 with the exception of the sequential monitoring , we deemed p values lower than 005 signi cant . 
one additional patient who received a transplant was retrospectively ( post - transplant ) determined by the treating institution to have had progressive disease at the end of induction ; thus table 1 presents a total of 38 patients in the purged group with end of induction progressive disease . 
the corresponding author had nal responsibility for the decision to submit for publication . results the trial ended after 495 patients had been enrolled ( patients were enrolled from march 16 , 2001 , to feb 24 , 2006 )  . 
baseline characteristics were much the same in each group and seemed similar to the cog overall high risk cohort ( table 1 ) .2 median age of the patients was 31 years ( range 02291 years )  . 
of the 486 eligible for randomisation , 137 ( 28% ) patients subsequently enrolled in the cog anbl0032 trial after transplantation , and 78 ( 16% ) were assigned to the ch14.18 antibody group ( 36 of 243 in the purged group and 42 of 243 in the non - purged group )  . we obtained pbsc from 465 ( 96% ) of 486 randomised patients : 229 in the purged group and 236 in the nonpurged group . 
reasons patients were not transplanted included progressive disease ( 28 from purged group and 25 from non - purged group ) or death during induction ( eight from purged group and seven from non - purged group ) , organ toxic e ects ( seven from purged group and ve from non - purged group ) , withdrawal from protocol ( three from purged group ) , insu cient pbsc ( ve from purged group and one from non - purged group ) , insu cient response ( two from purged group and four from non - purged group ) , and other ( ten from purged group and nine from non - purged group )  . 
29 patients randomly assigned to purged pbsc could not comply because of insu cient pbsc yield for purging ( 12 patients ) or after purging ( eight patients ) , regulatory or technical issues ( six patients ) , positive microbial culture of pbsc ( one patient ) , and parental refusal ( two patients )  . 
the fth patient , also assigned to receive nonpurged pbsc , had a negative sample from day 1 immunocytology , but the pooled pbsc collection had positive immunocytology before purging . 
we also noted no di erence in event - free survival or overall survival from the time of transplantation between the purged and non - purged groups who completed transplantation ( gure 3c , d )  . 
post - hoc analysis by treatment actually received showed no di erence in event - free survival ( p = 081 ) or overall survival ( p = 089 ) from study enrolment between groups ; similar results were noted when event - free survival ( p = 015 ) and overall survival time of transplantation ( data not shown )  . 
in the 354 patients with stage 4 disease older than 18 months , event - free survival ( p = 032 ) or overall survival ( p = 077 ) from enrolment did not di er between the purged and nonpurged groups . 
outcome was similar for individuals with protocol - de ned low compared with normal gfrs . ( p = 023 ) were measured from although potentially underpowered and done post - hoc , analyses suggested that 5 - year event - free and overall survival for the 270 patients with stage 4 disease with invaded bone marrow at diagnosis did not signi cantly di er between groups ( p = 020 for event - free survival and p = 050 for overall survival )  . 
similarly , for the 120 patients who were stage 4 with invaded bone marrow after two cycles of chemotherapy ( at the time of pbsc collection ) , there was no di erence between groups in terms of 5 - year event - free or overall survival ( p = 022 for event - free survival and p = 052 for overall survival )  . 
 the 245 patients with tlda results from day 1 of leukapheresis ( before purging ) were representative of all 486 patients in terms of clinical and prognostic characteristics ( data not shown )  . 
of these 245 patients , 122 ( 50% ) had detectable tumour mrna by the ve - gene tlda : 68 ( 53% ) of 129 patients in the purged group and 54 ( 47% ) of 116 patients in the non - purged group ( table 1 )  . 
 patients with detectable tlda had lower event - free survival ( at 5 years 29% , 95% ci 2138 ) and overall survival ( at 5 years 41% , 95% ci 3250 ) than did patients with undetectable tlda ( 5 - year event - free survival 51% , 95% ci 4260 ; p = 00003 ; and 5 - year overall survival 62% , 95% ci 5370 ; p = 00017 ; gure 4 )  . 
when we analysed the same data using only expression of th and phox2b , 62 ( 25% ) patients had detectable tlda ( 34 in the purged group and 28 in the non - purged group ) , with lower event - free survival ( at 5 years 26% , 95% ci 1637 ) and overall survival ( at 5 years 35% , 95% ci 2347 ) than those with undetectable tlda ( 5 - year event - free survival 45% , 95% ci 3852 ; p = 0005 ; and 5 - year overall survival 58% , 95% ci 5065 ; p = 001 )  . 
60 ( 33% ) of 183 pbsc with undetectable two - gene tlda ( phox2b and th ; 34 in the purged group and 26 in the non - purged group ) were detectable using ve genes . su cient numbers of cd34 cells per protocol criteria were obtained in 443 of 465 patients : 221 of 229 in the purged group and 222 of 236 in the non - purged group . 
 unknown day 1 immunocytology tlda analysis of pbsc from day 1 of leukapheresis tumour detectable tumour undetectable no tlda specimen obtained or specimen of insu cient quality overall response at the end of induction number proceeding to stem - cell transplantation 180 / 243 ( 74% ) 192 / 243 ( 79% ) number for whom any stem - cell product infused was not the product randomised 35 / 180 ( 19% ) 5 / 192 ( 3% ) number for whom back - up pbsc infusion was given 5 / 180 ( 3% ) 6 / 192 ( 3% ) number receiving post - stem - cell transplantation anti - gd2 antibody 36 / 180 ( 20% ) 42 / 192 ( 22% ) post - induction gfr 100 ml / min per 173 m ( normal gfr ) < 100 ml / min per 173 m ( low gfr ) unknown 163 / 194 ( 84% ) 156 / 201 ( 78% ) 31 / 194 ( 16% ) 45 / 201 ( 22% ) proportions have been calculated excluding patients with unknown values . 
all but two patients without day 1 immunocytological data had immunocytology testing on a separate stem - cell sample before stem cell - infusion for transplantation ; treating physicians chose to infuse non - immunocytology tested products in those two patients . 
percentages calculated on the basis of the number of patients who were harvested and who had a specimen of su cient quality ( 129 purged , 116 non - purged , 245 overall )  . 
one additional patient who received a transplant was retrospectively ( post - transplant ) determined by the treating institution to have had progressive disease at the end of induction . table 1 : patient characteristics vol 14 september 2013 1003 articles p = 077 p = 081 time from study enrolment ( months ) time from study enrolment ( months ) number at risk purged 243 non - purged 243 173 179 119 123 100 20 243 243 203 212 171 175 142 147 124 131 purged pbsc ( n = 180 ) non - purged pbsc ( n = 192 ) purged pbsc ( n = 180 ) non - purged pbsc ( n = 192 ) purged pbsc ( n = 243 ) non - purged pbsc ( n = 243 ) purged pbsc ( n = 243 ) non - purged pbsc ( n = 243 ) 40% ( 95% ci 3346 ) 36% ( 95% ci 3042 ) 49% ( 95% ci 4156 ) 42% ( 95% ci 3448 ) 51% ( 95% ci 4457 ) 50% ( 95% ci 4356 ) 55% ( 95% ci 4762 ) 54% ( 95% ci 4660 ) p = 033 number at risk time from transplantation ( months ) time from transplantation ( months ) purged 180 non - purged 192 126 133 180 192 152 165 133 143 113 125 106 p = 076 figure 3 : event - free survival and overall survival ( a ) event - free survival for intention - to - treat population from time of enrolment or randomisation . 
 ( c ) event - free survival for comparison of patients randomly assigned to purged treatment group versus patients randomly assigned to non - purged treatment group , from time of transplantation . 
 ( d ) overall survival for comparison of patients randomly assigned to purged treatment group versus patients randomly assigned to non - purged treatment group , from time of transplantation . the median number of cd34 cells per kg infused was signi cantly greater for non - purged versus purged pbsc ( 56 [ iqr 37107 ] vs 37 [ 2163 ] million ; p < 00001 )  . 
 patients receiving non - purged pbsc had shorter median time to neutrophil engraftment ( 11 [ iqr 1012 ] vs 12 [ 1013 ] days ; p = 0007 ) and platelet engraftment ( 19 [ 1436 ] vs 28 [ 1640 ] days ; p = 0006 ) than did those receiving purged pbsc , with no evidence of a di erence in infection rates . five patients ( three in the purged group , two in the non - purged group ) required additional pbsc infusions for delayed neutrophil engraftment ; all subsequently engrafted . 
six patients ( two in the purged group , four in the non - purged group ) with initial neutrophil engraftment received additional pbsc infusion because of secondary neutropenia or thrombocytopenia . at the end of induction , 242 ( 51% ) of 477 patients attained an overall complete response or very good partial response ( table 1 ) , 207 ( 53% ) of 388 had a complete response by i or i - meta - iodobenzylguanidine ( mibg ) scan and 349 ( 82% ) of 424 had no tumour detectable in bone marrow by standard morphology ( table 1 )  . 
70 ( 15% ) of 477 patients progressed during induction ( table 1 )  . for brevity , the summary of toxic e ects ( table 2 ) is limited to all protocol - required ( targeted ) toxic e ects and any non - haematological toxic e ects ( non - targeted ) 1004 vol 14 september 2013 articles 62% ( 95% ci 5370 ) 41% ( 95% ci 3250 ) undetectable tlda ( n = 123 ) detectable tlda ( n = 122 ) 51% ( 95% ci 4260 ) 29% ( 95% ci 2138 ) p = 00003 number at risk time from study enrolment ( months ) time from study enrolment ( months ) p = 00017 undetectable 123 detectable 122 123 122 110 109 figure 4 : event - free survival and overall survival by tlda test results ( a ) event - free survival . 
12 ( 7% ) patients in the purged group and 17 ( 9% ) of patients in the non - purged group had sinusoidal obstructive syndrome of grade 3 or higher . 
sinusoidal obstructive syndrome was reported as severe in 15 ( 4% ) patients ( 10 of 177 in the purged group , ve of 191 in the non - purged group ) , life - threatening in 13 ( 3% ) patients ( one of 177 in the purged group , 12 of 191 in the non - purged group ) , or fatal in one ( < 1% ) patient in the purged group . the 15 ( 3% ) deaths that occurred during induction were due to infection ( four in the purged group and one in the non - purged group ) , tumour bleeding ( three in the purged group and one in the non - purged group ) , tumour - related organ compromise ( one in the purged group and two in the non - purged group ) , multi - organ failure ( one death in non - purged group ) , unrelated event ( one death in the non - purged group ) , and central venous line placement ( one death in the purged group )  . 
 infectious deaths were from typhlitis ( one death in the non - purged group ) , or fungal ( two deaths in the purged group ) and viral ( two deaths in the purged group ) causes . 
despite not requiring morphologically tumour - negative bone marrow before pbsc collection , only 1% of pbsc samples had tumour detectable by immunocytology ; therefore , immunocytological testing of pbsc has been eliminated in cog studies . following the proportion of patients who achieved complete or very good partial induction response chemotherapy in this trial was 51% , similar to other groups24 , 25 compared with 875% as originally reported ( with small patient cohort at one institution ) .26 response and progressive disease rates were similar to the less intensive ccg 3891 induction , which had fewer induction deaths.2 this trial escalated carboplatin , etoposide , and melphalan doses from the ccg 3891 regimen and omitted total body radiation ( tbi ) , while maintaining a 5 - year event - free survival similar to that reported in the myeloablative chemotherapy plus isotretinoin group from ccg 3891.2 tbi was replaced with irradiation to the primary tumour site and post - induction mibg avid metastatic sites . 
 table 2 : summary of protocol - required targeted toxic e ects , and non - hematological toxic e ects that occurred in 5% of patients or more sinusoidal obstructive syndrome of grade 3 or higher occurring in roughly the same proportion of patients as with the ccg 3891 cem - tbi regimen , 2 where it led to death in 3% of patients . 
similar results were obtained in a pilot study of tandem high dose chemotherapy using cyclophosphamide and thiotepa followed by cem with pbsc rescue.12 immunomagnetic purging of pbsc did not improve outcome , possibly because of incomplete purging or due to residual tumour in patients . 
in preclinical modelling , immunomagnetic purging removed 34 logs of tumour cells from bone marrow when starting with 1020% tumour cells.16 all ve pbsc products with tumour detected by immunocytology from the sample of day 1 became undetectable after purging , which supports a purging e ect . 
the number of randomised patients achieving complete response were insu cient to resolve the issue of whether residual tumour in patients was a possible cause for the failure of purging to improve outcome . 
this postconsolidation therapy might have eliminated tumour cells infused in the stem - cell product , which could obscure an e ect of purging . low apheresis was planned after cycle two of induction to obtain adequate cd34 cell per kg yield and avoid stemcell exposure to topoisomerases to decrease secondary leukaemia risk.26 results from a previous study5 showed a very immunocytology - detectable tumour in pbsc even when bone marrow contained residual neuroblastoma at the time of pheresis.5 this result was con rmed in our current study , with only 12% of pbsc products having immunocytologydetectable tumour . incidence of we assessed tlda on an aliquot of pbsc from day 1 of leukapheresis to assess the prognostic signi cance of tlda before any manipulation of pbsc for all patients . 
 1006 vol 14 september 2013 articles panel : research in context systematic review we searched pubmed for all publications with the terms neuroblastoma , randomized , transplant , peripheral blood stem cells and purging . 
we identi ed one randomised trial23 of ex - vivo cd34 cell selected or unselected pbsc transplantation in patients with multiple myeloma in which response and progression - free survival did not di er between groups . interpretation in our trial , purging did not improve outcome in high - risk neuroblastoma patients receiving dose intensive induction and consolidation with autologous pbsc transplantation followed by isotretinoin with or without anti - gd2 antibody . 
it will be important to assess the prognostic signi cance of tlda analysis of pbsc products using a multivariable analysis with other prognostic factors . information our analysis showed a detectable signal by ve - gene tlda was associated with a worse outcome . 
we did an additional analysis of our tlda data using only th and phox2b expression to compare with other studies.68 our patients with a detectable signal with either th or phox2b also had signi cantly worse outcome compared with those patients with an undetectable signal . 
a higher number of patients had a detectable signal with the vegene than with the two - gene analysis , providing more sensitive or less speci c , or both , tumour mrna detection . 
 smaller series have shown con icting results regarding the prognostic value of minimum tumour detection in pbsc.68 data from other groups support the prognostic signi cance of qrtpcr detection of neuroblastoma mrna in bone marrow.28 , 29 an international task force is currently assessing qrtpcr methodologies to reach a consensus technology.30 multivariable analysis of signi cance of tlda compared with other prognostic factors is ongoing . 
further analyses that are still in progress include the detection of tumour mrna by ve - gene tlda in bone marrow and peripheral blood and multivariate analysis of tlda , mibg score , bone marrow morphology , and overall clinical response . implementing this for the study was designed to assess the e ect of purging in patients with high - risk neuroblastoma as de ned by the cog . 
although we measured this in a subset of patients , the purging methodology might have caused technical interference with interpretation of the tlda assay , which would prevent accurate quanti cation of the tumour mrna reduction after purging . 
 in conclusion , our results support the use of nonpurged pbsc products following myeloablative therapy of high - risk neuroblastoma . contributors sgk , rcs , kkm , mpl , dah - k , jrp , slc , jmm , cpr , and jgv were involved in the design and development of the study . 
all authors have seen and reviewed the nal manuscript draft . con icts of interest we declare that we have no con icts of interest . acknowledgments this work was supported by u10 - ca98543 cog group chairs grant , cog statistics and data center grants : u10 - ca98413 , u10 - ca37379 , u10ca30969 , and u10 - ca29139 ; r33 - ca152809 - 01 , alexs lemonade stand foundation . 
immunomagnetic bead purging of pbsc was done under a us food and drug administration ( fda ) investigational new device exemption ( ide ) bb - ide 2259 with periodic review done as required by law . 
we thank the childrens hospital of los angeles sta in the hematopoietic stem cell processing / purging laboratory ( carolyn billups , jin - hua min , maybelle sim , and robert torres ) , the immunocytology laboratory ( rich gallego , alfonso parra ) , and the tlda laboratory ( cathy wei yao liu and betty liu ) for their essential contributions , and peter wakamatsu for his statistical and database e orts . 
we also thank the cog sta , cra , nursing and pharmacy committee members for their contributions : dina willis ( cog statistics and data center ) , sally jones ( washington university school of medicine , mo , usa ) , casey hook ( university of minnesota medical center , fairview , mn , usa ) , and john t wiernikowski ( mcmaster university , on , canada ) for providing technical and pharmaceutical assistance . long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial ian smith * , john robertson * , lucy kilburn , maggie wilcox , abigail evans , chris holcombe , kieran horgan , cliona kirwan , elizabeth mallon , mark sibbering , anthony skene , raghavan vidya , maggie cheang , jane banerji , james morden , kally sidhu , andrew dodson , judith m bliss , mitch dowsett summary background preoperative and perioperative aromatase inhibitor ( poai ) therapy has the potential to improve outcomes in women with operable oestrogen receptor - positive primary breast cancer . 
the poetic trial aimed to test these two hypotheses . methods poetic was an open - label , multicentre , parallel - group , randomised , phase 3 trial ( done in 130 uk hospitals ) in which postmenopausal women aged at least 50 years with who performance status 01 and hormone receptor - positive , operable breast cancer were randomly assigned ( 2 : 1 ) to poai ( letrozole 25 mg per day orally or anastrozole 1 mg per day orally ) for 14 days before and following surgery or no poai ( control )  . 
recruitment is complete and long - term follow - up is ongoing . findings between oct 13 , 2008 , and april 16 , 2014 , 4480 women were recruited and randomly assigned to poai ( n = 2976 ) or control ( n = 1504 )  . 
 434 ( 10% ) of 4480 women had a breast cancer recurrence ( 280 [ 9% ] poai ; 154 [ 10% ] control ) , hazard ratio 092 ( 95% ci 075112 ) ; p = 040 with the proportion free from breast cancer recurrence at 5 years of 910% ( 95% ci 899920 ) for patients in the poai group and 904% ( 887919 ) in the control group . 
within the poai - treated her2 - negative subpopulation , 5 - year recurrence risk in women with low ki67b and ki672w ( lowlow ) was 43% ( 95% ci 2963 ) , 84% ( 68105 ) with high ki67b and low ki672w ( highlow ) and 215% ( 171270 ) with high ki67b and ki672w ( highhigh )  . 
within the poai - treated her2 - positive subpopulation , 5 - year recurrence risk in the lowlow group was 101% ( 95% ci 32313 ) , 77% ( 34175 ) in the highlow group , and 157% ( 101244 ) in the highhigh group . 
the most commonly reported grade 3 adverse events were hot flushes ( 20 [ 1% ] of 2801 patients in the poai group vs six [ < 1% ] of 1400 in the control group ) and musculoskeletal pain ( 29 [ 1% ] vs 13 [ 1% ] )  . 
no treatment - related deaths were reported . interpretation poai has not been shown to improve treatment outcome , but can be used without detriment to help select appropriate adjuvant therapy based on tumour ki67 . 
we carried out a pubmed search for relevant clinical studies published from jan 1 , 1989 until dec 31 , 2019 using the terms neoadjuvant endocrine , breast cancer , clinical trial , and presurgical and endocrine therapy . 
before the initiation of poetic , two small clinical neoadjuvant trials , impact and z1031 , reported that tumour ki67 24 weeks after starting preoperative endocrine treatment predicted outcome better than baseline ki67 . 
another modestly sized trial used to triage patients with 24 week ki67 > 10% to chemotherapy and reporting the long - term outcome for those less than 10% , has led to a larger ongoing trial . 
the concept of complete cell cycle arrest has been developed as an additional possible cutoff for on - treatment ki67 . added value of this study results from poetic suggest that 2 weeks preoperative endocrine therapy makes no perceptible improvement in long - term outcome , but was nevertheless a safe treatment practice . 
in patients with a high baseline ki67 value ( > 10% ) a biopsy 2 weeks after starting preoperative endocrine therapy provides additional clinical utility by predicting long - term outcomes . 
the trial documents the relationship of 2 - week ki67 with risk of recurrence for estimating whether the prognosis of individual patients is sufficiently good on endocrine therapy alone or whether additional treatment such as chemotherapy or new targeted therapies should be considered . implications of all the available evidence the data show no reason for short - term presurgical treatment to be applied for its direct therapeutic potential , but support prescribing an aromatase inhibitor for the short - term period before breast cancer surgery in oestrogen receptor - positive tumours with a high proliferation rate to derive information on early endocrine responsiveness that can be used to predict a patients 5 - year prognosis on standard adjuvant therapy . 
the clinical manoeuvres to incorporate this in the patient pathway with reliable quality assured ki67 are straightforward and the measurement of ki67 is inexpensive , potentially making this an attractive approach to estimating the prognosis of patients with early breast cancer . introduction the poetic ( peri - operative endocrine therapy individualising care ) trial was designed to address two important hypotheses in the treatment of postmenopausal women with oestrogen receptor - positive early breast cancer . the first was that short duration presurgical endocrine therapy might improve clinical outcome . 
this hypothesis was plausible because 2 weeks preoperative endocrine therapy had been shown to markedly reduce proliferation in human breast cancer as measured by ki67.1 , 2 longstanding experimental evidence had shown that the stimulatory effect of surgery on the growth of metastases in mice could be inhibited by perioperative endocrine therapy.3 , 4 any improvement in long - term outcome following short exposure to preoperative or perioperative endocrine therapy would be achieved with no additional toxicity or resource implications and be of considerable clinical importance . the second hypothesis concerned identifying which patients with hormone receptor - positive early breast cancer have a sufficiently good prognosis such that standard of care medical treatment , often comprising adjuvant endocrine therapy alone , was sufficient and which group should be considered for additional therapies . 
traditional approaches to this problem had used standard prognostic parameters including size , grade , nodal involvement , and age , often integrated into a prognostic tool ( eg , nottingham prognostic index , 5 adjuvant online , 6 nhs predict7 ) , but these merely provided the predicted probability of benefit for a patient population with given tumour and demo - graphic characteristics . 
more recently , genomic platforms have been developed aimed at providing more accurate prognostic and predictive information for the individual patient.8 , 9 however , these genomic tests are expensive , by no means universally available , and differ among themselves in terms of the information they provide.10 a simple test which predicts outcome after short duration preoperative endocrine therapy could therefore be helpful in accurately selecting appropriate treatment in the individual patient , if it incorporated an in - vivo response to aromatase inhibitor . 
a small neoadjuvant trial ( impact ) had already suggested this might be feasible : results showed that tumour ki67 after 2 weeks ( ki672w ) of endocrine treatment predicted outcome better than at baseline ( ki67b ) , remaining significant multivariable analysis , whereas ki67b did not.11 , 12 similar 1444 vol 21 november 2020 articles see online for appendix results have subsequently been reported from another small trial comparing letrozole with tamoxifen13 and from a further trial comparing anastrozole , letrozole , and exemestane with one another.14 poetic , with a much larger patient population , aimed to build on these findings to provide the definitive clinical evidence to inform future practice . methods study design and participants this open - label , multicentre , parallel group , randomised , phase 3 trial recruited participants from 130 uk hospitals ( appendix p 2527 )  . 
eligible patients were postmenopausal women ( aged at least 50 years with amenorrhoea for more than 12 months , bilateral oophorectomy or hysterectomy , or had been on hormone replacement therapy within the previous 12 months , and with folliclestimulating hormone concentrations in the postmenopausal range if aged less than 55 years ) with oestrogen receptor - positive or progesterone receptorpositive ( allred 3 , h - score 2 , or 1% of positive cells , assessed in local pathology laboratories ) , her2 - positive or her2negative ( assessed locally ) , operable primary breast cancer and no evidence of metastatic spread investigated according to local guidelines . 
if palpable , a tumour of any size was sufficient , otherwise requiring an ultrasound size of at least 15 c women required who performance status 01 and an indication for standard adjuvant endocrine therapy . 
previous endocrine therapy or chemotherapy was not allowed , nor was concurrent use of hormone replacement therapy or any other oestrogen - containing medication ( within 4 weeks of randomisation )  . 
no previous use of oestrogen implants at any time , current , continuous , long - term systemic steroid usage , or treatment with an unlicensed or investigational drug within 4 weeks of randomisation was allowed . 
patients with invasive malignancy diagnosed within the previous 5 years or any severe co - incident medical disease were ineligible ( appendix p 1 )  . patients provided written informed consent before enrolment . 
poetic was sponsored by the institute of cancer research ( icr ) and royal marsden nhs foundation trust and approved by the londonsouth east research ethics committee ( reference 08 / h1102 / 37 ) and managed and analysed by the icr clinical trials and statistics unit ( icr - ctsu ; appendix p 1 for study oversight details )  . 
the protocol is in the appendix . randomisation and masking participants were randomly allocated ( 2 : 1 ) to perioperative aromatase inhibitor ( poai ) treatment or no perioperative treatment ( control ) by computer - generated permuted block method ( variable block size six or nine ) derived centrally by icr - ctsu using its dedicated randomisation system , stratified by hospital . 
no placebo was used ; clinicians and patients were not masked to treatment allocation , but central laboratory staff were masked . ratio weighted inhibitor procedures poai was a non - steroidal aromatase standard dosage ( oral anastrozole 1 mg per day or oral letrozole 25 mg per day ) ; choice of agent was declared by each participating hospital at trial outset . 
before randomisation , all patients had excisional surgery prebooked for around 2 weeks ( minimum 10 days ) later to ensure timing of surgery was not biased by treatment allocation . 
 treatment continued without interruption until 14 days after surgery . all non - trial adjuvant therapy , laboratory investigations , and disease staging were established on clinical grounds according to standard of care local practice ( appendix p 1 )  . 
in february , 2011 , a letter to investigators , followed by an approved protocol amendment , recommended that local multidisciplinary teams gave due consideration to other factors , including pretreatment grade on diagnostic core where available , when considering use of adjuvant chemotherapy . follow - up data were submitted annually to icr - ctsu ; disease - related events , second cancers and deaths were reported on occurrence . 
adverse event data were restricted three meno pausal symptoms ( hot flushes , sweating , and musculoskeletal pain ) at baseline , surgery , and at followup 2 weeks postsurgery ( assessed using national cancer institute common terminology criteria for adverse events version 3 ) as the safety profiles of the aromatase inhibitors used were well established . 
 participants were able to withdraw from the trial at any time for any reason . formalin - fixed paraffin - embedded tissue samples were required before randomisation ( baseline ) and at surgery . 
at surgery , samples could be either core biopsies or sections cut from the routine excision . vol 21 november 2020 1445 articles tissue samples were processed , stored , and analysed for ki67 staining centrally in the ralph lauren centre for breast cancer research at the royal marsden nhs foundation trust . 
ki67 was analysed immunohistochemically in a core biopsy taken at baseline ( ki67b ) , and in either a core biopsy or the excision biopsy taken at surgery ( ki672w ) , and was estimated as the percentage of cancer cells staining positive . 
we used mib1 as the primary antibody to ki67 and detection was done with the real envision system , both from dako ( glostrup , denmark until 2016 ; now agilent technologies , didcot , uk )  . 
scoring was according to methodology including between - batch quality control procedures as described by the international ki67 in breast cancer working group party.15 analysis of 2 - week samples from the control group was restricted to a randomly selected subset since minimal change from baseline was expected.16 outcomes the primary endpoint was time to recurrence ( time from randomisation to local , regional , or distant tumour recurrence or death from breast cancer without previous notification of relapse ) with second primary cancers and intercurrent deaths censored . 
secondary clinical endpoints included relapse - free survival ( as per time to recurrence but also including deaths from any cause as events ) , time to local recurrence ( time from randomisation to first confirmed local recurrence , censoring at previous distant recurrence , second primary cancer , or death ) , time to distant recurrence ( time from randomisation to first confirmed distant recurrence or breast cancer death without previous relapse , censoring at second primary cancer or intercurrent death ) and overall survival ( time from randomisation to death from any cause )  . 
breast cancer - free survival duplicated the definition of time to recurrence , and was listed in the protocol in error . ki67 was evaluated as a biomarker in relation to its effect on predicting disease outcomes ( one of the trials two key objectives ) and as the molecular secondary endpoint to assess proliferation rate at baseline ( ki67b ) and at surgery ( ki672w ) , thus assessing the impact of poai . 
the additional molecular secondary endpoint of gene expression profile at core biopsy and at surgical excision is not reported here as data analysis is ongoing . statistical analysis the sample size assumed the proportion of patients with recurrence by 5 years would be low ( approximately 10% ) given known recurrence rates for similar populations.17 , 18 with 4350 patients it would be possible to detect a 3% improvement in time to recurrence at 5 years ( 10% to 7% recurrences ) with 91% power ( two - sided of 5% )  . 
the sample size was increased originally from 4000 to 4350 patients to allow for underestimation of the relapse rate potentially owing to patients dying from other causes before breast cancer relapse . 
this change was endorsed by the trial steering committee and independent data monitoring committee and managed via a protocol amendment approved on dec 31 , 2012 . to modified analyses relating to clinical endpoints were done according intention - to - treatremoving patients who subsequently withdrew consent for use of data . 
patients who did not have primary breast surgery as planned were censored at the date of that decision . baseline demographic details , tumour characteristics , adjuvant treatment , and ki67 data are presented with descriptive statistics . 
protocol compliance between treatment groups ( time from randomisation to surgery and number of inpatient days for surgery ) was compared using wilcoxon rank - sum tests ; differences in tumour grade at surgery were assessed using a test for trend in prespecified analyses . 
in a post - hoc exploratory analysis , following initial planned analyses on the trial data , a multivariable logistic regression model was created , using a forward stepwise approach , to determine factors affecting chemotherapy use . for survival - related endpoints , kaplan - meier curves were plotted and treatment groups compared with the log - rank test . 
 comparisons between treatment groups were made with and without adjustment for progesterone receptor status ( positive , negative , unknown ) , her2 status ( positive , negative , unknown ) , presurgical tumour grade ( g1 , g2 , and g3 ) , pathological ( continuous ) , presurgical histological type ( ductal , lobular , special type ) , nodal status ( n0 , n13 , and n4 + ) , age at randomisation ( continuous ) and vascular invasion ( yes , no )  . 
subgroup analyses were done for baseline clinical characteristics and presented using a forest plot . tumour size associations between ki67b and ki672w and time to recurrence were done separately in the poai and control groups with the principal focus being to study the ontreatment effect of poai . 
assessment of ki67 in the control group was considered of low additional value because patients were not exposed to perioperative treatment and because of the lack of association between poai and time to recurrence . 
 to explore associations between ki67 and disease outcome in the poai group , ki67 scores were dichotomised and patients divided into four groups as follows : lowlow ( ki67b and ki672w < 10% ) ; highlow ( ki67b 10% , ki672w < 10% ) ; highhigh ( ki67b and ki672w 10% ) ; and lowhigh ( ki67b < 10% , ki672w 10% )  . 
in addition to the predefined 10% ki67 dichotomisation , chosen to ensure consistency with other neoadjuvant trials , 12 , 14 other cut - points were explored using harrells c coefficient19 including that for complete cell cycle arrest ( ccca ; ki67 27%20 )  . previous analyses21 of change in ki67 in 679 control group patients with paired samples available indicated that in patients with a core - cut surgery sample the median proportional reduction was 41% ( iqr 278 to 348 ) , whereas in those with a resection sample at surgery , the median proportional reduction in ki67 between baseline and surgery was 177% ( iqr 442 to 127 ) in contrast with an earlier small pilot study.16 from these findings , it was assumed that , for a given surgical sample , change in ki67 score would be proportionally approximately 15% less if the sample was core - cut rather than resection ( eg , 10% reduction with resection sample translated to 85% for core - cut )  . 
for cases where ki672w was 0% , no adjustment was made . this manuscript describes the primary endpoint analysis , time to recurrence after a 5 - year median followup for both hypotheses ; first by randomised poai allocation and second exploring the ability of ki67 to predict disease outcome . 
for this purpose , a database snapshot was taken on aug 8 , 2017 for data presented at the san antonio breast cancer conference 2017 and updated with a second database snapshot taken on feb 6 , 2018 . 
a p value of less than 005 was deemed to be significant . this study is registered with clinicaltrials.gov , nct02338310 ; the european clinical trials database , eudract2007 - 003877 - 21 ; and isrctn63882543 . the isrctn registry , role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all of the data in the study and had final responsibility for the decision to submit for publication . results between oct 13 , 2008 , and april 16 , 2014 , 4486 patients were entered from 130 uk centres . 
six patients subsequently withdrew consent for data to be used and therefore 4480 patients ( 2976 poai , 1504 control ) were included in the modified intention - to - treat analysis ( figure 1 )  . median age at randomisation was 671 years ( iqr 615748 ) , 2536 ( 57% ) of 4480 patients had a tumour size up to 2 cm , and all but eight ( < 1% ) patients were confirmed locally to have hormone receptor - positive tumours ( table 1 )  . 
23 ( 1% ) of 4480 patients did not have surgery as planned ( 16 patients in the poai group and seven in the control group ; figure 1 )  . 
 177 ( 6% ) of 2976 patients did not have the protocol defined duration of poai ( preoperatively < 10 days or > 21 days , post operatively < 10 days )  . 
the most common reasons were 63 ( 2% ) had their surgery changed , 35 ( 1% ) had less owing to adverse events ( 16 were in the presurgical period ) , and 30 ( 1% ) had less owing to patient choice or omission . 
surgical details and postsurgery tumour characteristics were well balanced between groups with the exception of pathological tumour grade , which was higher in the control group ( p < 00001 ; table 1 )  . 
 adjuvant chemo therapy was given to 770 ( 26% ) of 2957 patients in the poai group and 460 ( 31% ) of 1493 patients in the control group ( appendix p 15 ) with multivariable analyses attributing this to differences observed in postsurgical grade ( appendix p 16 )  . 
following surgery , most ( poai 2507 [ 86% ] of 2960 patients ; control 1186 [ 81% ] of 1497 patients ) women were prescribed aromatase inhibitor monotherapy ( appendix p 17 )  . with 629 months median follow - up ( iqr 581741 ) , 434 ( 10% ) of 4480 women had a breast cancer recurrence ( poai 280 [ 9% ] of 2976 patients , control 154 [ 10% ] of 1504 patients ; table 2 ) with no significant difference observed between the treatment groups ( hr 092 , 95% ci 075112 ; p = 040 , adjusted hr 096 , 077119 ; p = 070 ; figure 2a ) with the proportion free from breast cancer recurrence at 5 years of 910% ( 899920 ) in the poai group and 904% ( 887919 ) in the control group . 
 likewise , no significant differences between treatment groups were observed for relapse - free survival , time to local recurrence , and time to distant recurrence ( table 3 )  . 
 second breast cancer primaries developed in 26 ( < 1% ) of 2976 women in the poai group compared with 24 ( 2% ) of 1504 in the control group . 
5 - year overall survival was 889% ( 95% ci 877901 ) in the poai group versus 889% ( 872905 ) in the control group ( unadjusted hr 094 , 95% ci 079112 ; p = 050 , adjusted hr 091 , 075110 ; p = 033 ; figure 2b )  . selected menopausal symptoms were assessed in 4201 ( 94% ) of 4480 women , with higher symptom rates observed for poai ( appendix p 18 )  . 
the most commonly reported grade 3 adverse events were hot flushes ( 20 [ 1% ] of 2801 patients in the poai group vs six [ < 1% ] of 1400 in the control group ) and musculoskeletal pain ( 29 [ 1% ] vs 13 [ 1% ] )  . 
the most 1448 vol 21 november 2020 articles common were pulmonary embolism musculoskeletal pain ( n = 3 )  . ( n = 3 ) and 3913 ( 87% ) of 4480 participants had ki67b data available . 
 2528 ( 85% ) of 2976 patients in the poai group and 678 ( 45% ) of 1504 in the control group had paired ki67b and ki672w data available ( figure 1 )  . 
in 2316 ( 72% ) of 3206 participants with paired ki67 data , the surgical sample was a resection ( 1834 [ 73% ] of 2528 patients in the poai group ; 474 [ 70% ] of 678 patients in the control group ) or the surgical sample type was unknown ( six in the poai group and two in the control group ) and the ki672w scores for these resections and unknown surgical sample types were corrected as described . 
688 ( 27% ) of 2528 poai and 202 ( 30% ) of 678 control patients surgical sample type was core - cut biopsy . the median ki67b score in the 3913 of 4480 patients with a sample available was 152% ( iqr 86260 ; poai 153% [ 85264 ] ; control : 149% [ 86251 ] )  . 
ki67b values were different between her2 - negative and her2positive tumours ( median 143% [ iqr 82246 ] in her2 - negative tumours , median 266% [ 170374 ] in her2 - positive tumours ; p < 00001 )  . 
women whose ki672w remained high ( highhigh group ) were significantly more likely to have a recurrence than those whose ki672w had dropped below 10% ( highlow group ; unadjusted hr 259 , 95% ci 193347 ; p < 00001 , adjusted hr 210 , 148298 ; p < 00001 ; figure 3a )  . 
within the poai - treated her2negative subpopulation , 5 - year recurrence risk in women with low ki67b and ki672w ( lowlow ) was 43% ( 95% ci 2963 ) , 84% ( 68105 ) with high ki67b and low ki672w ( highlow ) and 215% ( 171270 ) with high ki67b and ki672w ( highhigh )  . 
within the poai - treated her2positive subpopulation , 5 - year recurrence risk in the low low group was 101% ( 95% ci 32313 ) , 77% ( 34175 ) in the high - low group , and 157% ( 101244 ) in the highhigh group . 
adding a high versus low classification at 2 weeks segregated groups in relation to their baseline ki67 ( appendix p 21 )  . the her2 - negative poai - treated subpopulation posthoc exploratory analyses relating to the combined effects of age and chemotherapy use suggested that in patients with ki67b of at least 10% , who did not receive adjuvant chemotherapy , the residual ki672w ( high or low ) conferred demographics at randomisation and tumour characteristics from the diagnostic core surgery details and tumour characteristics from surgery perioperative aromatase inhibitor group ( n = 2976 ) control group ( n = 1504 ) perioperative aromatase inhibitor group ( n = 2960 ) control group ( n = 1497 ) ( continued from previous page ) definitive breast surgery mastectomy conservative surgery definitive axillary surgery sentinal lymph node biopsy nodal status missing clearance sampling missing n13 missing missing vascular invasion not reported missing multi - focal disease 1051 ( 36% ) 1902 ( 64% ) 7 ( < 1% ) 503 ( 34% ) 992 ( 66% ) 2 ( < 1% ) 2911 ( 98% ) 1470 ( 98% ) 916 ( 31% ) 287 ( 10% ) 1708 ( 58% ) 42 ( 1% ) 7 ( < 1% ) 1815 ( 61% ) 801 ( 27% ) 334 ( 11% ) 10 ( < 1% ) 813 ( 27% ) 1990 ( 67% ) 143 ( 5% ) 14 ( < 1% ) 468 ( 31% ) 150 ( 10% ) 852 ( 57% ) 25 ( 2% ) 2 ( < 1% ) 892 ( 60% ) 434 ( 29% ) 165 ( 11% ) 6 ( < 1% ) 445 ( 30% ) 981 ( 66% ) 63 ( 4% ) 8 ( 1% ) 381 ( 13% ) 223 ( 15% ) 2563 ( 87% ) 1266 ( 85% ) 16 ( 1% ) 8 ( 1% ) data are n ( % ) and median ( iqr )  . 
 * one patient ( perioperative aromatase inhibitor ) with hormone receptor status unknown was her2 negative ; the remaining two patients ( control ) with hormone receptor status unknown also had her2 status unknown . 
special types from surgery specimen include mucinous , papillary , tubular , endocrine cell carcinoma , pure special type , metaplastic carcinoma clear cell , and basaloid , tubular , and cribiform carcinoma . 
patients are eligible if they have either a palpable tumour ( clinical examination ) of any size or a tumour with an ultrasound size of 15 c618 patients had tumour size < 15 cm , of which 607 had a tumour confirmed as palpable . table 1 : baseline characteristics a differential effect on prognosis as assessed by time to recurrence for both those aged less than 70 years and aged at least 70 years ( appendix pp 49 )  . 
numbers were too small to fully define effects for the corresponding group ( ie , ki67b 10% ) who did receive chemotherapy . in patients with her2 - negative breast cancer in the control group , 56 time to recurrence events were reported in the 597 of 678 patients for whom ki672w was available . 
if more than one first event was reported on the same date , it was included in the row here according to the following order of priority : distant recurrence , local recurrence , breast second primary cancer , non - breast second primary cancer , and intercurrent death . 
 included 25 patients ( 18 perioperative aromatase inhibitor , seven in the control group ) with unknown cause of death and no previous event ; one patient had a second primary cancer before unknown cause of death and was not included here . 
 other causes in the perioperative aromatase inhibitor group ( n = 13 ) were accident ( n = 2 ) , acute kidney injury , alzheimers disease , ascending aortic aneurysm , haematemesis secondary to gastric ulcer , hepatic cirrhosis , multiorgan failure , myelofibrosis , old age with vascular deterioration and chronic kidney disease , portal hypertension , a fall , ascites , evidence of cirrhosis , postoperative complications relating to pituitary tumour operation , and renal failure ; other causes in the control group ( n = 6 ) were complications post laparotomy , dementia , diabetes , meningioma , subdural haematoma , and suicide . table 2 : disease - related first events and deaths a post - hoc sensitivity analysis in the her2 - negative subgroup combining the baseline data for poai and control gave a 5 - year recurrence risk of 47% ( 95% ci 3563 ) for low ki67b and 115% ( 95% ci 101131 ) for high ki67b ( appendix p 24 )  . prespecified exploratory analysis in the her2 - negative subgroup suggested an optimal cut - point around 1520% for ki67b and around 68% for ki672w and that using the ccca threshold for ki672w had prognostic discrimination ( appendix pp 1113 )  . in patients with hormone receptor - positive , her2positive breast cancer in the poai group ( 273 [ 10% ] of 2528 patients ) , 33 time to recurrence events were reported . 
143 women in the ki67 highhigh group had a recurrence compared with 94 in the highlow group , although the difference was not significant ( unadjusted hr 208 , 95% ci 088490 ; p = 0093 , adjusted hr 183 , 071473 ; p = 021 ; figure 3b )  . 
similar to the her2negative group , absolute risk of recurrence at 1 , 3 , and 5 years was higher in the high - high group than in the highlow group ( appendix p 23 )  . 
5 - year recurrence risk in the low - low group was 101% ( 95% ci 32313 ) , 77% ( 34175 ) in the highlow group , and 157% ( 101244 ) in the highhigh group . 
in the 70 women with her2 - positive breast cancer in the control group , nine time to recurrence events were reported . discussion poetic is , to our knowledge , the largest trial of its kind to assess the potential of poai therapy in patients with postmenopausal , hormone receptor - positive early breast cancer and it did not show any significant long - term improvement in disease outcomes with this approach . 
 this was despite preclinical experimental evidence in a mouse model suggesting the contrary.3 , 4 a smaller phase 3 clinical trial , which reported after poetic was initiated , randomly assigned operable breast cancer patients ( n = 976 , 50% hormone receptor - positive , 45% hormone receptor - negative , and 5% hormone receptor unknown ) to surgery or an intramuscular injection of depot hydroxyprogesterone 500 mg 514 days before surgery ; no significant benefit was observed in the overall population ( hr 087 , 95% ci 068109 ; p = 023 ) , but the results suggested a hypothesis - generating potential disease - free survival in node - positive subgroups ( hr 072 , 054097 ; p = 002 ) .22 in contrast , consistent with the overall finding , poetic showed no suggestion of long - term outcome improvement with poai overall or in the node - positive subgroup . improvement in poetic , the frequency of chemotherapy was slightly lower in patients in the poai group than in those in the control group . 
multivariable regression supported the suggestion that this was probably because of multidisciplinary teams being influenced by pathological tumour grade , which was on average lower in the patients in the poai group . 
this absolute difference was small however ( 5% ) , and since the overall event rate was less than 20% would have had an imperceptible effect on outcome comparisons . on a pragmatic note , it is common practice to start some patients on preoperative endocrine therapy if there has to be a significant delay in surgery for any reason . 
 despite not showing any statistical evidence of clinical benefit , our results provide reassurance that there is no detriment to this practice . the second aim of this trial was to explore whether the measurement of tumour ki67 2 weeks after starting treatment could predict disease outcome better than baseline ki67 alone , thus providing the basis of a simple and inexpensive test to personalise adjuvant treatment in patients with hormone receptor - positive , her2negative breast cancer . 
previously , impact had shown 1450 vol 21 november 2020 articles a control perioperative aromatase inhibitor unadjusted hazard ratio 092 ( 95% ci 075112 ) ; p = 040 number at risk ( number censored ) perioperative aromatase inhibitor control 2976 ( 57 ) 1504 ( 21 ) 2871 ( 93 ) 1451 ( 42 ) 2793 ( 153 ) 1404 ( 71 ) 2681 ( 400 ) 1349 ( 194 ) 2374 ( 1021 ) 1197 ( 509 ) 1711 ( 1833 ) 862 ( 909 ) 875 ( 2382 ) 450 ( 1202 ) 317 ( ) 150 ( ) unadjusted hazard ratio 094 ( 95% ci 079112 ) ; p = 050 time from randomisation ( years ) number at risk ( number censored ) perioperative aromatase inhibitor control 2976 ( 38 ) 1504 ( 11 ) 2914 ( 45 ) 1474 ( 17 ) 2850 ( 75 ) 1442 ( 23 ) 2756 ( 294 ) 1393 ( 136 ) 2443 ( 904 ) 1237 ( 452 ) 1768 ( 1728 ) 893 ( 859 ) 905 ( 2290 ) 466 ( 1153 ) 323 ( ) 155 ( ) figure 2 : kaplan - meier survival curve by randomised treatment group for time to recurrence ( a ) and overall survival ( b ) in part a test for proportionality , p = 058 . 
in part b test for proportionality , p = 082 . that 2 - week on - treatment ki67 predicted outcome better than baseline and , unlike baseline , was significant in multivariable analysis.12 poetic has provided evidence for the clinical validity of on - treatment aromatase inhibitor ki672w in addition to ki67b to predict those with high residual risk of recurrence in spite of standard - ofcare therapy . 
our results provide an early indication of endocrine sensitivity or resistance including for the large number of patients who are not routinely considered for adjuvant chemotherapy . separate clearly defined adjuvant treatment pathways for her2 - positive and her2 - negative breast cancers now exist and we therefore analysed these groups separately when considering prognostic risk . 
focus for exploratory analysis was therefore on the her2 - negative subgroup , which comprised approximately 90% of the poetic population . number of events unadjusted hazard ratio adjusted hazard ratio 5 - year survival estimate perioperative aromatase inhibitor group control group 385 ( 13% ) 207 ( 14% ) 41 ( 1% ) 24 ( 2% ) 262 ( 9% ) 147 ( 10% ) relapse - free survival time to local recurrence time to distant recurrence 094 ( 079111 ) ; 047 086 ( 052143 ) ; 057 090 ( 073110 ) ; 030 095 ( 079114 ) ; 059 092 ( 054156 ) ; 075 094 ( 075118 ) ; 059 perioperative aromatase inhibitor group control group 879% ( 866891 ) 876% ( 857892 ) 986% ( 981990 ) 985% ( 976990 ) 917% ( 905926 ) 909% ( 892923 ) data are n ( % ) , hazard ratio ( 95% ci ) ; p value , and % ( 95% ci )  . 
models adjusted for progesterone receptor status ( positive , negative , unknown ) , her2 status ( positive , negative , unknown ) , presurgical tumour grade ( g1 , g2 , and g3 ) , pathological tumour size ( continuous ) , presurgical histological type ( ductal , lobular , special type ) , nodal status ( n0 , n13 , and n4 + ) , age at randomisation ( continuous ) , and vascular invasion ( yes , no )  . 
28 patients with hormone receptor - positive breast cancer and her2 - negative breast cancer and four patients with hormone receptor - positive and her2 - positive breast cancer in the low - high group were omitted from the figure . previously , it had been shown that patients with a low ki67b have a better prognosis than those with a high ki67b value.23 poetic confirmed this in a larger prospective population , dichotomising ki67b at 10% with 5 - year recurrence risk in her2 - negative patients in the poai group of 44% for low ki67b and 118% for high ki67b . 
to our knowledge , this is the first large published dataset that makes use of the ki67 scoring methodology recommended by the international ki67 in breast cancer working group ; the strong association of ki67 at baseline with prognosis served as a clinical validation of that methodology.15 patients whose ki67b was low did well on standard of care , with approximately 85% of those receiving endocrine therapy alone . 
but irrespective of adjuvant treatment , it is reasonable to conclude that ki672w did not add significant prognostic or predictive information in this subgroup . in contrast , for patients whose tumours had a high baseline ki67 in the poai group , 73% had a low ki672w 2 weeks after starting treatment ; those patients had a better prognosis at 5 years than those who continued to have a high ki672w ( 84% vs 215% 5 - year recurrence risk )  . 
older age has already been shown to be an independent prognostic factor in breast cancer24 and poetic patients aged at least 70 years had poorer outcomes than those aged below 70 years . 
since a substantial minority ( 26% ) of poai patients had adjuvant chemotherapy , this could be a potential confounding factor in the interpretation of ki672w in relation to prognosis and prediction of the value of endocrine therapy alone . 
in the corresponding groups who received chemotherapy , numbers were insufficient to determine a prognostic ki67 effect or to define a plausible beneficial chemotherapy effect . in the two - thirds of patients below the age of 70 years not receiving chemotherapy , the overall outcome in terms of recurrence risk was better , probably reflecting the choice of omitting chemotherapy for better prognosis patients . 
but the key point was that in this population of patients non - confounded by chemotherapy , 21% with high ki67b remained high at surgery ( highhigh ) and those had 112% 5 - year recurrence risk ( arguably meriting chemotherapy in addition ) , compared with the lowlow groups in which recurrence by 5 years was only 16% and the highlow group in which recurrence by 5 years was only 29% ( indicating that additional chemotherapy would be of no clinically relevant benefit )  . 
 this exploratory outcome must be interpreted with caution but further supports the prognostic value of measuring ki67 at 2 weeks . similar findings were observed for patients aged at least 70 years . 
in those 1452 vol 21 november 2020 articles aged at least 70 years who did not receive chemotherapy , there was again a large difference in outcome between the highlow and highhigh groups ( 5 - year recurrence risk 123% vs 345% ) , again supporting the discriminatory power of measuring ki67 at 2 weeks , even though the absolute risks were greater . the prespecified ki672w 10% cut - point was chosen for consistency with ongoing clinical trials ( alternate [ nct01953588 ] ; adapt [ nct01779206 ] )  . 
the relationship of ki672w with recurrence risk is continuous and as illustrated by our analysis by means of ccca , other cutpoints might be selected if appropriate for a specific use ( eg , assessing the value of well - tolerated additional treatment )  . in conclusion , in poetic , giving perioperative endocrine therapy with an aromatase inhibitor had no significant effect on long - term outcome . 
first , we believe that we have identified a subgroup with a low baseline ki67 who have a sufficiently good prognosis that the majority will do well on standard endocrine therapy alone ( except perhaps for a minority as dictated by other clinicalpathological factors ) and who do not require a repeat 2 - week biopsy . 
second , giving poai to the subgroup with high baseline ki67 can differentiate two groups of patients according to their 2 - week ki67 value : those who convert to a low ki67 might not need anything beyond adjuvant endocrine therapy ( taking consideration of other clinical - pathological factors ) , whereas those with a high ki67 that has remained high , should be considered for further adjuvant treatments and trials . 
there are , of course , now several commercially available genomic platforms developed to provide the same kind of prognostic and predictive information for the individual patient.8 , 9 but these tests are expensive , they often involve central testing of tissue , which has to be sent long distances with inevitable time delay , and results can differ between the platforms . 
all authors reviewed the manuscript before submission . declaration of interests md reports grants from cancer research uk , during the conduct of the study ; and personal fees from radius , roche , myriad , orion , g1 therapeutics , nanostring , abbvie , h3 biomedicine , lilly , and the icr rewards for inventors scheme , outside the submitted work . 
 jmb reports grants from cancer research uk , during the conduct of the study ; grants from medivation ; grants and non - financial support from astrazeneca , merck sharp & dohme , puma biotechnology , clovis oncology , pfizer , janssen - cilag , novartis , and roche , outside the submitted work . 
all other authors declare no competing interests . data sharing de - identified data will be made available to other researchers on request , subject to approval of a formal data access request in accordance with the icr - ctsu data and sample access policy . 
trial data is collected , managed , stored , shared , and archived according to icr - ctsu standard operating procedures in order to ensure the enduring quality , integrity , and utility of the data . 
formal requests for data sharing are considered in line with the institute of cancer research clinical trials and statistics unit ( icr - ctsu ) procedures with due regard given to funder and sponsor guidelines . 
data recipients are required to enter a formal data sharing agreement which describes the conditions for release and requirements for data transfer , storage , archiving , publication and intellectual property . 
additional documents might be shared if approved by the tmg and trial steering committee ( eg , statistical analysis plan and informed consent form )  . acknowledgments poetic is co - sponsored by the institute of cancer research and the royal marsden nhs foundation trust . 
we are grateful for the support from the national institute for health research ( nihr ) clinical research network and for the study grant from cancer research uk ( cruk / 07 / 015 grant reference a8671 )  . 
the poetic trial represents independent research supported by the national institute for health research biomedical research centre at the royal marsden nhs foundation trust and the institute of cancer research , london . 
we thank all the patients and their families who participated in this study , all staff involved at the 132 participating hospitals , the staff involved in the trial at icr - ctsu , ralph lauren centre for breast cancer research at the royal marsden nhs foundation trust , and the centre for molecular pathology at the institute of cancer research . 
finally , we thank the past and present colleagues on the poetic trial management group , and the poetic independent data monitoring committee and trial steering committee . uk cancer care threatened by government incompetence on oct 6 , 2020 , in response to questions in parliament regarding cancer outcomes during covid - 19 , the uk health secretary , matt hancock , stated the best way to keep cancer services running is to suppress [ coronavirus ]  . 
cancer care cannot be put on hold ; cancer care during the pandemic should not be beyond the capacity of the uks ostensibly world - class health system ; and patients with suspected or prevalent cancer must not be denied timely access to care . the devastating effect of the first uk lockdown earlier this year on cancer screening , diagnosis , treatment , and supportive care has been widely documented . 
so far , an estimated 3 million people have missed cancer screenings , and between april and august , 2020 , suspected cancer referrals were down 350 000 compared with the same period in 2019 . 
delays in diagnosis and referral will indisputably lead to excess early cancer mortality ; although exact numbers are uncertain , upwards of 60 000 life - years could be lost during the next 510 years . 
early in the pandemic , most clinical cancer trials in the uk were halted , and although these are now starting to reopen , the impact on both novel treatment development and individual patient outcomes is incalculable . 
following loosening of the initial lockdown restrictions , referrals and treatment have returned to near - normal levels , but , with a second wave of covid - 19 looming , hancock admits that the ability of the national health service ( nhs ) to see patients for reasons other than covid - 19 is now once again at risk . 
it is incredulous that 9 months after the first case of covid - 19 in the uk , and despite ample data regarding the effect of covid - 19 policies on cancer care services , the uk governments solution during the impending second wave of covid - 19 over the winter , is to again reduce or pause cancer care , rather than to find answers to maintain services . 
other countries have managed to continue with provision of cancer care despite covid - 19 and will not have the devastating legacy the uk will endure in the years to come . 
for example , france has successfully handled workforce issues by drawing on a voluntary reserve force of medical professionals , and several countries , including australia and germany , have responded to localised outbreaks by coordinating the redistribution of medical resources . 
most notably , in new zealand , cancer treatment ( surgery , medical oncology , radiation oncology , and haematology ) continued during the covid - 19 lockdown and is still being provided at pre - covid - 19 levels . 
unfortunately , after years of austerity , the nhs entered the pandemic with fewer doctors , nurses , and capital assets than did health systems in many other highincome countries , which has severely hampered its ability to deal with the pandemic . fortunately , despite matt hancock and the uk governments incompetence , the nhs has been working hard under its own guidance to prepare differently for the second wave of covid - 19 . 
cancer research uk has set out additional recommendations for preserving high - quality cancer care , including ways to increase the workforce , harness new technologies , and other long - term ambitions for improvement . 
it is the governments responsibility to encourage and support nhs efforts , not undermine them with threats . governmental failures have contributed to a second wave of covid - 19failures in testing and track and trace strategy and implementation , inadequate attention to the vulnerability of care homes , insufficient guidance and support for school exams and reopenings , unequal application of lockdown measures , and high - profile flouting of safety rules have eroded public trust . 
hancock , and by extension , the uk government , have set up a false choice between covid - 19 and other life - threatening diseases ; the way forward must be to find an equitable and humane way to address both . 
 the lancet oncology published online october 22 , 2020 s1470 - 2045 ( 20 ) 30638 - 0 for matt hancocks statement on oct 6 , 2020 see hansard.parliament.uk / commons / 2020 - 10 - 06 / debates / 81312f07 - 53f3 - 4861a50e - 49e65505d150 / canceroutcomes for more on cancer screening during the covid - 19 pandemic see cancerresearchuk . org / 2020 / 09 / 11 / whatshappened - to - cancer - servicesduring - the - covid - 19 - pandemic / for more on cancer diagnosis during covid - 19 see articles lancet oncol 2020 ; 21 : 102334 for more on cancer referrals during covid - 19 see articles lancet oncol 2020 ; 21 : 103544 for more on the effect of an impending second wave of covid - 19 on the nhs see health - 54463441 for more on health services in england during the pandemic see org.uk / files / 2020 - 07 / resuminghealth - services - web.pdf for more on cancer treatment during a second wave of covid - 19 see theguardian.com / society / 2020 / sep / 21 / nhs - england - covid - freehospitals - second - wave - cancer for cancer research uk recommendations see scienceblog.cancerresearchuk. org / 2020 / 06 / 22 / getting - cancerservices - back - on - track - duringthe - covid - 19 - pandemic / for more on matt hancocks statement on oct 15 , 2020 see commons / 2020 - 10 - 15 / debates / 65300455 - 4bf7 - 4e159eba - 5dfa1c639d20 / covid - 19 vol 21 november 2020 1387 editorial correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
 maintaining and improving cancer care interestingly , just before the covid - 19 pandemic , in addition to its changes to home care , the ontario government was in the process of consolidating the health - care system under one large superagency , which would eventually eliminate cancer care ontario ( cco ) , the agency responsible for cancer services . 
 many factors affect good cancer care , but important that diagnosis and treatment delays are avoided during times of stress , such as pandemics ; that quality home care is invested in ; and that leading cancer care and research organisations are maintained . sherene chen - see cancer never waits , but during the covid - 19 pandemic , its diagnosis and treatment had to . 
according to a survey com missioned by the canadian cancer survivor network ( ccsn ) , many cancer diagnostic tests and treatments were cancelled or postponed because of covid - 19 . 
because delays in cancer care can lead to progression of cancer , it was disheartening to think we might face a public health crisis down the road when more patients might develop into late - stage cancer [ because of delays to their treatment ] , says jackie manthorn ( ccsn , ottawa , on , canada )  . despite overall satisfaction with virtual visits , 71% of patients and caregivers in the survey remained concerned about receiving in - person care . 
they expressed concerns with their ability to receive hospital or emergency room care if needed , to get cancer - related tests , to see their doctor for follow - ups , to get help for new symptoms or sideeffects from treatment , and to receive cancer treatment in a timely fashion . 
some patients were not having their scheduled tests before an appointment , not having their physical exam when it was needed , not having tests done to see if cancer cells were growing , and having a procedure done with no follow up afterwards , says manthorn . 
 caregivers were also worried about their loved one being alone in the hospital in case they were given bad news or needed more treatment , and could not understand the information . the results of this survey were not surprising , says keith stewart ( princess margaret cancer centre , toronto , on , canada )  . 
 i was surprised though that caregivers were more concerned than patients , but it is worth reminding [ that ] there are people undergoing considerable emotional stress . to save lives , cancer diagnosis and care must continue during any public health crisis , says manthorn . 
 unless the system was completely overwhelmed , there is no reason why we could not continue with cancer care . importance of home care addressing delays is crucial , but manthorn also points out the importance of home care for some cancer patients after surgery , partially because many people feel more comfortable at home , especially during the pandemic , rather than at rehab or in a nursing home . 
the ontario government has been trying to privatise the provision of home health vol 21 august 2020 e374 news comment published online may 12 , 2015 s1470 - 2045 ( 15 ) 70201 - 9 see articles page 656 we declare no competing interests . evans mk , longo dl . 
n engl j med 2014 ; 371 : 497506 . cybulski c , kluniak w , huzarski t , et al , and the polish hereditary breast cancer consortiuclinical outcomes in women with breast cancer and a palb2 mutation : a prospective cohort analysis . 
in a meta - analysis that included 2447 patients with breast cancer treated in a rst - line setting , bevacizumab slightly improved progression - free survival ( hr 064 , 95% ci 057071 ; median 92 months vs 67 months ) and did not improve overall survival ( hr 097 , 95% ci 086108 ; 267 months vs 264 months ) .1 guidelines recommend this drug as an option only in selected cases because of the slight improvement in progression - free survival , lack of bene t in overall lack of predictive biomarkers , survival , high cost , and associated toxicities.2 more recently , a phase 3 randomised trial reported that bevacizumab did not improve outcome as adjuvant treatment in patients with triple - negative breast cancer.3 it is important to emphasise that this trial was done in patients with intermediate risk of relapse , and the e ect of bevacizumab in high - risk patients is still unknown . 
 overall , although the drug is still widely used in several countries , the enthusiasm associated with bevacizumab has dramatically decreased , and some countries have either restricted or stopped its use . 
 in the lancet oncology , helena earl and colleagues4 report pathological complete response results of a phase 3 randomised trial assessing the e cacy of bevacizumab in the neoadjuvant setting . 
a signi cantly greater proportion of patients treated with bevacizumab and chemotherapy achieved a pathological complete response ( 22% [ 95% ci 1827 ] ) compared with those treated with chemotherapy alone ( 17% [ 1321 ] )  . 
the magnitude of improvement was numerically more pronounced in patients with oestrogen receptor ( er ) negative ( 45% [ 95% ci 3655 ] vs 31% [ 2340 ] ) or er poor ( 51% [ 3468 ] vs 30% [ 1647 ] ) breast cancer , as opposed to those with er strongly positive breast cancer ( 6% [ 310 ] vs 7% [ 411 ] )  . 
nevertheless , this wave of randomised trials in the neoadjuvant setting , pending cooperation between the groups and support 600 vol 16 june 2015 comment from funding agencies , will certainly open a new era for the development of bevacizumab in breast cancer . 
a meta - analysis will allow better understanding about which population derives more bene t , which chemotherapy backbone is the most appropriate , and will assess the e ect of bevacizumab on outcome ( disease - free survival and overall survival ) in a large population of patients presenting with highrisk breast cancers . 
to what extent an improvement in pathological complete response translates into disease - free survival and overall survival bene t is still controversial in breast cancer , and this meta - analysis , based on a large number of patients , will certainly help . 
 several molecular predictors have already been proposed , including vascular cell adhesion molecule 1 , intercellular adhesion molecule 1 , e - selectin , and circulating vegfr - 2.8 because most trials were done in a metastatic setting , no opportunity existed until now to test tissue - based biomarkers in samples obtained at baseline before therapy . 
for example , bevacizumab has been reported to modulate the immune system through dendritic cells and regulatory t - cell functions , and could facilitate t - cell homing.9 if molecular analyses from neoadjuvant studies con rm an e ect of bevacizumab on the immune system , they could generate a rationale for immunogenic chemotherapy , anti - pd1 agents , and bevacizumab . 
 triple combination therapy of overall , the study by earl and colleagues , 4 consistent with previous trials , suggests that bevacizumab could improve pathological complete response in patients with breast cancer . 
these four trials could constitute the starting point of a new era for bevacizumab in breast oncology and could help to de ne which patients are more likely to bene t from bevacizumab , and which drug should optimally be combined with it . * fabrice andre , elise deluche , herve bonnefoi department of medical oncology , gustave roussy , villejuif , france ( fa , ed ) ; inserm unit u981 and universit paris sud , facult de medecine kremlin bicetre , kremlin bicetre , france ( fa ) ; and department of medical oncology , institut bergonie , bordeaux , france ( hb ) fandre@igr.fr fa reports grants from novartis , astrazeneca , and eisai , outside the submitted work . 
e cacy of neoadjuvant bevacizumab added to docetaxel followed by uorouracil , epirubicin , and cyclophosphamide , for women with her2 - negative early breast cancer ( artemis ) : an open - label , randomised , phase 3 trial . 
impact of the addition of carboplatin and / or bevacizumab to neoadjuvant once - per - week paclitaxel followed by dose - dense doxorubicin and cyclophosphamide on pathologic complete response rates in stage ii to iii triple - negative breast cancer : calgb 40603 ( alliance )  . 
parenthood in female survivors of hodgkins lymphoma in the lancet oncology , jurgen brmswig and colleagues1 report pregnancy outcomes in 467 female long - term survivors of hodgkins lymphoma who were younger than 18 years at diagnosis and treated in one of ve concurrent clinical trials in germany and austria between 1978 and 1995 . 
they have shown that the chance of these patients becoming a parent is similar to that in the female german population aged 1639 years , and not signi cantly a ected by potentially gonadotoxic see articles page 667 vol 16 june 2015 correction to lancet oncol 2019 ; 20 : 40819 correction to lancet oncol 2019 ; 20 : 125262 smith m , parker c , saad f , et al . 
 addition of radium - 223 to abiraterone acetate and prednisone or prednisolone in patients with castration - resistant prostate cancer and bone metastases ( era 223 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
this correction has been made to the online version as of sept 30 , 2019 . ieo and correction to lancet oncol 2019 ; 20 : 117182 nen nr , reisel d , leimbach a , et al . 
this correction has been made to the online version as of sept 30 , 2019 . correction to lancet oncol 2019 ; 20 : 137085 motzer rj , rini bi , mcdermott df , et al . 
nivolumab plus ipilimumab versus sunitinib in first - line treatment for advanced renal cell carcinoma : extended follow - up of efficacy and safety results from a randomised , controlled , phase 3 trial . 
lancet oncol 2019 ; 20 : 137085in figures 2 and 3 of this article , median and 95% ci data should have appeared in panel c and not in panel a . 
this correction has been made to the online version as of aug 21 , 2019 . published online august 21 , 2019 s1470 - 2045 ( 19 ) 30542 - x vol 20 october 2019 e559 corrections corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
minimal data are available on the effect of maintenance lenalidomide in more aggressive disease states , such as patients with cytogenetic high - risk disease or patients ineligible for transplantation . 
we aimed to assess lenalidomide maintenance versus observation in patients with newly diagnosed multiple myeloma , including cytogenetic risk and transplantation status subgroup analyses . methods the myeloma xi trial was an open - label , randomised , phase 3 , adaptive design trial with three randomisation stages done at 110 national health service hospitals in england , wales , and scotland . 
there were three potential randomisations in the study : induction treatment ( allocation by transplantation eligibility status ) ; intensification treatment ( allocation by response to induction therapy ) ; and maintenance treatment . 
eligible patients for maintenance randomisation were aged 18 years or older and had symptomatic or non - secretory multiple myeloma , had completed their assigned induction therapy as per protocol and had achieved at least a minimal response to protocol treatment , including lenalidomide . 
patients were randomly assigned ( 1 : 1 from jan 13 , 2011 , to jun 27 , 2013 , and 2 : 1 from jun 28 , 2013 , to aug 11 , 2017 ) to lenalidomide maintenance ( 10 mg orally on days 121 of a 28 - day cycle ) or observation , and stratified by allocated induction and intensification treatment , and centre . 
this study is registered with the isrctn registry , number isrctn49407852 , and clinicaltrialsregister.eu , number 2009 - 010956 - 93 , and has completed recruitment . findings between jan 13 , 2011 , and aug 11 , 2017 , 1917 patients were accrued to the maintenance treatment randomisation of the trial . 
 after a median follow - up of 31 months ( iqr 1850 ) , median progression - free survival was 39 months ( 95% ci 3642 ) with lenalidomide and 20 months ( 1822 ) with observation ( hazard ratio [ hr ] 046 [ 95% ci 041053 ] ; p < 00001 ) , and 3 - year overall survival was 786% ( 95% cl 756816 ) in the lenalidomide group and 758% ( 724792 ) in the observation group ( hr 087 [ 95% ci 073105 ] ; p = 015 )  . 
on prespecified subgroup analyses by transplantation status , 3 - year overall survival in transplantation - eligible patients was 875% ( 95% cl 843907 ) in the lenalidomide group and 802% ( 760844 ) in the observation group ( hr 069 [ 95% ci 052093 ] ; p = 0014 ) , and in transplantationineligible patients it was 668% ( 616721 ) in the lenalidomide group and 698% ( 644752 ) in the observation group ( 102 [ 080129 ] ; p = 088 )  . 
by cytogenetic risk group , in standard - risk patients , 3 - year overall survival was 864% ( 95% ci 800909 ) in the lenalidomide group compared with 813% ( 742867 ) in the observation group , and in high - risk patients , it was 74.9% ( 658819 ) in the lenalidomide group compared with 637% ( 528727 ) in the observation group ; and in ultra - high - risk patients it was 629% ( 460758 ) compared with 435% ( 222631 )  . 
the most common grade 3 or 4 adverse events for patients taking lenalidomide were haematological , including neutropenia ( 362 [ 33% ] patients ) , thrombocytopenia ( 72 [ 7% ] patients ) , and anaemia ( 42 [ 4% ] patients )  . 
 460 deaths occurred during maintenance treatment , 234 ( 21% ) in the lenalidomide group and 226 ( 27% ) in the observation group , and no deaths in the lenalidomide group were deemed treatment related . interpretation maintenance therapy with lenalidomide significantly improved progression - free survival in patients with newly diagnosed multiple myeloma compared with observation , but did not improve overall survival in the intention - to - treat analysis of the whole trial population . 
 in patients with high - risk disease , relapse is the result of the persistence of residual disease , 2 , 3 even at very low levels , and is associated with clonal evolution and progressive immune dysfunction.4 , 5 these biological features can impair the activity of subsequent lines of therapy ; therefore , finding strategies that could prevent relapse in this group would be a considerable step forward to improve the outcomes of these patients.6 control or elimination of residual disease clones might be achieved by maintenance therapy , and several strategies have been assessed in this setting , with lenalidomide being the most promising because of its mode of action and tolerability.79 our preceding study , the medical research council myeloma ix trial , 10 compared the use of the immunomodulatory agent thalidomide as maintenance therapy with observation in patients with newly diagnosed multiple myeloma . 
our findings were consistent with the results of other contemporaneous thalidomide maintenance studies.11 , 12 the myeloma xi study was therefore designed to assess whether the newer , better tolerated , immunomodulatory agent lenalidomide limitations of thalidomide as could overcome the maintenance improve therapy progression - free survival and overall survival in patients with newly diagnosed multiple myeloma . this setting and binding of lenalidomide to the cereblon complex13 leads to the ubiquitination of substrates , including the transcription factors ikaros and aiolos , marking them for proteasomal degradation and resulting in decreased expression of interferon regulatory factor 4 ( irf4 ) .14 , 15 lenalidomide has direct tumouricidal effects on myeloma cells and also triggers indirect immuno modulatory effects , including activation of natural killer and t cells , which might help with elimination of minimal residual disease in patients with multiple myeloma.1417 whether or not these mechanisms can help to control residual clonal disease in patients with high - risk cytogenetic disease is unknown . three previous studies have shown that lenalidomide maintenance can delay disease progression after research in context evidence before this study a search of pubmed for clinical trial reports published in english before may , 2010 , using the terms lenalidomide and myeloma and maintenance revealed no published randomised studies of lenalidomide maintenance in patients with newly diagnosed myeloma . 
we showed a significant benefit of lenalidomide maintenance therapy in terms of progression - free survival , which was consistent across both patients eligible for transplantation and those who were ineligible , as well as patients across all cytogenetic risk groups , even those with high - risk disease . 
however , a preplanned subgroup analysis indicates an overall survival benefit in transplantation - eligible patients across all cytogenetic risk groups , even those with high - risk disease , when treated with lenalidomide maintenance therapy after transplantation . implications of all the available evidence the results of the myeloma xi trial contribute to a body of evidence that suggests that the use of lenalidomide as maintenance therapy should be considered for patients with newly diagnosed multiple myeloma , of all cytogenetic risk groups , after autologous stem - cell transplantation . 
with the addition of these new data from the myeloma xi trial , a metaanalysis of all published trials of lenalidomide maintenance after autologous stem - cell transplantation , including 3179 patients , confirmed the overall survival benefit of lenalidomide maintenance therapy compared with observation in this setting ( hazard ratio 072 [ 95% ci 056091 ] )  . 
 in transplantation - ineligible patients , novel approaches to improve overall survival are warranted . vol 20 january 2019 articles autologous stem - cell transplantation in patients with multiple myeloma.79 overall survival outcomes were inconsistent between these studies , none of which was appropriately powered to make robust conclusions based on this endpoint . 
one study8 showed a clear overall survival benefit for those patients treated with maintenance lenalidomide compared with observation , whereas the other two studies7 , 9 showed no significant benefit . 
however , a recently published meta - analysis18 including these trials showed that lenalidomide main tenance can improve overall survival compared with observation in this setting , and it is now approved for use by both the european medicines agency and us food and drug administration . 
 for patients with multiple myeloma who are ineligible for trans plantation , continuous therapy with lenalidomide plus low - dose dexamethasone improved progression - free survival and overall survival compared with a combination of melphalan , prednisone , and thalidomide.19 , 20 no previous studies of either transplantation - eligible or transplantation - ineligible patients had sufficient num bers to assess the effect of lenalidomide maintenance therapy in patients with multiple myeloma and high - risk cytogenetics . here , we aimed to assess the effect of lenalidomide maintenance on the survival of patients with newly diagnosed multiple myeloma , including preplanned subgroup analyses by cytogenetic risk group and transplantation status . methods study design and participants the myeloma xi was a phase 3 , open - label , randomised , adaptive design trial with three randomisation stages ( figure 1 )  . 
there were three potential randomisations in the study : at trial entry for all patients to allocate induction treatment separately for those considered eligible or ineligible for transplantation ; after induction treatment for those patients with a suboptimal response to treatment ( minimal or partial response ) to allocate induction intensification ; and at the completion of induction and intensification or autologous stem - cell transplantation ( where applicable ) to allocate main tenance treatment . 
the trial was done at 110 national health service hospitals in england , wales , and scotland ( appendix p 2 )  . intensification the full study protocol including the inclusion criteria for each randomisation is available in the appendix ( p 34 )  . 
 patients aged at least 18 years and who had symptomatic multiple myeloma or non - secretory multiple myeloma based on bone marrow clonal plasma cells , organ or tissue impairment considered by the clinician to be myeloma related , or paraprotein ( m - protein ) in serum or initial randomisation . 
 urine were eligible for exclusion criteria for the initial randomisation included the previous or concurrent malig nancies , including myelodysplastic syndromes ; previous treatment for myeloma ( except local radiotherapy , bisphosphonates , and corticosteroids ) ; grade 2 or worse peripheral neuro pathy , acute renal failure ( unresponsive to up to 72 h of rehydration , characterised by creatinine > 500 mol / l or urine output < 400 ml per day , or requiring dialysis ) ; and active or previous hepatitis c infection . transplantation ( transplantation patients who were young and fit to tolerate autologous stem - cell eligible ) entered the intensive treatment pathway . 
however , generally , patients aged 60 years or younger entered the intensive ( younger , fitter ) pathway ; those aged 70 years or older entered the nonintensive ( older , less fit ) pathway ; and those aged 6169 years were eligible for either intensive or nonintensive therapy . 
the decision of treatment pathway was made on an individual patient basis , taking into account eastern cooperative oncology group performance status , clinician judgment , and patient preference . for the maintenance therapy randomisation , eligible patients were those who completed their assigned induction therapy according to the protocol ( a minimum of four cycles of cyclophosphamide , thalidomide , and dexamethasone [ ctd ] ; cyclophosphamide , lenali domide , and dexamethasone [ crd ] ; or carfilzomib , cyclophosphamide , lenalidomide , and dexamethasone [ kcrd ] in the intensive pathway , or a minimum of six cycles of attenuated ctd or attenuated crd in the non - intensive pathway ) , and had achieved at least a minimal response and received at least 100 mg / m melphalan if assigned to intensive treatment . the study was approved by the national ethics review board ( national research ethics service , london , uk ) , institutional review boards of the participating centres , and the competent regulatory authority ( medicines and healthcare products regulatory agency , london , uk ) , and was undertaken according to the declaration of helsinki and the principles of good clinical practice as espoused in the medicines for human use ( clinical trials ) regulations . 
the study is closed for accrual , but follow - up continues for planned long - term analysis . randomisation and masking patients considered eligible for transplantation at trial entry were randomly assigned ( 1 : 1 ) to induction treatment with either ctd or crd . 
a computer - generated minimisation algorithm was used to avoid chance imbalances in six variables measured at trial entry : microglobulin ( < 35 mg / l vs 35 < 55 mg / l vs 55 mg / l vs or unknown ) , haemoglobin ( < 115 g / l vs 115 g / l for men ; < 95 g / l vs 95 g / l for women ) , corrected serum see online for appendix vol 20 january 2019 articles induction 4420 patients randomly assigned to induction therapy * 2568 allocated to intensive treatment ( transplantation - eligible patients ) 1852 allocated to non - intensive treatment ( transplantation - ineligible patients ) 2142 excluded 368 died without progression 601 progressed and died 618 progressed and alive 478 withdrew from treatment 58 ineligible 19 unknown reasons 307 patients allocated to the lenalidomide and vorinostat group ( not part of this analysis ) maintenance 1971 randomly assigned to maintenance treatment 1137 allocated to the lenalidomide group ( intention - to - treat population ) 834 allocated to the observation group ( intention - to - treat population ) 40 patients did not commence lenalidomide 12 progressed before treatment initiation 23 withdrew consent 5 missing 1097 received allocated intervention ( safety population ) 834 received allocated intervention ( safety population ) 39 died without progression 193 progressed and died 224 progressed and alive 456 progression - free survival events and 234 overall survival events 8 progressed before randomisation and alive 2 progressed before randomisation and died 533 progression - free survival events and 226 overall survival events 13 died without progression 213 progressed and died 307 progressed and alive 7 progressed before randomisation and alive 671 patients are alive and progression free 294 patients are alive and progression free figure 1 : trial profile * randomisation occurred between may 26 , 2010 , and april 20 , 2016 . 
following a protocol amendment on june 28 , 2013 , and after the accrual of 1512 patients , patients considered eligible for trans plantation were randomly assigned ( 1 : 1 : 2 ) to ctd , crd , or kcrd . 
a similar minimisation algorithm was used to avoid chance imbalances in the six variables measured at trial entry . patients with a suboptimal response to induction treatment were randomly assigned ( 1 : 1 ) to cyclophosphamide , bortezomib and dexamethasone ( cvd ) or no cvd . 
a minimisation algorithm was used to avoid chance imbalances in three variables : allocated induction treatment ( ctd vs crd vs attenuated ctd vs attenuated crd ) , response to induction treatment ( minimal response or partial response ) , and centre . 
 patients allocated to kcrd induction treatment were ineligible for this randomisation . vol 20 january 2019 articles in induction and patients completing three variables : allocated intensification treatment ( where applicable ) and eligible were randomly assigned ( 1 : 1 ) to lenalidomide maintenance or observation . 
 a minimisation algorithm was used to avoid chance imbalances induction treatment ( ctd vs crd vs attenuated ctd vs attenuated crd ) , allocated intensification treatment ( no cvd vs cvd vs not randomised at intensification randomisation ) , and centre . 
following a protocol amendment on june 28 , 2013 , and after accrual of 615 further patients under protocol version 5.0 , patients were randomly assigned ( 2 : 1 ) to lenalidomide or observation . 
a similar minimisation algorithm was used to avoid chance imbalances in the same three variables with the same categories but with the addition of kcrd to the induction treatment options . 
these changes were made to add and remove research questions in this adaptive design study . all randomisations were done at the clinical trials research unit ( leeds , uk ) by authorised members of staff with a centralised automated 24 h telephone system according to a validated minimisation algorithm produced under the supervision of wmg . 
the funders remained masked to treatment results until data cutoff for analysis . procedures the dose , schedule , and route of administration of each drug included in the induction and consolidation regimens are in the protocol ( appendix p 34 )  . 
briefly , in transplantation - eligible patients , induction therapy with ctd , crd , or kcrd continued for at least four cycles in the absence of progressive disease , until maximum response or intolerance was observed . 
for all patients , bisphosphonates were recom mended until progressive disease and thrombo prophylaxis was recom mended for at least the first 3 months of treatment as per imwg recommendations . 
growth factor support and prophylaxis for pneumonia , varicella , fungal infection , and tumour lysis syndrome were allowed as per local practice . transplantation - eligible patients receiving kcrd proceeded to high - dose melphalan and autologous stem - cell transplantation . 
patients receiving immunomodulatory - based triplets ( ctd vs crd ) followed a response - adapted approach : those with complete response or very good partial response ( assessed according to international myeloma working group [ imwg ] criteria ) proceeded to autologous stem - cell transplantation in the transplantation - eligible pathway , whereas transplantation - ineligible patients proceeded directly to maintenance randomisation . 
for maintenance therapy , 100 days after autologous stem - cell transplantation or once a maximum response was achieved for transplantation - ineligible patients , patients initially received lenalidomide 25 mg per day ( orally on days 121 of each 28 - day cycle ) or were observed without lenalidomide therapy . 
following a protocol amendment on sept 14 , 2011 , and after accrual of 442 patients , patients were allocated ( 1 : 1 : 1 ) to receive lenalidomide 10 mg per day ( orally on days 121 of each 28 - day cycle ) , lenalidomide 10 mg per day ( orally on days 121 of each 28 - day cycle ) plus vorinostat 300 mg per day ( orally on days 17 and 1521 of each 28 - day cycle ) , or observation . 
after accrual of 615 more patients , a further protocol amendment on june 28 , 2013 , allocated patients to receive lenalidomide 10 mg per day ( orally on days 121 of each 28 - day cycle ) or observation in a 2 : 1 ratio , and the lenalidomide plus vorinostat group was discontinued . 
this change was proposed by the myeloma xi trial management group and approved by the myeloma xi data monitoring and ethics committee ( dmec ) on june 24 , 2011 . 
the change in dose was based on emerging results from previous studies using 10 mg lenalidomide weighted against the potential for late toxicity ( increased secondary primary malignancy ) , which was being reported in other trials at that time . 
patients receiving lenalidomide in combination with vorinostat will be reported elsewhere when the primary endpoint has been met in that group . response and disease progression were assessed on the basis of imwg uniform response criteria21 , 22 and reviewed centrally by an expert panel masked to treatment allocation . 
 serious adverse events were reported for all patients from the date of randomisation until 30 days after the date of disease progression except in the case of serious adverse reactions or second primary malignancies , which were collected for the duration of the trial . 
second primary malignancies were reported as serious adverse events for the duration of the study ( ie , until death for each patient or when the study closes , whichever was earlier )  . 
 on recovery , treatment was restarted at the previous dose , with the addition of granulocyte colony - stimulating factor in the case of grade 3 neutropenia with fever or grade 4 neutropenia . 
if neutropenia or thrombocytopenia occurred a second time , then the dose was reduced by one dose level as stipulated in the protocol ( eg , from 10 mg daily to 5 mg daily )  . 
full details of the dose reduction schedules are shown in the protocol ( appendix p 34 )  . cytogenetic risk profiling was performed by use of multiplex ligation - dependent probe amplification and quantitative real - time pcr using dna and rna respectively , which was extracted from cd138 - selected plasma cells from bone marrow biopsy samples taken before treatment initiation . 
quantitative real - time pcr was used to assess the expression of translocation gene partners including t ( 4 ; 14 ) : mmset , fgfr3 , t ( 14 ; 16 ) : maf , and t ( 14 ; 20 ) : mafb . 
multiplex ligation - dependent probe amplifi cation was used to assess copy number aberrations by including probe sets at sites of the commonly deleted or amplified regions in myeloma ( eg , at genes cks1b on 1q21.3 and tp53 on 17p13 )  . 
these techniques are validated and provide equivalent results to interphase fluorescence in - situ hybridisation.2325 patients were classified into three cytogenetic risk groups for the preplanned analysis of outcomes : standard risk ( no adverse cytogenetic abnormalities ) , high risk ( one adverse cytogenetic abnormality ) , or ultra - high risk ( two or more adverse cytogenetic abnormalities )  . 
adverse cytogenetic abnormalities were defined as gain ( 1q ) , t ( 4 ; 14 ) , t ( 14 ; 16 ) , t ( 14 ; 20 ) , or del ( 17p ) .2 , 3 in a post - hoc analysis , an alternative cytogenetic high - risk classification was used , including patients with t ( 4 ; 14 ) , del ( 17p ) , or t ( 4 ; 14 ) and del ( 17p ) .7 outcomes the co - primary endpoints of the maintenance evaluation of the trial were progression - free survival and overall survival . 
overall survival was defined as the time from maintenance randomisation to death from any cause or last follow - up . secondary endpoints were progression - free survival 2 , defined as the time from maintenance randomisation to the date of second progressive disease , start of third antimyeloma treatment , or death from any cause ; the time to improved response ; and toxicity . 
exploratory analyses of progression - free survival , overall survival , and response by cytogenetic risk group in the overall population and by cytogenetic risk group were prespecified by protocol and by induction / intensification treatment were prespecified in the statistical analysis plan within each pathway . lactate dehydrogenase , iu / l 262 ( 178381 ) 271 ( 183366 ) cytogenetic risk assessment available transplantation eligibility and induction regimen transplantation eligible kcrd transplantation ineligible attenuated ctd attenuated crd vol 20 january 2019 articles this in the statistical analysis the data cutoff date for this analysis was oct 23 , 2017 . 
we present here the results of the co - primary endpoints , some secondary endpoints ( progression - free survival 2 and toxicity ) , and prespecified subgroup analysis for the trial . 
for progression - free survival , the trial was designed to demonstrate a 67 - month increase in median progression - free survival lenalidomide group ( median 267 months ) compared with the observation group ( median 200 months , hazard ratio [ hr ] 075 ) when 509 progression - free survival events had been observed . 
 for overall survival , it was designed to demonstrate a 10% increase in 5 - year overall survival in the lenalidomide group ( 60% at 5 years ) compared with the observation group ( 50% at 5 years , hr 074 ) when 458 overall survival events had been observed . 
each of these calculations assumed the time to event was exponentially distributed and that recruitment would last 325 years with 4 years of further follow - up , a two - sided 5% significance level , and 90% power . 
patients randomly assigned during a transient period of the trial to the combination of lenalidomide and vorinostat ( n = 307 ) , as per the protocol modification on sept 14 , 2011 , were excluded from this analysis and will be reported elsewhere . for the co - primary endpoints , we estimated summaries of time to event per treatment group using the kaplanmeier method . 
we made comparisons between the allocated groups using the cox proportional hazards model stratified by the minimisation stratification factors , excluding centre , and to estimate hrs and 95% cis . 
we also did sensitivity analyses for progression - free survival using similar models in which those participants identified to have progressed in advance of maintenance randomisation were defined as having an event at the time of maintenance randomisation . 
subgroup analysis was prespecified for the presence or absence of individual adverse cytogenetic abnormalities , cytogenetic risk status , and induction and consolidation treatment ( cvd intensification and transplantation eligibility )  . 
we did a likelihood ratio test for heterogeneity of treatment effect using cox models identical to those used for the main analysis , with the inclusion of terms for the lenalidomide group ( n = 1137 ) observation group ( n = 834 ) ( continued from previous page ) cvd randomisation after minimal or partial response allocated to cvd allocated to no cvd received cvd after stable or progressive disease response at maintenance randomisation complete or very good partial response partial or minimal response stable or progressive disease unable to assess unknown 79 ( 7% ) 98 ( 9% ) 16 ( 1% ) 945 ( 83% ) 172 ( 15% ) 8 ( 1% ) 10 ( 1% ) 2 ( < 1% ) 63 ( 8% ) 78 ( 9% ) 8 ( 1% ) 705 ( 85% ) 118 ( 14% ) 6 ( 1% ) 1 ( < 1% ) 4 ( < 1% ) data are median ( iqr ) , n ( % ) , or n / n ( % )  . 
 stratification factor in minimisation algorithm . table 1 : baseline characteristics subgroup in question and the appropriate interaction ter the reported test for heterogeneity for subgroup analysis corresponds to a one degree of freedom test for two category subgroups and a two degrees of freedom test for three category subgroups . we summarised toxicity , in terms of adverse events , descriptively . 
we used fine and gray competing risks regression to compare the hazard of second primary malignancies by allocated treatment , adjusting for the minimisation stratification factors , with unrelated deaths specified as a competing risk . 
we calculated person - years on trial as the sum of all patients receiving at least one dose of study treatment of the time in years from randomisation to death or last date known to be alive . 
to ensure an overall significance level of 5% was maintained , we used the obrien and fleming alpha - spending function with bounds specified at the time of the interim analysis related to the proportion of information accrued ( interim analysis bound 094% , final analysis bound 47% )  . 
all reported p values are two sided and considered significant at an overall significance level of 5% . we used sas ( version 9.4 ) , stata / ic , and r ( version 3.2.3 ) for statistical analyses . this study is registered with the isrctn registry , number isrctn49407852 , and clinicaltrialsregister.eu , number 2009 - 010956 - 93 . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results the maintenance 1971 patients were accrued randomisation between jan 13 , 2011 , and aug 11 , 2017 . 
 patient and disease characteristics were well balanced between groups ( table 1 )  . lenalidomide and 20 months the median follow - up after randomisation for this analysis was 31 months ( iqr 1850 )  . 
for the primary analyses , 456 ( 40% ) of 1137 patients in the lenalidomide group and 533 ( 64% ) of 834 patients in the observation group had disease progression or died . 
median progression - free survival was 39 months ( 95% ci 3642 ) with ( 1822 ) with observation ( hr 046 [ 95% ci 041053 ] ; p < 00001 ; figure 2a )  . 
a sensitivity analysis including those patients who had disease progression before maintenance randomisation , in which events were defined at the time of maintenance randomisation rather than being censored at the time of maintenance randomisation , gave similar results ( appendix p 33 )  . 234 ( 21% ) of 1137 patients died in the lenalidomide group and 226 ( 27% ) of 834 patients died in the observation group . 
 3 - year overall survival was 786% ( 95% cl 756816 ) in the lenalidomide group and 758% ( 724792 ) in the observation group , and 5 - year overall survival was 613% ( 95% cl 566661 ) in the lenalidomide group and the observation group . 
no 566% ( 515617 ) difference was detected between lenalidomide and observation for overall survival ( hr 087 [ 95% ci 073105 ] ; p = 015 ; figure 2b )  . 
the most common cause of death was tumour load ( appendix p 25 )  . 285 ( 25% ) of 1137 patients in the lenalidomide group and 328 ( 39% ) of 834 patients in the observation group had second disease progression or died . 
median progressionfree survival 2 was 64 months ( 95% ci 57not reached ) vol 20 january 2019 articles with lenalidomide and 45 months ( 4150 ) with observation ( hr 065 [ 95% ci 056077 ] ; p < 00001 ; figure 3 )  . at the time of analysis , the median duration of therapy was 18 cycles lenalidomide maintenance ( iqr 630 )  . 
reasons for discontinuing in the 594 patients who had ceased lenalidomide maintenance were disease progression or death in 320 ( 54% ) patients , adverse events in 167 ( 28% ) patients , patient preference in 45 ( 8% ) patients , other reasons for 43 ( 7% ) patients , and unknown reasons for 19 ( 3% ) patients . 
the most common grade 3 or 4 haematological adverse reactions in the lenalidomide group were neutropenia in 362 ( 33% ) patients , thrombocytopenia in 72 ( 7% ) patients , and anaemia in 42 ( 4% ) patients . 
serious adverse events were reported in 494 ( 45% ) of 1097 patients receiving lenalidomide compared with 150 ( 17% ) of 874 patients on observation ( appendix p 29 )  . 
the 3 - year cumulative incidence of second primary malignancies was low , but higher in the lenalidomide group than the observation group ( 53% [ 95% ci 3671 ] vs 31% [ 1845 ] ; hr 185 [ 95% ci 118290 ] ; appendix p 5 )  . 
the overall incidence of second primary malignancies per 100 patient - years was 24 ( 95% ci 1931 ) in the lenalidomide group and 14 ( 1020 ) in the observation group . 
the 3 - year cumulative incidence of deaths related to second primary malignancies was low in both groups ( 20% [ 95% ci 0931 ] in the lenalidomide group vs 09% [ 0216 ] in the observation group ; appendix p 6 )  . 
 a summary of all second primary malignancies by intervention group is shown in the appendix ( p 30 )  . the most common serious adverse events were infections in both the lenalidomide group and the observation group . 
460 deaths occurred during maintenance treatment , 234 ( 21% ) in the lenalidomide group and 226 ( 27% ) in the observation group , and no deaths in the lenalidomide group were reported as treatmentrelated ( appendix p 25 )  . in the subgroup analyses , the benefit of lenalidomide on progression - free survival was seen across most sub groups of patients ( figure 4a ) , including those prespecified ( transplantation - eligible and transplantation - ineligible patients and those defined as standard risk , high - risk and ultra - high risk genetics )  . 
the only significant heterogeneity was between patients who achieved a complete or very good partial response and those who had a partial or minimal therapy ( pheterogeneity < 00001 )  . 
the table includes grade 1 or 2 adverse events occurring in at least 10% of patients and grade 3 or 4 events in at least 1% of patients ( the rest of the grade 3 and 4 adverse events are in the appendix pp 2628 )  . 
 table 2 : adverse events in patients treated with lenalidomide maintenance therapy ( n = 1097 ) vol 20 january 2019 articles progression - free survival was 57 months ( 95% ci 50not reached ) in the lenalidomide group and 30 months ( 2532 ) in the observation group in transplantationeligible patients ( hr 048 [ 95% ci 040058 ] ; p < 00001 ; figure 4b ) , and in transplantation - ineligible patients , median progression - free survival was 26 months ( 95% ci 2231 ) with lenalidomide and 11 months ( 523 ) with observation ( hr 044 [ 95% ci 037053 ] ; p < 00001 ; figure 4c )  . for the prespecified subgroup analysis by cytogenetic risk group , the baseline characteristics between patients with ( 774 [ 39% ] of 1971 ) and without ( 1197 [ 61% ] of 1971 ) cytogenetic data available were balanced ( appendix p 31 )  . 
 progression - free survival was improved in patients of all cytogenetic risk groups ( standard risk , high risk , and ultra - high risk ) who received lenalidomide compared with those on observation ( appendix p 9 ) ; the benefit lenalidomide was also seen across these risk categories when the intention - to - treat popu lation was divided into transplantation - eligible and transplantationineligible patients , with no significant heterogeneity between genetic subgroups ( pheterogeneity = 098 for transplantation - eligible patients , pheterogeneity = 076 for transplantation - ineligible patients ; appendix pp 1011 )  . 
similar results for progression - free survival were seen if the definition of high risk was restricted to patients with t ( 4 ; 14 ) , t ( 4 ; 14 ) and del ( 17p ) , or del ( 17p ) compared with those with out either t ( 4 ; 14 ) or del ( 17p ) , independently of transplantation eligibility ( appendix pp 1214 )  . 
 * likelihood ratio test for heterogeneity of effect among patients with subgroup data available . in the subgroup analysis of overall survival ( figure 5a ) , there was significant heterogeneity in outcomes based on pathway for previous induction treatment ( pheterogeneity = 00445 ) and age ( pheterogeneity = 00442 ) , with age probably acting as a surrogate for transplantation pathway eligibility . 
a significant improvement in overall survival was seen in transplantation - eligible patients treated with lenalidomide compared with those assigned vol 20 january 2019 articles to observation ( 3 - year overall survival in transplant [ 95% cl 843907 ] with eligible patients 875% lenalidomide and 802% [ 760844 ] with observation ; hr 069 [ 95% ci 052093 ] ; p = 0014 ; figure 5b )  . 
 however , lenalidomide maintenance therapy did not improve overall survival in transplantation - ineligible patients ( 3 - year overall survival 668% [ 616721 ] with lenalidomide and 698% [ 644752 ] with observation ; hr 102 [ 95% ci 080129 ] ; p = 088 ; figure 5c )  . 
the benefit of lenalidomide maintenance therapy on overall survival in the transplantation - eligible patients was also confirmed across subgroups based on age , disease stage , induction therapy , and response at baseline ( appendix p 15 )  . 
 * likelihood ratio test for heterogeneity of effect amongst patients with subgroup data available . 59 months ( 95% ci 52not reached ) for the observation group ( hr 057 , 95% ci 044073 ; p < 00001 ) ; and for transplant - ineligible patients it was 43 months ( 3948 ) for the lenalidomide group and 35 months ( 3139 ) for the observation group ( hr 072 , 058088 ; p = 00016 )  . 
the transplantationineligible group of patients had a higher frequency of nonmyeloma - related deaths ( appendix p 25 ) , and a high proportion of these patients initially assigned to the observation group subsequently received lenalidomide ( 103 [ 33% ] of 316 patients ) or ceased treatment before disease progression without intolerance ( 119 [ 29% ] of 407 patients )  . finally , to take account of all available results of lenalidomide as maintenance therapy for patients with multiple myeloma , we did a summary meta - analysis of our data with those previously published , including 3179 patients . 
these results show the hr for overall survival with the use of a lenalidomide maintenance regimen was 072 ( 95% ci 056091 ; appendix p 24 )  . the heterogeneity statistic i = 546 indicated potential moderate heterogeneity . 
no analysis of risk of bias was undertaken . discussion in this phase 3 , open - label , randomised trialwhich is , to our knowledge , the largest of its kindlenalidomide main tenance significantly improved progression - free survival compared with observation in adult patients with newly diagnosed multiple myeloma . 
however , overall survival was not improved with this treatment regimen in the intention - to - treat analysis . the progression - free survival benefit of maintenance therapy with lenalidomide seems to continue through the subsequent line of therapy with progression - free survival 2 significantly improved with lenalidomide compared with observation in both transplantation - eligible and trans plantation - ineligible patients . 
this hypo thesis is also supported by previous analyses indicating that lenalidomide maintenance did not increase genomic change or mutational load.26 , 27 a prespecified subgroup analysis suggested that continuous lenalidomide improved overall survival in transplantation - eligible patients but not in transplantationineligible patients . 
we speculate that any overall survival benefit in trans plantation - ineligible patients might have been attenuated by a high proportion of patients ceasing treatment prematurely and those initially randomised to observation who received lenalidomide in later lines of treatment . 
additional secondary and exploratory endpoints including response , survival after progression , time to progression , time to next line of treatment , changes in mean paraprotein during protocol treatment , and time to improved response will also be presented subsequently . an adverse cytogenetic profile is a major risk factor for relapse , and outcomes for patients with high - risk cytogenetics are poor.1 , 3 , 28 data supporting the use of lenalidomide maintenance in patients with adverse cytogenetics are scarce , and results thus far have been inconclusive . 
although the myeloma xi had a much larger sample size than that of previous studies , our subgroup analyses were not powered and further therefore are not conclusive and warrant investigation . 
however , baseline characteristics and outcomes were similar between patients with and without cytogenetic data available . another limitation of the trial is the lack of prospectively collected quality - of - life data . 
however , given that the time until first disease progression is often when patients with myeloma have a better quality of life , the improvement in progression - free survival and progression - free survival 2 seen in our study suggests the use of maintenance lenalidomide would be of benefit in the transplantationineligible setting . cytogenetic high risk has been defined by several groups using different markers . 
in our previous study , 3 identified adverse cytogenetic abnormalities as gain ( 1q ) , t ( 4 ; 14 ) , t ( 14 ; 16 ) , t ( 14 ; 20 ) , or del ( 17p ) , with standard risk ( no adverse cytogenetic abnormalities ) ; high risk ( one adverse cytogenetic abnormality ) , or ultrahigh risk ( two or more adverse cytogenetic abnormalities ) groups identified , and this classification was used in our prespecified analysis . 
 data using both of nevertheless , cannot equilibrate the outcomes for high - risk patients to those of standard risk , and patients with high - risk lesions still have combining maintenance lenalidomide with additional agents might be beneficial and could be investigated . 
in the myeloma xi trial , a separate group of patients received vorinostat plus lenalidomide in the maintenance randomisation because of a protocol amendment , and the outcomes of these patients will be reported elsewhere . 
in transplantation - eligible patients , three studies have shown that the addition of lenalidomide maintenance after autologous stem - cell transplantation reduces the risk of progression or death by approximately 50% compared with placebo or no maintenance.79 a significant improvement in overall survival has only been observed in one previous trial , 8 although a recent meta - analysis did suggest an overall survival improvement in patients treated with lenalidomide in this setting.15 to take account of all available results so far now including the myeloma xi study , we did a summary for transplantation - ineligible patients with multiple myeloma , a significant improvement in progression - free survival has been reported when lenalidomide maintenance was given after a regimen of melphalan , prednisone , and lenalidomide ( median progression - free survival from start of induction 31 months vs 14 months ) ; the 3 - year overall survival in this study was 70% with maintenance and 62% without maintenance therapy.29 furthermore , in a study comparing treatment with lenalidomide and low - dose dexamethasone given either continuously or for a limited number of cycles , 21 continuous treatment significantly improved progressionfree survival ( median 26 months vs 21 months from start of induction , hr 070 , 95% ci 060081 ) but there was no difference in overall survival ( median 591 months vs 623 months , 102 , 086120 )  . 
taken together , these observations suggest that alternative approaches to improving overall survival in older patients who are not eligible for transplantation are warranted . the current findings with lenalidomide maintenance compare favourably to those achieved with other novel therapies in the maintenance setting . 
thalidomide has been shown to improve progression - free survival when given as maintenance therapy in the myeloma ix trial ( median progression - free survival 22 months vs 15 months ; hr 144 , 95% ci 122170 ; p < 00001 ) , but the median overall survival was similar in both groups ( 60 months vs 60 months ; 096 , 079117 ; p = 070 ) .10 , 30 in a subgroup analysis , patients with high - risk status receiving thalidomide had no progression - free survival or overall survival benefit . 
by contrast , in this current study , we have shown that lenalidomide improves progression - free survival irrespective of cytogenetic risk status , which might be due to mechanistic differences between these drugs . 
although thalidomide and lenalidomide share a similar mechanism of action , recent studies suggest that subtle variations in the chemical structure between the molecules can modulate the range of substrates targeted for degradation by the e3 ubiquitin ligase , leading to different downstream effects.31 in the myeloma xi trial , few patients discontinued because of adverse events or patient preference and there was no evidence of cumulative toxicity . 
the risk of second primary malignancies was increased in patients treated with maintenance lenalidomide , but the 3 - year cumulative incidence of second primary malignancies remained low in both treatment groups . in summary , lenalidomide maintenance improved progression - free survival therapy significantly patients with newly diagnosed multiple myeloma compared with observation , but overall survival was not improved in the intention - to - treat analysis across the whole trial population . 
additionally , prespecified subgroups analyses by cytogenetic risk and transplantation status suggested a progression - free survival benefit across vol 20 january 2019 articles all cytogenetic risk groups , and an overall survival benefit in transplantation - eligible patients . should be directed to the corresponding author in the first instance ; to gain access , data requestors will need to sign a data access agreement . contributors ghj , fed , nhr , and gjm were chief investigators . 
all authors contributed to the review and amendments of the manuscript for important intellectual content and approved this final version for submission . declaration of interests ghj has received consultancy fees , honoraria and speakers bureau fees from roche , amgen , janssen , and merck sharp and dohme ; and consultancy fees , honoraria , travel support , research funding , and speakers bureau fees from celgene corporation and takeda . 
cdw has received honoraria , travel support , and speakers bureau fees from takeda , janssen , and celgene corporation ; honoraria and speakers bureau fees from amgen ; and honoraria from novartis . 
jl has received consultancy fees from janssen ; travel support from novartis and takeda ; consultancy fees and travel support from bristol - myers squibb ; and honoraria and travel support from celgene corporation . 
mwj has received consultancy fees , honoraria , travel support , and research funding from janssen ; consultancy fees , honoraria , and travel support from takeda and amgen ; consultancy fees , honoraria , and research funding from celgene corporation ; and consultancy fees and honoraria from novartis . 
gc has received consultancy fees , honoraria , research funding , and speakers bureau fees from takeda , celgene corporation , janssen , and amgen ; consultancy fees and honoraria from glycomimetics and bristol - myers squibb ; and consultancy fees , honoraria , and speakers bureau fees from sanofi . 
mfk has received consultancy fees and travel support from bristol - myers squibb and takeda ; consultancy fees from chugai ; consultancy fees and honoraria from janssen and amgen ; and consultancy fees , honoraria , and research funding from celgene corporation . 
 gjm has received research funding from janssen ; consultancy fees and honoraria from bristol - myers squibb and takeda ; and consultancy fees , honoraria , and research funding from celgene corporation . data sharing de - identified participant data will be made available when all trial primary and secondary endpoints have been met . 
any requests for trial data and supporting material ( data dictionary , protocol , and statistical analysis plan ) will be reviewed by the trial management group in the first instance . 
we are grateful to the uk national cancer research institute haematological oncology clinical studies group ; uk myeloma research alliance ; and all principal investigators , subinvestigators , and local centre staff for their dedication and commitment to recruiting patients to the study . 
 the support of the clinical trials research unit at the university of leeds ( uk ) was essential to the successful running of the study ; we thank all their staff who have contributed , past and present . 
central laboratory analysis was done at the institute of immunology and immunotherapy , university of birmingham ( uk ) ; the institute of cancer research , london ( uk ) ; and the haematological malignancy diagnostic service , st jamess university hospital , leeds . 
we investigated infertility and time to pregnancy in female childhood cancer survivors , and analysed treatment characteristics associated with infertility and subsequent pregnancy . methods the childhood cancer survivor study ( ccss ) is a cohort study including 5 year cancer survivors from 26 canadian and us institutions who were younger than 21 years at the time of diagnosis between jan 1 , 1970 , and dec 31 , 1986 , and a sibling control group . 
self - reported infertility , medical treatment for infertility , time to rst pregnancy in survivors and siblings , and the risk of infertility in survivors by demographic , disease , and treatment variables were analysed . findings 3531 survivors and 1366 female sibling controls who enrolled between nov 3 , 1992 , and april 4 , 2004 , were included . 
compared with their siblings , survivors had an increased risk ( relative risk [ rr ] 148 [ 95% ci 123178 ] ; p < 00001 ) of clinical infertility ( ie , > 1 year of attempts at conception without success ) , which was most pronounced at early reproductive ages ( rr 292 [ 95% ci 118720 ] , p = 0020 , in participants 24 years ; 161 [ 105248 ] , p = 0029 , in those aged 2529 years ; and 137 [ 111169 ] , p = 00035 , in those aged 3040 years )  . 
despite being equally likely to seek treatment for infertility , survivors were less likely than were their siblings to be prescribed drugs for treatment of infertility ( 057 [ 95% ci 046070 ] , p < 00001 )  . 
although survivors had an increased time to pregnancy compared with their siblings ( p = 0032 ) , 292 ( 64% ) of 455 participants with self - reported clinical infertility achieved a pregnancy . interpretation a more comprehensive understanding of infertility after cancer is crucial for counselling and decision making about future conception attempts and fertility preservation . funding national cancer institute , american lebanese syrian associated charities , swim across america . introduction substantial improvements in cancer treatment have greatly increased 5 year survival for childhood cancers , which now exceeds 80% in the usa.1 infertility is reported as a major concern about the long - term e ects of female cancer survivors.2 , 3 treatment , especially menstruation is not a sensitive way to identify the gonadotoxic e ects of treatment and many survivors of childhood cancer are at risk of unrecognised infertility.4 the risk of non - surgical premature menopause in childhood cancer survivors is increased compared with that in their siblings , with a cumulative incidence of 8% by age 40 years.5 furthermore , childhood cancer survivors are less likely to become pregnant than are their siblings.6 , 7 likelihood of pregnancy as a measure of fertility does not take into account individual desires for childbearing or attempts at pregnancy and thus does not assess infertility . 
therefore , previous studies might the prevalence of have underestimated the risk of infertility in survivors of childhood cancer . we quanti ed the risk of infertility in survivors of childhood cancer on the basis of clinical de nitions of infertility and treatment characteristics in childhood cancer that increase the risk of infertility . 
additionally , we assessed if the length of time to pregnancy is longer in survivors of childhood cancer than in their siblings who have conceived . identi ed disease and methods study design and participants details of design , cohort characteristics , and baseline data collection of the childhood cancer survivor study ( ccss ) have been published previously.8 , 9 brie y , ccss is a collaborative study at 26 clinical centres in canada and the usa in which a cohort of 5 year cancer survivors who were diagnosed with an eligible malignancy before age 21 years between jan 1 , 1970 , and dec 31 , 1986 , was assembled . 
eligible malignancies were leukaemia , cns cancer , hodgkins lymphoma , vol 14 august 2013 articles lymphoma , wilms non - hodgkin tumour , neuroblastoma , soft - tissue sarcoma , and bone tumours . 
the next - of - kin ( usually parents or spouse ) of patients who had survived at least 5 years but subsequently died was contacted . participants in the ccss are required to complete a baseline questionnaire when they join the study . 
for our study , we included women who were aged 1839 years when they completed the baseline questionnaire between nov 3 , 1992 , and april 4 , 2004 , who reported they had ever been sexually active . previously published ccss data8 show no di erences in clinical or demographic characteristics between participants in the study and non - participants , other than a high rate of non - participation in the next - of - kin of patients who had died and a somewhat low proportion of male participants . 
written institution approved consent was obtained from all participants . procedures data about disease and treatment characteristics ( type and dose of chemotherapeutic drugs ; radiation eld size , 20 690 eligible survivors 17 632 available survivors 14 358 completed baseline questionnaire 3058 lost to follow - up after tracing 3274 chose not to participate 3962 were < 18 years or 10 827 were excluded active * 40 years at contact 5618 were male 1247 were never sexually 3531 women aged 1839 years who reported ever being sexually active comprised the study population figure 1 : flowchart of cancer survivor cohort included in infertility analyses * includes uncertain or incomplete data . site , and dose ) were gathered by medical record abstraction at each collaborating institution.5 the total exposure to alkylating agents was quanti ed with the alkylating agent score , which accounted for the number of alkylating agents given and the doses of each individual agent ( total dose per m of body surface area )  . 
distribution of doses of each alkylating agent was determined and each patient was assigned a score of 0 to 3 for each drug ( 0 represents no exposure and 1 , 2 , and 3 represent the lower , middle , and upper tertile of doses of that drug , respectively )  . 
doses of individual alkylating agents used to derive the score have been previously published.6 individual drug scores for each patient were summed , and an overall score of 0 to 3 was assigned.10 individual chemotherapeutic drugs , bone marrow transplantation , history of relapse , and history of second malignancy before completion of the baseline questionnaire were deemed additional exposures . 
doses of radiation therapy to the ovaries , uterus , and hypothalamus pituitary were estimated as previously described by stovall and colleagues.11 , 12 to become pregnant , without we used two de nitions of infertility . 
the rst , clinical the commonly accepted infertility , was based on de nition for infertility and included anyone who responded yes to the question , was there ever a period in your life when you and a partner tried for 1 year or more success ? .13 the second de nition , total infertility , included clinically infertile women and those who reported ovarian failure , which was de ned as never having had a menstrual period or menstrual periods stopping 5 years or more before the baseline questionnaire . 
patients were asked to recall any instance of infertility that occurred up to the time of the baseline questionnaire . participants who reported at least one pregnancy at any point after their cancer diagnosis were asked to complete a pregnancy questionnaire , which included questions about whether the pregnancy was planned , and , if so , how many months the participant tried to get pregnant for . 
we did not ask patients when they began trying to become pregnant or when they experienced infertility , and therefore could not account for individual di erences in follow - up time . 
inclusion of covariates in the multivariate models was based on clinical judgment and examination of the univariate estimates . 874 vol 14 august 2013 articles analyses subsequent risk of total infertility and clinical infertility were rst assessed in a model comparing survivors and siblings . 
potential factors for inclusion in multivariate models were age at baseline questionnaire , race , education level , smoking status , and body - mass index ( bmi )  . 
we postulated that the risk of infertility would increase with age and that the relative risk of infertility in survivors versus siblings would fall with age at time of baseline questionnaire . 
in view of the high correlation between these variables , we could not t a multivariate model included both uterine that radiotherapy dose and maximum ovarian radiotherapy dose , and thus uterine dose is reported in this study to exposure . 
 we used a modi ed poission regression with robust variance estimates for all relative risk ( rr ) estimates and 95% cis.14 and gonadal from and on the basis of data from the supplemental pregnancy questionnaire , we compared time to rst conception between survivors and siblings , who were included if they reported at least one planned pregnancy . 
to describe di erences between groups de ned by survivor status ( ie , survivor vs sibling ) , or among survivors between treatment exposures , we examined empirical cumulative distribution plots and used wilcoxon rank - sum or kruskal - wallis tests . 
we used sas ( version 9.2 ) for all statistical analyses . role of the funding source the study sponsors had no role in study design ; collection , analysis , or interpretation of data ; writing of the article ; or the decision to submit for publication . 
jsn and wml had full access to raw data , and the corresponding author had full access to all the data and the nal responsibility to submit for publication . results 20 690 survivors were eligible for inclusion , 3058 ( 15% ) of whom could not be located after intensive tracing e orts . 
4775 eligible siblings were contacted and 4023 ( 84% ) participated . 14 358 of the 17 632 ( 81% ) survivors contacted provided a baseline questionnaire ( gure 1 ) and 3531 were eligible for inclusion . 
n = 208 in the survivor group and 75 in the sibling group . table 2 : comparison of infertility and use of medical services for infertility between survivors and their siblings group . 
2894 of 3531 ( 82% ) survivors and 1186 of 1366 ( 87% ) siblings were still menstruating at the time of the baseline questionnaire . compared with their siblings , cancer survivors had an increased risk of both clinical and total infertility . 
 after adjustment for known sociodemographic and behavioural risk factors , the rr of clinical infertility in survivors siblings was 148 ( 95% ci 123178 ; p < 00001 )  . 
this adjusted risk was more pronounced at younger ages at study participation ( rr 292 [ 95% ci 118720 ] , p = 0020 , in participants 24 years ; 161 [ 105248 ] , p = 0029 , in those aged 2529 years ; and 137 [ 111169 ] , p = 00035 , in those aged 3040 years )  . compared with their the likelihood of visiting a doctor for infertility did not di er between survivors and siblings who reported clinical infertility , neither did the likelihood of the doctor nding a reason for infertility ( table 2 )  . 
however , survivors were signi cantly less likely than were their siblings to receive drugs to help them become pregnant ( rr 057 [ 95% ci 046070 ] , p < 00001 ; table 2 )  . 
 we noted signi cant unadjusted increases in risk of infertility in female cancer survivors who were older at childhood cancer diagnosis , older at study entry , currently or previously married , or current smokers and those with high bmis or lower educational attainment ( table 3 )  . 
in adjusted models , only associations with older age ( ie , > 29 years vs 2429 years ) at the time of the baseline questionnaire ( rr 168 [ 95% ci 126224 ] ; p = 00004 ) , marital status ( currently married vs never married ; 791 [ 4581368 ] ; p < 00001 ) , and bmi ( > 30 kg / m vs 185 < 250 ; 171 [ 130226 ] ; p = 00002 ) remained signi cant . 
a signi cant association between age at primary diagnosis and infertility was not recorded after adjustment . in unadjusted models , cancer survivors with a history of lymphoma or who received any radiotherapy , total body irradiation , or radiotherapy to the abdomen or pelvis had an increased risk of infertility ( table 3 )  . 
 additionally , increasing doses of uterine radiotherapy , exposure to high cumulative doses of alkylating agents ( ie , an alkylating agent score of 3 ) , and pituitary radiation doses of 130 gy signi cantly increased the risk of infertility ( table 3 )  . 
in adjusted models , compared with no uterine radiotherapy , uterine radiotherapy doses of greater than 5 gy ( rr 248 [ 95% ci 154401 ] , p = 00002 , for 51100 gy ; 202 [ 127323 ] , p = 00032 , for 101200 gy ; and 195 [ 95% ci 119319 ] , p = 00080 , for > 200 gy ) signi cantly increased the risk of infertility , as did an alkylating agent score of 3 compared with a score of 0 ( 148 [ 110199 ] , p = 00093 )  . 704 participants reported a planned rst pregnancy . 
time to pregnancy did not di er signi cantly on the basis of alkylating agent score ( gure 2d )  . took signi cantly longer nearly two - thirds ( 292 of 455 [ 64% ] ) of survivors with self - reported clinical infertility achieved a pregnancy . 
 in adjusted analyses , infertile survivors who received more than 10 gy of uterine radiotherapy were signi cantly less likely to become pregnant than were those who were not exposed ( rr 033 for 10120 gy ; [ 95% ci 014075 ] , p = 00087 , 021 [ 008060 ] , p = 00023 for > 20 gy )  . 
referent. table 3 : unadjusted relative risk of clinical infertility by demographic , disease , and treatment characteristics in survivors of childhood cancer 878 vol 14 august 2013 articles p = 0032 p = 0045 sibling ( n = 253 ) survivor ( n = 423 ) no abdominal radiotherapy ( n = 284 ) any abdominal radiotherapy ( n = 94 ) p = 0091 p = 0088 no brain or head radiotherapy ( n = 287 ) any brain or head radiotherapy ( n = 90 ) time ( months ) time ( months ) figure 2 : time to rst pregnancy among survivors and siblings by group ( a ) , abdominal radiotherapy ( b ) , brain or head radiotherapy ( c ) , and alkylating score ( d ) for presentation purposes , plots were truncated at 40 months . 
however , all available data were used in estimations of distributions and group comparisons . score = 0 ( n = 138 ) score = 1 ( n = 49 ) score = 2 ( n = 37 ) score = 3 ( n = 27 ) discussion our data show an increased risk of infertility in childhood cancer survivors starting at a very young reproductive age . 
 however , nearly two - thirds of survivors with clinical infertility reported a pregnancy . than were infertility function , and counselling about treatment for childhood cancer has variable e ects on the reproductive likelihood of fertility in survivors remains challenging . 
 previous studies have characterised risk factors for childlessness or pregnancy , but did not assess a group of women who desired pregnancy and reported an inability to conceive within a year . 
to our knowledge , ours is the rst large study of female childhood cancer survivors to quantify the risk of infertility that is based on a clinical de nition and characterises the use and success of infertility treatments in this setting ( panel )  . survivors who had received radiotherapy to the brain had a signi cantly shorter time to pregnancy than did other survivors . 
survivors who receive high doses of brain radiotherapy might have substantial neurocognitive impairments and be less likely to partner or attempt pregnancy.16 the shortened time to pregnancy in this survivor group in our study is probably a result of selection bias for a good prognosis group that received low dose radiotherapy that did not a ect ovarian reserve . survivors were roughly half as likely to be medically treated for infertility as were their siblings , which is a cause for concern . 
 alternatively , reproductive medicine providers might have been uncomfortable with perceived medical comorbidities . take drugs after previous extensive vol 14 august 2013 articles panel : research in context systematic review we were familiar with previous childhood cancer survivor study work6 about the relative risk of pregnancy in childhood cancer survivors compared with their siblings . 
to our knowledge , no previous studies that included childhood cancer survivors have included direct measures of infertility . interpretation our data support earlier work showing that cancer therapies have negative gonadal e ects on young female cancer survivors , leading to an increased risk of infertility and childlessness . 
our data di er from those from other studies , which suggest that earlier age at cancer diagnosis is protective against the development of infertility , probably because our multivariate models were adjusted for treatment - related factors ( and sociodemographic variables associated with infertility )  . 
we noted an increased risk of infertility in cancer survivors at very young ages , even though most young female cancer survivors resume menstruation ( more than 50% of our cohort was aged < 30 years when they answered questions about infertility ) , showing that menstrual function does not equate to normal fecundity . 
clinicians should alert cancer survivors with ovarian function of the risk of infertility , and refer to reproductive specialists for possible fertility preservation if they are not ready to attempt conception . 
small uterine volumes , impaired blood ow , and endometrial damage might have roles in infertility or adverse pregnancy outcomes ( increased frequency of low birthweights and miscarriage , and fewer livebirths ) in survivors who received uterine radiotherapy.1720 independently of to our knowledge , our study is the most comprehensive investigation into infertility in childhood cancer survivors so far . 
importantly , previous ccss work did not show an overall higher risk of miscarriage or stillbirth in survivors than in their siblings , despite a lower rate of livebirths in survivors . 
additionally , previous reports19 have shown an increased rate of elective terminations in young survivors ( aged 2125 years ) , which lowers the livebirth rate but is not associated with fertility potential . 
women with ovarian failure were not included in the analysis of likelihood of pregnancy , and the proportion of infertile survivors achieving pregnancy would have been lower if that group had been included . 
because of the young age of our cohort ( median 276 years ) and the lower marriage rate in survivors than in their siblings , we might be underestimating the overall burden of infertility in their lifespan . 
previous reports2123 about childhood cancer survivors have shown diminished ovarian reserve even with regular menstruation and timely puberty , and studies15 , 24 of adult cancer survivors have shown that infertility . 
similarly , amenorrhoea underestimates survivors might be at risk for secondary infertility if they want more than one child . another important limitation of these data is that participants answered infertility questions starting in 1992 , when use of assisted reproduction such as in - vitro fertilisation was less common and less successful than it is now . 
 finally , antineoplastic treatments have evolved towards gonad - sparing regimens in some cases , and the late reproductive e ects of such regimens might be less pronounced than those of older regimens . 
however , alkylating agents and pelvic radiation are still used , which emphasises the importance of our analysis , especially in view of advances in reproductive technology . increased reproductive medicine o ers options for fertility preservation before cancer treatment . 
 the american society of clinical oncology recommends that oncologists should refer interested and appropriate patients to reproductive specialists as soon as possible.25 because assisted reproductive outcomes after cancer treatment seem poor , fertility preservation interventions are preferred at diagnosis when possible.26 fertility preservation techniques before ( or early in ) cancer treatment include oophoropexy and cryopreservation of oocytes , ovarian tissue , or embryos , and depend on demographic and clinical factors and resource availability . 
 importantly , multiple livebirths have been reported from ovarian freezing.2729 collaboration between oncologists and reproductive medicine providers might increase timely access to fertility preservation for patients in need and prevent provider bias when treating cancer survivors for infertility . modern tissue 880 vol 14 august 2013 articles contributors seb , jsn , esg , wml , ms , cas , llr , and ld had roles in design and conduct of the study ; collection , management , analysis , and interpretation of data ; and preparation , review , or approval of the article . 
 rew had roles in collection , management , analysis , and interpretation of data and preparation , review , or approval of the article . con icts of interest we declare that we have no con icts of interest . acknowledgments this study was funded by grant u24 ca55727 ( awarded to llr , the principal investigator ) from the us national cancer institute , support to st jude childrens research hospital from the american lebanese syrian associated charities , and support to ld from swim across america . the burden of cancers and their variations across the states of india : the global burden of disease study 19902016 india state - level disease burden initiative cancer collaborators * summary background previous efforts to report estimates of cancer incidence and mortality in india and its different parts include the national cancer registry programme reports , sample registration system cause of death findings , cancer incidence in five continents series , and globocan . 
we present a comprehensive picture of the patterns and time trends of the burden of total cancer and specific cancer types in each state of india estimated as part of the global burden of diseases , injuries , and risk factors study ( gbd ) 2016 because such a systematic compilation is not readily available . methods we used all accessible data from multiple sources , including 42 population - based cancer registries and the nationwide sample registration system of india , to estimate the incidence of 28 types of cancer in every state of india from 1990 to 2016 and the deaths and disability - adjusted life - years ( dalys ) caused by them , as part of gbd 2016 . 
 we present incidence , dalys , and death rates for all cancers together , and the trends of all types of cancers , highlighting the heterogeneity in the burden of specific types of cancers across the states of india . 
we also present the contribution of major risk factors to cancer dalys in india . findings 83% ( 95% uncertainty interval [ ui ] 7986 ) of the total deaths and 50% ( 4655 ) of the total dalys in india in 2016 were due to cancer , which was double the contribution of cancer in 1990 . 
the ten cancers responsible for the highest proportion of cancer dalys in india in 2016 were stomach ( 90% of the total cancer dalys ) , breast ( 82% ) , lung ( 75% ) , lip and oral cavity ( 72% ) , pharynx other than nasopharynx ( 68% ) , colon and rectum ( 58% ) , leukaemia ( 52% ) , cervical ( 52% ) , oesophageal ( 43% ) , and brain and nervous system ( 35% ) cancer . 
among these cancers , the age - standardised incidence rate of breast cancer increased significantly by 407% ( 95% ui 70856 ) from 1990 to 2016 , whereas it decreased for stomach ( 397% ; 343440 ) , lip and oral cavity ( 64% ; 04186 ) , cervical ( 397% ; 265573 ) , and oesophageal cancer ( 312% ; 279349 ) , and leukaemia ( 161% ; 43242 )  . 
we found substantial inter - state heterogeneity in the age - standardised incidence rate of the different types of cancers in 2016 , with a 33 times to 116 times variation for the four most frequent cancers ( lip and oral , breast , lung , and stomach )  . 
tobacco use was the leading risk factor for cancers in india to which the highest proportion ( 109% ) of cancer dalys could be attributed in 2016 . lancet oncol 2018 ; 19 : 1289306 published online september 12 , 2018 s1470 - 2045 ( 18 ) 30447 - 9 see comment page 1260 see online / comment lancet 2018 ; published online sept 12 . 
 s2214 - 109x ( 18 ) 30387 - 5 , s2214 - 109x ( 18 ) 30407 - 8 , and s2214 - 109x ( 18 ) 30409 - 1 see online / articles lancet public health 2018 ; published online sept 12 . 
 s2468 - 2667 ( 18 ) 30138 - 5 * collaborators listed at the end of the article correspondence to : prof lalit dandona , public health foundation of india , gurugram 122002 , national capital region , india lalit.dandona@phfi.org interpretation the substantial heterogeneity in the state - level incidence rate and health loss trends of the different types of cancer in india over this 26 - year period should be taken into account to strengthen infrastructure and human resources for cancer prevention and control at both the national and state levels . 
these efforts should focus on the ten cancers contributing the highest dalys in india , including cancers of the stomach , lung , pharynx other than nasopharynx , colon and rectum , leukaemia , oesophageal , and brain and nervous system , in addition to breast , lip and oral cavity , and cervical cancer , which are currently the focus of screening and early detection programmes . funding bill & melinda gates foundation ; and indian council of medical research , department of health research , ministry of health and family welfare , government of india . copyright the author ( s )  . 
we found a wide variety of valuable data for cancer distribution in india and several states , but no studies that comprehensively described incidence , prevalence , mortality , and disability - adjusted life - years ( dalys ) for all cancer types in every state of india over a long period of time . added value of this study to our knowledge , this is the first report to produce comprehensive estimates of incidence , prevalence , mortality , and dalys for 28 types of cancers in every state of india over 26 years from 1990 to 2016 . 
this analysis was part of the global burden of diseases , injuries , and risk factors study 2016 that assessed all causes of disease burden , using data from all accessible sources . 
this study estimates that while the agestandardised incidence rate of all cancers considered together has not changed substantially in india during this 26 - year period , the proportion of total disease burden caused by cancers has doubled . 
this study reports the substantial heterogeneity in the incidence , mortality , and dalys of different cancers across the states of india and documents that tobacco use is the highest contributing risk to cancer burden in india . implications of all the available evidence this systematic and comprehensive description of the variations in the distribution and trends of cancer types in different parts of the country can serve as a useful reference for further planning of prevention and management of cancer across india . 
more large - scale collaborative research is needed to understand the reasons behind the changing trends of the different types of cancers in india . types of cancers in each state of india is not readily available . 
this is needed to inform action for cancer control that is commensurate with the need in each state , since delivery of health care is a state subject in india . the united nations sustainable development goals target the reduction of premature mortality from non - communicable diseases , which includes cancer , by one - third by 2030 through prevention and treatment.21 the national cancer registry programme in india was established in 1981 to generate data on the magnitude and patterns of cancer through population - based registries.22 , 23 the number of registries has grown under this programme , and other population - based registries have also been started in recent years.22 however , many populous states have no cancer registries yet , and most registries in india are in urban areas , leading to difficulties in assessing population - level cancer burden trends in all parts of the country . the india state - level disease burden initiative is a collaboration with the global burden of diseases , injuries , and risk factors study ( gbd ) to produce subnational disease burden estimates for india . 
this initiative recently reported the variable health transition across the states of india from 1990 to 2016 based on analysis done as part of gbd 2016.4 , 24 here , we report detailed trends of the incidence and health loss due to each type of cancer in every state of india from 1990 to 2016 . methods overview the india state - level disease burden initiative recently reported the overall trends of diseases , injuries , and risk factors from 1990 to 2016 for every state of india.4 , 24 this analysis was done as part of gbd 2016 , which estimated disease burden due to 333 diseases and injuries and 84 risk factors in all age groups using all accessible data from multiple sources . 
the india state - level disease burden initiative was supported by the efforts of several expert groups and a vast network of collaborators to identify and access all available data sources , assess their scope and quality for inclusion , and participate in the analysis and interpretation of the findings . 
the health ministry screening committee at the indian council of medical research and the ethics committee of the public health foundation of india approved the work of this initiative . estimation of cancer burden a detailed description of methods to estimate cancer mortality , incidence , prevalence , and disability - adjusted life - years ( dalys ) , and the analytical approaches used in gbd 2016 have been reported elsewhere , and are summarised in the appendix ( pp 316 ) .1 , 2529 briefly , the major data inputs to determine cancer mortality in india included the nationwide sample registration system ( srs ) cause of death data , the medically certified cause of death data , and 42 population - based cancer registries ( appendix pp 68 )  . 
srs verbal autopsy cause of death data on 455 460 deaths covering the rural and urban populations of every state of india from 2004 to 2013 were included.4 for states with at least one population - based cancer registry , the incidence data were trans formed to mortality by multiplying incidence data with an independently modelled urban or rural mortality - incidence ( mi ) ratio for the respective states . 
 cancer registry data were used as the gold - standard against which other data sources ( srs or medically see online for appendix 1290 vol 19 october 2018 articles substantially sources differed certified cause of death data ) were compared . 
if the from other data the registry data , they were excluded.1 , 30 because of limitations associated with the medically certified cause of death mortality data , these were used only when the cancer type was not captured by the srs cause of death data . 
 the codcorrect algorithm was used to adjust cancer subtypes to the parent cause and to adjust the sum of predicted deaths from these models for each type of cancers in an agesexstateyear group to be consistent with the results from all - cause mortality estimation . the estimation of cancer incidence was driven by registry data from india . 
the mortality estimates that were derived from transformation of incidence data using the mi ratios , as noted above , were transformed back to incidence after the codem and codcorrect model adjustments.1 10 - year cancer prevalence was estimated by modelling survival using the mi ratio as a surrogate for access to cancer care . 
lifetime prevalence was only estimated for 10 years post incidence1 and for long - term sequelae from procedures ( mastectomy , laryngectomy , stoma , incontinence cystectomy , and prostatectomy )  . 
dalys , a summary measure of total health loss , were computed by adding ylls and ylds for each cancer type for location , year , age and sex.1 , 28 the appendix provides a list of data inputs used for these estimations ( pp 1729 )  . a description of estimation of risk factor exposure and its contribution to disease burden in gbd is available elsewhere.29 briefly , this includes determination of risk exposure and disease outcome pairs based on available evidence and inclusion criteria , assessment of risk exposure from all accessible data sources , and estimation of disease burden attributable to risks based on published relative risks . 
estimates of dalys for specific types of cancers that were attributable to each risk factor were produced by location , age , sex , and year . gbd uses covariates , which are explanatory variables that have a known association with the outcome of interest , to arrive at the best possible estimate of the outcome of interest when data for the outcome are scarce but data for the covariates are available.2529 this approach was part of the estimation process for the findings presented in this report . analysis presented in this paper the findings are reported for 31 geographical units in india : 29 states , union territory of delhi , and the union territories other than delhi ( combining the six smaller union territories of andaman and nicobar islands , chandigarh , dadra and nagar haveli , daman and diu , lakshadweep , and puducherry )  . 
for trends from 1990 onwards , the data for these four new states were disaggregated from their parent states on the basis of data from the districts that now constitute these states . 
 the findings are also presented for four groups of states based on epidemiological transition level ( etl ) as described previously.4 briefly , the etl state groups were defined on the basis of the ratio of dalys from communicable , maternal , neonatal and nutritional diseases to those from non - communicable diseases and injuries combined in 2016 , with a relatively lower ratio indicating higher etl : level etl state group ( ratio 056075 ) , lower - middle etl state group ( 041055 ) , higher - middle etl state group ( 031040 ) , and high etl state group ( less than 031 )  . 
we have reported previously that epidemiological transition ratios of the states of india have a significant inverse relation with the socio - demographic index calculated by the gbd study and based on income , education , and fertility levels , which indicates broad correspondence of etl groups with sociodemographic development levels.4 low we present trends of incidence ( new cases in a year ) , mortality , and dalys due to all cancers together and different types of cancers from 1990 to 2016 for every state of india . 
we regarded dalys as the main metric for disease burden because it includes both mortality and morbidity and is recommended by the national health policy of india for tracking disease burden.31 first , we present the 1990 to 2016 trends for the overall burden from all cancers together in terms of dalys , followed by incidence and deaths . 
we also describe briefly another six cancer types that are among the ten leading incident cancers in females or males in india in 2016 , which are not included in the previous ten cancers causing the highest dalys . 
 we present both crude and age - standardised rates , since crude rates provide the actual situation in each state that vol 19 october 2018 1291 articles 1990 jammu and kashmir ( 691 ) punjab ( 580 ) haryana ( 710 ) himachal pradesh ( 698 ) uttarakhand ( 693 ) delhi ( 646 ) sikkim ( 678 ) arunachal pradesh ( 759 ) rajasthan ( 588 ) uttar pradesh ( 720 ) bihar ( 449 ) assam ( 687 ) nagaland ( 631 ) manipur ( 481 ) mizoram ( 891 ) jharkhand ( 580 ) odisha ( 686 ) meghalaya ( 690 ) tripura ( 529 ) west bengal ( 639 ) chhattisgarh ( 588 ) incidence rate per 100 000 105 901049 75899 60749 45599 449 himachal pradesh ( 916 ) uttarakhand ( 910 ) delhi ( 1029 ) sikkim ( 744 ) arunachal pradesh ( 785 ) rajasthan ( 726 ) uttar pradesh ( 790 ) bihar ( 539 ) assam ( 902 ) nagaland ( 703 ) manipur ( 643 ) mizoram ( 1217 ) jharkhand ( 643 ) odisha ( 836 ) meghalaya ( 814 ) tripura ( 690 ) west bengal ( 854 ) chhattisgarh ( 820 ) gujarat ( 555 ) madhya pradesh ( 694 ) maharashtra ( 620 ) karnataka ( 762 ) telangana ( 549 ) andhra pradesh ( 581 ) ( 525 ) tamil nadu ( 589 ) kerala ( 741 ) 2016 punjab ( 855 ) haryana ( 1033 ) jammu and kashmir ( 792 ) gujarat ( 758 ) madhya pradesh ( 831 ) maharashtra ( 802 ) telangana ( 726 ) andhra pradesh ( 766 ) goa ( 970 ) karnataka ( 1016 ) tamil nadu ( 829 ) kerala ( 1353 ) is preferred by policy makers , and age - standardised rates allow comparisons over time and between states after adjusting for the differences in the age structure of the population . 
 these were based on 1000 runs of the models for each quantity of interest , with the mean considered as the point estimate and the 25th and 975th percentiles considered as the 95% ui ( appendix p 15 ) .2528 role of the funding source some staff of the indian council of medical research are co - authors on this paper as they contributed to various aspects of the study and analysis . 
 the corresponding author had full access to all of the data in the study and had final responsibility for the decision to submit for publication . results all cancers together contributed 50% ( 95% ui 4655 ) of the total dalys and 83% ( 7986 ) of the total deaths in india in 2016 , an increase of 909% and 1128% respectively from 1990 . 
the crude cancer daly rate in india increased by 253% ( 168342 ) from 1990 to 2016 , but the age - standardised cancer daly rate did not change substantially during the same period.32 the agestandardised cancer daly rate had a 26 times variation across the states of india in 2016 ( appendix p 30 )  . 
the highest crude cancer daly rates in 2016 were in the states of mizoram , kerala , assam , haryana , and meghalaya , and the highest age - standardised rates were in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam ( appendix p 30 )  . to 1 069 000 ( 1 043 0001 101 000 ) the estimated number of incident cancer cases in india increased from 548 000 ( 95% ui 520 000576 000 ) in 1990 in 2016 ( appendix p 31 )  . 
the crude cancer incidence rate in india increased by 282% ( 95% ui 199355 ) from 634 per 100 000 in 1990 to 812 per 100 000 in 2016 , but there was no change in the age - standardised incidence rate ( appendix p 32 )  . 
crude cancer incidence rate was highest in kerala and mizoram , followed by haryana , delhi , karnataka , goa , himachal pradesh , uttarakhand , and assam ( figure 1 , appendix p 30 )  . 
age - standardised incidence rates were highest in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam , figure 1 : crude annual incidence rate of all cancers together in the states of india , 1990 and 2016 the states of chhattisgarh , jharkhand , telangana , and uttarakhand did not exist in 1990 , as they were created from existing larger states in 2000 or later . 
crude cancer incidence rate increased substantially from 1990 to 2016 in all etl state groups , with the highest increase in the high etl group ( appendix p 32 )  . the number of deaths due to cancer in india increased from 382 000 ( 95% ui 351 000412 000 ) in 1990 to 813 000 ( 767 000850 000 ) in 2016 ( appendix p 31 )  . 
the crude cancer death rate in india in 2016 was 618 ( 95% ui 583646 ) per 100 000 , as compared with 442 ( 406477 ) in 1990 ( appendix p 32 )  . 
male cancer patients had a 123% ( 95% ui 29233 ) increase in agestandardised death rate over the 26 - year time period , whereas no substantial changes over time were found in female cancer patients ( appendix p 32 )  . 
the crude death rate for both sexes combined was highest in mizoram , kerala , and haryana in 2016 , followed by assam , karnataka , odisha , uttarakhand , meghalaya , and himachal pradesh ( appendix pp 30 , 33 )  . 
the agestandardised death rates were highest in the northeast states of mizoram , meghalaya , arunachal pradesh , and assam ( appendix p 30 )  . the crude cancer mi ratio in india in 2016 was 076 ( 95% ui 072079 )  . 
the mi ratio was higher in low and lower - middle etl state groups than the high and higher - middle etl groups in 2016 ( figure 2 )  . 
the mi ratio for males was more than 080 in all states from the low etl group and most of the lower - middle etl states , with a higher ratio in odisha in low etl , and mizoram and arunachal pradesh in the lower - middle etl state group in 2016 . 
the mi ratio was below 080 for females in most of the states in india in 2016 , except for bihar and meghalaya . the leading types of cancer in india in 2016 , those responsible for more than 5% of the total cancer dalys among both sexes combined , were stomach cancer ( 90% ) , breast cancer ( 82% ) , lung cancer ( 75% ) , lip and oral cavity cancer ( 72% ) , pharynx cancer other than nasopharynx ( 68% ) , colon and rectum cancer ( 58% ) , leukaemia ( 52% ) , and cervical cancer ( 52% ; figure 3 )  . 
the age - standardised daly rate increased significantly in india from 1990 to 2016 for liver cancer ( 512% ; 95% ui 240659 ) , non - hodgkin lymphoma ( 354% ; 207488 ) , ovarian cancer ( 281% ; 151443 ) and myeloma ( 282% ; 56631 )  . 
 age - standardised daly rates from 1990 to 2016 was highest for testicular cancer ( 592% ; 538654 ) and hodgkins lymphoma ( 548% ; 396625 ) , followed by cervical ( 387% ; 230563 ) , nasopharynx ( 335% ; 198461 ) , larynx ( 316% ; 257367 ) , uterine ( 315% ; 178400 ) , and stomach cancer ( 314% ; 237373 )  . 
the highest cancer dalys among males in india in 2016 were due to lung cancer , followed by lip and oral cavity cancer , other pharynx cancer , and stomach cancer ( figure 3 )  . among both boys and girls aged 014 years , leukaemia was responsible for the highest dalys in india in 2016 , followed by brain and nervous system cancer ( figure 5 , appendix pp 3440 )  . 
daly rates for lung cancer and stomach cancer increased in males after the age of 35 years in 2016 , while prostate cancer increased after the age of 50 years . tobacco use , alcohol use , and dietary risks were estimated by gbd to contribute the highest cancer dalys in 2016 ; they were responsible for 109% , 66% and 60% of the total cancer dalys , respectively ( appendix pp 4142 )  . stomach cancer the estimated number of incident stomach cancer cases in india in 2016 was 75 000 ( 95% ui 73 00078 000 ) and the prevalent cases were 112 000 ( 109 000116 000 ; appendix p 31 )  . 
there was a substantial reduction in the age - standardised incidence rate of stomach cancer ( 397% ; 95% ui 343440 ) from 1990 to 2016 in india ( figure 6 )  . 
in 2016 , stomach cancer was the first or second highest cause of cancer deaths in 15 states for females and in 18 states for males ( figure 8 )  . 
only a small proportion of the stomach cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( dietary risks [ 41% ] and smoking [ 35% ] ; appendix pp 4142 )  . breast cancer the estimated number of incident breast cancer cases in india in 2016 was 118 000 ( 95% ui 107 000130 000 ) , 981% of which were in females , and the prevalent cases were 526 000 ( 474 000574 000 ; appendix p 31 )  . 
breast cancer is the leading cancer in indian females , accounting for the largest crude incidence rate and prevalence of any cancer type ( appendix pp 49 , 50 )  . 
over the 26 - year period , the agestandardised incidence rate of breast cancer in females increased by 391% ( 95% ui 51855 ) from 1990 to 2016 , with increase observed in every state of the country ( appendix pp 51 )  . 
the highest crude daly rates for breast cancer were in kerala , punjab , and tamil nadu in the high etl state group , followed by delhi , maharashtra , karnataka , and haryana in the higher - middle etl group . 
only a small proportion of breast cancer dalys in india in 2016 could be attributed to risk factors included [ 49% ] and in gbd ( high fasting plasma glucose secondhand smoke [ 24% ] ; appendix pp 4142 )  . lung cancer we refer to tracheal , bronchus , and lung cancer as lung cancer in this report for simplicity . 
the number of vol 19 october 2018 1295 articles a females b males 8000 7000 6000 5000 4000 3000 2000 1000 8000 7000 6000 5000 4000 3000 2000 1000 bladder cancer brain and nervous system cancer breast cancer cervical cancer colon and rectum cancer gallbladder and biliary tract cancer hodgkins lymphoma kidney cancer larynx cancer leukaemia lip and oral cavity cancer liver cancer lung cancer malignant skin melanoma mesothelioma multiple myeloma nasopharynx cancer non - hodgkin lymphoma non - melanoma skin cancer oesophageal cancer pharynx cancer other than nasopharynx ovarian cancer pancreatic cancer stomach cancer thyroid cancer uterine cancer bladder cancer brain and nervous system cancer breast cancer colon and rectum cancer gallbladder and biliary tract cancer hodgkins lymphoma kidney cancer larynx cancer leukaemia lip and oral cavity cancer liver cancer lung cancer malignant skin melanoma mesothelioma multiple myeloma nasopharynx cancer non - hodgkin lymphoma non - melanoma skin cancer oesophageal cancer pharynx cancer other than nasopharynx pancreatic cancer prostate cancer stomach cancer testicular cancer thyroid cancer 1014 1519 2024 2529 3034 3539 4044 4549 5054 5559 6064 6569 7074 7579 age range ( years ) figure 5 : age - specific dalys for different types of cancers by sex in india , 2016 dalys = disability - adjusted life - years . incident lung cancer cases in india in 2016 was 67 000 ( 95% ui 63 00072 000 ) , 722% of which were in males , and the prevalent cases were 74 000 ( 70 00080 000 ; appendix p 31 )  . 
the crude lung cancer incidence rate in males was highest in kerala and mizoram , and in females was highest in mizoram and manipur ( appendix pp 49 , 50 )  . 
there was a substantial reduction in the age - standardised incidence rate of lip and oral cavity cancer ( 64% ; 95% ui 04186 ) from 1990 to 2016 in india ( figure 6 )  . 
the age - standardised incidence rate for lip and oral cavity cancer varied 51 times among both sexes combined across the states of india in 2016 ( appendix pp 4348 )  . 
smokeless tobacco , alcohol use and smoking were the leading risk factors in gbd for lip and oral cavity cancer in india in 2016 to which 332% , 298% , and 209% of the lip and oral cavity cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . pharynx cancer other than nasopharynx the number of incident pharynx cancer other than nasopharynx cases in india in 2016 was 65 000 ( 95% ui 58 00070 000 ) , 702% of which were in males , and the prevalent cases were 152 000 ( 137 000163 000 ; appendix p 31 )  . 
the age - standardised incidence rate for other pharynx cancer varied 98 times for both sexes combined across the states of india in 2016 ( appendix pp 4348 )  . 
alcohol use was the leading risk factor in gbd for other pharynx cancer in india in 2016 to which 30.1% of the other pharynx cancer dalys could be attributed ( appendix pp 41 , 42 )  . colon and rectum cancer the number of incident colon and rectum cancer cases in india in 2016 was 63 000 ( 95% ui 58 00066 000 ) and the prevalent cases were 185 000 ( 171 000195 000 ; appendix p 31 )  . 
colon and rectum cancer incidence rate in both sexes was higher in the high etl as compared with other etl state groups ( appendix pp 49 , 50 )  . 
dietary risks were the leading risk factor in gbd for colon and rectum cancer in india in 2016 to which 432% of the colon and rectum cancer dalys could be attributed ( appendix pp 41 , 42 )  . leukaemia the number of incident leukaemia cancer cases in india in 2016 was 34 000 ( 95% ui 30 00038 000 ) and the prevalent cases were 105 000 ( 96 000120 000 ; appendix p 31 )  . 
among children aged 014 years , leukaemia was responsible for the highest proportion of the cancer dalys ( 346% ) in india in 2016 , which was similar among boys and girls ( figure 5 , appendix pp 3440 )  . 
in males , leukaemia was the third and fifth leading cause of cancer deaths in delhi and punjab respectively in 2016 , but lower in other states ( figure 8 )  . cervical cancer cervical cancer was the second most common cancer in females in india in 2016 , with 77 000 ( 95% ui 68 00096 000 ) incident cervical cancer cases in india in 2016 and 288 000 ( 247 000342 000 ) prevalent cases ( appendix p 31 )  . 
it is important to note that other unknown risk factors could also be contributing to cervical cancer as the population - attributable fractions of different risks can add up to more than 100% . vol 19 october 2018 1299 articles for rate cancer oesophageal oesophageal cancer the number of incident oesophageal cancer cases in india in 2016 was 37 000 ( 95% ui 36 00038 000 ) , 608% of which were in males , and the prevalent cases were 41 000 ( 39 00042 000 ) ( appendix p 31 )  . 
there was a substantial reduction in the age - standardised incidence rate of oesophageal cancer ( 312% ; 95% ui 279349 ) in india from 1990 to 2016 ( figure 6 )  . 
smokeless tobacco , dietary risks , and smoking were the leading risk factors in gbd for oesophageal cancer in india in 2016 to which 226% , 215% , and 174% of the oesophageal cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . brain and nervous system cancer the number of incident brain and nervous system cancer cases in india in 2016 was 23 000 ( 95% ui 21 00028 000 ) and the prevalent cases were 49 000 ( 44 00057 000 ; appendix p 31 )  . 
among children aged 014 years , brain and nervous system cancer was responsible for the second highest proportion of the cancer dalys ( 16% ) in india in 2016 , which was similar among boys and girls ( figure 5 , appendix pp 3440 )  . 
the daly rate for brain and nervous system cancer was highest in delhi followed by sikki the ranking of deaths due to brain and nervous system cancer was relatively low in all states as compared with the other high burden cancers ( figure 8 )  . 
 prostate cancer prostate cancer had the fifth highest incidence rate among males in india in 2016 ( 48 per 100 000 , 95% ui 3858 ) , with 33 000 ( 26 00040 000 ) incident cases and 112 000 ( 87 000137 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
there were 31 000 ( 95% ui 30 00033 000 ) incident cases in india , of which 835% were in males , and there were 96 000 ( 93 000100 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
the crude incidence rate for larynx cancer in males was highest in kerala in 2016 , followed by delhi , haryana , and assam ( appendix p 50 )  . 
smoking and alcohol use were the leading risk factors in gbd for larynx cancer in india in 2016 to which 379% and 172% of the larynx cancer dalys could be attributed , respectively ( appendix pp 41 , 42 )  . liver cancer liver cancer had the ninth highest incidence rate among males in 2016 in india ( 31 per 100 000 , 95% ui 29 32 )  . 
 there were 30 000 ( 95% ui 29 00032 000 ) incident cases in india , of which 689% were in males , and 12 000 ( 11 00014 000 ) prevalent cases ( appendix pp 31 , 50 )  . 
the crude incidence rate for liver cancer in males in 2016 was highest in arunachal pradesh , followed by kerala , sikkim , and mizoram ( appendix p 50 )  . 
 to 2016 the sixth highest ovarian cancer ovarian cancer had incidence rate among females in 2016 in india ( 40 per 100 000 , 95% ui 3743 ) , with 26 000 ( 95% ui 24 00027 000 ) incident cases and 76 000 ( 69 00080 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
only a small proportion of the ovarian cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( high fasting plasma glucose [ 55% ] ; appendix pp 41 , 42 )  . gallbladder and biliary tract cancer gallbladder and biliary tract cancer had the ninth highest incidence rate among females in 2016 in india ( 26 per 100 000 , 95% ui 2328 )  . 
there were 26 000 ( 95% ui 23 00029 000 ) incident cases in india , of which 644% were in females , and there were 21 000 ( 18 00023 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
the crude incidence of gallbladder and biliary tract cancer in females 1300 vol 19 october 2018 articles was highest in the states of assam and delhi in 2016 ( appendix p 49 )  . 
91% of the gallbladder and biliary tract cancer dalys in india in 2016 could be attributed to high body - mass index in gbd ( appendix pp 41 , 42 )  . thyroid cancer thyroid cancer had the tenth highest incidence rate among females in 2016 in india ( 25 per 100 000 , 95% ui 2326 )  . 
there were 21 000 ( 95% ui 20 00023 000 ) incident cases in india , of which 743% were in females , and there were 106 000 ( 101 000115 000 ) prevalent cases ( appendix pp 31 , 49 )  . 
the crude incidence rate of thyroid cancer was highest in females in kerala , followed by sikkim , nagaland , and goa in 2016 ( appendix p 49 )  . 
 only a small proportion of the thyroid cancer dalys in india in 2016 could be attributed to risk factors included in gbd ( high body - mass index [ 51% ] ; appendix pp 41 , 42 )  . discussion the number of new cases and deaths due to cancer doubled in india from 1990 to 2016 , as did the proportional contribution of cancers to the total dalys and deaths in the country . 
however , there was no change in the age - standardised rates for both sexes combined , highlighting the contribution of ageing and population growth to the increasing cancer burden of the country . 
 males had higher mi ratios than females in every state of the country . the trends observed in sex - specific and cancer typespecific incidence rates over time in india are likely due to a variety of factors , such as population ageing , changes in cancer literacy , detection , health - care access , and a variety of risk factors . 
the substantial decrease in the age - standardised incidence rate of stomach cancer across the country might be due to lifestyle changes such as reduced consumption of salt - preserved foods , better availability of refrigeration , and increasing fruit con sumption , and to decreases in smoking prevalence.3234 the prevalence of helicobacter pylori remains persistently high in indians , 35 and hence this is an unlikely factor in the decreasing incidence of stomach cancer . 
for breast cancer , a substantial increase in age - standardised incidence rate is consistent with changes in some risk factors over time in india , such as later age at first birth , lower parity , and increase in overweight and obesity.32 , 36 , 37 the substantial decrease in the age - standardised incidence rate of oesophageal cancer might be partly due to the decrease in smoking prevalence over the 26 - year period and in smokeless tobacco use over the past 10 years.32 , 34 the absence of change in the age - standardised incidence rate of lung cancer in india might be related to the mixed trends of its major risk factors , which include decrease in smoking and household air pollution but an increase in ambient air pollution , but also due to the patterns of other unknown risk factors.32 , 34 the small decrease in the age - standardised incidence rate of lip and oral cavity cancer in india could be related to the reduction in use of smokeless tobacco in india during the past decade.32 the decreasing age - standardised incidence rate of cervical cancer could be inversely related to the reproductive risk factors mentioned for breast cancer increase above.36 in the absence of systematic human papilloma virus ( hpv ) testing in india , there is no evidence of changing seroprevalence of hpv and its subtypes over time in india . 
leukaemia has been associated with genetic , infectious , and environmental risks , 38 but the reasons for the substantial reduction in its age - standardised incidence rate in india from 1990 to 2016 are unclear . the interplay of the trends of the two risk factors to which the highest proportion of cancer dalys in india could be attributed , tobacco and alcohol , is interesting in relation to the trends of some of the leading cancers . 
while tobacco use in india has decreased during this period , alcohol use has increased.32 the drop in incidence rate of lip and oral cavity , oesophageal , and larynx cancers could be partly related to a larger influence of tobacco than alcohol on these cancers , and the increase in incidence rate of liver cancer could be partly related to a larger influence of alcohol than tobacco on this cancer , in addition to the trends of yet unknown other risk factors contributing to all of these cancers . 
collaborative multi - institutional research efforts on cancer risk factors can help address such knowledge gaps , as well as lead to a better understanding of the reasons for the substantial decreases or increases in the incidence of different types of cancers in different parts of india . 
detailed decomposition analyses are needed to tease apart the contribution of population structure changes , risk factors , interventions , and other determinants to the trends of leading cancers in india . the heterogeneity of the incidence rate of different types of cancers across india is vast . 
major variations exist even within the same geographical region , such as neighbouring states in the northeastfor example , a 15 times difference in age - standardised incidence rates of naso pharynx cancer between the neighbouring north - eastern states of nagaland and tripura . 
the states in the northeast of vol 19 october 2018 1301 articles india generally have high tobacco use as well as a high incidence of lung , oesophageal , nasopharynx and other pharynx cancers that are associated with tobacco use . 
 there are also unique tobacco consumption patterns in these states , such as use of tobacco - infused water in mizoram.39 , 40 hpv and cervical cancer are both high in dindigul in tamil nadu , 41 consumption of smoked or preserved meats and stomach cancer are high in mizoram , 42 and delayed childbearing and lower parity are high in kerala as is breast cancer.43 the many variations between the states indicate the need for state - specific approaches for cancer control . 
if the reasons for the heterogeneous distribution of the major cancer types in different parts of india are understood better through large - scale collaborative research , this knowledge could help plan more specific efforts to reduce the cancer burden across the states of india . the national cancer control programme was initiated by the government of india in 1975 to equip tertiary care cancer hospitals and institutions to implement systematic , equitable , and evidence - based strategies for prevention , early detection , diagnosis , treatment , and palliation , using available resources.44 state cancer institutes and tertiary care cancer centres have been established under this programme that are responsible for improved cancer awareness and management at the state level.45 despite these attempts , access to critical cancer treatment is low in the country . 
for example , availability of radiotherapy machines is poor , there are delays in treatment , and there is geographic inequity in the distribution of such resources.10 , 11 , 46 with the launch of the national programme for control of cancer , diabetes , cvd and stroke in 2010 in india , the cancer control efforts are now part of this umbrella programme for noncommunicable diseases.47 the national programme aims to tackle cancer by addressing preventable common risk factors through community - level , cost - effective screening for high - burden cancers , which include clinical breast examination for breast cancer , visual inspection with acetic acid for cervical cancer and visual examination for oral cancers.14 however , there are many challenges with these efforts , including difficulties with trained human resources , follow - up of positive tests , timely diagnosis , and well - tracked referral pathways.48 additionally , there are limited population - level screening modalities available for some of the cancers responsible for the highest cancer burden in india , such as stomach and lung cancers . 
for secondary prevention , less invasive tests for h pylori may offer cost - effective first - line tests for referrals to more invasive endoscopic tests for early detection of stomach cancer.49 faecal occult blood testing as a non - invasive , cost - effective approach to screen for colorectal cancer should also be considered.50 ideally , national and state - level efforts should coordinate to facilitate the development of a prevention - to - palliation system of upward referral for early confirmatory diagnosis and prompt treatment of cancers , and downward referral for adequate follow - up , including palliative care and pain relief . 
india pioneered the establishment and expansion of the national cancer registry programme ( ncrp ) under the indian council of medical research through a network of cancer registries during the past 30 years , which now covers 23 states and union territories.23 the gbd methods rely substantially on the ncrp data from india , but they also use data from all accessible data sources , including some registries that are not part of the ncrp , cause of death data from the 1302 vol 19 october 2018 articles srs and other sources , and a variety of covariates to arrive at the best possible estimates for states where registries do not exist . 
accordingly , differences are expected between the gbd estimates and the statistics reported by the ncrp , which are based entirely on population - based registries.23 the objectives and advantages of the gbd and ncrp approaches are complementary . 
while the ncrp adheres to a standardised methodology established by whos international agency for research in cancer , the gbd methodology provides a standardised approach that also incorporates other sources of data for estimations for all states of india , including those where registries do not exist such as the populous states of bihar , chhattisgarh , jharkhand , and uttar pradesh . 
the gbd methodology is integrated into a larger total disease framework estimation process that allows comparison of the cancer burden to that of other diseases , which has helped to highlight the increasing contribution of cancers to the disease burden in india over the past quarter century . 
it has also further highlighted the need to establish cancer registries in large states of north india where none exist , as well as adequate coverage of rural populations . the limitations of the findings in this report include the general limitations of the gbd approach that are described elsewhere.1 , 2528 input data used to generate cancer mortality can be biased in multiple ways.1 a high proportion of ill - defined cancer cases in the registry data or ill - defined causes of death in mortality data sources require redistribution of these cases , which can introduce bias . 
underreporting of cancers that require advanced diagnostic techniques ( eg , leukaemia , brain , pancreatic , and liver cancer ) can be an issue in data from areas where access to these technologies is scarce . 
in addition , risk factors for breast and cervical cancer that are related to reproductive history in women , such as age at first birth and parity , are not yet included in the gbd risk factor assessment . 
a specific limitation for india is an inadequate cause of death reporting as part of the vital registration system , which reports medically certified cause of death only for a small proportion of deaths in india so far , with variable coverage across the states . 
the srs provides cause of death data using verbal autopsy for all states in india , which is a reasonable alternative data source when the cause - specific data are not fully available from vital registration systems.4 however , this situation highlights the need to improve vital registration and improve training to code cause of death across india . 
the absence of population - based registries in major populous states of north india such as bihar and uttar pradesh leaves open questions about the magnitude of some cancers such as gallbladder cancer , which are expected by the india cancer community to be high there , but this cannot be substantiated yet because of the paucity of population - level evidence . 
in cancer datascarce locations , the estimates for the types of cancer were calculated using covariates , which are explanatory variables with a causal relation to cancer incidence and mortality.1 the strengths of the findings presented in this report were the use of standardised gbd methodology and inclusion of all accessible data from multiple sources , and the substantial contribution of a large network of cancer experts from india in the analysis and inter pretation of the findings . in conclusion , the detailed epidemiology of 28 types of cancer in every state of india over a quarter century described the substantial this report highlights variations between the states for the different types of cancer , and can serve as a useful reference for more targeted planning of cancer control that is commensurate with the trends of different cancers in each state of india . 
 the increasing overall contribution of cancer to disease burden in india should motivate more systematic and large - scale approaches to reduce this burden at the population level across the country . 
these efforts should include improved human resources and infrastructure for prevention , screening , treatment , and palliative care for cancers , as well as adequate financial protection for cancer care . 
these approaches should focus at least on the ten cancers that contribute the highest dalys in indiaie , stomach , breast , lung , lip and oral cavity , pharynx other than nasopharynx , colon and rectum , leukaemia , cervical , oesophageal , and brain and nervous system cancers . 
all authors agreed with the final version of the report . declaration of interests pma , an , rm , dks , rsd , tk , rnv , jkc , mc , pd , jm , sp , ksa , kv , and ss are or have been employees of the indian council of medical research , which partly funded this research . 
all other authors declare no competing interests . acknowledgments the research reported in this publication was funded by the bill & melinda gates foundation and the indian council of medical research , department of health research , government of india . 
 the content of this publication is solely the responsibility of the authors and does not necessarily represent the official views of the bill & melinda gates foundation or the government of india . 
 we gratefully acknowledge the ministry of health and family welfare of the government of india for its support and encouragement of the india state - level disease burden initiative , the governments of the states of india for their support of this work , the many institutions across india that contributed valuable data to the national cancer registry programme and to the other cancer registries , the valuable guidance of the advisory board of this initiative , and the large number of staff at the indian council of medical research , public health foundation of india and the institute for health metrics and evaluation for their contribution to various aspects of the work of this initiative . corrections correction to lancet oncol 2015 ; 16 : 522 correction to lancet oncol 2016 ; 17 : 553 correction to lancet oncol 2016 ; 17 : 733 philip , pa . 
 this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . eggermont amm , chiarion - sileni v , grob j - j , et al . 
this correction has been made to the online version as of june 1 , 2016 . correction to lancet oncol 2016 ; 17 : 751 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . vol 17 june 2016 e223 articles validation of gene signatures that predict the response of breast cancer to neoadjuvant chemotherapy : a substudy of the eortc 10994 / big 00 - 01 clinical trial herv bonnefoi , anil potti , mauro delorenzi , louis mauriac , mario campone , michle tubiana - hulin , thierry petit , philippe rouanet , jacek jassem , emmanuel blot , vronique becette , pierre farmer , sylvie andr , chaitanya r acharya , sayan mukherjee , david cameron , jonas bergh , joseph r nevins , richard d iggo summary background we have previously described gene - expression signatures that predict growth inhibitory and cytotoxic e ects of common chemotherapeutic drugs in vitro . 
the aim of this study was to con rm the validity of these geneexpression signatures in a large series of patients with oestrogen - receptor - negative breast tumours who were treated in a phase iii neoadjuvant clinical trial . 
 methods this trial compares a non - taxane regimen ( uorouracil , epirubicin , and cyclophosphamide [ fec ] for six cycles ) with a taxane regimen ( docetaxel for three cycles followed by epirubicin plus docetaxel [ tet ] for three cycles ) in women with oestrogen - receptor - negative breast cancer . 
pathological complete response , de ned as complete disappearance of the tumour with no more than a few scattered tumour cells detected by the pathologist in the resection specimen , was used to assess chemosensitivity . 
this study is registered on the clinical trials site of the us national cancer institute website findings of 212 patients with oestrogen - receptor - negative tumours assessed , 87 patients were excluded . 
125 oestrogenreceptor - negative tumours ( 55 that showed pathological complete responses ) were tested : 66 in the fec group ( 28 that showed pathological complete responses ) and 59 in the tet group ( 27 that showed pathological complete responses )  . 
the fec predictor had a sensitivity of 96% ( 27 of 28 patients [ 95% ci 8299 ] ) , speci city of 66% ( 25 of 38 patients [ 5079 ] ) , positive predictive value ( ppv ) of 68% ( 27 of 40 patients [ 5280 ] ) , and negative predictive value ( npv ) of 96% ( 25 of 26 patients [ 8199 ] )  . 
analysis of tumour size , grade , nodal status , age , and regimen - speci c signatures showed that the genomic signatures were the only independent variables predicting pathological complete response at p < 001 . 
the high npv of both signatures may allow early selection of patients with breast cancer who should be considered for trials with new drugs . introduction systemic chemotherapy for the treatment of breast cancer improves overall survival , whether given preoperatively or as postoperative adjuvant treatment.1 newer chemotherapy regimens containing taxanes further improve survival compared with standard regimens , 2 but taxanes are expensive , toxic , and might bene t only a small number of patients . 
several single - arm neoadjuvant chemotherapy trials have reported geneexpression signatures obtained from tumour biopsies taken at diagnosis.39 most of these studies described signa tures that predict clinical or pathological response , although one failed to identify any genes that predicted response.9 these studies have two weaknesses that restrict their use in routine practice . 
 we have previously reported gene - expression signatures that predict the response of cell lines and tumours to a range of chemotherapeutic drugs.15 the aim of the present study was to con rm the ability of these signatures to predict the response of oestrogen - receptor - negative breast tumours to chemotherapy in a large series of patients enrolled in a phase iii neoadjuvant trial . 
 methods patient selection and sample processing this substudy was restricted to patients with oestrogenreceptor - negative tumours because studies that contain both patients with oestrogen - receptor - positive tumours and pa tients with oestrogen - receptor - negative tumours are easily confounded by genes linked to oestrogen - receptor status ; additionally , pathological complete response is so rare after treatment with either regimen in patients with oestrogen - receptor - positive tumours that better selection of patients will have the greatest e ect in oestrogenreceptor - negative disease . 
pathological com plete response was used as a surrogate measure of chemosensitivity because this measure consistently predicts better survival after neoadjuvant chemotherapy.1114 , 16 , 17 we undertook this study in the context of a prospective phase iii intergroup trial of neoadjuvant chemotherapy ( european organisation for research and treatment of cancer [ eortc ] 10994 / breast international group [ big ] 00 - 01 ) , the design of which is shown in gure 1 . 
eligible patients had no evidence of distant metastatic disease ( ie , m0 , as de ned by the tumour , nodes , and metastasis [ tnm ] staging system ) , and had a histologically con rmed large , operable , invasive tumour ( tumour size t2 or t3 , node status n0 or n1 ) 18 or locally advanced breast cancer ( any t , n2 ; or t4 )  . 
this substudy was restricted to all patients who were assessed at the eortc data centre on april 1 , 2005 , who met the following criteria : oestrogenreceptor - negative tumours by immuno histochemistry of the pretreatment formalinxed biopsy ; completion of the planned chemotherapy regimen with no major protocol violation ; non - t4 tumours ; and good - quality and more than 200 ng yield of rna available from a pretreatment frozen biopsy . 
 in this substudy , patients were randomly assigned to a european non - taxane regimen of six cycles of 500 mg / m uor ouracil , 100 mg / m epirubicin , and 500 mg / m cyclophosphamide ( fec ) treatment , or to three cycles of 100 mg / m docetaxel followed by three cycles of 90 mg / m epirubicin plus 70 mg / m docetaxel ( tet )  . 
pathological complete response was used as the outcome measure , and was de ned as disappearance of the invasive component of the primary tumour after treatment , with at most a few scattered tumour cells detected by the pathologist in the resection specimen . 
the a ymetrix cel les were normalised breast cancer : large operable , or locally advanced , or inammatory randomisation non - taxane regimen : fec 100x6 surgery * taxane regimen : tx3 followed by etx3 surgery * first sample : standard xation histology and oestrogen - receptor status core biopsy second sample : snap frozen microarray figure 1 : study design of eortc 10994 / big 00 - 01 trial fec = uor ouracil , epirubicin , and cyclo phosphamide . 
 * surgery was followed by radiotherapy or hormonal therapy ( or both ) according to each centres policy . 1072 vol 8 december 2007 retracted articles for information on the robust multi - array average ( rma ) algorithm see bioconductor.org see online for webappendix , webpanel and webtable 1 with the robust multi - array average ( rma ) algorithto infer the presence of erbb2 amplicons , 40 genes from trip3 to rapgefl in the erbb2 region on chromosome 17q were clustered by use of euclidian distance and wards linkage method . 
the anthracycline used in the eortc clinical study was epirubic since data on epirubicin sensitivity were not available , we used the cell - line signature for doxorubicin , an anthracycline very similar to epirubicweights generated by binaryregression analysis were applied to the expression values and summed to create metagene scores that were converted to probabilities by applying a probit function ( webappendix , webpanel , and webtable 1 )  . 
the singledrug probabilities were combined to yield the predicted probabilities of pathological complete response to fec and tet regimens as previously described.15 receiver operating characteristic ( roc ) curves were used to test the quality of the predictions . 
bootstrapping fec group ( n = 66 ) tet group ( n = 59 ) 2670 3470 with 100 000 resampled datasets was used to nd 95% ci of the area under the curve ( auc ) of the roc curves . 
the youden index20 ( sensitivity + speci city1 ) was used to select a threshold for estimation of sensitivity , speci city , positive predictive value ( ppv ) , negative predictive value ( npv ) , and overall accuracy . 
when a category of an ordinal variable had too few observations , these were pooled with an adjacent ( consecutive ) category ( grade 1 and 2 , tumour size t1 and t2 , node status n1 and n2 )  . 
 binary estimates of age and the signatures , cut at the median of the tested population , were used for fishers exact test ; age was dichotomised as a surrogate indicator of menopausal status ( median age was 495 years )  . 
missing values for grade were fec group fec predictor tet group fec predictor age , years median range histology invasive ductal invasive lobular other * tnm stage grade hormone receptor status pr negative erbb2 status ampli ed response no pcr p < 00001 ( wilcoxon ) , n = 66 p = 0302 ( wilcoxon ) , n = 59 no pcr no pcr fec group tet predictor tet group tet predictor na = not available . 
pr and oestrogen receptor ( er ) were assessed locally in each centre ; cases where less than 10% of tumour cells stained positive for pr by immunohistochemistry were deemed negative . 
 table 1 : clinical and demographic characteristics of patients p = 0044 ( wilcoxon ) , n = 66 p < 00001 ( wilcoxon ) , n = 59 no pcr no pcr figure 2 : prediction of pathological complete response with genomic signatures strati ed by trial group pcr = pathological complete response . 
black dashed lines show maximum empirical youden index ; those in the upper - left and lower - right panels were used to calculate the performance metrics in table 2 . 
classi cation statistics at the optimum threshold ( maximum empirical youden index ) with 95% ci are shown . see online for webtable 2 table 2 : performance metrics of genomic regimen - speci c signatures fec group tet group auc ( 95% ci ) auc ( 95% ci ) doxorubicin fluorouracil 066 ( 053079 ) 073 ( 059085 ) 0023 0002 076 ( 063088 ) 040 ( 025056 ) cyclophosphamide 094 ( 088099 ) < 00001 056 ( 041071 ) docetaxel fec signature tet signature 037 ( 024051 ) 0068 090 ( 081097 ) 086 ( 076094 ) < 00001 058 ( 042073 ) 065 ( 051077 ) 0044 085 ( 074094 ) 00004 0211 0401 < 00001 0302 < 00001 auc by group , approximate 95% ci ( 100 000 bootstrap samples ) , and p value ( two - sided wilcoxon rank sum test ) for the null hypothesis of no di erence . table 3 : area under roc curves of genomic signatures ( single agents and regimen - speci c signatures ) by group fec group fec predictor tet group fec predictor auc = 086 ( n = 66 ) auc = 058 ( n = 59 ) maximum youden index = 062 maximum youden index = 029 1specicity 1specicity fec group tet predictor tet group tet predictor auc = 065 ( n = 66 ) auc = 085 ( n = 59 ) maximum youden index = 03 maximum youden index = 061 1specicity 1specicity figure 3 : roc analysis of the ability of genomic signatures to discriminate patients with a pathological complete response from patients with residual disease auc , number of cases ( n ) , and location of the maximum empirical youden index ( green point ) are shown . 
 to model the potential bene t from selecting the treatment regimen according to the predicted probabilities of pathological complete response to the individual regimens , a regimen preference score was calculated by subtracting the predicted probability of pathological complete response to tet from the predicted probability of pathological complete response to fec . 
use of zero as the threshold for allocation to one or other regimen assumes that the predicted probabilities of pathological complete response to the two regimens are perfectly matched , but this is unlikely because they were independently derived from cell - line data . 
hypothetical pathological complete response rates for the entire group of 125 patients were calculated at di erent regimen allocation thresholds by taking into account the observed pathological complete response rate and the number of patients in each group at that threshold . 
this study is registered on the clinical trials site of the us national cancer institute website role of the funding source the sponsor of the trial ( eortc ) designed and coordinated the trial . 
the funding sources of the study had no role in the design of the study ; collection , analysis , or interpretation of the data ; or in the writing of this report . 
the corresponding author had full access to all of the data and had the nal responsibility to submit for publication . results of 212 patients with oestrogen - receptor - negative tumours assessed at the data centre on april 1 , 2005 , 87 patients were excluded because of major protocol violation ( two patients ) , t4 tumours ( 30 patients ) , below 20% tumour - cell content in pretreatment incisional or core biopsy ( 25 patients ) , or poor quality rna or less than 200 ng yield of rna , or both ( 30 patients )  . 
biopsies from 66 tumours in the fec group and 59 tumours in the tet group of the eortc 10994 / big 00 - 01 study were tested on a ymetrix x3p microarrays . 
response predictors were constructed by taking genes that predict the response of cell lines to uorouracil , cyclophos phamide , docetaxel , and epirubicin given as single drugs , then combining these single - drug signatures to form regimen - speci c genomic signatures , as previously described.15 figure 2 shows the predicted probability of pathological complete response to fec and tet calculated with the regimen - speci c genomic signatures in the two treatment groups . 
the signatures signi cantly predict response in patients that received 1074 vol 8 december 2007 retracted articles fec group or ( 95% ci ) size t3 vs t1 and t2 077 ( 025233 ) grade 1 and 2 vs 3 039 ( 011135 ) nodal status 1 and 2 vs 0 087 ( 029264 ) erbb2 status a vs n * 176 ( 044733 ) age older vs younger 163 ( 055495 ) 062 011 081 037 046 tet group or ( 95% ci ) 026 ( 006096 ) 067 ( 016254 ) 057 ( 017187 ) 095 ( 028321 ) 141 ( 045449 ) 210 ( 067687 ) 003 056 042 100 060 020 fec signature tet signature 865 ( 2553384 ) 272 ( 090861 ) 00001 008 1476 ( 3787024 ) < 00001 or = odds ratio . 
univariate and multivariate linear regression models including age and the genomic signatures as continuous variables are shown in webtables 3 and 4 . table 4 : two - sided fishers exact tests for association of clinical variables and genomic signatures with pathological complete response by group fec group pcr fec group no pcr tet group pcr tet group no pcr predicted probability of pcr to tet figure 4 : predicted probabilities of pathological complete response to fec and tet treatments pcr = pathological complete response . 
as would be expected given the absence of e ect of the clinical or pathological variables in univariate analysis , the genomic signatures remain signi cant in formal multivariate testing ( webtable 4 )  . a plot of the predicted probabilities of pathological complete response to the two regimens can be divided the appropriate drugs ( p < 00001 )  . 
to assess the ability of the signatures to identify responders , we did a roc analysis ; the youden index was used to identify the threshold for calculation of the performance . 
the accuracy of prediction for the regimen - speci c signatures is 79% ( 52 of 66 patients [ 95% ci 6787 ] ) for patients in the fec group and 80% ( 47 of 59 patients [ 6888 ] ) for patients in the tet group ( table 2 )  . 
furthermore , the signatures are speci c to the two regimens ; table 3 and gure 3 show that the sign atures predict response in the correct group ( ie , the fec signature predicts response to fec treatment , and the tet signature predicts response to tet treatment ) , but not in the wrong group ( ie , fec to tet , or tet to fec )  . 
both treatment regimens in the eortc study contain epirubicin , albeit in di ering schedules and total doses , therefore a small amount of crossover between the predictors in the opposing groups might be anticipated . 
we noted a weak prediction by the tet signature in the fec group ( albeit the lower boundary of the ci of the auc [ 051 ] barely exceeds the 050 value for a random classi er ) but none with the fec signature in the tet group ( the ci of the auc overlaps 050 )  . 
the design of the study called for exposure of tumours to three cycles of full - dose docetaxel ( t ) before giving combined anthracycline plus ( et )  . 
to further study the role of individual drugs in the two groups , roc analysis was used to assess the performance of the singledrug predictors ( table 3 and web gure )  . 
we conclude that the regimen - speci c signatures predict pathological complete response because they are built from individual drug signatures that predict pathological complete response . taxane tumour size , and the clinical variables age at diagnosis , node status , the pathological variables and histological grade and erbb2 status were tested for their ability to predict pathological complete response by use of fishers exact test ( table 4 ) and by univariate logistic regression ( webtable 3 )  . 
tumour size in patients in the tet group showed a borderline signi cant association with response ( p = 003 ; this would not be signi cant the 14 comparisons in table 4 or the 18 comparisons in webtable 2 )  . 
the upper - right quadrant contains many patients who responded well to treatment ( triangles ) ; the undesirable side - e ects of taxanes mean these patients are candidates for conventional fec treatment . 
the lowerright quadrant contains many patients who failed to respond to fec ( green circles ) , but have a high predicted probability of pathological complete response to tet ; the upper - left quadrant contains some patients who failed to respond to tet ( blue circles ) , but have a high predicted probability of pathological complete response to fec . 
 inspection of the plot shows that dividing it with a diagonal line might form the basis of a rule to allocate patients to di erent regimens : patients below the diagonal line should receive tet , and patients above the line should receive fec . 
 at least two reasons exist for asking what might happen if this threshold were altered ( ie , the diagonal line were displaced vertically ) : rst , it might be desirable to decrease the number of patients receiving taxanes because of their side - e ects ; second , the predicted probabilities of pathological complete response to the two regimens are independently derived and unlikely to be matched precisely . 
to do this , we rst calculated a regimen preference score ; this was simply the predicted probability of pathological complete response to fec treatment minus the predicted probability of pathological complete response to tet treatment . 
in the treatment allocation model , patients were assigned to fec treatment when the regimen preference score was above the threshold ( above the diagonal line ) and to tet when the regimen preference score was below the threshold ( below the diagonal line )  . 
the diagonal line in gure 4 corresponds to a threshold of zero in gure 5 ; the patient marked by the arrow would be allocated to treatment with tet because their regimen preference score ( 02 ) was below zero . 
the ratio of green triangles to green circles above the diagonal line gives the pathological complete response rate for fec treatment ; this number multiplied by the total number of points above the line gives the number of responders in the group allocated to fec treatment ; likewise , the ratio of blue triangles to blue circles below the line gives the pathological complete response rate for tet treatment ; this number multiplied by the total number of points below the line gives the number of responders in the group allocated to tet treatment ; these are combined to calculate the hypothetical pathological complete response rate for both groups together . 
 when the threshold is lowered ( ie , the diagonal line in gure 4 is moved vertically down ) , more patients are assigned to fec treatment ( green dashed line in gure 5 ) , whereas when it is raised more patients are assigned to tet treatment ( blue dashed line )  . 
for example , for the point marked by an arrow ( regimen preference score of 02 ) , decreasing the regimen allocation threshold to 03 would mean that the score was now above the threshold and the patient would receive fec treatment . 
 generally , the lower the score the more likely a patient is to receive tet treatment ; conversely , the lower the threshold the more likely a patient is to receive fec treatment . 
for a wide range of thresholds the hypothetical pathological complete response rate ( red line ) is 6570% , well above the 42% and 46% pathological complete response rates noted in the fec and tet groups in the clinical trial . 
the peak of the red curve is displaced to the left of zero , suggesting that fec treatment could be safely used more frequently if treatment were selected by use of the signatures described here . 
we conclude that clinical application of these regimen - speci c genomic signatures could have a useful e ect on overall treatment success and decrease the number of patients exposed to the side - e ects of taxanes . 1076 vol 8 december 2007 retracted articles discussion this study con rms that gene - expression signatures based on cell lines can be used to predict pathological complete response of breast tumours to chemotherapy . 
 to our knowledge , this is the rst study in which genomic predictors for two di erent treatments have been studied in a large cohort of patients enrolled in a multicentre randomised phase iii clinical trial . 
long - term follow - up will be required to establish whether regimen - speci c genomic signatures also predict long - term survival , but this is likely since most previous studies have noted that patients achieving a pathological complete response indeed have longer survival , and this remains true after multivariate analysis.11 , 16 , 17 the ndings reported here used a doxorubicin signature instead of an epirubicin signature . 
the a ymetrix x3p chip we used was developed for analysis of para n - embedded material , so only small modi cations to the protocol might be needed to test para n - embedded material . 
alternatively , pcr techniques developed by gianni and colleagues4 could be used to measure the expression of the genes in our genomic signatures . there it necessitates is no universally accepted de nition of pathological complete response . 
pathological complete response de ned as disappearance of the invasive component of the primary tumour after treatment , with at most a few scattered tumour cells detected by the pathologist in the resection specimen , is standardisation of proof that a large mass of tumour cells has disappeared . 
killing large numbers of tumour cells is desirable , but does not guarantee long - term survival of patients , possibly because rare tumour stem cells are the crucial determinants of relapse.21 hence , validation of the clinical relevance of the signatures reported here will best be done by showing regimen - speci c prediction of improved survival of patients in a large adjuvant study , where the de nition of pathological complete response is not relevant . 
indeed , the pathological complete response rate is so low in this group in the neoadjuvant setting that a study ten times larger than the one we have undertaken would be needed to identify con dently a signature with similar predictive power in the oestrogen - receptor - positive group . to neoadjuvant the treatment allocation model explored in gures 4 and 5 suggests that selection of the treatment regimen with our genomic signatures has the potential to increase the pathological complete response rate from 44% to around 70% . 
an important caveat is that this will apply only to patients with oestrogen - receptor - negative the oestrogen - receptor - negative group there are two major tumours with radically di erent geneclasses of expression pro les ( called the erbb2 and basal - like classes in the stanford classi cation22 )  . 
 this makes it feasible to identify at an early stage patients who are unlikely to respond to fec or tet treatment and hence have the most to bene t from new drugs . 
 organising clinical trials on this basis would have important implications for the subsequent use of new drugs being tested , because the information obtained would apply only to a narrowly de ned group , albeit one vol 8 december 2007 1077 retracted articles with a poor outcome with conventional treatment . 
we aimed to assess and define these genes to provide evidence for future screening guidelines . methods in this international , multicentre study , we analysed patients with medulloblastoma from retrospective cohorts ( international cancer genome consortium [ icgc ] pedbrain , medulloblastoma advanced genomics international consortium [ magic ] , and the cefalo series ) and from prospective cohorts from four clinical studies ( sjmb03 , sjmb12 , sjyc07 , and i - hit - med )  . 
dna methylation profiling was done to determine consensus molecular subgroups : wnt ( mbwnt ) , shh ( mbshh ) , group 3 ( mbgroup3 ) , and group 4 ( mbgroup4 )  . 
previously defined somatic mutational signatures were used to further classify medulloblastoma genomes into two groups , a clock - like group ( signatures 1 and 5 ) and a homologous recombination repair deficiency - like group ( signatures 3 and 8 ) , and chromothripsis was investigated using previously established criteria . 
progression - free survival and overall survival were modelled for patients with a genetic predisposition to medulloblastoma . findings we included a total of 1022 patients with medulloblastoma from the retrospective cohorts ( n = 673 ) and the four prospective studies ( n = 349 ) , from whom blood samples ( n = 1022 ) and tumour samples ( n = 800 ) were analysed for germline mutations in 110 cancer predisposition genes . 
in our rare variant burden analysis , we compared these against 53 105 sequenced controls from exac and identified apc , brca2 , palb2 , ptch1 , sufu , and tp53 as consensus medulloblastoma predisposition genes according to our rare variant burden analysis and estimated that germline mutations accounted for 6% of medulloblastoma diagnoses in the retrospective cohort . 
the prevalence of genetic predispositions differed between molecular subgroups in the retrospective cohort and was highest for patients in the mbshh subgroup ( 20% in the retrospective cohort )  . 
these estimates were replicated in the prospective clinical cohort ( germline mutations accounted for 5% of medulloblastoma diagnoses , with the highest prevalence [ 14% ] in the mbshh subgroup )  . 
patients with germline apc mutations developed mbwnt and accounted for most ( five [ 71% ] of seven ) cases of mbwnt that had no somatic ctnnb1 exon 3 mutations . 
germline tp53 mutations presented only in childhood patients in the mbshh subgroup and explained more than half ( eight [ 57% ] of 14 ) of all chromothripsis events in this subgroup . 
 germline mutations in palb2 and brca2 were observed across the mbshh , mbgroup3 , and mbgroup4 molecular subgroups and were associated with mutational signatures typical of homologous recombination repair deficiency . 
 funding german cancer aid ; german federal ministry of education and research ; german childhood cancer foundation ( deutsche kinderkrebsstiftung ) ; european research council ; national institutes of health ; canadian institutes for health research ; german cancer research center ; st jude comprehensive cancer center ; american lebanese syrian associated charities ; swiss national science foundation ; european molecular biology organization ; cancer research uk ; hertie foundation ; alexander and margaret stewart trust ; v foundation for cancer research ; sontag foundation ; musicians against childhood cancer ; bc cancer foundation ; swedish council for health , working life and welfare ; swedish research council ; swedish cancer society ; the swedish radiation protection authority ; danish strategic research council ; swiss federal office of public health ; swiss research foundation on mobile communication ; masaryk university ; ministry of health of the czech republic ; research council of norway ; genome canada ; genome bc ; terry fox research institute ; ontario institute for cancer research ; pediatric oncology group of ontario ; the family of kathleen lorette and the clark h smith brain tumour centre ; montreal childrens hospital foundation ; the hospital for sick children : sonia and arthur labatt brain tumour research centre , chief of research fund , cancer genetics program , garron family cancer centre , mdts garron family endowment ; bc childhood cancer parents association ; cure search foundation ; pediatric brain tumor foundation ; brainchild ; and the government of ontario . copyright 2018 the author ( s )  . 
following the recognition9 of four consensus molecular subgroups ( wnt [ mbwnt ] , shh [ mbshh ] , group 3 [ mbgroup3 ] , and group 4 [ mbgroup4 ] ) with distinct demographics and clinical outcomes , 10 patients with germline tp53 , sufu , and ptch1 mutations have been reported to be predisposed to develop mbshh.11 , 12 although several case studies have reported in patients with fanconi medullo blastomas arising specific anaemia , whether medulloblastoma subgroups , and whether heterozygous germline mutations13 also confer an increased risk of developing medulloblastoma , remain unknown . 
a comprehensive study14 of damaging germline mutations in cancer predisposition genes across a diverse set of paediatric cancers identified variants likely to predispose to the disease in three ( 8% ) of 37 patients with medulloblastomaa cohort size that is too small to allow these predispose these issues to be thoroughly addressed . 
owing to these uncertainties , and since knowledge about germline mutations can be useful for clinical practice , 8 assessment of larger patient series is crucial for the identification of consensus medullo blastoma predisposition genes to estimate the con tribution of genetic predisposition towards consensus molecular sub groups , and investigate whether affected patients have distinct clinical outcomes . 
a comprehensive under standing of molecular alterations in affected patients would further help in the development of clinical screening guidelines for genetic risk assessment in paediatric patients . in this study , we provide a comprehensive description of genetic risk factors across 1022 patients with medulloblastoma based on a retrospective discovery cohort and validation in a prospective clinical cohort . 
additionally , which patients would benefit from genetic counselling in the context of molecular subgroupingnowadays routinely applied in clinical trials and implemented into the revised who classification of cns tumours in 2016and whether genetic predisposition can be recognised based on familial patterns were unclear . 
additionally , several paediatric cancer centres have implemented routine multigene panel analysis and whole - exome analysis of medulloblastomas ; however , these centres encounter several germline mutations with uncertain clinical significance . 
no study has previously aimed to define a consensus set of medulloblastoma predisposition genes or has investigated under which circumstances genetic counselling and testing should be offered to patients with medulloblastoma . added value of this study this study is based on an international cohort of 1022 patients with medulloblastoma , and includes detailed information about medulloblastoma subgroups ( wnt [ mbwnt ] , shh [ mbshh ] , group 3 [ mbgroup3 ] , and group 4 [ mbgroup4 ] ) , somatic mutation landscapes , and clinical outcomes . 
we defined and characterised six consensus , clinically relevant medulloblastoma predisposition genes on the basis of rare variant burden analysis ( apc , brca2 , palb2 , ptch1 , sufu , and tp53 )  . 
half of all patients with damaging germline mutations were not recognised based on familial history of cancer ; however , these patients exhibited distinct phenotypes with respect to age at diagnosis , molecular subgroups , somatic mutation patterns , and clinical outcomes . 
about one in five patients in the mbshh subgroup developed medulloblastoma in the context of a genetic predisposition , underscoring the need for a dedicated genetic screening programme and surveillance programme in this patient group . 
damaging germline mutations in known cancer predisposition genes were rare in paediatric patients in the mbgroup3 and mbgroup4 subgroups , which indicates conservative ordering of genetic tests in these groups . 
we propose clinical guidelines for genetic screening in medulloblastoma based on routinely acquired clinical and molecular tumour phenotypes . implications of all the available evidence a significant prevalence of clinically important germline mutations in two of four molecular subgroups reveals that genetic counselling and testing should be established as a standard - of - care procedure in the management of patients with medulloblastoma . 
we obtained biological samples from all patients , who all provided written informed consent , in accordance with institutional review board guidelines . patient accrual for our retrospective cohort was done from 2003 until 2016 . 
patient accrual for the sjmb03 trial was done from sept 9 , 2003 , until march 7 , 2013 and for the sjyc07 trial was done from dec 17 , 2007 , until march 31 , 2017 . 
the age limit for eligibility in the prospective studies was 5 years or younger ( sjyc07 ) , 321 years ( sjmb03 ) , and 339 years ( sjmb12 )  . 
 patients in the i - hit - med study were excluded if they were registered in another clinical trial for the same diagnosis ( relapse is defined as a second diagnosis ) or if a valid ethical committee approval was lacking . procedures whole - genome and whole - exome sequencing data for germline and tumour samples were generated at the german cancer research centre ( icgc pedbrain ; heidelberg , germany ) , canadas michael smith genome sciences centre ( magic ; vancouver , bc , canada ) , broad institute of massachusetts institute of technology and harvard ( cambridge , ma , usa ) , and st jude childrens research hospital ( pediatric cancer genome project ; memphis , tn , usa )  . to ensure standardisation of genomic data processing , we used the same uniform computational analysis workflows for all germline and tumour samples . 
we used delly for germline genomic structural variant discovery with default settings for whole - genome sequencing samples and a custom read - depth - based copy - number variation ( cnv ) - calling pipeline for whole - exome sequencing samples . 
we based this custom pipeline on read quantification by bedtools in exome capture regions ( maq > 30 ) , followed by variance stabilising transformation of count data with the vst function from the deseq2 r package ( version 1.8.2 ) , unsupervised estimation of hidden confounders using the r package peer ( 30 hidden confounders ) , and copynumber segmentation based on standardised residuals using circular binary segmentation ( r package dnacopy , version 1.50 , default settings )  . 
raw cnv calls were filtered further for size ( to include only those > 10 kb ) , minimum number of exons ( > 2 ) , and cnv signal intensity ( > 4 sds )  . 
 any snv , short indel , and mnv that was observed at low variant allele frequency in blood ( 315% ) and high variant allele frequency in tumours ( > 50% ) was considered a putative mosaic mutation . 
we restricted the analysis to reads with mapping quality of more than 30 ( 10 log10 pr [ mapping position is wrong ] ) , base quality of more than 20 ( 10 log10 pr [ mapping position is wrong ] ) , and sites with more than 30 times sequencing coverage ( ie , number of reads )  . 
we excluded any variant that was present in public genetic archives and discovered in germline genomes of other patients with medulloblastoma . for classification of damaging germline mutations , germline variants were annotated with the ensembl variant effect predictor ( vep ; r81 )  . 
high - impact ( ie , damaging ) germline mutations were defined as frameshift , stop gain , start lost , canonical splice site , exon or gene deletions , known ( clinvar ; accessed feb 16 , 2017 ) damaging non - canonical splice site variants , and somatic mosaic mutations ( defined as mutations present in a subset of normal cells )  . 
putative damaging germline mutations were removed if the estimated minor allele frequency in at least one continental population was more than 01% , which we judged on the basis of 53 105 sequenced individuals that were assigned to known ( control ) populations and without a cancer diagnosis from the exome aggregation consortium ( exac ) resource , the 1000 genomes project , and the national heart , lung , and blood institute go exome sequencing project . 
putative gain - of - function missense variants in tp53 were further evaluated by use of information in the international agency for research on cancer tp53 database and annotated as pathogenic if tp53 mutations were classified as non - functional in experimental transcriptional activity assays . 
we estimated the primary population ancestry ( european , african , east asian , south asian , and native american ) for all patients with medulloblastoma with a supervised decomposition approach20 and ancestry - informative markers that are within exac - defined exome capture target regions . identification of somatic mutations ( snvs , small indels , and copy - number alterations ) was pursued in a standardised manner across all samples ( matched tumour or normal genome as well as exome pairs ) with the german cancer research center ( known as dkfz ) and european molecular biology laboratory cancer genome analysis workflow of the pcawg consortiu somatic snvs and indels were further stringently filtered for germline contamination using information from dbsnp and the 1000 genomes project . 
we used a highstringency structural variant set by additionally filtering somatic structural variants detected in at least 1% of a set of 1105 germline samples from healthy individuals belonging to phase 1 of the 1000 genomes project , and by requiring absence of somatic structural variants in all medulloblastoma germline samples of this study . 
for inference of high - stringency structural variants , we additionally required at least four supporting read pairs21 with a minimum mapping quality of 20 ( 10 log10 pr [ mapping position is wrong ] ) and restricted valid somatic structural variant sizes from 100 bp to 500 mb . we quantified previously defined somatic mutational signatures22 ( termed 1 , 3 , 5 , and 8 ) using tumour - specific somatic point - mutation spectra and published signature probabilities . 
 signatures 1 and 5 ( clock - like signatures ) are associated with ageing ( a clock - like accumulation of mutations ) and occur in normal , non - malignant cells , 22 whereas signatures 3 and 8 are associated with homologous recombination repair deficiency ( hrd ) and have been reported in cancer tissues . 
we used these mutational vol 19 june 2018 articles signatures to further classify medulloblastoma genomes into two groups , a clock - like group ( signatures 1 and 5 ) and a hrd - like group ( signatures 3 and 8 )  . 
somatic mutation spectra were quantified with the r package somaticsignatures ( version 2.6 ) and decomposed into contributions of known mutational signatures based on the lawsonhanson algorithm for non - negative least squares ( nnls version 1.1 , r package )  . 
the quantification error ( residual sum of squares ) was correlated with the total somatic mutation burden ( spearmans r = 074 ; p < 00001 ) and it was highest in tumours with fewer than 100 somatic snvs . 
 medulloblastomas were classified as homo logous recombination repair deficient if most ( > 50% ) somatic snvs were assigned to mutational signatures 3 or 8 . to assess the burden of rare germline snvs and indels in cancer predisposition genes , we performed case control association testing in a subgroup - specific manner as well as across all subgroups based on a collection 110 autosomal cancer predisposition genes8 , 23 ( appendix p 2 )  . 
to ensure comparability with variants found in patients with medulloblastoma , exac germline mutations were normalised with vt normalize , annotated with vep ( r81 ) , and filtered for sites that passed quality controls , as defined by exac . 
moreover , we excluded any germline mutations that were present outside exacdefined target regions to reduce any possible advantages derived from improved variant calling in whole - genome sequences ( eg , exons not being covered in exac )  . 
we assumed equal effect sizes for frameshift , nonsense , splice site , and gain - of - function missense variants , as well as for variants located at any position along a gene . 
allelic relative risks were estimated by the odds ratio ( or ) , which describes the association between medullo blastoma and damaging alleles by comparing the odds of medullo blastoma in an individual carrying a wild - type allele to the odds of medulloblastoma in an individual carrying one damaging allele . 
we assumed that the penetrance of monoallelic germline mutations was lower than that of biallelic germline mutations ( ie , homozygous and compound heterozygous mutations )  . we assessed secondary somatic gene hits in tumours on three levels : point mutations , loss - of - heterozygosity , and allele - specific gene expression . 
loss of heterozygosity was quantified by use of genotyping germline alleles in available tumour genomes or exomes with freebayes and requiring a minimum coverage of ten reads , minimum base quality of 10 ( 10 log10 pr [ base is wrong ] ) , and minimum mapping quality of 10 ( 10 log10 pr [ mapping position is wrong ] )  . 
 allele - specific gene expression was quantified at heterozygous snvs and indels and mrna sequencing data by use of freebayes ( minimum mapping quality of [ 10 log10 pr ( mapping position is wrong ) ] and minimum base quality of 10 [ 10 log10 pr ( base is wrong ) ] ) and was predicted on the basis of binomial tests , an expected ratio of 05 , and p values lower than 005 . 
 when possible , multiple sites within the same gene were phased with paired - end rna sequencing data and individual sites were merged to calculate haplotypespecific expression ratios . investigated chromothripsis using previously established criteria.24 these criteria distinguish chromothripsis from dna rearrangements occurring in a stepwise fashion . 
first , we analysed breakpoint clustering in the entire genome based on highconfidence somatic structural variant calls and did statistical analysis for non - randomness of breakpoint distributions , under the assumption of an exponential distribution ( null hypothesis )  . 
overall survival and progression - free survival were based on definitions consistent with how they were evaluated within each respective patient cohort from each prospective trial : sjmb03 , sjmb12 , and sjyc07 . 
one - sided binomial tests were used for replication analysis with the alternative hypothesis defined as a lower probability of observing germline mutations in the replication cohort . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding authors had full access to all the data and had the final responsibility to submit for publication . tumour genomes were results we analysed germline genome - sequencing and exomesequencing data ( appendix pp 89 ) from 1022 patients with medulloblastoma , of whom 673 were in the retrospective discovery cohort and 349 were in the prospective clinical study cohort ( figure 1a , appendix p 3 )  . 
patientfor matched 800 samples from both cohorts ( n = 451 retrospective and n = 349 prospective ) from whole - genome sequencing ( n = 397 ) and whole - exome sequencing ( n = 403 ; figure 1a )  . 
snvs , mnvs , small ( < 30 bp ) indels , and large structural variants were predicted across 110 paediatric - onset and adult - onset cancer predisposition genes8 , 23 and classified as pathogenic based on stringent criteria . 
most damaging germline mutations have been previously described in the literature ( in 55 [ 71% ] of 77 mutations ) and already classified as ( likely ) pathogenic ( 42 [ 55% ] of 77 ) in public archives ( clinvar , lovd ; appendix pp 1012 )  . 
in total , six genes showed a significant excess of damaging germline mutations for patients with medulloblastoma namely , apc , brca2 , palb2 , ptch1 , sufu , and tp53 ( adjusted p value for multiple testing < 005 ; figure 1b , appendix p 4 )  . 
 however , a single patient in our discovery cohort harboured a heterozygous germline mutation in msh6 ( appendix pp 1012 )  . the overall prevalence of genetic predisposition based on these six genes in the retrospective discovery cohort was 6% ( 40 / 673 ) , with a highest prevalence of 20% ( 28 / 141 ) in patients in the mbshh subgroup ( figure 1c )  . 
key patient characteristics , such as sex , age at diagnosis , and molecular tumour subgroups , were similar between both cohorts ( psex = 068 , page = 017 , psubgroup = 012 ; figure 1a )  . 
the overall prevalence of genetic predisposition in our prospective cohort ( 17 [ 5% ] of 349 ) was consistent with estimates ( p = 024 ; from our retrospective cohort figure 1d , appendix pp 1012 )  . 
notably , patients in the mbwnt subgroup also had an increased prevalence of germline predisposition in both the discovery and replication cohort , albeit more modest than for patients in the mbshh subgroup ( figure 1c , d )  . genes we closely analysed key demographic , clinical , and molecular characteristics of patients with a genetic predisposition in these six genes . 
most patients with available subgroup information developed mbshh ( 41 [ 76% ] of 54 ; figure 2a ) and age at diagnosis also differed significantly between patients with germline mutations in medulloblastoma predisposition ( p < 00001 ; figure 2b )  . 
patients with germline sufu or ptch1 mutations were typically diagnosed as infants at a median age of 20 years ( iqr 1323 ) , whereas patients with apc or tp53 mutations were diagnosed as children at a median age of 98 years ( iqr 8011 )  . 
clinical signs of a genetic predisposition were noted in 16 ( 41% ) of 39 patients and familial history of cancer in 17 ( 46% ) of 37 patients , and both were different between patients with germline mutations in medulloblastoma pre disposition genes ( p = 0017 and p = 0046 , respectively ; figure 2c , 2d )  . 
for example , only one ( 9% ) of all 11 ptch1 and sufu mutation carriers with available medical records had a family history of cancer ; however , eight ( 67% ) of records had 12 patients with available medical clinical symptoms consistent with gorlins syndrome 790 vol 19 june 2018 articles a male ( 63% ) male ( 64% ) medulloblastoma cohort retrospective : n = 673 prospective : n = 349 whole - genome and whole - exome squencing germline : n = 1022 tumour : n = 800 molecular subgroup 844 tumours 110 cancer predisposition genes age at diagnosis molecular subgroup female ( 37% ) female ( 36% ) child ( 70% ) child ( 79% ) infant ( 17% ) adult ( 13% ) infant ( 16% ) adult ( 5% ) group 4 ( 38% ) group 4 ( 40% ) ( 28% ) ( 27% ) group 3 ( 27% ) wnt ( 6% ) group 3 ( 22% ) wnt ( 10% ) sufu ptch1 tp53 palb2 brca2 retrospective cohort prospective cohort 1000 all subgroups of medulloblastoma group 3 group 4 rr ( 95% ci ) n = 349 p = 024 n = 673 group 3 group 4 group 3 group 4 n = 32 20% n = 141 n = 134 n = 189 n = 36 p = 081 14% n = 95 p = 0080 n = 78 p = 048 n = 139 p = 0051 figure 1 : discovery and replication of medulloblastoma predisposition genes ( a ) study design and patient characteristics . 
patients with damaging germline mutations in apc , ptch1 , sufu , tp53 , palb2 , and brca2 . ( eg , macrocephaly , jaw cysts , and frontal bossing ; appendix pp 1012 )  . 
by contrast , all four apc mutation carriers with available medical records had a familial history of familial adenomatous polyposis and associated cancers ( eg , adrenocortical carcinoma )  . 
of note , additional malignancies were observed in six ( 12% ) of 50 patients with medulloblastoma and all were restricted to patients with germline apc ( n = 3 ) or tp53 ( n = 3 ) mutations ( appendix pp 1012 )  . at a median follow - up of 48 months ( iqr 2878 ) , 5 - year progression - free survival for 49 patients with a genetic predisposition who were evaluable for this outcome was 52% ( 95% ci 4069 )  . 
progression - free survival ( logrank p = 00056 ) and overall survival ( log - rank p = 000032 ) differed significantly across patients with germline mutations in different medullo blastoma predisposition genes ( figure 3 )  . germline apc mutations were found in seven ( 1% ) of all 1022 patients with medulloblastoma and included one infant , five children , and one adult patient . 
two of these seven patients harboured partial or full gene deletions ( appendix p 5 ) and the remaining five patients had frameshift and nonsense mutations between codons 554 and 1113 , a region associated with classical familial adenomatous polyposis phenotypes . 
all five wnt - driven medulloblastomas lost the wild - type apc allele and the shhdriven medulloblastoma showed retention of the wild - type allele ( figure 4a )  . 
furthermore , germline apc mutations in mbwnt patients were mutually exclusive with somatic ctnnb1 exon 3 mutations ( p < 00001 ) , the primary26 somatic driver event in mbwnt ( figure 4b )  . 
 overall , germline apc mutations were identified in five ( 71% ) of seven ctnnb1 - wild - type mbwnt cases and , together with somatic ctnnb1 mutations , explained 97% ( 64 / 66 ) of all wnt - driven medulloblastomas . 
by contrast , monosomy 6a frequent somatic chromosome aberration in mbwnt ( in 55 [ 83% ] of 66 cases ) was not mutually exclusive with germline apc mutation status ( p = 019 ) ; although we observed two patients with vol 19 june 2018 articles a group 4 group 3 n = 54 ; p < 00001 patients ( % ) 100% n = 57 ; p < 00001 age at diagnosis ( years ) ( 12 ) ( 23 ) ( 35 ) ( 530 ) ( 410 ) ( 911 ) ( 711 ) brca2 * ptch1 sufu tp53 palb2 brca2 sufu ptch1 brca2 * palb2 brca2 tp53 n = 37 ; p = 0046 n = 39 ; p = 0017 adult ( 18 ) child ( 4 - 17 ) infant ( 3 ) ptch1 sufu tp53 palb2 brca2 brca2 * palb2 tp53 brca2 sufu ptch1 brca2 * figure 2 : clinical characteristics of patients with a genetic predisposition ( a ) molecular tumour subgroups . 
overall and progression - free survival for patients with apc - mbwnt was 100% ( 95% ci 100100 )  . germline tp53 mutations were found in 14 ( 1% ) of all 1022 patients with medulloblastoma and were only present in patients with mbshh ( 13 / 13 ; data missing for one patient )  . 
notably , germline tp53 mutations were identified in 13 ( 8% ) of 170 paediatric mbshh patients and 13 ( 20% ) of 63 children aged between 5 years and 16 years with mbshh . 
most germline tp53 mutations ( 13 / 14 ) clustered within the dna - binding domain ( appendix p 6 ) and somatic inactivation of the wild - type tp53 allele was detected in all 13 available medullo blastoma genomes via loss of heterozygosity ( figure 4a )  . 
all eight whole - genome - sequenced tp53deficient mbshh exhibited complex somatic genomic rearrangements consistent with chromothripsis21 and accounted for eight ( 57% ) of all 14 chromothripsis events in the mbshh subgroup . 
5 - year overall survival for patients with germline tp53 mutations was 27% ( 95% ci 1072 ; figure 3 )  . germline sufu and ptch1 mutations were detected in 20 ( 2% ) of all 1022 patients with medulloblastoma , exclusively the mbshh subgroup ( 19 / 19 ; data missing for one patient ) , and accounted for 11% ( 18 / 170 ) of all paediatric patients with mbshh and 21% ( 17 / 80 ) of all infant patients with mbshh . 
we observed somatic loss of the sufu or ptch1 wild - type allele in all ( n = 18 ) sequenced mbshh that were diagnosed in patients with germline sufu or ptch1 mutations . 
only six of 20 germline sufu and ptch1 mutations have been previously described in the literature ( appendix pp 1012 ) , suggesting either appreciable amounts of de - novo mutagenesis or poor reporting to public archives . 
in support of the de - novo mutagenesis theory , a de - novo germline ptch1 mutation was observed in a patient with mbshh from our retrospective cohort , for whom whole - exome sequences were also available for both parents . 
clinical information was frequency ranged 792 vol 19 june 2018 articles a available for one patient with a mosaic ptch1 mutation , which showed that the patient was clinically diagnosed with gorlins syndrome and the patient had no family history of cancer and no family history of gorlins syndrome . 
moreover , comparison of clinical outcomes between patients with germline mutations in sufu and ptch1 showed no differences in progression - free survival ( p = 050 , 16 patients with germline mutations ) and overall survival ( p = 091 , 17 patients with germline mutations )  . 
notably , patients with germline mutations in either sufu or ptch1 had a better overall survival than progression - free survival ( combined 5 - year progressionfree survival 56% for sufu and ptch1 mutations , 95% ci 3787 ; combined 5 - year overall survival 85% , 95% ci 67100 ; figure 3 )  . germline brca2 mutations were present in 11 ( 1% ) of all 1022 patients with medulloblastoma and included ten paediatric patients and one adult ( survival data not available for all patients with these mutations )  . 
clinical signs of a genetic predisposition or family history of cancer were noted in all four compound heterozygous patients and in four ( 80% ) of five heterozygous patients with available medical records . 
patients with compound heterozygous mutations at brca2 developed exclusively mbshh ( p = 00060 when compared with any other subgroup ; figure 2a ) and exhibited worse progression - free survival ( p = 0025 ) and overall survival ( p = 0022 ) relative to patients with heterozygous germline brca2 mutations ( figure 3 )  . 
when compared with 53 105 controls , the burden of rare germline mutations in brca2 was associated with increased risk of mbshh ( relative risk [ rr ] 138 [ 54294 ] ; p < 00001 ) and mbgroup3 / 4 ( rr 42 [ 14101 ] ; p = 00077 )  . 
 additional details about family history of cancer , parental genetic testing , and somatic mutation profiles heterozygous and compound heterozygous brca2 mutation carriers are provided in the appendix ( p 1 )  . germline palb2 mutations were found in five ( < 1% ) of all 1022 patients with medulloblastoma . 
all five damaging germline mutations were heterozygous in patients affected with medullo blastoma and were previously reported in familial pancreatic and breast cancer studies.27 all five germline mutations were classified as pathogenic according to clinvar ( appendix pp 1012 )  . 
log - rank p values indicate differences across all patient groups . adult - onset cancers ( eg , breast cancer ) , predisposition to paediatric malignancies has so far only been described in the context of fanconi anaemia.28 we excluded the predisposition to fanconi anaemia in all five cases because of an absence of additional rare germline mutations ( including protein - truncating variants , missense mutations , and inframe indels )  . 
analysis of vol 19 june 2018 articles b germline apc mutation somatic ctnnb1 mutation somatic monosomy 6 somatic ctnnb1 mutation germline apc mutation * mbwnt mutant cases wild - type cases 76% 894% 833% n = 66 ; p = 092 age at diagnosis ( years ) tp53 sufu ptch1 palb2 brca2 n = 49 signature 1 associated with ageing seen in healthy cells and tumour cells signature 3 associated with hrd seen in breast cancer signature 5 associated with ageing seen in healthy cells and tumour cells signature 8 associated with hrd seen in medulloblastoma and breast cancer patients ( % ) 100% n = 375 brca2 palb2 wild - type brca2 palb2 wild - type brca2 palb2 wild - type brca2 palb2 wild - type figure 4 : molecular medulloblastoma characteristics for patients with a genetic predisposition ( a ) patterns of somatic inactivation of wild - type alleles for all patients with a germline mutation in one of the consensus medulloblastoma predisposition genes . 
 ( b ) somatic driver events in patients with medulloblastoma in the wnt subgroup ( top panel ) and age at diagnosis for all patients with germline apc mutations and patients in the wnt subgroup with somatic ctnnb1 mutations ( bottom panel )  . 
 ( c ) association between germline palb2 ( n = 5 ) and brca2 ( n = 7 ) mutation status and somatic mutational signatures 1 , 3 , 5 , and 8 . 
additional details about family history of cancer , parental genetic testing , and somatic mutation profiles available for one affected patient are presented in the appendix ( p 1 )  . since the clinical relevance of heterozygous germline mutations in palb2 and brca2 is uncertain , we aimed to corroborate our findings through investigation of somatic mutation patterns ( mutational signatures ) in medulloblastoma genomes . 
quantification of four previously implicated mutational signatures ( signatures 1 , 3 , 5 , and 8 ) across 375 medulloblastoma genomes showed a significant association between both hrd signatures ( signatures 3 and 8 ) and germline brca2 and palb2 mutation status ( figure 4c , appendix p 7 )  . 
moreover , although the overall prevalence of an hrd - like mutation spectrum was modest in medulloblastoma ( 58 [ 15% ] of 375 ) , it was enriched in tumours as brca2 - deficient and palb2 - deficient compared with tumours with other genetic mutations ( or 190 [ 95% ci 45113 ] , p < 00001 )  . 
in total , nine ( 75% ) of 12 brca2 - deficient and palb2 - deficient tumours showed evidence for an hrd - like mutation spectru strikingly , eight ( 89% ) of nine patients with mbshh and an hrd - like mutation spectrum harboured germline mutations in consensus medulloblastoma predisposition genes ( brca2 n = 4 , palb2 n = 2 , and tp53 n = 2 ) , suggesting that hrd might serve as a biomarker for genetic predisposition in this patient group . 
we also observed five patients in the mbwnt subgroup with an hrd - like mutation spectrum and noticed that four ( 89% ) of five cases were diagnosed as adults ( p = 00003 for paediatric vs adult cases )  . 
 the only paediatric patient in the mbwnt subgroup with an hrd - like mutation spectrum harboured a pathogenic heterozygous germline mutation in atm along with somatic inactivation of the wild - type atm allele ( appendix pp 1012 )  . 
finally , we also identified heterozygous germline mutations in fanca ( n = 1 ) and fancq ( n = 1 ) in patients with mbgroup3 and mbgroup4 , respectively , and an hrd - like mutation spectru taken together , these results corroborate our genetic findings and indicate that genetic 794 vol 19 june 2018 articles alteration of homologous recom bination genes is associated with an hrd - like mutation spectrum in medul loblastoma . 
our rare variant burden analyses revealed that genetic predisposition has a major role in the cause of medulloblastoma after accounting for molecular subgroups , with a high prevalence in mbwnt and mbshh patient subgroups . 
recommendations for surveillance and clinical management of individual childhood cancer predisposition syndromes have been summarised in a series of articles29 from the american association for cancer research childhood cancer predisposition workshop . 
 our study complements these recommendations by providing additional diagnostic criteria based on clinical and molecular characteristics . the urgent need here , we identified heterozygous germline apc mutations in 68% of patients in the mbwnt molecular subgroup and showed that genetic cases were indistinguishable from sporadic cases based on age at diagnosis . 
 importantly , all patients with apc - deficient mbwnt did not have the hallmark somatic driver event of mbwntnamely , somatic missense mutations in ctnnb1 ( the gene encoding - catenin )  . 
 in our series , patients with mbwnt and germline apc mutations showed favourable clinical outcomes , which mirrors the favourable outcome for patients with mbwnt with nuclear accumulation of - catenin.30 nevertheless , several patients with germline apc mutations had an additional malignancy , which emphasises the need to provide genetic counselling for patients with mbwnt in the future , irrespective of clinical outcomes . 
additional studies will be needed to assess whether or not germline apc mutations are a genetic risk factor for mbshh . given the particularly high prevalence of damaging germline mutations in patients with mbshh , we recommend that all patients with mbshh should be counselled for genetic testing . 
patients younger medulloblastoma subgroup group 3 group 4 genetic testing of family history of brca - associated cancers , or homologous recombination repair deciency , or both genetic testing of absence of somatic ctnnb1 exon 3 mutation prioritisation of genetic testing based on age or genomic instability , or both sufu , ptch1 tp53 , palb2 , and brca2 palb2 and brca2 figure 5 : proposed clinical guidelines for genetic counselling and testing in medulloblastoma based on clinical and molecular tumour characteristics than 3 years of age should initially be tested for germline mutations in sufu and ptch1 ( especially in view of the high prevalence of sufu mutations in infant patients with mbshh in our study , which is consistent with previous reports31 ) , and children older than 3 years for germline tp53 mutations . 
based on these findings we recommend conservative ordering of genetic tests in these patient groups ( eg , those with familial history of brca - associated cancers or mutational signatures are suggestive of hr deficiency specifically signatures 3 and 8 , the latter of which has previously been reported to be associated with breast cancer ) .32 genetic counselling and testing for germline palb2 and brca2 mutations in paediatric patients has so far been pursued only in case of suspected fanconi anaemia . 
 by use of integrative genomic analyses , we showed that heterozygous mutations in brca2 and palb2 are associated with an increased risk of medulloblastoma and of hr - deficient tumours . 
all identified heterozygous germline mutations are rare in the general population ( minor allele frequency < 001% ) and were classified in most patients as ( likely ) pathogenic in clinvar . 
magnusson and colleagues33 reported that families with germline mutations in brca2 had an increased prevalence of vol 19 june 2018 articles childhood tumours compared with population - based control families . 
for example , it was shown that cells from heterozygous palb2 mutation carriers exhibited an aberrant dna replication stress response and increased amounts of spontaneous genomic instability , 34 and analysis of double - strand break repair outcomes35 revealed a shift towards error - prone dna repair pathways . 
 furthermore , one study36 presented evidence showing that naturally occurring concentrations of formaldehyde , a product of cellular metabolism , can selectively deplete brca2 via proteasomal degradation and induce genomic instability . 
moreover , consequent identification of paediatric patients with heterozygous germline mutations in palb2 and brca2 will be valuable to further evaluate whether hr - deficient tumours show a particularly favourable response to standard platinum - based chemotherapy and whether they might benefit from combination therapies with parp inhibitors . germline mutations in tp53 accounted for the highest proportion of genetic cases among paediatric patients in the mbshh subgroup . 
this finding underscores the need for a dedicated treatment protocol , which is being prepared by the international society of paediatric oncology pnet 5 medulloblastoma study group and by an international registry for this high - risk patient group.37 additionally , clinical surveillance of germline tp53 mutation carriers has been shown to result in earlier detection of tumours and therefore improved long - term survival.38 we also observed rare and damaging germline mutations with potential clinical relevance in additional genes based on loss of heterozygosity analysis and somatic mutation patterns ( eg , atm and pten )  . 
a single patient harboured a heterozygous germline msh6 mutation in our discovery cohort ; however , the meaning of this observation remains uncertain owing to the absence of tumour material for molecular analyses . our study does have some limitations . 
because of the multiple ( and in part heterogeneous ) cohorts used in our study , familial history of cancer could not be obtained in a standardised form for all patients carrying a genetic predisposition . 
 larger cohort sizes in further studies will be necessary to assess the impact of germline mutations on clinical outcomes within molecular subgroups as well as relative to patients who develop sporadic medulloblastoma due to somatic mutations in the same set of genes ( eg , ptch1 , sufu , and tp53 )  . 
 furthermore , we note that our rare variant burden analysis against exac was restricted to regions covered by whole - exome sequencing , was restricted to genes previously in cancer predisposition , and excluded pathogenic germline structural variants . 
 although these steps aimed to reduce potential biases from analysing heterogeneous sequencing cohorts , we cannot rule out that particular classes of germline variation might have been under - represented . 
finally , it is also possible that additional genes are involved in medulloblastoma predisposition , which were not previously associated with hereditary cancer syndromes . involved contributors jok , pan , smp , and smw contributed to manuscript preparation and to study design . 
ag , cb , cdb , cpk , crb , cs , dm , fmdlv , kbg , kwp , and sss contributed to data interpretation . declaration of interests smw reports grants from the european molecular biology organization ( embo ) and from the swiss national science foundation , during the conduct of the study . 
mf reports grants from the swedish research council , the swedish council for health , working life and welfare , the swedish cancer society , the swedish childhood cancer foundation , and the swedish radiation protection authority , during the conduct of the study . 
cdb reports grants from the national institutes of health ( nih ) , during the conduct of the study ; grants from the university of miami , financial activities from the university of chicago ; university of california , los angeles ; hugo ; new york genome center ; university of iowa ; rockefeller university ; alexandria ; fh foundation ; concert genetics ; national autonomous university of 796 vol 19 june 2018 articles mexico ; mexican institute of social security ; colorado state university ; macarthur foundation ; and gordon conference ; and personal fees from cdb consulting ltd , personalis , inc , 23andme roots into the future project , ancestry.com , liberty biosecurity , med - tek , identifygenomics llc , mars inc , etalon inc , fish & richardson pc , eden roc , hypatia , the nicklaus childrens hospital research institute , knox medical , arc bio llc , embark veterinary , digitalis ventures , humancode , web shield , and luna dna , outside the submitted work . 
all other authors declare no competing interests . acknowledgments this project was supported by the pedbrain tumor project contributing to the icgc , funded by german cancer aid ( 109252 ) , the german federal ministry of education and research ( bmbf ; 01ku1201a and 01ku1201c ) , and additionally through bmbf grants biotop ( 01ek1502a and 01ek1502b ) , icgc - data mining ( 01ku1505f ) , medsys ( 0315416c ) and ngfnplus ( 01gs0883 )  . 
pan is the recipient of a roman - herzog postdoctoral fellowship ( hertie foundation ) , v foundation v scholar award , sontag foundation distinguished scientist award , and is a pew - stewart scholar for cancer research ( alexander and margaret stewart trust )  . 
mdt is supported by the garron family chair in childhood cancer research , and grants from the cure search foundation , the national institutes of health ( r01ca148699 and r01ca159859 ) , the pediatric brain tumor foundation , the terry fox research institute , and brainchild . 
tissue banking was supported by funds from the faculty of medicine , masaryk university ( brno , czech republic ) and kz was supported by the project azv 15 - 30657a from the ministry of health of the czech republic . 
the medulloblastoma advanced genomics international consortium ( or magic ) project is financially supported by genome canada , genome bc , terry fox research institute , ontario institute for cancer research , pediatric oncology group ontario , funds from the family of kathleen lorette and the clark h smith brain tumour centre , montreal childrens hospital foundation , hospital for sick children : sonia and arthur labatt brain tumour research centre , chief of research fund , cancer genetics program , garron family cancer centre , brain child , mdts garron family endowment , and bc childhood cancer parents association . 
we thank the dkfz genomics and proteomics core facility , andrea wittmann ( pediatric glioma research group , dkfz , heidelberg , germany ) , laura sieber ( division of pediatric neurooncology , dkfz ) , rolf kabbe ( division of theoretical bioinformatics , dkfz ; department for bioinformatics and functional genomics , institute for pharmacy and molecular biotechnology , and bioquant , heidelberg university , heidelberg , germany ) , matthias bieg ( division of theoretical bioinformatics , heidelberg center for personalised oncology , dkfz ) , matthias schlesner ( bioinformatics and omics data analytics , dkfz ) , and bernd klaus ( genome biology unit , european molecular biology laboratory [ embl ] , heidelberg , germany ) for technical support . 
this work is dedicated to prof dr enno kleihauer , who introduced molecular genetics to the field of neuro - oncology in the early 1980s , and who was one of the most influential paediatric haematologist - oncologists in germany and beyond . reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com despite state of the art normal imaging , 37 ( 52% ) of 71 patients who underwent second - look laparotomy had macroscopic peritoneal disease reported by the surgeon , and in four patients this disease was not resectable . 
perhaps surprisingly , only 26 ( 70% ) of the 37 cases of metastases suspected by the surgeons were confirmed pathologically , presumably due to chemotherapy down staging or alternative diagnoses.9 the main finding in prophylochip was no difference in disease - free survival between patients receiving active surveillance versus second - look surgery plus hipec . 
after a median follow - up of 508 months ( iqr 470548 ) , 3 - year disease - free survival was 53% ( 95%ci 4164 ) in the surveillance group versus 44% ( 3356 ) in the second - look surgery group ( hazard ratio 097 [ 95% ci 061156 ] ; p = 082 )  . 
this trial has finally answered a longstanding question : should groups at high risk of colorectal peritoneal metastases have second - look surgery ? the answer is clearly no , provided that primary surgery has been optimal and complete . 
 recent results of randomised trials6 , 8 allows for important observations : complete tumour removal by surgeons experienced in the principles and practice of cytoreductive surgery is crucial ; low - volume imaging does not detect peritoneal disease ; and high - risk features can predict peritoneal recurrence . 
congratulations to my french colleagues for showing in two elegant complex trials that optimal surgery is the best treatment for colorectal peritoneal metastases and that second - look surgery is not required , provided that primary surgery is optimal . 
perhaps follow - up should be intensified for high - risk groups , but all oncologists , surgeons , and combining these two the multidisciplinary teams should be very aware that no imaging modality is sensitive , or specific , for peritoneal metastases . 
second - look surgery plus hyperthermic intraperitoneal chemotherapy versus surveillance in patients at high risk of developing colorectal peritoneal metastases ( prophylochipprodige 15 ) : a randomised , phase 3 study . 
proc am soc clin oncol 2018 ; 36 ( suppl ) : lba3503 . panagiotopoulou ig , shah n , rowaiye b , chandrakumaran k , carr nj , moran b . 
 colorectal dis 2019 ; 21 : 88693 . final results of the uk age trial on breast cancer screening age in the lancet oncology , the findings from a 23 - year follow - up of the uk age trial are presented by stephen duffy and colleagues.1 no difference mortality from breast cancer was found between the group that began yearly mammography screening at age 3941 years until they entered the national health service ( nhs ) breast screening programme at age 5052 years , and a group that did not begin mammography screening until they entered the nhs breast screening programme ( 126 deaths vs 255 deaths occurring after more than 10 years of follow - up ; relative rate 098 [ 95% ci 079122 ] ; p = 086 )  . the trial was well conducted , utilising the facilities of the centres already participating in the nhs breast screening programme that had the capacity to screen additional women . 
as participating women were flagged with the nhs central register , mortality from breast cancer in the compared groups could be accurately ascertained . unfortunately , the debate over whether to initiate breast screening at age 40 or 50 years will not have published online august 12 , 2020 s1470 - 2045 ( 20 ) 30428 - 9 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on september 1 , 2020 see articles page 1165 vol 21 september 2020 1125 comment been resolved by the uk age trial , as the lack of a control group who were not offered screening at any age precluded determining whether either group in the trial derived any benefit . 
although there is the possibility that in the intervention group ( screening initiated at age 3941 years ) some person - years were saved by the earlier detection of breast cancer than in the control group , overall there was no mortality reduction in the intervention group compared to the control group by the end of follow - up . 
those who favour screening will be left with a conundrum , but those who believe that mammography screening has little or no benefit will feel their views have been justified . one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
we also confirmed that adjuvant chemotherapy was used , but found no benefit from mammography screening , 6 and instead found a harmful effect , especially from overdiagnosis.7 thus , although duffy and colleagues should be com mended for providing long - term data from a well conducted study , it could be argued that breast screening with mammography should not be initiated at any age , but rather women should be encouraged to practise breast awareness , with mammography used as a diagnostic test , while always remembering that in young women mammography can be negative even in the presence of physically detectable breast cancer . 
geneva : world health organization , 2017 . chemoradiotherapy plus a smac mimetic for locally advanced squamous cell carcinoma of the head and neck published online august 3 , 2020 s1470 - 2045 ( 20 ) 30383 - 1 see articles page 1173 led to the availability of checkpoint inhibitors has substantial progress in the treatment of patients with recurrent or metastatic squamous cell carcinoma of the head and neck . 
 however , the treatment outcome of locoregionally advanced squamous cell carcinoma of the head and neck , traditionally associated with alcohol and nicotine 1126 vol 21 september 2020 comment not old , just older : considering age in cancer care in 2019 , the number of people older than 65 years worldwide surpassed that of children younger than 5 years for the first time . 
yet , older patients are undeniably under - represented and even discriminated against in cancer care . comorbidities in patients aged 65 years or older can preclude their inclusion in cancer clinical trials . 
 one analysis quantified this fact : people in this age group accounted for just 29% of patients included in colon cancer trials and 15% of those in breast cancer trials . 
another study showed larger age disparities between study participants and the incident disease population in trials with industry sponsorship than in those not sponsored by industrya bias that one could argue cynically encourages more positive results . when patient selection is so stringent , it calls into question whether the study population is representative . 
can results from such trials be truly representative of the average patient with cancer ? as an example , although the incidence of colorectal cancer is increasing in younger people , with an average age of onset of 68 years in men and 72 years in women , a standard upper limit of 65 years can lead to the exclusion of many diagnosed cases , leaving an atypical population with an earlier onsetand perhaps more aggressiveform of the disease . 
therefore , age inclusion criteria in trials that are dependent and relevant to the cancer type should be used . although a move away from paternalism in cancer care is essential , this shift has gone too far in some areas . 
the number of major upper - abdominal resections done in octogenarians with cancer ( aged 8089 years ) was found to have risen in 200111 , despite an increased morbidity risk . 
patient choice might be a factor in the rising incidence of complex surgeries , so it is vital that the risks and benefits of all clinical options are clearly communicated to patients , especially those at greater risk of complications , so that the best choice is made for each individual irrespective of chronological age . with under - representation in trials on one end of the scale and potential overuse of surgery on the other , the ideal scenario for older patients lies somewhere in between . 
increasingly , clinicians are realising that use of chronological age , created arbitrarily by sociolegal norms , can be poorly representative of an individuals health status , and instead are opting to use geriatric assessments tools to evaluate older patients health to inform cancer care . 
 the american college of surgeons coalition for quality in geriatric surgery have also developed a new geriatric surgery verification programme , which sets out standards that hospitals should meet to improve surgical outcomes for older patients . 
but with a report from the community oncology alliance showing that some 423 us community cancer clinics had closed between 2008 and 2018 , and that 45 practices reported sending medicare patients to other clinics for cancer care , neglect of older patients is clearly an ongoing concern . 
thus , better collaboration and coordination between all health - care providers is needed to develop personalised evidence - based treatment plans delivered in the right place at the right time . it can be easy to perceive those over a certain age as weak or frail . 
but remove two letters from the word elderly and you will arrive at an entirely different word , elder with its connotations of knowledge and wisdo older patients should not be viewed as fragile or side - lined , but should be recognised as a population from whom much can be learned . 
the lancet oncology for the lancet oncology series on geriatric oncology see series / geriatric - oncology for the study on geriatric patients in cancer clinical trials see proc am soc clin oncol 2019 ; 37 ( suppl ) : e23032 ( abstr ) for the study on age disparities in trial participants by industry sponsorship see jama oncol 2019 ; published online june 3 . 
 antibodies lancet oncol 2015 ; 16 : 73839in this comment , the chemotherapy backbone used in the squire trial was incorrectly referred to as gemcitabine and carboplatin in four instances in the third paragraph ; it should read gemcitabine and cisplat these corrections have been made to the online version as of june 29 , 2015 , and the printed version is correct . torri v , broggini m , garassino mc . 
lancet oncol 2015 ; 16 : 74648the seventh sentence of the nal paragraph of this comment should read : results for leu858arg are still inconclusive because although progression - free survival is higher in patients given all egfr inhibitors versus chemotherapy , overall survival seems to be better with chemotherapy than with afatinib for these patients . 
 this correction has been made to the online version as of june 29 , 2015 , and the printed version is correct . for future lowy dr , herrero r , hildesheim a , for the participants in the iarc / nci workshop on primary endpoints for prophylactic hpv vaccine trial . 
 lancet oncol 2015 ; 16 : e22633 in the panel , in the section on the quadrivalent vaccine for men , the second bullet point should read : approved in the eu by the ema for the prevention of vaccine - type related anal lesions and for the prevention of vaccine - type related genital warts ( ages 9 )  . 
lancet oncol 2015 ; 16 : this news e316in item , the nal two sentences of paragraph 3 read : according to the scale , treatment late - stage egfr - mutated nonsquamous lung cancer with erlotinib provides a gain in progression - free survival ( pfs ) of 85 months ( hazard ratio [ hr ] 016 [ 95% ci 010026 ] ) and an improvement in quality of life compared with carboplatin and gemcitabine , earning an esmo - mcbs score of 4 / 5 . 
in contrast , the same drug when used to treat metas tatic pancreatic cancer provides an overall gain of only 9 days compared with chemotherapy treatment , and had a score of 1 / 5 . 
this correction has been made as of june 12 , 2015 . vol 16 july 2015 e313 without chemotherapy , we must continue to focus not only on quantity of survival , but also its quality . osoba d , rodrigues g , myles j , zee b , pater j . 
health - related quality of life with nbl has received institutional research funding from array , astrazeneca , guardant health , merck sharp & dohme , pfizer , and roche ; honoraria ( continuing medical education lectures ) from bristol - myers squibb , merck sharp & dohme , and roche ; and consulting fees from the canadian agency of drugs and technologies in health and excovery . 
asf declares no competing interests . andrea s fung , * natasha b leighl natasha.leighl@uhn.ca division of medical oncology / hematology , princess margaret cancer centre , university of toronto , on m5g 1z5 , canada ( asf , nbl ) gandhi l , rodrguez - abreu d , gadgeel s , et al . 
patient - reported outcomes following pembrolizumab or placebo plus pemetrexed and platinum in patients with previously untreated , metastatic , non - squamous non - small - cell lung cancer ( keynote - 189 ) : a multicentre , double - blind , randomised , placebo - controlled , phase 3 trial . 
j clin oncol 2006 ; 24 : 383137 . carboplatin - paclitaxel or nab - paclitaxel with or without pembrolizumab in patients with metastatic squamous non - small - cell lung cancer . 
health - related quality - of - life results for pembrolizumab versus chemotherapy in advanced , pd - l1 - positive nsclc ( keynote - 024 ) : a multicentre , international , randomised , open - label phase 3 trial . 
nivolumab plus ipilimumab versus chemotherapy as first - line treatment in advanced non - small - cell lung cancer with high tumour mutational burden : patient - reported outcomes results from the randomised , open - label , phase iii checkmate 227 trial . 
development of the functional assessment of cancer therapy - immune checkpoint modulator ( fact - icm ) : a toxicity subscale to measure quality of life in patients with cancer who are treated with iccancer 2020 ; published online jan 8 . 
j med econ 2018 ; 21 : 1191205 . egfr antibodies in resectable metastatic colorectal liver metastasis : more harm than benefit ? the current standard of care for resectable liver - limited colorectal cancer is perioperative chemotherapy followed by curative resection , based on the eortc trial , which showed a modest improvement in 3 - year progressionfree survival.1 since the addition of a biological agent to systemic therapy leads to increased proportions of patients achieving a response in the metastatic setting , a logical subsequent trial would investigate the role of biological agents in the perioperative setting . in the new epoc study , the results of which were published by john a bridgewater and colleagues in the lancet oncology , patients with resectable kras exon 2 wild - type colorectal liver - limited metastases were randomly assigned to perioperative chemotherapy ( oxaliplatin plus fluorouracil , oxaliplatin plus capecitabine , or irinotecan plus fluorouracil ) with or without addition of the epidermal growth factor receptor ( egfr ) antibody cetuximab.2 , 3 although the concept was rational and the trial well designed , the initially reported results were rather unexpected and controversial.3 although the addition of cetuximab to chemotherapy numerically increased the proportion of patients with a response , it showed shorter progression - free survival , with a hazard ratio of 148 ( 95% ci 104212 ; p = 0030 ) in patients given chemotherapy with cetuximab versus those who had chemotherapy alone . 
 these results led to a controversial debate reflected in an exchange of letters in a different journal.4 in their longterm analysis , bridgewater and colleagues now confirm the initial results , showing shorter overall survival in patients given chemotherapy plus cetuximab compared with patients given chemotherapy alone ( 554 months [ 95% ci 435715 ] vs 810 months [ 596 to not reached ] ; hr 145 , 95% ci 102205 ; p = 0036 )  . 
finally , the results were largely driven by post - recurrence survival , suggesting either the development of a more aggressive disease phenotype or imbalances in post - recurrence treatment approaches . since the initial publication of the study , new insights into prognostic and predictive molecular signatures of metastatic colorectal cancer have emerged . 
in rightsided colon cancer , first - line cetuximab has shown to published online january 31 , 2020 s1470 - 2045 ( 20 ) 30003 - 6 see articles page 398 324 vol 21 march 2020 comment decrease overall survival compared with bevacizumab.5 additionally , several studies suggest detrimental effects ( ie , shorter survival ) of anti - egfr therapy in patients with other molecular alterations such as non - kras exon2 ras mutations , braf mutations , her2 amplifications , and microsatellite in new epoc , no instability.6 significant differences were observed in the distribution of ras / raf mutations between treatment groups , but this observation does not rule out imbalances in other molecular alterations that could have affected sensitivity to egfr antibody therapy . 
moreover , the heterogeneity of the systemic therapy in the perioperative setting could be seen as a limitation since the detrimental effect was mainly seen in patients treated with oxaliplatin plus fluorouracil plus cetuximab . 
importantly , only 10% of the patients within the cetuximab group received cetuximab as part of subsequent palliative therapy upon recurrence compared with 30% of patients in the chemotherapy alone groupa factor that might have led to lower overall survival because of decreased exposure to cetuximab upon recurrence.2 the authors offer the expression of the microrna mir - 313p in primary colorectal cancer of patients with metastatic disease treated with cetuximab or panitumumab as a potential explanation for resistance to egfr inhibition and disease progression.7 some preclinical models suggest an epithelialmesenchymal - like transition as potential mechanism of anti - egfr therapy.8 in vitro , a correlation between e - cadherin expression and growth inhibition by egfr inhibitors was observed in colorectal cancer cells . 
several other alterations , such as presence of met amplification have been shown to play a role in antiegfr resistance.8 these hypotheses could point to potential biological mechanisms for cetuximabs association with poor outcomes in early - stage disease . 
in stage iii colon cancer ( according to the american joint committee on cancer staging system ) , the addition of cetuximab to adjuvant fluorouracil plus oxaliplatin showed no difference in disease - free survival , although the hazard ratio point estimate suggested a detriment in survival , independent of ras mutation status.9 multiple preclinical studies suggest that a substantial portion of the effects attributed to egfr antibody treatment could be based on indirect effects beyond cancer cells , including the tumour microenvironment and immunecancer cell interactions.10 various mechan isms of resistance to anti - egfr therapy exist in colorectal cancer , ranging from molecular and immune alterations to histological transformations , allowing for intratumoral heterogeneity , independent of the ras mutation status . certainly , the study has some limitations surrounding surgical quality , including imbalances in the number of patients not undergoing surgery ( 21 in the chemotherapy plus cetuximab group vs 15 in the chemotherapy alone group ) and the use of ablation rather than resection ( 11 vs 5 )  . 
despite these limitations , surgery was done in high - volume expert centres and randomisation conceivably helped to balance these factors . we commend the authors for completing a large interdisciplinary trial addressing important clinical and biological questions . 
although historically good responses have been achieved with more aggressive therapies in the advanced setting , cetuximab and cytotoxic therapy ( oxaliplatin plus fluorouracil ) in resectable stage iv and iii colorectal cancers apparently might have a detrimental effect on survival . at this point in time , egfr antibodies should not be used as a component of neoadjuvant or perioperative therapy in resectable stage iv colorectal cancer . 
although we believe that egfr antibodies added to chemotherapy still play a role in the preoperative conversion setting , when high anatomical response are desired , we caution against their use as postoperative therapy after resection of metastatic disease . 
additional studies with predefined subgroups ( eg , sided ness or different molecular and immune profiles ) and novel combination treatment strategies are warranted in patients with operable colorectal liver metastases . we declare no competing interests . copyright 2020 the author ( s )  . 
perioperative folfox4 chemotherapy and surgery versus surgery alone for resectable liver metastases from colorectal cancer ( eortc 40983 ) : long - term results of a randomised , controlled , phase 3 trial . 
lancet oncol 2013 ; 14 : 120815 . vol 21 march 2020 comment published online january 27 , 2020 s1470 - 2045 ( 20 ) 30009 - 7 see articles page 412 bridgewater ja , pugh sa , maishman t , et al . 
systemic chemotherapy with or without cetuximab in patients with resectable colorectal liver metastasis ( new epoc ) : long - term results of a multicentre , randomised , controlled , phase 3 trial . 
should the results of the new epoc trial change practice in the management of patients with resectable metastatic colorectal cancer confined to the liver ? j clin oncol 2015 ; 33 : 24143 . venook ap , niedzwiecki d , lenz hj , et al . 
effect of first - line chemotherapy combined with cetuximab or bevacizumab on overall survival in patients with kras wild - type advanced or metastatic colorectal cancer : a randomized clinical trial . 
cancers ( basel ) 2019 ; 11 : e1089 . tas - 102 plus bevacizumab : a new standard for metastatic colorectal cancer ? from oxaliplatin and for patients with surgically unresectable metastatic colorectal cancer , a continuum of care is offered to improve their overall outcome . 
few treatment options irinotecan - based exist apart therapies ; even fewer exist for patients with ras mutations , who account for 3060% of all patients with metastatic colorectal cancer.1 when the oral agent , tas - 102 , was approved by the us food and drug administration in 2017 , it offered another potential option for patients with surgically unresectable , metastatic colorectal cancer.2 often incorrectly touted as a modified oral fluorouracil , tas - 102 differentiates itself by being comprised of two components : trifluridine , a nucleoside analogue , and tipiracil hydrochloride , a in a thymidine phosphorylase 10 : 05 ratio . 
the phase 3 recourse trial3 randomly assigned patients ( 2 : 1 ) with metastatic colorectal cancer ( n = 800 ) to receive either tas - 102 ( 35 mg / m , days 15 and 812 ) or placebo . 
the primary endpoint of overall survival was met , with longer median overall survival in the tas - 102 group ( 71 months vs 53 months in the placebo group ) with a hazard ratio ( hr ) of 068 ( 95% ci 058081 ; p < 0001 )  . 
progression - free survival was also longer in the tas - 102 group than in the placebo group ( 20 months vs 17 months [ 048 , 041057 ; p < 0001 ] ) ; and a response was achieved in 16% of patients in the tas - 102 group versus 04% in the placebo group ( p = 029 )  . 
the most common adverse event inhibitor , combined in the tas - 102 group was grade 3 or 4 neutropenia occurring , in 359% of patients . despite its oral formulation and ease of administration , in the metastatic overall enthusiasm for tas - 102 colorectal cancer treatment arsenal was subdued because the overall survival benefit was only 18 months compared with placebo in a heavily pretreated patient population . 
 furthermore , this improvement in overall survival did little to distinguish tas - 102 from the oral multikinase inhibitor regorafenib ( absolute improvement in overall survival of 14 months compared with placebo )  . 
the average cost for one tas - 102 treatment cycle is reported to be us$10 94770 for an individual with a body surface area of 17 m.4 in their article in the lancet oncology , per pfeiffer and colleagues5 report the results from the first randomised phase 2 study comparing tas - 102 plus bevacizumab with tas - 102 alone in patients with refractory metastatic colorectal cancer , done in demark . 
unique to this setting is that anti - vegf therapy with aflibercept and ramucirumab in the second - line setting , and regorafenib in the refractory setting , are not approved in denmark . 
the treatment provided was a standard dose of tas - 102 ( 35 mg / m twice daily on days 15 and 812 ) alone or in combination with 5 mg / kg bevacizumab on days 1 and 15 of each 28 - day cycle . 
in the eortc trial , eligible women had biopsy - proven international federation of gynecology and obstetrics ( figo ) stage iiic or iv invasive epithelial tubo - ovarian carcinoma . 
the main aim of the pooled analysis was to show noninferiority in overall survival with neoadjuvant chemotherapy compared with upfront debulking surgery , using the reverse kaplan - meier method . 
tests for heterogeneity were based on cochrans q heterogeneity statistic . findings data for 1220 women were included in the pooled analysis , 670 from the eortc trial and 550 from the chorus trial . 
55 ( 5% ) women had figo stage iiiiib disease , 831 ( 68% ) had stage iiic disease , and 230 ( 19% ) had stage iv disease , with staging data missing for 104 ( 9% ) women . 
in the entire population , no difference in median overall survival was noted between patients who underwent neoadjuvant chemotherapy and upfront debulking surgery ( 276 months [ iqr 141513 ] and 269 months [ 127501 ] , respectively ; hazard ratio [ hr ] 097 , 95% ci 086109 ; p = 0586 )  . 
median overall survival for eortc and chorus patients was significantly different at 302 months ( iqr 157537 ) and 236 months ( 105469 ) , respectively ( hr 120 , 95% ci 106136 ; p = 0004 ) , but was not heterogeneous ( cochrans q , p = 017 )  . 
women with stage iv disease had significantly better outcomes with neoadjuvant chemotherapy compared with upfront debulking surgery ( median overall survival 243 months [ iqr 141476 ] and 212 months [ 100364 ] , respectively ; hr 076 , 95% ci 058100 ; p = 0048 ; median progression - free survival 106 months [ 79150 ] and 97 months [ 52132 ] , respectively ; hr 077 , 95% ci 059100 ; p = 0049 )  . interpretation long - term follow - up data substantiate previous results showing that neoadjuvant chemotherapy and upfront debulking surgery result in similar overall survival in advanced tubo - ovarian cancer , with better survival in women with stage iv disease with neoadjuvant chemotherapy . 
 we found that survival data from randomised studies had been published for only two trials : the european organisation for research and treatment of cancer ( eortc ) 55971 trial , and the medical research council chemotherapy or upfront surgery ( chorus ) trial . 
both trials concluded that neoadjuvant chemotherapy followed by interval debulking surgery was not inferior to primary debulking surgery followed by chemotherapy in patients with international federation of gynecology and obstetrics ( figo ) stage iiic or iv ovarian carcinoma . 
in addition to these two trials , the scorpion and jcog0602 randomised trials concluded that perioperative morbidity was better with interval debulking after neoadjuvant chemotherapy than after primary debulking surgery . added value of this study we report a per - protocol pooled analysis of individual patient data from the eortc 55971 and chorus randomised trials , to examine the long - term outcomes in patients with advanced ovarian cancer treated with neoadjuvant chemotherapy followed by interval debulking versus upfront debulking surgery followed by chemotherapy . 
we also did subgroup analyses on the basis of stratification factors that were common to both trialsie , randomising centre , largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 cm to 20 cm , and > 20 cm ) , and clinical figo stage . 
our analysis shows that , with longer median follow - up , both neoadjuvant chemotherapy followed by interval debulking surgery and upfront debulking surgery followed by chemotherapy are associated with similar overall survival and progression - free survival . 
we also show that neoadjuvant chemotherapy is associated with better progression - free survival and overall survival in women presenting with figo stage iv disease , and patients with figo stage iiic disease with extrapelvic metastases smaller than 5 cm have better progression - free survival after upfront debulking . implications of all the available incidence earlier studies showed already that overall survival is similar in patients with stage iiiciv tubo - ovarian cancer treated with neoadjuvant chemotherapy followed by interval debulking surgery , compared with upfront debulking surgery followed by chemotherapy . 
participants in this study had figo stage iiic or iv tubo - ovarian cancer with metastatic disease with a high tumour burden at presentation , and many had a poor performance status . 
this individual patient data pooled analysis suggests that neoadjuvant chemotherapy should be the standard of care for most patients with stage iv tubo - ovarian cancer and that primary surgery should only be undertaken in exceptional circumstances in patients with figo stage iv disease on an individual basis . 
however , women with figo stage iiic disease with extrapelvic metastases smaller than 5 cm had a significantly better progression - free survival with upfront debulking surgery than with neoadjuvant chemotherapy , so these patients should first be considered for primary debulking surgery . 
in 2010 , the european organisation for research and treatment of cancer ( eortc ) published the first findings from a trial comparing neoadjuvant chemotherapy followed by interval debulking surgery with upfront debulking surgery ( eortc 55971 ) .4 this study showed both treatment strategies had similar overall survival and progression - free survival in women with international federation of gynecology and obstetrics ( figo ) stage iiic or iv tubo - ovarian cancer , and operative and postoperative morbidity was lower with neoadjuvant chemotherapy . 
these results were later substantiated in the randomised medical research council ( mrc ) chemotherapy or upfront surgery ( chorus ) trial , 5 leading to the acceptance of neoadjuvant chemotherapy followed by interval debulking surgery as an alternative to upfront debulking surgery in women with stage iiic and iv tubo - ovarian cancer.6 however , the selection of women with advanced ovarian cancer for neoadjuvant chemotherapy or upfront debulking surgery remains controversial.7 therefore , we did a pooled analysis of the long - term outcomes of the eortc 55971 and chorus trials to identify subgroups of women who could benefit from neoadjuvant chemotherapy in this setting . 
 that might benefit see online for appendix vol 19 december 2018 1681 articles n the trial steering committees of both the eortc and chorus trials agreed on a strategy for database pooling and analyses ; both trials had similar eligibility criteria , treatment , and examination schedules to facilitate pooling 2 studies prospectively selected for database pooling 1220 patients records screened 670 patients enrolled in eortc 550 patients enrolled in chorus 1220 individual patient data included in synthesis ( pooled analysis ) figure 1 : prisma flow diagram eortc = european organisation for research and treatment of cancer 55971 trial . 
eortc = european organisation for research and treatment of cancer 55971 trial . table 1 : baseline characteristics , by study eligibility criteria for these trials and their study designs have been reported elsewhere.4 , 5 the appendix includes the protocols of the eortc ( pp 1270 ) and chorus ( pp 71117 ) trials . 
a list of recruiting sites and investigators is also in the appendix ( pp 122124 )  . briefly , in the eortc trial , 4 women were eligible if they had biopsy - proven figo stage iiic or iv invasive epithelial ovarian , primary peritoneal , or fallopian tube carcinoma . 
 if a biopsy specimen was not available , fine - needle aspiration showing an adeno carcinoma was acceptable under the following conditions : presence of a pelvic adnexal mass , presence of extrapelvic metastases of 2 cm or larger ( measured during dia gnostic laparoscopy or laparotomy , or if laparoscopy or laparotomy was not done , on the basis on ct findings ) , and a ratio of cancer antigen 125 ( ca125 ) to carcino embryonic antigen ( cea ) greater than 25 ; biopsy findings were mandatory for inclusion in the trial if any of these three criteria were not present . 
the size of the largest metastasis was estimated on the basis of ct imaging only in the chorus trial . in both trials , participants were randomly allocated to receive either upfront debulking surgery followed by at least six courses of platinum - based chemotherapy , three courses of neoadjuvant platinum - based chemotherapy followed by interval debulking surgery followed by at least three additional courses of platinumbased chemotherapy.4 , 5 in women allocated to receive upfront debulking surgery whose surgery was completed without optimum cytoreduction , interval debulking surgery was permitted , and these patients were included for analyses in the upfront debulking surgery group . 
in the eortc trial , randomisation used a minimisation technique and was stratified by the following factors : institution , method of biopsy ( image - guided , laparoscopy , laparo tomy , or fine - needle aspiration ) , figo stage iiic or iv disease , and largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 to 20 cm , or > 20 cm )  . 
in the chorus trial , randomisation used a minimisation method with a random element , which stratified patients according to randomising centre , largest radiological tumour size , clinical figo stage , and prespecified chemotherapy regimen . 
for details on size of residual tumour , residual tumour per country , type of surgery , number of cycles and type of chemotherapy , and time to ( re ) initiation of chemotherapy , we refer to the original reports.4 , 5 procedures our analysis was designed in 2003 by the chief investigators of the eortc and chorus trials ( iv and sk ) and members of the eortc and mrc trial managing committees , according to a formal protocol . 
we derived median follow - up with the eortc standard method , which uses the reverse kaplan - meier method and calculates time - toevents for all patients ; in the original chorus paper , however , only the median duration of follow - up for surviving patients was calculated . the primary outcome of our pooled analysis was overall survival , and the prespecified secondary endpoint was progression - free survival . 
prespecified subgroup analyses were done on the basis of stratification factors that were common to both trials : randomising centre , largest tumour size ( excluding ovaries ) before surgery ( < 5 cm , 5 to 10 cm , > 10 to 20 cm , and > 20 cm ) , and clinical figo stage . 
definitions for overall survival and progression - free survival have been published elsewhere.4 statistical analysis patients data from both trials were updated and merged into one database ( database lock for eortc was on june 6 , 2015 ; for chorus , june 3 , 2014 ) , which contained 1220 patients with tubo - ovarian cancer who had been randomly allocated to receive either upfront debulking surgery or neoadjuvant chemotherapy . 
assuming a median overall survival of 3 years , this number of events allowed assessment of noninferiority , 9 , 10 with a one - sided type i error of 005 and a power of 80% , with inferiority regarded as an increase of more than 1819% in hazard . 
applying a two - sided test of superiority at 5% , the dataset would allow detection of an 18% increase in hazard with 80% power . the principal analysis was done on an intention - totreat basis . 
 in those subgroups for which the proportional hazards assumption was violated , restricted mean survival times were calculated to provide a more useful general measure than the hr estimates and their 95% cis obtained from a cox proportional hazards model to report the average survival times between the two treatment groups.11 multivariable time - to - event analyses were done using a cox proportional hazards model , with univariate screening followed by a multi variable stepwise selection procedure.12 all baseline characteristics and results were checked for homogeneity between the two studies and stratified per trial when possible . 
all analyses were done with sas , version 9.4. role of the funding source the funders of the studies had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 upfront debulking surgery neoadjuvant chemotherapy hazard ratio 076 , 95% cl 058100 overall score stratied for study , p = 0048 time after randomisation ( years ) number at risk ( number censored ) upfront debulking surgery neoadjuvant chemotherapy 118 ( 0 ) 11 ( 0 ) 53 ( 2 ) 57 ( 1 ) 13 ( 3 ) 25 ( 3 ) 7 ( 3 ) 8 ( 4 ) 2 ( 5 ) 4 ( 6 ) 0 ( 6 ) 2 ( 8 ) figure 4 : overall survival in patients with figo stage iv disease , by treatment figo = international federation of gynecology and obstetrics . overall survival of 276 months ( iqr 141513 ) and 269 months ( 127501 ) , respectively ( hr 097 , 95% ci 086109 ; p = 0586 ) , and progression - free survival of 116 months ( iqr 79177 ) and 111 months ( 64175 ) , respectively ( hr 098 , 95% ci 087110 ; p = 0688 ; figure 2 )  . 
the lower one - sided 95% cis for overall survival and progression - free survival excluded the 18% non - inferiority margin . overall survival was significantly improved in the eortc trial as compared with the chorus trial ( median 302 months [ iqr 157537 ] vs 236 months [ 105469 ] ; hr 120 , 95% ci 106136 ; p = 0004 ; figure 3 ) , but progression - free survival was similar in the two trials ( median 115 months [ iqr 80170 ] vs 109 months [ 61181 ] ; hr 096 , 95% ci 086108 ; p = 0531 ; appendix p 1 )  . 
cochrans q for heterogeneity was not significant for either overall survival ( p = 017 ) or progression - free survival ( p = 032 )  . median overall survival was significantly different for women with figo stage iv disease compared with those with stage iii and ii cancer ( median 233 months [ iqr 124408 ] vs 300 months [ 156557 ] and 454 months [ 316not reached ] , respectively ; for stage iv vs stage ii , hr 275 , 95% ci 149508 ; for stage iii vs stage ii , 192 , 95% ci 105349 ; p < 00001 for trend ; appendix p 4 )  . 
overall survival was similar with neoadjuvant chemotherapy and upfront debulking surgery in patients with stage iiic disease ( respectively , median 308 months [ iqr 165513 ] and 284 months [ 141557 ] ; hr 104 , 95% ci 090121 ; p = 0569 ; appendix p 5 )  . 
progression - free survival was also similar with neoadjuvant chemotherapy and upfront debulking surgery in patients with stage iiic disease ( median 122 months [ iqr 84183 ] and 117 months [ 75199 ] , respectively ; hr 106 , 95% ci 092122 ; p = 0429 ; appendix p 6 )  . 
however , progression - free survival was significantly better in stage iv disease with neoadjuvant chemotherapy than with upfront debulking surgery ( median 106 months [ iqr 79150 ] vs 97 months [ 52132 ] , respectively ; hr 077 , 95% ci 059100 ; p = 0049 ; appendix p 7 )  . 
additionally , in patients with stage iv tubo - ovarian cancer , neoadjuvant chemotherapy was associated with significantly better overall survival than was upfront debulking ( median 243 months [ iqr 141476 ] vs 212 months [ 100364 ] ; hr 076 , 95% ci 058100 ; p = 0048 ; figure 4 )  . 
in patients with figo stage iiic disease and a largest metastatic tumour size less than 5 cm , progression - free survival was better with upfront debulking surgery than with neoadjuvant chemotherapy ( median 122 months [ iqr 85233 ] vs 117 months [ 83164 ] ; hr 136 , 95% ci 106175 ; p = 0017 ; figure 5a ) forest plots for progression - free survival according to largest metastatic tumour size are in the appendix ( p 9 )  . 
overall survival did not differ between upfront debulking surgery and neoadjuvant chemotherapy ( median 330 months [ iqr 135787 ] and 302 months [ 165513 ] , respec t ively ; hr 126 , 95% ci 096165 ; p = 0092 ; figure 5b )  . 
 1684 vol 19 december 2018 articles age and performance status were not predictive for treatment effect on survival ( appendix p 11 ) discussion this preplanned analysis of updated data from the eortc 55971 and chorus trials assessing neoadjuvant chemotherapy versus upfront debulking surgery in advanced tubo - ovarian cancer ( stage iiic and iv ) shows that , with long - term follow - up , neoadjuvant chemotherapy results in non - inferior overall survival and progression - free survival as compared with upfront debulking surgery . 
the planned non - inferiority margin an increase in hr of more than 1819%was well outside the upper bounds of the 95% cis ( 10% and 9% for progression - free survival and overall survival , respectively )  . 
hence , this pooled analysis with long - term follow - up substantiated previous findings showing that both upfront debulking surgery and neoadjuvant chemotherapy are potential treatment options for patients with figo stage iiic or iv tubo - ovarian cancer . 
 the analysis also showed that patients diagnosed with stage iv disease had significantly better progression - free survival and overall survival with neoadjuvant chemotherapy as compared with upfront debulking surgery , whereas women with stage iiic disease with extrapelvic metastases smaller than 5 cm had significantly better progression - free survival with upfront debulking surgery as compared with neoadjuvant chemotherapy . 
our analyses showed that in women with stage iiic disease and extrapelvic metastases at diagnosis smaller than 5 cm , survival curves for both progressionfree survival and overall survival cross in both treatment groups , indicating deviation from the proportional hazards assumptions . 
obtaining tissue for histological examination is usually possible by use of image - guided biopsy ( usually of the omental cake ) , although a laparoscopic approach is necessary in some cases and provides additional information on disease distribution , which can be included in the decision - making process.1517 both the eortc and chorus trials investigated the timing of surgery in advanced tubo - ovarian cancer , but these trials have been criticised for inclusion of low proportions of patients with no macroscopic disease ( r0 ) and because patients with poor prognosis were enrolled and died sooner than expected independent of the timing of surgery . 
however , at the time the patients in these trials were enrolled , neoadjuvant chemotherapy was not accepted as an alternative to upfront debulking surgery , and furthermore most patients recruited to these trials had extensive figo stage iiic or iv disease that was visible on ct . 
moreover , the scorpion15 and jcog060218 randomised trials compared the morbidity of interval debulking surgery after neoadjuvant chemotherapy with upfront debulking surgery and concluded that interval debulking surgery was associated with improved perioperative morbidity as compared with primary debulking surgery . 
a ran domised trial of neoadjuvant chemotherapy versus primary debulking surgery in advanced tubo - ovarian cancer ( the trust trial , nct02828618 ) is recruiting only in centres with historically documented maximum cytoreduction ( r0 ) in patients with stage iii or stage iv tubo - ovarian cancer of at least 50% . 
the results of this trial are awaited . one limitation of our pooled analysis is that only patients with figo stage iiic and iv disease were included in the eortc trial , whereas in the chorus trial a few patients with stage iiia and stage iiib disease were included . 
furthermore , the number of patients with stage iiic and stage iv disease without residual tumour after upfront debulking surgery was lower in the chorus trial than in the eortc trial . application of the findings of this analysis to the care of women with figo stage iiic or iv tubo - ovarian cancer should be assessed in the context of each patients clinical picture . 
women in the eortc and chorus studies that contributed data to this analysis had metastatic disease with a high tumour burden at presentation , and many had a poor performance status.19 this clinical scenario is not uncommon , and improving outcomes for this population is as important as for patients with better prognostic factors . 
our chemotherapy should be the standard of care for most patients with figo stage iv tubo - ovarian cancer , and primary surgery should only be undertaken in these stage iv patients in exceptional circumstances with easily resectable disease . suggest data contributors all authors contributed to study design and study implementation . 
all authors have seen and approved the final version and , after consultation with the collaborators , agreed to submit for publication . declaration of interests mn reports grants from the medical research council clinical trials unit and cancer research uk , during the conduct of the study . 
 nj reports that the royal united hospital ( his employing institution ) received support from eortc for a clinical trials nurse , who obtained and verified data from some participants in the chorus trial . 
 cm reports personal fees and travel expenses from roche farma espaa , outside the submitted work ; travel expenses from astrazeneca , outside the submitted work ; and travel expenses from pharmamar , outside the submitted work . 
tp reports personal fees and non - financial support from astrazeneca , outside the submitted work ; non - financial support from roche and igea medical , outside the submitted work ; and is co - chief investigator for the icon7 trial of bevacizumab in first - line treatment of patients with advanced ovarian cancer . 
iv , cc , gbk , mkbp , te , gcj , ams , rv , wgm , pbp , gk , ac , gs , nsr , and sk declare no competing interests . acknowledgments this study was supported by grants ( 2u10 ca11488 - 28 through 2u10 ca011488 - 36 ) from the national cancer institute ; and by a donation from the vlaamse liga tegen kanker ( flemish league against cancer ) to the eortc charitable trust . 
funding for a pilot phase of the chorus trial was provided by the royal college of obstetricians and gynaecologists and was supported by core medical research council ( mrc ) clinical trials unit funding . 
in this news article , the rst sentence of the fourth paragraph should have read the researchers found that a daily serving of unprocessed red meat increased the risk of cancer mortality by 10% , whereas a daily serving of processed meat was responsible for a 16% increased risk . 
this correction has been made as of march 26 , 2012 . published online march 26 , 2012 doi : 10.1016 / s14702045 ( 12 ) 70130 - 4 see news page e147 e135 vol 13 april 2012 re ection and reaction with endemic burkitts lymphoma in africa from poor families , and will gladly share more detailed information with interested colleagues . 
the socit franaise doncologie pdiatrique lmb89 protocol : highly e ective multiagent chemotherapy tailored to the tumor burden and initial response in 561 unselected children with b - cell lymphomas and l3 leukemia . 
follow - up is done by dedicated health - care workers who actively seek out patients in their villages . colleagues in kenya and uganda did not accept the invitation to join in the rst study supported by siop , 3 perhaps because the proposed treatment schedule might have been perceived at the time as being worse than established treatment schedules , such as cyclophosphamide , doxorubicin , vincristine , and pred nisolone . 
 however , the french - african pediatric oncology group has now used the same schedule of cyclophosphamide and intrathecal methotrexate in several sub - saharan francophone countries , with comparable e cacy ( jean lemerle , socit franaise doncologie pdiatrique , personal communication ) .6 patients with primary resistance to this treatment , or who relapsed after treatment , have been treated with a 15 - day schedule of cyclophosphamide ( 60 mg / kg ) , vincristine ( 15 mg / m2 ) , and standard - dose intrathecal methotrexate on days 1 , 8 , and 15.7 a third of these patients remain in continuous remission after more than a years follow - up and are considered cured.7 thus , this approach has lead to an overall 1 - year survival of 67% for the group of patients enrolled in these rst - line and refractory studies.4 , 5 , 7 we believe that we have established an e ective , welltolerated , and a ordable treatment option for patients erratum veldeman l , madani i , hulstaert f , de meerleer m , mareel m , de neve w . 
although not legally enforceable , the report is an essential step forward in guiding future drug development , highlighting novel treatment combinations that should speed up drug development , reduce costs , and give patients faster access to new treatments . 
 so what are the qualifying criteria ? the disease must be considered serious and only drugs that have a robust biological rationale for use in combination , as opposed to use individually , should be assessedie , combined agents should have more than additive e cacy or provide a more durable response . 
examples include agents that are inactive alone but potentiate the activity of another drug , drugs against which resistance occurs rapidly when used as a monotherapy but in combination remain e ective for longer , and drugs that target di erent , but complementary , biological pathways . 
two or more marketed drugs have been used very successfully in combination in patients with cancer , and this guidance is the next logical step to prompt novel treatments for drugs that have not been tested and marketed individually , enabling fast - track marketing approval and earlier patient access . 
as the report suggests , co - development will generally provide less data on safety and e cacy , and when safety cannot be tested in phase 1 studies of individual drugs ( eg , because of resistance ) , preclinical evidence , pharmacokinetic data , and biomarker evaluation should be sought . 
 indeed the guidance states that co - development could present a greater risk to the patient than if the drugs are developed initially as single agents . co - development allows innovative adaptive trial designs in which patients treated with single agents that prove ine ective can crossover to the more active combination treatment . 
however , the biggest advance in the development of new treatment regimens could be made if the fda now focused its attention wholeheartedly on facilitating head - to - head comparative e ectiveness studies of drugs already on the marketas called for by the obama administration . 
comparative e ectiveness studiesa current buzz phraserefers to many types of study and is described by the fda as intended to help make decisions more consistent , transparent , and rational , and useful in identifying gaps and uncertainties . 
however , these studies are often large randomised trials , and therefore expensive to complete , and can include a placebo control as well as the head - to - head comparison ( s ) , adding further to the time and e ort involved . 
unsurprisingly , therefore , these are a di cult sell to drug manufacturers who are likely to have little interest in an expensive trial of their latest topselling drug given their vested interests . 
it is now time , however , for the fda to use its considerable in uence more e ectively to incentivise manufacturers to complete such comparative research and provide speci c guidance as to what it expects in terms of the optimum trial design . 
 the rhetoric now needs to be translated into detailed speci cs of how such collaborative and comparative research might be achieved so patients are best served . the us national cancer institute ( nci ) has been at the forefront of cutting edge and practice - changing trial research and will be vital in complementing the fda in its e orts . 
the nci recently re - organised its clinical trials programme following recommendations from the institute of medicine report in april , 2010 , and has consolidated its nine trial groups for adult cancer into fourwith the aim of making the overall programme more cost e ective and e cient . 
by collaborating with the fda on combination drug trials for unmarketed agents , comparative e ectiveness studies for marketed drugs , as well as drug and diagnostic co - development strategies , the nci will ensure patients have access to more treatment options , better personalised treatment , and the latest magic bullets . 
 the lancet oncology vol 12 february 2011 corrections correction to lancet oncol 2014 ; 15 : 1280 correction to lancet oncol 2014 ; 15 : 310 , 311 boughey jc . 
how do the amaros trial results change practice ? lancet oncol 2014 ; 15 : 128081the last sentence of the fourth paragraph of this comment should read with both the amaros1 and z00112 , 3 studies , the data interpreted should be with caution and should not be extrapolated to patients with three , four , or more positive sentinel lymph nodes . 
this correction has been made to the online version as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e395403 weller m , van den bent m , hopkins k , et al , for the european association for neuro - oncology ( eano ) task force on malignant glioma . 
 lancet oncol 2014 ; 15 : e395403 the appendix of this review was incorrect ; the correct appendix has been uploaded as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e591 furlow b . 
 this correction has been made to the online article as of nov 24 , 2014 . conroy t , galais m - p , raoul j - l , et al , for the fdration francophone de cancrologie digestive and unicancer - gi group . 
de nitive chemo radiotherapy with folfox versus uorouracil and cisplatin in patients with oesophageal cancer ( prodige5 / accord17 ) : final results of a randomised , phase 2 / 3 trial . 
the last sentence of the eighth paragraph in the results section should read an endoscopic complete response at week 15 was achieved in 61 ( 53% ) of 115 patients in the folfox group versus 57 ( 48% ) of 120 patients in the uorouracil plus cisplatin group . 
folfox = uorouracil , leucovorin , and oxaliplat recist = response evaluation criteria in solid tumours.21 * 115 patients assessable in the folfox group and 120 assessable in the uorouracil and cisplatin group . table 2 : tumour response to treatment correction to lancet oncol 2014 ; 15 : 1464 sestak i , singh s , cuzick j , et al . 
changes in bone mineral density at 3 years in postmenopausal women receiving anastrozole and risedronate in the ibis - ii bone substudy : an international , doubleblind , randomised , placebo - controlled trial . 
this correction has been made to the online version as of nov 24 , 2014 , and the printed version is correct . c lumbar spine d total hip 05 10 15 20 25 30 35 40 45 50 12% 40% 18% 40% anastrozole placebo baseline 12 months anastrozole placebo 36 months baseline 12 months 36 months vol 15 december 2014 e587 clinical characteristics , outcomes , and risk factors for mortality in patients with cancer and covid - 19 in hubei , china : a multicentre , retrospective , cohort study kunyu yang * , yuhan sheng * , chaolin huang * , yang jin * , nian xiong * , ke jiang * , hongda lu * , jing liu , jiyuan yang , youhong dong , dongfeng pan , chengrong shu , jun li , jielin wei , yu huang , ling peng , mengjiao wu , ruiguang zhang , bian wu , yuhui li , liqiong cai , guiling li , tao zhang , gang wu summary background patients with cancer are a high - risk population in the covid - 19 pandemic . 
we aimed to describe clinical characteristics and outcomes of patients with cancer and covid - 19 , and examined risk factors for mortality in this population . methods we did a retrospective , multicentre , cohort study of 205 patients with laboratory - confirmed severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection and with a pathological diagnosis of a malignant tumour in nine hospitals within hubei , china , from jan 13 to march 18 , 2020 . 
risk factors for mortality were identified by univariable and multivariable logistic regression models . findings between jan 13 and mar 18 , 2020 , 205 patients with cancer and laboratory - confirmed sars - cov - 2 infection were enrolled ( median age 63 years [ iqr 5670 ; range 1496 ] ; 109 [ 53% ] women )  . 
patients with haematological malignancies had poorer prognoses than did those with solid tumours : nine ( 41% ) of 22 patients with haematological malignancies died versus 31 ( 17% ) of 183 patients with solid tumours ( hazard ratio for death 328 [ 95% ci 156691 ] ; log rank p = 00009 )  . 
multivariable regression analysis showed that receiving chemotherapy within 4 weeks before symptom onset ( odds ratio [ or ] 351 [ 95% ci 1161059 ] ; p = 0026 ) and male sex ( or 386 [ 95% ci 157950 ] ; p = 00033 ) were risk factors for death during admission to hospital . interpretation patients with cancer and covid - 19 who were admitted to hospital had a high case - fatality rate . 
it spread rapidly across the world during the following few weeks.1 , 2 as of may 27 , 2020 , 5 491 678 cases have been confirmed worldwide , with 349 190 deaths.3 , 4 in wuhan , the initial centre of the epidemic , 50 340 covid - 19 cases and 3869 deaths have been confirmed , as of may 26 , 2020.5 patients with cancer are a vulnerable population during the covid - 19 pandemic . 
therefore , they are at increased risk of opportunistic infections , developing severe complications , requiring admission to an intensive care unit ( icu ) , or even death.69 liang and colleagues10 analysed data from 18 patients with cancer , from a sample of 1590 patients with covid - 19 , and found a higher risk of covid - 19 and poorer outcomes in patients with cancer than in those without . 
large studies are needed to comprehensively describe the characteristics and outcomes of patients with cancer and covid - 19 . we collected and analysed data from patients with cancer and covid - 19 who were admitted to nine local hospitals in hubei , china . 
recent studies have shown that receiving antitumour treatments and patchy consolidation on ct scans were associated with development of severe events in covid - 19 ( requiring admission to the intensive care unit , the use of mechanical ventilation , or death )  . 
 however , we found no published multicentre study with a large sample size discussing clinical characteristics , outcomes , and risk factors of mortality of patients with cancer and a confirmed diagnosis of covid - 19 . diagnosed with covid - 19 , and to identify risk factors associated with in - hospital mortality . methods study design and participants this retrospective , multicentre , cohort study was led by wuhan union hospital ( wuhan , china )  . 
the list of participating hospitals is as follows : cancer center of wuhan union hospital , west branch of wuhan union hospital , jin yin - tan hospital , wuhan red cross hospital , the central hospital of wuhan , huanggang central hospital , the first peoples hospital affiliated to yangtze university , xianning central hospital , and suizhou central hospital ( appendix p 1 )  . 
diagnosis of covid - 19 followed who interim guidance.12 from jan 13 to march 18 , 2020 , we enrolled 205 patients with a history of cancer , irrespective of when the cancer had been diagnosed . 
 the inclusion criteria were strictly based on pathological diagnosis of a malignant tumour and laboratory confirmation of sars - cov - 2 infection ; patients clinically diagnosed with covid - 19 were excluded . 
 the presence of sars - cov - 2 infection was confirmed by rt - pcr and next - generation sequencing analysis of samples collected from nasopharyngeal swabs.4 , 13 we aimed to explore the clinical characteristics and outcomes of patients with covid - 19 who had malignant tumours . 
there was no formal determination added value of this study in this retrospective , multicentre , cohort study , we report demographic , clinical , laboratory , and radiological findings , as well as treatments and outcomes , for 205 patients with cancer and laboratory - confirmed severe acute respiratory distress syndrome coronavirus 2 ( sars - cov - 2 ) infection in hubei , china . 
 receiving chemotherapy within 4 weeks before symptom onset , and male sex were risk factors for death during admission to hospital . implications of all the available evidence patients with cancer are a vulnerable population with a higher case - fatality from covid - 19 than the general population . 
 male patients with cancer and those receiving chemotherapy within 4 weeks before symptom onset might require additional medical attention and supportive care once diagnosed with covid - 19 , as they appear to be at increased risk of in - hospital mortality . 8161 patients diagnosed with covid - 19 in electronic medical record system from nine hospitals in hubei , china , between jan 13 and march 18 , 2020 248 patients with a history of a tumour identied from the electronic medical record system 21 patients excluded 12 with benign tumours 9 without pathological conrmation 22 patients without laboratory conrmation of sars - cov - 2 infection excluded 205 patients included in the study figure : study profile sars - cov - 2 = severe acute respiratory syndrome coronavirus 2 . of sample size and all patients meeting the inclusion criteria were recruited . 
the cutoff date for our study was april 20 , 2020 . ethics approval was obtained from the ethics committee of wuhan union hospital , tongji medical college , huazhong university of science and technology , wuhan , china , at the beginning of the study . 
data on spo were missing for 17 patients . table 1 : demographics and baseline characteristics of patients with cancer and covid - 19 data collection we obtained information about demographic data , clinical manifestations , cancer histories , laboratory findings , chest ct examinations , treatments , and outcomes of all enrolled patients from electronic medical records and patients interviews . 
based on the tnm staging system , cancer stage was defined as early ( iii ) or late ( iiiiv ) stage for solid tumours ( staging information for brain cancer was not recorded )  . 
we also recorded information about treatments ( administration of anti biotics and for covid - 19 antivirals , oxygen therapy , and mechanical ventilation ) , compli cations , and outcomes during admission to hospital . definitions acute respiratory distress syndrome was defined according to the berlin definition.15 acute heart failure , acute kidney injury , septic shock , and secondary infection were defined according to previous studies.13 leucocytosis was defined as a white blood cell count of more than 10 cells per l . 
 * stroke , acute heart failure , myocardial ischaemia , electrolyte disturbance , and other complications . table 3 : treatments and complications of patients with cancer and covid - 19 00012 045 00014 069 094 034 0014 < 00001 < 00001 00011 < 00001 < 00001 00039 00004 < 00001 < 00001 < 00001 00001 < 00001 < 00001 00034 statistical analysis we hypothesised that differences exist in demographic , clinical , and laboratory characteristics , treatments , and cancer history between survivors and non - survivors of covid - 19 with cancer . 
quantitative variables were presented as medians ( iqr ) , and qualitative vari ables were presented by frequencies and percentages ( only available data were calculated )  . the mann - whitney u test , fishers exact test , test , and yates continuity correction were applied to analyse the differences between groups according to the type of data . 
we chose receiving chemotherapy within 4 weeks before symptom onset as the cutoff according to the number of patients within groupings and the significance of the logistic regression analysis ( appendix p 1 )  . 
for the multivariable logistic regression analysis , we chose four variables to avoid overfitting of the regression model because of the small number of endpoint events ( n = 40 ) in our research . 
variable selection was based on significance from the univariable logistic regression analysis ( p < 005 ) , the correlation between indicators , basic baseline clinical characteristics , and the accuracy and availability of data . 
other laboratory tests , including creatinine , lactate dehydrogenase , creatine kinase , d - dimer , interleukin - 6 , and c - reactive protein can be unavailable in emergency situations . 
the time period of hospital admission was not included because some patients might have been admitted to other hospitals and been given treatment ( eg , antibiotics , antiviral medication , oxygen therapy ) before they were transferred to the current hospital . 
therefore , receiving chemotherapy within 4 weeks before symptom onset , cancer type ( solid vs haematological ) , time since cancer diagnosis , and sex were chosen in our multi variable logistic regression model . 
the differences between groups were considered to be significant when the p value was less than 005 . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results from jan 13 to march 18 , 2020 , 227 patients with cancer were screened from 8161 patients with covid - 19 admitted to nine hospitals in hubei province . 
184 ( 90% ) of 205 patients were identified from among the 6485 patients admitted to five hospitals designated for patients with covid - 19 in the city of wuhan . 
among 8161 patients with covid - 19 , 205 ( 25% ) had cancer . of the 205 patients with cancer included ( table 1 ) , 40 ( 20% ) had died as of april 20 , 2020 , and 34 ( 18% ) of 184 patients in wuhan city had died . 
no significant differences in age and other comorbidities were observed between survivors and non - survivors . data for abnormal blood cell counts in the 203 patients for whom these data were available included 25 ( 12% ) cases of leucocytosis , 54 ( 27% ) of leucopenia , 32 ( 16% ) of neutro penia , 102 ( 50% ) of lymphocytopenia , and 25 ( 12% ) of thrombocytopenia ( table 2 )  . 
129 ( 70% ) of 185 patients had elevated concentrations of d - dimer , 115 ( 60% ) of 192 patients had elevated concentrations of c - reactive protein , and 78 ( 49% ) of 160 patients had increased lactate dehydro genase . 
compared with survivors ( table 2 ) , non - survivors had higher nlr and higher concentrations of creatinine , blood urea nitrogen , lactate dehydrogenase , creatine kinase , d - dimer , c - reactive protein , procalcitonin , and interleukin - 6 , and lower lymphocyte and platelet counts , and albumin and calcium concentrations . of the 205 patients included , 144 ( 70% ) received intravenous antibiotics and 192 ( 94% ) received antiviral medications ( table 3 )  . 
compared with survivors ( table 3 ) , non - survivors were more likely to receive intravenous medication ( antibiotics , immunoglobulin , or corticosteroids ) , receive oxygen therapy , require mechanical ventilation , be transferred to the icu , and develop complications such as acute respiratory distress syndrome , secondary infection , acute renal failure , and septic shock ( table 3 )  . 38 ( 20% ) of 192 patients had been diagnosed with cancer within the past year , and 20 ( 12% ) of 162 patients had an ecog score higher than 1 before admission . 
54 ( 30% ) of 182 patients received antitumour therapy within 4 weeks before symptom onset , and 15 ( 8% ) of 182 received more than one treatment , including seven ( 4% ) of 182 who received both chemotherapy and targeted therapy . 
 910 vol 21 july 2020 articles the case - fatality rate in patients with haematological malignancies was 41% ( nine of 22 patients ) and that in solid tumours was 17% ( 31 of 183 patients ; hr 328 [ 95% ci 156691 ] ; log rank p = 00009 ; appendix p 3 )  . 
for example , two of three patients with multiple myeloma died ; case - fatality rates were lower for patients with breast cancer , thyroid cancer , and cervical cancer . we did a comparative analysis of clinical characteristics , treatments , laboratory data , and radiological data from patients with solid tumours and those with haematological malignancies ( appendix pp 46 )  . 
patients with haematological malignancies were younger than those with solid tumours ( median age 55 years [ iqr 2662 ] vs 64 years [ 5770 ] ) , and most ( 15 [ 68% ] of 22 ) were male . 
 [ 27% ] of acute respiratory distress syndrome ( six 22 patients vs 17 [ 10% ] of 177 patients ) and coagulopathy ( five [ 23% ] of 22 patients vs 13 [ 7% ] of 177 patients ) were more frequently seen in patients with haematological malig nancies than in those with solid tumours . 
14 ( 70% ) of 20 patients with haematological malignancies received antitumour treatments in the past 4 weeks before symptom onset , compared with 40 ( 25% ) of 162 patients with solid tumours . 
11 ( 55% ) of 20 patients with haematological malignancies and 20 ( 12% ) of 162 patients with solid tumours received chemotherapy within 4 weeks before symptom onset . in univariable logistic regression analysis , cancer type , time since cancer diagnosis , cancer stage , male sex , leuco cytosis , lymphopenia , high nlr , thrombocytopenia , lactate dehydrogenase , d - dimer , creatine kinase , c - reactive protein , creatinine , receipt of chemotherapy or targeted therapy within 4 weeks before symptom onset , and hospital admission were associated with death ( table 5 )  . 
we included 180 patients with complete data in the multivariable regression analysis ( 146 survivors and 34 non - survivors ) , in which we included four variables : sex , cancer type , receipt of chemotherapy within the previous 4 weeks , and time since cancer diagnosis . 
receiving chemotherapy within 4 weeks before symptom onset ( or 351 [ 95% ci 1161059 ] ; p = 0026 ) and male sex ( 386 [ 157950 ] ; p = 00033 ) were associated with increased odds of death during admission to hospital ( table 5 )  . 
similar results were shown after adjusting for study centre or different cancer types ( appendix p 8 )  . discussion patients with cancer are a vulnerable population in the ongoing covid - 19 pandemic . 
 to our knowledge , this is the first multicentre , retrospective , cohort study to describe the clinical features , outcomes , and risk factors for mortality in patients with cancer and diagnosed with covid - 19 . 
severe pneumonia occurred in 52 ( 25% ) patients and the in - hospital univariable or ( 95% ci ) p value multivariable or ( 95% ci ) p value ( continued from previous page ) cancer type solid tumour ecog score haematological malignancy 339 ( 133863 ) 0010 207 ( 068635 ) 020 1 ( ref ) 1 ( ref ) 1 ( ref ) 129 ( 050329 ) 177 ( 043726 ) 398 ( 0811953 ) 060 043 0088 100 hospital admission before feb 13 , 2020 807 ( 2752370 ) 00001 1 ( ref ) or = odds ratio . 
hospital admission before feb 13 , 2020 , is used as a factor to represent the time period of the covid - 19 pandemic . table 5 : bivariate logistic regression analysis of factors associated with death during admission to hospital case - fatality rate in patients with covid - 19 and cancer was 20% , which is much higher than the case - fatality rate for covid - 19 in the overall chinese population ( 1% ) .13 in wuhan , the case - fatality rate of patients with cancer in our study was 18% ( 34 of 184 patients ) , which was higher than the overall case - fatality rate reported for patients with covid - 19 ( 8% ) .5 in particular , male sex and receiving chemotherapy within 4 weeks before symptom onset were identified as risk factors for death in patients with cancer who were diagnosed with covid - 19 . the proportion of patients with cancer among those with covid - 19 who were admitted to the nine hospitals in our study was 25% , which was higher than that reported in the overall chinese population ( 029% ) 18 and in a previous report of patients with covid - 19 ( 1% ) .10 this finding suggests that patients with cancer are more susceptible to covid - 19 than the general population . 
by contrast with four other human coronaviruses ( hcov - nl63 , hcov - 229e , hcov - oc43 , and hku1 ) , which induce only mild upper respiratory diseases , 19 sars - cov - 2 behaves like sars - cov and middle east respiratory syndrome coronavirus ( mers - cov ) to some extent , and leads to higher rates of severe respiratory syndrome.20 similar to our study , fever and cough were the most common clinical manifestations among patients with covid - 19.16 although older age and underlying diseases have been found to be risk factors for severe events in a previous study , 10 this was not observed in our study . 
we found bilateral lung lesions in 91% of patients with available records , which was higher than the figure reported previously by xu and colleagues ( bilateral lung lesions in 53 [ 59% ] of vol 21 july 2020 articles 90 patients with laboratory - confirmed sars - cov - 2 infection ) , 21 sug gesting that patients with cancer were more vulnerable once they became infected with sars - cov - 2 . men were found to be at a higher risk of mortality than women in this study . 
in addition to sex differences in smoking rate , 22 differences in the immune and endocrine systems between men and women23 , 24 might exert different responses against sars - cov - 2 infection . 
62 ( 57% ) of 109 women in our study had one of these three types of cancers . lymphocytopenia is one of the clinical features of covid - 19 , 4 indicating that the virus tends to diminish the antiviral immunity of the host . 
since we do not yet have highly effective drugs targeting sars - cov - 2 , a patients inherent immunity might be a determining factor for their prognosis after effective supportive care . 
it has been recommended that the mode of admin istration ( from infusion to oral administration ) and intervals of chemotherapy should be adjusted according to patients conditions.25 although molecular - targeted therapy rarely impairs patients immunity , those receiving maintenance molecular - targeted therapy all had advanced disease , and seven ( 58% ) of 12 received chemotherapy concurrently within 4 weeks before symptom onset , which might have accounted for the increased risk of death . 
immunosuppressive treatments administered more than 4 weeks before symptom onset might not worsen the outcome of covid - 19 , which can be partially explained by the recovery of patients from side - effects of cytotoxic treatments . 
because of the small number of patients in our study who received chest radiotherapy 4 weeks before onset of covid - 19 , we were not able to analyse the effect of recent chest radiotherapy on patient outcomes . many haematological malignancies change how blood cells in the immune system function . 
lower respiratory tract diseases caused by human coronaviruses in patients with haematological malignancies have been associated with high rates of oxygen use and mortality.26 in our study , patients with haematological malignancies had poorer prognoses than those with solid tumours . 
besides the inherent differences between haematological malignancies and solid tumours , more patients with haematological malignancies received chemotherapy within 4 weeks before symptom onset ( 11 [ 55% ] of 20 vs 20 [ 12% ] of 162 ) , which might partly explain our finding of worse outcomes in these patients . in addition to lymphocytes , neutrophils are the mainstay in fighting off various infections . 
nlr is considered to reflect host inflammation and is a predictor of bacterial infection.27 it has also been found to be associated with clinical outcome and treatment efficacy in several cancers.28 in patients with covid - 19 , high neutrophil counts have frequently been seen in refractory disease.29 in line with a previous study , 30 we found a high nlr to be associated with poor prognosis in patients with cancer and covid - 19 . 
sars - cov - 2 infection and subsequent bacterial infection might have caused a deterioration of lung function and contributed to death , although this hypothesis requires further investigation . our study had some limitations . 
 additionally , we did not compare the case - fatality rate , characteristics , outcomes , and treatment strategies of patients with cancer against a control group of patients without cancer . 
dynamic changes in the titre of the igm and igg antibodies , sars - cov - 2 nucleic acid , and other laboratory tests such as tumour - related cytokines besides interleukin - 6 ( eg , tumour necrosis factorand interferon - ) in the course of disease should be further recorded and analysed . 
finally , the impact of covid - 19 on cancer needs to be evaluated with long - term follow - up of survivors . in conclusion , patients with cancer and covid - 19 require urgent and special attention , since they are a vulnerable population with a much higher case - fatality rate than the general population . 
receiving chemotherapy 4 weeks before symptom onset and male sex are two indicators that might help clinicians to identify patients with cancer who are at high risk of fatal outcomes at an early stage . contributors gw and ky had the idea for and designed the study and provided financial support . 
gw , ky , bw , ch , yj , nx , kj , and hl critically revised the manuscript for important intellectual content . declaration of interests we declare no competing interests . acknowledgments this work was supported by the national natural science foundation of china ( nsfc 81874218 , nsfc 81672978 )  . 
based on the sample size calculation , we planned to analyse overall survival when 190 deaths occurred ; this target has now been reached , after a median 10 years of follow - up . methods rt01 was a phase 3 , open - label , international , randomised controlled trial enrolling men with histologically con rmed t1bt3a , n0 , m0 prostate cancer with prostate speci c antigen of less than 50 ng / ml . 
patients were randomly assigned centrally in a 1 : 1 ratio , using a computer - based minimisation algorithm stratifying by risk of seminal vesicle invasion and centre to either the control group ( 64 gy in 32 fractions , the standard dose at the time the trial was designed ) or the escalated - dose group ( 74 gy in 37 fractions )  . 
this trial is registered , number isrctn47772397 . findings between jan 7 , 1998 , and dec 20 , 2001 , 862 men were registered and 843 subsequently randomly assigned : 422 to the escalated - dose group and 421 to the control group . 
biochemical progression or progressive disease occurred in 391 patients ( 221 [ 57% ] in the control group and 170 [ 43% ] in the escalated - dose group )  . 
at 10 years , biochemical progression - free survival was 43% ( 95% ci 3848 ) in the control group and 55% ( 5061 ) in the escalated - dose group ( hr 069 , 95% ci 056084 ; p = 00003 )  . interpretation at a median follow - up of 10 years , escalated - dose conformal radiotherapy with neoadjuvant androgen deprivation therapy showed an advantage in biochemical progression - free survival , but this advantage did not translate into an improvement in overall survival . 
open access article distributed under the terms of cc by . introduction external beam radiotherapy is one of the standard curative options for men with localised prostate cancer and is particularly appropriate for men with intermediate - risk or high - risk disease.1 , 2 improved radiotherapy techniques , such as conformal radiotherapy , allow high treatment doses to be given safely3 , 4 and several phase 3 randomised controlled trials of dose escalation have reported improved biochemical progression - free survival.510 the medical research council ( mrc ) rt01 trial is the largest of these trials to have reported results , and since its initial report of results dose - escalated conformal radiotherapy has been the standard of care in the uk since 2008.1 the trial mandated the use of short - course neoadjuvant androgen deprivation therapy ( adt ) ; neoadjuvant adt has since been shown to improve overall and cancer - speci c survival in patients with advanced localised disease.1114 overall the aim of the rt01 trial was to assess the e ect of survival , biochemical dose - escalation progression - free survival , and toxicity , by comparing doses of 74 gy and 64 gy delivered by use of conformal radiotherapy techniques . 
64 gy in 32 fractions was chosen as the radiotherapy schedule for the control group in our randomised trial , because that was the standard 464 vol 15 april 2014 articles 862 assessed for eligibility 19 excluded 8 intercurrent illness 6 patients preference 3 hospital error 2 disease progression 843 randomised 4 received more than planned dose 421 patients assigned to control group ( 64 gy in 32 fractions ) 2 had less than planned dose 4 did not receive radiotherapy 1 dose information not available 410 received planned dose 422 patients assigned to escalated - dose group ( 74 gy in 37 fractions ) 14 received less than planned dose 7 did not receive radiotherapy 401 received planned dose 421 patients analysed 422 patients analysed figure 1 : trial pro le age ( years ) median ( range ) t stage t1b / t1c t2a / t2b t3a / t3b not known gleason score * 6 or lower 8 or higher not known median ( iqr ) mean ( sd ) moderate nccn risk group * high intermediate unobtainable control group ( n = 421 ) escalated - dose group ( n = 422 ) 67 ( 4680 ) 67 ( 4880 ) 106 ( 26% ) 236 ( 57% ) 71 ( 17% ) 103 ( 25% ) 239 ( 57% ) 76 ( 18% ) 261 ( 62% ) 105 ( 25% ) 52 ( 12% ) 249 ( 59% ) 117 ( 28% ) 54 ( 13% ) 128 ( 84200 ) 128 ( 78202 ) 156 ( 100 ) 152 ( 96 ) 137 ( 33% ) 284 ( 67% ) 138 ( 33% ) 284 ( 67% ) 79 ( 19% ) 159 ( 38% ) 178 ( 43% ) 81 ( 19% ) 152 ( 36% ) 184 ( 44% ) prehormone psa ( ng / ml ) risk group for involvement of seminal vesicles data are n ( % ) unless otherwise speci ed . 
 * if gleason score was missing , who di erentiation was used in the following way : well , moderate , or poor di erentiation is classi ed as gleason score of 6 , 7 , or 8 , respectively . 
we initially reported ndings of the trial with a 5 - year median followup and now update these results with a median follow - up of 10 years , because the target number of deaths for analysis of overall survival has been reached . 
treatmentrelated side - e ects have been reported previously.7 , 15 , 16 methods study design and participants rt01 was a phase 3 , open - label , international , randomised controlled trial comparing dose - escalated conformal radiotherapy with control - dose conformal radiotherapy . 
it was preceded by a pilot study at the royal marsden hospital.5 patients were registered , initiated on neoadjuvant adt , and then randomly assigned to receive either control or escalated radiotherapy using conformal radiotherapy techniques . 
men 18 years or older with histologically con rmed t1bt3a , n0 , m0 prostate cancer and prostate - speci c antigen ( psa ) of less than 50 ng per ml , with no contraindications for radical radiotherapy were included in the trial . 
this study was done in compliance with the declaration of helsinki , and the protocol was approved by the appropriate research ethics committees . randomisation and masking consenting patients were randomly assigned in a 1 : 1 ratio to control or escalated - dose conformal radiotherapy centrally at the mrc clinical trials unit ( ctu ) using a computer - based minimisation algorithm , stratifying for risk of seminal vesicle invasion and centre . 
the random allocation list was created by the mrc ctu . injections of procedures as reported previously , androgen deprivation was achieved using luteinising - hormonereleasing hormone agonists every 4 weeks and was accompanied by antiandrogen therapy to prevent are events.7 neoadjuvant adt was given for 36 months before commencement of conformal radiotherapy and continued until the end of conformal radiotherapy . men were randomised to receive either a control - dose schedule ( 64 gy in 32 fractions ; control group ) schedule , or an escalated - dose schedule ( 74 gy in 37 fractions )  . 
all radiotherapy treatments used three - dimensional conformal techniques as previously described.7 , 11 , 17 the radiotherapy phase 1 target volume included the prostate and all or part of the seminal vesicles , depending on the vol 15 april 2014 articles risk of seminal vesicle invasion.18 all patients were treated to a dose of 64 gy in 32 fractions over 65 weeks using a standard threeeld plan ( anterior eld and left and right lateral or posterior oblique elds ) with a 10 cm marg patients randomised to the escalated - dose group had a phase 2 boost to the prostate alone using a sixeld technique ( left and right anterior oblique , left and right posterior oblique , and left and right lateral elds ) with no margin added . 
veri cation was with daily and then weekly port lms and images . men were followed - up throughout radiotherapy at 6 monthly intervals up to 2 years , and annually thereafter . 
 acute and late treatment - related side - e ects were collected using radiation therapy oncology group19 and late e ects of normal tissues - subjective objective management analytic scales20 and timed from the start of radiotherapy . 
the design , objectives , eligibility criteria for patients , treatment methods , and statistical considerations are detailed elsewhere.7 , 17 outcomes the coprimary outcome measures were overall survival and biochemical progression - free survival . 
overall 020 015 010 005 005 010 015 020 020 015 010 005 005 010 015 020 control group by kaplan - meier control group by exible parametric model escalated - dose group by kaplan - meier escalated - dose group by exible parametric model number at risk control group escalated - dose group 95% ci overall survival by exible parametric model control group by kaplan - meier control group by exible parametric model escalated - dose group by kaplan - meier escalated - dose group by exible parametric model time from randomisation ( years ) number at risk control group escalated - dose group 95% ci biochemical progression - free survival by exible parametric model time from randomisation ( years ) figure 2 : primary analysis of overall survival and biochemical progression - free survival ( a ) overall survival , predicted from kaplan - meier function and exible parametric model . 
 ( d ) absolute di erence in biochemical progression - free survival , from exible parametric model . 466 vol 15 april 2014 articles hr ( 95% ci ) 096 ( 054170 ) 101 ( 076134 ) 077 ( 032187 ) 113 ( 073174 ) 095 ( 068134 ) 080 ( 054118 ) 066 ( 052083 ) 061 ( 034109 ) 084 ( 059119 ) 060 ( 046079 ) with cox models , adjusted for seminal vesicle risk group.18 we applied the restricted mean survival time method to overall survival and biochemical progressionfree survival , as an additional method of estimating di erence between the treatments , with the restriction time being 10 years . 
 all comparisons are expressed relative to the control group ; therefore , an hr of less than 10 indicates a decreased risk in the escalated - dose group . we did a competing - risk analysis for prostate cancer death because the number of deaths from causes other than prostate cancer exceeded the prespeci ed level of 20% . 
for this analysis , time to prostate cancer death is presented with cumulative incidence function rather than survival function ; sub - hr is presented with 95% ci and p value . 
cause - speci c hrs are presented for both prostate cancer and non - prostate - cancer deaths . we did pre - planned , exploratory subgroup analyses to examine consistency of e ect across seminal vesicle risk group ( low vs moderate ) and national comprehensive cancer network ( nccn ) risk group ( low vs intermediate vs high ) .2 this analysis uses tests for heterogeneity of interaction or trend when appropriate , and examines overall survival and biochemical progression - free survival . 
this trial is registered , number isrctn47772397 . low risk intermediate risk test for heterogeneity : p = 089 low risk intermediate risk high risk test for heterogeneity : p = 070 low - risk intermediate - risk test for heterogeneity : p = 042 low risk intermediate risk high risk test for heterogeneity : p = 032 survival was de ned as time from randomisation to death from any cause or censoring at date of last contact . 
 biochemical progression - free survival was de ned as time from randomisation to biochemical failure , death from prostate cancer , or development of local , nodal , or metastatic disease , whichever occurred rst . additional outcome measures were biochemical failure ( an increase in psa concentration to 50% above nadir and above 2 ng / ml 6 months or more after the start of radiotherapy ) ; progression - free survival ( excluding psa failure ) ; initiation of long - term salvage adt ; development of metastases ; death from prostate cancer ; and metastasesfree survival ( time to development of any metastases or death from prostate cancer )  . 
cause of death was reviewed by pairs of clinicians from a panel of ve individuals who were masked to treatment allocation . the original protocol speci ed ve primary outcome measures survival ( biochemical progression - free [ named as biochemical control in the protocol , local progression , metastases free freedom from survival , overall survival , and late toxicity ) ; with sample size calculations included for local control and overall survival . 
during the course of the trial , the trial management group , independent data monitoring committee , and trial steering committee agreed from external evidence that biochemical progression - free survival was a more important outcome measure than local control . 
all outcome measures are reported . statistical analysis we estimated that inclusion of about 800 patients would meet the targets for the numbers of patients in the subgroups at low - risk and intermediate - risk of seminal vesicle involvement.17 we assumed that survival at 5 years would be 50% in patients in the control group , and the trial aimed to achieve a 15% increase in survival at 5 years in the escalated - dose group . 
with 90% power and a 5% two - sided signi cance level , we established that about 194 deaths were needed for this analysis of overall survival . we did all analyses on an intention - to - treat basis , with patients analysed according to allocated treatment group . 
 all analysed outcome measures are presented in this report . we used standard survival analysis methods to investigate time from randomisation to the rst reported event for each outcome measure , except for time to death from prostate cancer . 
hazard ratios ( hr ) were estimated favours escalated - dose favours control figure 3 : subgroup analyses of overall survival and biochemical progression - free survival ( a ) overall survival and risk of seminal vesicle involvement . 
 results between jan 7 , 1998 , and dec 20 , 2001 , 862 men were registered and 843 subsequently randomised : 422 to the escalated - dose group and 421 to the control group ( gure 1 )  . table 1 shows characteristics of the patients at baseline ; the groups were balanced . 
209 ( 25% ) of 831 patients had t1 stage cancers , 475 ( 57% ) had t2 stage , and 147 ( 18% ) had t3 cancers ; t stage was unavailable for 12 patients . 
 analyses of biopsy specimens were reported by local histopathologists , and showed gleason scores of 6 or lower in 510 ( 61% ) of the 838 enrolled patients , a score of 7 in 222 ( 26% ) of patients , and a score 8 of or higher in 13% ( 106 ) of patients ; gleason score was not available for ve patients . 
160 ( 19% ) of 833 patients had low - risk disease according to nccn criteria , 311 ( 37% ) had intermediate - risk disease , and 362 ( 43% ) had high - risk disease ; unavailability of t - stage or histological grading precluded ascertainment of risk group in ten patients . 
overall , 117 patients were alive at 11 years and 30 at 12 years . as of aug 2 , 2011 , 236 deaths had been reported , 118 in each group , triggering the overall survival analysis . 
there was no di erence in 10 year overall survival between groups : 10 year overall survival was 71% ( 95% ci 6675 ) in both groups ( hr 099 , 95% ci 077128 , p = 096 , gure 2 )  . 
mean overall survival , using the exible parametric model and when restricted to 10 years , was 930 years ( 95% ci 908952 ) for the control group and 928 years ( 906950 ) for the escalated - dose group . 
there was no evidence of a di erence between restricted mean survival : 002 years ( 95% ci 034 to 029 ; p = 088 )  . for patients who had not yet reported a biochemical progression event , adherence to psa testing was 90% complete at 5 years and 76% complete at 10 years . 
 biochemical progression - free survival was better in the escalated - dose group , being 43% at 10 years ( 95% ci 3848 ) in the control group and 55% ( 5061 ) in the escalated - dose group ( hr 069 , 95% ci 056084 ; p = 00003 , gure 2 )  . 
mean biochemical progressionfree survival , when time of analysis was restricted to 10 years , was 733 years ( 95% ci 687780 ) in the control group and 801 years ( 760840 ) in the escalated - dose group , leading to an improvement in restricted mean survival of 069 years with escalateddose radiotherapy ( 95% ci 008130 ; p = 003 )  . 
||cause - speci c hr . table 2 : outcome measures 468 vol 15 april 2014 articles 020 015 010 005 control group escalated - dose group number at risk control group escalated - dose group control groups , pc death control groups , non - pc death escalated - dose groups , pc death escalated - dose groups , non - pc death number at risk control group escalated - dose group time from randomisation ( years ) time from randomisation ( years ) figure 4 : additional outcome measures ( a ) progression - free survival , kaplan - meier plot . 
progression - free survival , biochemical failure , and delayed commencement of salvage adt were all signi cantly better the escalated - dose group compared to the control group ( table 2 , gure 4 )  . 
of patients who had biochemical progression , a lower proportion ( 67 [ 30% ] of 221 patients ) in the control group had metastases , or died from prostate cancer compared to the escalated - dose group ( 65 [ 38% ] of 170 patients )  . 
notably , of the 391 patients who developed psa failure or progressive disease , only 220 ( 56% ) reported commencing long - term salvage adt ( 123 in the control group , 97 in the escalated - dose group )  . 
of 268 men who had clinical evidence of progressive disease , 132 ( 49% ) developed metastases or died from prostate cancer ( 67 in the control group , 65 in the escalated - dose group )  . according to the central , blinded review of deaths , 91 of 236 ( 39% ) deaths were from prostate cancer ( 44 in the control group , 47 in the escalated - dose group ) , 132 ( 56% ) were from other causes ( 68 in the control group vs 64 in the escalated - dose group ) , and for 13 ( 6% ) patients there were insu cient data for the reviewers to assign cause of death ( six control vs seven escalated dose ) : for ten , the investigator de ned causality as not prostate cancer ( which was accepted ) , and for the other three , no evidence of recurrent prostate cancer had been recorded . 
 we did a competing - risk analysis for prostate cancer death because 145 ( 61% ) of 236 deaths were from causes other the than prostate cancer , which exceeded prespeci ed level of 20% . 
the sub - hr for the comparison of cumulative incidences is 107 ( 95% ci 071161 ; p = 075 ) in favour of the control group with a cause - speci c hr for prostate cancer deaths of 106 ( 95% ci 070160 ; p = 079 ) and for other deaths of 096 ( 069132 ; p = 078 )  . nccn risk group was available for 90 of the 91 patients who died from prostate cancer . 
only one of 160 ( 1% ) men with low - risk disease died from prostate cancer compared with 21 of 311 ( 7% ) with intermediate - risk disease and 68 of 362 ( 19% ) with high - risk disease . 
as a proportion of total deaths , for lowrisk disease , one ( control group ) of 20 ( 5% ) were from prostate cancer compared with 21 ( nine control vs 12 escalated - dose ) of 81 ( 26% ) for intermediate - risk disease and 68 ( 34 control vs 34 escalated - dose ) of 133 ( 51% ) for high - risk disease . 
we identi ed no evidence of heterogeneity of e ect of dose escalation between these subgroups . discussion the previously reported advantage of escalated - dose conformal radiotherapy treatment compared to controldose conformal radiotherapy in biochemical progressionfree survival after a median follow - up of about 5 years was maintained in the present study with more mature data and a median follow - up of 10 years . 
this improvement in biochemical control of disease has not translated into an advantage for metastases - free survival , prostate - cancer - speci c survival , or overall survival . 
we identi ed no evidence of heterogeneity of treatment e ect between low , intermediate , and highrisk groups . we recorded a signi cant delay in the reported time to initiation of long - term , salvage adt in the escalated - dose group ; using the hr there was an absolute improvement of 7% ( 95% ci 012 ) at 10 years from 45% . 
this advantage of reducing or delaying the initiation of long - term adt , which is associated with well - documented andropausal side - e ects , 22 must be balanced against the known small increase in bowel side - e ects from the ve extra treatments in the escalated - dose group , which we and others have reported.5 , 6 , 8 , 10 , 16 , 23 why has the di erence in psa control not translated into an advantage for metastasis - free survival and prostate - cancer - speci c survival ? several factors might be involved . 
first , it is likely that there were more indolent recurrences con ned to the prostate in the control group : a lower proportion of patients in the control group had metastases or died from prostate cancer than those in the escalated - dose group . 
moreover , of patients who developed psa failure or progressive disease , only 56% reported commencing long - term salvage adt , and only 49% of patients who had clinical evidence of progressive disease developed metastases or died from prostate cancer . 
we now know that some men with indolent local disease do not necessarily need treatment , for example men with low - risk disease or older than 65 years do not bene t from radical prostatectomy , 24 , 25 and active surveillance has become a standard of care for patients with a favourable outlook.26 second , there is a long time from commencement of salvage adt to death . 
in an international trial of intermittent or continuous salvage androgen suppression , 22 time from salvage adt to death was estimated at about 9 years , but with only about 17% of patients dying of prostate cancer after 7 years . 
in the control group of rt01 , 25% of patients had a biochemical progression - free survival event by 26 years after randomisation , but it was 57 years from randomisation before 25% of patients had reported initiation of salvage adt ; median times for these outcome measures have not been reached . 
moreover , our results clearly show that nccn risk group was related to the probability of dying from prostate cancer . the lower bound of the 95% ci for overall survival was 077 , and therefore our results cannot rule out some improvement in overall survival . 
 after 14 years of follow - up , the small pilot study ( n = 126 ) which recruited before the start of rt01 suggested an overall survival advantage for the escalated - dose group ( 74 gy ) with hr 059 , but with only 19 prostate cancer deaths the 95% cis were wide ( 023149 ) .5 the phoenix de nition27 our trial was designed in 1997 and launched in 1998 before for biochemical recurrence became established , but our chosen de nition of psa failure with 2 ng / ml has much the same speci city and sensitivity.28 our results are in alignment with reported data from other studies of dose - escalated external beam radiotherapy ( table 3 ) , which have shown absolute advantages in psa failure - free survival of 619% for dose - escalated treatments . even in trials with a high proportion of patients with poor prognostic factors and long follow - up , none have yet reported prostate - cancer - speci c mortality of greater than 15% . 
a meta - analysis with the other randomised trials would provide a larger number of events from patients with high - risk disease to assess the e ect of dose - escalation on death from prostate cancer . our ndings draw attention to two issues for future trials . 
 survival - based outcome measures must remain of paramount importance , but there are implications for recruiting centres , trials units , and funding bodies in collecting long - term data . 
 * freedom from biochemical ( psa ) or clinical failure . table 3 : data from randomised controlled trials of dose - escalated external beam radiotherapy for prostate cancer absolute reduction in psa failure in dose escalated group ( 10 year ) ( 10 year ) ( 10 year ) 19% * ( 8 year ) ( 12 year ) 85% ( 5 year ) ( 10 year ) ( 10 year ) ( ns ) ( 8 year ) about ( 14 year ) ( ns ) outcome data needs to be explored . 
we have previously reported our comparative side - e ect data , which we planned to collect only to 5 years , 7 , 15 , 16 and a limitation of the present report is that no 10 - year patient - reported outcome data are available . by contrast with the dose - escalation trials , phase 3 studies assessing the addition of neoadjuvant adt to radical prostate radiotherapy have shown clear evidence of improved overall survival and cause - speci c survival in meta - analysis.29 , 30 review of additional trial results1114 shows that survival bene ts become apparent about 35 years after randomisation . 
one interpretation is that , in addition to short - course adt having an e ect on local control of disease , 11 6 months of adt also has a direct e ect on eradication of micrometastatic disease . 
 these trials have been in patients given modest doses of radiotherapy by present standards ( equivalent to 70 gy or lower ) but large institutional us series have suggested much the same bene ts of neoadjuvant adt in patients given doses of 7681 gy.31 , 32 either what are the relative merits of dose escalation and combined modality treatment with neoadjuvant adt ? dose escalation leads to excellent local disease control using brachytherapy33 in lower risk disease . 
by use of a biopsy sample obtained 2 years after treatment as a gold radiotherapy external beam panel : research in context systematic review radiotherapy dose is limited by treatment - related side - e ects . 
advancing radiotherapy techniques using conformal radiotherapy had been shown to reduce the occurrence of side - e ects.3 dose - escalation therefore became feasible with the hypothesis that higher radiation doses would lead to improved outcomes.5 , 3739 interpretation as far as we are aware , this study is the largest dose - escalation trial to have reported long - term e cacy results . 
 however , none of these trials have convincingly shown a positive e ect on overall or prostate - cancer - speci c survival after 10 years of follow - up . 
dose escalation improves intermediate disease outcomes and reduces the use of salvage hormonal treatment , but at the cost of a modest increase in treatment - related side - e ects . 
further improvements in radiotherapy techniques have been shown to reduce the e ect of dose - escalation on side - e ects4 , 40 , 41 and should be used to maintain the reported advantages of dose - escalation while minimising treatment sequelae . 
 standard method34 to detect local recurrence , a 3 - month period of neoadjuvant adt given with modest - dose or high - dose radiotherapy reduced positive biopsy ndings from 46% to 10%.35 in a preplanned substudy of the rt01 trial , only six ( 6% ) of 97 men in the escalated - dose group who agreed to have a biopsy 2 years after treatment had positive histology ( unpublished )  . 
the use of neoadjuvant adt , however , must be balanced against the usually short - lasting increase in morbidity from vol 15 april 2014 articles short - term adt.36 clinical trials that are in progress , including eortc study 22991 ( nct00021450 ) , will more completely de ne the role of combined modality treatment and high - dose radiotherapy . and since we designed our trial using conformal radiotherapy methods , technology advances have led to the widespread introduction of intensity - modulated , image - directed , techniques image - guided including the combined use of external beam radiotherapy with high - dose or low - dose rate brachytherapy , which have enabled high - dose treat ment to be given with a reduced prevalence of side - e ects using conventional or hypofractionated schedules ( panel ) .4 , 40 , 41 high - quality treatments are essential to maintain the potential advantages of dose - escalated treatment in improving disease control and avoiding salvage therapy , while maintaining low levels of treatmentrelated side - e ects . in conclusion , we have shown a clear and maintained advantage in biochemical ( psa ) assessment of disease control , which has translated into a modest reduction in salvage adt , but no evidence of a bene t in survivalbased outcome measures with a median follow - up of 10 years . 
all authors were involved in data interpretation , manuscript review , and approval of the nal manuscript . declaration of interests mrs , mkbp , gj , cm are employees of the sponsor at the medical research council , clinical trials unit at ucl , london , uk . 
randomized trial comparing conventional - dose with high - dose conformal radiation therapy in early - stage adenocarcinoma of the prostate : long - term results from proton radiation oncology group / american college of radiology 95 - 09 . 
the early toxicity of escalated versus standard dose conformal radiotherapy with neo - adjuvant androgen suppression for patients with localised prostate cancer : results from the mrc rt01 trial ( isrctn47772397 )  . 
implementing the uk medical research council ( mrc ) rt01 trial ( isrctn 47772397 ) : methods and practicalities of a randomised controlled trial of conformal radiotherapy in men with localised prostate cancer . 
j natl cancer inst monogr 2012 ; 45 : 23441 . 472 vol 15 april 2014 articles 27 roach m 3rd , hanks g , thames h jr , et al . 
is androgen deprivation therapy necessary in all intermediate - risk prostate cancer patients treated in the dose escalation era ? int j radiat oncol biol phys 2013 ; 85 : 69399 . 33 morris wj , keyes m , spadinger i , et al . 
int j radiat oncol biol phys 1998 ; 41 : 491500 . 36 stephens rj , dearnaley dp , cowan r , sydes m , naylor s , fallow eld l . 
 cancer treat rev 2014 ; 40 : 41425 . vol 15 april 2014 corrections correction to lancet oncol 2012 ; 13 : 559 correction to lancet oncol 2012 ; 13 : 696 lancet oncology . 
 lancet oncol 2012 ; 13 : 559 the second sentence of the third paragraph of this editorial should read in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
pixantrone dimaleate versus other chemotherapeutic agents as a singleagent salvage treatment in patients with relapsed or refractory aggressive non - hodgkin lymphoma : a phase 3 , multicentre , open - label , randomised trial . 
this correction has been made to the online version as of june 29 , 2012 , and the printed article is correct . vol 13 july 2012 e285 re ection and reaction ms has received consultancy fees from glaxosmithkline , and payment for lectures from physicians educational resources . 
production of hyperpolarized [ 1 , 4 - 13c2 ] malate from [ 1 , 4 - 13c2 ] fumarate is a marker of cell necrosis and treatment response in tumors . 
isocitrate dehydrogenase - 1 mutations : a fundamentally new understanding of di use glioma ? lancet oncol 2010 ; published online july 7 , doi : 10.1016 / s1470 - 2045 ( 10 ) 70053 - xin table 1 , data cited for acute myelogenous leukaemia should read 1% not 0% of idh1 mutations . 
these corrections have been made to the online version as of october 4 , 2010 . isocitrate wild - type idh1 nadp + nadph + co2 + h + - ketoglutarate mutant - idh1 nadph + h + nadp + 2 - hydroxyglutarate wild - type 922 vol 11 october 2010 correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections reportage managing patients with cancer during the covid - 19 pandemic : frontline experience from wuhan december , 2019 , witnessed a massive outbreak of coronavirus disease 2019 ( covid - 19 ) triggered by the severe acute respiratory syndrome coronavirus 2 ( sarscov - 2 ) in wuhan , hubei , china , which has now turned into a global public health crisis . 
fighting the pandemic of covid - 19 has become the main challenge for all clinicians . the wuhan union hospital is in the eye of the storm , treating patients within three designated medical settings , including a cancer centre . 
between january and march , 2020 , we have treated more than 5200 hospitalised patients with covid - 19 and cared for more than 20 000 with fever at our outpatient clinics . 
moreover , we have attended to more than 80 000 patients on our internet platform and operated two makeshift hospitals ( so - called fangcang hospitals ) , making wuhan union hospital the hospital that admitted and treated the highest number of patients with covid - 19 in wuhan . 
unlike many other patients , the immunity of patients with cancer is often compromised and they heavily depend on the availability of medical resources , which renders them extremely vulnerable to the impact of the epidemic and overwhelmed medical resources mean their lives are on the line . 
therefore , we were faced with the great challenge of how to protect our patients with cancer from infection while continuing routine patient care . zhong nanshan ( guangzhou medical university , guangzhou , guangdong ) , head of the national health commissions team investigating the novel corona virus outbreak , pointed out that sars - cov - 2 carried the risk of human - to - human transmission on jan 20 , 2020 . 
since institute of hematology ( h mei , y wang , l tang , y hu ) , and cancer center ( x dong ) , union hospital , tongji medical college , huazhong university of science and technology , wuhan , hubei 430022 , china dr_huyu@126.com we declare no competing interests yh is funded by a key special project of the ministry of science and technology of china ( 2020yfc0845700 ) for more on on the risk of human - to - human transmission see xinhuanet.com / english / 202001 / 20 / c_138721762.htm then , our cancer centre began to screen patients and healthcare workers infected with sars - cov - 2 in the hospital by means of nucleic acid and antibody tests in combination with ct scans . 
24 patients with cancer ( infection rate of 2% ) and 13 of 766 health - care workers ( infection rate of 17% ) were found to have been infected with sars - cov - 2 . 
the first 15 days after wuhan lockdown , starting from jan 23 , was the toughest time we experienced , during which seven patients with blood cancer and two patients with solid tumours died of covid - 19 . 
after our cancer centre was mandatorily designated a hospital on feb 15 , and thus only admitted patients with covid - 19 , a large amount of medical supplies began to arrive and reinforcement medical teams from all parts of china joined us . 
looking back , we gained a lot of experience and learned some lessons . for the management of hospitalised patients with cancer , the top priority is the control of nosocomial infection . 
at the early stage of the outbreak , because of a lack of awareness on personal protection , limited knowledge about the new virus , and an inadequate supply of nucleic acid tests , the number of infected patients increased substantially and some medical staff were infected . 
during the middle of january , some hospitalised patients began to develop fever and diarrhoea , but were not definitively diagnosed with covid - 19 because of a shortage of tests . 
therefore , we escalated the preventive measures , including early stage testing of patients , caregivers , and medical staff ( using nucleic acid tests , antibody tests , and ct scans ) ; isolation of confirmed patients in a single room without visits ; wearing of surgical masks by patients and caregivers ; mandatory hand sanitisation ; and separate disposal of patient waste . 
 634 vol 21 may 2020 perspectives hospital workers are at high risk of developing covid - 19 from nosocomial infection during an outbreak , as in the epidemics of sars and middle east respiratory syndrome . 
 during a pandemic of an infectious disease , medical workers should be well informed about its status to achieve their own early detection , prompt isolation , and expeditious treatment . 
to ensure the normal operation of oncology departments , the hospital authorities redeployed and temporarily relocated 50 doctors and nurses from other not - in - service departments to oncology departments . 
it is worth mentioning that medical workers in the reinforcement medical teams consisted of specialists in serious infections and management of respiratory tract diseases , and they had important roles in the management of severe and critical patients in the cancer center of wuhan union hospital . to treat the growing number of patients with suspected covid - 19 infection , confirmed cases were admitted as early as possible and non - confirmed cases were redirected to other hospitals . 
we set up a free - of - charge online fever clinic on feb 1 , and received 12 000 visits per day at the peak , including visits by many patients with cancer . 
stable patients ( ie , those without progression or deterioration in tumour burden or severe complications after treatment ) generally should not be hospitalised ; patients scheduled for elective operations should , whenever possible , be admitted after the pandemic . 
apart from these measures , when not enough beds are available , patients with suspected or mild - symptom disease can be referred to fangcang hospitals , but should be under close watch . 
for instance , nine patients admitted after feb 15 were transferred to our hospital from fangcang hospitals and received excellent treatment . patients with cancer are a special group of patients because treatment of their primary disease cannot be discontinued however , to decrease the risk of infection with sars - cov - 2 , postoperative chemotherapy could be postponed . 
with patients on radiotherapy , concurrent chemotherapy could be withheld for some time , including preradiotherapy preparation ( such as pretreatment imaging for tumour localisation and treatment planning )  . 
 with patients who are at home or visiting online clinics , chemotherapy - free alternatives involving oral or targeted drugswhich do not require in - hospital administration should be given whenever possible . 
although his blood virus tests turned negative after an initial positive result , the long isolation and the pain due to graft - versus - host disease psychologically affected the patient . 
therefore , psychological intervention important for patients with covid - 19 who have experienced other issues , physically and mentally , apart from their primary disease . is extremely it is worth mentioning that telemedicine has an important role in the diagnosis and treatment of patients with cancer in home care . 
patients with newly diagnosed cancer or those on anti - tumour therapy should use internet or telephone services as the first choice to contact their doctors , refraining from going directly to hospital , to avoid infection . 
by comparing the numbers of the patients who sought medical help online , we found that each of 24 oncologists who provided these services , on average , attended 19 patients online and 97 clinic visitors during the first 2 weeks before jan 20 . 
conversely , during the 2 weeks after jan 20 , the number of online patients rose to 42 whereas the number of clinic visitors dropped to 36 ( figure 2 )  . 
we believe , in the future , telemedicine will be an important practicing mode for oncologists or other clinicians during pandemics . between january and march , 2020 , we witnessed the infection and deaths of a large number of people because of lack of protection , shortage of beds , and inadequate isolation . 
to prevent the epidemic from returning , we should be well informed about covid - 19 , do early screening , protect our medical workers , properly equip our hospitals for both routine service and future crises and expand our services to internet platforms . 
as oncologists , we hope that society extends its compassion towards patients with cancer during the covid - 19 pandemic . heng mei , xiaorong dong , yadan wang , liang tang , * yu hu two weeks before january 20 two weeks after january 20 online oine online oine figure 2 : average number of online and clinic visitors per week per oncologist chemotherapy protocol should be adjusted , the dose reduced , or both . 
patients with blood cancer were more predisposed to sars - cov - 2 infection than were patients with solid tumours ( in hospitalised patients , the rate of sarscov - 2 infection was ten [ 61% ] of 165 patients with blood tumours and 14 [ 14% ] of 1021 patients with solid tumours )  . 
among the 33 patients with cancer with covid - 19 ( figure 1 ) , eight treated by targeted therapies ( kinase inhibitors and proteasome inhibitors ) and two receiving immune checkpoint inhibitors had more 636 vol 21 may 2020 perspectives oncology , fake news , and legal liability in trust between the the decline lay public and professional opinion is a major chal lenge . 
at the centre of this crisis , is a collision between personal autonomy , specious journalism , social media , widespread dis infor mation , and political marginalisation , which together undermine the value placed on science and academic endeavour . 
in oncology , this situation manifests itself in numerous waysmost notably through patient selfdiagnosis and demand for specific treatments irrespective of their doctors advice ; escalating numbers of patients using alternative unproven therapies ; and increasing reliance on socalled defensive medicine to fend off lawsuits . institute in 2017 , researchers in a jama oncology study published on july 19 , 2018 , and in an earlier article in the journal of the national cancer investigated the association between the use of complementary and alternative medicine , adherence to conventional treatment , and overall survival in patients with cancer . 
 found that patients using together , the studies complementary medicine are more likely to refuse surgery , radiotherapy , or chemotherapy , and patients using complementary or alternative medicine are more than twice as likely to die than those treated with conventional medicine . 
how has society got to this point , where unproven interventions are being chosen in preference to evidencebased , effective treatments ? unfortunately , disinformation andfranklylies are propagated widely and with the same magnitude as verified evidence due to the ease with which social media , ubiquitous online news platforms , and disreputable marketing exercises can populate information channels , which often do not have sufficient funding to employ subjectspecific journalists to weed out facts from fiction . a further consequence of public distrust in mainstream medicine , spread by socalled fake news , misreporting , or contradictory stories , is a tendency for doctors to overtreat patients to prevent claims of malpractice . 
this number was met with scepticism , but a recent us national bureau of economic research working paper provides some evidence to support the under lying hypothesis that huge sums of money are spent needlessly . 
the article shows the fear of lawsuits increases us healthcare expenditure by about 5% ( equivalent to about $170 billion ) and outcomes for patients who get extra care are no better than in those who do not . 
numerous legal reforms have been suggested to shield doctors from excessive liability , including immunity from malpractice claims , caps on the amount of damages awarded , or the use of administrative courts rather than juries . 
 despite these existential pressures , according to the 2018 medscape oncologist compensation report , twothirds of us oncologists still say the most rewarding part of their job is their relationship with patients , the challenge of making the right diagnosis , or being proud of the job they do . 
however , the report , which surveyed over 20 000 oncologists , also found that 41% were worried about the number of rules and regulations they must comply with , problems associated with dealing with difficult patients , or being sued , all of which emphasises the levels of stress health professionals are exposed to and the constant battle against external factors beyond the satisfaction of their core role . in the current era of fake news and public distrust in the establishment , efforts must be redoubled to better communicate medical advances accurately with the lay public and with patients to ensure genuine knowledge can be separated from false material . 
for example , the uk charity , macmillan cancer support , has recently hired a digital nurse specialist to help debunk fake news via an online questionandanswer service , and the us national institutes of health give detailed tips on how to evaluate health information on the internet . 
 if these challenges are not addressed soon , the great advances in science and medicine that have markedly improved human health worldwide could be easily undone and society will come to regret such inaction and reliance on unreliable sources of information . 
we aimed to assess the value of her2 and top2a as predictive markers of response to anthracycline - based adjuvant therapy in patients with early breast cancer . methods we did a meta - analysis of individual patient data from ve randomised adjuvant trials that compared anthracycline - based regimens with cyclophosphamide , methotrexate , and uorouracil ( cmf ) regimens . 
we calculated hazard ratios ( hr ) to compare event - free survival ( efs ) and overall survival in patients receiving anthracycline - based treatment with those receiving cmf in two her2 cohorts ( her2 ampli ed and non - ampli ed tumours ) and in three top2a cohorts ( normal , ampli ed , and deleted tumours )  . findings we analysed data for 3452 patients for her2 and 3102 patients for top2a . 
for efs , hrs were 089 ( 95% ci 079101 ) for her2 non - ampli ed patients and 071 ( 058086 ) for her2 - ampli ed patients ( pinteraction = 00485 ) ; for overall survival , hrs were 091 ( 95% ci 079105 ) for her2 non - ampli ed patients and 073 ( 059089 ) for her2 - ampli ed patients ( pinteraction = 00718 )  . 
in analysis of top2a status , hrs for efs were 088 ( 078100 ) for normal , 063 ( 046087 ) for deleted , and 062 ( 043090 ) for ampli ed ( pinteraction = 00513 ) ; hrs for overall survival were 089 ( 078103 ) for normal , 068 ( 049095 ) for deleted , and 067 ( 046098 ) for ampli ed ( pinteraction = 01608 )  . 
 when patients with top2a - deleted and top2a - ampli ed tumours were grouped together ( altered cohort ) and compared with data from patients with normal top2a tumours , hrs for efs were 064 ( 050081 ) for altered and 088 ( 078100 ) for normal ( pinteraction = 00183 ) ; hrs for overall survival were 067 ( 052086 ) for altered and 089 ( 078103 ) for normal ( pinteraction = 00455 )  . interpretation although her2 ampli cation and combined top2a ampli cation and deletion may have some value in the prediction of responsiveness to anthracycline - based chemotherapy , our ndings do not support the use of anthracyclines only in patients with her2 - ampli ed or top2a - aberrated tumours . funding associazione italiana ricerca cancro , academy of finland , belgian federation against cancer , cancer research uk , les amis de linstitut bordet , scottish breast cancer trials group , ncic clinical trials group , canadian cancer society research institute , danish council for strategic research , pharmacia - upjohn ( now p zer ) , and abbott laboratories . from several introduction findings retrospective analyses of randomised trials have suggested that anthracyclinecontaining adjuvant therapy might be bene cial to only those patients with breast cancer who have her2 gene ampli cation or protein overexpression , 14 but this e ect cannot be explained by any biological rationale . 
one of the the topoisomerase ii proteinthe gene for which , top2a , is on chromosome 17q12 - q21.5 other retrospective analyses have suggested that anthracycline - containing adjuvant therapy might be most e ective in patients whose tumours carry ampli ed top2a.68 however , this association was not seen in a study reported in 2008.9 two studies suggested that top2a gene deletion might targets of anthracycline intracellular also confer increased sensitivity to anthracyclines , 10 , 11 although , as with her2 , this e ect cannot be explained by any biological rationale.5 these studies have lent support to the idea of a tailored approach to the use of anthracyclines . 
nevertheless , none of them alone could safely lead to rm conclusions for daily practice , because small study sample sizes have necessitated caution in application to routine care of patients . 
 national laboratories quality control an external laboratory ( laboratory of cancer biology , university of tampere , tampere , finland ) was originally going to do the central assessment of her2 and top2a for all tumour specimens with sections cut from tissue microarrays . 
however , in december , 2006 , the protocol was amended because preliminary data showed suboptimum concordance between results from the external laboratory and those from the four national laboratories that did the assessments for the original studies when the external laboratory tested her2 and top2a on tissue microarray sections . 
testing for both markers at the four national laboratories was done by uorescent in - situ hybridisation ( fish ) , as described in the individual publications.4 , 6 , 911 in the external laboratory , testing was done by fish with three probes for her2 , top2a , and the centromere of chromosome 17 ( abbott laboratories , abbott park , il , usa )  . 
for this analysis , a tumour was de ned as her2 ampli ed or top2a ampli ed if the ratio between her2 or top2a gene copy number and number of copies of chromosome 17 centromere was two or more ; we regarded top2a gene to be deleted if the ratio was 08 or lower and to be top2a normal if the ratio was greater than 08 but lower than two . 
we estimated concordance in her2 and top2a scores between the external and the four national laboratories by calculating the proportion of cases with the same de nition of gene status ( ie , ampli ed or non - ampli ed for her2 , and ampli ed , deleted , or normal for top2a )  . 
 during on - site monitoring visits , local data , sample ow , and fish protocols were collected and veri ed for at least 50 randomly selected patients in each national laboratory . 
 level of compliance to randomised interventions was veri ed for each individual trial . subgroup analysis we prospectively de ned four biologically homogeneous cohorts : ( 1 ) highly hormone - sensitive tumours , de ned as oestrogen - receptor and progesterone - receptor positive ( 10% of immunostained cells ) , her2 non - ampli ed , and grade 12 ; ( 2 ) moderately hormone - sensitive tumours , de ned as oestrogen - receptor positive and progesteronereceptor negative independent of grade and her2 gene status , or oestrogen - receptor and progesterone - receptor positive and grade 3 , or her2 gene ampli ed ; ( 3 ) her2ampli ed tumours which were oestrogen - receptor and progesterone - receptor negative ; and ( 4 ) triple - negative tumours , de ned as oestrogen - receptor and progesteronereceptor negative and her2 non - ampli ed . 
we identi ed these four cohorts on the basis of gene expression signature studies reported in the past decade.17 oestrogenreceptor , progesterone - receptor , and histological grading were assessed at either local pathology units ( piccart and colleagues , 14 ejlersten and colleagues , 15 and poole and colleagues [ neat and br9601 trials ] 16 ) or the national laboratory ( levine and colleagues13 )  . 
 considering this assump tion , we ran the analysis by molecular subgroups twiceie , with and without the data from the neat and br9601 trials.16 the two analyses gave very similar results , so the molecular subgroup analyses include data from the neat and br9601 trials.16 statistical analysis the primary study endpoint was the comparison in terms of efs and overall survival between patients who received anthracycline - based treatment and those who received cmf in the two her2 cohorts ( her2 ampli ed and non - ampli ed tumours ) and in the three top2a cohorts ( top2a normal , ampli ed , and deleted tumours )  . 
in a secondary efs and overall survival analysis , the log - rank test was adjusted by the main prognostic factorspathological tumour size ( 2 cm or > 2 cm ) and number of ipsilateral positive axillary nodes ( node - negative , 13 positive nodes , or 4 positive nodes )  . 
 the test for interaction had two degrees of freedom when patients were divided by top2a status into three cohorts ( ie , normal , ampli ed , or deleted ) and one degree of freedom when patients were allocated in two cohorts ( ie , normal or aberrated )  . 
we used sas version 9.1 and splus version 7 for statistical analyses . role of funding sources the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results 1003 ( 22% ) of 4558 of patients could not be assessed in the meta - analysis because of an absence of data for her2 or top2a gene status ( table 1 )  . 
when efs curves from patients who participated in the meta - analysis were compared with those from patients who did not , within each trial and by treatment group , we recorded no statistically signi cant di erences ( data not shown )  . 
in piccart and colleagues trial , 14 top2a gene status was assessed only within the her2 ampli ed cohort , which might explain why the rate of top2a gene ampli cation is more than double than that in the other trials . 
likewise , the high proportion of her2 gene ampli cation reported in the ejlertsen and colleagues trial15 might be explained by most patients having oestrogen - receptor - negative disease . 
 the bene t of treatment with anthracyclines over treatment with cmf was greater for individuals with her2 gene ampli cation than it was for individuals without her2 gene ampli cation when analysing efs ( pinteraction = 00485 ) , but not when analysing overall survival ( pinteraction = 00718 ; gure 1 and gure 2 )  . 
we recorded no signi cant di erence in the bene t of treatment with anthracyclines over treatment with cmf when assessing the three separate top2a cohorts in terms of either efs ( pinteraction = 00513 ) or overall survival ( pinteraction = 01608 ; 1138 vol 12 november 2011 articles hazard ratio ( 95% ci ) 139 ( 075257 ) 099 ( 063155 ) 176 ( 048642 ) 070 ( 033149 ) 123 ( 080188 ) 111 ( 087143 ) 122 ( 076196 ) 067 ( 047095 ) 177 ( 032969 ) 061 ( 031123 ) 090 ( 063127 ) 084 ( 069103 ) 043 ( 012147 ) 068 ( 030155 ) 068 ( 040114 ) 086 ( 035211 ) 076 ( 042139 ) 070 ( 051096 ) 134 ( 050362 ) 094 ( 050176 ) 072 ( 040131 ) 037 ( 015090 ) 089 ( 060131 ) 082 ( 063107 ) gure 1 and gure 2 )  . 
however , when top2a ampli cations and deletions were combined ( altered cohort ) , we recorded a signi cant di erence in the bene t of treatment with anthracyclines over treatment with cmf between patients with normal top2a status and those with altered top2a status when analysing both efs ( pinteraction = 00183 ) and overall survival ( pinteraction = 00455 ; gure 1 and gure 2 )  . 
 for when adjusted according to the main prognostic factors ( ie , pathological tumour size and number of positive the e ect of ipsilateral axillary nodes ) , hrs anthracyclines versus cmf in patients with her2 gene ampli cation were 070 ( 95% ci 057085 ; p = 00004 ) for efs and 073 ( 059090 ; p = 0003 ) for overall survival , and , for patients without her2 gene ampli cation , were 085 ( 075096 ; p = 0012 ) for efs and 087 ( 075101 ; p = 0061 ) for overall survival . 
after adjustment , the bene t of treatment with anthracyclines over treatment with cmf was not statistically di erent between individuals with her2 ampli cation and those without her2 ampli cation in either efs ( pinteraction = 010 ) or overall survival ( pinteraction = 017 )  . 
 for top2a , adjusted hrs were 062 ( 042092 ; p = 0019 ) for efs and 068 ( 045102 ; p = 0060 ) for overall survival for patients with top2a ampli cation , 057 ( 041081 ; p = 0002 ) for efs and 064 ( 045092 ; p = 0016 ) for overall survival for patients with top2a deletion , and 086 ( 076098 ; p = 0024 ) for efs and 087 ( 075 100 ; p = 0057 ) for overall survival for patients with top2a normal . 
after adjustment , the bene t of treatment with anthracyclines over treatment with cmf di ered signi cantly between the three groups in terms of efs ( pinteraction = 004 ) but not in overall survival ( pinteraction = 019 )  . 
when top2a ampli cations and deletions were combined , adjusted hrs were 060 ( 047077 ; p = 00001 ) for efs and 063 ( 048082 ; p = 00005 ) for overall survival in patients with top2a alterations , and 086 ( 076098 ; p = 0024 ) for efs and 087 ( 075100 ; p = 0056 ) for overall survival in patients with top2a - normal tumours . 
the bene t of treatment with anthracyclines over treatment with cmf di ered signi cantly between the two groups in terms of both efs ( pinteraction = 0013 ) and overall survival ( pinteraction = 0033 )  . of 2588 patients with data that could be assessed , 740 ( 29% ) were de ned as highly hormone - sensitive , 878 ( 34% ) as moderately hormone - sensitive , 311 ( 12% ) as her2 ampli ed and oestrogen - receptor and progesterone - receptor negative , and 659 ( 25% ) as triple negative ( gure 3 and gure 4 )  . 
we recorded no signi cant di erence treatment e ect of anthracyclines or cmf between molecular subgroups , but individuals with her2 - ampli ed tumours seemed to respond better to anthracyclines and those with highly hormone - sensitive tumours seemed to respond better to cmf ( gure 3 )  . 
we compared treatment groups by top2a gene status within the her2 positive molecular subgroup , and , in all three cohorts , anthracycline - based therapy seemed to be more e ective than cmf ( webappendix p 2 )  . 
 discussion our ndings show a greater bene t from anthracyclinebased adjuvant therapy in patients with her2 gene ampli cation than in patients without such ampli cation and in patients with top2a gene alterations than in patients with normal top2a status . 
however , our study also shows that patients with her2 non - ampli ed or top2a normal tumours might have some additional bene t from treatment with anthracyclines , which than a qualitative suggests a quantitative rather interaction between anthracycline activity and her2 or top2a status . 
 this meta - analysis we trials with di erences in the type of anthracycline - based regimens or in the cmf schedules used ( webappendix p 1 ) , which included vol 12 november 2011 1139 articles patients events risk group anthracycline - based patients events risk group anthracycline - based number at risk anthracycline - based year year patients events risk group anthracycline - based patients events risk group anthracycline - based number at risk anthracycline - based year year figure 4 : event - free survival analysis , by molecular subgroups survival in patients with ( a ) highly hormone - sensitive tumours , ( b ) moderately hormone - sensitive tumours , ( c ) her2 - ampli ed tumours , and ( d ) triple - negative tumours . is a potential limitation in the interpretation of the study results , although we recorded similar associations in the interaction between the activity of treatments and her2 or top2a status in each individual trial . 
 two pooled analyses of previously published data have investigated her2 , but not top2a , in the same setting with similar results.18 , 19 neither of these studies did an external quality control substudy for the testing of her2 or top2a . 
our study design chose the external laboratory as the gold standard , but because tumour samples assessed in the external laboratory were not tested in another laboratory , and because samples from the four national laboratories were not cross - compared , we cannot identify the reason behind the recorded discordance . 
in view of the retrospective nature of this assessment and the restricted sample size , the results of this subgroup analysis have to be regarded as merely hypothesis - generating and should not lead to changes in clinical practice . 
this analysis , prompted by the known molecular and clinical heterogeneity of breast cancer , 17 suggests that , in contradiction to previously reported studies that analysed the her2 non - ampli ed cohort as a homogeneous group , 14 , 6 , 9 , 10 , 18 , 19 di erential bene t from anthracyclines might exist within the her2 non - ampli ed cohort . 
in our analysis individuals with triple - negative or moderately hormone - sensitive tumours 1140 vol 12 november 2011 articles seemed to respond better to treatment with anthracyclines than to treatment with cmf . 
because all triple - negative tumours and almost 90% of moderately hormone - sensitive tumours from this study did not carry top2a gene ampli cation , other mechanisms of increased sensitivity to anthracycline might exist . 
we de ned triple - negative tumours as such if oestrogen - receptor and progesteronereceptor immunostaining was less than 10% , and not less than 1% as suggested in international guidelines.20 however we regard this discrepancy as irrelevant with regard to the suggested bene t from anthracyclines in patients who do not carry top2a gene ampli cation . 
 triple - negative tumours and moderately hormonesensitive tumours are often characterised by high proliferation rates.2123 proliferation signals can lead to topoisomerase ii protein over - expression independently of top2a gene status.24 , 25 indeed , data reported elsewhere2627 draw attention to the absence of concordance between top2a gene status and protein concentrations within the same tumour . 
ideally , quanti cation of nuclear concentrations of the topoisomerase ii protein ( ie , the active protein isoform ) might be the most appropriate way to investigate its predictive value.28 other biological factors not related to top2a have been investigated as potential markers of sensitivity to anthracyclines . 
among those , polysomy of chromosome 17 , which could be a marker of genomic instability and dna repair dysfunction , might play a part.29 moreover , factors involved in the regulation of the stromatumour interaction or in the immune response against a tumour might also be involved.3032 future studies looking at molecular markers to predict response to anthracyclines will have to take into account the fact that probably only a multifactorial system will predict responsiveness to anthracyclines . in conclusion , our ndings do not justify routine use of her2 and top2a as molecular markers to predict anthracycline activity , because women with non - her2 ampli ed and non - top2a altered tumours seem to derive bene ts from treatment with anthracyclines , and because problems exist with the reproducibility of top2a gene status assessment by fish . contributors adl , jmsb , be , kip , cp , ji , hm , fpom , dc , mjp , and mb had the idea for and designed the study . 
cd , jmsb , be , kip , dl , cp , he , hm , fpom , fc , am , cjt , cs , ls , dc , and mjp provided study materials . con icts of interest adl has a consultancy and advisory role for and has received honoraria from schering - plough . 
kip has a consultancy and advisory role for and has received honoraria from roche , abraxis , astrazeneca , p zer , novartis , and amgen , and has given expert testimony for novartis and astrazeneca . 
all other authors declare that they have no con icts of interest . acknowledgments we thank associazione italiana ricerca cancro , abbott laboratories , academy of finland , belgian federation against cancer , cancer research uk , les amis de linstitut bordet , p zer , scottish bc trials group , ncic clinical trials group , the canadian cancer society research institite ( ccsri ) , and the danish council for strategic research for funding . correction to lancet oncol 2014 ; 15 : 150312 correction to lancet oncol 2019 ; 20 : 76980 correction to lancet oncol 2019 ; 20 : 98699 open - label phase 1 / 2 jg , niesvizky r , kumar sk , berdeja et al . 
 lancet oncol 2014 ; 15 : 150312in the eighth paragraph of the results section of this article , the first sentence should have been overall responses were noted in 59 ( 92% , 95% ci 8397 ) of 64 patients ( table 5 )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 765 ben - aharon i , goshen - lago t , fontana e , et al . 
this correction has been made to the online version as of july 1 , 2019 . 2018 jacob s , yap ml , wilson be , ferlay j , bray f , barton mb . 
 lancet oncol 2019 ; 20 : 76980 in the affiliations for this article , dr mei ling yap should have been affiliated with the university of new south wales ( sydney , nsw , australia )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 795805 randomised , controlled hofvind s , holen s , aase hs , et al . 
 lancet oncol 2019 ; 20 : 795805 in figure 1 , the number of patients with screen - detected breast cancer in the digital breast tomosynthesis group should have read 95 , and the number of patients in the digital mammography group should have read 87 . 
 quizartinib versus salvage chemotherapy in relapsed or refractory flt3 - itd acute myeloid leukaemia ( quantum - r ) : a multicentre , randomised , controlled , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 98699in this article , the second sentence in the statistical analysis section should have read the sample size calculation wording in the original protocol specified a 5% , two - sided calculation ; however , this wording was inaccurate , and subsequently , a one - sided calculation at 25% was implemented to solely test for superiority of quizartinib , which is consistent with the primary aim of the study . 
this correction has been made to the online version as of july 1 , 2019 , and the printed article is correct . correction to lancet oncol 2019 ; 20 : e30212 hillengass j , usmani s , rajkumar sv , et al . 
these corrections have been made to the online version as of july 1 , 2019 . vol 20 july 2019 e346 corrections infinity ( f / k / a mosaic biomedicals ) , pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo and bristol myers squibb , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 143748 shitara k , doi t , dvorkin m , et al . 
lancet oncol 2018 ; 19 : 143748in figure 3 in this article , several datapoints were incorrectly plotted , and one value on the scale on the x - axis was incorrect . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in table 1 , under the subheading duration of response the first line should have read patients with an event / patients with objective responses ( % )  . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2018 ; 19 : 151629 velikova g , williams lj , willis s , et al . 
 quality of life after postmastectomy in patients with radiotherapy intermediate - risk breast cancer ( supremo ) : 2 - year follow - up results of a randomised controlled trial . 
in addition to overall survival , both progressionfree survival ( median 82 months vs 59 months ) and the proportion of patients who achieved an objective tumour response ( 48% vs 36% ) were signi cantly improved with the combination of bevacizumab with either of two chemotherapy doublets ( cisplatinpaclitaxel or topotecan paclitaxel ) .1 none of these ndings were accompanied by a signi cant deterioration in quality of life.2 these results led directly to the approval of bevacizumab by the us food and drug administration and the european medicines agency . in the lancet oncology , paul symonds and colleagues3 report the results of the randomised phase 2 , doubleblind , placebo - controlled circca trial . 
the authors report signi cantly improved progression - free survival with six cycles of carboplatinpaclitaxel plus daily administration of cediranib , continued until disease progression or the development of intolerable toxicity ( hazard ratio 058 [ 80% ci 040085 ] ; p = 0032 ) .3 cediranib , a vegfr13 oral tyrosine kinase inhibitor , joins tnp - 470 , 4 pazopanib , 5 and bevacizumab1 , 6 as an anti - angiogenic drug with demonstrable activity in cervical cancer , with the latter two drugs also inhibiting vegf - dependent signalling.7 although this trial was not powered to assess overall survival , the proportion of patients with a response ( 64% ) in the cediranib group is the highest reported for any regimen in this disease.3 the use of carboplatin in circca deserves comment . 
an absence of perceived bene t in colorectal cancer , lung cancer , and glioblastoma curtailed enthusiasm for further development until the results of circca and the icon6 ovarian cancer study were made available . 
 importantly , icon6 represents one of eight pivotal phase 3 anti - angiogenesis trials in ovarian cancer , all of which met their primary endpoint ( progression - free survival ) , with icon6 being the only study to show an overall survival advantage.9 stalled development of cediranib had implications for circca , but fortunately development of the drug has since been resurrected to focus on gynaecological malignancies . similarities in eligibility criteria between circca and gog 240 ( eg , ecog performance status restricted to 01 and no previous chemotherapy allowed for recurrent disease ) suggest that a correlation of the progressionfree survival results might be reasonable ( ie , 81 months in circca is similar to 82 months in gog 240 ) .1 , 3 coste ectiveness remains an issue , 10 especially for low - income nations where the incidence of cervical cancer is highest . 
potential future trial designs might use strategies to study chemotherapy plus bevacizumab with and without cediranib , or randomisation to cediranib maintenance therapy in patients who derive clinical bene t from chemotherapy plus bevacizumab ( eg , stable disease )  . 
if active as a monotherapy , a maintenance could have major cediranib strategy toxicology implications given that the median duration of cediranib treatment in both groups in circca was 19 weeks and overlapped with chemotherapy . 
clearly , the results of circca provide additional clinical evidence that vegf - dependent tumour angiogenesis remains a valid target in cervical cancer and that the need to explore novel anti - angiogenesis combinations and sequencing is implicit . containing krishnansu s tewari the division of gynecologic oncology , university of california , irvine , ca 92660 , usa ktewari@uci.edu i have participated on two advisory boards for genentech / roche ( march , 2014 , and july , 2014 )  . 
cedirinib combined with carboplatin and paclitaxel in patients with metastatic or recurrent cervical cancer ( circca ) : a randomised , double - blind , placebo - controlled phase 2 trial . 
gynecol oncol 2015 ; 137 : 49096 . busulfan - based conditioning regimens : not all partners are equal regimens , many since its introduction in 1987 , the combination of busulfan and cyclophosphamide has been the most frequently used non - total body irradiation - containing myeloablative regimen for acute myeloid leukaemia throughout the world.1 with the introduction of udarabine - containing investigators reduced conditioning replaced the cyclophosphamide with udarabine in an e ort to reduce the toxic e ects that were thought to be caused by cyclophosphamide metabolites.24 the busulfan plus udarabine regimen has become increasingly popular , and although multiple retrospective comparisons have reported that the combination of busulfan and udarabine is less toxic and compares favourably with the classic busulfan plus cyclophosphamide regimen , only two randomised trials5 , 6 have been done , with con icting results . 
both trials were hampered by sample size and patient heterogeneity . in the lancet oncology , alessandro rambaldi and colleagues report the results of a multicentre , randomised trial done through the gruppo italiano de trapianto midollo osseo ( gitmo ) network , which compared busulfan plus cyclophosphamide with busulfan plus udarabine.7 the trial was restricted to patients with acute myeloid leukaemia aged older than 40 years . 
252 patients were randomly assigned to receive intravenous busulfan ( 128 mg / kg ) , in combination with cyclophosphamide ( 120 mg / kg ) or udarabine ( 160 mg / m )  . 
1 - year nonrelapse mortality was 172% ( 95% ci 116254 ) in the busulfan plus cyclophosphamide group compared with 79% ( 43143 ) in the busulfan plus udarabine group ( p = 0026 ) , and this di erence remained signi cant even at 2 and 5 years after transplantation . 
however , no signi cant di erence existed in 5 - year leukaemia - free survival between the two groups ( 429% [ 344536 ] for busulfan plus cyclophosphamide vs 518% [ 436617 ] 1 - year for busulfan plus udarabine ; p = 029 )  . 
the foxfire , sirflox , and foxfire - global randomised studies evaluated the efficacy of combining first - line chemotherapy with sirt using yttrium - 90 resin microspheres in patients with metastatic colorectal cancer with liver metastases . 
the studies were designed for combined analysis of overall survival . methods foxfire , sirflox , and foxfire - global were randomised , phase 3 trials done in hospitals and specialist liver centres in 14 countries worldwide ( australia , belgium , france , germany , israel , italy , new zealand , portugal , south korea , singapore , spain , taiwan , the uk , and the usa )  . 
chemotherapy - naive patients with metastatic colorectal cancer ( who performance status 0 or 1 ) with liver metastases not suitable for curative resection or ablation were randomly assigned ( 1 : 1 ) to either oxaliplatin - based chemotherapy ( folfox : leucovorin , fluorouracil , and oxaliplatin ) or folfox plus single treatment sirt concurrent with cycle 1 or 2 of chemotherapy . 
in foxfire , folfox chemotherapy was oxmdg ( oxaliplatin modified de gramont chemotherapy ; 85 mg / m oxaliplatin infusion over 2 h , l - leucovorin 175 mg or d , l - leucovorin 350 mg infusion over 2 h , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
in sirflox and foxfire - global , folfox chemotherapy was modified folfox6 ( 85 mg / m oxaliplatin infusion over 2 h , 200 mg leucovorin , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
randomisation was done by central minimisation with four factors : presence of extrahepatic metastases , tumour involvement of the liver , planned use of a biological agent , and investigational centre . 
the primary endpoint was overall survival , analysed in the intention - to - treat population , using a two - stage meta - analysis of pooled individual patient data . 
sirflox and foxfire - global are registered with clinicaltrials.gov , numbers nct00724503 ( sirflox ) and nct01721954 ( foxfire - global )  . findings between oct 11 , 2006 , and dec 23 , 2014 , 549 patients were randomly assigned to folfox alone and 554 patients were assigned folfox plus sirt . 
there were 411 ( 75% ) deaths in 549 patients in the folfox alone group and 433 ( 78% ) deaths in 554 patients in the folfox plus sirt group . 
the median survival time in the folfox plus sirt group was 226 months ( 95% ci 210245 ) compared with 233 months ( 218247 ) in the folfox alone group . 
in the safety population containing patients who received at least one dose of study treatment , as treated , the most common grade 34 adverse event was neutropenia ( 137 [ 24% ] of 571 patients receiving folfox alone vs 186 ( 37% ) of 507 patients receiving folfox plus sirt )  . 
serious adverse events of any grade occurred in 244 ( 43% ) of 571 patients receiving folfox alone and 274 ( 54% ) of 507 patients receiving folfox plus sirt . 
10 patients in the folfox plus sirt group and 11 patients in the folfox alone group died due to an adverse event ; eight treatment - related deaths occurred in the folfox plus sirt group and three treatment - related deaths occurred in the folfox alone group . interpretation addition of sirt to first - line folfox chemotherapy for patients with liver - only and liver - dominant metastatic colorectal cancer did not improve overall survival compared with that for folfox alone . 
after complete resection of liver metastases from metastatic colorectal cancer , approximately 3540% of patients survive for 5 years.5 the european organisation for research and treatment of cancer ( eortc ) intergroup clocc 400046 randomised study of the addition of radiofrequency ablation with or without surgery to chemotherapy in 119 patients with up to nine colorectal liver metastases , a significant effect on progression - free survival did translate into a significant overall survival benefit . is a at present , the proportion of patients eligible for surgical resection is only 20%.7 among the liver - directed therapies that might improve local control and increase downsizing of tumours to operability , selective internal leading technology.8 radiation therapy ( sirt ) sir - spheres y - 90 resin microspheres ( sirtex medical limited ; sydney , nsw , australia ) containing the - emitter yttrium - 90 ( y - 90 ) are delivered into the arterial supply of the liver under fluoroscopic guidance . 
the delivery of the resin microspheres into branches of the hepatic artery , which supplies the majority of blood to liver tumours , results in selective targeting by high - dose radiotherapy because the healthy liver is supplied predominantly by the portal venous system and therefore relatively spared from radiation exposure.9 research in context evidence before this study metastatic disease affects up to 50% of the more than one million patients diagnosed with colorectal cancer worldwide every year . 
the efficacy of sirt in third - line or subsequent therapy for metastatic colorectal cancer has been evaluated and there are data to suggest that sirt has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . 
we previously published a phase 1 / 2 trial that established the maximum tolerated dose of oxaliplatin - fluorouracil ( folfox ) chemotherapy to combine as concomitant radiosensitising chemotherapy with sirt . 
at the time of planning our studies in 2006 , we searched pubmed and web of science for articles published between jan 1 , 1980 , and may 31 , 2006 , with the search terms : colorectal cancer , colon cancer , rectal cancer , oxaliplatin chemotherapy , 5 - fluourouracil chemotherapy , fluoropyrimidine , selective internal radiotherapy , yttrium - 90 microsphere , radio - embolization , radio - embolisation , trans - arterial radio - embolization , liver metastasis , and hepatic metastasis original articles and review articles , published in english , were reviewed . 
no meta - analyses of sirt treatment of liver metastasis were identified at the time of protocol writing in 2006 . added value of this study the foxfire , sirflox , and foxfire - global , randomised clinical trials were designed to study whether sirt in combination with folfox chemotherapy as first - line therapy for metastatic colorectal cancer can improve overall survival compared with folfox alone . 
to our knowledge , the combined study represents the largest , randomised analysis performed in the field of interventional oncology to address the question of whether improved local control of colorectal liver metastases impacts on overall survival . 
despite higher proportions of patients achieving a response and improved liver - specific progression - free survival , the addition of sirt to first - line oxaliplatin - fluorouracil chemotherapy for patients with liver - only and liver - dominant metastatic colorectal cancer did not improve overall survival or progression - free survival . 
 additionally , to our knowledge , this study provides the most comprehensive account of the risk of adverse events which can occur secondary to sirt when it is used in combination with folfox chemotherapy . implications of all the available evidence because of the absence of overall survival benefit , early use of sirt in combination with first - line , oxaliplatin - fluorouracil - based chemotherapy in unselected patients with metastatic colorectal cancer cannot be recommended . 
careful patient selection and studies investigating the role of sirt as a post - chemotherapy consolidation therapy are required to define the role of sirt in treating metastatic colorectal cancer . 1160 vol 18 september 2017 articles chemotherapy with sirt , 10 building on our phase 1 / 2 trial , in which we established the maximum tolerated dose of oxaliplatin - fluorouracil ( folfox ) chemotherapy to combine as concomitant radiosensitising the foxfire , sirflox , and foxfire - global clinical trials were designed to study sirt in combination with folfox chemotherapy compared with folfox alone as first - line therapy for metastatic colorectal cancer.11 , 12 eligibility criteria and trial designs were pre - planned to be similar so that the three trials could be prospectively combined for analysis of overall survival and secondary endpoints . 
we previously reported that the combination of sirt with folfox in sirflox13 increased liverspecific progression - free compared with folfox chemotherapy alone , but there was no effect on overall progression - free survival . 
in this combined study , we sought to address the question of whether improved local control of colorectal liver metastases impacts on overall survival . survival methods study design and participants the foxfire , sirflox , and foxfire - global randomised , phase 3 trials were done in 14 countries ( australia , belgium , france , germany , israel , italy , new zealand , portugal , south korea , singapore , spain , taiwan , the uk , and the usa ) : in 28 hospitals and specialist liver centres for foxfire , 87 hospitals or centres for sirflox , and 69 hospitals or centres for foxfire - global ( appendix pp 2834 )  . 
two complementary trials were originally planned ( foxfire and sirflox ) , but the foxfire study took longer than anticipated to set up and recruit , so a third study ( foxfire - global ) was added as an independent trial . 
 liver - only or patients had to be eligible for systemic chemotherapy as first - line treatment for metastatic colorectal cancer.1114 eligibility criteria were similar between the three trials , but not identical . 
similarities and differences are highlighted in the combined study protocol paper.14 inclusion criteria included histologically confirmed colorectal cancer with liver - dominant metastases with or without the primary tumour in situ , who performance status of 0 or 1 , limited extrahepatic disease , age of 18 years or older , and life expectancy 3 months or longer . 
exclusion criteria included ascites , cirrhosis , or portal hypertension ( all established by clinical or radiological assessment ) ; thrombosis of the main portal vein ; and peripheral neuropathy grade 1 or worse . 
the protocols for foxfire and sirlox trials and for this combined study have previously been published.11 , 12 , 14 randomisation and masking in all three trials , patients were randomly assigned ( 1 : 1 ) to either folfox chemotherapy alone or folfox plus sirt with minimisation , based on the strata metastasis site ( liver - only vs liver plus extrahepatic metastases ) , extent of tumour involvement of the liver ( 25% vs > 25% measured objectively on baseline ct scan ) , planned use of a biological agent , and investigational centre . in foxfire , patients were allocated using minimisation with a probability of 08 to the treatment that most reduced the imbalance of the above factors . 
the first 30 treatments were allocated using ( simple ) block randomisation ( using variable block sizes of 2 , 4 , and 6 in a ratio of 1 : 2 : 1 )  . 
in sirflox and foxfire - global , an imbalance window of 5 was used ; if the treatment imbalance between the two groups was less than 5 , the treatment was randomly allocated . 
while the trial was in progress , access to the full randomisation lists was restricted to the database development manager at octo and the trial statistician at the centre for statistics in medicine ( csm ; oxford , uk )  . 
in sirflox and foxfire - global , randomisation was done centrally at the national health and medical research council clinical trials centre ( camperdown , nsw , australia ) via an interactive voice response syste participants were enrolled by the investigators in all three trials . 
as none of the trials were masked , once patients were allocated to treatment , participants , all members of the trial team , and treating medical staff knew the treatment allocation . procedures in foxfire , systemic folfox chemotherapy consisted of oxmdg ( oxaliplatin modified de gramont chemo therapy ; 85 mg / m oxaliplatin infusion over 2 h , l - leucovorin 175 mg or d , l - leucovorin 350 mg infusion over 2 h , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
systemic folfox chemotherapy in sirflox and foxfire - global consisted of modified folfox6 ( 85 mg / m oxaliplatin infusion over 2 h , 200 mg leucovorin , and 400 mg / m bolus fluorouracil followed by a 2400 mg / m continuous fluorouracil infusion over 46 h )  . 
 in foxfire , protocol chemotherapy was 12 cycles ; in sirflox and foxfire - global , protocol chemotherapy continued until disease progression or dose - limiting see online for appendix vol 18 september 2017 1161 articles toxicity . 
the oxaliplatin dose was reduced from 85 mg / m to 60 mg / m for three cycles from the cycle coinciding with sirt administration and for two cycles thereafter , based on phase 1 / 2 data.10 dose modifications were permitted in line with standard care ( appendix pp 38 )  . 
we used the patients body surface area , percentage of tumour involvement , and magnitude of liver - to - lung shunting to establish the activity ( gbq ) per dosing chart.12 planned sirt was done on cycle 1 day 3 or 4 or cycle 2 day 3 or 4.10 in foxfire , patients could receive anti - vegf ( eg , bevacizumab ) or anti - egfr ( eg , cetuximab ) from cycle 1 in the folfox alone group and from cycle 7 onwards in the folfox plus sirt group . 
the addition of anti - vegf or anti - egfr treatments to protocol therapy was at the discretion of the treating physician and doses prescribed were according to local policy at the treating centre . foxfire - global , patients could we assessed patients by ct scan every 812 weeks until hepatic progression . 
follow - up assessments included clinical assessment ; ct of chest , abdomen , and pelvis ; and health related quality - of - life ( hrqol ) assessment.11 , 12 , 14 scans were independently reviewed by pharmtrace ( berlin , germany ) for overall and hepatic progression in foxfire using response evaluation criteria in solid tumors ( recist ; version 1.0 ) and in sirflox with recist ( version 1.0 ) with minor modifications.13 independent reviews were not done in foxfire - global . 
all patients were followed up until death or for a minimum of 2 years . health - related quality of life was assessed with the euroqol - 5d three - level questionnaire ( eq - 5d - 3l ) , a generic hrqol instrument15 measuring health in five dimensions ( mobility , self - care , usual activities , pain or discomfort , and anxiety or depression ) , which summarised as a utility score.16 the eq - 5d - 3l was administered during clinic visits at baseline , between the second and the third months after randomisation , at 6 months , at 12 months , and once per year until 60 months from the start of protocol treatment . 
grading of adverse events used the national cancer institute common terminology criteria for adverse events ( version 3 )  . outcomes the primary outcome of this analysis was overall survival , defined as the time from randomisation to death from any cause , with patients who were still alive censored at their last known follow - up date . 
the proportion of patients achieving an objective response in each treatment group was defined as the number of patients achieving a complete or partial response at any point during the trial , up to their first occurrence of hepatic resection , over the number randomised in that group ( early deaths by any cause and unknown responses were included in the demominator )  . 
 the percentage resected in each group was defined as the number of patients who underwent a hepatic resection divided by the number randomly assigned to that group . for progression - free survival or liver - specific progression - free statistical analysis for the primary combined overall survival analysis , a sample size of 810 was originally calculated , but subsequently updated to 1075 patients ( 710 deaths ) using a protocol - specified hazard ratio ( hr ) of 08 , with a control group median overall survival of 197 months and sirt group median overall survival of 246 months , two - sided 5% significance , 80% power , and allowing for 5% noncompliance.14 the updated sample size allowed for a higher median overall survival , the addition of biological agents to protocol chemotherapy ( planned use added as a stratification factor to the randomisation in may , 2011 , for foxfire and sirflox , and incorporated in foxfireglobal since set - up ) and crossover in both directions . 
the study also had 80% power to detect a 6 - month overall survival benefit in the subgroup of patients with metastatic disease restricted to the liver : 708 patients ( 463 deaths ) were needed . 
the cutoff for analysis was chosen such that there was a minimum of 710 deaths overall and 463 deaths in the liver - only subgroup ( assuming a 6 - month increase in overall survival in the sirt - treated , liver - metastasisonly patients ) and a minimum follow - up of 2 years since 1162 vol 18 september 2017 articles the last patient was randomly assigned to treatment . 
 we did two interim toxicity and safety analyses with the combined data from the foxfire and sirflox trials 8 months after at least 80 patients were randomly assigned ( 40 patients per trial ) and 8 months after 300 were randomly assigned ( minimum of 120 patients per trial ) ; foxfire - global was not included in the interim analyses on the combined data . we calculated median follow - up time using the reverse kaplan - meier method . 
we did all efficacy analyses on an intention - to - treat basis per the published statistical analysis plan.14 we estimated overall survival and progression - free survival for each trial using kaplan - meier survival curves , unadjusted log - rank tests , and cox proportional hazards the proportionality survival models . 
hrs for overall survival and progression - free survival from the individual trials were combined using a two - stage , fixed - effect , inverse - variance weighted individual participant data meta - analysis approach.17 the i statistic indicates the proportion of variation in the treatment effect that is due to heterogeneity rather than chance . 
we also estimated causespecific hazards.19 for overall survival , progression - free survival , and liver - specific progression - free survival , we investigated the potential treatment benefit in patients presenting with disease confined to the liver using survival models stratified by trial ( prespecified subgroup analysis )  . 
 the odds of patients having a resection or achieving a response ( overall and liver - specific ) were compared between treatment groups by pooling individual trial odds ratios ( or ) using two - stage individual participant data meta - analysis . 
 a minimum clinically significant difference in eq - 5d scores of 008 has been suggested across all cancers.20 we used analysis of covariance to analyse differences in eq - 5d - 3l utility scores between the two treatment groups , adjusted for eq - 5d - 3l baseline values . 
we made post - hoc comparisons between treatment groups of treatment received after protocol therapy using the mantel - haenszel test , stratifying by trial . we did safety analyses on patients who received at least one dose of chemotherapy in either group and on an astreated basis . 
we included adverse events reported up to 28 days after the end of trial treatment or 7 months after foxfire 1282 discussed at mdt meeting or screened sirflox 561 screened foxfire - global 240 screened 31 failed screening 31 failed screening 918 excluded 712 did not meet inclusion or exclusion criteria 110 patient refusal 96 other reason 364 randomly assigned 530 randomly assigned 209 randomly assigned 182 assigned oxmdg 263 assigned mfolfox6 104 assigned mfolfox6 267 assigned mfolfox6 plus sirt 105 assigned mfolfox6 plus sirt 182 assigned oxmdg plus sirt 179 started folfox chemotherapy 180 started folfox chemotherapy 167 sirt given 252 started folfox chemotherapy 263 started folfox chemotherapy 247 sirt given 102 started folfox chemotherapy 102 started folfox chemotherapy 93 sirt given 1103 included in individual participant data analysis * 549 folfox chemotherapy group 554 folfox chemotherapy plus sirt group figure 1 : trial profile oxmdg and mfolfox6 are equivalent oxaliplatin - fluorouracil - based folfox chemotherapy regimens . 
discontinuation data were available for patients in foxfire and for a subset of patients in sirflox , but were not available for patients in foxfire - global . vol 18 september 2017 1163 articles folfox alone ( n = 549 ) folfox plus sirt ( n = 554 ) folfox alone ( n = 549 ) folfox plus sirt ( n = 554 ) age at randomisation ( years ) 627 ( 231890 ) 634 ( 284896 ) ( continued from previous column ) 14 ( 0923 ) 14 ( 0923 ) extrahepatic metastases status 12 ( 0818 ) 12 ( 0718 ) extent of liver involvement time since diagnosis of primary tumour to randomisation ( months ) time since diagnosis of liver metastases to randomisation ( months ) who performance status primary tumour site not categorisable * primary tumour in situ male female missing missing colon rectum missing missing 361 ( 66% ) 187 ( 34% ) 1 ( < 1% ) 347 ( 63% ) 200 ( 36% ) 2 ( < 1% ) 392 ( 71% ) 137 ( 25% ) 8 ( 1% ) 12 ( 2% ) 302 ( 55% ) 246 ( 45% ) 1 ( < 1% ) 363 ( 66% ) 191 ( 34% ) 354 ( 64% ) 198 ( 36% ) 2 ( < 1% ) 421 ( 76% ) 116 ( 21% ) 5 ( 1% ) 12 ( 2% ) 278 ( 50% ) 275 ( 50% ) 1 ( < 1% ) previous adjuvant chemotherapy 28 ( 5% ) 31 ( 6% ) 520 ( 95% ) 523 ( 94% ) missing 1 ( < 1% ) metastases present at initial diagnosis yes ( synchronous ) no ( metachronous ) missing 475 ( 87% ) 71 ( 13% ) 3 ( 1% ) 483 ( 87% ) 68 ( 12% ) 3 ( 1% ) ( table 1 continues in next column ) randomisation , whichever was earlier ( deemed the safety window )  . 
 * site of primary tumour recorded as both colon and rectum ; the only options in foxfire were colon or rectu minimisation factors ; treating site was also a minimisation factor . 
extrahepatic disease permitted as per trial protocols were foxfire : no more than five metastases in the lung and metastases should have been , in the opinion of either the local multidisciplinary team meeting or after central review of scans arranged via the trials office , amenable to future definitive local therapy , in addition to lung metastases , a single site of other extrahepatic disease was permitted ( eg , multiple lymph nodes in one lymph node region ) after approval by the trials office ; for sirflox and foxfire - global : limited extrahepatic metastases in the lung , lymph nodes , or both were permitted , no more than five nodules in the metastases in the lung were allowed , which were no more than 1 cm in diameter or up to 17 cm in diameter per single lesion ; involvement of lymph nodes in one single anatomic area ( pelvis , abdomen , or chest ) was permitted provided their longest diameter measured less than 2 cintention to treat with a biological agent was not a minimisation factor for these patients because it was introduced after these patients entered the study . table 1 : baseline characteristics of participants in the combined study nct00724503 ( foxfire - global )  . ( sirflox ) and nct01721954 role of the funding source the sponsor had no role in the foxfire study design , data collection , or data analysis . 
jmo , pd , psv , and sl had full access to all of the data in the study and the corresponding author had final responsibility for the decision to submit for publication . results between oct 11 , 2006 , and dec 23 , 2014 , 1103 patients were enrolled and randomly assigned to either folfox chemotherapy ( n = 549 ) or folfox plus single treatment sirt ( n = 554 ) ( figure 1 )  . 
end of follow - up was oct 31 , 2016 , for foxfire , june 1 , 2016 , for sirflox , and nov 30 , 2016 , for foxfire - global , ensuring 2 years of follow - up after the last patient was enrolled ( appendix p 13 )  . 
median followup was 433 months ( iqr 316584 )  . in the first 12 cycles of treatment , 3193 ( 59% of 5369 ) oxaliplatin cycles in the folfox plus sirt group and 3608 ( 68% ) of 5344 cycles in the folfox alone group were at full protocol dose . 
the median number of cycles of folfox treatment was 12 ( iqr 713 ) in the folfox plus sirt group and 12 ( 715 ) in the folfox alone group . 
 in foxfire , 13 ( 4% ) of 364 patients received cetuximab ( four in the folfox plus sirt group and nine in the to 197 folfox group )  . 
after finishing protocol therapy , fewer patients in the folxfox plus sirt group were given irinotecan , fluoropyrimidine , anti - vegf , or anti - egfr systemic therapies upon progression than were patients in the folfox alone group ( appendix p 16 )  . 
66 ( 12% ) of 549 patients randomly assigned to the folfox alone group received sirt in a later course of therapy , whereas 47 ( 8% ) of 554 patients randomly assigned to sirt did not receive sirt . there were 844 ( 77% ) deaths in 1103 patients in the intention - to - treat population over the follow - up period : 296 ( 81% ) deaths in 364 patients in foxfire , 424 ( 80% ) in 530 patients in sirflox , and 124 ( 59% ) in 209 patients in foxfire - global . 
 the median survival time in the folfox plus sirt group was 226 months ( 95% ci 210245 ) compared with 233 months ( 218247 ) in the folfox alone group ; the pooled hr was 104 ( 95% ci 090119 , p = 061 ; figure 2a , c )  . 
sirt = selective internal radiotherapy . ( 261 [ 73% ] of 358 patients in the folfox group , median overall survival 246 months , 95% ci 221264 ; 264 [ 74% ] of 355 patients in the folfox plus sirt group , 245 months , 223263 ; pooled hr 100 , 95% ci 085119 , p = 096 )  . 
in a sensitivity analysis of overall [ 11% ] of survival excluding ineligible patients ( 62 549 patients in the folfox group and 60 [ 11% ] of 554 patients in the folfox plus sirt group were ineligible ; reasons for ineligibility not reported ) , there were 360 deaths ( 74% ) in 487 patients in the folfox group and 382 deaths ( 77% ) in 494 patients in the folfox plus sirt group . 
median overall survival was 239 months ( 95% ci 218250 ) in the folfox group and 234 months ( 218252 ) in the folfox plus sirt group ; pooled hr was 101 ( 95% ci 088117 , p = 086 )  . 
 subgroup comparisons for overall survival of the prespecified subgroups metastatic site , liver involvement , age , sex , who performance status , and tumour in situ , and the post - hoc subgroups primary tumour site , bevacizumab administration , and timing of metastasis are shown in figure 3 . 941 ( 85% ) of 1103 patients had an observed radiological progression or died before progression : 304 ( 84% ) of 364 patients in foxfire , 452 ( 85% ) of 530 patients in sirflox , and 185 ( 89% ) of 209 patients in foxfireglobal . 
progression - free survival was not significantly different between treatment groups ( pooled hr 090 , 95% ci 079102 , p = 011 ; figure 2b , d )  . 
the median progression - free survival in the folfox plus sirt group was 110 months ( 95% ci 102118 ) compared with 103 months ( 97109 ) in the folfox alone group . 
similar results were found in the pre specified subgroup analysis restricted to patients with liver - only metastatic colorectal cancer at baseline ; 297 ( 83% ) of 358 patients in the folfox group had progressed or died in the liver - only subgroup analysis ( median progressionfree survival 111 months , 95% ci 100121 ) ; 292 ( 82% ) of 355 patients in the folfox plus sirt group had progressed or died ( 119 months , 110138 ; hr 086 , 95% ci 073101 , p = 0066 )  . 
the results of a prespecified sensitivity analysis using radiological scan data as reported by sites from all three trials were consistent with the analysis of the centrally reviewed data ( hr 091 , 95% ci 080103 , p = 015 )  . in 271 ( 49% ) of 549 patients in the folfox and 173 ( 31% ) of 554 patients in the folfox plus sirt group , first progression events were radiologically observed in the liver ( figure 4a )  . 
the cumulative incidence of first progression in the liver was lower in the folfox plus sirt group than the folfox alone group ( figure 4a ; appendix p 17 )  . 
the cumulative incidence of progression within the liver in the first 12 months of follow - up was 22% ( 95% ci 1926 ) in the folfox plus sirt group and 39% ( 3543 ) in the folfox alone group . 
in 196 ( 36% ) of 549 patients in the folfox group and 301 ( 54% ) of 554 patients in the folfox plus sirt group , first progression was extrahepatic or death occurred before recorded radiological progression ( figure 4b , appendix p 17 )  . 
table shows grade 3 or worse haematological events occurring in at least 5% of patients , grade 3 or worse non - haematological events occurring in at least 5% of patients , and all sirt - associated adverse events . 
sirt = selective internal radiotherapy . table 2 : adverse events reported in each treatment group sirt group than in the folfox alone group ( figure 4b ; appendix p 17 )  . 
the cumulative incidence of progression outside the liver or death before recorded radiological progression in 12 months of follow - up was 33% ( 95% ci 2937 ) in the folfox plus sirt group and 19% ( 1623 ) in the folfox alone group . 
cause - specific hrs were in the same direction as , and of similar magnitudes to , the subdistribution hrs ( appendix p 17 )  . an objective ( complete or partial ) response over the study duration was achieved in 746 ( 68% ) of 1103 patients ; 400 ( 72% ) of 554 in the folfox plus sirt group and 346 ( 63% ) of 549 in the folfox alone group ( pooled or 152 , 95% ci 118196 , p = 00012 ; appendix pp 10 , 17 )  . 
an objective response was observed in more patients in the folfox plus sirt group than in the folfox alone group in each of the individual trials ( appendix p 17 )  . 
the odds of achieving an objective response in the liver were also higher in the folfox plus sirt group than in the folfox alone group ( pooled or 178 , 95% ci 137231 , p < 00001 ; appendix p 18 )  . vol 18 september 2017 1167 articles over the follow - up period , 182 ( 17% ) of 1103 patients had at least one hepatic resection . 
overall , 94 ( 17% ) of 554 patients in the folfox plus sirt group and 88 ( 16% ) of 549 patients in the folfox alone group had a resection . 
the odds of undergoing a resection were not significantly different between treatment groups ( pooled or 107 , 95% ci 078148 , p = 067 ; appendix p 11 )  . the proportion of patients who had a grade 3 or worse adverse event at each treatment cycle by treatment group , overall and for haematological adverse events , non - haematological adverse events , and neutropenia are shown in the appendix ( p 12 )  . 
of 1078 patients who received at least one dose of study treatment in the astreated population , 755 ( 70% ) had a grade 3 or worse adverse event ( up to 28 days after the end of protocol chemotherapy or the first 7 months after randomisation , whichever was earlier ) ; 375 ( 74% ) of 507 patients in the folfox plus sirt group and 380 ( 67% ) of 571 patients in the folfox alone group ( table 2 )  . 
the odds of a patient having a grade 3 or worse adverse event were higher in the folfox plus sirt group than in the folfox alone group ( pooled or 142 , 95% ci 109185 , p = 00089 , appendix p 13 )  . 
 of 507 patients who received sirt , 231 ( 46% ) had a haematological grade 3 or worse adverse event , whereas 165 ( 29% ) of the 571 patients who did not have sirt had a haematological grade 3 or worse adverse event , the most frequent being neutropenia ( 186 [ 37% ] in the folfox plus sirt group vs 138 [ 24% ] in the folfox alone group ; table 2 )  . 
adverse events of grade 1 or 2 occurring in 10% of patients or more and all grade 3 or worse events are shown in the appendix ( pp 1826 )  . 
 in foxfire , 15 ( 8% ) of 182 patients in the folfox group and 25 ( 14% ) of 182 patients in the folfox plus sirt group discontinued treatment because of an adverse event or serious adverse event ; data were not fully available for sirflox and not available for foxfire - global . 
serious adverse events of any grade occurred in 244 ( 43% ) of 571 patients receiving folfox alone and 274 ( 54% ) of 507 patients receiving folfox plus sirt ( appendix p 27 )  . 
10 patients in the folfox plus sirt group and 11 patients in the folfox alone group died due to an adverse event during the main safety window ( appendix p 26 )  . 
of the eight treatment - related deaths in the folfox plus sirt group , three deaths due to radiation - induced complications of surgery , one due to liver failure , one due to drug - induced pneumonitis , and one due to offtarget delivery of microspheres . 
there were three treatment - related deaths in the folfox alone group : one due to complications of surgery , one due to neutropenic sepsis , and one due to bowel perforation . 
average unadjusted eq - 5d - 3l utility scores were not significantly different between treatment groups at any time point except at 23 months ( appendix p 27 ) ; however , this difference would not be deemed clinically meaningful . discussion the foxfire , sirflox , and foxfire - global randomised studies designed to definitively assess the combination of sirt with folfox versus folfox alone for colorectal liver metastases in the first - line setting have not shown a benefit of adding sirt on overall survival . 
the combined analysis of these three randomised clinical that a global , multidisciplinary trial involving a complex liver - directed therapy can be done with adequate power to answer an important clinical question . trials shows the efficacy of sirt in third - line or subsequent therapy for metastatic colorectal cancer ( ie , salvage therapy of chemotherapy - refractory disease ) has previously been evaluated.21 a randomised trial22 of salvage in patients with metastatic colorectal cancer with liver - confined disease showed a significant benefit of chemotherapy plus sirt versus chemotherapy alone in time to progression . 
these data suggest that sirt has clinical benefit in patients with colorectal liver metastases with liver - dominant disease after chemotherapy . in our study , metastatic colorectal cancer in which the liver is the only site of disease occurs frequently in a subset of patients ; some of these patients can be resected with long - term cures.23 the significant improvement in liver disease control assessed by competing risk analyses did not translate to a benefit in overall survival . 
the absence of benefit of the addition of sirt to folfox on progression - free survival and overall survival in our combined study could be partly explained by the high proportion of patients who developed first progression at an extrahepatic site , independently of whether the metastases were liver - only at baseline or whether there were extrahepatic metastases or primary tumour in situ at baseline . 
despite the better liver control in the folfox plus sirt group compared with the folfox alone group , this observation of extrahepatic progression might also explain the absence of a 1168 vol 18 september 2017 articles in the groups significant difference between the frequency of surgical resection of the liver metastases being done during or after protocol therapy . 
to avoid possible ascertainment bias in interpreting responses and difficulties differentiating disease progression from radiation reaction of the hepatic parenchyma in patients undergoing liver interventional procedure , scans were centrally reviewed by independent readers . 
the absence of an overall survival benefit suggests that early use of sirt in combination with firstline recommended in unselected patients with metastatic colorectal cancer . oxaliplatin - based chemotherapy radiotherapy cannot the in our study , the sirt - treated patients had a similar quality of life to the patients who had chemotherapy only . 
in the as - treated population in the folfox plus sirt group ( n = 507 patients ) , hepatic failure resulted in death of one patient during the main safety window and death of a further two patients during extended follow - up . 
this study provides the most comprehensive account of the risk of adverse events that might occur secondary to sirt when used in combination with folfox chemotherapy . one possible limitation of our study is that significant changes to the management of metastatic colorectal cancer occurred during the 8 - year recruitment period with the introduction of bevacizumab and egfr inhibitors as first - line standards of care , and increased use of liver interventions such as surgery and ablation . 
the non - identical design of the individual trials might also be considered a limitation , but is accounted for by the use of appropriate statistical methods . little progress has been reported in improving overall survival in molecularly unselected populations since the crystal , prime , and tribe studies.2427 in our study , crossover was anticipated and 12% of patients randomised to folfox alone received sirt with a later line of therapy . 
furthermore , 8% of patients assigned to sirt did not receive sirt , a proportion consistent with our previously published data in patients with metastatic colorectal cancer.13 the difference in exposure to posttrial treatments between the two treatment groups might have affected the primary endpoint . 
it is possible that the improved liver disease control observed in the folfox plus sirt group might have influenced physicians to bias towards intensive subsequent treatment , particularly as so - called treatment - holiday strategies were evolving during the recruitment and follow - up periods of less these trials . 
alternatively , it could be postulated that the reduced use of irinotecan after protocol therapy might have been related to increased or prolonged toxicities in the patients in the folfox plus sirt group , including the risk of myelosuppression . 
our analysis of these toxicities for both groups over time showed an apparent increase of grade 3 or worse adverse events in the folfox plus sirt group , particularly haematological events , with the curves gradually converging after 6 months of protocol therapy . in the past decade , the focus of clinical trials has been on improving outcomes for selected biological subtypes in metastatic colorectal cancer with predefined molecular criteria ( eg , mutant ras or braf )  . 
several studies from the past 2 years have reported that patients with rightsided primary tumours have worse survival outcomes and it is possible that these patients benefit less from standard therapies.2830 molecular subtypes in our study are not currently available , but in the dataset available , 179 ( 25% ) of 718 patients had right sided - tumours . 
further analyses are underway to investigate this exploratory finding , with specific scrutiny of ras mutation , braf mutation , and tumour location in study populations who have received sirt in clinical trials . 
 further studies designed to define the potential benefit of sirt to treat colorectal liver metastases from rightsided primaries are warranted . improved radiological response , in conclusion , despite better liver - specific disease control and the foxfire prospective trials did not show a benefitof the combination of sirt with folfox for progression - free survival or overall survival . 
further studies are needed to study the role of sirt in carefully selected patient populations and as a consolidation therapy after chemotherapy . contributors hsw , pg , sl , vg , ag , gvh , and ras designed the study and wrote the protocol . 
hsw , pg , nks , jt , vh , jr , mp , mf , aw , jmi , cw , ra , af , jmo , psv , pd , sl , vg , ag , gvh , and ras interpreted the data , wrote the manuscript , and approved the paper . declaration of interests hsw reports grants , personal fees , non - financial support , and other uncompensated work from sirtex medical and merck serono ; personal fees and non - financial support from celgene ; grants and non - financial support from pfizer ; personal fees and non - financial support from roche and lily outside the submitted work . 
pg reports personal fees from sirtex ; grants and personal fees from roche , amgen , pfizer , merck , bayer , and servier , during the conduct of the study . 
vh vol 18 september 2017 1169 articles reports grants , personal fees , and non - financial support from sirtex medical , merck , and roche , during the conduct of the study ; involvement in a scientific project on radiological imaging from sirtex medical ; grants , personal fees , and non - financial support from merck and roche ; grants and non - financial support from amgen ; grants and personal fees from sanofi ; grants from pfizer and boehringer ingelheim ; and personal fees from bristol - myers squibb , msd , and novartis , outside the submitted work . 
jmi reports personal fees from sirtex medical , during the conduct of the study ; grants from sirtex medical ; and personal fees from sirtex medical , astellas , jannessen , lily , and roche , outside the submitted work . 
jmo reports grants from cancer research uk and sirtex medical , during the conduct of the study ; and non - financial support from sirtex medical , outside the submitted work . 
pd reports grants from cancer research uk and sirtex medical , during the conduct of the study ; and non - financial support from sirtex medical , outside the submitted work . 
gvh reports personal fees and non - financial support from sirtex medical , during the conduct of the study ; and personal fees and non - financial support from sirtex medical , outside the submitted work . 
ras is a consultant for and reports grants and personal fees from sirtex medical and btg , during the conduct of the study ; and reports personal fees from affidea , astrazeneca , boston scientific , cancer research technology , eisai , terumo , and varian , outside the submitted work . 
aw declares no competing interests . acknowledgments the foxfire study design was reviewed and endorsed by the clinical trials awards and advisory committee of cancer research uk , was approved by the national research ethics service committee south central - berkshire ( research ethics committee reference 09 / h0505 / 1 ) , was developed by the national cancer research institute colorectal clinical study group and the national institute for health research clinical research network and equivalents in devolved nations , and was sponsored by the university of oxford . 
we thank georgie perry for secretarial support . re ection and reaction richard g grundy childrens brain tumour research centre , university of nottingham , the medical school , queens medical centre , nottingham ng7 2uh , uk richard.grundy@nottingham.ac.uk the author declared no con icts of interest . grundy rg , wilne sa , weston cl , et al . 
pediatr neurosurg 1998 ; 28 : 21522 . bou et e , perilongo g , canete a , massimino m et al intracranial ependymoma in children ; a critical review of prognostic markers and a plea for cooperation . 
med pediatr oncol 1998 ; 40 : 3440 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zupancic m , shah pc , shah - khan f , nagendra s . 
in this review , the author list should have read : melanie zupancic , prabodh c shah , farheen shah - khan , sanjai nagendra . grundy rg , wilne sa , weston cl , et al . 
 full total resection less than full total resection 100 075 050 025 000 numbers at risk total resection 44 partial resection 45 time from surgery ( years ) 7 figure 5 : overall survival based on neurosurgical assessment of the extent of resection at the end of surgery vol 8 september 2007 comment with colorectal cancer ? there are some arguments against this opinion . 
first , the results of the focus2 trial6 supported the use of rst - line oxaliplatin - based combination chemotherapy rather than uoropyrimidine monotherapy in elderly or frail patients with advanced colorectal cancer , although the primary endpoint of progression - free survival did not di er signi cantly . 
 second , pooled analyses7 , 8 of elderly patients randomised studies showed a bene t of oxaliplatinbased or irinotecan - based combination chemotherapy in patients aged 70 years and older similar to that in younger patients . 
finally , a pooled analysis9 showed that upfront combination chemotherapy ( compared with uoropyrimidine monotherapy ) showed a slightly higher in patients with a performance status of 2 than in those with a performance status of 01 , 9 which suggests that e ective rst - line combination chemotherapy is necessary for preventing early cancer - related death in some elderly patients without comorbidities , but with heavy tumour load . 
 stefan kubicka cancer center reutlingen , 72764 reutlingen , germany kubicka_s@klin - rt.de i am a scienti c advisor to , and have received honoraria from , merck , amgen , sano - aventis , and roche . kopetz s , chang gj , overman mj , et al . 
ann oncol 2012 ; 23 : 153136 . seymour mt , thompson lc , wasan hs , et al , on behalf of the focus2 investigators and the national cancer research institute colorectal cancer clinical studies group . 
irinotecan / uorouracil combination in rst - line therapy of older and younger patients with metastatic colorectal cancer : combined analysis of 2 , 691 patients in randomized controlled trials . 
pooled safety and e cacy analysis examining the e ect of performance status on outcomes in nine rst - line treatment trials using individual data from patients with metastatic colorectal cancer . 
j clin oncol 2013 ; 31 : 146470 . see articles page 1086 hypofractionated breast radiation : preferred standard of care ? in the lancet oncology , joanne haviland and colleagues1 report important 10 - year outcomes of the uk standardisation of breast radiotherapy ( start ) - a and start - b trials.2 , 3 these trials examined whether a shorter hypofractionation radiation schedule was as safe and e ective as the standard 5 week fractionation schedule for the treatment of breast cancer . 
coupled with long - term results from a similar randomised trial led by the ontario clinical oncology group , 4 these ndings provide robust evidence that most patients with breast cancer can receive a hypofractionated schedule that remains bene cial whilst decreasing treatment duration . 
of these two studies , the 1032 vol 14 october 2013 comment start - b trial is more clinically relevant because this study contracted the overall treatment time from 5 to 3 weeks , which provides clear socioeconomic bene ts for both patients and health systems . 
start - b compared the standard treatment of 50 gy given in 25 fractions over 5 weeks with or without a 1 week tumour bed boost with a schedule of 40 gy in 15 fractions over 3 weeks ( hypofractionation ) with or without a 1 week tumour bed boost . 
they found that the two schedules led to similar numbers of patients having local - regional relapse at 10 years ( 55% , 95% ci 4272 vs 43% , 3259 ; hazard ratio [ hr ] 077 , 95% ci 051116 ; p = 021 )  . 
 should these ndings lead to abandonment of the 56 week standard for all patients with breast cancer ? because only a minority of patients ( 116 [ 7% ] of 2215 ) in start - b received regional lymphatic radiation , a more conservative approach might be to continue to use the standard regimen in patients who receive regional nodal irradiation after lumpectomy or mastectomy . 
however , the investigators reported no evidence of increased normal tissue e ects of the brachial plexus , arm oedema , or shoulder sti ness with hypofractionation in patients who did receive lymphatic treatment . 
these clinical outcomes are also consistent with theoretical modelling of normal tissue e ects , which predicts that 40 gy in 15 fractions should be as safe as 50 gy in 25 fractions for all normal tissues.5 thus , we agree with haviland and colleagues that hypofractionation is a reasonable approach even when treating the regional lymph nodes . 
 however , we also understand why many physicians might choose a more conservative approach as far more data are available about the standard regimen for treatment of regional lymph nodes . 
we also concur with the authors that techniques used to protect the heart are important for both radiotherapy schedules and the choice of fractionation should not be a ected by whether the tumour is in the right or left breast . 
 another subject of controversy is whether patients treated with the hypofractionated schedule could subsequently be treated with a tumour bed boost , as is often done for patients treated with the standard radiotherapy regimen . 
although use of a tumour bed boost was optional in the start trials , it was common : 1152 ( 61% ) of 1900 patients who had breast - conserving surgery had tumour bed boost radiotherapy in start - a , as did 868 ( 43% ) of 2038 patients in start - b . 
however , as tumour control and normal tissue outcomes did not di er signi cantly between patients who received tumour bed boost and those who did not , we therefore agree with the authors that the use of a boost with a hypofractionated schedule seems to be safe and e ective . 
 breast cancers are molecularly heterogeneous and tumours with di erent oestrogen , progesterone , and her2 statuses respond di erently to treatment.6 most patients in both the start trials and the ontario study had oestrogen receptor - positive , her2 - negative tumours , therefore the analyses were underpowered to measure the e ect of breast cancer subtype on e cacy of the hypofractionated schedule . 
tumour grade did not have an e ect in the start trials2 , 3 whereas in the ontario trial4 patients with high grade disease had better outcomes with standard radiotherapy . 
 vol 14 october 2013 1033 comment published online september 12 , 2013 s1470 - 2045 ( 13 ) 70403 - 0 see articles page 1095 * bruce g ha ty , thomas a buchholz department of radiation oncology , rutgers - cancer institute of new jersey , robert wood johnson medical school and new jersey medical school , new brunswick , nj 08903 , usa ( bgh ) ; and division of radiation oncology , university of texas , md anderson cancer center , houston , tx , usa ( tab ) ha tybg@cinj.rutgers.edu we declare that we have no con icts of interest . 1 haviland js , owen jr , dewar ja , et al . 
the uk standardisation of breast radiotherapy ( start ) trials of radiotherapy hypofractionation for treatment of early breast cancer : 10 - year follow - up results of two randomised controlled trials . 
jama 2012 ; 308 : 163536 . bayesian analysis unravels pancreas - cancer adjuvant therapy of all the recent advances being made in pancreatic cancer , the three - times improvement in long - term survival from the use of adjuvant chemotherapy after pancreas - cancer resection is the most striking . this notion was rst introduced by the gastrointestinal tumor study group in the usa in the 1970s in a randomised controlled trial comparing a combination of adjuvant chemoradiation with uorouracil with subsequent maintenance chemotherapy , also with uorouracil , with a control group of post - resection observation.1 the target was 150 patients , but this trial was closed after 8 years with just 43 patients recruited , in part because of substantial concerns over toxic e ects . 
 however , there was still a signi cant survival advantage for the adjuvant chemoradiation and maintenance uorouracil group compared to the control group.1 this regimen became common practice in the usa , but the strength of evidence was thought too weak to greatly alter clinical practice elsewhere . 
 that was until the adjuvant european study for pancreatic cancer ( espac ) 1 trial provided strong evidence for improved survival using just maintenance chemotherapy ( using uorouracil and folinic acid ) but , perhaps surprisingly at the time , there was no evidence from the trial data that adjuvant chemoradiation provided any survival bene t.2 , 3 controversially , the factorial design of espac 1 , which aimed to answer the two main questions on adjuvant therapywhether and whether chemotherapy chemoradiotherapy improved survivalwas heavily criticised by some us radiation oncologists and there were also claims of poor radiotherapy quality control.4 however , an eortc trial of adjuvant chemoradiation improved survival follow - on maintenance ( without chemotherapy ) 5 was promoted as supporting evidence for chemoradiotherapy , but was said to be underpowered because there was no signi cant survival advantage compared to the control observation group.4 it was not until 2008 that the rst major us adjuvant trial was published by the radiation therapy oncology group ( rtog ; 9704 trial ) , in which 538 patients were randomised to receive either gemcitabine before ( with uorouracil ) or and after chemoradiation uorouracil before and after chemoradiation.6 there was no di erence in median survival in the 451 patients analysed ( 167 and 18.8 months respectively ) and median survival was actually less than in the espac - 1 chemoradiotherapy group . 
although the rtog 9704 investigators reported the lowest local recurrence rate reported so far ( 23% ) , metastatic spread to the liver and elsewhere was still very high ( 70% ) suggesting relative lack of systemic e cacy in the combination used.6 despite the mounting evidence supporting chemotherapy , now in the form of gemcitabine7 as well as uorouracil plus folinic acid , adjuvant chemoradiation was still being promoted . 
 the simmering controversy led to a strong editorial by renee twombly8 in the journal of the national cancer institute , calling for more data to inform the debate on the use of adjuvant chemoradiation . 
despite further randomised trials supporting adjuvant chemotherapy , adjuvant chemoradiation is still recommended in the usa . in the lancet oncology , a study by wei - chih liao and colleagues9 now pulls together nine controlled trials with a total of 3033 patients randomised to receive 1034 vol 14 october 2013 articles lancet oncol 2014 ; 15 : 110918 published online august 20 , 2014 s1470 - 2045 ( 14 ) 70361 - 4 this online publication has been corrected . 
we report the study design , participant sociodemographic and clinical characteristics , and the initial results of the testing and diagnostic phase of the prostate testing for cancer and treatment ( protect ) trial , which aims to investigate the e ectiveness of treatments for localised prostate cancer . methods in this randomised phase 3 trial , men aged 5069 years registered at 337 primary care centres in nine uk cities were invited to attend a specialist nurse appointment for a serum prostate - speci c antigen ( psa ) test . 
consenting participants with clinically localised prostate cancer were randomly assigned to active monitoring ( surveillance strategy ) , radical prostatectomy , or three - dimensional conformal external - beam radiotherapy by a computer - generated allocation syste randomisation was strati ed by site ( minimised for di erences in participant age , psa results , and gleason score )  . 
 the primary endpoint is prostate cancer mortality at a median 10 - year follow - up , ascertained by an independent committee , which will be analysed by intention to treat in 2016 . 
this trial is registered with clinicaltrials.gov , number nct02044172 , and as an international standard randomised controlled trial , number isrctn20141297 . findings between oct 1 , 2001 , and jan 20 , 2009 , 228 966 men were invited to attend an appointment with a specialist nurse . 
2896 men were diagnosed with prostate cancer ( 4% of tested men and 39% of those who had a biopsy ) , of whom 2417 ( 83% ) had clinically localised disease ( mostly t1c , gleason score 6 )  . 
with the addition of 247 pilot study participants recruited between 1999 and 2001 , 2664 men were eligible for the treatment trial and 1643 ( 62% ) agreed to be randomly assigned ( 545 to active monitoring , 545 to radiotherapy , and 553 to radical prostatectomy )  . 
clinical and sociodemographic characteristics of randomly assigned participants were balanced across treatment groups . interpretation the protect trial randomly assigned 1643 men with localised prostate cancer to active monitoring , radiotherapy , or surgery . 
open access article distributed under the terms of cc by . introduction prostate cancer is the most frequently diagnosed cancer in men in developed countries , with an estimated 241 740 new cases and 28 171 deaths caused by the disease every year in the usa alone.1 in the uk , it is the second most common cause of cancer deaths in men ( 13% ) with 41 763 new cases diagnosed and 10 793 deaths caused by the disease in 2011.2 the disease can be detected early by prostate - speci c antigen ( psa ) measurement followed by prostate biopsy . 
however , most screen - detected cancers are at low risk of progression , and potential harm could be caused by unnecessary diagnosis and treatment . the publication of two population - based randomised controlled trials3 , 4 of screening has not resolved this dilemma . 
the european randomized study of screening for prostate cancer ( erspc ) 3 reported a clear but relatively small disease - speci c survival bene t from screening compared with no active intervention at 8 years and 13 years follow - up , with a larger e ect reported in a smaller scandinavian cohort at 14 years after diagnosis.4 by contrast , the us - based prostate , lung , colorectal , and ovarian ( plco ) trial5 reported no bene t from screening with a similar length of follow - up , but was limited by substantial contamination from previous psa testing in the control group in more than 50% of the unscreened men . most men diagnosed with psa - detected prostate cancer tend to undergo radical treatment . 
the us - based prostate cancer intervention versus observation trial ( pivot ) 6 reported no overall mortality bene t from surgery in patients with psa - detected cancer , whereas the scandinavian prostate cancer group 4 trial ( spcg - 4 ) 7 showed a clear diseasespeci c and overall survival bene t for surgery in patients presenting clinically , as well as a reduction in progression to metastatic disease . androgen the prostate testing for cancer and treatment ( protect ) randomised trial was designed to assess the e ectiveness and cost - e ectiveness of active monitoring ( a surveillance protocol ) , external beam conformal radiotherapy with neoadjuvant radical prostatectomy for men with psa - detected clinically localised prostate cancer . 
the recruitment was undertaken in two stages : a feasibility pilot in three english cities ( in 24 primary care centres linked to three university hospitals ) from june , 1999 , to september , 2001 ( isrctn08435261 ) , and the main trial from october , 2001 , to january , 2009 , in nine cities ( seven in england , one in scotland , and one in wales ) .8 also in 2001 , the cap trial ( cluster randomised trial of psa testing for prostate cancer ; isrctn92187251 ) commenced , which is an extension to the protect trial . 
 the cap trial randomly assigned primary care centres to undertake either the protect trial or standard uk national health service ( nhs ) management ( no routine psa testing ; gure 1 ) , to assess population - based screening in addition to treatment e ectiveness of clinically localised disease identi ed in protect.9 further details of the cap trial design and randomisation have been published previously.10 a written invitation was sent by 337 primary care centres assigned to undertake the protect trial to registered men aged 5069 years , excluding those with a previous malignancy ( apart from skin cancer ) , renal transplant or on renal dialysis , major cardiovascular or respiratory comorbidities , bilateral hip replacement , or an estimated life expectancy of less 10 years . 
men who responded received a protect patient information sheet and an appointment with a specialist nurse who explained the complexities of psa testing , assessed trial eligibility , and sought written informed consent . 
participants with a psa concentration of at least 30 g / l were invited to attend secondary care centres within the nine participating cities for a physical and digital rectal examination and standardised transrectalultrasound - guided prostate biopsies . 
participants with an initial psa concentration at least 200 g / l at diagnosis were excluded because of the high likelihood that they had more advanced cancer . ten - core individual received a protect patients were staged using a combination of digital rectal examination , psa concentration , transrectal ultrasound - guided biopsies , and isotope bone scanning ( if psa was 10 g / l )  . 
men with a psa concentration of 10 g / l or higher or a gleason score of greater than 7 points underwent an isotope bone scan to exclude metastatic disease . 
men with a benign rst biopsy sample and a free - to - total psa ratio below 11% , or atypical small acinar proliferation or 1110 vol 15 september 2014 articles for the study protocol see projects / hta / 962099 high - grade prostatic intraepithelial neoplasia , were o ered further biopsies ; if these repeat biopsy samples were benign , these men were managed in primary care and excluded from the trial . 
no further trial follow - up occurred after the one round of psa testing or identi cation of cancers after referral to the nhs . approval was obtained from the uk trent multicentre research ethics committee ( 01 / 4 / 025 )  . 
study training programmes and on - site monitoring visits were used to standardise trial conduct.11 , 12 randomisation and masking men discussed treatment options with the specialist nurses , and if they agreed to the three - group randomisation ( 1 : 1 : 1 ) , the nurse telephoned a central system in the bristol trials o ce ( bristol , uk ) and logged participant details . 
 allocations were computer - generated as required for each participant , originally using microsoft excel functions , and subsequently in c + + , strati ed by site with stochastic minimisation to improve the balance across the groups in relation to age at primary care patient identi cation date , gleason sum score ( < 7 , 7 , or 810 points ) and mean of baseline and rst biopsy psa results ( < 60 , 6099 , or > 99 g / l )  . 
eligible participants were o ered the choice of a two - group randomisation ( radical prostatectomy or radiotherapy ) , or a three - group randomisation ( with the addition of active monitoring to the two treatment groups )  . 
in 2003 , the independent data monitoring committee ( dmc ) terminated the two - group option because of limited uptake , and the only option for participants who consented was three - group randomisation throughout the remaining period of recruitment . 
men who declined randomisation were o ered identical follow - up and formed a comprehensive cohort within the study design . the procedures participant sociodemographic characteristics , family history of cancer , and previous psa tests were obtained at recruitment . 
 imaging of the skeleton was recommended if serum psa reached 10 g / l , using isotope bone scintigraphy , plain radiographs , and mri as necessary . in patients randomly assigned to active monitoring , the protocol aim was to avoid immediate radical treatment while assessing the disease over time , with radical treatment o ered if disease progression was evident . 
the specialist nurses also met with participants yearly to assess their overall health , and discuss graphical displays of psa results and any concerns raised , overseen by each centres local clinical investigator . 
if the psa concentrations were persistently raised , or the patient had any other concerns , a review appointment was made with the centre urologist for discussion of further tests including re - biopsy and all relevant management options . in patients randomly assigned to receive external beam 3d conformal radiotherapy , neoadjuvant androgen suppression was given for 36 months before and concomitantly with 3d - conformal radiotherapy delivered at 74 gy in 37 fractions.13 quality assurance followed the rt01 trial procedures.14 , 15 psa concentrations were measured every 6 months for the rst year and then yearly . 
the study oncologist held a review appointment with participants if the psa concentrations rose by at least 20 g / l post - nadir or concerns were raised about disease progression.16 management options were discussed , including continued monitoring , further tests , salvage , radical , or palliative treatments as indicated . in patients randomly assigned to receive radical prostatectomy , the predominant approach was open retropubic radical prostatectomy with individual - level quality assurance according to minimum standards.17 participants with a baseline psa concen tration of at least 10 g / l or a biopsy gleason score of at least 7 points received bilateral lymph adenectomy . 
the centre urologist held a review appointment their postoperative psa conwith participants centrations reached 02 g / l or higher to discuss adjuvant radiotherapy . linked translational study obtained biological specimens and epidemiological data.9 outcomes outcome measures were selected for relevance to patients and health - care providers . 
the primary outcome was de ned as de nite or probable prostate cancer mortality , including intervention - related deaths , at a median of 10 years follow - up . 
the process used to assess cause of death was adapted from the plco algorithm5 and erspc process3 and then combined to vol 15 september 2014 1111 articles assess deaths in both the cap and protect studies . 
a full list of all prespeci ed outcomes can be found in our study protocol . for statistical analysis before the start of the trial , a sample - size target of 1434 randomly assigned men ( 478 in each group ) was identi ed as su cient to estimate the absolute di erence in mortality probability between two treatment groups with a 95% ci of 0045 , on the basis of an assumed mortality rate of 15% , consistent with prostate cancerspeci c mortality in men aged 5569 years with clinically detected disease managed conservatively at that time and a di erence that would be deemed clinically signi cant by the nhs . 
 however , more recent data10 suggested that diseasespeci c mortality with non - radical treatment was likely to be closer to 10% at 10 years , because of improvements in disease management . 
as a result , the dmc advised in 2008 that recruitment should continue to the planned end date , with 1590 men ( 530 per group ) expected to be randomly allocated by that point . 
this sample size would enable a 46% reduction in prostate cancer mortality to be detected with 80% power at a 5% signi cance level for a pairwise comparison of a radical treatment with active monitoring . 
this calculation assumes a 10% prostate cancer - speci c mortality at 10 years with active monitoring , and hence a 54% risk with radical treatmentan absolute di erence very similar to the margin of error speci ed in the rst calculation . 
these sample size targets are based on di erences in and ratios of risk rather than the hazard ratios planned for the primary analysis , because the resulting calculations are simpler and more exible . 
when a median of 10 years of follow - up has accumulated ( november , 2015 ) , the primary outcome measure of prostate cancer mortality will be compared between ( cox treatment groups using a survival analysis proportional hazards regression model ) adjusted for strati cation and minimisation variables . 
hazard ratios are interpreted in the same way as rate ratios ; the advantage of hazard ratios and coxs proportional hazards model for this study is the accommodation of variation in the underlying rate of prostate cancer mortality during follow - up . 
 pairwise signi cance tests will only be done if a test of an equal 10 - year disease - speci c mortality risk across all three groups yields a p value of less than 005.26 this approach will be used for event - based secondary outcomesie , grouped analyses of de nite , probable , or possible prostate cancer , all - cause mortality , and metastatic disease . pairwise comparisons of symptom burden will use multilevel models for repeated measures to estimate the average treatment e ect over the median 10 - year followup . 
prespeci ed subgroup analyses will investigate whether treatment e ectiveness in the reduction of prostate cancer - speci c mortality is modi ed by baseline clinical stage , gleason grade , age , or psa concentration using strati ed analyses for descriptive statistics and by formally including interaction terms in the relevant regression models . 
secondary analyses will estimate the e cacy of radical treatment versus active monitoring in the reduction of prostate cancer mortality in individuals who complied with their allocated treatment , by using a method to derive an unbiased estimate in parallel with the per - protocol analysis originally speci ed in the trial protocol.27 , 28 an analysis of primary and secondary outcome measures by trial group is reported yearly to the dmc . 
the dmc recommends changes to the trial steering committee if clear evidence ( of the order of p < 0001 ) of a positive or negative balance of risks and bene ts emerges for one intervention in comparison with the others . data from the recruitment , diagnostic , and randomisation phases are presented , and categorisation of continuous variables is either based on clinical thresholds ( eg , for psa ) or the aim of equal group sizes ( other measures )  . 
129 men were 49 years of age when the primary care list was generated , 120 of whom were 50 years old by recruitment ; 25 men were 70 years or older at generation of the primary care list , of whom four were 71 years of age and one was 72 years of age ; at the time of recruitment , all men who were enrolled tted the stated inclusion criteria as per protocol . 
based on resident area - based material and social deprivation scoreseg , percentage of social housing . table 1 : demographic and clinical characteristics according to diagnosis of prostate cancer in patients recruited into the main protect trial 228 966 men aged 5069 years were invited to participate 106 464 did not respond 122 502 responded 100 444 attended appointment 82 429 were recruited 8566 had an eligible psa result 7414 received prostate biopsies 5468 single biopsy 1946 more than one biopsies 18 015 not recruited 7665 ineligible 10 350 declined to participate 73 863 ineligible psa results 73 538 < 30 g / l 279 200 g / l 46 results not given 1152 did not receive biopsy 3504 biopsy negative or mild 4518 biopsy negative or other 756 high grade pin 255 asap atypia 3 inadequate specimen 479 ineligible 270 advanced disease 209 localised but excluded 2896 had a positive biopsy result for prostate cancer 2417 eligible for randomisation ( localised prostate cancer ) figure 2 : flow diagram of the diagnostic phase of the main protect trial results are from one round of psa testing . 
jal , fch , jld , and den had full access to all the data for this analysis ( full outcome data will become accessible to them from nov 15 , 2015 ) and had nal responsibility for the decision to submit for publication . results between oct 1 , 2001 , and jan 20 , 2009 , 228 966 men were invited to participate in the protect study , of whom 122 502 ( 54% ) responded , although 5954 ( 5% ) of respondents declined to participate and 16 104 ( 13% ) did not attend the appointment with the specialist nurse ( gure 2 )  . 
of the men who attended their appointment , 10 350 ( 10% ) did not enrol or return their second consent form and 7665 ( 8% ) were deemed ineligible . 73 538 ( 89% ) of the 82429 recruited participants had a psa concentration that was below the biopsy cuto point . 
date of birth could not be obtained or age was out of eligible range for 130 recruited participants ; age was out of eligible range for two participants invited for biopsy ; two participants who received biopsy ; and one participant who was diagnosed with prostate cancer . 
 table 2 : psa distribution , biopsy , and prostate cancer diagnosis by age and psa concentration in the main protect trial 2664 participants were eligible 2417 recruited in main trial 247 recruited in pilot study 1643 participants were randomly assigned 1497 from main trial 146 from pilot study 1021 were not randomly assigned 997 selected treatment 24 were randomly assigned to two groups 545 allocated to active monitoring 545 allocated to radiotherapy 553 allocated to surgery figure 3 : flow diagram of the randomisation phase of th e protect trial biopsies were o ered to the 2357 ( 32% ) men without a de nitive diagnosis ; 1563 those o ered underwent the repeat procedure , with a further 322 ( 14% ) receiving a repeat biopsy after advice from a urologist . ( 66% ) of 2896 men were diagnosed with prostate cancer ( 4% of those recruited ; 39% of those who had a biopsy )  . 
additionally , of men with a positive biopsy result , 270 ( 9% ) were ineligible for locally advanced , randomisation because they had advanced , or metastatic disease , and 209 ( 7% ) were excluded because of comorbidity . predominantly , recruited protect participants were white and married or living with a partner , and 4082 ( 5% ) reported a family history of prostate cancer ( table 1 )  . 
 median age was 58 years ( range 5069 ) in the total cohort , with slightly more men younger than 60 years recruited than older men ( table 2 ) , and 11 011 ( 13% ) men had received a previous psa test . 
the relation between higher psa concentrations and prostate cancer diagnosis was unchanged by adjustment for age , whereas the relation between the proportion of recruited patients diagnosed with prostate cancer and increased age was attenuated by adjustment for psa concentration ( unadjusted odds ratio [ or ] data not shown ; table 2 )  . 
ethnic origin , married or partnership status , and extent of material deprivation did not di er between participants diagnosed with cancer and those without cancer ( table 1 )  . ( 62% ) of these eligible patients agreed 2417 men recruited to the main protect trial were eligible , as were 247 from the feasibility pilot phase.8 1643 randomisation ( gure 3 )  . 
the median follow - up is currently 86 years ( iqr 71104 ) and we have obtained vital status ( primary outcome ) info for 99% of patients , and secondary outcomes have been measured in 93% . of the 997 men who declined to be randomly assigned and expressed a preference for a particular treatment , 529 ( 53% ) opted for active monitoring , 273 ( 27% ) for radical prostatectomy , 133 ( 13% ) for radiotherapy , 50 ( 5% ) for brachytherapy , and 12 ( 1% ) selected other treatments . 
 1114 vol 15 september 2014 articles these participants had similar clinical and sociodemographic characteristics to those who were randomly assigned ( table 4 ) , except that they were less likely to reside in an area of material deprivation ( or of increased deprivation in randomised versus non - randomised participants of 074 [ 95% ci 058094 ] )  . discussion the protect trial recruited and tested more than 82 000 community - based men aged 5069 years . 
more than 8000 men had a psa concentration of 30 g / l or more , and of those , 87% received a biopsy , resulting in nearly 3000 men diagnosed with prostate cancer ( 4% of those recruited )  . 
in this initial report , median 8 - year follow - up is more than 93% for all endpoints ( 99% for the primary outcome )  . to active monitoring , the ndings the robustness of the including three conventional the the protect trial was designed to address key issues in the management of clinically localised prostate cancer , speci cally the comparative e ectiveness and coste ectiveness of treatment trade - o between early modalities , diagnosis with psa testing and the risks of over - detection and over - treatment . 
trial design features that will enhance include standardised diagnostic , treatment , and follow - up protocols ; internal and external quality assurance processes ; allocation concealment ; high compliance with follow - up ; extensive secondary outcomes ; and an independent , masked primary endpoint committee . 
the recruitment process was based on psa testing , which is known to over - detect prostate cancer , and has the potential to be superseded by newer diagnostic modalities such as pre - biopsy imaging . 
 additionally , the long natural history of the disease means that the study will have taken more than 15 years to report , from rst patient participation in 1999 to the planned analysis of primary outcome after a median 10 - year follow - up in november , 2015 . 
furthermore , during the past decade radical surgery has evolved with the introduction of robot - assisted and laparoscopic techniques , but few of these new approaches were undertaken in this trial . 
other treatments have also changed : brachytherapy , dose escalation , and intensitymodulated radiotherapy are not being assessed in protect , and active surveillance cohorts now tend to focus on men with a gleason score of 6 points and use scheduled prostate biopsieseg , prias ( prostate cancer research international active surveillance ) .29 another limitation is that the lack of ethnic diversity in the study population might limit the applicability of the protect ndings to non - white populations . 
one patient from the feasibility study had a serum psa concentration of 209 g / l at the specialist nurse visit ; the concentration fell to 176 g / l on repeat measurement and he became eligible for recruitment . table 3 : participant and clinical characteristics at randomisation in the protect trial randomised ( n = 1643 ) non - randomised ( n = 997 ) p value 62 ( 4969 ) 62 ( 5069 ) married or living with partner 1375 ( 84% ) living in area of deprivation 239 ( 15% ) family history of prostate cancer 119 ( 7% ) 1606 ( 98% ) 10 ( < 1% ) 37 ( 2% ) 58 ( 30 ) 1266 ( 77% ) 339 ( 21% ) 37 ( 2% ) 1 ( < 1% ) 1249 ( 76% ) 394 ( 24% ) 984 ( 99% ) 2 ( < 1% ) 11 ( 1% ) 841 ( 84% ) 111 ( 11% ) 83 ( 8% ) 58 ( 31 ) 755 ( 76% ) 218 ( 22% ) 24 ( 2% ) 758 ( 76% ) 239 ( 24% ) 060 031 072 0015 028 067 042 096 4954 5559 6064 6569 psa ( g / l ) 3059 6099 100 gleason score 810 missing clinical stage age ( years ) * ethnic origin white other african - caribbean psa ( g / l ) gleason score 810 missing clinical stage data are median ( range ) or number ( % )  . 
 * 24 patients are classi ed as non - randomised because they were part of the early study with randomisation only between radical treatments ( not active monitoring )  . 
based on resident area - based material and social deprivation scores using several indicators of income and living conditionseg , percentage of social housing . table 4 : demographic and clinical characteristics at randomisation according to randomisation status in the protect trial vol 15 september 2014 1115 articles were men with a psa concentration of 20 g / l or higher because they were likely to harbour non - localised cancer and an increased risk of lymph node metastasis , as shown by joniau and colleagues.30 although we acknowledge that recent advances in imaging techniques would have improved staging in these patients , only 279 ( 03% ) of 82 429 participants in our tested cohort had a psa concentration of 20 g / l or higher . additionally , the recruited population could be generally healthier than the overall population , as often occurs in screening trials , but this does not a ect the compara tive e ectiveness analyses of treat ments.3 , 5 furthermore , uk statistics in 2008 suggested that prostate cancer mortality in the active monitoring group would be around 10% after 10 yearslower than expected at the trial outset . 
 therefore the mortality risk di erence of 46% , upon which the original sample size was based , roughly corresponds to a hazard ratio of 054 in the revised calculationa substantial bene t of radical compared with conservative management . 
should results from this trial support early active intervention , evidence will be needed that bene ts are su ciently large to outweigh the well recognised complications of radical treatments . 
 the primary analysis will be highly informative for clinicians , patients , and decision makers because the trial has been designed to consider mortality , resource use , and quality - of - life outcomes . 
and , as with the other treatment trials , the ndings will continue to be of interest as the data mature over time . treatment options the studys limitations need to be balanced against a number of strengths that ensure that the protect trial will be of pivotal importance in establishing the comparative e ectiveness of the three most frequently used in psa - detected clinically localised prostate cancer . 
it is the largest ongoing randomised controlled trial of prostate cancer treatments worldwide , with standardised protocols for diagnosis , treatment , and follow - up and enabling an assessment of screening through the linked cap trial . 
high levels of generalisability are assured by embedding protect within the cap randomised control trial of population - based psa testing involving about 15% of all uk men aged 5069 years recruited from randomly selected primary care centres . 
 participants with intermediate and some high - risk disease features were included and will help to establish whether active monitoring protocols can o er an alternative to immediate radical intervention in these patients . 
the planned subgroup analyses of treatment erspc ( europe ) 3 plco ( usa ) 5 protect ( uk ) pivot ( usa ) 6 spcg - 4 ( sweden ) 7 screening vs control screening vs control am vs rp vs rt 19932001 19992009 rp vs ww 19942002 rp vs ww 198999 199399 30 / 40 68 896 variable 38 350 228 966 100 444 psa tested ( % of attendees ) * 56 064 ( 2991% ) 34 244 ( 89% ) 82 559 ( 82% ) interventions recruitment period psa biopsy threshold ( g / l ) number of biopsy cores men invited men attended raised psa results biopsy uptake diagnosed with prostate cancer randomly assigned to treatment white ethnic origin mean psa , g / l clinical stage * not recorded gleason score * 26 ( erspc 27 ) * * 710 ( erspc 810 ) * * not recorded 27% 101 130 16% 05% 04% 35% 1643 ( 62% ) 5069 ( 61 ) age range , years ( mean age ) 5569 ( 6063 ) 5575 ( 60 ) 731 ( 15% ) < 75 ( 67 ) 695 ( nk ) < 75 ( 65 ) am = active monitoring . 
 * * erspc gleason grades 24 ( 15% ) and 57 ( 76% ) have been combined ; 810 ( 6% )  . table 5 : design , and participant and clinical characteristics , of the principal screening and treatment trials in clinically localised prostate cancer 1116 vol 15 september 2014 articles panel : research in context systematic review a systematic review of the evidence was done before the design of the trial and informed our protocol development . 
 the review was commissioned by the health technology assessment programme of the national institute for health research in the uk.36 the following search terms were used for a text search within the title , abstract , and keywords : prostate cancer and related terms , and therapy ( speci cally radiotherapy and prostatectomy )  . 
the systematic review concluded that there was insu cient evidence to establish the e ectiveness or cost - e ectiveness of screening or treatments for localised prostate cancer because of the shortage of robust randomised evidence at the time . interpretation the protect trial is , to our knowledge , the largest contemporary randomised controlled trial investigating the e ectiveness of conventional treatment options in men with clinically localised prostate cancer detected after psa testing . 
 the protect trial clearly di ers from two previously published treatment trials6 , 7 that compared surgery with watchful waiting ( a passive observational option ) in men with clinically detected disease ( spcg - 4 ) 7 and older veterans administration men with psa - detected disease ( pivot ) .6 in the protect trial , these baseline results show that we successfully recruited men aged 5069 years after community - based psa testing and a high proportion agreed to be randomly assigned between the three major conventional contemporary options ( surveillance , surgery , and radiotherapy ) , and have achieved high levels of follow - up . 
in 2016 , the trial will publish its outcome data . e ectiveness by stage and grade will investigate this aspect and assist comparison with spcg - 4 and pivot treatment trial patients . 
furthermore , the assessment of a radiotherapy and neoadjuvant regimen will be relevant for patients with higher risk disease because good evidence already exists for endocrine therapy combined with radiotherapy for advanced disease.31 protect detected more prostate cancer in the rst round of testing than did the erspc and plco trials , probably because of protects lower psa threshold combined with the minimum ten - core biopsy protocol in a population previously unexposed to routine psa testing . 
the clinical characteristics of the participants cancers in the protect trial are similar to those of other unscreened populations.32 cancer was generally detected at a lower stage and grade in protect participants than in a uk cohort of patients with clinically detected prostate cancer in the early 2000s.33 however , this reduction in stage and grade would have been mitigated by the upward grade migration reported in gleason scoring in nhs practice between 2000 and 2010.34 nevertheless , the mean proportion of uk men whose psa concentration has been tested remains low by international standards at 6% ( range 29 ) in primary care centres in the mid2000s . 
compared with the pivot6 and spcg - 47 treatment trials , protect participants had the lowest psa concentration , age , and included fewer higher stage cancers at the point of randomisation ( table 5 )  . 
 randomisation of eligible participants was higher in protect ( 62% ) than in pivot ( 15% ) , and other similar trials did not complete recruitment ( eg , start , spirit )  . 
 the acceptability of randomisation in the protect trial was enhanced by integrated qualitative research.35 most notably , protect participants received active monitoring , not watchful waiting as in pivot6 and spcg - 4.7 current active surveillance protocols have more restrictive entry criteria and rely more on scheduled re - biopsy than in protect , but protect trial results will provide , to our knowledge , for a monitoring strategy that includes the option of radical treatment ( panel )  . the rst randomised evidence in 2016 , the protect trial will provide data for the comparative e ectiveness and cost - e ectiveness of active monitoring , radical prostatectomy , and radiotherapy in men diagnosed with localised prostate cancer after psa testing with a median 10 - year follow - up . 
the major ndings will provide key information needed to underpin the management of clinically localised prostate cancer , including the crucial trade - o between survival gains and potential harm caused by over - detection and unnecessary radical treatment in psa - detected prostate cancer . contributors fch , jld , and den designed the protect trial and obtained the funding . 
jal , fch , jld , and den are the guarantors of the manuscript . declaration of interests jld reports grants from the uk national institute for health research ( nihr )  . 
all other authors declare no competing interests . acknowledgments the protect trial is funded by the uk national institute for health research ( nihr ) health technology assessment programme ( projects 96 / 20 / 06 , 96 / 20 / 99 ) with the university of oxford ( oxford , uk ) as vol 15 september 2014 1117 articles sponsor . 
we acknowledge the tremendous contribution of all the protect study participants , investigators , researchers , data monitoring committee , and trial steering comittee ( chair : michael baum )  . 
we acknowledge the support from the oxford nihr biomedical research centre through the surgical innovation and evaluation theme and the surgical interventional trials unit , and cancer research uk through the oxford cancer research centre . 
we are grateful to joke snoeck for her assistance in the preparation of this manuscript . corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 editorial see cancer and society page 812 see articles page 813 see articles lancet 2013 ; published online july 20 . 
 s0140 - 6736 ( 13 ) 61167 - 8 see news lancet respir med 2013 ; 1 : 12 see news lancet respir med 2013 ; published online july 4 . 
 s2213 - 2600 ( 13 ) 70141 - 3 cleaning our polluted skies in this issue of the lancet oncology , ole raaschou - nielsen and colleagues report data from the european study of cohorts for air pollution e ects ( escape ) , a collaboration of more than 30 european cohort studies including almost 1 million participants , which aims to quantify the health risks of air pollution . 
the researchers noted a higher risk of lung cancer , especially adenocarcinoma , with increasing exposure to coarse particulate matter ( less than 10 m in diameter ; pm10 ) , and evidence of a raised risk with increasing exposure to ne particulate matter ( less than 25 m in diameter ; pm25 )  . 
however , perhaps most alarmingly , their data suggest that the risk of lung cancer remains increased even at particulate matter concentrations below current european union ( eu ) limits , challenging existing regulations on air quality . air pollution is a major environmental problem that a ects everyone , with health e ects reaching far beyond lung cancer alone ; indeed , the escape project is also examining the e ects of air pollution on respiratory and cardiovascular diseases , and also on all - cause mortality . 
 of the six most common pollutantsparticulate matter , ground - level ozone , carbon monoxide , sulphur oxides , nitrogen oxides , and leadparticulate matter and ozone represent the greatest risk to health , particularly ne particulate matter , which can penetrate the lungs and bloodstreaa great deal of air pollution results from anthropogenic activity , with the burning of various fuels high on the list of culpritsin industry ( eg , power plants , factories , waste incinerators ) , generated by furnaces and stoves ( ie , use of traditional biomass ) , from motor vehicles , and from agricultural practices ( eg , controlled burns )  . 
 although the 2005 who air quality guidelines were designed to establish global criteria for reducing the health e ects of air pollution , there is wide variation in uptake and adherence . 
at present eu standards , for instance , are more stringent than who guidelines for both ne and coarse particulate matter ; by contrast , concentrations in the us environmental protection agencys december , 2012 , revision of the national ambient air quality standards are more liberal than those recommended by who . 
nevertheless , legislation to limit emissions from industry and transport is in place in both regions , and measures to reduce long - range pollution across country borders have been adopted . 
 for instance , china only began to monitor pm25 concentrations in beijing in october , 20122 years after the us embassy in beijing reported air quality index levels of 755 , a gure more than 20 times higher than safe limits according to who criteria . 
furthermore , it took until june this year for the chinese government to announce ten new measures to improve air quality , including plans to reduce emissions from key industries by 30% by 2017 and to monitor pollution levels in 116 other cities . 
given that recent data suggest that pollution has reduced life expectancy in northern china by as much as 55 years , these initiativesalthough conceived a little too latemust not be allowed to fail . elsewhere , political lobbying stands in the way of progress . 
for instance , burning of the rainforest by farmers to clear land in indonesia for production of palm oil resulted in concentrations of air pollutants in singapore , malaysia , and southern thailand climbing to record levels in june , 2013 . 
although indonesia has a no - burn policy , it is rarely enforced , and the country remains the only member state of the association of southeast asian nations not to have signed up to the groups agreement on transboundary haze pollution . 
 despite measures and recommendations currently in place , escape shows that the risk of lung cancer remains increased even at particulate matter concentrations below levels that are currently deemed to be safe . 
existing e orts , including new energy sources , increased legislation for industry and farming , carbon caps and o setting , and encouraging the use of greener transport and e orts to reduce the need to travel , are undoubtedly part of the solution . 
 however , new solutions are needed that are both pragmatic and e ective , and free from the in uence of competing interestsan ambition that unfortunately still eludes even the most creative ideas to date . 
 the lancet oncology vol 14 august 2013 correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections editorial for the association of schools and programs of public healths response to moonshot see correspondence lancet oncol 2016 ; 17 : e17880 shooting for the moon , and the stars ? spearheaded by us vice president joe biden , cancer moonshot aims to double the rate of progress in the understanding , prevention , diagnosis , and treatment of cancer in the usa in the next 5 years . 
on june 29 , 2016 , biden convened a one - day summit at howard university ( washington , dc ) to bolster support for the programme , emphasising the urgent need to accelerate progress . 
the meeting , attended by hundreds of doctors , researchers , advocates , and patients , was part of a national day of action involving 270 events across the usa . 
so , what can we expect in the coming months and years ? bidens moonshot federal taskforce has big plans : more than 30 public and private sector initiatives were unveiled at the summit , including a new oncology center of excellence at the us food and drug administration ( fda ) to accelerate the development of new cancer therapies ; the redesign of the national cancer institutes ( nci ) cancer.gov portal to make clinical trial data more accessible to oncologists and patients ; the expansion of the ncis open access genomic data commons , providing access to cancer genome data from more than 32 000 patients ; and the creation of new publicprivate partnerships , including a collaboration between the nci , charities , and 2030 pharmaceutical and biotechnology companies to share data and expedite trials . 
the additional funds have yet to be realised or approved , but are anticipated to come from multiple sources : the government has asked congress for another $755 million in 2017 , of which $680 million will go to the nih and $75 million to the fda ; and $200 million in research funding over the next 5 years has been promised by the american cancer society . 
meanwhile , the escalating cost of cancer drugs is another nancial concern : at the summit , biden questioned why pharmaceutical companies have raised the prices of these drugs to astronomical levels since they rst entered the market . 
ironically , such partnerships might drive up drug prices further to maintain pro t margins . in the for accelerating on the other hand , such partnerships should also facilitate data sharingone of the main goals initiatives newly announced of moonshot . 
 partnership therapies , cancer 12 companies have promised to share data with each other and with academic and government researchers , focusing on developing biomarkers , disease modelling , rare cancer treatments , and encouraging trials of combination therapies . 
however , poor enforcement has meant that many research institutions , including those that receive vast government grants , do not adhere to this timescale , and some do not deposit their data at all . 
concerns about data - poaching make researchers reluctant to release data before publication and risk losing credit for their work , plus issues surrounding patient con dentiality also need careful consideration . 
in the coming months , in addition to attainment of su cient funding and the forging of e ective collaborations , careful steps should be taken and safeguards implemented to make sure that researchers feel that they can safely share trial data before publication . 
furthermore , it is vital not to take an overly reductionist view of cancer , and to ensure that other important components of the bigger picturesuch as prevention , universal access to current treatments , and e ective palliative and end - of - life careare not forgotten in the clamour for fashionable objectives . 
 the lancet oncology vol 17 august 2016 1019 published online april 9 , 2020 s1470 - 2045 ( 20 ) 30223 - 0 for more on masks for nhs heroes see crowdfunder.co.uk / masks4nhsheroes for more on the modelling by who on ppe needs see detail / 03 - 03 - 2020 - shortage - ofpersonal - protective - equipmentendangering - health - workersworldwide for more on guidelines on cancer care during covid - 19 see coronavirus - information / careindividuals - cancer - duringcovid - 19%20f workers at the highest risk of acquiring an infection , but the nurses working on the bone marrow transplant unit also need them . disruptions in care patients with cancer are at a high risk of severe covid - 19 disease if they become infected with the virus , and decisions have to be made to reduce their exposure to the virus . 
 but we have to balance the risk of exposure with the risk of not treating or undertreating patients , challinor said . additionally , facilities also reallocated resources to treat patients with covid - 19 , which has resulted in disruptions in routine cancer care . 
guidelines from professional organisations , such as the american society of clinical oncology , suggest implementing protocols that delay elective surgeries , switching from intravenous to oral therapies possible ( to decrease the frequency of clinic visits ) , or modifying or withholding chemotherapy depending on the situation . 
but as the number of patients with covid - 19 increases , many hospitals have deferred all but the most urgent treatment to conserve staff and equipment . however , cancer care cannot be stopped for most patients , and nurses and other personnel caring for patients lack of protective gear disrupts oncology care a recent crowdfunding campaign caught the attention of scottish actor james mcavoy , who was inspired to donate 275 000 to the campaign . 
 coined masks for nhs heroes , the physician - led initiative is raising money to increase the amount of certified one face masks , visors , surgical gowns , and gloves that are available to health - care workers caring for patients with coronavirus disease 2019 ( covid - 19 )  . the outpouring of support from the public has been enormous . 
in their appeal , the doctors note that : unfortunately current hospital supplies are not sufficient and while we are reassured the government is doing everything it can , health - care workers on the frontline are risking themselves daily without adequate protection to care for sick patients . 
health - care workers on the frontline without ppe [ personal protective equipment ] is the equivalent of going to war without armour and protection . the new target was increased to 1 500 000 and the campaign has reached this target ( by april 8 )  . the availability of ppe is largely taken for granted by health - care personnel who work in high - income countries , but the advent of covid - 19 set off a global frenzy to secure supplies that would be needed to provide appropriate protection to health - care workers . 
modelling done by who estimated that 89 million medical masks , 76 million examination gloves , and 16 million goggles would be needed for the covid - 19 response vol 21 may 2020 every month . 
who guidance also called for the rational and appropriate use of ppe for health - care workers and effective management of supply chains . in a response to the current ppe shortage , dame donna kinnair , chief executive and general secretary of the royal college of nursing , said that even though the government is finally prioritising covid - 19 testing for nhs staff , including social care , it is completely unacceptable that weeks into this crisis , there are colleagues in all settingshospitals , community , or care homeswho have not been provided with ppe . she added , i am hearing from nurses who are treating patients in covid - 19 wards without any protection at all . 
 they are putting themselves , their families , and their patients at risk . although much of the attention has focused on ppe use for covid - 19 , the shortage has also affected cancer care , where it is used for both patient and health - care worker protection . 
 the use of chemotherapy - tested gloves , single - use disposable gowns , respirators or masks , eye protection , and closed - system transfer devices are recommended to protect nurses and pharmacists against unintentional exposure to antineoplastic drugs , and protective gear is required to care for patients with cancer who are in isolation or during certain procedures . they are not just for preventing infection but are needed for protecting the health - care workers and any one handling hazardous drugs , said julia m challinor , an international nursing consultant for oncology . 
there is no gold standard on how to measure exposure , but we do know that its not okay to be exposed every day . the idea is also to prioritise equipment , challinor noted . 
face masks , for example , are prioritised for health - care news for more on ons guidelines see interim - guidelines for more on covid - 19 cases among health - care workers in italy see nursingtimes.net / news / coronavirus / nurses - amongconfirmed - deaths - from - covid19 - around - theworld - 20 - 03 - 2020 / for more on covid - 19 cases in spain see com / 2020 / 03 / 24 / world / europe / coronavirus - europe - covid - 19 . html for more on ringwelskis story see com / 2020 / 04 / 01 / opinion / coronavirus - doctors - protectiveequipment.html ? referringsource = articleshare for more on mazurkiewiczs story see chicagotribune.com / news / breaking / ct - nurse - northwesternmemorial - hospital coronavirus - 202003246smjuxbn6fgnxpaiyzzkjymorqstory.html for more on the bellingham hospital story see seattletimes.com / seattle - news / health / er - doctor - who - criticizedbellingham - hospitalscoronavirus - protections - hasbeen - fired / for more on the nyu langone and montefiore health system recommendations regarding media see bloomberg.com / news / articles / 2020 - 03 - 31 / hospitalstell - doctors - they - ll - be - fired - ifthey - talk - to - press for more on gagging of nhs staff see theguardian.com / society / 2020 / mar / 31 / nhs - staff - gagged - overcoronavirus - protectiveequipmentshortages#maincontent need appropriate ppe . 
 the us oncology nursing society ( ons ) has acknowledged that nurses working in cancer care are facing difficult choices if the recommended ppe supplies are not available to the they are making choices regarding the protection of themselves and their patients from potential covid - 19 infection and use of ppe for safe handling of hazardous cancer drugs , says the ons . 
in response to this crisis , the ons has issued interim guidelines for ppe use in oncology settings where ppe supplies might be limited . the royal marsden hospital in london ( uk ) has confirmed that that they have a good supply of ppe , distributed across the hospital according to the latest national guidelines . 
the royal free london nhs trust foundation also reports no issues with ppe . elaine tomlins , consultant oncology nurse , stated that at a hospital on the south coast of england , the oncology unit has moved to a private hospital where there is no covid - 19 care at the current time . 
but there are ppe shortages across the hospital and disinfectant wipes are not available for routine care in oncology . a district general hospital in the west midlands is also reporting shortages in the oncology unit , said young . facing termination about 9% of covid - 19 cases in italy , a country that has been hit hard by the virus , are health - care workers . 
however , many workers do not speak up about the lack of ppe for fear of losing their jobs . in new york city , ny , usa , ania ringwelski , an emergency room physician at weill cornell medical center , did not feel that the ppe supplied by the facility was adequate so she obtained her own . 
in another us city , chicago , il , lauri mazurkiewicz , a nurse working at northwestern memorial hospital , had been warning her coworkers that the standard face masks being distributed by the hospital were not safe for caring for patients with covid - 19 . 
in turn , hospitals have threatened to fire employees who publicly speak about their working conditions and one instance , an emergency room doctor in bellingham , wa , usa , openly discussed the conditions at the facility where he was employed . 
 two health - care systems new york city , nyu langone and montefiore health system , have sent all employees memos reminding them of policies that all media requests must go through the public relations department . 
nyu langone also added that employees would be subject to disciplinary action , including termination , if they did not comply . a similar situation has been reported in the uk , where according to evidence collected by the doctors association uk ( dauk ) , nhs staff are being gagged from speaking out about widespread shortages of ppe . 
one of the testimonies given to dauk was from an intensive care physician who was concerned about the facemasks , but was told by the hospital that if we hear of these concerns going outside these four walls your career and your position here will be untenable . future concerns the us centers for disease control and prevention ( cdc ) has issued guidelines to optimise the use of ppe under the current situation . 
considering that the landscape is changing daily , this is an urgent situation , since hospitals have not faced ppe shortages in the us ever before , so there are no studies showing what is appropriate action , she said . 
what i am afraid of , is that governments in low - income and middle - income countries in the future will say they do not have to buy ppe for oncology nurses because they saw us government agencies recommending homemade ppe for covid - 19 and so they should be fine for oncology as well . 
we do not want governments to be thinking that if it is good enough for covid - 19 , it is good enough for chemotherapy , she added . roxanne nelson 632 vol 21 may 2020 news corrections correction to lancet oncol 2013 ; 14 : 1242 correction to lancet oncol 2014 ; 15 : 606 correction to lancet oncol 2014 ; 15 : 621 rst - line metastatic rini bi , melichar b , ueda t , et al . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : preplanned interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in figure 1 of this article , the box indicating how many patients received the intervention should have read : 652 patients received intervention . 
 this change has been made to the online version as of may 26 , 2014 . vol 15 june 2014 e253 correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
 this correction has been made to the online version as of jan 31 , 2018 . vol 19 february 2018 corrections correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections editorial for more on cancer risk after organ transplantation see jama 2011 ; 306 : 1891901 for more on tg4010 see articles lancet oncol 2011 ; 12 : 112533 tapping our immune potential to realise the ultimate goal last month , the immune surveillance theorywhich proposes that the immune system continuously identi es , and removes , malignant cells as they arisewas lent further weight by an article in jama , which showed that recipients of organ transplants have an increased risk for an array of cancersboth related and unrelated to infection compared with the general population . 
an increase in infection - related cancers ( eg , non - hodgkin lymphoma , gastric cancer , anal cancer , and kaposis sarcoma ) might be anticipated , given that use of immunosuppression to reduce the risk of transplant rejection is likely to result in poor immune control of known oncogenic pathogens . 
 however , the increased risk of , for example , lung and kidney cancers after transplantation noted in a range of patients receiving di erent organs cannot be so easily explained . 
although underlying medical disorders or treatment - related toxicities might have a role , the dampening of the immune system is also likely to be a factor in the development of cancers that are seemingly unrelated to infection . harnessing the immune system to combat cancer has long been a major goal , potentially o ering a more targeted and thus safer means of treatment . 
early attempts to alter the immune milieu for therapeutic gain involved the use of various cytokines , but despite eliciting some durable responses , cytokine treatments can be associated with substantial toxicities , in part because of their non - speci c mode of action . 
further , haemopoietic stem - cell transplantation has long been used in the treatment of haematological malignancies to induce a graft versus disease e ect ; however , treatment - related mortality , availability of donors , and complications from graft versus host disease remain problematic . a more targeted immune approach is an attractive proposition . 
as a result of the successful development of many vaccines against infectious diseases , and their more speci c e ects on the immune system , much e ort has been expended on vaccination strategies against viruses associated with malignancies . 
successes have been achieved with prophylactic vaccines , such as the human papillomavirus ( hpv ) vaccines aimed at precursors of cervical cancer ; however , vaccines against infection by other cancer - associated viruses such as epsteinbarr virus have remained elusive , despite many decades of research and clinical e orts . 
 despite the notable achievement of e ective prophylactic hpv vaccines , less progress has been made in therapeutic vaccine design , both against hpv and other viruses , or in the development of immune - targeted vaccines , with many attempts yielding little evidence of clinical activity . 
 the e cacy of therapeutic vaccines is also limited by the fact that many tumour antigens are self - antigens , and as such the body has an inbuilt tolerance to them ; immunological responses elicited in response to vaccines are thus often insu cient to produce a clinical bene t . however , highlighting the potential usefulness of treatments that manipulate the immune system , several therapeutic strategies are in late - stage trials or entering the clinic . 
 immunomodulatory drugs , such as thalidomide and lenalidomide , are also an established part of the therapeutic armamentarium for various haematological malignancies , although these drugs have multiple modes of action , not only on the immune systefurthermore , combinations of immunotherapy with more conventional anticancer approaches are beginning to yield promising results , as exempli ed by the improvements in progression - free survival for patients with non - small - cell lung cancer seen with the combination of tg4010 , a muc1 - targeted vaccine , and chemotherapy . to fully realise the potential of an immune - based approach , our understanding of the immune systems complex machinery will need to continue to improve at an exponential rate . 
only then can our approaches to control and make use of the hosts immune system become more sophisticated and e cient , allowing us to develop more re ned approaches that tap into a patients natural defence mechanisms , with the ultimate goal of treating cancer without poisoning the patient . 
 the lancet oncology vol 12 december 2011 1175 reection and reaction use of endomyocardial biopsy to assess anthracyclineinduced cardiotoxicity a reection and reaction article , by young and colleagues1 has a few issues with regard to cumulative dose and endomyocardial assessment of cardiotoxicity that need to be corrected . 
none of the three articles quoted by these authors recorded a higher cumulative dose of liposomal doxorubicin than the dose in our report.2 only one of these publications included patients who had undergone endomyocardial biopsy assessment to exclude cardiotoxicity pathologically . 
 in the patients with kaposis sarcoma who were given a different anthracycline , liposomal daunorubicin , only 48% were assessed with at least one echocardiogram and none had histological assessment of anthracycline - induced cardiotoxicity . 
young and colleagues refer to the retrospective study comparing endomyocardial biopsy results ( by use of the billingham scale ) of patients given conventional and liposomal doxorubicin.1 however , the highest cumulative dose of 860 mg / m2 , in a patient who had no documentation of concomitant left - ventricular ejection fraction ( lvef ) , is much lower than the cumulative dose achieved by our patient . intervals furthermore , several important publications were not discussed in the commentary.1 a case series of 42 patients given pegylated liposomal doxorubicin were assessed at baseline and at specic for evidence of cardiotoxicity by use of multigated acquisition scans ( muga ) .3 some of these patients had received previous conventional anthracyclines . 
one patient in this series underwent three endomyocardial biopsies at cumulative liposomal doxorubicin doses of 600 mg / m2 , 900 mg / m2 , and 1320 mg / m2 , with no pathological evidence of cardiotoxicity on the billingham scale . 
a prospective study by gabizon and colleagues4 had enrolled eight patients with advanced malignant disease , all of whom had received previous chemotherapy ( four had been given conventional doxorubicin )  . 
in ve patients with kaposis sarcoma , liposomal doxorubicin cumulative doses ranged from 16802360 mg / m2 but no accompanying endomyocardial documentation of lack of cardiotoxicity was supplied.5 however , three patients had a decrease in lvef on echocardiography . endomyocardial biopsy is the most sensitive and specic investigation available for assessment of anthracyclineinduced cardiotoxicity , but the invasive nature of this test limits routine use.5 endomyocardial biopsy examination can detect cardiotoxicity before any ventricular dysfunction on muga or echocardiography.6 indication of leftcompared with our case , none of the publications described had a higher cumulative dose of liposomal doxorubicin with concurrent endomyocardial conrmation of the absence of cardiotoxicity . 
moreover , the dose achieved was much higher than the lifetime recommended cumulative dose of 450550 mg / m2 for conventional doxorubic this raises the interesting possibility of treatment with liposomal doxorubicin until progression in some circumstances . 
the use of liposomal anthracyclines in combination with other agents , especially trastuzumab , important message we hoped to reinforce . is another * robin l jones , david w miles * department of medical oncology , royal marsden hospital , london , uk . 
department of medical oncology , guys hospital , london , uk ; and breast unit , mount vernon hospital , northwood , middlesex , uk robin.jones@icr.ac.uk we declare no conicts of interest . young am , dhillon t , bower m . 
see - and - treat strategy for diagnosis and management of cervical squamous intraepithelial lesions . lancet oncol 2004 ; 6 : 4350 . in table 2 , data for ref 8 should have been cervical stenosis , 35 of 911 ( 38% )  . 
22 of 101 ( 218% ) occurred with lletz cone and 13 of 810 ( 16% ) with lletz . vol 6 february 2005 correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
lancet oncol 2017 ; 18 : e638 in the declaration of interests section of this correspondence , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics vol 19 december 2018 e667 corrections farewell to four greats as we begin a new year with optimistic anticipation of further achievements in oncology , we must pause to pay tribute to four major innovators and mentors who sadly died at the start of 2019 . on jan 2 , professor waun ki hong , a pioneering physician and scientist at the md anderson cancer center ( houston , tx , usa ) , died aged 76 . 
his work contributed to notable advances in chemoprevention , organ preservation in laryngeal cancer , and personalised targeted therapy . professor bertrand coiffier , who also died on jan 2 , aged 71 , was a leading lymphoma expert , who focused on developing new drug regimens to improve outcomes for aggressive lymphoma . 
he was a professor of hematology at the hospices civils de lyon and the university claude bernard ( lyon , france ) , and was a founding member and president of the groupe detude des lymphomes de ladulte , which later merged with another group to form the world - renowned lymphoma study association . jan 7 , professor john mendelsohn , a former president of the md anderson cancer center , died from glioblastoma , aged 82 . 
he helped to develop the monoclonal antibody cetuximab , which is used to treat colorectal , head and neck , and lung cancers . martin gore , professor of cancer medicine at the institute of cancer research and medical director at the royal marsden hospital ( london , uk ) , died suddenly on jan 10 aged 67 , reportedly after a yellow fever vaccination . 
 he received a cbe in the queens 2016 birthday honours list for services to oncology . as we reflect on the untimely loss of these four inspirational , leading oncologists , this has been a sadand unprecedentedway to start 2019 . 
 the lancet oncology big influences on anti - obesity strategies obesity , the second biggest preventable cause of cancer after tobacco smoking , is a major public health problem worldwide . 
governments must take steps to address this issue ; however , recent reports suggest that chinas antiobesity policies are being influenced by external players . increasingly westernised diets , escalating rural - to - urban migration , and sedentary lifestyles have caused chinas obesity levels to more than double since 1991 . 
in response , the chinese government has launched several public health campaigns , including happy 10 minutes , which encourages schoolchildren to have daily 10 - min breaks for exercise . 
why ? according to recent studies in the bmj and the journal of public health policy , the chinese governments attempts to tackle obesity are being supported by several large multinational food companies , including coca - cola , pepsi - cola , and nestl . 
these companies fund a noninternational life profit research organisation , the sciences institute ( ilsi ) , originally established in the usa in 1978 by a coca - cola executive . 
for several decades , ilsichina has led public health initiatives emphasising the importance of exercise and physical activityrather than nutritionas key to solving the obesity proble by focusing more on physical activity than on a healthy diet , attention is diverted away from highly processed food and calorie - dense snacks and drinks . 
shaping public health policy in this way could help the funding companies to protect sales of their own products and potentially avoid food regulations , advertising rules , and sugar taxes that have been introduced elsewhere . however , diet is clearly crucial . 
governments must not allow their public health strategies to be unduly influenced by powerful multinationals who might be more concerned with protecting their own interests than helping to solve this ongoing health crisis . 
 the lancet oncology vol 20 february 2019 for the bmj report see bmj 2019 ; 364 : k5050 . for the the journal of public health policy study see j public health pol 2019 ; published online jan 9 . 
10.1016 / s0140 - 6736 ( 18 ) 32822 - 8 editorial comment see editorial page 539 any given case of soft - tissue sarcoma the conversation is not as simple as might be inferred by this excellent nomogram , and the conversation must be thorough and nuanced to the individual aspects of each patient . * r lor randall , matthew g cable university of utah , huntsman cancer institute , salt lake city , ut 84112 , usa r.lor.randall@hsc.utah.edu rlr reports other from mts and biomet , outside the submitted work . 
development and external validation of two nomograms to predict overall survival and occurrence of distant metastases in adults after surgical resection of localised soft - tissue sarcomas of the extremities : a retrospective analysis . 
validation and adaptation of a nomogram for predicting the survival of patients with extremity soft tissue sarcoma using a three - grade systecancer 2005 ; 103 : 40208 . bagaria sp , wagie ae , gray rj , et al . 
sarcoma 2015 ; 2015 : 745163 . the eu : whats best for uk cancer research and patients ? the uk faces a momentous decision on june 23 , 2016 , that will determine its future and in uence the future of europe . 
how might the so - called brexit a ect cancer research and cancer care in the uk ? cancer research is a global e ort to which the uk makes a substantial and internationally well - respected contribution . 
uk charities and the government spend approximately 500 million per year on cancer research , and signi cant outputs include world - leading publications across the cancer research spectrum , a prominent role in understanding cancer outcomes at the european level , and world - leading participation in clinical trials . 
the uk in uences and bene ts from eu strategy in cancer research and control , and is learning examples of good practice from other eu countries , such as early cancer diagnosis ( from denmark ) and the management of older patients with cancer ( from france )  . 
from the funding perspective , uk researchers successfully competed for innovations part of the eus 15 billion cancer research funding within the seventh framework programme scheme ( 200714 ) with involvement in more than 80% of funded projects . 
in the prestigious european research council programme , the success of uk cancer researchers has been impressive , securing 77 ( 165% ) of the overall total of 466 grants awarded in all subject areas with a value of 150 million , placing them in europes top tier . 
the 2001 european clinical trials directive , which sought harmonisation and simpli cation of regulations , actually resulted in increased costs and bureaucracy and held back uk clinical trial activity.1 there has been an animated debate and legitimate concerns have been raised about the new eu general data protection regulation and its potential to ( inadvertently ) hinder clinical research . 
 although the eu currently recognises health - care provision as a member state responsibility , emerging data about substantial diversity in cancer costs across the eu2 emphasise the need for europe - wide cooperation for patient inequalities and cancer 556 vol 17 may 2016 comment bene t . 
the relatively poor outcomes observed for uk patients with cancer in the 1990s and early 2000s led to collaborative research , which con rmed and partly explained why cancer survival was lower in , for instance , the uk and denmark , than in some other european countries.3 many of the uks problems have been tackled successfully , but much remains to be done . 
the eu has funded a series of successful member state joint actions against cancer , which inform national cancer plans.4 the launch of the european cancer patients bill of rights in the european parliament on world cancer day 20145 represented an important catalyst for change for patients with cancer ( both uk - wide and europe - wide ) and leadership from europes patient advocates and health - care professionals . 
 involved substantial although collaborations between european cancer researchers , patients , and institutions are still expected to continue if the uks relationship with the eu were to change , their scale and impact would be compromised by a uk exit . 
how would uk researchers fare if access to eu funding ( for which the uk competes so well ) was no longer possible ? could continued access be negotiated or would the uk government subsidise the ( substantial ) shortfall ? human capital in cancer research and control is also a global commodity . 
at a broader level , if a uk exit precipitated a sustained period of nancial uncertainty , this could lead to poorer health outcomes , especially in areas of social deprivation . 
 uk spending on cancer care already falls below the european average , 2 and if nancial uncertainty caused it to fall further we would expect further deterioration in cancer outcomes as a consequence of reduced spending on health care , and the consequential reduction in sta and facilities . 
 we believe that a continued strong collaboration and shared work and funding in cancer research with eu partners , together with sharing best practice in cancer care , is vital to maintain the uks role in improve uk cancer services . 
we must continue to in uence and share european policy in important domains such as clinical trials , data sharing , and clinical best practice , and deliver the highest quality cancer research that underpins improved cancer care for our patients . 
it is for these reasons that we oppose the uk leaving the eu . * peter selby , mark lawler , ian banks , patrick johnston , paul nurse cancer medicine , university of leeds , leeds , uk ( ps ) ; school of medicine , dentistry and biomedical sciences ( ml ) , queens university belfast , belfast , northern ireland , uk ( pj ) ; european cancer concord , leeds , uk ( ps , ml , ib , pj , pn ) ; and francis crick institute , london , uk ( pn ) p.j.selby@leeds.ac.uk ps and ml are joint rst authors . 
ps is president , ml and ib are vice - presidents , and pj and pn are members of the european cancer concord , which is an equal partnership of cancer patients and cancer professionals , and works to promote improvements in cancer outcomes through collaboration in europe in service development and research and innovation ; european cancer concord is not eu funded . 
pj has received personal fees and advising and consulting fees from chugai and p zer , and reports stock shareholding with almac diagnostics , cv6 therapeutics , and fusion antibodies . 
 global surveillance of cancer survival 19952009 : analysis of individual data for 25 676 887 patients from 279 population - based registries in 67 countries ( concord - 2 )  . 
le / 0014 / 235211 / boosting - innovation - and - cooperation - in - europeancancer - control.pdf ? ua = 1 ( accessed april 7 , 2016 )  . lawler m , le chevalier t , banks i , et al , on behalf of the european cancer concord ( ecc )  . 
 lancet oncol 2014 ; 15 : 25860 . vol 17 may 2016 articles lancet oncol 2010 ; 11 : 45058 published online april 14 , 2010 doi : 10.1016 / s14702045 ( 10 ) 70038 - 3 see re ection and reaction page 406 kings college london , school of medicine , division of cancer studies , cancer epidemiology group , london , uk ( m van hemelrijck msc , h garmo phd , prof l holmberg md ) ; oncological centre , clintec department , karolinska institutet , stockholm , sweden ( j adolfsson md ) ; regional oncologic centre , uppsala university , uppsala , sweden ( h garmo , m lambe md , l holmberg ) ; department of urology , uppsala university , uppsala , sweden , and department of clinical cancer epidemiology , karolinska institutet , stockholm , sweden ( a bill - axelson md ) ; department of urology , helsingborg hospital , lund university , sweden ( o bratt md ) ; department of medical epidemiology and biostatistics , karolinska institutet , stockholm , sweden ( e ingelsson md , m lambe ) ; and department of surgical and perioperative sciences , urology and andrology , ume university , ume , sweden ( prof p stattin ) correspondence to : ms m van hemelrijck , kings college london , school of medicine , division of cancer studies , cancer epidemiology group , research oncology , 3rd floor , bermondsey wing , guys hospital , london se1 9rt , uk mieke.vanhemelrijck@kcl.ac.uk risk of thromboembolic diseases in men with prostate cancer : results from the population - based pcbase sweden mieke van hemelrijck , jan adolfsson , hans garmo , anna bill - axelson , ola bratt , erik ingelsson , mats lambe , pr stattin , lars holmberg summary background cancer is associated with an increased risk of thromboembolic diseases , but data on the association between prostate cancer and thromboembolic diseases are scarce . 
we investigated the risk of thromboembolic disease in men with prostate cancer who were receiving endocrine treatment , curative treatment , or surveillance . methods we analysed data from pcbase sweden , a database based on the national prostate cancer register , which covers over 96% of prostate cancer cases in sweden . 
standardised incidence ratios ( sir ) of deep - venous thrombosis ( dvt ) , pulmonary embolism , and arterial embolism were calculated by comparing observed and expected ( using the total swedish male population ) occurrences of thromboembolic disease , taking into account age , calendar - time , number of thromboembolic diseases , and time since previous thromboembolic disease . 
 findings between jan 1 , 1997 , and dec 31 , 2007 , 30 642 men received primary endocrine therapy , 26 432 curative treatment , and 19 526 surveillance . 
for men on endocrine therapy , risks for dvt ( sir 248 , 95% ci 225273 ) and pulmonary embolism ( 195 , 181215 ) were increased , although this was not the case for arterial embolism ( 100 , 082120 )  . 
similar patterns were seen for men who received curative treatment ( dvt : 173 , 147201 ; pulmonary embolism : 203 , 179230 ; arterial embolism : 095 , 069127 ) and men who were on surveillance ( dvt : 127 , 108147 ; pulmonary embolism : 157 , 138178 ; arterial embolism : 108 , 087133 )  . 
 increased risks for thromboembolic disease were maintained when patients were strati ed by age and tumour stage . interpretation all men with prostate cancer were at higher risk of thromboembolic diseases , with the highest risk for those on endocrine therapy . 
 introduction cancer is a risk factor for thromboembolic disease , and patients with cancer are estimated to be around four times more likely to develop a thrombosis than a similar individual without cancer.1 treatments for cancer might also increase the risk of thromboembolic disease . 
for prostate cancer , deep - venous thrombosis ( dvt ) and thromboembolism are common complications after prostatectomy , with risks ranging from 05% to 40% in the 30 days after the operation.25 additionally , the risk of thromboembolic disease increases exponentially with age.6 while several studies have investigated whether patients with prostate cancer treated with endocrine treatment are at higher risk for cardiovascular disease , few populationbased studies have investigated the risk of thromboembolic disease following endocrine treatment.79 during the 1980s , varenhorst and colleagues8 , 9 reported a positive association between the use of cyproterone acetate ( a steroidal antiandrogen ) and brinolytic activity , suggesting a decreased risk of thromboembolisa more recent study , including 11 199 men with prostate cancer , of whom 229 had a venous thromboembolism after diagnosis , showed a greater risk of venous thrombosis associated with cyproterone acetate than with gonadrotropin releasing - hormone ( gnrh ) agonists or orchiectomy.7 thought to have investigation of the risk of thromboembolic disease after endocrine treatment is important for several reasons . 
testosterone cardioprotective e ect , since androgen receptors have been identi ed on the cardiomyocytes and the valves of the heart.1015 preliminary experimental ndings have suggested that androgens might have a role in the regulation of arterial thrombosis through their e ect on platelet activation.16 endocrine treatment is used in a large proportion of men with prostate cancer during the course of the disease , and is the cornerstone treatment for men with locally advanced or metastatic prostate cancer.17 , 18 the indications for endocrine treatment have been widening because of more active treatment in men with advanced disease , and because of neoadjuvant and adjuvant use in men with localised high - risk tumours , resulting in more men of all ages and with all types of prostate tumour receiving endocrine treatment for longer periods.19 we studied a comprehensive population - based cohort with complete follow - up through record linkage of pertinent registers , to assess the risk of thromboembolic disease in men with prostate cancer who had received curative treatment , surveillance , or endocrine treatment . 
 450 vol 11 may 2010 articles methods data collection pcbase sweden is based on the national prostate cancer register ( npcr ) of sweden , which started in 1996 and captures more than 96% of all newly diagnosed , biopsycon rmed prostate cancers . 
this compares favourably with the swedish cancer registry , 20 which misses less than 37% of prostate cancer cases.21 the npcr includes date of diagnosis , age at diagnosis , tumour stage , tumour di erentiation , serum concentration of prostate cancerspeci c antigen ( psa ) at the time of diagnosis , and primary treatment given or planned up to 6 months after the date of diagnosis . 
the validity of primary treatment registered in npcr is more than 90% for curative treatment and surveillance , and more than 95% for endocrine treatment ( stattin p , unpublished )  . 
because of psa screening , the rate of curative treatment increased dramatically during the period of study , whereas the rate of primary endocrine treatment was more or less constant over the same period . 
 the proportion of men with localised disease put on surveillance decreased during this time.22 most endocrine treatment was with gnrh agonists or orchiectomy , although anti - androgens ( not combined with other endocrine treatment ) were prescribed in about 10% of cases . 
 for hormone - resistant prostate cancers , oestrogens and estramustine phosphate were prescribed most often.22 for information by using the swedish 10 - digit personal identity number , pcbase was linked to other national registers , demographics , allowing comorbidities , socio economic status , and causes of death to be collected.23 , 24 in 1987 , the hospital discharge register started collecting information regarding inpatient care . 
each record contains medical information on surgical and anaesthetic procedures , hospital department , and discharge diagnoses coded according to the who international classi cation of diseases 10 ( icd10 ) .23 for heart diseases , the primary diagnoses have been shown to be correct in around 95% of cases , as judged by the european society of cardiology diagnosis guidelines.2527 socioeconomic characteristics were assessed by record linkages to the 196090 5 - yearly census databases , and based on socioeconomic status . 
 socioeconomic status is based on occupational group , and strati es men into white - collar worker ( salaried professionals or educated workers who perform a semiprofessional o ce , administrative , or sales coordination ) , blue - collar worker ( manual workers ) , not gainfully employed , and unknown.24 as of 1997 , the cause of death register collected date and underlying cause of death coded according to icd10.23 detailed information on the data content of pcbase is given elsewhere.28 for our analyses , the following information was taken from pcbase : age , serum concentrations of psa , and treatment information at time of diagnosis , tumour grade and stage , socioeconomic status , history of thromboembolic disease ( primary diagnoses ) , and date of death . 
if who tumour grade was reported primarily instead of gleason score ( 25% of men ) , conversion to gleason score was done as follows : g1 = gleason 26 , g2 = gleason 7 , and g3 = gleason 810 . 
prostate cancer stage was de ned based on the tumour , node , metastasis ( tnm ) stages used in the npcr ( panel ) .22 men with prostate cancer were selected if they received curative treatment , surveillance , or endocrine treatment as primary treatment . 
endocrine treatment was grouped into anti - androgens , oestrogens , orchiectomy , gnrh agonists , gnrh agonist combined with long - term anti - androgens , and other types of endocrine treatment . 
 the swedish central ethics committee ( dnr 14 - 2007 ) the ethics committee at ume university and ( dnr 07 - 049m ) approved this study . statistical analysis we analysed the relation between the di erent types of prostate cancer treatment and subtypes of thromboembolic disease : dvt ( icd10 : i8082 ) , pulmonary embolism ( icd10 : i26 ) , and arterial embolism ( icd10 : k55 , i74 )  . 
 since pcbase is based on the entire swedish population , standardised incidence ratios ( sir ) could be calculated by comparing observed events in the selected cohort ( men with prostate cancer ) with the expected events in the swedish male population . 
the number of events for this standard population was based on the number of men in sweden each year on dec 31 ( register of the total population 19972007 ) .23 , 24 all numbers of events were based on the rst event of thromboembolic disease after a diagnosis of prostate cancer . panel : prostate cancer stage grouping in the national prostate cancer register ( npcr ) of sweden 1 localised ( prostate - speci c antigen [ psa ] < 20 ng / ml ) t02 , n0 or nx , m0 or mx , all grades , psa < 20 ng / ml 2 localised ( psa 20 ng / ml but < 50 ng / ml ) : t02 , n0 or nx , m0 or mx , all grades , psa 20 ng / ml but < 50 ng / ml 3 locally advancedt34 , n0 or nx , m0 or mx , all grades , 4 intermediate groupm0 or mx , psa 100 ng / ml , not in psa < 50 ng / ml stage group 1 , 2 , or 3 5 metastatic diseasem1 or psa > 100 ng / ml 6 missing datamissing t or n or m category / categories or missing grade or missing psa vol 11 may 2010 articles see online for webappendix total ( n ) mean follow - up time ( sd ) age group ( years ) 6574 date period 199799 200002 200306 gleason score 810 missing data prostate cancer stage group localised : psa < 20 ng / ml locally advanced intermediate missing data civil status married single missing data socioeconomic status white collar blue collar 452 the sirs were thus de ned as the ratio of the observed number of a particular thromboembolic disease to the expected number of that thromboembolic disease . 
time of follow - up was taken from the observed numbers of thromboembolic disease , and age - speci c and period - speci c incidence rates were calculated as the incidence of thromboembolic disease in the background population divided by the corresponding person - time in took this background population . 
all calculations thromboembolic disease history into account , since men with a history of previous thromboembolism are at an increased risk for being diagnosed with prostate cancer or a subsequent thromboembolic disease.29 the 95% ci for the sirs were estimated by assuming that the observed cases had a poisson distribution using byars normal approximation.30 , 31 to take comorbidities into account before prostate cancer diagnosis , sir calculations were also strati ed by history of ischaemic heart disease ( icd10 : i20 - 25 ) , circulatory disease ( icd10 : i00 - i99 ) , and stroke ( icd10 : i6064 , g45 )  . 
the absolute risk di erences by di erent types of thromboembolic disease and prostate cancer treatment were calculated , and sensitivity analyses were done to test the assumption of intention - to - treat . 
 finally , we calculated the bias in the sirs due to using the general population rates to estimate the expected numbers of thromboembolic disease , based on the formulas by jones and swerdlow.32 statistical analyses were done with sas version 9.1.3 , and r version 2.7.2. 
 role of the funding source the funding organisations had no in uence on the design and conduct of the study , data collection , management , analysis , interpretation , and preparation , review , or approval of the manuscript . 
the corresponding author had full access to all data , and the nal responsibility to submit the manuscript for publication . results between jan 1 , 1997 , and dec 31 , 2007 , pcbase registered 76 600 men diagnosed with prostate cancer , of whom 30 642 received endocrine treatment as their primary treatment . 
speci cally , 3391 men received anti - androgen therapy ; 5340 underwent orchiectomy ; 9066 received a gnrh agonist ; and 11 646 men received gnrh agonists combined with short - term anti - androgen therapy ( table 1 )  . 
18 446 ( 602% ) of the men given endocrine treatment were aged 75 years or more , compared with 9465 ( 485% ) of those on surveillance , and 1799 ( 68% ) of those who received curative treatment . 
in the endocrine treatment group , 4298 ( 140% ) patients had a localised tumour and psa concentration less than 20 ng / ml , compared with 12 879 ( 660% ) in the surveillance group , and 18 850 ( 713% ) in the curative treatment group . 
 in the group treated with anti - androgens , 838 ( 247% ) men had localised tumours , compared with 643 ( 190% ) with locally advanced disease , and 671 ( 198% ) with metastatic disease . 
 1881 men developed a thromboembolic disease after being diagnosed with prostate cancer : 767 men had a dvt , 873 a pulmonary embolism , and 241 an arterial embolis in the total group with prostate cancer , the sir was 190 ( 95% ci 177204 ) for dvt , 185 ( 173197 ) for pulmonary embolism , and 102 ( 089115 ) for arterial embolis when analysed according to prostate cancer treatment , the risks for dvt and pulmonary embolism were increased irrespective of whether patients received endocrine treatment , were treated curatively , or were on surveillance ( table 2 )  . 
results according to prostate cancer treatment were also analysed for di erent strata of comorbidities before prostate cancer diagnosis , but there was no indication of e ect modi cation by history of any circulatory disease ( data not shown )  . detailed analysis showed that adjustment for gleason score or civil status did not alter the sirs appreciably ( data not shown ) , but di erent e ects by age and tumour stage at time of diagnosis were found . 
age - strati ed and tumour - strati ed analyses showed a larger sir for men younger than 75 years , and for those with metastatic disease , in each treatment group ( table 3 )  . 
overall , the sirs for dvt were larger for men on endocrine treatment than for men who had undergone curative treatment or men who were on surveillance , but there was not such a distinct pattern for pulmonary embolism ( table 3 )  . 
 in age - strati ed analyses for di erent types of endocrine treatment , the smallest sir for both dvt and pulmonary embolism was noted for men treated with anti - androgens , whereas the largest was seen for orchiectomy ( table 4 )  . 
the age e ect seen for the overall endocrine treatment group in table 3 was also noted for each type of endocrine treatment , although it was less strong because endocrine treatment preferences vary by agearound 20% of the men in the two younger age groups received anti - androgens , and 9% underwent orchiectomy , whereas in men aged 75 years and over a higher proportion underwent orchiectomy ( 20% ) and a lower proportion received anti - androgens ( 10% )  . 
 sensitivity analyses excluding men who had an event of thromboembolic disease within 31 days after prostate patients with prostate cancer on endocrine treatment patients with prostate cancer on curative treatment patients with prostate cancer on surveillance sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp sir ( 95% ci ) deep - venous thrombosis 248 ( 225273 ) pulmonary embolism arterial embolism 195 ( 181215 ) 100 ( 082120 ) 436 / 1756 380 / 1952 108 / 1085 173 ( 147201 ) 203 ( 179230 ) 095 ( 069127 ) 160 / 927 248 / 1221 44 / 464 127 ( 108147 ) 157 ( 138178 ) 108 ( 087133 ) obs / exp 171 / 1351 245 / 1556 89 / 821 obs = observed . 
 table 3 : standard incidence ratios ( sir ) for di erent groups of thromboembolic diseases in patients with prostate cancer according to their treatment and strati ed by age and tumour stage cancer diagnosis did not alter the previous ndings signi cantly : changes in sirs ranged between 0% and 050% ( data not shown )  . 
increased risks for thromboembolic events for all treatment groups seem to be dominated by events occurring during the rst 18 months after diagnosis , but an increased risk was still noted after more than 4 years . 
a more detailed analysis of curative treatment indicated that the risks were highest during the rst 6 months , and were higher for radical prostatectomy than for radiotherapy ( data not shown )  . 
for the general population , it can be seen that the absolute risk for dvt was higher among men aged 75 years and over than for those aged under 75 years ( table 7 ) ; by contrast , the absolute risk for dvt in men treated with endocrine 454 vol 11 may 2010 articles anti - androgens orchiectomy gnrh agonists gnrh agonists plus short - term anti - androgen therapy sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp all ages 156 ( 103227 ) 27 / 173 281 ( 226345 ) 90 / 321 242 ( 204286 ) 142 / 586 251 ( 213294 ) 154 / 613 deep - venous thrombosis < 65 years * 114 ( 021636 ) 6574 years 069 ( 027173 ) 75 years 098 ( 047207 ) pulmonary embolism < 65 years * 023 ( 003173 ) 6574 years 046 ( 016136 ) 75 years 081 ( 039167 ) 176 ( 0231351 ) 136 ( 054342 ) 181 ( 103 318 ) 065 ( 008550 ) 077 ( 025236 ) 117 ( 062218 ) 403 ( 0941732 ) 096 ( 041223 ) 149 ( 089250 ) 063 ( 010408 ) 083 ( 031220 ) 084 ( 047151 ) 232 ( 0531016 ) 138 ( 060317 ) 130 ( 076222 ) 036 ( 005242 ) 082 ( 031221 ) 098 ( 054 177 ) all ages 135 ( 091194 ) 29 / 214 226 ( 177284 ) 73 / 324 184 ( 152220 ) 118 / 641 200 ( 168236 ) 141 / 706 obs = observed . 
gnrh = gonadotropin - releasing hormone . table 4 : standard incidence ratios ( sir ) for di erent groups of thromboembolic disease by type of endocrine treatment treatment was comparable for younger and older men . 
 therefore , the absolute risk increase after exposure to endocrine treatment was larger for those in the youngest age groups ( < 65 years and 6574 years ) than those in the oldest age group . 
the pattern was similar for pulmonary embolism ( data not shown )  . finally , we calculated the possible bias in the sirs due to using general population rates to estimate expected numbers of thromboembolic disease . 
the true relative risk ( rr ) of dvt was de ned as sir ( 1prev ) / ( 1 ( prevsir ) ) , where the prevalence ( prev ) of men with prostate cancer receiving endocrine treatment was estimated to be 560 / 100 000.33 this resulted in the following bias : [ ( rrsir ) / sir ] 100 = [ ( 250248 ) / 248 ] 100 = 084% , indicating that including men with prostate cancer in the general population only resulted in a deviation of less than 1% from the so - called true sir estimates . 
the size of the bias was similar for other thromboembolic diseases and other treatment groups ( data not shown )  . discussion in this large population - based study , we compared the risk of thromboembolic disease between swedish men with prostate cancer and swedish men in the background population . 
additionally , the relative risk of thromboembolic disease in men treated with endocrine therapy was higher for younger men ( < 65 years ) and for men with metastatic disease , while the absolute risk was similar for all three age groups ( < 65 , 6574 , and 75 years )  . 
 first , a baseline risk might be present because of physiological alterations due to the tumour , which seems to be supported by the fact that the risk of thromboembolic disease increases as tumour stage increases . 
second , the di erent patterns of risk associated with di erent types of treatment indicate that treatments , and the selection of these treatments , can a ect the risk of thromboembolic disease . 
curative treatment , such as prostatectomy , and surveillance are also associated with an increased risk of thromboembolic disease , and indicate that some men might have received surveillance because of ongoing comorbidities.34 third , the higher risks , through each vol 11 may 2010 articles absolute risk for men with prostate cancer absolute risk for men in the general population absolute risk di erence ( 95% ci ) deep - venous thrombosis endocrine treatment curative treatment surveillance pulmonary embolism endocrine treatment curative treatment surveillance 408 140 189 355 217 270 164 081 149 183 107 172 244 ( 205282 ) 059 ( 037080 ) 039 ( 011068 ) 173 ( 137209 ) 110 ( 083137 ) 099 ( 065133 ) table 6 : absolute risk and absolute risk di erence for deep - venous thromboembolism and pulmonary embolism disease by prostate cancer treatment in pcbase sweden absolute risk for men with prostate cancer absolute risk for men in the general population absolute risk di erence ( 95% ci ) endocrine treatment curative treatment < 65 years 6574 years 75 years < 65 years 6574 years 75 years surveillance < 65 years 6574 years 75 years 443 405 404 123 144 284 066 066 340 072 039 258 055 061 529 062 041 277 371 ( 246 to 496 ) 366 ( 300 to 431 ) 145 ( 094 to 196 ) 067 ( 039 to 095 ) 083 ( 049 to 117 ) 245 ( 384 to 106 ) 004 ( 041 to 050 ) 025 ( 001 to 051 ) 064 ( 007 to 121 ) table 7 : absolute risk and absolute risk di erence of deep - venous thrombosis by prostate cancer treatment and age group in pcbase sweden stage of the analysis , for men primarily treated with endocrine treatment indicate a risk conferred by endocrine treatment over and above the other treatments and indications for treatment . people with cancer have an increased risk of thromboembolic disease . 
even though this association has long been recognised in clinical practice , few studies have quanti ed this risk for men with prostate cancer in detail.7 , 35 , 36 high rates of thrombosis have been reported in other cancers , especially in people with advanced disease receiving antitumour treatment . 
clinical trials on breast cancer reported a rate of thrombosis of 110% in women with node - positive breast cancer , whereas development of venous thrombosis was reported in 10% of women with advanced ovarian cancer and in up to 28% of people with malignant gliomas.36 treatment for prostate cancer can also be associated with an increased risk of thromboembolic disease . 
 a cohort study based on 5951 patients undergoing prostatectomy showed an incidence of 05% ( 95% ci symptomatic dvt and pulmonary 0407 ) embolism.35 additionally , a british study including 11 199 men with advanced prostate cancer showed that patients treated with cyproterone acetate had a signi cantly higher risk for venous thromboembolism than did men for who underwent orchiectomy or were prescribed gnrh agonists ( adjusted odds ratio 523 , 95% ci 312879 ) .7 than lower all - cause mortality we caution that the observed contrasts in thromboembolic disease between di erent treatment groups should be interpreted as how treatment and treatment selection modify the risk of thromboembolic disease in men with prostate cancer . 
for several reasons , this study cannot directly quantify how much the observed di erences in thromboembolic disease risk between treatment groups are due to the treatments themselves.1 factors taken into account during the process of selecting treatment might also be associated with risk of thromboembolic disease . 
most men receiving curative treatment were recommended surgery , and had to be healthy enough to undergo radical prostatectomy.34 we made a similar observation in our study : men 75 years or older who had undergone curative treatment had a much lower absolute risk for dvt than men of the same age in the standard population , illustrating a selection bias towards healthy men for radiotherapy and prostatectomy . 
 the increased risk of thromboembolism in the group treated with curative intent occurred mainly during the rst 6 months of follow - up , indicating that the surgical intervention was important . 
however , a selection phenomenon might lead to a wrong conclusion about the e ect of surgery in a direct comparison with the rst period of follow - up in , for example , men under surveillance.2 there might have been di erences in diagnostic activity ( frequency of check - ups and di erences in the types of testing used ) for thromboembolic disease between the groups . 
vigilance for thromboembolic disease is likely to have been similar in men with advanced cancer and those o ered curative treatment , but might have been less intense in men under surveillance . 
it is also possible that a rapidly fatal pulmonary embolism in patients with advanced cancer could be interpreted as the fatal end - stage of the cancer , and therefore not coded in hospital charts . 
however , this misclassi cation would only a ect a smaller number of patients , and mainly those on endocrine treatment , biasing their estimates towards null.3 the comparison between the treatment groups might be confounded by the introduction of second - line treatment eg , men treated with curative intent or surveillance will have been exposed to endocrine treatment when the disease progressed . 
 babiker and colleagues37 showed that the early release of 456 vol 11 may 2010 articles into suggested from prostate cancer cells prostasomes the circulation might evoke blood - clotting e ects causing thromboembolic disease . 
another study by li and colleagues16 showed a possible link between endocrine treatment and thromboembolic disease , in which they noted that the prevention of experimental arterial thrombosis by the use of androgens at physiological concentrations is mediated by the androgen receptor through modulation of platelet activation . 
some studies have also testosterone has an that antithrombotic e ect , because higher concentrations are associated with an increase in antithrombin 3.9 , 38 , 39 this possible antithrombotic e ect of testosterone is supported by our treatment - speci c analyses of endocrine treatment , which showed that men treated with anti - androgens have the lowest sir . 
because of the e ect of anti - androgens in the hypothalamus , the testosterone concentrations in serum might even be increased , and thus androgen - dependent pathways in other organs can still function.40 the higher sirs in the youngest age group ( table 3 ) can be explained by a lower absolute thromboembolic disease risk for younger men than for older men in the general population , and similar absolute risks for younger and older men with prostate cancer . 
this age e ect was seen within each tumour stage ; however , a stronger e ect was seen for those with metastatic disease at time of diagnosis , suggesting that advanced cancer potentiates the risk due to the associated predisposition for thromboembolic disease . 
 that allow for detailed the npcr database contains data from more than 76 000 men with prostate cancer , and provides complete follow - up for each patient , as well as linkage to other registers information on thromboembolic disease morbidity . 
the bias in the sirs due to the use of general population rates , which included men with prostate cancer , to estimate expected numbers of thromboembolic disease was found to be negligible . 
however , as suggested by miettinen , 41 the physician or patients choice of endocrine treatment primarily constitutes a confounder for the study of the intended e ect ( palliative treatment for prostate cancer ) , but not for the study of side - e ects such as thromboembolic disease . 
this is because at the time the data were collected , the literature did not suggest a strong association between endocrine treatment and cardio vascular side - e ects , thus it was not standard clinical practice to take thromboembolic disease history into account when initiating treatment . 
 the diagnosis of prostate cancer itself can also bias the results , because these men receive more intensive medical care ( eg , increased number of clinical visits ) , and are therefore more likely to be diagnosed with a thromboembolic disease event when it occurs . 
based on the swedish drug registry , it was shown that it takes about 1 month before men with prostate cancer start taking their endocrine treatment ( stattin p , unpublished )  . 
the e ect of delayed start of treatment was assessed with a sensitivity analysis excluding cardiovascular disease events that occurred within 1 month of the prostate cancer diagnosis , and showed almost no change in sir estimates ( data not shown )  . 
furthermore , an unknown proportion of men treated curatively , on surveillance , or on anti - androgens , subsequently changed to gnrh agonists , which could dilute a true di erence in risk between anti - androgens and gnrh agonists . 
we had no information about smoking habits , diabetes , body - mass index , or hypertension , but none of these factors are strongly associated with prostate - cancer risk , and are therefore unlikely to explain the current ndings.42 no information was available on history of comorbidities other than circulatory diseases . our ndings indicate that it is important to consider thromboembolic side - e ects when treating patients with prostate cancer , especially those who require endocrine treatment . 
risk patterns for thromboembolic disease that di er according to prostate - cancer treatment , age , and tumour stage , are probably explained by the physiological e ects of prostate cancer , treatments for prostate cancer , and the factors taken into consideration when selecting these treatments . 
all other authors declared no con icts of interest . vol 11 may 2010 articles acknowledgments funding came from the swedish research council 825 - 2008 - 5910 , stockholm cancer society , and cancer research uk . 
this project was made possible by the continuous work of the national prostate cancer register of sweden steering group : pr stattin ( chairman ) , anders widmark , lars egevad , magnus trnblom , jan adolfsson , anna bill - axelson , jan - erik johanssson , david robinson , jonas hugosson , jan - erik damber , ola bratt , gran ahlgren , and roy ehrnstrm . correction to lancet oncol 2017 ; 18 : 1493501 correction to lancet oncol 2017 ; 18 : 156566 tawbi ha , burgess m , bolejack v , et al . 
 pembrolizumab in advanced soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
this correction has been made to the online version as of dec 29 , 2017 . vol 19 january 2018 corrections correction to lancet oncol 2020 ; 21 : 26170 correction to lancet oncol 2020 ; 21 : 80820 correction to lancet oncol 2020 ; 21 : 92334 blay j - y , serrano c , heinrich mc , et al . 
quality of life in patients with cervical cancer after open versus minimally invasive radical hysterectomy ( lacc ) : a secondary outcome of a multicentre , randomised , open - label , phase 3 , noninferiority trial . 
this correction has been made to the online version as of june 29 , 2020 . vol 21 july 2020 e341 corrections acting on misinformation to prevent patient harm a group of government ministers are in discussions to call for an expansion of the remit of the uks cancer act , according to a recent report . 
the aim is to broaden the scope of the act to include the regulation of clinically unproven diagnostic procedures , to prohibit dangerous treatments , and to introduce stricter controls of social media posts about purported cancer cures . 
 lockdown following an unprecedented national intro duced across the uk in march , 2020 , as a result of the initial covid - 19 outbreak , cancer screening services were suspended , routine diagnostic work was postponed , and urgent referrals for suspected cancer declined dramatically . 
the absence of national health service ( nhs ) - based cancer diagnosis and treatment , and fears about a huge backlog of patients with cancer in the uk , have left a vacuum that those peddling unproven and unapproved tests and interventions have tried to fill . 
thus , review and revision of the cancer act to address this emerging threat to patient safety is welcome . enacted by the uk houses of parliament in 1939 , the cancer act was introduced with the aim to make further provision for the treatment of cancer , to authorise the minister of health to lend money to the national radium trust , to prohibit particular advertisements relating to cancer , and for purposes connected with the matters aforesaid . 
although the act has since been revised , the remaining provision prohibiting any advertisements that offer to treat or cure cancer remains in effect to this day , and has led to the prosecution of many individuals guilty of advertising unproven cures for cancer , including in the past decade . 
crucially , the act does not cover advertising of purported cancer diagnostic tests ( eg , thermography ) or the undertaking of such tests that , although unapproved and often debunked , have been shown to lead to false hope for those with cancer and even the tragic deaths of some patients . 
tighter regulation is , therefore , needed to prevent the dissemination of misleading claims used to market health products or tests , especially online . online advertisements , and particularly social media , are largely responsible for the the widespread visibility of unapproved cancer diagnostic tests and false cancer cures . 
individuals preying on the vulnerability of patients to sell fake medical products is an age - old problem , but the advent of social media has led to an exponential proliferation of advertising of such products online . 
with the added challenge of covid - 19 lockdowns in various countries affecting cancer care , patients with cancer and their families might be even more susceptible to advertisements that offer hope for their illness . 
in some countries , such as the usa , advertisement of genuine and clinically proven cancer treatments are permitted , which can make the regulation of unproven so - called miracle cures for cancer particularly difficult in the absence of relevant regulations . fortunately , steps are being taken to combat this rise in misinformation . 
 but the rise in misleading information in relation to the covid - 19 pandemic suggests that existing measures are not suffi cient and further efforts are needed to halt this trend . increase vigilance are , of course , to reduce , if not eliminate , the promotion of fake cancer cures , a multifaceted approach is needed . 
within an international consortium investigating the genetics of barretts oesophagus and oesophageal adenocarcinoma , we aimed to identify novel genetic risk variants for the development of barretts oesophagus and oesophageal adenocarcinoma . methods we did a meta - analysis of all genome - wide association studies of barretts oesophagus and oesophageal adenocarcinoma available in pubmed up to feb 29 , 2016 ; all patients were of european ancestry and disease was con rmed histopathologically . 
meta - analysis was done with a xed - e ects inverse variance - weighting approach and with a standard genome - wide signi cance threshold ( p < 5 10 )  . 
furthermore , the entire dataset was analysed with bioinformatics approachesincluding functional annotation databases and gene - based and pathway - based methodsto identify pathophysiologically relevant cellular mechanisms . findings our sample comprised 6167 patients with barretts oesophagus and 4112 individuals with oesophageal adenocarcinoma , in addition to 17 159 representative controls from four genome - wide association studies in europe , north america , and australia . 
we identi ed eight new risk loci associated with either barretts oesophagus or oesophageal adenocarcinoma , within or near the genes cftr ( rs17451754 ; p = 48 10 ) , msra ( rs17749155 ; p = 52 10 ) , linc00208 and blk ( rs10108511 ; p = 21 10 ) , khdrbs2 ( rs62423175 ; p = 30 10 ) , tppp and cep72 ( rs9918259 ; p = 32 10 ) , tmod1 ( rs7852462 ; p = 15 10 ) , satb2 ( rs139606545 ; p = 20 10 ) , and htr3c and abcc5 ( rs9823696 ; p = 16 10 )  . 
the locus identi ed near htr3c and abcc5 ( rs9823696 ) was associated speci cally with oesophageal adenocarcinoma ( p = 16 10 ) and was independent of barretts oesophagus development ( p = 045 )  . 
the strongest disease pathways identi ed ( p < 10 ) belonged to muscle cell di erentiation and to mesenchyme development and di erentiation . interpretation our meta - analysis of genome - wide association studies doubled the number of known risk loci for barretts oesophagus and oesophageal adenocarcinoma and revealed new insights into causes of these diseases . 
 furthermore , the speci c association between oesophageal adenocarcinoma and the locus near htr3c and abcc5 might constitute a novel genetic marker for prediction of the transition from barretts oesophagus to oesophageal adenocarcinoma . 
 barretts oesophagus and oesophageal adenocarcinoma have heritable components with substantial overlap in the set of genes contributing to risk of each condition.6 however , genetic risk factors contributing speci cally to barretts oesophagus or oesophageal adenocarcinoma alone might also exist . 
so far , genome - wide association studies have identi ed four loci within or near mhc , foxf1 , gdf7 , and tbx5 associated with the development of barretts oesophagus , 7 , 8 and four additional loci within or near crtc1 , barx1 , foxp1 , and aldh1a2 associated with development of both barretts oesophagus and oesophageal adenocarcinoma.8 , 9 however , because of small sample sizes analysed so far , these loci account for only a part of the genetic variance of barretts oesophagus and oesophageal adeno carcinoma.6 furthermore , these loci are insu cient to predict the transition from barretts oesophagus to oesophageal adenocarcinoma , because no speci c marker for oesophageal adenocarcinoma has been identi ed up to now . therefore , our international consortium aimed to do a meta - analysis of all available datasets from genome - wide for barretts oesophagus and association studies research in context evidence before this study we searched pubmed on feb 29 , 2016 , to identify genetic risk markers for barretts oesophagus and oesophageal adenocarcinoma identi ed through genome - wide association studies . 
three genome - wide association studies have been published to date and have led to the identi cation of eight genetic risk loci contributing to both barretts oesophagus and oesophageal adenocarcinoma . 
in particular , no variants have been identi ed so far that contribute solely to development of oesophageal adenocarcinoma and , thereby , might serve as markers for more e ective surveillance and intervention strategies for barretts oesophagus . added value of this study within an international consortium , we did a meta - analysis of four datasets available to date from genome - wide association studies , totalling more than 27 000 individuals . 
patients with cystic brosis show highly increased incidence of gastro - oesophageal re ux , and this re ux represents the main risk factor for barretts oesophagus and oesophageal adenocarcinoma . 
therefore , our data suggest that cystic brosis , barretts oesophagus , and oesophageal adenocarcinoma might have a common pathophysiological feature of gastro - oesophageal re ux , with cftr playing an important part in this process . 
this variant might constitute a novel marker for the prediction of transition from barretts oesophagus to oesophageal adenocarcinoma . implications of all the available evidence identi cation of novel risk loci and cellular pathways provides further insights into the causes of barretts oesophagus and oesophageal adenocarcinoma and impetus for further functional studies . 
together , this information should lead to better molecular treatments and individualised prevention and intervention strategies for clinical management of barretts oesophagus and oesophageal adenocarcinoma . vol 17 october 2016 to oesophageal adenocarcinoma identify additional genetic variants associated with risk for both disorders . 
 furthermore , we aimed to identify genetic variants that contribute speci cally to risk for oesophageal adenocarcinoma and , thereby , might serve as markers for individualised surveillance and intervention strategies for barretts oesophagus . 
to our knowledge , our study is the rst in which datasets from genome - wide association studies have been analysed using bioinformatics approaches to gain further information about the underlying genes and cellular pathways associated with barretts oesophagus and oesophageal adenocarcinoma . 
 methods study design and participants we obtained genome - wide genotype data for patients with barretts oesophagus , individuals with oesophageal adenocarcinoma , and representative controls from four genome - wide association studies in europe , north america , and australia : 79 the barretts and esophageal adenocarcinoma consortium ( beacon ) study ; and studies from bonn , cambridge , and oxford ( appendix pp 56 , 11 )  . 
all participants were of european ancestry , and dna samples extracted from blood or saliva were genotyped on high - density single nucleotide polymorphism ( illumina , san diego , ca , usa )  . 
we removed all individuals with more than 3% of missing genotypes ; snps with a successful genotyping rate of less than 97% ; snps with a minor allele frequency less than 001 ; snps with a p value of less than 00001 in controls and less than 5 10 in patients for hardy - weinberg equilibrium ; and snps with a signi cant ( p < 0001 ) di erence in missingness between cases and controls . 
based on identity by descent calculated from autosomal markers , we removed one of each pair of individuals with high levels of relatedness ( p - hat > 02 ) and a higher proportion of missing genotypes . 
we also removed participants who lay beyond six sds from the mean of the rst two genotypic principal components of the 1000 genomes european descent population.11 vol 17 october 2016 for the imputation , we used shapeit version 2.1212 for phasing of the genotyped snps and impute2 version 2.3.113 , 14 for imputation of missing snps , using the 1000 genomes phase 1 haplotypes ( june , 2014 release ) as a reference panel.15 we did the imputation in 5 mb sections . 
we set a 250 kb bu er anking the imputation sections and an e ective size of the sampled population of 20 000 , as recommended for impute2 version 2.3.1.13 , 14 statistical analysis we did association testing for barretts oesophagus and oesophageal adenocarcinoma as separate disorders . 
we assessed associations in snptest version 2.5.2 , 16 adjusted for sex and study - speci c top principal components , under an additive genetic model using dosage scores ( based on the probabilities for each of the three possible genotypes of every snp ) obtained from the imputation . 
dosage scores account for imputation uncertainty in the association analysis , by contrast with the best - guess approach , whereby the most probable genotype of every snp obtained from imputation is regarded as the actual genotype for that snp . 
a high in ation factor might indicate presence of population strati cation , unknown familial relationships , undetected sample duplications , technical problems with the data , or application of incorrect statistical methods . we analysed snps that passed the post - imputation quality control assessment in every study ( imputation quality score > 04 , minor allele frequency > 0001 ) and were present in at least three studies of barretts oesophagus and two studies of oesophageal adenocarcinoma . 
an imputation quality score greater than 04 ensures that snps that were not well imputed were excluded , and a minor allele frequency greater than 0001 ensures that snps that were not common in our study population were excluded from the analysis ( appendix pp 56 )  . 
we did the meta - analysis with the xed - e ects inverse variance - weighting approach in metal version 2011 - 03 - 25 , 17 with a standard genomewide signi cant threshold of 5 10 . we investigated the presence of genetic heterogeneity between studies with the i statistic , and we calculated p values for heterogeneity with cochrans q test , as implemented in metal version 2011 - 03 - 25.17 presence of genetic heterogeneity indicates that e ect sizes are not similar between studies , emphasising the possibility of a distribution of true e ect sizes between studies . 
 investigate whether independent associations exist in regions of genome - wide signi cance , we did association analyses conditioned on the strongest associated snp in every region ( 1 mb either side of the top snps ) with meta - analysis summary statistics and the approach implemented in gcta version 1.25.2.19 this approach uses both summary - level statistics from genome - wide association studies and estimated linkage disequilibrium from a reference sample ( the imputed beacon data in this study ) to investigate whether single or multiple independent associations exist for every locus . 
 because some snps could be associated with barretts oesophagus and oesophageal adenocarcinoma but not meet the genome - wide signi cance threshold because of insu cient statistical power ( ie , snps with small e ect sizes cannot be detected in our current sample size using stringent criteria for signi cance ) , we used a new approach20 in which functional annotation loci is information from genome - wide signi cant used to reweight the results . 
incorporating functional annotation information to reweight data from genomewide association studies could result in identi cation of new risk loci that otherwise might not reach the genome - wide signi cance threshold in standard genome - wide association studies . 
this approach , which is implemented in fgwas version 1.0 , 20 is capable of identifying additional high - con dence risk loci , resulting in a roughly 5% increase in the number of identi ed loci when tested on previously published data from genome - wide association studies.20 we looked at enrichment of 450 genomic annotations as implemented in fgwas version 1.020 ( default settings : 5000 snps per window )  . 
some annotations were correlated and , hence , we built a model by adding terms sequentially in decreasing order of signi cance until no more annotations signi cantly ( p < 005 ) improved the log - likelihood of the model . 
a posterior probability greater this approach performed similarly to the genome - wide signi cance threshold in genome - wide association studies ( p < 5 10 ) based on the analysis20 of previously published genome - wide association studies.20 than 09 we did gene - based association tests with the approach implemented in vegas version 2 , 21 a simulation - based approach that combines the test statistics for single variants within gene boundaries while accounting for linkage disequilibrium between markers . 
we set the bonferroni - corrected threshold for gene - wide signicance to a p value of less than 28 10 ( considering 17 787 autosomal genes used in vegas version 2 )  . we analysed pathways and tissue enrichment with methods implemented in depict version 1.1.22 the preference is to use genome - wide signi cant snps as long as at least ten independent loci are available . 
this omission is because many snps that do not meet the genome - wide signi cance threshold might still be associated with either barretts oesophagus or oesophageal adenocarcinoma ( or both ) , but might not be detected because of insu cient statistical power . 
 accordingly , we included loci from the combined barretts oesophagus and oesophageal adenocarcinoma meta - analysis that achieved one of three p value thresholds ( p < 5 10 , p < 10 , and p < 10 ) for pathways analysis . 
we set the bonferroni - corrected threshold for pathways analysis at a p value of less than 115 10 ( considering multiple testing with the three p - value thresholds and assuming all 14 463 pathways used in depict version 1.1 are independent ) and a false discovery rate of less than 005 . 
similarly , we set the bonferronicorrected threshold for tissue - enrichment analysis to a p value of less than 8 10 ( considering multiple testing with the three p - value thresholds and assuming that gene expression in all 209 tissue and cell samples used in depict version 1.1 is independent ) and a false discovery rate less than 005 . 
we investigated whether published risk loci for gastro - oesophageal re ux - predisposing traits ( eg , body - mass index [ bmi ] and obesity ) , which have shown genome - wide signi cant associations , 23 represent risk loci for barretts oesophagus and oesophageal adeno carcinoma . 
we also estimated the peak snps identi ed in this study in the genome - wide association analysis for bmi undertaken by the genetic investigation of anthropometric traits ( giant ) consortium.24 additional details of methods used for functional annotation enrichment analysis , gene - based analysis , and tissue enrichment analysis are in the appendix ( p 7 )  . role of the funding source the funders had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
new risk variants at genome - wide signi cance level ( p < 5 10 )  . table : top snps from loci meeting the threshold for genome - wide signi cance in the combined barretts oesophagus and oesophageal adenocarcinoma meta - analysis results 6167 people with barretts oesophagus , 4112 individuals with oesophageal adenocarcinoma , and 17 159 representative controls from four genome - wide association studies in europe , north america , and australia were included in the meta - analysis . 
in total , 11 942 825 snps for barretts oesophagus , 13 074 274 for oesophageal adenocarcinoma , and 11 951 684 for both barretts oesophagus and oesophageal adenocarcinoma were used for the meta - analysis of genome - wide association studies . 
q - q and manhattan plots from the separate barretts oesophagus and oesophageal adenocarcinoma meta - analyses , and the combined barretts oesophagus and oesophageal adenocarcinoma metaanalysis , are shown in the appendix ( pp 89 )  . 
the scaled genomic in ation factor lambda ( ) was 1043 for the barretts oesophagus meta - analysis , 1005 for the oesophageal adenocarcinoma meta - analysis , and 1049 for the combined barretts oesophagus and oesophageal adenocarcinoma meta - analysis . 
 from five genome - wide signi cant associated loci ( p < 5 10 ) were identi ed for barretts oesophagus alone , of which three were not previously reported ( appendix p 11 )  . 
 moreover , ve genome - wide signi cant associated loci ( p < 5 10 ) for oesophageal adeno carcinoma alone were identi ed , of which four were previously unreported ( appendix p 12 )  . 
the combined meta - analysis for barretts oesophagus and oesophageal adenocarcinoma identi ed 14 genome - wide signi cant associated loci ( p < 5 10 ) , of which seven were previously unreported ( table )  . 
of note , loci from all seven new genome - wide signi cant the separate barretts oesophagus and oesophageal adenocarcinoma meta - analyses were also identi ed in the combined meta - analysis except locus on chromosome 3q27 near htr3c and abcc5 ( rs9823696 ) that was only recorded in the oesophageal adenocarcinoma for one meta - analysis and , therefore , was speci c for this disorder ( risk for oesophageal adenocarcinoma : odds ratio [ or ] 117 , 95% ci 111124 ; p = 164 10 ; risk for barretts oesophagus : 102 , 097106 ; p = 045 )  . 
the most strongly associated snps were rs17451754 on chromosome 7q31 within cftr ( p = 477 10 ; gure 1a ) , rs17749155 on chromosome 8p23 within msra ( p = 521 10 ; gure 1b ) , rs10108511 on chromosome 8p23 within linc00208 and blk ( p = 212 10 ; gure 1c ) , rs62423175 on chromosome 6q11 near khdrbs2 and mtrnr2l9 ( p = 295 10 ; gure 1d ) , rs9918259 on chromosome 5p15 within tppp and cep72 ( p = 323 10 ; gure 1e ) , rs7852462 on chromosome 9q22 within tmod1 ( p = 149 10 ; gure 1f ) , and rs139606545 on chromosome 2q33 near satb2 ( p = 202 10 ; gure 1g )  . 
although rs12207195 did not reach genome - wide signi cance in the frequentist analysis ( p = 21 10 ) , the posterior probability for the region containing lpa was 0925 in the empirical bayesian approach ( compared with 0863 without weighting by annotation ; appendix p 7 ) , corresponding to p < 5 10 in the frequentist inference . 
the appendix ( p 13 ) shows the association results of the top associated snps from the combined meta - analysis in the separate barretts oesophagus and oesophageal adenocarcinoma analyses . 
 figure 2 shows regional association results for the oesophageal adenocarcinoma - speci c locus near in oesophageal htr3c and abcc5 ( rs9823696 ) vol 17 october 2016 1367 articles figure 1 : regional plots for loci meeting the threshold for genome - wide signi cance in both barretts oesophagus and oesophageal adenocarcinoma regional associations for the most signi cantly associated single nucleotide polymorphisms ( snps ; marked as solid purple diamonds ) in the combined barretts oesophagus and oesophageal adenocarcinoma meta - analysis ( includes 10 279 patients with barretts oesophagus and oesophageal adenocarcinoma and 17 159 controls )  . 
although we did not identify any secondary peaks ( ie , associations of snps with oesophageal adenocarcinoma and barretts oesophagus that were independent of the top hits ) at genome - wide signi cance in the conditional association loci analysis of ( rs34817486 near foxf1 - as1 [ also known as fendrr ] and foxf1 , and rs62331139 near lpcat1 and slc6a3 ) showed some evidence of secondary peaks ( p < 10 ; appendix p 10 )  . the combined meta - analysis , two of the nine newly identi ed risk loci , only snps within or near tppp and cep72 showed signi cant ( p < 005 ) heterogeneity for the magnitudes of association of snps between studies in the xed - e ects meta - analysis ( heterogeneity i = 645 and p = 00375 for rs9918259 , the most signi cantly associated snp at this locus ; table )  . 
however , the magnitude of association was larger in the bonn study compared with the other studiesie , the bonn study or was 143 ( 95% ci 125164 ) for the risk allele of rs9918259 , whereas it was 118 ( 108129 ) in the beacon study , 111 ( 098249 ) in the cambridge study , and 112 ( 099128 ) in the oxford study . 
 under a random - e ects model , the snp rs9918259 was less signi cantly associated with barretts oesophagus and oesophageal adenocarcinoma in the combined meta - analysis ( p = 47 10 ) than with the xed e ects meta - analysis ( p = 32 10 )  . 
consistent with p values for heterogeneity for the other risk loci ( table ) , the magnitude and direction of e ect were consistent between all studies for the remaining risk loci . 
thus , we did not do a random - e ects meta - analysis for these loci . all previously reported genome - wide signi cant loci79including gdf7 , aldh1a2 , tbx5 , crtc1 , foxp1 , foxf1 , and the mhc region ( table ) were also associated with both barretts oesophagus and the genome - wide oesophageal adenocarcinoma at signi cance threshold . 
only the barx1 locus9 did not meet the genome - wide signi cance threshold , but it still showed strong association with barretts oesophagus and oesophageal adenocarcinoma in the combined meta - analysis ( p = 62 10 for rs11789015 )  . 
apart from the risk loci identi ed in the single variant analysis , we did not loci reaching gene - based genome - wide signi cance ( p < 28 10 ) after correction for genomic in ation in the gene - based association analysis ( appendix p 7 )  . 
 identify other the pathway analyses , no pathways were signi cantly associated with barretts oesophagus and oesophageal adenocarcinoma at the thresholds p < 115 10 and false discovery rate < 005 using snps satisfying p < 5 10 and p < 10 in the combined meta - analysis . 
however , for snps satisfying p < 1 10 in the combined meta - analysis , four pathways were signi cantly associated with barretts oesophagus and oesophageal adenocarcinoma ( appendix p 14 ) : negative klhl24 map6d1 abcc5 htr3e ap2m1 ece2 clcn2 yeats2 parl abcc5as1 eif2b5 vwa5b2 eif4g1 htr3d dvl3 mir1224 fam131a htr3c abcf3 psmd2 chrd alg3 polr2h camk2n2 thpo snord66 klhl24 map6d1 abcc5 htr3e ap2m1 ece2 clcn2 yeats2 parl abcc5as1 eif2b5 vwa5b2 eif4g1 htr3d dvl3 mir1224 fam131a htr3c abcf3 psmd2 chrd alg3 polr2h camk2n2 thpo snord66 1834 1836 1838 position on chromosome 3 ( mb ) 1840 figure 2 : regional plots for the oesophageal adenocarcinoma - speci c locus rs9823696 near htr3c and abcc5 regional associations for the most signi cantly associated single nucleotide polymorphism ( snp ; marked as a solid purple diamond ) , rs9823696 , in the oesophageal adenocarcinoma meta - analysis . 
 regulation of muscle - cell di erentiation ( go : 0051148 ) ; mesenchyme development ( go : 0060485 ) ; bmpr2 ppi subnetwork ( ensg00000204217 ) ; and mesenchymal cell di erentiation ( go : 0048762 )  . 
in tissue enrichment analyses , genes within the combined barretts oesophagus and vol 17 october 2016 1369 articles oesophageal adenocarcinoma associated regions were highly expressed in the digestive system , as well as in the endocrine system , cardiovascular system , and in smooth muscle ( appendix pp 7 , 15 )  . 
 none of the published genome - wide signi cant risk loci for bmi and obesity were associated with barretts oesophagus and oesophageal adenocarcinoma in the combined meta - analysis at the genome - wide signi cance level ( data not shown )  . 
however , rs2898290 ( within linc00208 and blk ) , which is strongly associated with barretts oesophagus and oesophageal adenocarcinoma ( p = 12 10 ) , showed some evidence of association with bmi in the giant study24 ( p = 0001058 )  . the nine newly identi ed barretts oesophagus and oesophageal adenocarcinoma risk loci were characterised by analysis of multiple functional annotation databases ( appendix pp 1618 )  . 
furthermore , some of the identi ed risk variantsor variants that are highly correlated with them ( r > 080 ) represent expression quantitative trait loci that regulate the expression of genes within the regions . 
 moreover , several of the implicated risk variants change sequence motifs for protein binding sites and are located within dnaase hypersensitivity regions and within regions with enhancer or promoter motifs . discussion our meta - analysis identi ed 16 independent risk loci for development of barretts oesophagus , oesophageal adenocarcinoma , or both , at the level of genome - wide signi cance . 
thus , our study has more than doubled the number of known risk loci for barretts oesophagus and oesophageal adenocarcinoma , which further exempli es the scienti c value of meta - analysis of genome - wide association studies through international collaborations . 
 the newly findings of the functional annotation database analysis identi ed barretts oesophagus and oesophageal adenocarcinoma risk loci exemplify how data from genome - wide association studies can uncover new causal and clinical aspects of barretts oesophagus and oesophageal adenocarcinoma ( appendix pp 1819 )  . 
this snp is located within intron 21 of the cftr gene and a ects a region marked by enhancer histone modi cations in the gastrointestinal tract mucosa and by dnase hypersensitivity.25 cftr encodes an atp - binding cassette membrane protein that functions as a chloride channel and is mutated in cystic brosis , 26 the most common autosomal recessive disorder among people of european ancestry . 
up to 81% of patients with cystic brosis have gastro - oesophageal re ux , a major risk factor for barretts oesophagus and oesophageal adenocarcinoma , and more than 50% of these individuals are treated with proton - pump in high - income countries.27 according to ndings of a 20 - year nationwide survey from the usa , 28 incidence of cancer at the gastrooesophageal junction is also increased among patients with cystic brosis , with evidence of barretts oesophagus in these patients . 
although the cause of gastro - oesophageal re ux seems to di er between most patients with and without cystic brosis , the exact mechanism of re ux in patients with cystic brosis is still not understood fully . 
favoured pathophysiological ideas about gastrooesophageal re ux in patients with cystic brosis include lower inspiratory intrathoracic pressure with altered gastro - oesophageal pressure gradients , 29 delayed gastric emptying , 30 and impaired neutralisation of re ux - acidi ed oesophageal mucosa because of reduced bicarbonate secretion or hyperacidity of re uxed gastric contents.31 however , the phenotypic overlap for gastro - oesophageal re ux and cystic brosis , and for gastro - oesophageal re ux and both barretts oesophagus and oesophageal adeno carcinoma , combined with the identi cation of cftr risk variants in patients with barretts oesophagus and oesophageal adenocarcinoma , it seems plausible that a common pathophysiological mechanism for gastro - oesophageal re ux is triggered by cftr . 
fine mapping of all genetic variation at this locus , and extensive functional studies , are needed to test this hypothesis because other pathomechanisms and risk genes cannot be excluded entirely . 
moreover , detailed genotypephenotype studies of barretts oesophagus and oeso phageal adenocarcinoma , and of isolated patients with gastro - oesophageal re ux strati ed for the cftr risk variant , are needed that take the implicated mechanisms of gastro - oesophageal re ux in cystic brosis into account . 
this work might yield new insights in the area of barretts oesophagus and oesophageal adenocarcinoma research . in view of to our knowledge , the rst risk locus to be identi ed that is speci c to oesophageal adenocarcinoma is rs9823696 on chromosome 3q27 . 
highly correlated variants of this marker ( r > 080 ) have been identi ed as regulatory active expression quantitative trait loci that a ect expression of the abcc5 gene at this locus.32 however , these regulatory e ects were studied in blood cells32 and , thus , further work needs to be done to nd out if these expression quantitative trait loci are also present in tissues relevant to oesophageal adenocarcinoma . 
the corresponding gene product belongs to the group of atp - binding cassette membrane proteins that play a part in energy - dependent transport of various endogenous and exo genous substrates and has been implicated in cancer development and progression.33 , 34 furthermore , as with other oesophageal adenocarcinoma genes implicated by genome - wide association studies ( eg , foxf1 and foxp1 ) , 7 , 9 abcc5 has a role during embryonal develop ment of the intestine.35 apart from the exact functional role of rs9823696 , markers that contribute solely to oesophageal adenocarcinoma development could serve as predictors for disease progression in barretts oesophagus . 
because barretts oesophagus is common in the population and only a few patients develop oesophageal adenocarcinoma , speci c markers for the transition of barretts oesophagus to oesophageal adeno carcinoma are needed . 
the risk locus near htr3c and abcc5 alone accounts for only a fraction of the phenotypic variance ; the or is 117 between patients with oesophageal adenocarcinoma and controls , and 102 between individuals with barretts oesophagus and controls . 
however , identi cation of further oesophageal adenocarcinoma - speci c markers with larger samples of patients with barretts oesophagus and oesophageal adenocarcinoma , together with incorporation of relevant environmental and clinical data ( eg , length of barretts oesophagus segments , presence of low - grade dysplasia ) , and application of modern polygenic score approaches will help to identify patients with barretts oesophagus at higher risk for oesophageal adenocarcinoma . 
development of such risk - prediction methods would be an important advance in clinical management , because this information could be used for more e ective and individualised surveillance and intervention strategies . 
since genetic data can be used for risk prediction at very early stages ( eg , before development of barretts oesophagus ) , risk pro ling approaches should also focus on markers that contribute solely to development of barretts oesophagus and are independent of the cause of gastro - oesophageal re ux . pathways analyses showed that cellular processes related to muscle - cell di erentiation and mesenchyme development and cell di erentiation are associated with development of barretts oesophagus and oesophageal adenocarcinoma . 
involvement of the muscle - cell differentiation pathway is especially interesting because to cellular this pathway might represent a link mechanisms in the development of hiatal hernias , which have been associated with gastro - oesophageal re ux and barretts oesophagus.36 , 37 in particular , in the most common type 1 hernia , the muscles of the oesophageal hiatus are absent or reduced to a few atrophic strands.38 thus , muscle - cell di erentiation pathways could have a role in formation of hiatal hernia , which in turn might increase the risk for gastro - oesophageal re ux and barretts oesophagus and oesophageal adenocarcinoma . 
 by contrast , both mesenchyme - related pathways imply that the epithelial - mesenchymal transition plays a part in development of barretts oesophagus and oesophageal adenocarcinoma , which is characterised by loss of cell adhesion and increased cell migration and invasion . 
 the epithelial - mesenchymal transition represents an essential step in invasion and metastasis of human cancers , particularly in early oesophageal adenocarcinoma originating from barretts oesophagus.39 however , methods used in pathways analyses can di er between studies , and results are not necessarily consistent . 
thus , although the top pathways in this study are supported by the current pathophysiological ideas about barretts oesophagus and oesophageal adenocarcinoma , further pathways analyses and functional studies could con rm the involvement of these pathways in development of barretts oesophagus and oesophageal adenocarcinoma . 
this nding points to a so - called winners curse e ect ( ie , the phenomenon in which the e ect size of a newly identi ed genetic association is overestimated because of the insu cient statistical power of the original study ) in the bonn study rather than to systematic di erences between studies , because heterogeneity was only noted at this locus . our study has several limitations . 
although we have provided bioinformatics evidence for the functional relevance of our ndings , we do not provide in - vitro or in - vivo evidence for the biological function of these ndings . 
although most controls were probably not a ected by barretts oesophagus , inclusion of individuals screened for the absence of barretts oesophagus would have increased our power to detect further risk loci for barretts oesophagus and oesophageal adenocarcinoma . 
such data would have enabled us to identify risk variants that are predictive for the transition from gastro - oesophageal re ux to vol 17 october 2016 1371 articles barretts oesophagus . 
although we have used the largest available sample of genome - wide association study data analysed so far from individuals with barretts oesophagus and oesophageal adenocarcinoma , further data from additional patients would have led to identi cation of more risk loci . in conclusion , our meta - analysis identi ed nine new risk loci for barretts oesophagus and oesophageal adenocarcinoma and highlighted genes and cellular pathways likely to be implicated in disease development . 
although the strength of genomewide association study meta - analyses is identi cation of loci , ne - mapping and functional studies disease of new risk loci are now needed to reveal the disease pathophysiology . 
this next steptogether with identi cation of additional risk loci using larger sample sizes through international collaborative e ortsshould lead to identi cation of key molecules that have an important role in development of barretts oesophagus and oesophageal adenocarcinoma , which should nally pave the way for new molecular targets for development of advanced prevention and intervention strategies . 
genotyping of these controls were done through the university of texas md anderson cancer center ( utmdacc ) and the johns hopkins university center for inherited disease research ( cidr )  . 
this work , in part , used data from the national institute of neurological disorders and stroke ( ninds ) dbgap database from the cidr : neurogenetics research consortium parkinsons disease study . 
this report was not prepared in collaboration with investigators of the cric study and does not necessarily re ect the opinions or views of the cric study , the niddk central repositories , or the niddk . 
we acknowledge the principal investigators and the project o cer of this study : harold i feldman , raymond r townsend , lawrence j appel , mahboob rahman , akinlolu ojo , james p lash , jiang he , alan s go , and john w kusek . 
 de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
only reproduce with permission from the lancet publishing group . correction to lancet oncol 2020 ; 21 : e57588 correction to lancet oncol 2021 ; 22 : 2942 correction to lancet oncol 2021 ; 22 : 8597 bahadoer rr , dijkstra ea , van etten b , et al . 
short - course radiotherapy followed by chemotherapy before total mesorectal excision ( tme ) versus preoperative chemoradiotherapy , tme , and optional adjuvant chemotherapy locally advanced rectal cancer ( rapido ) : a randomised , open - label , phase 3 trial . 
 lancet oncol 2021 ; 22 : 2942in figure 1 in this article , in the standard of care group , of the 187 patients who had adjuvant chemotherapy , 185 should have been indicated as having this chemotherapy according to hospital policy . 
fixeddose combination of pertuzumab and trastuzumab for subcutaneous injection plus chemotherapy in her2 - positive early breast cancer ( federica ) : a randomised , open - label , multicentre , non - inferiority , phase 3 study . 
lancet oncol 2021 ; 22 : 8597in table 2 of this article , the cycle 7 ( predose cycle 8 ) pertuzumab serum geometric mean auc 021 days ( percentage cv ) , g / ml per day should have been 2440 ( 242 ) for the intravenous infusion group and 2440 ( 262 ) for the fixed - dose combination group , and the cycle 7 ( predose cycle 8 ) trastuzumab serum geometric mean ( percentage cv ) , auc 021 days g / ml per day should have been 1640 ( 240 ) for the intravenous infusion group and 1700 ( 289 ) for the fixed - dose combination group . 
intermittent schedules of the oral rafmek inhibitor ch5126766 / vs - 6766 in patients with ras / raf - mutant solid tumours and multiple myeloma : a single - centre , open - label , phase 1 dose - escalation and basket dose - expansion study . 
also , sentence two of paragraph four of the discussion should have read these tumours harboured a range of ras and raf mutations , including kras gly12asp , kras gly12val , kras gly12arg , brafve , and hras gly13arg . 
 vol 22 february 2021 corrections corrections correction to lancet oncol 2014 ; 15 : 856 correction to lancet oncol 2015 ; 16 : 60 , 61 ledermann j , harter p , gourley c , et al . 
lancet oncol 2014 ; 15 : 85261 in this article , the second sentence of the rst paragraph of the results section should read on the basis local germline brca mutation testing reported on case report forms , germline brca mutation status was known for 98 ( 37% ) of 265 patients ( 50 [ 37% ] of 136 in the olaparib group vs 48 [ 37% ] of 129 in the placebo group )  . 
this correction has been made to the online version as of march 30 , 2015 . a multi - centre , topp ms , gckbuget n , stein as , et al . 
lancet oncol 2015 ; 16 : 5766in table 2 of this article , the mrd response during rst two cycles in patients with cr or crh row should not have been indented , and should have been the last row in the table . 
these corrections have been made to the online version as of march 30 , 2015 . after vol 16 april 2015 e158 interest of a new indication , convincing evidence might arrive late , when the drug patent has already expired . 
generic drugs ( or biosimilars ) might become newly available and the price of the originator rapidly falls ; therefore , in starting a pharmaceutical companies registration process at ema declines , or disappears altogether . 
the story of bisphosphonates as adjuvant treatment for early breast cancer roughly corresponds to this profile : convincing evidence coming mostly from academic studies , including the previously mentioned meta - analysis , arriving late to their goal , and also because of the good prognosis of the disease . academic groups have a important role in identifying treatment strategies that ultimately improve prognosis of patients.8 however , the results of academic trials might not translate into clinical practice , including in europe where country - level discussion about reimbursement for new drugs starts only after ema approval on request of pharmaceutical companies . 
 ema does allow for academic groups to act as medicine developers ; however , we suspect that either no or very few cancer drugs have been approved based on a request from the academic community . 
this situation is due to academic researchers leaving the agenda of registration trials to the pharmaceutical industry and not continuing to remain engaged through to the end of the drug development process . 
solving discrepancies between scientific recommendations and regulatory approval ( eg , in the case of bisphosphonates in early breast cancer ) should be a mission of academic researchers who contributed to developing scientific evidence . * francesco perrone , adriano gravina clinical trial unit , istituto nazionale per lo studio e la cura dei tumori irccs fondazione g pascale , naples 80131 , italy f.perrone@istitutotumori.na.it fp reports personal fees from bayer , janssen cilag , pierre fabre , astrazeneca , celgene , incyte , sandoz , bristol - myers squibb , ipsen , and eli lilly , outside of the submitted work . 
adjuvant denosumab in postmenopausal patients with hormone receptor - positive breast cancer ( abcsg - 18 ) : disease - free survival results from a randomised , double - blind , placebo - controlled , phase 3 trial . 
zoledronic acid combined with adjuvant endocrine therapy of tamoxifen versus anastrozol plus ovarian function suppression in premenopausal early breast cancer : final analysis of the austrian breast and colorectal cancer study group trial 12 . 
 j law med ethics 2019 ; 47 : 46567 . earlier diagnosis : the importance of cancer symptoms people diagnosed earlier with cancer are not only more likely to survive , but importantly also to have better experiences of care , lower treatment morbidity , and improved quality of life compared with those diagnosed late.1 efforts to improve earlier diagnosis of cancer are complex and multifaceted and have been at the forefront of international policy and charity ( eg , cancer research uk ) initiatives . 
these are attending cancer screening , which aims to detect cancer before it is symptomatic ( eg , mammography for breast cancer ) and presenting promptly to primary care with potential cancer symptoms . published online november 5 , 2019 s1470 - 2045 ( 19 ) 30658 - 8 see articles page 73 for be clear on cancer see on - cancer the fact that , in england , more than 90% of cancers are detected outside the three national screening programmes2 ( for cervical , breast , and bowel cancers ) highlights the importance of presenting promptly to primary care with potential cancer symptoms . 
in england , these campaigns come under the umbrella of be clear on cancer ; however , they are emulated across the world , including more recently in low - income and middle - income countries such as india , malaysia , and south africa . 
one challenge , which so far has remained largely unanswered , is whether these campaigns truly capture people with early - stage disease and thus provide a meaningful contribution to the early diagnosis effort . 
accumulating evidence vol 21 january 2020 comment shows that they increase public awareness , and the likelihood of visiting a doctor , being referred for investigations , and being diagnosed at an earlier stage of the disease.3 , 4 however , others have argued that the cancers detected are mainly advanced , 5 which would make awareness campaigns less worthy of the attention and investment they draw . in nearly 8000 patients and in their article in the lancet oncology , monica koo and colleagues6 present novel epidemiological evidence that tackles this issue head on . 
the data showed that the proportion of patients diagnosed with advanced disease ( ie , stage iv ) varied substantially by presenting sympto for example , a neck lump was associated with greater odds of advanced disease , while symptoms including abnormal mole , breast lump , post - menopausal bleeding , and rectal bleeding ( common symptoms that have already featured in public awareness campaigns ) were associated with lower odds of advanced disease . 
these findings provide support for the emphasis on factors that are important pre - presentation ( eg , knowledge of warning signs ) because understanding and responding to cancer symptoms can help to identify cancer before it has spread . koo and colleagues contribution is an essential jigsaw piece in the early diagnosis puzzle , although several questions remafor example , what symptoms should be featured ? who should the campaigns be targeted at ? what barriers ( other than poor knowledge of warning signs ) should they address ? how should the campaigns be evaluated ? it is also crucial to ensure campaigns do not serve to escalate persistent inequalities in cancer survival , 7 so understanding how barriers vary by sociodemographic characteristics including age , socioeconomic status , and ethnicity will be key . 
behavioural science has much to add here , in terms of identifying important barriers to symptomatic presentation such as worry about wasting a doctors time , fatalism , and fear , as well as designing appropriately tailored interventions or campaigns to address these barriers.8 in the readiness to their findings also have important implications for referral health - care professionals because prompt and investigation of potential cancer symptoms post - presentation is another step in ensuring timely diagnosis . 
research shows that international variation exists investigate or refer to secondary care for suspected cancer symptoms , and countries where health - care professionals demonstrate greater readiness observe the highest cancer survival rates.9 finallya message for policy makersadvocating more people going to the doctor , more referrals , and more investigations means it is imperative that health - care systems have a well equipped and well funded workforce to deal with this core and essential activity . although answers to many of these challenges will require an ongoing multidisciplinary and international effort , early diagnosis is likely to remain the holy grail of cancer care . 
with this in mind , it is reassuring and bolstering to see that global approaches to cancer control are on the right track . katriina whitaker school of health sciences , university of surrey , guildford , gu27xh , uk k.whitaker@surrey.ac.uk i declare no competing interests . copyright 2019 the author ( s )  . 
bmj 2018 ; 360 : k764 . vol 21 january 2020 comment m published online december 11 , 2019 s1470 - 2045 ( 19 ) 30715 - 6 see articles page 80 8 moriarty y , townson j , quinn - scoggins h , et al . 
improving cancer symptom awareness and help - seeking among adults living in socioeconomically deprived communities in the uk using a facilitated health check : a protocol for the awareness and beliefs about cancer ( abacus ) randomised control trial . 
bmj open 2015 ; 5 : e007212 . the role of self - management in cancer survivorship care is now earlier diagnosis of many cancers as well as more effective treatments are substantial contributors to increasing cancer survival . 
in 2016 in the usa alone , there were an estimated 155 million cancer survivors , with this number expected to increase to 203 million by 2026.1 cancer largely recognised as a chronic condition , and survivors continue to experience myriad symptoms , as well as late effects , well beyond the end of their cancer treatment . 
the challenges of delivering survivorship care through already overburdened health systems have increased our focus on research examining the acceptability , cost , and effectiveness of alternative models of follow - up care , such as follow - up care jointly provided with the patients general practitioner , with evidence of their effectiveness as well as acceptability to patients.2 another area gaining substantial research attention is self - management , in particular , equipping survivors with the skills and knowledge to manage the myriad cancer - related and treatment - related consequences.3 , 4 the paper by anja van der hout and colleagues in the lancet oncology5 reports the results of a randomised controlled trial evaluating the efficacy , reach , and usage of a fully automated self - management intervention oncokompas . 
although the key finding of the study was that oncokompas was not effective in improving the level of knowledge , skills , and confidence for self - management among cancer survivors ( difference in patient activation measure at 6 months 17 [ 95% ci 08 to 42 ] , p = 041 ) , this is possibly the largest randomised controlled trial ( n = 625 cancer survivors ) of self - management interventions reported in the literature to date and hence , contributes to that evidence base in a meaningful way . 
unlike previous studies , most of which focused on women with breast cancer , 3 the study by van der hout and colleagues5 included a range of survivors with prevalent and less prevalent solid and non - solid tumour types ( head and neck cancer , colorectal cancer , breast cancer , hodgkin lymphoma , and non - hodgkin lymphoma )  . 
this study therefore contributes substantial new knowledge on the reach and usage of self - management by a broader population of cancer survivors . supporting survivors to self - manage their symptoms and quality of life requires an understanding of the optimal timing for delivery of self - management interventions . 
self - management resources provided early in the cancer pathway might be more beneficial , longer - term survivors will probably have as many already found the information and support they need to build their skills and confidence to manage cancerrelated concerns . 
in the study in the lancet oncology , 5 only approximately half ( 167 [ 52% ] of 320 ) of the intervention group used the self - management platform at least once during the 6 - month follow - up period , and this group had a higher attrition rate ( 60 [ 19% ] participants withdrew from the study ) than the control group ( 36 [ 12% ] participants )  . 
the pilot work that informed this randomised controlled trial and which showed great promise for oncokompas , was done with survivors who were approximately 14 months post - diagnosis , so it is perplexing that the randomised controlled trial included a sample of predominantly much longer - term survivors . 
 as the authors suggested , the intervention might have been more beneficial if presented earlier . however , longer - term cancer survivors have unmet needs too and many will experience late effects of their vol 21 january 2020 comment comment published online july 7 , 2016 s1470 - 2045 ( 16 ) 30152 - 8 see articles page 1114 bernardi d , macaskill p , pellegrini m , et al . 
breast cancer screening with tomosynthesis ( 3d mammography ) with acquired or synthetic 2d mammography compared with 2d mammography alone ( storm - 2 ) : a population - based prospective study . 
radiology 2014 ; 271 : 65563 . combined modality adjuvant therapy for high - risk endometrial cancer the incidence of endometrial cancer has steadily increased over the past decade , with 320 000 new cases reported worldwide in 2012.1 endometrial cancer is the fth most common cancer in women , and incidence is projected to increase2 because of an increased prevalence of obesity and an ageing population . 
although most patients present with early - stage low - risk disease , a rise in incidence is expected to lead to an increasing number of high - risk cases at presentation . 
this heterogenous group of tumours is characterised by higher grade and stage , lymph - vascular space deep myometrial invasion , or non - endometrioid histologies , such as serous or clear - cell cancers . 
external beam radiotherapy showed a signi cant reduction in the risk of local relapse compared with observation , but did not show a signi cant survival advantage in a high - risk subgroup meta - analysis.3 invasion , although endometrial cancers are generally radiosensitive and local relapse might be prevented by radiotherapy , many patients with high - risk disease still have distant metastatic relapses . 
hogberg and colleagues5 pooled the data of the nsgo - ec - 95016 and the mango iliade - iii trials and reported on 534 patients randomly assigned to either radiotherapy or combined colleagues4 previously and sequential radiotherapy and chemotherapy in the adjuvant setting . 
the nsgo - ec - 9501 study and both studies combined showed a signi cant improvement in progression - free and cancer - speci c survival in the combined treatment group . in the lancet oncology , stephanie de boer and colleagues7 report the rst results of the multicentre portec - 3 randomised trial , focusing on toxicity and 2 - year quality in those who received radiotherapy and those who received chemotherapy plus radiotherapy . 
 toxicity and quality of life data were available for 660 patients and showed a higher incidence of severe adverse events and patient - reported symptoms in the combined group with radiotherapy and chemotherapy , mainly related to the well known side - e ects of paclitaxel and carboplatin therapy . 
 most patients with adverse events recovered quickly after the end of the treatment , although peripheral sensory neuropathy was deemed troublesome by a quarter of all patients in the combined group at 2 years . 
although the toxicities of combined treatment were shown to be manageable , whether this investment of adding chemotherapy will be rewarded by an improved outcome in the long term remains unclear . 
the fact that a toxicity and quality of life analysis were included as secondary endpoints in the trial design , which was not the case for the combined nsgo - ec - 9501 and mango iliade - iii trials , 5 is a merit to the researchers . 
more than a third of all vol 17 august 2016 1029 comment patients in both groups did not receive a complete staging surgery , including lymphadenectomy , because lymphadenectomy was optional . 
this could lead to the underestimation of stage iiic disease in which the addition of chemotherapy has been shown to increase survival.4 , 5 although two large randomised trials8 , 9 could not establish the value of a systematic lymphadenectomy in stage i endometrial cancer , the number of high - risk cases in these studies was rather small . 
to establish the value of a pelvic and para - aortic lymphadenectomy in high - risk endometrial cancer , the statec study ( selective targeting of adjuvant therapy for endometrial cancer , nct02566811 ) is in preparation at present . 
furthermore , if future results of the portec - 3 trial con rm the progressionfree and cancer - speci c survival bene t for the combined treatment group observed in the combined nsgo - ec - 9501 and mango iliade - iii trials , the question remains of how much radiotherapy adds to the observed e ect of adjuvant chemotherapy . 
 this will be addressed by the results of the ongoing gog - 258 the ( nct00942357 ) , same combined chemoradiotherapy regimen as in portec - 3 . studying trial overall , the study by de boer and colleagues clearly shows the feasibility of combined modality if the therapy for high - risk endometrial cancer . 
 study shows a survival bene t for the adjuvant chemotherapy plus radiotherapy , combined therapy is expected to become the standard - of - care for high - risk endometrial cancer . 
with the present data on toxicity and quality of life , the ( yet to be determined ) survival bene ts of chemotherapy can be weighed against the adverse events and quality of life measures reported in this study , which will improve the adjuvant therapy for women with high - risk endometrial cancer . adriaan vanderstichele , * patrick neven , ignace vergote department of gynaecology and obstetrics , university hospitals leuven , leuven , belgium ( av , pn , iv ) ; and division of gynaecological oncology , leuven cancer institute , ku leuven , leuven , belgium ( av , pn , iv ) patrick.neven@uz.kuleuven.ac.be we declare no competing interests . 
usa endometrial cancer projections to 2030 : should we be concerned ? future oncol 2014 ; 10 : 256168 . kong a , johnson n , kitchener hc , lawrie ta . 
a randomized phase - iii study on adjuvant treatment with radiation ( rt ) + / chemotherapy ( ct ) in early stage high - risk endometrial cancer ( nsgo - ec - 9501 / eortc 55991 )  . 
toxicity and quality of life after adjuvant chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer ( portec - 3 ) : an open - label , multicentre , randomised , phase 3 trial . 
j natl cancer inst 2008 ; 100 : 170716 . early treatment for high - risk smouldering myeloma : has the time come ? published online july 8 , 2016 s1470 - 2045 ( 16 ) 30151 - 6 see articles page 1127 initiation a central question in oncology refers to the optimum timing of treatment in asymptomatic patients with a malignant phenotype . 
early treatment initiation did not improve survival in studies of chronic lymphocytic leukaemia1 and asymptomatic low - grade non - hodgkin lymphoma , 2 , 3 but this outcome might change with the use of novel drugs . 
 first , the prognosis of patients with smouldering myeloma is very heterogeneous , with some patients progressing to multiple myeloma rapidly and others only after long - term follow - up or even not at all . 
 second , before the introduction of novel drugs , the e cacy of available treatment was suboptimum at best ; 1030 vol 17 august 2016 hong kong : long civil unrest with long - term consequences hong kong has experienced a period of civil unrest in the past 6 months , which has affected the everyday lives of citizens . 
health - care services have been disrupted , with physical injuries resulting from clashes between protesters and police and the extensive use of chemical weapons at the forefront of medical concerns . 
these effects should be of concern for oncologists , most notably the poorly understood risks of accumulated chemicals and air pollution and the disruption of treatment services and research projects . from both sides of the conflict , the use of chemical weapons is an issue . 
the hong kong police has been criticised for their heavy use of tear gas , with an estimated 16 000 canisters deployed since june , 2019 , including near kindergartens , hospitals , and care homes . 
 the police have declined to divulge the chemical composition of the gas , making it difficult to assess the real risks , but nonetheless tear gas is known to be associated with several health hazards , including lung injuries and eye and skin problems . 
however , its combination with volatile chemicals from firebombs used by protesters , resulting in the emission of copious amounts of carbon monoxide and hydrogen cyanide , and the poor air quality , which was already a problem in hong kong , creates the perfect storm for the development or exacerbation of skin , eye , and lung conditions . 
with protests lasting hours or even days , both protesters and the police are being exposed for substantial amounts of time to toxic agents and many might be unable to use decontamination measures after exposure . 
for vulnerable populations , such as children , the elderly , and patients with chronic diseases who are at high risk of comorbidities , the effect of accumulated toxic chemicals might be devastating . 
 with the number of new cases of cancers predicted to increase by 3040% in hong kong by 2030 compared with 2016 , and with lung cancer expected to represent one of the largest increases , a toxic environment might easily aggravate the cancer epidemic in the region . disruption of services is a major concern for patients with cancer because their care requires many hospital visits , from diagnosis to treatment and years of followup . 
with hospitals now overburdened with injured people and , understandably , a focus on emergency services and deployment of doctors , nurses , and paramedics in the conflict areas , resources for tertiary care , both in terms of staff and equipment , might be scarce . 
transportation has also been affected and with the visible devastation in the streets and citizens concerned for their own safety , patients and hospital personnel might not be willing or able to access treatment or get into work because of disruption of the metro system and other means of public transportation . 
the damage goes beyond infrastructure destruction : several chemicals have been stolen to produce weapons against the police ; there is uncertainty regarding the quality of water and air , and the adequacy of electricity supplies ; and animals used for research have not been properly supervised and cared for . 
therefore , results from in - vitro and invivo research are likely to be rendered invalid , with a consequent substantial financial and scientific loss for these universities , in addition to the costs needed to repair structural damage . 
the hong kong cancer fund , for example , had to cancel its annual fundraising initiative , stride for a cure , which should have taken place on dec 8 , 2019 , and would have seen the participation of around 2000 people united to raise money to fund cancer research . the management of this conflict must go beyond the actions of protesters and police and the short - term treatment of injuries . 
the lancet oncology for more on health - care disruption see editorial lancet 2019 ; 394 : 2040 for more on the use of tear gas see com / 2019 / 12 / article / hk - policeunder - fire - over - use - of - tear - gas / for more on the exposure of the hong kong population to tear gas see com / news / articles / 2019 - 11 - 05 / up - to - 88 - of - hong - kongpopulation - exposed - to - tear - gassince - june for more on the use of firebombs see scmp.com / news / hong - kong / politics / article / 3031760 / hongkong - fire - officials - worriedprotesters - could - follow for more on the rise of cancer incidence see scmp.com / news / hong - kong / health - environment / article / 2174199 / new - cancercases - hong - kong - projected - rise40 - cent for more on the medical teams helping in the field see science / article / pii / s0140673619329095 ? via%3dihub for more on research disruption see news / hong - kong / healthenvironment / article / 3040165 / polytechnic - university - facingimmeasurable - loss for more on stride for a cure cancellation see scmp.com / comment / letters / article / 3040688 / hong - kongcancer - fundraiser - walkcancelled - heartbreaking - decision vol 21 january 2020 editorial re ection and reaction cancer patterns in inuit populations i wish to congratulate friborg and melbye1 on their informative review of cancer patterns in inuit populations , published in the september issue of the lancet oncology . 
as a clinician working with inuit in the nunavik region of northern quebec , i believe there are a few additional points worth mentioning . individuals first , there are a few small , but noteworthy , caseseries describing kaposis sarcoma in hiv seronegative inuit from greenland and nunavik . 
 although classic kaposis sarcoma is associated with human herpesvirus - 8 and is usually seen in elderly male patients of mediterranian or jewish descent , this disease has been described in eight immunocompetent inuit patients since 1974.2 a similar combination of genetic susceptibility and viral factors , as described by the authors with respect to nasopharyngeal carcinoma and epstein - barr virus in the inuit , might be responsible . second , with respect to the high incidence of cancers of the nasopharynx and lung , two signi cant exposures were not mentioned . 
although modern housing conditions have decreased exposure to fumes from lamps and open res for cooking , it is important to recognise that many groups of inuit still spend substantial amounts of time out on the land , cooking on open stoves inside their tents . 
additionally , the epidemic of marijuana smoking in 85% of adults ( according to 2004 nunavik public - health data ) 3 might play a part in the high incidence of lung and nasopharyngeal cancers . last , but not least , it is important to recognise that inuit face substantial challenges with respect to access to healthcare , and that these challenges represent part of a more far - reaching social inequality . 
 public - health statistics from the last 5 - year case period in nunavik suggest that both cancer incidence and mortality are higher overall for the subarctic inuit of the region than for age - matched southern patients.4 , 5 with life expectancy for canadian inuit more than 12 years less than the national average , 6 we must not forget that documents such as the universal declaration of human rights and the recommendations for worldwide cancer life expectancy for inuit is less than national average control mentioned in a comment by john se rin7 need to be applied for minority populations within developed countries as well as throughout the global community . barbara m young general internal medicine division , mcgill university , montreal , quebec , canada barbara.young@mcgill.ca the author declared no con icts of interest . friborg jt , melbye m . 
resumes_nunavik / anglais / alcoholdruguseandgamblingamongtheinuito fnunavik.pdf ( accessed nov 7 , 2008 )  . taux dincidence pour lensemble des sieges , excluant le cancer de la peau sans melanoma 2000 2004 . 
msss fichier des decs ( qubec ) , october 2005 ( electronic version )  . 6 wilkins r , uppal s , fins p , sencal s , guimond e , dion r . 
in this article , the header of the second column in table 2 should have read : time since diagnosis ( months )  . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology 1124 vol 9 december 2008 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper go to thelancetoncology for information for authors see authors / oncology / authorinfo goldhirsch a , wood wc , gelber rd , et al . 
ann oncol 2007 ; 18 : 113344 . arimidex , tamoxifen , alone or in combination ( atac ) trialists group.e ect of anastrozole and tamoxifen as adjuvant treatment for early - stage breast cancer : 100 - month analysis of the atac trial . 
skeletal e ects of exemestane on bone - mineral density , bone biomarkers , and fracture incidence in postmenopausal women with early breast cancer participating in the intergroup exemestane study ( ies ) : a randomised controlled study . 
eur j cancer 2006 ; 42 : 296875 . call for papers : lung cancer , storyboard , and from the archives in 2007 the lancet oncology published themed issues on paediatric oncology and on breast cancer . 
despite many advances in treatment over recent years , lung cancer is still the number one cause of death due to cancer in the world1 and mean relative 5 - year survival is only 126% in europe2 . 
accepted in the lancet oncology papers will be published to coincide with the international lung cancer conference ( [ ilcc ] liverpool , uk , july 912 , 2008 )  . 
if your study describes , in part or wholly , a study accepted for presentation at the ilcc , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication in the lancet oncology can be scheduled to comply with ilccs embargo policies . 
articles should be submitted via the lancet oncologys online submission service , and all authors must clearly state in the covering letter that their submission is in response to the lung cancer call for papers . 
 storyboard will provide and entertaining opportunity to present new oncological in pictorial form and will allow the techniques progressive accumulation of knowledge by leading a reader from panel - to - panel . 
from the archives will be a short report based on a reference of historical importance in oncology that has contributed to a substantial change in thinking in the era originally published . 
please see our information for authors for full details of these new sections . lidia siemaszkiewicz the lancet oncology , london nw1 7by , uk parkin dm , bray f , ferlay j , pisani b . 
the last two sentences of the summarys findings should have read st gallen guidelines identi ed 353 ( 83% ) patients with poor prognosis and discordance with the signature in 168 ( 39% ) patients . 
 nottingham prognostic index recorded 179 ( 42% ) patients with poor prognosis and discordance with the signature in 117 ( 27% ) patients . vol 9 january 2008 correction to lancet oncol 2020 ; 21 : 26170 correction to lancet oncol 2020 ; 21 : 80820 correction to lancet oncol 2020 ; 21 : 92334 blay j - y , serrano c , heinrich mc , et al . 
quality of life in patients with cervical cancer after open versus minimally invasive radical hysterectomy ( lacc ) : a secondary outcome of a multicentre , randomised , open - label , phase 3 , noninferiority trial . 
this correction has been made to the online version as of june 29 , 2020 . vol 21 july 2020 e341 corrections expanding access to radiotherapy in sub - saharan africa an international collaboration has brought together experts in medical physics , accelerator technology , and oncology for an innovative project that aims to develop novel radiotherapy technologies for subsaharan africa . 
 the project , innovative technologies towards building affordable and equitable global radiotherapy capacity ( itar ) , funded by the uk science and technology facilities council , involves 22 african countries and presents an opportunity to expand global access to radiotherapy . in 2015 , the lancet oncology published a commission on expan ding global access to radiotherapy . 
 insufficient the report showed radiotherapy coverage in many lowincome and middleincome countries ( lmics ) and estimated that 2600 radiotherapy departments , 5200 machines , and 55 800 radiation oncologists , medical physicists , and radiotherapy technologists would be needed by 2035 to meet demands . the inequities in radiotherapy access are still relevant today . 
the 2020 who world cancer report highlighted from an epidemiological shift incidence of communicable to non communicable diseases in africa and included data showing the significant relationship between the number of available radiotherapy machines and cancer mortality . a common misconception sur rounding radiotherapy access in africa is that the base cost of the machines is too high . 
the base cost is not what limits their usage , says graeme burt ( lancaster university , lancaster , uk and leader of the itar project ) , the maintenance cost is the big burden and it is this burden that the itar project is trying to reduce . 
if budgets are constrained , machines sit dormant compromising urgent treatment , explained burt . designing a robust and tailored machine requires extensive data from the clinicians and hospitals so a key question is what exactly are the challenges right now in these settings ? says taofeeq ige ( national hospital abuja , abuja , nigeria )  . 
 therefore , collecting realtime data on what the issues are then trying to feed this back into what the solutions are going to be is a key component of the project , says ige . 
these data have been obtained by questionnaires returned by 25 health care facilities across 20 african countries ; this information will enable the formulation of effective solutions that are tailored for each country and setting . 
there is a granularity within subsaharan africa , which is why the ongoing in country data analysis is so important . itar is a crucial component of a bigger projectsmart technology to extend lives with linear accelerators ( project stella ) a multidisciplinary collaboration that aims to produce effective radiotherapy machines and provide access to relevant training and mentoring . 
nina wendling , ( international cancer expert corps [ icec ] ) , says that one of the issues is that people have these wonderful machines but not the support to be able to deliver treatment . 
they can vol 21 august 2020 published online june 25 , 2020 s14702045 ( 20 ) 303764 for the the lancet oncology commission see lancet oncol 2015 ; 16 : 115386 for the 2020 who world cancer report see iarc.fr / 586 for more on radiotherapy machine access and cancer mortality see dovepress.com / numberof radiotherapytreatment machinesinthepopulation and cancerpeerreviewed articleclep for more on the stella and itar projects see iceccancer.org / innovative radiotherapytechnologies pick up the phone or get on a zoom call when they have a question , explains wendling . 
having virtual training sessions enables individual and group discussions to take place and international partnerships to be formed , which is particularly relevant during the ongoing covid19 pandemic ; however , the training also has the capacity for inperson demonstrations and workshops . 
the medical experts and training input of icec is an asset for the collaborators working on stella and itar , believes manjit dosanjh ( university of oxford , oxford , uk and stella project lead ) , because they are able to set up seed centres and partnerships in africa that facilitate this transfer of knowledge and create centres of excellence that will last into the future . the ultimate aim of itar is to have a robust , lowmaintenance in africa radiotherapy machine saving lives says burt , but project stella is more than that : it is about delivering training and mentoring expertiserendering programmes for professionals in lmics to help ensure the safe and efficient delivery of quality cancer radiotherapy . 
this international collaboration connects medical engi neering with education and holistic strengthening of health care systems , thus providing hope for improving global radiotherapy access . rebecca barksby 1019 news building a more resilient cancer healthcare system the outbreak of the covid - 19 pandemic has resulted in major disruptions to cancer care worldwide , including cancer screening programmes . 
 however , an increased focus on the prevention and early diagnosis of cancer could increase health - system resilience and lessen reliance on resource - intensive interventions , because early stage cancers can be treated more effectively , and cost - efficiently , than advanced stage disease . 
for this endeavour to succeed , clinical and technological developments in early cancer diagnosis are key . with screening so important , it is a stark statistic that for lung cancer , screening rates are as low as 6% in at - risk populations compared with 6080% for breast , colon , or cervical cancer screening , even though identification through screening can reduce early the risk of lung cancer death by 20% . 
us research shows that nearly two - thirds of newly diagnosed patients with lung cancer do not meet current us preventive services taskforce ( uspstf ) criteria for annual lung cancer scans with low - dose ct , but have a similar risk of death to those who meet the criteria . 
the minimum age of inclusion would be reduced by 5 years to include adults aged 5080 years who have a 20 pack - year smoking history , as opposed to the threshold of 30 pack - years in the current guidance . 
around 1015% of patients with lung cancer in the uk have never smoked , while in east asia , the incidence of lung cancer in non - smokers is about 53% and predominantly occurs in women . 
with nonsmokers not necessarily meeting the criteria for lung cancer screening programmes , understanding the early processes of lung carcinogenesis in non - smokers is necessary to ensure early detection . 
 undertaking genomic , transcriptomic , proteomic , and phosphorylation analyses on 103 samples of early - stage non - small - cell lung cancer ( nsclc ) tumours from nonsmokers , chen and colleagues found that tumours in women often had egfr mutations whereas kras and apc gene alterations were more common in men . 
the study also found a high prevalence of apobec mutations in 75% of tumours from female patients younger than 60 years and genetic mutations resulting from exposure to environmental carcinogens , such as air pollution , in tumours from older women . 
these differences highlight not only a need for new treatments and diagnostic approaches for non - smokers with lung cancer , but also targeted interventions differentiated by sex . on july 3 , 2020 , the uk government together with various charities , announced a 16 million commitment to fund the development of integrated diagnostics to enable earlier detection and diagnosis of oesophageal , bowel , and lung cancer . 
 for example , data from the tracerx study , showed that ai - driven lung cancer screening combined with next - generation sequencing can map the evolution of lung cancer to predict clinical outcomes at the point of diagnosis . 
research such as this could transform the way cancer is diagnosed and better select those patients who are most likely to relapse and for whom treatments should be initiated earlier . building better resilience into cancer care systems is a clear lesson from covid - 19 , and the pandemic provides an important opportunity to re - evaluate and re - configure strategies for global cancer control by directing available resources where they are most likely to have the largest benefit . 
all stakeholders should redouble their efforts on prevention and early detection to ensure cancer healthcare systems are not stressed beyond breaking point in response to another highly disruptive event in the future . 
we sought to establish whether indocyanine green fluorescent dye is non - inferior to isosulfan blue dye in detecting sentinel lymph nodes in women with cervical and uterine cancers . methods in this non - inferiority , within - patient comparison study , patients aged 18 years or older with clinical stage i endometrial or cervical cancer undergoing curative surgery were randomly assigned 1 : 1 to lymphatic mapping with isosulfan blue dye ( visualised by white light ) followed by indocyanine green ( visualised by near - infrared imaging ) , or indocyanine green followed by isosulfan blue dye . 
 the primary outcome was efficacy of intraoperative indocyanine green with near - infrared fluorescence imaging versus that of isosulfan blue dye in the identification of lymph nodes , defined as the number of lymph nodes identified by indocyanine green and isosulfan blue dye , respectively ( and confirmed as lymphoid tissue by histology ) , divided by the number of lymph nodes identified intraoperatively and excised . 
the study had a 5% non - inferiority margin needed to show non - inferiority of the frequency of lymph node detection with indocyanine green to that with isosulfan blue dye with 80% power at a 5% two - sided significance level . 
the trial was registered with clinicaltrials.gov , number nct02209532 , and is completed and closed . findings between dec 21 , 2015 , and june 19 , 2017 , 180 patients were enrolled and randomly assigned to the two groups ( 90 to each group ) ; 176 patients received the intervention and were evaluable ( modified intention - totreat population )  . 
517 sentinel nodes were identified in the per - protocol population ( n = 163 ) , of which 478 ( 92% ) were confirmed to be lymph nodes on pathological processing : 219 ( 92% ) of 238 nodes that were both blue and green , all seven nodes that were blue only , and 252 ( 95% ) of 265 nodes that were green only ( p = 033 )  . 
 in total , 471 ( 97% ) of 485 lymph nodes were identified with the green dye and 226 ( 47% ) with the blue dye ( difference 50% , 95% ci 3962 ; p < 00001 )  . 
in the modified intention - to - treat population ( n = 176 ) , 545 nodes were identified , of which 513 ( 94% ) were confirmed to be lymph nodes on pathological processing : 229 ( 92% ) of 248 nodes that were both blue and green , all nine nodes that were blue only , and 266 ( 95% ) of 279 nodes that were green only ( p = 030 )  . 
the technique of lymphatic mapping and sentinel lymph node biopsy has improved surgeons ability to detect small - volume disease in lymph nodes while greatly reducing intraoperative and postoperative morbidity . 
this technique has been validated and is 1394 vol 19 october 2018 articles research in context evidence before this study before development of the concept for the film study and the production of the subsequent protocol , we reviewed the medical literature to evaluate the off - label use of indocyanine green and near - infrared imaging for lymphatic mapping and sentinel lymph node biopsy in all solid tumours . 
we searched pubmed and clinicaltrials.gov , without date or language restrictions , using the terms indocyanine green , icg , near infrared imaging , lymphatic mapping , and sentinel node . 
we identified several small , single - institution retrospective reports of interstitial injection of indocyanine green for lymphatic mapping in a wide range of solid tumours including breast , uterine , cervical , vulval , lung , kidney , and colon cancers as well as cutaneous melanoma . 
 all these studies showed that use of indocyanine green with near - infrared imaging was feasible and safe for lymphatic mapping in solid tumours and that the technique might potentially improve on substances currently approved by the us food and drug administration for mapping such as patent blue dyes and radiocolloids . 
however , no prospective , controlled studies had compared the use of indocyanine green as a mapping substance with standard of care . added value of this study although the film study was designed as a non - inferiority comparison of the efficacy of intraoperative indocyanine green with near - infrared imaging to blue dye in the identification of lymph nodes , our results showed superiority of the experimental group over standard of care . 
it also identified all sentinel nodes with metastatic disease , whereas isosulfan blue dye missed a large proportion of them . implications of all the available evidence the results of this study will serve as the basis for an application to the food and drug administration for on - label use of interstitial injection of indocyanine green combined with near - infrared imaging for lymphatic mapping . 
if it is approved for on - label use , it will hopefully become the new standard of care for lymphatic mapping and sentinel lymph node biopsy for women with cervical and uterine cancers , and could subsequently be adopted as the mapping substance of choice across multiple subspecialties in surgical oncology . widely accepted as part of the surgical treatment of vulval and breast carcinomas and cutaneous melanoma . 
 gynaecological oncologists are also starting to adopt lymphatic mapping and sentinel node biopsy for women with cervical and uterine cancers.13 in lymphatic mapping for cervical and uterine cancers , mapping agents are most commonly injected into the cervix , a practice that should result in drainage to bilateral sentinel nodes in the pelvis . 
if lymphatic mapping does not identify bilateral sentinel nodes , well accepted algorithms recommend complete pelvic lymphadenectomy on the side with no sentinel nodes detected.4 , 5 because complete pelvic lymphadenectomy increases surgical time and the risks of intraoperative vascular injury and postoperative lower extremity lymphoedema and lymphocyst formation , it is crucial that lymphatic mapping identifies bilateral sentinel nodes . historically , patent blue dye with or without radiocolloid has been the most commonly used agent for lymphatic mapping in women with uterine cancers . 
 however , blue dye alone identifies at least one sentinel node in only 80% of patients and bilateral sentinel nodes in as few as 50% of patients.6 combining blue dye with radiotracer increases the rate of detection of at least one sentinel node to 88% , but the rate of detection of bilateral sentinel nodes to only 51%.6 with either technique , therefore , almost half of women with uterine cancer undergoing lymphatic mapping might require unilateral or bilateral pelvic lymphadenectomy , which increases the risk of surgical complications and long - term morbidity . the fluorescent dye indocyanine green has been explored as an off - label alternative to blue dye for lymphatic mapping in cervical and uterine cancers . 
 small series have shown the potential of interstitial indocyanine green injection to improve frequency of sentinel node detection over that observed with blue dye.79 however , no prospective , randomised studies have compared interstitial blue dye with indocyanine green injections for lymphatic mapping in cervical and uterine cancers . 
we therefore conducted the film ( fluorescence imaging for lymphatic mapping ) trial , which was designed to compare the detection of lymph nodes after interstitial indocyanine green injection versus interstitial isosulfan blue dye injection ( the standard of care ) in women with cervical and uterine cancers . methods study design and participants the film trial was an international , multicentre , randomised , open - label , phase 3 study designed to assess the safety and efficacy of indocyanine green and pinpoint near - infrared fluorescence imaging ( stryker , kalamazoo , mi , usa ) in identification of lymph nodes in women with cervical and uterine malignancies undergoing lymphatic mapping following interstitial vol 19 october 2018 1395 articles see online for appendix cervical injection of coloured dye . 
 comparison we chose this design because it would meet our primary objective and give us reliable results with fewer patients than if we had two separate randomised groups . participating surgeons were required to have completed at least ten lymphatic mapping procedures , including at least three with the pinpoint near - infrared fluorescence imaging system , before the initiation of enrolment . 
 patients were eligible for enrolment if they were 18 years of age or older , diagnosed with international federation of gynecology and obstetrics clinical stage i cervical or uterine cancer ( any histology ) , and were scheduled for curative surgery that included lymph node assessment . 
patients were ineligible if they had previous pelvic dissection or irradiation , advanced cervical or uterine cancer , t3 or t4 lesions , cervical tumour size larger than 2 cm , hepatic dysfunction defined as a model for end - stage liver disease score of 10 or greater , renal dysfunction defined as serum creatinine of 20 mg / dl or greater , or a known allergy to indocyanine green , iodine , iodine dyes , isosulfan blue , or triphenylmethane . the protocol was approved by institutional review boards at each centre , and all patients enrolled gave written informed consent . 
the protocol is available in the appendix ( p 3 )  . randomisation and masking participants were prospectively enrolled into the film trial and underwent random assignment on the day of surgery . 
 participants were randomly assigned on a 1 : 1 basis to either lymph node mapping with isosulfan blue dye followed by lymph node mapping with indocyanine green dye and near - infrared imaging ( pinpoint ) , or lymph node mapping with indocyanine green dye and near - infrared imaging ( pinpoint ) followed by lymph node mapping with isosulfan blue dye . 
randomisation was stratified by study site , with permuted block randomisation within the opportunity for the sequence to be predicted , the block size was variable and randomly chosen from small multiples of two ( ie , two , four , or six )  . 
all participants were masked to their randomisation assignment ( because they were under anaesthesia ) until after the procedure . procedures patients were removed from the study if found to not meet eligibility criteria or if they requested removal at any time before surgery ( patients could request removal at any time during the study )  . 
after general anaesthesia was achieved , the first dye was injected in the cervix deeply and superficially at both 0300 h and 0900 h , followed by the second dye deeply and superficially at both 0300 h and 0900 h , for a total of eight injections . 
for the blue dyeindocyanine green group , the isosulfan blue dye injections were done first , and for the indocyanine greenblue dye group , the indocyanine green injections were done first . 
each blue dye injection consisted of 1 ml of a 10 mg / ml isosulfan blue dye solution ( 1% isosulfan blue ) , for a total dose of 40 mg ; each indocyanine green injection consisted of 1 ml of a 125 mg / ml indocyanine green solution ( novadaq technologies , mississauga , on , canada ) for a total dose of 5 mg . the surgeon identified lymph nodes and lymphatic vessels with white light for isosulfan blue dye ( blue nodes ) or near - infrared imaging with pinpoint for indocyanine green ( green fluorescent nodes ) depending on random isation cohort . 
to minimise the chance that leakage of blue dye or indocyanine green would interfere with mapping , mapping was done first on one side of the pelvis and then on the other side . 
in both patient groups , mapping with the first dye was completed before mapping with the second dye was started , and mapping with both dyes was completed before any lymph nodes were excised . 
mapping with indocyanine green was considered complete when the surgeon identified all green nodes or determined that green nodes could not be identified and the surgeon had scanned the full 360 - degree area within the abdominal cavity . 
 1396 vol 19 october 2018 articles 199 patients screened 19 excluded 180 enrolled and randomly assigned 3 did not receive intervention 1 due to iodine allergy 1 due to negative margins on cone biopsy 1 due to presence of intraperitoneal metastatic disease on laparoscopic exploration 6 protocol violations 2 due to pregnancy test not done on day 0 1 due to incorrect blue dye used 1 due to presence of intraperitoneal metastatic disease on laparoscopic exploration 1 due to no calculation of meld score 1 due to equipment malfunction 90 assigned to blue dyeindocyanine green 90 assigned to indocyanine greenblue dye 87 received intervention and included in mitt analysis 89 received intervention and included in mitt analysis 1 did not receive intervention 1 had excessive bleeding and did not undergo injection of mapping substances 7 protocol violations 3 due to no calculation of meld score 1 due to equipment malfunction 1 due to conversion to open surgery 1 due to incorrect dose of blue and green dye injections 1 due to participation in another trial 81 included in per - protocol analysis 82 included in per - protocol analysis figure : trial profile mitt = modified intention - to - treat . 
 bilateral lymphatic mapping was done according to published national comprehensive cancer network guidelines.4 , 5 all sentinel lymph nodes resected had confirmation of nodal tissue by haematoxylin and eosin staining . 
all participants had standard - ofcare assessments throughout the study according to the hospital or institutions standard procedures , and study - specific visits to monitor occurrence of any adverse events or adverse device effects on postoperative day 1 , the date of discharge , and day 30 ( or within 7 days before or after this date )  . 
 adverse events were characterised as mild , moderate , or severe and assigned relationship ( suspected or not suspected ) to either dyes or device . outcomes the primary endpoint was efficacy of intraoperative indocyanine green with near - infrared fluorescence imaging versus that of blue dye in the identification of lymph nodes , defined as the number of lymph nodes identified by each dye ( and confirmed as lymphoid tissue by histology ) divided by the number of lymph nodes identified intraoperatively and excised . 
secondary end points were the rate of intraoperative detection of at least one sentinel node per patient and the rate of detection of bilateral sentinel nodes with indocyanine green compared with isosulfan blue dye , and the safety of each detection method . 
two other secondary endpoints ( the proportion of lymph nodes identified from following lymphatic channels and the anatomical distribution of lymph nodes ) will be reported in a separate publication . statistical analysis we hypothesised that the use of indocyanine green and near - infrared imaging would be non - inferior to isosulfan blue dye in the detection of sentinel nodes . 
analysis of the primary endpoint was done with a two - sided 95% ci for the difference in proportions using the approach described by nam and kwon for clustered matched - pair data ( the clustering in question being lymph nodes nested within patients ) .11 formal testing for hetero geneity was not completed . 
 results between dec 21 , 2015 , and june 19 , 2017 , 180 patients were enrolled and randomly assigned to the two groups ( 90 to each group ) , of whom 176 received the intervention and were evaluable ( figure )  . 
169 ( 96% ) of 176 patients had uterine cancer and seven ( 4% ) had cervical cancer . after exclusion of 13 patients with major protocol violations ( six in the blue dyeindocyanine green group and seven in the indocyanine greenblue dye group ) , there were 163 in the per - protocol population and primary analytical cohort . 
in this population , 517 nodes were identified intraoperatively and excised , of which 478 ( 92% ) were confirmed to be lymph nodes : 219 ( 92% ) of 238 nodes that were both blue and green , all seven nodes that were blue only , and 252 ( 95% ) of 265 nodes that were green only ( p = 033 ; table 2 )  . 
in total , 471 ( 97% ) of 485 lymph nodes were identified with the green dye and 226 ( 47% ) with the blue dye ( difference 50% , 95% ci 3962 ; p < 00001 )  . 
thus , we were able to conclude that indocyanine green is not inferior to isosulfan blue dye in the identification of nodes . the mean number of nodes per patient in the per - protocol population was 32 ( sd 16 )  . 
at least one node was identified in 159 ( 98% ) of 163 patients with indocyanine green and in 124 ( 76% ) of 163 patients 1398 vol 19 october 2018 articles with isosulfan blue dye ( difference 22% , 95% ci 1732 ; p < 00001 )  . 
bilateral sentinel nodes were identified in 134 ( 82% ) patients , 52 ( 32% ) with isosulfan blue dye and 132 ( 81% ) with indocyanine green ( 49% , 4157 ; p < 00001 )  . 176 evaluable patients received at least one injection of indocyanine green or blue dye and constituted the mitt population . 
545 nodes were identified in total , of which 513 ( 94% ) were confirmed to be lymph nodes : 229 ( 92% ) of 248 nodes that were both blue and green , all nine nodes that were blue only , and 266 ( 95% ) of 279 nodes that were green only ( p = 030 ; table 2 )  . 
thus , we were able to conclude that indo cyanine green is superior to isosulfan blue dye in the identification of nodes . in the mitt population , at least one node was identified in 168 ( 95% ) of 176 patients with indocyanine green and 131 ( 74% ) patients with isosulfan blue dye ( difference 21% , 95% ci 1428 ; p < 00001 )  . 
bilateral sentinel nodes were identified in 54 ( 31% ) of 176 patients with isosulfan blue dye and 138 ( 78% ) of 176 patients with indocyanine green ( 47% , 3056 ; p < 00001 )  . in the 545 nodes ( mean 31 nodes [ sd 17 ] per patient ) identified in the mitt population , isosulfan blue dye identified 257 ( 47% ) sentinel nodes ( mean 15 [ 13 ] per patient ) and indocyanine green identified 527 ( 97% ) sentinel nodes ( mean 30 [ 17 ] per patient ; difference 50% ; 95% ci 3961 ; p < 00001 )  . 
difference estimates and 95% cis indicated that estimates of superiority were consistent throughout all sites ( data not shown )  . randomisation group did not affect the ability of isosulfan blue dye or indocyanine green to detect any or bilateral sentinel nodes in the mitt population . 
in the 87 patients in the blue dyeindocyanine green group , at least one sentinel node was identified in 63 ( 72% ) patients with isosulfan blue dye and in 83 ( 95% ) patients with indocyanine green . 
in the 89 patients in the indocyanine greenblue dye group , at least one sentinel node was identified in 68 ( 76% ) patients with isosulfan blue dye and in 85 ( 96% ) patients with indocyanine green . 
in the indocyanine greenblue dye group , isosulfan blue dye detected a sentinel node in two ( 2% ) patients without a sentinel node detected by indocyanine green . per - protocol population modified intention - to - treat population proportion detected p value p value proportion detected 033 030 219 / 238 229 / 248 indocyanine green only 252 / 265 confirmation of nodal tissue in sentinel lymph node blue dye plus indocyanine green blue dye only identification of one or more sentinel lymph nodes indocyanine green only blue dye only identification of bilateral sentinel lymph nodes indocyanine green only blue dye only 100% 159 / 163 124 / 163 132 / 163 54 / 163 100% 266 / 279 168 / 176 131 / 176 138 / 176 54 / 176 < 00001 < 00001 < 00001 < 00001 table 2 : sentinel lymph node identification by indocyanine green and isosulfan blue dye in the blue dyeindocyanine green group , isosulfan blue dye identified bilateral sentinel nodes in 28 ( 32% ) of 87 patients , indocyanine green identified bilateral sentinel nodes in 67 ( 77% ) patients , and indocyanine green identified bilateral sentinel nodes in 40 ( 46% ) patients without bilateral sentinel nodes identified by isosulfan blue dye . 
in the indocyanine greenblue dye group , isosulfan blue dye identified bilateral sentinel nodes in 26 ( 29% ) of 89 patients , indocyanine green identified bilateral sentinel nodes in 71 patients ( 80% ) , and isosulfan blue dye identified bilateral sentinel nodes in two patients ( 2% ) without bilateral sentinel nodes identified by indocyanine green . as a post - hoc analysis , we assessed metastatic disease . 
macrometastatic disease was found in eight ( 38% ) of 21 sentinel nodes , micro metastatic disease in five ( 24% ) , and isolated tumour cells in eight ( 38% )  . there were no allergic reactions or adverse events attributable to either isosulfan blue dye or indocyanine green . 
most adverse events were related to surgery ( eg , postoperative pain or ileus )  . discussion although this study was designed as a non - inferiority trial , our findings suggest that indocyanine green was superior to isosulfan blue dye in identifying sentinel lymph nodes in women with cervical and uterine cancer because indocyanine green identified sentinel lymph nodes in a much larger proportion of patients than isosulfan blue dye did . 
indocyanine green was also significantly superior to isosulfan blue dye in detecting vol 19 october 2018 1399 articles together does not seem at least one sentinel node and in detecting bilateral sentinel nodes . 
the use of indocyanine green and isosulfan blue dye be necessary , because the addition of isosulfan blue dye to indocyanine green identified few sentinel nodes beyond those identified with indocyanine green alone . 
 finally , interstitial injection of indocyanine green seems to be safe , as we recorded no adverse events related to the compound . our findings that isosulfan blue dye detected at least one sentinel node in 131 ( 74% ) of 176 patients and indocyanine green detected at least one sentinel node in 168 ( 96% ) of 176 patients in the mitt population are similar to what has been previously reported in the literature.6 however , blue dye alone detected bilateral lymph nodes in only 54 ( 31% ) patients in the mitt population , which is lower than the 5560% reported in previous studies.13 , 14 all surgeons participating in our study had attained proficiency in the mapping procedure , so it is difficult to attribute the low rate of detection of bilateral nodes with isosulfan blue dye alone to poor technique or learning curve . 
multiple single - institution studies have found indocyanine green to be superior to blue dye and radiocolloid in detecting bilateral sentinel nodes after a cervical injection , 15 , 16 but a large , multi - institutional retrospective study did not show a difference between the two techniques.17 systematic reviews and meta - analyses also present conflicting results , with some showing combination blue dye and radiocolloid equivalent to indocyanine green in detecting bilateral sentinel nodes18 whereas others show that compared with use of blue dye alone , combined tracers might improve detection of at least one sentinel node but not detection of bilateral nodes.6 although the combination of blue dye and radiocolloid might be better than blue dye alone and equivalent to indocyanine green in detecting sentinel nodes , no studieseither prospective or retrospective have compared the combination of blue dye and radiocolloid with indocyanine green . 
however , the effect was much more pronounced with blue dye alone than with indocyanine green alone.8 because of the high rate of obesity in women with uterine cancer , many gynaecological oncologists have adopted the robotic system to assist in performing hysterectomy and staging , citing as their reason that the robotic system makes it easier to perform the lymphadenectomy portion of the surgery in women with a high bmi.19 , 20 the most commonly used robotic platform , the da vinci surgical system ( intuitive surgical , sunnyvale , ca , usa ) , includes an option for intraoperative near - infrared imaging called the firefly ( originally developed by novadaq technologies )  . 
 the fires trial , 21 a prospective cohort study , showed that indocyanine green and near - infrared imaging in the da vinci system had a sensitivity of 97% in detecting metastatic disease in sentinel nodes . 
the film protocol did not require completion of lymphadenectomy after sentinel node detection , so sensitivity and negative predictive values for the pinpoint system cannot be calculated in our study . 
moreover , the pinpoint technology and image display used in our study differed from that of the firefly , so the results of our study cannot be extrapolated to robotic surgery . 
in the fires study , at least one sentinel node was identified in 293 ( 86% ) of 340 patients , which is lower than the proportion of patients shown to have at least one sentinal node with indocyanine green and the pinpoint system in our study . 
additionally , the indocyanine green used in this study ( ic2000 ) might differ from the indocyanine green used in the fires trial ( no details given in the trial )  . 
 however , we believe lymphatic mapping and sentinel node detection with indocyanine green and near - infrared imaging is probably similar in the two systems , with potential applications of the technique in other cancers , including breast cancer and melanoma . breast cancer , like uterine cancer , has highly predictable lymphatic drainage . 
 consequently , preoperative lymphatic mapping with radiocolloid and dynamic imaging ( eg , lympho scintigraphy or single photon emission ctct [ spect / ct ] ) to establish site of incision is unnecessary for lymphatic mapping in breast cancer . 
for example , a direct comparison showed that indo cyanine green detected a sentinel node in 97100% of patients with breast cancer whereas blue dyes detected a sentinel node in 8889%.22 , 23 additionally , indocyanine green detects more sentinel nodes per patient than does blue dye . 
when compared with radiocolloid , indocyanine green does not appear to detect more sentinel nodes overall but might detect more metastatic sentinel nodes.24 for melanoma , interest in indocyanine green as an alternative to radiocolloid for lymphatic mapping and sentinel node biopsy has been somewhat more tempered . 
lymphatic drainage of melanoma can often be 1400 vol 19 october 2018 articles ambiguous , especially for lesions located on the trunk , head , or neck.25 preoperative lymphatic mapping with dynamic imaging ( lymphoscintigraphy or spect / ct ) is often necessary to identify draining nodal basins and to determine sites for surgical incision and exploration . 
 the penetrance of near - infrared cameras to detect sentinel nodes through the skin is only 23 mm , so the use of indocyanine green as a substitute for radiocolloid is largely ineffective , especially for lesions located in anatomical areas with ambiguous drainage.26 lymphatic mapping and sentinel node biopsy is an image - guided , precision surgical procedure that is increasingly being adopted for the surgical staging of apparent cervical - confined and uterine - confined malignancies . 
as use of indocyanine green for lymphatic mapping in cervical and uterine malignancies becomes more routine , we should also be aware of the potential pitfalls of this new exciting technology . 
this result is likely due to the bright green effect of the imaging with a laser - based near - infrared syste occasionally , dilated lymphatic channels can lead to a very bright signal that leads to the channels being mistaken for nodes and excised . 
mistaken excision of lymphatic trunks or adipose tissue instead of a node is potentially a major pitfall as sentinel node biopsy without complete lymphadenectomy becomes more common ; failure to excise a true node could leave the disease status of an entire hemipelvis unknown . 
if the surgeon has any doubt , it is reasonable to send the presumed nodal tissue for an confirm nodal content . intraoperative pathological consultation a second major potential pitfall of lymphatic mapping and sentinel node biopsy for cervical and uterine malignancies is the removal of multiple bright green nodes that appear to be true sentinel nodes but are in fact second - echelon and third - echelon nodes . 
this pitfall also relates to the bright signal from a laser - based , nearinfrared imaging platfor unlike isosulfan blue dye , which rarely can be seen beyond the first or true sentinel node to secondary - echelon nodes , indocyanine green often produces bright green signal in not only the true sentinel node but also secondary , tertiary , and more distant nodal basins . 
further , the enhanced pathology protocol evaluation should be limited to the true sentinel nodes , which in most studies average about three per patient with uterine malignancy . although the initial capital expenditures needed to incorporate the use of indocyanine green and near - infrared imaging for lymphatic mapping in patients with cervical and uterine cancers might be prohibitively high for some institutions , the near - infrared imaging system could also be used for other purposes , such as evaluating perfusion of bowel or oesophageal anastomoses or delineating anatomy during cholecystectomy.2729 moreover , the alternative to this approach is to continue to use the combination of blue dye and radiocolloid in these patients ( since we have shown that blue dye alone for lymphatic mapping is suboptimal )  . 
although blue dye is quite inexpensive , the use of radiocolloid is not , because its administration requires additional nuclear medicine technicians , nurses , and physicians , and the use of nuclear medicine facilities . 
finally , incorporation of sentinel lymph node biopsy with indocyanine green and near - infrared imaging might be the most cost - effective approach in treating women with gynaecological cancers when compared with complete lymphadenectomy in all patients or lymphatic mapping and sentinel node biopsy with radiocolloid or blue dye.30 this study is limited in its inability to determine the sensitivity , negative predictive value , and oncological outcomes for lymphatic mapping and sentinel node biopsy in women with cervical and uterine cancers . 
 the protocol was designed only to compare indocyanine green and isosulfan blue dye as mapping substances in these patients , and not as a trial to determine the validity the sentinel node concept . 
however , although the combination of blue dye and radiocolloid might have improved detection rates in the standard group , on the basis of the literature , 31 we believe the retrospective data indocyanine green would still be superior in detecting sentinel nodes in women with cervical and uterine cancers . 
surgeons who are new to lymphatic mapping and sentinel lymph node biopsy should perform the procedure followed by complete lymphadenectomy until they are confident that they have achieved proficiency in accurately detecting sentinel nodes . 
finally , as mentioned , the results can only be assumed valid for the specific compound ( ic2000 ) and near - infrared system ( pinpoint ) used in the study . 
however , we believe that studies using other formulations of indocyanine green and other nearinfrared imaging systems will probably yield similar results to our study . the us food and drug administration indications for indocyanine green include only intravenous injection to determine cardiac output , to evaluate perfusion of solid vol 19 october 2018 1401 articles organs , and to perform ophthalmic angiography . 
the manufacturer of ic2000 indocyanine green dye has submitted an application to the food and drug administration on the basis of the results from this study for on - label use of interstitial injection of indocyanine green combined with near - infrared imaging for lymphatic mapping . 
 for women with cervical and uterine cancers , increasing evidence suggests that lymphatic mapping and sentinel node biopsy not only improves detection of disease in regional nodes but also decreases operative morbidity.32 , 33 as lymphatic mapping and sentinel node biopsy become the standard of care in the surgical treatment of cervical and uterine cancers , improving sentinel node detection , particularly detection of bilateral sentinel nodes , will become the focus of research . 
as shown in this study , the incorporation of indocyanine green cervical injection and near - infrared imaging into the mapping improvement over procedure could represent an existing approaches ( ie , blue dye , radiocolloid , or both ) and might in the future become a standard method in these and other solid tumours . contributors mf and nra - r participated in study conception and design , acquisition of data , analysis and interpretation of data , drafting of the report , and critical revision . 
dlu participated in study conception and design , analysis and interpretation of data , and critical revision of the report . declaration of interests mf reports grants from novadaq / stryker , during the conduct of the study , and personal fees from novadaq / stryker , grants from navidea , personal fees from johnson and johnson , and personal fees from genentech , outside the submitted work . 
the other authors declare no competing interests . acknowledgments mf and dlu are supported by the national institutes of health / national cancer institute under award number p30ca016672 . comment formal establishment of national borders does not make for good cancer science , treatment , or care . 
 to get the best out of europe , we all need to be in it and not isolated from it . * josep tabernero , fortunato ciardiello medical oncology department , vall dhebron university hospital , vall dhebron institute of oncology , 08035 barcelona , spain ( jt ) ; seconda universit degli studi di napoli , naples , italy ( fc ) jtabernero@vhio.net fc has served on advisory boards for merck serono , roche , bayer , lilly , astrazeneca , and sano , and has received research grants from roche , bayer , and astrazeneca . 
at the same time , oncology therapy is advancing rapidly ( eg , precision medicine , targeted therapies , and robotic surgery ) , as is radiotherapy technology ( eg , stereotactic body radiotherapy , novel imaging and treatment delivery systems , and proton therapy )  . conventional proton therapy is a promising innovation in cancer care . 
compared with x - ray - based treatment , low - dose radiation to normal tissues is reduced while the dose to tumours remains high , which can lessen the risk of treatment - related toxic e ects and improve cancer outcomes . 
yock and colleagues1 assessed proton therapy for paediatric medulloblastoma , and its use as a treatment for more common malignant diseases , such as prostate , lung , and breast cancers , is being investigated in randomised trials . proton therapy was rst used to treat patients in 1954 , and received us food and drug administration ( fda ) approval in 1988 . 
the amount needed to develop centres often exceeds us$100 million for large multi - room facilities , and the treatment cost to payers might be nearly double the cost of conventional x - ray - based radiotherapy.2 the number of centres providing proton therapy is still far below that of centres o ering other forms of radiotherapy , meaning that many patients have to travel for treatment , leading conventional compared with to transport and temporary housing costs and loss of wages . 
proton therapy has become a standard of care for several cancers , but whether it provides additional bene ts , such as reduced toxic e ects and increased survival , therapies remains unclear . 
 e orts to establish high - quality evidence are supported by professional societies , such as the american society for radiation oncology and nrg oncology , and federal agencies , such as the national institutes of health ( nih ) and the patient - centered outcomes research institute . not having health insurance is a barrier to cancer care in the usa . 
additionally , the routine costs associated with participation in trials are generally too expensive for those who do not have insurance and are often not covered for those who do . 
this situation a ects many patients who are willing to participate in studies of proton therapy.3 for instance , in a federally funded multicentre , randomised , phase 3 clinical intensity - modulated trial of proton therapy versus radiotherapy ( imrt ) for localised prostate cancer ( nct01617161 ) , nearly 30% of eligible participants have restrictive insurance policies or have coverage denied and cannot participate . 
the high frequency of coverage denial severely hinders participant accrual and timely completion of trials , which increases trial costs and skews the study population towards older patients who have medicare coverage for proton therapy . 
thus , despite calls from diverse stakeholders , including patients , physicians , policymakers , and payers , the generation of evidence for proton therapy is being greatly slowed . vol 17 may 2016 comment while patients access to clinical trials has improved over the past 25 years , the high frequency of insurance denial for proton therapy trial participation underscores impediments to receiving advanced therapies and the generation of evidence to support their use . 
the nih revitalization act of 1993 encouraged the inclusion of women and ethnic minorities in nih - sponsored trials , which led to nearly 50% increase in accrual over the subsequent decade . 
for example , inclusion of elderly patients southwest oncology group trials sponsored by the us national cancer increased by 12%.4 institute nevertheless , the policy did not address clinical trial coverage for the substantial proportion of us citizens not eligible for medicare . 
in 2010 , section 2709 of the patient protection and a ordable care act prevented insurers from denying coverage for routine care costs during participation in approved clinical trials beginning in 2014 ( including trials for fda investigational new drug applications and drug trials exempt from these requirements )  . 
of note , section 2709 does not apply to medicaid plans or so - called grandfathered health plans ( ie , all health plans in existence on march 23 , 2010 ) , which still prevent a substantial proportion of people in the usa from participating in these trials . 
with the paucity of clinical data , many payers continue to argue that proton therapy is investigational , even though it has been in use for more than 50 years and has been used in well over 100 000 patients worldwide . despite the legislative e orts to ensure a minimum standard for insurance coverage of patients in clinical trials , how private payers address these obligations di ers between states . 
although some degree of clinical trial coverage is mandated for residents of 38 states and the district of columbia , policies can be ill de ned or non - existent in other states . 
the 2014 guidance by the washington state health technology assessment program deemed that proton therapy should be covered for selected cancers ( eg , paediatric and central nervous system tumours ) , 5 but no provision was made for common cancers , such as prostate and lung cancers , where high - quality evidence is much needed . private insurers have led the way in some assessments of advanced radiotherapy coverage . 
this collaborative engagement led to a strong consensus and improved guidance for clinicians , which led to more judicious use of imrt based on criteria often developed in the absence of level 1 evidence , and resulted in a 17% decrease in imrt use in 1 year and estimated savings of up to us$5 million per year.6 this model of communication between providers and an insurance organisation and ensuing development of a community standard of care could be useful for other advanced technologies where the science is immature , the data are evolving , or both . 
 blue cross blue shield of massachusetts now covers proton therapy for patients who have speci c cancers and are enrolled in prospective clinical studies , including prostate and left - sided breast cancers ( owing to the proximity of the heart ) , which might facilitate timely completion of these studies . in his state of the union address in january , 2016 , president barack obama cited a new moonshot and called for the usa to be the country that cures cancer once and for all . 
nearly two - thirds of patients with cancer receive radiotherapy at some point in their care ; proton therapy is a promising treatment for many of these patients , but comparative trials are overdue . 
in the near term , we ask private and public insurers to cover medical costs for patients enrolled in proton therapy clinical trials , at least for phase 3 or federally funded studies . 
although we do not encourage coverage of expensive therapies with marginal bene ts , the provision of insurance coverage 560 vol 17 may 2016 comment for participants in well designed proton therapy studies is a unique opportunity to generate timely high - quality clinical evidence for some of the most pressing questions in cancer research . anand shah , kelsey i ricci , * jason a efstathiou department of radiation oncology , columbia university medical center , new york , ny , usa ( as ) and department of radiation oncology , massachusetts general hospital , harvard medical school , boston , ma 02114 , usa ( kir , jae ) jefstathiou@partners.org as is a member of the american society for radiation oncology congressional relations subcommittee and chair of the south carolina 5th congressional district health care advisory board . 
jae serves as principal investigator of the partiqol multi - centre randomised phase 3 clinical trial of proton therapy versus intensity - modulated radiotherapy for localised prostate cancer and acknowledges funding support from the federal share of program income earned by massachusetts general hospital ( grant c06 ca059267 ) and the prostate cancer foundation . 
as part of the second phase of the international cancer benchmarking partnership ( icbp ) , the cancer survival in high - income countries ( survmark - 2 ) project aims to provide a comprehensive overview of cancer survival across seven high - income countries and a comparative assessment of corresponding incidence and mortality trends . methods in this longitudinal , population - based study , we collected patient - level data on 39 million patients with cancer from population - based cancer registries in 21 jurisdictions in seven countries ( australia , canada , denmark , ireland , new zealand , norway , and the uk ) for seven sites of cancer ( oesophagus , stomach , colon , rectum , pancreas , lung , and ovary ) diagnosed between 1995 and 2014 , and followed up until dec 31 , 2015 . 
we mapped changes in incidence and mortality to changes in survival to assess progress in cancer control . findings in 19 eligible jurisdictions , 3 764 543 cases of cancer were eligible for inclusion in the study . 
in the 19 included jurisdictions , over 19952014 , 1 - year and 5 - year net survival increased in each country across almost all cancer types , with , for example , 5 - year rectal cancer survival increasing more than 13 percentage points in denmark , ireland , and the uk . 
over the study period , larger survival improvements were observed for patients younger than 75 years at diagnosis than those aged 75 years and older , and notably for cancers with a poor prognosis ( ie , oesophagus , stomach , pancreas , and lung )  . 
progress in cancer control ( ie , increased survival , decreased mortality and incidence ) over the study period was evident for stomach , colon , lung ( in males ) , and ovarian cancer . interpretation the joint evaluation of trends in incidence , mortality , and survival indicated progress in four of the seven studied cancers . 
while truly valid comparisons require differences in registration practice , classification , and coding to be minimal , stage of disease at diagnosis , timely access to effective treatment , and the extent of comorbidity are likely the main determinants of patient outcomes . 
benchmarking international population - based cancer survival differences has proven to be a highly complex but crucial way to develop and assess early - detection strategies , the quality of clinical care , and the management of cancer patients . 
although consistent improvements in cancer survival have been reported in the past two decades , survival differences appear to persist for most cancer sites , motivating policy reforms in specific countries . added value of this study as part of the second phase of the international cancer benchmarking partnership ( icbp ) , the cancer survival in high - income countries ( survmark - 2 ) benchmarks 1 - year and 5 - year net survival by age and period of diagnosis for seven cancers ( oesophagus , stomach , colon , rectum , pancreas , lung , and ovary ) in seven countries ( australia , canada , denmark , ireland , new zealand , norway , and the uk ) , using data from 21 high - quality population - based cancer registries for the period 19952014 , with follow - up until dec 31 , 2015 . 
 high levels of data scrutiny , close interactions with a multidisciplinary group of data providers , epidemiologists , and clinicians , and efforts to extend the set of relevant indicators make this study unique . 
this report builds on previous studies by providing a combined assessment of trends in incidence , mortality , and survival to measure successes in cancer control . implications of all the available evidence we found that cancer survival continues to improve across high - income countries , although international disparities persist even for cancers with poor prognoses . 
the favourable 20 - year stomach , colon , lung ( males ) , and ovarian cancer incidence and mortality trends are probably attributable to the delivery of interventions across the spectrum of cancer control , including effective cancer prevention and treatment . 
 innovative measures of cancer survival will be included in forthcoming papers and made publicly available via an online tool to facilitate the next generation of benchmarking studies . that have sought of studies to comprehensively understand and address international cancer survival variations , including an assessment of four cancers over the period 19952007 in six countries.2 during the second phase of icbp , the cancer survival in high - income countries ( survmark - 2 ) project3 was established to further explore the underlying reasons for observed survival differences across an expanded set of cancer types , with a focus on indicators that inform clinical practice and public health , and engagement with a multidisciplinary group of collaborators and stakeholders . several studies in high - income countries have shown consistent improvements in cancer survival over the past two decades , yet survival differences between countries have been a permanent feature for most cancer sites and continue to persist , albeit to varying extents.2 , 4 , 5 these differences have been interpreted , and in some cases validated , as partly reflecting variations in progress in advancing cancer services , motivating policy reforms across countries.1 however , evolving cancer control plans need to be assessed not only in light of improvements in survival , but also taking into account trends in incidence and mortality to better understand the underlying biological , epidemiological , and clinical processes involved . benchmarking in cancer survival remains a highly complex exercise given the numerous potential factors that might explain observed international variations variations . 
in addition to factors that directly affect patient outcomes , such as stage at diagnosis and treatment , 69 survival can also be influenced by differences in how cancer cases are registered and classified.10 additionally , national and subnational variability in factors linked to the underlying health systems , cancer policy , and clinical practice could all be important drivers . 
only invasive tumours ( behaviour code 3 ) were included , and all borderline ovarian cancers were excluded ( third revision of the icd for oncology codes 8442 , 8451 , 8462 , 8472 , and 8473 )  . we collected patient - level information on the following variables : histology , morphology , basis of diagnosis , stage at diagnosis , and treatment . 
three registries could not provide incidence data for the full 20 - year period ( data were available for new south wales for 19952012 , ireland for 19952013 , and quebec for 20002011 )  . 
given our focus on temporal comparisons of patients diagnosed during 19952014 , data from two canadian jurisdictions were excluded : quebec , because they only had data available from 2000 , and newfoundland and labrador , because linkage of registered cases to vital status information was not systematically carried out before 2005 . 
given the complexities in registration , classifi cation , and differentiation of primary and secondary tumours of the liver , survival comparisons from this cancer site were not included here and will be presented in a separate paper . of all cases eligible for analysis in the 19 jurisdictions , we excluded cases diagnosed on the basis of death certificate only or at autopsy ; those with invalid or missing dates , age , or non - malignant behaviour ; those in patients aged younger than 15 years or older than 99 years at diagnosis ; and second or higher order cancers at the same site ( ie , if a patient had two colon cancers during the study period , only the first would be included )  . national estimates of cancer mortality for the period 19952014 were obtained from the following sources : australian bureau of statistics ( all australian jurisdictions ) , statistics canada ( all canadian jurisdictions ) , the danish health data authority , central statistics office ireland , norwegian institute of public health , new zealand ministry of health , office for national statistics ( wales and england , uk ) , national records of scotland , and the general registrars office for northern ireland . 
all data were submitted through a secured portal at the international agency for research on cancer ( iarc ) and the data were handled according to applicable data protection and privacy laws , rules , and regulations . 
 ethical approval was obtained from each participating registry and from the iarc ethics committee . quality control we subjected each registry dataset to several data quality assessments , which included scrutinising data for specific anomalies , such as instances of negative survival duration ( date of death occurring before date of diagnosis ) ; out - ofrange dates of diagnosis or dates of death , or both ; and invalid vital status codes . 
additionally , every case was checked for consistency in terms of patient sex and sexspecific cancer site ; site and morphology ; age and site ; age and morphology ; and age , site , and morphology . 
we constructed tables including data quality indicators and communicated these to the registries and any issues identified were followed up and discussed in detail via one - to - one interviews between the investigators and registry staff . 
interviews with key staff at the registries were carried out at an early phase of the study ( in parallel with the call for data ) to inform local case finding and ascertainment mechanisms , linkage to vital statistics , and coding and classification practices . 
the overall flow of data , including checks and exclusions , are in the appendix ( p 25 )  . statistical analysis we calculated net survival to estimate population - based cancer survival , which was taken as the survival of patients in a defined resident population if cancer was the only possible cause of death . 
follow - up was available until dec 31 , 2015 , for all patients except for those in ontario , where follow - up was limited to dec 31 , 2014 . we obtained background mortality in the general population of each jurisdiction from lifetables of allcause mortality by sex , single year of age , and calendar year of death during 19952014 . 
complete lifetables were available for all but one juris diction ( prince edward island , canada ) , for which we used a poisson model to interpolate 1 - year intervals from an abridged ( 5 - year ) lifetable . 
we supplemented missing years or ages , or both , in the lifetables for new zealand with data from the human mortality database . we calculated survival estimates at 1 year and 5 years after diagnosis by age group ( < 75 years vs 75 years ) , time period of diagnosis ( ie 199599 , 200004 , 200509 , and 201014 ) , and cancer site for each jurisdiction using pohar perme estimators and the user - written stata command stnet.13 , 14 we did age - standardised survival estimates using inter national cancer survival standard for international association of cancer registries check and conversion program see php ? option = com_content&view = article&id = 72 : iarccrgtools&catid = 68&itemid = 445 for recommendations by the european network of cancer registeries see encr.eu / working - groups - andrecommendations see online for appendix for the human mortality database see vol 20 november 2019 1495 articles weights.15 we used the cohort approach for 199599 , 200004 , and 200509 , and we used the period approach for patients diagnosed in 201014 ( period window : 201214 )  . 
this assumption represents the most extreme scenario to assess the potential maximum ( unrealistic ) effect of inclusion of these cases . we calculated trends in age - standardised cancer incidence and mortality for patients aged 25 years and older using the age - truncated world standard population data16 and expressed per 100 000 person - years . 
because previous analyses have highlighted the importance of survival differences by age , we also presented the results by broad age groups at diagnosis ( < 75 years vs 75 years )  . 
 * data inconsistencies included invalid age , missing or incomplete dates , tumours with non - malignant behaviour , and tumours with invalid morphological or topographical codes . table 1 : number of cancer cases identified and included in analysis 19952014 by cancer site and country role of the funding source the funders had a role in writing of the report and had no role in study design , data collection , data analysis , or data interpretation . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results of the 3 890 934 cancer cases that were eligible for analysis in the 19 jurisdictions , 126 391 ( 32% ) were excluded due to the cancer diagnosis only being based on a death certificate or at autopsy ( 77 578 [ 20% ] ) ; invalid or missing dates , age , or non - malignant behaviour of the cancer ( 4471 [ 01% ] ) ; the patient being younger than 15 years or older than 99 years at diagnosis ( 2438 [ < 01% ] ) ; and second or higher order cancers being present at the same site as the primary cancer ( 41 904 [ 11% ] )  . 
hence , 3 764 543 ( 968% ) of eligible cancer cases were included in the analyses ( table 1 ; appendix p 25 )  . in the most recent 5 - year period of diagnosis ( 201014 ) , the highest 1 - year survival for most cancer sites was in australia , followed by canada and norway ( appendix pp 1112 )  . 
the lowest 1 - year survival was observed for stomach , colon , rectal , and lung cancer in the uk ; and for oesophageal cancer in canada , pancreatic cancer in new zealand , and ovarian cancer in ireland . 
similar patterns were observed for 5 - year survival ( table 2 ) , with consistently higher survival in australia than in the other countries , except for lung ( canada ) and ovarian cancer ( norway ) , and lower survival in the uk , except for oesophageal ( denmark ) and ovarian cancer ( ireland )  . 
the uk includes its four consituents countries : england , scotland , wales , and northern ireland . table 2 : age - standardised 5 - year net survival by cancer site , country , and period of diagnosis 1498 vol 20 november 2019 articles oesophagus stomach colon rectum pancreas lung ovary 5 - year net survival ( % ) australia canada denmark ireland new zealand norway 5 - year net survival ( % ) figure 1 : age - standardised 5 - year net survival by site , country , and period of diagnosis , 19952014 age - standardised net survival is for patients aged 1599 years at diagnosis . 
australia includes new south wales ( 19952012 ) , victoria , and western australia ; canada includes alberta , british columbia , manitoba , new brunswick , nova scotia , ontario , prince edward island , and saskatchewan ; ireland ( 19952013 ) ; the uk includes its four constituent countries : england , scotland , wales , and northern ireland ; all other countries with national data ( 19952014 )  . reduced by a maximum of 06 percentage points across all countries in 201014 . differences in 1 - year and 5 - year survival across jurisdictions within countries were observed over time , with large variations for 201014 found in 5 - year survival for oesophageal cancer in australia ( 26% in victoria vs 19% in new south wales ) , pancreatic cancer in canada ( 13% in manitoba vs 7% in nova scotia ) , and colon cancer in the uk ( 63% in northern ireland vs 57% in wales ; appendix pp 1722 )  . cancer survival increased in all seven countries over the 20 - year study period , and improvements , at least in relative terms , were most substantial for the cancer sites associated with a generally poor prognosis ( oesophagus , stomach , pancreas , and lung ; figure 1 ) , and for patients younger than 75 years at diagnosis ( table 3 ; appendix pp 1314 )  . 
the most pronounced increases in 5 - year survival were observed in denmark for cancers of the colon , with a 166 percentage point absolute increase , and rectum , with a 21 percentage point absolute increase , between the 199599 and 201014 time periods ( table 2 , figure 1 )  . 
the survival gap between countries narrowed over time for 1 - year survival for all cancers except pancreatic cancer ( because of substantial increases in survival in all countries ) , whereas for 5 - year survival the survival gap only narrowed for oesophageal and rectal cancer ( table 2 )  . 
differences in 5 - year survival across countries were greater among patients aged 75 years and older than those younger than 75 years , and the survival gap widened for ovarian cancer in those older than 75 years over the 20 - year period but remained fairly stable for other cancer sites ( tables 3 and 4 )  . both 1 - year and 5 - year survival from oesophageal cancer increased substantially in all countries among patients diagnosed in the period 201014 compared with those diagnosed in 199599 ( table 2 ; appendix pp 1112 )  . 
 comparing the periods 199599 and 201014 , 5 - year survival from oesophageal cancer increased by up to 11 percentage points ( in ireland and norway ) , which was more pronounced in those younger than 75 years at diagnosis ( up to 14 percentage points in ireland and norway ) than in those aged 75 years and older ( up to 7 percentage points in denmark ; tables 3 and 4 )  . 
the uk includes its four consituents countries : england , scotland , wales , and northern ireland . table 4 : age - standardised 5 - year net survival by cancer site , country and period of diagnosis in patients aged 75 years and older vol 20 november 2019 1501 articles oesophagus stomach colon rectum pancreas countries over time ( except in norway ) , incidence has increased ( except for in ireland and australia ; figure 2 ; appendix p 30 )  . improvements in survival from stomach cancer were equally uniform across countries ( table 2 ; appendix pp 1112 )  . 
increases were more pronounced among patients younger than 75 years , and most notably in ireland , where 5 - year survival increased from 20% to 33% over the 20 - year period ( table 3 )  . 
all countries saw concurrent decreases in both incidence and mortality since 1995 ( figure 2 ; appendix p 31 )  . 5 - year survival from colon cancer increased in all countries over 19952014 ( table 2 )  . 
the increases were greater in patients younger than 75 years than among those older than 75 years , with an at least 13 percentage point increase observed in ireland , denmark , and the uk ( table 3 )  . 
slight increases in incidence were observed in norway , denmark , and the uk ( figure 2 ; appendix p 32 )  . cancers of the rectum had the highest survival among the cancers studied , up to 90% for 1 - year survival and 71% for 5 - year survival in 201014 , both in australia ( appendix pp 1112 ) , with the most substantial increases in survival seen among patients younger than 75 years ( table 3 ; appendix pp 1314 )  . 
considerable variations in incidence and mortality were seen across countries ; although mortality decreased in all countries except canada , incidence remained largely stable , except in canada and denmark , where incidence increased slightly ( figure 2 ; appendix p 33 )  . pancreatic cancer had the lowest survival among the studied cancer sites , although survival increases were observed over time in most countries except new zealand ( table 2 ; appendix pp 1112 )  . 
slight increases in pancreatic cancer incidence were seen in all countries , although no appreciable changes were observed in mortality over time ( figure 2 ; appendix p 34 )  . for lung cancer , although survival was highest in canada , with a 5 - year survival of 22% in 201014 , survival increased most in denmark , ireland , and norway , with a 1011 percentage point increase when comparing the periods 199599 with 201014 ( table 2 ; appendix p 35 )  . 
although survival improved for both sexes , incidence , and mortality varied by sex ( appendix p 29 ) ; both incidence and mortality decreased in males , whereas in females incidence increased and mortality remained stable . the highest 5 - year survival for ovarian cancer was observed in norway , followed by australia and denmark , relative change in mortality ( % ) relative change in incidence ( % ) australia canada denmark ireland new zealand norway jurisdictions countries ( figure 2 continues on next page ) 1502 vol 20 november 2019 articles lung ovary with survival ranging from 36% to 46% across countries for diagnoses in 201014 ( table 2 )  . 
following considerable absolute improvements in survival over 19952014 across all countries , including ireland and the uk , the most recent survival estimates in these countries , and in new zealand , remained relatively low at around 3637% . 
 compared with the first phase of icbp , the number of cancer sites analysed has been expanded , including lung , colon , rectal , ovarian , oesophageal , stomach , and pancreatic cancer , and survival improve ments have been notable for cancers associated with worse prognoses and in patients diagnosed when younger than 75 years . 
international differences narrowed across the study period for 1 - year survival after diagnosis for all cancers except pancreatic cancer , whereas at 5 years after diagnosis differences across countries only narrowed for oesophageal and rectal cancer . 
our combined description of trends in incidence , mortality , and survival suggests substantial progress has been made in cancer control across these seven countries for stomach , colon , lung ( in males ) , and ovarian cancer . the uniform improvements in cancer survival in this study are probably the direct consequence of major health care reforms and technological advances that have enabled earlier diagnosis , more effective and tailored treatment , and better patient management than in previous periods . 
for example , rectal cancer had one of the most substantial increases in 5 - year net survival over time , increasing between 9 and 21 percentage points in all seven countries . 
improvements in surgical techniques , including the implementation of total mesorectal excision and new guidelines that include preoperative radiotherapy are among the key changes that have improved patient outcomes.17 improvements in survival were largely seen among younger patients ( aged < 75 years ) and might relate to the relatively wider access to adjuvant chemotherapy and ability of these patients to tolerate more aggressive treatments than older age groups . 
additionally , better diagnosis and staging with new technologies such as pet - ct imaging , alongside greater precision in the selection of patients for targeted therapies on the basis of molecular markers , have probably contributed . 
 in denmark , the substantial increases in survival seen across all cancers , particularly colorectal cancer , might have partly resulted from national health - care reforms in 2007 when cancer became regarded as an acute relative change in mortality ( % ) relative change in incidence ( % ) australia canada denmark ireland new zealand norway jurisdictions countries figure 2 : changes in age - standardised 5 - year net survival against changes in mortality and incidence , 201014 compared with 199599 age - standardised net survival is for patients aged 1599 years at diagnosis , and age - standardised incidence and mortality are for patients aged 25 years and older at diagnosis . 
australia includes new south wales ( 19952012 ) , victoria and western australia ; canada includes alberta , british columbia , manitoba , new brunswick , nova scotia , ontario , and saskatchewan ; ireland ( 19952013 ) ; the uk includes its four constituent countries : england , scotland , wales , and northern ireland ; and all other countries with national data ( 19952014 )  . 
estimates for prince edward island ( canada ) are not shown because of large fluctuations in rates compared with the small number of cases . for the survmark - 2 interactive tool see iarc.fr / survival / survmark life - threatening disease , after which cancer - specific pathways for diagnosis and treatment were accelerated , including reduced waiting times in hospitals and large investments in radio therapy.18 , 19 international differences in access to diagnostic services , screening practices , treatments , patient pathways , and health - care systems , and their effect on survival are being further explored in icbp studies . differences in coding and classification systems and cancer registration practices in different jurisdictions and countries are potential challenges to international population - based comparisons of cancer survival . 
taking the example of staginga principle determinant of cancer survivalthe implementation of common recording systems has been hindered by variations in the availability of clinical information to determine the stage of cancer , the application of different staging guidelines , and differences in the pace of change in diagnostic and treatment practice.20 the validity of the definition of date of diagnosis , accuracy of ascertainment of death , and extent of trace - back of cases first notified by death certificateseg . 
still , an earlier icbp study10 has shown that local registration practices , including the prioritisation of earlier incidence dates and the exclusion of second or higher order tumours , might inflate survival and partly account for survival gaps between jurisdictions . 
however , specific aspects of registration that might influence survival are uncollectable or beyond the control of the registry , such as the completeness of registration , characteristics of patients with cancer who are not included in the registries , and incomplete ascertainment of deaths . 
insights into data collection processes and an in - depth assessment of coding , classification , and registration in collaboration with registry staff , biostatisticians , and clinicians are key to informing future strategies to improve international survival benchmarking . the datasets assembled in this study are unique in several ways . 
stringent protocols for data processing and harmonisation were put in place and extensive exchanges with both registry staff and clinical advisors in each jurisdiction ensured optimal compar ability in the final datasets . 
the resulting survival estimates are analogous to those from previous international studies , 2 , 4 although slight deviations might have occurred through differences in exclusion criteria and methodological approaches ( eg , differences in the diagnostic window for period analyses and cancer definitions )  . this study has several limitations . 
although net survival is not subject to potential errors in cause of death certification , it remains a conceptual metric that is of little use to express the survival of an individual patient with cancer . 
 although we made every effort to ensure data comparability , differences in registration practices , and sources of information available to the individual registries might account for some of the variation in cancer survival seen across countries . 
furthermore , the proportion of cases eligible for analysis varied by country and depended heavily on the proportion of cases of cancer determined by death certificate ( or autopsy ) only ( varying between 23% and 48% for pancreatic cancer , and from 05% to 34% for the remaining cancer sites ) , and other quality control measures such as inconsistencies between dates . 
in new zealand , originally higher proportions of cases diagnosed by death certificate only can be linked to the 1994 cancer registry act that mandated all laboratories to submit new diagnoses of cancer to the national registry . 
because registrations were thus obtained from pathology , hospital discharge , or mortality sources , some clinically diagnosed cases not admitted to a hospital were notified to the registry via death certificates only after the patients had died . 
in this study , an additional assessment of inclusion of cases determined by death certificate onlyunder the extreme assumption that survival equalled 1 dayreduced the 5 - year survival estimates by a maximum of 06 percentage points in the most recent period . 
moreover , data from canada and australia were not national but covered most of their populations ( 76% of canadas population and 70% of australias population ) , which is unlikely to restrict their representativeness . 
such progress in the control of the cancer types studied here , particularly cancers of the stomach , colon , lung ( in males ) , and ovary , can be attributed to the delivery of multiple evidence - based and effective interventions that span the spectrum of cancer control , during the past two decades . contributors ma , mjr , is , and fb conceived the study , contributed to study design and analysis , and wrote the first draft of the manuscript . 
tm - la , tm , gp , jb , hb , dcc , sh , dmp , ps , pcl , and bm contributed to the study design , interpretation of the results , and finalising the report . 
all other authors declare no competing interests . 1504 vol 20 november 2019 articles acknowledgments this study was funded by canadian partnership against cancer ; cancer council victoria ; cancer institute new south wales ; cancer research uk ; danish cancer society ; national cancer registry ireland ; the cancer society of new zealand ; national health service england ; norwegian cancer society ; public health agency northern ireland , on behalf of the northern ireland cancer registry ; the scottish government ; western australia department of health ; and wales cancer network . 
 the authors alone are responsible for the views expressed in this article and they do not necessarily represent the views , decisions , or policies of the institutions with which they are affiliated . 
we thank lucie hooper , samantha harrison , charles norell , shanta keshwala , charlotte lynch , deborah robinson , and irene reguilon of cancer research uk for managing the programme . 
a full list of all investigators can be found in the appendix ( pp 310 )  . correction to lancet oncol 2019 ; 20 : 168190 correction to lancet oncol 2020 ; 21 : 24249 correction to lancet oncol 2020 ; 21 : 27182 j - y , lee kh , ahn m - j , han et al . 
lazertinib in patients with egfr mutation - positive advanced non - smallcell lung cancer : results from the dose escalation and dose expansion parts of a first - in - human , open - label , multicentre , phase 12 study . 
olanzapine 5 mg plus stand ard antiemetic therapy for the prevention of chemotherapy - induced nausea and vomiting ( j - force ) : a multicentre , randomised , double - blind , placebocontrolled , phase 3 trial . 
tumour treating fields in combination with pemetrexed and cisplatin or carboplatin as first - line treatment for unresectable malignant pleural mesothelioma ( stellar ) : a multi centre , single - arm phase 2 trial . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 26170 drilon a , siena s , dziadziuszko r , et al . 
 lancet oncol 2020 ; 21 : 26170in the results section of this article , the median treatment duration for patients with cd74ros1 fusions should have been 146 months ( iqr 72181 ) and the median intracranial progression - free survival in 20 patients with cns disease should have been 77 months ( 95% ci 38193 )  . 
 lancet oncol 2019 ; 21 : 27182in the statistical analysis section of this article , the overall safety - evaluable population should have included safety data from the paediatric phase 1 study startrk - ng patients aged 4920 years . 
this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . correction to lancet oncol 2020 ; 21 : e10 f i e l d s tr e a t i n g ceresoli gl , gianoncelli l , grosso f , on behalf of stellar investigators . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 22232 strm p , kartasalo k , olsson h , et al . 
 this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . vol 21 february 2020 corrections reflection & reaction truly informed the report . 
 honest patient - orientated information on survival for different types of cancer and options for palliative care must be made widely available to choices , ensure according it also demands the development of practice guidelines and standards with followup research to assess their effects . 
at a top policy level , the nci is urged to state - of - the - science convene meeting , include palliative care among its members , and to fund a high - profile research agenda to examine the quality of care , in addition for cures . searching specialist leadership of the nci should promote excellence and help produce the best possible practice guidelines . such guidance could help achieve a paradigm that patients palliative - care needs are assessed early in the course of their disease , while they are undergoing treatment , rather than waiting until death is very near . 
in the uk , increasing integration of hospices the national health service with ( nhs ) have continuity of good palliative care throughout the course of their disease . education and research in palliative techniques and psychosocial support now occur in several units in the uk . but charities cannot expect nhs funding to be standardised across the uk without the parameters of service provision being defined . 
the death in america project should be mirrored in europe , research and identifying more beacons of good practice . irene j higginson * and ilora g finlay facilitating * department of palliative care and policy , kings college london , weston education centre , cutcombe road , london , se5 9rj , uk . 
university of wales college of medicine section of oncology and palliative medicine , velindre hospital , whitchurch , cardiff , cf14 2tl . 1 esteve j , kricker a , ferlay j , parkin dm ( eds )  . 
facts and figures of cancer in the european community international agency for research on cancer commission of the european communities world health organization europe against cancer , 1993 . 2 foley km , gelband h . 
 3 lynn j , teno jm , phillips rs , et al . perceptions by family members of the dying experience of older and seriously ill patients : support investigators study to understand prognoses and preferences for outcomes and risks of treatments . 
 j clin oncol 2001 ; 19 : 20512 . erratum antisense therapy for cancerthe time of truth by burkhard jansen and uwe zangemeister - wittke . lancet oncol 2002 ; 3 : 67283 . the second paragraph on page 677 following the citation for figure 5 inferred that all patients survived beyond 1 year . 
only reproduce with permission from the lancet publishing group . correction to lancet oncol 2016 ; 17 : 74756 correction to lancet oncol 2018 ; 19 : 153042 correction to lancet oncol 2019 ; 20 : 81626 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
lancet oncol 2016 ; 17 : 74756in results , median overall survival should have been median time of death ( after randomisation ) in eleven patients who died from progressive disease . 
prognostic value of end - of - induction pet response after first - line immunochemotherapy for ( gallium ) : follicular secondary analysis of a randomised , phase 3 trial . 
 lancet oncol 2019 ; 20 : 81626 the appendix of this article has been updated as of may 10 , 2019 . published online april 29 , 2019 s1470 - 2045 ( 19 ) 30280 - 3 published online may 10 , 2019 s1470 - 2045 ( 19 ) 30292 - x published online may 10 , 2019 s1470 - 2045 ( 19 ) 30293 - 1 correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
this correction has been made to the online version as of may 29 , 2019 . correction to lancet oncol 2019 ; 20 : 82736 shitara k , iwata h , takahashi s , et al . 
lancet oncol 2019 ; 20 : 82736the appendix of this article has been updated as of may 10 , 2019 . correction to lancet oncol 2019 ; 20 : 84961 eng c , kim tw , bendell j , et al . 
 atezolizumab with or without cobimetinib versus regorafenib previously treated metastatic colorectal cancer ( imblaze370 ) : a multicentre , open - label , phase 3 , randomised , controlled trial . 
this correction has been made to the online version as of may 29 , 2019 and the printed article is correct . correction to lancet oncol 2019 ; 20 : e26273 ngiam ky , khor iw . 
lancet oncol 2019 ; 20 : e26273tables 1 and 2 in this article have been corrected as of april 29 , 2019 . correction to lancet oncol 2019 ; 20 : 297310 cella d , grnwald v , escudier b , et al . 
this update has been made online as of may 29 , 2019 . vol 20 june 2019 e293 corrections correction to lancet oncol 2019 ; 20 : 38393 correction to lancet oncol 2019 ; 20 : 134959 correction to lancet oncol 2019 ; 20 : e64552 oar a , moraes fy , romero y , ilbawi a , yap ml . 
 lancet oncol 2019 ; 20 : 38393in table 2 of this article , data in the any adverse event , n ( % ) row were corrected for the grade 3 and grade 4 columns . 
these corrections have been made to the online version as of dec 2 , 2019 . correction to lancet oncol 2019 ; 20 : 134244 oladeru ot , perni s , williams b . 
 this correction has been made to the online version as of dec 2 , 2019 . correction to lancet oncol 2019 ; 20 : 154455 infante naing a , wong dj , jr , et al . 
the appendix has been updated as of dec 2 , 2019 . vol 20 december 2019 e663 correction correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
 this correction has been made to the online version as of jan 31 , 2018 . vol 19 february 2018 corrections de libris what could be a truly magnificent textbook of intraabdominal oncology . it is difficult to know for whom this book is written . histo - pathologists will probably gain elementary morphological discussions . 
clinicians could benefit from its succinct classifications and broad view , but the clinical content itself is very limited . from little the well - packaged and orderly presentation seems ideal for rapid assimilation and erudite regurgitation . 
that is probably an unkind way of saying that it provides a good introduction that may provide a basis on which to develop sound knowledge . although this book does not represent a complete triumph of form over content ; the form does distract from the intellectual strength of the work . 
unfortunately , it cannot replace the standard atlases on the subject and could not be classified as a textbook either . graham j stewart chemical aspects of photodynamic therapy by r bonnett gordon & breach science publishers ; 2000 30 ; pp 342 isbn 9056992481 this book is written primarily advanced chemistry undergraduates and organic chemistry research students , but the recent advances in the clinical practice of photodynamic therapy ( pdt ) make the text relevant to a much wider audience . 
 i suspect , however , that most doctors reading this book will struggle with the chemistry , even if the chemists do not struggle with the clinical aspects ! the content is up - to - date quite an achievement in this fast moving area and the text is clearly laid out and well referenced . 
it traces the use of light in the treatment of various diseases , from the early enthusiasts such as hippocrates , through the finsen era of phototherapy , up to the first descriptions of haematoporphyrin derivative pdt by kelly and snell in london , this is followed by three key chapters describing the mechanism of pdt that is to say the physics and chemistry of the interactions between light , drugs , and tissue . 
some of these concepts are difficult to grasp , but they are clearly set out and well explained , without too many assumptions about previous knowledge of the subject . most of the remainder of the book deals comprehensively with the chemistry of photosensitising drugs in clinical and preclinical use . 
often , these chapters are either already out of date or wildly speculative in their content , but i was pleased to see that the author had fallen into neither of these traps . 
there is a comprehensive review of the commercialisation of the main drugs under development and website addresses are provided , so that readers can get the very latest information about the drugs described . while this book will not appeal to a wide medical audience , it is certainly essential reading for photochemistry students and recommended for anyone wishing to be involved in the development of pdt . colin hopper errata jefford m , maraskovsky e , cebon j , davis id . 
lancet oncol 2001 ; 2 : 34353 . the first line of the text should have read dendritic cells ( dc ) are bone - marrow - derived antigen - presenting cells . 
in table 2 , the text in the column headed antigen loading should have read hla - restricted melanoma associated antigens or tumour lysate for references 31 and 32 , and hla - restricted melanoma associated antigens for references 33 , 37 , and 38 . 
this correction has been made to the online version as of may 28 , 2012 , and the printed article is correct . vol 13 june 2012 e231 correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections mailbox spindle cell carcinomas are uncommon his the own article tongue are we are intrigued by the statement by borislav dimitrov that most cancers spindle - cell carcinomas.1 we do not have access to the reference given by the author encyclopaedia of human nutrition.2 however , in our own experience and from the literature , it is clear that conventional squamous carcinoma is the most common cancer of the tongue . 
at the tata memorial hospital , mumbai , india , in 1995 , there were cell four carcinomas of the tongue compared spindle with 354 conventional squamous carcinomas . there are few papers on spindlecell carcinomas of the tongue in the literature , which is line with the fact that they are uncommon . 
to our knowledge , the biggest series on spindle cell carcinomas of the oral cavity was studied by ellis and corio.3 they analysed 59 cases , 12 of which tongue . 
oral surg 1980 ; 50 : 523534 . clinical testing of ukrain some remarks in the letter about ukrain in the lancet oncology ( dec 2000 ) by farrugia and slevin1 are based upon a misunderstanding , especially the assertion that we , as the producers of ukrain , are unable or unwilling to take the opportunity for a sober assessment of the drug . 
 the drug we agreed immediately to the proposal for a clinical study at st bartholomews hospital and agreed to supply free of charge . however , we assumed that a clinical study at a major european teaching hospital would be carried out according to good clinical practice ( gcp ) with independent monitoring , which is a requirement of gcp . 
 followed most of the clinical studies carried out on ukrain so far have taken place outside the european union and while have investigators guidelines of gcp the studies have been criticised because not all the formalities were observed . 
 we were therefore unable understand why farrugia and slevin were unwilling to carry out the study according to gcp with independent monitoring , a precondition which we took for granted would be met at a major european teaching hospital . 
 we would like to emphasise that we are most willing for an objective , independently monitored study accordance with gcp to be carried out on ukrain , that we are prepared to supply the drug free of charge for such a study and that we hope that the study proposed by farrugia and slevin can in fact take place . 
lancet oncol 2000 ; 1 : 204 . authors reply the proposed study , which we outlined in our letter , was in keeping with standard practice for phase ii studies and had the approval of our institutions ethics committee . 
the issue of an independent monitoring committee was never raised by nowicky and we would have no objection to this , if the company would bear the cost , although it is not a routine part of phase ii studies . it was the need for an objective assessment of this compound ( which as he rightly says , is lacking in all the clinical papers reported by nowicky and his colleagues ) , which prompted us to suggest this study . we intended to subject ukrain to the same assessment that any other anti - cancer agent would receive within the context of a phase ii study . 
it seems to us that the issue of gcp is a red herring designed to prevent the study taking place and to us why nowicky decided to withdraw his support . david farrugia * , maurice l slevin * cheltenham hospital , cheltenham , gloustershire gl53 7an , uk . 
not to be reproduced without permission of the lancet . correction to lancet oncol 2016 ; 17 : 74756 correction to lancet oncol 2018 ; 19 : 153042 correction to lancet oncol 2019 ; 20 : 81626 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
lancet oncol 2016 ; 17 : 74756in results , median overall survival should have been median time of death ( after randomisation ) in eleven patients who died from progressive disease . 
prognostic value of end - of - induction pet response after first - line immunochemotherapy for ( gallium ) : follicular secondary analysis of a randomised , phase 3 trial . 
 lancet oncol 2019 ; 20 : 81626 the appendix of this article has been updated as of may 10 , 2019 . published online april 29 , 2019 s1470 - 2045 ( 19 ) 30280 - 3 published online may 10 , 2019 s1470 - 2045 ( 19 ) 30292 - x published online may 10 , 2019 s1470 - 2045 ( 19 ) 30293 - 1 correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
this correction has been made to the online version as of may 29 , 2019 . correction to lancet oncol 2019 ; 20 : 82736 shitara k , iwata h , takahashi s , et al . 
lancet oncol 2019 ; 20 : 82736the appendix of this article has been updated as of may 10 , 2019 . correction to lancet oncol 2019 ; 20 : 84961 eng c , kim tw , bendell j , et al . 
 atezolizumab with or without cobimetinib versus regorafenib previously treated metastatic colorectal cancer ( imblaze370 ) : a multicentre , open - label , phase 3 , randomised , controlled trial . 
this correction has been made to the online version as of may 29 , 2019 and the printed article is correct . correction to lancet oncol 2019 ; 20 : e26273 ngiam ky , khor iw . 
lancet oncol 2019 ; 20 : e26273tables 1 and 2 in this article have been corrected as of april 29 , 2019 . correction to lancet oncol 2019 ; 20 : 297310 cella d , grnwald v , escudier b , et al . 
this update has been made online as of may 29 , 2019 . vol 20 june 2019 e293 corrections published online december 11 , 2017 s1470 - 2045 ( 17 ) 30914 - 2 see articles page 27 neoadjuvant chemotherapy in breast cancer : more than just downsizing the early breast cancer trialists collaborative group ( ebctcg ) has established a new milestone in evidencebased treatment for early breast cancer . 
through longstanding collaboration , mutual trust , and data transparency , they have gathered individual patient data for 4756 women randomly allocated in ten trials to either neoadjuvant chemotherapy ( nact ) or adjuvant chemotherapy , with a median follow - up of 9 years ( iqr 514 )  . 
the results of this meta - analysis , 1 published in the lancet oncology , substantiate that nact results in higher rates of breast - conserving therapy than does adjuvant chemotherapy ( rate ratio 128 [ 95% ci 122134 ] ) , without compromising on distant recurrence , breast cancer survival , or overall survival . 
 much emphasis is given by the authors to an increase in local recurrence in the nact group ( 15 year absolute increase of 55% [ 95% ci 2486 ] )  . 
the metaanalysis by mieog and colleagues2 showed no significant difference in local recurrence between patients receiving breast - conserving surgery after nact and breastconserving surgery followed by adjuvant chemotherapy , even with inclusion of those receiving nact that were initially scheduled for mastectomy . in the meta - analysis by the ebctcg , 1 nact led to response of the primary tumour , which undoubtedly led to concomitant downstaging of the axillary lymph nodes . 
 studies3 , 4 have shown that pathological complete response ( pcr ) of the axilla is achieved in 4175% of patients with her2 - positive or triple - negative cancer lymph node dissection receiving nact . 
especially among patients with an ultrasound - positive or cytological - positive axilla who had a clinical response with downstaging to a negative axilla , controversy still exists regarding the timing and accuracy of nodal staging with sentinel lymph node biopsy.5 , 6 several studies have addressed the accuracy of nodal staging after nact and current consensus is that sentinel lymph node biopsy after nact in patients with initial positive axilla is considered accurate if at least three or more sentinel nodes are detected and examined.6 although the willingness of surgeons to omit axillary lymph node dissection or radiotherapy of the axilla in patients with complete response to nact is high , 7 no studies have yet investigated locoregional outcomes . 
a randomised phase 3 trial8 is ongoing to assess the role of axillary radiotherapy versus no axillary radiotherapy in patients who converted to pathologically node - negative disease after nact . 
 improvements as was shown in the ebctcg meta - analysis , patients with high - grade , hormone receptor - negative tumours were most likely to achieve a complete clinical response of the primary tumour after nact . 
with the introduction of targeted therapies and improved systemic strategies , substantial pcr have been seen in the past decade , especially in patients with her2 - positive or triple - negative breast cancers . 
several trials have reported consistently high pcr proportions of up to 83% among her2positive , hormone receptor - negative cancers treated preoperatively with combination chemotherapy and ( dual ) targeted anti - her2 agents.9 these complete responders are offered routine breast cancer surgery similar to patients who did not receive nact . 
 several groups are investigating the accuracy of core needle biopsies in the marked area to establish pcr after neoadjuvant treatment , in either those with radiological complete response ( micra study ; trialregister.nl , number ntr6120 ) or those with her2 - positive or triple - negative disease with partial or complete response ( nct02455791 )  . 
on the basis of initial findings of high accuracy of core needle biopsies in small studies , single - arm studies have started recruitment to establish long - term outcomes for omission of breast surgery ( nct02945579 ) .9 , 10 with the evidence generated from this meta - analysis , patients with large tumours can be recommended to have nact and subsequent breast - conserving surgery depending on response assessment . 
time to stop operating on breast cancer patients with pathological complete response ? eur j surg oncol 2013 ; 39 : 92430 . 10 van la parra rf , kuerer hm . 
 breast cancer res 2016 ; 18 : 28 . tumour infiltrating lymphocytes in breast cancer : increasing clinical relevance the immune microenvironment is now recognised as crucial in the treatment of cancer . 
the tumour immune infiltrate has been noted to be associated with better outcomes in her2 - positive breast cancer and triple - negative breast cancer ( tnbc ) , in both the early - stage and the advanced disease setting.1 , 2 incorporating the quantity of the pre - existing immune response with other prognostic clinical pathological factors , such as tumour size and nodal status , will allow clinicians to better estimate long - term survival after breast cancer diagnosis.3 such data will help clinicians improve their treatment recommendations and allow us to design clinical trials of novel treatments for the subgroups that need the most improvement in survival . in the lancet oncology , carsten denkert and colleagues4 have assessed the predictive and prognostic effect of the concentration of tumour - infiltrating lymphocytes ( tils ) , assessed by use of pretreatment haematoxylin and eosin ( h&e ) stained slides of core biopsies , from patients enrolled in six randomised trials investigating neo - adjuvant treatment in breast cancer.4 3771 patient samples were assessed , which constituted the largest pooled analysis on the effect of tils in the neoadjuvant setting to date . 
the authors confirmed the importance of til quantity in the prediction of pathological complete response , independent of breast cancer subtype , and pathological complete response was strongly associated with a better prognosis ( disease free - survival ) in patients with tnbc and her2 - positive breast cancer , but not in a small luminalher2 - negative subgroup . 
 published online december 7 , 2017 s1470 - 2045 ( 17 ) 30905 - 1 see articles page 40 vol 19 january 2018 comment editorial for the grail website see liquid cancer biopsy : the future of cancer detection ? this years jp morgan annual healthcare conference ( jan 1115 , 2016 ) in san francisco , ca , usa , saw the announcement of a new biotechnology company called graila spino from illumina ( san diego , ca , usa ; one of the worlds largest diagnostics companies )  . 
chaired by the illumina chief executive o cer jay flatley , and with a science advisory board headed by jos baselga ( memorial sloan kettering cancer center , new york , ny , usa ) , grail declared its mission to be the early detection of cancer in asymptomatic individuals through a blood screen . 
 the notion of cancer detection by liquid biopsy is not a new concept : indeed , many other companies are also developing blood - based tests to monitor cancer progression or screen high - risk asymptomatic individuals . 
however , such tests to date have focused on speci c cancer types , rather than a single test to detect all aysmptomatic cancers based on circulating tumour dna ( ctdna )  . 
is this objective possible ? and what are the wider implications for patients with cancer ? the presence of ctdna in the blood of patients with cancer is a well - recognised phenomenon and increasingly well - characterised in many cancers . 
but increased sensitivity can lead to increased genetic noise , which in turn , can make it di cult to di erentiate between tumour - associated dna mutations and non - tumour - associated dna mutationsleading to an increased risk of false positives . 
crucially , there are also other questions to address , such as what exactly the test would detect and what it could di erentiate betweeneg , not all cancers are associated with discrete and consistent early genetic mutations and many have multiple mutations that can arise at any disease stage in an unpredictable manner . 
rather , research has shown that ctdna concentrations are not only directly correlated with tumour burden , but also with ease of transit into the bloodstream overcoming obstacles such as the bloodbrain barrier or mucinous tissues . 
finally , any new diagnostic test must undergo clinical validationa necessary step for regulatory approval and far from trivial . another issue is what clinicians and the public will do with the information from a pan - tumour test . 
 overtreatment can severely worsen quality of life ; for example , present guidelines in several parts of the world no longer advocate prostatectomy on the basis of screening results and instead recommend watch - and - wait strategies . 
thus , if a universal cancer test shows a true positive , should the individual be treated immediately ? furthermore , if a positive result was found in a population - based screening programme with a universal marker , what would be the implications for obtaining health insurance for asymptomatic patients who might not need treatment for years , or at all ? and a further paradox could arise for those cancers detected that have no curative treatment . 
no matter how early some cancers are found and what treatment options are available to palliate symptoms , is the trade - o between early detection and psychological distress really a desired outcome ? the use of venture capitalists and tight timelines in grails undertaking re ects a growing trend in clinical and scienti c research of attacking a speci c scienti c or clinical problem with massive resourcesabout us$100 million in this casecombined with public demand for rapid solutions . 
ambition in some cases exceeds the realities and feasibility of a solution , and projects can become too narrowly focused on speci c avenues of research in an attempt to meet deadlines . 
 it is possible that a focus on ctdna over - and - above other biomarkers and networks in tumour biology , such as immune signatures , proteomes , kinomes , microbiomes , and other multifactorial interactions in the tumour microenvironment and host response , might be an oversimpli cation . 
 the lancet oncology vol 17 february 2016 head and neck surgery recommendations during the covid - 19 pandemic we read the recent international consensus recommendations from hisham mehanna and colleagues1 in the lancet oncology regarding head and neck surgical practice in the setting of resource constraint due to the covid - 19 pandemic interest . 
the monograph characterised treatment of advanced head and neck cancer with do not delay surgery ; operate within 4 weeks of diagnosis , while adopting a more permissive policy toward t1t2 n0 oral cancer and t1 n0 laryngeal cancer : do not delay surgery beyond 8 or 12 weeks . 
although it seems logical to assign high treatment priority to advanced tumours in a setting of resource constraint , 2 the limited data testing the precept do not fully support these recommendations . head and neck squamous cancers progress at a rate that can be measured in the course of typical clinical practice.3 node progression due to prolonged time to treatment initiation replaces stage iii with stage iiiiv cancer . 
the survival impact of such progression is reflected in the staging system.4 in a setting of resource constraint the crucial issue should be consideration of which outcome is most affected by prolonged time to begin treatment . 
 which is more detrimental to survival : t1 n0 progressing to t1 n1 or t3 n2b developing greater node burden ? murphy and colleagues5 addressed this question for squamous cancers . 
 a treatment delay of 3160 days adversely affects survival for stage iii head and neck cancer ( hr 117 ; 95% ci 112123 ) , but not stage iii - iv ( 102 ; 099107 )  . 
a similar relation exists for longer delays of 6190 days for early stage ( hr 154 ; 95% ci 141168 ) and advanced stage ( 108 ; 102114 ) squamous cancer . 
although it seems logical to operate on a patient soon to become formally unresectable or develop more advanced nodal disease , the data suggest that stage iii patients ( with a more favourable prognosis before progression ) will derive greater benefit . the covid - 19 pandemic creates challenges in the management of patients with head and neck cancer . 
 j clin oncol 2016 ; 34 : 16978 . vol 21 september 2020 e416 correspondence correction to lancet oncol 2019 ; 20 : 155665 correction to lancet oncol 2019 ; 20 : e658 correction to lancet oncol 2020 ; 21 : e31729 bertelsen ca , neuenschwander au , jansen je , et al . 
lancet oncol 2019 ; 20 : 155665in this article , two patients ( one in the control group and one in the complete mesocolic excision group ) were incorrectly classified as not having recurrences , due to an error in data extraction . 
 the incorrect data have been updated in the summary findings , the results , figures 2a and 2c , table 3 , supplementary figures 2c and 2f in the appendix , and the discussion . 
complete mesocolic excision for colon cancer : is now the time for a change in practice ? lancet oncol 2019 ; 20 : 147476in this comment , the cumulative incidence of recurrence in each group has been amended , owing to these data being corrected in the linked article by bertelsen and colleagues . 
lancet oncol 2019 ; 20 : e658 in this correspondence , the absolute in risk of recurrence reduction has been amended , owing to this being corrected in the linked article by bertelsen and colleagues . 
this correction has been made to the online version as of aug 3 , 2020 . correction to lancet oncol 2020 ; 21 : e33036 cooney tm , cohen jk , guimaraes cv , et al . 
these corrections have been made to the online version as of aug 3 , 2020 . vol 21 august 2020 e372 corrections comment published online july 4 , 2013 s1470 - 2045 ( 13 ) 70300 - 0 see articles page 834 dose - intensive cisplatin for hepatoblastoma : have you heard ? although survival rates for paediatric cancer have improved greatly during the past four decades , outcomes for children diagnosed with metastatic solid tumours have barely changed . 
unfortunately only about a third of newly diagnosed patients are amenable to resection at diagnosis.1 neoadjuvant chemotherapy can render tumours in many of these patients resectable , but typically a quarter to a third of such patients might never get to resection . 
about a quarter of newly diagnosed patients present with metastatic disease and typically have had survival rates less than 30%.1 whether these metastatic patients have better outcomes if their pulmonary disease is eradicated by chemotherapy or by surgical resection has never been formally studied and is not clear or known . in the lancet oncology , jzsef zsiros and his siopel colleagues2 are to be congratulated for their report of improvement in outcome of patients with highrisk hepatoblastoma , many of whom had pulmonary metastases . 
3 - year event - free survival was 76% ( 95% ci 6587 ) in the 62 patients studied ( 77% , 95% ci 6390 , in the 39 patients with metastasis )  . 
because cisplatin is thought to be the most active drug in this disease , the investigators used a novel , well designed therapeutic schema that incorporated weekly dose - dense cisplatin chemotherapyrevisiting an old basic tenet of chemotherapy administration that has never been fully evaluated in paediatric malignancies.3 the use of dose intensi cation of chemotherapy has had some success in adult malignancies but has been used rarely in paediatric cancers.4 interval compression of chemotherapy has been shown to be e ective in acute myeloid leukemia and ewings sarcoma , although with substantial costs and burden of care , and is now being explored for rhabdomyosarcoma.5 , 6 trials in patients with osteosarcoma have shown positive bene ts in some trials but no e ect in others.7 a previous hepatoblastoma trial from the childrens intensify oncology group ( p9645 ) 8 attempted to platinum delivered therapy by alternating cisplatin and carboplatin on an every 2 week schedule . 
ultimately , this regimen was inferior to the standard control group , perhaps because of decreased dose intensity of cisplatin . the siopel - 4 trial seems to be a success . 
zsiros and colleagues correctly point out the limitations of this study being a single arm trial that compared outcomes with historical results and therefore needing further study before the approach can be adopted as standard of care . 
the only statistical criterion the study met was that it did not exceed the number of expected serious adverse events , although 18 occurred , which seems quite generous for this sample size . 
this result is consistent with some studies in adults that have used a similar approach and might be regarded as acceptable.7 however , febrile neutropenia occurred in 71% of patients and four patients had toxic deaths ( two from infection , one from surgical bleeding , and one with tumour bleeding )  . 
since ototoxocity is di cult to measure , notoriously under - reported , and can progress vol 14 august 2013 comment published online july 1 , 2013 s1470 - 2045 ( 13 ) 70324 - 3 see articles page 843 over time , the question remains as to what hearing function these very young patients will have in the long run and whether this loss is an acceptable price to pay for the survival rates observed . 
lastly , during the three cycles of weekly cisplatin therapy , patients typically had average cumulative delays of 10 days ( range 4 to 63 days ) , which resulted in dose reductions in 9% of the initial chemotherapy block a cycles . 
this outcome somewhat contradicts the study conclusion that dose intensity was the reason for improvement , since the outstanding results were even seen in patients who had delays and reductions in therapy ( unless all patients exceeded the dose - density threshold )  . the entire importantly , international paediatric oncology community , including europe , japan , and south and north america , are now working together to create uni ed approaches to liver tumour classi cation and treatment and there are plans for a single forthcoming trial . 
as exciting as these results are , they emphasise the urgent need for new drugs that hold the promise of a cure with acceptable long - term side - e ects . muna qayed , * howard m katzenstein emory university school of medicine and the a ac cancer center of childrens healthcare of atlanta , atlanta , ga , usa ( mq ) ; and vanderbilt university school of medicine and the monroe carell jr childrens hospital at vanderbilt , nashville , tn 37232 - 6310 , usa ( hmk ) howard.katzenstein@vanderbilt.edu we declare that we have no con icts of interest . trobaugh - lotrario ad , katzenstein hm . 
 pediatr blood cancer 2012 ; 59 : 80912 . zsiros j , brugieres l , brock p , et al , for the international childhood liver tumours strategy group ( siopel )  . 
dose - dense cisplatin - based chemotherapy and surgery for children with high - risk hepatoblastoma ( siopel - 4 ) : a prospective , single - arm , feasibility study . 
extragonadal germ - cell tumours are more common in children than in adults ; many patients are very young , with tumours localised to abdominal or pelvic sites that might be di cult to eradicate . 
presacral lesions containing malignant germ - cell tumor elements , such as yolk sac tumours , are noted later in the rst years of life.1 although most benign neonatal sacrococcygeal tumours can be treated with resection and observation , malignant tumours require a multidisciplinary approach including chemotherapy with platinum - based compounds and surgery . 
survival rates of 8090% have been achieved with this method.24 but surgery , which is essential to survival , is often very di cult to do in these young patients . 
longterm longitudinal studies , after initial surgery , have shown that patients are at risk of developing neurological de cits such as bowel and urinary incontinence.5 , 6 there are two basic strategies for treating sacrococcygeal tumours with malignant elements : resection , followed by adjuvant chemotherapy4 or neoadjuvant chemotherapy before resection.2 but refractory disease and recurrence are possibilities . 
patients in this trial7 who had received previous intensive therapy , and whose tumours were refractory or recurrent , received 792 vol 14 august 2013 correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections in china ( nct03739944 ) , which will enrol 700 patients allocated to laparoscopic radical hysterectomy or trachelectomy , or laparotomic radical hysterectomy or trachelectomy . 
both studies have planned to assess the long - term evaluation of quality of life , the results of which will hopefully provide relevant findings . we declare no competing interests . * gabriella ferrandina , giacomo corrado , giovanni scambia gabriella.ferrandina@gmail.com fondazione policlinico universitario a gemelli , irccs , uoc di ginecologia oncologica , dipartimento per la salute della donna e del bambino e della salute pubblica , rome , italy ( gf , gc , gs ) ; and universit cattolica del sacro cuore , istituto di ginecologia e ostetricia , rome 00168 , italy ( gf , gs ) frumovitz m , obermair a , coleman rl , et al . 
quality of life in patients with cervical cancer after open versus minimally invasive radical hysterectomy ( lacc ) : a secondary outcome of a multicentre , randomised , open - label , phase 3 , non - inferiority trial . 
the lacc trial : has minimally invasive surgery for early - stage cervical cancer been dealt a knockout punch ? int j gynecol cancer 2018 ; 28 : 124850 . impact of the covid - 19 pandemic on the symptomatic diagnosis of cancer : the view from primary care the entire landscape of cancer management in primary care , from case identification to the management of people living with and beyond cancer , is evolving rapidly in the face of the coronavirus disease 2019 ( covid - 19 ) pandemic.1 in a climate of fear and mandated avoidance of all but essential clinical services , delays in patient , population , and health - care system responses to suspected cancer symptoms seem inevitable . screening , case identification , and referral in symptomatic cancer diagnosis have all been affected by the covid - 19 pandemic . 
uk national cancer screening programmesaccounting for approximately 5% of all cancer diagnoses each yearhave been suspended.2 consequently , early diagnoses from screening will be delayed and symptom - based diagnosis of cancer will become more important.3 unfortunately , postponing screening sends a message to the public and primary care that cancer can wait . timely presentation to primary care of patients with symptoms is driven by a combination of appraising symptoms as warranting attention , perceived or actual ability to consult a health - care professional , perceived consequences of seeking help , and priority over competing goals.4 it is probable that patients with well recognised red flag symptoms , such as a new lump or rectal bleeding , will continue to present to primary care . 
 with covid - 19 at the forefront , however , vague cancer symptoms such as fatigue , change in bowel habit , and weight loss might be dismissed by the patient as trivial.5 respiratory symptoms , including persistent cough , might be attributed to covid - 19 and not acted on . 
 patients might be reluctant to present because of fear of interacting with others , limited capacity to use video or teleconsultations , and concerns about wasting the doctors time.6 , 7 for family doctors , the covid - 19 pandemic affecting all aspects of normal working life , including a reduced workforce due to illness and self - isolation , and the reduced availability of appointments and investigations in primary and secondary care . 
remote consulting might also be less suited to vulnerable patients and individuals low socioeconomic backgrounds than to patients from high socio economic settings , compounding inequalities already apparent in early cancer diagnosis.8 if patients with cancer symptoms from published online april 30 , 2020 s1470 - 2045 ( 20 ) 30242 - 4 for more on the challenges of cancer care during the covid - 19 pandemic see editorial lancet oncol 2020 ; 21 : 603 for more on the impact of covid - 19 on cancer diagnosis see comment page 750 748 vol 21 june 2020 comment do present to primary care , there is no consensus on how they should be managed during the pandemic , or safety - netted . 
when patients are referred , they are likely to be triaged or delayed.9 for example , the cancellation of all but emergency endoscopy will inevitably prolong the time to diagnosis of gastrointestinal cancers . management and follow - up of patients with cancer is also affected by the covid - 19 pandemic . 
many patients with cancer , especially those under going chemotherapy , radical radiotherapy , and immuno therapy , are at greater risk from the symptoms and sequelae of covid - 19 . 
the national health service guidelines state that patients will want to discuss whether the benefits of continuing active cancer treatment outweigh the risks of potentially being seriously unwell if they contract covid - 19 , which is a role that could well fall to primary care.9 the uk cancer charity macmillan cancer support reports that a quarter of calls to its support line are from patients with cancer who are anxious about covid - 19.10 although cancer charities provide a vital support role , primary care needs to support the physical and mental health of patients for whom potentially lifesaving cancer treatments are being postponed . cancer treatments are a priority in the healthcare system , but as health - care become increasingly occupied with caring for patients with covid - 19 , these patients will inevitably take precedence . 
in this situation , the psychological effect on patients and clinical staff will be enormous . the covid - 19 pandemic has implications for primary care and the crisis has highlighted potential solutions for dealing with future global health threats . 
if done well , remote consulting could benefit previously underserved patient populations ( ie , individuals living in remote areas )  . behavioural interventions to encourage the timely symptomatic diagnosis of cancer are important . 
public awareness campaigns should signal that early helpseeking is welcome and legitimate , and might use social media and community networks that have grown in response to covid - 19 . 
clinicians should be aware of so - called diagnostic overshadowing from covid - 19 and remember that patients might have markedly delayed presentation already and need additional support navigating the next steps in terms of their referral and safety - netting . if cancer is suspected , clinicians should not be deterred from referring patients urgently because of covid - 19 or other future global health threats . 
 biomarker and machine - learning approaches might support prioritisation of patients who are at greatest risk , diverting health - care resources towards managing patients who are seriously ill . when patients are diagnosed with cancer , or are living with or beyond cancer , providers of primary care might have to accept enhanced roles in supporting decisions on cancer treatment , palliative care , and advanced planning around resuscitation and preferred places of care . when normal service resumes at a population and health - service level , there will be a huge backlog of patients with potential cancer symptoms needing urgent assessment . 
this research is linked to the cantest collaborative , which is funded by cancer research uk ( c8640 / a23385 ) , of which rdn is an associate director and ses is a co - investigator . 
differences in cancer awareness and beliefs between australia , canada , denmark , norway , sweden and the uk ( the international cancer benchmarking partnership ) : do they contribute to differences in cancer survival ? brit j cancer 2013 ; 108 : 292300 . llanwarne n , newbould j , burt j , campbell jl , roland m . 
covid - 19 and long term conditions : what if you have cancer , diabetes , or chronic kidney disease ? bmj 2020 ; 368 : m1174 . fewer cancer diagnoses during the covid - 19 epidemic in the netherlands published online april 30 , 2020 s1470 - 2045 ( 20 ) 30265 - 5 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on may 4 , 2020 for more on the challenges of cancer care during the covid - 19 pandemic see editorial lancet oncol 2020 ; 21 : 603 for more on the impact of covid - 19 on cancer diagnosis see comment page 748 see online for appendix the dreadful consequences of coronavirus disease 2019 ( covid - 19 ) put an unprecedented pressure on health - care services across the globe.1 the netherlands , a country with 174 million inhabitants that provides its citizens with universal access to essential healthcare serviceswith the general practitioner as the gatekeeper to secondary careis no exception in this regard . the first patient with covid - 19 in the netherlands was confirmed on feb 27 , 2020 , in the southern part of the country.2 thereafter , the disease spread rapidly throughout the country . 
subsequently , strict social distancing policies were implemented by the dutch government as of march 15 , 2020 , to mitigate the spread of covid - 19.3 , 4 all sites ( excluding skin cancer ) skin cancers ( excluding basal cell carcinoma ) first conrmed case of covid - 19 in the netherlands nationwide implementation of strict social distancing policies and temporary halt of national cancer screening programmes public awareness campaign about lesser cancer diagnoses 39% 40% 6 jan 13 jan 20 jan 27 jan 3 feb 10 feb 17 feb 24 feb 2 m arch 9 m arch 16 m arch 23 m arch 30 m arch 6 april calendar week in 2020 figure : number of cancer diagnoses by week in the netherlands in the period between jan 6 , 2020 ( calendar week 2 ) and april 12 , 2020 ( calendar week 15 ) basal cell carcinoma of the skin is not included in the statistics . 
the point estimates for the change in cancer diagnoses per calendar week are based on the mean total number of cancer diagnoses in the calendar weeks from 2 to 8 ; that is , the period before the covid - 19 outbreak in the netherlands . 
data from the nationwide netherlands cancer registry in the period between feb 24 , 2020 , and april 12 , 2020which are based on initial case ascertain ment through pathological cancer notifications from the nationwide network of histopathology and cytopathologyshow that there is a notable decrease in cancer diagnoses when compared with the period before the covid - 19 outbreak . 
this effect was most pronounced for skin cancers ( figure ) and observed across all age groups and geographical regions , and almost all cancer sites ( appendix )  . 
first , individuals with potential , non - specific symptoms of cancer might have barriers to consulting a general practitioner , including moral concerns about wasting the general practitioners time for non - covid - 19 - related symptoms , assumptions about insufficient capacity for essential noncovid - 19 - related health - care services , and anxiety about acquiring covid - 19 in a health - care setting . 
a general practitioner might , therefore , postpone initial investigations for symptoms that do not immediately hint towards a potential cancer diagnosis , resulting in delayed or postponed hospital referrals . 
third , hospitals might have postponed diagnostic evaluation or have longer turnaround times for diagnostic evaluation because many hospital - based resources are being allocated to tackle covid - 19 . 
lastly , national screening programmes for breast , colorectal , and cervical cancer are temporarily halted as of march 16 , 2020 , to alleviate the demand on the health - care system due to covid - 19 . 
we designed the portec - 3 trial to investigate the bene t of adjuvant chemoradiotherapy compared with radiotherapy alone for women with high - risk endometrial cancer . methods portec - 3 was a multicentre , open - label , randomised , international trial . 
women with high - risk endometrial cancer were randomly allocated ( 1 : 1 ) to radiotherapy alone ( 486 gy ) in 18 gy fractions ve times a week or chemoradiotherapy ( two cycles concurrent cisplatin 50 mg / m and four adjuvant cycles of carboplatin area under the curve [ auc ] 5 and paclitaxel 175 mg / m ) using a biased coin minimisation procedure with strati cation for participating centre , lymphadenectomy , stage of cancer , and histological type . 
at 12 and 24 months , global health or quality of life was similar between groups , whereas physical functioning scores remained slightly lower in patients who received chemoradiotherapy compared with patients who received radiotherapy alone . 
at 24 months , 48 ( 25% ) of 194 patients in the chemoradiotherapy group reported severe tingling or numbness compared with 11 ( 6% ) of 170 patients in the radiotherapy alone group ( p < 00001 )  . 
grade 2 or worse adverse events were found during treatment in 309 ( 94% ) of 327 patients in the chemoradiotherapy group versus 145 ( 44% ) of 326 patients in the radiotherapy alone group , and grade 3 or worse events were found in 198 ( 61% ) of 327 patients in the chemoradiotherapy group versus 42 ( 13% ) of 326 patients in the radiotherapy alone group ( p < 00001 ) , with most of the grade 3 adverse events being haematological ( 45% )  . 
at 12 and 24 months , no signi cant di erences in grade 3 or worse adverse events were found between groups ; only grade 2 or higher sensory neuropathy adverse events persisted at 24 months ( 25 [ 10% ] of 240 patients in the chemoradiotherapy group vs one [ < 1% ] of 247 patients in the radiotherapy alone group ; p < 00001 )  . interpretation despite the increased physician and patient - reported toxicities , this schedule of adjuvant chemotherapy given during and after radiotherapy in patients with high - risk endometrial cancer is feasible , with rapid recovery after treatment , but with persistence of patient - reported sensory neurological symptoms in 25% of patients . 
we await the analysis of primary endpoints before nal conclusions are made . funding dutch cancer society , cancer research uk , national health and medical research council , project grant , cancer australia grant , italian medicines agency , and canadian cancer society research institute . copyright the author ( s )  . 
 we identi ed eight relevant publications , mostly small studies of which most used a sequential schedule with various chemotherapy drugs , and only two trials assessed combined chemotherapy and radiotherapy . 
the phase 2 rtog 9708 trial , which assessed toxicity of the combined chemotherapy and radiotherapy schedule , and on which the portec - 3 treatment schedule was based , reported a 98% completion rate among 46 patients . 
acute grade 3 adverse events were reported in 12 ( 27% ) patients and grade 4 adverse events in one ( 2% ) patient during concurrent chemoradiotherapy and in nine patients ( 21% ) and 26 patients ( 62% ) during adjuvant chemotherapy . 
 for chronic toxicities , grade 3 adverse events were found in seven ( 16% ) patients and grade 4 adverse events were found in two ( 5% ) patients ; no quality of life data were available . added value of this study to our knowledge , this is the rst randomised study reporting adverse events and quality of life of this combined chemotherapy and radiotherapy schedule . 
we assessed the toxicity and quality of life of patients with high - risk endometrial cancer treated in the international randomised portec - 3 trial with pelvic radiotherapy alone or the combination of radiotherapy with concurrent ( cisplatin ) and adjuvant ( carboplatin - paclitaxel ) chemotherapy . 
grade 2 neurological adverse events persisted in 10% of patients in the chemoradiotherapy group versus < 1% of patients in the radiotherapy group alone , with 25% of patients in the chemoradiotherapy group reporting quite a bit or very much tingling or numbness . implications of all the available evidence combined adjuvant chemoradiotherapy for women with high - risk endometrial cancer is feasible , with increased rates of adverse events and a higher e ect on health - related quality of life during and after treatment . 
 final analysis of the portec - 3 trial is awaited to determine the trade - o of the survival bene t versus e ect on quality of life of added chemotherapy in women with high - risk endometrial cancer . 
 introduction endometrial cancer is most commonly diagnosed at an early stage and most women are cured with surgery alone.1 adjuvant treatment for early stage endometrial cancer is based on risk factors , such as histological grade , myometrial invasion , age , and lymph - vascular space invasion.24 the portec - 2 trial5 , 6 showed the e cacy of vaginal brachytherapy in reducing vaginal recurrence of endometrial cancer in women with high - intermediate - risk endometrial cancer . 
about 15% of all patients with endometrial cancer have high - risk disease ( classi ed as stage i grade 3 cancer with deep invasion or with substantial lymph - vascular space invasion , stage ii or iii cancer , or cancer with non - endometrioid histology ) .1 higher incidence of distant metastases and endometrial cancer - related deaths has been reported for these patients.710 serous and clear cell endometrial cancer are histological subtypes with poorer prognosis because of their high risk of metastasis , but when diagnosed at an early stage to grade 3 seem endometrioid endometrial cancer.11 to have similar survival rates pelvic external beam radiotherapy has been the standard adjuvant treatment for women with high - risk endometrial cancer for several decades . 
because increased pelvic relapse has been reported with adjuvant chemotherapy alone , use of pelvic radiotherapy combined with adjuvant chemotherapy has been advocated.14 , 15 the rtog9708 phase 2 trial16 investigated a combination of external beam radiotherapy with two cycles of cisplatin , followed by four cycles of cisplatin - paclitaxel in 46 women with high - risk endometrial cancer . 
this trial was published in a pooled analysis with the mango iliade - iii trial17 with a combined total of 534 patients , and showed statistically signi cantly improved progression - free survival with the addition of chemotherapy . 
establishing both the bene t of more intensive adjuvant treatment and the e ect in terms of added morbidity and e ect on health - related quality of life are essential . radiotherapy alone with we initiated the international portec - 3 trial to investigate survival bene t and toxicities of chemotherapy vol 17 august 2016 1115 articles for the protocol see combined with external beam radiotherapy compared with external beam radiotherapy alone for high - risk endometrial cancer . 
we did this analysis to establish and compare adverse events and patientreported symptoms and health - related quality of life in women with high - risk endometrial cancer treated in portec - 3 . methods study design and participants portec - 3 was a multicentre , open - label , randomised intergroup trial led by the dutch gynaecological oncology group . 
exclusion criteria were having uterine sarcoma , previous malignancy less than 10 years ago , receipt of previous pelvic radiotherapy , hormonal or chemotherapy , gross cervical radical hysterectomy , in ammatory bowel disease , residual macroscopic tumour , impaired renal or cardiac function , neuropathy grade 2 or worse , hearing impairment grade 3 or worse , or congenital hearing disorder . surgery comprised of total abdominal or laparoscopic hysterectomy with bilateral salpingo - oophorectomy . 
upfront central pathology review was undertaken by the reference gynaecological pathologists of the participating groups to con rm nal eligibility for the study . involvement with written informed consent was obtained from all patients . 
treatment was allocated with a biased coin minimisation procedure , with strati cation according to participating centre , lymphadenectomy ( yes or no ) , stage , and histological type . 
participants and investigators were not masked to treatment allocation . procedures pelvic radiotherapy was given in both treatment groups ( 486 gy in 18 gy fractions , ve times a week for 55 weeks )  . 
the clinical target volume included the proximal vagina , parametrial tissues , and internal , external , and common iliac lymph node regions up to the upper s1 level ( the level of promontory )  . 
treatment breaks were avoided and could not exceed 2 days , overall treatment time for radiotherapy could not exceed 50 days . patients in the chemoradiotherapy group received two cycles of cisplatin 50 mg / m in the rst and fourth week of radiotherapy , followed by four cycles of carboplatin area under the curve ( auc ) 5 and paclitaxel 175 mg / m at 21 - day intervals ( and a 28 - day interval between the second concurrent and rst adjuvant cycle )  . 
after recovery or reduction to grade 1 adverse events , paclitaxel dose was reduced to 1116 vol 17 august 2016 articles 135 mg / carboplatin and paclitaxel were delayed for other grade 34 toxicities , and discontinued if there was no recovery or reduction to grade 1 adverse events . 
 toxicity was graded with the common terminology criteria for adverse events version 3.0 and was assessed at baseline ( after surgery ) , completion of radiotherapy , at each chemotherapy cycle , and at 6 - month follow - up intervals from randomisation until 5 years and at 7 and 10 years . 
health - related quality of life questionnaires were completed at baseline after surgery and after completion of radiotherapy , at 6 - month intervals from randomisation until 24 months , and at 36 and 60 months . 
on the symptom subscales , higher scores re ected higher levels of symptoms . all adverse events were graded and adverse events of grade 2 or worse were reported on case record forms , irrespective of the relation with study treatment . 
time from randomisation was used to compare severity and duration of toxicities between the treatment groups ; importantly , the 6 - month timepoint was about 1 month after completion of chemotherapy in the chemoradiotherapy group . outcomes primary endpoints were overall survival and failure - free survival , with failure de ned as any relapse or death related to endometrial carcinoma . 
secondary endpoints were treatment - related toxicity , health - related quality of life , and pelvic or distant relapse . statistical analysis the portec - 3 trial was powered ( 80% ) to detect a di erence of 10% ( hr 067 ) in 5 - year overall survival ( 65% to 75% ) ; for this , 198 events were required , and a minimum of 655 patients . 
safety outcomes were assessed in all patients who received at least one cycle of chemotherapy and 1 week of radiotherapy ( in the chemoradiotherapy group ) and 1 week of radiotherapy ( in the radiotherapy alone group )  . 
although no speci c power calculations were done for the toxicity and health - related quality of life analysis , the minimum required number of 655 patients ensured su cient power to detect clinically relevant di erences . 
 formal tests for the di erences in relapse and survival rates between the two groups were done with the kaplan - meier method , the log - rank test , and cox regression analysis . 
 we measured toxicity at baseline , at completion of radiotherapy , every cycle of concurrent and adjuvant chemotherapy , and 6 , 12 , 18 , and 24 months ; quality of life was measured at baseline , completion of radiotherapy , and 6 , 12 , 18 , and 24 months after randomisation . 
the time during treatment was de ned as all toxicity forms related to radiotherapy and all cycles of concurrent and adjuvant chemotherapy . criteria to be removed from the analysis were ineligibility or withdrawal of informed consent before the start of treatment . 
patients were evaluable for health - related quality of life analysis if they had completed baseline and at least one follow - up formissing data for patients were handled as missing - at - random , assuming that missing data was not related to the values of the unobserved variables . 
this is an assumption that is not possible to verify statistically.22 the prevalence of toxicity graded according to the common terminology criteria for adverse events version 3.0 was calculated at each timepoint . 
a prespeci ed health - related quality of life analysis was done according to the eortc quality of life group guidelines.23 baseline scores of both treatment groups were compared with a t test , or armitage trend test for single items . 
single items were analysed with ( binary ) logistic regression with random e ect , combining scores of 12 ( not at all and a little ) vol 17 august 2016 1117 articles and 34 ( quite a bit and very much )  . 
the di erence in health - related quality of life between the groups over time was tested by a joint wald test of all treatment - by - time interaction in the linear or logistic mixed model . 
the central data manager ( kwv - a ) , the principal ( clc ) and associated investigators ( smdb , ran ) , and trial statistician ( hp ) had full access to the data . 
 the corresponding author and chief investigator had full investigator 686 patients randomly assigned 13 excluded 4 immediate informed consent 9 ineligible withdrawal 13 excluded 9 immediate informed consent 4 ineligible withdrawal 330 assigned to radiotherapy ( intention to treat ) 330 assigned to chemotherapy and radiotherapy ( intention to treat ) 2 received radiotherapy and chemotherapy 5 received radiotherapy only 328 received radiotherapy 325 received chemoradiotherapy 330 included in intention - to - treat primary analysis 330 included in intention - to - treat primary analysis 333 included in toxicity analysis of radiotherapy group 327 included in toxicity analysis of chemoradiotherapy group figure 1 : trial pro le 1118 access to all of the data and the nal responsibility to submit for publication . the allocated results between sept 15 , 2006 , and dec 20 , 2013 , we recruited 686 patients to the portec - 3 trial recruited . 
another 13 patients withdrew their informed consent immediately after randomisation and were excluded from this analysis , leaving 660 patients ( 330 in each group ) for intention - to - treat analysis . 
for analysis of toxicity and health - related quality of life these seven patients were assessed by treatment received , resulting in 327 patients in the chemoradiotherapy group the radiotherapy alone group . 
median follow - up at the time of analysis for all patients was 423 months ( iqr 258551 ) ; 421 months ( 257547 ) in the chemoradiotherapy group and 424 months ( 271 554 ) in the radiotherapy alone group . 
radiotherapy was discontinued by one ( < 1% ) patient who received chemoradiotherapy because of disease progression and by ve ( 2% ) patients who received radiotherapy alone because of toxicity ( n = 4 ) and an accidental fall with femur fracture ( n = 1 )  . 
a brachytherapy boost was given in 149 ( 46% ) of 327 patients in the chemoradiotherapy group and 156 ( 47% ) of 333 patients in the radiotherapy alone group . 
chemotherapy was discontinued in 61 ( 19% ) patients because of drug - related toxicity in 31 ( 9% ) patients , patient decision in 20 ( 6% ) patients , disease progression in seven ( 2% ) patients , or for other reasons in three ( 1% ) patients . 
90 ( 14% ) of 660 patients could not be assessed for health - related quality of life , mostly because of a missing form at baseline , whereas some questionnaires were invalid because of missing dates of completion or a completion date after the rst day of radiotherapy . 
at 24 months , health - related quality of life scores of 364 ( 55% ) patients had been received , which corresponds to 64% of the 570 responders : ( 194 [ 66% ] of 292 patients in the chemoradiotherapy group and 170 [ 61% ] of 278 patients the radiotherapy alone group )  . 
who performance score was di erent between those who responded to the questionnaire and those who did not , with who 01 recorded in 565 ( 99% ) of 570 patients who responded versus 85 ( 94% ) of 90 patients who did not respond , and who score of 2 or more in ve ( 1% ) patients who responded versus ve ( 6% ) patients who did not respond ( p = 0007 )  . 
baseline grade 2 adverse events were reported for 109 ( 33% ) of 327 patients who received chemoradiotherapy and 93 ( 29% ) of 326 patients who received radiotherapy alone , and grade 34 toxicities were reported in 33 ( 10% ) patients who received chemoradiotherapy and 28 ( 9% ) patients who received radiotherapy alone . 
no deaths occurred during treatment ; two patients ( one in each group ) died shortly after treatment : one patient in the chemoradiotherapy group died from pneumonia after surgery for bowel obstruction because of adhesions ; one elderly patient in the radiotherapy alone group died 3 weeks after radiotherapy because of pneumonia and subsequent multiorgan failure . 
the death of both patients was not related to the study treatment as reported by the treating physician . during treatment and follow - up period , 89 ( 27% ) of 327 patients in the chemoradiotherapy group versus 154 ( 47% ) of 326 patients in the radiotherapy alone group had a maximum toxicity of grade 2 adverse events . 
grade 3 adverse events or worse were reported for 229 ( 70% ) of 327 patients in the chemoradiotherapy group versus 112 ( 34% ) of 326 patients in the radiotherapy alone group ( gure 2 )  . 
during treatment , grade 2 or worse adverse events were found in 309 ( 94% ) of 327 patients including whole the study , data are median ( iqr ) or n ( % )  . 
eec = endometrioid endometrial carcinoma . table 1 : characteristics of as - treated population by treatment group vol 17 august 2016 1119 articles 1120 vol 17 august 2016 articles patient - reported lymphoedema did not di er between the two treatment groups ( appendix p 7 )  . 
severe lymphoedema was reported more frequently by patients who had undergone a lymphadenectomy ( both treatment groups combined ) : 47 ( 17% ) of 276 patients after lymphadenectomy versus 13 ( 8% ) of 163 patients without lymphadenectomy at 12 months ( p = 001 ) and 38 ( 16% ) of 237 patients versus 14 ( 11% ) of 127 patients at 24 months ( p = 02 )  . 
after lymphadenectomy , severe lymphoedema was reported by 18 ( 15% ) of 120 patients in the chemoradiotherapy group and 20 ( 17% ) of 117 patients in the radiotherapy alone group at 24 months ( p = 084 ) , compared with seven ( 10% ) of 69 patients and seven ( 12% ) of 58 patients , respectively , who had no lympha denectomy ( p = 069 ; appendix , p 9 )  . 
sexual activity was low in grade 4 adverse events grade 3 adverse events grade 2 adverse events concurrent radiotherapy baseline and che m otherapy adjuvant che m otherapy 6 m onths 12 m onths 24 m onths in the chemoradiotherapy group versus 145 ( 44% ) of 326 patients in the radiotherapy alone group ( p < 00001 ) ; grade 3 or higher were found in 198 ( 61% ) patients in the chemoradiotherapy group versus 42 ( 13% ) patients in the radiotherapy alone group ( p < 00001 ; gure 2 , table 2 )  . 
during treatment , grade 3 or worse sensory neuropathy was reported in 22 ( 7% ) patients and motor neuropathy was reported in four ( 1% ) patients , all in the chemo radiotherapy group . 
the most important persisting toxicity was grade 2 or worse sensory neuropathy at 12 months in 30 ( 10% ) patients in the chemoradiotherapy group versus three ( 1% ) patients in the radiotherapy group , and 25 ( 10% ) patients in the chemoradio therapy group versus one ( < 1% ) patient in the radiotherapy alone group at 24 months ( p < 00001 )  . 
during treatment , patients treated with chemoradiotherapy scored signi cantly lower on most eortc functioning scales ; 1020 - point lower scores on physical , role , and social functioning , and global health status compared with patients treated with radiotherapy alone . 
however , rapid recovery was reported , and at 12 months physical functioning was the only signi cant di erence between the two treatment groups ( gure 3 )  . in 80 ( 37% ) of 214 patients in 111 ( 52% ) of 214 patients the most frequently reported severe ( quite a bit or very much ) symptoms at 6 months were tingling or numbness the chemoradiotherapy group versus 15 ( 7% ) of 209 patients in the radiotherapy alone group ( p < 00001 ) , muscle or joint pain the chemoradiotherapy group versus 45 ( 22% ) of 207 patients in the radiotherapy alone group ( p = 0002 ) , fatigue in 66 ( 31% ) of 210 patients versus 36 ( 17% ) patients ( p = 00004 ) , weakness in the arms or legs in 76 ( 36% ) of 214 patients versus 24 ( 11% ) of 209 patients ( p < 00001 ) , and hair loss in 88 ( 44% ) of 200 patients versus eight ( 4% ) of 208 patients the chemoradiotherapy group signi cantly higher in all these cases . 
 * subscale symptom experience included abdominal cramps , controlling bowels , blood in stool , urinary frequency , dysuria , urinary incontinence , di culty emptying bladder , lower back pain , vaginal irritation or soreness , vaginal discharge , and abnormal vaginal bleeding . 
 both groups , but was slightly higher in the radiotherapy alone group during treatment ( p = 0006 ) , and similar thereafter ( see appendix p 8 )  . 
 incidence of signi cantly higher discussion this analysis of toxicity and 2 - year health - related quality of life in the portec - 3 trial for women with high - risk endometrial cancer clearly shows that adjuvant chemotherapy given during and after pelvic radiotherapy causes severe adverse events and of patient - reported symptoms , and a decreased level of patient functioning and health - related life compared with radiotherapy alone . 
 quality of however , rapid recovery was seen , with reduction of all incidence and grades of adverse events between 6 and 12 months after randomisation , and without signi cant di erences in grade 3 or worse adverse events at 12 and 24 months . 
the only remaining signi cant di erence in adverse events at 12 and 24 months was increased grade 2 or worse sensory neuropathy in the chemoradiotherapy group compared with the radiotherapy alone group ( 25 [ 10% ] of 240 vs 1 [ < 1% ] of 247 ) , with health - related quality of life showing quite a bit or very much tingling or numbness reported by 25% of patients in the chemoradiotherapy group versus 6% of patients the radiotherapy alone group . 
the association between individual symptoms and overall quality of life will be a subject of further investigation . the 6 - month timepoint when most severe adverse events and worst quality of life were reported by patients receiving chemoradiotherapy was only 1 month after completion of chemotherapy , whereas patients treated with radiotherapy alone already had 4 months of recovery time . 
these results represent the toxicity pro les of the patients in the two treatment groups and provide a the realistic view of chemoradiotherapy group , which is of relevance for patient counselling when considering chemotherapy . time with toxicity the data for the toxicity of chemotherapy in advanced or metastatic endometrial cancer are mainly available from the randomised trials27 in which doxorubicin and vol 17 august 2016 1123 articles a tingling or numbness radiotherapy alone chemoradiotherapy b muscle or joint pain radiotherapy alone chemoradiotherapy c diarrhoea radiotherapy alone chemoradiotherapy baseline co m pletion of radiotherapy 6 m onths 12 m onths 18 m onths 24 m onths 6 m onths 12 m onths 18 m onths 24 m onths baseline co m pletion of radiotherapy timepoint timepoint not at all a little quite a bit very much figure 4 : patient responses on single - item symptom scales over time for tingling or numbness ( a ) , muscle or joint pain ( b ) , and diarrhoea ( c ) in the chemoradiotherapy group and the radiotherapy alone group those sensory neuropathy cisplatin with or without paclitaxel were used . 
incidence trials during chemotherapy was signi cantly higher than in the portec - 3 trial , with 27% of patients having grade 2 adverse events and 12% of patients having grade 3 neuropathy when treated with the doxorubicin , cisplatin , and paclitaxel triplet combination . 
results of the randomised gog - 20928 triplet trial chemotherapy was compared with carboplatin - paclitaxel are pending , but an abstract reported similar e cacy with a better toxicity pro le of carboplatin - paclitaxel in which the ( nct00063999 )  . 
the gog - 249 trial29 compared pelvic radiotherapy alone with vaginal brachytherapy followed three cycles of carboplatin and paclitaxel patients with stage iii endometrial cancer with high - intermediate - risk or high - risk features . 
first results at a median follow - up of 24 months showed no di erences in recurrence - free and overall survival , with more acute toxicity in the chemotherapy group . 
data for health - related quality of life are pending . data for toxicity and health - related quality of life treated with carboplatin or paclitaxel of women chemotherapy are mainly available from rst - line therapy in ovarian cancer trials . 
comparison is relevant , as patients with ovarian cancer are of similar age and the have also had previous pelvic surgery , and combination of radiation and chemotherapy was expected to be more toxic than chemotherapy alone . 
 ovarian cancer trials with a 3 - weekly schema of carboplatin auc6 and paclitaxel 175180 mg / ml reported mainly grade 34 haematological toxicities , with similar grades of haematological toxicity and febrile neutropenia in the mito - 7 trial30 compared with portec - 3 , and higher grades reported in the jgog - 3016 trial.31 additionally with this 3 - weekly schema , grade 34 sensory and motor neuropathy were reported in 6% and 4% respectively in jgog 3016 , compared with 7% and 1% in portec - 3 , and 3% had any grade 34 neuropathy in the mito - 7 trial . at 24 months after randomisation , patient - reported sensory neuropathy remained signi cantly worse in the chemoradiotherapy group than in the radiotherapy alone group . 
a population - based study in ovarian cancer survivors reported peripheral neuropathy ( as measured with eortc - ov28 ) in 51% of patients treated with chemotherapy versus 27% of participants treated without chemotherapy.32 neuropathy is a common symptom in the general population , increasing with age and with the prevalence of diabetes.33 women with higher levels of neuropathy reported lower levels of functioning and quality of life , and more fatigue.32 than lower completion rates for chemotherapy were 93% for cisplatin , 80% for carboplatin , and 72% for paclitaxel , with dose reductions in 7% of carboplatin and 10% of paclitaxel cycles . 
similar to health - related quality of life ndings in the portec - 1 and portec - 2 trials , baseline sexual activity just after surgery and during treatment was low , with improvement over time , but sexual activity in this elderly patient group remained lower compared with population data.6 the current endometrial cancer module ( en24 ) was not yet available when the portec - 3 trial was 1124 vol 17 august 2016 articles designed . 
 this could be a possible limitation to the study , although the en24 module is very similar to cx24 , with some of the same chemotherapy - related questions as in ov28 included.34 portec - 3 assessed both physician - reported and patient - reported toxicities . 
limited agreement between patient and physician reported scoring of toxicities has been shown , with signi cant physician under - reporting of lower grade toxicities.35 in the portec - 3 study , physicians were required to report grade 2 or worse adverse events to focus on more severe toxicities , and patient - reported outcomes were used for mild toxicities . 
 although patient - reported and physician - reported symptoms use di erent scales , similar trends in types of symptoms over time were seen . both the portec - 3 trial and the gog - 258 trial used the same combined chemotherapyradiotherapy schedule , but in comparison with radiotherapy alone and chemotherapy alone , respectively . 
for ovarian cancer , several trials have been done to compare di erent ( weekly ) infusion schedules to achieve a balance between optimum therapy and acceptable toxicity.30 , 31 overall , combined adjuvant chemotherapy and radiotherapy for high - risk endometrial cancer caused signi cantly higher incidence of severe adverse events and reduced health - related quality of life during and after treatment compared with radiotherapy alone , but with rapid recovery . 
final analysis of the portec - 3 and gog258 trials are awaited , to determine the bene t of chemoradiotherapy in women with high - risk endometrial cancer . contributors clc was the chief investigator of the trial . 
all authors contributed to the preparation and writing of the manuscript and approved the nal manuscript . declaration of interests we declare no competing interests . acknowledgments the portec - 3 study was supported by a grant from the dutch cancer society , netherlands ( grant number ul2006 - 4168 / ckto 2006 - 04 )  . 
participation in the portec - 3 trial by the australian and new zealand gynaecologic oncology group and the trans tasman radiation oncology group were supported by the national health and medical research council project grant 570894 ( 2008 ) and by a cancer australia grant ( awarded through the 2011 round of the priority - driven collaborative cancer research scheme and funded by cancer australia )  . 
we thank all the participating groups : dutch gynaecology oncology group ( netherlands ) , the national cancer research institute ( united kingdom ) , australian and new zealand gynaecologic oncology group ( australia & new zealand ) , mango ( italy ) , fedegyn ( france ) , and canadian cancer trials group ( canada ) ; their coordinating teams , principal investigators , sta , and clinical research teams at the groups participating centres for all their work and e orts , and the patients who participated and contributed by lling in questionnaires . 
this study was presented in part at the annual meeting of the american society of clinical oncology , chicago , usa , may 29june 2 , 2015 and presented in part as a poster presentation at the 19th international meeting of the european society of gynaecologic oncology , nice , france , oct 2327 , 2015 . 
 reflection & reaction hrpt2 and parathyroid cancer we read with interest the lancet oncologys news article entitled , vital gene linked to parathyroid carcinoma that highlighted a paper by shattuck and colleagues in the new england journal of medicine.1 , 2 the article by shattuck et al was accompanied by an editorial , 3 which clearly acknowledged an earlier publication in this field by howell and co - workers entitled , hrpt2 mutations are associated with malignancy in sporadic parathyroid tumors.4 in the linked - editorial , weinstein and simonds clearly refer to the study of howell et al : another recent study identified similar mutations in four of four tumours from patients with parathyroid carcinoma , but not in parathyroid adenomas , suggesting that such mutations are markers of cancer . 
while shattuck et al only screened parathyroid carcinomas for hrpt2 mutations , howell colleagues carried out a more extensive screening programme for hrpt2 in : benign parathyroid mutations lesions ( 25 sporadic adenomas , two lithium - associated tumours , 11 secondary , and six tertiary hyperplastic glands ) ; familial parathyroid tumours ( three with familial isolated hyperparathroidism , five with hyperparathyroidism jaw tumour syndrome , three with multiple endocrine neoplasia type 1 , and one with multiple endocrine neoplasia type 2 ) ; and sporadic parathyroid carcinomas . 
 in their series , howell and coworkers found the hrpt2 mutation was specific to the sporadic parathyroid cancer subtype ( in addition to the germline hrpt2 mutations already reported in a subset of families with hyperparathyroidism jaw tumour syndrome5 )  . 
shattuck et al were unable to draw this conclusion in their study because they did not include sporadic benign parathyroid tumours . in summary , prior to shattuck et al , howell and colleagues had clearly established the presence of a somatic hrpt2 mutation in sporadic parathyroid carcinoma . 
additionally , howell et al have previously shown that somatic hrpt2 mutations are specific to the carcinoma subtype in sporadic neoplastic parathyroid disease , with the exception of somatic hrpt2 mutation in 4% of sporadic adenomas with cystic features.5 deborah j marsh * , hans morreau , and bin t teh * kolling institute of medical research , royal north shore hospital , sydney , nsw , australia and department of molecular medicine , university of sydney , sydney , nsw , australia , department of pathology , leiden university medical center , leiden , netherlands , laboratory of cancer genetics , van andel research institute , grand rapids , mi , usa . corrections correction to lancet oncol 2014 ; 16 : 767 correction to lancet oncol 2016 ; 17 : 431 , 434 , 435 correction to lancet oncol 2016 ; 17 : 953 weber js , geo gibney , sullivan rj , et al . 
 sequential administration of nivolumab and ipilimumab with a planned switch in patients with advanced melanoma ( checkmate 064 ) : an open - label , randomised , phase 2 trial . 
lancet oncol 2016 ; 17 : 94355in gure 5 , under the headings nivolumab followed by ipilimumab and ipilimumab followed by nivolumab , the text should have read number of events / number of patients . 
this correction has been made to the online version as of june 28 , 2016 , and the printed version is correct . correction to lancet oncol 2016 ; 17 : 995 , 1002 cella d , grnwald v , nathan p , et al . 
 quality of life in patients with advanced renal cell carcinoma given nivolumab versus everolimus in checkmate 025 : a randomised , open - label , phase 3 trial lancet oncol 2016 ; 17 : 9941003in this article , the order of references 711 has been corrected and the fourth sentence of the second paragraph of the introduction has been corrected to read furthermore , an analysis of hrqol scores according to the functional assessment of cancer therapy - kidney symptom index - disease related symptoms ( fksi - drs ) questionnaire ( a subscale of the 15 - item fksi - 15 ) showed that median change from baseline increased over time with nivolumab treatment . 
these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . jeong s - y , park jw , nam bh , et al . 
open versus laparoscopic surgery for mid - rectal or low - rectal cancer after neoadjuvant chemoradiotherapy ( corean trial ) : survival outcomes of an open - label , non - inferiority , randomised controlled trial . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2015 ; 16 : 1479 motzer rj , hutson te , glen h , et al . 
lancet oncol 2015 ; 16 : 147382in table 3 of this article , the number of patients in the lenvatinib plus everolimus group with grade 3 constipation should be 0 . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 351 untch m , jackisch c , schneeweiss a , et al . 
 lancet oncol 2016 ; 17 : 34556in this article , the data in the second sentence of the third paragraph of the results section should have read in multivariable logistic regression analysis , nab - paclitaxel remained an independent predictor for achievement of pathological complete response after adjustment for baseline and minimisation factors ( or 159 ; 95% ci 120211 ; p = 00013 )  . 
fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment o f h o r m o n e r e c e p t o r p o s i t i v e , her2 - negative metastatic breast cancer that progressed on previous endocrine therapy ( paloma - 3 ) : final analysis of the multicentre , doubleblind , phase 3 randomised controlled trial . 
lancet oncol 2016 ; 17 : 42539 in figures 2a , 5a , 5b , and 5c , the kaplan - meier curves should have intersected with the y - axis at the 100% mark . 
these corrections have been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 888 , 890 , 892 cancer antonia sj , lpez - martin ja , bendell j , et al . 
 lancet oncol 2016 ; 17 : 88395in this article , the rst line in the third paragraph of the results , blinded independent central review should have been investigator - assessed recist . 
in the seventh paragraph of the results , the number of patients in the nivolumab 3 mg / kg plus ipilimumab 1 mg / kg cohort who had diarrhoea as a serious adverse event should have been two ( 4% ) , not four ( 7% )  . 
 these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . vol 17 july 2016 e270 corrections correction to lancet oncol 2015 ; 16 : 1013 correction to lancet oncol 2015 ; 16 : 1143 correction to lancet oncol 2015 ; 16 : 1289 declaration kopans db . 
 lancet oncol 2015 ; 16 : 1143the last line of the rst paragraph of this comment should read only this year , for example , did who add several commonly used , extremely e ective drugs , such as imatinib , trastuzumab , and cisplatin to its list of essential medicines . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the paragraph on survival with oligometastatic hcc should read the researchers found that patients with oligometastatic disease had a significantly longer overall survival than patients with extensive disease ( 104 months versus 63 months , p = 0034 )  . 
these data raise the question whether the pursuit of improved survival outcomes comes with a trade - o in tolerability that is reaching an unsustainable level . leboulleux and colleagues study in the september issue of the lancet oncology serves to further illustrate this point . 
despite an improvement in progressionfree survival of more than 5 months , patients with di erentiated thyroid cancer given vandetanib were at substantially greater risk of side - e ects such as severe diarrhoea and were more than ve times more likely to discontinue treatment because of toxicity than were those in the control group . 
and in another article in the current issue , by ismael and colleagues , a novel subcutaneous formulation of trastuzumab increase treatment - related toxicity and mortality compared with the standard intravenous administrationwhich in turn suggests that the potential for increased patient convenience with the new formulation is not necessarily a clear - cut bene t . 
 is shown to one would have hoped that the advent of targeted therapythe premise of which revolves around an ability to more precisely direct treatments to disease would have lessened the amount of adverse e ects a patient might experience . 
in an analysis of the selectivity of various kinase inhibitors , in which a range of targeted agents were screened across a panel of more than 300 kinases , sorafenibas just one examplewas found to bind to 10% of o - target kinases with a similar a nity to its primary targets of vegfr and braf . 
the barrier for agents to proceed to later stage trials should be raised , and in some instances , when clinical bene t is marginaleg , bevacizumab for breast cancerone wonders whether the current accelerated approval processes might in fact have become too accelerated . 
given the marked increase in complications when targeted agents are combined with chemotherapeutic agents , greater emphasis should be placed on undertaking phase 1 trials of combinations of drugs , and only when there is a clear mechanistic rationale for the drugs co - administration . 
 more comparative phase 2 trials should be done , and should also incorporate extensive biomarker analyses not just for e cacy , but also for a better understanding of the molecular mechanisms of toxicity . 
in so doing , phase 3 trials can be better designed not only to enrol solely those patients most likely to bene t , but also those least likely to be harmed . 
greater attention must also be paid to collecting quality - of - life data , in particular patient - reported outcomes , to determine whether the quality of any lengthening of survival is not outweighed by toxicity . 
 finally , post - marketing phase 4 studies should be more widely done , and databases set up to rigorously and prospectively collect data for adverse events as they are reported in the community , so that a new drugs activity and toxicity can be better examined in a less selected patient population . 
indeed , an analysis of updated drug labels for anticancer drugs that had been approved by the fda showed that more than 40% of targeted agents gained one or more boxed warnings for serious adverse drug reactions within about 4 years of initial approval , with half of the additional adverse reactions potentially being fatal , highlighting the value of continued surveillance . 
 the lancet oncology vol 13 september 2012 in checkmate 141 , 2 patients who had a worse qol at baseline were lost to follow - up sooner than those who remained on the treatment longer . 
i think it is possible that the pros were influenced by this : patients who received the new treatment might have been more hopeful , with consequently a better qol . limitations in mind , checkmate 141 offers valuable insight into the potential effects of nivolumab on certain qol domains in patients with advanced head and neck cancer who are reasonably fit ( eastern cooperative oncology group performance status of 0 or 1 )  . 
domains that are most important to patients with head and neck cancer according to an international eortc study3 are worrying , swallowing , talking , eating , sticky saliva , dry mouth , and pain in the mouth . 
problems with skin could not be measured in this trial , though the toxicity profile suggests there might be more problems after nivolumab than after investigators choice.1 this issue needs to be investigated in future trials . overall , it is highly appreciated that the pros of checkmate 141 are presented fully and in a timely manner . 
 for instance , progression or death could be considered as competing events for qoleg , with multistate modelling . susanne singer division of epidemiology and health services research , institute of medical biostatistics , epidemiology , and informatics , university medical centre mainz , 55131 mainz , germany singers@uni - mainz.de i have received a grant from pfizer , the quality of life prize from lilly , travel grants from genzyme , and lecture fees from astrazeneca , pfizer , bristol - myers squibb , and boehringeringelhei ferris rl , blumenschein g , fayette j , et al . 
nivolumab versus standard , single - agent therapy of investigators choice in recurrent or metastatic squamous cell carcinoma of the head and neck ( checkmate 141 ) : healthrelated quality - of - life results from a randomised , phase 3 trial . 
lancet oncol 2016 ; 17 : 9941003 . which fractionation of radiotherapy is best for limited - stage small - cell lung cancer ? the role of radiotherapy in the treatment of small - cell lung cancer has been established through a series of clinical trials and meta - analyses during the past 20 years , which showed that local radiotherapy in addition to chemotherapy1 and whole - brain radiotherapy2 can improve patient prognosis . 
results from the intergroup 0096 trial4 showed that a radiotherapy dose of 45 gy given twice daily led to improved prognosis fractionation when compared with once - daily regimens employing the same total radiotherapy dose . 
 this study was criticised because the dose ( 45 gy ) in the conventional treatment group was regarded as insufficient , since some studies have shown that a 60 gy dose can achieve better results than 45 gy in conventionally fractionated schedules.5 in the lancet oncology , corinne faivre - finn and colleagues report results from the convert trial , 6 which compared a twice - daily radiotherapy regimen ( 45 gy delivered in 30 twice - daily fractions of 15 gy ) with a once - daily radiotherapy regimen ( 66 gy delivered in 33 once - daily fractions of 2 gy ) , both given in published online june 19 , 2017 s1470 - 2045 ( 17 ) 30439 - 4 see articles page 1116 994 vol 18 august 2017 comment in patients with combination with chemotherapy , limited - stage small - cell lung cancer . 
the authors found no difference between the treatment groups in the primary endpoint of overall survival ( median overall survival 30 months [ 95% ci 2434 ] in the twice - daily group vs 25 months [ 2131 ] in the once - daily group ; hazard ratio 118 [ 95% ci 095145 ] , p = 014 )  . 
they also reported no differences between the groups in local or metastatic progression - free survival . in the convert trial , the authors were able to address an important radio - oncological question concerning the superiority of a fractionation schedule in a large patient population . 
unlike the intergroup trial 0096 , this study shows no significant disadvantage of once - daily fractionation schedules , but the use of a high radiation dose ( 66 gy ) was necessary with this regimen . 
this fact underlines that not only is the radiotherapy dose crucial for the effects of treatment , but so also is the time in which this dose is applied ( 19 days in the twice - daily group vs 45 days in the once - daily group )  . 
a shorter duration of radiotherapy delivery might reduce the dose required . 5 - year overall survival results for both regimens ( 31% in the once - daily group and 34% in the twice - daily group ) were higher than those reported by other trials so far ( eg , 1626% in intergroup trial 0096 ) .5 remarkably , this outcome was achieved with lower than anticipated acute and long - term toxicity in both groups ( eg , acute grade 34 pneumonitis 2% and grade 4 oesophagitis 19% , in both groups )  . 
this outcome was achieved by modifying two steps of the treatment protocol : 312 ( 57% ) of 547 patients were staged by pet / ct and the radiotherapy dose was limited to areas definitely involved by tumour , without any elective irradiation . 
however , radiotherapy was delivered over the planned treatment time more often in the twicedaily group than in the once - daily group ( 63% vs 48% ; p = 00004 ) ; unfortunately , the authors do not give more information about this finding . 
additionally , more patients received the full dose of radiotherapy in the twice - daily group ( 98% twice - daily vs 83% once - daily ; p < 00001 )  . 
the authors speculate that dose constraints for lung and spinal cord in particular were easier to meet because of the lower total dose in the twice - daily radiotherapy group . 
additionally , more patients did not receive treatment as originally prescribed in the oncedaily group ( 39 [ 14% ] of 270 ) than in the twice - daily group ( 26 [ 10% ] of 273 )  . 
 since there were no significant differences in survival outcomes , twice - daily radiotherapy up to a total dose of 45 gy will remain the standard treatment for smallcell lung cancer . 
phase i study to determine the maximum - tolerated dose of radiation in standard daily and hyperfractionated - accelerated twice - daily radiation schedules with concurrent chemotherapy for limited - stage small - cell lung cancer . 
concurrent once - daily versus twice - daily chemoradiotherapy in patients with limited - stage small - cell lung cancer ( convert ) : an open - label , phase 3 , randomised , superiority trial . 
our aim was to investigate these associations in a large uk prospective cohort with su cient information on incident cancer to allow direct comparison of height - associated risk across cancer sites and in relation to major potential confounding and modifying factors . methods information on height and other factors relevant for cancer was obtained in 19962001 for middle - aged women without previous cancer who were followed up for cancer incidence . 
we used cox regression models to calculate adjusted relative risks ( rrs ) per 10 cm increase in measured height for total incident cancer and for 17 speci c cancer sites , taking attained age as the underlying time variable . 
 findings 1 297 124 women included in our analysis were followed up for a total of 117 million person - years ( median 94 years per woman , iqr 84102 ) , during which time 97 376 incident cancers occurred . 
risk increased for 15 of the 17 cancer sites we assessed , and was statistically signi cant for ten sites : colon ( rr per 10 cm increase in height 125 , 95% ci 119130 ) , rectum ( 114 , 107122 ) , malignant melanoma ( 132 , 124140 ) , breast ( 117 , 115119 ) , endometrium ( 119 , 113124 ) , ovary ( 117 , 111123 ) , kidney ( 129 , 119141 ) , cns ( 120 , 112129 ) , nonhodgkin lymphoma ( 121 , 114129 ) , and leukaemia ( 126 , 115138 )  . 
the increase in total cancer rr per 10 cm increase in height did not vary signi cantly by socioeconomic status or by ten other personal characteristics we assessed , but was signi cantly lower in current than in never smokers ( p < 00001 )  . 
in current smokers , smokingrelated cancers were not as strongly related to height as were other cancers ( rr per 10 cm increase in height 105 , 95% ci 101109 , and 117 , 113122 , respectively ; p = 00004 )  . 
in a meta - analysis of our study and ten other prospective studies , height - associated rrs for total cancer showed little variation across europe , north america , australasia , and asia . interpretation cancer incidence increases with increasing adult height for most cancer sites . 
the relation between height and total cancer rr is similar in di erent populations . funding cancer research uk and the uk medical research council . introduction tall people are at increased risk of cancer . 
increasing cancer risk with increasing adult height has been reported for all cancers combined and for several common cancers , such as those of the breast , ovary , prostate , and large bowel.17 evidence is limited , however , for incident , rather than fatal , disease and for less common cancer sites . 
 moreover , it is not clear to what extent height - associated risks vary by cancer site , or how other factors , such as smoking and socioeconomic status , a ect these associations.8 , 9 because the range of height in a given population is usually narrow , large numbers of events are needed for reliable estimation of risk . 
we also did a meta - analysis of published results from prospective studies on the relation between height and total cancer incidence or mortality . methods participants between 1996 and 2001 , 13 million middle - aged women invited to attend the uks national health service ( nhs ) breast screening programme completed a million women study recruitment questionnaire , which asked , among other things , about social , demographic , and lifestyle factors , including current height and weight . 
of women who answered a study questionnaire in 200607 , a sample selected at random ( on the basis of day of birth ) were asked in 200609 to have their height measured by their family doctor : 3762 women did so . 
in this validation sample , the correlation between measured and reported heights was excellent ( pearson correlation coe cient 088 )  . vol 12 august 2011 articles all participants gave written consent to take part in our study , and approval was obtained from the oxford and anglia multi - centre research ethics committee . 
all study participants have a unique nhs number and are automatically followed up for death , emigration , and cancer registration through the nhs central registers with that number and other identifying details . 
the registers regularly provide study investigators with information on the date of any such event in participants , and code the underlying cause of death and cancer site with the international classi cation of diseases , 10th revision ( icd - 10 ) .10 follow - up is complete for over 99% of study participants . 
 procedures our main endpoints were incident invasive cancer at 17 individual sites with at least 1000 incident cases : mouth and pharynx ( icd - 10 c00 - c14 ) , oesophagus ( c15 ) , stomach ( c16 ) , colon ( c18 ) , rectum ( c19 - 20 ) , pancreas ( c25 ) , lung ( c34 ) , malignant melanoma ( c43 ) , breast ( c50 ) , endometrium ( c54 ) , ovary ( c56 ) , kidney ( c64 ) , bladder ( c67 ) , central nervous system ( c7072 , d32 , 33 , 42 , and 43 ) , non - hodgkin lymphoma ( c82 - 85 ) , multiple myeloma ( c90 ) , and leukaemia ( c91 - 95 )  . 
we included all other invasive cancers ( the remaining icd - 10 c codes , except non - melanoma skin cancer [ c44 ] ) as other and unspeci ed cancers . there concluded has su cient evidence of carcinogenicity in human beings in relation to active tobacco smoking : 11 , 12 of the sites listed above , mouth and pharynx , oesophagus , stomach , colorectum , pancreas , lung , mucinous tumours of the ovary , kidney , and myeloid leukaemia ( c92 ) , and , additionally , liver ( c22 ) , larynx , nasal cavity and nasal sinuses ( c30 - 32 ) , cervix ( c53 ) , and urinary tract , including renal pelvis and ureter ( c65 , 66 , 68 )  . 
when comparing smoking - related and other cancers , we excluded from our analysis cancers of ill - de ned and unspeci ed sites , which might include some smokingrelated cancers ( icd - 10 c26 , c39 , c57 , c76 - 80 and c95 - 96 ) , and cancers of the ovary ( for a substantial proportion of which histological subtype was not known , and which might have included mucinous tumours )  . cm , 1601649 height was reported by participants at recruitment in feet and inches , and converted to centimetres for our analysis . 
for the analyses , women were divided into six categories of reported height ( < 155 cm [ reference group ] , cm , 1551599 1701749 cm , and 175 cm and taller ) ; we took the average height in each of these categories to be the mean measured height in that category in the sample whose height was measured in 200609 . 
standardised to the distribution of categories of self - reported height in our whole analysis population . table 1 : baseline characteristics by height and follow - up for incident cancer in the million women study 786 vol 12 august 2011 articles women rr ( 95% fci ) incident cancers < 155 cm ( mean 1528 cm ) 233 516 15 792 100 ( 098102 ) 155 cm ( mean 1565 cm ) 196 773 14 213 108 ( 107110 ) 160 cm ( mean 1604 cm ) 388 515 28 806 112 ( 111114 ) 165 cm ( mean 1649 cm ) 288 893 22 571 120 ( 118122 ) 170 cm ( mean 1690 cm ) 143 289 11 902 128 ( 125130 ) 175 cm ( mean 1738 cm ) 46 138 4092 137 ( 133142 ) analysis strati ed by age at recruitment and region and adjusted for socioeconomic status , smoking , alcohol intake , body mass index , strenuous exercise , age at menarche , parity , and age at rst birth . table 2 : relative risks ( rrs ) and 95% oated cis ( fcis ) for total cancer incidence , by category of height reported at recruitment ( mean measured height ) cancer ( icd10 c44 ) registered before recruitment and if they did not have valid information on height at recruitment ( including a small proportion , about 005% whose reported height was < 120 cm or > 200 cm )  . 
for analyses including endometrial and / or cervical cancers , we excluded women if they reported a hysterectomy at recruitment , or if their hysterectomy status was unknown ; similarly , for analyses of ovarian cancer , we excluded women reported a bilateral they oophorectomy at recruitment , or if their oophorectomy status was unknown . from we calculated woman - years the date of recruitment to the date of rst cancer registration ( at any site ) , death , or the last date of follow - up , whichever was rst . 
for analyses of cancer incidence , the last date of follow - up was dec 31 , 2008 , for the uk regions of east anglia and south west ; june 30 , 2008 , for oxford , thames , west midlands , and north west ( mersey ) ; and dec 31 , 2007 , for northern and yorkshire , trent , north west ( manchester and lancashire ) , and scotland . statistical analysis we used cox regression models to estimate relative risks ( rrs ) and cis in relation to height at recruitment , taking attained age as the underlying time variable . 
we strati ed all analyses by age at recruitment ( < 52 , 5355 , 5658 , 5961 , 6264 , 65 years ) and region ( ten regions covered by ten cancer registries ) , and adjusted , as appropriate , for quintiles of socioeconomic group ( based on townsend deprivation score13 ) , body - mass index ( < 225 , 225249 , 250274 , 275299 , 30 kg / m ) , strenuous exercise ( less than once a week , once a week or more ) , alcohol consumption ( none , 2 units per week , 3 units per week ) , smoking ( never , past , current 114 cigarettes per day , current 15 cigarettes per day ) , age at menarche ( < 13 , 13 , 14 years ) , parity ( 0 , 12 , 3 full - term pregnancies ) , and age at rst birth ( < 25 , 25 years )  . 
 we calculated the rr per 10 cm increase in height as a trend across the six category means using the measured mean height in each category of reported height.14 we assessed heterogeneity of trends in rrs between di erent cancer sites with a ( ) contrast test , under the survival analysis assumptions that estimates at each cancer site are asymptotically normally distributed and , because of censoring at rst cancer diagnosis at any site , uncorrelated ( and that therefore site - speci c estimates account for competing risks of cancers at other sites ) .15 where two categories of exposure are compared ( as in the text ) conventional cis are given . 
for analyses of total cancer , where more than two categories are compared ( as in the gures ) , oated cis ( fcis ) were estimated by treating the rrs as oating absolute risks ( fars ) .16 , 17 use mean height ( cm ) figure 1 : relative risks ( rrs ) and 95% oated cis ( fcis ) for total incident cancer , by height rrs are adjusted for age , region , socioeconomic status , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth , and are plotted against the mean measured height in each category . 
all results are presented in the text with 95% cis , but for analyses by cancer site , when multiple rrs were estimated , 99% cis are given in the gures . where we present results in the form of plots , the rrs and their corresponding fcis or cis are represented by squares and lines with the area of each square inversely proportional to the variance of the logarithm of the corresponding rr . 
this shows the amount of statistical information involved . meta - analysis we identi ed published prospective studies of adult height and risk of total cancer ( incidence or mortality ) through electronic searches of published work ( medline and embase , up to april , 2011 ) with combinations of the search terms height , body size , anthropometr * , neoplasms , mortality , and risk factors , and vol 12 august 2011 articles number of incident cancers mouth and pharynx 1095 oesophagus 1167 stomach 1177 colon 6281 rectum 3190 pancreas 2044 lung 8074 melanoma 3583 breast 39 299 endometrium 5810 ovary 4830 kidney 1665 bladder 1354 cns 2328 non - hodgkin lymphoma 3411 1215 multiple myeloma leukaemias 1482 other and unspecifed 8997 total cancer 97 376 rr * & 99% ci 094 ( 082108 ) 104 ( 091119 ) 103 ( 090118 ) 125 ( 117132 ) 114 ( 105124 ) 105 ( 095117 ) 103 ( 098108 ) 132 ( 122142 ) 117 ( 114120 ) 119 ( 112126 ) 117 ( 109125 ) 129 ( 115145 ) 100 ( 088114 ) 120 ( 109132 ) 121 ( 112131 ) 113 ( 099129 ) 126 ( 111142 ) 115 ( 110121 ) 116 ( 114117 ) through cited references in identi ed papers . 
we included in our meta - analysis all identi ed studies with published age - adjusted rr and 95% cis for total cancer per 10 cm increase in height , or with su cient published data to allow estimation of such rrs . 
where only categorical results were published , we calculated the trend in rr per 10 cm increase in height using the mean height in each height category ( estimated , where necessary , as category midpoints , or by other methods ) , 18 assuming linearity of log rrs and with a summary trend estimate obtained by the method of generalised least squares.19 we combined results for subgroups of total cancer ( eg , smoking - related and other cancers ) by least squares , where necessary . 
where the mean year of birth of the study population was not given , we made an estimate with the average age at , and year of , study recruitment . 
 results the 1 297 124 women included in our analysis had a mean age at recruitment of 561 years ( sd 49 ) and an average year of birth of 1942 . 
the median length of follow - up was 94 years per woman ( iqr 84102 years ) , for a total of 117 million person - years , during which 97 376 incident cancers were noti ed . table 1 shows characteristics of the study population , including measured height , by six categories of height reported at recruitment . 
taller women tended to be of higher socioeconomic status , to drink more alcohol , to be more active , to have a later age at menarche , to have fewer children , and to have their rst child later in life than shorter women . 
based on heights measured in the validation sample , the mean height in the study population was 1609 cm ( sd 64 )  . total cancer incidence rose with increasing height ( table 2 )  . 
comparing women in the tallest group with 075 125 figure 2 : relative risks ( rrs ) and 99% cis per 10 cm increase in height for incident cancer at 17 speci c sites and for total cancer the doted line represents the rr per 10 cm increase in height for total cancer . 
 there is heterogeneity across cancer sites ( contrast test [ 17 degrees of freedom ] = 1152 ; p < 00001 ) mostly because of the greater than average increase in risk with increasing height for colon cancer and for malignant melanoma , and the lower than average risk for lung cancer . 
however , the overall rr of incident cancer in relation to height was not materially altered when we excluded breast cancer cases from our analysis ( rr per 10 cm increase in height 115 , 95% ci 113116 )  . 
 we adjusted our results in gures 1 and 2 and in table 2 by age , region , socioeconomic status , smoking , alcohol , body - mass index , physical activity , age at menarche , parity , and age at rst birth . 
table 3 shows the e ect of adjustment by potential confounding variables on the rr for total cancer per 10 cm increase in height in an analysis restricted to the 1 087 489 women with full information on all adjustment variables . 
compared with the risk with adjustment for age and region only ( rr 114 , 95% ci 113115 ) , additional adjustment by the remaining factors increases the rr slightly to 116 ( 115118 )  . figure 3 shows the rr for total cancer per 10 cm increase in height , and the mean measured height , in subgroups of women de ned by their year of birth , socioeconomic status , smoking status , alcohol con sumption , body - mass index , physical activity , age at menarche , parity , age at rst birth , menopausal status , and use of oral contraceptives and hormone replacement therapy . 
as we expected , women born before 1939 were shorter than women born in 1946 or later ( mean measured height 1599 vs 1615 cm ) , as were women from the lowest compared to the highest socioeconomic tertile ( 1601 vs 1614 cm )  . 
although the risk for total cancer is somewhat higher in women in the lowest tertile of socioeconomic 125 figure 3 : relative risks ( rrs ) and 99% cis per 10 cm increase in height for all incident cancer , by various characteristics at recruitment the dotted line represents the rr per 10 cm increase in height for all women . 
rrs are adjusted as appropriate for age , region , socioeconomic status , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
the rr per 10 cm greater height was 119 ( 95% ci 117121 ) in never smokers , but only 111 ( 108114 ) in current smokers ( p < 00001 for hetero geneity )  . 
 vol 12 august 2011 articles mouth and pharynx oesophagus stomach colon rectum pancreas lung melanoma breast ovary kidney bladder endometrium 2960 1493 1943 18 533 3192 2426 1194 non - hodgkin lymphoma 1630 multiple myeloma leukaemias other and unspecifed 3616 total cancer 42 244 highest socioeconomic third middle socioeconomic third lowest socioeconomic third mean height ( cm ) figure 4 : relative risks ( rrs ) and 95% oated cis ( fcis ) for all incident cancer in relation to height , and by socioeconomic status the baseline category ( rr = 10 ) is women shorter than 160 cm from the highest socioeconomic group . 
rrs are adjusted for age , region , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
rrs are plotted against the mean measured height in each category of height ( < 160 cm , 160165 cm , 165170 cm , 170 cm ) , within categories of socioeconomic status . never smokers number of incident cancers current smokers number of incident cancers figure 5 shows the rrs per 10 cm increase in height by cancer site in never smokers and in current smokers ( results in past smokers are uninterpretable , because they are a heterogeneous group with a wide range of times since last smoking )  . 
the mix of cancers di ers in the two groups with , as expected , a higher proportion of women with lung and other smoking - related cancers in current smokers than in never smokers . 
in never - smokers , heterogeneity across cancer sites was substantially weaker ( p = 0004 ) than in current smokers ( p < 00001 )  . for smoking - related cancers , the rr per 10 cm greater height was substantially smaller in current smokers than in never smokers ( 105 vs 117 , p for di erence = 00004 ; gure 6 )  . 
 * rrs are adjusted for age , region , socioeconomic status , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
the overall pattern of rrs remained similar , with lower risk for smoking - related cancers than for other cancers in current smokers , although the di erence between these risks was reduced ( rr per 10 cm height 102 , 95% ci 097106 , in current smokers and 110 , 103117 , in never smokers ; p for di erence = 005 ) ; for other speci ed cancers , risks remained similar to those in our main analysis ( rrs 118 , 114122 , in current smokers and 119 , 116121 , in never smokers )  . 
 because breast cancer dominates our ndings , we repeated our analyses shown in gure 3 separately for the ve most common cancers in our study : breast , lung , colon , endometrium , and ovary , and for the remaining cancers . 
overall , we did not identify signi cant heterogeneity , by the 12 factors we show in gure 3 , for these cancer sites ( test for heterogeneity aggregated across all characteristics : colon p = 07 , lung p = 02 , breast p = 03 , endometrium p = 05 , ovary p = 02 , remaining cancers p = 02 )  . because there was no strong variation by cancer site in our study except in smokers , we did a meta - analysis of published studies of all - cancer risk , noting for each study the proportion of current smokers in the study population . 
 figure 7 shows details of our study together with ten other prospective studies1 , 3 , 8 , 2128 that have published results in such a way as to allow estimation of the rr of total cancer incidence or mortality per 10 cm increase in height . 
the populations covered include men and women from asia , australasia , europe , and north america , with mean years of birth ranging over three decades ( 1917 to 1946 ) , and with mean heights ranging over 24 cm ( 155 to 179 cm )  . 
there was no signi cant heterogeneity between the results from studies in men ( i for heterogeneity 0% , p = 09 ) or between those in women ( i for heterogeneity 31% , p = 02 ) , but there was a slightly lower height - associated rr in men than in women ( 110 vs 115 , p for di erence < 00001 )  . 
when we excluded the ndings of our study , the summary rr in women was slightly reduced ( summary rr per 10 cm greater height 113 , 95% ci 110116 ; i for heterogeneity 25% ; p = 02 ) , and there was no longer signi cant heterogeneity between studies in men and those in women ( p for di erence = 01 )  . 
all of the mortality studies we included provided rrs adjusted for at least one measure of socioeconomic status , which should have minimised potential confounding due to the relation in many populations between socioeconomic status and cancer survival.29 discussion we identi ed a clear and highly signi cant trend of increasing cancer risk with increasing height in this large prospective study of uk women , with rr for total incident cancer of 116 ( 99% ci 114117 ) for every 10 cm greater height . 
the magnitude of the height - associated increase in cancer risk was similar for women with di erent years of birth , from di erent socioeconomic groups , and across subgroups de ned by alcohol intake , body - mass index , physical activity , age at menarche , parity , age at rst birth , menopausal status , and use of oral contraceptives or hormone replacement therapy . 
by contrast , current smokers had a lower rr for total cancer incidence per 10 cm increase in height than never smokers , and this was largely because the height - associated cancer rrs in smokers were lower for smoking - related than for other cancers . 
 each of the 17 most common speci c sites we assessed included 1000 or more cancers , and together they constitute some 90% of total incident cancers in our study population . 
most previous studies had limited statistical power to study site - speci c cancer risk and tended to focus on a few common cancer sites , and our results for the common cancers are consistent with their ndings.2 , 47 all study participants were routinely linked to records of the nhs central registers and details of every incident cancer and death were coded before noti cation to the study investigators , thus providing complete and nondi erential ascertainment of cancer incidence during follow - up . 
there was excellent correlation between self - reported and measured height , consistent with previous ndings for height and some this cohort.30 , 31 other anthropometric variables nevertheless , we corrected for measurement error , and for changes in height over time , by use of the mean measured height in each category to calculate rr per 10 cm increase in height . 
 as expected , the average height of women in this population was slightly greater the more recently they were born and with increasing socioeconomic status ( gure 3 )  . 
method of chne and thompson18 used to estimate mean heights in height categories . 075 group , age at menarche , parity , age at rst birth , bodymass index , physical activity , smoking status , and alcohol consumption . 
women in higher socioeconomic groups are on average taller ( table 1 ) , and socioeconomic status is related to total cancer incidence ( gure 4 ) , 29 yet the association between height and risk of cancer was similar for women of low , medium , and high socioeconomic status . 
as in other studies that could adjust for a range of potential confounding factors , our results suggest that the relation between height and cancer risk is not due to other known risk factors for cancer.9 our ndings show that the height - related rr of cancer was lower for smoking - related cancers than for other cancers , but only in current smokers . 
in accordance with our ndings kabat and colleagues32 have reported that lung cancer incidence in the womens health initiative study showed a stronger association with height in never smokers than in current or past smokers . 
smoking - related cancers are more common in current smokers than in never smokers , with agestandardised incidence rates of 599 and 176 , respectively per 100 000 women per year , in this cohort . 
the estimated excess age - standardised incidence rate for every 10 cm increase in height for smoking - related cancers is about 30 per 100 000 women per year , both in current and in never smokers ( 599 005 for current smokers and 176 017 for never smokers )  . we found no other modi cation of height - associated rr by the 11 other factors we assessed , either for total cancer , or separately for the ve most common cancers ( breast , lung , colon , endometrium , and ovary )  . 
 there was little variation in height - associated rrs at speci c cancer sites in never smokers , in whom the e ect of height on cancer risk is free from modi cation by smoking . 
in general , studies have found taller people to be at increased risk of a range of cancers with varying causes , with no individual cancer site consistently identi ed as showing no association.2 , 47 our nding of di erences in height - related rr between smokers and never smokers might provide an explanation for some reported inconsistencies in height - associated risk for smoking - related cancers.2 our meta - analysis of height and total cancer risk shows that ndings are very consistent for incidence and for mortality , and in populations from europe , north america , asia , and australasia with mean years of birth ranging over 30 years , and with mean heights ranging from 155 cm to 179 cwomen in these studies were less likely than men to be current smokers ( gure 7 ) and this might partly explain the slightly higher heightassociated rr in women than in men in our metaanalysis . 
the overall result in women is also strongly weighted by the results from the million women study , in which there has been allowance for measurement error , and more extensive adjustment than in the other studies , both of which tended to increase the estimated rr . 
as in any meta - analysis of published data , our ndings need to be interpreted in the knowledge that other studies with relevant data might not have published their results . 
 the similarity of the height - associated rr for di erent cancers and in di erent populations suggests that a basic common mechanism , possibly acting in early life , might be involved.8 adult height reaches its maximum between the ages of 20 and 30 years . 
variation in height relates to genetic and environmental in uences acting mostly in the rst 20 years , or so , of life ; environmental factors , including childhood nutrition and infections , are believed to predominate.3336 hormone levels , especially of growth factors such as insulin - like growth factors ( igfs ) , both in childhood and in adult life , might be relevant.2 , 9 circulating levels of igfs in adulthood and childhood a ect cancer risk ; 3740 igf - i levels in childhood and adolescence are strongly related to skeletal growth , 38 and levels in adulthood , although less strongly , to adult height.41 , 42 another possibility is that height predicts cancer risk because taller people have more cells ( including stem cells ) , and thus a greater opportunity for mutations leading to malignant transformation.43 , 44 height might thus be related to cancer risk through increased cell turnover mediated by growth factors , or through increased cell numbers . 
adult height in european populations has increased by about 1 cm per decade throughout the 20th century.33 , 45 , 46 the increase in adult height during the past century could thus have resulted in an increase in cancer incidence some 1015% above that expected if population height had remained constant . 
all authors approved the report . con icts of interest we declare that we have no con icts of interest . acknowledgments we thank all the women who participated in the study , sta from participating nhs breast screening centres , and family doctors , practice nurses , and other primary - care sta for help with validation measurements . 
we thank gary whitlock for helpful contributions to the manuscript . violence , crime , corruption , and cuts in public spending : how to re - establish cancer control in latin america ? october , 2018 , saw the controversial far - right candidate , jair bolsonaro , win 46% of the presidential vote for brazil . 
 although just falling short of a majority , bolsonaro led a successful campaign that capitalised on fear of rising crime and corruption , championed economic freedom through the promise of privatisation , and pledged the relaxing of gun laws . 
although much of this rhetoric resonates with the populist political agenda in recent years , firm commitments to health - care policy were notably absent from his , as well as his opponents , political programmea critical omission at a time when brazil has been hit with economic and structural weakness , political precariousness , and austerity policies that have capped public expenditure on the growth and sustainability of its health - care syste although unified health system brazils ( sus ) has made substantial progress in recent years , a chronic lack of funds , suboptimal resource allocation , and poor organisation and governance , means that it is struggling to deliver its targets . the prohibition of indeed , these problems are not just isolated incidences in latin america . 
the un and the inter - american commission on human rights declared that the health system in venezuela is in a state of crisis as it witnessed the deaths of at least 16 children in one hospital as a result of deteriorating health facilities , poor sanitation , and a shortage of supplies and medicinesno doubt conditions that are symptomatic of a country suffering from extreme economic instability and political weaknesses , compounded by international humanitarian aid . 
further north , mexicoa country that elected the leftist candidate andrs manuel lpez obrador as president - elect earlier this year to combat similar fears of extreme violence , inequality , and corruptionhas seen its public health insurance scheme , seguro popular , suffer from system fragmentation , underfunding , coverage limitations , and corruption . 
similarly , in honduras , the right - wing president juan orlando hernndez has been accused of rigging elections in late 2017 , in which protestors were killed by security forces , while nicaragua is suffering from extreme political instability , with more than 200 killed in political violence earlier this year amid calls for the former guerrilla daniel ortega to leave the presidential palace . cancera disease reliant on stable , well - funded health systems for continuity and consistency in care delivery will inevitably be affected by these political disturbances . 
 indeed , it is ironic that in the lancet oncologys 2015 commission on cancer control in latin america and the caribbean , paul goss and colleagues attributed the success of the human papillomavirus vaccination programme in brazil to widespread immunisation coverage targets and financial buy - in that were secured by the then ministry of healthan initiative that is now at risk of becoming undone should bolsonaro opt for decreased public expenditure and de - centralised financing . 
hopefully , strong advocacy movements , such as those that feature prominently in brazil , will hold the government to account on their legislative obligationsbut these measures should neither be taken as guaranteed , nor should such movements be expected to become the main drivers of change when governments fail to deliver . the developments unfolding in latin america show that the struggle for democracy is no longer a politics of left versus right , realism versus extremism , or truisms versus tropes . 
in the face of such political upheavals , leaders of these nations would do well to remember that the need for cancer care and control remains unchanged , whoever is in power . 
thus , a key priority for any government is to ensure that there are policies and investments for cancer control that are enshrined in law to ensure there is a level and continuum of care that can be safely delivered to its population irrespective of temporal political disruption . the recommended actions from the 2015 commission on cancer control in latin america and the caribbean still stand today . 
consolidating fragmented health systems , focusing palliative care , improving national cancer registries and cancer control plans , increasing healthcare expenditure , training of oncology and palliative care specialists , and addressing disparities in cancer control are still essential components of effective cancer health systems . 
but only if governments , irrespective of individual party politics , recognise , respond to , and prioritise cancerand indeed all non - communicable diseasesas a persistent and growing health burden , will the fragility of health systems and the needless loss of life be overcome . 
com / journals / lancet / article / piis0140 - 6736 ( 18 ) 32396 - 1 / fulltext for more on iachr report on the venezuelan health system see iachr / media_center / preleases / 2018 / 215.asp for more on the collapse of the venezuelan health system see editorial lancet 2108 ; 391 : 1331 for more on the victory of obrador and the political instability in latin america see com / 2018 / 07 / 10 / opinion / victory - mexican - democracy . html for the 2015 lancet oncology commission on cancer control in latin america and the caribbean see lancet oncol 2015 ; 16 : 140538 vol 19 november 2018 1417 editorial correction to lancet oncol 2016 ; 17 : 163738 correction to lancet oncol 2017 ; 18 : 14931501 correction to lancet oncol 2017 ; 18 : 155556 bestvina cm and vokes e . 
lancet oncol 2017 ; 18 : 155556in this comment , the sixth sentence in the third paragraph should have read grade 3 or worse pulmonary toxicity occurred in 3% of patients treated with brigatinib . 
 this correction has been made as of nov 29 , 2017 , and the printed version is correct . guyton kz , loomis d , grosse y , et al , on behalf of the international agency for research on cancer monograph working group . 
warren foster ( a member of the monograph working group ) has previously contributed to the literature on endocrine disruption , for which he was compensated by exponent through funds provided by the american chemistry council . 
 the necessary amendments to his interest have been declaration of made to the online version of the news piece as of nov 29 , 2017 . tawbi ha , burgess m , bolejack v , in advanced et al . 
pembrolizumab soft - tissue sarcoma and bone sarcoma ( sarc028 ) : a multicentre , two - cohort , single - arm , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 14931501 in this article ( published online on oct 4 , 2017 ) , the interpretation in the summary should have read the primary endpoint of overall response for either cohort . 
this correction has been made to the online version as of nov 29 , 2017 . dedifferentiated characterise correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
lancet oncol 2017 ; 18 : 106175in table s9 in the supplementary appendix of this article , the composite remission in patients with itd and d835 mutations should have been 7 ( 54% )  . 
the appendix has been corrected as of nov 29 , 2017 . vol 18 december 2017 e711 corrections re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper to the lancet go to thelancet / to submit a paper to the lancet oncology go to ees.elsevier.com / thelancetoncology / recommendations in light of the new data presented by raaijmakers and colleagues.3 piet dirix * , sandra nuyts department of radiation oncology , university hospitals leuven , leuven , belgium , piet.dirix@uzleuven.be the authors declared no con icts of interest . raaijmakers cp , roesink jm , dijkema t , houweling ac , terhaard ch . 
first results of a phase iii multicenter randomized controlled trial of intensity modulated ( imrt ) versus conventional radiotherapy ( rt ) in head and neck cancer ( parsport : isrctn48243537 ; cruk / 03 / 005 )  . 
proc am soc clin oncol 2009 ; 27 : abstr lba6006 . call for papersoncology and haematology the lancet and the lancet oncology are announcing plans for issues of each journal to be devoted to speci c topics in oncology and also to haematology . 
the former will be timed to coincide with the european society of medical oncology ( esmo ) congress in milan , italy ( oct 812 , 2010 ) , and the latter with the american society of hematology ( ash ) annual meeting in orlando , fl , usa ( dec 47 , 2010 )  . 
we would like to invite submissions of high - quality original research about cancers of the breast , lung , prostate , and gastrointestinal tract , or on any topic in haematology or haematological oncology . 
accepted papers will be published in either the lancet or the lancet oncology via fast - track peer review to coincide with either the esmo or ash annual meetings , as appropriate . 
 submissions to coincide with the esmo annual meeting must be received by june 25 , 2010 , and those for the ash annual meeting by oct 1 , 2010 , via either the lancet or the lancet oncologys online submission systems . 
please state in your covering letter that the submission is in response to this call for papers . if your work is being presented at either meeting and falls under an embargo policy , please tell us the date and time of the presentation , and whether the study is to be presented orally or in a poster . 
if your paper is accepted , online publication can be scheduled to coincide with the presentation and comply with any press embargo . jane godsland , zo mullan , richard turner , david collingridge the lancet ( jg , zm , and rt ) and the lancet oncology ( dc ) , 32 jamestown road , london nw1 7by , uk errata relling mv , altman rb , goetz mp , evans we . 
clinical implementation of pharmacogenomics : overcoming genetic exceptionalislancet oncol 2010 ; 11 : 50709the acknowledgment in this comment ( published online first on april 21 , 2010 ) should have read we thank colleagues in nihs pharmacogenomics research network . 
in the second paragraph , the last sentence was misspelt and should have read despite evidence linking pharmacogenomic variation with drug exposure , toxic e ects , and e cacy , many clinicians , regulators , and payors hold pharmacogenetic evidence to excessively high standards . 
lancet oncol 2010 ; 11 : 42938in this article , the acknowledgments statement should also have included : the uk medical research council funded the original all97 / 99 trial and supported the childhood leukaemia working party . 
lancet oncol 2007 ; 8 : 31722in this article , the equation for acpgbi in panel 2 should read loge [ r / ( 1r ) ] = ( 4859 + total score )  . 
additionally , in table 3 , 158 was added in error next to the heading clinicopathological staging . 516 vol 11 june 2010 4 gy versus 24 gy radiotherapy for patients with indolent lymphoma ( fort ) : a randomised phase 3 non - inferiority trial peter j hoskin , amy a kirkwood , bilyana popova , paul smith , martin robinson , eve gallop - evans , stewart coltart , timothy illidge , krishnaswamy madhavan , caroline brammer , patricia diez , andrew jack , isabel syndikus summary background follicular lymphoma has been shown to be highly radiosensitive with responses to doses as low as 4 gy in two fractions . 
this trial was designed to explore the dose response for follicular lymphoma comparing 4 gy in two fractions with 24 gy in 12 fractions methods fort is a prospective randomised , unblinded , phase 3 non - inferiority study comparing radiotherapy given as 4 gy in two fractions with a standard dose of 24 gy in 12 fractions . 
entry criteria included all patients aged over 18 years , having local radiotherapy for radical or palliative local control , with follicular lymphoma or marginal zone lymphoma , who had received no previous treatment for at least 1 month before . 
radiotherapy target sites were randomised ( 1 : 1 ) with minimisation strati ed by histology ( follicular lymphoma vs marginal zone lymphoma ) , treatment intent ( palliative or curative ) and centre . 
after a median follow - up of 26 months ( range 039754 ) , 91 local progressions had been recorded ( 21 in the 24 gy group and 70 in the 4 gy group )  . 
mucositis was the most common event in the 24 gy group ( two patients with acute mucositis and two with late mucositis ; all grade 3 ) and was not reported in the 4 gy group . 
 the most common acute e ect was pain at the site of irradiation ( two patients in the 4 gy group , one patient in the 24 gy group ; all grade 3 ) , and the most common late e ect was fatigue ( two patients in the 4 gy group , one patient in the 24 gy group ; all grade 3 )  . interpretation 24 gy in 12 fractions is the more e ective radiation schedule for indolent lymphoma and should be regarded as the standard of care . 
a large randomised study1 con rmed that a dose of 24 gy in 12 fractions was as e ective for local control as 40 gy in 20 fractions in terms of overall response and within eld progression . evidence for the e cacy of even lower doses has been reported over many years with the exquisite sensitivity of follicular lymphoma described using doses as low as 075 gy given as total body irradiation.2 an initial report3 of the use of 4 gy in two fractions in advanced indolent lymphoma was published in 1994 , with 89% of patients having a response . 
since then , several centres have reported similarly impressive high responses.4 the largest of these series comes from a study5 in the netherlands in which 96 patients with follicular lymphoma received 4 gy in two fractions . 
this study5 reported that 92% of patients had a response , with 61% achieving a complete response , and a median duration of complete remission of 42 months . against this background of an increasing number of studies con rming that 4 gy in two fractions was an e ective dose in the local treatment of follicular lymphoma , we did a randomised trial in patients receiving local external beam radiotherapy for control of follicular lymphoma , with the aim of showing that a lower dose of 4 gy in two fractions ( easier to give with hopefully fewer toxic e ects ) is as e ective in terms of local control as the standard 24 gy in 12 fractions . methods participants and study design the protocol for this study can be found online . 
the aim of the trial was to demonstrate that low - dose radiotherapy ( 4 gy ) is as e ective as conventional dose radiotherapy ( 24 gy ) in terms of tumour progression within the irradiated eld . 
as progression was to be assessed locally , it was decided that radiotherapy target sites would be randomised rather than patients , therefore individual patients could be randomly assigned more than once . treatment for control of patients were eligible for this study if they had a histologically con rmed diagnosis of follicular lymphoma and were to receive local radiotherapy with the aim of local control . 
initially , this trial was open only to patients local receiving palliative symptoms , but subsequently , protocol amendments allowed patients having radiotherapy for early stage localised disease in a curative setting to be included as well as those with marginal zone lymphoma . 
we excluded patients with histology results other than follicular lymphoma ( and later marginal zone lymphoma ) , those who had chemotherapy within 4 weeks of radiotherapy and a predicted prognosis of less than 3 months . the east of englandcambridge south research ethics committee reviewed the study and all patients provided written informed consent . randomisation and masking central randomisation was through the cancer research uk and university college london cancer trials centre using the minim6 progra sites were randomly assigned ( 1 : 1 ) to either 4 gy or 24 gy radiotherapy using minimisation strati ed by histology ( follicular lymphoma vs marginal zone lymphoma ) , treatment intent ( palliative vs curative ) and centre . 
we used no blinding since sham radiotherapy was not considered appropriate and followup was undertaken by the treating clinicians . procedures we delivered treatment using external megavoltage x - ray beams unless the lesion was super cial , when electrons or kilovoltage x - rays were allowed . 
 we treated some patients with ap - pa elds using orthogonal x - ray localisation whereas we treated most patients using 3d ct - based volume de nition and conformal beam arrangements . 
treatment was delivered using 2 gy per fraction , treating daily monday to friday . we monitored patients for acute toxic e ects before and during radiotherapy , and at 4 weeks after radiotherapy . 
 * flipi score was calculated using the stage ( worst seen at randomisation ) , baseline lactate dehydrogenase concentration , baseline hb , and number of nodal sites ( total seen , including earlier randomisations )  . 
 quality of life was recorded at each follow - up using the equation 5d ( eq - 5d ) health questionnaire . outcomes the primary outcome was time to local progression and was analysed on an intention - to - treat basis with all radiotherapy sites included . 
secondary endpoints were overall survival , response , toxic e ects , and quality of life . statistical analysis the study was designed as a non - inferiority trial to reliably exclude the chance that 4 gy might increase the rate of local progression at 2 years by more than 10% , which translates to the hr of 137 . at 2 years , we assumed that 60% of radiotherapy sites would be progression - free and using a one - sided 5% signi cance level and 90% power this requires 364 events ( a sample size of 650 target sites )  . we randomly selected the radiotherapy target site used in the analysis of overall survival ( each patient included only once ) before analyses were done . 
we used a cox proportional hazards model to estimate the hazard ratio ( hr ) between the the proportionality assumption using the schoenfeld residuals.7 all analyses were done with stata version 12.1. 
ph had full access to all of the data and the nal responsibility to submit for publication . results we randomly assigned 614 sites from 548 patients in 43 uk centres ( listed in the appendix ) to treatment groups vol 15 april 2014 299 allocated to radiotherapy 24 gy 315 allocated to radiotherapy 4 gy 3 did not receive trial radiotherapy 1 clinicians decision 1 treatment sites would overlap 1 patient too unwell 614 sites randomised 6 did not receive trial radiotherapy 1 emergency radiotherapy needed 1 patient refusal 1 did not want 24 gy 1 patient wanted a lower dose 1 surgery given , radiotherapy no 1 unknown ( missing treatment longer needed form ) 293 received trial radiotherapy 312 received trial radiotherapy 1 did not complete treatment ( patients choice after 6 gy ) 4 did not receive randomised dose 1 error ( received 8 gy ) 3 trial stopped , advised to switch groups 292 completed full protocol treatment 308 completed full protocol treatment 299 available for analysis * 315 available for analysis * 3 withdrew after treatment 296 available for follow - up 315 available for follow - up figure 1 : trial pro le all numbers refer to randomised sites , not patients . 
 * all radiotherapy target sites are included in the analysis of local progression ( the primary endpoint )  . the committee between april 7 , 2006 , and june 8 , 2011 , when the independent data monitoring ( idmc ) trial . 
although 94% of recommended halting recruitment had been completed , the idmc felt that the study question had been answered and patients should not be randomly assigned to a treatment believed to be inferior . 299 sites were randomly assigned to receive 24 gy and 315 sites to receive 4 gy . 
the medians seemed to di er between the two groups , with patients in the 24 gy group having longer times between diagnosis and randomisation than those in the 4 gy group ( 116 months vs 70 months ) , however , when we compared the distribution of the times further , we did not feel there was an imbalance . because of the sometimes lengthy periods between diagnosis and randomisation , patients had often received other treatments . 
151 ( 25% ) had received previous radiotherapy and 207 ( 34% ) previous chemotherapy ; these were also well balanced between the treatment groups ( table 1 )  . see online for appendix articles 482 tumour biopsies were reviewed centrally ; diagnoses could not be con rmed for 67 ( 14% ) of these samples ( 48 had insu cient material , 11 were reported to show no clear evidence of lymphoma , and another eight showed reactive changes only )  . 
of the 415 for which diagnoses were given , 386 ( 93% ) were follicular lymphoma and 46 ( 11% ) were marginal zone lymphoma ( table 1 )  . compliance with radiotherapy was very good ( gure 1 )  . 
 nine patients ( nine target sites ) were withdrawn before treatment started ; of target sites , 292 ( > 99% ) of the 293 sites in the 24 gy group and 308 ( 99% ) of the 312 sites in the 4 gy group received the complete , randomised dose . 
 the remaining stable disease ( including < 30% regression ) 22 ( 8% ) partial regression ( > 30% ) 53 ( 23% ) stable disease ( including < 30% regression ) 19 ( 8% ) 78 ( 32% ) 40 ( 16% ) all patients * complete regression partial regression ( > 30% ) progression total follicular lymphoma complete regression progression total marginal zone lymphoma complete regression partial regression ( > 30% ) stable disease progression total 24 gy 4 gy 176 ( 68% ) 137 ( 49% ) 60 ( 23% ) 90 ( 32% ) 44 ( 16% ) 2 ( < 1% ) 10 ( 4% ) 152 ( 67% ) 116 ( 48% ) 2 ( < 1% ) 9 ( 4% ) 24 ( 71% ) 7 ( 21% ) 3 ( 1 % ) 21 ( 55% ) 12 ( 32% ) 4 ( 11% ) 1 ( 3% ) data are number of sites ( % )  . 
 * patients who withdrew before treatment or with missing treatment data have been excluded , as have the three patients who switched from 4 gy to 24 gy after the trial was closed . 
there were also 43 ( 20 in the 24 gy group and 23 in the 4 gy group ) with no measurable disease at baseline and 17 ( 13 in the 24 gy group and four in the 4 gy group ) with missing response data . 
the exclusion of sites without measurable disease at baseline and those with missing response data showed that 236 ( 91% ) of 260 sites in the 24 gy group and 227 ( 81% ) of 281 in the 4 gy group had a complete or partial response ( p = 000095 )  . 
progressive disease was noted in more target sites in the 4 gy group than in the 24 gy group , but numbers in both groups were small ( two [ < 1% ] in the 24 gy group vs 10 [ 4% ] in the 4 gy group )  . 
although the marginal zone group was small ( and the di erence between 24 gy and 4 gy not signi cant , p = 071 ) the responses showed a similar pattern ( table 2 )  . we also looked at the subgroups of patients with early stage disease and those treated with curative intent . 
 although there were more responses , the di erence between the groups was slightly larger and remained statistically signi cant ( table 3 )  . after a median follow - up of 26 months ( 039754 ) , 91 local progressions had been recorded ( 21 in the 24 gy group and 70 in the 4 gy group ) giving an hr for time to local progression of 342 ( 95% ci 210557 , p < 00001 , gure 2a )  . 
although this is well below the 364 events required in the sample size calculation , it is not expected that longer follow - up will reduce the hr to a level that would meet the non - inferiority margin ( di erence in local progression - free interval at 3 years currently 198% ; 95% ci 278 to 134 )  . to explore the e ect of multiple randomisations within a patient , we did a sensitivity analysis using just one observation from each patient ( appendix )  . 
the hr was just below 1 in all samples , therefore there is currently no evidence to suggest that 4 gy has a negative e ect on overall survival . as patients often had more than one site of disease , many received additional anti - cancer therapies before local progression . 
this treatment was systemic therapy or radiotherapy either given to the target site for residual disease ( 12 patients ) or more often due to overlap with an adjacent site receiving radiation . 
this analysis reduced the number of events by seven , but the hr remained similar ( 373 ; 95% ci 223622 , p < 00001 )  . we did subgroup analyses for baseline size , treatment intent , karnofsky score , stage , time from diagnosis , and follicular lymphoma international prognostic index ( flipi ) score . 
we did not note any evidence of a di erence in treatment e ect within any of the subgroups ( appendix )  . we also tested the group of patients with con rmed follicular lymphoma treated with curative intent . 
this was a small group of only 134 patients ( 16 events ) but 4 gy remained inferior in terms of local progression ( hr 637 , 95% ci 1442818 , p = 00051 )  . toxic e ects were low , with just eight ( 3% ) sites in the 24 gy group and four ( 1% ) in the 4 gy group having grade 3 or 4 acute toxic e ects . 
a similar pattern was seen in late e ects with 105 sites ( 37% ) in the 24 gy group and 71 sites ( 23% ) in the 4 gy group a ected . we recorded quality of life using the eq - 5d form at 7 set timepoints and yearly thereafter , only patients with a single randomisation ( 228 in the 24 gy group and 239 in the 4 gy group ) were included in the analysis . 
we did not note any di erence between the two treatments ( p = 092 ; appendix )  . indolent b - cell non - hodgkin discussion our data suggest that , although 4 gy is an e ective dose local progression - free survival is inferior to a higher dose of 24 gy in 12 fractions . 
we noted no di erence in overall survival between groups ; however , these data are relatively lymphoma , 24 gy 4 gy number at risk 24 gy 4 gy time since randomisation ( months ) number at risk 24 gy 4 gy figure 2 : progression - free survival for all sites ( a ) and overall survival for one site per patient ( b ) immature , and we will re - analyse these data as further follow - up data are obtained and more events recorded . in our previous study1 of 24 gy compared with 40 gy in indolent lymphoma , 92% of patients had a response , similar to the 91% seen in this cohort , despite di erences in the populations : 62% of patients in the earlier study were treated with radical intent for stage one disease whereas in the current study , 60% of patients were treated with palliative intent and only 40% radically . 
while this is similar to the 91% in the 24 gy group , a striking , much larger , di erence is apparent in vol 15 april 2014 articles 24 gy 4 gy panel : research in context acute toxic e ects diarrhoea mucositis fatigue pain in target dry mouth oral candidiasis cerebrovascular ischaemia total late toxic e ects mucositis fatigue pressure sore constipation pharyngitis dry mouth total neutropenia and thrombocytopenia 1 * ( 04% ) any ( each patient only counted once ) 4 ( 13% ) 1 ( 04% ) 2 ( 07% ) 2 ( 07% ) 1 ( 04% ) 1 ( 04% ) 1 ( 04% ) 8 ( 28% ) 2 ( 07% ) 1 ( 04% ) 1 ( 04% ) 1 ( 04% ) 1 ( 03% ) 2 ( 07% ) 1 ( 03% ) 2 ( 06% ) 1 ( 03% ) 1 ( 03% ) 4 ( 13% ) any ( each patient only counted once ) 4 ( 14% ) all events were grade 3 , except where indicated . 
at the time of developing the protocol in 2004 , we did a formal literature search using medline and search terms follicular lymphoma , lymphoma , indolent lymphoma , low grade lymphoma , and radiotherapy . 
we identi ed no relevant randomised trials in the cochrane central register of controlled trials . interpretation the results of this trial con rm that 4 gy is e ective in many patients but that it is inferior to 24 gy in terms of time to local progression in both the radical and palliative setting when treating follicular lymphoma . 
4 gy has , however , a potential role as a simpler , shorter , and more pragmatic schedule in patients being treated for local control in the palliative setting , in which durable response might be less important . 
the proportion of patients with a complete response in previously published series of 4 gy in follicular lymphoma varied from 36% to 84% with a median value of 46% , 4 which is remarkably similar to that achieved in this study . 
it would seem reasonable therefore to propose that the di erence we noted between 4 gy and 24 gy regimens is real and that on balance , 24 gy in 12 fractions should be deemed the standard in this setting ( panel )  . both radical early stage and more advanced stage palliative patients were included in this study . 
however , in some patients with advanced disease and limited life span 4 gy is a very convenient and pragmatic alternative . the inclusion of marginal zone lymphoma in the latter part of the trial was a re ection of slow accrual at the time and was successful in signi cantly increasing the rate of patient entry . 
although it is di cult to draw any de nitive conclusions for marginal zone lymphoma as a distinct subgroup , the overall pattern of response was similar to that seen in follicular lymphoma and it would seem reasonable to conclude that 24 gy is better than 4 gy in this group as well , and should be considered the standard . the design of this trial allowed multiple sequential randomisations in one patient , which has been criticised in the past . 
however , we applied strict criteria to this approach ensuring response and toxic e ects were speci c to every site , and the results of the sensitivity analysis provide further reassurance that this feature did not compromise the results as presented here . 
premature closure of a trial is always a concern , however , the recommendation by the idmc in this case was as a result of mature data , the trial having been running for more than 5 years at the time of the decision and at the time of closure 94% of the planned accrual had been reached . despite the results of this trial , that a dose as low as 4 gy can achieve responses in a signi cant proportion of the population remains remarkable , and , indeed , more than 40% of sites were in complete remission after this dose . 
these events include apoptosis with inactivation of bcl - 2 overexpression , which is a characteristic of follicular lymphoma.8 this inactivation might result in overexpression of p53 and caspase - 8 and caspase - 9 . 
macrophage activation might also be upregulated.9 with such potent biological e ects within the cell , it is therefore tempting to suggest that a dose in excess of 4 gy , but much lower than 24 gy , could be optimum and further studies exploring intermediate doses might be of biological interest . toxic e ects with such low radiation doses are not a dose - limiting issue , unlike the situation in the radical treatment of epithelial cancers . 
however , we noted about half the incidence of acute grade 3 or higher toxic e ects in the 4 gy group compared with that in the 24 gy group . 
 this does not detract from the recommendation that 24 gy should be the standard treatment for indolent b - cell lymphoma , but supports the use of 4 gy for palliative treatment of patients with poor performance status . 
combination therapy using low - dose radiotherapy and other drugs that might similarly induce apoptosis , such as rituximab , could be of interest.10 in - vitro evidence suggests rituximab can enhance radiation - induced apoptosis in lymphoma cells and combination schedules with low - dose radiotherapy might therefore result in both optimum local control and carry the advantage of systemic e ects for more widespread disease control . contributors ph was chief investigator and lead author . 
ph , is , mr , eg - e , km , and cb were members of the trial management group and local principal investigators responsible for trial design , data collection , and interpretation . 
ti and sc were principal investigators , major contributors of data , and involved in interpretation , writing , and approval of report . declaration of interests we declare that we have no competing interests . acknowledgments we thank all patients , participating centres and sta , the lymphoma research trust , and members of the trials steering committee and independent data monitoring committee . this trial was funded by cancer research uk ( cruk / 05 / 015 ) and conducted by the cancer rresearch uk and ucl cancer trials centre . corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 editorial impact of brexit on cancer care and research on june 23 , 2016 , the uk will vote in a referendum on whether to leave the european union ( eu )  . 
in so doing , they join other scientists and clinicians who have publicly declared their belief that it would be best to remain . part of the inherent di culty with this debate is that the repercussions of leaving can only be speculated on : this would be the rst time a member state has left the eu . 
 finally , limiting the free movement of researchers between the eu and uk would , at best , leave the uk without access to some of the best researchers and clinicians in the world , and , at worst , cause a brain drain of the brightest international talent out of the uk . almost all scienti c researchers and clinicians who have spoken out in this debate have expressed their preference to remain in the eu , citing the need to maintain the position of strength that the uk currently occupies . 
to rock this solid foundation would undermine the provision of care to all patients with cancernot just for those patients currently in multicountry clinical trials , or under the care of an eu specialistand would weaken vital research that could save lives in the future . 
 the lancet oncology see comment pages 556 and 558 see editorial lancet haematol 2016 ; 3 : e99 to read more about scientists support for staying within the eu see cms / s / 0 / e1ba8974 - d981 - 11e5a72f - 1e7744c66818 . html#axzz41boanmda , and writtenevidence / committeeevidence.svc / evidencedocument / science - andtechnology - committee - lords / relationship - between - eumembership - and - theeffectiveness - of - uk - science / written / 24828.pdf improved drug access in low and middle - income countries on march 31 , 2016 , glaxosmithkline announced that it would no longer le for patent protection on its products in low - income countries , and would seek to grant licences to generic manufacturers to supply generic versions of its products in low - income and middle - income countries ( lmics )  . 
moreover , in response to the growing burden of cancer in lmics , the company will commit its future oncology products to patent pooling , possibly via the medicines patent pool . 
 the medicines patent pool is a public health organisation endorsed by the united nations , which works with governments , industry , and key stakeholders to expand access to essential medicines in lmics by encouraging generic manufacturing and the development of new drug formulations . 
currently , the organisation only provides access to infectious disease - related drugs , but the addition of oncology medicines to the portfolio would be a welcome acknowledgement of the growing burden of non - communicable diseases in lmics . 
notably , this programme includes anastrozole , tamoxifen , and letrozole for the treatment of breast cancer . with patents expiring soon on many drugs , including , for the rst time , biological agents , challenges surrounding access to highly e cacious medicines are set to increase . 
thus , the provision of oncology drugs from pharmaceutical companies in expanded access schemes to lmics might set a precedent for improved distribution of anticancer in the drugs to the most vulnerable patients world . 
patients preferences for adjuvant chemotherapy in early stage breast cancer : is treatment available ? br j cancer 2001 ; 84 : 155785 . palda va , llewellyn - thomas ha , mackenzie rg , et al . 
clin therap 1998 ; 20 : c2025 . 14 cruzan v director , missouri department of health , 497 vs 261 : 1990 . errata migliorati ca , siegel ma , elting ls . 
in this personal view , the fth sentence of the second paragraph in the future directions section ( p 512 ) should have read : yet , in bisphosphonate - associated osteonecrosis , the maxilla is a ected much more than it is in osteoradionecrosis , suggesting occurrence of a di erent form of vascular pathogenesis or other mechanism . sobrero a , khne c - h . 
in this debate , the fourth sentence of the last paragraph in the argument for the proposal ( p 516 ) should have read : however , these data also mean that in patients who will probably relapse with no adjuvant treatment , one in ve will not relapse with uorouracil and leucovorin and one in three will not relapse with adjuvant folfox . azizi aa , haberler c , czech t , et al . 
in this case report , the rst sentence of the fth paragraph ( p 522 ) should have read : restaging in october , 2004 , revealed progression of the 15 known lesions as well as 12 new pulmonary lesions ( gure 2a , c )  . vol 7 july 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology correction to lancet oncol 2019 ; 20 : 143243 corn pg , heath ei , zurita a , et al . 
lancet oncol 2019 ; 20 : 143243in this article , the national institutes of health and national cancer institute should have been included in the list of funders in the summary . 
this correction has been made to the online version as of jan 2 , 2020 . vol 21 january 2020 corrections articles dose - dense cisplatin - based chemotherapy and surgery for children with high - risk hepatoblastoma ( siopel - 4 ) : a prospective , single - arm , feasibility study jzsef zsiros , laurence brugieres , penelope brock , derek roebuck , rudolf maibach , arthur zimmermann , margaret childs , daniele pariente , veronique laithier , jean - bernard otte , sophie branchereau , daniel aronson , arun rangaswami , milind ronghe , michela casanova , michael sullivan , bruce morland , piotr czauderna , giorgio perilongo , for the international childhood liver tumours strategy group ( siopel ) * summary background the objective of this study was to establish the e cacy and safety of a new treatment regimen consisting of dose - dense cisplatin - based chemotherapy and radical surgery in children with high - risk hepatoblastoma . methods siopel - 4 was a prospective single - arm feasibility study . 
patients aged 18 years or younger with newly diagnosed hepatoblastoma with either metastatic disease , tumour in all liver segments , abdominal extrahepatic disease , major vascular invasion , low fetoprotein , or tumour rupture were eligible . 
treatment consisted of preoperative chemotherapy ( cycles a1a3 : cisplatin 80 mg / m per day intravenous in 24 h on day 1 ; cisplatin 70 mg / m per day intravenous in 24 h on days 8 , 15 , 29 , 36 , 43 , 57 , and 64 ; and doxorubicin 30 mg / m per day intravenous in 24 h on days 8 , 9 , 36 , 37 , 57 , and 58 ) followed by surgical removal of all remaining tumour lesions if feasible ( including liver transplantation and metastasectomy , if needed )  . 
patients whose tumour remained unresectable received additional preoperative chemotherapy ( cycle b : doxorubicin 25 mg / m per day in 24 h on days 13 and 2224 , and carboplatin area under the curve [ auc ] 106 mg / ml per min per day intravenous in 1 h on days 1 and 22 ) before surgery was attempted . 
with a median follow - up of 52 months , 3 - year event - free survival was 76% ( 95% ci 6587 ) and 3 - year overall survival was 83% ( 7393 )  . 
60 ( 97% ) patients had grade 34 haematological toxicity ( anaemia , neutropenia , or thrombocytopenia ) and 44 ( 71% ) had at least one episode of febrile neutropenia . 
other main grade 3 or 4 toxicities were documented infections ( 17 patients , 27% ) , anorexia ( 22 , 35% ) , and mucositis ( seven , 11% )  . 
18 serious adverse events ( including two deaths ) re ecting the observed side - e ects were reported in the trial ( the most common was ototoxicity in ve patients )  . interpretation the siopel - 4 treatment regimen is feasible and e cacious for complete remission at the end of treatment for patients with high - risk hepatoblastoma . funding cancer research uk and cancer research switzerland / oncosuisse . introduction despite important progress in the cure of children with localised hepatoblastoma , the prognosis of patients with metastatic disease remains poor , with 5 - year event - free survival of 2128% and 5 - year overall survival of 2757%.114 only the most recently published study of the international childhood liver tumours strategy group ( siopel - 3 ) , 15 which used intensive multiagent chemotherapy and aggressive surgery , managed to achieve a better outcome for these children ( 3 - year eventfree survival 56% , 3 - year overall survival 62% )  . 
to further improve the number of children cured with high risk , in particular metastatic hepatoblastoma , new and therapeutic approaches are needed that can increase treatment e cacy without excessive toxicity . data from earlier studies suggest that cisplatin is the key chemotherapeutic drug in the treatment of hepatoblastoma , but its optimum schedule and dose in this setting is not yet established . 
 according to these results , high risk was de ned as involving all four hepatic sections ( pretumour treatment extent of disease [ pretext ] - iv23 , 24 ) , or presence of distant metastases , or tumour extension into the vena cava or all three hepatic veins , or into the main or both branches of the portal vein , or extrahepatic intraabdominal disease , or serum fetoprotein ( afp ) less than 100 g / l at diagnosis , or tumour rupture . 
tumour extension was assessed by pretreatment imaging ( ultrasound , ct , and mri ) according to the pretext system.23 , 24 for the purposes of eligibility for this trial , pulmonary lesions were judged to be metastases if there was one nodule more than 10 mm or several nodules with at least one more than 5 mbiopsy and histological evaluation of the primary tumour was mandatory for all children . chemotherapy was given as procedures treatment consisted of three cycles of preoperative chemotherapy ( cycles a1a3 ) followed by surgical removal of all remaining tumour lesions if feasible ( including liver transplantation and metastasectomy if needed ) followed by postoperative chemotherapy ( cycle c )  . 
for infants and children with bodyweight less than 10 kg and in case of delay in chemotherapy because of toxicity , dose reduction was recommended by the protocol ( appendix )  . 
to assist optimum treatment decisions by the treating centres , the protocol provided detailed guidelines tumour assessment and surgery including the issue of di cult or extreme resection , liver transplantation , and metastasectomy ( appendix )  . 
ca * = carboplatin area under the curve ( auc ) 106 mg / ml per min per day intravenous infusion in 1 h ; on days 1 and 22 in cycle b . 
empty circle = assessment of response and resectability . vol 14 august 2013 articles which is a good surrogate for event - free survival and was thought to be an adequate outcome measure for this trial . 
tumour response and resectability were assessed by imaging and serum afp concentration after each chemotherapy cycle according to the following criteria : complete response , 67 patients enrolled 62 eligible 5 misdiagnosis 1 primary surgery 60 complete or partial response after preoperative chemotherapy 1 stable disease after preoperative chemotherapy , withdrawn before surgery * 2 death before surgery 1 withdrawn before surgery 1 no documentation of surgery 1 unresectable disease 2 surgical death 6 liver resection in the presence of residual lung lesions ( small lesions ) , no metastasectomy 1 liver resection in the presence of residual lung lesions ( unresectable ) , no metastasectomy 46 complete surgical resection of all remaining lesions after preoperative chemotherapy 4 no complete remission 49 in complete remission at the end of treatment figure 2 : enrolment , treatment , and outcome of patients * withdrawn after second preoperative chemotherapy cycle ( a2 ) because of grade 3 ototoxicity . 
unresectable because of multiple lung lesions , no surgery attempted . de ned as no evidence of disease and normal afp ( for age ) ; partial response , de ned as any tumour volume shrinkage and a decrease of afp greater than 1 log below the original measurement ; stable disease , de ned as no tumour volume change and no change or less than 1 log fall of afp ; progressive disease , de ned as unequivocal increase of tumour size in one or more dimensions or any unequivocal increase of the afp concentration , or both ; complete surgical resection , de ned as total macroscopic removal of all tumour lesions ; and complete remission , de ned as no evidence of tumour on imaging and normal ( for age ) serum afp . 
toxicity was graded according to the national cancer institute common toxicity criteria for adverse events version 3.0 and the brock grading for ototoxicity.25 the trial was monitored for excessive toxicity by regular evaluation of severe adverse event reports and toxicity data . 
 these data were reported to an independent data monitoring committee that assessed and judged observed toxicity at least once a year and made recommendations for amendments or closing of the study if necessary . 
 statistical analysis we used simons two - stage optimal design with a probability of complete remission in 60% of patients or less ( from the siopel - 3hr study ) as the null hypothesis and a probability of 80% of patients or higher as the alternative hypothesis . 
the sample size was n1 = 19 for stage 1 and n2 = 34 for stage 2 , resulting in a maximum sample size of 53 if the trial was not stopped after stage 1 analysis . 
the stage 1 evaluation was done on the rst 19 treated patients in february , 2007 , and concluded that early stopping criteria were not met and the trial could be continued . 
a stopping rule for safety was devised on the basis of the number of patients in whom possible treatment - related severe adverse events developed , including death and grade 4 toxic e ects . 
the corresponding author had full access to all data in the study and had nal responsibility for the decision to submit for publication . 836 vol 14 august 2013 articles results between jan 1 , 2005 , and aug 31 , 2009 , 67 patients were enrolled in the trial from 18 countries worldwide ( gure 2 )  . 
no children were excluded because of abnormal cardiac , renal , or liver function or pre - existing hearing loss . table 1 shows the number of chemotherapy cycles given in total and per patient . 
the cumulative delay in the administration of the second and third cycles of preoperative therapy ( a2 and a3 ) because of toxicity ranged from 4 to 63 days ( median 7 days , mean 10 days ) ; reasons for early start of the next cycle of chemotherapy in some patients were good haematological recovery and clinical condition . 
two patients who withdrew from the study received some non - protocol chemotherapy after withdrawal . 60 ( 98% , 95% ci 91100 ) of 61 evaluable patients ( one child underwent primary hepatectomy ) had a partial response to preoperative chemotherapy . 
of the 39 patients with initial lung metastases , a complete response of the lung lesions was achieved in 20 patients and partial response in 18 patients , with preoperative chemotherapy alone ( 97% patients responded )  . 
in one patient no evaluation of the lung lesions was done . in 53 ( 85% ) of the 62 patients , complete macroscopic resection of the primary tumour was achieved with partial hepatectomy ( n = 37 ) or liver transplantation ( n = 16 )  . 
in ve patients , no surgery was attempted because of unresectable disease ( one patient ) , early death ( two ) , or withdrawal before surgery ( two )  . 
 in seven patients with residual lung lesions after chemotherapy , the liver tumour was resected but no metastasectomy was done ( gure 2 )  . 16 patients were transplanted , eight with pretext - iv , ve with pretext - iii , and three with pretext - ii tumour . 
none of these seven patients had a ( pulmonary ) relapse . given according of the 46 patients with complete resection of all tumour lesions , one developed recurrent lung lesions before the end of treatment . 
 conversely , six patients with small residual pulmonary lesions after liver surgery who did not undergo metastasectomy achieved complete remission with postsurgical chemotherapy total 49 ( 79% , 95% ci 6788 ) of 62 patients were in complete remission at the end of therapy , including the one who underwent primary hepatectomy , close to the prespeci ed goal of 80% . 
one patient died of postoperative complications , in one no reported toxicity in cycles a1a3 number of patients with reported toxicity in cycle b number of patients with reported toxicity in cycle c number of patients number of cycles ( continued from previous page ) ( one , fungal infection in profound neutropenia ) , surgical compli cations ( two , one intra operative bleeding and shock ; one , lethal postoperative wound infection ) , or tumour bleeding ( one , spontaneous intratumour bleeding with irreversible haemorrhagic shock before the second cycle of chemo therapy )  . 
the kaplan - meier estimate of 3 - year eventfree survival was 76% ( 95% ci 6587 ) and of overall survival was 83% ( 95% ci 7393 ) for the whole group ( gure 3 )  . 
 the relapses occurred 548 months after the end of treatment at the following sites : locoregional ( three ) , lungs ( one ) , unknown ( one )  . 
two of the ve patients died of their cancer , the other three had a second complete remission . 19 of the 20 patients with metastatic disease with complete response in the lungs were in complete remission at the end of treatment . 
in two of the 18 children the lung lesions remained unresectable ; in one the liver tumour was resected but no metastasectomy was done , and in the other no surgery was attempted . 
of the remaining ten patients , six did not achieve complete remission because of residual pulmonary disease : in one patient lung lesions disappeared with preoperative chemotherapy but recurred after liver surgery ; in two patients pulmonary lesions were diminished , but remained unresectable ; and in three patients no visible tumour was left , but afp remained slightly raised at the end of treatment . 
3 - year eventfree survival was 77% ( 95% ci 6390 ) and 3 - year overall survival was 79% ( 95% ci 6692 ) for the 39 patients with metastasis . 
in an exploratory analysis , 27 ( 78% ) of 37 patients with metastatic disease and afp higher than 100 g / l had achieved continuous complete remission at the end of therapy . 
 in 11 of the 16 patients with initial pretext - iv tumour , chemotherapy led to downstaging of the liver mass to category iii in six , category ii in four , and category i in one patient as assessed preoperatively . 
cycles a1a3 were given to 62 patients ( in total 182 cycles ) , additional preoperative chemotherapy ( cycle b ) to 13 patients , and postoperative chemotherapy ( cycle c ) to 37 patients . 
 table 2 : short - term toxicity in the siopel - 4 trial vol 14 august 2013 articles surgery was attempted because of unresectable lung disease , and two patients were withdrawn before surgery . 
3 - year event - free survival was 73% ( 95% ci 5196 ) and overall survival was 80% ( 95% ci 60100 ) for the 16 patients with pretext - iv tumours , including the seven with lung metastases . 
of the nine patients who did not have metastatic disease at diagnosis , eight ( 89% ) had a complete resection and eight ( 89% ) achieved complete remission . 60 ( 97% ) patients had grade 34 haematological toxicity after at least one of the cycles . 
the highest frequency of neutropenia and thrombocytopenia was after additional preoperative chemotherapy ( cycle b ; 12 [ 92% ] and 11 [ 85% ] , respectively ) , which was given only to 13 patients . 
one patient died of fungal infection in profound neutropenia . of the 61 children who received at least two preoperative cycles , ototoxicity was evaluated and documented in 54 , with at least two measurements , both done after at least two cycles or during follow - up . 
in seven patients ( 10% ) ototoxicity was not su ciently documented . panel : research in context systematic review we searched pubmed on jan 20 , 2004 , for clinical trials published in english before jan 1 , 2004 , using the keywords hepatoblastoma , metastatic , or high risk , or locally advanced or unresectable hepatoblastoma and identi ed 11 articles that provided prospective survival data for at least one of these patient groups . 
four more relevant articles were identi ed , one of which showed improved resultscompared with the previous datain high - risk hepatoblastoma ( 3 year event - free survival 65% , overall survival 69% ; 56% and 62% for the metastatic subgroup )  . 
systematic search for publications on the use of ( high ) dose - dense or weekly cisplatin in childhood cancer retrieved no articles . interpretation our study used a novel and unique design of dose - dense ( weekly ) cisplatin in the treatment of patients with high - risk hepatoblastoma and provides rm evidence for the feasibility and e cacy of this approach . 
the reported outcome , in particular for those with metastatic disease , is higher than ever before achieved for children with high - risk hepatoblastoma and denotes an important improvement in the prognosis of these children . 
although further evaluation of the long - term toxicity is needed , the presented treatment strategy could be now regarded as rst choice in the treatment of patients with metastatic or very high - risk hepatoblastoma . 18 serious adverse events , including two deaths , were reported ( appendix )  . 
on the basis of the observed toxicity , the independent data monitoring committee did not recommend any changes or amendment to the protocol during the trial . discussion the siopel - 4 trial addressed the question of whether increased dose density of cisplatin in the preoperative phase can improve the prognosis of children with highrisk , in particular metastatic , hepatoblastoma ( panel )  . 
the proportion of patients with complete remission and the 3 - year eventfree and overall survival compare favourably with results of previous studies and suggest an improvement in the prognosis of children with high - risk hepatoblastoma . in view of the rarity of high - risk hepatoblastoma , a randomised controlled study to directly prove the superiority of the study treatment was not deemed feasible within an acceptable timeframe . 
instead , a single - arm study was designed with complete remission at the end of trial treatment as the primary endpoint , which is an objective and relevant outcome measure and allows analysis shortly after the study is closed . 
siopel - 4 aimed to achieve an improvement in proportion of patients with complete remission of 20% or more ( from 60% [ in siopel - 3hr ] to 80% ) , which is regarded as a clinically relevant and signi cant improvement . since tumour - free status at the end of treatment is a prerequisite for cure and the relapse rate in high - risk hepatoblastoma is low , complete remission is thought to be a good surrogate for overall and event - free survival . 
 additionally , to produce robust survival data that can be adequately compared with previously published results , patients were followed up for a median of 52 months ( table 3 )  . 
on the basis of these data the current follow - up seems largely su cient for a good estimate of the long - term e cacy of the regimen and gives a good basis for comparison with other studies . although we acknowledge that comparison with historical controls does not provide the highest level of evidence , we are convinced that in this context the use of historical controls is the best available option to indicate improvement . 
we believe that the high similarities in patient populations , inclusion and exclusion criteria , and trial design , conduct , and analysis make the comparison with previous siopel studies appropriate . 840 vol 14 august 2013 articles the most important progress has been achieved in the cure of children with metastases . 
the complete response in the lungs achieved in this way appears stable , since 19 ( 95% ) of the 20 patients remained in continuous complete remission , including the six who underwent liver transplantation . 
25 of the 39 patients had complete remission without pulmonary surgery and two additional patients had no viable tumour cells in their metastasectomy specimens , emphasising the e cacy of the applied chemotherapy . 
additionally , two of the six children who did not have complete remission because of pulmonary disease had low initial afp and scud histology , both features known as bad prognostic factors.26 , 27 the outcome of patients with metastatic disease achieved in this study appears to be better than the results of all previously published studies , including siopel3hr , and denotes a major improvement in the cure of these children ( table 3 )  . the excellent response of lung metastases to preoperative chemotherapy in this study is in line with the promising results of the previous siopel study ( 3hr ) , which seem to be further improved by the highly e ective siopel - 4 regimen . 
 surgery remains important in patients whose lung lesions are not cleared by chemotherapy alone . the presented results for patients with pretext - iv tumour con rm the fairly good prognosis of this subgroup and might suggest a slight improvement in overall survival compared with previous siopel studies ( table 3 )  . 
 because of an excellent response to chemotherapy , the tumour extent decreased signi cantly in most patients and partial hepatectomy became feasible in four children who otherwise would have needed liver transplantation . 
this study con rms that transplantation is a safe and potentially curative option for patients whose primary tumour remains unresectable with partial hepatectomy.2830 these results also emphasise that the presence of lung metastases at diagnosis is not a contraindication to liver transplantation , provided that e ective preoperative chemotherapy is given , the lung lesions respond to chemotherapy , and are completely cleared before transplantation by chemotherapy and metastasectomy ( if needed )  . we believe that the most important explanation for the improved results is the increased preoperative dose density of cisplatin used in this treatment regimen ( 475 mg / m per week vs 229 mg / m per week in siopel - 3hr ) , in the context of the previously established multidisciplinary approach . 
our results encourage exploration of the role of dose - dense cisplatin - based regimens in the treatment of other paediatric tumours . as expected , the main toxicity was haematological , leading to profound neutropenia in most children . 
however , because of the young age of most patients , follow - up audiology investigations will be needed to establish the incidence and severity of long - term ototoxicity after this regimen . in conclusion , the siopel - 4 treatment regimen with dose - dense administration of cisplatin and radical surgery is a feasible and e ective treatment and improves the prognosis of children with high - risk hepatoblastoma , in particular of those with metastatic disease . contributors jz , lb , pb , dr , rm , az , mch , j - bo , da , ms , pc , and gp were involved in the design and concept of the study and in writing of the protocol . 
all authors have participated in drafting and nalising the report and have approved the nal draft . con icts of interest we declare that we have no con icts of interest . acknowledgments this study was partly supported by cancer research uk and cancer research switzerland / oncosuisse grants to the siopel group . 
we assessed whether children and young people with clinical standard and intermediate - risk all who have persistent mrd at the end of induction therapy bene t from augmented post - remission therapy . methods between oct 1 , 2003 , and june 30 , 2011 , we enrolled eligible patients aged 124 years and initially categorised them into clinical standard - risk , intermediate - risk , and high - risk groups on the basis of a combination of national cancer institute criteria , cytogenetics , and early morphological response to induction therapy . 
clinical standard - risk and intermediate - risk patients with mrd of 001% or higher at day 29 of induction ( mrd high risk ) were randomly assigned ( 1 : 1 ) to standard therapy ( treatment regimens a and b ) or augmented post - remission therapy ( regimen c )  . 
 compared with standard therapy , the augmented treatment regimen ( regimen c ) included an additional eight doses of pegylated asparaginase , 18 doses of vincristine , and escalated - dose intravenous methotrexate without folinic acid rescue during interim maintenance courses . 
computer randomisation was used for treatment allocation and was balanced for sex , age ( < 10 years vs 10 years ) , and white blood cell count at diagnosis ( < 50 10 / l vs 50 10 / l ) by minimisation . 
this trial is registered with current controlled trials , number isrctn07355119 . findings 533 mrd high - risk patients were randomly assigned to receive standard ( n = 266 ) or augmented ( n = 267 ) post - remission therapy . 
after a median follow - up of 70 months ( iqr 5291 ) , 5 - year event - free survival was better in the augmented treatment group ( 896% [ 95% ci 859933 ] ) than in the standard group ( 828% [ 781875 ] ; odds ratio [ or ] 061 [ 95% ci 039098 ] , p = 004 )  . 
overall survival at 5 years was numerically , but not signi cantly , higher in the augmented treatment group ( 929% [ 95% ci 898960 ] ) than in the standard therapy group ( 889% [ 850928 ] ; or 067 [ 95% ci 038117 ] , p = 016 )  . 
more adverse events occurred in the augmented treatment group than in the standard group ( asparaginase - related hypersensitivity in 18 [ 67% ] in the augmented group vs two [ 08% ] in the standard group and asparaginase - related pancreatitis in eight [ 30% ] vs one [ 04% ] ; intravenous methotrexaterelated mucositis in 11 [ 41% ] vs three [ 11% ] and methotrexate - related stomatitis in 48 [ 180% ] vs 12 [ 45% ] )  . interpretation our ndings suggest that children and young people with acute lymphoblastic leukaemia and 001% or more mrd at the end of remission induction therapy could bene t from augmented post - remission therapy . 
 however , the asparaginase and intravenous methotrexate used in the augmented treatment regimen is associated with more adverse events than is the standard post - remission treatment regimen . funding medical research council and leukaemia and lymphoma research . introduction sub - microscopic amounts of leukaemia , or minimal residual disease ( mrd ) , can be detected and quanti ed with a range of techniques in patients receiving treatment for acute lymphoblastic leukaemia . 
several large studies have shown that assessment of mrd after remission provides the most sensitive and speci c in children with acute predictor of relapse risk leukaemia.13 patients who have lymphoblastic undetectable mrd by the end of remission induction therapy have a very low risk of relapse , whereas those with persistent mrd at that point are at a signi cantly higher risk . 
however , no published evidence from a randomised study exists to show that strati cation of treatment by mrd response improves outcomes . vol 15 july 2014 articles see online for appendix in the ukall 2003 randomised trial , we tested whether adjustment of treatment intensity according to mrd risk strati cation was feasible . 
acute lymphoblastic leukaemia was diagnosed with standard morphological and ow cytometric criteria as previously described.8 patients younger than 1 year of age or with mature b - cell acute lymphoblastic leukaemia were not eligible . 
patients with philadelphia chromosomepositive acute lymphoblastic leukaemia were also not eligible and were transferred to other protocols such as the european study for philadelphia - chromosomepositive all ( esphall ) 9 or ukall xii10 when their philadelphia chromosome status was known . the upper age limit of entry was 18 years at the start of the trial , but was increased to 20 years on feb 1 , 2006 , and to 24 years from aug 1 , 2007 , because retrospective studies showed that young people had an improved outcome when treated with paediatric protocols . 
we had to reduce the overall treatment intensity for patients with downs syndrome after june 1 , 2008 , because of excess treatment - related mortality in this patient group ; from that time , patients with downs syndrome were registered on the trial but did not undergo randomisation and were treated as clinical standard - risk patients , with adjustment of post - induction treatment according to their response to induction therapy . at diagnosis , patients were strati ed according to their risk of relapse on the basis of three metrics : the national cancer institute ( nci ) risk criteria ( nci standard risk : patients younger than 10 years with a white blood cell count < 50 10 per l ; nci high risk : patients aged 10 years or older and those with a white blood cell count 50 10 per l ) ; high - risk cytogenetics ( mll rearrangements , near haploidy low hypodiploidy [ 3039 chromosomes ] , t [ 17 ; 19 ] [ q23 ; p13 ] , or intrachromosomal ampli cation of chromosome 21 ) ; and early response to induction therapy as assessed by bone - marrow morphology on days 8 and 15 of treatment in patients younger than 16 years . 
 all patients aged 16 years or older were treated as clinical intermediate risk irrespective of day 8 or 15 bone marrow response and were eligible for mrd strati cation and randomisation . 
 patients who were not in complete remission at day 29 of induction were not eligible for mrd strati cation and randomisation . to be eligible we strati ed clinical standard - risk and intermediaterisk groups by bone marrow mrd at the end of induction ( day 29 from the start of treatment )  . 
the assay was done in four uk laboratories that participated in a european qualityassurance scheme.11 , 12 all mrd results were centrally reviewed by ng and jh . patients with undetectable mrd after induction ( day 29 ) and before interim maintenance were classi ed as mrd low risk , as were those who had detectable ( < 001% ) mrd at the end of induction but undetectable mrd before the start of interim maintenance . 
patients in whom mrd could not be measured because no or poor - quality samples were available and those with persistent disease that was less than 001% mrd before the start of interim maintenance were classi ed as mrd indeterminate . the protocol was approved by the scottish multicentre research ethics committee . 
the trial was monitored by an independent data monitoring committee , which reviewed safety and e cacy data annually . randomisation and masking we randomly assigned eligible mrd high - risk patients in a 1 : 1 ratio to receive standard post - remission treatment ( regimen a or b , depending on clinical risk ) or an augmented intensity schedule ( regimen c ; gure 1 )  . 
randomisation was balanced for sex , age ( < 10 years vs 10 years ) , and white blood cell count at diagnosis 810 vol 15 july 2014 articles ( < 50 10 / l vs 50 10 / l ) by method of minimisation . 
 patients , clinicans , and data analysts were not masked to treatment allocation . regimen c received an additional four doses of vincristine and two doses of pegylated asparaginase during the bfm consolidation course . procedures three escalating - intensity patients received one of treatment regimens depending on their clinical and mrd risk grouping . 
clinical standard - risk patients received regimen a , clinical intermediate - risk patients received regimen b , and clinical high - risk patients and those mrd high - risk patients who were randomly allocated to this treatment received the augmented therapyregimen c ( gure 1 ) ; appendix pp 24 provide the full regimen details and cumulative drug doses . initially , nci standard - risk patients received a threedrug induction of vincristine , steroids , and asparaginase for 4 weeks . 
all patients received two doses of intrathecal methotrexate during induction , and those who had blasts in their csf at diagnosis received an additional two doses on days 15 and 21 . after induction , mrd high - risk patients randomly assigned to standard treatment continued on regimen a ( if nci standard risk ) or b ( if nci high risk ) , whereas those randomly assigned to augmented treatment received regimen c ( gures 1 and 2 )  . 
patients assigned to for interim maintenance treatment , patients allocated to regimens a and b received the same treatment courses for 8 weeks : daily oral mercaptopurine and weekly methotrexate with monthly vincristine and steroid pulses . 
regimen c interim maintenance comprised increasing doses of intravenous methotrexate without folinic acid rescue , and vincristine and intensi cation pegylated treatment courses were the same in regimens a and b : one dose of pegylated asparaginase on day 4 ; vincristine , dexamethasone ( alternate weeks ) , and doxorubicin for 3 weeks ; and then 4 weeks of cyclophosphamide and cytarabine as during the bfm consolidation course . 
male patients received treatment for 3 years and female patients for 2 years from the start of interim maintenance the higher risk of relapse in boys . to account for all patients were given 6 mg / m oral dexamethasone daily during induction and maintenance courses , with a maximum dose of 10 mg . 
in delayed intensi cation courses , all patients received 10 mg / m clinical standard - risk patients ( regimen a ) induction cns - directed therapy + im1 continuing therapy 23 24 31 3839 clinical intermediate - risk patients ( regimen b ) bfm consolidation induction + cns - directed therapy 16 17 continuing therapy 9 10 17 18 24 25 3940 clinical high - risk and mrd high - risk patients randomly assigned to augmented therapy ( regimen c ) induction capizzi im1 capizzi continuing therapy bfm consolidation + cns - directed therapy female patients to week 112 male patients to week 164 female patients to week 112 male patients to week 164 female patients to week 117 male patients to week 169 13 14 21 22 29 30 45 46 time ( weeks ) figure 1 : outline of treatment regimens for clinical risk groups im = interim maintenance . 
mrd high - risk patients assigned to augmented therapy transferred to regimen c after induction . vol 15 july 2014 articles 3207 patients registered in the trial 81 excluded for ineligibility 3 had been registered twice 12 had been misdiagnosed * 59 philadelphia chromosome - positive 7 withdrew consent 3126 eligible for analysis 1732 clinical standard risk 989 clinical intermediate risk 405 clinical high risk ( not eligible for mrd stratication ) 2721 eligible for mrd stratication 819 indeterminate mrd status 808 high - risk mrd 1059 low - risk mrd 35 died within 35 days or never achieved remission 6 had m2 marrow ( 525% leukaemic blasts ) 2 had protocol violation 4 ser ( patients aged 16 years and entered before age amendment ) 124 refused 275 not randomly assigned 23 doctors choice 18 toxicity 8 other reason 79 unknown 3 withdrawn 7 had downs syndrome 1 cytogenetics ( high hyperdiploid ) 533 randomly assigned 266 assigned to standard therapy 267 assigned to augmented therapy figure 2 : trial pro le mrd = minimal residual disease . 
 * one patient had burkitts lymphoma , one t - cell lymphoma , one t - cell non - hodgkin lymphoma , one mature b - cell acute lymphoblastic leukaemia , two acute myeloid leukaemia , ve mixed - phenotype acute leukaemia , and one precursor b non - hodgkin lymphoma . 
no high - risk randomised patients were lost to follow - up within 1 year or excluded from analysis . daily dexamethasone ( without a cap ) for 2 weeks on alternate weeks . 
all patients received pegylated asparaginase ( oncaspar ; medac gmbh , wedel , germany [ now distributed by sigma - tau , gaithersburg , md , intramuscularly usa ] ) throughout treatment . 1000 units / m per dose patients with ve leucocytes per l or more and blasts in a diagnostic sample of csf with fewer than ten red blood cells per l received an extra two doses of intrathecal methotrexate in induction and 24 - gy cranial radiotherapy during consolidation until august , 2009 , after which point they received only the additional doses of intrathecal methotrexate during induction . 
patients with traumatic lumbar puncture and blasts in the csf , and those with fewer than ve blasts per l , also received an extra two doses of intrathecal methotrexate during induction . 
 * p value for heterogeneity , comparing those mrd high - risk patients who were randomised ( n = 533 ) vs those who were not ( n = 275 )  . 
 table 1 : baseline patient characteristics , in the trial overall , and in the mrd high - risk patients standard therapy ( n = 266 ) augmented therapy ( n = 267 ) statistics for augmented therapy group events actuarial percentage at 5 years ( 95% ci ) events actuarial percentage at 5 years ( 95% ci ) unadjusted odds ratio * ( 95% ci ) p value any relapse any bone marrow relapse any non - bone marrow relapse death during remission event - free survival overall survival 142% ( 97187 ) 105% ( 66144 ) 41% ( 1468 ) 35% ( 1357 ) 828% ( 781875 ) 889% ( 850928 ) 75% ( 42108 ) 055 ( 033094 ) 46% ( 1973 ) 31% ( 0953 ) 27% ( 0747 ) 042 ( 022081 ) 095 ( 038239 ) 076 ( 028202 ) 896% ( 859933 ) 061 ( 039098 ) 929% ( 898960 ) 067 ( 038117 ) 003 0009 091 059 004 016 mrd = minimal residual disease . 
the secondary outcomes were cumulative risk of relapse and treatment - related toxic e ects . details of all permitted dose reductions and interruptions during the trial are provided in the study protocol . 
the only criterion for removal of patients from the study was withdrawal of patient consent , which did not occur for any patients in this trial . for analysis of the e ect of augmented intervention on cytogenetic sub - groups , we classi ed patients with b - cell precursor acute lymphoblastic leukaemia into three cytogenetic risk groups according to the presence of ( ie , good chromosomal abnormalities : good risk prognosis ) : hyperdiploidy etv6 - runx1 , ( 5165 chromosomes ) , and high - risk cytogenetics ( as above ) ; poor risk ( loss of 13q or 17p ) ; or intermediate risk ( all others ) , as previously described.13 high outcomes the primary outcomes were event - free survival and overall survival . 
event - free survival was de ned as time from diagnosis to relapse , secondary tumour , or death , and overall survival was de ned as time to death . 
diagnosis of relapse or secondary tumour was not centrally reviewed but death was con rmed by central review of death augmented therapy standard therapy statistical analysis on the basis of the results of a retrospective mrd study in patients treated in a previous trial , all 97 / 99 , 14 we expected that 50% of patients would fall into the mrd high - risk category and carry a 30% risk of relapse at 5 years . 
therefore , at the start of the trial , the planned sample size for the mrd high - risk randomisation was 660 ( after allowance for 10% dropout ) with expected closure of recruitment in october , 2009 , which would give 84% power to detect an event - free survival di erence of 10% . 
however , non - randomised changes to treatment resulted in the mrd high - risk group being smaller ( around 30% of all patients ) and having a better outcome ( 20% actuarial risk of relapse at 5 years ) in ukall 2003 than expected . 
the revised power calculations estimated that 450 randomised patients , with an 80% event - free survival in the standard treatment group , would yield an 84% chance of detecting a 10% improvement in event - free survival to 90% in the intensi cation group ( 82% allowing for 10% dropout )  . 
we counted only rst events , censoring at competing eventseg , time to bone - marrow relapse included censoring at nonbone marrow relapse or death in remission for patients with these events as their rst . 
 they were included in analyses of event - free and overall survival but excluded from analyses of relapse or remission death . we calculated odds ratios [ ors ] and 95% cis as exp [ ( oe ) / v + / 196 / v ] , in which o is the observed events , e is the expected events , and v is the variance.15 plots of event - free survival by high - risk randomised allocation were done to show the relative e ect of treatment group within subgroups . 
within each subgroup , the observed minus expected ( oe ) number of events and its variance ( v ) are given.16 all analyses were by intention to treat and p values were two - sided . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results of 3207 patients registered in the trial ( gure 2 ) , 81 were excluded for ineligibility , including 59 ( 2% ) who were philadelphia chromosome positive : 52 ( 2% ) were transferred to esphall and seven ( 02% ) to ukall xii . 
on the basis of cytogenetics and early bone - marrow response , 1732 of 3126 ( 55% ) patients were reclassi ed as clinical standard risk , 989 ( 32% ) clinical intermediate risk , and 405 ( 13% ) clinical high risk . 
all trial patients , with the exception of those who died within 35 days or never achieved remission ( 35 / 3126 [ 1% ] ) , were tested for mrd status after induction and before rst interim maintenance , but clinical high - risk patients were not eligible for mrd strati cation and randomisation . 
of 2686 clinical standard or intermediate - risk patients tested for mrd status , 1059 ( 39% ) were low risk , 808 ( 30% ) high risk , and 819 ( 30% ) indeterminate risk . of 808 eligible mrd high - risk patients , 533 ( 66% ) underwent randomisation to standard or augmented therapy ( gure 2 )  . 
we recorded no di erence in the characteristics of eligible mrd high - risk patients who did or did not undergo randomisation , or between those randomly allocated to standard or augmented therapy ( table 1 )  . 
smaller numbers of patients were included in the overall adjusted analysis because the mrd level on day 29 was unknown in six patients and the cytogenetic risk group was unknown in 32 patients . 
2 1 = 1 degree of freedom in 2 test . vol 15 july 2014 articles and 70 months ( 5291 ) for patients who underwent the mrd high - risk randomisation . the outcome for patients in the trial overall and the results of the low - risk randomisation have been reported previously.7 after a further 2 years of follow - up , the 5 - year event - free survival , overall survival , and cumulative risk of relapse remain stable at 873% ( 95% ci 861885 ) , 916% ( 906926 ) , and 88% ( 7898 ) , respectively , for all patients who were eligible for analyses in the trial overall . 
we continue to record no di erence in event - free survival , overall survival , or relapse risk between standard or reduced treatment groups in the mrd low - risk randomisation ( appendix p 8 )  . recorded randomisation , we in the population of mrd high - risk patients who underwent improvement in event - free survival with augmented therapy compared with standard treatment ( or 061 [ 95% ci 039098 ] , p = 004 )  . 
5 - year event - free survival was 896% ( 95% ci 859933 ) in the augmented therapy group versus 828% ( 781875 ) in the standard group ( table 2 )  . 
this improvement was attributable to a decreased risk of any relapse in the augmented therapy group compared with the standard therapy group ( table 2 , gure 3 )  . 
this reduction in relapse risk was composed mainly of a decrease in the risk of relapse involving the bone marrow in the augmented treatment group compared with the standard group ( table 2 )  . 
 patients given augmented therapy also had a numerically , but not signi cantly , improved overall survival ( 5 - year event - free survival 929% [ 95% ci standard therapy group ( n = 266 ) augmented therapy group ( n = 267 ) p value for augmented vs standard therapy serious adverse events any serious adverse event infection encephalopathy asparaginase hypersensitivity pancreatitis avascular necrosis thrombosis neuropathy mucositis ctcae grade 3 or 4 adverse events any adverse event infection haemorrhage thrombosis mood stomatitis constipation vomiting 91 ( 34% ) 44 ( 17% ) 20 ( 8% ) 2 ( < 1% ) 1 ( < 1% ) 16 ( 6% ) 8 ( 3% ) 6 ( 2% ) 3 ( 1% ) 223 ( 84% ) 129 ( 49% ) 4 ( 2% ) 8 ( 3% ) 14 ( 5% ) 12 ( 5% ) 3 ( 1% ) 9 ( 3% ) ctcae = common terminology criteria for adverse events . table 3 : toxicity by treatment group 119 ( 45% ) 43 ( 16% ) 33 ( 12% ) 18 ( 7% ) 8 ( 3% ) 13 ( 5% ) 10 ( 4% ) 6 ( 2% ) 11 ( 4% ) 229 ( 86% ) 115 ( 43% ) 4 ( 2% ) 9 ( 3% ) 6 ( 2% ) 48 ( 18% ) 4 ( 2% ) 20 ( 8% ) 00003 002 091 006 004 057 081 100 005 055 022 100 100 007 100 005 < 00001 898960 ] the augmented group vs 889% [ 850928 ] in the standard group ; or 067 [ 95% ci 038117 ] , p = 016 )  . 
in the standard treatment group ( n = 266 ) , nine patients died in remission ( two gramnegative septicaemia , one sepsis , one pseudomonas septicaemia / necrotising fascitis , two pneumonia , one fungal infection , one disseminated herpes simplex virus , and one seizure )  . signi cantly more patients the augmented treatment group had at least one serious adverse event ( 119 / 267 [ 45% ] ) than did those in the standard treatment group ( 91 / 266 [ 34% ] ; p = 002 )  . 
speci cally , in the augmented treatment group there was an excess number of serious adverse events and grade 34 adverse events related to asparaginase ( hypersensitivity and pancreatitis ) and intravenous methotrexate ( mucositis and stomatitis ; table 3 )  . 
as expected , more patients needed dose reductions below 90% of protocolmandated doses during post - remission therapy with regimens b and c than with regimen a ( appendix p 5 )  . 
 only ve patients crossed over from regimen c to the standard regimen because of toxicity ( the reasons for which were : one prolonged neutropenia , one two capizzi methotrexate - related neurotoxicity , mucositis , and one other toxicity , for which no further information was provided )  . therapy because discussion in this randomised trial of children and young people with acute lymphoblastic leukaemia who had persistent mrd at the end of remission induction therapy , we showed that event - free survival with augmented postremission therapy was signi cantly better than that with standard risk was substantially reduced in the augmented treatment group . 
 although many recent and ongoing studies have adopted a strategy of intensifying treatment for patients de ned as high risk by mrd strati cation , our study is the rst to show that such a strategy is , in fact , bene cial ( panel )  . 
the need for the trial and the questions to be answered were established by a combination of non - systematic literature review , discussions in the national childhood and adult leukaemia clinical study groups and clinician networks , and consultation with experts from the us childrens oncology group and european childhood leukaemia study groups . 
 during planning , the evidence base indicated that on - treatment monitoring and detection of sub - microscopic levels of leukaemia ( minimal residual disease [ mrd ] ) was the best predictor of relapse risk in children with acute lymphoblastic leukaemia , but whether treatment intensi cation would bene t mrd de ned high - risk patients was not known . 
we aimed to establish whether treatment for childhood acute lymphoblastic leukaemia could be strati ed by risk of relapse predicted by mrd response . interpretation we have reported that augmented post - remission treatment bene ts children and young adults with clinical standard - risk and intermediate - risk acute lymphoblastic leukaemia and mrd of 001% or higher at the end of induction treatment . 
in addition to the results of the mrd low - risk randomisation reported previously , this trial has shown that mrd response provides the best possible strategy for the selection of patients who will bene t from treatment escalation or de - escalation of post - remission therapy . for been demonstrated translation of while retaining the overall e cacy of treatment , as has already philadelphia chromosome - positive acute lymphoblastic leukaemia.9 additionally , understanding of the molecular biology of acute lymphoblastic leukaemia and its e ect on phenotype and clinical outcome22 , 23 will help to re ne risk strati cation and reveal new drug targets that might be of particular bene t to patients with disease refractory to existing drugs . recent advances in combination with the results of the mrd low - risk randomisation reported previously , ukall 2003 has shown that mrd strati cation provides the best available approach to risk - directed therapy . contributors av , ng , and cm designed the trial . 
av , ng , cm , rh , and cr gathered and analysed data , helped to address queries from local investigators , dealt with treatment di culties , and contributed to the writing of the report . 
rw gathered and analysed data and contributed to the writing of the report . declaration of interests we declare no competing interests . acknowledgments this trial was supported by grants from leukaemia and lymphoma research ( uk ) and the medical research council ( uk )  . 
we thank the patients and their families who participated in these trials and the study pharmacists , nurses , and clinicians who supported them ; all the laboratory sta for providing timely and accurate mrd results for patients ; and member laboratories of the uk cancer cytogenetic group for providing cytogenetic data . 
special thanks go to sue richards for her support of this trial , and of past uk paediatric acute lymphoblastic leukaemia trials in the past 30 years , until her retirement in 2012 . the augmented therapy we tested has previously been shown to reduce the risk of relapse for slow morphological early responders in a us childhood cancer group study.17 hence , slow early responders received nonrandomised augmented therapy as did those patients with high - risk cytogenetics . 
the proportion of nci highrisk patients and those with t - cell immunophenotypes are therefore under - represented in the randomised cohort because these subgroups are more likely to have a slow early response than are nci standard risk and b - cell lineage patients.18 regardless , the e ect of augmented therapy on relapse risk was recorded in all subgroups analysed ( data not shown )  . we classi ed patients as mrd high risk if they had an mrd level of 001% or higher at day 29 of induction . 
 this identi ed quite a large group ( 4060% of the cohort , depending on age and white cell count ) with an intermediate prognosis compared with a smaller highrisk group ( < 10% ) with a much higher risk of relapse identi ed by other study groups ( mrd > 1% at day 42 in the st jude study5 or > 005% at week 12 in the aieopbfm study12 )  . 
whether or not our augmentation strategy would bene t this very - high - risk group is unknown because we did not monitor mrd at later timepoints in our mrd high - risk cohort . 
therefore , in our current trial , ukall 2011 , patients who have persistent high - level mrd ( > 05% ) after augmented consolidation therapy are candidates for treatment with novel agents followed by a rst remission allogeneic transplant . compared with standard therapy , the augmented regimen included an additional eight doses of pegylated asparaginase , 18 doses of vincristine , and escalated - dose intravenous methotrexate without folinic acid rescue instead of oral methotrexate during interim maintenance courses . 
therefore , not unexpectedly , augmented therapy was signi cantly more likely to cause toxic e ects related to asparaginase ( hypersensitivity and pancreatitis ) and intravenous methotrexate ( stomatitis and mucositis )  . 
the excess toxicity was not associated with a higher treatment - related mortality or a signi cant e ect on quality of life ( data not shown ) and , with the exception of pancreatitis , resolved fully without late sequelae . to reduce the toxicity of augmented therapy , and based on the results of a us childhood cancer group study of nci high - risk patients19 that showed no bene t from a second delayed intensi cation course , mrd delayed receive high - risk intensi cation course in our ongoing trial , ukall 2011 . 
 in the future , new drugs20 , 21 designed to target leukaemiaspeci c receptors and proteins could replace elements of conventional chemotherapy regimens responsible for some of the major toxicities , thereby reducing toxicity patients only one vol 15 july 2014 articles correction to lancet oncol 2020 ; 21 : 76375 correction to lancet oncol 2021 ; 22 : 198211 paz - ares l , ciuleanu t - e , cobo m , et al . 
 first - line nivolumab plus ipilimumab combined with two cycles of chemotherapy in patients with non - smallcell lung cancer ( checkmate 9la ) : an international , randomised , open - label , phase 3 trial . 
lancet oncol 2021 ; 22 : 198211in figure 4c of this article , the number at risk at 15 months in the nivolumab plus ipilimumab with chemotherapy group should have been 107 . 
abemaciclib plus trastuzumab with or without fulvestrant versus trastuzumab plus standard - of - care chemotherapy in women with hormone receptor - positive , her2 - positive advanced breast cancer ( monarcher ) : a randomised , open - label , phase 2 trial . 
the text in the results section ( page 769 ) should have read as follows : eight patients in group a , 12 patients in group b , and six patients in group c discontinued at least one study treatment owing to adverse events ( figure 1 )  . 
five patients in group b and four patients in group c discontinued all treatments in the study regimen owing to adverse events and one patient in group a discontinued all treatments in the triplet combination . 
two of the 12 patients in group b discontinued at least one study treatment owing to cardiac failure , two additional patients in group b discontinued study treatment owing to decreased neutrophil count , and another two patients discontinued study treatment due to neutropenia . 
at a median follow - up of 5 years , ndings from our previously published randomised trial of narrow ( 1 cm ) versus wide ( 3 cm ) excision margins in patients with thick cutaneous melanomas showed that narrow margins were associated with an increased frequency of locoregional relapse , but no signi cant di erence in overall survival was apparent . 
we now report a long - term survival analysis of that trial . methods we did a randomised , open - label multicentre trial in 59 hospitals57 in the uk , one in poland , and one in south africa . 
patients with one primary localised cutaneous melanoma greater than 2 mm in breslow thickness on the trunk or limbs ( excluding palms or soles ) were randomly assigned ( 1 : 1 ) centrally to receive surgery with either a 1 cm or 3 cm excision margin following an initial surgery . 
this trial was not registered because it predated mandatory trial registration . findings between dec 16 , 1992 , and may 22 , 2001 , we randomly assigned 900 patients to surgery with either a 1 cm excision margin ( n = 453 ) or a 3 cm excision margin ( n = 447 )  . 
194 deaths were attributed to melanoma in the 1 cm group compared with 165 in the 3 cm group ( unadjusted hazard ratio [ hr ] 124 [ 95% ci 101153 ] ; p = 0041 )  . 
although a higher number of deaths overall occurred in the 1 cm group compared with the 3 cm group ( 253 vs 241 ) , the di erence was not signi cant ( unadjusted hr 114 [ 95% ci 096136 ] ; p = 014 )  . 
 surgical complications were reported in 35 ( 8% ) patients in the 1 cm excision margin group and 65 ( 15% ) patients in the 3 cm group . interpretation our ndings suggest that a 1 cm excision margin is inadequate for cutaneous melanoma with breslow thickness greater than 2 mm on the trunk and limbs . 
open access article distributed under the terms of cc by . introduction the risk of metastatic spread from a malignant melanoma is estimated on the basis of histopathological features such as the breslow thickness , mitotic rate , and the presence of microscopic ulceration.1 , 2 whether the surgical margins that are taken around the primary tumour a ect metastatic spread is unclear , despite having been the subject of several randomised clinical trials.37 historically , wide surgical margins of 5 cm or more were taken around primary melanomas in an attempt to not only excise the primary tumour but also to encompass local micrometastatic disease in the vicinity of the tumour.8 , 9 in ndings from all previously reported randomised trials comparing wide ( 35 cm ) with narrow ( 12 cm ) margins , no signi cant di erence in overall survival between the groups has been reported . 
 for melanoma - speci c survival , although no trial has shown a signi cant di erential risk associated with di erent surgical margin widths , ndings from two trials3 , 4 and the previous report of this trial10 suggest a possible detrimental e ect of narrow margins on melanoma - speci c survival . 
in a swedish melanoma 184 vol 17 february 2016 articles research in context evidence before this study we searched pubmed for articles published up to aug 1 , 2015 , on randomised trials assessing surgical excision margins in cutaneous melanoma , using the search terms melanoma , margins , excision , and surgery . 
 however , some of these studies have shown non - signi cant results favouring wider margins in minimising locoregional and distant relapse . added value of this study this study reports on long - term survival analysis and , to our knowledge , is the rst to show that wider surgical margins result in a signi cant improvement in melanoma - speci c survival . implications of all the available evidence this study , alongside the other randomised trials , reiterates current international guidelines stating that a 1 cm margin is inadequate for the treatment of a melanoma greater than 2 mm in breslow thickness . 
it lends support to further investigation of the adequacy of a 1 cm margin for melanomas between 1 mm and 2 mm in thickness , especially those with other poor prognostic features , for which most international guidelines at present still advise a 1 cm excision . 
 900 patients enrolled 742 received 1 mm margin initial excision * and randomised 158 received 1 cm margin initial excision and randomised 372 assigned to 1 cm margin 370 assigned to 3 cm margin 81 assigned to 1 cm margin ( ie , no further excision ) 77 assigned to 3 cm margin ( ie , 2 cm further excision ) 453 assigned to 1 cm margin 442 received assigned treatment 447 assigned to 3 cm margin 436 received assigned treatment 2 lost to follow - up 253 died 453 included in long - term intention - to - treat analysis 2 lost to follow - up 241 died 447 included in long - term intention - to - treat analysis figure 1 : trial pro le * initial excision by the proposed pathway . 
initial excision by the alternative pathway . study group trial3 of patients randomly assigned to excision margins of either 2 cm or 5 cm for trunk and extremity melanomas with a breslow thickness 0820 mm ( median 12 mm ) , the hazard ratio ( hr ) for melanoma deaths for narrow margins compared with wide margins was 122 ( 95% ci 088169 ; p = 024 ) with a median follow - up of 11 years . 
additionally , the intergroup melanoma surgical trial4 of patients randomly assigned to either a 2 cm or 4 cm excision margin for trunk and extremity melanomas with breslow thickness 14 mm ( median 196 mm ) showed a non - signi cant di erence ( p = 007 ) in 10 - year diseasespeci c survival between groups ( 70% for the 2 cm group and 77% for the 4 cm group )  . 
however , ndings from a second swedish melanoma study group trial6 that randomly assigned patients with melanomas of breslow thickness greater than 2 mm ( median 31 mm ) to either a 2 cm or a 4 cm excision margin showed no di erence in melanoma - speci c survival between the two groups ( hr 099 [ 95% ci 078126 ] ; p = 095 )  . ( breslow in 2004 , we reported the ndings from our randomised clinical trial10 of patients with high - risk malignant melanoma thickness 2 mm ) randomly assigned to excision margins of either 1 cm or 3 cm , with a median follow - up of 5 years . 
we now report an extended follow - up of the survival endpoints of this trial with a median follow - up of 88 years . methods study design and participants we have previously described the study design , patient eligibility criteria , trial protocol , and endpoints of the randomised trial in detail.10 brie y , between dec 16 , 1992 , and may 22 , 2001 , we did a randomised , open - label multicentre trial in 59 centres in the uk , south africa , and poland . 
the trial was done under the auspices of the uk melanoma study group , the british association of plastic surgeons , and the scottish cancer therapy network and was approved by local ethics committees of all participating centres . 
patients aged the 18 years or older with one primary localised cutaneous melanoma greater than 2 mm in breslow thickness arising on the trunk or limbs ( but not including the soles of feet or palms of hands ) were eligible for the study . 
before randomisation , the primary melanoma was excised in an initial surgery with either a 1 mm ( proposed pathway ) or 1 cm ( alternative pathway ) margin of excision . 
 table 1 : baseline characteristics of the intention - to - treat population randomisation and masking we randomly assigned patients ( 1 : 1 ) to either a 1 cm surgical excision or a 3 cm surgical excision as the measured clinical margin taken around the primary melanoma lesion . 
we did the randomisation centrally by telephone call from the patients treating centre to the institute of cancer research clinical trials and statistics unit ( icr - ctsu )  . 
elective lymph node dissection and sentinel node biopsy were not part of routine practice at the time the trial was undertaken and adjuvant chemotherapy was not allowed in the trial protocol . 
after treatment , patients were followed up for local and distant relapse and death every 3 months for the rst 2 years , then every 6 months for up to 5 years , and annually thereafter . 
 to maximise the amount of survival data obtained , we also traced uk patients ( n = 790 ) for their vital status and in january , 2012 , we requested the death certi cates of patients known to have died to identify the cause of death as stated on the certi cate . 
death was classed as melanoma - speci c if the cause of death was reported as melanoma on the clinical trial case - report form for 186 vol 17 february 2016 articles death , or if any evidence was present of distant metastatic melanoma at the time of death ( as reported in patient les or on death certi cates )  . 
attribution of the cause of death as stated on the death certi cate was masked to clinical records and treatment group . outcomes the primary endpoints of the original trial10 were locoregional recurrence and disease - free survival . 
instead , we assessed the original secondary endpoints of overall survival , measured as time from randomisation to death from any cause , and melanoma - speci c survival , measured as time from randomisation to death reported to be from melanoma . 
for the competing risks analysis , we plotted cumulative incidence functions for each cause of death ( melanoma and non - melanoma ) and compared treatment groups with grays test . 
hrs were obtained from the univariate fine and gray model.13 , 14 we also did a multivariable analysis with the fine and gray model , including the same variables as the multivariable cox model . 
to explore the e ect of age on cause of death , patients were classi ed at randomisation in ve age groups containing about equal numbers of patients ( < 45 years , 4553 years , 5463 years , 6470 years , and 71 years ) , de ned using quintiles and rounding to the nearest whole number . 
we estimated the rates of death from melanoma and other causes for each age group as 1 cm margin 3 cm margin hr 114 ( 95% ci 096136 ) ; log - rank p = 014 statistical analysis the original planned sample size was 600 patients , based on an expected 3 - year local or in - transit recurrence rate of 15% ; however , because of a lower recurrence rate than expected , the sample size was increased to 900 after discussion with the trial management group and the data monitoring committee.10 at the time of writing the protocol , we expected that 4050% of patients with a 3 cm excision would have disease recurrence within 23 years . 
 for melanoma - speci c survival , patients who died of non - melanoma causes were censored at the time of death and patients who died from an unknown cause were censored on the day before their date of death . 
to assess the robustness of these assumptions we did a competingrisks analysis , treating con rmed non - melanoma deaths as the competing event . we constructed kaplan - meier curves11 and calculated hrs using the cox proportional hazards model ; 12 we compared treatment groups using the log - rank test . 
 we calculated absolute risk di erence at 10 years with normal estimated 95% cis and assessed the e ect of individual prognostic factors in a multivariable analysis using the same cox proportional hazards model as in our previous report , 10 adjusting for age . 
variables are included in the model as categorical indicators , other than tumour thickness which was classi ed as 0249 mm , 250349 mm , 350449 mm , 450549 mm , and 550 mm or more , and tted as a linear e ect . 
for this analysis we constructed kaplan - meier curves and calculated hrs using the cox proportional hazards model for uk patients only . we did a post - hoc subgroup analysis to assess whether sex , tumour thickness , age group , site , ulceration , and proposed versus alternative pathway initial excision were associated with treatment e ect . 
we used two - sided signi cance tests throughout . this was the rst and only analysis that had been done on this dataset since the initial report of this trial . 
we did the competing risks analysis with r 3.0.2 and all other analyses with stata version 11.2. role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or n ( % ) overall survival melanoma - speci c survival 388 ( 50% ) 100 * 385 ( 50% ) 119 ( 099145 ) 128 ( 102161 ) 354 ( 46% ) 100 * 419 ( 54% ) 138 ( 111171 ) 138 ( 107177 ) tumour thickness ( mm ) 773 ( 100% ) 118 ( 110127 ) 477 ( 62% ) 100 * 296 ( 38% ) 168 ( 138204 ) 174 ( 139219 ) excision margin 3 cm 1 cm p value female male p value p value ulceration absent present p value site distal limb proximal limb age ( years ) trunk p value p value 0070 00035 < 00001 < 00001 0029 00001 244 ( 32% ) 100 * 174 ( 23% ) 123 ( 093163 ) 355 ( 46% ) 141 ( 109181 ) 100 * 0031 100 * 0013 123 ( 113133 ) < 00001 100 * < 00001 100 * 146 ( 104205 ) 171 ( 126231 ) 00026 100 * 034 400 ( 52% ) 100 * 373 ( 48% ) 149 ( 123181 ) 112 ( 089139 ) data are n ( % ) , hazard ratio ( 95% ci ) of 773 patients with available data . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between dec 16 , 1992 , and may 22 , 2001 , 900 patients were enrolled at 57 hospitals in the uk , one hospital in poland , and one hospital in south africa ( appendix ) and received an initial excision of 1 mm or 1 cm , and were then randomly allocated to either a total 1 cm surgical margin ( n = 453 ) or a total 3 cm surgical margin ( n = 447 ; gure 1 )  . 
 median follow - up for all patients was 57 years ( 68 months [ iqr 35103 ] ) and median follow - up in patients not known to have died ( censoring at death ) was 88 years ( 106 months [ 76135 ] )  . 
median follow - up for the uk patients for whom a death certi cate analysis was done ( censoring at death ) was 93 years ( 111 months [ iqr 82141 ] ) and median follow - up in non - uk patients was 63 years ( 76 months [ 62100 ] )  . 
 for three participants ( two in the 1 cm margin group , one in the 3 cm group ) , melanoma was present at the time of death but this was not the cause of death . 
four patients did not have any follow - up after randomisation and were censored at randomisation . the snapshot used for the current analysis was taken on aug 31 , 2012 , after information from the death certi cate analysis had been obtained . 
253 deaths occurred overall in 453 patients in the 1 cm margin group and 241 occurred in 447 patients in the 3 cm group ( unadjusted hr 114 [ 95% ci 096136 ] ; p = 014 ; gure 2 )  . 
194 deaths attributed to melanoma occurred in the 1 cm margin group compared with 165 in the 3 cm margin group ( unadjusted hr 124 [ 95% ci 101153 ] ; p = 0041 ; gure 2 )  . 
results from the sensitivity analysis of uk patients only ( n = 338 in the 1 cm margin group ; n = 392 in the 3 cm margin group ) showed hrs of 111 ( 95% ci 092133 ) for overall survival and 121 ( 097150 ) for melanoma - speci c survival ; the results were consistent with the primary result . 773 patients ( 385 in the 1 cm group and 388 in the 3 cm group ) had complete data for all known prognostic factors and were included in a multivariable analysis ( table 2 )  . 
when we assessed interactions between margin width and sex , 188 vol 17 february 2016 articles tumour thickness , age group , site , and ulceration in a subgroup analysis , none were signi cant for either overall survival or melanoma - speci c survival ( gure 3 )  . 
 when the e ect of competing deaths due to other causes was taken in account , the cumulative incidence of death from melanoma was higher in the 1 cm margin events ( n ) patients ( n ) hazard ratio ( 99% ci * ) 114 ( 096136 ) all patients male female < 60 years 60 years 000399 mm 400599 mm 6 mm site distal limb proximal limb trunk ulceration present absent protocol type alternative proposed all patients male female < 60 years 60 years 000399 mm 400599 mm 6 mm site distal limb proximal limb trunk ulceration present absent protocol type alternative proposed 126 ( 093172 ) 094 ( 065136 ) 135 ( 094193 ) 101 ( 074138 ) 107 ( 079146 ) 111 ( 069177 ) 181 ( 099334 ) 082 ( 051130 ) 126 ( 076208 ) 129 ( 093179 ) 135 ( 094194 ) 095 ( 067135 ) 075 ( 045126 ) 126 ( 093172 ) 137 ( 096196 ) 100 ( 064155 ) 141 ( 096207 ) 108 ( 073159 ) 124 ( 086180 ) 116 ( 068198 ) 167 ( 084332 ) 099 ( 054180 ) 147 ( 081267 ) 130 ( 090188 ) 134 ( 089202 ) 106 ( 070160 ) 078 ( 044141 ) 137 ( 096196 ) favours 1 cm favours 3 cm events ( n ) patients ( n ) hazard ratio ( 99% ci * ) 124 ( 101153 ) favours 1 cm favours 3 cm figure 3 : univariable subgroup analyses of overall survival ( a ) and melanoma - speci c survival ( b ) the dotted line shows the hazard ratio for all patients . 
the multivariable analysis done with fine and grays model for melanomaspeci c deaths showed similar results to the cox model for melanoma - speci c survival ( appendix )  . 
no di erences between the two margin widths were noted regarding the cumulative incidence of death due to other causes ( gure 4 ; point estimates of cumulative incidence at 88 years were 145% [ 95% ci 101206 ] in the 1 cm margin group , 182% [ 136240 ] in the 3 cm group )  . 
 the number of non - melanoma deaths in younger age groups was negligible , but became more predominant in later years of follow - up for older patients ( table 3 )  . 
surgical complications were reported in 35 ( 8% ) of 453 patients in the 1 cm group and 65 ( 15% ) of 447 patients in the 3 cm group . 
the most common complications were partial or complete graft loss ( ten [ 2% ] in the 1 cm group , 20 [ 4% ] in the 3 cm group ) and wound dehiscence ( seven [ 2% ] in the 1 cm group , nine [ 2% ] in the 3 cm group )  . discussion at a median follow - up of 88 years ( 106 months ) the risk of death from melanoma was signi cantly higher in the narrow ( 1 cm ) margin group than in the wider ( 3 cm ) margin group . 
 the estimated risk of death from any cause was higher in the 1 cm margin group than in the 3 cm margin group , although this di erence was not signi cant . 
 a limitation of our study is that complete data were not available for all patients ; in particular , death certi cates were not obtained for non - uk patients . 
however , the results of a sensitivity analysis of uk patients only were consistent with the primary results . findings from our previous report of this trial10 with a median follow - up of 5 years showed that , in patients with high - risk melanoma , a 1 cm excision margin was associated with a signi cant increase in locoregional relapse compared with a 3 cm excision margin that report , although the number of deaths di ered between the two study groups , the di erence was not signi cant ( 128 deaths from melanoma in the group with 1 cm excision margins compared with 105 in the group with 3 cm excision margins ; hr 124 [ 95% ci 096161 ] , p = 01 )  . 
additionally , no di erences were noted in overall survival between the two groups ( 322% in the 1 cm group vs 309% in the 3 cm group ; hr 107 [ 95% ci 075136 ] , p = 06 )  . the current analysis does not include an updated analysis of the locoregional recurrence endpoint because follow - up data for locoregional relapse beyond 5 years are sparse . 
this report describes analyses only of melanomaspeci c survival and overall survival , and shows that a narrow margin signi cantly reduced melanoma - speci c survival compared with a wider marg locoregional relapse is the most common rst site of relapse of metastatic melanoma and , accordingly , an increased risk of locoregional relapse in the narrow margin group might suggest an increased future risk of melanoma - speci c death . 
during the period of this study , when no e ective systemic therapies for metastatic melanoma were available , stage iv disease was associated with a very poor prognosis with a median survival of between 8 and 18 months depending on the pattern of metastatic spread.15 although age , sex , tumour thickness , ulceration , and tumour site all seem to be prognostic factors for overall survival , only age was shown to a ect non - melanoma deaths , which occurred in similar numbers in the 1 cm and the 3 cm groups . 190 vol 17 february 2016 articles the prognostic because sentinel node biopsy was not done routinely in this trial , 10 the trial groups might have been imbalanced in terms of clinically occult disease within regional lymph nodes at the time of randomisation , which could have biased the outcome of the trial . 
any imbalances in unobserved factors in this study would be due to chance and a chance imbalance in a study of this size is unlikely to a ect the outcomes . 
 because the trial groups were well balanced in terms of other known prognostic factors for outcome at the time of trial recruitment ( eg , sex , tumour thickness , disease site ) and ulceration was slightly more prevalent in the 3 cm group , the sentinel node status is unlikely to be worse in the 1 cm group than in the 3 cm group , although a chance imbalance remains possible . this study cannot establish whether locoregional relapse predisposes patients to the subsequent development of distant metastatic disease , or whether the development of locoregional disease is merely correlated with and predates the development of metastatic disease . 
 because a 3 cm margin resulted in a decreased number of melanoma deaths , this would suggest that surgically intervening in a micrometastatic process in the 3 cm around the primary tumour can somehow a ect the later metastatic process at more distant sites . 
previous studies have shown a signi cant increase in local recurrence rates after 1 cm excisions , 6 , 16 suggesting that 1 cm margins might not be adequate to deal with local microsatellitosis . previous randomised studies of elective1721 or selective22 lymph node dissection have not shown a signi cant di erence in melanoma - speci c survival . 
the absence of a proven survival bene t in these nodal studies is at odds with the probable biological hypothesis for an e ect on survival shown in this studyie , that removal of microsatellites around the primary tumour a ects the development of metastatic disease . 
however , because subgroup analyses in these studies raised the possibility of survival bene t for prophylactic lymph node clearance that was not detected at the point of randomisation , 22 there might be a consistent biological process underlying the e ect noted in this study and in previous studies of prophylactic lymph node clearance . current international guidelines advise a 2 cm excision for melanomas greater than 2 mm in thickness and ndings from the other major randomised study for thick melanomas6 suggested that a 4 cm excision was not better than a 2 cm excision in terms of melanoma - speci c survival . 
deaths presented as n or n ( % )  . table 3 : deaths from melanoma and other causes in di erent age groups of melanomas thicker than 2 mm , margins greater than 2 cm need not necessarily be taken . 
our study has re - emphasised that the choice of surgical margins taken around a cutaneous melanoma is important and , to our knowledge , for the rst time provides evidence to suggest that a narrower excision margin used for thick primary tumours a ects melanoma - speci c survival . 
this nding might be pertinent for speci c melanomas for which narrow ( 1 cm ) margins are presently advisedie , melanomas between 1 mm and 2 mm in thickness with other adverse prognostic features ( ulceration or high mitotic rate , or both )  . 
the possible di erence between a 1 cm and 2 cm margin for melanomas greater than 1 mm in thickness is being investigated in a randomised trial in progress ( nct02385214 )  . 
all authors were involved in the writing , review , and approval of the nal manuscript , and all agreed to the submission of the nal version of the manuscript . veronesi u , cascinelli n , adamus j , et al . 
lancet 1907 ; 169 : 9961003 . declaration of interests jmt is a trustee of the meirion thomas cancer research fund that funded the administrative fee needed to retrieve copies of death certi cates for patients within the trial . 
all other authors declare no competing interests . acknowledgments this study was funded by the north thames national health service executive , northern and yorkshire national health service executive , british united provident association foundation , british association of plastic surgeons , and the meirion thomas cancer research fund . 
 continued data collection and analysis was made possible by programme grant funding to the institute of cancer research ( icr ) clinical trials and statistics unit from cancer research uk ( c1491 / a15955 )  . 
we acknowledge the national institute for health and research biomedical research centre funding to the royal marsden nhs foundation trust and icr , the contributions of all patients who agreed to join the trial , the e orts of all the contributors and institutions as cited in the initial report of this trial , and roger ahern for his statistical input . correction to lancet oncol 2017 ; 18 : e35463 correction to lancet oncol 2018 ; 19 : 87100 correction to lancet oncol 2018 ; 19 : 25766 oconnor oa , lue jk , sawas a , et al . 
 for lancet oncol 2017 ; 18 : e35463 in this review , the second sentence of the abstract should read additional improvements have been reported in three phase 3 colon cancer trials when oxaliplatin was added to fluoropyrimidines , the effect was mainly on disease - free survival . 
this correction has been made to the online version as of feb 28 , 2018 although women fulvestrant johnston s , lee ks , et di leo a , al . 
buparlisib plus with postmenopausal her2hormone - receptor - positive , negative , advanced breast cancer progressing on or after mtor inhibition ( belle - 3 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
in the results section , the following sentence should have read in the 11 ( 13% ) cases of discordance , a pik3ca wild - type tumour sample and pik3ca - mutated ctdna were reported in three ( 4% ) patients and pik3ca mutations detected in the tumour sample but not in ctdna ( 9% ) patients . 
these corrections have been made to the online version as of feb 28 , 2018 . seven vol 19 march 2018 e137 corrections editorial for the cancer research uk commission on the health of nhs cancer services see default / les / measuring_up_ health_of_nhs_cancer_services_ sept2014.pdf emotion - based medicine or evidence - based medicine ? the uk national institute for health and care excellence ( nice ) is once again under the microscope because of recent recommendations for various cancer drugs . 
nab - paclitaxel for metastatic pancreatic cancer ( sept 8 , 2014 ) ; trastuzumab emtansine for her2positive breast cancer ( aug 7 , 2014 ) ; and abiraterone for metastatic , hormone - resistant prostate cancer ( aug 14 , 2014 ) have all been rejected on the grounds of insu cient cost - e ectiveness . 
unfortunately , a report commissioned by cancer research uk ( cruk ) published on sept 8 , 2014 , concluded that cancer care by the national health service ( nhs ) in england is at breaking point . 
further reports on sept 16 , 2014 , stated more than half of all hospitals are in de cit and the nhs will end the year with almost 1 billion of debt , adding yet more emotion to the debate surrounding nice decisions . predictably , in response to the criticism of nice , the uks health secretary , jeremy hunt , has engaged in gesture politics . 
on aug 27 , 2014 , hunt ordered a review of the system by which nice approves cancer drugs , and announced an increase in the cancer drugs fund from 200 million to 280 million . 
cancer charities and patient groups have responded positively , but warn that this is a temporary x to a systemic problem in need of major reform to enable long - term sustainability . 
 furthermore , while nice decisions are undermined by the cancer drugs fund in england , their decisions are undone elsewhere in the uk too ; for example , the welsh medicines strategy group has approved nab - paclitaxel for use in wales , creating more fragmentation and further disparities in the level of care available across the uk , the very thing nice was created to eradicate . but , is nice really broken ? and are current circumstances really creating a second - rate cancer service in nhs england , as suggested by the manipulative and emotive language of the mainstream media ? there are no easy answers to these questions . 
on july 22 , 2014 , the institute approved two expensive cancer drugs : ipilimumab for rst - line treatment of advanced malignant melanoma and enzalutamide for progressive prostate cancer . 
 furthermore , the cruk commission shows that , in spite of a 50% increase in the number of cancer referrals from general practitioners in the past 4 years , the health service has managed this substantial increase in cases remarkably wellsurvival is at record highs , and nine out of ten patients say the care they receive is excellent or very good . 
in june , 2014 , a report by the us - based commonwealth fund comparing us health care with that in ten other countries concluded that the uk ranked rst for quality , access , and e ciency of care , and second for health - care equity . 
the uk is also not the only country to restrict access to new medicines on the basis of costeven in the usa increasing numbers of payers are excluding drugs from their formularies for similar reasons ( but without equitable cost - e ectiveness criteria )  . current criticisms of nice and nhs england need to be kept in perspective . 
while it is fair to question whether the qalys used by the institute to determine coste ectiveness are aligned with present - day expectations , it is equally important to recognise the regulator is not fully responsible for the current situation , that nices recommendations are informed by costs and data outside of its control , and that health - care equity can only be achieved by use of consistent algorithms . 
 equally , although the recommendations made by the cruk commission to ensure future sustainability of nhs cancer services are very reasonable given recent reforms , the drive to deliver greater e ciencies in the nhs are also rational . 
 similar counterpoints can be made for all other vested interests in this debate too , but , ultimately rather than point - scoring and in ghting , all parties should work together to deliver the best possible care within the constraints of a world that will , unfortunately , never o er a utopian solution . 
 the lancet oncology vol 15 october 2014 1177 corrections correction to lancet oncol 2011 ; 12 : 1051 correction to lancet oncol 2015 ; 16 : 634 , 637 histological sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
 independent lancet oncol 2011 ; 12 : 104552 in the discussion of this article , the second sentence of the fth paragraph should read the proportion of patients a ected by grade 34 fatigue in this study ( 7% ) is similar to that reported for trabectedin ( 78% ) or gemcitabine with docetaxel ( 16% ) .12 , 13 this correction has been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 388 kang hj , loftus s , taylor a , dicristina c , green s , zwaan cm . 
 lancet oncol 2015 ; 16 : 38594 in table 2 of the article , the dose ( mg / kg ) of dexamethasone used in the aprepitant group should read 008 ( 002019 )  . 
this correction has been made to the online version as of aug 31 , 2015 . of medical a airs , from april , 2006 , to december , 2012 , during the design and conduct of the stars trial . 
these cor rections have been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 96778 valle jw , wasan h , lopes a , et al . 
lancet oncol 2015 ; 16 : 96778 in gure 3 of the appendix of this article , parts a and b were mislabelled ; part a shows overall survival data and part b shows progression - free survival data . 
open access article distributed under the terms of cc by . correction to lancet oncol 2015 ; 16 : 1127 moss sm , wale c , smith r , evans a , cuckle h , duffy sw . 
lancet oncol 2015 ; 16 : 112332in the fourth paragraph of the results section of this article , the absolute mortality reduction in the intervention group should read 003 per 1000 womenyears . 
this correction has been made to the online version as of aug 31 , 2015 and the printed version is correct . chang jy , senan s , paul ma , et al . 
lancet oncol 2015 ; 16 : 63037in this article , the role of the funding source should read : this analysis was designed by the principal and coprincipal investigators of both trials . 
for the stars protocol , accuray speci ed that the cyberknife platform was the sole platform to be used for the study , but did not have a role in any other aspect of the study design . 
beyond providing nancial support , neither funder was in accessing involved the raw data , collection , analysis , or interpretation of the data , or writing of the report . 
dab has received grants from accuray , and is the co - owner of berry consultants , a company that designs clinical trials for pharmaceutical and medical device companies , and international healthcare consortia . 
od was an employee of accuray , as senior vice - president responses vol 16 september 2015 e427 correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections reportage a risk - based approach to experimental early phase clinical trials during the covid - 19 pandemic introduction experimental cancer medicine has evolved over the past decade , with increasing trial complexity and operational demands . 
in this perspectives piece , we reflect on the extraordinary reshaping of delivery of patient care in our experimental phase 1 cancer clinical trials unit . riskbenefit and safety in early clinical trials during the pandemic patient safety is the prime objective of early phase trials , which might need to be ranked on the basis of their risk benefit profile ( figure )  . 
drug development clinicians weigh up potential benefit from novel drugs against toxicity risk , while adhering to complex protocols to ensure accurate data collection pertaining to trial - specific endpoints . 
when initial reports suggested that patients with cancer were at increased risk of covid - 19 morbidity and mortality , it was imperative that they would be shielded to reduce exposure . 
as one of the largest oncology phase 1 trials unit in europe , treating more than 300 new patients on nearly 60 actively recruiting trials per year , we had to employ risk management strategies to safeguard patient safety while ensuring integrity of trial conduct . 
we made the unprecedented , but necessary , decision to temporarily halt recruitment onto cancer clinical trials nationally in light of concerns regarding intensive - care bed availability . for patients already participating in a phase 1 trial , the first question was whether their net clinical benefit ( clinical benefit minus toxicity ) was sufficient to expose them to the risk of contracting severe acute respiratory syndrome coronavirus - 2 ( sars - cov - 2 ) while on an investigational medicinal product ( imp )  . 
the second question was how to continue to deliver safe patient care to those continuing on trials while delivering the requirements of trial protocols and ensuring data integrity , following regulatory authority guidance . implementation of the risk assessment at the onset of the lockdown , we had 98 patients on investigational trials , with a further 29 in screening before commencement . 
34 ( 35% ) of 98 patients were deriving a clear clinical benefit without substantial toxic effects and had received more than four courses of treatment ( at least 12 weeks ) , so they continued on trial . 
novel drugs belonging to a class of drugs already studied in humans , or a combination of new and approved drugs , or combinations of drugs belonging to classes of drugs already safely combined with important clinical antitumour activity , have moderate risk . 
food - effect studies , drugdrug interaction studies , the testing of new formulations of a drug , or testing in a specific population ( eg , patients with renal or hepatic impairment ) are much lower risk . 
 vol 21 july 2020 perspectives of the 58 patients within the first 12 weeks of trial , four ( 7% ) withdrew consent due to covid - 19 concerns , 36 ( 62% ) were discontinued from trial participation because of a deemed lack of clear benefit ( progressive disease or stable disease with increasing size of target lesions )  . 
only 16 ( 28% ) of 58 patients continued on trial , with both clinicians and the patients agreeing that the riskbenefit balance merited this . of the 29 patients in screening , 15 ( 52% ) patients did not proceed to trial participation because of patient anxiety about the risks of covid - 19 or were assessed by their clinician as high risk to proceed . 
one patient had passed screening and was planned to commence an untested dose level of a novel drug , but was moved to a previously cleared dose cohort following sponsor discussion . all patients who had elected to participate or continue on study within their dose - limiting toxicity ( dlt ) reporting period had all trial - related assessments done per protocol , ensuring collection of crucial safety parameters . 
patients outside the dlt period but within first 12 weeks of trial were overseen by a combination of monitoring by telephone and in - person hospital visits , depending on adverse events and imp tolerance and including delivery of protocol - specified trial endpoint assessments ( pharmacokinetic or pharmacodynamic sampling and imaging assessments )  . 
patients who had received four or more courses of treatment were monitored by telephone ( including documenting and grading of adverse events and concomitant medications ) , with an in - person visit offered if symptoms changed . 
 those on oral imp were dispensed two courses , which could be couriered if needed , whereas those receiving intravenous imp attended unaccompanied on days of imp administration ( having been screened for covid - 19 symptoms over the telephone the day before )  . clinical trial data integrity as recommended by the uk medicines and healthcare products regulatory agency , communication between site and sponsor ensured clear documentation of contingency measures . 
we held our weekly safety multidisciplinary meeting online , and continued to discuss all trials and patients ; urgent safety updates and training pertaining to covid - 19 enabled continued oversight . 
when the timely obtaining of wet - ink signatures was no longer possible , email confirmation from a verified institutional account was deemed acceptable . centre initiatives awarded to the institute of cancer research and the royal marsden hospital national health service foundation trust . 
ub reports grants from onyx pharmaceuticals / btg international and astrazeneca ; personal fees from eli lilly , phoenix act , karus therapeutics , novartis , astellas , janssen , boehringer - ingelheim ; and other support from bayer , all outside the submitted work . 
 arm reports personal fees from janssen pharmaceuticals , faron pharmaceuticals , bayer pharmaceuticals , novartis oncology , and merck pharmaceuticals ; and other support from loxo oncology , all outside the submitted work . 
 jsdb reports personal fees and non - financial support from astellas pharma and sanofi ; grants , personal fees , and nonfinancial support from astrazeneca ; personal fees from genentech / roche , pfizer , bayer , boehringer ingelheim , merck serono , merck sharp & dohme , and janssen ; non - financial support from genmab , orion pharma gmbh , qiagen , taiho pharmaceutical , and vertex ; and personal fees and other support from cellcentric , daiichi , glaxosmithklein , menarini / silicon biosystems , and sierra oncology , all outside the submitted work . 
in addition , jsdb has a patent on 17 - substituted steroids useful in cancer treatment with royalties paid to janssen , and a patent on parp inhibitors and dna repair defects with royalties paid to astrazeneca . 
 for more on the risks of covid - 19 for patients with cancer see lancet oncol 2020 ; 21 : 33537 for more on regulatory authority guidance for covid - 19 see uk / guidance / managing - clinicaltrials - during - coronaviruscovid - 19 , and gov / regulatory - information / search - fda - guidancedocuments / fda - guidanceconduct - clinical - trials - medicalproducts - during - covid - 19public - health - emergency 890 accurate collection , collation , and transcription of clinical data remained a priority ; remote access to electronic health records and the use of video conferencing enabled the continuation of data entry and query resolution in a timely manner by staff working off - site . 
we pursued options for remote source data verification and source data review , including emailing de - identified source documents or screen sharing them using videoconferencing , prioritising the monitoring of patients within the dlt period or those with notable drug - induced adverse events , and the monitoring of other crucial data pertaining to trial - specific endpoints . horizon scanning covid - 19 is unlikely to be eradicated soon , and social distan cing and shielding will probably remain necessary for some time . 
as we plan a resumption of clinical trial activity , we can speculate on how procedures will evolve ; the postcovid - 19 clinical trials landscape will most likely look quite different to the one which preceded the pandemic . 
higher risk phase 1 trials such as first - inhuman , first - in - human combinations , and all dose - finding studies , should be done in dedicated drug development units ( figure )  . 
the high frequency of in - person visits , safety monitoring , and investigator oversight is crucial to safeguard patients . the number of new cases of covid - 19 in our hospital is low , and decreasing . 
by keeping our drug development unit as covid - 19 - free as possible , we hope to reduce the risk of patients being non - evaluable or having additional adverse events . 
 as familiarity with a novel drug increases , and with establishment of safe dose and transition to expansion phases , it might be possible to introduce a more nuanced approach while ensuring accurate data . 
as experience increases with second - generation and third - generation drugs targeting similar pathways , these phase 1 trials might be considered lower in risk and suitable for a less intense schedule . 
this adaptive approach might include reducing the frequency of in - person visits , using remote vol 21 july 2020 perspectives monitoring ( either by teleconferencing , shared care with local providers , or electronic patient - reported outcome tools )  . 
the lessons we have learnt during the covid - 19 outbreak need to be evaluated and potentially incorporated into new operating procedures and protocols . a risk - based approach to operational management is an established standard in early clinical trials . 
however , need being the mother of invention , the covid - 19 pandemic might result in new ways to increase efficiency , reduce trial costs , and , possibly accelerate drug development . 
investments in digital infrastructure will propel us towards a paperless future , with electronic site files and training documentation workflows that can simplify work processes , ensuring a robust audit trail . the changes required in response to the restrictions imposed by the covid - 19 pandemic have , in effect , telescoped the future . 
we must embrace these changes , ensuring that we continue to improve the early clinical trials process . fore more on uk recommendations for covid - 19 see lancet oncol 2020 ; 21 : 62427 for more on risk - monitoring strategies see appliedclinicaltrialsonline.com / risking - it - all - going - all - rbmadoption crescens tiu , rajiv shinde , christina yap , bindumalini rao baikady , udai banerji , anna r minchom , johann s de bono , * juanita s lopez contributed equally digital oncology digital tools for sharing genetic information with family members created by genetic risk algorithms . 
patients might also be concerned that sharing information will cause distress or harm to family members , for instance because of genetic discrimination ( ie , treating an individual or a group unjustly or prejudicially on the basis of their genetic characteristics , for example , for insurance or employment purposes )  . 
 famgenix november , 2019 , that enables users to share genetic information with relatives , including autogenerated pedigrees is a privately developed app released vol 21 july 2020 perspectives for more on jos cervical cancer trust report see jostrust.org.uk / sites / default / files / jos_physical_disability_ report_0.pdf for more on the issues of health - care access experienced by people with disabilities see editorial lancet 2019 ; 394 : 187 for more on the us study on cancer screening prevalence among adults with disabilities see prev chronic dis 2017 ; 14 : e09 disability in cancer care : time for change ? in the past few decades , numerous studies have found that provision of timely cancer screening for individuals with physical disabilities is inadequate . 
 indeed , a report by the uk charity jos cervical cancer trust , which surveyed 335 women with diverse physical disabilities and conditions , ranging from spinal muscular atrophy to cerebral palsy , found that a high proportion of respondents ( 63% ) said that they had previously been unable to attend a cervical screening appointment because they could not access screening services or did not have the option for home visits . 
these findings are worrying in terms of equality of access to cancer care , especially in the context of global issues of overall health - care access for people with disabilities . these findings are not confined to the uk . 
a study from the usa in 2017 investigated how many people with and without disabilities received recommended breast , cervical , and colorectal cancer screening tests , stratified by disability type ( hearing , vision , cognitive , and mobility )  . 
according to data from the 2013 national health interview survey , individuals with disabilities , irrespective of type , reported fewer cancer screening test visits than those without disabilities , including pap tests , mammography , and colorectal cancer screening . 
 although these barriers to access are common across many patient populations , these findings show that logistical difficulties can compound a situation in which people with disabilities are already disproportionally disadvantaged in terms of adequate can health - care include insurance cover ( despite legal requirements to protect people with disabilities by the americans with disabilities act ) , provider misperception about how to screen people with disabilities , insufficient experience coverage . 
these disadvantages with assistance for screening examinations , lack of equipment such as height - adjustable couches , in the types of services geographical variation offered , and lack of available outreach and education programmes . what both reports clearly show is that disparities persist among people with disabilities in need of preventive services and health - care access . 
not only is increased awareness needed to identify gaps in accessing cancer screening services for those with disabilities , but also robust , comprehensive , and equitable interventions to ensure that such individuals are not overlooked for cancer screening . 
 moreover , incorrect assumptions are often made about people with disabilitythe result of common stigmas perpetuated by include inability to recognise long - term health conditions or debilitating symptoms that are not visible , or a belief that people with disabilities are not sexually active and therefore do not need health - care information about cervical cancer , or hiv . 
given the diversity and complexity of disabilities that exist , it is imperative that healthcare practitioners recognise that individuals with disabilities are a heterogenous group with needs and requirements that will vary depending on the nature of their disabilities . societywhich transmitted infections , sexually regarding practical these prevailing issues can be addressed by some immediate and modest measures to increase the use of cancer care services for people with disabilities : increasing education in medical training on treating people with disability , both from a clinical perspective issues around medical and procedures ; improving accessibility to screening services in the primary - care setting ; developing better education and outreach programmes that specifically target people with disabilities ; and ensuring fair and equal access to cancer services , regardless of geographical location . 
 the lancet oncology vol 20 september 2019 1183 editorial correction to lancet oncol 2014 ; 15 : 150312 correction to lancet oncol 2019 ; 20 : 76980 correction to lancet oncol 2019 ; 20 : 98699 open - label phase 1 / 2 jg , niesvizky r , kumar sk , berdeja et al . 
 lancet oncol 2014 ; 15 : 150312in the eighth paragraph of the results section of this article , the first sentence should have been overall responses were noted in 59 ( 92% , 95% ci 8397 ) of 64 patients ( table 5 )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 765 ben - aharon i , goshen - lago t , fontana e , et al . 
this correction has been made to the online version as of july 1 , 2019 . 2018 jacob s , yap ml , wilson be , ferlay j , bray f , barton mb . 
 lancet oncol 2019 ; 20 : 76980 in the affiliations for this article , dr mei ling yap should have been affiliated with the university of new south wales ( sydney , nsw , australia )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 795805 randomised , controlled hofvind s , holen s , aase hs , et al . 
 lancet oncol 2019 ; 20 : 795805 in figure 1 , the number of patients with screen - detected breast cancer in the digital breast tomosynthesis group should have read 95 , and the number of patients in the digital mammography group should have read 87 . 
 quizartinib versus salvage chemotherapy in relapsed or refractory flt3 - itd acute myeloid leukaemia ( quantum - r ) : a multicentre , randomised , controlled , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 98699in this article , the second sentence in the statistical analysis section should have read the sample size calculation wording in the original protocol specified a 5% , two - sided calculation ; however , this wording was inaccurate , and subsequently , a one - sided calculation at 25% was implemented to solely test for superiority of quizartinib , which is consistent with the primary aim of the study . 
this correction has been made to the online version as of july 1 , 2019 , and the printed article is correct . correction to lancet oncol 2019 ; 20 : e30212 hillengass j , usmani s , rajkumar sv , et al . 
these corrections have been made to the online version as of july 1 , 2019 . vol 20 july 2019 e346 corrections published online august 6 , 2019 s1470 - 2045 ( 19 ) 30530 - 3 published online july 30 , 2019 s1470 - 2045 ( 19 ) 30521 - 2 correction to lancet oncol 2019 ; 20 : 114859 correction to lancet oncol 2019 ; 20 : 121125 bonvalot s , rutkowski pl , thariat j , et al . 
 nbtxr3 , a first - in - class radioenhancer hafnium oxide nanoparticle , plus radiotherapy versus radiotherapy alone in patients with locally advanced soft - tissue sarcoma ( act.in.sarc ) : a multicentre , phase 23 , randomised , controlled trial . 
 lancet oncol 2019 ; 20 : 114859in this article , the funder pharmaengine , inc , was inadvertently omitted and has now been added to the funding line in the summary and to the acknowledgments . 
a repeated sentence has been deleted from the fifth paragraph of the statistical analysis section of the methods , and some minor typographical errors have been corrected throughout the paper . 
 these corrections have been made to the online version as of sept 2 , 2019 . correction to lancet oncol 2019 ; 20 : 117182 nen nr , reisel d , leimbach a , et al . 
the following sentence has been added to the figure 4 caption : sdi quintiles are ordered from high to low sdi quintile , and gbd super - regions are alphabetically ordered . 
the next sentence should read : country order selected by total absolute dalys ; countries with the greatest total absolute dalys , of the fifty most populous countries in the world , are listed first . 
this correction has been made to the online version as of aug 6 , 2019 . correction to lancet oncol 2019 ; 20 : 127385 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
lancet oncol 2019 ; 20 : 127385in this article , data ( hazard ratios , 95% cis , and p values ) in the following sentence on p 1279 have been corrected : in women with stage iii disease , 5 - year overall survival was 838% ( 95% ci 784895 ) with chemoradiotherapy versus 820% ( 95% ci 765877 ) with radio therapy alone ( hr 084 [ 95% ci 052138 ] ; p = 050 ) , and 5 - year failure - free survival was 813% ( 95% ci 747863 ) with chemoradiotherapy versus 773% ( 95% ci 705827 ) with radiotherapy alone ( hr 087 [ 95% ci 056136 ] p = 054 ; appendix p 8 )  . 
on p 1282 , the same data ( hazard ratios and 95% cis ) in the following sentence have also been corrected : for women with stage iii endometrial cancer , combined adjuvant treatment yielded only a small absolute improvement of 2% ( hr 084 ; 95% ci 052138 ) in 5 - year overall survival and of 4% ( 087 ; 056136 ) in failure - free survival . 
 these corrections have been made to the online version as of sept 2 , 2019 , and the printed version is correct . correction to lancet oncol 2019 ; 20 : e41733 herrera fg , irving m , kandalaft le , coukos g . 
 this correction has been made as of july 30 , 2019 . correction to lancet oncol 2019 ; 20 : e50321 spence d , dyer r , andall - brereton g , et al . 
 lancet oncol 2019 ; 20 : e50321the affiliations of authors dingle spence and m austin argentieri have been corrected in the online version as of sept 2 , 2019 . vol 20 september 2019 e468 corrections articles lancet oncol 2008 ; 9 : 33141 published online march 19 , 2008 doi : 10.1016 / s14702045 ( 08 ) 70077 - 9 see lancet online / articles doi : 10.1016 / s01406736 ( 08 ) 60348 - 7 see lancet online / comment doi : 10.1016 / s01406736 ( 08 ) 60349 - 9 * trialists listed at end of paper correspondence to : prof john yarnold , department of clinical radiotherapy , royal marsden hospital , sutton , surrey sm2 5pt , uk the uk standardisation of breast radiotherapy ( start ) trial a of radiotherapy hypofractionation for treatment of early breast cancer : a randomised trial the start trialists group * summary background the international standard radiotherapy schedule for breast cancer treatment delivers a high total dose in 25 small daily doses ( fractions )  . 
however , a lower total dose delivered in fewer , larger fractions ( hypofractionation ) is hypothesised to be at least as safe and e ective as the standard treatment . 
we tested two dose levels of a 13 - fraction schedule against the standard regimen with the aim of measuring the sensitivity of normal and malignant tissues to fraction size . methods between 1998 and 2002 , 2236 women with early breast cancer ( pt1 - 3a pn0 - 1 m0 ) at 17 centres in the uk were randomly assigned after primary surgery to receive 50 gy in 25 fractions of 20 gy versus 416 gy or 39 gy in 13 fractions of 32 gy or 30 gy over 5 weeks . 
the protocol - speci ed principal endpoints were local - regional tumour relapse , de ned as reappearance of cancer at irradiated sites , late normal tissue e ects , and quality of life . 
 this study is registered as an international standard randomised controlled trial , number isrctn59368779 . findings 749 women were assigned to the 50 gy group , 750 to the 416 gy group , and 737 to the 39 gy group . 
the estimated absolute di erences in 5 - year local - regional relapse rates compared with 50 gy were 02% ( 95% ci 13% to 26% ) after 416 gy and 09% ( 95% ci 08% to 37% ) after 39 gy . 
photographic and patient self - assessments suggested lower rates of late adverse e ects after 39 gy than with 50 gy , with an hr for late change in breast appearance ( photographic ) of 069 ( 95% ci 052091 , p = 001 )  . 
from a planned meta - analysis with the pilot trial , the adjusted estimates of / value for tumour control was 46 gy ( 95% ci 1181 ) and for late change in breast appearance ( photographic ) was 34 gy ( 95% ci 2345 )  . 
416 gy in 13 fractions was similar to the control regimen of 50 gy in 25 fractions in terms of local - regional tumour control and late normal tissue e ects , a result consistent with the result of start trial b . 
a lower total dose in a smaller number of fractions could o er similar rates of tumour control and normal tissue damage as the international standard fractionation schedule of 50 gy in 25 fractions . introduction in women with early breast cancer prescribed radiotherapy after tumour excision or mastectomy , the e ective dose of radiation is adjusted to balance the risk of local cancer recurrence against the risk of harmful e ects on healthy tissues . 
radiotherapy reduces the risk of local relapse by about 70% and reduces breast cancer mortality.1 such treatment is o ered to nearly all patients after local tumour excision and to selected patients after mastectomy . 
this schedule has evolved pragmatically , and is based on an assumption that a high total dose delivered in small fractions of 20 gy keeps the amount of normal tissue damage to a minimum while gaining the maximum level of tumour control . 
this perception was strengthened when early studies of hypofractionation , which did not use adequate reductions in total dose , reported unacceptably high rates of normal tissue injury.2 normal and malignant tissues vary in their responses to radiotherapy fraction size , termed fractionation sensitivity . 
responses are described by a model in which the sensitivity ( measured by the degree of tissue damage for normal tissues , and tumour recurrence rates for malignant tumours ) to fraction size is represented by the ratio of two constants and .3 the lower the ratio of to ( expressed in gy ) , the greater the e ect on normal and malignant tissues of changes in fraction size . 
healthy tissues of the breast and ribcage are sensitive to fraction size , with / values 5 gy or less , 4 so small changes in fraction size can produce relatively large changes in the e ects of radiotherapy on these tissues . 
this sensitivity is typical vol 9 april 2008 articles of so - called late - reacting normal tissues that take months or years to develop atrophy or brosis after radiotherapy . 
in head and neck cancer , radiotherapy delivered in small fractions ( 20 gy ) to a high total dose spares late - responding normal tissues relative to tumour.5 breast cancer has previously been thought to be insensitive to fraction size and best treated with fractions of 20 gy or less . 
however , some trials have tested the hypothesis that breast cancer is as sensitive to fraction size as the normal tissues of the breast and underlying rib cage.68 if con rmed , these ndings could indicate that small fraction sizes of 20 gy or lower o er no therapeutic advantage , and that a more e ective strategy would be to deliver fewer , larger fractions to a lower total dose . between 1986 and 1998 at the royal marsden hospital ( rmh ) and gloucestershire oncology centre ( goc ) in the uk , 1410 patients prescribed whole breast radiotherapy after breast conservation surgery were randomised to 50 gy in 25 fractions or to two dose levels of a 13 - fraction regimen over 5 weeks39 gy in 30 gy fractions and 429 gy in 33 gy fractions.7 , 8 the primary endpoint was late normal tissue e ects , with local tumour control as a secondary endpoint , and the results were consistent with breast cancer having a similar sensitivity to fraction size as the late - reacting healthy tissues . 
based on this pilot study , the standardisation of breast radiotherapy ( start ) trials were initiated by the uk coordinating committee for cancer research ( now national cancer research institute ) to extend the testing of radiotherapy schedules using fraction sizes larger than 20 gy , in terms of local - regional tumour control , normal tissue e ects , quality of life , and health economic consequences . 
trial a maintained the explanatory design of the rmh / goc trial , with a reduction in one of the test group doses from 429 gy in 33 gy fractions to 416 gy in 32 gy fractions , following advice from the independent data monitoring committee . 
 the trial was designed to allow interpolation between two 13 - fraction regimens in order to identify the schedule equivalent to 50 gy in 25 fractions in terms of late normal tissue e ects , and to compare local tumour control at this test - dose level . 
the protocol - speci ed intent was to combine the datasets of the pilot trial and start trial a under guidance of the independent data monitoring committee to more precisely estimate the fractionation sensitivity of breast cancer . 
by contrast , start trial b9 was a more pragmatic trial that compared a commonly used schedule in the uk ( 40 gy in 15 fractions in 3 weeks ) with a control group of 50 gy in 25 fractions over 5 weeks . 
 this paper presents the results of trial a . ( continues on next page ) methods participation was open to all uk centres that provided radiotherapy treatment to patients with early breast 332 vol 9 april 2008 articles cancer . 
due to earlier completion of recruitment in trial b , those centres were invited to join trial a after accrual to trial b was complete . operable invasive breast patients women with cancer ( international union against cancer pt1 - 3a pn0 - 1 m0 ) requiring radiotherapy after surgery ( breast - conserving surgery or mastectomy , with clear tumour margins 1 mm ) were eligible for the trial if they were aged over 18 years , did not have an immediate surgical reconstruction , and were available for follow - up . 
unlike the pilot study , which had normal tissue e ects as the primary endpoint , mastectomy patients were included in trial a , since tumour control was one of the principal endpoints . 
patients from 13 centres participating in trial a were also recruited into the quality of life and health economics studies ( health economics data not reported here , baseline quality of life data have been published elsewhere10 )  . 
13 centres recruited patients who had breast - conserving surgery into the photographic assessment substudy ( 12 centres were in both the quality of life and photographic studies )  . 
patients from 12 centres also consented to donate a 20 ml blood sample for the study and to complete an associated family history questionnaire ( substudy not reported here )  . 
written informed consent was obtained for all patients . procedures start trial a patients were randomised to either 50 gy in 25 fractions ( control group ) or 416 gy in 13 fractions or 39 gy in 13 fractions ( experimental schedules )  . 
this treatment involved ve fractions per week in the control group and ve treatments per fortnight ( monday , wednesday , friday one week , tuesday and thursday the next week ) in each of the two experimental schedules . randomisation was arranged via telephone at the clinical trials and statistics unit at the institute of cancer research ( icr - ctsu ) , sutton , uk , where patient details were recorded and treatment was allocated . 
computer - generated random permuted blocks were used as the method of allocation , with patients strati ed by hospital , type of surgery ( breast conserving surgery or mastectomy ) , and intention to give a tumour bed boost dose or not . 
use of adjuvant systemic treatment was recorded , with a requirement of at least a 2 - week gap between exposure to chemotherapy and radiotherapy . patients lay in a supine treatment position . 
the planning target volume was de ned as the whole breast the total dose administered with a 1 cm margin to palpable breast tissue ; where regional radiotherapy was indicated , the planning target volume was supraclavicular nodes with or without axillary chain with a 1 cm margthe decision to give regional radiotherapy was made before randomisation and was only used in 14% of patients ( table 1 )  . 
in two patients prescribed radiotherapy to the breast and supraclavicular fossa and randomised to the 416 gy schedule , the supraclavicular fossa was reduced to 39 gy because of the sensitivity of brachial plexus to fraction size . 
most patients were treated with 6 mv x - rays , although treatment with higher energies or cobalt - rays was allowed after discussion with the start trial radiotherapy quality assurance teaplanning protocols were speci ed at the time of noti cation of participation into the study and had to conform to the minimum quality criteria described in the start trial a protocol . 
other endocrine therapies include combinations of tamoxifen / anastrozole / letrozole / exemestane / goserelin , mostly within randomised trials . table 1 : demographic and clinical characteristics at randomisation of the 2236 patients in start trial a vol 9 april 2008 articles 2236 patients randomised 749 allocated 50 gy in 750 allocated 416 gy in 737 allocated 39 gy in 25 fractions over 5 weeks 13 fractions over 5 weeks 13 fractions over 5 weeks 735 received allocated treatment * 8 refused allocated treatment 1 whole breast treatment 741 received allocated treatment * 4 given non - allocated treatment 1 whole breast treatment 731 received allocated treatment * 4 given non - allocated treatment 1 refused to complete not given 1 recurrence found 3 severe skin reactions , treatment stopped after 23 fractions 1 withdrew after randomisation due to depression not given 1 withdrew after randomisation 1 continual wound infection ( given 50 gy ) ( given 50 gy ) 1 treatment delayed for 18 days 1 found to have metastases requiring further surgery , so radiotherapy suspended treatmentiridium implant given 1 withdrew after randomisation ( given 40 gy in 20 fractions ) 5 with baseline data only 3 withdrew consent to follow - up after randomisation 2 moved 2 with baseline data only 1 moved 1 unknown 2 with baseline data only 2 withdrew consent to follow - up after randomisation 749 included in analysis 750 included in analysis 737 included in analysis figure 1 : trial pro le for start trial a * only major treatment deviations listed . 
minor deviations due to public holidays , machine service days , and machine breakdowns not included . all centres submitted details of the standard radiotherapy technique , after which a visit by the quality assurance team checked dosimetric measurements in a 2d and 3d breast phantom , including the junction region between supraclavicular fossa and tangential breast or chest wall elds.1215 the mean di erence between prescribed and measured dose in a phantom was 21% . 
additionally , a third of the radiotherapy treatment plans were collected and analysed by the quality assurance team to ensure compliance with the protocol terms of prescription point , dose homogeneity , and lung depth . 
a random sample of patients had in - vivo thermoluminescent dosimeter measurements taken.1618 the protocol allowed for a dose variation ( in the planning target volume ) between 95% and 105% of that at the reference point on the central axis . 
these results con rmed a good compliance with the technical aspects of the trial protocol . the principal endpoints speci ed in the protocol were local - regional relapse , normal tissue e ects , and quality of life . 
local - regional tumour relapse was de ned as local relapse in breast or chest wall , and regional relapse in ipsilateral axilla or supraclavicular fossa if it had been within an irradiated target volume . 
disease - free survival was de ned as time to any breast cancer - related event ( local - regional or distant relapse , contralateral breast cancer , or death from breast cancer )  . 
brachial and plexopathy was reported if damage to the brachial plexus was suspected and the patient had symptoms of pain , parasthesia , numbness , or other sensory symptoms ( graded on a 4 - point scale )  . 
photographs were taken at baseline ( post - surgery and pre - radiotherapy ) and then at 2 and 5 years to assess changes to the breast based on change in size , shrinkage , and shape , and scored on a 3 - point graded scale . 
changes in breast appearance ( photographic ) were scored by three observers blind to patient identity , treatment allocation , and year of follow - up , and a nal agreed score reached by consensus . 
the assessment of change in breast appearance from photographs was fully validated in the pilot study.7 breast size and surgical de cit were both de ned from the baseline photographs by the same three observers applying 3 - point graded scales . 
post - baseline quality of life questionnaires included an additional four protocolspeci c items relating to changes in the a ected breast after radiotherapy ( skin changes in the area of the a ected breast , overall change in breast appearance , rmness to touch of the a ected breast , and reduction in size of the a ected breast )  . 
 the trial was overseen by a steering committee of several 334 vol 9 april 2008 articles independent experts joined by members of the icr - ctsu , start trial management group , and representatives of the funding bodies ( as observers )  . 
the trial management group was responsible for the day - to - day management of the trial , and the emerging safety and e cacy data was reviewed regularly by the independent data monitoring committee . 
central statistical monitoring of data was done by icr - ctsu , supplemented by selected on - site source document veri cation . statistical analysis the sample size was estimated with the intent of measuring di erences in local - regional tumour relapse between each 13 - fraction schedule and the control group . 
a 5 - year local - regional tumour relapse rate of 10% in the 50 gy group was predicted , based on the rmh / goc pilot target sample size of 2000 patients was de ned in trial a to provide 80% power to detect a di erence of 5% in the local - regional relapse rate between the control group and each test group ( two - sided = 005 )  . 
 kaplan - meier estimates of 5 - year relapse rates , rates of normal tissue e ects , rates of any breast - cancer related event , and mortality rates were calculated ( with 95% cis )  . 
 for the patient quality of life self - assessments of normal tissue e ects an event was de ned as the rst occurrence of a moderate or marked symptom ( graded quite a bit or very much )  . 
the scores from the photographic assessments of change in breast appearance at 2 and 5 years were dichotomised as none versus mild or marked change , and the rst occurrence of such a change was taken as the endpoint for the survival analysis . 
there were too few patients with marked change in breast appearance ( photographic ) to be able to analyse this category separately . the wald test was used to compare between pairs of fractionation schedules . 
since point estimates of di erences in event rates can , by chance , be atypical of the overall pattern of di erences between schedules , estimates of the absolute di erence in 5 - year event rates taking the whole range of observation times into account were obtained by applying the hazard ratios obtained from the cox model to the kaplan - meier estimate of the rate in the 50 gy control group.23 both one - sided and two - sided 95% cis were calculated for the absolute di erence in local - regional relapse rates at 5 years , since the upper limit is of greater clinical interest , in view of concern about a possible excess risk caused by hypofractionated schedules . 
plots were censored at the median length of follow - up ( rounded to nearest year )  . a direct estimate of the / value for breast cancer was obtained by tting a cox proportional hazards regression model containing terms for total dose , and total dose multiplied by dose per fraction , to the local - regional relapse data . 
similarly , an estimate of the / value for dose - limiting normal tissues was obtained by tting the same regression model to the photographic data for change in breast appearance . 
in each case , the / ratio was calculated by dividing the two parameter estimates ( estimate for total dose / estimate for total dose dose per fraction )  . 
where appropriate , the cox models included covariates associated with relapse and late normal tissue e ects , so the resulting / value estimates ( and 95% ci ) were adjusted for prognostic factors . 
local relapse de ned as ipsilateral local tumour relapse in breast parenchyma / breast skin / chest wall skbreast cancer - related events : local , regional , or distant relapse , breast cancer death , contralateral breast cancer ( disease - free survival )  . table 2 : survival analyses of relapse and mortality according to fractionation schedule in start trial a vol 9 april 2008 articles 006 005 004 003 002 001 role of the funding source the funding sources provided peer - reviewed approval for the trial and have had representation ( as observers ) on the trial steering committee , but had no other role in the design , conduct , data collection , data analysis or the results . 
the the study or interpretation of corresponding author had full access to all the data in the study , and had nal responsibility for the decision to submit for publication . 1999 , january , results between and december , 2002 , 2236 patients were enrolled in start trial a at 17 centres in the uk ( gure 1 )  . 
a total of 1129 patients enrolled in the quality of life study and 1306 in the photographic assessment study ( with 878 patients enrolled in both substudies )  . and clinical demographic characteristics randomisation were well balanced between treatment groups ( table 1 )  . 
of the women prescribed chemotherapy , many ( 555 / 793 , 700% ) received an anthracyclinecontaining regimen , which was balanced between randomised radiotherapy schedules ( 178 / 259 [ 687% ] for 50 gy ; 185 / 264 [ 701% ] for 416 gy ; and 192 / 270 [ 711% ] for 39 gy )  . 
cyclophosphamide , methotrexate , and uorouracil combination therapy alone was prescribed in 227 women ( 286% of those receiving chemotherapy ) , which was similarly balanced between randomised groups ( 77 [ 297% ] for 50 gy ; 78 [ 295% ] for 416 gy ; and 72 [ 267% ] for 39 gy )  . 
 of the 1805 women prescribed tamoxifen or another endocrine therapy , most ( 1790 , 992% ) were continuing treatment at randomisation ( 603 / 606 [ 995% ] for 50 gy ; 611 / 618 [ 989% ] for 416 gy ; and 576 / 581 [ 991% ] for 39 gy )  . 
 data for oestrogen receptor status was not collected as part of start trial a , but routine policy in most of the centres during the accrual period was to prescribe tamoxifen only to patients who were oestrogen - receptor positive or whose oestrogen receptor status was unknown . 
there were only 29 major treatment deviations ( including early stopping of treatment , patient refusal of allocated treatment , and patients found to be ineligible for reasons including presence of relapses ) , resulting in 987% compliance with allocated treatment ( gure 1 )  . 
compliance with completion of quality of life questionnaires over 5 years was more than 90% . unadjusted / = 48 gy ( 95%ci 0163 ) number at risk 50 gy 416 gy 39 gy 50 gy ( 28 / 749 ) 41.6 gy ( 30 / 750 ) 39 gy ( 35 / 737 ) years since randomisation 50 gy 41.6 gy 39 gy figure 2 : kaplan - meier plot ( a ) and nelson - aalen cumulative hazard plot ( b ) of local - regional tumour relapse in 2236 patients / ratios were truncated at zero when the calculated limit was negative . the protocol speci ed that the start trial a data would be combined with the rmh / goc pilot study data8 to obtain a combined estimate of the adjusted / values for breast cancer and for normal tissues . 
in view of the di erences between the trials in terms of absolute rates of local relapse and patient characteristics , a meta - analysis was subsequently considered more appropriate , on the advice of the independent data monitoring committee . 
repeating the meta - analysis by pooling the adjusted estimates from each trial ( rather than using individual patient data ) made little di erence to the combined estimates ( data not shown )  . analysis included all randomised patients on an intention - to - treat basis . 
this study is registered as an international standard randomised controlled trial , number isrctn59368779 . median follow - up of surviving patients was 51 years ( iqr 4460 ) , with a maximum follow - up of 80 years . 
at the time of analysis , 1881 patients ( 841% ) were alive and without relapse , 36 ( 16% ) were alive with local - regional 336 vol 9 april 2008 articles relapse ( without distant relapse ) , 54 ( 24% ) were alive with distant relapse ( including 14 with local - regional relapse ) , 256 ( 114% ) had died ( including 43 with local - regional relapse ) , and nine ( 04% ) had no follow - up . at the time of analysis , 93 ( 42% ) patients had had local - regional tumour relapse , and the hazard ratios relative to the 50 gy group were 105 ( 95% ci 063175 ) after 416 gy and 126 ( 95% ci 077208 ) after 39 gy ( table 2 )  . 
 the estimated absolute di erences in local - regional relapse rates compared with 50 gy at 5 years were 02% ( 95% ci 13% to 26% ) after 416 gy and 09% ( 95% ci 08% to 37% ) after 39 gy . 
since the main concern over hypofractionation is an excess risk rather than a possible bene t , a more precise estimate of the potential excess risk of local - regional relapse was obtained from the upper limit of the one - sided 95% ci for the absolute di erence in 5 - year local - regional relapse rates for each 13 - fraction schedule compared with 50 gy . 
 the kaplan - meier and cumulative hazard rate plots for local - regional relapse according to fractionation schedule ( gure 2 ) illustrate the low event rate in all randomised groups . the unadjusted / value for local - regional relapse estimated from a cox proportional hazards regression model was 48 gy ( 95% ci 0163 )  . 
adjusting for prognostic factors resulted in extremely wide con dence limits , since the main e ects for total dose and total dose x dose per fraction were not independently predictive of local - regional relapse in the regression model . 
hence , the / value for local - regional relapse was left as a crude estimate . rates of distant relapse , disease - free survival , and overall survival were similar between the fractionation schedules , with no evidence of a clinically signi cant detriment for either of the hypofractionated schedules compared with 50 gy ( table 2 )  . change in breast appearance ( photographic ) was assessed in 1055 patients with both a baseline and at least one follow - up image ( 354 for 50 gy , 357 for 416 gy , and 344 for 39 gy )  . 
not all patients had photographs available at both 2 and 5 years , for reasons including the 5 - year assessment not yet being due at the time of scoring and analysis , patient refusal , and withdrawal from the photographic study due to relapse . 
there were no associations between score for change in breast appearance ( photographic ) at 2 years or patient demographic or treatment characteristics and whether or not the patient had a 5 - year assessment ( data not shown )  . 
the hazard ratios for any ( mild or marked ) change in breast appearance compared with the 50 gy group were 109 ( 95% ci 085140 , p = 062 ) after 416 gy and 069 ( 95% ci 052091 , p = 001 ) after 39 gy ( gures 3 and 4 )  . 
reported cases include three with rib fracture after bone metastases and nine after trauma . table 3 : incidence of ischaemic heart disease , symptomatic rib fracture , and symptomatic lung brosis according to fractionation schedule and persisted to 5 years . 
the / estimate for any change in breast appearance ( photographic ) was 31 gy ( 95% ci 1646 ) adjusted for age , adjuvant therapy , lymphatic radiotherapy , breast size , and surgical de cit . for least one completed patient quality of life self - assessments of late normal tissue e ects were available 1080 patients ( 957% of all patients in the quality of life study ) with a baseline and at follow - up questionnaire ( 359 for 50 gy , 364 for 416 gy , and 357 for 39 gy )  . 
according to patient quality of life self - assessments of ve key normal tissue e ects on the breast or breast area , rates of moderate or marked e ects by 5 years were similar after 416 gy and 50 gy . 
 rates of moderate or marked normal tissue e ects tended to be lower after 39 gy than after 50 gy , with a signi cantly lower rate of change in skin appearance after 39 gy than after 50 gy ( p = 0004 )  . 
in the 416 gy group , there was one case of pneumonitis 9 months after treatment and one patient who developed mild symptoms and signs of brachial plexopathy 2 years after treatment . 
the remaining 24 incidences of second primary cancers consisted of one or two cases of several di erent types . when all patients in the rmh / goc trial ( 1410 patients ) and start trial a ( 2236 ) were included in a meta - analysis , the unadjusted estimate of the / value for local - regional relapse was 41 gy ( 95% ci 0974 )  . 
adjusting for known prognostic factors ( age , chemotherapy , tamoxifen , lymphatic radiotherapy , type of primary surgery , boost , and pathological tumour size ) gave an adjusted / value for local - regional relapse of 46 gy ( 95% ci 1181 )  . 
 including all the 1202 rmh / goc trial and 1055 start trial a patients with available photographic assessment data in a meta - analysis , the unadjusted estimate of the / value for any change in breast appearance was 36 gy ( 95% ci 2449 )  . 
adjusting for age , chemotherapy , tamoxifen , breast size , and surgical de cit gave an adjusted / value of 34 gy ( 95% ci 2345 )  . discussion the results of start trial a are consistent with the hypothesis that breast cancer is as sensitive to fraction size as the normal tissues . 
the rst indication that breast cancer could be safely and e ectively treated using fraction sizes above 20 gy was rst raised more than 20 years ago , when biological models were applied to retrospective clinical data.24 , 25 in start trial a , 416 gy in 13 fractions was similar to the control regimen of 50 gy in 25 fractions in terms of normal tissue e ects and also in terms of local tumour control.24 , 25 this result is consistent with that of the start trial b , in which 40 gy in 15 fractions over 3 weeks seemed at least as safe and e ective as 50 gy in 25 fractions . 
 the fractionation sensitivity of breast cancer quanti ed by an / ratio of 48 gy , but the small number of local - regional tumour relapse events ( n = 93 ) limits precision ( 95% ci 0163 gy )  . 
statistical power is enhanced by considering the results of start trial a together with a larger number of local - regional relapses ( n = 185 ) recorded by the pilot trial over a 15 - year period.8 a meta - analysis of the pilot data and start trial a generates an / ratio for breast cancer of 46 gy ( 95% ci 1181 )  . 
the con dence limits of such an estimate are still fairly wide but closer to the estimate of / ratio for 338 vol 9 april 2008 articles normal tissue e ects of 34 gy ( 95% ci 2345 ) from the meta - analysis of the photographic assessments . 
 despite the residual imprecision in estimating fraction size sensitivity , breast cancer seems to respond di erently to human squamous carcinomas of the bronchus and head and neck region , and to experimental animal tumours characterised by / values of 10 gy or more.5 this distinction is important , not only because it has potential implications for breast cancer treatment , but also because it contributes to accumulating evidence that cancers vary in their sensitivity to fraction size.26 the molecular mechanisms fractionation sensitivity are not yet understood , but the cellular correlates include recovery from sub - lethal and potentially lethal damage.27 the ability to predict fractionation sensitivity from the tumour phenotype or genotype might allow fraction size to be adjusted more accurately to the individual cancer . governing that time , adhering the initial estimate of a 10% rate of local - regional relapse at 5 years in the 50 gy control group was based on the pilot trial started in 1986 . 
since then , improvements in surgery , radiotherapy techniques , systemic therapy , and more e ective multidisciplinary working have reduced risks of both local and metastatic breast cancer relapse . 
at to appropriate governance procedures , the potential e ects of the predicted lower than expected relapse rates were discussed by the independent trial steering committee and the independent data monitoring committee . 
since the local - regional relapse rate was lower than expected ( < 4% ) , the study actually has greater power than originally planned to detect a 5% absolute di erence ( 97% power , assuming 4% in the control group ) , which represents a much larger relative treatment e ect ( 4% in control group vs 9% in test group compared with 10% vs 15% as speci ed in the protocol )  . 
for example , with a 4% local - regional relapse rate in the control group , the study is able to detect an absolute di erence of 35% with a similar level ( 82% ) of power as originally planned . the photographic assessments of normal tissue e ects con rm a dose - response relation between the two test doses , from which a precise estimate of / value has been derived , consistent with previous published work.27 assuming a conservative / value of 3 gy for all normal tissue e ects except nerve injury , the 39 gy and 416 gy test doses are equivalent to 468 gy and 516 gy in 20 gy equivalents , respectively . 
the fractionation sensitivity of underlying lung tissue or heart might di er from that of ribcage and breast , but this uncertainty is less relevant now that the heart can usually be physically shielded when advanced techniques of radiotherapy planning and delivery are applied.28 the results of patient quality of life self - assessments of normal tissue e ects in start trial a are largely consistent with the dose response e ect seen in the photographic assessments . physician assessments of normal tissue e ects have not been presented in this paper . 
preliminary analysis of these data produce estimates of the relative e ects of the fractionation schedules which seem similar to those assessed by the photographic and patient self - assessments . 
since the level of detail included in the hospital case notes varied within and between centres , this practice , although unbiased between treatment groups , could have led to underreporting of physician - assessed normal tissue e ects . 
the results of the physician assessments will thus be the subject of a separate paper , reporting also the sensitivity of the endpoints according to method of completion of case report forms . the 115% absolute di erence in breast appearance at 5 years between the two test regimens generates a value of 14 at the steepest part of the dose - response curve ( the value measures the gradient of the dose response curve as the percent increase in e ect per percent increase in total dose delivered in 20 gy fractions29 ) , which converts into a 52% absolute increase in normal tissue e ects per 20 gy fraction . 
the local - regional relapse data from start trial a generate a value of 02 , which gives some indication of the small gains expected from dose escalation when tumour control is more than 95%.30 this nding has implications for modelling the imprecision in the estimate of breast cancer fractionation sensitivity . 
taking into account the higher 10 - year local - regional relapse rates in the rmh / goc pilot trial , the current precision of the / estimate can be shown by estimating a 95% ci for the 10 - year local - regional relapse rate of a speci c fractionation schedule . 
if the / value for tumour control is as high as 81 gy ( the upper 95% con dence limit ) , a 13 - fraction regimen matched to 50 gy in 25 fractions for late normal tissue e ects would have an anti - tumour e ect equivalent to 473 gy in 20 gy fractions , accounting for 15% more local - regional relapses compared with 50 gy in 25 fractions . 
 if the / value for tumour control is as low as 11 gy ( the lower 95% con dence limit ) , the same schedule would be responsible for 43% fewer local - regional relapses at 10 years compared with 50 gy in 25 fractions . 
with the lower 5 - year local - regional relapse rates in start ( 34% ) compared with the rmh / goc pilot trial ( 8% ) , the absolute excess local - regional is roughly half in the start patient population . vol 9 april 2008 articles a median follow - up of 5 years is too short to allow assessment of all the potential late normal tissue e ects such as cardiac damage . 
however , the rmh / goc pilot data ( median follow - up 10 years ) showed that the relative e ects of di erent fractionation schedules remain unchanged over time . 
the short - term priority is to protect the heart from exposure to radiotherapy ; something that is now possible with advanced radiotherapy technologies . is unlikely in conclusion , our data are consistent with the hypothesis that breast cancer shows similar responsiveness to fraction size as the late responding normal tissues of the breast , as indicated by the / estimates . 
 independent data monitoring committee : h lucraft ( chair , newcastle general hospital ) , m parmar ( mrc clinical trials unit , london ) , i turesson ( akadamiska sjukhuset , uppsala , sweden )  . consumers ( observers to trial management group ) : m carling ( rage ) , j pritchard ( independent ) , m king ( ex - member of rage , deceased ) , e parkin ( ex - member of rage )  . funders ( observers to trial steering committee ) : k law ( cancer research uk ) , s perkins ( medical research council ) , u wells ( department of health )  . con ict of interest statement j brown is an employee of eli lilly & company , who are not a sponsor . 
 we declare that we have no con ict of interest . acknowledgments we thank all the patients who participated in this study , and the doctors , nurses , radiographers , physicists , and data managers at the participating centres . 
we acknowledge the support of the royal college of radiologists ( uk ) and radiotherapy action group exposure ( rage ) , especially margaret king , deceased , to whom this manuscript is dedicated . 
we acknowledge the contributions of colleagues who previously worked on the trial , including c cruickshank , c dawson , e marriage , l gamaldo , c harper , d hussey ( all ex - icr - ctsu ) and a deighton , s gri ths , e miles ( all ex - trial management group )  . 
we thank cancer research uk , the uk medical research council , and the department of health for providing the funds to undertake this research ( grant g9600656 )  . 
currently , the standard treatment for patients with vulval intraepithelial neoplasia is surgery , but this approach does not guarantee cure and can be dis guring , causing physical and psychological problems , particularly in women of reproductive age . 
we aimed to assess the activity , safety , and feasibility of two topical treatments cidofovir and imiquimodas an alternative to surgery in female patients with vulval intraepithelial neoplasia . methods we recruited female patients ( age 16 years or older ) from 32 centres to an open - label , randomised , phase 2 trial . 
we randomly allocated patients to topical treatment with either 1% cidofovir ( supplied as a gel in a 10 g tube , to last 6 weeks ) or 5% imiquimod ( one 250 mg sachet for every application ) , to be self - applied three times a week for a maximum of 24 weeks . 
randomisation ( 1 : 1 ) was done by strati ed minimisation via a central computerised system , with strati cation by hospital , disease focality , and presentation stage . 
the primary endpoint was a histologically con rmed complete response at the post - treatment assessment visit 6 weeks after the end of treatment ( a maximum of 30 weeks after treatment started )  . 
this trial is registered with current controlled trials , isrctn 34420460 . findings between oct 21 , 2009 , and jan 11 , 2013 , 180 participants were enrolled to the study ; 89 patients were randomly allocated cidofovir and 91 were assigned imiquimod . 
at the post - treatment assessment visit , a complete response had been achieved by 41 ( 46% ; 90% ci 370553 ) patients allocated cidofovir and by 42 ( 46% ; 372553 ) patients assigned imiquimod . 
adverse events of grade 3 or higher were reported in 31 ( 37% ) of 84 patients allocated cidofovir and 39 ( 46% ) of 84 patients assigned imiquimod ; the most frequent grade 3 and 4 events were pain in the vulva , pruritus , fatigue , and headache . interpretation cidofovir and imiquimod were active , safe , and feasible for treatment of vulval intraepithelial neoplasia and warrant further investigation in a phase 3 setting . 
open access article distributed under the terms of cc by . introduction vulval intraepithelial neoplasia is a chronic pre malignant disorder that a ects the vulval skthe age - standardised incidence is about one case per 100 000 women per year , with a peak at 3049 years of age , and incidence has been rising over recent decades.1 , 2 vulval intraepithelial neoplasia is graded as 1 , 2 , or 3 according to the proportion of the epithelium containing undi erentiated cells , with grade 3 disease showing full thickness neoplasia.3 symptoms can be severe and include pain , itching , and dyspareunia , with treatment generally needed on these grounds alone.4 the disorder might be related to lichen sclerosus.5 more than 80% of women with vulval intraepithelial neoplasia have lesions associated with high - risk types of human papillomavirus ( hpv ) , most typically hpv type 16 . 
 persistent infection with high - risk types of hpv typically precedes deregulation of viral gene expression , leading to increased amounts of e6 and e7 oncoproteins and resulting in loss of activity of the tumour - suppressor proteins p53 and rb , respectively . 
the rate of progression to invasive disease is di cult to estimate , because most patients undergo surgery to remove lesions , but it can be up to 5% per year , or 12% a year with surgery.6 spontaneous regression happens in 12% of patients and vol 15 november 2014 1361 articles usually takes place within the rst 10 months.6 surgery ( either excision or ablation ) is the standard treatment , but this approach can be associated with substantial morbidity , 4 , 7 and recurrence is high ( 3060% ) .8 alternatives to surgery for vulval intraepithelial neoplasia are needed , and topical drugs and systemic treatments ( eg , photodynamic therapy and immunotherapy ) have been investigated . 
in previous small studies of topical imiquimod ( n15 ) , a complete response was reported in 28 ( 41% ) of 67 women with vulval intraepithelial neoplasia , but with substantial variation among studies ( 073% ) .1116 we aimed to assess the activity , safety , and feasibility of cidofovir and imiquimod in the randomised trial of topical treatment in women with vulval intraepithelial neoplasia ( rtvin ) , an open - label , randomised phase 2 trial developed in the uk on behalf of the uks national cancer research institute . methods study design and patients we did an open - label , randomised phase 2 trial at 32 teaching and general hospitals located in wales and england ( appendix p 3 )  . 
we included female patients who were age 16 years or older , had biopsy - proven vulval intraepithelial neoplasia grade 3 ( including visible perianal disease not extending into the anal canal ) within the past 3 months , and had at least one lesion that could be measured accurately with either a longest diameter of at least 20 mm or an area greater than 120 mm ( ascertained by measurement of two perpendicular dimensions )  . 
 about halfway through recruitment ( sept 28 , 2011 ) , we expanded the inclusion criterion for size of lesion from at least one lesion with longest diameter of at least 20 mm to that described , to allow more patients to be entered into the study while ensuring that all lesions would be of su cient size to allow a biopsy specimen to be taken . 
clinicians with a special interest in vulval intraepithelial neoplasia recruited the participants . we excluded early invasive disease by clinical and vulvoscopic examination ( and , if necessary , biopsy ) , which was done by skilled clinicians . 
we also excluded pregnant women ( by measurement of human chorionic gonadotropin in urine ) and patients with impaired renal function ( de ned as serum creatinine > 133 mol / l )  . 
 moreover , we excluded individuals who had received active treatment for vulval intraepithelial neoplasia within the previous 4 weeks or who had a recorded failure on imiquimod or cidofovir after treatment three times a week for a minimum of 12 weeks . 
we obtained appropriate regulatory approval from the uk medicines and healthcare products regulatory agency ( 21323 / 0020 / 001 - 0001 ) , the o ce for research ethics committees northern ireland ( 08 / nir03 / 82 ) , and nhs research and development departments at participating sites . randomisation and masking we randomly allocated patients in a 1 : 1 ratio to topical treatment with either imiquimod or cidofovir via a vol 15 november 2014 articles central computerised system by strati ed minimisation ( with an 80 : 20 random element )  . 
furthermore , masking was not possible because cidofovir gel has a very di erent appearance from imiquimod . procedures a licensed pharmaceutical unit ( st marys pharmaceutical unit [ smpu ] , cardi & vale university health board ) converted commercially available intravenous cidofovir into 1% topical gel ( the same concentration as used in the pilot study ) , 10 which was supplied to recruiting centres in 10 g tubes . 
we asked patients allocated cidofovir to spread a thin layer of the gel over the whole a ected area three times a week for a maximum of 24 weeks , with every 10 g tube to last about 6 weeks , requiring four tubes in total . 
we asked patients assigned imiquimod to spread the contents of one sachet ( 250 mg ) over the whole a ected area three times a week for a maximum of 24 weeks , requiring 72 sachets in total . 
we advised patients to apply the treatment at night and wash with aqueous cream and water the next day . if the patient was unable to tolerate three applications per week , we allowed them to reduce the dosage by one application a week , then two applications if intolerance continued . 
if new lesions arose during the trial they were also treated , but we did not include them in the assessments . at baseline , we recorded the patients medical history , did a clinical assessment of the lesion with adapted response evaluation criteria in solid tumors ( recist ; appendix pp 12 ) , did a pregnancy test , assessed toxic e ects with the national cancer institutes common terminology criteria for adverse events ( ctcae ) version 3.0 , analysed urine for protein , and did a 4 mm punch biopsy for hpv testing . 
 reporting of serious adverse events was real - time until 30 days after the last participant received their last dose of treatment . we assessed patients at 6 , 12 , 18 , and 24 weeks of treatment . 
 * included if at least one patient had an event of grade 3 or higher , or if grade 12 toxic e ects in more than 10% of the population were present in any column . table 2 : adverse events at baseline cidofovir ( n = 89 ) imiquimod ( n = 91 ) patients meeting 6 - week adherence endpoint 78 ( 88% ) 78 ( 86% ) patients with all four record cards completed * 50 ( 56% ) 37 ( 41% ) 17 ( 1618 ) 16 ( 1418 ) first 6 weeks of the study lost to follow - up withdrew from treatment ( intolerance or patients choice ) incomplete record card number of treatment applications during the 24 - week treatment stage lost to follow - up withdrew from treatment ( intolerance or patients choice ) clinician stopped treatment because of complications stopped early , progression stopped early , complete response incomplete record card number of treatment applications data are number of patients ( % ) or median ( iqr )  . 
 * record cards completed at 6 , 12 , 18 , and 24 weeks . table 3 : treatment adherence and reasons for stopping treatment 675 ( 6471 ) 630 ( 5067 ) ( de ned by adapted recist )  . 
we also took two 4 mm biopsy specimens to assess histological response and for hpv testing , and we obtained blood samples for measurement of haemoglobin , white blood cell count , urea , and electrolytes . 
if more than one lesion was present , we took the biopsy specimen from the same lesion as the original diagnostic biopsy ( and other lesions if judged clinically necessary )  . 
if no lesion was visible at the post - treatment assessment visit , we took a biopsy specimen from the same site as the original diagnostic biopsy . we followed up patients who had a histological complete response at the post - treatment assessment visit every 6 months ( at 6 , 12 , 18 , and 24 months )  . 
we also took blood samples at baseline , at 6 weeks of treatment , and at the post - treatment assessment visit , and we banked these specimens for future translational research . the 24 - week if a participant had a complete response or disease progression ( de ned by adapted recist ) at any time during treatment stage , we stopped treatment and did the post - treatment assessment visit 6 weeks later . 
patients who had stable disease or disease progression ( by adapted recist ) at the post - treatment assessment visit , for whom invasive disease had been ruled out , were eligible for crossover to the alternate treatment for a maximum of 24 weeks . 
subsequent management beyond the post - treatment assessment visit in patients without a complete response was at the discretion of the treating clinician . outcomes the primary endpoint was a histologically con rmed complete response in baseline lesions at the post - treatment assessment visit ( 6 weeks after completion of treatment , a maximum of 30 weeks after the start of treatment )  . 
secondary endpoints were adherence to the dosing regimen at 6 weeks and 24 weeks during the treatment stage ( to assess feasibility ) , toxic e ects during the 24 - week treatment stage and at the post - treatment assessment visit ( to assess safety ) , prediction of response according to hpv status , and the proportion of patients who had a recurrence ( histologically con rmed vulval intraepithelial neoplasia grade 3 ) at 12 months . statistical analysis the primary aim of the rtvin trial was to assess e cacy of cidofovir and imiquimod in terms of the primary endpoint . 
we used a flemings single - stage design in each treatment arm of the study to show e cacy for cidofovir and imiquimod separately ; the study was not formally powered to compare the complete response at 30 weeks between arms . 
if fewer than 30% of patients had had a complete response at 30 weeks in either treatment arm , the treatment would be deemed insu ciently active to warrant further study ; if , however , 45% or more patients had a complete response in either treatment arm , the treatment would be deemed worthy of further investigation . 
with flemings single - stage design , a p1 value of 030 and a p2 value of 045 , an of 005 ( one - sided ) , and 90% power , we calculated that 87 participants needed to be assigned to each treatment group , giving a total of 174 participants . 
 for the primary endpoint , we analysed each treatment arm by both intention to treat ( ie , including all patients randomly allocated to a group ) and per protocol ( ie , including all individuals who continued treat ment until 1364 vol 15 november 2014 articles complete response , disease progression , or 24 weeks )  . 
 we recorded the number of patients with a histologically con rmed complete response at the post - treatment assessment visit in each treatment group and calculated the corresponding proportion ; we used the clopperpearson exact binomial method to calculate the 90% ci for the proportion . 
to look for predictors of response in each treatment group , we did per - protocol subgroup analyses of the primary endpoint for several prede ned variables , using either pearsons test or fishers exact method ( if any cell included fewer than ve patients )  . we assessed adherence to treatment at 6 weeks and 24 weeks in terms of the median ( iqr ) number of applications during each period for all patients completing treatment ( and treatment diary cards ) up to those timepoints . 
we recorded the number of toxic e ects at baseline and in all patients who applied the assigned treatment at least once , in terms of the worst grade reported during treatment and at the post - treatment assessment visit , and we calculated proportions for each treatment group . 
these events were fatigue , pruritus , ulceration , pain in the vulva , headache , muscle pain , and proteinuria ; we reported ndings separately for these adverse events . 
for example , we compared between treatment arms the proportions of expected adverse events and of all toxic e ects of grade 2 or higher recorded during treatment , using pearsons test . 
 also , we assessed the di erence in symptom scores from baseline to the post - treatment assessment visit for pruritus and vulval pain for each treatment arm , using mcnemars test ( and fishers exact method if fewer than ve patients were recorded in any cell )  . 
we also combined data for reported serious adverse events with toxic e ects recorded on crfs . this trial is registered with current controlled trials , isrctn 34420460 . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation of data , or writing of the report . 
 five ( 6% ) of 89 patients assigned cidofovir and seven ( 8% ) of 91 patients allocated imiquimod were lost to follow - up before the rst assessment for toxic e ects and were excluded from this analysis . 
 * response assessed with adapted recist ( appendix pp 12 )  . table 5 : response of patients at the ptav and characteristics of complete responders ( per - protocol population ) results between oct 21 , 2009 , and jan 11 , 2013 , 180 patients were enrolled from 32 hospitals across the uk ( appendix p 3 ) ; 89 were randomly allocated to receive cidofovir and 91 were assigned to receive imiquimod ( gure )  . 
baseline demographics , disease variables , and hpv characteristics were balanced between treatment groups ( table 1 ) , and adverse events at baseline ( de ned by ctcae version 3 ) were also similar ( table 2 )  . five ( 6% ) of 89 patients allocated cidofovir and seven ( 8% ) of 91 assigned imiquimod either withdrew or were lost to follow - up before the rst 6 - week assessment and were regarded as non - compliant with the protocol . 
adherence to treatment was similar in each group at both 6 and 24 weeks , and the median number of treat ment applications by patients did not di er at these timepoints for either cidofovir or imiquimod ( table 3 )  . 
treatment was stopped early because of intolerance in ten ( 11% ; 95% ci 57201 ) of 87 patients allocated cidofovir and 15 ( 17% ; 98263 ) of 89 assigned imiquimod . 
adverse events of grade 2 or individuals allocated higher were less frequent in patients assigned cidofovir imiquimod compared with ( 61 [ 73% ] of 84 patients vs 73 [ 87% ] of 84 patients ; p = 0021 )  . 
the main di erences between treatments with respect to toxic e ects of grade 2 or higher were fatigue , pruritus , and headache , which were all at least 10% more frequent in the imiquimod arm ( table 4 )  . 
 toxic e ects of grade 3 or higher were similar between groups ( 31 [ 37% ] of 84 patients allocated cidofovir vs 39 [ 46% ] of 84 patients assigned imiquimod ; p = 0211 )  . 
 by per - protocol analysis , the propor tion of patients with pruritus grade 2 or higher fell signi cantly between baseline and the post - treatment assessment in both treatment groups ( cidofovir , 14 [ 19% ] of 72 patients vs ve [ 7% ] of 72 patients ; p = 0013 ; imiquimod , 15 [ 22% ] of 69 patients vs ve [ 7% ] of 69 patients ; p = 0008 )  . 
 no di erence in the proportion of patients with grade 2 or higher vulval pain was seen between baseline and the post - treatment assessment ( cidofovir , nine [ 13% ] of 72 patients vs three [ 4% ] of 72 patients ; p = 0109 ; imiquimod , four [ 6% ] of 69 patients vs four [ 6% ] of 69 patients ; p = 1000 )  . 
new lesions arose during the 24 - week treatment stage in 19 ( 21% ) of 87 patients assigned cidofovir and 11 ( 12% ) of 91 patients allocated imiquimod ; however , we do not know whether any of these new lesions arose within the treatment area or not . 
six individuals assigned imiquimod had also been immunocompromised , of whom two responded and four did not . 23 patients crossed over to the alternative treatment ( gure ) , of whom 16 had a post - treatment biopsy sample taken . 
three ( 43% ) of seven patients who received cidofovir after crossover had a complete response compared with four ( 44% ) of nine individuals who were given imiquimod after crossover . ( median is not yet mature follow - up data for the 83 patients who had a complete response follow - up 249 months [ iqr 135312 ] ) , but ndings currently suggest that complete response ( ie , absence of vulval intraepithelial neoplasia ) is maintained at 12 months . 
 at the time of this analysis , 20 ( 87% ) of 23 patients assigned cidofovir still had a complete response at 12 - month follow - up , as did 25 ( 78% ) of 32 individuals allocated imiquimod . 1366 vol 15 november 2014 articles discussion the ndings of the rtvin trial show that both imiquimod and cidofovir are safe , active , and feasible for treatment of vulval intraepithelial neoplasia grade 3 . 
as far as we know , our study is the largest to date to assess topical treatments for vulval intraepithelial neoplasia , with patients recruited from both teaching and general hospitals , supporting the relevance of these ndings to general clinical practice ( panel )  . 
although cidofovir had slightly fewer reported toxic e ects , imiquimod is available for use and is an e ective alternative to surgery that can be o ered to women with vulval intraepithelial neoplasia after exclusion of occult invasive disease . the international society for the study of vulval disease uses morphological criteria to classify vulval intraepithelial neoplasia into usual - type ( hpv - related ) or di erentiated ( non - hpv - related )  . 
in the rtvin trial , we wanted to use a de nition that was familiar to pathologists in the uk , provided a clear threshold for entry into the study , and minimised intra observer variability . 
we considered central histo logical review , but that would have caused substantial logistical di culties in an already challenging trial . table 3 shows that the primary reason for exclusion from the per - protocol analysis was withdrawal from treatment because of intolerance or by patients choice . 
data for adherence to treatment tailed o after the rst 6 weeks of the study ; however , before this timepoint , data collection was good ( around 86% ) and response to treatment did not seem to be related to adherence . 
although the rtvin trial was randomised , the flemings design is not aimed primarily at direct comparison between arms ; thus , the study was not powered to detect a di erence in e cacy between cidofovir and imiquimod . 
more adverse events were noted with panel : research in context systematic review current options for the management of vulval intraepithelial neoplasia are conservative , surgery , or an unlicensed alternative . 
 a cochrane systematic review of medical treatments for vulval intraepithelial neoplasia was done in 2011 , which comprised three randomised controlled trials of imiquimod treatment for vulval intraepithelial neoplasia , but no published studies were included for cidofovir or other topical treatments.18 findings of the three randomised trials showed a combined complete response in 36 ( 58% ) of 62 patients assigned imiquimod compared with none of 42 allocated a placebo.1921 also , two retrospective studies including outcomes after treatment with imiquimod have been published , in which complete responses were reported in 47 ( 76% ) of 62 patients and ten ( 31% ) of 32 patients.22 , 23 to date , no further randomised trials of topical treatment for vulval intraepithelial neoplasia have been completed . 
in addition to our cidofovir pilot study , in which a complete response was seen in four ( 40% ) of ten women completing treatment , 10 one further trial of topical treatment with cidofovir for patients with vulval intraepithelial neoplasia has been completeda phase 2a study in men and women with high - grade anal intraepithelial neoplasia and vulval intraepithelial neoplasia , all of whom were hiv - positive.24 treatment was for 5 days , with a 9 - day treatment gap , repeated for a total of six cycles . 
by intention - to - treat , a complete response was noted in ve ( 15% ) of 33 patients and a partial response was recorded in 12 ( 36% )  . 
an update of the cochrane review awaits publication of data from the rt3vin trial . interpretation allowing for di erences in treatment regimens , the results of previous studies accord with those of the rt3vin trial . 
our study providesto the best of our knowledgethe largest evidence - base so far from which an alternative to surgery can be o ered : either topical imiquimod or cidofovir . 
although more adverse events were noted with imiquimod , most were grade 2 , and imiquimod is already licensed for use on the vulva , is readily available for prescription within hospitals as a topical treatment , and is much cheaper than cidofovir . 
no validated method for measurement of quality of life in patients with vulval intraepithelial neoplasia was available at the start of the rtvin trial ; therefore , we did not gather these data , other than for symptoms and adverse events . 
such a method is now in development , 25 and future trials should include quality - of - life data , along with a health - economic analysis . in view of the complexity of setting up trials in uncommon disorders such as vulval intraepithelial neoplasia , future studies should allow new topical treatments to be assessed alongside existing ones in phase 3 assessments . 
in our trial , cidofovir seemed to be better tolerated than imiquimod ; therefore , in future studies , we might be able to augment complete responses vol 15 november 2014 1367 articles suggest potential predictive by increasing the dose of cidofovir in patients who do not respond initially . 
also , predictive markers for treatment response are needed urgently , because up to now , researchers have been unable to identify patients who are likely to respond to topical treatment . 
 comparing either cidofovir or imiquimod with excisional surgery will be fraught with di culty : the outcomes that are the most important to women are not always easy to measure : methods to assess quality of life will emphasise symptoms that could be associated with one treatment or another . 
in the meantime , a pragmatic approach will most likely have to be taken , whereby we explain to patients the potential bene ts and risks of the available treatment options and take their priorities for treatment into account in this di cult management decision . contributors at , af , gg , cnh , sm , and np designed and developed the study and wrote and reviewed the protocol . 
all authors have seen and approved the nal report . declaration of interests gg has received educational grants from p zer for investigator - initiated clinical trials and has acted as a statistical consultant to p zer . 
all other authors declare no competing interests . acknowledgments the rtvin trial was funded by cancer research uk ( cruk / 06 / 024 ) and cruk core funding to the wales clinical trial unit ( wctu ) at cardi university . 
gilead sciences supported the study by provision of cidofovir at a discounted price , which was funded by a central subvention from the department of health ( england ) and the national institute for social care and health research ( wales )  . 
we thank current and former sta of cardi university and cardi & vale nhs trust for supporting the development and running of this trial ; kim smith , the patients representative on the trial management group ; and members of the independent data monitoring committee and trial steering committee . 
 errata risk ratio lower limit upper limit z value p value risk ratio ( 95% ci ) meyer18 lee19 hull20 deitcher21 overall 0704 0509 0438 0690 0509 0121 0329 0188 0124 0351 4091 0789 1017 3832 0737 0391 3018 1920 0425 3571 0696 0003 0055 0671 < 00001 * noble sir , shelley md , coles b , et al . 
the burgeoning ageing population means that treating diseases of elderly people , such as cancer , have unique challenges that cannot be overcome solely by increasing health - care budgets . 
given the rising global burden of cancer , how can publicly funded health - care systems address the shortfall in cancer care services ? gaps in public services have often been filled by charities . 
in several countries , cancer charities are federally regulated to prevent mismanagement and exploitation of public funds , and have a tradition of working with governments to support patient care and research . 
for example , in canada , despite the existence of a universal health - care system , cancer charities have propped up cancer care for decades , plugging gaps in home care , travel costs , research funding , and palliative care , as well as helping patients navigate the complexities of the health system itself . 
although several provinces do not have a cancer care plan , the canadian cancer society routinely produces one for each province , in addition to working with several government agencies to create a federal strategy . 
 however , ideally charities should provide extra services and assistance in times of crisis , rather than providing basic services integrated into a health - care syste this overreliance on charity in canada has potentially perilous consequences because of the increasing budgetary strain on charities . 
 these two charities together fund more than 10% of all canadian cancer research , and their combined spending on all services has fallen by can$24 million in the past 4 years . 
the overburdened health - care system is unlikely to be able to pick up the slack , placing the residual financial responsibility on patients themselves . faced with governments struggling to rectify this shortfall in services and finding charities unable to help , patients are increasingly turning to crowdfunding to support their care . 
the online fundraising platform justgiving.com reported a seven - times increase in the number of appeals set up for patients with cancer since 2015 ; more than gb45 million was raised in 2016 , compared with 530 000 in 2015 . 
although fundraising for patients requiring novel , rare , or expensive treatments isnt new , the phenomenon of online crowdfunding is different from that done offline in the past , where money was often raised for prohibitively expensive , but effective , treatments suggested by health - care providers . 
increasingly , patients with more common diseases are taking health care into their own hands , seeking treatments that might not only be unavailable due to cost , but also absent of clinical benefit . 
crowdfunding for cancer care is also completely unregulated , lending the system itself to abuse , both by those creating false cancer claims and by those advertising unsubstantiated therapies . what are reasonable , viable alternatives ? health - care systems need to improve integration with social care to decrease overreliance on emergency care , which in turn will ensure efficient hospital discharge , outpatient management , and longitudinal care . 
moreover , publicly funded health care does not mean free care : the public are paying stakeholders in a large service project and as such are entitled to an efficient , transparent , and effective value - based syste the lancet oncology vol 18 march 2017 editorial corrections correction to lancet oncol 2011 ; 12 : 1051 correction to lancet oncol 2015 ; 16 : 634 , 637 histological sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
 independent lancet oncol 2011 ; 12 : 104552 in the discussion of this article , the second sentence of the fth paragraph should read the proportion of patients a ected by grade 34 fatigue in this study ( 7% ) is similar to that reported for trabectedin ( 78% ) or gemcitabine with docetaxel ( 16% ) .12 , 13 this correction has been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 388 kang hj , loftus s , taylor a , dicristina c , green s , zwaan cm . 
 lancet oncol 2015 ; 16 : 38594 in table 2 of the article , the dose ( mg / kg ) of dexamethasone used in the aprepitant group should read 008 ( 002019 )  . 
this correction has been made to the online version as of aug 31 , 2015 . of medical a airs , from april , 2006 , to december , 2012 , during the design and conduct of the stars trial . 
these cor rections have been made to the online version as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 96778 valle jw , wasan h , lopes a , et al . 
lancet oncol 2015 ; 16 : 96778 in gure 3 of the appendix of this article , parts a and b were mislabelled ; part a shows overall survival data and part b shows progression - free survival data . 
the appendix has been corrected as of aug 31 , 2015 . correction to lancet oncol 2015 ; 16 : 1127 moss sm , wale c , smith r , evans a , cuckle h , duffy sw . 
lancet oncol 2015 ; 16 : 112332in the fourth paragraph of the results section of this article , the absolute mortality reduction in the intervention group should read 003 per 1000 womenyears . 
this correction has been made to the online version as of aug 31 , 2015 and the printed version is correct . chang jy , senan s , paul ma , et al . 
lancet oncol 2015 ; 16 : 63037in this article , the role of the funding source should read : this analysis was designed by the principal and coprincipal investigators of both trials . 
for the stars protocol , accuray speci ed that the cyberknife platform was the sole platform to be used for the study , but did not have a role in any other aspect of the study design . 
beyond providing nancial support , neither funder was in accessing involved the raw data , collection , analysis , or interpretation of the data , or writing of the report . 
dab has received grants from accuray , and is the co - owner of berry consultants , a company that designs clinical trials for pharmaceutical and medical device companies , and international healthcare consortia . 
od was an employee of accuray , as senior vice - president responses vol 16 september 2015 e427 published online july 10 , 2020 s14702045 ( 20 ) 303892 for the survey see worldovariancancercoalition . org / wpcontent / uploads / 2020 / 06 / theimpactofcovid19 oncancerpatient organisations12thjune2020 final.pdf organisations for patients with cancer feel the brunt of covid - 19 pandemic the ongoing covid19 pandemic has disrupted all facets of cancer care , from delaying diagnoses and treatment to halting clinical trials and biomedical research . 
patient organisations have not been spared from the impact , with all aspects of their work affected , and in some cases , their very viability . to assess the impact of the pan demic in organisations for patients with cancer , a survey was done by a joint initiative of the world ovarian cancer coalition , the world pancreatic cancer coalition , the lymphoma coalition , the advanced breast cancer global alliance , and the world bladder cancer patient coalitions . 
most of the responses came from the usa ( 28 responses ) followed by australia ( ten ) , and then canada , italy , and the uk ( eight each )  . overall , the findings showed that every aspect of the work done by these organisations has been affected to varying degrees by the pandemic . 
 89% of organisations reported that they had to change their services for patients with cancer in some way , but were experiencing an increase in calls and requests for assistance from patients with cancer . 
more than half ( 57% ) of organisations have had an increase in the number of calls and emails that they have received , with a mean increase of 44% . but as the need for supportive services rose , the organisations increasingly found themselves having to cut back on their activities , advocacy , and research , with some struggling just to stay afloat . 
half of the organisations involved in raising awareness reported having to change their activities by cancelling or postponing events , whereas more than twothirds ( 68% ) involved in health professional education activities had to change their services , move materials online , or temporarily halt their programmes . 
 therefore , many of the organi sations are struggling financially and only 5% felt that they were confident of their financial position during this time . all were concerned for their viability and our survey showed that the situation is very dire and concerning in terms of the number of organisations that might not survive , said clara mackay ( world ovarian cancer coalition ) , one of the groups conducting the survey . 
the pandemic has been the perfect storm in terms of its catastrophic financial impact . mackay explained that most organisations raise money through fundraising events , and those were cancelled seemingly overnight . 
 many of the people who support charitable organisations have also faced financial uncertainty and have decreased their donations . many patients rely on the services of organisations and these services have also been cut back , as this survey indicates , said jeremy l warner ( vanderbilt university , nashville , tn , usa )  . 
i am very concerned about the financial viability of some of these organisations , large and small , and hope that there will be governmental actions to prevent insolvency , if necessary . fundraising the organisations activities was practiced by nearly all survey participants , but support more than threequarters ( 79% ) predicted that their income will decline during the next 12 months . 
across the board , every type of fundraising has been affected , including grants , major donors , online donations , and events . the average expected decrease in income was 46% , although this decrease varied from 7% to 95% . 
 about a fifth of groups feared that the decline in income would affect their viability , although a few organisations reported that they had actually had an increase in funding from sources that included major donors , grant providers , and pharmaceutical companies . 
as a result of decreased funding , 71% of organisations reported the need to review budgets and available income and over half ( 55% ) have already had to reduce costs . for those organisations involved in research , 30% reported concern about the viability of their current projects , and only 48% expect to be able to resume funding or their research when the pandemic is over . 
 key issues that affected research were continuing costs associated with projects , pauses in clinical trials , and repurposing of laboratories for covid19 research . issues related to funding was the most prominent concern , followed by concerns about patient care and lack of direct access with patients . respondents also offered advice for other groups facing similar issues . 
another was to boldly review plans , and to collaborate and share data and ideas . roxanne nelson 1020 vol 21 august 2020 news comment published online july 29 , 2013 s1470 - 2045 ( 13 ) 70364 - 4 see articles page 989 copyright buzdar . 
 the tailor study will contribute to more rational use of chemotherapy and egfr tyrosine kinase inhibitors in the treatment of nsclc , based on its molecular pro le . * jacek jassem , rafa dziadziuszko department of oncology and radiotherapy , medical university of gdask , 80 211 gdask , poland jjassem@gumed.edu.pl we declare that we have no con icts of interest . shepherd fa , rodrigues pereira j , ciuleanu t , et al . 
erlotinib versus standard chemotherapy as rst - line treatment for european patients with advanced egfr mutation - positive non - small - cell lung cancer ( eurtac ) : a multicentre , open - label , randomised phase 3 trial . 
ge tinib versus cisplatin plus docetaxel in patients with non - small - cell lung cancer harbouring mutations of the epidermal growth factor receptor ( wjtog3405 ) : an open label , randomised phase 3 trial . 
erlotinib versus chemotherapy as rst - line treatment for patients with advanced egfr mutation - positive non - small - cell lung cancer ( optimal , ctong - 0802 ) : a multicentre , open - label , randomised , phase 3 study . 
a randomised trial of erlotinib versus docetaxel as second - line treatment of patients with advanced non - small cell lung cancer and wild - type epidermal growth factor receptor ( tailor )  . 
 combination endocrine treatments unproven in breast cancer and although ovarian ablation , which was introduced more than 100 years ago , was the rst endocrine treatment for advanced breast cancer , followed by adrenalectomy and hypophysectomy . 
these ablative therapies have since been replaced by antioestrogen treatments , luteinisinghormone - releasing hormone agonists , and aromatase inhibitors.1 other endocrine treatments with di erent mechanisms of action have also become available for breast cancer : oestrogens , progestins , androgens , antiandrogens , selective oestrogen - receptor downregulators . 
 the combinations of superiority of chemotherapeutic agents with di erent mechanisms of action to single agents has been established in the treatment of early and advanced breast cancer , 2 that of combinations of endocrine treatments has not been shown.1 several combinations of hormonal agents have been assessed in patients with advanced breast cancer , with no consistent improvement in either time to progression of disease or survival.3 additionally , the combination of an antioestrogen treatment ( tamoxifen ) and ovarian suppression with luteinising - hormone - releasing hormone agonist does not lead to improvements in disease - free or overall survival when compared with antioestrogen treatment alone in premenopausal women with early breast cancer.4 a large , prospective , double - blind trial5 comparing tamoxifen with an aromatase inhibitor ( anastrozole ) and tamoxifen or anastrozole alone as adjuvant treatment for breast cancer showed that the combination did not improve either disease - free or overall survival . 
indeed , the group who received the combination was discontinued after initial analysis of the data.5 suggested aromatase that inhibitor because preclinical data6 the and combination of fulvestranta member of the newest class of hormonal agents , selective oestrogen receptor downregulators was superior to either agent alone against breast tumours in mice , three prospective studies79 have assessed this approach in postmenopausal women with advanced breast cancer . 
in the lancet oncology , stephen johnston and colleagues report results of a phase 3 , european , multicentre trial.7 postmenopausal women with hormone - receptor - positive breast cancer who had relapsed or progressed while receiving a nonsteroidal aromatase inhibitor were randomly assigned to receive fulvestrant plus anastrozole , fulvestrant plus vol 14 september 2013 comment anastrozole - matched placebo , or the steroidal aromatase inhibitor exemestane . 
no improvement in progressionfree survival was recorded in the group who received fulvestrant plus anastrozole ( median 44 months , 95% ci 3454 ) compared with fulvestrant plus placebo ( 48 months , 3655 ; hazard ratio [ hr ] 100 , 95% ci 083121 ; log - rank p = 098 ) , or in the group given fulvestrant plus placebo compared with exemestane ( 34 months , 3046 ; hr 095 , 079114 ; log - rank p = 056 )  . 
 another phase 3 study8 comparing the combination of anastrozole and fulvestrant as rst - line treatment in postmenopausal patients with hormone - receptorpositive advanced breast cancer also showed no advantages in terms of clinical e cacy for the combination compared with anastrozole alone . 
 by contrast , a phase 3 trial from north america9 compared the combination of anastrozole and fulvestrant with anastrozole alone as rst - line treatment in postmenopausal women with hormonereceptor - positive advanced breast cancer , and showed increased control of disease and survival with the combination of fulvestrant and anastrozole . 
however , as understanding of the mechanisms of resistance to endocrine treatment has improved , targeting of some pathways has resulted in new approaches that o er hope for disease control . 
 for example , postmenopausal patients with hormoneadvanced breast receptor - positive , her2 - positive cancer given endocrine and anti - her2 treatments have had longer control of disease than have those given endocrine treatment alone.1 indeed , a combination of an aromatase inhibitor with an anti - her2 treatment has been approved by the us food and drug administration for the management of postmenopausal patients with hormone - receptor - positive , her2 - positive advanced breast cancer.1 another e ective approach has been the combination of an mtor inhibitor ( everolimus ) with exemestane.10 the combination of exemestane with a histone deacetylase inhibitor ( entinostat ) has also had encouraging results.11 in conclusion , a combination of endocrine agents with di erent mechanisms of action will probably not result in a meaningful improvement in outcomes for patients with breast cancer . 
however , understanding of the mechanisms of resistance to hormonal agents continues to advance , and combinations of endocrine treatment with targeted agents that block resistance pathways should improve the outlook for patients with breast cancer that is resistant to endocrine treatment . aman u buzdar department of breast medical oncology , university of texas md anderson cancer center , houston , tx 77030 , usa abuzdar@mdanderson.org i declare that i have no con icts of interest . barrios c , forbes jf , jonat w , et al . 
use of luteinisinghormone - releasing hormone agonists as adjuvant treatment in premenopausal patients with hormone - receptor - positive breast cancer : a meta - analysis of individual patient data from randomised adjuvant trials . 
fulvestrant plus anastrozole or placebo versus exemestane alone after progression on non - steroidal aromatase inhibitors in postmenopausal patients with hormonereceptor - positive locally advanced or metastatic breast cancer ( sofea ) : a composite , multicentre , phase 3 randomised trial . 
fact : an open - label randomized phase iii study of fulvestrant and anastrozole in combination compared with anastrozole alone as rst - line therapy for patients with receptorpositive postmenopausal breast cancer . 
randomized phase ii , double - blind , placebo - controlled study of exemestane with or without entinostat in postmenopausal women with locally recurrent or metastatic estrogen receptor - positive breast cancer progressing on treatment with a nonsteroidal aromatase inhibitor . 
j clin oncol 2013 ; 31 : 212835 . 918 vol 14 september 2013 articles characterisation of retinoblastomas without rb1 mutations : genomic , gene expression , and clinical studies diane e rushlow , berber m mol , * jennifer y kennett , * stephanie yee , * sanja pajovic , brigitte l thriault , nadia l prigoda - lee , clarellen spencer , helen dimaras , timothy w corson , rene pang , christine massey , roseline godbout , zhe jiang , eldad zacksenhaus , katherine paton , annette c moll , claude houdayer , anthony raizis , william halliday , wan l lam , paul c boutros , dietmar lohmann , josephine c dorsman , brenda l gallie summary background retinoblastoma is the childhood retinal cancer that de ned tumour - suppressor genes . 
we aimed to characterise non - familial retinoblastoma tumours with no detectable rb1 mutations . methods of 1068 unilateral non - familial retinoblastoma tumours , we compared those with no evidence of rb1 mutations ( rb1 + / + ) with tumours carrying a mutation in both alleles ( rb1 / )  . 
we analysed genomic copy number , rb1 gene expression and protein function , retinal gene expression , histological features , and clinical data . findings no rb1 mutations ( rb1 + / + ) were reported in 29 ( 27% ) of 1068 unilateral retinoblastoma tumours . 
15 of the 29 rb1 + / + tumours had high - level mycn oncogene ampli cation ( 28121 copies ; rb1 + / + mycna ) , whereas none of 93 rb1 / primary tumours tested showed mycn ampli cation ( p < 00001 )  . 
rb1 + / + mycna tumours expressed functional rb1 protein , had fewer overall genomic copy - number changes in genes characteristic of retinoblastoma than did rb1 / tumours , and showed distinct aggressive histological features . 
median age at diagnosis of the 17 children with rb1 + / + mycna tumours was 45 months ( iqr 3510 ) , compared with 24 months ( 1537 ) for 79 children with nonfamilial unilateral rb1 / retinoblastoma . interpretation ampli cation of the mycn oncogene might initiate retinoblastoma in the presence of non - mutated rb1 genes . 
these unilateral rb1 + / + mycna retinoblastomas are characterised by distinct histological features , only a few of the genomic copy - number changes that are characteristic of retinoblastoma , and very early age of diagnosis . funding national cancer institutenational institutes of health , canadian institutes of health research , german research foundation , canadian retinoblastoma society , hyland foundation , toronto netralaya and doctors lions clubs , ontario ministry of health and long term care , uk - essen , and foundations avanti - str and kika . that predisposes introduction retinoblastoma set the paradigm for tumour - suppressor genes , with knudsons classic hypothesis predicting that two rate - limiting hits initiate this childhood eye cancer.1 the two hits were later attributed to the retinoblastoma gene ( rb1 ) .2 40% of children with retinoblastoma have bilateral disease . 
accepted dogma is that disruption of both rb1 alleles ( rb1 / ) initiates all cases of retinoblastoma.24 the mutant rb1 allele is identi able in blood samples of 95% of bilaterally a ected patients . 
low - level mosaicism can account for the remaining 5% of blood samples in which no mutation is found.5 previously , we have identi ed mutations in both rb1 alleles ( or promoter methylation ) in more than 95% of tumours from unilateral probands with no known family history.5 , 6 in 34% of tumours , we iden ti ed only one rb1 mutation , and in 2% we saw no disruption to rb1 . 
we obtained tissue samples and clinical data for identi cation of rb1 mutations from children in clinical care at these labora tories , and laboratory contributed both local and international families . 
we did either qm - pcr ( toronto ) or mlpa or snp analyses ( amsterdam ) to measure genomic copy numbers of ve genes known to be commonly altered in rb1 / retinoblastomas ( kif14 , dek , e2f3 , cdh11 , and mycn )  . 
we used sub - megabase resolution array comparative genomic hybridisation ( acgh ) or snp array to assess overall genomic copy numbers and nontumour cell contamination ( appendix p 3 )  . we placed three primary rb1 + / + mycna tumours in the same culture conditions that support growth of rb1 / cell lines , and we developed these into cell lines ( appendix p 4 )  . 
we stained para n - embedded sections of retinoblastomas and adjacent normal retinas for fulllength rb1 protein ( antibodies targeted n - terminal and c - terminal rb1 protein ) and mycn protein.8 we did western blots on rb1 + / + mycna and rb1 / primary tumours and cell lines , control rb1 + / + human fetal and adult retina , and lines lymphoblastoid and neuroblastoma cell ( appendix pp 34 )  . 
we did western blotting to assess the function of rb1 protein , using phospho - speci c anti - rb1 and coimmunoprecipitation of rb1 and its major e ector molecule e2f1 . 
we used endpoint reverse transcriptase pcr ( rt - pcr ) or quantitative real - time pcr to measure expression of rb1 , mycn , and genes re ecting the proliferative status and retinal derivation of tumours . statistical analysis to assess the likelihood that rb1 + / + tumours originated from two undetected rb1 mutations , we did the goodness - oft test , using default probabilities of p1 = 00025 for rb1 + / + and p2 = 09975 for rb1 / samples ( appendix pp 45 )  . 
to compare the proportion of rb1 + / + unilateral tumours at every study site and frequencies of speci c genomic copy - number changes of tumours with di erent rb1 statuses , we used fishers exact test ( appendix p 13 ) .9 we used the t test with welchs adjustment to compare the total number of bp altered per region between rb1 + / + mycna and rb1 / tumours ( appendix p 5 )  . 
 we processed normalised intensity values with the circular binary segmentation algorithm , with data ltered identify only high quality ( greater than three con rmatory probes ) and suitably sized ( > 25 kbp ) regions of clear di erential signal relative to normal ( |meansignal| > 01 )  . 
we used a contrast matrix to identify the number of di erentially abundant probes relative to normal sam ples with an empirical bayes moderation of se and a false - discovery rate adjustment 328 vol 14 april 2013 articles for multiple testing . 
to ascertain if ages at diagnosis were from a one - hit or two - hit distribution , 1 we estimated the parameter k in the equation ln s = kt ( in which s is the proportion of cases not yet diagnosed and t is age at diagnosis ) through a simple linear nointercept regres sion analysis . 
we regressed the empirical values of s on age at diagnosis , 1 assuming an exponential distribution ( one - hit ) , and in the equation ln s = kt , assuming a weibull distribution with shape parameter of two ( two - hit )  . 
to compare the relative t of these data to the two assumptions , we plotted data points for rb1 / and rb1 + / + mycna cases and the besttting curves . 
we used sas version 9.3 ( ts level 1m1 ) for analyses of number of events to initiate retinoblastoma . role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
all authors had full access to all data in the study ; the corresponding author ( blg ) had nal responsibility for the decision to submit for publication . results during clinical work in toronto , we found seven ( 16% ) of 441 unilateral retinoblastoma tumours with no rb1 mutations , no promoter methylation , and no rb1 loss of heterozygosity ( rb1 + / + )  . 
we used qm - pcr to measure , in rb1 + / + tumours , copy numbers of genes at 6p , 1q , 16q , and 2p that are characteristically gained or lost in rb1 / retinoblastoma tumours.10 unexpectedly , ve of seven rb1 + / + tumours showed striking ampli cation of the mycn oncogene ( mycna )  . 
we combined our data on 1068 primary unilateral non - familial retinoblastoma tumours after statistical analysis showed that frequencies did not di er by much ( p = 008 ) between the ve laboratories ( table 1 )  . 
 laboratories the standard sensitivity for nding the rb1 mutation in blood samples of bilaterally a ected individuals is greater than 95%.57 the probability of nding no rb1 mutations in a tumour with no rb1 loss of hetero zygosity is equivalent two independent rb1 mutations in one sample ( 005005 ) or 025% . 
qm - pcr = quantitative multiplex pcr . non - familial tumours , we identi ed 29 ( 27% ) rb1 + / + tumours , tenfold more than expected ( p < 00001 ; table 1 )  . 
 subsequently , a new patient was predicted clinically and pathologically to have an rb1 + / + mycna tumour ( t101 ) , con rmed by mycn copy number ; thus , 30 rb1 + / + retinoblastomas were included in further analyses ( appendix p 6 )  . to characterise copy numbers of genes commonly gained or lost in retinoblastomas , 10 we used qm - pcr ( toronto ) or mlpa and snp ( amsterdam ) analyses . 
except for mycn copy number , acgh ( gure 2a ) con rmed a reduced frequency in rb1 + / + mycna retino blastomas of the speci c genomic copy - number changes characteristic of rb1 / retinoblastomas ( gure 1 ; appendix p 13 ) .10 also , rb1 + / + mycna retino blastomas showed signi cantly fewer altered bp and acgh clones overall than did rb1 / retinoblastomas ( p = 0033 ; gure 2a ; appendix pp 31 , 1428 )  . we used acgh11 or snp analysis3 to study mycn ampli cations in 14 rb1 + / + mycna retinoblastomas , one rb1 + / tumour ( t33 , with 73 mycn copies ) , and one rb1 / primary tumour ( rb381 , with 92 copies of mycn )  . 
of the 35 remaining unilateral tumours tested by acgh ( ten rb1 / , 13 rb1 / + , and 12 rb1 + / + ) , 24 showed no gain or loss at mycn , and 11 had moderate gain spanning a broad region of at least 28 mbp of chromosome 2p , too large to meet the de nition of ampli cation.13 amplicon de ned by three of 14 rb1 + / + mycna tumours showed 17q213 - qter or 17q243 - qter gain ; two showed 11q loss . 
both regions are commonly altered in neuroblastoma , 14 , 15 but changes are rare in rb1 / retinoblastoma.16 , 17 other changes in rb1 + / + mycna retinoblastomas not typically seen in rb1 / retinoblastoma were gains at 14q and 18q and losses at 11p ( gure 2a ; appendix pp 1420 , 33 )  . retinoblastoma t33 ( rb1 + / ) showed high - level mycn ampli cation and loss of one copy of most of 13q , including rb1 ; we suspect that ampli cation of mycn initiated proliferation , followed by 13q deletion . 
since t33 showed several characteristics of rb1 + / + mycna tumours , we included t33 with mycna retinoblastomas in clinical analyses ( gure 2 , gure 3a ; appendix pp 32 , 34 )  . rb1 + / + mycna retinoblastomas and retinal cell types ( ganglion cells , speci c inner nuclear cells , and cone photoreceptors ) 18 expressed functional rb1 protein and showed nuclear staining for c - terminal ( gure 4a ; appendix p 34 ) and n - terminal ( data not shown ) epitopes , whereas rb1 / and rb1 + / tumours were negative or stained weakly , depending on their rb1 mutations . 
 western blots and three rb1 + / + mycna cell lines ( a3 , rb522 , and t101 ) derived from rb1 + / + mycna primary retinoblastomas showed functional , nuclear , full - length rb1 protein ( appendix pp 3435 ) , normally hypophosphorylated and hyperphosphorylated ( gure 4b ; appendix p 35 ) , and bound to e2f1 ( gure 4c ) , which is the major target of rb1 protein and controls the cell cycle.19 full - length 28 kbp rb1 transcripts were detected by endpoint and real - time immunoprecipitation age at diagnosis ( months ) rb1 / rb1 + / + mycna age at diagnosis ( months ) figure 3 : clinical features of children with retinoblastomas ( a ) age at diagnosis of children with retinoblastomas . 
 ( b ) knudson one - hit and two - hit plots for children with rb1 / or rb1 + / + mycna tumours , comparing proportion not yet diagnosed with age at diagnosis , using birth as a surrogate for initiation . 
scatterplot does not distinguish children of identical ages . children with rb1 + / + mycna tumours , dna from available blood samples showed two mycn copies . tumours showed a the 16 rb1 + / + mycna lower frequency of copy - number changes in four other genes characteristic of retinoblastoma , compared with rb1 / retinoblastoma : gain of oncogenes kif14 ( three of 16 [ 19% ] vs 55 of 89 [ 62% ] ; p = 0002 ) , dek ( one of 16 [ 6% ] vs 50 of 87 [ 57% ] ; p = 00002 ) , and e2f3 ( one of 16 [ 6% ] vs 52 of 90 [ 58% ] ; p = 00002 ) ; and loss of tumour - suppressor gene cdh11 ( two of 16 [ 13% ] vs 50 of 90 [ 56% ] ; p = 0002 ; gure 1 ; appendix pp 613 )  . 
snp analysis indicated that level of non - tumour cell contamination the rb1 + / + mycna tumours was low and similar to rb1 / tumours ( appendix p 3 )  . to probe for other genomic gains or losses , we studied dna from 48 unilateral retinoblastomas by acgh11 ( 11 rb1 + / + mycna , 12 rb1 + / + , 14 rb1 / , and 11 rb1 + / in samples from canada , germany , france , and new zealand ) and three rb1 + / + mycna tumours by snp analysis ( netherlands ; gure 2a ; appendix pp 612 , 1428 , 33 )  . 
 none of the rb1 + / + mycna retino blastomas showed any evidence of copy - number changes or translocations12 at the 330 vol 14 april 2013 articles rt - pcr in three rb1 + / + mycna primary retinoblastomas for which mrna was available ( appendix pp 29 , 36 )  . 
 by contrast , four primary rb1 / retinoblastomas expressed low rb1 transcript levels relative to fetal and adult retina . rb1 + / + mycna primary retinoblastomas ( gure 4a ) and three derived cell lines ( data not shown ) stained strongly for mycn prote mycn and ki67 transcripts ( indicative of proliferation ) were found at low levels in adult retina , at higher levels in fetal retina and in rb1 / retinoblastomas without mycn ampli cation , and at very high levels in primary rb1 + / + mycna retinoblastoma and rb1 / cell lines with mycn ampli cation ( appendix pp 29 , 36 )  . 
rb1 + / + mycna tumours showed reduced expression of the oncogene kif14 , 10 by contrast with healthy fetal retina and rb1 / primary retinoblastomas , which overexpressed kif14 ( appendix pp 29 , 36 )  . rb1 + / + mycna tumours expressed embryonic cell markers consistent with a retinal origmrna of cone cell marker x - arrestin20 and crx ( a marker of retinal and pineal lineage in rb1 / tumours , which retinoblastoma but not in neuroblastoma ) 21 were expressed in fetal retina , human adult retina , and rb1 + / + mycna and rb1 / primary retinoblastomas ( appendix p 36 )  . is strongly expressed children with rb1 + / + mycna retinoblastomas were much younger at diagnosis than were those with uni lateral rb1 / retinoblastomas . 
we estimated that 18% of children diagnosed with non - familial unilateral retinoblastoma at age 6 months or younger will have rb1 + / + mycna retino blastoma ( appendix p 5 )  . analysis of age at diagnosis versus proportion not yet diagnosed led knudson to propose his two - hit model for initiation of retinoblastoma.1 our data for 79 unilaterally a ected rb1 / patients accorded with knudsons model and t a two - hit curve , representative of two independent mutational events in a tumour - suppressor gene ( gure 3b )  . 
 similar analysis of rb1 + / + mycna tumours was inconclusive : although datapoints for 12 children diagnosed before age 10 months approximated the calculated one - hit curve , ages for older children deviated ( gure 3b )  . rb1 + / + mycna tumours had distinctive histological features , comprising undi erentiated cells with large , prominent , multiple nucleoli , and necrosis , apoptosis , and little calci cation . 
flexnerwintersteiner rosettes23 and nuclear moulding , which are characteristic of prototypic rb1 / retinoblastoma ( gure 5b ) , were absent . mycn 60 m 60 m 60 m specimen total prb1 e2f1 60 m e2f1 e2f1 e2f1 immunoprecipitate e2f1 immunoprecipitate e2f1 e2f1 e2f1 e2f1 e2f1 figure 4 : expression of rb1 and mycn ( a ) staining of adjacent retinal tissue and rb1 + / + mycna or rb1 mutant retinoblastoma for mycn protein and rb1 protein ( c - terminus antibody )  . 
 ( b ) western blots with anti - rb1 that recognises both hypophosphorylated and hyperphosphorylated rb1 protein ( total rb1 ) , phospho - rb1 ( ser795 ) antibody ( prb1 ) , and anti - e2f1 . 
 ( c ) cell lysates immunoprecipitated with antibodies against mouse igg ( negative control ) , rb1 protein , and e2f1 , and western blots done with antibodies to rb1 and e2f . clinically , rb1 + / + mycna retinoblastomas were large and invasive , in view of the young age of a ected children ( gure 5c ; appendix p 37 )  . 
 ( c ) rb1 + / + mycna retinoblastoma in an 11 - month - old child ( a2 ) with extraocular extension into the optic nerve ( triple arrows ; haemoxylin and eosin staining )  . 
 ( d ) 35 - month - old child with a small , heritable , rb1 / retinoblastoma present in the inner nuclear layer of the retina on optical coherence tomography ( oct )  . mutation of which is widely assumed to initiate all retinoblastoma ( panel )  . 
in this report , we have described a previously unrecognised form of retinoblastoma that has no evidence of rb1 muta tions , displays functional protein , and is probably initiated by ampli cation of the mycn oncogene . 1068 unilateral non - familial retinoblastomas , identi ed a distinct rb1 + / + mycna subtype that constituted 14% of the sample ( n = 15 )  . 
despite the low frequency of rb1 + / + mycna retinoblastoma , this tumour subtype was discovered and characterised independently in two laboratories ( toronto and amsterdam ) , using di erent cohorts and technologies . 
 statistical analyses show that although rare , rb1 + / + mycna retinoblastomas a ect an im portant subset of patients . rb1 + / + mycna retinoblastomas , but we did not have enough rb1 + / + tumour samples for gene expression or protein studies . 
although rb1 + / + mycna retinoblastomas have not been recognised previously as a distinct subtype , they resemble large nucleolar neuro blastomas with mycn ampli cation and poor out come.22 similar to mycn - ampli ed neuroblastomas , 15 rb1 + / + mycna tumours have less complex alterations of genomic copy number than do tumours without mycn ampli cation , suggesting that mycna could be the important driver of malignancy . 
loss of rb1 to genomic time less are rb1 + / + mycna tumours truly retinoblastomas ? these malignant subtypes arise in and express markers of embryonic retina , meeting the de nition of retinoblastoma as a blast - cell tumour arising from the retina.20 , 21 , 29 we showed intact rb1 genes in primary rb1 + / + mycna retinoblastomas with strong nuclear rb1 antibody staining . 
three rb1 + / + mycna cell lines expressed full - length rb1 mrna and inactive hyperphosphorylated and active hypophosphorylated rb1 protein that coimmunoprecipitated with e2f1 , indicating normal functional rb1 protein.19 the possibility that nonmalignant cell contamination could be masking rb1 mutations in rb1 + / + mycna tumours is ruled out because three rb1 + / + mycna cell lines grew rapidly from the primary tumours , unlike rb1 / retinoblastoma , and maintained the rb1 + / + mycna genotype of the primary tumours . although next - generation dna sequencing is a powerful discovery technique , its clinical application has not yet achieved sensitivity to match rb1 mutation technologies . 
if an rb1 mutation were detection identi ed by the next - generation enhanced read depth approach , that variant would represent convergent evolution to knockout rb1 protein with cancer progression , common in many cancers , rather than an initiating rb1 mutation . 
based on the cell - line genotypes , the mycn ampli cation would still be the event common to all cells and , thereby , the probable initiating event . we also identi ed 14 rb1 + / + retinoblastomas without mycn ampli cation . 
acgh showed genomic gains and losses that were distinct from either rb1 / or the very early presentation of rb1 + / + mycna retinoblastomas , absence of rb1 mutations , functional rb1 protein , and high mycn ampli cation in a genome with a 332 vol 14 april 2013 articles fairly stable copy number suggests that these tumours arise by somatic mycn oncogene ampli cation in a retinal progenitor cell . 
this idea is supported by the nding of one rb1 + / + mycna tumour in which mycn ampli cation was the only identi ed genomic copy - number change . 
the method by which mycn ampli cation is initiated , and whether mycn ampli cation alone is su cient to initiate retinoblastoma , remains to be shown formally . treatment , which in retinal development , the mycn protein can sup port cell division without activation of the e2f family of transcription factors ; presumably , unregu lated mycn expression associated with high - level gene ampli cation in rb1 + / + mycna tumours promotes cell division by indirect inactivation of rb1 protein.30 the relative genomic stability of rb1 + / + mycna retino blastomas could result in less resistance in rb1 / retinoblastoma associated with progressive genomic rearrangements . 
we predict that , worldwide , infants younger than 1 year24 with extraocular retinoblastoma could have rb1 + / + mycna tumours and might bene t from anti - mycn treatment.31 this idea accords with an anecdotal observation by one of us ( blg ) during review of retinoblastoma pathology slides in kenya , of rb1 + / + mycna histological ndings in an orbital recurrence , later con rmed to have 40 mycn copies . is seen the young age at diagnosis of unilateral retinoblastoma is interpreted frequently as an indication of heritable disease and is cited as a reason to try to cure the cancer without enucleation . 
although we predict that 18% of children diagnosed with non - familial unilateral retinoblastoma at age 6 months or younger will have rb1 + / + mycna retinoblastoma ( appendix p 5 ) , if tumour size is also considered , rb1 + / + mycna tumours might be clinically predictable , facilitating prompt removal of these eyes with good outcomes for children . including invasion standard care for unilateral non - familial retinoblastoma is identi cation of the rb1 mutant alleles in the tumour and examination of blood to ascertain whether either mutant allele is germline . 
diagnosis panel : research in context systematic review we systematically searched pubmed with the terms : retinoblastoma , initiation , and genetics ; retinoblastoma tumour genetics ; retinoblastoma development ; and retinoblastoma initiation . 
we identi ed no data to challenge knudsons 1971 conclusion that two rate - limiting events , 1 later shown to be loss of both rb1 gene alleles , 25 , 7 are essential , but not necessarily su cient , for development of retinoblastoma . 
we found no data to suggest other forms of retinoblastoma . interpretation with our collaborative studies , we identi ed a previously unrecognised disease : retinoblastoma with normal rb1 genes , apparently driven by mycn oncogene ampli cation . 
attempts to salvage the eye on the assumption of heritable disease in young children could incur high treatment morbidity and failure to cure these aggressive oncogene - driven retinoblastomas . rb1 status rb1 protein expression mycn copy number mycn mrna expression histological characteristics classic rb1 ( cid : 8 ) / ( cid : 8 ) novel rb1 / mycna / rare moderate rosettes full - length , nuclear , phosphorylated , binds e2f1 high multiple nucleoli and blast cells speci c and general genomic gains and losses common uncommon 29 copies , wide region 28121 copies , narrow amplicon median ( iqr ) age at diagnosis ( months ) 24 ( 1537 ) 45 ( 3510 ) table 2 : di erences between classic rb1 ( cid : 8 ) / ( cid : 8 ) tumours and novel rb1 / mycna unilateral non - familial retinoblastoma of rb1 + / + mycna retinoblastoma strongly suggests nonhereditary disease , with normal population risks for retinoblastomas in the other eye and for other cancers throughout life , and no familial risks . our ndings challenge the longstanding dogma that all retinoblastomas are initiated by rb1 gene mutations . 
 rb1 + / + mycna retinoblastoma di ers from classic retinoblastoma in terms of both genetics and clinical characteristics ( table 2 ) , with immediate relevance to patients . contributors der recognised the initial connection between mycn ampli cation and rb1 mutation status , did the literature search and qm - pcr analysis , supervised rb1 mutation analysis , coordinated collaborations with the other sites , and made a major contribution to preparation of the report . 
hd and twc did the vol 14 april 2013 articles literature search , assisted with data analysis and ideas for the discussion , and contributed to preparation of gures and the report . 
rg discovered and characterised the rst tumour with mycn ampli cation and normal rb1 protein ( rb522 ; now rb1 + / + mycna ) and provided the cell line and western blot showing multiple bands of rb1 protezj and ez did western blots speci c to phosphorylated rb1 protekp and acm provided and interpreted clinical data and images . 
all authors contributed ideas and helped to write the report . con icts of interest blg was part - owner of solutions by sequence and was a board member of retinoblastoma solutions ( now impact genetics , of which blg is medical director )  . 
all other authors declare that they have no con icts of interest . acknowledgments we thank the sponsors of the study : the national cancer institute national institutes of health ( grant 5r01ca118830 - 05 [ blg ] ) ; canadian institutes for health research ( grants mop - 86731 , mop - 77903 , and mop - 110949 [ wll ] , and mop - 77710 [ ez ] ) ; the canadian retinoblastoma society ; hyland foundation ; toronto netralaya and doctors lions clubs ; the alcon research institute ; the ontario ministry of health and long term care ; retinoblastoma solutions and solutions by sequence ( now impact genetics ) ; the german research foundation ( grant lo 530 / 6 - 2 ) ; uk - essen ; avanti - str ( jcd , j cloos , and acm ) ; kika ( jcd , h te riele , j cloos , acm ) ; vu university medical center ; ontario institute for cancer research and the government of ontario ( pcb ) ; cca / v - ici / avanti - str ( bmm ) ; the vision science research program of the university health network and the university of toronto ( sy ) ; and queens university school of medicine ( great west life studentship [ rp ] )  . 
we thank : irsan kooi ( vu university medical center ) for assessment of normal - cell contamination by snp data ; leslie mackeen for the collage of retcam images in gure 3b ; valerie white ( university of british columbia ) for clinical and pathological details and images ; cynthia vandenhoven for clinical images in gure 5 ; members of the vu university medical center / the netherlands cancer institute , institut curie , institut fr humangenetik , toronto retinoblastoma teams , and other colleagues for useful discussions ; and the children and families who donated tissues for these studies . 
 correction to lancet oncol 2019 ; 20 : 168190 correction to lancet oncol 2020 ; 21 : 24249 correction to lancet oncol 2020 ; 21 : 27182 j - y , lee kh , ahn m - j , han et al . 
lazertinib in patients with egfr mutation - positive advanced non - smallcell lung cancer : results from the dose escalation and dose expansion parts of a first - in - human , open - label , multicentre , phase 12 study . 
olanzapine 5 mg plus stand ard antiemetic therapy for the prevention of chemotherapy - induced nausea and vomiting ( j - force ) : a multicentre , randomised , double - blind , placebocontrolled , phase 3 trial . 
tumour treating fields in combination with pemetrexed and cisplatin or carboplatin as first - line treatment for unresectable malignant pleural mesothelioma ( stellar ) : a multi centre , single - arm phase 2 trial . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 26170 drilon a , siena s , dziadziuszko r , et al . 
 lancet oncol 2020 ; 21 : 26170in the results section of this article , the median treatment duration for patients with cd74ros1 fusions should have been 146 months ( iqr 72181 ) and the median intracranial progression - free survival in 20 patients with cns disease should have been 77 months ( 95% ci 38193 )  . 
 lancet oncol 2019 ; 21 : 27182in the statistical analysis section of this article , the overall safety - evaluable population should have included safety data from the paediatric phase 1 study startrk - ng patients aged 4920 years . 
this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . correction to lancet oncol 2020 ; 21 : e10 f i e l d s tr e a t i n g ceresoli gl , gianoncelli l , grosso f , on behalf of stellar investigators . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 22232 strm p , kartasalo k , olsson h , et al . 
 this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . vol 21 february 2020 corrections effect of delays in the 2 - week - wait cancer referral pathway during the covid - 19 pandemic on cancer survival in the uk : a modelling study amit sud * , bethany torr * , michael e jones , john broggio , stephen scott , chey loveday , alice garrett , firza gronthoud , david l nicol , shaman jhanji , stephen a boyce , matthew williams , elio riboli , david c muller , emma kipps , james larkin , neal navani , charles swanton , georgios lyratzopoulos , ethna mcferran , mark lawler , richard houlston , clare turnbull summary background during the covid - 19 lockdown , referrals via the 2 - week - wait urgent pathway for suspected cancer in england , uk , are reported to have decreased by up to 84% . 
we aimed to examine the impact of different scenarios of lockdown - accumulated backlog in cancer referrals on cancer survival , and the impact on survival per referred patient due to delayed referral versus risk of death from nosocomial infection with severe acute respiratory syndrome coronavirus 2 . methods in this modelling study , we used age - stratified and stage - stratified 10 - year cancer survival estimates for patients in england , uk , for 20 common tumour types diagnosed in 200817 at age 30 years and older from public health england . 
we quantified the annual numbers of cancers at stage iiii diagnosed via the 2 - week - wait pathway using 2 - week - wait age - specific and stage - specific breakdowns . 
 from these numbers , we estimated the aggregate number of lives and life - years lost in england for per - patient delays of 16 months in presentation , diagnosis , or cancer treatment , or a combination of these . 
we assessed three scenarios of a 3 - month period of lockdown during which 25% , 50% , and 75% of the normal monthly volumes of symptomatic patients delayed their presentation until after lockdown . 
using referral - to - diagnosis conversion rates and covid - 19 case - fatality rates , we also estimated the survival increment per patient referred . findings across england in 201316 , an average of 6281 patients with stage iiii cancer were diagnosed via the 2 - week - wait pathway per month , of whom 1691 ( 27% ) would be predicted to die within 10 years from their disease . 
 delays in presentation via the 2 - week - wait pathway over a 3 - month lockdown period ( with an average presentational delay of 2 months per patient ) would result in 181 additional lives and 3316 life - years lost as a result of a backlog of referrals of 25% , 361 additional lives and 6632 life - years lost for a 50% backlog of referrals , and 542 additional lives and 9948 life - years lost for a 75% backlog in referrals . 
compared with all diagnostics for the backlog being done in month 1 after lockdown , additional capacity across months 13 would result in 90 additional lives and 1662 live - years lost due to diagnostic delays for the 25% backlog scenario , 183 additional lives and 3362 life - years lost under the 50% backlog scenario , and 276 additional lives and 5075 life - years lost under the 75% backlog scenario . 
however , a delay in additional diagnostic capacity with provision spread across months 38 after lockdown would result in 401 additional lives and 7332 life - years lost due to diagnostic delays under the 25% backlog scenario , 811 additional lives and 14 873 life - years lost under the 50% backlog scenario , and 1231 additional lives and 22 635 life - years lost under the 75% backlog scenario . 
a 2 - month delay in 2 - week - wait investigatory referrals results in an estimated loss of between 00 and 07 life - years per referred patient , depending on age and tumour type . interpretation prompt provision of additional capacity to address the backlog of diagnostics will minimise deaths as a result of diagnostic delays that could add to those predicted due to expected presentational delays . 
overall , studies are highly heterogeneous in design and findings , including the durations of delay studied , the duration of survival follow - up , the method by which impact is captured ( percentages , odds ratios , hazard ratios ) , and how and when staging is done . 
to our knowledge , no study had modelled the impact in lives and life - years lost of systematic delays in referral pathways in a standardised fashion across tumour types until we recently reported a health - care resource analysis focused on systemic delays at point of surgery . added value of this study across multiple tumour types , we used a standardised approach using per - day fatality hazard ratios to quantify the effect of different durations of delay on survival , examining both the referred patient and the diagnosed patient , and examining delays for individual tumour types and subtypes and aggregated across major tumour types . 
 although pertinent to ongoing forecasting of the impact of covid - 19 - related delays , these models could apply to any systemic delays to cancer pathways . implications of all the available evidence incorporating previous observational studies of delay and examining crudely estimated , non - naturalistic per - patient delays , our models predict that covid - 19 - related delays in presentation , diagnosis , and subsequent treatment , will result in loss of life and life - years that varies widely according to patient age and tumour type . 
data regarding the true duration and extent of service disruption and per - patient cancer pathway delay across the uk as a result of the covid - 19 lockdown are currently immature . 
direct predictions regarding attributable cancer deaths will be possible once more accurate patient - level data become available . any delay in cancer treatment has the real risk of patients tumours progressing from being curable ( with near - normal life expectancy ) to becoming non - curable ( with very reduced life expectancy )  . 
specific pathways have been established in the uk for referral from primary care for urgent specialist evaluation and investigation of individuals with so - called red flag symptoms suggestive of a specific cancer type , termed the 2 - week - wait pathway . 
 reductions of up to 84% have been reported in 2 - weekwait referrals in marchmay , 2020 ( lawler m , unpublished ) .24 large backlogs of patients accrued as a consequence of the lockdown are predicted to first place pressure on diagnostic services in secondary care , and affect other areas of the pathway thereafter.5 we aimed to address two key questions relating to this potential surge in presentations of symptomatic patients . 
second , accounting for the risk of death associated with nosocomial severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection , we examined the gain in survival and life - years through prompt investigation per patients referred via 2 - week - wait investigatory referral by age group and tumour referral group ( the high - level grouping of tumour types via which referrals are made [ appendix 1 pp 45 ] )  . 
to do these analyses , we developed a model using data on 10 - year cancer survival for 200817 ( stratified by age and cancer stage ) combined with a per - day hazard ratio ( hr ) for delay and applied it to agespecific and stage - specific case and referral volumes based on the 2 - week - wait pathway.6 methods data sources in this modelling study , we obtained patient numbers , agestratified and cancer stage - stratified 5 - year ( 201317 ) and age - stratified 10 - year ( 200817 ) cancer survival data for all diagnoses , and those cancers associated with surgical resection for non - haematological malignancies , from public health englands national cancer registration and analysis service ( ncras ) , including by subtype of breast cancer ( appendix 1 pp 13 )  . 
we obtained data on route to diagnosis by age and cancer stage from national health services ( nhs ) england clinical commissioning groups collections.7 we used data on proportion of referrals for suspected cancer that translated into cancer diagnoses ( the diagnostic - con version rate ) from cancer waits - faster diagnosis standard data for west london , uk , for 201920.8 we used data from across england for cancer cases diagnosed when the patient was aged 30 years or older . 
we concentrated our analysis on the 20 most common cancers referred via 2 - week - wait pathways , for which we analysed ncras survival data from 2 314 822 cancer cases ( 200817 ) and 2 - week - wait diagnoses for 385 156 cancer cases ( 201316 ) ( appendix 1 pp 45 )  . 
 we calculated life expectancy on the basis of uk office of national statistics life tables for 201618.9 we estimated nosocomial infection rates and median duration of hospital stay for treatment of each cancer type on the basis of aggregated and anonymised information from 1036 vol 21 august 2020 articles three large uk surgical oncology centres ( gronthoud f , unpublished )  . 
since long - term survival rates for most cancers are only known 510 years after diagnosis , we used 10 - year cancer stage - specific survival data in our calculations . 
 because 10 - year stage - specific survival data are not directly available for recent cancer cohorts in england , we estimated these data using established methods , by taking the ratio of stage - specific to all - stage 5 - year survival data and applying it to 10 - year all - stage survival data.12 we used the midpoint per 10 - year age group for life expectancy to estimate life - years gained , averaged per patient.9 to calculate covid - 19 - related mortality in patients with cancer , we first estimated peri - surgical mortality from nosocomial infection as the product of operationspecific duration of surgical admission , age - specific casefatality rates , and the rate of nosocomial infection per day ( 1% , 2% , 5% , or 10% )  . 
then we estimated covid - 19related mortality in the community ascribing the patient a year of active cancer management status ; this estimate was the product of the likelihood of community - acquired covid - 19 during the year ( 1% , 10% , 20% , or 50% ) , agespecific case - fatality rates , and the increase in covid - 19 case - fatality rate as a consequence of cancer as a comorbidity ( two times or five times ) .10 , 11 for the calculation of the hr for per - day delay in management , we used published data on the impact of delay in cancer surgery on overall survival for stage iiii disease to estimate per - day hrs associated with delay to definitive treatment.1321 since sufficient observational data were only available to generate summary delay hrs for breast , colorectal , and bladder cancers , we assigned delay hrs to other tumours on the basis of similarity of 5 - year survival , categorising tumour progressiveness as being low ( with a 5 - year survival for stage ii disease being > 90% ) , moderate ( 5090% ) , or high ( < 50% )  . 
because of the scarcity of published observational data on tumours of high progressiveness ( eg , oesophageal and gastric cancers ) , we conservatively considered this group as having a similar delay hr as moderately progressive tumours ( appendix 1 pp 13 )  . 
finally , we assumed that delay to treatment for stage iv cancer would not affect 10 - year survival . because patients younger than 60 years with stage iiii cancers typically have treatment with curative intent , we generated the stage - specific ratio from this group of those having major resection to those having other definitive treatment ( eg , endoscopic resection or curative radiotherapy )  . 
we applied this ratio to age - specific and cancer stage - specific strata for those aged 60 years and older having major resection to estimate the proportion of patients who have been diagnosed who are having other types of definitive treatment . to estimate 10 - year survival for individuals diagnosed with stage iiii cancer who have no delay in treatment , we used ncras 10 - year survival data and adjusted for covid - 19 - related peri - surgical and community mortality . 
 to estimate 10 - year survival associated with delay , we applied the delay hr relating to the specified number of days of delay , along with the covid - 19 - related perisurgical and community mortality , to the ncras 10 - year survival ( formulas are in appendix 1 [ pp 13 ] )  . 
we conservatively assumed that no additional downstream delays would occur after the diagnostic delay . we quantified the annual numbers of cancers diagnosed via the 2 - week - wait pathway using the 2 - week - wait age - specific and stage - specific breakdowns . 
from these , our outcome measures were estimated aggregate number of lives lost and life - years lost in england for per - patient delays of 16 months . scenarios analysed using the model we assessed the scenario of a 3 - month period of lockdown during which a proportion of symptomatic patients delayed their presentation until after lockdown ( ie , backlog patients ) , set at 25% , 50% , and 75% of normal monthly volumes . 
we modelled all backlog patients presenting in month 1 after lockdown or with variable presentation across months 13 ( appendix 2 )  . lives and life - years we then did a per - patient riskbenefit analysis for 2 - week - wait investigatory referral . 
we combined per - day rates of nosocomial infection with the age - specific covid - 19 case - fatality rates to quantify the covid - 19 - related fatality associated with investigatory referral . 
we combined this estimate with a so - called tech nical fatality risk for invasive investigations ( eg , a one in 10 000 risk of death from perforation from colonoscopy ) 22 to produce a combined per - referral mortality . using the diagnostic - conversion rates , we estimated the survival benefit per patient from an investigatory referral for each age group and tumour group . 
we considered the potential to delay referral by 2 , 4 , and 6 months against varying rates of nosocomial infection per investigatory see online for appendix 2 vol 21 august 2020 1037 articles age group ( years ) 3039 4049 5059 6069 7079 bladder 1579% 1495% 1429% 1548% 1715% 1703% brain 1175% 1415% 1782% 1824% 1664% 1670% breast 488% 327% 249% 214% 371% 770% cervix 559% 903% 1220% 1573% 1798% 1552% colorectal 1022% 1138% 1082% 1059% 1310% 1636% kidney 501% 650% 853% 1053% 1310% 1741% larynx 1107% 1429% 1345% 1494% 1586% 1679% liver 1668% 1729% 1617% 1467% 1189% 1478% lung 1687% 1826% 1680% 1537% 1178% 670% melanoma of skin 313% 396% 489% 566% 732% 1256% oesophagus 1685% 1621% 1612% 1518% 1228% 459% oral cavity 1283% 1698% 1827% 1828% 1788% 1662% oropharynx 1179% 1448% 1677% 1831% 1708% 1373% ovary 724% 1387% 1738% 1828% 1708% 1586% pancreas 1286% 1176% 1211% 900% 718% 1074% prostate 068% 067% 032% 369% stomach 1858% 1854% 1803% 1734% 1611% 885% testis 058% 036% thyroid 011% 063% 035% 022% 063% 162% 257% uterus 243% 527% 868% 1183% 1443% 076% 133% 604% figure 1 : reduction in 10 - year net survival incurred from a 3 - month delay for the 20 most common tumour types , by age group red indicates the highest decile of survival decrement , scaling down through orange and yellow to pale green , which indicates the lowest decile of survival decrement . 
we estimated benefit in proportional survival and life - years gained from gain in cancer survival versus fatality risk ( covid - 19 and technical )  . the combined statistical analysis we combined indivi dual log ( hr ) s , by stage and days of delay , using weighted linear regression to calculate the summary per - day delay - log ( hr ) ( ie , delay hr ) and sd of this estimate ( ie , se ) , expressing it as a percentage of the estimate . 
we did multivariate sensitivity analyses across ranges of para meter estimates , including 2 sd of delay hr and per day nosocomial infection rates of 1% , 2% , 5% , and 10% . 
unless otherwise specified , we applied the default values for likelihood of community - acquired covid - 19 , which was 20% , and per - day rate of nosocomial infection , which was 2% , which were selected to be conservatively high . 
for cancer - related increase in mortality due to community - acquired covid - 19 , we used a default value of two times , which is at the low - tointermediate end of the published estimates ( reflecting a non - metastatic cancer population ; appendix 1 p 1 )  . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results for several cancers , including those of the colorectum , oesophagus , lung , liver , bladder , pancreas , stomach , larynx , and oropharynx , a 3 - month delay to diagnosis is predicted to result in a reduction in long - term ( 10 - year ) survival of more than 10% in most age groups ( figure 1 )  . 
differences in the effects of a 3 - month diagnostic delay were observed for different cancer stages across all tumour types and for different subtypes and stages of breast cancer ( appendix 1 p 7 )  . the aggregated impact of universal delays in the 2 - week - wait pathway on lives lost and life - years lost varies widely by tumour type ( figure 2 )  . 
these predicted outcomes are driven by aspects of the model including age - specific incidence , the proportion of cancers diagnosed via the 2 - week - wait pathway , the proportion of cancers diagnosed as stage iiii via the 2 - week - wait pathway , and tumour the aggressiveness of ( appendix 1 pp 45 )  . 
similarly , pancreatic , gastric , and liver cancers only contribute moderately to the estimated total lives and life - years lost because fewer patients present via the 2 - week - wait pathway and high proportions have stage iv disease at presentation ( appendix 1 pp 45 )  . the across the 20 cancer types , on average an estimated 243 098 cancers are diagnosed annually . 
of these , an estimated 96 289 are diagnosed via the 2 - week - wait pathway , of which 75 369 ( 783% ) are diagnosed at stage iiii ( table )  . 
20 293 ( 269% ) of 75 369 patients would be predicted to die due to cancer within 10 years of diagnosis , representing a loss of 304 129 life - years . 
a uniform per - patient delay of 1 month would be predicted to result in attributable additional lives lost of 1412 and 1038 vol 21 august 2020 articles attributable lives lost by length of delay attributable life - years lost by length of delay 1 month 2 months 3 months 4 months 5 months 6 months 1 month 2 months 3 months 4 months 5 months 6 months 2979 4633 6365 8139 9910 breast 41 845 22 678 1014 1312 1629 9839 15 339 21 255 27 608 34 418 cervix 2128 1246 1636 2054 colorectal 32 979 10 620 1366 1773 2196 4308 9126 14 460 20 296 26 591 33 275 number of cases diagnosed per year number of cases diagnosed per year via pathbladder 8524 3654 brain 8102 7642 3339 1161 1710 2142 1594 kidney 8764 2459 larynx liver 1850 4712 lung 36 668 10 343 melanoma of skin 12 110 oesophagus oral cavity oropharynx 7427 2629 2905 ovary 6398 pancreas 8260 prostate 40 834 19 272 stomach 5332 1654 testis 1355 thyroid 2673 1430 4733 3605 2501 1498 1171 1968 1079 6873 5403 2850 1415 3143 1692 4011 2145 1379 5239 4452 2344 5897 7471 3027 3725 9704 12 030 13 829 15 128 8756 12 614 17 028 22 051 4952 5665 6163 2864 1866 3551 4183 2347 2810 1411 2051 2619 3096 3475 1688 3445 7027 8765 10 406 uterus 7604 4390 1837 3932 6305 8970 11 936 15 201 total 243 098 96 289 1412 2892 4429 6013 7633 9280 25 812 53 057 81 589 111 263 141 950 173 540 figure 2 : annual lives and life - years lost attributable to delay , aggregated for all patients diagnosed via the 2 - week - wait pathway for the 20 most common tumour types based on 10 - year net survival data for england , uk , 200817 . 
greatest decrements in lives and life - years lost are shown in darker shades of orange . life - years lost of 25 812 and a per - patient delay of 6 months would be attributed to an additional 9280 lives and 173 540 life - years lost over the subsequent 10 years for an annual cohort of cancer cases diagnosed via 2 - week wait at stage iiii ( figure 2 )  . on the basis of preliminary estimates of 2 - week - wait referral decreases , we estimated the predicted effects of 25% , 50% , and 75% reductions in presentations over a 3 - month lockdown period ( appendix 2 ) .24 based on data for 201316 , for these 20 cancer types on average an estimated 149 000 2 - week - wait referrals are made each month , resulting in 8024 diagnoses of cancer , of which 6281 are diagnosed at stage iiii ( appendix 1 pp 45 )  . 
 1691 ( 27% ) of these 6281 patients will typically die from their cancer within 10 years.7 we estimated the national toll of presentational delay accrued over a 3 - month lockdown period to be 181 attributable additional lives and 3316 life - years lost for a backlog rate of 25% , 361 additional lives and 6632 life - years lost for a backlog rate of 50% , and 542 additional lives and 9948 life - years lost assuming a backlog rate of 75% , with an average presentational delay of 2 months per patient . 
assuming the patients all present in month 1 after lockdown , normal diagnostic capacity would need to work at least 175% under the 25% backlog scenario , 250% under the 50% backlog scenario , and 325% under the 75% backlog scenario to clear the backlog ( appendix 2 )  . 
however , it is unlikely that all extra diag nostic capacity required can be provided in a single month ; therefore , we estimated the additional lives and life - years that might be lost due to subsequent diagnostic delays . 
diagnostic conversion rates reflect all diagnoses of invasive cancers ( exceptions are that breast includes carcinoma in situ , skin excludes basal cell carcinomas , urology excludes pta bladder tumours )  . 
conversely , delayed additional capacity provided across months 38 after lockdown would result in 401 additional lives and 7332 life - years lost due to diagnostic delays under the 25% backlog scenario , 811 additional lives and 14 873 life - years lost under the 50% backlog scenario , and 1231 additional lives and 22 635 life - years lost under the 75% backlog scenario ( appendix 2 )  . we assessed the riskbenefit balance per individual for investigatory referral , considering different rates of nosocomial infection . 
first , we considered absolute survival benefit , comparing prompt referral , diagnosis , and management with no referral or subsequent medical intervention ( appendix 1 p 9 )  . 
if the risk of infection is high ( 25% per referral ) , for patients older than 70 years , the risk associated with investigatory referral might exceed the absolute survival benefit for tumour - referral groups with poorer outcomes , such as upper gastrointestinal ( pancreas , oesophagus , liver , and stomach ) and brain tumours ( appendix 1 p 9 )  . second , we sought to address a common dilemma for primary care physiciansnamely , to establish in which patients referral could be delayed by a few months , either to await reduction in nosocomial infection rates or to reduce pressure on diagnostic services . 
a 2 - month delay in 2 - week - wait investigatory referrals results in an average loss of between 00 and 07 life - years per referred patient , depending on age and tumour type ( appendix 1 p 12 )  . 
we compared risk of death from investigatory referral with delay - associated increase in risk of cancer death per patient referred ( figure 3 ; appendix 1 pp 1011 )  . 
factors associated with benefit of immediate referral over delay included younger patient age ( < 70 years ) , high tumour progressiveness , high diagnostic - conversion rates , and higher proportion of cases diagnosed with stage iiii disease ( appendix 1 pp 1 , 4 , 10 , 12 )  . 
for those younger than 60 years , provided daily nosocomial infection rates are 25% or lower , even for short delays ( 2 months ) the delayrelated cancer - fatality rate largely exceeds investigationrelated fatality . 
 sars - cov - 2 = severe acute respiratory syndrome coronavirus 2 . 1041 articles when the nosocomial infection rate is higher than 1% , investigation - related fatality for several tumour types of good prognosis ( eg , prostate , testicular , and thyroid ) or very poor prognosis ( eg , pancreas , liver , oropharynx ) is predicted to be greater than delay - related cancer fatality for as long as 6 months ( appendix 1 pp 1011 )  . 
bladder and kidney cancers exemplify tumour types for which prompt referral is most impactful , since these groups have a high diagnostic - conversion rate , the tumours are moderately progressive , but are predomi nantly stage iiii at diagnosis . 
in the event of stable , low nosocomial infection rate ( 05% per referral ) , we determined life - years lost for delayed referrals ( appendix 1 p 12 )  . 
for those referred with symptoms of bladder cancer , for a 2 - month delay the average decrement per referred patient is 069 life - years for those aged 3039 years and 010 life - years for those aged 7079 years ; for those referred with symptoms of brain tumour , the average decrement is 003 life - years for those aged 3039 years and 001 for those aged 7079 years . in multivariate sensitivity analyses , outcomes from the model were mostly sensitive to changes in the estimated per - day delay hr . 
varying the delay hr by 2 sds ( eg , 16% ) in the scenario of a 2% nosocomial infection rate , the total lives lost annually for the 2 - week - wait population attributable to a 2 - month delay ranged from 2412 to 3378 , and attributable life - years lost ranged from 44 192 to 62 055 ( appendix 1 p 13 )  . 
using a proportionately higher per - day delay hr for tumours of high pro gres sive ness ( delay hr = 00105 vs default delay hr = 00056 ) increased the impact of a 2 - month delay to 3772 lives lost and 72 053 life - years lost . 
varying the rate of nosocomial infection , the community infection rate , and the cancer mortality multiplier had a small effect on the impact of delay on survival . discussion for most solid cancers , 10 - year survival is generally considered to equate to cure , reflecting the proportion of stage iiii tumours for which their surgery ( or radical radiotherapy ) has enabled the restoration to normal or near - normal life expectancy . 
our estimates suggest that , for many cancers , delays to treatment of 26 months will lead to a substantial proportion of patients with earlystage tumours progressing from having curable to incurable disease . 
however , this varies widely between tumour types , reflecting variation in the proportion of patients diagnosed through the 2 - week - wait pathway , the proportion diagnosed with stage iiii tumours , the age profile of patients diagnosed with those cancers , and the diagnostic - conversion rate , which inevitably means that the overall impact of delays in referral via the 2 - week - wait pathway is far from uniform between cancers . during the lockdown in the uk in marchjune , 2020 , substantial temporal and geographical variation has been seen in rates of patient deferment in accessing urgent referral for cancer symptoms , with estimates as high as 84% ( lawler m , unpublished ) .2 , 3 substantial additional morta lity from diagnostic delay on top of the presentational delay accrued during patient deferment is possible , especially if additional diagnostic capacity for catching up with the backlog is delayed . 
the additional capacity must include not only expanded technical provision for endoscopy , imaging , interventional radiology , and nuclear medicine , but also increased staffing for specialist assessment and pathology . 
innovative solutions will be required to deliver this extra capacity in a timely fashion , which might include procurement of private sector provision , expanded roles for health - care professionals such as endo scopy nurses , and pathway adaptationeg , use of faecal im muno chemical testing ( fit ) for triage of colorectal cancer referrals . investment in expansion of capacity for nhs diagnostics and treatment is a priority if cancer services are to become more resilient to future extrinsic disruption , which could include additional waves of covid - 19 . 
furthermore , pre - emptive public education is required to discourage patients from deferring presentation of cancer symptoms along with modification of pathways to and through primary care . diagnostic delays will affect patient groups differently . 
conversely , for older groups ( 70 years ) , perreferral risk of death from nosocomial infection is much higher and might exceed the average decrement of a moderate delay , in particular for more indolent cancer types ( eg , prostate cancer ) or cancers with a poor overall prognosis ( eg , upper gastrointestinal tract cancers )  . 
even in the absence of concerns about nosocomial infection , if there are pressures on diagnostic capacity , prioritisation and deprioritisation of patients according to tumour referral group and age warrants consideration as a strategy to mitigate the population - level cost of diagnostic delays in terms of lives and life - years lost . whether or not deaths due to sars - cov - 2 infection , both direct and indirect ( eg , compromise in collateral health - care delivery ) will be outweighed by the positive impacts on mortality ( eg , reduced air pollution , fewer road - traffic accidents , and handwashing ) as a result of the covid - 19 and lockdown period is a matter of debate . 
 although our analyses examine cancer - specific survival only , the estimations of life - years gained would be altered by any sizeable shifts in life expectancy . here we used data for england , but cancer survival is similar across most economically developed countries , so we believe our estimates of the impact of delay for each tumour type are broadly applicable . 
overall , in areas where cancer incidence , population structure , and 1042 vol 21 august 2020 articles background rates of population mortality are broadly similar to those in england , our model would provide insights relevant to other health systems , although pathways to diagnosis for different cancers , eligibility criteria , and proportions of different cancers ascertained differ between countries . 
issues of capacity and delays in diagnosis are of global interest as part of moving towards bench marked metrics ( eg , international cancer benchmarking partnership ) .3 , 23 our analysis focused only on invasive disease in common adult tumour types . 
 additional analyses will be required to assess the impact of delays for those having non - curative treatments . as with all modelling , the accuracy of our predictions is contingent on the validity of assumptions and paraidentified suitable meter estimates . 
although we observational data for delays in treatment for stages iiii for three tumour types , uniform application of these delay hrs across tumour types and over time will invariably oversimplify the complex , dynamic , tumour type - specific , age - specific , and stage - specific nature of cancer pro gression . 
to enable systematic insights across tumour types , routine capture of delays in referral pathways should be incorporated into all national cancer data collections . our analyses at the level of referral are subject to the limitations of data collection for diagnostic - conversion rates , which were only available at the level of tumourreferral group , precluding analyses specific to age stratum or tumour type - specific symptomatology . 
further more , our analysis does not capture the impact of delay on survival when a 2 - week - wait referral resulted in diagnosis of a different cancer outside of the index tumour - referral group ( appendix 1 pp 45 )  . the current model presents a what - if prediction , in which we have included what we believe to be plausible estimates of delay applied in a simplistic non - naturalistic manner . 
the severity of local covid - 19 patterns , method - specific diagnostic capacity , and organisation of cancer services will all have an effect , as will local variation in pathway innovations in both diagnostics ( fit triage , colonography ) and treatment ( a priori use of radiotherapy and hormonal treatments )  . 
 initiatives such as data - can , the uk health data research hub for cancer , are assembling accurate realworld data quantifying in detail true delays and patient volumes and distributions ; these data could be applied to our models to refine our predictions . 
over the coming months , we will also be able to quantify whether the postlockdown surge in presentations directly mirrors the in standard 2 - week - wait deficit during lockdown presentations , or whether a proportion of these patients ( ie , do not need medical genuinely self - resolve attention ) .24 the availability of models such as those we have used will also enable more agile prospective resource planning in the face of future instances of systematic disruption of cancer services , which could include future major waves of covid - 19 , other pandemics , or economic contractions . although the linear elements vary for the different routes to diagnosis ( urgent , routine , emergency , and screen ing ) , at each step convergence exists in the resources used for diagnostics and treatment . 
for example , patients referred for suspected lung cancer typically receive a ct scan , but only a subset of patients have an endobronchial ultrasound or bronchoscopy ; nevertheless , subsequent pet - ct for staging might be the narrowest of bottlenecks in the lung pathway . 
to optimise recovery , integrated time - course health system analyses across different routes to diagnosis will be required , accounting for all the linear steps up to and including surgical and adjuvant treatment and considering local variation in bottlenecks to capacity.6 the impact of covid - 19 - related disruption on cancer care is likely to be an ongoing issue until a vaccine or effective treatment is identified . 
unlike acute pathologies , such as stroke and myocardial infarction , the true excess mortality due to covid - 19 - related disruption to cancer pathways will not be fully evident for 10 years or longer . contributors as , ct , and rh designed the model . 
mej , jb , ml , em , ct , rh , as , gl , er , dcm , and mw provided epidemiological expertise in the parameterisation of the model and relevant literature . 
cs reports grants from pfizer and boehringer ingelheim ; grants and personal fees from bristol myers squibb , astrazeneca , ono pharmaceutical , and roche - ventana ; personal fees from novartis , msd , illumina , celgene , glaxosmithkline , genentech , medicxi , and sarah canon research institute ; personal fees and stock options from grail ; stock options from epic biosciences and apogen biotech ; and personal fees and being a co - founder of achilles therapeutics during the conduct of the study . 
cs has patents issued for an immune checkpoint intervention in cancer ( pct / ep2016 / 071471 ) , for a method for treating cancer based on identification of clonal neo - antigens ( pct / ep2016 / 059401 ) , for methods for lung cancer detection for more on data - can see data - can - health - data - researchhub - cancer / vol 21 august 2020 1043 articles ( pct / us2017 / 028013 ) , for a method of detecting tumour recurrence ( pct / gb2017 / 053289 ) , for a method for treating cancer ( pct / ep2016 / 059401 ) , for a method of treating cancer by targeting insertion / deletion mutations ( pct / gb2018 / 051893 ) , for a method of identifying insertion / deletion mutation targets ( pct / gb2018 / 051892 ) , for a method for determining whether an hla allele is lost in a tumour ( pct / gb2018 / 052004 ) , for a method for identifying responders to cancer treatment ( pct / gb2018 / 051912 ) , and for a method of predicting survival rates for cancer patients ( pct / gb2020 / 050221 )  . 
jl reports grants and personal fees from achilles therapeutics , bristol - myers squibb , msd , nektar , novartis , pfizer , roche , and immunocore ; personal fees from astrazeneca , boston biomedical , eisai , eusa pharma , glaxosmithkline , ipsen , imugene , incyte , ionctura , kymab , merck sorono , pierre fabre , secarna , vitaccess , and covance ; and grants from aveo and pharmacyclics outside of the submitted work . 
gl is supported by a cancer research uk advanced clinician scientist fellowship award ( c18081 / a18180 ) and is associate director of the multi - institutional cantest collaborative funded by cancer research uk ( c8640 / a23385 )  . 
this work was supported by the francis crick institute that receives its core funding from cancer research uk ( fc001169 ) , the uk medical research council ( fc001169 ) , and the wellcome trust ( fc001169 )  . correction to lancet oncol 2020 ; 21 : 101718 correction to lancet oncol 2020 ; 21 : 93546 correction to lancet oncol 2020 ; 21 : 112526 iarc monographs vol 127 group . 
lancet oncol 2020 ; 21 : 101718in this news piece , the web links in the margin for the preamble to the iarc monographs and for the iarc declarations of interest were incorrect and have been amended . 
 lancet oncol 2020 ; 21 : 112526in this comment , the fourth paragraph should read one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
because overdiagnosis appears to increase with age , it is possible that overdiagnosis occurred in both groups after the age of 50 years , but could not be detected because of the design of the trial . 
 this correction has been made as of sept 1 , 2020 , and the printed version is correct . vol 21 september 2020 e418 corrections editorial see comment page 578 for the letter from the royal colleges see rcplondon.ac.uk / press - releases / royal - colleges - join - forcesaustralian - counterparts - callstandard - packs for the lancets series on tobacco control see thelancet.com / themed / tobaccocontrol uk government panders to tobacco industry and lacks social conscience one of the most important roles of any government is to protect its citizens . 
however , on may 8 , 2013 , the uk government condemned 150 000 children per year to a lifetime of addiction , poor health , and for many , premature death . 
in the days running up to the annual state opening of parliament , speculation had been made about the contents of the queens speech , in which the government detailed legislative measures it wishes to pass through parliament over the next 12 months . 
 last year , the former uk health secretary andrew lansley declared smoking should no longer be an acceptable part of normal life , smoking was the largest avoidable cause of early mortality , and government was committed to act against the habit . 
 indeed , anne milton , a former uk health minister , is also on record as saying just last year that , we cannot ignore the fact that young people are recruited into smoking by colourful , eye - catching , cigarette displays . 
the roy castle lung cancer foundation remarked on may 8 , 2013 , that , packaging of tobacco products remains the last form of tobacco promotion legislated in the uk and is produced to attract [ consumers with ] colourful and targeted eyecatching designs . 
it is also absurd that the governments own systematic review backing the introduction of standardised packaging , public health minister anna soubrys public support for plain packaging , and opinion polls showing 62% of adults in england favour the use of standardised packaging , have all been conveniently forgotten . it is also curious that senior department of health o cials are reported to have held meetings earlier this year with imperial tobacco , british american tobacco , philip morris international , and japan tobacco international . 
why the uk government felt the need to entertain representatives from these companies is hard to comprehend given none would likely say anything that wasnt biased and self - serving . 
equally , recent election successes by the right - winged uk independence party , which aligns itself with smokers , leads to suspicions that the conservative partythe dominant force in the current coalition governmentdoes not want to be seen as overtly anti - smoking in the run - up to the 2015 general election because of the possible loss of potential votes . 
 australia , by contrast , have stayed resolute on the issue and have seen o the cynical arguments put forward by the tobacco industry , and those of the pro - tobacco lobbying of lynton crosbys company , crosby textor , to become the rst country to implement legislation restricting tobacco products to plain packagingan initiative quite - rightly referred to as brave and groundbreaking in a letter published on may 3 , 2013 , in the uk newspaper , the independent , and written by the presidents of uk royal college of physicians , the uk royal college of paediatrics and child health , and the royal australasian college of physicians . 
these three colleges all make a strong plea in their letter for jeremy hunt to pursue similar legislation as soon as possible and condemn the uk government for delaying its plans in this regard . 
interestingly , in the rst 6 months of packaging legislation in australia , none of the calamitous predictions made by the tobacco industry about the negative e ects on the economy , loss of jobs , and increased illicit trade , have come to pass . the uk has a strong record on implementation of tobacco - control policies , and is ranked as one of the leaders among european countries ; however , conservative party interests within the current government undermine progress by pandering to the tobacco lobby and by letting self - interests weaken health policy . 
ironic , too , that a government so obsessed with austerity does not see the cost bene t to the national health service of eliminating the scourge of tobacco usage from the health of a nation . 
 the lancet oncology vol 14 june 2013 published online august 3 , 2017 s1470 - 2045 ( 17 ) 30589 - 2 see articles page 1159 selective internal radiotherapy in advanced colorectal cancer : only for right - sided tumours ? colorectal cancer is a biologically unique tumour entity ; in 3040% of patients , metastases are confined exclusively to the liver , lung , or both , with or without minor additional lymph node involvement . 
different from all other tumour types , r0 - resection of these lesions is not always followed by systemic relapse in other regions , therefore this local approach isdespite systemic spread of the diseaseleads to a potentially curative resection in up to 61% of patients.1 , 2 therefore , locoregional treatment of metastases is of key importance . ( transarterial chemoembolisation if surgery alone is not appropriate , other locoregional modalities can be given , 3 such as hepatic arterial infusion of floxuridine , mitomycin , and oxaliplatin ; addition of starch microspheres or application of drug - coated glass beads ( eg , irinotecan beads ) for prolonged arterial drug chemoexposure ; embol ization ; tace ) ; ablation - techniques ( eg , radiofrequency , ultrasound , laser - ablation , heat - ablation , or cryoablation , radio surgery , and brachytherapy [ yttrium - 90 resin microspheres ; selective internal radiotherapy ; sirt ] )  . 
 however , randomised trials testing the individual value of any one treatment are rare ; only radiofrequency ablation with or without surgical resection plus chemotherapy has been prospectively proven effective for superior overall survival versus chemotherapy alone ( phase 3 clocc trial4 )  . 
 beyond this , sirt also showed clinically relevant efficacy on liver metastases in three small randomised in patients refractory to standard systemic trials chemotherapy ; therefore , a broad first - line therapy was justified . 
in the lancet oncology , harpreet wasan and colleagues5 report the results of a combined analysis of three trials of first - line folfox ( leucovorin , fluorouracil , and oxaliplatin ) chemotherapy with or without sirt . 
eligibility criteria used in the three trials were more or less comparable , including patients with unresectable , but limited , liver metastases , with or without lung metastases , and with or without lymph node metastases.6 as expected , the local effect of sirt is clear , with an improved proportion of patients achieving an overall response and liver - only progression . 
however , this locoregional effect did not translate into improved overall progression - free survival or overall survival , even in those patients with metastases restricted to the liver investigation ( one third of the patients )  . 
 why does this proven effective locoregional approach not alter the overall course of disease , even in liver - only disease ? several potential contributing factors that caused imbalance between the groups might have been involved , including different eligibility criteria in each of the three trials , different oxaliplatin dose between treatment groups ( 29% less in the folfox plus sirt group in cycles 13 than in the folfox alone group ) , lower dose of bevacizumab starting 23 months later in the folfox plus sirt group , fewer patients who had bevacizumab in the folfox plus sirt group compared with the folfox alone group ( 197 [ 36% ] vs 256 [ 47% ] ) , less salvage treatment in the folfox plus sirt group , and heterogeneity of the sirt dose between patients , centres , and treatment times . 
more relevant factors might be the fact 47 ( 8% ) of 554 patients randomly assigned to sirt did not receive sirt , that 41 ( 7% ) patients only had unilobar application , and 18 ( 3% ) patients crossed over from folfox alone to folfox plus sirt . 
however , even if those patients are eliminated from the analysis , the overall outcome would not change substantially . another relevant factor might be the short overall survival of patients in all three trials , which was shorter than that of other trials with comparable patient populations but that included treatment with one or two targeted drugs ( bevacizumab and egfr inhibitors ) .7 in the foxfire trials , egfr inhibitors were not used and vegf inhibitors were used in only one third of patients . 
this difference is mainly due to the enrolment and treatment era of the largest trial included in the analysis , sirflox ( 200613 ) and also the fact that patients were treated in countries without routine access to the targeted drugs . 
however , if systemic treatment is weak as in this case , shouldnt sirt have a bigger effect on overall survival ? this is obviously not the case , because , beyond the local treatment only , complete metastases resection after optimal and highly active chemotherapy can improve the long term outcome.4 1138 vol 18 september 2017 comment furthermore , although the local sirt approach improved frequency of resection , it only marginally increased the depth of response , the most important prerequisite for complete secondary resection . 
therefore , the frequency of secondary resection of liver ( and lung ) metastases was not sufficiently increased to improve survival . however , in an important subgroup analysis , 8 sirt was shown to significantly improve overall survival ( p = 0007 ) and progression - free survival ( p = 0053 ) in one third of patients with right - sided primary tumours , known to be much less sensitive to all types of systemic treatment versus left sided tumours , but had no effect in patients with left - sided primary tumours.sirt , which is not affected by chemoresistance in the same way , appears to overcome the intrinsic chemoresistance of liver metastases of right - sided primary tumours . 
this is an important message from wasan and colleagues study , the hr for overall survival in patients with right - sided tumours was 067 ( 048092 ) versus nonsignificant for left - sided tumours , which could have an impact on further clinical research , to improve the poor outcome of patients who have right - sided tumours . 
first - line selective internal radiotherapy plus chemotherapy versus chemotherapy alone in patients with liver metastases from colorectal cancer ( foxfire , sirflox , and foxfire - global ) : a combined analysis of three multicentre , randomised , phase 3 trials . 
protocol for combined analysis of foxfire , sirflox , and foxfire - global randomized phase iii trials of chemotherapy + / selective internal radiation therapy as first - line treatment for patients with metastatic colorectal cancer . 
phosphorylated trifluridine concentration and tumour growth inhibition are increased with the combination of tas - 102 and bevacizumab compared with either drug alone.4 the available clinical data5 suggest that the real benefit of tas - 102 monotherapy is small , therefore strategies to extend this benefit are urgently needed . 
 authors planned to enrol 25 patients , with at least 21 patients needed to have 80% power to reject the null hypothesis of 25% of patients free of progression at 16 weeks by central review . 
this design highlights two points of strength of this study : first , in this setting , 25% progression - free survival after four cycles is clinically relevant ; and second , independent review of response , which is uncommon in phase 2 studies , grants reliability to the results . 
the original hypothesis required at least nine ( 43% ) of the 21 patients included in the primary efficacy analysis to be free of progression at 16 weeksindeed , exactly nine patients achieved such a result . 
from a methodological perspective , this result shifts the attention to the level of the study , published online july 28 , 2017 s1470 - 2045 ( 17 ) 30574 - 0 see articles page 1172 vol 18 september 2017 1139 comment editorial trips , an international agreement on trade related aspects of intellectual property rights for more on australias stance on tobacco and plain packaging see news lancet oncol 2011 ; 12 : 427 for more on the marketing of anticancer campaigns in developing countries see editorial lancet 2011 ; 378 : 200 for more on the australian bill see parlinfo / download / legislation / bills / r4613_ rst / toc_ pdf / 11136b01 . pdf ; letype = application%2fpdf cigarettes and plain packaging : the battle lines are drawn on july 6 , 2011 , australia became the rst country to send a bill to their parliament on plain packaging for cigarettes . 
the legislation aims to reduce the number of current and new smokers by increasing the e ectiveness of the health warnings and also by reducing the appeal of the product . 
 the legislation has been referred to the trips council and the technical barriers to trade committee in the world trade organisation ( wto ) in an intellectual property rights battle , but rather than being headed - up by the tobacco companies , this move is spearheaded by low - income and middle - income countries . momentum from antismoking advocates to tackle the tobacco epidemic is gathering pace , and it needs to . 
 however , at a trips council meeting on june 7 , 2011 , the dominican republic , with support or sympathy from honduras , nicaragua , ukraine , the phillipines , zambia , mexico , cuba , and ecuador , said it had serious and grave concerns about the australian draft law in that it violated trademark law and would drive down the costs of cigarettes thereby increasing consumption and paving the way for counterfeiting . 
by contrast , new zealand , uruguay , and norway all supported the proposed law , and india said that studies have shown that plain packaging is an e ective antismoking strategy . 
whether the law is a violation of trademark law remains a contentious issue , because the brand name will remain , albeit in a standard typeface and size , with the packets covered in large health warnings . 
legal supporters told the lancet oncology that they were con dent the proposed law was fully compliant with wto obligations and hoped the case would provide an endorsement under international law of the importance of the who framework convention on tobacco control . 
 that the dominican republic , and others , should align themselves with the tobacco industrys stance in what is clearly a corporate e ort to save industry pro ts might seem strange , but the tobacco industry is thought to be important economically for many of these countries in terms of tax revenue and jobs . 
intriguingly , in an echo of thoughts put to wto by the dominican republic , the industry has also suggested that plain packaging will lead to an increase in the australian counterfeit market . 
but this is a separate issue to helping smokers quit or preventing new smokers taking up the habit , and should not deter the australian government from making every e ort to break the addictive cycle that smokers endure . 
 other defensive strategies by the tobacco industry include advertising campaigns to win over the australian public with spoof sketches of popular television programmes and the labelling of australia as a nanny state . 
phillip morris asia has also made a peremptory strike by ling notice of a legal claim from the australian government citing a violation of a previous investment treaty between hong kong and australia , an odd strategy given any losses are currently unknown . 
furthermore , contrary to this claim , the tobacco industry has suggested there is no evidence to support the e ectiveness of plain packaging as a strategy to reduce smoking ; experts believe plain packets can break the a liation smokers have with a particular brand helping them to quit and can also prevent teenagers from becoming smokers . 
 the australian tobacco market is comparatively small , representing only a$998 billion in 2009 , but much e ort is being expended to stop this law because it will set a precedent with canada , the uk , and new zealand all predicted to follow australias lead . 
 the lancet oncology vol 12 august 2011 editorial see review page e234 cancer immunotherapy : enthusiasm and reality aligning at last in this issue of the lancet oncology , a review by eliza hawkes and colleagues provides a timely overview of pd - 1 inhibition in lymphoma . 
moreover , since the approval of ipilimumab for use in treatment of metastatic melanoma in 2011 , there has been increased interest , and success , in use of immunotherapies for the treatment of cancer . 
ironically , after several decades without any truly viable treatment options , melanoma has become a proving ground for immunotherapy , revolutionising the standard of care for these patients and paving the way for immunotherapies in other advanced cancers . 
but , we must take care not to allow our enthusiasm for these new treatments to outpace the data . ipilimumab , which targets the ctla - 4 antigen , was the rst immune - modulating antibody to show activity and be approved for cancer treatment rst in metastatic melanoma , and more recently in non - smallcell lung cancer . 
nivolumab and pembrolizumab , which inhibit the interaction between pd - 1 and its ligand , have also been approved for metastatic melanoma , and have activity in bladder cancer , non - small - cell lung cancer , and renal - cell cancer . 
these immunotherapies act by removing a block or checkpoint on t - cell activation , by contrast with earlier drugs like interleukin 2 , which simply stimulated the immune systeother immuneinvestigated , are modulating including antichemokine receptor antibodies , such as mogamulizumab ; therapeutic cancer vaccines , including dendritic cell - based vaccines ; and oncolytic viruses . therapies being in many immunotherapy trials , durable responses and extended long - term survival are seen only in a subset of patients , highlighting the importance of identi cation of distinguishing clinical and molecular characteristics . 
this will not only provide clues about what factors might predict response , but also presents an opportunity to develop immunological or other methods to promote response in refractory patients . 
 recently , the recist guidelines have been amended to include immune - related progression criteria ; however , the adoption of these guidelines is uneven , and the relationship between progression events based on these criteria and overall survival remains unclear . 
in view of the complexity in this area , validated endpoints are needed urgently so that the de nition of tumour response is a reliable surrogate of harder oncological outcomes , and that treatment successes are clear and genuine . another way to in a broad array of patients improve the e ectiveness of immunotherapies to investigate the e ect of combining modalities : what is the e ect of using immunotherapies with chemotherapy , targeted therapy , and even other immunotherapies ? there is some evidence , for example , that combining nivolumab and ipilimumab can result in greater responses in a proportion of patients with metastatic melanoma . 
caution recommended , though , for treatment combinations ; additive and synergistic responses might be expected from our understanding of biological mechanisms , but the complexity of the immune response could result in unexpected serious adverse events . 
the fact that autoimmunity might be linked to a greater proportion of patients achieving a response in some studies is all the more reason to determine optimal dose and scheduling for these drugs before approval and widespread use . immunotherapies hold great promise for patients far beyond what weve already seen , but we must remain aware of the risks associated with modi cation of the immune system , and avoid misinterpretation or overinterpretation of surrogate endpoints when reporting trial results . 
improved understanding of the biology and role of smarcb1 has enabled identi cation of new targets for small molecule inhibitors to combine with chemotherapy backbones that we might establish from the current epssg and cog studies . introduction beckwith and colleagues1 rst described extracranial rhabdoid tumours as a distinct pathological entity in 1978 . 
 in 1981 , haas and colleagues2 recognised rhabdoid tumour of the kidney as a separate tumour rather than a variant of wilms , and introduced the term rhabdoid because of the tumour cells close histological resemblance to rhabdomyoblasts . 
results of subsequent studies have not con rmed a myogenic origin of the tumour cells , but the term is still used.2 in 1989 , weeks and colleagues3 published 111 cases of rhabdoid tumour of the kidneys from the national wilms tumour study ( nwts ) pathology centrethe tumour was then recognised as a distinct entity . 
within this family , rhabdoid tumours have speci c clinical and histological features , that from other smarcb1 - de cient distinguish tumours , and therefore make them of speci c interest . 
 they usually contain the classic rhabdoid cell with vesicular and eccentrically placed nuclei containing a single prominent nucleolus , and eosinophilic inclusions in the cytoplas them incidence and epidemiology 106 children younger than 15 years were diagnosed with extracranial rhabdoid tumours in the uk between 1993 and 2010.4 the age - standardised annual incidence was 06 per 1 million children . 
incidence was ve per million in the rst year of life and decreased to 06 per million at age 14 years , 01 at age 59 years , and 004 at age 1014 years . 
 14% of tumours arose in the head and neck , 13% in the liver , and 25% in a wide range of other sites in the trunk and arms , but no cases of rhabdoid tumour of the lower limbs were recorded . 
the proportions of rhabdoid tumours at di erent sites that were diagnosed in infants ( aged 012 months ) were 79% for liver , 65% for kidney , 47% for head and neck , and 54% for other sites . 
in children aged 114 years rhabdoid tumours accounted for less than 2% of each of these categories . population - based data for rhabdoid tumours in other countries or in adolescents and adults are scarce . 
the estimated age - standardised annual incidence of rhabdoid tumours of the kidney across 19 european countries in 198897 was 01 per million and the rate in the rst year of life was 10 per million.5 these rates are substantially lower than the uk data and probably indicate underrecording rather than geographical or temporal variations in incidence . 
in the usa surveillance epidemiology and end results ( seer ) registries between 1973 and 2006 , rhabdoid tumours accounted for 14% of all soft - tissue sarcomas diagnosed in the rst year of life6the same proportion as in the uk data . 
in the seer data , 65 ( 60% ) of 109 extrarenal , extracranial rhabdoid tumours were in people aged 20 years and older.7 malignant rhabdoid tumours in adults are less well described and hence the adult tumours included in the seer data might not be the classical rhabdoid tumours , but rather other tumours with a rhabdoid phenotype . 
inactivation of both copies of the smarcb1 gene leads to loss of protein expression in the nucleus , which can be detected by a smarcb1 immunohistochemistry assay , most frequently using the baf47 age at diagnosis 0 years 1 years 24 years 514 years kidney liver other total head and neck total data are from the national registry of childhood tumours.4 * other sites : arm / shoulder ( ve ) , thorax ( nine ) , abdomen / pelvis ( ve ) , trunk not otherwise speci ed ( four ) , omentum ( one ) , ovary ( one ) , bladder ( one )  . table : distribution of non - cns rhabdoid tumours in the uk , 19932010 vol 14 july 2013 e329 review antibody ( gure 1 ) .8 loss of expression of smarcb1 has also been shown in other tumoursepithelioid sarcomas , epithelioid malignant peripheral nerve sheath tumours , extraskeletal myxoid chondrosarcoma , renal medullary carcinoma , myoepithelial carcinomathat might have been included in the adult rhabdoid tumours in the seer programme.7 , 9 although this group of tumours seems varied , they all have loss of smarcb1 expression , often with rhabdoid cytomorphology , and sometimes other immunohistochemical and histological features . 
however , careful attention to the other immunohistochemical ndings and appropriate use of con rmatory cytogenetic studies will usually aid appropriate tumour classi cation.9 results have been reported from the only populationbased aetiological study of rhabdoid tumours.10 this record - based case - control study included 105 cases ascertained from the california cancer registry . 
results were presented as odds ratios ( or ) adjusted for birth year , maternal age , maternal ethnicity , and method of payment for antenatal care ( as a proxy for income level )  . 
the risk of extracranial rhabdoid tumour was signi cantly raised for children with low birthweight ( < 2500 g ; or 243 , 95% ci 109541 ) , gestation of less than 37 weeks ( 263 , 134517 ) , gestation of more than 42 weeks ( 366 , 154871 ) , or who were a member of a multiple birth ( 308 , 111855 )  . 
 translocations and deletions of the 22q11.2 cytoband were subsequently identi ed.11 positional cloning identi ed the biallelic inactivation of smarcb1 , located at 22q11.2 , as the main oncogenic event in rhabdoid tumour formation.12 rhabdoid tumour , liver smarcb1 - negative positive endothelial cells figure 1 : rhabdoid tumour of the liver ( a ) , and tumour cells showing loss of staining for smarcb1 ( b ) note the internal positive control in the form of the endothelial cells . the complete inactivation of this tumour suppressor large gene results from various combinations of interstitial chromosome 22q deletions encompassing the whole gene ( in about half of cases ) , whole exon duplication or deletion , oligo nucleotide insertions or deletions leading to frame shift and subsequent premature stop codons , and nonsense mutations ( in about 25% of cases ) .1315 homozygous deletions might be more frequent in extracranial tumours . 
in some cases , base pair substitutions in the 3 ( cid : 568 ) untranslated region have o ered putative explanations ; otherwise , intronic base pair variations leading to the illegitimate insertion of a pseudoexon in the transcript might also account for the full inactivation of smarcb1 in rare rhabdoid tumours . 
in all cases the genetic abnormalities lead to a total loss of protein expression , as shown by immunohisto chemistry.16 , 17 the mechanisms underlying the chromosome 22q11.2 rearrangements are mostly unknown ; however , the rst hit might be present at a germline level in 1530% of cases.14 , 18 , 19 on rare occasions germline mutations are inherited from asymptomatic parents , either because of gonadal mosaicism or incomplete penetrant mutations.20 in cases harbouring a germline deletion , precise mapping of the breakpoints has suggested that the low - copy repeats of the 22q11.2 region are particularly targeted by the chromosomal rearrangements , and so - called fragile sites might account for the location of the chromosomal breakages.19 , 21 the presence of germline alterations of smarcb1 predisposes these individuals to rhabdoid tumours in the brain and extracranial sites , often with several primary tumours.13 these children tend to be younger , often presenting in the rst year of life , and have a poor prognosis . 
whether this poor prognosis is because of their young age and therefore the inability to deliver all therapies , the germline mutation itself in all cells , or the presence of multiple primaries , is unclear.19 germline smarcb1 mutations have also been reported in familial schwannomatosis , but the development of schwannomas is probably by a mechanism distinct from that of rhabdoid tumours in which the smarcb1 protein is completely absent in tumour cells.22 finally , roughly 5% of rhabdoid tumours do not harbour any mutation in smarcb1 . 
a candidate gene approach in one family has allowed identi cation of truncating mutations of smarca4 as an alternative genetic event in the rare smarcb1 - non - de cient rhabdoid tumours.23 similarly to smarcb1 , the few smarca4 mutations reported are severe , leading to a complete loss of gene expression.24 although small , the exact proportion of rhabdoid tumours that are smarca4 - dependent needs further investigation . another striking feature of rhabdoid tumours is their remarkably stable genome . 
mckenna and colleagues25 e330 vol 14 july 2013 review showed that smarcb1 de ciency does not a ect the ability of rhabdoid cell lines to maintain genome integrity when exposed to dna - damaging agents . 
this experimental observation ts with the remarkably stable karyotypes and largely normal ( with the exception of chromosome 22 ) comparative genomic hybridisation or single nucleotide polymorphism array ndings in human rhabdoid tumours.15 , 26 high - throughput sequencing assays have con rmed this highly stable genome at the nucleotide sequence level.27 kieran and colleagues27 analysed a restricted panel of more than 900 genes ( 115 oncogenes ) and showed the absence of mutations in the usual oncogenes and tumour suppressor genes ( one single nras mutation in one of 25 tumours )  . 
apart from smarcb1 biallelic inactivation , rhabdoid tumours harbour very few , if any , genetic abnormalities , either recurrent or isolated , which suggests that smarcb1 gene mutation is su cient to promote oncogenic transformation , and acts as a suppressor gene.29 this information also suggests that potential synergistic events either result from variations in non - coding regions , or from epigenetic deregulation . 
 biological features linked to smarcb1 de ciency smarcb1 encodes the 47 kda smarcb1 ( also known as baf47 ) , which constitutes a ubiquitous and indispensable component of the atp - dependent chromatin remodelling complex swi / snf . 
smarca4 , the second gene inactivated in rhabdoid tumours , encodes another essential member of the swi / snf complexthe highly conserved brg1 protein , which harbours the atpase activity of the complex . 
rhabdoid tumour physiopathology therefore intimately depends on the roles of the swi / snf complex . the main function of the swi / snf complex is to control chromatin compaction , and hence gene expression . 
in particular , the rapid embryonic lethality of smarcb1 homozygous deletion in mice suggests a crucial role in early developmental processes.30 likewise , signi cant expression of stem cell - associated factors has been recorded in both pro ling of transcriptomes and immunohistochemical studies on rhabdoid tumours.31 , 32 to speculate that smarcb1 de ciency might severely a ect the normal di erentiation programme of immature embryonic progenitors , which could be the cells of origin of rhabdoid tumours , is tempting . 
the prodi erentiation function of smarcb1 has consistently been addressed in various rhabdoid cell lines , and seems to a ect di erent mesenchymal or neural lineages.33 , 34 several experimental studies show antagonistic roles between the swi / snf complex and the polycomb repressor complex ( prc2 ; gure 2 ) .35 , 36 in particular , wilson and colleagues36 showed that the regulation of the stem cell - associated programme , which is maintained by the repressive e ect of the ezh2 - dependent prc2 , is disrupted by smarcb1 reexpression.36 this process needs to be proven , but these results allow speculation about the basic pathophysiology for rhabdoid tumours : that the inactivation of smarcb1 in early progenitors or stem cells might enforce the the ezh2 / prc2 complex , repressive maintain pro genitors or embryonic stem cells in an undi erentiated state , and therefore a ect the expression of dozens of oncogenes and tumour suppressor genes . 
the results of this study emphasise the direct modi cations of histone methylation in smarcb1 - dependent oncogenesis , and the e ect of smarcb1 inactivation on cell cycle control . 
the fact that smarcb1 de ciency results in an increased g1 - to - s transition , and acts upstream of rb phosphorylation , is accepted.37 , 38 apart from defective expression of p16 , higher expression of cyclin d1 might also be necessary for this oncogenic process.39 various in - vitro assays examining the re - expression of smarcb1 in rhabdoid cell lines have pointed out several other biologically relevant genes and cellular processes ; these include myc , gli1 and the sonic hedgehog pathway , aurora kinase a , rhoa - gtpase related cytoskeleton dynamics , and bin1.4043 although swi / snf prc2 smarca4 smarcb1 polycomb antagonism chromatin decompaction maintenance of stem cell programme hdac recruitment , cell cycling ( cyclin d1 , p16 ) figure 2 : antagonistic e ects of smarcb1 within the swi / snf complex and prc2 complex the swi / snf complex is an antagonist of prc2 . 
after inactivation of the two smarcb1 alleles in rhabdoid cells , the methylation ( red circle , m ) of histone h3k27 is no longer inhibited ( red cross ) , and the repressive pattern of methylation - characterising stem cells is maintained . 
 vol 14 july 2013 e331 review weak , transcriptome pro lingmostly done on a small number of extracranial rhabdoid tumours31shows discrepant results about these lists of genes , but does o er some putative candidates for targeted therapies . 
 expression pro ling might also help to decipher the speci c diagnostic markers for cranial and extracranial tumours , and could give clues to enable rhabdoid tumours to be distinguished from other smarcb1de cient tumours . clinical features : renal versus extrarenal rhabdoid tumours the initial clinical reports of extracranial rhabdoid tumours were separated between renal and extrarenal sites , either in single or multiple case reports , often in pathological journals with a focus on distinguishing between the renal and extrarenal site.3 , 4446 wick and colleagues review47 summarised over 70 of the early case reports and suggested the concept that malignant rhabdoid tumours are a distinct pathological entity that occurs at renal and extrarenal sites , and in the brain where they are termed atypical teratoid or rhabdoid tumours . 
the later genetic characterisation of these tumours showed that most had a mutation of smarcb1 , and despite the variability of their clinical behaviour are the same type of tumour.13 at the renal site ( gure 3 ) , rhabdoid tumours tend to present earlier , usually in the rst year of life.48 in tomlinson and colleagues series49 of 142 renal rhabdoid tumours from the nwts , the median age at presentation was 106 months , with two cases presenting in the newborn period and a male preponderance ( male to female ratio of 137 : 1 )  . 
a further peculiarity of renal rhabdoid tumours is the association with hypercalcaemia , possibly driven by parathyroid hormone secretion.3 , 48 patients who present with renal rhabdoid tumours in the rst year of life tend to develop brain tumours that were initially judged to be separate pathological entities but are now recognised as atypical teratoid or rhabdoid tumours or primary rhabdoid tumours in the brain.49 these individuals are likely to have a germline mutation right left of smarcb1 and have a worse prognosis , probably linked to the early onset of their tumours.13 non - renal extracranial rhabdoid tumours occur in a range of locations including the liver , soft tissues , peripheral nerves , thymus , salivary glands , gastrointestinal tract , and genitourinary tract.47 children with extrarenal non - cranial rhabdoid tumours tend to be older and have a lower stage compared with those with renal non - cranial rhabdoid tumours , with most occurring in the musculoskeletal system.50 the age range at presentation is broader in extrarenal noncranial rhabdoid tumours , with some occurring in adults.50 survival rhabdoid tumours are often described as lethal , and little evidence of improving survival has been noted . 
in the 106 children diagnosed with extracranial rhabdoid tumour in the uk from 1993 to 2010 , 1 - year survival was only 31% . the 1996 international society of paediatric oncology intermediate nephroblastoma series48 found 22 cases of rhabdoid tumour of the kidney in 2392 renal tumours in children . 
only two patients in the series survived , and both had localised disease ( stage ii ) .48 in the nwts series49 of 142 renal rhabdoid tumours between 1969 and 2002 , overall survival at 4 years was 232% . 
an important factor for outcome was stage at diagnosis4 - year overall survival was 418% for stage iii tumours compared with 159% in those with stage iii , iv , or v disease . 
in a multivariate model applied only to children and adolescents with extracranial rhabdoid tumours , tumour stage is a signi cant predictor of survival ( p = 000014 )  . 
in tomlinson and colleagues series49 from nwts of renal rhabdoid tumours , survival increased with age4 - year overall survival was 88% for infants aged 05 months and 411% in children older than 2 years . 
this factor is con rmed by the seer programme , which includes all sitescranial , renal , and extrarenalwith the worst outcome for those younger than 24 months ( hazard ratio 179 ) or older than 18 years ( 183 ) .50 in the uk , infants ( aged 012 months ) with extracranial rhabdoid tumours had a lower 1 - year survival ( 170% ) than did older children ( aged > 1 year ) ( 540% )  . the nwts series , and the population - based series from the uk , and the seer programme all showed no improvement in outcome with time . 
in the seer data survival of patients diagnosed in the last 5 years of the study period ( 200105 ) was not greater than those diagnosed in 19862000 ( p = 078 ) .50 figure 3 : ct scan of the abdomen at diagnosis showing a left renal rhabdoid tumour e332 vol 14 july 2013 review for the childrens oncology group see childrensoncologygroup.org for the european paediatric soft tissue sarcoma group protocol see cineca.org / clinical - trials.htm small series focused either on extrarenal non - cranial rhabdoid tumours or on liver sites show even worse survival.51 , 52 in a series by bourdeaut and colleagues51 of extrarenal non - cranial rhabdoid tumours the median time to progression was 5 months ( range 044 ) , with only one patient remaining free of disease at 7 years . 
30 patients died , either of disease or treatment complications ; most ( 21 ) had metastases.52 in the uk , 1 - year survival of children by primary site was 14% for liver , 25% for kidney , 33% for head and neck , and 50% for other sites . 
 role of chemotherapy since extracranial rhabdoid tumours are rare , no standard therapeutic pathway exists and no randomised trials that examine the role of chemotherapy combinations or addition of new drugs have been done . 
two case reports of patients with metastatic renal rhabdoid tumours are often cited because of their successful outcome.53 , 54 the chemotherapy described in the reports forms the basis for the current childrens oncology group study of high - risk kidney tumours , which includes extracranial rhabdoid tumours , and the european paediatric soft tissue sarcoma group protocol for extracranial malignant rhabdoid tumours . 
in both protocols the philosophy of treatment indicates early surgical resection of the primary tumour if feasible , intensive multi - agent chemotherapy , derived from the case reports of waldron and colleagues53 and wagner and colleagues , 54 and local radiotherapy to all sites of disease . 
 in the case reported by waldron and colleagues , 53 courses of vincristine , doxorubicin , and cyclophosphamide chemotherapy were alternated with courses of ifosfamide and etoposide in an intensive 2 - weekly schedule in a child with a metastatic renal rhabdoid tumour . 
the patient was free of disease 5 years after diagnosis.53 similarly , wagner and colleagues54 described successful outcomes for two cases of metastatic renal rhabdoid tumours in which ifosfamide , cyclophosphamide , and etoposide alternating with vincristine , doxorubicin , and cyclophosphamide were used . 
the inclusion of doxorubicin in chemotherapy combinations is suggested to be important for survival in extracranial rhabdoid tumours.53 in tomlinson and colleagues series from nwts , 49 58% of the patients with renal rhabdoid tumours received doxorubicin , but survival did not di er between those who did and did not receive it.49 the absence of information about the type and use of chemotherapy from the seer programme in the sultan and colleagues series prevented further exploration of this factor in relation to outcome and prognosis.50 further possible evidence for the role of chemotherapy in particular ifosfamideis provided by a single historical institutional series from st jude childrens research hospital ( memphis , tn , usa ) .55 this series included only 13 children with extracranial rhabdoid tumours , but patients who responded to chemotherapy had regimens containing ifosfamide and hence the authors argue that it has a role in treatment of rhabdoid tumours . 
 although not deemed to be standard of care in extracranial rhabdoid tumours , high - dose chemotherapy with stem - cell rescue is very well reported in intracranial rhabdoid tumours either after relapse or as part of upfront therapy to delay use of irradiation for young children . 
the role of this treatment in extracranial rhabdoid tumours is not yet clear , although its use in two children with renal rhabdoid tumours has been reported.56 the series discussed so far show that recommendation of a standard treatment , or generation of a hypothesis to test additional chemotherapy regimens or drugs is di cult , especially because no phase 2 chemotherapy studies in rhabdoid tumours have been published . role of radiotherapy a small series of renal rhabdoid tumours from nwts57 suggests a role of radiotherapy in local control of extracranial rhabdoid tumours . 
this e ect of radiation was di cult to analyse because radiation tended to be given to those who were older and with higher stage disease ; furthermore , the older patients were more likely to receive a higher radiation dose . 
 only one infant received a dose greater than 25 gy ; therefore , after adjusting for age and stage , which are known prognostic factors , the relative risk of death after 25 gy was 085 ( p = 083 ) compared with no radiotherapy , and hence the apparent e ect of radiotherapy on survival was greatly reduced and no longer signi cant.49 in a multivariate model applied to the seer programme series , three factors were signi cant , including use of radiotherapy.50 in particular , if the multivariate model was only applied to patients younger than 18 years with extracranial rhabdoid tumours , use of radiotherapy remained a signi cant predictor of survival ( p = 00006 )  . 
 radiotherapy was only used in 35% of patients , but no signi cant di erence in its use at the di erent primary tumour sites was observed ( p = 090 ) .50 however , only 23% of children younger than 3 years received radiotherapy , which was a signi cantly lower proportion than that of the older patients46% of patients aged 3 years and older ( p = 00085 )  . 
the seer programme does not include data for the dose and volume of the radiotherapy.50 vol 14 july 2013 e333 review search strategy and selection criteria we searched pubmed using the terms rhabdoid tumour and atypical teratoid / rhabdoid tumour for references from jan 1 , 1980 to dec 31 , 2012 . 
we included relevant references from the articles identi ed by the search strategy . new targeted therapies the poor prognosis of patients with rhabdoid tumours who have chemotherapy suggests the use of targeted therapies for future treatment strategies . 
the combination of fenretinide and 4oh - tamoxifen induces apoptosis and cell cycle arrest in rhabdoid cell lines , and cell cycle arrest , connected to the strong repression of cyclin d1.58 to restore cell cycle control the pan - cdk inhibitor alvocidib has been used in xenografted mice and genetically engineered models.59 , 60 the e cient stabilisation and reduction of these tumours is promising and suggests a role for cdk inhibitors in clinical trials . 
the main rationale for these inhibitors is the e ect on the methylation or acetylation patterns of histones rhabdoid tumours , supported by the antagonistic e ects of prc2 and swi / snf complexes on histone modications . 
moreover , part of the swi / snf complex activity relies on regulation of hdac recruitment to the loci of their target genes ; therefore hdac inhibition might restore some of the regulation processes that are lost in a smarcb1 - de cient context.61 in that light , results of invitro studies have shown an interesting e ect of romidepsin on cell growth and apoptosis , 62 possibly related to induction of autophagy in rhabdoid tumour cell lines.63 sodium valproate , a common anticonvulsant used in children , has shown some hdac inhibition properties , and is therefore a possible candidate for therapy . 
the suberoylanalide achieved in clinical hydroxamic acid ( saha ) hdac inhibitor vorinostat has also shown promise in phase 1 trials in adults64 and children with refractory solid tumours ; 65 however , e cacy in rhabdoid tumours has not yet been proven . 
 despite the wide interest in tyrosine kinase inhibitors in early clinical trials , few studies have assessed their potential bene t in rhabdoid tumours , 66 , 67 probably because of the reduced expression in rhabdoid tumours . 
 however , the identi cation of the serinethreonine aurora kinase a as a downstream target of smarcb1 might suggest a role for aurora kinase inhibitors in rhabdoid tumours.41 as for saha , aurora kinase a might have a radiosensitiser role.68 a phase 1 trial of at9283 an inhibitor of aurora kinase ( nct00985868 ) could show a more realistic targeted therapy in rhabdoid tumours than those drugs suggested by murine models or cell lines , which might not reach paediatric clinical practice . where next ? extracranial rhabdoid tumours continue to be aggressive tumours with poor survival rates . 
further research is needed to gain understanding of rhabdoid tumour biology and the true cell of origin , and further knowledge of the role of smarcb1 in rhabdoid tumour development . 
this knowledge could identify more and better targets for therapy , and could also bene t other tumours from the smarcb1 - de cient family of tumours that might have the same targets . although no standard therapeutic pathway exists for rhabdoid tumours , the outcome from the current epssg and cog studies might at least establish a standard chemotherapy backbone to add small molecule inhibitors to what are known targets . 
we might need to take a leap of faith on the basis of cell line data and preclinical mouse models to put these agents straight into phase 3 clinical trials while not having data from phase 2 trials in rhabdoid tumours ; at least toxicity data will be available from phase 1 and 2 studies in more common paediatric tumours . 
the outcome of patients with rhabdoid tumours is unlikely to improve with current chemotherapy , which is already at maximum tolerance ; new targeted agents , to be given in combination , are needed . contributors cs wrote the incidence and epidemiology section , and prepared the table . 
all authors revised and approved the nal version . con icts of interest we declare that we have no con icts of interest . correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections covid - 19 and the us health insurance conundrum the devastating effects of the covid - 19 pandemic go far beyond public health ; with many industries on hold and unemployment increasing worldwide , the global economy is approaching the deepest recession in living memory . 
in the usa , where health insurance is largely provided by employers and more than 30 million people have filed for unemployment in the past 2 months , such a recession could cause an unprecedented surge in uninsured or underinsured people . 
indeed , an analysis published on may 4 , 2020 , has estimated that if unemployment in the usa reaches 20% , 2543 million people could lose their health insurance . 
for patients with cancer , for whom care is already expensive and long lasting , this could be a fatal blow . a recent report has estimated a delay in more than 22 million cancer screening tests and a 20% decrease in the number of interactions between patients and their oncologists in the usa during the covid - 19 pandemic . 
although this approach is understandable at this time , delayed screening and reduced treatment of early stage disease could result in the need for longer and more complex treatments for more advanced stage disease . 
coupled with the anguish and mental health effects associated with the uncertainty of treatment plans and outcomes , the demands on cancer care will inevitably increase in the future , driving individual health - care costs even higher , just at a time when patients ability to pay is hugely compromised . the options for us patients with no health insurance are scarce . 
some companies and charities are fighting to improve health insurance access , but a large increase in out - of - pocket health expenses could drive many patients into bankruptcy . 
although some might find respite in opting for medicaid or cobra ( a federal insurance after mechanism employment ends ) , not everyone is eligible for the former , and the latter can be unaffordable . that extends health although efforts to fight the covid - 19 pandemic are of paramount importance , in the usa , measures are urgently needed to avoid severe economic and social outcomes , and a tighter regulation on health - care prices , with a particular focus on private community oncology providers , is needed urgently . 
 the lancet oncology cancer detection : the quest for a single liquid biopsy for all in an editorial published in 2016 , the lancet oncology commented on the plans of the company , grail , to create a universal blood test that would allow screening of asymptomatic people for several types of cancer . 
 we raised several questions , including the sensitivity and specificity of these tests , what tumours could be detected , the ethical implications for positive cases , and how to best inform clinical practice and guide the patient . 
one clear lesson from the covid - 19 pandemic is that , even in high - income countries , mass testing can quickly exacerbate existing funding frail ties in health systems . 
the case for long - term savings made by detecting and treating cancers earlier must be made more clearly to governments and insurers alike . 4 years after grails ambition was announced , we now see encouraging scientific progress . 
the report highlighted that nearly 13 million cancer deaths are predicted for europe this year , and thatwith the exception of lung cancer in womenage - standardised death rates for most cancers decreased or remained unchanged since 2007 . 
about 127 million cancer cases and 76 million cancer deaths are estimated to have occurred in 2008 , with 56% of the cases and 64% of the deaths in developing countries . 
but can developing countries learn from the experiences of wealthier nations ? an increasing proportion of cancer deaths in developing countries are attributable to lifestyle changes such as smoking , diet , and physical inactivityin addition to the well documented disproportionately high burden of cancers related to infection . 
populations in countries with emerging economies will be increasingly exposed to the known risk factors associated with a uence , whereas those from poorer countries will continue to have high rates of infection , and limited or no access to treatment . 
 lack of basic infrastructure , rurality , con icts , and political instability mean many africans have no access to screening , early diagnosis , treatment , or palliative care . 
the incidence of cancer is increasing , but it remains a low public - health priority that has to compete for attention with other pressing and devastating health issues such as aids , malaria , and tuberculosis . in the a sustainable cancer control programme adapted to resource - constrained countries is crucial to tackle this predicted epidemic . 
without substantially increased prevention programmes , and a focus on early detection , the cancer burden in developing countries will make treatment una ordable long ter cancer management can be tailored and adapted to the resource level of the country or region . 
 but complacency would be unwarrantedafrica is likely at the early stages of a tobacco epidemic since smoking prevalence among boys is higher than in adults in some african countries . e orts to control cancer should be synergised with collaborative health initiatives , such as vaccination for liver and cervical cancers and public - health campaigns promoting physical activity and healthy diets . 
other initiatives include promoting cancer prevention information to over 3000 youths in lagos national stadium and o ering free hpv vaccines to 5000 girls in nigeria on world cancer day . 
aortic ( african organisation for research and training in africa ) has announced an initiative to improve cancer prevention , control , and care in africa through the integration and facilitation of evidencebased interventions . 
these examples are encouraging , but implementation will be the crucial factor . so can the battle against cancernotably absent from the millennium development goalsmove up the global health agenda ? this september , the un will hold a high - level summit to develop a global response to the growing threat of non - communicable diseases . 
 the lancet oncology vol 12 march 2011 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com anne szarewski cancer research uk centre for epidemiology , mathematics , and statistics , wolfson institute of preventive medicine , london ec1m 6bq , uk anne.szarewski@cancer.org.uk i have been sponsored by various pharmaceutical companies that manufacture contraceptive drugs to attend or lecture at many conferences , to give expert testimonies , or to act in a consultancy capacity . 
london : chapman and hall , 1991 . authors reply iarc thanks samuel shapiro and anne szarewski for their remarks regarding the policy watch article on combined oestrogenprogestagen contraceptives and menopausal treatment.1 samuel shapiro participated in the monograph meeting at our invitation , and the discussions beneted from his knowledge . 
according to iarc rules , samuel shapiro did not participate in the assessments because of the conict of interest he declared before the meeting . samuel shapiro believes that the working group was restricted from the assessment of evidence for the carcinogenicity of oestrogen - only or progestagen - only products . 
all iarc working groups are free to consider any published studies they regard as pertinent , and iarc made the previous monograph on single - ingredient products2 available to the working group . 
however , the effects of combined oestrogen and progestagen products are complex , and to extrapolate from studies of singleingredient products to predict the carcinogenicity of combined products would have been difcult . 
the working group noted , for example , that the increased risk of breast cancer is higher with combined menopausal treatment than with oestrogen - only menopausal treatment , and that the increased risk of endometrial cancer with combined treatment depends on the number of days per cycle progestagens are taken . epidemiological studies on the combined products themselves were more informative in assessing their carcinogenicity and consequently the working group decided to specically focus on these studies . 
carcinogenicity of combined oestrogenprogestagen contraceptives and menopausal treatment . lancet oncol 2005 ; 6 : 55253 . iarc monographs on the evaluation of carcinogenic risks to humans , volume 72 , hormonal contraception and post - menopausal hormonal therapy . 
lancet oncol 2005 ; 6 : 263the rst sentence of the second paragraph should read : in the rst study , researchers from mayo clinic ( rochester , mn , usa ) analysed survival of 842 patients who had radical prostatectomy for ct3 prostate cancer . vol 6 october 2005 correction to lancet oncol 2019 ; 20 : 155665 correction to lancet oncol 2019 ; 20 : e658 correction to lancet oncol 2020 ; 21 : e31729 bertelsen ca , neuenschwander au , jansen je , et al . 
lancet oncol 2019 ; 20 : 155665in this article , two patients ( one in the control group and one in the complete mesocolic excision group ) were incorrectly classified as not having recurrences , due to an error in data extraction . 
 the incorrect data have been updated in the summary findings , the results , figures 2a and 2c , table 3 , supplementary figures 2c and 2f in the appendix , and the discussion . 
complete mesocolic excision for colon cancer : is now the time for a change in practice ? lancet oncol 2019 ; 20 : 147476in this comment , the cumulative incidence of recurrence in each group has been amended , owing to these data being corrected in the linked article by bertelsen and colleagues . 
lancet oncol 2019 ; 20 : e658 in this correspondence , the absolute in risk of recurrence reduction has been amended , owing to this being corrected in the linked article by bertelsen and colleagues . 
this correction has been made to the online version as of aug 3 , 2020 . correction to lancet oncol 2020 ; 21 : e33036 cooney tm , cohen jk , guimaraes cv , et al . 
these corrections have been made to the online version as of aug 3 , 2020 . vol 21 august 2020 e372 corrections corrections correction to lancet oncol 2015 ; 16 : 733 correction to lancet oncol 2016 ; 17 : 1055 correction to lancet oncol 2016 ; 17 : 1163 , 1165 basset - seguin n , hauschild a , grob jj , et al . 
 this correction has been made to the online version as of july 26 , 2016 . published online june 24 , 2016 s1470 - 2045 ( 16 ) 30273 - x dearnaley d , syndikus i , mossop h , et al . 
 conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
 lancet oncol 2016 ; 17 : 104760 in gure 4b of this article , the curves for 57 gy grade 1 + and 60 gy grade 1 + were incorrect . 
these corrections have been made to the online version as of june 24 , 2016 , and the printed version is correct . van maaren mc , de munck l , de bock gh , et al . 
lancet oncol 2016 ; 17 : 115870in gures 2b and 3b , the label for the bottom row of number at risk should have read t2n1 , and in gure 3b , the label for the top row should have read t1n0 . 
we aimed to provide conclusive results for the clinical bene ts of hyperbaric oxygen in patients with chronic bowel dysfunction after radiotherapy for pelvic malignancies . methods hot2 was a double - blind , sham - controlled , phase 3 randomised study of patients ( 18 years ) with chronic gastrointestinal symptoms for 12 months or more after radiotherapy and which persisted despite at least 3 months of optimal medical therapy and no evidence of cancer recurrence . 
participants were strati ed by participating hyperbaric centre and randomly assigned ( 2 : 1 ) by a computer - generated list ( block size nine or 12 ) to receive treatment with hyperbaric oxygen therapy or shaparticipants in the active treatment group breathed 100% oxygen at 24 atmospheres of absolute pressure ( ata ) and the control group breathed 21% oxygen at 13 ata ; both treatment groups received 90 - min air pressure exposures once daily for 5 days per week for a total of 8 weeks ( total of 40 exposures )  . 
sta at the participating hyperbaric medicine facilities knew the allocated treatment , but patients , clinicians , nurse practitioners , and other health - care professionals associated with patients care were masked to treatment allocation . 
primary endpoints were changes in the bowel component of the modi ed in ammatory bowel disease questionnaire ( ibdq ) score and the ibdq rectal bleeding score 12 months after start of treatment relative to baseline . 
the primary outcome was analysed in a modi ed intention - to - treat population , excluding patients who did not provide ibdq scores within a predetermined time - frame . 
 the trial is registered with the isrctn registry , number isrctn86894066 . findings between aug 14 , 2009 , and oct 23 , 2012 , 84 participants were randomly assigned : 55 to hyperbaric oxygen and 29 to sham control . 
75 ( 89% ) participants received 40 pressure exposures , all participants returned the ibdq at baseline , 75 ( 89% ) participants returned the ibdq at 2 weeks post - treatment , and 79 ( 94% ) participants returned the ibdq at 12 months post - start of treatment . 
in an analysis of 46 participants in the active treatment group and 23 participants in the control group , we found no signi cant di erences in the change of ibdq bowel component score ( median change from baseline to 12 months of 4 ( iqr 3 to 11 ) in the treatment group vs 4 ( 6 to 9 ) in the sham group ; mann - whitney u score 067 , p = 050 )  . 
in an analysis of 29 participants in the active treatment group and 11 participants in the sham group with rectal bleeding at baseline , we also found no signi cant di erences in the change of ibdq rectal bleeding score ( median change from baseline to 12 months of 3 [ 1 to 3 ] in the treatment group vs 1 [ 1 to 2 ] in the sham group ; u score 169 , p = 0092 )  . 
common adverse events in both groups were eye refractive changes ( three [ 11% ] of 28 patients in the control group vs 16 [ 30% ] of 53 patients in the treatment group ) , increased fatigue ( three [ 11% ] vs two [ 4% ] ) , and ear pain ( six [ 21% ] vs 15 [ 28% ] )  . 
eight serious adverse events were reported in eight patients : two were reported in two patients in the control group ( tonsillitis requiring surgery [ grade 3 ] ; recurrent cancer of the vulva [ grade 4 ] ) and six serious adverse events were reported in six patients in the treatment group ( malignant spinal cord compression requiring surgery [ grade 3 ] ; malignant paraortic lymph node involvement requiring surgery [ grade 3 ] ; recurrence of vomiting and dehydration [ grade 3 ] ; diarrhoea and fever associated with campylobacter infection [ grade 3 ] ; recurrence of abdominal pain , bloating , diarrhoea , and urinary tract infection [ grade 3 ] ; aneurysm [ grade 4 ] ) , none of which were deemed treatment - related . interpretation we found no evidence that patients with radiation - induced chronic gastrointestinal symptoms , including those patients with rectal bleeding , bene t from hyperbaric oxygen therapy . 
open access article distributed under the terms of cc by . 224 vol 17 february 2016 articles see online for appendix research in context evidence before this study hyperbaric oxygen is widely used to treat chronic adverse e ects of curative radiotherapy in long - term survivors of pelvic malignancy , especially those with rectal bleeding . 
we searched pubmed from jan 1 , 1970 , to dec 31 , 2008 , with the terms clinical trials and hyperbaric oxygen and pelvic or pelvis or bowel and radiotherapy . 
the results of a single randomised , sham - controlled trial from 2008 ( hortis ) reported signi cant clinical bene ts for patients treated with hyperbaric oxygen 2 weeks post - treatment . 
a cochrane intervention review from 2012 con rmed the retrospective nature of much research and detected no other level 1 evidence on which to base an assessment of this treatment modality for patients with chronic radiation - induced bowel dysfunction . added value of this study the results of this double - blind , sham - controlled clinical trial fail to con rm earlier positive results of hyperbaric therapy for cancer survivors with chronic bowel dysfunction , including a subset of patients with rectal bleeding , after curative radiotherapy for pelvic malignancy , with a similarly sized minority of volunteers in each randomised group reporting some improvement in symptoms . 
this trial is only the second randomised study in this important patient population . implications of all the available evidence the contribution of hyperbaric oxygen to the management of a growing population of long - term cancer survivors with severe restrictions on daily activities and impaired quality of life as a consequence of bowel injuries after curative radiotherapy for pelvic malignancy remains unclear and requires more evidence from well designed clinical trials . 
additional exclusion criteria included medical history of cancer recurrence , rectal surgery , previous hyperbaric oxygen therapy ( except for illness ) , exposure to bleomycin , claustrophobia , epilepsy , uncontrolled asthma , bullous lung disease , some types of ear surgery , and inability to equalise the middle ear . 
individuals with a past history of prostate cancer had to have three serial measurements of serum prostate - speci c antigen within the normal concentration range ( less than 3 ng / ml for men aged 5059 years , 4 ng / ml for men aged 6069 years , 5 ng / ml for men 70 years or older )  . treatment of decompression patients with symptoms attributed to radiotherapy entered a minimum 3 - month period of optimum standard treatment , including antibiotic treatment for small bowel bacterial overgrowth , treatment of bile acid malabsorption , 7 lifestyle advice , or several of these interventions , and were supervised by a gastroenterologist . 
individuals were considered eligible for the study only if the 3 - month period of optimal standard treatment was unsuccessful . vol 17 february 2016 articles for the study report see clinical - study - report.pdf for the trial protocol see trial - protocol.pdf all patients provided written informed consent . 
the study was approved by the mhra ( 2008 - 002152 - 26 ) and the nres committee north east - york ( 08 / h0903 / 40 )  . 
the full case study report and trial protocol are available online . randomisation and masking eligible participants were randomly assigned ( 2 : 1 ) to receive hyperbaric oxygen treatment or sha randomisation was arranged by a telephone call from the treating hyperbaric medicine facility to the institute of cancer research clinical trials and statistics unit ( icr - ctsu )  . 
 to deliver the correct treatment , only engineers and technicians operating the hyperbaric chamber were informed of the allocated treatment by the trials o ce , and care was taken to ensure that patients , clinicians , nurse practitioners , and other health - care professionals associated with patients care remained masked to treatment allocation . 
the most important precaution was to disallow any non - trial patient sharing the chamber with a trial patient . for the ctcae protocols see protocoldevelopment / electronic_applications / ctc.htm procedures participants attended the participating hyperbaric oxygen medicine facility most convenient for them , where they panel : bowel function component of the modi ed in ammatory bowel disease questionnaire ( ibdq ) 11 question 1 : have you had your bowel open ? question 5 : have you had loose bowel movements ? question 9 : have you been troubled by pain in your bottom ? question 13 : have you had cramp in tummy or bottom ? question 17 : have you passed a large amount of gas ? question 20 : have you been troubled by bloating ? question 22 : have you had a problem with bleeding from your bottom ? question 24 : have you felt like you need to have your bowel open but nothing happens ? question 26 : have you been troubled by accidental soiling ? question 29 : have you felt disgusted about your bowel problems ? each question is linked to the following response options on a 7 - point graded scale : 1 = more than ever before ; 2 = extremely frequently ; 3 = very frequently ; 4 = moderate increase in frequency ; 5 = some increase in frequency ; 6 = slight increase in frequency ; 7 = normal / not at all . 
the possible range of summed results for the 10 questions is 1070 , where 10 represents the most severe , and 70 the least severe , levels of e ect , this metric represents a co - primary endpoint . 
 patients in the hyperbaric oxygen therapy group received 40 pressure exposures at 24 atmospheres of absolute pressure ( ata ; 243 kpa ) breathing 100% oxygen for 90 min ( including 5 - min air breaks at 30 - min intervals ) , whereas patients in the control group received 40 pressure exposures at 13 ata ( 131 kpa ) breathing 21% oxygen ( ie , air ) for 90 min with two simulated 5 - min air breaks . 
dose reductions were not permitted . participants were asked to complete the modi ed in ammatory bowel disease questionnaire ( ibdq ) 8 and the european organisation for research and treatment of cancer ( eortc ) c30 core quality of life questionnaire ( qlq - c30 ) and cr38 colorectal module ( qlq - cr38 ) 9 , 10 at baseline , 2 weeks after end of treatment , and again at 3 months , 6 months , 9 months , and 12 months after start of treatment . 
 on the basis of results from a previous study , 14 we considered a reduction in ibdq bowel component 226 vol 17 february 2016 articles score of 7 ( sd 10 ) from baseline to 12 months to be clinically relevant . 
during the recruitment phase of the trial ( february , 2012 ) , the independent data monitoring committee agreed that the signi cance level of 5% could be split to allow additional analyses in patients reporting rectal bleeding in the ibdq at baseline . 
we estimated that 75 evaluable patients would allow us to detect a di erence in ibdq bowel symptom score of 75 with 80% power at a two - sided signi cance level of 3% . 
the bowel component is made up of ten questions , and we used all ten items in the bowel component of the modi ed ibdq to analyse overall bowel function and analysed rectal bleeding using the single rectal bleeding question in the modi ed ibdq . 
 the di erence in change from baseline to 12 months between the two study groups was analysed using the mann - whitney u test due to the non - normality of the data . 
we did two exploratory subgroup analyses of the primary endpoints ; one analysis considered the group of patients who received radiotherapy 15 years before randomisation , and the other considered the group of patients whose trial treatment was delivered by hood ( or monochamber )  . 228 vol 17 february 2016 articles we used stata version 13 for all statistical analyses . 
the trial is registered with the isrctn registry , number isrctn86894066 . role of funding source the funder had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data and had nal responsibility for the decision to submit for publication . treatment ; results between aug 14 , 2009 , and oct 23 , 2012 , 241 patients were given a rigorous initial assessment followed by a 3 - month period of optimised medication . 
84 participants were considered eligible for trial entry and were randomly assigned to treatment with hyperbaric oxygen ( active treatment group ; n = 55 ) or with sham control ( control group ; n = 29 ; gure )  . 
two - thirds of participants had faecal frequency , incontinence , or both , symptoms that suggest injury to the colon as well as rectum , and a similar proportion reported rectal bleeding . 
75 ( 89% ) participants received all 40 planned pressure exposures , and nine ( 11% ) patients received 38 exposures or less ( one patient received 38 exposures , one patient received 31 exposures , one patient received 18 exposures , one patient received 11 exposures , one patient received four exposures , one patient received three patients received no two exposures , and exposures )  . 
of the patients in the modi ed intention - to - treat population who reported slight increase in frequency or worse rectal bleeding on ibdq at baseline , ten ( 67% ) of 15 patients in the control group and 26 ( 74% ) of 35 patients in the treatment group reported an improvement of at least 1 point in the ibdq rectal bleeding score at 12 months ( absolute di erence 76% [ 95% ci 203 to 355 ] ; p = 058 ; appendix p 2 )  . 
 * others were anal canal ( n = 1 ) and vulva ( n = 1 ) in the control group and retroperitoneum ( n = 1 ) , pelvis ( n = 1 ) , rectum ( n = 1 ) , and bladder ( n = 1 ) in the hyperbaric oxygen therapy group . table 3 : patient characteristics at pretrial eligibility assessments irrespective of time of return , showed that the di erence in change from baseline to 12 months between the two study groups was consistent with the modi ed intention - to - treat analysis ( u score 071 [ p = 048 ] for overall bowel function ; u score 206 [ p = 0040 ] for rectal bleeding )  . 
40 ( 47% ) of 84 patients scored grade 15 ( clinically signi cant ) rectal bleeding on the ibdq bowel function component , compared with 57 ( 68% ) patients reporting any rectal bleeding in their medical history ( panel )  . 
planned descriptive analysis of changes in ctcae grades at baseline , 2 weeks post - treatment , and at 12 months also did not show di erences between the treatment groups ( appendix p 4 )  . 
 exploratory subgroup analyses of patients who completed radiotherapy 15 years before entering the study did not show any di erence in ibdq scores between the two groups ( u score 059 [ p = 056 ] for overall bowel function ; u score 157 [ p = 012 ] for rectal bleeding )  . 
exploratory subgroup analysis in patients receiving treatment using a hood or monochamber showed no di erence in overall bowel function but did suggest a di erence in rectal bleeding ( u score 031 [ p = 076 ] for overall bowel function ; u score 29 [ p = 0004 ] for rectal bleeding )  . we analysed toxic e ects in the safety population , which included the 81 patients who received at least one treatment ( 53 in the hyperbaric oxygen therapy group and 28 in the sham control group )  . 
the most commonly reported adverse events were eye refractive change , including myopia ( three [ 11% ] of 28 patients in the control group vs 16 [ 30% ] of 53 patients in the treatment group ) , increased fatigue or tiredness ( three [ 11% ] vs two [ 4% ] ) , and ear pain or barotrauma ( six [ 21% ] vs 15 [ 28% ] )  . 
eight serious adverse events were reported in eight patients : two were reported in two patients in the control group ( tonsillitis requiring surgery [ grade 3 ] ; recurrent cancer of the vulva [ grade 4 ] ) and six serious adverse events were reported six patients in the treatment group ( malignant spinal cord compression requiring surgery [ grade3 ] ; malignant paraortic lymph node involvement requiring surgery [ grade 3 ] ; recurrence of vomiting and dehydration [ grade 3 ] ; diarrhoea and fever associated with campylobacter infection [ grade 3 ] ; recurrence of abdominal pain , bloating , diarrhoea , and urinary tract infection [ grade 3 ] ; aneurysm [ grade 4 ] )  . 
no treatmentrelated deaths were noted . and some clinical evidence discussion despite plausible pathophysiological mechanisms justifying an expectation of therapeutic e ect of hyperbaric oxygen therapy , the hot2 trial results detected no clinically relevant bene t of hyperbaric oxygen therapy in individuals with a wide range of chronic gastrointestinal dysfunction , including rectal bleeding , after curative radiotherapy for pelvic malignancy . 
histologically , progressive obliterative endarteritis is a classic feature and ischaemic atrophy is an important element of the pathophysiology , but direct radiation e ects on other tissue elements , including epithelia , also contribute to symptoms.18 the tissues rendered ischaemic by vascular atrophy do not share the steep oxygen gradients that stimulate angiogenesis in acute surgical wounds unless these gradients are arti cially introduced.19 in studies of animal and human skin , 20 , 21 hyperbaric oxygen therapy has been shown to restore virtually normal small vessel density and tension after transcutaneous oxygen high - dose radiotherapy , an e ect that peaked after 2030 treatments in human beings . 
the proposed therapeutic mechanisms include marrow stem - cell mobilisation and consequent vasculogenesis , although our results do not suggest that these processes , if activated by hyperbaric oxygen , were of therapeutic value.22 our trial results are inconsistent with a long history of striking anecdotes and reviews of non - randomised studies.2 , 2325 a cochrane intervention review3 identi ed two randomised trials testing hyperbaric oxygen in patients with chronic gastrointestinal symptoms after pelvic radiotherapy , but the analysis was restricted to the hortis trial4 because of a high risk of bias identi ed in the other study . 
the hortis trial randomly assigned 150 patients from mexico , turkey , south africa , and australia with a 3 - month or longer medical history of radiation proctitis to breathe air at 11 ata ( sham group ) or 100% oxygen at 20 ata ( active treatment group ) for 90 min for 30 sessions within 68 weeks , with an individual ten sessions depending on additional responses . 
the hortis investigators also reported a signi cant bene t of hyperbaric oxygen in patients with bowel bother , a group of symptoms that include faecal incontinence , faecal urgency , and pa the authors of the cochrane vol 17 february 2016 articles review interpreted these results as non - signi cant and sensitive to randomised patients excluded from primary analysis but concluded that hortis supported the continued use of hyperbaric oxygen for patients with radiation proctitis . it is unclear why the results of hot2 fail to reproduce the hortis4 ndings . 
patient selection was unusually rigorous , including assessment by a gastroenterologist specialised in radiation enteropathy and a 3 - month run - in period of optimised oral drug treatment to ensure that eligible patients had radiation - induced symptoms that could not be controlled by standard measures . 
the trial population is considered representative of patients with radiation enteropathy in terms of their symptoms , although patients with severe faecal incontinence or transfusion - dependent rectal bleeding are likely to be under - represented , the former being too restricted to leave their homes and the latter considered too seriously at risk to be considered by their primary physicians for entry into a trial with a sham treatment option . 
we assessed 20 characteristics relating to bowel dysfunction at baseline , and despite small imbalances in the proportion of patients with a medical history of rectal bleeding ( 23 [ 79% ] of 29 patients in the control group vs 34 [ 62% ] of 55 patients in the treatment group ) , this imbalance did not apply to baseline ibdq rectal bleeding scores analysed as the primary endpoint . 
in other respects , symptom duration in hot2 , at a median 37 years ( iqr 2468 ) postradiotherapy , is consistent with that of the hortis population , and hot2 patient characteristics are well balanced between randomised groups . in a literature review26 of ten retrospective studies published between 1960 and 2004 reporting favourable results of hyperbaric oxygen therapy for patients with radiation proctitis , patients had an average of 24 treatments each . 
compliance with treatment in hot2 was reasonably high , with 75 ( 88% ) of 84 patients eligible for inclusion in the intention - to - treat population , as required by the analysis plan . 
pre - trial investigations designed to exclude patients with residual malignant disease ensured that only three patients developed cancer recurrence while participating in the study . other relevant points of di erence between the hortis4 and hot2 trials include the immediate post - treatment timepoint for the primary analysis in hortis , compared with the primary analysis at 12 months post - treatment in hot2 . 
exploratory analyses of the 2 - week post - treatment in hot2 showed no di erence between e ects the primary endpoint randomised groups for any of the primary or secondary endpoints . 
unlike hot2 , in which we analysed a modi ed intention - to - treat population , the primary analysis in hortis excluded 30 of 150 randomised patients who did not complete the treatment protocol ( plus one patient lost to follow - up ) , although unplanned analyses of the outcomes of clinical assessments by intention - to - treat were also consistent with a bene cial e ect of hyperbaric oxygen in hortis . 
in other exploratory analyses of hot2 endpoints ( including subgroup analysis of patients completing radiotherapy 15 years before randomisation and subgroup analysis of patients receiving treatment by hood or hyperbaric chamber rather than mask ) , we could not identify variables that might explain di erences trials . 
 randomisation appears to have resulted in a reasonably even distribution of patient characteristics between the treatment and control groups in our study , to the extent that the total e ect of these covariates would not be expected to mask any e ect of hyperbaric oxygen . 
the very small number of patients with transfusion - dependent rectal bleeding in this study prevents us from commenting on the use of hyperbaric oxygen therapy for patients referred for this potentially life - threatening complication . reported outcomes between these two our trial was designed to have a power of 80% ; with 69 evaluable patients , we had a power of about 75% to detect a di erence of the magnitude expected in the rst of the primary endpoints . 
we did not detect a clinically or statistically signi cant clinical bene t of hyperbaric oxygen therapy for patients with chronic gastrointestinal dysfunction , including rectal bleeding , after pelvic radiotherapy . 
the ndings contrast with previous reports , highlighting an urgent need for more level 1 evidence to determine with con dence whether hyperbaric oxygen therapy can be recommended as a standard of care for this group of patients . contributors jy was the chief investigator of the trial , was involved in study design , was responsible for the clinical supervision of patients and performance of the study , and contributed to the preparation and writing of the report . 
 mg , grs , hja , beb , pb , of , lg , jh , mi , gl , sm , dm , celp , sp , and gs were were study investigators responsible for patient recruitment , clinical supervision , and treatment of patients , were involved in the acquisition , analysis , and interpretation of the data , and contributed to the writing of the report . 
lm was responsible for the acquisition and analysis of the data , and contributed to the writing of the report . declaration of interests we declare no competing interests . acknowledgments we thank the volunteers and site personnel participating in this study for their support and commitment . 
the national institute for health research biomedical research centre at the royal marsden and the icr received funding from the national health service . 232 vol 17 february 2016 articles corrections published online december 21 , 2016 s1470 - 2045 ( 16 ) 30686 - 6 correction to lancet oncol 2017 ; 18 : 205 , 206 , 208 , ( d ) low jg , berglund a , schell mj , scott et al . 
in gure 1 , the footnote should have read pie charts show dose assignments for patients in gard score groups : ( b ) high ( 8941100 percentile ) ; ( c ) middle ( 3041894 percentile ) ; and ( 0304 percentile )  . 
in the second paragraph of the results , the third sentence should have read however , although 1456 ( 58% ) of 2517 patients assigned to 45 gy were in the low gard group , 1023 ( 21% ) of 4877 patients in the middle gard group and 38 ( 4% ) of 887 patients in the high gard group were assigned to 45 gy ( gure 1 )  . 
the fth sentence in this paragraph should have read similarly , although most patients assigned to 70 gy were in the high gard group , 588 ( 11% ) of 4877 patients in the middle gard group were assigned to 70 gy ( gure 1 )  . 
in the fth paragraph of the discussion , the start of the eighth sentence should have read : finally , while we use the gene - expressionbased a backbone for our analyses , the calculation of gard could use other measures of radiosensitivity or be expanded to include other biological parameters including hypoxia , dna repair , proliferation , and the immune systethese corrections were made to the online version as of dec 21 , 2016 , and printed article is correct . radiosensitivity index vol 18 february 2017 e ects of zoledronic acid versus clodronic acid on skeletal morbidity in patients with newly diagnosed multiple myeloma ( mrc myeloma ix ) : secondary outcomes from a randomised controlled trial gareth j morgan * , j anthony child * , walter m gregory , alex j szubert , kim cocks , sue e bell , nuria navarro - coy , mark t drayson , roger g owen , sylvia feyler , a john ashcroft , fiona m ross , jennifer byrne , huw roddie , claudius rudin , gordon cook , graham h jackson , ping wu , faith e davies , on behalf of the national cancer research institute haematological oncology clinical studies group summary background bisphosphonates are the standard of care for reducing the risk of skeletal - related events in patients with bone lesions from multiple myeloma . 
here , we report the secondary outcomes relating to skeletal events . methods patients ( 18 years ) with newly diagnosed multiple myeloma were enrolled from 120 centres in the uk and received intensive or non - intensive antimyeloma treatment . 
a computer - generated randomisation sequence was used to allocate patients in a 1 : 1 ratio , through an automated telephone service to intravenous zoledronic acid ( 4 mg every 2128 days ) or oral clodronic acid ( 1600 mg / day ) , and the drugs were continued at least until disease progression . 
at a median follow - up of 37 years ( iqr 2947 ) , patients in the zoledronic acid group had a lower incidence of skeletal - related events than did those in the clodronic acid group ( 265 [ 27% ] vs 346 [ 35% ] , respectively ; hazard ratio 074 , 95% ci 062087 ; p = 00004 )  . 
zoledronic acid was also associated with a lower risk of any skeletal - related event in the subsets of patients with ( 233 [ 35% ] of 668 vs 292 [ 43% ] of 682 with clodronic acid ; 077 , 065092 ; p = 00038 ) and without bone lesions at baseline ( 29 [ 10% ] of 302 vs 48 [ 17% ] of 276 with clodronic acid ; 053 , 033084 ; p = 00068 )  . 
fewer patients in the zoledronic acid group had vertebral fractures than did those in the clodronic acid group ( 50 [ 5% ] in the zoledronic acid group vs 88 [ 9% ] in the clodronic acid group ; p = 00008 ) , other fractures ( 45 [ 5% ] vs 66 [ 7% ] ; p = 004 ) , and new osteolytic lesions ( 46 [ 5% ] vs 95 [ 10% ] ; p < 00001 )  . 
 interpretation the results of this study support the early use of zoledronic acid rather than clodronic acid in patients with newly diagnosed multiple myeloma for the prevention of skeletal - related events , irrespective of bone disease status at baseline . funding medical research council ( london , uk ) , novartis , schering health care , chugai , pharmion , celgene , and ortho biotech . introduction multiple myeloma , which is diagnosed in more than 100 000 people every year , 1 is characterised by the growth of malignant plasma cells in the bone marrow.2 , 3 interactions between myeloma cells and bone marrow stromal cells are fundamental to the excessive activation and proliferation of osteoclasts , causing localised bone destruction.4 myeloma cells also secrete factors that inhibit osteoblasts , blocking the repair of osteolytic damage . 
results from this trial showed that patients given zoledronic acid had signi cantly improved progression - free survival ( hazard ratio [ hr ] 088 , 95% ci 080098 ; p = 00179 ) and a reduced risk of death ( 084 , 074096 ; p = 00118 ) versus clodronic acid , with overall survival prolonged by 55 months.12 importantly , improved overall survival with zoledronic acid remained signi cant after adjustment for the e ect of skeletal - related events that ( 085 , 074097 ; p = 0018 ) , suggesting zoledronic acid has direct antimyeloma activity . 
in this analysis , we investigated in detail the e ects of clodronic acid and zoledronic acid on skeletal - related events in patients with newly diagnosed multiple myeloma . methods trial design the mrc myeloma ix trial was a multicentre ( n = 120 ) , randomised , open - label , two - by - two factorial trial , with 1970 patients with newly diagnosed multiple myeloma randomly assigned to bisphosphonates 1960 analysed ( intention - to - treat population ) 979 clodrononic and cvad , ctd , mp , or ctda 981 zoledronic acid and cvad , ctd , mp , or ctda 917 started clodronic acid 11 started zoledronic acid 15 started pamidronic acid 0 started etidronic acid 31 bisphosphonate not initiated 5 bisphosphonate not conrmed 887 started zoledronic acid 25 started clodronic acid 14 started pamidronic acid 1 started etidronic acid 45 bisphosphonate not initiated 9 bisphosphonate not conrmed 820 randomly assigned to thalidomide maintenance or watchful waiting 2 excluded 1 no consent 1 withdrew consent 408 thalidomide 410 no thalidomide 195 clodronic acid 213 zoledronic acid 195 clodronic acid 215 zoledronic acid figure 1 : trial pro le the complete trial protocol is provided in morgan and colleagues.12 cvad = cyclophosphamide , vincristine , doxorubicin , and dexamethasone . 
full details have already been reported.12 patients adult patients ( 18 years ) with newly diagnosed and histologically con rmed symptomatic multiple myeloma were eligible for inclusion in the trial . 
 exclusion criteria included previous or concurrent active tumours , acute renal failure ( de ned as serum creatinine concentration > 500 mol / l that was unresponsive to 72 h of rehydration , urine output < 400 ml / day , or requirement for dialysis ) , and previous treatment for multiple myeloma ( except local radiotherapy for bone pain or spinal cord compression , bisphosphonates for hypercalcaemia of malignancy , or low - dose corticosteroids )  . the trial was approved by the north west multi - centre research ethics committee and local review committees at all participating centres . 
all patients provided written informed consent . randomisation and masking the methods of randomisation and masking for this study have been previously described in detail.12 brie y , a computer - generated randomisation sequence was used to allocate patients in a 1 : 1 ratio by use of an automated telephone service to zoledronic acid or clodronic acid . 
 no investigators , sta , or patients were masked to treatment allocation . treatment patients were allocated to two main treatment pathways ( intensive and non - intensive ) , as previously described in detail.12 in each pathway , patients were randomly assigned to oral clodronic acid ( 1600 mg / day ) or intravenous zoledronic acid ( 4 mg , 15 min infusion every 34 weeks with induction chemotherapy and every 4 weeks thereafter )  . 
dose adjustment for patients with impaired renal function at baseline and delays in administration of the dose in patients with increases in serum creatinine concentration during the study were implemented for zoledronic acid , per the prescribing information . 
data for skeletal - related events , de ned as vertebral fractures , other fractures , spinal cord compression , need for radiation or surgery for bone lesions , and new osteolytic lesions , were analysed until disease progression . 
 these included bone fracture , radiation to bone , surgery for bone lesions and spinal cord compression , and height loss ( as an indicator for further imaging follow - up )  . 
additional prespeci ed analyses of hypercalcaemia of malignancy and exploratory analyses of skeletal - related events , excluding the development of new osteolytic lesions , were undertaken . statistical analysis the primary endpoints of progression - free survival , overall survival , and overall response rate , and the secondary endpoint of safety have been reported previously.12 here , we report the secondary endpoint of skeletal - related events . 
in the intensive pathway , we aimed to recruit 1080 patients ( 540 per group ) to test the hypothesis that cyclophosphamide , thalidomide , and dexamethasone ( ctd ) was not inferior to cyclo phosphamide , vincristine , doxorubicin , and dexamethasone ( cvad ) , with a hazard ratio of 12 and 80% power at a 5% signi cance level . 
in the non - intensive pathway , we aimed to recruit 850 patients ( 425 per group ) to assess whether attenuated ctd ( ctda ) was superior to standard chemotherapy with melphalan plus prednisolone , with 80% power at a 5% signi cance level . 
we calculated that the sample size for the intensive and non - intensive pathways combined had su cient power ( > 80% ) to detect a reduction of 10% in the proportion of patients with skeletal - related events for zoledronic acid compared with clodronic acid . analyses were based on the treatment that patients with histologically con rmed multiple myeloma who provided written informed consent were randomly assigned to receive ( intention - to - treat population )  . 
data , in part , from morgan and colleagues.12 table 1 : baseline demographics and disease characteristics of the intention - to - treat population clodronic acid zoledronic acid hr 074 ( 95% ci 062087 ) ; p = 00004 * number at risk clodronic acid zoledronic acid time from randomisation ( months ) hr 053 ( 95% ci 033084 ) ; log - rank p = 00068 hr 077 ( 95% ci 065092 ) ; log - rank p = 00038 time from randomisation ( months ) time from randomisation ( months ) number at risk clodronic acid zoledronic acid figure 2 : time to rst skeletal - related event overall ( a ) , in patients with bone lesions at baseline ( b ) , and in patients without bone lesions at baseline ( c ) hr = hazard ratio . 
to reduce the potential e ects of related skeletal - related events ( eg , a fracture requiring surgery ) in multiple - event analyses , only one skeletal - related event per 21 days was included ( eg , skeletal - related events of possibly linked causality were counted only once , and judged to be one skeletal - related event )  . 
post - hoc analyses that included all skeletal - related events irrespective of whether they were the rst or subsequent skeletal - related events within 21 days ( not reported ) were done and provided results consistent with those in which the linked events were counted as one skeletal - related event . 
all hypothesis tests were the 5% signi cance level , without adjustment for multiplicity . this trial is registered , number isrctn68454111 . two - sided and undertaken at role of the funding source no funding organisation was involved in study design , data collection , data analysis or interpretation , writing , or decision about publication submission . 
all authors had full access to trial data ; gjm , jac , and ghj had nal responsibility for the decision to submit for publication . results 1970 patients were enrolled between may 14 , 2003 , and nov 20 , 2007 , and 1960 were the intention - to - treat population ( gure 1 )  . 
baseline demographics and disease characteristics of patients were well balanced between the zoledronic acid and clodronic acid groups ( table 1 ) .12 1898 ( 97% ) of 1960 patients were white , 1401 ( 71% ) had myeloma bone disease at baseline , 562 ( 29% ) had a history of vertebral fractures , 231 ( 12% ) had previous non - vertebral fractures , 1010 ( 52% ) had been diagnosed with osteolytic lesions , and 258 ( 13% ) had previous radiotherapy ( table 1 )  . 
median follow - up was 37 years ( iqr 2847 ) for patients in the zoledronic acid group and 38 years ( 2947 ) for those in the clodronic acid group ; 582 ( 30% ) patients had been given zoledronic acid or clodronic acid for at least 2 years ( 290 [ 30% ] of 981 in the zoledronic acid group and 292 [ 30% ] of 979 in the clodronic acid group )  . 
in the overall patient population , fewer patients assigned to zoledronic acid had a skeletal - related event than did those assigned to clodronic acid ( 265 [ 27% ] of 981 vs 346 [ 35% ] of 979 , respectively ) , with zoledronic acid signi cantly reducing the risk of skeletal - related events versus clodronic acid 746 vol 12 august 2011 articles skeletal - related events incidence ( 95% ci ) overall di erence ( 95% ci ) between clodronic acid and zoledronic acid * p value for preceding 12 months clodronic acid ( n = 979 ) zoledronic acid ( n = 981 ) clodronic acid ( n = 979 ) zoledronic acid ( n = 981 ) 12 months 24 months 36 months 48 months 60 months 451 ( 46% ) 333 ( 34% ) 043 ( 038048 ) 033 ( 028037 ) 011 ( 004018 ) 93 ( 9% ) 28 ( 3% ) 13 ( 1% ) 2 ( < 1% ) 54 ( 6% ) 16 ( 2% ) 4 ( < 1% ) 2 ( < 1% ) 060 ( 053066 ) 042 ( 036048 ) 018 ( 009026 ) 069 ( 061078 ) 047 ( 040053 ) 023 ( 012033 ) 080 ( 068091 ) 049 ( 042056 ) 030 ( 017044 ) 083 ( 070095 ) 051 ( 043058 ) 032 ( 018046 ) 00002 00024 00089 00510 05359 data are number ( % ) , unless otherwise indicated . 
unadjusted p value for the comparison of incidence of skeletal - related events in zoledronic acid group versus clodronic acid group per 12 months ( eg , 24 - month p value is for incidence between 12 months and 24 months )  . table 2 : cumulative annual incidence of rst and subsequent skeletal - related events for the intention - to - treat population after randomisation clodronic acid zoledronic acid ( gure 2a )  . 
the total number of skeletal - related events reported was also lower in the zoledronic acid group than in the clodronic acid group ( 419 vs 597 , respectively )  . 
the proportion of patients with at least one skeletal - related event was consistently lower in the zoledronic acid group versus the clodronic acid group at each timepoint ( p < 00001 overall ; table 2 )  . 
the di erence in incidences of skeletal - related events for zoledronic acid versus clodronic acid was signi cant for each of the rst 3 years separately , but the total number of skeletalrelated events was low at 48 months and 60 months , and reduced the statistical power for the respective 12 - month comparisons ( table 2 )  . 
similar distributions of skeletalrelated events were noted for patients treated with zoledronic acid and clodronic acid in the intensive ( zoledronic acid , 155 [ 28% ] of 555 ; clodronic acid , 202 [ 36% ] of 556 ; log - rank p = 0003 ) and non - intensive pathways ( zoledronic acid , 110 [ 26% ] of 426 ; clodronic acid , 144 [ 34% ] of 423 ; log - rank p = 0008 )  . 
the mean skeletal morbidity rate was lower with zoledronic acid versus clodronic acid in the intensive and non - intensive pathways ( 04 skeletal - related events per patient per year vs 08 per patient per year , respectively )  . 
however , patients who did not have myeloma bone disease at baseline had lower rates of bone pain ( 248 [ 43% ] of 578 vs 1136 [ 84% ] of 1350 ) , and higher rates of anaemia ( 330 [ 57% ] vs 523 [ 39% ] ) , renal failure ( 96 [ 17% ] vs 171 [ 13% ] ) , and infection ( 74 [ 13% ] vs 90 [ 7% ] ) than did patients with bone disease at baseline . in an exploratory analysis that excluded new osteolytic lesions from the de nition of skeletal - related event , the outcome was similar to the analysis that included new osteolytic lesions , and the reduction in risk of skeletalrelated events with zoledronic acid was still signi cant ( hr 076 , 95% ci 064089 ; log - rank p = 00011 )  . 
 further exploratory analysis by patients risk of skeletalrelated events , as identi ed in another assessment of the myeloma ix patients , 16 showed a reduced risk of p < 00001 p = 0070 any skeletal - related event except hypercalcaemia of malignancy p = 00031 p < 00001 p = 037 p = 00008 p = 0040 p = 029 radiotherapy lesion surgery to bone vertebral fracture other fracture spinal cord compresssion p = 00069 p = 022 p < 00001 p = 023 p = 0035 any skeletal - related event except hypercalcaemia of malignancy radiotherapy lesion radiotherapy lesion any skeletal - related event except hypercalcaemia of malignancy figure 3 : proportion of patients with an on - study skeletal - related event overall ( a ) , with bone lesions at baseline ( b ) , and without bone lesions at baseline ( c ) skeletal - related events with zoledronic acid versus clodronic acid in the high - risk and low - risk populations ( data not shown )  . 
analysis by cytogenetic markers ( poor prognosis de ned by use of uorescence in - situ hybridisation [ fish ] as adverse igh translocations , gain of 1q , and loss of 17p ) showed that the bene t vol 12 august 2011 articles ctda vs melphalan + prednisolone ( non - intensive pathway ) 075 ( 060094 ) zoledronic acid vs clodronic acid ctd vs cvad ( intensive pathway ) serum calcium concentration ( high vs low ) serum creatinine concentration ( high vs low ) haemoglobin concentration ( high vs low ) platelets ( high vs low ) skeletal - related events at baseline * no vs yes missing vs yes centre hazard ratio ( 95% ci ) p value 072 ( 062084 ) 091 ( 076110 ) 131 ( 111155 ) 093 ( 077112 ) 108 ( 092126 ) 119 ( 093153 ) 035 ( 028044 ) 083 ( 046152 ) < 00001 03399 00141 00012 04362 03489 01623 < 00001 05532 < 00001 ctd = cyclophosphamide , thalidomide , and dexamethasone . 
overall p value , but not hazard ratio , reported for 120 centres . table 3 : multivariate model for risk of skeletal - related events associated with zoledronic acid in terms of skeletalrelated events was attributable to the non - poor prognosis subset , 16 wherein the bene ts of zoledronic acid were especially meaningful ( log - rank p = 00012 ; data not the poor - prognosis subset , disease shown )  . 
 progression was fairly rapid , and very few patients were assessable for the time to rst skeletal - related - event endpoint at later timepoints ( 48 months and 60 months ; data not shown )  . 
 in an exploratory analysis , patients with osteolytic lesions at baseline showed a non - signi cantly longer progression - free survival than did those with no osteolytic lesions ( 20 months , 95% ci 1821 , vs 18 months , 1719 , hr 090 , 082100 ; p = 00535 )  . 
however , patients with bone disease at baseline had a higher incidence of skeletal - related events than did those without bone disease at baseline ( 525 [ 39% ] of 1350 vs 77 [ 13% ] of 578 , respectively ; p < 00001 )  . 
moreover , zoledronic acid , compared with clodronic acid , was associated with a signi cantly reduced risk of any skeletal - related event in patients with ( 233 [ 35% ] of 668 vs 292 [ 43% ] of 682 ; gure 2b ) and without bone disease at baseline ( 29 [ 10% ] of 302 vs 48 [ 17% ] of 276 ; gure 2c )  . 
zoledronic acid was associated with a reduced incidence of each type of skeletal - related event versus clodronic acid in the overall population ( gure 3a ) , and signi cant reductions were noted for any skeletal - related event ( 265 [ 27% ] of 981 vs 346 [ 35% ] of 979 for clodronic acid ; p < 00001 ) , new osteolytic lesions ( 46 [ 5% ] vs 95 [ 10% ] for clodronic acid ; p < 00001 ) , vertebral fractures ( 50 [ 5% ] vs 88 [ 9% ] for clodronic acid ; p = 00008 ) , and other fractures ( 45 [ 5% ] vs 66 [ 7% ] for clodronic acid ; p = 004 ) , but not radiotherapy ( 179 [ 18% ] vs 211 [ 22% ] for clodronic acid ; p = 007 ) , surgery to the bone ( 49 [ 5% ] vs 58 [ 6% ] for clodronic acid ; p = 037 ) , and spinal - cord compression ( 13 [ 1% ] vs 19 [ 2% ] for clodronic acid ; p = 029 )  . 
 zoledronic acid was associated with a signi cantly reduced incidence of any skeletal - related event in patients with ( gure 3b ) and without bone disease at baseline ( gure 3c )  . in a prespeci ed multivariate model of all on - study skeletal - related events , the reduction in such events with zoledronic acid versus clodronic acid remained signi cant ( table 3 )  . 
baseline serum calcium concentration , baseline skeletal - related event , melphalan plus prednisolone versus ctda ( in the non - intensive pathway ) , and treatment centre also showed signi cant correlations with risk of skeletalrelated events ( table 3 )  . 
overall , exclusion of new osteolytic lesions from the skeletal - related - events composite endpoint did not a ect model outcomes ( data not shown )  . results of further exploratory analyses showed that the proportion of patients with a skeletal - related event was signi cantly lower with zoledronic acid versus clodronic acid when the rst 12 months ( log - rank p = 00012 ) or 24 months ( log - rank p = 00102 ) were excluded from the analyses ( data not shown )  . 
furthermore , signi cantly fewer patients in the zoledronic acid group than in the clodronic acid group had at least one skeletal - related event after randomisation to maintenance thalidomide or no maintenance ( log - rank p = 00005 ; data not shown )  . 
 the incidences of most adverse events were similar in zoledronic acid and clodronic acid groups and have been previously reported.12 overall , the rates of acute renal failure were low and similar for patients in the zoledronic acid and clodronic acid groups ( 57 [ 6% ] of 983 [ two patients for whom con rmation of consent was not received were included in the safety population ] vs 60 [ 6% ] of 979 , respectively ; p = 078 )  . 
during the study , 47 ( 5% ) of 979 patients in the clodronic acid group and 43 ( 4% ) of 981 in the zoledronic acid group died of renal failure ( p = 067 ) , and 123 ( 13% ) patients in the clodronic acid group and 92 ( 9% ) in the zoledronic acid group died of multiple myeloma or treatmentrelated infections ( p = 0025 )  . 
28 ( 3% ) patients in the clodronic acid group and 28 ( 3% ) in the zoledronic acid group had hypercalcaemia , which was reported as a serious adverse event in six ( < 1% ) of 979 patients in the clodronic acid group and six ( < 1% ) of 983 in the zoledronic acid group . 
as previously reported , 12 con rmed osteonecrosis of the jaw was rare , but the rate was higher in the zoledronic acid group than in the clodronic acid group ( 35 [ 4% ] vs three [ < 1% ] , respectively ; p < 00001 )  . 
gastrointestinal serious adverse events were not signi cantly di erent with clodronic acid versus zoledronic acid ( 30 [ 3% ] vs 24 [ 2% ] , respectively ; p = 041 )  . 
 treatment - emergent serious adverse events that were suspected to be related to bisphosphonate use arose in 41 ( 45 events ) of 983 patients in the zoledronic acid group versus 33 ( 34 events ) of 979 patients in the clodronic acid group , and represented a subset of the overall treatmentemergent serious adverse events that were suspected to be 748 vol 12 august 2011 articles tenderness related to any of the study drugs as previously reported.12 in patients given zoledronic acid , treatment - emergent serious adverse events were musculoskeletal , connective tissue , and bone disorders ( n = 16 ) ; renal and urinary disorders ( n = 8 ) ; haematological disorders ( n = 5 ) ; gastrointestinal [ n = 1 ] , nausea and vomiting , disorders ( dehydration epigastric [ n = 1 ] , and nausea , vomiting , constipation , dehydration [ n = 1 ] ) ; endocrine , metabolism , or nutrition disorders ( n = 3 ) ; infections ( n = 3 ) ; cardiovascular disorders ( n = 2 ) ; skin and subcutaneous disorders ( n = 2 ) ; uid or electrolyte disturbance ( n = 1 ) ; general disorder or administration - site condition ( n = 1 ) ; and nervous system disorder ( n = 1 )  . 
in patients in the clodronic acid group , treatment - emergent events were gastrointestinal disorders ( diarrhoea [ n = 2 ] , abdominal pain and bloating [ n = 1 ] , nausea or vomiting [ n = 6 ] , oesophagitis [ n = 1 ] , haematemesis [ n = 1 ] , and gastrointestinal disturbance [ n = 1 ] ) ; renal and urinary disorders ( n = 9 ) ; infections ( n = 5 ) ; haematological disorders ( n = 2 ) ; skin and subcutaneous disorders ( n = 2 ) ; cardiovascular disorder ( n = 1 ) ; general disorder or administration - site condition ( n = 1 ) ; hepatic disorder ( n = 1 ) ; and reproductive system or breast disorder ( n = 1 )  . 
 adverse serious in progression - free discussion the results of the current analysis of the mrc myeloma ix trial show that zoledronic acid was associated with a signi cantly reduced risk of skeletal - related events versus clodronic acid in patients with newly diagnosed multiple myeloma irrespective of their bone disease status at baseline . 
additionally , zoledronic acid was associated with a reduced incidence of skeletal - related events in the intensive and non - intensive pathways , suggesting that all patients undergoing initial treatment for multiple myeloma could bene t from early use of zoledronic acid . 
 previous analyses showed that zoledronic acid was associated with a signi cant reduction in the risk of death ( hr 084 , 95% ci 074096 ; p = 00118 ) and a signi cant improvement ( 088 , 080098 ; p = 00179 ) , providing signi cant clinical bene ts and not just reduction in rates of skeletal - related events ( panel ) .12 although clinical guidelines recommend bisphosphonates for patients with documented bone lesions , 4 , 7 , 8 , 17 all patients ( ie , with or without bone disease at baseline ) could bene t when bisphosphonates are begun early in the course of multiple myeloma . 
moreover , the reductions in skeletal - related events with zoledronic acid versus clodronic acid noted throughout the course of the trial support the continued use of zoledronic acid in patients with multiple myeloma at least until disease progression , when patients went o study in this trial and data for skeletal - related events were no longer collected . 
however , the optimum duration of zoledronic acid is not known , and some patients might bene t from continuing zoledronic acid , possibly at a reduced dose , during disease remission . 
additional clinical trials are needed to further re ne these aspects of treatment . survival panel : research in context systematic review in addition to the experience obtained from previous mrc myeloma trials of clodronic acid , a review of the reports of clinical trials of a wide variety of combination chemotherapy regimens and bisphosphonates was undertaken and used to develop the 22 factorial trial design for the myeloma ix trial . 
at the time that the myeloma ix trial was initiated , most patients with symptomatic multiple myeloma in the uk were treated long - term with bisphosphonates ; however , there was no consensus for the optimum timing and duration of treatment with bisphosphonates , or the e cacy for prevention of skeletal - related events of all the available bisphosphonates and their potential to a ect disease outcomes and survival variables in patients with multiple myeloma . 
in the myeloma ix trial , we assessed the possible enhanced e ects on disease - related bone changes and survival of a third - generation bisphosphonate ( zoledronic acid ) in comparison with a standard older - generation oral agent ( clodronic acid )  . interpretation the results of the myeloma ix trial showed signi cant bene ts with zoledronic acid versus clodronic acid on progression - free survival , overall survival , and several variables for skeletal - related events , and , to our knowledge , for the rst time established the superiority of one bisphosphonate over another in patients with multiple myeloma . 
moreover , exploratory analyses have shown signi cant bene ts with treatment before the onset of bone lesions and also with long - term treatment ( eg , during maintenance therapy or long - term follow - up )  . 
the data from myeloma ix provide compelling evidence that zoledronic acid should be considered an essential component of therapeutic regimens for patients starting treatment for newly diagnosed multiple myeloma irrespective of whether bone lesions are already present , and support the continuation of zoledronic acid at least until disease progression . 
however , the results of this study do not provide insight into whether the frequency of dosing with zoledronic acid can be reduced after initial treatment , such as in patients with long - term remission of their disease . in patients with multiple myeloma , renal adverse events and osteonecrosis of the jaw are causes for concern and should be monitored and managed appropriately . 
indeed , because monitoring the concentrations of creatinine in vol 12 august 2011 articles ( ie , and reactions strategies that were colleagues13 ) the serum was less frequent for the clodronic acid group than for the zoledronic acid group ( ie , every 3 months vs monthly , respectively ) , any observation bias would be in favour of clodronic acid . 
this bias suggests that the renal adverse events reported in the myeloma ix trial were most likely a result of the disease , antimyeloma treatments , non - myeloma - related drugs , or other comorbidities rather than toxicity associated with bisphosphonates , validating the renal safety protocols for zoledronic acid . 
 recommendations for prevention and management of osteonecrosis of the jaw were implemented in myeloma ix from june , 2006 , onwards , 13 but further reductions in the risk of osteonecrosis of the jaw might be possible with prevention reported subsequently . 
the results of a study in postmenopausal women ( n = 7765 ) given intravenous zoledronic acid ( 5 mg per year ) for osteoporosis showed that the acutephase reaction lasted about 3 days and the incidence was similar to that with placebo by the third infusion.19 in myeloma ix , acute - phase reactions , which are thought to result from immune - cell activation after the rst infusion of zoledronic acid , might have been less frequent than in the postmenopausal osteoporosis setting because of the fairly high prevalence of disease and treatment - related myelosuppression in patients with multiple myeloma . 
gastrointestinal adverse events are generally more common in patients given oral bisphosphonates , as noted heregastrointestinal treatment - emergent serious adverse events arose more frequently with clodronic acid than with zoledronic acid ( 12 vs three events , respectively )  . 
 are serious , potentially debilitating complications a ecting most patients with multiple myeloma , especially those who do not receive bone - targeted therapy.6 bisphosphonates can e ectively reduce the risk of skeletal - related events in this population.2022 consequently , clinical practice guidelines and recommendations include bisphosphonates as a key component of disease treatment for patients with myeloma bone disease.4 , 78 , 17 in the previous mrc myeloma studies , 9 , 10 clodronic acid was of particular bene t ( ie , slowing progression of skeletal disease and reducing skeletal morbidity ) to patients without bone skeletal - related events lesions at treatment initiation.9 , 10 moreover , subgroup analysis suggested that clodronic acid might confer survival bene ts in patients without overt bone disease at diagnosis.10 three bisphosphonates have been approved for patients with osteolytic bone lesions from multiple myelomazoledronic acid and pamidronic acid in the usa and europe , and clodronic acid in europe . 
previous comparison of zoledronic acid with pamidronic acid in patients with multiple myeloma showed no signi cant di erence in the incidence of skeletal - related events ( 86 [ 47% ] of 183 vs 82 [ 49% ] of 167 , respectively ) , 20 or the time to rst skeletal - related event ( 380 days vs 286 days , respectively ; p = 0538 ) among patients with multiple lesions.21 the myeloma and established osteolytic more recently introduced nitrogen - containing bisphosphonates , pamidronic acid and zoledronic acid , are more potent inhibitors of osteoclastic activity than are the earlier , non - nitrogen - containing bisphosphonates ( eg , clodronic acid ) .23 however , pamidronic acid is more similar to clodronic acid in terms of antiresorptive potency than it is to zoledronic acid , which has more potent anticancer e ects in preclinical models of myeloma and other cancers.2325 because of the short infusion time and particular antiresorptive potency of zoledronic acid compared with pamidronic acid con rmed in preclinical and clinical investigationsit was adopted as the comparator for clodronic acid , a uk standard , in the myeloma ix trial . 
treatment regimens for multiple myeloma also changed between the completion of the trial of zoledronic acid versus pamidronic acid , 21 and the start of the myeloma ix trial . induction chemotherapy regimens used to treat patients with multiple myeloma are continually evolving as new drugs and new combinations are assessed in clinical trials . 
 in recent years , there has been interest in the potential for immunomodulatory drugs ( eg , lenalidomide ) and bortezomib to slow osteolytic bone destruction in multiple myeloma through inhibition of osteoclast activity , ( eg , bortezomib ) .2630 so far , these data are derived from preclinical clinical assessments of biochemical markers of bone resorption and bone mineral density and have not yet been correlated with a reduction in the risk of skeletal - related events . 
there is no evidence to suggest that antimyeloma treatment alone can replace bisphosphonates for treatment of multiple myeloma bone disease ; however , the potential for synergistic and between bisphosphonates is intriguing . 
on the basis of the data this study , for skeletal - related events obtained studies and osteoblast increased activity e ects drugs these and 750 vol 12 august 2011 articles zoledronic acid is very likely to provide clinically in combination with newer signi cant bene ts antimyeloma regimens because it has proved bene cial in the prevention of skeletal - related events in patients with solid tumours who were given a broad range of primary anticancer treatments.21 , 31 , 32 however , clinical studies are needed to con rm this theory . 
 the myeloma ix study is the rst large , independent clinical trial in patients with newly diagnosed multiple myeloma , and its results show unequivocal superiority of one bisphosphonate over another for reduction of the risk of skeletal - related events . 
overall , the data from this study support the early use of zoledronic acid for reduction in the risk of skeletal - related events in all patients with newly diagnosed multiple myeloma . contributors gjm , jac , and ghj were chief investigators . 
gjm , jac , wmg , kc , seb , ajs , nn - c , and pw contributed to writing the report , generation of tables and gures , or data interpretation . 
gjm developed an early draft , and all authors contributed to the review and amendments and approved the submitted report . con icts of interest gjm has participated on advisory boards for , received payment for lectures and development of educational presentations from , and received travel support from celgene , novartis , merck , and johnson and johnson . 
gc has received speakers fees from celgene and janssen - cilag , payment for the development of educational presentations from celgene , acted as a consultant for celgene , janssen - cilag , and novartis , and received travel support to attend meetings from celgene and janssen - cilag . 
 fed has participated on advisory boards and spoken at meetings for celgene , ortho biotech , and novartis , and has received travel support to attend meetings from celgene and ortho biotech . 
we thank all the patients , investigators , and sta who participated in the mrc myeloma ix trial ; sta at the clinical trials research unit , university of leeds , leeds , uk , for trial coordination and data management ; sta at the department of immunology , university of birmingham , birmingham , uk ; sta at wessex regional genetics laboratory , university of southampton , southampton , uk ; sta at haematological malignancy diagnostic service , leeds teaching hospitals nhs trust , leeds , uk ; sta at institute of cancer research , london , uk , for central laboratory investigations ; david bowen for independent safety oversight ; the mrc leukaemia data monitoring and ethics committee ; the mrc leukaemia trial steering committee ; the national cancer research institute haematological oncology clinical studies group ; myeloma uk ; the national institute for health research for support , through the national cancer research network ; the support of biomedical research centre at the royal marsden hospital ; lead investigators , as previously reported ; 12 and michael hobert ( proed communications , beachwood , oh , usa ) , for his medical editorial assistance with this report . 
 surgery was delayed beyond 30 days , radiation should be given immediately instead . similarly , the section of our review1 on overall prioritisation of patients for surgery is highly nuanced , factoring in the important issues that should be considered when deciding on priority . 
the availability of alternative effective treatment modalities , for example , chemoradiotherapy for t2 n1 oropharyngeal cancer or radiotherapy for t1 n0 laryngeal cancer , results in deprioritisation of these cases for surgery ( not for treatment ) during severe resource constraint compared with cases in which surgery is the only , or significantly better , option ( eg , for advanced disease or t1 n0 oral cancer )  . hm is the director and a shareholder of warwickshire head and neck clinic ; chair of the head and neck cancer international group ; and past president of the british association of head and neck oncologists . 
hm also reports personal fees and grants from astrazeneca and sanofi pasteur ; grants from glaxosmithkline biologicals ; non - financial support from merck ; and personal fees , grants , and non - financial support from merck sharp and dohme . 
 j clin oncol 2016 ; 34 : 16978 . head and neck surgery recommendations during the covid - 19 pandemic authors reply we thank thomas j galloway and colleagues for their letter . 
however , the covid - 19 pandemic has resulted in an unprecedented situation in which there are little or no available data , and where the extrapolation of existing evidence is not appropriate in many cases . 
 for example , although reporting that early cancers were more affected by treatment delay , colin murphy and colleagues2 also reported that oral cancer outcomes were much less affected by delays in treatment than were laryngeal cancer outcomes . 
 murphy and colleagues2 also showed that the threshold for treatment delay that resulted in significant detriment was 67 days . we also urge galloway and colleagues to read our recommendations more carefully , including the explanatory text , as they are more nuanced than described in their letter . 
there was strong agreement not to delay up to 90 days . furthermore , our recommendations pertain to delays in surgery , which should not be conflated with delays in treatment , as many tumours can be treated by alternative , equally effective , non - surgical methods . 
for example , for laryngeal cancer , which is more affected by delays than oral cancer , there was agreement that if vol 21 september 2020 e417 correspondence the impact of the covid - 19 pandemic on cancer deaths due to delays in diagnosis in england , uk : a national , population - based , modelling study camille maringe , james spicer , melanie morris , arnie purushotham , ellen nolte , richard sullivan , bernard rachet * , ajay aggarwal * summary background since a national lockdown was introduced across the uk in march , 2020 , in response to the covid - 19 pandemic , cancer screening has been suspended , routine diagnostic work deferred , and only urgent symptomatic cases prioritised for diagnostic intervention . 
in this study , we estimated the impact of delays in diagnosis on cancer survival outcomes in four major tumour types . methods in this national population - based modelling study , we used linked english national health service ( nhs ) cancer registration and hospital administrative datasets for patients aged 1584 years , diagnosed with breast , colorectal , and oesophageal cancer between jan 1 , 2010 , and dec 31 , 2010 , with follow - up data until dec 31 , 2014 , and diagnosed with lung cancer between jan 1 , 2012 , and dec 31 , 2012 , with follow - up data until dec 31 , 2015 . 
we use a routes - to - diagnosis framework to estimate the impact of diagnostic delays over a 12 - month period from the commencement of physical distancing measures , on march 16 , 2020 , up to 1 , 3 , and 5 years after diagnosis . 
to model the subsequent impact of diagnostic delays on survival , we reallocated patients who were on screening and routine referral pathways to urgent and emergency pathways that are associated with more advanced stage of disease at diagnosis . 
we considered three reallocation scenarios representing the best to worst case scenarios and reflect actual changes in the diagnostic pathway being seen in the nhs , as of march 16 , 2020 , and estimated the impact on net survival at 1 , 3 , and 5 years after diagnosis to calculate the additional deaths that can be attributed to cancer , and the total years of life lost ( ylls ) compared with pre - pandemic data . findings we collected data for 32 583 patients with breast cancer , 24 975 with colorectal cancer , 6744 with oesophageal cancer , and 29 305 with lung cancer . 
across the three different scenarios , compared with pre - pandemic figures , we estimate a 7996% increase in the number of deaths due to breast cancer up to year 5 after diagnosis , corresponding to between 281 ( 95% ci 266295 ) and 344 ( 329358 ) additional deaths . 
for colorectal cancer , we estimate 1445 ( 13921591 ) to 1563 ( 15341592 ) additional deaths , a 153166% increase ; for lung cancer , 1235 ( 12201254 ) to 1372 ( 13431401 ) additional deaths , a 4853% increase ; and for oesophageal cancer , 330 ( 324335 ) to 342 ( 336348 ) additional deaths , 5860% increase up to 5 years after diagnosis . 
the total additional ylls across these cancers is estimated to be 59 20463 229 years . interpretation substantial increases in the number of avoidable cancer deaths in england are to be expected as a result of diagnostic delays due to the covid - 19 pandemic in the uk . 
urgent policy interventions are necessary , particularly the need to manage the backlog within routine diagnostic services to mitigate the expected impact of the covid - 19 pandemic on patients with cancer . funding uk research and innovation economic and social research council . copyright 2020 the author ( s )  . 
these patient groups include patients with cancer for whom timely diagnosis and the prompt initiation of treatment is vital for ensuring optimal outcomes.2 , 3 since the beginning of the pandemic , multiple changes in the provision of cancer care from the point of diagnosis , including modification of treatment schedules ( change in therapy , deferral , or omission ) , have been advised by professional bodies and commissioners of services globally.47 however , substantial heterogeneity has been seen in the imple mentation of these recommendations lancet oncol 2020 ; 21 : 102334 published online july 20 , 2020 s1470 - 2045 ( 20 ) 30388 - 0 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on december 30 , 2020 see comment page 1000 * joint senior authors department of non - communicable disease epidemiology ( c maringe phd , prof b rachet phd ) and department of health services research and policy ( m morris phd , prof e nolte phd , a aggarwal phd ) , london school of hygiene & tropical medicine , london , uk ; school of cancer and pharmaceutical sciences ( prof j spicer phd , prof a purushotham md , prof r sullivan phd ) and institute of cancer policy ( prof r sullivan , a aggarwal ) , kings college london , london , uk ; and department of oncology , guys and st thomas nhs foundation trust , london , uk ( prof j spicer , prof a purushotham , prof r sullivan , a aggarwal ) correspondence to : dr ajay aggarwal , department of health services research and policy , london school of hygiene & tropical medicine , london , wc1h 9sh , uk ajay.aggarwal@lshtm.ac.uk vol 21 august 2020 1023 articles research in context evidence before this study in the uk , national covid - 19 pandemic measures since march 16 , 2020 , have resulted in the suspension of cancer screening and deferral of routine diagnostic investigations . 
 additionally , urgent 2 - week wait referrals for patients with suspected cancer initiated by general practitioners ( gps ) have decreased by up to 80% in response to physical distancing . 
to date , no study has attempted to model the impact of changes in health - seeking behaviour and in the availability of and access to diagnostic services in the uk as a result of the covid - 19 lockdown on cancer survival and the additional number of deaths expected . added value of this study to our knowledge , this study is the first of its kind to estimate the impact of delays in diagnostic pathways due to pandemic lockdown measures on cancer survival for four major tumour types . 
we use linked national cancer registration and hospital datasets , which provide a robust template for understanding the impact of current and predicted changes in availability , access , and health - seeking behaviour in response to the covid - 19 pandemic on cancer survival . 
we used a routes - to - diagnosis framework , which is novel and provides a transparent approach to understanding what components of the diagnostic pathway need to be targeted as part of health service mitigation and recovery programmes . 
we also estimated the years of life lost to understand the wider welfare effects resulting from avoidable cancer deaths , and how this varies according to tumour type and the age profile of men and women diagnosed with these cancers . 
 implications of all the available evidence our results are conservative estimates of the number of additional deaths and years of life lost because we do not consider the effect of suboptimal or delayed cancer treatment . 
 these data are essential for policy makers to drive changes in national lockdown and stay - at - home messaging , and to urgently reduce diagnostic delays , particularly for routine investigations , through outreach and accessibility programmes . 
 our model can also be used by other countries in their unique health - care settings to understand the impact of delays in diagnosis on cancer outcomes . across providers nationally and internationally and for individual patients . 
such variations in the extent of treatment delay , and in changes to treatment doses and schedules ( including new treat ment techniques ) mean that modelling of these variations in practice on cancer outcomes at a population level is challenging . instead , in this study , we focused on analysing the impact of changes in cancer diagnostic pathways and subsequent delays in diagnosis during the covid - 19 pandemic . 
routine non - urgent diagnostic work initiated by referral from both primary care ( general practitioners [ gps ] ) and secondary care teams ( eg , for radiology or endoscopic procedures8 ) has been deferred across the uk . 
cancer screening services have been suspended , and patients only routes to diagnosis since lockdown began have been via urgent 2 - week - wait referral pathways for suspected cancer initiated by the gp or through direct presentation to an emergency department.9 patients are eligible for these rapid access 2 - week - wait pathways to access diagnostic investigations , on the basis of their age , symptom profile ( eg , dysphagia ) , signs ( eg , breast lump ) , or results of investigations ( eg , iron deficiency anaemia ) as specified by guidelines developed by the national institute for health and care excellence.9 however , since march , 2020 , changes in health - seeking behaviour have been observed , with urgent 2 - week - wait cancer referrals decreasing by up to 80% in response to physical distancing and concerns about contracting severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) .10 additionally , some form of physical distancing is expected to continue for up to 12 months , which will probably further affect presentations to healthcare services.11 , 12 quantifying the impact of delays in diagnosis on stage and prognosis is complex , but a routes - to - diagnosis approach provides a validated methodological framework for understanding their effect . 
for example , urgent 2 - weekwait referrals for suspected cancer and emergency presentations are asso ciated with later stage of disease at diagnosis than diag noses via routine gp and secondary care referral routes and screening . 
additionally , diagnosis after initial presen tation to an emergency department is consistently asso ciated with the worst survival outcomes compared with all other routes.13 given the changes in health - seeking behaviour and availability and access to diagnostic services as a result of the covid - 19 lockdown , these routes to diagnosis provide a framework for estimating the impact of these changes on stage migration and excess cancer mortality on the basis of patients moving to different referral routes during the pandemic . the effect of delayed presentation on patients with cancer is not immediate , and premature death as a result 1024 vol 21 august 2020 articles might occur up to 5 years later and will differ according to tumour type . 
in this study , using national population datasets of patients diagnosed and treated in the english nhs , we estimated the impact of delays in diagnosis that are attributed to the lockdown measures put in place in the uk in march , 2020 , for four major tumour types : breast , colorectal , lung , and oesophageal . 
we chose these tumour types because they differ in their predominant routes to referral ( including screening ) , stage at presentation , and both short - term and long - term prognoses according to stage . 
we estimated the effect on patient survival and the number of additional deaths expected due to these cancers , and the additional years of life lost ( ylls )  . international classification methods study design and population in this national , population - based , modelling study , we obtained information on adults in england , uk , with non - small - cell lung cancer ( hereafter referred to as lung of diseases cancer : 10th edition c33 , c34 ) , cancers of the colon ( c18 ) and rectum ( c19 ) , cancers of the oesophagus and gastrooesophageal junction ( c15 , c16.0 ) , and women with breast cancer ( c50 ) from the national cancer registration service . 
the pre - pandemic cohort refers to patients diagnosed between jan 1 , 2010 , and dec 31 , 2010 , with follow - up data until dec 31 , 2014 , for cancers of the colon , rectum , oesophagus , and breast , and to patients diagnosed between jan 1 , 2012 , and dec 31 , 2012 , with follow - up data until dec 31 , 2015 , for lung cancer . 
we restricted the analyses to patients aged 1584 years at diagnosis and those who had a known route of diagnosis coded ( ie , 91% of patients for colorectal cancer , 93% of patients for oesophageal cancer , 94% of patients for breast cancer , and 97% of patients for lung cancer )  . the national cancer registration service records and updates patient and tumour characteristics for almost all cancers diagnosed in england ( 98100% ) .14 we derived infor mation on referral pathways from linkages of the cancer registrations with secondary care data ( hospital episode statistics ) , screening records , and data on cancer waiting times.13 we did these linkages using deterministic linkage methods using each individual patients nhs number , with a linkage success of 99100%.14 we derived information on patients comorbidity status from hospital episode statistics diagnostic codes when patients attend hospital.15 we determined levels of deprivation via the quintiles of the index of multiple deprivation income domain for the patients residential postcodes , measured at lower super output area level.16 we used this information to link each patient with their expected mortality according to age , sex , deprivation , and region of residence using general population life tables . this study was done in accordance with existing statutory and ethical approvals from the confidentiality advisory group and research ethics committee ( piag 105 ( c ) / 2007 and rec 13 / lo / 0610 )  . conceptual framework we assumed that the incidence of each of the four tumour types of interest will remain relatively stable year on year on the basis of trends in previous years ( 201018 ) , 17 and that the ongoing covid - 19 pandemic and uk lockdown will mean patients are more likely to delay presentation . 
 we estimated the subsequent impact on survival by reallocating patients from screening and non - urgent routine referral pathways ( from gps and secondary care ) to urgent pathwaysnamely , 2 - week wait referral routes and presentation at an emergency department . 
both of these urgent pathways are associated with later stage of diagnosis and enabled us to estimate the impact of diagnostic delay on stage migration and survival outcome . we justified our reallocation model on four assumed factors . 
second , although routine diagnostic work and non - urgent referral pathways are delayed and screening suspended , some patients awaiting investigation will become symptomatic as their cancer progresses and will meet the criteria for urgent 2 - week wait referral for suspected cancer or present as emergencies direct to secondary care . 
third , for patients awaiting routine diagnostic investigations from their gp and secondary care referrals , substantial delays are expected ( > 6 months ) 12 due to the backlogs of routine work across all medical and surgical services increasing the likelihood of disease progression , which we estimated via reallocation to 2 - week wait and emergency pathways . 
finally , changes in health - seeking behaviour as a result of the pandemic means that some patients will delay presentation until more prominent symptoms develop , and these patients will be more likely to present through 2 - week - wait and emergency pathways . the starting point for our estimation is from march 16 , 2020 , which is the date physical distancing measures were introduced in the uk , and the impact is modelled over a 12 - month period to account for the expected duration of disruption to services and patterns of referral . 
this period defines our cohort of expected number of cancer diagnoses for each tumour type , but we acknowledge that patients might present and be diagnosed beyond this period because of diagnostic delay . 
for example , if 10% of new diagnoses for a given tumour type are after an emergency department presentation , and 90% are via an outpatient referral , our simulation analysis will maintain these proportions when reallocating patients from screening and routine referral pathways . for patients with breast cancer diagnosed via the screening referral pathway , we accounted for the fact that many are diagnosed with pre - invasive disease18 or disease that is unlikely to progress even within a 12 - month period . 
this percentage reflects for more on the hospital episode statistics database see vol 21 august 2020 1025 articles pre - pandemic referral routes 2 - week wait emergency presentation gp routine routine ( outpatients ) routine ( inpatients ) screening 2 - week wait or emergency presentation , both at 100% capacity 2 - week wait , at 20% capacity emergency presentation , at 100% capacity 2 - week wait or emergency presentation , both at 100% capacity 2 - week wait , at 20% capacity emergency presentation , at 100% capacity 2 - week wait , at 75% capacity emergency presentation , at 100% capacity 2 - week wait or emergency presentation , both at 100% capacity scenario time since march 16 , 2020 ( months ) figure 1 : conceptual framework for reallocation of pre - pandemic referral routes in three modelling scenarios ( a , b , and c ) for breast cancer , in addition to patients on routine pathways , only 25% of patients diagnosed through screening ( ie , the proportion of patients with tumour stage iii or iv , node - positive , or metastatic disease ) were reallocated to 2 - week wait or emergency presentation in the pandemic scenarios . 
for colorectal cancer , we undertook reallocation separately for colon and rectal cancer because the proportion of patients presenting via the different referral routes differed between the two cancers , as did the cancer stage at the time of diagnosis . scenarios we based our analysis on three sets of predictions according to possible changes in referral patterns ( figure 1 ) representing the best and worst case scenarios . 
 for scenario a , we estimated survival outcomes for patients by reallocating those who are expected to be diagnosed through screening and routine referral pathways ( gp or secondary care ) to 2 - week - wait and emergency presentation pathways , from march 16 , 2020 . 
 scenario b is the same as scenario a , but from march 16 , we simulated the effect of an 80% reduction in 2 - weekwait referrals , which has already been observed during the lockdown period , 10 and assumed that this reduction will continue ( due to covid - 19 - related concerns ) for up to 3 months . 
and scenario c is the same as scenario b , but we simulated the effect of 2 - week - wait referrals continuing to be reduced beyond the first 3 - month period by 25% for a further 3 - month periodie , until month 6 after introduction of physical distancing measures . 
 therefore , we re - allocated the backlog of patients in months 712 to 2 - week - wait pathways and emergency presentations . statistical analysis we randomly modified the mode of presentation and dates of diagnosis of the pre - pandemic cohorts according to scenarios ac . 
for scenarios b and c , we reallocated a proportion of patients diagnosed through the 2 - week - wait pathway because under these scenarios this referral route was assumed to operate at 20% ( scenario b ) and 75% ( scenario c ) of its usual capacity . we estimated the reallocation of patients from routine and screening pathways to the emergency presentation route at the same proportion observed in the prepandemic cohorts ( table 1 )  . to estimate the impact that the response to the covid - 19 pandemic could have on cancer survival , we compared the net survival of pre - pandemic cohorts of patients with cancer to that of patients diagnosed according to the postulated scenarios ac . 
notably , for colorectal cancer , even though the reallocation from routine to urgent pathways was done separately for patients with rectal and colon cancer , the survival estimates are for the combined colorectal cancer population . 
compared with the number of deaths due to cancer in the pre - pandemic cohorts , we derived the additional number of deaths due to cancer and addi tional number of ylls . 
for breast cancer , in addition to patients on routine pathways , only 25% ( n = 2700 ) of patients diagnosed through screening ( ie , the proportion of patients with t3 , t4 , node positive , or metastatic disease ) were reallocated to 2 - week wait and emergency presentation in the pandemic scenarios . 
 * the proportion of patients diagnosed with stage iii or iv disease is based on patients with available staging information in the cancer registry dataset and has been reported to show the stage variation according to diagnostic referral route ; information on cancer stage is not used in the modelling of net survival . 
point estimates and 95% cis were calculated from bootstrap samples of the original data . table 2 : estimated cumulative number of deaths due to cancer up to 1 year , 3 years , and 5 years after diagnosis , in the pre - pandemic period and for each pandemic scenario ac ( also presented as additional number of deaths ) government office regions . 
since each cancer site - specific mortality is a negligible cause of death , all - cause mortality , as estimated from population life tables , is the mortality that patients with cancer would experience , had they not been diagnosed with cancer.20 , 21 further details and mathe matical formulae are in the appendix ( pp 13 )  . 
cm , br , and aa had full access to all the data in the study and had final responsibility for the decision to submit to publication . results we analysed data on 32 583 patients with breast cancer , 24 975 with colorectal cancer , 29 305 with lung cancer , and 6744 with oesophageal cancer ( table 1 )  . 
patients were aged 1584 years and the mean age at diagnosis was 605 years ( sd 126 ) for breast cancer , 685 years ( 107 ) for colorectal cancer , 685 years ( 103 ) for oesophageal cancer , and 698 years ( 93 ) for lung cancer . 
10 441 ( 418% ) of 24 975 patients diagnosed with colorectal cancer , 13 211 ( 451% ) of 29 305 diagnosed with lung cancer , and 1894 ( 281% ) of see online for appendix vol 21 august 2020 1029 articles b colorectal scenario a scenario b scenario c lung cancer ( n = 29 305 ) oesophageal breast 1500 1000 lung 1500 1000 follow - up time ( years ) follow - up time ( years ) figure 2 : estimated additional number of cancer deaths for each pandemic scenario ac , for breast cancer ( a ) , colorectal cancer ( b ) , lung cancer ( c ) , and oesophageal cancer ( d ) 6744 diagnosed with oesophageal cancer were women . 
in the pre - pandemic period , survival varied substantially by tumour type and referral pathway , with the worst prognosis evident for oesophageal and lung cancers and for patients diagnosed after an emergency presentation . 
these differences in sur vival between referral path ways correlated with increased proportions of patients diagnosed at stages iii and iv , irrespective of tumour type ( table 1 ; appendix p 4 )  . 
notably , 2 - week - wait referral pathways are not associated with substantial differences in stage or survival compared with nonurgent referral routes . we estimated the impact of diagnostic delay for the 12 - month period from march 16 , 2020 , to march 15 , 2021 . 
 across scenarios ac , we estimated an absolute decrease in cancer survival ranging between 1011% ( breast , all scenarios ) and 6163% ( oesophageal , scenarios b and c ) at 1 year after diagnosis , and between 35% ( lung , scenario a ) and 64% ( colorectal , scenario c ) at 5 years after diagnosis ( table 1 )  . the differences in survival translate into substantial additional numbers of deaths due to cancer in the first 5 years of follow - up . 
the estimated number of deaths due to each cancer up to 1 , 3 , and 5 years after diagnosis in the pre - pandemic period and across scenarios ac are shown in table 2 . 
the number of additional cancer deaths estimated across the scenarios are shown as cumulative estimates up to year 5 ( table 2 , figure 2 )  . breast cancer ( n = 32 583 ) colorectal cancer ( n = 24 975 ) scenario a scenario b scenario c scenario a scenario b scenario c scenario a scenario b scenario c scenario a scenario b scenario c oesophageal cancer ( n = 6744 ) years of life lost ( 95% ci ) 8181 ( 77978535 ) 9033 ( 86389390 ) 9261 ( 88439631 ) 27 735 ( 27 18828 241 ) 25 583 ( 24 79227 744 ) 27 043 ( 26 23429 968 ) 20 537 ( 20 18420 947 ) 20 860 ( 20 25021 277 ) 20 413 ( 19 83320 909 ) 5373 ( 52275530 ) 5152 ( 50065301 ) 5027 ( 48615213 ) point estimates and 95% cis were calculated from bootstrap samples of the original data . table 3 : estimated years of life lost from additional deaths due to cancer , at 5 years from diagnosis , for each pandemic scenario we estimated across scenarios ac , compared with the pre - pandemic period , a 2166% increase in the number of deaths due to breast cancer up to year 1 ( corresponding to between 20 [ 95% ci 1525 ] and 63 [ 5770 ] additional deaths ) , a 6891% increase up to year 3 ( 169 [ 159179 ] to 228 [ 218239 ] additional deaths ) , and a 7996% increase up to year 5 ( 281 [ 266295 ] to 344 [ 329358 ] additional deaths )  . 
for lung cancer across scenarios ac , we estimated a 6077% increase in the number of deaths due to cancer up to year 1 ( 1102 [ 10871117 ] to 1412 [ 13791447 ] additional deaths ) , a 5158% increase up to year 3 ( 1231 [ 12161249 ] to 1412 [ 13811442 ] additional deaths ) , and a 4853% increase up to year 5 ( 1235 [ 12201254 ] to 1372 [ 13431401 ] additional deaths )  . 
for oesophageal cancer , across scenarios ac , we estimated a 93103% increase in deaths due to cancer up to year 1 ( 339 [ 334343 ] to 377 [ 372383 ] additional deaths ) , a 6467% increase up to year 3 ( 343 [ 337348 ] to 359 [ 354365 ] additional deaths ) and a 5860% increase up to year 5 ( 330 [ 324335 ] to 342 [ 336348 ] additional deaths )  . the plateau in additional deaths due to cancer over the 5 - year period for lung and oesophageal cancer ( figure 2 ) reflects relatively higher proportions of early cancer deaths at year 1 due to more advanced stage at presentation in our scenarios . 
in the pre - pandemic period , some of these patients would have been expected to die 1030 vol 21 august 2020 articles beyond year 1 as a result of less advanced disease at presentation compared with the pandemic scenarios . overall , in comparison with the pre - pandemic period , the estimated number of additional deaths attributable to these four cancers at 5 years is between 3291 and 3621 deaths across the scenarios due to delays in cancer diagnosis ( table 2 , figure 2 )  . 
we estimated the expected ylls to be between 59 204 and 63 229 years because of additional deaths due to these four cancers in the first 5 years after diagnosis . discussion we estimated that across the four major tumour types , breast , colorectal , lung , and oesophageal , 3291 to 3621 avoid able deaths and an additional 59 204 to 63 229 ylls will be attributable to delays in cancer diagnosis alone as a result of the covid - 19 lockdown in the uk . 
these additional deaths are projected to occur as a conse quence of the national covid - 19 pandemic measures , which have reduced the number of people seeking health care and access to and availability of diagnostic services . 
our findings complement those from a study by sud and colleagues22 showing the impact of treatment delay , predominantly surgical , on excess mortality . from the onset of the lockdown , essential diagnostic services ( eg , endoscopy ) were suspended or operating at substantially reduced capacity , even through the urgent 2 - week - wait referral pathway . 
the number of endo scopies done in april , 2020 , was 90% fewer than the number done in each of the first three months of 2020.23 as of june , 2020 , these diagnostic services had restarted but at reduced capacities.24 these suspensions were due to the perceived risk of exposure to sars - cov - 2 for patients and clinicians , and because of re - deployment of staff towards critical care to manage patients with covid - 19 . 
our results also highlight the substantial proportion of patients diag nosed with cancer through routine outpatient referral pathways ( 3040% ) and the subsequent effect of deferral and delay in these referral pathways during the pandemic . 
even when routine diagnostic services are re - initiated , substantial delays in routine and 2 - week - wait referral pathways are to be expected due to backlogs currently building up across all benign and malignant medical and surgical subspecialities . changes in health - seeking behaviour have meant that routine referrals from gps have reduced in volume because patients are being asked to only present if they have major or urgent concerns.12 additionally , whether the increasing number of remote consultations via telephone or videoconferencing will result in an increased proportion of missed diagnoses , without the ability to examine and triage the patient directly , is unknown . conversely , increased diagnostic efficiency has potentially been introduced into the system as a result of the pandemic . 
for example , patients who now report a symptom to their gp are an enriched population compared with those who reported in the pre - pandemic period and are potentially more likely to have cancer . 
additionally , as of june 18 , 2020 , 2 - week - wait referrals are still not operat ing at level , particularly for endoscopic intervention.25 their usual pre - pandemic our findings reflect the urgent need for policy interventions to mitigate the predicted additional cancer deaths resulting from delays in diagnosis . 
key areas to consider include public health messaging , the publics perception of their personal risk of severe illness from covid - 19 versus the risks of not seeking health - care advice if they are experiencing symptoms suggestive of cancer , provision of evidence - based information to enable health - care workers to adequately manage the risks for patients with suspected cancer during the pandemic with respect to the balance of risks and benefits of procedures , and to consider options and opportunities for increasing diagnostic capacity . in the uk , the stay at home and subsequent stay alert public health messaging has had a substantial effect on health - seeking behaviour.26 even as lockdown measures are being relaxed , presentation to primary care services continues to be much lower than pre - pandemic levels , 25 and we cannot assume that , once all restrictions have been lifted , presentations will return to pre - pandemic levels in the next 36 months . 
any exit strategy from lockdown27 therefore needs to include accurate and measured public health messaging that is tailored towards patients , gps , and secondary care services that puts into perspective the risk of death from covid - 19 compared with other serious illnesses . 
dedicated cancer awareness programmes will need to consider a range of media channels to reach their target groups , including direct messaging from gps to their patients to seek attention if they are having new or worrying symptoms . increasing diagnostic capacity is complex because it necessitates effective coordination across all hospital subspecialities and not just in specialist cancer teams . 
 additionally , the requirement for full personal protective equipment when doing procedures and the initiation of robust cleaning protocols between patients has reduced capacity compared with pre - pandemic levels . 
in the short term , diagnostic capacity can be increased through vol 21 august 2020 1031 articles changes in working patternseg , increased working hours and 7 days - a - week working . 
furthermore , a central coordinating system for diagnostic investigations in a similar vein to a choose - and - book approach , whereby primary care physicians are able to refer patients to any nhs hospital , will optimise use of capacity.28 for detection of bowel cancer , surgeons are increasingly using new tools such as the faecal immuno chemical test29 to triage their patients for investigation to avoid unnecessary colonoscopy and ct imaging and therefore improving capacity in this diagnostic pathway . the paucity of information for health - care workers and patients regarding their risk of contracting covid - 19 from different health - care interactions remains a challenge as hospitals plan for restarting routine services . 
 antibody testing would increase confidence in clinicians doing procedures if immunity to sars - cov - 2 does exist for even a short period.30 the health - care community needs accurate data on the true nosocomial risk of covid - 19 depending on the type of diagnostic procedure being doneeg , colonoscopy versus ct scan . 
equally , the implication of contracting covid - 19 needs to be consideredspecifically , to be able to counsel patients effectively on the true risk of lifethreatening illness and death . a strength of this study is the use of linked national administrative health records of actual patients diagnosed and treated in the nhs for the four tumour types . 
these records provide a robust template for understanding the impact of current and predicted changes in availability , access , and health - seeking behaviour in response to the covid - 19 pandemic on cancer survival . 
this method does not require any de - novo estimation of changes in cancer outcomes but derives this estimation from previous real - world observations . we chose the routes - to - diagnosis concept as our method to analyse diagnostic delay to overcome some of the challenges that have been raised in the scientific literature regarding the relative risk of death from diagnostic delay across tumours.2 , 31 , 32 inconsistencies in the evidence are primarily associated with flaws in study design in which the true onset of symptoms remains unclear . 
additionally , recent work has pointed to a waiting time paradox , whereby quicker diagnosis is associated with later stage of presentation ; this paradox confounds assessment of the impact of diagnostic delay on outcomes.33 , 34 modelling the extent and duration of diagnostic delay at the population level is challenging because diagnostic delays are predicated on health system factors , such as access and availability of diagnostic capacity , and patient - level factors ( awareness , symptoms , health - seeking behaviour )  . 
we acknowledge that our approach might underestimate or overestimate the impact of diagnostic delay on survival , and retrospective evaluation will be necessary to further appraise this modelling approach . 6 months after our model assumes that disruptions due to the covid - 19 pandemic will affect timely access to routine and urgent diagnostic services and alter health - seeking behaviour for a 12 - month period . 
these assumptions are likely given the changes in patterns of patient presentation and availability of diagnostic services observed since the start of lockdown.1 , 11 , 12 , 24 , 25 since beginning our modelling study , substantial reduction in 2 - week - wait referrals have indeed been seen in the first 3 months , as we predicted in scenarios b and c . 
given the ongoing reductions in the volume of 2 - week - wait referrals ( estimates suggest a 4050% reduction ) , 35 reductions are expected to continue for up to 6 months as predicted in scenario c because of the effects of pandemic lockdown measures on patients presenting to their gp or health - care provider . 
 these measures include advice to minimise non - essential travel and the continued shielding of high - risk groups.1 , 12 cancer research uk has estimated that the first 10 weeks of the uk lockdown has already resulted in 21 million deferred cancer screening investigations with 290 000 fewer people being referred on 2 - week - wait pathways.35 the implementation of physical distancing mea sures the backlog of patients with potential cancers awaiting investigation will be considerable , and health - care presentations will continue to be affected due to physical distancing measures that are expected to continue until 2021.11 , 12 additionally , nhs hospital trusts suspended their routine diagnostic services at the start of lockdown , which is concerning because routine referral routes account for 3040% of cancer diagnoses and the backlog in this pathway once routine services restart will include all patients still awaiting diagnostic investigations both from before and after lockdown started . 
further competition for capacity will subsequently come from the increase in new referrals for suspected cancers on 2 - weekwait referrals and those referred for investigation or follow up of seemingly benign health conditions . 
at the same time , diagnostic capacity has decreased for some procedures due the increased time taken per case since the introduction of new infection control measures.36 together , all these factors will increase the likelihood of patients becoming symptomatic and presenting via 2 - week - wait referral or emergency pathways . 
alternatively , if or when patients are diagnosed through routine pathways , the likelihood of stage migration and associated worse prognosis due to delays in diagnosis is increased . our analysis used a retrospective population cohort , therefore , the predicted survival for patients as of 2020 presenting via the different referral pathways , even for patients with stage iv disease , has slightly improved37 in the past decade because of improvements in treatments and processes of care . 
however , our analysis focuses on 1032 vol 21 august 2020 articles treatment on survival during the differences in cancer deaths between two situations ( pre - pandemic and pandemic periods ) and not on the absolute numbers of cancer deaths . 
additionally , these estimates do not consider the impact of treatment delay or suboptimal the pandemic.22 the proportions of patients presenting through different referral pathways has changed over time , with decreasing proportions of patients presenting via emergency depart ments in the past decade , which might also affect our results.38 however , we consider the probable effect on the overall results to be small given the steady trajectories of improvements in patterns of presentation we have seen over the past 5 years.37 , 38 we did not analyse patients aged 85 years or older at diagnosis because competing events , such as deaths from other causes , are predominant in this population . 
 although delays in cancer diagnosis in older populations will lead to excess short - term cancer mortality , the effect on national population - levels is less likely to be affected . 
 furthermore , because we report survival up to 5 years after diagnosis , such an estimate is less reliable in patients aged 90 years and older . in the screening population , we recognise that not all patients diagnosed with breast cancer through this route would have progressed or developed symptomatic disease . 
for colorectal cancer , 10% of patients are diagnosed through the screening route , of whom 45% are diagnosed with stage iiiiv disease ( 70% stage iiiv ) compared with 6% diagnosed with stage iiiiv tumours through breast cancer screening ; hence , we showed that more patients with colorectal cancer are diagnosed with advanced disease at screening compared with those diagnosed with breast cancer . 
overdiagnosis and overtreatment are not specific concerns associated with the bowel screening programme , 39 whereas they are concerns associated with breast screening , and the suspension of the bowel screening programme is likely to result in delayed presentation and stage migration if cancers remain untreated.40 our model also considered the english nhs as a whole , and therefore assigned blanket reallocation across the country . 
however , we recognise that variation is probable across the country in terms of gp access , the burden of covid - 19 , and the extent of discontinuation of critical diagnostic services in secondary care settings . 
 in this regard , we acknowledge that 2 - week - wait referrals have not decreased uniformly by 80% across all tumour types and uk regions , as per our estimations in scenarios b and c . 
additionally , variation will exist in the recovery of services across regions and individual hospitals , which are not included in our estimations . in summary , we estimated that changes in healthseeking behaviour and the availability of and access to essential diagnostic services resulting from national pandemic measures will result in a large number of additional deaths from breast , colorectal , lung , and oesophageal cancer in the medium ( 1 year ) and longer term ( 5 years )  . 
our study results do not consider the effect of delay on other cancer types , or the additional effect of changes in treatment pathways for these cancers that are likely to substantially increase the expected avoidable deaths beyond what we have estimated . 
these interventions should focus on increasing routine diagnostic capacity through which up to 40% of patients with cancer are diagnosed , public health messaging that accurately conveys the risk of severe illness from covid - 19 versus the risks of not seeking healthcare advice if patients are symptomatic , and the provision of evidence - based information for clinicians to adequately manage the risks of patients to the risk and benefits of procedures during the pandemic . contributors aa , mm , en , rs , and br conceived and designed the study . 
cm , js , mm , ap , en , rs , br , and aa were involved in reviewing and editing drafts of the paper and approving the manuscript . declaration of interests we declare no competing interests . data sharing this study was based on english national cancer registry data . 
we do not own these data and hence are not permitted to share them in the original forthe data are available from the office for data release at public health england . 
cm and br are funded through the cancer research uk population research committee funding scheme : cancer research uk population research committee programme award ( c7923 / a20987 and c7923 / a29018 )  . 
js is supported by the nihr biomedical research centre based at guys and st thomas nhs foundation trust and kings college london ( is - brc - 1215 - 20006 ) , and the cancer research uk kings health partners centre at kings college london ( c604 / a25135 )  . 
the portec - 3 trial was initiated to investigate the benefit of adjuvant chemotherapy during and after radiotherapy ( chemoradiotherapy ) versus pelvic radiotherapy alone for women with high - risk endometrial cancer . methods portec - 3 was an open - label , international , randomised , phase 3 trial involving 103 centres in six clinical trials collaborating in the gynaecological cancer intergroup . 
eligible women had high - risk endometrial cancer with figo 2009 stage i , endometrioid - type grade 3 with deep myometrial invasion or lymph - vascular space invasion ( or both ) , endometrioid - type stage ii or iii , or stage i to iii with serous or clear cell histology . 
women were randomly assigned ( 1 : 1 ) to receive radiotherapy alone ( 486 gy in 18 gy fractions given on 5 days per week ) or radiotherapy and chemotherapy ( consisting of two cycles of cisplatin 50 mg / m given during radiotherapy , followed by four cycles of carboplatin auc5 and paclitaxel 175 mg / m ) using a biased - coin minimisation procedure with stratification for participating centre , lymphadenectomy , stage of cancer , and histological type . 
5 - year overall survival was 818% ( 95% ci 775862 ) with chemoradiotherapy versus 767% ( 721816 ) with radiotherapy ( adjusted hazard ratio [ hr ] 076 , 95% ci 054106 ; p = 011 ) ; 5 - year failure - free survival was 755% ( 95% ci 703799 ) versus 686% ( 631734 ; hr 071 , 95% ci 053095 ; p = 0022 )  . 
grade 3 or worse adverse events during treatment occurred in 198 ( 60% ) of 330 who received chemoradiotherapy versus 41 ( 12% ) of 330 patients who received radiotherapy ( p < 00001 )  . 
 neuropathy ( grade 2 or worse ) persisted significantly more often after chemoradiotherapy than after radiotherapy ( 20 [ 8% ] women vs one [ 1% ] at 3 years ; p < 00001 )  . 
most deaths were due to endometrial cancer ; in four patients ( two in each group ) , the cause of death was uncerta one death in the radiotherapy group was due to either disease progression or late treatment complications ; three deaths ( two in the chemoradiotherapy group and one in the radiotherapy group ) were due to either intercurrent disease or late treatment - related toxicity . interpretation adjuvant chemotherapy given during and after radiotherapy for high - risk endometrial cancer did not improve 5 - year overall survival , although it did increase failure - free survival . 
continued follow - up is needed to evaluate long - term survival . funding dutch cancer society , cancer research uk , national health and medical research council project grant and cancer australia , lagenzia italiana del farmaco , and canadian cancer society research institute . copyright the author ( s )  . 
in adjusted analysis , improved progression - free survival and overall survival were reported for patients treated with chemotherapy , but with high proportions of patients with toxicity and similar event rates in both groups . 
two trials ( one in italy and one in japan ) compared pelvic radiotherapy with three cycles or five cycles of cyclophosphamidedoxorubicincisplatin chemotherapy in stage iiii disease and neither showed any difference in overall survival or relapse - free survival . 
in the italian trial , most patients had stage iii disease , and chemotherapy delayed distant metastases and radiotherapy delayed pelvic recurrence , but without differences in overall survival or progression - free survival . 
the phase 2 rtog - 9708 trial , which assessed toxicity on the chemoradiotherapy schedule on which portec - 3 is based , reported 4 - year overall survival of 85% and disease - free survival of 81% . 
the nsgo - ec - 9501 / eortc - 55991 trial was published in a pooled analysis with the unfinished mango iliade phase 3 trial , and showed significantly improved progression - free survival and a trend for improved overall survival with the addition of four cycles of platinum - based chemotherapy given sequentially before or after pelvic radiotherapy . 
the results of the gog - 249 trial , which compared pelvic radiotherapy with a combination of three cycles of carboplatin - paclitaxel chemotherapy and vaginal brachytherapy in stage iii patients with high ( intermediate ) risk factors reported overlapping progressionfree survival and overall survival curves , and significantly more pelvic and para - aortic recurrences in the chemotherapy group . 
no differences in overall or recurrence - free survival were reported , but significantly more vaginal and pelvic or para - aortic recurrences were reported in the chemotherapy group . added value of this study we report the overall survival and failure - free survival of patients with high - risk endometrial cancer treated in the international portec - 3 trial . 
the treatment duration was longer in the chemoradiotherapy group than in the radiotherapy group , and significantly higher rates of adverse events were reported in the chemoradiotherapy group during , and in the first year after , treatment . implications of all the available evidence combined adjuvant chemotherapy and radiotherapy cannot be recommended as a new standard of care for patients with stage iii endometrial cancer because no survival differences were found and pelvic control was high with radiotherapy alone . 
patients with stage iii cancer had the greatest benefit with chemoradiotherapy because of their higher risk of disease recurrence ; for these patients , combined treatment should be considered to maximise failure - free survival . 
 nevertheless , the benefits and risks should be discussed for each individual patient . introduction the majority of women with endometrial cancer present with early - stage disease and have a favourable prognosis . 
 about 15% of women with endometrial cancer are diagnosed with high - risk disease , which comprises endometrioid endometrial cancer stage i , grade 3 with deep invasion or with lymph - vascular space invasion ( lvsi ) , stage ii or iii endometrioid endometrial cancer , or non - endometrioid ( serous or clear cell ) histology . 
women with high - risk endometrial cancer are at increased risk of distant metastases and cancer - related death.14 serous and clear cell cancers have a higher risk of aggressive spread and a worse prognosis ; however , in the early stages they have similar outcomes to grade 3 endometrioid endometrial cancer.5 pelvic external beam radiotherapy has been the standard adjuvant treatment for women with high - risk endometrial cancer for many decades , although there is a improvement of survival . 
 radiotherapy was shown to delay pelvic recurrence and chemotherapy was shown to delay distant metastases , but no differences in survival were found . external beam compared have 296 vol 19 march 2018 articles correspondence to : dr stephanie m de boer , department of radiation oncology , leiden university medical center , 2333 za leiden , netherlands s.m.de_boer.onco@lumc.nl see online for appendix for the study protocol see because increased incidence of pelvic relapse has been reported with chemotherapy alone , the combination of external beam radiotherapy with chemotherapy has been explored . 
in a phase 2 trial ( rtog 9708 ) 8 among women with high - risk endometrial cancer , the combination of external beam radiotherapy with two concurrent cycles of cisplatin , followed by four adjuvant cycles of cisplatin and paclitaxel , was tested , resulting in 4 - year overall survival of 85% and disease - free survival of 81% . the combination of because radiotherapy and seemed more ( chemoradiotherapy ) chemotherapy effective than either treatment alone , and because data for toxicity and quality of lacking , the randomised portec - 3 trial was initiated to evaluate the benefit of chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer in terms of overall survival and failure - free survival improvement , as well as toxicity and effects on health - related quality of life . 
analysis of 2 - year toxicity and health - related quality of life in the portec - 3 trial showed significantly higher rates of adverse events and reduced health - related quality of life during and after chemoradiotherapy treatment , with rapid recovery thereafter.9 life were here , we present the final analysis of the primary survival endpoints of the portec - 3 trial . methods study design and participants portec - 3 was an open - label , randomised , phase 3 trial at 103 centres ( oncology centres , university hospitals , regional hospitals , or radiation oncology centres with referrals from regional hospitals ) in six clinical trial groups collaborating in the gynaecological cancer intergroup . 
participating groups were the national cancer research institute ( ncri ; uk ) , australia and new zealand gynaecologic oncology group ( anzgog ; australia and new zealand ) , mario negri gynaecologic oncology group ( mango ; italy ) , canadian cancer trials group ( cctg ; canada ) , and fedegyn ( france )  . stage ( parametrial ( figo ) 2009 patients were eligible if they had endometrial cancer with either international federation of gynecology and 1a endometrioid obstetrics endometrial cancer grade 3 with documented lvsi ; stage ib endometrioid endometrial cancer grade 3 ; stage ii endometrioid endometrial cancer ; stage iiia , iiib invasion ) , or iiic endometrioid endometrial cancer ; or serous or clear - cell histology endometrial cancer with stages ia ( with invasion ) , ib , ii , or iii . 
eligibility also included who performance score 02 ; adequate bone marrow function ( white blood cells 30 10 / l , platelets 100 10 / l ) , function ( bilirubin 15 upper normal limit [ unl ] , aspartate amino transferase aminotransferase 25 unl ) , kidney function ( creatinine clearance > 60 ml per min calculated according to cockroft and gault10 or > 50 ml per min edta clearance ) , and aged 18 years or older ( without an upper age limit , because elderly women alanine liver and might benefit from the study treatment if deemed fit enough to undergo chemotherapy )  . 
exclusion criteria were uterine ( carcino ) sarcoma ; malignancy in the 10 years before diagnosis of endometrial cancer ; previous pelvic radiotherapy , hormonal therapy , or chemotherapy ; bulky cervical involvement with radical hysterectomy ; inflammatory bowel disease ; residual macroscopic tumour ; impaired renal or cardiac function ; grade 2 or worse neuropathy ; grade 3 or worse hearing impairment ; or congenital hearing disorder . surgery comprised total abdominal or laparoscopic hysterectomy with bilateral salpingo - oophorectomy . 
 lymphadenectomy , whether systemic or sampling , was left to the discretion of participating centres , while lymph node debulking and para - aortic lymph - node sampling were recommended in cases of macroscopic positive pelvic nodes or para - aortic nodes ( or both )  . 
lymphadenectomy was not mandated in view of the lack of improvement in overall or progression - free survival in early - stage disease and its associated toxicity , mainly lymph oedema.11 , 12 for high - risk disease , the value of lymphadenectomy debated , 13 and the international statec trial14 has been initiated to address this issue . 
central pathology review by the groups reference gynaecopathologists was required before randomisation to confirm patients ' final suitability for study entry . to direct adjuvant treatment written informed consent was obtained from all patients . 
treatment was allocated with a biased - coin minimisation procedure , ensuring balance overall and within each stratum of the stratification factors ( participating centre , lymphadenectomy , stage of cancer , and histological type )  . 
 investigators were not masked to participants and treatment allocation . procedures central pathology review was done by reference gynaecopathologists ( as appointed by each participating group before the start of the trial ) to determine final eligibility . 
in case of serosal breach , metastases in the stroma of the fallopian tubes , in the ovaries , or on the peritoneal surface of the tubes or ovaries ( or both ) , the stage was defined as iiia . 
after determination of eligibility and patient consent , a tumour sample was centrally stored for future translational research . external beam pelvic radiotherapy was given in both treatment groups to a total dose of 486 gy in 18 gy fractions , 5 days a week . 
the clinical target volume was extended to include the aortic bifurcation in case of iliac lymph node involvement ; to include the lower peri - aortic region for common iliac node involvement ; and to include the higher para - aortic region in case of para - aortic involvement ( with a margin of 2 cm above the highest involved lymph node )  . 
 brachytherapy dose was equivalent to 14 gy in 2 gy fractions ( with recommended scheme of 10 gy high - dose rate [ hdr ] in fractions of 5 gy ) , specified at 5 mm from the vaginal vault surface . 
most patients were treated with a four - field technique ; use of intensity - modulated radiotherapy was allowed for centres per approval by their groups principal investigator . treatment was recommended to start within 46 weeks of surgery , but no later than 8 weeks . 
however , the trans - tasman radiation oncology group ( trog ) initiated a bench - marking and quality assurance programme for the anzgog group , 16 and in 2012 , a protocol amendment allowed a short quality - assurance programme to be activated for all other participating sites , with independent review of a single radiotherapy plan for each site . patients in the chemoradiotherapy group received two cycles of intravenous cisplatin 50 mg / m in the first and fourth week of external beam pelvic radiotherapy , followed by four cycles of intravenous carboplatin auc5 and paclitaxel 175 mg / m at 21 - day intervals . 
this schedule was based on the rtog - 9708 trial , 8 with substitution of cisplatin by carboplatin in the adjuvant phase to reduce toxicity and in view of the use of carboplatinpaclitaxel chemotherapy in metastatic disease.17 adjuvant chemotherapy was to be started within 3 weeks after completion of external beam pelvic radiotherapy , and with a 28 - day interval from the second concurrent cycle . 
details on chemotherapy stopping rules have been described previously.9 at each follow - up , patient history was taken with emphasis on toxicities and symptoms of recurrent disease , and physical and pelvic examination were done . 
long - term follow - up ( by hospital visit or information from the general practitioner ) was required at 7 years and 10 years . outcomes the coprimary endpoints were overall survival and failure - free survival . 
failure - free survival ( defined as any relapse or death related to endometrial cancer or treatment ) was defined as time from randomisation to date of first failure - free survival event . 
abdominal recurrences outside the pelvic area ( peritoneal carcinomatosis , liver , and para - aortic lymph nodal metastases ) were considered distant metastases , with specification of site . toxicity was assessed and graded with common terminology criteria for adverse events ( ctcae ) version 3.018 at baseline ( after surgery ) , at completion of radiotherapy , after each chemotherapy cycle , at 6 - month intervals from randomisation until 5 years , and at 7 years 298 vol 19 march 2018 articles and 10 years . 
for evaluation of mild ( grade 1 ) toxicities , patient - reported health - related quality - of - life symptoms were used because patient reporting of grade 1 toxicities was considered most reliable.19 serious adverse events had to be reported within 24 h , specifying adverse event grade and whether or not they were associated with study treatment . statistical analysis the portec - 3 trial was powered ( 80% ) to detect a 10% difference in 5 - year overall survival ( increase from 65% to 75% ; hazard ratio [ hr ] 067 ) , with a two - sided value of 005 . 
power calculation of the coprimary endpoint failure - free survival was based on the same principles as overall survival . the first prespecified interim analysis was done after 48 overall survival events ( a third of the required events ) had occurred in september , 2013 , only 3 months before reaching complete accrual . 
in october , 2016 , we decided , with permission from the data safety monitoring board ( dsmb ) , not to do the prespecified second interim analysis at two - thirds of overall survival events , because this would have no consequences for the trial and would reduce - spending . 
for analysis of the coprimary endpoints , failure - free survival with a overall survival and correlation between the test - statistics of the coprimary endpoints of 07859 ( based on 136 overall survival events and 186 failure - free survival events ) , a nominal of 00309 was used for each of the analyses , resulting in an overall level of 00498.20 because deaths in the portec - 3 trial were lower than expected at the time of trial design , the required number of overall survival events was not expected to be reached before late 2018 . 
for these reasons , the dsmb approved the final analysis becoming time - based rather than event - based , with final analysis at a median follow - up of 5 years and 42 months additional follow - up after inclusion of the last patient . 
for analysis of failure - free survival and recurrence , competing - risk methods were used.23 for failure - free survival , intercurrent death was used as a competing risk . 
the median follow - up was estimated with the reverse kaplan meier method . regression with this study is registered with isrctn , number and clinicaltrials.gov , number isrctn14387080 nct00411138 . role of the funding source the funding bodies had no role in study design , data collection , data interpretation , data analysis , or writing of this report . 
the central data manager ( kwv ) , the chief investigator ( clc ) , the associated investigators ( smdb , ran ) , and the trial statistician ( hp ) had full access to all the data . 
the corresponding author and chief investigator had full access to all the data and the final responsibility to submit for publication . results between nov 23 , 2006 , and dec 20 , 2013 , 686 women were enrolled and randomly assigned to chemoradiotherapy ( n = 343 ) or radiotherapy ( n = 343 )  . 
660 patients were included 686 patients enrolled and randomly assigned 343 randomly assigned to radiotherapy 343 randomly assigned to chemoradiotherapy 13 excluded 4 withdrew informed consent 9 did not meet eligibility criteria 13 excluded 9 withdrew informed consent 4 did not meet eligibility criteria 330 assigned to radiotherapy 328 received allocated treatment 2 received chemoradiotherapy 330 assigned to chemoradiotherapy 325 received allocated treatment 5 received radiotherapy only 660 patients in intention - to - treat population 330 in the radiotherapy group 330 in the chemoradiotherapy group figure 1 : trial profile vol 19 march 2018 articles in in the primary analysis ( chemoradiotherapy , n = 330 ; radiotherapy , n = 330 )  . 
median follow - up was 602 months ( iqr 481731 ) overall and was 600 months ( 478731 ) the chemoradiotherapy group and 607 months ( 487729 ) in the radiotherapy group . 
 there were seven major protocol violations : in the chemoradiotherapy group , five patients refused chemotherapy and received radiotherapy only ; in the radiotherapy group , two patients asked to switch to chemoradiotherapy ( figure 1 )  . chemoradiotherapy ( n = 330 ) radiotherapy alone ( n = 330 ) age at randomisation ( years ) 624 ( 565679 ) 620 ( 558682 ) patient characteristics were well balanced between the treatment groups ( table 1 )  . 
lymphadenectomy , lymph node sampling , or full surgical staging were done in 190 patients ( 58% ) 192 patients ( 58% ) in the radiotherapy group . chemoradiotherapy group and the radiotherapy was discontinued in one patient ( < 1% ) in the chemoradiotherapy group because of disease progression and five patients ( 15% ) in the radiotherapy group because of toxicity ( table 1 )  . 
329 ( 100% ) of 330 patients in the chemoradiotherapy group and 322 ( 98% ) of 330 patients in the radiotherapy group received an external beam pelvic radiotherapy dose between 450 and 504 gy . 
 ( table 1 continues on next column ) table 1 : patient , tumour , and treatment characteristics 300 vol 19 march 2018 articles 309 ( 47% ) patients ( 151 [ 46% ] chemoradiotherapy patients vs 158 [ 48% ] radiotherapy patients )  . 
apart from the protocol indication for brachytherapy boost ( cervical invasion ) , 28 ( 4% ) patients received a brachytherapy boost for locally perceived reasons such as lvsi , grade 3 , or stage iii . chemotherapy was both cycles of concurrent cisplatin were completed by 304 ( 92% ) of 330 patients in the chemoradiotherapy group . 
adjuvant started by 304 ( 92% ) patients , while 262 ( 79% ) patients completed all four cycles of carboplatin and 233 ( 71% ) patients completed all four cycles of paclitaxel ( table 1 )  . 
at least one dose reduction of cisplatin ( to 40 mg / m ) was recorded for five ( 2% ) patients , of carboplatin ( from auc5 to auc4 ) for 36 ( 11% ) patients , and of paclitaxel ( from 175 mg / m to 135 mg / m ) for 50 ( 15% ) patients . 
 chemotherapy was discontinued in 61 ( 18% ) patients ; in 31 ( 9% ) because of toxicity , patient decision in 20 ( 6% ) , disease progression in seven ( 2% ) , and for other reasons in three ( 1% )  . evaluation of the trog quality assurance programme for the anzgog group showed that a radiotherapy benchmarking exercise before participation in the trial ensured high conformity and low rates of both minor and major contouring deviations.16 evaluation of radiotherapy plans from centres in other countries is ongoing and will be reported separately . at final database lock on may 1 , 2017 , 136 patients had died ( 61 in the chemoradiotherapy group and 75 in the radiotherapy group ) and 186 patients had a failure - free survival event ( 83 in the chemoradiotherapy group and 103 in the radiotherapy group )  . 
among the patients assigned to chemoradiotherapy , 50 ( 82% ) had died from endometrial cancer , four ( 7% ) from a second cancer , three ( 5% ) from other intercurrent disease , and two ( 3% ) from treatment for metastatic disease . 
for the remaining four patients ( two patients treated with chemoradiotherapy and two patients with radiotherapy ) , the cause of death was uncertain one patient in the radiotherapy group , death was due to either disease progression or late treatment complications ; in two patients in the chemoradiotherapy group and one in the radiotherapy group , death was due to either intercurrent disease or late treatment - related toxicity . 
 these four deaths were counted as failure - free survival events after discussion with the dsmb . estimated overall survival adjusted for stratification factors at 5 years was 818% ( 95% ci 775862 ) for patients the chemoradiotherapy group versus 767% ( 721816 ) for patients in the radiotherapy group ( hr 076 , 95% ci 054106 ; p = 0109 ; table 2 , figure 2 )  . 
 5 - year failure - free survival was 755% ( 703799 ) in the chemoradiotherapy group versus 686% ( 631734 ) in the radiotherapy group ( hr 071 , 053095 ; p = 0022 )  . 
 without adjusting for the stratification factors , the hr events 5 - year estimate , % ( 95% ci ) hazard ratio ( 95% ci ) p value 076 ( 054106 ) 071 ( 053095 ) 0109 0022 overall survival * failure - free survival * overall survival chemoradiotherapy radiotherapy failure - free survival chemoradiotherapy radiotherapy chemoradiotherapy radiotherapy chemoradiotherapy radiotherapy vaginal recurrence ( first recurrence ) pelvic recurrence ( first recurrence ) distant metastases ( first recurrence ) chemoradiotherapy radiotherapy vaginal recurrence ( total ) chemoradiotherapy radiotherapy pelvic recurrence ( total ) chemoradiotherapy radiotherapy distant metastases ( total ) chemoradiotherapy radiotherapy 818% ( 775862 ) 081 ( 058113 ) 0213 767% ( 721816 ) 755% ( 703799 ) 076 ( 057102 ) 0067 686% ( 631734 ) 03% ( 0021 ) 099 ( 0061590 ) 0999 10% ( 0329 ) 060 ( 014249 ) 0473 03% ( 0021 ) 15% ( 0636 ) 21% ( 1044 ) 92% ( 65129 ) 224% ( 181274 ) 078 ( 058106 ) 0108 283% ( 237337 ) 21% ( 1044 ) 099 ( 037265 ) 0995 49% ( 3079 ) 051 ( 028092 ) 0026 231% ( 188283 ) 077 ( 057103 ) 0077 297% ( 249351 ) * data are chemotherapy versus radiotherapy ( cox - adjusted p value ) , adjusted for stratification factors : participating groups , type of surgery ( abdominal hysterectomy and salpingo - oophorectomy vs abdominal surgery plus lymphadenectomy vs laparoscopic procedure vs laparoscopic procedure plus lymphadenectomy ) , stage ( figo 2009 ia vs ib vs ii vs iii ) , and histological type ( endometrioid carcinoma vs serous or clear cell carcinoma )  . 
 table 2 : survival and recurrence outcomes for overall survival was 081 ( 95% ci 058113 ; p = 0213 ) and for failure - free survival was 076 ( 057102 ; p = 0067 ; table 2 , figure 2 )  . in subgroup analysis , women with stage iii lower overall endometrial cancer had significantly survival and failure - free survival than those with stage iii disease ( tables 3 , 4 )  . 
5 - year overall survival for stage iii cancer was 787% ( 95% ci 722857 ) in the chemoradiotherapy group versus 698% ( 624781 ) in the radiotherapy group ( hr 071 , 95% ci 045111 ; p = 013 ; adjusted p = 0074 )  . 
5 - year failure - free survival for stage iii cancer was 693% ( 95% ci 611762 ) in the chemoradiotherapy group versus 580% ( 493657 ) in the radiotherapy group ( hr 066 , 95% ci 045097 ; p = 0031 ; adjusted p = 0014 ; figure 2 )  . 
5 - year failure - free survival for stage iii patients was 808% ( 741860 ) in the chemoradiotherapy group versus 766% ( 695822 ) in the radiotherapy group ( 085 , 054133 ; p = 047 )  . serous cancers ( > 25% serous component ) had lower overall survival and failure - free significantly vol 19 march 2018 articles number at risk ( number censored ) radiotherapy chemoradiotherapy pcox - adjusted = 011 plog - rank = 021 , hr 076 ( 95% ci 054106 ) pcox - adjusted = 0022 plog - rank = 0067 , hr 071 ( 95% ci 053095 ) ( 11 ) ( 18 ) ( 60 ) ( 71 ) ( 123 ) ( 130 ) ( 10 ) ( 16 ) ( 50 ) ( 63 ) ( 105 ) ( 120 ) radiotherapy chemoradiotherapy number at risk ( number censored ) radiotherapy chemoradiotherapy pcox - adjusted = 0074 plog - rank = 013 , hr 071 ( 95% ci 045111 ) pcox - adjusted = 0014 plog - rank = 0031 , hr 066 ( 95% ci 045097 ) time since randomisation ( years ) time since randomisation ( years ) ( 23 ) ( 26 ) ( 53 ) ( 52 ) ( 18 ) ( 23 ) ( 44 ) ( 50 ) figure 2 : overall survival and failure - free survival kaplan - meier survival curves for overall survival ( a ) and failure - free survival ( b ) in all patients , and for overall survival ( c ) and failure - free survival ( d ) of patients with stage iii endometrial cancer . 
the number of patients and events are , however , small in these subgroups ( appendix p 3 )  . isolated vaginal and pelvic recurrences were rare , with isolated vaginal recurrence diagnosed in one ( < 1% ) patient in the chemoradiotherapy group and in one ( < 1% ) patient in the radiotherapy group ( p = 0995 ) , and isolated pelvic in the chemorecurrence in three ( 1% ) patients radiotherapy group versus five ( 2% ) patients in the radiotherapy group ( p = 0473 )  . 
most recurrences were distant metastases : 76 ( 22% ) patients in the chemoradiotherapy group versus 93 ( 28% ) patients in the radiotherapy group were diagnosed with distant metastases ( p = 0108 )  . 
the 5 - year estimate of pelvic recurrence ( both isolated and combined pelvic and distant recurrences ) was 49% ( 95% ci 3079 ) for the chemoradiotherapy group versus 92% ( 65129 ) for the radiotherapy group ( p = 0026 ; table 2 )  . in the multivariable analysis , the following covariates were included together with treatment : stage , histological type and grade , type of surgery , participating groups , lvsi , and age . 
most factors , except lymphadenectomy , were significantly correlated with failure - free survival ( table 4 )  . in multivariable analysis for failure - free survival , only age group was found to be predictive of treatment effect , with a strong treatment - by - age effect ( pinteraction = 0012 , figure 3 )  . 
women aged 70 years or older had the greatest benefit from chemoradiotherapy . grade 2 or worse adverse events were reported during treatment in 308 ( 93% ) women in the chemoradiotherapy group versus 144 ( 43% ) in the radiotherapy group , and grade 3 or worse in 198 ( 60% ) versus 41 ( 12% ; p < 00001 ; table 5 ) ; the majority of grade 3 or worse adverse events were haematological . 
table 6 shows an overview of adverse events at 6 months after randomisation , which 302 vol 19 march 2018 articles was about 1 month after completion of treatment in the chemoradiotherapy group . 
the number of patients with grade 2 or worse adverse events was 86 ( 32% ) for chemoradiotherapy versus 64 ( 24% ) for radiotherapy at 3 years ( p = 0034 ) , and 57 ( 40% ) versus 38 ( 28% ) at 5 years ( p = 0033 )  . 
the most significant and clinically relevant difference between the arms was found for grade 2 or worse sensory neuropathy , which persisted in 20 ( 8% ) women in the chemoradiotherapy group versus one ( 1% ) women in the radiotherapy group at 3 years and 12 ( 9% ) women versus no women at 5 years ( both p < 00001 )  . 
an extensive overview of adverse events during follow - up is in the appendix ( pp 45 )  . improve overall discussion the final results of the portec - 3 trial showed that the combination of adjuvant chemotherapy and radiotherapy for high - risk endometrial cancer did not significantly survival . 
patients with stage iii diseasewho had a higher risk of recurrence than those with stages iiihad a hr of 066 and 11% absolute improvement of failure - free survival with chemo - radiotherapy , which is clinically relevant and exceeds the 10% improvement used when designing the study . the improvement in failure - free survival in the chemoradiotherapy group should be weighed against the severity and duration of toxicity of combined treatment , especially since overall survival was not significantly improved . 
although significantly higher incidences of adverse events and reduced health - related quality of life were reported in the chemoradiotherapy group during and after treatment , 9 rapid recovery was seen , with no differences in grade 34 adverse events from 12 months onwards . 
grade 2 sensory neuropathy , however , persisted significantly more often treated with chemoradiotherapy , with 25% of patients reporting quite a bit or very much tingling or numbness at 2 years , compared with 6% for radiotherapy.9 sensory neuropathy is associated with lower levels of functioning and quality of life , and more fatigue.24 in patients for decades , standard adjuvant treatment for women with high - risk endometrial cancer has been pelvic external beam radiotherapy . 
randomised trials comparing adjuvant chemotherapy with external beam radiotherapy failed progression - free survival.6 , 7 retrospective studies reported substantial rates of pelvic recurrence if high - risk patients were treated without radiotherapy , supporting the combined use of pelvic to show an improvement survival overall patients events 5 - year overall survival ( 95% ci ) hazard ratio ( 95% ci ) p value total 79% ( 748839 ) chemoradiotherapy 82% ( 775862 ) 073 ( 052103 ) 77% ( 721816 ) treatment group radiotherapy age ( years ) 6069 stage stage i and ii stage iii histology and grade endometrioid grade 1 and 2 endometrioid grade 3 serous / clear cell lvsi lymphadenectomy 89% ( 850929 ) 75% ( 696806 ) 231 ( 148359 ) 67% ( 587763 ) 329 ( 199544 ) 83% ( 791873 ) 74% ( 693797 ) 86% ( 819909 ) 241 ( 166351 ) 79% ( 730857 ) 71% ( 652774 ) 176 ( 110281 ) 235 ( 148372 ) 85% ( 805894 ) 75% ( 709799 ) 136 ( 093198 ) 77% ( 714821 ) 81% ( 771852 ) 082 ( 055122 ) 0075 < 00001 < 00001 < 00001 011 033 adjusted for participating groups . 
lvsi = lymph - vascular space invasion . table 3 : multivariable analysis of prognostic factors for overall survival radiotherapy with adjuvant chemotherapy , as first explored in the rtog 9708 phase 2 trial.8 , 25 , 26 randomised studies have compared radiotherapy with the combination of chemotherapy and radiotherapy in patients with high - risk endometrial cancer . 
the nsgo - ec - 9501 / eortc - 55991 trial compared external beam radiotherapy alone with external beam radiotherapy and four cycles of platinum - based chemotherapy , given sequentially before or after external beam radiotherapy . 
 a pooled analysis with the mango iliade 3 trial27 with a total cohort of 534 patients showed , in line with our results , improved progression - free survival ( 78% vs 69% , p = 001 ) and a trend for improved survival ( 82% vs 75% , p = 007 ) with the addition of chemotherapy to radiotherapy alone . the schedule of combined radiotherapy with concurrent and adjuvant chemotherapy used in the portec - 3 trial seemed likely to be most effective because both treatments were started early after surgery and thus maximum benefit of the combination could be expected . 
a retrospective single institution study28 reporting on 40 patients with stage iiia or iiic endometrial cancer treated with the same combination of chemoradiotherapy showed 5 - year overall survival of 85% and relapse - free survival of 79% . 
 in the chemoradiotherapy group of the portec - 3 trial the 5 - year overall survival probability was 82% and the thus survival probability was failure - free 76% , vol 19 march 2018 articles patients events 5 - year failure - free survival ( 95% ci ) hazard ratio ( 95% ci ) p value total 72% ( 667767 ) 68% ( 631734 ) 75% ( 703799 ) 81% ( 753850 ) 67% ( 607724 ) 64% ( 544717 ) 79% ( 739826 ) 64% ( 580692 ) 78% ( 727831 ) treatment group radiotherapy chemoradiotherapy age ( years ) 6069 stage stage i and ii stage iii histology and grade endometrioid grade 1 and 2 lvsi lymphadenectomy 068 ( 051091 ) 174 ( 123246 ) 214 ( 141325 ) 262 ( 190361 ) 0010 < 00001 < 00001 < 00001 0054 041 77% ( 714818 ) 68% ( 634729 ) 136 ( 099187 ) 72% ( 657766 ) 72% ( 674767 ) 087 ( 061122 ) endometrioid grade 3 serous or clear cell 71% ( 645771 ) 64% ( 566704 ) 156 ( 106230 ) 215 ( 146316 ) adjusted for participating groups . 
overall and relapse - free survival in the pooled nsgo - ec - 9501 / eortc - 55991 / iliade trials27 were also similar at 82% and 78% , with only 20% patients with stage iii disease . trials in chemotherapy high - risk endometrial cancer is heterogeneous , including various histological types and stages of disease . 
 in the nsgo - ec - 9501 / eortc - 55991 trial , although progression - free survival was significantly improved for patients with endometrioid endometrial cancer , this improvement was not found for serous and clear cell cancers . 
in the portec - 3 trial , women with serous or clear - cell cancers had at least as much improvement in failure - free survival with the addition of chemotherapy as women with endometriod endometrial cancer did . 
when comparing serous cancers with other histological types , as expected , worse overall survival and failure - free survival were found for serous cancers ; patients with serous cancers had a failure - free survival benefit with chemoradiotherapy , but this benefit was not significant in view of the small numbers of serous cancers and events . the multivariable analysis indicated that women older than 70 years seemed to have a greater failure - free survival benefit from chemotherapy than younger women . 
age is a well - known risk factor for endometrial cancer and a greater benefit of chemotherapy in older women has been reported previously.7 , 30 although selection of fitter older women in this randomised trial might have occurred , physicians should not be reticent to counsel older women about the possible benefits of combined chemotherapy and radiotherapy . analysed by stage , patients with stage iii endometrial cancer who have the highest frequency of recurrence , also had the greatest absolute benefit from the combined treatment . 
the smaller failure - free survival improvement for patients with stage iii disease seems not to outweigh the cost in terms of toxicity and quality - of - life impairment . 
 this finding is in line with the results of the gog - 249 trial , in which patients with stage i and ii endometrial cancer with high - intermediate or high - risk factors were randomly assigned to pelvic radiotherapy alone or to chemotherapy ( three cycles of carboplatin and paclitaxel ) followed by vaginal brachytherapy . 
no superiority of three cycles chemotherapy plus vaginal brachytherapy over external bean radiotherapy alone was found , with overlapping progression - free and overall survival curves and significantly more pelvic and para - aortic recurrences in the chemotherapy group.31 , 32 the majority because of in 47% of all patients , a vaginal brachytherapy boost was given ( 46% for chemoradiotherapy vs 48% for radiotherapy ) ; cervical involvement and 4% because of other reasons , such as lvsi or grade 3 endometrial cancer . 
this finding is in line with other studies among patients with stage iiiii endometrial cancer.33 although the addition of a brachytherapy boost might have added to the good local control seen in both groups , we do not expect this would have affected the results , because the proportion of women receiving a brachytherapy boost was equal in the two treatment groups . the portec - 3 to compare the radiotherapy and chemotherapy trial with schedule as used chemotherapy alone for advanced stage endometrial cancer , the gog - 258 trial randomly assigned participants to receive chemoradiotherapy or six cycles of carboplatin and paclitaxel.34 final results are pending , but a presented abstract34 reported no differences in overall or recurrence - free survival , while significantly more vaginal and pelvic or para - aortic recurrences were reported in patients treated with chemotherapy alone . 
furthermore , acute gastrointestinal and genitourinary toxicity of pelvic radiotherapy will be reduced with the current standard use of intensitymodulated radiotherapy.36 portec - 3 was a multicentre trial with strong international collaboration among six participating groups and , therefore , highly representative of current practice worldwide . 
 analysis of pathology review in the netherlands and the uk ( 48% of portec - 3 participants ) revealed that 83% of patients did not fulfil the eligibility criteria after central pathology review . 
these patients did not enter the trial.15 a limitation of this trial might be that because of the death and failure - free survival event rates were lower than expected at the time of trial design , the required number of overall survival events was not reached and the final analysis was time - based rather than eventbased , with final analysis at a median follow - up of 5 years ( 42 months after inclusion of the last patient )  . 
 the number of overall survival events was 136 ( 69% of the required number of overall survival events ) , and the number of failure - free survival events was 186 ( 94% of the required events )  . 
 long - term outcomes will be analysed , especially for overall survival . the costs of chemoradiotherapy in terms of toxicity and treatment duration should be weighed against the benefits , and this costbenefit tradeoff could be seen differently from the patient or physician perspective . 
in a patient preference study done by the anzgog group among portec - 3 participants , 37 more than 50% of patients rated 5% survival improvement sufficient to make chemotherapy worthwhile . 
although the trial results are in the range of this benefit for failure - free survival , the overall survival difference was not significant , thus individual patient counselling remains essential . 
translational studies of molecular risk factors and tumour characteristics with the tumour samples of the portec - 3 participants might identify those who could most benefit from chemotherapy or targeted agents and individualise treatment of women with highrisk endometrial cancer.38 vol 19 march 2018 articles in conclusion , although treatment with chemoradiotherapy significantly improved 5 - year failure - free survival for patients with high - risk endometrial cancer compared with radiotherapy alone , there was no significant difference in overall survival . 
for each patient , the cost in terms of increased toxicity and longer treatment duration should be weighed against the benefit in terms of improvement in failure - free survival . 
however , in view of the higher risk of recurrence among women with stage iii disease , this chemoradiotherapy schedule should be considered to maximise failure - free survival , and benefits and risks should be individually discussed . contributors clc was the chief investigator of the trial . 
all authors contributed to the manuscript and approved the final manuscript . declaration of interests we declare no competing interests . acknowledgments the portec - 3 study was supported by a grant from the dutch cancer society ( ul20064168 / ckto 200604 ; the netherlands )  . 
 participation in the portec - 3 trial by anzgog and trog were supported by the nhmrc project grant 570894 ( 2008 ) and by a cancer australia grant ( awarded through the 2011 round of the priority - driven collaborative cancer research scheme and funded by cancer australia )  . 
the portec - 3 trial involved a strong international collaboration within the gynaecological oncology intergroup ( gcig ) and the support of the gcig officers and member groups is gratefully acknowledged . 
this study was presented in part at the annual meeting of the american society of clinical oncology ( chicago , il , usa ; june 26 , 2017 )  . editorial for our earlier editorial on direct - to - consumer genetic testing see lancet oncol 2008 ; 9 : 1113 black - box warning : direct - to - consumer marketing on nov 22 , 2013 , the us food and drug administration ( fda ) ordered the company 23andme to immediately discontinue sale and marketing of its saliva collection kit and personal genome service , stating that it was being marketed without fda approval . 
23andme had recently begun a series of television adverts to market their test , which is billed as providing data on 254 diseases and conditions , including data on carrier status , health risk , and responses to drugs . 
the warning letter stated that the fda had received no assurances from the company that the personal genome service was analytically or clinically validated for its intended uses , and that the tests could put patients at risk when decisions are made on false positive or negative assessments for high - risk indications . 
for instance , the letter highlighted that a false positive result for a brcarelated risk assessment could lead a patient to undergo intensive prophylactic screening , or other morbidity - inducing actions , while a false negative result could result in a patient failing to recognise an actual risk that might exist . 
in response , 23andme have suspended marketing the product , and halted the provision of health - related results to new customers , although ancestry - related information and raw genetic data will still be provided . chemoprevention , surgery , these concerns are the crux of the issue with publicly available genetic tests . 
while genetic testing has a role in the clinic , the provision of complex genetic data to lay individuals , especially without access to expert genetic counselling , is a risky business . 
 further , it is premature to believe that we understand the overall genetic complexity of common diseases to the extent that we can accurately predict whether or not an individual will succumb to that condition in the long run . one must also consider what a consumer can actually do with the results of their genetic tests . 
although in a handful of situationseg , testing positive for brca1 / 2 with a strong family history of brca - related cancerradical steps can be taken to prevent or treat the disease , many conditions do not have such obvious courses of action . 
most frequently , the only possible recommendation for a patient would be to modify diet and lifestyle , but one could argue that this should be done by many people , irrespective of knowledge of their genetics . 
and would knowledge of the risk of an untreatable condition cause long - lasting anxiety , the adoption of a fatalistic attitude to bad news , or use of unproven interventions , perhaps at great personal expense ? as we have noted previously , is the ready availability of such information ethical , when little can be done with it , and could be the source of distress ? is also an instance , 23andmes database currently contains data for 400 000 people . 
 what guarantees does an individual have that this information will not nd its way to health insurers , resulting in in ated premiums or the refusal to grant coverage ? in an unauthorised data protection information issuefor to use inherent many of the fears raised by this particular issue are common to other direct - to - consumer marketed health products . 
 or is it perhaps time to ban outright product - speci c adverts of health - care products aimed directly at the consumer ? the lancet oncology vol 15 january 2014 corrections correction to lancet oncol 2015 ; 16 : 303 correction to lancet oncol 2016 ; 17 : 65 correction to lancet oncol 2016 ; 17 : e8 penson rt , huang hq , wenzel lb , et al . 
lancet oncol 2015 ; 16 : 30111in the 6 months post - cycle 1 section of table 1 of this article , in the received row of the second column ( headed cisplatin and paclitaxel plus bevacizumab ) , the data should have been 66 ( 57% )  . 
 bendamustine plus rituximab versus udarabine plus rituximab for patients with relapsed indolent and mantle - cell lymphomas : a multicentre , randomised , open - label , non - inferiority phase 3 trial . 
 lancet oncol 2016 ; 17 : 5766in this article , on page 65 , paragraph 6 , of the discussion section , reference 3 was incorrectly added to the sentence results of our published study8 in the rst - line setting . 
lancet oncol 2016 ; 17 : e8in paragraph two of this news piece , the percentage of genetic mutations in paediatric should have read 95 ( 85% ) of 1120 patients had genetic mutations in their normal tissue that increased their risk of developing cancer during childhood . 
 this correction has been made to the online version as of dec 22 , 2015 . vol 17 january 2016 catching up on medical device safety after a joint investigation into the global medical devices industry , several media outlets published their findings of the implant files in 2018 . 
elsewhere , non - clinical grade materials continue to be used in breast implants , despite the 2010 pip scandal in which implants were found to be manufactured with unapproved silicone gel and were prone to rupture . 
although reports have now emerged of an alarming association between textured breast implants and the development of breast large - cell implant - associated anaplastic lymphomaa rare form of t - cell lymphoma that can occur in the fibrous scar capsule that forms around breast the underlying causal mechanisms have yet to be defined , early detection of localised disease and complete removal of the implant and capsule can lead to recovery . 
meanwhile , cases of breast implant - associated anaplastic large - cell lymphoma are increasing : 615 cases have been reported worldwide since the first report in 1997 , including 45 cases in the uk , 72 in australia , and 252 in the usa . 
the concern is so great that the french national agency for medicines and health products has recommended that surgeons switch to smooth implants as the link between textured implants and anaplastic large - cell lymphoma is investigated . for any woman undergoing mastectomy to treat breast cancer , the possibility of developing another cancer because of a medical device must be devastating . 
but , as for any medical procedure , blame cannot , and should not , be apportioned to the patient , especially when risks are not adequately recorded and reported , let alone communicated to the patient . 
data for anaplastic largecell lymphoma are scarce , highlighting a wider concern about the worldwide regulation of medical devices . many countries have systems in places for reporting adverse events associated with medical devices . 
however , such systems do not appear to be compulsoryfor example , the uk registry is not mandatory for clinicians and although large - cell lymphoma as a data item , reporting cases is optional . 
how can clinicians be expected to communicate risks to patients or make clinical decisions without accurate and reliable data ? the existing system of passive monitoring of medical device safety clearly needs to be addressed . include anaplastic it does drug safety monitoring could be a good model for the medical device industry and provide more reassurance to doctors and patients alike . 
reporting of clinical trial data on new drugs has improved , and data from robust trials , including full reporting of adverse events , are essential for any drug approval . 
the same stringent data are not needed for medical devices ; for example , in the european economic area , market approval is granted through ce certification , for which clinical trial data are not mandatory . 
similarly , a new eu regulation on medical devices , due to come into force in 2020 , includes key issues of transparency around medical devices and reinforcement of rules of clinical evidence . the steps taken by the fda and the eu are a good start in a long overdue assessment of medical devices , which undoubtedly hold much promise for many patients . 
 the lancet oncology for the implant files see investigations / implant - files / for safety concerns of breast implants see theguardian.com / society / 2018 / nov / 26 / breast - implants - studyreveals - serious - safety - concerns for more on the pip scandal see pip - implants / for reports on breast implantassociated anaplastic large cell lymphoma see theguardian.com / society / 2018 / nov / 26 / rare - cancer - linkedbreast - implant - used - bymillions - women - lymphoma for the maude database see scripts / cdrh / cfdocs / cfmaude / search.cfm for the australian registry see for the uk registry see information / clinical - audits - andregistries / breast - and - cosmetic - implantregistry for the us action plan see centersoffices / officeofmedical productsandtobacco / cdrh / cdrhreports / ucm604500.htm for the eu regulation see sectors / medical - devices / regulatory - framework_en vol 20 january 2019 editorial correction to lancet oncol 2017 ; 18 : e35463 correction to lancet oncol 2018 ; 19 : 87100 correction to lancet oncol 2018 ; 19 : 25766 oconnor oa , lue jk , sawas a , et al . 
 for lancet oncol 2017 ; 18 : e35463 in this review , the second sentence of the abstract should read additional improvements have been reported in three phase 3 colon cancer trials when oxaliplatin was added to fluoropyrimidines , the effect was mainly on disease - free survival . 
this correction has been made to the online version as of feb 28 , 2018 although women fulvestrant johnston s , lee ks , et di leo a , al . 
buparlisib plus with postmenopausal her2hormone - receptor - positive , negative , advanced breast cancer progressing on or after mtor inhibition ( belle - 3 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
in the results section , the following sentence should have read in the 11 ( 13% ) cases of discordance , a pik3ca wild - type tumour sample and pik3ca - mutated ctdna were reported in three ( 4% ) patients and pik3ca mutations detected in the tumour sample but not in ctdna ( 9% ) patients . 
these corrections have been made to the online version as of feb 28 , 2018 . seven vol 19 march 2018 e137 corrections correction to lancet oncol 2019 ; 20 : 193201 correction to lancet oncol 2020 ; 21 : 796807 correction to lancet oncol 2020 ; 21 : 130916 li x , zhang s , zhang q , et al . 
lancet oncol 2019 ; 20 : 193201in this article , the number of patients with thyroid cancer and non - thyroid cancer in the tianjin , jilin , and weihai validation sets listed in figure 1 have been corrected . 
these corrections have been made to the online version as of sept 28 , 2020 . published online september 3 , 2020 s1470 - 2045 ( 20 ) 30531 - 3 aboualfa gk , macarulla javle mm , et al . 
 lancet oncol 2020 ; 21 : 796807 in this article , in figure 4a , the colour for the eleventh patient from the bottom of the figure should be amended from unknown ( purple ) to not evaluable ( light blue )  . 
these corrections have been made to the online version as of sept 3 , 2020 , and will be made to the printed version . vol 21 october 2020 e462 corrections gemcitabine and docetaxel versus doxorubicin as first - line treatment in previously untreated advanced unresectable or metastatic soft - tissue sarcomas ( geddis ) : a randomised controlled phase 3 trial beatrice seddon , sandra j strauss , jeremy whelan , michael leahy , penella j woll , fiona cowie , christian rothermundt , zoe wood , charlotte benson , nasim ali , maria marples , gareth j veal , david jamieson , katja kver , roberto tirabosco , sharon forsyth , stephen nash , hakim - moulay dehbi , sandy beare summary background for many years , first - line treatment for locally advanced or metastatic soft - tissue sarcoma has been doxorubicthis study compared gemcitabine and docetaxel versus doxorubicin as first - line treatment for advanced or metastatic soft - tissue sarcoma . methods the geddis trial was a randomised controlled phase 3 trial done in 24 uk hospitals and one swiss group for clinical cancer research ( sakk ) hospital . 
eligible patients had histologically confirmed locally advanced or metastatic soft - tissue sarcoma of trojani grade 2 or 3 , disease progression before enrolment , and no previous chemotherapy for sarcoma or previous doxorubicin for any cancer . 
patients were randomly assigned 1 : 1 to receive six cycles of intravenous doxorubicin 75 mg / m on day 1 every 3 weeks , or intravenous gemcitabine 675 mg / m on days 1 and 8 and intravenous docetaxel 75 mg / m on day 8 every 3 weeks . 
the trial was registered with the european clinical trials ( eudract ) database ( no 200901490729 ) and with the international standard randomised controlled trial registry ( isrctn07742377 ) , and is now closed to patient entry . findings between dec 3 , 2010 , and jan 20 , 2014 , 257 patients were enrolled and randomly assigned to the two treatment groups ( 129 to doxorubicin and 128 to gemcitabine and docetaxel )  . 
 the proportion of patients alive and progression free at 24 weeks did not differ between those who received doxorubicin versus those who received gemcitabine and docetaxel ( 463% [ 95% ci 375546 ] vs 464% [ 375548 ] ) ; median progression - free survival ( 233 weeks [ 95% ci 196304 ] vs 237 weeks [ 181200 ] ; hazard ratio [ hr ] for progressionfree survival 128 , 95% ci 099165 , p = 006 )  . 
the most common grade 3 and 4 adverse events were neutropenia ( 32 [ 25% ] of 128 patients who received doxorubicin and 25 [ 20% ] of 126 patients who received gemcitabine and docetaxel ) , febrile neutropenia ( 26 [ 20% ] and 15 [ 12% ] ) , fatigue ( eight [ 6% ] and 17 [ 14% ] ) , oral mucositis ( 18 [ 14% ] and two [ 2% ] ) , and pain ( ten [ 8% ] and 13 [ 10% ] )  . 
154 ( 60% ) of 257 patients died in the intention - to - treat population : 74 ( 57% ) of 129 patients in the doxorubicin group and 80 ( 63% ) of 128 in the gemcitabine and docetaxel group . 
no deaths were related to the treatment , but two deaths were due to a combination of disease progression and treatment . interpretation doxorubicin should remain the standard first - line treatment for most patients with advanced softtissue sarcoma . 
these results provide evidence for clinicians to consider with their patients when selecting first - line treatment for locally advanced or metastatic soft - tissue sarcoma . funding cancer research uk , sarcoma uk , and clinical trial unit kantonsspital st gallen . copyright the author ( s )  . 
we identified six published randomised controlled trials , none of which showed a survival advantage for any schedule over single - agent doxorubicwe identified a further randomised controlled study comparing single - agent doxorubicin versus doxorubicin and ifosfamide chemotherapy , which was recruiting at that time , and which has since been published in 2014 , showing an advantage for the combination for progression - free survival but not overall survival . 
 although we identified three phase 2 studies ( one of which was a randomised phase 2 study comparing gemcitabine versus gemcitabine and docetaxel ) , we were unable to find any phase 3 trials comparing this combination with doxorubicin . added value of this study to our knowledge , this is the first randomised controlled trial that compares two commonly used treatmentsdoxorubicin versus gemcitabine and docetaxelas first - line treatment in advanced soft - tissue sarcoma . 
furthermore , planned subgroup analyses have not identified any subgroup for which gemcitabine and docetaxel was superior , and in particular we did not observe superiority for either leiomyosarcoma or uterine leiomyosarcoma , for which gemcitabine and docetaxel has previously been believed to be particularly active . 
we found worse treatment adherence with gemcitabine and docetaxel compared with doxorubicin , with more dose delays , lower dose intensity , and more patients stopping treatment early due to toxicity , and lower quality - of - life scores . implications of all the available evidence these results provide evidence for clinicians to consider with patients when selecting first - line treatment for advanced soft - tissue sarcoma . 
although the observed similar progression - free survival and overall survival of gemcitabine and docetaxel and doxorubicin might support a conclusion that either schedule can be used according to patient or clinician preference , our results indicate the need for caution with such an approach given the greater difficulty in delivery and toxicity of gemcitabine and docetaxel , and indeed the higher cost of this combination regimen . 
the data support the conclusion that doxorubicin should remain standard of care as first - line treatment for most patients with advanced soft - tissue sarcoma , and that there is no subgroup of patients for whom gemcitabine and docetaxel should be routinely recommended . introduction soft - tissue sarcoma comprises a number of rare malignancies , with 3298 patients newly diagnosed with the disease in the uk in 2010.1 surgery with radiotherapy is the most common treatment for localised disease , with associated 5 - year overall survival of 55% in 200610.1 survival outcomes for locally advanced or metastatic softtissue sarcoma are poor , with a median overall survival of 128143 months after diagnosis.2 , 3 doxorubicin has been used as first - line treatment for locally advanced or metastatic soft - tissue sarcoma for more than 40 years . 
a trial2 comparing randomised controlled phase 3 combination doxorubicin versus doxorubicin alone showed a significant increase in progression - free survival in the combination treatment group , but with no increase in overall survival . 
toxicity was predictably higher in the combination group , and the authors concluded their results do not support the use of intensified doxorubicin and ifosfamide for palliation of advanced soft - tissue sarcoma unless the specific goal is tumour shrinkage . 
subsequently , two first - line phase 3 trials4 , 5 have combined doxorubicin with novel agents ( doxorubicin and palifosfamide compared with doxorubicin and placebo , 4 and doxorubicin and evofosfamide compared with doxorubicin alone5 ) , and neither study ifosfamide and was able to show improved progression - free survival or overall survival for the combination treatments . 
thus , no regimen has proved to be unequivocally superior to doxorubicin as first - line treatment for locally advanced or metastatic soft - tissue sarcoma . gemcitabine and docetaxel was first reported as a treatment for locally advanced or metastatic soft - tissue sarcoma in 2002 . 
this study also compared plasma levels of gemcitabine achieved with a 90 - min infusion versus a 30 - min infusion , and showed that the 90 - min infusion was associated with a longer duration of plasma gemcitabine concentrations above 10 mol / l , which is the threshold for saturation of intracellular accumulation of the active form of the drug , gemcitabine triphosphate . 
a further retrospective review of gemcitabine and docetaxel in patients with locally advanced or metastatic disease included an in - vitro study to investigate the dosing sequence of gemcitabine and docetaxel , finding that gemcitabine followed by docetaxel was synergistic , whereas docetaxel followed by gemcitabine was antagonistic.7 hence , the currently used schedule of gemcitabine and docetaxel in locally advanced or metastatic soft - tissue sarcoma was established . 
subsequently , several 1398 vol 18 october 2017 articles retrospective studies and phase 2 studies , in both leiomyosarcoma811 and unselected soft - tissue sarcoma , 7 , 12 , 13 have all showed activity of the combination . 
the observed responsiveness of leiomyosarcoma in particular has led to some clinicians adopting gemcitabine and docetaxel as a first - line treatment option for locally advanced or metastatic leiomyosarcoma , in the absence of evidence from phase 3 trials . 
with increasing use of the combination in both leiomyosarcoma and locally advanced or metastatic softtissue sarcoma , robust evidence is needed to establish the roles of gemcitabine and docetaxel and doxorubicin as firstline treatments for this disease . the geddis trial aimed to compare the efficacy of gemcitabine and docetaxel versus doxorubicin in the firstline setting for locally advanced or metastatic soft - tissue sarcoma . 
a pharmacogenomics study was also done to investigate the influence of single - nucleotide polymorphisms ( snps ) on treatment efficacy and toxicity . methods study design and participants geddis was a multicentre , randomised , phase 3 trial , which recruited patients from 24 uk hospitals , and one swiss group for clinical cancer research ( sakk ) hospital in switzerland ( appendix p 1 )  . 
patients were required to have adequate organ function ( absolute neutrophil count 10 10 per l ; platelet count 100 10 per l ; bilirubin 15 upper limit of normal [ uln ] ; aspartate transaminase , alanine transaminase , or both 30 uln ; alkaline phosphatase 30 uln [ patients were eligible with a higher alkaline phosphatase concentration if this was shown to be due to bone isoenzyme ] ; measured or calculated creatinine clearance 30 ml / min ; and cardiac ejection fraction within local normal limits )  . 
tumour tissue was required to be available for central review . treatment delays patients were excluded from the trial if they had alveolar soft part sarcoma , gastrointestinal stromal tumour , ewings dermatofibrosarcoma sarcoma , alveolar or embryonal rhabdomyosarcoma , desmo plastic small round cell tumour , extraskeletal myxoid chondrosarcoma , protuberans , malignant mixed mesodermal tumour or carcinosarcoma of the uterus , smooth muscle tumours of uncertain malignant potential of uterus , known active or uncontrolled brain metastases , active uncontrolled infection , or grade 3 or 4 peripheral neuropathy . 
pregnant or lactating women were excluded , as were patients with a history of malignancy other than sarcoma ( exceptions included basal or squamous cell carcinoma of the skin and carcinoma in situ of the cervix , breast , or prostate ) within 3 years before enrolment . samples of formalin - fixed , paraffin - embedded tumour tissue and haematoxylin and eosin - stained slides were submitted for central review for confirmation of sarcoma diagnosis and histological subtype , although patients were enrolled on the basis of the local pathology report . 
all samples were reviewed by a single histopathologist ( rt )  . the trial was approved by the national research ethics service committee : london , bloomsbury ( 10 / h0713 / 54 ) , the medicines and healthcare products regulatory agency ( clinical trials authorisation number 20363 / 0285 / 001 0001 ) , and by the research and development department of each participating nhs trust . 
gemcitabine was administered over 90 min and docetaxel was administered over 60 mdose capping according to sites local policy and dose banding to within plus or minus 5% of the calculated dose were permitted . 
in both groups , patients completed up to six cycles of treatment in the absence of disease progression , intolerable side - effects , or withdrawal of consent . laboratory monitoring ( blood count and biochemistry ) was done within 72 h of day 1 of each cycle , with additional monitoring on day 8 ( blood count only ) for gemcitabine and docetaxel treatment . 
to proceed with treatment on day 1 of each cycle ( both groups ) the following were required : absolute neutrophil count of at least 10 10 per l , platelet count of at least 100 10 per l , bilirubin of up to 15 uln , and aspartate transaminase , alanine trans aminase , or both of up to 30 uln . 
for administration of treatment on day 8 ( in the gemcitabine and docetaxel group ) the following were required : absolute neutrophil count of at least 10 10 per l and platelets of at least 75 10 per l . 
dose modifications for adverse events were made according to prespecified criteria : dose reductions of 20% ( first occurrence ) nd then 33% ( second occurrence ) were permitted for doxorubicin ( in the case of grade 3 or worse febrile neutropenia ) and gemcitabine and docetaxel ( for grade 3 or worse febrile neutropenia , grade 2 neuropathy , or any grade pulmonary toxicity ) ; a third occurrence required the patient to be withdrawn from treatment . 
 dose delays of up to 2 weeks for haematological toxicity and up to 3 weeks for non - haematological toxicity were allowed ; delays longer than this required the patient to be withdrawn from treatment . 
for doxorubicin , patients were advised to be withdrawn from treatment if left ventricular ejection fraction was less than 45% or reduced by 20% from baseline ( cardiotoxicity monitoring was done according to local institutional policies )  . 
for gemcitabine and docetaxel , patients were withdrawn for the following events : grade 3 pulmonary fibrosis , any grade 4 pulmonary toxicity , grade 3 or 4 hypersensitivity reactions ( docetaxel only ) , or grade 3 weight gain . adverse events were assessed according to the national cancer institute common terminology criteria for adverse events ( ctcae ) version 4.03 , from informed consent until 30 days after last trial treatment administration . 
serious adverse events were reported from informed consent until 30 days after last trial treatment administration , or later if the investigator felt that an event was related to trial treatment . disease status was assessed by ct scan , mri scan , or both at baseline , 12 and 24 weeks after randomisation , and then every 12 weeks until disease progression ( including patients who discontinued treatment for any reason other than disease progression )  . 
 for the pharmacogenomics analyses , dna was extracted from 4 ml whole blood using a qiaamp dna blood maxi kit ( qiagen , manchester , uk ) , according to the manufacturers instructions . 
individual candidate snps the pharmacology of the three drugs were identified from relevant published literature , 1521 and taqman assay on demand probes ( applied biosystems , paisley , uk ) were used to genotype the samples . in genes associated with outcomes the primary endpoint was the proportion of patients alive and progression free at 24 weeks after the date of randomisation . 
secondary endpoints were the proportion of patients alive and progression free at 12 weeks after the date of randomisation , progression - free survival ( time from randomisation to date of progression or death from any cause , whichever occurred first ) , and overall survival ( time from randomisation to date of death from any cause ) , the proportion of patients achieving an objective response by recist 1.1 , the proportion of patients achieving an objective response by choi criteria ( retrospective analysis ) , assessment of adverse events , quality of life , and health economics evaluation . 
time to progression , proportion of patients achieving an objective response as assessed by choi criteria , the health economics assessment , and the planned sensitivity analyses will all be published separately at a later date . 
 statistical analysis under the assumption of a hazard ratio ( hr ) of 063 , 250 patients ( and 148 progressions or deaths ) were required to achieve 80% power with a two - sided of 5% . 
 we assumed a median progression - free survival of 35 months for doxorubicin22 ( corresponding with 30% of patients achieving 24 - week progression - free survival ) and a median progression - free survival of 5 months 1400 vol 18 october 2017 articles ( corresponding with 47% of patients achieving 24 - week progression - free survival ) for gemcitabine and docetaxel.6 , 13 we did the efficacy analysis in the intention - to - treat population of all randomised patients . 
we plotted kaplan - meier curves for progression - free survival and overall survival ; treatment effect hrs ( with 95% cis and p values ) were obtained from cox proportional hazards regression models , adjusted for randomisation stratification factors . 
these analyses were exploratory by nature , and were performed using tests for interaction . we presented adverse events as the worst grade per patient per event , and comparison between groups was done using a test of proportions . we assessed quality of life at the 12 - week postrandomisation visit . 
we used ancova and fitted a linear regression model adjusting for baseline score , stratification factors , and actual time between baseline and 12 - week assessments ( to allow for variation in the timings of assessments )  . 
we prospectively actual planned in our statistical analysis plan to use 99% cis to account for multiple comparisons within the different scales of quality of life , which is a robust approach when the risk of a type 1 error is inflated by making multiple comparisons . to assess the effect of snps on efficacy and toxicity within treatment groups , we used cox proportional hazards regressions on overall survival and progressionfree survival and logistic regressions on any grade 3 or 4 adverse events . we calculated dose intensity relative to the total planned dose using a formula that incorporated delays and dose reductions.23 we used stata version 14.2 for all statistical analyses . an external independent data monitoring committee oversaw the trial and assessed the safety and efficacy approximately annually . 
this study is registered with the european clinical trials ( eudract ) database ( no 2009 01490729 ) and as an international standard randomised controlled trial , number isrctn07742377 . role of the funding source the trial was sponsored by university college london ( ucl ) and coordinated centrally by cancer research uk and ucl ctc . 
the corresponding author had full access to all the data and the final responsibility to submit for publication . associated with raw data the results between dec 3 , 2010 , and jan 20 , 2014 , 257 patients from 24 uk hospitals and one swiss hospital ( appendix p 1 ) were enrolled and randomly assigned to receive doxorubicin ( 129 patients ) or gemcitabine and docetaxel ( 128 patients ; figure 1 )  . 
two randomised patients ( one in each group ) were later found to be ineligible ( figure 1 ) ; however , both are included in the intention - totreat analysis and received treatment . 
our safety population included 254 of the 257 randomised patients , 497 patients assessed for eligibility 240 excluded 91 did not meet inclusion criteria 96 declined to participate 53 other reasons * 257 patients enrolled and randomly assigned 129 allocated to doxorubicin 128 allocated to gemcitabine and docetaxel 1 did not start treatment 2 did not start treatment 128 received allocated intervention ( including 126 received allocated intervention ( including 1 ineligible patient ) 1 ineligible patient ) 3 lost to follow - up 58 discontinued intervention|| 1 lost to follow - up 79 discontinued intervention|| 129 included in intention - to - treat population 128 included in safety population 128 included in intention - to - treat population 126 included in safety population figure 1 : trial profile * other reasons were : 43 multidisciplinary team decision not to approach patient , five deaths , three referred to or treated at other hospital , one patient did not fully understand trial , one trial closed before patient finished radiotherapy . 
histology review reclassified as ineligible histological subtypes ( one gastrointestinal tumour in the doxorubicin group and one extra - skeletal myxoid chondrosarcoma in the gemcitabine and docetaxel group )  . 
||see appendix p 6 for a breakdown of reasons for treatment discontinuation . vol 18 october 2017 1401 articles because one patient who was assigned to doxorubicin and two patients who were assigned to gemcitabine and docetaxel did not receive at least one dose of their allocated treatment ( figure 1 )  . patient characteristics were similar in the two treatment groups at baseline ( table 1 )  . 
the analysis is based on the dataset in its version of sept 8 , 2015 ; at this point , the estimated median follow - up for all patients was 22 months ( iqr 157293 )  . of the 257 randomised patients , 244 ( 95% ) had central histopathology review done . 
51 ( 21% ) of 244 reports differed between the local histology report and the central review report , with 36 ( 14% ) major discrepancies resulting in reclassification of histology , and 15 ( 6% ) minor discrepancies ( eg , high - grade spindle cell sarcoma being reclassified as pleomorphic sarcoma )  . 
of the 13 ( 5% ) of 257 patients whose histology was not reviewed , six samples were never received , one patient had no tissue available , and for six patients there was no tumour tissue in the submitted blocks . more patients in the doxorubicin group ( 71 [ 56% ] of 128 patients ) received the full six cycles of chemotherapy than those in the gemcitabine and docetaxel group ( 49 [ 39% ] of 126 patients )  . 
mean dose intensity23 ( incorporating dose delays and reductions ) was 937% ( sd 009 ) in the doxorubicin group and 834% ( sd 020 ) in the gemcitabine and docetaxel group . 
 more patients in the gemcitabine and docetaxel group experienced dose delays ( 71 [ 56% ] of 126 patients ) than in the doxorubicin group ( 59 [ 46% ] of 128 patients )  . 
the main reasons for dose delays in both groups were febrile neutropenia ( seven [ 12% ] of 59 reasons in the doxorubicin group vs six [ 4% ] of 155 reasons in the gemcitabine and docetaxel group ) , other haematological toxicities ( 16 [ 27% ] vs 44 [ 28% ] ) , non - haematological toxicities ( five [ 8% ] vs seven [ 5% ] ) , other adverse events ( 14 [ 24% ] vs 29 [ 18% ] ) , and other practical or social reasons ( 11 [ 19% ] vs 32 [ 21% ] )  . 
 more patients had dose reductions in the doxorubicin group ( 34 [ 27% ] of 128 patients ) than in the gemcitabine and docetaxel group ( 23 [ 18% ] of 126 ; appendix p 17 ) ; the main reasons for dose reductions were febrile neutropenia ( eight [ 20% ] of 41 reasons in the doxorubicin group vs one [ 1% ] of 89 reasons in the gemcitabine and docetaxel group ) and other haematological toxicities ( seven [ 17% ] of 41 vs 26 [ 29% ] of 89 )  . 
one ( 1% ) of 128 patients in the doxorubicin group and 13 ( 10% ) of 126 in the gemcitabine and docetaxel group stopped treatment early because of toxicity ( appendix p 6 )  . at the time of data analysis , 223 ( 87% ) of 257 patients in the intention - to - treat population had experienced disease progression ; 106 ( 82% ) of 129 patients in the doxorubicin group and 117 ( 91% ) of 128 patients in the gemcitabine and docetaxel group . 
154 ( 60% ) of 257 patients died in the intention - to - treat population ; 74 ( 57% ) of 129 patients in the doxorubicin group and 80 ( 63% ) of 128 patients in the gemcitabine and docetaxel group . 
no deaths were related to the treatment , but two deaths were due to a combination of disease progression and treatment ( see appendix p 10 for the breakdown of causes of death by treatment group )  . 
no discrepancies were noted between the hospitals and the central review for any patients . progression - free survival at 24 weeks did not differ between the treatment groups ( 463% [ 95% ci 375546 ] in the doxorubicin group vs 464% [ 375548 ] in the gemcitabine and docetaxel group ; figure 2 )  . 
the unadjusted hr was 128 ( 95% ci 099165 ; p = 006 ) ; after adjusting for 1402 vol 18 october 2017 articles histological subtype , the hr was 126 ( 097163 ; p = 008 ) in favour of doxorubic although the kaplan - meier curves did not violate the proportional hazards assumption ( p = 046 for the adjusted model ) , they initially overlapped , and then separated after 24 weeks . overall survival did not significantly differ between the two groups . 
overall survival at 24 weeks was 868% ( 95% ci 796916 ) in the doxorubicin group and 826% ( 748882 ) in the gemcitabine and docetaxel group ( figure 3 )  . 
median overall survival was 763 weeks ( 95% ci 600913 ) in the doxorubicin group and 673 weeks ( 531831 ) in the gemcitabine and docetaxel group ( unadjusted hr 114 , 95% ci 083157 ; p = 041 )  . the proportion of patients achieving an objective response by recist 1.1 ( complete or partial response ) was similar in the two groups : 25 ( 19% ) of 129 patients in the doxorubicin group and 25 ( 20% ) of 128 in the gemcitabine and docetaxel group ( table 2 )  . 
 in our prospectively planned exploratory subgroup analysis , no evidence of a differential treatment effect by histological subtype was recorded ( p = 024 ; appendix p 11 )  . 
further subgroup analyses were done comparing leiomyosarcoma versus other sarcomas ( p = 014 ) , and uterine leiomyosarcoma versus other sarcomas ( p = 038 ) , but again no differential effect was evident between the two treatment groups . 
 the most common low - grade non - haematological adverse event was grade 1 and 2 alopecia , which occurred in 110 ( 86% ) of 128 patients in the doxorubicin group and 95 ( 75% ) of 126 patients in the gemcitabine and docetaxel group ( table 3 )  . 
the most common low - grade haematological adverse event was anaemia ( grade 12 in 91 [ 71% ] patients in the doxorubicin group vs 104 [ 83% ] in the gemcitabine and docetaxel group )  . 
the three most common serious adverse events , accounting for 111 ( 39% ) of all 285 serious adverse events , were febrile neutropenia ( 27 [ 17% ] of 155 serious adverse events in the doxorubicin group vs 15 [ 12% ] of 130 in the gemcitabine and docetaxel group ) , fever ( 18 [ 12% ] vs 19 [ 15% ] ) , and neutropenia ( 22 [ 14% ] vs ten [ 8% ] ; appendix pp 79 )  . we compared quality of life between the groups at 12 weeks postrandomisation . 
insufficient questionnaires were returned to be able to assess quality of life at 18 weeks and 24 weeks ( 83 [ 32% ] of 257 questionnaires were returned at both 18 weeks and 24 weeks , compared with 132 [ 51% ] of 257 at 12 weeks )  . 
however , the mean global health status score at 12 weeks was 638 ( sd 225 ) in the doxorubicin group ( based on 64 [ 50% ] of 129 patients ) and 591 ( sd 218 ) in the gemcitabine and docetaxel group doxorubicin gemcitabine and docetaxel hr 128 ( 95% ci 099165 ) ; p = 006 time since randomisation ( weeks ) 129 ( 0 ) 128 ( 0 ) 60 ( 1 ) 60 ( 2 ) 28 ( 6 ) 12 ( 4 ) 11 ( 10 ) 5 ( 6 ) 3 ( 11 ) 3 ( 6 ) number at risk ( number censored ) doxorubicin gemcitabine and docetaxel figure 2 : progression - free survival hr = hazard ratio . doxorubicin gemcitabine and docetaxel hr 114 ( 95% ci 083157 ) ; p = 041 time since randomisation ( weeks ) 129 ( 0 ) 128 ( 0 ) 108 ( 4 ) 104 ( 3 ) 80 ( 12 ) 74 ( 13 ) 47 ( 27 ) 44 ( 20 ) 20 ( 42 ) 24 ( 31 ) number at risk ( number censored ) doxorubicin gemcitabine and docetaxel figure 3 : overall survival hr = hazard ratio . complete response partial response stable disease progressive disease not evaluable data are n ( % )  . table 2 : objective responses doxorubicin ( n = 129 ) gemcitabine and docetaxel ( n = 128 ) 2 ( 2% ) 23 ( 18% ) 60 ( 47% ) 25 ( 19% ) 19 ( 15% ) 25 ( 20% ) 50 ( 39% ) 27 ( 21% ) 26 ( 20% ) ( based on 63 [ 49% ] of 128 patients )  . 
myocardial infarction ( grade 5 ) recorded in one patient who received doxorubicsudden death not otherwise specified ( grade 5 ) recorded in one patient who received gemcitabine and docetaxel . 
higher scores are associated with better quality of life ; a positive number indicates better functioning and quality of life on gemcitabine and docetaxel than on doxorubic lower scores are associated with better quality of life ; a positive number indicates worse symptoms on gemcitabine and docetaxel than on doxorubicc30 = eortc core quality - of - life questionnaire . 
 table 4 : difference in quality - of - life outcomes at 12 weeks after randomisation for the pharmacogenomics analysis in our translational from total dna was successfully extracted study , 240 patients : 119 in the doxorubicin group and 121 in the gemcitabine and docetaxel group . 
within the doxorubicin group , three of the four snps in the slc22a16 gene , all in linkage disequilibrium with each other , were associated with a worse progression - free survival ( appendix pp 12 , 15 ) , as was the minor allele of the slc29a1 snp ( rs9394992 , in both heterozygotes and homozygotes ; appendix p 14 )  . 
by contrast , the prdx4 snp ( rs518329 ) minor allele was associated with improved overall survival in the doxorubicin group in both heterozygotes and homozygotes ( appendix p 13 )  . 
analysis of the gemcitabine and docetaxel treatment group indicated a possible association of the abcb1 rs1045642 minor allele with worse progression - free survival in both heterozygotes and homozygotes ( appendix p 12 ) ; the cda rs2072671 snp was associated with worse overall survival ( appendix p 14 ) , and the cmpk1 rs4492666 snp was associated with improved overall survival in both heterozygotes and homozygotes ( appendix p 14 )  . 
the slc22a16 rs723685 minor allele was associated with a reduced frequency of grade 34 adverse events compared with wild type ( ten [ 48% ] of 21 patients vs 69 [ 71% ] of 97 patients ) in the doxorubicin treatment group but not in the gemcitabine and docetaxel group . 
 after completion of treatment within the trial , 58 ( 23% ) of 254 patients in the safety population ( 28 [ 22% ] of 128 patients receiving doxorubicin and 30 ( 24% ) of 126 receiving gemcitabine and docetaxel ) did not receive any additional treatment . 
the remaining 196 ( 77% ) patients received at least one additional treatment : chemotherapy for 139 ( 71% ) of 196 patients ( 62 [ 62% ] of 100 patients in the doxorubicin group and 77 [ 80% ] of 96 patients in the gemcitabine and docetaxel group ) , and local therapies for 57 ( 29% ) of 196 patients ( 38 [ 38% ] and 19 [ 20% ] )  . 
soft - tissue sarcoma is recognised to be a very heterogeneous disease with a large number of histological subtypes , and indeed our trial included 22 different subtypes , with very small numbers of patients with many of these subtypes . 
this heterogeneity is an inevitable feature of most large soft - tissue sarcoma trials , and as such we believe that the geddis trial population is representative of the general population with advanced soft - tissue sarcoma . the activity of combination gemcitabine and docetaxel has been used in locally advanced or metastatic soft - tissue sarcoma since 2002 , and has been investigated in several small studies , which have shown therapy.69 , 11 , 12 a randomised phase 2 study compared gemcitabine and docetaxel with gemcitabine alone in 122 patients with advanced soft - tissue sarcoma who had received between zero and three previous chemotherapy regimens , and reported superior median progression - free survival for gemcitabine and docetaxel compared with gemcitabine alone ( 62 months vs 30 months ) and overall survival ( 179 months vs 115 months ) .13 a subsequent randomised phase 2 study compared gemcitabine and docetaxel versus gemcitabine alone as second - line treatment in 90 patients with leiomyosarcoma , reporting that both schedules were effective second - line therapies , with similar proportions of patients achieving a response.10 gemcitabine and docetaxel has therefore become an accepted in metastatic soft - tissue sarcoma after first - line therapy.24 subsequent phase 1b / 2 studies have combined gemcitabine and docetaxel with bevacizumab showing feasibility and activity , 25 , 26 and also with pazopanib , 27 although that trial closed early because of slow accrual and substantial toxicity . 
a placebo - controlled phase 3 trial28 of gemcitabine and docetaxel in combination with bevacizumab in metastatic uterine leiomyosarcoma for first - line treatment did not show a benefit for progression - free survival or overall survival . treatment option since the first published study6 of gemcitabine and docetaxel , which was confined to patients with leiomyosarcoma , some clinicians have assumed that the combination is more active in leiomyosarcoma and uterine leiomyosarcoma than in other histological subtypes . 
 treatment eect favours doxorubicin favours gemicitabine and docetaxel figure 4 : quality - of - life outcomes at 12 weeks post - randomisation the plotted points represent the mean treatment effect between the groups ( a positive number for the treatment effect indicates a better quality of life on gemcitabine and docetaxel than doxorubicin )  . 
however , the results of the geddis trial refute these claims of superior activity in particular histological subtypes of locally advanced or metastatic softtissue sarcoma versus others , since our results show no evidence influenced by treatment effect was histological subtype . 
we did planned subgroup analyses to investigate whether patients with either leiomyosarcoma or uterine leiomyosarcoma responded better to gemcitabine and docetaxel than other soft - tissue sarcoma histological subtypes , but found no indication of a superior response to gemcitabine and docetaxel in either of these subgroups . that we chose 13 years as the minimum age for the trial , specifically to try to increase participation of the teenage and young adult population , because clinical trial recruitment of this age group is recognised to be poor.29 however , only one patient younger than 18 years of age was recruited , which we believe reflects the differing approaches to treatment of advanced soft - tissue sarcoma by uk paediatric and adult oncologistswith paediatric oncologists using more intensive chemotherapy regimens than those used in this trial . 
additionally , competing paediatric trials in this population were running in the uk at the time of recruitment to geddis , such that we believe that younger patients were preferentially recruited to those paediatric trials . why did gemcitabine and docetaxel fail to show superiority to doxorubicin ? this outcome might have been vol 18 october 2017 1407 articles partly due to the choice of lower dose and fewer cycles of treatment ; the 2002 study by hensley and colleagues6 delivered more cycles ( eight vs six ) , at higher doses ( gemcitabine 900 mg / m and docetaxel 100 mg / m vs gemcitabine 675 mg / m and docetaxel 75 mg / m ) than in geddis . 
our regimen was chosen on the basis of the randomised phase 2 study of maki and colleagues , 13 which had used the higher dose schedule , and had reported high frequency ( 46% ) of dose reductions for gemcitabine and docetaxel , lower dose intensity than gemcitabine , and more than 40% of patients on gemcitabine and docetaxel stopping within 6 months of starting therapy , for nonhaematological toxicities such as fatigue and myalgias , despite dose reductions . 
 additionally , a previous phase 2 study11 that the geddis chief investigator had led using this schedule had found that quite substantial toxicity was experienced in the uk population , such that eight ( 18% ) of 45 patients stopped treatment early due to toxicity , and only ten ( 20% ) patients received the full eight cycles . 
the lower doses used are reflected by the absence of grade 34 thrombocytopenia recorded ( no patients on gemcitabine and docetaxel experienced this toxicity ) compared with a 40% frequency in the previous randomised phase 2 study.13 it might be suggested that the gemcitabine and docetaxel doses we selected were too low . 
 however , despite modifying the gemcitabine and docetaxel schedule for the geddis trial , our results were similar for gemcitabine and docetaxel to those of maki and colleagues study , 13 with median progression - free survival of 55 months versus 62 months , and median overall survival of 155 months versus 179 months , respectively . receiving suitable for an additional factor in the lack of superiority of gemcitabine and docetaxel over doxorubicin at least for overall survival might be the lower overall exposure of patients to gemcitabine and docetaxel , as first - line and second - line treatments combined . 
of 96 patients in the gemcitabine and docetaxel group receiving a subsequent received doxorubicin , whereas of treatment , 60 100 patients in the doxorubicin group receiving a subsequent treatment , only 18 received gemcitabine and docetaxel . 
this difference is because for many uk hospitals at the time of the geddis trial , the combination of gemcitabine and docetaxel was not funded and thus unavailable to clinicians . despite the use of a modified gemcitabine and docetaxel schedule in our study , treatment adherence to gemcitabine and docetaxel was inferior to that for doxorubicpatients in the gemcitabine and docetaxel group experienced more dose delays and lower dose intensity than those in the doxorubicin group , with fewer patients in the gemcitabine and docetaxel group receiving all six cycles of chemotherapy and more patients stopping treatment early due to toxicity . 
docetaxel was omitted at these points according to protocol criteria for low neutrophils or platelets , or toxicity leading to a clinical decision to omit docetaxel ( notably , the most common non - haematological grade 34 toxicity in the gemcitabine and docetaxel group was fatigue )  . 
the excess of patients stopping gemcitabine and docetaxel early might also have reflected a bias in clinicians to stop treatment earlier in the experimental group , in the knowledge that patients could go on to receive standard doxorubicin - based treatment . 
it could be argued that the gemcitabine and docetaxel doses that were delayed or missed represent undertreatment in this group , which could explain the separation of the progression - free survival curves in figure 2 . although no significant difference was seen in any of the individual quality - of - life parameters between the treatment groups , the global health status was numerically lower for gemcitabine and docetaxel than in the doxorubicin group . 
 potential contributing factors are that gemcitabine and docetaxel requires an additional visit to hospital in each 3 - week cycle , and gemcitabine and docetaxel takes longer to deliver than doxorubicin , prolonging each hospital visit and resulting in an added burden on patients with incurable disease receiving palliative chemotherapy . 
the implication of these results is that gemcitabine and docetaxel was more difficult to deliver ( lower dose intensity , more treatment delays , and more patients stopping early due to toxicity ) , and was associated with a worse global health status than doxorubicthus , there does seem to be a disadvantage to patients in receiving gemcitabine and docetaxel as first - line treatment . 
furthermore , there are economic , as well as personal , disadvantages gemcitabine and docetaxel because it is a more expensive treatment regimen than doxorubicin because of higher drug costs , more frequent and longer hospital visits are needed for treatment , and increased requirements for supportive medications ( data not shown )  . importantly , the results of the current study are consistent with two other first - line studies in locally advanced or metastatic soft - tissue sarcoma that included doxorubicin as the control group , with the median progression - free survival of 233 weeks the doxorubicin group in the current study similar to the 225 weeks4 and 26 weeks5 reported in the other studies . 
 this is also true of median overall survival , which was 763 weeks in the doxorubicin group in the current study , compared with 732 weeks4 and 823 weeks5 with doxorubicin in the other studies . 
interestingly , all three studies showed an improvement in progressionfree survival and overall survival compared with the preceding published trial of judson and colleagues2 ( progression - free survival of 199 weeks and overall survival of 554 weeks ) , which had recruited patients several years earlier , suggesting that outcomes have improved for patients with locally advanced or metastatic 1408 vol 18 october 2017 articles soft - tissue sarcoma in recent years . 
clinicians might be better at selecting patients most likely to benefit from palliative chemotherapy for advanced soft - tissue sarcoma , and are treating patients more aggressively in terms of minimising dose reductions and treatment delays , with greater use of supportive medications such as growth factors . 
a further factor might be increasing use of local therapies such as radiotherapy and surgery for patients with metastatic disease , which has been associated with longer overall survival than for patients not receiving such therapies.30 indeed , 57 patients on the geddis trial went on to receive surgery or radiotherapy after completing study treatment . the pharmacogenomics data obtained in the current study suggest that snps in the organic cation transporter slc22a16 are associated with reduced efficacy and decreased toxicity following doxorubicin treatment . 
 these findings are in keeping with previously published data from a breast cancer patient cohort and are consistent with a loss of function in the transporter that results in reduced intracellular influx of doxorubicin.20 validation of these effects in an independent cohort of sarcoma patients would be valuable to ascertain the potential for this snp to influence clinical decisionmaking . 
two other snps , slc29a1 rs9394992 and prdx4 rs518329 , were also associated with outcomes in the doxorubicin group ; however , these genes are not known to be involved in the pharmacology of doxorubicin , so further investigation is required to understand these effects . 
there were indications that three snps predicted to affect gemcitabine pharmacokinetics were associated with an effect on overall survival , most notably the cda rs2072671 snp , which was associated with reduced overall survival in the gemcitabine and docetaxel group , with worse survival in patients homozygous ( rather than heterozygous ) for the minor allele ( this is referred to as a gene - dose effect )  . 
however , the same snp was not associated with a difference in progression - free survival , and insufficient evidence is currently available to advocate routine testing of these snps to influence clinical decision - making . limitations of the current study include the fact that we used a gemcitabine and docetaxel schedule that used fewer cycles and lower doses than in the originally published schedule , 6 which is widely used in other countries . 
 although we had a clear rationale for this decision , nevertheless we acknowledge that some might conclude that this limits the applicability of the trial results to the wider population of patients with advanced soft - tissue sarcoma beyond our trial . 
additionally , more patients stopped treatment early on gemcitabine and docetaxel than doxorubicin , which might have reflected the fact that clinicians knew that patients could go on to receive doxorubicin , whereas the reverse was not true due to the limited availability of gemcitabine and docetaxel in the uk at that time outside of clinical trials . how should these results inform our discussions with patients with advanced soft - tissue sarcoma ? the data do not support superiority for gemcitabine and docetaxel over doxorubicin on survival outcomes . 
although the similar progression - free survival and overall survival of gemcitabine and docetaxel and doxorubicin might support a conclusion that either schedule can be used according to patient or clinician preference , our results indicate the need for caution with such an approach , in that gemcitabine and docetaxel is more difficult to deliver than doxorubicin , and patients find it more toxic than doxorubicin , with some effects on quality of life . 
thus , the overall clinical conclusion should be that doxorubicin remains standard of care as first - line treatment for locally advanced or metastatic softtissue sarcoma , and that gemcitabine and docetaxel is not recommended as routine first - line treatment . 
there might of course be occasions when different choices are made depending on patient factors and preferences , such as using combination doxorubicin and ifosfamide for selected patients who need to optimise chances of tumour shrinkage , or using gemcitabine and docetaxel in patients with cardiac dysfunction that contraindicates use of doxorubichowever , for most patients , these results will hopefully provide evidence for clinicians to consider with their patients when selecting first - line treatment for advanced soft - tissue sarcoma . 
the study also highlights the importance of doing randomised trials in rare cancers to rigorously compare new treatments with established standard treatments , rather than extrapolating promising results from smaller non - comparative trials . contributors geddis was developed through and supported by the uk national cancer research institute sarcoma clinical studies group and was led by the trial management group ( composed of bs , sjs , jw , ml , pjw , fc , cr , zw , sf , and sb )  . 
sf and sb were responsible for the conduct of the trial , ensuring all required approvals were in place , and for collection and verification of the integrity of the data . 
all authors gave final approval of the version to be published . declaration of interests bs has received honoraria and travel grants from novartis , pharmamar , ariad , clinigen , daiichi , and lilly . 
 jw , ml , fc , zw , cb , gjv , dj , kk , rt , sf , sn , and h - md declare no competing interests . acknowledgments we thank all patients participating in geddis and their families . 
 the geddis trial was funded by cancer research uk ( c2921 / a11561 ) , with separate funding obtained from sarcoma uk ( suk16.2015 ) to support the pharmacogenomics studies described . 
we thank ian judson ( royal marsden hospital , london , uk ; retired ) for his review of the manuscript and shonit punwani ( university college london , london , uk ) for his input into the central ct scan review . 
 crs work on the trial was supported at the kantonsspital st gallen by a grant of the clinical trials unit commission , ctu 12 / 14 . corrections correction to lancet oncol 2014 ; 15 : 856 correction to lancet oncol 2015 ; 16 : 60 , 61 ledermann j , harter p , gourley c , et al . 
lancet oncol 2014 ; 15 : 85261 in this article , the second sentence of the rst paragraph of the results section should read on the basis local germline brca mutation testing reported on case report forms , germline brca mutation status was known for 98 ( 37% ) of 265 patients ( 50 [ 37% ] of 136 in the olaparib group vs 48 [ 37% ] of 129 in the placebo group )  . 
this correction has been made to the online version as of march 30 , 2015 . a multi - centre , topp ms , gckbuget n , stein as , et al . 
lancet oncol 2015 ; 16 : 5766in table 2 of this article , the mrd response during rst two cycles in patients with cr or crh row should not have been indented , and should have been the last row in the table . 
these corrections have been made to the online version as of march 30 , 2015 . after vol 16 april 2015 e158 published online may 9 , 2018 s1470 - 2045 ( 18 ) 30289 - 4 see articles page 785 genetic predisposition to medulloblastomas : just follow the tumour genome for a the actual contribution of germline mutations to paediatric cancers has been a major concern for paediatricians , basic researchers , geneticists , epidemiologists , and parents long time . 
 the first notable piece of work1 in this field was produced by researchers from the st jude research hospital the number of germline variants in known cancer genes , assessed using constitutional dna from more than 1000 paediatric patients . 
first , by use of the largest retrospective cohort constituted and validating it on prospectively collected dnas , it aimed to unbiasedly assess the actual incidence of cancer predisposition syndromes in patients with medulloblastoma . 
the authors identified six genes with a significant excess of damaging germline mutations for patients with medulloblastoma : apc , brca2 , palb2 , ptch1 , sufu , and tp53 . 
this study confirms the high prevalence of sufu and ptch1 mutations in infants with shh medulloblastomas , 3 , 4 and also substantiates the overall higher risk for tp53 or ptch1 germline mutations in shh medulloblastomas , whatever the age at onset.5 however , it also highlights that a familial history of cancer is often absent in these cases of shh medulloblastoma . 
 the study shows for the first time the phenotype of the rare ( seven [ 1% ] of 1022 patients ) germline apcrelated medulloblastomas ( five of whom were children in the wnt subgroup who had excellent overall survival of 100% at 36 months ) which , by contrast with shh medulloblastomas , usually occur in a clear familial context , emphasising the need for a careful interview regarding familial history in children with wnt medulloblastomas . 
 the second main finding was the refinement of the potential role of brca2 and palb2 germline mutations in medulloblastoma , so far known only in the context of fanconi anaemia.6 , 7 germline heterozygous brca2 ( seven [ 1% ] of 1022 patients ) and palb2 ( five [ < 1% ] of 1022 ) variants might also be associated with an increased risk of medulloblastoma in childhood . 
the presence of loss of heterozygosity of the wildtype brca2 and palb2 allele in some tumours or the tendency of corresponding tumours to present some signs of homologous recombination repair deficiency ( hrd ) might suggest pathogenicity . 
international collaboration to collect data from more families with brca2 and palb2 mutations with precise evaluation of the frequency of medulloblastomas might help to decipher the actual involvement of these heterozygous mutations in predisposition to medulloblastoma . 
 because chromothripsis medulloblastoma indicates the presence of tp53 mutations and can subsequently induce familial screening , 4 finding insights for hrd and brca2 and palb2 mutations in a child with medulloblastoma might eventually cause the initiation of tumour screening in the relatives . 
since early cancer detection in unaffected individuals is one major goal of genetic counselling , possible familial consequences of broad genetic analyses on tumour dna will need to be explicitly anticipated with parents ; moreover , the medical benefit and psychological effects of such findings on families with no cancer history should be prospectively evaluated . finally , the study does not identify any specific predisposing genes for group 3 and group 4 medulloblastomas , which shows that a young age at cancer 722 vol 19 june 2018 comment onset ( group 3 ) might not indicate a strong probability of predisposing syndrome per se . 
moreover , although many studies have investigated this class of high - penetrance predisposition genes , lowthe penetrance , high - frequency alleles remains unknown and still needs to be investigated through genome - wide association studies for medulloblastoma . 
the study highlights the major interest of somatic molecular criteria , in addition to family history and potential malformative syndrome , to suggest genetic predisposition and hence lead to genetic counselling and germline genetic assessment with a clear prioritisation scheme depending on the type of medulloblastoma . * franck bourdeaut , olivier delattre siredo pediatric cancer center , inserm u830 , institut curie , paris 75005 , france franck.bourdeaut@curie.fr we declare no competing interests . copyright the author ( s )  . 
blood 2004 ; 103 : 255459 . targeting the tumour vasculature in mesothelioma in 2018 , malignant mesothelioma remains a rapidly lethal cancer for which there is no standard second - line therapy . 
the disease represents both an opportunity for drug development and a substantial challenge , as evidenced by recent negative , yet appropriately controlled and powered , phase 3 trials.1 , 2 inter - patient heterogeneity , coupled with an absence of personalised strategies , account for these previous failures , highlighting an unmet need . 
these include the identification of the ezh2 subunit of polycomb in bap1 - mutated repressor complex 2 as a target mesothelioma , which is being explored in a proof - ofconcept phase 2 study ( nct02860286 ) .3 pegylated arginine deiminase has shown efficacy in mesotheliomas that do not express argino succinate synthetase , and a combination strategy is being investigated in the phase 3 atomic trial ( nct02709512 )  . 
checkpoint inhibition shows activity in the context of programmed cell death ligand 1 ( pdl - 1 ) expression ; 4 however , the jury is still out regarding the significance of this potential biomarker for patient selection in treating mesothelioma . 
 in the lancet oncology , vanesa gregorc and colleagues5 report the results of their phase 3 ngr015 trial , in which they tested a novel vascular disrupting agent ( ngr - htnf ) in an unselected population of patients . 
at picomolar concentrations , the endothelial barrier function of the neovasculature impaired , enhancing chemotherapy penetration in murine models.6 in a previous phase 2 trial , 7 ngrhtnf monotherapy showed an arguably modest disease control with 44% of patients achieving disease control , with evidence of partial response ( albeit 2% ) , and a median of 28 months progression - free survival . 
 published online may 9 , 2018 s1470 - 2045 ( 18 ) 30248 - 1 see articles page 799 vol 19 june 2018 comment news published online november 5 , 2020 s1470 - 2045 ( 20 ) 30678 - 1 for more on the budget cuts to eu4health see sciencebusiness.net / frameworkprogrammes / news / slashedeu4health - budget - willundermine - cancer - plan - meps - say for more on eu4health see funding / eu4health_en for the european health report see sites / health / files / state / docs / 2018_healthatglance_rep_ en.pdf for the 2020 estimates of cancer cases and deaths in europe see jrc / en / news / 2020 - cancerincidence - and - mortality - eu - 27countries for more on the europe beating cancer plan see non_communicable_diseases / cancer_en eu4health budget cut threatens europes beating cancer plan a dramatic reduction in the eu4health budgetfrom the 94 billion originally pledged to now less than 2 billionthreatens to cripple the europe beating cancer plan that it promised to fund earlier this year . the official announcement was made last week , on oct 27 , 2020 , by stella kyriakides , the european commissioner for health and food safety , when she appeared before the committee of members of european parliament ( meps ) responsible for overseeing the beating cancer plan . 
 the announcement left them shocked and disappointed , as they accused kyriakides of lacking ambition for , and commitment to , this momentous and crucial public health initiative . there is no explanation why the eu member states decided to cut the eu4health budget so drastically , commented bartosz arukowicz , mep and chair of the special committee on beating cancer . 
 today , in the context of a major health crisis , cutting vital funds on common actions in health care sends the worst possible signal both to the sector itself , but also to patients , he added . nicolae tefnu , another mep on the committee , expressed his frustration over the news , adding that the slashed budget could jeapordise european health goals : these cuts have transformed the bold ambitions of the eu4health programme into smoke and mirrors . 
 the long - term sustainability of our health - care systems and millions of lives depend upon the success of this programme that aims to win the battle against cancer . 
we must stop making compromises in terms of funding when it comes to such crucial endeavours concerning our health . eu4health is a dedicated funding programme for 202127 that has been established in response to the ongoing covid - 19 pandemic , which continues to create huge pressures and demands on medical and health - care staff and health systems in europe , with inevitable consequences for patients . 
eu4healths ambitious strategy involves tackling major cross - border health threats , building up reserves of medical supplies and health - care staff for crises , strengthening health systems , increasing preparedness for epidemics , and making medicines accessible and affordable across all eu countries , as well as improving health care access for vulnerable groups . cancer has long been a major concern for eu health officials as the second leading cause of death in europe after cardiovascular disease , accounting for 25% of all deaths in 2015 according to the most recent health report . 
despite representing less than 10% of the worlds population , europe has around a quarter of global cancer cases , with an estimated 27 million new cases and 13 million deaths in 2020 . 
on world cancer day this year ( feb 4 , 2020 ) , european commission president ursula von der leyen announced the launch of a public consultation for europes beating cancer plan as part of a major new effort to tackle the european cancer crisis through improvements in four key areas : cancer prevention , early diagnosis , treatment , and follow - up care . 
the plan also aims to address the issue of cancer - related inequalities between and within eu member states , with actions to support , coordinate , and complement individual member states efforts . europes beating cancer plan is an example of how the eu can work together to tackle a complex disease , such as cancer , explained solange peters , president of the european society of medical oncology ( esmo ) and speaking on behalf of the esmo board . 
unfortunately , the councils envisioned substantial budget cuts to eu4health , which is one of the primary funding sources for the plan , could adversely affect its implementation , and in turn cancer care . prevention , early diagnosis , supporting access to cancer services ( including medicines ) , avoiding medicines shortages , supporting the quality of life of patients with cancer as well as capacity building for continuous education in cancer care , are all crucial elements that would benefit from supranational coordination , peters continued . 
 we , as a community , need to ensure that we reduce the health inequalities our citizens face , and that every citizen receives equal access to optimal cancer care . 
as esmo , we request the member states to come together and prioritise health : as covid - 19 has shown us that without health , the world comes to a standstill . while elements of europes beating cancer programmesuch as professional training and the strengthening of eu reference networkswill still be supported by eu4health under the current plan , additional funding will be obtained through a variety of different sources , including eu research programmes such as horizon europe and contributions from member states . 
 meanwhile , they are continuing to attempt to negotiate a budget increase for eu4health . elizabeth gourd 1558 vol 21 december 2020 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com authors reply jonathan knisely expresses concern about several features of our paper , 1 which leads him to qualify the paper and the data presented as potentially misleading and awed . 
the argument that we did not analyse data for patients in whom central pathology review did not conrm a diagnosis of low - grade glioma is incorrect because these individuals formed part of the sensitivity analysis presented in the paper . 
to cite the present who classication , the main histopathological features of anaplastic glioma are those of a diffusely inltrating astrocytoma with increased cellularity , distinct nuclear atypia , and marked mitotic activity.2 similar , far - from - precise descriptions are given to dene low - grade oligodendroglioma from their anaplastic counterparts . 
substantial variation between researchers in the area of neuro - oncology exists precisely because of such arbitrary descriptions inherent to microscopic classication of brain tumours.3 , 4 i would indeed hope that an expert pathologist is involved in the routine care of patients with glioma , but even these specialists might disagree with each other . 
we need trials instead of speculation : for too long treatment of this disease has been dominated by expert opinion . martin van den bent , on behalf of the eortc 22845 trialists department of neuro - oncology , daniel den hoed oncology centre , rotterdam , the netherlands m.vandenbent@erasmusmc.nl i declare no conicts of interest . van den bent mj , afra d , de witte o , et al . 
fertility preservation for young patients with cancer : who is at risk and what can be offered ? lancet oncol 2005 ; 6 : 20918sections on the preservation of male fertility and on the ethics of fertility preservation in this review had substantial similarity with that of a previously published paper . 
asian j andol 2003 ; 5 : 32537 . vol 6 december 2005 re ection and reaction parameters and does not incorporate non - carcinoma variables , such as concomitant illnesses , which could also a ect patient outcome.2 however , in the midst of such uncertainty , fuzzy logic could have an important role in the decision - making process . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
the global , regional , and national burden of pancreatic cancer and its attributable risk factors in 195 countries and territories , 19902017 : a systematic analysis for the global burden of disease study . 
org / s2468 - 1253 ( 19 ) 30421 - 2 . cancer patients in sars - cov - 2 infection : a nationwide analysis in china china and the rest of the world are experiencing an outbreak of a novel betacoronavirus known as severe acute respiratory syndrome corona virus 2 ( sarscov - 2 ) .1 by feb 12 , 2020 , the rapid spread of the virus had caused 42 747 cases and 1017 deaths in china and cases have been reported in 25 countries , including the usa , japan , and spa who has declared 2019 novel coronavirus disease ( covid - 19 ) , caused by sars - cov - 2 , a public health emergency of international concern . 
in contrast to severe acute respiratory system coronavirus and middle east respiratory syndrome coronavirus , more deaths from covid - 19 have been caused by multiple organ dysfun ction syndrome rather than respiratory failure , 2 which might be attributable to the widespread distribution of angiotensin con verting enzyme 2the functional receptor for sars - cov - 2 in multiple organs.3 , 4 patients with cancer are more susceptible to infection than individuals without cancer because of their systemic immunosuppressive state caused by the malignancy and anticancer treat ments , such as chemotherapy or surgery.58 therefore , these patients might be at increased risk of covid - 19 and have a poorer prognosis . on behalf of the national clinical research center for respiratory disease , we worked together with the national health commission of the peoples republic of china to establish a prospective cohort to monitor covid - 19 cases throughout china . 
as of the data cutoff on jan 31 , 2020 , we have collected and analysed 2007 cases from 575 hospitals ( appendix pp 49 for a full list ) in 31 provincial administrative regions . 
 we excluded 417 cases because of insufficient records of previous disease history . ( 28583 18 ( 1% ; 95% ci 061165 ) of 1590 covid - 19 cases had a history of cancer , which seems to be higher than the incidence of cancer in the overall chinese [ 029% ] per 100 000 people , population according to 2015 cancer epidemiology statistics9 )  . 
four ( 25% ) of 16 patients ( two of the 18 patients had unknown treatment status ) with cancer with covid - 19 had received chemotherapy or surgery within the past month , and the other 12 ( 75% ) patients were cancer survivors in routine followup after primary resection . 
compared with patients without cancer , patients with cancer were older ( mean age 631 years [ sd 121 ] vs 487 years [ 162 ] ) , more likely to have a history of smoking ( four [ 22% ] of 18 patients vs 107 [ 7% ] of 1572 patients ) , had more polypnea ( eight [ 47% ] of 17 patients vs 323 [ 23% ] of 1377 patients ; some data were missing on polypnea ) , and more severe baseline ct manifestation ( 17 [ 94% ] of 18 patients vs 1113 [ 71% ] of 1572 patients ) , but had no signifi cant differences in sex , other baseline symptoms , other comorbidities , or baseline severity of x - ray ( appendix p 2 )  . importantly , patients with cancer were observed to have a higher risk of severe events ( a composite endpoint defined as the percentage of patients being admitted to the intensive care unit requiring invasive ventilation , or death ) compared with patients without cancer ( seven [ 39% ] of 18 patients vs 124 [ 8% ] of 1572 patients ; fishers exact p = 00003 )  . 
 most published online february 14 , 2020 s1470 - 2045 ( 20 ) 30096 - 6 see online for appendix vol 21 march 2020 comment invasive ventilation or icu admission , or death , plus clinical indication invasive ventilation or icu admission , or death no cancer cancer survivors patients with cancer cancer status patients without cancer patients with cancer hazard ratio 356 ( 95% ci 165769 ) time after disease onset ( days ) figure : severe events in patients without cancer , cancer survivors , and patients with cancer ( a ) and risks of developing severe events for patients with cancer and patients without cancer ( b ) icu = intensive care unit . we observed similar results when the severe events were defined both by the above objective events and physician evaluation ( nine [ 50% ] of 18 patients vs 245 [ 16% ] of 1572 patients ; fishers exact p = 00008 )  . 
 moreover , patients who underwent chemotherapy or surgery in the past month had a numerically higher risk ( three [ 75% ] of four patients ) of clinically severe events than did those not receiving chemotherapy or surgery ( six [ 43% ] of 14 patients ; figure )  . 
these odds were further confirmed by logistic regression ( odds ratio [ or ] 534 , 95% ci 1801618 ; p = 00026 ) after adjusting for other risk factors , including age , smoking history , and other comorbidities . 
 lung cancer did not have a higher patients with probability of severe events compared with patients with other cancer types ( one [ 20% ] of five patients with lung cancer vs eight [ 62% ] of 13 patients with other types of cancer ; p = 0294 )  . 
additionally , we used a cox regression model to evaluate the time - dependent hazards of developing severe events , and found that patients with cancer deteriorated more rapidly than those without cancer ( median time to severe events 13 days [ iqr 615 ] vs 43 days [ 20not reached ] ; p < 00001 ; hazard ratio 356 , 95% ci 165769 , after adjusting for age ; figure )  . in this study , we analysed the risk for severe covid - 19 in patients with cancer for the first time , to our knowledge ; only by nationwide analysis can we follow up patients with rare but important comorbidities , such as cancer . 
 additionally , we showed that patients with cancer had poorer outcomes from covid - 19 , providing a timely reminder to physicians that more intensive attention should be paid to patients with cancer , in case of rapid deterioration . therefore , we propose three major strategies for patients with cancer in this covid - 19 crisis , and in future attacks of severe infectious diseases . 
 third , more intensive surveillance or treatment should be considered when patients with cancer are infected with sars - cov - 2 , especially in older patients or those with other comorbidities . we declare no competing interests . 
this study is supported by the china national science foundation ( grant no 81871893 ) and the key project of guangzhou scientific research project ( grant no 201804020030 )  . wenhua liang , weijie guan , ruchong chen , wei wang , jianfu li , ke xu , caichen li , qing ai , weixiang lu , hengrui liang , shiyue li , * jianxing he drjianxing.he@gmail.com 336 vol 21 march 2020 comment joint first authors joint senior authors department of thoracic oncology and surgery ( wli , ww , jl , kx , cl , qa , wlu , hl , jh ) and department of respiratory disease ( wg , rc , sl ) , china state key laboratory of respiratory disease and national clinical research center for respiratory disease , the first affiliated hospital of guangzhou medical university , guangzhou 510120 , china chen n , zhou m , dong x , et al . 
zhonghua zhong liu za zhi 2019 ; 41 : 1928 ( in chinese )  . should patients who are incarcerated on death row receive palliative cancer care ? in modern society , it is accepted that individuals have the right to die with dignity . 
at present , there are more than 2600 incarcerated men and women in the usa who have been sentenced to death , most of whom have less than a high school diploma or high school equivalency certificate ( ged ) , and are disproportionately of minority racial or ethnic backgrounds ( 42% african - american representation on death row vs 13% african - american representation in the us census ) .1 the combination of poor health status , social determinants of health , and paucity of adequate care provided in correctional facilities is driving a public health emergency , which is endangering the incarcerated population . 
we can north american expect the prevalence and burden of chronic illness to rise concomitantly with the growth of the ageing population in us prisons.2 data suggest that cancer is the leading cause of illness - related deaths in us state prisons.2 in the absence of reform , the mass incarceration trends observed over the past three decades will substantially widen disparities , adversely affecting access to health care . 
this dilemma is bound to have a downstream effect on patients with cancer who have been sentenced to death and can affect the quality of palliative care provided in correctional facilities . 
in the community , a multidisciplinary team would manage the medical , mental health , and social service needs of a patient who chooses palliative care for a terminal diagnosis . 
but what of the patient who is sentenced to die by judicial execution ? that any such person should receive a benefit of any sort , including the traditional last meal , is met with public protest and outrage . 
such consternation will probably increase despite the fact that denying palliative care results in unnecessary suffering for the patient at no benefit to public safety . is well established that professional ethics forbids health - care staff from participating in any aspect of capital punishment . 
however , what of the incarcerated patient with cancer who is dying under the care of a physician with direct or indirect duties to the jurisdiction charged with judicial execution ? what are the duties of the physician expected to provide palliative care to the incarcerated if the patient desires it ? we argue that they are no different than those incumbent upon the physician and health - care staff in the community . 
the accepted framework of medico ethical principles requires that oncology practitioners consider pain relief and other principles of palliative vol 21 march 2020 comment correction to lancet oncol 2018 ; 19 : 156978 correction to lancet oncol 2018 ; 19 : 165467 correction to lancet oncol 2019 ; 20 : 4356 solomon bj , besse b , bauer tm , et al . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 168087 vergote i , coens c , nankivell m , et al . 
 ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 4356on figure 3 , del11p has been corrected to del11q , the 95% ci for the hazard ratio for age 65 years or greater has been corrected to 012037 , and the 95% ci for the hazard ratio for bulky disease of at least 5 cm has been corrected to 008040 . 
these corrections have been made to the online version as of jan 3 , 2019 and the printed version is correct . correction to lancet oncol 2019 ; 20 : 8899 mamounas ep , bandos h , lembersky bc , et al . 
 this correction has been made to the online version as of jan 3 , 2019 , and the printed version is correct . kulasingham s , malagn t , mayrand m - h , et al . 
lancet oncol 2018 ; 19 : 156978the title of this article was incorrect and should read age at last screening and remaining lifetime risk of cervical cancer in older , unvaccinated women : a modelling study . 
this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1590601 gibson tm , mostoufi - moab s , stratton kl , et al . 
 lancet oncol 2018 ; 19 : 1590601in this article , the second sentence of the introduction should read more than 80% of children diagnosed with a malignancy now achieve 5 - year survival , but these individuals have substantial risks of morbidity and mortality later in life because of the late effects of cancer and its treatments . 
the final sentence of the first paragraph of the methods should read the institutional review boards of the participating institutions approved the ccss protocol , and participants provided written informed consent to participate in the ccss study and to be part of research studies using the cohort . 
 this correction has been made to the online version as of jan 3 , 2019 . e10 vol 20 january 2019 corrections effect of patient choice and hospital competition on service configuration and technology adoption within cancer surgery : a national , population - based study ajay aggarwal , daniel lewis , malcolm mason , arnie purushotham , richard sullivan , jan van der meulen summary background there is a scarcity of evidence about the role of patient choice and hospital competition policies on surgical cancer services . 
in this national , population - based study we investigated the effect of patient mobility and hospital competition on service configuration and technology adoption in the national health service ( nhs ) in england , using prostate cancer surgery as a model . methods we mapped all patients in england who underwent radical prostatectomy between jan 1 , 2010 , and dec 31 , 2014 , according to place of residence and treatment location . 
for each radical prostatectomy centre we analysed the effect of hospital competition ( measured by use of a spatial competition index [ sci ] , with a score of 0 indicating weakest competition and 1 indicating strongest competition ) and the effect of being an established robotic radical prostatectomy centre at the start of 2010 on net gains or losses of patients ( difference between number of patients treated in a centre and number expected based on their residence ) , and the likelihood of closing their radical prostatectomy service . findings between jan 1 , 2010 , and dec 31 , 2014 , 19 256 patients underwent radical prostatectomy at an nhs provider in england . 
37 ( 57% ) of the 65 centres had a significant net loss of patients , of which two ( 5% ) were established robotic centres and ten ( 27% ) closed their radical prostatectomy service during the study period . 
radical prostatectomy centres that closed were more likely to be located in areas with stronger competition ( highest sci quartile [ 087092 ] ; p = 00081 ) than in areas with weaker competition . 
the number of centres performing robotic surgery increased from 12 ( 18% ) of the 65 centres at the beginning of 2010 to 39 ( 71% ) of 55 centres open at the end of 2014 . interpretation competitive factors , in addition to policies advocating centralisation and the requirement to do minimum numbers of surgical procedures , have contributed to large - scale investment in equipment for robotic surgery without evidence of superior outcomes and contributed to the closure of cancer surgery units . 
if quality performance and outcome indicators are not available to guide patient choice , these policies could threaten health services ability to deliver equitable and affordable cancer care . lancet oncol 2017 ; 18 : 144553 published online october 3 , 2017 s1470 - 2045 ( 17 ) 30572 - 7 see comment page 1424 department of health services research & policy ( a aggarwal md , prof j van der meulen phd ) and department of social and environment health research ( d lewis phd ) , london school of hygiene & tropical medicine , london , uk ; clinical effectiveness unit , royal college of surgeons of england , london , uk ( a aggarwal , prof j van der meulen ) ; school of medicine , cardiff university , cardiff , uk ( prof m mason md ) ; and division of cancer studies ( prof a purushotham md ) and institute of cancer policy ( prof r sullivan md ) , kings college london , london , uk correspondence to : dr ajay aggarwal , department of health services research & policy , london school of hygiene & tropical medicine , london wc1h 9sh , uk ajay.aggarwal@lshtm.ac.uk funding national institute for health research . copyright the author ( s )  . 
in health - care systems where hospitals compete on quality and not on price , competition is also in others8with expected to incentivise improvements in the quality of hospital services to attract patients.9 choice and competition , as well as centralisation , attempt to achieve improvements in patient outcomes , but they require different health - system configurations and provider incentives to operate effectively . 
finding the right balance between choice and competition on the one hand and centralisation on the other is therefore key , but there is little evidence to guide how best to achieve this.10 the uk national health service ( nhs ) is an example of a health system that remains committed to choice and competition as a health - care reform model since the inception of this model in 2006.11 the cost of providing vol 18 november 2017 1445 articles research in context evidence before this study several countries have introduced policies that allow patients to choose a specific health - care provider , with the aim of improving the quality of care . 
we did a systematic review to assess the evidence that patients with cancer are willing to travel beyond ( bypass ) their nearest hospital for cancer surgery , and to assess the effect of competition on outcomes of surgery . 
there was significant heterogeneity in the design of empirical studies , including differences in data quality , the geographical unit of analysis , and limited control for the influence of price competition . 
no studies had looked at the effect of competition on outcomes of cancer . added value of this study to our knowledge , this is the first national evaluation of the effect of choice and competition policies on the patterns of service configuration and technology adoption for cancer surgery . 
 the mobility of men to alternative , more distant centres resulted in substantial changes in market share for individual surgical centres , which were most marked in areas of highest competition . 
we found that , between 2010 and 2017 , there has been large - scale adoption of robot - assisted radical prostatectomy , increasing by three times , from 12 centres at the start of 2010 to 42 by 2017 . 
during the same time period , 16 of the 65 nhs radical prostatectomy centres in england closed their prostate cancer surgery unit . implications of all the available evidence patients with cancer respond to policies that enable them to choose a surgical provider of their choice . 
in the absence of appropriate information about quality of care , policies based on patient choice and hospital competition could create incentives for adoption of new technologies without evidence of superior outcomes as hospitals look to retain and attract new patients . 
 the resulting changes in market share for individual hospitals could threaten the viability of their surgical services . services is fixed under a national rate tariff scheme12 and hospitals are expected to compete for patients on the basis of quality . 
receiving care incurs no additional user charges at the point of access and patients have the right to choose and travel to any hospital that best meets their needs . additionally , national policy in the uk continues to advocate centralisation of specialist cancer services such as prostate and oesophagogastric surgery.1316 not only does this serve to reduce the number of hospitals that patients with cancer can choose from , but it is also expected that patients will receive care at their nearest ( local ) centre on the basis of established secondary care referral pathways for specialist cancer surgery.17 however , our 2017 analysis18 found that not all patients are following the expected referral patterns for specialised cancer surgery . 
one in three men who had a radical prostatectomy for prostate cancer between 2010 and 2014 in the nhs travelled beyond or bypassed their nearest prostate cancer surgery centre , in many cases across regional boundaries . 
in the absence of indicators that accurately reflect the quality of prostate cancer surgery , men were attracted to centres offering robot - assisted radical prostatectomy or centres that employed surgeons with a national reputation for prostate cancer surgery . there is little evidence about what effect patient mobility and hospital competition have had on the configuration of specialist cancer services and the introduction of new surgical technologies into clinical practice . 
we used patient - level data and geographical information system modelling to analyse the effect of patient mobility for cancer surgery and hospital competition on service configuration and technology adoption within the nhs , using prostate cancer as a model . 
in light of our findings , we appraised the international evidence exploring the role of choice and competition policies on the delivery of cancer surgery services and considered opportunities for developing the empirical research base in this area . methods patient population for this national , population - based study we obtained individual patient - level data from the national cancer registration and analysis service ( ncras ) for all men who were diagnosed with prostate cancer and underwent a radical prostatectomy in the nhs in england between jan 1 , 2010 , and dec 31 , 2014 . 
these data were linked at the individual patient level to hospital episode statistics ( hes ) , the administrative database of all hospital episodes in nhs hospitals in england.19 the study was exempt from nhs research ethics committee approval because it involved analysis of an for service existing dataset of anonymised data evaluation . see online for appendix for more on hospital episode statistics see digital.nhs.uk / hes 1446 vol 18 november 2017 articles study design to define each individual patients residence , we used the population - weighted centroids of small geographical areas termed lower super output areas ( lsoas )  . 
there are 34 753 of these small geographical areas ( ie , lsoas ) in england , with an average population of about 1600.20 both the lsoas and full postcodes for the hospitals where the surgery was done were inputted into a geographical information system ( esri arcgis 10.3 ) to calculate travel times according to the fastest route by car to all surgical centres in england ( calculated by use of the ordnance survey mastermap integrated transport network )  . 
those who did not receive care at their nearest surgical centre were classified as bypassers . for each surgical centre , we identified the number of leaverspatients for whom that centre was nearest but who had their treatment at an nhs centre further away . 
a centre was identified as being a winner ( ie , having a net gain of patients ) or loser ( ie , having a net loss of patients ) if the difference between leavers and arrivers was statistically significant based on the conditional method for testing a difference between two poisson means.21 for each surgical centre we calculated a spatial competition index ( sci ) as a measure of external competition.22 , 23 the sci provides a uniform metric that can be used across all surgical centres and that represents the demand for services and the availability of alternative hospitals . 
 conversely , london is 1572 km in size ( and the largest urbanised region in europe ) and had ten surgical centres at the start of the study period.24 ( one of nine english regions ) data analysis in this analysis , the sci for a surgical centre was calculated on the basis of both the number of eligible patients within a 60 - min drive and the number of surgical centres within a 60 - min drive for each eligible patient ; in the equation shown , the surgical centre i has n eligible patients within a 60 - min drive , and patient j in centre i has k surgical centres within a 60 - min drive : scii = 1 1 ji = 1 the sci ranges theoretically from 0 for centres in a monopoly environment to a value close to 1 for centres in the most competitive environment . at the start of the study period ( january , 2010 ) there were 65 prostate cancer surgical centres in england , of which 12 centres routinely performed robot - assisted radical prostatectomy procedures . 
an analysis of hes data , in addition to an organisational survey produced as part of the national prostate cancer audit , 17 was used to evaluate the change in configuration of prostate cancer surgical units across england and the availability of robotic surgery from 2010 onwards . 
all analyses were done with stata , version 14 , to assess the effect of competition , as measured by the sci , on changes in service configuration ( expressed as net gains or losses of patients as defined above ) and adoption of robotic surgery in the nhs . role of the funding source the funder of the study , national institute for health research , had no role in study design , data collection , data analysis , data interpretation , writing of the report , or the decision to submit for publication . 
aa and jvdm had full access to all the data in the study , take responsibility for the integrity of the data and the accuracy of the data analysis , and had final responsibility for the decision to submit for publication . results we identified 19 518 men who were diagnosed with prostate cancer and underwent radical prostatectomy in 19 518 men with hes - linked cancer repository records received radical prostatectomy from 2010 to 2014 19 365 men living in england received radical prostatectomy at an nhs provider in england 153 men excluded who lived outside england : scotland ( n = 8 ) , isle of wight ( n = 67 ) , wales ( n = 78 ) 109 men excluded as the treatment provider was not a recognised nhs provider or the provider was not operational on the date when the surgery was done 19 256 men matched to 65 providers of prostate cancer surgery 19 256 men included in nal cohort figure 1 : flowchart of men included in the study hes = hospital episode statistics . 
nhs = uk national health service . vol 18 november 2017 1447 articles a 50 km 25 km patient origins core users arrivers leavers radical prostatectomy centre 1 dot = 1 patient 100 km 100 km figure 2 : mobility patterns of patients receiving radical prostate cancer surgery at two selected nhs cancer centres maps of the uk , illustrating the mobility pattern of patients who received radical prostate cancer surgery at two selected national health service ( nhs ) cancer centres ( indicated with a + symbol in the area of core users ) located in the east of england ( a ) and southwest england ( b ) that had a net gain of patients from outside their local area ( ie , more arrivers than leavers )  . 
contains national statistics data , crown copyright and database right 2017 ; nhs research scotland ( nrs ) data , crown copyright and database right 2017 ; ordnance survey data crown copyright and database right 2017 ; and northern ireland statistics and research agency data . 
 of these 19 518 men , 262 ( 13% ) were excluded because they either lived outside england or could not be assigned to a particular hospital ; 19 256 were eligible for inclusion in the study ( figure 1 )  . figure 2 shows the places of residence for patients who had their prostate cancer surgery at two selected surgical centres located in the east of england ( figure 2a ) and southwest england ( figure 2b ) , both of which were classified as winners . 
conversely , some of the losers were doing approximately 200 fewer procedures than expected ( and 400 fewer in the case of one centre )  . figure 3 also shows the relationship between , on the one hand , radical prostatectomy centres having a net gain or net loss of patients and , on the other hand , being an established robotic centre or a centre that closed during the study period . 
centres with a net gain were 13 15 19 21 43 45 49 51 55 57 61 63 31 33 25 27 radical prostatectomy centre 37 39 figure 3 : net gains and losses of patients for each radical prostatectomy centre ( n = 65 ) during the study period established robotic radical prostatectomy centres ( n = 12 ) shown in green and centres that closed during the 201014 study period ( n = 10 ) shown in red . 
centres in blue are centres that were neither robotic radical prostectomy centres nor centres that closed during the study period . 1448 vol 18 november 2017 articles s 100 200 300 400 500 more likely to be established robotic centres ( ten [ 43% ] of the 23 winners were robotic centres , compared with two [ 5% ] of the 37 centres with a net loss ; p = 00043 )  . 
 conversely , ten ( 27% ) of the 37 centres with a net loss of patients closed down during the study period . centres with the largest net gains or losses were predominantly located in the most competitive areas ( figure 4 )  . 
seven ( 41% ) of the 17 centres in the highest sci quartile were established robotic centres compared with five ( 10% ) of the 48 other centres in the three other quartiles ( p = 00050 )  . 
similarly , for centre closures , six ( 35% ) of the 17 centres in the highest sci quartile closed compared with four ( 8% ) of the 48 other centres ( p = 00081 )  . 
 both the analysis of hes and the results of the national organisational survey showed profound changes in the organisation and practices of prostate cancer surgical care that continued beyond the end of the study period ( figure 5 )  . 
between 2010 and 2017 , there has been large - scale adoption of robotic surgery , increasing by three times , from 12 ( 18% ) of 65 centres open at the start of 2010 to 39 ( 71% ) of 55 centres open in 2014 to 42 ( 86% ) of 49 in 2017 . 
both the closures and the rapid and widespread adoption of robotic surgery have been unforeseen , effectively rendering commissioning guidelinespublished only in 2015 and recommending phased introduction of robotics for prostate cancer surgery within the nhsobsolete.25 discussion our results suggest that , during the study period analysed , patient choice and hospital competition , rather than a coordinated policy towards centralisation , have been drivers in the changing configuration of surgical cancer services . 
the proportion of patients who bypassed their nearest hospital to have prostate cancer surgery elsewhere has been far larger than the 510% considered to be necessary in the health economics literature to incentivise improvements in hospital quality.26 in the absence of data on outcomes , the mobility of patients has been driven by factors such as availability of advanced surgical technology and the reputation of individual hospitals and clinicians.18 the resulting competition between hospitals has contributed to the closure of radical prostatectomy centres in the nhs in england and widespread adoption of robot - assisted radical prostatectomy as centres have had to respond to potential changes in their market share , which threatened both their income and their ability to meet minimum procedure volume requirements . 
this finding indicates that patient choice and hospital competition , although rarely considered in redesign of cancer services , are potentially powerful drivers of service change , even spatial competition index figure 4 : effect of competition on the net gain or loss of patients for each radical prostatectomy centre during the study period the size of the circles corresponds to the number of men expected to have surgery at the centre . 
 robotic centres total surgical centres 2009 2010 2011 2012 2014 2015 2016 2017 2013 year figure 5 : changes in the number of robotic centres and total number of centres in the nhs in england ( 200917 ) within publicly funded systems . 
it is unlikely that these findings are limited to the nhs in england or to prostate cancer surgery alone . from a wider system perspective , the geographical layout of cancer services means that not all centres face the same competitive pressures and , in turn , will respond differently to choice and competition policies as mechanisms for quality improvement . 
however , we found that patients were prepared to travel substantial distances for treatment , in some cases bypassing several surgical units , which means that even centres within less competitive areas face some level of external competition for patients and subsequently become late adopters of technology to retain local patients.27 vol 18 november 2017 1449 articles attempts to coordinate cancer care services through centralisation and regionalisation have largely ignored the fact that patients are prepared to bypass their local services for treatment . 
this occurrence is partly due to the paucity of empirical evidence about the extent of patient mobility.2830 additionally , cancer care plans have exerted limited control of the available services and technology at the individual hospital level ( eg , introduction of new devices and practices of care ) , which can serve as proxy measures of quality in the absence of quality indicators.31 substantial levels of patient mobility mean that centres need to compete with other providers to meet minimum procedure volume thresholds as set down by national policy.16 in england , each prostate cancer surgery centre is expected to do a specified number of operations per year or face the threat of closure.15 , 32 competition policies have therefore stimulated a form of centralisation through natural selection , as centres act to protect their status as a cancer surgery centre , rather than through a coordinated process based on valid indicators of quality . 
 similar effects have been observed in the us health - care market , where both acute and non - acute care services have closed in response to competition.33 , 34 it is unclear whether these effects have improved the quality of care . none of the centres that closed during the study period did so because of explicit evidence of poor quality . 
further research is required to establish what effect the observed pattern of closures has had on travel times , outcomes , and equity in access to surgical services for the most vulnerable groups , given their decreased ability to travel.28 , 35 the patterns of patient mobility observed occurred at a time when comparative outcome measures for prostate cancer surgery were not available . 
this observation highlights that providers of cancer services , just like any other industry , will consider the use of alternative incentives to attract or retain patients.3638 patients will gravitate to places that make themselves attractive and by doing so they will create centres that treat large numbers of patients , which itself will attract further patients.39 patients with prostate cancer were more likely to travel to centres that were early adopters of robot - assisted radical prostatectomy , showing the powerful effect of advanced technology on perceptions of quality . 
the result of this travel pattern has been that other centres have invested in costly robotic surgery to avoid losing their patients to other centres and to maintain their market share to preserve their cancer centre status , despite a scarcity of evidence for the superiority of this surgical procedure with respect to functional and oncological outcomes.40 , 41 notably , none of the centres that adopted robotic surgery closed down . 
similar patterns have been observed in other health - care markets across the usa and europe , with cancer centres adopting robotic surgery to increase their market share.36 , 4244 our previous systematic review of the literature on patient choice and competition28 identified five empirical studies in high - income settings showing that patients with several tumour types , including breast , bladder , gastric , colorectal , and thoracic cancers , were prepared to bypass their nearest surgical centre.4550 the availability of advanced surgical techniques , procedure volume , and both surgeon and hospital reputation were identified as key drivers for patient mobility . 
patients of advanced age and from low socioeconomic backgrounds were less likely to consider alternatives than those who were younger and more affluent . hospital competition , rather than the pursuit of better quality care by itself , is also cited as a major factor influencing the adoption of new technologies and diversifying individual practices of care for both cancer surgery and radiotherapy.51 there is growing evidence of rapid adoption of technology for cancer surgery across a range of cancer types , beyond prostate cancer , such as renal , colorectal , and gynaecological cancer surgery.36 , 5255 for radiotherapy , where one would expect potentially less patient mobility than is normally observed for services because of the protracted duration of radiotherapy regimens , the past decade has also seen a substantial increase in the use of an array of high - cost technologies.41 these technologies have included intensity - modulated radiotherapy , and proton - beam therapy , with providers trying to gain a competitive advantage over others.51 stereotactic - beam radiotherapy , the question as to whether competition can stimulate improvements in outcomes of cancer surgery remains unanswered . 
two studies have analysed the effect of hospital competition on the pricing of pancreatic cancer56 and colon cancer57 surgery , and one study assessed the effect of such competition on the efficiency of cancer care delivery across tumour types in the us cancer health - care market.58 studies across other specialties have shown mixed results for the effect of fixed - price markets on improvements in health - care quality . 
8 , 23 , 5966 the dearth of studies on patient mobility in both high - income and emerging economies is a major limitation for evidenced - based policy making to decide how best to balance patient choice and top - down policy approaches to service coordination in cancer care . 
we have highlighted potential approaches for management of this health system challenge . for patients , having choice over their treatment or how a specific treatment is given might be more important than having a choice over the actual service provider.67 therefore , differences in availability of technology at the local level , even within a system that publishes validated outcome measures , can contribute to shifts in market share.28 investment in medical devices for cancer care51 seems to be driven predominantly by individual clinicians and clinical departments , possibly because the regulatory hurdles for adoption of new devices are relatively low compared with those of medicines.31 , 68 1450 vol 18 november 2017 articles the use of health technology assessment processes or value frameworks for all new technologies across the cancer care spectrum ( ie , medicines , radio therapy , and surgery ) would act as a meaningful first step towards providing stronger guidance on which inter ventions are likely to deliver the greatest value to patients and society.69 , 70 other options for coordination of technology adoption include coverage with evidence development schemes or establishment of nationally designated research centres to trial new technologies before considering reimbursement.71 however , a significant time lag remains before functional and oncological outcomes will be available inform national implementation , especially for conditions with a lengthy disease coursesuch as prostate cancer . competition between hospitals will continue irrespective of attempts to centralise cancer services . 
 whether public reporting of performance indicators could help to achieve improvements in care quality through competition is debatable.72 it might never be feasible to develop meaningful indicators for some tumour types . 
for example , the appropriateness of many available indicators is problematic because they can only be published after a long lag period ( eg , side - effects and survival rates at 1 and 5 years ) , during which clinical practice can change substantially.73 additionally , there is little evidence to suggest that individuals are more likely to use published performance indicators than proxies for quality , such as a hospitals or clinicians reputation.74 , 75 however , in the absence of any indicator , hospitals will try to differentiate themselves to attract new users , and patients will continue to be reliant on lay sources of industry marketing.76 this information , observation strengthens the need to develop and provide access to performance indicators across different tumour types to inform patients decision making . 
performance indicators are publicly available for oesophageal and bowel cancer surgery in the nhs.77 , 78 additionally , the national prostate cancer audit has completed a national patient reported outcome measures ( proms ) collection exercise for men following radical surgery or radiotherapy , with the aim of reporting risk - adjusted outcomes at the individual hospital level.79 public reporting of outcomes would mean improvement could be stimulated through hospitals competing for market share or aiming to avoid reputational losses.80 , 81 that quality including finally , the configuration of cancer services needs to account for existing patterns of patient mobility , hospital capacity , catchment areas , and clinical quality . 
to this end , location - allocation modelling provides a rigorous empirical approach to optimising the configuration of health - care services ( including decisions about service centralisation ) .82 , 83 for example , it can guide which centres should close to maximise outcomes , or minimise travel distances for those individuals who face difficulties in accessing services because of financial and physical constraints.82 , 84 a limitation of our study is that we used centroids of the lsoas as the representation of the patients residence . 
it is likely that this noise has attenuated rather than enhanced the observed relationships between spatial competition and technology adoption on the one hand and patient mobility on the other . influence on in conclusion , we show that patient choice and hospital competition can have a major the configuration of cancer services . 
all authors were involved in revising the work critically and approved the final version . declaration of interests jvdm reports grants from healthcare quality improvement partnership during the conduct of the study . 
the views expressed in this publication are those of the authors and not necessarily those of the nhs , the national institute for health research , or the department of health . 
we thank graham davies for his valuable comments and insights during the drafting of the manuscript . * krzysztof bujko , rafa sopyo i department of radiotherapy ( kb ) and department of surgery ( rs ) , m skodowska - curie memorial cancer centre , 02 781 warsaw , poland ( kb ) bujko@coi.waw.pl we declare no competing interests . ngan sy , burmeister b , fisher rj , et al . 
randomized trial of short - course radiotherapy versus long - course chemoradiation comparing rates of local recurrence in patients with t3 rectal cancer : trans - tasman radiation oncology group trial 01.04. 
effect of interval ( 7 or 11 weeks ) between neoadjuvant radiochemotherapy and surgery on complete pathologic response in rectal cancer : a multicenter , randomized , controlled trial ( greccar - 6 )  . 
 although this advice seems reasonable , the stockholm iii trial does not support this because 30 - day and 90 - day postoperative mortality was not decreased after delaying surgery ; 3 , 5 however , only a fourth of patients in this trial were older than 75 years . 
 one small prospective trial reported acute toxicity in 27% of patients in the short - course radiotherapy with delayed surgery group and in 64% of patients in the chemoradiation group ( p = 0001 ) .8 other trials investigating short - course radiotherapy with delayed surgery also reported lower frequencies of acute radiation toxicity compared with that usually observed after chemoradiation.3 , 6 , 9 of note , about 1% mortality due to chemoradiation toxicity has usually been reported , whereas to our knowledge , no mortality attributed to short - course radiotherapy has ever been described . 
simple digital rectal examination became the sole method for the assessment of response among these patients 276 vol 18 march 2017 comment without the requirement for complex , elaborate , or expensive studies to rule out the presence of microscopic disease . 
despite the inherent differences between anal and rectal cancers , this approach was considered years later to be applicable to patients with very distal rectal adenocarcinomas that had a complete clinical response after being treated with a chemoradiotherapy regimen similar to that used for anal cancer.4 however , nigros original findings and observational treatment approach endured slower acceptance in the clinical rectal oncology community . 
 these rectal cancers are located centimetres away from the anus and have been only recently more widely considered for an organ - preserving strategy without immediate radical surgery after a complete clinical response.5 , 6 the understanding of in the lancet oncology , robert glynne - jones important and colleagues , 7 , 8 provide an additional contribution in - vivo kinetics of anal tumour response to neoadjuvant chemoradiotherapy . 
the observation that the ideal interval to assess tumour response is 26 weeks is remarkable and a leap forward in clinical practice for the management of these patients , especially considering that this interval was formerly only 8 weeks.9 besides the issue of timing of assessment , the present study draws attention to a very interesting observation . 
 not only were patients unharmed by rather long periods of time without a definitive conclusion ( complete versus incomplete response ) , but were not prematurely given unnecessary surgical resection . 
ultimately , the inherent subjectivity of clinical response assessment and the variation in examiners and specific tools for assessment of response incorrectly might have accounted for some complete clinical responses being incomplete clinical response in the early intervals . 
furthermore , these results and the kinetics of tumour regression after neoadjuvant chemoradiotherapy and the accuracy of clinical assessment might not be unique to anal carcinoma and might again apply , at least to some extent , to rectal adenocarcinoma after neoadjuvant chemoradiotherapy . 
 * angelita habr - gama , guilherme pagin so julio , rodrigo oliva perez colorectal surgery division , university of so paulo , so paulo , brazil ( ah - g ) ; and gastroenterology department , angelita and joaquim gama institute , so paulo 04001 - 005 , brazil ( ah - g , gpsj , rop ) we declare no competing interests . the author ( s )  . 
 int j radiat oncol biol phys 2003 ; 56 : 125973 . vol 18 march 2017 comment corrections published online september 4 , 2014 s1470 - 2045 ( 14 ) 70239 - 6 correction to lancet oncol 2014 ; 15 : 1039 correction to lancet oncol 2014 ; 15 : 110918 correction to lancet oncol 2014 ; 15 : 114756 streams the lancet oncology . 
lancet oncol 2014 ; 15 : 1039in this editorial , the third and fourth sentences of the second paragraph should have read , this is not the rst time a pharmaceutical company has tried to maintain revenue the face of a declining pipeline and expiring patents . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy in research and development . 
we apologise for this error , which has been corrected online as of sept 4 , 2014 . investment correction to lancet oncol 2014 ; 15 : 1047 roobol mj , bokhorst lp . 
the protect trial : what c an we expect ? lancet oncol 2014 ; 15 : 104647in this comment , the last sentence in the second - tolast paragraph should have stated the 10 - year prostate cancer survival reported surveillance cohorts , with more similar tumour characteristics , ranges from 96100% . 
lancet oncol 2014 ; 15 : 104748in this comment , the fourth sentence of the second paragraph should read crizotinib was superior to chemotherapy as secondfor alk - positive line nsclc , with similar response rate and progression - free survival to the phase 1 trial.3. 
in table 3 , the rst footnote should have stated * one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
in table 4 , the second footnote should also have stated one person was aged 49 years when the primary care list was generated , but tted the stated inclusion criteria as per protocol . 
these corrections have been made to the online version as of sept 29 , 2014 . correction to lancet oncol 2014 ; 15 : 1239 seto t , kato t , nishio m , et al . 
erlotinib alone or with bevacizumab as rst - line therapy in patients with advanced nonsquamous non - small - cell lung cancer harbouring egfr mutations ( jo25567 ) : an open - label , randomised , multicentre , phase 2 study . 
lancet oncol 2014 ; 15 : 123644in gure 3 of this article ( published on aug 28 , 2014 ) , under the age ( years ) subheading , the rst subgroup should read < 75 . 
 this correction has been made to the online version as of sept 29 , 2014 , and the printed version is correct . fizazi k , scher hi , miller k , et al . 
e ect of enzalutamide on time to rst skeletalrelated event , pain , and quality of life in men with castration - resistant prostate cancer : results from the randomised , phase 3 affirm trial . 
lancet oncol 2014 ; 15 : 114756in the methods section of the summary , rst skeletal - related events should have been de ned as radiation therapy or surgery to bone , clinically apparent pathological bone fracture , spinal cord compression , or change of antineoplastic therapy to treat bone pain , and the nal sentence of the findings in the summary should have read patients in the enzalutamide group had longer median time to hrqol deterioration than did those in the placebo group ( 90 months , 95% ci 83111 , vs 37 months , 95% ci 3042 ; hr 045 , 95% ci 037055 ; p < 00001 )  . 
 in table 2 of this article , the number and percentage for the placebo group in the row for both bone and soft tissue disease localisation at screening should have been 241 ( 60% )  . 
the second sentence of the sixth paragraph of the results should have read compared with placebo , enzalutamide resulted in a signi cant increase in the time to pain progression ( median not yet reached [ 95% ci not yet reached to not yet reached ] in the enzalutamide group vs 138 [ 138 to not yet reached ] months in the placebo group , hr 056 [ 95% ci 041078 ] ; p = 00004 ; gure 3 )  . 
these corrections have been made to the online version as of sept 29 , 2014 . vol 15 october 2014 e475 bermuda cancer and health centre , and bermuda hospitals board , hamilton dv04 , bermuda ( c fosker mbchb ) christopher.fosker@bhb.bm i declare no competing interests at bchc , our clinical radiation team is very small : one physician , one physicist , three radiation therapists , and two nurses . 
the normal workflow of day - to - day work has altered drastically in weeks , moving to video consulting , scheduling staff rotas to minimise the risk of infection between team members , procuring personal protective equipment , and developing protocols for its use . 
we do our clinical treatment reviews as we collect patients from the car park one at a time , and escort them directly to the radiation medical linear accelerator ( linac ) machine . 
these new measures are all out of our normal comfort zone , but patients are as equally adaptable as the staff . although some of our new approaches are unique to our setup , decisions we have had to make in real time have been validated when protocols and guidance established elsewhere , including by the royal college of radiologists in the uk and the american college of radiology , have reached the same conclusions . 
bchc has a clinical collaboration with the dana - farber / brigham and womens cancer center ( boston , ma , usa ) and they have been incredibly helpful . beyond the focus on oncology , a group of local primary care physicians have set up a group email chat as a forum for information sharing for all physicians on the island . 
 the group email very quickly showed that the challenges being faced across all specialties were very similar and that we could learn and share a huge volume of ideas across the group . 
the conversation also exposed the challenges of an art of medicine covid - 19 and cancer care in bermuda bermuda is a very small island nation with a population of 62 400 people , located in the middle of the atlantic ocean . 
a high - income country with the third highest healthcare spending per capita in the world , it has close medical links to numerous top - ranked us hospitals and government ties to the uk . 
that was even before bermuda joined the world in trying to find a way to fight the coronavirus disease 2019 ( covid - 19 ) pandemic . there is no doubt that there are many places around the world with a more challenging situation than we find ourselves in bermuda . 
however , our geographical isolation combined with our very small population and small medical workforce means there is a sense of vulnerability that we probably share with other small island nations . 
 furthermore , our health - care system is generally not very integrated and collaboration between the public and private sectors has been forced to ramp up rapidly . my usual role is medical director and radiation oncologist at a charity , bermuda cancer and health centre ( bchc ) , and medical oncologist at king edward memorial hospital ( kemh )  . 
during the pandemic , i have also stepped in as deputy chief of medicine at kemh while the chief of medicine , the islands only infectious diseases specialist , focuses on covid - 19 preparedness . 
 as the pandemic shifted from theory to reality , workflow changes and difficult decisions have had to be made quickly , but without the support of committees , think tanks , and researchers that a larger country can call on . the earliest example was a decision to suspend routine screening mammography even before our first confirmed case of covid - 19 . 
new contingency protocols for which cancer diagnostic imaging studies were crucial had to be developed , and rationalisation of cancer treatment priorities and timing decided . vol 21 june 2020 perspectives unstructured health - care system without a clear leadership framework . it was clear that numerous groups were looking at the same problems . 
responsibilities and formal and informal roles were shared across a previously disconnected group , and pathways such as procurement of personal protective equipment have become more centralised . as alterations in pathways of care become the new reality in everyday working life , they will require continual reassessment . 
we can only do that if we work together . christopher fosker 762 vol 21 june 2020 perspectives correction to lancet oncol 2019 ; 20 : 40819 correction to lancet oncol 2019 ; 20 : 125262 smith m , parker c , saad f , et al . 
 addition of radium - 223 to abiraterone acetate and prednisone or prednisolone in patients with castration - resistant prostate cancer and bone metastases ( era 223 ) : a randomised , doubleblind , placebo - controlled , phase 3 trial . 
this correction has been made to the online version as of sept 30 , 2019 . ieo and correction to lancet oncol 2019 ; 20 : 117182 nen nr , reisel d , leimbach a , et al . 
this correction has been made to the online version as of sept 30 , 2019 . correction to lancet oncol 2019 ; 20 : 137085 motzer rj , rini bi , mcdermott df , et al . 
nivolumab plus ipilimumab versus sunitinib in first - line treatment for advanced renal cell carcinoma : extended follow - up of efficacy and safety results from a randomised , controlled , phase 3 trial . 
lancet oncol 2019 ; 20 : 137085in figures 2 and 3 of this article , median and 95% ci data should have appeared in panel c and not in panel a . 
this correction has been made to the online version as of aug 21 , 2019 . published online august 21 , 2019 s1470 - 2045 ( 19 ) 30542 - x vol 20 october 2019 e559 corrections reflection & reaction is a possibility of breast cancer as a result of smoking and that the risk is higher in those women who start to smoke while teenagers . 
 pankaj chaturvedi department of surgery , tata memorial hospital , mumbai , india . corrections correction to lancet oncol 2012 ; 13 : 817 , 818 , 822 correction to lancet oncol 2014 ; 15 : 1195206 correction to lancet oncol 2015 ; 16 : 52 shen q , fan j , yang x - r , et al . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
the protocol , drawn up in 1997 and o cially enforced from 2005 , required 37 industrialised nations , plus the european community , to reduce their greenhouse gas emissions by 2012 , to achieve a worldwide decrease of 52% compared with concentrations in 1990 . 
although 192 countries rati ed the protocol ( the usa being a notable exception ) , many countries that were classed as rapidly developing at the time of its draftingincluding india and china were exempt . incidence of non - communicable disease the need for countries to act on climate change is enshrined in one of the uns sustainable development goals ( sdg 13 ) , which calls on countries to take urgent action to combat climate change and its impact . 
unexpected or unseasonally heavy rain can lead to ooding , which can release potentially carcinogenic environment from contaminated groundwater by washing over industrial sites or through over ow of sewage . 
 data are already showing that those that had been locked into cold water and arctic ice are now coming out of solution , and are being released into the air as the oceans warm and polar ice melts . chemicals into the climate immediate human change will have costs . 
changing weather patterns could increase food instability ( eg , through drought , or spoiled or contaminated crops ) and in turn , food security concerns might precipitate the increased use of more intensive farming practices , including greater use of carcinogenic pesticides and preservatives . 
finally , climate change risks increasing the numbers of dispossessed peoples in the world , with people eeing either from natural encroachment on their homes by ooding , or from uninhabitable conditions . 
such climate refugees would not fall under any jurisdiction for health care and there is clear evidence of the extremely poor health care , including cancer services , such migrants receive . implementation of the reductions in greenhouse gas emissions would thus not only protect against future burdens , but could also have an immediate bystander e ect by in uencing the activities of heavy polluting industries . 
for example , greenhouse emissions from industry are often released in combination with other carcinogenic pollutantseg , particulate matter between 25 m and 10 m in size , which is signi cantly associated with an increased risk of developing lung cancer . 
the 25 m particulate matter concentration , as recorded by the us embassy in beijing , was reported to be 256 g / m3more than ten times higher than the uns safe limit of 25 g / m3 . climate change is a global problem that needs a global solution . 
the lancet commission on planetary health identi ed poor governance ( de ned as implementation failures ) as an issue that must be addressed if we are to maintain or improve human health in the face of harmful environmental change . 
 the aim of the 2015 paris talksencouraging countries to agree to reduce emissions to the extent that global temperatures increase by no more than 2cneeds all countries to accept responsibility without self - interest : our health , and that of future generations , depends on it . 
 the lancet oncology vol 17 january 2016 editorial for the coa report see userfiles / les / community_ oncology_practice_impact_ report_4 - 4 - 12f%281%29%281 %29.pdf for the avalere study see communityoncology.org / userfiles / les / avalere_cost%20 of_cancer_care_studyf.pdf to nd out more about the macmillan campaign see getinvolved / campaigns / countingthecostofcancer / countingthecostofcancer.aspx for the regional cancer care association see rc2acancercare.com / are patients counting the cost of the economic downturn ? impossible to the continuing global economic crisis remains far reaching and ignore . 
whether this will prove to be bene cialboth for the balance sheet and , more importantly , to the patientswill depend on the regional context and how the process is managed . on april 4 , 2012 , the community oncology alliance ( coa ) , a non - pro t organisation dedicated to community oncology in the usa , published an update to their practice impact report , showing that in the past 45 years , nearly 700 oncology practices and clinics across the usa closed or are struggling nancially , with many private oncology practices being bought out or consolidated into a hospital setting . 
the act changed the way in which medicare and medicaid pays for prescription drugs , with oncology practices seeing a signi cant reduction in payment for chemotherapy agents which often does not cover the cost of the drugs . 
the consequences of this act are far - reaching , with many private insurance companies following this lead , resulting in further di culties for cancer - care providers . for oncology services that are still being provided , those in a hospital setting potentially result in increased costs when compared with private clinics . 
a study by the healthcare research company avalere health , commissioned by the coa , found that treatment for patients receiving chemotherapy in a hospital outpatient environment costs an average of 24% more than those who receive the same treatment in a private oncology clinic . 
however , the study was unable to determine whether the level of care requirements were higher in hospitals . at the personal level in the usa , cancer patients often nd themselves left without a safety net if they eventually become too ill to work . 
 hospital closures in the uk and other countries have lead to a consolidation of care which has been blamed for increasing the nancial burden on cancer patients , mainly via increased transport costs to and from clinics to see oncologists . 
complaints about regional variation for the funding of cancer drugs and a lack of choice add further complexities to an over - burdened syste the uk charity macmillan cancer support has highlighted the concerns to patients in a recent report , and are working with the nhs in wales to ensure that all cancer patients are provided with advice to help them cope with increased nancial stra there can , however , be bene ts gained from a consolidation of care . 
in some health - care systems , organised groups of clinicians have better purchasing power to broker more favourable deals with drug companies and suppliers , and integration of care within a hospital group or within a private company does not necessarily mean a shrink in geographical coverage or levels of provision . 
the formation of the regional cancer care associates ( rc2a ) in new jersey , usa , is potentially an early indication on how consolidation can be done for the bene t of the patient . 
this large company works to one standard at all sites to provide a transparent standard of care , improve access for patients to clinical trials , and to reduce over - testing and over - treatment . it is clear that the consolidation of cancer care will continue , with both public and private health care systems a ected . 
although there are pros and cons to any structural reorganisation , it is imperative that all decisions are thought through carefully to ensure that above all patient care is not a ected , and second that any cost savings are not simply transferred to the patients own expenditure . 
 the lancet oncology vol 13 july 2012 weekly platinum - based chemotherapy versus 3 - weekly platinum - based chemotherapy for newly diagnosed ovarian cancer ( icon8 ) : quality - of - life results of a phase 3 , randomised , controlled trial sarah p blagden , adrian d cook , christopher poole , lesley howells , ian a mcneish , andrew dean , jae - weon kim , dearbhaile m odonnell , jane hook , elizabeth c james , ian r white , timothy perren , rosemary lord , graham dark , helena m earl , marcia hall , richard kaplan , jonathan a ledermann , andrew r clamp summary background the icon8 study reported no significant improvement in progression - free survival ( a primary endpoint ) with weekly chemotherapy compared with standard 3 - weekly treatment among patients with epithelial ovarian cancer . 
 all icon8 patients were eligible to take part in the accompanying health - related quality - of - life study , which measured the effect of treatment on self - reported wellbeing , reported here . methods in this open - label , randomised , controlled , phase 3 , three - arm , gynecologic cancer intergroup ( gcig ) trial done at 117 hospital sites in the uk , australia , new zealand , mexico , south korea , and republic of ireland , women ( aged at least 18 years ) with newly diagnosed , histologically confirmed international federation of gynecology and obstetrics stage iciv ovarian cancer and an eastern cooperative oncology group performance status of 02 were randomly assigned ( 1 : 1 : 1 ) centrally using minimisation to group 1 ( intravenous carboplatin area under the curve [ auc ] 5 or auc6 and 175 mg / m intravenous paclitaxel every 3 weeks ) , group 2 ( carboplatin auc5 or auc6 every 3 weeks and 80 mg / m paclitaxel weekly ) , or group 3 ( carboplatin auc2 weekly and 80 mg / m paclitaxel weekly )  . 
patients were asked to complete european organisation for research and treatment of cancer qlq - c30 and qlq - ov28 questionnaires at enrolment , before each chemotherapy cycle , then 6 - weekly up to 9 months , 3 - monthly up to 2 years , and 6 - monthly up to 5 years . 
within the quality - of - life study , the co - primary endpoints were qlq - c30 global health score at 9 months ( cross - sectional analysis ) and mean qlq - c30 global health score from randomisation to 9 months ( longitudinal analysis )  . 
the trial is registered on clinicaltrials . gov , nct01654146 and isrctn registry , isrctn10356387 , and is currently in long - term follow up . findings between june 6 , 2011 , and nov 28 , 2014 , 1566 patients were recruited into icon8 ( 522 were included in group 1 , 523 in group 2 , and 521 in group 3 )  . 
baseline quality - of - life questionnaires were completed by 1438 ( 92% ) of 1566 patients and 9 - month questionnaires by 882 ( 69% ) of 1280 patients . 
we observed no significant difference in global health score at 9 months ( cross - sectional analysis ) between study groups ( group 2 vs group 1 , difference in mean score 23 , 95% ci 04 to 49 , p = 0095 ; group 3 vs group 1 , 08 , 38 to 22 , p = 061 )  . 
using longitudinal analysis , we found lower global health scores for those receiving weekly paclitaxel than for those receiving 3 - weekly chemotherapy ( group 2 vs group 1 , mean difference 18 , 95% ci 36 to 01 , p = 0043 ; group 3 vs group 1 , 29 , 47 to 11 , p = 00018 )  . interpretation we found no evidence of a difference in global quality of life between treatment groups at 9 months ; however , patients receiving weekly treatment reported lower mean quality of life across the 9 - month period after randomisation . 
taken together with the lack of progression - free survival benefit , these findings do not support routine use of weekly paclitaxel - containing regimens in the management of newly diagnosed ovarian cancer . funding cancer research uk , medical research council , health research board ireland , irish cancer society , and cancer australia . copyright 2020 the author ( s )  . 
 the japanese jgog - 3016 study reported improved survival outcomes with no detriment to quality of life in patients with newly diagnosed ovarian cancer for weekly , dose - dense , paclitaxel and 3 - weekly carboplatin , compared with standard 3 - weekly carboplatin and paclitaxel . 
the gog - 0262 study compared similar dose schedules , but most patients also received bevacizumab , and the study reported no progression - free survival benefit and poorer quality of life with weekly treatment compared with 3 - weekly treatment . 
 the mito - 7 study compared weekly carboplatin plus weekly paclitaxel with 3 - weekly carboplatin plus 3 - weekly paclitaxel and reported improved quality of life with weekly treatment over the 9 - week evaluation period . 
the evidence from these three studies was that weekly paclitaxel - containing treatment was superior to , or at best equivalent to , standard 3 - weekly treatment with little quality - of - life detriment to patients . added value of this study to our knowledge , icon8 is the largest study to date of weekly treatment for primary ovarian cancer . 
the quality - of - life results show that , although the global quality of life of patients was similar between the three treatment groups at 9 months , those receiving dose - dense paclitaxel had poorer quality of life during chemotherapy treatment , with more severe peripheral neuropathy that lasted for up to 18 months . patients could have either immediate primary debulking surgery followed by chemotherapy or upfront chemotherapy that was interrupted by delayed primary surgery ; patients who had delayed surgery reported less detriment to quality of life with weekly treatment than did patients with immediate surgery . implications of all the available evidence the contrasting results of icon8 and jgog - 0316 support a differential response to dose - dense paclitaxel between asian and white patients . 
with no progression - free survival benefit and poorer quality of life , the icon8 results do not support the general use of weekly treatment among a primarily european population . 
the study was prompted by the phase 3 jgog - 3016 trial in which weekly paclitaxel ( 80 mg / m ) in combination with 3 - weekly carboplatin ( area under the curve [ auc ] 6 ) was found to confer improved progression - free survival and overall survival when compared with standard treatment in japanese patients with advanced ovarian cancer.1 as there is increasing evidence of pharma cogenomic distinctions between asian and white populations , icon8 was designed to explore whether the survival advantage observed in jgog - 3016 could also be observed in a mostly european population with ovarian cancer.2 , 3 results from icon8 have shown that weekly , dose - dense paclitaxel - containing conferred no progression - free survival advantage when com pared with standard 3 - weekly treatment.4 as a secondary endpoint of the main study , the effect on health - related quality of life ( referred to as quality of life throughout this article ) was assessed during treatment and in follow - up . 
here we report the quality - of - life results from the icon8 study . chemotherapy methods study design and participants icon8 was an open - label , randomised , controlled , phase 3 , three - arm trial done at 117 hospital sites in the uk , australia , new zealand , mexico , south korea , and republic of ireland ( appendix pp 13 )  . 
detailed methods for icon8 have been previously reported.4 eligible patients were aged 18 years or older and had histologically confirmed , newly diagnosed high - risk international feder ation of gynecology and obstetrics ( figo ) stage ic - iia or any advanced ( figo stage iib - iv ) epithelial ovarian , primary peritoneal , or fallopian tube carcinoma ( collectively termed ovarian cancer )  . 
 other inclusion criteria were an eastern cooperative oncology group ( ecog ) performance status of 02 ; life expectancy longer than 12 weeks ; adequate haematological , renal , and hepatic function ; and able to start chemotherapy within 8 weeks after immediate primary debulking surgery . 
all patients gave written informed consent to join the trial . exclusion criteria included previous malignancy within 5 years , previous or synchronous early - stage endometrial 970 vol 21 july 2020 articles for the study protocol see studies / all - studies / i / icon8 / cancer , evidence of brain metastasis , and pre - existing sensory or motor neuropathy of grade 2 or above . in the uk , ethical approval was granted by the london chelsea research ethics committee . 
 the protocol can be found online . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to standard threeweekly carboplatin and paclitaxel ( group 1 ) , three - weekly carboplatin and weekly dose - dense paclitaxel ( group 2 ) , or weekly carboplatin and weekly dose - dense paclitaxel ( group 3 ; appendix p 4 )  . 
patients were randomly assigned with the medical research council clinical trials unit university college london randomisation telephone service ; the method of minimisation was used with stratification factors of gcig group , disease stage ( figo stage ic high grade serous , clear cell , or grade iii carcinoma ; stage iia high grade serous , clear cell , or grade iii carcinoma ; stage iib ; stage iic ; stage iiia ; stage iiib ; stage iiic ; stage iv ) , and outcome and timing of surgery ( immediate surgery plus figo stage iciii with no visible residual disease ; immediate surgery plus figo stage iciii with residual disease 1 cm ; immediate surgery plus figo stage iv or iciii with residual disease > 1 cm ; no surgery currently planned ; or delayed primary surgery planned )  . 
patients and clinicians were not masked to their allocated group . procedures patients entering the trial could have upfront debulking surgery before starting chemotherapy , referred to as immediate primary surgery , delayed primary surgery after at least three cycles of neoadjuvant chemotherapy , or no planned surgery . 
patients in group 1 received carboplatin area under the curve [ auc ] 5 or auc6 by intravenous infusion over 3060 min and paclitaxel 175 mg / m by intravenous infusion for 3 h on day 1 of a 21 - day cycle for six cycles ; patients in group 2 received carboplatin as in group 1 and dose - fractionated paclitaxel 80 mg / m by intravenous infusion for 1 h on days 1 , 8 , and 15 of a 21 - day cycle for six cycles ; and patients in group 3 received carboplatin auc2 by intravenous infusion for 3060 min on days 1 , 8 , and 15 and paclitaxel 80 mg / m by intravenous infusion for 1 h on days 1 , 8 , and 15 of a 21 - day cycle for six cycles . 
additional details regarding treatment have been published.4 protocoldefined dose alterations ( delay , reduction , or omission ) were allowed for haematological and other toxic effects if deemed clinically necessary , as described previously.4 all patients were included in the quality of life study and invited to complete european organisation for research and treatment of cancer qlq - c30 and qlq - ov28 questionnaires to provide a subjective measure of their quality of life over the preceding 7 days . 
the qlq - c30 contains 30 items , including a global health status score , five function scales ( physical , role , emotional , cognitive , and social ) and nine symptom scales or items ( fatigue , nausea or vomiting , pain , dyspnoea , insomnia , appetite loss , constipation , diarrhoea , and financial difficulties ) .5 the qlq - ov28 contains 28 items relevant to ovarian cancer , including abdominal or gastrointestinal symp toms , peripheral neuropathy , chemotherapy side - effects , hormonal or menopausal symptoms , body image , attitude to disease or treatment , and sexual functioning.6 for global health status and function scales , higher scores indicate better function ( improved quality of life ) but for symptom scales , higher scores indicate greater symptoms ( poorer quality of life )  . 
the qlq - c30 and qlq - ov28 questionnaires have undergone extensive psychometric validation and multiple translations and are acceptable to patients.57 we interpreted a change in global health score over time of more than 5 points as being clinically significant following the methodology of cocks and king , who defined a change in the score of less than 5 as clinically trivial.810 qlq - c30 and qlq - ov28 questionnaires were completed during outpatient attendances at day 1 of each chemotherapy cycle and during follow - up visits 6 - weekly until 9 months from randomisation , 3 - monthly to 2 years from randomisation , and then 6 - monthly for up to 5 years from randomisation ( figure 1 )  . 
 centres were asked to report reasons for any missing questionnaires . outcomes the trial had co - primary endpoints of progression - free survival and overall survival , which have been previously reported.4 a secondary outcome , quality of life , is reported here . 
the quality - of - life study comprised two coprimary endpoints : cross - sectional analysis of qlq - c30 global health score 9 months after randomisation and longi tudinal analysis of qlq - c30 global health score from randomisation to 9 months . 
secondary quality - oflife endpoints were defined from four clinically relevant function and symptom scores , as follows : qlq - c30 emotional function , qlq - c30 social function , qlq - c30 fatigue , and qlq - ov28 peripheral neuro pathy . 
 analyses of all other function and symptom scores up to 18 months after randomisation were treated as exploratory . vol 21 july 2020 articles immediate primary surgery 6 weekly 3 monthly 6 monthly screening surgery follow - up delayed primary surgery screening surgery screening follow - up time since randomisation chemotherapy cycle debulking surgery quality - of - life assessment figure 1 : timing of quality - of - life questionnaires statistical analysis the sample size of icon8 was determined to detect a hazard ratio of 075 in progression - free survival between groups 1 and 2 , and groups 1 and 3 , with two - sided 25% significance and 90% power . 
for quality of life , a retrospective power calculation showed that the study had 90% power to detect a difference between groups of 5 points in global quality of life using the sd observed in group 1 . 
a quality - of - life expert panel ( comprised of lh , cp , spb , and rk ) , invited by the trial management group , convened on june 9 , 2016 , to define the primary , secondary , and exploratory endpoints . we compared each weekly treatment group with the 3 - weekly group , following the main analysis of clinical endpoints ( group 2 vs group 1 , and group 3 vs group 1 )  . 
to adjust for two comparisons against the same control group , we used a two - sided significance level of p = 0025 to judge statistical significance in primary and secondary analyses . 
descriptive data are presented for all other validated subscales of the qlq - c30 and qlq - ov28 . for cross - sectional comparisons of quality - of - life outcomes at 9 months , we used analysis of covariance adjusted for baseline score , hence omitting data from the chemotherapy period . 
longitudinal analyses used all data collected from baseline to 9 months ; we estimated scores at scheduled data collection points from a mixed effects regression model with a timetreatment interaction , unstructured covariance , and patient level random effects . 
the 9 - month timepoint was chosen as it represents a period of good quality of life for most patientsfew will have had disease progression , and most will have completed treatment some months earlier . 
the co - primary endpoints of cross - sectional and longitudinal changes in global health score are complementarylongitudinal analysis compares patient experience across the whole 9 - month period and crosssectional analysis compares scores at the 9 - month timepoint . 
thus , longitudinal analysis makes better use of the data and is the preferred method , whereas crosssectional analysis provides a post - treatment snapshot . for patients who had neo - adjuvant chemotherapy and underwent delayed primary surgery , chemo therapy cycles 4 to 6 and the end of treatment visit were around 4 weeks later than equivalent visits in the immediate surgery group . 
therefore , quality - of - life data were ordered by visit number rather than date . three post - hoc analyses were done : analysis of the primary and secondary outcomes separately for immediate surgery and delayed surgery patients ( including a comparison of baseline quality of life scores ) , a comparison of peripheral neuropathy scores from selfreported quality - of - life data with neuropathy adverse event data from clinicians ( according to common terminology criteria for adverse events version 4.0 ) , 4 and analysis of self - reported peripheral neuropathy scores 18 months after randomisation . we assessed the potential effect of missing data on the co - primary outcome using imputation to model the following scenarios : scenario 1 , a global score of 0 was imputed for patients who died within 9 months of enrolment ; scenarios 24 , all patients alive and without progression at 9 months but missing quality - of - life data were assigned a score , starting respectively with the mean 9 - month score , then the mean score minus 10 points , then mean minus 20 ; scenario 5 , a global score of 0 was imputed for patients who died within 9 months , all other patients ( including those with disease progression ) with a baseline global quality - of - life score but 972 vol 21 july 2020 articles missing their 9 - month global quality - of - life score were assigned the mean 9 - month score . 
the rationale for scenarios 24 was that patients might have missed submitting their questionnaires due to illness , in which case a lower quality of life would be expected . all analyses were done on an intention - to - treat basis with stata version 15.0. 
the trial is registered on clinicaltrials.gov , nct01654146 and isrctn registry , isrctn10356387 . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the trial management group had final responsibility for the decision to submit for publication . results between june 6 , 2011 , and nov 28 , 2014 , 1566 patients were recruited into icon8 ( 522 were included in group 1 , 523 in group 2 , and 521 in group 3 )  . 
baseline characteristics are described elsewhere.4 all patients were invited to partici pate in the quality - of - life study , and 1540 patients com pleted 17 515 quality - of - life questionnaires . 
9 months after randomisation , quality - of - life data were expected from 1280 patients in follow - up without disease progression ; 39 patients had died , 230 were alive after progression , and 17 had withdrawn or been lost to follow - up without progression . 
baseline questionnaires were completed by 1438 ( 92% ) of 1566 patients and 9 - month questionnaires by 882 ( 69% ) of 1280 patients ( table 1 )  . 
828 ( 65% ) of 1280 patients who could have contributed quality - of - life data at 9 months had both baseline and 9 - month data and were included in crosssectional analyses of primary and secondary outcomes . at the 9 - month timepoint we found no significant difference in qlq - c30 global health score between the three treatment groups with cross - sectional analysis ( group 2 vs group 1 , n = 555 , mean difference 23 , 95% ci 04 to 49 , p = 0094 ; group 3 vs group 1 , n = 522 , mean difference 08 , 38 to 22 ; p = 061 ; table 2 )  . 
we observed an improvement in mean global health score from baseline to 9 months post - random isation across the study population ( figure 2 ) , although a fall in global health score was observed during chemotherapy in all three treatment groups . 
with longitudinal analysis , mean global health scores across the 9 - month period were lower among patients in the weekly treatment groups , with a significant difference between group 3 and group 1 ( group 2 vs group 1 , 926 patients had global health score at baseline , and at least one score between baseline and 9 months , mean difference 18 , 95% ci 36 to 01 , p = 0043 ; group 3 vs group 1 , n = 915 patients had global health score at baseline , and at least one score between baseline and 9 months , mean difference 29 , 47 to 11 ; p = 00018 ; table 2 )  . 
 we found no difference in social functioning ( qlq - c30 ) between treatment groups using either cross - sectional or longitudinal analyses ( table 3 ; figure 2 )  . 
we observed no difference in fatigue ( qlq - c30 ) between groups by cross - sectional analysis ; although fatigue scores were significantly different between the weekly ( group 2 ) and 3 - weekly ( group 1 ) treatment groups by longitudinal analysis , they did not meet the threshold for clinical signifi cance ( table 3 ; figure 2 )  . 
by cross - sectional analysis , peripheral neuropathy scores ( qlq - ov28 ) were statisti cally and clinically significantly different between group 2 and group 1 ; however , there was no difference by longitudinal analysis ( table 3 ; figure 2 )  . 
 vol 21 july 2020 articles global health score emotional function group 1 group 1 group 2 group 2 group 3 group 3 social function fatigue symptoms peripheral neuropathy symptoms baseline cycle 6 time 9 months baseline cycle 6 time 9 months figure 2 : primary and secondary quality - of - life endpoints for global health status and function scales ( qlq - c30 global health status , emotional function , and social function ) , higher scores indicate better function ( improved quality of life ) but for symptom scales ( qlq - c30 fatigue and qlq - ov28 peripheral neuropathy ) , higher scores indicate greater symptoms ( poorer quality of life )  . 
the number of expected questionnaires and received questionnaires is reported in the appendix ( p 5 )  . the timing of neuropathy differed between groups ( figure 2 )  . exploratory cross - sectional analyses of the other qlq - c30 and qlq - ov28 subscales showed that differences between the three randomised groups were generally small ( appendix pp 56 )  . 
we did not analyse data on sexual function since more than 80% of patients reported that they were sexually inactive at baseline . a post - hoc analysis of peripheral neuropathy scores showed that , for patients who remained in follow - up without progression , high scores were still observed 18 months after randomisation for all treatment groups ( appendix p 7 )  . 
there was a statistically and clinically significant difference between group 2 and group 1 ( n = 298 with neuropathy score at baseline and 18 months , mean difference 107 , 95% ci 42 to 172 ; p = 00012 ) but not group 3 and group 1 ( n = 316 patients in group 1 or group 3 with neuropathy score at baseline and 18 months , 48 , 09 to 104 ; p = 0096 ) by cross - sectional analysis . 
 longi tudinal analysis did not show significant differences between the groups ( group 2 vs group 1 , n = 898 patients with neuropathy score at baseline and at least one neuropathy score between baseline and 18 months , mean difference 25 , 95% ci 12 to 61 , p = 018 ; group 3 vs group 1 , n = 901 patients with neuropathy score at baseline and at least one neuropathy score between baseline and 18 months , 25 , 12 to 61 , p = 019 )  . post - hoc analyses were done to investigate differences in quality of life related to timing of surgery ( immediate primary surgery vs delayed primary surgery ; appendix pp 810 )  . 
qlq - c30 global health score at baseline was significantly lower among patients who had delayed surgery ( n = 714 ) than those who had immediate surgery ( n = 675 ) ( mean 562 [ sd 243 ] vs [ 216 ] ; p < 00001 )  . 
baseline emotional mean 617 function ( delayed surgery , n = 716 , mean 686 [ sd 236 ] ; immediate surgery , n = 673 , mean 736 [ 215 ] ; p < 00001 ) and fatigue ( delayed surgery , n = 720 , mean 423 [ sd 270 ] ; immediate surgery , n = 679 , mean 358 [ 229 ] ; p < 00001 ) were also significantly worse among patients who had delayed surgery , but we observed no difference in baseline scores for social function or peripheral neuropathy between patients with different surgery timings ( data not shown )  . 
for patients who had immediate surgery , longi tudinal analysis of the global health score over 9 months mirrored that in the overall study population ( appendix pp 810 )  . 
however , among patients the difference between who had delayed surgery treatment groups was smaller than it was in the overall study population ( appendix pp 810 )  . we did a post - hoc analysis to assess concordance between self - reported peripheral neuropathy from the quality - of - life questionnaires and clinician - assessed peripheral neuropathy reported during the treatment period ; there was good agreement between the measures ( appendix p 12 )  . 
sensitivity analyses to assess the potential effect of missing data did not alter our interpretation of the data ( appendix p 13 )  . discussion the primary outcome of this study showed no difference between treatment groups in global health score at 9 months compared with baseline . 
however , longitudinal analysis revealed lower global health scores during chemotherapy for those in the weekly treatment groups than for those in the 3 - weekly treatment group , which , although statistically significant , was of marginal clinical significance . 
these findings indicate that patients receiving weekly paclitaxel - containing chemotherapy had slower improvement in their overall quality of life during treatment itself , but recovered to a similar level to those receiving 3 - weekly treatment at 9 months . 
other 974 vol 21 july 2020 articles secondary outcomes revealed slightly worse fatigue and more persistent peripheral neuropathy in the weekly paclitaxel - containing groups than in the 3 - weekly group , although other quality - of - life subscores were similar between the study groups . 
patients in the 3 - weekly treatment group had an earlier onset of , but more rapid improvement in , peripheral neuropathy symptoms after completion of chemotherapy than did patients in the weekly treatment groups . 
by contrast , symptoms of peripheral neuropathy developed more gradually for patients in the weekly treatment groups compared with the 3 - weekly treatment group but persisted beyond the end of treatment and into the follow - up period . the observed differences in these quality - of - life subscores are probably due to paclitaxel exposure . 
as with the jgog - 3016 and gog - 0262 studies , 11 , 12 patients in group 2 and group 3 of icon8 received up to 80 mg / m of paclitaxel per week , equivalent to 240 mg / m per cycle . 
by contrast , in the mito - 7 study , 13 a lower weekly dose of 60 mg / m paclitaxel was administered in the weekly group ( equivalent to 180 mg / m per cycle ) and lower neuropathy scores were reported in the weekly group compared to those in the 3 - weekly group ( who received a similar per cycle dose of paclitaxel ; appendix p 14 )  . 
these findings suggest that peripheral neuropathy could be caused by cumulative exposure to paclitaxel rather than dosing intensity , although the exact mechanism of taxane neurotoxicity remains incompletely understood . the large size of icon8 allowed comparison between the quality - of - life trajectories of patients who had immediate primary surgery and delayed primary surgery . 
 as the choice of upfront or delayed surgery was not randomly assigned , patients with more advanced - stage disease and poorer perfor mance status were selected for upfront chemo therapy and delayed surgery , intended to reduce their anaesthetic risk and allow chemotherapy downstaging . 
overall , patients who had delayed surgery had a larger incre mental improvement in quality of life from randomisation to 9 months than did patients with immediate surgery , although having started from a lower point this result might have been expected . 
by contrast , patients who had immediate surgery entered icon8 having recovered from surgery and with better quality of life ; although they had a quality - of - life nadir following chemotherapy ( at around 18 weeks ) , their quality of life recovered to the same level as those in the delayed surgery group at 9 months . 
we recommend this close method of tracking of quality of life , along with longitudinal rather than vol 21 july 2020 articles cross - sectional methods of analysis , to more accurately reflect changes over time . 
alternatively , standardised , continuous patient - reported outcome measures can be implemented to provide more reliable monitoring of the longer - term toxicities that affect patient wellbeing.12 because of the differences between non - randomised patients undergoing immediate or delayed surgery , we recommend that these two surgical groups are analysed separately in future quality - of - life studies . to our knowledge , icon8 provides the largest and most detailed quality - of - life dataset of any neoadjuvant ovarian cancer trial . 
a limitation of the study is the loss of qualityof - life data due to patients who did not complete or return their questionnaires , which poten tially introduced bias against those with more severe symptoms who might have been less able or willing to comply . 
questionnaire compliance was favourable compared with other similar studies ; baseline quality - of - life questionnaires were completed by 92% of patients in icon8 compared with 639% and 75% in the jgog - 3016 and mito - 7 studies , respectively . 
additionally , response shift is a limitation of quality - of - life studies , whereby patients adapt to and therefore underreport symptoms over time.14 as the main icon8 study revealed no progression - free survival advantage for weekly paclitaxel - containing regimens , our quality - of - life data do not support its use in favour of standard 3 - weekly carboplatin and paclitaxel after upfront surgery in ovarian cancer . 
however , our finding of no quality of life detriment between the groups among patients who had delayed surgery suggests that , in those unsuitable for upfront surgery , 3 - weekly and weekly schedules might be equivocal . 
in patients who have delayed surgery , who are likely to be in poorer health , the weekly scheduling of both carboplatin and paclitaxel allows more careful dosing modulation and symptom management than 3 - weekly dosing , and is equivalent to 3 - weekly dosing in terms of its effect on global quality of life . in conclusion , for patients undergoing upfront surgery , weekly paclitaxel - containing chemotherapy should not replace 3 - weekly carboplatin and paclitaxel as the standard of care for newly diagnosed ovarian cancer , since it neither improves progression - free survival nor is associated with improved quality of life . contributors spb , adc , ecj , cp , lh , and rk coordinated this study . 
spb and adc drafted the manuscript , the final version of which was approved by all coauthors . declaration of interests cp reports personal fees and non - financial support from pfizer , roche , genomic health , tesaro , and puma biotechnology , outside the submitted work . 
jal reports grants and personal fees from astrazeneca and merck sharp & dohme and personal fees from roche , clovis oncology , pfizer , and tesaro , outside the submitted work . 
arc reports grants from cancer research uk during the conduct of the study , grants , personal fees , and non - financial support from astrazeneca , non - financial support from clovis oncology , and personal fees from roche , outside the submitted work . 
all other authors declare no competing interests . data sharing data will be shared according to the medical research council clinical trial unit controlled access approach , based on the following principles : no data should be released that would compromise an ongoing trial or study ; there must be a strong scientific or other legitimate rationale for the data to be used for the requested purpose ; investigators who have invested time and effort into developing a trial or study should have a period of exclusivity in which to pursue their aims with the data , before key trial data are made available to other researchers ; the resources required to process requests should not be underestimated , particularly successful requests that lead to preparing data for release , therefore , adequate resources must be available to comply in a timely manner or at all , and the scientific aims of the study must justify the use of such resources ; and data exchange complies with information governance and data security policies in all of the relevant countries . 
we acknowledge experimental cancer medicines centres and national institute for health research biomedical research centre for support at icon8 uk centres . correction to lancet oncol 2020 ; 21 : 50818 correction to lancet oncol 2020 ; 21 : 34142 pishvaian mj , blais em , brody jr , et al . 
lancet oncol 2020 ; 21 : 50818.in this article , the x - axis label of figure 3b should have been time on therapy without disease progression ( months )  . 
this correction has been made to the online version as of march 30 , 2020 , and the printed article is correct . pagani bagliacca e , silva m , veneroni l , et al . 
this correction has been made to the online version as of march 30 , 2020 . vol 21 april 2020 e182 corrections corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 published online september 24 , 2020 s1470 - 2045 ( 20 ) 30584 - 2 for more on the two online surveys see org / meetings / esmo - virtualcongress - 2020 / daily - reporter / daily - reporter - news / covid19cancer - research for more on burnout rates among oncology physician assistants in the usa see record / 185959 / abstract for more on oncologists burnout in russia see record / 191626 / abstract for more on us oncologists burnout see j clin oncol 2014 ; 32 : 67886 for more on the cost of physician burnout in the usa see sections / health - shots / 2019 / 05 / 31 / 728334635 / whatsdoctor - burnout - costing - america burnout among cancer professionals during covid - 19 results released newly from two online surveys done by the european society for medical oncology ( esmo ) resilience task force have outlined the extent to which the covid - 19 pandemic has affected burnout , job performance , and wellbeing in the global oncology workforce . 
38% of respondents stated that they had experienced feelings of burnout and 78% had felt increased concern for their personal safety since the onset of the pandemic . july 16 the follow - up survey , which was done from aug 6 , 2020 , found that the proportion of respondents reporting feelings of burnout had risen to 49% . 
 but whereas 66% of respondents in the first survey felt unable to do their job as well as they had done before the pandemic , by the time of the second survey , this proportion had decreased to 49% . these results suggest oncology professionals are adapting to the covid - 19 circumstances with a better ability to manage patients with cancer during the pandemic , but a higher risk of distress and burnout , commented susana banerjee ( royal marsden national health service foundation trust and institute of cancer research , london , uk ) , lead author of the two surveys . the investigators found that as national covid - 19 mortality rates increased , wellbeing and job performance decreased . 
feeling burnout can take time to manifest itself , so i would not expect higher crude covid - 19 mortality rate alone at one timepoint to drive burnout , explained banerjee . 
 there was a lot of uncertainty and unpredictability and , at the time , we had very limited knowledge on the risks of covid - 19 for individual patients with cancer . 
as health - care systems prioritised patients with covid - 19 , referrals for suspected cancer dwindled , increasing the fear of delayed diagnosis and a pending increase in mortality . i think there is a sense of failure and helplessness associated with the pandemic that we have never experienced before , said tara sanft ( yale school of medicine , new haven , ct , usa )  . 
we are trying to manage patients with many more restrictions than we have in the past , and navigate care and communicate with families and teams , all mostly over the phone or video . oncologists are already at heightened risk of burnout , because they have to discuss lifechanging treatment decisions with patients , deliver bad news , and supervise therapies that can have adverse effects , which is not easy , particularly in an era of constrained resources . 
a poster presented at the american society of clinical oncology 2020 meeting noted that rates of burnout among oncology physician assistants in the usa increased from 35% in 2015 , to 49% in 2019 . 
a 2014 survey of more than 1100 us oncologists concluded that 45% had at least one symptom of burnout , although interestingly the same survey found that more than 80% of respondents were satisfied with their career and a similar proportion were satisfied with their specialty . 
there is a real risk of colleagues leaving the profession or early retirement and this impact on the workforce could affect patient care , banerjee told the lancet oncology . the majority of respondents to the esmo surveys believed that counselling and psychological support services would be helpful . 
 covid - 19 has meant that we had to do away with a lot of bureaucracy and hone in on what was important ; i hope systems can learn from this reprioritisation , she said . 
if we really want to address burnout we have to cut through all the red tape and get back to the business of taking care of the patient . talha khan burki 1402 vol 21 november 2020 news comment information about non - speci c side - e ects from providers and written material , such as those on consent forms and labels , without consideration of the nocebo e ect . for this model to work on behalf of patients , the risks and bene ts of a speci c treatment have to be completely unrelated to the act of information disclosure to the patient.8 although this notion might be true for some treatments , it is not uniformly applicable . 
with surgery , the outcome of treatment is more likely to be related to patient anatomy and surgical technique and less likely to be a ected by information exchange during the consent process . 
for example , a patient who develops insulin de ciency after undergoing surgery for pancreatic cancer can be counselled quite objectively that this risk is likely to manifest on the basis of the size of the tumour and location within the pancreas and is unlikely to be a ected by the act of disclosure of this risk to the patient before surgery . 
 for patients with cancer who undergo non - invasive treatments or are prescribed drugs associated with non - speci c side - e ects , the act of disclosure itself could a ect the possibility of side - e ect manifestation . 
 rather , in many clinical circumstances in which the potential for non - speci c side - e ects is high , such as in the non - invasive treatment of cancer , the act of information disclosure could be more accurately viewed as part of the riskbene t analysis , thus dependent on real - time discussion , and personalised to the patient . 
theor med bioeth 2011 ; 32 : 22943 . published online november 16 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70332 - 1 errata adams c , torode j , henshall s , cazap e , ryel al , grey n . 
lancet oncol 2011 ; 12 : 109192in this comment , the fourth sentence of the third paragraph should have read : who has committed to produce targets for its so - called best - buy interventions in time for the world health assembly in 2012 . 
these corrections have been made to the online version as of nov 25 , 2011 . 1182 vol 12 december 2011 correction to lancet oncol 2020 ; 21 : 64554 correction to lancet oncol 2020 ; 21 : 144354 correction to lancet oncol 2020 ; 21 : e51927 smith i , robertson j , kilburn l , et al . 
 long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial . 
lancet oncol 2020 ; 21 : e51927in this review , the second sentence of the first paragraph of the section entitled cancer burden now describing the number of new cancer cases worldwide in 2017 should read according to analysis from the global burden of disease study , there were 168 million new cases of cancer . 
this correction has been made to the online version as of nov 30 , 2020 . correction to lancet oncol 2020 ; 21 : 156373 powles t , plimack er , soulires d , et al . 
pembrolizumab plus axitinib versus sunitinib monotherapy as firstline treatment of advanced renal cell carcinoma ( keynote - 426 ) : extended follow - up from a randomised , openlabel , phase 3 trial . 
lancet oncol 2020 ; 21 : 156373in table 1 of this article the n ( % ) for previous nephrectomy should read 357 ( 83% ) for the pembrolizumab plus axitinib group and 358 ( 83% ) for the sunitinib group . 
these corrections have been made to the online version as of nov 30 , 2020 , and the printed version is correct . correction to lancet oncol 2020 ; 21 : e30516 fangusaro j , witt o , herniz driever p , et al . 
notably , this extension of treatment has translated into a durable remission , ongoing survival beyond 32 months , and maintenance of the patients quality of life and functional capacity . 
 to my knowledge , this case represents the rst , albeit anecdotal , report of preventing both cold - induced and cumulative psn in a patient receiving oxaliplat although dose - limiting toxicity has not yet been seen in this patient , his cumulative dose for second - line oxaliplatin already surpasses his rst use of the drug , and more than doubles the median of six cycles and 492 mg / m2 reported for the optimox ( oxaliplatin reintroduction ) strategy.8 , 9 such a de nitive and clinically meaningful bene t for the prevention of psn has not been possible by use of pharmacological measures , 6 which have been disappointing by comparison , or without risks to outcome , such as those associated with calcium - magnesium infusions.2 the challenge in con rming these ndings will be to design an appropriate trial . 
one that maximises use of the historical record of oxaliplatin - induced psn so as to avoid exposing patients to an inactive placebo might well be the most expedient route to improving the quality of life of thousands of patients who su er from this potentially preventable adverse event . 
 michael castro department of cancer medicine , st marys hospital , amsterdam , ny 12010 , usa mcastromd@yahoo.com the author declared no con icts of interest . gamelin l , boisdron - celle m , morel a , et al . 
e ect of intravenous ( iv ) calcium and magnesium ( ca / mg ) versus placebo on response to folfox + bevacizumab ( bev ) in the concept trial . 
2008 gastrointestinal cancers symposium ; orlando , fl , usa ; jan 2527 , 2008 ; abstract 280 . gamelin l , boisdron - celle m , delva r , et al . 
randomized double blind ( db ) placebo ( plcb ) controlled phase iii study assessing the e cacy of xaliproden ( x ) in reducing the cumulative peripheral sensory neuropathy ( psn ) induced by the oxaliplatin ( ox ) and 5 - fu / lv combination ( folfox4 ) in rst - line treatment of patients ( pts ) with metastatic colorectal cancer ( mcrc )  . 
 in this article , in tables 6 and 7 ( pages 78990 ) , some data for relative survival and 95% ci for prostate , kidney , and thyroid cancer , and nonhodgkin lymphoma were incorrect . 
 see online for webappendix 416 vol 9 may 2008 articles lancet oncol 2012 ; 13 : 114151 published online october 17 , 2012 s1470 - 2045 ( 12 ) 70425 - 4 see comment page 1071 * collaborators listed at end of paper correspondence to : secretariat , cancer epidemiology unit , richard doll building , oxford ox3 7lf , uk collaborations@ceu.ox.ac.uk see online for appendix menarche , menopause , and breast cancer risk : individual participant meta - analysis , including 118 964 women with breast cancer from 117 epidemiological studies collaborative group on hormonal factors in breast cancer * summary background menarche and menopause mark the onset and cessation , respectively , of ovarian activity associated with reproduction , and a ect breast cancer risk . 
our aim was to assess the strengths of their e ects and determine whether they depend on characteristics of the tumours or the a ected women . methods individual data from 117 epidemiological studies , including 118 964 women with invasive breast cancer and 306 091 without the disease , none of whom had used menopausal hormone therapy , were included in the analyses . 
 we calculated adjusted relative risks ( rrs ) associated with menarche and menopause for breast cancer overall , and by tumour histology and by oestrogen receptor expression . findings breast cancer risk increased by a factor of 1050 ( 95% ci 10441057 ; p < 00001 ) for every year younger at menarche , and independently by a smaller amount ( 1029 , 10251032 ; p < 00001 ) , for every year older at menopause . 
 premenopausal women had a greater risk of breast cancer than postmenopausal women of an identical age ( rr at age 4554 years 143 , 133152 , p < 0001 )  . 
all three of these associations were attenuated by increasing adiposity among postmenopausal women , but did not vary materially by womens year of birth , ethnic origin , childbearing history , smoking , alcohol consumption , or hormonal contraceptive use . 
the e ect of menopause in women of an identical age and trends by age at menopause were stronger for oestrogen receptor - positive disease than for oestrogen receptor - negative disease ( p < 001 for both comparisons )  . interpretation the e ects of menarche and menopause on breast cancer risk might not be acting merely by lengthening womens total number of reproductive years . 
 to assess reliably the strengths of these associations and whether they vary by tumour subtype or by characteristics of a ected women requires large numbers , and we address these questions by combining information from more than 100 epidemiological studies . 
combining individual participant data from many studies not only increases statistical power but also permits similar de nitions and similar analytical methods to be used across studies . methods search strategy and selection criteria this collaboration began in 1992 , and has published on breast cancer risk associated with use of hormonal therapies and childbearing practices.14 potentially eli gible epidemiological studies have been sought at regular intervals by computer - aided literature searches , by written communication and discussions with col leagues , and by discussions at scienti c meetings , including collaborators meetings in oxford in 1993 , 1995 , 2000 , 2005 , and 2011 ( appendix p 3 shows search strategy and selection criteria )  . 
so that similar analytical methods could be used across studies , we incorporated cohort studies using a nested case control design , in which up to four controls were selected at random , matched at follow - up to age of the case at cancer diagnosis and , where appropriate , by broad geographical region . 
data for a range of sociodemographic , reproductive , and other behavioural factors , covering the time period to onset of disease for cases and to an equivalent time for controls , were sought from principal investigators ( appendix p 3 )  . vol 13 november 2012 1141 articles we included studies in these analyses if individual data had been provided for womens menopausal status , age at menarche and , if appropriate , age at menopause , and whether or not they had had a hysterectomy or a bilateral oophorectomy . 
women who had had a natural menopause or who had had a bilateral oophorectomy before their natural menopause were classi ed as postmenopausal , but those who had had a hysterectomy without bilateral oophorectomy before their natural menopause were classi ed as being of unknown menopausal status ( because hysterectomy can mask cessation of ovarian activity )  . 
otherwise , we took de nitions used by principal investigators to classify each woman by her age at menarche , menopausal status and , for postmenopasual women , by her age at menopause . 
women with unknown menopausal status or unknown ages at menarche or menopause were excluded from analyses , as were women who had used menopausal hormone therapy , since such use can mask the onset of menopause and a age at menarche 9 10 11 12 13 14 15 16 17 18 19 20 age at menarche ( years ) b age at menopause age at natural menopause ( years ) figure 1 : cumulative distribution of ( a ) age at menarche and ( b ) age at natural menopause data are for women without breast cancerie , controls . 
results for age at menopause are based on data from 157 272 postmenopausal women aged older than 55 years at the time of reporting their age at menopause . modify associations between hormonal factors and breast cancer risk.1 we also sought information about tumour characteristicsie , about oestrogen receptor status and about tumour histology . 
we used information provided by principal investigators to classify tumours as oestrogen receptor - positive or oestrogen receptor - negative , and as ductal , lobular , or of other histology . from reports in previous statistical analysis we did all analyses using conditional logistic regression , similar in principle to the mantel - haenszel strati cation technique used this collaboration.16 when two groups were compared odds ratios ( ors , described as relative risks [ rrs ] when cases and controls are compared ) and standard cis are given . 
 when more than two groups were compared , we estimated variances for every group , treating the ors or rrs as oating absolute risks , 7 because this method enables valid comparisons between any two groups , even if neither is the baseline group . 
this method does not alter risk estimates , but yields variances for each nonbaseline group that are slightly smaller than the variances calculated with conventional methods ( because these include the variance of the baseline group ) and we used these variances to calculate group - speci c cis . 
any comparison between two risk estimates must take the variation in each group into account . analyses of the association between various factors and womens age at menarche and age at menopause were restricted to controls , and we calculated ors stratifying by study , by centre within study , and where appropriate by age at diagnosis ( 20 years , and then in 3 year age groups , 2123 years to 8789 years ) ; by year of birth ( < 1920 , 192029 , 193039 , 194049 , and 1950 ) ; by parity and age when rst child was born ( nulliparous women were a separate stratum and parous women were cross - classi ed by parity [ 12 , 3 ] and age at rst birth [ < 20 years , 2029 years , 30 years ] ) ; by current body - mass index ( bmi ; < 25 kg / m , 2529 kg / m , 30 kg / m ) ; by height ( < 160 cm , 160164 cm , 165 cm ) ; by smoking ( never , past , present ) ; and by alcohol consumption per week ( < 50 g and 50 g )  . 
we restricted analyses comparing breast cancer risk in premenopausal , perimenopausal , and postmenopausal women to women aged 4554 years ( since each category is represented in this narrow age band ) and we used the same strati cations as described above , except that age was strati ed by single years . 
or calculations were strati ed by study and , where appropriate , by age at diagnosis , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi ( results for bmi as a young adult are not strati ed by current bmi )  . 
bmi = body - mass index . vol 13 november 2012 1143 articles a age at menarche study , centre within study , age at diagnosis in single years , and year of birth , and adjusted by parity , age at rst birth , bmi , smoking , and alcohol consumption , also using the same categories as described previously . age at menarche ( years ) < 11 ( 97 ) 11 ( 110 ) 12 ( 120 ) 13 ( 130 ) 14 ( 140 ) 15 ( 150 ) 16 ( 166 ) 5511 / 11 685 119 ( 113125 ) 15 855 / 37 779 109 ( 106112 ) 25 806 / 61 512 107 ( 105109 ) 31 759 / 83 389 100 ( 098102 ) 20 599 / 53 212 098 ( 096100 ) 10 576 / 31 390 092 ( 089095 ) 8858 / 27 124 082 ( 079085 ) b age at menopause age group ( mean , years ) cases / controls ( 95% gs ci ) age group ( mean , years ) cases / controls ( 95% gs ci ) we calculated rrs for breast cancer per 1 year younger at menarche and per 1 year older at menopause by linear regression , using the mean age within each category . 
 signi cance tests for heterogeneity by tumour subtype were based on analyses within cases only ( because controls provide no additional information ) , strati ed by age , study , and bmi and adjusted for other variables listed previously . 
we did our analyses with stata ( version 11 )  . when results for large numbers of subgroups are presented in the gures 99% cis ( or group - speci c 99% cis ) are given , to take account of multiple testing . 
 in the text all cis quoted are 95% cis . role of the funding source the funders had no role in study design , data collection , analysis , or interpretation of data , preparation of the report , or decision to publish . 
all members of the analysis and writing committee ( vb , db , rp , kp , gr ) had access to the raw data and are responsible for the nal submission for publication . results overall 117 studies , together including 118 964 women with breast cancer ( cases ) and 306 091 without the disease ( controls ) , were included in these analyses . 
median age at cancer diagnosis was 54 years ( iqr 4464 )  . figure 1a shows the distribution of age at menarche reported by controlsie , women without breast cancer . 
 their mean age at menarche was 131 years ( sd 17 ) , with almost two - thirds ( 65% , 198 113 of 306 068 ) reporting menarche at ages 12 , 13 , or 14 years . 
only 16% ( 49 464 ) of the controls reported menarche at age 11 years or younger and 19% ( 58 514 ) reported menarche at age 15 years or older . 
having early menarche was associated with many factors known to a ect breast cancer risk , including parity , figure 4 : relative risk of breast cancer ( a ) per year younger at menarche and ( b ) per year older at menopause , in various subgroups and by tumour characteristics relative risks are calculated stratifying by study and age , and where appropriate , by year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi ( results for bmi as a young adult are not strati ed by current bmi )  . 
 * subgroup analyses for age at menarche are for age at menopause < 50 vs 50 years in postmenopausal women ; and for age at menopause are for age at menarche < 13 vs 13 years . 
case - case comparisons strati ed by study , age and year of birth , and adjusted by parity , age at rst birth , smoking , alcohol consumption , height , and current bmi . 
 age at menopause ( years ) < 40 ( 353 ) 4044 ( 419 ) 4549 ( 472 ) 5054 ( 515 ) 55 ( 561 ) 2397 / 7741 067 ( 062073 ) 5516 / 18 544 073 ( 070077 ) 17 336 / 52 040 086 ( 084089 ) 28 197 / 75 944 100 ( 098102 ) 6891 / 16 144 112 ( 107117 ) figure 3 : relative risk of breast cancer by ( a ) age at menarche and ( b ) age at menopause calculated stratifying by study , age , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current body - mass index . 
rrs strati ed by study , age at diagnosis in single years , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi . 
 * results for breast cancer risk are plotted against the time between menopause and the diagnosis of breast cancer for postmenopausal women , and against an estimate of that time for premenopausal and perimenopausal women . 
the premenopausal women aged 4554 years in these analyses would be expected to reach their menopause in the next 27 years , on average ( this estimate is based on the age distribution of the premenopausal women in these analyses and the age distribution of womens ages at menopause shown in gure 1b )  . 
perimenopausal women might be expected to reach their menopause in the next 6 months , on average . age at rst birth , height , and bmi ( gure 2a )  . 
associations with late menarche were generally the con verse of associations with an early menarche ( appendix p 7 )  . the younger women were at menarche , the greater was their subsequent risk of breast cancer , the rr increasing by a factor of 1050 ( 95% ci 10441057 , p < 00001 ) for every year younger at menarche ( gure 3a )  . 
results in figure 3a were strati ed by study , age , year of birth , parity and age at rst birth , height , current bmi , smoking , consumption . 
additional adjustment ( either individually or simultaneously ) by ethnic origin , hormonal contraceptive use , and family history of breast cancer , altered the excess rr estimate by less than 1% ( data not shown )  . alcohol and to assess consistency of ndings , we calculated the rr of breast cancer per year younger at menarche for 34 subgroups of women , subdivided by 14 of their personal characteristics : year of birth , age at diagnosis and menopausal status , ethnic origin , parity , age at rst birth , height , bmi as a young adult , current bmi , use of oral contraceptives , smoking , alcohol consumption , family history of breast cancer , menopausal status and , for their age at menopause postmenopausal women , ( gure 4a )  . 
both among premenopausal and among postmenopausal women , increasing bmi seemed to attenuate the relevance of age at menarche , but this attenuation was signi cant only among postmenopausal women ( hetero geneity p = 0006 )  . 
we noted some weakening of the association with age at menarche by attained age in postmenopausal women ( heterogeneity p = 004 ; trend p = 002 ) and family history of breast cancer ( heterogeneity p = 001 ) , but for all other personal characteristics examined heterogeneity across subgroups was not signi cant . 
the ndings were not dominated by the results in any particular study ( appendix pp 810 ) and there was no signi cant heterogeneity in the ndings by study design ( appendix p 6 )  . of the 117 contributing studies , 85 provided some information about tumour characteristics ( appendix pp 45 ) , and gure 4a shows the rrs per year younger at menarche for various tumour subtypes . 
the association with age at menarche was signi cantly stronger for lobular than ductal tumours ( heterogeneity p = 00001 ) , but there were no signi cant di erences by oestrogen receptor status . 
cross - classi cation by both oestrogen receptor status and tumour histology did not show any further interaction ( appendix p 6 )  . figure 1b shows the cumulative distribution of the reported age at natural menopause among postmenopausal controls . 
their mean age at natural menopause was 493 years ( sd 46 ) , with 15% ( 26 285 of 170 413 ) reporting menopause before age 45 years , 75% ( 127 984 ) between the ages 45 and 54 years , and 10% ( 16 144 ) at age 55 years or older . 
associations with an early meno pause were generally the converse of those associated with a late menopause ( appendix p 7 )  . ovarian production of hormones decreases rapidly at around the time of menopause , as is shown in gure 5a , using published data from a cohort study of women who were premenopausal at entry and who had repeated measures of serum oestradiol until after the menopause.8 the short - term e ect of these changes on breast cancer risk can be assessed by restricting analyses to the 31 000 cases and 70 000 controls aged 4554 years ( since pre menopausal , peri menopausal , and postmenopausal women are represented in this age group ) and by stratifying analyses by single years of age ( so that women of identical ages are being compared )  . 
among such women , breast cancer risk was greater among premeno pausal than postmenopausal women ( rr 143 , 95% ci 133152 , p < 00001 ) , with the risk for perimenopausal women being between the other two ( gure 5b ; p < 0001 for all comparisons )  . the consistency of the nding of a greater risk of breast cancer among premenopausal than post menopausal women of the same age was examined across 30 subgroups of women , subdivided by 13 of their characteristics ( appendix p 11 )  . 
this nding re ects , at least in part , known di erences between premenopausal and postmenopausal women in the relation between their current bmi and breast cancer risk , as shown in gure 5c . 
among premenopausal women , those who were overweight or obese ( bmi 25 kg / m ) had a lower risk of breast cancer than leaner women ( bmi < 25 kg / m ) , whereas the reverse was observed among postmenopausal women . 
however , at ages 4554 years , where both premenopausal and postmenopausal women are rep resented , a sudden decrease occurs at menopause in the proportion of oestrogen the proportion of tumours with lobular histology increases with age , with a sudden decrease around the time of menopause . 
after adjusting by single years of age and other potential confounding factors , the heterogeneity at ages and postmenopausal women is highly signi cant both for oestrogen receptor status ( hetero geneity p = 0003 ) and for tumour histology ( heterogeneity p < 00001 , appendix p 11 )  . in analyses restricted to postmenopausal women , the rr of breast cancer increased by a factor of 1029 ( 10251032 , p < 00001 ) for every year older at menopause ( gure 3b )  . 
the ndings in gure 3b were years between premenopausal 4554 b lobular breast cancers age at diagnosis ( years ) figure 6 : breast cancer by tumour characteristics and by womens age and menopausal status ( a ) oestrogen receptor - positive ( er + )  . 
results are shown for age groups < 40 years , 4044 years , 4554 years , 5559 years , 6064 years , and 65 years , and plotted against the mean age of women with breast cancer in each age group . strati ed by study , year of birth , age , parity and age at rst birth , height , current bmi , smoking , and alcohol consumption . 
additional adjustment by ethnic origin , age at menarche , family history of breast cancer , and hormonal contraceptive use ( both individually and simultaneously ) altered the excess rr estimate by less than 1% ( data not shown )  . 
rrs did not di er signi cantly between women with a natural menopause ( 1030 , 10261034 ) and bilateral oophor ectomy ( 1019 , 10041034 , heterogeneity p = 02 ; appendix p 12 )  . the association between age at menopause and breast cancer risk was examined in 30 subgroups and did not vary signi cantly across 11 of the 13 characteristics examined ( gure 4b )  . 
the relation between breast cancer risk and increasing age at vol 13 november 2012 1147 articles menopause was signi cantly greater for oestrogen receptor - positive disease than for oestrogen receptornegative disease ( p = 001 ) , and for lobular than for ductal tumours ( heterogeneity p = 0006 )  . 
the ndings were not dominated by the results in any particular study ( appendix pp 1315 ) and there was no signi cant variation by study design ( appendix p 6 )  . among postmenopausal women , for whom the e ect on breast cancer risk per year younger at menarche can be directly compared to the e ect per year older at menopause , breast cancer risk increased by a signi cantly greater amount per year of menarche than per year of menopause ( 1045 [ 10361054 ] vs 1029 [ 10251032 ] ; heterogeneity p = 0001 )  . discussion this worldwide collaboration has brought together and reanalysed individual participant data for 120 000 women with breast cancer and 300 000 controls without the disease from 117 epidemiological studies in 35 countries ( panel )  . while con rming that early menarche and late menopause increase breast cancer risk , we showed that these e ects were not equivalent , in that the excess risk panel : research in context systematic review the collaborative group on hormonal factors in breast cancer began in 1992 . 
since then published literature on epidemiological studies of breast cancer has been identi ed using electronic searches ( medline , embase , and pubmed , 19982011 ; using combinations of the search terms breast cancer , risk , epidem * , and hormones ) , supplemented by hand searching in review articles . 
eligible studies needed to have obtained individual information about reproductive factors and about use of hormonal therapies , from at least 400 women with breast cancer and similar information from controls without the disease . 
studies that had obtained relevant data , but had not published any results for breast cancer were sought by correspondence with colleagues , by discussions at collaborators meetings , and by electronic searches using additional terms cohort , prospective , women , and cancer risk . 117 eligible studies were included and principal investigators contributed information about almost 120 000 women with breast cancer who had never used menopausal hormonal therapies to this individual - participant meta - analysis . 
we report on the relation between menarche and menopause and breast cancer risk , overall , and by oestrogen receptor status and by histological subtypes of the tumours , adjusting for possible confounding factors . 
subgroup results are also shown by various sociodemographic and personal characteristics , including year of birth , ethnic origin , parity , age at rst birth , smoking , alcohol consumption , and body - mass index . interpretation breast cancer risk increased by a signi cantly greater factor for every year younger at menarche than for every year older at menopause , indicating that menarche and menopause may not a ect breast cancer risk merely by extending womens total reproductive years . 
endogenous ovarian hormones are more relevant for oestrogen receptor - positive disease than for oestrogen receptor - negative disease and for lobular than for ductal tumours . associated with lengthening womens reproductive years by one year at menarche was greater than the excess associated with one years lengthening at menopause . 
 we also found that oestrogen receptor - positive and lobular breast cancers are strongly a ected by womens menopausal status , and by their age . the production of steroid hormones by the ovary begins at around the time of menarche and decreases rapidly at around the time of menopause . 
 by restricting analyses to the 31 000 women with breast cancer in this narrow age range and stratifying by single years of age ( and by other potential confounding factors ) , valid comparisons can be made of the short - term e ect of the menopause , and breast cancer risk was about 40% higher in premenopausal than in postmenopausal women of the same age . 
since the postmenopausal women had reached their menopause only an average 46 years previously , the ndings indicate a rapid decline in breast cancer risk in women of identical ages soon after menopause . 
this nding probably explains the attening of the age - incidence curve at around age 50 years , the so - called clemmesens hook , 9 frequently observed in populations before the widespread use of hormonal therapies and screening . there is accumulating evidence that oestrogen receptorpositive and lobular breast cancers are more sensitive to ovarian hormones than are oestrogen receptor - negative and ductal cancers . 
not only are oestrogen receptorpositive and lobular tumours strongly a ected by the menopause , as we have shown , but postmenopausal women who use hormone therapy have a greater increase in oestrogen receptor - positive than oestrogen receptornegative tumours and in lobular than ductal breast cancers.10 , 11 furthermore , oestrogen - blocking treatments improve survival for oestrogen receptor - positive , but not for oestrogen receptor - negative breast cancer.12 womens adiposity was consistently shown to attenuate associations between menopause and breast cancer risk . 
 circulating oestradiol concentrations increase as postmenopausal womens bmi increases.13 that the rr of breast cancer risk falls more rapidly after the menopause in lean than in overweight and obese women is likely to re ect , at least in part , di erences in oestradiol concentrations between such women . 
oestradiol concentrations in postmenopausal women are greater the younger they were at menarche , 14 and this might , in part , account for the associations recorded between age at menarche and breast cancer risk . although a womans age at menarche does not coincide precisely with the onset of breast development , the two are highly correlated.15 breast cancer is almost unknown before menarche and extremely rare soon afterwards , making it e ectively impossible to study the short - term e ects of the hormonal changes associated with menarche by comparing breast cancer risk in women of identical ages before and soon after menarche . 1148 vol 13 november 2012 articles these ndings con rm that young age at menarche and old age at menopause increase breast cancer risk . 
many factors known to a ect breast cancer risk , including childbearing patterns , height , and bmi , are also associated both with womens age at menarche and with their age at menopause . 
to ensure as much comparability as possible between women with breast cancer and controls , and thus to minimise potential confounding , analyses were strati ed by these factors , and by study , age , year of birth , smoking , and alcohol consumption . 
the associations did not vary materially by womens personal characteristics , other than bmi among postmenopausal women . this meta - analysis of individual - participant data includes almost all available epidemiological evidence for the association between menarche and menopause and breast cancer risk . 
single studies do not have su cient power to examine these asso ciations in detail , so reviews based solely on the limited published evidence could well be susceptible to publication bias . 
although availability of information about oestrogen receptor status varied substantially over time , with most studies done before 1990 contributing relatively little information , analyses of all available data combined were su ciently powered to describe asso ciations separately within both oestrogen receptor - positive receptor - negative disease . 
another important advantage of this metaanalysis is that it seeks to review both published and unpublished ndings , thus avoiding unduly selective emphasis on published results or on only some studies . oestrogen and women included in these analyses generally reported their ages at menarche and at menopause many years after the events had occurred . 
comparisons of information recorded at around the time of menarche and menopause with that recalled many years later has shown substantial regression to the mean over time , especially for recalled age at menarche , 1623 which would dilute estimates of rr.23 , 24 the slight attenuation in the estimated rr with attained age thus relects , at least in part , misclassi cation of recalled ages at menarche and , to a lesser extent , of recalled age at menopause . 
 since sig ni cant associations were recorded at all ages , it is reasonable to conclude that the e ects of age at menarche and age at menopause on breast cancer risk persist throughout life . since the e ect on breast cancer risk of 1 year younger at menarche is signi cantly greater than that of 1 year older at menopause , these ndings suggest that the e ects of each may not be acting merely by lengthening the total duration of womens reproductive years . 
in most populations womens average age at menarche has been declining in successive birth cohorts , 25 contributing to increasing incidence of breast cancer worldwide . contributors vb , db , rp , kp , and gr analysed the data , had full access to the pooled data , wrote the rst draft of the report , and had nal responsibility for the decision to submit ; all are guarantors . 
funding for the contributing studies is described in the publications of those studies . corrections correction to lancet oncol 2016 ; 17 : 109 correction to lancet oncol 2016 ; 17 : 248 , 252 du y sw , dibden a , michalopoulos d , et al . 
lancet oncol 2016 ; 17 : 10914in the findings section of the summary of this article , the second sentence should read the average frequency of dcis detected at screening was 160 per 1000 women screened ( median 150 [ unit range 054356 ] per 1000 women )  . 
 addition of docetaxel or bisphosphonates to standard of care in men with localised or metastatic , hormone - sensitive prostate cancer : a systematic review and meta - analyses of aggregate data . 
 lancet oncol 2016 ; 17 : 24356in the results section , the third sentence of the second paragraph should read in the three remaining trials , 7 , 8 , 10 men aged 3691 years ( median 6366 years ) with a good performance status received androgen deprivation therapy - based treatments ( standard of care ) with or without docetaxel . 
 in figure 3 , the text under parts a and c should have read favours soc + bisphosphonate , and the text under parts b and d should have read favours soc + zoledronic acid . 
 these corrections have been made to the online version as of feb 2 , 2016 , and the printed version is correct . vol 17 february 2016 particularly if chemotherapy - free interventions prove successful.9 indeed , huet and colleagues show that the prognostic effect of the previously defined expression signatures of immune response 1 and 210 was lost in the prima study cohort , demonstrating how the fortunes of these predictors can fluctuate with changes in treatment , even if a role for genes linked to the tumour microenvironment was maintained . as the potency of these scoring systems continues to improve , it is essential to develop the multicentre collaborations necessary to further validate , standardise , comparisons between and enable head - to - head these different predictors . 
the wider community of follicular lymphoma oncologists must decide which models to prioritise for either validation or adoption in clinical trials , and it is imperative that a consensus is reached on the level of discrimination needed to guide treatment , especially for an indolent disease such as follicular lymphoma where a high prognostic accuracy is necessary . 
the expected refinements might well involve increasingly complex dynamic models with imaging and cell - free dna , but it is equally important that risk models do not become unnecessarily unwieldy and impractical for routine application . this new prognostic tool is an important step towards the goal of personalised care for patients with follicular lymphoma . 
there is now a pressing need to not only validate and compare emerging prognostic tools in prospective clinical trials but to consider the robustness and feasibility of these analyses in the real - world setting . shamzah araf , jessica okosun , * jude fitzgibbon centre for haemato - oncology , barts cancer institute , london ec1m 6bq , uk j.fitzgibbon@qmul.ac.uk jf declares grants from epizyme and personal fees from roche , gilead , janssen , and epizyme , outside the submitted work . 
early relapse of follicular lymphoma after rituximab plus cyclophosphamide , doxorubicin , vincristine , and prednisone defines patients at high risk for death : an analysis from the national lymphocare study . 
integration of gene mutations in risk prognostication for patients receiving first - line immunochemotherapy for follicular lymphoma : a retrospective analysis of a prospective clinical trial and validation in a population - based registry . 
 n engl j med 2004 ; 351 : 215969 . adjuvant therapy in colon cancer : less is more the results of the scot trial reported by timothy iveson and colleagues1 in the lancet oncology establish a new standard of care in the adjuvant treatment of stage iii colon cancer . 
the investigators showed the non - inferiority of treatment with 3 months of adjuvant chemotherapy versus 6 months of the same treatment in terms of 3 year disease - free survival . 
 patients treated with the shorter duration of therapy had significant reductions in adverse events , including a more than halving in the number of grade 2 or worse sensory neuropathy events . 
these results were robust in patients with low - risk stage iii ( t3 or n1 ) disease who received 3 months of capecitabine and oxaliplat however , the non - inferiority of 3 months of therapy versus 6 months could not be shown in higher risk t4 or n2 disease . 
like scot , see articles page 562 442 vol 19 april 2018 comment non - inferiority could not be shown for the shorter duration of therapy with capecitabine and oxaliplatin in the higher risk patients . 
 therapies what are the implications for changing practice to 3 months of adjuvant chemotherapy ? a shorter duration of adjuvant therapy could permit the earlier introduction of to be investigational used sequentially or combined with chemotherapy , particularly in higher risk patients . 
furthermore , it will be necessary to await the impact of findings from correlative studies done in scot and the other idea trials , given the now recognised prognostic importance of factors such as tumour sidedness , microsatellite instability , and braf or ras mutation . less might also be more in oesophageal and gastric cancers . 
in anal cancer treated with definitive chemoradiotherapy , the addition of extra cycles of chemotherapy either before or after chemoradiotherapy has been shown not to improve survival compared with chemoradiotherapy alone.6 , 7 an argument for less chemotherapy is also seen in results from trials investigating neoadjuvant or preoperative therapy in a randomised trial8 of oesophageal and gastro - oesophageal junction cancers reported by ajani and colleagues , the addition of 2 months of fluorouracil and oxaliplatin before preoperative fluorouracil plus oxaliplatin and radiotherapy did not improve survival compared with chemotherapy given only during radiotherapy . 
in the oeo5 trial , 9 which enrolled patients with oesophageal and gastro - oesophageal junction adenocarcinoma , alderson and colleagues also reported no survival benefit with four cycles of the ecx regimen ( epirubicin , cisplatin , and capecitabine ) beyond that achieved with two cycles of fluorouracil and cisplat these results support the use of a shorter duration of preoperative chemotherapy as well as the discontinuation of the use of epirubic al - batran and colleagues have reported that the addition of docetaxel to infused fluorouracil and oxaliplatin , using the flot regimen ( fluorouracil , leucovorin , oxaliplatin , and docetaxel ) as preoperative therapy , resulted in a significant survival benefit compared with preoperative ecx in patients with gastric and gastro - oesophageal junction cancers.10 if a third chemotherapy agent is to be added to preoperative fluorinated pyrimidine platinum chemotherapy , it should be docetaxel and not epirubicin . the scot investigators deserve congratulations for their practice - changing trial that can directly improve the lives of patients receiving adjuvant chemotherapy for stage iii colon cancer . 
 david h ilson gi oncology service , memorial sloan kettering cancer center , new york , ny 10011 , usa ilsond@mskcc.org i declare no competing interests . copyright the author ( s )  . 
3 versus 6 months of adjuvant oxaliplatin - fluoropyrimidine combination therapy for colorectal cancer ( scot ) : an international , randomised , phase 3 , non - inferiority trial . 
prospective pooled analysis of six phase iii trials investigating duration of adjuvant ( adjuv ) oxaliplatin - based therapy ( 3 vs 6 months ) for patients ( pts ) with stage iii colon cancer ( cc ) : the idea ( international duration evaluation of adjuvant chemotherapy ) collaboration . 
three versus six months adjuvant oxaliplatin - based chemotherapy for patients with stage iii colon cancer : the french participation to the international duration evaluation of adjuvant chemotherapy ( idea ) project . 
perioperative chemotherapy with docetaxel , oxaliplatin , and fluorouracil / leucovorin ( flot ) versus epirubicin , cisplatin , and fluorouracil or capecitabine ( ecf / ecx ) for resectable gastric or gastroesophageal junction ( gej ) adenocarcinoma ( flot4 - aio ) : a multicenter , randomized phase 3 trial . 
we assessed the prognostic value of a prede ned cell cycle progression ( ccp ) score in two cohorts of patients with prostate cancer . methods we measured the expression of 31 genes involved in ccp with quantitative rt - pcr on rna extracted from formalinxed para n - embedded tumour samples , and created a prede ned score and assessed its usefulness in the prediction of disease outcome . 
the signature was assessed retrospectively in a cohort of patients from the usa who had undergone radical prostatectomy , and in a cohort of randomly selected men with clinically localised prostate cancer diagnosed by use of a transurethral resection of the prostate ( turp ) in the uk who were managed conservatively . 
the primary endpoint was time to biochemical recurrence for the cohort of patients who had radical prostatectomy , and time to death from prostate cancer for the turp cohort . findings after prostatectomy , the ccp score was useful for predicting biochemical recurrence in the univariate analysis ( hazard ratio for a 1 - unit change [ doubling ] in ccp 189 ; 95% ci 154231 ; p = 5610 ) and the best multivariate analysis ( 177 , 140222 ; p = 4310 )  . 
in the best predictive model ( nal multivariate analysis ) , the ccp score and prostate - speci c antigen ( psa ) concentration were the most important variables and were more signi cant than any other clinical variable . 
in the turp cohort , the ccp score was the most important variable for prediction of time to death from prostate cancer in both univariate analysis ( 292 , 238357 , p = 6110 ) and the nal multivariate analysis ( 257 , 193343 ; p = 8210 ) , and was stronger than all other prognostic factors , although psa concentration also added useful information . 
heterogeneity in the hazard ratio for the ccp score was not noted in any case for any clinical variables . interpretation the results of this study provide strong evidence that the ccp score is a robust prognostic marker , which , after additional validation , could have an essential role in determining the appropriate treatment for patients with prostate cancer . funding cancer research uk , queen mary university of london , orchid appeal , us national institutes of health , and koch foundation . introduction prostate cancer is a common diagnosis , especially when prostate - speci c antigen ( psa ) screening is used , 1 and its natural history is highly variable and di cult to predict . 
we therefore selected a set of ccp genes and retrospectively tested their prognostic value in prediction of disease outcome using a prede ned score , in a cohort of patients with prostate cancer who had been treated with radical prostatectomy and in a cohort of conservatively treated patients . methods ccp gene selection to reliably generate expression data from formalinxed para n - embedded ( ffpe ) tissue , we selected 126 ccp 804 consecutive patients with radical prostatectomy 775 with clinical data 442 with available tumour tissue 410 eligible for analysis 29 no clinical data 333 no available tissue 32 excluded because of treatment with neoadjuvant therapies 44 excluded because of poor - quality cell - cycle - progression scores 366 analysed for gene expression data figure 1 : flow chart of cohort with radical prostatectomy genes from the gene expression omnibus database and tested their performance with rna extracted from 96 commercially available ffpe prostate tumour sections ( asterand , detroit , mi , usa ) obtained from anonymous patients . 
 therefore , we selected genes for inclusion in the signature on the basis of their correlation with the mean expression of the entire set of ccp genes ( webappendix pp 14 )  . 
the nal signature consisted of 31 ccp genes ( foxm1 , cdc20 , cdkn3 , cdc2 , kif11 , kiaa0101 , nusap1 , cenpf , aspm , bub1b , rrm2 , dlgap5 , birc5 , kif20a , plk1 , top2a , tk1 , pbk , asf1b , c18orf24 , rad54l , pttg1 , cdca3 , mcm10 , prc1 , dtl , cep55 , rad51 , cenpm , cdca8 , and orc6l )  . 
these highly correlated genes were used to provide a robust and highly reproducible measurement of cell proliferation and were not intended factors to capture ( eg , invasive potential )  . information to other related radical prostatectomy cohort men who had undergone radical prostatectomy for prostate cancer from 198595 were identi ed through the tumour registry at the scott and white clinic , temple , tx , usa . 
the specimens were inked , and pathological ndings were recorded as positive for bladder neck or urethral margin , invasion into the capsule , extension through the capsule , positive margins , and the involvement of the seminal vesicles . 
 biochemical recurrence was de ned as a psa concentration greater than 03 ng / ml based on the management policy used in the 1990s , and was not changed for this analysis . 
we selected patients who had not been treated with neoadjuvant drugs and for whom clinical data and tumour tissue were available for inclusion in this study to create a retrospective cohort . 
 institutional review board approval was obtained from the scott and white clinic . transurethral resection of prostate ( turp ) cohort for the population - based retrospective watchful - waiting cohort , potential cases of prostate cancer were identi ed 246 vol 12 march 2011 articles 214 ( 156293 ) 132 ( 094185 ) 164 ( 088306 ) 145 ( 110193 ) 215 ( 153301 ) 143 ( 109189 ) 224 ( 167301 ) 165 ( 126217 ) 220 ( 170285 ) 155 ( 114211 ) 189 ( 154231 ) 833% * 619% * 445% * 237% * ccp score recurrence hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) from six cancer registries in great britawithin each region , cases from collaborating hospitals were reviewed , and full details of these cases have been reported.31 men were included in this study if they had clinically localised prostate cancer , which was diagnosed by use of turp between 1990 and 1996 ( inclusively ) , were younger than 76 years at the time of diagnosis , and had a baseline psa measurement . 
men who had hormone therapy before diagnostic biopsy were also excluded because of the e ects of hormone treatment on interpretation of the gleason score . original histological specimens from the diagnostic procedure were requested , collected , and centrally reviewed by a panel of expert urological pathologists to con rm the turp diagnosis and , when necessary , to reassign gleason scores for all the prostate cancers by use of a contemporary interpretation16 of the gleason scoring syste follow - up was through the cancer registries and the last review took place in december , 2006 . 
 deaths were divided into two categories , those from prostate cancer and those from other causes , according to whos standardised criteria.32 national ethics approval was obtained from the northern multicentre research ethics committee , followed by local ethics committee approval at each of the turp cohort the collaborating hospitals for ( webappendix p 6 )  . gene expression depending on tumour volume , ve to 12 consecutive 5 m ( turp ) or 10 m ( prostatectomy ) ffpe tumour sections were used to isolate tumour - derived rna . 
we switched from rneasy ffpe to mirneasy because the new kit consistently generated figure 2 : analysis of cell cycle progression ( ccp ) score in cohort with radical prostatectomy ( a ) distribution of the ccp scores for 366 patients . 
2 values were 5493 , 415 , and 841 in the univariate analysis , multivariate analysis , and nal model , respectively , when gleason scores were assessed as a three - group categorical variable with 2 degrees of freedo table 1 : summary of statistical analysis of prostatectomy cohort , by biochemical recurrence better rna yields . 
no di erence was noted between the kits in terms of the data for gene expression . total rna was treated with dnase i ( sigma - aldrich , st louis , mo , usa ) before cdna synthesis . 
however , most samples ( 90% of radical prostatectomy cohort and 85% of turp cohort ) could be used to generate ccp scores , and therefore , had rna of adequate quality . before measurement of gene expression , the cdna was preampli ed in a pooled reaction containing taqman assays ( applied biosystems )  . 
the ampli cation reaction was diluted 1 : 20 with the 1tris - edta bu er before it was loaded on taqman low density arrays ( applied biosystems ) to assess the ampli ed genes . 
a total of 31 prede ned ccp genes and 15 housekeeper genes were ampli ed on one taqman low density array . ccp score the ccp score for each individual was calculated . 
the values of each of three replicates of each of the 31 ccp genes were normalised by subtraction of the average of up to 15 non - failed housekeeper genes for that replicate ( centred with a prede ned value ) to give c * t . 
this quantity was then converted to a value that was proportional to the copy number , calculated as 2c * for missing c * t values , due to low expression , 2c * was set as equal to 0 . 
for each ccp gene , the mean 2c * of the qualifying replicatesie , those with expression of at least 13 housekeeper genes , was then averaged over the qualifying ccp genes . 
this is the normalised average of 2c * t and was converted back to create the ccp score by taking a base 2 logaritha ccp gene was judged as having failed if more than one replicate did not qualify , or if two replicates quali ed and one of them had 2c * equal to 0 , or if the standard deviation between the three 248 vol 12 march 2011 articles replicate c * t values exceeded 05 . 
ccp scores with the number of failing ccp genes greater than nine of 31 , or a high sd between scores calculated from the three replicates , were rejected and excluded from the analysis . 
 the interassay variability has been established in our laboratory and the sd of the ccp score for experimental replicates is 01 . statistical analysis survival analysis was done with cox proportional hazards models . 
the clinical variables recorded for the prostatectomy cohort were diagnostic gleason score , most recent prebiopsy psa concentration , clinical stage , clinical grade , primary treatment ( no preoperative or postoperative hormones , orchiectomy , or adjuvant radiation ) , age at surgery , pathological tumour stage , pathological grade , pathological gleason score , and invasion features . the primary endpoint for the turp cohort was time to death from prostate cancer . 
biochemical progression was not an appropriate outcome for this cohort , since baseline psa concentrations remain elevated and some patients will have chosen to start hormones or have radical treatment without evidence of increasing psa concentration . 
the variables recorded for the turp cohort were centrally reviewed gleason grade and score , baseline psa value , clinical stage , extent of disease ( proportion of turp chips with disease ) , age at diagnosis , and initial treatment ( no initial treatment or early hormone management )  . 
 the analysis set and a complete analysis plan were agreed , and all ccp scores were assigned , before the clinical and outcome data were unmasked . in both cohorts , psa concentration was modelled as the natural logarithm of 1 + psa ( ng / ml )  . 
 as indicated above , for the prostatectomy cohort , only a single pathological gleason score was recorded at diagnosis ; for the turp cohort , 3 + 4 and 4 + 3 were shown to have nearly identical prognosis.13 , 31 therefore , a total gleason score of 7 was analysed as one group . 
 for simplicity , gleason scores were grouped into less combined risk score combined risk score stratied by gleason score figure 3 : 10 - year predicted risk of recurrence for di erent combined risk scores in cohort with radical prostatectomy ( a ) , and distribution of the combined risk scores for di erent subgroups based on gleason scores ( b ) the probability of recurrence was estimated from a cox proportional hazard model by use of the combined risk score . than 7 , 7 , and greater than 7 ( radical prostatectomy cohort : less than 7 [ 56% with score 6 ] , greater than 7 [ 75% with score 8 , 19% with score 9 ] ; turp cohort : less than 7 [ 88% with score 6 ( all 3 + 3 ) ] , 7 [ 34% with score 4 + 3 ] , and greater than 7 [ 51% with score 8 , 46% with score 9 ] )  . 
all p values were twosided and 95% cis and p values were based on statistics with 1 degree of freedom obtained from partial likelihood models . the main assessment was a univariate analysis of the association between outcome and ccp score . 
this later e ect was measured by use of the decrease in the likelihood ratio when the ccp score was omitted from a model containing it and the other relevant baseline clinicopathological variables . 
in construction of the best prognostic model , the goal was to capture most of the prognostic information from the ccp score and the clinical covariates in a simple linear model without over tting the data . 
a multivariate proportional ( cox ) hazards model was used to achieve this goal and to create a combined score based on the major clinical variable and the ccp score . 
the ccp score was evaluated vol 12 march 2011 articles 1658 reviewed histology and assigned gleason score 747 diagnosed by use of needle biopsy 2333 eligible patients 675 excluded 203 not requested 472 excluded after review 283 unknown or missing histology slides 43 incorrect pathology specimen 135 histologically ungradeable gleason score 6 no tissue in block 5 histologically ungradeable gleason score 911 diagnosed by use of turp 429 unselected samples identied for analysis 482 not included in this study 7 previous hormone therapy 31 ineligible for study 9 psa > 100 ng / ml 6 missing baseline psa 4 previous cancer 4 metastases within 6 months 1 biopsy not between 199096 61 excluded because of poor - quality cell - cycle progression scores 398 available for analysis 337 eligible in nal analysis figure 4 : flow chart of cohort with transurethral resection of prostate ( turp ) psa = prostate - speci c antigen . as a linear and a quadratic term , and tested for interactions with individual covariates . 
we used a forward stepwise regression in which a new variable was added only if it had a p value of less than 002 for the prostatectomy study and 005 for the turp study ( since fewer variables were tested )  . 
the corresponding author had full access to the data ( as did ss , jer , and dm ) , and takes full responsibility in submitting the report for publication . the results for radical prostatectomy cohort , patients characteristics and treatment outcomes have been reported previously.33 figure 1 summarises the selection of 410 patients for this study who underwent radical prostatectomy . 
the median preoperative psa concentration was 69 ng / ml ( 46109 ) , and 281 ( 71% ) of 397 patients had psa concentrations less than 10 ng / ml . 
a unit change in the score corresponds to a doubling in expression level . that were the the univariate analysis showed that in the patients who had undergone radical prostatectomy , a high ccp score was predictive of biochemical recurrence ( table 1 )  . 
 addition of a quadratic term for ccp score was not signi cant ( p = 063 ) , indicating that a simple linear model would capture most of the prognostic information from the signature . 
 the ccp score was only weakly correlated with other variables , the highest correlation was with the gleason score and psa ( pearsons ( cid : 1 ) values , 022 and 021 respectively )  . 
however , patients with higher clinical 250 vol 12 march 2011 articles 276 ( 103740 ) 205 ( 105401 ) 213 ( 160285 ) 267 ( 159447 ) 351 ( 195635 ) 505 ( 289883 ) 208 ( 134324 ) 412 ( 1671021 ) 246 ( 182333 ) 292 ( 199429 ) 560 ( 2671175 ) 225 ( 177287 ) 292 ( 239357 ) 783% * 346% * 131% * 22% * risk ( ie , gleason score > 6 and psa concentrations > 10 ng / ml ) tended to have a reduced ccp hazard ratio ( hr )  . 
the ccp score was predictive for death after disease progression ( hr 299 , 95% ci 169528 ; p = 00007 )  . in the full multivariate analysis of the prostatectomy cohort , ccp and psa concentration were the most signi cant predictors of biochemical recurrence , and provided more prognostic information than did any other variable ( table 1 )  . 
the best multivariate model was developed by forward stepwise regression and is given by combined risk score 055 ccp + 081 log ( 1 + psa ) + 028 tstage + 064 margin + { 030 ( gleason score 7 ) + 099 ( gleason score > 7 ) } figure 3a shows how the risk of biochemical recurrence in the nal 10 years increased as a function of the combined risk score , and given the central prognostic role of the gleason score , gure 3b shows the distribution of combined risk score in di erent gleason score categories . for the turp cohort , the selection of patients is summarised in gure 4 . 
we report the results obtained with a randomly selected subset of 337 men diagnosed by use of turp for which we were able to compute the ccp score ( gure 4 )  . 
within 10 years of diagnosis , 171 ( 51% ) of 337 men had died , 68 ( 20% ) from prostate cancer and 103 ( 31% ) from other causes . figure 5a shows the distribution of the ccp score among the 337 patients in the turp cohort . 
by comparison with the gleason score , psa , cancer extent , and ki67 , the ccp score provided the most prognostic information in the univariate analysis , with the being slightly greater than that for the gleason score ( table 2 ) , and substantially larger than for all other variables . 
 compared with the prostatectomy cohort , the ccp score figure 5 : analysis of cell cycle progression ( ccp ) score in cohort with transurethral resection of prostate ( turp ) ( a ) distribution of the ccp scores ( n = 337 )  . 
2 values were 813 , 54 , and 71 in the univariate analysis , multivariate analysis , and nal model , respectively , when gleason score was assessed as a three - group categorical variable with 2 df ( when increased to ve groups , 2 values were 94 , 54 , and 72 , respectively )  . 
 table 2 : summary of statistical analysis of transurethral resection of the prostate cohort combined risk score in the full multivariate analysis , after adjustment for psa concentration , gleason score , ki67 expression , and extent of disease , the ccp score was dominant ( table 2 ) , providing more information than did any other variable . 
 none of the variables showed a signi cant interaction with the ccp score , and the hr for the ccp score was only slightly attenuated when other factors were added to the model ( table 2 )  . 
 hormone treatment was signi cant in a univariate model ( hr 381 , 95% ci 240605 ) , but did not add signi cant predictive information in the multivariate model ( 112 , 068184 ) , presumably because the decision to use this treatment was based on the known prognostic factors . 
 addition of a quadratic term for ccp was also not signi cant in the multivariate model ( p = 013 )  . in the forward stepwise regression model , with the variables ccp , psa concentration , and gleason score , the best predictor was the combined risk score calculated as function of figure 6a shows the predicted 10 - year death rate from prostate cancer the increases as a combined score ; gure 6b shows the distribution of the combined score in di erent gleason score categories . 
for men with a tumour that was gleason score 6 or less , use of the combined score identi ed 28 ( 16% ) of 172 patients with a 10 - year risk of death from prostate cancer that was less than 2% , and 102 ( 59% ) of 172 with a risk less than 5% , but also identi ed 25 ( 15% ) with a risk greater than 10% , indicating that not all gleason score 6 or less tumours are low risk . 
for gleason score 7 combined risk score stratied by gleason score 095 ccp + 061 log ( 1 + psa ) + { 090 ( gleason score 7 ) + 100 ( gleason score > 7 ) } figure 6 : 10 - year predicted risk of prostate cancer death for di erent combined risk scores in cohort with transurethral resection of prostate ( a ) , and distribution of the combined risk scores for di erent subgroups based on gleason scores ( b ) the probability of prostate cancer death was estimated from a cox proportional hazard model by use of the combined risk score . correlated more with gleason score ( pearsons ( cid : 1 ) = 061 ) , log ( 1 + psa ) ( ( cid : 1 ) = 027 ) , ki67 ( ( cid : 1 ) = 050 ) , and extent of disease ( ( cid : 1 ) = 051 )  . 
the prognostic value of the ccp score was similar in di erent gleason categories and when strati ed by psa , extent of disease , and ki67 ( gure 5b )  . 
figure 5c shows a kaplan - meier plot of the proportion of patients dying of prostate cancer at di erent follow - up times grouped by integer values of the ccp score . 252 vol 12 march 2011 articles ( either 3 + 4 or 4 + 3 ) , the corresponding data were none of 73 patients , eight ( 11% ) , and 59 ( 81% ) , respectively . 
in the whole cohort , the numbers and percentages were 28 ( 8% ) of 337 , 111 ( 33% ) , and 173 ( 51% ) , respectively . when we assessed deaths from other causes , the only signi cant factor was age . 
neither the ccp score nor other major prognostic factors for prostate cancer death were signi cant causes , indicating that confounding by other deaths cannot explain these ndings . discussion the ccp score was predictive of outcome in both cohorts and provided substantially more prognostic information than did clinical variables alone . 
expression of ccp genes is higher in actively growing cells , and presumably by measuring the expression of ccp genes , we are indirectly measuring the growth rate and inherent aggressiveness of the tumour , which ultimately a ects outcome . 
three of the genes in our signaturetop2a , rrm2 , and birc5have been previously associated with prostate cancer outcome , 14 , 15 but we believe the use of a larger panel will ensure robustness of the score . 
notably , many ccp genes are putative targets of cytotoxic or radiation therapies : rrm ( pemetrexed and gemcitabine ) , top 2a ( anthracyclines ) , kif11 and kif20a ( taxanes ) , tk1 ( uorouracil ) , and rad51 and rad54l ( radiation , alkylating drugs , and novel targeted drugs ) , and therefore ccp may be useful in predicting response to treatment . both cohorts have their strengths and weaknesses . 
the cohort of patients who had undergone radical prostatectomy were mainly screen detected , and had lower baseline gleason scores and psa concentrations , but a very low death rate from prostate cancer . 
the turp cohort had more aggressive disease , which meant that prostate cancer mortality could be reliably modelled , but was all based on symptomatic patients and turp samples , which is unusual in contemporary practice . 
in both settings , ccp score and psa concentration were the dominant variables , whereas other clinical variables ( including gleason score ) did not retain most of their univariate prognostic usefulness . 
by contrast ki67 , which is coded for by a ccp gene and by itself can be predictive of outcome in this dataset , 34 was eliminated from models that immunohistochemical score . 
 assessment of ki67 is dominated in the predictive models probably because measurement of the ccp score through rna concentrations is more quantitative and better represents the underlying biology . included ccp panel : research in context systematic review we searched pubmed through the national center for biotechnology information search engine with key terms prostate cancer , prognostic , and rna expression . 
also , the ndings of most studies were not shown to be robust in terms of patient composition or clinical setting . to develop the cell cycle progression ( ccp ) score , we downloaded and analysed every large publicly available expression dataset that was associated with cancer outcome ( gene expression omnibus database )  . 
as a result , we concluded that ccp genes were the key components in every validated prognostic signature , and this conclusion was in accord with mosley and colleagues.29 interpretation although the appropriate management of early prostate cancer is widely acknowledged to be a major clinical issue , none of the previously de ned prognostic signatures have had a major e ect on clinical care . 
in this study , we addressed all these issues , and the results indicate that the ccp score can be helpful in assessing prognosis in a range of settings , especially for patients with a good prognosis such as gleason score 6 . 
the ccp score is a robust measure of the proliferative activity in the tumour and might be useful in ascertaining which prostate cancers can be safely managed with a conservative strategy . 
further validation studies are needed , especially for screen - detected cancers that are diagnosed by use of needle biopsy when conservative management is an option . the evidence presented here indicates that the ccp score adds signi cantly to the predictive power of the clinical variables typically used to predict disease outcome after surgery and at the time of disease diagnosis . 
although potentially useful in both of these settings , the most pressing clinical need is to accurately separate indolent disease in men with newly diagnosed cancer , which is unlikely to be fatal , from the more aggressive cancers treatment . 
 currently , gleason score and baseline psa concentration are the strongest predictors , and extent of disease and ki67 add only a small additional discrimination.34 clinical stage , which was only available for some of the turp cohort , was only weakly predictive of outcome in previous analyses.31 results from the univariate analysis of the turp cohort have shown that the ccp score was a stronger predictor of death from prostate cancer than in need of radical vol 12 march 2011 articles were any of the other variables , and multivariate analysis indicated that this score added a substantial amount of prognostic information not captured by any other measure . 
this result is supported by an hr of 174 in the prostatectomy cohort and 257 in the turp cohort in the multivariate model for a 1 - unit increase in the ccp score . 
when the ccp score was adjusted for clinical variables , the hrs were 168 and 306 , respectively , for a change from the 25th to 75th percentiles of the ccp score distributions in each cohort . 
although the area under the receiver operating characteristic curve ( auc ) does not account for time - to - event information or censoring , it has become a common way to compare predictive scores for an event . 
for an event in the rst 5 years , the auc in the prostatectomy cohort for biochemical recurrence was 0825 for the clinical score , and 0842 for the combined score ( including the ccp score )  . 
 additionally , the added value of the ccp score to clinical variables can be noted by comparison of the outcomes of patients in the lowest quartile versus highest quartile of the clinical score versus the combined score . 
comparison of the 10 - year event proportions in the highest quartile showed that the kaplan - meier estimates were 843% ( clinical score ) versus 836% ( combined score ) for the cohort of patients who had under gone radical prostatectomy ( biochemical recurrence ) , and 626% versus 674% , respectively , for the turp cohort ( death from prostate cancer )  . 
therefore , addition of the ccp score to clinical variables allows more accurate prediction of which men can be safely managed by watchful waiting , and , of equal importance , which men with apparently low - risk disease actually are at high risk of death from prostate cancer and might bene t from radical treatment . 
 for example , 8% of the entire cohort and 15% of men with a gleason score of 6 or less could be identi ed with a 10 - year death rate from prostate cancer of less than 2% , and 17% of those with a gleason score of 6 or less still had a 10 - year death rate from prostate cancer of more than 10% . versus ccp genes have been shown to be prognostic in breast cancer.29 they have also proven to be prognostic in lung and brain cancers.35 , 36 the results of these previous studies led us to assess whether ccp genes would be useful in prostate cancer . 
 as a result , the interpretation of this study is not complicated by the extensive multiple testing inherent in more comprehensive discovery strategies , and , its measurement therefore , we can be highly con dent about the main conclusions of this report . 
we do not claim , however , that the ccp score contains every gene that might be prognostic in prostate cancer , and additional studies might uncover biomarkers that greatly improve the overall performance of our predictive models . 
assessment of the value of the ccp score in clinical trials of adjuvant radiation , androgen deprivation , and other systemic treatments is warranted to establish whether this signature can help in the decisions about treatments in that setting too . important step is an contributors all authors approved the nal report and contributed to the study . 
for the turp cohort study , jc and gf contributed to the experimental design , writing the report , and data analysis ; dmb and csf participated in the pathology review and interpretation ; hm was involved in coordinating cancer registry clinical data ; es participated in specimen preparation ; ps and hm were involved in the study plan and design . 
for the prostatectomy cohort study , gps and arb were involved in the experimental design , writing the report , and data analysis ; vos participated in the pathology review and interpretation ; and jer , ag , and ddf contributed to the statistical analysis . con icts of interest jsl , ag , ss , sw , ay , ddf , jp , jer , and jdw are employees of myriad genetics . 
the other authors declared that they have no con icts of interest . acknowledgments we gratefully recognise the patients who participated in this study and the support from cancer research uk , queen mary university of london , the orchid appeal , national institutes of health ( spore ca92629 ) , and the koch foundation and myriad genetics . 
 we also thank investigators and sta in the cancer registries and participating hospitals for their support ( webappendix p 6 )  . correction to lancet oncol 2014 ; 15 : 150312 correction to lancet oncol 2019 ; 20 : 76980 correction to lancet oncol 2019 ; 20 : 98699 open - label phase 1 / 2 jg , niesvizky r , kumar sk , berdeja et al . 
 lancet oncol 2014 ; 15 : 150312in the eighth paragraph of the results section of this article , the first sentence should have been overall responses were noted in 59 ( 92% , 95% ci 8397 ) of 64 patients ( table 5 )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 765 ben - aharon i , goshen - lago t , fontana e , et al . 
this correction has been made to the online version as of july 1 , 2019 . 2018 jacob s , yap ml , wilson be , ferlay j , bray f , barton mb . 
 lancet oncol 2019 ; 20 : 76980 in the affiliations for this article , dr mei ling yap should have been affiliated with the university of new south wales ( sydney , nsw , australia )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 795805 randomised , controlled hofvind s , holen s , aase hs , et al . 
 lancet oncol 2019 ; 20 : 795805 in figure 1 , the number of patients with screen - detected breast cancer in the digital breast tomosynthesis group should have read 95 , and the number of patients in the digital mammography group should have read 87 . 
 quizartinib versus salvage chemotherapy in relapsed or refractory flt3 - itd acute myeloid leukaemia ( quantum - r ) : a multicentre , randomised , controlled , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 98699in this article , the second sentence in the statistical analysis section should have read the sample size calculation wording in the original protocol specified a 5% , two - sided calculation ; however , this wording was inaccurate , and subsequently , a one - sided calculation at 25% was implemented to solely test for superiority of quizartinib , which is consistent with the primary aim of the study . 
this correction has been made to the online version as of july 1 , 2019 , and the printed article is correct . correction to lancet oncol 2019 ; 20 : e30212 hillengass j , usmani s , rajkumar sv , et al . 
these corrections have been made to the online version as of july 1 , 2019 . vol 20 july 2019 e346 corrections the birmingham environment for academic research local cloud.10 ukccmp delivers meaningful real - time data to all uk cancer centres and clinicians to allow more personalised approaches to individual patient care and inform clinical decision making . 
this initiative will improve cancer care in the uk and beyond at this time of unprecedented global turmoil and reliance on health - care resources . we declare no other competing interests . 
the university of birmingham initiated this process , with the pro - vice - chancellor dedicating the computational and human resources of the universitys centre for computational biology , the institute of translational medicine , and scientists from the institute of cancer and genomic sciences . 
other academic institutions dedicating time and staff to the project include the university of oxford , university of leeds , university college london , edinburgh cancer centre , clatterbridge cancer centre , and kings college london . the uk coronavirus cancer monitoring project team lennard.lee@nhs.net huang c , wang y , li x , et al . 
 joint - mission - on - covid - 19 - final - report.pdf ( accessed april 9 , 2020 )  . coronavirus covid - 19 global cases by the center for systems science and engineering at johns hopkins university ( jhu )  . 
castles ( compute and storage for the life sciences ) : a collection of compute and storage resources for supporting research at the university of birminghabirmingham : birmingham environment for academic research , june 20 , 2019 . 
 ( accessed april 7 , 2020 )  . recommendations from national regulatory agencies for ongoing cancer trials during the covid - 19 pandemic clinical research has transformed cancer care and is often integrated seamlessly into routine oncology clinics , offering eligible patients additional treatment options or lines of therapy . 
typically , and particularly for diseases with poor prognoses or when trials entail biomarker - directed personalised treatment , clinical trial enrolment can be preferred ( by both doctors and patients ) over standard care.1 however , many barriers already preclude patients participation in clinical trials , with only a small proportion enrolled in interventional trials.2 the coronavirus disease 2019 ( covid - 19 ) pandemic presents an additional major barrier to patients enrolment and ongoing participation in clinical trials . 
institutions are adapting their oncology practice , considering alternative treat ment strategies to appropriately balance risks and benefits , despite the absolute individual risk increases from covid - 19 for patients being currently unknown.3 the us food and drug administration ( fda ) and other international bodies have released guidance for sponsors and study sites to ensure the safety of trial participants while maintaining compliance with good clinical practice and minimising risks to study integrity . 
this guidance is summarised in the panel.410 although this guidance is very welcome and helpful , specific considerations must be made for each trial , in view of the wide variety of study types , relative complexities , and perceived risks and benefits . 
many study sites and sponsors have already stopped study enrolment , and it is not clear when these studies will reopen because of the probable prolonged effects of the covid - 19 pandemic . 
for patients on study treatment , the difficult decision to stop or carry on with the investigational medical product or other study treatments should be discussed between see online for appendix members of the uk coronavirus cancer monitoring project team are listed in the appendix ( p 1 )  . 
bda = bulgarian drug agency . sponsors and study sites , but most between the investigator and patient . importantly substantial uncertainty remains about which interven tions or treatments might increase the risk for con tracting covid - 19 or for covid - 19 - related immuno supmorbidity or mortality . 
careful consideration of additional covid - 19associated risks of continuing these agents should be balanced against the potential issues with stopping or delaying treatment that might extend life , help with or delay symptoms , or reduce the risk for disease - related complications . interventions that allow we encourage all sponsors and regulatory authorities to permit rational changes to study assessments individualisation of and these complex decisions , putting the patient first while continuing to optimise safety and endpoint assessment . 
we hope that risk mitigation and easing of previously inflexible rules , which will put the patient at the centre of clinical research , will continue long into the future . gjd reports personal fees from astrazeneca , amgen , boehringer ingelheim , bayer , and roche , outside the submitted work ; and is principal or chief investigator for academic and industry - sponsored clinical trials . 
 documents / fda - guidance - conduct - clinical - trials - medical - productsduring - covid - 19 - pandemic ( accessed april 2 , 2020 )  . instituto nacional de vigilancia de medicamentos y alimentos . 
trials / management - of - clinical - trials - in - relation - to - covid - 19 ( accessed april 2 , 2020 )  . 7 medicines and healthcare products regulatory agency . 
s - department - of - clinical - trials - on - medicinal - 1 ( accessed april 2 , 2020 )  . 10 guidance on the management of clinical trials during the covid - 19 ( coronavirus ) pandemic . 
sites / health / files / files / eudralex / vol - 10 / guidanceclinicaltrials_covid19_ en.pdf ( accessed april 2 , 2020 )  . vol 21 may 2020 comment published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections correction to lancet oncol 2019 ; 20 : 155665 correction to lancet oncol 2019 ; 20 : e658 correction to lancet oncol 2020 ; 21 : e31729 bertelsen ca , neuenschwander au , jansen je , et al . 
lancet oncol 2019 ; 20 : 155665in this article , two patients ( one in the control group and one in the complete mesocolic excision group ) were incorrectly classified as not having recurrences , due to an error in data extraction . 
 the incorrect data have been updated in the summary findings , the results , figures 2a and 2c , table 3 , supplementary figures 2c and 2f in the appendix , and the discussion . 
complete mesocolic excision for colon cancer : is now the time for a change in practice ? lancet oncol 2019 ; 20 : 147476in this comment , the cumulative incidence of recurrence in each group has been amended , owing to these data being corrected in the linked article by bertelsen and colleagues . 
lancet oncol 2019 ; 20 : e658 in this correspondence , the absolute in risk of recurrence reduction has been amended , owing to this being corrected in the linked article by bertelsen and colleagues . 
this correction has been made to the online version as of aug 3 , 2020 . correction to lancet oncol 2020 ; 21 : e33036 cooney tm , cohen jk , guimaraes cv , et al . 
these corrections have been made to the online version as of aug 3 , 2020 . vol 21 august 2020 e372 corrections correction to lancet oncol 2019 ; 20 : 128694 correction to lancet oncol 2019 ; 20 : 1506517 correction to lancet oncol 2019 ; 20 : e616 burki tk . 
 ff l u c i c l o v i n e a n d ga - psma - 11 pet - ct in patients with early biochemical recurrence after prostatectomy : a prospective , single - centre , single - arm , comparative imaging trial . 
lancet oncol 2019 ; 20 : 128694in this article , in figure 2 , the f - fluciclovine detection rate for prostate bed has been corrected to 9 ( 18% )  . 
this correction has been made to the online version as of sept 23 , 2019 . correction to lancet oncol 2019 ; 20 : 160214 oscarsson n , mller b , rosn a , et al . 
lancet oncol 2019 ; 20 : 1602 14in the summary of this article , the first sentence of the findings section should have read of 223 patients screened between may 9 , 2012 , and dec 20 , 2017 , 87 patients were enrolled and randomly assigned to either hyperbaric oxygen therapy ( n = 42 ) or standard care ( n = 45 )  . 
 this correction has been made to the online version as of sept 23 , 2019 , and the printed article is correct . kato k , cho bc , takahashi m , et al . 
nivolumab versus chemotherapy in patients with advanced oesophageal squamous cell carcinoma refractory or intolerant to previous chemotherapy ( attraction - 3 ) : a multicentre , randomised , open - label , phase 3 trial . 
 lancet oncol 2019 ; 20 : 1506517in this article , the name of the funder should be ono pharmaceutical company , and in the results section , paragraph eight , the data for the comparison between groups for the utility index should have been 0076 , 00110142 ; p = 0023 . 
lancet oncol 2019 ; 20 : e52234in this series paper , the value 55% was missing from in the the following sentence first paragraph of the strategies for providing paediatric oncology services section : data from hospital - based registries in the english - speaking caribbean islands show a 2 - year survival rate of 55% compared with 85% in hics . 
this correction has been made to the online version as of oct 30 , 2019 . published online september 23 , 2019 s1470 - 2045 ( 19 ) 30594 - 7 vol 20 november 2019 e613 corrections aacr cancels annual meeting because of sars cases people have died from the disease , and there have been 111 probable and 95 suspected in ontario . 
 newsdesk the american association for cancer research cancelled its annual meeting 3 days before it was due to begin in toronto , canada ( april 59 , 2003 ) because of recent outbreak of severe acute respiratory syndrome ( sars )  . countrys the cancelling the meeting was a difficult decision to make , says the organisations chief executive officer margaret foti ( philadelphia , pa , usa )  . the aacr received 6900 abstracts , booked 400 speakers , and expected about 16 000 participants to attend the meeting , foti explains . 
ten torontos medical officer of health , sheela basrur , wrote a letter to the aacr emphasising the precautions that health - care providers should take while attending the meeting but did not advise the organisation to cancel the conference , says a spokesperson from toronto public health . 
however , we were still says foti . receiving cancellations , some cancer centres were advising their staff not to attend because of concerns about travelling to countries affected by sars and the potential transmission of the disease from health - care professionals to their immunocompromised patients with cancer , she explains . 
 the aacr contacted the world health organization , the us centers for disease control and prevention ( cdc ) , and toronto health officials , all of whom noted that there is not concern currently widespread transmission of sars to the community in toronto . 
 about india cuts budget for cancer treatment the indian government has cut financial support for cancer research and treatment , despite the country facing the massive challenge of nearly one million new cancer cases every year . 
in the central governments annual budget for 20032004 , allocation for the national cancer control programme ( nccp ) has been reduced to rs 520 million from rs 580 million . 
the nccp official approached by the lancet oncology preferred to remain anonymous but did say that the cut may be due to the fact that we were not able to absorb all the funds allotted to us in the past . jyotsna govil of the indian cancer society remarks : this is a prime example of tokenism in matters of health . the allocation has been so meagre that a state like delhi receives as little as rs15 million per annum for hospitals run by the local administration . 
govil points out that it is obvious the government has little use for a cancer education and prevention programme , despite every medical authority saying the incidence can be cut by 70% with screening and awareness programmes . experts say india needs rational budgeting for cancer programmes . 
at present , patients presenting with latestage disease , because of lack of awareness , prove to be a financial burden as scarce resources are used in their treatment without much outcome in terms of long - term survival . in addition to awareness and early detection , we need to spend money on treatment facilities to do away with lists . 
only reproduce with permission from the lancet publishing group . corrections correction to lancet oncol 2013 ; 14 : 297 correction to lancet oncol 2013 ; 14 : 481 correction to lancet oncol 2013 ; 14 : 557 motzer rj , escudier b , tomczak p , et al . 
this correction has been made to the online version as of may 28 , 2013 . galimberti v , cole bf , zurrida s , et al , for the international breast cancer study group trial 2301 investigators . 
 lancet oncol 2013 ; 14 : 297305in the summary of this article , the fourth sentence of the findings section should read : breast cancer - related events were recorded in 48 patients in the axillary dissection group and 47 in the no axillary dissection group ( ten local recurrences in the axillary dissection group and eight in the no axillary dissection group ; three and nine contralateral breast cancers ; one and ve regional recurrences ; and 34 and 25 distant relapses )  . 
 this correction has been made to the online version as of may 28 , 2013 . tom waddell , oesophagogastric randomised , waddell t , chau i , cunningham d , et al . 
lancet oncol 2013 ; 14 : 48189in this article , list of authors should have the read : ian chau , david cunningham , david gonzalez , alicia frances clare okines , andrew wotherspoon , claire sa ery , gary middleton , jonathan wadsley , david ferry , wasat mansoor , tom crosby , fareeda coxon , david smith , justin waters , timothy iveson , stephen falk , sarah slater , clare peckitt , yolanda barbachano . 
this correction has been made to the online version as of may 28 , 2013 . vol 14 june 2013 e254 corrections correction to lancet oncol 2014 ; 16 : 767 correction to lancet oncol 2016 ; 17 : 431 , 434 , 435 correction to lancet oncol 2016 ; 17 : 953 weber js , geo gibney , sullivan rj , et al . 
 sequential administration of nivolumab and ipilimumab with a planned switch in patients with advanced melanoma ( checkmate 064 ) : an open - label , randomised , phase 2 trial . 
lancet oncol 2016 ; 17 : 94355in gure 5 , under the headings nivolumab followed by ipilimumab and ipilimumab followed by nivolumab , the text should have read number of events / number of patients . 
this correction has been made to the online version as of june 28 , 2016 , and the printed version is correct . correction to lancet oncol 2016 ; 17 : 995 , 1002 cella d , grnwald v , nathan p , et al . 
 quality of life in patients with advanced renal cell carcinoma given nivolumab versus everolimus in checkmate 025 : a randomised , open - label , phase 3 trial lancet oncol 2016 ; 17 : 9941003in this article , the order of references 711 has been corrected and the fourth sentence of the second paragraph of the introduction has been corrected to read furthermore , an analysis of hrqol scores according to the functional assessment of cancer therapy - kidney symptom index - disease related symptoms ( fksi - drs ) questionnaire ( a subscale of the 15 - item fksi - 15 ) showed that median change from baseline increased over time with nivolumab treatment . 
these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . jeong s - y , park jw , nam bh , et al . 
open versus laparoscopic surgery for mid - rectal or low - rectal cancer after neoadjuvant chemoradiotherapy ( corean trial ) : survival outcomes of an open - label , non - inferiority , randomised controlled trial . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2015 ; 16 : 1479 motzer rj , hutson te , glen h , et al . 
lancet oncol 2015 ; 16 : 147382in table 3 of this article , the number of patients in the lenvatinib plus everolimus group with grade 3 constipation should be 0 . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 351 untch m , jackisch c , schneeweiss a , et al . 
 lancet oncol 2016 ; 17 : 34556in this article , the data in the second sentence of the third paragraph of the results section should have read in multivariable logistic regression analysis , nab - paclitaxel remained an independent predictor for achievement of pathological complete response after adjustment for baseline and minimisation factors ( or 159 ; 95% ci 120211 ; p = 00013 )  . 
fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment o f h o r m o n e r e c e p t o r p o s i t i v e , her2 - negative metastatic breast cancer that progressed on previous endocrine therapy ( paloma - 3 ) : final analysis of the multicentre , doubleblind , phase 3 randomised controlled trial . 
lancet oncol 2016 ; 17 : 42539 in figures 2a , 5a , 5b , and 5c , the kaplan - meier curves should have intersected with the y - axis at the 100% mark . 
these corrections have been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 888 , 890 , 892 cancer antonia sj , lpez - martin ja , bendell j , et al . 
 lancet oncol 2016 ; 17 : 88395in this article , the rst line in the third paragraph of the results , blinded independent central review should have been investigator - assessed recist . 
in the seventh paragraph of the results , the number of patients in the nivolumab 3 mg / kg plus ipilimumab 1 mg / kg cohort who had diarrhoea as a serious adverse event should have been two ( 4% ) , not four ( 7% )  . 
 these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . vol 17 july 2016 e270 editorial listen to the lancet news podcast ( november 30 , 2012 ) on the access to medicine index at com / lancet - news - audio - 2012 / for the access to medicine index 2012 report see accesstomedicineindex.org / for the projected increase in cancer burden in low - resource countries see articles lancet oncol 2012 ; 13 : 790801 for more on shortages of generic cancer drugs see editorial lancet oncol 2011 ; 12 : 313 for the inctr report on drug shortages in uganda see children - with - burkittlymphoma - are - dying - in - uganda access to cancer medicine in low - resource settings this chronic disease awareness of the global burden of cancer is growing , with increasingly a ecting countries of low to middle income . 
although the clinical focus on prevention , treatment , and research still lies very much within the domain of high - income countries , greater e orts have to be made globally . 
 in low - income settings , access to therapeutic drugs is also part of the problem : an issue addressed by the access to medicines index , published on nov 28 , 2012 , which speci cally examined the role of pharmaceutical companies in making their drug portfolios available to low - resource countries . the access of medicines index is published every 2 years and is funded by organisations including the uk department for international development and the bill and melinda gates foundation . 
 the index shows pharmaceutical companies are taking global access and their moral responsibilities seriously , by putting in place tiered - pricing schemes and ensuring that drugs research and development pipeline are relevant to developing countries . 
 companies who had not made major advances in the past 2 years , such as astrazeneca , found themselves slipping down the rankings , even though their e orts have not worsened . 
worryingly though , only four companies enforce codes of conduct in their use of contact research organisations , leaving trial participants from developing countries vulnerable to clinical malpractice . in the further caution is needed from an oncological point of view : much of the index focuses on drugs used to treat typical developing world diseases , such as hiv , malaria , and vaccines for infections . 
as low - resource countries make the transition to middle - income countries , cancer burden will increase as a result of an ageing population , new risk factors , and lifestyle changes . it could be argued that since access toand resources forcancer treatment are so limited in developing countries , the answer lies in a greater reliance on generic drugs . 
a recent defeat of a parliamentary bill in canada to alleviate restrictions on canadas access to medicines regimewhich would have made it easier for manufacturers to produce and distribute generic drugs globallyfurther indicates a reluctance to tackle this issue . 
individual hospitals that could previously purchase the drugs they required directly are now unable to do so , and consequently children are dying needlessly . as the focus on cancer shifts to developing nations , these countries must make the e ort to implement long - term health - care programmes that incorporate cancer care as a central component of their health coverage , rather than as an add - on . 
nevertheless , sustained commitment and partnership by all stakeholders is necessary to tackle the increasing burden of cancer , and the engagement of morally responsible corporate businesses are an important part of the equation . 
 the lancet oncology vol 14 january 2013 cancer care in the commonwealth caribbean in covid times the language of urgency that we have grown used to in these so - called covid times could well be applied to the problem of cancer care and control in the small island nations of the caribbean . 
as the second leading cause of death , 1 and with the prediction that cancer cases will rise by 66% in the next 10 years , 2 this alone should serve as an urgent call to arms for governments and health services in the region . the covid - 19 pandemic has shown us how well we can connect virtually when we need to , and how connections and partnerships that previously did not seem likely or possible have suddenly become the bedrock of our moving forward . 
we must also establish clear pathways of care , especially in small island nations who can link together to provide an expert consultation service with a wide reach . the commonwealth caribbean comprises 18 englishspeaking nations . 
many are classified as high - income countries ( hics ) or upper middle - income countries by the world bank ; however , their health services , including cancer care , are unlike those of larger hics.3 most have small , open economies , are heavily dependent on tourism , and are increasingly susceptible to climate change . 
 the most common cancer types are prostate cancer in men and breast cancer in women , and mortality from these cancers in the caribbean is among the highest in the world.1 additionally , cervical cancer , which should be entirely preventable , is still the second leading cause of cancer death in women in many caribbean countries.1 although primary health - care services are generally well established in the region , secondary and tertiary services vary greatly between countries . 
the capacity of caribbean health systems to provide optimal cancer care remains inadequate in the context of other competing priorities , with poor diagnostic and supporting service infrastructure , and an insufficient cadre of trained personnel to deliver the types of care needed . 
patients might have to travel long distances , including air travel , often at substantial expense , to access care.3 although core cancer treatments such as surgical oncology , medical oncology , and radiotherapy are more readily available in the larger islands ( eg , the bahamas and jamaica ) , inadequate numbers of trained specialists mean there are often long waiting lists , compounding the issue of advanced disease presentations.4 we need to reframe and reemphasise priorities for improved cancer care in the region . 
first , we must devise and implement strategies for improving existing cancer care services , focusing on : better cancer surveillance and data collection ; preventing the preventable ; streamlining referral pathways and linkages between cancer care providers , both within and between countries ; and developing and implementing resourcestratified guidelines across the cancer care continuum from prevention through to palliative and end - of - life care.4 second , we must propose new strategies for the expansion of cancer care in the region that are affordable and achievable and with the principal focus on the education and training that will expand the current cadre of health - care professionals . cancer data from cancer surveillance systems are critical to identify public health needs and help to drive policy , yet these are poorly developed in the caribbean . 
 to correct this situation , the international agency for research on cancer ( iarc ) has launched iarc caribbean cancer registry hub offerring technical assistance for the collection of high - quality cancer care data to support an evidence - based approach to cancer care policy and planning in the region within the framework of global initiative for cancer registry development . 
so far , 16 caribbean countries have been engaged with the caribbean hub and 13 countries have participated in capacity - building activities . for world banks country classification see datahelpdesk.worldbank.org / knowledgebase / articles / 906519 for caribbean cancer registry hub resources and technical assistance see caribbeancrh.carpha.org for global initiative for cancer registry development see vol 21 august 2020 1007 comment for more on organization of eastern caribbean states and full list of members see we - are / member - states in terms of preventing the preventable , we are reminded that cervical cancer is now earmarked for elimination in the countries of the americas , including the caribbean . 
thus , continued implementation of human papillomavirus ( hpv ) vaccination using the 9 - valent vaccine , effective against the highrisk hpv types circulating in the caribbean , 5 is urgently needed for 926 year olds , 6 along with targeted hpv screening of high - risk women , aged 30 years or older . 
 countries will need to achieve screening rates of at least 80% in this population to have the greatest impact in reducing deaths from cervical cancer . a focus on strengthening and streamlining existing clinical pathways and institutional guidelines for cancer care will be critical . 
implementing resource - appropriate , strategic plans to improve patient access to early diagnosis and early treatment in two or three common cancers would help reduce morbidity and mortality and health - care costs in the longer term.7 many of the larger island nations do have extensive resources for the treatment of breast , prostate , and colorectal cancers , although these might not be united under one roof , and referral pathways and linkages between the separate services of diagnostic imaging , surgery , pathology , medical and radiation oncology , and palliative care might not be robust or clearly defined8 ( yeung l , university of british columbia , personal communication )  . 
resources such as the breast health global initiatives publication , knowledge summaries for breast cancer , 4 provide an excellent template for health - care professionals aiming to improve patient access to existing services . 
improved coordination of services requires developing strong referral networks with clear guidelines for providers on how to refer patients efficiently and appropriately through the syste providers are encouraged to hold multi - disciplinary team meetings and tumour boards to foster better communication and regular collaboration . 
another valuable innovation , relatively new to the caribbean , is the introduction of cancer patient navigation programmes , which help to increase patient access to , and use of , appropriate resources for cancer care.9 such programmes are already being introduced in trinidad and tobago and jamaica . strategies for the further expansion of cancer care in the caribbean islands must take a broad view . 
models for this type of approach already exist in the region.3 task shifting through education and the development of community - based services , including palliative care , is imperative as we adjust to a new normal of social distancing and increasing barriers to traveling to seek care . inter - island and intra - island collaborative efforts are ongoing . 
the initiative includes professionals involved in all aspects of cancer care working together to use available expertise to facilitate the provision of optimal cancer diagnostic and treatment plans for their under - resourced include shared health systems . 
larger caribbean countries are urged to consider this type of approach that can increase collaboration and connectivity between service providers , to improve access and availability of care for all . we believe that by taking the steps discussed , we can make substantial improvements in the cancer care that is already offered in the caribbean and move towards offering excellent , guideline - recommended care for all people living in this region . we declare no competing interests . * glennis andall - brereton , brittany bromfield , steven smith , dingle spence andallgl@carpha.org 1008 vol 21 august 2020 comment caribbean public health agency , port of spain , trinidad and tobago ( ga - b ) ; jamaica cancer care and research institute , kingston , jamaica ( bb , ss , ds ) ; and hope institute hospital , kingston , jamaica ( ds ) razzaghi h , quesnel - crooks s , sherman r , et al . 
 health - sciences / epidemiology / bci - 25 / kspdf / ks%20planning%20 access%20030617.pdf ( accessed june 29 , 2020 )  . andall - brereton g , brown e , slater s , et al . 
cancer patient navigator tasks across the cancer care continuuj health care poor underserved 2012 ; 23 : 398413 . 100 european core quality standards for cancer care and research centres there have been calls for consensus around defining quality standards for cancer care , treatment , and research in europe , with a focus on cancer hospitals , centres , and networks . 
although cancer survival is generally improving , large variation in cancer survival between countries remains , as shown by results in the eurocare - 5 study.1 the european commissioner for health and food safety has launched europes beating cancer plan . 
 in addition , a cancer mission is being drafted by the european commission , 2 with some objectives most likely to be focused on the need to ensure quality of treatment , care , and research , and to create more comprehensive cancer centres and infrastructure.3 , 4 in europe , many cancer centres , which act as hubs interlocking clinical research networks , provide state - of - the - art cancer services . 
therefore , an aim for both the cancer mission and beating cancer plan could be to establish at least one comprehensive cancer centre or large clinical centre in each small eu member state , and to have one comprehensive cancer centre for every 510 million people in the population in larger eu member states , as part of an integrated infrastructure.5 in 2008 , the organisation of european cancer institutes ( oeci ) created a quality assurance accreditation and designation programme for cancer centres , 6 which includes 50 of the largest cancer centres in 14 of 27 eu member states , plus norway and the uk . 
collectively , these centres produce more than 12 400 peer - reviewed publications on cancer research annually , have a total annual research budget of over 1 billion , and have treated more than 1 million new patients since accreditation . 
although these centres treat only 10% of patients diagnosed with cancer in the eu each year , their effect on the quality of cancer care and research is substantial , as they are considered as national reference centres . the accreditation and designation programme focuses on institutional quality and capabilities , with the objective of providing comprehensive accreditation for quality oncology care , including prevention , care , research , education , networking , and patient involvement . 
inclusion of these issues is a unique feature of this oeci programme , compared with cancer accreditation systems in the usa and germany , where clinical care and cancer research are generally accredited separately . 
in addition , the oeci standards have been accredited by the international society for quality in health care . the 50 participating cancer centres are shown in the appendix ( p 1 )  . 
stampedean international , open - label , randomised controlled trialuses a novel multiarm , multistage design to assess whether the early additional use of one or two drugs ( docetaxel , zoledronic acid , celecoxib , zoledronic acid and docetaxel , or zoledronic acid and celecoxib ) improves survival in men starting rst - line , long - term hormone therapy . 
here , we report the preplanned , second intermediate analysis comparing hormone therapy plus celecoxib ( arm d ) with hormone therapy alone ( control arm a )  . methods eligible patients were men with newly diagnosed or rapidly relapsing prostate cancer who were starting long - term hormone therapy for the rst time . 
patients randomly allocated to arm d received celecoxib 400 mg twice daily , given orally , until 1 year or disease progression ( including prostate - speci c antigen [ psa ] failure )  . 
accrual of further patients was discontinued in any research arm showing safety concerns or insu cient evidence of activity ( lack of bene t ) compared with the control arthe minimum targeted activity at the second intermediate activity stage was a hazard ratio ( hr ) of 092 . 
this trial is registered with clinicaltrials.gov , number nct00268476 , and with current controlled trials , number isrctn78818544 . findings 2043 patients were enrolled in the trial from oct 17 , 2005 , to jan 31 , 2011 , of whom 584 were randomly allocated to receive hormone therapy alone ( control group ; arm a ) and 291 to receive hormone therapy plus celecoxib ( arm d )  . 
at the preplanned analysis of the second intermediate activity stage , with 305 ffs events ( 209 in arm a , 96 in arm d ) , there was no evidence of an advantage for hormone therapy plus celecoxib over hormone therapy alone : hr 094 ( 95% ci 074120 )  . 
there was no evidence of di erences in the incidence of adverse events between groups ( events of grade 3 or higher were noted at any time in 123 [ 23% , 95% ci 2027 ] patients in arm a and 64 [ 25% , 1930 ] in arm d )  . 
the most common grade 35 events adverse e ects in both groups were endocrine disorders ( 55 [ 11% ] of patients in arm a vs 19 [ 7% ] in arm d ) and musculoskeletal disorders ( 30 [ 6% ] of patients in arm a vs 15 [ 6% ] in arm d )  . 
the independent data monitoring committee recommended stopping accrual to both celecoxib - containing arms on grounds of lack of bene t and discontinuing celecoxib for patients currently on treatment , which was endorsed by the trial steering committee . interpretation celecoxib 400 mg twice daily for up to 1 year is insu ciently active in patients starting hormone therapy for high - risk prostate cancer , and we do not recommend its use in this setting . 
accrual continues seamlessly to the other research arms and follow - up of all arms will continue to assess e ects on overall survival . funding cancer research uk , p zer , novartis , sano - aventis , medical research council ( london , uk )  . introduction prostate cancer is a major health problem worldwide , accounting for nearly a fth of all newly diagnosed male cancers . 
in the uk , roughly 35 000 men are diagnosed with prostate cancer each year , and in 2008 almost 10 000 men died from the disease.1 globally , 913 000 cases were diagnosed in 2008.2 the current standard rst - line treatment for locally advanced or metastatic prostate cancer is hormone therapy , achieved either surgically with bilateral orchidectomy or medically with luteinising hormone releasing hormone ( lhrh ) agonists or antagonists , or oral antiandrogens , 3 with additional radiotherapy for locally advanced cases.4 , 5 hormone therapy produces responses in up to 95% of patients , but lancet oncol 2012 ; 13 : 54958 published online march 26 , 2012 doi : 10.1016 / s14702045 ( 12 ) 70088 - 8 this online publication has been corrected . 
at this point , patients are potentially tter and better able to tolerate treatment , and intervention in the hormone - naive setting might have a better and more durable e ect . innovative , multiarm , multistage the stampede trial ( systemic therapy for advanced or metastatic prostate cancer : evaluation of drug e cacy ; medical research council [ mrc ] pr08 ) is ( mams ) , multicentre , randomised controlled trial . 
we designed the trial to assess the e ects of a bisphosphonate ( zoledronic acid ) , a cytotoxic chemotherapy drug ( docetaxel ) , and a cyclo - oxygenase - 2 ( cox - 2 ) inhibitor ( celecoxib ) , as single agents or combinations , in patients locally advanced or starting hormone therapy for metastatic prostate cancer . 
the trial is designed with separate stages focusing on safety , activity , and e cacy data ; a research arm is only allowed to proceed to the nal stage of recruitment if the study treatment is shown to be acceptably safe and su ciently active . 
we refer to lack of su cient activity as lack of bene t . cox - 2 is an isoenzyme induced by various mitogens , cytokines , and growth factors that are associated with a range of processes including in ammation12 and carcinogenesis.13 , 14 various case - control studies have shown a reduction in risk of prostate cancer associated with the use of non - steroidal anti - in ammatory drugs ( nsaids ) , which include inhibition of cox - 2 among their mode of action.15 pathological studies show that cox - 2 is upregulated in carcinomas , 16 and one study suggested that nsaid use might delay progression from subclinical to clinical prostate cancer.17 this combination of preclinical and epidemiological data justi ed assessment of a cox - 2 inhibitor in the present trial . the trial development group ( including clinical researchers , statisticians , trialists , and patient representatives ) chose to assess the selective cox - 2 inhibitor , celecoxib , because data suggest that it is better tolerated than other nsaids , exhibits activity as a cancerpreventing agent , 18 and shows inhibition of angiogenesis and induction of apoptosis in human cancer cells including prostate cancer , 19 particularly at higher doses.20 this decision was taken after full consideration of the risks and bene ts , in view of reports of potential adverse cardiovascular e ects.21 no safety concerns were raised during the pilot phase and the rst intermediate activity analysis , and the celecoxib arms were permitted to continue accrual . 
here , we report the results of the second intermediate analysis comparing hormone therapy alone with hormone therapy plus celecoxib . methods study design and participants stampede uses an adaptive multiarm , multistage design.22 , 23 this seamless phase 23 design starts with several trial arms and uses an intermediate outcome to adaptively focus accrual away from the less encouraging research arms , continuing accrual only with the more active interventions . 
the intermediate primary outcome is failure - free survival ( ffs ) de ned as the rst of : psa failure ( psa > 4 ng / ml and psa > 50% above nadir ) ; local progression ; nodal progression ; progression of existing metastases or development of new metastases ; or death from prostate cancer . 
ffs is used as a screening method for activity on the assumption that any treatment that shows an advantage in overall survival will probably show an advantage in ffs beforehand , and that a survival advantage is unlikely if an advantage in ffs is not seen . 
it is not assumed that ffs is a surrogate for overall survival ; an advantage in ffs might not necessarily into a survival advantage . translate the trial is managed by a trial management group ( tmg ) chaired by the chief investigator . 
accumulating comparative data are reviewed by the independent data monitoring committee ( idmc ) and recommendations are made to the trial steering committee ( tsc ) , which includes independent members , who have the nal responsibility for decision making ( eg , on stopping arms )  . 
we included patients with newly diagnosed prostate cancer with metastases to bone , node - positive disease , or clinically localised disease with high - risk features ( at least two of the following : t category 3 or 4 , gleason sum score 810 , or psa 40 ng / ml )  . 
 additionally , men failing previous localised therapy were eligible ( subject to restrictions on prior hormone therapy ) if they had a psa concentration of 4 ng / ml or 550 vol 13 may 2012 articles higher and doubling time of less than 6 months , or psa 20 ng / ml or higher , or nodal or metastatic relapse . patients had to be t for any of the trial treatments , with adequate haematological , renal , and liver function , and have a who performance status of 0 or 1 . 
all patients provided written informed consent . randomisation and masking computer - based randomisation was done centrally ( via telephone ) using minimisation with a random element of 80% allocation towards minimising arms , balancing on minimisation factors of randomising centre , metastases , nodal involvement , age at randomisation , who performance status , type of hormone therapy , regular aspirin or nsaid use at baseline , and planned use of radiotherapy . 
patients could be allocated primary outcome hazard ratio power onesided alpha critical hazard ratio control events stage i : activity stage ii : activity stage iii : activity stage iv : e cacy os 075 075 075 075 0500 100 0250 092 0100 089 0025 ffs = failure - free survival . 
 further details on the design and conduct of the trial are presented elsewhere.24 , 25 procedures all patients were planned to receive long - term hormone therapy for at least 2 years , and were allowed to start longterm hormone therapy up to 12 weeks before randomisation . 
the permitted methods of hormone therapy were lhrh analogues ( with short - term antiandrogens to cover disease are when necessary ) , maximum androgen blockade , lhrh antagonists , orchidectomy , or , patients without metastasis , bicalutamide monotherapy ( 150 mg daily ) ; choice of hormone therapy was based on clinician and patient preference . 
radiotherapy was encouraged for men with n0m0 disease ( stratifying on intent ) , with a target window of 69 months after starting hormone therapy , so that radiotherapy could be given at the same time in all trial arms and patients would not have chemotherapy and radiotherapy concomitantly . 
 patients allocated to celecoxib were planned to receive one 400 mg capsule twice daily , taken orally , until 1 year or an ffs event . patients were followed up every 6 weeks for 6 months , then every 12 weeks for 2 years , then every 6 months for 5 years , and annually thereafter . 
 2043 men starting long - term hormone therapy for prostate cancer randomised 584 arm a ( control ht - alone ) 292 arm c ( ht + docetaxel ) 291 arm d ( ht + celecoxib ) 293 arm b ( ht + zoledronic acid ) 292 arm e ( ht + docetaxel + zoledronic acid ) 291 arm f ( ht + celecoxib + zoledronic acid ) intermediate data presented in this report data remain masked : excluded from this report data remain masked : excluded from this report intermediate data presented in this report data remain masked : excluded from this report data remain masked : excluded from this report 584 hormone therapy ( 100% ) 0 celecoxib ( 0% ) 582 activity analysis ( 100% ) * 527 safety analysis ( 90% ) 209 ffs events median ffs = 27 months 291 hormone therapy ( 100% ) 245 celecoxib ( 84% ) 291 activity analysis ( 100% ) 259 safety analysis ( 89% ) 96 ffs events median ffs = 24 months accrual continues follow - up ongoing accrual continues follow - up ongoing accrual continues follow - up ongoing accrual stopped follow - up ongoing accrual continues follow - up ongoing accrual stopped follow - up ongoing figure 1 : trial pro le ht = hormone therapy . 
this is because the control group is in every pairwise comparison and the power of these comparisons is improved by having more patients in this group . statistical analysis the sample size was calculated using - nstageand its predecessor programs . 
we targeted a 25% relative reduction in events ( hazard ratio [ hr ] 075 ) for both ffs and survival ; this translates to a 9% absolute improvement at the median time . 
these parameters were chosen to ensure that meaningful amounts of new data would be accumulated between intermediate analyses , which were triggered when speci c numbers of events had been reported in the control group ( table 1 )  . 
the overall alpha and power levels represent the values for each pairwise comparison of research arm against the common control arm , accounting for intermediate analyses and repeated use of the control arm . the statistical design parameters translate into a series of activity hurdles against which each research arm is compared at three prede ned intermediate analyses.24 at the end of the second activity stage , reported here , the hr cutpoint was 0924 , determined with 95% power and a one - sided alpha of 025 , with analyses planned for when roughly 216 ffs events had been reported in the control group . 
it was anticipated that research arms with an hr less favourable than the cutpoint would be considered as showing insu cient activity and accrual might therefore be stopped ; accrual would continue to the remaining trial arms to collect further evidence . there is no single sample size target for stampede ; the trial targets a total of 405 deaths in the control arm in comparisons with active research arms , but the number of patients required to observe these events depends on the accrual rate , actual event rate ( mix of patients joining the trial ) , and number of research arms shown the intermediate stages . 
the duration of accrual and follow - up are adjusted to obtain this target.24 we anticipated that around 25004000 patients would join stampede over 68 years , with around 1500 patients in comparisons of research arms showing encouraging evidence at each intermediate analysis . 
twice as many patients are recruited to the control group as to any of insu ciently active at to be standard survival analysis methods were used for time - to - event data . 
coxs proportional hazards models were used to estimate the relative treatment e ects , adjusting for key strati cation factors , with relative improvements expressed as hrs ; hr less than 100 favours a research ar the proportional hazards assumption was tested ; provision was made to report restricted mean survival times and to translate the stopping boundaries appropriately in the instance of a non - proportional treatment e ect over time.26 all cis are provided at the 95% level for tradition , but a one - sided 75% ci is also included for primary comparison of ffs , in line with the trial design . 
 analyses were done with stata ( version 11 )  . the trial is registered with clinicaltrials.gov , number nct00268476 , and with current controlled trials , number isrctn78818544 . role of the funding source the trial was sponsored by the mrc and conducted by the mrc clinical trials unit . 
 ( continues in next column ) table 2 : baseline characteristics vol 13 may 2012 articles months number of patients ( stopped ) 245 ( 28 ) 194 ( 25 ) 137 ( 19 ) 107 ( 32 ) 64 ( 52 ) 9 ( 7 ) figure 2 : time on celecoxib for patients in arm d ( hormone therapy plus celecoxib ) only patients who reported starting celecoxib treatment are included . 
the drop at 12 months re ects patients completing their trial treatment ; events before then represent patients stopping trial treatment sooner , for any reason . ht only ht + c time from randomisation ( months ) ( 160 ) ( 62 ) ( 35 ) ( 27 ) number of patients ( events ) ht only ht + c figure 3 : kaplan - meier curve of failure - free survival in arm a ( hormone therapy alone ) versus arm d ( hormone therapy plus celecoxib ) ht = hormone therapy . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results data were frozen on feb 1 , 2011 , for review by the idmc on march 31 , 2011 . 
figure 1 shows the ow of patients through the trial ; table 2 gives the baseline characteristics of patients in this comparison . in both arms , androgen - deprivation therapy was lhrh based in nearly all patients ( 574 of 584 [ 98% ] in the control group and 286 of 291 [ 98% ] in the hormone therapy plus celecoxib group ) , with radiotherapy planned for around a quarter of patients . 
the reason for stopping celecoxib was known for 107 of these patients : 45 ( 42% ) completed protocol treatment , 30 ( 28% ) had disease progression , 12 ( 11% ) had excessive toxicity , and 20 ( 19% ) stopped for other reasons . 
in the hormone therapy plus celecoxib group , median ffs was 24 months ( 95% ci 1733 ) , with an ffs at 2 years of 51% ( 95% ci 4358 )  . in the 209 patients in the control group who had an ffs event , the rst reported event was psa failure in 163 patients ( 78% ) , metastases in 33 ( 16% ) , local progression in ve ( 2% ) , lymph - node progression in ve ( 2% ) , and prostate - cancer - related death in three ( 1% )  . 
in the 96 patients in the hormone therapy plus celecoxib group who reported an ffs event , the rst event was psa failure in 75 ( 78% ) , metastases in 15 ( 16% ) , local progression in two ( 2% ) and prostate - cancer - related death in four ( 4% )  . at this second intermediate analysis , celecoxib showed insu cient evidence of activity , in terms of ffs , for continuation of accrual to this comparison : hr 094 from adjusted cox model ( 75% ci upper limit 103 ; 95% ci 074120 ; gure 3 )  . 
 because of the lack of bene t indicated by this analysis , the idmc recommended discontinuing recruitment to both celecoxib - containing groups ( hormone therapy plus celecoxib [ arm d ] , and hormone therapy plus celecoxib plus zoledronic acid [ arm f ] ) , and this was endorsed by the tsc . 
treatment with zoledronic acid continues in the combination group ( armf )  . there is some evidence of non - proportional hazards in the data , which is mostly explained by who performance status ( p = 0007 ) ; there was no evidence that the hazards for the treatment e ect are non - proportional over time ( p = 0387 )  . 
grade 35 tox icities were reported at any time by 123 ( 23% ; 95% ci 2027 ) patients in the control group and 64 ( 25% , 1930 ) in the hormone therapy plus celecoxib group . 
these data , including those for the hormone therapy plus celecoxib plus zoledronic acid group , remain con dential to the idmc and will only be available to the tsc after future analyses . discussion in the stampede trial , we are assessing several drugs in combination with hormone therapy in patients with high - risk localised or metastatic prostate cancer . 
 resources are focused on trial arms most likely to show a clinically meaningful survival bene t by using lack - of - bene t analyses and stopping intermediate accrual to arms showing insu cient activity or adverse safety pro les . the celecoxib arm continued accrual through the rst intermediate analysis ( target hr 100 ) , but accrual was stopped after the second intermediate analysis when the target hr was more di cult to pass , at 092 . 
although there were no safety concerns raised by the idmc , there was no evidence of bene t when the totality of the data were taken into consideration , and the tsc recommended that treatment with celecoxib stop for patients still receiving the drug . our premise is that an advantage in overall survival should be preceded by an advantage in ffs , so we do not anticipate a later bene t with celecoxib emerging ; however , this remains to be determined in subsequent analysis of overall survival after longer follow - up . 
in some crpc studies this assumption has not held up , particularly studies with the immunotherapy sipuleucel - t , where a survival advantage has been shown without a prior bene t in psa progression.10 the potential mechanisms of action of celecoxib are not androgen - linked , so it is reasonable to assume that they might not be re ected in psa - based measures of ffs ; on this basis , we continue long - term patient follow - up and avoid de nitive statements relating to the overall e cacy of cox - 2 inhibition and prostatecancer survival in this setting . recruitment was also stopped to the hormone therapy plus celecoxib plus zoledronic acid group ; data for this arm have not been revealed to avoid inappropriate in uence on recruitment in the other zoledronic acidcontaining arms . 
the patients in both celecoxib - containing groups remain in the trial and will continue to be followed vol 13 may 2012 articles up to provide data on overall survival . 
there would have been limited power for such a comparison at this stage . celecoxib , a selective cox - 2 inhibitor , was selected on the basis of preclinical13 , 14 , 19 and clinical1618 data suggesting possible utility in prostate cancer ( panel )  . 
the celecoxib dose and treatment duration chosen for the trial ( 400 mg twice daily for 12 months ) was based on the dose used for prevention of familial polyposis coli20 and the need to minimise potential for cardiovascular risk , which seems to present with treatment durations longer than 12 months.21 the dose and duration were selected after a comprehensive literature review followed by joint discussion with patient representatives on the tmg , emphasising the importance of such collaboration in the design and conduct of clinical trials . external clinical trial data that have emerged since the launch of stampede have been equivocal as to the value of cox - 2 inhibitors in prostate27 , 28 and colorectal29 , 30 cancers . 
so far , published trials have not supported the use of cox - 2 inhibitors unequivocally in any established cancer type ; our trial adds further evidence of their limited clinical utility in established tumours . 
we do note panel : research in context systematic review at the time of trial design , there was substantial epidemiological , laboratory , and clinical evidence that cox - 2 has a role in development and progression of a range of cancers , including prostate cancer . 
celecoxib was chosen for assessment in hormone - sensitive prostate cancer based on in - vitro evidence of activity and data in other cancers , particularly familial polyposis coli , where it has a role in prevention of progression from polyp to cancer . 
we assessed a range of drugs with cox - 2 - inhibitory properties and selected celecoxib based on the data in familial polyposis coli and its safety pro le in large - scale trials of other diseases . 
 data from trials of celecoxib in established cancers have been tracked through the registers ( including alerts and clinicaltrials.gov ) , and lead investigators have been contacted for information each time reviews are updated but registers do not include recent data . interpretation at the second preplanned intermediate analysis , we have shown that celecoxib given at 400 mg twice daily for 1 year is insu ciently active in high - risk , hormone - sensitive prostate cancer to signi cantly a ect failure - free survival . 
other trials in prostate cancer ( and other cancer types ) have not supported the use of cox - 2 inhibitors unequivocally in any setting , and our trial adds further evidence of the limited clinical utility of these drugs in established , advanced cancer . 
first , there could be lack of expression of the target molecule cox - 2 , which we could retrospectively assess by collecting tissue blocks and studying cox - 2 expression . 
second , there might be a lack of on - target activity ; celecoxib was chosen because of documented activity in the setting of familial polyposis coli , 20 thus it seems reasonable to assume that the drug dose and delivery are within the necessary therapeutic range . 
the initial planned duration of therapy was 2 years , but in view of the excess cardiovascular problems reported with rofecoxib29 just before accrual to stampede , a shorter duration was selected . 
even if the duration was too short for optimum e ect , we would still expect some e ect , particularly with a median time to progression of around 2 years . a key strength of stampede is that several therapeutic combinations are tested synchronously , thereby shortening the time to assess e cacy and toxicity in new drug combinations in hormone - naive patients undergoing hormone therapy . 
the entry criteria were intended to de ne a population with a poor prognosis , requiring long - term hormone therapy , and to test the hypothesis that interventions at the point of rst hormone manipulation improve long - term outcome . 
 the trial is predicated on the notion that high - risk prostate cancer includes a range of patients , from those with localised disease and poor prognostic characteristics ( based on t category , psa , and gleason score ) to those presenting with metastatic disease , and that current therapies have limited long - term e cacy in many cases . 
it seems likely that median survival will be higher than originally anticipated , which might be partly related to new , active therapies that patients can receive after their rst trial ffs event . 
further agents are emerging , including abiraterone , 34 cabazitaxel , 35 sipuleucel - t , 10 radium - 223 , 36 and mdv3100.37 , 38 with the recent demonstration of a 556 vol 13 may 2012 articles survival bene t with radical radiotherapy in patients with locally advanced disease , 4 , 5 we anticipate further improve ments in ffs and overall survival ; indeed , the trial was amended in november , 2011 , to mandate the use of radiotherapy in newly diagnosed n0m0 disease following these results.5 the accumulating event rate is monitored as part of trial oversight processes . the remaining trial arms continue to recruit new patients and their data remain masked . 
researchers might infer that there is at least some evidence of improved ffs in these arms , but such evidence is not su cient to stop or change the trial . 
a further change to the trial occurred in november , 2011 , with the intro duction of hormone therapy plus abiraterone as a new research arpatients in the new arm will only be compared with those randomised contemporaneously to the control group . 
the trial can adaptively introduce further research arms and stop early those arms showing a lack of bene t.24 further research arms are likely to be introduced into the trial . 
in conclusion , we have shown that celecoxib given 400 mg twice daily for 1 year is insu ciently active for men starting long - term therapy for high - risk prostate cancer , and we do not recommend its use in this setting . contributors ndj is chief investigator for the trial . 
all other authors declared that they have no con icts of interest . acknowledgments this work is partly funded by cancer research uk ( grant cruk / 06 / 019 )  . 
wededicate this report to the memory of jim stansfeld , patient representative on the trial management group at the design stage , who was crucial to the inclusion of celecoxib as a research arm in stampede . 
we thank members of the independent data monitoring committee ( christopher williams [ chair ] , doug altman , bertrand tombal , and reg hall ) , the trial steering committee ( jonathan ledermann [ chair ] , david kirk , and jim paul ) , and pamela bramble and altaf moledina from p zer , for providing technical advice on celecoxib . 
see appendix for the full list of investigators and sites , and for contributions from mrc sta members . comment all authors have received grant support from novartis switzerland for clinical trials of blood - concentration testing of imatinib . 
additionally , nw has received travel and accommodation support from novartis switzerland , and lad has received honoraria from novartis for blood - concentration testing of imatinib . us food and drug administration . 
enforcementactions / warningletters / ucm210191.htm ( accessed oct 10 , 2010 )  . larson ra , druker bj , guilhot f , et al , for the iris ( international randomized interferon vs sti571 ) study group . 
population pharmacokinetics of imatinib and the role of 1 - acid glycoprotebr j clin pharmacol 2006 ; 62 : 97112 . petain a , kattygnarath d , azard j , et al , for the innovative therapies with children with cancer european consortiupopulation pharmacokinetics and pharmacogenetics of imatinib in children and adults . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zhao f - h , lin mj , chen f , et al . 
performance of high - risk human papillomavirus dna testing as a primary screen for cervical cancer : a pooled analysis of individual patient data from 17 population - based studies from china . 
 lancet oncol 2010 ; 11 : 116071on page 1165 of this article , the right hand panel of gure 1a should state pooled speci city = 864% ( 838890 ) and the right hand panel of gure 1b should state pooled speci city = 851% ( 823879 )  . 
in table 1 of this review , data from hertel et al ( 2006 ) for number of conceptions , rst trimester loss , and deliveries , and from shepherd et al ( 2006 and 2008 ) and dargent et al ( 2007 and 2008 ) for number of deliveries were incorrect . 
 vol 12 january 2011 corrections correction to lancet oncol 2012 ; 13 : 817 , 818 , 822 correction to lancet oncol 2014 ; 15 : 1195206 correction to lancet oncol 2015 ; 16 : 52 shen q , fan j , yang x - r , et al . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . vol 16 january 2015 editorial this online publication has been corrected . 
the corrected version rst appeared at thelancet.com / oncology on june 29 , 2012 for more on the lancet oncologys call for gps to receive better education see leading edge lancet oncol 2009 ; 10 : 97 for more on variation in gp referral patterns for patients with cancer see articles lancet oncol 2012 ; 13 : 35365 for more on the partnership between cancer research uk and the royal college of general practitioners see news lancet oncol 2012 : 12 : e232 for more on qcancer risk calculators see for more on the challenges of supporting patients with multiple morbidities see articles lancet 2012 ; published online may 10 . 
a third of all young cancer patients reported their gps took no action despite presentation with common cancer symptoms and a quarter of patients had to visit the gp four or more times before their symptoms were taken seriously . 
if a young person presents with the same symptoms three times , gps should automatically refer them for further investigation . although the tct survey was small ( collating the opinions of only 300 patients ) , the ndings mirror those of lyratzopoulos and colleagues published in the lancet oncology in april , 2012 , that analysed more than 41 000 patients with 24 types of cancer . 
in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
 so what can be done to restore trust ? usefully , cancer research uk and the royal college of general practitioners have launched an initiative to support gps by putting together models of best practice , and by reviewing care pathways and thresholds for further investigation to ensure gps have better access to diagnostics and secondary care . 
 additionally , the department of health has announced a pilot project within gp practices of cancer - risk prediction tools ( qcancer risk calculators ) developed by researchers at the university of nottingha these successful these partnerships are good examples of engagement between policy makers and physicians with organisations that have a perceptive understanding of the patient viewpoint and of research realities and possibilities . 
 initiatives will be whether transforming the e ectiveness of the gp and improving patient care will take time to assess , but it is unlikely that they will prove to be a broad panacea . 
it is becoming increasingly clear , for example , that the uk health - care system is not designed to cope with multiple comorbiditiesa common situation among patients with cancerand in the future gps will need to take a central and proactive role in coordinating patient care throughout their entire journey within the national health service . 
this will require rethinking of the current infrastructure , and might require adjustments to gps case burdens to ensure su cient time is available for more thorough consultations , especially in socioeconomically deprived areas . while the role of the gp in cancer diagnosis is undeniably important , it is essential not to forget interdependency on improved patient education , screening , secondary care and access to latest treatments , supportive and palliative care , and coordinated long - term follow - up . 
 improved understanding of the factors contributing to the di erences between the uks cancer outcomes and those of other countries will provide important clues and solutions . 800 000 people visit a gp every day in the uk , but questions are increasingly being asked about the competency of those doctors that undermine patient trust . 
however , implementation of this bill could be a fresh start in a process of restoring trust and ensuring gps have access to the best tools necessary to provide a rst - class service and to guarantee all patients receive the best possible care . 
 the lancet oncology vol 13 june 2012 duplicate articles epirubicin , oxaliplatin , and capecitabine with or without panitumumab for patients with previously untreated advanced oesophagogastric cancer ( real3 ) : a randomised , open - label phase 3 trial tom waddell , ian chau , david cunningham , david gonzalez , alicia frances clare okines , andrew wotherspoon , claire sa ery , gary middleton , jonathan wadsley , david ferry , wasat mansoor , tom crosby , fareeda coxon , david smith , justin waters , timothy iveson , stephen falk , sarah slater , clare peckitt , yolanda barbachano summary background egfr overexpression occurs in 2755% of oesophagogastric adenocarcinomas , and correlates with poor prognosis . 
we aimed to assess addition of the anti - egfr antibody panitumumab to epirubicin , oxaliplatin , and capecitabine ( eoc ) in patients with advanced oesophagogastric adenocarcinoma . methods in this randomised , open - label phase 3 trial ( real3 ) , we enrolled patients with untreated , metastatic , or locally advanced oesophagogastric adenocarcinoma at 63 centres ( tertiary referral centres , teaching hospitals , and district general hospitals ) in the uk . 
eligible patients were randomly allocated ( 1 : 1 ) to receive up to eight 21 - day cycles of open - label eoc ( epirubicin 50 mg / m and oxaliplatin 130 mg / m on day 1 and capecitabine 1250 mg / m per day on days 121 ) or modi ed - dose eoc plus panitumumab ( meoc + p ; epirubicin 50 mg / m and oxaliplatin 100 mg / m on day 1 , capecitabine 1000 mg / m per day on days 121 , and panitumumab 9 mg / kg on day 1 )  . 
median overall survival in 275 patients allocated eoc was 113 months ( 95% ci 96130 ) compared with 88 months ( 7798 ) in 278 patients allocated meoc + p ( hazard ratio [ hr ] 137 , 95% ci 107176 ; p = 0013 )  . 
meoc + p was associated with increased incidence of grade 34 diarrhoea ( 48 [ 17% ] of 276 patients allocated meoc + p vs 29 [ 11% ] of 266 patients allocated eoc ) , rash ( 29 [ 11% ] vs two [ 1% ] ) , mucositis ( 14 [ 5% ] vs none ) , and hypomagnesaemia ( 13 [ 5% ] vs none ) but reduced incidence of haematological toxicity ( grade 3 neutropenia 35 [ 13% ] vs 74 [ 28% ] )  . interpretation addition of panitumumab to eoc chemotherapy does not increase overall survival and cannot be recommended for use in an unselected population with advanced oesophagogastric adenocarcinoma . 
 introduction gastric and oesophageal cancers are among the most common causes of cancer - related mortality , and were responsible for more than 11 million deaths worldwide in 2008.1 combination chemotherapy is bene cial in perioperative and advanced disease settings , although overall survival is poor . 
in patients with metastatic disease , median overall survival with best supportive care is about 3 months , which can be extended to about 10 months with chemotherapy.2 , 3 no inter nationally accepted standard of care regimen exists for advanced oesophagogastric although most adenocarcinoma , centres use doublet or triplet chemo therapy combinations with a platinumuoropyrimidine backbone . 
the real2 non - inferiority study established epirubicin , oxaliplatin , and capecitabine ( eoc ) as a standard rst - line regimen , and noted a median overall survival of 112 months.3 this result compared favourably with the alternative regimens assessed in real2 , including a combination of epirubicin , cisplatin , and uorouracil that had a median overall survival of 99 months . in the past decade , the egfr pathway has been recognised as one of the key proliferative pathways that is dysregulated during tumorigenesis . 
preclinical data con rm that transfection of egfr into human cancer cells is associated with an aggressive phenotype , 4 and several molecular aberrations within this pathway can function as potent oncogenes . 
in oesophagogastric adenocarcinoma , egfr overexpression is reported in 2755% of cases in published literature , 5 , 6 and has been associated with reduced overall survival in some series.5 , 7 ampli cation of egfr , measured by uorescence in - situ vol 14 may 2013 lancet oncol 2013 ; 14 : 48189 published online april 15 , 2013 s1470 - 2045 ( 13 ) 70096 - 2 this online publication has been corrected . 
 methods study design and participants real3 was an open - label , multicentre , phase 3 , randomised controlled trial , undertaken at 63 participating centres ( tertiary referral centres , teaching hospitals , and district general hospitals ) in the uk . 
the meoc + p schedule was established in an unplanned dosending study , 12 which was done because excessive toxicity ( primarily diarrhoea ) was noted when the drugs were initially combined at full dose . 
as reported previously , 12 eligible patients had histologically veri ed , untreated , metastatic or locally advanced inoperable adenocarcinoma or undi erentiated carcinoma of the oesophagus , gastro - oesophageal junction , or stomach . 
other eligibility criteria included who performance status see online for appendix 575 patients enrolled ( phase 13 ) 19 treated in phase 1 excluded from further analyses 3 ineligible 1 squamous - cell carcinoma ( on review ) 1 anaemia despite transfusions 1 cardiac comorbidities 553 included in phase 3 trial ( intention - to - treat population ) 275 randomly allocated eoc 278 randomly allocated meoc + p 4 withdrew after randomisation 5 deteriorated before treatment 1 deteriorated before treatment 1 had not started cycle 1 by trial closure 266 started eoc 276 started meoc + p figure 1 : trial pro le eoc = epirubicin , oxaliplatin , and capecitabine . 
exclusion criteria included previous chemotherapy ( including adjuvant chemo therapy ) , previous anti - egfr therapy , known brain metastases , and clinically signi cant cardiac disease or other signi cant comorbidity . 
recruitment largely oesophagogastric adeno carcinoma and therefore her2 status did not a ect eligibility . routine her2 predated testing the study was done in accordance with good clinical practice guidelines and the declaration of helsinki , and was approved by the north west research ethics committee . 
all patients provided written informed consent before screening investigations . randomisation and masking we randomly allocated patients ( 1 : 1 ) to standard eoc chemotherapy ( intravenous epirubicin 50 mg / m on day 1 , intravenous oxaliplatin 130 mg / m on day 1 , and oral capecitabine 1250 mg / m per day on days 121 ) or modi ed - dose eoc in combination with panitumumab ( meoc + p ; intravenous epirubicin 50 mg / m on day 1 , intravenous oxaliplatin 100 mg / m on day 1 , oral capecitabine 1000 mg / m per day on day 121 , and intravenous panitumumab 9 mg / kg on day 1 ) every 21 days . 
randomisation was done independently at the institute for cancer research clinical trials and statistics unit ( icr - ctsu ) by random permuted blocks ( block sizes of six and eight ) and strati ed by centre region ( locations were divided into 11 regions ) , extent of disease ( locally advanced vs metastatic disease ) , and performance status ( 0 vs 1 vs 2 )  . 
advice regarding dose modi cations for toxic e ects was provided in the protocol ( appendix )  . procedures the primary endpoint was overall survival , de ned as the time from randomisation until death from any cause . 
 secondary endpoints were progression - free survival ( pfs ) , de ned as the time from randomisation until documented disease progression or death from any cause ; response rate according to recist 1.0 criteria ; 13 toxicity graded according to national cancer institute common terminology criteria for adverse events ( nci - ctcae ) version 3.0 ; patient - reported outcomes ; and kras mutation status . 
results from patient - reported outcomes will be reported separately . data for patients recruited at royal marsden hospital were subject to source data veri cation by trust - appointed monitoring sta  . 
for other uk centres , the sponsor deemed it appropriate , in keeping with good clinical practice requirements , to undertake central monitoring and provide sites with training meetings and written guidance to ensure appropriate conduct of the trial . 
 participating centres were required to provide evidence con rming patient eligibility , including blood test results , histopathology reports , and imaging reports to ensure appropriate randomisation and strati cation at trial entry . 
recorded toxicities were cross - referenced against reported serious adverse events to ensure that all toxicities were captured and that all events meeting the criteria for a serious adverse event were reported as such . 
 statistical analysis the trial was powered to detect a 10% improvement in 1 year survival , from 45% for eoc to 55% with meoc + p , equating to a hazard ratio ( hr ) of 0749 . 
to achieve 90% power and a two - sided of 005 , we needed to include 509 events ( deaths from any cause ) and planned a total accrual of 730 patients . 
we also did a preplanned non - comparative interim analysis of response rate with meoc + p after the rst 200 patients were assessable for response ( phase 2 population )  . 
these data were reviewed by the independent data monitoring committee ( idmc ) , and con rmed an acceptable response rate of 52% in the meoc + p group , which exceeded the prede ned futility threshold of 45% . throughout the trial , unmasked data were reviewed by the idmc to examine the safety , scienti c validity , and conduct of the trial . 
at annual review of the data in october , 2011 , the idmc noted a statistically inferior overall survival outcome in the meoc + p group based on the occurrence of 169 events ( hr 153 , p = 00062 )  . 
in discussion with the trial management group , we decided to close the trial to further recruitment with immediate e ect , withdraw panitumumab , and cross all patients over to full - dose eoc . 
meoc + p = modi ed eoc plus panitumumab . table 1 : demographics and baseline characteristics of the intention - to - treat population 105 ( 38% ) 173 ( 62% ) 232 ( 83% ) 118 ( 42% ) 144 ( 52% ) 16 ( 6% ) 106 ( 38% ) 94 ( 34% ) 34 ( 12% ) 244 ( 88% ) 273 ( 98% ) 5 ( 2% ) meoc + p hazard ratio 137 ( 95% ci 107176 ; p = 0013 ) 100 number at risk meoc + p 278 135 130 time from randomisation ( months ) 49 38 12 10 3 2 figure 2 : overall survival in 553 patients in the intention - to - treat population , by treatment group patients still on treatment at the time of trial closure and treatment crossover were censored . 
meoc + p = modi ed eoc plus panitumumab . vol 14 may 2013 oesophagogastric junction 169 127 078207 overall locally advanced metastatic 1 metastatic site > 1 metastatic site stomach oesophagus age < 60 years age 60 years male female performance status 0 performance status 1 performance status 2 kras wild - type kras mutation patients 95% ci 553 494 302 192 167 217 215 338 458 235 287 164 137 107176 125 054288 139 107180 120 085169 179 120268 164 104258 132 090194 137 091207 136 099187 134 101176 152 085272 122 079190 148 107203 195 074513 150 103218 023 005115 articles 100 001 01 favours meoc + p favours eoc figure 3 : forest plot of hazard ratios ( hr ) for overall survival according to baseline characteristics eoc = epirubicin , oxaliplatin , and capecitabine . 
 * 61 patients were excluded because they were still on treatment and had not reached rst response assessment at time of data censoring . table 2 : responses by treatment group in 492 patients * results between june 2 , 2008 , and oct 17 , 2011 , we enrolled 575 patients , three of whom were withdrawn because they did not ful l eligibility criteria . 
additionally , 19 patients randomly allocated during the phase 1 dosending study were excluded from the intention - to - treat analysis.12 we included 553 eligible patients in the phase 3 intention - to - treat population , representing 76% of the planned accrual at the time of trial closure ( gure 1 ; table 1 )  . 
 median follow - up in patients who were alive at the time of analysis was 46 months ( iqr 18101 ) in the eoc group and 53 months ( 2695 ) in the meoc + p group . based on 251 events ( eoc 110 , meoc + p 141 ) at the time of reporting , median overall survival was lower in the meoc + p group than in the eoc group ( hr 137 , 95% ci 107176 , p = 0013 ; gure 2 )  . 
median overall survival was 88 months ( 95% ci 7798 ) in the number at risk meoc + p 275 278 113 100 time from randomisation ( months ) 25 24 6 4 2 0 figure 4 : progression - free survival in 553 patients in the intention - to - treat population , by treatment group patients still on treatment at the time of trial closure and treatment crossover were censored . 
 the funding sources were not involved in collection , analysis , and interpretation of data , writing of the report , or the decision to submit the paper for publication . 
 * p values are for comparison of grade 35 toxicity between the two groups . table 3 : reported toxicities according to treatment group in 542 assessable patients meoc + p group compared with 113 months ( 96130 ) in the eoc group ( gure 2 )  . 
35 ( 13% ) of 278 patients in the meoc + p group and 54 ( 20% ) of 275 patients in the eoc group were on treatment at the time of trial closure and were censored at this timepoint . 
figure 3 shows the forest plot analysis for subgroups tested , with a similar e ect favouring eoc noted between all subgroups . based on 333 events ( eoc 153 , meoc + p 180 ) , pfs did not di er between treatment groups ( hr 122 , 95% ci 098152 , p = 0068 ; gure 4 )  . 
1 - year pfs was 20% ( 95% ci 1426 ) in the meoc + p group compared with 21% ( 1427 ) in the eoc group . 61 patients who were still on treatment ( 37 in the eoc group and 24 in the meoc + p group ) and had not reached their rst response assessment at the time of data censoring were excluded from the response analysis . 
 116 ( 46% ) of 254 patients in the meoc + p group had a complete or partial response compared with 100 ( 42% ) of median relative dose intensity eoc group ( n = 266 ) meoc + p group ( n = 276 ) p value patients with relative dose intensity 80% epirubicin oxaliplatin capecitabine panitumumab epirubicin oxaliplatin capecitabine panitumumab 91% ( 7699 ) 89% ( 7599 ) 88% ( 7797 ) 184 ( 69% ) 177 ( 67% ) 188 ( 71% ) 92% ( 77100 ) 92% ( 78100 ) 88% ( 69100 ) 91% ( 77100 ) 198 ( 72% ) 200 ( 72% ) 175 ( 63% ) 196 ( 71% ) 036 0086 074 051 013 0072 data are median ( iqr ) or n ( % )  . 
 table 4 : relative dose intensity in 542 patients who started chemotherapy 238 patients in the eoc group ( odds ratio 116 , 95% ci 081166 , p = 042 ; table 2 )  . 542 patients received at least one cycle of chemotherapy and were assessed for toxicity ( table 3 )  . 
patients in the eoc group had increased rates of grade 34 peripheral neuropathy , neutropenia , febrile neutropenia , and thrombocytopenia compared with patients in the meoc + p group . 
overall , we noted no signi cant di erence between the two groups in terms of grade 35 toxicity when all toxicities were vol 14 may 2013 articles 100 log - rank p < 00001 median overall survival 43 months number at risk grade 14 rash grade 0 rash 219 17 113 5 34 1 8 0 2 grade 0 rash ( n = 57 ) grade 14 rash ( n = 219 ) median overall survival 103 months four patients died from toxicities regarded as related to meoc + p : one each of septicaemia , neutropenic sepsis , pulmonary embolism , and upper gastrointestinal haemorrhage . 
six patients died from toxicities regarded as related to eoc : one each of pneumonia , diarrhoea and dehydration , pneumonitis , and myocardial infarction , and two cases of neutropenic sepsis . for 542 patients who started treatment , the median number of cycles delivered was ve ( iqr three to eight ) in both trial groups . 
80 ( 30% ) of 266 patients who started eoc received all eight planned cycles of chemotherapy , as did 74 ( 27% ) of 276 patients who started meoc + p . 
 excluding these patients , the median number of cycles delivered was six ( iqr three to eight ) with eoc ( 80 [ 38% ] of 212 patients completed eight cycles ) and ve ( iqr three to eight ) with meoc + p ( 74 [ 31% ] of 241 patients completed eight cycles )  . overall , 1307 cycles of eoc were administered compared with 1375 cycles of meoc + p . 
table 4 shows the median relative dose intensity for each drug according to treatment group and the proportion of patients in each group achieving a relative intensity of at least 80% . in exploratory biomarker analyses of 276 patients treated with meoc + p , development of any grade of rash ( 219 patients ) was associated with signi cantly longer overall survival compared with patients with no rash ( 57 patients ; gure 5 )  . 
median overall survival was 103 months ( 95% ci 89116 ) and median pfs was 68 months ( 5978 ) in patients with grade 14 rash compared with median overall survival of 43 months ( 3354 ) and a median pfs of 37 months ( 2351 ) in patients with grade 0 rash ( p < 00001 for overall survival and pfs )  . however , outcomes in the grade 0 rash population might be negatively skewed by patients with rapid disease progression who received insu cient panitumumab to develop rash . 
 although possibly restricted by the smaller number of patients , in this analysis overall survival did not di er between patients who developed ( median 106 months [ 95% ci 90122 ] ) and those who did not ( 85 months [ 7199 ] ; hr 064 [ 95% ci 037111 ] , p = 011 )  . rash few tissue biomarker analyses have been undertaken to date . 
frequencies of tested biomarkers in the rst 200 patients are shown in table 5 and have been reported elsewhere.14 for ten patients with known kras mutant tumours , we noted a potential association with bene t from meoc + p , although this association was not signi cant ( gure 3 )  . 
further biomarker analyses are ongoing in the full trial cohort . discussion the real3 trial is one of two concurrent randomised phase 3 trials ( the other being the expand trial15 ) assessing the addition of anti - egfr monoclonal antibodies to chemotherapy in rst - line oesophagogastric cancer . 
based on the ndings of real3 , use of panitumumab in combination with eoc cannot be recommended in an unselected population with advanced oesophagogastric adenocarcinoma , and was associated with inferior overall survival and pfs . 
notably , this detrimental outcome in the experimental group was not predicted by the phase 2 endpoint of response rate ( overall response rate 52% with meoc + p )  . 
this trial does , however , con rm the e cacy of the eoc control group in this setting , with median overall survival and pfs results that are consistent with those previously reported in real2 ( 112 months for overall survival and 70 months for pfs ) .3 reported previously , 12 the poor outcome associated with meoc + p in this trial did not seem to be attributable to increased treatment - related deaths , and therefore other potential explanations for our ndings need to be considered . 
 first , combination of panitumumab with full - dose eoc in the initial stages of the trial was associated with unacceptably high rates of grade 3 diarrhoea ( four of the rst ve patients by cycle four )  . 
although doubtedly reduced the frequency of grade 34 diarrhoea with meoc + p ( 17% in phase 3 population ) , they also served to reduce the dose intensity of chemotherapy , which is re ected in the reduced incidence of grade 34 neutropenia and peripheral neuropathy noted in the meoc + p group . 
additionally , the dose intensity data show a reduced proportion of patients achieving at least 80% of the planned capecitabine dose in the experimental group , suggesting that meoc + p was still slightly more di cult to deliver than standard eoc . second , a negative interaction might have occurred between panitumumab and one or more of the eoc components . 
evidence in the setting of colorectal cancer suggests that the chemotherapy partner for anti - egfr therapy might be an important determinant of treatment e cacy , with oxaliplatin - containing regimens yielding inconsistent results . 
the opus16 and prime11 studies provide evidence of improved outcomes with the addition of cetuximab and panitumumab respectively , whereas no bene t was associated with the addition of cetuximab in the coin17 and nordic vii18 studies in the same setting . 
recent cell - line data also suggest that greater synergy might exist between anti - egfr therapy and irinotecan than with oxaliplatin.19 additionally , the coin trial17 results suggest that there might be a di erential bene t the uoropyrimidine partner , with patients receiving oxaliplatin plus uorouracil seemingly deriving increased bene t compared with those treated with oxaliplatin plus capecitabine . 
indeed , the 57% frequency of kras mutation in our population is in keeping with the 310% reported in other studies , 2022 and we did not note any braf mutations in 167 tumour samples tested . 
by contrast , gene copy number alterations ( ampli cations and deletions ) seem to be a relatively frequent nding in oesophagogastric adenocarcinoma and are more likely to represent the key molecular alterations driving carcinogenesis . 
two recent series23 , 24 of detailed genomic analyses in oesophagogastric adenocarcinoma reported that about 37% of tumours harbour copy number aberrations in genes that are deemed to be targetable , including kras , egfr , her2 , and met . 
randomised clinical trials are therefore needed to establish whether targeting of these oncogenic signal transduction pathways can meaningfully improve outcomes for patients . vol 14 may 2013 articles panel : research in context systematic review we designed the real3 trial in an attempt to improve outcomes with systemic therapy in advanced oesophagogastric adenocarcinoma . 
monoclonal antibodies directed against egfr had already been shown to improve outcomes in combination with chemotherapy in advanced colorectal cancer , therefore there was interest in pursuing this combination as a possible therapeutic strategy in upper gastrointestinal malignancy . 
 in preclinical studies , cetuximab can decrease egfr pathway signalling via reduced phosphorylation of egfr and akt in oesophagogastric cancer cell lines.25 in combination with chemotherapy , cetuximab results in synergistic inhibition of cell proliferation and enhanced apoptosis.2527 in hypoxic gastric cancer cell lines the addition of anti - egfr therapy reversed oxaliplatin resistance.26 additionally , a synergistic antitumour e ect of combined cetuximab and s - 1 was apparent in gastric cancer cell lines overexpressing egfr.25 , 27 in colorectal cancer , somatic mutations in codon 12 , 13 , or 61 of the kras oncogene confer resistance to panitumumab therapy.11 , 28 met ampli cation with or without kras mutations might be associated with resistance to cetuximab therapy in gastric cancer cell lines ; 29 however , no validated predictive biomarkers for this setting exist . therapy unfortunately , despite preclinical data suggesting a role for anti - egfr treatment of trial oesophagogastric adenocarcinoma , ndings are supported by two other phase 3 trials assessing anti - egfr therapy in this disease setting . 
the expand trial15 assessed the addition of cetuximab to a in 904 patients with cisplatin - capecitabine doublet previously untreated adenocarcinoma of the stomach the the real3 and gastro - oesophageal junction , and did not meet its primary endpoint of improved pfs ( hr 109 , 95% ci 092129 , p = 032 ) .15 expand also noted no improvement with the addition of cetuximab in either overall survival ( hr 100 , 95% ci 087117 , p = 095 ) or overall response rate ( 30% in the experimental group vs 29% for controls )  . 
the cog trial30 assessed the antiegfr tyrosine - kinase inhibitor ge tinib compared with placebo in the second - line treatment of 450 patients with oesophageal and type iii gastro - oesophageal junction cancers . 
however , improvements in pfs ( hr 0795 , p = 0017 ) and disease control at 8 weeks ( 255% in the experimental group vs 160% in controls , p = 0014 ) were noted , suggesting some activity of ge tinib in a small unde ned subset of patients . cancer trial dataset and taken together , these relatively consistent ndings suggest that the egfr pathway is unlikely to represent an important therapeutic target in most patients with oesophagogastric ( panel )  . 
however , this work is ongoing in the full translational analyses these represent a unique opportunity to further assess the molecular biology of advanced oesophagogastric adenocarcinoma within a randomised trial setting . 
furthermore , the evaluation of genetic aberrations in pathways linked to egfr signalling could still o er the prospect of identi cation of a low - frequency biomarker that identi es a subpopulation of patients bene ting from anti - egfr targeted therapy in this setting . contributors dc and ic were responsible for the initial concept and design of the trial . 
tw and afco were the trial physicians and were delegated responsibility for the day - to - day running of the study and real - time review of data on behalf of dc . 
all authors had input into the data interpretation and preparation of the nal report for publication . con icts of interest dc has received research funding from amgen , roche , sano - aventis , merck - serono , novartis , and celgene , and has had advisory roles ( uncompensated ) with roche and amgen . 
he has advisory roles with merck serono ( uncompensated ) , roche ( compensated ) , and sano - aventis ( compensated ) , and has received honoraria from roche and sano - aventis . 
 acknowledgments we thank all participating patients and sta at real3 trial sites , all uk principal investigators , and the royal marsden hospital research data management and statistics unit for additional statistical support . 
we also wish to acknowledge national health service ( nhs ) support provided through national institute for health research biomedical research centre funding at the royal marsden nhs foundation trust and institute of cancer research . 
 correction to lancet oncol 2020 ; 21 : 64554 correction to lancet oncol 2020 ; 21 : 144354 correction to lancet oncol 2020 ; 21 : e51927 smith i , robertson j , kilburn l , et al . 
 long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial . 
lancet oncol 2020 ; 21 : e51927in this review , the second sentence of the first paragraph of the section entitled cancer burden now describing the number of new cancer cases worldwide in 2017 should read according to analysis from the global burden of disease study , there were 168 million new cases of cancer . 
this correction has been made to the online version as of nov 30 , 2020 . correction to lancet oncol 2020 ; 21 : 156373 powles t , plimack er , soulires d , et al . 
pembrolizumab plus axitinib versus sunitinib monotherapy as firstline treatment of advanced renal cell carcinoma ( keynote - 426 ) : extended follow - up from a randomised , openlabel , phase 3 trial . 
lancet oncol 2020 ; 21 : 156373in table 1 of this article the n ( % ) for previous nephrectomy should read 357 ( 83% ) for the pembrolizumab plus axitinib group and 358 ( 83% ) for the sunitinib group . 
these corrections have been made to the online version as of nov 30 , 2020 , and the printed version is correct . correction to lancet oncol 2020 ; 21 : e30516 fangusaro j , witt o , herniz driever p , et al . 
these corrections have been made to the online version as of nov 30 , 2020 . vol 21 december 2020 e553 corrections reportage the challenges of breast cancer care in mexico during healthcare reforms and covid - 19 the recent outbreak of severe acute respiratory syndrome coronavirus 2 has placed an unprecedented strain on health - care systems worldwide . 
not only has the outbreak overwhelmed health - care facilities because of the sheer quantity of infected patients , but it has also forced physicians to prioritise the treatment of immediate life - threatening conditions over non - urgent ones to optimise resources and mitigate the spread of covid - 19 . 
 in the case of mexico , more than 1 410 000 cases of covid - 19 were confirmed in 2020 , with nearly 99 deaths registered per 100 000 population and a case fatality ratio of 88% . the covid - 19 pandemic reached mexico during a time of profound health - care restructuring . 
after a historic presidential election in july , 2018 , the new administration initiated a movement known as the cuarta transformacin , or fourth transformation , of the country ( the first was national independence in 1821 , the second was a reform movement that culminated in 1861 , and the third was the revolution in 1917 )  . 
specifically , the objectives of this new health policy are to guarantee that the uninsured sector of the population has access to free medical care , including primary care services , admission to hospitals , clinical tests , and medicines included in the national compendium of health supplies ; increase the efficiency , effectiveness , and quality of the national health system ; increase the human and infrastructural resources available to the institutions that comprise the national health system , with a particular emphasis on highly marginalised populations ; guarantee the effectiveness of public health strategies , programmes , and actions that facilitate health promotion and disease prevention ; and improve nationwide health protection under a comprehensive approach that prioritises disease prevention and implementation of timely interventions . following the announcement of these health objectives ( to be achieved by 2024 ) , a series of actions were undertaken with the goal of improving national health care . 
for example , a restructuring in the mechanisms related to the production , cost , and supply of medicines was initiated to demonopolise the pharmaceutical industry , eradicate corrupt activities , and reduce costs . 
 however , some undesired consequences occurred in the short term , including a national shortage of some essential antineoplastic drugs ( such as doxorubicin , cyclophosphamide , and paclitaxel ) and antiretrovirals . 
 this shortage temporarily left many around the country without access to their prescribed treatments , which in turn unleashed a series of protests in march , 2020 , led by patients and their families . in what is perhaps the most ambitious component of the health reform , the 17 - year - old public healthcare insurance plan seguro popular was replaced with a new scheme known as instituto de salud para el bienestar ( insabi )  . 
for context , mexicos healthcare system is fragmented into multiple insurance plans , including seguro popular ( replaced with insabi in january , 2020 ) , instituto mexicano del seguro social ( for formal sector workers ) , instituto de seguridad los trabajadores del estado y servicios sociales de ( for government workers ) , and the private sector . 
 seguro popular was intended for all those who were not affiliated to any other insurance plan , including people from underserved communities , informal sector workers , and the self - employed . 
 for instance , significant patient out - of - pocket spending , elevated administrative costs , and uneven quality of care remained important concerns many years after the introduction of this plan . 
thus , in november , 2019 , the chamber of deputies passed a reform to replace seguro popular with insabi , with the aim of delivering improved health care to the uninsured population through a more efficient syste however , some within the senate claimed that the operational rules of insabi were unclear and several states refused to accept this new health - care system , instead signing a non - adhesion agreement . 
 all of these actions have resulted in a complex and uneven medicos e investigadores en la lucha contra el cancer de mama , mexico city , mexico ( cv - g , anp , fm - c , alp ) ; centro de cancer de mama , hospital zambrano hellion tecsalud , tecnologico de monterrey , san pedro garza garcia , n.l. , mexico ( cv - g , aa - g , asf , fm - c ) ; and fundacion salvati , mexico city , mexico ( ia - t , aa - a ) platasale@hotmail.com cv - g reports consultancy fees or advisory role for roche , novartis , pfizer , and eli lilly ; speaker honoraria for roche , myriad genetics , and novartis ; and travel and accommodations expenses for roche , merck sharpe & dohme oncology , and pfizer . 
this situation has been especially worrisome for patients with breast cancer , as they make up the biggest proportion of oncology patients in the country and also lead its cancer - related mortality statistics . 
furthermore , patients with breast cancer in mexico are mostly diagnosed in advanced stages , which makes their timely and continued treatment an even more pressing issue . in response to this situation , many patients with breast cancer started reaching out to various associations to voice their concerns and publicly express the barriers they are facing to continue their treatments . 
hence , a collaborative initiative was started to provide these patients with a communication channel to document their concerns , with the ultimate goal of providing evidence to health policy makers regarding current obstacles to adequate breast cancer care . 
an online questionnaire was created to explore patients perceptions and experiences of current access to treatments in the mexican health - care systethe survey was developed by a team of medical oncologists , a psycho - oncologist , a clinical research fellow , and a public relations spokesperson , as well as by the leaders of both ngos . a total of 142 responses were registered from may to august , 2020 , with most originating from mexicos three largest cities . 
a considerable proportion of respondents had advanced breast cancer ( clinical stage iii or iv ) , an aggressive subtype ( her2 - positive or triple - negative ; appendix p 1 ) , or both . 
through the questionnaire , 118 ( 83% ) of respondents reported that their breast cancer treatments had been interrupted or modified at some point in the last year ( 13 [ 9% ] in the last trimester of 2019 , 32 [ 23% ] in the first trimester of 2020 , 54 [ 38% ] in the second trimester of 2020 , and 19 [ 13% ] did not specify the timing ) , whereas nine ( 6% ) reported not being able to start any form of treatment . 
the most frequently cited reasons for these two scenarios were vol 22 february 2021 the replacement of seguro popular with insabi ( 76 [ 60% ] of 127 ) , the covid - 19 pandemic ( 52 [ 41% ] ) , and the national shortage of antineoplastic drugs ( 44 [ 35% ] )  . 
 only 50 ( 39% ) of 127 respondents with suspended or non - initiated treatments answered that they were able to eventually resume or commence thethe median time from treatment suspension to re - initiation was 60 days ( iqr 3776 )  . 
furthermore , 98 ( 69% ) of 142 respondents reported that , between october 2019 and august 2020 , they had made an out - of - pocket payment for treatment regimens that were previously covered by their health insurance . the findings of this study indicate that the treatment of patients with breast cancer in mexico has been negatively affected by the concurrent covid - 19 contingency and the process of adaptation to the new health - care policies . 
however , we risk losing what has been achieved if we let patient care suffer during these times of global struggle . for more on the pitfalls of seguro popular see org / publications / oecd - reviews - ofhealth - systems - mexico - 20169789264230491 - en.htm for more on the exploitation of seguro popular resources see com / 2018 / 10 / denuncias - pgrseguro - popular / for more on insabi see mx / 2019 / 11 / 14 / insabi / for more on this non - adhesion agreement see senado.gob.mx / 2020 / 06 / desconoce - gppan - al - insabi - y - asu - titular - por - falta - de - capacidady - reglas - de - operacion / and estados / gobernadores - del - panfirman - convenio - de - noadhesion - al - insabi for more on the referral of patients to governmentsanctioned centres see politica / incan - hospitales - juarezacogen - pacientes - cancer for more on breast cancer management in mexico see review lancet oncol 2012 ; 13 : e33543 cynthia villarreal - garza , alejandro aranda - gutierrez , ana s ferrigno , ana platas , isabelle aloi - timeus , fernanda mesa - chavez , adela ayensa - alonso , * alejandra platas perspectives comment published online august 15 , 2014 s1470 - 2045 ( 14 ) 70378 - x see articles page 1129 seto t , kiura k , nishio m , et al . 
ch5424802 ( ro5424802 ) for patients with alk - rearranged advanced non - small - cell lung cancer ( af - 001jp study ) : a single - arm , open - label , phase 12 study . 
safety and activity of alectinib against systemic disease and brain metastases in patients with crizotinib - resistant alk - rearranged non - small - cell lung cancer ( af - 002jg ) : results from the dosending portion of a phase 1 / 2 study . 
j clin oncol 2014 ; 32 : 141218 . ovarian tissue cryopreservation in children with cancer ovarian tissue cryopreservation is now a major part of the strategies used to preserve fertility in prepubertal children given gonadotoxic treatments for cancer . 
unlike post - pubertal patients , oocyte or embryo cryobanking is not appropriate for children and cryopreservation of ovarian tissue remains the only therapeutic option in most of the cases . 
restoration of ovarian function after reimplantation of frozenthawed mature ovarian cortex and reports of subsequent pregnancies were the basis of the rationale that guided the development of this approach in the treatment of childhood cancer . 
however , the success rate of the procedure in adult women is unknown , and the potency of cryopreserved immature gonads to restore fertility in adult survivors of childhood cancer has not yet been assessed . 
nevertheless , recent data suggest that immature ovaries are able to restore hormonal function in prepubertal children , in the same way that mature ovaries can in adults.1 , 2 additionally , immature ovaries have been used to restore fertility in experimental models.3 , 4 although the conditions of tissue harvesting , conditioning , and storing are well supervised by national biomedical and bioethical frameworks , patient selection criteria are mainly left to the discretion local multidisciplinary committees , resulting substantial heterogeneity of inclusion criteria , not only worldwide , but also within individual countries . 
 the authors retrospectively compared the occurrence of premature ovarian insu ciency over 15 years in a population - based study of children treated for cancer , who were or not o ered this procedure . 
they report that the cumulative probability of developing premature ovarian insu ciency after treatment was completed was signi cantly higher for patients o ered ovarian tissue cryopreservation than for those who were not o ered ovarian tissue cryopreservation ( 15 - year probability 35% [ 95% ci 1053 ] vs 1% [ 02 ] ; p < 00001 ; hazard ratio 568 [ 95% ci 625216 ] at 10 years ) , suggesting that the edinburgh selection criteria accurately predicted which patients would or would not develop premature ovarian insu ciency . 
although the small number of assessable patients who had successfully undergone ovarian cryopreservation ( 14 , compared with 141 assessable patients in the not - o ered group ) weakened the comparison , this is the rst report that aimed to assess selection criteria for ovarian cryopreservation in children with cancer . 
 the o er of ovarian tissue cryopreservation in the paediatric context is especially sensitive because the delay between the procedure and the potential use of the ovarian cortex could reach decades ( the median age at diagnosis for childhood cancer is about 51 years ) .6 parents are asked to plan for a future they cannot yet imagine , and , at the same time this request suggests the possibility of recovery , and so could be perceived as a message of hope . 
in this context , the selection criteria and follow - up protocol for paediatric ovarian tissue cryopreservation , as with any treatment protocol for children with cancer , should undergo evidence - based standardisation . 
in view of the small size of population of childhood cancer patients who could bene t from the procedure , national or international studies will be necessary to properly assess the validity of these selection criteria . 
because of the di erent sensitivity of gonads to toxic treatment at di erent ages , 7 and the report of spontaneous recovery of hormonal function after premature menopause as vol 15 september 2014 1049 comment published online august 15 , 2014 s1470 - 2045 ( 14 ) 70342 - 0 see articles page 1137 a result of treatment , 8 the de nition of high - risk for premature ovarian insu ciency and of premature ovarian insu ciency itself , as well as the modalities of follow - up , should be key points of discussion in a process of harmonisation . 
other means to preserve fertility , such as ovarian transposition in case of pelvic radiotherapy , 9 should also be assessed either as an alternative or as a combined approach . almost two decades have passed since the rst ovarian tissue cryopreservation was o ered to children submitted to gonadotoxic treatment . 
it should take into account the risk of reseeding cancer , which is particularly high in blood - borne cancers ( the most common types of cancer in childhood )  . 
generation of oocytes by in - vitro culture of primordial follicles to avoid this risk is an option , but such studies are still underway and clinically relevant data are not yet available.10 the indication for reimplantation is also still debated , and many authors , including wallace and colleagues , 5 recommend that the procedure be limited to fertility use only ( rejecting its use for induction of puberty , which can be done with synthetic hormonal substitution ) , because of the limited lifespan of the ovary linked to ischaemia - related follicle depletion . 
3 , 4 the nal step of a story that began many years ago for the adult survivor of childhood cancer will therefore be taken by adult specialists ( eg , assisted reproduction physicians and surgeons ) , who are not always familiar with childhood cancers . 
int j dev biol 2012 ; 56 : 90107 . dual targeting of her2 with lapatinib and trastuzumab drugs targeting her2 are central to the treatment of patients with her2 - positive breast cancer , and dual targeting of her2 with two drugs has gained much attention since 2010.1 patients with metastatic her2positive breast cancer have better overall survival when treated with docetaxel and the two anti - her2 monoclonal antibodies ( trastuzumab and pertuzumab , which bind to di erent extracellular domains of the her2 kinase ) , than do patients treated only with docetaxel and trastuzumab.2 dual targeting of her2 is also supported by neoadjuvant studies . 
in these trials , a greater proportion of patients who were treated with chemotherapy , trastuzumab , and lapatinib ( a her1 and her2 inhibitor ) , 35 or with chemotherapy , trastuzumab , and pertuzumab6 achieved pathological complete response than did those treated with chemotherapy plus trastuzumab alone . the phase 3 , three - group neoaltto trial7 is one of the key studies to assess dual targeting of her2 . 
 in neoaltto , investigators compared trastuzumab , lapatinib , and their combination as neoadjuvant and adjuvant treatment in a population of 455 patients with early her2 - positive breast cancer . 
the anti - her2directed therapies were rst administered alone for 1050 vol 15 september 2014 corrections published online june 12 , 2015 s1470 - 2045 ( 15 ) 00056 - x correction to lancet oncol 2015 ; 16 : e227 correction to lancet oncol 2015 ; 16 : 738 correction to lancet oncol 2015 ; 16 : 747 schiller jh . 
 antibodies lancet oncol 2015 ; 16 : 73839in this comment , the chemotherapy backbone used in the squire trial was incorrectly referred to as gemcitabine and carboplatin in four instances in the third paragraph ; it should read gemcitabine and cisplat these corrections have been made to the online version as of june 29 , 2015 , and the printed version is correct . torri v , broggini m , garassino mc . 
lancet oncol 2015 ; 16 : 74648the seventh sentence of the nal paragraph of this comment should read : results for leu858arg are still inconclusive because although progression - free survival is higher in patients given all egfr inhibitors versus chemotherapy , overall survival seems to be better with chemotherapy than with afatinib for these patients . 
 this correction has been made to the online version as of june 29 , 2015 , and the printed version is correct . for future lowy dr , herrero r , hildesheim a , for the participants in the iarc / nci workshop on primary endpoints for prophylactic hpv vaccine trial . 
 lancet oncol 2015 ; 16 : e22633 in the panel , in the section on the quadrivalent vaccine for men , the second bullet point should read : approved in the eu by the ema for the prevention of vaccine - type related anal lesions and for the prevention of vaccine - type related genital warts ( ages 9 )  . 
lancet oncol 2015 ; 16 : this news e316in item , the nal two sentences of paragraph 3 read : according to the scale , treatment late - stage egfr - mutated nonsquamous lung cancer with erlotinib provides a gain in progression - free survival ( pfs ) of 85 months ( hazard ratio [ hr ] 016 [ 95% ci 010026 ] ) and an improvement in quality of life compared with carboplatin and gemcitabine , earning an esmo - mcbs score of 4 / 5 . 
in contrast , the same drug when used to treat metas tatic pancreatic cancer provides an overall gain of only 9 days compared with chemotherapy treatment , and had a score of 1 / 5 . 
this correction has been made as of june 12 , 2015 . vol 16 july 2015 e313 correction to lancet oncol 2016 ; 17 : 74756 correction to lancet oncol 2018 ; 19 : 153042 correction to lancet oncol 2019 ; 20 : 81626 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
lancet oncol 2016 ; 17 : 74756in results , median overall survival should have been median time of death ( after randomisation ) in eleven patients who died from progressive disease . 
prognostic value of end - of - induction pet response after first - line immunochemotherapy for ( gallium ) : follicular secondary analysis of a randomised , phase 3 trial . 
 lancet oncol 2019 ; 20 : 81626 the appendix of this article has been updated as of may 10 , 2019 . published online april 29 , 2019 s1470 - 2045 ( 19 ) 30280 - 3 published online may 10 , 2019 s1470 - 2045 ( 19 ) 30292 - x published online may 10 , 2019 s1470 - 2045 ( 19 ) 30293 - 1 correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
this correction has been made to the online version as of may 29 , 2019 . correction to lancet oncol 2019 ; 20 : 82736 shitara k , iwata h , takahashi s , et al . 
lancet oncol 2019 ; 20 : 82736the appendix of this article has been updated as of may 10 , 2019 . correction to lancet oncol 2019 ; 20 : 84961 eng c , kim tw , bendell j , et al . 
 atezolizumab with or without cobimetinib versus regorafenib previously treated metastatic colorectal cancer ( imblaze370 ) : a multicentre , open - label , phase 3 , randomised , controlled trial . 
this correction has been made to the online version as of may 29 , 2019 and the printed article is correct . correction to lancet oncol 2019 ; 20 : e26273 ngiam ky , khor iw . 
lancet oncol 2019 ; 20 : e26273tables 1 and 2 in this article have been corrected as of april 29 , 2019 . correction to lancet oncol 2019 ; 20 : 297310 cella d , grnwald v , escudier b , et al . 
this update has been made online as of may 29 , 2019 . vol 20 june 2019 e293 corrections re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a manuscript to the lancet oncology visit thelancetoncology to submit a manuscript to the lancet neurology visit ees.elsevier.com / thelancetneurology 1 mosterd k , krekels gam , nieman fhm , et al . 
surgical excision versus mohs micrographic surgery for primary and recurrent basal - cell carcinoma of the face : a prospective randomised controlled trial with 5 - years follow - up . 
however , it is also explained by the fact that some patients were lost to follow - up after 30 months , and were therefore unable to visit our department at that time , but returned into follow - up when they visited our department after a longer period . 
there was no di erence in the method of follow - up between our rst and second publications . regarding the second question raised , we agree that perineural tumour invasion is an important risk factor . 
 finally , although the netherlands indeed an ethnically diverse country , the patients included in our study were people with fitzpatrick skin type i ( 11% ) , ii ( 44% ) , iii ( 35% ) , and iv ( 10% )  . 
 k mosterd * , n kelleners - smeets department of dermatology , maastricht university medical centre , po box 5800 , 6202 az , maastricht , netherlands k.mosterd@mumc.nl the authors declared no con icts of interest . neuro - oncology : a call for papers despite considerable research and the introduction of new therapies , long - term positive outcomes for patients with brain tumours are rare , and most patients experience a recurrence or progression of their cancer irrespective of the intervention . 
we are speci cally interested in the results of randomised controlled trials and other original clinical studies that will have a profound e ect on clinical practice , or on the fundamental understanding of tumour or cns biology , or on the management of neurological sequelae . accepted papers will be published in either the lancet oncology or the lancet neurology , and publication will coincide with the quadrennial meeting of the world federation of neuro - oncology and 6th meeting of the asian society for neuro - oncology ( wfno / asno ) , to be held in yokohama , japan , on may 1114 , 2009 . 
if your submission describes , in part or wholly , a study accepted for presentation at the wfno / asno meeting , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication can be scheduled to comply with wfno / asno embargo policies . 
 articles can be submitted via either the lancet oncologys or the lancet neurologys online submission services , but all authors must clearly state in the covering letter that their submission is in response to the tlo / tln call for papers . 
the closing date for this call for papers is march 13 , 2009 . david collingridge , helen frankish the lancet oncology ( dc ) , the lancet neurology ( hf ) , london nw1 7by , uk erratum kubota k , kawahara m , ogawara m , et al . 
vinorelbine plus gemcitabine followed by docetaxel versus carboplatin plus paclitaxel in patients with advanced non - small - cell lung cancer : a randomised , open - label , phase iii study . 
in this article , the hr for overall survival in table 2 should have read : 0996 ( 078127 )  . vol 10 january 2009 correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections comment published online october 28 , 2015 s1470 - 2045 ( 15 ) 00364 - 2 see articles page 1605 hypofractionation for prostate cancer and pros radiotherapy study in the non - inferiority chhip trial , 3216 patients underwent for intensity - modulated compared cancer . 
the localised prostate conventional fractionation at a dose of 74 gy in 37 fractions , previously assessed in the rt01 trial , 1 with two moderately hypofractionated schedules : 60 gy in 20 fractions and 57 gy in 19 fractions , with fractions of 3 gy per day . 
the quality - of - life ( qol ) substudy by anna wilkins and colleagues2 describes the patient - reported outcomes ( pros ) of 2100 patients , which were assessed with several qol instruments . 
the incidence of bowel and urinary symptoms were low and similar in the control and hypofractionated groups up to 24 months of follow - up , with no di erences with respect to timeto - event analysis of small or worse overall bowel , urinary , and sexual bother . intensity - modulated radiotherapy is a high - precision external beam radiotherapy approach that is regarded as the gold standard for the treatment of localised prostate cancer.3 intensity modulation has o ered the opportunity to launch phase 3 randomised trials to investigate whether overall treatment times can be reduced by increasing the dose per fraction , without increasing acute and late toxic e ects , and while maintaining quality of life for patients . 
prostate cancer has a low cell renewal rate ; 4 its low / ratio , about 14 , 5 describes the association between the delivered dose and the clinical response . 
 an interim analysis of the chhip trial6 that included 457 patients reported no di erence between treatment groups in the proportion of patients with grade 2 or higher gastrointestinal or bladder toxic e ects . 
the trial had a comprehensive methodology and radiotherapy quality assurance with appropriate dose constraints , and is the rst to report quality of life with pros in such a large population . 
the inclusion of high - risk prostate cancer is controversial because pelvic lymph node irradiation is needed for such strict cases , which might be harmful if delivered by hypofractionation because of the radiosensitivity of the small bowel . 
the dose used in the control group ( 74 gy ) would usually be regarded as an intermediate dose : a high dose would typically fall in the range of 7880 gy . 
high - risk prostate cancer requires a longer duration of androgen deprivation therapy compared with lower risk forms : 23 years rather than 36 months.7 as mentioned by the authors , 2 radiotherapy - related toxic e ects , particularly faecal incontinence , rectal bleeding , and use of urinary pads , were likely to be underestimated because of the use of di erent qol instruments . 
 in both the chhip and rt01 trials , the intensitymodulated schedules show signi cantly fewer adverse gastrointestinal events compared with the 74 gy schedules.8 other phase 3 randomised trials have investigated moderate hypofractionation for localised prostate cancer , but these were done with di erent techniques and sometimes had no comprehensive health - related qol assessments : a systematic review9 of these studies supports the safety of moderate hypofractionation but also emphasises the scarcity of data about long - term e cacy . 
in oncology , treatment choices are based on e cacy , toxic e ects , patient quality of life , and nally treatment costs ( once the other parameters have been met )  . 
before moderate hypofractionation can be recommended in daily practice for low - risk and intermediate - risk prostate cancer , 10 mature data from the chhip trial are needed ( showing the non - inferiority of hypofractionated regimens and 5 - year urinary , bowel , and sexual adverse event data ) , as are results from trials such as the radiation therapy oncology group 0415 trial and the profit trial from the ontario clinical oncology group . 
 intensity - modulated fractionated in the near future , the use of hypofractionation including whether face other challenges , will 1570 vol 16 december 2015 comment published online november 16 , 2015 s1470 - 2045 ( 15 ) 00457 - x see articles page 1617 can be combined moderate hypofractionation with brachytherapy , and the advent of extreme hypofractionation ( 510 gy in four to seven fractions )  . 
 such approaches will have to be managed within the framework of clinical research , with careful estimation of each patients comorbidities and their gastrointestinal and genitourinary function , as assessed with the international prostate symptom recordings . 
hypofractionated radiotherapy versus conventionally fractionated radiotherapy for patients with intermediate - risk localised prostate cancer assessed with patient - reported outcomes : 2 - year follow up of the randomised , non - inferiority , phase 3 chhip trial . 
jama 1998 ; 280 : 96974 . continued role for asct in multiple myeloma in the lancet oncology , francesca gay and colleagues report ndings of an international , multicentre randomised study in patients with newly diagnosed multiple myeloma.1 lenalidomide and dexamethasone were administered as induction treatment , followed by randomisation to either cyclophosphamide , lenalido mide , and dexamethasone or high - dose melphalan and autologous stem - cell transplantation ( asct ) as consolidation , and either lenalidomide and prednisone lenalidomide alone or as maintenance . 
this work builds on a previous study in which induction was followed by randomisation to either oral melphalan , lenalidomide , and prednisone or tandem high - dose melphalan and asct.2 in that report , better progression - free survival and overall survival were reported for asct compared with chemotherapy . 
 lenalidomide gay and colleagues reported that median progressionfree survival was signi cantly longer for melphalan cyclophosphamide , and asct compared with lenalido mide , and dexamethasone ( 433 months [ 95% ci 332522 ] vs 286 months [ 206367 ] ; hazard ratio [ hr ] for the rst 24 months 251 , 95% ci 160394 ; p < 00001 )  . 
4 - year overall survival was signi cantly better for melphalan and asct compared with cyclophosphamide , lenalidomide , and dexamethasone ( 86% [ 95% ci 7992 ] vs 73% [ 6582 ] ; hr 240 , 95% ci 132438 ; p = 0004 )  . 
of note , only 53 ( 43% ) of 124 patients assigned cyclophosphamide , lenalidomide , and dexamethasone received salvage asct after progressive disease , showing that salvage asct after relapse is not always feasible . 
in this personal view , we discuss why small , low - grade gleason pattern prostate lesions , which are currently designated as prostate cancer , could be regarded as non - malignant . 
these lesions either do not meet the criteria of the hallmarks of cancer or robust evidence that they do so is absent , by contrast with large lesions with a high gleason grade , which seem to cause most metastatic disease . introduction diagnosis and treatment of localised prostate cancer has been a much debated topic and as such is fraught with controversy . 
this situation has not been helpful for men who are at risk of prostate cancer or who have been diagnosed with the disease.1 the issues have been well described : over diagnosis , underdiagnosis , missed diagnosis , misclassi cation of risk , overtreatment , and under treatment . 
despite a general acceptance that these issues are both real and important , few recommendations have been suggested to help to mitigate them . one approach that merits some discussion is the reclassi cation of the generic term prostate cancer ( when applied to disease localised to the prostate ) into two subtypesone that can be safely ignored , or better , not diagnosed and another that , if left untreated , would compromise either quality or quantity of life . 
possible bene ts of not diagnosing a lesion that is unlikely to a ect a patients life include reduction of the anxiety of living with a cancer diagnosis and avoidance of potential radical surgery that might not be of clinical bene t and could cause substantial side - e ects . 
add itionally , esserman and colleagues3 have argued that minimal risk lesions should not be called cancer , with these lesions perhaps instead being called indolent lesions of epithelial origin ( idle )  . 
others have o ered similar opinions in the past year.4 , 5 not all prostate cancers are destined to progress the future behaviour of lesions that are identi ed early in the natural history of several cancers remains uncertasome will regress , others will remain stable , some will seem stable because of very long celldoubling times , and a few will progress . 
although lung cancer is one of the most lethal cancers in terms of the ratio of diagnoses to cancer - speci c deaths , one in six individuals who die of causes other than lung cancer will have apparently malignant lesions at autopsy ; these lesions are now termed pseudodisease in recognition of their non - malignant behaviour . 
had these lesions been diagnosed during life rather than at autopsy , treatment would have resulted , but with little bene t to the patient and some harms and costs.6 thyroid cancer is closer to prostate cancer in terms of the burden of subclinical disease . 
an familiar with pathologists are increasing recognition that progression , metastases , and death are rare events in small renal masses has led to similar discussion about whether such lesions should also be deemed pseudo disease.9 low - risk , noninvasive bladder lesions have also been successfully reclassi ed from bladder cancer to papillary urothelial neoplasia of low malignant potential.10 these we believe , as do many others , that it is time to apply the same reasoning to low - risk prostate cancer . 
 prostate cancer is generally multifocal and consists of a dominant focus ( as measured by tumour volume ) , deemed the index lesion , and one or more separate , secondary tumour foci of smaller volume ( gure 1 )  . 
 much laboratory and clinical evidence has shown that we need to rethink the nomenclature we apply to lowgrade and low - volume lesions.11 we believe that small , low - grade gleason pattern lesions , which are currently designated as prostate cancer , could be regarded as nonmalignant . 
using the framework provided by hanahan and weinberg , 12 we argue that these lesions either do not meet the criteria of the six hallmarks of cancer , or robust evidence that they do so is absent , by contrast with larger , high - grade lesions , which seem to cause most metastatic disease . vol 13 november 2012 e509 personal view insensitivity to antigrowth signals decreased expression cdkn1b increased methylation of cyclin d2 resisting apoptosis overexpression of bcl2 overexpression of dad1 index lesion low - grade , low - volume secondary lesions unlimited replicative potential decreased androgen signalling overexpression of erg sustained angiogenesis increased microvessel density increased expression of proangiogenic factors self - suciency in growth signals overexpression of egfr amplication of her2 / neu local tissue invasion and metastasis overexpression of cxcr4 monoclonal nature of invasion and metastases of lesions very low mortality in men with only low - risk lesions figure 1 : hallmarks of cancer as applied to the index and secondary lesions in prostate cancer the changing face of gleason grading in 1966 , donald gleason rst published his unique grading system for prostate cancer based solely on the architectural pattern of the tumour.13 he developed a 5 - point scale on the basis of the outcomes of 270 patients , in which patterns 1 , 2 , and 3 represented tumours that most closely resembled healthy prostatic glands , and patterns 4 and 5 represented tumours ( or parts of tumours ) that were increasingly anaplastic in appearance ( gure 2 , table ) .14 an innovative aspect of this system was that , rather than assigning the worst grade as the grade of the carcinoma , the sum of the two most common patterns is calculated and reported as the gleason sum score . 
since the gleason system was introduced , pathologists have adopted modi cations to the original grading system as described , to adapt it to modern needs ( table )  . redesignation of cancer to non - cancer within the gleason system is not new . 
gleason patterns 1 and 2 , originally described by gleason as changes consistent with malignant transformation , are now regarded as normal variants of the prostate architecture.15 the redesignation of gleason pattern 3 ( possibly quali ed by an upper threshold on volume ) could be the next incremental step on a 40 - year process of re nement of the gleason classi cation systefor example , there has been an accepted grading shift upwardsone element of the so - called will rogers phenomenon16with the changing de nition of gleason pattern 4 resulting in the regrouping of cases previously regarded as gleason score 6 into the gleason score 7 classi cation . 
in many cases of cancer in which the patterns would previously have been assigned to the lowest gleason pattern 1 , advances immunohistochemistry have shown the presence of basal cells , identifying such cases as atypical adenomatous hyperplasia , a benign mimic of cancer.17 moreover , lesions with patterns 1 and 2 have been recognised as biologically similar to pattern 3 , further discouraging their use ( table )  . hallmark one : self - su ciency in growth signals tumour cells can generate their own growth signals and reduce their dependence on stimulation from the surrounding normal tissue microenvironment . ross and colleagues18 used laser capture microdissection to extract cells from radical prostatectomy specimens from 23 men to create two subgroups , those with either exclusive gleason pattern 3 ( gleason score 6 ) or those with exclusive pattern 4 ( gleason score 8 )  . 
the investigators measured mrna expression of 18 344 unique genes in the extracted cells , and noted di erential expression of 670 of these genes between gleason pattern 3 and gleason pattern 4 lesions . 
overexpression of both of these genes is associated with independent cell proliferation and enhanced cell motility through several signal transduction mechanisms , including the mapk , akt , and ras pathways . 
as well as the upregulation of egfr , the investigators showed overexpression of map2k4 and the egf - activated promigratory gene rala , and downregulation of reps2 ( which negatively regulates egfr via endocytosis ) , phlpp , and pml ( both of which inactivate the protein kinase phospho - akt , which mediates growth - factor associated cell survival ) in gleason pattern 4 lesions . skacel and colleagues19 used a tissue microarray of more than 300 tissue cores derived from radical prostatectomy specimens to show that her2 / neu protooncogene ampli cation , as measured by uorescent in situ hybridisation , was associated with high tumour volume of greater than 20 cm ( p = 0004 )  . 
ampli cation of her2 / neu , a member of the egfr family , was almost exclusively con ned to gleason pattern 4 lesions rather than gleason pattern 3 lesions . hallmark two : insensitivity to antigrowth signals cancer cells must be able to resist the normal antigrowth signals that push them into a quiescent phase of the cell cycle or enter into postmitotic phases that ensure speci c cell di erentiation . e510 vol 13 november 2012 personal view score ( lesions that included gleason patterns 4 and 5 ) compared with those that were only pattern 3 . hallmark four : unlimited replicative potential mammalian cells seem to have an inherent autonomous function , independent of cell - to - cell signalling , that limits their replicative ability . 
we have some evidence that exclusive gleason pattern 3 prostate lesions have this brake preserved and that high - grade cancers are more likely to have evolved a mechanism to overcome it . 
they used radical prostatectomy specimens ( 101 micro dissected specimens from 44 individuals ) to develop two phenotype tissue poolsone low - risk ( exclusive gleason pattern 3 ) and one high - risk ( gleason pattern 4 or higher )  . 
the high gleason grade lesions showed decreased androgen signalling , similar to metastatic prostate cancer , which could re ect dedi erentiation and account for the clinical association of the grade of the high - grade lesions with prognosis . 
this nding was also reported by hendriksen and colleagues , 26 who noted lower androgen signalling in high - grade gleason pattern prostate cancer than in low - grade gleason pat tern lesions . 
the researchers suggested that localised prostate cancer cells become more aggressive by selectively downregulating androgen - responsive genes , which results in increased tumour cell replication and proliferation , dedi erentiation , or reduced apoptosis . another mechanism that is available to the cell to overcome the intrinsic brake on replication is gene translocation . 
the tmprss2erg translocation is one of the most prevalent genetic changes in prostate cancer , the presence of which results in overexpression of the erg transcription factor , and therefore promotes proliferation . 
this loss of cdkn1b was associated with an increase in the proliferative index of high - grade prostate cancers . hallmark three : resisting cell death the ability of cancer cells to resist programmed cell death ( apoptosis ) is key to ensuring continued growth and proliferation . true and colleagues23 used laser capture microdissection to acquire speci c subpopulations of prostate cancer cells consistent with lesions containing gleason patterns 3 , 4 , and 5 from 29 radical prostatectomy specimens . 
they pro led transcript abundance using cdna micro array analysis and developed an 86 - gene model capable of di erentiating between lesions that contain gleason pattern 3 and those that contain higher patterns ( 4 and 5 )  . 
one speci c discriminatory gene identi ed was dad1 , a gene encoding defender against cell death 1 , which is a downstream target of the nfb survival pathway and displays an antiapoptotic function . 
 dad1 protein concentrations showed a strong association with gleason grade , with tumours of patterns 4 and 5 more likely to stain intensely compared with gleason pattern 3 . tissue another more familiar antiapoptotic gene is bcl2 , the role of which in carcinogenesis and castrate resistance in prostate cancer is well established . 
 ( d ) gleason grade 4 ( increased stromal invasion ; white arrows show some areas of gland fusion and poorly de ned lumens ; green arrow shows one of a few areas in which gleason pattern 3 is present ; original magni cation 40 )  . 
 since tmprss2erg fusions lead to frequent changes in the erg proto - oncogene in early - stage prostate cancer , investigation of this fusion in preneoplastic cells and multifocal lesions from the same patient has the potential to de ne its role in prostate cancer onset , progression , and heterogeneity . 
in a cross - sectional study27 in which individual cancers from radical prostatectomy specimens with two to three tumour foci of various sizes and grades were analysed , the researchers established that erg protein expression is signi cantly increased in tumours with large volumes and high gleason grade , presumably as a result of this transcription factor promoting tumour growth and proliferation . however , other evidence emphasises the uncertainty about the role of this particular gene fusion in prostate cancer development and progression . 
others29 have shown a strong relation between expression of tmprss2erg fusion mrna isoforms and pathological measures of clinical outcome ( seminal vesicle invasion , extracapsular exten sion ) in lesions from radical prostatectomy specimens . 
the same researchers also reported expression of the gene fusion in benign glands of the prostate . hallmark ve : sustained angiogenesis neoangiogenesis is a normal physiological process that takes place during embryonic development and wound healing . 
the process is also necessary for tumours to break through the volume threshold of 1 mm diameter , since tumours larger than this cannot rely on the di usion of oxygen from existing vessels . angiogenesis is probably necessary to support accelerated tumour growth , since the metabolic needs of the tumour must be met by an adequate blood supply.30 prostate cancer cells have the ability to produce several factors that promote new vessel formation . 
so the question arises , does this forced vascular proliferation occur preferentially in high - grade lesions or is it a transformation that is permissive for proliferation and dedi erentiation of prostate cancer cells ? raised vegf and increased microvessel density are related to a poor prognosis in prostate cancer , 31 and a close association exists between the two . 
moreover , this association seems to be more pronounced in high - grade and large tumours than in low - grade and small tumours.32 in a well designed study , mucci and col leagues33 established that poorly di erentiated tumours showed increased microvessel density and irregularity of the blood vessel lumen with reduced vessel size . 
men with tumours that had the smallest vessel diameter at inclusion were six times more likely ( 95% ci 18200 ) to develop metastatic prostate cancer or to die from the disease . 
 additionally , another subgroup was identi ed that had even greater propensity for clinical progression ; men who had irregularity of vessel diameter were 17 times more likely ( 95% ci 23128 ) to reach the same two endpoints . 
microvessel density itself was not linked to cancer - speci c mortality after results were adjusted for clinical factors.33 in higher - grade other factors are either required or facilitate new vessel formation . 
pericyte distribution was mapped from e512 vol 13 november 2012 personal view - smooth - muscle - actin - positive immune - stained histological sections and quanti ed by image analysis . 
 exclusive gleason pattern 3 lesions had a microvessel pericyte density score that could not be distinguished from benign prostate tissue , by contrast with the scores of higher - grade lesions . hallmark six : tissue invasion and metastasis the potential for invasion into adjacent anatomical structures and spread to distant sites are key attributes of cancer cells . 
for example , when individual prostate lesions derived from one patients primary prostate cancer specimen were implanted into mice , only one lesion out of three showed characteristics of local invasion and eventually formed metastases.36 this work reminds us that as well as histological heterogeneity within any one prostate lesion there are , within the cancer , distinct elements with a range of biological potentials . 
this g - protein - coupled transmembrane receptor has a key role in the directional migration of cancer cells to speci c metastatic sites in response to its ligand cxcl12 . 
additionally , cxcr4 upregulation has been associated with lymph node and bone metastasis in prostate cancer , possibly through activation of the ras oncogene family member rap1a , the expression of which is also upregulated in gleason pattern 4 lesions relative to those containing only gleason pattern 3 . 
 investigators of other studies have suggested that hypoxia induces cxcr4 expression in tumour cells via hypoxiainducible factor 1.37 , 38 large volume tumours are much more likely to have central hypoxic areas than are small volume tumours . 
expres sion of cxcr4 on the tumour cell membrane allows the cancer cells to migrate or metastasise away from the area of low oxygen tension , down a cxcl12 concentration gradient , to areas of high oxygen concentration . 
the ligand cxcl12 is secreted at especially high concen trations by lymph node and bone marrow stromal cells . most men have two to three distinct tumour foci in their prostate at presentation . 
other researchers40 have noted that 80% of secondary foci are smaller than 05 cm and have the same volume distribution as do tumours found incidentally in patients that undergo cystoprostatectomy for bladder cancer . 
tumour volume has been proposed to be associated with prostate - speci c antigen ( psa ) recur rence41 and prostate lesions smaller than 05 cm are almost always clinically insigni cant because of the long doubling times of such lesions.42 several authors43 , 44 have proposed that the threshold for signi cance of volume be placed higher , at 12 cm , on the basis of data from the european large - scale ran domised prostate cancer screening trial , in which volume thresholds of insigni cant disease were calculated on the basis of models of lifetime risk estimates of prostate cancer diagnosis in screened and non - screened participants . 
however , after accounting for tumour stage and grade , the threshold volumes for the index tumour and total tumour were 13 cm and 25 cm , respectively.43 , 44 a strong association also seems to exist between pathological and staging measures of poor prognosis ( extracapsular invasion , seminal vesicle invasion , metastases ) and individual cancer lesion volumes . 
lesions measuring 05 cm or more had a one in ten chance of capsular invasion , whereas lesions measuring 40 cm or more had a one in ten chance of seminal vesicle invasion . 
lesions measuring 50 cm or more had a one in ten chance of metastases.45 volume is an important determinant of grade ( or vice versa ) ; gleason pattern 4 or higher is very rare in lesions that are not attributed index status.46 if the volume of a lesion is a key attribute of progression , as it seems to be , 47 then multiplicity for any given overall tumour volume within a prostate should be a good prognostic sign . 
in other words , if 2 cm of tumour is distributed fairly equally among ve separate lesions , the mean lesion volume will be less than 05 c if , on the other hand , the cancer was unifocal ( seen in about one in ve men who present with prostate cancer ) , then the mean tumour volume will equate to the overall tumour volumeie , 2 cthe primacy of the index lesion as a determinant of progression seems to hold . the next question in relation to the volume of speci c prostate cancer foci is about the biological potential of these small lesions . 
schmid and colleagues48 have reported that 79% of men with vol 13 november 2012 e513 personal view previously untreated prostate cancer of all clinical stages , who had serial psa measurements during a period of at least 12 months , had a tumour doubling time greater than 24 months . 
primary tumour volumes that theoretically lead to distant metastases tend to be at least 4 cm in volume.49 as such , with an estimated tumour volume doubling time of 2 years , it would take about 6 years for a 05 cm lesion to reach a volume of 4 cm . although overwhelming evidence suggests that small tumours are very safe from a biological perspective , there remain some anomalies that remind us that our understanding is far from complete . 
up to one in four tumours that show capsular invasion can be identi ed as non - index lesions , 50 and although tumours that are locally invasive do need to achieve some volume threshold , they do not necessarily have to be very large.51 in fact , circulating tumour cells and occasionally lymph - node metastases have been reported in men who have lesions of 02 cm in volume.52 in a series of 239 patients with tumour volumes of less than 05 cm , investigators showed that 43 were poorly di erentiated , 11 had extracapsular extension , six had positive surgical margins , two had positive lymph nodes , and seven progressed within 5 years.53 greene and coworkers54 assessed dna ploidy status , which is an independent prognostic factor for localised prostate cancer . 
thus , tumour volume in itself did not adequately predict the biological potential of prostate cancer and so should be combined with other factors , predominantly gleason grade . the molecular association of individual lesions with lymph node metastases has added more force to the argument that , despite multifocality , prostate cancer disease progression is likely to be related to lesions that meet some minimum grade and volume thresholds . 
 tmprsserg gene fusions seen in lymph node metastases are also found in the index lesion and not in small , low - grade satellite lesions55 or secondary highlesions.56 results of one grade and high - volume important study57 showed that metastatic deposits taken from men in a rapid autopsy protocol shared one common cell of orighowever , the question of whether the metastatic clone originated from the index lesion is something that was not possible to address in this study because of the nature of the men from whom the tissue samples were taken ( ie , they had been through rst - line and second - line hormonal therapies in addition to chemotherapy in some instances , so the prostates were small and brotic , which made the delineation of individual lesions impossible ) .58 grasso and colleagues59 also noted the monoclonal origin of lethal , castrateresistant prostate cancer by sequencing the exomes of metastatic deposits in 50 lethal , heavily pretreated metastatic cancers obtained at autopsy . epidemiological evidence also supports the assertion that most prostate lesions , especially those of low volume and low gleason grade , currently called cancer , do not show tissue invasion and eventual metastases . 
similar frequencies are seen on assessment of prostates taken from cystoprostatectomy specimens from men who have undergone surgery for high - risk or invasive bladder cancer.40 therefore , since a third of men have prostate cancer that will not a ect them in their lifetimes , it is unsurprising that small , low - grade lesions have low ( or possibly absent ) malignant potential . this argument is lent support by ndings from longterm radical prostatectomy outcome series . 
for example , eggener and coworkers60 showed that , of 9775 men who had gleason 3 pattern in isolation con rmed on radical whole - mount prostatectomy specimens , only three died of prostate cancer in a 15 year period . 
in fact , when these three patients were reviewed , a small amount of gleason pattern 4 was seen.1 this nding cannot merely be accounted for by the success of surgery itself and is strong evidence that exclusive gleason pattern 3 lesions are not a metastatic phenotype . 
 prostate others61 , 62 have reported similar ndings in smaller cohorts of patients , but using biochemical recurrence as a surrogate out come measure . the scienti c literature about the advantages and disadvantages of active surveillance also helps the understanding of whether low - volume , low - grade disease behaves in a malignant way . 
warlick and colleagues63 investigated whether curability after surgery , which they de ned as surgical pathological characteristics that would generally confer a greater than 75% chance of remaining biochemically recurrence - free at 10 years , was a ected if treatment was delayed.64 in other words , is the window of opportunity for curesomething that con cerns patients and physicians alike when considering active surveillancelost in men with small , low - grade disease who have delayed curative treatment ? after comparing the burden of supposedly incurable cancer among patients undergoing delayed surgery at a median time of 265 months after diagnosis with that in patients undergoing immediate surgery ( who would have been eligible for active surveillance ) the investigators reported no association between adverse pathological changes on whole - mount specimens and the time period between diagnosis and surgery . 
clinical experience with active surveillance suggests that an estimated risk of metastasis exists of less than 1% at 28 years64 and disease - speci c mortality of 1% at 8 years in men undergoing surveillance for low - risk disease as classi ed by a diagnostic transrectal ultrasound - guided biopsy . 
early outcomes in men with intermediate - risk disease managed by active surveillance have also been encouraging.65 results of research that has assessed active surveillance have shown that all prostate cancer - related mortality occurred e514 vol 13 november 2012 personal view in men who had been reclassi ed as higher risk and who were o ered radical treatment . 
in other words , when compared with a more rigorous sampling strategy , transrectal ultrasound - guided biopsy undergrades and understages disease as a result of random and systematic errors in sampling the prostate.66 clinical implications when prostate cancer is identi ed from biopsies , the psychological connotations associated with having cancer mean that many men choose or are advised to undergo radical treatment that they stand little chance of bene ting from.67 most clinicians advising patients know that exclusive gleason pattern 3 carries very little lifetime risk to the patient , but many still recommend radical treatments that carry high toxicity pro les . 
the absence of precision means that the attribution of low risk is insecure in about one in three men who are deemed to be at low risk ( exclusive gleason pattern 3 disease ) , but in fact are not . 
if we could accurately identify men with gleason pattern 3 lesions in isolation , these men would be very likely to be at much lower ( possibly negligible ) risk of death from prostate cancer than men previously attributed a gleason pattern 3 diagnosis of cancer . 
if this situation came to pass , we might be in a position to reclassify exclusive gleason pattern 3 lesions to a term that substitutes the word cancer for something else , such as idle.3 such a term would seem to be appropriate ; if low - volume , lowgrade lesions were reclassi ed as non - cancer or idle lesions and this change met with widespread professional acceptance , the immediate implications for clinical practice would be profound . first , research into novel detection strategies and therapies is likely to need substantial rethinking . 
in fact , hundreds of millions of pounds have been spent on the discovery of an elusive biomarker during the past two to three decades , on the premise that the outcomes from the transrectal ultrasound - guided biopsy are the gold standard . 
a third of all men diagnosed with prostate cancer are estimated to have clinically insigni cant disease.64 , 68 , 69 furthermore , transrectal prostate biopsies can miss a clinically signi cant cancer that is likely to progress and metastasise within a mans lifetime ( which incorrectly designates the patient a true negative )  . 
40% of men who test negative on biopsy are estimated to have cancer ; 68 , 70 of these , a third have clinically signi cant cancer based on lesion volume and presence of high grade.69 second , a recalibration of what is deemed cancer is likely to substantially reduce the overdiagnosis and overtreatment burdens with which we are all familiar . 
the performance characteristics of multiparametric mri , for example , coupled with an intensive sampling strategy , in being able to rule out 05 cm lesions with a negative predictive value of about 9095% , is arguably an ideal test.71 a large multicentre study is in progress that is assessing the reproducibility of such imaging in men at risk before any biopsy , against a reference standard that can be applied in all men and not only those who undergo surgery ( nct01292291 )  . 
the key with imaging is that it could provide an accurate volume with indicators of high gleason grade before biopsy and act as a triage test to identify men who need biopsies , which would allow men with no clinically signi cant cancer to avoid entering the diagnostic pathway altogether.72 third , when compared with other solid organ malignancies , prostate cancer is an outlier . 
treatments for breast , renal , thyroid , liver , and pancreatic cancers all include tissue - preserving therapies , if appropriate , which are dependent on location and burden of the cancer . 
 these specialties in oncological surgery de veloped tissue preservation , as opposed to halsted prin ciples for wide surgical margins , because of upstream diagnostic methods that rely on identifying measurable ( by palpation or imaging ) disease that can undergo targeted sampling followed by targeted treatment . 
random and blind sampling has forced our hands as clinicians , so that we have to apply radical whole - gland principles because the exact disease statuses of regions of the prostate are search strategy and selection criteria we searched pubmed and medline for relevant publications from the past 10 years ( jan 1 , 2002 to april 16 , 2012 ) , and supplemented the results of our search with key articles from before this period when appropriate . 
so , if multifocality is overlooked in other organs by targeting only the measurable index lesion that which is largest by size and has elements of the highest gradethat targeting these lesions in prostate cancer might be su cient to lead to acceptable , possibly equivalent , cancer control rates to whole - gland therapy is a reasonable hypothesis . 
focal therapy certainly leads to reduced genitourinary and rectal sidee ects , if the results of early prospective studies are reproducible and surgeons.7375 however , the key will be to design longitudinal cohort and comparative e ectiveness studies that assess medium - term and long - term cancer control . 
such research will need to focus on the natural history of untreated benign and low - volume , low - grade prostate lesions . populations , centres , across contributors hua conceived the personal view , and ma and hua did the database searches and identi ed relevant articles . 
all authors redrafted the report through several iterations and approved the nal submitted version . con icts of interest me and hua received funding from ushifu , glaxosmithkline , and advanced medical diagnostics for clinical trials . 
none of these funding sources had any input or role in the production of the report . acknowledgments me and hua acknowledge funding from the medical research council ( uk ) , pelican cancer foundation , prostate action , st peters trust , wellcome trust , national institute for health research health technology assessment programme ( uk ) , the us national institutes of healthnational cancer institute , and the prostate cancer research centre . 
me receives funding in part from the uk national institute for health research university college london hospitals / university college london comprehensive biomedical research centre . reflection & reaction energy agency study . 
policy analysis of cervical cancer screening strategies in low - resource settings : clinical benefits and cost - effectiveness . jama 2001 ; 285 : 310715 . 5 hartley p , daubenton jd . 
estimates of lung - cancer incidence in europe , 2000 women country crude rate asr cumulative risk * no of cases crude rate asr cumulative risk * no of cases eastern europe 872 877 belarus 742 bulgaria 984 czech republic 1361 hungary 490 moldova 943 poland romania 671 russian federation 880 800 slovakia 823 ukraine northern europe denmark estonia finland iceland ireland latvia lithuania norway sweden united kingdom 735 764 923 572 405 509 824 735 557 393 821 southern europe 959 albania 650 bosnia herzegovina 937 croatia greece italy macedonia malta portugal slovenia spain yugoslavia 1241 1006 1077 558 601 521 906 868 1105 western europe austria belgium france germany luxembourg netherlands switzerland 839 605 1257 796 834 904 927 739 697 710 489 689 955 471 782 507 749 685 615 443 468 699 368 315 395 615 577 351 214 476 588 792 812 825 558 594 469 445 339 644 532 809 532 421 764 535 502 605 620 485 * cumulative risks are for ages 064 years . 
only reproduce with permission from the lancet . correction to lancet oncol 2020 ; 21 : 26170 correction to lancet oncol 2020 ; 21 : 80820 correction to lancet oncol 2020 ; 21 : 92334 blay j - y , serrano c , heinrich mc , et al . 
quality of life in patients with cervical cancer after open versus minimally invasive radical hysterectomy ( lacc ) : a secondary outcome of a multicentre , randomised , open - label , phase 3 , noninferiority trial . 
this long - awaited once in a generation opportunity to put ncds on the global agenda generated as many fears of a missed opportunity as it did hopes of a turning point for the health of millions around the world . 
the unanimous agreement by un member states to hold the summit on ncds signalled recognition of a growing global emergency and , at long last , a willingness to act . 
although often thought of as diseases of rich countries , ncds now disproportionately a ect more people in poorer nations , accounting for 80% of all ncd - related deaths . 
ncds include cancers , cardiovascular diseases , diabetes , and chronic respiratory diseases : all are largely preventable and share common risk factors , such as tobacco use , unhealthy diet , physical inactivity , and harmful use of alcohol . 
furthermore , the world economic forum identi ed ncds as a severe threat to economic development and put a price tag of $30 trillion on the expected burden of these diseases over the next 20 years . 
 the aim of the meeting was to secure commitment from heads of government for a coordinated global response , to raise awareness among the general public , and to adopt a comprehensive political declaration for health strategies . 
notably , governments decided to commit to multisectoral national and international policies to control ncds , to reduce individual exposure to ncd risk factors through international agreements such as the who framework convention on tobacco control , the who global strategy on diet , physical activity and health , and the who global strategy to reduce the harmful use of alcohol , to give greater priority to early detection , screening and diagnosis , to increase access to vaccines as part of national immunisation programmes , and to improve access to palliative care . 
 industry these commitments should be applauded as a good start in tackling the serious burden that ncds represent , and signal the start of attempts to reverse the undue long - term neglect the political arena has a orded such issues . 
 indeed , although the fundamental con ict of interest between the tobacco industry and public health is fully recognised in the declar ation , other groups from the food and drink industrywhich the un euphemistically refers to as civil society alongside organisations such as academiawere invited to participate in the meeting , although they were excluded from any decision - making . 
 in preparation for the meeting , the uiccas part of the ncd allianceproposed very speci c targets that could have been included , such as a commitment by 2025 to reduce avoidable deaths from ncds by 25%a target who believes is achievable . 
instead , the document calls on who simply to set up a comprehensive global monitoring framework and prepare recommendations for voluntarynot compulsoryglobal targets before the end of 2012 , and to report initial progress in 2013 . 
 the lancet oncology vol 12 october 2011 editorial published online september 18 , 2012 s1470 - 2045 ( 12 ) 70422 - 9 for more on mortality and cancer incidence in 9 / 11 survivors and emergency services personnel see articles lancet 2011 ; 378 : 87987 , and articles lancet 2011 ; 378 : 898905 9 / 11 survivors to get free cancer treatment the us national institute for occupational safety and health ( niosh ) announced on sept 11 , 2012 , that emergency services workers and other survivors from the terrorist attacks on the twin towers of the world trade center in new york , ny , usa , will now be eligible for free cancer treatment in addition to the compensation announced previously for other diseases . the world trade center health program was established by the james zadroga 9 / 11 health and compensation act of 2010 , and signed in to law by president barack obama in january , 2011 . 
the law , named after a new york police o cer who died of a respiratory disease attributed to working among the devastation , provides us$42 billion of health - care coverage . 
survivors of the attacks on the pentagon and at the crash site in shanksville , pa , usa , will become eligible for the programme later this year . compensation for cancer treatment was held - up by a dispute over whether cancer could be caused by the atrocities . 
although this early conclusion was misguided in view of the well - established links between smoke , particulates , occupational risk , and cancer , such uncertainty was understandable on the basis of the equivocal nature of the emerging 9 / 11 data . 
 a study of mortality in survivors published in the lancet in 2011 , showed no excess ; in fact , it showed a de cit of mortality possibly attributable to the higher levels of tness among emergency workers . 
in a second article , also in the lancet in 2011 , rachel zeig - owens and colleagues looked speci cally at early cancer occurrence , and these data were again di cult to interpret . 
the standardised incident rate ( sir ) ratio for all cancers combined was 121 for re ghters deployed to the world trade center between sept 11 , 2001 , and july 25 , 2002 , indicating the possibility of an occupational hazard and higher than expected number of cancers , but the con dence intervals did not reach signi cance , and for individual malignancies ( eg , lung cancer ) there was no signi cant di erence , suggesting it was too soon to detect cancers associated with exposure to toxins . 
 long - term continued monitoring and research will be essential to establish the full extent of any associations . the analytical methods used in the cancer outcomes study also contributed to the confounding in the conclusions . 
however , for re ghters , an occupational health risk is already wellestablished , plus the nature of the job involves shift work and tends to attract tter and healthier people than in the normal population , which in turn modi es the risk of disease . 
thus , comparing cancer incidence in re ghters with that in the general population does not answer the very speci c question of whether deployment to the twin towers in the aftermath of the terrorist attacks added additional risk to their already underlying occupational risk . 
to answer this question , the denominator in the sir calculation needed to be the expected number of cancers among re ghters in major metropolitan cities in the usa . the slaughter of innocent people in the terrorist attacks in new york in 2001 has undeniably had a direct and profound e ect on the lives of many people : families , rst responders , volunteers , survivors , and manhattan residents . 
irrespective of the scienti c debate surrounding the robustness of the data linking cancer incidence to the world trade center devastation , su cient evidence exists from other settings to conclude that exposure to harmful chemicals and inhalation of noxious fumes and particles is not healthy , and on the precautionary principle alone , it is only right that all people directly a ected by 9 / 11 should be a orded free health care . 
to quote john feal , a campaigner for the treatment of 9 / 11 survivors : we dont need a phd to tell us that 9 / 11 and its aftermath cause cancer . 
 it is often said , the rst role of any government is to protect the safety of its peopleproviding free health care is a just and compassionate response irrespective of the data thus far . 
is sidedness prognostically important across all stages of colorectal cancer ? lancet oncol 2016 ; 17 : 148082the first sentence of the last paragraph should have read , embryologically we know that the right colon is derived from the midgut , whereas the left side of the colon and rectum develop from the hindgut , and there are genomic di erences between these tissues that might underlie the observed divergence in outcome . 
this correction has been made to the online version as of nov 29 , 2016 . vol 17 december 2016 e519 published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
 n a d o f a r a g e n e k u l k a r n i firadenovec : a new gold standard for bcg - unresponsive bladder cancer ? lancet oncol 2021 ; 22 : 89in this comment , the declaration of interests statement was incorrect and should have read as follows : i report personal fees from merck , ferring , biosyent , tersera , abbvie , roche , theralase , and janssen , outside the submitted work . 
 this correction has been made to the online version as of dec 30 , 2020 , and the printed version is correct . maringe c , spicer j , morris m , et al . 
 the impact of the covid - 19 pandemic on cancer deaths due to delays in diagnosis in england , uk : a national , population - based , modelling study . 
lancet oncol 2020 ; 21 : 154950in this comment , on the second and eleventh lines of paragraph two , the drug name has been corrected to gx - 188e . 
durvalumab alone and durvalumab plus tremelimumab versus chemotherapy in previously untreated locally patients with unresectable , advanced or metastatic urothelial carcinoma ( danube ) : a randomised , open - label , multicentre , phase 3 trial . 
 lancet oncol 2020 ; 21 : 157488 in this article , the affiliation for ignacio duran should have been hospital universitario virgen del roco , seville , spathis correction has been made to the online version as of dec 30 , 2020 . correction to lancet oncol 2020 ; 21 : 160210 pm , welt ens poortmans fortpied c , et al . 
internal mammary and medial supraclavicular lymph node chain irradiation in stage iiii breast cancer ( eortc 22922 / 10925 ) : 15 - year results of a randomised , phase 3 trial . 
 lancet oncol 2020 ; 21 : 160210 in this article , the funders of the study should have been ligue nationale contre le cancer and kwf kankerbestrijding in the funding and acknowledgments sections . 
this correction has been made to the online version as of dec 30 , 20202 . vol 22 january 2021 corrections systemic chemotherapy with or without cetuximab in patients with resectable colorectal liver metastasis ( new epoc ) : long - term results of a multicentre , randomised , controlled , phase 3 trial john a bridgewater , sin a pugh , tom maishman , zina eminton , jane mellor , amy whitehead , louise stanton , michael radford , andrea corkhill , gareth o griffiths , stephen falk , juan w valle , derek oreilly , ajith k siriwardena , joanne hornbuckle , myrddin rees , timothy j iveson , tamas hickish , o james garden , david cunningham , timothy s maughan , john n primrose ; on behalf of the new epoc investigators * summary background the interim analysis of the multicentre new epoc trial in patients with resectable colorectal liver metastasis showed a significant reduction in progression - free survival in patients allocated to cetuximab plus chemotherapy compared with those given chemotherapy alone . 
the focus of the present analysis was to assess the effect on overall survival . methods new epoc was a multicentre , open - label , randomised , controlled , phase 3 trial . 
adult patients ( aged 18 years ) with kras wild - type ( codons 12 , 13 , and 61 ) resectable or suboptimally resectable colorectal liver metastases and a who performance status of 02 were randomly assigned ( 1 : 1 ) to receive chemotherapy with or without cetuximab before and after liver resection . 
randomisation was done centrally with minimisation factors of surgical centre , poor prognosis cancer , and previous adjuvant treatment with oxaliplat chemotherapy consisted of oxaliplatin 85 mg / m administered intravenously over 2 h , l - folinic acid ( 175 mg flat dose administered intravenously over 2 h ) or d , l - folinic acid ( 350 mg flat dose administered intravenously over 2 h ) , and fluorouracil bolus 400 mg / m administered intravenously over 5 min , followed by a 46 h infusion of fluorouracil 2400 mg / m repeated every 2 weeks ( regimen one ) , or oxaliplatin 130 mg / m administered intravenously over 2 h and oral capecitabine 1000 mg / m twice daily on days 114 repeated every 3 weeks ( regimen two )  . 
cetuximab was given intravenously , 500 mg / m every 2 weeks with regimen one and three or a loading dose of 400 mg / m followed by a weekly infusion of 250 mg / m with regimen two . 
this trial is registered with isrctn , number 22944367 . findings between feb 26 , 2007 , and oct 12 , 2012 , 257 eligible patients were randomly assigned to chemotherapy with cetuximab ( n = 129 ) or without cetuximab ( n = 128 )  . 
this analysis was carried out 5 years after the last patient was recruited , as defined in the protocol , at a median follow - up of 667 months ( iqr 580775 )  . 
median progression - free survival was 222 months ( 95% ci 183268 ) in the chemotherapy alone group and 155 months ( 138190 ) in the chemotherapy plus cetuximab group ( hazard ratio [ hr ] 117 , 95% ci 087156 ; p = 0304 )  . 
 median overall survival was 810 months ( 596 to not reached ) in the chemotherapy alone group and 554 months ( 435715 ) in the chemotherapy plus cetuximab group ( hr 145 , 102205 ; p = 0036 )  . 
the most common grade 34 adverse events reported were : neutrophil count decreased ( 26 [ 19% ] of 134 in the chemotherapy alone group vs 21 [ 15% ] of 137 in the chemotherapy plus cetuximab group ) , diarrhoea ( 13 [ 10% ] vs 14 [ 10% ] ) , skin rash ( one [ 1% ] vs 22 [ 16% ] ) , thromboembolic events ( ten [ 7% ] vs 11 [ 8% ] ) , lethargy ( ten [ 7% ] vs nine [ 7% ] ) , oral mucositis ( three [ 2% ] vs 14 [ 10% ] ) , vomiting ( seven [ 5% ] vs seven [ 5% ] ) , peripheral neuropathy ( eight [ 6% ] vs five [ 4% ] ) , and pain ( six [ 4% ] vs six [ 4% ] )  . interpretation although the addition of cetuximab to chemotherapy improves the overall survival in some studies in patients with advanced , inoperable metastatic disease , its use in the perioperative setting in patients with operable disease confers a significant disadvantage in terms of overall survival . 
substantial improvements in its management , with increasingly sophisticated combinations of systemic therapy and surgery , together with earlier diagnosis , have resulted in more than a doubling of the 5 - year survival from 25% to 50% in the past 50 years . 
in the setting of metastatic disease , outcomes are improving and , after liver resection , approximately 30% of patients will be long - term survivors.1 unfortunately , the majority of patients will have disease recurrence . the epoc study ( eortc 40983 ) showed an improvement in progression - free survival of 7% with the addition of perioperative systemic chemotherapy to surgical resection for colorectal liver metastasis.2 as a consequence , this treatment has become standard of care in most uk centres.3 the new epoc study was a logical progression from the epoc study , assessing the benefit of adding cetuximab , an antibody to egfr with confirmed efficacy in advanced disease , 4 to peri operative systemic chemo therapy . 
unexpectedly , this addition resulted in a shorter progression - free survival in the patients treated with cetuximab , and the study was closed to recruitment by the trial steering committee on advice from the independent data monitoring committee on nov 1 , 2012 . 
 the previously published results of the interim analysis showed the progression - free survival in the chemotherapy alone group to be 205 months ( 168267 ) , compared with 141 months ( 95% ci 118159 ) in the chemotherapy plus cetuximab group , with a hazard ratio ( hr ) of 148 ( 104212 ; p = 0030 ) , 5 at a median follow - up of 21 months . since the new epoc trial began accrual ( feb 26 , 2007 ) , several studies have evaluated the use of antibodies to egfr in advanced colorectal cancer . 
some studies found improved outcomes , 6 , 7 whereas others showed no difference.8 , 9 importantly , none have shown a detriment similar to the previously published new epoc study . 
 the present analysis was done after long - term follow - up of patients using a more complete dataset , not available at the time of the interim analysis , to assess the effect of the combination treatment on overall survival . methods study design and participants this multicentre , open - label , randomised , controlled , phase 3 study was coordinated by the cancer research uk southampton clinical trials unit . 
all patients were recruited from 39 uk national health service hospitals ( appendix pp 3 , 4 ) , in secondary care settings . eligible patients were aged 18 years or older , with a who performance status of 2 or lower , and resectable or suboptimally resectable colorectal liver metastasis without detectable extrahepatic distant metastatic disease . 
 patients were excluded if they had any uncontrolled medical comorbidity likely to interfere with treatment or research in context evidence before this study before designing the new epoc trial , pubmed , american society of clinical oncology abstracts , and european society of medical oncology abstracts were searched for articles published in english using the search terms colorectal cancer , colorectal liver metastases , chemotherapy , epidermal growth factor receptor , cetuximab , and panitumumab . 
 no meta - analysis was carried out , as in 2006 only one adequately powered trial of perioperative chemotherapy had been done . survival outcomes of chemotherapy for advanced colorectal cancer have improved during the past two decades , in part because of improvements in systemic therapies , including targeted therapies such as cetuximab , an antibody to egfr . 
 some , but not all , studies of chemotherapy plus cetuximab have shown the combination to improve the overall survival of patients with advanced inoperable kras wild - type colorectal cancer . 
at that time , overall survival data were immature . added value of this study this mature analysis shows that in the perioperative setting , cetuximab shortens overall survival by 2 years compared with chemotherapy alone . 
 toxicity from systemic therapy and complications of surgery could not explain these findings . implications of all the available evidence this study suggests that the addition of cetuximab to chemotherapy in the perioperative setting in patients with operable colorectal liver metastases induces , in some individuals , multisite metastatic recurrence and a shorter overall survival than does chemotherapy alone . 
cetuximab should not be used in patients with operable colorectal liver metastases . vol 21 march 2020 articles assessment of response ; any psychiatric or neurological disorder affecting ability to consent or comply with medication ; partial or complete bowel obstruction ; preexisting peripheral neuropathy of grade 1 or worse according to common toxicity criteria ; a personal or family history of dihydropyrimidine dehydrogenase deficiency , gilberts syndrome , or other congenital abnormality of biliary transport ; platelet counts less than 100 10 per l , an absolute neutrophil count less than 15 10 cells per l , serum bilirubin greater than one and a quarter times the upper limit of normal , or alkaline phosphatase greater than five times the upper limit of normal ; serum aminotransferase ( either aspartate aminotransferase or alanine aminotransferase ) greater than two and a half times the upper limit of normal ; or estimated creatinine clearance ( by cockcroft formula ) of less than 50 ml / min or measured glomerular filtration rate of less than 50 ml / m patients with another previous or current malignant disease , which , in the judgment of the treating investigator , was likely to interfere with the study treatment or assessment of response were also excluded . after the start of the trial , data emerged to support a benefit of cetuximab only in kras wild - type cancers , which led to a protocol amendment ( july 8 , 2008 ) to exclude patients with mutated kras . 
after completion of the study , a subset of tissue specimens were analysed for expanded ras / raf mutation status ( see appendix p 5 )  . the study was approved by the south west research ethics committee . 
written , informed consent was obtained from all patients before random assignment . randomisation and masking eligible patients were randomly assigned ( 1 : 1 ) to chemotherapy alone or chemotherapy plus cetuximab . 
a protocol amendment was then implemented on april 22 , 2009 , to condense the stratification factors to surgical centre , poor prognostic cancer ( yes vs no ) , and previous treatment with oxaliplatin as adjuvant ( yes vs no )  . 
poor prognostic cancer was defined as one or more of : four or more metastases ; n2 disease ( according to the tumour , node , and metastasis [ tnm ] staging system ) ; or poor differentiation of primary cancer . 
the amendment was made because the trial management group thought that the initial large number of stratification factors would be less effective at achieving balance between the treatment groups , as well as being logistically complicated . 
chemotherapy procedures patients were randomly assigned to chemotherapy with or without cetuximab for 12 weeks , followed by surgery and then a further 12 weeks of chemotherapy with or without consisted of oxaliplatin 85 mg / m administered intravenously over 2 h , l - folinic acid ( 175 mg flat dose administered intravenously over 2 h ) or d , l - folinic acid ( 350 mg flat dose administered intravenously over 2 h ) , and 5 - fluorouracil bolus 400 mg / m administered intravenously over 5 min , followed by a 46 - h infusion of fluorouracil 2400 mg / m repeated every 2 weeks ( regimen one ) , or oxaliplatin 130 mg / m administered intravenously over 2 h and oral capecitabine 1000 mg / m twice daily on days 114 repeated every 3 weeks ( regimen two )  . 
cetuximab was given as an intravenous dose of 500 mg / m every 2 weeks with regimens one and three or a loading dose of 400 mg / m followed by a weekly infusion of 250 mg / m with regimen two . 
briefly , 20% dose reductions for haematological or gastrointestinal toxic effects and dose delays of 2 weeks or longer were made for cetuximab toxic effects . chemotherapy were made there were several protocol changes throughout the duration of the study ( appendix pp 17 , 18 )  . 
the most important ones related to the restriction of recruitment to patients with kras wild - type cancers and the change in the sample size based on the predicted effect size from other studies . all surgery was done in high - volume liver centres in the uk with expertise in complex liver resections . 
treatment with ablation was not permitted by the protocol . all patients were followed up every 3 months for the first 2 years and every 6 months for a further 3 years until progression or death . 
adverse events and safety were assessed using the common terminology criteria for adverse events version 3 before each cycle unless there was a presentation earlier . illness preventing criteria for treatment to be discontinued were : progression while on therapy , unacceptable toxicity , inter current treatment , withdrawal of consent for treatment by the patient , or any alterations in the patients condition that justified the investigators discontinuation of opinion . treatment further the after nov 1 , 2012 , when the predefined futility criteria were met ( using a method proposed by freidlin and colleagues10 when the lower limit of the 95% ci for the progression - free survival hr was > 1 ) , the trial steering committee , on advice from the independent data monitoring committee , requested that cetuximab administration was stopped . 
data collection to inform outcomes was continued . outcomes the primary outcome was progression - free survival , which was defined as the time from randomisation to disease progression or death from any cause , whichever occurred first , and has been previously reported.5 patients without disease progression or death were censored at the date of the last assessment . 
as such , the assumption was made that any patient not recorded as having died could be assumed alive ( and censored ) 2 months before the nhs digital date of assessment of patient status ( ie , this excluded the possibility of missing a death event as the death had not yet reached the nhs digital database )  . 
for the evaluation of progression - free survival , patients lost to follow - up without progression were censored at the date of the last assessment , irrespective of whether or not the date of death was received subsequently via nhs digital . 
other secondary outcomes were preoperative response ( response after the end of the preoperative treatment period , assessed using recist ) , pathological resection status ( margin 1 cm , < 1 cm , or cancer on cut surface ) , safety , quality of life , and cost - effectiveness . 
other prespecified exploratory outcomes were post - progression survival in the primary analysis population who progressed and progression - free survival and overall survival in : patients treated with oxaliplatin , fluorouracil , and folinic acid ; patients who responded to preoperative chemotherapy ; patients with left - sided cancers ; and patients with rightsided cancers . 
all analyses presented were prespecified in the statistical analysis plan that was updated for this mature analysis ( appendix pp 196291 )  . statistical analysis the accrual target of the study was revised on jan 16 , 2012 , at the suggestion of the trial steering committee after a reconsideration of the potential effect of kras wild - type restriction . 
the revised sample size needed 268 patients ( and 212 disease progression events ) in patients with wild - type kras ( codons 12 , 13 , and 61 ) , under the assumptions of a log - rank test hr of 068 , 80% power , 5% two - sided significance level , 5% loss to follow - up , 3 - year recruitment , 5 years of follow - up , and progressionfree survival in the chemotherapy alone group of 67% at 1 year , 46% at 2 years , and 35% at 3 years . 
there was no correction of the p value to adjust for the previous analysis . an a - priori statistical analysis plan was devised for all analyses of these long - term data . 
the efficacy analyses were done on the primary analysis population ( composed of the intention - to - treat population including all patients with known kras [ codons 12 , 13 , and 61 ] wild - type status who had data available for the analysis being done ) , with hrs ( 95% cis ) and 2 - sided p values being calculated . 
data were reviewed by the data monitoring and ethics committee . for nhs digital see vol 21 march 2020 articles 823 patients assessed for eligibility 551 excluded 402 did not meet inclusion criteria 104 by patients or clinicians choice 45 other reasons 272 patients randomly assigned 1 incorrectly assigned 134 allocated to the chemotherapy alone group and included in safety analyses 137 allocated to the chemotherapy plus cetuximab group and included in safety analyses 6 not kras wild - type ( codons 12 / 31 / 61 ) 8 not kras wild - type ( codons 12 / 31 / 61 ) 128 included in the primary analysis population 113 operated 59 completed postoperative chemotherapy 129 included in the primary analysis population 108 operated 62 completed postoperative chemotherapy figure 1 : trial profile who performance status 0 or 1 128 ( 100% ) 126 ( 98% ) chemotherapy alone group ( n = 128 ) chemotherapy plus cetuximab group ( n = 129 ) 65 ( 5970 ) 64 ( 5969 ) 47 ( 37% ) 81 ( 63% ) 37 ( 29% ) 92 ( 71% ) 107 ( 84% ) 83 ( 65% ) 10 ( 8% ) 9 ( 7% ) 103 ( 80% ) 63 ( 49% ) 73 ( 57% ) 31 ( 24% ) 109 ( 84% ) 78 ( 60% ) 15 ( 12% ) 18 ( 14% ) 97 ( 75% ) 75 ( 58% ) 88 ( 68% ) 34 ( 26% ) age ( years ) * female male primary cancer t3 or t4 n1 or n2 poorly differentiated unresected 13 liver metastases one metastasis > 3 cm synchronous metastases carcinoembryonic antigen > 30 ng / ml extrahepatic disease 3 ( 2% ) 6 ( 5% ) data are median ( iqr ) or n ( % )  . 
 * in the previous publication , age was reported as mean ( iqr ) .5 according to the tumour , node , metastasis ( tnm ) staging syste data updated since the previous publication , which reported unresected primary cancer at trial entry in 13 ( 10% ) patients in the chemotherapy alone group and 18 ( 14% ) patients in the chemotherapy plus cetuximab group and synchronous metastases in 60 ( 47% ) patients in the chemotherapy alone group and 68 ( 53% ) patients in the chemotherapy plus cetuximab group.5 table 1 : baseline characteristics ( primary analysis population ) this study is registered with the international standard randomised controlled trial registry ( number 22944367 ) , with clinicaltrials.gov ( number 00482222 ) , and with the uk clinical research network ( number 2068 )  . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
tm , aw , and ls had full access to all the data in the study and all authors had final responsibility for the decision to submit for publication . results 272 patients were recruited from 39 institutions in the uk between feb 26 , 2007 , and oct 12 , 2012 , and randomly assigned to treatment . 
one patient was incorrectly assigned by mistake ( ie , the patient was eligible but the centre was asked to proceed with the opposite treatment to the one they had been assigned to ) , and was excluded from all analyses . 
an additional 14 patients ( six in the chemotherapy alone group and eight in the chemotherapy plus cetuximab group ) , who were randomly assigned before the amendment necessitating kras status testing and were retrospectively shown to have a kras mutation or indeterminate kras status , were also excluded from all analyses , except safety analyses . 
as such , the primary analysis population consisted of 257 patients , of whom 128 patients were randomly assigned to received chemotherapy alone and 129 to receive chemotherapy plus cetuximab ( figure 1 )  . 
table 1 shows the baseline characteristics , similar to those published previously.5 87 ( 68% ) of 128 patients in the chemotherapy alone group versus 89 ( 69% ) of 129 patients in the chemotherapy plus cetuximab group received oxaliplatin , 5 - fluorouracil , and folinic acid backbone treatment ( regimen 1 )  . 
smaller proportions of patients received capecitabine and oxaliplatin ( regimen 2 ; 27 [ 21% ] of 128 vs 24 [ 19% ] of 129 ) or irinotecan , 5 - fluorouracil , and folinic acid ( regimen 3 ; 11 [ 9% ] of 128 vs 15 [ 12% ] of 129 )  . 
 data on relative dose intensity are in the appendix ( pp 1924 )  . in this updated analysis , the median follow - up time was 667 months ( iqr 580775 ) : 669 months ( 583775 ) for patients in the chemo therapy alone group and 650 months ( 570775 ) in the chemotherapy plus cetuximab group . 
for the progression - free survival updated analysis there were 180 events ( 89 in the chemotherapy alone group and 91 in the chemotherapy plus cetuximab group ; since the preliminary analysis in 2013 , 57 additional events had occurred [ 33 in the chemotherapy alone group and 24 in the chemo therapy plus cetuximab group ] )  . 
the unadjusted hr for progression - free survival was 117 ( 95% ci 087156 ; p = 0304 ) for chemotherapy without versus with cetuximab , with an observed median progressionfree survival of 222 months ( 95% ci 183268 ) in the chemo therapy alone group and 155 months ( 138190 ) in the chemotherapy plus cetuximab group ( figure 2a )  . 
the remaining nine ( 7% ) deaths were due to other causes ( four [ 7% ] in the chemotherapy alone group and five the chemotherapy plus cetuximab group ; appendix p 29 )  . 
 the addition of cetuximab to chemo therapy resulted in an unadjusted hr for overall survival of 145 ( 95% ci 102205 ; p = 0036 ) , with an observed median overall [ 7% ] survival of 810 months ( 596not reached ) in the chemotherapy alone group and 554 months ( 435715 ) in the chemotherapy plus cetuximab group ( figure 2b )  . 
 the sensitivity analysis adjusting for the minimisation factors gave a similar result ( hr 144 , 102205 ; p = 0040 ; appendix p 27 )  . the response to preoperative chemotherapy is shown in the appendix ( p 25 )  . 
complete or partial response occurred in 78 ( 61% ) of 128 patients receiving chemotherapy alone and in 93 ( 72% ) of 129 patients receiving chemo therapy plus cetuximab . 
221 ( 86% ) of 257 randomly assigned patients underwent an operation , among whom 108 ( 96% ) of 113 patients in the chemotherapy alone group and 100 ( 93% ) of 108 patients in the chemotherapy plus cetuximab group proceeded to margin 1cm margin < 1cm no margin ( cancer visible on cut surface ) na ( no residual cancer ) missing ( limited surgery information available or ablation ) from second resection 36 / 108 ( 33% ) 29 / 100 ( 29% ) 54 / 108 ( 50% ) 49 / 100 ( 49% ) 8 / 108 ( 7% ) 12 / 100 ( 12% ) 10 / 108 ( 9% ) 0 / 108 ( 0% ) 7 / 100 ( 7% ) 3 / 100 ( 3% ) margin 1cm margin < 1cm 1 / 108 ( 1% ) 2 / 100 ( 2% ) 3 / 100 ( 3% ) no margin ( cancer visible on cut surface ) not applicable ( no residual cancer ) 1 / 108 ( 1% ) na ( ablation performed ) 1 / 108 ( 1% ) 1 / 100 ( 1% ) at least one surgical complication 28 / 113 ( 25% ) 27 / 108 ( 25% ) 1 / 108 ( 1% ) death during surgery postoperative death ( 30 days after liver resection ) data are n / n ( % )  . 
 * the preoperative chemotherapy period includes all randomised patients : n = 134 in the chemotherapy alone group , n = 137 in the chemotherapy plus cetuximab group ; the preoperative chemotherapy period lasted from the start of cycle 1 to the start of the last preoperative cycle plus 3 weeks for patients receiving chemotherapy regimen 1 or 3 or plus 4 weeks for patients receiving chemotherapy regimen 2 . 
only patients who had surgery and postoperative chemotherapy are included in the postoperative chemotherapy period , n = 116 in the chemotherapy alone group , n = 115 in the chemotherapy plus cetuximab group ; the postoperative chemotherapy period lasted from the start of the first postoperative chemotherapy cycle to the start of the last postoperative cycle plus 3 weeks for patients receiving chemotherapy regimen 1 or 3 or plus 4 weeks for patients receiving chemotherapy regimen 2 . table 3 : adverse events during the preoperative and postoperative chemotherapy periods the appendix ( pp 69 , 1215 )  . 
the results from the interaction subgroup analysis of overall survival and progression - free survival are in figure 3 and the appendix ( pp 10 , 11 )  . 164 ( 95% ci 092293 ) , with an observed median overall survival not reached ( 475not reached ) in the chemotherapy alone group and of 790 months ( 299not reached ) in the chemotherapy plus cetuximab group . extended ras / raf testing was successfully completed on primary colorectal cancer samples from 140 patients in the trial previously classified as kras wild - type ( codons 12 , 13 , and 61 )  . 
24 ( 17% ) of these 140 patients had mutations identified , comprising 13 patients with kras mutations , four patients with nras mutations , and seven patients with braf mutations . 
these mutations were balanced between the groups of the study with 12 in the chemotherapy alone group ( eight kras , one nras , three braf ) and 12 in the chemotherapy plus cetuximab group ( 5 kras , 3 nras , 4 braf )  . 
 99 ( 77% ) of 128 patients in the chemotherapy alone group and 103 ( 80% ) of 129 patients in the chemotherapy plus cetuximab group completed 12 weeks of preoperative chemotherapy ; 59 ( 52% ) of 113 patients in the chemotherapy alone group and 62 ( 57% ) of 108 patients in the chemotherapy plus cetuximab group completed 12 weeks of postoperative therapy . 
the proportion of patients requiring at least one dose modification was similar between the chemotherapy alone group ( 58 [ 45% ] of 128 in the preoperative period and 49 [ 43% ] of 113 in the postoperative period ) and the chemotherapy plus cetuximab group ( 60 [ 47% ] of 129 in the preoperative 408 vol 21 march 2020 articles period and 48 [ 44% ] of 108 in the postoperative period )  . 
 the proportion of patients requiring at least one dose delay was also similar between the chemotherapy alone group ( 65 [ 51% ] of 128 in the preoperative period and 38 [ 34% ] of 113 in the postoperative period ) and the chemotherapy plus cetuximab group ( 63 [ 49% ] of 129 in the preoperative period and 39 [ 36% ] of 108 in the postoperative period )  . 
there were 14 premature withdrawals from study treatment due to toxicity , six ( 4% ) of 134 in the chemo therapy alone group and eight ( 6% ) of 137 in the chemotherapy plus cetuximab group . the proportion of patients having least one preoperative grade 3 or worse toxicity and any postoperative grade 3 or worse toxicity was similar between the chemotherapy alone group ( 63 [ 47% ] of 134 in the preoperative period and 26 [ 22% ] of 116 in the postoperative period ) and the chemotherapy plus cetuximab group ( 72 [ 53% ] of 137 in the preoperative period and 34 [ 30% ] of 115 in the postoperative period ; table 3 )  . the most common grade 34 adverse events reported were neutrophil count decreased ( 26 [ 19% ] of 134 in the chemotherapy alone group vs 21 [ 15% ] of 137 in the chemotherapy plus cetuximab group ) , diarrhoea ( 13 [ 10% ] vs 14 [ 10% ] ) , skin rash ( one [ 1% ] vs 22 [ 16% ] ) , thromboembolic events ( ten [ 7% ] vs 11 [ 8% ] ) , lethargy ( ten [ 7% ] vs nine [ 7% ] ) , oral mucositis ( three [ 2% ] vs 14 [ 10% ] ) , vomiting ( seven [ 5% ] vs seven [ 5% ] ) , peripheral neuro pathy ( eight [ 6% ] vs five [ 4% ] ) , and pain ( six [ 4% ] vs six [ 4% ] )  . 
the most common serious adverse events reported of any grade were diarrhoea ( nine [ 7% ] vs seven [ 7% ] vs [ 5% ] ) , thromboembolic events ( nine seven [ 5% ] ) , vomiting ( seven [ 5% ] vs five [ 4% ] ) , fever ( six [ 4% ] vs three [ 2% ] ) , sepsis ( two [ 1% ] vs five [ 4% ] ) , and device - related infection ( two [ 1% ] vs five [ 4% ] )  . there were 26 drug - related serious adverse events in the chemotherapy alone group and 32 in the chemotherapy plus cetuximab group ( appendix pp 30 , 31 ) there were five deaths potentially related to treatment ( appendix p 29 )  . 
three of these related to systemic treatment , one in the chemotherapy alone group ( heart failure ) and two in the chemotherapy plus cetuximab group ( one pulmonary embolism and interstitial lung disease and one pulmonary embolism )  . 
another patient died of cardiac arrest within 90 days of surgery in the same treatment group and , although outside the protocol definition , this death might have been related to surgery . 
 surgical complications were reported in 28 ( 25% ) of 113 patients in the chemotherapy alone group and 27 ( 25% ) of 108 patients in the chemotherapy plus cetuximab group ( table 2 )  . 
protocol violations are recorded in the appendix ( pp 32 , 33 )  . discussion the interim analysis of the primary endpoint of the new epoc study showed a significantly shorter progression - free survival when cetuximab was added to perioperative chemotherapy , for patients with resectable colorectal liver metastasis.5 although progression - free survival has accepted validity as a surrogate endpoint , in the context of such an unexpected finding , the overall survival assumes a greater importance , despite being a secondary endpoint . 
this mature analysis found that the detriment in progression - free survival is no longer significant , although median overall survival was 26 months shorter for patients receiving cetuximab and chemotherapy than for those receiving chemotherapy alone . 
however , such a choice was neither standard nor technically feasible in 2005 , when the study started . the baseline characteristics of the chemotherapy plus cetuximab group are prognostically less favourable , with more patients having synchronous disease and a metastasis larger than 3 chowever , these differences are small and not significant . 
furthermore , review of the predefined subgroup analyses reveals the detriment with cetuximab in this present study occurred in patients with favourable characteristics ( not poorly differentiated , not n2 disease , fewer than four metastases )  . 
the subset with unfavour able prognostic features ( poorly differentiated histology , n2 disease , or four or more metastases ) did not benefit from addition of cetuximab to chemotherapy , but were not disadvantaged . 
as such , there is no evidence to suggest that any difference in the baseline variables contributed to the poor outcome of the cetuximab group . the quality of surgery following systemic therapy might have affected study outcome . 
at the time of the first publication it was not possible to present complete surgical data since not all patients had , at that time , undergone protocol - defined surgery . 
additional protocol violations included the two patients in the chemotherapy alone group who were not operated on during the period allowed by the protocol , because of a complete radiological response , and the two patients in the chemotherapy plus cetuximab group who were operated on , but not resected , because of a complete response . although it is natural to focus on the unexpected outcome in the experimental group of the trial , the survival achieved in the chemotherapy alone group should not be overlooked . 
indeed , the 5 - year survival in this group is comparable to the best of any case series , 1 despite the vol 21 march 2020 articles inclusion of borderline resectable patients . 
furthermore , there was only one 30 - day mortality in the 221 patients that underwent surgery , attesting to the quality of care in high - volume liver surgery centres in the uk . post - hoc analyses of other trials in advanced colorectal cancer have shown inferior survival outcomes with the addition of anti - egfr therapies to chemotherapy for kras - mutated and all ras - mutated cancers , 7 , 1113 and all ras wild - type testing before egfr therapy is now mandatory . 
the hr point estimate for detriment with cetuximab in the all ras / raf wild - type population was almost identical to that in the whole trial population , although it was not significant . 
this finding was not observed in the patients who had additional ras / raf pathway mutations discovered in the primary cancer on further the numbers are testing , but insufficient to make any definite conclusion . data to support a biological explanation for this unexpected trial outcome are accumulating . 
high expression of the microrna mir - 313p in primary colorectal cancer of patients with metastatic disease treated with cetuximab or panitumumab has been shown to be associated with resistance to egfr and disease progression.15 in the new epoc cohort , it was not possible to identify a patient subgroup in which mir - 313p expression levels were associated with an improvement in outcomes when cetuximab was added to chemotherapy.16 it is nevertheless interesting to observe that the poorer outcomes associated with the addition of cetuximab to chemotherapy were limited to patients with high mir - 313p expression in the primary cancer . 
this detrimental effect was not observed in patients with low mir - 313p expression levels.16 previous studies have suggested a predictive role for the expression of the egfr ligands amphiregulin ( areg ) and epiregulin ( ereg )  . 
in 2016 , survival benefit from the use of panitumumab in advanced colorectal cancer was observed in patients with high areg or ereg expression , or both , but not in those with low expression.17 by contrast , in new epoc , high ligand expression was associated with a decreased progressionfree survival with the addition of cetuximab , whereas patients with low ligand expression had a similar treatment progression - free survival allocation.18 rationalising these results with those of other studies is challenging , 17 , 1921 but serves to highlight the importance of biology , and possibly of an intact egfr signalling pathway , to the detriment in outcomes with the addition of cetuximab . 
this will be assessed in the translational analysis . irrespective of although studies of anti - egfr therapies in advanced disease have mostly been positive , those in the adjuvant setting have not , 22 , 23 with a trend towards detrimental outcomes in older patients.23 in the new epoc study , most patients were upfront operable and , therefore , the predominant effect of systemic intervention was likely to be on micrometastatic disease ; as such , these results are consistent with the adjuvant anti - egfr therapy data . 
this trial , therefore , does not preclude the possibility that there might be benefit from the addition of cetuximab in patients with more advanced and inoperable disease.6 , 7 the translational studies currently underway will hopefully provide an understanding of this possibility , thereby further informing the appropriate selection of patients for anti - egfr therapies . in the advanced disease setting , right - sided metastatic colon cancer has been reported to be less responsive to egfr inhibition , 24 the biology of which is currently being interrogated . 
in the new epoc trial , survival of patients with liver metastases from right - sided cancers was affected more than that of patients with left - sided cancers by the addition of cetuximab , although there were relatively few right - sided cancers and the difference was not significant . 
therefore , the biology underlying the right versus left phenomenon seen in advanced disease with egfr inhibition in the neoadjuvant setting should be investigated in future trials . further interrogation of the progression events in the new epoc population has revealed some informative observations.25 first , additional data collected after the interim analysis showed that there were numerically more multisite progressions in the chemotherapy plus cetuximab group than in the chemotherapy alone group . 
therefore , the addition of cetuximab seems to have not only accelerated disease progression , but also might have led to the development of a more aggressive disease genotype and phenotype . 
the translational studies that are underway will be crucial to explaining these complex observations . the survival curves suggests overall , we have shown that survival in patients with operable colorectal liver metastases is significantly worse with the use of cetuximab in combination with chemotherapy in the perioperative setting than with chemotherapy alone . 
cetuximab should not be used as neoadjuvant therapy in patients with operable colorectal liver metastases . 410 vol 21 march 2020 articles contributors jnp and jab conceived the study , designed the protocol , supervised the conduct and analysis of the trial . 
jwv reports grants from cancer research uk during the conduct of the study ; personal fees from ipsen , novartis , astrazeneca , merck , delcath , agios , pfizer , pci biotech , incyte , keocyt , qed , pieris pharmaceuticals , genoscience pharma , mundipharma edo , wren laboratories , nucana , and imaging equipment limited outside the submitted work ; and travel grants from celgene and nucana . 
th is a medical director for iqhealth tech , has received research funding ( to institution ) from pfizer , pierre fabre and has attended advisory boards for lilly and sobi . 
all other authors declare no competing interests . data sharing the anonymised derived data from this study including all fields will be made available to any investigator by application to the trial management group thorough the southampton clinical trials unit ( ctu@soton.ac.uk ) from the time of publication and thereafter . 
these data are available for any analysis with or without support of the investigators . acknowledgments we thank the patients for their participation in this study and their families , and all investigators and onsite personnel . 
this research study was funded by cancer research uk ( c317 / a7275 ) , and supported by the uk national institute of health research clinical research network : cancer . 
this study was also supported by a medical grant from merck kgaa ( darmstadt , germany ) , which also supported the provision of cetuximab for the study and the original kras testing . 
lancet oncol 2012 ; 13 : 81726in this article , the validation cohort began recruitment in february , 2009 , and the logistic regression equation in the statistical analysis section should have read : 6152 + 5517 dkk1 + 6867 afp the appendix has also been updated . 
panobinostat plus bortezomib and dexamethasone versus placebo plus bortezomib and dexamethasone in patients with relapsed or relapsed refractory multiple myeloma : and a multicentre , randomised , doubleblind phase 3 trial . 
lancet oncol 2014 ; 15 : 1195206in this article , the nal sentence of the third paragraph in the results section should read : independent progression - free survival was consistent with the investigator review : median progression - free survival was 1199 months ( 95% ci 10511350 ) for the panobinostat group and 831 months for ( hr 063 , the placebo group 95% ci 052076 ; p < 00001 ; appendix p 18 )  . 
whole - breast irradiation with or without a boost for patients treated with breast - conserving surgery for early breast cancer : 20 - year follow - up of a randomised phase 3 trial . 
lancet oncol 2015 ; 16 : 4756the fth sentence of the fth paragraph of the results section should read we recorded no signi cant di erence in the cumulative incidence of second primary tumour in the contralateral breast ( 208 in the no boost group vs 232 in the boost group ) , or at sites other than the breast ( 216 vs 240 ; appendix )  . 
 this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . correction to lancet oncol 2015 ; 16 : 91 oza am , cibula d , benzaquen ao , et al . 
 lancet oncol 2015 ; 16 : 8797in the results section of this article ( published online first on dec 4 , 2014 ) , the second sentence of the fifth paragraph should read the median duration of follow - up was 334 months ( iqr 204429 ) in the olaparib plus chemotherapy group and 322 months ( 195436 ) in the chemotherapy alone group . 
this correction has been made to the online version as of dec 29 , 2014 , and the printed article is correct . vol 16 january 2015 corrections correction to lancet oncol 2015 ; 16 : 133 correction to lancet oncol 2015 ; 16 : 181 , 184 correction to lancet oncol 2015 ; 16 : 237 published online january 29 , 2015 s1470 - 2045 ( 14 ) 70483 - 8 dp . 
 radiotherapy lancet oncol 2015 ; 16 : 23739in this comment , the fth line of the third paragraph should read : by contrast , acute gastrointestinal toxicity was increased with hypofractionation [ 95% ci 372469 ] of ( 420% patients the hypofractionation group had grade 2 adverse events vs 312% [ 266358 ] in the standard fractionation di erence 108% , 90% ci 5251643 ; p = 00015 ) although were similar 3 months after treatment , and non - inferiority was not con rmed . 
these corrections have been made to the online version as of march 2 , 2015 , and have been made to the printed comment . group , cavalli f , atun r . 
lancet oncol 2015 ; 16 : 13334 in this comment , the second sentence should have been : deaths from cancer are projected to increase from the present level of around 8 million a year to more than 13 million by 2030 , with most of the burden being in poorer countries . 
this correction has been made as of jan 29 , 2015 . correction to lancet oncol 2015 ; 16 : 266 ih , williams lj , kunkler jack wjl , cameron da , dixon jm , on behalf of investigators . 
 lancet oncol 2015 ; 16 : 26673in the interpretation section of the summary , the rst sentence should read postoperative whole - breast radiotherapy after breast - conserving surgery and adjuvant endocrine treatment resulted in a signi cant but modest reduction in local recurrence for women aged 65 years or older with early breast cancer 5 years after randomisation . 
this correction has been made to the online version as o f march 2 , 2015 , and to the printed article . thomas a , rajan a , berman a , in patients with et al . 
lancet oncol 2015 ; 16 : 17786 in the key of gure 2a of this article , the text for the red line should read thymic carcinoma ( 16 / 24 failed ) and that for the blue line should read in the thymoma ( 11 / 16 failed )  . 
 key of gure 4b , the text for the red line should read no change / increase ( 0 / 18 failed ) and that for the blue line should read decrease ( 4 / 4 failed )  . 
lancet oncol 2015 ; 16 : 27483in this article , the interpretation should have read : hypofractionated radiotherapy was not non - inferior to standard fractionated radiotherapy in terms of acute genitourinary and gastrofor men with intestinal intermediate - risk high - risk and prostate cancer . 
this correction has been made to the online version as of march 2 , 2015 and to the printed article . toxicity vol 16 march 2015 e105 correction to lancet oncol 2020 ; 21 : 101718 correction to lancet oncol 2020 ; 21 : 93546 correction to lancet oncol 2020 ; 21 : 112526 iarc monographs vol 127 group . 
lancet oncol 2020 ; 21 : 101718in this news piece , the web links in the margin for the preamble to the iarc monographs and for the iarc declarations of interest were incorrect and have been amended . 
 lancet oncol 2020 ; 21 : 112526in this comment , the fourth paragraph should read one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
because overdiagnosis appears to increase with age , it is possible that overdiagnosis occurred in both groups after the age of 50 years , but could not be detected because of the design of the trial . 
 this correction has been made as of sept 1 , 2020 , and the printed version is correct . vol 21 september 2020 e418 corrections corrections correction to lancet oncol 2015 ; 16 : 522 correction to lancet oncol 2016 ; 17 : 553 correction to lancet oncol 2016 ; 17 : 733 philip , pa . 
 this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . eggermont amm , chiarion - sileni v , grob j - j , et al . 
this correction has been made to the online version as of june 1 , 2016 . correction to lancet oncol 2016 ; 17 : 751 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . vol 17 june 2016 e223 correction to lancet oncol 2014 ; 15 : 150312 correction to lancet oncol 2019 ; 20 : 76980 correction to lancet oncol 2019 ; 20 : 98699 open - label phase 1 / 2 jg , niesvizky r , kumar sk , berdeja et al . 
 lancet oncol 2014 ; 15 : 150312in the eighth paragraph of the results section of this article , the first sentence should have been overall responses were noted in 59 ( 92% , 95% ci 8397 ) of 64 patients ( table 5 )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 765 ben - aharon i , goshen - lago t , fontana e , et al . 
this correction has been made to the online version as of july 1 , 2019 . 2018 jacob s , yap ml , wilson be , ferlay j , bray f , barton mb . 
 lancet oncol 2019 ; 20 : 76980 in the affiliations for this article , dr mei ling yap should have been affiliated with the university of new south wales ( sydney , nsw , australia )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 795805 randomised , controlled hofvind s , holen s , aase hs , et al . 
 lancet oncol 2019 ; 20 : 795805 in figure 1 , the number of patients with screen - detected breast cancer in the digital breast tomosynthesis group should have read 95 , and the number of patients in the digital mammography group should have read 87 . 
 quizartinib versus salvage chemotherapy in relapsed or refractory flt3 - itd acute myeloid leukaemia ( quantum - r ) : a multicentre , randomised , controlled , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 98699in this article , the second sentence in the statistical analysis section should have read the sample size calculation wording in the original protocol specified a 5% , two - sided calculation ; however , this wording was inaccurate , and subsequently , a one - sided calculation at 25% was implemented to solely test for superiority of quizartinib , which is consistent with the primary aim of the study . 
this correction has been made to the online version as of july 1 , 2019 , and the printed article is correct . correction to lancet oncol 2019 ; 20 : e30212 hillengass j , usmani s , rajkumar sv , et al . 
these corrections have been made to the online version as of july 1 , 2019 . vol 20 july 2019 e346 corrections corrections correction to lancet oncol 2013 ; 14 : 199209 correction to lancet oncol 2014 ; 15 : e241 esserman lj , thompson im , reid b , et al . 
the de nition of mrd low risk in the summary should read ( undetectable mrd at the end of induction [ day 29 ] or detectable mrd [ less than 001% ] at day 29 that became undetectable by week 11 )  . 
in gure 2 and in the rst paragraph of the results section , 1732 patients were clinical standard risk , 989 patients were risk , clinical 405 patients were clinical high risk . 
also in gure 2 , 2721 patients were eligible for mrd strati cation , 820 patients had indeterminate mrd status , 808 had high - risk mrd , 1059 had low - risk mrd , 34 patients had died within 35 days or had never remitted , and 323 patients were identi ed after august , 2009 . 
for the mrd low risk patients in table 1 , the total number of patients should read 1059 , of whom 466 were female , 764 were aged 29 years , 978 were b - lineage , 673 ( 64% ) were standard nci risk , 494 ( 47% ) had a white blood cell count less than 10 109 cells per l , and 177 had a white blood cell count of 1019 109 cells per l . 
the last sentence of the sixth paragraph of the results should read additionally , we noted no di erence between patients with undetectable mrd and those with less than 0005% mrd at day 29 . 
 these corrections have been made to the online version of the article as of june 30 , 2014 . vol 15 july 2014 e308 time to talk about planetary health and cancer care the 46th annual scientific meeting of the clinical oncology society of australia ( cosa ) was held on nov 1214 , 2019 , in adelaide , sa , australia . 
amid sessions on the meetings themes of urological cancers , age and gender issues , and digital health , was one that discussed the interface between cancer and environmental and political change . 
as many communities across australia were dealing with an unprecedented week of bush fires , the decision to set aside time to discuss cancer care in the context of the environment comes at a watershed moment . 
the fires brought to the fore a debate on what is thought to be a major cause of the drought conditions that have precipitated the worsening bush fire season climate change . lauded although some appear to question the link between climate change and the bush fires , it cannot be denied that the health of the planet affects that of human for reducing beings . 
australia should be greenhouse gas emissions by championing renewable energy ; however , it is also the third biggest exporter of fossil fuels , as measured by co2 potential , which is likely to have consequences on global and national scales . 
 a reluctance to acknowledge the potential effects of climate change on human health on a global scale will hinder progress to mitigate such consequences . designating climate change as a public health issue , the 2019 report of the lancet countdown on health and climate change , published in november , 2019 , suggests that a child born today will live in a world that is more than 4c warmer than that in the pre - industrial age , with health consequences evident throughout life . 
in addition to the general global deterioration in air quality , isolated events , such as the bush fires , can have an immediate and direct effect on air pollution . 
furthermore , with climate change in food leading to proposed changes potentially production and human diet ( for example , as explored in the eatlancet commission ) , resultant changes in the human microbiome resulting from changing diet might also affect disease outcomes , given the recognised effect of the microbiome on responses to anticancer treatment such as immunotherapy . 
in addition to the known longterm health consequences , the destruction caused by increasing climate change - related emergencies will have an acute effect on health and health services . oncology is particularly susceptible to disruption caused by events related to climate change because of the need for long - term treatments requiring multiple trips to specialist care at tertiary hospitals ; unique and highly specialised medicines , equipment , and training ; the susceptibility of patients with cancer to other health issues ; and existing comorbidities of the patients . 
road closures , destruction of infrastructure , and population displacement due to natural disasters can lead to an array of consequences resulting in patient hardelays in the delivery of essential medical supplies ( eg , cancer drugs or time - sensitive deliveries of radioactive isotopes for cancer imaging or treatment ) , a shortage of specialist staff to provide services or perform operations in hospitals or clinics , and reduced access to clinics for the patients themselves are just some of the disruptions to vital oncology services that patients might experience . 
this issue is true whether for small island nations devastated by a category 5 hurricanecompounding the challenge of the growing cancer burden in these regionsor a city cloaked in thick smoke from a nearby forest fire . 
in 2017 , flooding from a tropical storm forced the md anderson cancer center ( houston , tx , usa ) to cancel hospital appointments due to impassable nearby roads and flooded buildings . 
with the incidence of climate - related emergencies likely to increase over time , patients with cancer are likely to feel the effects . the consequences of many years of inaction on climate change are now rapidly taking their toll on the environment and on human health worldwide . 
the lancet oncology for more on cosa 2019 see fore more on the australian bush fires see reuters.com / article / us - australiabushfires / lack - of - forecast - rainsto - prolong - australian - bushfiresthreat - iduskbn1xo01c for discussion of climate change and the bush fires see politics / federal / raving - innercity - lunatics - michaelmccormack - dismisses - linkbetween - climate - change - andbushfires - 20191111 - p539ap . html for more on renewable energy in australia theguardian.com / australianews / 2019 / oct / 24 / australiasemissions - to - start - fallingthanks - to - renewables - boomresearchers - say for more on australian fossil fuel exports net.au / news / science / 2019 - 08 - 19 / australia - co2exports - third - highestworldwide / 11420654 for the lancet countdown on health and climate change see review lancet 2019 ; published online nov 13 . 
 n a d o f a r a g e n e k u l k a r n i firadenovec : a new gold standard for bcg - unresponsive bladder cancer ? lancet oncol 2021 ; 22 : 89in this comment , the declaration of interests statement was incorrect and should have read as follows : i report personal fees from merck , ferring , biosyent , tersera , abbvie , roche , theralase , and janssen , outside the submitted work . 
 this correction has been made to the online version as of dec 30 , 2020 , and the printed version is correct . maringe c , spicer j , morris m , et al . 
 the impact of the covid - 19 pandemic on cancer deaths due to delays in diagnosis in england , uk : a national , population - based , modelling study . 
lancet oncol 2020 ; 21 : 154950in this comment , on the second and eleventh lines of paragraph two , the drug name has been corrected to gx - 188e . 
durvalumab alone and durvalumab plus tremelimumab versus chemotherapy in previously untreated locally patients with unresectable , advanced or metastatic urothelial carcinoma ( danube ) : a randomised , open - label , multicentre , phase 3 trial . 
 lancet oncol 2020 ; 21 : 157488 in this article , the affiliation for ignacio duran should have been hospital universitario virgen del roco , seville , spathis correction has been made to the online version as of dec 30 , 2020 . correction to lancet oncol 2020 ; 21 : 160210 pm , welt ens poortmans fortpied c , et al . 
internal mammary and medial supraclavicular lymph node chain irradiation in stage iiii breast cancer ( eortc 22922 / 10925 ) : 15 - year results of a randomised , phase 3 trial . 
 lancet oncol 2020 ; 21 : 160210 in this article , the funders of the study should have been ligue nationale contre le cancer and kwf kankerbestrijding in the funding and acknowledgments sections . 
this correction has been made to the online version as of dec 30 , 20202 . vol 22 january 2021 corrections articles immunogenicity and hpv infection after one , two , and three doses of quadrivalent hpv vaccine in girls in india : a multicentre prospective cohort study rengaswamy sankaranarayanan , priya ramesh prabhu , michael pawlita , tarik gheit , neerja bhatla , richard muwonge , bhagwan m nene , pulikottil okuru esmy , smita joshi , usha rani reddy poli , parimal jivarajani , yogesh verma , eric zomawia , maqsood siddiqi , surendra s shastri , kasturi jayant , sylla g malvi , eric lucas , angelika michel , julia butt , janki mohan babu vijayamma , subha sankaran , thiraviam pillai rameshwari ammal kannan , rintu varghese , uma divate , shila thomas , geeta joshi , martina willhauck - fleckenstein , tim waterboer , martin mller , peter sehr , sanjay hingmire , alka kriplani , gauravi mishra , sharmila pimple , radhika jadhav , catherine sauvaget , massimo tommasino , madhavan radhakrishna pillai , for the indian hpv vaccine study group summary background an increase in worldwide hpv vaccination could be facilitated if fewer than three doses of vaccine are as e ective as three doses . 
we originally aimed to compare the immunogenicity and frequency of persistent infection and cervical precancerous lesions caused by vaccine - targeted hpv after vaccination with two doses of quadrivalent vaccine on days 1 and 180 or later , with three doses on days 1 , 60 , and 180 or later , in a cluster - randomised trial . 
 suspension of the recruitment and vaccination due to events unrelated to our study meant that some enrolled girls could not be vaccinated and some vaccinated girls received fewer than the planned number of vaccinations by default . 
participants were unmarried girls aged 1018 years vaccinated in four cohorts : girls who received three doses of vaccine on days 1 , 60 , and 180 or later , two doses on days 1 and 180 or later , two doses on days 1 and 60 by default , and one dose by default . 
the primary outcomes were immunogenicity in terms of l1 genotype - speci c binding antibody titres , neutralising antibody titres , and antibody avidity after vaccination for the vaccine - targeted hpv types 16 , 18 , 6 , and 11 and incident and persistent infections with these hpvs . 
4348 ( 25% ) girls received three doses , 4979 ( 28% ) received two doses on days 1 and 180 or later , 3452 ( 19% ) received two doses at days 1 and 60 , and 4950 ( 28% ) received one dose . 
immune response in the two - dose hpv vaccine group was non - inferior to the threedose group ( median uorescence intensity ratio for hpv 16 112 [ 95% ci 102123 ] and for hpv 18 104 [ 092119 ] ) at 7 months , but was inferior in the two - dose default ( 033 [ 029038 ] for hpv 16 and 051 [ 043059 ] for hpv 18 ) and one - dose default ( 009 [ 008011 ] for hpv 16 and 012 [ 010014 ] for hpv 18 ) groups at 18 months . 
fewer than three doses by design and default induced detectable concentrations of neutralising antibodies to all four vaccine - targeted hpv types , but at much lower concentration after one dose . 
cervical samples from 2649 participants were tested and the frequency of incident hpv 16 , 18 , 6 , and 11 infections was similar irrespective of the number of vaccine doses received . 
the testing of at least two samples from 838 participants showed that there was no persistent hpv 16 or 18 infections in any study group at a median follow - up of 47 years ( iqr 4251 )  . interpretation despite the limitations imposed by the suspension of the hpv vaccination , our ndings lend support to the who recommendation of two doses , at least 6 months apart , for routine vaccination of young girls . 
the shortterm protection a orded by one dose of hpv vaccine against persistent infection with hpv 16 , 18 , 6 , and 11 is similar to that a orded by two or three doses of vaccine and merits further assessment . funding bill & melinda gates foundation . copyright 2015 international agency for research on cancer ; licensee elsevier . 
 introduction persistent infection with a high - risk hpv causes cervical cancer , and worldwide 6882% of cervical cancers are attributed to hpv types 16 and 18.14 prophylactic vaccines containing recombinant virus - like particles assembled from the l1 capsid proteins of hpv 16 and 18 ( bivalent vaccine ) and hpv 6 , 11 , 16 , and 18 ( quadrivalent vaccine ) are used in hpv vaccination programmes . 
one and two doses of the bivalent hpv vaccine have been shown to protect against cervical hpv 16 and 18 infections as e ectively as three doses in women aged 1525 years . 
in a randomised trial , two doses of quadrivalent hpv vaccine given 6 months apart to girls aged 913 years resulted in a non - inferior immune response at 1 month after the last dose compared with three doses given to girls aged 913 years and to women aged 1626 years on day 1 , 2 months , and 6 months . 
 we searched pubmed and medline for full - length articles published between jan 1 , 2008 , and june 30 , 2015 , using the keywords hpv vaccination , less than three doses , alternate doses , one dose , two doses , three doses , immunogenicity , hpv infection , cervical intraepithelial neoplasia , clinical trials , randomised trials , follow - up studies ; we also searched clinicaltrials.gov for ongoing clinical trials of fewer than three doses of the hpv vaccine . 
we assessed all potentially relevant articles and found that neither the immunogenicity after one dose of quadrivalent hpv vaccination nor the extent of protection against hpv 16 and 18 infections a orded by fewer than three doses of quadrivalent hpv vaccine has been reported . added value of the study our ndings con rm that two doses of quadrivalent hpv vaccine , administered with an interval of 180 days or more , are immunologically non - inferior to the three - dose schedule and a ord protection against incident and persistent hpv 16 , 18 , 6 , and 11 infection that is similar to that a orded by three doses . 
 we also report the rst evidence to our knowledge that one dose of quadrivalent hpv vaccine induced detectable titres of hpv neutralising antibodies and that lower vaccine - induced antibody concentrations after one dose of quadrivalent hpv vaccine provide similar protection against vaccine - targeted hpv infections compared with the higher antibody concentrations induced after two or three doses . implications of all the available evidence our preliminary results suggest that future trials of hpv vaccines should include a single - dose arfurther long - term follow - up of vaccinated women in our study will clarify whether protection afforded after one dose of quadrivalent hpv vaccine is long - lasting . 
administration of three doses of hpv vaccine , or two doses as recommended by who , remains a challenge , and if one dose proves to be as efficacious as more doses , vaccine uptake will be improved and costs will be reduced . 
data on immunogenicity , durability of antibody response , and the frequency of persistent infection after one dose of vaccine will expedite the introduction of hpv vaccination in national immunisation programmes . 
 the e cacy of three doses of vaccine ( either bivalent or quadrivalent ) against high - grade cervical intraepithelial neoplasia caused by vaccine - targeted hpv was almost 100% in hpv - naive populations and greater than 55% in the intention - to - treat populations.13 the administration of three doses of the hpv vaccine , or even two doses as recommended by who , 4 , 5 is a challenge , and if one dose was as e ective as two or three doses then vaccine uptake would increase greatly and costs would be reduced . 
the high immune response in pre - adolescent girls given three doses suggests that reductions in dose number could prevent cervical neoplasia.6 , 7 data on immunogenicity , durability of antibody response , and frequency of persistent infection after one dose will enable the swift introduction of hpv vaccination in national immunisation programmes . 
 in 2009 , we initiated a cluster - randomised trial in india to compare the e ectiveness of two doses versus three targeting hpv doses of a quadrivalent vaccine types 16 , 18 , 6 , and 11 , in preventing cervical neoplasia . 
 however , recruitment and vaccination of the girls in the trial was suspended midway due to events unrelated to our study , which meant that some enrolled girls could not be vaccinated and some vaccinated girls received fewer than the planned number of vaccinations by default . 
here , we describe the immuno genicity and infection results after suspension of vaccination . immune methods study design and participants we initiated a multicentre , cluster - randomised trial in india on sept 1 , 2009 , to nd out whether two doses of quadrivalent hpv vaccine would be as e ective in inducing non - inferior preventing persistent vaccine - targeted hpv infection and cervical neoplasia as three doses . 
we recruited unmarried girls who were ambulant and in good general health aged 1018 years , living in 188 geographical clusters in nine locations in india ( osmanabad , dindigul , pune , mumbai , ahmedabad , delhi , hyderabad , gangtok in sikkim , and aizawl in mizoram )  . 
we obtained a new written informed consent from girls who became 18 years old during follow - up . procedures the vaccine used was the quadrivalent hpv vaccine ( gardasil ; merck sharp & dohme , whitehouse station , nj , usa )  . 
girls were originally randomly assigned to the two - dose group with vaccination on days 1 and 180 ( or later ) or the three - dose group with vaccination on days 1 , 60 , and 180 ( or later ) by the statistician at the international agency for research on cancer ( iarc )  . 
also using the computer - generated random allocation , the two groups in each study site were then randomly assigned to the two - dose group or the threedose group . 
vaccinations occurred from study start until april 8 , 2010 , when the indian authorities suspended all further recruitment and vaccination of girls in all hpv vaccination trials in india because of events unrelated to our study . 
the suspension meant that we had four groups of girls who were vaccinated : those on days 1 , 60 , and 180 or later ( original three - dose group ) ; those on days 1 and 180 or later ( original two - dose group ) ; those on days 1 and 60 by default ( two - dose default group ) ; and those with one dose only by default ( one - dose default group )  . at each study site , dedicated health workers and nurses were recruited and trained to identify and interview eligible girls for sociodemographic and reproductive information , explain the study to the participating girls and their parents or guardian , obtain informed consent , administer the vaccines , record adverse events , and do follow - up procedures , including obtaining blood and cervical cell samples . 
participants could contact a study clinician if they needed urgent medical attention using a 24 - h telephone help line . each participant was visited every year by a health worker or nurse in her household to enquire about her general health and wellbeing . 
details about marriage , medically signi cant events , pregnancy , antenatal and postnatal events , delivery , and migration were gathered and documented through the household visits , a network of social workers , medical - care providers , hospitals , and relatives . 
samples were treated with edta and analysed with luminex ( austin , tx , usa ) based multiplex serology8 , 9 to assess the concentration of binding antibodies against the major capsid protein l1 of hpv 16 , 18 , 6 , and 11 as mean median uorescence intensity ( mfi ; appendix )  . 
mfi values as a measure of antibody concentration quanti ed by use of hpv multiplex serology are directly comparable with optical densities measured with elisa8 and mfi values for hpv 16 in natural and vaccine - induced hpv 16 - speci c antibody responses are strongly correlated with endpoint the neutralisation assay.9 seropositivity cuto s for seroconversion were calculated for each hpv type , based on the mfi values of serum samples obtained from the participants at baseline after allowing for 5% seropositivity in the total baseline samples . 
the hpv genotyping method involved hpv - type - speci c e7 pcr bead - based multiplex genotyping.10 , 11 the multiplex hpv - type - speci c e7 pcr uses hpv type - speci c primers targeting the e7 region for the detection of 19 high - risk or probable highrisk hpv types ( 16 , 18 , 26 , 31 , 33 , 35 , 39 , 45 , 51 , 52 , 53 , 56 , 58 , 59 , 66 , 68a , 68b , 70 , 73 , and 82 ) , and two low - risk hpv types ( 6 and 11 ) , with detection limits ranging from ten to 1000 copies of the viral genome . 
the method was validated at the rajiv gandhi centre for biotechnology ( rgcb ; thiruvananthapuram , india ) under the supervision of scientists from iarc and the cervical cell samples were tested at rgcb . 
we de ned incident infections that persisted for 12 months or longer without an hpv negative test ( for the hpv type in question ) between the positive tests as persistent infections . immunological assays and hpv testing were done at rgcb , where a dedicated laboratory was established with technology transfer and external quality assurance from the german cancer research centre ( dkfz ; heidelberg , germany ) and the infections and cancer biology group at iarc ( lyon , france )  . 
scientists from rgcb were trained at dkfz , and the multiplex serology hpv - l1 antibody assays were done at rgcb by trained personnel , masked to the number of vaccine doses received by participants , under the technical supervision of experts from dkfz . outcomes the primary outcomes were immunogenicity outcomes : the hpv - l1 genotype - speci c binding antibody concentrations using geometric mean mfi , antibody avidity induced after vaccination using the geometric mean avidity index , and antibody concentrations speci c for neutralising epitopes in hpv - l1 using geometric mean neutralisation titres ( gmts ) ; and infection outcomes : rst incident and persistent infections of vaccinetargeted hpv types accumulated during follow - up . 
 cervical cells were taken 6 months after delivery or 18 months after marriage , whichever was earlier , and annually thereafter for 3 consecutive years . for the hpv - l1 binding antibodies outcome , we compared the geometric mean mfis at day 1 for all participants , at 7 months ( 1 month after the last dose ) , 18 months , 36 months , and 48 months after the rst dose of vaccination in the three - dose group versus the two - dose group , and at 18 months and 36 months after the rst dose vol 17 january 2016 articles of vaccination in the two - dose default and one - dose default groups versus the three - dose group . 
for the 12 - month comparison , the mfis in the one - dose default group were compared with those in the two - dose default group because other dose regimens were not measured at that timepoint . 
for the antibody avidity outcome , the geometric mean avidity indices were compared at 7 months for the two - dose and three - dose groups and at 18 months for all vaccination groups . 
for the neutralising antibody outcome , we compared the gmts at 18 months for hpv 16 , 18 , and 6 l1 in the two - dose , two - dose default , and one - dose default groups with those in the three - dose group . the secondary outcomes were cross - protection against non - vaccine targeted high - risk hpv types : rst incident and persistent non - targeted high - risk hpv infections accumulated during follow - up . the study will be monitored and assessed over 20 years . 
 long - term outcomes , such as the frequency of cervical intraepithelial neoplasia grades 2 and 3 and invasive cancer , will be assessed by screening of participating women and using data from population - based cancer registries . statistical analysis we aimed to recruit 20 000 girls from nine locations in india ( 7000 girls from osmanabad , 3000 each from dindigul , pune , and mumbai , 1000 each from ahmedabad , delhi , and hyderabad , and 500 each from gangtok in sikkim , and aizawl in mizoram ) , with 10 000 girls living in 100 clusters randomly allocated to the two - dose group and 10 000 girls in 88 clusters to the three - dose group . 
to test for non - inferiority of antibody concentrations in di erent dose groups , we used log - transformed mean mfis in linear regression models to obtain mfi ratios and their corresponding 95% cis . 
in keeping with other hpv immunogenicity studies , non - inferiority of a vaccination group was concluded if the lower bound of the 95% ci for its mfi ratio was greater than 05.1214 in a post - hoc power calculation , using the lowest limit of 95% ci with a sample size of 40 individuals per group , we had 90% power for non - inferiority testing between each of the observational groups and the three - dose group . the antibody avidity index was calculated by dividing the mfi values of urea - treated samples by the mfi values of the untreated samples and multiplied by 100% . 
 to compare the fewer than three - dose regimens with the three - dose regimen , log - transformed avidity index values were used in linear regression models to obtain avidity index ratios and their 95% cis . 
non - inferiority of the fewer than three - dose regimens to that of the three - dose regimen was concluded if the 95% ci lower bound of the avidity ratio index was greater than 05 . 
non - inferiority of the gmt was concluded if the 95% ci lower bound of the neutralisation gmt ratio was greater than 05 . hpv 16 l1 antibodies 10 000 hpv 18 l1 antibodies three - dose group two - dose group two - dose default group one - dose default group seropositivity cuto hpv 6 l1 antibodies hpv 11 l1 antibodies 1000 10 000 1000 7 or 12 * 7 or 12 * time after rst dose ( months ) time after rst dose ( months ) figure 2 : mean mfi values for hpv types 16 , 18 , 6 , and 11 l1 antibodies dashed lines show the threshold ( cuto ) values for seroconversion . 
 * mfi values for month 7 were used for the three - dose and two - dose vaccine groups , whereas mfi values for month 12 were used for the two - dose default and one - dose default groups . 
 vol 17 january 2016 articles hpv 16 l1 hpv 18 l1 hpv 6 l1 hpv 11 l1 three doses t w o doses three doses t w o doses , default t w o doses one dose , default three doses t w o doses three doses t w o doses , default t w o doses one dose , default month 7 month 18 month 7 month 18 sample time ( months ) and number of doses received figure 3 : box plots of the avidity index of mfi for hpv types 16 ( a ) , 18 ( b ) , 6 ( c ) , and 11 ( d ) l1 antibodies at 7 months and 18 months after the rst dose mfi = median uorescence intensity . 
for this reason , all regression analyses were adjusted for the cluster design by specifying the option in the regression models that allows the variance - covariance estimator to include the clustering e ect . hpv infection outcomes are reported as frequencies of the detection of rst incident infection and persistent infections of vaccine - targeted and non - targeted high - risk hpv infections accumulated during the follow - up . for both the primary and secondary outcomes , analysis was done per the actual number of vaccine doses a participant received . 
other than the donation of the vaccines , merck did not have any role in design , protocol development , study conduct , monitoring , and assessment , analysis of data , or writing of the report . 
the corresponding author had full access to all the data in the study and all the authors had nal approval for the decision to submit . results vaccination of eligible girls was initiated on sept 1 , 2009 , and continued until april 8 , 2010 . 
of the 21 258 eligible girls identi ed for recruitment in the 188 clusters , 17 729 ( 83% ) from 178 clusters were vaccinated at least once : 4348 ( 25% ) girls received three doses on days 1 , 60 , and 180 or later ( three - dose group ) ; 4979 ( 28% ) received two doses on days 1 and 180 or later ( two - dose group ) ; 3452 ( 19% ) received two doses on days 1 and 60 by default ( two - dose default group ) ; and 4950 ( 28% ) received one dose by default ( one - dose default group ; gure 1 ; appendix )  . 
the baseline characteristics of participants in the four groups show more or less similar age distribution , whereas we noted some di erences in average monthly household income and education ( table 1 )  . 
local and systemic reactions within 15 days of administering 34 856 vaccine doses in the study included injection - site pain ( number of reactions ; n = 1092 ) , low - grade fever ( n = 293 ) , injectionsite swelling ( n = 64 ) , headache ( n = 49 ) , nausea ( n = 30 ) , skin rash ( n = 15 ) , diarrhoea ( n = 13 ) , abdominal cramps ( n = 13 ) , and fainting attacks ( n = 10 )  . 
the mfi results of the hpv - l1 binding antibody analyses are in the for seroconversion for hpv 16 , 18 , 6 , and 11 l1 were 100 , 41 , 240 , and 48 , respectively . 
analysis of 625 plasma samples ( 308 in the three - dose group and 317 in the two - dose group ) obtained at month 7 for peak hpv - l1 binding antibody concentrations indicated that all girls in both groups had seroconverted and almost all girls in the twodose group had mfis equal to or higher than the lowest mfi in the three - dose group for all four vaccine - targeted hpv types ( appendix )  . 
the peak antibody concentrations at 7 months for vaccine - targeted hpv types in the twodose cohort were non - inferior to the mfis in the threedose group ( appendix )  . 
mfi ratios for the two - dose versus three - dose group were 112 ( 95% ci 102123 ) for hpv 16 l1 , 104 ( 092119 ) for hpv 18 l1 , 104 ( 097113 ) for hpv 6 l1 , and 112 ( 106119 ) for hpv 11 l1 . the hpv - l1 binding antibody concentrations for the vaccine - targeted hpv types were similar for the threedose and two - dose groups over 48 months ( gure 2 ; appendix )  . 
the antibody concentrations in the two - dose vaccine group had similar decay kinetics and were noninferior to those in the three - dose group at 7 months , 18 months , 36 months , and 48 months , over the 48 - month period ( appendix )  . 
at least 124 ( 98% ) of 127 girls in the two - dose group had antibody concentrations equal to or greater than the lowest antibody mfi in the three - dose group at 48 months ( appendix )  . 
 the hpv - l1 binding antibody concentrations for the vaccine - targeted hpv types in the two - dose default and one - dose default groups were inferior to the concentrations in the three - dose group at 18 months and 36 months . 
 at month 36 , the number of samples analysed was 271 in the three - dose group , 513 in the two - dose default group , and 510 in the one - dose default group ( appendix )  . 
at 36 months , 511 ( > 99% ) of 513 girls in the two - dose default group and 462 ( 91% ) of 510 the one - dose default group had antibody concentrations equal to or higher than the lowest mfi value in the three - dose group ( appendix )  . 
there was no correlation between age and antibody titres in the onedose default group ( correlation coe cient = 0067 )  . the values for geometric mean avidity index for hpv types 16 , 18 , 6 , and 11 after the two - dose schedule at 7 months and after the two - dose , two - dose default , and one - dose default schedules at 18 months , were noninferior to the value after the three - dose regimen . 
 for example , the avidity index ratio of the one - dose default group compared with the three - dose group for hpv 16 l1 was 110 ( 95% ci 101119 ; gure 3 ; appendix )  . the gmts of neutralising antibodies to hpv types 16 and 6 at 18 months after the rst dose in the two - dose group were non - inferior to the gmts in the three - dose group , but were inferior for hpv 18 . 
the gmt ratio of hpv 16 l1 neutralisation titres was 100 ( 95% ci 069145 ) for the two - dose group compared with the three - dose group , whereas for hpv 18 l1 neutralisation titres , it was 042 ( 027065 ) for the two - dose group compared with the three - dose group ( gure 4 ; appendix )  . 
 the gmt after the two - dose default and one - dose default schedules for hpv types 16 , 18 , and 6 were inferior to the gmt of the three - dose group ( gure 4 ; appendix )  . 
the gmt ratio of hpv 16 l1 neutralisation titres was 023 ( 016034 ) for the two - dose default group compared with the three - dose group . the median time between rst vaccination and rst cervical sample collection from 2649 participants was 39 years ( iqr 3047 )  . 
the medians were 41 years ( iqr 3348 ) for the three - dose group , 43 years ( 3348 ) for the two - dose group , 37 years ( 2946 ) for the two - dose default group , and 37 years ( 2945 ) for the one - dose default group . 
in 838 women for whom two or more samples were available for analysis , there were no persistent hpv 16 and 18 infections in any of the four study groups at a median follow - up of 47 years ( iqr 4251 ; table 2 )  . 
higher frequencies of persistent vaccine non - targeted hpv infections were noted in the four study groups as compared with vaccine - targeted hpv infections . discussion our ndings suggest that two doses of quadrivalent hpv vaccine , administered with an interval of 180 days or more between doses , are immunologically non - inferior to the three - dose schedule and a ord protection against incident and persistent hpv 16 , 18 , 6 , and 11 infections that is similar to that a orded by three doses . 
 * incident hpv infections with no subsequent sample to assess persistence . table 2 : incident hpv infection and hpv infection status frequency of hpv types 16 and 18 infections range from 3% to 9%.2023 in this context , our initial results provide new evidence that one and two doses of quadrivalent vaccine prevent incident and persistent cervical infections with hpv types 16 , 18 , 6 , and 11 , similar to the protection a orded after a three - dose schedule during a median follow - up of 47 years ( iqr 4251 )  . to our knowledge , our study is the rst in which immunogenicity and vaccine - targeted hpv infection frequencies are reported after one dose of quadrivalent vaccine . 
although the antibody concentrations after one dose were lower than those in the two - dose and three - dose groups , the titres were stable and the mean avidity index after one dose was non - inferior to that after three doses . 
one - dose vaccination also induced detectable titres of neutralising antibodies to all four vaccine - targeted hpv vol 17 january 2016 articles types in most of the participants that were assessed , but at a much lower concentration . 
there is no known minimum threshold concentration of antibodies that is protective ; seroconversion is an arbitrary cuto and does not represent the minimum threshold for protection.1 , 24 our immunogenicity ndings after three and two doses of vaccine are consistent with the results from a canadian randomised trial25 in which 261 girls aged 913 years were allocated to vaccine with three doses of quadrivalent vaccine at day 1 , 2 months , and 6 months ; 259 girls also aged 913 years were allocated to vaccine with two doses at day 1 and 6 months ; and 310 women aged 1626 years were allocated to vaccine with three doses also at day 1 , 2 months , and 6 months . 
the antibody concentrations for all four vaccine - targeted hpv types in the girls aged 913 years given two doses were non - inferior to those in women aged 1626 years who received three doses during a 36 - month period . 
our results suggest that the low vaccine - induced antibody concentrations after one dose a ord similar protection against vaccine - targeted hpv infections as the high antibody concentrations from two or three doses during a median follow - up of 47 years ( iqr 4251 )  . 
the similar frequency of incident nonvaccine hpv types in each dose group ( table 2 ) implies that hpv exposure was similar across the di erent groups and participants sexual behaviours were not related to the number of doses received . 
a follow - up of these women is planned over 20 years to assess the e cacy endpoints for the incidence of cervical intraepithelial neoplasia grades 2 and 3 and invasive cervical cancer caused by vaccine - targeted and non - targeted hpv types in the di erent dose groups by screening of participating women and using data from populationbased cancer registries . 
we have also recruited and are following up an age - matched and residence - matched cohort of unvaccinated women ( n = 1540 )  . the protection a orded by virus - like particle vaccines is believed to be mediated by neutralising antibodies leading produced by plasma cells , 31 , 32 most of which have short in peak antibody to declines lifespans , concentrations within a few months . 
 concentrations of antibodies measured 1218 months after the last dose of a virus - like particle vaccine generally represent the activity of long - lived plasma cells and are the best predictors of antibody persistence . the patterns of antibody responses after one dose of vaccine in our study and in the costa rica and patricia trials27 , 30 seem to be similar to the pattern after a live attenuated vaccine , which usually a ords long - lasting protection . 
the stable antibody response after one dose of the hpv l1 vaccine might be due to the structure of the hpv - like particles and the antigens it displays to the immune system might eliminate the need for doses after the priming dose.27 , 33 , 34 notably , in a cohort study35 in which girls aged 1024 years and women received three doses ( n = 98 252 ) , two doses by default ( n = 112 555 ) , and one dose by default ( n = 119 046 ) of the quadrivalent vaccine , the incidence rate ratios for the occurrence of condylomas were 018 , 029 , and 031 , respectively , implying that one dose and two doses with a short interval were associated with signi cant reduction in condyloma risk compared with 926 119 unvaccinated women . due to the disruption of recruitment and randomisation because of the suspension of vaccination midway in our planned two - arm randomised trial , our study has essentially become an observational cohort study of participants in four dose groups with similar socio demographic characteristics . 
vaccination was suspended in our study in response to instructions from the indian council of medical research in the context of all hpv vaccination studies in india pending an enquiry into the causes of death of ve girls ( subsequently proven unrelated to hpv vaccination ) recruited for an hpv vaccination demonstration project in the states of andhra pradesh and gujarat . 
major limitations include the non - randomised comparison of the vaccination dose groups , an absence of memory b - cell response data , limitations in interpreting early results for girls given incomplete dose schedules , and biases that might have been introduced after vaccination interruption and loss of randomisation . 
despite these limitations , our study of hpv vaccination is representative of generalisable real - world conditions : it had varying dose schedules and a broad age range of participants in addition to the di culties and challenges inherent in running hpv vaccination studies in low - income and middle - income countries . 
moreover , the inclusion of sexually naive girls aged 1018 years ( the primary and secondary target age groups for vaccination ) , the possibility of long - term followup , and the technology transfer that allowed validated and quality assured execution of antibody assays and hpv genotyping and the resultant independence in assessing outcomes without having to rely on pharmaceutical industry laboratories or laboratories abroad are important strengths of our study . vol 17 january 2016 articles our preliminary results after one dose of quadrivalent vaccine by default , although promising , should be interpreted with caution and suggest that future trials of hpv vaccines should include a single dose arfurther longterm follow - up of vaccinated women in our study will clarify lasting protection after one dose . 
because of the programmatic advantages of one dose in terms of cost savings , logistics , and coverage , and the high proportion of participants who default after immunisation programmes , particularly in developed countries , 36 , 37 assessment of the clinical e cacy of a single dose is of substantial public health signi cance . 
a single dose of hpv vaccine , providing strong and sustained protection against hpv infection in the long term , is the best way to overcome the barriers to vaccine uptake globally . 
 the rst dose our ndings support the who recommendation to use two doses separated by 6 months or more for vaccination of young girls , and indicate that a single dose of the hpv vaccine merits further assessment . contributors rs had the initial idea for the study , and was responsible for the conception , design , and conduct , monitoring , and supervision of the study , and acquisition , analysis , and interpretation of the data . 
tg was a co - investigator , and was responsible for the overall supervision of the laboratory analyses of the cervical cell samples , and technology transfer to sta from the indian central laboratory . 
nb was the study representative for the indian authorities on behalf of all participants ; she was responsible for the on - site conduct of the study in delhi , participated in monitoring , supervision , acquisition , and interpretation of the data , and the provision of clinical services at the study site . 
bmn and sgm were responsible for the on - site conduct of the study in barshi , poe in ambilikkai , sj in pune , urrp in hyderabad , pj in ahmedabad , yv and ms in sikkim , ez and ms in mizoram , and sss , gm , and sp in mumbai , and they participated in the monitoring , supervision , acquisition , and interpretation of the data , and the provision of clinical services at their respective study sites . 
establishment of the luminex - based assays at rgcb was partly supported by the european commission - seventh framework programme grant hpv - ahead ( fp7 - health - 2011 - 282562 )  . 
we assessed whether dose intensi cation of doxorubicin with ifosfamide improves survival of patients with advanced soft - tissue sarcoma compared with doxorubicin alone . methods we did this phase 3 randomised controlled trial ( eortc 62012 ) at 38 hospitals in ten countries . 
we included patients with locally advanced , unresectable , or metastatic high - grade soft - tissue sarcoma , age 1860 years with a who performance status of 0 or 1 . 
they were randomly assigned ( 1 : 1 ) by the minimisation method to either doxorubicin ( 75 mg / m by intravenous bolus on day 1 or 72 h continuous intravenous infusion ) or intensi ed doxorubicin ( 75 mg / m ; 25 mg / m per day , days 13 ) plus ifosfamide ( 10 g / m over 4 days with mesna and peg lgrastim ) as rst - line treatment . 
randomisation was strati ed by centre , performance status ( 0 vs 1 ) , age ( < 50 vs 50 years ) , presence of liver metastases , and histopathological grade ( 2 vs 3 )  . 
there was no signi cant di erence in overall survival between groups ( median overall survival 128 months [ 955% ci 105143 ] in the doxorubicin group vs 143 months [ 125165 ] in the doxorubicin and ifosfamide group ; hazard ratio [ hr ] 083 [ 955% ci 067103 ] ; strati ed logrank test p = 0076 )  . 
median progression - free survival was signi cantly higher for the doxorubicin and ifosfamide group ( 74 months [ 95% ci 6683 ] ) than for the doxorubicin group ( 46 months [ 2956 ] ; hr 074 [ 95% ci 060090 ] , strati ed log - rank test p = 0003 )  . 
more patients in the doxorubicin and ifosfamide group than in the doxorubicin group had an overall response ( 60 [ 26% ] of 227 patients vs 31 [ 14% ] of 228 ; p < 00006 )  . 
for a few sarcomasnotably , targeted gastrointestinal stromal treatment is available.1 however , although translocations or ampli cations have been associated with an increasing number of sarcoma subtypes , these ndings have led to innovative treatment for only a minority of cases.24 for most advanced sarcomas , clinicians rely on conventional tumourse ective chemotherapy for palliation , which is somewhat e ective , few patients achieve an objective response.5 but histological diagnosis can be used to guide treatment for some sarcomaseg , taxanes for angiosarcoma , 6 , 7 or gemcitabine - containing treatment for leiomyosarcoma and un di erentiated pleomorphic sarcoma.8 , 9 nevertheless , doxorubicin and ifosfamidewhich have been used to treat soft - tissue sarcoma for more than 30 yearsstill have an important role . 
 ifosfamide has a clear doseresponse relationship , with 9 g / m fractionated over 3 days producing a higher proportion of responses than 5 g / m given as a 24 h infusion.10 responses in as many as 5060% of patients have been reported for various regimens of anthracycline plus ifosfamide1113 but these ndings have not been replicated in randomised trials . 
in the palliative setting , disease control can delay deterioration of symptoms , therefore progression - free survival might be equally important as overall survival , although improved overall survival is still a key goal of treatment.14 we assessed whether the addition of ifosfamide to doxorubicin improved the survival of patients with locally advanced unresectable or metastatic soft - tissue sarcoma . 
 to establish the true value of the combination , we used a dose of ifosfamide used in previous phase 2 trials to enable direct comparison and the doxorubicin dose was identical in the two groups both to maximise dose intensi cation and to test the e ect of adding ifosfamide . methods study design and participants we did this phase 3 , randomised controlled trial ( eortc 62012 ) at 38 hospitals in ten countries ( belgium , canada , denmark , france , germany , netherlands , slovakia , spain , switzerland , uk ; appendix )  . 
patients had to be age 1860 years , with a who performance status17 of 0 or 1 , absolute neutrophil count more than 2 10 cells per l , more than 100 10 platelets per l , serum creatinine of 120 mol / l or less or calculated creatinine clearance ( cockroft and gault method ) more than 65 ml / min , two functioning kidneys , bilirubin 30 mol / l or less , and albumin more than 25 g / l . 
patients also had to have a normal ( according to local assessments ) left ventricular ejection fraction by multiple gated acquisition scan or echocardiogra liposarcoma , pleomorphic synovial women of child - bearing potential had to take adequate contraceptive measures and have a negative pregnancy test within 7 days of study entry . 
we excluded patients with : gastrointestinal stromal tumour , mixed mesodermal tumour , chondrosarcoma , malignant mesothelioma , neuroblastoma , osteosarcoma , ewings sarcoma , desmoplastic small round cell tumour , embryonal rhabdomyosarcoma , and alveolar soft part sarcoma . 
additional exclusion criteria were other severe illness ( eg , psychosis or previous history of cardiovascular disease ) , symptomatic or known cns metastases , previous or concurrent second primary malignant tumours ( except adequately treated insitu carcinoma of cervix or basal cell carcinoma )  . 
we also excluded patients who had had radiotherapy to the sole available lesion or those who had received chemotherapy for advanced disease , although previous adjuvant chemotherapy ( preoperative or postoperative ) was allowed if disease progression had not occurred within 6 months of completion . index the study protocol is available online . 
randomisation was strati ed by centre , performance status ( 0 vs 1 ) , age ( < 50 years vs 50 years ) , liver metastases ( present vs absent ) , and histological grade ( 2 vs 3 )  . 
neither patients nor investigators were masked to treatment allocation . procedures patients assigned to receive doxorubicin alone were given doxorubicin 75 mg / m by intravenous bolus on day 1 or 72 h continuous intravenous infusion . 
those assigned to receive intensi ed doxorubicin and ifosfamide received doxorubicin 25 mg / m per day on days 13 and ifosfamide ( 25 g / m per day , days 14 ) plus mesna ( 05 g / m by intravenous bolus before ifosfamide , 15 g / m concurrent with ifosfamide , and 1 g / m orally 2 h and 6 h after completion of ifosfamide infusion ) , followed by peg lgrastim ( 6 mg subcutaneously , day 5 ; appendix )  . 
clinical assessments of safety , including physical examination , performance status , blood chemistry , and urinalysis ( with dipstick ) were done at baseline and before each cycle of treatment . 
doxorubicin causes cumulative cardiotoxicity and ifosfamide can cause cumulative renal impairment , bladder toxic e ects , and central encephalopathy . disease was assessed after every two cycles of treatment with chest radiography and either ct or mri scans . 
for patients with complete response , partial response , or stable disease at the end of treatment ( assessed with recist 1.0 ) , assessments were continued every 6 weeks . 
for stable disease , a minimum of 6 weeks was speci ed . statistical analysis the trial was powered to detect a hazard ratio ( hr ) of 0737 at most . 
the choice of 50% as comparator was based on an analysis of more than 2000 patients with sarcoma treated with rst - line anthracycline - containing chemotherapy , survival was for whom median 12 months.19 366 events were needed to detect such a di erence with a two - sided strati ed log - rank test ( = 005 , power = 80% )  . 
we did two interim analyses : one futility analysis after 52 events ( progression or death ) to assess if progression - free survival at 6 months was signi cantly greater in the doxorubicin and the doxorubicin group ( target hr 05 , = 005 ) and one based on overall survival after 188 deaths ( using an error spending function with a boundary parameter of 02 )  . 
 we used a stopping rule for toxic e ects , with ongoing analyses once every 6 months , such that if febrile neutropenia occurred in more than 30% of cycles of treatment with doxorubicin and ifosfamide , the study would be stopped . ifosfamide group than overall survival was computed from the date of randomisation to the date of death from any cause . 
patients alive and progression - free at the time of analysis were censored at the date of last follow - up . we estimated overall survival and progression - free survival with the kaplan - meier method and compared treatment groups with a two - sided log - rank test . 
we used a signi cance level of 00451 ( adjusted for interim analysis , associated cis are 955% ) for the analysis of overall survival , whereas we used 005 for the other endpoints . we did the primary e cacy analyses for the intentionto - treat populationie , all randomly assigned patients ( including those retrospectively found to be ineligible ) according to their allocated treatment . 
we did sensitivity e cacy analyses for the per - protocol populationie , all randomly assigned patients who satis ed the eligibility criteria and started their allocated treatment . 455 patients randomly assigned 228 assigned to doxorubicin only 227 assigned to doxorubicin and ifosfamide 8 ineligible according to study coordinator ( ij ) review * 7 ineligible according to study coordinator ( ij ) review 3 refused treatment 3 did not start treatment 1 refused 1 performance status worsened 1 clinical progressive disease 2 started treatment , but did not follow the allocated approach 1 by mistake 1 reason unknown before rst cycle 217 eligible and started allocated treatment 215 eligible and started allocated treatment 94 relapsed or died because of 45 relapsed or died because of 117 discontinued progressive disease 5 had toxic eects 4 refused 4 intercurrent deaths 10 for other reasons progressive disease 103 discontinued 36 had toxic eects 10 refused 1 intercurrent death 11 for other reasons 228 included in intention - to - treat ecacy analyses 223 included in safety analyses 217 included in per - protocol analyses 227 included in intention - to - treat ecacy analyses 224 included in safety analyses 215 included in per - protocol analyses figure 1 : trial pro le * one of whom started treatment but did not follow the allocated approach . vol 15 april 2014 articles the clinical cuto date was july 5 , 2012 . 
the corresponding author had the nal responsibility for the decision to submit for publication . results we enrolled 455 patients between april 30 , 2003 , and may 25 , 2010 . 
although information about degree of di erentiation and necrosis was available , missing data for mitotic count for ten patients precluded accurate distinction between intermediate and high grade ; thus , they were strati ed as high grade for randomisation . 
15 patients were deemed ineligible by the study coordinator ( ij ; gure 1 ) , reasons were : inappropriate histological results on central review ( n = 9 ) , treatment started before randomisation ( n = 1 ) , previous treatment ( n = 1 ) , too old ( n = 2 ) , impaired renal function ( n = 1 ) , only one kidney because of previous kidney cancer ( n = 1 ) , and poor performance status ( n = 2 )  . 
as a result , the safety population consisted of 447 patients and the per - protocol population of 432 patients ( gure 1 )  . median follow - up was 56 months ( iqr 3177 ) for the doxorubicin group versus 59 months ( iqr 3672 ) for the doxorubicin and ifosfamide group . 
most patients died as a result of progressive disease ( table 2 ) ; 30 patients ( 13 vs 17 ) were still alive and progression - free at the cuto date . there was no signi cant di erence between groups in terms of overall survival ( gure 2a )  . 
median overall survival was 128 months ( 955% ci 105143 ) in the doxorubicin group versus 143 months ( 125165 ) in the doxorubicin and ifosfamide group ( hr 083 , 955% ci 067103 ; strati ed log - rank test p = 0076 )  . 
 overall survival at 1 year was 51% ( 955% ci 4458 ) in the doxorubicin alone group versus 60% ( 5366 ) in the doxorubicin and ifosfamide group , whereas at 2 years it was 28% ( 2234 ) and 31% ( 2538 ) , respectively . 
no signi cant di erence was noted between the groups in the per - protocol analysis ( p = 0057 )  . the doxorubicin and median progression - free survival was signi cantly higher ifosfamide group ( 74 months , 95% ci 6683 ) than in the doxorubicin group ( 46 months , 95% ci 2956 ; hr 074 , 955% ci 060090 , strati ed log - rank test p = 0003 ; gure 2b )  . 
figure 3 also shows a bene t of combination treatment for patients aged 4049 years , which might have been a result of statistical imbalances for this age groupboth for performance status and the tumour gradewhich combination treatment group ( data not shown )  . 
best overall response to treatment di ered signi cantly between the two groups in favour of doxorubicin and ifosfamide ( 31 [ 14% ] of patients in the doxorubicin group and 60 [ 26% ] in the doxorubicin and ifosfamide group had an overall response ; test , p = 00006 )  . the occurrence of toxic e ects di ered between treatment groups . 
roughly half of all patients completed six cycles of treatment , 102 ( 45% ) of 228 patients with doxorubicin and 115 ( 51% ) of 227 with doxorubicin and ifosfamide . 
those taking doxorubicin and ifosfamide were more likely than those taking doxorubicin only to need a dose reduction ( 71 [ 32% ] of 224 patients vs 20 [ 9% ] of 223 had a reduction of doxorubicin ; 84 [ 38% ] of 224 had a reduction of ifosfamide )  . 
likewise , treatment interruptions were more common in patients taking the combination compared with the single drug treatment ( 15 [ 7% ] of 224 vs ve [ 2% ] of 223 needed interruption of doxorubicin , 17 [ 8% ] of 224 required interruption of ifosfamide )  . 
 however , treatment discontinuation because of disease progression occurred more often in those who received doxorubicin only than in those who received doxorubicin and ifosfamide ( table 4 )  . than grade 34 adverse events were signi cantly more prevalent in patients treated with doxorubicin and ifosfamide than in those treated with doxorubicin only ( table 5 , appendix lists all grades )  . 
 likewise , grade 2 and grade 3 vomiting was more common in the doxorubicin and ifosfamide group ( 53 [ 24% ] and 13 [ 5% ] , respectively ) compared with the doxorubicin group ( 32 [ 14% ] and six [ 3% ] , respectively )  . 
despite the toxic e ects associated with doxorubicin and ifosfamide , toxic deaths occurred in much the same proportion in each group ( table 2 )  . hr 083 , 955% ci 067103 ; p = 0076 228 227 170 197 113 130 number at risk doxorubicin doxorubicin and ifosfamide hr 074 , 955% ci 060090 ; p = 0003 time ( months ) number at risk doxorubicin doxorubicin and ifosfamide 228 227 104 149 figure 2 : kaplan - meier curves for overall survival ( a ) and progression - free survival ( b ) hr = hazard ratio . post - protocol treatment did not di er substantially between groups other than that patients treated with doxorubicin were more likely to receive subsequent ifosfamide than were those who received doxorubicin and ifosfamide ( table 6 )  . 
once patients progressed while taking study treatment , investigators were required to collect only survival data . discussion we found no improvement in overall survival from the administration of intensi ed combination chemotherapy ifosfamide compared with with doxorubicin plus doxorubicin alone . 
most data for high - dose combinations come from single - centre phase 2 studies of highly selected groups of patients.1214 few randomised studies have been done , mostly with a dose of dose of 5 g / m , none of which have shown a survival advantage ( panel )  . 
 doxorubicin , for example , a randomised trial20 done by the eortc soft tissue and bone sarcoma group compared doxorubicin alone with a combination of doxorubicin and ifosfamide 5 g / m or a four - drug regimen of cyclophosphamide , and vincristine , dacarbazine . 
the combination treatments did not signi cantly increase the proportion of patients who responsed , progression - free survival , or overall survival and were signi cantly more toxic than the single drug treatment.20 a phase 3 study comparing single - agent doxorubicin with a combination of doxorubicin with either ifosfamide 75 g / m , or mitomycin and cisplatin showed a greater proportion of responses with combination treatment but no di erence in survival.21 similarly , a comparing doxorubicin plus dacarbazine with or without ifosfamide , for treatment of soft - tissue sarcoma and bone sarcoma also showed a signi cantly greater proportion of responses and longer progression - free survival , but no survival advantage , for the ifosfamide - containing regimen than for the regimen without ifosfamide . trial22 other studies have investigated the role of dose intensi cation . 
for example , a randomised phase 2 trial of ifosfamide 6 g / m versus 12 g / m with doxorubicin showed no advantage for disease - free survival or overall survival for the higher dose.23 dose intensi cation of the 420 vol 15 april 2014 articles progression of disease or death caused by progressive disease 95 ( 42% ) toxic e ect ( including toxic death ) toxic death patients refusal ( not related to toxic e ects ) intercurrent death ( not related to malignant disease or toxic e ects ) other data are n ( % )  . table 4 : reasons for discontinuation of treatment doxorubicin group ( n = 228 ) doxorubicin and ifosfamide group ( n = 227 ) 6 ( 3% ) 5 ( 2% ) 4 ( 2% ) 4 ( 2% ) 12 ( 5% ) 47 ( 21% ) 40 ( 18% ) 2 ( 1% ) 10 ( 4% ) 1 ( < 1% ) 11 ( 5% ) doxorubicin , ifosfamide , and dacarbazine regimen originally developed in the late 1980sproduced no improvement in responses , progression - free survival , or overall survival compared with the standard dose regimen.24 a phase 3 trial of dose intensi cation of doxorubicin ( 75 mg / m vs 50 mg / m ) with ifosfamide 5 g / m showed no improvement in responses or overall survival , but did show a longer progression - free survival for patients taking the higher dose of doxorubicin.25 other studies of dose intensi cation showed no advantage compared with doxorubicin alone.26 , 27 two meta - analyses of dose - intensive chemotherapy and ifosfamide - based chemotherapy have combination provided the same conclusion.28 , 29 in this context , our study was uniquely powered for overall survival as the primary endpoint . 
however , we did note a signi cant 28 month improvement in median progression - free survival with the dose - intensi ed regimen , and a greater proportion of patients responded to the combination therapy than to doxorubicin alone . intravenous the study was not masked , which might have biased the assessment of response and disease progression . 
as in most previous studies , combination treatment was signi cantly more toxic than the single - drug regimen , but there was no excess of toxic deaths . the proportion of patients who had a response in both groups was lower than reported in somebut not all previous eortc studies , 10 , 11 and lower for the combination than that reported in single - centre studies.1214 eligible patients had to have high grade disease and progression within 6 weeks of study entry ; thus , the prognosis for participants was poor . 
however , the high proportion of patients with synovial sarcoma suggests that such a bias did not have a major role . how can these data be used to guide clinical practice ? if palliative chemotherapy is being given to control metastatictypically pulmonarydisease , rather than to relieve acute symptoms , then sequential single - drug chemotherapy will probably be less toxic without signi cantly impairing survival . 
conversely , if acute symptoms are best relieved by tumour shrinkage , the use of combination treatment would be justi ed ; likewise , if is being given before surgery or chemotherapy doxorubicin group ( n = 223 ) doxorubicin and ifosfamide group ( n = 224 ) 83 ( 37% ) 40 ( 18% ) 30 ( 13% ) 10 ( 4% ) 1 ( < 1% ) 93 ( 42% ) 97 ( 43% ) 103 ( 46% ) 78 ( 35% ) 75 ( 33% ) neutropenia leucopenia febrile neutropenia anaemia thrombocytopenia data are n ( % )  . 
clinical situations might also exist for which delaying disease progression for as long as possible is the priority ; for example , if adjacent critical structures such as nerves are involved . 
although some older patients can vol 15 april 2014 articles panel : research in context systematic review we searched pubmed for reports published in english from jan 1 , 1983 , to jan 1 , 2014 , for all randomised trials assessing dose intensi cation for treatment of soft - tissue sarcoma with the terms : randomis ( z ) ed , trial ( s ) , advanced , soft tissue , sarcoma ( s ) , ifosfamide , and doxorubicwe found eight randomised trials2027 and two metaanalyses.28 , 29 our search also returned single group and randomised phase 2 trials of higher dose treatment . 
combination treatment has been shown to improve the proportion of patients who responded and progression - free survival but not overall survival in some , but not all trials.22 , 25 , 26 interpretation in our study both doxorubicin and ifosfamide doses were higher than those used in previous randomised trials . 
if the goal of treatment is disease control , doxorubicin alone remains an appropriate treatment but combination treatment can be justi ed if tumour shrinkage is desired , either to relieve symptoms or before another intervention . 
the lack of improvement in overall survival shows the need for better treatments for advanced soft tissue sarcoma . tolerate intensive combination treatment , the regimen we used is very myelosuppressive , therefore our data cannot be extrapolated to patients older than 60 years . these data should also be considered in the context of the diversi cation of chemotherapy and other systemic treatment that is taking place in the management of softtissue sarcoma . 
pazopanib has recently been approved for the treatment of soft - tissue sarcoma on the basis of its e ect on progression - free survival.32 nevertheless , an urgent need still exists for treatment that improves survival in patients with advanced disease . contributors ij wrote the protocol , reviewed all the case record forms for eligibility and protocol violations , recruited patients , and wrote and edited the report with sl . 
all authors reviewed the nal version of the report . declaration of interests we have no competing interests . acknowledgments we thank anne kirkpatrick and the other sta at eortc headquarters who contributed to the success of the trial . 
we acknowledge nhs funding to the royal marsden / icr national institute for health research biomedical research centre and researchers at the nihr university college london hospitals biomedical research centre . 
the eortc received nancial support from amgen for the cost of peg lgrastithe contribution of ncic clinical trials group was supported by the canadian cancer society research institute ( grant 021039 )  . correction to lancet oncol 2020 ; 21 : 64554 correction to lancet oncol 2020 ; 21 : 144354 correction to lancet oncol 2020 ; 21 : e51927 smith i , robertson j , kilburn l , et al . 
 long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial . 
lancet oncol 2020 ; 21 : e51927in this review , the second sentence of the first paragraph of the section entitled cancer burden now describing the number of new cancer cases worldwide in 2017 should read according to analysis from the global burden of disease study , there were 168 million new cases of cancer . 
this correction has been made to the online version as of nov 30 , 2020 . correction to lancet oncol 2020 ; 21 : 156373 powles t , plimack er , soulires d , et al . 
pembrolizumab plus axitinib versus sunitinib monotherapy as firstline treatment of advanced renal cell carcinoma ( keynote - 426 ) : extended follow - up from a randomised , openlabel , phase 3 trial . 
lancet oncol 2020 ; 21 : 156373in table 1 of this article the n ( % ) for previous nephrectomy should read 357 ( 83% ) for the pembrolizumab plus axitinib group and 358 ( 83% ) for the sunitinib group . 
these corrections have been made to the online version as of nov 30 , 2020 , and the printed version is correct . correction to lancet oncol 2020 ; 21 : e30516 fangusaro j , witt o , herniz driever p , et al . 
the aim of this study was to assess the relative importance of di erent risk factors for treatment - emergent joint symptoms in patients assigned to anastrozole or tamoxifen as adjuvant treatment for postmenopausal breast cancer . methods the arimidex tamoxifen alone or in combination ( atac ) trial randomly assigned 9366 postmenopausal women to anastrozole ( 1 mg / day ) , to tamoxifen ( 20 mg / day ) , or to a combination of both . 
our analyses were based on data from case reports of 5433 women who were randomly assigned to anastrozole or tamoxifen , who started with their allocated treatment , and who did not have joint symptoms at entry ( anastrozole group : n = 2698 ; tamoxifen group : n = 2735 )  . 
joint symptoms were de ned as any report of arthralgia , arthrosis , arthritis , or joint disorder on a case - report forjoint disorders were de ned as reports of cervical spondylosis , osteoarthritis , and disc herniation . 
the atac trial is registered as an international standard randomised controlled trial , number isrctn18233230 . findings 777 of 1914 women ( 406% ) who used hormone replacement therapy ( hrt ) before trial entry developed joint symptoms compared with 1001 of 3519 women ( 284% ) without previous hrt use ( odds ratio [ or ] 172 [ 95% ci 153193 ] )  . 
women with hormone - receptor - negative breast cancer developed signi cantly fewer joint symptoms compared with those with hormone - receptor - positive tumours ( 124 of 461 [ 269% ] vs 1556 of 4548 [ 342% ] ; or 071 [ 057088 ] )  . 
women for whom chemotherapy was part of their initial treatment developed signi cantly more joint symptoms than those who did not receive it ( 461 of 1219 women [ 378% ] vs 1317 of 4214 women [ 313% ] ; or 134 [ 117153 ] )  . 
all signi cant risk factors from the univariate analysis were included in a multivariate analysis and remained signi cant with little change . interpretation in this trial , the major risk factors for developing joint symptoms were previous hrt , hormonereceptor positivity , previous chemotherapy , obesity , and treatment with anastrozole . 
discussion of identi ed risk factors is appropriate when counselling women before initiation of adjuvant hormonal treatment . funding this study was funded by cancer research uk and astrazeneca ( maccles eld , uk )  . introduction oestrogen de ciency has been associated with joint symptoms ( eg , arthralgia and arthritis ) in several di erent settings . 
in the general population , postmenopausal status and low oestrogen concentrations are associated with the development of joint pain and joint symptoms.1 , 2 these symptoms are most prominent around the ages of 50 to 59 years , 1 , 2 are more common in postmenopausal women than in premenopausal and perimenopausal women of the same age , 3 and often improve during use of hormone replacement therapy ( hrt ) .4 , 5 further evidence linking joint symptoms with decreased oestrogen concentrations comes from adjuvant trials of aromatase inhibitors in patients with early breast cancer , where increased joint symptoms ( eg , arthralgia and arthritis ) have been noted for all three thirdgeneration aromatase inhibitors.68 women treated with chemotherapy for breast cancer have also shown joint symptoms and other joint or muscle - related problems.9 , 10 however , tamoxifen does not seem to have an e ect on joint symptoms . 
in the rst international breast cancer intervention study , 11 joint symptoms were similarly distributed between treatment groups in postmenopausal women ( 159 of 3579 women in the tamoxifen group vs 147 of 3575 women in the placebo group ; p = 05 )  . 
 table 1 : patients with joint symptoms by severity and treatment rst received for all women ( safety population ) and for those without joint symptoms at entry ( study population ) symptoms in the arimidex tamoxifen alone or in combination ( atac ) trial , 13 and assess whether these risk factors act di erently in the presence of anastrozole treatment . 
 methods the atac trial13 was a double - blind randomised clinical trial in which postmenopausal women with early breast cancer were randomly assigned to oral daily anastrozole ( 1 mg ) alone , tamoxifen ( 20 mg ) alone , or a combination of both in a double - blind fashion , so that each woman took two tablets , at least one of which was active . 
 only women who started with their randomly assigned treatment and who did not report joint symptoms at entry were included in this analysis ( anastrozole group : n = 2698 ; tamoxifen group : n = 2735 )  . 
our analysis was based on the 100 - month median follow - up data set , at which point all patients had completed their study medication.14 because most symptoms occurred relatively early , and the e ects of treatment and other variables were not constant with time , the analysis was restricted to the occurrence of joint symptoms at any time during active treatment or within 14 days of its discontinuation . 
joint symptoms were de ned as any report of arthralgia , arthrosis , arthritis , or joint disorder ( coding symbols for a thesaurus of adverse reaction terms ) 15 on a case - report for joint disorders were de ned as reports of cervical spondylosis , anastrozole tamoxifen number at risk anastrozole tamoxifen 2698 2735 follow - up time ( years ) 2239 2372 1950 2085 1710 1859 1534 1656 1354 1464 figure 1 : patients ( % ) developing joint symptoms at or before a speci ed follow - up time during active treatment according to treatment rst received in women without joint symptoms at entry ( study population ) osteoarthritis , and disc herniation . 
for the atac trial , all side - e ect data were the result of elicited responses recorded on case - report forms and a speci c symptom check list was not used . 
interactions between treatment and subgroups were based on likelihood ratio tests for an added interaction terhazard plots were smoothed by use of an epanechnikov kernel with the optimum bandwidth chosen by cross validation.16 all p values are two - sided , with level of signi cance set at 005 , and all con dence intervals are at the 95% level . 
394 women in the anastrozole group and 359 women in the tamoxifen group ( or 090 [ 077105 ] ) reported a history of joint symptoms at entry into the trial . 
figure 1 shows the higher prevalence of joint symptoms reported by women without a history of joint symptoms at study entry in the anastrozole group compared with the tamoxifen group . 
in both treatment groups , most joint symptoms were of mild or moderate severity , and the intensity of symptoms was similarly distributed in both treatment groups ( table 1 )  . 
1067 of 1778 patients ( 60% ) who reported joint symptoms received treatment , with 960 of these patients ( 90% ) using a non - steroidal anti - in ammatory drug alone or in combination with a mild analgesic . potential risk factors for developing joint symptoms are shown for each treatment group in table 2 . 
after exclusion of women with baseline joint symptoms , 949 of 2698 women ( 352% ) reported joint symptoms in the anastrozole group compared with 829 of 2735 women ( 303% ) in the tamoxifen group ( or 125 [ 95% ci 111140 ; p < 00001 ] ; table 3 )  . 
for women who previously used hrt , 777 of 1914 ( 406% ) developed joint symptoms compared with 1001 of 3519 women ( 284% ) without previous hrt use ( or 172 [ 153193 ] ; p < 00001 )  . 
joint symptoms were increased by a similar amount for women who stopped hrt less than 6 months before trial entry compared with those who stopped hrt more than 6 months before entry ( 502 of 1201 women ( 418% ) vs 142 of 335 women ( 424% ) ; or 108 [ 084140 ] ; p = 054 )  . 
 women with hormone - receptor - negative breast cancer developed signi cantly fewer joint symptoms than those with hormone - receptor - positive tumours ( 124 of 461 ( 269% ) vs 1556 of 4548 ( 342% ) ; or 071 [ 057088 ] ; p = 0002 ; table 3 )  . 
 * north america = usa and canada . table 2 : selected baseline characteristics ( % ) according to treatment group ( study population ) role of the funding source this study was funded by cancer research uk and astrazeneca ( maccles eld , uk )  . 
 when all signi cant variables in the univariate models were entered into a multivariate model , the odds ratios were similar to the univariate ndings , except for smoking status , which became non - signi cant ( table 3 )  . 
 similar ndings for the univariate and multivariate analyses of risk factors were obtained if the population was restricted to hormone - receptor - positive women ( data not shown )  . 
additionally , there were no signi cant interactions of any factors with treatment , except for a weak interaction between treatment and previous hrt use ( pinteraction = 005 ; table 4 )  . 
 women from the usa and canada ( grouped as north america ) reported signi cantly more joint symptoms than those from the uk or the reference group of the rest of the world ( 738 of 1611 ( 458% ; or 244 [ 212280 ] ; p < 00001 ) vs 523 of 1815 ( 288% ; or 117 [ 101135 ] ; p = 003 ) vs 517 of 2007 ( 258% ) ; table 3 )  . 
data missing for 245 patients . table 4 : number ( % ) of women reporting joint symptoms at any time during treatment according to treatment rst received and selected risk factors in women without joint symptoms at entry ( study population ) no signi cant interactions of key variables in the univariate model were seen with region in the multivariate model ( data not shown )  . 
 discussion in this trial , the major risk factors for developing joint symptoms in women not reporting them at entry were previous hrt use , hormone - receptor positivity , previous chemotherapy , obesity , and treatment with anastrozole versus tamoxifen , leading to signi cant absolute increases of 121% , 73% , 65% , 62% , and 49% , respectively . 
women with pre - existing joint symptoms were excluded from this analysis to focus on new treatment - emergent symptoms . the e ect of previous hrt was especially striking , which could be because most women previously using hrt , for whom we had data , came o it within 6 months before entry into the study ( 1201 of 1536 women [ 782% ] ) , although the e ect was similar in women who had stopped their hrt treatment earlier . 
furthermore , the e ects of hrt seemed to be additive , resulting in an 181% increase in joint symptoms in women who previously used hrt and were on anastrozole compared with those on tamoxifen with no previous hrt use . 
 recent users of hrt ( ie , those who stopped use less than 6 months ago ) are likely to have a greater decrease in oestrogen concen trations with endocrine treatment than those who stopped use more than 6 months ago , and most , 17 , 18 but not all studies , 19 have shown that they are more likely than never users to have oestrogen - receptorpositive tumours . 
in our study , women with hormonereceptor - positive tumours reported more joint symptoms than those with hormone - receptor - negative tumours , but , paradoxically , the few women with tumours of unknown hormone - receptor status had the lowest number of joint symptoms . 
several studies have shown that women with high oestrogen concentrations are more likely to develop oestrogen - receptor - positive tumours than those with low oestrogen concentrations.20 , 21 obese women tend to have higher oestrogen concentrations than non - obese women as a result of aromatisation from the adipose tissue , 22 so the decrease in oestrogen concentration is likely to be greater in this group as well . 
obesity itself is also a risk factor for joint symptoms independent of endocrine treatment.23 however , crew and colleagues24 reported that women with a bmi between 25 and 30 kg / m developed fewer joint symptoms than those with a lower bmi . 
 chemotherapy is well known to induce arthralgia or myalgia and has been reported in several trials independently of endocrine treatment.10 , 2527 chemo therapy is known to damage ovarian function in premeno pausal women , and the e ects seen here could be a result of the ablation of any residual ovarian production of oestrogen in these postmenopausal women . 
again , the ndings were additive in anastrozole users so that the use of previous chemotherapy and anastrozole together resulted in a 124% increase in joint symptoms when compared with women on tamoxifen without previous chemo therapy . reports have suggested that side - e ects , such as joint symptoms , are under - reported in clinical trials compared with patient - recorded side - e ects.28 , 29 the atac trial was an international study , involving 21 countries . 
because of the nature of the collection , in which uniform de nition of symptoms was not provided , subcategories of joint symptoms were not thought to be reliable and were , therefore , not reported during the atac trial . 
additionally , the duration of symptoms and date of resolution of symptoms could not be assessed in detail , because data were collected at 3 months , 6 months , and at 6 - monthly intervals thereafter , so dates within these intervals were not recorded . 
because the study was blinded , there would have been no bias in relative rates , but the overall reporting rates for speci c symptoms could have been a ected . 
however , this approach did seem to be sensitive , because known minor side - e ects , and some previously unknown ones , were clearly detectable.30 the symptoms were assessed by clinicians and mapped to the relevant costart 870 vol 9 september 2008 articles terms.15 this ascertainment of joint symptoms needs to be taken into account when interpreting these ndings . 
 by contrast , a higher drop - out rate caused by joint symptoms was reported in two smaller uncontrolled studies , 31 , 32 but it is di cult to attribute all these events to an aromatase inhibitor , because joint symptoms are common in postmenopausal women ( eg , 31% of women receiving tamoxifen in the atac trial reported joint symptoms )  . the increased incidence of joint symptoms in the north american population is most probably consistent with di erent practices for recording symptoms . 
 although more patients had previous hrt use , previous chemotherapy , and a higher bmi in north america , compared with the uk and the rest of the world , the e ects of region were only slightly diminished when they were adjusted for in the multivariate model . 
 no signi cant interactions between region and risk factors were identi ed , suggesting that the di erences noted between regions were most probably due to di erent thresholds for reporting these symptoms in north america , especially because adverse events overall were more often reported in north american participants . in conclusion , several factors other than treatment with anastrozole were associated with the development of joint symptoms in this trial . 
joint symptoms were generally of mild to moderate intensity and for most women they do not override the clear bene ts of anastrozole over tamoxifen in terms of decreased recurrence and fewer other major side - e ects , including and gynaecological complications ( eg , endometrial cancer ) .14 however , for women with serious side - e ects on anastrozole , remains a viable option . 
 awareness of risk factors for joint symptoms will help both clinicians and patients to anticipate and manage these symptoms and ensure optimum adherence to endocrine treatment . thromboembolic tamoxifen venous events con icts of interest is declared no con icts of interest . 
all contributors took part in writing the paper and approved the nal version . acknowledgments this research was supported by cancer research uk and astrazeneca ( maccles eld , uk )  . 
we also thank the trial investigators , other supporting sta , and the members of the international steering committee . re ection and reaction panel : ten principles for a bill of rights for patients with cancer all patients , irrespective of domicile , have a right of access to : 1 high - quality , patient - focused cancer services that are commissioned , accredited , and monitored according to national standards 2 optimum cancer care , based on clinical needs and irrespective of means within the resources available 3 management by a multidisciplinary team of accredited cancer professionals in an environment of patientfriendly care 4 timely and sensitively delivered care according to national standards 5 evidence - based diagnostic treatment and supportive care that meet national standards at a location as close to place of domicile as is clinically appropriate 6 provision and maintenance of high - quality cancer registration , clinical notes , and clinical outcome data 7 equitable access to new developments in diagnosis and treatment 8 comprehensive information about treatment options 9 information about the compliance with quality standards of the commissioning and delivery of cancer services relating to the cancer network in which they are managed 10 right of redress if provision of care falls below national standards was adopted , alternative co - payment schemes and health insurance ( advocated by some commentators ) , 6 might also need to be considered to meet public expectation of cancer care as nhs investment falls beyond 2008 . how can the continued improvements in cancer services be sustained in the long - term , despite nhs reforms and changes in government and funding mechanisms ? one possibility would be a bill of rights for patients with cancer ( panel ) , which could apply to patients managed in either state or private sectors ( or both )  . 
since public support for cancer as a nhs priority is greater than that for any other disease , it is likely that such a bill would be supported by the electorate . 
the times ( london ) , april 4 , 2006 : 18 . erratum steven a narod , jan lubinski , parviz ghadirian , et al , for the hereditary breast cancer clinical study group . 
in this article , the authors surname domcheck should have been spelt domchek throughout . and their bene ts and risks i declare no con icts of interest . vol 7 june 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology corrections correction to lancet oncol 2014 ; 15 : 933 , 941 correction to lancet oncol 2014 ; 15 : 96674 correction to lancet oncol 2012 ; 13 : 1261 , 1263 denham jw , wilcox c , joseph d , et al . 
 quality of life in men with locally advanced prostate cancer treated with leuprorelin and radiotherapy with or without zoledronic acid ( trog 03.04 radar ) : secondary endpoints from a randomised phase 3 factorial trial . 
 lancet oncol 2014 ; 15 : 96674 for supplementary appendix the this article has been resupplied to include a table of treatment - emergent adverse events of grade 4 or higher . 
 the rst sentence of ninth paragraph of the results section now reads grade 3 or higher events reported in more than 5% of siltuximab - treated patients were fatigue and night sweats and , in participants receiving placebo , anaemia ( table 3 ) ; treatmentemergent adverse events of grade 4 or higher are shown in the appendix . 
 lancet oncol 2014 ; 15 : 93142in table 1 of this article , 176 ( 81% ) patients were available for survival analysis for hodgkins lymphoma in sassari , italy . 
these corrections have been made to the online version as of sept 1 , 2014 . correction to lancet oncol 2014 ; 15 : 957 melanoma : vemurafenib ribas a , gonzalez r , pavlick a , et al . 
lancet oncol 2014 ; 15 : 95465in the section on most common adverse events in table 3 of this article , the number of patients who had recently progressed on vemurafenib who had any grade photosensitivity or sunburn should read 10 ( 15% ) , and the number of patients who had never received a braf inhibitor with any grade photosensitivity or sunburn should read 42 ( 67% )  . 
 * three patients did not have an initial testosterone value . table 1 : characteristics of the 1071 randomly assigned patients and their tumours vol 15 september 2014 e417 articles sensitivity of transvaginal ultrasound screening for endometrial cancer in postmenopausal women : a case - control study within the ukctocs cohort ian jacobs , aleksandra gentry - maharaj , matthew burnell , ranjit manchanda , naveena singh , aarti sharma , andy ryan , mourad w seif , nazar n amso , gillian turner , carol brunell , gwendolen fletcher , rani rangar , kathy ford , keith godfrey , alberto lopes , david oram , jonathan herod , karin williamson , ian scott , howard jenkins , tim mould , robert woolas , john murdoch , stephen dobbs , simon leeson , derek cruickshank , steven j skates , lesley fallow eld , mahesh parmar , stuart campbell , usha menon summary background the increase in the worldwide incidence of endometrial cancer relates to rising obesity , falling fertility , and the ageing of the population . 
we report the performance of tvs screening in a large cohort . methods we did a nested case - control study of postmenopausal women who underwent tvs in the united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) following recruitment between april 17 , 2001 , and sept 29 , 2005 . 
 our study is registered with clinicaltrials.gov , number nct00058032 , and with the international standard randomised controlled trial register , number isrctn22488978 . findings 48 230 women underwent tvs in the ukctocs prevalence screen . 
9078 women were ineligible because they had undergone a hysterectomy and 2271 because their endometrial thickness had not been recorded ; however , 157 of these women had an endometrial abnormality on tvs and were included in the analysis . 
the optimum endometrial thickness cuto for endometrial cancer or aeh was 515 mm , with sensitivity of 805% ( 95% ci 727868 ) and speci city of 862% ( 858866 )  . 
sensitivity and speci city at a 5 mm or greater cuto were 805% ( 727868 ) and 857% ( 854862 ) ; for women with a 5 mm or greater cuto plus endometrial abnormalities , the sensitivity and speci city were 853% ( 782908 ) and 804% ( 800808 ) , respectively . 
when our analysis was restricted to the 96 women with endometrial cancer or aeh who reported no symptoms of postmenopausal bleeding at the ukctocs scan before diagnosis and had an endometrial thickness measurement available , a cuto of 5 mm achieved a sensitivity of 771% ( 678843 ) and speci city of 858% ( 857859 )  . 
the logistic regression model identi ed 25% of the population as at high risk and 395% of endometrial cancer or aeh cases were identi ed within this high risk group . 
in this high - risk population , a cuto at 675 mm achieved sensitivity of 843% ( 714930 ) and speci city of 899% ( 893905 )  . interpretation our ndings show that tvs screening for endometrial cancer has good sensitivity in postmenopausal women . 
 additional factors are mortality greater than 30% within 10 years of diagnosis10 and a proven link between stage and survival raising the possibility of a mortality bene t from earlier detection.10 of note , stage for stage , survival rates for endometrial cancer are similar to ovarian cancera cancer for which large - scale screening trials are underway.11 , 12 to assess the endometrium in symptomatic women are tvs and endometrial sampling . 
other studies1416 have included smaller populations , making the to assess sensitivity of screening , or to achieve con dent estimates of speci city or positive predictive value . techniques commonly used impossible the the opportunity to study the performance of tvs in a large cohort of postmenopausal women was provided by data from the united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) .12 , 17 ukctocs is a prospective trial of ovarian cancer screening , one arm of which involved pelvic ultrasound during which endometrial thickness was measured and recorded . 
we report on the characteristics of endometrial cancer screening in postmenopausal women in the general population to inform on the potential of screening for endometrial cancer . methods participants we did a nested case - control study within the ukctocs cohort with ultrasound ndings recorded at yearly screening appointments as part of the ovarian cancer screening trial . 
the pre - identi ed scottish centres dropped out because of logistical issues ( lack of space , retirement of potential research leads , unwillingness of nhs trust management to commit to a 10 - year trial , involvement in other ovarian cancer screening trials ) .17 participants completed a recruitment questionnaire , which requested baseline data on lifestyle and reproductive factors , previous cancer history , and family history of breast or ovarian cancer.17 the focus of the recruitment questionnaire was on risk factors for ovarian cancer and the trial was not resourced to collect all variables related to endometrial cancer risk at the initial visit . 
 50 639 participants were randomly assigned to yearly screening with tvs ; 48 230 attended the initial prevalence screen and are included in our study . all women assigned to screening with tvs who had undergone the prevalence screen were included as cases or controls . 
cases were women with a con rmed diagnosis of endometrial cancer or atypical endometrial hyperplasia ( aeh ) , complex endometrial hyperplasia ( ceh ) , endometrial stromal sarcoma ( ess ) , or carcino sarcoma . 
we excluded from our study all women assigned to screening with tvs who had undergone hysterectomy before random assignment in ukctocs or who had no endometrial thickness measurement or endometrial abnormality on the relevant scan . 
 our study was covered by the ethical approval obtained for the main ukctocs ( mrec reference 00 / 8 / 34 , granted by north west mrec )  . recorded procedures tvs with kretz / medison sa9900 ( medison , seoul , south korea ) ultrasound machines was done by experienced ultrasonographers at the 13 trial centres in the uk . 
during the course of the trial , they completed an accreditation programme and attended yearly ultrasound days . the ultrasonographers were instructed to ask about and record symptoms of postmenopausal bleeding . 
we do not know how accurately postmenopausal bleeding was documented and there might have been a bias to better documentation in women who had an endometrial thickness above the level which prompted clinical referral ( > 5 mm ) according to current guidelines . 
in all women who reported that they had experienced any irregular bleeding to the sonographer , data were recorded on the ultrasound for during scanning , details of ovarian morphology and size were recorded . 
representative grey - scale images of each ovary and the uterus were archived at the coordinating centre.12 vol 12 january 2011 articles at tvs , endometrial thickness was measured at its thickest point from the anterior to the posterior in the sagittal plane of the uterus . 
callipers were placed perpendicular to the outer edge of the endometriuif there was uid in the endometrial cavity , the endometrial thickness was measured as above but with the inclusion of the cavity uid and the double endometrial stripe , then the uid diameter was subtracted at the same point . 
 for the purposes of our study , thickened , irregular , cystic , heterogeneous , distended endometrium ; uid in the endometrial cavity ; or polyp or other mass or lesion were included under the de nition of endometrial abnormality . abnormal , in clinical practice , asymptomatic women are not investigated . 
in the absence of any de nitive data at the start of the trial , a pragmatic decision to recommend referral of asymptomatic women with an endometrial thickness greater than 10 mm was agreed on the basis of extensive discussion and consultation with clinicians . 
we emphasise that there was no systematic protocol - driven intervention based on endometrial thickness . trial guidelines for the management of endometrial thickness stated that all women with thickness greater than 5 mm should be questioned about bleeding . 
in the this , uk national health service , postmenopausal bleeding prompts a 2 - week referral to assess for cancer , and all centres would have irrespective of followed measurements of endometrial thickness . 
data on any di erences between the centres are not yet available . all participants were followed up through a agging study with the nhs information centre for health and social care ( formerly o ce of national statistics ) in england and wales and via the central services agency and cancer registry in northern ireland as appropriate . 
 * includes those with personal history of breast cancer . table 1 : baseline characteristics of ukctocs participants who underwent the rst yearly scan vol 12 january 2011 articles women without ec or aeh n = 36 731 women with ec or aeh n = 133 relative risk ( 95% ci ) < 5 mm 30 664 ( 835% ) 5 to 10 mm 10 to 20 mm 20 mm mean ( sd ) 4878 ( 133% ) 1116 ( 30% ) 73 ( 02% ) 26 ( 195% ) 33 ( 248% ) 59 ( 444% ) 15 ( 113% ) median ( iqr ) 29 mm ( 2040 ) 110 mm ( 60145 ) 346 mm ( 259 ) 1153 mm ( 781 ) 793 ( 4771318 ) 5927 ( 37679336 ) 2012 ( 1106436063 ) data are n ( % ) unless otherwise indicated . 
aeh = atypical endometrial hyperplasia . table 2 : distribution of endometrial thickness measurements in women with or without endometrial cancer or atypical endometrial hyperplasia optimum = 515 mm optimum = 580 mm 1specicity 1specicity figure 1 : receiver operator curves for detection of endometrial cancer and atypical endometrial hyperplasia endometrial thickness measurements alone ( a ) and a combination of endometrial thickness measurements and endometrial abnormality ( b )  . 
data on the relevant variables for the ultrasound group were then inserted into the derived high - risk model and a prior risk probability of endometrial cancer was calculated solely on the basis of epidemiological data . 
these groups were based on the cuto s of the ordered prior risk probabilities : the highest risk ( rst ) quartile , the second quartile , the third quartile , and those at lowest risk ( fourth quartile )  . 
 relative risks ( rrs ) were used because the prevalence of endometrial cancer was virtually unchanged from the prevalence of endometrial cancer in the trial population for those without hysterectomy . ovarian volume was assessed as another variable to identify women at higher risk of endometrial cancer or aeh by comparing measurements of those who developed endometrial cancer or aeh and those who had not . the relative risk of endometrial cancer or aeh in women with thickness measurements of 5 mm or greater or 10 mm or greater were calculated to show the endometrial thickness cuto s suggested by the ukctocs guidelines . 
our study is registered with clinicaltrials.gov , number nct00058032 , and with the international standard randomised controlled trial register , number isrctn22488978 . follow - up , copies of operative notes , histopathology reports , cytology reports , discharge summaries , multidisciplinary team meeting notes , and other correspondence were obtained . 
the nal diagnosiswhich included the primary site , stage , and grade of any cancerwas made on review of the medical notes by an independent gynaecological oncologist ( rm )  . our primary outcome measure was endometrial cancer and aeh . 
aeh was included because 40% of cases of aeh might have concurrent ec , 18 there is limited concordance between pathologists on the diagnosis of aeh or endometrial cancer , 19 and aeh is a precancerous state with greater than 25% of patients progressing to endometrial cancer ( estimates range from 25% to 82% ) .2025 ess , carcinosarcoma , and ceh were also analysed separately . statistical analysis the distribution of endometrial thickness was compared in women who did and did not develop endometrial cancer or aeh . 
these data were used to construct a receiver operator characteristic ( roc ) curve to assess the speci city and sensitivity of various thickness cuto s for detecting endometrial cancer or aeh . 
a multivariate logistic - regression analysis was done that combined thickness with the baseline characteristics of the study participants to develop an algorithm incorporating epidemiological variables that would identify a high - risk group who might bene t from a targeted approach to screening . 
further roc curves were constructed to assess the speci city and sensitivity of various endometrial thickness cuto s for detecting endometrial cancer or aeh in the di erent risk groups . further analyses assessed the sensitivity and speci city pro le of endometrial thickness for the detection of endometrial cancers , either alone or combined with ceh , ess , or carcinosarcoma , with a scan done within a year of diagnosis . 
since systematic protocol - driven intervention based on endometrial thickness , we did not analyse the data by stage of endometrial cancer . to explore the possibility of re ning screening in a higher - risk group , the baseline characteristics recorded at recruitment for women diagnosed with endometrial cancer in the control and multimodal groups of the trial were modelled as epidemiological risk factors for endometrial cancer with forward stepwise logistic regression . 
these factors were weight ; age at menarche ; use of the oral contraceptive pill ; personal history of breast , ovarian , lung , bowel , or other cancer ; age at scan ; and any pregnancy of longer than 6 months vol 12 january 2011 articles role of the funding source the sponsor of the study and the funding sources had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
ag - m , mb , rm , ar , and um also had access to the raw data . results table 1 shows the baseline characteristics of the women with and without endometrial cancer or aeh . 
the inclusion criteria and details of the ukctocs trial have been described in detail elsewhere.12 , 17 50 639 study participants were randomly assigned to the ultrasound arm of ukctocs . 
the resulting group of 37 038 women were included in our study ( web appendix pp 56 )  . absence of endometrial median follow - up from the scan to cancer registration ( iqr 405595 )  . 
since update was 511 years information on cancers can take up to 3 years to be recorded on the national cancer registries , we explored other sources of follow - up data in detail in the 985 women for whom the time from scan to cancer registry followup on feb 9 , 2009 , was less than 3 years . 
in this cohort , we had additional con rmation of endometrial cancer status in 849 women because they had attended further screening and in 66 of the remaining women through returned follow - up questionnaires . 
in 70 of 37 038 women , the only source of information on endometrial cancer status was cancer registry follow - up of less than 3 years from the date of scan . [ 2% ] , three mixed subtype the cohort of 37 038 women includes 125 women who developed endometrial cancer after random assignment ( 100 endometrioid [ 80% ] , six papillary serous [ 5% ] , two clear cell [ 2% ] , one mucoid [ 1% ] , and 13 endometrial carcinoma without speci cation of histological subtype [ 10% ] ) , six with ess , six with carcinosarcomas or mixed mllerian tumours , 11 with aeh , and two with ceh . 
ess = endometrial stromal sarcoma . table 3 : performance characteristics of endometrial thickness as a screening tool for endometrial cancer with and without endometrial abnormality vol 12 january 2011 articles developed endometrial cancer after random assignment were stage 1 , 11 were stage 2 , nine were stage 3 , and one was stage 4 . 
overall , 112 of the 136 women with endometrial cancer or aeh were asymptomatic and 24 were symptomatic at the last ukctocs scan before diagnosis ( of 99 women with endometrial cancer or aeh who reported no postmenopausal bleeding , 96 had endometrial thickness measurements available )  . the remainder of the cohort is 36 888 controls , who are women without a diagnosis of endometrial cancer or aeh within 1 year of their last ukctocs scan . 
the control group includes six women who had either a leiomyosarcoma or breast cancer that was metastatic to the endometrium and 23 women who had endometrial cancer or aeh diagnosed more than 1 year after the last ukctocs scan . 
the 5% missing data rate is in keeping with what was anticipated for a study of this type and size . weight , age , and personal history of cancer were associated with an increased risk of endometrial cancer or aeh , although oral contraceptive pill , age at menarche , and parity were associated with a decreased risk ( webappendix p 1 )  . table 2 shows the distribution of endometrial thickness measurements in the 36 731 women who did not have a diagnosis of endometrial cancer or aeh . 
most of the women had an endometrial thickness of less than 5 m in the 133 women with a diagnosis of endometrial cancer or aeh who had endometrial thickness recorded , 107 ( 81% ) had an endometrial thickness of 5 mm or greater . 
the optimum cuto for endometrial thickness was 515 mm with a rr of 252 ( 95% ci 165385 )  . the webappendix ( p 2 ) shows the distribution of endometrial thickness measurements according to the use of hormone replacement therapy ( hrt ) in the overall cohort . 
the median endometrial thickness in women in the whole cohort who did not use hrt was 27 mm ( iqr 20395 ) versus 36 mm ( 2551 ) in women that did and these results were similar in the subgroup of women without endometrial cancer or aeh ( p < 00001 )  . 
by contrast , the median thickness was 110 mm ( 59148 without hrt ; 70145 with hrt ) in women with endometrial cancer or aeh , irrespective of the use of hrt . 1406 women reported breast cancer diagnosis before entry into the trial . 
these women were more likely to have an endometrial thickness of 5 mm or greater to less than 10 mm ( rr 191 ; 95% ci 168218 ) , 10 mm or greater to less than 20 mm ( 450 ; 385525 ) , and 20 mm or greater ( 1101 ; 8041447 ) than women with no history of breast cancer ( webappendix , p 3 )  . 
of the women with no history of breast cancer , 29 757 ( 839% ) of 35 460 had an endometrial thickness of less than 5 mm compared with 940 ( 669% ) of 1406 women with history of breast cancerthe median endometrial thickness was 29 mm versus 36 mm ( p < 00001 ; webappendix p 3 )  . 
 a large proportion of this measurement in women with breast cancer was probably related to tamoxifen use , but treatment data were not systematically captured as part of the trial . we did an analysis of endometrial thickness by screening centre in the women who did not develop endometrial cancer . 
the median endometrial thickness was 29 mthe median thickness varied from 21 mm number % ( 95% ci ) number % ( 95% ci ) number % ( 95% ci ) positive for bleeding negative for bleeding 5 mm cuto > 5 mm 5 mm sensitivity speci city > 10 mm 10 mm sensitivity speci city positive predictive value negative predictive value 10 mm cuto positive predictive value negative predictive value overall 31 464 35 746 805% ( 727868 ) 857% ( 854862 ) 20% ( 1821 ) 999% ( 999999 ) 541% ( 453628 ) 972% ( 970974 ) 64% ( 5474 ) 998% ( 998999 ) 892% ( 769956 ) 422% ( 386440 ) 308% ( 266331 ) 931% ( 852972 ) 649% ( 510767 ) 773% ( 734808 ) 453% ( 357535 ) 884% ( 838923 ) 31 410 35 586 771% ( 678843 ) 858% ( 857859 ) 14% ( 1215 ) 999% ( 999100 ) 500% ( 403597 ) 972% ( 971973 ) 45% ( 3654 ) 999% ( 998999 ) table 4 : performance characteristics of endometrial thickness as a screening tool for endometrial cancer in women with and without postmenopausal bleeding vol 12 january 2011 articles optimum = 675 mm optimum = 485 mm optimum = 575 mm optimum = 465 mm 1specicity 1specicity figure 2 : receiver operator curve for endometrial thickness measurements for detection of endometrial cancer in the high - risk group first quartile ( a ) , second quartile ( b ) , third quartile ( c ) , and fourth quartile ( d )  . 
when dichotomised as endometrial thickness less than 5 mm and 5 mm or greater , the proportion of measurements greater than 5 mm per centre varied from 104% to 224% ( overall proportion 168% ; median centre proportion 166% , iqr 147198 )  . to assess the sensitivity and speci city pro le for detection of endometrial cancer or aeh , a roc curve was constructed with cuto points for endometrial thickness with or without data for endometrial abnormalities ( gure 1 , webappendix p 4 )  . 
our subgroup analyses that included endometrial cancer and aeh or a combination of endometrial cancer , aeh , ceh , and ess or carcinosarcoma showed similar levels of sensitivity and speci city . given the di erence noted in endometrial thickness distribution in users of hrt and non - users , the optimum cuto in hrt users was as expected higher ( 685 mm ) than non - users ( 455 mm ; table 3 )  . at the ukctocs scan , postmenopausal bleeding was recorded in 165 women ( 37 cases and 128 controls )  . 
table 4 shows the performance characteristics for women with and without postmenopausal bleeding . the relation between ovarian volume and endometrial cancer or aeh was assessed and no statistically signi cant correlation was identi ed ( p = 0956 ; data not shown )  . we explored the possibility of optimising approaches to endometrial cancer screening by incorporating epidemiological information provided in the recruitment questionnaire . 
logistic regression showed that decreased endometrial cancer or aeh risk was associated with the use of the oral contraceptive pill , age at menarche , and pregnancies longer than 6 months , while increased risk was associated with rising weight , increasing age , and personal history of breast and other cancer ( multivariate and univariate analyses are shown in webappendix p 1 )  . 
 on the basis of the logistic regression model , the population could be divided into quartiles with rrs for endometrial cancer compared with the entire population of 198 ( 139280 ) for the rst quartile , 107 ( 073158 ) for the second , 076 ( 049116 ) for the third , and 049 ( 030079 ) for the fourth ( table 5 )  . 
the population in the highest quartile of risk ( rst quartile ) included 395% of women with endometrial cancer or aeh ; in this population an optimum endometrial thickness cuto at 675 mm achieved a sensitivity of 843% and speci city of 899% ( gure 2 , table 5 )  . if endometrial we also assessed the number of further interventions that would be predicted thickness measurements were used as a screen for endometrial cancer or aeh ( table 6 )  . 
if the entire population were screened , an endometrial thickness cuto of 5 mm or greater would result in 58 women undergoing further investigation per case of endometrial cancer or aeh detected for the diagnosis of 805% ( 107 of 133 ) of cancers . 
 a cuto of 10 mm or greater , would lead to 17 women being investigated to detect each case of endometrial cancer ( 556% [ 74 of 133 cancers diagnosed ] )  . 
if the proportion of the population screened was reduced by the use of our logistic regression model to limit screening to the top quartile risk group , 22 women would have to undergo investigation per endometrial cancer detected for the detection of 43 ( 323% ) cases in the entire population . vol 12 january 2011 articles number of cases / controls proportion of cases included rr of ec ( 95% ci ) area under curve ( 95% ci ) > 5 mm et cuto > 10 mm et cuto optimum cuto first quartile second quartile third quartile fourth quartile 51 / 9015 395% 34 / 9081 264% 26 / 9104 202% 18 / 9115 140% 198 ( 139 280 ) 107 ( 073 158 ) 076 ( 049 116 ) 049 ( 030 079 ) 0902 ( 0848 0957 ) 0878 ( 0808 0948 ) 0744 ( 0623 0865 ) 0969 ( 0947 0991 ) sensitivity ( 95% ci ) speci city ( 95% ci ) sensitivity ( 95% ci ) speci city ( 95% ci ) cuto sensitivity ( 95% ci ) speci city ( 95% ci ) 0863 ( 0737 0943 ) 0794 ( 0621 0913 ) 0615 ( 0406 0798 ) 0944 ( 0727 0999 ) 7546 0837 ( 0829 0845 ) 7846 0864 ( 0857 0871 ) 7839 0861 ( 0854 0868 ) 7948 0872 ( 0865 0879 ) 0627 ( 0481 0759 ) 0471 ( 0298 0649 ) 0385 ( 0202 0594 ) 0667 ( 0410 0867 ) 8654 8863 8867 8914 0960 ( 0956 0964 ) 0976 ( 0973 0979 ) 0974 ( 0970 0977 ) 0978 ( 0975 0981 ) 485 mm 28 7574 675 mm 43 465 mm 17 575 mm 17 0843 ( 0714 0930 ) 0824 ( 0655 0932 ) 0654 ( 0443 0828 ) 0944 ( 0727 0999 ) 8104 0899 ( 0893 0905 ) 0834 ( 0826 0842 ) 7456 0819 ( 0811 0827 ) 8194 0899 ( 0893 0905 ) n = number . 
when we assessed this in our cohort , we found that for the left ovary , the use of the suggested cuto of 3 cm , the p value was 0063 and for the right ovary p was 0218 . discussion ultrasound imaging of the endometrium has long been thought a possible screening test for endometrial cancer . 
however , there has been a dearth of data about the performance of potential tests and the largest study involved fewer than 2000 women and only one endometrial cancer was diagnosed.13 the ukctocs protocol enabled us to assess the performance of tvs for endometrial screening cancer 37 038 postmenopausal women . 
 when the analysis was restricted to women who reported no symptoms of postmenopausal bleeding at the scan and had an endometrial thickness measurement available , a cuto of 5 mm achieved a sensitivity of 771% and speci city of 858% ( table 4 )  . 
although the role of population screening for endometrial cancer remains uncertain , the ndings are of immediate value in the management of increased endometrial thickness in postmenopausal women undergoing pelvic scans for reasons other than vaginal bleeding . our ndings con rm the strong correlation between tvs ndings and subsequent diagnosis of endometrial cancer , as shown by the rrs ( table 2 )  . 
 this correlation was shown by the levels of sensitivity et cut - o ( mm ) number of cases of ea / aeh with positive result proportion of ec cases detected number of women with positive result risk of ec / aeh relative risk of ec / aeh ( 95% ci ) number of investigations per case detected whole population screened whole population screened whole population screened whole population screened first quartile ( highest risk ) screened second quartile screened third quartile screened fourth quartile ( lowest risk ) screened > 675 > 485 > 465 > 575 10000% 8045% 5564% 1128% 3233% 2105% 1278% 1278% 36 864 6174 1263 1535 1665 036% 173% 586% 1705% 451% 182% 102% 181% 100 2047 ( 13393130 ) 3537 ( 25844950 ) 5315 ( 32118500 ) 4373 ( 20999032 ) * 2263 ( 9645319 ) * 838 ( 3821840 ) * 14588 ( 248186025 ) * * relative risk within the risk quartile . 
as expected , the optimum cuto in asymptomatic women of 445 mm is similar but lower than the 5 mm cuto reported for symptomatic women.26 of note , our report shows that 26 women ( 195% ) who developed endometrial cancer within a year of their scan on ukctocs had an endometrial thickness of less than 5 min a theoretical model , based on the estimate that 15% of endometrial cancers occur in women without vaginal bleeding , smith - bindman and colleagues27 calculated the risk of endometrial cancer to be 67% for an endometrial thickness greater than 11 mm.27 this ts satisfactorily with 59% risk of endometrial cancer in our cohort where 96 ( 722% ) of 133 women were asymptomatic at an endometrial cuto of 10 mm . although the data show that tvs can detect endometrial cancer before symptoms are detected in a high proportion of postmenopausal women , there are a range of issues that need to be addressed before population screening for endometrial cancer can be proposed . 
if we assume an incidence of 60 per 100 000 per year and 30% mortality at 5 - year follow - up , a randomised controlled trial would need 500 000 participants to document a 50% reduction in mortality . 
since a trial on this scale is almost certainly not feasible , decisions about whether or not to screen for endometrial cancer will have to be made on the basis of surrogate measures of e cacy . 
we explored the possibility of reducing the overall burden of screening by focusing on a group of the population identi ed as being at higher risk on the basis of epidemiological criteria . 
our logistic regression model that used epidemiological variables of the use of the oral contraceptive pill , age at menarche , number of pregnancies , weight , age , and history of cancer was able to separate the population into quartile groups at di erent levels of risk . 
 this would reduce the burden of screening to 25% of the population with detection of about 40% of the cases . the strengths of our study include the large size of our cohort , prospective data collection with standardised measurement of endometrial thickness as part of the trial protocol , systematic follow - up , and information on epidemiological variables . 
consistent with earlier reports of the correlation of endometrial thickness and hrt , 28 the median endometrial thickness in users of hrt in the control group was 36 mm versus 27 mm in non - users . 
this probably relates to the use of tamoxifen , which is known to be associated both with increased endometrial thickness ( range 49117 mm ) in postmenopausal women2934 and increased risk of endometrial cancer ( rates of 03% vs 006% in women on placebo ) .35 we were , however , unable to con rm a recently reported correlation between ovarian volume and the risk of endometrial cancer of aeh reported by the plco trialists.36 one of the limitations of our study was that endometrial cancer screening was not an interventional endpoint in the ukctocs . 
detailed data on the variety of procedures done was not collected , but this is unlikely to alter the performance characteristics of endometrial thickness . a further limitation of our study is the accuracy of the reports of postmenopausal bleeding . 
therefore , there might be bias in the recording of these data for women who had an endometrial thickness above the level that triggered clinical referral ( > 5 mm )  . there was a di erence in median endometrial thickness measurements in healthy women across the 13 centres . 
in addition to slight variations for measuring endometrial thickness in 36 731 individuals across 13 centres , it is also probably related to variations in the demographics such as body - mass index of patients between centres . 
it highlights the need to have training and quality assurance measures in place if ultrasound were to be used as a screen for endometrial cancer . the scanning techniques the cis around parameter estimates were wide because of low numbers of endometrial cancers despite the large overall number of participants . 
some key variables that could a ect risk of endometrial cancer , such as smoking , 38 diabetes , and hypertension , 39 could not be used in model building because the main focus of the recruitment questionnaire was on risk factors for ovarian cancer . 
variables were collected on follow - up and a greater percentage of women with endometrial cancer reported a history or diagnosis of diabetes ( nine [ 102% ] of 88 ) compared with those without endometrial vol 12 january 2011 articles panel : research in context systematic review a systematic review of ovarian cancer screening41 was published by the nhs centre for reviews and dissemination before submission of the grant proposal to the uk medical research council for united kingdom collaborative trial of ovarian cancer screening . 
no systematic review of endometrial cancer screening was done . a detailed review of published work of endometrial cancer screening in an asymptomatic population was done as part of our analysis . 
other studies1416 have included smaller populations making it impossible to assess the sensitivity of screening or to achieve con dent estimates of speci city or positive predictive value . interpretation our study provides to our knowledge the only large - scale data on the performance characteristics of tvs in endometrial cancer screening , and provides evidence that ultrasonography can detect endometrial cancer in asymptomatic women with 8090% sensitivity and similar levels of speci city . 
 clinicians faced with ultrasound data on endometrial thickness from scans done in various disorders aside from vaginal bleeding will now have data to inform their daily practice . the likely bene t of detection of endometrial cancer by ultrasound screening would be conjecture . 
we have limited ourselves to reporting and discussing the performance characteristics . the rising incidence of endometrial cancer and the di culty of doing a randomised controlled trial large enough to specify mortality as an endpoint , suggests that the decision to introduce screening for all or a subgroup of asymptomatic women will rest on surrogate criteria such as the performance characteristics described in our report and future studies of acceptability , health economics , and risk strati cation . 
we do not advocate population screening for endometrial cancer until further data are available from these studies . contributors ijj , agm , mb , sc , and um contributed to the study design , analysis and interpretation of the data , and drafting and revision of the report . 
um and ij has a nancial interest through ucl business and abcodia ltd in the third party exploitation of clinical trials biobanks , which have been developed through the research at ucl . 
all other authors declared no con icts of interest . acknowledgments the trial was core funded by the uk medical research council , cancer research uk , and the uk department of health with additional support from the eve appeal , special trustees of barts and the london , and special trustees of uclh . 
a substantial portion of this work was done at uclh / ucl within the womens health theme of the nihr cancer ( 1429 [ 50% ] of 28 801 ; data not shown )  . 
furthermore , although there was an association with weight , we could not con rm the link between the risk of endometrial cancer and body - mass index.40 a paucity of detailed information on type of hrt and duration of use at scan also reduced our ability to do further subanalyses . false - positive results on tvs screening for endometrial cancer will require a form of endometrial sampling that , although not a major procedure , will generate anxiety , inconvenience , and cost . 
there are of course complications as well as costs of hysteroscopy that would need to be assessed carefully in a risk - bene t analysis if screening for endometrial cancer with tvs was to be introduced . 
another important consideration for future studies of endometrial cancer screening is acceptability of the screening strategy . a cuto at 5 mm or greater would result in 58 diagnostic procedures for each case of endometrial cancer detected . 
we are exploring the possibility of further re ning risk strati cation by incorporating sex - steroid hormone pro ling . laparoscopy or whether ovarian cancer screening will save lives is currently unclear and whether the primary screen should be with tvs or a serum biomarker is debated . 
the extra cost of incorporating endometrial cancer screening within the scope of an ovarian cancer screening trial could be marginal and add bene t to the screening strategy if properly modelled . our report is to our knowledge the rst large - scale report of the performance characteristics of tvs in endometrial cancer screening ( panel )  . 
in particular , issues of early detection , morbidity , acceptability , and health economics of intervening on the basis of endometrial thickness will need to be the subject of future studies . 
we thank the women throughout the uk who are participating in the trial and to the entire medical , nursing , and administrative sta who work on the ukctocs . 21 kurman rj , kaminski pf , norris hj . 
the biologic signi cance of cytologic atypia see correspondence page e194 preventable cancer : off - limits for commonwealth meeting ? as the global burden of non - communicable diseases continues to exert its toll , the prevention , screening , and early diagnosis of cancer should be a priority for all countries . 
the letter , cosigned by eminent experts in cancer and population health , demands that issues surrounding cervical cancer and endemic childhood cancers are part of the commonwealth health ministers meeting in may 2017 . 
the signatories also call for screening , early detection , and improved awareness of various childhood cancers , which can be treated successfully if caught early or even prevented through effective control of malnutrition and infectious diseases . 
surely the health of women and children is paramount to achieve such goals ? cost - effective prevention and screening for cancers should be an integral part of any successful uhc agenda . 
the limited reply declares that the prevention , treatment , and care of cancers are a priority , but fails to suggest any amendments to the forthcoming meetings agenda to give these important issues the consideration they deserve . 
a recent report from the american cancer society warns that the incidence of the diseasein which typically 90% of patients are over 50 years of ageis increasing sharply in each generation born since 1950 . 
as national colorectal and bowel cancer awareness months are marked in march and april in the usa and uk , respectively , this timely report rings alarm bells for ominous changes in the aetiology of this disease . despite colorectal cancer being a slow growing disease in which symptoms may not present for many years , survival rates have improved in recent decades , mainly thanks to screening . 
major risk factors ( unhealthy diets , obesity , and sedentary lifestyles ) are becoming more prevalent in successive generations , raising the question of whether these factorsespecially in the early years of lifecould interact with an underlying genetic backdrop to trigger early onset of the disease . screening is the mainstay of colorectal cancer prevention and early detection . 
 furthermore , with the widespread belief that cancer is associated with ageing , family doctors can too easily discount the possibility of colorectal cancer in young patients , even when they present with characteristic symptoms such as blood in the stool and abdominal pain . what can be done ? although whole - population screening is not feasible , cost - effective , or truly warranted , genetic counselling and gene testing for those known to be at high risk because of family history or underlying genetic predisposition could be considered . 
 the lancet oncology vol 18 april 2017 editorial published online april 2 , 2019 s1470 - 2045 ( 19 ) 30216 - 5 correction to lancet oncol 2017 ; 18 : e14352 correction to lancet oncol 2019 ; 20 : 335 correction to lancet oncol 2019 ; 20 : 66373 seymour l , bogaerts j , perrone a , et al . 
lancet oncol 2017 18 : e14352on page e145 , under assessment of target , nontarget , and new lesions the beginning of the third paragraph should read : the assessment of non - target lesions at each timepoint follows similar principles . 
iupd ( but not icpd ) can have been documented before icr or when the criteria for neither cr nor pd have been met ( referred to as non - icr / non - iupd ) and can be assigned several times , as long as icpd was not confirmed . 
these corrections have been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 42035 fuchs cs , shitara k , di bartolomeo m , et al . 
ramucirumab with cisplatin and fluoropyrimidine as first - line therapy in patients with metastatic gastric or junctional adenocarcinoma ( rainfall ) : a double - blind , randomised , placebocontrolled , phase 3 trial . 
lancet oncol 2019 ; 20 : 42035in this article , the percentage of grade 4 gastrointestinal haemorrhage events in the ramucirumab plus fluoropyrimidine and cisplatin group in table 3 should have been 1% . 
 this correction has been made to the online version as of april 30 , 2019 . correction to lancet oncol 2019 ; 20 : 63648 moore kn , secord aa , geller ma , et al . 
lancet oncol 2019 ; 20 : 63648in the declaration of interests section of this article , angeles alvarez secords declaration should read aas reports research funding and honoraria or advisory board fees from tesaro during the conduct of the study ; and research funding from abbvie , amgen , astex pharmaceuticals , astrazeneca , clovis , astellas pharma , boehringer ingelheim , bristol - myers squibb , eisai , endocyte , exelixis , incyte , merck , pharmamar , immutep , roche , genentech , seattle genetics , and tapimmune , and honoraria or advisory board fees from alexion , aravive , astex pharmaceuticals , astrazeneca , clovis , janssen , johnson & johnson , merck , mersana , myriad , oncoquest , roche , and genentech , outside the submitted work . 
this correction has been made to the online version as of april 30 , 2019 , and the printed article is correct . ( bilcap ) : a primrose jn , fox rp , palmer dh , et al . 
 lancet oncol 2019 ; 20 : 66373 in the figure 4 n / n column , the capecitabine group should be labelled as the observation group , and vice versa , and n / n should be events / patients . 
this correction has been made to the online version as of april 2 , 2019 . correction to lancet oncol 2019 ; 20 : 67485 mohamad o , tabuchi t , nitta y , et al . 
 risk of subsequent primary cancers after carbon ion radiotherapy , photon radiotherapy , or surgery for localised prostate cancer : a propensity score - weighted , retrospective , cohort study . 
lancet oncology 2019 ; 20 : 67485the affiliation of dr hiroshi tsuji was added ( national institute of radiological sciences , national institutes for quantum and radiological science and technology , chiba , japan )  . 
this correction has been made to the online version as of april 30 , 2019 and the printed version is correct . vol 20 may 2019 e242 corrections corrections correction to lancet oncol 2012 ; 13 : 987 correction to lancet oncol 2014 ; 15 : 621 correction to lancet oncol 2014 ; 15 : 881 randomised , fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 lancet oncol 2012 ; 13 : 98392in table 3 of this article , the number of events / n in the abiraterone acetate plus prednisone group who had been exposed to docetaxel for more than 3 months should read 401 / 653 . 
 adjuvant bevacizumab in patients with melanoma at high risk of recurrence ( avast - m ) : interim results from a multicentre , open - label , randomised controlled phase 3 study . 
 lancet oncol 2014 ; 15 : 62030 in gure 1 of this article , of the 291 patients who discontinued early , 119 patients discontinued because recurrence and 112 patients discontinued because of unacceptable toxic e ects . 
 this correction has been made to the online version as of july 28 , 2014 . clinical cook g , williams c , brown jm , et al , for the national cancer research institute haemato - oncology studies group . 
high - dose chemotherapy plus autologous stem - cell transplantation as consolidation therapy in patients with relapsed multiple myeloma after previous autologous stem - cell transplantation ( ncri myeloma x relapse [ intensive trial ] ) : a randomised , open - label , phase 3 trial . 
lancet oncol 2014 ; 15 : 87485 in gure 3 of this article , the second subgroup of the 2 microglobulin at registration category should have > 35 mg / l . 
these have been made to the online version as of july 28 , 2014 . category vol 15 august 2014 e365 corrections published online june 12 , 2015 s1470 - 2045 ( 15 ) 00056 - x correction to lancet oncol 2015 ; 16 : e227 correction to lancet oncol 2015 ; 16 : 738 correction to lancet oncol 2015 ; 16 : 747 schiller jh . 
 antibodies lancet oncol 2015 ; 16 : 73839in this comment , the chemotherapy backbone used in the squire trial was incorrectly referred to as gemcitabine and carboplatin in four instances in the third paragraph ; it should read gemcitabine and cisplat these corrections have been made to the online version as of june 29 , 2015 , and the printed version is correct . torri v , broggini m , garassino mc . 
lancet oncol 2015 ; 16 : 74648the seventh sentence of the nal paragraph of this comment should read : results for leu858arg are still inconclusive because although progression - free survival is higher in patients given all egfr inhibitors versus chemotherapy , overall survival seems to be better with chemotherapy than with afatinib for these patients . 
 this correction has been made to the online version as of june 29 , 2015 , and the printed version is correct . for future lowy dr , herrero r , hildesheim a , for the participants in the iarc / nci workshop on primary endpoints for prophylactic hpv vaccine trial . 
 lancet oncol 2015 ; 16 : e22633 in the panel , in the section on the quadrivalent vaccine for men , the second bullet point should read : approved in the eu by the ema for the prevention of vaccine - type related anal lesions and for the prevention of vaccine - type related genital warts ( ages 9 )  . 
lancet oncol 2015 ; 16 : this news e316in item , the nal two sentences of paragraph 3 read : according to the scale , treatment late - stage egfr - mutated nonsquamous lung cancer with erlotinib provides a gain in progression - free survival ( pfs ) of 85 months ( hazard ratio [ hr ] 016 [ 95% ci 010026 ] ) and an improvement in quality of life compared with carboplatin and gemcitabine , earning an esmo - mcbs score of 4 / 5 . 
in contrast , the same drug when used to treat metas tatic pancreatic cancer provides an overall gain of only 9 days compared with chemotherapy treatment , and had a score of 1 / 5 . 
this correction has been made as of june 12 , 2015 . vol 16 july 2015 e313 correction to lancet oncol 2020 ; 21 : 101718 correction to lancet oncol 2020 ; 21 : 93546 correction to lancet oncol 2020 ; 21 : 112526 iarc monographs vol 127 group . 
lancet oncol 2020 ; 21 : 101718in this news piece , the web links in the margin for the preamble to the iarc monographs and for the iarc declarations of interest were incorrect and have been amended . 
 lancet oncol 2020 ; 21 : 112526in this comment , the fourth paragraph should read one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
because overdiagnosis appears to increase with age , it is possible that overdiagnosis occurred in both groups after the age of 50 years , but could not be detected because of the design of the trial . 
 this correction has been made as of sept 1 , 2020 , and the printed version is correct . vol 21 september 2020 e418 corrections errata see articles page 528 errata miller va , hirsh v , cadranel j , et al . 
afatinib versus placebo for patients with advanced , metastatic non - small - cell lung cancer after failure of erlotinib , ge tinib , or both , and one or two lines of chemotherapy ( lux - lung 1 ) : a phase 2b / 3 randomised trial . 
lancet oncol 2012 ; 13 : 52838in this article ( published online march 26 ) , the rst sentence of the fourth paragraph on the fourth page should have read we measured progression - free survival from the date of randomisation to disease progression or death , whichever occurred rst . 
this correction has been made to the online version as of april 24 , 2012 . see news page e194 vol 13 may 2012 e186 comment if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology as piration of mediastinal and hilar lymph nodes should be used to assess preoperative lung cancer status in countries where tuberculosis is endemic.10 finally , hiv infection is associated with increased lung cancer cases . 
can tuberculosis further increase this risk ? in a study11 that linked aids registry surveillance data for 322 675 patients with aids diagnosed between 1977 and 2002 , with cancer registries in 11 us regions , lung cancer risk over 10 years was unrelated to tuberculosis . 
 tuberculosis awareness in patients with cancer needs to be reinforced , especially in low - burden developed countries , and lung cancer awareness in patients with previous or suspected tuberculosis should be urgently strengthened in developing countries to increase the low numbers of potentially resectable tumours . * sandro vento , massimiliano lanzafame department of internal medicine , faculty of medicine and health sciences , university of botswana , gaborone , botswana ( sv ) ; and infectious diseases unit , gb rossi university hospital , verona , italy ( ml ) ventosandro@yahoo.it we declare that we have no con icts of interest . yu yh , liao cc , hsu wh , et al . 
lancet oncol 2011 ; 12 : 37786in this article ( april ) , on page 380 , the number of women with luminal a breast cancer tested for the kras variant should have been 478 in gure 2a and the percentage of premenopausal women diagnosed with luminal a breast cancer should have been 151% in gure 2b . 
lancet oncol 2011 ; 12 : 41516on page 415 , in the second column , it was stated that 17 variants showed moderate to strong evidence of a true association and were therefore candidates for clinical tests , this should have said 14 variants . 
this correction has been made to the online version as of may 18 , 2011 . published online may 18 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70127 - 9 522 vol 12 june 2011 preventing prevention : indian politics and public health clash recent move by the largest indian government , in a the countrys independent public health organisation , the public health foundation of india ( phfi ) , has been barred from receiving foreign funding , including donations from the bill & melinda gates foundation . 
the phfi , which helps to support central and local governments by promoting breast cancer awareness campaigns , developing population - based cancer registries , and promoting universal health care , will lose roughly 45% of its funding from foreign investment over concerns regarding alleged lobbying with parliamentarians and media on anti - tobacco messages , and the misuse of funds and bank accounts that were allegedly not disclosed to the home ministry . 
 this suspension is part of a wider move in recent years by the indian government to cancel foreign contribution ( regulation ) act licenses , which regulate the flow of funds from foreign donors , from which some 20 000 indian non - governmental organisations benefit . 
while some have seen these cancellations as part of a wider effort to appease affiliate groups to the government who have accused philanthropic organisations of pushing corporate interests , others believe that the government is trying to promote a wholly nationalistic agenda in a bid to retain power in the 2019 elections . the recent move to cut funds to the phfi comes at a time when public health is a growing concern in india . 
earlier this month , the indian government announced that it will miss its deadline of december 2017 to reduce coal emissions and airborne particulate matter by two - thirds , declaring instead that developed countries should be responsible for tackling global pollution levels . 
although indias per capita emissions are only 159 metric tonnes per year compared with 755 for china and 1639 for the usa , india is still the worlds third - biggest emitter of greenhouse gases in absolute terms , and has notable levels of air pollution , which killed nearly 11 million of its residents in 2015 alone . 
such an open and defiant attitude by the indian government about their failure to meet coal emission targets , and their dismissive attempt to shift the responsibility to other countries , is a careless and harmful attitude to adopt , but an understandable attitude at a time when the us government dismantling its own environmental protection agency and backtracking on former president barack obamas clean power plan . 
by failing to address such chronic causes of illness , the indian government stands to exacerbate the growing pressure the current public health system upon which a large proportion of indias working class and unemployed rely . 
as a result , indias public health - care system has wholly inadequate financial resources to sufficiently train , staff , equip , or sometimes even run , health facilities nationally an infrastructure that is sure to worsen as one of the countrys largest public health organisations loses a substantial portion of their funding from overseas . although aligning public health targets with a political agenda is certainly nothing new , these drastic steps taken by the current government will inevitably affect public health programmes and initiatives . 
cancer is an emerging health problem in india , and already causes 6% of all adult deaths every year , with the number of cancer deaths set to increase to nearly 1 million in 2025 . 
 this means increasing , not reducing , the availability of funds to help to promote public health campaigns that encourage healthy lifestyles , reduce tobacco use , improve cancer registries , and increase the availability of cancer screening . 
it is worrying that at a time when health care in india is most in need , the government has opted to push for a wholly political and nationalistic agenda at the cost of public health , which clearly needs foreign investment to realistically meet the growing burden of non - communicable diseases across the country . 
that the indian government openly makes moves to undermine public health goals is somewhat paradoxical to a vision of india as an emerging social and economic superpower , and will erode the true social and democratic value that improved health holds for the country . 
 the lancet oncology vol 18 june 2017 editorial correction to lancet oncol 2019 ; 20 : 128694 correction to lancet oncol 2019 ; 20 : 1506517 correction to lancet oncol 2019 ; 20 : e616 burki tk . 
 ff l u c i c l o v i n e a n d ga - psma - 11 pet - ct in patients with early biochemical recurrence after prostatectomy : a prospective , single - centre , single - arm , comparative imaging trial . 
lancet oncol 2019 ; 20 : 128694in this article , in figure 2 , the f - fluciclovine detection rate for prostate bed has been corrected to 9 ( 18% )  . 
this correction has been made to the online version as of sept 23 , 2019 . correction to lancet oncol 2019 ; 20 : 160214 oscarsson n , mller b , rosn a , et al . 
lancet oncol 2019 ; 20 : 1602 14in the summary of this article , the first sentence of the findings section should have read of 223 patients screened between may 9 , 2012 , and dec 20 , 2017 , 87 patients were enrolled and randomly assigned to either hyperbaric oxygen therapy ( n = 42 ) or standard care ( n = 45 )  . 
 this correction has been made to the online version as of sept 23 , 2019 , and the printed article is correct . kato k , cho bc , takahashi m , et al . 
nivolumab versus chemotherapy in patients with advanced oesophageal squamous cell carcinoma refractory or intolerant to previous chemotherapy ( attraction - 3 ) : a multicentre , randomised , open - label , phase 3 trial . 
 lancet oncol 2019 ; 20 : 1506517in this article , the name of the funder should be ono pharmaceutical company , and in the results section , paragraph eight , the data for the comparison between groups for the utility index should have been 0076 , 00110142 ; p = 0023 . 
lancet oncol 2019 ; 20 : e52234in this series paper , the value 55% was missing from in the the following sentence first paragraph of the strategies for providing paediatric oncology services section : data from hospital - based registries in the english - speaking caribbean islands show a 2 - year survival rate of 55% compared with 85% in hics . 
this correction has been made to the online version as of oct 30 , 2019 . published online september 23 , 2019 s1470 - 2045 ( 19 ) 30594 - 7 vol 20 november 2019 e613 corrections malignancies interest group database , 7 5% of patients with thymic carcinomas developed myasthenia gravis ; organotypia is usually mantained in thymic carcinomas and , therefore , confers a small risk of myasthenia gravis relative to thymomas . 
thus , the possibility of heterogeneity of thymoma and thymic carcinoma in one tumour challenges the use of immune checkpoint inhibitors for the treatment of thymic malignancies , both of which are associated with immune - related adverse events . the key limitations of this study will prevent immediate adoption of pembrolizumab versus other treatment for thymic carcinoma . 
first , pd - l1 expression has not been verified to be a reliable biomarker in this or other malignancies , but there are other immune components that might be better biomarkers for response to immune checkpoint inhibitors that have been used in previous studies.810 second , thymic carcinoma comprises histologically different subtypes of cancer . 
notably , the histological subtypes within the tumours of patients in this trial were 48% squamous cell carcinoma and 15% neuroendocrine carcinoma , which does not reflect the typical distribution of histological subtypes in thymic carcinoma . are ongoing although additional trials with immune checkpoint carcinoma , thymic inhibitors important . 
the small number of reproducibility patients in phase 2 trials does not have to be a limitation to achieving treatment advances for rare cancers : replicate sample collection in translational research can counter this shortcoming with demonstrated reproducibility . 
cooperative group collaborations , such as the international thymic malignancies interest group or the thoracic alliance for cancer trials , could be useful to generate sufficient evidence to solve this problem of small patient numbers . approved drugs for rare cancers are scarce , as giaccone and colleagues have mentioned ; the high cost of these drugs , such as sunitinib and pembrolizumab , make it difficult to treat patients with thymic carcinoma worldwide because many countries cannot afford these medicines . 
globally , treatment for recurrent thymic carcinoma is still often single - agent cytotoxic chemotherapy . giaccone and colleagues plan to investigate the combination of pembrolizumab and epacadostat as an immune - combination therapy in a future expansion of this phase 2 study . 
thus , we are facing the next step to develop further therapies for thymic malignancies . yusuke okuma department of thoracic oncology and respiratory medicine , tokyo metropolitan cancer and infectious diseases centre komagome hospital , tokyo 113 - 8677 , japan y - okuma@cick.jp i declare no competing interests . kelly rj , petrini i , rajan a , wang y , giaccone g . 
 clin cancer res 2013 ; 19 : 429596 . next - generation nuclear morphology to grade solid tumours a central task for surgical pathologists diagnosing tumours is to reliably assess tumour aggressiveness from morphologic features . 
typical components of grading systems are tissue architecture , degree of resemblance to the respective benign tissue , mitotic activity , necrosis , and aberrances in nuclear morphology ( ie , nuclear pleomorphism , variations chromatin size , nucleolar prominence , and published online february 2 , 2018 s1470 - 2045 ( 18 ) 30063 - 9 see articles page 356 vol 19 march 2018 comment distribution )  . 
flemming1 coined the term chromatin in 1879 when describing nuclear structures that could be stained with basic dyes in the interphase , whereas waldeyer2 introduced the term chromosome in 1888 when describing mitotic chromat soon after , chromosomal alterations in tumours were described by bovari , 3 who also hypothesised a causal role of unequal chromatin distribution in carcinogenesis . 
the dogma of all morphologists , that function follows form , also applies to chromatin structure , which directly affects genomic activity by activating or silencing genes and gene families . in our contemporary concept , chromatin contains the whole eukaryotic genome , rather densely packaged around histones ( h2a , h2b , h3 , and h4 )  . 
posttranslational modifications of histones ( eg , acetylation , methylation ) also determine chromatin compaction , structure , and dynamics , and it is not surprising that mutations in the genes responsible for these regulatory modifications are often seen in cancer.4 advances in sequencing technologies have massively broadened our knowledge of driver oncogenes and their role during tumour progression and have helped promote the development of therapeutic drugs , but a holistic view that integrates gene expression and higher chromatin regulation is yet to be established . 
 although most pathologists know that chromatin irregularities , especially coarse and clumped chromatin as seen under the light microscope , are typical of higher graded tumours , the diagnostic value of subnuclear morphology has not been unearthed so far . 
 dna cytometry , introduced in 1966 , is a simple approach to compare overall dna content in tumour cells and normal cells.5 this technique gained popularity because aberrant dna content ( aneuploidy ) was more common in more aggressive tumours and neoplastic lesions than in benign , reactive lesions . 
today , most clinicians and pathologists do not use data on dna ploidy in patient care , even though a re - evaluation of this technique might be warranted.6 to classify image analysis chromatin patterns with modern technology is an obvious next step in developing more standardised diagnostic algorithms that could become part of tumour grading in the future . that in the lancet oncology , kleppe and colleagues7 describe nucleotyping , an automated method to reveals determine chromatin heterogeneity relevant prognostic information in various solid tumour types , including colorectal , endometrial , and ovarian carcinoma . 
although the preparatory steps are similar to conventional dna cytometry ( eg , dissection of cells , feulgen stain , multiple images , etc ) , this procedure does not yield overall staining intensity ; instead , it gives a measure of chromatin organisation computed by the entropy of pixel grey levels . 
for all analysed tumour entities , survival times were consistently shorter in patients with chromatin heterogeneous tumours than patients with chromatin homogeneous tumours , and the prognostic value of chromatin heterogeneity was independent of other parameters in a cox analysis . 
 this is an important finding , especially because the technique is applicable to formalin - fixed , paraffinembedded tissue and could easily be added to any routine workflow complement conventional tumour grading . in pathology laboratories however , some questions rema is nucleotyping easily transferable to other academic institutes ? is this biomarker robust enough to perform comparably in a decentralised setting ? how relevant are the trained personnel who identified the nuclei of interest in terms of interobserver variability of the technique ? pending clarification of these questions , this excellent study serves as an example of next - generation morphology that might enrich the pathologists armamentarium in the digital future , which is only just beginning . glen kristiansen institute of pathology , university of bonn , 53127 bonn , germany glen.kristiansen@ukbonn.de i declare no competing interests . copyright the author ( s )  . 
archiv mikrosk anat 1888 ; 32 : 1122 . 276 vol 19 march 2018 comment published online february 8 , 2018 s1470 - 2045 ( 18 ) 30075 - 5 see articles page 370 bovari t . 
 denosumab is not inferior and might even be superior to zoledronic acid in reducing skeletal - related events and improving survival in patients with certain solid tumours.2 however , in a prospective , double - blind study2 comparing denosumab with zoledronic acid in patients with solid tumours ( except breast cancer ) or myeloma ( 10% of the study patients ) , an ad - hoc analysis suggested inferior survival for patients with myeloma treated with denosumab . 
this study had several limitations and zoledronic acid remained the standard of care for patients with myeloma.3 in the lancet oncology , noopur raje and colleagues4 report a large , randomised , double - blind , phase 3 study , in which patients were randomly assigned to either 4 - weekly intravenous zoledronic acid , the present standard of care for myeloma - related bone disease , or 4 - weekly subcutaneous denosumab . 
the study met its primary endpoint of non - inferiority for denosumab versus zoledronic acid regarding the time to first skeletal - related event ( hazard ratio 098 , 95% ci 085114 ; pnon - inferiority = 0010 )  . 
study patients had a high burden of bone disease : 1144 ( 67% ) of the 1718 enrolled patients had already had a skeletalrelated event before enrolment and 376 ( 44% ) of 859 patients in the denosumab group and 383 ( 45% ) of 859 patients in the zoledronic acid group had a first onstudy skeletal - related event . 
however , 60% of first onstudy skeletal - related events occurred during the first 3 months of the study and 81% in the first 6 months , suggesting that even potent osteoclast inhibitors could not prevent skeletal - related events in the short teras such , early identification of patients at risk and timely intervention are crucial to avoid bone complications . 
 in a post - hoc landmark analysis at 15 months , denosumab was associated with fewer skeletal - related events than zoledronic acid , but this analysis has to be interpreted cautiously and cannot confirm superiority of denosumab over zoledronic acid in skeletal - related event prevention . 
 although the study by raje and colleagues4 is the largest placebo - controlled study ever done in patients with myeloma , several questions remaonly patients with myeloma - related bone disease at diagnosis were enrolled and the benefits of denosumab patients without bone disease are uncertaa survival benefit for patients treated with zoledronic acid versus clodronate1 or placebo5 has been shown , but a survival benefit for denosumab over zoledronic acid has not yet been seen , and additional follow - up is needed . 
additionally , rankl is implicated in the growth , survival , and development of drug resistance vol 19 march 2018 comment corrections correction to lancet oncol 2016 ; 17 : 738 correction to lancet oncol 2016 ; 17 : e310 correction to lancet oncol 2016 ; 17 : 1203 , 06 , 08 , 09 , 11 published online august 31 , 2016 s1470 - 2045 ( 16 ) 30438 - 7 wallington m , saxon eb , bomb m , et al . 
 also , in the patients with nsclc column in table 1 of this article , and in the 30 - day mortality columns in tables 2 , 3 , 5 and 7 of this article , some percentages were incorrect . 
dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - ofconcept , multicentre , open - label , phase 2 trial . 
lancet oncol 2016 ; 17 : the declaration of interests section of this review , the declaration for rk should have included and has received lecture fees from japan vaccine co ltd and msd for lectures on the safety and e ectiveness of the hpv vaccine . 
 folfiri plus cetuximab versus folfiri plus bevacizumab for metastatic colorectal cancer ( fire - 3 ) : a post - hoc analysis of tumour dynamics in the final ras wild - type subgroup of this randomised open - label phase 3 trial . 
this correction has been made to the online version as of sept 1 , 2016 , and the printed version is correct . correction to lancet oncol 2016 ; 17 : e423 burki tk . 
disruptions caused by the covid - 19 pandemicmore than 40% of countries report partially or fully disrupted cancer servicesare now expected to further exacerbate disparities in access to cancer care and increase excess mortality.10 there must be renewed commitment to , and investments in , cancer control that spurs greater action and integration at all service levels , particularly primary care for prevention , early detection and palliative care , which also offer benefits in the broader prevention and control of non - communicable diseases . include cancer interventions in universal health coverage as essential health services , with associated financial protection from the catastrophic expenditure experienced by so many patients with cancer . 
geneva : world health organization , 2020 . published online february 8 , 2021 s1470 - 2045 ( 21 ) 00017 - 6 sars - cov - 2 vaccination and phase 1 cancer clinical trials there is now a rapid global roll - out of severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) vaccines as part of the response to the covid - 19 pandemic.1 approved sars - cov - 2 vaccines include those from pfizer - biontech , 2 moderna , 3 and oxford astrazeneca , 4 but who estimates that there are 52 ongoing clinical research projects developing sars - cov - 2 vaccines.1 different vaccine mechanisms have been explored using technologies based long viral on messenger rna ( mrna ) , synthetic peptides , plasmid dna , and inactivated , attenuated , or genetically modified viruses . 
efficacy data are encouraging , with the mrna - based vaccines reporting more than 90% protection from covid - 19 with good tolerability , although the durability of protection , and thus the need for repeated vaccinations , is uncertain . covid - 19 - associated morbidity and mortality in patients with cancer range from 5% to 61% based on data from the covid - 19 and cancer consortium registry and other groups , more than the 23% observed in the general population.1 although these morbidity and mortality figures are associated with confounding biases , it is clear that patients with cancer are vulnerable and have a high risk of serious covid - 19 symptoms . 
 intrinsic or therapy - induced 298 vol 22 march 2021 comment to the best of our knowledge , sars - cov - 2 vaccine trials have excluded patients in anticancer trials or taking immunosuppressive drugs , which limits formal experience in this area and means that further data are needed to address concerns regarding the effects of malignancies and anticancer drugs on vaccine efficacy . 
although policies covering the optimisation of the timing of vaccinations during standard - oftargeted drugs , care chemotherapy , immunotherapy , radiotherapy , and surgery are being introduced , it is unlikely that there will be any formal guidance on experimental phase 1 clinical trials of investigational medicinal products ( imps ) .5 , 6 this is especially pertinent for first - in - human , first - in - class phase 1 trials of novel anticancer drugs , in which toxicity and efficacy profiles are limited to preclinical in - vitro and in - vivo data . tumour - cell in general , with regards to phase 1 trials of anticancer drugs , two key questions arise : what are the potential effects of such imps on ( 1 ) the efficacy and ( 2 ) the toxic effects of sars - cov - 2 vaccinations ; and vice versa . 
for example , a sars - cov - 2 vaccine is likely to confer reduced protection in patients participating in phase 1 trials of experimental b cell - depleting antitumour drugs , such as monoclonal antibodies targeting cd10 , cd19 , or cd20 , or cd19 chimeric antigen receptor t cells , given that such patients are unlikely to mount an optimal immune response.7 from experience with influenza a vaccinations in patients receiving checkpoint inhi bitors targeting pd1 or pd - l1 , seroconversion and sero protection rates are generally high.8 toxicity is particularly important when considering the effects of vaccinations on trials that involve imps with a high risk of immune adverse events , including cytokine release syndrome , or novel drugs given in combination with immunotherapies . 
 although there is experience in administering well established vaccinations to patients with cancer in phase 1 trials , these tend to be limited to inactivated vaccines and exclude live - attenuated and replicationcompetent vector vaccines . 
this contrasts with the available sars - cov - 2 vaccines that are mrna - based , live attenuated , non - replicating , or that use more conventional protein subunits . the covid - 19 pandemic requires consideration of when patients participating in early cancer clinical trials should get vaccinated.5 typically , the timing of panel : recommendations for sars - cov - 2 vaccination and phase 1 cancer trials not started phase 1 trial avoid starting trial investigational medicinal product ( imp ) until 24 weeks after the second dose of severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) vaccine is administered safely for trial imps with cytokine release syndrome risk . already in phase 1 trial administer sars - cov - 2 vaccine during the phase 1 trial but avoid vaccination on days of parenteral imp dosing and the dose - limiting toxicity period . vaccination has depended on the individual patient and the type of trial therapy ; for example , vaccinations are recommended before systemic trial therapies commence , and are generally permitted on trial if the patient has already started systemic therapy . 
however , guidance on the administration of sars - cov - 2 vaccines from trial sponsors has been unclear , ranging from full approval for such vaccines to be given in parallel to the imp , to a complete avoidance of the vaccine during imp administration . we are an international group of medical oncologists based across the usa , the uk , canada , and europe and are involved in treating patients with advanced cancers in early phase clinical trials . 
on the basis of the promising clinical data for approved sars - cov - 2 vaccines , we believe that the benefits of vaccination in the covid - 19 pandemic should substantially outweigh the possible benefits of participating in a phase 1 trial in light of the high risk to these patients of contracting life - threatening sars - cov - 2 infection . 
we recommend applying risk stratification by considering trials with a risk of cytokine release syndrome ( eg , certain immunotherapies ) separately to those without such toxicities ( eg , non - immunotherapy studies involving molecularly targeted drugs )  . 
we also recommend that patients participating in early trials of anticancer drugs with unknown safety and tolerability should avoid starting trial imps until 24 weeks after the second dose of the sars - cov - 2 vaccine is administered safely , especially for those with a risk for cytokine release syndrome ( panel )  . 
if the trial involves proven anticancer drugs with known benefits , this wait might vol 22 march 2021 comment see online for appendix be more challenging for patients with progressing advanced cancers , and the risks and benefits of the delay must be carefully considered with the patient . 
 we also recommend that patients avoid receiving their vaccine on days of parenteral imp dosing ( and receive it at a time as distanced as possible from imp dosing ) and the dose - limiting toxicity period if administration of the sars - cov - 2 vaccine is mandated while the patient is participating in an early phase trial . 
this is particularly pertinent for common sars - cov - 2 vaccine adverse events , such as tiredness , headaches , muscle and joint aches , chills , and fever , which might be particularly prominent after the second vaccine dose or if the patient has already been exposed to asymptomatic sars - cov - 2 infection . 
 close monitoring of patients in real time after sars - cov - 2 vaccination will be essential to assess potential interactions , adverse events , and clinical outcomes , including those from both sars - cov - 2 infection and complications from cancer . 
in patients who have cancer trial imp - associated immune - related adverse events , such as colitis or pneumonitis , and are on steroids or other immunosuppressive drugs , the sars - cov - 2 vaccine should probably be avoided until the event is fully resolved or markedly improved . 
 clearly , such decisions need to be individualised to each patient and imp risk profile . because it is currently unclear how long immunity will last after vaccination , with this response likely to be temporary and lasting months to years , rather than decades or a lifetime , repeat vaccinations are likely to be required during a patients lifetime . 
sarscov - 2 infection has no doubt affected and delayed all components of care for patients with cancer , including screening , diagnosis , treatment , and monitoring and surveillance strategies , and has probably increased the risk of cancer - related morbidity and mortality.9 the pandemic also affects oncology trials , including patient accrual and logistical and economic aspects , and has the potential to affect the long - term development of promising life - saving anticancer drugs . although phase 1 oncology trials have unknown toxicity risks and are done primarily to recommend safe doses for future studies , the potential benefit to patients is well described.10 these factors need to be judiciously balanced with the unknown effects of the imp on sars - cov - 2 vaccination and the risk of such vaccines worsening the toxicity of a subset of novel anticancer drugs . 
it will therefore be essential for decisions to be made on an individual basis with patients and their advocates to assess the riskbenefit balance by considering known imp mechanisms and adverse events , and key patient characteristics , such as age , comorbidities , prognosis , and social factors . 
this is an opportunity for , and indeed a duty of , treating oncologists , trial sponsors , and regulatory agencies to monitor , document , and communicate outcomes of the different sars - cov - 2 vaccines during anticancer drug administration , as well as their effect on the development of covid - 19 , toxicity of anticancer drugs , and eventual cancer outcomes . 
as the vaccination programmes roll out globally , this early experience is likely to affect the timing , safety , and efficacy of sars - cov - 2 vaccination for a considerable period . we declare no competing interests related to the study , with full details of other competing interests listed in the appendix . 
tay thanks the md anderson cancer center for support grant p30 ca016672 and the sheikh khalifa bin zayed al nahyan institute for personalized cancer therapy at the md anderson cancer center for support grant 1u01 ca180964 . 
 rp , jsdb , and ub thank the experimental cancer centre and national institute of health biomedical research centre for infrastructural funding . * timothy a yap , lillian l siu , emiliano calvo , martijn p lolkema , patricia m lorusso , jean - charles soria , ruth plummer , johann s de bono , josep tabernero , udai banerji tyap@mdanderson.org investigational cancer therapeutics ( phase i program ) , university of texas md anderson cancer center , houston , tx 77030 , usa ( tay ) ; division of medical oncology and hematology , princess margaret cancer centre , university health network , toronto , on , canada ( lls ) ; early phase clinical drug development in oncology , start madrid - ciocc , centro integral oncolgico clara campal , madrid , spain ( ec ) ; department of medical oncology , erasmus mc cancer institute , erasmus university medical center rotterdam , rotterdam , netherlands ( mpl ) ; early phase clinical trials program , yale university medical center , new haven , ct , usa ( pml ) ; department of drug development , gustave roussy cancer institute , university paris saclay , villejuif , france ( j - cs ) ; northern institute for cancer care , freeman hospital and newcastle university , newcastle upon tyne , uk ( rp ) ; the institute of cancer research , london , uk ( jsdb , ub ) ; royal marsden nhs foundation trust , london , uk ( jsdb , ub ) ; department of medical oncology , vall dhebron institute of oncology , vall dhebron barcelona hospital campus , universitat autnoma de barcelona , barcelona , spain ( jt ) european society for medical oncology . 
esmo.org / covid - 19 - and - cancer / covid - 19 - vaccination ( accessed jan 7 , 2021 )  . 300 vol 22 march 2021 comment 2 polack fp , thomas sj , kitchin n , et al . 
safety and efficacy of the chadox1 ncov - 19 vaccine ( azd1222 ) against sars - cov - 2 : an interim analysis of four randomised controlled trials in brazil , south africa , and the uk . 
aboutsitc / press - releases / 2020 / sitc - statement - sars - cov - 2 - vaccinationcancer - immunotherapy ( accessed jan 7 , 2021 )  . yri oe , torfoss d , hungnes o , et al . 
nat rev clin oncol 2019 ; 16 : 77378 . quality assurance and cancer medicines in low - income and middle - income countries physical pain , or are worried about becoming a financial burden on their families.4 access to quality - assured medicines is integral to tackling inequality in cancer outcomes and for fostering a global patient - centred public health approach , which has increasingly been called for during the covid - 19 pandemic.5 delivery of quality - assured medicines at the point of access requires a robust regulatory syste when the regulatory system is deficient , substandard or falsified medicines can be accessed through formal supply routes that serve public facilities . 
although initiatives between high - income countries and lmics are helping to strengthen regulatory control , 1 challenges related to a scarcity of testing facilities , regulatory workforce and expertise , oversight , administration , and communications still exist.6 there is a need to simultaneously strengthen the formal supply chain workforce to maintain the quality substandard medicines are medicines that fail to meet their quality standards , whereas falsified medicines are those that have been deliberately misrepresented identity , composition , or source.1 both in their substandard and falsified medicines are a major burden on health and economic outcomes , particularly in low - income and middle - income countries ( lmics ) .1 who reports that one in ten medicines in lmics might be substandard or falsified , 1 although a systematic review suggests higher rates of 1148%.2 these medicines impact a broad range of therapies , including cancer treatments , antibiotics , and other life - saving therapies.1 there is vast global inequality in cancer outcomes , 3 which is attributed to factors such as sparse implementation of prevention strategies , delayed diagnosis , and difficulty accessing treatment . 
cancer control requires early diagnosis , effective intervention , and palliative care.3 treatment of cancer often leads to catastrophic financial costs for patients and their families , 3 which exacerbates existing inequalities , hinders socioeconomic progress in marginalised groups , and causes poverty cycles.4 these impacts are compounded by the infiltration of substandard or falsified medicines into health - care settings . 
the out - of - pocket spending and indirect costs of cancer ( eg , due to work loss ) increase if patients purchase ineffective medicines . income substandard or falsified medicines reduce patient confidence in health - care systems , which can lead to disengagement if patients do not perceive effective treatments to be available , or if they fear prolonged vol 22 march 2021 comment corrections correction to lancet oncol 2015 ; 16 : 1045 correction to lancet oncol 2015 ; 16 : 1499 tournigand c , chibaudel b , samson b , et al . 
 this correction has been made to the online version as of nov 29 , 2015 . correction to lancet oncol 2015 ; 16 : 1355 , 1363 hegewisch - becker s , graeven u , lerchenmller ca , et al . 
maintenance strategies after first - line oxaliplatin plus uoropyrimidine plus bevacizumab for patients with metastatic colorectal cancer ( aio 0207 ) : a randomised , noninferiority , open - label phase 3 trial . 
 lancet oncol 2015 ; 16 : 135569the fourth line of the findings section of the summary of this article should read bevacizumab alone was noninferior to standard uoropyrimidine plus bevacizumab ( hazard ratio [ hr ] 108 [ 95% ci 085137 ] ; p = 053 ; upper limit of the one - sided 988% ci 142 ) , whereas no treatment was not ( hr 126 [ 099160 ] ; p = 0056 ; upper limit of the one - sided 988% ci 165 )  . 
 lancet oncol 2015 ; 16 : 14931505in this article , the colours of the curves in both panels of gure 3 were inverted ; the correct version is shown below . 
 these corrections have been made to the online version as of nov 29 , 2015 . events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 49 ( 41 - 57 ) 54 ( 43 - 62 ) stratied hazard ratio 081 ( 066101 ) p = 0059 ( log - rank ) unstratied hazard ratio 078 ( 068096 ) p = 0019 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0023 events ( n ) median ( 95% ci ) bevacizumab bevacizumab plus erlotinib 221 ( 196267 ) 249 ( 214289 ) stratied hazard ratio 079 ( 063099 ) p = 0036 ( log - rank ) unstratied hazard ratio 079 ( 064098 ) p = 0035 ( log - rank ) restricted mean survival ( maximum follow - up 24 weeks ) p = 0024 number at risk bevacizumab bevacizumab plus erlotinib time ( months ) number at risk bevacizumab bevacizumab plus erlotinib vol 16 december 2015 e589 articles sensitivity and speci city of multimodal and ultrasound screening for ovarian cancer , and stage distribution of detected cancers : results of the prevalence screen of the uk collaborative trial of ovarian cancer screening ( ukctocs ) usha menon , aleksandra gentry - maharaj , rachel hallett , andy ryan , matthew burnell , aarti sharma , sara lewis , susan davies , susan philpott , alberto lopes , keith godfrey , david oram , jonathan herod , karin williamson , mourad w seif , ian scott , tim mould , robert woolas , john murdoch , stephen dobbs , nazar n amso , simon leeson , derek cruickshank , alistair mcguire , stuart campbell , lesley fallow eld , naveena singh , anne dawnay , steven j skates , mahesh parmar , ian jacobs summary background ovarian cancer has a high casefatality ratio , with most women not diagnosed until the disease is in its advanced stages . 
 methods between 2001 and 2005 , a total of 202 638 post - menopausal women aged 5074 years were randomly assigned to no treatment ( control ; n = 101 359 ) ; annual ca125 screening ( interpreted using a risk of ovarian cancer algorithm ) with transvaginal ultrasound scan as a second - line test ( multimodal screening [ mms ] ; n = 50 640 ) ; or annual screening with transvaginal ultrasound ( uss ; n = 50 639 ) alone in a 2 : 1 : 1 ratio using a computer - generated random number algorithall women provided a blood sample at recruitment . 
 the main reasons for withdrawal were death ( two mms , 28 uss ) , non - ovarian cancer or other disease ( none mms , 66 uss ) , removal of ovaries ( ve mms , 29 uss ) , relocation ( none mms , 39 uss ) , failure to attend three appointments for the screen ( 72 mms , 757 uss ) , and participant changing their mind ( 483 mms , 1490 uss )  . 
 overall , 4355 of 50 078 ( 8.7% ) women in the mms group and 5779 of 48 230 ( 120% ) women in the uss group required a repeat test , and 167 ( 03% ) women in the mms group and 1894 ( 39% ) women in the uss group required clinical evaluation . 
28 ( 16 mms , 12 uss ) of 58 ( 483% ; 95% ci 350618 ) of the invasive cancers were stage i / ii , with no di erence ( p = 0396 ) in stage distribution between the groups . 
the sensitivity , speci city , and positive - predictive values for all primary ovarian and tubal cancers were 894% , 998% , and 433% for mms , and 849% , 982% , and 53% for uss , respectively . 
for primary invasive epithelial ovarian and tubal cancers , the sensitivity , speci city , and positive - predictive values were 895% , 998% , and 351% for mms , and 750% , 982% , and 28% for uss , respectively . 
there was a signi cant di erence in speci city ( p < 00001 ) but not sensitivity between the two screening groups for both primary ovarian and tubal cancers as well as primary epithelial invasive ovarian and tubal cancers . interpretation the sensitivity of the mms and uss screening strategies is encouraging . 
 although advances in therapy have improved median survival during the past decade , there has been little or no change in the overall mortality rate.1 , 2 women are commonly diagnosed with stage iii / iv disease , for which 5 - year survival rates are around 27% and 16% , respectively.35 this has led to e orts over the past two decades to develop early detection strategies using serum ca125 and ultrasound.6 , 7 preliminary evidence from a previous randomised controlled trial suggests that screening sequentially with ca125 and ultrasound ( multimodal screening ) can result in a survival bene t.8 median survival was signi cantly increased in women who developed ovarian cancer in the screened group compared with the control group ( 729 vs 418 months , p = 00112 )  . 
improved survival has also been reported in a single - arm ultrasound - based study.9 re nements have been made to screening since the two previous studies , including the introduction of transvaginal ultrasound , 10 improvements in the interpretation of ultrasound ndings using morphology - based indices , 9 , 1113 and the development of a risk of ovarian cancer algorithm for the interpretation of serial ca125 results.14 , 15 the multicentre united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) is a randomised controlled trial designed to provide de nitive data on the e ect of ovarian cancer screening on mortality , as well as comprehensively addressing the cost , acceptance , physical and psychosocial morbidity , and performance characteristics of multimodal screening and ultrasoundbased screening . methods participants women were recruited through 13 regional trial centres located in national health service ( nhs ) trusts in england , wales , and northern ireland.16 all women provided written consent . 
eligibility criteria included age panel 1 : classi cation of ovarian morphology on ultrasound normal ovary of uniform hypoechogenicity and with a smooth outline with or without a single inclusion cyst or spots of calci cations inclusion cyst must be single , less than 10 mm in diameter and not distort the outline of the ovary simple cyst a single , thin walled , anechoic cyst with no septa or papillary projections complex any case in which the ovary has any non - uniform ovarian echogenicity , excluding single simple or inclusion cysts 5074 years , and postmenopausal status de ned as greater than and including 12 months , amenorrhoea following a natural or surgical menopause , or greater than and including 12 months of hormone - replacement therapy commenced for menopausal symptoms.17 women were excluded if they had a history of bilateral oophorectomy , active malignancy ( women with a past history of malignancy were eligible if they had no documented persistent or recurrent disease and had not received treatment for > 12 months ) , previous history of ovarian cancer , participation in other ovarian cancer screening trials , or increased risk of familial ovarian cancer . 
high - risk women were eligible for a separate trial : the united kingdom familial ovarian cancer screening study ( ukfocss ) .18 the study was approved by the uk north west multicentre research ethics committee ( 00 / 8 / 34 ) , with site - speci c approval from the local regional ethics committees and the caldicott guardians ( data controllers ) of the participating primary care trusts . scanned electronically using procedures invitations to participate in the trial were sent to women aged 5074 years whose details were obtained from the age and sex registers of the participating 27 primary care trusts.16 on enrolment at the trial centres , women viewed an information video and participated in a group discussion before completing a datasheet , consent forms , and undergoing venepuncture . 
the recruitment questionnaires were sent to the coordinating centre , where they were com puterised intelligent character - reading and optical - mark - reading software ( teleform elite version 8.1.1 , cardi software inc , vista , ca , usa )  . 
any inconsistency or information not recognised by the data - capture software was veri ed manually by trained data - entry sta , who validated the computer - interpreted data . 
once the custom - built trialmanagement system con rmed eligibility , participants were randomly assigned to either no treatment ( control ) ; annual ca125 screening ( interpreted using a patented risk - of - ovarian - cancer algorithm ) with transvaginal ultrasound scan as a second - line test ( multimodal screening ; mms ) ; or annual screening with transvaginal ultrasound ( uss ) alone in a 2 : 1 : 1 ratio with a computergenerated random number algorith randomisation was done as follows : rst , the trial management system allocated a set of 32 random numbers to each trial centre ; second , the lowest eight were allocated to the mms group , the next eight to the uss group , and the remaining 16 to the control group ; third , each successive volunteer within the trial centre was randomly allocated one of the random numbers and so randomly assigned a group ; and nally , when all 32 random numbers had been used up a further set of 32 was generated . 
randomisation was accomplished by the trial - management system using the visual basic randomisation statement and the rnd function . 328 vol 10 april 2009 articles following randomisation , letters were automatically printed and sent to each woman and their general practitioner con rming eligibility and randomisation status . 
blood samples were taken in gel tubes ( 8 ml gel separation serum tubes ; greiner bio - one 455071 , stonehouse , uk ) at the trial centres and transported overnight at ambient temperature to the central laboratory . 
serum ca125 electroconcentrations were chemiluminescence sandwich immunoassay on an elecsys 2010 ( roche diagnostics , burgess hill , uk ) using two monoclonal antibodies ( oc125 and m11 ; fujirebio diagnostics ab , gteborg , sweden )  . 
the rst scan ( level 1 scan ) , and any repeat level 1 scans needed because of an type 1 unsatisfactory rst scan , were done by sonographers , who were certi ed sonographers , trained midwives , or doctors with experience in gynaecological scanning who were working in the nhs . 
detailed description of all features the number and size of cysts , wall regularity , presence and thickness of septae , size of papillations , and echogenicity of the uid contentswere recorded . 
cysts and complex morphology were classi ed pictorially , initially using the format reported in the kentucky screening trial , 19 and from 2003 onwards using the ( iota ) international ovarian tumour analysis classi cation.13 measurement of the ovary was important to con rm that it had been visualised , and for audit purposes . 
only cyst volume panel 2 : possible outcomes after level 1 and level 2 screens in the mms group level 1 screen normal risk of ovarian cancer score : women returned to annual screening , with the next level 1 blood test scheduled on the next anniversary of the randomisation date intermediate risk of ovarian cancer score : women were recalled for a repeat ca125 measurement 12 weeks after the screen . 
any women whose risk of ovarian cancer remained intermediate after three ca125 tests were referred for a level 2 screen elevated risk of ovarian cancer score : women were recalled for a level 2 screen in 68 weeks , with earlier screens arranged where there was a high index of suspicion level 2 screen women with a normal transvaginal ultrasound scan result and normal or intermediate risk of ovarian cancer returned to annual screening , with the next level 1 test on the next anniversary of the randomisation date women with a normal transvaginal ultrasound scan result but an elevated risk of ovarian cancer , or an unsatisfactory scan irrespective of risk of ovarian cancer status , underwent a repeat level 2 screen in 6 weeks and were triaged again on the basis of the results to annual screening or clinical assessment women with an abnormal transvaginal ultrasound scan were referred for clinical assessment irrespective of their risk of ovarian cancer status panel 3 : possible outcomes after level 1 and level 2 screens in the uss group level 1 screen women with a normal scan returned to annual screening , with the next level 1 transvaginal ultrasound scan on the next anniversary of the randomisation date women with an unsatisfactory scan result attended a repeat level 1 scan in 12 weeks . 
women were returned to annual screening following two unsatisfactory scans women with an abnormal level 1 scan were referred for a level 2 scan in 68 weeks , with earlier scans arranged where there was a high index of suspicion level 2 screen women with a normal level 2 scan returned to annual screening , with the next level 1 transvaginal ultrasound scan on the next anniversary of the randomisation date an unsatisfactory level 2 scan led to a repeat level 2 scan in 6 weeks or earlier , and women were triaged on the basis of the ndings to annual screening or clinical assessment women with an abnormal scan were referred for clinical assessment vol 10 april 2009 articles was used for scan classi cation . 
when ovaries were not visualised , the sonographers speci ed whether a good view of iliac vessels had been obtained or a poor view owing to obstruction by the bowel , broids , pelvic varicosities , or for other reasons . 
ascites was de ned as a maximum vertical pool measurement of greater than or equal to 10 m based on the visualisation and morphology of the ovaries , the scan was classi ed as either a normal scan , in which both ovaries had normal morphology or simple cysts less than 60 cm , or were not visualised but a good view of the iliac vessels was obtained ; an unsatisfactory scan , in which one or both ovaries were not visualised owing to a poor view ; or an abnormal scan , in which one or both ovaries had complex morphology or simple cysts greater than 60 cm , or ascites . scan images were transferred weekly on magnetooptical discs for central archiving . 
trial centres were able to request central review of ultrasound images . cancer using screening strategies in the level 1 screen in the mms group , women underwent venepuncture and serum ca125 measurement . 
the assay results were uploaded directly into the trial - management system , which calcu lated the risk of ovarian algorithm developed previously.15 , 17 the rst risk of ovarian cancer determination was based on a single measurement of ca125 and the womans age - speci c incidence of ovarian cancer . 
women were triaged into three risk groups on the basis of their risk of ovarian cancer , which determined whether they returned to annual screening or went on to have a repeat ca125 measurement or level 2 screen ( panel 2 )  . 
level 2 change rate and the the 202 638 women all had a blood sample taken at recruitment screening involved venepuncture for repeat ca125 assay and a transvaginal ultrasound scan . 
the results of the level 2 screen triggered three possible courses of action , as shown in panel 2 . the initial cuto s used for intermediate and elevated risk of ovarian cancer were greater than or equal to 1 / 1818 and greater than or equal to 1 / 500 , respectively . 
as the proportion of women classi ed into these risk categories were less than the proposed 15% and 2% , respectively , the cuto s were revised on april 1 , 2005 , to greater than or equal to 1 / 3500 and greater than or equal to 1 / 1000 after extensive data review by the independent data monitoring and ethics and trial steering committees . 
 there were three possible courses of action depending on the results of the level 1 scan , including referral for a level 2 scan , the results of which triggered one of a further three courses of action , as shown in panel 3 . 
 all clinicians were provided written information on the risk estimates for malignancy associated with the various morphological classi cations from the iota series once the estimates had been presented at the annual european society of gynaecological oncology meeting in 2003 . 
 additionally , clinicians were made aware that women who had previously undergone a hysterectomy had an incidence of adhesions and peritoneal increased pseudocysts that may be reported as multilocular adnexal cysts . clinical assessment this was undertaken by a designated clinician and included clinical evaluation and investigations as appropriate . 
these included serum ca125 in women in the ultrasound group , repeat transvaginal scans and doppler studies , ct / mri of the abdomen and pelvis , and occasionally assessment of other tumour markers . 
 for women in the mms group with a normal transvaginal ultrasound scan but elevated risk of ovarian cancer , clinical assessment included ruling out other causes of increased ca125 concentrations . 
the management plan took the views of the individual into account , and also accounted for any signi cant comorbidity , the speci c morphological features of the detected lesion , and history of a previous hysterectomy or major pelvic surgery that could be responsible for false - positive ultrasound appearances . for women who underwent surgery , the recommendation was removal of both ovaries and fallopian tubes for histopathological examination , even if the ovaries appeared macroscopically normal . 
where pelvic adhesions were present and there was an increased risk of complications , the clinician could opt to remove only the ovary found to have an abnormality on ultrasound and not proceed to remove the contra lateral ovary . 
a laparotomy was undertaken if clinical ndings or laparoscopy led to a strong suspicion of ovarian cancer , or if a laparoscopic procedure was not felt to be appropriate for other reasons . 
women found to have ovarian or tubal cancer at a primary laparoscopic procedure underwent a subsequent staging pro cedure . bilateral a follow - up plan was drawn up if , after clinical assessment , investigation , and discussion with the woman , a decision was made to manage the ndings conservatively . 
most women were followed up with a transvaginal ultrasound scan and a serum ca125 assessment at 3 months with a possible repeat at 6 months , and returned to annual screening if the ndings were unchanged at this review . 
 follow - up all participants are being followed up through a agging study with the nhs information centre for health and social care ( formerly o ce for national statistics , ons ) in england and wales , and with the central services agency and cancer registry in northern ireland . 
 additionally , women continued to attend for subsequent annual screens , and those who had been in the trial for 35 years following randomisation were sent follow - up questionnaires . 
 statistical analysis the primary outcome measure in ukctocs is ovarian cancer mortality and the primary comparison is based on an intention - to - treat analysis between the control group and both screened groups combined ( mms plus uss )  . 
 however , as the operating characteristics of the two screening groups are di erent a comparison between the control group and an individual screen group ( mms or uss ) is of equal interest . 
the design provides greater than 90% power to detect a 30% reduction in ovarian cancer mortality between the control and combined screening groups , and greater than 80% power to detect a 30% reduction in mortality between the control and either one of the individual screening groups , with both comparisons tested at a signi cance level of 005 . 
it is important to note that if one of the comparisons ( control vs mms or uss ) is signi cant and the other is not , the result would not necessarily imply that one method is signi cantly better than the other . 
if , as anticipated , the di erence in ovarian cancer mortality between the two screened groups is modest , then this study will have limited power to detect such di erences . 
the choice of screening strategy will then be based on other outcome measures such as sensitivity , positive - predictive value , morbidity , quality of life , and health economics . this paper presents the outcome of the prevalence screen in women randomly assigned to either mms or uss . 
the prevalence screen was de ned as a single or series of serum ca125 assays with or without transvaginal ultrasound scan ( mms ) or transvaginal ultrasound scan alone ( uss ) culminating in surgery or a return to annual screening . 
the screen was considered positive ( screen positive ) if the woman was referred for surgery and negative ( screen negative ) if the woman was returned to annual screening . 
the primary outcome measure was primary ovarian or fallopian tube cancer ( icd - 10 code c56 and c57.0 , respectively ) diagnosed within 12 months of the last scan or serum ca125 test in the prevalence screen . 
women with primary peritoneal cancer ( icd - 10 code c48.2 ) and those with ovarian neoplasms of uncertain behaviour ( icd - 10 code d39.1 ) were not included in the outcome measure . 
the most common reasons for withdrawal were death ( two mms ; 28 uss ) , non - ovarian cancer or other disease ( 66 uss ) , removal of ovaries ( ve mms ; 29 uss ) , relocation ( 39 uss ) , failure to attend three appointments for the screen ( 72 mms ; 757 uss ) , and participant changing her mind ( 483 mms ; 1490 uss )  . 
in accordance with good practice for randomised controlled trials we did not statistically compare the baseline characteristics of the women assigned to the two groups ; 20 , 21 the groups were well balanced ( table 1 )  . of the 50 078 women who underwent a prevalence screen in the mms group , 45 523 ( 909% ) were classi ed as low risk by the risk of ovarian cancer algorithm and returned to annual screening . 
in the course of the screen , ve women in the mms group died from unrelated causes , 24 were diagnosed with cancers other than ovarian cancer , and 215 withdrew from the trial . of the 48 230 women randomly assigned to the uss group , 42 416 ( 879% ) had transvaginal ultrasound scans , 4325 ( 90% ) had transabdominal ultrasound scans , and 1489 ( 31% ) had both . 
 six women in the uss group died from unrelated causes during the course of screening , seven were diagnosed with cancers other than ovarian cancer , and 252 withdrew from the trial . overall , 942 ( 095% ) of the 98 308 women screened underwent surgery as a result of the prevalence screen , with 87 women in the uss group undergoing surgery for every one woman from the mss group who underwent surgery . 
 there was a di erence in surgical approach between the two groups , with 75 of 97 ( 773% ) operations in the mms group involving laparotomy versus 397 of 845 ( 469% ) in the uss group ( table 2 )  . 
834 ( 47 mms , 787 uss ) women who underwent surgery were found to have benign pathology or normal ovaries ( table 3 ) , of whom 24 ( 29% ; 95% ci 1740 ) experienced a major complication . 
 * * three breast cancers , one endometrial cancer , and one cancer of the appendix . table 3 : histology in women who underwent surgery as a result of screening ( screen positives ) nodule and residual ovary in left pelvic side wall , one pulmonary embolism , two cases of deep - vein thrombosis , four cases of wound dehiscence , one wound haematoma , two hernias , one signi cant ileus , one bowel obstruction , one bowel stula , and two cases of signi cant infection . ovarian or tubal malignancies were detected in 87 women : 42 in the mms group and 45 in the uss group ( table 3 )  . 
there was no signi cant di erence ( fishers exact test p = 0229 ) in the number of stage iii borderline cancers in the mms ( two of eight ) compared with the uss group ( one of 20 )  . 
 in the mms group , 33 ( 786% ) of the 42 women with ovarian or tubal malignancies had ovarian cancer detected as a result of an elevated risk of ovarian cancer on the level 1 screen ( rst blood test )  . 
in the uss group , all 45 ( 100% ) women had ovarian cancer detected as a result of an abnormal scan on the level 1 screen ( rst scan )  . 
the median time to surgery from level 1 scan in these women was similar to that for women in the mms group : 815 days ( iqr 6031125 )  . 
 however , nine ( 214% ) of the women in the mms group with ovarian or tubal malignancies had ovarian cancer detected after an intermediate risk of ovarian cancer at the level 1 screen that led to repeat tests . 
the median time to surgery from the level 1 screen in these women was 2739 days ( iqr 22003310 ) , since the protocol for managing intermediate risk was to repeat ca125 tests 334 vol 10 april 2009 articles over a period of 810 months ( gure 2 )  . 
one woman initially had a normal level 2 scan , and one woman had two normal level 2 scans but was operated on based on a severe risk of ovarian cancer classi cation . 
they include one woman in the mms group and two from the uss group who withdrew from the trial after their level 1 screen and had an ovarian cancer diagnosed more than 1 year later . 
at an incident screen 22 months later , an increase in size of the mass on ultrasound prompted bilateral salpingo - oophorectomy , and she was diagnosed with stage ic papillary serous cystadenocarcinoma . 
as information on cancers can take up to 3 years to be recorded by the national cancer registries , we explored in detail the other sources of follow - up data in the 12 658 women for whom time from censorship ( 1 year from the date of the last scan or ca125 test on the prevalence screen ) to cancer registry follow up on june 13 , 2008 , was less then 3 years . 
in this cohort , after the censorship date , we had additional con rmation of ovarian cancer status in 11 336 women , as they had attended for further screening , and in an additional 17 women through returned follow - up questionnaires . 
 the source of veri cation of ovarian cancer status was limited to cancer registry follow up that was less than 3 years from the date of censorship in only 1275 women ( 13% of the entire cohort ; table 5 )  . 
this included one primary borderline and four invasive epithelial ovarian cancers in the mms group , and eight primary invasive epithelial ovarian cancers in the uss group ( table 3 )  . 
the ca125 concentrations at the prevalence screen ranged from 7 to 24 iu / l in the ve women with ovarian and tubal cancers in the mms group , and the cancers were diagnosed at 92 , 204 , 254 , 294 , and 329 days after the screen . 
all of the prevalence scans were normal in the uss group , and the cancers were diagnosed at 30 , 203 , 255 , 267 , 278 , 293 , 301 , and 341 days after the screen . for all primary ovarian and tubal cancers , the sensitivity , speci city , and positive - predictive values for mms and uss screening are shown in table 6 . 
there were 23 ( 42 of 97 ) operations per case of ovarian cancer in the mms and 188 ( 45 of 845 ) operations per case of early ( i / ii ) stage cancers ( % ) 471% 298% 649% 500% 291% 709% 483% 350% 618% 750% 194% 994% 00% 00% 410% 250% 55% 572% stage lower 95% ci upper 95% ci morphology serous endometrioid clear cell carcinosarcoma adenocarcinoma grade not graded screen positive screen negative overall overall * in two cases a diagnosis was made on the basis of ascitic uid cytology , omental biopsy , and imaging : primary surgery was not undertaken . table 4 : characteristics of primary invasive epithelial ovarian and tubal cancers ( icd - 10 c56 and c57.0 ) ons follow - up > 3 years from censorship date or when death certi cate was available number of women who have had an appointment after censorship date * number of women who have completed a follow - up questionnaire after censorship date * mms ( n = 50 078 ) uss ( n = 48 230 ) overall ( n = 98 308 ) 45 544 ( 909% ) 40 106 ( 832% ) 85 650 ( 871% ) 4071 ( 81% ) 7295 ( 182% ) 11 366 ( 116% ) 4 ( 001% ) 13 ( 003% ) 17 ( 002% ) remaining * 459 ( 09% ) 816 ( 17% ) 1275 ( 13% ) * in women with ons follow - up < 3 years from censorship date . 
censorship date is 1 year from the date of the last scan or ca125 in the prevalence screen . table 5 : details of follow - up of women who underwent screening the in speci city between ovarian cancer in the uss group . 
 when the analysis was restricted to primary invasive epithelial ovarian and tubal cancers , sensitivity was , compared with values when all cancers were included ( table 6 ) , much the same in the mms group , but lower in the uss group , although the di erence in sensitivity between mms and uss was still not statistically signi cant ( p = 0126 )  . 
 vol 10 april 2009 articles total number of women number of surgeries screen positives screen negatives sensitivity 95% ci speci city 95% ci 95% ci positive - predictive value screen positives screen negatives sensitivity 95% ci speci city 95% ci 95% ci positive - predictive value primary ovarian and tubal malignancies ( icd - 10 c56 and c57.0 ) within 1 year of prevalence screen number of operations per screen positive 188 108 primary invasive epithelial ovarian and tubal malignancies within 1 year of prevalence screen overall p value * 48 230 98 308 50 078 894% 849% 870% 0564 769965 724933 788929 998% 982% 990% < 00001 998998 981984 990991 433% 333538 53% 3971 92% 75113 895% 750% 829% 0126 752971 566885 720908 998% 982% 990% < 00001 998998 981984 990991 351% 256454 28% 1842 62% 4779 162 number of operations per screen positive 352 * fishers exact test . 
 borderline epithelial ovarian cancers and ovarian neoplasms of uncertain behaviour treated as false positives . table 6 : performance characteristics for detection of malignant ovarian and tubal neoplasms ( icd - 10 c56 and c57.0 ) in the prevalence screen speci city was higher in the mms than in the uss group , resulting in fewer repeat tests and almost nine times fewer operations per cancer detected . 
the main strengths of the study are recruitment by random invitation using the health - authority registers of 27 primary care trusts , the multicentre design involving recruitment and screening through 13 nhs trusts , the scale of the trial , high compliance with screening , randomisation to two well - de ned screening strategies , and an independent review of surgical outcomes and detailed follow - up of the entire cohort . 
although primary peritoneal cancers are treated similarly to advanced primary ovarian carcinomas , neither the mms nor the uss screening strategies were developed to detect thehowever , data on these cancers would be interesting , so primary peritoneal cancers are listed separately in table 3 . 
however , we have ( low malignant potential ) ovarian neoplasms , since they share the same icd - 10 code ( c56 ) as primary invasive epithelial ovarian cancers . 
 included primary borderline problem 84 primary ovarian ( icd - 10 c56 ) and three tubal cancers ( icd - 10 c57.0 ) were detected on screening , with a further 13 primary ovarian cancers diagnosed clinically in the ensuing year . 
19% ( eight of 42 ) of the primary ovarian cancers detected were borderline in the mms group , compared with 15% reported in clinical series.24 however , 44% ( 20 of 45 ) of the primary ovarian cancers detected in the uss group were borderline . 
this highlights an issue that has already become a signi cant cancer - screening strategiesthe detection of cancers that may never have been diagnosed in an individuals lifetime had they not been screened . 
in cancer screening , estimates of overdetection range from 3 to 50% of cases in breast cancer screening26 and 22 to 34% in prostate cancer screening.27 a similar rate of 25% overdetection has been reported with chest radiography for lung cancer , with the use of ct expected to result in higher rates.28 in ovarian cancer , such false positives may include ovarian neoplasms of uncertain behaviour ( icd - 10 d39.1 ) and borderline disease . 
once borderline cancers are detected during screening , it is di cult not to operate given that borderline and stage i invasive other 336 vol 10 april 2009 articles results indicate inherent strategies . 
the ovarian cancers share common morphological features on ultrasound imaging.29 the novel design of ukctocs , which randomly assigns women to two very di erent screening strategies , provides some insight into the in the di erent extent of overdiagnosis that screening pseudodisease will be less apparent with a serum ca125based ovarian cancer screening strategy than with uss screening . 
this accords with results from the prevalence screen of the prostate lung colon ovarian cancer ( plco ) screening trial , in which only one of nine borderline ovarian neoplasms were detected by ca125 screening , whereas all nine were detected by ultrasound.23 there is a possibility that some of these borderline tumours may progress to invasive cancers if undetected , although there is little evidence to support this . 
 di erences between the screening groups on later follow - up should help to elucidate the issue , and allow de nite estimates of overdiagnosis to be calculated . given the issues surrounding borderline disease , a separate analysis was done excluding borderline lesions , e ectively treating such lesions as false positives . 
this resulted in a fall in the sensitivity of the uss screen from about 85% to 75% , with an attendant increase in the ratio of operations per true positive from 19 : 1 to 35 : 1 . 
the detection rates in the mms group remained at around 89% , with a small increase in the ratio of operations per true positive from 23 : 1 to 29 : 1 . 
however , the clinical e ect of this di erence will depend on the mortality e ect on follow up , and on issues such as patient satisfaction and acceptability . various factors may contribute to the detection of more primary invasive epithelial cancers in the mms group than in the uss group . 
it is possible that a transvaginal ultrasound scan done at the time of the level 1 screen , 75 months earlier than when the transvaginal ultrasound scan was actually done in these women , would not have detected an abnormality . 
 although an unsatisfactory scan in the uss group does lead to a repeat level 1 scan in 3 months , the follow - up is not equivalent to that of an intermediate risk of ovarian cancer , as women are returned to annual screening after two unsatisfactory scans but have continued follow - up with ca125 after two intermediate risk of ovarian cancer results . 
ultrasound , unlike ca125 , has a subjective element , and it is possible that the heightened awareness of a sonographer in view of rising ca125 concentrations contributed to a positive diagnosis . 
however , it is noteworthy that two of the nine women in the mms group who were diagnosed after initially being classi ed as intermediate risk had normal scans initially . 
by contrast , ultrasound has a subjective element , and accuracy is correlated with the experience of the sonographer.30 , 31 there are no described qualityassurance measures for scanning postmenopausal ovaries in asymptomatic women . 
more than 100 sonographers were required to deliver the scan load of 55 000 scans per year ; these individuals were fully certi ed sta working in ultrasound departments in the uk nhs . 
until then , it should be noted that the number of interval cancers and sensitivity in the uss group is in keeping with other large single - centre and multicentre series ( table 7 ) for which systematic follow - up and tracing of interval cancers has been undertaken . 
a previous ultrasound and autopsy study that 154% of 234 post menopausal women who had died from nongynaecological diseases had ovarian cysts.32 here , 1894 ( 39% ) of women were found to have abnormal scans . 
 clinical assessment in the uss group , which included the use of morphological features detected during ultrasound , serum ca125 , and other imaging modalities , decreased surgical rates to 446% ( 845 of 1894 ) of those found to have abnormalities compared with 581% ( 97 of 167 ) of those with abnormalities in the mms group ( table 2 )  . 
the lack of follow - up data on the outcome of pelvic masses with benign ultrasound morphology33 means that a proportion of women and clinicians will opt for surgery once a complex adnexal lesion is detected , even if it is more likely to be benign . 
this is exempli ed in this series , in which a lesion detected on ultrasound was not removed on laparoscopy because it was thought to be an ovarian broma ( table 2 )  . 
the higher proportion of laparoscopic procedures in the uss group than in the mms group ( 624% vs 286% ) re ects the lower suspicion of malignancy among clinicians for certain ultrasounddetected lesions . 
however , such decisions are not straightforward , as the risk of malignancy associated with lesions such as multilocular cysts in clinical series is 18% , rising to 49% if a solid component is also present.29 during further rounds of screening there is likely to be a substantial fall in the number of women undergoing surgery for benign lesions in the uss group , as most will have been removed or detected and managed conservatively during the prevalence screen . 
it is therefore important to wait for the results of incidence screening before drawing de nite conclusions about the positive - predictive value and speci city characteristics of the two screening strategies . 
in the ultrasound screening trial by van nagell and colleagues , 9 the number of operations per case of invasive epithelial ovarian cancer detected was 93 : 1 ( table 7 ) after a mean of 48 annual screens . 
29% of women undergoing surgery which resulted in benign pathology or normal ovaries being detected , experienced a major complication involving injury to a hollow viscus or signi cant haemorrhage . 
 there was no di erence in the complication rates in the two screening groups . the proportion of primary invasive ovarian and fallopian tube cancers diagnosed with stage i / ii disease ( 48% ) was encouraging compared with the 26% rate in the clinical series34 and 22% in the prevalence screen of the plco screening trial in the usa ( table 7 ) .23 the highest reported proportion of early - stage cancers detected on screening is from the university of kentucky screening programme , 9 where 82% of primary invasive epithelial ovarian cancers detected were stage i / ii . 
the overall number of ovarian cancers reported in the university of kentucky study was also lower ( table 7 ) .9 the e ect of this apparent stage shift on mortality will not be known until su cient events have accrued for a comparison with mortality in the control group , when the trial is completed in december , 2014 . 
 the di erences in the uptake of the initial screen between women randomly assigned to the mms group and uss group ( gure 1 ) must be interpreted with care . 
 it is important not to interpret this as indicating that women preferred a blood test to a scan , as a signi cant proportion of this di erence re ects trial design . 
analysis of the psychosocial data and compliance with annual screening will provide better measures of womens preferences . a limitation of trial design could be that the criteria used to classify scans did not incorporate one of the many weighted morphological indices that have been 338 vol 10 april 2009 articles proposed to improve discrimination between benign and malignant masses.29 , 35 however , it is important to note that most of these indices were derived from clinical series in symptomatic patients , in whom advanced cancers are the nordata on morphological characteristics of early ovarian cancers in asymptomatic long - term follow - up of patients and outcome on ultrasound - detected limited . 
simple lesions are unilocular cysts are an exception , for which long - term follow - up of women has shown that they are invariably benign.36 this was incorporated into the ukctocs trial design , with simple cysts less than 60 cm in size classi ed as normal and the women returned to annual screening with no further review . 
all clinicians were provided with pictorial depictions of complex morphology , initially using the kentucky format19 until the adoption in 2003 of the iota format , 13 and all clinicians were aware of the risk of malignancy associated with the features in the clinical series . 
 serum ca125 and transvaginal ultrasound remain at the core of all new screening and diagnostic strategies being proposed for ovarian cancer , and although many new markers have been discovered since 1999 , none have so far been validated in a prospective screening trial . 
the trial serum bank , which currently has over 350 000 samples , will make the retrospective testing of new markers possible . a nal limitation of this report is that no data are available on cancers in the control group . 
however , in line with other ovarian cancer screening randomised controlled trials , 23 it was felt by the overseeing committees that the release of such information when screening is ongoing would compromise the overall outcome of the trial . 
although this maximises external validity by excluding biases related to advertisement and self - referral , the cohort is still likely to be healthier than the general uk population because of the characteristics of the women who chose to respond . 
the multicentre design , nhs hospital setting , use of standard tests ( ca125 and transvaginal ultrasound ) done by sta those who would deliver a national similar programme , and the management of women with abnormalities in nhs clinics using national guidelines ensures that the ndings of the trial are applicable to the wider population . 
there are inherent di erences between the two strategies being tested , with a more subjective element inherent in the ultrasound - based strategy than with the ca125 test , for which it is easy to implement stringent quality control . 
mms has signi cantly better speci city than does uss , resulting in fewer repeat tests and less surgery ; sensitivity for the detection of primary epithelial cancers of the ovaries and fallopian tubes seems better with mms than with uss , although is not statistically signi cant . 
the results of ongoing screening are required before a conclusion can be drawn regarding the e ect of screening on mortality . the di erence contributors ij , um , mp , sjs , sc , lf , and am were involved in study design . 
none of the other authors declared any con icts of interest . acknowledgments we are particularly grateful to the women throughout the uk who are participating in the trial , to the entire medical , nursing , and administrative sta who work on the ukctocs and to the independent members of the numerous oversight committees . 
the trial was core funded by the medical research council , cancer research uk , and the department of health , with additional support from the eve appeal , special trustees of barts and the london , and special trustees of university college london hospital ( uclh )  . 
a large portion of this work was done at uclh / ucl within the womens health theme of the national institute for health research uclh / ucl comprehensive biomedical research centre supported by the department of health . 
 news published online april 2 , 2020 s1470 - 2045 ( 20 ) 30217 - 5 for more on the characteristics of covid - 19 patients see jama 2020 ; published online march 23 . 
on the one hand , a patient might be at high risk of contracting the infection and dying from it ; on the other hand , the patient might be at high risk of the cancer progressing or causing death if it is not treated appropriately . 
 physicians have to assess whether treatment plans should be initiated on schedule or delayed , and if so , for how long ? stresses nhs england that individual patient decisions have to be made by multidisciplinary its guidance establishes teams . 
patients who are awaiting non - curative therapy that is unlikely to offer palliation , tumour control , or more than 1 years cancer guidelines during the covid - 19 pandemic as of april 1 , 2020 , more than 800 000 cases of coronavirus disease 2019 ( covid - 19 ) had been confirmed worldwide . 
 on march 26 , gethin williams , a colorectal surgeon at the royal gwent hospital in newport , wales , warned that his institution was under severe strain , with operating theatres turned into intensive care units to accommodate the influx of patients with covid - 19 . 
 according to an analysis of italian patients published in march , 20% of those who died from covid - 19 in the country had active cancer . the esmo website includes general information on covid - 19 , a q&a section , and links to useful resources . 
there is also advice on supporting patients and on infection control . in its guidance for managing patients with cancer requiring acute treatment , nhs england warned that certain groups are particularly vulnerable to serious illness if they become infected with severe acute respiratory syndrome coronavirus 2 . 
the blood cancers often directly compromise the immune system , so those patients are probably most at risk , whereas cancers such as colon cancer , breast cancer , and lung cancer do not typically cause immune suppression that is not treatment - related . schilsky notes that standard chemotherapy regimens for most solid tumours mainly cause transient immune suppression that manifests in low white blood cell counts . 
you can prop up the white blood cells using colony - stimulating factors , so these patients are probably at lower risk than the blood cancer patients , he told the lancet oncology . the pandemic poses several challenges for oncology services . 
we are seeing systems adapt to this now , with telephone and telehealth consultations , people receiving laboratory testing at facilities closer to their homes , and some evaluations being delayed , said schilsky . 
nhs lists several englands guidance for more on the resources for covid - 19 offered by the society of surgical oncology see for more on the statement by esso see org / news / esso - statementcovid - 19 / for more on the information provided by asco see information for more on guidance from the american society of radiation oncology see astro.org / daily - practice / covid19 - recommendations - andinformation for more on the information by the american society for transplantation and cellular therapy see org / communities / publichome ? communitykey = d3949d84 - 3440 - 45f4 - 814290ea05adb0e5 for more on the information by ebmt see org / covid - 19 - and - bmt for more on the guidance by the us food and drug administration see download for more on the guidance by the us national cancer institute see gov / investigatorresources / corona_virus_guidance.htm for more on the guidance by ema see health / sites / health / files / files / eudralex / vol - 10 / guidanceclinicaltrials_covid19_ en.pdf for more on the guidance by the uk national institute for health and care excellence see guidance / ng162 for more on the global radiation oncology targeted response see sciencedirect.com / science / article / pii / s2405630820300227 extension of life are assigned the lowest priority level . 
for radiotherapy , there are five levels of priority , patients with rapidly proliferating tumours with little scope for delay are in the highest group . several other cancer societies have issued some guidance . 
the society of surgical oncology website includes disease - site specific resources to help guide decisions in the era of covid - 19 , as well as a series of podcasts from different specialists . 
 there are information sheets on a range of malignancies , including breast cancer , colorectal cancer , endocrine cancer , and melanoma , with each subdivided into disease types , when appropriate . in a statement issued on covid - 19 , the european society of surgical oncology ( esso ) advised against seeing patients older than 70 years in the clinic , unless urgent . 
rest and recuperation , as well as psychological support should be factored into planning , the statement concluded . the asco website also assembles a great deal of information on patient care and covid - 19 , along with links to guidance from organisations such as the us centers for disease control and prevention and several oncology societies . 
asco has produced guidance on how practices should ready themselves for the virus ; advice can be found on staffing , clinical preparedness , infection prevention and control , and patient scheduling . 
there is also a set of tips for enhancing mental and physical healthone suggested exercise is mindful handwashing , which could be a neat way to combine hygiene and wellbeing . the american society for radiation oncology website contains a large section on covid - 19 . 
its website contains frequently asked questions , several of which are directly relevant to clinical decision making , and links to journal articles and relevant websites . the american society for transplantation and cellular therapy and the european society for blood and marrow transplantation ( ebmt ) have both issued guidelines for covid - 19 management . 
due to the rapidly changing situation , access to a stem cell donor might be restricted either due to the donor becoming infected , logistical reasons at the harvest centres in the middle of a strained healthcare system , or travel restrictions across international borders , note the ebmt guidelines . 
it is therefore strongly recommended to have secured stem cell product access by freezing the product before start of conditioning and , in situations when this is not possible , to have an alternative donor as a back - up . on the regulatory side , the us food and drug administration has issued guidance on managing clinical trials during the time of covid - 19 , as have the us national cancer institute and the european medicines agency ( ema )  . 
the ema document outlines the changes and adaptations that might be required over the course of the pandemic , for example , if trial participants need to be isolated , access to public places is limited , or health - care professionals have to take up different duties . 
the uk national institute for health and care excellence has issued guidance on delivering radiotherapy and systemic cancer therapies , which draws from nhs englands guidance . finally , the global radiation oncology targeted response emerged from an online discussion involving 121 contributors march , 2020 . 
but they also point out that although deferring radical treatment for diseases with favourable biology might seem immediately preferable , it might have unintended consequence in creating a further unmanageable surge in activity when the crisis has passed . it is too early to tell what shape this pandemic will take . 
 yi - long wu ( guangdong lung cancer institute , guangdong , china ) points out that the major disruption in the country to cancer care occurred during the first two weeks of february . 
from late february , everywhere except for hubei province , we were able to start giving patients surgery , chemotherapy , and radiotherapy again , he told the lancet oncology . 
now we are coming back to normal . talha khan burki 630 vol 21 may 2020 news re ection and reaction many ovarian cancers are diagnosed as international federation of gynecology and obstetrics stage iii disease . 
women with this stage of disease have a 5 - year survival of only 302%57% , 8 therefore studies with these women needs to start at the time of diagnosis . 
the main advantage of a prospective study would be the accurate documentation of the use of oral contraceptives , and this could help establish the period of time a woman should be using oral contraceptives , for prevention of ovarian cancer . 
 given that oral contraception has been available for more than 45 years , it would be too draconian not to o er patients such an intervention for chemoprevention of ovarian cancer , especially because the management of high - risk women with a brca mutation is multimodal and includes intensi ed early detection and prophylactic surgery . 
in this article the a liations for prof f boccardo and prof a rubagotti should have read : university of genoa , italy , and national cancer research institute of genoa , italy ( prof f boccardo md , prof a rubagotti phd )  . 
 more work needs to be done on the assessment of the risks and bene ts of oral contraception in addition to the lowered risk of ovarian cancer , the increased risk of breast cancer among carriers of a brca mutation also needs to be discussed in this context . 
 from case - control studies we know that the relative risk for breast cancer is not increased5 or only modestly increased ( or 12 ; 95% ci 102140 ) , 6 by the use of oral contraceptives . 
in view of the fact that carriers of a brca mutation have a lifetime risk for the development of breast cancer of up to 84% , 7 an odds ratio of 12 is considerable and should to be taken into account in the risk management of these patients . 
conversely , the risk reduction for ovarian cancer noted in the study by mclaughin and co - workers2odds ratio of 056 ( 95% ci 045071 ) in carriers of a brca1 mutation and 039 ( 023066 ) in carriers of a brca2 mutationcan be o set against the potentially increased risk of breast cancer . 
what is needed is to be able to provide a risk pro le for an individual person to allow accurate risk management in an individual woman . case - control studies do have limitations because they do not acquire prospective data , such as real risks for the development of cancers , or disease - speci c survival data . 
 vol 8 january 2007 corrections correction to lancet oncol 2013 ; 14 : 297 correction to lancet oncol 2013 ; 14 : 481 correction to lancet oncol 2013 ; 14 : 557 motzer rj , escudier b , tomczak p , et al . 
this correction has been made to the online version as of may 28 , 2013 . galimberti v , cole bf , zurrida s , et al , for the international breast cancer study group trial 2301 investigators . 
 lancet oncol 2013 ; 14 : 297305in the summary of this article , the fourth sentence of the findings section should read : breast cancer - related events were recorded in 48 patients in the axillary dissection group and 47 in the no axillary dissection group ( ten local recurrences in the axillary dissection group and eight in the no axillary dissection group ; three and nine contralateral breast cancers ; one and ve regional recurrences ; and 34 and 25 distant relapses )  . 
 this correction has been made to the online version as of may 28 , 2013 . tom waddell , oesophagogastric randomised , waddell t , chau i , cunningham d , et al . 
lancet oncol 2013 ; 14 : 48189in this article , list of authors should have the read : ian chau , david cunningham , david gonzalez , alicia frances clare okines , andrew wotherspoon , claire sa ery , gary middleton , jonathan wadsley , david ferry , wasat mansoor , tom crosby , fareeda coxon , david smith , justin waters , timothy iveson , stephen falk , sarah slater , clare peckitt , yolanda barbachano . 
this correction has been made to the online version as of may 28 , 2013 . vol 14 june 2013 e254 3 mato ar , hill bt , lamanna n , et al . 
ibrutinib plus obinutuzumab versus chlorambucil plus obinutuzumab in first - line treatment of chronic lymphocytic leukaemia ( illuminate ) : a multicentre , randomised , open - label , phase 3 trial . 
haematologica 2015 ; 100 : e30206 . lenalidomide as maintenance for every newly diagnosed patient with multiple myeloma in patients with newly diagnosed multiple myeloma , how to maintain the responses achieved after optimal therapeutic strategies was a challenge , and maintenance therapy emerged as an option aiming to extend the duration of the response through continued treatment and thereby improving progression - free survival and overall survival . 
because maintenance treatment is administered as continuous therapy , emphasis is placed on the convenience of administration , tolerability , and toxicity.1 low - dose lenalidomide is the only approved single agent treatment for patients with newly diagnosed multiple myeloma after transplantation.2 in the lancet oncology , graham jackson and colleagues3 confirm the benefit of lenalidomide in terms of progression - free survival . 
 in transplantation - ineligible patients , the findings by jackson and colleagues also support the results reported with lenalidomide as maintenance after induction with melphalan , prednisone , and lenalidomide , and are in line with the use of full - dose lenalidomide and dexamethasone as continuous therapy reported in the first trial.4 , 5 although the debate in this setting has always been whether to use fixed or continuous therapy , the trend now is use of continuous therapy with either lenalidomide or daratumumab after induction with daratumumab in combination with bortezomib plus melphalan and prednisone.6 patient with newly diagnosed multiple myeloma , but new therapies or combinations of drugs are needed to improve overall survival in these patients . the approved dose of lenalidomide is convenient because it is administered orally , and this study did not report any unexpected toxicity data . 
additional studies assessing health - related quality of life through patient - reported outcomes are necessary to know the patients perspective . lenalidomide is 10 mg continuously with the possibility of increasing to 15 mg , but different doses and schedules have been so far used in different trials . 
whether different doses and schedules could potentially result in different outcomes is not known , but the results of this study3 regarding the median progression - free survival of 26 months ( 95% ci 2231 ) in transplantation - ineligible patients is similar to that reported in the first trial , in which lenalidomide was given at full dose combined therefore , with possible to switch to low - dose lenalidomide without dexamethasone in transplantation - ineligible patients after induction therapy ? low - dose dexamethasone . 
 it , lenalidomide maintenance seems to be effective , well tolerated , and convenient , despite the lack of overall survival benefit , because of the influence of rescue therapies in the overall survival . 
lenalidomide is , therefore , a maintenance therapy option for every new agents or combinations of these are being investigated as maintenance therapy in this setting and might result in new standards of care . 
for example , vorinostat was combined with lenalidomide in a subset of patients in this study , and we await the results . published online december 14 , 2018 s1470 - 2045 ( 18 ) 30764 - 2 see articles page 57 vol 20 january 2019 comment the results of this study3 support the benefit of lenalidomide maintenance across different subgroups of patients and highlights the progression - free survival benefit in patients with high - risk cytogenetic abnormalities . 
however , it is important to note that lenalidomide did not overcome the poor prognosis that the presence of high - risk abnormalities confer to patients , and therefore novel treatments to improve the outcomes of these patients are needed . whether all patients need continuous maintenance therapy regardless of the quality of the response achieved with previous treatments remains unclear . 
however , next - generation sequencing and cytometry provide an opportunity to investigate the role of minimal residual disease assessment for tailoring maintenance strategies and would allow physicians to prescribe maintenance therapy and reply to a very common question raised by the patients : how many cycles of treatment does maintenance therapy include ? furthermore , long - term minimal residual disease monitoring could guide preemptive treatment preventing clinical relapses and ensuring durable responses . maintenance with lenalidomide is the standard of care , but the future has to move towards a personalised medicine approach that aims to improve overall survival and quality of life , which means giving the right drug to the right patient at the right time for the optimal duration . * mara - victoria mateos , vernica gonzlez de la calle hematology department , university hospital of salamanca , ibsal , salamanca , spain mvmateos@usal.es m - vm has received honoraria for lectures from janssen , celgene , takeda , and amgen , and for participation in advisory boards from janssen , celgene , takeda , amgen , abbvie , glaxosmithkilne , and pharmamar . 
n engl j med 2018 ; 378 : 51828 . the importance of surgery in colorectal cancer treatment in the lancet oncology , sara benitez majano and colleagues1 have engaged with a very important topic . 
 previous data have indicated poorer treatment results for colorectal cancer in both denmark and england compared with those in similar western countries.2 the continuous audit and assessment of outcomes is important to better understand the reality of cancer care each country and thus , this study is of interest to the public . majano and colleagues identified that an important difference between the countries studied regarding surgery for colorectal cancer was probably not the technique , but rather the frequency of surgical resection . 
 the proportion of patients treated with resectional surgery ranged from 684% in england to 813% in sweden for colon cancer , and from 599% in england to 708% in sweden for rectal cancer ; this range was wider for patients older than 75 years ( colon cancer 597% to 809% ; rectal cancer 457% to 619% )  . 
it is possible that attitudes towards surgery in the older patient population should be altered in england , but the data in this study do not include comorbidity , and the risk for increased perioperative mortality should not be underestimated . 
 preoperative optimisation of patients must be a focus of research , to increase the percentage of patients that are able to undergo resectional surgery in the future . what other factors could be influencing these results ? during the study period , the standardised referral pathway had already been introduced in denmark in 2010 . 
there is scarce vol 20 january 2019 published online december 10 , 2018 s1470 - 2045 ( 18 ) 30679 - x see articles page 74 comment evans sm , tikellis g , brooks a , et al . 
health - related quality of life after apalutamide treatment in patients with metastatic castration - sensitive prostate cancer ( titan ) : a randomised , placebo - controlled , phase 3 study . 
abiraterone acetate plus prednisone in patients with newly diagnosed high - risk metastatic castration - sensitive prostate cancer ( latitude ) : final overall survival analysis of a randomised , double - blind , phase 3 trial . 
psychooncology 2018 ; 27 : 233948 . stereotactic beam radiotherapy for prostate cancer : is less , more ? either important trial , in the lancet oncology , douglas brand and colleagues1 report an in which the authors aimed to investigate the fractionation sensitivity of radiotherapy in the curative treatment of low - risk and intermediate - risk prostate cancer . 
acute toxicity might be worse when treatments are delivered in few large fractions and an overall treatment time as short as 12 weeks , compared with protracted schedules delivered in 68 weeks . 
although the study limits its focus to early tolerance ( up to 12 weeks after radiotherapy ) , this study is the first that was designed to use contem porary radiotherapy delivery techniquesie , linac - based volumetric modulated arc radiotherapy or cyberknife . is much more patient - friendly important dose constraints to the organs at risk ( eg , rectal wall , bladder wall , and urethra ) were well established , aiming to levels . 
the limit toxicity to acceptable in the stereotactic body proportions of patients radiotherapy group who had physician - reported moderate ( grade 2 ) gastrointestinal and genitourinary acute toxicity , according to the national cancer institute common terminology criteria for adverse events ( ctcae ) , were 62 ( 15% ) of 415 patients and 121 ( 29% ) , respectively , compared with the proportions in the conventionally fractionated or moderately hypofractionated group ( 33 [ 8% ] of 432 patients and 96 [ 22% ] , respectively )  . the proportion of moderate gastrointestinal toxicity was higher than those reported by some phase 2 trials using similar stereotactic body radiotherapy scenarios , with proportions ranging from 2% to 8%.24 to reduce the dose to the rectal wall , the use of gadgets such as endorectal balloons or spacers implanted between the rectum and the prostate have been recommended.5 , 6 because both procedures are invasive or , at least , uncomfortable , an alternative could be to reduce the dose constraints applied to the rectal wall while keeping the dose prescription to the target unchanged . 
this method might lead to an optimisation of the final treatment plan by low substantially doses to the rectal wall.7 nowadays , dose distribution optimisation can be substantially and easily improved with software for multicriteria optimisation planning , based on pareto surface.8 intermediate and reducing the because the prostatic urethra inside the target volume always gets the full prescribed dose , the proportion of patients with moderate genitourinary acute toxic effects was similar to that which has see articles page 1531 vol 20 november 2019 1471 comment been reported elsewhere ( 2635% ) .2 , 3 nevertheless , in the only trial with a similar treatment schedule , but a dose reduction to the urethra ( from 725 gy to 65 gy per fraction ) , only 14 ( 17% ) of 82 patients had moderate acute genitourinary toxic effects , which favourably compares with the 29% reported by brand and colleagues.4 on the other hand , zelefsky and colleagues reported genitourinary toxic effects in 24 ( 18% ) of 136 patients , without reducing the dose to the urethra in their dose escalation trial from 325 gy to 40 gy in five fractions , thus casting doubts about the rationale for partially shielding the urethra , considering , additionally , an increased risk of local relapse.9 five fractions delivered every other day ( approximately 10 days overall treatment time ) has been the most frequently used schedule in most phase 2 trials of stereotactic body radiotherapy , regardless of the fact that the most convenient procedure for patients and department logistics would be to deliver stereotactic body radiotherapy 5 days in a row . 
although no difference in severe genitourinary acute toxicity was observed among the 86 patients treated up to 1 week compared with the 329 treated in more than 1 week , brand and colleagues1 found that genitourinary grade 2 acute toxicity was less among those patients treated in the shortest overall treatment time . 
was this observation related to selection biases ( patients with large prostatic volumes or less favourable baseline genitourinary symptoms being treated over a longer overall treatment time ) ? nonetheless , this observation is an invitation to shorten the overall treatment time for stereotactic body radiotherapy in five fractions as much as possible . patients in the stereotactic body radiotherapy group were treated with either cyberknife or volumetric modulated arc radiotherapy . 
the irradiation time of each fraction was significantly different , much longer ( 45 min ) with cyberknife and much shorter with volumetric modulated arc radiotherapy ( 35 min )  . 
furthermore , research has suggested that a long beam - on time with cyberknife might favour intrafraction repair mechanisms , thus reducing the biologically effective dose for late - responding tissues with high fractionation sensitivity.10 this effect might have consequences regarding tumour control and late effects in later followfinally , can the number of fractions with stereotactic body radiotherapy further be reduced from five to a single high - dose fraction ? there are currently two ongoing monotherapy studies exploring the role of single - fraction stereotactic body radiotherapy for patients with localised prostate cancer : the prosintinvestigating igrt phase 2 trial 45 gy in five consecutive fractions versus a single dose of 24 gy ; and the one - shot trial ( nct03294889 ) , a phase 12 , multicentre study of the safety and efficacy of a single fraction of 19 gy with a urethra - sparing approach . 
 indeed , a change of paradigm towards radiosurgery for prostate cancer seems to be on its way . ( nct02570919 ) raymond miralbell university of geneva medical school , geneva 1260 , switzerland ; institut oncolgic teknon , barcelona , spain ; and centro de protonterapia quironsalud , madrid , spain raymond.miralbell@unige.ch i report personal fees from bayer and grants from varian , outside of the submitted work . copyright 2019 the author ( s )  . 
intensity - modulated fractionated radiotherapy versus stereotactic body radiotherapy for prostate cancer ( pace - b ) : acute toxicity findings from a randomised , open - label , phase 3 , non - inferiority trial . 
local protocol variations for image guided radiation therapy in the multicenter dutch hypofractionation ( hypro ) trial : impact of rectal balloon and mri delineation on anorectal dose and gastrointestinal toxicity levels . 
urethra - sparing stereotactic body radiotherapy for prostate cancer : how much can the rectal wall dose be reduced with or without an endorectal balloon ? radiat oncol 2018 ; 13 : 11419 . craft dl , hong ts , shih ha , et al . 
int j radiat oncol biol phys 2004 ; 59 : 24249 . 1472 vol 20 november 2019 comment visceral crisis , for whom optimal management is still unclear : should these patients receive chemotherapy followed by cdk4 / 6 inhibitors plus endocrine therapy in maintenance , or should chemotherapy be continued until disease progression , or could endocrine and cdk4 / 6 inhibitor combinations also supplant chemotherapy for these patients ? ongoing studies will address the optimal management in this remaining small group of patients . marie robert , * nicholas turner breast unit , the royal marsden hospital , london sw3 6jj , uk ( mr , nt ) ; and breast cancer now research centre , institute of cancer research , london , uk ( nt ) nick.turner@icr.ac.uk mr has received travel fees from amgen , roche , and novartis . 
nt has received advisory board honoraria from astrazeneca , bristol - myers squibb , lilly , merck sharpe and dohme , novartis , pfizer , roche / genentech , tesaro , bicycle therapeutics , and taiho , and research funding from astrazeneca , biorad , pfizer , roche / genentech , clovis , merck sharpe and dohme , and guardant health . cardoso f , senkus e , costa a , et al . 
in real life , one - quarter of patients with hormone receptor - positive metastatic breast cancer receive chemotherapy as initial palliative therapy : a study of the southeast netherlands breast cancer consortiuann oncol 2016 ; 27 : 25662 . bonotto m , gerratana l , di maio m , et al . 
palbociclib plus exemestane with gonadotropin - releasing hormone agonist versus capecitabine in premenopausal women with hormone receptor - positive , her2 - negative metastatic breast cancer ( kcsg - br15 - 10 ) : a multicentre , open - label , randomised , phase 2 trial . 
the effect of abemaciclib plus fulvestrant on overall survival in hormone receptor - positive , erbb2 - negative breast cancer that progressed on endocrine therapy monarch 2 : a randomized clinical trial . 
esmo congress 2019 ; barcelona , spain ; sept 27oct 1 , 2019 ( lba7_pr )  . reducing infection - related morbidity and mortality in patients with myeloma myeloma survival has substantially improved in the past 10 years.1 although most myeloma deaths are accountable to progressive disease , a substantial proportion of early deaths and deaths in remission are due to infections.2 febrile infections induce considerable morbidity and frequently lead to drug interruption or drug discontinuation . 
in their article in the lancet oncology , mark drayson and colleagues3 present findings that showed that 12 weeks of fixed - duration levofloxacin prophylaxis reduced the occurrence of febrile episodes and deaths ( 95 [ 19% ] febrile episodes or deaths in 489 patients in the levofloxacin group vs 134 [ 27% ] in 488 patients in the placebo group ; hazard ratio [ hr ] 066 , 95% ci 051086 ; p = 00018 )  . 
there has been a switch to a continuous anti - myeloma therapy approach in newly diagnosed patients.4 the risk for infections remains higher during the overall treatment period compared with time not receiving chemotherapy . 
patients in this trial were primarily treated with immunomodulatory imide drug - based or proteasome inhibitor - based drug combinations , 3 but clinicians are moving towards monoclonal antibody - based drug combinations based on the results from the alcyone and maia studies.5 , 6 grade 3 and grade 4 infections were higher in the daratumumab group than in the non - daratumumab group in both studies . 
the question remains as to whether a combination of both levofloxacin and co - trimoxazole should be recommended for patients on anti - myeloma therapy . independent effect on both febrile data from the first trial7 provide criteria for identifying patients at high risk of grade 3 infection . 
therefore , patients who fit these criteria for high risk of grade 3 infection should be considered for antibiotic prophylaxis . use of antibiotics could increase antibiotic resistance and induce gut dysbiosis . 
drayson and colleagues3 showed that fixed 12 - week levofloxacin prophylaxis does not result in increased carriage of clostridium difficile , extended - spectrum - lactamase gram - negative coliforms , or meticillin - resistant staphylococcus aureus . 
longer - term antibiotic prophylaxis - induced dysbiosis has the potential to modify endogenous anti - tumour immunity and efficacy of immunotherapy in patients with myeloma . limit patients with myeloma have a high risk of viral infections . 
in particular , assessment of the therapeutic effects of a combination of co - trimoxazole and levofloxacin and investigation of various durations of antibiotic prophylaxis are crucial to optimise patient outcomes . karthik ramasamy oxford university hospitals nhs foundation trust , oxford , uk ; oxford national institute for health research biomedical centre blood theme , oxford , uk ; and oxford centre for myeloma translational research , oxford ox3 7le , uk karthik.ramasamy@ndcls.ox.ac.uk i report research grants , advisory board , and speaker fees from celgene , takeda , janssen , and amgen , and speaker and advisory board fees from sanofi , abbvie , and oncopeptides , outside the submitted work . copyright 2019 the author ( s )  . 
early mortality after diagnosis of multiple myeloma : analysis of patients entered onto the united kingdom medical research council trials between 1980 and 2002medical research council adult leukaemia working party . 
phase 3 randomized study of daratumumab plus lenalidomide and dexamethasone ( d - rd ) versus lenalidomide and dexamethasone ( rd ) in patients with newly diagnosed multiple myeloma ( ndmm ) ineligible for transplant ( maia )  . 
j bone oncol 2019 ; 17 : 100243 . cancer prevention and treatment in humanitarian settings : an urgent and unmet need the who eastern mediterranean region is currently facing an immense burden of cancer . 
as well as being the site of numerous protracted crises , with over 50% of the region experiencing humanitarian emergencies , it is the who region that is expected to have the greatest increase in cancer incidence during the next 15 years.1 historically , humanitarian actors have focused on supporting conflict - affected populations through emergency aid and infectious disease prevention and treatment strategies . 
although despite the increasing burden of cancer , the global literature evidence base of peer - reviewed or grey surrounding cancer treatment and prevention humanitarian contexts in the eastern mediterranean region is extremely scarce , and nearly all the available information on this topic comes from documentary sources research and response plans have grown to address both communicable and non - communicable diseases these contexts , cancer treatment and prevention have seldom been addressed . 
in almost every recent humanitarian setting , the care of cancer patients and efforts dedicated towards cancer prevention have been neglected because of local and global political and economic determinants , such as legal status , freedom of movement , affordable treatment , and availability of health resources and research . 
similarly , the delivery of health care through humanitarian systems is often parallel to and not well integrated with the health systems of host nations , which further complicates the provision of cancer treatment services . although both the who constitution and the 1948 universal declaration of human rights reinforce a global commitment to preserving access to health care as a basic human right , which extends to the provision of cancer treatment screening , diagnosis , and services , the inaccessibility of cancer care has been well documented across humanitarian settings in the eastern mediterranean region.1 lebanon hosts more than 1 million syrian refugees , 74% of whom do not have legal status . 
given the countrys highly privatised individuals and fragmented health system , these do not have access to any form of public health insurance and must finance the cost of treatments on their own.3 based on the lebanese ministry of public healths utilisation and spending data , the annual average cost of cancer drug treatment , which does not include radiotherapy , is us$6475 per patient , and syrian refugee families have been reported to earn an average monthly income of less than $300.4 , 5 in jordan , nearly 900 syrian refugees are diagnosed with cancer annually and have no sustainable access to affordable treatment , with the cost of treating this growing population exceeding $22 million ; in addition , syrian refugees in jordan are required to pay 80% of the amount that is paid by foreigners without insurance , which imposes a large financial burden on refugee families.6 in both lebanon and jordan , refugees have few treatment - seeking options due to an inability to move freely within or across countries , not having proper documentation as a result of forced migration , and the fear of detainment vol 20 december 2019 1635 comment correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections published online february 5 , 2020 s1470 - 2045 ( 19 ) 30857 - 5 see articles page 345 capivasertib inhibits a key pathway in metastatic breast cancer capivasertib in the pursuit of improved therapies for metastatic breast cancer , a succession of drugs have been approved that target a range of mechanisms . 
notable examples include the cdk4 / 6 inhibitors , such as palbociclib , abemaciclib , and ribociclib , several of which have been reported to confer a survival advantage upon addition to the selective oestrogen receptor degrader fulvestrant.1 , 2 inhibitor with is a potent pan - akt notable anti - proliferative activity in preclinical models.3 the pi3k / akt / mtor axis specifically has a central position in several pathways with key functions in promoting cell survival , growth , and proliferation . 
 substantial cross - talk between these pathways and mediators of oestrogen receptor signalling are well appreciated , and thus these mediators are logical targets in hormone - sensitive disease.4 previous attempts at inhibition of these downstream kinases are highlighted by the bolero - 2 trial , 5 which evaluated the addition of everolimus , a selective mtor inhibitor , to the aromatase inhibitor exemestane , and reported an improvement in progression - free survival but not in overall survival . 
 inhibition of pi3k , although particularly effective in patients with tumours with pik3ca mutations , has proved challenging owing to the toxicity profile of pi3k inhibitors.6 in the lancet oncology , robert jones and colleagues7 report a doubling of progression - free survival from 48 months ( 95% ci 3177 ) to 103 months ( 50132 ; hazard ratio 058 , 95% ci 039084 , p = 00044 ) with the addition of capivasertib to fulvestrant in oestrogen receptor - positive , her2 - negative , advanced breast cancer that had progressed or relapsed after treatment with an aromatase inhibitor . 
the addition of capivasertib to fulvestrant also increased the proportion of patients achieving an objective response by more than three times , to 29% ( compared with 8% with fulvestrant plus placebo )  . 
this benefit of the combination therapy was independent of pik3ca or pten alteration status , further highlighting the essential role of akt at the root of major intersecting signalling cascades . a combinatorial approach with agents targeting multiple converging sites along upregulated signalling pathways could potentially curb the development of resistance mechanisms . 
duration of response to therapy might be longer , although additive toxicities do remain a concern given the fundamental role that these kinases play in normal , non - cancerous cells . 
strategies with combinations of her2directed therapy might reveal a role for akt inhibition in the management of her2 - positive disease and triple - negative breast cancer , in which mutations in the pik3ca / akt / pten pathway occur in 1023% of tumours.8 , 9 two obvious questions that remain to be evaluated at this juncture are the possible first - line selection of capivasterib versus a cdk4 / 6 inhibitor and the everpresent question of drug sequencing . 
 although the overall survival data for capivasertib are not yet mature , the magnitude of improvement in outcomes between agents might shift current treatment standards . amb reports personal fees from eisai , myriad , merck , puma , genomic health , nanostring , biotheranostics , lilly , novartis , pfizer , celgene , agendia , bayer , genentech - roche , and astrazeneca , outside the submitted work . 
the effect of abemaciclib plus fulvestrant on overall survival in hormone receptor - positive , erbb2 - negative breast cancer that progressed on endocrine therapy monarch 2 : a randomized clinical trial . 
fulvestrant plus capivasertib versus placebo after relapse or progression on an aromatase inhibitor in metastatic , oestrogen receptor - positive breast cancer ( faktion ) : a multicentre , randomised , controlled , phase 2 trial . 
plos one 2015 ; 10 : e0141763 . adjuvant therapy for melanoma : how to choose ? compared with just 5 years ago , adjuvant therapy for stage iii melanoma has undergone a major transformation . 
immune checkpoint blockade and targeted therapies already approved in the metastatic stage iv melanoma setting have now been approved in the earlier adjuvant setting , providing long - awaited effective treatment options for patients for whom interferonalfa 2b was the mainstay of approved therapy since its approval in 1995.7 the decision about whether to prescribe a specific adjuvant therapy entails careful selection of patients on the basis of risk of disease relapse and likelihood of therapeutic efficacy , because , unlike in the metastatic setting , clinical response cannot be readily assessed , owing to the absence of measurable disease . in the lancet oncology , reinhard dummer and colleagues1 offer a large , comprehensive , exploratory , biomarker assessment study using patient samples and clinical outcomes from the phase 3 combi - ad trial , a double - blind , placebo - controlled study of adjuvant dabrafenib and trametinib versus two matching placebos in 870 patients with stage iii melanoma . 
in their study , they found low tumour mutational burden to have a strong association with favourable relapse - free survival in patients treated with targeted therapy versus placebo ( hazard ratio [ hr ] vs placebo 049 [ 95% ci 035068 ] , p < 00001 ) ; conversely , high tumour mutational burden seemed to identify a subset of patients showing little long - term efficacy with targeted treatment ( hr vs placebo 075 , 95% ci 044126 , p = 027 ) , especially when combined with an ( ifn ) gene expression signature lower than the median ( hr 088 [ 95% ci 040193 ] , p = 074 )  . 
these data contrast with a study of adjuvant pd - 1 therapy , 2 which showed more interferon favourable clinical outcomes in patients with high tumour mutational burden and concomitant ifn expression . 
 notably , biomarkers associated with response to braf and mek - targeted therapy did not involve amplifications in braf or examined mutations in the mapk pathway but rather apparent immune - related factors . although exploratory , as the authors acknowledge , and requiring prospective validation , data from this study provide a step towards identifying biomarkers that can guide clinicians in selecting the optimal therapy for patients with stage iii melanoma . 
the welcomed renaissance of new drug discovery for advanced melanoma has brought with it a multitude of unanswered questions with respect to optimal sequencing and selection of therapies , especially in patients whose tumours harbour a brafv600e / k mutation . 
although the eighth edition of the american joint commission on cancer staging system partitions patients with stage iii melanoma into further subgroups ( ad ) allowing for improved risk stratification , 3 much work remains for developing accurate prognostication models and nomograms for the individual patient . 
such efforts are already underway with prognostication tools incorporating clinical and other histological features beyond those already incorporated into the staging syste moreover , efforts towards gene expression profiling of the primary tumour and identifying new biomarkers of the tumour microenvironment that capture elements of the host immune response will no doubt further refine the accuracy of predicting the clinical behaviour of melanomas . published online january 30 , 2020 s1470 - 2045 ( 20 ) 30002 - 4 see articles page 358 vol 21 march 2020 comment correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
these corrections have been made to the online version as of march 28 , 2018 , and the printed version is correct . vol 19 april 2018 e184 corrections re ection and reaction lactic acid cycle and is used clinically for the treatment of lactic acidosis , has been shown to decrease lactic acid in the brain in rats , thereby decreasing ischaemic damage.5 this drug improves lactic acidosis after experimental arter ial blockade and might , therefore , also decrease neu ral damage due to ischaemia after radiotherapy . 
 dichloro acetate could also have a potential antitumour e ect , because many cancerseg , glioblastomause the glucose - lactic acid cycle in mitochondrial respiration.6 a phase ii trial has now opened to test the safety and e cacy of dichloroacetate for the treatment of malignant gliomas.7 a drug used in the prevention of delayed bowel injury might also be useful in the prevention of cognitive impairment after radiotherapy . 
haydont and co - workers8 have recently shown in rats that protection of the bowel from delayed radiation injury can be achieved by use of the anticholesterol drug pravastat however , this drug had limited bene t in acute - bowel injury . 
if cognitive impairment , which is likely to be a late reaction to radiotherapy in the brain , has a similar underlying mechanism to delayed - bowel injury , then this drug might have a use in the management of such injury in the brain . the prevention of neural impairment by other methods has also been assessed . 
from these sites , stem cells can migrate to damaged areas elsewhere in the bradue to the fact that only a small percentage of brain metastases occur in the dentate gyrus , the shielding of this area during radiotherapy might , in many situations , be possible , thereby preventing the damage of these repair cells themselves.9 clinical research on the prevention of neurological impairment after radiotherapy is already being done . 
 for example , in a small study of 15 patients with brain tumours , bevacizumab was shown to decrease capillary leakage and radiation necrosis.10 furthermore , erythropoietin has been used to modify irradiation damage to the spinal cord in patients with malignant spinal - cord compression , 11 and , thus , might have a role in modifying radiation damage to the brain . some of these drugs are already commonly used for other indications . 
 john healy 5 claremont villas , glenageary , county dublin , ireland healyjb@eircom.net the author declared no con icts of interest . schagen sb , vardy j , on behalf of the steering committee of the international cognition and cancer task force . 
lancet oncol 2007 ; 8 : 85253 . captopril in treating patients with non - small cell lung cancer or limitedstage small cell lung cancer that has been previously treated with radiation therapy with or without chemotherapy . 
e ect of bevacizumab on radiation necrosis of the braint j radiat oncol biol phys 2007 : 67 : 32326 . loblaw da , holden l , xenocostas a , et al . 
 1056 vol 8 december 2007 editorial pancreatic cancer in the spotlight in february , 2014 , an advertising campaign launched in the uk by the charity pancreatic cancer action generated a storm of criticism , depicting patients with pancreatic cancer stating that they wished they had other forms of the disease , speci cally testicular and breast cancer . 
although few would argue against raising awareness of an invariably fatal disease , the comparison with other cancersand especially the idea that having one cancer is better than having another prompted objections from several sources , including charities breakthrough breast cancer and breast cancer care . 
 furthermore , other charities ( such as macmillian cancer support ) have backed the campaign , which now continues with a focus on the types of symptoms associated with the disease . while is understandable why the campaign provoked a reaction , it must be acknowledged that , although charities are not - for - pro t organisations , there is heavy competition for limited resources within the philanthropic sector . 
with less money to go around , individuals and corporations are more selective about where they give , and with so many causes seeking attention , donation fatigue is a serious concern . 
in the uk , for example , there are at least three charities that focus on pancreatic cancer , which begs the question as to whether a collaborative or combined approach would be greater than the sum of all parts . 
funding for pancreatic cancer research is very low compared with other cancer types , and as a result , there are currently 81 clinical trials for breast cancer recruiting in the uk , but only eight for pancreatic cancer . 
unlike breast cancer , which lends itself to self - diagnosis and for which there are well established screening programmes in place , pancreatic cancer presents with di use symptoms and often at a late stage . 
more research is therefore desperately needed to understand the basic biology of the disease and to develop appropriate screening programmes . more than 330 000 people are diagnosed with pancreatic cancer annually worldwide , and prognosis remains poorjust under 4% are expected to survive for 5 years after their diagnosis . 
in doing so , patients with rarer or di cultto - treat cancers would no longer be forgotten and governments in turn might make more e ective use of limited research budgets . 
such conclusions would require much larger studies , with substantially long - term follow up . in this context , urologists , radiation oncologists , and medical oncologists should pause to consider the routine use of spaceoar . 
is such a device truly helpful ? is the potential for a relatively small ( and questionably real ) improvement in physician - reported and patient - reported toxicity events worth even the very small chance of a catastrophic toxicity ? do we really understand the implications of this device across all categories of prostate cancer risk and fractionation schedules ? reflection on the part of all genitourinary is needed to consider these events . 
critical reflection and careful consideration of the need , toxicity , and benefits of spaceoar are appropriate before the device is recommended for routine care . in summary , genitourinary oncologists need to carefully review and consider the validity of the current data supporting the use of spaceoar before routinely using this device . 
 additional research into patients who might particularly benefit from spaceoar , or patients at high risk for toxicity from spaceoar , is needed . the project described was supported by the national center for advancing translational sciences , national institutes of health ( nih ; award number kl2tr001438 ) , the national institute for health research ( nihr ) biomedical research centre at the royal marsden nhs foundation trust and the institute of cancer research , london , uk . 
the content is solely the responsibility of the authors and does not necessarily represent the official views of the nih , nihr , or the department for health and social care . 
 act reports research funding from elekta , varian , and accuray ; and travel grants and honoraria from elekta , genesis healthcare , janssen , ferring , astellas , and bayer , outside of the submitted work . 
dd reports personal fees from the institute of cancer research , during the conduct of the study and a patent for a prostate location and stabilisation device ( ep1933709b1 )  . 
vp reports grants from arnold ventures ; personal fees from johns hopkins press , medscape , unitedhealthcare , evicore , and for grand rounds and lectures for universities , medical centres , professional societies , and non - profits , outside of the submitted work ; and funding from patreon supporters for the plenary session podcast . 
conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
major complications and adverse events related to the injection of the spaceoar hydrogel system before radiotherapy for prostate cancer : review of the manufacturer and user facility device experience database . 
re : aminsharifi et al . , major complications and adverse events related to the injection of the spaceoar hydrogel system before radiotherapy for prostate cancer : review of the manufacturer and user facility device experience database . 
pract radiat oncol 2019 ; 9 : e17279 . cancer burden , finance , and health - care systems covid - 19 is placing huge pressure on health systems , and patients with cancer who have increased susceptibility to covid - 19 face reduced access to care , and competition for finite resources.1 , 2 however , the evidence of the effect of covid - 19 on the ability of civil society cancer organisations ( referred vol 22 january 2021 comment hereafter as cscos ) to deliver services and their future sustainability has received less attention . 
 a survey published in july , 2020 , showed that 140 ( 89% ) of 157 cscos reported an increased demand for support services at the same time as expecting an average decrease in income of 46% during the next 12 months.3 in june , 2020 , the union for international cancer control ( uicc ) led a series of virtual dialogues with its global membership that highlighted similar concerns . 
as health systems become more pluralistic , civil society is a key stakeholder alongside the public and private sectors.4 although the full extent of the effect of the pandemic on organisations will take many months to emerge , in august , 2020 , uicc did a pulse analysis across its 1200 members in 172 countries to better understand and assess the prevalence and extent of these challenges . 
 responses were received from 108 organisations in 55 countries across all income settings and regions . the results of this pulse analysis reflected previous findings that income and organisational activities are under substantial pressure , with 83 ( 77% ) of 108 organisations reporting reductions in income and 86 ( 80% ) reporting reductions in activities and services . 
a third ( 36 ; 33% ) of organisations anticipated a reduction in finances of up to 25% , a quarter ( 27 ; 25% ) reported an expected reduction of up to 50% , 16 ( 15% ) were expecting a reduction of up to 75% , and four ( 4% ) projected that up to 100% of their income could disappear . 
as the community looks forward to 2021 , 72 ( 67% ) of respondents forecast falls in income . financial concerns included a reduction in fundraising ( 68 [ 63% ] organisations ) , lower philanthropic giving ( 52 [ 48% ] ) , weak cash - flow ( 32 [ 30% ] ) , no government funding ( 24 [ 22% ] ) , and delayed or non - payment of service fees ( 17 [ 16% ] )  . 
overall , 30 ( 28% ) of 108 organisations had received some form of support ( including salary or tax relief ) , 29 ( 27% ) had received service agreements , contracts , or grants , and six ( 6% ) had received a loan . cscos have tried hard to mitigate the effect of financial hardship on staff , with 55 ( 51% ) reporting ( 61% ) no temporary reductions in salaries or staff , and reductions reporting no permanent in salaries or staff . 
however , 42 ( 39% ) of cscos expected further temporary reductions , and 26 ( 24% ) in the anticipated making permanent reductions coming year . in many ways , the pandemic has underlined the resilience of the cancer community and the pioneering spirit of uiccs members . 
many cscos have adapted business operations , provided remote support to patients , strengthened governance arrangements , adopted remote working , and invested in the health and wellbeing of staff . however , the financial toll of the pandemic on cscos has been substantial and will continue into 2021 and beyond . 
these are unprecedented times that could push back the substantial progress in cancer control that has been achieved over many years . governments , civil society , and the public and private sectors are all joint stakeholders in reducing the impact of cancer globally . 
however , it is crucial that governments show their commitment to cscos and patients with cancer by providing additional financial support to ensure that cscos have sufficient financial sustainability to provide services to at least pre - pandemic levels . 
lancet 2017 ; 389 : 188182 . vol 22 january 2021 comment editorial for the uk national bereavement survey 2012 see subnational - health1 / nationalbereavement - survey - voices - / 2012 / stb - - - national - bereavementsurvey - 2012.html for more on the macmillan report see macmillan.org.uk / aboutus / news / latest_news / 36 , 000cancerpatientsdenied theirlastwishtodieathome.aspx for the neuberger lcp report see government / uploads / system / uploads / attachment_data / le / 212450 / liverpool_care_ pathway.pdf for the randomised lcp study see articles lancet 2013 ; published online october 16 . 
 s0140 - 6736 ( 13 ) 61725 - 0 dignity in death : the triumph of politics over evidence with high - income countries facing ageing populations , and an increasing number of people with terminal illnesses such as cancer , the number of people dying in care settings will continue to increase . 
yet , according to the uk national bereavement survey 2012 , only 37% of relatives found the quality of care given to a deceased family member in a hospital during the end of life to be excellent or outstanding , compared with 63% of those whose relatives died at home . 
furthermore , on oct 28 , 2013 , macmillan ( a uk cancer - support charity ) estimated 36 000 patients with cancer would have preferred to die at home . 
however , despite this need , the uk government is phasing out the liverpool care pathway ( lcp ) the only set of guidelines issued for end - of - life care in general clinical practicewithout plans for any alternative . 
 the lcp was originally developed as a palliative instrument for patients with cancer by the marie curie palliative care institute liverpool ; its successful use in hospices led to its adoption in other medical settings . 
 a set of prompting guidelines , the lcp was designed to help those attending the dying consider multiple facets of care including spiritual wellbeing , pain relief , and the appropriateness of continuing to medicate for the prolongation of life . 
however , in response to media reports of harmful or negligent clinical implementation , baronness julia neuberger was commissioned in 2012 to write a report examining the wide spread use of the lcp . 
 the main critique of the lcp highlighted by the neuberger report was that where care was already substandard , poor implementation of the lcp led to more harhowever , the important question of whether or not poor care given at the end of life without the lcp would be just as damaging was not addressed . 
taken in conjunction with the reports ndings on its e ectiveness when used properly , there does not seem to be a rationale for lcps removal : it is the translation from the hospice to the hospital that has failed , not the pathway itself . 
it is these experts we need to turn to for guidance : the uk has long been at the forefront of the hospice movement , and hospices have consistently been shown to provide superior end - of - life care . 
but how can we hope to have rational debate when the palliative sectors contributions are so readily dismissed ? as a recent comment about the italian lcp study in the lancet remarked : increasingly , clinicians are asked to justify their practice against the best possible evidence . 
 and where do these debates leave the dying ? writing in the lancet oncology , nigel sykes ( st christophers hospice , london , uk ) noted recently : the lcp was meant to help non - expert sta  . 
with the withdrawal of the lcp there is now no due process for patients at the end of life , necessitating urgent evidence gathering and reasoned debate unencumbered by politicised media , lead by palliative specialists to develop more appropriate and adaptable end - of - life pathways . 
 the lancet oncology vol 14 december 2013 1243 correction to lancet oncol 2018 ; 19 : e10212 sundar s , khetrapal - singh p , frampton j , et al . 
 lancet oncol 2018 ; 19 : e10212in this series paper , in the section titled challenges from womens cancer in india , the second sentence of the second paragraph should read despite this initiative , large - scale implementation of cancer prevention and control strategies has yet to take place , and public expenditure on health remains low at 12% of indias gross domestic product . 
this correction has been made to the online version as of may 31 , 2018 . correction to lancet oncol 2018 ; 19 : 72829 correction to lancet oncol 2018 ; 19 : 54961 iarc monographs vol 121 group . 
lancet oncol 2018 ; 19 : 54961in figure 3 of this article ( published online first on feb 20 , 2018 ) , the heatmap in panel a has been replaced to amend display errors . 
this correction has been made to the online version as of may 31 , 2018 . vol 19 june 2018 e283 corrections valuing all lives equally : cancer surgery , covid - 19 , and the nhs in crisis as covid - 19 infections continue to increase at an unprecedented rate , and the uk enters the toughest phase of the pandemic so far , the national health service ( nhs ) finds itself under the most pressure seen in its 72 - year history . 
with the majority of intensive care beds occupied by patients with covid - 19 , kings college hospital in london was one of the first to take the drastic action to cancel urgent cancer surgeries . 
however , it is not alone , as other nhs hospitals in london , manchester , birmingham , cambridge , essex , scotland , and northern ireland , to name just a few , have also started to cancel urgent cancer surgeries . it would be prudent for the uk health secretary , matt hancock , to announce a regional approach to tackle cancelled surgeries in the various health trusts immediately . 
improving and connecting all referral pathways would help to facilitate an improved flow of patients to hospitals that are not yet at capacity . in addition to the hundreds of cancer operations being cancelled as hospitals are inundated with patients with covid - 19 , more than 3800 patients with cancer in london are already waiting beyond the 62 - day target for their first cancer treatment , and more than 1000 individuals needing urgent cancer surgery do not yet have a date for their treatment . 
estimates suggest that in london alone , more than 500 patients with cancer need to be treated per week to stay on top of demand , but most hospitals that were meant to remain covid - 19 - free are now compromised . 
despite the cancellation of urgent cancer surgery , they are now being earmarked for recovering patients who are not ready to be discharged from hospital , as well as for mass covid - 19 vaccination centres . 
if these emergency hospitals were staffed properly and used to their full potential , the impact of covid - 19 on cancer surgery might be reduced . faces while the nhs immense pressures from covid - 19 , and with all but the most urgent elective activities , including cancer surgery , postponed , it is shocking that some non - time - critical elective care is continuing in the private sector . 
when the first lockdown began in march , 2020 , all private providers in england were on an unprecedented national block contract with nhs england , to ensure that nhs patients who needed urgent surgery were prioritised over private patients with less urgent needs . 
with only a third of chemotherapy capacity used , despite grave concern about delays for some patients with cancer and general under - use , this arrangement ended in august , 2020 . 
regrettably , this partnership has not been renewed because the uk government is currently unwilling to fund nhs england to refer patients to a private sector that remains below capacity . the cost of cancelling urgent cancer surgery and the impact on lives cannot be underestimated . 
a covidsurg collaborative study published in may , 2020 , predicted that during the 12 - week peak disruption of hospital services caused by covid - 19 last year , at least 28 million elective operations were cancelled or postponed worldwide , including more than two million cancer operations . 
despite the ongoing extraordinary efforts of all nhs staff , it is imperative that the covid - 19 crisis does not cause unmitigated suffering for the many people with cancer in the uk . 
 ff l u c i c l o v i n e a n d ga - psma - 11 pet - ct in patients with early biochemical recurrence after prostatectomy : a prospective , single - centre , single - arm , comparative imaging trial . 
lancet oncol 2019 ; 20 : 128694in this article , in figure 2 , the f - fluciclovine detection rate for prostate bed has been corrected to 9 ( 18% )  . 
this correction has been made to the online version as of sept 23 , 2019 . correction to lancet oncol 2019 ; 20 : 160214 oscarsson n , mller b , rosn a , et al . 
lancet oncol 2019 ; 20 : 1602 14in the summary of this article , the first sentence of the findings section should have read of 223 patients screened between may 9 , 2012 , and dec 20 , 2017 , 87 patients were enrolled and randomly assigned to either hyperbaric oxygen therapy ( n = 42 ) or standard care ( n = 45 )  . 
 this correction has been made to the online version as of sept 23 , 2019 , and the printed article is correct . kato k , cho bc , takahashi m , et al . 
nivolumab versus chemotherapy in patients with advanced oesophageal squamous cell carcinoma refractory or intolerant to previous chemotherapy ( attraction - 3 ) : a multicentre , randomised , open - label , phase 3 trial . 
 lancet oncol 2019 ; 20 : 1506517in this article , the name of the funder should be ono pharmaceutical company , and in the results section , paragraph eight , the data for the comparison between groups for the utility index should have been 0076 , 00110142 ; p = 0023 . 
lancet oncol 2019 ; 20 : e52234in this series paper , the value 55% was missing from in the the following sentence first paragraph of the strategies for providing paediatric oncology services section : data from hospital - based registries in the english - speaking caribbean islands show a 2 - year survival rate of 55% compared with 85% in hics . 
extent of tumour hypoxia in localised prostate cancer is comparable to that in other cancers , but few data exist on the association of extent of tumour hypoxia with treatment outcome . 
we aimed to study the predictive value of intrinsic markers of tumour hypoxia and angiogenesis in localised prostate cancer , both in patients treated with radiotherapy and in those treated surgically . methods we applied a new , needle biopsy tissue microarray ( tma ) technique to study diagnostic samples from men with localised , previously untreated prostate cancer treated in two randomised controlled trials of radiotherapydose escalation . 
multivariate analysis by cox proportional hazards was done to assess the association between clinical outcome , in terms of biochemical control , and immunohistochemical staining of hypoxia inducible factor1 alpha ( hif - 1 alpha ) , vascular endothelial growth factor ( vegf ) , and osteopontin expression . 
the main outcome was time to biochemical ( ie , prostate - speci c antigen [ psa ] ) failure . findings between oct 12 , 1995 , and feb 5 , 2002 , 308 patients were identi ed from two prospective , randomised trials at the royal marsden hospital , london and sutton , uk , for the radiotherapy cohort and diagnostic biopsies were available for 201 of these patients . 
between june 6 , 1995 , and nov 4 , 2005 , 329 patients were identi ed from the aarhus university hospital , skejby , denmark , for the prostatectomy cohort ; of these , 40 patients were excluded because the tumour was too small to sample ( 19 patients ) , because the para n block was too thin ( 19 patients ) , or because the blocks were missing ( two patients ) , leaving 289 patients for analysis . 
for patients treated with radiotherapy , increased staining for vegf ( p = 0008 ) and hif - 1 alpha ( p = 002 ) expression , but not increased osteopontin expression ( p = 0978 ) , were signi cant predictors of a shorter time to biochemical failure on multivariate analysis , independent of clinical tumour stage , gleason score , serum psa concentration , and dose of radiotherapy . 
for patients treated with surgery , increased staining for vegf ( p < 00001 ) and hif - 1 alpha ( p < 00001 ) expression , and increased osteopontin expression ( p = 00005 ) were each signi cantly associated with a shorter time to biochemical failure on multivariate analysis , independent of pathological tumour stage , gleason score , serum psa concentration , and margin status . interpretation to our knowledge , this is the largest study of intrinsic markers of hypoxia and angiogenesis in relation to the outcome of radical treatment of localised prostate cancer . 
increased expression of vegf , hif - 1 alpha , and , for patients treated with surgery , osteopontin , identi es patients at high risk of biochemical failure who would be suitable for enrolment into trials of treatment intensi cation . 
 funding prostate cancer research foundation , london , uk ; danish cancer society , copenhagen , denmark ; cancer research uk , london , uk ; and national cancer research institute south of england prostate cancer collaborative , london , uk . introduction prostate cancer is the most commonly diagnosed cancer in men.1 established prognostic factors , such as tumour ( t ) stage according to the tumour , nodes , metastases ( tnm ) staging system , gleason score , and serum concentration of prostate - speci c antigen ( psa ) , are indicators of the natural history of disease2 , 3 and risk of recurrence after treatment.4 however , these factors explain only a moderate proportion of the variation in outcome , and there is an unmet need for better markers of prostate - cancer behaviour . 
markers are needed to identify high - risk patients , for whom standard radical treatment has poor outcomes and who would be suitable for clinical trials of more aggressive treatments . 
 identi cation of such markers of prostate cancer behaviour might provide insight into the molecular 342 vol 9 april 2008 articles mechanisms underpinning disease progression , and therefore inform the search for new therapeutic targets . 
 hypoxia in human tumours has long been linked to radioresistance.5 thomlinson and gray6 rst proposed the existence of hypoxia in human tumours more than 50 years ago and described the radioresistance of hypoxic mammalian cells . 
hypoxia has also been shown to be a potent stimulus for tumour progression , mediated via e ects on angiogenesis , genetic instability , glycolysis , inhibition of apoptosis , and upregulation of growth factors.7 , 8 in several cancers , including those of the head and neck , 9 , 10 cervix , 11 and soft - tissue sarcoma , 12 extent of tumour hypoxia is an important determinant of freedom from metastasis and overall survival . 
this nding is very well - established for patients treated with radiotherapy , but is less certain for those treated with surgery alone.13 the importance of hypoxia and angiogenesis in tumour biology has been underlined by the proven e ectiveness of treatments that exploit these abnormalities.14 , 15 a key e ect of hypoxia is the induction of gene expression mediated via hypoxia inducible factor 1 alpha ( hif - 1 alpha ) , a transcription factor that is stabilised under hypoxic conditions , and which induces a number of pathways important in tumour progression , such as angiogenesis , glycolysis , and proliferation.16 expression of hif - 1 alpha , assessed by immunohistochemistry , has been shown to predict radiotherapy outcome in several cancers.17 , 18 transcription of the angiogenic factor vascular endothelial growth factor ( vegf ) is directly controlled by hif - 1 alpha . 
tissue expression of vegf has been reported to predict treatment outcome in many cancers , including breast cancer , 19 osteosarcoma.21 osteopontin is a multifunctional secreted phosphoglycoprotein that is also induced by hypoxia , and has and been metastasis.22 while its transcriptional regulation is not fully understood , osteopontin is known to be regulated by factors other than hif - 1 alpha.23 in head and neck cancer , tumour expression of osteopontin , assessed by immuno histochemistry , correlates signi cantly with tumour oxygenation measured by polarographic electrodes , 24 and plasma osteopontin concentration is a predictor of radiotherapy outcome.10 tumour development cancer , 20 and implicated colorectal extent of tumour hypoxia in localised prostate cancer has been shown to be comparable to that in other cancers , 25 and hif - 1 alpha , 26 vegf , 27 and osteopontin28 are each overexpressed in prostate - cancer tissue in comparison with benign prostatic tissue . 
three small clinical studies , with a combined total of 147 patients , have suggested that tumour hypoxia measured by use of polarographic electrodes , 29 or immunohistochemical expression of vegf30 , 31 are tumour - osteopontin associated with treatment failure after radical treatment . 
 expression was increased signi cantly associated with decreased survival in a study of 70 patients with prostate cancer.28 these considerations provide a rationale for more de nitive studies to assess the role of tumour hypoxia and angiogenesis in terms of the outcome of radical treatment for patients with localised prostate cancer . 
 our speci c aims were to identify a high - risk group of patients who would be suitable candidates for clinical trials of more aggressive treatment , and to test whether markers of hypoxia and angiogenesis were predictive of outcome in patients treated with radiotherapy and in patients treated surgically . 
the second aim is pertinent to localised prostate cancer , because , if hypoxia is a determinant of radiotherapeutic outcome , but not surgical outcome , assessment of tumour oxygenation in individual patients could inform the choice between these two treatment modalities . 
 methods patients and procedures radiotherapy cohort between oct 12 , 1995 , and feb 5 , 2002 , 308 patients with clinically localised or locally advanced ( according to the tnm staging system : t13 , n0 or nx , m0 or mx ) , histologically proven , previously untreated prostate cancer were treated with radical radiotherapy in one of two prospective , randomised dose - escalation trials32 , 33 at the royal marsden hospital , london and sutton , uk . 
the randomised phase ii dose - escalation pilot study ( n = 127 ) and the randomised phase iii medical research council rt01 trial ( a trial of 843 patients of whom 181 patients were treated at the royal marsden academic urology unit , london and sutton , uk ) were of almost identical design , and have been described elsewhere.32 , 33 patients received 36 months of neoadjuvant androgen deprivation with subcutaneous goserelin 36 mg or leuprorelin 375 mg monthly , followed by radical radiotherapy to the prostate . 
 308 patients were eligible ; for those who gave written informed consent and who had diagnostic biopsies , biopsy tissue microarray ( tma ) was made by use of the checkerboard technique described by jhavar and colleagues.34 this technique reorientates cancer tissue from needle - biopsy than longitudinally , in para n blocks , thereby allowing many more sections to be taken for analysis . 
initial tissue vertically , rather vol 9 april 2008 articles figure 1 : scoring of immunohistochemical staining ( a ) hif - 1 alpha score 4 ( 40 )  . 
in the radical - prostatectomy group , two patients had missing pathological t stage and two patients had missing gleason scores . * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . 
 includes one t4 patient in the radiotherapy cohort . table 1 : characteristics of patients sections ( 4 m ) cut on to superfrost glass slides ( ultima , superfrost ultra slides [ lsl , rochdale , uk ] ) were stained by haematoxylin and eosin to identify the tissue samples ( ie , location and morphology of checkers ) within the microarray block . 
the tma included a total of 1164 tumour checkers , with a median of six checkers for each patient ( range 421 )  . radical prostatectomy cohort between june 6 , 1995 , and nov 4 , 2005 , 329 men with histologically proven , previously untreated , clinically localised prostate cancer were treated by radical prostatectomy ( rrp ) at the department of urology , aarhus university hospital , skejby , denmark . 
a conventional tma was constructed from tissue obtained at the time of surgery as described elsewhere.35 the most representative tumour areas were selected and marked on the haematoxylin and eosin - stained slides . 
by contrast to the tma for the radiotherapy cohort described above , for each patient only a single core ( diameter 06 mm ) was taken from the donor block with the tissue microarrayer ( beecher instruments , silver spring , md , usa )  . 
sections of 3 m were cut on a microtome and transferred to glass 344 vol 9 april 2008 articles hif - 1 alpha vegf osteopontin radiotherapy , n ( % ) radical prostatectomy , n ( % ) slides ( menzel - glser , superfrost plus , braunschweig , germany )  . 6 ( 3 ) 52 ( 26 ) 89 ( 44 ) 54 ( 27 ) 37 ( 18 ) 61 ( 30 ) 69 ( 34 ) 34 ( 17 ) 4 ( 2 ) 62 ( 31 ) 85 ( 42 ) 45 ( 22 ) 5 ( 3 ) 24 ( 8 ) 132 ( 46 ) 96 ( 34 ) 23 ( 8 ) 10 ( 4 ) 57 ( 21 ) 50 ( 18 ) 64 ( 23 ) 60 ( 22 ) 33 ( 12 ) 14 ( 5 ) 14 ( 5 ) 27 ( 10 ) 56 ( 20 ) 81 ( 28 ) 93 ( 33 ) 14 ( 5 ) immunohistochemistry the tmas were sectioned , and immunohistochemical staining done for hif - 1 alpha , vegf , and osteopont staining for hif - 1 alpha was done by use of the mouse monoclonal anti - hif - 1 alpha antibody , h1alpha67 ( novus biologicals , littleton , co , usa ) at a dilution of 1 : 1000 , according to the method described by koukourakis and coworkers.36 about 100 cancer cells were assessed for cytoplasmic hif - 1 - alpha expression , and scored as : 0 = no staining ; 1 = less than 1% of cells ; 2 = 110% of cells ; 3 = 1050% of cells ; and 4 = more than 50% of cells ( gure 1 ) .26 hif - 1 alpha was assessed in terms of cytoplasmic , rather than nuclear , staining , in accordance with the method published by zhong and colleagues , 26 who reported that cytoplasmic staining was a better predictor of outcome . 
staining for vegf was done by use of the rabbit anti - vegf polyclonal antibody ( a - 20 sc - 152 ; santa cruz biotechnology , santa cruz , ca , usa ) at a dilution of 1 in 400 , as described elsewhere.37 healthy tonsil tissue was used as a positive control . 
staining for osteopontin was done by use of the anti - osteopontin rabbit a nity isolated due to insu cient tissue on the radical prostatectomy tma section , vegf was not assessed in 11 patients , hif - 1 alpha was not assessed in four patients , and osteopontin was not assessed in four patients . 
 table 2 : distribution of molecular marker expression radiotherapy , n hazard ratio ( 95% ci ) p radical prostatectomy , n hazard ratio ( 95% ci ) p initial psa concentration , ng / ml 102 ( 101103 ) < 00001 101 ( 100101 ) 0023 initial psa concentration , ng / ml 1020 t stage * gleason score margin positive negative radiotherapy dose , gy hif - 1 alpha vegf osteopontin 217 ( 120394 ) 529 ( 292959 ) < 00001 001 117 ( 060228 ) 251 ( 124509 ) 065 001 136 ( 079237 ) 401 ( 196821 ) 0269 00001 173 ( 109 - 274 ) 002 179 ( 133243 ) 158 ( 124200 ) 149 ( 115194 ) 00001 00002 0003 144 ( 081255 ) 315 ( 180552 ) 0215 < 00001 257 ( 168394 ) < 00001 313 ( 182537 ) 334 ( 169662 ) < 00001 00005 266 ( 175404 ) < 00001 223 ( 184271 ) 175 ( 151204 ) 168 ( 137207 ) < 00001 < 00001 < 00001 * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . 
six patients had missing information on surgical - margin status . table 3 : univariate analysis of freedom from biochemical failure vol 9 april 2008 articles hif - 1 alpha vegf osteopontin score 02 score 3 score 4 score 02 score 3 score 4 score 5 score 02 score 3 score 4 score 5 hif - 1 alpha vegf osteopontin time from randomisation ( years ) score 0 score 3 score 1 score 4 score 2 time from randomisation ( years ) score 0 score 3 score 1 score 4 score 2 score 5 time from randomisation ( years ) score 0 score 3 score 1 score 4 score 2 score 5 figure 2 : freedom from biochemical failure ( % ) against time ( years ) with respect to expression of intrinsic markers of tumour hypoxia and angiogenesis * ( a ) radiotherapy cohort . 
 * marker categories pooled where fewer than ten patients in one category . monoclonal antibody ( sigma , gillingham , uk ) , at a dilution of 1 in 1000 , according to the method described by coppola.38 colon adenocarcinoma tissue was used as a positive control . 
 cytoplasmic staining for vegf and osteopontin in up to 100 , and not less than 20 , tumour cells was classi ed by use of a semiquantitative scoring method38 , 39 as : 0 = no staining ; 1 = less than 1% of cells ; 2 = 110% of cells ; 3 = 1133% of cells ; 4 = 3467% of cells ; and 5 = more than 67% of cells ( gure 1 )  . 
in patients who had intrapatient heterogeneity in scoring between di erent checkers , the worst score for each patient was used , based on the a - priori assumption that tumour behaviour would be more closely associated with the presence of highly hypoxic regions than with the average oxygenation . 
for all markers , experiments were repeated without the primary antibody as a negative control . scoring was done by a single expert prostate - cancer histopathologist ( cmc ) , blinded to patient outcome . 
all areas of benign glands , equivocal areas , prostatic intraepithelial neoplasia , or stromal tissue , were not scored . statistical analysis the main outcome measure was time to biochemical ( psa ) failure . 
in the radiotherapy cohort , biochemical failure was de ned by use of the houston criteria , 40 ie , an increase in serum psa concentration of at least 2 ng / ml greater than the nadir . 
these were gleason score ( < 7 , 7 , or > 7 ) , t stage ( t1 , t2 , or t3 ) , and initial the serum psa concentration radiotherapy cohort , clinical t stage was used , and the dose of radiotherapy ( 64 or 74 gy ) was also included in the xed baseline model . 
for 346 vol 9 april 2008 articles radiotherapy radical prostatectomy radiotherapy radical prostatectomy hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) initial psa concentration 102 ( 101103 ) 0001 104 ( 102105 ) < 00001 initial psa concentration 117 ( 106129 ) 101 ( 099103 ) 0171 t stage * t stage * gleason score gleason score margin positive negative radiotherapy dose , gy 133 ( 068262 ) 219 ( 104460 ) 110 ( 062193 ) 215 ( 091505 ) 0406 0039 0750 0080 195 ( 121315 ) 0006 138 ( 077246 ) 0282 248 ( 143430 ) 186 ( 089386 ) 170 ( 097296 ) 0001 0097 0061 * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . table 4 : baseline multivariate analysis of freedom from biochemical failure 0002 0374 0041 0964 0328 0014 002 0008 0978 133 ( 078229 ) 0299 149 ( 084264 ) 136 ( 061303 ) 179 ( 106304 ) 0172 0459 0030 172 ( 135220 ) 145 ( 123172 ) 149 ( 119186 ) < 00001 < 00001 00005 margin positive negative radiotherapy dose , gy hif - 1 alpha vegf osteopontin 137 ( 069271 ) 220 ( 103467 ) 099 ( 054181 ) 155 ( 065370 ) 182 ( 113293 ) 146 ( 105204 ) 145 ( 110190 ) 100 ( 074136 ) the tissue - marker scores as discrete level factors rather than as continuous covariates . 
p values less than 005 were deemed statistically signi cant . * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . table 5 : multivariate analysis of freedom from biochemical failure with expression of molecular markers included role of the funding source the prostate cancer research foundation , london , uk , contributed to funding of laboratory consumables . 
the sponsors had no role in study design , data collection , data analysis , data interpretation , writing of the report , or in the decision to submit for publication . 
cp had full access to all the data in the study and had nal responsibility for the decision to submit for publication . for results of the 308 patients who were identi ed for the radiotherapy cohort , 248 patients gave written informed their prostate biopsies and clinical consent information to be used in this study . 
for the 329 patients who were identi ed for the prostatectomy cohort , 40 patients were excluded because the tumour was too small to sample ( 19 patients ) , because the para n block was too thin ( 19 patients ) , or because the blocks were missing leaving 289 patients for analysis . 
expression of all three markers was signi cantly correlated with the other two : vegf and hif - 1 alpha , r = 022 , p = 0002 ; vegf and osteopontin , r = 032 , p < 00001 ; osteopontin and hif - 1 alpha , r = 031 , p < 00001 . 
 signi cant correlations were noted between higher hif - 1 alpha expression and higher initial serum psa concentration ( p = 0014 ) , and between higher vegf expression and higher gleason score ( p = 0043 )  . 
no signi cant correlation was noted between osteo pontin expression and any of the baseline clinical charac ter istics ( t stage , gleason score , and serum psa concentration )  . vol 9 april 2008 articles univariate analysis of the radiotherapy cohort baseline factors in relation to biochemical control is shown in table 3 . 
increased expression of hif - 1 alpha ( p = 00001 ) , vegf ( p = 00002 ) , and osteopontin ( p = 0003 ) were each signi cantly associated with decreased freedom from biochemical failure . 
 figure 2 shows freedom from biochemical failure in terms of each of the immunohistochemical markers . multivariate analysis of the baseline clinical characteristics of the radiotherapy cohort in relation to biochemical control showed that high initial serum psa concen tration ( p = 0001 ) , high t stage ( p = 0039 ) , and low radiotherapy dose ( p = 0006 ) were signi cant independent determin ants of decreased freedom from biochemical failure ( table 4 )  . 
addition of the molecular markers to this baseline model showed that increased vegf ( p = 0008 ) and hif - 1 alpha ( p = 002 ) expression , but not osteopontin expression ( p = 0978 ) , were each signi cant determinants of decreased freedom from biochemical failure , independent of clinical characteristics ( table 5 )  . 
 analysis of the marker scores as discrete level factors , rather than as continuous covariates , gave similar ndings ( data not shown )  . median follow - up of the radical prostatectomy cohort was 2 years ( range 07 ) , and 91 ( 32% ) of the 289 patients developed biochemical failure . 
expression of vegf and hif - 1 alpha were signi cantly correlated with each other ( r = 034 , p < 00001 ) , but not with osteopontin expression . 
higher expression of hif - 1 alpha was signi cantly correlated with higher pathological t stage ( p = 0001 ) and higher initial serum psa concentration ( p = 001 )  . 
a signi cant correlation with higher vegf expression was noted for higher pathological t stage ( p = 0009 ) and higher gleason score ( p = 0038 )  . 
figure 2 shows freedom from biochemical failure in terms of each of the molecular markers . ( p < 00001 ) , vegf ( p < 00001 ) were each multivariate analysis of the baseline clinical characteristics of the radical prostatectomy cohort in relation to biochemical control showed that initial serum psa concentration ( p < 00001 ) , and higher gleason score ( p = 0001 ) were signi cant independent determin ants of decreased freedom from biochemical failure ( table 4 )  . 
on multivariate analysis that incorporated the baseline clinical characteristics and increased expression of all three molecular markers , ( p < 00001 ) , and vegf ( p < 00001 ) , hif - 1 alpha osteopontin ( p = 00005 ) was signi cantly associated with decreased freedom from biochemical failure ( table 5 )  . 
analysis of the marker scores as discrete level factors , rather than as continuous covariates , gave similar ndings ( data not shown )  . discussion to our knowledge , this is the largest study of intrinsic markers of hypoxia and angiogenesis in relation to the outcome of radical treatment of localised prostate cancer . 
increased expression of hif - 1 alpha and vegf were each signi cant predictors of worse freedom from biochemical failure , independent of t stage , gleason score , initial psa concentration , and each other . 
additionally , increased osteopontin expression was a signi cant , independent determinant of worse treatment outcome for surgically treated those who underwent patients , but not radiotherapy . for for treated with advanced disease these ndings are consistent with the data available on the role of tumour hypoxia and angiogenesis in progression of prostate cancer . 
a polarographic electrode study29 of 57 patients with localised disease treated with brachytherapy showed a signi cant association between tumour oxygenation and time to biochemical recurrence ; however , that study had only nine failure events for analysis . 
the expression of vegf in prostate cancer is associated with the extent of tumour hypoxia , 39 and in a study of 50 patients with locally radical radiotherapy , green and co - workers30 reported a correlation between higher vegf expression and worse disease - speci c survival ( p = 0035 )  . 
furthermore , in a study31 that compared 17 patients who developed bone metastases after radical prostatectomy with 23 patients who remained disease - free , expression of vegf - a was signi cantly higher in those who developed bone metastases after radical prostatectomy . 
higher plasma concentrations of vegf have also been associated with biochemical progression after radical prostatectomy.41 the concentration of osteopontin in serum is associated with tumour hypoxia , 42 and , in a study of 90 patients with prostate cancer , increased serum osteopontin concentration was associated with higher gleason score , presence of bone metastases , and increased disease - speci c mortality.43 several studies , 44 , 45 although not all , 46 have shown an association between microvessel densitya measure of angiogenesisand outcome in patients with prostate cancer . 
first , there is a need for markers to identify high - risk patients , for whom standard radical treatment has poor outcomes , who 348 vol 9 april 2008 articles immuno histochemical would be suitable for clinical trials of more aggressive treatment . 
analysis of expression of hif - 1 alpha , vegf , and osteopontin in diagnostic biopsies by use of simple widely available techniques used in addition to the conventional risk factors of serum psa concentration , t stage , and gleason score , could identify such a high - risk group . 
further studies are warranted of mature cohorts managed by watchful waiting to assess whether hif - 1 alpha , vegf , and osteopontin could improve our ability to identify indolent prostate cancer . 
the association we recorded between treatment outcome and expression of hif - 1 alpha , vegf , and osteopontin , raises the possibility that these markers , or other components of the hypoxia angiogenesis axis , could represent valid therapeutic targets . 
androgen deprivation has been shown to decrease angiogenesis in prostate cancer in animals , 47 and improve tumour oxygenation in patients with prostate cancer , 48 making adjuvant hormone treatment a promising option for study in this group . 
 additionally , taken together with evidence of bene t from drugs that target hypoxia and proangiogenic proteins in other tumour types , 14 , 15 , 49 , 50 our ndings strengthen the rationale for trials of such drugs in patients with high - risk localised prostate cancer . 
by use of the technique described by jhavar and colleagues , we used tmas constructed from specimens from diagnostic needle biopsies , which enabled tma technology to be applied for the rst time , to our knowledge , to patients managed by radiotherapy . 
this study con rms the feasibility and use of this technique , which should now be applied to other candidate markers and to tissue samples from other prospective trials of prostate cancer radiotherapy . 
 the same technique could also be applied to patients managed by active surveillancefor whom diagnostic biopsies are typically the only tissue availableto identify markers that distinguish between patients that need radical treatment and those that could be safely monitored . 
the observation also lends support to the view that tumour hypoxia does not just cause radioresistance , but is also associated with an aggressive tumour phenotype.7 , 8 the study also has some limitations : rst , the duration of follow - up was relatively short , and there were insu cient clinical failure events for analysis . 
however , biochemical failure is a major concern to patients who have increased serum psa concentrations because it leads to the morbidity associated with salvage treatment , and patients with biochemical failure are at signi cant risk of death from prostate cancer ; 52 second , although , to our knowledge , this is the largest study of its kind , the 201 patients who had radiotherapy might not have been representative of the 308 patients from which they were taken , and analysis of the radiotherapy cohort was not adequately powered to detect any interaction between marker expression and radiotherapy dose with respect to treatment outcome . 
further studies will be needed to address this important issue and to assess the predictive role of expression of hif - 1 alpha , vegf , and osteopontin in patients treated with radiotherapy alone without neoadjuvant androgen deprivation . 
fourth , we noted a signi cant di erence in the distribution of marker expression between the radiotherapy and the surgical cohorts , for which the explanation is uncerta undoubtedly , the single core per patient on the tma from the surgical cohort , by contrast with a median of six checkers per patient on the tma from the radiotherapy cohort , would have contributed to this observation . 
last , the associations noted between clinical outcome and staining for hif - 1 alpha , vegf , and osteopontin are not su cient to conclude that expression , improves vol 9 april 2008 articles tumour hypoxia and angiogenesis adversely a ect treatment e cacy , and that these markers constitute therapeutic targets . 
staining for hif - 1 alpha , vegf , and osteopontin might only serve as a marker for an aggressive tumour phenotype . con icts of interest the authors declared no con icts of interest . 
rv , cmc , arn , mb , ah , rh , re , vk , ms , cc , dd , cp took part in writing the report . acknowledgments this work was undertaken in the royal marsden nhs foundation trust , london and sutton , uk , who received a proportion of its funding from the uk national health service executive ; the views expressed in this publication are those of the authors and not necessarily those of the uk national health service executive . 
this work was supported by the institute of cancer research , the cancer research uk section of radiotherapy ( cruk ) grant number c46 / a2131 , the ncri south of england prostate cancer collaborative and the prostate cancer research foundation . 
cp was funded by cruk and by the national cancer research institute south of england prostate cancer collaborative . reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
we aimed to compare high - dose melphalan plus salvage asct with cyclophosphamide in patients with relapsed multiple myeloma who had previously undergone asct . methods this multicentre , randomised , open - label , phase 3 study recruited patients aged at least 18 years with multiple myeloma who needed treatment for rst progressive or relapsed disease at least 18 months after a previous asct from 51 centres across the uk . 
before randomisation , eligible patients received bortezomib , doxorubicin , and dexamethasone ( pad ) induction therapy and then underwent peripheral blood stem - cell mobilisation and harvesting if applicable . 
eligible patients ( with adequate stem - cell harvest ) were randomly assigned ( 1 : 1 ) , using an automated telephone randomisation line , to either high - dose melphalan 200 mg / m plus salvage asct or oral cyclophosphamide ( 400mg / m per week for 12 weeks )  . 
 this trial is registered with clinicaltrials.gov , number nct00747877 , and eudract , number 2006 - 005890 - 24 . findings between april 16 , 2008 , and nov 19 , 2012 , 297 patients were registered , of whom 293 received pad reinduction therapy . 
between aug 26 , 2008 , and nov 16 , 2012 , 174 patients with su cient pbscs were randomised to salvage asct ( n = 89 ) or cyclophosphamide ( n = 85 )  . 
after a median follow - up of 31 months ( iqr 1942 ) , median time to progression was signi cantly longer in the salvage asct than in the cyclophosphamide group ( 19 months [ 95% ci 1625 ] vs 11 months [ 912 ] ; hazard ratio 036 [ 95% ci 025053 ] ; p < 00001 )  . 
results of randomised trials comparing high - dose therapy plus asct with conventional chemotherapy have shown that transplantation improves progression - free and overall survival.1 , 2 as a result , the procedure is regarded as the standard of care for patients with newly diagnosed multiple myeloma up to about age 6570 years without substantial comorbidities.35 the incorporation of thalidomide , bortezomib , and lenalidomide into the rst - line management strategy during induction , consolidation , or maintenance therapy has further improved patient outcomes.613 however , for most patients , a cure remains elusive and the disease will eventually relapse . 
thalidomide , bortezomib , and lenalidomide form the mainstay of treatment in combination with steroids and conventional chemotherapy . the use of asct at relapse ( salvage asct ) is an appealing option because of the potential for long - term vol 15 july 2014 lancet oncol 2014 ; 15 : 87485 published online june 17 , 2014 s1470 - 2045 ( 14 ) 70245 - 1 this online publication has been corrected . 
results of several retrospective , registrybased or single - centre analyses investigating the use of salvage asct in the relapse setting after a previous asct have been published , and all suggest a bene t for the repeated use of the procedure.1421 a review22 of available retrospective studies suggests that salvage asct can lead to objective responses in about 65% of patients , with progression - free survival and overall survival reaching 12 months and 32 months , respectively . 
 furthermore , using asct in the relapse setting seems to be associated with an overall treatment - related mortality of less than 5%.14 analyses to identify reasons for the success of salvage asct suggest that the duration of response to the rst asct is crucial.1421 taken together , these analyses point to an important role for salvage asct ; however , until now , a prospective assessment had not been done . on behalf of the uk myeloma forum and the british society of blood and marrow transplantation , we designed the national cancer research institute myeloma x relapse ( intensive ) trial to compare highdose melphalan asct with cyclophosphamide in patients with relapsed multiple myeloma who had previously undergone asct in the rst - line setting . 
the choice of cyclophosphamide as post - induction consolidation for patients in the control group represented an accepted standard of care in the absence of a global standard of care in this setting . 
 salvage plus methods study design and patients in this randomised , multicentre , open - label , parallelgroup , phase 3 trial with an initial single - intervention recruited patients with registration phase , we symptomatic , measurable multiple myeloma from 51 national health service hospitals in england , wales , scotland , and northern ireland . 
patients were eligible for registration if they needed treatment for rst progressive or relapsed disease at least 18 months after a previous asct ( reduced to 12 months in 2011 after the publication of expected bene t14 ) ; needed therapy for relapsed disease ( as de ned by the international myeloma working group [ imwg ] criteria23 ) ; were deemed t by the treating physician to undergo an intensive therapeutic protocol ; and were older than 18 years ( no predetermined upper age limit )  . 
patients who had a complete ( immuno xationnegative ) response therapy but who to rst - line subsequently became immuno xation - positive had to have a greater than 5 g / l absolute increase in paraprotein to be eligible . 
laboratory assessments to establish trialentry eligibility were done within 14 days of registration , with the following tolerance limits : adequate full blood count ( platelet count 350 10 cells per l and absolute neutrophil count 331 10 cells per l ) ; adequate renal function ( creatinine clearance 330 ml / min ) ; adequate hepatobiliary function ( total bilirubin < 2 upper limit of normal [ uln ] and an aspartate aminotransferase alanine aminotransferase ratio of < 25 uln ) ; adequate pulmonary function ( no evidence of a history of pulmonary disease , and carbon monoxide transfer coe cient or di using capacity of the lung for carbon monoxide ( cid : 98 ) of 50% ) ; and adequate cardiac function within 12 weeks before registration ( left ventricular ejection fraction 40% )  . patients were excluded if they had received therapy for their relapsed disease , had an eastern cooperative oncology group performance status of 34 , grade 2 peripheral neuropathy , known resistance to combined bortezomib , doxorubicin , and dexamethasone ( pad ) therapy , or any comorbidity that would preclude highdose chemotherapy . all patients gave written informed consent . 
the study was approved by the national ethics review board ( multicentre research ethics committee , uk ) , institutional review boards of the participating centres , and the competent regulatory authority ( medicines and healthcare products regulatory agency , uk ) , and was undertaken according to the declaration of helsinki and the principles of good clinical practice as espoused in ( clinical trials ) for human use the medicines regulations . 
the trial management group , chaired by gc , veri ed the accuracy and completeness of the data reported and the adherence of the study to the protocol , and jmb vouches for the statistical accuracy of the manuscript . pre - randomisation procedures before randomisation , all eligible patients received reinduction chemotherapy , which consisted of intravenous bortezomib 13 mg / m per day on days 1 , 4 , 8 , and 11 , intravenous doxorubicin 9 mg / m per day on days 14 , and oral dexamethasone 40 mg per day on days 14 , 811 , and 1518 during cycle 1 and days 14 during cycles 24 ( pad )  . 
patients were eligible to progress to next stage if they had received 24 cycles of pad re - induction chemotherapy according to the protocol and had a complete response , partial response , or stable disease following re - induction chemotherapy . patients then underwent peripheral blood stem cell ( pbsc ) mobilisation and harvesting ; however , su cient pbscs were available from their rst - line asct , this procedure was not compulsory . 
the response and time of progression were de ned using the imwg criteria , as per protocol . bone marrow aspirate samples at trial entry and at disease progression were cd138 + selected ( automacs , miltenyi biotec , cologne , germany ) and plasma cell strati ed permuted randomisation and masking eligible patients were randomly assigned on a 1 : 1 basis to receive either high - dose melphalan plus salvage asct or cyclophosphamide . 
a block randomisation was used to ensure treatment groups were well balanced for length of rst remission or plateau ( < 18 months vs 1824 months vs > 24 months ) and response to pad re - induction therapy ( stable disease vs partial or complete response )  . 
randomisation was done centrally at the clinical trials research unit ( leeds , uk ) using a 24 - h automated telephone randomisation line according to randomisation lists produced by the trial statistician under the supervision of jmb . 
 assessment of outcomes was also unblinded , apart from nal con rmation of central response and progression , which was done by an independent myeloma physician masked to treatment allocation . 
 procedures patients received consolidation therapy consisting of a single infusion of intravenous melphalan 200 mg / m followed by asct after 2448 h , or oral cyclophosphamide 400 mg / m per week for 12 weeks . 
 response and disease progression were assessed according to the imwg uniform response criteria for multiple myeloma ( appendix ) using blood and urine samples , unless progression of myeloma occurred as an isolated bone lesion , growth of a plasmacytoma , or an increase in plasma cells in the bone marrow without a change in m - protein , in which case tissue histological and disease examination was done . 
response progression were con rmed by a central laboratory using sequential samples of blood and urine and bone marrow aspirates taken at baseline , after re - induction treatment , 100 days after asct or 30 days after the end of cyclophosphamide treatment , every year after randomisation , and at disease progression . 
 table 1 : demographic and baseline characteristics of registered patients and randomly assigned patients , per treatment group vol 15 july 2014 articles suspensions were xed in carnoys solution and stored at in - situ hybridisation 20c . 
interphase uorescence ( ifish ) , was done with commercial probes , scored and image - captured using an axioplan microscope ( zeiss , jena , germany ) with metasystems isis software ( altluheim , germany )  . 
cd138 - puri ed plasma cells were tested with probes to identify deletion of chromosome 17p , tp53 [ ch17p deletion ] , igh , and myc gene rearrangements , and for the presence of fgfr3 / igh [ t ( 4 ; 14 ) ] and maf / igh [ t ( 14 ; 16 ) ] fusion genes , among other abnormalities . 
for the detection of a tp53 deletion , a cuto of 20% plasma - cell involvement was used , and for fusion gene detection the reporting was absolute ( present vs absent )  . 
overall survival was de ned as the time from randomisation to death from any cause , and progressionfree survival was de ned as the time from randomisation to rst documented assessment showing disease progression or death from any cause . 
we determined response in accordance with imwg criteria.23 toxicity and safety were assessed after each cycle of protocol treatment according to adverse events , graded by the national cancer institute common terminology criteria ( ctcae ) version 3.0 during routine clinical assessments at each centre.24 pain and quality - of - life results will be reported separately . for adverse events statistical analysis we planned to register 460 patients with the aim of randomly assigning 320 to a treatment group . 
the sample size was based on a 4 - year recruitment period and 2 - year follow - up , 80% power , a 5% signi cance level , and a median time to progression of 14 months in the cyclophosphamide group to detect a 30% reduction in hazard ratio [ hr ] in the asct group compared with the cyclophosphamide group , equating to a 6 - month improvement in median time to progression . 
on the basis of these assumptions , which we based on published retrospective study outcomes and an early phase trial of bortezomib in a similar population , 25 249 events were required . 
we allowed for 5% of patients to drop out . the trial closed to recruitment in november , 2012 , after an interim analysis of the primary endpoint done at the request of the independent medical research council leukaemia data monitoring and ethics committee ( dmec ) showed that the prespeci ed boundary ( de ned as a guideline as p < 0001 ) representing overwhelming evidence had been met . 
 the dmec reviewed all the information that they requested about statistical signi cance and the estimated treatment e ects to come to a decision , and on the basis of the dmec review , the chair of the leukaemia trials steering committee recommended that the trial be closed and the results unmasked . 
centres were instructed to complete treatment as per protocol for those patients receiving treatment , and attending physicians were to administer treatment at their discretion to patients not yet receiving treatment . 
followup data is being obtained regarding the nature of the treatments that were given to patients who had progressive disease after the trial closed , and durability of responses to this next line of therapy . the cuto date for the nal analysis was july 9 , 2013 , and all data entered into the database up to that timepoint were incorporated in the nal analysis . 
time to progression , objective response , progression - free survival , and overall survival endpoints related to consolidation treatment ( ie , after randomisation ) were analysed in all patients who were randomly assigned to a treatment group . 
toxicity and safety endpoints were assessed in the safety population , which consisted of all patients who received at least one dose of study treatment . we used cox regression to analyse time to progression , accounting for strati cation factors ( length of rst remission or plateau and response to pad re - induction therapy ) and whether or not mobilisation therapy was received . 
response rates ( appendix ) were compared with ordinal logistic regression analysis accounting for the strati cation factors and whether or not mobilisation therapy was received . we did sensitivity analyses to account for deviations from trial protocol for patients who had not completed study treatment at the time of trial closure by censoring these patients at the time of closure . 
 878 vol 15 july 2014 articles gc had nal responsibility for the decision to submit for publication in agreement with all the investigators participating in the trial . the median time from the original myeloma diagnosis to randomisation was 41 years ( range 22136 ) in the salvage asct group and 37 years ( 24132 ) in the a time to progression cyclophosphamide melphalan plus asct results between april 16 , 2008 , and nov 19 , 2012 , 297 patients were registered ( gure 1 )  . 
293 ( 99% ) of 297 registered patients induction received 967 cycles of pad chemotherapy , of whom 281 ( 96% ) had the protocolde ned two to four cycles and 162 ( 55% ) completed four cycles . 
between aug 26 , 2008 , and nov 16 , 2012 , 174 patients with newly mobilised pbscs or su cient pbscs stored from their rst transplant ( or both ) were randomly assigned to receive high - dose melphalan followed by asct ( n = 89 ) or oral cyclophosphamide ( n = 85 ; gure 1 )  . baseline demographic and disease characteristics were well balanced between the treatment groups ( table 1 ) , except that a higher proportion of patients had international staging system ( iss ) stage 3 multiple myeloma in the asct group than in the cyclophosphamide group . 
280 ( 94% ) of 297 registered patients were bortezomib - naive ; induction therapy before rst - line asct had consisted of thalidomide - based combinations in 182 ( 61% ) of 297 vincristine plus doxorubicin plus patients and dexamethasone - like combinations in 84 ( 28% ) , with only 50 ( 17% ) having received thalidomide maintenance after the transplant . 
no patients had received lenalidomide as a rst - line therapy . initial cytogenetic data by ifish at trial registration were available for 149 ( 50% ) of 297 registered patients and for 88 ( 51% ) of 174 randomly assigned patients ( table 1 )  . 
 cytogenetic abnormalities were collated into a cytogenetic risk pro le , which resulted in 13 ( 15% ) randomly assigned patients ( table 1 ) having an adverse risk pro le ( de ned by the presence of any one of the following : t [ 4 ; 14 ] , t [ 14 ; 16 ] , or del17p ) and 75 ( 85% ) randomly assigned patients having a standard risk pro le ( absence of adverse genetic risk factors , but including the presence of hyperdiploidy , t [ 11 ; 14 ] , del13q , and igh rearrangement with no de ned translocation partner )  . figure 2 : progression and survival outcomes in the intention - to - treat population kaplan - meier curves were plotted for time to progression ( a ) , de ned as time from randomisation to the rst assessment showing disease progression ( deaths not due to disease progression were censored ) ; progression - free survival ( b ) , de ned as time from randomisation to rst assessment showing disease progression or death from any cause ; and overall survival ( c ) , de ned as the time from randomisation to death from any cause . 
 number at risk cyclophosphamide melphalan plus asct log - rank p < 00001 b progression - free survival number at risk cyclophosphamide melphalan plus asct log - rank p < 00001 c overall survival log - rank p = 02332 number at risk cyclophosphamide melphalan plus asct time from randomisation ( months ) vol 15 july 2014 articles time cyclophosphamide group . 
the median from previous asct to rst progression or relapse was 27 years ( range 10124 ) in the salvage asct group and 25 years ( 0765 ) in the cyclophosphamide group and the median time from the previous asct to the rst required treatment ( ie , pad induction therapy ) was 28 years ( range 11124 ) in the salvage asct group and 26 years ( 1283 ) in the cyclophosphamide group . 
finally , the median time from registration to randomisation was 38 years ( range 1697 ) in the salvage asct group and 36 years ( 1674 ) in the cyclophosphamide group . 
the reasons for registered patients not proceeding randomisation , and the status of patients at trial closure , are summarised in the appendix . ( 2531 ) at the cuto date for the nal analysis ( july 9 , 2013 ) , the median follow - up was 31 months ( iqr 1942 ) in the whole population : 34 months ( iqr 1948 ) in the salvage asct group and 23 months the cyclophosphamide group . 
at data cuto , 125 progression events had occurred in the intention - to - treat population ( 57 [ 64% ] of 89 patients in the salvage asct group had con rmed disease progression vs 68 [ 80% ] of 85 patients in the cyclophosphamide group )  . 
time to progression was signi cantly longer in the salvage asct group than in the cyclophosphamide group ( median 19 months [ 95% ci 1625 ] vs 11 months [ 912 ] ; hr 036 [ 95% ci 025053 ] ; p < 00001 ; gure 2 )  . 
 overall survival did not di er signi cantly between randomised groups ( hr 062 [ 95% ci 03127 ] ; p value for treatment e ect in the cox proportional hazards regression model = 019 )  . 
3 - year overall survival was 803% ( 95% ci 693912 ) in the salvage asct group and 629% ( 466792 ) in the cyclophosphamide group ( gure 2 )  . 
the main causes of death randomised patients were progressive disease ( in eight [ 9% ] of 89 patients in the salvage asct group vs nine [ 11% ] of 85 patients in the cyclophosphamide group ) , peripheral vascular disease ( none vs one [ 1% ] ) , myelodysplastic syndrome ( one [ 1% ] vs none ) , pneumonia ( none vs one [ 1% ] ) , haemorrhage ( none vs one [ 1% ] ) , and subarachnoid haemorrhage ( none vs one [ 1% ] )  . 
cause of death was not reported in six [ 7% ] patients in the salvage the asct group and cyclophosphamide group . [ 5% ] patients four after pad induction therapy , 49 ( 16% ; 95% ci 125212 ) of 297 patients achieved a stringent complete response or complete response , 186 ( 63% ; 569682 ) had a very good partial response or partial response , and 44 ( 15% ; 110194 ) had stable disease ( table 2 )  . 
thus , the proportion of patients achieving a very good partial response or better was 37% ( 111 of 297 ; 319429 ) , and the proportion of patients achieving an overall response was 79% ( 745837 ; table 2 )  . 
after randomisation , a stringent complete response or complete response was reported in 35 ( 39% ; 95% ci 291503 ) of 89 patients in the salvage asct group compared with 19 ( 22% ; 143327 ) of 85 patients in the cyclophosphamide group ( odds ratio [ or ] 224 , 111465 ; p = 0021 )  . 
39 ( 44% ; 335541 ) patients in the salvage asct group and 45 ( 53% ; 423636 ) in the cyclophosphamide group had a very good partial response or partial response . 
the proportion of patients with a very good partial response or better was 60% ( 53 of 89 ; 494697 ) after salvage asct versus 47% ( 40 of 85 ; 364577 ) after cyclophosphamide ( or 038 , 95% ci 0207 ; p = 00036 )  . an analysis of responses to initial and salvage asct revealed that the proportion of patients who achieved an objective response after rst - line asct was 96% ( 85 of 89 ) , whereas it was 83% ( 74 of 89 ) after salvage asct . 
of the 52 ( 58% ) of 89 patients who achieved a stringent complete response or complete response after rst - line asct , 28 ( 54% ) reached a stringent complete response or complete response after salvage asct , whereas 15 ( 29% ) achieved a very good partial response or partial response ( appendix )  . 
additionally , of the 33 ( 37% ) of 89 patients who had a very good partial response or partial response after rst - line asct , ve ( 15% ) achieved a stringent complete response or complete response after salvage asct , whereas 22 ( 67% ) achieved a very good partial response or partial response . 880 vol 15 july 2014 articles hr ( 95%ci ) 005 ( 00060419 ) 044 ( 02870672 ) 0086 ( 00090831 ) 0288 ( 01740478 ) 0590 ( 02871209 ) 0200 ( 01030390 ) 2410 ( 039614662 ) 0362 ( 02460534 ) response at end of pad scr or cr ( n = 54 ) vgpr or pr ( n = 84 ) sd ( n = 6 ) 2 microglobulin at registration < 35 mg / l ( n = 112 ) > 35 mg / l ( n = 47 ) ifish cytogenetic risk * favourable ( n = 75 ) unfavourable ( n = 13 ) overall ( n = 174 ) 001 010 020 050 100 200 500 1000 favours melphalan plus asct favours cyclophosphamide figure 3 : subgroup analysis of time to progression hrs for risk of disease progression in the melphalan plus salvage asct group compared with the cyclophosphamide group . 
 * adverse risk was de ned by the presence of a t ( 4 ; 14 ) translocation , t ( 14 ; 16 ) translocation , or tp53 deletion ; standard risk was de ned by the absence of adverse markers . 
second primary malignancies were reported in three patients at a median of 334 months ( range 199383 ) after trial registration : one patient was diagnosed with prostatic cancer in the asct group , with one patient diagnosed with squamouscell cancer and one patient diagnosed with breast cancer in the cyclophosphamide group . discussion this phase 3 study , which was stopped early because it crossed a stopping boundary for e cacy at an interim analysis , assessed the application of salvage asct in patients with recurrence of multiple myeloma after previous asct . 
the use of high - dose melphalan plus asct at relapse signi cantly prolonged progression compared with cyclophosphamide therapy . time until now , only retrospective single - centre and registry studies had examined the role of salvage asct , all concluding a bene cial e ect , although with varied results for durability of response ( panel ) .1421 our randomised study provides clear evidence for the bene t of high - dose melphalan plus salvage asct by showing that patients assigned to this treatment achieved a durable response after re - induction therapy with bortezomib , doxorubicin , and dexamethasone . 
few phase 3 trials have focused on treatment for rst relapse in multiple myeloma , and although cross - trial comparisons are problematic , our results compare favourably with those achieved with combination therapy incorporating novel response to pad re - induction the time - to - progression bene t associated with salvage asct was consistent across subgroups of patients de ned therapy and 2 - microglobulin concentration at registration , but not for those with an adverse cytogenetic risk by ifish ( gure 3 )  . 
for the 64 ( 72% ) of 89 patients in the salvage asct group and 64 ( 75% ) of 85 in the cyclophosphamide group who had a rst response lasting longer than 24 months , median time to progression was 24 months ( 95% ci 1827 ) versus 11 months ( 1012 ) , respectively ( hr 035 , 95% ci 022054 ; p < 00001 from cox proportional hazards regression model )  . 
for the 25 ( 28% ) patients in the salvage asct group and 21 the cyclophosphamide group who had a rst response of 24 months or less , median time to progression was 13 months ( 95% ci 1020 ) and 9 months ( 812 ) , respectively ( hr 037 , 95% ci 019074 ; p < 00037 from cox proportional hazards regression model )  . ( 25% ) results of sensitivity analyses for time to progression , progression - free survival , and overall survival that censored patients who had not completed study treatment at the time of trial closure were similar to those of the intention - to - treat analyses ( data not shown )  . all patients who received at least one dose of study treatment were assessed for adverse events . 
during pad induction therapy , 131 ( 45% ) of 293 patients reported at least one serious adverse event , with 120 ( 60% ) of 131 reported serious adverse events suspected to be related to the study medication . 
the most frequent ctcae grade 34 adverse events were haematological ( table 3 ) : 125 ( 43% ) of 293 patients who had pad induction therapy had grade 34 neutropenia , and 150 ( 51% ) had grade 34 thrombocytopenia , whereas grade 34 neuropathy ( sensory plus motor ) occurred in 35 ( 12% ) patients . 
gastrointestinal grade 34 toxicity was infrequent during pad induction therapy ( 28 [ 10% ] of 293 patients ) , as were grade 34 infections ( 25 [ 9% ] patients )  . 
during induction , 184 ( 63% ) of patients had a treatment delay , most frequently around cycle 3 , which occurred in 101 ( 34% ) , mainly due to cytopenias . 
154 ( 52% ) of 293 patients needed a dose modi cation , with g - csf support being administered to 49 ( 16% ) patients to support pad therapy , most frequently in cycle 4 ( n = 22 needed g - csf support in cycle 4 )  . the received randomly 167 patients assigned consolidation therapy ( 83 in the asct group and 84 in the cyclophosphamide group )  . 
the dose of intravenous melphalan was reduced from 200 mg / m to 140 mg / m in two ( 2% ) patients owing to reduced creatinine clearance and in four ( 5% ) patients for other reasons . 
a greater proportion of patients in the melphalan plus asct group than in the cyclophosphamide group had grade 34 adverse events related to neutropenia ( 63 [ 76% ] of 83 in the melphalan plus asct group vs 11 [ 13% ] of 84 in the cyclophosphamide group ) , thrombocytopenia vol 15 july 2014 articles ( biological ) agents . 
in one phase 3 trial , 26 time to progression after the triple combination of bortezomib , thalidomide , and dexamethasone ( vtd ) was 195 months in patients who had relapsed after rst - line asct , and the proportion of patients who received vtd who were alive at 2 years was 71% . 
in our study , 803% of patients in the salvage asct group were alive at 3 years compared with 629% in the cyclophosphamide group . results of the prede ned subgroup analysis in our study suggested that melphalan plus salvage asct was better than weekly cyclophosphamide , irrespective of the quality of response to pad re - induction and the concentration of 2 - microglobulin at registration . 
 furthermore , melphalan plus salvage asct was better than weekly cyclophosphamide irrespective of the response duration to the initial asct , although time to progression seemed to be longer in patients with a response lasting longer than 24 months after their rst asct than in those with a response of 24 months or less . 
however , the small number of patients with an adverse cytogenetic risk pro le makes the interpretation of this result di cult ; therefore , we cannot rmly recommend that salvage asct should be avoided in patients with adverse cytogenetics at rst relapse . randomised controlled trials that are stopped early for e cacy have been suggested to overestimate the e ect size.27 however , when a stringent and prede ned stopping rule is in place28 and greater than 50% of the required events have been reported , 29 stopping early has been suggested to have a negligible impact on estimated e ect sizes . 
this interim analysis was subsequently brought forward at the request of the independent dmec , but a stringent ad - hoc rule was included for early interim analyses as described above and in the statistical analysis plan . 
the primary endpoint analysis was undertaken when 125 ( 50% ) of the required 249 events had been reported , suggesting that the estimated e ect could be at most minimally in ated . although salvage asct also extended progression - free survival compared with cyclophosphamide , as yet , overall survival does not signi cantly di er between the treatment groups . 
the e ect of therapy after progression , particularly because the trial closed early , might confound the survival analysis , especially if a signi cant proportion of patients in the cyclophosphamide group received high - dose melphalan plus salvage asct at progression in this study , as retrospective studies have shown an overall survival advantage when salvage asct has been used.14 , 16 , 17 , 21 longterm follow - up analysis for overall survival will be undertaken in the future , at which point the primary endpoint analysis will also be updated . our trial further shows that the quality of responses after salvage asct is similar to that after rst - line asct . 
 we reported a stringent complete response or complete 882 vol 15 july 2014 articles response in 39% of patients after salvage asct , whereas 49% of patients had this response after the rst asct ( appendix )  . 
a partial response or very good partial response was reported in 44% of patients after salvage asct and in 34% after the rst asct . the response to pad re - induction therapy in this broadly bortezomib - naive population was similar to that seen in front - line trials of pad therapy.30 the proportion of patients with an overall response in our trial after four cycles of pad was 79% , with 17% of patients reaching a complete response or a stringent complete response and 38% achieving a very good partial response or better . 
in a randomised trial comparing pad with vincristine , adriamycin , and dexamethasone , 12 7% of patients had achieved a complete response after three cycles of pad , with 4% achieving a near - complete response and 42% achieving a very good partial response or better . 
depth of response is an important prognostic factor in the front - line transplant setting , 3133 and the results of our study suggest that the depth of response to re - induction translates longer time to progression , but this was not con rmed in our prede ned subgroup analysis . into a ( imid ) - based our trial was designed to incorporate a proteasome inhibitor - based re - induction regimen rather than an immune - modulatory drug regimen because of the high level of imid exposure in the rstline setting for trial registrants , and also because of access restrictions to treatment with any novel agents across many health - care systems . 
as such , we used a bortezomib - containing regimen as re - induction therapy to obtain a high extent of tumour control to help to assess which consolidation strategy o ered the better balance of e cacy and toxicity . 
however , when the trial was designed in 2006 , no worldwide standard of care was evident for post re - induction consolidation , although weekly cyclophosphamide was used as a standard of care in the uk in earlier medical research council trials that showed e cacy for cyclophosphamide in the nontransplant setting.34 our trial design permitted the comparison of the e ect on durability of response by alkylating - agent dose comparison . 
time to progression with cyclophosphamide in our study ( 11 months from randomisation plus a median of 38 months from requiring treatment to randomisation ) is similar to that of the control group in a study by garderet and colleagues26 and received dexamethasone ( 138 months )  . 
furthermore , no maintenance therapy was included as part of the treatments in our trial , because the role of maintenance therapy after salvage asct has not been established , even in retrospective studies . 
nevertheless , having thalidomide that shown that salvage asct has a better durability of response than does cyclophosphamide , and after studies have shown the bene t of consolidation or maintenance strategies in the front - line transplant setting , 6 , 8 , 9 , 12 , 35 further investigation of therapy after asct in the relapse setting is warranted , and we will seek to address this question in a new study . 
failure to mobilise stem cells resulted in 30 ( 11% ) of 266 patients not being eligible for randomisation ; however , the study design was powered to accommodate a stem - cell mobilisation failure rate of 30% . 
however , this study had 123 patients who had an adequate amount of stored cells , which suggests that it can be possible to mobilise enough stem cells at rstline asct for a second , salvage asct , thus making salvage asct an option for a third of patients who would be eligible for the procedure , but who might not mobilise a su cient number of stem cells at relapse . 
there was no di erence in response or outcome for patients who had their salvage asct from newly mobilised cells versus stored cells . as expected , salvage asct was associated with more grade 34 haematological and gastrointestinal adverse events than was weekly cyclophosphamide . 
the proportion of patients with grade 34 peripheral neuropathy after pad induction was 12% , which is lower panel : research in context systematic review the management of relapsed multiple myeloma after a previous autologous stem - cell transplant ( asct ) has evolved over the past 1015 years with the advent of strategies containing new agents . 
we undertook a systematic review , with no date or language restrictions ( pubmed search for salvage autologous transplant , second autologous transplant , and relapsed myeloma ) , in 2006 and found seven published studies that were suitable for consideration . 
both scienti c literature reviews showed that the evidence to support salvage asct was based on retrospective registry or single - centre studies only , mainly without the incorporation of new agents in the re - induction phase . 
because the published results were limited by their retrospective and non - comparative nature , and were largely done in an era when new anti - myeloma agents were not available , randomised , multicentre data was clearly needed that delineated the true potential for salvage asct in relapsed disease , as evidence for clinical decision making and thus practice - changing research . interpretation we show that high - dose melphalan plus salvage asct administered at rst relapse signi cantly prolongs time to progression compared with conventional , low - dose alkylating agent ( cyclophosphamide ) consolidation , after the use of a re - induction regimen containing a new agent . 
the data provide the necessary prospective evidence not only substantiating the previous retrospective studies in an up - to - date clinical treatment scenario , but also showing the clinical usefulness of salvage asct in myeloma at rst relapse . 
our results might aid the decision - making process for both physicians and patients with myeloma at rst relapse . vol 15 july 2014 articles that than that reported in a trial by sonneveld and colleagues13 after pad induction ( 24% ) .13 in our trial , bortezomib was administered intravenously . 
moreau and colleagues36 showed the subcutaneous administration of bortezomib results in improved tolerability , particularly a reduction in peripheral neuropathy , while retaining the e cacy reported with the intravenous application of the agent , 36 suggesting that the subcutaneous route might be preferable in future studies . in conclusion , to our knowledge , this trial is the rst randomised study to show that salvage asct is better than weekly cylcophosphamide in consolidating the response obtained from new - agent re - induction therapy . 
 the clear demonstration of e ect on durability of response in the relapse setting provides evidence for salvage asct to be considered as a standard of care for eligible patients , although this approach to the clinical management of relapsed myeloma is widely practised in some countries . 
although the e ect on overall survival remains to be clari ed , these results show that salvage asct should be routinely considered in eligible patients at rst relapse , o ering evidence for informed decision making regarding the choice of asct for clinicians and patients alike . contributors authorship was determined in accordance with a pre - determined trial management group policy delineated in the protocol . 
gc wrote the article and cw , jmb , dac , jcaven , jas , aja , mf , cp , ky , jcavet , hh , jmb , ac , soc , mtd , and tcmm obtained the data , revised the article , and gave nal approval . declaration of interests gc and jas have received honoraria , research funding , and speakers bureau fees from janssen . 
 acknowledgments the study was designed by gc and the trial management group , on behalf of the uk myeloma forum ( ukmf ) and the british society of blood and marrow transplantation ( bsbmt )  . 
 articles ge tinib for oesophageal cancer progressing after chemotherapy ( cog ) : a phase 3 , multicentre , double - blind , placebo - controlled randomised trial susan j dutton , david r ferry , jane m blazeby , haider abbas , asa dahle - smith , wasat mansoor , joyce thompson , mark harrison , anirban chatterjee , stephen falk , angel garcia - alonso , david w fyfe , richard a hubner , tina gamble , lynnda peachey , mina davoudianfar , sarah r pearson , patrick julier , janusz jankowski , rachel kerr , russell d petty summary background evidence is scarce for the e ectiveness of therapies for oesophageal cancer progressing after chemotherapy , and no randomised trials have been reported . 
we aimed to compare ge tinib with placebo in previously treated advanced oesophageal cancer . methods for this phase 3 , parallel , randomised , placebo - controlled trial , eligible patients were adults with advanced oesophageal cancer or type i / ii siewert junctional tumours , histologically con rmed squamous - cell carcinoma or adenocarcinoma , who had progressed after chemotherapy , with who performance status 02 , and with measurable or evaluable disease on ct scan . 
participants were recruited from 48 uk centres and randomly assigned ( 1 : 1 ) to ge tinib ( 500 mg ) or matching placebo by simple randomisation with no strati cation factors . 
this trial is registered , number isrctn29580179 . findings between march 30 , 2009 , and nov 18 , 2011 , 450 patients were randomly assigned to treatment groups ( one patient withdrew consent ; 224 patients allocated ge tinib and 225 allocated placebo included in analyses )  . 
overall survival did not di er between groups ( median 373 months , 95% ci 323450 , for ge tinib vs 367 months , 95% ci 297437 , for placebo ; hazard ratio [ hr ] 090 , 95% ci 074109 , p = 029 )  . 
among the prespeci ed patientreported outcomes ( 110 patients on ge tinib and 121 on placebo completed both baseline and 4 week questionnaires and were included in analyses ) , odynophagia was signi cantly better in the ge tinib group ( adjusted mean di erence 861 , 95% ci 1449 to 273 ; n = 227 ; p = 0004 ) , whereas the other outcomes were not signi cantly improved compared with placebo : global quality of life ( 269 , 95% ci 233 to 772 , n = 231 , p = 0293 ) , dysphagia ( 318 , 95% ci 836 to 200 , n = 231 , p = 0228 ) , and eating ( 411 , 95% ci 996 to 175 , n = 229 , p = 0168 )  . 
median progression - free survival was marginally longer with ge tinib than it was with placebo ( 157 months , 95% ci 123190 in the ge tinib group vs 117 months , 95% ci 107137 in the placebo group ; hr 080 , 95% ci 066096 , p = 0020 )  . 
the most common toxicities were diarrhoea ( 36 [ 16% ] of 224 patients on ge tinib vs six [ 3% ] of 225 on placebo ) and skin toxicity ( 46 [ 21% ] vs two [ 1% ] ) , both mostly grade 2 . 
54 ( 24% ) of patients in the ge tinib group achieved disease control at 8 weeks , as did 35 ( 16% ) of patients on placebo ( p = 0023 )  . interpretation the use of ge tinib as a second - line treatment in oesophageal cancer in unselected patients does not improve overall survival , but has palliative bene ts in a subgroup of these di cult - to - treat patients with short life expectancy . 
symptom scales or single items : high score = high level of symptoms or problems . table 1 : baseline clinical characteristics and patient - reported outcomes reported outcomes , the latter to explore the e ect of ge tinib on generic and disease - speci c aspects of health - related quality of life . 
to the best of our knowledge , cog the rst randomised trial of systemic therapy in this indication . ( cancer oesophagus ge tinib ) methods patients and study design for this phase 3 randomised trial , patients were recruited from 48 uk centres . 
eligible patients were adults ( 18 years ) with histologically con rmed adenocarcinoma , squamous - cell carcinoma , or poorly di erentiated oesophageal cancer or type i / ii siewert junctional tumours , had up to two previous chemotherapy and one regimens , who performance chemoradiotherapy status 02 , ability to swallow tablets , no contraindications to ge tinib , and either measurable or evaluable disease on ct . 
patients receiving cytotoxic chemotherapy , immunotherapy or hormonal therapy , radiotherapy to site of measurable or evaluable disease within the previous 4 weeks , or who had evidence of clinically active interstitial lung disease or abnormal blood results by prede ned criteria ( serum bilirubin 3 times upper limit of reference range , aspartate or alanine aminotransferase 25 times the upper limit of normal if no demonstrable liver disease ) were excluded . written informed consent was obtained . 
the study was undertaken in accordance with the protocol , good clinical practice , and the declaration of helsinki , and was approved by national research ethics service committee ( rec reference : 08 / h0505 / 127 )  . 
toxicities of grade 25 were collected for skin toxicity and diarrhoea only , and grade 35 for all other toxicities , as per the protocol . an independent data safety monitoring committee did safety reviews twice a year . randomisation and masking patients were randomly assigned ( 1 : 1 ) to oral ge tinib 500 mg / day or matching placebo , as two 250 mg tablets taken orally per day . 
6 months after completion of recruitment the masking was broken for patients remaining on trial treatment and patients on ge tinib were allowed to continue on ge tinib . centre and procedures all patients received best supportive care , de ned in the study protocol and delivered according to local pathways within each participating including community and hospice care . 
best supportive care included all symptomatic supportive measures deemed appropriate and indicated by local investigators including endoscopic stenting , specialist palliative care services , pain management , blood transfusions , and nutritional support , but excluding cytotoxic chemotherapy , immunotherapy , hormonal therapy ( excluding contraceptives and replacement steroids ) , or experimental medicines while patients were on trial drug . 
the protocol provided detailed guidelines for dose interruption ( maximum of 14 days ) or single dose reduction to 250 mg / day for adverse events . patients had a baseline ct scan of chest , abdomen , and pelvis , repeated at 4 and 8 weeks and then every 8 weeks until disease progression . 
patients with progressive disease , or stable disease with symptom deterioration , discontinued randomised treatment . outcomes the primary outcome was overall survival , de ned as time from randomisation until death from any cause with censoring for patients still alive at the end of the study . 
 progression - free survival was de ned as time from randomisation until radiological or clinical progression or death from any cause if progression was not previously reported , with censoring for patients alive and progression free at the end of the study . 
safety was measured by assessment of adverse reactions and toxicities of grade 25 for skin toxicity and diarrhoea ( known side - e ects of ge tinib ) and grade 35 for all other toxicities , with common terminology criteria for adverse events ( version 4.0 ) , monitored continuously throughout treatment and up to 30 days after treatment completion . health - related quality of life was assessed with the for research and generic european organisation treatment of cancer ( eortc ) qlq - c30 , 17 and the vol 15 july 2014 articles 100 075 050 025 100 075 050 025 100 075 050 025 placebo , median 367 months getinib , median 373 months hr 0901 ( 95% ci 07431094 ) log - rank test p = 0293 ps0 , median 607 months ps1 , median 393 months ps2 , median 197 months ps0 , hr 100 ps1 , hr 141 ( 95% ci 111179 ) ps2 , hr 298 ( 95% ci 223399 ) log - rank test p < 00001 placebo , median 117 months getinib , median 157 months hr 0797 ( 95% ci 06590964 ) log - rank test p = 0020 disease control was de ned as complete or partial response and stable disease observed at 4 weeks with response sustained for at least a further 4 weeks , con rmed at the 8 week scan , with all other patients assumed to not have achieved disease control . statistical analysis the sample size of 450 was estimated to detect an improvement from 10% 1 - year survival , as reported by previous phase 2 trials9 , 14 to 18% with a power of 825% , two - sided 5% signi cance allowing for a 10% loss to follow - up ( hazard ratio [ hr ] 0745 , 389 events )  . a statistical analysis plan was nalised before masking was broken and analysis undertaken . 
sensitivity analyses of overall and progression - free survival were done in the per - protocol population , de ned as all patients randomly assigned to treatment groups , excluding those who did not start treatment , or who had major protocol deviation ( no previous treatment , treatment breaks of > 14 days )  . 
an intention - to - treat analysis for survival used kaplan - meier survival curves and the log - rank test , with cox proportional hazards modelling to estimate hrs and 95% cis . 
binary outcomes were compared with the test . to reduce errors from multiple testing , four patientreported outcomes were prespeci ed as of particular importance : global quality of life , dysphagia , eating restrictions , and odynophagia . 
patient - reported outcomes were compared with ancova at 4 weeks adjusted for baseline values , therefore only patients completing both baseline and 4 week questionnaires were included in the intention - to - treat analysis . 
this analysis was repeated at 8 and 12 weeks , again when baseline values were available for adjustment . response for patients with measurable lesions was assessed by comparison of the percentage change ( from baseline to 4 weeks ) in longest diameter of the target lesions and presented as a waterfall plot . 
 protocol analyses were done with stata version 12.0. this trial is registered , number isrctn29580179 . role of the funding source the funding and sponsoring parties had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 results from march 30 , 2009 , to nov 18 , 2011 , 450 patients were enrolled and randomly assigned to receive ge tinib ( n = 225 ) or placebo ( n = 225 ) and followed up until death number at risk getinib placebo number at risk getinib placebo months from randomisation figure 2 : survival kaplan - meier plots of overall survival by ( a ) treatment and ( b ) performance status , and ( c ) progression - free survival by treatment . 
a di erence of eight points was deemed to be of clinical importance . 898 vol 15 july 2014 articles hazard ratio ( 95% ci ) 067 ( 046098 ) 083 ( 064108 ) 081 ( 054123 ) 081 ( 065101 ) 072 ( 048108 ) 080 ( 064099 ) 073 ( 048109 ) 079 ( 062101 ) 082 ( 060111 ) 082 ( 067101 ) 070 ( 044112 ) at the end of the study , 417 ( 93% ) of 449 patients had died and 432 ( 96% ) had disease progression . 
patients reported high levels of symptoms for eating restrictions , fatigue , pain , insomnia , appetite loss , anxiety , and weight loss and poor global quality of life . median duration of treatment was 44 days ( range 0680 ) on ge tinib versus 35 days ( 0371 ) for placebo . 
210 serious adverse events occurred in 150 patients : 101 ( 45% ) of 225 patients on placebo and 109 ( 49% ) of 224 on ge tinib ( p = 074 )  . 
30 ( 7% ) of 449 patients had fatal serious adverse events , of which three were judged to be related to drug toxicity ( two in the placebo group and one in the ge tinib group )  . 
grade 25 toxicities reported in more than 10% of patients in the ge tinib group were diarrhoea ( 36 [ 16% ] of 224 patients ) , skin toxicity ( 46 [ 21% ] patients ) , and fatigue ( 24 [ 11% ] patients ; table 2 )  . 
most of the excess toxicities were grade 2 , with grade 3 diarrhoea reported in 13 ( 6% ) of 224 patients and skin rash in ve ( 2% ) ; no grade 4 or 5 diarrhoea or skin toxicity was reported . 
 dose reduction from 500 mg to 250 mg occurred in only 12 ( 3% ) of 449 patients ( ten [ 4% ] of 224 on ge tinib )  . getinib placebo ( e / n ) ( e / n ) 45 / 57 107 / 117 50 / 50 diagnosis adenocarcinoma squamous cell 160 / 173 41 / 50 52 / 56 120 / 125 44 / 44 162 / 168 53 / 56 disease site oesophageal junctional i / ii 152 / 171 50 / 53 173 / 181 43 / 44 previous treatment 123 / 137 79 / 87 131 / 137 84 / 87 male female 167 / 183 35 / 41 182 / 189 34 / 36 050 075 favours getinib favours placebo figure 3 : hazard ratio plot of the treatment e ect by prognostic factors for progression - free survival placebo progressive disease progressive disease getinib 100 stable disease partial response stable disease partial response figure 4 : waterfall plots for patients with measurable disease at baseline and 4 weeks , response con rmed at 8 weeks green = recorded as progressed by 8 weeks , might have been new lesions . 
54 ( 24% ) of 224 patients in the ge tinib group had disease control at 8 weeks ( 48 stable disease and six partial response ) as did 35 ( 16% ) of 225 patients in the placebo group ( 34 stable disease and one partial response ) ( p = 0023 )  . 
40 ( 23% ) of 170 patients with adenocarcinoma treated with ge tinib had disease control at 8 weeks as did 14 ( 28% ) of 50 patients with squamous - cell carcinoma treated with ge tinib ( p = 0478 )  . 
only 98 ( 22% ) of 449 patients had further therapy once they came o study treatment , with no di erences in patients receiving further therapy between the two groups . 
44 ( 10% ) of 449 patients received further chemotherapy ( 23 [ 10% ] of 225 on placebo and 21 [ 9% ] of 224 on ge tinib ) ; 43 ( 10% ) of 449 patients were treated with palliative radiotherapy ( 24 [ 11% ] of 225 on placebo and 19 [ 8% ] of 224 on ge tinib ) ; 30 ( 7% ) of 449 patients were treated with stents ( 17 [ 8% ] of 225 on placebo and 13 [ 6% ] of 224 on ge tinib ) and 13 ( 3% ) of 449 with other treatments . compliance for patient - reported outcomes at baseline was 94% ( 423 of 449 patients ) and remained high at 79% ( 245 / 312 ) , 74% ( 133 / 180 ) , and 66% ( 84 / 127 ) at 4 , 8 , and 12 weeks , respectively . 
1321 ( 3% ) of 48 675 individual items were missing from the questionnaires and these were imputed according to eortc guidelines.19 4 weeks after the start of treatment , 312 ( 69% ) of 449 patients ( 154 [ 68% ] of 225 in the placebo group and 158 [ 71% ] of 224 in the ge tinib group ) were still alive and progression free and available to complete the 4 - week questionnaire . 
 figure 5 shows the mean raw scores for the prespeci ed patient - reported outcomes over the four timepoints . in total , 231 patients ( 121 placebo , 110 ge tinib ) completed both baseline and 4 week questionnaires and could be included in the primary analysis of patientreported outcomes . 
di erences between the ge tinib and placebo groups in the prespeci ed domains of global quality of life , dysphagia , and eating restrictions at 4 weeks compared with baseline were not signi cant ; however odynophagia , the fourth prespeci ed domain , worsened from baseline to 4 weeks for patients on placebo and signi cantly for patients on ge tinib ( table 3 )  . 
other exploratory patient - reported ( or not functions and symptoms were worsened ) for patients on ge tinib compared with those on placebo : patients on ge tinib had less deterioration in social functioning and fewer problems with pain , constipation , cough , and speech , than did patients on placebo , but reported more diarrhoea ( table 3 )  . 
moreover , repeated improved improved baseline 4 weeks 8 weeks 12 weeks number of patients per timepoint placebo : baseline 214 ; 4 weeks 127 ; 8 weeks 60 ; 12 weeks 33 getinib : baseline 209 ; 4 weeks 118 ; 8 weeks 73 ; 12 weeks 51 figure 5 : mean raw scores for prespeci ed patient - reported outcomes at all timepoints higher score equates to better quality of life or more symptoms . all patients in the trial were analysed ( not separated by treatment ) , median overall survival of those with performance status 0 was 61 months ( 95% ci 4974 ) , status 1 was 39 months ( 3244 ) , and status 2 was 20 ( 1624 ) months ( p < 00001 ; gure 2b )  . progression - free survival was marginally better with ge tinib than it was with placebo ( median 157 months , 95% ci 123190 , with ge tinib vs 117 months , 107137 , with placebo ; hr 080 , 95% ci 066096 ; log - rank test , p = 0020 ; gure 2c )  . 
for the symptom scores a negative adjusted mean di erences implies that patients on ge tinib has less deterioration or even improvement of symptoms compared with those on placebo , whereas a positive di erence implies that the symptoms have worsened more for those on ge tinib . 
 table 3 : treatment e ect at 4 weeks for patient - reported outcomes measures over time did not detect any statistical di erences in the four prespeci ed domains . discussion cog is the rst randomised trial of systemic therapy in patients with oesophageal cancer progressing after chemotherapy ( panel )  . 
 cog showed no overall survival bene t for ge tinib over placebo , but a small bene t in progression - free survival and some aspects of health - related quality of life were observed , including an improvement in a prespeci ed patient - reported outcome , odynophagia . 
the toxicity pro le observed in the current study was generally consistent with that previously observed for ge tinib in in other tumour types20 with no new safety signals identi ed . a suggestion of progression - free survival bene t for ge tinib was observed across most subgroups , including adenocarcinoma , squamous - cell cancers , and oesophagus and junctional cancers , although not all di erences were signi cant . 
although the biological di erences between adenocarcinoma and squamous - cell vol 15 july 2014 articles global quality of life cognitive physical emotional role social constipation hair loss speech cough odynophagia pain dyspnoea anxiety sleep saliva reux eating pain and discomfort appetite choking dysphagia eating with others taste finance fatigue nausea / vomiting body image weight loss dry mouth diarrhoea than combination with chemotherapy as well as tkis , oesophagogastric cancers have also been treated with anti - egfr antibodies . 
single agent activity is low22 and investigators have focused on combination with chemotherapy.23 , 24 however , in phase 3 trials combining anti - egfr monoclonal antibodies with chemotherapy in the rst - line setting , overall survival was lower with targeted agents such as panitumumab and cetuximab than with chemotherapy.23 , 24 one explanation is that anti - egfr therapies are not clinically active in oesophagogastric cancer . 
however a similar absence of bene t in molecularly unselected patients has also been reported when egfr tkis or anti - egfr antibodies are combined with platinum - based chemotherapy in several studies in various other malignancies , notably in non - small - cell lung cancer25 and colorectal cancer.26 monotherapy with egfr tkis and anti - egfr antibodies after chemotherapy has proven useful in nonsmall - cell lung cancer and colorectal cancer.27 , 28 our nding of anti - tumour activity for ge tinib in a subgroup of responsive patients in the cog trial similarly suggests that single agent anti - egfr therapy might be more e ective oesophageal cancer . 
in oesophageal cancer a predictive biomarker that identi es a ge tinib - responsive subgroup might also be useful for other anti - egfr therapies , such as monoclonal antibodies , in this disease type . study has including detailed strengths , examination of the e ect of treatment on patient - reported outcomes , and it is the rst multicentre randomised trial in oesophageal cancer that has included a well - designed comprehensive assessment of patient - reported outcomes . 
for example , only patients who had not had disease progression at 4 weeks were asked to complete the patient - reported outcome questionnaires and are included in the analysis . 
this approach might have a ected the results and patients with disease progression at this timepoint might have had a di erent outcome pro le because treatment might have been withdrawn earlier because of general deterioration . 
skin toxicity is a known side - e ect of ge tinib and was not directly measured with the patient - reported outcomes , although the global quality - of - life score re ects problems with skin toxicity , and this outcome did not vary between groups . our in conclusion , the phase 3 cog study did not meet its primary endpoint of a signi cant overall survival bene t for ge tinib compared with placebo in unselected mean dierence between groups getinib better placebo better figure 6 : mean change in health - related quality - of - life outcomes from baseline to 4 weeks positive values on the functioning scale and negative values on the symptom scale denote bene t from ge tinib compared with placebo . carcinoma are increasingly characterised , 21 these data were not available at the time of study design and there was no consistent indication from phase 2 trials of ge tinib or erlotinib that histological subtypes of oesophageal cancer responded di erently . 
in the context of the rst randomised trial in the second - line setting in oesophageal cancer , we believe that this observation is clinically signi cant . the increased disease control , bene t in some patient - reported outcomes , and progression - free survival might suggest the existence of a ge tinibresponsive subgroup of patients with oesophageal cancer . 
we are undertaking tumour specimens from cog to identify predictive biomarkers for ge tinib ( transcog study )  . translational research 902 vol 15 july 2014 articles see online for appendix panel : research in context systematic review pubmed was searched for clinical trials ( published in english only ) assessing second - line therapies in patients with oesophageal cancer progressing after chemotherapy . 
the search terms used were oesophageal or esophageal , cancer or neoplasm or malignancy or malignant , second - line or salvage or supportive care or advanced , randomised or randomized , with no publication date parameter . 
evidence is scarce and no phase 3 trials have been done to support use of second - line therapies in this setting , and very few data exist for the e ect of treatments on health - related quality of life , which is important in clinical decision making in such situations when life expectancy is poor . 
because of biological di erences between gastric and oesophageal cancers , extrapolation of data from phase 3 trials in gastric cancer to oesophageal cancer is likely to result in suboptimum outcomes for patients . 
a systematic review of the use of egfr tyrosine - kinase inhibitors in oesophageal cancer showed that in a series of phase 2 trials , objective responses to ge tinib or erlotinib were observed in patients who had disease progression after previous chemotherapy and the toxicity of treatment was mild.9 to the best of our knowledge , cog was established as the rst phase 3 study in oesophageal cancer to investigate both survival and patient - reported outcomes in the second - line setting with patients randomly assigned to treatment with ge tinib or placebo . interpretation we noted no signi cant di erence between ge tinib and placebo for the primary outcome , overall survival ; however , ge tinib was well tolerated and improved progression - free survival , disease control , and patient - reported outcomes . 
the data also suggest that a subgroup of patients might gain clinically signi cant bene ts from this treatment and identi cation of a predictive biomarker for this ge tinib - responsive subgroup of patients is important . patients with oesophageal cancer progressing after previous systemic chemotherapy . 
 together with the observation of rapid and durable responses and prolonged disease control in a few patients treated with ge tinib , this nding suggests antipossible tumour activity in an as yet unidenti ed small ge tinib - responsive subgroup . 
the data presented are valuable for clinical practice and decision making , indicating that without biomarker strati cation , ge tinib has marginal clinical bene ts in advanced oesophageal cancer ; however , patient - reported outcomes suggest some useful palliation of symptoms . 
 identi cation of a predictive biomarker to identify any of patients with subgroup ge tinib - responsive oesophageal cancer would greatly increase clinical usefulness and is the priority for ongoing work . speci c contributors drf was chief investigator for the trial . 
jmb was the quality - of - life adviser for the trial and was involved in the study design , data analysis , and the interpretation and writing of this paper . 
all authors have contributed to , seen , and approved the nal draa full list of all cog study investigators is shown in the appendix . declaration of interests drf received a grant from astrazeneca to continue with ongoing research into frgr inhibitor azd4547 and money for an educational dvd on egfr mutation analysis . 
jmb is supported by the mrc conduct - ii hub for trials methodology research acknowledgments the study was funded by cancer research uk and jointly sponsored by the university of oxford and the royal wolverhampton hospitals nhs trust . 
we thank the patients who participated in the cog trial ; the investigators , the research nurses , clinical sta from the individual trial centres and sta members from the oncology clinical trials o ce ( octo ) at the university of oxford who provided ongoing support . 
we thank the members of the trial steering committee ( tom crosby [ velindre cancer centre ] , christopher poole [ university of warwick ] , and helen marshall [ university of leeds ] ) , and the independent data and safety monitoring committee ( matthew sydes [ mrc clinical trials unit ] , mark saunders [ christie hospital nhs foundation trust ] , and nicola levitt [ john radcli e hospital ] )  . corrections correction to lancet oncol 2013 ; 14 : 790 correction to lancet oncol 2013 ; 14 : 989 vandendriessche chuah mk . 
 fulvestrant placebo versus exemestane alone after progression on non - steroidal aromatase inhibitors in postmenopausal patients with hormone - receptor - positive locally advanced or metastatic breast cancer ( sofea ) : a composite , multicentre , phase 3 randomised trial . 
lancet oncol 2013 ; 14 : 98998in the methods section of the summary of this article , the rst part of the third sentence should have read participants were randomly assigned ( 1 : 1 : 1 ) to receive intramuscular fulvestrant ( 500 mg injection on day 1 , followed by 250 mg doses on days 15 and 29 , and then every 28 days )  . 
 vol 14 september 2013 e391 news published online august 13 , 2020 s1470 - 2045 ( 20 ) 30470 - 8 for more on the explosions in beirut see uk / news / world - middleeast - 53720383 for more on the impact of the disaster on saint george hospital see nytimes.com / 2020 / 08 / 04 / world / middleeast / beirutexplosion - blast.html for more on the destruction of medicine stockpiles see beirut - explosion - hospitalsdamaged - cant - admit - patientsafter - blast - 2020 - 8 ? r = us&ir = t for more on the toxic air pollutants released by the explosions see airqualitynews.com / 2020 / 08 / 05 / major - air - pollution - concernfollowing - beruit - explosion / and news / 2020 / 08 / 04 / hugeexplosions - rock - central - beirutcitys - hiroshima / patients with cancer hit hard by deadly explosions in beirut last weeks explosions in beirut , lebanon , caused devastating and widespread damage , including destruc tion of hospitals and decimation of medical supplies , leaving already vulnerable patients with cancer in shock and without access to treatment . government officials have now confirmed that the two explosions , which occurred in the early evening on aug 4 , 2020 , after a warehouse caught fire on beiruts northern industrial waterfront , resulted from the detonation of 2750 tonnes of ammonium nitrate that had been incorrectly stored for the past 6 years in a depot nearby . 
the incident , which killed at least 220 people and left more than 6000 injured , devastated huge areas of the city , including hospitals and health - care facilities , piling enormous new pressures on a health - care system whose resources were already stretched financially and by the ongoing covid - 19 pandemic . saint george hospital university medical center , located in the city centre and one of the biggest hospitals in beirut , was so badly damaged as a result of the explosions that it was forced to close and send its patients elsewhere . 
those affected included patients with cancer who were in the middle of their chemotherapy treatmentsome of whom panicked and fled without notifying medical staff . rabih said , a member of the oncology team at saint george hospital university medical center , described the challenges faced by staff in the chaos of evacuating patients from a hospital that had been demolished by the blasts . 
we lost some of our colleagues in the explosions , while patients witnessed the traumatic death and serious injury of family members and others within the hospital . it was particularly challenging to organise the evacuation of patients with cancer who were immunocompromised and cytopenic , raising the risk of bleeding and infection , especially during the covid - 19 pandemic . peter noun , a paediatric oncologist who works with more than 100 children in units at saint george and the lebanese hospital geitaouianother nearby hospital that was severely damaged and forced to closeis worried about the disruption this has caused to his patients treatment . our major concern now is where to continue the chemotherapy for our kids , noun explained . 
more than 45 of our patients have already missed one chemotherapy session , and it may be weeks before we are able to resume their treatment schedules . further to the damage and disruption caused to hospitals and medical centres , a warehouse containing large stocks of medicines was also destroyed near the site of the explosions . 
as well as vaccines and other essential medicines , it contained a supply of chemotherapy products to be distributed to patients across lebanon . although we do not yet know the extent of the damage , a significant number of cancer drugs were stored in a warehouse close to the explosion site , said confirmed . 
this is hugely concerning , as there was already a shortage of cancer treatments due to lebanons financial crisis and the cost of cancer drugs , making access to various expensive medications a challenge even before the blasts . there are also concerns over toxins released by the explosions , which could pose severe health risks in both the short and long term , including an increased incidence of cancer . 
lebanons health minister issued a warning about the potentially hazardous effects of toxic air pollutants , such as nitrogen dioxide , following the incident , advising those who were able to leave the area to do so . friends after months of severe economic crisis , our close from lebanon will have to survive another disaster , reflected benjamin besse ( gustave roussy institute , villejuif , france )  . 
with more than 6000 injured people , hospitals have to prioritise first aid over cancer diagnosis and care . enrique soto prez de celis ( national institute of medical science and nutrition , mexico city , mexico ) agreed : disasters such as this one can be extremely challenging for health - care systems , not only by causing direct loss of life , but also by compromising the availability of medical services to treat other diseases such as cancer . damage to clinics and hospitals can break the continuity of cancer therapy and jeopardise patient care , particularly for the most vulnerable , such as older adults or those receiving palliative or end - of - life care , who are in risk of losing access to urgent medications , he continued . 
this highlights the relevance of training first responders who are part of rapidresponse teams deployed to disaster areas to implement essential noncommunicable disease interventions , include essential cancer and to medications in emergency kits . meanwhile , richard penson ( harvard medical school , boston , ma , usa ) commented on the international relief response to the disaster : covid - 19 has distanced us from our patients and our neighbours , but somehow heightened an awareness of the need to meet injustice with action . 
clinical characteristics , outcomes , and risk factors for mortality in patients with cancer and covid - 19 in hubei , china : a multicentre , retrospective , cohort study . 
 j hematol oncol 2020 ; 13 : 43 . risk factors for in - hospital mortality in patients with cancer and covid - 19 the covid - 19 pandemic is getting worse globally . 
we read with interest the recent article by kunyu yang and colleagues1 in the lancet oncology , which was , to our knowledge , the first to focus on the mortality of covid - 19 in patients with cancer . 
 the authors concluded that receiving chemotherapy within 4 weeks before symptom onset and male sex were independent prognostic factors for in - hospital mortality in patients with cancer and covid - 19 . first , the data in the article showed that 40 ( 20% ) of 205 patients with cancer and covid - 19 had died . 
 however , this finding is insufficient to conclude that patients with cancer and covid - 19 had a higher casefatality rate than did the general patient population with covid - 19 . 
 additionally , in wuhan , the mortality rate of inpatients with covid - 19 was 28% , regardless of whether or not they had cancer.2 second , we reviewed the cancer history of the 205 patients listed in the article.1 based on data availability , we found that 98 ( 77% ) of 127 survivors were at early cancer stage ( stage iii ) , 121 ( 82% ) of 148 survivors underwent surgery , and 73 ( 47% ) of 156 survivors survived for more than 5 years since their cancer diagnosis , 1 indicating that a substantial proportion of these patients might be clinically cured of their cancer . 
therefore , there was a large amount of heterogeneity among the patients with cancer and it would be better to study the association between mortality related to covid - 19 and primary or metastatic thoracic malig nancies . 
 third , the main causes of death for the general patient population with covid - 19 include sepsis , respiratory failure , and acute respiratory distress syndrome.2 older age , high sequential organ failure assessment score , and d - dimer concentration greater than 1 g / ml are potential risk factors for poor prognosis.2 although there were only 40 endpoint events in this article , 1 it is not appropriate to establish the multivariable logistic regression model by use of cancer - related variables , rather than these key risk factors . 
 because of scarce evidence of the correlation between these factors and mortality in patients with cancer and covid - 19 , as well as the small sample size , the conclusion that receiving chemotherapy within 4 weeks before symptom onset is an unfavourable prognostic factor for these patients should be interpreted with caution . 
 furthermore , biological sex affects immune responses and covid - 19 outcomes in all populations , not just patients with cancer.3 because the expression of angiotensin - converting enzyme 2 ( ace2 ) is also different in various cancers , 4 an analysis of the relation between case - fatality rate and ace2 expression in patients with cancer and covid - 19 would be of interest . overall , the available evidence might not strongly prove that patients with cancer and covid - 19 have a much higher case - fatality rate than do the general patient population with covid - 19 . 
the decision of whether or not to use chemotherapy should be especially cautious for patients with cancer and covid - 19 . we declare no competing interests . kaibo guo , leitao sun , li yuan , harpreet s wasan , * shanming ruan shanmingruan@zcmu.edu.cn joint first authors the first clinical medical college of zhejiang chinese medical university , hangzhou , zhejiang , china ( kg , ly ) ; department of medical oncology , the first affiliated hospital of zhejiang chinese medical university , hangzhou 310006 , zhejiang , china ( ls , sr ) ; and department of cancer medicine , hammersmith hospital , imperial college healthcare nhs trust , london , uk ( hsw ) vol 21 september 2020 e406 correspondence editorial see comment page 1192 see articles page 1203 for the nhs figures see statistical - work - areas / cancerwaiting - times / measuring the quality of cancer care in uk hospitals analyses of cancer registries are accepted methods of documenting the burden of disease within a region , providing a wealth of data ranging from cancer types endemic in the population to the e ects of available treatments . 
such analyses have been integral to the creation of national cancer care plans , and help policy makers to decide which areas of cancer care to invest to address geographical disparities in cancer care , there has been a trend to break down these regional data into smaller geographical areas . 
but what is the best way to measure the quality of care at such a level ? waiting times from general practitioner ( gp ) referral to rst cancer treatment ; hospital discharge rates ; 30 - day mortality ; and hospital - level cancer survival statistics are all routinely debated as viable options . obtaining su cient data to produce useable quality - of - care metrics at the hospital - level is di cult . 
 even for common cancers , most hospitals will not see enough patients over the course of a year to produce relevant statistics , and thus comparisons between hospitals can be confounded by small numbers and low statistical power . 
moreover , patients with cancer sometimes attend more than one hospital for their care ; thus , attributing patients and their outcomes to a particular hospital is unavoidably complicated and can skew data . 
jeremy hunt , the uks health secretary , has repeatedly called for cancer survival statistics by hospital in an e ort to highlight geographical disparities in care and draw attention to poor performers . 
 however , as discussed by melanie morris and colleagues in this issue of the lancet oncology , these metrics are awed , most obviously by referral bias , which misrepresents hospital performance due to the patient case mix . 
 for patients with cancer , the time between referral from their gp to receipt of their rst interventional treatment has also captured public attention as a measure of quality of care , and the latest gures show the national health service in england is falling short of the 2 - month target . 
 but is this metric any better than other targets , given it too can be heavily confounded ? an alternative to survival statistics and referral time is the measurement of mortality . 
in todays issue of the lancet oncology , we publish the rst report on 30 - day mortality per hospital trust after palliative and curative chemotherapy for patients with breast and lung cancer . 
 based on the systemic anti - cancer therapy ( sact ) database , and in contrast to survival statistics , this metric allows some interpretation of the quality of treatment at the hospital - level . 
as discussed by the authors of the report , another major di culty with interpreting the data is the lack of complete information : for example , several hospitals only had data for patients who completed just one cycle of chemotherapy . 
moreover , data on performance status , which is known to a ect a patients ability to receive certain treatments , or their response , was missing for many individuals thereby limiting interpretation . 
 clearly , the availability of relevant cancer statistics to measure and analyse quality of care , and its use to rank hospital quality in a meaningful way is an ongoing challenge . 
 the more pressing issue of how to measure and analyse data once it is collected is more di cult , and a composite approach made up of several measures , similar to the approach already used by the uk care quality commission , is required . 
it is easy to call for greater transparency in the reporting of the quality of care , as politicians have done , and it is indeed laudable and necessary to do so . 
our previous report found that two - thirds of newly diagnosed patients with lung cancer do not meet these criteria ; they are reported to be either long - term quitters ( 15 years since quitting ) or from a younger age group ( age 5054 years )  . 
we aimed to assess survival outcomes in these two subgroups . methods for this prospective , observational cohort study we identified and followed up patients aged 5080 years with lung cancer , with a smoking history of 30 pack - years or more , and included both current smokers and former smokers who quit within the past 30 years . 
we identified patients from two cohorts in the usa : a hospital cohort ( mayo clinic , rochester , mn ) and a community cohort ( olmsted county , mn )  . 
patients were divided into those meeting uspstf criteria ( uspstf group ) versus those not meeting uspstf criteria ( long - term quitters or the younger age group )  . 
the uspstf group was subdivided into two age subgroups ( 5569 years and 7080 years ) for multivariable regression analysis . findings between jan 1 , 1997 , and dec 31 , 2017 , 8739 patients with lung cancer were identified and followed up . 
 5 - year overall survival was 27% ( 95% ci 2530 ) in long - term quitters , 22% ( 1925 ) in the younger age group , and 23% ( 2224 ) in the uspstf group . 
in both cohorts , 5 - year overall survival did not differ significantly between long - term quitters and the uspstf group ( hospital cohort : hazard ratio [ hr ] 102 [ 95% ci 094110 ] ; p = 072 ; community cohort : 097 [ 075126 ] ; p = 082 ) ; matched analysis showed similar results in both cohorts . 
5 - year overall survival also did not differ significantly between the younger age group and the uspstf group in both cohorts ( hospital cohort : hr 116 [ 95% ci 098138 ] , p = 008 ; community cohort : 116 [ 074182 ] ; p = 052 ) ; multivariable regression analyses stratified by age group yielded similar findings . interpretation patients with lung cancer who quit 15 or more years before diagnosis and those who are up to 5 years younger than the age cutoff recommended for screening , but otherwise meet uspstf criteria , have a similar risk of death to those individuals who meet all uspstf criteria . 
based on the results of the national lung screening trial ( nlst ) , which showed a 20% reduction in lung cancer mortality from screening of high - risk individuals by use of low - dose ct , 4 the us preventive services task force ( uspstf ) recommends screening for lung cancer in individuals aged 5580 years , who have a smoking history of 30 pack - years or more , and who either currently smoke or quit within the past 15 years.5 a comparative the uspstf criteria modelling study based on predicted that an estimated 18 000 lives per year could be saved in the usa if low - dose ct is widely used in the eligible population.6 however , the surveillance epidemiology and end results program ( seer ) database as well as data from two other independent cohorts have shown that only a third of patients diagnosed with lung cancer in the usa meet the uspstf screening criteria , 79 suggesting that many potentially high - risk individuals are not eligible for low - dose ct screening . 
among patients outside of the 1098 vol 20 august 2019 correspondence to : prof ping yang , division of epidemiology , department of health sciences research , mayo clinic , scottsdale , az 85259 , usa yang.ping@mayo.edu research in context evidence before this study we searched pubmed for articles published up to oct 31 , 2018 , using the terms lung cancer , screening , low - dose ct , smoking cessation , former smoker , and younger age , without any language restrictions . 
this search showed that screening of high - risk individuals by use of low - dose ct in the national lung screening trial was associated with a 20% reduction in lung cancer mortality . 
the us preventive services task force ( uspstf ) recommends screening for lung cancer in individuals aged 5580 years , who have a smoking history of 30 or more pack - years , and who currently smoke or quit within the past 15 years . 
the results of the nelson randomised controlled screening trial have shown a 26% reduction in the risk of death from lung cancer with lowdose ct screening of individuals aged 5074 years , who have a history of smoking more than ten cigarettes daily for more than 30 years or more than 15 cigarettes daily for more than 25 years , and who currently smoke or quit within the past 10 years . 
 however , the surveillance epidemiology and end results program database as well as data from two other independent cohorts have shown that only a third of patients with lung cancer would have met the uspstf screening criteria , suggesting that many potentially high - risk individuals are not eligible for low - dose ct screening . 
among patients outside of the high - risk population defined by the uspstf , the three largest subgroups at potentially high risk for developing lung cancer are patients who quit smoking 1530 years before diagnosis ( termed long - term quitters ) , those aged 5054 years at the time of lung cancer diagnosis ( termed the younger age group ) , and those with a smoking history of around 2030 pack - years . added value of this study to the best of our knowledge , no previous study has directly compared overall survival between patients with lung cancer who meet uspstf screening criteria and those who are ineligible because they are long - term quitters ( those who quit smoking 15 years before diagnosis ) or aged 5054 years at the time of lung cancer diagnosis . 
the younger age group also had similar 5 - year overall survival to the uspstf group ; age - group stratified analysis yielded similar findings . implications of all the available evidence our findings suggest that patients with lung cancer who quit smoking more than 15 years before diagnosis or those who are 5 years younger than those who are eligible for screening but otherwise meet the uspstf screening criteria have similar lung cancer survival to those who meet all the uspstf screening criteria . 
in future , more sophisticated screening programmes combining low - dose ct and biomarkers could be developed to identify high - risk individuals who would benefit most from screening . lung cancer high - risk population defined by the uspstf , the three largest subgroups at potentially high risk for developing lung cancer are patients who quit smoking 1530 years before lung cancer diagnosis ( termed longterm quitters ) , those aged 5054 years at the time of lung cancer diagnosis ( termed the younger age group ) , and those with a smoking history of around 2030 packyears.8 , 9 the risk of developing individuals in these groups remains high.10 , 11 our previous reports revealed that nearly two - thirds of patients ( 4162 [ 61% ] of 6838 ) with newly diagnosed lung cancer did not meet the uspstf criteria and that almost a fifth ( 1285 [ 19% ] of 6838 ) were either longterm quitters or in the younger age group.8 , 9 by contrast with the high - risk population defined by the uspstf , multiple organisations including the international association for the study of lung cancer , the american association of thoracic surgery , the american college of chest physicians , and the national comprehensive cancer network have recommended low - dose ct screening of patients according to nlst smoking history criteria or of patients aged 5054 years , along with one additional lung cancer risk factor , which could include occupational exposure or a history of pulmonary disease.1214 the results of the nelson randomised controlled screening trial showed a 26% reduction in the risk of death from lung cancer in individuals aged 5074 years , who have a history of smoking more than ten cigarettes daily for more than 30 years or more than 15 cigarettes daily for more than 25 years , and who either currently smoke or quit within the past 10 years . 
 the nelson trial thus included individuals younger than 55 years and those with a shorter smoking history than the patients enrolled in the nlst.15 screening has been an essential component of efforts to decrease the burden from lung cancer in high - risk populations.16 the ultimate measure of an effective screening tool is mortality reduction , and it remains unclear whether any additional randomised trials have been planned to investigate and justify any adjustments to current criteria . 
 * long - term quitters : individuals aged 5580 years , who have a smoking history of 30 or more pack - years and quit smoking within the past 1530 years . 
uspstf criteria : individuals aged 5580 years , who have a current or past smoking history of 30 or more pack - years ; if former smokers , those who had quit within the past 15 years . 
unknown stage : 30 ( 2% ) of the 1299 long - term quitters and 104 ( 2% ) of 5869 patients among the uspstf group in the hospital cohort . 
||unknown treatment : 57 ( 4% ) of 1299 long - term quitters and 246 ( 4% ) of 5869 patients among the uspstf group in the hospital cohort . table 1 : characteristics of 8031 patients aged 5580 years in the hospital cohort and community cohort , including long - term quitters , diagnosed 19972015 because they are classified as long - term quitters or in a younger age group at the time of lung cancer diagnosis . 
 we estimated 5 - year overall survival after diagnosis in both of these subgroups , assessed 5 - year overall survival after matching age and pack - years smoked for long - term quitters , and did a regression analysis stratified by age group for the younger age group . methods study population for this prospective , observational cohort study , patients with pathologically diagnosed primary lung cancer , aged 5080 years , with 30 or more pack - years of smoking history , who were either current smokers or former smokers who quit within the past 30 years , were identified 1100 vol 20 august 2019 articles and enrolled from a hospital cohort ( mayo clinic , rochester , mn , usa ) and a community cohort ( olmsted county , mn , usa )  . 
 based on age at the time of lung cancer diagnosis , all enrolled patients who quit smoking within the past 15 years were divided into the uspstf group ( age 5580 years ) and the younger age group ( age 5054 years ) in both cohorts . 
the long - term quitters and the younger age group were selected on the basis of our previous studies , 8 , 9 where we evaluated the top seven potential highrisk subgroups by frequency that missed uspstf criteria for low - dose ct screening ; long - term quitters and younger age group were ranked the highest . 
the community cohort comprised patients in the rochester epidemiology project database with medical records of all people residing in olmsted county , and the hospital cohort comprised patients diagnosed at the mayo clinic in minnesota between jan 1 , 1997 , and dec 31 , 2015 ( excluding olmsted county residents )  . 
the community cohort was matched to the same 19 years of diagnosis as the hospital cohort.9 the community cohort consisted of approximately 140 000 people , 83% of whom are non - hispanic white ; the population is socioeconomically similar to the white population of the usa and is representative of the population of the midwestern usa.8 , 9 , 17 the institutional review boards of mayo foundation and olmsted county medical center approved this study . 
no written consent from patients was needed for this study . data collection detailed procedures of patient enrolment , data collection , and routine follow - up have been reported in previous studies8 , 9 , 17 and in the appendix ( p 2 ) , including the definition of pack - years and years since quitting.8 , 9 , 18 a never - smoker was defined as an individual who had smoked fewer than 100 cigarettes during their lifetime . 
current smokers were defined as individuals who were actively smoking , and who had stopped smoking within 1 year before lung cancer diagnosis . outcomes the main outcome was overall survival , defined as the time from the date of diagnosis to death from any cause in the hospital and community cohorts ; patients who were alive or lost to follow - up were censored . 
5 - year overall survival after diagnosis was also analysed for long - term quitters , the younger age group , and the uspstf group . statistical analysis patient characteristics are presented as means ( sd ) and medians ( iqr ) for continuous variables and as events patients hr ( 95% ci ) p value events patients hr ( 95% ci ) p value a hospital cohort unmatched multivariable long - term quitters uspstf group 4361 1299 5869 matched multivariable long - term quitters uspstf group 1224 1224 b community cohort unmatched multivariable long - term quitters uspstf group matched multivariable long - term quitters uspstf group favours long - term quitters favours uspstf group figure 1 : multivariable cox proportional hazard models of overall survival in patients meeting uspstf screening criteria versus long - term quitters ( a ) hospital cohort . 
multivariable cox proportional hazards models were used to adjust for age , sex , race , smoking status , pack - years smoked , tumour histology and stage , and treatment modalities . 
uspstf = us preventive services task force . 102 ( 094110 ) 100 ( ref ) 072 105 ( 095117 ) 100 ( ref ) 035 097 ( 075126 ) 100 ( ref ) 082 103 ( 079135 ) 100 ( ref ) 084 see online for appendix frequency ( % ) for categorical variables . 
 univariable cox proportional hazards models were used to assess the association of known prognostic factors ( ie , age at diagnosis , sex , cigarette smoking history , tumour histology , stage , and treatment modalities ) with estimated 5 - year survival . 
multivariable cox models were developed with significant variables ( defined as p < 010 ) in the univariable analysis , and hazard ratios ( hr ) with 95% ci were calculated . 
 * long - term quitters : individuals aged 5580 years , who have a smoking history of 30 or more pack - years and quit smoking within the past 1530 years . 
uspstf criteria : individuals aged 5580 years , who have a current or past smoking history of 30 or more pack - years ; if former smokers , those who quit within the past 15 years . 
large - cell neuroendocrine and adenosquamous carcinoma . table 2 : characteristics of matched sets in the hospital and community cohorts ( long - term quitters and those meeting uspstf criteria ) , diagnosed 19972015 while including optimal case numbers . 
additionally , bootstrapping was used as a form of internal cross - validation , where 1000 replicate samples were drawn with replacements from the original sample , each with the same sample size . considering age and competing causes of death , we did a multivariable regression analysis stratified by age group , and compared 5 - year overall survival the uspstf age subgroups ( five consecutive 5 - year age groups : 5559 years , 6064 years , 6569 years , 7074 years , and 7580 years ) with that in the younger 1102 vol 20 august 2019 articles a hospital cohort unmatched analysis matched analysis long - term quitter uspstf group age at diagnosis ( years ) age at diagnosis ( years ) pack - years pack - years b community cohort 006 004 002 0025 0020 0015 0010 0005 006 004 002 0015 0010 0005 age at diagnosis ( years ) age at diagnosis ( years ) 0020 0015 0010 0005 pack - years pack - years vol 20 august 2019 figure 2 : kernel density plots showing the balance improvement for age at diagnosis and pack - years smoked between patients meeting uspstf screening criteria and long - term quitters ( a ) hospital cohort . 
 the density of the kernel density plot represents the kernel density estimate of the probability function of a variable from patients ( eg , age or pack - year ) , which is interpreted as a probability differential . 
 * younger age group : individuals aged 5054 years , with a smoking history of 30 or more pack - years , and currently smoke or quit within the past 15 years . 
uspstf criteria : individuals aged 5580 years , with a smoking history of 30 or more pack - years , and who currently smoke or quit within the past 15 years . 
unknown stage : 14 ( 2% ) of 630 patients among the younger age group and 104 ( 2% ) of 5869 patients among the uspstf group in the hospital cohort . 
||unknown treatment : 19 ( 3% ) of 630 patients among the younger age group and 246 ( 4% ) of 5869 patients among the uspstf group in the hospital cohort . table 3 : characteristics of 7335 patients aged 5080 years in the hospital cohort and community cohort , including the younger age group , diagnosed 19972015 age group . 
missing data were not included in our analyses . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the manuscript . 
the corresponding author had full access to all the data in the study , and had final responsibility for the decision to submit for publication . results between jan 1 , 1997 , and dec 31 , 2017 , 8739 patients with lung cancer were identified and followed up , with a median follow - up of 65 ( iqr 38100 ) years . 
among all patients in the hospital cohort , lung cancer stage was unknown for 30 ( 2% ) of 1299 patients termed long - term quitters , for 104 ( 2% ) of 5869 patients in uspstf group , and for 14 ( 2% ) of 630 patients in the younger age group . 
 treatment was unknown for 57 ( 4% ) of 1299 long - term quitters , 246 ( 4% ) of 5869 patients in uspstf group , and 19 ( 3% ) of 630 patients in the younger age group . 
the characteristics of 8031 patients aged 5580 years who quit within the past 30 years from the hospital cohorts and community cohorts , stratified by uspstf criteria , are shown in table 1 . 
long - term quitters were significantly older , and more frequently men , more likely to have smoked fewer pack - years , and to have adenocarcinoma histology than were those who met uspstf screening criteria . median overall survival was 169 months ( 95% ci 162175 ) in the study population . 
5 - year overall survival was 27% ( 95% ci 2530 ) in long - term quitters , 22% ( 1925 ) in the younger age group , and 23% ( 2224 ) in the uspstf group . in univariable cox models , known prognostic factors including age , sex , race , smoking status , pack - years smoked , tumour histology , stage , and treatment modality were significant variables , which were then analysed in multivariable cox models . 
in multivariable analyses , 5 - year overall survival was not significantly different in long - term quitters in the hospital cohort versus in those who met uspstf criteria ( hr 102 ; 95% ci 094110 ; p = 072 ) after adjustment of significant variables in univariable analysis ( figure 1a )  . 
in the community cohort , long - term quitters also had the same mortality risk at 5 years as did those who met the uspstf criteria ( hr 097 ; 95% ci 075126 ; p = 082 ; figure 1b )  . 
a bootstrap validation did not alter the results in the fitness of both models ( data not shown )  . matching based on age at diagnosis and pack - years smoked yielded 1224 patient pairs in the hospital cohort , and 315 individuals meeting uspstf criteria versus 105 long - term quitters in the community cohort ( table 2 )  . 
in the multivariable analysis , 5 - year overall survival did not differ significantly between long - term quitters and patients meeting uspstf criteria in the hospital cohort ( figure 1a ) or in the community cohort ( figure 1b )  . the characteristics of 7335 patients aged 5080 years who quit within the past 15 years from the hospital cohort and community cohort , stratified by uspstf criteria , are shown in table 3 . 
 a hospital cohort age 5054 years uspstf criteria number at risk ( number censored ) age 5054 years uspstf criteria 5869 time since diagnosis ( years ) ( 11 ) 3497 ( 100 ) ( 20 ) 2312 ( 182 ) ( 28 ) 1740 ( 259 ) ( 30 ) 1409 ( 313 ) ( 36 ) 1127 ( 381 ) b community cohort number at risk ( number censored ) age 5054 years uspstf criteria time since diagnosis ( years ) ( 16 ) ( 28 ) ( 34 ) figure 3 : kaplan - meier curves of overall survival of the younger age group and uspstf group ( a ) 5 - year overall survival in the hospital cohort . 
compared with the uspstf group , the younger age group comprised mostly current smokers , and most patients were female , with stage iii / iv lung cancer and adenocarcinoma . for patients in the hospital cohort , median overall survival was 174 months ( 95% ci 155197 ) in the younger age group and 172 months ( 165182 ) in the uspstf group . 
in the community vol 20 august 2019 1105 articles a hospital cohort multivariable analysis 5054 years 5580 years 4361 multivariable risk - adjusted analysis 5054 years 5569 years 2757 5054 years 7080 years 1604 b community cohort multivariable analysis 5054 years 5580 years multivariable risk - adjusted analysis 5054 years 5569 years 5054 years 7080 years 5869 3774 2095 events patients hr ( 95% ci ) p value events patients hr ( 95% ci ) p value 116 ( 098138 ) 100 ( ref ) 109 ( 089133 ) 100 ( ref ) 008 039 129 ( 080208 ) 100 ( ref ) 030 052 033 077 116 ( 074182 ) 100 ( ref ) 127 ( 079203 ) 100 ( ref ) 093 ( 059149 ) 100 ( ref ) favours younger age group favours uspstf group figure 4 : multivariable cox proportional hazard models of patients meeting uspstf screening criteria versus the younger age group ( a ) hospital cohort . 
 in univariable cox models , sex , cigarette smoking status , pack - years smoked , years since quitting , tumour histology , stage , and treatment modality were significant variables , which were then analysed in multiple cox models . 
in multivariable analyses , 5 - year overall survival was not significantly different between the younger age group in the hospital cohort and the uspstf group ( hr 116 ; 95% ci 098138 ; p = 008 ; figure 4a )  . 
in the community cohort , 5 - year overall survival was not significantly different between the younger age group and the uspstf group ( hr 116 ; 95% ci 074182 ; p = 052 ; figure 4b )  . the uspstf group ( patients aged 5580 years ) was subdivided into five consecutive 5 - year age groups . 
three uspstf subgroups with similar risks ( 5559 years , 6064 years , and 6569 years ) were combined into the younger uspstf subgroup ( age 5569 years ) , and the other two subgroups with similar risks ( 7074 years and 7580 years ) were combined into the older uspstf subgroup ( age 7080 years ; appendix pp 34 )  . in multivariable risk - adjusted analysis , 5 - year overall survival was not significantly different between the younger age group and the two uspstf subgroups in the hospital cohort ( figure 4a )  . 
similarly , 5 - year overall survival did not differ significantly between the younger age group and the younger uspstf subgroup in the community cohort ( figure 4b )  . 
the younger age group had the same risk of death at 5 years as the older uspstf subgroup in the community cohort . discussion the results of this prospective , observational cohort study suggest that 5 - year overall survival after lung cancer diagnosis in patients who do not meet certain uspstf criteria ( long - term quitters and younger age groups ) is similar to that of patients who meet uspstf criteria . 
most patients were white ; the effect of racial or ethnic background was analysed , but was not significant as an independent covariate , which might reflect the small sample size of patients who were not white . 
our previous study showed that expanding the uspstf screening criteria to include long - term quitters might save more lives without significantly increasing the number of cases of overdiagnosis.9 findings from this study indicate that long - term quitters have similar overall criteria . 
 to patients meeting uspstf survival additionally , our results show a higher frequency of early - stage lung cancer among long - term quitters than among the uspstf group in the hospital and community cohorts . 
therefore , in terms of tumour stage , long - term quitters might have a higher survival benefit from screening than those who quit within the past 15 years , as a result of greater detection of early - stage lung cancer . patients aged 5054 years with lung cancer ( ie , the younger age group ) who otherwise meet the uspstf screening criteria are one of the three largest subgroups at potentially high risk of developing lung cancer outside of the high - risk population defined by the uspstf.8 , 9 our data suggest that overall survival in individuals in the younger age group was similar to that of those in the uspstf group , suggesting that the risk of death in the younger age group might be underestimated by the uspstf criteria . 
therefore , the use of 55 years as the lower age limit in the uspstf criteria might exclude younger patients who could benefit from earlier detection of their lung cancer at a potentially curable stage . 
furthermore , the incidence and mortality of most malignancies , including lung cancer , usually increases with age until the age of about 80 years.3 , 20 however , the older uspstf subgroup in this study did not have worse overall survival than the younger age group , which is consistent with previous reports suggesting that lung cancer occurring in younger individuals might represent a biologically distinct subgroup associated with higher mortality , 21 so identification and screening of high - risk younger individuals is essential . 
a recent study indicated that 50 years of age was as a useful cutoff for prognosis and genomic alterations in non - small - cell lung cancer , 22 which is supported by our study in which patients aged 1106 vol 20 august 2019 articles 5054 years had the same overall survival as those aged 7080 years ( ie , the older uspstf subgroup )  . 
collectively , patients with lung cancer who are 50 years or older represent a subgroup with a similar risk of death after lung cancer diagnosis , and therefore patients aged 5054 years should also be included in the screening criteria . previous studies have shown that the risk of lung cancer exponentially decreases within 15 years of quitting ; 10 , 11 however , our results suggest that patients with lung cancer aged 5580 years , with 30 or more pack - years smoked and who quit smoking within the past 1530 years ( long - term quitters ) had the same survival 5 years after diagnosis as patients who quit smoking less than 15 years since diagnosis . 
these findings are compatible with data from the nlst and the prostate , lung , colorectal and ovarian cancer screening trial.4 , 23 previous research has reported that abnormalities detected at screening are significantly associated with subsequent smoking behaviour and could be used as a learning point for smoking cessation interventions.24 accordingly , lung cancer screening in could , by uncovering the younger age group abnormalities , help to increase smoking cessation in this group relative to that in patients who meet uspstf screening criteria . 
from the viewpoint of smoking cessation , patients aged 5054 years might benefit more from screening than those aged 55 years and older , which could also affect other smoking - related diseases , such as stroke and cardiovascular and pulmonary disease . 
screening of the younger age group could , therefore , substantially reduce morbidity and mortality and extend life expectancy . substantial progress lung cancer screening , diagnosis , and treatment has led to improved survival over the past decades . 
however , older patients are reported to be more likely to be ineligible for novel therapies because of comorbidities.25 , 26 therefore , the younger age group might benefit more than the uspstf group from continuous advances in lung cancer care . cost - effectiveness is especially important for lung cancer screening programmes , and the selection of age groups for screening has a large impact on costeffectiveness.6 a previous investigation showed that screening of individuals aged 50 years or older was the most cost - effective option , whereas screening of those aged 60 years or older was the least cost - effective.27 additionally , screening for long - term quitters might identify 16% more lung cancers with an acceptable cost and minimal harm.9 collectively , these studies imply that patients who can be classified as long - term quitters and who are 5054 years of age should be included in screening criteria for lung cancer ; future studies about the overall cost - effectiveness of expanding efficacious screening to long - term quitters and the younger age group are warranted . although this study enrolled the next largest subgroups at high risk for lung cancer ( ie , long - term quitters and the younger age group ) outside of the high - risk population defined by the uspstf , other potentially high - risk groups might also exist that are ineligible for screening . 
additional large randomised trials that only focus on differing cutoffs of age and smoking history might not be cost - effective ; instead , promising biological and physiological markers should be tested on a regular basis . 
molecular biomarkers in the biological fluid , such as blood , urine , saliva , and sputum , have been intensively investigated and shown the potential ability to improve selection of patients for lung cancer screening , and to assess the likelihood of malignancy in lung nodules detected at screening.28 combination of low - dose ct and biomarkers with optimal discriminating power in highrisk individuals before or after screening has the potential to optimise the efficacy of screening.29 a limitation of this study is that all patients were diagnosed with lung cancer , which makes it difficult to accurately examine trade - offs between the benefits and potential harms of screening . 
another concern is that approximately 1% of patients were initially identified via low - dose ct screening with a relatively earlier stage ; 30 however , the effect of staging has been carefully adjusted in our analyses . 
furthermore , missing data for stage and treatment were not included in our analyses , although the magnitude of missing data is minimal , and the proportions of missing data were similar between patients who met all uspstf criteria and those who did not . 
first , we carefully chose two independent cohorts : the hospital cohort represents the natural setting of an observational patient population at a tertiary medical centre , whereas the community cohort represents the midwest region of the usa . 
data were collected from these two prospectively observed cohorts with a long - term follow - up ; therefore , longitudinal and comprehensive data could be obtained , which enabled us to adjust for major known prognostic factors . 
third , smoking history was obtained from medical records and further confirmed with a follow - up questionnaire or an interview . in conclusion , our findings suggest that patients with lung cancer who quit smoking more than 15 years before a diagnosis or were up to 5 years younger than the age cutoff outlined in the uspstf screening criteria but who otherwise met the uspstf screening criteria were not vol 20 august 2019 1107 articles only at substantially high risk of developing the disease but also had similar survival to patients meeting the uspstf screening criteria . 
 individuals in these two subgroups might benefit from screening as expanding the uspstf criteria to include these subgroups could enable earlier detection of lung cancer . contributors py and dem contributed to the concept and design of this report . 
 we appreciate chia - sui weng for her technical assistance with the manuscript . comparison of breast cancer and cervical cancer stage distributions in ten newly independent states of the former soviet union : a population - based study anton ryzhov , marilys corbex , marion pieros , anton barchuk , diana andreasyan , sayde djanklich , vadim ghervas , olga gretsova , dilyara kaidarova , konstantin kazanjan , fuad mardanli , yuriy michailovich , elena ten , alesya yaumenenka , freddie bray , ariana znaor summary background screening for breast cancer and cervical cancer in the newly independent states of the former soviet union is largely opportunistic , and countries in the region have among the highest cervical cancer incidence in the who european region . 
we aimed to compare the stage - specific distributions and changes over time in breast cancer and cervical cancer incidence in the newly independent states of the former soviet union . methods we collected breast cancer and cervical cancer incidence data from official statistics from armenia , azerbaijan , belarus , georgia , kazakhstan , kyrgyzstan , republic of moldova , russian federation , ukraine , and uzbekistan for the years 200817 by tumour , node , metastasis ( tnm ) stage , and by age where population - based cancer registry data were available . 
we used log - linear regression to quantify the changes over time in age - standardised rates . findings during the period 201317 , more than 50% of breast cancer cases across the analysed countries , and more than 75% of breast cancer cases in belarus , kazakhstan , and ukraine , were registered at stages iii . 
the proportion of stage i breast cancer cases was highest in the screening age group ( 5069 years ) compared with other ages in moldova and the russian registries , but was highest in those aged 1549 years in georgia and ukraine . 
for cervical cancer , the proportions of cancers diagnosed at a late stage ( stages iii and iv ) were high , particularly in moldova and armenia ( > 50% )  . 
stage - specific incidence rates of cervical cancer generally increased over the period 200817 . interpretation our results suggest modest progress in early detection of breast cancer in the newly independent states of the former soviet union . 
the high proportions of early - stage disease in the absence of mammography screening ( eg , in belarus ) provide a benchmark for what is achievable with rapid diagnosis . 
a radical shift in national policies away from opportunistic screening toward organised , population - based , quality - assured human papillomavirus vaccination and screening programmes is urgently needed . funding union for international cancer control , who regional office for europe , and ministry of health of ukraine . copyright 2021 world health organization ; licensee elsevier . 
in this study , we focused on the stage distributions and incidence trends of breast and cervical cancer given their high contribution to cancer burden and frequent inadequate screening practices in the newly independent states of the former soviet union . 
the information on cancer registration and screening practices collected during the activities in the scope of the partnership between iarc and the who regional office for europe in supporting cancer surveillance was used to identify collaborators and support data interpretation . 
we searched pubmed using the terms tnm stage , breast cancer , cervix cancer , incidence trends , russia , central asia , and former soviet union with no date restrictions . 
we used the membership lists of the international association of cancer registries and the european network of cancer registries to identify european cancer registry websites and search them for available data by tnm stage . 
we scrutinised the available site visit reports at iarc and who regional office for europe for information on cervical and breast cancer screening practices in the newly independent states of the former soviet union . 
we assessed identified documents in english , russian , and czech languages . added value of this study to our knowledge , this study is the first combined investigation of breast cancer and cervical cancer stage - specific distributions and changes over time in the newly independent states of the former soviet union . 
we observed later stages at diagnosis of breast cancer and cervical cancer in the newly independent states of the former soviet union compared with other european countries , as well as increasing stage - specific changes in incidence over time . 
our results indicate that current breast cancer and cervical cancer screening practices in the newly independent states of the former soviet union are far from optimal , and provide a benchmark for breast and cervical cancer control planning in countries in the region . implications of all the available evidence screening practices for breast cancer and cervical cancer that are not evidence driven remain common in the newly independent states of the former soviet union . 
 advancing the quality of cancer registry data and strengthening the role of such data in cancer control will be critical for planning , monitoring , and evaluating progress . cancers amenable to early detection , such as breast and cervical cancers , stage distribution reflects awareness of cancer symptoms , delays in seeking care , access to care , and the effectiveness of screening programmes for the target age groups.6 breast cancer incidence in the newly independent states of the former soviet union is generally lower than in european countries , with estimated agestandardised rates ( world standard population ) ranging from 195 cases per 100 000 population ( tajikistan ) to 575 cases per 100 000 population ( georgia ) in 2020 , while mortality is similar or even higher ( from 80 cases per 100 000 population in tajikistan to 235 cases per 100 000 population in georgia ) .7 the dispensary system , which includes regular clinical breast examinations for women of a broad age range , remains intensively practiced in some newly independent states of the former soviet union ( eg , belarus ) , but has been practically withdrawn in others , such as georgia and kyrgyzstan ( who , unpublished )  . 
according to the who country capacity survey 2019 , 8 most newly independent states of the former soviet union have mammography screening programmes , but overall coverage is low ( mostly < 50% ) , and screening is usually offered on an opportunistic basis with suboptimal quality assurance . 
the target age includes those aged 5069 years in seven countries where mammography screening is available , but extends to women aged 4049 years or younger in georgia , kazakhstan , russian federation , and turkmenistan.9 compared with other european countries , newly independent states of the former soviet union have high cervical cancer incidence ( age - standardised rate > 150 per 100 000 population in kazakhstan and kyrgyzstan , and 163 per 100 000 population in moldova , compared with 70 per 100 000 population in western europe , according to globocan 2020 estimates ) .7 this high incidence is mainly attributed to insufficient organised screening program mes and inadequate diagnostic capacity.9 although free - of - charge annual cervical screening is available for women of reproductive age , the quality of cytology is frequently poor . 
even though this practice is not evidence - based , it remains common in the region . the aim of this study was to analyse stage - specific distributions and changes over time in breast cancer and cervical cancer incidence in the newly independent states of the former soviet union , to compare our results with european countries with available 362 vol 22 march 2021 articles population - based data on tnm stage , and to interpret the collected data in the context of national cancer control activities in the region . methods study design we defined newly independent states of the former soviet union as armenia , azerbaijan , belarus , georgia , kazakhstan , kyrgyzstan , republic of moldova , russian federation , tajikistan , turkmenistan , ukraine , and uzbekistan , excluding the baltic countries ( estonia , latvia , and lithuania ) that form part of the eu and as such abide by eu recommendations and guidelines on breast cancer and cervical cancer screening ( a corresponding updated and evidence - based set of guidelines is not available for the newly independent states of the former soviet union )  . 
we contacted national cancer registries and cancer statistics offices in 12 newly independent states and identified collaborators , to whom we sent letters of invitation , data collection templates , and study protocols ( in english and russian )  . we collected aggregated incidence data , defined using the international classification of diseases tenth revision ( icd - 10 ) 10 codes for breast cancer ( c50 ) and cervical cancer ( c53 ) , as well as cervical carcinoma in situ ( d06 ) by 5 - year age group and calendar year , as well as the following corresponding data quality indicators : the proportion of microscopically verified cases , the proportion of patients registered posthumously ( a specific indicator in the newly independent states of the former soviet union referring to cases registered based on autopsy or death certificate only3 ) , and the mortality to incidence ratio , where available . 
 for the mortality to incidence ratio , cancer mortality data were extracted from the who mortality database.11 no individual data were requested or used . we received data from ten ( 83% ) of 12 countries ; turkmenistan and tajikistan did not submit data . 
information on cervical carcinoma in situ was available in four countries ( belarus , georgia , russia , and ukraine )  . data sources population counts or estimates for the period 200817 were received from the statistics office of each country . 
thus , the data for these respective regions and periods were not included in the analysis . we used official cancer statistics data from armenia , azerbaijan , belarus , georgia , kazakhstan , kyrgyzstan , moldova , russia , ukraine , and uzbekistan . 
the obligatory reporting of cancer statistics in the newly independent states of the soviet union involves collection and processing of predefined paper - based registration forms at the medical statistics office of a regional oncology centre . 
reporting is required for all cases of malignant and in situ neoplasms ( icd - 10 codes c00c96 and d00d09 ) .12 in addition to the standard variables required for cancer registration , the registration form includes additional clinical information , such as tnm stage ( for all solid tumours , including female genital cancers ) , details of treatment , and follow - up for disease progression . 
stage distributions of cancers of visually accessible sites are reported as an indicator of preventive activities of regional oncology services.12 the data are reported from regional to national oncology centres , as well as annually to the ministry of health in an aggregated format . 
this data collection and reporting system has been preserved in most newly independent states , which continued the use of standard paper - based forms after the dissolution of the former soviet union . the annual report to the ministry of health contains two tables with data on the number of new cases or patients by cancer site ( icd - 10 codes ) as well as tnm stage , with stages i and ii grouped in most countries . 
 female and male breast cancers by stage are not reported separately . internationally published population - based cancer registry data from newly independent states of the former soviet union are sparse . 
saint petersburg ( russia ) and belarus cancer registries , included in cancer incidence in five continents volumes from 1983 , continued submitting data every 5 years , with some additional registries from the region included in later volumes.13 we used population - based cancer registry data from belarus , georgia , moldova , ukraine ( national ) , and russia ( 60 regions combined )  . 
additional requests for data were sent to the population - based cancer registries of arkhangelsk and samara ( both included in cancer incidence in five continents volume xi ) , tomsk , and the north western federal regions of russia . 
data on stage i and stage ii cancers were available separately from the population - based cancer registry data . data analysis we chose to present the stage distributions for official statistics ( overall ) as well as for population - based data ( by age group ) for the time period 201317 to enable comparisons with other countries . 
to assess these data in the context of screening , we examined breast cancer cases by stage for the age groups 1549 years , 5069 years , and 70 years , and for cervical cancer for age groups 1534 years , 3559 years , and 60 years . 
given well known difficulties in comparing staging data in different settingseg , as a result of variations in the completeness and accuracy of the source information we refrained from providing statistical measures of uncertainty . 
we used r ( version 3.6.3 ) software for all analyses . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
all authors had full access to all of the data and the final responsibility to submit for publication . results the description of data sources and data quality indicators is shown in the table . 
the proportion of patients diagnosed posthumously was < 2% in all countries ( data not shown )  . according to official statistics reports , over 50% of breast cancer cases in all countries were registered at stages iii , whereas in belarus , kazakhstan , and ukraine this proportion exceeded 75% ( figure 1a ; appendix p 1 )  . 
 more than 35% of breast cancer diagnoses were at late stages ( iiiiv ) in azerbaijan , georgia , kyrgyzstan , and uzbekistan ( figure 1a ; appendix p 1 )  . 
according to the population - based data , the proportion of stage i breast cancer cases was highest in the youngest age group in belarus , georgia , and ukraine , but in moldova and russia most stage i cases were diagnosed in those aged 5069 years ( figure 2a )  . 
georgia and moldova had a large proportion of breast cancers diagnosed at stages iii and iv , particularly in those aged 70 years and older . for cervical cancer , at least 70% of cases were registered as stage i or ii in kazakhstan , ukraine , and belarus . 
by contrast , in moldova and armenia , the proportion of stage iii - iv diagnoses was high ( > 50% ; figure 1b ; appendix p 1 )  . 
according to the population - based data , the proportion of stage i cervical cancer cases decreased with age in all countries , whereas the proportions of cases diagnosed at a late stage ( stages iii and iv ) increased with age , exceeding 50% in moldova and the tomsk region in those aged 60 years and older ( figure 2b )  . 
most invasive cervical cancers diagnosed at younger ages ( 1534 years ) were diagnosed at stage i , except in moldova . the number of cases and truncated ( 15 years ) agestandardised rates by cancer site in the participating cancer registries 201317 alongside corresponding population data are available in the appendix ( p 1 )  . 
 analysis of stage - specific changes over time indicated large and uniform increases in stage i breast cancer incidence , with the estimated annual percentage change ranging from 5% to 9% ( figure 3a ; appendix p 2 )  . 
incidence of stage iii breast cancer was stable or increasing across all regions , whereas the incidence of stage iv breast cancer increased in belarus and the north western federal regions of russia , but declined or was stable in the remaining regions . 
the incidence of cancers of unknown stage see online for appendix 364 vol 22 march 2021 articles a stage iii unknown kazakhstan belarus ukraine russia arm enia kyrgyzstan m oldova uzbekistan azerbaijan georgia decreased in all russian regions , but increased in belarus and ukraine . no decreases in truncated cervical cancer rates for all stages combined were observed over the 200817 period ( appendix p 3 )  . 
in belarus , the incidence of cervical carcinoma in situ was higher than for invasive cancer stages and increased from 2008 to 2017 ( estimated annual percentage change 8% ; appendix p 2 ) , as did the incidence of stage iii and stage iv disease , whereas the incidence of stage i and stage ii disease decreased ( figure 3b )  . 
similar increases in the incidence kazakhstan ukraine belarus russia kyrgyzstan uzbekistan georgia azerbaijan m oldova arm enia country figure 1 : proportion of new patients with breast cancer ( a ) and cervical cancer ( b ) or cases reported in official statistics by stage per diagnosis and country , 201317 male breast cancer cases are included . 
data for moldova are for 201316 . of localised disease , alongside stable diagnoses of metastatic breast cancer , have been reported from other countries during the imple mentation phase of organised screening , with a subsequent flattening of early - stage cancer incidence rates after full imple mentation of the programme.17 , 19 in this study , we observed generally stable incidence of late - stage breast cancer cases . 
increasing incidence of vol 22 march 2021 articles a stage unknown belarus georgia moldova nwfr arkhangelsk samara tomsk ukraine 60 regions of russia combined 1549 5069 1549 5069 1549 5069 1549 5069 1549 5069 1549 5069 1549 5069 1549 5069 1549 5069 belarus georgia moldova nwfr arkhangelsk samara tomsk ukraine 60 regions of russia combined 1534 3559 1534 3559 1534 3559 1534 3559 1534 3559 1534 3559 1534 3559 1534 3559 1534 3559 age group ( years ) age group ( years ) age group ( years ) age group ( years ) age group ( years ) age group ( years ) age group ( years ) age group ( years ) age group ( years ) figure 2 : proportion of new breast cancer ( a ) and cervical cancer ( b ) cases by stage and age group for each participating population - based cancer registry , 201317 data for georgia are for 201517 . 
nwfr = north western federal regions of russia . early - stage cancers with concomitant stable trends at metastatic stages is suggestive of overdiagnosis , which is a common concern with mammography screening.20 however , late - stage cancers could be biologically distinct , being more aggressive and more likely to present as interval cancers.21 despite modest screening coverage , 366 vol 22 march 2021 articles stage belarus iv unknown 60 regions of russia combined nwfr arkhangelsk samara tomsk ukraine 500 200 100 200 100 2008 2012 2016 2008 2012 2016 2008 2012 2016 2008 2012 2016 2008 2012 2016 2008 2012 2016 2008 2012 2016 year year year year year year year figure 3 : changes over time in truncated age - standardised incidence of breast cancer ( a ) and cervical cancer ( b ) by stage and participating population - based cancer registry , 200817 nwfr = north western federal regions of russia . overdiagnosis cannot be ruled out as a contributor to the marked increases in stage i cancers that were observed across the newly independent states of the former soviet union . 
the absence of a decline in late - stage cancers ( apart from in selected russian regions ) is consistent with overall increases in breast cancer incidence in the newly independent states . the newly independent states of the former soviet union have among the highest incidence of cervical cancer in the who european region , particularly among central asian countries , where cervical cancer incidence ranks second in frequency after breast cancer.22 our results indicate that , in contrast with recorded rates in most regions of the world , cervical cancer incidence is increasing in the newly vol 22 march 2021 articles independent states of the former soviet union . 
stagespecific results show the high proportion of cervical cancers diagnosed at late stages ( iiiiv ) , particularly in moldova and armenia , compared with corresponding proportions of 203% in norway , 21% in northern ireland ( uk ) , and 366% in czech republic.16 , 23 , 24 the absence of a decline in the incidence of late - stage cervical cancers in belarus , russian regions , and ukraine suggests little progress in prevention over the last decade , despite the potential of effective screening to prevent more than 150 000 cervical cancer cases by 2040 in russia alone.9 screening practices in the region are still largely untargeted and opportunistic , based predominantly on romanowsky - giemsa staining techniques , and without standard guidelines for management of abnormal cytology findings.25 although use of romanowsky - giemsa staining is common , there are considerable intercountry and intracountry variations across the newly independent states of the former soviet union , with the choice of staining technique depending on the hospital or laboratory , the regulations in place , and resources available . 
as each newly inde pendent state of the former soviet union is in a different phase of health - care system transition , accurate diagnosis and access to treatment for all cancers remains a challenge in many countries , given the lack of availability of chemotherapy or radiotherapy in some countries and a reliance on out - of - pocket payments for health services . 
 additionally , suboptimal pathology practices , exemplified by the persisting use of romanowski - giemsa staining for cervical cancer screening , can further delay accurate diagnosis , staging , and treatment . a major strength of this study is the use of previously unpublished data on tnm stage that are available from cancer registration systems across the newly independent states of the former soviet union.1 yet the parallel use of different tnm editions for registration and treatment purposes , often due to the absence of consensus within the clinical community , is a potential limitation of the results presented here . 
only six of 12 newly independent states of the former soviet union ( excluding baltic states ) have national or subnational population - based cancer registries in operation , with incidence data from belarus , ukraine , and four regional registries from russia considered high quality given their inclusion in the most recent volume of cancer incidence in five continents.26 variations in the reported mortality to incidence ratio could reflect differences in survival , as well as in completeness and validity of source data , and thus this indicator is difficult to interpret given the varying quality of mortality data in the region.27 in georgia and moldova , population - based cancer registries were established less than 5 years ago , and it is too early for the analysis of changes over time . 
elsewhere in the newly independent states of the former soviet union , despite existing cancer reporting systems , the implementation of population - based cancer registries remains in an early phase . 
nonetheless , even with the challenge of ensuring comparability of data across populations , we believe that the data on tnm stage at diagnosis collected from all cancer hospitals in the newly independent statesvia the long - established cancer reporting systems in each countryare representative of the distributions in the respective populations , and are therefore comparable . to prevent premature deaths , certain breast cancer and cervical cancer practices , such as opportunistic screening across non - targeted age groups with non - standard techniques ( eg , romanowsky - giemsa testing for cervical cancer , and ultrasound for screening of breast cancer among young women ) , need to be replaced by evidencebased and resource - adequate interventions . 
results of the who cervical cancer modelling consortium tasked with informing the who cervical cancer elimination strategy have shown that girls - only human papillomavirus ( hpv ) vaccination with 90% coverage alongside twicelifetime hpv - based screening could halve cervical cancer incidence in low - income and middle - income countries by 2048.28 alongside the introduction of hpv vaccination , moving from current opportunistic screening practices to population - based , quality - assured hpv screening for women beyond vaccination age would place the newly independent states of the former soviet union on the road to cervical cancer elimination as a public health problem over the coming decades . with respect to breast cancer , the decision over whether to implement rapid diagnosis or organised populationbased mammo graphy screening programmes should be tailored based on a situation analysis of each country , including the assessment of capacity for mammography screening and follow - up of positive cases , but also the public health capacity to establish , maintain , and manage quality assurance , including centralised screening databases that encompass all of the required functions . 
all authors had full access to all the raw data in the study and take final responsibility for the decision to submit for publication . declaration of interests ab reports personal fees from msd and biocad , outside the submitted work . 
all other authors declare no competing interests . data sharing the data that support the findings of this study are available from the first author upon reasonable request and with the permission of the contributing cancer registries . acknowledgments ar has been supported by a union for international cancer control ( uicc ) yamagiwa - yoshida memorial international cancer study grant ( uicc yamagiwa - yoshida award yy1 / 18 / 604150 )  . 
we thank the cancer registries of the following countries and their staff : armenia , azerbaijan , belarus , georgia , kazakhstan , kyrgyzstan , moldova , ukraine ( national registries ) , and the regional ( arkhangelsk , north - western region , samara , tomsk ) and federal registry of russia . 
where authors are identified as personnel of the international agency for research on cancer ( iarc ) or who , the authors alone are responsible for the views expressed in this article and they do not necessarily represent the decisions , policy or views of the iarc or who . peri - operative chemotherapy with or without bevacizumab in operable oesophagogastric adenocarcinoma ( uk medical research council st03 ) : primary analysis results of a multicentre , open - label , randomised phase 23 trial david cunningham , sally p stenning , elizabeth c smyth , alicia f okines , william h allum , sam rowley , laura stevenson , heike i grabsch , derek alderson , thomas crosby , s michael griffin , wasat mansoor , fareeda y coxon , stephen j falk , suzanne darby , kate a sumpter , jane m blazeby , ruth e langley summary background peri - operative chemotherapy and surgery is a standard of care for patients with resectable oesophagogastric adenocarcinoma . 
 methods in this multicentre , randomised , open - label phase 23 trial , we recruited patients aged 18 years and older with histologically proven , resectable oesophagogastric adenocarcinoma from 87 uk hospitals and cancer centres . 
patients in the control group ( chemotherapy alone ) received three pre - operative and three post - operative cycles of epirubicin , cisplatin , and capecitabine chemotherapy : 50 mg / m epirubicin and 60 mg / m cisplatin on day 1 and 1250 mg / m oral capecitabine on days 121 . 
patients in the investigational group received the same treatment as the control group plus 75 mg / kg intravenous bevacizumab on day 1 of every cycle of chemotherapy and for six further doses once every 21 days following chemotherapy , as maintenance treatment . 
randomisation was done by means of a telephone call to the medical research council clinical trials unit , where staff used a computer programme that implemented a minimisation algorithm with a random element to establish the allocation for the patient at the point of randomisation . 
the primary outcome for the phase 3 stage of the trial was overall survival ( defined as the time from randomisation until death from any cause ) , analysed in the intention - to - treat population . 
 findings between oct 31 , 2007 , and march 25 , 2014 , 1063 patients were enrolled and randomly assigned to receive chemotherapy alone ( n = 533 ) or chemotherapy plus bevacizumab ( n = 530 )  . 
3 - year overall survival was 503% ( 95% ci 455549 ) in the chemotherapy alone group and 481% ( 432527 ) in the chemotherapy plus bevacizumab group ( hazard ratio [ hr ] 108 , 95% ci 091129 ; p = 036 )  . 
wound healing complications were more prevalent in the bevacizumab group , occurring in 53 ( 12% ) patients in this group compared with 33 ( 7% ) patients in the chemotherapy alone group . 
in patients who underwent oesophagogastrectomy , post - operative anastomotic leak rates were higher in the chemotherapy plus bevacizumab group ( 23 [ 10% ] of 233 in the chemotherapy alone group vs 52 [ 24% ] of 220 in the chemotherapy plus bevacizumab group ) ; therefore , recruitment of patients with lower oesophageal or junctional tumours planned for an oesophagogastric resection was stopped towards the end of the trial . 
serious adverse events for all patients included anastomotic leaks ( 30 events in chemotherapy alone group vs 69 in the chemotherapy plus bevacizumab group ) , and infections with normal neutrophil count ( 42 events vs 53 )  . interpretation the results of this trial do not provide any evidence for the use of bevacizumab in combination with peri - operative epiribicin , cisplatin , and capecitabine chemotherapy for patients with resectable gastric , oesophagogastric junction , or lower oesophageal adenocarcinoma . 
 despite this increase in survival , mortality in patients with this disease remains high , with 5 - year overall survival for localised disease at diagnosis of only about 40%.3 , 4 bevacizumab , a monoclonal antibody that targets vegf , improves responses to chemotherapy and progressionfree survival , but not overall survival , in patients with advanced gastric cancer.5 , 6 in oesophagogastric cancer , a complete surgical resection ( r0 resection ) is an important predictor of long - term survival.7 we postulated that a higher proportion of patients responding to pre - operative chemotherapy would increase the likelihood of an r0 resection and lead to improved survival outcomes.8 therefore , we designed st03 as a phase 23 trial to assess the safety and efficacy of adding bevacizumab to perioperative chemotherapy for patients with resectable oesophagogastric cancer . the initial phase 2 stage of the trial focused on safety and feasibility in the first 200 patients ; these results have been reported previously.9 the addition of bevacizumab was feasible and did not seem to significantly increase toxic effects or the likelihood or severity of surgical complications . 
therefore , the study proceeded to the phase 3 stage . methods study design and participants we recruited patients aged 18 years and older with previously untreated , histologically proven , resectable junction adenocarcinoma of the lower oesophagus , oesophagogastric junction , or stomach from 87 uk hospitals and cancer centres . 
to be eligible , patients were required to have a who performance status of 0 or 1 and adequate cardiac , liver , renal , and bone marrow function to be eligible . 
in 2006 , the magic trial showed an improvement in progression - free survival and overall survival when peri - operative chemotherapy was given in addition to surgery , compared with surgery alone , in patients with resectable oesophagogastric adenocarcinoma . 
in 2011 , the avagast trial in advanced gastric cancer reported an improvement in tumour response and progression - free survival , but not overall survival , when bevacizumab was combined with chemotherapy . added value of this study to the best of our knowledge , this trial is the first study in which bevacizumab was given to patients with resectable oesophagogastric adenocarcinoma in the peri - operative setting ; the results provide no evidence of a benefit of bevacizumab administration in combination with peri - operative chemotherapy in these patients . 
moreover , the safety results indicate that bevacizumab administration might also be associated with impaired wound healing . implications of all the available evidence the results of this trial suggest that there is unlikely to be a role for bevacizumab in the treatment of localised , operable oesophagogastric cancer . 
every participating centre obtained local approvals . cisplatin , epiribicin , peri - operative randomisation and masking eligible patients were randomly assigned ( 1 : 1 ) to receive either and capecitabine chemotherapy or epiribicin , cisplatin , and capecitabine plus bevacizumab , in addition to surgery . 
 treatment allocation was done via a telephone call to the medical research council clinical trials unit at university college london ( normally by the research nurse at the site who was responsible for following up the patient ) , where trial management staff used a computer programme that implemented a minimisation algorithm with a random element and stratification by chemo therapy centre , site of tumour ( lower oesophagus vs oesophagogastric junction type i vs type ii vs type iii vs stomach ) , and tumour stage ( according to tnm 6th edition )  . 
 patients and investigators were not masked to treatment allocation . procedures epirubicin , cisplatin , and capecitabine chemotherapy was given as three pre - operative and three post - operative 21 - day cycles , consisting of 50 mg / m intravenous epirubicin and 60 mg / m cisplatin on day 1 and 1250 mg / m oral capecitabine on days 121 . 
patients in the chemotherapy plus bevacizumab group were given 75 mg / kg bevacizumab as a continuous intravenous infusion on day 1 of each of the chemotherapy cycles ( either before or after the chemotherapy was given )  . 
to maximise any potential treatment effect with an acceptable toxicity profile , patients in the bevacizumab group also received six further infusions of bevacizumab alone ( 75 mg / kg intravenously alone every 21 days ) as maintenance treatment after post - operative chemotherapy . no bevacizumab dose reductions were allowed . 
 bevacizumab was discontinued in the event of any new case of gastrointestinal perforation , arterial thromboembolic events ( including transient ischaemic attack , stroke , myocardial infarction , or new diagnosis of ischaemic heart disease ) , grade 3 or 4 haemorrhage , grade 3 or 4 congestive heart failure or left ventricular dysfunction , grade 4 hypertension , grade 4 proteinuria , tracheoesophageal fistula at any grade or any other fistula deemed to be possibly related to bevacizumab . 
all serious adverse events were reviewed for categorisation and severity by the chief investigator ( dc ) or trial physicians ( ecs , afo )  . surgery was scheduled 56 weeks after the last day of the final pre - operative chemotherapy cycle ; therefore , there were at least 8 weeks between the last pre - operative bevacizumab administration and surgery . 
surgical procedures were specified as follows ; for gastric or siewert type iii oesophagogastric junction tumours either proximal , total , or distal subtotal gastrectomy was recommended with a lymphadenectomy to include as a minimum lymph node stations 17 to ensure at least 15 nodes were excised ; for siewert type ii oesophagogastric junction tumours , either extended gastrectomy or two - field two - phase oesophago - gastrectomy with a lymph adenectomy ; for siewert type i oesophagogastric junction or lower oesophageal tumours , oesophagogastrectomy with either a two phase right thoracoabdominal approach or a left thoracoabdominal approach with a two field lymphadenectomy . 
minimal access procedures were allowed only in centres that had sufficient experience ( at least 20 such procedures done ) after review of outcomes and complication rates by surgeons from the trial management group . 
pathological evaluation of resected tumour specimens followed guidance that was compliant with the royal college of pathologists dataset for oesophagogastric cancer resections . we assessed to pre - operative tumour response chemotherapy with response evaluation criteria in solid tumors ( recist ) criteria ( version 1.0 ; assessed by ct scan , with laparoscopy , endoscopic ultrasound , or pet scans if clinically indicated ) and post - operatively at each centre by pathologists who assessed the resected tumour specimen to establish the extent of resection , margin involvement , extent of lymph node dissection , and mandard tumour regression grade . 
resections were judged to be curative ( r0 ) if the pathologist considered a radical resection had been undertaken and there was no evidence of microscopic residual disease with longitudinal margins ( proximal and distal ) microscopically clear and there were no viable tumour cells present within 1 mm of the oesophageal circumferential resection margins . 
cause of death and disease vol 18 march 2017 articles progression events were reported according to local investigator assessment . analysis of quality of life will be presented in a separate publication . 
 we assessed quality - of - life data with the european organisation for research and treatment of cancer ( eortc ) qlq - c30 and sto22 questionnaires , administered before and after post - operative chemo therapy and twice during the maintenance phase , then every 6 months post - surgery for 3 years and annually thereafter . 
 epiribicin , cisplatin , and capecitabine chemotherapy alone ( n = 533 ) epiribicin , cisplatin , and capecitabine chemotherapy plus bevacizumab ( n = 530 ) 425 ( 80% ) 108 ( 20% ) 434 ( 82% ) 96 ( 18% ) women age ( years ) median ( iqr ) ; range 63 ( 5668 ) ; 3179 64 ( 5669 ) ; 2882 we assessed cardiac function by echocardiogram or multiple gated acquisition scan at baseline and after preoperative and post - operative chemotherapy . 
in february , 2010 , a protocol amendment mandated a nadir neutrophil count on day 10 of the first pre - operative chemotherapy cycle with granulocyte colony stimulating factor ( gcsf ) recommended for all cases of grade 4 neutropenia , and at the investigators discretion for grade 3 cases , during all subsequent chemotherapy cycles . outcomes for the phase 3 analysis , the primary outcome measure from was overall survival defined as randomisation until death . 
stage 4a patients : t2 n1 m1a ( one in the chemotherapy alone group ) ; t3 n0n1 m1a ( two in the chemotherapy alone group and one in the chemotherapy plus bevacizumab group )  . 
these patients were randomly assigned after the inclusion of type ii oesophagogastric junction tumours but before oesophageal tumour staging was added to case report forms and were therefore staged under the gastric staging systestage 4 patients : all t4 n1n2 m0 . ( table 1 continues on next column ) table 1 : baseline characteristics 360 vol 18 march 2017 articles and curative ( r0 ) resection rates . 
all efficacy analyses were done on an intention - to - treat basis . disease - free survival was measured from a landmark point , taken to be 6 months from randomisation to allow for any difference in timing of surgery across all patients , to the first occurrence of disease recurrence or death . 
 patients who had an event before the landmark point and those who had a macroscopically incomplete ( r2 ) resection or no resection were deemed to have had a disease - free survival event at time zero . 
progression - free survival was measured from randomisation to the first occurrence of disease recurrence or death ; unlike disease - free survival , an r2 resection was not considered an event for this outcome measure . 
for the analysis of pathological tumour response , a mandard tumour regression grade of 1 , 2 , or 3 was considered a response and in the intentionto - treat comparison those who did not undergo a resection were included as non - responders . 
 sensitivity analysis of overall survival was repeated on the following pre - defined baseline subgroups : age ( < 60 years ; 6070 years ; > 70 years ) ; sex ; who performance status ; baseline tumour site ; baseline tumour stage ( separately for gastric / type iii oesophagogastric junction tumours and type i / ii oesophagogastric junction / lower oesophageal tumours )  . 
we did not do an analysis by the type of surgery because this was not known at baseline ; instead we analysed tumour site as a baseline surrogate for this variable . statistical analysis 5 - year overall survival in the epiribicin , cisplatin , and capecitabine chemotherapy alone group was estimated to be 40% . 
this estimate was based on the proportion of patients in the peri - operative chemotherapy group of the magic trial who were alive at 5 years ( 36% ) , 1 taking into consideration the possible effect of improvements in surgical technique , staging , and supportive care over time . 
a 10% improvement in survival would have been consistent with the benefit seen when adding bevacizumab in other settings at the time the trial was designed.10 to detect an absolute 10% improvement in 5 - year survival ( corresponding hazard ratio [ hr ] 076 ) , with 80% power and a two - sided 5% significance level , 420 deaths were required . 
on the assumption that the trial would take 34 years to complete recruitment , with 1824 months follow - up , the target sample size was estimated to be between 900 and 1100 patients . 
the accumulating data were monitored by an independent data monitoring committee ( idmc ) , which met 13 times between may , 2008 , and november , 2014 , to review safety data and efficacy analyses . 
analyses of overall survival , disease - free survival , and progression - free survival were based on all randomly assigned patients , whereas analysis of overall survival by resection status and mandard tumour regression grade were based on all randomly assigned patients with available pathological resection status and mandard 1063 patients recruited 533 randomly assigned to epirubicin , cisplatin , and capecitabine 530 randomly assigned to epirubicin , cisplatin , and capecitabine plus bevacizumab 4 did not start chemotherapy 1 ineligible 1 withdrew 2 straight to surgery 5 did not start chemotherapy 2 ineligible 2 withdrew 1 diagnosed with a colon lesion 529 started pre - operative chemotherapy 525 started pre - operative chemotherapy 472 completed three cycles 463 completed three cycles 73 had no resection 87 had no resection 21 found to be inoperable 10 died before surgery due 21 disease progression 2 comorbidity 2 patient refused surgery 8 other reasons 9 reason unknown 30 found to be inoperable 13 died before surgery due 16 disease progression 3 comorbidity 2 patient refused surgery 11 other reasons 12 reason unknown 457 underwent a resection 1 did not start pre - operative chemotherapy 438 underwent a resection 167 had no post - operative 181 had no post - operative chemotherapy 64 change in condition or not t 32 unacceptable toxicity 22 patient choice 15 died before due to start 12 post - operative complications 9 disease progression 8 incomplete resection 5 other or unknown reason chemotherapy 72 change in condition or not t 32 unacceptable toxicity 20 patient choice 15 died before due to start 18 post - operative complications 12 disease progression 5 incomplete resection 7 other or unknown reason 293 started post - operative chemotherapy 257 started post - operative chemotherapy 215 completed all three cycles 197 completed all three cycles 179 started maintenance dosing 119 received six doses 27 received ve doses 12 received four doses 8 received three doses 5 received two doses 8 received one dose figure 1 : trial profile vol 18 march 2017 articles tumour regression grade , respectively . 
 to compare the two groups in terms of the proportions of patients responding to chemotherapy and the proportions in whom curative resection was achieved , we used the test based on all randomly assigned patients who had available data from the relevant assessment . 
 results between oct 31 , 2007 , and march 25 , 2014 , 1063 patients to receive were enrolled and randomly assigned see online for appendix epirubicin , cisplatin , and capecitabine epirubicin , cisplatin , and capecitabine plus bevacizumab hr 108 in favour of the chemotherapy alone group , 95% ci 091129 ; log - rank p = 036 time from randomisation ( months ) 533 ( 11 ) 404 ( 52 ) 271 ( 85 ) 135 ( 59 ) 65 ( 31 ) 30 ( 20 ) 9 ( 8 ) 1 ( 0 ) 0 ( 0 ) 530 ( 11 ) 397 ( 52 ) 254 ( 69 ) 142 ( 71 ) 57 ( 27 ) 26 ( 12 ) 13 ( 13 ) 1 ( 0 ) 0 ( 0 ) number at risk ( number censored ) epirubicin , cisplatin , and capecitabine epirubicin , cisplatin , and capecitabine plus bevacizumab figure 2 : kaplan - meier plot of overall survival hr = hazard ratio . 
the median age of all enrolled patients was 63 years ( iqr 5668 ) , 859 ( 81% ) of 1063 patients were men , and 646 ( 61% ) had stage 3 or 4 disease ( according to tnm 6th edition )  . 
144 ( 14% ) had lower oesophageal tumours , 128 ( 12% ) siewert type i , 199 ( 19% ) siewert type ii , 209 ( 20% ) siewert type iii , and 383 ( 36% ) gastric . 
the proportion of patients undergoing pet scanning as part of staging has increased steadily during the course of the trial ( table 1 ) , but did not appear to differ between the groups . 
 1054 ( 99% ) of 1063 patients ( 529 in the chemotherapy alone group and 525 the chemotherapy plus bevacizumab group ) started chemotherapy after randomisation ( figure 1 )  . 
472 ( 89% ) of 529 patients in the chemotherapy group and 463 ( 88% ) of 525 in the chemo therapy plus bevacizumab group who started chemo therapy received all three pre - operative cycles . 
895 ( 84% ) of 1063 randomly assigned patients ( 457 [ 86% ] of 533 in the chemotherapy alone group vs 438 [ 83% ] of 530 in the chemotherapy plus bevacizumab group ) underwent a resection in the trial . 
 the median time from the start of the last pre - operative cycle to surgery was 62 days ( iqr 5668 ) in the chemotherapy alone group and 62 days ( 5769 ) in the chemotherapy plus bevacizumab group . 
293 ( 55% ) of 533 patients randomly assigned in the chemotherapy group and 257 ( 48% ) of 530 randomly assigned in the chemotherapy plus bevacizumab group re - commenced chemo therapy post - operatively ; 215 ( 73% ) of 293 patients in the chemotherapy group and 197 ( 77% ) of 257 patients in the chemotherapy and bevacizumab group received all three post - operative cycles ( figure 1 )  . 
of all randomly assigned patients , 212 ( 40% ) of 533 in the chemotherapy alone group and 195 ( 37% ) of 530 in the chemotherapy and bevacizumab group received all six scheduled cycles of chemotherapy . 
the appendix provides further details about pre - operative and postoperative chemotherapy , including numbers of patients who discontinued treatment or had dose reductions ( appendix pp 4 , 5 )  . 
 at the time of analysis , we used a reverse kaplan - meier method to calculate median follow - up , which was 384 months ( iqr 275508 ) in the whole population and 362 months ( 274514 ) in the chemotherapy alone group and 391 months ( 276505 ) in the chemotherapy and bevacizumab group . 
508 patients died ( 248 in the chemotherapy group and 260 in the chemotherapy and bevacizumab group ) and 85% of patients in each group 362 vol 18 march 2017 articles ( 451 of 533 given chemotherapy alone and 452 of 530 given chemotherapy and bevacizumab ) had either died or been followed up for at least 2 years . 
3 - year overall survival was similar in the two groups : 503% ( 95% ci 455549 ) in the chemotherapy alone group and 481% ( 432527 ) in the chemotherapy and bevacizumab group ( hr 109 in favour of the chemotherapy alone group , 95% ci 091129 ; log - rank p = 036 ; figure 2 )  . 
 insufficient patients ( n = 56 ) had reached the 5 - year timepoint at the time of analysis to give a reliable estimate of 5 - year overall survival . 
disease recurrence was confirmed in 210 and 192 patients , respectively ( 170 and 159 of whom subsequently died ) , with the remaining events attributable to death before reported recurrence ( 78 in the chemotherapy group and 101 in the chemotherapy plus bevacizumab group ) and a macro scopically incomplete resection ( 12 vs 10 )  . 
for progression - free survival , a macroscopically incomplete resection was not considered an event of interest , so the total number of events was therefore 288 in the chemotherapy alone group and 293 in the chemotherapy plus bevacizumab group . 
there was no evidence of a treatment effect of bevacizumab on either disease - free survival ( hr 104 , 95% ci 089122 ; p = 062 ) or progression - free survival ( hr 105 , 95% ci 089123 ; p = 056 )  . the analysis of recist responses to pre - operative chemotherapy ( partial or complete response vs stable disease , progressive disease , or death before tumour assessment ) is based on 875 patients ( 438 in the chemotherapy alone group and 437 in the chemotherapy plus bevacizumab group ) ; we excluded 188 patients ( 95 in the chemotherapy alone group and 93 the chemotherapy plus bevacizumab group ) with missing response data from the pre - operative tumour assessment . 
 the proportion of patients responding to treatment according to recist were similar in the two groups ( 183 [ 42% ] of 438 patients in the chemotherapy group vs 177 [ 41% ] of 437 in the chemo therapy and bevacizumab tumour group ; p = 070 )  . 
analysis of pathological responses based on mandard tumour regression grade ( grade 13 vs grade 45 or no resection ) includes 895 patients ( 452 chemotherapy alone , 443 chemotherapy plus bevacizumab ) ; those excluded are those who underwent a resection but had unavailable pathological tumour assessment data . 
the proportion of patients achieving pathological tumour responses were also similar between the groups ( 147 [ 33% ] of 452 patients in the chemotherapy alone group vs 135 [ 30% ] of 443 in the chemotherapy plus bevacizumab group ; p = 051 )  . 
percentages are based on all patients with non - missing data ; in the summary of lymph node dissection and mandard tumour regression grade , percentages are based on patients with non - missing data who underwent a resection only . 
includes those patients in which a viable tumour was present either at the circumferential margin or within 1 mm of the circumferential margin ( the above categories combined )  . 
resections were judged to be r0 by local pathologists in 321 ( 64% ) of 505 patients in the chemotherapy alone group and 305 ( 61% ) of 497 in the chemotherapy plus bevacizumab group ( p = 047 )  . 
when the comparison was repeated including only patients who underwent a resection ( r0 vs r1 ) , the proportions of r0 resections were again similar between the groups ( 321 [ 75% ] of 429 patients in the chemotherapy alone group vs 305 [ 75% ] of 405 in the chemotherapy plus bevacizumab group )  . 
 proportion of r0 resections varied by baseline tumour site ; gastric tumours had the highest proportion of r0 resections ( 265 [ 87% ] of 304 resections ) , compared with type iii oesophagogastric junction ( 117 [ 75% ] of 157 ) , type ii oesophagogastric junction ( 106 [ 72% ] of 148 ) , type i oesophagogastric junction ( 62 [ 61% ] of 102 ) , and lower oesophageal ( 76 [ 66% ] of 116 )  . 
circumferential margin involvement was only reported routinely by the pathologist for oesophagogastrectomies ; of 146 r1 oesophagogastrectomies , 72 ( 49% ) had a positive circumferential margin and 132 ( 90% ) were either at or within 1 mm of the circumferential margin . figure 3 shows the results of pre - defined baseline subgroup analyses for overall survival . 
in particular , in patients aged 70 years and older , significantly fewer patients who received chemo therapy alone died compared with those given chemo therapy plus bevacizumab ( figure 3 )  . 
however , in this subgroup , the proportion of deaths that were reported to be non - disease related was higher in the chemotherapy plus bevacizumab group than in the chemotherapy alone group ( 61 [ 30% ] patients given chemotherapy and bevacixumab vs seven [ 19% ] of 36 patients given chemotherapy alone )  . survival beyond the scheduled surgery timepoint assesed post - hoc was significantly longer in patients who had an r0 resection than in those with an r1 resection or no resection ( hr 023 , 95% ci 019028 ; p < 00001 ; figure 4 )  . 
our earlier comparison of the proportion of patients achieving a pathological tumour response categorised patients with a mandard tumour regression grade of 1 , 2 , or 3 as responders . 
however , our data suggest that those patients with a mandard tumour regression grade of 1 or 2 might represent a group with improved post - operative survival ( figure 5 )  . 
when such patients were compared with those with a mandard tumour regression grade of 3 , 4 , or 5 , or no resection post - hoc , post - operative survival was significantly better ( hr 030 , 95% ci 021044 ; p < 00001 ; figure 5 )  . the frequency and severity of adverse events occurring during either pre - operative or post - operative chemotherapy were similar between the groups ( table 3 , table 4 )  . 
neutropenia was the most common grade 3 or worse adverse event , both pre - operatively ( occurring in 145 [ 27% ] of 529 patients in the chemotherapy alone group vs 139 [ 26% ] of 525 patients in the chemotherapy plus bevacizumab group ) and post - operatively ( 95 [ 33% ] of 292 vs 81 [ 32% ] of 254 )  . 
this includes two fatal cases of 364 vol 18 march 2017 articles in the 257 patients infection with neutropenia , one in the chemotherapy in the chemotherapy plus alone group and one bevacizumab group . 
of the chemotherapy plus bevacizumab group who began post - operative chemotherapy , 179 ( 69% ) went on to receive maintenance bevacizumab and 16 ( 9% ) of these 179 patients reported a grade 3 or 4 toxicity during maintenance treatment , the most common of which were neutropenia ( four patients ) , anorexia ( 3 patients ) and lethargy ( 3 patients )  . 
the most commonly reported serious adverse events were gastrointestinal ( 60 events in the chemotherapy alone group vs 63 in the chemotherapy plus bevacizumab group ) , anastomotic leaks ( 30 events vs 69 ) , and infections with normal neutrophil count ( 42 events vs 53 )  . 
causes of death were reported to be mainly disease - related the ( 204 chemotherapy alone group vs 204 [ 78% ] of 260 in the chemotherapy plus bevacizimab group ) ; other deaths were due to chemotherapy - related toxic effects ( six [ 2% ] vs five [ 2% ] ) , or related to resection or reoperations ( 13 [ 5% ] in each group )  . 
other reasons were given for 58 patients ( 23 [ 9% ] in the chemotherapy group vs 35 [ 13% ] in the chemotherapy plus bevacizumab group ; appendix ) and the cause of death was unavailable for the remaining five patients ( two [ < 1% ] vs three [ < 1% ] )  . 
 resection 30 - day post - operative mortality was similar in the two groups ( 14 [ 3% ] of 457 patients who underwent resection in the chemotherapy alone group vs 11 [ 3% ] of 438 who underwent the chemotherapy and bevacizumab group )  . 
21 ( 5% ) of 457 patients in the chemo therapy alone group and 22 ( 5% ) of 438 in the chemotherapy and bevacizumab group died within 90 days of surgery . 
of the patents who underwent a resection , data from the post - operative assessment were available for 446 patients in the chemotherapy alone group and 427 in the chemotherapy plus bevacizumab group . 
the overall incidence of post - operative complications was slightly higher in the chemotherapy plus bevacizumab group , with 215 ( 48% ) of 446 patients in the chemotherapy alone group reporting complications com pared with 243 ( 57% ) of 427 patients in the chemotherapy plus bevacizumab group . 
wound healing complications in particular were more prevalent in the bevacizumab group , occurring in 53 ( 12% ) patients in this group compared with 33 ( 7% ) patients in the chemotherapy alone group . 
however , the overall incidence of complications that were deemed to be life - threatening was similar in both groups , at 8% ( 37 of 446 patients in the chemotherapy alone group and 34 of 427 in the chemotherapy plus bevacizumab group )  . 
 appendix p 6 provides full details of the post - operative complications . an increased incidence of post - operative anastomotic leak in the chemotherapy plus bevacizumab group became apparent towards the end of the trial . 
at a planned idmc review in june , 2013 , leaks were recorded in 30 ( 10% ) of 312 patients in the chemotherapy group and 48 ( 16% ) of 297 in the chemotherapy plus bevacizumab group ( compared with 14 [ 8% ] of 179 and 19 [ 11% ] of 170 , respectively , at the previous idmc review in july , 2012 )  . 
overall post - operative survival times given by the extent of resection , calculated from 6 months post - randomisation until death ( to allow for the difference in timing of surgery between the groups )  . 
overall post - operative survival times given by mandard tumour regression grade , calculated from 6 months post - randomisation until death ( to allow for the difference in timing of surgery between the groups )  . 
 survival curves are unadjusted for covariates and the analysis includes all patients with non - missing mandard tumour regression grade ( 168 patients with missing data are excluded )  . 
in june , 2013 , 12 ( 9% ) of 132 patients in this subgroup who received chemotherapy alone had post - operative anastomotic leak versus 29 ( 24% ) of 123 who received bevacizumab , compared with 18 ( 10% ) of 180 versus 19 ( 11% ) of 174 , respectively , in all other patients . 
no other relevant clinical characteristics were identified that might explain the increased frequency of anastomotic leak , nor was there any evidence of a centre effect ( data not shown )  . 
 * these toxic effects were added to the chemotherapy toxicity assessment case report forms after the trial started and as such , not all participants were asked about these specific toxic effects . table 3 : adverse events reported during pre - operative chemotherapy 366 vol 18 march 2017 articles tumours planned for an oesophagogastric resection , and pre - operative bevacizumab was discontinued in such patients who had already been recruited . at the time of the final analysis ( sept 30 , 2015 ) , in patients undergoing oesophago - gastrectomy , we recorded ( 10% ) of post - operative anastomotic 233 patients in the chemotherapy alone group versus 52 ( 24% ) of 220 in the chemotherapy plus bevacizumab group compared with 20 ( 9% ) of 213 and 23 ( 11% ) of 207 , in 23 leaks respectively , in all other patients . 
overall , most of the 103 cases in which onset dates were available occurred during the period immediately after surgery ( 40 [ 39% ] within 5 days of surgery and 80 [ 78% ] within 10 days )  . 
 leak onset dates were provided on serious adverse event reports and were therefore not available for 15 cases in which the event did not satisfy the criteria for a serious adverse event . 
 * these toxic effects were added to the chemotherapy toxic effect assessment case report forms after the trial started and as such , not all participants were asked about these specific toxic effects . table 4 : adverse events reported during post - operative chemotherapy vol 18 march 2017 articles died within 30 days of the operation versus seven ( 9% ) of 75 in the chemotherapy plus bevacizumab group and revisional operations 22 ( 51% ) of 43 patients in the chemotherapy alone group compared with 24 ( 32% ) of 75 in the chemotherapy plus bevacizumab group . ( appendix ) were required discussion the results of our trial show that the addition of bevacizumab to peri - operative epiribicin , cisplatin , and capecitabine chemotherapy did not improve overall survival resectable in patients with potentially oesophagogastric adenocarcinoma . 
there was no clinical evidence of a differential biological effect on tumour growth ; the proportions of patients responding to preoperative chemotherapy assessed by both radiological recist criteria and mandard tumour regression grade from the resected specimen , as well as r0 resection rates , were similar in both groups . 
 this finding is in contrast to those of one small study ( n = 80 ) , which reported that bevacizumab in combination with docetaxel , oxaliplatin , and fluorouracil increased the proportion of r0 resections achieved in patients with locally advanced gastric cancer , 12 and results from studies in advanced ( unresectable and metastatic ) gastric cancer in which bevacizumab in combination with cisplatin and capecitabine given as first - line treatment increased the proportion of patients achieving a response ( 374% vs 460% ; p = 0032 ) and progression - free survival ( hr 080 ; p = 0037 ) but not overall survival.5 additionally , ramucirumab , a monoclonal antibody against vegf receptor 2 , increases median overall survival compared with placebo from 38 months to 52 months as secondline treatment in advanced disease13 and from 74 to 96 months compared with placebo , in combination with paclitaxel in the same setting.14 although an insufficient number of patients had reached the 5 - year timepoint to give a reliable estimate of 5 - year overall survival , the scarcity of evidence for an effect on tumour growth and overall survival to this point suggest that it is unlikely a treatment effect would emerge with longer follow - up . neoadjuvant bevacizumab has also been assessed in other tumour types and has been associated with increased clinical and pathological responses ; 1517 however , such an effect was not evident in the st03 trial . 
most ( 88% ) patients in the st03 trial received 9 weeks of pre - operative chemotherapy , which has previously been shown to enhance tumour down - staging1 and improve overall survival . 
however , the lack of effect shares similarities with results from studies in other tumour types in which promising results with bevacizumab in the advanced setting have not been replicated in earlier stage disease , although these studies were mainly done in the adjuvant setting , for example in breast18 and colorectal19 , 20 cancer . the finding of an increased anastomotic leak rate in patients who had undergone oesophago - gastrectomy was unexpected . 
this period extends well beyond the reported half - life of bevacizumab ( 20 days ) and was believed to be sufficient to prevent effects on post - operative outcomes . 
the primary outcome measures for the phase 2 component were based on tumour perforation rates , cardiac assessments , and post - operative complications.11 in the phase 2 analysis ( n = 200 ; 101 patients in the chemotherapy alone group , 99 in the chemotherapy plus bevacizumab group ) , the anastomotic leak rate was 4% in both groups ( five cases in each group ) with 107 ( 54% ) patients having gastric tumours , 71 ( 36% ) oesophagogastric junction type iii , and 22 ( 11% ) oesophagogastric junction type ii . 
 these figures compare to 275 ( 32% ) , 141 ( 16% ) , and 175 ( 21% ) , respectively in the subsequent 863 patients , with the remainder having oesophagogastric junction type i ( 128 patients ) and lower oesophageal ( 144 patients ) tumours ( recruited after march , 2011 )  . 
this change in eligibility criteria increased the proportion of patients undergoing oesophago - gastrectomy , potentially explaining why the increased leak rate was not apparent earlier in the trial . the treatment of anastomotic leaks varies across the uk ; however , centres in this study used the same treatment irrespective of which group the patient was surgeons used omentum for anastomosis coverage according to standard practice , although at the time of designing the study , randomised data were not available to support this practice . 
although there is a possibility that this method overdiagnosed even small ( non - clinically significant ) leaks , we do not believe that this had a differential effect on rates in each group . careful review of possible confounding factors including centre and laparoscopic surgical approaches did not provide any clear explanation for the increased leak rate and suggests that there could be a prolonged effect of bevacizumab that impairs wound healing . 
findings of one study21 showed that bevacizumab has sustained effects on vegf inhibition more than 6 weeks after dosing , and findings of several rectal cancer in which bevacizumab was used in conjunction with neoadjuvant chemotherapy or chemoradiotherapy showed increased rates of post - operative complications.2225 tumour and blood specimens were collected at baseline in this trial and will be used to investigate whether patients susceptible to long - term effects of bevacizumab such as impaired wound healing can be identified . trials the potential limitations of our study were the inclusion of both gastric and oesophageal tumours and a generous targeted difference of 10% absolute difference in survival . 
however , in our subgroup analysis we recorded no indication of a differential effect by tumour site , or any evidence of a differential biological effect based on r0 resection rates , disease - free survival , or 368 vol 18 march 2017 articles progression - free survival . 
as with the magic trial1 that compared surgery alone with surgery and peri - operative chemotherapy , about half of patients ( 550 [ 52% ] of 1063 ) started post - operative chemotherapy and only 119 ( 22% ) of 530 in the chemotherapy plus bevacizumab group completed all chemotherapy cycles plus the six cycles of maintenance bevacizumab . our data are consistent with findings that r0 resection is an important predictor of long - term survival . 
in future clinical trials , identification of patients at risk of a positive resection margin might have a role in treatment selection ; careful consideration of the clinicopathological features associated with r1 resection will help to inform these decisions . 
the suggestion from these results that a mandard grade of 1 or 2 predicts a better survival outcome ( as opposed to the usual approach of considering mandard grades 13 as a response and grades 45 as no response ) requires further evaluation ; however , in this trial , patients with a mandard grade 1 or 2 seem to have improved survival compared with those with grade 3 . 
a similar survival advantage for mandard grade 1 and 2 responses was seen in the magic trial26 and in the recently reported mrc oe05 trial27 in which two cycles of neoadjuvant cisplatin and docetaxel , oxaliplatin , and fluorouracil were compared against four cycles of neoadjuvant epirubicin , cisplatin , oesophagogastric junction and oesophageal adeno carcinoma . 
however , as intensification of chemotherapy in the oe05 trial did not lead to improved overall survival for the group of patients treated with chemotherapy as a whole , it is unclear whether mandard tumour regression grade 12 ( or complete pathological response ) is a valid surrogate for overall survival as an endpoint in clinical trials . capecitabine and for in conclusion , the addition of bevacizumab to perioperative chemotherapy for patients with resectable oesophagogastric cancer did not lead to an overall survival benefit ; therefore these results are not practice changing . 
all authors contributed to the interpretation of the data and reviewing of the report . declaration of interests dc holds grants from amgen , astrazeneca , bayer , celgene , merrimack , medimmune , merck serono , and sanofi . 
sps , sr , ls , and rel are employed by the uk medical research council , which received funding from cancer research uk and an educational grant from f hoffmann la - roche limited . 
dc and ecs are funded by the national institute for health research biomedical research centre based at the royal marsden and institute of cancer research . published online june 12 , 2020 s1470 - 2045 ( 20 ) 30352 - 1 for the lancets editorial see lancet 2020 ; 395 : 1813 for more on ascos ethnic diversity strategic plan see j clin oncol 2017 : 35 : 257679 for more on lori pierces statement see connection.asco.org / blogs / responding - racism - and - healthinequality - cancer - carecommunity for more on whitecoats4blacklives see racism , discrimination , and the practice of oncology the appalling death of george floyd on may 25 , 2020 , at the hands of the minneapolis police in the usa has sparked large rallies and protests on a global scale . 
we have seldom had to consider our skin colour as a determinant of what happens in our lives and can hardly imagine the consequences of such an indiscriminate and baseless notion , or the daily psychological trauma of confronting this issue . on june 11 , 2020 , an editorial in the lancet stated that racism is a public health emergency of global concern . 
we echo this and go furtherwith specific reference to the african slave trade , this is a public health crisis that started in the 15th century , but one that society chose to ignore for generations despite very notable remonstrations , movements , and uprisings . 
one shocking statistic of current relevancy is that a black man in some states in the usa nowadays has a higher chance of being killed by law enforcement than by covid - 19 . 
among us oncologists , for example , just 23% self - identify as black or african american , despite the fact that people of this ethnic origin account for 13% of the us population . 
on a broader scale , in 2018 , just 5% of all active physicians in the usa were black or african american , a mere 36% had university tenure , and 84% of applicants to medical school were black or african american . 
these enormous disparities highlight the astounding scale of inequity . in 2017 , the american society of clinical oncology ( asco ) published a strategic plan for increasing racial and ethnic diversity in the oncology workforce . 
responding to the current crisis on june 3 , 2020 , the new asco president , lori pierce , remarked , we must commit the same energy and focus we pour in to conquering cancer to addressing the systemic issues that affect the health of people of colourwe must work together to enact meaningful change . 
a culturally diverse workforce makes a lot of sense , not just in terms of a fundamental fairness in society , but also from the perspective of having a better appreciation of the prevailing socioeconomic challenges and other factors among ethnic groups that affect access to health care and clinical trials , and treatment outcome . 
 having a more representative , multicultural workforce that understands these important distinctions improves care for all patients , irrespective of race or ethnic origin . journals also have a part to play in representing the interests of black and ethnic minorities by ensuring fair representation in the media ; highlighting disparities where they exist ; educating readers on the underlying medical , scientific , and health system challenges specific to diverse peoples ; championing change and an end to discrimination ; andcruciallylistening and adapting to the communitys needs . 
in the past two decades , the lancet oncology has published numerous series and commissions dedicated to these types of issues , but more can , and will , be done . 
indeed , the lancet has pledged solidarity with the black lives matter movement and committed to turn this pledge into real actions through the material published , the work commissioned , and the people recognised in the pages of its many whitecoats4blacklives is a us organisation run by medical students with a mission to eliminate racism in medicine and promote health and better lives for people of colour . 
they have three goals : to foster debate on racism as a public health concern , to end race discrimination in medical care , and to prepare future doctors to be advocates for racial justice . 
the lancet oncology vol 21 july 2020 editorial articles preventable fractions of cervical cancer via e ective screening in six baltic , central , and eastern european countries 201740 : a population - based study salvatore vaccarella , silvia franceschi , david zaridze , mario poljak , piret veerus , martyn plummer , freddie bray summary background cervical cancer incidence remains high in several baltic , central , and eastern european ( bcee ) countries , mainly as a result of a historical absence of e ective screening programmes . 
as a catalyst for action , we aimed to estimate the number of women who could be spared from cervical cancer across six countries in the region during the next 25 years , if e ective screening interventions were introduced . methods in this population - based study , we applied ageperiodcohort models with spline functions within a bayesian framework to incidence data from six bcee countries ( estonia , latvia , lithuania , belarus , bulgaria , and russia ) to develop projections of the future number of new cases of cervical cancer from 2017 to 2040 based on two future scenarios : continued absence of screening ( scenario a ) versus the introduction of e ective screening from 2017 onwards ( scenario b )  . 
projected rates up to 2040 were obtained in scenario a by extrapolating cohort - speci c trends , a marker of changing risk of human papillomavirus ( hpv ) infection , assuming a continued absence of e ective screening in future years . 
scenario b added the e ect of gradual introduction of screening in each country , under the assumption period e ects would be equivalent to the decreasing trend by calendar year seen in denmark ( our comparator country ) since the progressive regional introduction of screening from the late 1960s . findings according to scenario a , projected incidence rates will continue to increase substantially in many bcee countries . 
very high age - standardised rates of cervical cancer are predicted in lithuania , latvia , belarus , and estonia ( up to 88 cases per 100 000 )  . 
according to scenario b , the bene cial e ects of e ective screening will increase progressively over time , leading to a 5060% reduction of the projected incidence rates by around 2040 , resulting in the prevention of cervical cancer in 1500 women in estonia and more than 150 000 women in russia . 
this notice should be preserved along with the articles original url . introduction in the next few decades , several million women living in the baltic , central , and eastern european ( bcee ) region will be at high risk of developing cervical cancer . 
 at present , cervical cancer incidence and mortality are higher in bcee countries than elsewhere in europe1 and are rising , 24 partly due to an absence of screening interventions that are , at best , opportunistic with relatively low coverage and quality.5 although the introduction of prophylactic vaccination against human papillomavirus ( hpv ) would substantially reduce the number of future cases of cervical cancer , the full e ect , in terms of a reduction in all - ages cervical cancer incidence , will not be detectable for more than 30 years.6 hence , the imple mentation of high - quality screening activities can still potentially play a major role in the prevention of cervical cancer and bridge the gap until the longer - term e ects of hpv vaccination programmes are seen . changes in sexual behaviour and increased exposure to high - risk hpv ( eg , hpv - 16 or hpv - 18 types ) , the main cause of cervical cancer , led to increasingly higher risks of women developing cervical cancer in the generations of women born around or after the 193050s in most vol 17 october 2016 1445 articles for the iarcs cancer incidence in five continents series see for russias national database of regional cancer registries see statistics / malignant_tumors research in context evidence before this study we searched pubmed with the search terms cervical cancer and trends and ( eastern europe or baltic ) and cervical cancer and ( prevention or screening ) and ( eastern europe or baltic ) to assess available evidence for time trends and historical cervical cancer prevention activities in each of the six countries studied in these regions . 
despite some e orts , screening activities have been absent or , at best , opportunistic with low coverage and quality in the studied countries of estonia , lithuania , latvia , belarus , bulgaria , and russia . 
 added value of this study as a catalyst for action , we analysed cervical cancer incidence from population - based cancer registries in these bcee countries and projected the number of women that could be spared from cervical cancer diagnoses over the next 25 years in the region upon swift introduction in 2017 of e ective screening programmes . 
under the assumption that screening - related gains could be as favourable as those shown in the long - term trends in cervical cancer incidence in denmark , we estimate that 180 000 new cases of cervical cancer could be prevented from 2017 to 2040 in the six countries . 
 implications of all the available evidence the scale of the rapid increase in risk in recent generations of women , most of whom are outside the target age range of the hpv vaccine , and the clear evidence of a prevention e ect can and must strengthen the resolve to immediately launch e ective screening programmes in baltic , central , and eastern european countries . 
the use of hpv testing - based screening programmes , as recommended by who for countries without established cytology - based programmes , could further accelerate the screening bene ts and , in combination with a prompt introduction of hpv vaccination , drastically reduce the burden of cervical cancer . european countries , 24 , 7 especially for those born after world war 2.8 indirect evidence also suggests that high - risk hpv infection has become progressively more prevalent since the 1960s in several european countries , 911 including countries in central and eastern europe.12 , 13 in regions where high - quality , cytology - based cervical cancer screening programmes were implemented several decades ago ( eg , in northern europe ) , the intervention has countered the increasing generational risks , and incidence has uniformly decreased , making cervical cancer a relatively rare disease . 
the recorded trends in nordic countries have provided an important evidence base long - term e ectiveness of high - quality mass screening programmes since their introduction in the 1960s , 14 a period when the incidence of women with cervical cancer was very high and , in some cases ( eg , in denmark ) , equivalent to that seen in some eastern african populations ( uganda and zimbabwe ) today.1 the for as a catalyst for the implementation of screening activities , we quanti ed the maximum potential e ect of screening , in terms of the number of cervical cancer cases that could theoretically be prevented in bcee countries by the year 2040 , if screening were introduced by 2017 with a level of e ectiveness similar to that seen historically in denmark . 
we developed a robust method for the projection that re ect the two underlying factors a ecting cervical cancer incidence : period e ects that re ect changes in cervical cancer risk through time , implementation of e ective screening mimic programmes , with declining incidence downwards across targeted age groups ; and birth cohort e ects , which are proxies for changes in sexual behaviour and increased risk of infection with high - risk hpv in successive generations of women.15 the methods study design and data sources in this population - based study , we tted ageperiod cohort ( apc ) models to incidence data to develop projections of the future number of new cases of cervical cancer in six bcee countries from 2017 to 2040 under two scenarios . 
in scenario a , we calculated the number of new cases that would have arisen in the continued absence of screening , and in scenario b , the number of new cases that would have arisen after e ective screening from 2017 . 
 we selected three baltic countries ( estonia , latvia , and lithuania ) , and three central or eastern european countries ( belarus , bulgaria , and russia ) , based on the availability of high - quality and representative cancer inicidence data . 
for all countries except russia , new cases of invasive cervical cancer were obtained from national population - based cancer registries of the international agency for research on cancers ( iarc ) cancer incidence in five continents series , of which the most recent ( volume x ) spans to 2007 . 
 population data were based on the country - speci c and age - speci c population estimates of 201540 from the united nations population division ( the 2010 revision ) .16 procedures and statistical analysis analyses were restricted to include cervical cancer diagnoses at ages 3074 years because recommended screening ages tend to range from 2564 years , with bene cial e ects starting a few years after screening to 74 years of age . 
truncated and extending ( asr , hereafter incidence age - standardised rates 1446 vol 17 october 2016 articles see online for appendix referred to as incidence ) adjusted for the e ect of age using weights of the world standard population were calculated by year of cancer diagnosis.17 we used the apc forecasting model based on our previous work ( appendix pp 12 ) .3 , 7 in brief , poisson regression models were tted within a bayesian generalised additive models framework to summarise trends in terms of age , period , and cohort e ects.18 we circumvented the non - identi ability problem that characterises apc models by taking advantage of the consistent association between age and cervical cancer that has been recorded in unscreened populations ( ie , a steady rise in prevalence up to roughly 45 years of age , followed by a plateau ) .19 this pattern was also recorded in populations from nordic countries in pre - screening periods . 
we could , therefore , constrain incidence rates in both screened and unscreened populations to be equal at ages 4549 years and 6569 years , thus enabling the estimation of a unique set of parameters for the age , period , and cohort e ects.3 , 7 , 19 , 20 in scenario a , we made forecasts assuming continued absence of e ective screening . 
we obtained expected future incidence rates of cervical cancer up to 2040 by extrapolating period and cohort e ects with smoothing functions , under the assumption that age e ects remain unchanged in future years . 
the canonical log link function for apc models for period and cohort e ects was replaced by the corresponding rst - order approximation of the taylor series expansion for the exponential , resulting in more conservative projections than those that would be obtained by using the log link function.21 using a bayesian framework and gibbs sampling , we obtained the expected number of cervical cancer cases by running chains of 10 000 iterations after discarding the rst 1000 possibly unstable samples . 
prediction intervals for future cancer incidence projections were not reported . in scenario b , we made forecasts under the assumption that e ective screening in all six countries took place from 2017 . 
in this second scenario , we postulated that the gradual e ect of implementing e ective screening on cervical cancer incidence would be equivalent to the decreasing trend by calendar year recorded in denmark ( our comparator country ) upon early implementation of high - quality conventional cytology screening in the late 1960s . 
the key assumption was that decreases in periodspeci c e ects in denmark represent an achievable bene cial e ect of screening activities on cervical cancer incidence , whereas the absence of such period e ects , as seen in bcee countries , represents an absence of e ective screening activities . 
although the e ect of screening - related decreases was reasonably consistent across nordic countries since the late 1960s , the largest decreases by calendar period as estimated by the apc analyses occurred in denmark.3 , 7 , 20 national projections were based on a scenario in which high - quality screening would be implemented in bcee countries in 2017 , extrapolating the age and cohort e ects into the future , while projecting the equivalent period e ects only until 2017 and , thereafter , projecting a declining trend with a slope equal to that estimated for period e ects in denmark after the introduction of screening in the period from the late 1960s to 2010 ( appendix pp 12 ) .3 , 7 we estimated the number and proportion of cervical cancer cases that could be prevented by screening during 201740 from the di erence between projected rates derived in scenario a versus scenario b . 
extensive sensitivity analyses were done ( appendix )  . role of the funding source the funder of the study had no involvement in data collection , analysis , or interpretation of the results ; study design ; patient recruitment ; writing of the report , or any observed projected prediction base ( timespan in years ) mean cases per year , n person - years * asr 200307 per 100 000 women asr 203640 with no screening asr 203640 with screening from 2017 cumulative number of incident cases , 201740 with no screening cumulative number of incident cases , 201740 with screening from 2017 number of cervical cancer cases potentially preventable by screening ( % of total with no screening ) , 201740 with screening from 2017 estonia 19682007 ( 40 ) lithuania 19782007 ( 30 ) latvia belarus 19832007 ( 25 ) 19782007 ( 30 ) bulgaria 19932008 ( 16 ) 1010 19932012 ( 20 ) 11 043 russia total 431 354 456 268 261 442 252 644 875 684 672 551 502 314 434 301 306 278 233 4853 16 105 7773 34 911 29 967 452 173 3392 11 322 5003 22 594 21 576 301 999 1461 ( 30% ) 4783 ( 30% ) 2770 ( 36% ) 12 318 ( 35% ) 8392 ( 28% ) 150 175 ( 33% ) 179 899 asr = age - standardised incidence rate . 
 table : observed and projected cases and incidence of cervical cancer under di erent scenarios for women aged 3074 years in the six countries vol 17 october 2016 1447 estonia belarus observed projected observed projected articles lithuania bulgaria latvia russia 1461 cases 2770 cases 8392 cases 1970 1990 2010 2030 1970 1990 2010 2030 year year no screening ( scenario a ) screening from 2017 ( scenario b ) preventable cases figure 1 : observed and projected incidence of cervical cancer in six baltic , central , and eastern european countries forecasts of future cervical cancer rates according to two scenarios : no screening ( red circles ) and e ective screening commencing in 2017 ( purple circles )  . 
the introduction of e ective screening shows a progressive e ect similar to that recorded in denmark after the introduction of screening in the 1960s . aspect pertinent to the study . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results in total , our analysis included 280 149 recorded cases of cervical cancer in the six bcee countries and approximately 1060 million women - years of follow - up . 
 the observed incidence in 200307 varied substantially across countries , ranging from roughly 2526 cases per 100 000 in russia , latvia , and belarus to about 4445 per 100 000 in lithuania and bulgaria . 
increases in cohort - speci c risks in successive generations of women born between the 1940s and 1950s were seen in all studied countries ( appendix p 3 )  . 
 under the scenario a assumption ( no e ective screening ) , the projected cohort e ects will continue until 2040 with period e ects being quite stable ( appendix p 3 )  . 
our projections suggest that a failure to introduce screening will result in more than 450 000 new cases of cervical cancer being diagnosed in russia , 35 000 in belarus , 30 000 in bulgaria , and more than 25 000 combined in estonia , lithuania , and latvia during 201740 . 
the forecasts to 2040 suggest that the incidence will at least double in the absence of screening in ve of the six countries , reaching an incidence of more than 60 per 100 000 for 203640 in estonia , latvia , and belarus and more than 85 per 100 000 in lithuania ( gure 1 )  . 
a smaller increase in the forecasted incidence is predicted in bulgaria where , despite the high incidence in 200307 , projections of cohort - speci c e ects are expected to be more modest ( table )  . scenario b projections suggest that the implementation of high - quality cervical cancer screening programmes in bcee countries from 2017 will have a progressive e ect after the introduction of screening , with decreases in cervical cancer incidence projected to 2040 ( gure 1 )  . 
the projected incidence in 203640 is approximately half of the projected rates obtained in scenario a of no e ective screening , which is about 30 or lower per 100 000 in all selected bcee countries other than lithuania , where the incidence increases to roughly 43 per 100 000 ( table )  . 
 the cumulative number of cervical cancer cases that could be theoretically prevented by screening during 201740 varies between countries , from almost 1500 in estonia to more than 150 000 in russia ( gure 1 , table )  . 
 the percentage of new cases of cervical cancer potentially preventable by screening on average during the period 201740 was estimated to range from 28% ( bulgaria ) to 36% ( latvia ; table )  . 
this proportion , however , increases progressively with time , with reductions in incidence being similar across the six countries , reaching 5060% in 2040 , to the no e ective screening scenario ( gure 2 )  . 
 discussion our study supports the notion that e ective screening programmes could have a major e ect in the next few decades in countries where the incidence of cervical cancer is frequent and implementation of screening activities has been limited . 
the bene cial e ects after implementation of screening in 2017 increase progressively over time , with a projected reduction in cervical cancer incidence of 5060% by 2040 and with only minor di erences across the studied countries that are mainly due to the di erent projections for the cohort e ects.7 , 22 our projections suggest that an increasing number of women in the six bcee countries will be 1448 vol 17 october 2016 articles latvia russia belarus estonia lithuania bulgaria diagnosed with cervical cancer during the next 30 years in the absence of e ective screening . 
incidence in 203640 is thus predicted to be similar to that observed in women in denmark ( incidence of approximately 68 per 100 000 ) around 1960 , 17 before the advent of organised screening . 
according to our projections , the immediate launch of e ective screening programmes would substantially change this adverse future scenario , preventing almost 180 000 new diagnoses of cervical cancer over a 25 - year period in the six countries . dynamic models suggest that hpv vaccination is expected to change all - age cervical cancer incidence only after several decades6 and thus will have a limited e ect on incidence before 2040 . 
bulgaria and latvia ( as well as slovenia , the czech republic , macedonia , hungary , and croatia ) have integrated hpv vaccines into their national immuni sation programme started providing routine vaccination free of charge to adolescent girls.5 coverage is not , however , reported . 
in russia , only small - scale regional vaccination programmes have been implemented , resulting in more than 20 000 girls being vaccinated.23 in most bcee countries , including lithuania , estonia , and belarus , hpv vac cination has yet to be incorporated into national programmes.5 , 23 however , even in the best - case scenario of an accelerated implementation of the vaccine national coverage , the next two to three generations of women beyond the target age for vaccination will be at high risk of cervical cancer.24 so far , none of the studied bcee countries have established organised , high - quality or high - coverage cervical cancer screening programmes , and roughly the same situation applies to other countries in the region . 
some e orts , however , have been made , 25 , 26 especially after the release of the european union guidelines on screening in 2008.27 the baltic countries of estonia , lithuania , and latvia established organised cytology - based screening programmes around 2005 that partly function , although low coverage , absence of quality assurance , and opportunistic screening outside the main programme are major obstacles.28 , 29 in bulgaria , cervical cancer screening has been opportunistic for the past few decades , and plans for organised screening have not yet started.30 in russia , and in belarus and other countries of the former soviet union , screening is mainly opportunistic . 
since 2002 , the moscow region reorganised screening activities based on a callrecall system ( inviting women for screening on a regular basis ) and the number of gynaecological examinations increased substantially , although no centralised screening database exists and the coverage of the targeted population is not known.23 romania and croatia started organised screening in 2012 , but programme indicators have not been reported ( poljak m , university of ljubjana , personal communication )  . 
indeed , reliable screening indicators 2020 2025 2030 2035 2040 year figure 2 : estimated percentage of cervical cancer cases expected to be potentially preventable by screening in 2040 in six baltic and eastern european countries the percentage of cervical cancer cases prevented is calculated as : projected 1projected 2 100 / projected 1 . 
 are absent in all bcee countries , and the low participation rates in the screening programme point to a need for central governments to ensure a vastly improved population coverage by organised screening . 
a particularly positive example comes from slovenia , where , in a relatively short time and with a ordable investment , the country moved from an opportunistic to an organised national screening programme ; the result was a dramatic drop in cervical cancer incidence rates , from 15 to six cases per 100 000 during 200315.25 none of the bcee countries seem to have planned for the use of hpv - based screening which , compared with cytology , provides better and more durable negative predictive value against high - grade cervical disease , requires a simpler logistic and health - care infrastructure , is more reproducible , and is likely to be more cost e ective.30 , 31 the use of the more sensitive hpv testing is recommended by who guidelines for countries without an already functioning e ective , high - coverage cytologybased programme.32 the comparisons across di erent areas in europe sharing similar underlying risk factors allowed us to build projections for bcee countries in a scenario where the possible future onset of screening activities could theoretically produce a similar e ect on cervical cancer risk as that produced historically in nordic countries . 
 adopting the principles of pre ventability , denmark was vol 17 october 2016 1449 articles in denmark those recorded chosen as the reference country because , of the nordic countries , it had the largest screening - related decrease in period e ects and therefore represented the largest prevention gain through cytology - based screening.3 furthermore , rates of cervical cancer in denmark in the 1960s were even higher compared with bcee countries , possibly because of di erences in sexual behaviour and persistent high - risk hpv infections . 
despite varying baseline incidence , the relative e ect of screening in driving down incidence has been quite consistent across nordic countries.7 we therefore believe that the use of di erent reference countries would not have changed our projected scenarios substantially . 
although the estimated risk reduction might be over - optimistic if bcee countries are unable to implement screening programmes that are as e ective as those implemented in nordic countries in the past , our projection allows an estimate of the upper limit of cervical cancer cases that are preventable by cytology - based programmes . 
the use of the hpv test as the primary test would most probably enhance screening e ectiveness , and lead to an even greater number of prevented cervical cancer cases , provided that high coverage quality control of test results , exhaustive work - up , and , when necessary , treatment of screening - positive women were in place . 
 additionally , the higher sensitivity of hpv testing enables screening to begin after age 30 years and the adoption of longer screening intervals . our approach circumvented the non - identi ability problem of the apc models based on the observation of a uniform age curve for cervical cancer incidence , thus allowing the estimation of a unique set of parameters for period and cohort e ects . 
although there are no identi ability issues in projecting future incidence rates , 33 , 34 speci c parameterisations of period and cohort trends were essential in our analysis to ensure appropriate interpretation of cervical cancer incidence trends and the development of alternative scenarios of future burden . 
 screening is expected to de ect the incidence trends downward across all targeted age groups and this should be visible as a period e ect , whereas changes in risk factors chie y manifest themselves as variations in risk across successive birth cohorts of women ( ie , a cohort e ect )  . 
strong support for such an interpretation of the risk pro le of period and cohort e ects is gained by the results from previous analyses that compared the e ect of long - term screening programmes ( in nordic countries ) with their absence ( in eastern european and baltic countries ) .2 , 3 nordic countries and eastern european countries showed similar increases in cervical cancer prevalence in the birth cohorts born after 1950 , 3 probably due to a progressive increase in the risk of hpv exposure . 
in nordic countries , the strong period - related decreases are visible and the consequences of rising high - risk hpv - related generational risks are largely negated.3 , 7 , 20 conversely , in bcee countries , where screening - related e ects are absent , the result is a remarkable and avoidable rise in future cervical cancer incidence , re ecting the increasing risk in successive generations of women . 
 a possible limitation of this study is that the projected generational risks were based on trends recorded in the youngest generations of women , for which data might be sparse , and were assumed to continue to increase across the whole study period . 
distinct observable changes in cohort e ects have been noted in historical trends ( eg , a u - shaped pattern in several european countries ) , with decreases in cervical cancer cases before the introduction of screening reported for generations of women born during 192030 followed by risk increases in successive generations . 
 previous reports have postulated that cohort e ects for the risk of some cancers , including cervical cancer , might follow a roughly cyclical pattern.35 , 36 however , the patterns found in our study seem irregular and vary by country , mainly related to di erent changes in sexual behaviour and perhaps parity , which is also a risk factor for cervical cancer . 
the use of spline functions to parametrise our model enabled a exible assessment of changing patterns , including possible cyclical patterns , of the cohort e ects within the prediction base and a projection of the most recent trend into the future . 
mathematical transmission models would help to understand the future generational trends , although they would require a number of additional assumptions about the sexual habits and spread of hpv in di erent populations . 
 infection comes we cannot precisely estimate the future incidence rates and burden of cervical cancer and it is possible that trends will evolve di erently from those predicted by our model . 
predictions by their nature are fraught with future uncertainty and , until methodological developments allow meaningful uncertainty intervals to be for cancer intervals 1450 vol 17 october 2016 articles estimated , several authors have explicitly discouraged their reporting.38 , 4042 our projections represent the best possible assessment of future scenarios given the data available and it is reassuring that forecasts obtained with a di erent method ( nordpred ) , produced very similar results for the scenario with no future screening improvements . 
we restricted our analyses to age groups that are usually targeted for cervical cancer screening and extended them to age groups where the protective e ect of screening is strong . 
hpv vaccination is the best strategy for preventing cervical cancer in bcee countries in the long term , yet strengthening screening activities is a key intervention to prevent a future increase in cervical cancer diagnoses in the next two or three generations of women.5 protocols combining hpv vaccination of adolescents with several rounds of organised hpv - based screening have been proposed as a viable option in high - risk populations such as the bcee countries.31 , 32 in the absence of action , the cervical cancer risk in women living in these countries might reach levels similar to those seen in some sub - saharan african countries today43 and in denmark half a century ago.44 contributors sv and fb conceived and designed the study , contributed to data collection and analysis and interpretation of the results , and wrote the rst draft of the report . 
all authors contributed to the interpretation of the data and approved the nal version of the report . declaration of interests mpo reports grants and personal fees from abbott and grants from merck sharp & dohme received during 200714 ; he declares no competing interest since september , 2014 . 
all other authors declare no competing interests . acknowledgments mpo is supported by the seventh framework programme of directorate - general research of the european commission , through the coheahr network ( grant number 603019 )  . 
we thank the directors and sta of the cancer registries in europe who collected the data used in this study in belarus , bulgaria , denmark , estonia , latvia , lithuania , and russia . 
 correction to lancet oncol 2020 ; 21 : e57588 correction to lancet oncol 2021 ; 22 : 2942 correction to lancet oncol 2021 ; 22 : 8597 bahadoer rr , dijkstra ea , van etten b , et al . 
short - course radiotherapy followed by chemotherapy before total mesorectal excision ( tme ) versus preoperative chemoradiotherapy , tme , and optional adjuvant chemotherapy locally advanced rectal cancer ( rapido ) : a randomised , open - label , phase 3 trial . 
 lancet oncol 2021 ; 22 : 2942in figure 1 in this article , in the standard of care group , of the 187 patients who had adjuvant chemotherapy , 185 should have been indicated as having this chemotherapy according to hospital policy . 
fixeddose combination of pertuzumab and trastuzumab for subcutaneous injection plus chemotherapy in her2 - positive early breast cancer ( federica ) : a randomised , open - label , multicentre , non - inferiority , phase 3 study . 
lancet oncol 2021 ; 22 : 8597in table 2 of this article , the cycle 7 ( predose cycle 8 ) pertuzumab serum geometric mean auc 021 days ( percentage cv ) , g / ml per day should have been 2440 ( 242 ) for the intravenous infusion group and 2440 ( 262 ) for the fixed - dose combination group , and the cycle 7 ( predose cycle 8 ) trastuzumab serum geometric mean ( percentage cv ) , auc 021 days g / ml per day should have been 1640 ( 240 ) for the intravenous infusion group and 1700 ( 289 ) for the fixed - dose combination group . 
intermittent schedules of the oral rafmek inhibitor ch5126766 / vs - 6766 in patients with ras / raf - mutant solid tumours and multiple myeloma : a single - centre , open - label , phase 1 dose - escalation and basket dose - expansion study . 
also , sentence two of paragraph four of the discussion should have read these tumours harboured a range of ras and raf mutations , including kras gly12asp , kras gly12val , kras gly12arg , brafve , and hras gly13arg . 
however , given that one in two people will be diagnosed with cancer in their lifetime , and with the prospect of a growing and ageing population , the absolute number of people living with cancer is set to increase substantially in the near future . 
a cancer diagnosis is a serious and potentially life - threatening condition , and there is no desire to trivialise it , but a reluctance to speak about diagnosis , treatment , and supportive care , out of fear or stigma , isolates patients and their carers . 
moreover , this silence prevents survivors from grappling with the more mundane , but crucial , aspects of long - term care and survival , such as reintegration into home and work life after end of treatment , behaviours for long - term wellness , and end - of - life considerations . although online forums , patient support groups , and charity and advocacy groups exist to support those living with cancer , the mainstream media is uniquely positioned to widely disseminate stories and viewpoints of people living with and surviving cancer . 
 such advocacy can simultaneously give a voice to the issues and educate the public about the diversity of people living with cancer and their experiences , as well as reveal the areas where medicine and society could better serve the survivor community as a whole . 
in one such column in the new york times , called living with cancer , susan gubar , a professor emeritus of english at indiana university , in , usa , uses her experience as a survivor of ovarian cancer to discuss the realities , challenges , and hopes of patients with cancer and survivors . 
columns like these serve to inculcate the general public with an understanding , and thereby acceptance of , cancer as a part of life . by contrast , the mainstream media has done less well at illuminating end - of - life care for patients with terminal illness . 
an example that bucks the trend , however , is the emergence of death cafes , as reported recently in the guardian : these meetings are opportunities to discuss the often overlooked and di cult aspects of end - of - life care , such as preparing for death and quality of death . 
shedding light on the issues patients face at this juncture is crucial to improve end - of - life care as well as to break the silence around this di cult topic . 
death cafes o er venues for supportive discussion of the anxieties surrounding death , and their existance highlights both the desire and need for these types of dialogue . mainstream media could go further to raise the pro le of cancer and end - of - life care beyond a few column inches in newspapers and magazines , using more subtle means to capture the experience of patients , carers , and medics . 
inclusion of characters and storylines via the arts ( for example , in the british radio sitcom bad salsa ) that incorporate cancer not as the subject , but simply as one aspect of a story , help us to trans gure the feared and unknown into the familiar and routine fabric of the public consciousness . cancer is becoming an ever - expanding presence in our society , and we would bene t from reconciling its ability to scare and isolate with its ubiquity and c , cancer must longer the big survivability . 
an increasing focus and re ection on cancer in the mainstream media is a good way of destigmatising and desensitising issues among the general public , while also bringing comfort , hope , and perhaps , some useful advice to patients and survivors alike . 
we investigated whether replacing mitomycin with cisplatin in chemoradiation improves response , and whether maintenance chemotherapy after chemoradiation improves survival . methods in this 22 factorial trial , we enrolled patients with histologically con rmed squamous - cell carcinoma of the anus without metastatic disease from 59 centres in the uk . 
patients were randomly assigned to one of four groups , to receive either mitomycin ( 12 mg / m on day 1 ) or cisplatin ( 60 mg / m on days 1 and 29 ) , with uorouracil ( 1000 mg / m per day on days 14 and 2932 ) and radiotherapy ( 504 gy in 28 daily fractions ) ; with or without two courses of maintenance chemotherapy ( uorouracil and cisplatin at weeks 11 and 14 )  . 
391 of 432 ( 905% ) patients in the mitomycin group versus 386 of 431 ( 896% ) in the cisplatin group had a complete response at 26 weeks ( di erence 09% , 95% ci 49 to 31 ; p = 064 )  . 
overall , toxic e ects were similar in each group ( 334 / 472 [ 71% ] for mitomycin vs 337 / 468 [ 72% ] for cisplatin )  . 
3 - year progression - free survival was 74% ( 95% ci 6977 ; maintenance ) versus 73% ( 95% ci 6877 ; no maintenance ; hazard ratio 095 , 95% ci 075121 ; p = 070 )  . 
chemoradiation became the standard of care for treatment of squamous - cell cancer of the anus after three phase 3 trials35 showed that radiotherapy with concurrent uorouracil and mitomycin resulted in better local control and recurrence - free or progression - free survival than did radiotherapy alone , or radiotherapy with uorouracil . 
the rationale for comparing 516 vol 14 may 2013 articles for the ucl clinical trials centre see patients , clinicians ( including those assessing patients ) , and investigators analysing data were not masked to treatment allocation . 
minimisation was used and strati ed according to primary site ( canal vs margin ) , t stage , n stage , age ( < 65 years vs 65 years ) , sex , and glomerular ltration rate ( < 60 ml / min vs 60 ml / min )  . 
 phase 1 delivered 306 gy in 17 daily fractions to the international commission of radiological units and measurements ( icru ) intersection point , as determined following the guidelines in icru report 50 , 13 using nonconformal rectangular parallel - opposed elds aiming to treat all pelvic nodes ( except the common iliac ) to a dose of 306 gy . 
phase 2 was conformally planned using ct images to deliver 198 gy to the icru intersection point in 11 daily fractions over 15 days ( weekends excluded ) treating the primary tumour and the whole anal canal with a 3 cm margin around all macroscopic tumours de ning the eld size ( for further details see protocol , available from the ucl clinical trials centre website )  . 
 the quality assurance of this trial will be reported elsewhere . patients received uorouracil 1000 mg / m per day on days 14 ( week 1 ) and 2932 ( week 5 ) by continuous 24 h intravenous infusion with radiotherapy , and either 12 mg / m of mitomycin as an intravenous bolus on day 1 only ( maximum single dose 20 mg ) or 60 mg / m of cisplatin by intravenous infusion on days 1 and 29 ( up to a maximum surface area of 20 m , therefore maximum single dose was 120 mg )  . 
maintenance chemotherapy 940 patients randomly assigned 246 assigned to cisplatin and no maintenance * 222 assigned to 246 assigned to 226 assigned to cisplatin and maintenance mitomycin and no maintenance * mitomycin and maintenance 246 in intention - to - treat analysis 222 in intention - to - treat analysis 246 in intention - to - treat analysis 226 in intention - to - treat analysis figure 1 : trial pro le four patients assigned to cisplatin received mitomycin : two treated o trial , one administrative error , one had an inadequate glomerular ltration rate ; two patients assigned to mitomycin received cisplatin during week 5 of chemoradiation : one treated o trial , one because of toxic e ects ( see appendix for details of compliance )  . 
 * 23 patients assigned to the cisplatin group and 23 assigned to the mitomycin group were not eligible for maintenance randomisation and were excluded from the analysis of progression - free survival for the maintenance endpoint . 
 cisplatin instead of mitomycin with uorouracil - based chemoradiation was based on seemingly higher complete response rates with cisplatin , 79 and acceptable acute toxic e ects in phase 2 trials . 
patients were eligible if they had histologically con rmed invasive squamous cell , basaloid or cloacogenic carcinoma of the anal canal and margin that was deemed t for investigated treatment ; a glomerular ltration rate of more than 50 ml / min ; acceptable blood test results ( haemoglobin > 100 g / l , > 1 10 platelets per l , > 3 10 white blood cells per l ) ; liver function tests within two times the normal range ; and adequate cardiac function . 
exclusion criteria were metastatic disease , other major malignancy likely to compromise life expectancy or completion of trial treatment , comorbidity including being hiv - positive and cardiac diseases , previous complete local excision , and previous radiotherapy to the pelvis . 
the study was approved by local research ethics committees , and all patients provided written informed consent . randomisation and masking patients were randomly assigned before starting initial treatment to one of four treatment groups . 
patients were assessed for tumour response by digital examination using the response evaluation criteria in solid tumors ( recist ) 15 at 11 , 18 , and 26 weeks from the start of treatment . 
routine biopsies were not recommended because of the risk of radionecrosis but the 26 - week assessment included imaging ( abdominopelvic ct and radiography and whole body ct ) as at baseline . 
haematological toxic e ects were assessed at week 11 for all patients , and for those receiving maintenance treatment , haematological toxic e ects were checked before the rst and second cycles of maintenance treatment and non - haematological toxic e ects were checked weekly until 30 days after the last dose of study drug . 
 after the assessment at week 26 , patients were reassessed once every 2 months in the rst year , once every 3 months in the second year , once every 6 months until the fth year , and yearly thereafter . 
abdominopelvic ct was done at 12 and 24 months after the start of treatment and afterwards only when clinically indicated or if the patient had signs or symptoms of recurrence . for the comparison of mitomycin with cisplatin the primary endpoints were complete response ( complete disappearance of clinically or radiologically overt disease ) at 26 weeks from start of chemoradiation , and grade 3 or 4 acute toxic e ects for 4 weeks after chemoradiation ( haematological , gastrointestinal , and genitourinary )  . 
for the comparison of maintenance with no maintenance treatment the primary endpoint was progression - free survival . secondary endpoints included colostomy - free survival ( including pretreatment colostomies not reversed within 8 months after starting treatment , or any colostomies after treatment ) ; ineld recurrence rate ; cause - speci c survival ; and overall survival ( death from any cause )  . 
we also analysed progression - free survival by treatment during chemoradiation ; by disease stage ( t1 or t2 and t3 or t4 ) ; and by node status ( node positive and node negative disease )  . statistical analysis we calculated a target sample size of 950 patients based on detecting an improvement in 3 - year progression - free survival from 750% to 825% ( for the maintenance comparison )  . 
this sample size would enable us to detect an increase in the number of patients with complete response from 90% to 95% for cisplatin versus mitomycboth comparisons had 80% power and twosided 5% statistical signi cance . 
the sample size was increased in march , 2007 , from 600 to 950 patients , on the recommendation of the independent data monitoring committee because fewer progression - free survival events occurred than expected . events included in progression - free survival were progressive disease , local recurrence ( with or without metastatic disease ) , metastases , or death from any cause , but new tumours were not included . 
colostomy - free survival events were all post - treatment colostomies , hr 095 ( 95% ci 075121 ; p = 070 ) number at risk no maintenance maintenance mitomycin , no maintenance cisplatin , no maintenance mitomycin , maintenance cisplatin , maintenance time since randomisation ( years ) number at risk mitomycin , no maintenance cisplatin , no maintenance mitomycin , maintenance cisplatin , maintenance figure 2 : progression - free survival comparing the maintenance versus no maintenance groups ( a ) , and all four groups ( b )  . 
the four curves in b overlap , providing no evidence for an interaction between chemoradiotherapy regimen and maintenance ( p = 094 )  . vol 14 may 2013 articles see online for appendix pretreatment colostomies not reversed within 8 months from the start of treatment , and death from any cause . 
 all survival endpoints were measured from the date of randomisation , and patients who did not have the event of interest were censored at the date of last follow - up . 
 role of the funding source the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
of the 46 patients assigned to mitomycin or cisplatin , but not randomly assigned to a maintenance group , ten died : seven from anal cancer , one related to surgery , one from another cancer , and one not related to cancer . 
one case of neutropenic sepsis in the mitomycin , no maintenance group ; one acute myocardial infarction in the cisplatin , no maintenance group ; one case of pancolitis in the mitomycin , maintenance group ; and one bowel perforation in the cisplatin , maintenance group . 
these patients were excluded from the analysis of progression - free survival for the maintenance endpoint . total compliance to radiotherapy was good with few patients failing to complete the planned dose of 504 gy in either group ( 37 of 472 [ 8% ] in the mitomycin group and 44 of 468 [ 9% ] in the cisplatin group )  . 
370 of 472 patients ( 78% ) in the mitomycin group versus 352 of 468 ( 75% ) in the cisplatin group completed radiotherapy as planned ( ie , with no treatment gap or dose reduction ; appendix )  . 
 only 18 patientsnine in the mitomycin group and nine cisplatin grouphad interruptions to treatment for 8 days or more . 862 of 940 ( 92% ) patients received the full rst course of uorouracil with mitomycin or cisplatin without delays or dose reductions ( 433 of 472 in the mitomycin group , 429 of 468 in the cisplatin group , appendix )  . 
703 of 940 patients ( 75% ) completed the entire chemotherapy regimen during chemoradiation without delays or dose reductions ( 365 of 472 in the mitomycin group , 338 of 468 in the cisplatin group )  . 
of the 237 who did not , 222 ( 94% ) had either dose delays , reductions , or both in line with protocol recommendations or to prevent toxic e ects . 
only two ( < 1% ) were not given any chemotherapy during chemoradiation ( one died and did not have radiotherapy , and one withdrew from the study , both in the cisplatin group ; not excluded from the intention - totreat analysis ) ; and data were missing for six patients in the cisplatin group and seven in the mitomycin group . 
 the main reasons for non - completion were toxic e ects ( 66 patients in the mitomycin group and 78 in the cisplatin group )  . 357 of 448 to receive maintenance chemotherapy started treatment . 
286 ( 64% ) completed the rst course of treatment according to schedule , and 196 ( 44% ) completed both courses without any delay or dose reduction ( 105 of 226 [ 46% ] in the mitomycin group and 91 of 222 [ 41% ] assigned to cisplatin ; appendix )  . 
119 patients had dose modi cation because of maintenance did not receive it , 41 of the 91 ( 45% ) choosing not to receive any maintenance chemotherapy ( appendix )  . 
386 ( 896% ) in the cisplatin group and 391 ( 905% ) in the mitomycin group had a complete response at 26 weeks ; absolute di erence 09% ( 95 ci 49 to 31 ; p = 064 ; table 2 )  . 
 we assessed progression - free survival in 223 patients in the cisplatin , no maintenance group ; 222 in the cisplatin , maintenance group ; 223 in the mitomycin , no maintenance group ; and 226 in the mitomycin , maintenance group . 
3 - year progression - free survival was 74% ( 95% ci 6977 ) in the maintenance group and 73% ( 6877 ) in the no maintenance group ( hr 095 , 95% ci 075121 ; p = 070 ; gure 2 )  . 
 progression - free survival did not di er signi cantly between patients who took mitomycin and cisplatin during chemoradiation ( hr 095 , 95% ci 075119 ; p = 063 ; appendix )  . 
3 - year progression - free survival of patients without maintenance treatment was 73% ( 95% ci 6778 ) in the mitomycin group versus 72% ( 6678 ) in the cisplatin group ; for those who were given maintenance treatment , it was 73% ( 6678 ) versus 74% ( 6880 )  . 
 3 - year progression - free survival of patients with stage t1 or t2 disease was 80% ( 95% ci 7484 ) for patients taking maintenance treatment , 84% ( 7888 ) for those not taking maintenance treatment , 80% ( 7484 ) for those taking mitomycin , and 83% ( 7887 ) for those taking cisplat the respective progression - free survivals for t3 or t4 disease were 67% ( 6073 ) , 62% ( 5568 ) , 65% ( 5971 ) , and 62% ( 5569 )  . 
overall progression - free survival was 68% ( 6273 ) for node - positive patients and 76% ( 7279 ) for node - negative patients ; with similar rates for the treatment groups ( 67% [ 5974 ] with mitomycin vs 69% [ 6176 ] with cisplatin for nodepositive disease ; 76% [ 7080 ] vs 76% [ 7181 ] for nodenegative disease )  . 
the overlapping curves in gure 2b suggest no interaction between the two treatment strategies ( p = 094 )  . 211 patients died , 155 from anal cancer ( including treatment - related deaths ; table 3 )  . 
the hr for cisplatin versus mitomycin was 105 ( 95% ci 080138 ; p = 070 ) ; and for maintenance versus no maintenance the hr was 107 ( 081141 ; p = 065 )  . 
 3 - year anal cancer survival rates were also much the same for each treatment group ( appendix )  . 118 of 884 ( 13% ) assessable patients had colostomies at randomisation ( appendix )  . 
3 - year colostomy - free survival was 73% ( 95% ci 6779 ) in the mitomycin , main tenance group , 75% ( 6880 ) in the cisplatin , maintenance group , 75% ( 6880 ) in the mitomycin , no maintenance group , and 72% ( 6677 ) in the cisplatin , no maintenance group ( appendix )  . 
 table 5 : reported grade 34 adverse events during maintenance treatment with t1 or t2 disease and 61% ( 5666 ) for patients with t3 or t4 disease . toxic e ects during chemoradiation were as expected for this population and were much the same in the mitomycin and cisplatin treatment groups ( table 4 )  . 
the proportion of patients who had a maximum grade 12 adverse event was 133 of 472 ( 28% ) in the mitomycin group versus 126 of 468 ( 27% ) in the cisplatin group and the proportion of patients who had grade 34 adverse events was 334 of 472 ( 71% ) versus 337 of 468 ( 72% ; table 4 ) , although more patients had grade 3 haematological toxic e ects in the mitomycin group than in the cisplatin group ( 26% vs 16% ; p < 0001 )  . 
grade 3 or 4 toxic e ects were generally uncommon , and occurred in similar proportions in patients who had previously taken mitomycin ( 39 / 226 ; 17% ) and those who had previously taken cisplatin ( 39 / 222 ; 18% ; table 5 )  . 
treatment - related mortality was less than 1% ( n = 8 , four died during or up to 4 weeks after chemoradiation , three died 58 weeks after chemoradiation , and one died shortly after maintenance ; table 3 )  . 
subgroup analyses according to baseline characteristics did not show signi cant di erences in progression - free survival for any comparison ( appendix ) , or overall survival ( data not shown )  . discussion our results show no evidence of any improvement in the complete response rate or 3 - year progression - free survival , and similar acute grade 34 toxic e ects , when uorouracil plus cisplatin chemoradiation is compared with uorouracil plus mitomycin chemoradiation . 
our 22 randomisation enables us to examine complete response to chemoradiation with either concurrent mitomycin or cisplatin in a straightforward and simple manner , and also to test the bene t of adding further maintenance chemotherapy after initial chemoradiation to assess whether it enhances the chemoradiation response , or improves progression - free survival . 
preliminary results from our trial have already been used to guide practice.17 also , maintenance chemotherapy with uorouracil and cisplatinwhich had been used in some placescould now be stopped , and future patients can avoid unnecessary treatment ( as well as reducing nancial costs )  . 
 although grade 34 haematological toxic e ects were less common with uorouracil plus cisplatin ( 26% vs 16% ) patients , these were almost entirely related to white blood cells but were not su cient to increase neutropenic sepsis . 
this marginal bene t is likely to be outweighed by the extra resources needed to administer cisplatintwo courses of either all day or overnight intravenous treatment with hydration , compared with only a single dose of mitomycin delivered over 10 m cisplatin contraindicated ; however , this situation is rare . could be used when mitomycin survival maintenance chemotherapy using two cycles of uorouracil plus cisplatin did not improve progressionfree compared with no maintenance chemotherapy . 
exploratory subset analyses ( appendix ) show no evidence of any bene t for maintenance chemotherapy in any subgroups including patients with a high rate of relapse ( t3 or t4 and n + disease )  . 
these ndings accord with the rtog - 98 and accord - 03 trials , 10 , 11 , 16 which used neoadjuvant cisplatin - based chemotherapy before chemoradiation . our ndings are based on a 22 factorial trial design in which no evidence exists of an interaction between the chemoradiation and maintenance chemotherapy comparisons . 
fluorouracil and mitomycin chemoradiation should remain the standard of care for anal cancer because of similar e cacy and toxic e ects , fewer cycles of chemotherapy , fewer non - chemotherapy drugs , less time in the chemotherapy suite , less expense , and no risk of neuropathy compared with cisplatin , and the addition of maintenance chemotherapy in routine clinical practice is not justi ed . the high complete response rate ( 90% ) , similar 3 - year progression - free survival in the mitomycin and cisplatin groups , an overall 3 - year colostomy - free survival of 74% , and the very few ( 14 of 844 patients ) colostomies done for 522 vol 14 may 2013 articles ascribe late treatment e ects compares favourably with the results of other phase 3 trials.10 , 11 , 16 75% of patients had local control with organ preservation and avoided colostomy . these outcomes e cient radiobiological schedule . 
the two main achievements of our trial were the ability to maintain high compliance with 504 gy and the ability to give concurrent chemotherapy over a short overall treatment time by avoiding a planned gap in treatment.18 , 19 the median overall treatment time in the rtog 8704 trial was 49 days and in the rtog 9811 trial it was 42 days.5 , 11 , 20 a shorter overall treatment time is clinically important because a longer overall duration of radiation treatment adversely a ects local control in anal cancer.21 , 22 in the ecog e4292 phase 2 study using cisplatin - based chemoradiotherapy , 23 the clinical complete response rates were higher in patients who did not get a planned radiotherapy treatment break compared with those who did ( 12 / 13 vs 13 / 19 ; 92% vs 68% )  . 
possible strategies for improvement include the use of a non - cross - resistant induction chemotherapy ( eg , a taxane , 24 as used in head and neck cancer ) , the integration of biological agents ( eg , an egfr inhibitor25 ) , or dose - escalation above 504 gy enabled by intensity - modulated radiotherapy , which should be tested in appropriately designed clinical trials . intensiveness of our study has several limitations . 
we did not collect quality - of - life data ( patient - reported outcomes ) to investigate the pattern and severity of late radiotherapy - related toxic e ects . 
because of the the chemoradiation , maintenance treatment was di cult to deliver at full doses because of cumulative toxicity and low compliance , although most dose reductions were according to protocol . 
additionally , 41 maintenance patients chose not to start treatment and investigators might not have encouraged full complianceespecially at the start of the trialsince the e ectiveness of maintenance treatments is unproven . 
finally , panel : research in context systematic review we searched pubmed , medline , and cancerlit and abstracts of asco / astro / estro meetings with the terms anal cancer , squamous cell carcinoma , complete clinical response , local recurrence , survival , concurrent , chemotherapy , cisplatin , mitomycin c , radiotherapy , chemoradiation , radiochemotherapy , and combined modality . 
we found two other phase 3 trials in progress testing additional neoadjuvant cisplatin - based chemotherapy ( accord 03 and rtog 9811 ) , 10 , 11 , 16 but found no studies testing additional maintenance chemotherapy . interpretation in our trial , uorouracil and cisplatin had the same e ect on complete response rate , progression - free survival , and colostomy - free survival compared with uorouracil and mitomycnor did we see any improvement in progressionfree survival when additional maintenance chemotherapy was used . 
the low dose of elective nodal irradiation and a continuous radiotherapy schedule might have contributed to the good long - term outcomes . in conclusion , large phase 3 trials of primary anal cancer are feasible , even though this disease is uncommon ( we recruited roughly 25% of the uk incident cases )  . 
neither of the two strategies investigatedchemo radiation with cisplatin , and further maintenance chemotherapy using uorouracil and cisplatinis more e ective than standard care with mitomycin for achieving complete response , progression - free survival , or overall survival . 
 con icts of interest we declare that we have no con icts of interest . acknowledgments preliminary results of this trial were presented at the american society of clinical oncology meeting chicago in 2009 . 
the trial management group when the trial was designed were : roger d james ( chairman ) , david cunningham , rob glynne - jones , jonathan ledermann , helen m meadows , john northover , david sebag - monte ore , and maurice slevdc receives funding from biomedical research centre at royal marsden hospital ( uk ) and institute of cancer research ( uk )  . 
 we thank all those who participated in this trial , clinicians , their sta and patients , neil balderson and susan wan for study coordination , allan hackshaw and mark jitlal for comments on the report , and rubina begum for data management . 
we also thank the independent data vol 14 may 2013 articles monitoring committee ( richard gray , adrian crellin , and john shepherd ) and the independent trial steering committee ( peter hoskin , nicholas reed , and john tidy )  . articles lancet oncol 2016 ; 17 : 120316 this online publication has been corrected . 
the systemic anti - cancer therapy ( sact ) dataset collated by public health england allows the assessment of factors a ecting 30 - day mortality in a national patient population . 
the aim of this rst study based on the sact dataset was to establish national 30 - day mortality benchmarks for breast and lung cancer patients receiving sact in england , and to start to identify where patient care could be improved . methods in this population - based study , we included all women with breast cancer and all men and women with lung cancer residing in england , who were 24 years or older and who started a cycle of sact in 2014 irrespective of the number of previous treatment cycles or programmes , and irrespective of their position within the disease trajectory . 
we did logistic regression analyses , adjusting for relevant factors , to examine whether patient , tumour , or treatment - related factors were associated with the risk of 30 - day mortality . 
for each cancer type and intent , we calculated 30 - day mortality rates and patient volume at the hospital trust level , and contrasted these in a funnel plot . findings between jan 1 , and dec , 31 , 2014 , we included 23 228 patients with breast cancer and 9634 patients with non - small cell lung cancer ( nsclc ) in our regression and trust - level analyses . 
30 - day mortality increased with age for both patients with breast cancer and patients with nsclc treated with curative intent , and decreased with age for patients receiving palliative sact ( breast curative : odds ratio [ or ] 1085 , 99% ci 10401132 ; p < 00001 ; nsclc curative : 1045 , 10131079 ; p = 000033 ; breast palliative : 0987 , 09770996 ; p = 000034 ; nsclc palliative : 0987 , 09760998 ; p = 00015 )  . 
30 - day mortality was also signi cantly higher for patients receiving their rst reported curative or palliative sact versus those who received sact previously ( breast palliative : or 2326 99% ci 16343312 ; p < 00001 ; nsclc curative : 3371 , 15547316 ; p < 00001 ; nsclc palliative : 2667 , 21093373 ; p < 00001 ) , and for patients with worse general wellbeing ( performance status 24 ) versus those who were generally well ( breast curative : 6057 , 133327513 ; p = 00021 ; breast palliative : 6241 , 41809319 ; p < 00001 ; nsclc palliative : 3384 , 22765032 ; p < 00001 )  . 
we identi ed trusts with mortality rates in excess of the 95% control limits ; this included seven for curative breast cancer , four for palliative breast cancer , ve for curative nsclc , and seven for palliative nsclc . interpretation our ndings show that several factors a ect the risk of early mortality of breast and lung cancer patients in england and that some groups are at a substantially increased risk of 30 - day mortality . 
furthermore , our results highlight the importance of collecting routine data beyond clinical trials to better understand the factors placing patients at higher risk of 30 - day mortality , and ultimately improve clinical decision making . 
they can also be given for palliative purposes , to improve the quality of life for patients with advanced incurable cancers for as long as possible by controlling cancer growth and providing vol 17 september 2016 1203 articles research in context evidence before this study we searched pubmed for articles published up to feb 29 , 2016 , reporting on 30 - day mortality after chemotherapy for breast and lung cancer . 
we also consulted leading clinicians in this specialty for relevant , recent published work . we identi ed four studies investigating the factors associated with high 30 - day mortality following anticancer treatment in patients with a range of cancers including breast and lung , and two recent clinical trials that reported on 30 - day mortality after treatment with current standard treatments for breast and lung cancer . the four studies identi ed were all regional rather than national , and the clinical trials were done in selected groups of patients ( restricted to certain age and performance status ranges or with limited comorbidities ) so the results do not necessarily apply to the national cancer patient population in england . 
we also identi ed previous published work that showed variation in 30 - day postoperative mortality between trusts using funnel plots . added value of this study this study reports on patient , tumour - related , and treatment - related factors associated with 30 - day mortality after systemic anticancer treatment . 
we studied the diverse populations of patients with breast and lung cancer in england throughout 2014 using data from the newly available systemic anti - cancer therapy ( sact ) dataset . 
to our knowledge , this is the rst time this topic has been investigated at a national level . implications of all the available evidence this study shows that the sact dataset provides insight into the factors a ecting early mortality of patients in england . 
 it suggests that treatment intent ( curative or palliative ) , age , performance status , whether patients had received sact before the qualifying treatment used for this study , and sex and stage ( lung cancer only ) all a ect the 30 - day mortality risk . 
for some patients , this approach might also increase survival time . patients dying within 30 days after beginning treatment with sact are unlikely to have gained the survival or palliative bene ts of the treatment , and in view of the side - e ects sometimes caused by sact , are more likely to have su ered harin particular , the risk of neutropenic sepsis ( infection resulting from low blood neutrophil count , probably the most important cause of sact - related death ) is highest in the 30 days after sact , peaking at around 1115 days after treatment.5 sact cycles are typically 21 or , less commonly , 28 days long , so death from neutropenic sepsis from the previous treatment is captured within the 30 - day mortality metric . 
simply reducing doses of or avoiding sact altogether would reduce or eliminate instances of treatment - related early mortality , but at the cost of some patients being denied e ective sact and hence the survival and palliation bene ts . to maximise the bene ts of sacts it is therefore important to gain a more detailed understanding of how the many di erent patient and tumour characteristics can predict patient outcomes , such as the risk of early mortality . 
only a small number of local observational studies have assessed 30 - day mortality after sact , but each has pointed to areas in which patient care could be improved.58 treatment - related early mortality is also commonly measured in clinical trials of sact , but , by necessity , patient cohorts are often selected on the basis of protocoldriven inclusion criteriaeg , within a certain age range , good performance status , or limited comorbidities.9 , 10 the ndings from these trials are therefore less reliable estimates of treatment - related early mortality in the groups not included from the general cancer patient population . 
 there is thus a clear need to make use of population - based data to establish 30 - day mortality benchmarks for the full range of patient types , to investigate how patient and treatment - related factors a ect the risk of 30 - day mortality , and to identify di erences between provider trusts to help improve clinical outcomes . here we examine factors that a ect the risk of 30 - day mortality in patients with breast and lung cancer in 2014 using data collected from nhs hospital trusts across england in the sact dataset . 
 we additionally characterised the extent of variation in 30 - day mortality rates between hospital trusts england , and identi ed those with signi cantly higher 30 - day mortality rates . 
this is the rst time , to our knowledge , that 30 - day mortality following recently reported sact has been investigated on a large scale in a population that re ects the real diversity of patients with breast and lung cancer being treated in the national health service ( nhs ) in england . 1204 vol 17 september 2016 articles see online for appendix methods study design and data this population - based , observational study11 included all breast and lung cancer patients aged 24 years and older reported to have received sact in england between jan 1 , and dec 31 , 2014 , according to the sact dataset , irrespective of the number of previous treatment cycles or programmes , and irrespective of their position within the disease trajectory . 
 the sact dataset is a new resource at public health england , which started a phased implementation in 2012 , and which collects information reported routinely by nhs hospital trusts about the treatment of cancer in england12 in four key areas : patient and tumour characteristics including age , sex , morphology , and performance status ; hospital and consultant details , including general medical council ( gmc ) number ; treatment characteristics including drug names and drug combinations ( regimens ) ; and outcome elds including date of most recent treatment and date of death ( when applicable )  . the appendix provides the full data standard , including a description of all 43 items recorded , with data eld formats as described in the nhs data dictionary13 ( appendix p 1 )  . 
these are primary patient and hospital trust identi ers ( nhs number , birth date , postcode , sact provider organisation code ) and key treatment details ( sact regimen name , regimen start date , and cycle number )  . phased introduction of data entry started in april , 2012 . 
by january , 2014 , 141 ( 95% ) of 148 trusts were routinely submitting at least the mandatory data items ; because of trust mergers , the total number of trusts expected reduced to 147 by july 2014 . 
we selected a reporting period of january to december , 2014 , because this was the most complete calendar year of data that was available at the time this analysis was completed.14 this reporting period also allowed linkage with the english national cancer registration and analysis service ( ncras ) , which improved data completeness when morphology , stage at diagnosis , and dates of death were missing from the sact dataset . treatment and patients we de ned sact as any cytotoxic chemotherapy , active anticancer therapies such as monoclonal antibodies ( eg , trastuzumab ) , and targeted biological treatments such as egfr tyrosine kinase inhibitors . 
 we did not distinguish between patients receiving combined chemo - radiotherapy and those receiving chemotherapy only , as this was poorly recorded in the sact dataset at this stage . we examined data for breast and lung cancer patients ( identi ed by the clinical codes in panel 1 ) because both had good data completeness in the sact dataset ; in 2014 , data had been submitted for 18 976 ( 94% ) of 20 265 patients with breast cancer and 13 405 ( 92% ) of 14 527 patients with lung cancer who were reported to have commenced chemotherapy.13 we provide descriptive statistics on small cell lung cancer ( sclc ) and non - small cell lung cancer ( nsclc ) separately , based on morphology data ( supplemented from cancer registry data where missing from the sact dataset ) because these cancer types generally require di erent treatment strategies . 
we excluded from our regression analysis all patients for whom the start date of their last reported cycle of sact was not reported because this precluded an assessment of 30 - day mortality . outcomes of the patients with breast or lung cancer reported to have received sact in england between jan 1 , 2014 , and dec 31 , 2014 , we identi ed those that died within 30 days of sact ( from all causes , including iatrogenic deaths or those due to disease progression ) by calculating the time between the start date of the most recently reported sact cycle in 2014 and , when relevant , the date of death for each patient . 
 from this , we calculated a national 30 - day mortality rate by dividing the number of patients that received sact within 30 days of their death by the total number of patients that received sact in the reporting period . 
we mainly used the date of death as reported for a patient through sact dataset returns , but when that was unavailable , we extracted it from records in the ncras . 
all patients were traced through the nhs demographics services using matched identi ers ( including nhs number , date of birth , and sex )  . there were 22 deaths for patients with breast cancer and 35 deaths for patients with lung cancer that were only recorded in ncras , not the sact dataset or the nhs demographics service . 
 608 patients with breast cancer and 732 patients with nsclc had con icting dates of death recorded in the sact versus ncras datasets ; this resulted in a con ict about 30 - day mortality status ( records agged as death within 30 days in one source but not the other ) for 16 patients with breast cancer and 20 with nsclc . for 26 patients who died within 30 days of receiving sact , death certi cate data could not be found . 
 one patient with lung cancer in the 30 - day mortality group had a di erent date of birth recorded in the cancer registry , so we used their date of birth recorded in the sact dataset . 
for all other patients , nhs number , date of birth , and sex were identical in both databases . some trusts reported a high proportion of patients as having received only the rst cycle of sact : 13 trusts that treated 574 patients with breast cancer , and 14 trusts that treated 302 patients with lung cancer , had a very high proportion ( > 80% ) of patients for whom only the rst cycle of sact was reported . 
 * these total numbers are patients treated with curative and palliative intents only , and do not include those for whom treatment intent was unknown . table 1 : patterns of missing values in the sact dataset for ps , stage , and bmi for all patients with breast or nsclc these patients might have had subsequent cycles of chemotherapy that were not recorded in the sact dataset . statistical analysis and explanatory variables we examined the association of age , performance status , income deprivation , whether patients had received previous sact ( as recorded in the sact dataset ) , and bmi with 30 - day mortality after sact for breast and nsclc patients . 
these variables are linked to patient care in a clinical setting in relation to sact treatment ; income deprivation , while not directly linked to patient care , re ects other factors that arefor example , those in low - income areas might be more likely to smoke and have higher levels of comorbidity . we also examined the association of sex and cancer stage at diagnosis with 30 - day mortality for nsclc patients only . 
we also did not examine the association of cancer stage at diagnosis with 30 - day mortality for breast cancer because there can be a substantial time interval between diagnosis and sact treatment for many breast cancer patients ( eg , patients who relapse with metastatic disease several years after the initial diagnosis ) , making this indicator less clinically relevant than for lung cancer . income deprivation was not reported directly by nhs hospital trusts in the sact dataset . 
instead , we used patient postcodes , as reported in the dataset , to derive each patients income deprivation score from the english indices of deprivation 2010 , 15 and assigned patients into ve groups from least ( group 1 ) to most ( group 5 ) income deprived . 
we chose income deprivation over health - related indices , which would have been interrelated with our 30 - day mortality outcome measure . the dataset this measure : there were missing values for performance status and bmi for patients with breast cancer or nsclc , and stage for nsclc ( table 1 )  . 
 inspection of the data showed that for performance status , this was mainly the result of a few trusts not reporting trusts reported no performance status data , one of which was a large trust , and 12 trusts had 10% or less completion of performance status data . 
we assumed data were missing completely at random ( mcar ) at the patient level because we found no evidence to the contrary , and these trusts provided care for a range of patients . four height and weight data ( used to calculate bmi ) are likely to be recorded for patients receiving less treatments with a xed dose ; however , many patients included in our study received treatments that were dosed according to body surface area or weight , some of whom also had missing height and weight data , which probably obscures this association between bmi and 1206 vol 17 september 2016 articles treatment regimen . 
additionally , some trusts with low patient volumes ( < 400 patients ) reported no height or weight data , giving some evidence for an association between bmi and treating trust , although this link is probably weak . data for stage at diagnosis were more complete : stage was reported for 10 408 ( 93% ) of 11 199 patients with lung cancer and 13 883 ( 89% ) of 15 626 patients with curative breast cancer , compared with 4159 ( 55% ) of 7602 patients with palliative breast cancer , suggesting that stage at diagnosis data were more likely to be reported when patients had a smaller time interval between diagnosis and last reported treatment . 
most patients with breast cancer receiving palliative treatment are likely to be stage iv ( the most advanced stage ) ; therefore , clinicians might be less likely to record stage at diagnosis for these patients because it is assumed to be stage iv . 
thus , there was evidence of an association between stage at diagnosis and treatment intent . because we assumed that performance status was mcar , and that bmi and stage seemed to be only weakly related to treatment regimen and intent , respectively , we hypothesised that there would be no variables upon which we could base multiple imputation . 
we tested this by attempting multiple imputation16 using the ice command in stata , based on variables of age , sex , intent of treatment , patients not having received any previous sact as recorded in the dataset from 201214 ( treatment naive ) , regimen , income deprivation group , cancer type ( breast or lung cancer ) , treating trust , and death within 30 days . we used a train - test approach to assess the accuracy of this imputed data , whereby from all known data , we used the multiple imputation algorithm to estimate 1% , 5% , 10% , and 20% of the data in multiple tests . 
these unknown categories were also used for risk adjustment in the funnel plot . regression analysis and risk - adjustment we used logistic regression analysis to assess any associations between the explanatory variables and 30 - day mortality . 
we present the results of these logistic regression analyses as adjusted odds ratios ( or ) that re ect the e ect of each variable in our multivariable regression model , alongside the unadjusted or and proportion of patients with 30 - day mortality . 
for each model , the mean variance in ation factor was lower than 104 , which suggests that there were no issues with co - linearity between model terms . we plotted the errors of the residuals in the model , which showed that the variables in our model were equally variable and indicated that the assumptions of our regression model were valid . 
 in addition to testing the main e ects presented here , we tested models with interactions modelled between age and performance status , age and bmi , and for nsclc only , sex and performance status , and sex and bmi . 
in each case , the model t was inferior . analyses were completed separately by cancer type ( breast or nsclc ) further separated by treatment intent ( curative or palliative ) in four regression analyses . 
in this rst analysis of the sact dataset , we did not do separate regression analyses for each mode of treatment we included as curative ( panel 2 ) , because this would have resulted in smaller group sizes and thus lower statistical power . we compared 30 - day mortality rates between the following groups for age , performance status , income deprivations , previous sact treatment , bmi , sex ( nsclc ) , and tumour stage at diagnosis ( nsclc )  . 
 for performance status , we recorded patients as ps 0 ( asymptomatic ) , ps 1 ( symptomatic , still able to carry out light activities ) , ps 24 ( symptomatic patients requiring any amount of bed rest during the day , or who were completely bed bound , grouped together because of small patient numbers ) , and performance status not recorded . 
for income deprivation , we compared patients panel 2 : typical de nitions of curative and palliative intent used in this study , as recorded by trusts in electronic prescribing systems curative modes of treatment 1 adjuvant : given after surgery to reduce the chance of the cancer spreading or coming back 2 neoadjuvant : given before surgery to shrink a tumour and make surgery possible or less dis guring 3 curative : given alone without other forms of treatment to try to cure the cancer completely palliative modes of treatment 1 palliative : given to maintain or improve the quality of life for patients with advanced incurable cancer for as long as possible , by controlling the growth of a cancer and providing symptom relief vol 17 september 2016 1207 articles patients receiving sact in 2014 29 112 women with breast cancer 15 545 patients with lung cancer 30 - day mortality patients dying within 30 days of most recently recorded cycle of sact in 2014 still alive > 30 days patients alive for 31 or more days after most recently recorded cycle of sact in 2014 700 women with breast cancer 1274 patients with lung cancer 867 patients with nsclc 27 664 patients with breast cancer 13 771 patients with lung cancer 10 332 patients with nsclc excluded patients for whom no sact cycle start date was present 748 patients with breast cancer 500 patients with lung cancer * figure 1 : study pro le for our analyses in this report nsclc = non - small cell lung cancer . 
 * the number of excluded patients with nsclc is not shown here , as the excluded patient group was not traced in the national cancer registration and analysis service for additional morphology data . breast , curative breast , palliative breast , not recorded total patients 30 - day mortality 15 626 / 28 364 ( 55% ) 41 ( < 1% ) 7602 / 28 364 ( 27% ) 5136 / 28 364 ( 18% ) breast , all intents combined 28 364 ( 100% ) lung ( all subtypes ) , curative lung ( all subtypes ) , palliative 2429 / 15 045 ( 16% ) 10 587 / 15 045 ( 70% ) lung ( all subtypes ) , not recorded 2029 / 15 045 ( 14% ) lung ( all subtypes ) , all intents combined 15 045 ( 100% ) data are n ( % ) of total patients by cancer type and treatment intent ; and n ( % ) of deaths occurring within 30 days of systemic anticancer therapy for each of those groups . 
sclc = small cell lung cancer . table 3 : 30 - day mortality rates in patients with lung cancer by morphology and treatment intent in income domain group 3 ( the middle level of socioeconomic deprivation based on household income ) with those in group 1 ( least deprived ) , 2 , 4 , and 5 ( most deprived )  . 
for previous sact treatment , we compared patients for whom one or more previous systemic anticancer treatments were recorded in the sact dataset before the qualifying treatment used in this study with patients for whom no previous systemic anticancer treatments were recorded in any year ( 201214 ) of the database ( treatment naive )  . 
for bmi , we compared patients with bmi scores in the healthy weight range ( bmi 185 to < 25 kg / m ) with those in the underweight range ( bmi < 185 kg / m ) , overweight ( bmi 25 to < 30 kg / m ) , and obese categories ( bmi > 30 kg / m ) , and those for whom bmi information was not recorded . 
the factors included in the risk adjustment were the same as those detailed for the logistic regression analyses ( eg , age , perfor mance status , bmi , and stage at diagnosis )  . as noted in the methods for multiple imputation , the large number of missing values for performance status were a result of a small number of trusts not providing any performance status information . 
we used the risk - adjusted mortality rate to create funnel plots using the funnelcompar command in stata , which gave the 95% and 998% control limits ( dashed lines on the graphs ) and the national risk - adjusted 30 - day mortality rate ( the horizontal line on each graph )  . role of the funding source there was no funding source for this study . 
the corresponding author had full access to all aggregated data and analyses and the nal responsibility to submit for publication . results of the patients in the sact database , 748 ( 3% ) of 29 112 patients with breast cancer and 500 ( 3% ) of 15 545 patients with lung cancer receiving sact were excluded from the analysis due to missing cycle start dates . 
treatment intent was not recorded for 5136 ( 18% ) of 28 364 patients with breast cancer and 2029 ( 14% ) of 15 045 patients with lung cancer ; these patients were excluded from the regression and trust - level analyses . 
because of lower patient numbers for sclc ( n = 3352 ) , we only did the regression and trust - level analyses for patients with nsclc ( 11 199 patients including those for whom treatment intent was not recorded )  . 
in view of the exclusions , the 1208 vol 17 september 2016 articles nal cohort for regression and trust - level analyses included 23 228 patients with breast cancer and 9634 patients with nsclc . the median patient age was 54 years ( iqr 4764 ) for patients with breast cancer treated with curative intent ; 61 years ( 5170 ) for patients with palliative breast cancer ; 67 years ( 6173 ) for patients with nsclc treated with curative intent ; and 68 years ( 6174 ) for patients with nsclc treated with palliative intent . 
the appendix shows the distribution of age , performance status , income deprivation , and bmi by age for patients with breast and nsclc treated with curative and palliative intent ( appendix pp 24 )  . data for performance status , a measure of patients level of cancer symptoms and general wellbeing , 20 was not reported for 6919 ( 30% ) of 23 228 patients with breast cancer and 2968 ( 31% ) of 9634 patients with nsclc , for whom treatment intent was recorded . 
a further 2139 ( 42% ) of 5136 patients with breast cancer and 530 ( 34% ) of 1565 patients with nsclc , were missing both performance status and treatment intent . overall , 30 - day mortality was higher for patients with lung cancer ( 1274 / 15 045 [ 9% ] ; table 2 ) than patients with breast cancer ( 700 / 28 364 [ 3% ] ; table 2 ) , and in each treatment intent category ( curative , palliative , and unknown ; table 2 )  . 
30 - day mortality was lowest for patients with breast or lung cancer receiving systemic anticancer therapy for curative rather than for palliative purposes : 41 / 15 626 ( < 1% ) versus 569 / 7602 ( 8% ) for breast cancer , and 70 / 2429 ( 3% ) versus 1061 / 10 587 ( 10% ) for lung cancer ( table 2 )  . 
for the remaining 105 ( 8% ) of patients , most death certi cates mentioned cancer . table 4 and the appendix ( p 4 ) show all results of the regression analysis for patients with breast cancer treated with curative intent . 
30 - day mortality was also higher for patients with ps 24 compared with those with ps 0 , though con dence intervals were large ( or 6057 , 99% ci 133327513 ; p = 00021 )  . table 5 and the appendix ( p 5 ) show results of the regression analysis for patients with breast cancer treated with palliative intent . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of breast cancer patients receiving curative sact who had 30 - day mortality . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of patients with breast cancer receiving palliative sact who had 30 - day mortality . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of patients with nsclc receiving curative sact who had 30 - day mortality . 
patients for whom performance status was not recorded also had a higher 30 - day mortality than those with ps 0 ( 2719 , 18883918 ; p < 00001 )  . 
 treatment - naive patients receiving palliative treatment had a signi cantly higher 30 - day mortality than those for whom previous sacts are recorded in the dataset between 2012 and 2014 ( or 2326 , 99% ci 16343312 ; p < 00001 )  . table 6 and the appendix ( p 6 ) show results of the regression analysis for patients with nsclc treated with curative intent . 
as with patients with breast cancer , 30 - day mortality signi cantly increased with age for patients with nsclc treated with curative intent ( or 1045 , 99% ci 10131079 ; p < 000033 )  . 
treatment - naive patients had signi cantly higher 30 - day mortality than those for whom previous systemic anticancer treatments were recorded in the dataset between 2012 and 2014 ( or 3371 , 99% ci 15547316 ; p = 000033 )  . table 7 and the appendix ( p 7 ) show results of the regression analysis for patients with nsclc treated with palliative intent . 
as for breast cancer patients , 30 - day mortality decreased with age for patients with nsclc treated with palliative intent ( or 0987 , 99% ci 09760998 ; p = 00015 )  . 
treatment - naive patients had signi cantly higher 30 - day mortality than those for whom previous sact was recorded in the dataset between 2012 and 2014 ( or 2667 , 99% ci 21093373 ; p < 00001 )  . 
30 - day mortality was also signi cantly higher for patients with stage iv ( advanced ) than stage iii tumours ( or 1438 , 95% ci 10991883 ; p = 000051 )  . figures 25 show risk - adjusted funnel plots for di erent modalities of treatment and cancer type , by hospital trust . 
this included seven trusts for breast curative , four for breast palliative , ve for nsclc curative , and seven for nsclc palliative . discussion in our population - based study of english breast and lung cancer patients , 30 - day mortality increased with age for both patients with breast cancer or nsclc receiving curative sact , and decreased with age for patients receiving palliative sact . 
patients with breast cancer or nsclc with worse general wellbeing ( indicated by higher ps scores ) had higher 30 - day mortality than those who were generally well ( ps 0 ) , and 30 - day mortality was also higher for treatment - naive patients than those who had any previously recorded cycles of sact between 2012 and 2014 . 
individual trust data will be discussed in a public health england report . to our knowledge , this is the rst time these benchmarks in 30 - day mortality after sact have been established on a national basis . 
the 2011 national cancer strategy for england proposed 30 - day mortality as a potential national clinical indicator of avoidable harm from sact21 and it has been used as a clinically relevant indicator for sact in previously published work.5 these benchmarks can provide a better understanding of the patient characteristics associated with increased 30 - day mortality and start improved clinical treatment decision making and identify those hospital trusts where clinical practice and data management should be reviewed . to support a particular strength of 30 - day mortality as an outcome measure is that it avoids issues with the details and coding of causes of death on death certi cates . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of patients with nsclc receiving palliative sact who had 30 - day mortality . 
 table 7 : regression analysis results showing 30 - day mortality for patients with nsclc treated with palliative intent by age , ps , id , previous sact ( previously treated or treatment naive ) , bmi , sex , and cancer stage nearly all patients in our study , including those dying within 30 days of receiving sact . 
however , we know that patients who die within 30 days of receiving sact are very unlikely to receive any bene t from it irrespective of what their cause of death was . 
it is therefore not necessary to know whether death was caused by side - e ects from treatment , cancer progression , or any other causes to examine factors that increase the risk of experiencing net harm rather than net bene t from receiving sact . the large cohort of breast and lung cancer patients included in the sact dataset gives con dence that the associations we recorded between a number of variables and higher early mortality in england are real , despite some issues with data completeness , which we expect to improve in subsequent years of data collection . the large , signi cant increase in 30 - day mortality for treatment - naive patients suggests that particular care and an emphasis on the early reporting of toxic e ects should be undertaken in patients who are sact treatment naive . 
this approach is consistent with ndings of a previous study of the toxic e ects from lung cancer treatment.22 to our knowledge there are no previous studies of treatment - naive status in this context , so we are unable to identify the reasons behind the increased 30 - day mortality for these patients . there our identi cation of treatment - naive patients relied on treatment records taken from the sact dataset alone and there are two known data issues reducing the accuracy of this grouping . 
the database was only implemented in 2012 and made mandatory in april , 2014 , so data for previous sact treatments might be missing for some patients ( eg , those who received a previous issue will be most treatment before 2012 )  . 
 additionally , the challenge of some trusts only recording patients rst cycle of sact means we might be underestimating early mortality from sact and overestimating increased risk associated with the treatment - naive patients . 
as data completeness improves in subsequent years , a clearer understanding of the association between treatment - naive status and 30 - day mortality will be possible . is a 30 - day mortality increased with age for patients with breast cancer and nsclc treated with curative intent , figure 2 : funnel plot of variation in risk - adjusted 30 - day mortality in patients with breast cancer given systemic anticancer therapy with curative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . female male stage i stage ii stage iii stage iv vol 17 september 2016 1211 1000 1100 1200 number of patients receiving chemotherapy ( 2014 ) articles number of patients receiving chemotherapy ( 2014 ) figure 3 : funnel plot of variation in risk - adjusted 30 - day mortality in patients with breast cancer given systemic anticancer therapy with palliative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . the nding that 30 - day mortality increased with worsening performance status for patients with breast cancer or nsclc treated with palliative intent could be because patients with poorer general health are less able to tolerate the negative side - e ects of sact compared with healthier individuals , to an extent where the toxic e ects outweigh the bene cial e ects.5 these ndings suggest great care is required when advising chemotherapy in this patient group . we noted that 30 - day mortality was signi cantly higher for patients with breast cancer or nsclc receiving palliative sact for whom performance status was not recorded compared with those with ps 0 . 
this result might be because ps 0 is relatively easy to de ne , but it might be more di cult for clinicians to score the extent of reduced wellbeing . our nding that 30 - day mortality was lower in women with lung cancer than in men with lung cancer given palliative sact was expected . 
previous data suggest that women with lung cancer are generally diagnosed at an earlier age , with a more localised cancer , and have better survival.20 however , to our knowledge there have been no speci c investigations of early mortality in this context prior to our study , so we are unable at this stage to suggest why sex a ects 30 - day mortality risk in particular . 
 the increased 30 - day mortality for nsclc patients receiving palliative sact who had advanced cancers was also expected because these patients are typically less well ; although again , no previous studies have , to our knowledge , investigated the e ect of cancer stage on early mortality speci cally . the nding that overweight nsclc patients treated with palliative intent had a reduced 30 - day mortality compared with those in the healthy bmi group could be explained by dose - limitation practices . 
chemotherapy doses are calculated according to patient height and weight , but smaller doses than this are often given to patients with higher bmi.24 , 25 these practices might reduce short - term mortality in overweight patients . 
 however , long - term survival might be lower for these patients than those with a healthy bmi if the administered dose is not high enough to e ectively reduce tumour growth and spread . 
research into whether there are longer - term survival di erences between overweight and healthy weight patients could help to elucidate whether there is a problem with under - dosing for larger patients . 
 weight loss is an adverse prognostic factor in lung cancer26 and could explain this trend , though the di erence recorded was non - signi cant . the relative risk of overall mortality in obese and overweight patients with breast cancer is increased compared with healthy weight individuals , 27 which number of patients receiving chemotherapy ( 2014 ) figure 4 : funnel plot showing variation in risk - adjusted 30 - day mortality in patients with non - small cell lung cancer given systemic anticancer therapy with curative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . perhaps because older patients are generally more frail and less able to tolerate sact than are younger patients . 
 conversely , 30 - day mortality decreased with age for patients with breast cancer and nsclc treated with palliative intent , perhaps because older patients are less likely likely than younger patients to accept or be prescribed sact treatment that might extend their life in favour of other palliative care options to relieve pain or discomfort . 
alternatively younger patients might have more aggressive disease with a higher risk of noniatrogenic cancer mortality.23 1212 vol 17 september 2016 articles suggests that a high bmi itself does not generally confer a signi cant biological protective e ect against mortality . 
if the e ects we recorded are due to dose - limitation or patient weight loss , an association between bmi and 30 - day mortality will probably be noted for other cancer types in future reports on the sact dataset . for patients with nsclc treated palliatively with no recorded bmi , 30 - day mortality was signi cantly lower than for those with a healthy bmi , but this reduction in risk was smaller than for overweight and obese patients , suggesting the bmi unknown group is probably mainly a mix of healthy weight and overweight patients . 
as data completeness improves , we will better understand the distribution of bmi scores amongst patients receiving sact , and obtain improved estimates of 30 - day mortality for each bmi group . although we identi ed several factors a ecting 30 - day mortality risk , our population - based dataset included only patients that received sact , so we cannot con rm whether patients would have had better outcomes if they had not received sact . 
through more sophisticated links with audit data and other data sources in future , we intend to investigate treatment rates alongside mortality by trust , which would provide some information about outcomes for these patient groups . 
this cohort represents a large proportion of number of patients receiving chemotherapy ( 2014 ) figure 5 : funnel plot showing variation in risk - adjusted 30 - day mortality in patients with non - small cell lung cancer given systemic anticancer therapy with palliative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . patients with breast cancer with higher mortality than is typically reported in clinical trials : 26% of patients with breast cancer diagnosed in england in 2013 were older than 60 years , with incidence peaking between the ages of 65 and 69 years.29 this might be because clinical trials typically recruit a tter cohort of patients with a lower disease burden and better performance status than the overall patient population receiving treatment to clearly determine the e ects of the interventions under investigation , and to ensure older and less well patients are not put at risk . 
patients in trials also tend to receive more intensive support and follow up . therefore , our analysis highlights the value of investigating sact treatment outcomes on a national scale , and shows that ndings of clinical trials in selected age cohorts cannot readily be generalised to all patients . 
lung cancer often occurs in patients with signi cant smoking - related comorbidities , which are likely to increase the risk of 30 - day mortality , 6 although lack of available comorbidity data meant that we could not account for them in these analyses . 
future analyses will pool data for multiple years ( as it becomes available ) to provide su ciently large patient cohorts to examine the impact of patient and disease characteristics on 30 - day mortality from sclc . the we predicted higher 30 - day mortality for patients receiving palliative sact because these patients are not expected to recover from their cancer and the burden of vol 17 september 2016 1213 articles disease is generally high . 
however , it remains important to weigh up the important bene ts some patients receive from palliative treatment with emerging evidence suggesting that patients prescribed chemotherapy at the end of life overall experience a net reduction in their quality of life.30 , 31 patient choice is an important factor in these decisions ; previous ndings showed that patients with cancer were much more likely to accept intensive sact treatment with only a small chance of bene t compared with doctors and nurses.32 to help clinicians and patients to make treatment decisions that are most likely to produce the desired outcomes , we must understand the factors a ecting the balance between bene ts and harms of palliative sact , which we have started to investigate here . 
these factors should be a focus of discussions about treatment between patients and their clinicians to allow better informed decisions and improved outcomes . in future studies based on the sact dataset , we hope to examine di erences in the factors a ecting 30 - day mortality between subcategories of patients that received curative sact ( adjuvant , neoadjuvant , and curative ) , which we were unable to do in this initial analysis due to insu cient patient numbers in each sub - category . 
 this analysis will be possible once data on more patients become available in subsequent years . we also identi ed several trusts with signi cantly higher levels of 30 - day mortality . 
we have written to all trusts to inform them of their 30 - day mortality rates , and have speci cally encouraged outlier trusts to review both their clinical practice and also their data management systems . 
 analogously , simply because a hospital trust fell within the control limits of the funnel plots , it does not guarantee that each patient received optimal treatment , as data issues may be obscuring instances of suboptimal clinical decision making . 
it is also possible that hospitals with signi cantly lower 30 - day mortality rates are not tolerating any risk and are treating only the ttest patients , which may have the unintended consequence of not treating patients who could have potentially bene ted from receiving sact . 
more comprehensive case mix adjustment and better data completeness will , in time , allow national datasets such as the sact dataset to be used as a performance management tool . although we have made some important insights into 30 - day mortality using the sact dataset , some limitations and gaps in reporting still remathe sact dataset uses only routinely reported data with no clinical note or pro - forma review . 
therefore , the dataset does not include items such as laboratory indicator test resultseg , for liver and renal function , so we are unable to analyse any association between these indicators and 30 - day mortality , or use them in risk adjustment models . at this stage , we did not assess whether drug dosage was appropriate , and whether this was associated with 30 - day mortality because this was beyond the scope of our rst report . 
however , analyses of these data in future reports would be valuable , for example in assessing whether sact regimens are both clinically e ective and cost - e ective . 
subsequently , some of those patients probably received subsequent cycles that were not recorded in the dataset , whose absence from the sact dataset would arti cially increase the time between cycle start date and date of death , and lower 30 - day mortality . 
 this omission might also arti cially increase the risk of 30 - day mortality associated with being treatment naive , because later cycles of sact , and therefore any deaths within 30 days of those later cycles , were not recorded . 
 issues with missing data will be resolved through improvements in sact data reporting by trusts through e - prescribing systems in subsequent years . compared with the national cancer waiting times database , the sact dataset captured 94% and 92% of patients with breast and lung cancer , respectively , reported to have received sact in 2014.13 3% of both patients with breast cancer and with lung cancer receiving sact were also excluded from the analyses in this report due to missing cycle start dates . 
some of these missing data could be due to delayed or phased reporting because the dataset was only mandated from april , 2014 ( the proportion of trusts reporting on at least the mandatory data elds was 141 [ 95% ] of 148 in january , 2014 , but 147 [ 100% ] of 147 by july )  . some nhs trusts reported incorrect names for the combinations of sacts ( regimens ) given to some con rmed breast and lung cancer patients included in our analyses , which highlights the need for trusts to improve the quality of their regimen data reporting . 
this error could be because sact is recorded some time before its administration , and the record might not be updated if treatment is delayed or omitted , which is likely to falsely increase 30 - day mortality . we acknowledge that performance status might not have accurately re ected comorbidity status , which can be associated with socioeconomic deprivation ( eg , through a higher prevalence of smoking amongst more socioeconomically deprived patients ) , which might a ect whether these patients receive sact . 
therefore , improved data collection on comorbidity status would the association between enable us socioeconomic deprivation and 30 - day mortality more thoroughly in future . investigate for the rst time to our knowledge , our analysis of the for linkage and mortality sact dataset morphology , at diagnosis , the ncras ( with stage 1214 vol 17 september 2016 articles information ) gives us important insights into 30 - day mortality in a large , representative population of patients with breast or lung cancer receiving systemic anticancer therapy in england . 
our data suggest that treatment intent , patient age , performance status , whether patients had received previous systemic anticancer treatments , and sex all a ect 30 - day mortality risk in this context . 
some patients may not have bene ted from decisions to give sact ; accurate and complete reporting of sact data on a national scale is therefore crucial to provide real world information to support clinicians with decision making on treatment , complementing evidence from clinical trial data . contributors dd , mwa , mp , and sm led on study design and concept . 
dd , mwa , mp , sm as well as ebs , mb , rs , mwi , jr , dc , jd , dt , tp , and cw all actively and substantially contributed to the writing of this manuscript , performing literature searches , interpreting data and providing comment on multiple iterations of the manuscript . declaration of interests dd reports that public health england ( phe ) provided funding for the project team and are preparing a report on the subject of 30 - day mortality in england ( 2014 ) for publication . 
mp reports personal fees from roche pharmaceuticals ltd , personal fees from pierre fabre oncology ltd , personal fees from eli lilly , personal fees from astrazeneca , grants from msd , outside the submitted work . 
we thank the following colleagues for constructive comments and helpful discussions during the analysis of the data and drafting of this report : sara hiom ( cancer research uk ) , members from the chemotherapy clinical information and lung cancer site speci c clinical reference groups at phe , particularly michael lind , and eva morris ( university of leeds )  . 
 corrections correction to lancet oncol 2015 ; 16 : 522 correction to lancet oncol 2016 ; 17 : 553 correction to lancet oncol 2016 ; 17 : 733 philip , pa . 
 this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . eggermont amm , chiarion - sileni v , grob j - j , et al . 
this correction has been made to the online version as of june 1 , 2016 . correction to lancet oncol 2016 ; 17 : 751 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . vol 17 june 2016 e223 re ection and reaction causation of pathophysiological changes that ultimately lead to cancer , h pylori is frequently not detectable at the time of neoplasia development.24 moreover , in a large proportion of patients with gastric cancer who were classi ed as h - pylori negative by use of routine elisa , past infection could be proved by analysis of antibodies to caga igg , which persist longer after loss of infection than do igg antibodies identi ed by conventional testing.3 , 4 di culties in the identi cation of past h - pylori infection frequently lead to an underestimation of the cancer risk attributable this bacterium.3 , 4 in 1994 , the international agency for research on cancer classi ed h pylori as a type 1 carcinogena de nite cause of human cancer.2 meimarakis and colleagues nding1 that infection with the carcinogenic bacterium is bene cial once cancer has developed seems paradoxical at rst , but might have a biological basis . 
however , the supporting evidence they provide is not convincing : the assumption that patients negative for h pylori have increased regulatory - t - cell responses in tumour tissue is biased by the use of ox40 ( tumour necrosis factor receptor superfamily member 4 ) as a mar ker of cd4 - positive , cd25positive regulatory t cells . 
although ox40 is expressed on regulatory t cells , it is not speci c for this cell type and is expressed by other types of lymphocytes such as activated type 1 and type 2 t - helper ( th ) cells.7 nevertheless , a model in which a microbe - induced immune response a ects tumour growth is plausible . 
 several physiological processes necessary for tumour devel opment , such as angiogenesis , cell survival , and tissue remodelling , are regulated by leucocytic in ltrates in the neoplastic environment , either directly or by secreted products . 
in stomach cancer , the extent of in ltration by cytotoxic t cells and natural - killer cells into the neoplasticcell nest is a signi cant predictor of patient survival.8 , 9 thus , microbe - induced in ammation might modulate antitumour immunity and a ect immune surveillance in the stomach or lymph nodes . 
this idea is consistent with the nding that h - pylori infection inhibits the progression of chemically induced gastric carcinogenesis in mice.10 vol 7 may 2006 more than 15% of all human cancer is thought to be caused by infections , some of which indirectly promote carcinogenesis through induction of chronic in ammatory states . 
in animal studies , an in ammatory response induced by h pylori is of fundamental importance for the development of bacteria - related gastric malig nant disease.11 in human beings , proin ammatory polymorphisms in cytokine genes strongly enhance cancer risk associated with h - pylori infection.12 however , once cancer has developed , persistent h - pylori infection and in ltration with some leucocyte subsets seem to correlate with a favourable prognosis . 
the results of meimarakis and colleagues1 re ect the clinical implications of this multifaceted and complex biology of infection and disease . * roland rad , christian prinz , roland m schmid 2nd department of internal medicine and gastroenterology , technical university of munich , ismaningerstr 22 , 81675 munich , germany roland.rad@lrz.tum.de we declare no con icts of interest . helicobacter pylori as a prognostic indicator after curative resection of gastric carcinoma : a prospective study . 
is helicobacter pylori infection a necessary condition for noncardia gastric cancer ? am j epidemiol 2004 ; 159 : 25258 . uemura n , okamoto s , yamamoto s , et al . 
lancet oncol 2006 ; 7 : 29596the fourth sentence in the third paragraph should have read : exposure to carbon - black particles occurs mainly in the form of aggregates ( ie , particle size , 50600 nm ) and agglomerates ( 27 m )  . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology correction to lancet oncol 2020 ; 21 : 50818 correction to lancet oncol 2020 ; 21 : 34142 pishvaian mj , blais em , brody jr , et al . 
lancet oncol 2020 ; 21 : 50818.in this article , the x - axis label of figure 3b should have been time on therapy without disease progression ( months )  . 
this correction has been made to the online version as of march 30 , 2020 , and the printed article is correct . pagani bagliacca e , silva m , veneroni l , et al . 
this correction has been made to the online version as of march 30 , 2020 . vol 21 april 2020 e182 corrections surgical treatment and survival from colorectal cancer in denmark , england , norway , and sweden : a population - based study sara benitez majano , chiara di girolamo , bernard rachet , camille maringe , marianne grnlie guren , bengt glimelius , lene hjerrild iversen , edrun andrea schnell , kristina lundqvist , jane christensen , melanie morris , michel p coleman , sarah walters summary background survival from colorectal cancer has been shown to be lower in denmark and england than in comparable high - income countries . 
we used data from national colorectal cancer registries to assess whether differences in the proportion of patients receiving resectional surgery could contribute to international differences in colorectal cancer survival . methods in this population - based study , we collected data from all patients aged 1899 years diagnosed with primary , invasive , colorectal adenocarcinoma from jan 1 , 2010 , to dec 31 , 2012 , in denmark , england , norway , and sweden , from national colo rectal cancer registries . 
we used logistic regression to predict the resectional surgery status patients would have had if they had been treated as in the best performing country , given their individual characteristics . findings we extracted registry data for 139 457 adult patients with invasive colorectal adenocarcinoma : 12 958 patients in denmark , 97 466 in england , 11 450 in norway , and 17 583 in sweden . 
3 - year colon cancer survival was lower in england ( 639% , 95% ci 635643 ) and denmark ( 657% , 647668 ) than in norway ( 695% , 684705 ) and sweden ( 721% , 712730 )  . 
rectal cancer survival was lower in england ( 697% , 691703 ) than in the other three countries ( denmark 725% , 711740 ; sweden 741% , 727754 ; and norway 750% , 731768 )  . 
3 - year survival after stage ii or iii rectal cancer and stage iv colon cancer was consistently lower in england ( stage ii rectal cancer 864% , 95% ci 850876 ; stage iii rectal cancer 755% , 742767 ; and stage iv colon cancer 205% , 199211 ) than in norway ( 941% , 915960 ; 834% , 801861 ; and 330% , 310351 ) and sweden ( 929% , 908946 ; 806% , 782827 ; and 237% , 220253 )  . 
3 - year survival after stage ii rectal cancer and stage iv colon cancer was also lower in england than in denmark ( stage ii rectal cancer 912% , 888931 ; and stage iv colon cancer 235% , 219251 )  . 
the total proportion of patients treated with resectional surgery ranged from 47 803 ( 684% ) of 69 867 patients in england to 9582 ( 813% ) of 11 786 in sweden for colon cancer , and from 16 544 ( 599% ) of 27 599 in england to 4106 ( 708% ) of 5797 in sweden for rectal cancer . 
this range was widest for patients older than 75 years ( colon cancer 19 078 [ 597% ] of 31 946 patients in england to 4429 [ 809% ] of 5474 in sweden ; rectal cancer 4663 [ 457% ] of 10 195 in england to 1342 [ 619% ] of 2169 in sweden ) , and the proportion of patients treated with resectional surgery was consistently lowest in england . 
in the hypothetical scenario where all patients were treated as in sweden , given their age , sex , and disease stage , the largest increase in resectional surgery would be for patients with stage iii rectal cancer in england ( increasing from 703% to 882% )  . interpretation survival from colon cancer and rectal cancer in england and colon cancer in denmark was lower than in norway and sweden . 
differences in patient selection for surgery , especially in patients older than 75 years or individuals with advanced disease , might partly explain these differences in international colorectal cancer survival . funding early diagnosis policy research grant from cancer research uk ( c7923 / a18348 )  . copyright 2018 the author ( s )  . 
 analysts who did this research pointed to the need for research into differences in stage - specific treatment between these countries . added value of this study we used national population - based clinical data to compare stage - specific survival of patients diagnosed with primary colorectal adenocarcinoma in denmark , england , norway , and sweden between 2010 and 2012 , and to assess whether the international survival differences could be explained by differences in patient care . 
we showed that net survival up to 3 years after colon cancer was substantially lower in england and denmark than in norway and sweden , and survival from rectal cancer was lower in england than in the other three countries . 
we also found a steep declining age gradient in the probability of receiving resectional surgery in england , which was less noticeable or not evident in the other countries . implications of all the available evidence these findings have important policy implications , showing that the colorectal cancer survival deficit in england can be attributed partly to shortfalls in treatment . 
we highlight the need for more patient data on comorbidities , frailty , and additional therapies to understand these differences better . the primary treatment for colorectal cancer is surgical removal of the main tumour or tumours and affected tissues . 
total mesorectal excision became the standard surgery for rectal cancer in denmark , norway , and sweden in the mid - 1990s68 and some years later in england.9 this technique entails the removal of the rectum and surrounding tissues , including lymph nodes and fascia , 10 and requires particular surgical training and skills to secure good results . 
the surgical principle of resection in the embryological plane , which is used in mesorectal excision , was later applied to colon cancer surgery , with favourable results in terms of recurrences and survival.11 , 12 preoperative ( neo - adjuvant ) or postoperative ( adjuvant ) radiotherapy or chemotherapy can be used to reduce the risk of recurrence and treat micrometastases.13 , 14 the decision to treat patients with colorectal cancer with neo - adjuvant or adjuvant therapy depends on the extent of disease and risk of recurrence . 
in general , clinical guide lines do not recommend additional therapy for early - stage colon tumours or rectal tumours treated with surgery with adequate resection margins.1315 the use of neo - adjuvant or adjuvant therapy for stage ii or iii tumours is variable betweenand within16countries , particularly for rectal tumours.17 we used population - based data from national colorectal cancer registries to estimate stage - specific and age - standardised net survival at 3 years of patients diagnosed with colorectal cancer in denmark , england , norway , and sweden , and to compare the proportions of patients receiving resectional surgery in those countries by patient and tumour characteristics . methods study design and data sources in this population - based study , we included all patients aged 1899 years diagnosed with primary , invasive colorectal adenocarcinomas from jan 1 , 2010 , dec 31 , 2012 . 
patients diagnosed by their death certification alone and patients with records with invalid date sequences were excluded.18 in denmark , england , and norway , we extracted data from population - based national cancer registries . 
by linking individual patient records in denmark to the danish colorectal cancer group database , 19 additional clinical information was available for 11 746 ( 907% ) patients registered with colorectal adenocarcino mas in the danish national cancer registry . 
similarly , 97 185 ( 997% ) english national cancer registry records for patients with colorectal cancer were linked to at least one of the national bowel cancer audit data , hospital episode statistics inpatient and outpatient records , and the cancer waiting times monitoring data set . 
norwegian national cancer registry data are routinely linked to the norwegian colorectal cancer registry , a specialised registry that contains detailed clinical infor mation on all patients with colorectal cancer nationwide.8 the swedish vol 20 january 2019 for more on the danish colorectal cancer group see for the national bowel cancer audit see org.uk / for the hospital episode statistics see digital.nhs.uk / data - andinformation / data - tools - andservices / data - services / hospital - episode - statistics for the cancer waiting times monitoring data set see information / data - collectionsand - data - sets / data - collections / cancerwaitingtimescwt for the norwegian colorectal cancer registry see registries / clinical - registries / colorectal - cancer - registry / articles for more on the swedish colorectal cancer registry see samverkan / cancerdiagnoser / tjocktarm - andtarm - och - anal / tjock - - och - andtarm / kvalitetsregister / see online for appendix colorectal cancer registry provided clinical data on patients with colorectal cancer in sweden ; 7 its coverage for the study period was near complete.20 definitions of clinical variables ( site , stage , or treatment ) were agreed with in - country clinicians and specialised cancer registry staff to reconcile differences in coding between the various data sources . 
some further discussions with clinicians and registry staff were held to understand and reconcile differences in coding and clinical practices in those countries . all patients included in this study were followed up from time of diagnosis until death or until dec 31 , 2014 , whichever occurred first . 
tumours with morphological codes for non - adenocarcinoma were excluded from analyses . we applied consistent quality control measures to all records ( appendix pp 12 ) .18 in cases of multiple tumours diagnosed at the same site within 6 months of each other , we retained the date of diagnosis of the first tumour ; where stage and type of surgery were inconsistent between records ( n = 327 , 023% ) , we selected the most advanced stage and most extensive surgery . 
for all patients with record of more than one surgery , we selected the most extensive surgery . disease extent ( stage ) , as defined by the union for international cancer control tnm classification of malignant tumours , was characterised by applying a hierarchical algorithm previously described.22 priority was given to pathological confirmation of tumour , lymph node extension , and distant metastases ( if positive ) , over clinical tnm components . 
there is broad comparability between the main stage categories among these tnm editions.22 we defined resectional surgery as the surgical removal of the primary tumour , irrespective of the intent and outcome of surgery , done within 9 months of diagnosis . 
in denmark and england , surgical status was categorised as missing when patients were registered in the national cancer registry but were not recorded in the specialised colorectal cancer registry ( or in hospital episode statistics for england )  . 
we calculated the potential range of the proportion of patients that might have had resectional surgery in denmark and england , first assuming that all patients with missing data were treated and then assuming that they were all untreated . 
we then estimated upper and lower limits of the probable distribution of resectional surgery in each of these countries . information regarding radiotherapy and planned chemo therapy within 6 months of diagnosis was extracted from colorectal cancer registry data in denmark , norway , and sweden , and from national bowel cancer audit and cancer waiting times records in england . we hold approvals from the uk health research authority ( reference ecc 304 ( i ) / 2011 ) , the national health service research ethics service ( 11 / lo / 0331 ) , and the london school of hygiene & tropical medicine ( lshtm , 12171 )  . 
we have a data proces sing agreement with the danish cancer society and approval from the danish data protection agency to use data from the danish colorectal cancer group ; a data disclosure agreement with the cancer registry of norway to use the norwegian data ; and ethical approval from the regional ethical committee in uppsala to use the swedish data . 
data were extracted and transferred with a standard data structure protocol and file transmission procedure , in line with the concord programme for the global surveillance of cancer survival.24 outcomes our primary aim was to assess the estimated agestandardised net survival up to 3 years after diagnosis by country and disease stage and the estimated probability of patients receiving resectional surgery by stage and age in each country . 
we also estimated the hypothetical change in the probability of receiving resectional surgery that patients would have had if they had been treated as in the best performing country , given their individual characteristics . statistical analysis we compared the demographic and clinical characteristics of patients with colorectal cancer diagnosed in denmark , england , norway , and sweden , including patients age , sex , and disease stage . 
received within 6 months of diagnosis ; sources and completeness of information on chemotherapy or radiotherapy varied greatly between countries , with a high proportion of missing information in england . 
 table 1 : characteristics of patients diagnosed with colorectal adenocarcinoma , 201012 information on the cause of death , ( background mortality ) and is suitable for use in international comparisons of survival because background mortality differs between countries . 
in the absence of reliable the background mortality hazard was provided by life tables for the general population defined by country , sex , single year of age , and year.26 we used a multivariable modelling approach to estimate the excess mortality hazard ( ie , due to colorectal cancer ) and predict net survival . 
we used a model selection strategy to test for non - linearity and time dependence of the effects of sex and age on the excess mortality hazard and their interactions.27 survival was predicted by age group , defined by the international cancer survival standard . 
we used international cancer survival standard weights to produce a weighted average of the survival estimates ( age - standardisation ) , to allow for differences between countries in the age distribution of the population of patients with cancer.28 we used the stata command strcs to fit flexible parametric survival models on the log - hazard scale.29 we used multivariate logistic regression models to compare the probability of receiving resectional surgery between countries . 
subsequently , we applied the model coefficients of the best performing country to individuals from the other countries , to assess the hypothetical change in the probability of receiving resectional surgery if patients had been treated as in the best performing country , given their observed characteristics . 
the corresponding author had full access to all the data in the study , and the final responsibility for the decision to submit for publication . results we included information from 139 457 patients diagnosed with colorectal adenocarcinoma in england , denmark , norway , and sweden in our analyses . 
in patients with known disease stage , the proportion diagnosed with stage iiii colon cancer was higher in sweden than in england , vol 20 january 2019 articles norway , and denmark ; for rectal cancer , the proportion diagnosed with stage iiii rectal cancer was higher in england than in sweden , denmark , and norway ( table 1 )  . 3 - year age - standardised net survival from colon cancer was higher in sweden and norway than in denmark and england . 
3 - year survival from rectal cancer was generally similar between denmark , norway , and sweden , and lower in england ( table 2 )  . net survival decreased with the increase in disease stage ( table 2 , figure 1 )  . 
3 - year survival for patients with stage ii tumours was about 90% or higher in all countries , although survival for patients with rectal or colon cancer in england and colon cancer in denmark was notably lower than for patients in sweden or norway . 
 although generally higher than 75% , survival for patients with stage iii colon and rectal cancer was lower in england than in norway and sweden up to 3 years after diagnosis , and in denmark 1 year after diagnosis . 
resectional surgery defined as surgery to remove the primary tumour within 9 months of diagnosis , excluding diagnostic and palliative procedures . table 3 : proportion of patients diagnosed with colorectal adenocarcinoma in 201012 that received resectional surgery by age , sex , and disease stage 205% for england and 330% for norway at 3 years . 
for stage iv rectal cancer , survival was lowest in sweden and england ( 267% in sweden and 271% in england ) and highest in norway ( 385% ) at 3 years ( figure 1 )  . the overall proportion of patients who received resectional surgery was higher for colon than for rectal cancer in all countries ( table 1 )  . 
we could not establish the surgical status of some patients in denmark because they were not registered in the danish colorectal cancer group database ( 949 [ 111% ] of 8567 patients with colon cancer and 263 [ 60% ] of 4391 patients with rectal cancer )  . 
patients with colorectal cancer who were not registered in the danish colorectal cancer group database were more likely to have advanced stage disease or missing stage information and be slightly older than patients registered in the database . 
data on surgery were unavailable for 03% of patients with colorectal cancer in england because their national cancer registry records could not be linked to the additional databases ( hospital episode statistics , national bowel cancer audit , or cancer waiting times )  . 
the proportion of patients receiving resectional surgery was highest in sweden and lowest in england , for both types of cancer ( table 1 )  . in younger patients the proportion of patients treated with resectional surgery was lower in individuals aged 75 years or older than in each country , and international differences in resectional surgery use widened with increasing age of patients ( table 3 )  . 
the share of patients aged 75 years or older with colon cancer with evidence of resectional surgery varied from 19 078 ( 597% ) of 31 946 patients in england to 4429 ( 809% ) of 5474 in sweden . 
in patients aged 75 years or older with rectal cancer , the share of those with resectional surgery varied from 4663 ( 457% ) of 10 195 patients in england to 1342 ( 619% ) of 2169 in sweden . 
for rectal cancer , norway and sweden had the highest proportions of resectional surgery for all but the youngest age group , where denmark had the highest proportion of patients treated . 
england had the lowest proportion of patients treated with resectional surgery for rectal cancer in all age groups and for colon cancer in the two oldest age groups ( table 3 )  . to account for differences in disease stage distribution , we examined the proportion of patients treated by stage and age group ( figure 2 )  . 
the proportion of patients with colon cancer with evidence of resectional surgery for each stage and age group was mostly similar between the four countries for stages i and ii and in patients aged 75 years or younger . 
 however , we observed a steep decline in the proportion of patients that had surgical treatment in the older age categories in england for each disease stage and for both types of cancer , which was not evident in the other countries ( figure 2 )  . 
for instance , a higher proportion of patients received resectional surgery for stage i colon tumours in the 7584 age group than in the 85 and older age group in all countries , but the absolute difference between these age groups was 180% in england vol 20 january 2019 articles compared with 2955% in the other countries . 
information on surgery was missing for some patients in denmark and for a small proportion of patients in england : light grey areas represent the proportion of patients with unknown surgical status by stage and age group ; overall height of the bars shows the proportion of patients that would receive surgery if all patients with missing treatment data had surgical treatment . vol 20 january 2019 articles denmark england norway sweden * colon : stage i colon : stage ii colon : stage iii colon : stage iv rectum : stage i rectum : stage ii rectum : stage iii rectum : stage iv being treated with resectional surgery in any of the four countries . 
however , for patients with rectal cancer diagnosed with stage iiiiv disease , the proportion treated was lower in england than in the other countries in our study , particularly in the oldest age groups ( figure 2 )  . 
we observed an age gradient in the proportion of patients receiving resectional surgery with all rectal cancer stages in denmark , england , and sweden , with lower proportions among patients aged 85 years or older than among younger patients . 
for instance , between patients aged 7584 years and those aged 85 years or older , the absolute difference in the proportion of patients who received resectional surgery for stage iii rectal tumours was 296% in england , 209% in sweden , and 128% in denmark . 
we found no age gradient in the proportion of patients treated for rectal cancer in norway , except for patients with stage iv cancer . to assess the validity of our findings and check whether the age differences in the likelihood of patients receiving resectional surgery were driven by differences in the management of patients diagnosed at aged 90 years or older , we repeated the analyses with exclusion of this patient group . 
the patterns we observed persisted in this reanalysis ( appendix pp 3 , 67 )  . overall , sweden had the highest survival for colon and rectal cancer and the highest proportion of patients receiving resectional surgery , compared with those of the other countries ( although outcomes in norway were generally similar , or better in specific strata , to those in sweden )  . 
to highlight any groups of patients who might be at a disadvantage in the likelihood of receiving resectional surgery compared with patients in other countries , we applied the coefficients for sweden to data from the other three countries and interpreted it as the probability of a patient receiving resectional surgery if they had been treated as in sweden , given their observed age , sex , and disease stage . 
the number of events per parameter was above the recommended threshold of ten in all categories , 31 at 100 events per parameter for our most complex model in the category with fewest events ( stage iv rectal cancer )  . in this hypothetical scenario , changes in the proportion of patients with stage i colon or rectal cancer receiving resectional surgery would be minor ( figure 3 )  . 
in england , denmark , and norway there would be a higher proportion treated among patients with stage ii and iii colon and rectal cancer , if treated as in sweden . 
overall , the largest improvements in the proportion of patients receiving resectional surgery would be seen in patients with stage ii ( from 789% to 907% ) or iii ( from 703% to 882% ) rectal cancer in england . 
the proportion of patients receiving resectional surgery for stage iv colon cancer in denmark and england would increase ( from 391% to 511% in denmark and from 400% to 498% in england ) whereas in norway , the proportion would decrease ( from 556% to 499% ) if patients had been figure 3 : predicted probability of receiving resectional surgery by patient characteristics ( age and sex ) and tumour characteristics ( stage at diagnosis ) error bars are 95% ci . 
 * predicted probabilities of patients receiving resectional surgery by applying the coefficients of the swedish logistic model to the cohorts of patients in each country , on the basis of the country - specific distributions of patient characteristics . 
the overall height of the bars shows the proportion we would observe if all patients with missing treatment data had received surgery . among patients younger than 85 years with rectal cancer who were diagnosed with stage i or ii disease , we observed no significant differences in the likelihood of vol 20 january 2019 articles treated as in sweden . 
the hypothetical decrease in the proportion of stage iv patients receiving surgery in norway would be even larger for rectal cancer ( from 474% to 288% )  . patients with missing disease stage were slightly older than the mean age for each country and cancer type ( range 753773 years for colon cancer and 745754 years for rectal cancer )  . 
the proportion of patients with colon cancer without known disease stage who had evidence of having resectional surgery was lower than that of any known stage category in each country and higher in england than in the other three countries ( table 3 )  . 
additionally , survival of these patients was higher than that of patients with known stage iii disease and lower than that of patients with known stage iv disease , in all four countries ( table 2 )  . discussion in this study , to understand the mechanisms underlying international differences in cancer outcomes , we compared the characteristics of patients diagnosed with colorectal adenocarcinoma in denmark , england , norway , and sweden . 
we provide updated figures of up to 3 - year net survival in these countries , and our results support previous findings of lower survival for patients in england and , to a lesser degree , in denmark , than in sweden or norway.25 our results also support findings that denmark seems to be closing the survival gap with sweden and norway , particularly for rectal cancer.4 , 6 , 24 in the stagespecific analyses , we noted no significant differences between countries in survival for patients diagnosed with early stage ( i or ii ) colorectal adenocarcinomas , but wider international survival differences in patients with more advanced disease stages ( iii or iv )  . 
additional information on treatment , available from specialised colorectal cancer registries , helped us to understand these survival differences better . cancer survival is largely determined by receipt of potentially curative treatment , which , in the case of colorectal cancer , is primarily surgery . 
treatment options mainly depend on disease stage and the underlying health status of patients , which is determined by their comorbidities , frailty , and age . clinical guidelines for cancer treatment aim to standardise and assure adequate cancer care for a population . 
 the amount of detail in the national clinical guidelines regarding colorectal cancer management varied , with recom mendations from england being generally less specific than guidelines from denmark , norway , and sweden.14 , 15 , 32 , 33 nonetheless , indications for surgery were largely consistent between these countries , especially for rectal tumours . 
treatment guidelines for colon cancer in denmark , norway , and sweden explicitly recommend the removal of the part of the bowel that contains the tumour and its mesentery ( and en - bloc resection , if the visceral fascia is compromised because of ingrowth of the tumour into neighbouring organs ) .13 , 14 , 32 by contrast , english guidelines recognise mesorectal excision as the standard surgery for most rectal tumours but do not explicitly recommend the corresponding procedure ( dissection in the embryological plane ) for colon tumours.15 none of the guidelines for the countries in our study mentions age as an exclusion criterion for receiving surgical treatment . 
older patients ( aged 75 years or older with stage iiiv rectal cancer or stage iv colon cancer and aged 85 years or older for the other stages of rectal and colon cancer ) in england had a lower probability of receiving resectional surgery than patients of a similar age with similar disease extension in the other three countries , and a lower probability than younger patients in england . 
england had the steepest negative age gradient in the proportion of patients receiving resectional surgery and had a survival deficit in comparison with the other three countries , particularly for rectal cancer . 
conversely , we noted a higher proportion of patients younger than 85 years who were diagnosed with stage i or ii tumours who had evidence of resectional surgery in england than in the other three countries . 
of the countries studied , only england had a colorectal cancer screening programme with national coverage during the study period.34 the diagnosis and treatment of asymptomatic disease through screening might explain the high proportion of patients surgically treated for early stage disease in the eligible age group in england . 
in the other countries in our study , screening was not imple mented at national level during the study period34 and could not have affected the disease stage distribution or population - based survival . although less aggressive treatment for older patients might sometimes be justified because of comorbidity or frailty , concerns have been raised that some of the disparities in age - related cancer care in england arise because of clinical decision making on the basis of chronological age.35 a 2011 report36 showed lower resection rates in older patients with cancer in england during 200406 than those of younger patients , with less than 2% of patients aged 80 years or older having a major resection surgery for six of 13 cancers examined . although an increase in the proportion of patients receiving resectional surgery does not necessarily translate into better short - term survival because aggressive treatment might be associated with high short - term vol 20 january 2019 articles that mortality , our findings suggest international differences in survival are , at least in part , determined by differences in patient selection practices for surgical treatment . 
choices in management of older patients with colorectal cancer might greatly affect populationbased survival because the mean age at diagnosis is about 70 years.37 patients in countries with a greater proportion of patients treated with surgery and better short - term fewer complications survival might also have more access to laparoscopic surgery or better postoperative care than in the other countries . 
although there is conflicting evidence about the long - term benefit of a laparoscopic versus an open surgical approach for rectal cancer , 38 , 39 laparoscopic surgery is associated with lower perioperative mortality and surgery.40 , 41 in denmark , the increasing use of laparoscopic surgery for colorectal cancer has been associated with a reduction in perioperative mortality rates.42 differences between countries in the use of this approach might explain some of the differences in the proportion of patients receiving surgical treatment and , potentially , in survival . 
however , we were not able to account for this information in our analysis because not all datasets had sufficiently complete data for this question . than open our study has some limitations . 
these include core variables that have previously been examined for comparability and validated in these and other european colorectal cancer registries.43 however , some residual data quality issues might affect the comparability of results . 
performance status scales , which are commonly used to assess patients general condition ( such as their degree of independence ) and eligibility for specific treatments , 44 might not be ideal for older patients with cancer , especially those with mul tiple comorbidities.45 although comprehensive geriatric assessment scales have been proposed and validated , 45 they are rarely used , documented , or routinely collected.46 nevertheless , at the population level , the burden of cardiovascular disease the most common contra indication for surgeryis similar in the four countries included in our study.47 population - based all - cause mortality and life expectancy in older ages are also similar in these four countries ( appendix p 4 ) , supporting the validity of the findings in our study . the overall proportion of patients with unknown disease stage is notably higher in england than in denmark , norway , and sweden . 
the reasons for stage information to be missing are likely to differ according to how high or low the proportion of unknown stage is and , therefore , probably differ between countries . 
patients with unknown disease stage had a lower probability of receiving resectional surgery than patients with known stage , and had similar survival to that of patients with advanced disease stages . 
therefore , our complete - case analysis might overestimate stage - specific survival and the proportion of patients receiving resectional surgery in england , and provides a conservative estimate of the disparities between england and the other three countries in our study . in denmark , 93% of patients were not registered in the danish colorectal cancer group database and thus , their treatment status remained undetermined . 
by contrast with the danish national cancer registry , the danish colorectal cancer group database only includes adults with a first - time diagnosis of colorectal adenocarcinoma treated in danish public hospitals who were in contact with a surgical department.19 therefore , we calculated a potential range of the proportion of patients that might have had resectional surgery and estimated upper and lower limits of the probable distribution of resectional surgery in denmark . 
because of the danish colorectal cancer group databases exclusion criteria and the stage distribution of patients without a danish colorectal cancer group database record , it is probable that a substantial number of these patients did not undergo resectional surgery . 
assuming that none of these patients received resectional surgery , the proportion of patients with rectal cancer who received resectional surgery was still higher in denmark than in england and similar to that in sweden for most combinations of age and disease stage . 
nevertheless , these missing data might have masked some age and stage trends in the likelihood of patients undergoing resectional surgery , especially for colon cancer . we were not able to ascertain treatment intent , residual disease status , venous invasion status , or postoperative complications in patients who received resectional surgery . 
systematic differences in the distribution of such patients between these four countries , or differences in their perioperative management , might affect the between - country comparability of these results . 
 further more , patients with non - resectable tumours in better - performing countries might be more likely to be offered other treatment ( such as treatment to prolong life or make tumours amenable to resection ) than patients in worse - performing countries . 
for example , clinical the guidelines importance of neo - adjuvant or conversion treatment of metastatic tumours to render them resectable , 13 , 14 whereas guidelines in england prioritise symptom control and state that initial systemic treatment followed by surgery should be considered only if both primary and metastatic in norway and sweden describe vol 20 january 2019 articles tumours are judged to be resectable.15 moreover , in countries that frequently use neo - adjuvant therapy with delayed surgery for rectal cancer , the resulting downstaging could cause an under estimation of the differences in stage - specific survival when these countries are compared with settings where neo - adjuvant treatment is more variable or followed by immediate surgery . the completeness and granularity of the data collected by the colorectal cancer registries regarding chemotherapy and radiotherapy varied greatly during the study periodfrom complete registration of radiotherapy protocols in norway and sweden to a high proportion of missing information in england . 
adjuvant chemotherapy is associated with improved outcomes in stage iii colon cancer and is used universally , but for stage ii colon cancer and rectal cancer ( in general ) its value and therefore its use have been more variable.4850 neo - adjuvant radiotherapy decreases recur rence rates , but evidence for its effect on survival is conflicting and so use also varies within countries16 , 51 and between countries.17 the use of targeted therapy in com bination with chemotherapy might help to make tumours amenable to resection in some patients with metastatic or locally advanced disease , 52 but no survival benefit has been shown for this combination.53 for patients with metastatic disease treated with non - curative intent , optimal use of systemic therapy contributes to longer survival.52 , 54 variability between countries in the use of these additional therapies , and other differences in oncological care beyond surgery , might also contribute to the observed differences in survival . despite the limitations of the data included in our study , we have identified important international differences in the distribution of resectional surgery by age and disease stage . 
the main data quality issue ( the higher proportion of patients with unknown disease stage in england ) is likely to have led to a conservative estimate of the differences found in stage - specific survival outcomes in england compared with those of other countries . 
we noted that differences in survival between patients with colorectal cancer treated in england , denmark , norway , and sweden tended to increase with time after diagnosis , and it is possible that these differences between countries would widen with longer follow - up . changes in practice during and after the study period are likely to affect future trends . 
over the past two or three decades , colorectal cancer outcomes have improved in all the countries compared in our study.3 , 24 , 55 the centralisation and specialisation of colorectal cancer surgery have been suggested as important drivers of this improvement.4 a 2012 cochrane review56 found a clear association between operative mortality and 5 - year survival with hospital and surgeon caseload and specialisation . 
however , it is likely that centralisation and specialisation vary between the four countries in our study , and these changes in practice are also likely to affect patient survival differently in these countries.4 , 6 expedited referral routes were initiated in england and denmark in the 2000s , in response to low cancer survival related to system delays.57 , 58 similar rapid referral routes were introduced in norway and sweden in 2016 , following the danish experience . 
although diagnostic delays are important factors in cancer care , the effect of these referral routes on cancer survival remains uncertain . in denmark , a nationwide screening programme with a monitoring database was introduced in 2014.59 the norwegian directorate of health is planning to introduce a national colorectal cancer screening programme in norway in 2019 , offering a faecal immunochemical test or colonoscopy to individuals when they turn 55 years.60 similarly , a national colorectal cancer screening programme is due to be implemented in sweden in 2019 , following regional screening programmes.61 in england , a one - off screening test with flexible sigmoidoscopy for people aged 55 years is being rolled out.62 with increases in diagnosis and treatment of asymptomatic disease , it is likely that survival and the proportion of patients treated for early stage disease will increase in the future . since 2013 , surgeon - specific outcomes have been reported annually as quality measures in england.63 it is hoped that this increase in accountability will lead to improvements in patient care . 
the major reorganisation of the nhs in 2013 , 64 alongside sub stantial resource constraints in the nhs65 in the past decade , has had a potentially negative effect on cancer services . 
for instance , the 62 - day treat ment waiting time targetthe aim that a patient should wait no more than 2 months from the date that the hospital receives an urgent referral for suspected cancer to the start of their treatmenthas been missed for several quarters running , showing that services are unable to meet the demands placed on them.66 given the ongoing financial pressures and austerity in the uk and the nhs , the future trends in survival for patients with cancer in england are uncertain . our findings have important policy implications , suggesting that the colorectal cancer survival deficit in england as compared with denmark , norway , and sweden can be attributed partly to shortfalls in provision of surgical treatment . 
we showed that older patients in england , in particular , were less likely to receive resectional surgery than patients with similar characteristics in the other countries in our study . 
we posit that increases in the proportion of patients receiving resectional surgery might translate into better longer - term outcomes in england , provided that adequate postoperative care is also available . improving the capture of information on patients with colorectal cancer in specialised clinical registries , vol 20 january 2019 articles including data from individuals who are not eligible for surgery , would allow a more complete population - based comparison of colorectal cancer outcomes . 
complete and comparable data on comorbidities , frailty , and additional therapies are required to improve understanding of international differences and inequalities in cancer outcomes . contributors sw , br , mpc , and sbm designed the study . 
 jc and lhi ( denmark ) , sbm and cdg ( england ) , eas and mgg ( norway ) , and kl and bg ( sweden ) prepared national datasets according to the protocol . 
all authors had access to results at the data preparation and analysis stages , contributed to the interpretation of the results , revised and critically reviewed the manuscript , and approved the submitted version . 
sbm , cdg , sw , br , and mpc had access to all the data in the study and take responsibility for its integrity and the accuracy of the analyses . declaration of interests br reports grants from the uk department of health , outside the submitted work . 
all other authors declare no competing interests . acknowledgments this study was funded by an early diagnosis policy research grant from cancer research uk to the cancer policy programme at the london school of hygiene & tropical medicine ( lshtm ; award number c7923 / a18348 )  . 
we thank the national colorectal cancer registries in denmark , england , norway , and sweden for their sustained efforts in collecting data for patients with colorectal cancer to the highest quality standards . 
we are grateful for advice received from members of the cancer policy programme scientific advisory group ( peter sasieni , deborah ashby , paul aylin , andrew roddam , and sally vernon )  . 
the number of patients reporting no pain from bone metastases , as measured by the bpi , increased from 39 of 149 ( 26% ) before sbrt to 55 of 102 ( 54% ) 6 months after sbrt ( p < 00001 )  . 
bpi - reported pain reduction from baseline to 4 weeks after sbrt was clinically meaningful ( mean 34 [ sd 29 ] on the bpi pain - at - its - worst item at baseline , 21 [ 24 ] at 4 weeks ; e ect size 047 , p = 000076 )  . 
these improvements were accompanied by signi cant reduction in opioid use during the rst 6 months after sbrt ( 43 [ 289% ] of 149 patients with strong opioid use at baseline vs 20 [ 200% ] of 100 at 6 months ; p = 0011 )  . 
ordinal regression modelling showed that patients reported signi cant pain reduction according to the mdasi during the rst 6 months after sbrt ( p = 000003 ) , and signi cant reductions in a composite score of the six mdasi symptom interference with daily life items ( p = 00066 )  . 
 only a few instances of non - neurological grade 3 toxicities occurred : nausea ( one event ) , vomiting ( one ) , diarrhoea ( one ) , fatigue ( one ) , dysphagia ( one ) , neck pain ( one ) , and diaphoresis ( one ) ; pain associated with severe tongue oedema and trismus occurred twice ; and non - cardiac chest pain was reported three times . 
signi cant reductions in patient - reported pain and other symptoms were evident 6 months after sbrt , along with satisfactory progression - free survival and no late spinal cord toxicities . funding national cancer institute of the us national institutes of health . 
 introduction almost 40% of patients with cancer develop spinal metastases during the course of their disease.1 , 2 inadequately treated spinal metastases can lead to pain and neurological complications , including metastatic epidural spinal cord compression . 
as a result , patients might experience severe symptom burden and diminished health - related quality of life ( hrqol ) .35 palliative radiotherapy e ectively controls pain for patients with spinal metastases ; 4 however , higher - dose radiotherapy might be needed for durable tumour control and prevention of bony destruction of the spinal column , which results in spinal instability . 
the spinal cords sensitivity to radiation generally precludes high radiation doses to the spine or re - irradiation using conventional techniques.6 accordingly , new techniques have been developed to optimise radiation dose delivery to bone metastases while sparing the spinal cord . 
 stereotactic body radiotherapy ( sbrt ) , an emerging technique , uses image guidance to deliver high - dose radiation precisely , creating a steep dose gradient at the interface between spinal cord and tumour . 
this approach increases the therapeutic window by lowering the risk for spinal cord myelopathy.68 delivered in high doses and one to ve fractions , spinal sbrt is available on various platforms , some of which include ct imageguided stereotaxy . 
sbrt can be used in combination with or in lieu of surgery and allows patients to avoid possible perioperative risk factors , such as general anaesthesia , bleeding , infection , or hospitalisation . 
in a preliminary report of a prospective phase 12 trial of sbrt , we detailed the safety , e cacy , and patterns of failure for sbrt using results from a vol 13 april 2012 articles subset of patients ( n = 63 ) with spinal metastases who were followed for up to 50 months.2 in the present analysis of the entire patient cohort , we investigated the symptomreduction bene t of spinal sbrt during the rst 6 months post - treatment , and clinical bene t for up to 2 years . 
we hypothesised that , for patients with mech an ically stable spinal metastases , sbrt is a clinically e ective therapy for tumour control ( evidenced by radio graphic depiction of tumour progression ) and sympto matic improvement ( evidenced by patient - reported outcomes )  . 
 methods patients this phase 12 trial was approved by the institutional review board of the university of texas md anderson cancer center ( houston , tx , usa )  . 
 eligibility requirements included a diagnosis of cancer ( excluding multiple myeloma ) , a karnofsky performance status score of at least 40 , and an mri scan documenting spinal or paraspinal metastasis within 4 weeks of enrolment . 
acceptable indications included oligometastatic disease arising from a known primary tumour , failure of previous conventional external beam radiotherapy or surgery , residual tumour after surgery , medical inoperability , and refusal to undergo surgery . 
 patients with mechanically unstable spine or epidural spinal cord compression were excluded ; however , patients with previously documented spinal cord compression that had been decompressed and stabilised were eligible . 
 patients were excluded if they had a pacemaker , were unable to undergo mri , or had received systemic radiotherapy ( strontium 89 ) or cytotoxic chemotherapy within 30 days of enrolment , or spinal external beam radiotherapy within 3 months of enrolment . 
 procedures all patients underwent intensity - modulated , nearsimultaneous , ct - guided sbrt ( ct - linac system [ exact targeting system , varian medical systems , palo alto , ca , usa ] or trilogy treatment delivery systems with on - board imager cone beam ct [ varian medical systems ] ) using a bluebag bodyfix total body immobilisation system ( elekta , stockholm , sweden ) , consisting of a whole - body vacuum cushion , carbon bre base plate , and plastic xation sheet . 
patients received a total dose of 2730 gy , typically delivered in three fractions given every other day , with 10 - gy radiation volume received by the spinal cord limited to 001 c gross target volume encompassed the lesion as visualised on the pretreatment ct scan . 
the clinical target volume encompassed the gross target volume and surrounding vertebral body ( including superior and inferior endplates and any existing paraspinal component ) , along with all additional spinal structures deemed to be at risk for recurrence , such as the pedicle , lamina , and posterior elements . 
in patients with postsurgical metallic artifacts near the area of interest , intrathecal contrast injection with iohexol ( ge healthcare canada inc , mississauga , on , canada ) was done 3060 min before ct image acquisition to assist with accurate spinal cord delineation . 
we measured pain at metastatic sites treated with sbrt via the brief pain inventory ( bpi ) .9 the bpi assesses pain at present and pain at its worst , least , and on average in the past 24 h , on a 010 scale . 
the bpi and mdasi are well validated in patients with various types of cancer.9 , 10 the medical outcomes study 12 - item shortform health survey ( sf - 12 ) was administered as an hrqol measure.11 patient - reported symptoms were assessed in the clinic via the bpi , mdasi , and sf - 12 pre - sbrt ( baseline ) and at 3 months and 6 months post - sbrt ; assessments at 2 weeks , 4 weeks , and 2 months were completed by the patient at home and returned by post , with a reminder call from a study nurse . 
 mri scans of the region treated were done at 3 , 6 , 9 , 12 , 18 , and 24 months post - sbrt and then every 6 months thereafter , as standard care . 
 history , neurological exam results , and mccormick functional classi cation12 were obtained at baseline and at each follow - up visit ( during the same timepoints as patient - reported outcomes assessments )  . 
toxicity was graded by the patients treatment team according to the national cancer institute common toxicity criteria for adverse events , version 2.0.13 statisticsmean , median , sd , statistical analysis descriptive and proportionsare used to describe patient and clinical characteristics . 
to account for multiple comparisons in the symptom and hrqol outcomes , which required eight modellings , we adjusted the individual type i error to be 005 / 8 = 000625 to maintain a conservative family - wise error rate of 005 . using pain cutpoints established by serlin and colleagues , 14 we categorised ratings of the bpis pain - atits - worst item as no pain ( 0 ) , mild pain ( 14 ) , moderate pain ( 56 ) , and severe pain ( 710 )  . 
concordance between bpi and mdasi painat - its - worst ratings , both scored on a 010 scale in the past 24 h , was examined using paired t tests . 
e ect sizes were calculated to estimate the magnitude of change in bpi and mdasi ratings ( composite score for all patients ) between baseline and 4 weeks post - treatment.15 , 16 for patient - reported outcomes measures , e ect sizes are clinically meaningful at roughly one - half sd or higher , the level often used in distribution - based methods of determining meaningful di erences.17 lowess curves , 18 which represent a smoothed estimate of average mdasi symptom severity and interference as a function of time , were constructed from baseline to 6 months post - sbrt . 
 ordinal regression models19 and generalised linear mixed models were tted to examine symptom development for the ve most - severe mdasi symptoms and the symptom - interference component score from baseline to 6 months post - sbrt . 
independent variables included weeks from start of therapy , age , sex , tumour volume of spinal metastasis at baseline , type of primary cancer , disease progression status 6 months after sbrt based on radiographic ( spinal mri ) results , opioid use , and karnofsky performance status at baseline . progression - free survival ( pfs ) and overall survival curves from date of enrolment were generated using the kaplan - meier method . 
spinal mris were done for 142 of 149 patients ( 95% ) at the 6 - month follow - up . baseline characteristics ( n = 149 ) 564 ( 125 ) 580 ( 200880 ) karnofsky performance status number of lesions age in years mean ( sd ) median ( range ) male female 8090 none primary histology breast cancer colon cancer melanoma thyroid cancer renal cancer sarcoma other unknown sbrt site cervical thoracic lumbar sacral previous therapy to spinal site radiotherapy alone surgery alone radiotherapy and surgery non - small - cell lung cancer 77 ( 52% ) 72 ( 48% ) 8 ( 5% ) 108 ( 72% ) 30 ( 20% ) 3 ( 2% ) 40 ( 27% ) 22 ( 15% ) 39 ( 26% ) 48 ( 32% ) 15 ( 10% ) 6 ( 4% ) 15 ( 10% ) 4 ( 3% ) 14 ( 9% ) 47 ( 32% ) 17 ( 11% ) 28 ( 19% ) 3 ( 2% ) 28 ( 19% ) 66 ( 44% ) 51 ( 34% ) 4 ( 3% ) metastatic tumour volume in cm , median ( range ) 382 ( 163579 ) data are number of patients ( % ) unless otherwise stated . 
sbrt = stereotactic body radiotherapy . at the time of analysis , 40 of 149 patients ( 27% ) were still alive , with a median follow - up of 159 months ( range 10916 ; iqr 95303 ) and mean 209 months ( sd 171 )  . 
median overall survival was 23 months ( 95% ci 186272 ) post - sbrt , with 1 - year and 2 - year actuarial survival of 685% ( 601754 ) and 464% ( 378547 ) , respectively . 
tumour progression was seen in 41 of 149 patients ( 28% ) and occurred at a median of 13 months ( range < 1101 ) , based on mri scans . 
actuarial pfs based on mri scans at 6 months , 1 year , and 2 years post - sbrt was 861% ( 95% ci 794907 ) , 805% ( 729861 ) , and 724% ( 631797 ) , respectively . 
 * no signi cant di erences between bpi pain - at - its - worst mean scores and mdasi pain item mean scores ( paired t tests ) were found at any timepoint other than the 6 - month assessment ( p = 0022 )  . 
the number of patients for whom analgesia data were available di ered slightly from the number of patients who provided symptom data . table 2 : pain severity scores and opioid use over time , before and after sbrt pain - at - its - worst ratings , at baseline and post - sbrt assessments . 
 the proportion of patients reporting no spine pain on the bpi increased signi cantly between baseline and 4 weeks post - sbrt , from 39 of 149 ( 26% ) to 43 of 109 ( 39% ) ( p = 0038 )  . 
this improvement continued throughout the study , with 53 of 120 ( 44% ) reporting no pain at 3 months ( p = 0004 ) and 55 of 102 ( 54% ) reporting no pain at 6 months ( p < 00001 )  . 
further , a signi cant decrease in the percentage of patients with moderate - tosevere bpi spine pain ( rated 5 on the 010 scale ) was noted from baseline to 4 weeks ( p = 0003 ) , 2 months ( p < 00001 ) , and 6 months ( p = 0002 ) post - sbrt . we noted clinically meaningful reductions in mean mdasi pain ratings between baseline and 4 weeks posttreatment ( from 34 [ sd 31 ] at baseline to 21 [ 26 ] at 4 weeks on the mdasis 010 scale ; e ect size 047 )  . 
 di erences in mean pain severity ratings between the bpi ( metastatic bone pain ) and mdasi ( general pain ) were noted only for the 6 - month assessment ( p = 0022 ; table 2 )  . 
we noted signi cant reduction in opioid use from baseline to 3 months ( p = 0021 ) and baseline to 6 months ( p = 0011 ) post - sbrt ( table 2 )  . 
 during the 6 months of observation , the ve most severe mdasi symptoms were fatigue , pain , disturbed sleep , 398 vol 13 april 2012 articles fatigue pain disturbed sleep drowsiness distress general activity normal work walking ability enjoyment of life mood relations with other people drowsiness , and distress . 
the lowess curves in gure 2 show that symptom interference lessened over time . reduction table 3 gives p values from ordinal regression modelling of mdasi symptom severity and interference , and sf - 12 physical and mental health component scores , adjusted for independent variables . 
patients reported signi cant pain ( p = 000003 ) 6 months after sbrt , and signi cant reduction in disturbed sleep , drowsiness , sadness ( all p < 00001 ) , fatigue , distress , lack of appetite , nausea , and di culty remembering ( all p < 005 )  . 
ordinal regression modelling showed that a composite score of all six interference items decreased signi cantly at each successive assess ment during the 6 months after sbrt ( p = 00066 )  . 
 patients whose lesions were categorised as progressive at the 6 - month follow - up examination ( 19 of 149 ; 13% ) reported signi cantly more - severe mdasi pain ( p < 00001 ) , fatigue ( p = 001 ) , and drowsiness ( p = 000008 ) than did patients with stable or smaller lesions . 
patients who received opioids during the 6 months after sbrt reported more severe mdasi pain , fatigue ( both p < 00001 ) , disturbed sleep , distress , and drowsiness ( allp < 0001 ) than did patients not using opioids . 
grade 3 toxicities were nausea ( one event ) , vomiting ( one event ) , diarrhoea ( one event ) , fatigue ( one event ) , non - cardiac chest pain ( three events ) , dysphagia ( one event ) , neck pain ( one event ) , diaphoresis ( one event ) , and pain associated with severe tongue oedema and trismus ( two events )  . 
 discussion this study incorporated validated single - symptom ( bpi ) and multisymptom ( mdasi ) assessments to measure patient - reported outcomes for pain and other symptoms in patients with metastatic spine lesions who received sbrt . 
in accordance with our previous report documenting the safety , e ectiveness , and patterns of failure of spinal sbrt , 2 here we showed signi cant reductions in the severity of pain and consistent reductions in other patient - reported symptoms and symptom interference 6 months after spinal sbrt , along with satisfactory pfs and no late spinal cord toxicities . 
 signi cant at p < 000625 , after adjusting for multiple comparisons ( eight models )  . table 3 : signi cance of reduced score for patient - reported outcomes during the rst 6 months after sbrt , adjusted for independent variables panel : research in context systematic review in recent years , spinal stereotactic body radiation therapy ( sbrt ) has become an increasingly established technique for the management of spinal metastases ; however , when this phase 12 trial was designed and activated in 2002 , spinal sbrt literature was in its infancy , consisting of preliminary technical reports with sparse outcomes data . 
drawing on previous experience in symptom research , 25 , 26 we applied well - established symptom - assessment methods to analyse outcomes data acquired from our prospective cohort . interpretation the results of this study show that sbrt is an e ective primary or salvage treatment for mechanically stable spinal metastasis . 
signi cant reduction in patient - reported pain and other symptoms was evident 6 months after sbrt , along with satisfactory progression - free survival and no late spinal cord toxicities . 
for patients with evidence of tumour progression 6 months after sbrt , such progression was signi cantly associated with more severe pain , as expected , suggesting a true ( non - placebo ) palliative e ect for sbrt . 
 this trial provides prospective data that support the careful use of spinal sbrt in selected patients , since sbrt safely and reliably halts the progression of disease while reducing patient symptoms and improving functioning in daily life , as measured by validated methods . 
this study also highlights the importance of integrating patient - reported symptom assessments with clinical outcome evaluations to fully demonstrate the bene t of sbrt in patients with metastatic spinal disease . 
between baseline and 4 weeks post - sbrt , we observed medium , but clinically meaningful , e ect sizes for pain reduction as reported on both the bpi pain - at - its - worst and mdasi pain items , along with signi cant increase in the number of patients reporting complete pain relief as early as 4 weeks post - sbrt . 
signi cant improvement in bpi pain ratings and e ect size relative to pre - sbrt scores was even larger 6 months after treatment ( e ect size 064 , p < 00001 ) , when only two patients had tumour progression and high pain severity and were receiving opioid therapy . 
the e ectiveness of sbrt for tumour and pain control was further evidenced by a reduction over time in the use of strong opioids , astandard of care for managing severe pa patient - reported data from the bpi and the mdasi , which use the same 010 pain - severity rating scale and 24 - h recall period ( table 2 ) , did not di er signi cantly in this cohort of patients with advanced cancer . 
this result suggests that researchers can use either scale in clinical studies when pain at its worst is the outcome of interest , and the same rating is expected with either scale . 
 the present study shows that pain reduction and functional improvement can also be re ected in the reduction of associated symptoms , such as fatigue , distress , and disturbed sleep.21 using a sensitive multiplesymptom assessment method ( the mdasi ) with a highly selective but comprehensive set of symptom items , 22 , 23 we not only prospectively identi ed pain and other major symptoms in a cohort of patients who received spinal sbrt , but also showed how multiple symptoms improved over time after treatment . 
signi cant reductions in the severity of several 400 vol 13 april 2012 articles symptoms in addition to metastatic pain suggest that spinal sbrt produces minimum symptom burden and toxic e ects for patients with late - stage cancer . 
we did not nd a signi cant di erence between renal - cell carcinoma and other primary histologies on patient - reported severity of any mdasi symptom ( data not shown )  . fatigue was consistently the most severe symptom over time , possibly as a result of advanced disease and continuous use of opioids . 
although fatigue improved over the 6 months post - sbrt ( p = 0037 ) , the physical and mental health component scores of the sf - 12 remained more or less constant in follow - up . 
these results are consistent with those of degen and colleagues , 24 who reported signi cant pain reduction 4 weeks after spinal sbrt that was durable to 1 year , but no signi cant change in physical or mental well - being data from the sf - 12 . 
in the present study , lower baseline karnofsky performance status was signi cantly associated with higher total symp tom interference on the mdasi and worsening physical well - being as measured by the sf - 12 ( table 3 )  . 
 the e cacy and safety of sbrt we report in this study are supported by the structured schedule with de ned assessment intervals and follow - up serial spinal mris , which permitted close assessment of the procedure . 
in this study , sbrt did not lead to any radiation - related spinal cord myelopathy ; the numbness reported by some patients was probably caused by pre - sbrt chemotherapy . 
in the present study , 24 patients did not return their paper - and - pencil symptom assessment results by post at the 2 - week assessment timepoint ; nonetheless , most of these patients contributed symptom data at subsequent timepoints . 
however , it is well accepted that sbrt has a quanti able clinical e ect on tumour growth with an accompanying reduction in pain at the radiation site , as shown in our previous report in a subset of this cohort of patients with stage iv cancer.2 one strength of the present study is that multiple symptoms were assessed simultaneously and longitudinally for each patient and compared with baseline , with each patient serving as his or her own control . 
such a trial is currently ongoing with the radiation therapy oncology group 06 - 31 study . in reviewing patient records , we found that 16 patients were positive for adrenal metastasis and 12 were positive for brain metastasis at enrolment . 
for this reason , although the protocol designated data collection up to 24 months , we did not use patient - reported outcomes data beyond 6 months , after which the symptomreduction bene t from sbrt could be confounded by increased pain from rapid disease progression at or near the end of life in this cohort with very advanced cancer . 
 further study of this data is warranted to determine the entire pro le of pain and other symptoms , from beyond 6 months post - sbrt to near the time of death . 
 radiation the role of sbrt in treating mechanically stable spinal metastases without spinal cord compression is continuing to develop in an era in which new tech nologies and treatments are being highly scrutinised . 
nonetheless , the current study provides additional data that support the clinical bene t of sbrt for carefully selected patients and suggests that sbrt reliably halts the progression of disease , reduces patient symptoms , and leads to improved functioning in daily lifethus demonstrating both symptomatic and clinical bene t ( panel )  . 
this study also highlights the importance of integrating patient - reported symptom assessments with clinical outcome evaluations to fully demonstrate the bene t of sbrt in patients with metastatic spinal disease . 
 all other authors declare that they have no con icts of interest . acknowledgments the researchers from the department of symptom research are partially funded by a grant from the national cancer institute ( nci ) of the us national institutes of health ( nih )  . 
therefore , our results seem applicable to the community at large . unfortunately , several known risk factors were not reported in many patients , and cross - tabulations showed di erences in the three treatment groups for detection method ( p = 0001 ) , tumour size ( p = 0002 ) , tumour grade ( p = 004 ) , margin status ( p < 00001 ) , and oestrogen receptor status ( p = 006 )  . 
when comparing patients receiving radiotherapy who were given boost with those who were not , we found that the distribution for detection method tumour grade , or oestrogen receptor status was very similar between the two groups . 
as expected , patients with a boost had more tumours of unknown size ( 49% vs 31% ) , and unknown margin ( 43% vs 25% ) than patients who did not receive a boost . 
for example , in the european organisation for research and treatment of cancer ( eortc ) study , poor di erentiation was ( illogically ) better in terms of local recurrence than intermediate di erentiation in multivariate analysis.2 as in our study , age , margin status , and radiotherapy were important variables , and the researchers concluded that young women and those with involved margins are at high risk of local recurrence , even after radiotherapy with 50 gy.2 we know that young women are at high risk for local failure , so why shouldnt we use a boost with a proven bene t3 to improve the results in dcis too ? furthermore , boost radiotherapy was well - tolerated in the eortc study , 3 with only 1% severe breast brosis ( similar to that in the standard group ) and led to only a small reduction in excellent or good cosmesis . in our retrospective study , a boost was probably given more often in the presence of adverse prognostic factors . 
i agree that results might have been even better with a radiotherapeutic quality programme , and that an improved de nition of the exact boost volume might have been achieved . our results indicate the situation in invasive breast cancer , and in the absence of other data , they justify boost radiotherapy in young patients with dcis . 
the attainment of level 1 evidence from adequately powered randomised trials with a quality assurance programme is desirable , and future research by the international breast cancer study group ( ibcsg ) and eortc might one day address this . 
the question of which treatment should be used as standard is debatable , but we think boost treatment is the most promising strategy . guenther gruber coordinator of the radiation oncology task force , ibcsg international breast cancer study group , institute of radiation oncology , kantonsspital , aarau , switzerland guenther.gruber@ksa.ch i declare no con icts of interest . omlin a , amichetti m , azria d , et al . 
breast - conserving treatment with or without radiotherapy in ductal carcinoma in situ : ten - year results of european organisation for research and treatment of cancer randomized phase iii trial 10853a study by the eortc breast cancer cooperative group and eortc radiotherapy group . 
in table 6 of this health - care research article ( p 592 ) , the estimated demand for megavoltage machines in 2002 for chile should have read 44 , and the total estimated demand for megavoltage machines in 2002 should have read 1060 . douillard j - y , rosell r , de lena m , et al . 
adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ibiiia non - smallcell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
the a liation for v lorusso should have read irccs oncologico , bari , italy ( v lorusso md ) in the author address list ( p 719 ) and m de lena , v lorusso ( irccs oncologico , bari ) in the investigator list ( p 726 )  . 
in the investigator list ( p 726 ) , e massa ( policlinico universitario , cagliari ) should have read g mantovani , e massa ( policlinico universitario , cagliari )  . gajjar a , chintagumpala m , ashley d , et al . 
risk - adapted craniospinal radiotherapy followed by high - dose chemotherapy and stem - cell rescue in children with newly diagnosed medulloblastoma ( st jude medulloblastoma96 ) : long - term results from a prospective , multicentre trial . 
the fourth sentence of the second paragraph in the results ( p 816 ) should have read : 5 - year event - free survival was 66% ( 4883 ) for the 42 patients with metastatic disease and 63% ( 4483 ) for the 33 patients with m23 disease . vol 7 october 2006 correction to lancet oncol 2017 ; 18 : 55657 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 104048 stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 917 28justin affiliations stebbings should have read division of cancer , department of surgery and cancer , imperial college london , london , uk , and his declaration of interests statement should have read js is supported by the biomedical research centre , imperial college london , and the national institute for health research . 
lancet oncol 2017 ; 18 : 104048in figure 2 of this article , the key for the treatment groups the observation group in blue and the srs group initials of in red . 
these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . should have shown sentences follows : kotsakis a , georgoulias v . 
the two related should have affected read however , important finding from these two studies was that the frequency of infusion - related reactions exceeded 20% ; infusion - related reactions are uncommon with the other approved immunotherapeutic agents , with an estimated frequency of about 12% and once again , ongoing phase 3 trials ( nct02395172 , nct02576574 ) might shed light on the frequency , significance , and severity of infusionrelated adverse events and how best to manage the these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 73242 breast cancer emtansine diras v , miles d , verma s , et al . 
 trastuzumab versus capecitabine plus lapatinib in patients with previously treated her2 - positive ( emilia ) : advanced a descriptive analysis of final overall survival results from a randomised , openlabel , phase 3 trial . 
these corrections have been made to the online version as of july 26 , 2017 . correction to lancet oncol 2017 ; 18 : 102239 rarecareneta centralised rare tumours : gatta g , capocaccia r , botta l , et al , for the rarecarenet working group . 
 in the results section , but soft tissue sarcomas were treated more centrally than bone sarcoma should have been but soft tissue sarcomas were treated centrally less than bone sarcoma . 
 these corrections have been made to the online version as of july 26 , 2017 , and the printed article is correct . vol 18 august 2017 e433 corrections editorial for the society of gynecological oncologys position statement see newsroom / positionstatements - 2 / morcellation / patient safety must be a priority in all aspects of care in december , 2013 , the society of gynecologic oncology ( sgo ) released a position statement regarding intracorporeal morcellation , a technique by which tissues excised during minimally invasive surgery are cut up to facilitate removal through small excisions , which might increase the risk of disseminating tumour cells . 
the statement follows the case of a harvard anaesthetist who had a hysterectomy involving intracorporeal morcellation at brigham and womens hospital , boston , ma , usa , to treat presumed benign broids , and was subsequently found to have leiomyosarcoma ; the patient is now being treated for stage iv disease . 
subsequent to this case and another similar incident at the same hospital , the chair of obstetrics and gynaecology issued a note to medical sta warning that morcellation of an occult tumour may occur in between one in 400 and one in 1000 women who have this procedurea risk at least ten times higher than previously assumed . 
in view of the strong risk of developing high - grade cancer following the procedure , this advice is prudent , but does it go far enough ? minimally invasive surgery does , of course , have major advantages and the advent of these techniques has heralded an era of shorter hospital stays , lower infection risk , quicker recovery times , reduced use of donor blood , and less scarring . 
in most areas of life , new technologies are received with an implied assumption that they are better than the device or procedure they are intended to replace , and so seems to be the case in medicine . 
 however , contrary to the situation with new drugs , medical devices do not have to undergo such rigorous testing and safety pro ling before they are propelled into everyday clinical practice by the manufacturers extensive , unregulated marketing . 
it is not practical to subject every new surgical procedure to the same trial processes as new drugs , but nevertheless structured follow - up and full reporting of adverse events should be the minimum standards . 
guidelines should err on the side of caution where hazards are reported , as has been the case with intracorporeal morcellationthe risk of disseminating malignant cells by morcellation has been shown numerous times over the past couple of decades . 
for instance , the patient information website for one manufacturers minimally invasive system extols the bene ts of the system in hysterectomy for a range of conditionsincluding cancerbut fails to mention that morcellation could spread cancer cells . 
this problem needs urgent attention , not only because hysterectomy is extremely common and a one in 400 risk of morcellating an occult tumour is unacceptable , but also because these techniques are used in a wide range of settings . 
 moreover , comparison of visual scores assessments with of the pten reaction product histological slides can show important discrepancies.6 thus , pten score values estimated by an observer should not be used as a simpli ed surrogate computerised optical density for measurement . 
a computer - assisted reassessment of the stained sections used by obyrne and colleagues , 1 followed by survival models based on continuous data for pten expression , would give more reliable results . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata kreimer ar , gonzlez p , katki ha , et al , for the cvt vaccine group . 
e cacy of a bivalent hpv 16 / 18 vaccine against anal hpv 16 / 18 infection among young women : a nested analysis within the costa rica vaccine trial . 
 lancet oncol 2011 ; 12 : 86270in the trial pro le of this study , virgins who were excluded from the restricted cohort were wrongly classi ed as missing cervical dna results . 
in the results section , the follow - up time for the hpv group should have been 542 months ( range 470748 ) and for the control group 542 months ( range 470744 ) , with a median follow - up time of 542 months and a p value for di erence by arm of 0975 . 
lancet oncol 2011 ; 12 : 98889contrary to the statement made in this comment , we have been subsequently alerted to the fact that translational studies associated with sch ski and colleagues trial had been undertaken but are not yet published . 1096 vol 12 november 2011 editorial to read more about the lancet oncologys cancer campaign and the four commissions go to campaigns / cancer / for our previous editorial on direct - to - consumer marketing see lancet oncol 2008 ; 9 : 1113 tackling the cancer epidemic rising cancer is the primary cause of death in many countries , now exceeding heart disease . 
in lower income countries , fast , creating unprecedented incidence challenges for health systems , many of which were designed in an era that did not foresee , were simply incap able of pre - empting , or knowingly ignored the future . 
 however , these remarkable achievements come at a pricethe cost of care is outpacing national budgets , the numbers of cancer patients and survivors are putting greater pressures on health - care systems , and increasing numbers of vulnerable patients from less traditional demographics , such as children and younger adults , require di erent clinical solutions that have yet to be fully conceived . this month , the lancet oncology launches a campaign focused on tackling the cancer epidemic at a systems level . 
we will document , via monthly updates , the evolution of four commissions intended for publication later this year that aim to de ne the scale of the challenge , the underlying drivers , and the improvements needed to cancer - care systems . 
these special reports will cover global access to radiotherapy , surgical resource availability and its fundamental role in cancer treatment , the intersection of primary care in a comprehensive cancer service t for the 21st century , and the ongoing oncology requirements in the low - to - middle income countries of latin america . 
 the lancet oncology dangers of direct - to - consumer advertising exposed again direct - to - consumer ( dtc ) advertising is in the headlines agaon feb 19 , 2015 , 23andme was granted approval by the us food and drug administration ( fda ) to market a genetic test for bloom syndrome . 
and on feb 25 , 2015 , the us federal trade commission ( ftc ) ned two companies for marketing melanoma detection apps ( melapp and mole detective ) and banned them from making misleading or unsubstantiated health claims in the future . 
 the decision to permit 23andme limited access to the dtc market is a remarkable turnaround for a company that on nov 22 , 2013 , received an fda warning letter instructing them to stop all marketing . 
at that time , the fda insisted the company seek approval for each speci c indi cation in their pan - genomic test along with robust evidence for each claimin line with the requirements for other over - the - counter home - use tests . 
despite the seeming appro priate ness of the decision , it creates an uneasy precedentone that could open the door to other less reliable tests if the delineations of the ruling are not rmly upheld . 
these concerns are further underscored by the jnci article showing that websites promoting person alised cancer medicine products contain more information about the bene ts than the limitations , and most focus on one or more non - standard tests . ensuring people take an active interest in their health is central to a strong health - care system , but health - care decisions need to be a bilateral process between patients and their doctors . 
in our december , 2008 , editorial , we con cluded that the marketing of tests should be restricted to health professionals , rather than the lay public , and only accessed through health - care providers on the basis of their advice . 
 the corrected version rst appeared at thelancet.com / oncology on sept 4 , 2014 see articles lancet oncol 2014 ; 15 : 68999 see editorial lancet oncol 2014 ; 15 : 667 patient priority in the era of patent expiries on aug 8 , 2014 , the uk national institute for health and care excellence ( nice ) ruled that trastuzumab emtansine is not cost e ective for routine use for patients with her2 - positive breast cancer in englands national health service . 
 using clinical data from the emilia and th3resa trials , roche valued the drug at just over 90 000 per patient more than twice the price of trastuzumab alonedespite a lack of head - to - head evidence showing trastuzumab emtansines greater e cacy compared with trastuzumab to justify the higher price . 
on july 28 , 2014only 11 days before nice issued their press releasethe patent for trastuzumab ( which earnt the company us$59 billion in 2011 alone ) expired in the european union ( eu )  . 
earlier this year , p zer attempted a takeover of astrazeneca in the uk in a deal estimated at 63 billion , a move considered by many as not only a means to avoid corporation tax in the usa , but also a way to substantially boost the companys pipeline without heavy investment in research and development . 
despite the deal falling through , the attempted acquisition may be representative of pharmaceutical companies responses in recent years to try to recoup losses from a series of drugs that have simultaneously gone o patent . 
 this phenomenonthe so - called patent cli has been extensively reported since one of the rst blockbusters , atorvastatin , a cholesterol - lowering drug that had estimated global sales in excess of 64 billion a year , went o patent in 2011 . 
since then , and in light of an unprecedented number of blockbuster drugs coming o or soon to come o patent , a urry of mergers and acquisitions by pharmaceutical companies has taken place in an attempt to revive pro ts , most notably in diversifying their portfolio in to low - risk revenue streams ( eg , animal health , medical devices , and generic drugs ) as well as expanding their pipelines to include biological agents . 
despite the number of legitimate steps taken to extend patent licences , there have also been a series of morally dubious legal strategies used by patent proprietors to extend their patents . 
in addition to applying for supplementary protection certi cates ( allowing the patent to be extended up to 5 years in the eu ) , and 6 - month paediatric exclusivity licences , both of which are common practices to extend patent protection , pharmaceutical companies have explored other ways to gain extensions to their existing patents , such as new approvals in di erent medical settings to the original application . but where is the line between legitimate patentable development , and abusive extension of patent rights ? in 2001 , glaxosmithkline accumulated 5 years of 30 - month stay approval from the us food and drug administrationan automatic period granted to originator companies if threatened by patent infringementfor the drug paroxetine . 
although lawful , this example does raise the question as to whether these strategies are a violation of patients rights of access to a ordable , e ective medicines , especially considering the unsustainable nancial burdens faced by health - care systems worldwide . 
in a bid to maintain income , it is worrying that the pharmaceutical industry might opt to prioritise loopholes in legislation , undertake litigation , and consider mergers and acquisitions as a more rewarding primary focus to secure revenue , as opposed to competitive income from the development of new medicinal products . 
it is crucial , therefore , that appropriate legislation is in place to encourage strike a balance pharmaceutical between their own pro t ability and upholding a contemporary social and ethical responsibility to allow a ordable access to medicines to those most in need . 
 the lancet oncology companies vol 15 september 2014 1039 correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections the real worth of cancer drugs launched in november , 2020 , we witnessed one of the most awaited elections in recent timesthe usa elected joe biden as its new president , and with this decision comes renewed hope for science . 
for oncology , we wait in anticipation to see whether the cancer moonshot programme , in 2016 under the obama administration and overseen by then vice - president biden , will be rebooted . 
at the time , congress had authorised us $18 billion in funding for cancer research over a 7 - year timeframe , which expires in 2022 , making next years budget review crucial . 
given bidens support in 2017 for our commission on future cancer research priorities in the usa , we are hopeful that these recommendations will be reprioritised . one of the aims of the cancer moonshot was to provide more treatment options by accelerating cancer research . 
 approval of new drugs , their cost to health systems and patients , and the amount of out - of - pocket expenses versus their efficacy is a long - running and contentious issue . 
a new study , however , has shown that novel drugs approved between 2000 and 2016 to treat the 15 most common cancers prevented 12 million deaths in the usa . 
these results highlight the importance of investing in new cancer treatments and how scientific advancements can pay off on a cumulative basis , even if some drugs provide only small incremental benefits over their predecessors . profit remains a crucial driver of oncology drug development worldwide . 
although the global oncology market is expected to contract by 11% in 2020 compared with 2019 due to covid - 19 - related pauses in drug manufacturing and clinical trials , it is still one of the biggest health - care markets worldwide . 
for example , astrazeneca has projected a 55% increase in thirdquarter earnings this yearmainly due to increased sales of cancer drugs rather than investments related to its vaccine for covid - 19 . 
pharmaceutical companies naturally expect large returns on investment , but a compromise must be reached for fair pricing to ensure all patients with cancer have access to life - saving treatments . 
if ethics is not reason enough to support this notion , recently , it has been shown that us states that expanded medicaid coverage as part of the affordable care act saw significant reductions in mortality in patients with some newly diagnosed cancers compared with that in non - expansion states . 
these results add to the evidence that access to effective cancer drugs can yield long - term benefits to public health . several strategies have been proposed to provide a way to approve drugs based on a more equitable compromise between profits for pharmaceutical companies and afford ability for public and private health insurers , which is a global issue not specific to the usa . 
this year , in a push to expedite access to new cancer drugs in the uk , the institute of cancer research ( icr ) published a consensus statement with suggestions on how to bridge the gap between drug price and patient access . 
although survival outcome - based pricing is also proposed by the american society of clinical oncology and the european society for medical oncology , the icr consensus proposes the use of surrogate endpoints instead of survival to help accelerate drug approvals . 
moreover , the underlying principle behind some of the recommendations is that governments and the pharmaceutical industry must work closely together from the point of drug discovery , and not only when new treatments need approval and market licensing . 
this strategy would allow alignment of interestsincluding funding and regulationsof both parties , which should prioritise patients interests and needs . president - elect biden symbolises a new hope for science - based political decisions and , importantly , the reinstatement of international collaboration , including for previous international funding commitments and re - engagement with who . 
we hope to see data - driven decision - making and consensus on fair drug prices that will help overcome the long - term consequences of public health and financial crises . 
in this fight , public and private parties must not be on opposite sides of the barricade , rather they must work together to achieve the best outcomes for patients with cancer . 
 the lancet oncology for more on the cancer moonshot initiative see initiatives / moonshot - cancerinitiative for the lancet oncology commission see thelancet.com / commissions / usa - oncology for more on improved outcomes due to novel cancer drugs see j med econ 2020 ; published online nov 9 . 
lazertinib in patients with egfr mutation - positive advanced non - smallcell lung cancer : results from the dose escalation and dose expansion parts of a first - in - human , open - label , multicentre , phase 12 study . 
olanzapine 5 mg plus stand ard antiemetic therapy for the prevention of chemotherapy - induced nausea and vomiting ( j - force ) : a multicentre , randomised , double - blind , placebocontrolled , phase 3 trial . 
tumour treating fields in combination with pemetrexed and cisplatin or carboplatin as first - line treatment for unresectable malignant pleural mesothelioma ( stellar ) : a multi centre , single - arm phase 2 trial . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 26170 drilon a , siena s , dziadziuszko r , et al . 
 lancet oncol 2020 ; 21 : 26170in the results section of this article , the median treatment duration for patients with cd74ros1 fusions should have been 146 months ( iqr 72181 ) and the median intracranial progression - free survival in 20 patients with cns disease should have been 77 months ( 95% ci 38193 )  . 
 lancet oncol 2019 ; 21 : 27182in the statistical analysis section of this article , the overall safety - evaluable population should have included safety data from the paediatric phase 1 study startrk - ng patients aged 4920 years . 
this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . correction to lancet oncol 2020 ; 21 : e10 f i e l d s tr e a t i n g ceresoli gl , gianoncelli l , grosso f , on behalf of stellar investigators . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 22232 strm p , kartasalo k , olsson h , et al . 
 this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . vol 21 february 2020 corrections corrections correction to lancet oncol 2014 ; 15 : 1280 correction to lancet oncol 2014 ; 15 : 310 , 311 boughey jc . 
how do the amaros trial results change practice ? lancet oncol 2014 ; 15 : 128081the last sentence of the fourth paragraph of this comment should read with both the amaros1 and z00112 , 3 studies , the data interpreted should be with caution and should not be extrapolated to patients with three , four , or more positive sentinel lymph nodes . 
this correction has been made to the online version as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e395403 weller m , van den bent m , hopkins k , et al , for the european association for neuro - oncology ( eano ) task force on malignant glioma . 
 lancet oncol 2014 ; 15 : e395403 the appendix of this review was incorrect ; the correct appendix has been uploaded as of nov 24 , 2014 . correction to lancet oncol 2014 ; 15 : e591 furlow b . 
 this correction has been made to the online article as of nov 24 , 2014 . conroy t , galais m - p , raoul j - l , et al , for the fdration francophone de cancrologie digestive and unicancer - gi group . 
de nitive chemo radiotherapy with folfox versus uorouracil and cisplatin in patients with oesophageal cancer ( prodige5 / accord17 ) : final results of a randomised , phase 2 / 3 trial . 
the last sentence of the eighth paragraph in the results section should read an endoscopic complete response at week 15 was achieved in 61 ( 53% ) of 115 patients in the folfox group versus 57 ( 48% ) of 120 patients in the uorouracil plus cisplatin group . 
folfox = uorouracil , leucovorin , and oxaliplat recist = response evaluation criteria in solid tumours.21 * 115 patients assessable in the folfox group and 120 assessable in the uorouracil and cisplatin group . table 2 : tumour response to treatment correction to lancet oncol 2014 ; 15 : 1464 sestak i , singh s , cuzick j , et al . 
changes in bone mineral density at 3 years in postmenopausal women receiving anastrozole and risedronate in the ibis - ii bone substudy : an international , doubleblind , randomised , placebo - controlled trial . 
this review summarises the present understanding of how mirnas operate at the molecular level ; how their dysregulation is a crucial part of tumour formation , maintenance , and metastasis ; how they can be used as biomarkers for disease type and grade ; and how mirna - based treatments could be used for diverse types of malignancies . introduction micrornas ( mirnas ) are small non - coding rnas ( 2123 nucleotides ) encoded in the genome of plants , invertebrates , and vertebrates . 
these small molecules mainly bind imperfectly to the 3 untranslated region of target messenger rnas ( mrnas ) .1 they negatively regulate gene expression post - transcriptionally by inhibiting translation and causing degradation of target mrna . 
additionally , they are key regulators in many diseaseseg , neurological disorders , heart disease , vascular diseases , viral infection , and cancer.1 the discovery of mirnas led to a worldwide research e ort to establish their roles in cancer . 
 mirnas regulate molecular pathways in cancer by targeting various oncogenes and tumour suppressors , 1 and have a role in cancer - stem - cell biology , angiogenesis , the epithelialmesenchymal transition , metastasis , and drug resistance . 
because mirna - based regulation is dependent on expression of its mrna targets , which are not always ubiquitously expressed , an mirna can have e ects speci c to cells types and conditions . researchers are beginning to uncover the complex role that mirnas have in malignant disease . 
 importantly , this knowledge could be used in the development of anticancer therapies . invaluable regulation of cancer pathways gene regulation and mutations in 2002 , the rst report about the role of mirnas in cancer established that the gene cluster containing the mirnas mir - 15 and mir - 16 is deleted in most people with chronic lymphocytic leukaemia ( cll ) .2 further studies have shown that mir - 15 and mir - 16 act as tumour suppressors by targeting the oncogene bcl2 , which encodes a protein involved in cell survival.3 conversely , mir - 21 is an excellent example of an oncogenic mirna ( a so - called oncomir )  . 
it is overexpressed in most cancerseg , breast cancer , colorectal cancer , lung cancer , pancreatic cancer , glioblastoma , neuroblastoma , leukaemia , and lymphoma.47 overexpression of this mirna can cause tumour growth , maintenance , and survival in vivo.8 importantly , these tumours are completely dependent on expression of mir - 21.8 mir - 21 targets several tumour - suppressor genes , including pten , to increase proliferation and decrease apoptosis.9 , 10 mir - 21 could also promote tumour migration by targeting pro - invasion genes.11 modulation of mirna expression is increasingly thought to be an important mechanism by which tumoursuppressor proteins and oncoproteins exert some of their e ects . 
the proto - oncogene myc transcriptionally activates the mir - 17 - 92 clustera polycistronic transcript of mirnas 17 , 18a , 19a , 20a , 19b - 1 , and 92a - 1.12 the oncogenicity of mir - 17 - 92 is attributed mainly to mir - 19 , which inhibits pten to activate akt signalling and promote cancer - cell survival ( gure 2 ) .13 myc also represses transcription of many tumour - suppressor mirnas , including the let - 7 family.14 reduced expression of let - 7 mirnas is recorded in many cancers , 1 and correlates with poor survival . 
let - 7a , let - 7c , and let - 7g are deleted in lung cancer tumours , and many mirnas of the let - 7 family are located in the genomic region frequently deleted in patients with lung cancer.15 involved the tumour suppressor p53 transcriptionally induces the mir - 34 family of mirnas in response to dna damage ( gure 2 )  . 
mir - 34a is expressed from one genomic site , but mir - 34b and mir - 34c are produced together from one primary transcript at another site.16 , 17 loss of mir - 34a expression is associated with metastasis and recurrence of prostate cancer.18 restoration of mir - 34 in pancreatic cancer cells substantially expression inhibited clonogenic cell growth and invasion , induced vol 13 june 2012 e249 review oncogenic mirnas tumour - suppressing mirnas additionally , genetic variation in the mir - 221 binding site in the 3 utr of kit is associated with a heightened risk of acral melanoma.24 mutations loss of function mutations loss of function oncogenic mirna tumour - suppressing mirna tumour - suppressor mrna oncogene mrna mirna resistance mirna resistance tumour - suppressor mrna oncogene mrna upregulation more transcription gene amplication hypomethylation downregulation less transcription genomic deletion hypermethylation tumour - supressor mrna tumorigenesis oncogene mrna figure 1 : regulation of tumorigenesis by mirnas tumorigenesis can be regulated by mirnas at di erent levels . 
upregulation of oncogenic mirnas reduces expression of tumour - suppressor protein , but downregulation of tumour - suppressing mirnas results in an increased production of oncogenic proteloss - of - function mutations in tumour - suppressing mirnas and mutation of the target section of oncogene mrna can cause tumorigenesis , because expression of oncogenic proteins is no longer regulated . 
similarly , studies of prostate cancer stem cells show that reintroduction of mir - 34a into tumours and cancer cell lines leads to corresponding reductions of cd44 and tumour size.19 expression of mir - 34b and mir34c is lost through deletion or hypermethylation , or is downregulated , in 90% of colorectal cancers.20 , 21 in their absence , both p53 - dependent and p38 - mapk - dependent responses to dna damage are attenuated , leading to oncogenesis.21 , 22 importantly , myc is a target of mir - 34b and mir - 34c , substantiating the inter connected nature of mirna expression in malignancies ( gure 2 )  . gene regulation is not the only way in which mirnas are implicated in malignancies ( gure 1 )  . 
for example , a single nucleotide polymorphism in the 3 utr of the kras oncogene signi cantly increases risk of non - small - cell lung cancer.23 cancer stem cells cancer stem cellsalso called tumour - initiating cells are a small population of cells within a tumour that are thought to arise from somatic stem cells . 
they have enhanced self - renewal capacities , tumorigenic potential , and expression of unique surface markers ; 25 and are often essential for tumour maintenance , treatment resistance , tumour progression , and distant metastasis . 
some mirnas involved in stem - cell regulation are mir - 296 , mir - 134 , mir - 470 , and the mir - 34 family , which targets genes essential for pluripotency and stem - cell function ( eg , oct4 , nanog , sox2 , notch , and bcl2 ) .26 let - 7 in vitro and regulation of cancer stem cells . 
 in breast cancer , let - 7 and mir - 30 are important for the downregulated in breast - cancer stem cells.27 when overexpressed in mice , it can reduce numbers of undi erentiated cells inhibit cell proliferation , tumour formation , and metastasis.28 mir - 30 expression is also low and can inhibit the selfrenewal ability of breast - cancer stem cells . 
the combination of both inhibits self - renewal and mammosphere formation in breast - cancer stem cells.28 let - 7 and mir - 30 angiogenesis promotion of angiogenesis by tumours necessitates activation of proliferation and migration pathways in vascular smooth muscle cells . 
in nasopharyngeal carcinoma cells , the mir - 15a / 16 - 1 cluster regulates angiogenesis ( gure 3 ) by targeting the angiogenic factors vegfa and met.29 mir - 145 blocks migration of vascular smooth muscle cells by inhibiting fli1 , 30 and mir - 143 by targeting the versican protein involved in migration induced by platelet - derived growth factor.31 the mir - 143 cluster is downregulated in cancers of the prostate , colon , gastric , and bladder , and in cll and b - cell lymphomas.32 transition the epithelialmesenchymal epithelialmesenchymal transition and metastasis epithelial cells undergo several molecular changes during assume a mesenchymal cell phenotype necessary for tumour metastasis and progression ( gure 3 ) .33 expression of e - cadherin ( cdh1 ) is essential for retaining an epithelial cell type . 
similarly , expression of mir - 200 in breast cancers is positively correlated with concen trations of e - cadher the e250 vol 13 june 2012 review importance of this association is supported by evidence that restoration of mir - 200 expression is su cient to reverse the transition ( ie , mesenchymal to epithelial ) in a kidney - derived cell line.34 however , other mirnas are needed epithelialmesenchymal the transition . 
in pancreatic epithe lial cells , the expression of mirnas from the mir - 30 family inversely correlates with the mesenchymal pheno type.35 in mesenchymallike ovarian cancer cell lines , overexpression of mir429 reverses the transition.36 to prevent the to supplement clinical potential diagnosis and classi cation the development of cytogenetic , immunological , and traditional molecular methods morphological classi cation systems has re ned the identi cation of cancer subtypes.37 for instance , transcriptome pro ling studies of di erent cancer types with large - scale genomic approaches showed that a 97 - gene expression pro le is better for classi cation of breast cancer histological grade than are lymph - node status and tumour size.37 gene - expression pro ling has also led to development of breast - cancer prognostic pro ling tests , which have been approved for clinical use.38 as with mrna , whole - genome mirna pro ling has shown that mirna expression changes substantially in most human cancers.39 mirna expression signatures provide a more accurate method of cancer subtype classi cation than does expression pro ling of an entire group of known protein - coding rnas.40 mirna pro les can contribute to the diagnostic and prognostic classication of human malignancies ( table ) .2 , 4148 the use of the traditional , gold standard , histological examination in the diagnosis and classi cation of cancers can be limited by availability of adequately preserved tissue and the possibility of subjective interpretation by pathologists . 
by contrast , mirnas show resistance to degradation and their expression levels can be established in a few hours with as little as 10 ng of total rna ; therefore , mirnas are ideal as both diagnostic and prognostic indicators in clinical settings . screenings of resected tumours and biopsy samples have identi ed mirna signatures that can be used to di erentiate between malignant and benign condi tions in several organs . 
seven mirnas are di erentially expressed in biopsied pancreatic ductal adenocarcinomas compared with benign and healthy tissues.49 a multi centre trial50 showed that use of signatures from these mirnas gives greater accuracy than does conventional cytology . 
one mirna was overexpressed in 19 of 20 malignant samples.51 mirna expression can also be used to identify well characterised genotypeseg , to distinguish between dna damage drosha mir - 34 carcinogenesis mirna processing mir - 17 - 92 cluster pten figure 2 : oncogenic and tumour - suppressing mirnas in the dna damage response dna damage can lead to the upregulation of the mir - 34 family through the activation of the p38 map - kinase and p53 pathways . 
 vol 13 june 2012 e251 review these two mirnas are deleted or down regulated in 68% of patients with cll.2 furthermore , cll can be classi ed into ve di erent categories according to genetic instabilities ( deletion of chromosomal regions 11q , 13q , and 17p ; trisomy 12 ; and normal karyotype )  . 
studies show that the speci c expression pattern of 32 individual mirnas can di erentiate between these di erent chromosomal abnormalities ( table ) .42 other forms of genomic instability can be inferred with mirna pro ling ( table )  . prognostic indicators many identi ed genotypes are associated with distinct prognoses ( table )  . 
by comparing two main groups of patients with good prognosis ( low zap70 expression , mutated immunoglobulin variable region genes ) and poor prognosis ( high zap70 , immunoglobulin variable region genes not mutated ) , they identi ed 13 mirnas with variable expression according to prognosis ( table ) .41 prognosis or outcome microrna expression reference chronic lymphocytic leukaemia high zap70 ; immunoglobulin variable region not mutated poor 13q14.3 deletion indolent 17p deletion aggressive calin41 calin2 visone42 mir - 15a mir - 16 - 1 mir - 16 - 2 mir - 195 mir - 221 mir - 23b mir - 155 mir - 24 - 1 mir - 146 mir - 223 mir - 29a - 2 mir - 29b - 2 mir - 29c mir - 15a mir - 16 - 1 mir - 130b mir - 129 - 3p mir - 632 mir - 768 - 5p mir - 638 mir - 453 mir - 29b / c mir - 181b / c / d mir - 342 - 3p mir - 223 mir - 181a mir - 367 mir - 205 mir - 96 mir - 182 mir - 183 down down down down down down down down down down down down disease progression mir - 181 visone42 trisomy 12 lung cancer non - squamous non - small - cell lung cancer ( stages ii , iii , and iv ) and lymph - node metastasis poor lebanony43 zhu44 zhu44 zhu44 ( continues on next page ) in lung cancer , researchers focusing on the mir - 183 family of mirnas ( mir - 183 , mir - 182 and mir - 96 ) have recorded a link between the expression of these mirnas and progression of non - small - cell lung cancer . 
expression of the mir - 183 family can also help to identify tumours with heightened lymph - node metastasis ; an increased likelihood of progression to stage ii , iii , or iv ; and poor survival ( table ) .44 many biomarkers are prognostic indicators for breast cancer . 
the two most common are the oestrogen receptor , expression of which predicts a good outcome ; and her2 , which when over expressed is associated with poor outcome , anti - oestrogen treatment resistance , and metastasis.53 although identi cation of these two markers has been invaluable for breast cancer management , other molecular methods are needed for classi cation of subtypes . 
analysis of 93 breast - cancer samples showed that speci c patterns of mirna expression were associated with breast - tumour subtypes of di erent clinical outcomes.45 one investigation45 showed that expression of 31 mirnas was signi cantly associated with clinical factors . 
14 were overexpressed in grade iii , oestrogen - receptor - negative malignancies of basal - like subtype , seven of which were also associated with her2 - overexpressing cancers.45 import antly , six were related to the same clinical outcomes in another independent dataset ( table ) .46 although the expression pattern of several mirnas can give useful information about stage and prognosis , one mirna alone can have accurate predictive power . 
 the predictive e ect of mir - 210 was so strong that the researchers noted that the overexpression of mir - 210 alone allowed prediction of prognosis to the same level as a 76 - gene mrna signature test ( gene76 )  . 
overexpression of mir - 210 is associated with an increased risk of recurrence and a reduced chance of relapse - free survival.46 in cll with trisomy 12 , when expression of immuno globulin variable region genes and zap70 does not predict clinical outcome , the overexpression of one mirna , mir - 181 , can predict disease progression ( table ) .42 to colorectal cancers resistant mirna pro ling can identify treatment - resistant cancers . 
as with overexpression of her2 in breast cancer , overexpression of four mirnas have been linked to egfr antagonists.48 screening for mirnas could enable treatment to be tailored to individual patients and thus increase the chances of survival . 
urine cytology of speci c markers can also be used but this method does not have the sensitivity biomarkers in body uids although mirna pro ling of tumours could be an excellent prognostic test , invasive procedures such as biopsy , aspiration biopsy , or excision surgery of alreadyexisting tumours are necessary to obtain samples . 
an ideal biomarker should be accessible with non - invasive methods , sensitive enough to detect early presence of tumours before clinical symptoms present , and absent or low in healthy , tumour - free individuals.54 stable , degradationresistant , extracellular mirnas could be detected in body uids such as serum , urine , saliva , tears , breast milk , seminal uid , and faecal matter . 
one breast cancer study comparing the circulating mirna pro le in healthy women with that of those with early - stage breast cancer62 showed that downregulation of mir - 181a and mir - 1304 is associated with the disease . 
mir - 195 and let - 7a concentrations are higher in the plasma of patients with breast cancer than in healthy individuals.62 after tumourexcision surgery , postoperative serum concentrations of both these mirnas return to values reported in the healthy control group.59 researchers investigating the plasma levels of mirnas in 74 patients diagnosed with di erent types of lung cancer63 identi ed three mirnas ( mir - 155 , mir - 197 , and mir - 182 ) that were at a higher concentration in patients with cancer than in control individuals . 
 the serum the investigators also reported that vol 13 june 2012 e253 review for detection of low - grade bladder cancer , 64 driving the search for new speci c and sensitive biomarkers . 
 a proof - of - concept study65 showed that mir - 126 , mir - 182 and mir - 199a concentrations are signi cantly increased in the urine of patients with stage 1 bladder cancer , as well as in those with stage 2 and stage 3 disease . 
 the concentration of these markers in urine continues to increase as malignancy progresses and decreases after tumour - excision operations.65 for those with a positive for colorectal cancer , patients older than 60 years are o ered screening every 2 years with non - invasive faecal occult blood testing , 66 with a subsequent colonoscopic result . 
 investigation unfortunately , the test has only 3350% sensitivity ; use of novel biomarkers would prevent many healthy individuals undergoing an expensive , painful procedure with the risk of serious medical complications.67 mir - 21 and mir - 106 are upregulated in the stool of patients with colorectal neoplasia ( colorectal cancer or adenoma )  . 
mir144 * is increased in the faeces of patients with colorectal cancer with a sensitivity of 74% and a speci city of 87% , and is thus another potential biomarker to help diagnosis of colorectal cancer.68 samples extracted with the faecal blood - test kits could also be used to extract mirnas ; clinicians could undertake both tests simultaneously to increase the sensitivity of diagnosis.67 mirnas as cancer treatment the development of new treatments has contributed substantially to increased 5 - year survival and the reduction in overall mortality rates.62 , 69 however , although the classi cation of cancers has become increasingly diver si ed , the variety and speci city of treatment options has lagged behind . 
more than 2000 gene - therapy - based clinical trials are in progress for various illnesses , but only one is of mirna treatment.32 treatment can be targeted to mirnas in two ways : mirna reduction and mirna replacement ( gure 4 )  . 
new mirna - based treatments would need to have selective and accurate delivery of the agents to the target tumours to increase the therapeutic potential and reduce possible side - e ects . two major di culties have impeded development of mirna - based treatments . 
first , rna has low stability in vivo ; mirna introduced into mice via the tail vein is cleared from the circulatory system in 30 min.70 unmodi ed , saline - formulated , double - stranded rna injected intravenously undergoes rnase - mediated degradation and rapid renal excretion . 
an increase could be achieved by improved mirna stability or by protection from rna - hostile environments . substitution of phosphodiester by phosphorothioate in the rna backbone , and of the ribose moieties to 2 - o - methyl or other 2 substitutions confer substantial nuclease resistance.71 locked nucleic acid ( lna ) is a modi ed rna nucleotide that has an extra bridge connecting the 2 oxygen and 4 carbon . 
these modi cations increase the thermostability of lna - rna duplexes , increase target speci city , and are resistant to exonucleases and endonucleases , thereby improving stability of mirnas in vitro and in vivo.72 finally , introduced rna can be conjugated to a cholesterol moiety , increasing stability in the circulation . 
for example , an antagonist of mir - 16 with 2o - methyl modi ed nucleotides and cholesterol linked to its end via a hydroxyprolinol linkage is stable and e ciently silences mirna expression.73 protection from hostile environ ments is typically achieved by encasing of lna or mirna mimics in nanoparticles to form micelle - like structures ( gure 4 )  . the second di culty is how to ensure tumour - speci c delivery and retention of mirnas . 
e orts to achieve targeted delivery could be further hindered by rst - pass metabolism and rapid localisation of small molecules delivered systemically to the kidney and liver.74 targeted delivery to speci c tissues can be done when tumour - speci c ligands are linked to nanoparticles , which can be directed to tumour cells via active or passive targeting . 
nanoparticles between 15 nm and 100 nm are the best for systemic delivery.76 active targeting of nanoparticles necessitates their conjugation with di erent compounds that have a speci c a nity to tumours . 
various cancer - associated cell - surface proteins ( eg , her2 , 77 egfr , 78 and ca - 12579 ) and hyaluronic acid80 could potentially be used for this conjugation . 
investigators have developed a poly ( ethylene glycol ) hyaluronic acid nanoparticle ( p - ha - np ) that can be used to deliver doxorubicin and camptothecin to mouse cells.81 the nanoparticles were internalised successfully into cancer cells ( scc7 and mda - 3t3 ) , but rarely taken up by normal broblasts ( nih - 3t3 )  . 
tumour - bearing mice were systemically treated with camptothecin de livered with p - ha - np , and tumour growth was success fully stopped for at least 35 days . 
these nanoparticles could e254 vol 13 june 2012 review mirna modied rna target mrna nanoparticle antibody cancer - specic ligands cell membrane figure 4 : mirna - based treatment in mirna reduction treatment ( a ) , single - stranded lna molecules ( anti - mirnas ) bind to mirnas complementarily , preventing the mirnas from binding to target mrnas . 
 possibly be modi ed to carry mirnas to speci cally targeted cancer stem cells.81 furthermore , integrin - - 3 - targeted nanoparticles used to deliver anti - mir - 132 had promising results in inhibition of angiogenesis and breast tumour metastasis.82 the goal of mirna replacement is the reintroduction of mirnas depleted in cancer cells and the reactivation of cellular pathways that drive a therapeutic response . 
 trang and co - workers70 concluded that a chemically synthesised mir - 34a packaged into a lipid - based delivery vehicle and given locally or systemically could block tumour growth in mouse models of non - small - cell lung cancer . 
systemic delivery of formulated mir - 34a did not induce a rise in cytokines or liver and kidney enzymes in serum , suggesting that the formulation is well tolerated and that side - e ects could be negligible . 
similar results were noted in another study of a mouse model of non - smallcell lung cancer with activated kras ; 70 an mir - 34a or let - 7 mimic mirna formed a complex with a neutral lipid emulsion , which led to a 60% reduction in tumour area.70 additionally , systemic delivery of atelocollagenconjugated mir - 16 in a mouse xenograft model of prostate cancer inhibited metastasis into bone.83 mirna reduction with lna has been done with antimir - 21 to treat autoimmune splenomegaly in mice with systemic lupus erythematosus ; 84 mir - 21 is upregulated in all subsets of lupus mouse lymphocytes . 
targeting of mir - 21 with an intraperitoneally injected lna - based antagonist decreases manifestation of cardinal systemic lupus erythematosus and leads to the reversal of splenomegaly.84 the only mirna - based treatment tested in people is anti - mir - 122 for the treatment of infection with hepatitis c virus ( hcv )  . 
mir - 122 is an essential mirna for hcv replication and is predominantly in the liver.85 in 2010 , data from a drug trial of an intravenously delivered lna to remove mir - 122 and stop infection in chimpanzees was reported.86 lna given to chronically infected chim panzees once a week for 12 weeks led to a reduction in viral load in the serum and the liver . 
a phase 1 trial87 in 77 healthy volunteers established that anti - mir - 122 is safe and vol 13 june 2012 e255 review search strategy and selection criteria data for this review were identi ed by searches of pubmed with the term microrna in combination with cancer , in vivo , circulating , systemic delivery , therapeutics , or lna . 
the subsequent phase 2a trial87 assessed the safety and antiviral activity of subcutaneous anti - mir - 122 given at doses of 3 mg / kg , 5 mg / kg , and 7 mg / kg every week for 29 days ; patients were followed up until week 18 . 
this trial87 drew attention to the potential of lnas for cancer treatment . conclusion the discovery of mirnas has changed the way control of gene expression is thought about and , perhaps more importantly , has set a precedent for the development of new diagnostic methods and treatments of diseases , including malignancies . 
in the long term , work to identify major mirna targets and to develop safe and speci c methods of delivery of mirna - based treatments could allow modulation of mirnas to become a central feature of cancer treatment and management . contributors ywk and df - m did the literature search , wrote and edited the report , and designed the gures . 
mb wrote and edited the report . con icts of interest ywk and mb have led a patent relating to microrna delivery with nanoparticles conjugated to cancer - targeting anti - cd4 antibodies . 
we thank ania wilczynska and samantha johnston for reading and commenting on this review . comment information about non - speci c side - e ects from providers and written material , such as those on consent forms and labels , without consideration of the nocebo e ect . for this model to work on behalf of patients , the risks and bene ts of a speci c treatment have to be completely unrelated to the act of information disclosure to the patient.8 although this notion might be true for some treatments , it is not uniformly applicable . 
with surgery , the outcome of treatment is more likely to be related to patient anatomy and surgical technique and less likely to be a ected by information exchange during the consent process . 
for example , a patient who develops insulin de ciency after undergoing surgery for pancreatic cancer can be counselled quite objectively that this risk is likely to manifest on the basis of the size of the tumour and location within the pancreas and is unlikely to be a ected by the act of disclosure of this risk to the patient before surgery . 
 for patients with cancer who undergo non - invasive treatments or are prescribed drugs associated with non - speci c side - e ects , the act of disclosure itself could a ect the possibility of side - e ect manifestation . 
 rather , in many clinical circumstances in which the potential for non - speci c side - e ects is high , such as in the non - invasive treatment of cancer , the act of information disclosure could be more accurately viewed as part of the riskbene t analysis , thus dependent on real - time discussion , and personalised to the patient . 
theor med bioeth 2011 ; 32 : 22943 . published online november 16 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70332 - 1 errata adams c , torode j , henshall s , cazap e , ryel al , grey n . 
lancet oncol 2011 ; 12 : 109192in this comment , the fourth sentence of the third paragraph should have read : who has committed to produce targets for its so - called best - buy interventions in time for the world health assembly in 2012 . 
we aimed to assess whether exposure to ionising radiation through mammography screening was associated with risk of breast cancer in brca1 or brca2 mutation carriers . methods we identi ed 1600 cases of breast cancer and 1600 controls without breast cancer who were matched for brca mutation , date of birth ( within 1 year ) , and country of residence from an international registry of brca1 and brca2 mutation carriers . 
 results we found no association between ever having screening mammography and risk of breast cancer ( odds ratio [ or ] 103 [ 95% ci 085125 ] , adjusted for parity , oral - contraceptive use , ethnic origin , and bilateral oophorectomy )  . 
 the association was much the same for brca1 mutation carriers and brca2 mutation carriers ( 104 [ 084129 ] vs 106 [ 067166 ] , respectively , adjusted for parity , oral - contraceptive use , ethnic origin , and bilateral oophorectomy )  . interpretation these ndings do not lend support to the idea that exposure to ionising radiation through routine screening mammography contributes substantially to the burden of breast cancer in brca1 and brca2 mutation carriers . 
prospective studies are needed to con rm the results of this initial report , and , where possible , these studies should assess a more appropriate endpoint of total exposure . introduction women with a germline mutation in brca1 or brca2 have increased risks of developing breast and ovarian cancer . 
because the risk of breast cancer rises substantially from age 25 years and peaks between age 3050 years , some researchers1 , 2 recommended that screening should start early ( ie , at age 25 years )  . 
current methods of screening for breast cancer include mammography , ultrasonography , clinical examination , and mri.3 at present , mammography is the most widely used imaging modality . screening mammography is associated with a small dose of radiation to the breast . 
this dose is not thought to be high enough to increase the risk of breast cancer in the general population , but women who are at increased genetic risk might be particularly sensitive to the dnadamaging e ects of ionising radiation.46 hereditary breast cancer typically occurs at a young age ( ie , women in their thrities and forties ) , and brca1 and brca2 have a role in the repair of dna damage.7 , 8 these two proteins help repair double - strand dna breaks , which are characteristic of lesions induced by ionising radiation . 
radiation is an established risk factor for early - onset breast cancer in the general population , 911 although exposure levels associated with this risk are many times greater than that associated with screening mammography . 
we aimed to assess whether screening mammography was associated with risk of breast cancer in brca1 and brca2 mutation carriers . methods participants women with a brca1 or brca2 mutation were identi ed through a registry of mutation carriers , which was located at the centre for research on womens health , university of toronto , ontario , canada . 
data for these women were gathered from women with known pathogenic brca1 and brca2 mutations during genetic counselling and mutation testing at 44 centres in six countries in north america , europe , and israel . 
when a mutation in brca1 or brca2 was found in a proband or in her relative , genetic testing was o ered to other at - risk women in her family . 
mutations were identi ed by use of various techniques during the course of genetic testing , but all 402 vol 7 may 2006 articles abnormal nucleotide sequences were con rmed by direct sequencing of dna . 
 from april 26 1992 , to july 12 2005 , data were submitted to the registry for 4951 women with a brca1 or brca2 mutation and with information on history of mammography , including age at rst mammography . 
41 women were excluded because they were diagnosed with ovarian cancer or any other cancer before diagnosis with breast cancer ; 165 women were excluded because they had had three women were prophylactic mastectomy ; and excluded because of missing data for important variables . 
 after exclusions , there were 4742 eligible brca mutation carriers2181 women with breast cancer ( ie , cases ) and 2561 women without breast cancer ( ie , con trols )  . 
cases and controls were matched for date of birth ( within 1 year ) , brca mutation ( brca1 vs brca2 ) , and country of residence ; matching was done by ps using a computer prograthe control could not have been diagnosed with any cancer before the age of diagnosis of breast cancer for the case . 
for this study , questionnaires were excluded if age at breast - cancer diagnosis or age at rst mammography were missing . the questionnaire inquired about whether participants had ever had screening mammography , and , if so , the age at which they rst had the procedure ; and about the total number of mammography procedures they had had in their lifetime ( ie , until the date of questionnaire completion )  . 
because of the di culty in distinguishing between screening mammography and diagnostic mammography for cases , we restricted our analyses to the rst mammography that took place at least 1 year before the year of diagnosis of breast cancerie , a mammography procedure was excluded from analyses if it was reported to have occurred in the same calendar year as breast - cancer diagnosis or in the year before breast - cancer diagnosis . 
information on cancer diagnoses were obtained from the questionnaire . information for family history was derived from pedigrees , which were drawn by research personnel at every centre ; pedigrees were sent to the study centre in toronto with , but separate from , questionnaires . 
 statistical analyses we analysed age at rst mammography for every case and matched control by classifying women into three age - groups : 30 years or younger ; 3140 years ; and 41 years age ( years ) median ( range ) year of birth year ( range ) mutation brca1 brca2 parity mean ( sd ) nulliparous oral contraceptives bilateral oophorectomy country of residence ever use ever usa canada poland norway israel austria ethnic origin jewish french - canadian other white other controls ( n = 1600 ) cases ( n = 1600 ) 467 ( 214832 ) 473 ( 189826 ) 011 * 1953 ( 19151981 ) 1953 ( 19151980 ) matched 1260 ( 79% ) 340 ( 21% ) 20 ( 14 ) 288 ( 18% ) 1260 ( 79% ) 340 ( 21% ) 20 ( 13 ) 249 ( 16% ) 945 ( 59% ) 941 ( 59% ) 76 ( 5% ) 51 ( 3% ) 520 ( 33% ) 474 ( 30% ) 461 ( 29% ) 71 ( 4% ) 50 ( 3% ) 24 ( 2% ) 330 ( 21% ) 128 ( 8% ) 1119 ( 70% ) 23 ( 1% ) 520 ( 33% ) 474 ( 30% ) 461 ( 29% ) 71 ( 4% ) 50 ( 3% ) 24 ( 2% ) 271 ( 17% ) 145 ( 9% ) 1144 ( 72% ) 40 ( 3% ) matched 03 * 007 09 002 matched 001 family history of breast cancer one or more rst - degree relatives with breast cancer 803 ( 59% ) 764 ( 57% ) || 037 data are number ( % ) , unless otherwise stated ; data might not add to 100% because of rounding . 
 * adjusted for parity , oral - contraceptive use , bilateral oophorectomy , and ethnic orig table 2 : association between age of rst mammography and risk of breast cancer for all women and by brca mutation , age at breast - cancer diagnosis , and cancer not identi ed by mammography or older . 
because ionising radiation is thought to be a risk factor for early - onset breast cancer in particular , analyses were repeated after strati cation of cases by age of diagnosis ( 40 years vs > 40 years )  . 
furthermore , because the intensity of screening mammography might a ect the age of breast - cancer diagnosis ( ie , women who have regular screening might have breast cancer diagnosed earlier than women who do not participate in a screening programme ) , we did a subgroup analysis of cases with breast cancer diagnosed by procedures other than mammographyie , by self - examination or physician examination . 
 role of the funding source the sponsor of this study had no role in the study design ; in the collection , analysis , or interpretation of the data ; or in the writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results table 1 shows the characteristics of the 1600 cases and 1600 matched controls . 
controls were signi cantly more likely to have had bilateral oophorectomy than were cases , but only 127 ( 4% ) of all participants had had a bilateral oophorectomy before the age of breast - cancer diagnosed in the case . 
we did not receive a pedigree for all participants for whom a questionnaire was available : detailed family history was available for 2706 ( 85% ) participants : 1367 ( 85% ) cases and 1339 ( 84% ) controls . 
 the mean age of breast - cancer diagnosis in cases was 405 years ( 81 ) for brca1 mutation carriers and 418 years ( 80 ) for brca2 mutation carriers . 
199 ( 12% ) cases were diagnosed by screening mammography , and 1281 ( 80% ) were diagnosed by other procedures ( usually palpation of a mass by physician or self - examination ) ; 120 ( 8% ) cases did not have information for method of diagnosis because of missing data or diagnosis by more than one method . 
 more brca2 mutation carriers were diagnosed by 404 vol 7 may 2006 articles mammo graphy compared with brca1 mutation carriers ( 77 [ 23% ] of 340 vs 122 [ 10% ] of 1260 , p < 00001 )  . 661 ( 41% ) cases and 729 ( 46% ) controls had at least one screening mammography procedure 1 year or more before the calendar year in which the case was diagnosed . 
 mean age at rst screening mammography was 353 years ( sd 78 ) for cases and 355 years ( 80 ) for controls ( p = 070 , t test )  . 
201 ( 13% ) cases and 234 ( 15% ) controls rst had mammography at age 30 years or younger ; 342 ( 21% ) cases and 355 ( 22% ) controls rst had mammography at age 3140 years ; and 118 ( 7% ) cases and 140 ( 9% ) controls rst had a mammography at age 41 years or older . 
for 760 ( 48% ) of the 1600 matched pairs , the case had her rst mammography at a younger age than the control ; for 706 ( 44% ) matched pairs , the control had her rst mammography at a younger age than the case ( p = 016 , t test ) ; and for 134 ( 8% ) matched pairs , the case and control had the same age at rst mammography or neither had mammography . after rst mammography , controls had a mean of 64 mammography procedures ( sd 038 ) every 10 years . 
 the frequency of mammography was much the same for controls who initiated the procedure in their thirties ( mean 67 [ 037 ] every 10 years ) and those who initiated it in their forties ( 68 mammograms [ 038 ] every 10 years )  . table 2 shows the association between age at rst mammography and risk of breast cancer for all women and for subgroups . 
the associations were much the same for subgroups with brca1 and brca2 mutations , and for those who were diagnosed at age 40 years or younger and at older than 40 years ( table 2 )  . 
 initiation of mammography in the thirties was associated with diagnosis of breast cancer at age 40 years or younger ( table 2 ) , but no association was noted for earlier initiation of mammography ( ie , at age 30 years , table 2 )  . 
subgroup analysis that excluded the 199 cases and their matched controls who had breast cancer identi ed by mammography showed no association between mammography and risk of breast cancer for women who had a breastcancer diagnosis by methods other than that of mammography . 
subgroup analysis showed that initiation of mammog raphy at age 3140 years was associated with an increased risk of breast - cancer diagnosis before age 40 years ; however , this nding might be due to chance . 
 we did a large study of 1600 matched pairs , and , on the basis of the 95% ci , were able to exclude an overall increase in risk associated with ever having mammography of higher than 125 . 
nevertheless , the numbers of women in some subgroups were small , and for women diagnosed with breast cancer before age 40 years , we could not exclude an increase in risk of 155 . we questioned cases and controls on the total number of mammography procedures they had had until the date of questionnaire completion , but we did not record the date of every mammography , only the rst procedure . 
however , in the absence of a comprehensive review of medical records , desticntion between diagnostic mammography ( ie , that initiated in response to an abnormal breast nding ) and screening mammography ( ie , that done only for the purpose of screening ) can be di cult . 
in the study reported here , we excluded all mammography that took place in the same calendar year as diagnosis of breast cancer in cases and controls and those done in the previous year to avoid any potential misclassi cation of screening and diagnostic mammography . 
although a young woman might have mammography only for assessment of a suspicious mass ( eg , a cyst ) , and thus the procedure might not be an indicator of long - term screening behaviour , we expect that such women will be a minority . 
in our study , the mean frequency of this for controls was mammography recommendationone mammography procedure every 19 months , or about 13 mammography procedures over a surveillance period of 20 years . than less a case - control study such as that reported here would be di cult to do in the general population because women at high risk of cancer are more likely to participate in a screening programme than are women at average risk or low risk . 
such selection bias would probably be a particular problem for assess ment of the e ect of early - onset mammography , which is generally recommended only for women at high risk of breast cancer . 
by contrast , self - selection for screening by inherent risk level is probably less important for mutation carriers because the main vol 7 may 2006 articles if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology determinant of risk is the mutation . 
furthermore , self - selection to have early mammography by women with a strong family history of breast cancer would lead to a spurious positive association between mammography exposure and breast - cancer risk , and not to the null nding that we recorded . the possibility of recall bias must be assessed in a casecontrol study . 
 women who have regular screening might be more likely to be diagnosed with breast cancer than unscreened women as a result of intensi ed surveillancea situation that would result in an excess of breast cancer identi ed by screening in the women under close surveillance . 
 therefore , we repeated our analysis on women who did not have cancer identi ed by mammography , and found that these women were not at increased risk of breast cancer . 
furthermore , only 199 ( 12% ) of the 1600 cases reported that the breast cancer was diagnosed as a result of breast - cancer screening . we planned this study on the premise that radiation exposure from a screening mammography might be su cient to raise the cancer risk in women with genetic susceptibility to the disease . 
on the basis of the similarities of radiation - induced breast cancer and hereditary breast cancer , we have previously raised caution that such screening might be hazardous.6 our ndings reported here do not lend support to the idea that brca1 or brca2 mutation carriers are at increased risk of breast cancer after exposure to mammography . 
 other studies12 , 13 of the e ects of radiation exposure in brca carriers have been negativeie , they reported12 , 13 no increase in the risk of second primary ipsilateral or contralateral breast cancer associated with radiotherapy as treatment for a rst breast cancer . 
our data should be reassuring to women and their physicians , and suggest that mammography is not a risk factor for breast cancer in carriers of brca1 or brca2 mutations . 
the decision of whether to o er mammography screening to high - risk women should be based rst on an assessment of the sensitivity of the screening tool and the potential bene ts of early detection in this high - risk group . 
we thank anna tulman and nicole phillips ( centre for research on womens health , university of toronto , ontario , canada ) for data management . con icts of interest we declare no con icts of interest . other members of the hereditary breast cancer clinical study group austriat wagner . canadap ainsworth , a chudley , a eisen , d gilchrist , e lemire , d provencher , w meschino , e warner . israelr gershoni - baruch , e friedman , g rennert . 
 italyb pasini , c bellati . usaf couch , m daly , c eng , d fishman , b karlan , j mclennan , w mckinnon , s merajver , s neuhausen , b pasche , o olopade , m osborne , k sweet , h saal , n tung , j weitzel , m wood . correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2019 ; 20 : 137085 correction to lancet oncol 2020 ; 21 : 137886 glynne - jones r , sebag - montefiore d , meadows hm , et al . 
lancet oncol 2017 ; 18 : 34756the last clause of the last sentence of the first paragraph of the introduction of this article should have read or by giving maintenance chemotherapy after chemoradiotherapy.7 this correction has been made to the online version as of nov 2 , 2020 . motzer rj , rini bi , mcdermott df , et al , on behalf of the checkmate 214 investigators . 
nivolumab plus ipilimumab versus sunitinib in firstline treatment for advanced renal cell carcinoma : extended follow - up of efficacy and safety results from a randomised , controlled , phase 3 trial . 
 lancet oncol 2019 ; 20 : 137085 in this article , supplementary table 1 in the appendix has been updated to correct international metastatic renal cell carcinoma database consortium risk percentage values in patients in the intention to treat group . 
lancet oncol 2020 ; 21 : 137886in table 2 of this article , the reference value for absolute risk reduction of incident gastric cancer over 10 years in indi viduals with an unfavourable life style should have been 0 for low genetic risk , intermediate genetic risk , and high genetic risk . 
these corrections have been made to the online version as of nov 2 , 2020 . vol 21 november 2020 e518 corrections and advisory board and consulting fees from eli lilly ; has received personal fees and held stock as a member of advisory board from seragon ; has received reimbursement for travel and in - kind items and services from roche , outside the submitted work . 
 s - ai reports grant support from astrazeneca and advisory consultant roles for astrazeneca , eisai , novartis , pfizer , roche / genentech and spectrum , outside the submitted work . 
hi reports grant support and personal fees from novartis during the conduct of the study ; hi was also an uncompensated member of the steering committee of this study ; hi has received personal fees in the form of honoraria and consulting fees from astrazeneca , pfizer , lilly , daiichi - sankyo , and f hoffman la - roche via chugai , outside the submitted work . 
jc reports personal fees from novartis , celgene , cellestia , astrazeneca , biothera pharmaceuticals , merus , seattle genetics , daiichi sankyo , erytech , pfizer , eisai , and samsung ; has received stock , patents , and intellectual property from medsir ; has received personal fees and research funding to his institution from roche , outside the submitted work . 
mdls reports personal fees in the form of speakers honoraria and advisory board honoraria from novartis , roche , lilly , pfizer , eisai , ipsen , and teva , outside the submitted work . 
cla reports personal fees for participation in a steering committee for the clinical trial from novartis , during the conduct of the study ; and personal fees for an expert advisory role from eli lilly , astrazeneca , genentech , millennium , celgene , pfizer , radius , and merck , outside the submitted work . 
sc also reports personal fees received in the form of honoraria for advisory boards from novartis , hoffmann laroche , pfizer , astrazeneca , and genomic health ; and institutional research support from novartis , hoffmann laroche , pfizer , astrazeneca , genomic health , genentech , merck , and bms , outside the submitted work . 
she also reports grant support from ambryx , amgen , bayer , obi pharma , bimarin , cascadian , daiichi sankyo , dignitana , genentech , gsk , lilly , macrogenics , medivation , merrimack , novartis , pfizer , pieris , puma , roche , seattle genetics , and travel support from lilly , novartis , and obi pharma , outside the submitted work . 
 reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
pv reports grant support from novartis during the conduct of this study ; he also reports personal fees for advisory board participation from novartis , speakers fees from pfizer and astrazeneca , and fees for advisory board participation and travel grants from roche , outside the submitted work . 
this correction has been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 15964 wolf a , naylor k , tam m , et al . 
these corrections have been made to the online version as of feb 1 , 2019 . correction to lancet oncol 2019 ; 20 : 17980 massari f , di nunno v . 
lancet oncol 2019 ; 20 ; 17980in this comment , the following sentence has been edited from time to deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab to risk of deterioration in pro scores was lower for patients who were given nivolumab plus ipilimumab . 
 this correction has been made to the online version as of feb 1 , 2019 , and the printed version is correct . vol 20 february 2019 corrections comment unknown primary is hampered by the inability of direct validation , because , by de nition , the primary cancer diagnosis cannot be veri ed . 
ideally , validation of tumour of origin should be based on patients autopsies in a prospective study ; however , in view of legal and ethical issues , such studies are very di cult to do in current clinical practice . 
 historically , cancer of unknown primary has been viewed as a distinct disease entity , mainly treated with empirical chemotherapy , and most patients have a dismal prognosis , with a median survival of 9 months.7 moran and colleagues noted that patients who were treated with site - speci c therapy based on their epicup diagnosis had improved overall survival ( hazard ratio 324 , 95% ci 142738 ; p = 00051 )  . 
 consistent with this result , in a large prospective study , patients who received site - speci c therapy based on tumour of origin molecular assays , had a median survival of 125 months compared with historical controls , 8 although this study has received major criticism because of design limitations , namely lack of randomisation.9 in the current era of personalised medicine , there individualising is a push towards patient management ; however , due to the rarity of cancer of unknown primary , no randomised study has ever been done for patients receiving site - speci c therapy compared with empirical therapy . 
ideally , a well - designed prospective randomised study could identify subsets of patients who would help to bene t more from targeted therapies , with the view improve clinical outcomes without maximising costs . 
however , a question that remains unanswered is whether a cancer of unknown primary with a molecular signature of a speci c primary behaves similarly to a typical metastatic cancer . 
a vision of the future would be the creation of a clinically useful diagnostic algorithm , which would incorporate pathological ndings and molecular pro ling tests along with crucial clinical judgment to maximise clinical bene t and limit costs . 
 panagiota economopoulou , * george pentheroudakis department of internal medicine , section of medical oncology , attikon university hospital , national kapodistrian university of athens , school of medicine , athens , greece ( pe ) ; and department of medical oncology , school of medicine , university of ioannina , 45110 ioannina , greece ( gp ) gpenther@otenet.gr we declare no competing interests . pentheroudakis g , gol nopoulos v , pavlidis n . 
multicenter validation of a 1 , 550 - gene expression pro le for identi cation of tumor tissue of orig j clin oncol 2009 ; 27 : 250308 . 6 ma xj , patel r , wang x , et al . 
molecular gene expression pro ling to predict the tissue of origin and direct site - speci c therapy in patients with carcinoma of unknown primary site : a prospective trial of the sarah cannon research institute . 
j clin oncol 2013 ; 31 : 251314 . maximum bene t of chemotherapy for osteosarcoma achievedwhat are the next steps ? published online august 25 , 2016 s1470 - 2045 ( 16 ) 30270 - 4 see articles page 1396 the survival rates for osteosarcoma have remained stagnant at 6065% for more than 25 years . 
the cisplatin , three - drug doxorubicin , and methotrexate ( map ) form the chemotherapy regimen of response therapy , and backbone induction chemotherapy correlates with patient outcome.1 debate remains about the usefulness of adding dose - intensive ifosphamide with or without etoposide 1340 vol 17 october 2016 comment to the three - drug map regimen ( mapie ) to improve the outcome of patients with a poor response ( de ned as 90% tum our necrosis ) to induction chemotherapy . 
 the results of the euramos - 1 international trial presented in the lancet oncology , 2 focused on patients with newly diagnosed , non - metastatic osteosarcoma , who had a poor response ( 90% tumour necrosis ) after neoadjuvant three - drug chemotherapy ( map ) and were randomly assigned postoperatively to map or map plus high dose ifosphamide ( dose used was 14 g / m at 28 g / m per day ) and etoposide ( mapie )  . 
 the study aimed to establish whether the addition of ifosphamide and etoposide , previously thought to improve outcome , would have a signi cant e ect on event - free ( the primary endpoint ) and overall survival . 
 no di erence in either event - free survival ( hazard ratio [ hr ] 098 [ 95% ci 078123 ] ) or overall survival was seen between the two groups . this trial investigate the euramos - 1 study shows that international collaborations are feasible , can be used to increase accrual of patient numbers , and are a powerful approach to studying rare cancers . 
this is the rst randomised important question , and not only shows that there was no patient bene t from ifosphamide and etoposide but also that there was an signi cant increase in regimen toxicity for high - grade non - haematological adverse events ( p = 00024 ) , particularly in grade 4 non - haematological adverse events ( 35 [ 12% ] of 301 in the map group vs 71 [ 24% ] of 298 in the mapie group )  . 
this study is both timely and important because it provides crucial information for oncologists on how to approach the care of paediatric , adolescent , and young adult patients with osteosarcoma who have responded poorly to preoperative chemotherapy . two other randomised trials3 , 4 investigated whether the addition of ifosphamide at the standard dose improved the 6065% survival of patients with osteosarcoma achieved with the three - drug regimen . 
 similar to the euramos - 1 trial , the childrens oncology group ( cog ) trial reported in 2008 , 3 and the italian sarcoma group trial reported in 2012 , 4 showed no ifosphamide to the three drug bene t regimen as judged by event - free survival and overall survival . 
a meta - analysis published in 2011 showed that although treatment with three drugs is superior to that with two drugs , no bene t existed for using in adding increasing the dose of four drugs compared with three drugs.5 therefore , despite ifosphamide and adding etoposide to the postoperative treatment , the euramos - 1 study corroborated the previous ndings . 
 the authors suggested that because ifosphamide and etoposide therapy was not initiated until week ve postoperatively , this delay might account for the lack of bene t of the more intensive regimen . 
however , this theory is questionable in light of these two trials , which initiated therapy with ifosphamide earlier than the euramos - 1 study.3 , 4 although the study design for the cog trial was di erent to that of the euramos - 1 trial in that ifosphamide was substituted for cisplatin in the preoperative regimen , the number of courses of cisplatin , doxorubicin , and methotrexate administered to patients was the same in both groups . 
the only di erence was the addition of ifosphamide , and in this trial , ifosphamide was administered early in the course of treatment.3 in addition to showing no improvement in event - free survival and overall survival , the cog trial also showed that there was no bene t in use of ifosphamide preoperatively because the percentage of patients with a good response to induction therapy was the same with or without ifosphamide . 
because response to induction chemotherapy is the only reliable marker of patient outcome , 1 these ndings support the conclusion that ifosphamide at either the standard - dose or high - dose provides no patient bene t . 
 responses to the time has come to put aside the hope that the addition of ifosphamide ( standard - dose or high - dose , with or without etoposide ) will provide the long improving the 6570% overall sought answer to survival achieved with the three - drug regimen , cisplatin , doxorubicin , and methotrexate . 
 although ifosphamide have been observed , this has not been translated into longer survival , the most important variable.6 the toxicity of adding ifosphamide with or without etopiside has also been documented many times , most recently in the euramos - 1 study . 
the addition of high - dose increased ifosphamide plus etoposide resulted toxicity and more cases of secondary leukaemia , which is by stark contrast with the addition of the three - drug immunotherapy mifamuride regimen , which resulted in a reduction in mortality the vol 17 october 2016 1341 comment published online september 13 , 2016 s1470 - 2045 ( 16 ) 30442 - 9 see articles page 1409 ( hr 071 [ 95% ci 052096 ] ) and an increase in survival from 70% to 78% at 8 years.3 the success of mifamurtide shows that osteosarcoma is sensitive to immunotherapy , suggesting that this should be the focus for future international trials . eugenie kleinerman md anderson cancer center , houston , tx , usa ekleiner@mdanderson.org i declare no competing interests . copyright the author ( s )  . 
grade of chemotherapy - induced necrosis as a predictor of local and systemic control in 881 patients with non - metastatic osteosarcoma of the extremities treated with neoadjuvant chemotherapy in a single institution . 
comparison of mapie versus map in patients with a poor response to preoperative chemotherapy for newly diagnosed high - grade osteosarcoma ( euramos - 1 ) : an open - label , international , randomised controlled trial . 
neoadjuvant chemotherapy with methotrexate , cisplatin , and doxorubicin with or without ifosfamide in nonmetastatic osteosarcoma of the extremity : an italian sarcoma group trial isg / os - 1 . 
chemotherapeutic adjuvant treatment for osteosarcoma : where do we stand ? eur j cancer 2011 ; 47 : 243145 . lewis ij , nooij ma , whelan j , et al . 
j natl cancer inst 2007 ; 99 : 11228 . ibrutinib holds promise for patients with 17p deletion cll the heterogeneity of the disease course and outcome leukaemia in patients with chronic lymphocytic is well known in haematological oncology.1 this heterogeneity is exempli ed by patients who carry aberrations in the tp53 gene , namely deletion 17p ( del17p ) or mutations in this gene . 
allogeneic transplantation may be the only viable treatment option for these patients , although this is often not possible because this disease is more common in older patients who are unable to undergo such procedure.1 the recently , the poor prognosis for these patients has improved radically with the approval of new kinase inhibitors ( often de ned as bcr inhibitors ) that seem to be equally active in this high - risk group of patients . 
 this impression mainly originated from ndings from subgroup analyses of phase 1b / 2 and 3 trials that showed , for example in the case of the btk inhibitor ibrutinib , 24 that patients with chronic lymphocytic leukaemia carrying del17p responded as well as those without this deletion , and achieved a longer that with other progression - free treatments in the relapsed or refractory setting and more than double that achieved by the udarabine , cyclophosphamide , and rituximab combination treatment - naive patients . survival than idelalisib for these reasons and despite the absence of robust scienti c evidence , ibrutinib ( and similarly the pi3k inhibitor in combination with rituximab that showed similar results to ibrutinib5 ) has also been approved by the regulatory agencies , with unprecedented foresight , for use in treatment - naive high - risk patients and adopted quickly by the haematological community as the treatment of choice for patients with tp53 aberrations in general.6 , 7 the widespread recommendation on the use of ibrutinib in high - risk patients despite the absence of robust evidence could be described as a leap of faith ; thus , susan obrien and colleagues study8 in the lancet oncology of the e cacy of ibrutinib in 144 patients with relapsed or refractory chronic lymphocytic leukaemia carrying del17p ( resonate - 17 ) is reassuring . 
at the prespeci ed primary analysis ( median follow - up of 115 months [ iqr 111138 ] ) , 92 ( 64% , 95% ci 5671 ) of 144 patients had reached the primary endpoint of an overall response in an extended as assessed by central review ; analysis with a median follow - up of 276 months ( iqr 146277 ) , 120 patients ( 83% , 95% ci 7689 ) had an investigator - assessed overall response . 
however , in a brief four - page document outlining his health - care plans , the main points of focus are the immediate dismantling of the a ordable care act ( aca ) and a reduction in funding for medicaid and medicare . 
the most concrete point made in the document is that the free market should determine provision of health care , with insurers free to o er plans across state lines . 
he also calls for greater transparency on health - care costs , and explicitly stipulates that the us market should be open to cheaper drugs from international sources . the aca was introduced in an insurance - based system to enable the many millions of uninsured americans its access to health carean ambition that has been partially realised . 
while an attempted repeal of the aca now looks inevitable given trumps hardline stance and the republican partys control of both houses of congress , it should not be withdrawn until a workable substitute has been drawn up . 
although the aca is awedespecially implementation , rising premiums , decreasing coverage , and inability to provide cover for all noninsured americansit currently stands as the main barrier between poorer americans and the risk of either a premature death or being bankrupted by the worlds most expensive health - care systewhat is needed is strong , policy - driven leadership and a commitment of funds to tackle the fast - rising incidence of cancer and other non - communicable diseases in the american population . the lack of detail in trumps plans allows for exibility in their execution . 
 the lancet oncology drug approval by regulators : who watches the watchers ? randomised in this issue of the lancet oncology , ian tannock and colleagues discuss some important parameters controlled governing outcomes of trials . 
they note that this concept is , in part , a consequence of regulators such as the us food and drug administration and the european medicines agency requiring statistical signi cance versus a comparator for a speci c endpoint to license drugs , rather than an indication that a drug has greater clinical utility compared with those already available . 
also , drug approvals usually require full disclosure of toxicities to regulators , who then have the relevant data and in - house knowledge to undertake thorough meta - analyses across multiple trials to determine drug safety . 
while there is always a need to collect real - world data to ensure e cacy in an unselected patient population , these processes can sometimes lead to a duplication of e ort and a waste of taxpayers moneypublic grants and taxes fund agency operating costs and later analyses . 
 for regulatory agencies to truly serve the public that they are designed to protect , there should be greater transparency in the approval process , with approval being clearly made on clinical , not just statistical , e cacy . 
 the lancet oncology vol 17 december 2016 1621 see articles page 1009 a step towards predicting checkpoint inhibitor response in kidney cancer in this issue of the lancet oncology , samra turaljic and colleagues report a heroic undertaking , using wholeexome sequencing data from 5777 patients representing 19 solid tumour types.1 in their series , the presence of frameshift indels across this large pan - cancer cohort was associated with more tumour - specific neoantigens compared with non - synonymous single nucleotide variant ( nssnv ) mutations . 
in renal cell carcinoma , frameshift indels were more prevalent compared with in other tumour types and were associated with enhanced antigen - presenting machinery and t - cell activation . 
their analysis helps to resolve a rather perplexing translational conundrumspecifically , that patients with renal cell carcinoma , a disease with a modest mutational load , show responses to checkpoint inhibitors on par with other diseases with considerably higher mutational loads.2 in non - small - cell lung cancer , melanoma , and other highmutational burden cancers , emerging evidence supports a link between mutational load and clinical outcome.3 , 4 by contrast , results from studies linking mutational load to outcome in renal cell carcinoma are mixed at best.57 the need to identify a predictor of checkpoint inhibitor response in metastatic renal cell carcinoma has never been greater . 
efforts to develop predictive biomarkers have largely failedeg , pd - l1 expression has shown a prognostic role , but did not predict outcome with nivolumab in the phase 3 comparison of this drug to everolimus in metastatic renal clear cell . 
results of the cabosun trial , 8 a randomised , phase 2 study comparing sunitinib and cabozantinib , have shown a significant improvement in progression - free survival in intermediate - risk and poor - risk patients with cabozantinib . 
if multiple studies have positive results , the clinician will need to discern the appropriate patient for either targeted therapy alone ( eg , cabozantinib ) , targeted therapy combined with a checkpoint inhibitor , or immunotherapeutic strategies alone . despite the poor predictive value of pd - l1 in this setting , other biomarkers show early promise . 
atkins and colleagues9 have reported a t - effector gene signature , generated in the context of a randomised , phase 2 study that compared sunitinib , bevacizumab and atezolizumab , and atezolizumab alone . 
 these results suggest a requisite step for turaljic and colleagues , namely , to define the predictive value of frameshift indel load for checkpoint inhibitor response in metastatic renal cell carcinoma . 
without question , they have shown that frameshift indels occur more frequently in the context of renal cell carcinoma , and that frameshift indels are associated with substantial neoantigen immunogenicity compared production with greater with nssnv neoantigens . 
they retrospectively predicate the link between frameshift indel load and checkpoint inhibitor response on four datasets , three including patients with melanoma and one including patients with non - small - cell lung cancer . 
moreover , none of these experiences include randomisation to a non - checkpoint in response assessment and 982 vol 18 august 2017 comment inhibitor control , making it unclear whether frameshift indel load might merely be prognostic rather than predictive . 
supporting this premise , in a previous series of 100 patients with non - small - cell lung cancer treated with a non - checkpoint inhibitor , the authors of this report1 found a higher relapse - free survival in those patients with higher frameshift indel load . 
 with a burgeoning array of clinical trials juxtaposing checkpoint inhibitor combinations against vegf - directed therapies in metastatic renal cell carcinoma , there should be ample opportunity to discern the predictive value of frameshift indel load in metastatic renal cell carcinoma . 
such confirmation is essential because certain frequent frameshift indels in renal cell carcinoma ( eg , vhl , pbrm1 , and kmd5c ) might themselves play a role in predicting response to vegf - directed therapy.10 if validated in randomised trials that compare checkpoint inhibitor interventions with non - checkpoint inhibitor interventions , frameshift indel load could represent a predictive biomarker for immunotherapy benefit that has yet remained elusive in metastatic renal cell carcinoma . 
 manuel caitano maia , eddy s yang , neeraj agarwal , * sumanta k pal department of medical oncology and experimental therapeutics , city of hope comprehensive cancer center , duarte , ca 91010 , usa ( mcm , skp ) ; department of radiation oncology , university of alabama at birmingham comprehensive cancer center , birmingham , al , usa ( esy ) ; hugh kaul precision medicine institute , university of alabama at birmingham school of medicine , birmingham , al , usa ( esy ) ; and division of medical oncology , university of utah huntsman cancer institute , salt lake city , ut , usa ( na ) spal@coh.org skp reports personal fees from pfizer , novartis , ipsen , astellas , bristol - myers squibb , gentech , and roche , outside of the submitted work . 
na reports personal fees from pfizer , exelixis , cerulean pharma , medivation / astellas , eisai , merck , novartis , emd serono , clovis oncology , and genentech / roche , outside of the submitted work . 
immotion150 : a phase ii trial in untreated metastatic renal cell carcinoma ( mrcc ) patients ( pts ) of atezolizumab ( atezo ) and bevacizumab ( bev ) vs and following atezo or sunitinib ( sun )  . 
eur urol 2017 ; 71 : 40514 . all tumours are rare , but some are rarer than others the report from the rarecare consortium1 in the lancet oncology , which updates the estimates of the burden of rare cancers in europe raises questions well beyond its immediate subject matter : what is the purpose of cancer registries ; how important is the quality of their data ; how should we , in the 21st century , classify cancer ? cancer registries have a long and distinguished history . 
subsequently , their role has expanded to include investigations of the causes of cancer , planning the organisation and funding of health services , and comparing outcomes across time and geographies . 
the rarecare initiative has used data from cancer registries across europe to assess the spectrum and combined incidence of rare cancersrare is defined as an annual incidence of less than six cases per 100 000 people . 
they conclude that 24% of all new patients with cancer in the european standard population ( eu28 ) have a rare cancera figure that is almost double the incidence of 13% reported from the usa using an identical definition of rare.2 even within analyses based on data from european registries , discrepancies exist ( figure )  . 
maintenance therapy with vinflunine plus best supportive care versus best supportive care alone in patients with advanced urothelial carcinoma with a response after first - line chemotherapy ( maja ; sogug 2011 / 02 ) : a multicentre , randomised , controlled , open - label , phase 2 trial . 
 lancet oncol 2017 ; 18 : 67281in this article , the declaration of interests should read jg - d reports personal fees from astellas , janssen ; grants and personal fees from astrazeneca , pfizer , pierre fabre , merck , bioclin , bristol myers squibb , novartis , and msd ; grants , personal fees , and non - financial support from roche ; and grants from gammamabs , outside the submitted work . 
af reports grants from astellas , astrazeneca , pierre - fabre ; personal fees and non - financial support from sanofi , janssen , bayer , and roche , outside the submitted work . 
bp - v reports personal fees from astellas pharma , novartis , pfizer , pierre fabre , bayer , sanofi , bristol - myers squibb , ipsen , and janssen - cilag , during the conduct of the study . 
jaa reports grants and personal fees from glaxosmithkline and novartis ; personal fees and nonfinancial support from jansen cilag ; grants , personal fees and non - financial support from bms ; personal fees from pfizer , roche , and eusa ; grants from sanofi and pierre fabre , outside the submitted work . 
nl reports personal fees from pfizer , sanofi , pierre fabre , roche , ipsen , pharma mar , bms , bayer , astrazeneca , astellas , and msd , outside the submitted work . 
jcv - g reports personal fees from pfizer , astellas , janssen , msd , bayer , roche , bristol , astrazeneca , boehringer , pierre fabre , novartis , ipsen , celgene , lilly , merck , sanofi , and mundipharma , outside the submitted work . 
bm reports personal fees and non - financial support from pfizer and janssen ; personal fees from novartis , astellas oncology , bms , sanofi , ipsen , bayer ; and grants and personal fees from roche , outside the submitted work . 
agda reports advisory board , consultancy and speaker honoraria or travel support from pierre fabre , roche , bristol - myers squibb , msd , pfizer , novartis , bayer , janssen , sanofi , astellas , eusa pharma , and eisai ; and research funding from astellas . 
dc reports personal fees from janssen , roche , astellas , msd , ipsen , pfizer , bms , bayer , astrazeneca , novartis , lilly , sanofi , pierre fabre , and boheringer , outside the submitted work . 
eg reports grants from pierrefabre , during the conduct of the study ; personal fees and non - financial support from janssen , pfizer , bayer , ipsen , novartis , bms , rovi ; personal fees from menarini and leo pharma ; and nonfinancial support from pierre - fabre , outside the submitted work . 
ua reports non - financial support from novartis , pierre fabre , and ipsen ; personal fees from bayer , janssen , astellas , and pfizer ; and personal fees and nonfinancial support from sanofi , roche , and bms , outside the submitted work . 
 xgdm reports personal fees from pfizer , ipsen , bms , roche , lilly , pharmamar , eusapharma , and pierre fabre ; and grants from astrazeneca , outside the submitted work . 
md has participated in advisory boards , consultancy , and speaker bureaus for roche , bristol - myers squibb , msd , pfizer , janssen , sanofi , astellas ; and received travel and accommodations expenses from roche , astellas , janssen , bayer , and lilly . 
jp has received honoraria as a consultant on advisory boards from pfizer , astellas , janssen , msd , bayer , roche , bms , boehringer , astrazeneca , ipsen , novartis , eusa pharma , eisai , and sanofi ; and as speaker from kyowa , pierre - fabre , celgene , lilly , and merck . 
 rm - b has served as a consultant or on advisory and / or speakers bureaus for sanofi aventis , bayer , janssen , astrazeneca , merck sharp & dohme , and asofarma ; and received travel and accommodations expenses from roche , sanofi aventis , astellas , janssen , merck sharp & dohme , bayer , pharmacyclics , clovis oncology , and lilly . 
jlp - g reports non - financial support from pierre fabre , during the conduct of the study ; non - financial support from roche , bms , and msd , outside the submitted work . 
jb reports grants and personal fees from pfizer , merck , bms ; personal fees from genentech , astrazeneca , pierre - fabre ; and grants from takeda , during the conduct of the study . 
 this correction has been made to the online version as of jan 3 , 2019 . correction to lancet oncol 2018 ; 19 : 1493503 zackrisson s , lng k , rosso a , et al . 
 lancet oncol 2018 ; 19 : 1493503 in this article , in table 1 and table 4 , the age groups should have been listed as follows : 4049 , > 4959 , > 5969 , and > 69 . 
the title and legend of figure 2 should have read as follows : number of false - positive results among participants over the trial period who were recalled only on digital breast tomosynthesis and digital mammography , respectively . 
 these corrections have been made to the online version as of jan 3 , 2019 . vol 20 january 2019 corrections for more on the study of skin cancer apps see birmingham.ac.uk / news / latest / 2018 / 07 / skin - cancerphone - apps - research.aspx for more on the apple watch emoji study see proc am soc clin oncol 2018 ; 36 ( suppl ) : abstr 6501 digital oncology apps : revolution or evolution ? the uks recent spell of hot and sunny weather serves as a reminder of the need to be cognisant of the association between increased sun exposure and heightened skin cancer risk . 
in a timely study presented at the british association of dermatologists 98th annual meeting ( july 35 , 2018 ; edinburgh , uk ) , researchers evaluated the increasing number of new digital apps to aid in skin cancer diagnosis that are entering the digital oncology market . 
 could such technologies revolutionise the detection and treatment of this disease ? and how much do theyand the rapidly emerging digital health market as a whole add to existing standards of care ? early diagnosis is key in determining outcomes from skin cancer : 5 - year rates can be high with early diagnosis , but as low as 10% if diagnosed at an advanced stage . 
although theoretically these apps could potentially increase selfawareness of skin changes and improve cancer detection rates , the study presented in edinburgh found that some apps were more successful than others at identifying both malignant and benign moles and lesions , with many unable to detect rare or unusual skin cancers . 
 the researchers found that flaws in the computing algorithms and technology and little medical specialist input during development mean that the apps cannot identify suspicious lesions as accurately as a dermatologist could . 
 the range in quality and accuracy of skin cancer detection apps is often a result of hasty development and a lack of high - level evidence from properly conducted trials to show how effectively they work compared with the current standard of care . 
consequently , with the goal of delivering a working product quickly to make money back from the initial investment , the development process can be rushed , without sufficient input from medical experts or rigorous testing . moreover , although these new technologies initially look exciting , careful consideration is needed when comparing them to standard health - care practices . 
 how much clinical value do they truly add ? educational health apps might help to increase awareness about some health conditions , and a recently reported study showed that patients with cancer using an apple watch and emojis to record their quality of life symptoms could be a promising new way to record and track patientreported outcomes . 
indeed , the most successful skin cancer apps are those that involve sending an image directly to a dermatologist for review , showing that medical specialists are still needed to obtain an accurate diagnosis . 
the algorithms on which the technologies are based must undergo thorough peer review and the data ought to be made available in the public doma additionally , digital oncology reporting guidelines should be created , similar to those that already exist for drug trials . 
robust randomised controlled trials comparing these new methods with existing standards of care and head - tohead comparisons of different technologies are needed to provide solid evidence about which ones work and which do not . 
we must not fall into the same commercial traps with digital health technologies as we already have with the pharmaceutical industry in which trials directly comparing competing agents for the same indication are scarce . 
without solid evidence from proper trials to prove the effectiveness of digital health technologies , there is a real danger of compromising public and patient safety , especially when products like the skin cancer apps make bold claims about their ability to detect cancer . 
 as we enter this new world of digital health , we must not allow ourselves to be dazzled by the exciting technologies suddenly on offer and their role in health care needs careful consideration . 
this is a new field , and it needs close scrutiny to ensure that it is appropriate for the health sector , is cost - effective , and , above all , does not compromise patient safety . 
 the lancet oncology vol 19 august 2018 editorial published online march 3 , 2020 s1470 - 2045 ( 20 ) 30150 - 9 key laboratory of respiratory disease of zhejiang province , department of respiratory and critical care medicine ( yx , rj , wl , hs ) and department of medical oncology ( jz ) , second affiliated hospital of zhejiang university school of medicine , hangzhou , zhejiang 310052 , china liang w , guan w , chen r , et al . 
the authors concluded that patients with cancer had a higher risk of covid - 19 and with a poorer prognosis than those without cancer . first , the data in the comment by liang and colleagues1 showed a higher percentage of patients with cancer in the covid - 19 cohort than in the overall population . 
second , we reviewed the cancer history of the 18 individuals discussed in liang and colleagues comment.1 we are concerned that such a small sample size with a large amount of heterogeneity , presenting as various cancer types with different biological behaviours , highly variable disease courses ( from 016 years ) , and diverse treatment strategies , might be filled with contingency and thus not ideally representative of the whole population with cancer . 
notably , half of the patients with cancer had a disease course of more than 4 years , indicating that a substantial proportion of these patients might be clinically cured . 
third , 13 ( 72% ) of 18 patients with cancer had a history of surgical resection ; the prolonged effects induced by surgery including immunosuppression should not be neglected . 
comparison of patients with covid - 19 and surgical history with and without cancer would be of interest . important additionally , the authors reported that patients with cancer were prone to severe events ( admission to the intensive care unit requiring invasive ventilation , or death ) from covid - 19 . 
evidence indicates that overwhelming inflammation lung and cytokine - associated injury could be instigating these severe events in patients with covid - 19.2 however , accumulated evidence has shown that development of cancer usually associated with a blunted immune status3 characterised by overexpressed immunosuppressive induction cytokines , suppressed o f p r o i n f l a m m a t o r y d a n g e r signals , impaired dendritic cell maturation , and enhanced functional leukocyte immunosuppressive populations , which is contradictory to the events believed to result in severe events in patients with indeed , one of the covid - 19 . 
 data have shown that tobacco use significantly increases the gene expression of angiotensinconverting enzyme 2 , the binding receptor for severe acute respiratory syndrome coronavirus 2 , which could explain the elevated susceptibility to covid - 19 in smokers.4 furthermore , cigarette smoking is the leading cause of chronic obstructive pulmonary disease , which has been identified as an independent risk factor in severe covid - 19 cases.5 overall , current evidence remains insufficient to explain a conclusive association between cancer and covid - 19 . we declare no competing interests . yang xia , rui jin , jing zhao , wen li , * huahao shen huahaoshen@zju.edu.cn joint first authors vol 21 april 2020 e180 correspondence corrections correction to lancet oncol 2015 ; 16 : 1338 correction to lancet oncol 2015 ; 16 : e434 bagcchi s . 
lancet oncol 2015 ; 16 : e434in this news item , the fourth sentence of the third paragraph should read patients with ccnd1 mutations had worse 2 - year overall survival than those without ( 381% [ 95% ci 14100 ] vs 80% [ 7684 ] ; p = 0005 ) ; similar outcomes were noted with alterations in the dna repair pathways ( tp53 , atm , atr , and znfhx4 mutations )  . 
triage by methylation - marker testing versus cytology in women who test hpvpositive on self - collected cervicovaginal specimens ( prohtect - 3 ) : a randomised controlled non - inferiority trial . 
lancet oncol 2015 ; 16 : 133543in this article , the title of figure 2 should have been kaplan - meier analysis of cumulative incidence of leukaemia for children with or without enterovirus infection after accounting for death as the competing risk . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . correction to lancet oncol 2015 ; 16 : 1289 lokody , i . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the fourth paragraph on liver transplants for patients with high risk hcc has been changed to read : of these , 17 had a liver transplant . 
the 5 - year survival of these patients was superior to those high risk patients that did not have a liver transplant ( 82% vs 38% ; p = 0033 )  . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . vol 16 october 2015 e480 corrections correction to lancet oncol 2015 ; 16 : 1013 correction to lancet oncol 2015 ; 16 : 1143 correction to lancet oncol 2015 ; 16 : 1289 declaration kopans db . 
 lancet oncol 2015 ; 16 : 1143the last line of the rst paragraph of this comment should read only this year , for example , did who add several commonly used , extremely e ective drugs , such as imatinib , trastuzumab , and cisplatin to its list of essential medicines . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the paragraph on survival with oligometastatic hcc should read the researchers found that patients with oligometastatic disease had a significantly longer overall survival than patients with extensive disease ( 104 months versus 63 months , p = 0034 )  . 
 vol 16 november 2015 e528 correction to lancet oncol 2016 ; 17 : e14962 correction to lancet oncol 2017 ; 18 : 1089103 correction to lancet oncol 2017 ; 18 : e713 shaikh f , murray mj , amatruda jf , et al . 
in order to investigate the e ects of these therapies and to respond to emerging evidence , we aimed to systematically review all relevant trials using a framework for adaptive meta - analysis . 
 methods for this systematic review and meta - analysis , we searched medline , embase , lilacs , and the cochrane central register of controlled trials , trial registers , conference proceedings , review articles , and reference lists of trial publications for all relevant randomised controlled trials ( published , unpublished , and ongoing ) comparing either standard of care with or without docetaxel or standard of care with or without bisphosphonates for men with high - risk localised or metastatic hormone - sensitive prostate cancer . 
for each trial , we extracted hazard ratios ( hrs ) of the e ects of docetaxel or bisphosphonates on survival ( time from randomisation until death from any cause ) and failure - free survival ( time from randomisation to biochemical or clinical failure or death from any cause ) from published trial reports or presentations or obtained them directly from trial investigators . 
 results from three ( chaarted , getug - 15 , stampede ) of these trials ( 2992 [ 93% ] of 3206 men randomised ) showed that the addition of docetaxel to standard of care improved survival . 
the hr of 077 ( 95% ci 068087 ; p < 00001 ) translates to an absolute improvement in 4 - year survival of 9% ( 95% ci 514 )  . 
docetaxel in addition to standard of care also improved failure - free survival , with the hr of 064 ( 058070 ; p < 00001 ) translating into a reduction in absolute 4 - year failure rates of 16% ( 95% ci 1219 )  . 
survival results from three ( getug - 12 , rtog 0521 , stampede ) of these trials ( 2121 [ 53% ] of 3978 men ) showed no evidence of a bene t from the addition of docetaxel ( hr 087 [ 95% ci 069109 ] ; p = 0218 ) , whereas failure - free survival data from four ( getug - 12 , rtog 0521 , stampede , tax 3501 ) of these trials ( 2348 [ 59% ] of 3978 men ) showed that docetaxel improved failure - free survival ( 070 [ 061081 ] ; p < 00001 ) , which translates into a reduced absolute 4 - year failure rate of 8% ( 510 )  . 
survival results from three of these trials ( 2740 [ 88% ] of 3109 men ) showed that addition of bisphosphonates improved survival ( 088 [ 079098 ] ; p = 0025 ) , which translates to 5% ( 18 ) absolute improvement , but this result was in uenced by the positive result of one trial of sodium clodronate , and we found no evidence of a bene t from the addition of zoledronic acid ( 094 [ 083107 ] ; p = 0323 ) , which translates to an absolute improvement in survival of 2% ( 3 to 7 )  . 
of 17 trials of bisphosphonates for men with m0 disease , survival results from four trials ( 4079 [ 66% ] of 6220 men ) showed no evidence of bene t from the addition of bisphosphonates ( 103 [ 089118 ] ; p = 0724 ) or zoledronic acid ( 098 [ 082116 ] ; p = 0782 )  . 
failure - free survival de nitions were too inconsistent for formal meta - analyses for the bisphosphonate trials . interpretation the addition of docetaxel to standard of care should be considered standard care for men with m1 hormone - sensitive prostate cancer who are starting treatment for the rst time . 
no evidence exists to suggest that zoledronic acid improves survival in men with m1 or m0 disease , and any potential bene t is probably small . funding medical research council uk . 
open access article distributed under the terms of cc - by . vol 17 february 2016 lancet oncol 2016 ; 17 : 24356 published online december 21 , 2015 s1470 - 2045 ( 15 ) 00489 - 1 this online publication has been corrected . 
with 11 million diagnoses ( 15% of all cancers diagnosed in men ) and 307 000 deaths estimated to have taken the in 2012 , prostate cancer has become place fth leading cause of death from cancer in men worldwide.1 therapy with for many decades , initial ( rst - line ) treatments for both locally advanced and metastatic prostate cancer have been surgical castration by bilateral orchidectomy or androgen deprivation luteinising hormone - releasing hormone agonists or antagonists.2 the aim of these approaches is to reduce testosterone concentrations . 
however , the disease progresses in virtually all patients who have metastatic disease and in many patients with non - metastatic disease.3 , 4 a number treatments , such as bisphosphonates , cytotoxic chemotherapy , new hormone therapies , and radium - 223 , have therefore been assessed in combination with primary androgen deprivation therapy with the aim of reducing progression rates and improving survival . one such treatment , docetaxel ( given with or without estramustine ) , was shown in two pivotal randomised controlled trials5 , 6 to improve survival in men with castrate - resistant prostate cancer that was no longer responsive to testosterone suppression alone . 
this nding led to the international approval by regulatory authorities of docetaxel for this disease setting and a number of randomised controlled trials , in which men with metastatic or high - risk localised prostate cancer , starting long - term androgen deprivation therapy for the rst time , were randomly assigned to receive standard androgen deprivation therapy - based treatment alone or supplemented with docetaxel ( with or without other agents )  . 
in the chaarted7 and stampede8 trials , men with metastatic disease had signi cant improvements in survival with the addition of docetaxel , whereas results of the similar getug - 15 trial9 , 10 showed no evidence of a survival bene t from docetaxel . 
a small number of trials of docetaxel for men with non - metastatic disease have produced promising results for relapse or failure - free survival , but the e ect on survival is unclear . bisphosphonates are a class of drugs that have been shown to have a number of anti - cancer e ects.11 in randomised controlled trials , the rst - generation bisphosphonate , clodronate , delayed time to progression in men with bone metastases when given alongside long - term androgen deprivation therapy . 
some evidence suggests that biphosphonates might improve survival.12 newer ( third - generation ) bisphosphonates , notably zoledronic acid , have been found to reduce the risk of skeletal complications ( eg , fractures ) in patients with bone metastases from breast cancer and castrate - resistant prostate cancer.13 in the wake of these results , a number of randomised controlled trials have been designed to investigate whether men who are commencing long - term androgen deprivation therapy for either metastatic or localised hormone - sensitive prostate cancer bene t from bisphosphonates . as part of the wider systemic treatment options for prostate cancer ( stopcap ) meta - analysis project , we aimed to systematically review all relevant randomised controlled trials that tested the addition of docetaxel or bisphosphonates to standard of care . 
we prospectively planned meta - analyses that would respond and adapt to the emergence of new trial results , while also assessing the potential e ect of trials that are yet to be completed or reported . methods systematic review and framework for adaptive meta - analysis standard systematic reviews of both aggregate and individual participant data can take many years to complete and are usually retrospective , so they cannot always keep pace with therapeutic developments . 
we therefore used a framework for adaptive meta - analysis ( fame ) being developed by the mrc clinical trials unit at ucl ( london , uk ) to rapidly and robustly assess the e ects of therapies and to respond to emerging evidence . 
the key principle is to systematically identify all trials using established methods , then synthesise what is already known about the e ects of therapies from aggregate data , and consider how trials that are ongoing or yet to be reported might a ect these results . 
 thus , we deliberately began the review process before many trials of docetaxel and bisphosphonates had been completed and reported so as to build a picture of how information and evidence of the e ects of these drugs might accumulate . 
this review process allowed us to decide prospectively when we were likely to have su cient results or power , or both , for reliable aggregate data meta - analyses and to interpret our results , taking into account the possible e ect of any as yet unavailable evidence . 
this also helped us determine the potential value of updating meta - analyses , and whether these meta - analyses should be based on aggregate data or individual patient data . study selection and data extraction randomised controlled trials comparing either standard of care versus standard of care plus docetaxel or standard of care versus standard of care plus bisphosphonate ( at a therapeutic dose ) were eligible if they aimed to include men with high - risk localised or metastatic , hormonesensitive ( ie , not castrate - resistant ) prostate cancer . 
we unpublished , with no searched medline , 14 embase , 15 lilacs , 16 and the 244 vol 17 february 2016 articles see online for appendix for the protocol see crd.york.ac.uk / prospero / display_record . asp ? id = crd42015020059 4372 records retrieved from electronic databases searching 1213 from medline 2355 from embase 617 from cochrane central 187 from lilacs 769 records retrieved from clinicaltrials.gov and screened 1191 duplicates removed 738 irrelevant comparison 3181 unique records screened 3132 irrelevant comparison 3 potentially eligible trials identied via conference proceedings 49 assessed for eligibility 34 assessed for eligibility 28 excluded 14 duplicate references to the same trial 14 ineligible after full paper screened 12 not treatment dose 1 crpc 1 not randomised controlled trial 20 excluded 10 duplicate trials already identied via electronic databases 10 ineligible 6 not treatment dose 1 crpc 1 not randomised controlled trial 2 irrelevant comparison 21 eligible trials 14 eligible trials 35 included in systematic review 22 included in meta - analysis of bisphosphonate comparison * 14 included in docetaxel comparison * figure 1 : study ow chart crpc = castrate - resistant prostate cancer . 
search terms used are listed in the appendix . for all eligible trials , we extracted data on : the accrual period , actual or ( if ongoing ) planned number of participants ; whether previous androgen deprivation therapy was allowed ; control group treatments ( eg , type of androgen deprivation therapy used ) ; docetaxel dose and scheduling ; bisphosphonate type ; dose and duration of bisphosphonate treatment ; median patient age ; metastatic status ; performance status ; tnm status ; gleason score ; and median psa concentration at the start of androgen deprivation therapy . 
we also extracted data on methods of sequence generation , allocation concealment , completeness of outcome data reporting , and attrition from trial reports or protocols , or both , to assess the risk of bias of individual trials.17 methods were prespeci ed and are available in an online protocol . outcomes the primary outcome , survival , was de ned as the time from randomisation until death from any cause . 
psa = prostate - speci c antigen . * this value is the mean ( no sd was available ) table 1 : characteristics of studies included in the systematic review and meta - analysis all potential participants , would become available by june , 2015 , with a median follow - up of about 34 years . 
 the typical 4 - year survival reported in trials in this group of men was 40% , which we set as our baseline for predicting the power a meta - analysis of these trials would be likely to provide . 
we estimated that we would have about 70% power to detect an absolute di erence of 5% in 4 - year survival ( hazard ratio [ hr ] 087 ) and more than 99% power to detect a 10% di erence in 4 - year survival ( hr 075 ) ; these are the sort of moderate e ects one might expect in advanced prostate cancer . 
for the bisphosphonate comparison in m1 disease , we predicted that we would have results from trials that included about 85% of all potential participants and , using the same baseline survival , would achieve about 65% power to detect an absolute di erence of 5% in 4 - year survival and more than 99% power to detect a 10% di erence in 4 - year survival . 
these estimates gave us a clear trigger to conduct meta - analyses in the m1 disease setting . we were aware that mature results of trials in m0 disease would lag behind those in the m1 setting owing to a more favourable prognosis , so we expected fewer data for the docetaxel and bisphosphonate comparisons ( around 60% of potential participants )  . 
nevertheless , on the basis of an average baseline 4 - year survival of around 80% in the reported trials , we predicted that we would still have reasonable power ( 60% ) to detect a 5% di erence in 4 - year survival and more than 99% power to detect a 10% di erence in 4 - year survival , allowing us to compare the evidence between the two settings and ascertain if and when further meta - analyses are needed . for each trial , we extracted hrs of the e ects of docetaxel or bisphosphonates on survival and failure - free survival from trial reports , estimated them from published kaplan - meier curves or other summary statistics , 1820 or obtained them directly from trialists . 
for example , we could obtain the hr for the addition of docetaxel to standard of care plus zoledronic acid versus standard of care plus zoledronic acid alone for the stampede trial8 from the ratio of the hrs for the separate comparisons of standard of care with or without zoledronic acid and standard of care with or without zoledronic acid plus docetaxel . 
 we combined the hrs from each of the individual , eligible trials in a meta - analysis using the xed - e ect model ( mantel - haenzsel )  . 
we also used the randome ects model to assess the robustness of the results to the choice of this model for the primary analysis.22 we assessed the heterogeneity in treatment e ects between trials using the i statistic and test . 
we planned to combine all trials and , providing that su cient trials or data were available , preplanned analyses that would compare trials ( or patients within trials ) grouped by metastatic status , use of previous local cancer , planned for prostate radiotherapy as part of the standard of care , type of and length of time on androgen deprivation therapy allowed before randomisation , total planned dose of docetaxel , additional agents in the docetaxel group only , type of bisphosphonate , and dose of zoledronic acid . 
we also planned to investigate whether there were interactions between any the following covariates : age ; performance status ; tnm stage ; gleason score ; whether newly diagnosed or not ; previous androgen deprivation therapy ; and ( for m1 disease only ) the location and volume of all metastases and the volume of bone metastases . 
the interaction hr in each trial was calculated from the ratio of the estimated hrs for each subgroup ( eg , the hr for previous androgen deprivation therapy divided by the hr for no previous androgen deprivation therapy ) ; these hrs were then combined across trials using a xed - e ect meta - analysis.24 we used stata version 13 for all analyses . 
 role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results our searches of bibliographic databases , trial registers , and conference proceedings identi ed 5141 articles and records ( gure 1 )  . 
in total , 35 trials were eligible ; 14 trials were eligible for inclusion in the docetaxel comparison , and 22 the bisphosphonate comparison ( table 1 , table 2 ) .2547 one large multiarm trial ( stampede ) , 8 which incorporates multiple treatment comparisons in men with both m0 and m1 disease , contributes to both the docetaxel and bisphosphonates meta - analyses . trials were eligible for in men with m1 disease . 
one five trials compared standard of care with or without trial docetaxel ( goup 01 / 04 [ nct00796458 ] ) , including 200 men , is still recruiting , and another trial , 32 including 14 men , has yet to report suitable outcome data ( table 2 )  . 
in the three remaining trials , 7 , 8 , 10 men aged 3691 years ( median 6366 years ) with a good performance status received androgen deprivation therapy - based treatments ( standard of care ) with or without docetaxel ( table 1 )  . 
 table 2 : characteristics of studies included in the systematic review that could not be included in the meta - analyses given at a standard dose of 75 mg / m per cycle every 3 weeks for six to nine cycles , and median follow - up ranged from 29 months to 829 months ( table 1 )  . 
 all trials were assessed as being at low risk of bias ( table 3 )  . survival data from these three trials7 , 8 , 10 were available for 2992 ( 93% ) of 3206 men with m1 disease ( table 1 ) , and 1271 deaths had been recorded . 
nhs = national health service . table 3 : assessment of risk of bias 40 patients ( 3% of total randomised ) excluded from analyses ; seven patients were ineligible ; 27 patients withdrew consent ; six patients were lost to follow - up ; exclusions are balanced by group in the primary analysis , no randomised patients were excluded from the analyses ; in the analysis with long - term follow - up , 37 patients were excluded as they had not been agged with the nhs information centre in the primary analysis , no randomised patients were excluded from the analyses ; in the analysis with long - term follow - up , 33 patients were excluded as they had not been agged with the nhs information centre all randomised patients included in the analyses reports survival , but not failure - free survival as de ned in the meta - analysis reports survival , but not failure - free survival as de ned in the meta - analysis reports survival , but not failure - free survival as de ned in the meta - analysis yes , outcomes of interest are reported , including survival and failure - free survival translates to a 9% ( 95% ci 514 ) absolute improvement with standard of care plus docetaxel relative to standard of care alone ( gure 2 )  . 
statistical heterogeneity was very low throughout all analyses , so the estimates generated using a random - e ects model were consistent with those generated with the xed - e ect model . failure - free survival was de ned similarly in all trials . 
 however , in the stampede trial , 8 only prostate cancer speci c deaths were included ( rather than death by any cause ) , and in the chaarted trial7 the most similar reported outcome to our de nition of failure - free survival was time to hormone - refractory disease , which was de ned as the time from randomisation until clinical or serological progression . 
all trials were assessed as being at low risk of bias ( table 3 )  . survival results were available for 2740 ( 88% ) of 3109 men from three trials , and 1365 deaths have been recorded . 
again , we found no evidence of variation between the trial results . we identi ed 11 trials that compared standard of care with or without docetaxel for men with non - metastatic disease ( m0 )  . 
two trials ( can - ncic - pr12 [ nct00651326 ] and 05 - 043 [ nct00116142 ] ) , including 398 men , have nished accrual but have yet to report any results . 
the four remaining trials , 8 , 25 , 27 , 28 all of which have reported survival or failure - free survival , or both , were included in the meta - analysis . 
men of median age 6266 years ( ranges not reported for all trials ) with non - metastatic disease and good performance status were randomly assigned to receive standard of care with or without docetaxel ( table 1 )  . 
docetaxel was given at a standard dose of 75 mg / m per cycle every 3 weeks for six cycles , except in one trial , 25 which used docetaxel 70 mg / m plus estramustine 10 mg / kg on days 15 of each cycle . 
all trials were assessed as being at low risk of bias ( table 3 )  . survival data were available for 2121 ( 53% ) of 3978 men from three of the four trials , 8 , 25 , 28 and 340 deaths have been recorded . 
the meta - analysis hr of 087 ( 95% ci 069109 ; p = 0218 ) translates to a potential absolute improvement of 2% ( 95% ci 2 to 7 ) , assuming a typical baseline 4 - year survival of 80% ( gure 2 ) ; however , the con dence intervals are wide , and the result is not statistically signi cant . 
we found no evidence of variation between the trial results . failure - free survival was de ned consistently in all four trials , 8 , 25 , 27 , 28 but in the stampede trial , 8 only prostate cancer - speci c deaths were included ( rather than death by any cause ) , and the getug - 12 trial26 included time - to - salvage treatment . 
the meta - analysis hr of 070 ( 95% ci 061081 ; p < 00001 ) translates to an absolute improvement of 8% ( 95% ci 510 ) , reducing 4 - year failure rates from 30% to 22% , assuming a baseline 4 - year failure - free survival of 70% ( gure 2 )  . 
again , no evidence exists of variation between the trial results . we identi ed seven trials that compared standard of care with or without bisphosphonates in men with m1 disease . 
the results of one trial ( kyuh - trigu0705 [ nct00685646 ] ) , including 227 men , have yet to be reported , and in three other trials , 37 , 42 , 47 including 142 men , skeletal - related events , changes in bone mineral density , or both were the primary outcomes , and survival was not reported ( table 2 )  . 
in the three remaining trials , 8 , 12 , 30 men of median age 6671 years ( range 4088 ) with good performance status were randomly assigned to receive standard of care with or without either zoledronic acid8 , 30 or sodium clodronate12 ( table 1 )  . 
however , when the analysis was restricted to the two trials ( 1107 deaths among 2462 men ) that compared standard of care with and without zoledronic acid , we found no evidence of a bene t of standard of care plus zoledronic acid ( hr 094 [ 95% ci 083107 ] ; p = 0323 ) , with a potential absolute improvement in survival of 2% ( 95% ci 3 to 7 ; gure 3 ) , although these di erences were not statistically signi cant . 
 in the one trial of sodium clodronate , 12 a clear treatment bene t was reported ( hr 077 [ 95% ci 060098 ] , p = 0032 )  . failure - free survival was only reported in one trial , with other trials reporting a variety of intermediate outcomes ( eg , bone metastases - free survival , time to rst skeletal - related event ) , such that no formal meta - analysis was possible . we identi ed 17 trials that compared standard of care with or without bisphosphonates for men with m0 disease . 
the results of three trials ( cecog [ nct00181584 ] , zenith [ nct00063609 ] , and nu - 02u1 [ nct00058188 ] ) , including 646 men , are unpublished , and ten other trials , 3641 , 4346 including 1494 men , have reported results for outcomes other than survival ( table 2 )  . 
in the four remaining trials8 , 12 , 21 , 29 included in the meta - analysis , men aged 4087 years ( median 6670 years ) with good performance status were randomly assigned to receive standard of care with or without either zoledronic acid8 , 21 , 29 or sodium clodronate12 ( table 1 )  . 
in two of the trials , 21 , 29 zoledronic acid was given at a dose of 4 mg every 3 months for either 18 months or 4 years , whereas in the third trial , 8 zoledronic acid 4 mg was given every 3 weeks for 2 years . 
all trials were assessed as being at low risk of bias ( table 3 )  . follow - up across trials ranged the survival results were available for 4079 ( 66% ) of 6220 men from four trials , and 918 deaths have been recorded . 
assuming a baseline 4 - year survival of 80% , this hr translates to a potential absolute detriment in survival of 1% ( 95% ci 3 to 2 ; gure 3 ) , although this is not statistically signi cant , and we found no evidence of variation between the trial results . 
results were similar when the analysis was restricted to trials that tested standard of care with or without zoledronic acid ( three trials , 637 deaths , 3608 men ; hr 098 [ 082116 ] ; p = 0782 ) , suggesting no potential absolute improvement in survival ( 0% , [ 95% ci 3 to 3 ] ; gure 3 ) , again with no evidence of variation between the trial results . 
failure - free survival was only reported in one trial so no formal meta - analysis was done . for both the docetaxel and bisphosphonate comparisons , far fewer results were available for the m0 disease setting than for the m1 setting , which is why the meta - analyses for the m1 and m0 settings are presented separately . 
moreover , within these meta - analyses , not enough trials have assessed whether any e ect varied by other trial characteristics ( eg , use of radiotherapy plus androgen deprivation therapy )  . 
also , results by patient 252 vol 17 february 2016 articles subgroup were either too sparse , or the de nitions too inconsistent , to allow for meaningful analyses from the available reported data . discussion this meta - analysis provides substantial and reliable evidence that adding docetaxel to standard of care improves the survival of men with m1 disease , with an absolute improvement of around 9% at 4 years . 
for men with m0 disease , evidence to date supports an 8% reduction in absolute failure rates at 4 years with docetaxel , but the evidence is insu cient to reliably assess the e ects on survival . 
although evidence suggests the addition of bisphosphonates to standard of care for men with m1 prostate cancer , this e ect appeared to be largely driven by one trial of the drug sodium clodronate , and our results suggest that any potential bene t of zoledronic acid is small . 
we found no evidence that bisphosphonates improve survival in men with m0 disease . improved survival with cancer the results are reliable and robust for men with m1 hormone - sensitive prostate treated with docetaxel because , although based on three trials only , these results are derived from 93% of all men who were randomly assigned to treatment groups and 1271 deaths . 
although additional results might become available in this setting , from both the goup 01 / 04 and the gentax32 trials , these results are unlikely to materially a ect our ndings . 
importantly , however , in three of the included trials7 , 8 , 10 most of the men who were randomly assigned to treatment groups were newly diagnosed with metastatic disease . 
while we see no reason for why the observed bene t of docetaxel should not be generalisable , the only way to appropriately assess this , or any other remaining questions , is through the collection and re - analysis of individual participant data . 
nevertheless , docetaxel combined with androgen deprivation therapy should be considered a new standard of care for men with metastatic disease starting on long - term androgen deprivation therapy for the rst time who are t to receive chemotherapy and willing to accept these risks . 
future trials in this setting should also consider this as an appropriate control group.48 in men with non - metastatic disease , we found evidence that docetaxel improves failure - free survival ; however , this conclusion is based on data from four trials including just over half of all men who were randomly assigned to treatment groups . 
nevertheless , as the estimate of e ect ( hr 070 ) is in keeping with that for men with metastatic disease ( hr 064 ) and the con dence interval is narrow , this nding provides a clear and early signal of potential bene t . 
for overall survival , however , the available data are less mature , such that the estimate of e ect is based on half of all men who were randomly assigned to treatment groups and 340 deaths , and the con dence interval is wide . 
this meta - analysis will be important to update , to include mature results of unreported trials and long - term followup of those already reported , to reliably assess any e ect of docetaxel on survival . 
we will need to collaborate with trial investigators to determine when these data are likely to emerge so that we can predict when a meta - analysis that includes a much larger proportion of the men randomised in this setting and provides su cient power to detect moderate survival bene ts will be feasible . 
thus , we will also need to examine the e ects of docetaxel on prostate cancer - speci c survival , which will only be possible through our planned international individual participant data meta - analysis . despite the bene ts of bisphosphonates with respect to skeletal - related events and bone pain , 49 , 50 the e ect of bisphosphonates on survival in men with hormonesensitive prostate cancer is less clear . 
in men with m1 disease , although based only on three trials , these results represent 87% of men who were randomly assigned to treatment groups and suggest a small potential survival bene t . 
in the non - metastatic setting , although based on only four of 17 trials , the analysis includes around 65% of randomly assigned men , and we found no evidence of a bene t of bisphosphonates on survival . 
 data from other identi ed trials might provide enough power to detect a small bene t , but our results at present suggest that even a small bene t of zoledronic acid is unlikely . in both the metastatic and non - metastatic disease settings , we are aware of a number of limitations of a meta - analysis based on trials of bisphosphonates , not least that many of the trials identi ed in the systematic review have not reported survival and so could not contribute to the meta - analysis . 
for example , in the stampede trial , 8 treatment was stopped at the time of progression , whereas in the calgb 90202 trial , 30 patients crossed over to receive zoledronic acid when evidence of biochemical failure was found . 
the ongoing icecap the most in men with appropriate hormone - sensitive prostate cancer . initiative51 should help de ne intermediate outcomes the two trials rigorous systematic review methods helped us treatment identify all relevant comparisons , they were irrespective of whether completed or reported . 
this approach allowed us to decide prospectively when we would be likely to have su cient data and power to detect meaningful e ects of docetaxel or bisphosphonates in combination with standard of care , at least in the m1 disease setting . 
 despite knowing that there would be fewer data and less power to assess the e ects of both treatments in the non - metastatic disease setting than in the metastatic disease setting , we have been able to establish early signals of both bene t ( docetaxel ) and no bene t ( bisphosphonates ) , consistency of results with those in metastatic disease , and whether new data are likely to change the results . 
by using an approach that is responsive to the emerging trial results and adaptive to potential future data , we have been able to achieve robust answers to speci c therapeutic questions quickly and determine which meta - analyses will need updating in the future and which will require individual patient data for more reliable and detailed results . in summary , for men with metastatic prostate cancer starting therapy for the rst time , we found strong evidence to support the addition of docetaxel to androgen deprivation therapy as the new standard of care , and this combination should be o ered to men who are t to receive chemotherapy . 
more reliable evidence of the e ect of docetaxel on overall survival and prostate cancer - speci c survival is still needed in the m0 disease setting and will be achieved through our planned collaborative international meta - analysis of individual participant data . 
 although additional trials are yet to be reported , the suggestion from our analyses is that any likely bene t of zoledronic acid will probably be small and not clinically meaningful . contributors sb , clv , lhmr , jft , mrs , and df comprised the project management group and , with the help of la , nwc , kf , gg , ndj , mdm , mkbp , cjs , and bt ( the international advisory group ; appendix p 6 ) , contributed to the conception of the study . 
the international advisory group contributed to the interpretation of the results and various revisions of the article . declaration of interests la has been on advisory boards at amgen and sano  . 
cjs has been a consultant for sano , janssen , astrellas , bind therapeutic , leuchemix , and bayer healthcare , has stock ownership in bind therapeutics and genentech , has patents in parthenolide ( dimethylaminoparthenolide ) as a cancer treatment and a patent pending with exelixis . 
mrs has received educational grants from astrellas , janssen , novartis , p zer , and sano - aventis and has received drug and distribution costs from merck & co . 
clv , sb , lhmr , nwc , df , gg , mkbp , and jft declare no competing interests . acknowledgments the stopcap steering group thanks all patients who participated in the trials and contributed to this research . 
the project management group was funded by the uk medical research council . olaparib in patients with metastatic castration - resistant prostate cancer with dna repair gene aberrations ( toparp - b ) : a multicentre , open - label , randomised , phase 2 trial joaquin mateo * , nuria porta * , diletta bianchini , ursula mcgovern , tony elliott , robert jones , isabel syndikus , christy ralph , suneil jain , mohini varughese , omi parikh , simon crabb , angus robinson , duncan mclaren , alison birtle , jacob tanguay , susana miranda , ines figueiredo , george seed , claudia bertan , penny flohr , berni ebbs , pasquale rescigno , gemma fowler , ana ferreira , ruth riisnaes , rita pereira , andra curcean , robert chandler , matthew clarke , bora gurel , mateus crespo , daniel nava rodrigues , shahneen sandhu , aude espinasse , peter chatfield , nina tunariu , wei yuan , emma hall , suzanne carreira , johann s de bono summary background metastatic castration - resistant prostate cancer is enriched in dna damage response ( ddr ) gene aberrations . 
the toparp - b trial aims to prospectively validate the association between ddr gene aberrations and response to olaparib in metastatic castration - resistant prostate cancer . methods in this open - label , investigator - initiated , randomised phase 2 trial following a selection ( or pick - thewinner ) design , we recruited participants from 17 uk hospitals . 
men aged 18 years or older with progressing metastatic castration - resistant prostate cancer previously treated with one or two taxane chemotherapy regimens and with an eastern cooperative oncology group performance status of 2 or less had tumour biopsies tested with targeted sequencing . 
patients with ddr gene aberrations were randomly assigned ( 1 : 1 ) by a computer - generated minimisation method , with balancing for circulating tumour cell count at screening , to receive 400 mg or 300 mg olaparib twice daily , given continuously in 4 - week cycles until disease progression or unacceptable toxicity . 
the primary endpoint of confirmed response was defined as a composite of all patients presenting with any of the following outcomes : radiological objective response ( as assessed by response evaluation criteria in solid tumors 1.1 ) , a decrease in prostate - specific antigen ( psa ) of 50% or more ( psa50 ) from baseline , or conversion of circulating tumour cell count ( from 5 cells per 75 ml blood at baseline to < 5 cells per 75 ml blood )  . 
recruitment for the trial has completed and follow - up is ongoing . findings 711 patients consented for targeted screening between april 1 , 2015 , and aug 30 , 2018 . 
161 patients had ddr gene aberrations , 98 of whom were randomly assigned and treated ( 49 patients for each olaparib dose ) , with 92 evaluable for the primary endpoint ( 46 patients for each olaparib dose )  . 
confirmed composite response was achieved in 25 ( 543% ; 95% ci 390691 ) of 46 evaluable patients in the 400 mg cohort , and 18 ( 391% ; 251546 ) of 46 evaluable patients in the 300 mg cohort . 
radiological response was achieved in eight ( 242% ; 111423 ) of 33 evaluable patients in the 400 mg cohort and six ( 162% ; 62320 ) of 37 in the 300 mg cohort ; psa50 response was achieved in 17 ( 370% ; 232525 ) of 46 and 13 ( 302% ; 172461 ) of 43 ; and circulating tumour cell count conversion was achieved in 15 ( 536% ; 339725 ) of 28 and 13 ( 481% ; 287681 ) of 27 . 
the most common grade 34 adverse event in both cohorts was anaemia ( 15 [ 31% ] of 49 patients in the 300 mg cohort and 18 [ 37% ] of 49 in the 400 mg cohort )  . 
one death possibly related to treatment ( myocardial infarction ) occurred after 11 days of treatment in the 300 mg cohort . interpretation olaparib has antitumour activity against metastatic castration - resistant prostate cancer with ddr gene aberrations , supporting the implementation of genomic stratification of metastatic castration - resistant prostate cancer in clinical practice . funding cancer research uk , astrazeneca , prostate cancer uk , the prostate cancer foundation , the experimental cancer medicine centres network , and the national institute for health research biomedical research centres . copyright 2019 the author ( s )  . 
before starting this study , several genomic landscape studies were published describing an enrichment for aberrations in dna repair genes in metastatic prostate cancers ( studies identified in pubmed , searching for prostate cancer , genomics , and biopsy , between jan 1 , 2010 and nov 1 , 2015 , with no language restrictions )  . 
preclinical and clinical studies identified in pubmed ( searching for cancer , parp , and brca or dna repair between jan 1 , 2005 and july 1 , 2019 , with no language restrictions ) have established a correlation between different dna repair defects and sensitivity to parp inhibition in different tumour types , leading to drug approvals in ovarian and breast cancer . 
in the toparp - a trial , we identified an association between somatic alterations in dna repair genes and antitumour activity of olaparib in 49 patients with metastatic prostate cancer . 
other clinical trials of parp inhibitors in prostate cancer were identified on the clinicaltrials.gov website , searching for prostate cancer and parp for studies published from database inception to july 1 , 2019 , without language restriction . added value of this study to our knowledge , toparp - b is the first prospective clinical trial in a genomically defined population of patients with metastatic prostate cancer . 
this study has confirmed the antitumour activity of olaparib against metastatic prostate cancer with defective dna repair secondary to either germline or somatic gene inactivation . implications of all the available evidence randomised phase 3 trials for dna repair - defective prostate cancers are now ongoing based on the toparp data . 
our results , if confirmed in registration studies , would support the implementation of tumour genomic testing in clinical practice for treatment stratification in advanced prostate cancer . these drugs have introduction molecular stratification for treatment is not currently the standard of care for metastatic prostate cancers despite evidence of substantial interpatient genomic hetero geneity . 
most therapeutic strategies for advanced prostate cancers target androgen receptor signalling ; taxane based chemotherapies and radiopharmaceuticals are also approved.1 although improved outcomes in the past decade , metastatic prostate cancer remains invariably fatal and new therapeutic strategies involving molecular stratification are urgently needed . 
 genomic studies of metastatic prostate cancer have identified a number of potentially actionable recurrent genomic lossoffunction alterations in dna repair genes in 2025% of cases , such as defects in homologous recombinationmediated repair genes.3 among these , germline or somatic alterations in brca2 are the most common , accounting for 612% of cases across studies.24 these data underpin the evaluation of poly ( adpribose ) polymerase ( parp ) inhibitors in metastatic prostate cancer.5 , 6 aberrations , 24 including olaparib is an orally bioavailable inhibitor of the catalytic activity of parp1 and parp2 , which have key roles in dna damage response ( ddr )  . 
olaparib is approved for the treatment of advanced ovarian and breast cancers associated with germline brca1 or brca2 mutations.7 it is also approved as a maintenance therapy after response to platinumbased chemotherapy for ovarian cancer , indicating benefit from parp inhibition beyond tumours with brca1 / 2 mutations.8 , 9 furthermore , olaparib has antitumour activity in vitro and in vivo in models that are defective in other ddr proteins , including palb2 , atm , fancd2 , rad51 , and rad54 , among others , although the magnitude of preclinical sensitisation varies between proteins , with brca2 loss being arguably the most potent sensitising event.10 , 11 to evaluate the antitumour activity of olaparib against metastatic castrationresistant prostate cancer , we designed toparp , an adaptive programme of serial phase 2 clinical trials aimed at identifying predictive biomarkers for response to parp inhibition in metastatic castrationresistant prostate cancer . 
in the first trial , toparpa , we identified an association between putatively deleterious ddr gene aberrations and res ponse to olaparib in 49 molecularly unselected patients.12 in this article , we present the results of toparpb , which was designed to validate the observed antitumour activity of olaparib in patients with metastatic castration resistant prostate cancer presenting with ddr gene aberrations . methods study design and participants toparpb is a multicentre , openlabel , investigator initiated , randomised phase 2 trial . 
patients were recruited from 17 uk hospitals ( appendix p 2 )  . patients with prostate cancer that had developed metastasis and castration resistance were first registered on the trial for molecular preselection by targeted next generation sequencing ( ngs ) of primary or metastatic prostate cancer biopsies . 
other inclusion criteria included : documented prostate cancer progres sion at trial entry , defined by either rising prostate specific antigen ( psa ) serum concentration ( according to the prostate cancer working group 2 [ pcwg2 ] criteria13 ) or radiologically ( according to modified response evaluation criteria in solid tumors [ recist ] version 1.114 or by bone scan as per pcwg2 criteria ) ; a castrate testosterone concentration of less than 50 ng / dl ; an eastern cooperative oncology group ( ecog ) perfor mance status of 2 or less ; and adequate organ function ( including haemoglobin 9 g / dl after a protocol amend ment on march 15 , 2018 [ previously 10 g / dl ] , platelets 100 10 per l , serum creatinine 15 times the institu tional upper limit of normal , and albumin > 25 g / l )  . 
 tumour cells the baseline count ( cellsearch system ; menarini silicon biosystems , castel maggiore , italy ) had to be five cells per 75 ml blood or higher except in patients with radiologically measurable target lesions of 2 cm or more in diameter on the baseline ct scan and a psa concentration of 2 ng / ml or higher on screening . 
the complete study protocol is available in the appendix . treated with parp for circulating the study was approved by the londonsurrey borders research ethics committee ( rec reference 11 / lo / 2019 ) , and cosponsored by the royal marsden nhs foundation trust and the institute of cancer research ( icr ) , london , uk . 
patients provided written informed consent before enrolment , both for the ngs prescreening and treatment stages . randomisation and masking eligible patients were randomly allocated ( 1 : 1 ) to receive olaparib at 300 mg ( approved dose for the tablet formulation in ovarian and breast cancer15 ) or 400 mg twice a day . 
the allocation sequence was generated centrally by a computergenerated mini misation algorithm derived by the icrctsu , with circulating tumour cell count at screening ( 5 cells per 75 ml blood vs < 5 cells per 75 ml blood ) as a balancing factor . 
further details on the sample processing , quality control , bioinformatics pipelines , and panel design are available in the appendix ( pp 57 ) .16 patients previously known to have germline aberrations were eligible only on confirmatory tumour testing by ngs . all patients received oral olaparib ( 300 mg or 400 mg , tablet formulation ) twice daily continuously in 4week cycles until evidence of radiographic progression ( based on recist 1.1 for soft tissue disease , or the appearance of 2 lesions on bone scan ) , unacceptable toxicity according to investigator review , or patient decision to discontinue . 
patients treated with 300 mg twice daily were offered the option of dose escalation to 400 mg twice daily on confirmation of radiographic progression , providing the escalation was considered to be clinically indicated by the treating physician and the patient had not previously required a dose reduction for management of toxicity . examination , routine blood clinical assessments , including reviews of adverse events ( according to the national cancer institute common terminology criteria for adverse events [ ctcae ] version 4.02 ) and ecog performance status , physical tests and ( haematology and biochemistry ) , took place 2 weeks after the start of treatment , and then at the start of every new 4week cycle . 
local radiological response assessments were used for the primary endpoint definition ; all recist 1.1 responses were confirmed by central review by radiologists at icr ( ac and nt )  . 
circulating tumour cell counts were centrally analysed at the cancer biomarkers laboratory at icr ( by pf , be , and gf ) and results were not made available to the treating physician . 
psa serum measure ments were collected every cycle if available , and every 164 vol 21 january 2020 articles 12 weeks at a minimu blood samples for correlative biomarker studies were taken every 4 weeks . 
to be judged a response confirmation in a second consecutive assessment at least 4 weeks later was required . secondary endpoints were : radiographic progression free survival , defined as the time from randomisation to first evidence of radiographic progression ( according to recist 1.1 or bone scan as per pcwg2 criteria ) or death ; time to radiographic progression , defined as the time from randomisation to first evidence of radiographic progression ; progressionfree survival , defined as the time from randomisation to radiographic progression , unequivocal clinical pro gression , or death ; overall survival , defined as the time from randomisation to death from any cause ; time to psa progression , defined as a confirmed increase of 25% or more and an absolute increase of 2 ng / ml or more in psa from the nadir ( pcwg2 ) ; duration of psa response , defined as the time from the first documented psa decrease of 50% or greater to psa progression ; best percentage change in psa from baseline while on treatment ; percentage change in psa from baseline at 12 weeks ( or earlier if therapy was discontinued ) ; proportion of patients with circulating tumour cell count conversion ; and the safety and tolerability profile of olaparib . a prespecified exploratory endpoint was response in patients in whom dose was escalated to 400 mg twice daily after progression on 300 mg twice daily . 
a pharma cokinetics substudy was planned but because of patients declining recruitment it was closed prematurely with no analyses pursued . statistical analysis this trial followed a selection ( or pickthewinner ) design.18 each dose cohort was assessed independently for the primary endpoint . 
the sample size needed to show the minimum desired antitumour activity was determined on the basis of aherns onestage design , with a response of 30% or less for the null hypothesis , and a response of more than 50% for the alternative hypothesis ( onesided level of 005 and a level of 015 )  . 
following the ahern design , if at least 19 ( 43% ) of 44 evaluable patients in a dose cohort responded , then the dose cohort would be considered successful . 
if the 400 mg twice daily dose cohort was deemed successful , the ddr biomarker identified in toparpa , in which all patients received 400 mg twice daily , would be considered validated as being predictive of response . 
no formal interim analyses were planned . for the primary endpoint , the evaluable population was defined as all randomly assigned patients who met all of the eligibility criteria and commenced trial treatment , unless they discontinued treatment prior to 12 weeks for reasons that were not related to the study drug or disease . 
sensitivity analyses of the primary endpoint were done in the intentiontotreat ( itt ) population ( all randomly assigned patients ) and per protocol population ( all evaluable patients who received at least one cycle of olaparib and had no eligibility violations )  . 
a posthoc sensitivity analysis in patients with a circulating tumour cell count of five or more cells per 75 ml blood at baseline was done for comparison with toparpa results . 
toxicity was analysed in all patients who received at least one dose of olaparib , and the worst grades of adverse events that occurred during treatment for each dose cohort are reported . 
serious adverse events and deaths observed within 30 days of the last dose of study treatment were summarised by dose cohort , as well as the exposure to study drug and reasons for discon tinuation , dose modification or interruption , and treatment delay . ( in for analysis of the primary endpoint was triggered when all patients had completed at least 6 months of treat ment the absence of prior discontinuation )  . 
for time to radiographic progression , patients who did not progress radiologically were censored at the last scheduled disease assessment during the study or date of death , whichever occurred first . 
 * non - mutually exclusive subgroups : one patient had brca1 / 2 , cdk12 , and other mutations , and two patients had both palb2 and other mutations ( included in each subgroup )  . 
assessment of ctc count at screening not possible due to ctc kit shortage ; the patient was allowed to be randomly assigned as he had recist 11 measurable disease ; for randomisation ctc count was assumed to be < 5 cells per 75 ml blood but the patient was unevaluable for ctc response . 
five nonmutually exclusive subgroups were predefined : patients with alterations in brca1 / 2 , atm , cdk12 , palb2 , and any other gene related to ddr or associated with parp inhibitor sensitivity . 
the corresponding author had full access to all data in the study and had final responsibility for the decision to submit for publication . to ngs prescreening results between april 1 , 2015 and aug 30 , 2018 , 711 patients consented ( figure 1a )  . 
from 681 patients with at least one sample available , 779 tumour samples were analysed ( 637 [ 82% ] primary tumour samples and 142 [ 18% ] postcastration resistance metastatic biopsies )  . 
 * non - mutually exclusive subgroups : one patient treated at 300 mg had brca1 / 2 , cdk12 , and other mutations , and two patients treated at 300 mg had both palb2 and other mutations . 
one - sided exact binomial 95% confidence intervals . table 2 : overall antitumour activity of olaparib in patients with dna damage response gene aberrations by dose cohort and gene subgroup sample or the sequencing data not fulfilling quality control parameters . of the 592 patients with evaluable tissue samples , 161 ( 27% ) had ddr gene aberrations on the basis of ngs . 
the most commonly detected ddr gene aberrations were mutations or homozygous deletions in brca2 ( 44 [ 7% ] of the 592 patients ) , atm ( 40 [ 7% ] ) , and cdk12 ( 33 [ 6% ] )  . 98 patients with ddr gene aberrations were randomly assigned and treated in the two dose cohorts ( 49 patients in each cohort )  . 
a greater number of participants were recruited than originally planned , at the recommendation of the independent data monitoring committee , to account for six participants ( three in each cohort ) who were deemed not evaluable ( ineligible post randomisation ) for the primary end point analyses . 
baseline features of each gene aberration subgroup are summarised in the appendix ( p 8 )  . 92 patients ( 46 in each dose cohort ) were evaluable for the primary endpoint . 
70 ( 76% ) patients were evaluable for the recist 1.1 response , 89 ( 97% ) for psa response , and 55 ( 60% ) for circulating tumour cell conversion . 
 a confirmed com posite response was observed in 25 ( 543% ; 95% ci 390691 ) of 46 patients in the 400 mg cohort and 18 ( 391% ; 251546 ) of 46 patients in the 300 mg cohort ( p = 014 ; table 2 )  . 
radiological response according to recist 1.1 was observed in eight ( 242% ; 95% ci 111423 ) of 33 evaluable patients in the 400 mg cohort and six ( 162% ; 62320 ) of 37 in the 300 mg cohort ; psa50 response was observed in 17 ( 370% ; 232525 ) of 46 and 13 ( 302% ; 172461 ) of 43 , respectively ; and circulating tumour cell count conversion was observed in 15 ( 536% ; 339725 ) of 28 and 13 ( 481% ; 287681 ) of 27 , respectively . 
based on the first 44 evaluable patients included in each cohort ( as planned initially ) , 25 ( 57% ) confirmed responses were recorded in the 400 mg cohort and 18 ( 41% ) in the 300 mg cohort ; thus , the predefined criteria for success was met for the 400 mg regimen but not for the 300 mg regimen . when including in the analysis only the 55 evalu able patients with a circulating tumour cell count of 5 cells per 75 ml blood at baseline , confirmed composite response was observed in 17 ( 607% ; 95% ci 406785 ) of 28 evaluable patients in the 400 mg cohort and 13 ( 481% ; 287681 ) of 27 in the 300 mg cohort ( appendix p 9 )  . 
in keeping with previous reports , 17 , 20 circulating tumour cell conversions posttreatment were significantly associated with longer radiographic progressionfree survival and overall survival in landmark analyses ( appendix p 15 )  . the best percentage change from baseline in psa concentration and in the sum of target lesions in each patient in the intentiontotreat population are pre sented in figure 2a and 2b . 
at the time of analysis , 45 ( 92% ) of 49 patients on 400 mg olaparib and 46 ( 94% ) of 49 patients on 300 mg olaparib had radio graphic progression or died ; median radiographic progressionfree survival was 55 months ( 95% ci 4483 ) in the 400 mg cohort and 56 months ( 3777 ) in the 300 mg cohort ( figure 2c )  . 
39 ( 80% ) patients on 400 mg and 38 ( 78% ) patients on 300 mg had died , with a median overall survival of 143 months ( 97189 ) in the 400 mg cohort and 101 months ( 90177 ) in the 300 mg cohort . 
 ( d ) swimmers plot of time on treatment for each patient , indicating periods of treatment interruptions , dose reductions , and , in the 300 mg cohort , dose escalations . 
a summary of treatment dose reductions , escalations ( 300 mg cohort ) , interruptions , and discontinuations in each dose cohort is presented in the appendix ( p 10 )  . dose escalation from 300 mg to 400 mg was pursued in 11 patients . 
none of these patients achieved a response after dose escalation . the confirmed composite response , and response by individual components , for each of the predefined gene subgroups are shown in table 2 . 
the brca1 / 2 subgroup had the highest number of responses both for the composite endpoint of confirmed response and across all its component outcomes ( table 2 ) and the longest median radiographic progressionfree survival ( figure 3c ) of all ddr gene aberration subgroups . 
of the 32 patients in the brca1 / 2 subgroup , 13 had germline mutations in brca2 , six somatic mutations in brca2 , 11 homozygous deletions in brca2 , and the remaining two cases had mutations in brca1 ( one germline and one somatic )  . 
 ten patients in the brca1 / 2 subgroup ( five allocated to 400 mg and five to 300 mg ) remained on treatment for more than 1 year . 21 patients with suspected deleterious atm aber rations were treated ( table 1 ; one patient with homozygous deletion and the rest with germline or somatic mutations that are predicted to result in either truncation or missense mutations affecting the kinase domain ) , and 19 were evaluable for response ( table 2 )  . 
conversely , four of seven patients with palb2 mutations responded to treatment ( table 2 )  . 20 patients were evaluated in the subgroup with other gene alterations associated with ddr or parp inhibitor sensitivity ( table 2 )  . 
psa50 responses were seen in two patients : one with a somatic nonsense mutation in fanca and one with a chek2 mutation . the safety population included all 98 patients treated ( table 3 )  . 
the tolerability profile was in line with what has been previously reported for olaparib and other parp inhibitors.2123 the most common grade 34 adverse event in both cohorts was anaemia ( 15 [ 31% ] in the 300 mg cohort and 18 [ 37% ] in the 400 mg cohort )  . 18 ( 37% ) patients in the 400 mg cohort and six ( 12% ) in the 300 mg cohort required at least one dose reduction ( appendix p 10 ) , with anaemia being the most common adverse event leading to dose reductions ( two patients in the 300 mg cohort and nine in the 400 mg cohort )  . 
 overall , 18 ( 19% ) of the 98 patients were permanently discontinued from olaparib treatment due to adverse events ( appendix p 10 ) the most common adverse events leading to discon tinuation were anaemia ( two of five patients who discontinued on 400 mg and five of 13 on 300 mg ) and fatigue ( three on 400 mg and four on 300 mg )  . 107 serious adverse events were 49 ( 50% ) patients ( 300 mg cohort : 49 events in 22 patients ; 400 mg cohort : 58 events in 24 patients ) with 19 serious reported 170 vol 21 january 2020 articles adverse reactions ( possibly related to study drug ; 11 in the 300 mg cohort and eight in the 400 mg cohort ) in 13 patients ( 8 patients in the 300 mg cohort and 5 in the 400 mg cohort )  . 
all other deaths were unrelated to treatment ( n = 76 ; 70 due to disease and six due to other causes )  . discussion the toparpb trial has confirmed the antitumour activity of olaparib against metastatic castrationresistant prostate cancer with specific ddr gene aberrations . 
the number of composite responses observed in the cohort of patients who received 400 mg tablets of olaparib twice daily met the predefined criteria for success , validating the ddr biomarker identified in toparpa as being predictive of response.12 overall , the data suggest that both drug dose and the specific type of ddr gene aberration might influence antitumour activity , given that the composite response at the 300 mg regimen was lower and did not reach the predefined criteria for success . 
the antitumour activity observed varied considerably for different ddr gene aberrations , with the greatest antitumour activity seen in the subgroup with brca1 / 2 alterations . despite randomisation , cdk12 aberrations were imbalanced between the cohorts , with an enrichment in the 300 mg cohort . 
this imbalance might explain , at least in part , the inferior composite response in the 300 mg cohort.4 , 24 the rationale to explore the two doses originated from prior clinical observations indicating a doseresponse relationship for olaparib between 100 mg and 400 mg at twice daily dosing , although 400 mg has been associated with enhanced toxicity.25 , 26 in keeping with this finding , 37% patients at 400 mg had to reduce their dose to 300 mg , most commonly because of anaemia . 
all of these data would need to be considered when assessing the optimal dose of olaparib for prostate cancer treatment . our results support the implementation of routine genomic testing of metastatic prostate cancer , to detect dna repair defects for targeting by parp inhibition . 
 * one death due to myocardial infarction ( grade 5 event deemed a suspected unexpected serious adverse reaction ) was reported ( not included in table )  . table 3 : treatment - emergent adverse events germline ngs testing in all men with metastatic prostate cancer per national comprehensive cancer network guidelines . 
the antitumour activity of olaparib indicated in this trial , in patients with metastatic castration resistant prostate cancer with both germline and somatic aberrations of brca2 , now supports the implementation of ngs testing of tumour samples . antitumour activity was also observed in other ddr gene aberration subgroups . 
circulating conversely , germline and somatic atm aberrations are common in metastatic prostate cancer ; atm functions as a cell cycle checkpoint , preventing cell cycle progression in the presence of dna damage rather than directly mediating repair , unlike brca2 and palb2 . 
in the toparpa trial , five patients had atm aberrations in tumour biopsies : two of these had a psa response , and two more had circulating tumour cell conversion . 
 preliminary results suggest that rucaparib , another parp inhibitor , results in few psa decreases in patients with atm aberrations.30 in toparpb , we treated 21 patients with suspected deleterious atm aberrations : two achieved a recist or psa response , and several others had circulating tumour cell count conversions following tumour cell count decreases seen in this subgroup were associated with increased duration on the trial , tumour shrinkage per recist , and a psa decrease , as was the case for the overall toparpb population , with circulating tumour cell conversions robustly associating with increased radiographic progressionfree survival and overall survival . 
overall , the data suggest that the antitumour activity of olaparib in metastatic castrationresistant prostate cancer with atm loss is less than that for brcaaltered tumours ; nevertheless , a subset of patients with atm - altered metastatic castrationresistant prostate cancer appear to derive benefit . 
further studies , as well as the study of rational drug combinations , are now needed to elucidate how to best evaluate and treat metastatic castrationresistant prostate cancer with atm alter ations . 
furthermore , because all patients in our study had ddr gene aberrations and received olaparib , we are not able to fully differentiate the predictive value versus the prognostic effect of the gene aberrations in terms of survival . 
randomised trials including patients with and without the biomarkers will be more able to clinically qualify putative predictive biomarkers . nonetheless , the results from toparpb have overall driven the design and conduct of several registration trials of parp inhibitors in metastatic castration resistant prostate cancer ( nct02987543 , nct02975934 , and nct03148795 ) , which are likely to guide the clinical use of parp inhibitors in metastatic prostate cancer in the future . 
other studies , in parallel , are exploring the addition of parp inhibitors to the standardofcare drugs targeting the androgen receptor ( nct03732820 and nct03395197 ) , on the basis of results from a phase 2 clinical trial indicating that a broader target population than just patients with gene aberrations might benefit from these drugs.31 in conclusion , the data from toparpb have confirmed the antitumour activity of olaparib against meta static prostate cancer with particular ddr gene aberrations . 
the high response observed in patients with metastatic castrationresistant prostate cancer with germline or somatic brca1 / 2 aberrations , and the durability of many of these responses , support the use of olaparib in this subpopulation . 
the antitumour activity observed against tumours with atm , palb2 , fanca , or chek2 aberrations suggest that parp inhibitors might have a role as single drug therapies or in rational combinations against these other subtypes of metastatic prostate cancer , although further data are needed to precisely assess the clinical relevance of each of these different ddr gene aberrations in prostate cancer . contributors jm , np , ss , eh , and jsdb designed the trial . 
rj reports grants and personal fees from astellas , astrazeneca , exelixis , and roche ; personal fees and nonfinancial support from bristolmyers squibb , janssen pharmaceutica , ipsen , and merck sharp & dohme ; grants , personal fees , and nonfinancial support from bayer ; and personal fees from merck serono , novartis , pfizer , sanofi genzyme , and eusa , outside of the submitted work . 
ab reports advisory board fees and speaker fees from sanofi and bayer , advisory board fees from astellas , speaker fees from janssen pharmaceutica , merck sharp & dohme , and roche , and provision of educational support to janssen pharmaceutica , outside of the submitted work . 
ss reports grants and consultancy honoraria from bristolmyers squibb , merck sharp & dohme , and roche , and grants from endocyte and astrazeneca , outside of the submitted work . 
she also reports grants and nonfinancial support from merck sharp & dohme , astrazeneca , and bayer ; and grants from janssen pharmaceutica , kyowa kirin , alliance pharma , sanofi , and accuray , outside of the submitted work . 
 he also reports personal fees and nonfinancial support from astellas pharma , sanofi , and menarini silicon biosystems ; grants , personal fees , and nonfinancial support from astrazeneca , daiichi , sierra oncology , and cellcentric ; personal fees from genentech , pfizer , bayer , boehringer ingelheim , merck serono , and merck sharp & dohme ; and nonfinancial support from genmab , glaxosmithkline , orion pharma , qiagen , taiho pharmaceutical , and vertex , outside of the submitted work . 
jsdb has an abiraterone rewards to inventors patent with royalties paid to the institute of cancer research ( icr ; london , uk ) , and a parp inhibitors and dna repair defects patent with royalties paid to icr . 
the authors affiliated to icr disclose that the institution is a joint applicant for the patent entitled dna damage repair inhibitors for treatment of cancer , which includes the granted application us8143241 . 
 all other authors declare no competing interests . data sharing the institute of cancer research clinical trials and statistics unit ( icrctsu ) , london , uk , supports the wider dissemination of information from the research it does , and increased cooperation between investigators . 
trial data is collected , managed , stored , shared , and archived according to icrctsu standard operating procedures to ensure the enduring quality , integrity , and use of the data . 
data recipients are required to enter a formal data sharing agreement that describes the conditions for release and requirements for data transfer , storage , archiving , publication , and intellectual property . 
data sharing is permitted if proposed projects have a sound scientific or patient benefit rationale as agreed by the trial management group and approved by the icrctsu independent data monitoring and steering committee as required . 
 additionally , all indirect identifiers that might lead to deductive disclosures will be removed in line with cancer research uk data sharing guidelines . acknowledgments we are grateful for the support and funding from astrazeneca , and for the study grants from cancer research uk ( cruk / 11 / 029 , c12540 / a12829 , c12540 / a13230 , and c12540 / a20447 ) , prostate cancer uk and the movember foundation through the london movember centre of excellence ( ceo13_2002 ) , and the prostate cancer foundation ( 20131017 )  . 
the institute of cancer research ( icr ) clinical trials and statistics unit ( icrctsu ) , london , uk , also receives programme grant funding from cancer research uk ( c1491 / a15955 and c1491 / a25351 )  . 
we also acknowledge support from the uk national institute for health research ( nihr ) cancer research network and the uk national health service ( nhs ) funding to the nihr biomedical research centre at the royal marsden nhs foundation trust and icr ( london , uk ) , and support from the uk experimental cancer medicine centres network . 
the views expressed in this article are those of the author ( s ) and not necessarily those of the uk national health service , the nihr , or the uk department of health . 
we thank all patients and their families for participating in this study , all staff involved at the vol 21 january 2020 articles 17 participating hospitals , and the staff involved in the trial at the cancer biomarkers group at icr , at the prostate cancer targeted therapy group at the royal marsden hospital ( london , uk ) , and at icrctsu . 
we assessed whether rituximab use could delay the need for chemotherapy or radiotherapy compared with watchful waiting and the e ect of this strategy on quality of life ( qol )  . methods asymptomatic patients ( aged 18 years ) with low - tumour - burden follicular lymphoma ( grades 1 , 2 , and 3a ) were randomly assigned centrally ( 1 : 1 : 1 ) , by the minimisation approach strati ed by institution , grade , stage , and age , to watchful waiting , rituximab 375 mg / m weekly for 4 weeks ( rituximab induction ) , or rituximab induction followed by a maintenance schedule of 12 further infusions given at 2 - monthly intervals for 2 years ( maintenance rituximab )  . 
there was a signi cant di erence in the time to start of new treatment , with 46% ( 95% ci 3953 ) of patients in the watchful waiting group not needing treatment at 3 years compared with 88% ( 8392 ) in the maintenance rituximab group ( hazard ratio [ hr ] 021 , 95% ci 014031 ; p < 00001 )  . 
78% ( 95% ci 6987 ) of patients in the rituximab induction group did not need treatment at 3 years , which was signi cantly more than in the watchful waiting group ( hr 035 , 95% ci 022056 ; p < 00001 ) , but no di erent compared with the maintenance rituximab group ( 075 , 041134 ; p = 033 )  . 
compared with the watchful waiting group , patients in the maintenance rituximab group had signi cant improvements in the mental adjustment to cancer scale score ( p = 00004 ) , and illness coping style score ( p = 00012 ) between baseline and month 7 . 
 there were 18 serious adverse events reported in the rituximab groups ( four in the rituximab induction group and 14 in the maintenance rituximab group ) , 12 of which were grade 3 or 4 ( ve infections , three allergic reactions , and four cases of neutropenia ) , all of which fully resolved . interpretation rituximab monotherapy should be considered as a treatment option for patients with asymptomatic , advanced - stage , low - tumour - burden follicular lymphoma . funding cancer research uk , lymphoma research trust , lymphoma association , and roche . low - grade introduction findings from retrospective analyses of asymptomatic lymphoma patients with advanced - stage , showed no reduction in overall survival when systemic treatment was deferred until development of symptoms or organ failure , 1 , 2 which generally occurred about 30 months after diagnosis . 
these ndings were subsequently con rmed in three randomised trials.35 in the largest of these trials , 3 309 patients were randomly assigned to either watchful waiting or an intensive chlorambucil regimen . 
at a median follow - up of 16 years , there was no survival advantage to early start of treatment , and at 10 years , 19% of patients still did not need advanced - stage , chemotherapy . 
these trial data support the widely practised strategy of watch and wait in asymptomatic low - tumour - burden patients with follicular lymphoma , which is based on the assumption that the delay in exposure to chemotherapy and its attendant side - e ects would result in an improved quality of life ( qol )  . 
this assumption has not been formally assessed , and there is anecdotal evidence that in some patients this strategy can lead to a worse qol because patients nd being diagnosed with a malignant disorder without receiving treatment psychologically demanding . rituximab is a chimeric monoclonal antibody directed against cd20 . 
low tumour burden was de ned as normal lactate dehydrogenase , largest nodal or extranodal mass less than 7 cm , up to three nodal sites containing nodes with a diameter greater than 3 cm , no clinically signi cant serous e usions detectable by physical examination or ct scan , and spleen enlargement up to 16 cm by ct . this trial was overseen by an independent trial steering committee and independent data monitoring committee . 
 the protocol was approved by the uk medicines and articles of sydney , sydney , nsw , australia ( prof k bradstock phd ) correspondence to : dr kirit m ardeshna , department of haematology , university college hospital , 250 euston road , london nw1 2pg , uk kirit.ardeshna@uclh.nhs.uk for the trial protocol see trialprotocols.aspx 484 patients enrolled 21 excluded 8 reasons unknown 7 not eligible 1 stage 1 disease 5 high tumour burden 1 reason not stated 3 physician started treatment 1 second malignancy discovered 1 consent withdrawn 1 diagnosis revised to mantle - cell lymphoma 463 patients randomly assigned 187 patients assigned to watch and wait * 84 patients assigned to rituximab induction 192 patients assigned to maintenance rituximab * 2 stopped early because of toxicity 1 missing information 1 missing information 81 received four infusions 191 received four induction infusions 36 stopped early 156 received 12 maintenance infusions 187 included in intention - to - treat population 84 included in intention - to - treat population 192 included in intention - to - treat population figure 1 : trial pro le on sept 30 , 2007 , recruitment into the rituximab induction group was closed and the study was amended to a two - arm study . 
 * inclusive of the patients enrolled in the three - arm study ( 83 in the watch and wait group and 85 in the maintenance rituximab group )  . vol 15 april 2014 articles healthcare products regulatory agency and cambridge south research ethics committee , and was done in accordance with the declaration of helsinki and the eu clinical trials directive . 
all patients provided written informed consent before enrolment . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to be carefully observed until treatment was needed ( watchful waiting ) , to receive rituximab induction , or to receive maintenance rituximab . 
some percentages do not total 100% because of rounding . table 1 : demographics and baseline characteristics procedures patients randomly assigned to the rituximab induction group received intravenous rituximab ( 375 mg / m ) every week for 4 weeks ( rituximab induction ) , while those in the maintenance rituximab group received the same rituximab induction followed by 12 infusions of rituximab given at 2 - monthly intervals for 2 years . 
no dose reductions were recommended . clinical assessments including full blood count and renal and liver function tests were done at baseline , 1 month , and then every 2 months for 2 years or until start of treatment . 
a bone marrow trephine biopsy was taken for restaging only if patients were in complete remission or uncon rmed complete remission on radiological assessment at month 7 , 13 , or 25 , or before starting rst chemotherapy or radiotherapy . safety data were collected while patients in the rituximab induction and maintenance groups were on treatment with rituximab and for up to 30 days afterwards unless a late complication of rituximab was reported . qol was assessed at baseline ( before randomisation ) , after randomisation ( within 1 week and before treatment ) , at each clinic visit during the rst 2 years , and then every 6 months for 2 years . 
the questionnaires used were the functional assessment of cancer therapygeneral ( fact - g ) , hospital anxiety and depression scale ( hads ) , impact of event scalerevised , and questions from the illness coping style , illness impact bank , and mental adjustment to cancer scale together with four additional questions relating to lymphoma ( appendix )  . and scales summary subscales or emotional wellbeing , for each qol questionnaire were derived according to their score manuals . 
there are four subscales of the fact - g questionnaire : physical wellbeing , social or family wellbeing , functional wellbeing , each scored 0100 , with higher scores suggesting better qol . 
the hads is summarised by anxiety and depression subscales , which are classi ed as normal ( score 07 ) , borderline ( score 810 ) , and case ( score 1114 )  . 
there are 27 items in the impact of event scalerevised questionnaire , which are summarised as avoidance , intrusions , and hyperarousal subscales ; scores of all subscales are scaled as 0100 , with higher scores suggesting better qol . 
one summary measure each is derived from the illness coping style , the illness impact bank , and the mental adjustment to cancer 426 vol 15 april 2014 articles scale questionnaires ; scores of each are scaled as 0100 , with higher scores suggesting better qol . outcomes the primary outcome measures were the time to start of new treatment and qol at month 7 ( 6 months after completion of induction treatment )  . 
progression - free survival and time to histological transformation were analysed post hoc . time to start of new treatment was calculated from the date of randomisation to the date of starting new systemic chemotherapy or radiotherapy . 
 we recognised that de ning clearly when disease progression is su cient to warrant the start of chemotherapy or radiotherapy is di cult and so we provided a detailed guidance ( appendix )  . 
standard criteria for response assess ment were used.8 survival was de ned as time from random isation to death from any cause ( overall survival ) or progression or death from any cause ( progression - free survival )  . 
 statistical analysis with an estimated median time to start of new treatment of 30 months in the watchful waiting arm , the original three - arm trial was designed to detect an improvement in the median time to start of new treatment in each of the rituximab groups of 18 months ( from 30 to 48 months ) with a 25% signi cance level ( allowing for the multiple comparisons ) and 90% power . 
recruitment of 600 patients was planned . on sept 30 , 2007 , about 3 years after the start of enrolment , recruitment into the rituximab induction group was closed because of a low recruitment rate and because other studies had shown a bene t of maintenance rituximab compared with watchful waiting after induction with rituximab with or without chemotherapy , 9 , 10 although in only one of these studies was the rituximab induction administered as a monotherapy . 
this change was approved by the independent trial steering committee , independent data monitoring committee , and regulatory and ethics committees . for the two - arm trial , the study was redesigned to detect an improvement in the median time to start of new treatment in the maintenance rituximab arm of 18 months ( from 30 to 48 months ) with a 5% signi cance level and 90% power . 
recruitment of 360 patients was planned . the primary analysis was done using an unstrati ed log - rank test for the di erence in the distribution of time to start of new treatment between the di erent groups . 
interaction analyses were done to assess the di erence in the size of treatment e ects in subgroups classi ed according to age , sex , stage , follicular lymphoma international prognostic index , 11 and 2 microglobulin concentration . 
however , on march 26 , 2010 , the independent data monitoring committee concluded that the data regarding the clinical primary outcome measure were mature and suitable for full analysis and publication . 
this decision was approved by the independent trial steering committee . watch and wait overall remission spontaneous complete remission spontaneous partial remission uncon rmed complete response no change disease progression rituximab induction overall response complete response partial response no change disease progression maintenance rituximab overall response complete response partial response no change disease progression data are n / n ( % )  . 
 the change in qol from baseline to month 7 within each arm was also compared between the arms and this was judged to be the most important comparison . except for anxiety or depression subscales , a change of 5 points for a subscale was regarded as the minimum clinically signi cant di erence . 
statistical analyses were done using sas version 9.2. this study is registered with clinicaltrials.gov , nct00112931 , and eudract , 2004 - 001621 - 16 . role of the funding source the trial sponsor ( university college london ) was responsible for randomisation , data collection , entry , and validation ; monitoring procedures ; reporting of serious adverse events ; organisation of central pathological review ; liaison with investigators ; data analysis ; and writing of the report . 
roche , the lymphoma association , and the lymphoma research trust had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between oct 15 , 2004 , and march 25 , 2009 , 463 patients were randomly assigned from 118 centres in the uk , australia , new zealand , turkey , and poland . 
252 patients were randomly assigned in the original three - arm study ( 83 to the watchful waiting group , 84 to the rituximab induction group , and 85 to the maintenance rituximab group )  . 
in the two - arm study , 379 patients were randomly assigned between the watchful waiting group ( n = 187 ) and the maintenance rituximab group ( n = 192 ; gure 1 )  . 
 a time to start of new treatment b progression - free survival watch and wait maintenance rituximab hr 021 ( 95% ci 014031 ) log - rank p < 00001 number at risk watch and wait maintenance rituximab hr 023 ( 95% ci 016032 ) log - rank p < 00001 c overall survival d time to histological transformation hr 073 ( 95% ci 034154 ) log - rank p = 040 number at risk watch and wait maintenance rituximab hr 062 ( 95% ci 031126 ) log - rank p = 019 years from randomisation years from randomisation figure 2 : kaplan - meier curves for the two - arm study ( a ) time to start of new treatment , ( b ) progression - free survival , ( c ) overall survival , and ( d ) time to histological transformation . 
 428 vol 15 april 2014 articles a time to start of new treatment b progression - free survival watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 035 ( 95% ci 022056 ) ; log - rank p < 00001 maintenance rituximab vs rituximab induction hr 075 ( 95% ci 041134 ) ; log - rank p = 033 number at risk watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 055 ( 95% ci 037083 ) ; log - rank p = 00034 maintenance rituximab vs rituximab induction hr 053 ( 95% ci 032087 ) ; log - rank p = 0011 c overall survival d time to histological transformation rituximab induction vs watch and wait hr 104 ( 95% ci 039280 ) ; log - rank p = 093 maintenance rituximab vs rituximab induction hr 112 ( 95% ci 043290 ) ; log - rank p = 082 years from randomisation number at risk watch and wait rituximab induction maintenance rituximab rituximab induction vs watch and wait hr 034 ( 95% ci 011106 ) ; log - rank p = 0052 maintenance rituximab vs rituximab induction hr 147 ( 95% ci 042522 ) ; log - rank p = 055 years from randomisation figure 3 : kaplan - meier curves for the 252 patients randomly assigned in the initial three - arm study ( a ) time to start of new treatment , ( b ) progression - free survival , ( c ) overall survival , and ( d ) time to histological transformation . 
 the 4 - week rituximab induction was administered to all patients except for two patients in the rituximab induction group who only received one and three infusions , respectively , because of toxicity . 
 maintenance was stopped because of progressive disease or new treatment ( n = 13 ) ; other illness taking priority or resulting in death ( n = 5 ) ; infection ( n = 3 ) ; patient choice ( n = 6 ) ; reclassi cation as di use large b - cell lymphoma ( n = 1 ) ; neutropenia ( n = 3 ) ; or uncertain reasons ( n = 2 )  . 
there were no dose reductions . 18 serious adverse events occurred in the two rituximabcontaining groups , which were considered possibly , probably , or de nitely related to the rituximab : nine infections ( induction group n = 1 , maintenance group n = 8 ) , ve allergies ( induction group n = 3 , maintenance group n = 2 ) , and four neutropenia ( all in the maintenance group )  . 
there were ve grade 3 infections in the maintenance rituximab group ( two pneumonia , one viral meningitis , one de - novo hepatitis b infection , and one urinary tract infection )  . 
 vol 15 april 2014 articles the fourth patient developed grade 3 neutropenic sepsis 5 months after randomisation and was treated with antibiotics and granulocyte colony - stimulating factor and the rituximab was stopped . 
there were no other grade 3 or 4 adverse events . the rate of spontaneous remissions in the watchful waiting group was low : by month 25 , only 15 ( 12% ) of 128 patients had shown radiological regressions over 50% ( ie , overall remission ) , with only eight ( 6% ) patients having a spontaneous complete remission or uncon rmed spontaneous complete remission . 
162 ( 88% ) of 184 patients in the maintenance rituximab group had had a response at 7 months , as had 144 ( 83% ) of 173 at 25 months . 
 radiologically identi ed complete responses , or un conrmed complete responses , were noted in 109 ( 59% ) of 184 patients at month 7 and in 130 ( 75% ) of 173 patients at month25 ( table 2 )  . analysis of the 252 patients recruited to the three - arm study showed that there were signi cantly more overall responses in the maintenance rituximab group than in the rituximab induction group at both month 7 ( 77 / 85 [ 91% ] vs 62 / 81 [ 77% ] ; p = 0043 ) and month 25 ( 67 / 80 [ 84% ] vs 43 / 75 [ 57% ] ; p = 0001 ; appendix )  . 
 investigator compliance with bone marrow examination when a radiological complete remission or uncon rmed complete remission was achieved was suboptimum ; incorporation of these ndings underestimated rates of complete remission or uncon rmed complete remission ( appendix )  . 
 in the two - arm study , 105 ( 56% ) of 187 patients in the watchful waiting group and 33 ( 17% ) of 192 patients in the maintenance rituximab group needed new treatment ; the reason for starting new treatment was disease progression except for six ( 4% ) patients ( three watch and wait ( n = 187 ) rituximab induction ( n = 84 ) maintenance rituximab ( n = 192 ) total breast lung colorectal squamous cell stomach prostate basal - cell carcinoma melanoma pancreas unknown primary hodgkins lymphoma total table 3 : list of second malignancies patient choice in the watchful waiting group , one clinician choice in the watchful waiting group , and one in each group reclassi ed as di use large b - cell lymphoma )  . 
 the estimated median time to start of new treatment was 311 months ( 95% ci 255460 ) in the watchful waiting group and has not been reached in the maintenance rituximab group . 
at 3 years , the estimated percentage of patients not needing new treatment was 46% ( 95% ci 3953 ) in the watchful waiting group , and 88% ( 8392 ) in the maintenance rituximab group ( hr 021 , 95% ci 014031 ; p < 00001 ; gure 2a )  . 
all prespeci ed patient subgroups showed prolongation of time to start of new treatment with maintenance rituximab . in the three - arm study , 97 of 252 patients randomly assigned into the three - arm study needed to start new treatment : 52 ( 63% ) of 83 in the watchful waiting group , 25 ( 30% ) of 84 in the rituximab induction group , and 20 ( 24% ) of 85 in the maintenance rituximab group . 
for patients randomly assigned to the rituximab induction group , the median time to start of new treatment has not been reached and new treatment had not been started in 78% ( 95% ci 6987 ) of patients at 3 years . 
the hr was 035 ( 95% ci 022056 ; p < 00001 ) for rituximab induction versus watchful waiting and was 075 ( 041134 ; p = 033 ) for maintenance rituximab versus rituximab induction ( gure 3a )  . 
exploratory analyses of patient subgroups are summarised in the appendix . in the two - arm study , 121 ( 65% ) of 187 patients in the watchful waiting group and 43 ( 22% ) of 192 patients in the maintenance rituximab group had either developed progressive disease or died . 
median progression - free survival was 241 months ( 95% ci 171253 ) in the watchful waiting group , but has not yet been reached in the maintenance rituximab group . 
3 - year progression - free survival was 36% ( 95% ci 2943 ) in the watchful waiting group and 82% ( 7788 ) in the maintenance rituximab group ( hr 023 , 95% ci 016032 ; p < 00001 ; gure 2b )  . in the three - arm study , 41 ( 49% ) of 84 patients in the rituximab induction group had either developed progressive disease or died . 
3 - year progression - free survival was 60% ( 95% ci 4971 ) in the rituximab induction group , which was signi cantly di erent from the other two arms : hr 053 ( 95% ci 032087 ; p = 0011 ) for the comparison between maintenance rituximab and rituximab induction and hr 055 ( 037083 ; p = 00034 ) for the comparison between rituximab induction and watchful waiting ( gure 3b ; appendix )  . in the two - arm study , 28 ( 7% ) of 379 patients had died : 16 ( 9% ) of 187 in the watchful waiting group and 12 ( 6% ) of 192 in the maintenance rituximab group . 
eight patients died in the rituximab induction group , giving a 3 - year overall survival of 96% ( 95% ci 92100 ) , with no di erence between the three groups ( gure 3c ; appendix )  . 
six second malignancies occurred in the rituximab induction group , two were fatal ( table 3 )  . by data cuto ( sept 8 , 2012 ) , 33 patients had had biopsy - proven transformation in the two - arm study ( 20 [ 11% ] of 187 in the watchful waiting group and 13 [ 7% ] of 192 in the maintenance rituximab group )  . 
a further four patients have had biopsyproven transformation in the rituximab induction group , with no evidence of di erences between the rituximab group and the other groups in the three - arm study ( gure 3d ; appendix )  . time table 4 summarises the qol results for the two - arm study at month 7 . 
there was a signi cant improvement in the mental adjustment to cancer scale score from baseline to month 7 in the maintenance rituximab group ( p = 00001 ) that did not occur in the watchful waiting group ( p = 019 )  . 
compared with baseline , scores at month 7 for the illness coping style were much the same in the maintenance rituximab group ( p = 0072 ) and deteriorated in the watchful waiting group ( p = 00063 )  . 
 patients in the maintenance rituximab group were also signi cantly less worried about the need for treatment or more treatment than patients in the watchful waiting group by month 7 compared with baseline ( p = 00037 )  . 
 there were no other clinically signi cant di erences between the two arms in all other qol measures between baseline and month 7 ; all measures either improved or remained unchanged between baseline and month 7 ( table 4 )  . this di erence was signi cant in the three - arm study , there was no evidence of di erence in qol between baseline and month 7 when the rituximab induction group was compared with the watchful waiting group . 
in accordance with these data , more patients in the watchful waiting group had started new treatment compared with those in the rituximab induction group , and also compared with those in the maintenance rituximab group . 
the nding that the administration of rituximab delayed progression and time to start of new treatment is not surprising , but the magnitude of remarkable , with more than three times fewer patients needing treatment by 3 years in the maintenance rituximab group than in the watchful waiting group . 
the di erence between the time to start of new treatment in the rituximab induction and maintenance groups was not signi cant , but the start of new treatment lags behind progression and once the trial was amended to two arms , the trial was underpowered for the comparison of the two rituximab groups . this e ect longer follow - up is needed to ascertain the median time to progression and time until new treatment becomes necessary in the rituximab - containing groups , but three other studies are relevant to this issue . 
colombat and colleagues6 updated the results of their phase 2 study in patients with previously untreated low - tumour - burden follicular lymphoma who received infusions of rituximab induction without maintenance every 4 weeks . 
in the sakk 35 / 98 study , 9 , 10 standard rituximab induction was administered and patients were randomly assigned to observation or four further doses of rituximab given at 2 - monthly intervals . 
in the subgroup of previously untreated patients ( not all asymptomatic or with low tumour burden ) who responded to induction , 22% remained event free without maintenance at 8 years compared with 45% in the maintenance group . 
similarly , in the resort study , 12 the proportion of patients remaining free of cytotoxic treatment at 3 years was signi cantly greater receiving extended maintenance rituximab than in those receiving rituximab re - treatment upon progression . those in the present study , we chose time to start of new treatment rather than progression - free survival as the primary endpoint . 
we acknowledge that there is some subjectivity as to when treatment is needed , even when guidance is provided , but oncologists are familiar with making this decision in routine clinical practice and this pragmatic endpoint is of greatest relevance to the patient . 
 the de nition of progression covers a wide spectrum of clinical scenarios , some of which would not warrant the start of treatmenteg , the appearance of a new small nodethus reducing its utility in patients with indolent lymphoma . 
 * worsened or stayed as very much , quite a bit , or somewhat . table 4 : quality of life at baseline and month 7 from randomisation duration after rst new treatment as well as time to second new treatment . 
preliminary data from the us lymphocare study14 suggest that the time to second systemic treatment is signi cantly longer in patients who received rituximab monotherapy than in those who were initially on watchful waiting . 
the estimated 5 - year overall survival in the watchful waiting arm in the present study is over 90% , which compares favourably with the 58% in our previous study.35 this di erence , in the space of fewer than two decades , is substantial and probably due in baseline patient characteristics between the two studies and newer treatment options that have become available . 
for example , in our initial study , bulk disease per se was not an exclusion criterion , there was no requirement for a to di erences treatment in the watchful waiting group was very close to that reported in previous studies1 , 35 further shows the reproducibility of this endpoint . findings from this trial also show that rituximab induction can be delivered without a reduction in qol : patients receiving maintenance rituximab actually had an improvement in some aspects of their qol when compared with those on watchful waiting . 
at month 7 , patients in the maintenance rituximab group were signi cantly more likely to feel in control of their situation than those in the rituximab induction group and the watchful waiting group , as shown by the mental adjustment to cancer scores . 
conversely , patients in the watchful waiting group were signi cantly more likely to avoid learning or thinking about their illness and to have unpleasant connotations with their clinic visits , as shown by the illness coping style scores , and to be worrying about the need for treatment than those in the maintenance rituximab group . 
therefore , the administration of rituximab does not seem to negatively a ect patients qol and patients who receive a maintenance schedule seem to feel more empowered and better adjusted to their diagnosis . 
this nding might be because these patients felt that something active was being done to combat their lymphoma , and many of them would have noticed physical evidence such as lymph nodes shrinking to suggest that this was the case . rituximab monotherapy seems to be well tolerated , with only eight cases of grade 3 infection or allergy . 
this nding might be a result of the fact that patients included in the study were well at the outset , had low tumour burden , and had not received treatment previously . 
follow - up is short so far and long - term sequelae of rituximab might appear ; however , rituximab has been in use for 15 years and the follow - up of patients treated in other trials with rituximab is extensive . so far there is no overall survival di erence between the three groups , and much longer follow - up will be needed to assess the e ect of this strategy on overall survival . 
we have extended the follow - up of this study to collect information regarding response and response vol 15 april 2014 articles panel : research in context systematic review we searched pubmed from january , 1987 , until august , 2013 , for randomised trials published in english with the terms lymphoma and watchful waiting or observation or delayed treatment . 
we found three randomised studies , 35 each of which showed no survival bene t when systemic treatment was started immediately in patients with advanced - stage asymptomatic low - tumourburden low - grade lymphoma compared with a watchful waiting approach in which treatment was deferred until disease progression . 
there were no other studies comparing watchful waiting with the administration of rituximab monotherapy in this patient group . interpretation in this study , we show that rituximab monotherapy is e ective at deferring disease progression and the need for chemotherapy or radiotherapy in patients with asymptomatic low - tumour - burden follicular lymphoma , and when administered as a maintenance schedule it can be delivered with minimum toxicity and results in improved quality of life compared with watchful waiting . 
however , probably the most important reason for the improvement in overall survival is the routine therapeutic use of monoclonal antibodies . with a median follow - up of nearly 4 years , there was no di erence in the incidence of histological transformation between the three groups . 
previous retrospective studies have di ered as to whether a watchful waiting approach increased the risk of transformation ; that a di erence will emerge is not inconceivable and further follow - up is clearly necessary.15 , 16 we found that maintenance rituximab compared with rituximab induction had a numerically greater e ect on time to initiation of new treatment in women than in men . 
although the heterogeneity of to sex was not signi cant , response with regard gisselbrecht and colleagues17 also found that maintenance rituximab improved overall survival when compared with observation in women , but not in men , when administered after autologous stem - cell transplantation for relapsed refractory di use large b - cell lymphoma . 
the reason for this nding is unclear , but might relate to the di erential clearance of rituximab from the serum between the sexes.18 management options for patients with low - tumourlymphoma burden are varied and include watchful waiting , immediate asymptomatic follicular that rituximab time . 
in this study we show induction alone can delay chemotherapy and is not signi cantly less e ective than a m aintenance schedule ; however , the number of responses was lower and the rate of progression after induction alone was signi cantly higher than that after maintenance . 
thus , a di erence in time to start of new treatment will probably emerge between these two the cost approaches with associated with the administration of maintenance rituximab over 2 years and that the use of rituximab induction alone was attractive in terms of reduced number of hospital visits for administration of rituximab and cost , but the improvements in qol that occurred with the maintenance schedule did not occur for rituximab induction alone . 
this absence in improvement of qol might have been because the amended study was not powered su ciently to show a qol di erence between the rituximab induction group and the watchful waiting group . 
however , despite this factor , patients receiving maintenance rituximab still had a signi cant improvement in their mental adjustment to cancer score between baseline and month 7 compared with those receiving rituximab induction alone , suggesting a qol bene t of the maintenance approach between randomisation and month 7 . watchful waiting might still be appropriate for some patients . 
we have previously shown that 40% of patients over 70 years of age will never need any treatment and will not die of their lymphoma ; 3 however , this nding must be balanced against the improved qol achieved with maintenance rituximab . 
 furthermore , by administering rituximab to the whole group of patients older than 70 years , an even larger cohort might never need chemotherapy , which would be advantageous in view of the comorbidities and the reduced ability to withstand the side - e ects of treatment in this age group . 
if watchful waiting is used , clinicians will need to be alert to whether the patient is anxious that no treatment is experiencing feelings of is being administered , helplessness , or is having di culty adjusting to their diagnosis . 
if these are substantial concerns then the treatment approach should be reconsidered . in conclusion , our results suggest that rituximab monotherapy should be regarded as a standard approach in the management of many patients with asymptomatic , low - tumour - burden follicular lymphoma . 
the full results of other studies that address the optimum schedule of rituximab monotherapy administration , such as the resort study , 12 are awaited with interest . 434 vol 15 april 2014 articles contributors kma and dcl designed the study , interpreted data , and wrote and approved the report . 
all authors have reviewed and approved the nal version of the report . declaration of interests kma has received funding from roche for being an advisory board member , speaker , and data manager , and for travel and accommodation at international conferences . 
dcl has been chair of an oversight committee for cellmedica , adviser for cellectsis , an advisory board member and speaker for roche and chugai , and an advisory board member for millenniuwq , ps , nb , ll , pp , jwar , ls , fm , rs , bf , and kb declare that they have no competing interests . acknowledgments roche provided rituximab free of charge . 
we aimed to establish agreement between these ssps for identi cation of breast cancer molecular subtypes . methods previously described microarray - based ssps were applied to one in - house ( n = 53 ) and three publicly available ( n = 779 ) breast cancer datasets . 
the proportion of cases classi ed as basal - like in each cohort was consistent irrespective of the ssp used ; however , the proportion of each remaining molecular subtype varied substantially . 
 however , di erent ssps produced broadly similar survival curves . interpretation although every ssp identi es molecular subtypes with similar survival , they do not reliably assign the same patients to the same molecular subtypes . 
for molecular subtype classi cation to be incorporated into routine clinical practice and treatment decision making , stringent standardisation of methodologies and de nitions for identi cation of breast cancer molecular subtypes is needed . funding breakthrough breast cancer , cancer research uk . introduction breast cancers are a diverse and heterogeneous group of diseases , and clinicopathological features and the status of oestrogen receptor and her2 guide treatment of patients . 
microarray - based gene expression pro ling has led to a paradigm shift in the way breast cancer is perceived , and has shown conclusively that breast cancer is not a single disease at the molecular level.16 the molecular heterogeneity of breast cancer and its implications are gradually being incorporated into clinical trial design , 7 and treatment strategies are being tailored to speci c subgroups of patients with breast cancer whose tumours have particular molecular aberrations ( eg , trastuzumab or lapatinib for women with her2 - positive disease )  . 
breast cancers can be classi ed by hierarchical cluster analysis , using an intrinsic gene list , into one of ve molecular subtypes : luminal a , luminal b , basal - like , her2 , and normal breast - like.15 , 8 however , this approach can only be applied retrospectively to su ciently sized cohorts of patients.8 an alternative strategy for classi cation of single samples into one of these molecular subtypes is the single sample predictor ( ssp ) , 35 which is based on similarities between a given case and molecular subtype centroids.3 , 4 breast cancer molecular subtypes identi ed by these approaches have been clinical presentations , 9 sites of relapse , 10 histological features , 11 responses to chemotherapy , 5 , 12 and outcomes.2 , 4 , 8 , 13 to have distinct suggested for consistent and clinically applicable molecular subtype assignment of breast cancers , a standardised methodology with reproducible results is fundamental.13 in the past 10 years , ve distinct intrinsic gene lists15 and three di erent ssps35 have been described to classify breast cancers into molecular subtype classes . 
molecular subtypes identi ed in separate studies with di erent ssps are assumed to be similar , if not identical , with respect to their clinical , biological , and prognostic characteristics ( ie , luminal a cancers in study a identi ed by the ssp - a are synonymous with luminal a cancers in study b identi ed by the ssp - b )  . 
nevertheless , some researchers have advocated that this molecular taxonomy should be used to design clinical studies6 , 14 and to guide decision - making regarding therapy.14 this assumption has not been the aims of this study were to assess the clinical usefulness of ssps by establishing agreement between di erent methods of breast cancer molecular subtype vol 11 april 2010 articles for the r code used see rock.icr.ac.uk / collaborations / mackay / for arrayexpress see see online for webappendix assignment ( ie , do di erent ssps assign the same patients to the same molecular subtype ? ) , and to ascertain whether each ssp identi es molecular subtypes with similar associations with outcome . 
to address these objectives , we analysed a cohort of consecutive invasive ductal carcinomas of no special type of histological grade iii , which were microdissected to minimise the e ect of varying amounts of stromal contamination , 15 and three cohorts of breast cancer samples the public domain.1618 methods sample collection we obtained 64 anonymised samples of consecutively accrued grade iii invasive ductal carcinomas of no special type from hospital la paz , madrid , spadetails of this cohort are described elsewhere.15 we de ned her2 status with us food and drug administration ( fda ) - approved methods for immuno histochemistry and dual - colour uorescence in - situ hybridisation ( fish ) as previously described , 19 and we scored status according to guidelines of the american society of clinical oncology and college of american pathologists ( webappendix pp 14 ) .20 we micro dissected representative frozen sections of tumours to ensure a consistent proportion of at least 90% tumour cells , and we extracted rna with trizol ( invitrogen , paisley , uk ) as previously described.15 53 cases produced su cient rna of optimum quality and underwent geneexpression pro ling with the illumina human wg6 version 2 array ( illumina inc , san diego , usa )  . 
the local research ethics committees approved this project . we analysed breast cancers from the publicly available nki - 295 ( n = 295 ) , 16 wang ( n = 286 ) , 17 and transbig ( n = 198 ) 18 datasets for molecular subtype classes and association with outcome . 
we obtained normalised microarray - based gene - expression data and clinical ndings from the ( nki - 295 , 22 wang internet or public repositories [ geo : gse2034 ] , transbig [ geo : gse7390 ] )  . 
details for the cohorts are provided in the webappendix ( p 5 )  . procedures methods related to mapping of centroid / ssp gene lists and breast cancer datasets and molecular subtype assignment are described in detail in the webappendix ( pp 14 )  . 
we have attempted to follow details for ssp analysis described in published work.35 to minimise the need to make assumptions , we tested several methods of gene and probe annotations and of handling of multiple probes for the same gene ( webappendix pp 14 )  . 
 table 1 : molecular subtype classi cations of breast cancers 340 vol 11 april 2010 articles for ensembl see ensembl.org previously published23 , 24 molecular subtype assignments of the nki - 295 dataset cancers with ssps described by sorlie and colleagues3 and hu and coworkers.4 in brief , annotations of centroid / ssp gene lists and breast cancer datasets were comprehensively updated and mapped to build 36 of the human genome ( ensembl assembly 54 ) ; annotation overlays were done with human genome organisation ( hugo ) gene symbols . 
to de ne whether a tumour pertained to the basal - like , her2 , luminal a , luminal b , or normal breastlike molecular subtype class , we correlated the gene expression of each tumour with 500 gene centroids by sorlie and colleagues3 ( sorlies ssp ) , 306 gene centroids by hu and coworkers4 ( hus ssp ) , and 50 gene centroids ( pam50 ) by parker and colleagues5 ( parkers ssp )  . 
we judged values of 001020 slight agreement , 021040 fair agreement , 041060 moderate agreement , 061080 substantial agreement , and 081099 almost - perfect agreement.26 survival curves were calculated by the kaplan - meier method and compared with the log - rank test . 
we applied a proportional - hazards model by coxs regression analysis to estimate hazard ratios and 95% ci for overall survival ( nki - 295 and transbig datasets ) and metastasis - free survival ( wang cohort , in addition to nki - 295 and transbig cohorts )  . 
in a multivariate analysis , tumour size was tted as continuous variable , tumour grade was tted as an ordinal variable , and oestrogen - receptor status and nodal status were tted as binary variables ( positive vs negative )  . 
in this case , we strati ed the cox model by dataset ; this process allowed baseline hazard functions to di er in each dataset but constrained the estimated hazard ratios to be the same across the datasets . 
it reduces the e ect of confounding on hazard ratio estimates caused by prognosis between di erent datasets but , similar to metainherent di erences 0740 ( 05660913 ) 0238 ( 01480328 ) sorlie ssp hu ssp basal luminal a luminal b normal her2 ( 95% ci ) basal luminal a luminal b normal her2 ( 95% ci ) 53 grade iii invasive ductal carcinomas 0274 ( 01730375 ) nki - 295 dataset hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 0532 ( 04620603 ) 0528 ( 04560601 ) 0656 ( 05920721 ) ( continues on next page ) vol 11 april 2010 articles ( continued from previous page ) wang dataset transbig dataset hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 sorlie ssp hu ssp basal luminal a luminal b normal her2 ( 95% ci ) basal luminal a luminal b normal her2 ( 95% ci ) 0439 ( 03550522 ) 0393 ( 03310455 ) 0459 ( 03940524 ) 0404 ( 03280480 ) 0488 ( 03880587 ) 0475 ( 03980553 ) ssp = single sample predictor . table 2 : agreement between single sample predictors for molecular subtype assignments analysis , it uses all co horts in one analysis , maximising the power to detect e ects . statistical analyses were done with r version 2.9.0 and spss version 11.5. 
 role of the funding source the sponsors had no role in study design , data collection , data analysis , data interpretation , writing of the report , or in the decision to submit for publication . 
bw , am , md , aa , and jsr - f took nal responsibility for the decision to submit the report for publication . results first , we sought to de ne the exact methods used previously to classify breast cancers according to three ssps . 
in the ssp analysis process , parameters and procedures were not described in su cient detail in the original publications.35 to minimise the need to make assumptions on methodology for assignment of molecular subtypes and to reduce inconsistencies in analysis methods , we aimed to reproduce the molecular the same gene subtype predictions of the nki - 295 dataset of breast cancers , which were previously classi ed into molecular subtypes by the sorlie or hu ssps ( webappendix pp 68 ) .23 , 24 agreement in molecular subtype assignment between the methods tested here and those previously published was 07150940 and depended on three factors : ( 1 ) use of di erent gene annotations for mapping of centroid / ssp gene lists and datasets ; ( 2 ) use of all probes identifying a gene versus averaging of multiple probes representing to establish correlations to a centroid / ssp gene list ; and ( 3 ) inclusion or exclusion of unclassi ed cases with a correlation less than 01 to any centroid.3 , 23 this cut - o was described by sorlie and colleagues3 as a conservative approach to include only cases with a strong correlation to a molecular subtype ( webappendix pp 14 , 9 )  . 
substantial agreement was noted ( 0646 [ 05650727 ] ) after exclusion of 109 unclassi ed cases with weak correlation ( < 01 ) to any centroids by sorlie and colleagues3 , 23 ( webappendix pp 68 )  . 
 we next ascertained molecular subtype classes ( table 1 ) and agreement between subtype assignments produced by the three distinct ssps in the four breast cancer cohorts ( table 2 , webappendix pp 1020 )  . 
we recorded only fair - to - moderate agreement between classi cations provided by sorlies and hus ssps ( 02740532 ; table 2 ) , moderate - to - substantial agreement between sorlies and parkers ssps ( 04390740 , table 2 ) , and fair - to - substantial agreement between hus and parkers ssps ( 02380656 ; table 2 , webappendix pp 1920 )  . 
 tables 1 and 2 show that in all four cohorts , the number of cases assigned to her2 , luminal a , luminal b , and normal breast - like molecular subtypes di ered remarkably , as did the number of unclassi ed cases with a correlation less than 01 to any centroid ( table 1 , gures 13 , webappendix pp 3137 )  . 
of the ve molecular subtypes , only the proportion of basal - like tumours was similar between the three distinct ssps tested . none of the microdissected grade iii invasive ductal carcinomas with a tumour - cell content of at least 90% nki - 295 dataset sorlie ssp 20033 patients er positive er negative grade 1 grade 2 grade 3 node positive node negative 2 cm > 2 cm basal - like her2 luminal a luminal b normal breast - like hu ssp 20064 parker ssp 20095 basal - like her2 luminal a luminal b normal breast - like patients at risk 29 p < 00001 sorlie ssp3 hu ssp4 parker ssp5 er status histological grade lymph - node status tumour size patients at risk 56 37 133 48 21 years patients at risk 25 years p < 00001 p < 00001 figure 1 : molecular subtype classi cation of nki - 295 breast cancers and overall survival of patients assigned to molecular substypes according to three single sample predictors er = oestrogen receptor . 
ssp = single sample predictor . vol 11 april 2010 articles sorlie ssp3 hu ssp4 parker ssp5 er status patients er positive er negative basal - like her2 luminal a luminal b normal breast - like patients at risk 53 basal - like 42 her2 171 luminal a 19 luminal b normal breast - like 1 wang dataset sorlie ssp 20033 hu ssp 20064 parker ssp 20095 p = 00372 patients at risk 49 104 124 0 patients at risk 54 15 65 139 13 years years p = 00017 p = 00133 figure 2 : molecular subtype classi cation of wang breast cancers and metastasis - free survival of patients assigned to molecular subtypes according to three single sample predictors er = oestrogen receptor . 
seven of 13 her2 - ampli ed grade iii invasive ductal carcinomasas indicated by immuno histochemistry and fishwere assigned to the molecular her2 subtype group with hus ssp , whereas the sorlie and parker ssps assigned all her2ampli ed cases to the luminal b subtype class ( webappendix p 10 )  . 
agreement between her2 , luminal a , and luminal b subtypes classi ed with sorlies , hus , or parkers ssps was generally only fair to moderate ( table 3 , webappendix p 21 )  . 
in the wang and transbig cohorts , concordance in assignment of tumours to luminal b class between sorlies and hus ssps , and between hus and parkers ssps , was only slight . 
almost - perfect concordance was noted only for classi cation of the basal - like subtype by all three ssps ( 08121000 ) , which was also recorded when unclassi ed cases were included in the analysis ( webappendix p 21 )  . 
our ndings show that , for assignment of her2 , luminal a , luminal b , and normal breast - like subtype classes , agreement between distinct ssps is only modest , but concordance for basal - like class is high . 
independent of the ssp used , molecular classi cation was associated signi cantly with overall survival survival ( webappendix p 31 ) in the nki - 295 dataset and with metastasis - free survival ( no information on overall survival is available publicly for this cohort ; gure 2 )  . 
these associations were also noted when unclassi ed cases ( ie , correlation < 01 to any centroid / ssp gene list ) were included in the analysis , with the exception of the assignment by sorlies ssp in the wang dataset ( webappendix pp 3234 )  . 
in the transbig data set , molecular subtypes were only associated signi cantly with overall survival ( gure 3 ) and metastasis - free survival ( webappendix pp 3537 ) when classi cations were made with hus ssp ; similar ndings were seen when un classi ed cases were included in the the wang dataset 344 vol 11 april 2010 articles transbig dataset sorlie ssp 20033 basal - like her2 luminal a luminal b normal breast - like patients er positive er negative grade 1 grade 2 grade 3 2 cm > 2 cm patients at risk 30 basal - like 11 her2 64 luminal a 90 luminal b 3 normal breast - like p = 00547 hu ssp 20064 parker ssp 20095 sorlie ssp3 hu ssp4 parker ssp5 er status histological grade tumour size patients at risk 40 30 119 0 years years p = 00067 p = 01118 figure 3 : molecular subtype classi cation of transbig breast cancers and overall survival of patients assigned to molecular subtypes according to three single sample predictors er = oestrogen receptor . 
importantly , the number and identity of cases assigned to molecular sub types in each cohort di ered by the ssp used , with the exception of basal - like subtype ( gures 13 , tables 1 and 2 )  . survival multivariate coxs hazard analysisincluding histological grade , tumour size , lymph node status , and oestrogen receptor statusshowed that , in the nki - 295 dataset , molecular subtypes only added independent prognostic information when assigned by the parker ssp for overall survival and by the hu and parker ssps for ( webappendix pp 2225 )  . 
 metastasis - free multivariate coxs hazard analysis of the transbig dataset ( lymph - node negative patients only ) , which included histological grade , tumour size , and oestrogen receptor status , indicated that molecular subtypes only added independent prognostic information when assigned by the hu ssp for overall survival and metastasis - free survival ( webappendix pp 2225 )  . 
for the wang dataset , no information on tumour size and histological grade was available publicly . to assess associations with outcome of each molecular subtype individually , circumventing the few samples assigned to each molecular subtype and maximising power to detect e ects , the nki - 295 , wang , and transbig cohorts were combined into one dataset ( table 4 )  . 
this analysis indicated that all ssps were prognostic for metastasis - free survival , and they were all prognostic for overall survival in the nki - 295 and transbig cohorts ( no overall survival data were available for the wang dataset )  . 
however , the signi cance of the association between luminal b and normal breast - like groups and metastasis - free survival was dependent on the ssp used for their assignment ( table 4 )  . discussion our ndings show that di erent ssps and methods used for molecular subtype assignment35 produce inconsistent results . 
the number of cases assigned to each molecular subtype di ered depending on the ssp used , and agreement for each class was modest ( ranging from fair to substantial ) , with the exception of the basal - like subtype . 
these results indicate that assignment of a given patient to a molecular subtype other than basal - like is strongly dependent on the ssp used and that results from studies of a speci c ssp cannot necessarily be generalised . 
this result could be accounted for in part by associations between molecular subtypes and clinico patho logical features linked to outcome ( webappendix pp 2629 ) and with expression levels of oestrogen receptor , her2 , and proliferationrelated genes ( webappendix pp 3861 )  . 
however , they suggest that the use of current ssps to allocate cases into her2 , luminal a , luminal b , and normal breast - like subtypes might be premature for strati cation of patients or in the context of clinical trials . the luminal b subtype was not identi ed reproducibly by di erent ssps . 
since distinction between luminal a and luminal b tumours seems to be driven by expression of proliferation - related genes , 4 , 14 the absence of consistency in allocation of these two subtypes should perhaps not come as a surprise . 
findings of several studies have shown that proliferation in oestrogen receptor - positive breast cancers is a continuum , 27 and allocation of speci c subgroups ( eg , luminal a and b ) might be arbitrary . one criticism levelled at molecular classi cation of breast cancer is that normal breast - like tumours could be an artifact derived from analysis of tumour specimens with a high proportion of normal tissue contamination.4 , 5 , 8 , 14 indeed , none of the microdissected breast cancer specimens with a tumour - cell content of at least 90% was assigned to the normal breast - like group ; however , the cases included in this study were all histological grade iii , and normal breast - like cancers were reported less frequently to be of grade iii in the nki - 295 series ( gure 1 , webappendix p 27 ) .11 despite several lines of evidence to suggest that the proportion of stromal cells has a substantial e ect on results of expression pro ling analysis and on gene classi ers , and that variable amounts of stromal cells in tumours introduce a confounding factor in interpretation of results of microarray analysis , 28 no previous study of molecular taxonomy of breast cancer has taken the degree of stromal contamination into account . 
 standardisation of tissue composition is needed if expression pro ling is to be used for breast cancer classi cation in clinical practice . several groups , including ours , have attempted to develop surrogate immunohistochemical markers for the molecular subtypes of breast cancer as de ned by microarrays ; 2931 however , results from these studies should be interpreted with caution , in view of the low stability of classes other than basal - like . 
in fact , validity of multiple surrogate markers for luminal b subtypes ( oestrogen receptor ( er ) - positive and / or progesterone receptor ( pr ) - positive , and her2 - positive ; 9 , 31 or er - positive and / or pr - positive and either her2positive and / or high ki67 expression ) 30 remains to be established . 
 table 4 : univariate and multivariate coxs regression analysis of overall and metastasis - free survival for the nki - 295 , wang , and transbig datasets combined metastasis - free survival overall basal - like her2 luminal b luminal a luminal b vs luminal a histological grade * oestrogen receptor status tumour size overall survival overall basal - like her2 luminal b luminal a luminal b vs luminal a histological grade * oestrogen receptor status tumour size between proposed immuno histochemical surrogates and microarray - de ned molecular subtypes.34 based subtyping should not be used to decide treatment for this group of patients . the pam50 method5 has provided an approach for breast cancer molecular classi cation , which is possibly clinically applicable ; however , reported agreement between the her2 pam50 - de ned subtype and her2 clinically positive cases ( as ascertained by immunohistochemistry and fish ) was only moderate.5 consistent with this observation , of cases classi ed as her2 - positive by fda - approved methods in our in - house dataset of grade iii invasive ductal carcinomas , just over half were assigned to the her2 molecular subtype by hus ssp , whereas all these cases were assigned to the luminal b subtype class by the other two ssps . 
these results show that the her2 group , as de ned by microarray gene pro ling analysis , does not equate with the clinical subgroup of her2 - positive breast cancers . 
since patients with her2 - positive cancers are eligible for targeted treatments ( ie , trastuzumab or lapatinib ) , extensive misassignment of these cases indicates that microarrayalthough microarray - based gene expression pro ling analysis has been reported as able to provide reasonably reproducible results for molecular classi cation of breast cancer , 3 , 4 our ndings show that without thorough standardisation , these tumours cannot be classi ed reliably by this approach . 
as emphasised by ioannidis and colleagues , 35 other investigators might only be able to predict molecular subtypes accurately when a detailed description of data processing and analytical methods is provided . 
 cancer molecular furthermore , careful standardisation of preanalytical variables that have a direct e ect on expression pro les , such as stromal component28 and tissue processing , 37 are equally crucial for development of reliable and reproducible classi ers . taxonomy vol 11 april 2010 articles limitations of our study include use of retrospectively accrued cohorts , the fact that three cohorts were retrieved from public repositories and some clinicopathological features were not available in one of the cohorts ( ie , tumour size and grade in the wang dataset ) , 17 and varied follow - up length in di erent datasets.1618 these limitations are also applicable to other studies of molecular taxonomy of breast cancer.13 for translation of current knowledge on the molecular features of breast cancer , the mechanisms of action of chemotherapy agents , and the availability of many compounds that target speci c molecular pathways or networks , molecular classi cations should have direct functional implications and be predictive of response to speci c therapeutic agents , rather than being descriptive and prognostic.8 , 38 , 39 this requirement is likely to need an integrative approach , combining descriptive data from su ciently powered cohorts40 and many sources , including clinicopathological features , massively parallel dna and rna sequencing , and proteomics , with detailed functional data from large panels of cancer models ( eg , high throughput rna interference and chemical screens ) .8 , 38 , 39 , 41 , 42 in conclusion , although ssps identify molecular subtypes with similar trends for association with outcome , they do not assign reliably the same patients to the same molecular subtypes . 
before molecular subtype classi cation can be incorporated into routine clinical practice and treatment decision making , standardisation of methodologies and stringent de nitions for identi cation of breast cancer molecular subtypes is needed . 
sufficient and sustainable health financing mitigates against social injustices and inequalitiesthey are therefore matters of human rights and the value of democracy . every nation will have a different process towards implementing universal health coverage and improved cancer control , yet international platforms , such as the commonwealth , create opportunities to work towards universal health coverage together . 
collaborative approaches can improve spending efficiency by minimising costs to health - care systems , obtaining a good return on investment in cancer services , optimising the workforce , and exploring procurement possibilities . commonwealth nations have made commitments to the promotion of universal health coverage and equity in cancer control . 
 the views expressed are those of the authors and not necessarily those of the institution with which they are affiliated . * andr ilbawi , gwenal dhaene , filip meheus , melanie bertram ilbawia@who.int department of noncommunicable diseases ( ai ) and department of health systems governance and financing ( gd , mb ) , world health organization , ch - 1211 geneva 27 , switzerland ; and section of cancer surveillance , international agency for research on cancer , lyon , france ( fm ) 2020 world health organization . 
report_2019.pdf ( accessed april 1 , 2020 )  . the role of the commonwealth in the wider cancer control agenda the number of new cases of cancer reported in the commonwealth nations rose by 35% between 2008 and 2018 . 
in 2018 , nearly 17 million people died from cancer in these countries : equivalent to one death every 18 seconds.1 estimates based on expected population growth predict a further 35% increase in incidence of cancer in the commonwealth in the next 12 years ( 201830 ) , and a 39% increase in cancer mortality.1 what should we expect the commonwealth to do about this worsening situation ? the core purpose of the commonwealth was affirmed by the commonwealth heads of government meeting ( port of spain , trinidad and tobago ) in the november , 2009 : we reaffirm our belief commonwealth as a voluntary association of sovereign influence independent states whose pursuit of common principles continues to international society to the benefit of all.2 it has long been the view of the head of the commonwealth that the commonwealth is not an organisation with a mission . 
it is rather an opportunity for its people to work together to achieve practical solutions to problems.3 where does this view leave population health care ? traditionally , this issue is low on the commonwealths list of priorities . 
access to health and education was ranked 10th of 12 core values listed in the 2009 affirmation.2 the influential 2011 report by the commonwealth eminent persons group to the commonwealth heads further discouragement.3 of government provides re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology department of radiation oncology , all india institute of medical sciences , new delhi , india sharmadn@hotmail.com the authors declared no con icts of interest . powell jw , dexter e , scalzetti em , bogart ja . 
long term results of endobronchial brachytherapy : a curative treatment ? int j radiat oncol biol phys 2007 ; 67 : 42530 . brach b , buhler c , hayman mh , joyner lr jr , liprie sf . 
 chest 2005 ; 127 : 223742 . screening newborns for tp53 in the september issue of the lancet oncology , achatz and colleagues1 discuss the possibility of screening newborns in southeast brazil for a highly prevalent tp53 mutation ( 1 : 300 individuals ) that predisposes to many cancers . 
the authors present the justi cations and the problems associated with such a screening e ort , and conclude that on the basis of current scienti c and medical knowledge the r337h mutation does not meet all the criteria for mass newborn screening . 
 in my opinion , this type of screening will never meet the criteria for newborn screening , which is intended to detect conditions for which the population is at risk but there is no other way to assess risk in newborns . 
newborn screening is done for sporadic diseases such as congenital hypothyroidism and autosomal recessive disorders , in which carrier detection is di cult or impossible , but never applies for a disorder caused by the presence of a founder dominant mutation . 
a founder mutation in a newborn will be carried by one of the parents , so the detection of the child can be done by knowing who the adult carrier is . 
cascade screening is the most economically e ective , o ering the screening test to rst - degree relatives of carriers of the mutation , and several countries have chosen this approach.2 the problem with this type of screening is that it involves the cooperation of relatives who are not always willing , and so an alternative has been the creation of databases to store information on patients.3 in my view , population screening of informed and consenting adults is much better suited for the tp53 mutation . 
 this approach identi es families at risk and has been implemented in pilot studies for haemochromatosis.4 as emphasised by achatz and colleagues , 1 such population screeningin the context of appropriate genetic counsellingallows at - risk families the informed decision of whether or not to test the probands o spring . joel zlotogora department of community genetics , ministry of health , jerusalem , israel joelz@cc.huji.ac.il the author declared no con icts of interest . achatz miw , hainaut p , ashton - prolla p . 
 clin genet 2004 ; 66 : 48387 . had eld sg , horara s , starr bj , et al ; steering group for the department of health familial hypercholesterolaemia cascade testing audit project . 
lancet oncol 2009 ; 10 : 940in this news report , the nal sentence of the 90y radioembolisation paragraph should have read only one patient experienced radiation - induced pneumonitis ; three had gastrointestinal ulcers that did not require surgical treatment , and radioembolisation - induced liver disease was noted in 24 patients ( fatal for four )  . huober j , thrlimann b . 
lancet oncol 2009 ; 10 : 102829in this re ection and reaction , the a liation for both authors should read breast center , kantonsspital st gallen , 9007 st gallen , switzerland . 
the authors would also like to thank karen price for her useful comments on the article . 1142 vol 10 december 2009 shortages of cancer drugs in the usa on feb 7 , 2011 , senators amy klobuchar and robert casey introduced the preserving access to life saving medications act . 
this new legislation means that manufacturers of prescription drugs will be required to notify the us food and drug administration ( fda ) when a drug is going to be discontinued or if any di culties arise that might a ect manufacture of a drug . 
 drug shortages in the usa have steadily increased in recent years , with 211 new shortages identi ed in 2010 compared with 166 in 2009 , 149 in 2008 , 129 in 2007 , and 70 in 2006 . 
furthermore , shortages are not just restricted to drugs , but also extend to medical supplieseg , technetium - 99m was in short supply after a nuclear reactor in canada , where it was produced , was temporarily closed down for repairs . 
so where does this leave health - care services , in particular cancer treatment , in the usa , and will changes in the legislation introduced earlier this year help ? 150 drugs are judged to be medically necessary . 
substitution of one drug with another might result in worse side - e ects or reduced e cacy , violate the protocol of a clinical trial , or lead to a shortage of the alternative drug . 
asco suggested substitution of leucovorin with levofolinate , which is much more expensive and is only approved by the fda for use as a rescue drug after administration of high - dose methotrexate in patients with osteosarcoma . 
 levofolinate irinotecan and uorouracil seems e ective in patients with metastatic colorectal cancer , but it is unclear whether addition in combination with of this agent to other chemotherapy regimens would replicate the responses expected of leucovorin ; thus there is a risk attached to this strategy . since one or only a few manufacturers are likely to be producing a particular generic drug , shortages are perhaps inevitable . 
the production of sterile injectable drugs takes a long time and is a complex process ; therefore , if one manufacturer is unable to produce a drug for whatever reason , other manufacturers might not be able , or willing , to ramp - up production . 
the reasons for drug shortages include increased demand ; di culties in obtaining , or discontinuations in , the bulk materials ; halted production in response to the fdas enforcement of good manufacturing practices ; change in formulation ; discontinuation because of insu cient nancial returns ; patent expiration ; mergers leading to discontinuation of one of two similar products ; and antitrust laws that prevent manufacturers from sharing information . because of concern about drug shortages in the usa , a drug shortages summit was convened on nov 5 , 2010 , in bethesda , md , usa , by the american society of health - system pharmacists ( ashp ) , american society of anesthesiologists , asco , and the institute for safe medication practices . 
before the klobucharcasey bill , manufacturers were only encouraged , but not required , to inform the fda of any di culties in the supply chathere is a risk that healthcare providers , after nding out about an impending drug shortage , might now decide to stockpile , which would only exacerbate the proble whether the fda will be able to enforce alternative or extended production remains to be seen . drug shortages mean that patients are not given the best treatment or that their treatment might be delayed . 
legally , non - fda - approved drugs ( including foreign - made versions of usa - approved drugs ) cannot be imported into the usa , and perhaps a solution would be either to relax some of the laws ( with appropriate safeguards ) to allow the import of life - saving treatments or to incentivise increased production in us facilities . 
 in this retrospective analysis , the relation between the reported incidence of vasomotor or joint symptoms and breast cancer recurrence in the arimidex , tamoxifen , alone or in combination ( atac ) trial is assessed . methods women with hormone - receptor - positive tumours who reported vasomotor or joint symptoms at the rst follow - up visit ( 3 months ) in the atac trial , ( which assessed tamoxifen or anastrozole for adjuvant treatment of postmenopausal breast cancer ) , were compared with women without these symptoms to see if there was a relation between these symptoms and subsequent recurrence . 
the atac trial is registered as an international standard randomised controlled trial , number isrctn18233230 . findings 1486 of 3964 ( 375% ) eligible women reported newly emergent vasomotor symptoms at the 3 - month followup visit and had lower subsequent recurrence than those who did not report these symptoms ( 223 during 10 752 women - years of follow - up vs 366 during 11 573 woman - years of follow - up , respectively ; hazard ratio [ hr ] 084 [ 95% ci 071100 ] , p = 004 ; adjusted for age , body - mass index , previous hormone - replacement therapy , nodal status , tumour size , and tumour grade )  . 
a greater decrease in breast - cancer recurrence was seen for the 1245 of 3964 ( 314% ) eligible women who reported new joint symptoms at the 3 - month follow - up visit compared with those not reporting these symptoms ( 158 during 9242 women - years of follow - up vs 366 during 11 573 women - years of followup ; adjusted hr 060 [ 050072 ] , p < 00001 )  . interpretation the appearance of new vasomotor symptoms or joint symptoms within the rst 3 months of treatment is a useful biomarker , suggesting a greater response to endocrine treatment compared with women without these symptoms . 
awareness of the relation between early treatment - emergent symptoms and bene cial response to therapy might be useful when reassuring patients who present with them , and might help to improve long - term treatment adherence when symptoms cannot be alleviated e ectively . funding cancer research uk and astrazeneca . introduction side - e ects often limit the dose of drugs that can be delivered , especially for cytotoxic chemotherapy where bone marrow , neurological , or gastrointestinal toxic e ects sometimes limit the achievable dose . 
for example , the occurrence of graft - versus - host disease in patients receiving allogeneic bone - marrow transplantation for haematological malignancies predicts overall survival.14 the occurrence of an acnei - form skin rash during the use of epidermal growth factor receptor ( egfr ) antibodies ( eg , cetuximab , panitumumab , or matuzumab ) , and also the kinase inhibitors , ge tinib and erlotinib , is another example where a side - e ect is associated with a higher probability of treatment response.5 , 6 side - e ects triggered by the therapeutic mechanism of action can be dose - independent . 
for example , in hormone therapy for breast cancer , neither inhibitors have a steep tamoxifen nor aromatase doseresponse curve for either side - e ects or e cacy.7 , 8 the appearance of vasomotor symptoms or joint symptoms is more likely to be related to the individual response to these drugs than to the dose . vasomotor symptoms ( eg , hot ushes , night sweats , and cold sweats ) are common side - e ects of endocrine treatment in women with early breast cancer.9 additionally , treatment with aromatase inhibitors increases the incidence of arthralgia and other joint symptoms.1012 for tamoxifen , there have been a few reports that women who developed vasomotor symptoms1316 had a lower risk of breast cancer recurrence than those who did not have these side - e ects , but no data on vasomotor symptoms exist for aromatase inhibitors . 
additionally , the incidence of joint symptoms is increased by all three vol 9 december 2008 1143 articles inhibitors third - generation aromatase ( anastrozole , letrozole , and exemestane ) , and is probably , at least partly , the result of the profound decrease in oestrogen concentrations.10 , 1719 however , to our knowledge , no associ ation between the development of joint symptoms and breast cancer recurrence has been reported . here , we investigate whether the early occurrence of endocrine symptoms ( speci cally vasomotor symptoms or joint symptoms ) is associated with treatment e cacy . 
 thus , the occurrence of certain symptoms could be the ultimate bioassay , which might be a re ection of the degree of biologically relevant oestrogen suppression produced in individual women by a speci c treatment . methods the arimidex , tamoxifen , alone or in combination ( atac ) study was a double - blind randomised clinical trial in which postmenopausal women with histologically con rmed localised breast cancer were randomly assigned to receive daily anastrozole ( 1 mg ) alone , tamoxifen ( 20 mg ) alone , or the combination in a double blind , method for 5 years as adjuvant treatment . 
details of trial design , methods , and primary objectives have been published elsewhere.9 after the initial analysis at 33 months of follow - up , 9 the combination group was stopped because no bene t compared with tamoxifen alone was seen , in terms of either e cacy or tolerability , and follow - up data were not subsequently collected . 
 therefore , our current analysis does not include these women and ndings will be presented only for the monotherapy groups , with focus on women who started their initial therapy , who had a hormone - receptorpositive tumour ( oestrogen - receptor positive or progesterone - receptor positive or both positive ) , and who did not report vasomotor symptoms or joint symptoms at entry . 
vasomotor symptoms were de ned as hot ushes , night sweats , or cold sweats and joint symptoms included reports of arthralgia , arthritis , arthrosis , or joint disorder . 
most symptoms occur soon after women start endocrine treatment , 20 , 21 so we used the recording of these symptoms ( all severities ) at the initial 3 - month follow - up visit as our measure of symptom occurrence . 
symptoms reported after 3 - months of initiation of the study therapy are not included in this analysis . regulatory and ethics authorities for all participating centres in 21 countries approved the protocol before enrolment of participants . 
 statistical analysis the rate of breast cancer recurrence was calculated by dividing the number of observed events by the number of woman - years of follow - up for each group . 
follow - up accrued until a breast cancer recurrence , death , or the cut - o date for this analysis ( march 31 , 2007 ) , which was the same as for the most recent 100 - month followup analysis.11 odds ratios ( or ) were used to compare factors a ecting the occurrence of vasomotor symptoms or joint symptoms at the 3 - month visit . 
for the post3 - month period , hazard ratios ( hr ) and corresponding 95% cis were estimated by the proportional hazards regression model , both with and without adjustment for age , body - mass index ( bmi ) , previous use of hormone replacement therapy ( hrt ) , nodal status , tumour size , and tumour grade.22 time - to - recurrence curves were formed by use of the kaplan - meier method.23 all p values are two - sided . 
 results overall , 590 of 6186 women ( 95% ) who started treat ment had vasomotor symptoms and 577 women ( 93% ) had joint symptoms at baseline ( table 1 )  . 
the size of these groups was small so subsequent recurrences were few ( four women with vasomotor symptoms and three women with joint symptoms ) , but were not signi cantly di erent from those in patients who did not report baseline symptoms ( vasomotor symptoms : hr 092 [ 95% ci 02959 ] , p = 07 ; joint symptoms : 068 [ 016286 ] , p = 06 )  . 
women with baseline symptoms tended to report fewer new endocrine symptoms during the trial than those without baseline symptoms ( data not shown )  . 1144 vol 9 december 2008 articles anastrozole tamoxifen all randomised women , n 3125 3116 exclusions , n ( % ) did not start randomised treatment 33 ( 11 ) 22 ( 07 ) joint symptoms only hormone - receptor negative or unknown status 502 ( 161 ) 512 ( 164 ) vasomotor symptoms only joint symptoms only at baseline 303 ( 97 ) 274 ( 88 ) vasomotor symptoms only at baseline 300 ( 96 ) 290 ( 93 ) both side - e ects at baseline 20 ( 06 ) 21 ( 07 ) study population * 1967 1997 * started allocated treatment , hormone - receptor positive , and no endocrine symptoms reported at trial entry . table 1 : exclusions from the randomised population by treatment group to obtain the study population women with hormone - receptor - negative tumours or with unknown hormone - receptor status and those with pre - existing vasomotor symptoms or joint symptoms at entry were excluded from the main analysis , leaving 1967 women in the anastrozole group ( 13 824 womanyears ) and 1997 in the tamoxifen group ( 13 637 womanyears ; table 1 )  . 
676 of 1967 women ( 344% ) in the anastrozole group reported vasomotor symptoms ( with or without joint symptoms ) compared with 810 of 1997 ( 401% ) in the tamoxifen group ( or 077 [ 95% ci 067087 ] , p = 00001 )  . 
in the anastrozole group , 665 of 1967 women ( 338% ) reported joint symptoms ( with or without vasomotor symptoms ) compared with 580 of 1997 ( 290% ) in the tamoxifen group ( or 125 [ 109143 ] , p = 0001 )  . 
more patients in the tamoxifen group reported vasomotor symptoms , whereas more patients in the anastrozole group reported joint symptoms , leading to a similar overall percentage of women reporting at least one of these symptoms ( 55% in both groups ; 1092 of 1967 in the tamoxifen group vs 1096 of 1997 in the anastrozole group )  . 
 after adjustment for age , bmi , previous hrt use , nodal status , tumour size , and tumour grade , women in the study population who reported vasomotor symptoms ( with or without joint symptoms ) at the 3 - month followup visit had fewer breast cancer recurrences than those who did not report these symptoms ( hr 084 [ 95% ci 071100 ] , p = 004 ; table 3 )  . 
those reporting only vasomotor symptoms , but not joint symptoms , had a similar decrease in recurrence rates to those reporting vasomotor stymptoms with or without joint symptoms ( not signi cant ; table 3 )  . 
 anastrozole no symptoms both symptoms tamoxifen no symptoms joint symptoms only vasomotor symptoms only both symptoms data are n ( % )  . patients 875 ( 445 ) 416 ( 211 ) 427 ( 217 ) 249 ( 127 ) 901 ( 451 ) 286 ( 143 ) 516 ( 258 ) 294 ( 147 ) table 2 : women with hormone - receptor - positive tumours and who did not report either symptom at trial entry with vasomotor symptoms or joint symptoms at the 3 - month follow - up visit according to treatment group the decrease in breast cancer recurrences for those reporting vasomotor or joint symptoms was equally clear for patients with local or distant recurrences . 
 there was no evidence of heterogeneity for vasomotor symptoms ( local recurrence : hr 080 [ 95% ci 057112 ] ; distant recurrence : 083 [ 068102 ] ; pheterogeneity = 05 ) or joint symptoms ( local recurrence : hr 064 recurrence : 060 [ 048074 ] ; pheterogeneity = 03 )  . 
for the e ect size for vasomotor symptoms ( with or without joint symptoms ) was larger in an unadjusted analysis ( hr 075 [ 95% ci 063091 ] , p = 0003 ) , and of the adjustment factors , only previous hrt use was a signi cant confounding those without previous hrt use , the e ect of vasomotor symptoms on subsequent recurrence was small ( hr 093 [ 077113 ] , p = 05 ) and similar in both treatment groups ( anastrozole group : hr 091 [ 068122 ] ; tamoxifen group : 093 [ 072120 ] )  . 
for those with previous hrt use , the e ect was substantially larger ( hr 063 [ 046085 ] , p = 0003 ) and apparent in both treatment groups ( anastrozole group : hr 053 [ 031088 ] ; tamoxifen [ 045096 ] )  . 
 signi cantly fewer women in the study population reporting joint symptoms ( with or without vasomotor symptoms ) at the 3 - month follow - up visit had a recurrence of breast cancer than those not reporting these symptoms ( hr 060 [ 95% ci 050072 ] , p < 00001 ; table 3 )  . 
figure 1 presents the recurrence proportion as a function of follow - up time according to treatment group and joint symptoms at the 3 - month follow - up visit . 
for women reporting both side - e ects at the 3 - month followup visit , a signi cantly greater decrease in breast cancer recurrence was noted compared with those not reporting any of these symptoms ( table 3 and gure 2 )  . 
 compared with women who reported neither symptom at the 3 - month follow - up visit , women who reported both side - e ects had an absolute decrease in recurrence of 114% ( 95% ci 99125 ) after 9 years of follow - up , those with joint symptoms only had a 10% ( 87108 ) absolute decrease , those who reported either side - e ect had a 8% ( 8280 ) absolute decrease , and those with vasomotor symptoms had only a 6% ( 6272 ) absolute risk decrease . discussion we present a retrospective analysis of the atac trial , assessing whether the occurrence of treatment - related symptoms ( vasomotor symptoms or joint symptoms ) is associated with breast cancer recurrence . 
a signi cantly larger e ect was noted for joint symptoms , which was similar in all subgroups , whereas the e ect of vasomotor symptoms was smaller and of borderline signi cance overall . 
the di erence in recurrence in patients with vasomotor symptoms ( with or without joint symptoms ) was substantially decreased after adjustment for age , bmi , previous hrt , nodal status , tumour size , and tumour grade and was most apparent in women who had taken hrt before trial entry . 
 analyses were restricted to patients with hormonereceptor - positive breast cancer , but similar ndings were obtained if analyses were based on all eligible randomised patients ( data not shown )  . 
 the analysis showed no signi cant di erence in recurrence in women who reported these symptoms at entry into the trial compared with those who did not report symptoms at entry . 
this nding adds weight to the interpretation of these data as re ecting a causal treatmentpatient interaction and not just a patients predisposition to these endocrine symptoms in the 1146 vol 9 december 2008 articles neither side - eect vasomotor symptoms only either side - eect joint symptoms only both side - eects 025 number at risk neither side - eect vasomotor symptoms only either side - eect joint symptoms only both side - eects 2017 912 1947 696 539 1583 880 1555 676 533 follow - up time ( years ) 1416 821 1449 629 509 1172 702 1262 561 444 796 471 855 385 324 215 165 figure 2 : breast cancer recurrence for anastrozole and tamoxifen treatments combined at di erent follow - up times according to endocrine symptoms reported at the 3 - month follow - up visit in women with hormonereceptor - positive tumours and without endocrine symptoms at entry di erences in drug metabolism or end - organ response , but this notion has yet to be fully elucidated . 
they showed that women with a wild - type genotype had a lower risk of disease relapse and a higher incidence of vasomotor symptoms than those without a wild - type genotype in the italian tamoxifen cyp2d6 . 
researchers from prevention trial assessed the frequency of the variants cyp2d6 ( * 4 / * 4 ) and noted that women who developed breast cancer on tamoxifen had a higher frequency in cyp2d6 * 4 / * 4 than those without breast cancer.24 additionally , pharmacological managing vasomotor symptomseg , the selective serotonin reuptake inhibitorsinhibit cyp2d6 and therefore decrease the e cacy of tamoxifen . 
in our study , a relation between vasomotor symptoms and breast cancer recurrence was seen , not only for tamoxifen , but also for the aromatase inhibitor anastrozole , suggesting that factors other than the cyp2d6 polymorphism are also involved . 
one possibility is the cyp19 gene ( aromatase ) itself , 25 but the full picture is likely to be more complicated and might involve other genetic loci . interventions used this analysis supports an inverse association between the occurrence of vasomotor symptoms and breast cancer recurrence previously reported for tamoxifen , 16 and extends this association to the aromatase inhibitor anastrozole and also to the presence of joint symptoms . 
 both of these symptoms are believed to be related to lowered oestrogen concentrations , although the speci c underlying cause of aromatase - inhibitor - induced joint symptoms is , as yet , unknown . 
additionally , patients who reported symptoms at baseline had fewer subsequent reports of these symptoms , but this might re ect a reporting bias in favour of new versus continuing symptoms . the e ect size was similar in both treatment groups , and an overall lower recurrence rate in patients assigned anastrozole compared with those assigned tamoxifen was apparent , regardless of whether symptoms were present or not . 
however , the size of the e ect of symptoms on recurrence was similar to , or larger than , the di erence the between anastrozole and importance of this nding . 
a detailed symptom questionnaire was not used , so it is possible that a larger e ect might have been observed if details were fully recorded . tamoxifen , supporting because the study only included women who began their allocated treatment , and endocrine symptoms were measured at the rst follow - up visit , reported adherence to treatment in the rst 3 - month period was high ( 3952 of 3964 [ 997% ] ) and is unlikely to a ect the reports of these symptoms . 
women reporting either symptom took 88% ( 1925 of 2188 ) of their prescribed treatment ( up to recurrence ) compared with 84% ( 1492 of 1776 ) in those with neither symptoit seems unlikely that these small di erences could explain the di erences in recurrences , but the reported di erences in adherence might re ect larger real di erences , which could confound our ndings . additionally , the appearance of symptoms would lead to the use of medicines that could also decrease recurrence as an additional e ect . 
details of aspirin and other non - steroidal anti - in ammatory drugs were not collected accurately , but use of cyclo - oxygenase - 2 inhibitors was collected accurately and only 12% ( 476 of 3964 ) of our study population used these drugs at any stage during the treatment . 
usage was higher in patients who reported vasomotor or joint symptoms than those who did not report these symptoms ( data not shown ) , but the hr for recurrence was unchanged if use of cox - 2 inhibitors was added to the model . 
for those with joint symptoms , the hazard ratio was only slightly changed ( hr 059 [ 95% ci 049072 ] ) if the use of either of these drugs was added to the model . the correlation of side - e ects with response to treatment has been noted in a few other situations , notably graft - versus - host disease for allogeneic bonemarrow transplantation and skin rash for antibodies directed at the egfr or tyrosine - kinase inhibitors . 
 however , this is the rst example to our knowledge where side - e ects of relatively non - toxic drugs with at doseresponse curves ( for both e cacy and side - e ects ) have been useful in predicting treatment response . 
this e ect is likely to be mediated by individual genetic vol 9 december 2008 1147 articles further work in understanding the genetic basis for individual response to treatment , these ndings also have important implications for communication between health - care professionals and patients with symptoms caused by endocrine therapy . 
several reports2628 have documented poor adherence to long - term endocrine therapy and an appreciation that endocrine symptoms indicate a stronger treatment e ect should help to encourage better symptomatic management and improve adherence for women receiving endocrine treatment . 
 these ndings also raise questions about the e ect that drugs aimed at ameliorating endocrine symptoms might have on the e cacy of endocrine treatments , if they target the same mechanism of action . contributors jc was responsible for the conception and design of the study , and assembly and analysis of the data . 
all contributors took part in writing the paper and approved the nal version . con icts of interest jc has received research funds from astrazeneca and acted as a consultant to astrazeneca and novartis . 
we also thank the trial investigators , other supporting sta , and the members of the international steering committee . articles the uk standardisation of breast radiotherapy ( start ) trials of radiotherapy hypofractionation for treatment of early breast cancer : 10 - year follow - up results of two randomised controlled trials joanne s haviland , j roger owen , john a dewar , rajiv k agrawal , jane barrett , peter j barrett - lee , h jane dobbs , penelope hopwood , pat a lawton , brian j magee , judith mills , sandra simmons , mark a sydenham , karen venables , judith m bliss * , john r yarnold * , on behalf of the start trialists group summary background 5 - year results of the uk standardisation of breast radiotherapy ( start ) trials suggested that lower total doses of radiotherapy delivered in fewer , larger doses ( fractions ) are at least as safe and e ective as the historical standard regimen ( 50 gy in 25 fractions ) for women after primary surgery for early breast cancer . 
in this prespeci ed analysis , we report the 10 - year follow - up of the start trials testing 13 fraction and 15 fraction regimens . methods from 1999 to 2002 , women with completely excised invasive breast cancer ( pt13a , pn01 , m0 ) were enrolled from 35 uk radiotherapy centres . 
in start - a , a regimen of 50 gy in 25 fractions over 5 weeks was compared with 416 gy or 39 gy in 13 fractions over 5 weeks . 
in start - a , moderate or marked breast induration , telangiectasia , and breast oedema were signi cantly less common normal tissue e ects in the 39 gy group than in the 50 gy group . 
the proportion of patients with local - regional relapse at 10 years did not di er signi cantly between the 40 gy group ( 43% , 95% ci 3259 ) and the 50 gy group ( 55% , 95% ci 4272 ; hr 077 , 95% ci 051116 ; p = 021 )  . 
in start - b , breast shrinkage , telangiectasia , and breast oedema were signi cantly less common normal tissue e ects in the 40 gy group than in the 50 gy group . 
the results support the continued use of 40 gy in 15 fractions , which has already been adopted by most uk centres as the standard of care for women requiring adjuvant radiotherapy for invasive early breast cancer . funding cancer research uk , uk medical research council , uk department of health . introduction the local cancer control and overall survival bene ts of adjuvant radiotherapy for women with early breast cancer have been established by a systematic review of 17 randomised trials involving more than 10 000 patients.1 in most studies , a total dose of 50 gy was delivered in 25 fractions of 2 gy over 5 weeks . 
5 - year results for local tumour control and late - occurring normal tissue e ects assessed by patients and from photographs were consistent with the hypothesis that breast cancer tissue and the doselimiting normal tissues are similarly sensitive to fraction size.8 , 9 start - b had a pragmatic design , with 5 - year results suggesting that local tumour control and safety of normal tissue e ects are as good after 40 gy in 15 fractions over 3 weeks ( used in the uk and canada for decades ) as with 50 gy in 25 fractions over 5 weeks.9 , 10 the 5 - year results of the start trials had a large e ect on breast cancer radiotherapy practice both in the uk and worldwide . 
start results have subsequently informed national institute for health and care excellence ( nice ) and american society for radiation oncology ( astro ) guidelines for breast radiotherapy fractionation.11 , 12 a 2010 cochrane review concluded that hypofractionation did not seem to compromise safety and e cacy , but that longer follow - up was needed for a more complete assessment.13 we here present a 10 - year update of start - a and start - b , including assessment of long - term e cacy and adverse e ects . interval was required before methods study design and participants the start trials were two randomised , unmasked trials of women recruited between 1999 and 2002 , from uk radiotherapy centres17 centres for start - a and 23 for start - b . 
patients in start - a were randomly assigned to either 50 gy in 25 fractions ( control group ) or 416 gy in 13 fractions or 39 gy in 13 fractions over 5 weeks , and start - b patients to either 50 gy in 25 fractions ( control group ) over 5 weeks or 40 gy in 15 fractions over 3 weeks . 
 randomisation method was computer - generated , and strati ed by centre , type of primary surgery ( breastconservation surgery or mastectomy ) , and tumour bed boost trials permitted prescription of a sequential tumour bed boost dose of 10 gy in ve fractions , which needed to be planned before randomisation to ensure that the independent e ect of tumour bed boost radiotherapy on adverse e ects did not a ect the comparisons of fractionation schedules . 
both start and details of the radiotherapy planning , delivery , and veri cation protocols have been previously reported.810 the start trials were approved by the south thames multi - research ethics committee in september , 1998 , and by the local ethics committees of all participating centres . 
 written informed consent was obtained for all patients . the principal endpoints were local - regional relapse de ned as relapse in breast or chest wall , ipsilateral axilla , or supraclavicular fossa within an irradiated target volumeand late normal tissue e ects . 
physician assessments of normal tissue e ects in the treated breast compared with the contralateral breast were scored on a four - point scale ( none , a little , quite a bit , or very much )  . 
 table 1 : relapse and mortality according to fractionation schedule in start - a vol 14 october 2013 1087 statistical analysis we predicted a 5 - year local - regional tumour relapse rate of 10% in the 50 gy schedule group ( control ) , on the basis of the start pilot trial.7 start - a had a target sample size of 2000 patients to provide 80% power to detect a di erence of 5% in the local - regional relapse rate between the control and each test schedule ( two - sided = 005 )  . 
start - b had a target of 1840 patients to provide 95% power to exclude an increase of 5% in the localregional relapse rate in the 40 gy schedule compared with control ( one - sided = 0025 )  . we used survival analysis methods to compare endpoint occurrences between fractionation schedules . 
 both one - sided and two - sided 95% cis were calculated for the absolute di erence in local - regional relapse rates because the upper limit is of greater clinical interest , in view of concern about a possible excess risk caused by hypofractionated schedules . 
we plotted kaplan - meier survival curves and cumulative hazard rates according to fractionation schedule , censoring at the median length of follow - up . we obtained direct estimates of the / value for breast cancer and the dose - limiting normal tissues from cox proportional hazards regression models containing terms for total dose , and total dose multiplied by dose per fraction as well as known prognostic factors ( appendix )  . 
 the / value is derived from an empirical model that describes sensitivity of a normal or malignant tissue to fraction size ; / values less than 10 gy indicate relative sensitivity to fraction size . 
we carried out meta - analyses of start - a , start - b , and the start pilot trial by tting the cox proportional hazards regression models to all individual patient data from the three trials . 
analyses were done with spss ( version 19 ) and stata ( version 9 )  . the trial is registered as an international standard randomised controlled trial , number isrctn59368779 . role of the funding source the funders of the study provided peer - reviewed approval for the trials and had no role other than as representatives ( as observers ) on the trial steering committee . 
the corresponding author had full access to all the data , and had nal responsibility for the decision to submit for publication . results 2236 women were recruited into start - a between jan 20 , 1999 , and dec 20 , 2002 ; median age was 57 years ( range 2585 ) ( appendix )  . 
1900 ( 85% ) had received breast - conserving surgery , 1138 ( 51% ) had tumours smaller than 2 cm , 643 ( 29% ) had positive lymph nodes , 1572 ( 70% ) had grade 1 or 2 disease , 793 ( 35% ) received adjuvant chemotherapy , 1758 ( 79% ) received tamoxifen , and 318 ( 14% ) received lymphatic radiotherapy . 
at a median follow - up in survivors of 93 years ( iqr 80100 , maximum 124 years ) , 1700 of 2236 patients ( 760% ) were alive and without relapse , 57 ( 25% ) were 40 gy vs 50 gy hr 077 , 95% ci 051116 ; p = 021 time from randomisation ( years ) 1077 1085 1047 1055 1002 1016 number at risk 50 gy 40 gy 1105 1110 figure 1 : cumulative risk of local - regional tumour relapse in start - a ( a ) and start - b ( b )  . 1088 vol 14 october 2013 articles 50 gy 416 gy 39 gy 50 gy 40 gy alive with local - regional relapse ( without distant relapse ) , 78 ( 35% ) were alive with distant relapse ( including 16 with local - regional relapse ) , 392 ( 175% ) had died ( including 66 with local - regional relapse ) , and nine ( 04% ) had had no follow - up . at the time of analysis ( feb 20 , 2012 ) , 139 of 2236 ( 62% ) patients in start - a had local - regional tumour relapse . 
the hrs for local - regional relapse relative to the 50 gy schedule were 091 ( 95% ci 059138 ) for the 416 gy schedule and 118 ( 079176 ) for the 39 gy schedule ( table 1 )  . 
the estimated absolute di erences in the proportion of patients with local - regional relapses at 10 years compared with 50 gy were 06% ( 95% ci 30 to 27 ) for 416 gy and 13% ( 15 to 52 ) for 39 gy . 
the upper limits of the one - sided 95% ci for the absolute di erence in 10 - year local - regional relapse rates indicated an estimated maximum 20% excess risk with 416 gy and 45% with 39 gy compared with 50 gy . 
the estimated / value for local - regional relapse in start - a was 4 gy ( 95% ci 0089 ) , adjusting for age , tumour size , type of primary surgery , use of adjuvant chemotherapy , use of tamoxifen , lymphatic radiotherapy , and tumour bed boost radiotherapy . 
15 ( 577% ) of the 26 deaths from cardiac disease in start - a were in women with left - sided primary tumours ( four of seven with 50 gy , ten of 13 with 416 gy , and one of six with 39 gy )  . 
distant relapses , disease - free survival , and overall survival were not signi cantly di erent between schedules start - a , with no evidence of a clinically signi cant detriment for either of the hypofractionated schedules compared with 50 gy ( table 1 , gure 2 )  . breast shrinkage and induration were the most common normal tissue e ects at 10 years in start - a ( table 2 )  . 
moderate or marked breast induration , telangiectasia , and breast oedema were signi cantly less common in the 39 gy regimen patients group than in the 50 gy regimen group ( table 2 , gure 3 )  . 
 / estimates for normal tissue endpoints in start - a ( adjusting for age , breast size , surgical de cit , lymphatic radiotherapy , and tumour bed boost radiotherapy ) were 35 gy ( 95% ci 0764 ) for breast shrinkage , 416 gy vs 50 gy hr 094 , 95% ci 075117 ; p = 057 39 gy vs 50 gy hr 108 , 95% ci 087135 ; p = 048 number at risk 50 gy 416 gy 39 gy 40 gy vs 50 gy hr 079 , 95% ci 065097 ; p = 0022 number at risk 50 gy 40 gy 1105 1110 time from randomisation ( years ) 1064 1080 1021 1040 figure 2 : kaplan - meier analysis of disease - free survival in start - a ( a ) and start - b ( b )  . 4 gy ( 2356 ) for breast induration , 38 gy ( 1857 ) for telangiectasia , and 47 gy ( 2470 ) for breast oedema . 
 ischaemic heart disease , symptomatic rib fracture , and symptomatic lung brosis were rare at 10 years ( table 3 ) and occurred in much the same proportions with each treatment schedule . 2215 women were recruited into start - b between jan 4 , 1999 , and oct 12 , 2001 . 
2038 of 2215 ( 92% ) patients had received breastconserving surgery , 1412 ( 64% ) had tumours smaller than 2 cm , 504 ( 23% ) had positive lymph nodes , 1667 ( 75% ) had grade 1 or 2 disease , 491 ( 22% ) received adjuvant chemotherapy , 1928 ( 87% ) received tamoxifen , and 161 ( 7% ) received lymphatic radiotherapy ( appendix )  . 
restricted to women who received lymphatic radiotherapy ( to axilla or supraclavicular fossa )  . table 2 : physician - assessed normal tissue e ects by fractionation schedule in start - a alive with local - regional relapse ( without distant relapse ) , 63 ( 28% ) were alive with distant relapse ( including ten with local - regional relapse ) , 351 ( 158% ) had died ( including 35 with local - regional relapse ) , and 19 ( 09% ) had no follow - up . at the time of the analysis , 95 of 2215 ( 43% ) patients in start - b had had local - regional tumour relapse , a lower proportion than in start - a , which is probably a result of the slightly better prognosis of patients recruited into start - b compared with start - a . 
the estimated absolute di erence in the proportion of patients with 10 - year local - regional relapse for 40 gy compared with 50 gy was 12% ( 95% ci 26% to 10% )  . 
the upper limit of the one - sided 95% ci for the absolute di erence in 10 - year local - regional relapse rates suggested an estimated 04% excess risk associated with the 15 fraction schedule . 
the kaplanmeier and cumulative hazard rate plots for local - regional relapse according to fractionation schedule ( gure 1 , appendix ) show the low number of recurrences in both randomised groups in start - b . 236 of 351 ( 672% ) deaths in start - b were from breast cancer ( 130 with 50 gy and 106 with 40 gy ) , 17 ( 48% ) were related to cardiac disease only ( 12 with 50 gy and ve with 40 gy ) , 48 ( 137% ) were from other cancers ( 25 with 50 gy and 23 with 40 gy ) , 40 ( 114% ) were from other noncancer causes ( 21 with 50 gy and 19 with 40 gy ) , and ten ( 28% ) were from unknown cause ( four with 50 gy and six with 40 gy )  . 
11 ( 647% ) of the 17 deaths from cardiac disease were in women with left - sided primary tumours ( eight of 12 with 50 gy and three of ve with 40 gy )  . 
 * reported cases include seven after trauma ( ve in start - a , two in start - b ) , and ten after metastases ( ve in starta and ve in start - b )  . 
 hazard ratio ( 95% ci ) table 3 : incidence of other late adverse e ects according to fractionation schedule 20 30 40 favours 40 gy favours 50 gy local - regional relapse figure 3 : late normal tissue e ects in start - a ( a ) and start - b ( b )  . 
moderate or marked breast shrinkage , telangiectasia , and breast oedema were signi cantly lower with 40 gy than with 50 gy ( gure 3 , table 5 )  . 
 ischaemic heart disease , symptomatic rib fracture , and symptomatic lung brosis were rare and occurred in much the same proportions with each treatment schedule ( table 3 )  . post - hoc subgroup analyses of the combined hypofractionated regimens versus the control groups for localregional relapse in start - a , start - b , and the pilot trial ( n = 5861 ) showed that the treatment e ect was not signi cantly di erent irrespective of age , type of primary surgery , axillary node status , tumour grade , adjuvant chemotherapy use , or use of tumour bed boost radiotherapy ( gure 4 )  . 
in a post - hoc analysis , the incidence of any moderate or marked physician - assessed normal tissue e ects in the breast ( shrinkage , induration , oedema , or telangiectasia ) for the 4660 women with data available from start - a , start - b , and the pilot trial showed that the treatment e ect was similar irrespective of age , breast size , use of tumour bed boost radiotherapy , adjuvant chemotherapy , or tamoxifen ( gure 5 )  . local relapse 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy events ( n / patients ; % ) estimated proportion of patients with event by 5 years ( % ; 95% ci ) estimated proportion of patients with event by 10 years ( % ; 95% ci ) crude hazard ratio ( 95% ci ) value * 50 / 1105 ( 45% ) 33% ( 2446 ) 52% ( 3969 ) 100 36 / 1110 ( 32% ) 19% ( 1230 ) 38% ( 2752 ) 070 ( 046107 ) 010 53 / 1105 ( 48% ) 35% ( 2548 ) 55% ( 4272 ) 100 42 / 1110 ( 38% ) 23% ( 1534 ) 43% ( 3259 ) 077 ( 051116 ) 021 158 / 1105 ( 143% ) 105% ( 88125 ) 160% ( 138185 ) 100 121 / 1110 ( 109% ) 75% ( 6092 ) 123% ( 103146 ) 074 ( 059094 ) 0014 any breast cancer - related event all - cause mortality 222 / 1105 ( 201% ) 143% ( 123165 ) 222% ( 197250 ) 100 182 / 1110 ( 164% ) 104% ( 87124 ) 183% ( 160209 ) 079 ( 065097 ) 0022 192 / 1105 ( 174% ) 109% ( 91129 ) 192% ( 168219 ) 100 159 / 1110 ( 143% ) 79% ( 6496 ) 159% ( 137184 ) 080 ( 065099 ) 0042 * assessed with log - rank test compared with 50 gy . 
 table 4 : relapse and mortality according to fractionation schedule in start - b time , the relative di erences between discussion although the absolute numbers of events have increased over the hypofractionated and control schedules at 10 years remain similar to those at 5 years , con rming that appropriately dosed hypofractionated radiotherapy for women with early breast cancer is safe and e ective.810 in start - a , 416 gy in 13 fractions over 5 weeks remains a safe and e ective alternative to 50 gy in 25 fractions the two regimens have much the same anti - tumour and adverse e ects . 
 restricted to women who received lymphatic radiotherapy ( to axilla or supraclavicular fossa )  . table 5 : physician - assessed normal tissue e ects by fractionation schedule in start - b number of events / patients age ( years ) 4049 5059 primary surgery axillary nodes ( pn ) negative positive tumour grade breast conservation surgery 409 / 5348 mastectomy 35 / 513 60 / 343 116 / 1046 154 / 2226 114 / 2246 289 / 4318 149 / 1421 41 / 1213 108 / 2398 114 / 1272 199 / 2749 241 / 3071 303 / 4346 139 / 1480 tumour bed boost radiotherapy adjuvant chemotherapy 1092 12 14 16 18 20 favours fraction sizes > 20 gy favours fraction size 20 gy figure 4 : meta - analysis of local - regional relapse comparing hypofractionated regimens versus 50 gy in 25 fractions includes 5861 patients from the start pilot trial , start - a , and start - b . average treatment groups enabled an unconfounded test of sensitivity to fraction size . 
the cis around the / estimate for breast cancer become narrower as more data are collected , and the low value is supported by the evidence from the combined hypofractionation trials.14 an underlying estimate describes the distribution of / that can be narrow or broad : its characterisation is a challenge for correlative research . 
 the 10 - year results of start - b con rm that 40 gy in 15 fractions over 3 weeks is at least as safe and e ective as 50 gy in 25 fractions over 5 weeks . 
application of an / value of 35 gy for breast shrinkageas obtained from start - aand assuming no e ect of treatment time on late normal tissue e ects , 40 gy in 15 fractions corresponds to 45 gy in 2 gy equivalents . 
the 15 fraction regimen is less harmful to normal tissues , and there is no suggestion that it is less e ective in treating the cancer . the data from the start trials are consistent with the 10 - year results of the ontario trial , which reported that local tumour control and breast cosmesis were no worse with a regimen of 425 gy in 16 fractions over 32 weeks compared with 50 gy in 25 fractions over 5 weeks.5 the start pilot trial , ontario trial , and start - a and start - b trials , considered together , present robust evidence that hypofractionation is a safe and e ective approach to breast cancer radiotherapy ( panel ) .15 the corollary is that the continued use of small ( 2 gy ) fractions spares the cancer as much as the normal tissues , thereby bringing no bene t to patients . 
the proportion of patients who had distant metastases di ered after the rst few years of follow - up , which translated into an overall survival bene t ( table 4 )  . 
this e ect did not occur in start - a and it occurs too early to be a result of better local control , in which case the survival bene t would not be apparent until after 15 years . 
similarly , it is unlikely to be caused by baseline di erences in patient and treatment characteristics , which were well balanced between schedules , and unknown factors are unlikely to be imbalanced in randomised trials of this size . 
following publication of the start trials 5 - year results , most uk centres pragmatically adopted the 15 fraction schedule as standard of care , as recommended by nice guidelines in 2009.11 the 15 fraction schedule was already in widespread use in the uk and elsewhere before the start trials , but had not been formally tested in a randomised controlled setting . controversy remains about generalising trial ndings to all patients satisfying the eligibility criteria of the start trials.12 to address this concern , we did unplanned subgroup meta - analyses of the start - a and start - b trial comparing all trials and the start pilot vol 14 october 2013 hazard ratio ( 95% ci ) 079 ( 047134 ) 088 ( 060128 ) 103 ( 074144 ) 111 ( 075163 ) 097 ( 080119 ) 091 ( 046181 ) 110 ( 086140 ) 080 ( 057111 ) 096 ( 051182 ) 107 ( 072159 ) 086 ( 059125 ) 099 ( 074132 ) 099 ( 076129 ) 109 ( 086138 ) 081 ( 057114 ) articles hazard ratio ( 95% ci ) 085 ( 056128 ) 109 ( 086137 ) 078 ( 068091 ) 080 ( 069092 ) 096 ( 065142 ) 077 ( 068087 ) 091 ( 072115 ) 080 ( 069092 ) 086 ( 076096 ) 083 ( 075091 ) 088 ( 071108 ) 083 ( 068102 ) 084 ( 076093 ) hypofractionated schedules combined versus the control schedules . 
although direct comparisons of results across the di erent trials are inadvisable because of the di erent patient populations , our subgroup analyses lend no support to a conservative approach with respect to patient age , breast size , tumour grade , axillary node status , type of surgery , cytotoxic chemotherapy , tumour bed boost radiotherapy , and lymphatic radiotherapy , although numbers are small in some groups . 
along with other investigators , 16 we have found no suggestion of a detrimental e ect of hypofractionated radiotherapy on risk of local relapse in grade 3 tumours , which does not support a subgroup analysis of the ontario trial.5 whether or not a tumour bed boost radiotherapy was given did not alter the e ect of hypofractionation on risk of late normal tissue e ects , and tumour bed boost radiotherapy could not have a confounding e ect because it was prescribed before randomisation and was given to similar proportions of patients in each treatment schedule group . 
one exclusion criterion from the start trials was immediate breast reconstruction , and a conservative approach might be to defer from using a 15 fraction regimen in such patients , despite the very high likelihood , in our opinion , that the 15 fraction schedule would reduce normal tissue e ects and provide equivalent local - regional control . 
finally , concerns have been raised about doses to the heart with hypofractionated schedules.12 our results showed that although follow - up was still short for cardiac events , there was no major di erence between the schedules for the number of cases of heart disease in women with left - sided primary tumours . 
some research suggests that hypofractionated breast radiotherapy might be safer for the heart than are conventional regimens.18 although such ndings are reassuring , the heart is sensitive to radiation whatever fractionation is used , with no lower dose threshold for adverse e ects.19 thus , the heart should be protected irrespective of the dose fractionation regimen used . other ongoing or planned trials of hypofractionation for whole breast radiotherapy aim to validate the ndings from the start trials in di erent popu lations . 
 * assessed from baseline photographs . panel : research in context systematic review the start trials began with the pilot study in 1986 , at which time there was no evidence available from randomised trials comparing alternative fractionation schedules for breast cancer radiotherapy . 
alternative shorter fractionation schedules were in use at some uk centres and in canada , but the only evidence available for these schedules was from case series and cohort studies . 
5 - year results of the start trials were published in 2008 , and in 2002 for the ontario trial , which suggested that the hypofractionated regimens were as safe and e ective as the historical standard control schedule of 50 gy in 25 fractions . 
10 - year follow - up results of the ontario trial were published in 2010 , and an updated cochrane systematic review was published in 2010 . interpretation following publication of 5 - year results from the ontario and start trials , long - term follow - up was needed to con rm the safety and e cacy of the hypofractionated schedules . 
the 10 - year start trial results presented here , together with the long - term results of the ontario trial , con rm the earlier ndings and strengthen the evidence in favour of using hypofractionated schedules for breast cancer radiotherapy . 
they support the continued use of 40 gy in 15 fractions as the uk standard of care as recommended by the national institute for health and care excellence , and contribute further to the worldwide debate about breast cancer radiotherapy hypofractionation . vol 14 october 2013 1093 articles informed by the results of the pilot fast trial ( n = 915 ) .20 in conclusion , long - term follow - up of the start trials con rms that appropriately dosed hypofractionated radiotherapy is safe and e ective for patients with early breast cancer . contributors jry was chief investigator and chair of the trial management group . 
 rka , jb , pjb - l , hjd , pal , and bjm contributed to trial design , trial management , data interpretation , and commented on the report . con icts of interest we declare that we have no con icts of interest . 
we thank cancer research uk , the uk medical research council , and the uk department of health for providing the funds to undertake this research ( grant g9600656 )  . 
the start trialists group consists of the trial management group ( appendix ) , consumers , trial steering committee , independent data monitoring committee , and the principal and main co - investigators at the participating centres ( published previously ) .8 , 10 published online august 6 , 2019 s1470 - 2045 ( 19 ) 30530 - 3 published online july 30 , 2019 s1470 - 2045 ( 19 ) 30521 - 2 correction to lancet oncol 2019 ; 20 : 114859 correction to lancet oncol 2019 ; 20 : 121125 bonvalot s , rutkowski pl , thariat j , et al . 
 nbtxr3 , a first - in - class radioenhancer hafnium oxide nanoparticle , plus radiotherapy versus radiotherapy alone in patients with locally advanced soft - tissue sarcoma ( act.in.sarc ) : a multicentre , phase 23 , randomised , controlled trial . 
 lancet oncol 2019 ; 20 : 114859in this article , the funder pharmaengine , inc , was inadvertently omitted and has now been added to the funding line in the summary and to the acknowledgments . 
a repeated sentence has been deleted from the fifth paragraph of the statistical analysis section of the methods , and some minor typographical errors have been corrected throughout the paper . 
 these corrections have been made to the online version as of sept 2 , 2019 . correction to lancet oncol 2019 ; 20 : 117182 nen nr , reisel d , leimbach a , et al . 
the following sentence has been added to the figure 4 caption : sdi quintiles are ordered from high to low sdi quintile , and gbd super - regions are alphabetically ordered . 
the next sentence should read : country order selected by total absolute dalys ; countries with the greatest total absolute dalys , of the fifty most populous countries in the world , are listed first . 
this correction has been made to the online version as of aug 6 , 2019 . correction to lancet oncol 2019 ; 20 : 127385 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
lancet oncol 2019 ; 20 : 127385in this article , data ( hazard ratios , 95% cis , and p values ) in the following sentence on p 1279 have been corrected : in women with stage iii disease , 5 - year overall survival was 838% ( 95% ci 784895 ) with chemoradiotherapy versus 820% ( 95% ci 765877 ) with radio therapy alone ( hr 084 [ 95% ci 052138 ] ; p = 050 ) , and 5 - year failure - free survival was 813% ( 95% ci 747863 ) with chemoradiotherapy versus 773% ( 95% ci 705827 ) with radiotherapy alone ( hr 087 [ 95% ci 056136 ] p = 054 ; appendix p 8 )  . 
on p 1282 , the same data ( hazard ratios and 95% cis ) in the following sentence have also been corrected : for women with stage iii endometrial cancer , combined adjuvant treatment yielded only a small absolute improvement of 2% ( hr 084 ; 95% ci 052138 ) in 5 - year overall survival and of 4% ( 087 ; 056136 ) in failure - free survival . 
 these corrections have been made to the online version as of sept 2 , 2019 , and the printed version is correct . correction to lancet oncol 2019 ; 20 : e41733 herrera fg , irving m , kandalaft le , coukos g . 
 this correction has been made as of july 30 , 2019 . correction to lancet oncol 2019 ; 20 : e50321 spence d , dyer r , andall - brereton g , et al . 
 lancet oncol 2019 ; 20 : e50321the affiliations of authors dingle spence and m austin argentieri have been corrected in the online version as of sept 2 , 2019 . vol 20 september 2019 e468 corrections correction to lancet oncol 2013 ; 14 : 106776 sgroi dc , sestak i , cuzick j , et al . 
 prediction of late distant recurrence in patients with oestrogen - receptor - positive breast cancer : a prospective comparison of the breast - cancer index ( bci ) assay , 21 - gene recurrence score , and ihc4 in the transatac study population . 
 lancet oncol 2013 ; 14 : 106776 in this article , the 95% ci curves in figure 3 , and the graphs on appendix p 7 and p 10 , were found to have been calculated using an incorrect statistical method , and as such the width of the ci lines ( not the risk curves ) needed to be corrected . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2017 ; 18 : 122137 lacas b , bourhis j , overgaard j , et al . 
these corrections have been made to the online version as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 295309 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone for women with highrisk endometrial cancer ( portec - 3 ) : final results of an international , open - label , multicentre , randomised , phase 3 trial . 
addition of platinum salts to neoadjuvant chemotherapy in triplenegative breast cancer : a new standard of care ? lancet oncol 2018 ; 19 : 43436 in this comment , the bracketed text in the third sentence of the first paragraph should have read , ( 168 [ 53% ] of 316 patients vs 49 [ 31% ] of 158 patients , p < 00001 ) , and the bracketed text in the fourth sentence of the second paragraph should have read , ( 26 [ 57% ] of 46 patients in the paclitaxel plus carboplatin plus veliparib group vs 12 [ 50% ] of 24 in the paclitaxel plus carboplatin group vs nine [ 41% ] of 22 in the paclitaxel alone group )  . 
these corrections have been made in the online version as of march 28 , 2018 , and the printed version is correct . correction to lancet oncol 2018 ; 19 : 47485 de placido s , gallo c , de laurentiis m , et al . 
 adjuvant anastrozole versus exemestane versus letrozole , upfront or after 2 years of tamoxifen , in endocrine - sensitive breast cancer ( fata - gim3 ) : a randomised , phase 3 trial . 
additionally , the supplementary appendix of this article has been corrected as of march 28 , 2018 . correction to lancet oncol 2018 ; 19 : 51020 maio m , lewis k , demidov l , et al . 
 adjuvant vemurafenib in resected , brafv600 mutation - positive melanoma ( brim8 ) : a randomised , double - blind , placebo - controlled , multicentre , phase 3 trial . 
we investigated whether the frameshift nature of indel mutations , which create novel open reading frames and a large quantity of mutagenic peptides highly distinct from self , might contribute to the immunogenic phenotype . methods we analysed whole - exome sequencing data from 5777 solid tumours , spanning 19 cancer types from the cancer genome atlas . 
we assessed in - silico tumour - specific neoantigen predictions by mutation type with pan - cancer analysis , together with rnaseq profiling in renal clear cell carcinoma cases ( n = 392 ) , to compare immune gene expression across patient subgroups . 
associations between indel burden and treatment response were assessed across four checkpoint inhibitor datasets . findings we observed renal cell carcinomas to have the highest proportion ( 012 ) and number of indel mutations across the pan - cancer cohort ( p < 22 10 ) , more than double the median proportion of indel mutations in all other cancer types examined . 
immune gene expression analysis in the renal clear cell carcinoma cohort showed that the presence of mutant - specific neoantigens was associated with upregulation of antigen presentation genes , which correlated ( r = 078 ) with t - cell activation as measured by cd8 - positive expression . 
finally , analysis of checkpoint inhibitor response data revealed frameshift indel count to be significantly associated with checkpoint inhibitor response across three separate melanoma cohorts ( p = 47 10 )  . interpretation renal cell carcinomas have the highest pan - cancer proportion and number of indel mutations . 
 evidence suggests indels are a highly immunogenic mutational class , which can trigger an increased abundance of neoantigens and greater mutant - binding specificity . funding cancer research uk , uk national institute for health research ( nihr ) at the royal marsden hospital national health service foundation trust , institute of cancer research and university college london hospitals biomedical research centres , the uk medical research council , the rosetrees trust , novo nordisk foundation , the prostate cancer foundation , the breast cancer research foundation , the european research council . copyright the author ( s )  . 
the data have also been scrutinised for mutations that might play a role in the recognition of cancer cells by the immune syste the focus of these analyses to a large extent is on the single nucleotide variants ( snvs ) , on account of the relative simplicity and reliability of calling sequence changes of one base pair ( bp ) fixed length . 
as a consequence , the effect of small scale insertion and deletion mutations ( indels ) on antitumour immunity has been poorly characterised despite the clear link of such mutations to oncogenesis3 and their potential to generate highly immunogenic peptides . inhibitor the notion the success of checkpoint therapies underlines tumour - specific t - cell that responses pre - exist in some patients and are kept under tight control via immune modulatory mechanisms . 
the predominant focus of existing literature was on single nucleotide variation ( snv ) mutations , with no previous study done of insertion and deletion ( indel ) mutations on a pan - cancer basis . 
regarding the association between somatic mutations and upregulation of antitumour immunity via checkpoint inhibition , several previous studies reported a link between high snv load and improved response to checkpoint inhibition . 
no previous pan - cancer study has investigated the difference between snv and indel - derived neoantigens , despite the propensity of indels to generate highly mutagenic peptides via creation of a shifted novel open reading frame . added value of this study we did a pan - cancer assessment of indel load across 5777 tumour samples spanning 19 cancer types . 
kidney tumours were observed to have the highest proportion and absolute count of indel mutations on a pan - cancer basis , a result which was replicated in two further independent datasets . 
finally , we assessed the association between indel load and checkpoint inhibitor response in three melanoma cohorts , which showed indel load to be more strongly associated with response than non - synonymous ( ns ) snv load . implications of all the available evidence our data highlight the importance of frameshift neoantigens alongside nssnv neoantigens as determinants of immunotherapy efficacy and potentially crucial targets for vaccine and cell therapy interventions . 
t cells reactive to tumour - specific mutant antigens ( neoantigens ) have been detected epithelial malignancies4 and neoantigens are increasingly shown to be the target of checkpoint inhibitor - induced t - cell responses5 , 6 and adoptively transferred t cells.79 many investigators are leveraging whole - exome sequencing and rna sequencing , focusing on non - synonymous snvs ( nssnvs ) , to predict expressed mutated peptides that bind mhc class i molecules ( snv - neoantigens )  . 
 neoantigen burden is closely related to the nssnv burden , which varies significantly across cancer types , from one nssnv in paediatric tumours to more than 1500 nssnvs in tumours associated with microsatellite instability.10 however , less than 1% of the nssnvs in expressed genes lead to detectable cd4 - positive11 or cd8 - positive t - cell7 reactivities in tumour - infiltrating lymphocytes . 
accordingly , efficacy of checkpoint inhibitors is most marked in tumour types with a high nssnv lung adenocarcinoma , lung squamous cell carcinoma , head and neck squamous cell carcinoma , and carcinoma of the bladder , 10 which reflects a higher probability of creating a neoantigen that will be presented to and recognised by t cells . 
furthermore , within these tumour types , nssnv and neoantigen burdens correlate with response to checkpoint inhibitors.1216 a notable outlier is renal clear cell carcinoma , which has a relatively low nssnv burden ( around ten times lower than melanoma )  . 
 including melanoma , burden , renal clear cell carcinoma is characterised by a high level of tumour - infiltrating immune cells17 and has been interferon - , high - dose shown interleukin 2 , 18 , 19 and , more recently , checkpoint inhibitors , 20 , 21 but the mutational and antigenic determinants of these responses are unknown . respond from self indel mutations that cause a frameshift ( frameshift indels ) create a novel open reading frame and could produce a large quantity of neoantigenic peptides highly distinct ( appendix p 5 )  . 
it has been hypothesised22 that novel open reading frames might be an ideal source of tumour - derived neoantigens and so induce multiple neoantigen reactive t cells , because of both an increased number of mutant peptides and reduced susceptibility to self - tolerance mechanisms . 
on this basis , we aimed to characterise the pattern of indel mutations with pan - cancer analysis and investigate their association with antitumour immune response and outcome following checkpoint blockade . methods study design and participants pan - cancer somatic mutational data were obtained from the cancer genome atlas ( tcga ) for whole - exome sequencing data of 5777 solid tumours , across 19 cancer types : bladder urothelial carcinoma , invasive breast carcinoma , cervical and endocervical cancers , colorectal adenocarcinoma , glioma , head and neck squamous cell carcinoma , chromophobe renal cell carcinoma , renal clear cell carcinoma , renal papillary cell carcinoma , liver hepatocellular carcinoma , lung adenocarcinoma , serous lung carcinoma , ovarian squamous cell 1010 vol 18 august 2017 articles pancreatic cystadenocarcinoma , adenocarcinoma , prostate adeno carcinoma , skin cutaneous melanoma , stomach adenocarcinoma , thyroid carcinoma , and uterine carcinosarcoma . 
we performed replication analyses in two additional cohorts of patients with renal clear cell carcinoma : a whole - exome sequencing study of 106 patients with renal clear cell carcinomas reported by sato and colleagues23 and a whole - exome sequencing study of ten patients with renal clear cell carcinomas reported by gerlinger and colleagues.24 we obtained final post - quality control patient - level mutation annotation files for each study . to further test for an association between nssnvs or indel loads and patient response to checkpoint inhibitor therapy we used four patient cohorts . 
the first dataset consisted of 38 patients with melanoma treated with anti - pd - 1 therapy , as reported by hugo and colleagues.25 we obtained final post - quality control mutation annotation files and clinical outcome data , and 34 patients were retained for analysis after exclusion of cases in which dna had been extracted from patientderived cell lines and patients in whom tissue tumor purity was below 20% . 
four samples from hugo and colleagues25 were taken after a short period on treatment , which raises the possibility that checkpoint inhibitor therapy itself might have affected mutational frequencies through possible elimination of immunogenic tumour clones . 
to be consistent with the original study , these samples were not excluded ; however , we note the frameshift indel association presented becomes more significant with these cases removed . 
the second checkpoint inhibitor cohort comprised of 62 patients with melanoma treated with anti - ctla - 4 therapy , as reported by snyder and colleagues.13 all patients samples were taken from fresh snap frozen tumour tissue with tumour purity of more than 20% so , accordingly , all 62 cases were retained for analysis . 
the snyder and colleagues cohort also contained a number of samples taken on treatment ; these samples have been retained for consistency ; however , we note again the significance of results strengthens if they are removed . 
 the third checkpoint inhibitor cohort comprised of 100 patients with melanoma treated with anti - ctla - 4 therapy , as reported by van allen and colleagues ; 12 one patient ( pat21 ) was excluded because of a tumour purity of less than 20% . 
the final checkpoint inhibitor cohort comprised of 31 patients with non - small - cell lung cancer treated with anti - pd - 1 therapy , as reported by rizvi and colleagues ; 14 all patients were eligible for inclusion . 
for these four cohorts , 1214 final mutation annotation files , including indel mutations , were not available , so we obtained raw bam files and undertook variant calling using a standardised bioinformatics pipeline . 
to assess for a general association between nssnvs or indel loads and patient overall survival we used a final cohort of 100 patients with non - small - cell lung cancer , as reported by jamal - hanjani and colleagues.26 we obtained final post - quality control mutation annotation files and clinical outcome data , and 88 patients were retained for analysis after exclusion of non - smokers . 
we used picard tools , gatk ( version 2.8.1 ) , and fastqc ( version 0.10.1 ) to produce quality samtools mpileup ( version 0.1.19 ) 29 was used to locate non - reference positions in tumour and germline samples . 
 following completion , variants called by mutect were filtered according to the filter parameter pass . in the pan - cancer cohort , snv and indel mutation counts were computed per case , considering all variant types . 
we estimated the extent of nmd for all indel and snv mutations ( with snv mutations used as a benchmark comparator ) by comparing mrna expression in samples with a mutation to the median mrna expression of the same transcript across all other tumour samples in which the mutation was absent . 
specifically , mrna expression of every mutation - bearing transcript was divided by the median mrna expression of that transcript in non - mutated samples , to give an nmd index . 
tumour purity in the renal clear cell carcinoma cohort was 054 , 32 quantified by histological assessment , and assuming constant expression in the remaining 046 normal cellular content , that would yield an adjusted 14% drop in expression in indel - mutationbearing cancer cells . 
if we assume that tumour mutations are clonal , of heterozygote genotype , in a diploid genomic region , and wild - type allele expression in mutated cancer cells remains constant , a purity - adjusted reduction of 05 would be expected under a model of fully effective nmd . 
these data are presented as a global approximation of nmd efficiency , using methods in line with previous publications.33 nmd index values were log indicating no mrna degradation and plotted for indel or snv mutations . transformed , with 0 we used pyclone34 and ascat35 to determine the clonal status of variants in the cohorts by snyder and colleagues13 and van allen and colleagues.12 for each case variant calls were integrated with local allele - specific copy number ( obtained from ascat ) , tumour purity ( also obtained from ascat ) , and variant allele frequency . 
for a number of tumours the reliable copy number , mutation , and purity estimations could not be clonal architecture analysis extracted , rendering and colleagues in snyder intractable and these tumours were omitted from the analysis . 
a strong binding threshold was used for wild - type alleles to ensure fair comparison between snv - derived and indel - derived neoantigens , in view of the high incidence of wild - type non - binders for indels . 
we excluded ( from the pancancer neoantigen analyses ) cancers that were associated with a high level of viral genome integration , including cervical ( > 80% rate of human papillomavirus integration ) and hepatocellular carcinoma ( > 50% rate of hepatitis b integration ) , but not head and neck squamous cell ( < 15% rate of human papillomavirus carcinoma integration )  . 
no tcga dataset was available for merkel cell carcinoma . immune gene signature data were obtained from rooney and colleagues , 40 with gene sets defined as stated in the appendix ( p 3 )  . 
a high burden of frameshift indel high - affinity neoantigens was defined as more than 10 per case ( n = 32 ) , and the percentage difference in expression was compared between the high indel neoantigen group and all other patients across each immune signature . 
the same analysis was repeated for a high burden of snv - derived high - affinity 1012 vol 18 august 2017 articles neoantigens , with a threshold of more than 17 snv neoantigens selected to size match the high burden groups ( equal number of patients ; n = 32 across all highload groups ) across mutational types . 
 we did correlation analysis within the high - frameshift indel neoantigen group ( n = 32 patients with renal clear cell carcinoma )  . outcomes across the four cohorts of patients treated with checkpoint inhibitors , we tested nssnv , all - coding indel , and frameshift indel variant counts for an association with patient response to therapy . 
 for snyder and colleagues cohort , 13 long - term clinical benefit was defined as radiographic evidence of freedom from disease , evidence of a stable disease , or decreased volume of disease for more than 6 months . 
no long - term clinical benefit was defined as tumour growth on every ct scan after the initiation of treatment ( no benefit ) or a clinical benefit lasting 6 months or less ( minimal benefit )  . 
for hugo and colleagues cohort , 25 responding tumours were complete response , partial response , and stable disease , and non - responding tumours were defined as disease progression . 
for van allen and colleagues cohort , 12 clinical benefit was defined as complete response , partial response , or stable disease , and no clinical benefit was progressive disease or stable disease with overall survival less than 1 year . 
for rizvi and colleagues cohort , 14 durable clinical benefit was defined as partial response or stable disease lasting longer than 6 months , and no durable benefit was progressive disease less than 6 months from beginning of therapy . 
 multivariate cox regression was done with relapse - free survival versus indel load with stage , adjuvant therapy ( yes or no ) , age , and histology included in the model . we compared indel burden and proportion measures between renal cell carcinomas and all other non - kidney cancers with a two - sided mann - whitney u test . 
in the checkpoint inhibitor response analysis , nssnv , exonic indel , and frameshift indel counts were each compared to patient response outcome using a two - sided mannwhitney u test . 
we carried out statistical analyses using r ( version 3.0.2 ) and considered a p value of 005 or less ( two - sided ) as being statistically significant . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results we observed a median indel proportion value of 005 and a median indel count of 4 , cohort - wide . 
across all tumour types , renal clear cell carcinoma was found to have the highest proportion of coding indels , 012 ( p < 22 10 ; figure 1 ) , a 24 times increase when compared with the pan - cancer average . 
this result was replicated in two further independent cohorts , with median observed indel proportions of 010 in sato and colleagues study23 and 012 in gerlinger and colleagues study24 ( figure 1 )  . 
renal papillary cell carcinoma and chromophobe renal cell carcinoma had the second and third highest indel proportion , suggesting a possible tissue - specific mutational process contributing to the acquisition of indels in renal cancers . 
renal papillary cell carcinoma ( median indel number of 10 [ 95% ci 911 ] ) and chromophobe renal cell carcinoma ( 8 [ 710 ] ) had the highest absolute indel count across all tumour types , closely followed by renal clear cell carcinoma ( 7 [ 68 ] )  . 
 renal clear cell carcinoma is characterised by loss - offunction mutations in one or more tumour - suppressor genes : vhl , pbrm1 , setd2 , bap1 , and kdm5c , 32 which can be inactivated by nssnv or indel mutations . 
 to exclude the possibility that these hallmark mutations were distorting the results , we recalculated renal clear cell carcinoma indel proportion excluding these genes ; the revised indel proportion remained at 012 . 
when we used previously published multiregion whole - exome sequencing data24 from ten cases of renal clear cell carcinoma to assess the clonal nature of indel mutations , 53 ( 48% ) of 110 frameshifting indels were clonal in nature ( present in all tumour regions )  . the overall effect of nmd on the expression of indelmutated genes was estimated to be 14% ( 7% drop divided by 054 tumour purity ) , suggesting it operates on a subset of transcripts ( appendix p 6 )  . next we sought to investigate the potential immunogenicity of nssnv and indel mutations through analysis of mhc class i - associated tumour - specific neoantigen binding predictions in the pan - cancer tcga cohort . 
the last two boxplots are additional independent renal clear cell carcinoma replication datasets from sato and colleagues23 and gerlinger and colleagues.24 statistical comparison is renal clear cell carcinoma cohort compared with all other non - kidney tcga samples . 
 mutations ( n ) neoantigens ( n ) * mutant - specific neoantigens ( n ) neoantigens per mutation mutant - specific neoantigens per mutation nssnvs fs - indels 335 594 19 849 214 882 39 768 75 224 39 608 enrichment 064 200 313 022 200 894 nssnvs = non - synonymous single nucleotide variants . 
in a similar manner , predictions were made on 19 849 frameshift indel mutations , resulting in 39 768 high - affinity binders with a rate of 200 neoantigens per frameshift mutation ( frameshift neoantigens ; table )  . 
thus on a per mutation basis , frameshift indels could generate around three times more high - affinity neoantigen binders than nssnvs ( table ) , consistent with the prediction in a recent analysis of a colorectal cancer cohort.41 when both wild - type and mutant peptides are predicted to bind , central immune tolerance mechanisms might delete cells with the reactive t - cell receptor.42 therefore , we repeated a pancancer analysis restricting the neoantigens to mutantspecific binders ( ie , where the wild - type peptide is not predicted to be a strong binder ) , and showed that frameshift indels were nine times enriched for mutantallele - only binders ( table )  . of particular interest were genes that are frequently altered via frameshift mutations and with high propensity for mhc binding . 
in a pan - cancer analysis , these genes were enriched for classic tumour - suppressor genes , including tp53 , arid1a , pten , kmt2d , kmt2c , apc , and vhl ( figure 2 )  . 
collectively , the top 15 genes with the highest number of frameshift mutations were mutated in more than 500 samples ( approximately 10% of the cohort with 5777 samples ) with more than 2400 highaffinity neoantigens predicted . 
 furthermore , by virtue of being founder events , many alterations in tumour - suppressor genes are clonal , present in all cancer cells , rendering them compelling targets for immunotherapy.43 we next considered the clinical effect of indel mutations the association between neoantigen by assessing enrichment and therapeutic benefit . 
consistent with a potential role of frameshifts in the generation of neoantigens , those tumour types approved for the use of checkpoint inhibitors were all found to harbour an above average number of frameshift neoantigens , despite substantial differences in the total snv or indel mutational burdeneg , renal cell carcinoma ( figure 3 )  . 
 overall , the number of frameshift neoantigens were significantly higher in the checkpoint inhibitor - approved tumour types versus those that have not been approved to date ( p < 22 10 )  . 
however , the potential presence of frameshift neoantigens alone does not imply that they induce t - cell responses , and hence we tested their effect on checkpoint inhibitor efficacy . 
 although nssnvs ( p = 027 ) and in - frame ( 3n ) indels from an anti - pd - 1 study25 1014 vol 18 august 2017 articles ( p = 019 ) had no association with response to treatment , frameshift indel mutations were significantly associated with anti - pd - 1 response ( p = 0023 ; figure 4a )  . 
the upper quartile of patients with the highest burden of frameshift indels had an 88% ( seven of eight cases ) response to antipd - 1 therapy , compared with 43% ( 11 of 26 cases ) for the lower three quartiles ( odds ratio 95 [ 95% ci 1028923 ] ; figure 4b )  . 
to confirm the reproducibility of this association , further checkpoint inhibitor response data were obtained from two additional melanoma cohorts : snyder and colleagues cohort13 ( n = 62 , anti - ctla - 4 treated ) and van allen and colleagues cohort12 ( n = 100 , anti - ctla - 4 treated )  . 
we did the same analysis in each cohort and frameshift indel burden was significantly associated with checkpoint inhibitor response in both datasets ( hr 34 [ 95% ci 1051127 ] ; p = 00074 for snyder and colleagues cohort and 29 [ 115755 ] ; p = 0032 for van allen and colleagues cohort ; figure 4a )  . 
 an overall meta - analysis across the three cohorts confirmed frameshift indel count to be associated with checkpoint inhibitor response ( p = 47 10 ) , and with a more significant association than nssnv count ( p = 48 10 )  . 
the effect of clonality was additionally assessed , and clonal frameshift indels were found to have a further significantly predictive advantage beyond all frameshift indels ( clonal and subclonal ; appendix p 7 ) , supporting previous work reported by our group.43 overall survival analysis was not different between high and low frameshift indel groups , possibly because of the effect of subsequent therapies on the overall survival ( or 243 [ 95% ci 077773 ] ; p = 0228 for hugo and colleagues cohort25 ; appendix p 8 )  . 
we assessed the association between frameshift indel load and checkpoint inhibitor response in another tumour type by using data obtained from rizvi and colleagues small cohort14 of 31 patients with non - small - cell lung cancer treated with anti - pd - 1 therapy ; no difference was observed ( p = 023 )  . 
 to further investigate the importance of frameshift indels in non - small - cell lung cancer , we did additional analysis using data from jamal - hanjani and colleagues cohort26 of 100 cases , none of whom received treatment with checkpoint inhibitors . 
consistent with our previous findings , 43 we observed lung adenocarcinoma whose tumour 's harboured a high clonal neoantigen burden ( higher than upper quartile of cohort ) survival compared with the bottom three quartiles ( p = 0026 )  . 
 however , across all histological subtypes of non - smallcell lung cancer , survival was found to be significantly improved for patients with a high load of frameshift indels ( vs low load : hr 025 [ 95% ci 006108 ] ; p = 0045 ) ; by contrast , nssnv load was not formally associated ( 036 [ 011121 ] ; p = 0084 ; appendix p 9 )  . 
 of note , the strongest prognostic predictor was for patients in the patients with a high load of both nssnvs and frameshift indels , with elevated levels of both frameshift indels and nssnvs , with no events in this that patients with relapse - free improved exhibited arid1a mll3 mll2 tp53 vps13c map3k1 flna fat1 notch1 pten number of samples mutated figure 2 : recurrent genes with frameshift indel neoantigens data are from all patients in the cancer genome atlas pan - cancer cohort . 
the graph shows the number of unique samples containing a frameshift indel neoantigen and the number of unique neoantigens ( ie , each mutation can generate multiple neoantigens )  . 
multivariate analysis showed some evidence of correlation between variables ( appendix p 2 ) , so further investigation of nssnvs and frameshift indels as predictors in larger patient cohort will be required to draw definitive conclusions . analyses of the indel load and proportion of response achieved from phase 2 studies for the tumour types not approved for checkpoint inhibition were limited by the small sample size and variable patient inclusion criteria such as pdl - 1 immunohistochemistry ( appendix p 4 )  . 
 nevertheless , the proportion of patients achieving a response was higher in triple - negative breast cancer44 compared with other invasive breast carcinoma molecular subtypes , and triple - negative invasive breast carcinoma has a higher burden of frameshift and mutant - specific neoantigens ( figure 3 )  . 
furthermore , mutational burden has been reported as higher in brca1 - mutated triplenegative breast cancer compared with brca - wild - type triple - negative breast cancer , 45 and we specifically observed a higher indel load in these cases ( appendix p 10 )  . 
 however , this outcome did not correlate with tumourinfiltrating lymphocyte density ( appendix p 10 ) , possibly because of the small sample size , absence of indel immunogenicity in this tissue type , or additional factors that modulate tumour - infiltrating lymphocyte density . finally , although genomic data are not available to correlate with checkpoint inhibitor response in renal clear cell carcinoma , we analysed the association between frameshift neoantigen load and immune responses within the tumour using rnaseq gene expression data . 
a high load of frameshift neoantigens was associated with upregulation of immune signatures classically linked to immune activation , including mhc class i antigen and presen tation , cd8 - positive t - cell increased cytolytic activity , a pattern not observed in the high snv - neoantigen group ( figure 5 )  . 
furthermore , correlation analysis within the high frameshift neoantigen group showed that cd8 - positive t - cell signature was correlated with both mhc class i antigen presentation genes ( r = 078 ) and cytolytic activity ( r = 083 ; figure 5 )  . activation , discussion in this study , we analysed the pattern of indel mutations across 19 solid tumour types and found that renal clear cell carcinoma , renal papillary cell carcinoma , and chromophobe renal cell carcinoma have the highest indel rate as a proportion of their total mutational burden and the highest overall indel count and are enriched for mutant - specific neoantigens . 
we also observed that indel number is significantly associated with checkpoint inhibitor response in melanoma . in non - smoking non - small - cell indels are thought to occur as a result of dna strand slippage during dna synthesis46 and their frequency is higher in repetitive sequences , especially those that are at - rich . 
indels are also generated through mutagen exposure , with a higher number observed in smoking than lung cancer ( lung adenocarcinoma ) 40 and higher in uv - exposed ( cutaneous ) versus uv - protected ( mucosal ) melanomas.47 less is known about the repair of indels than snvs ; however , the role of the mismatch repair mechanism instability - high phenotype , characterised by excess indels in repetitive sequences as seen in patients with lynch syndrome . 
 although renal clear cell carcinoma has been reported in patients with lynch syndrome , 48 this cannot account for the overall pattern of indel rates across renal clear cell the microsatellite illustrated by figure 3 : tumour - specific neoantigen counts by cancer type count of snv - derived neoantigens ( a ) , frameshift indel - derived neoantigens ( b ) , and mutant - only neoantigen binders ( c ) , and proportion of neoantigens derived from snvs and indels ( d ) and neoantigens in which mutant allele - only binds ( e )  . 
most renal clear cell carcinomas have loss of chromosome 3p , which encodes the mismatch repair gene mlh1 , but the remaining allele is rarely mutated in sporadic renal clear cell carcinoma . 
another relevant gene encoded on 3p is fhit , and its deficiency has been linked with indel accumulation in knockout mouse models , but the consequences of the heterozygous knockout ( whether haploinsufficient ) are unknown.49 however , as loss of 3p is an infrequent event in renal papillary cell carcinoma and chromophobe renal cell carcinoma and indels are also elevated in both these tumour types , other tissuespecific phenomena are likely to contribute to the increased indel burden across all renal carcinoma subtypes.50 renal clear cell carcinoma and renal papillary in the proximal tubule and cell carcinoma arise chromophobe renal cell carcinoma in the distal tubule of the nephron , and this shared tissue context might be important , even if the three subtypes are molecularly distinct.32 , 50 , 51 the nephron , and the proximal tubule in particular , play a crucial role in the reabsorption of vast volumes of renal filtrate and elimination of waste products of metabolism and toxins , with the effects of toxin elimination evident in the increased incidence of renal clear cell carcinoma in those individuals exposed to aristolochic acid.52 ochratoxin a , a mycotoxin , induces renal tumours in rodents by causing double - strand breaks.53 poly morphisms in genes involved in the repair of double - strand breaks are associated with an increased risk of renal clear cell carcinoma.54 double - strand breaks are mostly repaired by non - homologous end - joining , which is error - prone and can increase the rate of small indels ( 110 bp )  . 
therefore , it is possible that an environmental toxin causes an excess of double - strand vol 18 august 2017 1017 articles a co - inhibition_apc type_ii_ifn_response cytolytic_activity co - inhibition_t_cell co - stimulation_apc pdcs mhc_class_i cd8_t_cells r = 078 mhc class i if - indel - m utations fs - indel - neoatgs ns - snv - neoatgs r = 083 cytolytic activity figure 5 : immune gene signatures in patients with renal clear cell carcinoma ( a ) percentage change in median gene signature expression is shown between high and low groups for each metric on the x - axis as labelled . 
 ( b ) correlation analysis within the high fs - indel - neoatgs group showed the cd8 + t - cell signature was correlated with both mhc class i antigen presentation genes and cytolytic activity . 
brca1 has been shown to inhibit error prone non - homologous endjoining.55 however , we did not observe a correlation between indel load and tumour - infiltrating leucocytes density invasive breast carcinoma . 
 triple - negative in brca1 we observed that indels , which alter the reading frame , generate three times as many predicted neoantigens as nssnvs and nine times as many strong mutant - binding neoantigens where the wild - type sequence is not predicted to strongly bind the hla molecule ( ic50 > 50 nm )  . 
in keeping with this notion , microsatellite instability - high colorectal cancer cd8 - positive leucocytes density correlates positively with the total number of frameshift mutations.56 with the exception of polyomavirus - positive merkel cell carcinoma and hodgkins lymphoma , renal clear cell carcinoma is the only tumour type with a relatively low nssnv burden among the tumour types for which checkpoint inhibitors have been approved for tumour - infiltrating its clinical use . 
however , owing to a comparable frameshift level of mutant - specific high - affinity burden neoantigens is similar to that observed in non - small - cell lung cancer and melanoma , and the same is true of renal papillary cell carcinoma and chromophobe renal the cell carcinoma . 
although immunogenicity of renal papillary cell carcinoma is sparse , complete responses have been noted with the use of both high - dose interleukin 257 and anti - pd - 1 therapy.58 , 59 therapeutic data in chromophobe renal cell carcinoma are limited . the evidence for inhibitor drugs , efforts given the differential benefit across patients , the spectrum of immune - related adverse events , and the cost of checkpoint identify biomarkers of response are ongoing . 
mutational and neoantigen burdens have been shown to correlate with clinical outcomes from checkpoint inhibitor therapy in patients with advanced melanoma , colorectal cancer , and nonsmall - cell lung cancer.13 , 14 , 16 however , some patients with cutaneous melanoma with a low nssnv burden still derive benefit from checkpoint inhibitors , as do some patients with uv - protected mucosal melanomas , 60 which have a characteristically low nssnv burden.61 we analysed three melanoma datasets for which both response and mutational data were available . 
in two of the three studies , 13 , 14 comprising a total of 96 patients treated with either anti - pd - 1 or anti - ctla - 4 therapy , frameshift indel burden was a better predictor of response than nssnv burden . 
in the third study12 of 100 patients treated with anti - ctla - 4 therapy , the nssnv burden and frameshift burden were both significantly associated with checkpoint inhibitor response . 
we note that most of the patients in van allen and colleagues cohort12 were pretreated and therefore any mutational biomarker assessment in this group might be less reliable . although nssnvs contribute greatly towards tumour immunogenicity in heavily mutated tumours , our analyses suggest that frameshift mutations also make a significant contribution relative to their overall low number . 
the contribution of frameshift indels in low nssnv burden tumours might be of greater importance still , as illustrated by the fact that frameshift mutations contribute over a third of the neoantigen load in renal clear cell carcinoma . 
mutational and checkpoint inhibitor response data were not available for renal clear cell carcinoma , hence we could not establish a direct association between frameshift indels and positive checkpoint inhibitor response . 
in terms of indirect evidence in renal clear cell carcinoma , we observed an association between the frameshift neoantigens and upregulation of machinery necessary for antigen presentation by the mhc complex and t - cell activation . 
 furthermore , the cd8 - positive t - cell signature in the frameshift neoantigen - high group was closely related to cytolytic activity , suggesting the presence of antitumour 1018 vol 18 august 2017 articles effectors that could confer sensitivity to immunotherapy . 
 however , no definitive conclusions can be drawn until checkpoint inhibitor response and indel load is directly investigated in a sufficiently powered series of renal clear cell carcinoma cases . lead to the for frameshift neoantigens to contribute to antitumour immunity the mutant peptides must be expressed . 
published analyses62 of germline samples show that premature loss of termination codons frequently expression of the variant allele , but that some mutant transcripts escape nmd on the basis of the exact location of the frameshift within a gene . 
combined analyses of than mutational and expression data 10 000 cancer samples showed that nmd is triggered with variable efficacy , and even when effective might not alter expression because of factors such as short mrna halflife.33 rnaseq analysis in renal clear cell carcinoma cases showed a minimal change in mrna transcript levels for frameshift indel - mutated tumours , suggesting nmd is operating on a subset of transcripts , as expected . 
in this context , the strongly hypoxic microenvironment that characterises renal clear cell carcinomas might be a contributing factor , with evidence showing nmd inhibition in cells subject to hypoxia and other perturbed microenvironmental conditions.63 from more clonal frameshift mutations could be an important source of tumour - specific antigens for personalised immunotherapy strategies , including peptide vaccines and adoptive cell therapy . 
tumour - reactive t cells recognising a frameshifted product of the cdkn2a tumour - suppressor gene were reported to mediate a potent in - vivo response in melanoma.64 in microsatellite instability - high colorectal cancer , frameshift neopeptidespecific cytotoxic t - cell responses were observed in patients harbouring those mutations.65 cytotoxic t - lymphocyte responses to frameshifted proteins have been detected in healthy hereditary non - polyposis colorectal cancer - mutation carriers , raising the possibility of protective immunosurveillance in this population.66 frameshift neoantigens are particularly pertinent in the context of mismatch repair - deficiency , which is a pancancer event , and crucially , frameshifts commonly occurring in microsatellite instability - high colorectal carcinomas have been shown to generate nmd - resistant transcripts.67 in support of this , in a study68 of pd - 1 blockade in patients with microsatellite instability - high tumours from various cancer subtypes , functional analyses in - vivo in a responding patient showed expansion of frameshift neoantigen - specific t - cell clones . frameshift neoantigens provide a unique opportunity to target common tumour - suppressor genes , such as such as tp53 and bap1 , 69 and their founder status also enriches for clonal neoantigens . 
neoantigens derived from driver mutations elicit profound t - cell exhaustion via chronic antigen stimulation , generating t - cell pools refractory to immune therapy.70 thus , early administration of checkpoint blockade might further improve clinical benefit in cancers with particularly antigenic mutations such as renal clear cell carcinoma . 
it is also noteworthy that a high differential affinity between wild - type and mutant peptides is indicative of enhanced tumour protection in vivo.71 the enrichment of mutant - only binders by nine times in neoantigens derived from frameshift mutations relative to nssnvs might therefore partly explain the predictive power of frameshift neoantigens in checkpoint inhibitor responses . a widely recognised challenge in bioinformatics is indel variant calling , due to the inherent nature of shortread sequencing technology ; however , accurate indel calling can be achieved within both a research and clinical context with strict quality control procedures.72 while strict quality control procedures can ensure a low false - positive rate , as a consequence the true rate of indel mutations might be underestimated . in conclusion , we report that kidney cancers carry the indel mutations . 
 highest pan - cancer burden of futhermore , our data suggest that frameshift indels are a highly immunogenic mutational class ; triggering an increased quantity of neoantigens and greater mutant binding specificity . 
collectively , these data might reconcile the outlier nature of immunotherapy responses in renal clear cell carcinoma , highlighting frameshift indels as a potential biomarker of checkpoint inhibitor response and supporting targeting of clonal frameshift indels by both vaccine and cell therapy approaches . the contributors st , kl , and cs designed the study and wrote the manuscript . 
all authors interpreted the data . declaration of interests st reports grants from ventana , outside the submitted work ; and has a patent on indel burden and checkpoint inhibitor response pending , and a patent on targeting of frameshift neoantigens for personalised immunotherapy pending . 
 nm reports personal fees from achilles therapeutics , outside of the submitted work ; and has two patents pending ( pct / ep2016 / 059401 and pct / ep2016 / 071471 )  . 
 jl reports personal fees from eisai , glaxosmithkline , kymab , roche / genentech , secarna , pierre fabre , and eusa pharma ; and grants and personal fees from bristol - myers squibb , merck sharp & dohme , pfizer , and novartis , outside of the submitted work . 
cs reports personal fees from janssen , boehringer ingelheim , ventana , novartis , roche , sequenom , natera , achilles therapeutics , and sarah cannon research institute , and personal fees and other from apogen biotechnologies , epic sciences , and grail , outside of the submitted work ; and has a patent on indel burden and checkpoint inhibitor response pending and a patent on targeting of frameshift neoantigens for personalised immunotherapy pending . 
all other authors declare no competing interests . vol 18 august 2017 1019 articles acknowledgments st is funded by cancer research uk ( grant reference number c50947 / a )  . 
tc , st , mg , and jl are funded by the national institute for health research ( nihr ) biomedical research centre at the royal marsden hospital national health service foundation trust ( st grant reference number a109 )  . 
cs is funded by cancer research uk ( tracerx ) , the rosetrees trust , novonordisk foundation ( id 16584 ) , eu fp7 ( projects predict and responsify , id number 259303 ) , the prostate cancer foundation , the breast cancer research foundation , the european research council ( theseus ) , and national institute for health research university college london hospitals biomedical research centre . 
we thank levi garraway , eli van allen , alexandra snyder , matthew hellman , naiyer rizvi , and timothy chan for kindly allowing access to their checkpoint inhibitor datasets . 
the results published here are in part based on data generated by the cancer genome atlas research network . published online august 6 , 2019 s1470 - 2045 ( 19 ) 30530 - 3 published online july 30 , 2019 s1470 - 2045 ( 19 ) 30521 - 2 correction to lancet oncol 2019 ; 20 : 114859 correction to lancet oncol 2019 ; 20 : 121125 bonvalot s , rutkowski pl , thariat j , et al . 
 nbtxr3 , a first - in - class radioenhancer hafnium oxide nanoparticle , plus radiotherapy versus radiotherapy alone in patients with locally advanced soft - tissue sarcoma ( act.in.sarc ) : a multicentre , phase 23 , randomised , controlled trial . 
 lancet oncol 2019 ; 20 : 114859in this article , the funder pharmaengine , inc , was inadvertently omitted and has now been added to the funding line in the summary and to the acknowledgments . 
a repeated sentence has been deleted from the fifth paragraph of the statistical analysis section of the methods , and some minor typographical errors have been corrected throughout the paper . 
 these corrections have been made to the online version as of sept 2 , 2019 . correction to lancet oncol 2019 ; 20 : 117182 nen nr , reisel d , leimbach a , et al . 
the following sentence has been added to the figure 4 caption : sdi quintiles are ordered from high to low sdi quintile , and gbd super - regions are alphabetically ordered . 
the next sentence should read : country order selected by total absolute dalys ; countries with the greatest total absolute dalys , of the fifty most populous countries in the world , are listed first . 
this correction has been made to the online version as of aug 6 , 2019 . correction to lancet oncol 2019 ; 20 : 127385 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
lancet oncol 2019 ; 20 : 127385in this article , data ( hazard ratios , 95% cis , and p values ) in the following sentence on p 1279 have been corrected : in women with stage iii disease , 5 - year overall survival was 838% ( 95% ci 784895 ) with chemoradiotherapy versus 820% ( 95% ci 765877 ) with radio therapy alone ( hr 084 [ 95% ci 052138 ] ; p = 050 ) , and 5 - year failure - free survival was 813% ( 95% ci 747863 ) with chemoradiotherapy versus 773% ( 95% ci 705827 ) with radiotherapy alone ( hr 087 [ 95% ci 056136 ] p = 054 ; appendix p 8 )  . 
on p 1282 , the same data ( hazard ratios and 95% cis ) in the following sentence have also been corrected : for women with stage iii endometrial cancer , combined adjuvant treatment yielded only a small absolute improvement of 2% ( hr 084 ; 95% ci 052138 ) in 5 - year overall survival and of 4% ( 087 ; 056136 ) in failure - free survival . 
 these corrections have been made to the online version as of sept 2 , 2019 , and the printed version is correct . correction to lancet oncol 2019 ; 20 : e41733 herrera fg , irving m , kandalaft le , coukos g . 
 this correction has been made as of july 30 , 2019 . correction to lancet oncol 2019 ; 20 : e50321 spence d , dyer r , andall - brereton g , et al . 
 lancet oncol 2019 ; 20 : e50321the affiliations of authors dingle spence and m austin argentieri have been corrected in the online version as of sept 2 , 2019 . vol 20 september 2019 e468 corrections correction to lancet oncol 2016 ; 17 : 72737 correction to lancet oncol 2017 ; 18 : 91728 correction to lancet oncol 2017 ; 18 : 127484 published online july 28 , 2017 s1470 - 2045 ( 17 ) 30575 - 2 published online august 8 , 2017 s1470 - 2045 ( 17 ) 30591 - 0 and cancer ledermann randomised , platinum - sensitive , ( solo2 / engot - ov21 ) : pujade - lauraine e , ja , selle f , et al , and the solo2 / engotinvestigators . 
lancet oncol 2017 ; 18 : 127484in the methods section of the summary and in the randomisation and masking section of the main paper , the stratification groups interval for platinum - free should have been > 612 months vs > 12 months . 
in table 2 , the first line of the legend should have read grade 12 adverse events , presented as haematological or nonhaematological , occurring in at least 10% of patients in either treatment group are shown , together with their associated grade 3 and grade 4 adverse events . 
these corrections have been made to the online version as of sept 1 , 2017 , and the printed article is correct . for progression - free phase active - controlled , stebbing j , baranau y , baryash v , et al . 
lancet oncol 2017 ; 18 : 91728in this article , difference values representing the proportion of patients achieving pathological complete response between groups should have been listed without % following signs . 
additionally , sentence should have read the treatment outcome difference was 003 ( 95% ci 011 to 005 ) , with the 95% ci falling within the prespecified 015 equivalence marg these corrections have been made to the online version as of sept 1 , 2017 . the correction to lancet oncol 2017 ; 18 : 118291 mj , mcdermott overman leach jl , et al . 
nivolumab in patients with metastatic dna mismatch repairdeficient or microsatellite instability - high colorectal cancer ( checkmate 142 ) : an open - label , multicentre , phase 2 study . 
 lancet oncol 2017 ; 18 : 118291in this article , in the findings section of the summary , and in the results section of the main paper , kaplanmeier 12 - month estimate should have been stated before the estimate 86% , 95% ci 6295 . 
these corrections have been made to the online version as of sept 1 , and the printed article is correct . duchesne gm , woo hh , bassett jk , et al . 
lancet oncol 2016 ; 17 : 72737in figure 1 of this article , the number of patients who withdrew after randomisation should have been 1 in the delayed adt group and 2 in the immediate adt group . 
lancet oncol 2017 ; 18 : e429 the title of this correspondence should have been evidenced - based medicine in glioma : molecular biology is only part of the story and not evidencebased management of adult patients with diffuse glioma . 
this correction has been made to the online version as of aug 8 , 2017 . correction to lancet oncol 2017 ; 18 : 104048 mahajan a , ahmed s , mcaleer mf , et al . 
 lancet oncol 2017 ; 18 : 104048in the eighth paragraph in the results of this article , the phrase 12 - month time to distant brain recurrence should have said 12 - month freedom from distant brain recurrence . 
this correction has been made to the online version as of sept 1 , 2017 . vol 18 september 2017 e510 corrections correction to lancet oncol 2017 ; 18 : 132737 correction to lancet oncol 2017 ; 18 : 133847 correction to lancet oncol 2017 ; 18 : e564 dimopoulos ma , goldschmidt h , niesvizky r , et al . 
 lancet oncol 2017 ; 18 : 132737in the results section of this article , the data presented for any - grade adverse diarrhoea events should read diarrhoea ( 168 [ 36% ] vs 185 [ 41% ] )  . 
 these corrections have been made to the online version as of sept 27 , 2017 , and the printed article is correct . myelodysplastic in patients with platzbecker u , germing u , gtze ks , et al . 
luspatercept for the treatment of anaemia lowerrisk syndromes ( pace - mds ) : a multicentre , openlabel phase 2 dose - finding study with long - term extension study . 
 18 : e564in the second paragraph of brian samuels affiliation , the sentence in parentheses should have read ( summit cancer centers , post falls , id , usa )  . 
in the third paragraph , the sentence and quote from brian samuels as should have samuels summarised , we decided to recapitulate the original phase 2 study in liposarcomas pazopanib is active in the treatment of liposarcomas , just as it is for other subtypes of sarcoma . 
 these corrections has been made to the online version as of sept 27 , 2017 . vol 18 october 2017 e562 corrections editorial for the study of necitumumab in lung cancer see articles page 328 for the study in the journal of the national cancer institute see j natl cancer inst 2014 ; doi : 10.1093 / jnci / dju302 rethinking trial eligibility in the ncd era patient eligibility represents one of the most challenging factors in the design of a clinical trial . 
in this issue of the lancet oncology , a study of necitumumab plus pemetrexed and cisplatin for rst - line treatment of patients with non - small - cell lung cancer lists one of its exclusion criteria as patients having symptomatic brain metastases , despite this being a common occurrence in this setting . 
an article in the november , 2014 , issue of the journal of the national cancer institute reported that up to 18% of patients are not permitted to participate in clinical trials because of previous cancer diagnoses . 
 this bias towards accruing patient populations that maximise the apparent bene ts of a treatment highlights an important issue at the heart of clinical trial design that will become more prevalent as the number of cancer survivors , and people living longer with conditions considered to be chronic diseases , increases . the practice of excluding patients with previous cancer diagnoses is based on the assumption that this population are more likely to be less t , less likely to tolerate or respond to treatment , more prone to develop clinical or radiological changes that may not be attributable to the index disease , carry comorbidities , and have di erent survival rates than those with a rst - time diagnosis of cancer . 
in fact , in the journal of the national cancer institute article , the authors conclude that patient outcomes can be as good asor even better thanthose of patients with no previous cancer diagnosis , possibly because of more intensive clinical and radiographic surveillance during follow - up of the primary cancer , resulting in an earlier diagnosis of the secondary cancer . 
moreover , these exclusions hinder attempts to increase patient participation in oncology clinical trialsparticularly concerning when around one in ve adult cancer trials closes early for reasons unrelated to the safety or e cacy of the intervention , with poor accrual being the most common cause . 
factors such as age , sex , concomitant medication use , and comorbidities ( most notably hiv , and liver and renal diseasewhich are now generally considered to be manageable , chronic conditions ) , are all common barriers to patient enrolment , which could , in turn , prevent fair access to cutting - edge treatments for these groups of patients . 
 but , is exclusion of these patient populations really justi ed ? and is their omission right , ethically ? all trials must have an a - priori protocol and analysis plan in place before patient accrual , and thus theoretically there is no reason why trial designs could not include strati cation factors related to these inclusion and exclusion criteria , and carry out subgroup analyses to take them into account . 
with the ageing population and increasing burden of non - communicable diseases , the validity of extrapolating existing evidence , based on results from younger , healthier populations , becomes increasingly disconnected from the realities in the target population . as treatment outcomes continue to improve for all diseases , not just cancer , it is inevitable that the incidence of patients with chronic diseases will continue to rise . 
if study investigators are able to strike a balance between accruing patient populations that are representative of the general population , and accruing patient populations that will not be prone to major losses or who have comorbidities that might a ect the clinical outcome of their study , then widening lead to improved patient eligibility criteria could patient accrual , higher completion rates , and greater treatment equity . 
 the lancet oncology vol 16 march 2015 articles intensity - modulated fractionated radiotherapy versus stereotactic body radiotherapy for prostate cancer ( pace - b ) : acute toxicity findings from an international , randomised , open - label , phase 3 , non - inferiority trial douglas h brand * , alison c tree * , peter ostler , hans van der voet , andrew loblaw , william chu , daniel ford , shaun tolan , suneil jain , alexander martin , john staffurth , philip camilleri , kiran kancherla , john frew , andrew chan , ian s dayes , daniel henderson , stephanie brown , clare cruickshank , stephanie burnett , aileen duffton , clare griffin , victoria hinder , kirsty morrison , olivia naismith , emma hall , nicholas van as , on behalf of the pace trial investigators summary background localised prostate cancer treated with external - beam radiotherapy . 
we report the acute toxicity findings from a randomised trial of standard - of - care conventionally fractionated or moderately hypofractionated radiotherapy versus five - fraction stereotactic body radiotherapy for low - risk to intermediate - risk localised prostate cancer . is commonly methods pace is an international , phase 3 , open - label , randomised , non - inferiority trial . 
in pace - b , eligible men aged 18 years and older , with who performance status 02 , low - risk or intermediate - risk prostate adenocarcinoma ( gleason 4 + 3 excluded ) , and scheduled to receive radiotherapy were recruited from 37 centres in three countries ( uk , ireland , and canada )  . 
participants were randomly allocated ( 1 : 1 ) by computerised central randomisation with permuted blocks ( size four and six ) , stratified by centre and risk group , to conventionally fractionated or moderately hypofractionated radiotherapy ( 78 gy in 39 fractions over 78 weeks or 62 gy in 20 fractions over 4 weeks , respectively ) or stereotactic body radiotherapy ( 3625 gy in five fractions over 12 weeks )  . 
the coprimary outcomes for this acute toxicity substudy were worst grade 2 or more severe radiation therapy oncology group ( rtog ) gastrointestinal or genitourinary toxic effects score up to 12 weeks after radiotherapy . 
pace - b recruitment is complete and follow - up is ongoing . findings between aug 7 , 2012 , and jan 4 , 2018 , we randomly assigned 874 men to conventionally fractionated or moderately hypofractionated radiotherapy ( n = 441 ) or stereotactic body radiotherapy ( n = 433 )  . 
432 ( 98% ) of 441 patients allocated to conventionally fractionated or moderately hypofractionated radiotherapy and 415 ( 96% ) of 433 patients allocated to stereotactic body radiotherapy received at least one fraction of allocated treatment . 
worst acute rtog gastrointestinal toxic effect proportions were as follows : grade 2 or more severe toxic events in 53 ( 12% ) of 432 patients in the conventionally fractionated or moderately hypofractionated radiotherapy group versus 43 ( 10% ) of 415 patients in the stereotactic body radiotherapy group ( difference 19 percentage points , 95% ci 62 to 24 ; p = 038 )  . 
worst acute rtog genitourinary toxicity proportions were as follows : grade 2 or worse toxicity in 118 ( 27% ) of 432 patients in the conventionally fractionated or moderately hypofractionated radiotherapy group versus 96 ( 23% ) of 415 patients in the stereotactic body radiotherapy group ( difference 42 percentage points , 95% ci 100 to 17 ; p = 016 )  . 
by contrast , our results suggest that substantially shortening treatment courses with stereotactic body radiotherapy does not increase either gastrointestinal or genitourinary acute toxicity . funding accuray and national institute of health research . copyright 2019 the author ( s )  . 
grade 2 or worse acute toxicity estimates for ultra - hypofractionation were similar to standard fractionation , ranging from 424% for gastrointestinal toxicity and 440% for genitourinary toxicity . added value of this study to our knowledge , this is the first published phase 3 randomised trial investigating acute toxicity after ultra - hypofractionated stereotactic body radiotherapy , delivered over five fractions , compared with standard fractionation schedules . 
overall , this study showed similar acute toxicity for ultra - hypofractionation compared with standard fractionation , with only common terminology criteria for adverse events grade 2 or more severe gastrointestinal toxicity being significantly worse . 
proportions of patients with acute grade 3 toxicity were low , which adds to the body of evidence for low acute toxicity , as was also reported for seven - fraction hypofractionated radiotherapy in the hypo - rt - pc trial . implications of all the available evidence ultra - hypofractionated radiotherapy over five fractions appears to be tolerable in the short term in men with low - risk of intermediate - risk prostate adenocarcinoma . 
the hypo - rt - pc trial showed that a schedule of 427 gy delivered every other day over 25 weeks ( 61 gy per fraction ) was non - inferior in terms of failure - free survival compared with conventional fractionation of 78 gy over 8 weeks ( 2 gy per fraction ) , with similar proportions of late toxicity in each group . 
late toxicity and efficacy data for the pace - b trial are awaited and are required before a new standard of care for localised prostate cancer can be recommended . data from the randomised protect trial , which compared surgery , ebrt , and active monitoring , have given reassurance that cancer outcomes are similar for lowrisk and intermediate - risk disease , regardless of the management option used.5 therefore , side - effects might influence decision making , with gastrointestinal , genitourinary , and sexual side - effects being common concerns.6 additionally , the tolerability of treatment for a given patient is crucial , with anaesthetic and intraoperative risks balanced against the inconvenience of multiweek courses of ebrt . hypofractionationincreasing the dose per fraction above the conventional 2 gy , thus reducing the total fractions requiredis an appealing approach . 
first , the greater fraction size sensitivity of prostate cancer ( indicated by a lower / ratio710 ) , relative to the relevant late gastrointestinal and genitourinary side - effects , means that the therapeutic ratio might be improved by hypofractionation.11 second , fewer fractions are needed with hypofractionation , allowing for quicker and more cost - effective ebrt treatment courses.12 three major non - inferiority phase 3 randomised controlled trials have confirmed the safety and efficacy of moderate hypofractionation ( 2530 gy per fraction ) , 11 , 13 , 14 which has gained acceptance as a standardof - care option.15 , 16 although the proportions of patients with late toxicity were low , some intertrial differences in the proportion of patients who experienced acute toxicity were observed . 
the chhip trial reported significantly higher proportions of patients with peak acute radiation therapy oncology group ( rtog ) grade 2 or worse gastrointestinal toxicity38% in both hypofractionated fractionation groupscompared with conventional ( 25% ; p < 00001 for both comparisons ) .11 similarly , the profit trial reported a significantly ( p = 0003 ) higher proportion of patients with cumulative acute rtog grade 2 or worse gastrointestinal toxic effect proportions in the hypofractionated arm ( 167% ) versus conventional fractionation ( 105% ) .14 for both trials , acute grade 2 or worse genitourinary toxic effects were similar between hypofractionated and conventionally fractionated groups . 
 by contrast , the rtog - 0415 hypo fractionation trial did not find a significant difference in acute gastrointestinal or genitourinary toxic effects between groups.13 although more profound hypofractionation beyond 30 gy per fraction would allow further reductions in the overall treatment time , the accelerated schedule might worsen acute toxicity , as seen in the chhip trial , 11 potentially leading to late effects.17 substantial evidence exists for the efficacy of ultrahypofractionation , with over 6000 patients treated in prospective studies and excellent 5 - year biochemical progression - free survival in a recent meta - analysis ( 953% , 95% ci 913975 ) .18 a phase 3 trial ( hypo - rt - pc ) reported good bio chemical progression - free survival and acceptable proportions of toxic effects for seven - fraction ultra - hypofractionated radiotherapy.19 to our knowledge , 1532 vol 20 november 2019 articles see online for appendix phase 3 randomised toxic effect data for five - fraction treatment have not previously been reported . we report the acute toxicity findings ( both clinicianreported and patient - reported ) the pace - b randomised , controlled trial , which compared standardof - care conventionally fractionated or moderately hypofractionated radiotherapy with five - fraction stereotactic body radiotherapy for low - risk to intermediate - risk localised prostate cancer . from is an methods study design and participants international , phase 3 , open - label , pace - b randomised , non - inferiority centres ( appendix p 7 ) in three countries ( uk , ireland , and canada ) aiming to assess non - inferiority of stereotactic body radiotherapy compared with conventionally fractionated or moderately hypofractionated radiotherapy for biochemical or clinical failure . at 37 trial ( psa ) concentration the pace study comprises multiple cohorts ( pace - a , pace - b , and pace - c ) which were independently randomised . 
eligible patients were men aged at least 18 years , with who performance status of 02 , 20 life expectancy of at least 5 years , and histologically confirmed prostate adenocarcinoma . 
 all patients had nccn low - risk or intermediate - risk disease.4 low - risk patients had ct1ct2a ( tnm 6th edition21 ) , n0 - x , m0 - x , gleason score 6 or less , and prostate - specific antigen less than 10 ng / ml . 
intermediate - risk patients had at least one of the following criteria : t2c , gleason score 7 ( 3 + 4 for pace ; gleason 4 + 3 was excluded ) , and psa 1020 ng / ml . 
 a minimum of ten biopsy cores taken within the last 18 months before randomisation were required , except for those progres sing on active surveillance , whose last biopsy was suitable for pace - b and required treatment ( eg , psa or mri progression )  . 
detailed inclusion and exclusion criteria are in the protocol ( appendix pp 8283 )  . the trial was approved by the london chelsea research ethics committee ( reference 11 / lo / 1915 ) in the uk and the relevant institutional review boards in ireland and canada . 
all participants provided voluntary written informed consent . randomisation and masking patients were randomly assigned ( 1 : 1 ) to conventionally fractionated or moderately hypofractionated radiotherapy or stereotactic body radiotherapy . 
randomisation was done centrally by the institute of cancer research clinical trials and statistics unit ( icr - ctsu ) , by telephone ( uk and ireland ) or fax ( canada ) , with allocation by computer generated random permuted blocks ( size four and six ) and stratification by centre and risk group ( low or intermediate )  . 
sequence generation , enrolment , and trial group assignment were done by icr - ctsu staff who were not involved in the clinical running of the trial or data collection . 
participants and researchers were not masked to treatment assignment . procedures before radiotherapy , three or more prostatic fiducial markers were strongly recommended for all participants to permit more accurate image - guided radiotherapy and ct or mri fusion . 
the clinical target volume ( ctv ) was the prostate only ( low - risk patients ) or prostate and proximal 1 cm of seminal vesicles ( intermediate - risk patients )  . 
the recommended conventionally fractionated or moderately hypofractionated radiotherapy ctv to planning target volume ( ptv ) expansion was 59 mm isometric , except posteriorly 37 mthe recommended stereotactic body radiotherapy ctv to ptv expansion was 45 mm isometric , except posteriorly 35 mdose constraints were applied to organs at risk and were amended during the trial . 
androgen deprivation therapy was not permitted . the conventionally fractionated or moderately hypofractionated radiotherapy ptv dose was 78 gy in 39 daily fractions or , following an approved protocol amendment ( on march 24 , 2016 ) , 62 gy in 20 daily fractions . 
this change followed the chhip trial data supporting moderate hypofractionation , 11 but with a higher dose ( 62 gy vs 60 gy ) because the pace - b protocol prohibits androgen deprivation therapy . 
data from the profit trial which assessed 60 gy in 20 fractions , without androgen deprivation therapy , were not available at that time.14 after the protocol amendment , centres were required to choose either 78 gy in 39 fractions or 62 gy in 20 fractions as their control treatment for all subsequent patients . 
the stereotactic body radiotherapy ptv dose was 3625 gy in five fractions over 12 weeks ( ie , daily or alternate days , at centre discretion ) , with an additional secondary ctv dose target of 40 gy . 
the cyberknife treatment platform ( accuray ; sunnyvale , ca , usa ) was vol 20 november 2019 1533 articles initially mandatory for all stereotactic body radiotherapy ; however , sponsorship changes prompted a protocol amendment ( on oct 24 , 2014 ) permitting stereotactic body radiotherapy delivery on conventional linear accelerators . 
detailed prescription objectives , along with minor variations permitted , are listed in the protocol ( appendix pp 93100 )  . treatment was mandated to commence within 12 weeks of randomisation , with 8 weeks or less strongly recommended . 
for stereotactic body radiotherapy , intrafractional motion monitoring was permitted ; otherwise , a repeat static image was required for stereotactic body radiotherapy fraction delivery extending beyond 3 m a radiotherapy quality assurance programme was undertaken for each centre to ensure consistency with the trial protocol and quality of radiotherapy treatments ( appendix p 113 )  . participants were assessed on alternate weeks during conventionally fractionated or moderately hypo fractionated radiotherapy and on the final fraction for stereotactic body radiotherapy , and at weeks 2 , 4 , 8 , and 12 after the end of treatment for all patients in both groups . 
 two clinician - reported outcomes were collectedrtog ( gastrointestinal and genitourinary domains ) at baseline and every visit and common terminology criteria for adverse events ( ctcae version 4.03 ) at baseline and follow - up weeks 2 , 4 , 8 , and 12 , with additional end - oftreatment assessment for patients in the stereotactic body radio therapy group . 
specific ctcae items in the gastrointestinal composite are anal pain , colitis , constipation , diarrhoea , diverticulitis , faecal incontinence , fistula , gastro intestinal pain , haemor rhoids , gastro intestinal haemorrhage , proctitis , rectal pain , gastro intestinal unspecified , and rectal prolapse . 
specific ctcae items in the genitourinary composite are bladder spasm , cystitis , haematuria , prostatic obstruction , urinary frequency , urinary incontinence , urinary retention , urinary urgency , and urethral stricture . 
we used paper questionnaires to collect four patient - reported outcome measures expanded prostate cancer index composite short form ( epic - 26 ) and the vaizey faecal incontinence score , at baseline and weeks 4 and 12 ; international prostate symptom score ( ipss ) , at baseline and weeks 2 , 4 , 8 , and 12 ; and the international index of erectile function 5 - question ( iief - 5 ) score , at baseline and week 12 . 
 subsequent follow - up is ongoing ( and will continue until all patients have reached 10 years ) , with the full schedule , along with criteria for removal of patients from the study , available in the protocol ( appendix pp 8492 )  . 
for each scale , the baseline , worst , worst above baseline , and week 12 ( residual ) toxic effects were of interest , with exact definitions detailed in the statistical analysis plan ( appendix pp 14547 )  . outcomes the primary endpoint of pace - b is freedom from biochemical or clinical failure , the data for which is not yet mature . 
a statistical analysis plan for this substudy ( appendix pp 129158 ) was prospectively written , with worst grade 2 or worse rtog toxic effects score , up to week 12 follow - up after radiotherapy finished , for both gastrointestinal and genitourinary systems , as coprimary sub - study endpoints . separately for gastrointestinal and genitourinary systems , the numerator was patients with recorded rtog grade 2 or worse toxic effects at any point after baseline up to week 12 after radiotherapy . 
pace - b secondary endpoints were acute toxicity ( ctcae ) , late toxicity ( ctcae and rtog ) , progression - free survival , disease - specific survival , overall survival , distant progression , commencement of hormone therapy , and acute and late patient - reported toxicity ( epic , ipss , iief - 5 , and vaizey scales )  . 
all but the physicianreported and patient - reported toxicity outcomes will be reported elsewhere . statistical analysis for this acute toxicity analysis , patients were analysed per protocol , with those receiving one or more fractions of conventionally fractionated or moderately hypofractionated radiotherapy or stereotactic body radiotherapy included . 
patients receiving both conventionally fractionated or moderately hypo fractionated radiotherapy and stereotactic body radiotherapy fractions were excluded unless the reason was toxicity - related , where analysis was on the first treatment fraction received . 
the pace - b trial targeted recruitment of 858 patients to exclude a hazard ratio [ hr ] of 145 in biochemical or clinical failure at 5 years , with consideration given to also excluding a 6% increase in grade 2 gastrointestinal or genitourinary late toxicity at 2 years ( appendix pp 10708 )  . 
for this acute toxicity substudy , we assumed conventionally fractionated or moderately hypofractionated radiotherapy group acute rtog grade 2 or worse toxic effect proportions of 25% ( gastrointestinal ) and 40% ( genitourinary ) , as per the chhip trial.11 with two - sided = 0025 for each endpoint , 1534 vol 20 november 2019 articles we estimated that ongoing pace - b recruitment would provide 83% power to exclude a 10% increase in acute gastrointestinal toxic effects and 845% power to exclude an 11% increase in acute genitourinary toxic effects for the stereotactic body radiotherapy group ( appendix pp 13940 )  . we used the test to compare treatment groups for the coprimary endpoints . 
the different durations of radiotherapy ( conventionally fractionated or moderately hypofractionated radiotherapy 4 or 78 weeks ; stereotactic body radiotherapy 1 or 2 weeks ) led to differing timepoints of toxicity assessment . 
rtog ( assessed during radiotherapy ) and ctcae ( assessed at end of radiotherapy for stereotactic body radiotherapy ) graphical presentation is therefore protrayed as four different groups and also displayed grouped as 12 weeks and 475 weeks ( interpolation detailed in appendix p 6 )  . 
we calculated confidence intervals for the difference in proportions by normal approximation . we rescaled epic - 26 scores to a 0100 point scale , with higher scores representing better quality of life.22 subdomains were scored if sufficient questions were completed as follows : urinary incontinence ( four of four questions ) , urinary obstructive ( four of four questions ) , bowel ( five of six questions ) , sexual ( five of six questions ) , and hormonal ( four of five questions ) .22 a clinically important point reduction in epic - 26 subdomain score was as follows : urinary incontinence ( 8 points ) , urinary obstruction ( 6 points ) , bowel ( 5 points ) , sexual ( 11 points ) , and hormonal ( 5 points ) .23 ipss severity categories were assessed as none ( 0 points ) , mild ( 17 points ) , moderate ( 819 points ) , and severe ( 2035 points ) .24 exploratory examination of cyberknife versus standard linear accelerators for patients undergoing stereotactic body radiotherapy was prespecified in the protocol when amendment permitted standard linear accelerators ( aug 5 , 2014 )  . 
the prespecified statistical analysis plan called for a multivariate analysis , which will be published subsequently , but a post - hoc decision due to the paucity of published non - cyberknife toxicity data was made to analyse the worst rtog grade 2 or more severe gastrointestinal and genitourinary toxic effects for patients undergoing stereotactic body radiotherapy , split by cyberknife and non - cyberknife use , interpreted at a significant p - value of 0001 . 
since centre - level effects could influence this non - randomised analysis ( eg , variation in toxic effect reporting ) , we did similar analysis for patients undergoing conventionally fractionated or moderately hypofractionated radiotherapy , separated by whether their centre used cyberknife or non - cyberknife for stereotactic body radiotherapy treatments . the study was overseen by a trial steering committee and an independent data monitoring committee ( idmc ; appendix p 3 )  . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results between aug 7 , 2012 , and jan 4 , 2018 , we randomly assigned 874 men to conventionally fractionated or moderately hypofractionated radiotherapy ( n = 441 ) or stereotactic body radiotherapy ( n = 433 ; figure 1 )  . 
11 patients received non - protocol regimens due to crossing over treatment groups ( figure 1 ; appendix p 8 ) ; one cross over was toxicityrelated ( a patient in the stereotactic body radiotherapy group with grade 3 urinary toxicity ) , meaning that 432 patients received at least one fraction of conventionally fractionated or moderately hypo fractionated radiotherapy and 416 patients received at least one fraction of stereotactic body radiotherapy . 
two men received both stereotactic body radiotherapy and conventionally fractionated or moderately hypo fractionated radiotherapy treatments one patient who received two fractions of stereotactic body radiotherapy ( 145 gy ) then developed grade 3 toxicity ( urosepsis ) and switched to conventionally fractionated or moderately hypofractionated radiotherapy ( further 46 gy in 23 fractions ) was not excluded from the toxicity analysis because he had toxic effects after two fractions of sterotactic body radiotherapy and one patient who received a single incomplete fraction of stereotactic body radiotherapy ( < 725 gy , set - up issues ) and switched to conventionally fractionated or moderately hypo fractionated radiotherapy ( further 55 gy in 20 fractions ) was excluded ( figure 1 )  . baseline characteristics for each per - protocol treat ment group were similar ( table 1 )  . 
radiotherapy delivery techniques ( planning , image - guided radiotherapy , and margins ) differed between arms , as expected , although recorded supportive prescribing appeared to be similar ( appendix pp 911 )  . 
despite fiducial recommendations for both groups , more patients in the stereotactic body radiotherapy group received fiducial markers ( 303 [ 73% ] of 415 patients ) than did patients in the conventionally fractionated or moderately hypofractionated radio therapy group ( 245 [ 57% ] of 432 patients )  . 
 * one patient who received two fractions of stereotactic body radiotherapy then developed grade 3 toxicity ( urosepsis ) and switched to conventionally fractionated or moderately hypofractionated radiotherapy ( further 46 gy in 23 fractions ) was not excluded from the toxicity analysis because he had toxic effects after two fractions of sterotactic body radiotherapy . 
patient illness caused non - completion of three rtog forms ( two in the conventionally fractionated or moderately hypo fractionated radiotherapy group and one in the stereotactic body radiotherapy group ) and one ctcae form in the stereotactic body radiotherapy group . 
psa = prostate - specific antigen . active surveillance before trial enrolment ( table 1 continues in next column ) gastrointestinal toxic effects ( appendix p 15 ) , including worst rtog gastrointestinal toxic effects of grade 3 or more severe ( four [ 1% ] of 432 patients in the conventionally fractionated or moderately hypo fraction ated radiotherapy group vs one [ < 1% ] of 415 patients in the stereotactic body radiotherapy group ; difference 07 percentage points , 95% ci 17 to 03 ; p = 037 ) , nor for genitourinary toxic effects ( appendix p 16 ) , including worst rtog genitourinary toxic effects of grade 3 or more severe ( seven [ 2% ] of 432 patients in the conventionally fractionated or moderately hypofraction ated radiotherapy group vs ten [ 2% ] of 415 patients in the stereotactic body radiotherapy group ; difference 08 percentage points , 11 to 27 ; p = 047 )  . we recorded rtog acute toxicity over time for gastrointestinal and genitourinary toxic effects and observed a similar time course of toxicity peak and recovery between the groups ( figure 2 )  . 
graphical representation of the four different durations of treatment separately ( stereotactic body radiotherapy 1 week and 2 weeks and conventionally fractionated or moderately hypofractionated radiotherapy 4 weeks and 78 weeks ) is shown in the appendix ( p 17 )  . 
the rtog baseline , worst , worst ( exceeding baseline ) , and week - 12 after radiotherapy vol 20 november 2019 1537 articles conventionally fractionated or moderately hypofractionated radiotherapy ( n = 432 ) stereotactic body radiotherapy ( n = 415 ) grade 1 grade 2 grade 3 grade 4 grade 1 grade 2 gastrointestinal genitourinary 264 ( 61% ) 254 ( 59% ) 49 ( 11% ) 111 ( 26% ) 4 ( 1% ) 6 ( 1% ) 1 ( < 1% ) 219 ( 53% ) 236 ( 57% ) 42 ( 10% ) 86 ( 21% ) grade 3 1 ( < 1% ) 8 ( 2% ) grade 4 2 ( < 1% ) data are n ( % )  . 
numbers at risk for each arm are asynchronous because they are shown only at data collection timepoints ( which are non - simultaneous relative to the start of radiotherapy )  . 
 sbrt = stereotactic body radiotherapy . gastrointestinal and geni tourinary toxic effects are summarised in the appendix ( pp 1516 )  . a summary table of all common and serious ctcae adverse events is provided in the appendix ( pp 1819 )  . 
 17 serious adverse events were reported ( five in the conventionally fractionated or moderately hypo fractionated radiotherapy group and 12 in the stereotactic body radiotherapy group ) up to 12 weeks after radiotherapy , of which 15 ( five in the conventionally fractionated or moderately hypofractionated radiotherapy and ten in the stereotactic body radiotherapy group ) were related to treatment ( appendix p 20 )  . 
we recorded ctcae acute toxicity over time for composite gastrointestinal and genitourinary toxic effects , and observed a similar time course of toxicity peak and recovery between stereotactic body radiotherapy and conventionally fractionated or moderately hypofractionated radiotherapy ( figure 3 )  . 
 graphical representation of the four different durations of treatment separately ( stereotactic body radiotherapy 1 week and 2 weeks and conventionally fractionated or moderately hypofractionated radiotherapy 4 weeks and 78 weeks ) is shown in the appendix ( p 21 )  . 
data for toxic composite gastrointestinal and genitourinary effects , at baseline , worst , worst ( exceeding baseline ) , and week 12 after radiotherapy are summarised in the appendix ( pp 2223 ) , with the results of hypothesis testing . 
stereotactic body radiotherapy was statistically significantly worse compared with the conventionally fractionated or moderately hypofractionated radiotherapy for two of the ctcae secondary endpoints analysed worst ctcae grade 2 or more severe gastrointestinal toxic effects ( 36 [ 8% ] of 430 patients vs 65 [ 16% ] of 415 patients ; difference 73 percentage points , 95% ci 29117 ; p = 00011 ) , corroborated by worst ctcae grade 2 or more severe gastrointestinal toxic effects exceeding baseline ( 34 [ 8% ] of 427 patients vs 63 [ 15% ] of 413 patients ; difference 73 percentage points , 95% ci 30116 ; p = 000095 ; appendix p 22 )  . 
we observed no other significant differences in ctcae gastrointestinal secondary endpoints for conventionally fractionated or moderately hypo frac tionated radio therapy compared with stereotactic body radiotherapy ( appendix p 22 ) , including worst ctcae 1538 vol 20 november 2019 articles gastrointestinal grade 3 or more severe toxic effects [ 1% ] of 430 patients in the conventionally ( three fractionated or moderately hypofractionated radiotherapy vs three [ 1% ] of 415 patients in the stereotactic body radiotherapy group )  . 
we observed no significant differences in ctcae genitourinary secondary endpoints between the conven tionally fractionated or moderately hypofractionated radiotherapy and stereotactic body radiotherapy groups ( appendix p 23 ) , including worst ctcae genitourinary grade 3 or more severe toxic effects ( three [ 1% ] of 430 patients vs seven [ 2% ] of 415 patients )  . 
 further tables broken down into individual ctcae toxicity for gastrointestinal and genitourinary systems , are presented in the appendix ( pp 2439 ) and show baseline ctcae toxicity , worst acute ctcae toxicity , worst ( exceeding baseline ) acute ctcae toxicity , and week 12 ctcae toxicity . items , separately epic - 26 mean changes in subdomain scores over time were similar , both for change from baseline ( figure 4 ) and absolute scores ( appendix p 40 )  . 
comparison over each of the five epic - 26 subdomains and overall urinary bother for scores at baseline , worst , worst minus baseline , and week 12 after radiotherapy showed no significant differences between the trial groups ( appendix p 41 )  . 
we observed no significant difference between the study groups in the proportion of patients with a clinically significant reduction from baseline for any epic - 26 subdomain score area , neither assessed at any time ( appendix p 42 ) nor at week - 12 only ( appendix p 43 )  . ipss subscores , total score , and quality of life over time were similar between the study groups , both for change from baseline ( appendix p 44 ) and absolute scores ( appendix p 45 )  . 
we observed no significant differences between treatment groups for median scores of worst ipss total , week - 12 ipss total , worst ipss quality of life , or week - 12 ipss quality of life ( appendix p 46 )  . 
ipss severity categories ( none , mild , moderate , or severe ) over time were similar between the treatment groups ( appendix p 47 ) , with no significant differences in ipss total score categories at baseline , worst , and week - 12 after radiotherapy ( appendix p 48 )  . for iief - 5 , we observed no significant differences between conventionally fractionated or moder ately hypofractionated radiotherapy and stereo tactic body radiotherapy at baseline or at week 12 after radiotherapy ( appendix p 49 )  . 
numbers at risk for each arm are asynchronous because they are shown only at data collection timepoints ( which are non - simultaneous relative to the start of radiotherapy )  . 
 for patients in the stereotactic body radiotherapy group , worst rtog grade 2 or more severe genitourinary ( without reference to baseline ) toxic effects for noncyberknife ( 75 [ 31% ] of 245 patients ) versus cyberknife ( 21 [ 12% ] of 170 patients ) delivery were significantly different ( difference 183 percentage points , 95% ci 107 to 259 ; p < 00001 ) , consistent with observations over time ( appendix p 54 )  . 
the time period between baseline scoring and week 4 after radiotherapy follow - up is variable , since the total time of radiotherapy delivery varied ( sbrt in 1 or 2 weeks ; cfmhrt in 4 or 78 weeks )  . 
for patients in the conventionally fractionated or moder ately hypo fractionated radiotherapy group , worst rtog gastro intestinal grade 2 or more severe ( without reference to baseline ) toxic effects in non - cyberknifeusing centres ( 25 [ 10% ] of 252 patients ) versus cyberknife centres ( 28 [ 16% ] of 180 patients ) were not different ( difference 56 percentage points , 95% ci 08 to 121 ; p = 0078 ) , consistent with grade 2 and grade 3 observations over time ( appendix p 55 )  . 
for patients in the conventionally fractionated or moderately hypofractionated radiotherapy group , worst rtog grade 2 or more severe genitourinary ( without reference to baseline ) toxic effects in non - cyberknife - using centres ( 73 [ 29% ] of 252 patients ) versus cyberknife - using centres ( 45 [ 25% ] of 180 patients ) were not significantly different ( difference 40 percentage points , 95% ci 124 to 45 ; p = 0361 ) , contrary to possible graphical interpretation over time ( appendix p 56 )  . discussion this pre - planned analysis of acute toxicity in the pace - b trial , occurring up to 12 weeks after radiotherapy delivery completion , does not suggest that patients have greater acute rtog toxic effects with stereotactic body radiotherapy compared with conventionally fractionated or moderately hypo fractionated radiotherapy . 
of the secondary endpoints examined , only worst ctcae grade 2 or more severe composite toxic effects ( both with and without reference to baseline ) showed significantly higher proportions of patients with toxic effects when treated with stereotactic body radiotherapy compared with conventionally fractionated or moderately hypofractionated radiotherapy . 
overall , our results do not provide consistent evidence of higher acute toxicity with stereotactic body radiotherapy compared with conven tionally fractionated or moderately hypofractionated radiotherapy . it is notable that the control group in our trial fractionated or moderately hypo ( conventionally fractionated radiotherapy ) had lower acute toxicity than in the preceding chhip trial , 11 with toxicity more comparable to the profit trial ( appendix p 57 ) .14 although image - guided radiotherapy was mandatory in both the pace and profit14 trials , it was only used in 30% of chhip participants , which could have caused this difference . 
the chhip trial used androgen deprivation therapy for most patients , which was not permitted in pace or profit ; however , androgen deprivation therapy is not known to alter acute toxicity . 
conceivably , the cumulative proportion of higher worst rtog grade 2 or more severe events in chhip and profit versus pace - b might result from recall selection bias due to more frequent sampling in profit and chhip . the most similar phase 3 randomised controlled trial to pace - b is the scandinavian hypo - rt - pc trial , which randomly assigned ( 1 : 1 ) intermediate - risk and high - risk patients with prostate cancer to 78 gy in 39 fractions over 78 weeks or 427 gy in seven fractions over 25 weeks , therapy.19 important without androgen deprivation differences between pace - b and hypo - rt - pc are as follows : hypo - rt - pc recruited 11% high - risk patients and 89% intermediate - risk patients ( vs 8% low - risk patients and 92% intermediate - risk patients in pace - b ) , treated a ctv of prostate only , and mostly ( 80% ) used three - dimensional ( 3d ) conformal radiotherapy . 
the control groups differ between hypo - rt - pc ( all 78 gy in 39 fractions ) and pace - b ( 70% receiving 62 gy in 20 fractions )  . 
this difference is important given the higher acute gastrointestinal toxicity observed for moderate hypo fractionation in the chhip trial.11 hypo - rt - pc made only a single end - of - treatment toxicity assessment during the acute toxicity window , and reported significantly higher rtog genitourinary and patient - reported outcome acute toxic effects with ultra - hypofractionation . 
comparison of rtog toxicity for pace - b with hypo - rt - pc ( estimates approximated from graphs in paper19 ) produces similar results , although reported grade 3 to grade 4 toxicity for hypo - rt - pc is higher than most reports of ultrahypofractionation ( appendix p 58 )  . 
although measured on different patient - reported outcome scales hypo - rt - pc , our results do not suggest a difference in patient - reported outcome acute side - effects . we identified no up to date systematic literature review of acute toxicity in this setting . 
therefore , we prospectively collated acute toxicity data from smaller studies of stereotactic body radiotherapy in low - risk and intermediate - risk prostate cancer ( appendix p 58 )  . 
for example , a multicentre phase 2 study of 309 men25 recorded cumulative acute toxicity of ctcae gastrointestinal grade 2 or worse of 12% and ctcae genitourinary grade 2 or worse of 26% , similar to the 157% and 308% , respectively , for patients the stereotactic body radiotherapy group in pace - b . strengths of these data relate predominantly to trial design . 
this is a large phase 3 randomised , controlled trial , and represents , to our knowledge , the first published phase 3 acute toxicity data on five - fraction stereotactic body radiotherapy compared with standard fractionation . 
the protocol amendment relating to treatment in the control group strengthened the trial by allowing most patients in that group to receive moderate hypofractionation at 62 gy in 20 fractions , close to the 60 gy in 20 fractions regimen shown to be effective in chhip11 and profit.14 the pace - b acute toxicity sampling frequency exceeded hypo - rt - pc ( assessed only at end of radiotherapy and 6 months )  . 
combined with the high proportions of assessment forms returned , this is a major strength given the dynamic nature of acute toxicity . limitations arise from the external applicability of the patients recruited to pace - b . 
we also note the higher fiducial marker use for image - guided radio therapy in patients undergoing stereo tactic body radiotherapy compared with conventionally fractionated or moderately hypo fractionated radiotherapy in pace - b . 
furthermore , the multiple radiotherapy schedule dura tions meant that some undesirable vol 20 november 2019 1541 articles interpolation was needed to present two arm graphs ( rtog and ctcae )  . 
this fact also means that the follow up of 12 weeks after radiotherapy refers to quite different period of time for someone receiving 1 week of stereotactic body radiotherapy ( ie , 13 weeks from the start of radiotherapy ) versus 78 weeks of conventional fractionation ( ie , 198 weeks after commencing treatment )  . 
future trials should consider a follow - up schedule fixed by radiotherapy start date rather than end date . stereotactic body radiotherapy is already the standard of care in some centres and is an option for men with low and favourable intermediate - risk prostate cancer in the nccn guidelines.28 the hypo - rt - pc trial suggested similar oncological outcomes with ultra - hypofractionation.19 this result was attenuated by increased acute toxicity in the study , notably higher grade 3 or worse toxic effects than other reports of stereotactic body radiotherapy , which might potentially be driven by the 3d conformal radiotherapy technique predominantly used in the hypo - rt - pc study . 
other earlier phase studies , most of which used the same 3625 gy dose as pace ( appendix p 58 ) , suggest good oncological outcomes and low late toxicity with stereotactic body radiotherapy , but the mature results of pace - b are required before definite oncological outcome statements can be made . the method of stereotactic body radiotherapy delivery for example , cyberknife versus non - cyberknifemight influence acute toxicity , a prespecified area of interest after the introduction of conventional linear accelerator stereotactic body radiotherapy . 
there are many reasons why there might be a systematic difference between cyberknife and non - cyberknife stereotactic body radiotherapy outcomes , including variations in dosimetry , image guidance , and treatment times ( typically 45 min for cyberknife and < 5 min for conventional linear accelerators )  . 
our post - hoc analysis of the same primary endpoint rtog metrics shows similar grade 2 or worse gastrointestinal toxic effects , but less grade 2 or worse genitourinary toxic effects with cyberknife . 
we compared conventionally fractionated or moderately hypofractionated radiotherapy toxic effects between centres using cyberknife versus those not using cyberknife and found no significant difference for either worst rtog grade 2 or more severe gastrointestinal or genitourinary toxic effects . 
we caution that this result is hypothesisgenerating and intend to explore further in multivariate analyses once digital imaging and communications in medicine data have been centralised for all patients . to our knowledge , we present the first published prospective phase 3 acute toxicity results for random assignment of patients between five - fraction stereotactic body radiotherapy and either conventional or moderately hypofractionated radiotherapy . 
the absence of increased toxicity in the stereotactic body radiotherapy group is reassuring given the higher acute toxicity suggested in the only previously published phase 3 ultra - hypofractionation trial , 19 especially given the more abbreviated ( five - fraction ) investigational radiotherapy protocol used in pace - b . 
 all authors provided critical academic review of content for the manuscript and gave final approval for submission of the work to the journal . declaration of interests dhb reports a phd studentship award from cancer research uk , during the conduct of the study . 
act reports grants from accuray , during the conduct of the study , grants and personal fees from elekta , grants from merck sharpe & dohme , and personal fees from janssen , astellas , and ferring , outside the submitted work . 
eh reports grants from accuray and cancer research uk , during the conduct of the study , grants and non - financial support from merck sharp & dohme , astra zeneca , and bayer , and grants from janssen - cilag , kyowa hakko uk , alliance pharma ( previously cambridge laboratories ) , and aventis pharma limited ( sanofi ) , outside the submitted work . 
 all other authors declare no competing interests . data sharing the institute of cancer research clinical trials and statistics unit ( icr - ctsu ) supports the wider dissemination of information from the research it conducts and increased cooperation between investigators . 
 trial data is collected , managed , stored , shared , and archived according to icr - ctsu standard operating procedures to ensure the enduring quality , integrity , and utility of the data . 
data recipients are required to enter a formal data sharing agreement , which describes the conditions for release and requirements for data transfer , storage , archiving , publication , and intellectual property . 
data sharing is undertaken if proposed projects have a sound 1542 vol 20 november 2019 articles scientific or patient benefit rationale as agreed by the tmg and approved by the independent data monitoring and steering committee as required . 
additionally , all indirect identifiers that might lead to deductive disclosures will be removed in line with cancer research uk data sharing guidelines . acknowledgments the pace - b study is funded by accuray . 
funding for delegated tasks outside the uk was as follows : in ireland the study was coordinated by the irish clinical oncology research group clg trading as cancer trials ireland and in canada the study was supported by the prostate cure foundation . 
the icr - ctsu receives programme grant funding from cancer research uk ( c1491 / a15955 ) , which supported in part this endorsed study ( cruke / 12 / 025 )  . 
we also thank the independent data monitoring committee and trial steering committee . editorial for more on the genome - wide association report see n engl j med 2012 ; 366 : 88391 for more on the pi3k inhibitor comment see j clin oncol 2012 ; 30 : 76566 biology - driven medicine : tissue matters cancer therapy has been revolutionised by the advent of targeted agents . 
as a result , patient selection through genetic testing is a rapidly growing industry , but this has posed extra challenges for the patient and oncological team including cost , legal obstacles , test accuracy , and management of tissue . 
the report showed that up to two - thirds of genetic results in renal - cell carcinoma will vary throughout the tumour specimen when tissue is assessed in a multiregional sequencing analysis . 
so what are the consequences of this nding for the use of single biopsies to guide treatments in the clinic ? one of the rst targeted drugs to show e cacy was imatinib for patients with chronic myeloid leukaemia . 
without selection , a dilution of the therapeutic e ect occurs where a new treatment might be abandoned because patients without the target , and who do not respond , mask the activity in those that do . 
 the reverse situation , testing to exclude patients from treatment , can also applyeg , patients with colorectal cancer and kras mutations in exons 12 and 13 do poorly with egfr inhibitors . with the growing complexity of tests , targets , and treatment pathways , obtaining tissue su cient to meet therapeutic needs has become ever more important . 
tissue might need to be sampled at di erent times , as therapeutic targets can change over time , and samples must also be of appropriate quality and representative of the tumour as a whole . 
although intra - tumoral heterogeneity has long been appreciated , the nejm report is alarming because it suggests that heterogeneity could seriously hamper accurate patient selection , and not just the therapeutic ratioas a result , patients could be inappropriately treated with expensive drugs they are unlikely to respond to , or be omitted from active treatment . 
selection is therefore vital to avoid dilution of e cacy and reduce patient har furthermore , according to speakers at the 13th european congress on perspectives in lung cancer held in amsterdam , netherlands , on march 910 , 2012 , the role of the pathologist is paramount in ensuring not only that enough tissue is left after histological diagnosis to do essential testssuch as those to predict bene t from the egfr inhibitorsbut also that testing is not done until the evidence linking the target to the e cacy of the drug , and any potential future treatments , are considered . 
a multidisciplinary environment is therefore essential to ensure an appropriate discussion of the timing of any pathological testing , and , where possible , to enable tissue to be saved to help guide future decisionmaking . 
this point was a rmed in a recent comment in the journal of clinical oncology in which the authors suggested that excluding patients without the proposed target for treatment of breast and gynaecological cancer with pi3k / mtor inhibitors should not be done until a stronger predictive relationship emerges . 
use of blood might help overcome some of the di culties associated with tissue resources , and several studies have been done using serum samples to de ne predictors of response to treatment , but these investigations are fraught with di culties , including linking any serum changes to the tumour itself . deciding who to test , how , and when , will help realise the vast potential of personalised medicine for cancer . 
 however , integration of biology - driven therapy into the clinic is becoming increasingly complex and intratumoral heterogeneity could prove to be the achilles heel of targeted therapy in an era in which tissue has become an extremely precious resource that must be used sparingly , pragmatically , and within a multidisciplinary decisionmaking tea the lancet oncology vol 13 april 2012 editorial evolution : the lancet oncologyan online - enhanced journal long - standing readers of the lancet oncology will have noticed changes in the journal over the years . 
as a result , we strongly encourage print readers to activate their online accounts , and for all our online - only subscribers to check the website regularly for new content . why are we doing this ? since 2005 , the lancet oncology has seen a 70% increase in the number of articles submitted from the united states , europe , and asia . 
furthermore , because cancer is fast becoming the number one cause of death in many countries , there is an ever - pressing demand for more information and rapid dissemination of ndings . 
having an online focus will also better align the journal with the majority of our readers main way of accessing content . what will change ? editorials , comment , cancer and society , and articles will continue in print and online . 
 correspondence , reviews , historical reviews , personal views , and health - care development articles will become online - only content , but the quantity will increase from the monthly current average of two to three , to four to ve . 
finally , podcasts will feature interviews with authors and will be published on the same day as the corresponding article . we hope you share our enthusiasm for the new feel of the journal and we look forward to bringing you even more of the high - quality material youve come to expect of the lancet oncology in the months and years ahead . 
 the lancet oncology budget cuts in the usa : a short - term win ? on nov 18 , 2011 , president barack obama signed a bill into law that will a ect the funding for several science agencies . 
the white house o ce of science and technology policy , which advices the executive o ce about the e ects of science and technology on domestic and international a airs , has had its funding cut by more than 30% , leaving just $45 million . 
the usas budget cuts to quell the national de cit of $12 trillion by 2021 mean that several key agencies such as the national institutes of health ( nih ) and national science foundation had below - in ation increases to their funding . 
such reductions in funding might not bode well for federally funded organisationsincluding the nih and centers for disease control and prevention ( cdc ) that fund much of the cancer research in the usa . the budget cuts also extend to preventive measures , which are needed in addition to funding for research into the causes of and treatments for cancers . 
the cdc has recommended a total of $37 billion in funding for tobacco prevention programmes , but collectively individual states have only budgeted $4567 million ( 12% ) of this amount . if the usa is to remain a world leader in terms of research , any budget cuts to cancer research and prevention programmes need to be implemented judiciously because although the short - term win of saving a few dollars will look good on a budget sheet , it will not translate into medium - term and long - term solutions of stopping the rising burden of cancer . 
the usa need only look at ireland , which even in austere times , is providing improved care for patients as a result of a reorganisation of its health structures into specialist centres . 
 the lancet oncology see news page 17 for more on cuts to tobacco prevention funding see releases / post / 2011_11_30_ state_report for more on the white house o ce of science and technology policy budget cut see chemistryworld / news / 2011 / november / 21111101.asp for more on the usas budget cuts see com / news / what - does - the - usbudget - stalemate - mean - forresearch - 1.9475 for more on the rising burden of cancer see the lancet oncology commission thelancet.com / commission / delivering - a ordable - cancercare - in - high - income - countries vol 13 january 2012 re ection and reaction richard g grundy childrens brain tumour research centre , university of nottingham , the medical school , queens medical centre , nottingham ng7 2uh , uk richard.grundy@nottingham.ac.uk the author declared no con icts of interest . grundy rg , wilne sa , weston cl , et al . 
pediatr neurosurg 1998 ; 28 : 21522 . bou et e , perilongo g , canete a , massimino m et al intracranial ependymoma in children ; a critical review of prognostic markers and a plea for cooperation . 
med pediatr oncol 1998 ; 40 : 3440 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zupancic m , shah pc , shah - khan f , nagendra s . 
in this review , the author list should have read : melanie zupancic , prabodh c shah , farheen shah - khan , sanjai nagendra . grundy rg , wilne sa , weston cl , et al . 
 full total resection less than full total resection 100 075 050 025 000 numbers at risk total resection 44 partial resection 45 time from surgery ( years ) 7 figure 5 : overall survival based on neurosurgical assessment of the extent of resection at the end of surgery vol 8 september 2007 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology chosen as one of the endpoints.2 patients recruited in this trial were offered radiofrequency ablation , because they were considered by the treating physician to be unsuitable for surgery and unfit for radiotherapy or chemotherapy as a result of either underlying chronic obstructive pulmonary disease or major associated comorbidities . 
because the patients had small , asymptomatic pulmonary tumours , no improvement in quality of life was noted after treatment with radiofrequency ablation , despite the high number of complete responses . 
nevertheless , we think that the absence of any significant worsening in short form ( sf ) - 12 ( physical and mental summary ) scores and functional assessment of cancer therapylung ( fact - l ; lung - cancer scale and trial outcome index ) scores provides evidence that the minimallyinvasive treatment approach used in these patients did preserve their quality of life . 
the number at risk for part b of gures 3 and 4 of this article should have been interventional group ( top ) and control group ( bottom )  . 
also , the second sentence in the discussion should have read , however , preoperative chemoradiotherapy in patients undergoing surgery signi cantly increased the proportion of those with complete resection ; and in those with complete resection , preoperative chemoradiotherapy increased the proportion of patients with mediastinal downstaging and histopathological response . bo etta p , hecht s , gray n , gupta p , straif k . 
during the immediate months preceding submission of the review sh was acting in the capacity of an expert witness for the plainti in a future court case against a smokeless tobacco company . 
sh declares his participation in this case in no way in uenced his writing or involvement in the review . bonnefoi h , potti a , delorenzi m , et al . 
in the webpanel of this article , the headings for docetaxel should have been resistant cell lines ( rst ) and sensitive cell lines ( second )  . 822 vol 9 september 2008 reflection & reaction graham j caine and gregory yh lip haemostasis , thrombosis , and vascular biology unit , university department of medicine , city hospital , birmingham b18 7qh , uk . 1 nash gf , turner lf , scully mf , kakkar ak . 
incidence of cancer after prophylaxis with warfarin against recurrent venous thromboembolisn engl j med 2000 ; 342 : 195358 . 5 smorenburg sm , vink r , otten h - m , et al . the effects of vitamin k - antagonists on survival of patients with malignancy : a systematic analysis . 
clin exp metastasis 1991 ; 9 : 311 . 8 maurer lh , herndon je , hollis dr , et al . randomized trial of chemotherapy and radiation therapy with or without warfarin for limited - stage small - cell lung cancer : a cancer and leukaemia group b study . 
lancet 1994 ; 343 : 88689 . 10 chahinian ap , propert kj , ware jh , et al . a randomized trial of anticoagulation with warfarin and of alternating chemotherapy in extensive small - cell lung cancer by the cancer and leukaemia group b . 
in addition , the symptom duration for class iv should have read ( cid : 2 ) 3 months and the total radiation dose for class vi should have read ( cid : 2 ) 544 gy . 
only reproduce with permission from the lancet publishing group . correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2019 ; 20 : 137085 correction to lancet oncol 2020 ; 21 : 137886 glynne - jones r , sebag - montefiore d , meadows hm , et al . 
lancet oncol 2017 ; 18 : 34756the last clause of the last sentence of the first paragraph of the introduction of this article should have read or by giving maintenance chemotherapy after chemoradiotherapy.7 this correction has been made to the online version as of nov 2 , 2020 . motzer rj , rini bi , mcdermott df , et al , on behalf of the checkmate 214 investigators . 
nivolumab plus ipilimumab versus sunitinib in firstline treatment for advanced renal cell carcinoma : extended follow - up of efficacy and safety results from a randomised , controlled , phase 3 trial . 
 lancet oncol 2019 ; 20 : 137085 in this article , supplementary table 1 in the appendix has been updated to correct international metastatic renal cell carcinoma database consortium risk percentage values in patients in the intention to treat group . 
lancet oncol 2020 ; 21 : 137886in table 2 of this article , the reference value for absolute risk reduction of incident gastric cancer over 10 years in indi viduals with an unfavourable life style should have been 0 for low genetic risk , intermediate genetic risk , and high genetic risk . 
these corrections have been made to the online version as of nov 2 , 2020 . vol 21 november 2020 e518 corrections articles lancet oncol 2015 ; 16 : 106170 published online august 5 , 2015 s1470 - 2045 ( 15 ) 00212 - 0 see comment page 1004 * collaborators listed in appendix p 3 correspondence to : secretariat , cancer epidemiology unit , richard doll building , oxford ox3 7lf , uk collaborations@ceu.ox.ac.uk see online for appendix endometrial cancer and oral contraceptives : an individual participant meta - analysis of 27 276 women with endometrial cancer from 36 epidemiological studies collaborative group on epidemiological studies on endometrial cancer * summary background oral contraceptives are known to reduce the incidence rate of endometrial cancer , but it is uncertain how long this e ect lasts after use ceases , or whether it is modi ed by other factors . methods individual participant datasets were sought from principal investigators and provided centrally for 27 276 women with endometrial cancer ( cases ) and 115 743 without endometrial cancer ( controls ) from 36 epidemiological studies . 
the relative risks ( rrs ) of endometrial cancer associated with oral contraceptive use were estimated using logistic regression , strati ed by study , age , parity , body - mass index , smoking , and use of menopausal hormone therapy . findings the median age of cases was 63 years ( iqr 5768 ) and the median year of cancer diagnosis was 2001 ( iqr 19942005 )  . 
9459 ( 35% ) of 27 276 cases and 45 625 ( 39% ) of 115 743 controls had ever used oral contraceptives , for median durations of 30 years ( iqr 17 ) and 44 years ( iqr 29 ) , respectively . 
the longer that women had used oral contraceptives , the greater the reduction in risk of endometrial cancer ; every 5 years of use was associated with a risk ratio of 076 ( 95% ci 073078 ; p < 00001 )  . 
this reduction in risk persisted for more than 30 years after oral contraceptive use had ceased , with no apparent decrease between the rrs for use during the 1960s , 1970s , and 1980s , despite higher oestrogen doses in pills used in the early years . 
however , the reduction in risk associated with ever having used oral contraceptives di ered by tumour type , being stronger for carcinomas ( rr 069 , 95% ci 066071 ) than sarcomas ( 083 , 067104 ; case - case comparison : p = 002 )  . 
in high - income countries , 10 years use of oral contraceptives was estimated to reduce the absolute risk of endometrial cancer arising before age 75 years from 23 to 13 per 100 women . interpretation use of oral contraceptives confers long - term protection against endometrial cancer . 
these results suggest that , in developed countries , about 400 000 cases of endometrial cancer before the age of 75 years have been prevented over the past 50 years ( 19652014 ) by oral contraceptives , including 200 000 in the past decade ( 200514 )  . funding medical research council , cancer research uk . introduction use of oral contraceptives is known to reduce the incidence of endometrial cancer.1 because endometrial cancer is uncommon in young women but its incidence increases sharply with age , the public health e ects of this inverse association depend mainly on the extent to which the reduced risk of endometrial cancer persists long after use ceases . 
to investigate the association between use of oral contraceptives and the subsequent risk of endometrial cancer , individual participant data from 36 epidemiological studies of endometrial cancer have been brought together and analysed centrally . methods identi cation of studies and collection of data this collaboration was established in 2005 . 
since 2012 , epidemio logical studies were eligible for inclusion if they collected individual data about use of hormonal con traceptives and reproductive history from at least 400 women with endometrial cancer in retrospective studies , and at least 200 women in prospective studies . 
eligible studies were identi ed from review articles , computer - aided literature searches in pubmed and medline ( up to jan 31 , 2012 ) , using combinations of the search terms endometrial cancer risk , endometrium cancer risk , hormon * , oral contraceptive , and oc , plus the additional terms cohort , prospective , women , and cancer risk , and from discussions with colleagues . 
e orts were made to identify all studies that included relevant information , irrespective of whether or not results about oral contraceptives had been published , and principal investigators from each eligible study were invited to participate . cases were de ned as women with invasive cancer of any histological type of the body of the uterus who were without previous cancer ( except non - melanoma skin cancer ) ; controls were women without previous cancer who had an intact uterus . 
prospective studies were incorporated by a nested case - control design , in which up to four controls were selected at random from cohort vol 16 september 2015 1061 articles investigators members , matched for exact year of birth , date of recruitment ( within 6 months ) , duration of follow - up ( at disease onset ) , and , when appropriate , other matching criteria used by ( eg , the principal geographical region )  . 
individual participant data on sociodemographic and repro ductive factors , use of contraceptives , use of hormonal therapies for the menopause , reproductive history , height , weight , consumption of alcohol and tobacco , and family history of breast and endometrial cancer were sought from the principal investi gators of every study . 
for prospective studies , reported information on the use of oral contraceptives was taken from the last record before disease onset , to calculate duration of use and time since last use ( assuming no further use )  . 
 apparent inconsistencies in the data were discussed with the study investigators and if they could not be recti ed , decisions were made about which values to incorporate into the pooled dataset . 
after the records had been checked and corrected , investigators were sent summary analyses of the variables to be used for nal con rmation that their data had been interpreted correctly . 44 eligible studies were identi ed245 of which 36 are included in the current analysis.237 four groups of researchers declined to participate in this collaboration3841 and a further four groups agreed in principle to provide data at a future date.4245 principal individual investigators provided information about whether or not women had ever used hormonal contraceptives ( as de ned by each study ) and most also provided information about the total duration of use and age or calendar year at rst and last use . 
only 13 studies collected information on the type of hormonal contraceptives ; 7 , 17 , 19 , 21 , 2530 , 33 , 35 , 36 women from the remaining 23 studies were assumed to be using combined oral contraceptives ( ie , those containing both oestrogen and progestin ) because more than 95% of hormonal contraceptive users included in studies with such information reported using combined preparations . 
 there were too few women with endometrial cancer exclusively progestin - only oral who had used contraceptives ( 56 cases ) , progestin - only injectable hormonal contraceptives ( 19 cases ) , combined injectable hormonal contraceptives ( three cases ) or sequential oral contraceptives ( 41 cases ) for reliable analysis . statistical analysis statistical analyses were done with stata version 13.0. 
when several groups were compared , with one taken as the reference group with an rr of 1 , the variance of the log risk in the reference group and in each of the other groups was calculated from the variances and covariances of the log rrs in those other groups.47 these group - speci c variances yield the groupspeci c cis for each group ( including the reference group ) that are plotted in the gures . all analyses were strati ed by study , centre ( for multicentre studies ) , age group ( 1619 , 2024 years , and so on up to 7579 , 8084 , and 8589 years ) , parity ( 0 , 1 , 2 , 3 , 4 , 5 , or not known ) , body - mass index ( bmi < 25 , 2530 , 30 kg / m , or not known ) , smoking ( never , ever , or unknown ) and type of menopausal hormone therapy used ( never , oestrogen - only exclusively , combined exclusively , both oestrogen - only and combined , other types , or unknown use )  . 
the e ect on the main ndings of further strati cation by ethnic origin , education , age at rst birth , age at last birth , age at menarche , age at menopause , menopausal status , and family history of endometrial cancer was examined by comparing results before and after strati cation for each variable separately . 
 women with missing information for any of these adjustment factors were assigned to a separate stratum for the relevant variable to conserve total numbers analysed ; sensitivity analyses excluded these women . the rr of endometrial cancer per 5 - year duration of oral contraceptive use was estimated by tting a loglinear trend across categories of duration ( never , < 1 , 1 < 5 , 5 < 10 , 10 < 15 , and 15 years ) , using the median value within each category . the association of endometrial cancer risk and duration of oral contraceptive use was cross - classi ed by time since last use and by mid - calendar - year of use ( grouped as 196069 , 197079 , and 198089 ) to assess the independent e ect , if any , of these factors on risk . 
 although the composition of oral contraceptive pills has varied substantially over time , a strong association exists between calendar year of use and oestrogen dose in the oral contraceptives typically used.4850 in the usa and uk , for example , the oral contraceptives prescribed before 1970 were typically high - dose preparations , often containing 100 g or more of oestrogen ; between 1970 and 1980 prescriptions were typically for medium - dose preparations containing about 50 g of oestrogen ; and by 1980 most prescriptions were for low - dose preparations , containing 35 g or less of oestrogen.49 , 50 thus , in these analyses , decade of use was taken as a correlate of oestrogen dose of oral contraceptives . the classi cation system adopted in each study was used centrally to categorise tumours into three broad histological subtypes : type i ( endometrioid carcinomas ) ; type ii ( non - endometrioid carcinomas ) ; and uterine sarcomas . 
 uterine sarcomas were de ned as sarcoma , not otherwise speci ed ( 88008806 ) , brosarcoma ( 88108833 ) , liposarcoma ( 88508858 ) , myosarcoma ( 88908896 ) , rhabdomyosarcoma ( 89008902 , 89108912 ) , endometrial stromal sarcoma ( 89308931 ) , or cancer coded as sarcoma by study investigators . 
signi cance tests for heterogeneity of the relative risks for oral contraceptive use by tumour subtype compared cases only ( case - case comparisons ) , because controls provide no additional information . 
hence , although they were still strati ed by study ( centre ) and age , to retain su cient statistical information within each stratum they were adjusted rather than strati ed for parity , bmi , smoking , and type of menopausal hormone therapy used . when results are presented in the form of plots , rrs are represented by squares and their corresponding cis or group - speci c cis by horizontal lines . 
the position of the square indicates the point estimate of the rr , and the area of the square is inversely proportional to the variance of the logarithm of the rr ( or , for multigroup analyses , log risk ) , thus providing an indication of the amount of statistical information available for that particular estimate . 
because of the large number of rr estimates presented , 99% cis are generally used in the gures ; however , throughout the text 95% cis are quoted . cumulative incidence rates of endometrial cancer ( up to the age of 75 years ) associated with di erent durations of use of oral contraceptives were estimated by application of rr estimates for endometrial cancer from the present analyses to age - speci c incidence rates for women in 21 high - income countries in western europe , north america , and australasia ( appendix p 8 ) .52 absolute numbers of cancers prevented were estimated from birth cohort - speci c prevalences of oral contraceptive use.53 role of the funding source the funders of the study had no role in the study design , data collection , data analysis , data interpretation , writing of the report , or the decision to submit for publication . 
 the writing committee had full access to all the data , could request any analyses , and had nal responsibility for the decision to submit for publication . results table 1 presents the details of the 36 participating studies . 
the median year of cancer diagnosis was 2001 ( iqr 19942005 ) and the median age at diagnosis was 63 years ( iqr 5768 ) , with 847 ( 3% ) of women diagnosed before 45 years of age , 3743 ( 14% ) at 4554 years , 11 287 ( 41% ) at 5564 years , and 11 399 ( 42% ) at 65 years or older . overall , 9459 ( 35% ) of 27 276 women with endometrial cancer and 45 625 ( 39% ) of 115 743 controls had ever used oral contraceptives , with a median duration of use of 30 years ( iqr 17 ) and 44 years ( 29 ) , respectively . 
the prevalence of ever having used oral contraceptives was substantially lower in controls from asia ( 899 / 11 180 ; 8% ) than in controls from europe and north america ( 39 050 / 86 293 ; 45% )  . figure 1 shows the study - speci c and combined relative risks of endometrial cancer in ever - users compared with never - users of oral contraceptives and , in the ever - users , the rr per 5 years of use . 
studies with a low information content ( de ned as 1 / var [ ln rr ] < 20 ) are included in the other category for each relevant study design . 
overall , the risk of endometrial cancer was signi cantly lower in women who had ever used oral contraceptives than in women who had never used them ( rr 069 , 95% ci 067072 ) , with no signi cant heterogeneity between the three types of study design ( heterogeneity test ; p = 015 )  . duration of use of oral contraceptives ( years ) years of use cases / controls rr ( 99% gsci ) 1595 / 6428 097 ( 088107 ) 1 < 5 3624 / 15 938 081 ( 076086 ) 5 < 10 2096 / 11 070 064 ( 059069 ) 10 < 15 1136 / 6927 052 ( 047058 ) 422 / 3420 032 ( 028038 ) never - users 30 years since last use 1529 years since last use < 15 years since last use duration of use of oral contraceptives ( years ) figure 2 : relative risk of endometrial cancer in users of oral contraceptives compared with never - users , by ( a ) duration of use , and ( b ) duration of use and time since last use of oral contraceptives gsci = group - speci c ci . 
never users in studies with data on time since last use include 15 169 cases and 55 965 controls with relative risk of 100 ( 99% gsci 096104 )  . 
 the longer women had used oral contraceptives for , the lower their risk of endometrial cancer was , with each 5 years of use associated with an rr of 076 ( 95% ci 073078 , p < 00001 ) , based on 8873 cases and 43 783 controls who were ever - users ( gure 1 )  . 
the proportional reduction in risk of endometrial cancer per 5 years of oral contraceptive use varied slightly by age at diagnosis ( heterogeneity test ; p = 0004 ) , with rr 071 ( 95% ci 067075 ) for women diagnosed before 60 years of age and rr 079 ( 075082 ) for women diagnosed at 60 years of age or older . 
the association did not vary by bmi , parity , use of menopausal hormone therapy , menopausal status , smoking status , age at menarche , ethnic origin , or alcohol use ( gure 3 )  . 
the exclusion of women with missing values for any of these strati cation variables also made a negligible di erence to the risk estimates ( making the fully strati ed rr per 5 years use of oral contraceptives 075 , 95% ci 072077 )  . ( median most women with endometrial cancer had stopped using oral contraceptives many years before their cancer diagnosis last use 29 years time since [ iqr 2234 ] )  . 
women who had used oral contraceptives more recently had also , on average , used them for a longer duration ( eg , women who had used oral contraceptives less than 15 years previously had a median duration of use of 47 years [ iqr 1399 ] , whereas women who had last used oral contraceptives 30 years or more previously had a median duration of use of 30 years [ 1053 ] )  . 
for a given duration of use , the reduction in risk was slightly greater in women with more recent use , although a signi cant protective e ect remained more than 30 years after use had ceased ( gure 2b and appendix p 5 )  . in 7452 women with endometrial cancer for whom information about the timing of their oral contraceptive use was available , 3235 ( 43% ) had a mid - year of oral contraceptive use in the 1960s and 371 ( 5% ) had a midyear of use in the 1980s ( appendix p 6 )  . 
the rrs per 5 years duration of use of oral contraceptives in the 1960s , 1970s , and 1980s did not vary signi cantly ( heterogeneity test ; p = 015 , appendix p 6 )  . 
there was also no signi cant heterogeneity in the rr per 5 years of use by age at rst use or age at last use ( appendix p 7 )  . however , there was some evidence that the rr depended on the histological subtype of endometrial cancer ( table 2 )  . 
compared with women who had never used oral contraceptives , ever - users had an rr of 069 ( 95% ci 066071 ) for carcinomas , based on 26 877 cases , which was similar for type i and type ii carcinomas . 
 few cases , ever - use of oral based on relatively contraceptives was not signi cantly associated with the risk of uterine sarcoma ( rr 083 [ 95% ci 067104 ] , based on 399 cases ; heterogeneity , from direct case - case comparison of sarcomas vs carcinomas p = 002 )  . 
analyses were also done in women with information about 50 g per week 1 = 0005 , p = 094 figure 3 : relative risk of endometrial cancer per 5 years use of oral contraceptives , by various lifestyle and reproductive characteristics rr = relative risk . 
 * rr strati ed by study ( centre ) , age , parity , body - mass index , smoking , and type of menopausal hormone therapy used , where appropriate . 
 menopausal hormone replacement similar results were obtained when the analyses were 1066 vol 16 september 2015 articles ever - users never - users relative risk ( 95% ci ) for ever vs never use of oral contraceptives carcinoma type i carcinoma type ii carcinoma sarcoma cases 9280 6096 controls cases controls 45 625 39 191 39 191 40 024 17 597 9921 70 118 56 365 56 365 57 788 069 ( 066071 ) 068 ( 065071 ) 075 ( 066085 ) 083 ( 067104 ) in a case - case comparison of sarcoma vs carcinoma , p = 002 . 
information about histological subtype ( type i , type ii , or uterine sarcoma ) was available for 17 754 ( 65% ) of 27 276 cases ; the remaining cases were classi ed as carcinoma , unspeci ed . 
 table 2 : relative risk of endometrial cancer in ever versus never users of oral contraceptives by histological subtype * duration of oral contraceptive use ( incidence up to 75 years of age ) never users ( risk to age 75 years : 23% ) 5 years use ( risk to age 75 years : 17% ) 10 years use ( risk to age 75 years : 13% ) 15 years use ( risk to age 75 years : 10% ) age ( years ) figure 4 : absolute risk of endometrial cancer incidence per 100 women up to 75 years of age in high - income countries by duration of oral contraceptive use ( population - weighted rates , 200307 , for 21 countries in western europe , north america , and australasia ) endometrial cancer incidence rates are extremely low before the age of 35 years . random errors , and it also avoids the biases that could be produced by undue emphasis on particular studies with extreme results . 
only a third of the eligible studies have published on oral contraceptives and endometrial cancer , 4 , 7 , 8 , 10 , 17 , 18 , 21 , 24 , 2931 , 33 , 35 so a review based solely on these studies could be a ected by publication bias . 
despite extensive e orts to identify all studies with unpublished results , it is impossible to guarantee that others do not exist ; furthermore , it is not possible to have completely up - to - date information from the continuing prospective studies . 
however , the eight eligible studies that were identi ed but did not contribute data to this collaboration together contain only about 12% as many women with endometrial cancer as the included studies . 
only one of these eight studies has published results on oral contraceptives and endometrial cancer , and its reported ndings are broadly similar to ours.39 the 36 included studies were of varied design and were done in di erent settings , with wide duration of oral contraceptive use . 
for carcinoma , the rr per 5 years use of oral contraceptives was 075 ( 95% ci 073077 , based on 8701 cases ) ; for uterine sarcoma , the corresponding rr was 088 ( 95% ci 074103 , based on 172 cases ; heterogeneity , from direct case - case comparison of sarcomas vs carcinoma p = 024 )  . based on the rrs presented in gure 2 and age - speci c rates of endometrial cancer for women in high - income countries , cumulative incidence rates of endometrial cancer were estimated for never - users of oral contraceptives and for women who had used them for di erent durations , beginning at 20 years of age . 
the corresponding cumulative incidence rate for women who had used oral contraceptives for 5 , 10 , and 15 years was estimated to be 17 , 13 , and 10 per 100 users , respectively ( gure 4 )  . 
in this age range , the number of women who were ever - users of oral contraceptives has grown steeply over the past 50 years , from essentially zero in the 1960s to about three - quarters in high - income countries today.53 hence , the annual number of endometrial cancers prevented by ever - use of oral contraceptives has also increased steeply over the past 50 years . 
using birth cohort - speci c in western prevalences of oral contraceptive use developed countries , 53 we estimate that over the past 50 years ( 19652014 ) in 21 countries in western europe , north america , and australasia , oral contraceptive use has prevented a total of about 400 000 endometrial cancers , including 200 000 in the past 10 years ( 200514 ) , at ages 3074 years ( appendix p 8 )  . 
because these results are based on population they automatically allow for the di erent rates of hysterectomy in those populations . incidence rates , discussion this international collaboration has brought together and re - analysed almost all of the available epidemiological evidence on the reduction in endometrial cancer incidence associated with oral contraceptive use , and includes data from 27 000 women with endometrial cancer from 36 studies . 
a protective e ect persists for at least 30 years after use ceases , and does not seem to depend much on the dose of oestrogen in the contraceptive formulations or on personal characteristics such as parity , adiposity , or menopausal status . combining results from many studies has the obvious advantage of yielding a large sample size , which reduces vol 16 september 2015 1067 articles variation in the duration of use and time since last use of oral contraceptives . 
 the main analyses were strati ed simultaneously by study , centre within study , age at diagnosis , parity , bmi , smoking , and use of menopausal hormone therapy . 
it meant that the analyses of the association between oral contraceptive use and risk of endometrial cancer are based on comparisons between women in the same study who were of the same age and who had a similar history of other risk factors for endometrial cancer . although few studies provided information about hormonal constituents of the preparations used , the oral contraceptives of the 1960s would generally have contained much higher doses of oestrogen than those of the 1980s . 
these results show that the amount of oestrogen in the lower - dose pills is still su cient to reduce the incidence of endometrial cancer , which is consistent with ndings from two studies that have assessed the hormonal dosages constituents.41 , 54 the numbers of women who reported using anything other than combined oral contraceptives ( eg , sequential oral or progestin - only oral contraceptives and / or injectable hormonal contraceptives ) were too small for reliable analysis . individual the decline in endometrial cancer risk with increasing duration of use does not seem to vary substantially with parity , bmi , use of menopausal hormone therapy , menopausal status , smoking status , age at menarche , ethnic origin , or alcohol intake . 
the reduction in risk associated with 5 years use of oral contraceptives was slightly greater in women diagnosed before 60 years of age than in women diagnosed at an older age , but given the number of signi cance tests done , this could be due to chance . 
the reduction in endometrial cancer risk with increasing duration of use does not seem to vary much with factors related to the timing of use , such as age of rst or last use , time since last use , or calendar period of use . the e ect of oral contraceptives does , however , seem to vary by histological subtype , with ever - use strongly associated with a reduced risk of type i and probably of type ii endometrial carcinoma , but somewhat less strongly associated with a reduced risk of uterine sarcomaa much rarer type of cancer . 
another pooled analysis that included 15 studies , most of which contributed to the current analysis , also reported a similar reduction in risk of both type i and type ii endometrial carcinoma for ever use of oral contraceptives51 but no signi cant association with uterine sarcoma.55 taken together , it is reasonable to infer that the associations recorded here are causal ( ie , that current or past oral contraceptive use reduces the incidence of the menstrual cycle , endometrial cancer in otherwise similar women )  . 
almost all of the hormonal contraceptive use in these studies is likely to involve combined oral contraceptives , which contain oestrogen plus progest these contraceptives might protect against endometrial cancer by minimising exposure to unopposed oestrogen during the follicular phase of inhibiting oestrogen - induced cell proliferation ; 56 , 57 moreover , the addition of a progestin to menopausal hormone therapy has been shown to reduce the adverse e ects of oestrogen on the risk of endometrial cancer in postmenopausal women.53 , 5860 however , the exact mechanisms by which oral contraceptives cause substantial protection against endometrial cancer many years after cessation of use are still unclear . 
 thereby since the introduction of oral contraception in the early 1960s , about 400 million women have used it in highincome countries alone , 61 often for prolonged periods during early adulthood.53 medium - to - long - term use of oral con traceptives ( eg , for 5 years or longer ) results in a substantial proportional reduction in the incidence of endometrial cancer , the magnitude of which is similar to that seen for ovarian cancer.53 because this reduction in risk persists more than 30 years after use has ceased , and the incidence of endometrial cancer increases steeply with age , the public health e ect of oral contraceptive use on endometrial cancer is most apparent many years after use has stopped . 
the present results , taken together with what what is known about past patterns of use , suggest that in high - income countries oral contraceptives have , over the past 50 years ( 19652014 ) , already prevented a total of about 400 000 endometrial cancers before the age of 75 years , including 200 000 in the past decade ( 200514 )  . 
 contributors na , vb , swk , rs , ss , and toy identi ed studies , received and checked data , did analyses , and had full access to all materials and results . 
na , vb , gr , ss , and rp drafted the report , and all writing committee members helped to revise it before and after circulation to the collaborators for comment . analysis and writing committee clinical trial service unit & epidemiological studies unit , nu eld department of population health , university of oxford , oxford , uk : n allen , r peto . 
department of primary care health sciences , university of oxford , oxford , uk : r stevens . declaration of interests we declare no competing interests . editorial for calls for reformation see jama 2013 ; 309 : 60709 for the lancet oncologys call to support comparative studies see editorial lancet oncol 2010 ; 11 : 499 for the iom report see php ? record_id = 12214 for more on pcori see quality and value in cancer care in these times of stringent nancial cuts , it is more important than ever to ensure excellent value for money in health - care delivery . 
for example , an e ective therapy with a lower adverse event rate is likely to be more economical than is a lower - cost drug that requires more supportive care . 
identifying a biological approach for a cancer treatment inevitably stimulates a race between pharmaceutical companies to bring a drug to market , often resulting in several agents that act against the same target , but with no evidence of their relative e ectiveness . 
this has brought about an increasing cynicism and scepticism towards the pharmaceutical industry , and calls for reformation to restore con dence . the development of the aromatase inhibitors for hormone - dependent breast cancer is a good example of the need for comparative research . 
although the e cacy and toxicity pro les of exemestane , letrozole , and anastrozole have been shown for each drug , only a few studies have compared pairs of these agents with each other and there are no convincing three - way comparisons . comparative e ectiveness research must be done and funded by organisations that are independent of manufacturers , and that therefore do not have a vested interest . 
further proposed funding cuts of 51% at nih in 2013 makes decisions surrounding the rational use of the decreasing budget ever more urgent . the political climate is right for this policy because optimum delivery of quality and value in health care is being widely debated . 
a report by the us institute of medicine ( iom ) in 2011 stated that , in 2009 , nearly us$25 trillion was spent on health care in the usa , but less than 01% of that sum was allocated to discovering what works best . 
comparative e ectiveness research is a central component of the us patient protection and a ordable care act and resulted in the formation of the patient - centered outcomes research institute ( pcori ) , with a remit to produce research based on both systematic reviews and clinical trials . 
however , the act also mandated that representatives from pharmaceutical companies should be represented on the board , and , because pcori is a private non - pro t corporation , there are concerns about independence and the lack of accountability . 
with hindsight , it would perhaps have been better for pcori to have been embedded within the nih to allow full partnering with research divisions such as the national cancer institute . 
in the rst cycle of award funding , pcori approved 25 grants totalling $407 million , which incredibly included only one oncology project , aimed at improving end - of - life care in a single paediatric cancer . 
 this was a missed opportunity to expand comparative e ectiveness research to improve basic cancer treatment and drive down the unsustainable rise in medical costs in the usa , and pcori should be encouraged to have bigger ambitions in its next round of grant approvals . research e ectiveness nih and iom have a role to ensure us citizens have access to the best care based on scienti c knowledge . 
although president obamas administration recognises that this approach is vital for quality and value in health care , cancer health - care professionals must be vigilant to prevent nancial policy makers cutting back on health - care resources irrespective of e ects on clinical outcomes . 
 the lancet oncology vol 14 march 2013 corrections correction to lancet oncol 2012 ; 13 : 1045 woll pj , reichardt p , le cesne a , et al , for the eortc soft tissue and bone sarcoma group and the ncic clinical trials group sarcoma disease site committee . 
lancet oncol 2012 ; 13 : 104554in this article ( published online sept 4 , 2012 ) , in gure 5 , the total number of events in the control group should have been 499 . 
this correction has been made to the online version as of sept 28 , 2012 , and the printed article is correct . vol 13 october 2012 e412 correction to lancet oncol 2014 ; 15 : 68384 correction to lancet oncol 2018 ; 19 : e510 correction to lancet oncol 2018 ; 19 : e514 venkatesan p . 
this correction has been made to the online version as of oct 1 , 2018 and the printed version is correct . published online august 23 , 2018 s1470 - 2045 ( 18 ) 30652 - 1 correction to lancet oncol 2018 ; 19 : 115556 correction to lancet oncol 2018 ; 19 : 131527 faust js . 
 lancet oncol 2018 ; 19 : 115556 the figure citation has been moved to the following sentence : figure 1 is organised like twitter , facebook , or instagram feeds ( figure ) , except in the place of political rants and pictures of glamorous vacations that you cannot possibly affordbut that somehow your own employees and students canare medical images accompanied by case vignettes . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
lancet oncol 2018 ; 19 : 131527the webappendix of this article ( published online first on sept 12 , 2018 ) has been corrected as of oct 1 , 2018 . straif k , loomis d , guyton k , et al . 
 lancet oncol 2014 ; 15 : 68384 in this news article , it has come to our attention that after the conclusion of the iarc meeting , dr christopher j portier ( the chairman of the iarc monograph advisory group ) declared that he was working part time ( one day per week ) for the environmental defense fund , a us - based non - profit environmental advocacy group . 
the declaration of interests statement in the news article has been updated accordingly as of oct 1 , 2018 . correction to lancet oncol 2015 ; 16 : 147382 motzer rj , hutson te , glen h , et al . 
 lancet oncol 2015 ; 16 : 147382 in the summary of this article , the 95% ci for the hazard ratio of lenvatinib plus everolimus versus lenvatinib alone should have been 039110 . 
this correction has been made to the online version as of oct 1 , 2018 . vol 19 october 2018 e509 corrections erratum fleischhauer k , shaw be , gooley t , et al . 
in the abstract , the rst line of the methods should have read hla and clinical data for unrelated - donor transplantations submitted to the international histocompatibility working group in haemopoietic - cell transplantation were analysed retrospectively . 
in this news article , the rst sentence of the fourth paragraph should have read the researchers found that a daily serving of unprocessed red meat increased the risk of cancer mortality by 10% , whereas a daily serving of processed meat was responsible for a 16% increased risk . 
this correction has been made as of march 26 , 2012 . published online march 26 , 2012 doi : 10.1016 / s14702045 ( 12 ) 70130 - 4 see news page e147 e135 vol 13 april 2012 corrections correction to lancet oncol 2012 ; 13 : 983 , 986 correction to lancet oncol 2012 ; 13 : 1028 correction to lancet oncol 2012 ; 13 : e468 fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 this correction has been made as of oct 29 , 2012 . randomised , chemorefractory jfw , van den smits mlj , nijsen holmium - 166 bosch maaj , et al . 
lancet oncol 2012 ; 13 : 102534in table 1 of this article , the total number of patients with ocular melanoma should have been six , as should the total number of patients with colorectal carcinoma . 
lancet oncol 2012 ; 13 : e468in this news item , the second and third sentences of the second paragraph should have read : median pfs was 94 months ( 95% ci 86167 ) in the combination group compared with 58 months ( 4674 ) in the dabrafenib monotherapy group ( hazard ratio 039 , 95% ci 025062 ; p < 0001 )  . 
 lancet oncol 2015 ; 16 : 8797in the summary of this article ( published online first on dec 4 , 2014 ) , the interpretation section should have read olaparib plus paclitaxel and carboplatin followed by maintenance monotherapy signi cantly improved progression - free survival versus paclitaxel plus carboplatin alone , with the greatest clinical benefit in brca - mutated patients , and had an acceptable and manageable tolerability pro le . 
this correction has been made to the online version as of jan 29 , 2015 . vol 16 february 2015 for more on human mismanagement of the planet see the lancet planetary health journals / lanplh / issue / current for more on developments in us air pollution policies see editorial lancet resp med 2017 ; 5 : 361 for the global burden of disease attributable to ambient air pollution see articles lancet 2017 ; published online april 10 . 
this years annual meeting of the american association for cancer research ( aacr ) in washington , dc , usa ( april 15 , 2017 ) was no exception , and last years meeting saw the launch of the ambitious cancer moonshot programme , which laid out plans to accelerate two - fold the transition of genetic and immunological findings from laboratories to the clinica goal formally recognised when the us senate approved dedicated funding via the 21st century cures act . 
but can this insatiable desire to enhance our fundamental understanding of tumour biology overshadow the health gains that could be secured by improved environmental protection ? many genetic loci associated with increased risk of developing cancer have been discovered , and some can lead to preventive actions . 
 on march 14 , 2017 , the us department of veteran affairs amended a ruling regarding payments to army personnel who had resided at marine corps base camp lejeune ( jacksonville , nc , usa ) for 30 days or longer between aug 1 , 1953 , and dec 31 , 1987all veterans , former reservists , and former national guard members who had been stationed there during this time , and had subsequently been diagnosed with one of several types of cancer , would be entitled to veteran disability benefits . 
 the allowance was made because those who had served at the camp , and their families , had spent the duration of their stay drinking and bathing in water contaminated with an estimated 70 organic volatile compounds known to be carcinogenic . 
since the town changed its water supply in april , 2014 , from lake huron to the flint river , residents noted that their tapwater had become yellow and cloudy . 
after declaring an emergency and enlisting the help of the national guard in 2016 , flint river water was re - declared as unsafe , and work began on replacing lead - contaminated pipes . 
 the consequences of 3 years worth of exposure to lead - contaminated water for flints residentsand especially their growing childrenare unknown , but in view of leads classification as probably carcinogenic to humans in a recent iarc monograph , they are likely to be at an increased risk of developing cancer in the future . 
in view of the precedent set by camp lejeune , where the total settlement has now reached around us$2 billion , this incident will plague and cost residents and regulators alike for decades to come . 
such incidents of neglect inevitably occur elsewhere too : a british water utility company , thames water , was fined a record 203 million on march 22 , 2017 , for a series of leaks of untreated sewage during 201314 into the river thames ( which indirectly supplies londons drinking water ) , its tributaries , and the adjacent land . 
and , contaminated water supplies in china have been long documented . a large - scale economic inefficiency clearly exists , with financial resources being divided into both the science of cancer prevention and also into efforts to help those who have developed cancer as a direct result of human mismanagement of the planet . 
 paradoxically , recent moves by the us government to reduce the funding of the environmental protection agency , to increase coal production , and to review corporate average fuel economy standards will probably increase the populations exposure to carcinogenic pollutants , while at the same time the moonshot programme aims to counter the adverse consequences . 
 outside the usa , the european commission issued a final warning to the uk on feb 15 , 2017 , regarding its repeated breaches of legal air pollution limits , and globally , 42 million deaths in 2015 have been attributed to ambient particulate matter . 
to eradicate cancer , governments need to both identify and act not only on increased risk susceptibility , but also ensure that people are not exposed to carcinogenic materials through gross environmental mismanagement . 
 the lancet oncology vol 18 may 2017 editorial for more on the nhs existential crisis see editorial lancet oncol 2018 ; 19 : 1 for more on wilmshursts letter see brit med j 2018 ; 360 : k549 uk national health servicebeyond repair ? in a recent editorial , we highlighted the disconnect between the uk national health service ( nhs ) and its founding philosophy , and the existential crisis facing british health care . 
recent weeks have seen the highest numbers of patients on record not being treated within prescribed waiting times , patients being queued on trolleys in hospital corridors , and urgent surgeries cancelled because of insufficient intensive - care beds . 
 moreover , dangerous , financially - motivated , clinical decisions are being proposed , patients are donating chemotherapy equipment to under - resourced hospitals , and more protest marches by junior doctors and the public alike are happening than ever before . is a failures these extreme pressures on the nhs are leading in cancer care . 
examples of clinical mismanagement have been highlighted in wales , with one patient diagnosed with a liver mass of 5 cm in january , 2017 , having to wait 8 months for treatment , by which point the tumour was 15 cm and incurable . 
far more leaked memo from the churchill concerning hospital in oxford , uk , where the chemotherapy lead allegedly wrote to fellow oncologists suggesting changes in the provision of chemotherapy . 
as a result of having insufficient nurses in the day treatment unit to administer treatment , the specialist suggested delaying initiation of chemotherapy by 4 weeks , and then increasing the length of each cycle while reducing the number . 
 through diarised anecdotes in his candid bestseller , this is going to hurt : secret diaries of a junior doctor , adam kay starkly illustrates the problems that nhs doctors face , including chronic understaffing , lack of cover , a paucity of senior doctors , long hours , stress , and junior doctors left in charge of large caseloads . 
such circumstances underpin the tragic case of 6 - year old jack adcock who died from a cardiac arrest as a result of sepsis whilst under the care of junior paediatrician hadiza bawa - garba at leicester royal infirmary , leicester , uk , in february , 2018 . 
but , was this a fair and proportionate response ? an enlightening piece on sheri browns blog , confessions of a junior doctor , suggests that , whilst the death of jack adcock is an unacceptable tragedy , it was the manifestation of system failure rather than the actions of a single person . 
other doctors have come out in support of bawe - garbeeg , consultant cardiologist peter wilmshurst has called on the general medical council to investigate his own clinical practice , and urges other doctors to do the same . 
wilmshursts aim is to emphasise that clinical errors do occurno one is infalliblebut such tragic failures of care often result from structural problems in the nhs system rather than from malpractice . a free at the point - of - care , universal health service is widely supported in the uk , but a radical rethink is essential . 
a thorough review of other universal health systems in comparable countries , such as germany and france , could yield important insights in to how to make the service more effective and patient - centric . 
equally , a detailed appraisal of the management , organisation , and intersection between primary care , hospitals , and social care ; the degree of safe staffing ; and realistic funding levels are crucial to define effective changes . 
the idea of a ring - fenced tax dedicated specifically to the nhs could potentially solve funding gaps if introduced in tandem with a governance structure that gives the nhs quasiindependence from governments and politicking , and necessary structural reform . the uk can no longer pretend the nhs can be rectified by short - term solutions . 
 delivering world - class cancer care and all other health services is more than humanitarian goodness , it serves an economic necessity to have a healthy working - age , taxpaying nation . 
other countries have patient - centric and adequately resourced universal health systems , so why not the ukthe country that pioneered the welfare state and is one of richest in the world ? the lancet oncology vol 19 march 2018 editorial for cancer waiting time statistics in england see statistical - work - areas / cancerwaiting - times / ; in scotland see health - topics / waiting - times / cancer / ; in wales see wales / statistics - and - research / nhs - activity - performancesummary / ? skip = 1&lang = en for the general medical council study findings see theguardian.com / society / 2017 / nov / 26 / safety - fears - as - juniordoctors - left - to - run - aes - andother - hospital - units for the lancet oncology editorial see lancet oncol 2015 ; 16 : 1273 for the nhs statement about the budget see theguardian.com / society / 2017 / nov / 30 / nhs - bosses - waiting - timetargets - abandoned - next - year the nhs : failing to deliver on beveridges promise ? just over 75 years have passed since sir william beveridge published his report outlining the parameters for a social welfare state for the uk , which crucially included comprehensive health and rehabilitation services for prevention and cure of disease . 
although the vision of beveridge and bevanto provide free , adequate , and equally accessible health care for allremains in high regard today , the execution and delivery of their goal is currently falling short . 
is the uk in danger of losing the nhs because the government is uninterested in or incapable of the effort needed to save it ? 2017 was a year of great difficulty for the nhs . 
 moreover , and worryingly , in december , 2017 , cancer x - ray diagnostic services came under national review by the care quality commission , after the discovery that between april 1 , 2016 , and march 31 , 2017 , more than 20 000 x - ray images had not been reviewed by a radiologist or properly trained clinician . 
indeed , a study from the general medical council has shown that , due to chronic staff shortages , inexperienced doctors without sufficient training or competence are being left in charge of hospital departments . 
it is thus hardly surprising that nearly 1000 patients have received cancer misdiagnosis settlements totalling 757 million in the past 10 years and that the cost of the nhs clinical negligence scheme has in 200607 to 16 billion in 201617 . increased from 400 million such issues are regrettably reminiscent of nhs difficulties that we highlighted in a previous editorial in october , 2015 . 
long - term underfunding , which in turn has led to deficiencies prevalent for decades in staffing , training , and infrastructure , has been at least partly responsible for this deficit of care . 
 however , analyses indicate that real - term spending on the nhs is decreasing or remaining stagnant , while demand is increasing by up to 7% per year , fuelled by a growing and ageing population with a rising incidence indeed , as high as this of chronic comorbidities . 
 budgetary addition might seem , it will barely cover the cost of the clinical negligence scheme alone and will not get to the root of the problem or provide a net benefit to the systeas service needs rise and resources remain the same , services will exceed capacity and become potentially unsafe . in the late 1940s , with a world war in recent memory , british society was in favour of a social welfare state and there was near cross - party governmental support to provide services such as the nhs . 
 in response to the provision in the 2017 autumn budget , nhs england issued a damning statementit would have to ignore waiting time limits , stop prescribing some over the counter medications , and would not be able to guarantee to act on any new nice guidance , all of which would breach the nhs constitution . 
 in terms of oncology recommendations , hunt did promise to hire 500 more cancer experts , but this addition barely covers current critical shortfalls in staffing , and does not address infrastructure or treatment requirements . 
 on dec 11 , 2017 , kings college hospital nhs foundation trust chairman lord robert kerslake resigned , telling the bbc that he believes the government and regulator are unrealistic about the scale of the challenge facing the nhs . 
yet nhs governance is not blamelessfurther funding is of no use if smart and judicious decisions are not made to ensure the service is optimised around efficiency , safety , and patients . 
it is a paradox that at a time when more and more countries aspire to universal health care that the country that spearheaded the model is moving further from it . 
 the lancet oncology vol 19 january 2018 editorial correction to lancet oncol 2020 ; 21 : e57588 correction to lancet oncol 2021 ; 22 : 2942 correction to lancet oncol 2021 ; 22 : 8597 bahadoer rr , dijkstra ea , van etten b , et al . 
short - course radiotherapy followed by chemotherapy before total mesorectal excision ( tme ) versus preoperative chemoradiotherapy , tme , and optional adjuvant chemotherapy locally advanced rectal cancer ( rapido ) : a randomised , open - label , phase 3 trial . 
 lancet oncol 2021 ; 22 : 2942in figure 1 in this article , in the standard of care group , of the 187 patients who had adjuvant chemotherapy , 185 should have been indicated as having this chemotherapy according to hospital policy . 
fixeddose combination of pertuzumab and trastuzumab for subcutaneous injection plus chemotherapy in her2 - positive early breast cancer ( federica ) : a randomised , open - label , multicentre , non - inferiority , phase 3 study . 
lancet oncol 2021 ; 22 : 8597in table 2 of this article , the cycle 7 ( predose cycle 8 ) pertuzumab serum geometric mean auc 021 days ( percentage cv ) , g / ml per day should have been 2440 ( 242 ) for the intravenous infusion group and 2440 ( 262 ) for the fixed - dose combination group , and the cycle 7 ( predose cycle 8 ) trastuzumab serum geometric mean ( percentage cv ) , auc 021 days g / ml per day should have been 1640 ( 240 ) for the intravenous infusion group and 1700 ( 289 ) for the fixed - dose combination group . 
intermittent schedules of the oral rafmek inhibitor ch5126766 / vs - 6766 in patients with ras / raf - mutant solid tumours and multiple myeloma : a single - centre , open - label , phase 1 dose - escalation and basket dose - expansion study . 
also , sentence two of paragraph four of the discussion should have read these tumours harboured a range of ras and raf mutations , including kras gly12asp , kras gly12val , kras gly12arg , brafve , and hras gly13arg . 
 vol 22 february 2021 corrections editorial for the acs letter see center / acs - can - requestssurgeon - generals - report - onsugar - sweetened - beverages / for more on overweight and obesity and cancer see n engl j med 2003 ; 348 : 162538 for more on the 2012 cancer prevention guidelines see ca cancer j clin 2012 ; 62 : 3067 for more on physical activity see comment lancet 2012 ; 380 : 18990 for more on the food industry see plos med 2012 ; 9 : e1001246 for more on cynical marketing and brand alignment see editorial lancet 2012 ; 380 : 188 for more on the un declaration on non - communicable diseases see editorial lancet oncol 2011 ; 12 : 981 healthy choice should be the easy choice on july 3 , 2012 , the american cancer society ( acs ) cancer action network asked the us surgeon general to initiate a comprehensive review of the consumption of sugarsweetened beverages and their e ects on healthwith the aim of raising public consciousness and changing behaviours in choices of food and beverages . 
 the acss request is in line with its recent guidelines on nutrition and physical activity for cancer prevention , which proposed individuals recommendations ( eg , limit consumption of high - calorie foods and beverages ) and for community action ( eg , decrease access to and marketing of food and beverages of low nutritional value , particularly to youth )  . for current trends towards increasing portion sizes , sugarsweetened drinks , additives , high - calorie convenience foods , and ready meals , compounded by decreased physical activity , have contributed to the obesity epidemic in the usa , and similar trends are now being seen in many other countries worldwide . 
 the availability of healthy choices are made by individuals , but they can be either facilitated or impeded by social , physical , and economic factors , and by the regulatory environment . 
 access to , and a ordability of healthy foods , compared inexpensive , extensively with marketed high - calorie foods and beverages of low nutritional value , and barriers to physical activity , all contribute to obesity . 
e orts are therefore essential to create an environment that encourages healthy choices , promoting physical activity and increasing access to a ordable , healthy food while decreasing access toand exposure to marketing of food and beverages of low nutritional value . 
 cynical marketing and brand alignment often culminate in the junk food and drink giantseg , mcdonalds , coca cola , and cadburys at the 2012 olympics games in londonacting as major sponsors of sporting and social events . 
corporate responsibility campaigns that deftly shift responsibility for overconsumption from corporations to individuals to forestall regulation and promote brandtactics similar to those employed by the tobacco industryare also worrying and should be strongly discouraged . 
for instance , companies could be incentivised to decrease additive content over longer periods of time to gradually acclimatise consumers to the di erence while not having a major e ect on the viability of their business . interventions and strategies should aim to make healthy choices the easiest choices . 
at both the individual and community level , health policies should aim to : improve awareness and information about bene ts of a healthy lifestyle ; introduce appropriate scal measures to make healthy food more a ordable ; and enhance regulatory mechanisms and measures that increase nutritional information or restrict marketing of unhealthy food . 
the 2004 who global strategy on diet , physical activity , and health , and the 2011 un highlevel summit political declaration on the prevention of non - communicable diseasesin response to the rapid changes in nutrition and physical activity all over the globeprovide a framework that should be implemented and strengthened . 
it took nearly ve decades from the us surgeon generals report on tobacco and cancer for e ective public health policies to be put in place ; we cannot wait that long this time . 
 the lancet oncology vol 13 august 2012 circulating tumour dna analysis to direct therapy in advanced breast cancer ( plasmamatch ) : a multicentre , multicohort , phase 2a , platform trial nicholas c turner , belinda kingston , lucy s kilburn , sarah kernaghan , andrew m wardley , iain r macpherson , richard d baird , rebecca roylance , peter stephens , olga oikonomidou , jeremy p braybrooke , mark tuthill , jacinta abraham , matthew c winter , hannah bye , michael hubank , heidrun gevensleben , ros cutts , claire snowdon , daniel rea , david cameron , abeer shaaban , katrina randle , sue martin , katie wilkinson , laura moretti , judith m bliss * , alistair ring * summary background circulating tumour dna ( ctdna ) testing might provide a current assessment of the genomic profile of advanced cancer , without the need to repeat tumour biopsy . 
we aimed to assess the accuracy of ctdna testing in advanced breast cancer and the ability of ctdna testing to select patients for mutation - directed therapy . methods we did an open - label , multicohort , phase 2a , platform trial of ctdna testing in 18 uk hospitals . 
 patients were recruited into four parallel treatment cohorts matched to mutations identified in ctdna : cohort a comprised patients with esr1 mutations ( treated with intramuscular extended - dose fulvestrant 500 mg ) ; cohort b comprised patients with her2 mutations ( treated with oral neratinib 240 mg , and if oestrogen receptor - positive with intramuscular standard - dose fulvestrant ) ; cohort c comprised patients with akt1 mutations and oestrogen receptor - positive cancer ( treated with oral capivasertib 400 mg plus intramuscular standard - dose fulvestrant ) ; and cohort d comprised patients with akt1 mutations and oestrogen receptor - negative cancer or pten mutation ( treated with oral capivasertib 480 mg )  . 
 for cohort a , 13 or more responses among 78 evaluable patients were required to infer activity and three or more among 16 were required for cohorts b , c , and d . 
this trial is registered with clinicaltrials.gov , nct03182634 ; the european clinical trials database , eudract2015 - 003735 - 36 ; and the isrctn registry , isrctn16945804 . findings between dec 21 , 2016 , and april 26 , 2019 , 1051 patients registered for the study , with ctdna results available for 1034 patients . 
cohorts b and c met or exceeded the target number of responses , with five ( 25% [ 95% ci 949 ] ) of 20 patients in cohort b and four ( 22% [ 648 ] ) of 18 patients in cohort c having a response . 
 cohorts a and d did not reach the target number of responses , with six ( 8% [ 95% ci 317 ] ) of 74 in cohort a and two ( 11% [ 133 ] ) of 19 patients in cohort d having a response . 
17 serious adverse reactions occurred in 11 patients , and there was one treatment - related death caused by grade 4 dyspnoea ( in cohort c )  . interpretation ctdna testing offers accurate , rapid genotyping that enables the selection of mutation - directed therapies for patients with breast cancer , with sufficient clinical validity for adoption into routine clinical practice . 
our results demonstrate clinically relevant activity of targeted therapies against rare her2 and akt1 mutations , confirming these mutations could be targetable for breast cancer treatment . funding cancer research uk , astrazeneca , and puma biotechnology . copyright 2020 the author ( s )  . 
however , there has been uncertainty about the validity of ctdna testing in routine practice , as there have been few large prospective studies to assess the accuracy and utility of ctdna testing . 
in addition , sensitivity has not been perfect in previous retrospective studies , suggesting the potential for false negative ctdna results , and , in routine clinical practice , reflex testing of tumour tissue is advised to confirm negative results . 
in 2018 , the american society of clinical oncology and college of american pathologists guidelines committee on ctdna analysis concluded that the absence of prospective trials was one of the major weaknesses in the evidence for bringing ctdna testing to routine practice , with a need for trials that recruited patients solely on the basis of ctdna testing without tissue testing beforehand . added value of this study plasmamatch is , to our knowledge , the first large , prospective , multicentre study assessing the feasibility and clinical utility of ctdna analysis to direct therapy in patients with advanced breast cancer . 
patients with rare , potentially targetable mutations in her2 and akt1 in ctdna had clinically important responses with the her2 inhibitor neratinib and akt inhibitor capivasertib , respectively , similar to activity seen in previous tissue sequencing - directed trials . 
these findings confirm that these mutations are targetable for breast cancer therapy , and demonstrate the validity and clinical utility of using ctdna testing to screen patients for rare mutations . implications of all the available evidence these findings show that ctdna testing for mutations has sufficient accuracy for widespread adoption in clinical practice , with the assays used . 
the high sensitivity of ctdna testing for tissue mutations calls into question the need for reflex tissue testing for negative ctdna results , within the pretreated metastatic breast cancer patient population studied . 
 highly sensitive assays have been developed in the past 5 years to analyse circulating tumour dna ( ctdna ) , which is released into the plasma in small quantities as cancer cells die , providing the opportunity for a scalable , non - invasive approach to profile tumours for somatic mutations.10 retrospective studies show high agreement between ctdna analysis and tumour tissue - based analysis in patients with advanced cancer.11 however , previous prospective studies comparing commercially available ctdna assays have shown there might be substantial discordance in ctdna testing results , 12 , 13 raising concerns over whether ctdna testing is ready for widespread clinical adoption.14 we aimed to assess the clinical validity of ctdna testing , and to investigate the clinical utility of using ctdna to select targeted therapies for patients without previous tissue testing . methods study design and participants plasmamatch is a multicohort , open - label , nonrandomised , phase 2a clinical trial platform run across 18 uk hospitals ( appendix p 2 )  . 
those with potentially targetable mutations identified in ctdna testing ( esr1 , her2 , akt1 , or pten ) were offered entry into one of four parallel treatment cohorts ( ad ) according to the see online for appendix vol 21 october 2020 1297 articles identified , with therapies matched mutation mutations . 
a fifth cohort ( e ) recruiting patients with triple - negative breast cancer with no targetable mutation , designated to receive olaparib plus the atr inhibitor azd6738 , is ongoing and will be reported separately . 
 eligible patients were women at least 18 years of age with histologically confirmed advanced breast cancer that was not suitable for treatment with radical or curative intent , who had measurable disease , an eastern cooperative oncology group performance status of 02 , estimated life expectancy of more than 3 months , and were suitable for a baseline advanced disease biopsy or had an archival advanced disease biopsy available for subsequent retrospective sequencing and comparison with ctdna . 
 patients were required to have had disease progression on radiological or clinical assessment at registration ( with radiological confirmation required before treatment cohort entry ) , and to have completed at least one previous line of treatment for advanced breast cancer , or relapsed within 12 months of neoadjuvant or adjuvant chemotherapy . 
patients with her2 - positive breast cancer must have had at least two previous lines of her2 - targeted therapy in the advanced setting ( or one line if no further her2 - targeted therapies were available )  . 
an approved protocol amendment implemented on feb 19 , 2018 , after 515 patients had been recruited , required a maximum of two previous lines of chemo therapy , antibodydrug conjugate , or immunotherapy . 
exclusion criteria for ctdna testing included uncon trolled cns or cardiac disease , ongoing toxicities of grade 1 or higher from previous treatments , and malignancies of other types within the past 3 years . 
cohort - specific eligibility criteria are given in the protocol ( appendix )  . the study was co - sponsored by the institute of cancer research and the royal marsden national health service ( nhs ) foundation trust , london , uk , and approved by a research ethics committee ( 16 / sc / 0271 )  . 
digital droplet pcr was done at a central laboratory in the national institute for health research centre for molecular pathology at the royal marsden nhs foundation trust and institute of cancer research prospectively in all patients , for mutations in pik3ca , esr1 , her2 , and akt1 ( appendix p 4 )  . 
from july 10 , 2018 ( after recruitment of 680 patients ) , prospective testing also included error - corrected targeted sequencing with guardant360 ( guardant health ; redwood city , ca , usa ) for a panel of 73 genes including pik3ca , esr1 , her2 , akt1 , pten , and tp53 , with retro spective for previously enrolled patients . 
for sequencing results , tumour comparison with ctdna tissue sequencing using advanced disease tissue biopsies was done retro spectively for patients who entered a treatment cohort ( appendix p 5 )  . 
testing for pik3ca mutations was included to test the validity of the pik3ca ctdna testing , but was not used for entry to therapeutic cohorts as phase 3 studies of treatments for breast cancer with pik3ca mutations were ongoing when plasmamatch started recruitment.1 a positive result by either ctdna assay was sufficient for cohort entry . 
if more than one mutation was identified , entry to cohorts bd took preference to cohort a . received extended - dose 500 mg cohort a included individuals with esr1 mutations ; they fulvestrant ( a selective oestrogen receptor downregulator ) administered intramuscularly on days 1 , 8 , and 15 in cycle 1 , and days 1 and 15 in cycle 2 onwards , on a 28 - day cycle . 
in cohort a , as a prespecified exploratory analysis , esr1 mutations were determined to be clonally dominant or subclonal , with a clonally dominant mutation indicating a summed esr1 allele fraction of 50% or greater of maximum allele fraction detected in the sample by targeted sequencing to correct for variations in the purity of ctdna in plasma dna ( appendix p 5 )  . cohort b included individuals with her2 mutations ; they received 240 mg neratinib ( an irreversible pan - her tyrosine kinase inhibitor ) orally once a day on a continuous schedule . 
in patients with oestrogen receptorpositive breast cancer , this treatment was administered together with fulvestrant 500 mg intramuscularly at standard dosing ( days 1 and 15 in cycle 1 and day 1 in cycle 2 onwards on a 28 - day cycle )  . cohort c included individuals with akt1 mutations and oestrogen receptor - positive breast cancer ; they received 400 mg capivasertib ( selective akt inhibitor ) orally twice a day for 4 days on followed by 3 days off continuously with fulvestrant 500 mg intramuscularly at standard dosing . cohort d included individuals with an akt pathway activating mutation ( mutations in akt1 with oestrogen receptor - negative breast cancer , or pten inactivating mutations or homozygous deletion [ irrespective of oestrogen receptor status ] ; full criteria are described in the appendix p 6 )  . 
this cohort received 480 mg capivasertib monotherapy orally , twice a day for 4 days on , followed by 3 days off , continuously . in addition to the eligibility criteria for ctdna testing , for cohort assignment patients with a relevant targetable mutation had to have adequate haematological , renal , and hepatic function ( adequate defined as absolute neutrophil count 10 10 cells per l , platelet count 100 10 per l , 1298 vol 21 october 2020 articles haemoglobin 9 g / dl , serum crea tinine 15 the upper limit of normal [ uln ] , total bilirubin 15 uln , alanine aminotransferase and aspartate aminotransferase 3 uln [ or 5 uln in the presence of liver metastases ] )  . 
for cohorts c and d , patients were excluded if baseline glycated haemoglobin ( hba1c ) was 80% ( 64 mmol / mol ) or fasting plasma glucose was 70 mmol / l ( 126 mg / dl ) , or they had poorly controlled diabetes . 
patients were eligible for cohort entry with detection of a mutation at any allele fraction , and clonal dominance was not considered in eligibility . once enrolled into a cohort , treatment was given until disease progression , unacceptable toxicity , or pregnancy . 
laboratory assessments , adverse event recording , and vital signs were performed every 4 weeks at a minimu toxicity was assessed using national cancer institute common terminology criteria for adverse events version 4 . 
coding was done with use of the medical dictionary for regulatory activities version 22 . outcomes the primary endpoint for cohorts ad was confirmed objective response rate defined as a confirmed complete response or partial response according to recist criteria at any point during trial treatment . 
secondary endpoints included duration of response ( defined as time from the first documentation of complete response or partial response until date of disease progression or last date of follow - up ) , clinical benefit rate ( defined as complete response , partial response , or stable disease for more than 6 months during trial treatment ) , progression - free survival ( defined as time from cohort entry to first date of either confirmed progression of disease according to recist criteria or death from any cause ) , safety and tolerability of therapies , frequency of mutations , accuracy of ctdna testing by agreement between ctdna mutation status and tissue mutation status and the proportion of patients entering a cohort , and pharmacokinetics ( for cohorts a and b )  . 
prespecified exploratory endpoints included confirmed response rate in clonally dominant versus subclonal mutations in cohort a . statistical analysis all cohorts used a single - stage ahern design with 5% , to have 80% power . 
cohort a assumed an unacceptable response rate of 10% and a target response rate of 20% in the final design , requiring 13 or more responses from 78 evaluable patients to infer activity . 
this assumption was an approved amendment ( on may 1 , 2018 ) to the original two - stage design to account for the ctdna testing detecting subclonal mutations as well as clonal mutations where the response rate was expected to be lower ( appendix p 6 )  . 
cohorts b , c , and d each assumed an unacceptable response rate of 5% and a target response rate of 25% , requiring three or more responses from 16 evaluable patients . 
this number gave 85% probability of identifying 25 patients for a mutation with prevalence of 3% for each of cohorts b , c , and d individually , allowing for 36% attrition between ctdna screening and cohort entry . objective response rate , duration of response , and clinical benefit rate were measured in an evaluable population defined as those patients with measurable disease per recist at baseline and at least one on - treatment assessment ; patients who stopped treatment because of intolerable toxicity or death without having a scan after baseline were evaluable and recorded as non - responders . 
proportions and two - sided 95% cis for estimation purposes were reported for each cohort and in prespecified subgroup analyses ( by clonally dominant versus subclonal mutations in cohort a , compared using a fishers exact test , by hormone receptor status in cohort b , and by akt1 or pten mutation in cohort d )  . 
analysis of clonality of her2 mutations in cohort b and of akt1 in cohort c was a post - hoc analysis . in post - hoc exploratory analyses , response rates for each cohort were reported by pik3ca and tp53 mutation status and , for cohort a , tissue mutation status . 
for inference purposes , thus corresponding to the design characteristics underpinning the trials hypothesis testing ( ie , alpha 5% , one - sided ) , proportions and two - sided 90% cis are reported . progression - free survival was measured in the intentionto - treat population . 
patients who were alive and progression free were censored at date of last follow - up ; patients who had non - recist confirmed progression ( eg , clinically judged progression or radiologically confirmed but lesions not measured according to recist ) were censored at the date progression was reported . 
the safety population included all patients who had at least one dose of treatment , regardless of their eligibility , and treatment - emergent adverse events where more than 10% of patients reported any grade of the adverse event or any patients reported the adverse event at grade 3 or higher were presented . 
in addition , pharmacokinetics were reported as a percentage vol 21 october 2020 1299 articles change from an approved historical population pharmacokinetic model for standard - dosing 500 mg fulvestrant , in cohort a only . 
this study is registered with clinicaltrials.gov , nct03182634 ; the european clinical the trials database , eudract2015 - 003735 - 36 ; and isrctn registry , isrctn16945804 . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 the corresponding author had full access to all of the data and the final responsibility to submit for publication . results between dec 21 , 2016 , and april 26 , 2019 , 1051 patients were registered into the study ( 1044 via ctdna screening , seven via previous tumour sequencing ; figure 1 ; appendix p 17 ) with ctdna results available for 1034 patients ( 990% )  . 
digital pcr results were available for 1025 patients ( 982% ) and targeted sequencing results were available for 800 patients ( 766% ; 364 prospective and 436 retrospective )  . 
patients had a median of one ( iqr 02 ) previous lines of chemotherapy , and a median of two ( 13 ) previous lines of systemic therapy ( table )  . a somatic mutation was detected in 743 ( 93% ) of 800 patients with ctdna targeted sequencing results ( appendix p 18 )  . 
esr1 mutations were found almost exclusively in hormone receptor - positive breast cancer , were found at lower average allele fractions than other mutations , and were frequently polyclonal ( appendix pp 1718 )  . 
her2 mutations were found least frequently in triple - negative breast cancer , while akt1 mutations were found at a similar frequency in hormone receptorpositive her2 - negative breast cancer and triple - negative breast cancer ( appendix p 18 )  . gene - level agreement identification between ctdna digital pcr and targeted sequencing ( n = 800 ) was 9699% ( kappa 089093 ; figure 1 )  . 
 for mutation sensitivity ( or percent - positive agreement reflecting the absence of gold standard ) for digital pcr was 93% ( 95% ci 8398 ) overall and 98% ( 87100 ) in patients with contemporaneous biopsies ( appendix pp 17 , 20 )  . 
 specificity for both digital pcr and sequencing ( or percent - negative agreement reflecting the absence of gold standard ) was high for akt1 , her2 , and pik3ca , varying by gene ( appendix p 17 )  . 
esr1 mutations had lower percent - negative agreement . identified mutations were in 533 for ctdna ( 511% ) of 1044 patients registered testing and 357 ( 345% ) of 1034 with results had targetable mutations eligible for cohort entry , of whom 136 entered one of the five available cohorts . 
the most common reason for not entering a cohort was that the patient was ineligible based on the specific eligibility criteria for the relevant cohort , or in the case of cohort a ( esr1 mutation ) , 64 patients did not enter because of cohort a being suspended ( while the protocol amendment to change the design was ongoing ) or closed ( figure 1 ; appendix p 7 )  . 84 ( 38% ) of 222 patients with an esr1 mutation in ctdna identified while cohort a was open to recruitment were enrolled in cohort a ( figure 1 , table )  . 
the most common esr1 mutations detected in plasma were asp538gly ( 45 [ 54% ] of 84 ) , tyr537ser ( 31 [ 37% ] ) , and glu380gln ( 29 [ 35% ] )  . 
 six ( 8% [ 95% ci 317 ] ) of 74 patients had a confirmed partial response with a median duration of response of 70 months ( iqr 3783 ) and four patients continuing on treatment at data cutoff ( figure 2 )  . 
in a pre - planned exploratory analysis , five ( 12% [ 95% ci 426 ] ) of 41 patients with clonally dominant esr1 mutations , and none ( 0% [ 013 ] ) of 27 patients with subclonal mutations had a confirmed response ( p = 015 ; 27 [ 40% ] of 68 esr1 mutations were subclonal ) ; six patients had unknown clonality . 
the main reason for treatment increased 1300 vol 21 october 2020 articles 1051 met inclusion criteria and registered for plasmamatch 7 registered to cohort d with previous tumour tissue sequencing 10 results not available ( test failed or not done ) 501 with no mutation or amplication identied 176 not eligible for cohort 148 pik3ca mutation 20 her2 amplication 8 pik3ca mutation and her2 amplication 221 did not enter a cohort 67 ineligible 22 patient choice 40 clinician decision 64 cohort a suspended or closed 6 other cohort closed ( deadline passed for cohort entry ) 8 died before cohort entry 14 unknown 1044 registered for ctdna testing 1034 ctdna testing results available * 1025 digital pcr 364 targeted sequencing 533 with mutation or amplication identied 357 with targetable mutation ( s ) identied 136 entered a cohort via ctdna testing 18 entered cohort c ( akt1 mutation and oestrogen receptor - positive breast cancer ) 18 initiated treatment 18 were evaluable for response 84 entered cohort a ( esr1 mutation ) 21 entered cohort b ( her2 mutation ) 80 initiated treatment 74 were evaluable for response 20 initiated treatment 20 were evaluable for response 1 entered cohort e ; to be reported at a later date ( triplenegative breast cancer with no mutation ) 19 entered cohort d ( akt basket ; akt1 mutation with oestrogen breast cancer , or pten mutation ) receptor - negative 19 initiated treatment 19 were evaluable for response figure 1 : trial profile further detail on accuracy of ctdna testing is provided in the appendix ( p 17 )  . 
 * 436 additional samples were analysed by targeted sequencing retrospectively ; these were not used for determining cohort suitability ; agreement between digital pcr and targeted sequencing ( n = 800 ) was as follows : akt1 kappa 093 ( 95% ci 087099 ) , her2 kappa 0.89 ( 079098 ) , esr1 kappa 090 ( 086093 ) , and pik3ca kappa 092 ( 089095 )  . vol 21 october 2020 1301 articles discontinuation was disease progression ( 72 [ 95% ] of 76 patients ; appendix p 8 )  . 
fulvestrant activity was similar in patients with and without esr1 mutations in tissue sequencing ( appendix p 29 )  . 21 ( 58% ) of 36 patients with an her2 mutation in ctdna were enrolled in cohort b ( figure 1 , table )  . 
the ( ten most common her2 mutations detected in plasma were [ 48% ] of 21 patients ) , val777leu leu755ser ( four [ 19% ] ) , and ser310phe ( three [ 14% ] )  . 
five ( 25% [ 95% ci 949 ) of 20 patients had a confirmed response ( one complete and four partial ) , and an additional three patients had unconfirmed partial responses ( figure 3 )  . 
for patients with oestrogen receptor - negative breast cancer and akt1 mutation or pten mutation the denominator is patients with hr - positive disease only ( for those who entered cohort d n = 13 ; for those that did not enter cohort d n = 11 )  . 
||patients may be included in more than one type of systemic therapy , but patients are only included once in each category ( eg , if a patient had trastuzumab and pertuzumab they are counted once in the anti - her2 therapy category )  . 
in the subgroup of patients with hormone receptor - positive her2 - negative breast cancer treated with neratinib and fulvestrant , four ( 24% [ 95% ci 750 ] ) of 17 patients had a confirmed response ( figure 3 )  . 
the most common grade 3 or grade 4 adverse events were diarrhoea ( four [ 20% ] of 20 patients ) and hypertension ( three [ 15% ] ; appendix p 11 )  . 
ctdna = circulating tumour dna . previous fulvestrant therapy no previous fulvestrant therapy neratinib plus fulvestrant neratinib hr positive , her2 negative hr negative , her2 negative hr negative , her2 positive insertion ser310phe val777leu leu755ser val697leu figure 3 : neratinib in her2 - mutant breast cancer ( cohort b ) waterfall plot of maximum change in tumour size in individual patients with her2 mutations in ctdna treated with neratinib alone or neratinib plus fulvestrant . 
ctdna = circulating tumour dna . patients 18 ( 60% ) of 30 patients with an akt1 mutation in ctdna and oestrogen receptor - positive cancer were enrolled in cohort c ( figure 1 ; table )  . 
all 18 patients were evaluable ; four ( 22% [ 95% ci 648 ] ) patients had a confirmed partial response , and an additional four patients had unconfirmed partial responses ( figure 4a )  . 
in a post - hoc analysis , four ( 23% ) of 17 akt1 mutations ( clonality was assessable in 17 patients ) were subclonal ( appendix p 24 )  . 
the median relative dose intensity was 88% ( iqr 7099 , range 25101 ) for capivasertib and 99% ( iqr 97100 , range 94102 ) for fulvestrant . 19 patients were enrolled in cohort d , 12 following ctdna testing and seven following tumour testing ( figure 1 , table 1 )  . 
 the most common grade 3 or grade 4 adverse events were rash ( five [ 26% ] of 19 patients ) , hypertension ( two [ 11% ] ) , aminotransferase increase ( two [ 11% ] ) , gamma - glutamyltransferase increase ( two [ 11% ] ) , and vomiting ( two [ 11% ] ; appendix p 15 )  . 
 the median relative dose intensity of capivasertib was 94% ( iqr 63100 , range 42102 )  . 1304 vol 21 october 2020 articles previous fulvestrant therapy no previous fulvestrant therapy 100 100 in post - hoc analyses , the response rates in cohorts ad did not vary by pik3ca or tp53 co - mutational status ( appendix pp 2728 )  . discussion in this large , prospective trial of ctdna testing in advanced breast cancer , we found that ctdna testing was highly accurate , with high agreement between different ctdna testing techniques , and high sensitivity for mutations identified in advanced breast cancer tissue biopsies . 
ctdna testing identified patients with rare targetable mutations and these patients were recruited into cohorts that were given targeted therapies ( matched to mutations ) without confirmatory tumour testing , with activity comparable to previous studies involving tumour tissue testing.4 , 5 we enrolled more than 1000 patients across the uk in less than 3 years , and the dynamic trial platform design allowed for the simultaneous evaluation of multiple targeted treatment options . the availability and accuracy of ctdna testing shown in this study compares favourably with tissue - based mutation testing . 
nearly all patients ( 99% ) received a result from ctdna tumour testing , contrasting with previous sequencing studies where results were typically received in only 7090% of patients.15 , 16 in addition , previous tumour sequencing studies generally only included patients with disease that could be biopsied , which is not a constraint for ctdna testing . 
results were received relatively quickly after blood draw , compared with results for tissue - based testing , and this led to a high conversion rate of patients with ctdna mutations into the corresponding treatment cohort . 
the accuracy of ctdna testing was also similar to that achieved with tissue sequencing.17 discordance between ctdna results was still observed for patients at low allele frequency mutations , suggesting further potential for assay development . 
esr1 mutations had lower percent - negative agreement , probably reflecting the subclonality of acquired esr1 mutations , with ctdna detecting mutations present in metastasic sites other than the one biopsied . 
533 ( 511% ) of 1044 patients who underwent ctdna testing had a potentially targetable mutation ( pik3ca , esr1 , her2 , akt1 , or pten ) , indicating a potential value for ctdna testing . testing could replace akt1 leu52arg akt1 glu17lys entered trial on the basis of ctdna testing entered trial on the basis of tissue sequencing hr positive , her2 negative hr negative , her2 negative akt1 glu17lys akt1 leu52arg pten single nucleotide variant pten truncating pten deletion patients figure 4 : capivasertib in akt1 - mutant and pten - mutant breast cancer ( cohorts c and d ) ( a ) waterfall plot of maximum change in tumour size in individual patients with hr - positive cancer and akt1 mutations in ctdna , treated with capivasertib plus fulvestrant ( cohort c )  . 
 ( b ) waterfall plot of maximum change in tumour size in individual patients with akt1 mutations and hr - negative breast cancer , or with activating pten mutations , treated with capivasertib ( cohort d )  . 
in a previous phase 1 study with an expansion cohort of those with her2 - mutant breast cancer identified in tissue , who were given neratinib , there was a 32% unconfirmed response rate after 8 weeks of treatment.4 in our study , neratinib for her2 - mutant breast cancer identified by ctdna testing had comparable activity to that observed when guided by tissue testing , with durable responses . 
similarly , capivasertib had high activity in patients with ctdna - identified akt1 mutations , vol 21 october 2020 1305 articles both in hormone receptor - positive cancer with fulvestrant and in hormone receptor - negative cancer as a single agent , again con firming the results of a previous phase 1 study.5 these results confirm the high activity of these drugs against her2 and akt1 mutations , and strongly support the need for registration trials , facilitated by a ctdna testing programme . our study did not show benefit from increasing the dose of fulvestrant in patients with esr1 mutations in ctdna . 
previous research has suggested that fulvestrant at standard doses does not maximally inhibit or degrade mutated esr1 , 18 and we assessed whether more frequent administration of fulvestrant would increase therapeutic utility . 
although exposure was increased in later cycles , this was insufficient to enhance activity , with the response rate remaining similar to that previously reported.19 , 20 we note however that our study recruited a heavily pretreated population , and this might have reduced the activity of fulvestrant . 
more potent oestrogen receptor inhibitors , such as novel oral oestrogen receptor degraders and modulators , are also likely to be required.21 we found that patients with tyr537ser esr1 mutations were no less sensitive to fulvestrant than those with other that esr1 mutations were esr1 mutations , and frequently subclonal , with detection of esr1 mutations in ctdna that were not present in contemporaneous single site tissue biopsies , reflecting the limited sampling of single site tissue biopsies . 
inclusion of relatively heavily pretreated patients might reduce activity of the targeted drugs , especially in cohort a , and future ctdna selection trials might benefit from more restrictive entry criteria . 
 the study was designed to assess the activity of therapies against specific genomic events , but it did not target pik3ca mutations , 1 and as a result relatively few of the patients registered to the trial had a response to therapy ( 17 [ 16% ] of 1051 patients )  . 
although we identified low activity of capi vasertib in pten - mutant cancers when used as a single agent , akt inhibition in combination with paclitaxel chemotherapy might be efficacious in ptenmutant cancers.22 , 23 capivasertib plus fulvestrant might be efficacious in endocrine - resistant oestrogen receptorpositive breast cancer without mutation selection , as shown in the faktion trial.24 it is not possible to robustly compare plasmamatch with faktion , as patients enrolled in plasmamatch had more previous lines of treatment , and akt1 mutations were not assessed and would be few in number in faktion.24 in conclusion , we show that ctdna testing , with the assays employed in this study , has sufficient accuracy for widespread adoption in routine clinical practice to identify patients with breast cancer who are suitable for licensed targeted therapies , such as pik3ca - mutant breast cancer , with the transformative potential of efficient and rapid screening for clinical trials . 
a high proportion of patients with specific targeted mutations were able to enrol on the matching treatment cohort , with clinically important activity observed with therapies matched to akt1 and her2 mutations . 
with mutationmatching therapy now approved in breast cancer , with alpelisib for pik3ca - mutant disease , ctdna testing can be seen as a standard - of - care test for both common and rare targetable genetic events . contributors nct is the chief investigator , and ar is the coordinating investigator for the trial . 
jmb is the trials methodology lead within the institute of cancer research clinical trials and statistics unit ( icr - ctsu ) and provided oversight and guidance for trial management , statistics , and data interpretation throughout the trial . 
 amw , irm , rdb , rr , and ar are all cohort clinical leads responsible for the clinical oversight and safety review and evaluation for a defined treatment cohort within the trial . 
amw , irm , rdb , rr , ps , oo , jpb , mt , mcw , dr , dc , as , mh , and kr are members of the plasmamatch trial management group , which contributed to study design , was responsible for oversight throughout the trial , and contributed to data interpretation and manuscript preparation . 
ps , oo , jpb , mt , ja , mcw , and dc were involved in recruitment and treatment of participants and contributed to data collection and manuscript preparation . 
 all authors reviewed and approved the manuscript . declaration of interests nct , ar , jmb , lsk , cs , lm , sk , kw , sm , hb , mh , bk , and rc report grants from cancer research uk , grants and non - financial support in the form of study drug provision from astrazeneca and puma biotechnology , non - financial support in the form of ctdna sequencing from guardant health , and provision of reagents from biorad , during the conduct of the study . 
nct also reports grants and personal fees from astrazeneca , pfizer , and roche genentech , personal fees from bristolmyers squibb , lilly , merck sharpe & dohme , novartis , bicycle therapeutics , taiho pharmaceutical , zeno pharmaceuticals , and repare therapeutics , and grants from biorad , clovis , merck sharpe and dohme , and guardant health , outside the submitted work . 
 amw reports personal fees from roche , personal fees and other support from novartis , pfizer , lilly , daiichi sankyo , merck sharpe & dohme , astrazeneca , and athenex , and other support from seattle genetics , andrew wardley , and manchester cancer academy and outreach research and innovation group , outside the submitted work . 
irm reports personal fees and non - financial support from roche , eli lilly , and eisai , and personal fees from novartis , pfizer , daiichi sankyo , genomic health , pierre fabre , and merck sharpe & dohme , outside the submitted work . 
rr reports personal fees from novartis , eli lilly , and pfizer , personal fees and non - financial support 1306 vol 21 october 2020 articles from daiichi sankyo and g1 therapeutics , and non - financial support from roche and astrazeneca , outside the submitted work . 
oo reports grants and personal fees from pfizer and eisai , personal fees from roche genentech and tesaro , non - financial support from astrazeneca , personal fees and non - financial support from eli lilly , and grants from novartis , outside the submitted work . 
 mt reports personal fees from pfizer , novartis , roche , vaccitech , oxford vacmedix , lilly , astellas , genomic health , and eisai , personal fees and non - financial support from janssen , bristol - myers squibb , and ipsen , and non - financial support from eusa pharma , outside the submitted work . 
mcw reports personal fees and non - financial support from eisai , lilly , and roche , and personal fees from pfizer , genomic health , and novartis , outside the submitted work . 
dr reports personal fees from novartis , pfizer , roche , daiichi sankyo , lily , and genomic health , non - financial support from daiichi sankyo and eisai , and grants from celgene , roche , biotheranostics , and rna diagnostics , outside the submitted work . 
 dc reports other support from novartis , astrazeneca , pfizer , roche , eli lilly , puma biotechnology , daiichi sankyo , synthon , seagen , zymeworks , elsevier , european cancer organisation , celgene , succint medical communications , prima biomed , oncolytics biotech , celldex therapeutics , san antonio breast cancer consortium , highfield communication , samsung bioepis , prime oncology , merck sharp & dohme , rti health solutions , and eisai , and grants from cancer research uk , chief scientist office , breast cancer institute , pfs genomics , and national institute for health research health technology assessment , outside the submitted work . 
as reports grants from ventana roche , and genomic heath , personal fees from daiichi sankyo , hologic , genomic health , and ventana roche , outside the submitted work . 
jmb also reports grants and non - financial support from astrazeneca , novartis , janssen cilag , merck sharpe & dohme , pfizer , roche , and clovis oncology , and grants from medivation , outside the submitted work . 
 all other authors declare no competing interests . data sharing de - identified individual participant data , together with a data dictionary defining each field in the dataset , will be made available to other researchers on request , subject to approval of a formal data access request in accordance with the icr - ctsu data and sample access policy . 
trial data are collected , managed , stored , shared , and archived according to icr - ctsu standard operating procedures to ensure the enduring quality , integrity , and utility of the data . 
data recipients are required to enter a formal data sharing agreement , which describes the conditions for data release and requirements for data transfer , storage , archiving , publication , and intellectual property . 
data sharing is undertaken if proposed projects have a sound scientific or patient benefit rationale , as agreed by the trial management group and approved by the trial steering committee , as required . 
additional documents may be shared if approved by the trial management group and trial steering committeeeg , statistical analysis plan and informed consent form . acknowledgments plasmamatch is funded by cancer research uk ( cruk / 15 / 010 , c30746 / a19505 ) with additional support from astrazeneca , puma biotechnology , guardant health , and biorad . 
thanks also to staff at participating centres , the icr - ctsu trial team , the staff at central laboratories , and syed haider and his team in the breast cancer now toby robins research centre bioinformatics core facility for bioinformatics support . 
 plasmamatch is supported by the national institute for health research ( nihr ) manchester clinical research facility at the christie hospital , manchester , uk , and by the cancer research uk cambridge centre , the cambridge nihr biomedical research centre , and the cambridge experimental cancer medicine centre , cambridge , uk . 
 plasmamatch is supported at participating sites in england by the nihr clinical research network , in scotland by the chief scientist office , and in wales by health and care research wales . 
this study represents independent research supported by the nihr biomedical research centre at the royal marsden national health service foundation trust and the institute of cancer research , london , uk . 
the authors also acknowledge past and present colleagues on the plasmamatch trial management group , the independent data monitoring committee , and the trial steering committee , who provided oversight of the trial ( appendix p 3 )  . editorial for the who policy brief see bitstream / 10665 / 179517 / 1 / who_hiv_2015.17_eng. pdf ? ua = 1&ua = 1 for the report of the national transgender discrimination survey see thetaskforce.org / static_html / downloads / reports / reports / ntds_full.pdf for more on transgender health in the usa see world report lancet 2015 ; 386 : 72728 cancer risk in the transgender community for hiv control and care on july 8 , who released a new policy summarising recommendations transgender populations . 
indeed , there is scant information on cancer outcomes for transgender people because of an absence of large - scale prospective studies investigating cancer incidence and mortality in lesbian , gay , bisexual , and transgender people . 
 case reports and anecdotal evidence suggest that transgender people have a disproportionate cancer burden , but without high - level evidence , health - care providers are sti ed in their ability to provide adequate guidance . 
according to a 2011 report by the us national center for transgender equality and the national gay and lesbian task force , transgender people frequently face discrimination by health - care providers . 
this is further underlined by a world report published in the lancet on august 21 , which documents how a lack of provider knowledge about transgender health in the usa might result in intrusive questioning and harassment . 
this can be complicated by the transgender people opting out of cancer screening and examinations because of emotional or physical distress associated with the discordance between their gender and their natal genitalia . disengagement from gender - oriented health care , for any reason , results in missed opportunities for cancer screening and diagnosis , and likely contributes to care disparities in this population . 
the use of oestrogen , progestin , and testosterone , to induce or sustain sex transitions , are often used in excessive doses and continued without medical guidancethe e ect of this on cancer development is unclear . 
additionally , actions considered preventative for certain gynaecological cancers in non - trans women , such as taking the birth control pill , might not be considered by trans men . 
 finally , as reported for lesbians , gay men , and bisexual people , transgender people are also more likely to smoke and drink alcohol , and have a greater chance of contracting hiv and human papillomavirus than the overall population , all of which contribute to an increased cancer risk . cancer care for transgender people is a growing concern and health - care services that are both respectful of this populations di erences , and also relevant to and inclusive of them are needed . 
moreover , research into how cancer a ects the transgender community , as well as how to prevent , screen , and treat cancer in this population , will improve cancer control . 
 the lancet oncology vol 16 september 2015 editorial for the paho report see new.paho.org / hq / index.php ? option = com_docman&task = doc_ download&gid = 16836&itemid = for more on tobacco content in video games see cancer and society page 237 for the welsh government campaign see uk / newsroom / healthandsocial care / 2012 / 120206smoking / ? lang = en for the british medical associations policy brie ng see images / smokinginvehicles_v3_ tcm41 - 210651.pdf for more on laws banning smoking in vehicles carrying children see news / pdf / prevention.pdf tobacco control : time to protect children on feb 8 , 2012 , the pan american health organization ( paho ) published a report on tobacco control measures for the americas summarising the progress made in the implementation of the who framework convention on tobacco control ( fctc )  . 
signed by 168 countries in 2005 , the fctc requires state parties to apply a series of policies and measures aimed at reducing tobacco consumption , preventing young people from beginning to smoke , and protecting non - smokers from second - hand smoke ( shs )  . 
 although a growing number of south american countries are adopting e ective tobacco control policies , the paho report recommends further measures , particularly increases in tobacco taxes and bans on tobacco advertising . 
 such bans have reduced the amount of tobacco imagery in traditional media channels , but indirect advertising through new media is increasing ; targeting technology that has a large youth following . 
protection of children from smoking should be placed at the forefront of political agendas and , encouragingly , several countries , both within and outside the americas , have challenged the tobacco companies about such practices in recent years . tobacco advertising is known to be e ective in enticing new customers , and as traditional markets have shrunk , tobacco companies have used more inventive and under hand means to promote their products , increasingly targeting the child and teen markets . 
for example , as reported by barrientos - gutierrez and colleagues in this issue of the lancet oncology , the prevalence of tobacco content in video games in the usa , canada , and mexico , increased from 08% in 2005 to 126% in 2011 in games that are rated appropriate for 10 - year - olds and older . 
 however , while the protection of teenagers from indirect increased , protecting tobacco advertising should be children from tobacco smoke itself , and its associated carcinogens , should be placed even higher up national political agendas . 
article 8 of whos fctc calls for parties to take action to provide protection from exposure to tobacco smoke , and surely emphasis should be placed on the youngest members of societies , who perhaps are the most vulnerable biologically and psychologically . both the us environmental protection agency and the international agency for research on cancer have classi ed shs as a de nitive cause of cancer . 
the presence of shs in enclosed spaces , such as homes and vehicles , can result in signi cant morbidity for children , and increased hospital visits and health - care expenditures . 
since no level of shs exposure has been shown to be safe , parties should expand the scope of smoke - free legislation to include other locations where evidence exists to support such bans . 
 measures to protect children are gaining momentum and on feb 6 , 2012 , an educational campaign to stop people smoking in cars when children are present was launched by the welsh government . 
legislation will be considered depending on the success of the 3 - year campaign , although scant details on how success will be measured , or how this legislation will be enforced , have been provided . 
indeed , laws prohibiting smoking in vehicles carrying children have already been adopted in south africa , mauritius , bahrain , and puerto rico , and in several regions of canada , australia , and the usa . 
 the welsh proposal might be in the spirit of fctc recommendations , but it could be argued that the use of the law to enforce and legislate in this manner is the start of a slippery slope of state sanctions against peoples rights and freedoms . 
 furthermore , a broad range of antismoking initiatives has proved popular among the general population and has substantially reduced the numbers of individuals who smoke indoors , thereby decreasing shs in private spaces . 
 societies must protect those groups that are most vulnerable , whilst maintaining an individuals freedom of choice , and many countries have made great strides to achieve this di cult balancing act . 
 the lancet oncology vol 13 march 2012 articles the sex hormone system in carriers of brca1 / 2 mutations : a case - control study martin widschwendter * , adam n rosenthal * , sue philpott , ivana rizzuto , lindsay fraser , jane hayward , maria p intermaggio , christopher k edlund , susan j ramus , simon a gayther , louis dubeau , evangelia ourania fourkala , alexey zaikin , usha menon , ian j jacobs summary background penetrance for breast cancer , ovarian cancer , or both in carriers of brca1 / brca2 mutations is disproportionately high . 
 follicular and luteal oestradiol and progesterone serum titres were grouped into quartiles and odds ratios were calculated with logistic regression . findings follicular phase endometrial thickness of carriers of the mutations adjusted for age and day of the menstrual cycle was higher ( odds ratio [ or ] 111 , 95% ci 103120 ; p = 00063 ) and luteal phase endometrial thickness lower ( 090 , 083098 ; p = 0027 ) than for women negative for the mutations . 
median luteal phase titres of progesterone were 121% higher ( p = 000037 ) in carriers than in women negative for the mutations , and for oestradiol were 33% higher ( p = 0007 ) ie , 59% of carriers had concentrations of serum progesterone that would have been in the top quartile of concentrations in the control group ( or 80 , 95% ci 215257 ; p = 0008 )  . interpretation carriers of brca1 / brca2 mutations are exposed to higher titres of oestradiol and progesterone known risk - factors for breast cancer . 
our ndings could not be explained by di erential contraceptive pill use . funding eve appeal , european union , cancer research uk , and us national institutes of health . introduction in all inherited cancer syndromes the germline mutation is thought to have a so - called local e ect in an organ that is predisposed to the development of cancer , because these mutations do not cause cancers in all organs . 
for example , the increased cancer risk in carriers of the brca1 and brca2 mutations is predominantly that of breast cancer , ovarian cancer , or both.1 these mutations are thought to cause cancer via a defect in dna damage response or in the dna repair pathway.2 however , this defect does not explain the organ - speci c cancer penetrance . 
that removal of both ovaries and fallopian tubes reduces not only the risk of ovarian but also breast cancer3 implicates a systemic dysregulation of hormone production in carriers of the mutation , which a ects both the mllerian epithelium , as the cell of origin for ovarian cancer , 4 and breast epitheliuevidence from preclinical models suggests that both hormone production and hormone sensitivity of end organs is altered in carriers of the brca1 mutation . 
studies in animals57 showed that mice carrying a brca1 mutation in the steroid - hormoneproducing granulosa cells had a longer pro - oestrus phase , corresponding with the oestrogen - dominant follicular phase of the human menstrual cycle . 
also , the insulin - like growth factor system has a fundamental role endometrial biology , acting via autocrine and paracrine mechanisms.8 there are strong interactions between the factor and brca1 signalling insulin - like growth pathways , which also involve oestrogen signalling ; 9 hence , it is possible that the endometrium of carriers of the brca1 mutation has altered sensitivity to hormones . cyclical change in oestradiol and progesterone titres alters endometrial thickness and menstrual bleeding in premenopausal women . 
because many women in the study had undergone clinical genetic for brca1 / 2 mutations , we had a cohort of women known to carry the mutation and a cohort known to be negative for the mutation to compare . 
 to establish the mutation status of these women , highthroughput next generation sequencing provided the fastest and most cost - e ective method of rapidly detecting carriers of the mutations , albeit with potentially lower sensitivity than clinical testing , which in the uk uses a combination of sanger sequencing ( including limited ashkenazi mutation screening where appropriate ) and multiplex ligation probe ampli cation . methods participants after ethical approval ( eastern mrec 97 / 5 / 007 ) , ukfocss recruited from 44 uk regional centres . 
 between june , 2002 , and september , 2010 , women older than 35 years , at an estimated minimum 10% lifetime risk of ovarian cancer based on family history or predisposing germline gene mutations ( appendix ) were recruited and screening data and outcomes were collected prospectively . 
so far , about 25% of the study population have undergone clinically initiated testing for brca1 and brca2 mutations ( either before or after recruitment )  . after ethical approval ( joint university college london / university college london hospital ethics committee , ref 06 / q0505 / 102 ) , we selected all premenopausal ukfocss participants with no previous or subsequent history of cancer ( to avoid including women on hormonal therapy or women with a subclinical cancer , which could have triggered an altered hormonal environment and which could have confounded our analyses ) and no intrauterine device . procedures ovarian cancer screening was done with transvaginal sonography to assess ovarian morphology and serum ca125 tumour marker measurement . 
all centres scanned study participants and all scans were done by sonographers , radiologists , or gynaecologists approved by the uks national health service ( nhs ) , employed by the local hospital for gynaecological scanning , and subject to local nhs quality control . 
participants were included if they matched our inclusion criteria and had provided a dna sample . oestradiol and progesterone were measured with automated immunoassays on the elecsys 2010 analyser ( roche diagnostics gmbh , mannheim , germany )  . 
the progesterone intra - assay cv is 1527% and interassay cv is 3754% . statistical analysis endometrial thickness for each group was averaged for each day of menstrual cycle and smoothed using the averaging running window of 5 days . 
on start and end days of the menstrual cycle the dependencies were prolongedeg , for day 1 , endometrial thickness was averaged over days 30 , 31 , 1 , 2 , and 3 . 
to quantify di erences we focused on days 1014 and days 2126 ( because these were the times in the cycle when di erences were most pronounced ) , and calculated the area under the curve ( auc )  . 
to construct the distributions for aucs , the endometrial thickness values were bootstrapped : for each cycle day the thickness value was sampled with replacement , then the obtained dependence was averaged using a window of 5 days and the auc was calculated for the obtained dependence between days 1014 and 2126 . 
the odds ratios ( ors ) for brca status were obtained for endometrial thickness , treated as a continuous predictor variable , and adjusted in the logistic regression for age and the speci c menstrual cycle day as continuous variables . follicular and luteal oestradiol and progesterone serum titres were grouped into quartiles and ors were calculated with logistic regression . 
therefore the only di erence between b and a is that the former would have had a lower a - priori risk of being mutation carriersthis explains the lower prevalence of mutations recorded in b versus a . 
 however , there was no di erence in ultrasound methods , data collection , sample collection , or storage for these women , so this is not a source of bias . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results 2808 endometrial - thickness measurements and associated last menstrual period dates were available from 1460 eligible women , including 1573 endometrial thickness measurements in women negative for both mutations , 203 in carriers of bcra1 , and 190 in carriers of brca2 ( baseline data shown in the appendix )  . 
in view of this statistically similar endometrial thickness pattern in carriers of the mutations , we combined these groups , and noted clear di erences between the combined carrier group and the group negative for mutations ( gure 2 and table 2 )  . 
in the follicular phase , the carrier groups endometrial thickness was signi cantly higher , whereas thickness was signi cantly lower than that of non - carriers , even after using logistic regression analysis and adjusting for age and menstrual cycle day . 
to assess whether a womans knowledge of her mutation status might a ect the results ( eg , by changing her lifestyle in an attempt to minimise her cancer risk ) , we separately analysed the 728 women in the next generation sequencing group who did not know their mutation status during the trial . 
to be certain that the endometrial thickness di erences were not due to di erential oral contraceptive pill use , we analysed the 1318 endometrial thickness scans for which the women had reported no oral contraceptive pill use in the decade the scan was done ( table 1 )  . 
again , we noted the same endometrial thickness patterns as before ( appendix ) , with higher follicular phase endometrial thickness and lower luteal phase endometrial thickness in carriers of the mutations than for women negative for the mutations . luteal phase endometrial the 1228 vol 14 november 2013 articles brca1 and 2 negative brca1 mutation brca2 mutation brca1 and 2 negative brca1 and 2 mutation the di erences in endometrial thickness between carriers and those negative for the mutations could be a consequence of di erent hormonal sensitivity of the target tissue ( ie , the endometrium ) in carriers of the mutations , triggered by di erent titres of the steroid hormones known to regulate endometrial biology , or a combination of the two . 
although it is di cult to assess hormonal sensitivity directly , to assess the triggering threshold we analysed oestradiol and progesterone in stored serum samples from all premenopausal carriers of the mutations who provided samples between days 1014 ( follicular phase ) and 2126 ( luteal phase ; n = 59 , mean age 406 years , 70 samples ) , and all women negative for the mutations ( n = 283 , mean age 435 years , 339 samples )  . 
 progesterone titres during day 1014 were not measured in all women because pilot data in 38 carriers and 44 controls showed such low titres ( median 127 nmol / l in carriers and controls ) that no signi cant di erences would become apparent on testing all available samples . 
 median luteal phase titres of progesterone were 121% higher ( p = 000034 ) in carriers than in women negative for the mutations , and oestradiol titres were 33% higher ( p = 0007 ) ie , 59% of carriers had concentrations of serum progesterone that would have been in the top quartile of concentrations in the control group ( or 80 , 95% ci 215257 ; p = 0008 ; appendix , gure 3 )  . discussion in cyclical our ndings show clear di erences endometrial thickness in carriers of brca1 / 2 mutations compared with wild - type controls . 
our cohort of well matched premenopausal carriers and controls with combined endometrial thickness information , and serum samples with known menstrual cycle data , was ideal for testing the hypothesis that the organspeci c cancer penetrance in carriers is due to hormonal dysregulation . 
 we speculate that the high luteal phase oestradiol we recorded in carriers triggers increased expression of progesterone receptors , 11 thus potentiating any possible mutagenic e ect of the higher luteal progesterone . 
our ndings support those from studies in mice carrying a brca1 mutation in ovarian granulosa cells.6 , 7 although data on endogenous premenopausal progesterone exposure or = 111 * ( 95% ci 103120 ) p = 00063 or = 090 * ( 95% ci 083098 ) p = 0027 menstrual cycle ( days ) figure 2 : endometrial thickness as a function of the menstrual cycle ( a ) endometrial thickness calculated from 1573 transvaginal ultrasound scans from 754 women negative for both mutations , 203 scans from 116 carriers of the brca1 mutation , and 190 scans from 112 carriers of the brca2 mutation . 
 ( b ) endometrial thickness in 754 women negative for both mutations ( 1573 scans ) and the combined 228 women who were carriers of either mutation ( 393 scans )  . 
 * adjusted for menstrual cycle day and age . and cancer risk is less extensive and less conclusive , 12 postmenopausal exogenous progesterone exposure is a well established risk factor for breast cancer.11 , 1315 we were recently part of a collaborative report suggesting that progestogens cause breast cancer by inducing expression of the receptor activator of nf - b ligand ( rankl ) , and that deleting the receptor for this ligand delays the onset of progestogen - driven breast cancers.16 there is already an vol 14 november 2013 1229 articles area under curve p value panel : research in context days 1014 of cycle days 2126 of cycle < 00001 < 00001 separate brca analysis brca1 mutation brca2 mutation brca1 / 2 negative combined brca analysis brca1 / 2 mutated brca1 / 2 negative auc = area under curve . 
n = number of volunteers . table 2 : endometrial thickness as a function of menstrual cycle in women by brca1 and brca2 mutation status p = 00074 1000 p = 000034 systematic review we searched pubmed for studies on brca mutation and alterations in the female premenopausal reproductive hormone system published in english between sept 1 , 1993 , and feb 28 , 2013 . 
we established that studies in animals showed aberrant hormonal regulation upon loss of brca1 in granulosa cells and that premenopausal surgical resection of the ovaries in women carrying the brca1 or brca2 mutation led to a substantial reduction in the risk of breast cancer.3 systemic endocrine e ects of brca1 or brca2 mutations have not previously been assessed in humans . interpretation our ndings suggest that brca1 / 2 germline mutations are driving carcinogenesis only in part via altered molecular pathways ( eg , those involved in dna repair ) in the organ at risk , and that brca1 / 2 - associated changes in the endocrine system are additional factors . 
potential agents for these trials include selective oestrogen or progesterone receptor modulators , and the anti - rankl ( receptor activator of nf - b ligand ) antibody denosumab ( currently used for osteoporosis treatment , but known to block the downstream carcinogenic e ects of progestogens )  . negative brca1 / 2 mutation negative brca1 / 2 mutation figure 3 : serum progesterone and oestradiol analysis during luteal phase of the menstrual cycle boxplots with horizontal line show 25% , 50% , and 75% quartiles . 
in conjunction with data that show the potential of a progesterone antagonist to prevent brca1 - mediated mammary tumorigenesis in mice , 17 our ndings provide an additional rationale for treatment that interferes with progesterone signalling to prevent breast cancer in carriers of brca1 / brca2 mutations . 
this nding suggests that the endometrium of carriers might be more sensitive to oestrogen - receptor agonists . for ovarian cancer , oestrogen replacement usage21 and obesity ( a hyperoestrogenic state ) 22 are established epidemiological risk implicating hormonal factors dysregulation in its pathogenesis . 
our data , suggesting higher oestradiol titres in the luteal phase of the menstrual cycle in women who are carriers of the brca1 / 2 mutations compared with women negative for the mutations supports this hypothesis . 
we speculate that the higher titres of progesterone with concordant reduced endometrial thickness recorded in the luteal phase in the carrier group compared with the control group might explain why the penetrance for the third triggered cancernamely endometrial hormonally cancerin carriers is much lower than that for ovarian and breast cancer ; it is well recognised that progestogens suppress endometrial proliferation , 23 resulting in a thinner endometrial thickness and lower lifetime risk of endometrial cancer.24 1230 vol 14 november 2013 articles our study has certain limitations . 
furthermore , in view of the age of the cohort ( all were > 35 years ) and their known increased risk of breast cancer , it is probable the proportion using the contraceptive pill at the time of sample donation would have been even lower than the data above . 
most importantly , excluding women with unreported pill use and those known to have taken the pill in the same decade as the scan did not reduce the statistical signi cance of the endometrial thickness di erences between carriers and controls . the control group could have included participants that carry brca1 / 2 mutations who were missed using our next generation sequencing mutation - detection methods ( eg , mutations in regions of low sequence coverage or large genomic rearrangements )  . 
although it is not possible to estimate the frequency of missed mutations , the individuals screened were una ected and therefore had at most a 50% chance of inheriting a germline mutation even if it were present in their family . 
any mutation carriers in the screen - negative group would bias our nding towards the null , suggesting that our study has underestimated rather than overestimated the strength of the recorded e ects . we had insu cient numbers of scans with last menstrual period dates of a cycle length greater than 28 days to draw any conclusions about whether carriers of brca1 / brca2 mutations might have a longer menstrual cycle than women negative for the mutations , as was evident in the previously described mouse model.57 if this were the case , then we speculate that longer cumulative exposure , and the observed higher absolute titres of progesterone and to a lesser extent oestradiol , might contribute to the excess breast cancer risk of carriers of the mutations . our study cannot address whether endometrial thickness and hormone titres are respectively a marker and e ector of breast cancer risk within a brca1 / 2mutant population . 
as a result addressing the question as to whether altered endometrial thickness and steroid hormone titres in premenopausal women are markers for subsequent breast cancer risk or not would be di cult to do . 
it would need a substantial prospective long - term study of pre menopausal brcacarriers who were unwilling to undergo risk - reducing surgery but willing to be followed up for decades . 
our ndings suggest that sex steroids are one of the major drivers for development of breast cancer in this population . we deliberately excluded patients who had a previous diagnosis of breast or ovarian cancer because they could have been on antiendocrine therapy or chemotherapy , which would have altered their ovarian function and biased our ndings . 
it is well known that sex steroids are locally produced within invasive but also within non - invasive breast carcinoma , 25 which might not have been clinically apparent at the time of sample donation . 
hence we decided a priori not to include women with a diagnosis of breast or ovarian cancer subsequent to sample donation to avoid any bias that would favour the hypothesis of an aberrant endocrine system being associated with cancer development in high - risk women . 
however , despite this , we have noted hormonal changes that would be expected to increase breast cancer risk ( ie , raised oestradiol and progesterone in carriers vs controls )  . 
 furthermore , because of the young age of the study group ( all were premenopausal ) , most have not yet reached the age at which their breast cancer would be likely to occur , so most of the excess breast cancer risk of the study population has yet to accrue . 
excluding the small number of women who we know developed breast cancer subsequent to sample donation would be likely to minimise di erences between carriers and controls , making our ndings more compelling . to improve statistical power , we combined carriers of brca1 and brca2 mutations into a single study group . 
 although we acknowledge that it is possible that there are biological di erences between these groups relevant to our investigation , we did not identify statistical di erences between them with respect to endometrial thickness or hormone titres ( appendix )  . 
furthermore , gure 2 clearly shows that both groups have a similar pattern of higher follicular phase endometrial thickness and lower luteal phase endometrial thickness compared with women negative for the mutations . although we have in e ect analysed multiple crosssectional data rather than longitudinal data , we have still identi ed statistically signi cant di erences between carriers and controls . 
we feel such a study would be logistically challenging and recruitment for it would be extremely di cult . carriers and controls , vol 14 november 2013 1231 articles for more on the eve appeal see the control group was not a random sample from the general population , but rather was deliberately selected for high familial risk of ovarian cancer ( to minimise any di erences between mutation carriers and controls )  . 
however , their shared increased ovarian cancer risk makes them the most appropriate control group to compare with carriers of brca1 / brca2 mutations . in conclusion , our ndings provide novel insights into the high penetrance for breast cancer ( via higher progesterone and oestrogen titres ) and also possibly ovarian cancer ( via higher oestrogen titres and potentially lower titres of anti - mllerian hormone26 ) in carriers of brca1 / brca2 mutations . 
 con icts of interest we declare that we have no con icts of interest . acknowledgments this work was funded by the eve appeal and the european unions seventh framework programme ( fp7 / 2007 - 2013 ) under grant agreement number 305428 ( project epifemcare ) and done at uclh / ucl , which received a proportion of its funding from the department of health nihr biomedical research centres ( brc ) funding scheme . 
 we thank david conti for his help in the bioinformatic analysis of next generation sequencing data . published online august 6 , 2019 s1470 - 2045 ( 19 ) 30530 - 3 published online july 30 , 2019 s1470 - 2045 ( 19 ) 30521 - 2 correction to lancet oncol 2019 ; 20 : 114859 correction to lancet oncol 2019 ; 20 : 121125 bonvalot s , rutkowski pl , thariat j , et al . 
 nbtxr3 , a first - in - class radioenhancer hafnium oxide nanoparticle , plus radiotherapy versus radiotherapy alone in patients with locally advanced soft - tissue sarcoma ( act.in.sarc ) : a multicentre , phase 23 , randomised , controlled trial . 
 lancet oncol 2019 ; 20 : 114859in this article , the funder pharmaengine , inc , was inadvertently omitted and has now been added to the funding line in the summary and to the acknowledgments . 
a repeated sentence has been deleted from the fifth paragraph of the statistical analysis section of the methods , and some minor typographical errors have been corrected throughout the paper . 
 these corrections have been made to the online version as of sept 2 , 2019 . correction to lancet oncol 2019 ; 20 : 117182 nen nr , reisel d , leimbach a , et al . 
the following sentence has been added to the figure 4 caption : sdi quintiles are ordered from high to low sdi quintile , and gbd super - regions are alphabetically ordered . 
the next sentence should read : country order selected by total absolute dalys ; countries with the greatest total absolute dalys , of the fifty most populous countries in the world , are listed first . 
this correction has been made to the online version as of aug 6 , 2019 . correction to lancet oncol 2019 ; 20 : 127385 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
lancet oncol 2019 ; 20 : 127385in this article , data ( hazard ratios , 95% cis , and p values ) in the following sentence on p 1279 have been corrected : in women with stage iii disease , 5 - year overall survival was 838% ( 95% ci 784895 ) with chemoradiotherapy versus 820% ( 95% ci 765877 ) with radio therapy alone ( hr 084 [ 95% ci 052138 ] ; p = 050 ) , and 5 - year failure - free survival was 813% ( 95% ci 747863 ) with chemoradiotherapy versus 773% ( 95% ci 705827 ) with radiotherapy alone ( hr 087 [ 95% ci 056136 ] p = 054 ; appendix p 8 )  . 
on p 1282 , the same data ( hazard ratios and 95% cis ) in the following sentence have also been corrected : for women with stage iii endometrial cancer , combined adjuvant treatment yielded only a small absolute improvement of 2% ( hr 084 ; 95% ci 052138 ) in 5 - year overall survival and of 4% ( 087 ; 056136 ) in failure - free survival . 
 these corrections have been made to the online version as of sept 2 , 2019 , and the printed version is correct . correction to lancet oncol 2019 ; 20 : e41733 herrera fg , irving m , kandalaft le , coukos g . 
 this correction has been made as of july 30 , 2019 . correction to lancet oncol 2019 ; 20 : e50321 spence d , dyer r , andall - brereton g , et al . 
 lancet oncol 2019 ; 20 : e50321the affiliations of authors dingle spence and m austin argentieri have been corrected in the online version as of sept 2 , 2019 . vol 20 september 2019 e468 corrections instead be invested in smarter clinical trial designs that can answer relevant clinical questions , such as whether sequencing of drugs is better than combination therapies , or defining the optimal duration of adjuvant treatment . 
 fortunately , an embarrassment of riches . juan martin - liberal melanoma , sarcoma and genitourinary tumors unit , institut catal doncologia ( ico ) lhospitalet , 08907 barcelona , spain ; and molecular therapeutics research unit ( uitm ) , vall dhebron institute of oncology ( vhio ) , 08035 barcelona , spain jmartinliberal@gmail.com i have received lecture fees and travel grants from roche , novartis , msd , and bristol - myers squibb . luke jj , flaherty kt , ribas a , long gv . 
overall survival in patients with braf - mutant melanoma receiving encorafenib plus binimetinib versus vemurafenib or encorafenib ( columbus ) : a multicentre , open - label , randomised , phase 3 trial . 
gb / document_library / summary_of_opinion_ - _initial_authorisation / human / 004579 / wc500252668.pdf ( accessed sept 5 , 2018 )  . another step towards improving oncofertility counselling of young women with hodgkins lymphoma possible chemotherapy - induced premature ovarian insufficiency is of great concern for female premenopausal patients with cancer . 
therefore , appropriate counselling on the risk of premature ovarian insufficiency is now mandatory in all countries.1 , 2 oncofertility counselling is of particular importance for women who have hodgkins lymphoma , who are often diagnosed at a young age . 
however , the counselling of these women can be quite complex because of the paucity of accurate data to estimate the effect of different chemotherapy regimens on their gonadal function . 
previous studies in this setting were mostly retrospective or relied only on menstrual function after treatment to define premature ovarian insufficiency , a measure that is not an optimal surrogate for assessing gonadal damage associated with treatment . in the lancet oncology , richard a anderson and colleagues3 report important results for helping physicians informing premenopausal women with advanced hodgkins lymphoma about the risk of chemotherapyinduced premature ovarian insufficiency associated with doxorubicin , bleomycin , vinblastine , and dacarbazine ( abvd ) or avd , or bleomycin , etoposide , doxorubicin , cyclophosphamide , vincristine , procarbazine , and prednisone ( beacopp ) chemotherapy.3 in this substudy , done within the rathl trial ( nct00678327 ) , biomarkers of ovarian function during and up to 3 years after chemotherapy were assessed in women younger than 45 years at the time of diagnosis . 
specifically , 67 participants were monitored for serum antimllerian hormone concentrations and 321 participants for follicle - stimulating hormone concentrations despite a few limitations , including the small sample size of the antimllerian hormone analysis , particularly of those who were treated with beacopp , and the lack of collection of participant information from the main rathl cohort that could have had a potential effect on outcomes ( eg , use of hormonal contraceptives , previous fertility preservation procedures , and menstrual status after chemotherapy ) , this study provides more precise information than previous reports to counsel women with hodgkins lymphoma on gonadal damage induced by abvd , avd , or beacopp . 
 first , the study confirms that both the type of chemotherapy and patients age at the time of treatment remain the two major determinants of risk of premature ovarian insufficiency for all patients with cancer.4 , 5 antimllerian hormone concentrations decreased sub stantially during both chemotherapy regimens ; however , while antimllerian hormone published online september 13 , 2018 s1470 - 2045 ( 18 ) 30562 - x see articles page 1328 1264 vol 19 october 2018 comment concentrations recovered to before treatment levels in those patients given abvd or avd by 1 year after treatment , little recovery of antimllerian hormone concentrations was treatment with beacopp.3 in anderson and colleagues study , age was shown to be a crucial factor , with increased risk of chemotherapy - induced premature ovarian insufficiency after both regimens in women aged 35 years and older at the time of diagnosis . seen after second , these results highlight the need for a standardised definition of premature ovarian insufficiency . 
different endpoints ( menstrual function only , ovarian biomarkers onlyas in the present studyor a combination of the two ) and timing of its assessment ( ranging from a few months up to several years after chemotherapy ) have been used to define chemotherapyinduced premature ovarian insufficiency . 
 guidelines suggest use of a composite endpoint that includes both amenorrhoea and a hormone profile after menopause , 6 , 7 and assessing chemotherapy - induced pre mature ovarian insufficiency at least 2 years after the end of treatment.7 in the present study , recovery of ovarian function , as measured by follicle - stimulating hormone concentrations , occurred by 1 year after the end of treatment for most patients ( 75% treated with abvd or avd and 33% treated with beacopp ) , but recovery can also happen during the second year ( 18% of participants treated with abvd or avd and 50% with beacopp ) with little chance of recovery thereafter . 
these results support the expert opinionbased indication to assess ovarian function after chemotherapy no earlier than 2 years after treatment completion.7 third , although this study provides further evidence on the role of antimllerian hormone as a biomarker of gonadotoxicity , the clinical utility of its assessment during treatment and subsequent follow - up remains to be fully determined . 
as shown in other studies , 8 , 9 both resumption of menstrual function and spontaneous conception can be observed low concentrations of antimllerian hormone.8 , 9 similarly , in anderson and colleagues study , 3 some pregnancies were observed in women with very low antimllerian hormone levels . 
hence , the best predictor of infertility in cancer survivors remains to be identified . in women with finally , this study raises the crucial issue of discussing the possibility of reducing the risk of premature ovarian insufficiency.1 , 2 preservation of ovarian function ( ie , reducing the risk of chemotherapy - induced premature ovarian insufficiency ) should be distinguished from preservation of fertility ( ie , improving the chances of pregnancy after treatment ) and can be considered of important value also by women without childbearing desire . 
while cryopreservation of gametes is the first option to preserve fertility , the use of temporary ovarian suppression with gonadotropin - releasing hormone agonists during chemotherapy can now be offered for ovarian function preservation in patients with breast cancer , but its efficacy has not yet been shown in patients with hodgkins lymphoma.9 , 10 the results of anderson and colleagues study highlight the importance of discussing access to these options in women older than 35 years , irrespective of chemotherapy type , and among candidates to the beacopp regimen , irrespective of their age . 
very young women undergoing abvd or avd chemotherapy probably do not need to access these options , but they could be proposed later in life if additional treatments are required . results from the ovarian function biomarker analysis ongoing within the ahl 2011 trial ( nct01358747 ) are awaited to provide further evidence on the gonadotoxicity of beacopp chemotherapy in premenopausal women with hodgkins lymphoma . * matteo lambertini , isabelle demeestere breast cancer translational research laboratory , department of medical oncology , institut jules bordet ( ml ) and research laboratory on human reproduction , fertility clinic , cub - hpital erasme ( id ) , universit libre de bruxelles ( ulb ) , brussels 1000 , belgium matteo.lambertini85@gmail.com we declare no competing interests . 
j clin oncol 2013 ; 31 : 23139 . vol 19 october 2018 1265 comment published online september 10 , 2018 s1470 - 2045 ( 18 ) 30579 - 5 see articles page 1338 lambertini m , campbell c , bines j , et al . 
no evidence for the benefit of gonadotropin - releasing hormone agonist in preserving ovarian function and fertility in lymphoma survivors treated with chemotherapy : final long - term report of a prospective randomized trial . 
gonadotropin - releasing hormone agonists during chemotherapy for preservation of ovarian function and fertility in premenopausal patients with early breast cancer : a systematic review and meta - analysis of individual patient - level data . 
 camrelizumab for nasopharyngeal carcinoma : a new hope ? wenfeng fang and colleagues1 report on two phase 1 studies of the programmed cell death - 1 ( pd - 1 ) inhibitor , camrelizumab ( shr - 1210 ) , as a treatment for patients with recurrent or metastatic nasopharyngeal carcinoma . 
 the more interesting findings are the preliminary antitumor activity of camrelizumab in both settings : 31 ( 34% ; 95% ci 2444 ) of 91 patients who received previous treatment achieved an overall response with camrelizumab monotherapy ( two patients had a complete response ) and 20 ( 91% ; 7797 ) of 22 patients with the combination of camrelizumab and chemotherapy as first - line treatment ( one patient had a complete response )  . 
the keynote - 028 study2 showed that seven ( 26% ; 95% ci 111463 ) of 27 patients with previously treated , advanced disease achieved an objective response with pembrolizumab . 
the nci - 9741 trial3 showed that nine ( 205% ; 95% ci 98353 ; one complete repsonse ) of 44 patients with previously treated recurrent or metastatic naso pharyngeal carcinoma international studies achieved an objective response with nivolumab . 
both keynote - 028 and nci - 9741 are including 63% and 822% asian patients , respectively ; whereas the current study by fang and colleagues1 was done in an endemic chinese population . 
the proportion of who type 2 or 3 tumours in keynote - 028 was 667% , 822% in nci - 9742 , and 82% in the camrelizumab monotherapy trial of the current study . 
in terms of patient selection , keynote - 028 only included patients with programmed cell death ligand - 1 ( pd - l1 ) - positive tumours , whereas both nci - 9742 and the current study enrolled patients with unselected histologies . 
in nci - 9742 , 40% of patients had pd - l1 - positive tumours , which was associated with an improved response ( six [ 33% ] of 18 patients ) compared with pd - l1 - negative tumours ( three [ 13% ] of 23 patients )  . 
pd - l1 positivity also appears to be predictive of response to pd - 1 inhibitors in other head and neck squamous cell carcinomas.4 , 5 pd - l1 status was not reported by fang and colleagues in the current study . 
this outcome might suggest that previous priming with ipilimumab could improve the 1266 vol 19 october 2018 comment published online august 8 , 2018 s1470 - 2045 ( 18 ) 30498 - 4 see articles page 1159 increasing incidence of cancer in children and competing risks the automated childhood cancer information system ( accis ) has been registering data on cancer occurrence from birth to age 20 years in most european countries since the 1970s . 
in the lancet oncology , eva steliarova - foucher and colleagues1 report the latest accis data analysis trends for the period 19912010 for malignant neoplasms in children aged 014 years and adolescents aged 1519 years . 
first , cancer incidence in children aged 014 years has gradually increased over the 19912010 period.1 increasing incidence was observed for all cancers ( 054% ( 95% ci 044 to 065 ) per year ) , leukaemia ( 066% [ 048 to 084 ] per year ) , lymphoma ( 026% [ 001 to 054 ] per year ) , cns malignant tumours ( 049% [ 020 to 077 ] per year ) , and other cancers ( 056% [ 040 to 072 ] per year )  . 
second , for all five cancer categories investigated , incidence increases were similar in all four regions . remain the accis data reinforce the notion that the slow but steady increase in the incidence of many childhood cancers reported since the 1970s is real , and that it is particularly notable for leukaemia.24 unfortunately , epidemiological studies so far have not identified clear risk factors for childhood cancer . 
however , relating the accis data to the tremendous changes in environmental , living , socioeconomic , and public health conditions in european countries after world war 2 might provide clues as to the nature of these reasons . 
if improvements in medical imaging technology were the reason underlying the increased incidence trends of tumours of the cns , then a lower incidence of these tumours should have been observed in the early 1990s in east europe compared with west europe , with a catch up in incidence afterwards . 
however , incidence and incidence trends observed trends from 1991 to 2010 were about the same in east europe and west europe.1 another contrast across european regions concerns the use of pesticides in agriculture . 
in 2014 , the quantities of pesticide sales per capita were about three times greater in spain , italy , and france than in sweden or the uk.5 if increasing cancer incidence trends were due to pesticides , dissimilarities in incidence trends for leukaemia and lymphoma would be expected between european regions , which was not the case.1 a search for marked changes in health events specific to all european children rapidly identifies the dramatic decreases in mortality of children younger than 15 years after world war 2 . 
for example , infant mortality in europe ranged from 160775 deaths per 1000 newborns in 1960 and dropped to 2398 deaths per 1000 newborns in 2010a decrease of 44% per year on average.5 this phenomenon leads to the hypothesis that the death of some children before they reached a certain age precluded the occurrence of cancer by that age . 
death would represent a competing risk ( or event ) in the sense that cancer can no longer occur after death.6 furthermore , children who would have died could also have been at higher risk of cancer for two possible reasons . 
these hypotheses assume that if a child escapes death either because he or she has been protected against potentially deadly diseases ( eg , by vaccination or improved living conditions ) or has survived its occurrence ( eg , because of efficient therapy ) , then the risk of cancer occurrence would be greater in this child than in other children . 
this hypothesis could explain why the peak incidence of leukaemia has shifted towards younger ages over time.4 , 7 steadily decreasing mortality in the months following birth would increase the number of younger children at higher risk for leukaemia . the competing risk hypothesis essentially rests on ecological observations . 
lancet 2004 ; 364 : 2097105 . bevacizumab therapy for recurrent gliomas : another disappointment ? in their article in the lancet oncology , martin van den bent and colleagues1 report on their clinical trial of bevacizumab in the treatment of recurrent grade ii and iii gliomas , and they report the effects of this treatment on overall survival , progression - free survival , quality of life , toxicity , and neurocognitive function . 
 their study was designed as a phase 2 trial and therefore was not powered to show a definite advantage of bevacizumab in these patients , although a high number of patients ( n = 155 ) were enrolled and randomly allocated to the two treatment groups ( temozolomide plus bevacizumab or temozolomide monotherapy )  . 
 to our knowledge , this is the largest study on the use of bevacizumab , with the highest quality data , in patients with recurrent who grade ii and iii gliomas . bevacizumab was previously regarded as a promising new chemotherapeutic drug for the treatment of gliomas . 
 several large trials that used considerable resources were therefore done , although the findings from the study by van den bent and colleagues is mostly in line with the available data on bevacizumab in the treatment of gliomas . 
the authors found no evidence of improved overall survival with bevacizumab and temozolomide combination therapy versus temo zolomide monotherapy : overall survival at 12 months was achieved by 44 ( 61% [ 80% ci 5369 ] ) of 72 patients in the monotherapy group and 38 ( 55% [ 4769 ] ) of 69 in the combination group . 
the results of the study by van den bent and colleagues are disappointing and continue the pattern of failed clinical trials of bevacizumab , which was thought to be a silver bullet in the treatment of intrinsic brain tumours , but which now seems confirmed to be an ineffective chemotherapeutic drug for this indication.24 validated treatment options for recurrent intrinsic brain tumours are scarce . 
although surgery has become more aggressive in the past 1015 years ( an approach that is not supported by robust evidence ) , potent and effective therapeutic drugs for treatment of recurrent tumours are not available.5 , 6 notably , bevacizumab treatment provided no benefit in the secondary efficacy outcomes of this trial , and side - effects were more common in patients receiving bevacizumab . 
despite its failure to improve overall survival , bevacizumab is still used as an adjunct therapy because of its supposed anti - oedematous effects and reported improvements in progression - free survival of patients with glioblastomas.7 it is of note that these anti - oedematous effects and improvements to progression - free survival were only measured by mri ; however , molecular imaging methods such as aminoacid positron emission tomography scans could reveal different tumour progression or overall response to treatment than is shown by mri alone.8 if bevacizumab has a substantial effect on tumour progression and oedema in patients with glioblastoma that outweighs its side - effects , this effect was not shown in patients with who grade ii and iii gliomas in the study by van den bent and colleagues . 
there are several possible published online august 13 , 2018 s1470 - 2045 ( 18 ) 30601 - 6 see articles page 1170 vol 19 september 2018 1137 comment re ection and reaction panel : concepts applicable to various histologies ( excluding small - cell carcinoma , germ - cell tumors , and lymphoma ) in the analysis of brain metastasis trials involving radiosurgery and adjuvant wbrt patients eligible for radiosurgery have brain metastases less than 34 cm in diameter adjuvant wbrt probably decreases the risk of distant brain tumour recurrence for most histologies including melanoma adjuvant wbrt probably does not improve overall survival adjuvant wbrt is associated with a greater decline in learning and memory function at 4 to 6 months in a heterogenous population of primary cancer types wbrt causes acute fatigue and hair loss wbrt frequently delays the prompt initiation of systemic therapy a substantial proportion of patients with brain metastases do not need adjuvant wbrt in their lifetime a substantial proportion of patients with brain metastases initially treated with radiosurgery can be salvaged with additional radiosurgery delaying , or obviating the need for giving wbrt completely radiosurgery , like wbrt , can be used to address uncontrolled brain metastases in patients seeking to enroll on and qualify for clinical trials who would be otherwise excluded di culty inherent in accruing su cient numbers of patients to a site - speci c brain metastasis trial . 
however , there are common elements and fundamental concepts that seem to be valid across various histologies ( excluding small - cell carcinoma , germ - cell tumours , and lymphoma ) involving in the analysis of brain metastasis trials radiosurgery and adjuvant whole brain radiation therapy ( wbrt ; panel )  . 
perhaps in the future , the combination of advanced functional neuro - imaging and gene - expression pro ling techniques will enable us to identify better the subgroup of patients who are at greatest risk for developing distant brain metastases . 
the current preference and practice of medical oncologists in the department of melanoma medical oncology at md anderson cancer is to refer patients with oligo brain metastases to undergo radiosurgery alone to facilitate rapid enrolment on systemic therapy protocols . 
it is agreed that specialised brain metastasis trials focused exclusively on melanoma patients would help further elucidate the respective roles of surgery , radiosurgery , adjuvant wbrt , and systemic treatments . 
a phase 2 eastern cooperative oncology group ( e 6397 ) study of radiosurgery alone in patients with one to three brain metastases from renalcell carcinoma , melanoma , or sarcoma concluded that delaying wbrt might be appropriate for some subgroups of patients.2 in the meantime , the management of patients with melanoma brain metastases relies on the extrapolation of data gleaned from existing reports on brain metastasis , rst - hand knowledge of the patient history , and multidisciplinary discussion to provide the best treatment plan individualised for each patient . eric l chang * , patrick hwu department of radiation oncology ( elc ) , department of melanoma medical oncology ( ph ) , the university of texas md anderson cancer center houston , tx , usa echang@mdanderson.org the authors declared no con icts of interest . chang el , wefel js , hess kr , et al . 
phase ii trial of radiosurgery for one to three newly diagnosed brain metastases from renal cell carcinoma , melanoma , and sarcoma : an eastern cooperative oncology group study ( e 6397 )  . 
radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
lancet oncol 2010 ; 11 : 2128in gure 3 of this article ( published online first on nov 7 , 2009 ) , the data presented for unknown in the sex subgroup should have been in the egfr - positive cells subgroup . 
these corrections have been made to the printed article in this issue , and to the online version as of jan 6 , 2010 . rajkumar sv , jacobus s , callander ns , et al , for the eastern cooperative oncology group . 
lancet oncol 2010 ; 11 : 2937the webappendix of this article ( published online first on oct 22 , 2009 ) has been corrected as of jan 6 , 2010 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology vol 11 january 2010 correction to lancet oncol 2014 ; 15 : 64047 gianni l , eiermann w , semiglazov v , et al . 
 neoadjuvant and adjuvant trastuzumab in patients with her2 - positive locally advanced breast cancer ( noah ) : follow - up of a randomised controlled superiority trial with a parallel her2negative cohort . 
lancet oncol 2014 ; 15 : 64047in the declarations of interests section of this article , jose baselgas declarations should read jb reports personal fees and non - financial support from roche / genentech , during the conduct of the study ; personal fees and non - financial support from novartis , eli lilly , chugai pharamaceuticals , astrazeneca , sanofi - aventis , and bayer pharmaceuticals ; personal fees and stock from auro biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , juno therapeutics , and seragon ; personal fees from verastem ; and stock from aragon pharmaceuticals and apogen biotechnologies , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 5262 luen sj , salgado r , fox s , et al . 
 tumour - infiltrating lymphocytes in advanced her2 - positive breast cancer treated with pertuzumab or placebo in addition to trastuzumab and docetaxel : a retrospective analysis of the cleopatra study . 
lancet oncol 2017 ; 18 : 5262 in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentech during the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , grail and seragon ; stock from apogen biotechnologies ; and personal fees and non - financial support from novartis and eli lilly , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 73242 plus lapatinib previously emtansine diras v , miles d , verma s , et al . 
 versus trastuzumab capecitabine treated patients with her2 - positive advanced breast cancer ( emilia ) : a descriptive analysis of final overall survival results from a randomised , open - label , phase 3 trial . 
 lancet oncol 2017 ; 18 : 73242in the declaration of interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic lethal ) , grail , varian medical systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and non - financial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
 this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : 136072 therapy the declaration of kim sb , dent r , im sa , et al . 
ipatasertib plus paclitaxel versus placebo plus paclitaxel as first - line for metastatic triplenegative breast cancer randomised , ( lotus ) : a multicentre , double - blind , placebo - controlled , phase 2 trial . 
lancet oncol 2017 ; 18 : 136072 interests section of this article , jose baselgas declarations should read jb reports non - financial support from roche / genentechduring the conduct of the study ; personal fees and stock from aura biosciences , northern biologics ( f / k / a mosaic biomedicals ) , infinity pharmaceuticals , pmv pharma , juno therapeutics , tango ( f / k / a synthetic varian medical lethal ) , grail , systems and seragon ; stock from apogen biotechnologies and foghorn therapeutics ; personal fees and nonfinancial support from novartis and eli lilly ; and non - financial support from daiichi sankyo , outside the submitted work . 
this correction has been made to the online version as of nov 28 , 2018 . correction to lancet oncol 2017 ; 18 : e638 kim sb , dent r , wongchenko mj , singel sm , baselga j ; lotus investigators . 
we report the nal analyses of long - term survival data with additional follow - up in both trials . methods 311 men with metastatic disease were recruited to pr05 between 1994 and 1998 , and 508 men with non - metastatic disease were recruited to pr04 from 1994 to 1997 . 
all men were treated according to the recruiting sites standard practice at the time : for metastatic disease , all men were starting or responding to long - term hormone therapy ; for non - metastatic disease , most men had radiotherapy , hormone therapy , or both . 
men were randomly assigned to take four tablets per day of sodium clodronate ( 2080 mg ) or matching placebo for up to 3 years ( metastatic disease ) or 5 years ( non - metastatic )  . 
long - term overall survival was assessed on an intention - to - treat basis in all men at sites in england and wales using data from the national health service information centre , which held data for 278 of 311 men in the pr05 trial and 471 of 508 men in the pr04 trial . 
these studies are registered international standardised randomised controlled trials , numbers isrctn38477744 ( pr05 ) and isrctn61384873 ( pr04 )  . findings of the 278 men with metastatic disease , 258 ( 93% ) were reported to have died . 
evidence of a bene t for those with metastatic disease from use of sodium clodronate compared with placebo was seen in overall survival ( hazard ratio [ hr ] 077 , 95% ci 060098 ; p = 0032 )  . 
the medical research council ( mrc ) pr051 and pr042 randomised controlled trials assessed the role of adjuvant sodium clodronate in men with metastatic ( m1 ) and non - metastatic ( m0 ) prostate cancer , respectively . 
 both trials have previously reported results on their primary outcome measures.1 , 2 overall survival was a secondary outcome measure in both trials , but the overall survival data were immature when the primary analyses were published . 
the metastatic trial , pr05 , previously showed some evidence of improvement in overall survival with clodronate ( hazard ratio [ hr ] 080 , 95% ci 062103 ) ; whereas the non - metastatic trial , pr04 , did not show evidence of a bene t in overall survival ( hr 102 , 95% ci 080130 )  . 
the aim of this paper is to report nal analyses of long - term survival data with additional follow - up in both trials . methods patients the methods for these two trials have been fully described previously.1 , 2 in summary , 311 men with bony metastases from prostate cancer ( m1 ) and 508 men with prostate cancer with out metastases ( m0 ) gave written informed consent to join these two multi centre , double - blind , placebo - controlled randomised controlled trials , which opened to recruit ment in june , 1994 , and successfully completed accrual in july , 1998 , and december , 1997 , respectively . 
the trial was run under a clinical trial marketing product licence from the regulatory authority . 872 vol 10 september 2009 articles long - term hormone randomisation and masking randomisation was done centrally using minimisation across a number of strati cation factors to ensure balanced groups . 
in the pr05 trial in men with metastatic disease , the strati cation factors were treatment centre , time since therapy ( 6 weeks vs starting > 6 weeks ) , type of hormone therapy ( monotherapy vs maximal androgen blockade ) , and who performance status . 
in the non - metastatic trial , pr04 , the strati cation factors were : treatment centre , tumour stage ( t2 vs t3 vs t4 ) , primary therapy ( given vs not given ) , time from primary therapy to trial entry ( none vs 12 months vs > 12 months ) , and prostate - speci c antigen ( psa ) concentration at study entry ( < 50 ng / ml vs 50 ng / ml )  . 
men were randomly assigned to supplement the usual treatment for their prostate cancer with four tablets each day of oral sodium clodronate ( 2080 mg ) , or a matching placebo . 
men with metastatic disease were just starting or were already responding to standard treatment with hormone therapy ( androgen suppression ) , which was maintained through out the trial period . 
the primary outcome measure was the progression of symptom atic bone metastases or death from prostate cancer in the metastatic setting , or the development of symptomatic bone metastases or death from prostate cancer in the non - metastatic setting . 
all patients from england and wales who were successfully agged are included in the analyses : 278 ( 89% ) of 311 men with metastatic disease , and 471 ( 93% ) of 508 men with non - metastatic disease . 
exploratory interaction analyses were done using either tests for interaction or trend , as appropriate , to examine the consistency of the treatment e ect in di erent subgroups ; the degrees of freedom are speci ed in each instance . 
the subgroups used were the same as those used for previous analyses.1 , 2 ci are given at the 95% level ; p values are given to two signi cant gures . 
these studies are registered international standardised randomised controlled trials , numbers isrctn38477744 ( pr05 ) and isrctn61384873 ( pr04 )  . role of funding source the sponsor and main funder of the trial had no role in the design and conduct of the trial or in the analysis of the data . 
roche products ltd were involved in the design of the study , but not the analysis ; they were invited to submit comments on an early version of this manuscript . 
all patients on pr04 were agged before the main , previously reported analyses , but agging was not done in 190 patients in the pr05 trial who were already known to have died by that point . 
the estimated 5 - year survival was 80% with placebo and 78% with clodronate ; 10 - year survival rates were 51% with placebo and 48% with clodronate ( gure 2b )  . 
tests for interaction showed some evidence of heterogeneity in treatment e ect on survival in subgroups de ned by alkaline phos phatase ( heterogeneity = 435 , df 1 ; p = 0037 ) and serum creatinine ( heterogeneity = 516 , df 1 ; p = 0023 ; gure 3a ) , with larger treatment e ects with higher concentrations of alkaline phosphatase and serum creatinine . 
tests for inter action also showed some evidence of an increased treatment e ect in men who had bone metastases for a shorter time before randomisation ( hetero geneity = 369 , df 1 ; p = 0055 ) , and in men who had a shorter time from diagnosis to trial entry ( heterogeneity = 361 , df 1 ; p = 0058 ; gure 3a )  . 
 in the pr04 trial of men with non - metastatic disease , exploratory interaction analyses focused on the choice of primary treatment , although the numbers are small in each of these groups . 
this analysis showed no evidence of an interaction of clodronate with primary therapy given as radio therapy , hormone therapy , or both in terms of overall survival ( gure 3b ; heterogeneity = 113 , df 2 ; p = 057 )  . 
there was no evidence of heterogeneity of the treatment e ect of clodronate in patients receiving clodronate with long - term hormone therapy in the metastatic trial and the non - metastatic trial ( gure 3b ; heterogeneity = 084 , df 1 ; p = 036 )  . discussion overall survival remains an important long - term outcome measure in both metastatic and non - metastatic disease . 
here , we report an advantage in overall survival conferred by clodronate in men with metastases who joined the pr05 trial , but no evidence of a di erence in survival in men without metastases in the pr04 trial . 
the numbers of events are presented in parentheses , representing the deaths during these intervals . had nal responsibility for the decision to submit the manuscript for publication . results over the 5 - year period since the previous results , maturity in the metastatic trial , pr05 , increased from 235 ( 76% ) reported deaths in 311 men at the previously reported analyses to 258 ( 93% ) deaths in 278 men here , with a median follow - up of 115 years , compared with 49 years previously . 
for overall survival , there is evidence that clodronate confers a bene t compared with placebo , with an hr of 077 ( 95% ci 060098 ; p = 0032 )  . 
the estimated 5 - year survival was 21% with placebo and 30% with clodronate ; the estimated 10 - year survival was 9% with placebo and 17% with clodronate ( gure 2a )  . 
they have an established role in the management of myeloma and metastatic breast cancer , and the treatment of hypercalcaemia related to malignancy.6 , 7 prostate cancer is characterised by osteoblastic metastases , and it remains controversial as to whether osteoclast activation is a necessary precursor for the development of these sclerotic skeletal metastases , or occurs as a consequence of their presence.810 the results of our pair of trials support the latter hypothesis , as the bene t of clodronate seemed to be restricted to the progression of established metastases . 
 never theless , the more potent amino - bisphosphonates might also have direct e ects on tumour cells ; inducing apop tosis and inhibiting invasion through the inhibition of the mevalonate pathway.11 indeed , a recent study in local ised breast cancer12 suggests an improvement in disease - free survival in patients treated with zoledronic acid compared with placebo ( hr 064 , 95% ci 046091 )  . 
 when the trials started in the early 1990s , chemotherapy was not routinely used in the uk to any extent to treat prostate cancer , and the options for treatment after rst - line hormone therapy were very limited . 
 why have these two trials given apparently contradictory resultsis this due to biological factors related to the development and progression of bone metastases or just the play of chance ? certainly , both trials are modestly sized , with just over 800 patients recruited in total . 
the power calculations were based around the previously reported primary outcome measures rather than overall survival and di erences in survival might be attributable to chance , even though these analyses are based on 281 deaths in the non - metastatic setting and 258 deaths in the metastatic setting . 
 however , in the metastatic setting ( pr05 ) we have previously reported other bene ts in terms of symptomaticbone - progression - free survival with an increase in time to deterioration of performance status ( hr 071 , 95% ci 056092 ) and biologically measured favourable e ects on both alkaline phosphatase and psa nadir levels in favour of clodronate therapy.1 exploratory interaction analyses for the metastatic trial , reported here and previously , 1 suggest greater relative bene t with prompt initiation of clodronate for men with poorer prognostic features such as raised alkaline phosphatase and creatinine . 
 patients with raised alkaline phosphatase would be expected to have increased osteoblastic activity , and we speculate that this patient population with an increased disease burden might also have a greater degree of osteoclast activation and bone lysis , which might be modi ed with early bisphosphonate treatment . 
a raised creatinine level might lead to decreased bisphosphonate excretion , and therefore relatively greater drug exposure and more biological e ect . in the trial in men with non - metastatic disease ( pr04 ) , exploratory interaction analyses focused on primary therapy , because the choice of primary therapy would have been a re ection of both disease stage and standard local practice . 
for the group treated with a combination of radiotherapy and androgen deprivation , which would now be regarded as the standard of care for men with intermediate and high - risk localised disease , 35 the hr was 095 ( 95% ci 057157 )  . the principal action of bisphosphonates is to decrease osteoclast activity , and therefore bone resorption . 
 additional e ects might include a secondary reduction of tumour - producing growth factors , inhibition of the vol 10 september 2009 articles alternative additional treatments in most cases in both trials , and these were previously summarised for the metastatic trial.1 there were also very few data to suggest that variations in second - line or third - line hormone treatment would make a di erence to survival . 
there is no good reason to think there is an imbalance of these treatments across the trial groups . in prostate cancer , trials with much more potent bisphosphonates such as zoledronic acid should help clarify the situation for men with hormone - sensitive prostate cancer in due course ; a non - statistically signi cant trend for improved survival has already been reported using zoledronic acid in men with castrate - resistant disease.13 in men with hormone - sensitive disease , ongoing randomised controlled trials for men with high - risk locally advanced disease include the european association of urologys zeus trial ( isrctn66626762 ) across europe , which compares standard treatment with or without 4 mg infusions of zoledronic acid every 3 months for a total of 4 years . 
additionally , the trans - tasman radiation oncology groups radar trial ( nct00193856 ) in australia and new zealand , which is a four - arm trial in men having standard radiotherapy for prostate cancer , is comparing the e ects on survival of duration of androgen suppression ( given for either 5 or 18 months ) and use of zoledronic acid ( not given or given as 4 mg every 3 months for 18 months )  . 
 additionally , the lead investigators from pr04 and pr05 have been involved in the design and conduct of the ongoing mrc - led stampede trial ( isrctn78818554 ) .14 , 15 stampede is a trial for men with locally advanced or metastatic disease , and recruits similar populations to the pr04 and pr05 trials . 
in this six - arm trial , men starting long - term hormone therapy for the rst time are randomly assigned to supplement this treatment with 4 mg zoledronic acid given intravenously every 34 weeks for 2 years . 
the other research drugs in stampede are the taxane chemotherapy docetaxel , which is given for six cycles , and the cox2 inhibitor celecoxib , which is given for 1 year . 
patients in stampede are randomly assigned to receive hormone therapy alone ( control group ) , or hormone therapy plus docetaxel ; hormone therapy plus zoledronic acid ; hormone therapy plus celecoxib ; hormone therapy plus docetaxel plus zoledronic acid ; or hormone therapy plus zoledronic acid plus celecoxib . 
between 2000 and 3000 men will join the trial ; over 1000 patients have already been enrolled . in conclusion , pr05 is the rst trial , to our knowledge , to show an overall survival bene t conferred by an oral bisphosphonate when given in addition to standard hormone therapy to men with bone metastases who are starting or responding to hormone therapy for prostate cancer . 
however , there is no evidence that clodronate is of any bene t when given as an adjuvant to treatment in men with non - metastatic prostate cancer . contributors dpd and mdm co - led the drafting of the manuscript , participated in the design of the trials , participated in the implementation of trials , and read and approved the nal manuscript . 
mrs led the drafting of the manuscript , participated in the implementation of the trial , did the analyses , and read and approved the nal manuscript . con icts of interest mkbp , ks , and ms are all employed by the medical research council , a publicly funded body in the uk , who sponsored the trial . 
the other authors declared that they have no con icts of interest . acknowledgments this study was funded by the uk medical research council , and an education grant and free drugs from roche products ltd . articles e ects of the addition of gemcitabine , and paclitaxelrst sequencing , in neoadjuvant sequential epirubicin , cyclophosphamide , and paclitaxel for women with high - risk early breast cancer ( neo - tango ) : an open - label , 22 factorial randomised phase 3 trial helena m earl , anne - laure vallier , louise hiller , nicola fenwick , jennie young , mahesh iddawela , jean abraham , luke hughes - davies , ioannis gounaris , karen mcadam , stephen houston , tamas hickish , anthony skene , stephen chan , susan dean , diana ritchie , robert laing , mark harries , christopher gallagher , gordon wishart , janet dunn , elena provenzano , carlos caldas , for the neo - tango investigators summary background anthracyclines and taxanes have been the standard neoadjuvant chemotherapies for breast cancer in the past decade . 
we aimed to assess safety and e cacy of the addition of gemcitabine to accelerated paclitaxel with epirubicin and cyclophosphamide , and also the e ect of sequencing the blocks of epirubicin and cyclophosphamide and paclitaxel ( with or without gemcitabine )  . methods in our randomised , open - label , 22 factorial phase 3 trial ( neo - tango ) , we enrolled women ( aged > 18 years ) with newly diagnosed breast cancer ( tumour size > 20 mm ) at 57 centres in the uk . 
patients were randomly assigned via a central randomisation procedure to epirubicin and cyclophosphamide then paclitaxel ( with or without gemcitabine ) or paclitaxel ( with or without gemcitabine ) then epirubicin and cyclophosphamide . 
207 ( 25% ) patients had in ammatory or locally advanced disease , 169 ( 20% ) patients had tumours larger than 50 mm , 413 ( 50% ) patients had clinical involvement of axillary nodes , 276 ( 33% ) patients had oestrogen receptor ( er ) - negative disease , and 191 ( 27% ) patients had her2 - positive disease . 
addition of gemcitabine did not increase pcr : 70 ( 17% , 95% ci 1421 ) of 404 patients in the epirubicin and cyclophosphamide then paclitaxel group achieved pcr compared with 71 ( 17% , 1421 ) of 408 patients who received additional gemcitabine ( p = 098 )  . 
receipt of a taxane before anthracycline was associated with improved pcr : 82 ( 20% , 95% ci 1624 ) of 406 patients who received paclitaxel with or without gemcitabine followed by epirubicin and cyclophosphamide achieved pcr compared with 59 ( 15% , 1118 ) of 406 patients who received epirubicin and cyclophosphamide rst ( p = 003 )  . 
grade 3 toxicities were reported at expected levels : 173 ( 21% ) of 812 patients who received treatment and had full treatment details had grade 3 neutropenia , 66 ( 8% ) had infection , 41 ( 5% ) had fatigue , 41 ( 5% ) had muscle and joint pains , 37 ( 5% ) had nausea , 36 ( 4% ) had vomiting , 34 ( 4% ) had neuropathy , 23 ( 3% ) had transaminitis , 16 ( 2% ) had acute hypersensitivity , and 20 ( 2% ) had a rash . 
86 ( 11% ) patients had grade 4 neutropenia and 3 ( < 1% ) had grade 4 infection . interpretation although addition of gemcitabine to paclitaxel and epirubicin and cyclophosphamide chemotherapy does not improve pcr , sequencing chemotherapy so that taxanes are received before anthracyclines could improve pcr in standard neoadjuvant chemotherapy for breast cancer . funding cancer research uk , eli lilly , bristol - myers squibb . introduction survival of patients with early breast cancer has improved substantially in the past 20 years.1 however , incidence of breast cancer has increased and continuesto be a major health proble the early breast cancer trialists collaborative group overview analyses , 2 , 3 and individual trial data have shown bene t for adjuvant anthracyclines46 and taxane - containing chemotherapy.79 progress made through large adjuvant randomised treatment trials has been relatively slow . 
follow - up is necessarily prolonged to meet the prespeci ed eventrate criteria for disease - free survival ( dfs ) and overall vol 15 february 2014 lancet oncol 2014 ; 15 : 20112 published online december 19 , 2013 s1470 - 2045 ( 13 ) 70554 - 0 see comment page 131 copyright earl et al . 
tango11 and neo - tango were designed to provide this cross reference , because both trials investigated the addition of gemcitabine to standard chemotherapy , although the sequence of chemotherapy was not addressed in tango . neo - tango was a randomised phase 3 neoadjuvant trial that aimed to assess bene ts of addition of gemcitabine to accelerated paclitaxel with epirubicin and cyclophosphamide , and also the e ect of sequencing of epirubicin and cyclophosphamide , and paclitaxel ( with and without gemcitabine ) blocks . 
gemcitabine is an e ective drug in metastatic disease12 , 13 and other neoadjuvant or adjuvant trials have addressed similar questions for antimetabolites , with gemcitabine14 , 15 or oral capecitabine.16 neo - tango was designed and started before the introduction of adjuvant trastuzumab for her2 - positive disease . methods study design and participants in the neo - tango phase 3 randomised trial , we used a 2 2 factorial design to address both the role of gemcitabine in a sequential neoadjuvant chemotherapy regimen of epirubicin and cyclophosphamide and paclitaxel , and also the sequence of administration of these treatment components , in terms of short - term and long - term outcomes in women presenting with early breast cancer . ipsilateral supraclavicular regarded hormone we enrolled women aged older than 18 years with a histological diagnosis of early invasive breast cancer , with a radiological tumour size of more than 20 mm with or without axillary involvement . 
women with in ammatory cancer , t4 tumours with direct extension to the chest wall or lymph - node skin , and involvement were eligible with any size of primary tumour . 
her2 status was regarded as positive when immunohistochemistry was 3 + , or 2 + with evidence of ampli cation of the her2 gene on uorescence in - situ hybridisation . 
other eligibility criteria were adequate cardiac function , no myocardial infarction during the previous 6 months , adequate bone marrow , hepatic , and renal function , and appropriate ecog performance status ( 02 )  . 
patients provided written informed consent . neo - tango was an investigator designed and led trial , which was granted clinical trials authorisation from the medicines and healthcare products regulatory agency ( mhra ) on june 17 , 2004 , and approved by the multicentre research ethics committee nationally on nov 1 , 2004 , and subsequently the local research ethics committees at all participating centres . 
the study was undertaken by the uk national cancer research institute ( ncri )  . randomisation and masking in our open - label trial , eligible participants were randomly allocated 1 : 1 : 1 : 1 to receive epirubicin and cyclophosphamide followed by paclitaxel , paclitaxel followed by epirubicin and cyclophosphamide , epirubicin and cyclophosphamide followed by paclitaxel and gemcitabine , or paclitaxel and gemcitabine followed by epirubicin and cyclophosphamide . 
strati cation by minimisation was undertaken by age ( 50 years and > 50 years ) , er status ( positive and negative ) , primary tumour size ( 5 cm and > 5 cm ) , clinical involvement of axillary nodes , and in ammatory or locally advanced disease . 
chemotherapy regimens used were epirubicin 90 mg / m and cyclophosphamide 600 mg / m once every 21 days , and paclitaxel 175 mg / m with or without gemcitabine 2000 mg / m once every 14 days . 
 treatment allocations were made by telephoning the cancer research uk trials unit ( birmingham , uk ) , who used their central computerised minimisation procedure to generate the patients random allocation . procedures our primary endpoint was pcr , de ned as absence of invasive breast cancer in the breast and axillary lymph nodes , after neoadjuvant chemotherapy . 
a two - reader review of pathology reports was undertaken , masked to treatment group , by the chief investigator ( hme ) and the study pathologist ( ep ) , for patients who had surgery . 
 a detailed analysis of this review process has been published elsewhere.17 residual non - invasive ductal carcinoma in situ was allowed . secondary endpoints reported here include dfs and overall survival . 
we also recorded use of growth factor support ( usually granulocyte colony stimulating factor [ gcsf ] )  . the maximum permitted dose delay or interruption was 4 weeks to allow recovery from severe toxicity or for unscheduled procedures ( eg , emergency surgery )  . if neutropenic fever or sepsis occurred after a cycle of chemotherapy , the next cycle was delayed until the absolute neutrophil count was at least 10 10 cells per l . 
 following a delay , either dose reduction of all drugs to 202 vol 15 february 2014 articles 80% , or gcsf support with 100% dose were allowed , and all remaining cycles of the same four - cycle block were given at those doses . 
for persistent thrombocytopenia , the next cycle was delayed until patients had at least 100 10 platelets per l and was reduced to 80% , maintaining this dose reduction for subsequent cycles . 
once started , prophylactic gcsf was usually continued into the second phase of chemotherapy at the discretion of the responsible physician . if grade 2 neuropathy occurred during treatment with paclitaxel , remaining doses were reduced to 135 mg / m ( gemcitabine was unchanged )  . 
her2 - negative de ned as immunohistochemistry score of 01 , or 2 , but uorescence in - situ hybridisation ( fish ) negative ; her2 - positive de ned as immunohistochemistry of 3 or 2 and fish positive . 
each tumour could have multiple types and characteristics recorded . table 1 : patient and tumour characteristics at baseline of six cycles in total , at the discretion of the treating consultant . gemcitabine was reduced to 80% in the event of grade 3 hepatic toxicity ( transaminitis ; aspartate aminotransferase or alanine aminotransferase 520 upper limit of normal [ uln ] ) on day of treatment , at clinicians discretion because transaminitis is not known to a ect gemcitabine clearance . 
we were unable to substantiate earlier concerns about gemcitabines potential for clinically signi cant hepatic impairment . cardiac toxicity was not anticipated at the cumulative doses of epirubicin of 360 mg / however , congestive cardiac failure developed , patients were investigated and treated as appropriate , epirubicin was discontinued , and other chemotherapy was given at the discretion of the treating clinician . in the event of gemcitabine - related pulmonary toxicity of ctcae grade 2 or worse , the patient was discontinued from study therapy . paclitaxel infusion was stopped if mild symptoms of skin rash , ushing , and localised pruritus occurred . 
 if severe symptoms occurred , including bronchospasm , generalised urticaria , angio - oedema , hypotension ( systolic blood pressure < 100 mm hg ) , or life - threatening infusion was stopped and anaphylaxis , paclitaxel treatment was given with intramuscular epinephrine 1 ml 1 : 1000 , intravenous steroids , and intravenous antihistamines ; rechallenge was contraindicated . surgery ( breast and axillary ) , radiotherapy , and adjuvant endocrine treatment were given according to local protocols . 
patients will continue to receive the national cancer intelligence network ( ncin ) who will monitor for dfs and overall survival . follow - up through statistical analysis our power calculations assumed that the pcr would be 20% after standard treatment ( epirubicin and cyclophosphamide followed by paclitaxel )  . 
on this basis , we aimed to randomly allocate 200 patients into each of the four treatment groups , yielding combined data for 400 patients into each group for the two questions ( ie , e cacy and safety of the addition of gemcitabine to paclitaxel plus epirubicin and cyclophosphamide treatment [ component analysis ] and order of chemo therapy regimens [ sequencing analysis ] )  . 
this would allow an absolute di erence in the pcr in excess of 10% to be detected at the 5% ( two - sided ) level of signi cance with 85% power . 
all reported p values are two - sided . vol 15 february 2014 articles for the primary analysis , we calculated pcr for all logistic treatment groups and used univariate regression to test the addition of gemcitabine and the role of sequencing . 
we used multivariate logistic regression to calculate p values for both the treatment and scheduling e ects after adjustment for prognostic factors . we calculated dfs from the date of randomisation to the date of rst event ( locoregional relapse , distant relapse , progression on neoadjuvant chemotherapy , or death ) , or to the date of censoring . 
we calculated overall survival from the date of randomisation to the date of death or to the date of each patients last clinic visit ( for women who are not known to have died )  . 
when assessing the association between pathological response and these outcomes , we calculated overall survival and dfs from date of surgery . the neo - tango protocol stated that the rst planned interim analysis of dfs and overall survival would occur when at least 120 events had occurred or when median follow - up was at least 3 years . 
the corresponding authors ( hme and lh ) had full access to all of the data and had nal responsibility for the decision to submit for publication . results between jan 18 , 2005 , and sept 28 , 2007 , we recruited 831 patients at 57 centres ; three patients were found to be ineligible after randomisation , leaving 828 for analysis ( gure 1 ; table 1 )  . 
adjusted for the ve strati cation variables ( age , er status , tumour size , clinical involvement of axillary nodes , and in ammatory or locally advanced disease )  . 
 tumour grade of each patients largest breast tumour at baseline . table 2 : rates of pathological complete response ( pcr ) 206 vol 15 february 2014 articles see online for appendix omission of the nal cycle of chemotherapy , with the patient proceeding straight to surgery . because the neo - tango protocol did not include neoadjuvant trastuzumab , we expected fewer patients with her2 - positive disease to enrol as the trial progressed . 
 107 patients enrolled in 200506 had her2 - positive disease ( 30% of the 357 tested ) compared with 84 in 2007 ( 24% of the 347 tested ; p = 019 )  . all patients had surgery ( breast and axilla ) according to local protocols and the details will form the basis of a future publication . 
all patients with er - positive disease ( 543 [ 67% ] patients were er - positive ) received appropriate adjuvant hormonal treatments and 750 patients ( 91% ) received radiotherapy treatments according to local protocols . 
141 ( 17% ) of these patients had pcr , which was much the same for patients in the epirubicin and cyclophosphamide plus paclitaxel , and the epirubicin and cyclophosphamide plus paclitaxel and gemcitabine groups ( between - group di erence 007% , 95% ci 5 to 5 ; table 2 )  . 
however , signi cantly more patients who received paclitaxel ( with or without gemcitabine ) before epirubicin and cyclophosphamide achieved pcr than did those who received epirubicin and cyclophosphamide rst ( between group di erence 6% , 05 to 11 ; table 2 )  . 
subgroup analysis by her2 status , er status , or tumour grade did not a ect the results ( table 2 , appendix )  . median follow - up was 47 months ( iqr 3751 )  . 
at the time of analysis , 167 ( 20% ) of the 828 eligible patients had died , 227 ( 27% ) had had locoregional or distant relapses , and 236 ( 29% ) had had dfs events . 
702 ( 86% ) of the remaining 812 patients received eight cycles of chemotherapy ; the main reasons for not receiving all eight cycles were toxicity ( 54 [ 49% ] of the 110 patients receiving between one and seven cycles ) , disease progression ( 28 [ 25% ] patients ) , allergic reaction to paclitaxel ( 15 [ 14% ] patients ) , poor response to chemotherapy ( seven [ 6% ] patients ) , or other reasons ( six [ 5% ] patients )  . the median cddi for the 819 patients was 97% ( iqr 9199% )  . 
no di erences between the component groups or the sequencing groups were detected ( p = 056 for component analysis and p = 018 for sequencing analysis )  . dose intensities over individual cycles did not notably deteriorate for any of the four randomised treatment groups ( appendix )  . 
more dose reductions for the fourth cycle of regimens containing paclitaxel ( with or without gemcitabine ) occurred when it was given second compared with prior administration ( 22% vs 10% , respectively ; appendix ) , and similarly for dose delays ( 15% vs 11% , respectively ; appendix )  . overall survival from surgery was longer for patients attaining pcr than it was for those who did not attain pcr ( gure 3 )  . 
grade 3 toxicities included neutropenia , muscle and joint pain , infection , neuropathy , transaminitis , fatigue , nausea and vomiting , rash , and acute hypersensitivity ( table 3 )  . 
one patient in the epirubicin and cyclophosphamide followed by paclitaxel group received only ve cycles of chemotherapy because of fatigue and anaphylaxis and then died 12 weeks later of respiratory failure ( distant recurrence with bilateral pleural e usion and extensive alveolar shadowing )  . 
 = no reported toxic e ects of this grade . table 4 : reported grade 4 severe toxic e ects discussion in our study , provision of a taxane before standard anthracycline chemotherapy was associated with a signi cant improvement in pcr , from 15% to 20% , compared with a standard anthracyclinerst sequence ( p = 003 ; panel )  . 
these ( p < 00001 ) and overall survival improvement ndings con rm the bene t of taxanerst sequencing that was noted in a large retrospective non - randomised study from the md anderson cancer center , tx , usa , 19 which reported data from 1414 patients treated with neoadjuvant chemotherapy and 1596 patients treated with adjuvant chemotherapy between 1994 and 2009 . 
 in addition all major international early breast cancer trials groups were contacted to discuss our proposed design of epirubicin and cyclophosphamide , and dose - dense paclitaxel with or without gemcitabine . 
the nsabp - b38 adjuvant trial had a similar experimental arm with dose - dense doxorubicin and cyclophosphamide , and dose - dense paclitaxel ( 175 mg / m every 2 weeks ) with or without gemcitabine ( 2000 mg / m every 2 weeks )  . 
in addition , neo - tango had a complementary adjuvant trial ( tango ) which also addressed the addition of gemcitabine . interpretation neo - tango con rms the nsabp - b38 , 14 nsabp - b40 , 15 and tango11 results , which show no bene t from the addition of gemcitabine to anthracycline and taxane - based chemotherapy treatments for early breast cancer . 
neo - tango shows a signi cant bene t from taxanerst sequencing , and is the largest randomised trial to con rm this e ect . 314 patients have been included in small randomised phase 2 adjuvant trials2024 and 276 patients have been included in neoadjuvant trials2528 addressing taxane and anthracycline sequencing . 
some of these studies report more dose reductions of taxane when anthracyclines are given rst , 2123 , 25 and one randomised neoadjuvant study showed a non - signi cant increase in incidence of pcr for taxanerst sequencing.27 indirect evidence from neoadjuvant randomised studies for taxanerst sequencing comes compared uorouracil , epirubicin , and cyclophosphamide with docetaxel followed by epirubicin and docetaxel . 
however , the neo - tango analysis showed no sequence - speci c di erence in cddi to explain this taxanerst sequence result . 10994 , 28 which from eortc preclinical and clinical studies have suggested mechanisms to explain the bene t of early receipt of taxanes . 
taghian and colleagues26 drew attention to increases in interstitial uid pressure and improved oxygenation within breast tumours after neoadjuvant paclitaxel , which might allow increased concentrations of anthracyclines to accumulate within tumour tissue when given afterwards . 
in addition , preclinical data show that in breast cancer cells with heat shock protein 27 overexpression , a paclitaxel then doxorubicin sequence is more e ective at cell killing than the more standard doxorubicin then paclitaxel sequence.31 taxanerst sequences allow early treatment with concomitant trastuzumab and bevacizumab , which might provide additional therapeutic advantage , shown for trastuzumab in the finher study.32 both the nsabp - b4015 and artemis33 trials of bevacizumab have adopted taxanerst sequencing for this reason . 
because all patients receive both the taxane and anthracycline components , taxanerst sequencing could be considered in all similar block - sequential adjuvant and neoadjuvant protocols . neo - tango con rms the result of tango11 and shows no signi cant bene t from addition of gemcitabine to a combination that already contains anthracycline , cyclophosphamide , and paclitaxel . 
however , gemcitabine has shown promising results in patients with metastatic disease when added to paclitaxel in the rst - line relapse setting.13 much the same results have already been reported in the adjuvant nsabp - b38 , 14 and neoadjuvant nsabp - b4015 studies . 
 gemcitabine was given at 666 mg / m per week ( compared with 1000 mg / m per week in neotango and nsabp - b38 ) and docetaxel doses were reduced to 75 mg / m , and showed no bene t in terms of pcr . 
in neo - tango , we noted a non - signi cant increase in pcr after the addition of gemcitabine in patients with highgrade disease ( table 2 )  . paclitaxel was delivered every 14 days at 175 mg / m ( with or without gemcitabine 2000 mg / m )  . 
this dose - dense protocol was delivered without any reported delays in 82% of paclitaxel - containing cycles and only 8% of cycles required growth factor support to maintain dose intensity . 
the use of neoadjuvant or adjuvant weekly paclitaxel is now often used as standard at 80 mg / m per week and therefore the taxanerst sequencing bene t seen in neo - tango with paclitaxel at 875 mg / m per week , is close to standard practice across the world . whether pcr in neoadjuvant trials can be a surrogate endpoint for dfs and overall survival has been debated . 
 von minckwitz and colleagues meta - analysis34 of 6377 patients in the german breast group and abobsg neoadjuvant chemotherapy the prognostic value of not achieving a pcr is most dependent on the molecular subtype of the original trials showed that 210 vol 15 february 2014 articles trastuzumab , whereas none of tumour . 
for luminal a subtype , 35 a meta - analysis included 46% of patients in this category with pcr of 89% , whereas neo - tango had 29% luminal a patients with pcr of 35% . 
in addition , 662 ( 50% ) of 1327 patients with her2 - positive disease in the meta - analysis received the neoadjuvant 187 patients with her2 - positive disease in neo - tango did . 
the metaanalysis shows pcr of 358% in 911 patients , although in a recent trial ( gepar quinto ) , 36 663 patients with triplenegative breast cancer had a pcr of 279% , increasing to 393% chemotherapy . 
the pcr for 94 such patients in neotango was 39% with the addition of gemcitabine and 40% with taxanerst sequence . addition of bevacizumab after the in the z1040 - alliance neoadjuvant study , 37 280 patients with her2 - positive breast cancer were randomly allocated to receive standard uorouracil , epirubicin , and cyclophosphamide followed by weekly paclitaxel with trastuzumab ( pcr in the breast 565% ) , and a taxanerst sequence with concurrent weekly trastuzumab throughout ( pcr in the breast 542% )  . 
however in neotango , 187 patients with her2 - positive disease had a pcr for taxanerst sequence of 26% compared with 17% for standard sequence ( p = 003 ; table 2 )  . 
notably , in neotango , in 121 er - positive , her2 - positive women , pcr was 28% for taxanerst sequencing and 9% for anthracyclinerst sequencing , and in 66 er - negative , her2 - positive women pcr was 23% for taxanerst sequencing and 32% for anthracyclinerst sequencing . 
however , the di erences between the neotango results and z1040 could be explained by the absence of neoadjuvant trastuzumab in neo - tango . the association a recent meta - analysis38 by the us food and drug administration ( fda ) con rms the strong correlation between pcr and dfs and overall survival in patients achieving a pcr , and this association was con rmed in neo - tango . 
 the fda proposed that pcr in neoadjuvant trials in highly proliferative breast cancers could now contribute to accelerated drug approval in these types of early breast cancer.39 this proposal is a landmark in neoadjuvant chemotherapy trials for highly proliferative breast cancer , and will facilitate more rapid introduction of new agents for this subtype . 
randomised neoadjuvant trials of chemotherapy in combination with target - directed novel agents will be able to focus on high proliferation molecular subtypes ( er - negative , her2 - positive , high grade , and patients with germline brca mutations ) in which the association between pcr and dfs and overall survival is expected to be correlated . 
 however , indicates the fda meta - analysis also subgroups of breast cancer with lower proliferative potential ( ie , er - positive , her2 - negative , low and intermediate grade ) that have a better prognosis independent of pcr . 
in these groups , the response to chemotherapy is poor and pcr is low but the long - term outcome is good , and survival is in uenced more by subsequent adjuvant hormonal treatment . 
in neotango , patients from all the di erent prognostic groups were included , and therefore the pro le of the trial population will weaken the correlation between pcr and long - term outcomes for the group as a whole . 
for patients with a previously known poor prognosis , who have high pcr incidence , a robust and reliable correlation will probably emerge between pcr and longer - term outcome . contributors hme , a - lv , lh , gw , jd , and cc designed the study and wrote grant applications . 
all authors collected data , revised the report and agreed to submit the paper for publication . con icts of interest this project was funded by cancer research uk ( project grant c57 / a4180 , 2004 - 2009 ) and was supported by the national cancer research network . 
all other authors declare that they have no con icts of interest relevant to this publication . acknowledgments we acknowledge 88 investigators and their teams from 57 participating centres who entered patients in neo - tango . 
we also thank the members of the data and safety monitoring board ( i craig henderson [ university of california , san francisco , ca , usa ] , luca gianni [ unit of new drugs and innovative therapies , department of medical oncology , san ra aele hospital , irccs , milan , italy ] , and mark f brady [ gynecologic oncology group statistical & data center , roswell park cancer institute , bu alo , ny , usa ] ) , and trials unit sta for the phase 3 coordination ( cancer research uk clinical trials unit , birmingham , uk ) , translational coordination ( university of cambridge , addenbrookes hospital , cambridge , uk ) , and statistical analysis ( warwick clinical trials unit , coventry , uk )  . re ection and reaction panel : concepts applicable to various histologies ( excluding small - cell carcinoma , germ - cell tumors , and lymphoma ) in the analysis of brain metastasis trials involving radiosurgery and adjuvant wbrt patients eligible for radiosurgery have brain metastases less than 34 cm in diameter adjuvant wbrt probably decreases the risk of distant brain tumour recurrence for most histologies including melanoma adjuvant wbrt probably does not improve overall survival adjuvant wbrt is associated with a greater decline in learning and memory function at 4 to 6 months in a heterogenous population of primary cancer types wbrt causes acute fatigue and hair loss wbrt frequently delays the prompt initiation of systemic therapy a substantial proportion of patients with brain metastases do not need adjuvant wbrt in their lifetime a substantial proportion of patients with brain metastases initially treated with radiosurgery can be salvaged with additional radiosurgery delaying , or obviating the need for giving wbrt completely radiosurgery , like wbrt , can be used to address uncontrolled brain metastases in patients seeking to enroll on and qualify for clinical trials who would be otherwise excluded di culty inherent in accruing su cient numbers of patients to a site - speci c brain metastasis trial . 
however , there are common elements and fundamental concepts that seem to be valid across various histologies ( excluding small - cell carcinoma , germ - cell tumours , and lymphoma ) involving in the analysis of brain metastasis trials radiosurgery and adjuvant whole brain radiation therapy ( wbrt ; panel )  . 
perhaps in the future , the combination of advanced functional neuro - imaging and gene - expression pro ling techniques will enable us to identify better the subgroup of patients who are at greatest risk for developing distant brain metastases . 
the current preference and practice of medical oncologists in the department of melanoma medical oncology at md anderson cancer is to refer patients with oligo brain metastases to undergo radiosurgery alone to facilitate rapid enrolment on systemic therapy protocols . 
it is agreed that specialised brain metastasis trials focused exclusively on melanoma patients would help further elucidate the respective roles of surgery , radiosurgery , adjuvant wbrt , and systemic treatments . 
a phase 2 eastern cooperative oncology group ( e 6397 ) study of radiosurgery alone in patients with one to three brain metastases from renalcell carcinoma , melanoma , or sarcoma concluded that delaying wbrt might be appropriate for some subgroups of patients.2 in the meantime , the management of patients with melanoma brain metastases relies on the extrapolation of data gleaned from existing reports on brain metastasis , rst - hand knowledge of the patient history , and multidisciplinary discussion to provide the best treatment plan individualised for each patient . eric l chang * , patrick hwu department of radiation oncology ( elc ) , department of melanoma medical oncology ( ph ) , the university of texas md anderson cancer center houston , tx , usa echang@mdanderson.org the authors declared no con icts of interest . chang el , wefel js , hess kr , et al . 
phase ii trial of radiosurgery for one to three newly diagnosed brain metastases from renal cell carcinoma , melanoma , and sarcoma : an eastern cooperative oncology group study ( e 6397 )  . 
radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
lancet oncol 2010 ; 11 : 2128in gure 3 of this article ( published online first on nov 7 , 2009 ) , the data presented for unknown in the sex subgroup should have been in the egfr - positive cells subgroup . 
these corrections have been made to the printed article in this issue , and to the online version as of jan 6 , 2010 . rajkumar sv , jacobus s , callander ns , et al , for the eastern cooperative oncology group . 
lancet oncol 2010 ; 11 : 2937the webappendix of this article ( published online first on oct 22 , 2009 ) has been corrected as of jan 6 , 2010 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology vol 11 january 2010 correction to lancet oncol 2020 ; 21 : 76375 correction to lancet oncol 2021 ; 22 : 198211 paz - ares l , ciuleanu t - e , cobo m , et al . 
 first - line nivolumab plus ipilimumab combined with two cycles of chemotherapy in patients with non - smallcell lung cancer ( checkmate 9la ) : an international , randomised , open - label , phase 3 trial . 
lancet oncol 2021 ; 22 : 198211in figure 4c of this article , the number at risk at 15 months in the nivolumab plus ipilimumab with chemotherapy group should have been 107 . 
abemaciclib plus trastuzumab with or without fulvestrant versus trastuzumab plus standard - of - care chemotherapy in women with hormone receptor - positive , her2 - positive advanced breast cancer ( monarcher ) : a randomised , open - label , phase 2 trial . 
the text in the results section ( page 769 ) should have read as follows : eight patients in group a , 12 patients in group b , and six patients in group c discontinued at least one study treatment owing to adverse events ( figure 1 )  . 
five patients in group b and four patients in group c discontinued all treatments in the study regimen owing to adverse events and one patient in group a discontinued all treatments in the triplet combination . 
two of the 12 patients in group b discontinued at least one study treatment owing to cardiac failure , two additional patients in group b discontinued study treatment owing to decreased neutrophil count , and another two patients discontinued study treatment due to neutropenia . 
 patients were randomly assigned ( 1 : 1 ) to receive either postoperative cisplatin , doxorubicin , and methotrexate ( map ) or map plus ifosfamide and etoposide ( mapie ) using concealed permuted blocks with three strati cation factors : trial group ; location of tumour ( proximal femur or proximal humerus vs other limb vs axial skeleton ) ; and presence of metastases ( no vs yes or possible )  . 
the map regimen consisted of cisplatin 120 mg / m , doxorubicin 375 mg / m per day on days 1 and 2 ( on weeks 1 and 6 ) followed 3 weeks later by high - dose methotrexate 12 g / m over 4 h . 
the mapie regimen consisted of map as a base regimen , with the addition of high - dose ifosfamide ( 14 g / m ) at 28 g / m per day with equidose mesna uroprotection , followed by etoposide 100 mg / m per day over 1 h on days 15 . 
median follow - up was 621 months ( iqr 466766 ) ; 623 months ( iqr 469771 ) for the map group and 611 months ( iqr 465753 ) for the mapie group . 
event - free survival did not di er between treatment groups ( hazard ratio [ hr ] 098 [ 95% ci 078123 ] ) ; hazards were non - proportional ( p = 00003 )  . 
the most common grade 34 adverse events were neutropenia ( 268 [ 89% ] patients in map vs 268 [ 90% ] in mapie ) , thrombocytopenia ( 231 [ 78% in map vs 248 [ 83% ] in mapie ) , and febrile neutropenia without documented infection ( 149 [ 50% ] in map vs 217 [ 73% ] in mapie )  . 
mapie was associated with more frequent grade 4 non - haematological toxicity than map ( 35 [ 12% ] of 301 in the map group vs 71 [ 24% ] of 298 in the mapie group )  . 
 two patients died during postoperative therapy , one from infection ( although their absolute neutrophil count was normal ) , which was de nitely related to their map treatment ( speci cally doxorubicin and cisplatin ) , and one from left ventricular systolic dysfunction , which was probably related to mapie treatment ( speci cally doxorubicin )  . 
 one suspected unexpected serious adverse reaction was reported in the map group : bone marrow infarction due to methotrexate . interpretation euramos - 1 results do not support the addition of ifosfamide and etoposide to postoperative chemotherapy in patients with poorly responding osteosarcoma because its administration was associated with increased toxicity without improving event - free survival . 
ifosfamide with16 , 17 or without etoposide17 also has activity in this setting and when incorporated into the treatment of patients with metastatic disease seems to improve event - free survival.18 though uncontrolled studies suggested that changing therapy on the basis of histological response improves outcomes , 3 , 5 , 19 the e cacy of this strategy had not been tested in a randomised trial . we report the primary results for patients who had a poor response and were randomised to the euramos - 1 trial , a collaboration between the childrens oncology group ( cog ) , the cooperative osteosarcoma study group ( coss ) , the european osteosarcoma intergroup ( eoi ) , and the scandinavian sarcoma group ( ssg )  . 
we did this trial to assess whether the addition of ifosfamide and etoposide to standard postoperative map would improve event - free survival in patients whose primary tumour showed a poor response to preoperative map . methods study design and participants euramos - 1 was an open - label , international , randomised , phase 3 , controlled trial . 
the main eligibility criteria for registration included having high - grade localised or metastatic extremity or axial osteosarcoma deemed resectable by the treating team , research in context evidence before this study osteosarcoma is a rare disease but is the most common bone tumour in children and adolescents and is associated with high mortality . 
before the euramos - 1 trial started , there has never been a study randomising patients with osteosarcoma following surgery to add chemotherapy to the preoperative backbone , and a formal literature review was not possible . 
through collaborations and pubmed searches , we were aware of the relevant publications in osteosarcoma which were about importance of histological response and use of ifosfamide in treating patients with a poor histological response . 
patients who have a poor response to chemotherapy ( 10% viable tumour ) have a substantially worse survival than those with a good response ( < 10% viable tumour ) with 5 - year overall survival of around 4555% and 7580% , respectively . 
therefore , no previous study has assessed in a randomised comparison whether adding an ifosfamide containing combination to standard treatment improves the outcome for patients identi ed as having a poor histological response . added value of this study randomisation of patients with a poor response in euramos - 1 trial represents a large , international comparison , with patients registered at the start of treatment and randomly assigned after surgery . 
patients were also required to have a serum bilirubin concentration of at most less than 15 times the upper limit of normal and a normal creatinine concentration for their age as per protocol . 
 the main eligibility criteria for randomisation were registeration before de nitive surgery to take part in euramos - 1 ; assessment of histological response in the primary tumour and randomisation within 35 days of de nitive surgery ( assessment by reference pathologist where possible ) ; age 5 years or younger at biopsy for patients with good response ; provision of all essential data ( entry form , preoperative chemotherapy forms , surgery , and pathology report ) ; receiving exactly two courses of cisplatin and doxorubicin , at least two courses , and no more than six courses of methotrexate ; macroscopically surgical resection of the primary tumour ; no evidence of local disease progression ; recovery from previous therapy allowing administration of post operative chemotherapy as planned ; no progression of metastatic disease or new metastases and removal of metastases ( in patients with metastatic disease at registration ) done or deemed feasible ( to be done after primary surgery ) ; macroscopically complete surgical resection of the primary tumor ; and written consent to participate in the study . 
 the data was collected in each data centre ( cog , coss , eoi , and ssg ) and transferred periodically to the coordinating data centre ( medical research council clinical trials unit )  . 
 before enrolment , all institutions were required to have obtained all regulatory and ethics approvals in accordance to their national , and for european centres , european rules and regulations , as mentioned in the protocol . 
 the protocol is available online . complete randomisation and masking patients were randomly allocated ( 1 : 1 ) to receive either map or map plus ifosfamide and etoposide ( mapie )  . 
 treatment allocation was done with centralised implementation of concealed random permuted blocks with three strati cation factors : trial group , location of tumour ( proximal femur or proximal humerus vs other limb vs axial skeleton ) , and presence of metastases ( no vs yes or possible )  . 
metastases were de ned as at least three lesions bigger than 5 mm or a single lesion bigger than 1 c patients with lung lesions not meeting these criteria were classi ed as having possible metastases . 
each treating institution was responsible for enrolling their patients into the trial , and patients were assigned to interventions using the medical research council clinical trials unit randomisation system ( for coss , eoi , and ssg sites ) and the cog randomisation system ( for cog sites )  . 
patients and investigators were not masked to treatment allocation . infusion intravenous procedures baseline assessment required a complete blood count , complete set of chemistry test data ( including liver and kidney function ) , a baseline echocardiogram and hearing test , imaging with an mri of the primary site , and a chest ct scan and a bone scan ( a pet scan could be used instead )  . 
all patients received preoperative therapy with map20 ( appendix p 10 ) for 10 weeks consisting of cisplatin 120 mg / m ( 4 h infusion of 60 mg / m per day for 2 days in cog sites ; continuous 72 h in other sites ) and doxorubicin 375 mg / m per day on days 1 and 2 ( on weeks 1 and 6 )  . 
this was followed by high - dose methotrexate 12 g / m over 4 h ( maximum dose 20 g at cog institutions ) with hyper - hydration , alkalinisation , and standard leucovorin rescue at a dose of 15 mg / m starting 2448 h from methotrexate infusion and continuing until methotrexate concentration was less than 01 m ( weeks 4 , 5 , 9 , and 10 ) .20 , 21 leucovorin rescue was adjusted with the dosing nomogram according to the methotrexate concentration . 
 to begin myelosuppressive cycles , patients needed an absolute neutrophil count of at least 750 cells per l and a platelet count of at least 75 000 platelets per l . 
 criteria for administering high - dose methotrexate were di erent and included an absolute neutrophil count of at least 250 cells per l and a platelet count of at least 50 000 platelets per l . patients were restaged at 10 weeks preoperatively ( with the same imaging studies done at diagnosis ) and investigator - assessed response was reported according to response to treatment in solid tumors ( recist ) criteria , version 1 . 
eligibility for postoperative randomisation included macroscopic tumour resection , at least 10% morph ologically viable tumour , no disease progression , no or resectable metastases , and ability to resume therapy within 35 days after surgery . 
 2260 patients were registered 1200 patients were not poor responders 1060 patients were poor responders 442 excluded 204 did not provide consent 111 had progression ( local or distant ) 45 late histology 31 had incorrect preoperative ct 16 no removal of metastasis or unresectable disease 7 had not recovered from prior therapy 6 had a change in diagnosis 5 had incomplete resection of primary tumour 17 other 618 patients were randomly assigned * 310 assigned to receive map ( intention - to - treat population ) 308 assigned to receive mapie ( intention - to - treat population ) 8 did not receive map 4 treatment refusal 1 protocol violation 1 not in patients best interest 2 lost to follow - up 8 did not receive mapie 5 treatment refusal 2 protocol violation 1 not in patients best interest 302 started map treatment 300 started mapie treatment 1 not assessed for toxicity 2 not assessed for toxicity 301 assessable for toxicity ( safety population ) 298 assessable for toxicity ( safety population ) 40 terminated treatment early 8 treatment refusal 20 disease progression or recurrence 3 excessive toxicity 6 not in patients best interest 1 death 2 other 87 terminated treatment early 36 treatment refusal 21 disease progression or recurrence 16 excessive toxicity 7 not in patients best interest 1 lost to follow - up 1 death 5 other 261 completed map treatment 211 completed mapie treatment figure 1 : trial pro le * we later found out that one patient actually had a good histological response ( allocated to map group at randomisation and analysed as in the map group )  . 
 imaging recommendations during treatment included a chest ct , a bone scan , and a plain radiograph of the primary tumour at 4 - month intervals . cisplatin , doxorubicin , and methotrexate were administered at the same doses as given preoperatively . 
 ifosfamide ( high dose 14 g / m ) at 28 g / m per day with equidose mesna uroprotection was administered , followed by etoposide 100 mg / m per day over 1 h on days 15 ( three postoperative cycles )  . 
two additional cycles of ifosfamide 3 g / m per day with mesna uroprotection on days 13 ( 9 g / m ) were given , with standard doxorubicinvestigators were allowed to use supportive care with myeloid growth factor support according to local practice . 
 patients treated with map received 29 weeks of treatment or four cycles of map and two cycles of methotrexate and doxorubicin ( cisplatin was discontinued after a cumulative dose of 480 mg / m )  . 
the protocol provided recommendations for dose reductions on the basis of the toxicity ( from the common toxicity criteria ) and therapy delays . outcomes the primary outcome measure was event - free survival , de ned as the time from randomisation until rst event ( local recurrence , evidence of new or progressive metastatic disease , second malignancy , death , or a combination of those events ) or censoring at last contact . 
 secondary outcomes were overall survival ( de ned as the time from randomisation until death from any cause or last contact ) , short - term and long - term toxicity , and quality of life . 
questionaires were administered at baseline ( before cycle 2 ) , at week 2022 ( on active treatment ) , 18 months after start of treatment , and 3 years after starting treatment . 
 table 1 : baseline characteristics 1400 vol 17 october 2016 the treatment e ect was estimated separately in the prespeci ed localised disease subgroup , and in the following subgroups de ned post hoc : sex , age , site of disease , location of cancer on bone , and baseline metastases ( lung and non - lung )  . 
 01 02 this number was increased to more than 2000 registered patients overall , after the observed randomisation rate was lower than anticipated.19 the study required at least 378 event - free survival events and at least 378 deaths to detect absolute improvements of 10% from 45% to 55% in 3 - year event - free survival and 5 - year overall survival ( hazard ratio [ hr ] 075 ) with 5% two - sided signi cance levels and 80% power.24 the estimated sample size was calculated with the george and desu method , and although this number of events was not reached , the independent data monitoring committee recommended early release of data because of the lower than predicted event rate and low likelihood that the planned number of events would be reached in a reasonable time . 
 a preplanned subgroup analysis for patients with localised disease required 270 events to detect an 11% improvement , from 50% to 61% ( hr 071 ) in 3 - year event - free survival , and 5 - year survival ( two - sided signi cance level 5% , power 80% ) , assuming 85% of randomised patients would have localised disease ( 590 patients expected )  . primary and secondary outcomes were measured in the intention - to - treat population . 
the kaplan - meier method was used to estimate survival functions , log - rank test for di erences between survival curves and cox models ( adjusted for strati cation factors ) to estimate the treatment e ect . 
the haybittle - peto stopping rule was used , and the trial was planned to stop if the p value for the event - free survival analysis was less than 0001 . 
the interim analyses were designed to examine safety of the patients , and therefore the protocol prespeci ed that if at interim analysis , the lower bound of the 95% ci for the proportion of patients in each group who died because of toxicity exceeded 3% , the future of the trial would be discussed with the trial steering committee . the the proportionality of hazards for the treatment e ect over time was tested . 
in the presence of non - proportionality , the di erence between the groups was estimated with restricted mean survival time ( rmst ) 25 , 26 after tting a exible parametric model . 
 rmst for event - free survival measures a mean time - torst event , when time of consideration was restricted to t * years after randomisation ; here t * was 6 years . 
the consistency of treatment e ect in patients with localised or metastatic disease was tested by tting a exible parametric model with interaction between allocated treatment and metastases . vol 17 october 2016 1401 articles metastases , progression of existing metastases , death , or a combination of those events were considered a competing event for reporting second malignancy . 
 role of the funding source the funders of this study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 the corresponding author had full access to all data in the study and all authors had nal responsibility for the decision to submit for publication . results between april 14 , 2005 , and june 30 , 2011 , 2260 patients were registered until the overall recruitment target was reached . 
 618 patients were randomly assigned from the poor responders group : 310 to receive map and 308 to receive mapie ( gure 1 ) ; this was lower than the anticipated target of 693 . 
 median trial population was 621 months ( iqr 466766 ) ; 623 months ( iqr 469771 ) for the map group and 611 months ( iqr 465753 ) for the mapie group . 
for patients last reported alive and not lost to follow - up , 325 ( 87% ) of 373 had follow - up within 14 months before the data freeze . 
29 ( 9% ) of 310 patients in map and 23 ( 7% ) of 308 patients in mapie were permanently lost to follow - up more than 14 months before the data freeze . the entire follow - up for 307 event - free survival events were reported : 153 in the map group and 154 in the mapie group . 
the hr for event - free survival comparison in mapie versus map the was 098 ( 95% ci 078123 , p = 086 ) , but proportionality of hazards assumption did not hold mapie ( p = 00003 ) ; therefore , we estimated event - free survival with the rmst approach . 
mean time to rst event was 433 months ( 95% ci 401464 ) for patients allocated to the map group , and 441 months ( 411471 ) for patients allocated to the mapie group , over a period of 6 years from randomisation . 
 involved in both groups , metastases133 ( 87% ) of 153 patients in the map group and 129 ( 84% ) of 154 patients in the mapie group . the rst event mostly 247 event - free survival events were reported 541 patients with localised disease at the time of registration ( 118 in the map group and 129 in the mapie group ; gure 2 )  . 
3 - year event - free survival estimates in localised disease were 60% ( 95% ci 5466 ) in the map group and 57% ( 5163 ) in the mapie group . 
the hr was 103 ( 081133 , p = 080 ) but with considerable non - proportionality estimated rmst between the mapie and map groups was 005 months ( 47 to 48 ; p = 098 ; gure 2 )  . 
3 - year event - free survival in patients who had metastases at registration was 24% ( 1338 ) in the map group and 18% ( 633 ) in the mapie group . 
 received details of standardised postoperative chemotherapy doses , the number of patients who received the target number of chemotherapy doses , and the number of patients who received at least 80% of the planned dose are shown in table 2 . 
of the 77 patients with metastases at registration , 75 of 77 either had resection or resection was no longer needed and two of 75 were not operated on ( one in the mapie group due to clinicians and patients choice group vs one in the map group who was inoperable )  . toxicity data are available for 301 ( 997% ) of 302 map and 298 ( 993% ) of 300 patients in the mapie group who started treatment ( table 3 ) , and the remaining three patients were not assessed for toxicity ( one in the map group and two in the mapie group )  . 
received cisplatin dose and number of cycles are not known for one patient . table 2 : summary of patients who received postoperative map and mapie the site and are taken into consideration when highest grade toxicity reported was determined ( table 4 )  . 
the grades of the toxicities recorded during postoperative chemotherapy were similar between di erent treatment groups : worst toxicity of grade 3 or above was reported by 287 ( 95% ) of 301 patients in map and 281 ( 94% ) of 298 in mapie group ( table 4 )  . 
mapie was associated with more frequent grade 4 non - haematological toxicity ( 35 [ 12% ] of patients in the map group vs 71 [ 24% ] of 298 patients in the mapie group ) , mainly because of infections with absolute neutrophil count of less than 1 10 neutrophils per l , febrile neutropenia without documented infection , and hypophosphataemia ( table 4 )  . 
two patients died during postoperative therapy , one due to infection although they had a normal absolute neutrophil count ( map group ) , and one due to left ventricular ( mapie group )  . 
dose was reduced or delayed according to criteria in the protocol for 176 ( 58% ) of 301 patients in the map group and 184 ( 62% ) of 298 patients in the mapie group . 
three patients were not assessed for dose reduction or delay , one in the map group and two in the mapie group . systolic dysfunction left ventricular systolic dysfunction grade 3 events were reported in three ( 2% ) of 134 patients in the mapie group and one ( 1% ) of 136 in the map group . 
renal failure grade 3 ( four [ 3% ] of 138 patients ) and grade 4 ( one [ 1% ] of 138 patients ) events were reported in the mapie group but not in the map group . 
there was no consistent pattern of reversibility for left ventricular systolic dysfunction or renal events , as some patients improved , whereas others did not , but the number of events was too small to analyse further . 13 second primary malignancies were reported ( three in the map group vs ten in the mapie group ; appendix pp 5 , 6 )  . 
most of the second malignancies were myeloid ( myelodysplasia and acute myeloid leukaemia ) : two of three in the map group and eight of ten in the mapie group , mostly recording cytogenetic abnormalities causally associated with administration of alkylating drugs ( monosomy - 7 or chromosome - 5 abnormalities ) or etoposide ( 11q23 abnormalities )  . 
a longer follow - up will allow for more precise estimates . discussion standard treatment for high - grade osteosarcoma includes preoperative chemotherapy followed by surgical resection and postoperative chemotherapy.14 , 8 although previous uncontrolled studies3 , 5 , 19 suggested that altering therapy on the basis of histological response improved outcome , this had not been tested in randomised controlled trials . 
 euramos - 1 is , to the best of our knowledge , the rst collaboration to assess in a randomised manner whether altering chemotherapy on the basis of histological response improves outcome for patients with osteosarcoma . 
our results for patients with a poor histological response show that the addition of ifosfamide and etoposide to standard postoperative therapy does not improve outcome and rather increases the incidence of toxic e ects . 
 bilirubin data was collected by the cooperative osteosarcoma study group , the european osteosarcoma intergroup , and the scandinavian sarcoma group sites only . table 3 : postoperative treatment - related adverse events 1404 vol 17 october 2016 articles map ( n = 301 ) mapie ( n = 298 ) test p value * grade 3 grade 4 grade 5 total grade 3 or worse grade 3 grade 4 grade 5 total grade 3 or worse any toxicity 26 ( 9% ) 260 ( 86% ) non - haematological events 197 ( 65% ) 35 ( 12% ) 1 ( < 1% ) 1 ( < 1% ) 287 ( 95% ) 233 ( 77% ) 20 ( 7% ) 260 ( 87% ) 187 ( 63% ) 71 ( 24% ) 1 ( < 1% ) 1 ( < 1% ) 281 ( 94% ) 259 ( 87% ) p = 056 p = 00024 * comparison of grade 3 or higher toxicity . 
any toxicity , excluding neutropenia , thrombocytopenia , anaemia , and leucopenia . table 4 : summary of worst grade toxicity during postoperative chemotherapy chemotherapy a previous randomised controlled trial29 of around 240 patients assessed the addition of ifosfamide to standard map for patients with osteosarcoma . 
this trial included an upfront randomisation to map versus map plus ifosfamide , with postoperative ifosfamide given to those who had received it preoperatively or whose tumour showed a poor histological response ( < 90% necrosis )  . 
 on the basis of these data and our euramos results , we recommend continuing with the same chemotherapy as used preoperatively for patients with a poor histological response to preoperative treatment . 
 to preoperative map our results are also consistent with the results of a previous randomised controlled trial2 by the cog , which cog assessed the role of ifosfamide and mifamurtide in patients with osteosarcoma . 
the study assessed whether the addition of ifosfamide or mifamurtide to the map regimen improved long - term outcomes ; patients were treated preoperatively with either map or map plus ifosfamide , and subsequently postoperatively treated with or without mifamurtide . 
no di erence in histological response was observed after the preoperative period , and no di erence in event - free survival or overall survival was observed between the two chemotherapy groups . 
our results are also consistent with the conclusion of a meta - analysis30 where outcomes for osteosarcoma patients were improved with the use of at least three drugs , but no improvement was noted with the use of map plus ifosfamide versus map . lower euramos - 1 was complicated by a than anticipated randomisation rate , probably related to the timing of the randomisation , close to the time of the intervention , after patients had been exposed to signi cant treatment - related toxicities . 
non - randomisation was 42% in known poor responders and occurred in all four trial groups ( cog , coss , eoi , and ssg ) ranging between 33% and 45% . 
most as anticipated , a larger number of mapie - treated patients developed second malignancies than patients treated with map , although the di erence was not statistically second malignancies were myeloid in origin , which is not unexpected given the short follow - up and the natural history of therapy - related myeloid disorders.31 , 32 the cytogenetic abnormalities in some of these leukaemias were consistent with exposure to alkylating drugs32 and etoposide.33 although second solid malignancies are more common after combined modality therapy , including irradiation , 34 alkylating drugs also contribute to this risk . 
overall survival will additionally be analysed with longer follow - up . the number of events was lower than anticipated , as event - free survival results were based on 307 event - free survival events , rather than the planned 378 ; event rate was lower than predicted and our 3 - year event - free survival estimate for map was 55% ( 95% ci 4960 ) rather than 45% . 
therefore early imaging assessments might not have been identically timed by group , resulting in the apparent early separation observed in the event - free survival curve in favour of the mapie group . 
 the timing of our intervention might have been too late because the rst cycle of ifosfamide plus etoposide was administered at week 17 ( 5 weeks from resumption of postoperative therapy )  . 
 ultimately , the best strategy for patients with a poor histological response might not be therapy intensi cation since this approach has been unsuccessful in childhood soft tissue sarcomas35 and in a previous study in osteosarcoma.4 the use of functional imaging early during treatment might identify patients who will have a poor response and allow incorporation of alternative treatment strategies earlier . 
 we included patients with both initially localised and initially metastatic disease in the same trial because it was not always possible to di erentiate up - front between patients with localised disease and those with vol 17 october 2016 1405 articles metastatic disease , and we have therefore also included patients with possible metastatic disease ; other prognostic factors are the same in patients with both metastatic and localised disease . 
 the 3 - year event - free survival for patients with metastases was 24% ( 1338 ) in the map group and 18% ( 633 ) in the mapie group , and these results are similar to those of other published series.37 , 38 the euramos - 1 trial included only 77 patients with metastases , which makes it di cult to draw rm conclusions regarding the outcome for these patients . 
 additionally , since the euramos - 1 patients with metastases needed to have resectable disease , the population included might not be entirely comparable to those included in the previous trials . 
because the study question was whether altering therapy on the basis of histological response improved outcome , we do not think collection of those data is crucial to the study results overall . 
 this is a potential limitation especially because patients treated in the experimental group appeared to receive less of the intended therapy . increases review the addition of mifamurtide to the map chemotherapy regimen for patients with localised osteosarcoma resulted in improved overall survival.2 the drug was approved for use in europe on the basis of those results , but has not been approved for use in the usa . 
we have subsequently reached an apparent plateau in outcomes for patients with osteosarcoma.39 the development of strategies to better understand the biology of this tumour40 might aid in the identi cation of drug targets . 
collaboration with veterinary oncologists might speed up target identi cation in human beings as canine osteosarcoma is more common than human osteosarcoma.41 genome - wide analysis of osteosarcoma samples might also help identify important targetable genetic mutations.42 the identi cation of genetic alterations that could be used as therapeutic targets is an important step to develop better treatment approaches . overall , euramos - 1 showed that treatment with mapie resulted in similar event - free survival to map , results in increased toxicity , decrease in total received doses , and more second malignancies . 
 all authors collated data and interpreted the data , and reviewed and approved the nal manuscript . declaration of interests nmm reports personal fees from jazz pharmaceutical , outside the submitted work . 
ssb reports grants from deutsche krebshilfe , deutsche forschungsgemeinschaft , and european science foundation , during the conduct of the study ; personal fees from lilly , bayer , celgene , clinigen , chugai , merck , roche , takeda millenium / idm , and p zer , outside the submitted work . 
gj reports grants from cancer research uk , grants from medical research council uk , during the conduct of the study , and grants from cancer research uk , outside of the submitted work . 
jmh reports grants from cancer research uk , medical research council uk , during the conduct of the study ; and grants from cancer research uk , outside of the submitted work . 
tb - b reports grants from federal ministry of education and research , and other fees from the european science foundation under the eurocores program european clinical trials and deutsche forschungsgemeinschaft , during the conduct of the study . 
pjl reports other fees from childrens oncology group , during the conduct of the study and other fees from eleison 1406 vol 17 october 2016 articles pharmaceuticals llc , outside of the submitted work . 
mrs reports grants and nonnancial support from sano - aventis , novartis , p zer , janssen , and astellas , and nonnancial support from merck , all outside of the submitted work . 
we aimed to test combined genomic and microenvironmental indices in prostate cancer to improve risk strati cation and complement clinical prognostic factors . methods we used dna - based indices alone or in combination with intra - prostatic hypoxia measurements to develop four prognostic indices in 126 low - risk to intermediate - risk patients ( toronto cohort ) who will receive image - guided radiotherapy . 
we validated these indices in two independent cohorts of 154 ( memorial sloan kettering cancer center cohort [ mskcc ] cohort ) and 117 ( cambridge cohort ) radical prostatectomy specimens from low - risk to high - risk patients . 
our primary endpoint was the development of a set of prognostic measures capable of stratifying patients for risk of biochemical relapse 5 years after primary treatment . findings biochemical relapse was associated with indices of tumour hypoxia , genomic instability , and genomic subtypes based on multivariate analyses . 
genomic instability is prognostic for relapse in both image - guided radiotherapy ( multivariate analysis hazard ratio [ hr ] 45 [ 95% ci 2198 ] ; p = 000013 ; area under the receiver operator curve [ auc ] 070 [ 95% ci 065076 ] ) and radical prostatectomy ( 40 [ 1697 ] ; p = 00024 ; auc 057 [ 052061 ] ) patients with prostate cancer , and its e ect is magni ed by intratumoral hypoxia ( 38 [ 1212 ] ; p = 0019 ; auc 067 [ 061073 ] )  . 
a novel 100 - loci dna signature accurately classi ed treatment outcome in the mskcc low - risk to intermediate - risk cohort ( multivariate analysis hr 61 [ 95% ci 2019 ] ; p = 00015 ; auc 074 [ 95% ci 065083 ] )  . 
in the independent mskcc and cambridge cohorts , this signature identi ed low - risk to high - risk patients who were most likely to fail treatment within 18 months ( combined cohorts multivariate analysis hr 29 [ 95% ci 1460 ] ; p = 00039 ; auc 068 [ 95% ci 063073 ] ) , and was better at predicting biochemical relapse than 23 previously published rna signatures . interpretation this is the rst study of cancer outcome to integrate dna - based and microenvironment - based failure indices to predict patient outcome . 
by contrast , patients with intermediate risk ( gleason scores of 7 , psa concentrations of 1020 ng / ml , or t2b - c ) and high risk or locally advanced ( gleason scores 8 , prostate speci c antigen concentrations 20 ng / ml , or t3 / 4 ) prostate cancer often undergo radical prostatectomy or image - guided radiotherapy , or receive intensi ed regimens adding adjuvant androgen deprivation therapy or novel systemic drugs to prevent progression to metastatic castration - resistant prostate cancer . 
however , use of treatment intensi cation for individual patients is imprecise : 3050% of patients have biochemical relapse despite radical prostatectomy or image - guided radiotherapy.4 , 5 furthermore , nearly 20% of intermediate - risk patients have biochemical failure within 18 months of primary local therapy ( ie , rapid failure )  . 
such failure might be be due to pre - existing occult metastatic disease , because rapid biochemical failure for prostate - cancer - speci c mortality.6 , 7 the basis of this interpatient clinical heterogeneity has not been clinically resolved.8 , 9 is a surrogate a signature to classify patients as potential responders or non - responders to local therapy would have great clinical use if it was treatment - independent ( ie , e ective both for patients undergoing radical prostatectomy or image - guided radiotherapy ) and could be done on initial diagnostic biopsies . 
such a signature could triage patients at greatest risk of failure into clinical trials for treatment intensi cation and justify potential added toxic e ects.7 , 10 dna copy number alterations in pten , nkx3 - 1 , myc , and star are associated with adverse prognosis , 11 , 12 and rna - based gene signatures might di erentiate indolent and non - indolent , lethal prostate cancer.13 - 15 tmprss2erg fusion status does not predict prognosis after radical prostatectomy or image - guided radiotherapy.16 , 17 importantly , tumour cells exist within a heterogeneous tumour microenvironment with dynamic gradients of hypoxia that have been linked to metastatic potential.9 , 18 indeed , patients with prostate cancer with hypoxic tumours rapidly fail treatment ( eg , within 2 years ) after radical prostatectomy or image - guided radiotherapy.19 , 20 up to now , the interplay of genomic instability and tumour microenvironment in modulation of treatment outcome has been unexplored . 
we therefore aimed to develop clinically relevant prognostic indices , with and microenvironmental indices , to robustly predict patient outcome . tumour dna integrated use signatures methods study design and patients our training ( toronto ) cohort for generation of biopsyconsisted of pre - image - guided based radiotherapy , clinically - staged patients with prostate cancer , who were classi ed as low - risk or intermediaterisk on the basis of national comprehensive cancer network guidelines ( appendix ) .3 to validate our ndings , we used copy number alteration pro les from two cohorts of clinically staged ( ie , similar to pre - imageguided radiotherapy patients ) low - risk to high - risk radical prostatectomy patients ( memorial sloan kettering cancer center cohort [ mskcc ] and cambridge cohorts ; appendix ) .8 the radical prostatectomy cohorts were considered both separately and together . 
second , we used the percentage of a patients genome harbouring copy number alterations ( percent genome alteration ) as a surrogate for genomic instability , and assessed this proportion together with tumour hypoxia . 
third , we undertook supervised machine learning with a random forest21 to develop a statistical model , resulting in a dna signature , which classi ed patients at risk of biochemical relapse on the basis of their copy - number pro les . 
we compared the resulting signature with published rnabased signatures . for and , increase ( de ned as an radiotherapy patients statistical analysis our main aim was the development of a set of prognostic measures capable of stratifying patients for risk of biochemical relapse concentration of prostate - speci c antigen of at least 2 ng / ml above the post - radiation nadir value for imageguided radical prostatectomy patients , as two consecutive concentration values > 02 ng / ml or triggered salvage radiotherapy22 , 23 ) 5 years after primary treatment . 
we modelled indices with univariate and multivariate analyses , with multivariate analyses correcting for gleason score and pre - treatment concentrations of psa ( and clinical t stage during assessment of high - risk patients ; appendix )  . 
all authors had full access to all the data in the study and the corresponding author had nal responsibility for the decision to submit for publication . results we used information derived from 126 pre - imageguided radiotherapy biopsies ( toronto cohort ) and did initial validation with 154 radical prostatectomy specimens ( mskcc cohort )  . 
we focused on clinically - matched validation cohorts containing intermediate - risk patients ( n = 210 ) who might need treatment intensi cation beyond local therapy alone , but also considered all patients with localised disease who might be candidates for intensi cation or de - intensi cation ( full validation cohort n = 271 )  . 
pretreatment psa was prognostic in imageguided radiotherapy patients , whereas pretreatment gleason score , t category , and psa were all prognostic in the full mskcc and cambridge cohorts ( table 1 )  . low - risk and our initial analyses showed that toronto and mskcc cohorts showed extensive genomic heterogeneity , even for patients who were low - risk or intermediate - risk , or had gleason scores of 6 or 7 ( appendix pp 13 , 4043 )  . 
the most recurrent copy number alterations in either cohort were 8p ampli cations and 8q deletions , in addition to deletions of 16q232 and 6q15 ( harbouring maf and map3k7 ; table 2 ) , which have been noted in aggressive tumours.24 we established the frequency of copy number alterations for a set of genes putatively prognostic for adverse outcomes , selected from our previous studies and image - guided radiotherapy biopsies ( appendix p 44 )  . 
we noted this variability across the genome , suggesting that genomically de ned subtypes of prostate cancer might be obtained from biopsies . the toronto literature , the unbiased hierarchical clustering in the toronto cohort ( appendix pp 4546 ) showed four localised prostate cancer subtypes with distinct genomic pro les : subtype 1 ( characterised by gain of chromosome 7 ) , subtype 2 ( deletion of 8p and gain of 8q ) , subtype 3 ( loss of 8p and 16q ) , and subtype 4 ( so - called quiet genomes due to few genomic alterations )  . 
for the toronto - igrt cohort , in which there were only low - risk to intermediate - risk patients , we compared t2t1 patients , whereas for the radical prostatectomy cohorts , we compared t3 patients with t12 patients . 
data are provided for dichotomised and continuous pga in each cohort , on the basis of cox proportional hazard models including only the marker of interest ( univariate ) and models including relevant clinical covariates as shown in the table ( multivariate )  . 
 * genes with most copy number alterations or those with known or putative cancer associations . table 2 : most recurrently aberrant regions | || | ||| || || || || | || || | | || || |||||| | | | || || || subtype 1 subtype 2 subtype 3 subtype 4 number at risk subtype 1 subtype 2 subtype 3 subtype 4 log - rank p < 00001 time ( years ) figure 1 : kaplan - meier analysis of biochemical - relapse free survival for patients strati ed by tumour subtype subtype 2 and 16q deletion in subtype 3 ( appendix p 14 )  . 
 all four subtypes were con rmed in the mskcc radical prostatectomy cohort and were not associated with tmprss2erg fusion , gleason score , or t category ( appendix pp 1517 , 4748 )  . in a pooled analysis of low - risk and intermediate - risk patients ( using the toronto and mskcc cohorts ; 250 patients ) , the four genomic subtypes of localised prostate cancer had signi cantly di erent prognoses , even after adjustment for clinical variables ( gure 1 , appendix pp 1519 , 4349 )  . 
biochemical relapse - free survival at 5 years was 58% ( 95% ci 3792 ) for subtype 1 , 55% ( 3781 ) for subtype 2 , 53% ( 3778 ) for subtype 3 , and 89% ( 8494 ) for subtype 4 . 
with the percentage of the genome showing a copy number alteration as a proxy for genomic instability , we noted interpatient variability in percentage of genome alteration ranging from 052% in the toronto cohort , to 034% in the mskcc cohort , and 028% in the cambridge cohort . 
indeed , individual gleason score - 6 tumours had a higher percentage of genome alteration than did some gleason score 4 + 3 tumours ( gure 2a ) , suggesting that percentage of genome alteration re nes biological description even in tumours of mainly pattern 4 . 
as expected , based on previous ndings , the percentage of genome alteration was increased in patients with prognostic chd1 deletions ( appendix p 50 ) .25 percentage of genome alteration was strongly prognostic , independent of clinical covariates , as previously reported.26 every 1% increase in percentage of alteration led to a 58% decrease in 5 - year biochemical relapse - free survival ( c - index 060072 ; appendix pp 2021 )  . 
to classify the likelihood of clinical failure on the basis of percentage of genome alteration , we set the upper tertile of 749% from the toronto cohort as the lower bound threshold , which e ciently strati ed patients who underwent either image - guided radiotherapy ( multivariate analysis hr for biochemical relapse 45 [ 95% ci 2198 ] ; wald p = 000013 ) or radical prostatectomy ( eg , pooled radical prostatectomy low - risk to intermediate - risk cohort : multivariate analysis hr for biochemical relapse 40 [ 1697 ] ; wald p = 00024 ; gure 3ac )  . 
the hr for the pooled radical prostatectomy full ( ie , low , intermediate , and high - risk ) cohort at 5 years was 27 ( 95% ci 1548 ; p = 00024 ; auc 057 [ 95% ci 052061 ] )  . 
percentage of genome alteration strati es patients at risk of rapid failure consistent with occult metastases , and was increased in 1524 vol 15 december 2014 articles outcome ( biochemical relapse - free survival at 5 years was 93% ) , whereas those with high levels of both measures had the worst ( 49% ; gure 4d )  . 
after the addition of percentage of genome alteration to the multivariate cox proportional hazard model for subtypes , only subtypes 2 and 3 remained prognostic , suggesting that their prognostic ability stems from both speci c genetic aberrations and general genomic instability ( appendix p 18 )  . hypoxia is an important aspect of cancer metabolism and in itself can be prognostic in patients with prostate cancer.19 , 20 we used three hypoxia rna signatures that have been validated in other tumour types to estimate hypoxia within the pooled radical prostatectomy mrna cohorts ( 108 mskcc patients and 110 cambridge patients ; table 3 and gure 4ac ; appendix p 22 ) .2729 none of these signatures were univariately prognostic , nor were they related to gleason score , psa , t category , or percentage of genome alteration ( appendix 5659 )  . 
 however , when we separated patients into four groups on the basis of high versus low percentage of genome alteration and high versus low hypoxia values , we found that hypoxia increased the prognostic accuracy of the percentage genome alteration for risk of biochemical relapse . 
patients with a high percentage of alteration and high hypoxia have the worst prognosis , whereas those with high hypoxia alone ( low percentage of alteration ) responded well after radical prostatectomy ( gure 4ac , appendix pp 2324 , 6061 )  . less to validate this nding , we used the toronto cohort the biobanking of frozen biopsies was because completed with simultaneous and direct assessment of tumour hypoxia at the same intraprostatic locale.20 this cohort therefore contained direct measurements of for hypoxia denoted by patient - speci c values proportion of oxygen measurements than 20 mm hg ( hp20 ; appendix p 25 ) .20 the median hp20 in our cohort was 81% ( range 6493 )  . 
 * the cox proportional hazard model was t with four levels ( percentage of genome alteration status / hypoxia status : + / + , + / , / + , and / , whereby + / + patients had a high percentage of genome alteration and high hypoxia , + / patients had high a high percentage of genome alteration and low hypoxia , etc ) , with / patients used as the baseline group . 
 table 3 : data for patients strati ed by hypoxia percentage of genome alteration and hypoxia ( unadjusted hr for biochemical relapse 38 [ 95% ci 1212 ] ; wald p = 0019 ; appendix pp 2627 ) when used as a combined prognostic index . 
again , patients whose tumour solely showed hypoxia , but not genome alteration , fared better than expected for patients with hypoxic tumours after image - guided radiotherapy , suggesting that cohorts of patients with high hypoxia and a high percentage of genome alteration could bene t from treatment intensi cation . because speci c genes ( gure 1 ) , general genomic instability ( gures 2 , 3 ) , and tumour microenvironment ( gure 4 ) all play a part in determination of patient prognosis , we postulated that a supervised machine learning approach would capture the complex and unknown interactions between genes underlying these events . 
using a random forest21 classi er trained on the toronto cohort , we developed a biopsy - driven prognostic signature that predicts biochemical failure and could guide clinical decisions before , and independent of , treatment ( appendix pp 6667 )  . 
 we rst veri ed the signature in the independent lowrisk and intermediate - risk mskcc cohort , in which it predicted biochemical relapse with an area under the curve of 074 ( 95% ci 065083 )  . 
 58% ( 95% ci 3596 ) of patients in the mskcc low - risk to intermediate - risk groups who were classi ed as poor prognosis were biochemical relapse - free at 5 years , compared with 89% ( 8596 ) for those classi ed as good prognosis , and this di erence remained signi cant after adjustment for clinical covariates ( multivariate analysis hr for biochemical relapse 61 [ 95% ci 2019 ] ; wald p = 00015 ; appendix pp 29 , 70 )  . 
 importantly , our signature e ectively identi ed patients at risk of relapse within 18 months in the full mskcc cohort , despite not including any high - risk patients in the initial training cohort ( 33 [ 1110 ] ; wald p = 0038 )  . 
 we validated this early - failure e ect in a second independent cambridge cohort ( 28 [ 1794 ] ; wald p = 0050 ; appendix pp 30 , 70 )  . 
when genomic instability ( pga ) and hypoxia ( hp20 ) were combined within the same patient , we noted a multiplicative and independent prognostic e ect in image - guided radiotherapy patients ( d )  . 
 importantly , the signature also identi ed patients who go on to develop metastasis ( auc 078 [ 95% ci 063093 ] ; appendix p 76 )  . to underpin the potential use of our dna signature , we noted that the signature had auc and c - index values that were greater than 97% ( 970 000 / 1 000 000 ) of the empirical null distribution from randomly sampled genesets ( appendix p 77 )  . 
furthermore , our signature outperformed 23 previously published rna signatures for prostate cancer biochemical relapse - free survival rates after training of random forests with a cohort of 1299 low - risk to high - risk patients with prostate cancer ( including 293 low - risk to intermediaterisk patients ) with mrna microarray data ( gure 6 )  . 
 application of these trained forests to the 108 mskcc patients with information about both mrna and copy number alteration showed that our dna signature has the highest overall auc ( gure 6a , b ; appendix pp 31 , 78 )  . there is a low alteration rate for most of the genes identi ed in the signature : 154 ( 56% ) of 276 genes had copy - number alterations in zero to 39 patients ( of a total sample size of 397 patients ) , which is less than 10% of the total combined cohorts size ( appendix p 79 )  . 
 vol 15 december 2014 1527 articles ||||| ||| | | ||||| | |||| ||| || | |||||||| | ||||| | | |||| || | | ||||||| || | || | ||||| || ||||| | || |||| | |||| |||| |||| ||| | ||| || | hr 27 ( 95% ci 1264 ) ; p = 0021 signature negative signature positive number at risk signature negative signature positive time ( years ) ||||| | | | ||| || | hr 29 ( 95% ci 1460 ) ; p = 0039 number at risk signature negative signature positive time ( months ) figure 5 : a prognostic dna signature for prostate cancer multivariate cox proportional hazard model adjusting for clinical covariates ( gleason score and pretreatment psa ) in the low - risk and intermediate - risk groups ( a ) and when applied to the full pooled radical prostatectomy cohort ( n = 271 ) the signature for copy number alteration identi es patients who will fail rapidly ( b )  . 
signature negative = patients whose tumour genomics were negative for the dna signature . these results strongly support the use of multigene models , because our biopsy - based dna signature outperformed reported prognostic genes ( appendix p 80 )  . 
notably , genes in these regions relate to lipid metabolism ( appendix p 82 )  . tumours have signi cantly we noted that the signature directly accounts for genomic instability ( appendix pp 8285 )  . 
first , patients lower with subtype - 4 signature risk scores than do those with other subtypes ( median 017 [ iqr 00026032 ] vs 041 [ 031061 ] ; p < 00001 , two - sided mann - whitney u test )  . 
second , percentage of genome alteration di ers signi cantly between the classes predicted by the signature and can be estimated from the gene signature ( spearmans correlation between whole - genome and signatureestimated percentage of genome alteration pga ( cid : 1 ) 073 ; thereby providing similar prognostic p < 00001 ) , information . 
importantly , signature - based estimates of percentage of alteration remain highly prognostic , and the addition of 30 genes ( selected from the toronto cohort ) improves estimates of percentage of alteration in the validation cohorts ( eg , mskcc : spearmans ( cid : 1 ) 073 vs 087 ; p < 00001 ; appendix p 32 )  . 
the hr of percentage of genome alteration as a continous variable estimated from these 306 genes is identical to that of the true percentage of genome alteration in the mskcc cohort and nearly identical to that of the cambridge cohort . 
taken together , these results show that our treatment - independent dna - prognostic signature measures genomic instability in addition to lipid metabolism pathways , suggesting our signature might identify candidates for treatment - intensi cation trials targetting these processes ( appendix pp 8691 )  . discussion our ndings show that combined indices of genomic instability and hypoxia can improve accuracy of prognosis in patients with localised prostate cancer in the context of present clinicopathological variables . 
development of prostate - cancer biomarkers to guide disease management at the time of diagnosis is a di cult but crucial challenge in view of the high rates of overtreatment and clinical relapse.30 initial investigation in the toronto cohort showed striking genomic heterogeneity in the pretreatment biopsies from these patients , and has implications for the discovery of driver mutations in prostate cancer . 
 identify inclusion of additional patients from the independent mskcc cohort of low - risk and intermediate - risk patients mskcc full cohort cambridge full cohort * univariate multivariate univariate multivariate 100 - loci dna signature 40 ( 2081 ; 000011 ) 28 ( 1460 ; 00060 ) 29 ( 1182 ; 0038 ) 29 ( 1082 ; 0050 ) c index 074 ( 068080 ) 084 ( 078089 ) 064 ( 057071 ) 075 ( 068083 ) 070 ( 061080 ) 074 ( 065083 ) 067 ( 054079 ) 073 ( 062085 ) data are hazard ratio ( 95% ci ; p value ) or hazard ratio ( 95% ci )  . 
data are provided for the 100 - loci dna signature in each full validation cohort on the basis of cox proportional hazard models including only the marker of interest ( univariate ) and models including relevant clinical covariates as in the multivariate models in table 1 ( multivariate )  . 
 * data are based on 18 - month biochemical recurrence . table 4 : performance of the 100 - loci dna signature 1528 vol 15 december 2014 articles cna_rf cuzick lapointe saal glinsky genomichealth talantov ramaswamy stephenson clinical singh bismar long varambally bibikova cna_rf glinsky cuzick saal bibikova lapointe bismar genomichealth ramaswamy varambally singh long clinical talantov stephenson led to larger subtype sizes amenable to analyses of biochemical relapse - free survival , showing signi cant di erences in patient outcome according to subtype . 
 patients agged by our copy - number alteration - based signature had biochemical relapse rates that were increased by up to six times , and were at risk of failure within 18 months , all within the clinical context of gleason score , t category , and psa . 
in particular , this signature is highly e ective for low - risk patients , because it can identify those ineligible for active surveillance and provide additional assurance for those who are . 
for instance , if the dna signature was used by clinicians today , of 1000 patients diagnosed with localised disease , 144 patients would be o ered more aggressive treatment ( all signature - positive patients ) and 650 would have the support for active surveillance instead of local treatment ( low - risk signature - negative patients )  . intermediate - risk to an image - guided preclinical experimental work supports hypoxia generating a mutator phenotype ( decreased dna repair leading increased mutation rate and genomic instability ) and selecting for genetically unstable clones , in addition increased capacity for distant metastases.18 this metastatic phenotype occurs independently of local treatment ; hypoxia is associated with both local relapse after image - guided radiotherapy and biochemical failure and distant metastasis in patients receiving radical prostatectomy for prostate cancer.19 , 20 here we have shown that simultaneous measurement of tumour hypoxia and genomic improve the prognostic capability of a pretreatment biopsy by combining the independent biology of cancer genomics with the tumour microenvironment . 
moreover , the poor prognosis previously associated with hypoxia19 , 20 might have been related to genomic instability within a subset of these specimens , because hypoxia itself was not associated with poor prognosis in the absence of a heightened percentage of genome alteration . instability can radiotherapy led cancer - cell metabolism ( increased glycolysis , high lactate , and hypoxia ) is related to oncogene activation and loss of tumour suppressor genes , and increased lipid and fatty acid synthesis have been associated with progression of prostate cancer.31 , 32 therefore it is striking that our supervised machine - learning approach the discovery of a genetic signature enriched for genes involved in lipid biology . 
combined with the nding that constitutive activation of mtorc1 renders hypoxic cells lipids , our dependent on exogenous desaturated signature could represent abnormalities in cancer metabolism amenable to targeting of lipid synthesis.3134 further more , our signature e ciently captures the prognostic e ect of percentage of genome alterationa surrogate for genomic instability . 
because androgen deprivation therapy improves oxygenation35 and reduces dna repair36 in patients with prostate cancer , we speculate that such therapies targeting hypoxia and figure 6 : training and comparison of random forest signatures for 23 previously published rna signatures for biochemical relapse - free survival we trained a clinical model ( in green ) with clinical variables : pretreatment psa , biopsy - based gleason score , and t category . 
we compared our dna - based signature ( cna_rf , shown in red ) with these signatures in the 108 memorial sloan kettering cancer center patients with information about both mrna and cna . 
the dna , rna , and clinical signatures were trained in a cohort of 293 lowrisk to intermediate - risk patients with prostate cancer ( a ) and 1299 low - risk to high - risk patients ( b ) , including some with locally advanced disease . 
patients agged by our signature might intensi cation with bene t androgen deprivation therapy or other systemic therapies from patient - speci c vol 15 december 2014 1529 articles to o set both local and systemic resistance , independent of primary treatment . to our knowledge , this is the rst report of biopsydriven , dna - based indices that predicts prognosis in patients who received either image - guided radiotherapy or radical prostatectomy as primary therapy for patients with prostate cancer ( panel )  . 
dna alterations might be less variable than rna abundance patterns within intraprostatic biopsies from dynamic tumour microenvironments , and more stable ex vivo during formalinxed , para n - embedded protocols . 
because our training cohort was obtained before primary the characterisation of complex indices , showing a priori interpatient heterogeneity , soon after diagnostic mriguided or transurethral ultrasound - guided biopsies . 
 indeed , we have shown that frozen biopsies are amenable to whole - genome sequencing to assess in genomic aberrations intrapatient heterogeneity ( boutros pc , unpublished )  . therapy , our study supports our study has several caveats . 
 nonetheless , our identi cation of patients with metastasis , and can identify patients who will have biochemical relapse before 18 months , which has been shown to be predictive for prostate cancer - speci c mortality.6 , 7 although the cohorts shows promise signature panel : research in context systematic review we reviewed previous studies on the basis of pubmed searches done between jan 1 , 1990 , and dec 31 , 2013 , with the terms : genomics , dna , rna , hypoxia , prognosis , radiotherapy , surgery , radical prostatectomy , acgh , rna expression , arrays , classi er , and biomarker . 
we focused on multigene indices that had been validated in at least one cohort , and noted many previously published rna signatures for prognosis in prostate cancer and for hypoxia in various tissue types . 
to the best of our knowledge , no multigene dna signature exists , and no biomarker assesses genomics and the tumour microenvironment simultaneously . interpretation we propose the use of dna - based and rna - based signatures to measure genomic instability and tumour hypoxia to guide clinical management of patients with primary diagnostic biopsies . 
our 100 - loci dna signature , which measures genomic instability and is enriched for lipid metabolism genes , outperforms previously published rna - based prognostic signatures for prostate cancer . 
once our assays undergo clinical quality assurance protocols within a hospital setting , clinicians can use this assay to divert patients to appropriate clinical trials . di er slightly in the distribution of clinicopathological factors , these di erences changed neither treatment nor survival , making it very unlikely that the di erences a ect the interpretation of our results . 
we will explore this outcome in new cohorts of patients treated with imageguided radiotherapy or radical prostatectomy with or without androgen deprivation therapy , and assess whether the biomarker would become a predictive , rather than a solely prognostic , biomarker . from a technical perspective , despite di erent resolutions between the copy number alteration platforms used for each cohort , the copy number alteration indices developed in the toronto cohort validated in the radical prostatectomy cohorts . 
in future studies we will characterise the dna , rna , and epigenetic pro les of foci within patients who receive oral pimonidazole before treatment to investigate the genomichypoxia prognostic association in ner detail . 
finally , e orts are underway to reduce the signature size without loss of prognostic information related to metabolism or genomic instability , and to improve the sensitivity of our signature with multimodal data sets ( eg , combined dna , rna and epigenetic analyses ) emerging from studies from the international cancer genome consortium and the cancer genome atlas . instability the use of genomic identi cation of the correct patients to treat while avoiding overtreatment in the low - risk to intermediaterisk group remains an important clinical dilemma . 
we and envision microenvironment signatures to divert patients from present clinical risk categories to novel clinical trials of treatment intensi cation , whereby patients with poor prognosis based on these novel biomarkers can be enrolled into trials that add combined local and systemic therapies . 
additionally , low - risk and intermediate - risk patients with low levels of hypoxia and and low percentages of genome alteration could be entered into clinical trials of active surveillance . 
these precision medicine approaches set the stage for novel treatment intensi cation and treatment deintensi cation trials to either increase cure rates by prevention of progression to metastatic castration - resistant prostate cancer or to reduce the burden of overtreatment . contributors el contributed to the bioinformatics analysis , machine learning , the statistical analysis , visualisation , and manuscript preparation . 
rgb contributed to study design , clinical analysis , and manuscript preparation declaration of interest el , pcb , and rgb have a patent biopsy - driven genomic signature for prostate cancer prognosis pending . 
 lll has a patent bladder cancer diagnostics pending , and ed has a patent systems and methods for expression - based discrimination of distinct clinical disease states in prostate cancer pending . 
 acknowledgments we thank study volunteers for their participation , and sta at the wellcome trust clinical research facility , addenbrookes clinical research centre , cambridge , uk for their help in conducting the study . 
 this study was done with the support of movember funds through prostate cancer canada and with the additional support of the ontario institute for cancer research , funded by the government of ontario and by a doctoral fellowship from the canadian institute for health research to el . 
we acknowledge the support of the national institutes of health research cambridge biomedical research centre and the national cancer research prostate cancer : mechanisms of progression and treatment ( prompt ) collaborative ( grant code g0500966 / 75466 ) , which has funded tissue and urine collections in cambridge . 
we acknowledge the support of the university of cambridge , cancer research uk and hutchison whampoa limited , and the support of cancer research uk cambridge institute genomics and bioinformatics core facilities . 
rgb is a recipient of a canadian cancer society research scientist award . articles e ect of hiv on survival in patients with non - small - cell lung cancer in the era of highly active antiretroviral therapy : a population - based study ramesh rengan , nandita mitra , kaijun liao , katrina armstrong , anil vachani summary background hiv - infected patients with lung cancer have been reported to have poorer survival than uninfected patients . 
we examined the e ect of hiv infection on clinical outcome in patients with lung cancer who are also receiving haart . methods patients diagnosed with non - small - cell lung cancer ( nsclc ) from jan 1 , 2000 , to dec 31 , 2005 , with or without hiv infection were identi ed by querying the surveillance , epidemiology , and end results registry and the medicare lung cancer database . 
survival analysis by stage and treatment delivered comparing the hiv - infected patients with uninfected controls was done with kaplan - meier and cox models with propensity score adjustments . findings 71 976 patients with nsclc were identi ed as uninfected controls and 322 patients with nsclc were identi ed in the hiv group ; median age was 75 years for both groups . 
median overall survival for all stages was 70 months ( 95% ci 7070 ) for uninfected controls versus 80 months ( 60100 ) for the hiv group ( p = 016 ) ; for those with stage i / ii disease it was 370 months ( 360390 ) versus 430 months ( 260580 ; p = 037 ) ; for those with stage iiia / iiib disease it was 70 months ( 7070 ) versus 30 months ( 2080 ; p = 0051 ) ; and for those with stage iv disease it was 30 months for both groups ( 95% ci 3030 for controls ; 2050 for hiv group ; p = 077 )  . 
since the adoption of haart in the mid - 1990s , the expected survival of patients with hiv has improved substantially.21 , 22 although haart e ectively treats the immunosuppression associated with hiv infection , data also suggest that these drugs could diminish the e cacy of the antineoplastic regimens routinely used in the treatment of lung cancer.23 therefore , the clinical outcome of hiv - infected patients with lung cancer in the era of haart remains unclear . our study was designed to assess overall survival in hiv - infected patients with nsclc in the era of haart compared with uninfected patients . 
additionally , for patients with early stage nsclc , for whom surgical resection is the standard of care , we have assessed overall survival in hiv - infected patients after surgical resection as compared with uninfected patients . 
our goal was to establish whether nsclc displayed a more aggressive phenotype in hiv - infected individuals , to quantify the e ect of viral infection on clinical outcome in patients with nsclc . 
the broader objective was to establish the role that hiv infection should have in clinical decision making in patients with nsclc . methods study design the seer - medicare database is the result of a linkage of two population - based data sources : the surveillance , epidemiology and end results ( seer ) registry , sponsored by the us national cancer institute ( nci ) , and medicare , a federally funded us programme that hiv + ( n = 322 ) control ( n = 71 976 ) p value for more on seer see median age ( iqr ) 75 ( 6981 ) 75 ( 6981 ) stage i / ii stage iiia / iiib stage iv race white african american other comorbidities 2 or more median income in bottom two quartiles ( range in us dollars ) table : patient characteristics 3540% 2981% 3478% 20 016 22 793 29 167 7174% 2360% 466% 497% 870% 8634% 4317 ( 732 492 ) 62 859 6056 3061 6164 11 660 54 152 33 117 2781% 3167% 4050% 8733% 841% 425% 856% 1620% 7524% 4601 ( 732 492 ) 0002 048 004 099 < 00001 < 00001 072 002 00003 < 00001 065 pro vides health insurance for people of age 65 years and over , disabled , or have end - stage renal disease . 
the linkage to medicare provides longitudinal data for all claims from the center for medicare and medicaid services from the time of eligibility to death.24 , 25 patients younger than 65 years are excluded from this registry unless they are disabled or have end - stage renal disease . this study was approved by the institutional review board of the university of pennsylvania . study population we developed an analytic dataset from the seermedicare linked database , consisting of patients with a diagnosis of lung cancer ( icd - 9 code 162xx ) and nonsmall - cell histology ( adenocarcinoma , squamous cell carcinoma , large cell , bronchoalveolar carcinoma , or nsclc not otherwise speci ed ) contained in the seer registry who were diagnosed between jan 1 , 2000 , and dec 31 , 2005 . 
patients who were enrolled in medicare , but receive their bene ts through a third party , such as a health maintenance organisation , or private fee - forservice plan , were excluded from this analysis because of incomplete claims data in medicare for these patients . 
survival comparisons were also done after strati cation for disease stage . we used propensity score methods to account for imbalances between the two comparison groups on measured covariates.27 , 28 we chose propensity score adjustment in our cox model rather than traditional covariate adjustment , since recent ndings have suggested that this method is advantageous when analysing large observational datasets such as seer - medicare.29 our group has previously used this method to examine seer - medicare data.30 , 31 in an observational study such 1204 vol 13 december 2012 articles log - rank p = 037 hiv - infected control 95% ci for hiv patients 95% ci for controls log - rank p = 016 number at risk hiv - infected control 71 976 20 999 9615 4132 1225 20 016 13 006 6950 3205 log - rank p = 0051 log - rank p = 077 number at risk hiv - infected control 22 793 5313 time ( months ) 2007 29 167 2671 time ( months ) figure 1 : kaplan - meier comparative survival of hiv - infected and uninfected control nsclc patients : ( a ) all stages ; ( b ) stage i / ii ; ( c ) stage iiia / iiib ; and ( d ) stage iv as this one , covariate imbalances could potentially lead to biased survival estimates due to confounding . 
we calculated propensity scores using multivariable logistic regression with hiv infection as the outcome of interest , with adjustment for race , median income , stage , sex , and comorbidities . 
we then used multivariable cox proportional hazards models to compare death from any cause between the hiv - infected and control groups after adjustment for the propensity score as a continuous variable . 
to assess the proportional hazards assumption , we used the schoenfeld residuals test and complementary log - log plots . the kaplan - meier method was used to compare patients with stage i and ii disease with or without hiv infection who underwent de nitive surgical resection to assess the e ect of hiv infection in patients undergoing de nitive surgical resection for treatment of early stage nsclc . 
all statistical analyses were done with the statistical analysis system ( sas ) version 9.3. role of the funding source the sponsor did not have any role in study design , collection , analysis , or interpretation of the data , or in writing of this report . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results 322 patients were identi ed from jan 1 , 2000 , to dec 31 , 2005 , with a diagnosis of hiv ( hiv group ) and 71 976 individuals with a diagnosis of nsclc were identi ed who were not associated with a diagnosis of hiv ( control group )  . 
a similar proportion of patients were stage iiia / iiib and stage iv in both groups , but there was a signi cantly greater proportion of patients with stage i / ii disease in the hiv - infected group than the control group ( p = 0002 , table )  . 
there was a signi cant di erence in ethnic background between the two groups , with the hiv - infected group containing a higher proportion of african americans ( 236% vs 84% , p < 00001 )  . 
 the proportion of patients with their median income in vol 13 december 2012 1205 articles the bottom two quartiles was much the same between the two groups ( table )  . 
 the unadjusted median survival for uninfected control patients with nsclc was 70 months ( 95% ci 7070 ) com pared with 80 months ( 60100 ) for the hiv group ( p = 016 )  . 
when strati ed by stage , the unadjusted median survival for stage i / ii patients was 370 months ( 95% ci 360390 ) for uninfected controls compared with 430 months ( 260580 ) for the hiv group ( p = 037 ) , for those with stage iiia / iiib disease , it was 70 months ( 7070 ) for uninfected controls compared with 30 months ( 2080 ) for the hiv group ( p = 0051 ) , and for those with stage iv disease , it was 30 months ( 3030 for control group and 2050 for hiv group ) for un infected controls and the hiv group ( p = 077 ; gure 1 )  . 
after using propensity score adjustment to account for potential confounders , there remained no di erence in survival between uninfected controls and the hiv group across all stages ( hazard ratio 103 , 95% ci 091117 ) , stage i / ii ( 122 , 09316 ) , stage iiia / iiib ( 088 , 071109 ) , and stage iv ( 099 , 082121 )  . to examine the e ect of treatment on survival , we restricted our analysis to stage i and ii patients undergoing de nitive surgical resection alone , which is the standard of care.32 of the 114 hiv - infected patients with stage i or ii disease , 92 ( 807% ) underwent surgical resection . 
 the 5 - year survival was 47% for hiv - infected patients undergoing surgical resection versus 49% for the control group ( p = 088 )  . hiv - infected control 95% ci for hiv patients 95% ci for controls log - rank p = 088 discussion our results indicate that , across all stages , survival outcomes in hiv - infected patients with nsclc are not signi cantly di erent from uninfected patients . 
additionally , when assessing stage i / ii patients undergoing de nitive sur gical resection , survival was not signi cantly di erent in hivinfected patients undergoing surgery com pared with uninfected patients . 
taken together , these data suggest that nsclc does not display a more aggressive phenotype in hiv - infected patients . our ndings are in contrast to previously published reports that suggest that hiv - infected patients with lung cancer fare worse when compared with uninfected patients ( panel ) .17 , 18 notably , these previous studies included patients from the pre - haart era and spanned over three decades to identify adequate patient numbers . 
 these studies did not distinguish between nsclc and sclc , which have signi cantly di erent treatments and expected survival and as such cannot be grouped together for the purpose of examination of clinical outcome.1 , 2 , 33 a retrospective study by brock and colleagues18 examined the e ect of hiv infection across di erent stage subgroups in a combined cohort of sclc and nsclc and pre - haart and post - haart patients . 
although the authors did not note any signi cant di erence in stage - speci c survival , the overall survival of hivinfected patients with lung cancer was worse than hivindeterminate patients . 
their results may be due , in part , to the increased proportion of advanced stage patients ( iii and iv ) seen in the hiv - infected group relative to the hiv - indeterminate patients.18 in a report from the italian cooperative group on aids and tumors , spina and colleagues reported signi cantly poorer survival in 39 patients with hiv and lung cancer treated in the prehaart era ( 198697 ) than in matched controls ( median survival of 50 vs 100 months ; p < 00001 ) .34 , 35 a follow - up study36 com pared survival in hiv - infected patients with lung cancer from the pre - haart era to the haart era , demonstrating a signi cant improvement in survival ( from 38 to 70 months ; p = 001 )  . 
 although the exact reason for our observation is unclear , hiv - infected patients might have received regular medical care while on haart and therefore were diagnosed at an earlier stage . since the introduction of haart in 1996 , mortality from hiv / aids has decreased substantially . 
they further reported that this translated into an improvement in median survival of an hiv - infected patient in the haart era to 325 years from 76 years in the prehaart era.21 by contrast , the median survival of a patient with lung cancer across all stages is around 15 months.1 an analysis by persad and colleagues showed that 25% of all clinical trials for patients with nsclc and 29% of clinical trials for patients with sclc explicitly excluded patients with hiv.9 given the signi cant improvement in survival with hiv in the haart era , persad and coworkers argued for greater inclusion of patients with hiv in clinical trials across all cancers . there are several limitations to our analysis . 
although this study represents the largest study , to our knowledge , to date on the e ect of hiv on clinical outcome in nsclc , the number of hiv - infected patients identi ed is fairly small , leading to limited power to detect a small survival di erence . 
although there are data for the incidence of nsclc in patients with hiv , 16 there are limited data for the incidence of hiv in patients with nsclc , with reports ranging from 50 to 1800 hivinfected individuals per 100 000 patients with lung cancer.17 , 18 our data is concordant with these reports . 
although we restricted our analysis to patients treated between jan 1 , 2000 , and dec 31 , 2005 , when most hiv patients should have been receiving haart , we could not con rm that the patients included in our analysis were being treated with haart . 
a recent report assessing us trends in haart use showed widespread adoption of treatment during this period , with around 80% of hiv - infected therapy.40 seer - medicare patients on antiretroviral seer - medicare does not panel : research in context systematic review at the time that this study was designed , an increased incidence of nsclc in hiv - infected patients had been reported . 
before initiating our study , we searched the medical literature for comparative studies examining clinical outcome in hiv - infected lung cancer or hiv - infected patients with nsclc when compared with hiv - uninfected or indeterminate patients with lung cancer . 
we searched pubmed ( without any date or language restrictions ) using the following terms : hiv and survival and lung cancer , or hiv and survival and non - small cell lung cancer or hiv and lung cancer or hiv and non - small cell lung cancer and repeated these searches including the term antiretroviral therapy , highly active . 
we identi ed studies that had retrospectively examined the outcome of hiv - infected patients with lung cancer and reported this group to have poorer survival when compared to uninfected or hiv - indeterminate patients with lung cancer or historical benchmarks for survival . interpretation our data suggest that survival of hiv - infected patients with nsclc in the era of haart is comparable to hiv - uninfected patients with nsclc . 
haart regimens have previously been shown to interfere with the antineoplastic regimens that are routinely used in the treatment of lung cancer.23 the extent to which this interaction a ected the results seen in our study is unclear . 
the potential for drugdrug interactions must be taken into account when administering antineoplastic agents in patients with hiv / aids on haart.41 also , seer - medicare does not capture cd4 count data , a factor which has previously reported to correlate with survival in hiv - infected patients with lung cancer.19 seer - medicare does not capture in formation on the incidence of opportunistic infections or the administration of prophylactic regimens and therefore this is not included in this analysis . 
competing risks of death in hiv - infected patients with nsclc from opportunistic infec tions or complications from antineoplastic therapy , such as neutropenia , could not be quanti ed in our analysis . 
however , on the basis of our results , such an unmeasured confounder would have two to be signi cantly imbalanced between the vol 13 december 2012 1207 articles the hiv group comparison groups for to show signi cantly poorer survival than the uninfected controls.42 additionally , because the data in seer - medicare is mainly composed of people older than 65 years , we were unable to examine the e ect of hiv infection on survival in younger patients.1 notably , the median age of patients with hiv and lung cancer is generally reported to be younger than the average age of the lung cancer population.34 , 39 , 43 the clinical phenotype of lung cancer in younger patients with hiv could be distinct from that seen in patients over age 65 years . 
age has been shown to be an important prognostic factor for survival in lung can cer , with older patients faring more poorly.44 advanced age has also been shown to be an independent predictor of poor survival in hiv - infected patients initiating haart.45 however , since seer - medicare does not capture data for patients under the age of 65 years , whether the results reported in our trial are applicable to all hiv - infected patients with lung cancer is unclear . trials , where in conclusion , these data suggest that hiv infection alone in the era of haart should not play a role in clinical decision making in treatment of patients with nsclc . 
notably , the intergroupe francophone de cancerologie thoracique has recently initiated a phase 2 , multicentre prospective study evaluating the combination of pemetrexed plus carboplatin in hivpositive patients with lung cancer and accrual to this ( clinicaltrials.gov , number nct01296113 )  . 
additionally , these data suggest that improving access to modern diagnostic imaging and cancer therapies are likely to signi cantly bene t patients with nsclc with hiv since their outcome is similar to that of uninfected controls when treated with de nitive surgical resection . 
the clinical management of the hiv - infected patient with nsclc , as with all patients with lung cancer , requires a multidisciplinary approach to individualise and optimise therapy and to manage toxicities . is ongoing trial contributors rr , nm , kl , and av were responsible for the study concept and design . 
 correction to lancet oncol 2016 ; 17 : 74756 correction to lancet oncol 2018 ; 19 : 153042 correction to lancet oncol 2019 ; 20 : 81626 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
lancet oncol 2016 ; 17 : 74756in results , median overall survival should have been median time of death ( after randomisation ) in eleven patients who died from progressive disease . 
prognostic value of end - of - induction pet response after first - line immunochemotherapy for ( gallium ) : follicular secondary analysis of a randomised , phase 3 trial . 
 lancet oncol 2019 ; 20 : 81626 the appendix of this article has been updated as of may 10 , 2019 . published online april 29 , 2019 s1470 - 2045 ( 19 ) 30280 - 3 published online may 10 , 2019 s1470 - 2045 ( 19 ) 30292 - x published online may 10 , 2019 s1470 - 2045 ( 19 ) 30293 - 1 correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
this correction has been made to the online version as of may 29 , 2019 . correction to lancet oncol 2019 ; 20 : 82736 shitara k , iwata h , takahashi s , et al . 
lancet oncol 2019 ; 20 : 82736the appendix of this article has been updated as of may 10 , 2019 . correction to lancet oncol 2019 ; 20 : 84961 eng c , kim tw , bendell j , et al . 
 atezolizumab with or without cobimetinib versus regorafenib previously treated metastatic colorectal cancer ( imblaze370 ) : a multicentre , open - label , phase 3 , randomised , controlled trial . 
this correction has been made to the online version as of may 29 , 2019 and the printed article is correct . correction to lancet oncol 2019 ; 20 : e26273 ngiam ky , khor iw . 
lancet oncol 2019 ; 20 : e26273tables 1 and 2 in this article have been corrected as of april 29 , 2019 . correction to lancet oncol 2019 ; 20 : 297310 cella d , grnwald v , escudier b , et al . 
this update has been made online as of may 29 , 2019 . vol 20 june 2019 e293 corrections corrections correction to lancet oncol 2016 ; 17 : 109 correction to lancet oncol 2016 ; 17 : 248 , 252 du y sw , dibden a , michalopoulos d , et al . 
lancet oncol 2016 ; 17 : 10914in the findings section of the summary of this article , the second sentence should read the average frequency of dcis detected at screening was 160 per 1000 women screened ( median 150 [ unit range 054356 ] per 1000 women )  . 
 addition of docetaxel or bisphosphonates to standard of care in men with localised or metastatic , hormone - sensitive prostate cancer : a systematic review and meta - analyses of aggregate data . 
 lancet oncol 2016 ; 17 : 24356in the results section , the third sentence of the second paragraph should read in the three remaining trials , 7 , 8 , 10 men aged 3691 years ( median 6366 years ) with a good performance status received androgen deprivation therapy - based treatments ( standard of care ) with or without docetaxel . 
 in figure 3 , the text under parts a and c should have read favours soc + bisphosphonate , and the text under parts b and d should have read favours soc + zoledronic acid . 
open access article distributed under the terms of cc - by . vol 17 february 2016 errata see articles page 528 errata miller va , hirsh v , cadranel j , et al . 
afatinib versus placebo for patients with advanced , metastatic non - small - cell lung cancer after failure of erlotinib , ge tinib , or both , and one or two lines of chemotherapy ( lux - lung 1 ) : a phase 2b / 3 randomised trial . 
lancet oncol 2012 ; 13 : 52838in this article ( published online march 26 ) , the rst sentence of the fourth paragraph on the fourth page should have read we measured progression - free survival from the date of randomisation to disease progression or death , whichever occurred rst . 
this correction has been made to the online version as of april 24 , 2012 . see news page e194 vol 13 may 2012 e186 corrections published online november 22 , 2013 s1470 - 2045 ( 13 ) 70328 - 0 correction to lancet oncol 2013 ; 14 : 1279 , 1283 , 1285 correction to lancet oncol 2013 ; 14 : 1330 , 1333 , 1335 yamada y , takahari d , matsumoto h , et al . 
 leucovorin , fluorouracil , and oxaliplatin plus bevacizumab versus s - 1 and oxaliplatin plus bevacizumab in patients with metastatic colorectal cancer ( soft ) : an open - label , non - inferiority , randomised phase 3 trial . 
this has been corrected online as of dec 30 , 2013 . correction to lancet oncol 2013 ; 14 : 1295306 zhang j - x , song w , chen z - h , et al . 
 docetaxel or pemetrexed with or without cetuximab in recurrent or progressive non - small - cell lung cancer after platinum - based therapy : a phase 3 , open - label , randomised trial . 
 lancet oncol 2013 ; 14 : 132636in the online first version of this article ( published online nov 12 ) , in table 3 , all entries of ( > 1% ) should have read ( < 1% ) , and the rst two sentences of the third paragraph on page 1335 should state : a subsequent analysis of flex showed a signi cant association between egfr expression by immunohistochemistry and improved outcomes , with high egfr expression ( h - score 200 or higher ) being associated with improved overall survival , time - to - treatment failure , and a greater proportion of patients achieving objective responses when treated with cetuximab than when treated with cisplatin plus vinorelbine alone.13 there was no improvement in outcomes in the low h - score group ( h - score lower than 200 ) .13 these corrections were made to the print version of the article in the december issue of the journal , and have been made online as of nov 22 , 2013 . 
in table 1 , the entry for adenocarcinoma in the cetuximab and pemetrexed group should have read 161 ( 53% ) and the entry for all other diagnoses in the pemetrexed group should have read 41 ( 13% )  . 
in table 3 , in the cetuximab plus pemetrexed group , the entry for patients with one or more ctcae grades 12 should have read 89 ( 30% ) , that for grade 3 anaemia 16 ( 5% ) , for grade 4 infusion related reactions 5 ( 2% ) , and grade 3 lung infection 16 ( 5% )  . 
 in the pemetrexed group in the same table , the entry for patients with one or more grade 4 ctcae should have read 36 ( 12% ) and one or more grade 5 ctcae 10 ( 3% ) ; the entry for grade 12 diarrhoea should have read 36 ( 12% ) , that for grade 12 hyperglycaemia 10 ( 3% ) , and grade 12 maculopapular rash 39 ( 13% )  . 
lancet oncol 2015 ; 16 : e434in this news item , the fourth sentence of the third paragraph should read patients with ccnd1 mutations had worse 2 - year overall survival than those without ( 381% [ 95% ci 14100 ] vs 80% [ 7684 ] ; p = 0005 ) ; similar outcomes were noted with alterations in the dna repair pathways ( tp53 , atm , atr , and znfhx4 mutations )  . 
triage by methylation - marker testing versus cytology in women who test hpvpositive on self - collected cervicovaginal specimens ( prohtect - 3 ) : a randomised controlled non - inferiority trial . 
lancet oncol 2015 ; 16 : 133543in this article , the title of figure 2 should have been kaplan - meier analysis of cumulative incidence of leukaemia for children with or without enterovirus infection after accounting for death as the competing risk . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . correction to lancet oncol 2015 ; 16 : 1289 lokody , i . 
lancet oncol 2015 ; 16 : 1289in this news feature , the fourth sentence in the fourth paragraph on liver transplants for patients with high risk hcc has been changed to read : of these , 17 had a liver transplant . 
the 5 - year survival of these patients was superior to those high risk patients that did not have a liver transplant ( 82% vs 38% ; p = 0033 )  . 
this correction has been made to the online version as of oct 1 , 2015 and the printed version is correct . vol 16 october 2015 e480 correction to lancet oncol 2016 ; 17 : 16473 correction to lancet oncol 2018 ; 19 : 1289306 correction to lancet oncol 2018 ; 19 : 150415 published online october 3 , 2018 s1470 - 2045 ( 18 ) 30748 - 4 india state - level disease burden initiative cancer collaborators . 
the correction has been made to the online version as of oct 3 , 2018 . correction to lancet oncol 2018 ; 19 : 146879 barlesi f , vansteenkiste j , spigel d , et al . 
 avelumab versus docetaxel in patients with platinum - treated advanced non - small - cell lung cancer ( javelin lung 200 ) : an open - label , randomised , phase 3 study . 
lancet oncol 2018 ; 19 : 146879in this article ( published online first on sept 24 ) , the following sentence in the discussion ( page 1476 ) should have read as follows : our trial included a high proportion of asian patients in the pd - l1 - positive population ( 71 [ 27% ] in the avelumab group vs 81 [ 31% ] in the docetaxel group ) this correction has been made to the online version as of oct 31 , 2018 , and the printed article is correct . walker i , panzarella t , couban s , et al . 
 pretreatment with anti - thymocyte globulin versus no anti - thymocyte globulin in patients with haematological malignancies undergoing haemopoietic cell transplantation from unrelated donors : a randomised , controlled , open - label , phase 3 , multicentre trial . 
 lancet oncol 2016 ; 17 : 16473in this article , the data for atkinson life happiness rating in table 2 should read : adjusted mean ( se ) 790 ( 026 ) , n = 47 for the no atg group , adjusted mean ( se ) 791 ( 023 ) , n = 62 for the atg group , and p = 0967 . 
the first sentence of seventh paragraph of the results should read at 12 months , differences between the treatment groups were significant only for cgvhd symptoms ( lee scale ; table 2 , appendix )  . 
this correction has been made to the online version as of oct 31 , 2018 . correction to lancet oncol 2018 ; 19 : 1192204 kim yh , bagot m , pinter - brown l , et al . 
lancet oncol 2018 ; 19 : 1192204in this article , in the outcomes section of the methods , exploratory endpoints were overall survival and exposureresponse relationship of mogamulizumab ( to be reported separately ) , mogamulizumab was incorrectly . 
this has been spelt corrected in the online version as of oct 31 , 2018 . sentence the size field radiotherapy roach m , moughan j , lawton caf , et al . 
lancet oncol 2018 ; 19 : 150415in the summary of this article ( published online first on oct 10 , 2018 ) , the last sentence of the background section should read we provide a long - term update after 10 years of follow - up of the primary endpoint ( progression - free survival ) and report on the late toxicities of treatment . 
this correction has been made to the online version as of oct 31 , 2018 , and will be made to the printed article . correction to lancet oncol 2018 ; 19 : 148092 hodi fs , chiarion - sileni v , gonzalez r , et al . 
nivolumab plus ipilimumab or nivolumab alone versus ipilimumab alone in advanced melanoma ( checkmate 067 ) : 4 - year outcomes of a multicentre , randomised , phase 3 trial . 
 lancet oncol 2018 ; 19 : 148092 in this article ( published online first on oct 22 , 2018 ) , in figure 3b , the median ( iqr ) follow - ups listed for the post - hoc analysis of post - treatment outcomes in each group were incorrect . 
these should have been as follows : in the nivolumab plus ipilimumab group , median follow - up 516 months ( iqr 504528 ) ; in the nivolumab group , median follow - up 517 months ( iqr 504529 ) ; and in the ipilimumab group , median follow - up 514 months ( iqr 504527 )  . 
these corrections have been made to the online version as of oct 31 , 2018 , and the printed article is correct . vol 19 november 2018 e581 corrections re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology euthanasia ( destroyed brain activity after application ) and palliative sedation ( continued brain activity after application )  . 
however , palliative is only acceptable for the combination of both intolerable and refractory ( untreatable ) symptoms.2 although it is understandable that patients struggle with existential questions in the face of death , it is problematic to consider this struggle as a refractory symptom for palliative sedation , as the authors correctly note . 
 such an application of palliative sedation occurs only in exceptional circumstances ( it is mostly applied for severe delirium and dyspnoea ) and , therefore , should not be the example by which the entire practice is considered controversial.3 we have proposed that palliative sedation is morally acceptable only when excruciating and untreatable symptoms severely threaten a patients ability to be the further agent of his or her life.4 this precondition acknowledges that it should be the progressive disease , not the palliative sedation , which inhibits the patients ability to shape their own life . 
therefore , total sedation will be at one end of the spectrum of palliative sedation , and used in a restricted group of patients , with intermittent and super cial sedation at the other end . 
in this perspective , palliative sedation is not controversial but a well de ned medical last resort for intractable ( and irresolvable ) multidimensional needs and problems in human beings who are su ering . 
clinical guidelines and an obligatory expert consultation in palliative care will educate and strengthen a reliable practice.5 jeroen hasselaar * , stans verhagen , rob reuzel , evert van leeuwen , kris vissers department of anesthesia , pain and palliative medicine ( jh , sv , kv ) , department of epidemiology , bio - statistics , and health technology assessment ( rr ) , and section ethics , philosophy , and history of medicine , department of iq health care ( evl ) radboud university medical center , nijmegen , the netherlands j.hasselaar@anes.umcn.nl the authors declared no con icts of interest . 1 materstvedt lj , bosshard g . 
in this article , the number 169 in the mild dyskaryosis box on the right - hand side of gure 3 should have been given as 196 . 748 vol 10 august 2009 for more on euromonitors data on vaping see euromonitor.com / growthvapour - products for more on pulmonary illness and e - cigarette use in illinois and wisconsin see nejm.org / doi / full / 10.1056 / nejmoa1911614 for more on the cdc warning about lung illness and e - cigarette products see basic_information / e - cigarettes / severe - lung - disease.html for the lancet oncologys 2018 editorial on vaping see editorial lancet oncology 2018 ; 19 : 1543 for the fda letter to juul labs see inspections - complianceenforcement - and - criminalinvestigations / warning - letters / juul - labs - inc - 590950 - 09092019 vaping - related lung illnesses : time to act by 2021 , euromonitor , a strategic market research provider , estimates that 55 million people worldwide will regularly vape , with the usa being the largest consumer . 
however , a study by jennifer layden and colleagues published in the new england journal of medicine on sept 6 , 2019 , challenges the biggest of these misconceptions by providing more evidence linking pulmonary illness to e - cigarette use adding to the number of reported cases , which now stands at more than 200 in 25 us states since june , 2019 . this new study reports on 53 patients identified as part of a pulmonary disease cluster in the states of wisconsin and illinois . 
the most common respiratory symptoms at presentation were shortness of breath , cough , and chest pain along with gastrointestinal including nausea , vomiting , diarrhoea , symptoms and abdominal pa 48 patients had an abnormal chest radiograph showing complications such as pneumo mediastinum , pleural effusion , or pneumothorax . 
given the plausibility of the connection between these symptoms , the increasing number of cases nationwide , and the patients vaping behaviours , the us centers for disease control and prevention have warned that there might be a link to street - bought , illegal products , and advised that people should only buy vaping paraphernalia from official outlets and seek immediate medical attention if they have any health concerns . 
reflecting on the evidence so far , although a definitive cause - and - effect association has yet to be proven , the rising frequency of lung disease in e - cigarette lung cancer users must now trigger a far higher concern level for policy makersparticularly because the connection between many of these lung conditions and future development in a 2018 lancet oncology editorial , we called for a new , broader set of measures in the who framework convention on tobacco control . 
 a broader remit for the who framework convention on tobacco control would ensure that measures are in place internationally to prevent the us findings from becoming a global epidemic and enable more restrictive regulation around marketing of vaping products to prevent deceitful or misleading practices by vape manufacturers . 
for example , in a letter on sept 9 , 2019 , the us food and drug administration wrote to juul labs ( san francisco , ca , usa ) criticising them for illegally marketing their e - cigarettes as less harmful than regular cigarettes and instructing the company to make immediate corrections or face enforcement actions . 
this letter followed previous testimony to a house oversight and reform subcommittee into juuls marketing and promotion practices , which accused juul of using a sophisticated program to target children and teenagers , including at schools and summer camps . 
ironically , the usa remains one of the few nations worldwide that has yet to ratify the who framework convention on tobacco control , so even with an extended remit , the framework convention could not be used to help bolster efforts by us authorities and health practitioners . in 1610 , sir francis bacon noted that tobacco smoking seemed to be highly addictive and was a tough habit to quit . 
with vaping increasing at an unprecedented rate , we need to act swiftly to ensure we do not blunder in to another longrunning unhealthy , life shortening , odyssey of replacing one bad habit with another . 
 the lancet oncology vol 20 october 2019 1327 editorial re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology department of radiation oncology , all india institute of medical sciences , new delhi , india sharmadn@hotmail.com the authors declared no con icts of interest . powell jw , dexter e , scalzetti em , bogart ja . 
long term results of endobronchial brachytherapy : a curative treatment ? int j radiat oncol biol phys 2007 ; 67 : 42530 . brach b , buhler c , hayman mh , joyner lr jr , liprie sf . 
 chest 2005 ; 127 : 223742 . screening newborns for tp53 in the september issue of the lancet oncology , achatz and colleagues1 discuss the possibility of screening newborns in southeast brazil for a highly prevalent tp53 mutation ( 1 : 300 individuals ) that predisposes to many cancers . 
the authors present the justi cations and the problems associated with such a screening e ort , and conclude that on the basis of current scienti c and medical knowledge the r337h mutation does not meet all the criteria for mass newborn screening . 
 in my opinion , this type of screening will never meet the criteria for newborn screening , which is intended to detect conditions for which the population is at risk but there is no other way to assess risk in newborns . 
newborn screening is done for sporadic diseases such as congenital hypothyroidism and autosomal recessive disorders , in which carrier detection is di cult or impossible , but never applies for a disorder caused by the presence of a founder dominant mutation . 
a founder mutation in a newborn will be carried by one of the parents , so the detection of the child can be done by knowing who the adult carrier is . 
cascade screening is the most economically e ective , o ering the screening test to rst - degree relatives of carriers of the mutation , and several countries have chosen this approach.2 the problem with this type of screening is that it involves the cooperation of relatives who are not always willing , and so an alternative has been the creation of databases to store information on patients.3 in my view , population screening of informed and consenting adults is much better suited for the tp53 mutation . 
 this approach identi es families at risk and has been implemented in pilot studies for haemochromatosis.4 as emphasised by achatz and colleagues , 1 such population screeningin the context of appropriate genetic counsellingallows at - risk families the informed decision of whether or not to test the probands o spring . joel zlotogora department of community genetics , ministry of health , jerusalem , israel joelz@cc.huji.ac.il the author declared no con icts of interest . achatz miw , hainaut p , ashton - prolla p . 
 clin genet 2004 ; 66 : 48387 . had eld sg , horara s , starr bj , et al ; steering group for the department of health familial hypercholesterolaemia cascade testing audit project . 
lancet oncol 2009 ; 10 : 940in this news report , the nal sentence of the 90y radioembolisation paragraph should have read only one patient experienced radiation - induced pneumonitis ; three had gastrointestinal ulcers that did not require surgical treatment , and radioembolisation - induced liver disease was noted in 24 patients ( fatal for four )  . huober j , thrlimann b . 
lancet oncol 2009 ; 10 : 102829in this re ection and reaction , the a liation for both authors should read breast center , kantonsspital st gallen , 9007 st gallen , switzerland . 
the authors would also like to thank karen price for her useful comments on the article . 1142 vol 10 december 2009 editorial to read more about the lancet oncologys cancer campaign and the four commissions go to campaigns / cancer / for our previous editorial on direct - to - consumer marketing see lancet oncol 2008 ; 9 : 1113 tackling the cancer epidemic rising cancer is the primary cause of death in many countries , now exceeding heart disease . 
in lower income countries , fast , creating unprecedented incidence challenges for health systems , many of which were designed in an era that did not foresee , were simply incap able of pre - empting , or knowingly ignored the future . 
 however , these remarkable achievements come at a pricethe cost of care is outpacing national budgets , the numbers of cancer patients and survivors are putting greater pressures on health - care systems , and increasing numbers of vulnerable patients from less traditional demographics , such as children and younger adults , require di erent clinical solutions that have yet to be fully conceived . this month , the lancet oncology launches a campaign focused on tackling the cancer epidemic at a systems level . 
we will document , via monthly updates , the evolution of four commissions intended for publication later this year that aim to de ne the scale of the challenge , the underlying drivers , and the improvements needed to cancer - care systems . 
these special reports will cover global access to radiotherapy , surgical resource availability and its fundamental role in cancer treatment , the intersection of primary care in a comprehensive cancer service t for the 21st century , and the ongoing oncology requirements in the low - to - middle income countries of latin america . 
 the lancet oncology dangers of direct - to - consumer advertising exposed again direct - to - consumer ( dtc ) advertising is in the headlines agaon feb 19 , 2015 , 23andme was granted approval by the us food and drug administration ( fda ) to market a genetic test for bloom syndrome . 
and on feb 25 , 2015 , the us federal trade commission ( ftc ) ned two companies for marketing melanoma detection apps ( melapp and mole detective ) and banned them from making misleading or unsubstantiated health claims in the future . 
 the decision to permit 23andme limited access to the dtc market is a remarkable turnaround for a company that on nov 22 , 2013 , received an fda warning letter instructing them to stop all marketing . 
at that time , the fda insisted the company seek approval for each speci c indi cation in their pan - genomic test along with robust evidence for each claimin line with the requirements for other over - the - counter home - use tests . 
despite the seeming appro priate ness of the decision , it creates an uneasy precedentone that could open the door to other less reliable tests if the delineations of the ruling are not rmly upheld . 
these concerns are further underscored by the jnci article showing that websites promoting person alised cancer medicine products contain more information about the bene ts than the limitations , and most focus on one or more non - standard tests . ensuring people take an active interest in their health is central to a strong health - care system , but health - care decisions need to be a bilateral process between patients and their doctors . 
in our december , 2008 , editorial , we con cluded that the marketing of tests should be restricted to health professionals , rather than the lay public , and only accessed through health - care providers on the basis of their advice . 
 the lancet oncology vol 16 april 2015 correction to lancet oncol 2019 ; 20 : 155665 correction to lancet oncol 2019 ; 20 : e658 correction to lancet oncol 2020 ; 21 : e31729 bertelsen ca , neuenschwander au , jansen je , et al . 
lancet oncol 2019 ; 20 : 155665in this article , two patients ( one in the control group and one in the complete mesocolic excision group ) were incorrectly classified as not having recurrences , due to an error in data extraction . 
 the incorrect data have been updated in the summary findings , the results , figures 2a and 2c , table 3 , supplementary figures 2c and 2f in the appendix , and the discussion . 
complete mesocolic excision for colon cancer : is now the time for a change in practice ? lancet oncol 2019 ; 20 : 147476in this comment , the cumulative incidence of recurrence in each group has been amended , owing to these data being corrected in the linked article by bertelsen and colleagues . 
lancet oncol 2019 ; 20 : e658 in this correspondence , the absolute in risk of recurrence reduction has been amended , owing to this being corrected in the linked article by bertelsen and colleagues . 
this correction has been made to the online version as of aug 3 , 2020 . correction to lancet oncol 2020 ; 21 : e33036 cooney tm , cohen jk , guimaraes cv , et al . 
these corrections have been made to the online version as of aug 3 , 2020 . vol 21 august 2020 e372 corrections published online july 22 , 2019 s1470 - 2045 ( 19 ) 30416 - 4 see articles page 1273 garbay da , le cesne n , penel c , et al . 
j clin oncol 2009 ; 27 : 595864 . management of high - risk endometrial cancer : are we there yet ? endometrial cancer is a diverse disease that includes varying stages and histologies . 
as a result , the design , completion , and interpretation of large randomised trials comparing adjuvant therapies for this disease , even when well conducted and well analysed , is problematic . 
 this situation is especially true in the study of adjuvant therapy for advanced endometrial cancer , since many patients are diagnosed and treated surgically for early disease , with no indication for adjuvant treatment . the portec study group is to be commended for its work in refining the use of adjuvant therapy across various types of non - metastatic endometrial cancer . 
in the portec - 3 study , eligible patients included those with stages ii and iii and high - risk stage i endometrioid iiii serous and endometrial cancer and stages clear cell histologies.1 with more than 650 women enrolled , the combination of systemic chemotherapy and radiotherapy was shown to improve outcomes compared with radiotherapy alone . 
for example , 5 - year overall survival was 814% ( 95% ci 772858 ) with chemoradiotherapy versus 761% ( 716809 ) with radiotherapy alone ( adjusted hazard ratio [ hr ] 070 [ 95% ci 051097 ] , p = 0034 ) , and 5 - year failure - free survival was 765% ( 95% ci 715807 ) versus 691% ( 638738 ; hr 070 [ 052094 ] , p = 0016 )  . 
in the aftermath of these potentially practice - changing results , additional questions are raised . first , do these findings apply broadly to all subgroups included in the study ? in addition to the broad eligibility criteria of portec - 3 ( ie , different tumour stages and histologies ) , many clinicopathological variables have prognostic significance , such as tumour grade , depth of myometrial invasion , patient age , lymphovascular space invasion ( in the absence of positive lymph nodes ) , and the patients general condition . 
even within similar or identical subgroups , substantial differences exist among patients , such as extent of nodal dissection , which are potentially confounding variables . whether or not the results from portec - 3 are generally applicable across patient subgroups remains unknown . 
however , taking into account the statistical limitations of subgroup analyses , the therapeutic benefit of combined chemotherapy and radiotherapy ( vs radiotherapy alone ) appeared to remain confined to patients with stage iii disease and those with serous carcinomas of all stages . second , is chemotherapy alone a sufficient form of adjuvant therapy ? the gynecologic oncology group ( now nrg oncology ) did separate studies that overlap ( in terms of patient eligibility ) with portec 3 . 
in the nrg / gog 249 study , investigators randomly assigned high - risk patients with stage i and ii disease , including those with high - risk histologies , to chemotherapy plus vaginal cuff brachytherapy or pelvic radiotherapy with no chemotherapy . 
in the nrg / gog 249 study , the chemotherapy plus vaginal cuff brachytherapy group did not show improved overall survival or relapse - free survival compared with the group that received pelvic radiotherapy alone . 
however , the incidence of nodal failure was significantly higher in the absence of pelvic radiation therapy , and acute toxicity was greater in the vaginal cuff brachytherapy group.2 in the nrg / gog 258 trial , patients with stage iiiiva uterine cancer were randomly assigned to received adjuvant chemotherapy alone or combined chemotherapy with pelvic radiotherapy ( and para - aortic radiotherapy if nodal metastases were present )  . 
although recurrencefree survival and overall survival were not improved with the combined therapy , nodal and vaginal failures were significantly lower when radiotherapy was given.3 1192 vol 20 september 201 comment in these and other previous studies of adjuvant therapy within the portec - 3 eligibility groups , locoregional failure has been a notable and often predominant failure pattern in the absence of pelvic radiotherapy . the apparent complementarity of chemotherapy ( in limiting distant failure ) and radiotherapy ( in limiting local failure ) , is a consistent finding that is a reasonable basis for subsequent clinical investigation . 
several studies support the use of combined modality therapy rather than monotherapy.4 , 5 finally , is there a preferred way of combining chemotherapy with radiotherapy ? in both portec - 3 and nrg / gog 258 , the combined chemotherapy plus radiotherapy schedule was based on a phase 2 regimen piloted by the radiation therapy oncology group , rtog 9708.6 when nrg / gog 258 was designed , there was vigorous debate about the combined modality group , with various investigators favoring a sandwich regimen typically involving three cycles of chemotherapy , followed by involved - field radiotherapy , and then additional chemotherapy . 
however , multiple studies ( retrospective and prospective ) have demonstrated the safety and efficacy of the so - called sandwich approach.5 , 79 increasing evidence supports the use of upfront systemic therapy , when combined with radiotherapy , as a strategy to maximise both systemic and local control.10 many clinicians often use this regimen as a preferred adjuvant approach in locally advanced endometrial cancer . based on outstanding work done by the portec study group and others , we have made good progress in improving outcomes for women with high - risk and locally advanced endometrial cancers . 
however , we are not there yet . marcus randall department of radiation medicine , university of kentucky , lexington , ky 40536 , usa merand2@uky.edu i have received an honorarium from isoray medical within the past 2 years . copyright 2019 the author ( s )  . 
adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
gynecol oncol 2019 ; 153 : 4148 . the emerging role of pet - ct scan after radical prostatectomy : still a long way to go the management of biochemical recurrence after radical prostatectomy is a common challenge for urologists and radiation oncologists , because about 30% of patients have an increase in prostate - specific antigen ( psa ) concentrations after surgical treatment.1 however , the outcome of these patients is not always poor , varying substantially according to the site and the extent of recurrence.2 in this context , the role of imaging is of the utmost importance to establish the real burden of recurrent disease . 
the increasing use of pet - ct has led to a shift towards early detection of low - volume metastatic prostate cancer , 3 whereas several novel and promising pet tracers have been reported.4 however , no prospective clinical trials had tested the superiority of one tracer over the others in terms of diagnostic accuracy . published online july 30 , 2019 s1470 - 2045 ( 19 ) 30501 - 7 see articles page 1286 vol 20 september 201 9 1193 comment corrections published online march 25 , 2015 s1470 - 2045 ( 14 ) 71115 - 5 correction to lancet oncol 2013 ; 14 : e374 correction to lancet oncol 2015 ; 16 : e163 correction to lancet oncol 2015 ; 16 : 447 , 448 weller m , p ster sm , wick w , hegi me , reifenberger g , stupp r . 
the rst sentence should read : exposure to passive smoke among never smokers does not seem to increase the chances of acquiring somatic mutations in genes linked to non - small - cell lung cancer in smokers , a new study shows . 
 vorinostat in patients with advanced malignant pleural mesothelioma who have progressed on previous chemotherapy ( vantage - 014 ) : a phase 3 , double - blind , randomised , placebocontrolled trial . 
lancet oncol 2015 ; 16 : 44756in the a liation section , p bass should be listed at netherlands in the funding cancer section in the summary and in the a liations , merck & co has been changed to merck & co , inc . 
 lancet oncol 2015 ; 16 : 54149in the key of gure 2 of this article , the boxes should indicate patients who were ct positive for disease , not those who were circulating tumour dna positive for disease . 
this correction has been made to the online version as of april 30 , 2015 , and the printed version is correct . vol 16 may 2015 e199 clinical trial registry reporting : a transparent solution needed on april 30 , 2019 , transparimed , buko pharmakampagne , test - aankoop , and health action international , advocacy organisations that are concerned with transparency in medical research and equal access to medicines , released a document on the reporting of clinical trial data for 30 european universities that sponsor the largest number of trials governed by eu clinical trials regulation . 
the report shows that 778 ( 83% ) of 940 clinical trials sponsored by these universities due to post their results on the eu clinical trials register ( eudract ) had not done so . 
 this inaction violates eu rules that took effect in july , 2014 , which require all clinical trials registered in eudract to post summary results within 12 months of study completion . 
given the clear importance and ethical imperative for public reporting of trial data , what can be done to guarantee trial outcome transparency ? the reasons for legally requiring data to be reported on a registry file at the end of a trial are manifold and are ultimately in place to safeguard patients , protect research funding , and ensure an open scientific enterprise . 
thus , it is shocking that , according to the report , 14 of 30 european universities assessed have not reported any summary data on registries for trials that have completed , irrespective of whether these data have been published in the academic literature . 
although other trial registries also require data reporting after trial completion ( eg , australia and new zealands anzctr , since october , 2018 ) , the scope of any potential underreporting in these national trial registries is currently unknown . 
 it is noteworthy that the european report highlights the uk as an important outlier , showing that , for the five uk universities assessed , 107 ( 69% ) of 155 completed trials have posted summary results in eudract . 
it should be noted , however , that improvements in reporting behaviour in the uk have been relatively recent ( for some , since november , 2018 ) and have been made by only a small number of universities . 
thus , maintaining and enforcing compliance in a larger number of universities is critical , and in the long term , especially as the number of registered clinical trials increases every year . who is responsible for holding universities ( and all trial sponsors ) accountable for updating these data and how ? the fda amendments act authorises fines of us$10 000 for violations , but has yet to issue one ( as of october , 2018 )  . 
perhaps if there were tougher mechanisms to enforce trial reporting eg , a national or an international watchdog , with the authority to act and also with the necessary infrastructure , personnel , and budget to do sothen trial reporting would improve . 
punishing offenders is one way to recoup wasted effort , confirm data reporting , and deter failures to report , but it discounts positive measures that encourage trial sponsors to behave pro - actively to keep registries up to date . consideration of the reasons why universities fail to update summary trial data at the end of a trial , might provide clues towards a solution . 
according to the latest who data , oncology trials represent the largest proportion of all clinical trials being done across the medical continuu universities already face many hurdles when undertaking clinical trials , including cost , workload demands , and bureaucracy , which are already overburdensome . 
could automated email reminders from the registry to upload summary data be a simple solution that has been overlooked ? regardless of the increased burden , a combination of efforts is needed to improve public reporting of trial results , and immediate and robust action is necessary to eliminate research waste , improve the overall transparency of medical research , and fulfil our ethical obligations to patients . 
 the lancet oncology for the report on clinical trial data reporting from 30 european universities see 01f35d_42e869002189401d80 a672d4ecff3f73.pdf ? index = true for more on the mandate to post clinical trial summary results in eudract see news / posting - clinical - trialsummary - results - europeanclinical - trials - database - eudractbecome - mandatory for more on the who best practice guidelines see results / jointstatement / en / for the report on clinical trial data reporting from 40 american universities see clinicaltrials / assets / download / universitytransparency report2019.pdf for more on the lancet reward campaign against research waste see thelancet.com / campaigns / efficiency vol 20 june 2019 editorial correction to lancet oncol 2017 ; 18 : 132737 correction to lancet oncol 2017 ; 18 : 133847 correction to lancet oncol 2017 ; 18 : e564 dimopoulos ma , goldschmidt h , niesvizky r , et al . 
 lancet oncol 2017 ; 18 : 132737in the results section of this article , the data presented for any - grade adverse diarrhoea events should read diarrhoea ( 168 [ 36% ] vs 185 [ 41% ] )  . 
 these corrections have been made to the online version as of sept 27 , 2017 , and the printed article is correct . myelodysplastic in patients with platzbecker u , germing u , gtze ks , et al . 
luspatercept for the treatment of anaemia lowerrisk syndromes ( pace - mds ) : a multicentre , openlabel phase 2 dose - finding study with long - term extension study . 
 18 : e564in the second paragraph of brian samuels affiliation , the sentence in parentheses should have read ( summit cancer centers , post falls , id , usa )  . 
in the third paragraph , the sentence and quote from brian samuels as should have samuels summarised , we decided to recapitulate the original phase 2 study in liposarcomas pazopanib is active in the treatment of liposarcomas , just as it is for other subtypes of sarcoma . 
the authors provide the foundation necessary for a call to action for clinicians , policy makers , and researchers focused on reducing the substantial burden that cancer afflicts upon young adults . 
 unfortunately , even in very high - hdi regions , cervical cancer remains one of the top five causes of cancer death in young adults , highlighting the failures of our current policies and approaches . 
 other than cervical cancer , few cases of cancer in young adults can be effectively detected with screening ; one exception being breast cancer screening among women with a known cancer - causing genetic mutation . 
this highlights the importance of primary care providers taking a thorough family history and promptly referring to genetic counselling , as well as potentially testing when appropriate , such that targeted screening regimens for identified cancer predisposition syndromes are initiated appropriately . 
to reduce the incidence of kaposis sarcoma and liver cancer , particularly in africa and parts of asia , there needs to be continued focus on the prevention of hiv and hepatitis c virus ( hcv ) transmission . 
to date , in developing regions of the world , health education around condom use and safer sexual practices , has resulted in reducing the number of new hiv infections . 
 improvements in cure rates for young adults with cancer have lagged behind younger children and older adults.2 many explanations are possible for these worse outcomes , including a smaller proportion of young adult patients on clinical trials , delays in diagnosis , and biological differences in cancers between those in young adults and adults . 
for example , stock and colleagues3 compared the outcomes of young adults treated on paediatric and adult clinical trials for acute lymphoblastic leukaemia ( all ) and noted superior outcomes among those treated on paediatric trials . 
a concerted effort to examine the biology of other 1554 vol 18 december 2017 comment cancers in young adults and to do focused clinical trials among this age group is warranted to improve the outcomes of these patients . 
 lifelong tara o henderson , * kevin c oeffinger department of pediatrics , university of chicago , chicago , il , usa ( toh ) ; and department of medicine , duke university , durham , nc 27705 , usa ( koc ) kevin.oeffinger@duke.edu we declare no competing interests . the author ( s )  . 
what determines the outcomes for adolescents and young adults with acute lymphoblastic leukemia treated on cooperative group protocols ? a comparison of childrens cancer group and cancer and leukemia group b studies . 
crizotinib was approved as frontline therapy based on results showing longer progression - free survival ( 109 months [ 95% ci 83139 ] ) than that seen with platinum - based chemotherapy ( 70 months [ 95% ci 6882 ] ; hazard ratio [ hr ] for progression or death 045 , 95% ci 035060 ; p < 0001 ) .2 however , crizotinib has poor cns penetration , and the cns is the most common site of disease progression in alk - positive patients.3 alectinib has gained favour as frontline therapy after publication of the results of the alex3 and j - alex4 trials in 2017 , which assessed alectinib versus crizotinib treatment in tki - naive patients . 
in alex , 3 median progression - free survival was significantly longer with alectinib than crizotinib ( not reached vs 111 months ; hr 047 , 95% ci 034065 ; p < 00001 )  . 
cns progression was observed more frequently in patients treated with crizotinib ( 12 - month incidence of 414% [ 95% ci 332494 ] ) than alectinib ( 94% [ 54147 ] )  . 
ceritinib has also been shown to confer longer progression - free survival than chemotherapy in the frontline setting , although 78% of patients had grade 3 or 4 toxicity.5 the choice of second - line therapy and beyond is based on previous treatment exposure , presence of an alk resistance mutation , and the tki side - effect profile . 
ceritinib , alectinib , and brigatinib have resulted in progression - free survival of 54 , 6 81 , 7 and 1291 months , respectively , in patients previously treated with crizotinib . 
for patients with measurable cns disease at baseline , intracranial overall responses were achieved by 12 ( 75% ) of 16 patients treated with alectinib7 and 12 ( 67% ) of 18 patients treated with brigatinib.1 notably , responses to ceritinib have been seen in patients with and without resistance mutations.6 however , ceritinib has notable toxicity , including causing increased trans aminases , diarrhoea , nausea , vomiting , and fatigue , which often result in dose reductions . 
 in this clinical context , alice shaw and colleagues8 lorlatinib , report a phase 1 , multicentre study of published online october 23 , 2017 s1470 - 2045 ( 17 ) 30708 - 8 this online publication has been corrected . 
the oe05 trial assessed whether increasing the duration and intensity of neoadjuvant chemotherapy further improved survival compared with the current standard regimen . methods oe05 was an open - label , phase 3 , randomised clinical trial . 
 eligibility criteria included who performance status 0 or 1 , adequate respiratory , cardiac , and liver function , white blood cell count at least 3 10 cells per l , platelet count at least 100 10 platelets per l , and a glomerular filtration rate at least 60 ml / mparticipants were randomly allocated ( 1 : 1 ) using a computerised minimisation program with a random element and stratified by centre and tumour stage , to receive two cycles of cisplatin and fluorouracil ( cf ; two 3 - weekly cycles of cisplatin [ 80 mg / m intravenously on day 1 ] and fluorouracil [ 1 g / m per day intravenously on days 14 ] ) or four cycles of epirubicin , cisplatin , and capecitabine ( ecx ; four 3 - weekly cycles of epirubicin [ 50 mg / m ] and cisplatin [ 60 mg / m ] intravenously on day 1 , and capecitabine [ 1250 mg / m ] daily throughout the four cycles ) before surgery , stratified according to centre and clinical disease stage . 
this trial is registered with the isrctn registry ( number 01852072 ) and clinicaltrials.gov ( nct00041262 ) , and is completed . findings between jan 13 , 2005 , and oct 31 , 2011 , 897 patients were recruited and 451 were assigned to the cf group and 446 to the ecx group . 
no unexpected chemotherapy toxicity was seen , and neutropenia was the most commonly reported event ( grade 3 or 4 neutropenia : 74 [ 17% ] of 446 patients in the cf group vs 101 [ 23% ] of 441 people in the ecx group )  . 
the proportions of patients with postoperative complications ( 224 [ 56% ] of 398 people for whom data were available in the cf group and 233 [ 62% ] of 374 in the ecx group ; p = 0089 ) were similar between the two groups . 
one patient in the ecx group died of suspected treatment - related neutropenic sepsis . interpretation four cycles of neoadjuvant ecx compared with two cycles of cf did not increase survival , and cannot be considered standard of care . 
our study involved a large number of centres and detailed protocol with comprehensive prospective assessment of health - related quality of life in a patient population confined to people with adenocarcinomas of the oesophagus and gastro - oesophageal junction ( siewert types 1 and 2 )  . 
alternative chemotherapy regimens and neoadjuvant chemoradiation are being investigated to improve outcomes for patients with oesophageal carcinoma . funding cancer research uk and medical research council clinical trials unit at university college london . copyright the author ( s )  . 
these meta - analyses showed a significant survival benefit after treatment with neoadjuvant chemotherapy , both overall and for the subset of patients with adenocarcinoma who were considered in this study . 
these meta - analyses were unable to assess the benefits of different neoadjuvant chemotherapy regimens , and we can identify no phase 3 randomised trials that have directly compared different regimens . added value of this study to our knowledge , this is the largest randomised trial investigating whether an alternative neoadjuvant chemotherapy regimen might offer a survival benefit over the standard of two cycles of cisplatin and fluorouracil ( cf )  . 
this trial showed that giving four cycles of epirubicin , cisplatin , and capecitabine ( ecx ) neoadjuvantly might increase the level of tumour regression , but does not lead to any survival benefit . implications of all available evidence for patients with oesophageal adenocarcinoma , two cycles of cf should remain the standard choice of neoadjuvant chemotherapy regimen . 
further research is ongoing into the use of neoadjuvant chemoradiotherapy , but little evidence exists that directly compares it to neoadjuvant chemotherapy . studies were specifically powered to detect any such difference . 
few studies have been done only in patients with oesophageal adenocarcinoma.2124 high - quality data on the effect of neoadjuvant chemotherapy or chemoradiotherapy on health - related quality of life ( hrql ) are scarce ; more information is needed for clinical decision making , where small survival benefits might only be achieved with detrimental effects on many aspects of hrql . the results of the previous medical research council ( mrc ) oe02 randomised clinical trial19 showed a survival advantage at 2 years with neoadjuvant chemotherapy and surgery over surgery alone ( 43% vs 34% ; 9% increase [ 95% ci 314 ] ) , with a hazard ratio ( hr ) of 079 ( 95% ci 067093 ) , so two - cycle cisplatin with fluorouracil was used for the control group in this study . 
the results showed a 5 - year survival of 36% ( 95% ci 3043 ) for perioperative chemotherapy and surgery compared with 23% ( 1729 ) for surgery alone ( overall survival hr 075 , 95% ci 060093 ) .25 because 45% of participants in the magic trial ( 34% of people who had surgery ) did not receive postoperative treatment ( a similar pattern was also seen in the ffcd - fnclcc 9703 trial22 ) , we concluded that further assessment of perioperative chemotherapy would be challenging and increased it was decided neoadjuvant therapy would be the best strategy . 
oral capecitabine is readily available and has been shown to be equivalent to intravenous fluorouracil in colorectal cancer , 26 so we decided to investigate four cycles of neoadjuvant epirubicin , cisplatin , and capecitabine ( ecx ) as the investigational group without postoperative chemotherapy . 
given the results of the magic trial , that increasing the duration of neoadjuvant chemotherapy from two cycles to four cycles and adding anthracycline to the established doublet regimen was considered the most promising strategy for improving outcomes in patients with oesophageal adenocarcinoma in this study . 
participants were of any age with surgically resectable histologically verified adenocarcinoma of the oesophagus ( including siewert types 1 and 2 gastro - oesophageal junction tumours ) stage ct1n1 , ct2n1 , ct3n0 / n1 , or ct4n0 / n1 where invasion was thought to be confined to diaphragm , crura , or mediastinal pleura and surgically resectable ( union for international cancer control [ uicc ] tnm staging28 )  . 
additionally , patients had to meet the following criteria : who performance status 0 or 1 and adequate respiratory and cardiac function ( forced expiratory volume in 1 sec of > 15 l and cardiac ejection fraction of 50% on echocardiography or multigated acquisition scan ) within 4 weeks of randomisation . 
 within 1 week of randomisation , liver function tests needed to be at most 15 - times normal , white blood cell count at least 3 10 cells per l , platelet counts at least 100 10 platelets per l , and the calculated or measured glomerular filtration rate at least 60 ml / min . 1250 vol 18 september 2017 articles assessment of disease stage required a contrastenhanced multislice ct scan from neck to pelvis and endo scopic ultrasonography within 4 weeks of randomisation . 
the final staging of patients ( and siewert classification ) was done on the basis of a multidisciplinary team discussion following endoscopy , endoscopic ultrasonography , ct , and laparoscopy if appropriate . ( radiologically patients were ineligible if investigations indicated blood - borne metastases assessed ) , peritoneal dissemination , local invasion involving the tracheobronchial tree , aorta , pericardium or lung , or abdominal para - aortic lymphadenopathy greater than 1 cm in diameter on ct scan or more than 6 mm in diameter on endoscopic ultrasonography . 
patients were also excluded if they had received any previous treatment for oesophageal cancer , had siewert type 3 cancer , a medical condition that was likely to compromise the proposed trial treatment . 
uncontrolled angina pectoris , myocardial infarction in the 6 months before entry into the trial , heart failure , clinically significant uncontrolled cardiac arrhythmias , or any patient with a clinically significant abnormal ecg , as well as patients with abnormal left ventricular ejection fraction ( lvef ) diagnosed on muga scan or echocardiography , including areas of abnormal contractility , were excluded . 
 patients with positive serology for hiv or hepatitis c , active hepatitis b , or were pregnant were also excluded . participating centres were considered eligible if they had a multidisciplinary team structure , had experience of twophase oesophagectomy with two - field lymphadenectomy ( unproctored surgeons were recommended to have done a minimum of 12 such operations before joining the trial ) , access to multislice ct and endoscopic ultrasonography equipment , and had pathologists who were experienced in reporting oesophageal cancer . the protocol was approved by the south west multicentre research ethics committee ( 04 / 6 / 005 ) and all patients gave written consent for participation in the study . 
the protocol had five amendments during the course of the trial , predominantly for administrative reasons or to add clarity ; amendments did not affect the eligibility or treatment of patients . 
the most recent version of the protocol ( version 6.0 ) is available online . randomisation and masking eligible patients were enrolled by staff at participating centres who then called the randomisation line at the mrc clinical trials unit at ucl ( london , uk )  . 
no masking to treatment allocation was done because of the difference in the number of chemotherapy cycles in the two groups . chemotherapy control group procedures the regimen was two 3 - weekly cycles of cisplatin and fluorouracil . 
cisplatin ( 80 mg / m ) was infused intravenously on day 1 and fluorouracil ( 1 g / m per day ) was administered intravenously on days 14 ( total 4 g / m )  . the investigational chemotherapy was four 3 - weekly cycles of ecx . 
epirubicin ( 50 mg / m ) and cisplatin ( 60 mg / m ) were given intravenously on day 1 and capecitabine ( 1250 mg / m daily ) was given orally continuously over all four cycles ( for a total of 12 weeks )  . protocols for chemotherapy dose modifications were provided for haematological , renal , neurological , and hepatic toxicities , and for palmarplantar erythema , stomatitis , diarrhoea , nausea , and vomiting . 
 centres were allowed to use a minimal access surgery approach after providing evidence that complication rates and lymph node yields were similar to an open surgery approach from at least 20 patients who had had minimal access oesophagectomy . the stomach was the preferred conduit for reconstruction based on the right gastric and right gastroepiploic vessels . 
lymph node clearance in the abdomen was at the origin of the left gastric artery and along the hepatic and splenic arteries , the upper lesser curve , and at the right and left cardiac lymph node stations . 
dissection at the diaphragm was used to minimise a positive radial or circumferential resection margin by inclusion of sufficient crural fibres and a cuff of diaphragm based on endoscopic ultrasonography and intraoperative appearances . 
the extent of proximal lymphadenectomy for the upper paraoesophageal nodes was determined by the extent of division of the oesophagus ( ie , the length of oesophagus remaining after resection )  . reconstruction was recommended above the aortic arch for the right - sided approach and just below it for the left , and preferably within 5 cm of the thoracic inlet . 
trans - hiatal surgery was not permitted . postoperative complications , described as none , present but not life threatening , or life threatening , were for the oe05 clinical trial protocol version 6.0 see research / documents / cancer_ protocols / oe05_protocol_ version_6_23_dec_09.pdf vol 18 september 2017 1251 articles recorded for each patient . 
these complications were reviewed clinically , and assigned to categories . processing of the surgical resection specimens and histopathological assessment of all materials were done according to the recommendations of the royal college of pathologists : 30 r0 , no tumour cells remaining within 1 mm of any resection margin ; r1 , microscopically visible positive margin indicating the presence of tumour cells at or within 1 mm of a longitudinal or radial or circumferential resection margin ; and r2 , macroscopically visible tumour remaining . 
for patients not listed in above , cause of death was reported as sepsis - related multiple organ failure in one patient and oesophageal cancer in the remaining two patients . 
 in terms of both interobserver agreement ( ie , likelihood of two pathologists concluding the same grading by their independent assessments ) and prognostic ability.32 , 33 pathology data were collected from local pathologists at each centre , and used for the primary analyses of all pathology data . 
the hrql protocol prespecified four domains of hrql to be examined in the primary analyses and full details of all scales and items assessed in the questionnaires will be reported subsequently . 
clinical follow - up involved the same schedule with the use of tests to establish recurrent disease at the discretion of individual centres . outcomes the primary outcome measure of the trial was overall survival . 
secondary outcomes were disease - free survival , effects on the primary tumour ( as assessed by mandard trg ) , hrql , and morbidity related to chemotherapy and surgery . 
exploratory outcomes were progression - free survival ( where a progression - free survival event was defined as the first confirmed local or distant recurrence , or death from any cause ) , and an analysis of mandard trg using an amended responder definition . statistical analysis the sample size calculations were based on the primary outcome measure of overall survival . 
on the basis of the oe02 trial results , 19 which showed an absolute survival difference of 8% at 3 years , we thought it unlikely that any greater difference would be seen in this study . 
with a 5% two - sided significance level , this sample would provide 90% power to detect an 8% difference ( or 1252 vol 18 september 2017 articles 80% power to detect a 7% difference ) in 3 - year survival , from 30% in the cf group . 
in 2007 , following a period of lower than expected recruitment , the sample size was reassessed to ensure that an adequately powered study would still be achieved in a given timeframe . 
the updated sample size calculations required 842 patients with 677 events over 6 years with a minimum follow - up of 2 years before analysis , to provide at least 82% power to detect an 8% difference ( and 70% to detect a 7% difference ) at 3 years with a two - sided significance level of 5% . although we anticipated that the required events would be obtained 2 years after the final patient was randomly assigned , they accrued far more slowly than expected . 
 3 years after the final randomisation , a conditional survival analysis was done to assess the probability that continuing to wait for the full number of events would lead to a different trial conclusion . 
after discussion with the independent data monitoring committee and trial steering committee , a decision was reached that the current data were sufficiently robust for full analysis and dissemination , because the chance of obtaining a different conclusion with more events was less than 5% . all safety and primary analyses were done on an intention - to - treat basis . 
 patients either lost to follow - up or still alive at the time of analysis were censored at the date they were last known to be alive . because patients can only be deemed disease free after surgery , and to account for the different durations of preoperative chemotherapy , disease - free survival was analysed using a landmark analysis.36 rather than the date of randomisation , the time 1 week after the last patient had surgery was used as the start point , up to a maximum of 6 months from group assignment . 
patients who had an event before this point , who did not have surgery , or who were not macroscopically disease free at surgery , were said to have had an event on day 1 . 
 disease - free survival was calculated as the time from this modified origin until the first date of confirmed local recurrence , distant metastases , or death from any cause . 
 patients who had no evidence of relapse were censored on the last date they were known to be disease free . progression - free survival was calculated from random assignment to the date of the event or , in event - free patients , the date last known to be alive and free from recurrence . 
 specific site of t4 invasion is mediastinal pleura for eight patients ( four in the cisplatin and fluorouracil group vs four in the epirubicin , cisplatin , and capecitabine group ) , crura for 14 patients ( nine vs five ) , and diaphragm for five patients ( two vs three )  . table 1 : baseline characteristics grambsch - therneau test . 
the heterogeneity of treatment effects across levels of prespecified patient characteristics ( sex , age , performance status , clinical t - stage , and clinical n - stage ) were explored using cox proportional hazard models . to analyse tumour regression , the original five - point into responders mandard scale was dichotomised ( mandard trg 13 ) and non - responders ( mandard trg 45 )  . 
a second , unplanned analysis was also done because emerging evidence suggested that a more appropriate dichotomisation was mandard trg 12 as responders and grades 35 as non - responders . formal comparisons and summaries of hrql function and symptom scales were restricted to a number of prespecified outcome measures . 
global hrql and the effects of prespecified symptoms related chemotherapy and surgery ( appetite loss , dysphagia , pain , and reflux ) were compared immediately before surgery , and 3 , 12 , and 24 months after surgery , using an anova with adjustment for baseline score . 
these timepoints were considered separately , rather than using a repeated measures method of analysis . between comparisons toxicities , surgical complications , tumour regression , and resection were done using a test or fishers exact test , as appropriate . 
the corresponding author had final responsibility for the decision to submit for publication . results between jan 13 , 2005 , and oct 31 , 2011 , 897 patients were recruited from 72 uk hospitals and randomly allocated to the cf group ( n = 451 ) or the ecx group ( n = 446 ; figure 1 )  . 
the median number of patients per centre cisplatin and fluorouracil ( n = 451 ) epirubicin , cisplatin , and capecitabine ( n = 446 ) 411 ( 91% ) 387 ( 87% ) 40 ( 9% ) 59 ( 13% ) 3 ( 8% ) 11 ( 19% ) 6 ( 10% ) 4 ( 10% ) 4 ( 7% ) 6 ( 15% ) 2 ( 5% ) 1 ( 3% ) 9 ( 15% ) 7 ( 12% ) 8 ( 14% ) reason for no surgery * ct evidence of disease progression 13 ( 33% ) clinical evidence of disease progression laparoscopic evidence of disease progression surgery done comorbidity patient choice patient died resection done patient otherwise deemed inoperable 11 ( 28% ) 14 ( 24% ) surgical approach abdomen and right chest open abdomen ( laparoscopic ) and right chest open left thoracoabdominal incision totally laparoscopic other missing location mid - oesophagus siewert type 1 siewert type 2 missing 192 ( 50% ) 108 ( 28% ) 187 ( 51% ) 101 ( 28% ) 28 ( 7% ) 9 ( 2% ) 43 ( 11% ) 7 ( 2% ) 24 ( 7% ) 9 ( 2% ) 35 ( 10% ) 8 ( 2% ) 72 ( 19% ) 56 ( 15% ) 227 ( 59% ) 208 ( 57% ) 76 ( 20% ) 12 ( 3% ) 89 ( 24% ) 11 ( 3% ) data are n ( % )  . 
an open - close operation was deemed as one in which no resection was done , or the reason given on the case report form for not having surgery was that the patient was found to be inoperable at laparotomy or thoracotomy . 
after was eight chemotherapy , following retrospective review of the baseline ct scan , one patient was found to be ineligible because of adrenal metastases so did not have surgery , but was included in all summaries and analyses . 
the median age was 62 years ( iqr 5667 ; range 2781 ) , 810 ( 90% ) of 897 patients were male , 603 ( 67% ) had a who performance status of 0 , and 576 ( 64% ) had stage t3n1 cancer ( table 1 ; appendix pp 45 )  . three ( 4% ) of 72 recruiting centres did not take part in the hrql aspect of the trial for any of their patients , and hrql assessment data were omitted at baseline for the [ 4% ] of the total patients from these centres ( 37 897 patients )  . 
baseline hrql was also well balanced see online for appendix 1254 vol 18 september 2017 articles ( 1834 ) , appetite ( 2405 ) , pain 203 between the two groups . 
mean values ( sd ) for the five prespecified domains of interest were : global hrql ( 2798 ) , 760 reflux 173 ( 2050 ) , and dysphagia 739 ( 257 ) ; data per treatment group are in the appendix ( pp 810 )  . 
a higher score indicates better hrql for the global score and dysphagia , but worse hrql for the symptom scales . loss 374 details of the chemotherapy received are shown in table 2 . 
four patients ( < 1% ; two in the cf group and two in the ecx group ) of 897 withdrew consent before starting chemotherapy and five ( 1% ; one cf , four ecx ) died during chemotherapy . 
the number of patients who completed their allocated treatment was greater in the cf group than in the ecx group ( 435 [ 96% ] of 451 vs 363 [ 81% ] of 446 ; p < 00001 ) , although a similar number of patients in the cf ( 435 [ 96% ] of 451 ) and ecx ( 432 [ 97% ] of 446 ) groups received at least two cycles . 
of the 451 patients in the cf group , eight ( 2% ) stopped chemotherapy because of toxicity and one ( < 1% ) died , whereas in the ecx group , 46 ( 10% ) of 446 patients stopped because of toxicity , and five ( 1% ) died , one of which was thought to be related to chemotherapy toxicity ( figure 1 )  . 
the number of patients requiring dose reduction to any drug was smaller in the cf than in the ecx group ( 88 [ 20% ] of 451 vs 187 [ 42% ] of 446 ; p < 00001 ) , although the number receiving cisplatin dose reductions was similar between the groups ( 61 [ 14% ] of 451 in the cf group and 53 [ 12% ] of 446 in the ecx group )  . the median time from randomisation to surgery was 71 days ( iqr 6680 ) in the cf group and 127 days ( 119137 ) in the ecx group . 
the median time of surgery from the start of the last preoperative chemotherapy cycle was 44 days ( 3952 ) for patients in the cf group and 57 days ( 5264 ) for patients in the ecx group . 
of the 99 who did not have surgery , 41 ( 41% ) were because of disease progression , nine ( 9% ) died before surgery , nine ( 9% ) decided not to have surgery , that ( 15% ) developed significant comorbidities precluded surgery , and 25 ( 25% ) were deemed otherwise unsuitable for surgery . 
in total , 411 ( 91% ) of 451 patients in the cf group and 387 ( 87% ) of 446 patients in the ecx group proceeded to surgery ( figure 1 )  . 751 ( 84% ) of 897 people had resection and reconstruction , whereas 47 ( 5% ) of 897 patients were found to have progressive disease or to be inoperable during surgery ( table 3 )  . 
588 ( 78% ) of 751 resections were done via the abdomen and right chest using open surgery throughout ( ivor - lewis resection ) or as hybrid with a laparoscopic abdominal approach . 
the median follow - up of the surviving patients was 64 years ( iqr 4882 ) , and 250 ( 93% ) of 268 patients had at least 3 years of follow - up assessments . 
median overall survival was estimated to be 234 months ( 95% ci 206263 ) in the cf group and 261 months ( 225297 ) in the ecx group , with an hr of 090 ( 95% ci 077105 , p = 019 )  . 
no evidence indicated that the proportional hazards assumption was violated . figure 3 shows prespecified subgroup analyses of overall survival were done , considering sex , age group ( < 60 years , 6069 years , and 70 years ) , who performance status , clinical t - stage , and clinical n - stage ( appendix p 11 )  . median disease - free survival ( 347 events in the cf group vs 316 events in the ecx group , based on a 6 - month landmark analysis ; appendix p 13 ) was 116 months ( 95% ci 89133 ) in the cf group and 144 months ( 117165 ) in the ecx group , with an hr of 086 ( 95% ci 074100 , p = 0051 )  . chemotherapy toxicity data were not provided by three patients in each group and two in each group did not receive any chemotherapy . 
p values for heterogeneity of treatment effect are 069 for sex , 005 for age , 046 for who performance status , 011 for t - stage , and 0028 for n - stage . 
one patient in the epirubicin , cisplatin , and capecitabine group died of cerebrovascular incident ( reported as other toxicity )  . table 4 : chemotherapy toxicity group ( 0 , p < 00001 )  . 
 in patients for whom data were reported , no difference was seen in the overall prevalence of surgical complications between the two treatment groups ( 224 [ 56% ] of 398 people in the cf group and 233 [ 62% ] of 374 in the ecx group ; p = 0089 ) , although more people in the ecx group had respiratory complications ( 125 [ 33% ] of 374 ) than in the cf group ( 107 [ 27% ] of 398 ; p = 0048 ; appendix p 7 )  . 
at 30 days after surgery , ten ( 2% ) of 411 patients in the cf group and 11 ( 3% ) of 387 people in the ecx group had died , and at 90 days , 21 ( 5% ) people in the cf group and 23 ( 6% ) people in the ecx group had died . in the local pathologist review ( table 5 ) , the primary tumour was classified as mandard trg 13 in 44 ( 15% ) of the 288 specimens with available results from the cf group and 93 ( 32% ) of the 289 specimens from the ecx group ( p < 00001 )  . 
mandard primary tumour regression data were also available from central pathology review of 656 patients ( 87% of patients who had a resection ) and a total of 24 625 slides were received , with a median of 34 ( iqr 2445 ) slides per person . 
the proportions of patients who achieved r0 , r1 , and r2 were similar in both groups . no statistically and clinically relevant differences were seen between the treatment groups in terms of hrql ( appendix pp 810 ) in any of the prespecified domains ( global quality of life , pain , reflux , appetite loss , or dysphagia ) or at nearly all timepoints ( preoperatively and 3 , 12 , and 24 months postoperatively )  . 
r0 = no tumour cells within 1 mm of any resection margr1 = presence of tumour cells at or within 1 mm of a longitudinal or radial or circumferential resection marg r2 = macroscopically visible tumour left behind during surgery . 
the proportion of surviving patients who time , completed hrql assessments declined over with 725 ( 84% ) of 860 patients completing an assessment at randomisation , 339 ( 57% ) of 595 at 3 months after surgery , 208 ( 45% ) of 467 at 12 months , and 142 ( 44% ) of 322 at 24 months . when the trial and analyses were planned , we felt that mandard trg 1 , 2 , or 3 was the most suitable definition of good response to treatment . 
exploratory analyses ( appendix p 14 ) in patients who had available specimens suggested that postoperative survival of patients with tumours considered to be mandard trg 1 or 2 was significantly different ( appendix p 14 ) to survival in those with tumours considered to be mandard trg 3 , 4 , or 5 , so mandard trg 1 or 2 appeared to denote significant tumour regression . 
applying this definition to the locally collected histopathological data , 18 ( 6% ) of 288 patients in the cf group and 48 ( 17% ) of 289 patients in the ecx group regression ( p < 00001 )  . 
similarly , using the central review data , 12 ( 4% ) of 339 patients in the cf group and 37 ( 12% ) of 317 patients in the ecx group achieved notable tumour regression ( p < 00001 )  . significant achieved tumour in the exploratory analysis of progression - free survival , median progression - free survival ( 343 events in the cf group vs 313 in the ecx group ; appendix p 13 ) was vol 18 september 2017 1257 articles 184 months ( 95% ci 152205 ) in the cf group and 214 months ( 194240 ) in the ecx group , with an hr of 084 ( 95% ci 072098 , p = 0033 )  . 
the contributing progression - free survival event was either local recurrence ( 60 [ 17% ] of 343 patients in the cf group vs 46 [ 15% ] of 313 in the ecx group ) , distant metastases ( 94 [ 27% ] of 343 people vs 78 [ 25% ] of 313 ) , local recurrence and distant metastases ( 87 [ 25% ] of 343 vs 59 [ 19% ] of 313 ) , or death without confirmed progression ( 102 [ 30% ] of 343 vs 130 [ 42% ] of 313 )  . an exploratory analysis highlighted that the overall survival hr did not remain constant over time , and a strong interaction with year of randomisation was seen ( p = 00004 ; appendix p 12 )  . 
patients randomly assigned early in the trial ( 200507 ) had some survival benefit in the ecx group compared with those in the cf group , whereas those assigned in later years ( 2008 onwards ) did not . 
the use of pet scans increased greatly over the course of the trial , and so a further exploratory subgroup analysis was done looking at the effect of receiving a pet scan . 
 patients who did not have a pet scan had longer overall survival in the ecx group , whereas for patients who did receive a pet scan , ecx gave no survival advantage . discussion this study showed that more intensive neoadjuvant chemotherapy with four cycles of ecx provided no overall or disease - free survival advantage over two cycles of cf in 897 patients with oesophageal adenocarcinoma . 
chemotherapy toxicity and serious adverse events were reported more often with ecxas can be expected from four cycles of a triplet regimen compared with two cycles of a doublet regimen . 
these adverse events contributed to a greater number of patients completing their planned chemotherapy and undergoing surgery in the cf group than in the ecx group , although surgical resection , postoperative complications , and postoperative mortality were similar between the groups . 
in a post - hoc exploratory analysis , improved progression - free survival was shown with ecx treatment compared with cf treatment . more patients in the ecx group had a good pathological response to chemotherapy ( mandard trg 1 or 2 ) , and consequently more were staged as ypt0 or 1 or ypn0 after surgery , than were those in the cf group . 
results from the mrc gastro - oesophageal st0338 study showed that mandard trg 1 or 2 after chemotherapy was associated with improved survival compared with mandard trg 3 , 4 , or 5 . 
however , the absolute numbers of specimens assessed that were classified as mandard trg 1 or 2 ( 48 [ 17% ] of 289 in the ecx group vs 18 [ 6% ] of 288 in the cf group ) were low , and so this difference did not translate into an overall survival benefit . the results of this trial raise the question of the optimal number of preoperative chemotherapy cycles . 
in the current absence of a reliable biomarker that enables prediction of responses either before or midway through preoperative treatment , the extent of preoperative chemotherapy relies on the judgement of the clinician after discussion with the patient , to balance the possibility of achieving a good response against the risk of not being able to proceed to surgery . 
 however , two cycles of cf preoperatively has not been the perioperative approach directly compared with assessed in the magic trial , 25 which studied three cycles of ecx given preoperatively and post operatively . 
given the increased proportion of patients who achieved a response with ecx treatment in our study , a smaller number of preoperative cycles ( two or three ) with a triplet regimen combined with the selective use of postoperative chemotherapy for responding patients might be a better approach than either four cycles of ecx or two cycles of cf . oe05 showed an improvement in overall survival of patients in the cf group ( recruited 200511 ) compared with the same regimen in oe02 ( recruited 199298 ) , in which the median survival was 14 years compared with 20 years in oe05 . a number of potential factors could explain why the survival of patients with oesophageal cancer who were treated with cf improved with time . 
changes in referral patterns , moves towards centralisation of surgical services , the introduction of endoscopic ultrasonography , and the development of multidisciplinary teams are all events that occurred towards the end of recruitment to the oe02 study , and these changes might have led to better patient selection for attempted curative treatment by the time of this oe05 study . 
post - hoc analyses indicated that ecx offered a survival benefit in the early years of the study when pet scans were rarely used , but offered no benefit during the later years when pet was used for nearly all patients . 
patients with this type of disease are now usually identified and would have been ineligible for participation in the study . neoadjuvant chemoradiotherapy has also improved survival compared with surgery alone for patients with oesophageal adenocarcinoma and squamous cell cancers , with a median survival of 486 months ( 95% ci 321651 ) with adjuvant therapy compared with led 1258 vol 18 september 2017 articles 240 months ( 95% ci 142337 ) with surgery alone in the cross trial.39 the hrs for comparison with surgery alone are similar with chemoradiotherapy in cross ( 073 [ 95% ci 055088 ] in patients with adeno carcinoma ) and with chemotherapy in magic ( 075 [ 060093 ] ) , suggesting trials studied slightly different that although populations , the size of benefit might be similar . 
trials comparing these two approaches directly20 , 23 , 24 have shown an increased response with chemo radiotherapy , but without any subsequent improvement in overall survival . the the present study has a number of advantages over other oesophageal cancer trials . 
this study was confined to patients with adenocarcinomas of the oesophagus and gastro - oesophageal junction ( siewert type 1 and 2 ) , specifically excluding squamous cell cancers and siewert type 3 ( gastric cancer )  . 
to our knowledge , our study is the only prospective randomised trial in neoadjuvant treatment and surgery for oesophageal cancer to have included a comprehensive prospective assessment of hrql using validated generic and specific measures . 
 although no differences between trial groups were observed in hrql , the data confirm findings from much smaller cohort studies.40 neoadjuvant chemotherapy and surgery are associated with reduced hrql that persists for more than 6 months after surgery , and some features such as appetite loss persist for at least 12 months . 
 these hrql results should be accepted as the standard that can be achieved with current platinum - based or fluoropyrimidine - based neoadjuvant chemotherapy and surgery , and communicated to patients during shared decision making before surgery , along with the likely median survival data of the combined interventions . 
 limitations of this study include the changing use of pet scanning through the course of this trial as we have discussed and its potential effect on the prognosis of patients who entered the trial over time . 
additional limitations are the fact that postoperative chemotherapy was not assessed , and the challenge of interpreting and implementing these results in the face of the evolving role of chemoradiation in the management of oesophagogastric adenocarcinomas . data published in 2017 show a survival advantage for patients treated with docetaxel , oxaliplatin , and fluorouracil compared with epirubicin , cisplatin , and fluorouracil or ecx given perioperatively for junctional and gastric tumours , with a 3 - year overall survival of 57% for the docetaxel - containing regimen compared with 48% with epirubicin , cisplatin , and fluorouracil or ecx ( hr 077 , 95% ci 063094 ) .41 though an improvement in overall survival for biomarker - unselected patients , these results highlight that further improvements in outcomes are still needed for these patients . 
alternative neoadjuvant approaches such as chemoradiation are also being investigated.42 , 43 additional correlative science projects are planned for this trial with the aim of identifying subsets of patients who might specifically benefit from ecx neoadjuvant chemotherapy . contributors da and dc were joint chief investigators . 
all authors were involved in data interpretation , manuscript review , and approval of the final manuscript . declaration of interests dc reports grants from amgen , astrazeneca , bayer , celgene , merrimack , medimmune , merck serono , sanofi , and the national institute of health biomedical centre at the institute of research and royal marsden hospital . 
 also , in the patients with nsclc column in table 1 of this article , and in the 30 - day mortality columns in tables 2 , 3 , 5 and 7 of this article , some percentages were incorrect . 
 these corrections have been made to the online version as of aug 31 , 2016 . published online september 1 , 2016 s14702045 ( 16 ) 30440 - 5 sartore - bianchi a , trusolino l , martino c , et al . 
dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - ofconcept , multicentre , open - label , phase 2 trial . 
lancet oncol 2016 ; 17 : the declaration of interests section of this review , the declaration for rk should have included and has received lecture fees from japan vaccine co ltd and msd for lectures on the safety and e ectiveness of the hpv vaccine . 
 folfiri plus cetuximab versus folfiri plus bevacizumab for metastatic colorectal cancer ( fire - 3 ) : a post - hoc analysis of tumour dynamics in the final ras wild - type subgroup of this randomised open - label phase 3 trial . 
this correction has been made to the online version as of sept 1 , 2016 , and the printed version is correct . correction to lancet oncol 2016 ; 17 : e423 burki tk . 
this correction has been made to the online version as of oct 4 , 2016 . vol 17 october 2016 e420 corrections correction to lancet oncol 2015 ; 16 : e539 correction to lancet oncol 2016 ; 17 : e335 okada h , weller m , huang r , et al . 
lancet oncol 2015 ; 16 : e53442in table 1 of this review , in the progressive disease row , 25% decrease , 25% decrease , and 20% decrease should read 25% increase , 25% increase , and 20% increase , respectively . 
this correction has been made to the online version as of aug 30 , 2016 . vol 17 september 2016 e373 published online may 21 , 2020 s1470 - 2045 ( 20 ) 30287 - 4 for more on the costs of covid - 19 to uk universities see news / documents / uuk_ achieving - stability - highereducation - april - 2020.pdf for more on the situation in us universities see aau - files / key - issues / highereducation - legislation / instuitionaland studentaidproposal.pdf for the financial impacts of covid - 19 on universities in australia see universitiesaustralia.edu.au / media - item / uni - viability - crucialto - national - recovery / covid - 19 : consequences for higher education the covid - 19 pandemic has already cost uk universities an estimated 790 million . 
in the 2017 fiscal year , the us higher education sector earned about us$446 billion in so - called auxiliary revenues , such as bookstores , halls of residence , and summer camps . 
meanwhile , australia expects its higher education sector to lose somewhere in the region of aus$346 billion for the 201920 academic year . universities worldwide have been forced rapidly to scale up online teaching , which has typically entailed unexpected expenditure . 
yet , sizeable as the losses are for the current academic year , they could easily be dwarfed by those expected next year . the economic downturn will force thousands of youngsters to defer entering university . 
encouraged by successive governments , who wished to bolster commercial education , institutions have come to rely on this money , which represents about a third of the total income from tuition fees . 
terry hartle ( vice - president of the american council on education , washington , dc , usa ) expects international enrolments in us universities and colleges to fall by at least a quarter in 202021 . prospective students might also be put off by the physical distancing requirements that are likely to prevail on university campuses for the foreseeable future . 
very few schools in the usa are certain that they will be able to open on time . the shift to online learning looks set to continue at least until the advent of a successful vaccine for covid - 19 . 
students generally report that university is much more than just tuitionplace is also really important , said simon marginson ( professor of higher education at the university of oxford , oxford , uk )  . 
 if students are going to miss half of what usually constitutes the student experience , are they really receiving the same value for money ? furthermore , online learning is no substitute for laboratory work . moreover , recessions diminish the prospects for graduate employment . 
 you have a downgrading of the student experience and a downgrading of the value of the degree ; i think it is going to be difficult for universities to sustain the same level of fees that they have been , said marginson . 
without any action , universities will be forced to make huge cuts , jobs will be lost , and vital research will be halted , a spokesperson for universities uk , an umbrella group representing 137 institutions , told the lancet oncology . pretty much every university in the country is looking at voluntary redundancies , added malcolm reed ( dean of brighton and sussex medical school , brighton , uk , and co - chair of the medical schools council , london , uk )  . 
a lot of staff on short - term contracts are likely to go , and funding for phds is looking very precarious because of the impact on charities ; our pool of future researchers is going to be shallower . 
 prestigious research institutions , such as harvard ( cambridge , ma , usa ) or oxford ( uk ) universities , are well placed to weather the coming stor but places that fall lower down the league tables are vulnerable , especially if international student fees form a big part of their income . 
if the university is under threat , so is the medical school , he said . clinical placements for uk medical students in their penultimate year have been suspended since march . 
it would be a real threat to graduating on time next year . as the lancet oncology went to press , the number of confirmed cases of covid - 19 worldwide was approaching 5 million . 
it is going to leave a huge impression on the education sector . talha khan burki 758 vol 21 june 2020 news weekly platinum - based chemotherapy versus 3 - weekly platinum - based chemotherapy for newly diagnosed ovarian cancer ( icon8 ) : quality - of - life results of a phase 3 , randomised , controlled trial sarah p blagden , adrian d cook , christopher poole , lesley howells , ian a mcneish , andrew dean , jae - weon kim , dearbhaile m odonnell , jane hook , elizabeth c james , ian r white , timothy perren , rosemary lord , graham dark , helena m earl , marcia hall , richard kaplan , jonathan a ledermann , andrew r clamp summary background the icon8 study reported no significant improvement in progression - free survival ( a primary endpoint ) with weekly chemotherapy compared with standard 3 - weekly treatment among patients with epithelial ovarian cancer . 
 all icon8 patients were eligible to take part in the accompanying health - related quality - of - life study , which measured the effect of treatment on self - reported wellbeing , reported here . methods in this open - label , randomised , controlled , phase 3 , three - arm , gynecologic cancer intergroup ( gcig ) trial done at 117 hospital sites in the uk , australia , new zealand , mexico , south korea , and republic of ireland , women ( aged at least 18 years ) with newly diagnosed , histologically confirmed international federation of gynecology and obstetrics stage iciv ovarian cancer and an eastern cooperative oncology group performance status of 02 were randomly assigned ( 1 : 1 : 1 ) centrally using minimisation to group 1 ( intravenous carboplatin area under the curve [ auc ] 5 or auc6 and 175 mg / m intravenous paclitaxel every 3 weeks ) , group 2 ( carboplatin auc5 or auc6 every 3 weeks and 80 mg / m paclitaxel weekly ) , or group 3 ( carboplatin auc2 weekly and 80 mg / m paclitaxel weekly )  . 
patients were asked to complete european organisation for research and treatment of cancer qlq - c30 and qlq - ov28 questionnaires at enrolment , before each chemotherapy cycle , then 6 - weekly up to 9 months , 3 - monthly up to 2 years , and 6 - monthly up to 5 years . 
within the quality - of - life study , the co - primary endpoints were qlq - c30 global health score at 9 months ( cross - sectional analysis ) and mean qlq - c30 global health score from randomisation to 9 months ( longitudinal analysis )  . 
the trial is registered on clinicaltrials . gov , nct01654146 and isrctn registry , isrctn10356387 , and is currently in long - term follow up . findings between june 6 , 2011 , and nov 28 , 2014 , 1566 patients were recruited into icon8 ( 522 were included in group 1 , 523 in group 2 , and 521 in group 3 )  . 
baseline quality - of - life questionnaires were completed by 1438 ( 92% ) of 1566 patients and 9 - month questionnaires by 882 ( 69% ) of 1280 patients . 
we observed no significant difference in global health score at 9 months ( cross - sectional analysis ) between study groups ( group 2 vs group 1 , difference in mean score 23 , 95% ci 04 to 49 , p = 0095 ; group 3 vs group 1 , 08 , 38 to 22 , p = 061 )  . 
using longitudinal analysis , we found lower global health scores for those receiving weekly paclitaxel than for those receiving 3 - weekly chemotherapy ( group 2 vs group 1 , mean difference 18 , 95% ci 36 to 01 , p = 0043 ; group 3 vs group 1 , 29 , 47 to 11 , p = 00018 )  . interpretation we found no evidence of a difference in global quality of life between treatment groups at 9 months ; however , patients receiving weekly treatment reported lower mean quality of life across the 9 - month period after randomisation . 
taken together with the lack of progression - free survival benefit , these findings do not support routine use of weekly paclitaxel - containing regimens in the management of newly diagnosed ovarian cancer . funding cancer research uk , medical research council , health research board ireland , irish cancer society , and cancer australia . copyright 2020 the author ( s )  . 
 the japanese jgog - 3016 study reported improved survival outcomes with no detriment to quality of life in patients with newly diagnosed ovarian cancer for weekly , dose - dense , paclitaxel and 3 - weekly carboplatin , compared with standard 3 - weekly carboplatin and paclitaxel . 
the gog - 0262 study compared similar dose schedules , but most patients also received bevacizumab , and the study reported no progression - free survival benefit and poorer quality of life with weekly treatment compared with 3 - weekly treatment . 
 the mito - 7 study compared weekly carboplatin plus weekly paclitaxel with 3 - weekly carboplatin plus 3 - weekly paclitaxel and reported improved quality of life with weekly treatment over the 9 - week evaluation period . 
the evidence from these three studies was that weekly paclitaxel - containing treatment was superior to , or at best equivalent to , standard 3 - weekly treatment with little quality - of - life detriment to patients . added value of this study to our knowledge , icon8 is the largest study to date of weekly treatment for primary ovarian cancer . 
the quality - of - life results show that , although the global quality of life of patients was similar between the three treatment groups at 9 months , those receiving dose - dense paclitaxel had poorer quality of life during chemotherapy treatment , with more severe peripheral neuropathy that lasted for up to 18 months . patients could have either immediate primary debulking surgery followed by chemotherapy or upfront chemotherapy that was interrupted by delayed primary surgery ; patients who had delayed surgery reported less detriment to quality of life with weekly treatment than did patients with immediate surgery . implications of all the available evidence the contrasting results of icon8 and jgog - 0316 support a differential response to dose - dense paclitaxel between asian and white patients . 
with no progression - free survival benefit and poorer quality of life , the icon8 results do not support the general use of weekly treatment among a primarily european population . 
the study was prompted by the phase 3 jgog - 3016 trial in which weekly paclitaxel ( 80 mg / m ) in combination with 3 - weekly carboplatin ( area under the curve [ auc ] 6 ) was found to confer improved progression - free survival and overall survival when compared with standard treatment in japanese patients with advanced ovarian cancer.1 as there is increasing evidence of pharma cogenomic distinctions between asian and white populations , icon8 was designed to explore whether the survival advantage observed in jgog - 3016 could also be observed in a mostly european population with ovarian cancer.2 , 3 results from icon8 have shown that weekly , dose - dense paclitaxel - containing conferred no progression - free survival advantage when com pared with standard 3 - weekly treatment.4 as a secondary endpoint of the main study , the effect on health - related quality of life ( referred to as quality of life throughout this article ) was assessed during treatment and in follow - up . 
here we report the quality - of - life results from the icon8 study . chemotherapy methods study design and participants icon8 was an open - label , randomised , controlled , phase 3 , three - arm trial done at 117 hospital sites in the uk , australia , new zealand , mexico , south korea , and republic of ireland ( appendix pp 13 )  . 
detailed methods for icon8 have been previously reported.4 eligible patients were aged 18 years or older and had histologically confirmed , newly diagnosed high - risk international feder ation of gynecology and obstetrics ( figo ) stage ic - iia or any advanced ( figo stage iib - iv ) epithelial ovarian , primary peritoneal , or fallopian tube carcinoma ( collectively termed ovarian cancer )  . 
 other inclusion criteria were an eastern cooperative oncology group ( ecog ) performance status of 02 ; life expectancy longer than 12 weeks ; adequate haematological , renal , and hepatic function ; and able to start chemotherapy within 8 weeks after immediate primary debulking surgery . 
all patients gave written informed consent to join the trial . exclusion criteria included previous malignancy within 5 years , previous or synchronous early - stage endometrial 970 vol 21 july 2020 articles for the study protocol see studies / all - studies / i / icon8 / cancer , evidence of brain metastasis , and pre - existing sensory or motor neuropathy of grade 2 or above . in the uk , ethical approval was granted by the london chelsea research ethics committee . 
 the protocol can be found online . randomisation and masking patients were randomly assigned ( 1 : 1 : 1 ) to standard threeweekly carboplatin and paclitaxel ( group 1 ) , three - weekly carboplatin and weekly dose - dense paclitaxel ( group 2 ) , or weekly carboplatin and weekly dose - dense paclitaxel ( group 3 ; appendix p 4 )  . 
patients were randomly assigned with the medical research council clinical trials unit university college london randomisation telephone service ; the method of minimisation was used with stratification factors of gcig group , disease stage ( figo stage ic high grade serous , clear cell , or grade iii carcinoma ; stage iia high grade serous , clear cell , or grade iii carcinoma ; stage iib ; stage iic ; stage iiia ; stage iiib ; stage iiic ; stage iv ) , and outcome and timing of surgery ( immediate surgery plus figo stage iciii with no visible residual disease ; immediate surgery plus figo stage iciii with residual disease 1 cm ; immediate surgery plus figo stage iv or iciii with residual disease > 1 cm ; no surgery currently planned ; or delayed primary surgery planned )  . 
patients and clinicians were not masked to their allocated group . procedures patients entering the trial could have upfront debulking surgery before starting chemotherapy , referred to as immediate primary surgery , delayed primary surgery after at least three cycles of neoadjuvant chemotherapy , or no planned surgery . 
patients in group 1 received carboplatin area under the curve [ auc ] 5 or auc6 by intravenous infusion over 3060 min and paclitaxel 175 mg / m by intravenous infusion for 3 h on day 1 of a 21 - day cycle for six cycles ; patients in group 2 received carboplatin as in group 1 and dose - fractionated paclitaxel 80 mg / m by intravenous infusion for 1 h on days 1 , 8 , and 15 of a 21 - day cycle for six cycles ; and patients in group 3 received carboplatin auc2 by intravenous infusion for 3060 min on days 1 , 8 , and 15 and paclitaxel 80 mg / m by intravenous infusion for 1 h on days 1 , 8 , and 15 of a 21 - day cycle for six cycles . 
additional details regarding treatment have been published.4 protocoldefined dose alterations ( delay , reduction , or omission ) were allowed for haematological and other toxic effects if deemed clinically necessary , as described previously.4 all patients were included in the quality of life study and invited to complete european organisation for research and treatment of cancer qlq - c30 and qlq - ov28 questionnaires to provide a subjective measure of their quality of life over the preceding 7 days . 
the qlq - c30 contains 30 items , including a global health status score , five function scales ( physical , role , emotional , cognitive , and social ) and nine symptom scales or items ( fatigue , nausea or vomiting , pain , dyspnoea , insomnia , appetite loss , constipation , diarrhoea , and financial difficulties ) .5 the qlq - ov28 contains 28 items relevant to ovarian cancer , including abdominal or gastrointestinal symp toms , peripheral neuropathy , chemotherapy side - effects , hormonal or menopausal symptoms , body image , attitude to disease or treatment , and sexual functioning.6 for global health status and function scales , higher scores indicate better function ( improved quality of life ) but for symptom scales , higher scores indicate greater symptoms ( poorer quality of life )  . 
the qlq - c30 and qlq - ov28 questionnaires have undergone extensive psychometric validation and multiple translations and are acceptable to patients.57 we interpreted a change in global health score over time of more than 5 points as being clinically significant following the methodology of cocks and king , who defined a change in the score of less than 5 as clinically trivial.810 qlq - c30 and qlq - ov28 questionnaires were completed during outpatient attendances at day 1 of each chemotherapy cycle and during follow - up visits 6 - weekly until 9 months from randomisation , 3 - monthly to 2 years from randomisation , and then 6 - monthly for up to 5 years from randomisation ( figure 1 )  . 
 centres were asked to report reasons for any missing questionnaires . outcomes the trial had co - primary endpoints of progression - free survival and overall survival , which have been previously reported.4 a secondary outcome , quality of life , is reported here . 
the quality - of - life study comprised two coprimary endpoints : cross - sectional analysis of qlq - c30 global health score 9 months after randomisation and longi tudinal analysis of qlq - c30 global health score from randomisation to 9 months . 
secondary quality - oflife endpoints were defined from four clinically relevant function and symptom scores , as follows : qlq - c30 emotional function , qlq - c30 social function , qlq - c30 fatigue , and qlq - ov28 peripheral neuro pathy . 
 analyses of all other function and symptom scores up to 18 months after randomisation were treated as exploratory . vol 21 july 2020 articles immediate primary surgery 6 weekly 3 monthly 6 monthly screening surgery follow - up delayed primary surgery screening surgery screening follow - up time since randomisation chemotherapy cycle debulking surgery quality - of - life assessment figure 1 : timing of quality - of - life questionnaires statistical analysis the sample size of icon8 was determined to detect a hazard ratio of 075 in progression - free survival between groups 1 and 2 , and groups 1 and 3 , with two - sided 25% significance and 90% power . 
for quality of life , a retrospective power calculation showed that the study had 90% power to detect a difference between groups of 5 points in global quality of life using the sd observed in group 1 . 
a quality - of - life expert panel ( comprised of lh , cp , spb , and rk ) , invited by the trial management group , convened on june 9 , 2016 , to define the primary , secondary , and exploratory endpoints . we compared each weekly treatment group with the 3 - weekly group , following the main analysis of clinical endpoints ( group 2 vs group 1 , and group 3 vs group 1 )  . 
to adjust for two comparisons against the same control group , we used a two - sided significance level of p = 0025 to judge statistical significance in primary and secondary analyses . 
descriptive data are presented for all other validated subscales of the qlq - c30 and qlq - ov28 . for cross - sectional comparisons of quality - of - life outcomes at 9 months , we used analysis of covariance adjusted for baseline score , hence omitting data from the chemotherapy period . 
longitudinal analyses used all data collected from baseline to 9 months ; we estimated scores at scheduled data collection points from a mixed effects regression model with a timetreatment interaction , unstructured covariance , and patient level random effects . 
the 9 - month timepoint was chosen as it represents a period of good quality of life for most patientsfew will have had disease progression , and most will have completed treatment some months earlier . 
the co - primary endpoints of cross - sectional and longitudinal changes in global health score are complementarylongitudinal analysis compares patient experience across the whole 9 - month period and crosssectional analysis compares scores at the 9 - month timepoint . 
thus , longitudinal analysis makes better use of the data and is the preferred method , whereas crosssectional analysis provides a post - treatment snapshot . for patients who had neo - adjuvant chemotherapy and underwent delayed primary surgery , chemo therapy cycles 4 to 6 and the end of treatment visit were around 4 weeks later than equivalent visits in the immediate surgery group . 
therefore , quality - of - life data were ordered by visit number rather than date . three post - hoc analyses were done : analysis of the primary and secondary outcomes separately for immediate surgery and delayed surgery patients ( including a comparison of baseline quality of life scores ) , a comparison of peripheral neuropathy scores from selfreported quality - of - life data with neuropathy adverse event data from clinicians ( according to common terminology criteria for adverse events version 4.0 ) , 4 and analysis of self - reported peripheral neuropathy scores 18 months after randomisation . we assessed the potential effect of missing data on the co - primary outcome using imputation to model the following scenarios : scenario 1 , a global score of 0 was imputed for patients who died within 9 months of enrolment ; scenarios 24 , all patients alive and without progression at 9 months but missing quality - of - life data were assigned a score , starting respectively with the mean 9 - month score , then the mean score minus 10 points , then mean minus 20 ; scenario 5 , a global score of 0 was imputed for patients who died within 9 months , all other patients ( including those with disease progression ) with a baseline global quality - of - life score but 972 vol 21 july 2020 articles missing their 9 - month global quality - of - life score were assigned the mean 9 - month score . 
the rationale for scenarios 24 was that patients might have missed submitting their questionnaires due to illness , in which case a lower quality of life would be expected . all analyses were done on an intention - to - treat basis with stata version 15.0. 
the trial is registered on clinicaltrials.gov , nct01654146 and isrctn registry , isrctn10356387 . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the trial management group had final responsibility for the decision to submit for publication . results between june 6 , 2011 , and nov 28 , 2014 , 1566 patients were recruited into icon8 ( 522 were included in group 1 , 523 in group 2 , and 521 in group 3 )  . 
baseline characteristics are described elsewhere.4 all patients were invited to partici pate in the quality - of - life study , and 1540 patients com pleted 17 515 quality - of - life questionnaires . 
9 months after randomisation , quality - of - life data were expected from 1280 patients in follow - up without disease progression ; 39 patients had died , 230 were alive after progression , and 17 had withdrawn or been lost to follow - up without progression . 
baseline questionnaires were completed by 1438 ( 92% ) of 1566 patients and 9 - month questionnaires by 882 ( 69% ) of 1280 patients ( table 1 )  . 
828 ( 65% ) of 1280 patients who could have contributed quality - of - life data at 9 months had both baseline and 9 - month data and were included in crosssectional analyses of primary and secondary outcomes . at the 9 - month timepoint we found no significant difference in qlq - c30 global health score between the three treatment groups with cross - sectional analysis ( group 2 vs group 1 , n = 555 , mean difference 23 , 95% ci 04 to 49 , p = 0094 ; group 3 vs group 1 , n = 522 , mean difference 08 , 38 to 22 ; p = 061 ; table 2 )  . 
we observed an improvement in mean global health score from baseline to 9 months post - random isation across the study population ( figure 2 ) , although a fall in global health score was observed during chemotherapy in all three treatment groups . 
with longitudinal analysis , mean global health scores across the 9 - month period were lower among patients in the weekly treatment groups , with a significant difference between group 3 and group 1 ( group 2 vs group 1 , 926 patients had global health score at baseline , and at least one score between baseline and 9 months , mean difference 18 , 95% ci 36 to 01 , p = 0043 ; group 3 vs group 1 , n = 915 patients had global health score at baseline , and at least one score between baseline and 9 months , mean difference 29 , 47 to 11 ; p = 00018 ; table 2 )  . 
 we found no difference in social functioning ( qlq - c30 ) between treatment groups using either cross - sectional or longitudinal analyses ( table 3 ; figure 2 )  . 
we observed no difference in fatigue ( qlq - c30 ) between groups by cross - sectional analysis ; although fatigue scores were significantly different between the weekly ( group 2 ) and 3 - weekly ( group 1 ) treatment groups by longitudinal analysis , they did not meet the threshold for clinical signifi cance ( table 3 ; figure 2 )  . 
by cross - sectional analysis , peripheral neuropathy scores ( qlq - ov28 ) were statisti cally and clinically significantly different between group 2 and group 1 ; however , there was no difference by longitudinal analysis ( table 3 ; figure 2 )  . 
 vol 21 july 2020 articles global health score emotional function group 1 group 1 group 2 group 2 group 3 group 3 social function fatigue symptoms peripheral neuropathy symptoms baseline cycle 6 time 9 months baseline cycle 6 time 9 months figure 2 : primary and secondary quality - of - life endpoints for global health status and function scales ( qlq - c30 global health status , emotional function , and social function ) , higher scores indicate better function ( improved quality of life ) but for symptom scales ( qlq - c30 fatigue and qlq - ov28 peripheral neuropathy ) , higher scores indicate greater symptoms ( poorer quality of life )  . 
the number of expected questionnaires and received questionnaires is reported in the appendix ( p 5 )  . the timing of neuropathy differed between groups ( figure 2 )  . exploratory cross - sectional analyses of the other qlq - c30 and qlq - ov28 subscales showed that differences between the three randomised groups were generally small ( appendix pp 56 )  . 
we did not analyse data on sexual function since more than 80% of patients reported that they were sexually inactive at baseline . a post - hoc analysis of peripheral neuropathy scores showed that , for patients who remained in follow - up without progression , high scores were still observed 18 months after randomisation for all treatment groups ( appendix p 7 )  . 
there was a statistically and clinically significant difference between group 2 and group 1 ( n = 298 with neuropathy score at baseline and 18 months , mean difference 107 , 95% ci 42 to 172 ; p = 00012 ) but not group 3 and group 1 ( n = 316 patients in group 1 or group 3 with neuropathy score at baseline and 18 months , 48 , 09 to 104 ; p = 0096 ) by cross - sectional analysis . 
 longi tudinal analysis did not show significant differences between the groups ( group 2 vs group 1 , n = 898 patients with neuropathy score at baseline and at least one neuropathy score between baseline and 18 months , mean difference 25 , 95% ci 12 to 61 , p = 018 ; group 3 vs group 1 , n = 901 patients with neuropathy score at baseline and at least one neuropathy score between baseline and 18 months , 25 , 12 to 61 , p = 019 )  . post - hoc analyses were done to investigate differences in quality of life related to timing of surgery ( immediate primary surgery vs delayed primary surgery ; appendix pp 810 )  . 
qlq - c30 global health score at baseline was significantly lower among patients who had delayed surgery ( n = 714 ) than those who had immediate surgery ( n = 675 ) ( mean 562 [ sd 243 ] vs [ 216 ] ; p < 00001 )  . 
baseline emotional mean 617 function ( delayed surgery , n = 716 , mean 686 [ sd 236 ] ; immediate surgery , n = 673 , mean 736 [ 215 ] ; p < 00001 ) and fatigue ( delayed surgery , n = 720 , mean 423 [ sd 270 ] ; immediate surgery , n = 679 , mean 358 [ 229 ] ; p < 00001 ) were also significantly worse among patients who had delayed surgery , but we observed no difference in baseline scores for social function or peripheral neuropathy between patients with different surgery timings ( data not shown )  . 
for patients who had immediate surgery , longi tudinal analysis of the global health score over 9 months mirrored that in the overall study population ( appendix pp 810 )  . 
however , among patients the difference between who had delayed surgery treatment groups was smaller than it was in the overall study population ( appendix pp 810 )  . we did a post - hoc analysis to assess concordance between self - reported peripheral neuropathy from the quality - of - life questionnaires and clinician - assessed peripheral neuropathy reported during the treatment period ; there was good agreement between the measures ( appendix p 12 )  . 
sensitivity analyses to assess the potential effect of missing data did not alter our interpretation of the data ( appendix p 13 )  . discussion the primary outcome of this study showed no difference between treatment groups in global health score at 9 months compared with baseline . 
however , longitudinal analysis revealed lower global health scores during chemotherapy for those in the weekly treatment groups than for those in the 3 - weekly treatment group , which , although statistically significant , was of marginal clinical significance . 
these findings indicate that patients receiving weekly paclitaxel - containing chemotherapy had slower improvement in their overall quality of life during treatment itself , but recovered to a similar level to those receiving 3 - weekly treatment at 9 months . 
other 974 vol 21 july 2020 articles secondary outcomes revealed slightly worse fatigue and more persistent peripheral neuropathy in the weekly paclitaxel - containing groups than in the 3 - weekly group , although other quality - of - life subscores were similar between the study groups . 
patients in the 3 - weekly treatment group had an earlier onset of , but more rapid improvement in , peripheral neuropathy symptoms after completion of chemotherapy than did patients in the weekly treatment groups . 
by contrast , symptoms of peripheral neuropathy developed more gradually for patients in the weekly treatment groups compared with the 3 - weekly treatment group but persisted beyond the end of treatment and into the follow - up period . the observed differences in these quality - of - life subscores are probably due to paclitaxel exposure . 
as with the jgog - 3016 and gog - 0262 studies , 11 , 12 patients in group 2 and group 3 of icon8 received up to 80 mg / m of paclitaxel per week , equivalent to 240 mg / m per cycle . 
by contrast , in the mito - 7 study , 13 a lower weekly dose of 60 mg / m paclitaxel was administered in the weekly group ( equivalent to 180 mg / m per cycle ) and lower neuropathy scores were reported in the weekly group compared to those in the 3 - weekly group ( who received a similar per cycle dose of paclitaxel ; appendix p 14 )  . 
these findings suggest that peripheral neuropathy could be caused by cumulative exposure to paclitaxel rather than dosing intensity , although the exact mechanism of taxane neurotoxicity remains incompletely understood . the large size of icon8 allowed comparison between the quality - of - life trajectories of patients who had immediate primary surgery and delayed primary surgery . 
 as the choice of upfront or delayed surgery was not randomly assigned , patients with more advanced - stage disease and poorer perfor mance status were selected for upfront chemo therapy and delayed surgery , intended to reduce their anaesthetic risk and allow chemotherapy downstaging . 
overall , patients who had delayed surgery had a larger incre mental improvement in quality of life from randomisation to 9 months than did patients with immediate surgery , although having started from a lower point this result might have been expected . 
by contrast , patients who had immediate surgery entered icon8 having recovered from surgery and with better quality of life ; although they had a quality - of - life nadir following chemotherapy ( at around 18 weeks ) , their quality of life recovered to the same level as those in the delayed surgery group at 9 months . 
we recommend this close method of tracking of quality of life , along with longitudinal rather than vol 21 july 2020 articles cross - sectional methods of analysis , to more accurately reflect changes over time . 
alternatively , standardised , continuous patient - reported outcome measures can be implemented to provide more reliable monitoring of the longer - term toxicities that affect patient wellbeing.12 because of the differences between non - randomised patients undergoing immediate or delayed surgery , we recommend that these two surgical groups are analysed separately in future quality - of - life studies . to our knowledge , icon8 provides the largest and most detailed quality - of - life dataset of any neoadjuvant ovarian cancer trial . 
a limitation of the study is the loss of qualityof - life data due to patients who did not complete or return their questionnaires , which poten tially introduced bias against those with more severe symptoms who might have been less able or willing to comply . 
questionnaire compliance was favourable compared with other similar studies ; baseline quality - of - life questionnaires were completed by 92% of patients in icon8 compared with 639% and 75% in the jgog - 3016 and mito - 7 studies , respectively . 
additionally , response shift is a limitation of quality - of - life studies , whereby patients adapt to and therefore underreport symptoms over time.14 as the main icon8 study revealed no progression - free survival advantage for weekly paclitaxel - containing regimens , our quality - of - life data do not support its use in favour of standard 3 - weekly carboplatin and paclitaxel after upfront surgery in ovarian cancer . 
however , our finding of no quality of life detriment between the groups among patients who had delayed surgery suggests that , in those unsuitable for upfront surgery , 3 - weekly and weekly schedules might be equivocal . 
in patients who have delayed surgery , who are likely to be in poorer health , the weekly scheduling of both carboplatin and paclitaxel allows more careful dosing modulation and symptom management than 3 - weekly dosing , and is equivalent to 3 - weekly dosing in terms of its effect on global quality of life . in conclusion , for patients undergoing upfront surgery , weekly paclitaxel - containing chemotherapy should not replace 3 - weekly carboplatin and paclitaxel as the standard of care for newly diagnosed ovarian cancer , since it neither improves progression - free survival nor is associated with improved quality of life . contributors spb , adc , ecj , cp , lh , and rk coordinated this study . 
spb and adc drafted the manuscript , the final version of which was approved by all coauthors . declaration of interests cp reports personal fees and non - financial support from pfizer , roche , genomic health , tesaro , and puma biotechnology , outside the submitted work . 
jal reports grants and personal fees from astrazeneca and merck sharp & dohme and personal fees from roche , clovis oncology , pfizer , and tesaro , outside the submitted work . 
arc reports grants from cancer research uk during the conduct of the study , grants , personal fees , and non - financial support from astrazeneca , non - financial support from clovis oncology , and personal fees from roche , outside the submitted work . 
all other authors declare no competing interests . data sharing data will be shared according to the medical research council clinical trial unit controlled access approach , based on the following principles : no data should be released that would compromise an ongoing trial or study ; there must be a strong scientific or other legitimate rationale for the data to be used for the requested purpose ; investigators who have invested time and effort into developing a trial or study should have a period of exclusivity in which to pursue their aims with the data , before key trial data are made available to other researchers ; the resources required to process requests should not be underestimated , particularly successful requests that lead to preparing data for release , therefore , adequate resources must be available to comply in a timely manner or at all , and the scientific aims of the study must justify the use of such resources ; and data exchange complies with information governance and data security policies in all of the relevant countries . 
we acknowledge experimental cancer medicines centres and national institute for health research biomedical research centre for support at icon8 uk centres . corrections correction to lancet oncol 2015 ; 16 : 522 correction to lancet oncol 2016 ; 17 : 553 correction to lancet oncol 2016 ; 17 : 733 philip , pa . 
 this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . eggermont amm , chiarion - sileni v , grob j - j , et al . 
this correction has been made to the online version as of june 1 , 2016 . correction to lancet oncol 2016 ; 17 : 751 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . vol 17 june 2016 e223 correction to lancet oncol 2020 ; 21 : 64554 correction to lancet oncol 2020 ; 21 : 144354 correction to lancet oncol 2020 ; 21 : e51927 smith i , robertson j , kilburn l , et al . 
 long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial . 
lancet oncol 2020 ; 21 : e51927in this review , the second sentence of the first paragraph of the section entitled cancer burden now describing the number of new cancer cases worldwide in 2017 should read according to analysis from the global burden of disease study , there were 168 million new cases of cancer . 
this correction has been made to the online version as of nov 30 , 2020 . correction to lancet oncol 2020 ; 21 : 156373 powles t , plimack er , soulires d , et al . 
pembrolizumab plus axitinib versus sunitinib monotherapy as firstline treatment of advanced renal cell carcinoma ( keynote - 426 ) : extended follow - up from a randomised , openlabel , phase 3 trial . 
lancet oncol 2020 ; 21 : 156373in table 1 of this article the n ( % ) for previous nephrectomy should read 357 ( 83% ) for the pembrolizumab plus axitinib group and 358 ( 83% ) for the sunitinib group . 
these corrections have been made to the online version as of nov 30 , 2020 , and the printed version is correct . correction to lancet oncol 2020 ; 21 : e30516 fangusaro j , witt o , herniz driever p , et al . 
these corrections have been made to the online version as of nov 30 , 2020 . vol 21 december 2020 e553 corrections correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2019 ; 20 : 137085 correction to lancet oncol 2020 ; 21 : 137886 glynne - jones r , sebag - montefiore d , meadows hm , et al . 
lancet oncol 2017 ; 18 : 34756the last clause of the last sentence of the first paragraph of the introduction of this article should have read or by giving maintenance chemotherapy after chemoradiotherapy.7 this correction has been made to the online version as of nov 2 , 2020 . motzer rj , rini bi , mcdermott df , et al , on behalf of the checkmate 214 investigators . 
nivolumab plus ipilimumab versus sunitinib in firstline treatment for advanced renal cell carcinoma : extended follow - up of efficacy and safety results from a randomised , controlled , phase 3 trial . 
 lancet oncol 2019 ; 20 : 137085 in this article , supplementary table 1 in the appendix has been updated to correct international metastatic renal cell carcinoma database consortium risk percentage values in patients in the intention to treat group . 
lancet oncol 2020 ; 21 : 137886in table 2 of this article , the reference value for absolute risk reduction of incident gastric cancer over 10 years in indi viduals with an unfavourable life style should have been 0 for low genetic risk , intermediate genetic risk , and high genetic risk . 
these corrections have been made to the online version as of nov 2 , 2020 . vol 21 november 2020 e518 corrections correction to lancet oncol 2016 ; 17 : 74756 correction to lancet oncol 2018 ; 19 : 153042 correction to lancet oncol 2019 ; 20 : 81626 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
lancet oncol 2016 ; 17 : 74756in results , median overall survival should have been median time of death ( after randomisation ) in eleven patients who died from progressive disease . 
prognostic value of end - of - induction pet response after first - line immunochemotherapy for ( gallium ) : follicular secondary analysis of a randomised , phase 3 trial . 
 lancet oncol 2019 ; 20 : 81626 the appendix of this article has been updated as of may 10 , 2019 . published online april 29 , 2019 s1470 - 2045 ( 19 ) 30280 - 3 published online may 10 , 2019 s1470 - 2045 ( 19 ) 30292 - x published online may 10 , 2019 s1470 - 2045 ( 19 ) 30293 - 1 correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
this correction has been made to the online version as of may 29 , 2019 . correction to lancet oncol 2019 ; 20 : 82736 shitara k , iwata h , takahashi s , et al . 
lancet oncol 2019 ; 20 : 82736the appendix of this article has been updated as of may 10 , 2019 . correction to lancet oncol 2019 ; 20 : 84961 eng c , kim tw , bendell j , et al . 
 atezolizumab with or without cobimetinib versus regorafenib previously treated metastatic colorectal cancer ( imblaze370 ) : a multicentre , open - label , phase 3 , randomised , controlled trial . 
this correction has been made to the online version as of may 29 , 2019 and the printed article is correct . correction to lancet oncol 2019 ; 20 : e26273 ngiam ky , khor iw . 
lancet oncol 2019 ; 20 : e26273tables 1 and 2 in this article have been corrected as of april 29 , 2019 . correction to lancet oncol 2019 ; 20 : 297310 cella d , grnwald v , escudier b , et al . 
this update has been made online as of may 29 , 2019 . vol 20 june 2019 e293 corrections correction to lancet oncol 2020 ; 21 : 101718 correction to lancet oncol 2020 ; 21 : 93546 correction to lancet oncol 2020 ; 21 : 112526 iarc monographs vol 127 group . 
lancet oncol 2020 ; 21 : 101718in this news piece , the web links in the margin for the preamble to the iarc monographs and for the iarc declarations of interest were incorrect and have been amended . 
 lancet oncol 2020 ; 21 : 112526in this comment , the fourth paragraph should read one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
because overdiagnosis appears to increase with age , it is possible that overdiagnosis occurred in both groups after the age of 50 years , but could not be detected because of the design of the trial . 
 this correction has been made as of sept 1 , 2020 , and the printed version is correct . vol 21 september 2020 e418 corrections correction to lancet oncol 2014 ; 15 : 150312 correction to lancet oncol 2019 ; 20 : 76980 correction to lancet oncol 2019 ; 20 : 98699 open - label phase 1 / 2 jg , niesvizky r , kumar sk , berdeja et al . 
 lancet oncol 2014 ; 15 : 150312in the eighth paragraph of the results section of this article , the first sentence should have been overall responses were noted in 59 ( 92% , 95% ci 8397 ) of 64 patients ( table 5 )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 765 ben - aharon i , goshen - lago t , fontana e , et al . 
this correction has been made to the online version as of july 1 , 2019 . 2018 jacob s , yap ml , wilson be , ferlay j , bray f , barton mb . 
 lancet oncol 2019 ; 20 : 76980 in the affiliations for this article , dr mei ling yap should have been affiliated with the university of new south wales ( sydney , nsw , australia )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 795805 randomised , controlled hofvind s , holen s , aase hs , et al . 
 lancet oncol 2019 ; 20 : 795805 in figure 1 , the number of patients with screen - detected breast cancer in the digital breast tomosynthesis group should have read 95 , and the number of patients in the digital mammography group should have read 87 . 
 quizartinib versus salvage chemotherapy in relapsed or refractory flt3 - itd acute myeloid leukaemia ( quantum - r ) : a multicentre , randomised , controlled , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 98699in this article , the second sentence in the statistical analysis section should have read the sample size calculation wording in the original protocol specified a 5% , two - sided calculation ; however , this wording was inaccurate , and subsequently , a one - sided calculation at 25% was implemented to solely test for superiority of quizartinib , which is consistent with the primary aim of the study . 
this correction has been made to the online version as of july 1 , 2019 , and the printed article is correct . correction to lancet oncol 2019 ; 20 : e30212 hillengass j , usmani s , rajkumar sv , et al . 
these corrections have been made to the online version as of july 1 , 2019 . vol 20 july 2019 e346 corrections the real worth of cancer drugs launched in november , 2020 , we witnessed one of the most awaited elections in recent timesthe usa elected joe biden as its new president , and with this decision comes renewed hope for science . 
for oncology , we wait in anticipation to see whether the cancer moonshot programme , in 2016 under the obama administration and overseen by then vice - president biden , will be rebooted . 
at the time , congress had authorised us $18 billion in funding for cancer research over a 7 - year timeframe , which expires in 2022 , making next years budget review crucial . 
given bidens support in 2017 for our commission on future cancer research priorities in the usa , we are hopeful that these recommendations will be reprioritised . one of the aims of the cancer moonshot was to provide more treatment options by accelerating cancer research . 
 approval of new drugs , their cost to health systems and patients , and the amount of out - of - pocket expenses versus their efficacy is a long - running and contentious issue . 
a new study , however , has shown that novel drugs approved between 2000 and 2016 to treat the 15 most common cancers prevented 12 million deaths in the usa . 
these results highlight the importance of investing in new cancer treatments and how scientific advancements can pay off on a cumulative basis , even if some drugs provide only small incremental benefits over their predecessors . profit remains a crucial driver of oncology drug development worldwide . 
although the global oncology market is expected to contract by 11% in 2020 compared with 2019 due to covid - 19 - related pauses in drug manufacturing and clinical trials , it is still one of the biggest health - care markets worldwide . 
for example , astrazeneca has projected a 55% increase in thirdquarter earnings this yearmainly due to increased sales of cancer drugs rather than investments related to its vaccine for covid - 19 . 
pharmaceutical companies naturally expect large returns on investment , but a compromise must be reached for fair pricing to ensure all patients with cancer have access to life - saving treatments . 
if ethics is not reason enough to support this notion , recently , it has been shown that us states that expanded medicaid coverage as part of the affordable care act saw significant reductions in mortality in patients with some newly diagnosed cancers compared with that in non - expansion states . 
these results add to the evidence that access to effective cancer drugs can yield long - term benefits to public health . several strategies have been proposed to provide a way to approve drugs based on a more equitable compromise between profits for pharmaceutical companies and afford ability for public and private health insurers , which is a global issue not specific to the usa . 
this year , in a push to expedite access to new cancer drugs in the uk , the institute of cancer research ( icr ) published a consensus statement with suggestions on how to bridge the gap between drug price and patient access . 
although survival outcome - based pricing is also proposed by the american society of clinical oncology and the european society for medical oncology , the icr consensus proposes the use of surrogate endpoints instead of survival to help accelerate drug approvals . 
moreover , the underlying principle behind some of the recommendations is that governments and the pharmaceutical industry must work closely together from the point of drug discovery , and not only when new treatments need approval and market licensing . 
this strategy would allow alignment of interestsincluding funding and regulationsof both parties , which should prioritise patients interests and needs . president - elect biden symbolises a new hope for science - based political decisions and , importantly , the reinstatement of international collaboration , including for previous international funding commitments and re - engagement with who . 
we hope to see data - driven decision - making and consensus on fair drug prices that will help overcome the long - term consequences of public health and financial crises . 
in this fight , public and private parties must not be on opposite sides of the barricade , rather they must work together to achieve the best outcomes for patients with cancer . 
 the lancet oncology for more on the cancer moonshot initiative see initiatives / moonshot - cancerinitiative for the lancet oncology commission see thelancet.com / commissions / usa - oncology for more on improved outcomes due to novel cancer drugs see j med econ 2020 ; published online nov 9 . 
 the approval of gemcitabine for locally advanced or metastatic pancreatic cancer brought a much needed increase in 5 - year overall survival , but since then , the past 20 years have failed to yield new advances , despite e cacy of many other novel agents in other di cult - to - treat cancers , such as metastatic melanoma and non - small - cell lung cancer . japan , reported however , in june , 2016 , a phase 3 , randomised non - inferiority trial comparing adjuvant gemcitabine with s - 1 , a uoropyrimidine used almost exclusively in patients with advancedstage disease , a 5 - year overall survival of 24% with gemcitabine compared with a remarkable 44% with s - 1 . 
although the unique attributes of s - 1 , the patients , and japanese health systems might have contributed to this result , and its applicability to patients of other ethnicities remains to be assessed , this nding suggests that opportunities exist to tackle pancreatic cancer more e ectively . 
similarly , the european espac - 4 trial , reported at the american society for clinical oncology ( june 37 ; chicago , il , usa ) , compared gemcitabine plus capecitabine with gemcitabine alone after resection , and showed improved 5 - year overall this combination also survival ( 29% vs 16% )  . 
in an attempt to overcome this barrier , a phase 1b trial reported in may , 2016 , assessed the combination of a ccr2 inhibitor with uorouracil , leucovorin , irinotecan , and oxaliplatin in borderline resectable and advanced pancreatic cancer . 
 additionally , a study published in june , 2016 , of mice treated with gemcitabine plus cxcr2 inhibition which is thought to prevent neutrophil in ltration and promote antitumour immune activityreported that mice with pancreatic adenocarcinoma had an increased survival and experienced large numbers of tumour - in ltrating t - cells . 
 although preliminary , these ndings highlight the intriguing possibility that pancreatic cancer could immunotherapybut a greater be sensitised to understanding of both tumour biology and its interaction with the immune system is needed to capitalise on this potential . while it is crucial not to overstate the recent gains made in understanding and treating pancreatic cancer , we encourage researchers and clinicians to continue pursuing traditional and novel lines of investigation for this deadly disease . 
 the lancet oncology vol 17 july 2016 correction to lancet oncol 2020 ; 21 : e57588 correction to lancet oncol 2021 ; 22 : 2942 correction to lancet oncol 2021 ; 22 : 8597 bahadoer rr , dijkstra ea , van etten b , et al . 
short - course radiotherapy followed by chemotherapy before total mesorectal excision ( tme ) versus preoperative chemoradiotherapy , tme , and optional adjuvant chemotherapy locally advanced rectal cancer ( rapido ) : a randomised , open - label , phase 3 trial . 
 lancet oncol 2021 ; 22 : 2942in figure 1 in this article , in the standard of care group , of the 187 patients who had adjuvant chemotherapy , 185 should have been indicated as having this chemotherapy according to hospital policy . 
fixeddose combination of pertuzumab and trastuzumab for subcutaneous injection plus chemotherapy in her2 - positive early breast cancer ( federica ) : a randomised , open - label , multicentre , non - inferiority , phase 3 study . 
lancet oncol 2021 ; 22 : 8597in table 2 of this article , the cycle 7 ( predose cycle 8 ) pertuzumab serum geometric mean auc 021 days ( percentage cv ) , g / ml per day should have been 2440 ( 242 ) for the intravenous infusion group and 2440 ( 262 ) for the fixed - dose combination group , and the cycle 7 ( predose cycle 8 ) trastuzumab serum geometric mean ( percentage cv ) , auc 021 days g / ml per day should have been 1640 ( 240 ) for the intravenous infusion group and 1700 ( 289 ) for the fixed - dose combination group . 
intermittent schedules of the oral rafmek inhibitor ch5126766 / vs - 6766 in patients with ras / raf - mutant solid tumours and multiple myeloma : a single - centre , open - label , phase 1 dose - escalation and basket dose - expansion study . 
also , sentence two of paragraph four of the discussion should have read these tumours harboured a range of ras and raf mutations , including kras gly12asp , kras gly12val , kras gly12arg , brafve , and hras gly13arg . 
we updated the analysis to investigate patterns of recurrence and did a post - hoc survival analysis . methods in the multicentre randomised phase 3 portec - 3 trial , women with high - risk endometrial cancer were eligible if they had international federation of gynaecology and obstetrics ( figo ) 2009 stage i , endometrioid grade 3 cancer with deep myometrial invasion or lymphovascular space invasion , or both ; stage ii or iii disease ; or stage iiii disease with serous or clear cell histology ; were aged 18 years and older ; and had a who performance status of 02 . 
 participants were randomly assigned ( 1 : 1 ) to receive radiotherapy alone ( 486 gy in 18 gy fractions given on 5 days per week ) or chemoradiotherapy ( two cycles of cisplatin 50 mg / m given intravenously during radiotherapy , followed by four cycles of carboplatin auc5 and paclitaxel 175 mg / m given intravenously ) , by use of a biased coin minimisation procedure with stratification for participating centre , lymphadenectomy , stage , and histological type . 
at a median follow - up of 726 months ( iqr 599856 ) , 5 - year overall survival was 814% ( 95% ci 772858 ) with chemoradiotherapy versus 761% ( 716809 ) with radiotherapy alone ( adjusted hazard ratio [ hr ] 070 [ 95% ci 051097 ] , p = 0034 ) , and 5 - year failure - free survival was 765% ( 95% ci 715807 ) versus 691% ( 638738 ; hr 070 [ 052094 ] , p = 0016 )  . 
distant metastases were the first site of recurrence in most patients with a relapse , occurring in 78 of 330 women ( 5 - year probability 214% ; 95% ci 173263 ) in the chemoradiotherapy group versus 98 of 330 ( 5 - year probability 291% ; 244343 ) in the radiotherapy - alone group ( hr 074 [ 95% ci 055099 ] ; p = 0047 )  . 
isolated vaginal recurrence was the first site of recurrence in one patient ( 03% ; 95% ci 0021 ) in both groups ( hr 099 [ 95% ci 0061590 ] ; p = 099 ) , and isolated pelvic recurrence was the first site of recurrence in three women ( 09% [ 95% ci 0328 ] ) in the chemoradiotherapy group versus four ( 09% [ 95% ci 0328 ] ) in the radiotherapy - alone group ( hr 075 [ 95% ci 017333 ] ; p = 071 )  . 
at 5 years , reported grade 3 adverse events did not differ significantly between the two groups , occurring in 16 ( 8% ) of 201 women in the chemoradiotherapy group versus ten ( 5% ) of 187 in the radiotherapy - alone group ( p = 024 )  . 
at 5 years , grade 2 or worse adverse events were reported in 76 ( 38% ) of 201 women in the chemoradiotherapy group versus 43 ( 23% ) of 187 in the radiotherapy - alone group ( p = 0002 )  . 
 sensory neuropathy persisted more often after chemoradiotherapy than after radiotherapy alone , with 5 - year rates of grade 2 or worse neuropathy of 6% ( 13 of 201 women ) versus 0% ( 0 of 187 )  . 
this treatment schedule should be discussed and recommended , vol 20 september 2019 lancet oncol 2019 ; 20 : 127385 published online july 22 , 2019 s1470 - 2045 ( 19 ) 30395 - x this online publication has been corrected . 
follow - up is ongoing to evaluate long - term survival . funding dutch cancer society , cancer research uk , national health and medical research council , project grant , cancer australia grant , italian medicines agency , and the canadian cancer society research institute . copyright 2019 the author ( s )  . 
findings of clinical trials comparing adjuvant chemotherapy alone with external - beam radiotherapy alone have shown no differ ences in survival outcomes.5 , 6 because a higher incidence of pelvic relapses has been reported with chemotherapy alone compared with a treatment schedule including external - beam radiotherapy , 7 , 8 the combi nation of external - beam radiotherapy with chemo therapy has been explored in clinical trials . research in context evidence before this study we searched pubmed for clinical studies published in english between jan 1 , 1980 , and dec 31 , 2006 , with the terms endometrial cancer and radiation therapy and chemotherapy and survival or failure free survival and with the terms endometrial cancer and serous and radiation therapy and chemotherapy and survival or failure free survival . 
since the start of recruitment to the portec - 3 trial in 2006 , the results of a pooled analysis of the nsgo - ec - 9501 / eortc - 55991 trial and the mango iliade - iii trial were published , showing a significant improvement in progression - free survival and non - significant improvement in overall survival in women treated with four cycles of platinum - based chemotherapy given sequentially before or after pelvic radiotherapy versus those treated with radiotherapy alone . 
the gog - 249 trial did not show improved progression - free survival with three cycles of carboplatinpaclitaxel with vaginal brachytherapy compared with pelvic radiotherapy in women with stage iii disease with high ( intermediate ) risk factors . 
in the gog - 258 trial , women with stage iiiiv endometrial cancer were randomly assigned to receive chemoradiotherapy ( the same schedule as that used in the portec - 3 trial ) or six cycles of carboplatinpaclitaxel alone . 
 no differences in overall or recurrence - free survival were reported , but significantly more vaginal and pelvic or para - aortic recurrences were reported in the chemotherapy group than in the chemoradiotherapy group . 
 the nsgo / eortc trial reported improved progression - free survival with the addition of chemotherapy to radiotherapy for endometrioid cancers , but no such benefit was found for serous cancers . added value of this study we report on the patterns of recurrence and provide updated survival outcomes of patients with high - risk endometrial cancer treated in the international randomised phase 3 portec - 3 trial . 
 patients were randomly assigned to receive pelvic radiotherapy alone or the combination of radiotherapy with concurrent ( two cycles of cisplatin ) and adjuvant ( four cycles of carboplatinpaclitaxel ) chemotherapy . 
pelvic control was excellent in both groups . implications of all the available evidence combined adjuvant chemotherapy and radiotherapy should be discussed and recommended as a new standard of care , especially for women with stage iii endometrial cancer or serous cancers , or both . 
 previously reported efficacy results with a time - based analysis and a median follow - up of 602 months ( iqr 481731 ) showed a significant 7% improvement in failure - free survival for patients treated with chemo radiotherapy compared with those treated with radio therapy alone ( 76% vs 69% at 5 years ) without a significant difference in overall survival ( 82% vs 77% at 5 years ) .9 in a subgroup analysis , the largest failure - free survival benefit with chemoradiotherapy ( 11% ; 69% vs 58% at 5 years ) was observed in women with stage iii disease , who have a higher baseline risk of recurrence than women with stage iii disease . the aim of the present analysis of the portec - 3 trial is to present the patterns of recurrence , treatment , and survival after recurrence and an updated ( post - hoc ) analysis of the primary endpoints with prolonged follow - up . methods study design and participants portec - 3 was an open - label , multicentre , randomised intergroup phase 3 trial led by the dutch gynaecological oncology group ( dgog )  . 
the trial was done at 103 centres ( oncology centres , university hospitals , regional hospitals , or radiation oncology centres with referrals from regional hospitals ) in six clinical trial groups collaborating in the gynaecological cancer intergroup . 
participating groups were the national cancer research institute ( ncri ; uk ) , the australia and new zealand gynaecologic oncology group ( anzgog ; australia and new zealand ) , the mario negri gynaecologic oncology group ( mango ; italy ) , the canadian cancer trials group ( canadian cancer trials group ; canada ) , and fedegyn ( france )  . details about patient selection and treatment have been published previously.9 , 10 all patients first underwent surgery . 
the extent of lymph node removal was left to the discretion of the participating centres , although pelvic lymph node debulking and para - aortic lymph node sampling were recommended in case of macroscopic positive pelvic nodes or para - aortic nodes , or both . 
central pathology review was mandatory before randomisation to confirm eligibility for study entry.11 eligible patients were women with histologically confirmed endometrioid endometrial cancer with either international federation of gynecology and obstetrics ( figo ) 2009 stage ia grade 3 with documented lymphovascular space invasion ; stage ib grade 3 disease ; stage ii disease ; stage iiia , iiib ( parametrial invasion ) , or iiic disease ; or stage iaiii with serous or clear cell histology ( ia with invasion )  . 
eligibility criteria also included who performance score 02 ; adequate bone marrow function ( white blood cell count 30 10 cells per l , platelets 100 10 per l ) , liver function ( bilirubin 15 upper limit of normal , aspartate aminotransferase to alanine aminotransferase ratio 25 upper limit of normal ) and kidney function ( creatinine clearance > 60 ml / min calculated according to cockroft and gault or > 50 ml / min edetic acid [ edta ] clearance ) , and age 18 years or older ( without an upper age limit , because elderly women might benefit from the study treatment if they were deemed fit enough to undergo chemotherapy )  . 
exclusion criteria were uterine sarcoma or carcino sarcoma , previous malignancy ( except for nonmelanomatous skin cancer ) within the past 10 years , previous pelvic radiotherapy , previous hormonal therapy or chemotherapy , bulky cervical involvement with radical hysterectomy , inflammatory bowel disease , residual macro scopic tumour , impaired renal or cardiac function , neuropathy grade 2 or worse , hearing impairment grade 3 or worse , or a congenital hearing disorder . written informed consent was obtained from all patients . 
participants , physicians , and investigators were not masked to treatment allocation . procedures external - beam pelvic radiotherapy was given to patients in both treatment groups to a total dose of 486 gy in 18 gy fractions , 5 days per week . 
brachytherapy dose was equivalent to 14 gy in 2 gy fractions ( with a recommended scheme of 10 gy high - dose rate in fractions of 5 gy )  . 
overall radiotherapy treatment time was not to exceed 50 days . in the chemoradiotherapy group , women received two cycles of cisplatin 50 mg / m administered intravenously in the first and fourth week of external - beam radiotherapy , followed by four cycles of carboplatin auc5 and paclitaxel 175 mg / m administered intravenously at 21 - day intervals . 
cisplatin was postponed for 1 week in the event of haematological , renal , or other toxicities or discontinued if recovery required more than 1 week or in the case of grade 2 or worse neuropathy . 
details about chemotherapy stopping rules have been described previously.10 follow - up was focused on patient history and pelvic ( grade 2 to detect adverse events examination according to common terminology criteria for adverse events [ ctcae ] version 3.0 ) and symptoms of recurrent disease , with annual chest radiographs , blood counts , and chemistry tests ( including ca - 125 ) until 5 years after randomisation . 
healthrelated quality - of - life assessments were done at baseline , at the end of radiotherapy , at 6 - month intervals from randomisation until 24 months , and at 36 and 60 months . patients who immediately withdrew informed consent after randomisation without any information were excluded from the analysis , as were patients who were ineligible for the study . 
there were no other criteria for a patient to be removed from the study . 686 patients enrolled and randomly assigned 343 assigned to radiotherapy 343 assigned to chemoradiotherapy 13 excluded 4 immediately withdrew informed consent 9 not eligible 13 excluded 9 immediately withdrew informed consent 4 not eligible 330 received treatment and included in intention - to - treat population 328 received allocated treatment 2 received chemoradiotherapy 330 received treatment and included in intention - to - treat population 325 received allocated treatment 5 received radiotherapy only figure 1 : trial profile 1276 the outcomes the co - primary endpoints were overall survival and failure - free survival . 
secondary endpoints were vaginal , pelvic , or distant recurrence ; treatment - related toxicity ; and health - related quality of life.10 recurrences were analysed according to first site of recurrence as well as the total number of recurrences . 
an extensive update on quality of life will be reported separately in a future publication . statistical analysis the portec - 3 trial was powered ( 80% ) to detect a 10% difference in 5 - year overall survival between the treatment groups ( increase from 65% to 75% ; hazard ratio [ hr ] 067 ) , with a two - sided test at an level of 005 . 
the final analysis of the co - primary endpoints was published in february , 2018 , with permission of the data and safety monitoring board as a time - based analysis rather than an event - based analysis since a median follow - up of 602 months had been reached and because the event rate was lower than expected . to maintain an overall of 005 with a nominal level for the interim analysis of 00002 , the final analysis was done with a nominal of 00498 . 
the final time - based analysis was done with a correlation of 07859 between the test statistics of the coprimary endpoints overall survival and failure - free survival ( based on 136 overall survival events and 186 failure - free survival events ) , and a nominal of 00309 was used for each of the analyses , resulting in an overall level of 00498.13 the sequential rejection principle14 implies that if the null hypothesis of no treatment difference the co - primary endpoints is rejected ( p < 00309 ) , the null hypothesis of no treatment difference for the other co - primary endpoint can then be assessed at the 005 level , while still retaining a family - wise error rate of 005 . for one of the current analysis was done to evaluate patterns of recurrences , together with a non - prespecified post - hoc vol 20 september 2019 articles analysis of survival after recurrence as well as an updated analysis of overall survival and failure - free survival with prolonged follow - up and 5 - year adverse events . 
the analysis of the primary endpoints was adjusted for the stratification factors ( participating group , lymphaden ectomy , stage of type ) , since a stratified cancer , and histological minimisation procedure was used at randomi sation.15 , 16 for the adjusted analysis , stratification factors were included as covariates the cox model . 
the proportional hazards assumption for treatment was checked by use of schoenfeld residuals for overall survival and failure - free survival , and was not found to be violated.17 patient characteristics were compared with a test . 
endometrioid endometrial carcinoma including mixed tumours with less than 25% of serous or clear cell component . table 1 : baseline characteristics , by treatment group and by recurrence status vol 20 september 2019 1277 articles a overall survival radiotherapy chemoradiotherapy 5 - year overall survival : 814% ( chemoradiotherapy ) vs 761% ( radiotherapy ) hr 070 ( 95% ci 051097 ) ; pcoxadjusted = 0034 number at risk ( number censored ) radiotherapy chemoradiotherapy b failurefree survival 330 ( 0 ) 330 ( 0 ) 319 ( 1 ) 316 ( 0 ) 299 ( 1 ) 295 ( 1 ) 273 ( 3 ) 272 ( 7 ) 248 ( 13 ) 258 ( 19 ) 187 ( 66 ) 201 ( 69 ) 129 ( 120 ) 137 ( 130 ) 81 ( 166 ) 89 ( 177 ) 5 - year failure - free survival : 765% ( chemoradiotherapy ) vs 691% ( radiotherapy ) hr 070 ( 95% ci 052094 ) ; pcoxadjusted = 0016 number at risk ( number censored ) radiotherapy chemoradiotherapy time since randomisation ( years ) 330 ( 0 ) 330 ( 0 ) 286 ( 1 ) 304 ( 0 ) 257 ( 1 ) 275 ( 0 ) 230 ( 3 ) 256 ( 5 ) 215 ( 13 ) 237 ( 17 ) 163 ( 61 ) 182 ( 64 ) 116 ( 106 ) 120 ( 121 ) 75 ( 146 ) 78 ( 162 ) figure 2 : kaplan - meier survival curves for overall survival ( a ) and failure - free survival ( b ) in all patients hr = hazard ratio . methods were used for analysis of failure - free survival and recurrence , by calculating cumulative incidences and fine - gray regression.18 for failure - free survival , inter current death was used as a competing risk . 
the median follow - up and iqr was estimated with the reverse kaplan - meier method . together with treatment : included this study is registered with isrctn , number and clinicaltrials.gov , number isrctn14387080 , nct00411138 . role of the funding source the funders of the study had no role in study design , data collection , data interpretation , data analysis , or writing of this report . 
the central data manager ( kwv ) , the chief investigator ( clc ) , the associated investigators ( smdb and ran ) , and the trial statistician ( hp ) had full access to all the data . 
the corresponding author and chief investigator had full access to all the data in the study and had final responsibility for the decision to submit for publication . results between nov 23 , 2006 , and dec 20 , 2013 , 686 women were enrolled and randomly assigned to chemoradiotherapy ( n = 343 ) or radiotherapy ( n = 343 ) ; 26 patients were excluded after randomisation ( figure 1 ) , resulting in 660 patients intention - to - treat analysis ( 330 in each group )  . 
median follow - up was 726 months ( iqr 599856 ) at the time of the current analysis and 75% of participants had reached at least 5 years of follow - up . the patient characteristics were well balanced between the treatment groups ( table 1 )  . 
baseline characteristics of patients with and without a recurrence are given in table 1 . in 329 radiotherapy was completed ( > 99% ) of 330 women in the chemoradiotherapy group and in 325 ( 99% ) of 330 in the radiotherapy alone group . 
vaginal brachytherapy was given to 309 ( 47% ) of 660 patients : 151 ( 46% ) of 330 patients on chemoradiotherapy and 158 ( 48% ) of 330 on radiotherapy alone . 
in the chemoradiotherapy group , concurrent cis platin was completed by 304 ( 92% ) of 330 women , adjuvant carboplatin by 262 ( 79% ) , and adjuvant paclitaxel by 233 ( 71% )  . 
at least one dose reduction of cisplatin ( to 40 mg / m ) was recorded for five ( 2% ) patients , of carboplatin ( from auc5 to auc4 ) for 36 ( 11% ) patients , and of paclitaxel ( from 175 mg / m to 135 mg / m ) for 50 ( 15% ) patients . 
 chemotherapy was discontinued ( 18% ) of 330 patients : because of toxicity in 31 ( 9% ) , the patients decision in 20 ( 6% ) , disease progression in seven ( 2% ) , and for other reasons in three ( 1% ) .9 , 10 in 61 at the final database lock ( nov 29 , 2018 ) , 150 patients had died ( 65 in the chemoradiotherapy group and 85 in the radiotherapy alone group ) and 189 patients had a failure - free survival event ( 84 in the chemoradiotherapy group and 105 in the radiotherapy alone group )  . 
this number of events comprised 76% ( 150 of 198 ) of required overall survival events and 95% ( 189 of 198 ) of failure - free survival events for the final analysis . 
most deaths were 1278 vol 20 september 2019 articles related to endometrial cancer : 53 ( 82% ) of 65 in the chemoradiotherapy group versus 76 ( 89% ) of 85 in the radiotherapy group . 
among women assigned to chemoradiotherapy , other causes of death were second cancers ( in five [ 8% ] patients ) , other intercurrent disease ( in three [ 5% ] patients ) , and complications of treatment for metastatic disease ( in two [ 3% ] patients )  . 
among women assigned to radiotherapy alone , other causes of death were second cancers ( in five [ 6% ] patients ) , other intercurrent disease ( in one [ 1% ] patient ) , and complications of treatment for metastatic disease ( in one [ 1% ] patient )  . 
the cause of death was uncertain for two patients treated with chemoradiotherapy and two patients treated with radiotherapy alone ; these deaths were considered failure - free survival events since a relation to endometrial cancer or to treatment for endometrial cancer could not be excluded.9 survival adjusted estimated 5 - year overall for stratification factors was 814% ( 95% ci 772858 ) with chemoradiotherapy versus 761% ( 716809 ) with radiotherapy alone ( hr 070 [ 95% ci 051097 ] , p = 0034 )  . 
estimated 5 - year failure - free survival adjusted for stratification factors was 765% ( 95% ci 715807 ) with chemoradiotherapy versus 691% ( 638738 ) with radiotherapy alone ( hr 070 [ 95% ci 052094 ] , p = 0016 ; figure 2 )  . in our post - hoc exploratory analysis of survival outcomes by disease stage , women with stage iii disease had significantly lower overall survival and failure - free survival than women with stage iii disease , irrespective of treatment received ( appendix p 6 )  . 
in women with stage iii endometrial cancer , 5 - year overall survival was 785% ( 95% ci 722854 ) with chemoradiotherapy versus 685% ( 612767 ) with radiotherapy alone ( hr 063 [ 95% ci 041099 ] ; p = 0043 ) , and 5 - year failure - free survival was 709% ( 95% ci 629774 ) with chemo radiotherapy versus 584% ( 498660 ) with radiotherapy alone ( hr 061 [ 95% ci 042089 ] ; p = 0011 ; figure 3a , b )  . 
in the radiotherapy group , 74 ( 76% ) of these 98 recurrences were distant recurrence only ( of which 12 were isolated para - aortic nodal recurrences ) ; 20 patients had combined distant and pelvic recurrences ( including two with distant , pelvic , and vaginal recurrences ) , and four had combined distant and vaginal recurrences . 
in the chemoradiotherapy group , 63 ( 81% ) of 78 distant recurrences were distant only ( of which nine were isolated para - aortic nodal recurrences ) ; 11 were combined distant and pelvic recurrences ( including one with distant , pelvic , and vaginal recurrence ) , and four were combined distant and vaginal recurrences . isolated vaginal recurrence was the first site of recurrence in one patient ( 03% [ 95% ci 0021 ] ) in both groups ( hr 099 [ 95% ci 0061590 ] ; p = 099 ) , and isolated pelvic recurrence was the first site of recurrence in four women ( 09% [ 0328 ] ) in the radiotherapy group and in three ( 09% [ 0328 ] ) in the chemoradiotherapy group ( hr 075 [ 95% ci 017333 ] ; p = 071 ; table 2 )  . figure 4 shows recurrences by cancer stage and histological type . 
across the different histological types , the greatest risk of recurrence was for serous cancers ( 47 [ 448% ] of 105 ) , followed by clear cell cancers ( 17 [ 274% ] of 62 ) and grade 3 endometrioid endometrial cancer ( 59 [ 277% ] of 213 )  . median survival after recurrence was 14 years ( iqr 0537 ) in the total portec - 3 cohort and did not differ significantly between the two treatment groups : 14 years ( 0737 ) for patients in the radiotherapy group and 12 years ( 0489 ) in the chemoradiotherapy group ( hr 106 [ 95% ci 075151 ] ; p = 072 ; table 3 )  . 
in both groups , about 910% of patients ( n = 33 ; 16 in the radiotherapy group and 17 in the chemoradiotherapy group ) survived for several years after recurrence ( appendix p 12 )  . 
in the chemoradiotherapy group , various combinations of chemotherapy agents were used ( data not shown ) and only 12 ( 40% ) of 30 patients received carboplatin plus paclitaxel again ( details of treatment received by the other 18 women are provided in the appendix p 3 )  . 
60 months after randomisation , grade 3 adverse events were reported for 16 ( 8% ) of 201 women in the chemoradiotherapy group versus ten ( 5% ) of 187 women in the radiotherapy group ( p = 024 )  . 
the most frequently reported grade 3 adverse events were hypertension ( in four women [ 2% ] in both groups ) , any pain ( in three [ 1% ] women in the chemoradiotherapy group vs three [ 2% ] in the radio therapy group ) and other toxicities ( in three [ 1% ] women in the chemoradiotherapy group vs two [ 1% ] in the radiotherapy group )  . at 60 months , grade 2 or worse adverse events were reported for 76 ( 38% ) of 201 women in the chemoradiotherapy group versus 43 ( 23% ) of 187 women in the radiotherapy group ( p = 0002 )  . 
sensory neuropathy grade 2 or worse was the major difference between the two groups at 5 years , seen in 13 ( 6% ) of 201 patients after chemoradiotherapy versus no patients in the radiotherapy group ( table 4 )  . discussion these updated results of the portec - 3 trial , with a longer median follow - up of 72 months and with 75% of participants having reached 5 years of follow - up , showed a significant improvement in both overall and failurefree survival with chemoradiotherapy versus radiotherapy alone for high - risk endometrial cancer . 
the absolute improvement at 5 years was 5% ( hr 070 ; 95% ci 051097 ) for overall survival and 7% ( 070 ; 052094 ) for failure - free survival . 
women with serous cancers had worse overall survival and failure - free survival than those with other histological types , and for these women a significant improvement of overall survival ( absolute improvement 19% ; hr 048 [ 95% ci 024096 ] ) and failure - free survival ( absolute improvement 12% ; 042 [ 022080 ] ) was found with chemoradiotherapy compared with radiotherapy alone . external - beam radiotherapy has been the standard adjuvant treatment for women with high - risk endometrial cancer for several decades . 
since trials comparing adjuvant chemotherapy alone with external - beam radiotherapy alone did not show differences in survival , 5 , 6 the combination of external - beam radiotherapy with four cycles of platinum - based chemotherapy was investigated vaginal ( n = 16 ) pelvic ( n = 51 ) distant ( n = 179 ) any recurrence ( n = 185 ) recurrence type figure 4 : recurrences divided by stage ( a ) and histology ( b ) figo = international federation of gynaecology and obstetrics . in the randomised nsgo - ec - 9501 / eortc - 55991 trial.19 a pooled analysis with the mango iliade - iii trial showed a significant improvement in progression - free survival at 5 years with chemoradiotherapy versus radiotherapy alone ( 78% vs 69% , p = 001 ) and a nonsignificant improvement in 5 - year overall survival ( 82% vs 75% ; p = 007 ) .19 the rtog 9708 phase 2 trial investigated combined external - beam radiotherapy with concurrent and adjuvant chemotherapy , with both treatment modalities started early after surgery . 
 the portec - 3 trial confirmed these high survival rates in a large randomised trial , with estimated 5 - year overall vol 20 september 2019 1281 articles number events median survival , * years ( iqr ) hazard ratio ( 95% ci ) log - rank p value vaginal or pelvic recurrence chemoradiotherapy radiotherapy alone total distant metastases chemoradiotherapy radiotherapy alone total any recurrence chemoradiotherapy radiotherapy alone total 12 ( 07nr ) 14 ( 09nr ) 14 ( 09nr ) 12 ( 0389 ) 15 ( 0737 ) 14 ( 0537 ) 12 ( 0489 ) 14 ( 0737 ) 14 ( 0537 ) 131 ( 026655 ) 074 105 ( 073150 ) 079 106 ( 075151 ) 072 nr = not reached . 
for women with stage iii endometrial cancer , combined adjuvant treatment yielded only a small absolute improvement of 2% ( hr 084 ; 95% ci 052138 ) in 5 - year overall survival and of 4% ( 087 ; 056136 ) in failure - free survival . 
these results are supported by the results of the gynecologic oncology group ( gog ) - 249 trial , in which women with stage iii endometrial cancer were randomly assigned to receive external - beam radio therapy or vaginal brachy therapy and three cycles of carboplatin in overall paclitaxel chemo therapy . 
no differences survival or recurrence - free survival were reported , but pelvic and para - aortic recurrences were significantly more frequent after vaginal brachytherapy and chemotherapy.20 taking the results of the gog - 249 and portec - 3 trials together , a minimal benefit in failurefree survival and overall survival in stage iii endometrial cancer achieved with chemo radiotherapy does not seem to justify the increased frequency of adverse events , impaired quality of life , and longer treatment duration of combined treatment for these patients . for women with stage iii endometrial cancer in portec - 3 , a significant improvement in overall survival ( hr 063 ) and in failure - free survival ( hr 061 ) was found with chemoradiotherapy versus radiotherapy alone . 
 in the gog - 258 trial , 813 women with stage iiiiva endometrial cancer were randomly assigned to receive pelvic external - beam radiotherapy with concurrent and adjuvant chemotherapy ( with the same schedule as that of the portec - 3 trial ) , or to receive chemotherapy alone ( six cycles of carboplatin and paclitaxel ) .21 although no differences in recurrence - free and overall survival were found , significantly more vaginal recurrences ( hr 036 ) and pelvic or para - aortic , or both , recurrences ( hr 043 ) were seen in women treated with chemotherapy alone . 
 while using the same chemoradiotherapy schedule as in portec - 3 , recurrence - free survival in gog - 258 was 59% ( 97% stage iii ) compared with 71% in portec - 3 for stage iii disease . 
in retrospective cohorts , a high frequency of locoregional recurrence was also found after treatment with chemotherapy alone , 7 , 8 , 22 supporting the continued use of pelvic radiotherapy in patients undergoing adjuvant chemotherapy . 
taking the findings of these two recent large trials together , the addition of chemotherapy should be discussed and recommended for women with stage iii endometrial cancer to improve failure - free and overall survival as part of shared decision making between doctors and their patients . overall and failure - free survival for women with serous cancers were lower than for those with endometrioid and clear cell cancers , and the difference in overall survival and failure - free survival among the different disease stages was more pronounced for women with serous cancers than for those with other histologies . 
retrospective studies have reported improvements in overall survival and recurrence - free survival with chemotherapy for serous cancers.23 , 24 in several randomised trials , however , subgroup analyses for treatment effect in types did not confirm such different histological benefits.19 , 20 , 25 in a gog study of four randomised chemotherapy trials in women with meta static and recurrent endometrial cancer , comprising 1203 patients , no association was found between response and histological type.26 in the portec - 3 trial , however , a significant improvement in both overall survival and failure - free survival was found for women with serous cancers treated with chemoradiotherapy . 
in the current portec - 3 analysis , we found that the frequency of recurrence among women with clear cell cancers was similar to that of women with endometrioid tumours and clearly lower than that of women with serous cancers . 
for each adverse event , the maximum grade per patient was recorded ( worst ever by patient )  . table 4 : grade 2 and 3 adverse events reported at 60 months after randomisation in the portec - 3 trial , 105 patients with serous cancers were included . 
portec - 3 is the first randomised trial to show a significant improvement in overall survival and failure - free survival with combined adjuvant treatment for women with serous cancers , but in absolute terms mostly for higher stage disease . 
serous cancers are characterised by a high frequency of tp53 mutations , and in approximately 25% of patients an overexpression of her2 / neu has been reported , with a potential progression - free survival benefit by addition of trastuzumab to chemotherapy.27 , 28 most first recurrences in the portec - 3 trial were at distant sites , with only few simultaneous vaginal or pelvic recurrences . 
this finding is in line with other randomised trials that used radiotherapy in both groups.19 , 20 in the portec - 3 schedule , which was based on the rtog - 9708 phase 2 trial , 12 both treatment modalities were started early after surgery , aiming at achieving rapid efficacy of both treatment modalities and potential increase of the effect of radiotherapy by the two concurrent cycles . 
this schedule has now been proven safe and effective in two large , randomised trials with toxicity and qualityof - life data , whereas no phase 3 evidence is available for the specific benefit for other sequences of radiotherapy and chemotherapy.9 , 10 , 19 , 21 widespread differences exist in the practice of giving chemotherapy and vol 20 september 2019 1283 articles radiotherapy in either sequence or in a so - called sandwich schedule ; concurrent start of both modalities might be most effective and efficient . 
since most first recurrences were at distant sites ( although with fewer in the combined treatment group than in the radiotherapy - only group ) , one could speculate whether multi - agent chemotherapy should already be given concurrently . 
however , no evidence exists for other concurrent schedules in endometrial cancer , whereas , for example , weekly carboplatin and paclitaxel has been shown to be effective in patients with oesophageal cancer . in a patient preference study done by the anzgog group among their portec - 3 participants , 29 more than 50% of women reported a 5% survival improvement or an extra 1 year survival as being sufficient to make chemotherapy worthwhile . 
although both co - primary endpoints showed a significant improvement and are within this range , weighing the benefits of chemoradiotherapy against the increased risk of adverse events remains important . 
significantly more severe adverse events and reduced health - related quality of life were reported in the combined treatment group during the first year after treatment.9 , 10 however , rapid recovery was seen , with no significant differences in grade 34 adverse events from 12 months onwards . 
at 60 months after randomisation , significantly more patients reported grade 2 toxicity with the combination treatment , of which sensory neuropathy is the most significant ( 6% vs 0% ) and clinically relevant.9 , 10 a limitation of this analysis is that the subgroup analyses were not powered and the survival update was a non - prespecified , post - hoc analysis , with an additional follow - up time of 12 months after 95% of the required failure - free survival events had occurred . 
however , the previous ( time - based ) analysis already showed a significant improvement in failure - free survival , and the overall survival difference was close to significance . 
 the differences in overall and failure - free survival have remained and have even become stronger with a longer follow - up time and more events recorded . in terms of the statistical significance of our findings , the p value for failure - free survival was 0016 and that for overall survival was 0034 , whereas the boundary for claiming positivity of the study based on pocock correction was 0031 ( ie , if either or both of the p values were lower than 0031 the study is deemed positive )  . 
the sequential rejection principle14 implies that , since the null hypothesis of no treatment difference for failure - free survival was rejected ( p < 0031 ) , the null hypothesis of no treatment difference for the co - primary endpoint of overall survival can then be assessed at the 005 level , while still retaining a family - wise error rate of 005 . 
 application of this principle implies that the treatment effect for overall survival can be considered significant . better selection of women for adjuvant treatment might be achieved by integration of molecular characteristics . 
for intermediate - risk endo metrial cancer , an improved risk assessment was reported with an integrated profile of clinicopathological and molecular risk factors.30 this approach is currently being tested in the randomised portec - 4a trial ( nct03469674 )  . 
a pilot study of the transportec consortium showed that determination of the molecular subgroups as described by the cancer genome atlas group27 also improved risk assessment in high - risk endometrial cancer . 
the molecular subgroups and additional molecular characteristics will be ascertained and the benefit of adjuvant chemotherapy in relation to these factors will be explored . in conclusion , this updated analysis of the portec - 3 trial shows improved 5 - year overall and failure - free survival with chemoradiotherapy compared with radiotherapy alone for women with high - risk endometrial cancer , with the greatest absolute benefit for chemotherapy seen in women with stage iii disease or serous cancers , or both . 
molecular analysis has the potential to improve risk stratification and should be used to identify subgroups that can derive the greatest benefit from chemotherapy and to select patients for targeted therapies ; molecular studies on tissue samples donated by portec - 3 trial participants are ongoing . contributors clc was the chief investigator of the trial . 
lm reports that hospira provided paclitaxel chemotherapy for anzgog patients on the portec - 3 trial randomised to the experimental arpb reports grants from the canadian cancer trials group , during the conduct of the study . 
hwn reports grants from the dutch cancer society , grants from health holland , grants from umcg cancer fund , outside the submitted work ; is the founder of sme vicinivax ; and has collaborated with aduro , tron , and merck . 
all other authors declare no competing interests in relation to this study . data sharing de - identified participant data will be made available when analyses of all primary and secondary endpoints , including the translational research studies related to the trial , have been published , following the completion of a data transfer agreement . 
this will specifically be done in an appropriate intergroup setting . acknowledgments the portec - 3 study was supported by a grant from the dutch cancer society ( ul2006 - 4168 / ckto 2006 - 04 ) , the netherlands . 
participation in the portec - 3 trial by the australia and new zealand gynaecologic oncology group ( anzgog ) and the trans - tasman radiation oncology group ( trog ) were supported by the nhmrc project grant 570894 1284 vol 20 september 2019 articles ( 2008 ) and by a cancer australia grant ( awarded through the 2011 round of the priority - driven collaborative cancer research scheme and funded by cancer australia )  . 
we thank all the participating groups : dgog ( the netherlands ) , ncri ( uk ) , anzgog ( australia and new zealand ) , mango ( italy ) , fedegyn ( france ) , and the canadian cancer trials group ( canada ) ; their coordinating teams , principal investigators , staff , and clinical research teams at the groups participating centres for all their work and efforts , and the women who participated in the trial . 
 the portec - 3 trial involved a strong international collaboration within the gynaecological oncology intergroup ( gcig ) and the support of the gcig officers and member groups is gratefully acknowledged . 
this analysis was presented in part at the annual meeting of the european society for radiotherapy and oncology , april 2024 , 2018 , barcelona , spain . editorial see comment page 1192 see articles page 1203 for the nhs figures see statistical - work - areas / cancerwaiting - times / measuring the quality of cancer care in uk hospitals analyses of cancer registries are accepted methods of documenting the burden of disease within a region , providing a wealth of data ranging from cancer types endemic in the population to the e ects of available treatments . 
such analyses have been integral to the creation of national cancer care plans , and help policy makers to decide which areas of cancer care to invest to address geographical disparities in cancer care , there has been a trend to break down these regional data into smaller geographical areas . 
but what is the best way to measure the quality of care at such a level ? waiting times from general practitioner ( gp ) referral to rst cancer treatment ; hospital discharge rates ; 30 - day mortality ; and hospital - level cancer survival statistics are all routinely debated as viable options . obtaining su cient data to produce useable quality - of - care metrics at the hospital - level is di cult . 
 even for common cancers , most hospitals will not see enough patients over the course of a year to produce relevant statistics , and thus comparisons between hospitals can be confounded by small numbers and low statistical power . 
moreover , patients with cancer sometimes attend more than one hospital for their care ; thus , attributing patients and their outcomes to a particular hospital is unavoidably complicated and can skew data . 
jeremy hunt , the uks health secretary , has repeatedly called for cancer survival statistics by hospital in an e ort to highlight geographical disparities in care and draw attention to poor performers . 
 however , as discussed by melanie morris and colleagues in this issue of the lancet oncology , these metrics are awed , most obviously by referral bias , which misrepresents hospital performance due to the patient case mix . 
 for patients with cancer , the time between referral from their gp to receipt of their rst interventional treatment has also captured public attention as a measure of quality of care , and the latest gures show the national health service in england is falling short of the 2 - month target . 
 but is this metric any better than other targets , given it too can be heavily confounded ? an alternative to survival statistics and referral time is the measurement of mortality . 
in todays issue of the lancet oncology , we publish the rst report on 30 - day mortality per hospital trust after palliative and curative chemotherapy for patients with breast and lung cancer . 
 based on the systemic anti - cancer therapy ( sact ) database , and in contrast to survival statistics , this metric allows some interpretation of the quality of treatment at the hospital - level . 
as discussed by the authors of the report , another major di culty with interpreting the data is the lack of complete information : for example , several hospitals only had data for patients who completed just one cycle of chemotherapy . 
moreover , data on performance status , which is known to a ect a patients ability to receive certain treatments , or their response , was missing for many individuals thereby limiting interpretation . 
 clearly , the availability of relevant cancer statistics to measure and analyse quality of care , and its use to rank hospital quality in a meaningful way is an ongoing challenge . 
 the more pressing issue of how to measure and analyse data once it is collected is more di cult , and a composite approach made up of several measures , similar to the approach already used by the uk care quality commission , is required . 
it is easy to call for greater transparency in the reporting of the quality of care , as politicians have done , and it is indeed laudable and necessary to do so . 
 the lancet oncology vol 17 september 2016 1171 correction to lancet oncol 2017 ; 18 : 34756 correction to lancet oncol 2019 ; 20 : 137085 correction to lancet oncol 2020 ; 21 : 137886 glynne - jones r , sebag - montefiore d , meadows hm , et al . 
lancet oncol 2017 ; 18 : 34756the last clause of the last sentence of the first paragraph of the introduction of this article should have read or by giving maintenance chemotherapy after chemoradiotherapy.7 this correction has been made to the online version as of nov 2 , 2020 . motzer rj , rini bi , mcdermott df , et al , on behalf of the checkmate 214 investigators . 
nivolumab plus ipilimumab versus sunitinib in firstline treatment for advanced renal cell carcinoma : extended follow - up of efficacy and safety results from a randomised , controlled , phase 3 trial . 
 lancet oncol 2019 ; 20 : 137085 in this article , supplementary table 1 in the appendix has been updated to correct international metastatic renal cell carcinoma database consortium risk percentage values in patients in the intention to treat group . 
lancet oncol 2020 ; 21 : 137886in table 2 of this article , the reference value for absolute risk reduction of incident gastric cancer over 10 years in indi viduals with an unfavourable life style should have been 0 for low genetic risk , intermediate genetic risk , and high genetic risk . 
these corrections have been made to the online version as of nov 2 , 2020 . vol 21 november 2020 e518 corrections for more on slintecare see campaigns / slaintecareimplementation - strategy / for data on cancer survival in ireland see articles lancet oncol 2019 ; 20 : 1493505 for more on the eu beating cancer plan see europa.eu / health / sites / health / files / non_communicable_ diseases / docs / ev_20200204_ factsheet_en.pdf irelands general election : new goals for cancer care ? the 2020 irish general election took place on feb 8 , delivering a major shift in direction for mainstream irish politics . 
for the first time in history , sinn finpreviously a minority party with historical links to paramilitary organisation the irish republican army ( ira ) won the highest number of votes , changing the once two - party system into a clear three - horse race . 
many voters seemed to be calling for change in bringing sinn fin to the fore , neck - and - neck with previous opposition party fianna fil , and leaving outgoing taoiseach ( prime minister ) leo varadkars fine gael party in third place . 
if sinn fin were to secure a prominent role in the next irish government , how might this manifest in irelands health - care policies ? with the mission of giving workers and families a break , sinn fins policies have clearly struck a chord with a substantial portion of the voting public by answering their calls for improvement on the current state of social and housing affairs . 
in other health care - related policies , sinn fin pledged 45 billion to be spent on the health service ( more than twice that promised by fianna fil , but 05 billion less than fine gaels pledge )  . 
sinn fin also committed to implementing slintecarea 2017 all - party report into health - care reforthe proposed reforms aim to move ireland away from the current two - tier health system , in which out - of - pocket payments are required for some health - care services . 
as the only member of the european union ( eu ) that does not offer universal health coverage , moving towards a single - tier , universal healthcare system would be a major achievement . in its manifesto , sinn fin also outlined several policies to improve care for patients with cancer , such as implementing the national cancer strategy to improve cancer survival . 
although ireland saw the highest overall increases in cancer survival between 1995 and 2014 , it ranked lowest in terms of 5 - year survival for ovarian cancer compared with six other high - income countries in the international cancer benchmarking partnership . 
 the party also committed to improving education and awareness of breast cancer and cervical cancer and investing in clinics that provide long - term aftercare for patients with gynaecological cancers . 
sinn fin has made provision of medical cards to patients with cancer a priority , which would enable the estimated 40 000 people diagnosed with cancer in ireland annually to access free health care without incurring out - of - pocket expenses . 
 holders of medical cards are entitled to free hospital , general practitioner , and dental services , among others , as well as prescription drugs and medical devices , but they are currently only available to people receiving welfare payments , those on low incomes , and senior citizens . 
for example , funding for cancer research and clinical trials were promised in the manifestos of fianna fil and fine gael , but seem to be absent from their new opponents policies . 
sinn fins manifesto also lacks details about many other major cancers and on the challenges ireland has faced surrounding access to imaging , diagnostics , and state - of - the - art treatments . 
 however , in terms of health and cancer care at least , there does seem to be more that unites the three parties than separates the irelands membership of the eu might also help it to achieve some of the goals for health - care refor on feb 4 , 2020 , the president of the european commission , ursula von der leyen , launched a consultation on the eu beating cancer plan to build support among eu member states for an overarching strategy to address prevention , diagnosis , treatment , and aftercare of patients with cancer at a national level . 
with the percentage of eligible women receiving a mammogram in the past 2 years ranging from 02% to 82% in different eu member states , a unified strategy is clearly needed to align cancer priorities and fix disparities between countries . 
the plan will begin with a consultation phase , and although it is too early to tell how ambitious it will be , the opportunity to be part of the development and implementation of the plan will be valuable for member states such as ireland . 
 the lancet oncology vol 21 march 2020 editorial published online august 6 , 2019 s1470 - 2045 ( 19 ) 30530 - 3 published online july 30 , 2019 s1470 - 2045 ( 19 ) 30521 - 2 correction to lancet oncol 2019 ; 20 : 114859 correction to lancet oncol 2019 ; 20 : 121125 bonvalot s , rutkowski pl , thariat j , et al . 
 nbtxr3 , a first - in - class radioenhancer hafnium oxide nanoparticle , plus radiotherapy versus radiotherapy alone in patients with locally advanced soft - tissue sarcoma ( act.in.sarc ) : a multicentre , phase 23 , randomised , controlled trial . 
 lancet oncol 2019 ; 20 : 114859in this article , the funder pharmaengine , inc , was inadvertently omitted and has now been added to the funding line in the summary and to the acknowledgments . 
a repeated sentence has been deleted from the fifth paragraph of the statistical analysis section of the methods , and some minor typographical errors have been corrected throughout the paper . 
 these corrections have been made to the online version as of sept 2 , 2019 . correction to lancet oncol 2019 ; 20 : 117182 nen nr , reisel d , leimbach a , et al . 
the following sentence has been added to the figure 4 caption : sdi quintiles are ordered from high to low sdi quintile , and gbd super - regions are alphabetically ordered . 
the next sentence should read : country order selected by total absolute dalys ; countries with the greatest total absolute dalys , of the fifty most populous countries in the world , are listed first . 
this correction has been made to the online version as of aug 6 , 2019 . correction to lancet oncol 2019 ; 20 : 127385 de boer sm , powell me , mileshkin l , et al . 
adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
lancet oncol 2019 ; 20 : 127385in this article , data ( hazard ratios , 95% cis , and p values ) in the following sentence on p 1279 have been corrected : in women with stage iii disease , 5 - year overall survival was 838% ( 95% ci 784895 ) with chemoradiotherapy versus 820% ( 95% ci 765877 ) with radio therapy alone ( hr 084 [ 95% ci 052138 ] ; p = 050 ) , and 5 - year failure - free survival was 813% ( 95% ci 747863 ) with chemoradiotherapy versus 773% ( 95% ci 705827 ) with radiotherapy alone ( hr 087 [ 95% ci 056136 ] p = 054 ; appendix p 8 )  . 
on p 1282 , the same data ( hazard ratios and 95% cis ) in the following sentence have also been corrected : for women with stage iii endometrial cancer , combined adjuvant treatment yielded only a small absolute improvement of 2% ( hr 084 ; 95% ci 052138 ) in 5 - year overall survival and of 4% ( 087 ; 056136 ) in failure - free survival . 
 these corrections have been made to the online version as of sept 2 , 2019 , and the printed version is correct . correction to lancet oncol 2019 ; 20 : e41733 herrera fg , irving m , kandalaft le , coukos g . 
 this correction has been made as of july 30 , 2019 . correction to lancet oncol 2019 ; 20 : e50321 spence d , dyer r , andall - brereton g , et al . 
 lancet oncol 2019 ; 20 : e50321the affiliations of authors dingle spence and m austin argentieri have been corrected in the online version as of sept 2 , 2019 . vol 20 september 2019 e468 corrections correction to lancet oncol 2014 ; 15 : 150312 correction to lancet oncol 2019 ; 20 : 76980 correction to lancet oncol 2019 ; 20 : 98699 open - label phase 1 / 2 jg , niesvizky r , kumar sk , berdeja et al . 
 lancet oncol 2014 ; 15 : 150312in the eighth paragraph of the results section of this article , the first sentence should have been overall responses were noted in 59 ( 92% , 95% ci 8397 ) of 64 patients ( table 5 )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 765 ben - aharon i , goshen - lago t , fontana e , et al . 
this correction has been made to the online version as of july 1 , 2019 . 2018 jacob s , yap ml , wilson be , ferlay j , bray f , barton mb . 
 lancet oncol 2019 ; 20 : 76980 in the affiliations for this article , dr mei ling yap should have been affiliated with the university of new south wales ( sydney , nsw , australia )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 795805 randomised , controlled hofvind s , holen s , aase hs , et al . 
 lancet oncol 2019 ; 20 : 795805 in figure 1 , the number of patients with screen - detected breast cancer in the digital breast tomosynthesis group should have read 95 , and the number of patients in the digital mammography group should have read 87 . 
 quizartinib versus salvage chemotherapy in relapsed or refractory flt3 - itd acute myeloid leukaemia ( quantum - r ) : a multicentre , randomised , controlled , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 98699in this article , the second sentence in the statistical analysis section should have read the sample size calculation wording in the original protocol specified a 5% , two - sided calculation ; however , this wording was inaccurate , and subsequently , a one - sided calculation at 25% was implemented to solely test for superiority of quizartinib , which is consistent with the primary aim of the study . 
this correction has been made to the online version as of july 1 , 2019 , and the printed article is correct . correction to lancet oncol 2019 ; 20 : e30212 hillengass j , usmani s , rajkumar sv , et al . 
these corrections have been made to the online version as of july 1 , 2019 . vol 20 july 2019 e346 corrections news published online april 2 , 2020 s1470 - 2045 ( 20 ) 30217 - 5 for more on the characteristics of covid - 19 patients see jama 2020 ; published online march 23 . 
on the one hand , a patient might be at high risk of contracting the infection and dying from it ; on the other hand , the patient might be at high risk of the cancer progressing or causing death if it is not treated appropriately . 
 physicians have to assess whether treatment plans should be initiated on schedule or delayed , and if so , for how long ? stresses nhs england that individual patient decisions have to be made by multidisciplinary its guidance establishes teams . 
patients who are awaiting non - curative therapy that is unlikely to offer palliation , tumour control , or more than 1 years cancer guidelines during the covid - 19 pandemic as of april 1 , 2020 , more than 800 000 cases of coronavirus disease 2019 ( covid - 19 ) had been confirmed worldwide . 
 on march 26 , gethin williams , a colorectal surgeon at the royal gwent hospital in newport , wales , warned that his institution was under severe strain , with operating theatres turned into intensive care units to accommodate the influx of patients with covid - 19 . 
 according to an analysis of italian patients published in march , 20% of those who died from covid - 19 in the country had active cancer . the esmo website includes general information on covid - 19 , a q&a section , and links to useful resources . 
there is also advice on supporting patients and on infection control . in its guidance for managing patients with cancer requiring acute treatment , nhs england warned that certain groups are particularly vulnerable to serious illness if they become infected with severe acute respiratory syndrome coronavirus 2 . 
the blood cancers often directly compromise the immune system , so those patients are probably most at risk , whereas cancers such as colon cancer , breast cancer , and lung cancer do not typically cause immune suppression that is not treatment - related . schilsky notes that standard chemotherapy regimens for most solid tumours mainly cause transient immune suppression that manifests in low white blood cell counts . 
you can prop up the white blood cells using colony - stimulating factors , so these patients are probably at lower risk than the blood cancer patients , he told the lancet oncology . the pandemic poses several challenges for oncology services . 
we are seeing systems adapt to this now , with telephone and telehealth consultations , people receiving laboratory testing at facilities closer to their homes , and some evaluations being delayed , said schilsky . 
nhs lists several englands guidance for more on the resources for covid - 19 offered by the society of surgical oncology see for more on the statement by esso see org / news / esso - statementcovid - 19 / for more on the information provided by asco see information for more on guidance from the american society of radiation oncology see astro.org / daily - practice / covid19 - recommendations - andinformation for more on the information by the american society for transplantation and cellular therapy see org / communities / publichome ? communitykey = d3949d84 - 3440 - 45f4 - 814290ea05adb0e5 for more on the information by ebmt see org / covid - 19 - and - bmt for more on the guidance by the us food and drug administration see download for more on the guidance by the us national cancer institute see gov / investigatorresources / corona_virus_guidance.htm for more on the guidance by ema see health / sites / health / files / files / eudralex / vol - 10 / guidanceclinicaltrials_covid19_ en.pdf for more on the guidance by the uk national institute for health and care excellence see guidance / ng162 for more on the global radiation oncology targeted response see sciencedirect.com / science / article / pii / s2405630820300227 extension of life are assigned the lowest priority level . 
for radiotherapy , there are five levels of priority , patients with rapidly proliferating tumours with little scope for delay are in the highest group . several other cancer societies have issued some guidance . 
the society of surgical oncology website includes disease - site specific resources to help guide decisions in the era of covid - 19 , as well as a series of podcasts from different specialists . 
 there are information sheets on a range of malignancies , including breast cancer , colorectal cancer , endocrine cancer , and melanoma , with each subdivided into disease types , when appropriate . in a statement issued on covid - 19 , the european society of surgical oncology ( esso ) advised against seeing patients older than 70 years in the clinic , unless urgent . 
rest and recuperation , as well as psychological support should be factored into planning , the statement concluded . the asco website also assembles a great deal of information on patient care and covid - 19 , along with links to guidance from organisations such as the us centers for disease control and prevention and several oncology societies . 
asco has produced guidance on how practices should ready themselves for the virus ; advice can be found on staffing , clinical preparedness , infection prevention and control , and patient scheduling . 
there is also a set of tips for enhancing mental and physical healthone suggested exercise is mindful handwashing , which could be a neat way to combine hygiene and wellbeing . the american society for radiation oncology website contains a large section on covid - 19 . 
its website contains frequently asked questions , several of which are directly relevant to clinical decision making , and links to journal articles and relevant websites . the american society for transplantation and cellular therapy and the european society for blood and marrow transplantation ( ebmt ) have both issued guidelines for covid - 19 management . 
due to the rapidly changing situation , access to a stem cell donor might be restricted either due to the donor becoming infected , logistical reasons at the harvest centres in the middle of a strained healthcare system , or travel restrictions across international borders , note the ebmt guidelines . 
it is therefore strongly recommended to have secured stem cell product access by freezing the product before start of conditioning and , in situations when this is not possible , to have an alternative donor as a back - up . on the regulatory side , the us food and drug administration has issued guidance on managing clinical trials during the time of covid - 19 , as have the us national cancer institute and the european medicines agency ( ema )  . 
the ema document outlines the changes and adaptations that might be required over the course of the pandemic , for example , if trial participants need to be isolated , access to public places is limited , or health - care professionals have to take up different duties . 
the uk national institute for health and care excellence has issued guidance on delivering radiotherapy and systemic cancer therapies , which draws from nhs englands guidance . finally , the global radiation oncology targeted response emerged from an online discussion involving 121 contributors march , 2020 . 
but they also point out that although deferring radical treatment for diseases with favourable biology might seem immediately preferable , it might have unintended consequence in creating a further unmanageable surge in activity when the crisis has passed . it is too early to tell what shape this pandemic will take . 
 yi - long wu ( guangdong lung cancer institute , guangdong , china ) points out that the major disruption in the country to cancer care occurred during the first two weeks of february . 
from late february , everywhere except for hubei province , we were able to start giving patients surgery , chemotherapy , and radiotherapy again , he told the lancet oncology . 
now we are coming back to normal . talha khan burki 630 vol 21 may 2020 news bermuda cancer and health centre , and bermuda hospitals board , hamilton dv04 , bermuda ( c fosker mbchb ) christopher.fosker@bhb.bm i declare no competing interests at bchc , our clinical radiation team is very small : one physician , one physicist , three radiation therapists , and two nurses . 
the normal workflow of day - to - day work has altered drastically in weeks , moving to video consulting , scheduling staff rotas to minimise the risk of infection between team members , procuring personal protective equipment , and developing protocols for its use . 
we do our clinical treatment reviews as we collect patients from the car park one at a time , and escort them directly to the radiation medical linear accelerator ( linac ) machine . 
these new measures are all out of our normal comfort zone , but patients are as equally adaptable as the staff . although some of our new approaches are unique to our setup , decisions we have had to make in real time have been validated when protocols and guidance established elsewhere , including by the royal college of radiologists in the uk and the american college of radiology , have reached the same conclusions . 
bchc has a clinical collaboration with the dana - farber / brigham and womens cancer center ( boston , ma , usa ) and they have been incredibly helpful . beyond the focus on oncology , a group of local primary care physicians have set up a group email chat as a forum for information sharing for all physicians on the island . 
 the group email very quickly showed that the challenges being faced across all specialties were very similar and that we could learn and share a huge volume of ideas across the group . 
the conversation also exposed the challenges of an art of medicine covid - 19 and cancer care in bermuda bermuda is a very small island nation with a population of 62 400 people , located in the middle of the atlantic ocean . 
a high - income country with the third highest healthcare spending per capita in the world , it has close medical links to numerous top - ranked us hospitals and government ties to the uk . 
that was even before bermuda joined the world in trying to find a way to fight the coronavirus disease 2019 ( covid - 19 ) pandemic . there is no doubt that there are many places around the world with a more challenging situation than we find ourselves in bermuda . 
however , our geographical isolation combined with our very small population and small medical workforce means there is a sense of vulnerability that we probably share with other small island nations . 
 furthermore , our health - care system is generally not very integrated and collaboration between the public and private sectors has been forced to ramp up rapidly . my usual role is medical director and radiation oncologist at a charity , bermuda cancer and health centre ( bchc ) , and medical oncologist at king edward memorial hospital ( kemh )  . 
during the pandemic , i have also stepped in as deputy chief of medicine at kemh while the chief of medicine , the islands only infectious diseases specialist , focuses on covid - 19 preparedness . 
 as the pandemic shifted from theory to reality , workflow changes and difficult decisions have had to be made quickly , but without the support of committees , think tanks , and researchers that a larger country can call on . the earliest example was a decision to suspend routine screening mammography even before our first confirmed case of covid - 19 . 
new contingency protocols for which cancer diagnostic imaging studies were crucial had to be developed , and rationalisation of cancer treatment priorities and timing decided . vol 21 june 2020 perspectives unstructured health - care system without a clear leadership framework . it was clear that numerous groups were looking at the same problems . 
responsibilities and formal and informal roles were shared across a previously disconnected group , and pathways such as procurement of personal protective equipment have become more centralised . as alterations in pathways of care become the new reality in everyday working life , they will require continual reassessment . 
in nigeria , about 102 000 new cases of cancer occur annually , and 75 000 deaths per year are caused by cancer.3 one key area in which the new agency can contribute to reducing cancer mortality in nigeria is improving access to cancer medicines . 
in nigeria , cancer is not covered under the national health insurance scheme and the cost of cancer medicines is prohibitive.2 for instance , a course of trastuzumab for patients with breast cancer costs more than us$1585 , 2 which is about 28 - times the monthly wage of the lowest - paid government worker in nigeria . 
given that the challenge of access to cancer medications in low - income and middle - income countries such as nigeria can only be e ectively tackled through a combination of public and private e orts , 4 the new agency would be in a position to coordinate and mobilise partnerships for funding and technical support for access to cancer medicines in nigeria , similar to what has been achieved by the national agency for the control of aids , who has gained leverage over multistakeholder publicprivate partnerships to provide free or heavily subsided hiv medicines to nigerian patients . 
 certainly , the model of national and international the partnerships publicprivate deployed improvement of nancing and delivery of hiv medicines in low - income and middle - income countries is possible with cancer treatments.5 therefore , the nigerian government is urged to expedite actions towards the take - o of the proposed agency and to engage with all relevant stakeholders from both the public and private sectors in its planning and operation to ensure e ective and sustainable delivery of cancer care in nigeria . 
lancet 2010 ; 376 : 118693 . access to essential medicines for children with cancer : a joint siop - cci position statement treatment of cancer in childhood is both a major success of modern medicine and a stark reminder of its limits . 
in high - income countries , multimodality therapy cures more than 80% of children.1 in low - income and middle - income countries ( lmics ) , where most children with cancer live , far fewer children are cured than in high - income countries . 
whos essential medicines list ( eml ) sets the basic bar that all national governments should meet in provision of medicines.2 the revised eml includes an expanded list of core medicines required for multiple malignancies , including the most prevalent paediatric cancers.3 ensuring access to such medicines is an explicit component of the broad right to health enshrined in international human rights conventions.4 the international society of paediatric oncology ( siop ) and childhood cancer international ( cci ) held a symposium at the 48th siop congress in dublin , ireland , on oct 19 , 2016 , entitled essential medicines for children with cancer : dynamics and challenges . 
this joint position statement summarises the symposiums key consensus international oncology ndings to galvanise the community to achieve sustained improvements in access to medicines for children with cancer , regardless of disease or geography . 
the deliberations , situational analysis , and recommendations were framed by four vol 18 january 2017 comment commonly cited core domains of access : availability , accessibility , acceptability , and a ordability ; we included quality as a fth domain.5 availability relates to how medicines are produced and distributed . 
barriers to availability include but are not limited to : inadequate drug production , secondary to weak market incentives or poor forecasting of childhood cancer treatment needs ; national failures to comply with eml recommendations ; and rigid regulatory frameworks governing drug licensing and importation . 
cancer medicines are often inaccessible in lmics because of weak systems of supply management , inventory controls , fractured supply channels , and inadequate infrastructure for proper transport and storage . 
medicines for children with cancer are distinct since many require formulation as sterile injectables ; consequently , they are complicated to produce , require cold storage , and have short shelf lives . 
moreover , they are dosed by weight or body surface area , making it di cult to manufacture vials that minimise waste , or for pills , doses appropriate to varying stages of child development . 
 a ordability refers to the relationships between cost , price , and ability to pay and addresses issues related to drug price determination , how medicines are purchased , and the e ects of these factors on patient access . 
these barriers rest on multiple factors , including national resource constraints and competing health system priorities ; small , fragmented markets for paediatric cancer drugs ; thin industry pro t margins due to patent expiry ; and absence of public or employerbased health insurance . 
 in generic quality incorporates appraisals of drug safety and e cacy and addresses problems related to drug panel : recommendations to improve global access to childhood cancer medicines availability development of a database listing reliable suppliers of essential medicines for children research to assess and understand barriers to national formulary compliance with eml with cancer recommendations across lmics who - led attempts to harmonise national regulatory regimes through regional collaboration to facilitate pooled procurement e orts to develop a not - for - pro t capacity for development of o - patent cytotoxic drugs for children , with the potential for global scale - up accessibility human resource investments in paediatric pharmacists , whose scienti c and on - theground knowledge is crucial to sound policies on supply chain management for antineoplastic drugs development of speci c guidelines on infrastructural and oversight requirements for injectable chemotherapeutics for children formalised voice for childhood cancer experts in national policy making on drug procurement and supply acceptability development of intrainstitutional and interinstitutional policies to minimise waste of regional partnerships with trusted producers to ensure reliable production processes , with a view to minimisation of introduction of potential harmful excipients research into patient and provider experiences of use of cancer medicines in lmic medicines settings a ordability expanded public insurance coverage for essential childhood cancer medicines for children with cancer regionally pooled purchasing reduction or removal of importation tari s on childhood cancer medicines exploration of innovative nancing approaches to provision of o - patent cytotoxic drugs quality development of a who - certi ed list of reputable drug suppliers and formulations to guide national procurement improved methods of interinstitutional and health - care user knowledge sharing on drug quality , including through creative uses of mobile technology , to facilitate improved postmarketing quality surveillance enhanced training programs for lmic pharmacists and bedside providers in safe and accurate preparation and administration of chemotherapeutics in children expanded research into new , cost - e ective , point - of - care quality diagnostics eml = essential medicines list . 
the capacity for generic production of most essential medicines for children with cancer is a double - edged sword : it lowers prices but di uses production , complicating assessments of drug origination and thus quality assurances . 
such assurances are further compromised in many lmics by weak or absent pharmacovigilance in the vol 18 january 2017 comment face of decentralised and often labyrinthine systems of drug procurement and supply . our recommendations to improve global access to childhood cancer medicines are summarised in the panel . 
 ongoing e orts include formal collaboration with who on iterative updates to the eml for children and plans for cross - sectoral consultation at in - depth symposia during the 2017 siop and cci annual congresses in washington , dc , usa . 
only sustained advocacy and e ective policies in line with our recommendations will induce real and lasting gains in access to essential medicines for all children with cancer . * avram denburg , brijesh arora , ramandeep singh arora , carmen auste , poonam bagai , ronald barr , julia challinor , tim eden , edith grynzspancholc , ruth ho man , michael link division of haematology / oncology , hospital for sick children , university of toronto , toronto , on , m5g 1x8 , canada ( ad ) ; tata memorial hospital , mumbai , india ( ba ) ; max super speciality hospital , saket , new delhi , india ( rsa ) ; childhood cancer international , manila , philippines ( ca ) ; childhood cancer international , new delhi , india ( pb ) ; department of pediatrics , mcmaster university , hamilton , canada ( rb ) ; school of nursing , university of california san francisco , san francisco , ca , usa ( jc ) ; world child cancer , london , uk ( te ) ; fundacin natal dafne flexer , buenos aires , argentina ( eg ) ; american childhood cancer organization , washington , dc , usa ( rh ) ; and stanford university school of medicine , palo alto , ca , usa ( ml ) avram.denburg@sickkids.ca we declare no competing interests . 
we thank all participants in the joint international society of paediatric oncology - childhood cancer international essential medicines symposium at the 48th international society of paediatric oncology congress in dublin , ireland , on oct 19 , 2016 , on whose insights and input this position statement is based . 
arlington : management sciences for health , 2012 . biosimilar and generic cancer drugs unlikely to bend cost curve in the usa although biosimilar and generic oncology drugs have been positioned as so - called cost game - changers to the worldwide drug market , this label might be premature as it is unlikely that they will bend the cancer cost curve in the usa.1 , 2 generic drugs have the exact structure as their reference products , and assays indicate they typically have bioavailability between 80% and 125% of reference molecules . 
oncology biosimilar products , which are close copies of biological medicines , were rst approved in the usa in 2015 with the biosimilar lgrasti the biosimilar regulatory framework substantially di erent from that for generics and is rapidly evolving with substantial country - to - country variation . 10 years of lgrastim biosimilars in europe have resulted in cost reductions of 45%60% . 
1 year with biosimilar lgrastim in the usa , on the other hand , has resulted in cost savings of only 10% ; 3 however , in the usa there is only one biosimilar lgrastim and one reference lgrasti generic imatinib in the usa was associated with purchasing savings of 2%4% ; 4 however , generic imatinib outside the usa has been associated with purchasing savings of 50%95%.4 , 5 the price of patented imatinib in the usa is us$146 000 per year and $30 00038 000 per year in europe and canada.5 the price of generic imatinib is $140 000 per year in the usa , but only $50008000 per year in canada , and $400 per year in india and other developing nations.4 why are cost savings so low in the usa for both biosimilars and generics ? one reason might lie in litigation : the us department of justice and 18 state attorney generals have initiated lawsuits against generic manufacturers , alleging collusion in pricing . 
the us food and drug administration ( fda ) might also play a role : empirical data6 show that cost savings occur with vol 18 january 2017 corrections correction to lancet oncol 2015 ; 16 : 522 correction to lancet oncol 2016 ; 17 : 553 correction to lancet oncol 2016 ; 17 : 733 philip , pa . 
 this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . eggermont amm , chiarion - sileni v , grob j - j , et al . 
this correction has been made to the online version as of june 1 , 2016 . correction to lancet oncol 2016 ; 17 : 751 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . vol 17 june 2016 e223 correction to lancet oncol 2019 ; 20 : 168190 correction to lancet oncol 2020 ; 21 : 24249 correction to lancet oncol 2020 ; 21 : 27182 j - y , lee kh , ahn m - j , han et al . 
lazertinib in patients with egfr mutation - positive advanced non - smallcell lung cancer : results from the dose escalation and dose expansion parts of a first - in - human , open - label , multicentre , phase 12 study . 
olanzapine 5 mg plus stand ard antiemetic therapy for the prevention of chemotherapy - induced nausea and vomiting ( j - force ) : a multicentre , randomised , double - blind , placebocontrolled , phase 3 trial . 
tumour treating fields in combination with pemetrexed and cisplatin or carboplatin as first - line treatment for unresectable malignant pleural mesothelioma ( stellar ) : a multi centre , single - arm phase 2 trial . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 26170 drilon a , siena s , dziadziuszko r , et al . 
 lancet oncol 2020 ; 21 : 26170in the results section of this article , the median treatment duration for patients with cd74ros1 fusions should have been 146 months ( iqr 72181 ) and the median intracranial progression - free survival in 20 patients with cns disease should have been 77 months ( 95% ci 38193 )  . 
 lancet oncol 2019 ; 21 : 27182in the statistical analysis section of this article , the overall safety - evaluable population should have included safety data from the paediatric phase 1 study startrk - ng patients aged 4920 years . 
this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . correction to lancet oncol 2020 ; 21 : e10 f i e l d s tr e a t i n g ceresoli gl , gianoncelli l , grosso f , on behalf of stellar investigators . 
this correction has been made to the online version as of jan 30 , 2020 . correction to lancet oncol 2020 ; 21 : 22232 strm p , kartasalo k , olsson h , et al . 
 this correction has been made to the online version as of jan 30 , 2020 , and the printed article is correct . vol 21 february 2020 corrections editorial for the report see cancer.org / acs / groups / content / @editorial / documents / document / acspc - 048347.pdf making paediatric precision oncology a reality despite accounting for only 1% of all cancers , childhood cancer is the leading disease - related cause of death in children in both the usa and the uk . 
in a report released in september , 2016 , to coincide with childhood cancer awareness month , the american cancer society and the alliance for childhood cancer summarise progress in paediatric cancers , and highlight research gaps and ongoing challenges in these rare but devastating diseases . 
for example , 5 - year survival is now 78% for neuroblastoma overall , but only 4050% for some high - risk subtypes , and some tumours , such as di use intrinsic pontine glioma , are almost always fatal . 
 additionally , many childhood cancer survivors su er late e ects as a consequence of treatments administered during vulnerable phases of development : more than 40% of childhood cancer survivors aged 35 years or life - threatening older have experienced severe or treatment - related health problems and much still remains to be done to meet the health and psychosocial needs of long - term survivors . drug development for childhood cancers is a particularly di cult area . 
special ethical protection a orded to children states that there must be a potential bene t to every child enrolled in a clinical trial , and the process of obtaining informed consent is complicated . 
 the small numbers of children a ected by speci c cancer types also creates competition between di erent research projects to enrol potential participants . so , what can be done to accelerate research and drug development in childhood cancers ? incentives are needed to encourage investment in paediatric cancer - speci c research or in the further development of drugs already approved for adult indications . 
some progress has been made here : the usas 2003 pediatric research equity act ( prea ) requires sponsors who are developing a drug for adult indications to also test the drug in children with the same condition . 
meanwhile , the european society of paediatric oncology is calling for revisions to the eu paediatric medicine regulation to expedite the paediatric development of oncology drugs to increase young patients access to innovative therapies . 
networks and consortia that facilitate sharing of research data between trial groups can also ensure that trial sizes are su ciently large to achieve reliable results . in an era of rapid progress in targeted therapies against cancer , we must ensure that children do not miss out . 
the us national cancer institutes moonshot blue ribbon panel has identi ed the targeting of fusion oncoproteins in childhood cancera major driver of many childhood tumoursas a key priority to accelerate progress in cancer research . 
such goals , in combination with increasing childrens access to existing appropriate therapies , encouraging investment in new drug research and development , and re - evaluating trial designs for children , are all essential to help overcome the di cult , but surmountable , challenges unique to this small yet important patient population . 
 the lancet oncology vol 17 october 2016 1335 correction to lancet oncol 2020 ; 21 : 76375 correction to lancet oncol 2021 ; 22 : 198211 paz - ares l , ciuleanu t - e , cobo m , et al . 
 first - line nivolumab plus ipilimumab combined with two cycles of chemotherapy in patients with non - smallcell lung cancer ( checkmate 9la ) : an international , randomised , open - label , phase 3 trial . 
lancet oncol 2021 ; 22 : 198211in figure 4c of this article , the number at risk at 15 months in the nivolumab plus ipilimumab with chemotherapy group should have been 107 . 
abemaciclib plus trastuzumab with or without fulvestrant versus trastuzumab plus standard - of - care chemotherapy in women with hormone receptor - positive , her2 - positive advanced breast cancer ( monarcher ) : a randomised , open - label , phase 2 trial . 
the text in the results section ( page 769 ) should have read as follows : eight patients in group a , 12 patients in group b , and six patients in group c discontinued at least one study treatment owing to adverse events ( figure 1 )  . 
five patients in group b and four patients in group c discontinued all treatments in the study regimen owing to adverse events and one patient in group a discontinued all treatments in the triplet combination . 
two of the 12 patients in group b discontinued at least one study treatment owing to cardiac failure , two additional patients in group b discontinued study treatment owing to decreased neutrophil count , and another two patients discontinued study treatment due to neutropenia . 
these corrections have been made to the online version as of march 1 , 2021 . vol 22 march 2021 corrections covid - 19 in patients with thoracic malignancies ( teravolt ) : first results of an international , registry - based , cohort study marina chiara garassino , jennifer g whisenant , li - ching huang , annalisa trama , valter torri , francesco agustoni , javier baena , giuseppe banna , rossana berardi , anna cecilia bettini , emilio bria , matteo brighenti , jacques cadranel , alessandro de toma , claudio chini , alessio cortellini , enriqueta felip , giovanna finocchiaro , pilar garrido , carlo genova , raffaele giusti , vanesa gregorc , francesco grossi , federica grosso , salvatore intagliata , nicla la verde , stephen v liu , julien mazieres , edoardo mercadante , olivier michielin , gabriele minuti , denis moro - sibilot , giulia pasello , antonio passaro , vieri scotti , piergiorgio solli , elisa stroppa , marcello tiseo , giuseppe viscardi , luca voltolini , yi - long wu , silvia zai , vera pancaldi , anne - marie dingemans , jan van meerbeeck , fabrice barlesi , heather wakelee * , solange peters * , leora horn * , on behalf of the teravolt investigators summary background early reports on patients with cancer and covid - 19 have suggested a high mortality rate compared with the general population . 
patients with thoracic malignancies are thought to be particularly susceptible to covid - 19 given their older age , smoking habits , and pre - existing cardiopulmonary comorbidities , in addition to cancer treatments . 
 we aimed to study the effect of severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection on patients with thoracic malignancies . methods the thoracic cancers international covid - 19 collaboration ( teravolt ) registry is a multicentre observational study composed of a cross - sectional component and a longitudinal cohort component . 
eligibility criteria were the presence of any thoracic cancer ( non - small - cell lung cancer [ nsclc ] , small - cell lung cancer , mesothelioma , thymic epithelial tumours , and other pulmonary neuroendocrine neoplasms ) and a covid - 19 diagnosis , either laboratory confirmed with rt - pcr , suspected with symptoms and contacts , or radiologically suspected cases with lung imaging features consistent with covid - 19 pneumonia and symptoms . 
associations between demographic or clinical characteristics and outcomes were measured with odds ratios ( ors ) with 95% cis using univariable and multivariable logistic regression , with sex , age , smoking status , hypertension , and chronic obstructive pulmonary disease included in multivariable analysis . 
the registry continues to accept new sites and patient data . findings between march 26 and april 12 , 2020 , 200 patients with covid - 19 and thoracic cancers from eight countries were identified and included in the teravolt registry ; median age was 680 years ( 618750 ) and the majority had an eastern cooperative oncology group performance status of 01 ( 142 [ 72% ] of 196 patients ) , were current or former smokers ( 159 [ 81% ] of 196 ) , had non - small - cell lung cancer ( 151 [ 76% ] of 200 ) , and were on therapy at the time of covid - 19 diagnosis ( 147 [ 74% ] of 199 ) , with 112 ( 57% ) of 197 on first - line treatment . 
13 ( 10% ) of 134 patients who met criteria for icu admission were admitted to icu ; the remaining 121 were hospitalised , but were not admitted to icu . 
univariable analyses revealed that being older than 65 years ( or 188 , 95% 100362 ) , being a current or former smoker ( 424 , 1701295 ) , receiving treatment with chemotherapy alone ( 254 , 109611 ) , and the presence of any comorbidities ( 265 , 109746 ) were associated with increased risk of death . 
however , in multivariable analysis , only smoking history ( or 318 , 95% ci 111906 ) was associated with increased risk of death . interpretation with an ongoing global pandemic of covid - 19 , our data suggest high mortality and low admission to intensive care in patients with thoracic cancer . 
data on the impact of severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection on patients with cancer is scant and predominantly from retrospective series emerging from china . 
although previous reports on patients with cancer infected with sars - cov - 2 have suggested a higher mortality rate compared with the general population , the applicability of such data is hampered by small sample sizes , including 12% of the total patient population with multiple different tumour types , at a single institution . 
among them , patients with thoracic malignancies are thought to be particularly vulnerable . added value of this study to our knowledge , this is the first report of the effect of sars - cov - 2 infection on patients with thoracic cancers , using a global database ( teravolt ) that aims to understand the effect of sars - cov - 2 infection on this patient group . 
to date , we have obtained data from 200 patients with thoracic cancers in eight countries , predominantly in europe , with most patients on active treatment at the time of infection . 
only smoking seems to significantly correlate with higher death rates . implications of all the available evidence overall , patients with thoracic malignancies have a higher mortality compared with that reported for the general population , in line with previous reports from china . 
as most patients were on therapies that have been shown to improve survival at the time of sars - cov - 2 infection , a diagnosis of thoracic malignancy alone should not be an exclusion criteria for icu admission and care . 
teravolt will continue to register patients to identify those with higher risk of severe sars - cov - 2 infection and the effect of specific covid - 19 therapies on outcomes . cases and 416 000 deaths as of june 11.3 due to limited testing capacity , the true global infection and mortality rates are likely to far exceed the confirmed cases.4 one of the first publications describing patients infected with sars - cov - 2 came from the national health commission of china and reported on 1099 patients from 552 hospitals.5 they noted that 24% of patients had comorbidities associated with a more severe sars - cov - 2 infection . 
in patients admitted to hospital , the median duration of hospital stay was 12 days , 5% required an admission to the intensive care unit ( icu ) , 23% required mechanical ventilation and 14% died . 
in the largest report from italy on 1591 patients with covid - 19 admitted to the icu , 88% required mechanical venti lation and 68% had at least one comorbidity , with hyper tension in 49% of patients.6 at the time of publication , 16% of patients had been discharged and 26% had died , with age being the most significant risk factor for mortality . 
many other reports describe similar clinical features of patients presenting with covid - 19.711 the differences in patients demographics and mortality between the reports from china and those from italy and other countries have not yet been fully explained . 
a report of 1524 patients with cancer who were screened at zhongnan hospital in wuhan identified covid - 19 in 12 ( 08% ) patients , seven of whom had non - small - cell lung cancer ( nsclc ) and more than half of whom were on active therapy . 
screening rates allowing for earlier detection of cancers have also undoubtedly dropped as many health - care systems have postponed elective imaging procedures , as has been dramatically observed for breast , colon , and cervical cancer screenings.22 while such strict measures are necessary in the short term to protect patients from sars - cov - 2 infection , prolonged treatment delays could lead to an increase in cancer - related mortality . 
the thoracic cancers international covid - 19 collaboration ( teravolt ) is the first global registry aimed at understanding the effect of sars - cov - 2 infection on patients with thoracic malignancies . methods study design and participants this study is composed of a cross - sectional component and a longitudinal cohort component . 
the cross - sectional part describes the patients and disease characteristics both for cancer and for covid - 19 disease , including treatment received and complications due to therapy ; the longitudinal component is related to the association between potential prognostic factors and outcome . institutions from around the world were invited via email to collaborate . 
almost 200 centres have expressed interest in collaborating on the database ; to date , 87 have received institutional review board approval and have contributed data ( appendix pp 1213 )  . 
main eligibility criteria were patients with thoracic cancer ( nsclc , small - cell lung cancer , mesothelioma , thymic epithelial tumours , and other pulmonary neuroendocrine neoplasms ) with a covid - 19 diagnosis defined as any of the following : lab oratory confirmed ( using rt - pcr techniques ) covid - 19 ; sus pected covid - 19 with at least one of the following symptoms : fever higher than 375c , decrease of oxygen saturation of at least 5% , cough , diarrhoea , otitis , dysgeusia , myalgia , arthralgia , conjunc tivitis , and rhinor rhoea , and , when available , known exposure to a person with confirmed covid - 19 ; or radiologically suspected cases with lung imaging features consistent with covid - 19 pneumonia and symptoms . 
asymptomatic patients found positive for sars - cov - 2 were included in this analysis ; these patients were tested although asymptomatic according to local and institu tional policies or owing to known exposure to a person with confirmed covid - 19 . 
according to the regulation ( eu ) 2016 / 679 of the european parliament and of the council of april 27 , 2016 , the following require ments regarding personal data were guaranteed : pseudony misation and encryption , confidentiality , integrity , availa bility , resilience of treatment systems and services , and the ability to restore the availability and access of data in the event of a physical or technical accident . procedures data are entered into a de - identified redcap ( research electronic data capture ) database , with each institution assigned a unique number . 
redcap is a secure web platsform for building and managing online databases and surveys ; it provides easy data handling ( with audit trails for reporting , monitoring , and querying patient records ) and an automated export mechanism to common statistical packages ( spss , sas , stata , r / s - plus )  . clinical data were extracted from medical records of consecutive patients from jan 1 , 2020 , and will be collected until the end of pandemic declared by who . 
 data are divided into four main categories : demographics , oncological history and comorbidities , covid - 19 diagnosis , and course of illness and clinical outcomes ( appendix p 2 )  . 
 initial case report form variables were chosen according to available data from the literature and are updated on the basis of emerging evidence.23 basic demographic characteristics , including age , sex , smoking status , race , stage of disease at covid - 19 diagnosis ( american joint committee on cancer clinical stages ) , type of thoracic malignancy , current oncological treatment , comorbidities , concomitant medications , method for covid - 19 diag nosis , and need for hospital admission , were recorded ; a complete list can be found in the appendix ( p 2 )  . 
summary measures for asso cia tion between demographic and clinical characteristics and ( hospital isation , prolonged hos pital isation outcomes [ > 8 days ] , and death ) were assessed by univariable logistic models ; the association with risk of death was also assessed with multivariable logistic models . 
in multivariable analysis of factors associated with risk of death , we included sex , age ( > 65 years vs 65 years ) , smoking status ( current or former vs never ) , hypertension , and chronic ( copd ) all factors obstructive pulmonary disease known from the literature to be associated with covid - 19 outcomes in general patient populations . 
with about 150 centres contributing data and about five patients from every centre , a sample size of approximately 750 patients can produce a ci of 2% for estimates of proportion . 
in this study , we present preliminary data on the first 200 consecutive patients enrolled ; the cutoff number was not dependent on previous knowledge of results but was driven by the emergency and the lack of data provided in this setting so far . 
with a ci of less than 14% , we believe the results can assure a reasonably precise preliminary estimate for the purpose of our study . role of the funding source there was no funding source for this study . 
the corresponding author had full access to all of the data and the final responsibility to submit for publication . results between march 26 and april 12 , 2020 , data on the first 200 patients were entered into the teravolt registry , from 42 institutions across eight countries ( italy , spain , france , switzerland , netherlands , usa , uk , and china )  . 180 ( 91% ) of the 198 patients with covid - 19 diagnosis information were diagnosed with covid - 19 by rt - pcr , five ( 3% ) were diagnosed on the basis of clinical symptoms ( with fever > 375c [ n = 4 ] and dyspnoea [ n = 4 ] in most patients ) , and 13 ( 7% ) had radiological find ings that were highly suggestive of covid - 19 . 
most patients had stage iv disease , and 147 ( 74% ) patients were currently undergoing treatment , of whom smoking status age , years 5065 female male current former never race white other region europe asia country italy spain france switzerland netherlands china cancer stage at covid - 19 diagnosis cancer diagnosis nsclc small - cell lung cancer thymoma or thymic carcinoma carcinoid or neuroendocrine malignant pleural mesothelioma ecog performance status currently undergoing treatment 63 / 196 ( 32% ) 79 / 196 ( 40% ) 35 / 196 ( 18% ) 16 / 196 ( 8% ) 3 / 196 ( 2% ) 63 / 196 ( 32% ) 79 / 196 ( 40% ) 35 / 196 ( 18% ) 16 / 196 ( 8% ) 3 / 196 ( 2% ) 63 / 196 ( 32% ) 79 / 196 ( 40% ) 35 / 196 ( 18% ) 16 / 196 ( 8% ) 3 / 196 ( 2% ) 147 / 199 ( 74% ) 106 / 151 ( 70% ) 52 / 199 ( 26% ) 45 / 151 ( 30% ) 41 ( 85% ) 7 ( 15% ) ( table 1 continues on next page ) 144 were receiving systemic therapy ( table 1 )  . 
50 ( 26% ) of 195 patients were on anticoagulants and 42 ( 22% ) were on steroids ( table 1 )  . the most common presenting symptoms were fever , dyspnoea , and cough ( table 2 )  . 
24 ( 12% ) of 198 patients were asymptomatic ; 13 ( 54% ) of these patients were tested in hospitals due to known exposure to a patient with confirmed sars - cov - 2 infection , whereas six ( 25% ) had secondary findings on routine imaging for anti cancer therapy or surveillance ; details on the remaining five patients are unknown . of the 152 hospitalised patients , 134 ( 88% ) met criteria for icu admission , but only 13 ( 10% ) of these patients were admitted to the icu , nine of whom were mechanically ventilated ( table 3 )  . 
predominantly , the reasons for patients not being admitted to icu was reported as not indicated , which included institutional policy against icu admis sion , underlying cancer diagnosis and decision not to escalate to icu , or not indicated due to severity of covid - 19 illness and physician recommen dation not to escalate to icu for futility in patients with advanced - stage cancer ; only six ( 5% ) of 114 patients with data available that were offered icu - level care declined icu admission ( table 3 )  . 
of the 66 ( 33% ) patients who died , 52 ( 79% ) deaths were listed as due to complications from covid - 19 only , seven ( 11% ) as cancer progression only , three ( 5% ) as compli cations from covid - 19 and cancer progression , one ( 2% ) as complications from cancer therapy , one ( 2% ) as cancer progression and other reasons , and one ( 2% ) as other reasons . 
 52 ( 79% ) patients died in hospital , eight died in the icu ( 12% ) , and three ( 5% ) died at home ; details are unknown for the three ( 5% ) remaining deaths . univariable analyses revealed that being older than 65 years ( or 188 , 95% 100362 ) , being a current or former smoker ( 424 , 1701295 ) , receiving treatment with chemotherapy alone ( 254 , 109611 ) , and the presence of any comorbidities ( 265 , 109746 ) were associated with increased risk of death . 
dyspnoea was also associated with increased risk of death ( 620 , 3101323 ) , whereas experiencing no symptoms at the time of diagnosis was associated with decreased risk ( 008 , 000038 ; appendix pp 37 )  . 
although the 918 vol 21 july 2020 articles number of patients is small ( n = 28 ) , patients treated with tkis alone were less likely to be hospitalised ( 024 , 008071 ) than patients not on therapy , whereas patients with fever ( 246 , 127480 ) and dyspnoea ( 266 , 137532 ) were more likely to be hospitalised , as were patients with any comorbities ( 370 , 166821 ) , including copd ( 235 , 103609 )  . 
in multivariable analysis for risk of death , only smoking history ( 318 , 111906 ) was associated with increased risk of death ( table 4 )  . discussion teravolt is a global consortium that was formed to characterise the effects of sars - cov - 2 infection on patients with thoracic cancers . 
our initial report from the first 200 patients entered into the registry suggests that the mortality in patients with thoracic cancer is 33% , and might be as high as previously reported for patients in china.1213 , 17 in multivariable analysis , only smoking habits maintained a significant association with death . 
 comorbidities such as hypertension or ischaemic heart disease , which are associated with increased risk of death in the general population , did not appear to be predictors for poor outcomes in our patient population . 
 the question as to whether smoking exacerbated the effect of other clinically associated variables ( such as copd and other comorbidities ) or there is a net effect of smoking merits further investigation . 
however , these are preliminary data and we acknowledge that more events are needed to observe and confirm effects . while most deaths occurred during hospital isation , only 13 ( 9% ) of 147 patients in our cohort were admitted to the icu , nine of whom received mechanical ventilation . 
this is in contrast with previous reports in which 16% of hospitalised patients were cared for in the icu , 88% of whom received endotracheal intubation and mechanical ventilation , 6 as well as a report from new york city ( ny , usa ) showing that patients with all types of cancer were frequently intubated for covid - 19 treatment.24 part of this could be explained by the geographical locations included in this initial cohort , which were mainly european ( italy , france , and spain )  . 
in addition , our database includes hetero geneity among types of hospitals ( comprehensive cancer centres and general hospitals )  . we tried to capture the reasons for the low rate of icu admission . 
nonetheless , as targeted therapy and immuno therapy have dramatically shifted the paradigm of care and life expectancy for patients with metastatic nsclc , the decision to escalate care should be decided in a multi disciplinary setting and not on the basis of old pre conceptions limiting access to aggressive care for these patients . importantly , our data suggest that the type of systemic therapy , including tkis , chemotherapy , and immunotherapy , did not affect survival in patients with covid - 19 . 
 although the number of patients is small , patients treated with tkis alone were at decreased risk for hospitalisation , and despite initial concerns of increased mortality , immuno therapy did not worsen outcomes for vol 21 july 2020 articles received mechanical ventilation * prolonged hospitalisation ( > 8 days ) hospitalisation icu admission * not indicated no resources available institutional policy patient declined death ( during hospitalisation , icu , or at home ) reasons why patients were not admitted to the icu all patients ( n = 200 ) 152 ( 76% ) 48 ( 24% ) 13 / 147 ( 9% ) 134 / 147 ( 91% ) 9 / 147 ( 6% ) 138 / 147 ( 94% ) 31 / 58 ( 53% ) 27 / 58 ( 47% ) 66 ( 33% ) 125 ( 63% ) 97 / 114 ( 85% ) 4 / 114 ( 4% ) 7 / 114 ( 6% ) 6 / 114 ( 5% ) icu = intensive care unit . 
not indicated includes several factors : not indicated due to mild or moderate covid - 19 symptoms ; not indicated due to underlying cancer diagnosis and decision not to escalate to icu ; or not indicated due to severity of covid - 19 illness and physician recommendation not to escalate to icu for futility . 
for the majority of sites , it also included institutional policy concerning patients with lung cancer . table 3 : hospitalisation and mechanical ventilation use patients with cancer with covid - 19 in our analysis . 
moreover , it is important to acknowledge that previous studies have suggested that frequent contact with the health - care environment increases risk of sars - cov - 2 infection and thus a goal of minimising such contact , especially during cancer therapy , is important.7 , 17 the most common presenting symptoms for patients with thoracic cancer and covid - 19 are also those symptoms frequently noted by patients with thoracic cancer without covid - 19 , including dyspnoea , cough , and fatigue . 
furthermore , the majority of our patients had a stage iv disease ( 74% ) and a large proportion were on active oncological treatment ( 74% ) at the time of sars - cov - 2 infection ; in particular , 57% of patients were on first line with therapy administered a median of 7 days before covid - 19 diagnosis . 
the patients included in this analysis could represent a copd hypertension female sex ( vs male ) age > 65 years ( vs 65 years ) odds ratio ( 95% ci ) 118 ( 059237 ) 116 ( 061221 ) 069 ( 033144 ) 153 ( 077303 ) current or former smoker ( vs never smoker ) 318 ( 111906 ) outcome includes death during hospitalisation , in the intensive care unit , or at home . 
copd = chronic obstructive pulmonary disease . table 4 : multivariable model of factors associated with death selected pop ulation since this initial cohort did not capture many patients after surgery or radiotherapy ; efforts will be made to expand teravolt participation beyond med ical oncologists to include other thoracic cancer disciplines ( eg , thoracic surgeons and radiation oncologists )  . 
furthermore , we recognise that this is a preliminary report , written to provide more infor mation to clinicians at a crucial time , but that it does not yet have the statistical power to give final answers in terms of subgroup analyses . while the data presented here are representative of mainly symptomatic patients with nsclc stage iv disease on systemic therapy and importantly only include a small fraction of patients who were managed at home for their covid - 19 illness , data are urgently needed to plan the optimal diagnostic and therapeutic pathways for patients with cancer in an environment where sars - cov - 2 is still in circulation , often accompanied with only mild or no symptoms . 
although consecutive inclusion of patients controls the risk of selection bias , thus assuring a correct description of patients characteristics and outcomes , major limitations in the estimation and correct inter pretation of associations were related to control of con founding factors . 
more data on the prevalence and out comes of covid - 19 on asymptomatic patients with thoracic cancer could emerge as hospital systems imple ment broader testing on all patients seeking care . teravolt is a unique effort aimed at providing realtime data to support the optimal diagnostic and therapeutic pathways for all patients with thoracic cancer . 
calabr and colleagues have proposed routine testing for patients with cancer on active therapy ; 25 the continued shortage of testing kits and variances across countries makes such an approach difficult to achieve universally , but it could indeed be the optimal approach once an effective therapy for covid - 19 has been found . 
for now , emphasising social distancing and encouraging measures such as wearing face masks in the community might help to minimise a surge of cases , allowing the medical system to keep up with testing and decreasing the need for physicians to triage care on the basis of age and comor bidities . 
protecting all 920 vol 21 july 2020 articles susceptible members of our societies with protective measures supported by our current knowledge of sars - cov - 2 must remain a priority , while also respecting the needs of each indivi dual , including optimal care management . we believe that a multidisciplinary approach to the treatment of patients with thoracic cancer and sars - cov - 2 infection should consider both the indivi dual cancerspecific mortality and risk of a morbidity or mortality from covid - 19 . 
at this time , it is not clear if intu bation and more aggressive care in patients with cancer could improve covid - 19 - specific survival , or if such an approach would simply prolong the process of dying . 
however , in the absence of clear data , the inte gration of patients preferences could provide a benefit , especially in decisions in which uncer tainty is high.26 in this perspective , a shared decision - making paradigm will allow both patients and clinicians to recognise and pursue the option that best fits the individual . contributors fa , rb , gb , acb , eb , jb , mb , cc , ef , cg , rg , feg , frg , vg , si , svl , nlv , y - lw , dm - s , em , gm , gp , ap , es , vs , ps , lv , and sz collected data . 
hw participated in conception and design of the database , literature searching , and data analysis and interpretation and manuscript writing . declaration of interests all declarations of interest are outside of the submitted work , unless stated otherwise . 
mcg received grants , personal fees , and other financial support from merck sharp & dohme , astrazeneca , novartis , roche , pfizer , celgene ; grants and other financial support from tiziana sciences , clovis , glaxosmithkline , spectrum , and blueprint ; personal fees and other financial support from eli lilly and bristol myers squibb ; grants from merck and bayer ; personal fees from boheringer , otsuka pharma , incyte , inivata , takeda , bayer , sanofi , seattle genetics , and daichii sankyo ; and other financial support from merck serono . 
 glb received personal fees from jannsen - cilag , boheringer / ingelheim , and roche ; and non - financial support from bristol myers squibb , astrazeneca / medimmune , pierre fabre , and ipsen . 
rb has been on the advisory board for astrazeneca , boerhinger / ingelherim , lilly , merck sharp & dohme , and otsuka and has received institutional funding from novartis , lilly , and astrazeneca . 
eb has received personal fees and grants from astrazeneca and roche ; and personal fees from pfizer , merck sharp & dohme , helssin , eli - lilly , bristol myers squibb , and novartis . 
ac has received grants merck sharp & dohme , roche , bristol myers squibb , astrazeneca , and novartis ; and personal fees from merck sharp & dohme , astrazeneca , and astellas . 
ef has had an advisory role or been on a speakers bureau for abbvie , astrazeneca , blue print medicine , boheringer / ingelheim , bristol myers squibb , glaxosmithkline , eli lilly , guardant health , janssen , medscape , merck , merck sharp & dohme , novartis , pfizer , prime oncology , roche , samsung , springer , takeda , touchime , and grifols ; and has received research funding from grant for oncology innovation and fundacion merck salud . 
pg has received personal fees from roche , merck sharp & dohme , bristol myers squibb , boheringer , pfizer , abbvie , novartis , lilly , astrazeneca , jannsen , blueprint , takeda , gilead , and rovi . 
 svl has received grants , personal fees , and non - financial support from astrazeneca , merck sharpe & dohme , and roche ; grants and personal fees from bristol myers squibb , and pfizer ; grants from alkermes , bayer , blueprint , corvus , merus , molecular partners , rain therapeutics , rapt , spectrum , and turning point therapeutics ; personal fees from catalyst , cellgene , g1 therapeutics , guardant health , jannsen , lilly , loxo , pharmamar , regeneron , and takeda ; and non - financial support from boheringer . 
nlv received grants from eisai ; had an advisory role for roche , pfizer , novartis , cellgene , and merck sharp & dohme ; received travel and accomodation from roche , gentili , and pfizer ; and been on a speakers bureau from roche and gentili . 
jm has been on the advisory board for merck , roche , astrazeneca , merck sharp & dohme , bristol myers squibb , pfizer , hengruii , daichii , boheringer , and pierre fabre ; and has received research grants from roche , astrazeneca , and pierre fabre . 
 dm - s has received grants , personal fees , and non - financial support from astrazeneca , bristol myers squibb ; grants and personal fees from pfizer , abbvie , and boheringer ; personal fees and non - financial support from merck sharp & dohme and roche ; and personal fees from takeda , amgen , novartis , and lilly . 
y - lw received personal fees from astrazeneca , lilly , roche , pfizer , sanofi , boheringer , merck sharp & dohme , and bristol myers squibb , during the conduct of the study . 
vp has received grants from institute de recherche pierre fabre , fondation toulouse cancer sante , inser fb has received personal fees from astrazeneca , bayer , bristol myers squibb , boheringer / ingelheim , ely lilly , f hoffman / la roche , novartis , merck , merck sharp & dohme , pierre fabre , pfizer , and takeda . 
hw has received grants from gilead ; personal fees from astrazeneca , xcovery , jannsen , daichii , helssin , and mirati ; non - financial support from astrazeneca , takeda , cellworks , roche , merck , fishawak , medscape , onclive , phillips gillmore oncology , physician education resource , potomac centre , prime oncology , primo , research to practice , uptodate , webmdhealth , novartis , rgcon , japanese lung cancer society , korean society of medical oncology , stanford university , and international thymic malignancies interest group ; and other financial support from xcovery , roche , merck , acea therapeutics , arrys therapeutics , astrazeneca , bristol myers squibb , celgene , clovis , exelixis , lilly , pfizer , and pharmacyclis . 
 sp has received personal fees and non - financial support from amgen , astrazeneca , boheringer , bristol myers squibb , clovis , illumina , roche , merck sharpe & dohme , novartis , pfizer , and sanofi ; personal fees from abbvie , bayer , biocartis , daichii , debiofarm , eli lilly , foundation medicine , jannsen , merck , merrimack , pharma mar , bioinvent , regeneron , seattle genetics , and takeda ; and non - financial support from merck serono . 
lh has received grants , personal fees , and travel reimbursement from xcovery ; grants and travel reimbursement from bristol myers squibb ; grants from boheringer / ingelherim ; and personal fees from astrazeneca , roche , incyte , merck , pfizer , xcovery , emd , tesaro , abbvie , medscape , physicians education resource , research to practice , onclive , amgen , and bayer . 
the global , regional , and national burden of pancreatic cancer and its attributable risk factors in 195 countries and territories , 19902017 : a systematic analysis for the global burden of disease study . 
org / s2468 - 1253 ( 19 ) 30421 - 2 . cancer patients in sars - cov - 2 infection : a nationwide analysis in china china and the rest of the world are experiencing an outbreak of a novel betacoronavirus known as severe acute respiratory syndrome corona virus 2 ( sarscov - 2 ) .1 by feb 12 , 2020 , the rapid spread of the virus had caused 42 747 cases and 1017 deaths in china and cases have been reported in 25 countries , including the usa , japan , and spa who has declared 2019 novel coronavirus disease ( covid - 19 ) , caused by sars - cov - 2 , a public health emergency of international concern . 
in contrast to severe acute respiratory system coronavirus and middle east respiratory syndrome coronavirus , more deaths from covid - 19 have been caused by multiple organ dysfun ction syndrome rather than respiratory failure , 2 which might be attributable to the widespread distribution of angiotensin con verting enzyme 2the functional receptor for sars - cov - 2 in multiple organs.3 , 4 patients with cancer are more susceptible to infection than individuals without cancer because of their systemic immunosuppressive state caused by the malignancy and anticancer treat ments , such as chemotherapy or surgery.58 therefore , these patients might be at increased risk of covid - 19 and have a poorer prognosis . on behalf of the national clinical research center for respiratory disease , we worked together with the national health commission of the peoples republic of china to establish a prospective cohort to monitor covid - 19 cases throughout china . 
as of the data cutoff on jan 31 , 2020 , we have collected and analysed 2007 cases from 575 hospitals ( appendix pp 49 for a full list ) in 31 provincial administrative regions . 
 we excluded 417 cases because of insufficient records of previous disease history . ( 28583 18 ( 1% ; 95% ci 061165 ) of 1590 covid - 19 cases had a history of cancer , which seems to be higher than the incidence of cancer in the overall chinese [ 029% ] per 100 000 people , population according to 2015 cancer epidemiology statistics9 )  . 
four ( 25% ) of 16 patients ( two of the 18 patients had unknown treatment status ) with cancer with covid - 19 had received chemotherapy or surgery within the past month , and the other 12 ( 75% ) patients were cancer survivors in routine followup after primary resection . 
compared with patients without cancer , patients with cancer were older ( mean age 631 years [ sd 121 ] vs 487 years [ 162 ] ) , more likely to have a history of smoking ( four [ 22% ] of 18 patients vs 107 [ 7% ] of 1572 patients ) , had more polypnea ( eight [ 47% ] of 17 patients vs 323 [ 23% ] of 1377 patients ; some data were missing on polypnea ) , and more severe baseline ct manifestation ( 17 [ 94% ] of 18 patients vs 1113 [ 71% ] of 1572 patients ) , but had no signifi cant differences in sex , other baseline symptoms , other comorbidities , or baseline severity of x - ray ( appendix p 2 )  . importantly , patients with cancer were observed to have a higher risk of severe events ( a composite endpoint defined as the percentage of patients being admitted to the intensive care unit requiring invasive ventilation , or death ) compared with patients without cancer ( seven [ 39% ] of 18 patients vs 124 [ 8% ] of 1572 patients ; fishers exact p = 00003 )  . 
 most published online february 14 , 2020 s1470 - 2045 ( 20 ) 30096 - 6 see online for appendix vol 21 march 2020 comment invasive ventilation or icu admission , or death , plus clinical indication invasive ventilation or icu admission , or death no cancer cancer survivors patients with cancer cancer status patients without cancer patients with cancer hazard ratio 356 ( 95% ci 165769 ) time after disease onset ( days ) figure : severe events in patients without cancer , cancer survivors , and patients with cancer ( a ) and risks of developing severe events for patients with cancer and patients without cancer ( b ) icu = intensive care unit . we observed similar results when the severe events were defined both by the above objective events and physician evaluation ( nine [ 50% ] of 18 patients vs 245 [ 16% ] of 1572 patients ; fishers exact p = 00008 )  . 
 moreover , patients who underwent chemotherapy or surgery in the past month had a numerically higher risk ( three [ 75% ] of four patients ) of clinically severe events than did those not receiving chemotherapy or surgery ( six [ 43% ] of 14 patients ; figure )  . 
these odds were further confirmed by logistic regression ( odds ratio [ or ] 534 , 95% ci 1801618 ; p = 00026 ) after adjusting for other risk factors , including age , smoking history , and other comorbidities . 
 lung cancer did not have a higher patients with probability of severe events compared with patients with other cancer types ( one [ 20% ] of five patients with lung cancer vs eight [ 62% ] of 13 patients with other types of cancer ; p = 0294 )  . 
additionally , we used a cox regression model to evaluate the time - dependent hazards of developing severe events , and found that patients with cancer deteriorated more rapidly than those without cancer ( median time to severe events 13 days [ iqr 615 ] vs 43 days [ 20not reached ] ; p < 00001 ; hazard ratio 356 , 95% ci 165769 , after adjusting for age ; figure )  . in this study , we analysed the risk for severe covid - 19 in patients with cancer for the first time , to our knowledge ; only by nationwide analysis can we follow up patients with rare but important comorbidities , such as cancer . 
 additionally , we showed that patients with cancer had poorer outcomes from covid - 19 , providing a timely reminder to physicians that more intensive attention should be paid to patients with cancer , in case of rapid deterioration . therefore , we propose three major strategies for patients with cancer in this covid - 19 crisis , and in future attacks of severe infectious diseases . 
 third , more intensive surveillance or treatment should be considered when patients with cancer are infected with sars - cov - 2 , especially in older patients or those with other comorbidities . we declare no competing interests . 
this study is supported by the china national science foundation ( grant no 81871893 ) and the key project of guangzhou scientific research project ( grant no 201804020030 )  . wenhua liang , weijie guan , ruchong chen , wei wang , jianfu li , ke xu , caichen li , qing ai , weixiang lu , hengrui liang , shiyue li , * jianxing he drjianxing.he@gmail.com 336 vol 21 march 2020 comment joint first authors joint senior authors department of thoracic oncology and surgery ( wli , ww , jl , kx , cl , qa , wlu , hl , jh ) and department of respiratory disease ( wg , rc , sl ) , china state key laboratory of respiratory disease and national clinical research center for respiratory disease , the first affiliated hospital of guangzhou medical university , guangzhou 510120 , china chen n , zhou m , dong x , et al . 
zhonghua zhong liu za zhi 2019 ; 41 : 1928 ( in chinese )  . should patients who are incarcerated on death row receive palliative cancer care ? in modern society , it is accepted that individuals have the right to die with dignity . 
at present , there are more than 2600 incarcerated men and women in the usa who have been sentenced to death , most of whom have less than a high school diploma or high school equivalency certificate ( ged ) , and are disproportionately of minority racial or ethnic backgrounds ( 42% african - american representation on death row vs 13% african - american representation in the us census ) .1 the combination of poor health status , social determinants of health , and paucity of adequate care provided in correctional facilities is driving a public health emergency , which is endangering the incarcerated population . 
we can north american expect the prevalence and burden of chronic illness to rise concomitantly with the growth of the ageing population in us prisons.2 data suggest that cancer is the leading cause of illness - related deaths in us state prisons.2 in the absence of reform , the mass incarceration trends observed over the past three decades will substantially widen disparities , adversely affecting access to health care . 
this dilemma is bound to have a downstream effect on patients with cancer who have been sentenced to death and can affect the quality of palliative care provided in correctional facilities . 
in the community , a multidisciplinary team would manage the medical , mental health , and social service needs of a patient who chooses palliative care for a terminal diagnosis . 
but what of the patient who is sentenced to die by judicial execution ? that any such person should receive a benefit of any sort , including the traditional last meal , is met with public protest and outrage . 
such consternation will probably increase despite the fact that denying palliative care results in unnecessary suffering for the patient at no benefit to public safety . is well established that professional ethics forbids health - care staff from participating in any aspect of capital punishment . 
however , what of the incarcerated patient with cancer who is dying under the care of a physician with direct or indirect duties to the jurisdiction charged with judicial execution ? what are the duties of the physician expected to provide palliative care to the incarcerated if the patient desires it ? we argue that they are no different than those incumbent upon the physician and health - care staff in the community . 
the accepted framework of medico ethical principles requires that oncology practitioners consider pain relief and other principles of palliative vol 21 march 2020 comment published online april 9 , 2020 s1470 - 2045 ( 20 ) 30223 - 0 for more on masks for nhs heroes see crowdfunder.co.uk / masks4nhsheroes for more on the modelling by who on ppe needs see detail / 03 - 03 - 2020 - shortage - ofpersonal - protective - equipmentendangering - health - workersworldwide for more on guidelines on cancer care during covid - 19 see coronavirus - information / careindividuals - cancer - duringcovid - 19%20f workers at the highest risk of acquiring an infection , but the nurses working on the bone marrow transplant unit also need them . disruptions in care patients with cancer are at a high risk of severe covid - 19 disease if they become infected with the virus , and decisions have to be made to reduce their exposure to the virus . 
 but we have to balance the risk of exposure with the risk of not treating or undertreating patients , challinor said . additionally , facilities also reallocated resources to treat patients with covid - 19 , which has resulted in disruptions in routine cancer care . 
guidelines from professional organisations , such as the american society of clinical oncology , suggest implementing protocols that delay elective surgeries , switching from intravenous to oral therapies possible ( to decrease the frequency of clinic visits ) , or modifying or withholding chemotherapy depending on the situation . 
but as the number of patients with covid - 19 increases , many hospitals have deferred all but the most urgent treatment to conserve staff and equipment . however , cancer care cannot be stopped for most patients , and nurses and other personnel caring for patients lack of protective gear disrupts oncology care a recent crowdfunding campaign caught the attention of scottish actor james mcavoy , who was inspired to donate 275 000 to the campaign . 
 coined masks for nhs heroes , the physician - led initiative is raising money to increase the amount of certified one face masks , visors , surgical gowns , and gloves that are available to health - care workers caring for patients with coronavirus disease 2019 ( covid - 19 )  . the outpouring of support from the public has been enormous . 
in their appeal , the doctors note that : unfortunately current hospital supplies are not sufficient and while we are reassured the government is doing everything it can , health - care workers on the frontline are risking themselves daily without adequate protection to care for sick patients . 
health - care workers on the frontline without ppe [ personal protective equipment ] is the equivalent of going to war without armour and protection . the new target was increased to 1 500 000 and the campaign has reached this target ( by april 8 )  . the availability of ppe is largely taken for granted by health - care personnel who work in high - income countries , but the advent of covid - 19 set off a global frenzy to secure supplies that would be needed to provide appropriate protection to health - care workers . 
modelling done by who estimated that 89 million medical masks , 76 million examination gloves , and 16 million goggles would be needed for the covid - 19 response vol 21 may 2020 every month . 
who guidance also called for the rational and appropriate use of ppe for health - care workers and effective management of supply chains . in a response to the current ppe shortage , dame donna kinnair , chief executive and general secretary of the royal college of nursing , said that even though the government is finally prioritising covid - 19 testing for nhs staff , including social care , it is completely unacceptable that weeks into this crisis , there are colleagues in all settingshospitals , community , or care homeswho have not been provided with ppe . she added , i am hearing from nurses who are treating patients in covid - 19 wards without any protection at all . 
 they are putting themselves , their families , and their patients at risk . although much of the attention has focused on ppe use for covid - 19 , the shortage has also affected cancer care , where it is used for both patient and health - care worker protection . 
 the use of chemotherapy - tested gloves , single - use disposable gowns , respirators or masks , eye protection , and closed - system transfer devices are recommended to protect nurses and pharmacists against unintentional exposure to antineoplastic drugs , and protective gear is required to care for patients with cancer who are in isolation or during certain procedures . they are not just for preventing infection but are needed for protecting the health - care workers and any one handling hazardous drugs , said julia m challinor , an international nursing consultant for oncology . 
there is no gold standard on how to measure exposure , but we do know that its not okay to be exposed every day . the idea is also to prioritise equipment , challinor noted . 
face masks , for example , are prioritised for health - care news for more on ons guidelines see interim - guidelines for more on covid - 19 cases among health - care workers in italy see nursingtimes.net / news / coronavirus / nurses - amongconfirmed - deaths - from - covid19 - around - theworld - 20 - 03 - 2020 / for more on covid - 19 cases in spain see com / 2020 / 03 / 24 / world / europe / coronavirus - europe - covid - 19 . html for more on ringwelskis story see com / 2020 / 04 / 01 / opinion / coronavirus - doctors - protectiveequipment.html ? referringsource = articleshare for more on mazurkiewiczs story see chicagotribune.com / news / breaking / ct - nurse - northwesternmemorial - hospital coronavirus - 202003246smjuxbn6fgnxpaiyzzkjymorqstory.html for more on the bellingham hospital story see seattletimes.com / seattle - news / health / er - doctor - who - criticizedbellingham - hospitalscoronavirus - protections - hasbeen - fired / for more on the nyu langone and montefiore health system recommendations regarding media see bloomberg.com / news / articles / 2020 - 03 - 31 / hospitalstell - doctors - they - ll - be - fired - ifthey - talk - to - press for more on gagging of nhs staff see theguardian.com / society / 2020 / mar / 31 / nhs - staff - gagged - overcoronavirus - protectiveequipmentshortages#maincontent need appropriate ppe . 
 the us oncology nursing society ( ons ) has acknowledged that nurses working in cancer care are facing difficult choices if the recommended ppe supplies are not available to the they are making choices regarding the protection of themselves and their patients from potential covid - 19 infection and use of ppe for safe handling of hazardous cancer drugs , says the ons . 
in response to this crisis , the ons has issued interim guidelines for ppe use in oncology settings where ppe supplies might be limited . the royal marsden hospital in london ( uk ) has confirmed that that they have a good supply of ppe , distributed across the hospital according to the latest national guidelines . 
the royal free london nhs trust foundation also reports no issues with ppe . elaine tomlins , consultant oncology nurse , stated that at a hospital on the south coast of england , the oncology unit has moved to a private hospital where there is no covid - 19 care at the current time . 
but there are ppe shortages across the hospital and disinfectant wipes are not available for routine care in oncology . a district general hospital in the west midlands is also reporting shortages in the oncology unit , said young . facing termination about 9% of covid - 19 cases in italy , a country that has been hit hard by the virus , are health - care workers . 
however , many workers do not speak up about the lack of ppe for fear of losing their jobs . in new york city , ny , usa , ania ringwelski , an emergency room physician at weill cornell medical center , did not feel that the ppe supplied by the facility was adequate so she obtained her own . 
in another us city , chicago , il , lauri mazurkiewicz , a nurse working at northwestern memorial hospital , had been warning her coworkers that the standard face masks being distributed by the hospital were not safe for caring for patients with covid - 19 . 
in turn , hospitals have threatened to fire employees who publicly speak about their working conditions and one instance , an emergency room doctor in bellingham , wa , usa , openly discussed the conditions at the facility where he was employed . 
 two health - care systems new york city , nyu langone and montefiore health system , have sent all employees memos reminding them of policies that all media requests must go through the public relations department . 
nyu langone also added that employees would be subject to disciplinary action , including termination , if they did not comply . a similar situation has been reported in the uk , where according to evidence collected by the doctors association uk ( dauk ) , nhs staff are being gagged from speaking out about widespread shortages of ppe . 
one of the testimonies given to dauk was from an intensive care physician who was concerned about the facemasks , but was told by the hospital that if we hear of these concerns going outside these four walls your career and your position here will be untenable . future concerns the us centers for disease control and prevention ( cdc ) has issued guidelines to optimise the use of ppe under the current situation . 
considering that the landscape is changing daily , this is an urgent situation , since hospitals have not faced ppe shortages in the us ever before , so there are no studies showing what is appropriate action , she said . 
what i am afraid of , is that governments in low - income and middle - income countries in the future will say they do not have to buy ppe for oncology nurses because they saw us government agencies recommending homemade ppe for covid - 19 and so they should be fine for oncology as well . 
we do not want governments to be thinking that if it is good enough for covid - 19 , it is good enough for chemotherapy , she added . roxanne nelson 632 vol 21 may 2020 news correction to lancet oncol 2019 ; 20 : 155665 correction to lancet oncol 2019 ; 20 : e658 correction to lancet oncol 2020 ; 21 : e31729 bertelsen ca , neuenschwander au , jansen je , et al . 
lancet oncol 2019 ; 20 : 155665in this article , two patients ( one in the control group and one in the complete mesocolic excision group ) were incorrectly classified as not having recurrences , due to an error in data extraction . 
 the incorrect data have been updated in the summary findings , the results , figures 2a and 2c , table 3 , supplementary figures 2c and 2f in the appendix , and the discussion . 
complete mesocolic excision for colon cancer : is now the time for a change in practice ? lancet oncol 2019 ; 20 : 147476in this comment , the cumulative incidence of recurrence in each group has been amended , owing to these data being corrected in the linked article by bertelsen and colleagues . 
lancet oncol 2019 ; 20 : e658 in this correspondence , the absolute in risk of recurrence reduction has been amended , owing to this being corrected in the linked article by bertelsen and colleagues . 
this correction has been made to the online version as of aug 3 , 2020 . correction to lancet oncol 2020 ; 21 : e33036 cooney tm , cohen jk , guimaraes cv , et al . 
these corrections have been made to the online version as of aug 3 , 2020 . vol 21 august 2020 e372 corrections the impact of the covid - 19 pandemic on cancer deaths due to delays in diagnosis in england , uk : a national , population - based , modelling study camille maringe , james spicer , melanie morris , arnie purushotham , ellen nolte , richard sullivan , bernard rachet * , ajay aggarwal * summary background since a national lockdown was introduced across the uk in march , 2020 , in response to the covid - 19 pandemic , cancer screening has been suspended , routine diagnostic work deferred , and only urgent symptomatic cases prioritised for diagnostic intervention . 
in this study , we estimated the impact of delays in diagnosis on cancer survival outcomes in four major tumour types . methods in this national population - based modelling study , we used linked english national health service ( nhs ) cancer registration and hospital administrative datasets for patients aged 1584 years , diagnosed with breast , colorectal , and oesophageal cancer between jan 1 , 2010 , and dec 31 , 2010 , with follow - up data until dec 31 , 2014 , and diagnosed with lung cancer between jan 1 , 2012 , and dec 31 , 2012 , with follow - up data until dec 31 , 2015 . 
we use a routes - to - diagnosis framework to estimate the impact of diagnostic delays over a 12 - month period from the commencement of physical distancing measures , on march 16 , 2020 , up to 1 , 3 , and 5 years after diagnosis . 
to model the subsequent impact of diagnostic delays on survival , we reallocated patients who were on screening and routine referral pathways to urgent and emergency pathways that are associated with more advanced stage of disease at diagnosis . 
we considered three reallocation scenarios representing the best to worst case scenarios and reflect actual changes in the diagnostic pathway being seen in the nhs , as of march 16 , 2020 , and estimated the impact on net survival at 1 , 3 , and 5 years after diagnosis to calculate the additional deaths that can be attributed to cancer , and the total years of life lost ( ylls ) compared with pre - pandemic data . findings we collected data for 32 583 patients with breast cancer , 24 975 with colorectal cancer , 6744 with oesophageal cancer , and 29 305 with lung cancer . 
across the three different scenarios , compared with pre - pandemic figures , we estimate a 7996% increase in the number of deaths due to breast cancer up to year 5 after diagnosis , corresponding to between 281 ( 95% ci 266295 ) and 344 ( 329358 ) additional deaths . 
for colorectal cancer , we estimate 1445 ( 13921591 ) to 1563 ( 15341592 ) additional deaths , a 153166% increase ; for lung cancer , 1235 ( 12201254 ) to 1372 ( 13431401 ) additional deaths , a 4853% increase ; and for oesophageal cancer , 330 ( 324335 ) to 342 ( 336348 ) additional deaths , 5860% increase up to 5 years after diagnosis . 
the total additional ylls across these cancers is estimated to be 59 20463 229 years . interpretation substantial increases in the number of avoidable cancer deaths in england are to be expected as a result of diagnostic delays due to the covid - 19 pandemic in the uk . 
urgent policy interventions are necessary , particularly the need to manage the backlog within routine diagnostic services to mitigate the expected impact of the covid - 19 pandemic on patients with cancer . funding uk research and innovation economic and social research council . copyright 2020 the author ( s )  . 
these patient groups include patients with cancer for whom timely diagnosis and the prompt initiation of treatment is vital for ensuring optimal outcomes.2 , 3 since the beginning of the pandemic , multiple changes in the provision of cancer care from the point of diagnosis , including modification of treatment schedules ( change in therapy , deferral , or omission ) , have been advised by professional bodies and commissioners of services globally.47 however , substantial heterogeneity has been seen in the imple mentation of these recommendations lancet oncol 2020 ; 21 : 102334 published online july 20 , 2020 s1470 - 2045 ( 20 ) 30388 - 0 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on december 30 , 2020 see comment page 1000 * joint senior authors department of non - communicable disease epidemiology ( c maringe phd , prof b rachet phd ) and department of health services research and policy ( m morris phd , prof e nolte phd , a aggarwal phd ) , london school of hygiene & tropical medicine , london , uk ; school of cancer and pharmaceutical sciences ( prof j spicer phd , prof a purushotham md , prof r sullivan phd ) and institute of cancer policy ( prof r sullivan , a aggarwal ) , kings college london , london , uk ; and department of oncology , guys and st thomas nhs foundation trust , london , uk ( prof j spicer , prof a purushotham , prof r sullivan , a aggarwal ) correspondence to : dr ajay aggarwal , department of health services research and policy , london school of hygiene & tropical medicine , london , wc1h 9sh , uk ajay.aggarwal@lshtm.ac.uk vol 21 august 2020 1023 articles research in context evidence before this study in the uk , national covid - 19 pandemic measures since march 16 , 2020 , have resulted in the suspension of cancer screening and deferral of routine diagnostic investigations . 
 additionally , urgent 2 - week wait referrals for patients with suspected cancer initiated by general practitioners ( gps ) have decreased by up to 80% in response to physical distancing . 
to date , no study has attempted to model the impact of changes in health - seeking behaviour and in the availability of and access to diagnostic services in the uk as a result of the covid - 19 lockdown on cancer survival and the additional number of deaths expected . added value of this study to our knowledge , this study is the first of its kind to estimate the impact of delays in diagnostic pathways due to pandemic lockdown measures on cancer survival for four major tumour types . 
we use linked national cancer registration and hospital datasets , which provide a robust template for understanding the impact of current and predicted changes in availability , access , and health - seeking behaviour in response to the covid - 19 pandemic on cancer survival . 
we used a routes - to - diagnosis framework , which is novel and provides a transparent approach to understanding what components of the diagnostic pathway need to be targeted as part of health service mitigation and recovery programmes . 
we also estimated the years of life lost to understand the wider welfare effects resulting from avoidable cancer deaths , and how this varies according to tumour type and the age profile of men and women diagnosed with these cancers . 
 implications of all the available evidence our results are conservative estimates of the number of additional deaths and years of life lost because we do not consider the effect of suboptimal or delayed cancer treatment . 
 these data are essential for policy makers to drive changes in national lockdown and stay - at - home messaging , and to urgently reduce diagnostic delays , particularly for routine investigations , through outreach and accessibility programmes . 
 our model can also be used by other countries in their unique health - care settings to understand the impact of delays in diagnosis on cancer outcomes . across providers nationally and internationally and for individual patients . 
such variations in the extent of treatment delay , and in changes to treatment doses and schedules ( including new treat ment techniques ) mean that modelling of these variations in practice on cancer outcomes at a population level is challenging . instead , in this study , we focused on analysing the impact of changes in cancer diagnostic pathways and subsequent delays in diagnosis during the covid - 19 pandemic . 
routine non - urgent diagnostic work initiated by referral from both primary care ( general practitioners [ gps ] ) and secondary care teams ( eg , for radiology or endoscopic procedures8 ) has been deferred across the uk . 
cancer screening services have been suspended , and patients only routes to diagnosis since lockdown began have been via urgent 2 - week - wait referral pathways for suspected cancer initiated by the gp or through direct presentation to an emergency department.9 patients are eligible for these rapid access 2 - week - wait pathways to access diagnostic investigations , on the basis of their age , symptom profile ( eg , dysphagia ) , signs ( eg , breast lump ) , or results of investigations ( eg , iron deficiency anaemia ) as specified by guidelines developed by the national institute for health and care excellence.9 however , since march , 2020 , changes in health - seeking behaviour have been observed , with urgent 2 - week - wait cancer referrals decreasing by up to 80% in response to physical distancing and concerns about contracting severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) .10 additionally , some form of physical distancing is expected to continue for up to 12 months , which will probably further affect presentations to healthcare services.11 , 12 quantifying the impact of delays in diagnosis on stage and prognosis is complex , but a routes - to - diagnosis approach provides a validated methodological framework for understanding their effect . 
for example , urgent 2 - weekwait referrals for suspected cancer and emergency presentations are asso ciated with later stage of disease at diagnosis than diag noses via routine gp and secondary care referral routes and screening . 
additionally , diagnosis after initial presen tation to an emergency department is consistently asso ciated with the worst survival outcomes compared with all other routes.13 given the changes in health - seeking behaviour and availability and access to diagnostic services as a result of the covid - 19 lockdown , these routes to diagnosis provide a framework for estimating the impact of these changes on stage migration and excess cancer mortality on the basis of patients moving to different referral routes during the pandemic . the effect of delayed presentation on patients with cancer is not immediate , and premature death as a result 1024 vol 21 august 2020 articles might occur up to 5 years later and will differ according to tumour type . 
in this study , using national population datasets of patients diagnosed and treated in the english nhs , we estimated the impact of delays in diagnosis that are attributed to the lockdown measures put in place in the uk in march , 2020 , for four major tumour types : breast , colorectal , lung , and oesophageal . 
we chose these tumour types because they differ in their predominant routes to referral ( including screening ) , stage at presentation , and both short - term and long - term prognoses according to stage . 
we estimated the effect on patient survival and the number of additional deaths expected due to these cancers , and the additional years of life lost ( ylls )  . international classification methods study design and population in this national , population - based , modelling study , we obtained information on adults in england , uk , with non - small - cell lung cancer ( hereafter referred to as lung of diseases cancer : 10th edition c33 , c34 ) , cancers of the colon ( c18 ) and rectum ( c19 ) , cancers of the oesophagus and gastrooesophageal junction ( c15 , c16.0 ) , and women with breast cancer ( c50 ) from the national cancer registration service . 
the pre - pandemic cohort refers to patients diagnosed between jan 1 , 2010 , and dec 31 , 2010 , with follow - up data until dec 31 , 2014 , for cancers of the colon , rectum , oesophagus , and breast , and to patients diagnosed between jan 1 , 2012 , and dec 31 , 2012 , with follow - up data until dec 31 , 2015 , for lung cancer . 
we restricted the analyses to patients aged 1584 years at diagnosis and those who had a known route of diagnosis coded ( ie , 91% of patients for colorectal cancer , 93% of patients for oesophageal cancer , 94% of patients for breast cancer , and 97% of patients for lung cancer )  . the national cancer registration service records and updates patient and tumour characteristics for almost all cancers diagnosed in england ( 98100% ) .14 we derived infor mation on referral pathways from linkages of the cancer registrations with secondary care data ( hospital episode statistics ) , screening records , and data on cancer waiting times.13 we did these linkages using deterministic linkage methods using each individual patients nhs number , with a linkage success of 99100%.14 we derived information on patients comorbidity status from hospital episode statistics diagnostic codes when patients attend hospital.15 we determined levels of deprivation via the quintiles of the index of multiple deprivation income domain for the patients residential postcodes , measured at lower super output area level.16 we used this information to link each patient with their expected mortality according to age , sex , deprivation , and region of residence using general population life tables . this study was done in accordance with existing statutory and ethical approvals from the confidentiality advisory group and research ethics committee ( piag 105 ( c ) / 2007 and rec 13 / lo / 0610 )  . conceptual framework we assumed that the incidence of each of the four tumour types of interest will remain relatively stable year on year on the basis of trends in previous years ( 201018 ) , 17 and that the ongoing covid - 19 pandemic and uk lockdown will mean patients are more likely to delay presentation . 
 we estimated the subsequent impact on survival by reallocating patients from screening and non - urgent routine referral pathways ( from gps and secondary care ) to urgent pathwaysnamely , 2 - week wait referral routes and presentation at an emergency department . 
both of these urgent pathways are associated with later stage of diagnosis and enabled us to estimate the impact of diagnostic delay on stage migration and survival outcome . we justified our reallocation model on four assumed factors . 
second , although routine diagnostic work and non - urgent referral pathways are delayed and screening suspended , some patients awaiting investigation will become symptomatic as their cancer progresses and will meet the criteria for urgent 2 - week wait referral for suspected cancer or present as emergencies direct to secondary care . 
third , for patients awaiting routine diagnostic investigations from their gp and secondary care referrals , substantial delays are expected ( > 6 months ) 12 due to the backlogs of routine work across all medical and surgical services increasing the likelihood of disease progression , which we estimated via reallocation to 2 - week wait and emergency pathways . 
finally , changes in health - seeking behaviour as a result of the pandemic means that some patients will delay presentation until more prominent symptoms develop , and these patients will be more likely to present through 2 - week - wait and emergency pathways . the starting point for our estimation is from march 16 , 2020 , which is the date physical distancing measures were introduced in the uk , and the impact is modelled over a 12 - month period to account for the expected duration of disruption to services and patterns of referral . 
this period defines our cohort of expected number of cancer diagnoses for each tumour type , but we acknowledge that patients might present and be diagnosed beyond this period because of diagnostic delay . 
for example , if 10% of new diagnoses for a given tumour type are after an emergency department presentation , and 90% are via an outpatient referral , our simulation analysis will maintain these proportions when reallocating patients from screening and routine referral pathways . for patients with breast cancer diagnosed via the screening referral pathway , we accounted for the fact that many are diagnosed with pre - invasive disease18 or disease that is unlikely to progress even within a 12 - month period . 
this percentage reflects for more on the hospital episode statistics database see vol 21 august 2020 1025 articles pre - pandemic referral routes 2 - week wait emergency presentation gp routine routine ( outpatients ) routine ( inpatients ) screening 2 - week wait or emergency presentation , both at 100% capacity 2 - week wait , at 20% capacity emergency presentation , at 100% capacity 2 - week wait or emergency presentation , both at 100% capacity 2 - week wait , at 20% capacity emergency presentation , at 100% capacity 2 - week wait , at 75% capacity emergency presentation , at 100% capacity 2 - week wait or emergency presentation , both at 100% capacity scenario time since march 16 , 2020 ( months ) figure 1 : conceptual framework for reallocation of pre - pandemic referral routes in three modelling scenarios ( a , b , and c ) for breast cancer , in addition to patients on routine pathways , only 25% of patients diagnosed through screening ( ie , the proportion of patients with tumour stage iii or iv , node - positive , or metastatic disease ) were reallocated to 2 - week wait or emergency presentation in the pandemic scenarios . 
for colorectal cancer , we undertook reallocation separately for colon and rectal cancer because the proportion of patients presenting via the different referral routes differed between the two cancers , as did the cancer stage at the time of diagnosis . scenarios we based our analysis on three sets of predictions according to possible changes in referral patterns ( figure 1 ) representing the best and worst case scenarios . 
 for scenario a , we estimated survival outcomes for patients by reallocating those who are expected to be diagnosed through screening and routine referral pathways ( gp or secondary care ) to 2 - week - wait and emergency presentation pathways , from march 16 , 2020 . 
 scenario b is the same as scenario a , but from march 16 , we simulated the effect of an 80% reduction in 2 - weekwait referrals , which has already been observed during the lockdown period , 10 and assumed that this reduction will continue ( due to covid - 19 - related concerns ) for up to 3 months . 
and scenario c is the same as scenario b , but we simulated the effect of 2 - week - wait referrals continuing to be reduced beyond the first 3 - month period by 25% for a further 3 - month periodie , until month 6 after introduction of physical distancing measures . 
 therefore , we re - allocated the backlog of patients in months 712 to 2 - week - wait pathways and emergency presentations . statistical analysis we randomly modified the mode of presentation and dates of diagnosis of the pre - pandemic cohorts according to scenarios ac . 
for scenarios b and c , we reallocated a proportion of patients diagnosed through the 2 - week - wait pathway because under these scenarios this referral route was assumed to operate at 20% ( scenario b ) and 75% ( scenario c ) of its usual capacity . we estimated the reallocation of patients from routine and screening pathways to the emergency presentation route at the same proportion observed in the prepandemic cohorts ( table 1 )  . to estimate the impact that the response to the covid - 19 pandemic could have on cancer survival , we compared the net survival of pre - pandemic cohorts of patients with cancer to that of patients diagnosed according to the postulated scenarios ac . 
notably , for colorectal cancer , even though the reallocation from routine to urgent pathways was done separately for patients with rectal and colon cancer , the survival estimates are for the combined colorectal cancer population . 
compared with the number of deaths due to cancer in the pre - pandemic cohorts , we derived the additional number of deaths due to cancer and addi tional number of ylls . 
for breast cancer , in addition to patients on routine pathways , only 25% ( n = 2700 ) of patients diagnosed through screening ( ie , the proportion of patients with t3 , t4 , node positive , or metastatic disease ) were reallocated to 2 - week wait and emergency presentation in the pandemic scenarios . 
 * the proportion of patients diagnosed with stage iii or iv disease is based on patients with available staging information in the cancer registry dataset and has been reported to show the stage variation according to diagnostic referral route ; information on cancer stage is not used in the modelling of net survival . 
point estimates and 95% cis were calculated from bootstrap samples of the original data . table 2 : estimated cumulative number of deaths due to cancer up to 1 year , 3 years , and 5 years after diagnosis , in the pre - pandemic period and for each pandemic scenario ac ( also presented as additional number of deaths ) government office regions . 
since each cancer site - specific mortality is a negligible cause of death , all - cause mortality , as estimated from population life tables , is the mortality that patients with cancer would experience , had they not been diagnosed with cancer.20 , 21 further details and mathe matical formulae are in the appendix ( pp 13 )  . 
cm , br , and aa had full access to all the data in the study and had final responsibility for the decision to submit to publication . results we analysed data on 32 583 patients with breast cancer , 24 975 with colorectal cancer , 29 305 with lung cancer , and 6744 with oesophageal cancer ( table 1 )  . 
patients were aged 1584 years and the mean age at diagnosis was 605 years ( sd 126 ) for breast cancer , 685 years ( 107 ) for colorectal cancer , 685 years ( 103 ) for oesophageal cancer , and 698 years ( 93 ) for lung cancer . 
10 441 ( 418% ) of 24 975 patients diagnosed with colorectal cancer , 13 211 ( 451% ) of 29 305 diagnosed with lung cancer , and 1894 ( 281% ) of see online for appendix vol 21 august 2020 1029 articles b colorectal scenario a scenario b scenario c lung cancer ( n = 29 305 ) oesophageal breast 1500 1000 lung 1500 1000 follow - up time ( years ) follow - up time ( years ) figure 2 : estimated additional number of cancer deaths for each pandemic scenario ac , for breast cancer ( a ) , colorectal cancer ( b ) , lung cancer ( c ) , and oesophageal cancer ( d ) 6744 diagnosed with oesophageal cancer were women . 
in the pre - pandemic period , survival varied substantially by tumour type and referral pathway , with the worst prognosis evident for oesophageal and lung cancers and for patients diagnosed after an emergency presentation . 
these differences in sur vival between referral path ways correlated with increased proportions of patients diagnosed at stages iii and iv , irrespective of tumour type ( table 1 ; appendix p 4 )  . 
notably , 2 - week - wait referral pathways are not associated with substantial differences in stage or survival compared with nonurgent referral routes . we estimated the impact of diagnostic delay for the 12 - month period from march 16 , 2020 , to march 15 , 2021 . 
 across scenarios ac , we estimated an absolute decrease in cancer survival ranging between 1011% ( breast , all scenarios ) and 6163% ( oesophageal , scenarios b and c ) at 1 year after diagnosis , and between 35% ( lung , scenario a ) and 64% ( colorectal , scenario c ) at 5 years after diagnosis ( table 1 )  . the differences in survival translate into substantial additional numbers of deaths due to cancer in the first 5 years of follow - up . 
the estimated number of deaths due to each cancer up to 1 , 3 , and 5 years after diagnosis in the pre - pandemic period and across scenarios ac are shown in table 2 . 
the number of additional cancer deaths estimated across the scenarios are shown as cumulative estimates up to year 5 ( table 2 , figure 2 )  . breast cancer ( n = 32 583 ) colorectal cancer ( n = 24 975 ) scenario a scenario b scenario c scenario a scenario b scenario c scenario a scenario b scenario c scenario a scenario b scenario c oesophageal cancer ( n = 6744 ) years of life lost ( 95% ci ) 8181 ( 77978535 ) 9033 ( 86389390 ) 9261 ( 88439631 ) 27 735 ( 27 18828 241 ) 25 583 ( 24 79227 744 ) 27 043 ( 26 23429 968 ) 20 537 ( 20 18420 947 ) 20 860 ( 20 25021 277 ) 20 413 ( 19 83320 909 ) 5373 ( 52275530 ) 5152 ( 50065301 ) 5027 ( 48615213 ) point estimates and 95% cis were calculated from bootstrap samples of the original data . table 3 : estimated years of life lost from additional deaths due to cancer , at 5 years from diagnosis , for each pandemic scenario we estimated across scenarios ac , compared with the pre - pandemic period , a 2166% increase in the number of deaths due to breast cancer up to year 1 ( corresponding to between 20 [ 95% ci 1525 ] and 63 [ 5770 ] additional deaths ) , a 6891% increase up to year 3 ( 169 [ 159179 ] to 228 [ 218239 ] additional deaths ) , and a 7996% increase up to year 5 ( 281 [ 266295 ] to 344 [ 329358 ] additional deaths )  . 
for lung cancer across scenarios ac , we estimated a 6077% increase in the number of deaths due to cancer up to year 1 ( 1102 [ 10871117 ] to 1412 [ 13791447 ] additional deaths ) , a 5158% increase up to year 3 ( 1231 [ 12161249 ] to 1412 [ 13811442 ] additional deaths ) , and a 4853% increase up to year 5 ( 1235 [ 12201254 ] to 1372 [ 13431401 ] additional deaths )  . 
for oesophageal cancer , across scenarios ac , we estimated a 93103% increase in deaths due to cancer up to year 1 ( 339 [ 334343 ] to 377 [ 372383 ] additional deaths ) , a 6467% increase up to year 3 ( 343 [ 337348 ] to 359 [ 354365 ] additional deaths ) and a 5860% increase up to year 5 ( 330 [ 324335 ] to 342 [ 336348 ] additional deaths )  . the plateau in additional deaths due to cancer over the 5 - year period for lung and oesophageal cancer ( figure 2 ) reflects relatively higher proportions of early cancer deaths at year 1 due to more advanced stage at presentation in our scenarios . 
in the pre - pandemic period , some of these patients would have been expected to die 1030 vol 21 august 2020 articles beyond year 1 as a result of less advanced disease at presentation compared with the pandemic scenarios . overall , in comparison with the pre - pandemic period , the estimated number of additional deaths attributable to these four cancers at 5 years is between 3291 and 3621 deaths across the scenarios due to delays in cancer diagnosis ( table 2 , figure 2 )  . 
we estimated the expected ylls to be between 59 204 and 63 229 years because of additional deaths due to these four cancers in the first 5 years after diagnosis . discussion we estimated that across the four major tumour types , breast , colorectal , lung , and oesophageal , 3291 to 3621 avoid able deaths and an additional 59 204 to 63 229 ylls will be attributable to delays in cancer diagnosis alone as a result of the covid - 19 lockdown in the uk . 
these additional deaths are projected to occur as a conse quence of the national covid - 19 pandemic measures , which have reduced the number of people seeking health care and access to and availability of diagnostic services . 
our findings complement those from a study by sud and colleagues22 showing the impact of treatment delay , predominantly surgical , on excess mortality . from the onset of the lockdown , essential diagnostic services ( eg , endoscopy ) were suspended or operating at substantially reduced capacity , even through the urgent 2 - week - wait referral pathway . 
the number of endo scopies done in april , 2020 , was 90% fewer than the number done in each of the first three months of 2020.23 as of june , 2020 , these diagnostic services had restarted but at reduced capacities.24 these suspensions were due to the perceived risk of exposure to sars - cov - 2 for patients and clinicians , and because of re - deployment of staff towards critical care to manage patients with covid - 19 . 
our results also highlight the substantial proportion of patients diag nosed with cancer through routine outpatient referral pathways ( 3040% ) and the subsequent effect of deferral and delay in these referral pathways during the pandemic . 
even when routine diagnostic services are re - initiated , substantial delays in routine and 2 - week - wait referral pathways are to be expected due to backlogs currently building up across all benign and malignant medical and surgical subspecialities . changes in health - seeking behaviour have meant that routine referrals from gps have reduced in volume because patients are being asked to only present if they have major or urgent concerns.12 additionally , whether the increasing number of remote consultations via telephone or videoconferencing will result in an increased proportion of missed diagnoses , without the ability to examine and triage the patient directly , is unknown . conversely , increased diagnostic efficiency has potentially been introduced into the system as a result of the pandemic . 
for example , patients who now report a symptom to their gp are an enriched population compared with those who reported in the pre - pandemic period and are potentially more likely to have cancer . 
additionally , as of june 18 , 2020 , 2 - week - wait referrals are still not operat ing at level , particularly for endoscopic intervention.25 their usual pre - pandemic our findings reflect the urgent need for policy interventions to mitigate the predicted additional cancer deaths resulting from delays in diagnosis . 
key areas to consider include public health messaging , the publics perception of their personal risk of severe illness from covid - 19 versus the risks of not seeking health - care advice if they are experiencing symptoms suggestive of cancer , provision of evidence - based information to enable health - care workers to adequately manage the risks for patients with suspected cancer during the pandemic with respect to the balance of risks and benefits of procedures , and to consider options and opportunities for increasing diagnostic capacity . in the uk , the stay at home and subsequent stay alert public health messaging has had a substantial effect on health - seeking behaviour.26 even as lockdown measures are being relaxed , presentation to primary care services continues to be much lower than pre - pandemic levels , 25 and we cannot assume that , once all restrictions have been lifted , presentations will return to pre - pandemic levels in the next 36 months . 
any exit strategy from lockdown27 therefore needs to include accurate and measured public health messaging that is tailored towards patients , gps , and secondary care services that puts into perspective the risk of death from covid - 19 compared with other serious illnesses . 
dedicated cancer awareness programmes will need to consider a range of media channels to reach their target groups , including direct messaging from gps to their patients to seek attention if they are having new or worrying symptoms . increasing diagnostic capacity is complex because it necessitates effective coordination across all hospital subspecialities and not just in specialist cancer teams . 
 additionally , the requirement for full personal protective equipment when doing procedures and the initiation of robust cleaning protocols between patients has reduced capacity compared with pre - pandemic levels . 
in the short term , diagnostic capacity can be increased through vol 21 august 2020 1031 articles changes in working patternseg , increased working hours and 7 days - a - week working . 
furthermore , a central coordinating system for diagnostic investigations in a similar vein to a choose - and - book approach , whereby primary care physicians are able to refer patients to any nhs hospital , will optimise use of capacity.28 for detection of bowel cancer , surgeons are increasingly using new tools such as the faecal immuno chemical test29 to triage their patients for investigation to avoid unnecessary colonoscopy and ct imaging and therefore improving capacity in this diagnostic pathway . the paucity of information for health - care workers and patients regarding their risk of contracting covid - 19 from different health - care interactions remains a challenge as hospitals plan for restarting routine services . 
 antibody testing would increase confidence in clinicians doing procedures if immunity to sars - cov - 2 does exist for even a short period.30 the health - care community needs accurate data on the true nosocomial risk of covid - 19 depending on the type of diagnostic procedure being doneeg , colonoscopy versus ct scan . 
equally , the implication of contracting covid - 19 needs to be consideredspecifically , to be able to counsel patients effectively on the true risk of lifethreatening illness and death . a strength of this study is the use of linked national administrative health records of actual patients diagnosed and treated in the nhs for the four tumour types . 
these records provide a robust template for understanding the impact of current and predicted changes in availability , access , and health - seeking behaviour in response to the covid - 19 pandemic on cancer survival . 
this method does not require any de - novo estimation of changes in cancer outcomes but derives this estimation from previous real - world observations . we chose the routes - to - diagnosis concept as our method to analyse diagnostic delay to overcome some of the challenges that have been raised in the scientific literature regarding the relative risk of death from diagnostic delay across tumours.2 , 31 , 32 inconsistencies in the evidence are primarily associated with flaws in study design in which the true onset of symptoms remains unclear . 
additionally , recent work has pointed to a waiting time paradox , whereby quicker diagnosis is associated with later stage of presentation ; this paradox confounds assessment of the impact of diagnostic delay on outcomes.33 , 34 modelling the extent and duration of diagnostic delay at the population level is challenging because diagnostic delays are predicated on health system factors , such as access and availability of diagnostic capacity , and patient - level factors ( awareness , symptoms , health - seeking behaviour )  . 
we acknowledge that our approach might underestimate or overestimate the impact of diagnostic delay on survival , and retrospective evaluation will be necessary to further appraise this modelling approach . 6 months after our model assumes that disruptions due to the covid - 19 pandemic will affect timely access to routine and urgent diagnostic services and alter health - seeking behaviour for a 12 - month period . 
these assumptions are likely given the changes in patterns of patient presentation and availability of diagnostic services observed since the start of lockdown.1 , 11 , 12 , 24 , 25 since beginning our modelling study , substantial reduction in 2 - week - wait referrals have indeed been seen in the first 3 months , as we predicted in scenarios b and c . 
given the ongoing reductions in the volume of 2 - week - wait referrals ( estimates suggest a 4050% reduction ) , 35 reductions are expected to continue for up to 6 months as predicted in scenario c because of the effects of pandemic lockdown measures on patients presenting to their gp or health - care provider . 
 these measures include advice to minimise non - essential travel and the continued shielding of high - risk groups.1 , 12 cancer research uk has estimated that the first 10 weeks of the uk lockdown has already resulted in 21 million deferred cancer screening investigations with 290 000 fewer people being referred on 2 - week - wait pathways.35 the implementation of physical distancing mea sures the backlog of patients with potential cancers awaiting investigation will be considerable , and health - care presentations will continue to be affected due to physical distancing measures that are expected to continue until 2021.11 , 12 additionally , nhs hospital trusts suspended their routine diagnostic services at the start of lockdown , which is concerning because routine referral routes account for 3040% of cancer diagnoses and the backlog in this pathway once routine services restart will include all patients still awaiting diagnostic investigations both from before and after lockdown started . 
further competition for capacity will subsequently come from the increase in new referrals for suspected cancers on 2 - weekwait referrals and those referred for investigation or follow up of seemingly benign health conditions . 
at the same time , diagnostic capacity has decreased for some procedures due the increased time taken per case since the introduction of new infection control measures.36 together , all these factors will increase the likelihood of patients becoming symptomatic and presenting via 2 - week - wait referral or emergency pathways . 
alternatively , if or when patients are diagnosed through routine pathways , the likelihood of stage migration and associated worse prognosis due to delays in diagnosis is increased . our analysis used a retrospective population cohort , therefore , the predicted survival for patients as of 2020 presenting via the different referral pathways , even for patients with stage iv disease , has slightly improved37 in the past decade because of improvements in treatments and processes of care . 
however , our analysis focuses on 1032 vol 21 august 2020 articles treatment on survival during the differences in cancer deaths between two situations ( pre - pandemic and pandemic periods ) and not on the absolute numbers of cancer deaths . 
additionally , these estimates do not consider the impact of treatment delay or suboptimal the pandemic.22 the proportions of patients presenting through different referral pathways has changed over time , with decreasing proportions of patients presenting via emergency depart ments in the past decade , which might also affect our results.38 however , we consider the probable effect on the overall results to be small given the steady trajectories of improvements in patterns of presentation we have seen over the past 5 years.37 , 38 we did not analyse patients aged 85 years or older at diagnosis because competing events , such as deaths from other causes , are predominant in this population . 
 although delays in cancer diagnosis in older populations will lead to excess short - term cancer mortality , the effect on national population - levels is less likely to be affected . 
 furthermore , because we report survival up to 5 years after diagnosis , such an estimate is less reliable in patients aged 90 years and older . in the screening population , we recognise that not all patients diagnosed with breast cancer through this route would have progressed or developed symptomatic disease . 
for colorectal cancer , 10% of patients are diagnosed through the screening route , of whom 45% are diagnosed with stage iiiiv disease ( 70% stage iiiv ) compared with 6% diagnosed with stage iiiiv tumours through breast cancer screening ; hence , we showed that more patients with colorectal cancer are diagnosed with advanced disease at screening compared with those diagnosed with breast cancer . 
overdiagnosis and overtreatment are not specific concerns associated with the bowel screening programme , 39 whereas they are concerns associated with breast screening , and the suspension of the bowel screening programme is likely to result in delayed presentation and stage migration if cancers remain untreated.40 our model also considered the english nhs as a whole , and therefore assigned blanket reallocation across the country . 
however , we recognise that variation is probable across the country in terms of gp access , the burden of covid - 19 , and the extent of discontinuation of critical diagnostic services in secondary care settings . 
 in this regard , we acknowledge that 2 - week - wait referrals have not decreased uniformly by 80% across all tumour types and uk regions , as per our estimations in scenarios b and c . 
additionally , variation will exist in the recovery of services across regions and individual hospitals , which are not included in our estimations . in summary , we estimated that changes in healthseeking behaviour and the availability of and access to essential diagnostic services resulting from national pandemic measures will result in a large number of additional deaths from breast , colorectal , lung , and oesophageal cancer in the medium ( 1 year ) and longer term ( 5 years )  . 
our study results do not consider the effect of delay on other cancer types , or the additional effect of changes in treatment pathways for these cancers that are likely to substantially increase the expected avoidable deaths beyond what we have estimated . 
these interventions should focus on increasing routine diagnostic capacity through which up to 40% of patients with cancer are diagnosed , public health messaging that accurately conveys the risk of severe illness from covid - 19 versus the risks of not seeking healthcare advice if patients are symptomatic , and the provision of evidence - based information for clinicians to adequately manage the risks of patients to the risk and benefits of procedures during the pandemic . contributors aa , mm , en , rs , and br conceived and designed the study . 
cm , js , mm , ap , en , rs , br , and aa were involved in reviewing and editing drafts of the paper and approving the manuscript . declaration of interests we declare no competing interests . data sharing this study was based on english national cancer registry data . 
we do not own these data and hence are not permitted to share them in the original forthe data are available from the office for data release at public health england . 
cm and br are funded through the cancer research uk population research committee funding scheme : cancer research uk population research committee programme award ( c7923 / a20987 and c7923 / a29018 )  . 
js is supported by the nihr biomedical research centre based at guys and st thomas nhs foundation trust and kings college london ( is - brc - 1215 - 20006 ) , and the cancer research uk kings health partners centre at kings college london ( c604 / a25135 )  . 
the views expressed in this publication are those of the authors and not necessarily those of the nhs , the national institute for health research , or the department of health and social care . in china ( nct03739944 ) , which will enrol 700 patients allocated to laparoscopic radical hysterectomy or trachelectomy , or laparotomic radical hysterectomy or trachelectomy . 
both studies have planned to assess the long - term evaluation of quality of life , the results of which will hopefully provide relevant findings . we declare no competing interests . * gabriella ferrandina , giacomo corrado , giovanni scambia gabriella.ferrandina@gmail.com fondazione policlinico universitario a gemelli , irccs , uoc di ginecologia oncologica , dipartimento per la salute della donna e del bambino e della salute pubblica , rome , italy ( gf , gc , gs ) ; and universit cattolica del sacro cuore , istituto di ginecologia e ostetricia , rome 00168 , italy ( gf , gs ) frumovitz m , obermair a , coleman rl , et al . 
quality of life in patients with cervical cancer after open versus minimally invasive radical hysterectomy ( lacc ) : a secondary outcome of a multicentre , randomised , open - label , phase 3 , non - inferiority trial . 
the lacc trial : has minimally invasive surgery for early - stage cervical cancer been dealt a knockout punch ? int j gynecol cancer 2018 ; 28 : 124850 . impact of the covid - 19 pandemic on the symptomatic diagnosis of cancer : the view from primary care the entire landscape of cancer management in primary care , from case identification to the management of people living with and beyond cancer , is evolving rapidly in the face of the coronavirus disease 2019 ( covid - 19 ) pandemic.1 in a climate of fear and mandated avoidance of all but essential clinical services , delays in patient , population , and health - care system responses to suspected cancer symptoms seem inevitable . screening , case identification , and referral in symptomatic cancer diagnosis have all been affected by the covid - 19 pandemic . 
uk national cancer screening programmesaccounting for approximately 5% of all cancer diagnoses each yearhave been suspended.2 consequently , early diagnoses from screening will be delayed and symptom - based diagnosis of cancer will become more important.3 unfortunately , postponing screening sends a message to the public and primary care that cancer can wait . timely presentation to primary care of patients with symptoms is driven by a combination of appraising symptoms as warranting attention , perceived or actual ability to consult a health - care professional , perceived consequences of seeking help , and priority over competing goals.4 it is probable that patients with well recognised red flag symptoms , such as a new lump or rectal bleeding , will continue to present to primary care . 
 with covid - 19 at the forefront , however , vague cancer symptoms such as fatigue , change in bowel habit , and weight loss might be dismissed by the patient as trivial.5 respiratory symptoms , including persistent cough , might be attributed to covid - 19 and not acted on . 
 patients might be reluctant to present because of fear of interacting with others , limited capacity to use video or teleconsultations , and concerns about wasting the doctors time.6 , 7 for family doctors , the covid - 19 pandemic affecting all aspects of normal working life , including a reduced workforce due to illness and self - isolation , and the reduced availability of appointments and investigations in primary and secondary care . 
remote consulting might also be less suited to vulnerable patients and individuals low socioeconomic backgrounds than to patients from high socio economic settings , compounding inequalities already apparent in early cancer diagnosis.8 if patients with cancer symptoms from published online april 30 , 2020 s1470 - 2045 ( 20 ) 30242 - 4 for more on the challenges of cancer care during the covid - 19 pandemic see editorial lancet oncol 2020 ; 21 : 603 for more on the impact of covid - 19 on cancer diagnosis see comment page 750 748 vol 21 june 2020 comment do present to primary care , there is no consensus on how they should be managed during the pandemic , or safety - netted . 
when patients are referred , they are likely to be triaged or delayed.9 for example , the cancellation of all but emergency endoscopy will inevitably prolong the time to diagnosis of gastrointestinal cancers . management and follow - up of patients with cancer is also affected by the covid - 19 pandemic . 
many patients with cancer , especially those under going chemotherapy , radical radiotherapy , and immuno therapy , are at greater risk from the symptoms and sequelae of covid - 19 . 
the national health service guidelines state that patients will want to discuss whether the benefits of continuing active cancer treatment outweigh the risks of potentially being seriously unwell if they contract covid - 19 , which is a role that could well fall to primary care.9 the uk cancer charity macmillan cancer support reports that a quarter of calls to its support line are from patients with cancer who are anxious about covid - 19.10 although cancer charities provide a vital support role , primary care needs to support the physical and mental health of patients for whom potentially lifesaving cancer treatments are being postponed . cancer treatments are a priority in the healthcare system , but as health - care become increasingly occupied with caring for patients with covid - 19 , these patients will inevitably take precedence . 
in this situation , the psychological effect on patients and clinical staff will be enormous . the covid - 19 pandemic has implications for primary care and the crisis has highlighted potential solutions for dealing with future global health threats . 
if done well , remote consulting could benefit previously underserved patient populations ( ie , individuals living in remote areas )  . behavioural interventions to encourage the timely symptomatic diagnosis of cancer are important . 
public awareness campaigns should signal that early helpseeking is welcome and legitimate , and might use social media and community networks that have grown in response to covid - 19 . 
clinicians should be aware of so - called diagnostic overshadowing from covid - 19 and remember that patients might have markedly delayed presentation already and need additional support navigating the next steps in terms of their referral and safety - netting . if cancer is suspected , clinicians should not be deterred from referring patients urgently because of covid - 19 or other future global health threats . 
 biomarker and machine - learning approaches might support prioritisation of patients who are at greatest risk , diverting health - care resources towards managing patients who are seriously ill . when patients are diagnosed with cancer , or are living with or beyond cancer , providers of primary care might have to accept enhanced roles in supporting decisions on cancer treatment , palliative care , and advanced planning around resuscitation and preferred places of care . when normal service resumes at a population and health - service level , there will be a huge backlog of patients with potential cancer symptoms needing urgent assessment . 
this research is linked to the cantest collaborative , which is funded by cancer research uk ( c8640 / a23385 ) , of which rdn is an associate director and ses is a co - investigator . 
differences in cancer awareness and beliefs between australia , canada , denmark , norway , sweden and the uk ( the international cancer benchmarking partnership ) : do they contribute to differences in cancer survival ? brit j cancer 2013 ; 108 : 292300 . llanwarne n , newbould j , burt j , campbell jl , roland m . 
covid - 19 and long term conditions : what if you have cancer , diabetes , or chronic kidney disease ? bmj 2020 ; 368 : m1174 . fewer cancer diagnoses during the covid - 19 epidemic in the netherlands published online april 30 , 2020 s1470 - 2045 ( 20 ) 30265 - 5 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on may 4 , 2020 for more on the challenges of cancer care during the covid - 19 pandemic see editorial lancet oncol 2020 ; 21 : 603 for more on the impact of covid - 19 on cancer diagnosis see comment page 748 see online for appendix the dreadful consequences of coronavirus disease 2019 ( covid - 19 ) put an unprecedented pressure on health - care services across the globe.1 the netherlands , a country with 174 million inhabitants that provides its citizens with universal access to essential healthcare serviceswith the general practitioner as the gatekeeper to secondary careis no exception in this regard . the first patient with covid - 19 in the netherlands was confirmed on feb 27 , 2020 , in the southern part of the country.2 thereafter , the disease spread rapidly throughout the country . 
subsequently , strict social distancing policies were implemented by the dutch government as of march 15 , 2020 , to mitigate the spread of covid - 19.3 , 4 all sites ( excluding skin cancer ) skin cancers ( excluding basal cell carcinoma ) first conrmed case of covid - 19 in the netherlands nationwide implementation of strict social distancing policies and temporary halt of national cancer screening programmes public awareness campaign about lesser cancer diagnoses 39% 40% 6 jan 13 jan 20 jan 27 jan 3 feb 10 feb 17 feb 24 feb 2 m arch 9 m arch 16 m arch 23 m arch 30 m arch 6 april calendar week in 2020 figure : number of cancer diagnoses by week in the netherlands in the period between jan 6 , 2020 ( calendar week 2 ) and april 12 , 2020 ( calendar week 15 ) basal cell carcinoma of the skin is not included in the statistics . 
the point estimates for the change in cancer diagnoses per calendar week are based on the mean total number of cancer diagnoses in the calendar weeks from 2 to 8 ; that is , the period before the covid - 19 outbreak in the netherlands . 
data from the nationwide netherlands cancer registry in the period between feb 24 , 2020 , and april 12 , 2020which are based on initial case ascertain ment through pathological cancer notifications from the nationwide network of histopathology and cytopathologyshow that there is a notable decrease in cancer diagnoses when compared with the period before the covid - 19 outbreak . 
this effect was most pronounced for skin cancers ( figure ) and observed across all age groups and geographical regions , and almost all cancer sites ( appendix )  . 
first , individuals with potential , non - specific symptoms of cancer might have barriers to consulting a general practitioner , including moral concerns about wasting the general practitioners time for non - covid - 19 - related symptoms , assumptions about insufficient capacity for essential noncovid - 19 - related health - care services , and anxiety about acquiring covid - 19 in a health - care setting . 
a general practitioner might , therefore , postpone initial investigations for symptoms that do not immediately hint towards a potential cancer diagnosis , resulting in delayed or postponed hospital referrals . 
third , hospitals might have postponed diagnostic evaluation or have longer turnaround times for diagnostic evaluation because many hospital - based resources are being allocated to tackle covid - 19 . 
lastly , national screening programmes for breast , colorectal , and cervical cancer are temporarily halted as of march 16 , 2020 , to alleviate the demand on the health - care system due to covid - 19 . 
 750 vol 21 june 2020 comment for more on euromonitors data on vaping see euromonitor.com / growthvapour - products for more on pulmonary illness and e - cigarette use in illinois and wisconsin see nejm.org / doi / full / 10.1056 / nejmoa1911614 for more on the cdc warning about lung illness and e - cigarette products see basic_information / e - cigarettes / severe - lung - disease.html for the lancet oncologys 2018 editorial on vaping see editorial lancet oncology 2018 ; 19 : 1543 for the fda letter to juul labs see inspections - complianceenforcement - and - criminalinvestigations / warning - letters / juul - labs - inc - 590950 - 09092019 vaping - related lung illnesses : time to act by 2021 , euromonitor , a strategic market research provider , estimates that 55 million people worldwide will regularly vape , with the usa being the largest consumer . 
however , a study by jennifer layden and colleagues published in the new england journal of medicine on sept 6 , 2019 , challenges the biggest of these misconceptions by providing more evidence linking pulmonary illness to e - cigarette use adding to the number of reported cases , which now stands at more than 200 in 25 us states since june , 2019 . this new study reports on 53 patients identified as part of a pulmonary disease cluster in the states of wisconsin and illinois . 
the most common respiratory symptoms at presentation were shortness of breath , cough , and chest pain along with gastrointestinal including nausea , vomiting , diarrhoea , symptoms and abdominal pa 48 patients had an abnormal chest radiograph showing complications such as pneumo mediastinum , pleural effusion , or pneumothorax . 
given the plausibility of the connection between these symptoms , the increasing number of cases nationwide , and the patients vaping behaviours , the us centers for disease control and prevention have warned that there might be a link to street - bought , illegal products , and advised that people should only buy vaping paraphernalia from official outlets and seek immediate medical attention if they have any health concerns . 
reflecting on the evidence so far , although a definitive cause - and - effect association has yet to be proven , the rising frequency of lung disease in e - cigarette lung cancer users must now trigger a far higher concern level for policy makersparticularly because the connection between many of these lung conditions and future development in a 2018 lancet oncology editorial , we called for a new , broader set of measures in the who framework convention on tobacco control . 
 a broader remit for the who framework convention on tobacco control would ensure that measures are in place internationally to prevent the us findings from becoming a global epidemic and enable more restrictive regulation around marketing of vaping products to prevent deceitful or misleading practices by vape manufacturers . 
for example , in a letter on sept 9 , 2019 , the us food and drug administration wrote to juul labs ( san francisco , ca , usa ) criticising them for illegally marketing their e - cigarettes as less harmful than regular cigarettes and instructing the company to make immediate corrections or face enforcement actions . 
this letter followed previous testimony to a house oversight and reform subcommittee into juuls marketing and promotion practices , which accused juul of using a sophisticated program to target children and teenagers , including at schools and summer camps . 
ironically , the usa remains one of the few nations worldwide that has yet to ratify the who framework convention on tobacco control , so even with an extended remit , the framework convention could not be used to help bolster efforts by us authorities and health practitioners . in 1610 , sir francis bacon noted that tobacco smoking seemed to be highly addictive and was a tough habit to quit . 
with vaping increasing at an unprecedented rate , we need to act swiftly to ensure we do not blunder in to another longrunning unhealthy , life shortening , odyssey of replacing one bad habit with another . 
 the lancet oncology vol 20 october 2019 1327 editorial global elimination of cervical cancer is achievablewith commitment on sept 6 , 2019 , who called on countries in the southeast asia region to accelerate their efforts towards cervical cancer elimination . 
improvements in screening , diagnosis , and treatment are urgently needed , but widespread vaccination against human papillomavirus ( hpv ) will have the largest effect towards eliminating the disease . a modelling study published in the lancet oncology showed that if hpv vaccination and screening are quickly implemented in low - income and middle - income countries ( lmics ) , 125134 million cervical cancer cases could be avoided by 2069 . 
in the lancet public health , researchers showed how a national immunisation scheme with early adoption and high coverage , along with a national hpv screening programme , was on track to eliminate cervical cancer in australia ( < 4 cases per 100 000 by 2028 and < 1 case per 100 000 by 2066 )  . 
 crucially , long - term maintenance of these programmes , with support from the government and communities , would be required to sustain low cervical cancer incidence and mortality . among countries in south - east asia , bhutan , maldives , sri lanka , and thailand have introduced national hpv vaccination ; however , one glaring omission is india , which has the largest population in the region . 
in this issue of the lancet oncology , rengaswamy sankaranarayanan and colleagues highlight barriers to implementing a national hpv vaccination programme in india and the status of prevention efforts there . 
although the hpv vaccine was licensed in india in 2008 , state government - sponsored vaccination pro grammes in the states of andhra pradesh and gujarat and a clinical trial were suspended in 2010 after the deaths of several girls who were vaccinated . 
 despite evidence refuting a causal link between the deaths and the vaccine , and against recommendations from the indian national technical advisory group on immunisation , availability and uptake of the hpv vaccine has been severely hindered since then . 
moreover , because cervical cancer incidence has fallen in parts of india , arguments have been inappropriately made that vaccination and screening are not needed . similar to hpv vaccination , in south - east asia , only bhutan , indonesia , maldives , sri lanka , and thailand have widespread or national cervical cancer screening programmes . 
bangladesh is a lowresource country and this plan is an encouraging start , but whether it is ambitious enough to achieve cervical cancer control remains to be seen . reported even with high screening and vaccination coverage , cervical cancer elimination will take time , and substantial numbers of women will require treatment for the disease ; thus , improvements here are also needed . 
for example , to overcome costs of the hpv vaccine itself , both indian and chinese pharmaceutical companies are trialling generic hpv vaccines to provide more affordable alternatives to currently available formulations . national , publicly funded hpv vaccination programmes , high uptake of vaccination and screening , and access to high - quality diagnosis and treatment , are essential to tackle the global burden of cervical cancer . 
on june 29 , 2016 , biden convened a one - day summit at howard university ( washington , dc ) to bolster support for the programme , emphasising the urgent need to accelerate progress . 
the meeting , attended by hundreds of doctors , researchers , advocates , and patients , was part of a national day of action involving 270 events across the usa . 
so , what can we expect in the coming months and years ? bidens moonshot federal taskforce has big plans : more than 30 public and private sector initiatives were unveiled at the summit , including a new oncology center of excellence at the us food and drug administration ( fda ) to accelerate the development of new cancer therapies ; the redesign of the national cancer institutes ( nci ) cancer.gov portal to make clinical trial data more accessible to oncologists and patients ; the expansion of the ncis open access genomic data commons , providing access to cancer genome data from more than 32 000 patients ; and the creation of new publicprivate partnerships , including a collaboration between the nci , charities , and 2030 pharmaceutical and biotechnology companies to share data and expedite trials . 
the additional funds have yet to be realised or approved , but are anticipated to come from multiple sources : the government has asked congress for another $755 million in 2017 , of which $680 million will go to the nih and $75 million to the fda ; and $200 million in research funding over the next 5 years has been promised by the american cancer society . 
meanwhile , the escalating cost of cancer drugs is another nancial concern : at the summit , biden questioned why pharmaceutical companies have raised the prices of these drugs to astronomical levels since they rst entered the market . 
ironically , such partnerships might drive up drug prices further to maintain pro t margins . in the for accelerating on the other hand , such partnerships should also facilitate data sharingone of the main goals initiatives newly announced of moonshot . 
 partnership therapies , cancer 12 companies have promised to share data with each other and with academic and government researchers , focusing on developing biomarkers , disease modelling , rare cancer treatments , and encouraging trials of combination therapies . 
however , poor enforcement has meant that many research institutions , including those that receive vast government grants , do not adhere to this timescale , and some do not deposit their data at all . 
concerns about data - poaching make researchers reluctant to release data before publication and risk losing credit for their work , plus issues surrounding patient con dentiality also need careful consideration . 
in the coming months , in addition to attainment of su cient funding and the forging of e ective collaborations , careful steps should be taken and safeguards implemented to make sure that researchers feel that they can safely share trial data before publication . 
furthermore , it is vital not to take an overly reductionist view of cancer , and to ensure that other important components of the bigger picturesuch as prevention , universal access to current treatments , and e ective palliative and end - of - life careare not forgotten in the clamour for fashionable objectives . 
 patients were randomly assigned ( 1 : 1 ) to receive either postoperative cisplatin , doxorubicin , and methotrexate ( map ) or map plus ifosfamide and etoposide ( mapie ) using concealed permuted blocks with three strati cation factors : trial group ; location of tumour ( proximal femur or proximal humerus vs other limb vs axial skeleton ) ; and presence of metastases ( no vs yes or possible )  . 
the map regimen consisted of cisplatin 120 mg / m , doxorubicin 375 mg / m per day on days 1 and 2 ( on weeks 1 and 6 ) followed 3 weeks later by high - dose methotrexate 12 g / m over 4 h . 
the mapie regimen consisted of map as a base regimen , with the addition of high - dose ifosfamide ( 14 g / m ) at 28 g / m per day with equidose mesna uroprotection , followed by etoposide 100 mg / m per day over 1 h on days 15 . 
median follow - up was 621 months ( iqr 466766 ) ; 623 months ( iqr 469771 ) for the map group and 611 months ( iqr 465753 ) for the mapie group . 
event - free survival did not di er between treatment groups ( hazard ratio [ hr ] 098 [ 95% ci 078123 ] ) ; hazards were non - proportional ( p = 00003 )  . 
the most common grade 34 adverse events were neutropenia ( 268 [ 89% ] patients in map vs 268 [ 90% ] in mapie ) , thrombocytopenia ( 231 [ 78% in map vs 248 [ 83% ] in mapie ) , and febrile neutropenia without documented infection ( 149 [ 50% ] in map vs 217 [ 73% ] in mapie )  . 
mapie was associated with more frequent grade 4 non - haematological toxicity than map ( 35 [ 12% ] of 301 in the map group vs 71 [ 24% ] of 298 in the mapie group )  . 
 two patients died during postoperative therapy , one from infection ( although their absolute neutrophil count was normal ) , which was de nitely related to their map treatment ( speci cally doxorubicin and cisplatin ) , and one from left ventricular systolic dysfunction , which was probably related to mapie treatment ( speci cally doxorubicin )  . 
 one suspected unexpected serious adverse reaction was reported in the map group : bone marrow infarction due to methotrexate . interpretation euramos - 1 results do not support the addition of ifosfamide and etoposide to postoperative chemotherapy in patients with poorly responding osteosarcoma because its administration was associated with increased toxicity without improving event - free survival . 
ifosfamide with16 , 17 or without etoposide17 also has activity in this setting and when incorporated into the treatment of patients with metastatic disease seems to improve event - free survival.18 though uncontrolled studies suggested that changing therapy on the basis of histological response improves outcomes , 3 , 5 , 19 the e cacy of this strategy had not been tested in a randomised trial . we report the primary results for patients who had a poor response and were randomised to the euramos - 1 trial , a collaboration between the childrens oncology group ( cog ) , the cooperative osteosarcoma study group ( coss ) , the european osteosarcoma intergroup ( eoi ) , and the scandinavian sarcoma group ( ssg )  . 
we did this trial to assess whether the addition of ifosfamide and etoposide to standard postoperative map would improve event - free survival in patients whose primary tumour showed a poor response to preoperative map . methods study design and participants euramos - 1 was an open - label , international , randomised , phase 3 , controlled trial . 
the main eligibility criteria for registration included having high - grade localised or metastatic extremity or axial osteosarcoma deemed resectable by the treating team , research in context evidence before this study osteosarcoma is a rare disease but is the most common bone tumour in children and adolescents and is associated with high mortality . 
before the euramos - 1 trial started , there has never been a study randomising patients with osteosarcoma following surgery to add chemotherapy to the preoperative backbone , and a formal literature review was not possible . 
through collaborations and pubmed searches , we were aware of the relevant publications in osteosarcoma which were about importance of histological response and use of ifosfamide in treating patients with a poor histological response . 
patients who have a poor response to chemotherapy ( 10% viable tumour ) have a substantially worse survival than those with a good response ( < 10% viable tumour ) with 5 - year overall survival of around 4555% and 7580% , respectively . 
therefore , no previous study has assessed in a randomised comparison whether adding an ifosfamide containing combination to standard treatment improves the outcome for patients identi ed as having a poor histological response . added value of this study randomisation of patients with a poor response in euramos - 1 trial represents a large , international comparison , with patients registered at the start of treatment and randomly assigned after surgery . 
patients were also required to have a serum bilirubin concentration of at most less than 15 times the upper limit of normal and a normal creatinine concentration for their age as per protocol . 
 the main eligibility criteria for randomisation were registeration before de nitive surgery to take part in euramos - 1 ; assessment of histological response in the primary tumour and randomisation within 35 days of de nitive surgery ( assessment by reference pathologist where possible ) ; age 5 years or younger at biopsy for patients with good response ; provision of all essential data ( entry form , preoperative chemotherapy forms , surgery , and pathology report ) ; receiving exactly two courses of cisplatin and doxorubicin , at least two courses , and no more than six courses of methotrexate ; macroscopically surgical resection of the primary tumour ; no evidence of local disease progression ; recovery from previous therapy allowing administration of post operative chemotherapy as planned ; no progression of metastatic disease or new metastases and removal of metastases ( in patients with metastatic disease at registration ) done or deemed feasible ( to be done after primary surgery ) ; macroscopically complete surgical resection of the primary tumor ; and written consent to participate in the study . 
 the data was collected in each data centre ( cog , coss , eoi , and ssg ) and transferred periodically to the coordinating data centre ( medical research council clinical trials unit )  . 
 before enrolment , all institutions were required to have obtained all regulatory and ethics approvals in accordance to their national , and for european centres , european rules and regulations , as mentioned in the protocol . 
 the protocol is available online . complete randomisation and masking patients were randomly allocated ( 1 : 1 ) to receive either map or map plus ifosfamide and etoposide ( mapie )  . 
 treatment allocation was done with centralised implementation of concealed random permuted blocks with three strati cation factors : trial group , location of tumour ( proximal femur or proximal humerus vs other limb vs axial skeleton ) , and presence of metastases ( no vs yes or possible )  . 
metastases were de ned as at least three lesions bigger than 5 mm or a single lesion bigger than 1 c patients with lung lesions not meeting these criteria were classi ed as having possible metastases . 
each treating institution was responsible for enrolling their patients into the trial , and patients were assigned to interventions using the medical research council clinical trials unit randomisation system ( for coss , eoi , and ssg sites ) and the cog randomisation system ( for cog sites )  . 
patients and investigators were not masked to treatment allocation . infusion intravenous procedures baseline assessment required a complete blood count , complete set of chemistry test data ( including liver and kidney function ) , a baseline echocardiogram and hearing test , imaging with an mri of the primary site , and a chest ct scan and a bone scan ( a pet scan could be used instead )  . 
all patients received preoperative therapy with map20 ( appendix p 10 ) for 10 weeks consisting of cisplatin 120 mg / m ( 4 h infusion of 60 mg / m per day for 2 days in cog sites ; continuous 72 h in other sites ) and doxorubicin 375 mg / m per day on days 1 and 2 ( on weeks 1 and 6 )  . 
this was followed by high - dose methotrexate 12 g / m over 4 h ( maximum dose 20 g at cog institutions ) with hyper - hydration , alkalinisation , and standard leucovorin rescue at a dose of 15 mg / m starting 2448 h from methotrexate infusion and continuing until methotrexate concentration was less than 01 m ( weeks 4 , 5 , 9 , and 10 ) .20 , 21 leucovorin rescue was adjusted with the dosing nomogram according to the methotrexate concentration . 
 to begin myelosuppressive cycles , patients needed an absolute neutrophil count of at least 750 cells per l and a platelet count of at least 75 000 platelets per l . 
 criteria for administering high - dose methotrexate were di erent and included an absolute neutrophil count of at least 250 cells per l and a platelet count of at least 50 000 platelets per l . patients were restaged at 10 weeks preoperatively ( with the same imaging studies done at diagnosis ) and investigator - assessed response was reported according to response to treatment in solid tumors ( recist ) criteria , version 1 . 
eligibility for postoperative randomisation included macroscopic tumour resection , at least 10% morph ologically viable tumour , no disease progression , no or resectable metastases , and ability to resume therapy within 35 days after surgery . 
 2260 patients were registered 1200 patients were not poor responders 1060 patients were poor responders 442 excluded 204 did not provide consent 111 had progression ( local or distant ) 45 late histology 31 had incorrect preoperative ct 16 no removal of metastasis or unresectable disease 7 had not recovered from prior therapy 6 had a change in diagnosis 5 had incomplete resection of primary tumour 17 other 618 patients were randomly assigned * 310 assigned to receive map ( intention - to - treat population ) 308 assigned to receive mapie ( intention - to - treat population ) 8 did not receive map 4 treatment refusal 1 protocol violation 1 not in patients best interest 2 lost to follow - up 8 did not receive mapie 5 treatment refusal 2 protocol violation 1 not in patients best interest 302 started map treatment 300 started mapie treatment 1 not assessed for toxicity 2 not assessed for toxicity 301 assessable for toxicity ( safety population ) 298 assessable for toxicity ( safety population ) 40 terminated treatment early 8 treatment refusal 20 disease progression or recurrence 3 excessive toxicity 6 not in patients best interest 1 death 2 other 87 terminated treatment early 36 treatment refusal 21 disease progression or recurrence 16 excessive toxicity 7 not in patients best interest 1 lost to follow - up 1 death 5 other 261 completed map treatment 211 completed mapie treatment figure 1 : trial pro le * we later found out that one patient actually had a good histological response ( allocated to map group at randomisation and analysed as in the map group )  . 
 imaging recommendations during treatment included a chest ct , a bone scan , and a plain radiograph of the primary tumour at 4 - month intervals . cisplatin , doxorubicin , and methotrexate were administered at the same doses as given preoperatively . 
 ifosfamide ( high dose 14 g / m ) at 28 g / m per day with equidose mesna uroprotection was administered , followed by etoposide 100 mg / m per day over 1 h on days 15 ( three postoperative cycles )  . 
two additional cycles of ifosfamide 3 g / m per day with mesna uroprotection on days 13 ( 9 g / m ) were given , with standard doxorubicinvestigators were allowed to use supportive care with myeloid growth factor support according to local practice . 
 patients treated with map received 29 weeks of treatment or four cycles of map and two cycles of methotrexate and doxorubicin ( cisplatin was discontinued after a cumulative dose of 480 mg / m )  . 
the protocol provided recommendations for dose reductions on the basis of the toxicity ( from the common toxicity criteria ) and therapy delays . outcomes the primary outcome measure was event - free survival , de ned as the time from randomisation until rst event ( local recurrence , evidence of new or progressive metastatic disease , second malignancy , death , or a combination of those events ) or censoring at last contact . 
 secondary outcomes were overall survival ( de ned as the time from randomisation until death from any cause or last contact ) , short - term and long - term toxicity , and quality of life . 
questionaires were administered at baseline ( before cycle 2 ) , at week 2022 ( on active treatment ) , 18 months after start of treatment , and 3 years after starting treatment . 
 table 1 : baseline characteristics 1400 vol 17 october 2016 the treatment e ect was estimated separately in the prespeci ed localised disease subgroup , and in the following subgroups de ned post hoc : sex , age , site of disease , location of cancer on bone , and baseline metastases ( lung and non - lung )  . 
 01 02 this number was increased to more than 2000 registered patients overall , after the observed randomisation rate was lower than anticipated.19 the study required at least 378 event - free survival events and at least 378 deaths to detect absolute improvements of 10% from 45% to 55% in 3 - year event - free survival and 5 - year overall survival ( hazard ratio [ hr ] 075 ) with 5% two - sided signi cance levels and 80% power.24 the estimated sample size was calculated with the george and desu method , and although this number of events was not reached , the independent data monitoring committee recommended early release of data because of the lower than predicted event rate and low likelihood that the planned number of events would be reached in a reasonable time . 
 a preplanned subgroup analysis for patients with localised disease required 270 events to detect an 11% improvement , from 50% to 61% ( hr 071 ) in 3 - year event - free survival , and 5 - year survival ( two - sided signi cance level 5% , power 80% ) , assuming 85% of randomised patients would have localised disease ( 590 patients expected )  . primary and secondary outcomes were measured in the intention - to - treat population . 
the kaplan - meier method was used to estimate survival functions , log - rank test for di erences between survival curves and cox models ( adjusted for strati cation factors ) to estimate the treatment e ect . 
the haybittle - peto stopping rule was used , and the trial was planned to stop if the p value for the event - free survival analysis was less than 0001 . 
the interim analyses were designed to examine safety of the patients , and therefore the protocol prespeci ed that if at interim analysis , the lower bound of the 95% ci for the proportion of patients in each group who died because of toxicity exceeded 3% , the future of the trial would be discussed with the trial steering committee . the the proportionality of hazards for the treatment e ect over time was tested . 
in the presence of non - proportionality , the di erence between the groups was estimated with restricted mean survival time ( rmst ) 25 , 26 after tting a exible parametric model . 
 rmst for event - free survival measures a mean time - torst event , when time of consideration was restricted to t * years after randomisation ; here t * was 6 years . 
the consistency of treatment e ect in patients with localised or metastatic disease was tested by tting a exible parametric model with interaction between allocated treatment and metastases . vol 17 october 2016 1401 articles metastases , progression of existing metastases , death , or a combination of those events were considered a competing event for reporting second malignancy . 
 role of the funding source the funders of this study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 the corresponding author had full access to all data in the study and all authors had nal responsibility for the decision to submit for publication . results between april 14 , 2005 , and june 30 , 2011 , 2260 patients were registered until the overall recruitment target was reached . 
 618 patients were randomly assigned from the poor responders group : 310 to receive map and 308 to receive mapie ( gure 1 ) ; this was lower than the anticipated target of 693 . 
 median trial population was 621 months ( iqr 466766 ) ; 623 months ( iqr 469771 ) for the map group and 611 months ( iqr 465753 ) for the mapie group . 
for patients last reported alive and not lost to follow - up , 325 ( 87% ) of 373 had follow - up within 14 months before the data freeze . 
29 ( 9% ) of 310 patients in map and 23 ( 7% ) of 308 patients in mapie were permanently lost to follow - up more than 14 months before the data freeze . the entire follow - up for 307 event - free survival events were reported : 153 in the map group and 154 in the mapie group . 
the hr for event - free survival comparison in mapie versus map the was 098 ( 95% ci 078123 , p = 086 ) , but proportionality of hazards assumption did not hold mapie ( p = 00003 ) ; therefore , we estimated event - free survival with the rmst approach . 
mean time to rst event was 433 months ( 95% ci 401464 ) for patients allocated to the map group , and 441 months ( 411471 ) for patients allocated to the mapie group , over a period of 6 years from randomisation . 
 involved in both groups , metastases133 ( 87% ) of 153 patients in the map group and 129 ( 84% ) of 154 patients in the mapie group . the rst event mostly 247 event - free survival events were reported 541 patients with localised disease at the time of registration ( 118 in the map group and 129 in the mapie group ; gure 2 )  . 
3 - year event - free survival estimates in localised disease were 60% ( 95% ci 5466 ) in the map group and 57% ( 5163 ) in the mapie group . 
the hr was 103 ( 081133 , p = 080 ) but with considerable non - proportionality estimated rmst between the mapie and map groups was 005 months ( 47 to 48 ; p = 098 ; gure 2 )  . 
3 - year event - free survival in patients who had metastases at registration was 24% ( 1338 ) in the map group and 18% ( 633 ) in the mapie group . 
 received details of standardised postoperative chemotherapy doses , the number of patients who received the target number of chemotherapy doses , and the number of patients who received at least 80% of the planned dose are shown in table 2 . 
of the 77 patients with metastases at registration , 75 of 77 either had resection or resection was no longer needed and two of 75 were not operated on ( one in the mapie group due to clinicians and patients choice group vs one in the map group who was inoperable )  . toxicity data are available for 301 ( 997% ) of 302 map and 298 ( 993% ) of 300 patients in the mapie group who started treatment ( table 3 ) , and the remaining three patients were not assessed for toxicity ( one in the map group and two in the mapie group )  . 
received cisplatin dose and number of cycles are not known for one patient . table 2 : summary of patients who received postoperative map and mapie the site and are taken into consideration when highest grade toxicity reported was determined ( table 4 )  . 
the grades of the toxicities recorded during postoperative chemotherapy were similar between di erent treatment groups : worst toxicity of grade 3 or above was reported by 287 ( 95% ) of 301 patients in map and 281 ( 94% ) of 298 in mapie group ( table 4 )  . 
mapie was associated with more frequent grade 4 non - haematological toxicity ( 35 [ 12% ] of patients in the map group vs 71 [ 24% ] of 298 patients in the mapie group ) , mainly because of infections with absolute neutrophil count of less than 1 10 neutrophils per l , febrile neutropenia without documented infection , and hypophosphataemia ( table 4 )  . 
two patients died during postoperative therapy , one due to infection although they had a normal absolute neutrophil count ( map group ) , and one due to left ventricular ( mapie group )  . 
dose was reduced or delayed according to criteria in the protocol for 176 ( 58% ) of 301 patients in the map group and 184 ( 62% ) of 298 patients in the mapie group . 
three patients were not assessed for dose reduction or delay , one in the map group and two in the mapie group . systolic dysfunction left ventricular systolic dysfunction grade 3 events were reported in three ( 2% ) of 134 patients in the mapie group and one ( 1% ) of 136 in the map group . 
renal failure grade 3 ( four [ 3% ] of 138 patients ) and grade 4 ( one [ 1% ] of 138 patients ) events were reported in the mapie group but not in the map group . 
there was no consistent pattern of reversibility for left ventricular systolic dysfunction or renal events , as some patients improved , whereas others did not , but the number of events was too small to analyse further . 13 second primary malignancies were reported ( three in the map group vs ten in the mapie group ; appendix pp 5 , 6 )  . 
most of the second malignancies were myeloid ( myelodysplasia and acute myeloid leukaemia ) : two of three in the map group and eight of ten in the mapie group , mostly recording cytogenetic abnormalities causally associated with administration of alkylating drugs ( monosomy - 7 or chromosome - 5 abnormalities ) or etoposide ( 11q23 abnormalities )  . 
a longer follow - up will allow for more precise estimates . discussion standard treatment for high - grade osteosarcoma includes preoperative chemotherapy followed by surgical resection and postoperative chemotherapy.14 , 8 although previous uncontrolled studies3 , 5 , 19 suggested that altering therapy on the basis of histological response improved outcome , this had not been tested in randomised controlled trials . 
 euramos - 1 is , to the best of our knowledge , the rst collaboration to assess in a randomised manner whether altering chemotherapy on the basis of histological response improves outcome for patients with osteosarcoma . 
our results for patients with a poor histological response show that the addition of ifosfamide and etoposide to standard postoperative therapy does not improve outcome and rather increases the incidence of toxic e ects . 
 bilirubin data was collected by the cooperative osteosarcoma study group , the european osteosarcoma intergroup , and the scandinavian sarcoma group sites only . table 3 : postoperative treatment - related adverse events 1404 vol 17 october 2016 articles map ( n = 301 ) mapie ( n = 298 ) test p value * grade 3 grade 4 grade 5 total grade 3 or worse grade 3 grade 4 grade 5 total grade 3 or worse any toxicity 26 ( 9% ) 260 ( 86% ) non - haematological events 197 ( 65% ) 35 ( 12% ) 1 ( < 1% ) 1 ( < 1% ) 287 ( 95% ) 233 ( 77% ) 20 ( 7% ) 260 ( 87% ) 187 ( 63% ) 71 ( 24% ) 1 ( < 1% ) 1 ( < 1% ) 281 ( 94% ) 259 ( 87% ) p = 056 p = 00024 * comparison of grade 3 or higher toxicity . 
any toxicity , excluding neutropenia , thrombocytopenia , anaemia , and leucopenia . table 4 : summary of worst grade toxicity during postoperative chemotherapy chemotherapy a previous randomised controlled trial29 of around 240 patients assessed the addition of ifosfamide to standard map for patients with osteosarcoma . 
this trial included an upfront randomisation to map versus map plus ifosfamide , with postoperative ifosfamide given to those who had received it preoperatively or whose tumour showed a poor histological response ( < 90% necrosis )  . 
 on the basis of these data and our euramos results , we recommend continuing with the same chemotherapy as used preoperatively for patients with a poor histological response to preoperative treatment . 
 to preoperative map our results are also consistent with the results of a previous randomised controlled trial2 by the cog , which cog assessed the role of ifosfamide and mifamurtide in patients with osteosarcoma . 
the study assessed whether the addition of ifosfamide or mifamurtide to the map regimen improved long - term outcomes ; patients were treated preoperatively with either map or map plus ifosfamide , and subsequently postoperatively treated with or without mifamurtide . 
no di erence in histological response was observed after the preoperative period , and no di erence in event - free survival or overall survival was observed between the two chemotherapy groups . 
our results are also consistent with the conclusion of a meta - analysis30 where outcomes for osteosarcoma patients were improved with the use of at least three drugs , but no improvement was noted with the use of map plus ifosfamide versus map . lower euramos - 1 was complicated by a than anticipated randomisation rate , probably related to the timing of the randomisation , close to the time of the intervention , after patients had been exposed to signi cant treatment - related toxicities . 
non - randomisation was 42% in known poor responders and occurred in all four trial groups ( cog , coss , eoi , and ssg ) ranging between 33% and 45% . 
most as anticipated , a larger number of mapie - treated patients developed second malignancies than patients treated with map , although the di erence was not statistically second malignancies were myeloid in origin , which is not unexpected given the short follow - up and the natural history of therapy - related myeloid disorders.31 , 32 the cytogenetic abnormalities in some of these leukaemias were consistent with exposure to alkylating drugs32 and etoposide.33 although second solid malignancies are more common after combined modality therapy , including irradiation , 34 alkylating drugs also contribute to this risk . 
overall survival will additionally be analysed with longer follow - up . the number of events was lower than anticipated , as event - free survival results were based on 307 event - free survival events , rather than the planned 378 ; event rate was lower than predicted and our 3 - year event - free survival estimate for map was 55% ( 95% ci 4960 ) rather than 45% . 
therefore early imaging assessments might not have been identically timed by group , resulting in the apparent early separation observed in the event - free survival curve in favour of the mapie group . 
 the timing of our intervention might have been too late because the rst cycle of ifosfamide plus etoposide was administered at week 17 ( 5 weeks from resumption of postoperative therapy )  . 
 ultimately , the best strategy for patients with a poor histological response might not be therapy intensi cation since this approach has been unsuccessful in childhood soft tissue sarcomas35 and in a previous study in osteosarcoma.4 the use of functional imaging early during treatment might identify patients who will have a poor response and allow incorporation of alternative treatment strategies earlier . 
 we included patients with both initially localised and initially metastatic disease in the same trial because it was not always possible to di erentiate up - front between patients with localised disease and those with vol 17 october 2016 1405 articles metastatic disease , and we have therefore also included patients with possible metastatic disease ; other prognostic factors are the same in patients with both metastatic and localised disease . 
 the 3 - year event - free survival for patients with metastases was 24% ( 1338 ) in the map group and 18% ( 633 ) in the mapie group , and these results are similar to those of other published series.37 , 38 the euramos - 1 trial included only 77 patients with metastases , which makes it di cult to draw rm conclusions regarding the outcome for these patients . 
 additionally , since the euramos - 1 patients with metastases needed to have resectable disease , the population included might not be entirely comparable to those included in the previous trials . 
because the study question was whether altering therapy on the basis of histological response improved outcome , we do not think collection of those data is crucial to the study results overall . 
 this is a potential limitation especially because patients treated in the experimental group appeared to receive less of the intended therapy . increases review the addition of mifamurtide to the map chemotherapy regimen for patients with localised osteosarcoma resulted in improved overall survival.2 the drug was approved for use in europe on the basis of those results , but has not been approved for use in the usa . 
we have subsequently reached an apparent plateau in outcomes for patients with osteosarcoma.39 the development of strategies to better understand the biology of this tumour40 might aid in the identi cation of drug targets . 
collaboration with veterinary oncologists might speed up target identi cation in human beings as canine osteosarcoma is more common than human osteosarcoma.41 genome - wide analysis of osteosarcoma samples might also help identify important targetable genetic mutations.42 the identi cation of genetic alterations that could be used as therapeutic targets is an important step to develop better treatment approaches . overall , euramos - 1 showed that treatment with mapie resulted in similar event - free survival to map , results in increased toxicity , decrease in total received doses , and more second malignancies . 
 all authors collated data and interpreted the data , and reviewed and approved the nal manuscript . declaration of interests nmm reports personal fees from jazz pharmaceutical , outside the submitted work . 
ssb reports grants from deutsche krebshilfe , deutsche forschungsgemeinschaft , and european science foundation , during the conduct of the study ; personal fees from lilly , bayer , celgene , clinigen , chugai , merck , roche , takeda millenium / idm , and p zer , outside the submitted work . 
gj reports grants from cancer research uk , grants from medical research council uk , during the conduct of the study , and grants from cancer research uk , outside of the submitted work . 
jmh reports grants from cancer research uk , medical research council uk , during the conduct of the study ; and grants from cancer research uk , outside of the submitted work . 
tb - b reports grants from federal ministry of education and research , and other fees from the european science foundation under the eurocores program european clinical trials and deutsche forschungsgemeinschaft , during the conduct of the study . 
pjl reports other fees from childrens oncology group , during the conduct of the study and other fees from eleison 1406 vol 17 october 2016 articles pharmaceuticals llc , outside of the submitted work . 
mrs reports grants and nonnancial support from sano - aventis , novartis , p zer , janssen , and astellas , and nonnancial support from merck , all outside of the submitted work . 
lancet oncol 2019 ; 20 : 155665in this article , two patients ( one in the control group and one in the complete mesocolic excision group ) were incorrectly classified as not having recurrences , due to an error in data extraction . 
 the incorrect data have been updated in the summary findings , the results , figures 2a and 2c , table 3 , supplementary figures 2c and 2f in the appendix , and the discussion . 
complete mesocolic excision for colon cancer : is now the time for a change in practice ? lancet oncol 2019 ; 20 : 147476in this comment , the cumulative incidence of recurrence in each group has been amended , owing to these data being corrected in the linked article by bertelsen and colleagues . 
lancet oncol 2019 ; 20 : e658 in this correspondence , the absolute in risk of recurrence reduction has been amended , owing to this being corrected in the linked article by bertelsen and colleagues . 
this correction has been made to the online version as of aug 3 , 2020 . correction to lancet oncol 2020 ; 21 : e33036 cooney tm , cohen jk , guimaraes cv , et al . 
these corrections have been made to the online version as of aug 3 , 2020 . vol 21 august 2020 e372 corrections than likely , the success of surufatinib is attributable to both its novel mechanism of action and favourable business decisions around its development . 
we also need to study mechanisms of resistance to tyrosine kinase inhibitors , develop and validate predictive biomarkers , understand reasons for heterogeneity in objective response , and identify better quantitative radiological response criteria in the setting of angiogenesis inhibition . 
 given the chronicity of well differentiated nets , these patients will experience an accumulation of toxicities over years that include non - trivial drug side - effects , particularly with tyrosine kinase inhibitors . 
randomized phase ii study of everolimus ( e ) versus everolimus plus bevacizumab ( e + b ) in patients ( pts ) with locally advanced or metastatic pancreatic neuroendocrine tumors ( pnet ) , calgb 80701 ( alliance )  . 
med - plans - to - submit - surufatinib - nda - following - pre - nda - meeting - withfda / 2020 ( accessed sept 15 , 2020 )  . a roadmap for the early detection and diagnosis of cancer if we are to beat cancer , early detection and diagnosis are arguably the most effective means we have at our disposal . 
progress during the past 40 years has transformed the prospects of people diagnosed with cancer in the uk , with survival doubling since the 1970s.1 however , further improvements are still greatly needed , because cancer remains the leading cause of death in the uk , 2 with a stark projection of rising incidence to more than half a million cases per year by 2035.3 patients diagnosed with cancer at an early stage have the best chance of curative treatment and long - term survival ; for example , 57% of people with lung cancer survive their disease for 5 years or more when diagnosed at stage i compared with only 3% of those diagnosed at stage iv.4 despite cancer screening programmes , improved awareness , and more streamlined diagnostic pathways , only 54% of patients with cancer in england had their cancer detected at stage i or ii in 2018.5 with lower survival rates in the uk than in similar countries , such as australia , canada , or norway , 6 , 7 and notable inequalities in survival across the uk , 8 , 9 there is a pressing need to see a paradigm shift in our ability to accurately detect and diagnose cancer at an early stage . beyond the clear potential for health benefit , the uk has the capacity to be a world leader in developing a thriving early detection and diagnosis industry , capitalising on its excellent science base and vast national health service ( nhs ) and data infrastructure , and attracting global investment . 
this potential for health and wealth benefit is recognised by uks national governments , with ambitious targets set in nhs englands long term plan ( ie , a commitment to detect 75% of cancers at stage i and ii by 2028 ) and the scottish governments beating cancer strategy , 10 and investments to support progress in early detection and diagnosis ( eg , the accelerating detection of disease published online october 6 , 2020 s1470 - 2045 ( 20 ) 30593 - 3 for more on nhs englands long term plan for cancer see cancer / strategy / vol 21 november 2020 1397 comment for more on the accelerating detection of disease challenge see innovation / industrial - strategychallenge - fund / acceleratingdetection - of - disease for the early detection and diagnosis roadmap see org / funding - for - researchers / research - opportunities - in - earlydetection - and - diagnosis / earlydetection - and - diagnosisroadmap for more on the national artificial intelligence diagnostics lab see net / 2019 / 08 / government - 250million - artificial - intelligencelab - diagnostics / for more on the data to early diagnosis initiative see innovation / industrial - strategychallenge - fund / from - data - toearly - diagnosis - and - precisionmedicine / panel : key themes for action to deliver the roadmap understanding risk and prognosis , from biology to technology biomedical data science and systems incentivising and supporting development and commercialisation health - care system innovation and supporting adoption challenge , the national artificial intelligence diagnostics lab , and the data to early diagnosis initiative )  . the true potential of early detection and diagnosis largely unexploited globally due to many remains historical challenges . 
early detection research is a comparatively new and fragmented field with substantial barriers to achieving validation because of , for example , complex and unclear biology , a paucity of availability of quality samples , and insufficient funding for translation . 
 furthermore , corporate investment is scant because of the high cost of research and development ( eg , the requirement for expensive long - term studies to show beneficial effects on mortality ) , the low price point of diagnostics , undervaluing and underprioritisation of early detection and diagnosis by the health - care system , and complicated navigation of unclear regulatory and approval pathways . the multidisciplinary and multisectoral network needed for development and delivery of early detection and diagnosis is complex and fragmented , spanning academic research , industry , research funders , regu lators , investors , health - care professionals , nhs decision makers , government , andcruciallypatients and the public . 
without such a vision , progress has been slow . to unite the fragmented efforts of the early detection and diagnosis network , and to establish a pathway for early detection and diagnosis in the uk , cancer research uk consulted extensively with more than 100 expert stakeholders across a broad range of sectors to develop a roadmap for early detection and diagnosis of cancer . 
it highlights current challenges that are impeding progress and makes a series of tangible recommendations for research , development , health system delivery , and government policy on how to overcome these challenges and realise the shared vision ( panel )  . 
underlying every recommendation is a mandate to ensure early detection and diagnosis is delivered ethically , equitably , and transparently throughout the uk , with extensive involvement with patients and the public to reduce health inequalities . although this roadmap for early detection and diagnosis focuses on cancer , the future of health care lies not only in the effective treatment of symptomatic disease but also in health maintenanceie , a holistic , proactive approach to understanding disease risk , early detection of deviations away from health , and intervening appropriately , whatever the disease . 
 cancer acts as an example to establish technologies and approaches that will deliver benefit across a range of disease areas , incorporating disease prevention via interception of predisease , further underscoring the need for partnerships across the health network . 
the early detection and diagnosis roadmap steering group are billy boyle ( owlstone medical , cambridge , uk ) , caroline dive ( university of manchester , manchester , uk ) , rebecca fitzgerald ( university of cambridge , cambridge , uk ) , george b hanna ( imperial college london , london , uk ) , sue hill ( nhs england , london , uk ) , david hunter ( oxford university , oxford , uk ) , sam janes ( university college london , london , uk ) , stan kaye ( royal marsden hospital , london , uk ) , harpal kumar ( grail , london , uk ) , karin oien ( university of glasgow , glasgow , uk ) , cally palmer ( royal marsden hospital ) , andy richards ( london , uk ) , mike richards ( nhs , london , uk ) , peter sasieni ( kings college london , london , uk ) , bob steele ( university of dundee , dundee , uk ) , and fiona walter ( university of cambridge )  . 
the early detection and diagnosis roadmap steering group provided consultation on the content of this comment . * david crosby , nicole lyons , emma greenwood , samantha harrison , sara hiom , jodie moffat , talisia quallo , emlyn samuel , ian walker , and the early detection and diagnosis roadmap steering group david.crosby@cancer.org.uk cancer research uk , london e20 1jq , uk quaresma m , coleman mp , rachet b . 
40 - year trends in an index of survival for all cancers combined and survival adjusted for age and sex for each cancer in england and wales , 19712011 : a population - based study . 
br j cancer 2016 ; 115 : 114755 . 1398 vol 21 november 2020 comment published online october 21 , 2020 s1470 - 2045 ( 20 ) 30592 - 1 office for national statistics . 
government / statistics / case - mix - adjusted - percentage - cancers - diagnosedat - stages - 1 - and - 2 - by - ccg - in - england ( accessed sept 24 , 2020 )  . arnold m , rutherford mj , bardot a , et al . 
government%202016%20cancer%20plan.pdf ( accessed sept 28 , 2020 )  . how current assay approval policies are leading to unintended imprecision medicine pathologists are responsible for selecting the assays for the optimal identification of patients for targeted therapy . 
the current paradigm of regulatory assay approval is that when a clinical trial involving a drug and a biomarker , using a specific assay to identify patients that might respond to the drug , meets its endpoint , the assay is approved concomitantly as a companion diagnostic . 
use of us food and drug administration ( fda ) - approved assays is obligatory in some countries , like the usa and japan , to gain access to the drug . 
in the eu , the use of an fda - approved assay is not mandatory to gain access to the drug , as long as the laboratory - developed test or assay that is used is validated . thresholds for defining a positive biomarker in a clinical trial , and what constitutes a positive biomarker , are not standardised . 
moreover , companion assays are co - developed with a drug , as determined by the pharmaceutical company in collaboration with the company contracted to produce the assay , without regard to the other assays being developed for the same biomarker . 
for example , pd - l1 assay kits are approved by the fda in 15 different cancer types but the pd - l1 staining patterns , scoring methods , and positivity thresholds are different in almost all of these cancer types . 
there are at least five nonequivalent assays for pd - l1 , each with its own scoring system and tumour site indications . absence of assay standardisation is an emerging issue for triple - negative breast cancer . 
in 2019 , considering the results of the impassion130 trial , the fda approved the ventana pd - l1 ( sp142 ) assay ( ventana medical systems , tucson , az , usa ) and cut - point ( 1% of tumour - infiltrating immune cells ) to assess pd - l1 in patients with triple - negative breast cancer treated with atezolizumab.1 however , following the keynote 355 breast cancer trial , 2 the results of which were publicised in 2020 , investigating pembrolizumab in the same patient population , the fda is likely to approve the pd - l1 ihc 22c3 pharmdx assay ( agilent technologies , carpinteria , ca , usa ) and its combined positivity scorescoring system to assess pd - l1 . 
in the impassion130 trial , 46% of patients with triple - negative breast cancer were deemed to be positive using the ventana pd - l1 ( sp142 ) assay ; when using other assays ( eg , the pd - l1 ihc 22c3 pharmdx assay ) in the same patients , the pd - l1 positive prevalence increased to nearly 80%.3 the cause of these inconsistencies is multifactorial and includes reproducibility issues and variable antibody and assay sensitivity , even when different assays use the same antibody.46 one issue is the balance of risk , costs , and benefit . 
if treatment recommendations differ depending on the assay that is used , it is difficult for health - care providers to reliably analyse the cost - effectiveness for reimbursement of that particular treatment . 
some private governments insist on the use of fda - approved assays , vol 21 november 2020 1399 comment inform advocacy the commonwealth charter can for greater funding for health . 
sufficient and sustainable health financing mitigates against social injustices and inequalitiesthey are therefore matters of human rights and the value of democracy . every nation will have a different process towards implementing universal health coverage and improved cancer control , yet international platforms , such as the commonwealth , create opportunities to work towards universal health coverage together . 
collaborative approaches can improve spending efficiency by minimising costs to health - care systems , obtaining a good return on investment in cancer services , optimising the workforce , and exploring procurement possibilities . commonwealth nations have made commitments to the promotion of universal health coverage and equity in cancer control . 
 the views expressed are those of the authors and not necessarily those of the institution with which they are affiliated . * andr ilbawi , gwenal dhaene , filip meheus , melanie bertram ilbawia@who.int department of noncommunicable diseases ( ai ) and department of health systems governance and financing ( gd , mb ) , world health organization , ch - 1211 geneva 27 , switzerland ; and section of cancer surveillance , international agency for research on cancer , lyon , france ( fm ) 2020 world health organization . 
report_2019.pdf ( accessed april 1 , 2020 )  . the role of the commonwealth in the wider cancer control agenda the number of new cases of cancer reported in the commonwealth nations rose by 35% between 2008 and 2018 . 
in 2018 , nearly 17 million people died from cancer in these countries : equivalent to one death every 18 seconds.1 estimates based on expected population growth predict a further 35% increase in incidence of cancer in the commonwealth in the next 12 years ( 201830 ) , and a 39% increase in cancer mortality.1 what should we expect the commonwealth to do about this worsening situation ? the core purpose of the commonwealth was affirmed by the commonwealth heads of government meeting ( port of spain , trinidad and tobago ) in the november , 2009 : we reaffirm our belief commonwealth as a voluntary association of sovereign influence independent states whose pursuit of common principles continues to international society to the benefit of all.2 it has long been the view of the head of the commonwealth that the commonwealth is not an organisation with a mission . 
it is rather an opportunity for its people to work together to achieve practical solutions to problems.3 where does this view leave population health care ? traditionally , this issue is low on the commonwealths list of priorities . 
access to health and education was ranked 10th of 12 core values listed in the 2009 affirmation.2 the influential 2011 report by the commonwealth eminent persons group to the commonwealth heads further discouragement.3 of government provides corrections correction to lancet oncol 2016 ; 17 : 416 correction to lancet oncol 2016 ; 17 : 456 correction to lancet oncol 2016 ; 17 : 541 randall l , cable mg . 
 this correction has been made to the online version as of april 26 , 2016 , and the printed version is correct . kim d - w , mehra r , tan dsw , et al . 
 activity and safety of ceritinib in patients with alk - rearranged non - small - cell lung cancer ( ascend - 1 ) : updated results from the multicentre , open - label , phase 1 trial . 
lancet oncol 2016 ; 17 : 45263 in the statistical analysis section of this article , the phrase based on this bayesian approach , has been moved to the beginning of the preceding sentence , so that it now reads : based on this bayesian approach , given a sample size of 25 patients per group , assuming that 28% achieve an overall response , the 95% credible interval would be 126457 . 
however , in a brief four - page document outlining his health - care plans , the main points of focus are the immediate dismantling of the a ordable care act ( aca ) and a reduction in funding for medicaid and medicare . 
the most concrete point made in the document is that the free market should determine provision of health care , with insurers free to o er plans across state lines . 
he also calls for greater transparency on health - care costs , and explicitly stipulates that the us market should be open to cheaper drugs from international sources . the aca was introduced in an insurance - based system to enable the many millions of uninsured americans its access to health carean ambition that has been partially realised . 
while an attempted repeal of the aca now looks inevitable given trumps hardline stance and the republican partys control of both houses of congress , it should not be withdrawn until a workable substitute has been drawn up . 
although the aca is awedespecially implementation , rising premiums , decreasing coverage , and inability to provide cover for all noninsured americansit currently stands as the main barrier between poorer americans and the risk of either a premature death or being bankrupted by the worlds most expensive health - care systewhat is needed is strong , policy - driven leadership and a commitment of funds to tackle the fast - rising incidence of cancer and other non - communicable diseases in the american population . the lack of detail in trumps plans allows for exibility in their execution . 
 the lancet oncology drug approval by regulators : who watches the watchers ? randomised in this issue of the lancet oncology , ian tannock and colleagues discuss some important parameters controlled governing outcomes of trials . 
they note that this concept is , in part , a consequence of regulators such as the us food and drug administration and the european medicines agency requiring statistical signi cance versus a comparator for a speci c endpoint to license drugs , rather than an indication that a drug has greater clinical utility compared with those already available . 
also , drug approvals usually require full disclosure of toxicities to regulators , who then have the relevant data and in - house knowledge to undertake thorough meta - analyses across multiple trials to determine drug safety . 
while there is always a need to collect real - world data to ensure e cacy in an unselected patient population , these processes can sometimes lead to a duplication of e ort and a waste of taxpayers moneypublic grants and taxes fund agency operating costs and later analyses . 
 for regulatory agencies to truly serve the public that they are designed to protect , there should be greater transparency in the approval process , with approval being clearly made on clinical , not just statistical , e cacy . 
 the lancet oncology vol 17 december 2016 1621 corrections published online june 24 , 2016 s1470 - 2045 ( 16 ) 30273 - x correction to lancet oncol 2015 ; 16 : 733 correction to lancet oncol 2016 ; 17 : 1055 correction to lancet oncol 2016 ; 17 : 1163 , 1165 basset - seguin n , hauschild a , grob jj , et al . 
 conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
 lancet oncol 2016 ; 17 : 104760 in gure 4b of this article , the curves for 57 gy grade 1 + and 60 gy grade 1 + were incorrect . 
these corrections have been made to the online version as of june 24 , 2016 , and the printed version is correct . van maaren mc , de munck l , de bock gh , et al . 
lancet oncol 2016 ; 17 : 115870in gures 2b and 3b , the label for the bottom row of number at risk should have read t2n1 , and in gure 3b , the label for the top row should have read t1n0 . 
these corrections have been made to the online version as of july 26 , 2016 , and the printed version is correct . vol 17 august 2016 e321 evans sm , tikellis g , brooks a , et al . 
health - related quality of life after apalutamide treatment in patients with metastatic castration - sensitive prostate cancer ( titan ) : a randomised , placebo - controlled , phase 3 study . 
abiraterone acetate plus prednisone in patients with newly diagnosed high - risk metastatic castration - sensitive prostate cancer ( latitude ) : final overall survival analysis of a randomised , double - blind , phase 3 trial . 
psychooncology 2018 ; 27 : 233948 . stereotactic beam radiotherapy for prostate cancer : is less , more ? either important trial , in the lancet oncology , douglas brand and colleagues1 report an in which the authors aimed to investigate the fractionation sensitivity of radiotherapy in the curative treatment of low - risk and intermediate - risk prostate cancer . 
acute toxicity might be worse when treatments are delivered in few large fractions and an overall treatment time as short as 12 weeks , compared with protracted schedules delivered in 68 weeks . 
although the study limits its focus to early tolerance ( up to 12 weeks after radiotherapy ) , this study is the first that was designed to use contem porary radiotherapy delivery techniquesie , linac - based volumetric modulated arc radiotherapy or cyberknife . is much more patient - friendly important dose constraints to the organs at risk ( eg , rectal wall , bladder wall , and urethra ) were well established , aiming to levels . 
the limit toxicity to acceptable in the stereotactic body proportions of patients radiotherapy group who had physician - reported moderate ( grade 2 ) gastrointestinal and genitourinary acute toxicity , according to the national cancer institute common terminology criteria for adverse events ( ctcae ) , were 62 ( 15% ) of 415 patients and 121 ( 29% ) , respectively , compared with the proportions in the conventionally fractionated or moderately hypofractionated group ( 33 [ 8% ] of 432 patients and 96 [ 22% ] , respectively )  . the proportion of moderate gastrointestinal toxicity was higher than those reported by some phase 2 trials using similar stereotactic body radiotherapy scenarios , with proportions ranging from 2% to 8%.24 to reduce the dose to the rectal wall , the use of gadgets such as endorectal balloons or spacers implanted between the rectum and the prostate have been recommended.5 , 6 because both procedures are invasive or , at least , uncomfortable , an alternative could be to reduce the dose constraints applied to the rectal wall while keeping the dose prescription to the target unchanged . 
this method might lead to an optimisation of the final treatment plan by low substantially doses to the rectal wall.7 nowadays , dose distribution optimisation can be substantially and easily improved with software for multicriteria optimisation planning , based on pareto surface.8 intermediate and reducing the because the prostatic urethra inside the target volume always gets the full prescribed dose , the proportion of patients with moderate genitourinary acute toxic effects was similar to that which has see articles page 1531 vol 20 november 2019 1471 comment been reported elsewhere ( 2635% ) .2 , 3 nevertheless , in the only trial with a similar treatment schedule , but a dose reduction to the urethra ( from 725 gy to 65 gy per fraction ) , only 14 ( 17% ) of 82 patients had moderate acute genitourinary toxic effects , which favourably compares with the 29% reported by brand and colleagues.4 on the other hand , zelefsky and colleagues reported genitourinary toxic effects in 24 ( 18% ) of 136 patients , without reducing the dose to the urethra in their dose escalation trial from 325 gy to 40 gy in five fractions , thus casting doubts about the rationale for partially shielding the urethra , considering , additionally , an increased risk of local relapse.9 five fractions delivered every other day ( approximately 10 days overall treatment time ) has been the most frequently used schedule in most phase 2 trials of stereotactic body radiotherapy , regardless of the fact that the most convenient procedure for patients and department logistics would be to deliver stereotactic body radiotherapy 5 days in a row . 
although no difference in severe genitourinary acute toxicity was observed among the 86 patients treated up to 1 week compared with the 329 treated in more than 1 week , brand and colleagues1 found that genitourinary grade 2 acute toxicity was less among those patients treated in the shortest overall treatment time . 
was this observation related to selection biases ( patients with large prostatic volumes or less favourable baseline genitourinary symptoms being treated over a longer overall treatment time ) ? nonetheless , this observation is an invitation to shorten the overall treatment time for stereotactic body radiotherapy in five fractions as much as possible . patients in the stereotactic body radiotherapy group were treated with either cyberknife or volumetric modulated arc radiotherapy . 
the irradiation time of each fraction was significantly different , much longer ( 45 min ) with cyberknife and much shorter with volumetric modulated arc radiotherapy ( 35 min )  . 
furthermore , research has suggested that a long beam - on time with cyberknife might favour intrafraction repair mechanisms , thus reducing the biologically effective dose for late - responding tissues with high fractionation sensitivity.10 this effect might have consequences regarding tumour control and late effects in later followfinally , can the number of fractions with stereotactic body radiotherapy further be reduced from five to a single high - dose fraction ? there are currently two ongoing monotherapy studies exploring the role of single - fraction stereotactic body radiotherapy for patients with localised prostate cancer : the prosintinvestigating igrt phase 2 trial 45 gy in five consecutive fractions versus a single dose of 24 gy ; and the one - shot trial ( nct03294889 ) , a phase 12 , multicentre study of the safety and efficacy of a single fraction of 19 gy with a urethra - sparing approach . 
 indeed , a change of paradigm towards radiosurgery for prostate cancer seems to be on its way . ( nct02570919 ) raymond miralbell university of geneva medical school , geneva 1260 , switzerland ; institut oncolgic teknon , barcelona , spain ; and centro de protonterapia quironsalud , madrid , spain raymond.miralbell@unige.ch i report personal fees from bayer and grants from varian , outside of the submitted work . copyright 2019 the author ( s )  . 
intensity - modulated fractionated radiotherapy versus stereotactic body radiotherapy for prostate cancer ( pace - b ) : acute toxicity findings from a randomised , open - label , phase 3 , non - inferiority trial . 
local protocol variations for image guided radiation therapy in the multicenter dutch hypofractionation ( hypro ) trial : impact of rectal balloon and mri delineation on anorectal dose and gastrointestinal toxicity levels . 
urethra - sparing stereotactic body radiotherapy for prostate cancer : how much can the rectal wall dose be reduced with or without an endorectal balloon ? radiat oncol 2018 ; 13 : 11419 . craft dl , hong ts , shih ha , et al . 
int j radiat oncol biol phys 2004 ; 59 : 24249 . 1472 vol 20 november 2019 comment cancer care in the commonwealth caribbean in covid times the language of urgency that we have grown used to in these so - called covid times could well be applied to the problem of cancer care and control in the small island nations of the caribbean . 
as the second leading cause of death , 1 and with the prediction that cancer cases will rise by 66% in the next 10 years , 2 this alone should serve as an urgent call to arms for governments and health services in the region . the covid - 19 pandemic has shown us how well we can connect virtually when we need to , and how connections and partnerships that previously did not seem likely or possible have suddenly become the bedrock of our moving forward . 
we must also establish clear pathways of care , especially in small island nations who can link together to provide an expert consultation service with a wide reach . the commonwealth caribbean comprises 18 englishspeaking nations . 
many are classified as high - income countries ( hics ) or upper middle - income countries by the world bank ; however , their health services , including cancer care , are unlike those of larger hics.3 most have small , open economies , are heavily dependent on tourism , and are increasingly susceptible to climate change . 
 the most common cancer types are prostate cancer in men and breast cancer in women , and mortality from these cancers in the caribbean is among the highest in the world.1 additionally , cervical cancer , which should be entirely preventable , is still the second leading cause of cancer death in women in many caribbean countries.1 although primary health - care services are generally well established in the region , secondary and tertiary services vary greatly between countries . 
the capacity of caribbean health systems to provide optimal cancer care remains inadequate in the context of other competing priorities , with poor diagnostic and supporting service infrastructure , and an insufficient cadre of trained personnel to deliver the types of care needed . 
patients might have to travel long distances , including air travel , often at substantial expense , to access care.3 although core cancer treatments such as surgical oncology , medical oncology , and radiotherapy are more readily available in the larger islands ( eg , the bahamas and jamaica ) , inadequate numbers of trained specialists mean there are often long waiting lists , compounding the issue of advanced disease presentations.4 we need to reframe and reemphasise priorities for improved cancer care in the region . 
first , we must devise and implement strategies for improving existing cancer care services , focusing on : better cancer surveillance and data collection ; preventing the preventable ; streamlining referral pathways and linkages between cancer care providers , both within and between countries ; and developing and implementing resourcestratified guidelines across the cancer care continuum from prevention through to palliative and end - of - life care.4 second , we must propose new strategies for the expansion of cancer care in the region that are affordable and achievable and with the principal focus on the education and training that will expand the current cadre of health - care professionals . cancer data from cancer surveillance systems are critical to identify public health needs and help to drive policy , yet these are poorly developed in the caribbean . 
 to correct this situation , the international agency for research on cancer ( iarc ) has launched iarc caribbean cancer registry hub offerring technical assistance for the collection of high - quality cancer care data to support an evidence - based approach to cancer care policy and planning in the region within the framework of global initiative for cancer registry development . 
so far , 16 caribbean countries have been engaged with the caribbean hub and 13 countries have participated in capacity - building activities . for world banks country classification see datahelpdesk.worldbank.org / knowledgebase / articles / 906519 for caribbean cancer registry hub resources and technical assistance see caribbeancrh.carpha.org for global initiative for cancer registry development see vol 21 august 2020 1007 comment for more on organization of eastern caribbean states and full list of members see we - are / member - states in terms of preventing the preventable , we are reminded that cervical cancer is now earmarked for elimination in the countries of the americas , including the caribbean . 
thus , continued implementation of human papillomavirus ( hpv ) vaccination using the 9 - valent vaccine , effective against the highrisk hpv types circulating in the caribbean , 5 is urgently needed for 926 year olds , 6 along with targeted hpv screening of high - risk women , aged 30 years or older . 
 countries will need to achieve screening rates of at least 80% in this population to have the greatest impact in reducing deaths from cervical cancer . a focus on strengthening and streamlining existing clinical pathways and institutional guidelines for cancer care will be critical . 
implementing resource - appropriate , strategic plans to improve patient access to early diagnosis and early treatment in two or three common cancers would help reduce morbidity and mortality and health - care costs in the longer term.7 many of the larger island nations do have extensive resources for the treatment of breast , prostate , and colorectal cancers , although these might not be united under one roof , and referral pathways and linkages between the separate services of diagnostic imaging , surgery , pathology , medical and radiation oncology , and palliative care might not be robust or clearly defined8 ( yeung l , university of british columbia , personal communication )  . 
resources such as the breast health global initiatives publication , knowledge summaries for breast cancer , 4 provide an excellent template for health - care professionals aiming to improve patient access to existing services . 
improved coordination of services requires developing strong referral networks with clear guidelines for providers on how to refer patients efficiently and appropriately through the syste providers are encouraged to hold multi - disciplinary team meetings and tumour boards to foster better communication and regular collaboration . 
another valuable innovation , relatively new to the caribbean , is the introduction of cancer patient navigation programmes , which help to increase patient access to , and use of , appropriate resources for cancer care.9 such programmes are already being introduced in trinidad and tobago and jamaica . strategies for the further expansion of cancer care in the caribbean islands must take a broad view . 
models for this type of approach already exist in the region.3 task shifting through education and the development of community - based services , including palliative care , is imperative as we adjust to a new normal of social distancing and increasing barriers to traveling to seek care . inter - island and intra - island collaborative efforts are ongoing . 
the initiative includes professionals involved in all aspects of cancer care working together to use available expertise to facilitate the provision of optimal cancer diagnostic and treatment plans for their under - resourced include shared health systems . 
larger caribbean countries are urged to consider this type of approach that can increase collaboration and connectivity between service providers , to improve access and availability of care for all . we believe that by taking the steps discussed , we can make substantial improvements in the cancer care that is already offered in the caribbean and move towards offering excellent , guideline - recommended care for all people living in this region . we declare no competing interests . * glennis andall - brereton , brittany bromfield , steven smith , dingle spence andallgl@carpha.org 1008 vol 21 august 2020 comment caribbean public health agency , port of spain , trinidad and tobago ( ga - b ) ; jamaica cancer care and research institute , kingston , jamaica ( bb , ss , ds ) ; and hope institute hospital , kingston , jamaica ( ds ) razzaghi h , quesnel - crooks s , sherman r , et al . 
 health - sciences / epidemiology / bci - 25 / kspdf / ks%20planning%20 access%20030617.pdf ( accessed june 29 , 2020 )  . andall - brereton g , brown e , slater s , et al . 
cancer patient navigator tasks across the cancer care continuuj health care poor underserved 2012 ; 23 : 398413 . 100 european core quality standards for cancer care and research centres there have been calls for consensus around defining quality standards for cancer care , treatment , and research in europe , with a focus on cancer hospitals , centres , and networks . 
although cancer survival is generally improving , large variation in cancer survival between countries remains , as shown by results in the eurocare - 5 study.1 the european commissioner for health and food safety has launched europes beating cancer plan . 
 in addition , a cancer mission is being drafted by the european commission , 2 with some objectives most likely to be focused on the need to ensure quality of treatment , care , and research , and to create more comprehensive cancer centres and infrastructure.3 , 4 in europe , many cancer centres , which act as hubs interlocking clinical research networks , provide state - of - the - art cancer services . 
therefore , an aim for both the cancer mission and beating cancer plan could be to establish at least one comprehensive cancer centre or large clinical centre in each small eu member state , and to have one comprehensive cancer centre for every 510 million people in the population in larger eu member states , as part of an integrated infrastructure.5 in 2008 , the organisation of european cancer institutes ( oeci ) created a quality assurance accreditation and designation programme for cancer centres , 6 which includes 50 of the largest cancer centres in 14 of 27 eu member states , plus norway and the uk . 
collectively , these centres produce more than 12 400 peer - reviewed publications on cancer research annually , have a total annual research budget of over 1 billion , and have treated more than 1 million new patients since accreditation . 
although these centres treat only 10% of patients diagnosed with cancer in the eu each year , their effect on the quality of cancer care and research is substantial , as they are considered as national reference centres . the accreditation and designation programme focuses on institutional quality and capabilities , with the objective of providing comprehensive accreditation for quality oncology care , including prevention , care , research , education , networking , and patient involvement . 
inclusion of these issues is a unique feature of this oeci programme , compared with cancer accreditation systems in the usa and germany , where clinical care and cancer research are generally accredited separately . 
in addition , the oeci standards have been accredited by the international society for quality in health care . the 50 participating cancer centres are shown in the appendix ( p 1 )  . 
 sequential administration of nivolumab and ipilimumab with a planned switch in patients with advanced melanoma ( checkmate 064 ) : an open - label , randomised , phase 2 trial . 
lancet oncol 2016 ; 17 : 94355in gure 5 , under the headings nivolumab followed by ipilimumab and ipilimumab followed by nivolumab , the text should have read number of events / number of patients . 
this correction has been made to the online version as of june 28 , 2016 , and the printed version is correct . correction to lancet oncol 2016 ; 17 : 995 , 1002 cella d , grnwald v , nathan p , et al . 
 quality of life in patients with advanced renal cell carcinoma given nivolumab versus everolimus in checkmate 025 : a randomised , open - label , phase 3 trial lancet oncol 2016 ; 17 : 9941003in this article , the order of references 711 has been corrected and the fourth sentence of the second paragraph of the introduction has been corrected to read furthermore , an analysis of hrqol scores according to the functional assessment of cancer therapy - kidney symptom index - disease related symptoms ( fksi - drs ) questionnaire ( a subscale of the 15 - item fksi - 15 ) showed that median change from baseline increased over time with nivolumab treatment . 
these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . jeong s - y , park jw , nam bh , et al . 
open versus laparoscopic surgery for mid - rectal or low - rectal cancer after neoadjuvant chemoradiotherapy ( corean trial ) : survival outcomes of an open - label , non - inferiority , randomised controlled trial . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2015 ; 16 : 1479 motzer rj , hutson te , glen h , et al . 
lancet oncol 2015 ; 16 : 147382in table 3 of this article , the number of patients in the lenvatinib plus everolimus group with grade 3 constipation should be 0 . 
 this correction has been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 351 untch m , jackisch c , schneeweiss a , et al . 
 lancet oncol 2016 ; 17 : 34556in this article , the data in the second sentence of the third paragraph of the results section should have read in multivariable logistic regression analysis , nab - paclitaxel remained an independent predictor for achievement of pathological complete response after adjustment for baseline and minimisation factors ( or 159 ; 95% ci 120211 ; p = 00013 )  . 
fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment o f h o r m o n e r e c e p t o r p o s i t i v e , her2 - negative metastatic breast cancer that progressed on previous endocrine therapy ( paloma - 3 ) : final analysis of the multicentre , doubleblind , phase 3 randomised controlled trial . 
lancet oncol 2016 ; 17 : 42539 in figures 2a , 5a , 5b , and 5c , the kaplan - meier curves should have intersected with the y - axis at the 100% mark . 
these corrections have been made to the online version as of june 28 , 2016 . correction to lancet oncol 2016 ; 17 : 888 , 890 , 892 cancer antonia sj , lpez - martin ja , bendell j , et al . 
 lancet oncol 2016 ; 17 : 88395in this article , the rst line in the third paragraph of the results , blinded independent central review should have been investigator - assessed recist . 
in the seventh paragraph of the results , the number of patients in the nivolumab 3 mg / kg plus ipilimumab 1 mg / kg cohort who had diarrhoea as a serious adverse event should have been two ( 4% ) , not four ( 7% )  . 
 these corrections have been made to the online version as of june 28 , 2016 , and the printed version is correct . vol 17 july 2016 e270 visceral crisis , for whom optimal management is still unclear : should these patients receive chemotherapy followed by cdk4 / 6 inhibitors plus endocrine therapy in maintenance , or should chemotherapy be continued until disease progression , or could endocrine and cdk4 / 6 inhibitor combinations also supplant chemotherapy for these patients ? ongoing studies will address the optimal management in this remaining small group of patients . marie robert , * nicholas turner breast unit , the royal marsden hospital , london sw3 6jj , uk ( mr , nt ) ; and breast cancer now research centre , institute of cancer research , london , uk ( nt ) nick.turner@icr.ac.uk mr has received travel fees from amgen , roche , and novartis . 
nt has received advisory board honoraria from astrazeneca , bristol - myers squibb , lilly , merck sharpe and dohme , novartis , pfizer , roche / genentech , tesaro , bicycle therapeutics , and taiho , and research funding from astrazeneca , biorad , pfizer , roche / genentech , clovis , merck sharpe and dohme , and guardant health . cardoso f , senkus e , costa a , et al . 
in real life , one - quarter of patients with hormone receptor - positive metastatic breast cancer receive chemotherapy as initial palliative therapy : a study of the southeast netherlands breast cancer consortiuann oncol 2016 ; 27 : 25662 . bonotto m , gerratana l , di maio m , et al . 
palbociclib plus exemestane with gonadotropin - releasing hormone agonist versus capecitabine in premenopausal women with hormone receptor - positive , her2 - negative metastatic breast cancer ( kcsg - br15 - 10 ) : a multicentre , open - label , randomised , phase 2 trial . 
the effect of abemaciclib plus fulvestrant on overall survival in hormone receptor - positive , erbb2 - negative breast cancer that progressed on endocrine therapy monarch 2 : a randomized clinical trial . 
esmo congress 2019 ; barcelona , spain ; sept 27oct 1 , 2019 ( lba7_pr )  . reducing infection - related morbidity and mortality in patients with myeloma myeloma survival has substantially improved in the past 10 years.1 although most myeloma deaths are accountable to progressive disease , a substantial proportion of early deaths and deaths in remission are due to infections.2 febrile infections induce considerable morbidity and frequently lead to drug interruption or drug discontinuation . 
in their article in the lancet oncology , mark drayson and colleagues3 present findings that showed that 12 weeks of fixed - duration levofloxacin prophylaxis reduced the occurrence of febrile episodes and deaths ( 95 [ 19% ] febrile episodes or deaths in 489 patients in the levofloxacin group vs 134 [ 27% ] in 488 patients in the placebo group ; hazard ratio [ hr ] 066 , 95% ci 051086 ; p = 00018 )  . 
there has been a switch to a continuous anti - myeloma therapy approach in newly diagnosed patients.4 the risk for infections remains higher during the overall treatment period compared with time not receiving chemotherapy . 
patients in this trial were primarily treated with immunomodulatory imide drug - based or proteasome inhibitor - based drug combinations , 3 but clinicians are moving towards monoclonal antibody - based drug combinations based on the results from the alcyone and maia studies.5 , 6 grade 3 and grade 4 infections were higher in the daratumumab group than in the non - daratumumab group in both studies . 
the question remains as to whether a combination of both levofloxacin and co - trimoxazole should be recommended for patients on anti - myeloma therapy . independent effect on both febrile data from the first trial7 provide criteria for identifying patients at high risk of grade 3 infection . 
therefore , patients who fit these criteria for high risk of grade 3 infection should be considered for antibiotic prophylaxis . use of antibiotics could increase antibiotic resistance and induce gut dysbiosis . 
drayson and colleagues3 showed that fixed 12 - week levofloxacin prophylaxis does not result in increased carriage of clostridium difficile , extended - spectrum - lactamase gram - negative coliforms , or meticillin - resistant staphylococcus aureus . 
longer - term antibiotic prophylaxis - induced dysbiosis has the potential to modify endogenous anti - tumour immunity and efficacy of immunotherapy in patients with myeloma . limit patients with myeloma have a high risk of viral infections . 
in particular , assessment of the therapeutic effects of a combination of co - trimoxazole and levofloxacin and investigation of various durations of antibiotic prophylaxis are crucial to optimise patient outcomes . karthik ramasamy oxford university hospitals nhs foundation trust , oxford , uk ; oxford national institute for health research biomedical centre blood theme , oxford , uk ; and oxford centre for myeloma translational research , oxford ox3 7le , uk karthik.ramasamy@ndcls.ox.ac.uk i report research grants , advisory board , and speaker fees from celgene , takeda , janssen , and amgen , and speaker and advisory board fees from sanofi , abbvie , and oncopeptides , outside the submitted work . copyright 2019 the author ( s )  . 
early mortality after diagnosis of multiple myeloma : analysis of patients entered onto the united kingdom medical research council trials between 1980 and 2002medical research council adult leukaemia working party . 
phase 3 randomized study of daratumumab plus lenalidomide and dexamethasone ( d - rd ) versus lenalidomide and dexamethasone ( rd ) in patients with newly diagnosed multiple myeloma ( ndmm ) ineligible for transplant ( maia )  . 
j bone oncol 2019 ; 17 : 100243 . cancer prevention and treatment in humanitarian settings : an urgent and unmet need the who eastern mediterranean region is currently facing an immense burden of cancer . 
as well as being the site of numerous protracted crises , with over 50% of the region experiencing humanitarian emergencies , it is the who region that is expected to have the greatest increase in cancer incidence during the next 15 years.1 historically , humanitarian actors have focused on supporting conflict - affected populations through emergency aid and infectious disease prevention and treatment strategies . 
although despite the increasing burden of cancer , the global literature evidence base of peer - reviewed or grey surrounding cancer treatment and prevention humanitarian contexts in the eastern mediterranean region is extremely scarce , and nearly all the available information on this topic comes from documentary sources research and response plans have grown to address both communicable and non - communicable diseases these contexts , cancer treatment and prevention have seldom been addressed . 
in almost every recent humanitarian setting , the care of cancer patients and efforts dedicated towards cancer prevention have been neglected because of local and global political and economic determinants , such as legal status , freedom of movement , affordable treatment , and availability of health resources and research . 
similarly , the delivery of health care through humanitarian systems is often parallel to and not well integrated with the health systems of host nations , which further complicates the provision of cancer treatment services . although both the who constitution and the 1948 universal declaration of human rights reinforce a global commitment to preserving access to health care as a basic human right , which extends to the provision of cancer treatment screening , diagnosis , and services , the inaccessibility of cancer care has been well documented across humanitarian settings in the eastern mediterranean region.1 lebanon hosts more than 1 million syrian refugees , 74% of whom do not have legal status . 
given the countrys highly privatised individuals and fragmented health system , these do not have access to any form of public health insurance and must finance the cost of treatments on their own.3 based on the lebanese ministry of public healths utilisation and spending data , the annual average cost of cancer drug treatment , which does not include radiotherapy , is us$6475 per patient , and syrian refugee families have been reported to earn an average monthly income of less than $300.4 , 5 in jordan , nearly 900 syrian refugees are diagnosed with cancer annually and have no sustainable access to affordable treatment , with the cost of treating this growing population exceeding $22 million ; in addition , syrian refugees in jordan are required to pay 80% of the amount that is paid by foreigners without insurance , which imposes a large financial burden on refugee families.6 in both lebanon and jordan , refugees have few treatment - seeking options due to an inability to move freely within or across countries , not having proper documentation as a result of forced migration , and the fear of detainment vol 20 december 2019 1635 comment presenting symptoms of cancer and stage at diagnosis : evidence from a cross - sectional , population - based study minjoung monica koo , ruth swann , sean mcphail , gary a abel , lucy elliss - brookes , greg p rubin , georgios lyratzopoulos summary background early diagnosis interventions such as symptom awareness campaigns increasingly form part of global cancer control strategies . 
therefore , we aimed to examine associations between common presenting symptoms of cancer and stage at diagnosis . methods in this cross - sectional study , we analysed population - level data from the english national cancer diagnosis audit 2014 for patients aged 25 years and older with one of 12 types of solid tumours ( bladder , breast , colon , endometrial , laryngeal , lung , melanoma , oral or oropharyngeal , ovarian , prostate , rectal , and renal cancer )  . 
the proportion of patients diagnosed with stage iv cancer varied substantially by presenting symptom , from 1% ( 95% ci 13 ; eight of 584 patients ) for abnormal mole to 80% ( 7187 ; 84 of 105 patients ) for neck lump . 
three of the examined symptoms ( neck lump , chest pain , and back pain ) were consistently associated with increased odds of stage iv cancer , whether reported alone or with other symptoms , whereas the opposite was true for abnormal mole , breast lump , postmenopausal bleeding , and rectal bleeding . 
for 13 of the 20 symptoms ( abnormal mole , breast lump , post - menopausal bleeding , rectal bleeding , lower urinary tract symptoms , haematuria , change in bowel habit , hoarseness , fatigue , abdominal pain , lower abdominal pain , weight loss , and the any other symptom category ) , more than 50% of patients were diagnosed at stages other than stage iv ; for 19 of the 20 studied symptoms ( all except for neck lump ) , more than a third of patients were diagnosed at stages other than stage iv . interpretation despite specific presenting symptoms being more strongly associated with advanced stage at diagnosis than others , for most symptoms , large proportions of patients are diagnosed at stages other than stage iv . 
these findings provide support for early diagnosis interventions targeting common cancer symptoms , countering concerns that they might be simply expediting the detection of advanced stage disease . funding uk department of healths policy research unit in cancer awareness , screening and early diagnosis ; and cancer research uk . copyright 2019 the author ( s )  . 
we identified 12 studies on single cancer sites ( five on ovarian cancer , three on colon or colorectal cancer , one on lung cancer , one on anal cancer , one on pancreatic cancer , and one on renal cancer ) , of which three examined associations between presenting symptoms and stage , adjusting for possible confounders . 
 only one study ( on patients with colorectal cancer ) considered both single presenting symptoms and symptom combinations . added value of this study these findings characterise associations between common presenting symptoms and stage at diagnosis in a population - based incident cohort of patients with different cancers . 
for 13 of the 20 studied symptoms , more than 50% of patients were diagnosed with cancer at stages other than stage iv , and for 19 symptoms ( all except for neck lump ) more than a third were diagnosed at a stage other than stage iv . implications of all the available evidence common presenting symptoms have variable associations with advanced stage at diagnosis , although for all symptoms analysed in this cross - sectional study we found that large proportions of patients are diagnosed at stages other than stage iv . 
early diagnosis initiatives such as public health campaigns aimed at raising awareness of possible symptoms of cancer and clinical guidelines for the assessment and investigation of patients with symptoms have the potential to help detect cancer at a non - advanced stage . methods study design and participants for this cross - sectional , population - based study we analysed data of patients included in the national cancer diagnosis audit ( ncda ) in england.17 as described previously , general practitioners ( gps ) and other healthcare professionals in participating general practices provided information about the diagnostic pathway of patients identified as having been diagnosed with a malignant neoplasm in 2014 by public health englands national cancer registration and analysis service ( ncras )  . 
ethical approval for this study was obtained by the london hampstead research ethics committee ( rec reference : 8 / lo / 0377 )  . contemporary 439 general practices ( comprising approximately 5% of all practices in england ) submitted data on 17 042 tumour records . 
the sex , age , and cancer site distribution of included patients was representative of cohort.17 national the furthermore , participating practices were similar to non - participating practices with their demographic case - mix , patient experience scores , and referral rates for suspected cancer , but served slightly larger registered populations.17 incident regard we restricted our study population to symptomatic adult patients aged 25 years and older , diagnosed with one of 12 solid tumours with a high degree ( 85% ) of stage completeness ( in descending order ) : endometrial ( 95% complete staging ) , lung , rectal , breast , melanoma , renal , bladder , ovarian , oral or prostate , colon , oropharyngeal , or laryngeal cancer ( 85% complete staging ) , representing 79% of incident cases of solid tumours in england in the study year 201418 ( see appendix p 3 for the list of excluded cancers )  . procedures information about stage at diagnosis in the study population was available from ncras as tnm stage iiv ; we defined advanced stage as tnm stage iv ( see below for alternative categorisation of stage at diagnosis )  . information about presenting symptoms ( specified as symptoms noted at first presentation before diagnosis and referral ) was provided by participating gps based on health records using a list of 81 prespecified symptoms ( in yes and no format )  . 
we examined 19 symptoms recorded in at least 50 patients : abnormal mole , abdominal pain , back pain , breast lump , chest infection , chest pain , change in bowel habit , cough , dyspnoea , fatigue , haematuria , haemoptysis , hoarseness , lower abdominal pain , lower urinary tract symptoms , neck lump , post - menopausal bleeding , rectal bleeding , and weight loss . 
therefore , patients could have a single presenting symptom or multiple symptoms ( one or more of the above symptoms in any combination )  . statistical analysis we estimated the proportion of patients diagnosed at stage iv by single or multiple symptom status for each of the 20 symptoms . 
because patients with different cancers often present with the same symptom , 16 we examined the cancer site case - mix of each presenting symptom ( namely , the proportion of patients with different cancers that are diagnosed following presentation with a particular symptom ) to aid interpretation of our findings ( see appendix pp 56 for cancer site signatures of all 20 symptoms )  . subsequently , we examined patient - level associations between symptoms and stage at diagnosis using logistic regression ( stage iv vs stages iiii )  . 
ideally , we would have studied associations between every symptom vol 21 january 2020 articles combination ( each pair , triplet , and so on ) and stage at diagnosis , because the presence of additional symptoms could affect a given symptoms association with the outcome of interest ; however , this approach was not feasible given the large number of symptom combinations relative to the sample size . 
instead , we modelled each presenting symptom as a pair of binary variables : one denoting its presence or absence , and the other denoting its presence or absence when recorded with other symptoms . 
since we did not examine patients without symptoms , the constant was constrained to 0 , fixing the baseline odds of stage iv to 1 . the symptom for each symptom , two odds ratios ( ors ) could be estimated from the above model for each symptom : single and multiple . 
the single or represents the association of a given symptom with stage at diagnosis when seen alone , compared with change in bowel habit ( used as the reference category , since this was the most common study population )  . 
 furthermore , by adding the coefficients from the first and second binary variables for each symptom , we estimated a multiple or for each symptom , which represents its association with cancer stage when seen together with one or more of the other 19 symptom categories , compared with patients with multiple symptoms other than the symptom of interest . 
an or value of 1 implies that stage at diagnosis is no different between patients with and without the symptom of interest among those with multiple symptoms . we also adjusted for age group ( categorised as 2549 years , 5059 years , 6069 years , 7079 years , and 80 years ) , sex ( male vs female ) , index of multiple deprivation income domain quintiles ( from 1 to 5 , with 1 being least deprived and 5 being most deprived ) , ethnicity ( white , non - white , and missing ) , and cancer site ( 12 solid tumour sites , as described above )  . 
for the first , we repeated the main analysis by categorising advanced stage as stage iiiiv , compared with stage iii disease . imputation can make the second sensitivity analysis comprised an extreme case scenario for missing information about stage . 
 unlike with missing exposure variable data , a complete case analysis ( cca ) where only outcome variable data are missing ( as is the case for stage at diagnosis in our study ) is unbiased assuming the missing at random mechanis multiple the assumption of data missing at random more reasonable than it would be under cca only if auxiliary variables that are absent from the analysis model are used in the imputation model ; 20 however , no such variables were available and so the imputation model would have been of no value . 
although this extreme scenario is unlikely to be realistic , we can be reasonably confident that the true bias in our findings will be lower than that illustrated with this analysis.21 the third sensitivity analysis involved repeating the main analysis by restricting it to patients who had a diagnostic interval ( time from symptomatic presentation to diagnosis ) of 060 days , since time to diagnosis could influence the association between presenting symptoms and stage.22 for the fourth sensitivity analysis , we adjusted for route to diagnosis as the association between route to cancer diagnosis ( a patients health - care utilisation pathway before diagnosis ) and stage might also influence the association of interest.23 therefore , the main analysis was repeated with further adjustment for route to diagnosis among patients with complete information about their diagnostic route.24 specifically , we considered the following five diagnostic route categories : 2 - week - wait referral ( urgent referrals for suspected cancer from primary care to specialist hospital services in the uk ) , elective referral ( routine , non - urgent referrals ) , emergency presentation , secondary care ( both inpatient and outpatient ) routes , and unknown route . all analyses were done with stata se , version 15.1. 12 927 patients with non - screen detected cancer with complete information on symptoms 11 636 patients 8919 patients 8893 patients 1291 excluded ( diagnosed with leukaemia , lymphoma , myeloma , or brain cancer ) 2717 excluded ( patients with cancer sites where > 15% of patients had no information on stage * or were diagnosed with stage 0 ) 26 excluded ( aged 024 years ) 896 excluded ( with missing stage information ) 7997 patients included in nal analysis figure 1 : study population * n = 2707 . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results from an initial cohort of 12927 patients with non - screen detected cancers included in the ncda 2014 , we analysed data for 7997 patients diagnosed with solid tumours with high stage completeness ( figure 1 )  . 
breast lump was the most common presenting symptom , reported in 1260 patients in our study sample , and neck lump was the least common , reported in 105 ( table )  . 
a third of all patients ( 2685 of 7997 ; 34% [ 95% ci 3335 ] ) had two or more symptoms ; symptoms varied in their likelihood of being seen alone or with other symptoms ( figure 2 )  . some , typically localised , symptoms had relatively narrow cancer site signatures where the majority ( > 80% ) of patients were diagnosed with the same cancer site , such as breast lump ( breast cancer ) , abnormal mole ( melanoma ) , post - menopausal bleeding ( endometrial cancer ) , lower urinary tract symptoms ( prostate cancer ) , and haemoptysis , dyspnoea , chest infection , chest pain , and cough ( lung cancer )  . 
by contrast , less specific symptoms such as abdominal pain , change in bowel vol 21 january 2020 articles adjusted for symptoms adjusted for symptoms and covariates 005 002 001 habit , back pain , fatigue , and weight loss had more diverse cancer site signatures ( appendix pp 56 )  . the proportion of patients diagnosed at stage iv by symptom varied from 1% ( 95% ci 13 ; eight of 584 patients with an abnormal mole ) to 80% ( 7187 ; 84 of 105 patients with a neck lump ; table , figure 2 )  . 
for 13 of the 20 symptoms , more than 50% of patients were diagnosed with non - advanced stage cancer , while for all symptoms apart from neck lump , more than a third ( at least 38% ) were diagnosed at stages other than stage iv ( table , figure 2 )  . the pattern of variation symptom - specific associations with stage iv disease when reported alone ( figure 3 ) was similar to the associations seen for symptoms when reported with other symptoms ( both p < 00010 ; appendix pp 79 )  . 
three symptoms ( neck lump , chest pain , and back pain ) were consistently associated with an increased odds of stage iv disease , whereas abnormal mole , breast lump , post - menopausal bleeding , or rectal bleeding were associated with lower odds of stage iv disease ( appendix p 8 )  . adjusting for patient characteristics and cancer site made little difference to the order of symptom - specific odds of stage iv disease for both single and multiple symptoms , although effect sizes were generally smaller ( figure 3 ; appendix pp 710 )  . additional sensitivity analyses examining differences in categorisation of stage ( categorising advanced stage as stage iiiiv ) , an extreme case scenario for missing information on stage , stratification by diagnostic interval ( restricting the analysis to those with a diagnostic interval of 060 days ) , and additional adjustment for route to diagnosis also provided similar findings ( appendix pp 1120 )  . discussion in our population - based cohort of patients with cancer , certain presenting symptoms , such as neck lump , had stronger associations with stage iv disease than others , but for most symptoms we found that large proportions of patients were diagnosed at stages other than stage iv . 
adjustment for confounders including cancer site made little difference to the overall pattern of associations between symptoms and stage at diagnosis . with regard to associations between presenting symptoms and stage at diagnosis , direct comparisons with existing literature are challenging because published studies are cancer - site specific . 
evidence from such studies provides an incomplete picture of associations between presenting symptoms and stage at diagnosis , because individuals who present with the same symptoms could be diagnosed with cancers of different sites . 
by contrast , in this study , we evaluated the presenting symptoms of patients with a range of common and rarer neck lu m p chest pain lo w er abdo minal pain any other sy m pto m w eight loss dyspnoea abdo minal pain h oarseness change in bo w el habit cough lo w er urinary tract sy m pto m s fatigue back pain chest infection abnorm al m ole breast lu m p post - m enopausal bleeding hae m optysis hae m aturia rectal bleeding presenting symptoms of patients with cancer figure 3 : odds ratios of stage iv disease by presenting symptoms seen alone odds ratios of stage iv disease by symptom without adjustment ( blue ) ; and with adjustment for sex , age group , ethnicity , imd quintile , and cancer diagnosis ( red )  . 
for odds ratios of symptoms when reported with other symptoms , see appendix p 9 . cancers and examined associations with and without adjustment for the case - mix of cancer sites in our study population . 
nevertheless , in previous studies , among patients with colorectal cancer , rectal bleeding has been associated with earlier stage at diagnosis compared with abdominal pain and change in bowel habit , 9 , 14 whereas in patients with ovarian cancer , gastrointestinal symptoms ( including abdominal pain , digestive bowel symptoms , and distension ) have been more strongly associated with advanced stage cancer than gynaecological symptoms such as vaginal bleeding.8 , 10 except for one published study ( which examined three symptoms and their combinations with stage14 ) , the existing literature does not differentiate symptoms according to when they are reported on their own or when they are reported with other symptoms . 
by contrast , our study characterised associations between symptoms and stage , both when a symptom was reported alone and when it was reported together with other symptoms , which allowed us to adjust for potential interactions between all possible symptom combinations . a key strength of our study is that it examined the association between presenting symptoms and stage in a well - characterised population - based incident cohort of patients with different cancers . 
the ncda represents a unique combination of information provided by gps and other health - care professionals based on clinical insight and judgment , with high - quality information about patient and tumour characteristics from the national cancer registry in england.17 , 25 vol 21 january 2020 articles in addition to adjusting our findings by sociodemographic factors , we adjusted our results by cancer site . 
although this adjustment did not appear to substantially alter the observed patterns of variation , the associations between symptoms and stage at diagnosis might differ in a population - based incident cohort with a different distribution of cancer sites . our study does have some potential limitations . 
as is the case for other studies based on clinical audits of cancer diagnosis , 2628 elicitation and recording of symptoms during the index consultation , and subsequent extraction of information from primary care records , might be incomplete and prone to bias.29 nevertheless , alternative approaches based on self - reported data from individuals diagnosed with cancer are susceptible to under - representation of patients with a poor prognosis.30 with either method , it is possible that some of the recorded symptoms might relate to concomitant chronic illness , especially in patients with multiple symptoms . 
this observation provides a strong indication information about presenting that symptoms chiefly relates to the subsequently diagnosed cancer site rather than other conditions . recorded the the study population represents around four - fifths of patients diagnosed with solid tumours in england during 2014.18 among the cancer sites included in the study , a small proportion of patients with missing stage information were excluded from analyses , variably by cancer site . 
however , sensitivity analyses , which would demonstrate the effect of maximum possible bias arising from missing data ( ie , by assigning patients with missing stage information to stage iv ) provided similar findings to our main analysis . our findings refute concerns that early diagnosis interventions centred on common presenting symptoms of cancer would typically expedite the diagnosis of individuals with stage iv disease . 
this finding was the case even for patients with symptoms most strongly associated with advanced stage in our study , and for symptoms often considered indicative of advanced disease , such as weight loss . furthermore , evaluation of the effect of single and multiple symptoms separately indicates that the presence of multiple symptoms is a poor predictor of stage iv disease . 
this observation is reassuring , given that public health education campaigns typically do not focus on symptom combinations . symptom awareness and appraisal by patients and doctors is an important determinant of timely presentation and investigation3134 but the optimal design interventions aimed at earlier of early diagnosis recognition of possible cancer symptoms by members of the public and health - care professionals remains unclear . 
alongside considerations such as cancer site incidence , psychosocial barriers to presentation , and the predictive value of symptoms , evidence about the associations between presenting symptoms and stage at diagnosis can help to guide the design of early diagnosis interventions . 
our findings provide support for such interventions , and counter concerns that they simply expedite the detection of advanced - stage disease . contributors mmk , gpr , le - b , and gl conceived the study . 
all authors contributed to multiple revisions and approved the final manuscript . declaration of interests we declare no competing interests . acknowledgments the national cancer diagnosis audit ( ncda ) received enabling support from cancer research uk , nhs england , and the national cancer registration and analysis service . 
this work was supported by a grant from the uk department of health ( grant number 106 / 0001 ) as part of the programme of the policy research unit in cancer awareness , screening and early diagnosis . 
the policy research unit in cancer awareness , screening , and early diagnosis is a collaboration between researchers from seven institutions ( queen mary university of london , university college london , kings college london , london school of hygiene and tropical medicine , hull york medical school , durham university , and peninsula medical school / university of exeter )  . 
gpr is chair , gl associate director , gaa senior investigator , and mmk junior faculty member of the multi - institutional cantest collaborative , which is funded by cancer research uk ( grant number c8640 / a23385 )  . 
we thank all general practitioners and health professionals who participated in the ncda , and contributing cancer research uk staff ; the national cancer registration and analysis service , nhs england , the royal college of general practitioners , macmillan cancer support , and health data insight . 
the data are collated , maintained , and quality assured by the national cancer registration and analysis service , which is part of public health england . effect of delays in the 2 - week - wait cancer referral pathway during the covid - 19 pandemic on cancer survival in the uk : a modelling study amit sud * , bethany torr * , michael e jones , john broggio , stephen scott , chey loveday , alice garrett , firza gronthoud , david l nicol , shaman jhanji , stephen a boyce , matthew williams , elio riboli , david c muller , emma kipps , james larkin , neal navani , charles swanton , georgios lyratzopoulos , ethna mcferran , mark lawler , richard houlston , clare turnbull summary background during the covid - 19 lockdown , referrals via the 2 - week - wait urgent pathway for suspected cancer in england , uk , are reported to have decreased by up to 84% . 
we aimed to examine the impact of different scenarios of lockdown - accumulated backlog in cancer referrals on cancer survival , and the impact on survival per referred patient due to delayed referral versus risk of death from nosocomial infection with severe acute respiratory syndrome coronavirus 2 . methods in this modelling study , we used age - stratified and stage - stratified 10 - year cancer survival estimates for patients in england , uk , for 20 common tumour types diagnosed in 200817 at age 30 years and older from public health england . 
we quantified the annual numbers of cancers at stage iiii diagnosed via the 2 - week - wait pathway using 2 - week - wait age - specific and stage - specific breakdowns . 
 from these numbers , we estimated the aggregate number of lives and life - years lost in england for per - patient delays of 16 months in presentation , diagnosis , or cancer treatment , or a combination of these . 
we assessed three scenarios of a 3 - month period of lockdown during which 25% , 50% , and 75% of the normal monthly volumes of symptomatic patients delayed their presentation until after lockdown . 
using referral - to - diagnosis conversion rates and covid - 19 case - fatality rates , we also estimated the survival increment per patient referred . findings across england in 201316 , an average of 6281 patients with stage iiii cancer were diagnosed via the 2 - week - wait pathway per month , of whom 1691 ( 27% ) would be predicted to die within 10 years from their disease . 
 delays in presentation via the 2 - week - wait pathway over a 3 - month lockdown period ( with an average presentational delay of 2 months per patient ) would result in 181 additional lives and 3316 life - years lost as a result of a backlog of referrals of 25% , 361 additional lives and 6632 life - years lost for a 50% backlog of referrals , and 542 additional lives and 9948 life - years lost for a 75% backlog in referrals . 
compared with all diagnostics for the backlog being done in month 1 after lockdown , additional capacity across months 13 would result in 90 additional lives and 1662 live - years lost due to diagnostic delays for the 25% backlog scenario , 183 additional lives and 3362 life - years lost under the 50% backlog scenario , and 276 additional lives and 5075 life - years lost under the 75% backlog scenario . 
however , a delay in additional diagnostic capacity with provision spread across months 38 after lockdown would result in 401 additional lives and 7332 life - years lost due to diagnostic delays under the 25% backlog scenario , 811 additional lives and 14 873 life - years lost under the 50% backlog scenario , and 1231 additional lives and 22 635 life - years lost under the 75% backlog scenario . 
a 2 - month delay in 2 - week - wait investigatory referrals results in an estimated loss of between 00 and 07 life - years per referred patient , depending on age and tumour type . interpretation prompt provision of additional capacity to address the backlog of diagnostics will minimise deaths as a result of diagnostic delays that could add to those predicted due to expected presentational delays . 
overall , studies are highly heterogeneous in design and findings , including the durations of delay studied , the duration of survival follow - up , the method by which impact is captured ( percentages , odds ratios , hazard ratios ) , and how and when staging is done . 
to our knowledge , no study had modelled the impact in lives and life - years lost of systematic delays in referral pathways in a standardised fashion across tumour types until we recently reported a health - care resource analysis focused on systemic delays at point of surgery . added value of this study across multiple tumour types , we used a standardised approach using per - day fatality hazard ratios to quantify the effect of different durations of delay on survival , examining both the referred patient and the diagnosed patient , and examining delays for individual tumour types and subtypes and aggregated across major tumour types . 
 although pertinent to ongoing forecasting of the impact of covid - 19 - related delays , these models could apply to any systemic delays to cancer pathways . implications of all the available evidence incorporating previous observational studies of delay and examining crudely estimated , non - naturalistic per - patient delays , our models predict that covid - 19 - related delays in presentation , diagnosis , and subsequent treatment , will result in loss of life and life - years that varies widely according to patient age and tumour type . 
data regarding the true duration and extent of service disruption and per - patient cancer pathway delay across the uk as a result of the covid - 19 lockdown are currently immature . 
direct predictions regarding attributable cancer deaths will be possible once more accurate patient - level data become available . any delay in cancer treatment has the real risk of patients tumours progressing from being curable ( with near - normal life expectancy ) to becoming non - curable ( with very reduced life expectancy )  . 
specific pathways have been established in the uk for referral from primary care for urgent specialist evaluation and investigation of individuals with so - called red flag symptoms suggestive of a specific cancer type , termed the 2 - week - wait pathway . 
 reductions of up to 84% have been reported in 2 - weekwait referrals in marchmay , 2020 ( lawler m , unpublished ) .24 large backlogs of patients accrued as a consequence of the lockdown are predicted to first place pressure on diagnostic services in secondary care , and affect other areas of the pathway thereafter.5 we aimed to address two key questions relating to this potential surge in presentations of symptomatic patients . 
second , accounting for the risk of death associated with nosocomial severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection , we examined the gain in survival and life - years through prompt investigation per patients referred via 2 - week - wait investigatory referral by age group and tumour referral group ( the high - level grouping of tumour types via which referrals are made [ appendix 1 pp 45 ] )  . 
to do these analyses , we developed a model using data on 10 - year cancer survival for 200817 ( stratified by age and cancer stage ) combined with a per - day hazard ratio ( hr ) for delay and applied it to agespecific and stage - specific case and referral volumes based on the 2 - week - wait pathway.6 methods data sources in this modelling study , we obtained patient numbers , agestratified and cancer stage - stratified 5 - year ( 201317 ) and age - stratified 10 - year ( 200817 ) cancer survival data for all diagnoses , and those cancers associated with surgical resection for non - haematological malignancies , from public health englands national cancer registration and analysis service ( ncras ) , including by subtype of breast cancer ( appendix 1 pp 13 )  . 
we obtained data on route to diagnosis by age and cancer stage from national health services ( nhs ) england clinical commissioning groups collections.7 we used data on proportion of referrals for suspected cancer that translated into cancer diagnoses ( the diagnostic - con version rate ) from cancer waits - faster diagnosis standard data for west london , uk , for 201920.8 we used data from across england for cancer cases diagnosed when the patient was aged 30 years or older . 
we concentrated our analysis on the 20 most common cancers referred via 2 - week - wait pathways , for which we analysed ncras survival data from 2 314 822 cancer cases ( 200817 ) and 2 - week - wait diagnoses for 385 156 cancer cases ( 201316 ) ( appendix 1 pp 45 )  . 
 we calculated life expectancy on the basis of uk office of national statistics life tables for 201618.9 we estimated nosocomial infection rates and median duration of hospital stay for treatment of each cancer type on the basis of aggregated and anonymised information from 1036 vol 21 august 2020 articles three large uk surgical oncology centres ( gronthoud f , unpublished )  . 
since long - term survival rates for most cancers are only known 510 years after diagnosis , we used 10 - year cancer stage - specific survival data in our calculations . 
 because 10 - year stage - specific survival data are not directly available for recent cancer cohorts in england , we estimated these data using established methods , by taking the ratio of stage - specific to all - stage 5 - year survival data and applying it to 10 - year all - stage survival data.12 we used the midpoint per 10 - year age group for life expectancy to estimate life - years gained , averaged per patient.9 to calculate covid - 19 - related mortality in patients with cancer , we first estimated peri - surgical mortality from nosocomial infection as the product of operationspecific duration of surgical admission , age - specific casefatality rates , and the rate of nosocomial infection per day ( 1% , 2% , 5% , or 10% )  . 
then we estimated covid - 19related mortality in the community ascribing the patient a year of active cancer management status ; this estimate was the product of the likelihood of community - acquired covid - 19 during the year ( 1% , 10% , 20% , or 50% ) , agespecific case - fatality rates , and the increase in covid - 19 case - fatality rate as a consequence of cancer as a comorbidity ( two times or five times ) .10 , 11 for the calculation of the hr for per - day delay in management , we used published data on the impact of delay in cancer surgery on overall survival for stage iiii disease to estimate per - day hrs associated with delay to definitive treatment.1321 since sufficient observational data were only available to generate summary delay hrs for breast , colorectal , and bladder cancers , we assigned delay hrs to other tumours on the basis of similarity of 5 - year survival , categorising tumour progressiveness as being low ( with a 5 - year survival for stage ii disease being > 90% ) , moderate ( 5090% ) , or high ( < 50% )  . 
because of the scarcity of published observational data on tumours of high progressiveness ( eg , oesophageal and gastric cancers ) , we conservatively considered this group as having a similar delay hr as moderately progressive tumours ( appendix 1 pp 13 )  . 
finally , we assumed that delay to treatment for stage iv cancer would not affect 10 - year survival . because patients younger than 60 years with stage iiii cancers typically have treatment with curative intent , we generated the stage - specific ratio from this group of those having major resection to those having other definitive treatment ( eg , endoscopic resection or curative radiotherapy )  . 
we applied this ratio to age - specific and cancer stage - specific strata for those aged 60 years and older having major resection to estimate the proportion of patients who have been diagnosed who are having other types of definitive treatment . to estimate 10 - year survival for individuals diagnosed with stage iiii cancer who have no delay in treatment , we used ncras 10 - year survival data and adjusted for covid - 19 - related peri - surgical and community mortality . 
 to estimate 10 - year survival associated with delay , we applied the delay hr relating to the specified number of days of delay , along with the covid - 19 - related perisurgical and community mortality , to the ncras 10 - year survival ( formulas are in appendix 1 [ pp 13 ] )  . 
we conservatively assumed that no additional downstream delays would occur after the diagnostic delay . we quantified the annual numbers of cancers diagnosed via the 2 - week - wait pathway using the 2 - week - wait age - specific and stage - specific breakdowns . 
from these , our outcome measures were estimated aggregate number of lives lost and life - years lost in england for per - patient delays of 16 months . scenarios analysed using the model we assessed the scenario of a 3 - month period of lockdown during which a proportion of symptomatic patients delayed their presentation until after lockdown ( ie , backlog patients ) , set at 25% , 50% , and 75% of normal monthly volumes . 
we modelled all backlog patients presenting in month 1 after lockdown or with variable presentation across months 13 ( appendix 2 )  . lives and life - years we then did a per - patient riskbenefit analysis for 2 - week - wait investigatory referral . 
we combined per - day rates of nosocomial infection with the age - specific covid - 19 case - fatality rates to quantify the covid - 19 - related fatality associated with investigatory referral . 
we combined this estimate with a so - called tech nical fatality risk for invasive investigations ( eg , a one in 10 000 risk of death from perforation from colonoscopy ) 22 to produce a combined per - referral mortality . using the diagnostic - conversion rates , we estimated the survival benefit per patient from an investigatory referral for each age group and tumour group . 
we considered the potential to delay referral by 2 , 4 , and 6 months against varying rates of nosocomial infection per investigatory see online for appendix 2 vol 21 august 2020 1037 articles age group ( years ) 3039 4049 5059 6069 7079 bladder 1579% 1495% 1429% 1548% 1715% 1703% brain 1175% 1415% 1782% 1824% 1664% 1670% breast 488% 327% 249% 214% 371% 770% cervix 559% 903% 1220% 1573% 1798% 1552% colorectal 1022% 1138% 1082% 1059% 1310% 1636% kidney 501% 650% 853% 1053% 1310% 1741% larynx 1107% 1429% 1345% 1494% 1586% 1679% liver 1668% 1729% 1617% 1467% 1189% 1478% lung 1687% 1826% 1680% 1537% 1178% 670% melanoma of skin 313% 396% 489% 566% 732% 1256% oesophagus 1685% 1621% 1612% 1518% 1228% 459% oral cavity 1283% 1698% 1827% 1828% 1788% 1662% oropharynx 1179% 1448% 1677% 1831% 1708% 1373% ovary 724% 1387% 1738% 1828% 1708% 1586% pancreas 1286% 1176% 1211% 900% 718% 1074% prostate 068% 067% 032% 369% stomach 1858% 1854% 1803% 1734% 1611% 885% testis 058% 036% thyroid 011% 063% 035% 022% 063% 162% 257% uterus 243% 527% 868% 1183% 1443% 076% 133% 604% figure 1 : reduction in 10 - year net survival incurred from a 3 - month delay for the 20 most common tumour types , by age group red indicates the highest decile of survival decrement , scaling down through orange and yellow to pale green , which indicates the lowest decile of survival decrement . 
we estimated benefit in proportional survival and life - years gained from gain in cancer survival versus fatality risk ( covid - 19 and technical )  . the combined statistical analysis we combined indivi dual log ( hr ) s , by stage and days of delay , using weighted linear regression to calculate the summary per - day delay - log ( hr ) ( ie , delay hr ) and sd of this estimate ( ie , se ) , expressing it as a percentage of the estimate . 
we did multivariate sensitivity analyses across ranges of para meter estimates , including 2 sd of delay hr and per day nosocomial infection rates of 1% , 2% , 5% , and 10% . 
unless otherwise specified , we applied the default values for likelihood of community - acquired covid - 19 , which was 20% , and per - day rate of nosocomial infection , which was 2% , which were selected to be conservatively high . 
for cancer - related increase in mortality due to community - acquired covid - 19 , we used a default value of two times , which is at the low - tointermediate end of the published estimates ( reflecting a non - metastatic cancer population ; appendix 1 p 1 )  . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results for several cancers , including those of the colorectum , oesophagus , lung , liver , bladder , pancreas , stomach , larynx , and oropharynx , a 3 - month delay to diagnosis is predicted to result in a reduction in long - term ( 10 - year ) survival of more than 10% in most age groups ( figure 1 )  . 
differences in the effects of a 3 - month diagnostic delay were observed for different cancer stages across all tumour types and for different subtypes and stages of breast cancer ( appendix 1 p 7 )  . the aggregated impact of universal delays in the 2 - week - wait pathway on lives lost and life - years lost varies widely by tumour type ( figure 2 )  . 
these predicted outcomes are driven by aspects of the model including age - specific incidence , the proportion of cancers diagnosed via the 2 - week - wait pathway , the proportion of cancers diagnosed as stage iiii via the 2 - week - wait pathway , and tumour the aggressiveness of ( appendix 1 pp 45 )  . 
similarly , pancreatic , gastric , and liver cancers only contribute moderately to the estimated total lives and life - years lost because fewer patients present via the 2 - week - wait pathway and high proportions have stage iv disease at presentation ( appendix 1 pp 45 )  . the across the 20 cancer types , on average an estimated 243 098 cancers are diagnosed annually . 
of these , an estimated 96 289 are diagnosed via the 2 - week - wait pathway , of which 75 369 ( 783% ) are diagnosed at stage iiii ( table )  . 
20 293 ( 269% ) of 75 369 patients would be predicted to die due to cancer within 10 years of diagnosis , representing a loss of 304 129 life - years . 
a uniform per - patient delay of 1 month would be predicted to result in attributable additional lives lost of 1412 and 1038 vol 21 august 2020 articles attributable lives lost by length of delay attributable life - years lost by length of delay 1 month 2 months 3 months 4 months 5 months 6 months 1 month 2 months 3 months 4 months 5 months 6 months 2979 4633 6365 8139 9910 breast 41 845 22 678 1014 1312 1629 9839 15 339 21 255 27 608 34 418 cervix 2128 1246 1636 2054 colorectal 32 979 10 620 1366 1773 2196 4308 9126 14 460 20 296 26 591 33 275 number of cases diagnosed per year number of cases diagnosed per year via pathbladder 8524 3654 brain 8102 7642 3339 1161 1710 2142 1594 kidney 8764 2459 larynx liver 1850 4712 lung 36 668 10 343 melanoma of skin 12 110 oesophagus oral cavity oropharynx 7427 2629 2905 ovary 6398 pancreas 8260 prostate 40 834 19 272 stomach 5332 1654 testis 1355 thyroid 2673 1430 4733 3605 2501 1498 1171 1968 1079 6873 5403 2850 1415 3143 1692 4011 2145 1379 5239 4452 2344 5897 7471 3027 3725 9704 12 030 13 829 15 128 8756 12 614 17 028 22 051 4952 5665 6163 2864 1866 3551 4183 2347 2810 1411 2051 2619 3096 3475 1688 3445 7027 8765 10 406 uterus 7604 4390 1837 3932 6305 8970 11 936 15 201 total 243 098 96 289 1412 2892 4429 6013 7633 9280 25 812 53 057 81 589 111 263 141 950 173 540 figure 2 : annual lives and life - years lost attributable to delay , aggregated for all patients diagnosed via the 2 - week - wait pathway for the 20 most common tumour types based on 10 - year net survival data for england , uk , 200817 . 
greatest decrements in lives and life - years lost are shown in darker shades of orange . life - years lost of 25 812 and a per - patient delay of 6 months would be attributed to an additional 9280 lives and 173 540 life - years lost over the subsequent 10 years for an annual cohort of cancer cases diagnosed via 2 - week wait at stage iiii ( figure 2 )  . on the basis of preliminary estimates of 2 - week - wait referral decreases , we estimated the predicted effects of 25% , 50% , and 75% reductions in presentations over a 3 - month lockdown period ( appendix 2 ) .24 based on data for 201316 , for these 20 cancer types on average an estimated 149 000 2 - week - wait referrals are made each month , resulting in 8024 diagnoses of cancer , of which 6281 are diagnosed at stage iiii ( appendix 1 pp 45 )  . 
 1691 ( 27% ) of these 6281 patients will typically die from their cancer within 10 years.7 we estimated the national toll of presentational delay accrued over a 3 - month lockdown period to be 181 attributable additional lives and 3316 life - years lost for a backlog rate of 25% , 361 additional lives and 6632 life - years lost for a backlog rate of 50% , and 542 additional lives and 9948 life - years lost assuming a backlog rate of 75% , with an average presentational delay of 2 months per patient . 
assuming the patients all present in month 1 after lockdown , normal diagnostic capacity would need to work at least 175% under the 25% backlog scenario , 250% under the 50% backlog scenario , and 325% under the 75% backlog scenario to clear the backlog ( appendix 2 )  . 
however , it is unlikely that all extra diag nostic capacity required can be provided in a single month ; therefore , we estimated the additional lives and life - years that might be lost due to subsequent diagnostic delays . 
diagnostic conversion rates reflect all diagnoses of invasive cancers ( exceptions are that breast includes carcinoma in situ , skin excludes basal cell carcinomas , urology excludes pta bladder tumours )  . 
conversely , delayed additional capacity provided across months 38 after lockdown would result in 401 additional lives and 7332 life - years lost due to diagnostic delays under the 25% backlog scenario , 811 additional lives and 14 873 life - years lost under the 50% backlog scenario , and 1231 additional lives and 22 635 life - years lost under the 75% backlog scenario ( appendix 2 )  . we assessed the riskbenefit balance per individual for investigatory referral , considering different rates of nosocomial infection . 
first , we considered absolute survival benefit , comparing prompt referral , diagnosis , and management with no referral or subsequent medical intervention ( appendix 1 p 9 )  . 
if the risk of infection is high ( 25% per referral ) , for patients older than 70 years , the risk associated with investigatory referral might exceed the absolute survival benefit for tumour - referral groups with poorer outcomes , such as upper gastrointestinal ( pancreas , oesophagus , liver , and stomach ) and brain tumours ( appendix 1 p 9 )  . second , we sought to address a common dilemma for primary care physiciansnamely , to establish in which patients referral could be delayed by a few months , either to await reduction in nosocomial infection rates or to reduce pressure on diagnostic services . 
a 2 - month delay in 2 - week - wait investigatory referrals results in an average loss of between 00 and 07 life - years per referred patient , depending on age and tumour type ( appendix 1 p 12 )  . 
we compared risk of death from investigatory referral with delay - associated increase in risk of cancer death per patient referred ( figure 3 ; appendix 1 pp 1011 )  . 
factors associated with benefit of immediate referral over delay included younger patient age ( < 70 years ) , high tumour progressiveness , high diagnostic - conversion rates , and higher proportion of cases diagnosed with stage iiii disease ( appendix 1 pp 1 , 4 , 10 , 12 )  . 
for those younger than 60 years , provided daily nosocomial infection rates are 25% or lower , even for short delays ( 2 months ) the delayrelated cancer - fatality rate largely exceeds investigationrelated fatality . 
 sars - cov - 2 = severe acute respiratory syndrome coronavirus 2 . 1041 articles when the nosocomial infection rate is higher than 1% , investigation - related fatality for several tumour types of good prognosis ( eg , prostate , testicular , and thyroid ) or very poor prognosis ( eg , pancreas , liver , oropharynx ) is predicted to be greater than delay - related cancer fatality for as long as 6 months ( appendix 1 pp 1011 )  . 
bladder and kidney cancers exemplify tumour types for which prompt referral is most impactful , since these groups have a high diagnostic - conversion rate , the tumours are moderately progressive , but are predomi nantly stage iiii at diagnosis . 
in the event of stable , low nosocomial infection rate ( 05% per referral ) , we determined life - years lost for delayed referrals ( appendix 1 p 12 )  . 
for those referred with symptoms of bladder cancer , for a 2 - month delay the average decrement per referred patient is 069 life - years for those aged 3039 years and 010 life - years for those aged 7079 years ; for those referred with symptoms of brain tumour , the average decrement is 003 life - years for those aged 3039 years and 001 for those aged 7079 years . in multivariate sensitivity analyses , outcomes from the model were mostly sensitive to changes in the estimated per - day delay hr . 
varying the delay hr by 2 sds ( eg , 16% ) in the scenario of a 2% nosocomial infection rate , the total lives lost annually for the 2 - week - wait population attributable to a 2 - month delay ranged from 2412 to 3378 , and attributable life - years lost ranged from 44 192 to 62 055 ( appendix 1 p 13 )  . 
using a proportionately higher per - day delay hr for tumours of high pro gres sive ness ( delay hr = 00105 vs default delay hr = 00056 ) increased the impact of a 2 - month delay to 3772 lives lost and 72 053 life - years lost . 
varying the rate of nosocomial infection , the community infection rate , and the cancer mortality multiplier had a small effect on the impact of delay on survival . discussion for most solid cancers , 10 - year survival is generally considered to equate to cure , reflecting the proportion of stage iiii tumours for which their surgery ( or radical radiotherapy ) has enabled the restoration to normal or near - normal life expectancy . 
our estimates suggest that , for many cancers , delays to treatment of 26 months will lead to a substantial proportion of patients with earlystage tumours progressing from having curable to incurable disease . 
however , this varies widely between tumour types , reflecting variation in the proportion of patients diagnosed through the 2 - week - wait pathway , the proportion diagnosed with stage iiii tumours , the age profile of patients diagnosed with those cancers , and the diagnostic - conversion rate , which inevitably means that the overall impact of delays in referral via the 2 - week - wait pathway is far from uniform between cancers . during the lockdown in the uk in marchjune , 2020 , substantial temporal and geographical variation has been seen in rates of patient deferment in accessing urgent referral for cancer symptoms , with estimates as high as 84% ( lawler m , unpublished ) .2 , 3 substantial additional morta lity from diagnostic delay on top of the presentational delay accrued during patient deferment is possible , especially if additional diagnostic capacity for catching up with the backlog is delayed . 
the additional capacity must include not only expanded technical provision for endoscopy , imaging , interventional radiology , and nuclear medicine , but also increased staffing for specialist assessment and pathology . 
innovative solutions will be required to deliver this extra capacity in a timely fashion , which might include procurement of private sector provision , expanded roles for health - care professionals such as endo scopy nurses , and pathway adaptationeg , use of faecal im muno chemical testing ( fit ) for triage of colorectal cancer referrals . investment in expansion of capacity for nhs diagnostics and treatment is a priority if cancer services are to become more resilient to future extrinsic disruption , which could include additional waves of covid - 19 . 
furthermore , pre - emptive public education is required to discourage patients from deferring presentation of cancer symptoms along with modification of pathways to and through primary care . diagnostic delays will affect patient groups differently . 
conversely , for older groups ( 70 years ) , perreferral risk of death from nosocomial infection is much higher and might exceed the average decrement of a moderate delay , in particular for more indolent cancer types ( eg , prostate cancer ) or cancers with a poor overall prognosis ( eg , upper gastrointestinal tract cancers )  . 
even in the absence of concerns about nosocomial infection , if there are pressures on diagnostic capacity , prioritisation and deprioritisation of patients according to tumour referral group and age warrants consideration as a strategy to mitigate the population - level cost of diagnostic delays in terms of lives and life - years lost . whether or not deaths due to sars - cov - 2 infection , both direct and indirect ( eg , compromise in collateral health - care delivery ) will be outweighed by the positive impacts on mortality ( eg , reduced air pollution , fewer road - traffic accidents , and handwashing ) as a result of the covid - 19 and lockdown period is a matter of debate . 
 although our analyses examine cancer - specific survival only , the estimations of life - years gained would be altered by any sizeable shifts in life expectancy . here we used data for england , but cancer survival is similar across most economically developed countries , so we believe our estimates of the impact of delay for each tumour type are broadly applicable . 
overall , in areas where cancer incidence , population structure , and 1042 vol 21 august 2020 articles background rates of population mortality are broadly similar to those in england , our model would provide insights relevant to other health systems , although pathways to diagnosis for different cancers , eligibility criteria , and proportions of different cancers ascertained differ between countries . 
issues of capacity and delays in diagnosis are of global interest as part of moving towards bench marked metrics ( eg , international cancer benchmarking partnership ) .3 , 23 our analysis focused only on invasive disease in common adult tumour types . 
 additional analyses will be required to assess the impact of delays for those having non - curative treatments . as with all modelling , the accuracy of our predictions is contingent on the validity of assumptions and paraidentified suitable meter estimates . 
although we observational data for delays in treatment for stages iiii for three tumour types , uniform application of these delay hrs across tumour types and over time will invariably oversimplify the complex , dynamic , tumour type - specific , age - specific , and stage - specific nature of cancer pro gression . 
to enable systematic insights across tumour types , routine capture of delays in referral pathways should be incorporated into all national cancer data collections . our analyses at the level of referral are subject to the limitations of data collection for diagnostic - conversion rates , which were only available at the level of tumourreferral group , precluding analyses specific to age stratum or tumour type - specific symptomatology . 
further more , our analysis does not capture the impact of delay on survival when a 2 - week - wait referral resulted in diagnosis of a different cancer outside of the index tumour - referral group ( appendix 1 pp 45 )  . the current model presents a what - if prediction , in which we have included what we believe to be plausible estimates of delay applied in a simplistic non - naturalistic manner . 
the severity of local covid - 19 patterns , method - specific diagnostic capacity , and organisation of cancer services will all have an effect , as will local variation in pathway innovations in both diagnostics ( fit triage , colonography ) and treatment ( a priori use of radiotherapy and hormonal treatments )  . 
 initiatives such as data - can , the uk health data research hub for cancer , are assembling accurate realworld data quantifying in detail true delays and patient volumes and distributions ; these data could be applied to our models to refine our predictions . 
over the coming months , we will also be able to quantify whether the postlockdown surge in presentations directly mirrors the in standard 2 - week - wait deficit during lockdown presentations , or whether a proportion of these patients ( ie , do not need medical genuinely self - resolve attention ) .24 the availability of models such as those we have used will also enable more agile prospective resource planning in the face of future instances of systematic disruption of cancer services , which could include future major waves of covid - 19 , other pandemics , or economic contractions . although the linear elements vary for the different routes to diagnosis ( urgent , routine , emergency , and screen ing ) , at each step convergence exists in the resources used for diagnostics and treatment . 
for example , patients referred for suspected lung cancer typically receive a ct scan , but only a subset of patients have an endobronchial ultrasound or bronchoscopy ; nevertheless , subsequent pet - ct for staging might be the narrowest of bottlenecks in the lung pathway . 
to optimise recovery , integrated time - course health system analyses across different routes to diagnosis will be required , accounting for all the linear steps up to and including surgical and adjuvant treatment and considering local variation in bottlenecks to capacity.6 the impact of covid - 19 - related disruption on cancer care is likely to be an ongoing issue until a vaccine or effective treatment is identified . 
unlike acute pathologies , such as stroke and myocardial infarction , the true excess mortality due to covid - 19 - related disruption to cancer pathways will not be fully evident for 10 years or longer . contributors as , ct , and rh designed the model . 
mej , jb , ml , em , ct , rh , as , gl , er , dcm , and mw provided epidemiological expertise in the parameterisation of the model and relevant literature . 
cs reports grants from pfizer and boehringer ingelheim ; grants and personal fees from bristol myers squibb , astrazeneca , ono pharmaceutical , and roche - ventana ; personal fees from novartis , msd , illumina , celgene , glaxosmithkline , genentech , medicxi , and sarah canon research institute ; personal fees and stock options from grail ; stock options from epic biosciences and apogen biotech ; and personal fees and being a co - founder of achilles therapeutics during the conduct of the study . 
cs has patents issued for an immune checkpoint intervention in cancer ( pct / ep2016 / 071471 ) , for a method for treating cancer based on identification of clonal neo - antigens ( pct / ep2016 / 059401 ) , for methods for lung cancer detection for more on data - can see data - can - health - data - researchhub - cancer / vol 21 august 2020 1043 articles ( pct / us2017 / 028013 ) , for a method of detecting tumour recurrence ( pct / gb2017 / 053289 ) , for a method for treating cancer ( pct / ep2016 / 059401 ) , for a method of treating cancer by targeting insertion / deletion mutations ( pct / gb2018 / 051893 ) , for a method of identifying insertion / deletion mutation targets ( pct / gb2018 / 051892 ) , for a method for determining whether an hla allele is lost in a tumour ( pct / gb2018 / 052004 ) , for a method for identifying responders to cancer treatment ( pct / gb2018 / 051912 ) , and for a method of predicting survival rates for cancer patients ( pct / gb2020 / 050221 )  . 
jl reports grants and personal fees from achilles therapeutics , bristol - myers squibb , msd , nektar , novartis , pfizer , roche , and immunocore ; personal fees from astrazeneca , boston biomedical , eisai , eusa pharma , glaxosmithkline , ipsen , imugene , incyte , ionctura , kymab , merck sorono , pierre fabre , secarna , vitaccess , and covance ; and grants from aveo and pharmacyclics outside of the submitted work . 
gl is supported by a cancer research uk advanced clinician scientist fellowship award ( c18081 / a18180 ) and is associate director of the multi - institutional cantest collaborative funded by cancer research uk ( c8640 / a23385 )  . 
we aimed to assess the national impact of covid - 19 on the prescribing of systemic anticancer treatment in england , immediately after lockdown and after the introduction of new treatments to reduce patient risk . methods we did a retrospective analysis using data from a central national health service england web database mandated for clinicians to register intention to start all new systemic anticancer treatments approved for use in england since 2016 . 
we analysed the monthly number of treatment registrations in april , 2020 , after the implementation of societal lockdown on march 23 , 2020 , and after implementation of treatment options to reduce patient risk such as oral or less immunosuppressive drugs , in may and june , 2020 . 
we compared the number of registrations in apriljune , 2020 , with the mean number of registrations and sd during the previous 6 months of unaffected cancer care ( september , 2019 , to february , 2020 )  . 
we calculated the percentage change and absolute difference in sd units for the number of registrations overall , by tumour type , and by type and line of therapy . findings in april , 2020 , 2969 registrations were recorded , representing 1417 fewer registrations than in the control period ( monthly mean 4386 ; 32% reduction , absolute difference 42 sds , p < 00001 )  . 
in may , 2020 , total registrations increased to 3950 , representing a 10% reduction compared with the control period ( absolute difference 13 sds , p < 00001 )  . 
in june , 2020 , 5022 registrations were recorded , representing a 15% increase compared with the control period ( absolute difference 19 sds ; p < 00001 ] )  . interpretation after the onset of the covid - 19 pandemic , there was a reduction in systemic anticancer treatment initiation in england . 
however , following introduction of treatment options to reduce patient risk , registrations began to increase in may , 2020 , and reached higher numbers than the pre - pandemic mean in june , 2020 , when other clinical and societal risk mitigation factors ( such as telephone consultations , facemasks and physical distancing ) are likely to have contributed . 
additionally , strategies have been imple mented to reduce transmission of sarscov2 and protect patients and healthcare workers . patients with cancer can be particularly susceptible to covid19 due to several factors , such as advanced age , comorbidities , and the biologically plausible negative effect of the immunosuppressive nature of oncological treatment and cancer itself on the host response to sarscov2 infection.1 , 2 additionally , relatively frequent clinic visits for treatment and assessments might increase the risk of sarscov2 exposure in these patients . 
evidence on the effect of covid19 in patients with cancer has shown adverse outcomes in patients with cancer , such as higher mortality or higher probability of hospital admissions.311 the effect of systemic anticancer treatment on covid19 infection has not been fully recognised , although two large studies have reported no link between recent systemic anticancer treatment and increased mortality from covid19.12 , 13 many cancer services in england and elsewhere have undergone extensive changes to minimise covid19 exposure among patients with cancer and healthcare staff . 
these changes have included delayed surgery and radiotherapy , fewer chemotherapy treatment cycles , reduced outpatient visits ( often replaced with telephone assessments ) and , where possible , switching from therapies that require intravenous administration to oral drugs . 
diagnostic services have also been affected , with a clear reduction in cancer referrals.14 , 15 vol 22 january 2021 articles research in context evidence before this study due to the rapid emergence of severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) in england in 2020 , little evidence is available on the use of systemic anticancer treatments during this time . 
since the start of the covid - 19 pandemic , cancer services have been reduced to minimise viral exposure among patients with cancer ( an inherently susceptible population shown to have poor outcomes following covid - 19 infection ) and staff . 
data published in june and august , 2020 , have assessed the impact of systemic anticancer treatment on covid - 19 outcomes ; however , evidence on the use and provision of systemic anticancer treatment during the pandemic is scarce . added value of this study to our knowledge , this is the first study to assess how prescribing practice for anticancer treatments has changed at a national level since the pandemic began , based on all drugs approved by the national institute for health and care excellence since 2016 . 
we found that the number of patients who started these systemic therapies substantially reduced in april , 2020 , compared with a control period between september , 2019 , and february , 2020 , but began to increase in may , 2020 . 
these findings can provide some reassurance to patients and clinicians that treatment delays can be minimised or avoided if health - care providers are able to quickly implement guidance on drug prescribing . 
such guidance involves providing more treatment options via temporary approval of oral drug alternatives and the use of less immunosuppressive drugs in earlier lines of therapy , which are currently only licensed for use later in the treatment pathway . 
cytotoxic chemotherapies approved before 2016 and hormonal therapies are not included in our findings , so we are unable to comment on their prescribing patterns . implications of all the available evidence in england , which is a high - income country with an established health - care system , many patients did not start their expected systemic anticancer treatment in the early phase of the pandemic , although recovery of cancer therapy initiation in england was rapid . 
the impact of not prescribing or delaying systemic anticancer treatment on patient outcomes needs to be monitored in the forthcoming months , especially for non - curative therapies used for advanced disease ( some of which only extend survival by a few months ) , and for neoadjuvant treatment . 
considering the substantial impact estimated as a result of the second wave of covid - 19 , health - care systems should implement measures to ensure that patients with cancer can safely start their systemic anticancer treatment on time . guidance from the uk national health service ( nhs ) and the national institute for health and care excellence ( nice ) issued on march 20 , 2020 , aimed to aid clinical decision making by prioritising the need to retain systemic anticancer treatment services.16 clinicians were advised to categorise patients into six priority levels on the basis of their cancer stage and treatment : patients having highly curative treatment were assigned the highest level ( level 1 ) , and those being treated with noncurative therapies with an intermediate or low chance of palliation were assigned the lowest level ( level 6 )  . 
 translate considering the global nature of the pandemic and its effect on all healthcare services , similar guidance had also been published elsewhere , including by the european society of medical oncology.17 this guidance into in this study , we aimed to assess the impact of covid19 on the initiation of systemic anticancer treatment at a national level , during the first peak of the pandemic in april , 2020 , following societal lockdown on march 23 , 2020 , and after the nhs implemented additional and specific treatment options in april and may , 2020 , to mitigate the risk of covid19 in patients requiring systemic anticancer treatment . methods data sources we did a retrospective analysis using data from the nhs england prior approval system , which is a central web database mandated for clinicians to register inten tion for all patients commencing systemic anticancer treatment ( except hormone therapies ) for all drug indications recommended by nice since april , 2016 . 
 for each patient , clinicians select the appropriate indi cation , which includes cancer type , drug name , specific line of therapy in the treatment pathway , and mode of administration ( oral or intravenous )  . 
we extracted all available data for the period april 1 , 2019 , to june 30 , 2020 , and one author ( jjc ) used the indication descriptions to categorise intent of therapy ( curative or noncurative intent for advanced disease , and neoadjuvant or adjuvant intent for early stage disease ) , which was confirmed by a second clinician ( pc )  . 
all currently approved indications , including all treatment criteria that have to be satisfied for each indication , and the new covid19specific vol 22 january 2021 articles for the national cancer drug fund list see england.nhs.uk / cancer / cdf / cancer - drugs - fund - list / see online for appendix measures are included in the national cancer drug fund list . we classified all immunotherapies for solid tumours as noncurative in intent unless these were delivered with the specific indications of maintenance therapy ( eg , the potentially curative treatment of durvalumab following radical chemoradiotherapy in lung cancer ) or as adjuvant therapy in melanoma . 
the nhs england prior approval system captures all immunotherapies , all monoclonal antibodies ( excluding rituximab and trastuzumab ) , all antibodydrug conjugates , and the april , 2020 may , 2020 june , 2020 m unotherapies che m otherapies intravenous oral curative adjuvant neoadjuvant n on - curative therapy ( rst - line ) n on - curative therapy ( second - line ) n on - curative therapy ( third - line or later ) type and line of systemic anticancer therapy prostate follicular ly m pho m a and chronic ly m phocytic leukae mia w aldenstr m m acroglobulinae mia head and neck colorectal lung hepato - pancreato - biliary tumour type urothelial breast skin acute leukae mias m yelo m a other * renal gynaecological figure 1 : change in systemic anticancer treatment registrations for apriljune , 2020 , by intended treatment type and line of therapy ( a ) and tumour type ( b ) the number of registrations for april , may , and june , 2020 , were compared against the mean number for the control period . 
most cytotoxic chemotherapies are not included in the system because they were approved before 2016 . data analysis the main study outcome was the number of systemic anticancer treatment registrations recorded per month . 
 in england , societal lockdown was formalised on march 23 , 2020 ; therefore registrations during march reflect both normal use and the start of the impact of the pandemic in the healthcare systethus , we extracted the number of registrations recorded per calendar month in april , may , and june , 2020 . 
sept 1 , 2019 , to feb 29 , 2020 , was selected as the control period ( ie , the 6 months preceding april , 2020 , that were unaffected by the pandemic ) because these months were the closest in chronological time . 
the use of april to june , 2019 , as the control period would have been inappropriate because the number of systemic anticancer treatment regis trations is affected by the total number of newly approved drug indications , which differs for a particular month , from year to year . 
however , we also extracted data for the period of april 1 to june 30 , 2019 , to provide a secondary comparison . we calculated the mean number of monthly regis trations and accompanying sds for the control period . 
 we compared the mean number of monthly registrations in the control period with the number of registrations recorded per calendar month in april , may , and june 2020 , to calculate relative changes and absolute differences . 
we analysed data for april , may , and june , 2020 , separately because we had no expectations about any patterns and wanted to examine each month , and not fit trends . 
the absolute difference was calculated as the difference in sds from the monthly mean for the control period , to reflect the usual variability between the control months and to provide a standardised parameter considering that the number of registrations varies by tumour type , and line and type of therapy . 
nice recom mendations added two new indications in april , 2020 , ( larotrectinib and lorlatinib , both indications for a small number of patients ) and three new indications in may , 2020 ( atezolizumab for advanced triplenegative breast cancer and smallcell lung cancer and trastuzumab emtansine as adjuvant breast cancer therapy , all for potentially larger patient populations )  . 
other new treatment options in response to the pandemic were introduced on april 12 , 14 , and 28 , 2020 , and may 4 , 5 , and 22 , 2020 ( appendix pp 89 ) , which included oral drug alternatives and the earlier use of less immuno suppressive drugs only licensed for use later in the treatment pathway . in april , 2020 , 2969 registrations were recorded , which was lower than that in any month during the control period ( range 39224819 )  . 
compared with the mean number of registrations per month for the control period ( 4386 [ sd 335 ] ) , 1417 fewer registrations were recorded in april , 2020 , representing a relative reduction of 32% , and an absolute difference of 42 sds ( figure 1 , figure 2a ) , both of which were statistically significant ( p < 00001 )  . 
during may , 2020 , the total number of regis trations increased to 3950 , representing a 10% reduction compared with the control period ( 13 sd difference , p < 00001 )  . 
in june , 2020 , 5022 registrations were recorded , a 15% increase compared with the control period ( 19 sd difference , p < 00001 )  . for firstline noncurative therapies , the number of regis trations was significantly lower in april , 2020 ( relative reduction 30% ; absolute difference 48 sds , p < 00001 ) , similar in may , 2020 ( relative decrease 1% ; absolute difference 02 sds , p = 094 ) , and higher in june , 2020 ( relative increase 27% ; absolute difference 45 sds , p < 00001 ) , compared with the control period ( figure 2b )  . 
for secondline noncurative therapies , the number of registrations were significantly lower in april , 2020 ( relative reduction 36% ; absolute difference 33 sds , p < 00001 ) and may , 2020 ( relative reduction 25% ; absolute difference 23 sds , p < 00001 ) , and similar in june , 2020 ( relative increase 5% ; absolute difference 04 sds , p = 021 ) , compared with the control period ( figure 2c )  . 
the pattern was similar for thirdline non curative therapies or later ( figure 2d )  . compared with the control period , the number of registrations for immunotherapies decreased signifi cantly during april , 2020 ( relative reduction 39% ; absolute difference 54 sds , p < 00001 ) and may , 2020 ( relative reduction 10% ; absolute difference 14 sds , p < 00001 ) , but returned to typical levels in june , 2020 ( relative increase 7% ; absolute difference 10 sds , p = 0052 ; figure 3a )  . 
this pattern was similar for intravenous drugs ( figure 3b ) and a overall b first - line non - curative therapy 1417 fewer registrations ( 42 sds ) 532 fewer registrations ( 48 sds ) c second - line non - curative therapy 427 fewer registrations ( 33 sds ) d third - line non - curative therapy or later 332 fewer registrations ( 48 sds ) 2250 2000 1750 1500 1250 1000 m ay , 2020 april , 2020 february , 2020 n ove m ber , 2019 october , 2019 septe m ber , 2019 june , 2020 m arch , 2020 january , 2020 dece m ber , 2019 april , 2020 february , 2020 n ove m ber , 2019 septe m ber , 2019 june , 2020 m ay , 2020 m arch , 2020 january , 2020 dece m ber , 2019 october , 2019 month month figure 2 : the number of systemic anticancer treatment registrations observed per month , overall ( a ) and for first - line non - curative therapy ( b ) , second - line non - curative therapy ( c ) , and third - line or later non - curative therapy ( d ) the dashed horizontal line shows the mean number of registrations for the control period . chemotherapies ( figure 3c )  . 
for oral drugs , the number of registrations in april , 2020 , was significantly lower than the control period ( relative reduction 18% ; absolute difference 20 sds , p < 00001 ) , similar to the control period in may , 2020 ( relative increase 3% ; absolute difference 03 sds , p = 049 ) , and significantly higher than the control period in june , 2020 ( relative increase 28% ; absolute difference 33 sds , p < 00001 ; figure 3d )  . the reductions in the number of registrations in april , 2020 , were consistent across all groups , including intent of therapy , tumour type , line of noncurative therapy , and mode of administration ( the results and categories were not necessarily mutually exclusive ; appendix pp 1011 )  . 
for the four most common solid tumours , registrations were significantly april , 2020 , than the mean for the control period for each tumour type ( p < 00001 ; appendix p 4 )  . 
the number of registrations decreased by 33% ( absolute difference 42 sds ) for breast cancer , by 57% ( absolute differ ence 48 sds ) for prostate cancer , by 36% ( absolute difference 52 sds ) for lung cancer , and by 32% ( absolute difference 34 sds ) for skin cancers . 
during june , 2020 , the number of registrations for breast and skin cancer returned to typical levels , but were signifi cantly higher for prostate and lung cancer ( p < 00001 ) , with relative increases of 83% and 22% , respectively . lower vol 22 january 2021 articles a immunotherapies b intravenous drugs 322 fewer registrations ( 54 sds ) 1106 fewer registrations ( 60 sds ) 3000 2500 2000 1500 1000 2250 2000 1750 1500 1250 1000 1000 1400 1200 1000 c chemotherapies d oral drugs 556 fewer registrations ( 51 sds ) 309 fewer registrations ( 20 sds ) february , 2020 n ove m ber , 2019 october , 2019 septe m ber , 2019 m arch , 2020 january , 2020 dece m ber , 2019 m ay , 2020 april , 2020 june , 2020 m ay , 2020 april , 2020 february , 2020 june , 2020 m arch , 2020 n ove m ber , 2019 october , 2019 septe m ber , 2019 january , 2020 dece m ber , 2019 month month figure 3 : the number of systemic anticancer treatment registrations observed per month , for immunotherapies ( a ) , intravenous drugs ( b ) , chemotherapies ( c ) , and oral drugs ( d ) the dashed horizontal line shows the mean number of registrations for the control period . compared with the control period , the number of registrations remained significantly lower in may , 2020 , for neoadjuvant therapies , noncurative secondline therapies , noncurative thirdline therapies , cytotoxic chemo therapies , and intravenous drugs ( appendix p 10 )  . in june , 2020 , the number of registrations remained significantly lower than in the control period for neoadjuvant therapies , chronic lymphocytic leukaemia , and follicular lymphoma and waldenstrm macro globulinaemia . 
for all other tumour types , the regis trations were similar to or exceeded those in the control period . the covid19specific drug indications introduced by nhs england in april and may , 2020 , contributed substantially to the increase in the number of regis trations observed in may and june , 2020 . 
compared with april , 2020 , 2053 additional registrations were observed in june , 2020 , of which 896 ( 44% ) were for covid19specific drug indications . we also assessed the total number of monthly registrations between april 1 and june 30 , 2019 ( appendix p 7 )  . 
despite the usual variability in the number of new drug approvals per month and the expected seasonal decline in approvals in december , 2019 , the decreases between two adjacent months was larger between march and april , 2020 , than any other time period in the previous year ; and the increase between april and june , 2020 , was larger than that observed across any 2month period in the previous year ( appendix p 7 )  . 
 if april to june , 2019 , had been used as the comparison period ( mean number of registrations 3868 ) , the number of registrations observed in april , 2020 ( 2969 ) and june , 2020 ( 5022 ) would have remained significantly different ( p < 00001 ; appendix p 7 )  . discussion our study provides a national assessment of the effect of the covid19 pandemic on patients starting their systemic anticancer treatment , which is likely to be observed in other countries , particularly those with similar healthcare structures . 
we found that the covid19 pandemic had a negative impact on prescribing patterns in april , 2020 , at the start of the pandemic , followed by a quick recovery in most clinical scenarios by june , 2020 . the initial substantial reduction in april , 2020 , in patients starting recently approved systemic anticancer treatment drugs was probably due to several factors , including patient choice , clinical advice on the benefit and risks of starting treatment , and a reduction in referrals and subsequent diagnoses as a result of fewer patient presen tations or reduced service capacity . 
however , delayed diagnosis would have only affected patients having curative , adjuvant , neoadjuvant , and noncurative firstline treatments , which together comprised 56% of the population commencing registered systemic anti cancer treatments in the control period . 
additionally , we do not consider the changes observed between april and june , 2020 , to reflect seasonal variation since the only significant seasonal decline observed annually in registrations in the nhs occurs in december , which is modest . overall , the number of registrations significantly reduced at the start of the pandemic ( 32% reduction in april , 10% reduction in may ) , and the effect was greater for noncurative indications , particularly for later lines of therapy . 
compared with april , 2020 , marked increases in prescribing were observed in may , 2020 , particularly for curative and adjuvant treatments , immunotherapies , and firstline noncurative therapies , but reductions persisted by comparison to the control period , particularly for neoadjuvant therapies . 
by june , 2020 , the number of registrations was higher than the control period , a pattern that was observed for most intents of therapy and tumour types , with the exception of neoadjuvant treat ments and lowgrade lymphoid malignancies . the increases in registrations observed in may , 2020 , and particularly in june , 2020 , are likely to reflect both delayed initiation of treatment and an increase in referrals and diagnoses following the peak of the pandemic . 
 treatments given temporary approval by the nhs to vol 22 january 2021 articles reduce the risk to patients also contributed substantially to the increases observed in may ( 81% of the increase ) and june ( 44% of the increase )  . 
by june , a greater proportion of the increase was in routinely available treatments , signifying a substantial shift towards pre pandemic functioning with hospital systems making adjustments using physical distancing , tele phone consul tations , face masks , and routine sarscov2 testing with designated socalled clean treatment areas . 
these changes in prescribing reflect a healthcare system that can adapt quickly to the provision of new treatment options , many of which only became available in late april and early may , 2020 . the number of registrations for tumour subtypes such as prostate cancer and chronic lymphocytic leukaemia decreased substantially in april , 2020 . 
the typically older age of patients with these types of cancer , which has been associated with higher covid19 risk , and the less aggressive biology of these more indolent cancers , were likely to be factors when considering treatment delays . 
for example , for prostate cancer , the increase in registrations observed in may and june ( compared with the control period ) were likely to have been influenced by the introduction of firstline enzalutamide instead of chemotherapy for metastatic hormone sensitive prostate cancer . 
a reluctance to initiate therapy in lymphoid malignancy probably reflects the additional immunosuppression imposed by the disease itself and the reported high mortality among such patients with covid19 infection.18 , 19 a reduction in immunotherapy registrations was observed in april , 2020 . 
although immunotherapy is not generally considered to be immunosuppressive for most patients , it is likely that clinicians were reluctant to expose patients to multiple hospital visits and sought to avert treatment toxicity . 
 such concerns have not been corroborated in published reports , which have shown no association between pd1 blockade and covid19 severity.20 in april , 2020 , a larger reduction in intravenous treat ment registrations was observed than in oral therapy registrations , which reflects a strategy to maintain treat ment where possible , especially considering that many oral treatments ( eg , tyrosine kinase inhibitors ) are not strongly immuno suppressive and these drugs could be delivered to patients homes . 
a marked increase ( 28% ) was observed in june , 2020 , for oral drugs . some of the smallest reductions in registrations in april were observed for treatments deemed curative and adjuvant , reflecting their high longterm benefitrisk ratio . 
 examples of curative therapies that had fewer registrations include durvalumab after chemo radiotherapy for nonsmall cell lung cancer , and recently approved additions to chemotherapy for acute leukaemia , such as gemtuzumab ozogamicthe increase in curative treatments observed in may and june , 2020 , were likely to have been influenced by the provision of venetoclax combinations and gilteritinib for acute myeloid leukaemia . 
the adjuvant treatment regis trations were limited to her2positive breast cancer and melanoma , although the decrease in adjuvant therapies during april , 2020 , was largely observed for melanoma due to a decrease in adjuvant immunotherapy . 
one explanation for this reduction could be more aggressive risk stra tification , with less adjuvant treatment for patients deemed at lower risk of relapse , combined with a strategy to avoid potentially toxic treatment or hospital visits . 
the use of these adjuvant therapies increased quickly in may and june , 2020 , with the number of registrations increasing to numbers higher than that in the control period . the reduced number of registrations for neoadjuvant treatment is likely to reflect patients proceeding straight to surgery rather than risking chemotherapy complications and subsequent delays , and this pattern continued in may and june . our study has some limitations . 
first , the nhs registration system records an intention to treat that might not necessarily result in treatment itself , although previous audits have shown that 9295% of registrations result in actual treatment ( dominguezlezcano j , nhs england , personal communication )  . 
most adjuvant and neoadjuvant treatment for solid malignancies is conventional cytotoxic chemotherapy , which is not captured by the national registration syste similarly , many curative treatments were established before 2016 , including those for germcell tumours , lymphoma , and acute leukaemia , so data on these treat ments are not recorded . 
future patientlevel analyses might also show how age , sex , geographical location , tumour factors , and intent of therapy together affected the initiation of systemic anticancer treatment . the therapies listed on the national systemic anticancer treatment registration system have proven benefits for patients in terms of longer survival , or reduced risk of cancer progression or recurrence . 
failing to initiate or delaying these treatments by 12 months , particularly for patients with advanced cancers for whom approved vol 22 january 2021 articles drugs might improve survival by only a few months , could have negative consequences for patients . 
delays in treatment have been shown to lead to worse outcomes in some , 2123 but not all malignancies.24 similarly , the reduction in use of neoadjuvant therapies also requires assessment with regards to its effects on longerterm outcomes . our study shows the consequences of nhs england offering clinicians and patients a wide range of treatment options including drugs not yet appraised by nice or which are offlabel , but are likely to result in less risk to patients from the pandemic . 
the evidence from our study shows that these additional options contributed to the greater number of registrations for new patients starting systemic anticancer treatment in may and june , 2020 . in conclusion , our study has four key messages . 
 third , although it is important to consider a riskbenefit balance for each patient when determining the initiation of anticancer therapies , the emerging data on outcomes for patients receiving systemic anticancer treatment who contract covid19 highlight the need for continued scrutiny and discussion regarding overall gains of systemic anticancer treatment . 
many of these options were offlabel and the effects of these options will provide important data for healthcare providers . contributors jjc , ah , and pc created the initial concept and study design . 
jjc , dd , np , pc , pj , and ah were involved in writing the manuscript and the decision to submit for publication . declaration of interests jjc reports personal fees from pfizer , outside the submitted work . 
 pj reports grants from epizyme and janssen ; and personal fees from takeda , bristolmyers squibb , novartis , celgene , boehringer ingelheim , kite pharmaceuticals , and genmab and incyte , outside the submitted work . 
total numbers of registrations for the initiation of systemic anticancer therapies approved for use since july , 2016 funded by the cancer drugs fund are published by drug , indication , and month , and can be found online . 
registration data for drugs funded by the cancer drugs fund and by routine commissioning are subject to the rules governing freedom of information requests and nhs england can provide such data . 
the authors will not provide any raw data . acknowledgments this work was partly supported by cancer research uk ; ah is supported by a cancer research uk trials centre core grant to university college london ( c444 / a15953 )  . published online may 29 , 2020 s1470 - 2045 ( 20 ) 30312 - 0 for more on covid - 19 cases in maharashtra see mohfw.gov.in / for more on patients unable to travel home from mumbai see news / j%20&%20k / 44 - peopleincluding - 20 - cancer - patientstheir - attendants - stuck - inmumbai - since - march - 86958 for more on the delhi state cancer institute see com / india - news / 18 - healthcareworkers - of - delhi - state - cancerinstitute - test - positive - for - covid19 - hospital - shut / story u4j1ckevqoecscljikddgn.html for the modelling study see br j surg 2020 ; published online may 12 . 
the nationwide lockdown introduced to prevent spread of the virus has also had an impact on cancer care , since mumbai is a major destination for cancer treatment for patients from other states . 
 when the lockdown was announced on march 24 , many such patients were unable to travel home from mumbai after cancer treatment , while those scheduled for chemotherapy or surgery found it difficult to travel to mumbai , as all modes of transportation were suspended . 
the situation was similar in delhi , chennai , and bangalore , where large cancer hospitals are situated . more than 1 million new cases of cancer are reported in india every year . 
 at the beginning of the lockdown , the central ministry of health directed state governments to keep running non - covid - 19 - related essential health services , including cancer treatment and screening . 
however , few patients could access these services with no means of transport , and some hospitals , such as the delhi state cancer institute , were forced to shut outpatient units following covid - 19 outbreaks among staff . clinical services in most cancer centres remained curtailed for most of the lockdown , and few new cases of cancer have been registered . 
they are also scared of acquiring the infection in hospitals , not realising that cancer spread and the resultant poorer prognosis may be far more dangerous , explained ravi mehrotra ( chief executive officer , india cancer research consortium , new delhi , india )  . the tata memorial hospital in mumbai , however , continued to offer full services for patients who could access it during the lockdown period . 
we planned early on and initiated precautionary measures like restricting the number of attendants with each patient , banning visitors for inpatients , using teleconsultation for routine follow - ups , protecting vulnerable staff , maintaining supply chains and so on . 
their learnings were shared with members of indias national cancer grid and the city cancer challenge ( union for international cancer control , geneva , switzerland )  . the delay in treatment or detection of new cases is likely to affect the cancer burden soon . 
a global modelling study on the impact of the covid - 19 pandemic on surgeries projected that 597% of cancer surgeries were postponed in india during the peak 12 weeks of disruption , translating to 51 100 postponed cancer surgeries . delayed or postponed surgeries in tumours being might result upstaged and reaching the operation table at a later stage than they would have ordinarily . 
 both these scenarios may adversely affect long - term survivals and possibly lead to worse outcomes , commented dhruv ghosh , surgeon at christian medical college ( ludhiana , india ) and member of the global surgery research collaborative at the university of birmingham ( birmingham , uk )  . cancer in india is also a socioeconomic challenge . 
though treating hospitals are taking utmost care to best manage patients , increased out - of - pocket expense related to accommodation , food , medicines , and travel is an ongoing challenge which has accentuated during the lockdown , said yogendra kumar sapru of cancer patients aid association ( mumbai , india )  . 
when the lockdown ends , there will be a backlog , and we expect a sharp increase in the number of patients seeking financial assistance for treatment as many people have lost their livelihoods , he added . activities to promote cancer awareness and early diagnosis have also slowed down . 
on may 19 , 2020 , the indian government directed suspension of screening for oral cancers under the national cancer screening programme , on the basis of risks associated with examination of the oral cavity . pramesh added , cancer hospitals need to continue to provide cancer care while also managing patients with cancer and covid - 19 so that adverse cancer outcomes due to denied or delayed cancer care do not become a bigger problem than pandemic - related morbidity and mortality . dinesh c sharma 884 vol 21 july 2020 news the economic burden of cancer care for syrian refugees : a population - based modelling study rima a abdul - khalek * , ping guo * , forbes sharp , adrian gheorghe , omar shamieh , tezer kutluk , fouad fouad , adam coutts , ajay aggarwal , deborah mukherji , ghassan abu - sittah , kalipso chalkidou , richard sullivan , on behalf of the r4hc - mena collaboration summary background cancer represents a substantial health burden for refugees and host countries . 
we aimed to model the direct costs of cancer care among syrian refugee populations residing in jordan , lebanon , and turkey . methods in this population - based modelling study , direct cost per capita and per incident case for cancer care were estimated using generalised linear models , informed by a representative dataset of cancer costs drawn from 27 eu countries . 
a range of regression specifications were tested , in which cancer costs were modelled using different independent variables : gross domestic product ( gdp ) per capita , crude or age - standardised incidence , crude or agestandardised mortality , and total host country population size . 
total cancer care costs for syrian refugees in jordan , lebanon , and turkey were calculated by multiplying the estimated direct cancer care costs ( per capita ) by the total number of syrian refugees , or by multiplying the estimated direct cancer costs ( per incident case [ crude or age - standardised ] ) by the number of incident cancer cases in syrian refugee populations . 
all costs are expressed in 2017 euros ( )  . findings total cancer care costs for all 474 million syrian refugees in jordan , lebanon , and turkey in 2017 were estimated to be 14023 million using the cost per capita approach , 7902 million using the age - standardised incidence approach , and 3368 million using the crude incidence approach . 
under the lowest estimation , and with gdp and total country population as model predictors , the financial burden of cancer care was highest for turkey ( 2518 million ) , followed by lebanon ( 640 million ) , and then jordan ( 209 million )  . interpretation cancer among the syrian refugee population represents a substantial financial burden for host countries and humanitarian agencies , such as the un refugee agency . 
new ways to provide financial assistance need to be found and must be coupled with clear , prioritised pathways and models of care for refugees with cancer . funding uk research and innovation global challenges research fund : research for health in conflict - middle east and north africa region ( r4hc - mena )  . copyright 2020 the author ( s )  . 
however , the traditional humanitarian and refugee health response has focused on the provision of health - care services to address communicable diseases.3 the millions of refugees and internally displaced persons moving in and out of war zones through the middle east , asia , and europe illustrate the need to refocus the health response on ncds . 
 although major efforts have been made to fund the health sector by the un refugee agency ( unhcr ) and partner non - governmental organisations ( ngos ) , no analyses of the costs of delivering cancer care have been done . to identify studies reporting on the costs of cancer care in syrian refugee host countries , we did a literature search of medline , embase , and global health ( all via ovid ) for articles published between jan 1 , 2012 , and july 1 , 2019 , without language restrictions , to identify national estimates of direct costs for cancer care in jordan , lebanon , and turkey . 
we searched for articles related to cancer ( cancer or carcinom * or oncolog * or tumor * or neoplasm * ) and costs ( cost or economic or financ * or budget * or price * or pay * or reimburse * ) in the three host countries by searching the title , abstract , and keyword fields . 
we identified no cost - of - illness studies and less than 20 articles that focused on either specific cancer types or sites or on the cost of specific resources ( eg , drugs )  . 
previous cancer cost estimates were not directly comparable across the three countries , and they were insufficient to aggregate into the average cost per cancer case or per capita . added value of this study to our knowledge , this is the first study to estimate the cost of cancer treatment for syrian refugees in jordan , lebanon , and turkey . 
 we used different approaches to estimate costs : an approach that did not include the incidence of cancer in host countries ( cost per capita ) , and two approaches that adjusted for cancer incidence and estimated costs per incident cancer case ( either crude or age - standardised )  . 
the findings provide supporting information for planning the cost requirements for funding for cancer care , a disease with complex treatment pathways , by unhcr and partner ngos for syrian refugees . implications of all the available evidence our findings inform the dialogue between national governments , humanitarian actors , and donors on reducing cancer burden among refugees . 
the estimates of this study are important for decision making when planning funding for health care of refugees , and they contribute to the wider political economy evidence base on cancer care for refugees , internally displaced persons , and other vulnerable groups . 
in addition , host nations often struggle to provide adequate cancer services for refugees , partially due to the additional fiscal and health - care resource strains put on health systems in nations with refugee populations.12 however , in several countries neighbouring syria , the arrival of refugees has uncovered poorly developed pre - existing services and inadequate health system financing mechanisms , such as low health insurance coverage of local host populations and high out - of - pocket payments.13 , 14 for example , in lebanon , only 42% of the lebanese population are covered by public health insurance , and out - of - pocket payments represent 32% of total health expenditure ; in turkey , however , more than 90% of the population has public insurance and out - of - pocket expenditure represents 16% of health expenditure ( appendix 3 p 3 )  . provision of cancer care for refugees in the middle east and north africa region has been particularly challenging due to rising costs of care globally and the scarcity of effective cancer control plans in host countries.15 in addition , the quality of epidemiological , service - use , treatment effectiveness , and cost data from local ministries of health is low , and access to unhcr health registers is restricted . 
cancer registration among syrian refugees fluctuates according to changes in funding for the registries in jordan17 and other registries across the middle east and north africa region.18 in lebanon , syrian refugee cancer cases stopped being registered at the national cancer registry in 2015 ; thus , registered cancer cases might not be representative of the actual number of cases.19 for 246 approved cancer cases among refugees across syria and jordan , the mean expenditure approved per application was us$4626 ( range $41221 188 ) in 2011 , and $3501 ( $28918 873 ) in 2012 , 20 but these costs encompass only half of the cancer care funding requests submitted to the unhcr exceptional care committees . 
 given the scarcity of reliable data in the region , inadequate support for cancer care among refugees , and the fiscal and resource burden it presents for individuals 638 vol 21 may 2020 articles and host communities , generating estimates of the financial resources required to provide adequate care could help inform humanitarian resource planning and allocation . we present an econometric analysis of the financial burden of syrian refugees with cancer currently residing in jordan , lebanon , and turkey . 
we aim to fill some of the existing information gaps and inform the ongoing dialogue among national governments , humanitarian actors , and donors towards decisive , coordinated action to reduce the cancer burden among refugees . 
our approach could contribute to the wider political economy evidence base on cancer care for refugees , internally displaced persons , and other vulnerable groups . methods analysis framework with use of a population - based model , we estimated the direct costs of treating all cancers per annum among 474 million syrian refugees residing in jordan , lebanon , and turkey as of 2017.21 cancer was defined here using the who international classification of diseases , tenth revision , codes c0097 . 
the cost of treatment was defined as the cost of direct services provided by the respective national health system , specifically the cost of drugs and the use of four categories of health service : community services , outpatient visits , emergency room visits , and days spent as an inpatient ( eg , diagnostics , surgery , and radiotherapy )  . 
total costs were calculated using three approaches as the product of the estimated cancer care cost ( per capita , per incident cancer case [ crude ] , or per incident cancer case [ age - standardised ] ) and the total number of syrian refugees or syrian incident cancer cases , as appropriate , then summed across the three countries . 
prices were adjusted for inflation from 2009 to the most recent annual rate available ( year - end 2017 ) .22 the age - standardised data sources given the poor availability of data to estimate cancer treatment costs for syrian refugees , we made a pragmatic decision to use the validated cost dataset for cancer care in 27 eu countries ( hereafter referred to as the eu cancer dataset or eu cancer cost analysis ) 23 to estimate the average cost per capita and per incident case for syrian refugees in jordan , lebanon , and turkey ( appendix 3 p 4 )  . 
 the eu cancer cost analysis was based on data from several sources , including who , the organisation for economic co - operation and development , the statistical office of the european communities ( eurostat ) , national ministries of health , and statistical institutes . the six dependent variables derived from the eu cancer dataset were : number or frequency of health - care contacts ( per 1000 population ) ; cost per capita ( drugs plus services ) ; cost per capita ( services ) ; cost per capita ( drugs ) ; cost per incident case ( crude ) ; and cost per incident case ( age - standardised ; appendix 3 p 4 )  . 
the original cost per capita ( drugs plus services ) variable was split into its two constituent parts on the basis of evidence that the costs of drugs are potentially highly variable , and are affected by the markets , regulation practices , and other factors.24 , 25 we included the number of health - care contacts based on the hypothesis that there was a positive correlation between the frequency of service use and the burden of cancer within a given population . the cost per incident case was used to adjust costs at the final calculation stage and reflected the burden of cancer via the incidence of a given target population . 
three data sources were used to calculate this cost ( appendix 3 p 7 ) : the total cost for cancer services at the national level ( appendix 3 p 4 ) ; 23 national population figures ( appendix 3 p 5 ) ; 26 and national cancer incidence data ( appendix 3 p 6 ) .27 the crude and age - standardised incidences in this study refer to the reported incidence data for the year 2017 . six predictors of cancer care costs were selected on the basis of positive associations identified in the eu cancer cost analysis : gross domestic product ( gdp ) per capita , total country population size , crude incidence , age - standardised incidence , crude mortality , and agestandardised mortality ( appendix 3 p 8 )  . 
other health system financing variables , such as total health expenditure and public expenditure per capita , are correlated with gdp per capita , 28 and as such were omitted . 
we also considered using the density of radiotherapy equipment as a predictor of cost , but eurostat data are reported from 2015 onwards ( versus the reference year of 2009 in the eu cancer cost analysis ) and data were missing for seven countries ; therefore , it was excluded.23 estimation of cancer costs first , using regression diagnostic techniques , we tested for outliers within the eu cancer dataset with use of residual and standardised residual versus fitted value plots . 
we tested for a normal distribution of residuals using a normal q - q plot and tested for influential observations ( ie , countries or other observations that , when introduced into the model , induce significant changes to the model coefficients or regression line ) using cooks distance plot . 
using generalised linear models , single variable and multivariable regression models were constructed to predict average costs of cancer care in the eu cancer dataset , using cost per capita and cost per incident case approaches . 
we used a variety of distributions ( normal , inverse gaussian , gamma ) and compared the different models using the vol 21 may 2020 articles log and square - root links . 
the regression specifications with the best predictive performance were used to estimate costs of cancer care per capita and per incident case in jordan , lebanon , and turkey in 2009 , in euros , as per the eu cancer dataset , and later adjusted for inflation.22 these estimates were then multiplied by the corresponding number of individuals from the syrian population ( ie , the number of syrian refugees in each host country ) , and crude or age - standardised incidence in the syrian population ( which is expected to be the same in syrian refugees ) , to estimate total cancer care costs among syrian refugees in each country . 
when performing the out - of - sample pre dictions for cancer care costs in jordan , lebanon , and turkey ( ie , when values for some predictors [ eg , gdp ] were not in the range of values used for building the models in the eu cancer dataset ) , predictors were those of the host country . analyses were done using r statistical package version 3.6.0. 
model goodness - of - fit was measured using residual deviance ( by test ) and regression models were compared using the akaike information criterion , whereby models with a lower akaike information criterion were considered to have a better fit . 
given the small size of our dataset ( < 30 data points ) , we sought to prevent overfitting by specifying parsimonious models with up to two predictors . independent variables were tested in the final models in terms of both statistical and practical significance . 
 statistical significance was calculated at an level of 005 . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data and had final responsibility for the decision to submit for publication . results to understand the validity of our models we did a series of analyses to look at the distribution of variables . 
the distribution of most dependent variables was rightskewed ( ie , not normally distributed ) , with drug cost per capita closer to normal distribution than other variables ( appendix 3 p 10 )  . 
among the independent variables , the crude and age - standardised incidence and mortality variables were normally distributed ; however , gdp per capita and total population were right - skewed ( appendix 3 p 10 )  . 
therefore , for prediction purposes , log - transformed gdp and log - transformed total population size values were included in the models . for each of the dependent variables , associations were tested with six independent variables . 
an association was also noted between epidemiological variables ( incidence and mortality ) and the different types of costs , particularly for age - standardised mortality and age - standardised incidence . 
the dependent variable cost per capita ( drugs plus services ) showed stronger associations with almost all independent variables than did either of the component costs ( drugs or services ) when analysed in isolation ( appendix 3 pp 1114 )  . 
all independent variables showed weak associations with the dependent variable healthcare contacts ( data not shown ) ; therefore , it was excluded from additional models . all cost variables were strongly correlated with each other ( correlation coefficients 080098 ) , with the exception of the correlation between drug cost and service cost ( 068 ; appendix 3 p 14 )  . 
inde pendent variables ( incidence , mortality , gdp per capita , and country population size ) generally showed weaker corre lations with each other than did the cost variables ( appendix 3 p 14 )  . based on the associations between costs and independent variables , three costs were selected ( cost per capita [ drugs plus services ] , cost per incident case [ crude ] , and cost per incident case [ age - standardised ] ) to be modelled with the four independent variables that showed higher levels of association : log gdp , log population size , age - standardised incidence , and agestandardised mortality . after examining regression diagnostics in the eu dataset ( cooks distance plot for outliers , q - q plots for normality in response distribution , and plot of deviance residuals vs fitted values for linearity ) , luxembourg and greece were identified as outliers and excluded from the cost per capita and cost per incident case models , respectively . tested all models the association between the three selected costs and four independent variables ( models 115 ; appendix 3 pp 1517 )  . 
the model for cost per capita ( model 8 ) and the model for both cost per incident case ( crude ) and cost per incident case ( agestandardised ; model 5 ) had the lowest akaike information criterion across the three dependent variables . 
the final step of the modelling process adjusted the three estimated costs for either the population size or the cancer incidence of the refugee population , and for inflation of prices . for regression models that included country gdp and total population size as predictors in jordan , lebanon , and turkey , we estimated the total cost per capita using model 8 , and the total cost per incident case ( crude ) and total cost per incident case ( age - standardised ) using model 5 ( table )  . 
for practical reasons that outweigh the theoretical limitations , and because incidence is more 640 vol 21 may 2020 articles number of syrian refugees * incident cases ( crude ) incident cases ( age - standardised ) average costs , total costs , cost per capita cost per incident case ( crude ) cost per incident case ( age - standardised ) total cost per country ( per capita method ) total cost for cancer cases ( crude incidence method ) total cost for cancer cases ( age - standardised incidence method ) jordan 661 114 lebanon 1 001 051 turkey total 3 079 914 4 742 079 1033 3178 4893 1461 4494 6920 192 346 2779 5608 7169 4367 8910 12 075 1 041 710 21 348 457 2 094 721 6 401 953 117 835 418 25 179 655 140 225 585 33 676 329 4 657 732 14 385 792 59 973 338 79 016 862 regression dataset excludes luxembourg as an outlier in the cost per capita model , and greece in the cost per incident case models . 
 the incidence per 100 000 population ( crude or age - standardised ) can be calculated by dividing the incident cases by the syrian refugee population size and multiplying by 100 000 . 
from 2009 to 2016 ( most recent annual rate available ) ; a conversion factor of 1105102 was used to adjust for inflation of prices during this period . table : estimated costs for cancer - specific health - care services in the syrian refugee population in jordan , lebanon , and turkey for 2017 representative than the whole population size ( ie , the per capita method ) of the actual burden among cancer cases , we also report costs using the cost per incident case ( crude or age - standardised ) approach . 
the estimated total cost using the per incident case ( age - standardised ) method was 7902 million , and using the per incident case ( crude ) method was 3368 million . 
the agestandardised estimate of 7902 million translates to a cost of 11 417 per age - standardised incident case when con sidering a total of 6920 incident cases estimated in the three hosting countries . 
for the crude incident cases , which represent the actual cancer cost burden ( reflecting the current age structure of the syrian population ) , the estimated annual cost for providing cancer - specific care to the 474 million syrian refugees in jordan , lebanon , and turkey was 3368 million , comprising costs of 209 million in jordan , 640 million in lebanon , and 2518 million in turkey ( table )  . discussion in this study , we used two models to estimate the costs of cancer care for syrian refugees residing in jordan , lebanon , and turkey . 
we modelled the costs of cancer treatment in patients treated comprehensively and according to context - specific clinical guidelines applied to the refugee population in the middle east and north africa region using global and eu datasets . 
the estimated costs of care were for syrian refugees residing in jordan , lebanon , and turkey in particular , but they can be used to reflect on the needs of the wider refugee population . the positive correlation between cancer - related costs and the gdp of the country was expected , having been identified in the eu cancer cost analysis23 and other analyses.29 the correlation remains when health costs are expressed relative to at least one indicator of the burden of cancer in a population , such as cancer incidence or population size . 
moreover , cancer costs in high - income countries currently focus on expensive technologies and highly specialised services.30 our model was adjusted for both gdp and the total population size , and resulted in estimated costs that were lower than most high - income countries in europe . 
the use of age - standardised incidence allowed for the control of differing demographic profiles across samples and is considered a preferable method for corroboration purposes , because a dataset derived from one global region ( the eu ) is being used to estimate costs for a population in another region . 
 the substantially higher cost per incident case ( agestandardised ) than cost per incident case ( crude ) can be attributed to the fact that the refugee syrian population , and the syrian population in general , is young , with more than 50% of the population distribution between 15 and 64 years of age , which differs from the world standard population.21 , 31 the global refugee situation poses an enormous challenge to fragile health systems , and requires upscaling of the knowledge base and skills of health - care providers to respond to the needs of individuals , and must be addressed in the context of broader humanitarian and political issues.32 access to cancer services for refugees varies in jordan , lebanon , and turkey . 
the settlement of most syrian refugees outside of camps33 highlights the need to integrate cancer care into the existing health systems , and increase national capacities to provide cancer care to both nationals and refugees.34 , 35 additional care for refugees , if inte grated into such systems , would require changes and upscaling of capacities and resources . 
in jordan for example , availability and accessibility to opioids for the general population are interrupted , and information on diagnosis and prognosis is commonly concealed from patients.36 although specific details of cancer services in jordan , lebanon , and turkey are not known ( and are therefore difficult to corroborate ) , poor cancer outcomes due to low cancer - related health spending is a plausible interpretation of previous findings , considering the vol 21 may 2020 articles associations that have been identified between cancer outcomes and the availability of cancer services.37 , 38 the weak association between health - care contacts and explanatory variables could be explained by the frequency of health service use being affected by different healthcare - seeking behaviours and different levels of accessibility of services in host countries ; alternatively , the method applied in the eu cancer cost analysis to measure health - care contacts might not be representative of the actual use of services for cancer - specific support in jordan , lebanon , and turkey . in the context of humanitarian funding for the middle east and north africa region , the estimated overall cost of 3368 million ( approximately $38 million ) across the three host countries would constitute 110% of the annual budget of $345 million requested for syrian refugees in 2017 for jordan , lebanon , and turkey . 
in reference to what is actually funded , this represents 203% of the $187 million of funding for the health sector in 2017 for syrian refugees in the same countries.39 although a comprehensive analysis of cancer costs in the three middle east and north africa countries unavailable , previous studies have estimated specific costs for patients with cancer , and results are similar to our estimates for unit costs . 
for example , the direct medical cost for treating colorectal cancer in jordan was $10 114 per patient in 2014 ( equivalent to 7625 ) .40 this amount is slightly higher than our finding of 4367 per incident case ( age - standardised ) , although our estimate is not specific to colorectal cancer . 
for syrian refugees in jordan , the total cancer costs incurred at one centre were $114 million ( 97 million ) over 8 years ( 201118 ) , 17 which is higher than our estimate of $466 million at this centre . 
in lebanon , drug costs were $6475 per patient , as an average of expenditure during the years 20082013.41 when comparing the cost per incident case ( agestandardised ) between middle east and north africa and eu countries , estimated costs for lebanon and turkey were close to those in latvia and romania ( appendix 3 p 4 ) , whereas the cost for jordan was lower , and close to that for bulgaria ; therefore , for all three host countries , the estimated costs for cancer care among syrian refugees were among the lowest amounts spent by countries providing cancer care through their health systems . 
 countries such as bulgaria and slovenia had similar costs of 124 million and 145 million , respectively , but the cancer incidence in these countries was higher ( appendix 3 p 4 )  . a limitation of this study was the sample selected for analysis , which included only refugees and might not be representative of the wider population of persons of concern , as defined by the unhcr . 
the cost estimates used to predict cancer costs were transferred from european datasets , where reported incidence is much higher than in the middle east and north africa region , resulting in high cost per capita estimates . 
because of substantial variations in care provision between cancer services in each country and across countries , individual - level resource use data could be collected and used in future studies to ensure that more accurate cost data are calculated , rather than estimated with average costs . 
additionally , the types of cost estimated might not represent the necessary funds for cancer control programmes or systems , but instead represent the patient - centred costs ; as such , they ignore the costs of capital investments needed to provide the necessary services . 
the european cancer cost dataset does not distinguish between cancer stages , and therefore our estimates do not account for the proportion of cases diagnosed at each stage in each country . 
although evidence suggests that costs of care increase with stage at diagnosis , for example in breast cancer , 42 there are differences across cancer types in terms of selecting the cost predictors in the regression models.43 we adopted a pragmatic approach aligned with the european cancer cost analysis , given the scarce evidence on country - level predictors of cancer care costs , particularly in low - income and middle - income countries . 
further research should prioritise improving the performance of cross - country cancer cost models to improve the accuracy of such estimates when local data are not yet available . when considering funding for cancer care among refugees in wider international efforts to support cancer care , efforts are disorganised and inadequately funded.16 previous work from iraq showed that of 164 refugees diagnosed with a primary cancer , 79 ( 48% ) had attempted resettlement , indicating possible treatment insecurity and a lack of supportive cancer care.44 however , cancer among syrian refugees has remained largely unaddressed in the humanitarian response , mostly because of unhcr financial constraints.17 evidence from the global burden of disease study described cancer control in the eastern mediterranean region as having deficits in prevention , detection , diagnostics , treatment , and palliation.5 refugee cancer care is inefficient when taking into account the pre - existing vulnerability of the host populations in jordan , lebanon , and turkey . our results provide an initial indication of the magnitude of the cancer burden among syrian refugees and can inform the regional multi - stakeholder dialogue on coordinating action plans , scaling up existing initiatives , and investing in infrastructure and data systems . 
funding for cancer needs to go beyond current unhcr financing mechanisms ; sustainable , inclusive , and com prehensive financing mechanisms under the universal health coverage umbrella are necessary to account for the health needs of refugee populations and host communities , building on the political commitment taken by the governments of jordan , lebanon , and turkey towards universal health coverage . 
evidence from countries with privatised health - care systems , such as india , show that 642 vol 21 may 2020 articles low health insurance coverage for patients with cancer leads to catastrophic health expen ditures and families falling into poverty.45 the iraq and india case studies indicate that refugees travelling to different countries seeking cancer care in particular can accelerate financial catastrophe because of additional costs associated with travel and mobility . 
context - specific treatment protocols and guaranteed access and continuity of treatment will be crucial for improving models of cancer care in conflictaffected regions.46 the use of resource - stratified guidelines could help to ensure better access to , higher quality of , and fewer disparities in cancer care.16 contributors raa - k , pg , fs , ag , and rs conceptualised and designed the study . 
raa - k , pg , fs , ag , aa , and rs wrote the first draall authors reviewed and commented on drafts of the paper . declaration of interests we declare no competing interests . acknowledgments this publication is funded through the uk research and innovation global challenges research fund : research for health in conflict - middle east and north africa region ( r4hc - mena ) , project number es / p010962 / 1 . 
ag and kc are members of the mrc centre for global infectious disease analysis , jointly funded by the uk medical research council ( mrc ) and the uk department for international development ( dfid ) under the mrc / dfid concordat agreement and also part of the edctp2 programme supported by the eu . 
grant reference and affiliation : mr / r015600 / 1 ; mrc centre for global infectious disease analysis , school of public health , imperial college london ( london , uk )  . adjuvant dabrafenib plus trametinib versus placebo in patients with resected , brafv600 - mutant , stage iii melanoma ( combi - ad ) : exploratory biomarker analyses from a randomised , phase 3 trial reinhard dummer * , jan c brase * , james garrett , catarina d campbell , eduard gasal , matthew squires , daniel gusenleitner , mario santinami , victoria atkinson , mario mandal , vanna chiarion - sileni , keith flaherty , james larkin , caroline robert , richard kefford , john m kirkwood , axel hauschild , dirk schadendorf , georgina v long summary background adjuvant dabrafenib plus trametinib reduced the risk of relapse versus placebo in patients with resected , brafv600 - mutant , stage iii melanoma in the phase 3 combi - ad trial . 
this prespecified exploratory biomarker analysis aimed to evaluate potential prognostic or predictive factors and mechanisms of resistance to adjuvant targeted therapy . methods combi - ad is a randomised , double - blind , placebo - controlled , phase 3 trial comparing dabrafenib 150 mg orally twice daily plus trametinib 2 mg orally once daily versus two matched placebos . 
study participants were at least 18 years of age and underwent complete resection of stage iiia ( lymph node metastases > 1 mm ) , iiib , or iiic cutaneous melanoma , per american joint committee on cancer 7th edition criteria , with a brafv600e or brafv600k mutation . 
we assessed intrinsic tumour genomic features by use of next - generation dna sequencing and characteristics of the tumour microenvironment by use of a nanostring rna assay , which might provide prognostic and predictive information . 
this trial is registered with clinicaltrials.gov , number nct01682083 , and is ongoing but no longer recruiting participants . findings between jan 31 , 2013 , and dec 11 , 2014 , 870 patients were enrolled in the trial . 
median follow - up at data cutoff ( april 30 , 2018 ) was 44 months ( iqr 3849 ) in the dabrafenib plus trametinib group and 42 months ( 2149 ) in the placebo group . 
 tumour mutational burden was independently prognostic for relapse - free survival in the placebo group ( high tmb , top third ; hazard ratio [ hr ] 056 , 95% ci 037085 , p = 00056 ) , but not in the dabrafenib plus trametinib group ( 083 , 95% ci 053132 , p = 044 )  . 
patients with tumour mutational burden in the lower two terciles seem to derive a substantial long - term relapse - free survival benefit from targeted therapy ( hr [ versus placebo ] 049 , 95% ci 035068 , p < 00001 )  . 
however , patients with high tumour mutational burden seem to have a less pronounced benefit with targeted therapy ( hr [ versus placebo ] 075 , 95% ci 044126 , p = 027 ) , especially if they had an ifn signature lower than the median ( hr 088 [ 95% ci 040193 ] , p = 074 )  . interpretation tumour mutational burden alone or in combination with ifn gene expression signature or other markers for an adaptive immune response might be of relevance for identifying patients with stage iii melanoma who might derive clinical benefit from targeted therapy . 
reports from two prospective phase 3 trials of braf or mek inhibitor regimens in patients with resected brafv600 - mutant melanoma ( vemurafenib and dabrafenib plus trametinib ) and two phase 3 trials of adjuvant anti - pd - 1 therapies ( pembrolizumab and nivolumab ) were identified . 
results from a biomarker analysis of patients treated with adjuvant nivolumab or ipilimumab in the checkmate 238 trial were presented at the european society for medical oncology congress 2019 and showed the highest clinical benefit with both treatments in patients with a tumour mutational burden and interferongene expression signature greater than the median and lesser clinical benefit in patients with tumour mutational burden and interferonsignature smaller than the median . 
our search also identified a comprehensive biomarker analysis in patients with metastatic tumours treated with pembrolizumab , which showed enhanced response to anti - pd - 1 therapy in patients with high tumour mutational burden and a t - cell - inflamed signature . added value of this study we report findings from an analysis of mutational and gene expression profiling done on tissue samples collected at baseline and at relapse from the phase 3 combi - ad trial evaluating adjuvant dabrafenib plus trametinib versus placebo in patients with resected brafv600 - mutant stage iii melanoma . 
by contrast , patients with tumour mutational burden in the upper tercile seem to have less pronounced treatment benefit , particularly if they had a low interferongene signature ( expression equal to or below the median )  . implications of all the available evidence to our knowledge , this study is the first large - scale biomarker analysis with comprehensive dna sequencing and gene expression profiling in patients treated with targeted therapy in the adjuvant setting for melanoma . 
there are no predictive clinical or biological characteristics that identify patients with brafv600 - mutant melanoma who are most likely to benefit from available therapies ; the mechanisms of resistance to targeted therapy are heterogeneous , 6 and those associated with immune checkpoint inhibitors are largely unknown . 
evidence from studies of patients with metastatic tumours has implicated tumour mutational burden ( tmb ) and a t - cell - inflamed tumour microenvironment in the response to immune checkpoint inhibitors.711 a large - scale analysis in patients with advanced cancers treated with pembrolizumab7 showed that tmb and a t - cell - inflamed gene expression signature exhibited joint predictive utility in identifying responders and non - responders . 
results showed that patients with both a high tmb and a high t - cell - inflamed gene expression signature had the best outcomes and those with a low tmb and low t - cell - inflamed signature had the worst . 
similar results were reported in patients vol 21 march 2020 articles treated with adjuvant nivolumab in the checkmate 238 trial , with good clinical outcomes observed in patients with above - median tmb and interferon ( ifn ) expression and worse outcomes in patients with belowmedian tmb and ifn expression.12 although some evidence suggests that tmb and t - cell - inflamed gene expression signature together might provide the basis for a response axis in patients treated with immunotherapy , these markers have not yet been analysed together in patients receiving targeted therapy . 
 additionally , braf amplification and map2k1 / mek1 mutations ( among other mapk pathway alterations ) have been identified as putative resistance mechanisms to mapk pathway inhibitors in advanced melanoma and are frequently found in patients at the time of progression on braf or mek inhibitor therapy in the metastatic setting but are rarely detected before mapk inhibitor therapy.6 here , we report findings from an analysis of mutational and gene expression profiling done on tissue samples from the combi - ad trial that were collected at baseline and at relapse to evaluate potential prognostic or predictive factors and mechanisms of resistance to adjuvant targeted therapy . methods study design and participants combi - ad is a randomised , double - blind , placebocontrolled , phase 3 trial.1 eligible patients ( aged 18 years ) had complete resection of histologically confirmed stage iiia ( lymph node metastasis > 1 mm ) , iiib , or iiic cuta neous melanoma ( per american joint committee on cancer 7th edition ) that was positive for a brafv600e or brafv600k mutation confirmed in primary tumour or lymph node tissue by a central reference laboratory . 
 patients were required to have undergone and recovered from a complete lymphadenectomy without clinical or radiographic indication of regional nodal disease within 12 weeks of randomisation and to have an eastern cooperative oncology group performance status of 0 or 1 . patients were required to have adequate organ function , including haematological , hepatic , renal , and cardiac function . 
women of childbearing potential must have had a negative serum - subunit human chorionic gonadotropin pregnancy test within 7 days of the first dose of study treatment and agreed to use effective contra ception from 14 days before randomisation , throughout the treatment period , and for 4 months after the last dose of study treatment . patients were excluded if they had mucosal or ocular melanoma . 
patients presenting with initial resectable lymph node recurrence after a diagnosis of stage i or ii melanoma were eligible ; however , those with an unknown primary melanoma were not . 
patients were also ineligible if they had received an investigational anticancer drug within 28 days or five half - lives , whichever was longer , before randomisation , or if they had current or expected use of a prohibited medication . 
the investigator or designee contacted an interactive voice response system to register , randomly assign , and stratify patients by braf mutation type ( v600e or v600k ) and american joint committee on cancer 7th edition disease stage ( iiia , iiib , or iiic )  . 
matching placebos were used to ensure masking . procedures patients were randomly assigned to receive either oral dabrafenib 150 mg twice daily plus oral trametinib 2 mg once daily or two matched placebos . 
disease assessments by imaging using ct , mri , or both were done every 3 months for the initial 24 months and then every 6 months until study completion or disease relapse . 
 dermatological evaluations for disease recurrence or dermatological adverse events were done every 2 months during treatment , every 3 months during follow - up for the first 24 months , and every 6 months thereafter . if a dose adjustment was required , doses of both treatments were reduced simultaneously , with the exception of dose reductions for pyrexia , hypertension , or valvular toxicity ( reduce or interrupt dabrafenib dose only ) , and dose reductions for visual changes ( including retinal vein occlusion and central serous retinopathy ) , left ventricular ejection fraction reduction , rash , or pneumonitis ( reduce or interrupt trametinib dose only )  . 
 for dabrafenib , the dose was reduced to 100 mg on first reduction and 75 mg on second reduction ; however , the dose was not reduced to less than 75 mg . 
trametinib was reduced to 15 mg on first reduction and 1 mg on second reduction ; however , the dose was not reduced to less than 1 mg . 360 vol 21 march 2020 articles all patients in the combi - ad trial had surgical resection of the primary tumour and lymph nodes . 
 tissue samples were submitted for central braf testing at the time of screening , which was done using the biomrieux ( marcy letoile , france ) braf thxid assay in several sponsor - designated central laboratories . 
 a pathologist visually inspected archival formalin - fixed paraffin - embedded slides and freshly cut slides from the tumour blocks to identify and notate the approximate percentages of tumour content in the region of interest and total tumour area ( mm )  . 
dna and rna was coextracted from each baseline or relapse sample available using the qiagen ( hilden , germany ) allprep rna / dna extraction from a formalin - fixed paraffinembedded tissue kit . 
samples for biomarker analysis were excluded only if they did not pass quality control ( appendix pp 12 )  . for targeted sequencing and tumour mutational burden ( tmb ) analysis , dna was sheared ( covaris ultra sonicator ; woburn , ma , usa ) , and end repair , a - tailing , indexed adaptor ligation , and pcr amplification was done with the truseq nano library preparation kit ( illumina ; san diego , ca , usa )  . 
the next - generation sequencing library was denatured and hybridised to a set of rna baits designed to bind to fragments from specific genomic regions targeting 570 solid tumour - associated genes . 
the captured libraries were sequenced on an illumina hiseq using version 4 chemistry and producing 100 bp paired - end reads , achieving a mean target coverage of 550 times across sequenced libraries . 
quality control and downstream processing are outlined in the appendix ( p 1 )  . for gene - expression profiling , a customised nanostring gene panel of 800 genes ( 780 genes of interest and 20 housekeeping genes ) was used to assess rna . 
 per sample , up to 200 ng of rna was analysed on the nanostring counter platform . a previous study7 using datasets from the cancer genome atlas ( tcga ) showed that distinct patterns of underlying biology could be identified in a pooled analysis of multiple tumour indications using tmb and a t - cell - inflamed gene expression signature . 
to understand whether the same gene expression modules in brafv600 - mutant and subgroups are detectable melanoma and to evaluate the prognostic performance of tmb and ifn signatures , as well as underlying biology , we analysed the available rna sequencing datasets from brafv600 - mutant tumours of the tcga dataset across all stages , including patients with early and advanced melanoma . 
to understand whether the tmb and ifn subgroups had features , we simultaneously correlated genes and gene sets against tmb and ifn ( appendix p 2 )  . specific biological full methods for the biomarker analyses are detailed in the appendix ( pp 13 )  . outcomes the primary outcome of the combi - ad trial was relapsefree survival , defined as the time from randomisation until disease relapse ( or new primary melanoma ) or death from any cause . 
secondary outcomes were overall survival ( defined as the time from randomisation to the date of death , irrespective of the cause of death ) , distant metastasis - free survival ( time from randomisation to the date of first distant metastasis or date of death , whichever occurred first ) , freedom from relapse ( time from randomisation to recurrence , with censoring of data for patients who had died from causes other than melanoma or treatment - related adverse events ) , and safety . 
biomarker analysis , including mutation analysis in tumour tissue at baseline and relapse , pyrexia - associated cytokine assessment , characterisation of soluble proteins and systemic immune response in plasma , and molecular characterisation of treatment - emergent malignancies , was a prespecified exploratory outcome of the trial . 
this article reports analysis of tumour dna and rna samples to molecularly collected at baseline and relapse characterise relapses , analyse prognostic and predictive markers , and immune functions . statistical analysis this trial was designed to have at least 90% power to detect a 40% improvement in relapse - free survival with the combination therapy ( hr 07143 ; median relapsefree survival of 15 months in the placebo group and 21 months in the combination therapy group )  . 
the final analysis for relapse - free survival will be done when 467 events ( relapses or deaths ) have occurred . for these analyses , patient treatment group labels were those they were assigned at randomisation . 
in addition to the biomarkers and the treatment group , several other variables were evaluated as possible covariates to include in models : braf mutation type ( v600e or v600k ) and disease stage , which were used to stratify treatment randomisation , and tissue source ( lymph node , primary tumour , or in - transit metastases ) , age , sex , and number of involved lymph nodes . non - proportionality of hazards between the treatment and control groups was identified on the basis of exploratory semiparametric modelling ( appendix pp 23 ) and visual inspection of the kaplan - meier plots . 
the corresponding author had full access to all the data and had the final responsibility for the decision to submit for publication . results between jan 31 , 2013 , and dec 11 , 2014 , 870 patients from 169 hospitals and cancer institutes across 25 countries were enrolled ( appendix pp 47 )  . 
most baseline tissue samples were obtained from the primary tumour ( 305 [ 35% ] of 870 ) or locoregional lymph nodes ( 524 [ 60% ] of 870 ; table 1 )  . 
of the 870 patients enrolled , evaluable data for dna sequencing were obtained at baseline from 368 patients ( 42% ) and for geneexpression profiling from 507 ( 58% ) , with paired data available for 301 patients ( appendix pp 4951 )  . 
median follow - up at the time of the analysis was 44 months ( iqr 3849 ) in the dabrafenib plus trametinib group and 42 months ( 2149 ) in the placebo group . 
 hr estimates ( mutation vs no mutation ) within each treatment group and hrs ( dabrafenib plus trametinib vs placebo ) within mutation and no - mutation groups with 95% cis are shown , based on univariate cox models , as well as p values from log - rank tests . 
 similarly , when data from patients with at least one mapk pathway gene mutation at baseline were combined , no association with a change in clinical benefit from targeted therapy was observed ( figure 1 ) , even when only known activating mutations of oncogenic drivers were selected ( appendix p 52 )  . 
 although sample sizes precluded formal statistical comparisons , no noticeable differences were observed in clinical outcome and treatment benefit for patients with tumours that had the most frequently mutated tumour suppressor genes ( including inactivating mutations in cdkn2a , pten , and tp53 ) detected before therapy ( appendix pp 5354 )  . to investigate possible genomic characteristics of disease recurrence , we analysed available genomic data from 53 patients who had relapsed ( appendix p 8 )  . 
there was also no significant difference in tmb between baseline and relapse samples ( paired t test , p = 030 ) in both groups ( appendix p 56 )  . 
we also did not find differences in genetic alterations or potential resistance mechanisms between early relapse events ( on treatment or < 90 days after treatment discontinuation ) and late relapse events or subgroups with high versus low tmb , but the sample size of these subgroups was small ( data not shown )  . median tmb was 73 single - nucleotide variants per mb ( iqr 41113 ) in baseline tumours . 
simlar to results from a previous report , 14 baseline tmb was significantly higher in tumours with the brafv600k mutation ( wilcoxon rank - sum p < 00001 ; appendix p 57 )  . 
the hr estimates ( high tmb vs low tmb ) within each treatment group and hrs ( treatment vs placebo ) within tmb high and low groups with 95% cis are shown , based on univariate cox models . 
the p value for treatment interaction based on this kaplan - meier analysis ( using discrete tmb ) and the corresponding cox model not adjusting for other factors , is 016 for relapse - free survival , although the reliability of this test is questionable due to non - proportional hazards by treatment group . 
tmb = tumour mutational burden . associated with clinical outcome or response to therapy ( data not shown )  . tmb was significantly associated with relapse - free survival in the placebo group using the continuous tmb values and tmb subgroups ( high tmb , top third quantile ; hr 056 , 95% ci 037085 , p = 00056 ; figure 2 ; table 2 )  . 
in patients treated with dabrafenib plus trametinib , however , there was no significant association between continuous tmb values or tmb subgroups and relapse - free survival ( hr 083 , 95% ci 053132 , p = 044 ; figure 2 ; table 2 )  . because exploratory semiparametric modelling indicated non - proportionality with respect to treatment ( data not shown ; also supported by kaplan - meier curves ; figure 2 ) , we fitted cox models for the trial groups separately . 
 tmb was significantly associated with relapse - free survival after adjusting for stage in the placebo group , whereas no significant association existed with tmb in the multivariate analysis in the dabrafenib plus trametinib group ( continuous tmb [ table 2 ] ; similar results were observed in tmb subgroups ; appendix p 9 )  . the subgroup analyses also showed that patients with low tmb derived more benefit from adjuvant therapy with dabrafenib plus trametinib ( hr [ vs placebo ] 049 , 95% ci 035068 , p < 00001 ) than patients with high tmb ( hr [ vs placebo ] 075 , 95% ci 044126 , p = 027 ; figure 2 )  . 
we did not identify a significant interaction between tmb subgroups ( high vs low ; p = 022 when baseline stage iiib stage iiic dabrafenib plus trametinib group placebo group hazard ratio ( 95% ci ) p value hazard ratio ( 95% ci ) p value 1 ( ref ) 139 ( 062312 ) 139 ( 063309 ) 043 042 011 1 ( ref ) 138 ( 073260 ) 168 ( 089316 ) 032 011 tumour mutational burden 080 ( 061105 ) 064 ( 047087 ) 00047 table 2 : multivariate cox analysis for relapse - free survival in each treatment group , including tumour mutational burden ( continuous values ) and stage adjusted for stage ; appendix p 9 ) or continuous tmb and treatment ( p = 025 when adjusted for stage ; appendix p 9 ) , but non - proportionality diminishes the power of this test . despite the absence of association between tmb and relapse - free survival in the dabrafenib plus trametinib group , patients with high tmb still had good overall survival in both treatment groups , based on the premature overall survival data available ( appendix p 58 )  . after quality control and filtering , nanostring data for gene expression profiling were available for 507 ( %0% ) of 870 patients enrolled in the combi - ad trial ( 256 in the placebo group and 251 in the dabrafenib plus trametinib group )  . 
multiple immune signatures have been described ( eg , t - cell - inflamed and ifn ) , 1518 which are all highly correlated and help to identify inflamed ( or so - called hot ) tumours with pre - existing immunity in the tumour tissue . 
estimated hrs with 95% cis based on univariate cox models are shown for ifn classification ( high vs low ) within each treatment group and for treatment ( dabrafenib plus trametinib vs placebo ) within each ifn group . 
the p value for treatment interaction based on this kaplan - meier analysis ( using discrete ifn ) and the corresponding cox model not adjusting for other factors , yields p = 055 ; however , owing to non - proportional hazards between treatment groups , this might not be reliable . 
by contrast with other signatures ( eg , t - cell - inflamed gene expression signature ) , which focus on t cells or combine multiple features of the immune system ( eg , t - cell infiltration , antigen presen tation , and natural killer t - cell inhibitory pathways , such as checkpoints ) , the five - gene signature we selected only includes key genes of the ifn pathway . 
the five ifn - specific genes ( ifng , cxcl9 , cxcl10 , cxcl11 , and gbp1 ) were used to further characterise tumour immune activity , and results were stratified into high ifn gene expression signature ( higher than the median gene expression ) and low ifn gene expression signature ( less than or equal to the median gene expression )  . 
 the baseline ifn signature was strongly prognostic in both groups : patients with a high ifn signature had a statistically significant improvement in relapse - free survival ( figure 3 ) , but not in overall survival with the premature data available ( appendix p 60 )  . because exploratory semiparametric modelling ( appendix pp 23 ) indicated that hazards were nonproportional with respect to treatment group ( data not shown ; also supported by kaplan - meier curves ; figure 3 ) , we fitted cox models for each trial group separately ( table 3 )  . 
we evaluated age and sex in cox models but found no evidence for their value in either group ( appendix p 10 )  . in these cox models , ifn signature expression was significantly associated with relapse - free survival ( after adjustment for clinical variables , with or without tissue source [ data not shown ] ) and outperformed the most important prognostic clinical variable , disease stage ( continuous ifn ; table 3 ) ; similar results were observed in ifn subgroups ( appendix p 10 )  . 
cox analysis indicated no evidence of interaction with treatment ( ifn subgroup and adjusted for stage p = 063 , continuous ifn and adjusted for stage p = 032 ; appendix p 10 )  . we recorded only a modest correlation between baseline tmb and ifn gene expression ( appendix p 57 )  . 
the relapse - free survival in the low tmb and high ifn signature and high tmb and low ifn signature sub groups were in the middle of the two aforementioned extreme tmb and ifn signature subgroups ( figure 4a , d ; appendix p 61 )  . 
 although tmb and ifn contain independent prognostic information , as also confirmed in a multi variate cox model in the placebo group ( appendix p 61 ) , about 40% of patients with a favourable profile based on both markers would be estimated to have relapsed 5 years after randomisation ( high tmb , high ifn signature ; appendix p 61 ) ; therefore , omitting adjuvant therapy for these patients does not seem to be appropriate . vol 21 march 2020 articles in the dabrafenib plus trametinib group , the ifn gene expression signature identified patients with longer relapse - free survival independent of tmb ( appendix p 61 )  . 
as also confirmed in the multivariate cox model ( appendix p 61 ) , tmb had less effect on relapse - free survival in the dabrafenib plus trametinib group , and in this small - subgroup analysis , patients with high tmb had few relapse events in the first 12 months ( appendix p 62 )  . 
however , several relapse events occurred in the high tmb group after 12 months , especially in patients in the low ifn signature subgroup ( appendix p 62 )  . as the tmb and ifn gene expression signature results from the combi - ad placebo group showed , both markers contain independent prognostic information , and these subgroups seem to be similar to the predictive subgroups for response to checkpoint inhibitors in advanced melanoma.7 , 8 , 11 although our analysis was not powered to assess treatment interactions in small biomarker subgroups and the non - proportional - hazards ( based on semiparametric issue has been noted modelling and kaplan - meier plot ; figure 4 ) , the data suggest low tmb have more pronounced long - term relapse - free survival benefit from targeted therapy ( figure 4c , d ) whereas those with high tmb derive a lesser benefit from targeted therapy ( figure 4a , b ) , especially if ifn signature is low ( figure 4a )  . 
a premature overall survival analysis of the various subgroups by treatment is shown in the appendix ( p 63 )  . that patients with in the tcga dataset ( n = 202 ; appendix p 12 ) , the ifn gene expression signature and tmb were independently prognostic ( ifn p < 00001 , tmb p = 00027 ) , and both markers still contained prognostic information when adjusted for stage ( data not shown )  . 
cox proportional hazard analysis also showed that patients in the low tmb and low ifn signature subgroup had significantly ( p = 000097 ) more events than the high tmb and high ifn signature subgroup the brafv600 - mutant melanoma samples of the tcga cohort ( appendix p 64 )  . we found similar biological features in the brafv600mutant melanoma tcga cohort ( appendix p 65 ) as those described in a cohort of various tumours.7 as expected , we observed large numbers of rna sequencing reads for t - cell - based signatures in the high ifn signature subgroup ( appendix p 65 )  . 
an increase in expression of genes in the wnt signalling pathway was found in cold tumourstumours from patients in the low tmb and low ifn gene signature subgroup ( appendix p 65 )  . we also explored additional immune and tumour microenvironment signatures using 1329 published gene sets and pathways ( appendix p 2 ) to understand how the tumour microenvironment differs among patients with low tmb and low ifn gene expression signature . 
specifically , we examined the low tmb and high ifn signature and high tmb and low ifn signature subgroups , because they had the most and least treatment benefit with adjuvant dabrafenib plus trametinib , respectively . 
in the low tmb and high ifn signature subgroup , the highest - ranking gene sets were toll - like receptor ( tlr ) and fas signalling ( appendix p 66 )  . because we expected to observe more adaptive immune gene sets in the high tmb and high ifn subgroup , we systematically investigated single genes and gene sets that are correlated with both high tmb and high ifn signature as well as low tmb and high ifn signature subgroups . 
the top gene sets correlated with both high tmb and high ifn showed a mix of both adaptive and innate immune signatures ( pd - 1 signalling , cxcr3 and interleukin 12 pathways , and cytosolic dna sensing ) , as well as several antigenpresenting gene expression signatures ( class i - mediated antigen presentation and proteasome ; appendix p 67 )  . 
 top gene sets correlated with the low tmb and high ifn signature subgroup also contained signatures from both arms of the immune system ( adaptive and innate immunity ; fas and tlr signalling , cd8 , and cytotoxic t - lymphocyte pathways ) but not the antigenpresenting sets ( appendix p 67 )  . 
repeating this analysis with single genes across the entire transcriptome ( appendix p 68 ) , we observed that only the high tmb and high ifn signature subgroup included antigenpresenting genes ( tap1 and psmb9 ) , t - cell - specific genes ( cd8a / b , grzma / h , and klrd1 ) , and several immune checkpoint genes ( pd - l1 , pd - l2 , lag3 , ido1 , and tigit ; gene expression signatures of interest from the molecular signature database ; 19 appendix pp 1314 )  . 
 summary statistics for all genes and signatures analysed are presented in the appendix ( pp 1548 )  . discussion we do not yet have highly predictive clinical and biological characteristics to identify patients with brafv600 - mutant melanoma who will benefit most from targeted therapy or checkpoint inhibitor therapy in the adjuvant and metastatic settings . 
by contrast , patients with high tmb derived less benefit from dabrafenib plus 368 vol 21 march 2020 articles trametinib treatment , especially if their ifn signature was categorised as low . the baseline mutational landscape in combi - ad was similar to that reported in other analyses of patients with melanoma.20 no association was observed between baseline genetic alterations and clinical outcome or response to therapy . 
this finding is similar to initial findings from patients treated with dabrafenib plus trametinib in the metastatic setting , in which no association was observed between baseline resistance mutations and treatment benefit.21 mapk inhibitorresistant melanoma cells , which might have alterations in several mapk pathway genes , are represented by small and transient tumour subpopulations . 
only after therapy do the subpopulations become enriched and their resistance phenotype stabilised.22 overall , intratumoural heterogeneity ( genomic and transcriptional ) provides a challenge to identifying key pathways that control phenotypic resistance in most tumour cells . 
one potential means of addressing this challenge is through analysis of genomic features and the tumour microenvironment , including infiltrating immune populations and adaptive immune responses , or by using tmb as a broad measure of mutational density and genomic stability . we found a strong prognostic association between ifn signature and relapse - free survival in patients in both the placebo and dabrafenib plus trametinib groups . 
 a comparison of tmb and ifn signature showed that both markers are only moderately correlated and offer independent prognostic information in patients receiving placebo , but not in those receiving dabrafenib plus trametinib . 
similar results have been observed in the tcga dataset , in which mutational load was not correlated with th1 or ifn signature but provided independent prognostic value , 23 and we confirmed these findings by analysing tmb and ifn signature in all available brafv600 - mutant melanoma samples from the tcga cohort . 
the prognostic association between ifn signature and clinical outcome after treatment with dabrafenib and trametinib is in line with previously published results in advanced melanoma , in which immune gene expression signatures were associated with favourable clinical outcome after treatment with mapk inhibitors.18 considering that nearly half of the patients in the high ifn signature subgroup had a relapse event by 5 years in the placebo group and had a very long relapse - free survival after dabrafenib plus trametinib therapy , this prognostic signature allows the identification of patients with a relatively good clinical outcome , but it cannot be used to select patients who do not need adjuvant therapy . despite the absence of association in the dabrafenib plus trametinib group , patients with high tmb still had few overall survival events in both treatment groups , and this improved overall survival might be attributed subsequent lines of therapy after relapse . 
however , postrelapse therapy information was not collected for all patients in the combi - ad trial and post - relapse therapy subgroups in our biomarker populations were too small to allow us to draw any meaningful conclusions . comparison of dabrafenib plus trametinib versus placebo in the tmb subgroups suggests that patients in the high tmb subgroup derive a less pronounced benefit from targeted therapy than patients in the low tmb subgroup . 
analogous findings were reported in head and neck and lung cancers.24 , 25 tmb was found to be inversely associated with the efficacy of egfr tyrosine kinase inhibitor in egfr - mutant lung cancer.24 in the beril - 1 trial , 25 patients with squamous cell carcinoma of the head and neck with low mutational load derived survival benefit with the combination of buparlisib and paclitaxel versus placebo plus paclitaxel . 
overall , our findings and those from other reports suggest that high tmb might have a negative effect on targeted therapy , which could potentially be due to an enhanced number of escape mechanisms derived from genetic heterogeneity . reducing the combi - ad patients with low tmb and low immune gene expression had a poor response to immunotherapy in the setting of early and advanced melanoma in previously treatment published studies , potentially options.7 , 8 , 11 , 12 however , trial , a treatment benefit with dabrafenib plus trametinib was observed in the low tmb and low ifn gene expression signature subgroup , which is an interesting result because this subgroup generally has poor clinical outcomes and would not be expected to derive large benefit from immunotherapy.7 , 8 , 11 , 12 this finding suggests increased potential for this combination as a treatment option for this patient population . in the subgroup with high tmb , we observed differences in response based on ifn gene expression signature . 
at the same time , targeted therapy leads to cell death and increased antigen presentation , and high mutational burden can lead to immunogenic neoantigens that might be recognised by the immune system.26 therefore , high tmb also might lead to an increased likelihood that one of the non - synonymous mutations will ultimately be uniquely immunogenic and drive longterm immuno - editing . tmb alone was significantly associated with relapse - free survival in the placebo group , but high tmb was not significantly associated with improved clinical outcome in patients treated with adjuvant dabrafenib plus trametinib . 
 in this case , the well established immunomodulatory mechanism of dabrafenib plus trametinib might explain why patients do not relapse while receiving treatment but do not have a sustainable immune response.26 second , if the ifn signature is present , there might be an increased likelihood of immune tumour recognition and immune memory , supporting a potentially sustained long - term adaptive immune response . results from combi - ad and the tcga analysis , along with findings for tmb and immune gene expression signature from patients treated with antipd - 1 or anti - ctla - 4 therapy , 8 , 11 might provide insight into the biological basis of differential treatment benefit to targeted therapy versus immune checkpoint inhibitors . in the high tmb and low ifn signature subgroup , which showed less response to dabrafenib and trametinib than the other subgroups , potentially based on escape mechanisms , pyrimidine metabolism and myc pathway expression were among the top - ranking gene sets that were positively correlated with tmb and negatively correlated with ifn . 
altered metabolism has been extensively described as a mechanism of effector t - cell dysfunction , 27 whereas myc signalling has also been described as an immune suppression mechanism.28 , 29 this concept might provide some rationale as to why this subgroup had a lower response to dabrafenib plus trametinib than the other subgroups and , despite the high mutational load , also had a lower response to immunotherapy than tumours with high expression of immune gene signatures.7 , 8 , 11 , 12 additionally , a very low response ( 15% ) was observed for patients treated with anti - ctla - 4 therapy in the high tmb and low immune gene expression signature subgroup in the correlative analysis of the checkmate 067 trial.8 in the low tmb and high ifn signature subgroup , the population with the greatest treatment benefit in combiad , tlr and fas signalling were the highest - ranking gene sets that were highly correlated with ifn and not correlated with tmb . 
tumours , especially hypoxic ones , produce multiple cytokines that induce fas ligand , which could trigger apoptosis in t cells.30 additionally , our tcga analysis showed that tumours with low tmb and high ifn signature have lower expression of several immune checkpoint genes ( pd - l1 , pd - l2 , lag3 , ido1 , and tigit ) compared with the high tmb and high ifn signature subgroup . 
a subgroup analysis from the checkmate 067 trial8 showed that tumours with low tmb and high immune gene expression signature had a good response to anti - ctla - 4 therapy and seemed to derive the most benefit from combining anti - ctla - 4 and anti - pd - 1 therapies ( 79% of patients achieved an objective response )  . 
 our tcga analysis showed a lower activation of genes in the pd - l1pd - 1 axis in the low tmb and high ifn signature subgroup , which might explain the anti - ctla - 4 benefit observed in this subgroup in previous studies . 
 the results from combi - ad and checkmate 067 suggest that combination immunotherapy or a combination of targeted therapy and immunotherapy might be of particular relevance low tmb and high the immune gene expression signature subgroup . overall , the discrepancy in immune activation , checkpoint expression , and differences in the tumour microenvironment , regarding immunosuppressive markers , might have a role in the differential treatment benefit for immunotherapy versus targeted therapies and warrants further evaluation in trials with combination therapy . this study does have some limitations . 
 although we selected a signature that was robust and did not show any differences between skin and lymph node or between stage subgroups , the fact that 60% of the samples were obtained from lymph nodes might mean that immune biomarker data are more difficult to interpret , in view of the fact that the surrounding immune biomarker lymphoid structure can affect results . 
moreover , for each of the datasets for which we did multivariate modelling ( targeted dna sequencing , nanostring data , and their paired dna - rna ) , exploratory semiparametric modelling and visual assessment of the kaplan - meier plots indicated non - proportional hazards between the trial groups . 
 although cox modelling is evidently robust enough to identify a difference between the treatment and placebo groups , the effect on estimates of biomarker and covariate effectsand statistical tests for themmight be perturbed in unpredictable ways . 
we elected to present results separately per treatment group as our primary multivariate analysis to ensure that estimates and inferences are reliable , but this approach does not allow hypothesis tests or cis comparing biomarker effects across treatment groups . 
another potential limitation of this study is that slight imbalances were observed in key clinical variables ( ie , stage ) at baseline and relapse - free survival between the dna sequencing population and intention - to - treat population . 
the study was also not powered for analysis of benefit , and correlations with premature overall survival data in small biomarker subgroups should be considered as exploratory at best ; thus , overall confirmation of the the 370 vol 21 march 2020 articles findings is warranted , and future studies should include pathological features of the tumours and demographic data ( eg , age , sex difference , and constitutional factors ) in relation to the biomarkers of interest to further delineate which patients might benefit . to our knowledge , combi - ad is the first large adjuvant study to systematically analyse the prognostic and predictive effect of tmb and ifn signature . 
results from melanoma trials with immunotherapy in the adjuvant and advanced settings showed that patients with low tmb and low immune gene expression had relatively poor clinical outcomes on immunotherapy compared with all other biomarker subgroups of interest , suggesting that these markers might be of relevance for identifying patients deriving clinical benefit from immunotherapy.7 , 8 , 11 , 12 results from correlative analyses for these markers must be validated in prospective studies for targeted and checkpoint inhibitor therapy . contributors all the authors developed the initial draft of the manuscript and made the decision to submit it for publication ; all the authors contributed to subsequent drafts . 
conception or design of the work , acquisition , analysis , or interpretation of data , and drafting or revision of the work were done by rd , jcb , jg , eg , msq , cr , rk , jmk , ah , and gvl . 
acquisition , analysis , or interpretation of data and drafting or revising of the work were done by cdc , dg , msa , va , mm , vc - s , kf , jl , ds , and gvl . declaration of interests rd reports intermittent , project - focused consulting or advisory relationships with novartis , merck sharp & dohme , bristol - myers squibb , roche , amgen , takeda , pierre fabre , sun pharma , sanofi , catalym , and second genome , outside the submitted work . 
va reports advisory board membership for bristol - myers squibb , merck sharp & dohme , merck serono , novartis , pierre fabre , and roche ; speaker fees from bristol - myers squibb , merck sharp & dohme , merck serono , and novartis ; and travel support from bristol - myers squibb . 
mm reports consulting or advisory role for novartis , bristol - myers squibb , pierre fabre , roche - genentech , and merck sharp & dohme oncology ; honoraria from novartis , bristol - myers squibb , pierre fabre , roche - genentech , and merck sharp & dohme oncology ; and research funding ( to his institution ) from novartis and roche - genentech . 
 vc - s reports reimbursement for attending scientific meetings and advisory boards from novartis , bristol - myers squibb , merck sharp & dohme , pierre fabre , and merck serono . 
kf reports consultancy or advisory role for novartis , genentech , merck , lilly , amgen , sanofi , oncoceutics , bristol - myers squibb , adaptimmune , aeglea biotherapeutics , loxo , roche , asana biosciences , incyte , shattuck labs , tolero pharmaceuticals , array biopharma , fogpharma , neon therapeutics , tvardi , takeda , verastem , boston biomedical , pierre fabre , cell medica , and debiopharm group ; research funding from novartis and sanofi ; stock and other ownership interests in oncoceutics , loxo , shattuck labs , fogpharma , tvardi , clovis oncology , x4 pharma , strata oncology , pic therapeutics , fount therapeutics , apricity health , vivid biosciences , and checkmate pharmaceuticals ; and travel , accommodations , and expenses from pierre fabre and debiopharm group , outside of the submitted work . 
jl reports institutional research support from bristol - myers squibb , merck sharp & dohme , novartis , pfizer , achilles therapeutics , roche , nektar therapeutics , covance , immunocore , pharmacyclics , and aveo ; consultancy for merck shape & dohme , novartis , pfizer , achilles therapeutics , nektar therapeutics , astrazeneca , boston biomedical , bristol - myers squibb , eisai , eusa pharma , glaxosmithkline , ipsen , imugene , incyte , ionctura , kymab , merck serono , pierre fabre , roche - genentech , secarna , and vitaccess ; and support from the national institute for health research biomedical research centre at the royal marsden nhs foundation trust and the institute of cancer research . 
jmk reports grants from prometheus , merck , and immunocore ; and personal fees from merck , array biopharma , bristol - myers squibb , novartis , roche , immunocore , and amgen , outside of the submitted work . 
ah reports consulting or advisory role , travel , accommodations , expenses , and honoraria for amgen , bristol - myers squibb , medimmune , merck serono , merck sharp & dohme , novartis , oncosec , roche , nektar therapeutics , philogen , provectus , and regeneron ; and research funding from amgen , bristol - myers squibb , merck serono , merck sharp & dohme , novartis , roche , celgene , eisai , and glaxosmithkline . 
ds reports consulting or advisory role for roche - genentech , novartis , bristol - myers squibb , merck sharp & dohme , merck serono , amgen , immunocore , incyte , 4sc , pierre fabre , mologen , and sanofi - regeneron ; honoraria from roche - genentech , novartis , merck sharp & dohme , bristol - myers squibb , merck serono , amgen , immunocore , incyte , 4sc , pierre fabre , sysmex , grnenthal group , agenus , array biopharma , astrazeneca , leo pharma , pfizer , philogen , regeneron , and mologen ; travel , accommodations , and expenses from roche - genentech , novartis , bristol - myers squibb , merck serono , amgen , and merck ; speakers bureau for novartis , bristol - myers squibb , merck sharp & dohme , amgen , incyte , pierre fabre , and roche ; and research funding from novartis and bristol - myers squibb , outside of the submitted work . 
 gvl reports being consultant advisor for aduro , amgen , array , bristol - myers squibb , merck sharp & dohme , novartis , pierre fabre , oncosec , and roche , outside of the submitted work . 
msa declares no competing interests . data sharing novartis is committed to sharing with qualified external researchers , access to patient - level data , and supporting clinical documents from eligible studies . 
this trial data availability is according to the criteria and process described on clinicalstudydatarequest.com. acknowledgments the study in this analysis was sponsored by glaxosmithkline ; dabrafenib and trametinib are assets of novartis ag as of march 2 , 2015 . 
we thank the study site staff and additional investigators , xiaohong li , christian laing , reinhold pollner , and nathan riccitelli ( navigate biopharma services , inc ) , and mahtab marker , eric hajjar , noelle hanoteau , alexander savchenko , gll gorgun , agus darwanto , aislyn boran , rebecca leary , nathan houde , and others , for their contributions . 
medical writing assistance was provided by michael demars ( articulatescience llc ) , and was funded by novartis pharmaceuticals corporation . antihypertensive treatment and risk of cancer : an individual participant data meta - analysis emma copland , dexter canoy , milad nazarzadeh , zeinab bidel , rema ramakrishnan , mark woodward , john chalmers , koon k teo , carl j pepine , barry r davis , sverre kjeldsen , johan sundstrm , kazem rahimi , on behalf of the blood pressure lowering treatment trialists collaboration * summary background some studies have suggested a link between antihypertensive medication and cancer , but the evidence is so far inconclusive . 
thus , we aimed to investigate this association in a large individual patient data meta - analysis of randomised clinical trials . methods we searched pubmed , medline , the cochrane central register of controlled trials , and clinicaltrials.gov from jan 1 , 1966 , to sept 1 , 2019 , to identify potentially eligible randomised controlled trials . 
we pooled individual participant - level data from eligible trials and assessed the effects of angiotensin - converting enzyme inhibitors ( aceis ) , angiotensin ii receptor blockers ( arbs ) , blockers , calcium channel blockers , and thiazide diuretics on cancer risk in one - stage individual participant data and network meta - analyses . 
in the individual participant data meta - analysis comparing each drug class with all other comparators , no associations were identified between any antihypertensive drug class and risk of any cancer ( hr 099 [ 95% ci 095104 ] for aceis ; 096 [ 092101 ] for arbs ; 098 [ 089107 ] for blockers ; 101 [ 095107 ] for thiazides ) , with the exception of calcium channel blockers ( 106 [ 101111 ] )  . 
 in the network meta - analysis comparing drug classes against placebo , we found no excess cancer risk with any drug class ( hr 100 [ 95% ci 093109 ] for aceis ; 099 [ 092106 ] for arbs ; 099 [ 089111 ] for blockers ; 104 [ 096113 ] for calcium channel blockers ; 100 [ 090110 ] for thiazides )  . interpretation we found no consistent evidence that antihypertensive medication use had any effect on cancer risk . 
 although such findings are reassuring , evidence for some comparisons was insufficient to entirely rule out excess risk , in particular for calcium channel blockers . funding british heart foundation , national institute for health research , oxford martin school . copyright 2021 the author ( s )  . 
one study has suggested that using arbs increases the risk of cancer , 4 whereas two subsequent meta - analyses showed no such association.11 , 12 another meta - analysis of randomised controlled trials found no evidence linking any drug class with the incidence of any cancer , 12 but an increased risk of cancer with the use of angiotensin - converting enzyme inhibitors ( aceis ) in combination with arbs could not be ruled out . 
of the trials and meta - analyses that reported cancer outcomes , no consistent associations were identified between any antihypertensive drug class and cancer risk . added value of this study in this meta - analysis of individual patient - level data from 33 randomised controlled trials , to our knowledge , the one with the largest sample size to date , we found no compelling evidence that the use of any antihypertensive drug class had a significant effect on the risk of cancer when compared with placebo . 
furthermore , we found no consistent evidence that the use of any antihypertensive drug class had a material effect on the risk of developing breast , colon , lung , prostate , or skin cancer . 
 the effect also did not vary across groups stratified by age , sex , body - mass index , smoking status , or previous antihypertensive use at baseline . implications of all the available evidence our study addresses a gap in the evidence for the safety of antihypertensive medication . 
 however , evidence for some cancer types was insufficient to entirely rule out the possibility of some excess risk , in particular , after a duration of treatment longer than that considered in our study . findings from existing meta - analyses based on summary statistics are limited by the study design , because such methods could not account for competing risks . 
 additionally , these analyses could not assess the timing of cancer events , since events occurring shortly after treatment initiation are unlikely to be causally linked to treatment since it is biologically plausible that a latency period exists between exposure to the medication and cancer occurrence . 
 the blood pressure lowering treatment trialists collaboration ( bplttc ) is a collaboration of the principal investigators of major global clinical trials of pharmacological blood pressure lowering treatment , coordinated by the university of oxford ( oxford , uk )  . 
using the bplttc database , we aimed to investigate class - specific effects of antihypertensive drugs on the outcomes of cancer , cancer deaths , and site - specific cancers . methods study governance and data source for this meta - analysis of individual participant - level data , we used the bplttc database , 13 , 14 which currently has access to individual participant data from randomised controlled trials identified as described in the search strategy and selection criteria section and the study protocol.13 , 14 the study protocol was approved by the steering committee and collaborators before the data was released for analysis and is available in the appendix ( pp 2939 )  . 
ethical approval for the current study was obtained from the oxford tropical research ethics committee ( oxtrec reference 54514 )  . lowering the mesh search strategy and selection criteria the search strategy and primary criteria for inclusion in the bplttc have been published previously14 and are reported in the appendix ( pp 24 )  . 
briefly , we searched pubmed , medline , the cochrane central register of controlled trials , and clinicaltrials.gov for randomised controlled trials investigating pharma cological blood treatments published between pressure jan 1 , 1966 , and sept 1 , 2019 . 
 we also required that trials had at least 1000 participant years of follow - up in each treatment group and reported individual partici pant data on cancer events and timing of diagnosis during follow - up . 
we excluded trials that did not provide cancer event information . including possible variations terms data extraction two investigators ( dc , mn ) independently screened titles and abstracts for eligibility and any conflicts were vol 22 april 2021 articles resolved through discussion with a third investigator ( kr )  . 
analyses were confined to studies that compared one main drug class with a control group ( or groups ) and studies that compared more versus less intensive treatment regimens without a specific drug class group were excluded . 
we used the revised cochrane risk - of - bias tool15 to assess the risk of bias of individual trials . we extracted individual participant data for baseline characteristics ( appendix pp 1112 ) and follow - up blood pressure measurements , cancer events , and cancer deaths . outcomes the primary outcome was any cancer event , defined as the first occurrence of any cancer diagnosed after randomisation . 
the site - specific cancers analysed included common cancers and subtypes that have previously been reported to be associated with blood pressure lowering treatment , comprising of breast , colorectal , lung , prostate , and skin cancers.510 , 16 we describe the source of these outcomes for each trial , and whether or not these outcomes have been adjudicated by an endpoint committee on the basis of certain criteria , in the appendix ( pp 1317 )  . data analysis characteristics of the participants included in each drug class comparison at baseline were described using summary statistics . 
all analyses were time - to - event analyses done using cox proportional hazards models , stratified by trial , and were based on the intention - to - treat principle . 
in the absence of exact dates , the date of cancer diagnosis was approximated using the closest date to diagnosis on the basis of the date the cancer was first reported in the study or the date of death in participants for whom cancer had not been diagnosed or recorded before death with the underlying cause reported as cancer . 
we used cause - specific fixed - effects cox regression models for cancer events , with additional censoring for non - cancer deaths , to account for the competing risks . 
we also did a network meta - analysis to investigate the class - specific effects of antihypertensives compared with a placebo reference group.2023 in this prespecified analysis , the effects of drug classes were analysed simultaneously by combining all available direct and indirect evidence across the network of studies.2023 placebo - controlled trials contributed directly to the hazard ratio ( hr ) estimates of each antihypertensive drug class on cancer risk , and all other trials contributed indirectly . 
network metaanalyses were not done for site - specific outcomes due to small numbers of events from placebo - controlled trials . to assess any temporal variation in risk , we did a posthoc analysis to estimate the hr for each drug class according to specific timepoints during follow - up , and tested for heterogeneity and linear trend in risk across the follow - up duration . 
for cancer and cancer death outcomes , we prespecified subgroup analyses of the stratified effects of anti hypertensive drug classes by baseline age , sex , smoking status , and body - mass index ( bmi )  . 
we also stratified analyses based on previous use of anti hypertensive medication at baseline , to test the hypothesis that true harmful effects are masked by widespread use of non - randomised treatment before trial participation . 
for the 560 vol 22 april 2021 articles analyses stratified by follow - up period and patient characteristics , and analyses investigating site - specific cancer outcomes , we have presented unadjusted p values for heterogeneity and adjusted p values for multiple comparisons calculated using the bonferroni method . 
 we did the following sensitivity analyses : competing risk analysis using fine and gray subdistribution models to determine whether bias was introduced into the analysis due to competing risks ; two - stage meta - analysis combining estimates from individual trials using the fixedeffect inverse - variance weighting approach to ensure that the hrs from the two - stage approach were comparable with the one - stage approach ; and a comparison of the effects of each antihypertensive drug class on any cancer between trials that explicitly excluded cancer patients at baseline , and therefore only reported incident events , and those that did not exclude cancer patients at baseline and consequently might have reported recurrent events ( appendix p 3 )  . those from we reported hrs with corresponding 95% cis for all analyses , calculated from time - to - event models , and p values for all analyses of less than 005 were considered to indicate significance . 
this study is registered with prospero ( crd42018099283 )  . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . results the systematic review identified 11 494 studies , from which 100 trials were considered potentially eligible for the bplttc studies . 
of the 33 trials included in the analysis , 16 ( 48% ) trials that contributed to 11 833 ( 79% ) of 15 012 cancer events had previously reported on cancer risk or had been included in aggre gate meta - analyses of randomised controlled trials.4 , 11 , 12 3251 ( 21% ) cancer events from 12 trials included were published for the first time in this study . 
 the risk of bias assessment indicated that 29 trials were at low risk of bias , and four trials had some risk of bias ( appendix p 20 )  . 15 trials ( 118 574 participants ) included an acei drug class comparison ; 11 trials ( 99 711 participants ) included arbs ; five trials ( 35 169 participants ) included blockers ; 19 trials ( 150 745 participants ) included calcium channel blockers ; and six trials ( 58 185 participants ) included thiazides ( table )  . 
for the network metaanalysis comparing drug classes against placebo , individual participant data for total cancer events was available for 72 812 participants from 13 placebocontrolled trials : seven included an acei treatment group , three included an arb group , four included a calcium channel blocker group , and one included a thiazide diuretic group . 
individual participant data for cancer death was available for 51 038 participants included in eight placebo - controlled trials : three included aceis , three included arbs , and two included calcium channel blockers . 
 eight trials included more than two treatment groups : six trials included three intervention groups and two trials included four treatment groups ( appendix pp 1319 )  . the median age of participants across all trials was 66 years ( iqr 6072 )  . 
details of participant characteristics for individual trials are included in the appendix ( p 21 )  . after a median of 42 years ( iqr 3050 ) of follow - up , 15 012 participants were diagnosed with cancer across all 33 trials . 
we found no evidence of an association between antihypertensive drugs and any cancer when assessing all comparison groups ( hazard ratio [ hr ] 099 [ 95% ci [ 092101 ] for arbs ; 095104 ] for aceis ; 096 098 [ 089107 ] for blockers ; 101 [ 095107 ] for thiazides ) , with the exception of calcium channel blockers ( 106 [ 101111 ] ; figure 1a )  . 
since no data were available on cancer death outcomes for any placebo - controlled trials with a thiazide diuretic drug class comparison , the network estimate was based entirely on indirect evidence from trials that included a thiazide diuretic group ( two trials ) or a placebo group , but not both . in a post - hoc analysis , we also found no pattern of increasing or decreasing risk for any cancer or cancer death over time associated with any antihypertensive drug class ( figure 2 )  . 
although there was some evidence of heterogeneity in treatment effect across different time periods for any cancer with aceis ( pheterogeneity = 0004 ) , calcium channel blockers ( pheterogeneity = < 00001 ) , and thiazides ( pheterogeneity = < 00001 ) , and for cancer death with calcium channel blockers ( pheterogeneity = 006 ) and thiazides ( pheterogeneity = < 0001 ) , there was no indication that the risk increased consistently over time ( figure 2 )  . 
in prespecified subgroup analyses , we found no evidence for variation in treatment effects across different age groups , sex , bmi categories , smoking status , or previous use of antihypertensive drugs ( all pheterogeneity > 010 ; appendix pp 68 )  . 
we found no evidence for inconsistency in treatment effects across the network for any cancer or cancer death outcomes ( p = 060 for any cancer ; p = 088 for cancer death )  . we examined the effects of antihypertensive drug classes on risks of breast , colorectal , lung , prostate , and skin cancer compared with all other comparators ( figure 3 )  . 
across all drug classes and site - specific cancers , we found no evidence of any associations , with the exception of calcium channel blockers which were associated with increased risk of prostate and skin cancers . 
the excess risks for calcium channel blockers on prostate and skin cancers were driven by the comparison of calcium channel blockers compared with arbs ( data not shown )  . 
we also examined these effects according to duration of follow - up and found no consistent temporal pattern in the risks for all drug classes ( all p = 100 ; data not shown )  . the two - stage meta - analysis , the hrs were comparable in magnitude with the results of the one - stage meta - analysis ( appendix p 9 )  . 
we also found that the subdistribution hrs from the fine and gray models were comparable to the cause - specific hrs , thus there was no sign of bias due to competing risks ( data not shown )  . 
in the sensitivity analysis comparing the effects of anti hypertensive drug classes on any cancer between trials that explicitly excluded cancer patients at baseline and those that did not , no significant heterogeneity in treatment effects was identified for any drug class compared with all other comparators ( pheterogeneity = 099 for aceis ; pheterogeneity = 078 for arbs ; pheterogeneity = 055 for blockers ; pheterogeneity = 040 for calcium channel blockers ; pheterogeneity = 017 for thiazides ; appendix p 23 )  . favours lower cancer risk with drug class favours higher cancer risk with drug class figure 2 : effects of antihypertensive drug classes on risk of any cancer ( a ) and cancer death ( b ) , stratified by follow - up duration p values are for linear trend and heterogeneity adjusted for multiple testing . 
arb = angiotensin ii receptor blockers . cancer deaths , with the exception of thiazide diuretics , which were associated with an increased risk of death caused by cancer ( figure 1b )  . 
arb = angiotensin ii receptor blockers . discussion in this study , we found no consistent evidence that the use of antihypertensive medication overall increased the risk of any cancer or cancer death . 
we also found no strong evidence that the use of any particular antihypertensive drug class had a consistent effect on the risk of developing breast , colon , lung , prostate , or skin cancer . 
these findings were further corroborated in the vol 22 april 2021 articles network meta - analyses based on the direct and indirect comparisons of drug classes with placebo , and in the time - stratified analyses , which showed no evidence of increasing or decreasing effects over time . 
however , the excess risks identified for calcium channel blockers on any cancer , prostate cancer , and skin cancer and for thiazide diuretics on cancer death in some analyses requires further investigation in clinical trials with a larger number of events , particularly for placebocontrolled comparisons . although several observational studies have previously reported an association between cancer risk and increased blood pressure or its treatment , 5 , 6 , 7 , 16 , 75 , 76 evidence based on randomised data is scarce , and meta - analyses of randomised evidence are mainly based on analysis of published summary statistics.4 , 11 , 12 such study designs cannot account for competing risks , or investigate cancer events across different durations of follow - up . 
little evidence is available from meta - analyses of published findings from randomised controlled trials on the effects on site - specific cancers because it is unlikely that a single trial would have sufficient statistical power to report these effects . 
due to the large number of trials included in the bplttc database with individual participant data available , our study also addresses the paucity of evidence on antihypertensive drug use and cancer risk among important patient subgroups , and found no significant variation in the effects on any cancer across groups defined by age , sex , bmi , smoking status , or previous antihypertensive use with any antihypertensive drug class , indicating that any cancer - related adverse effects were unlikely to have been masked by widespread use of non - randomised treatment before trial participation . several hypotheses have been posited linking the pathways of specific drug classes to cancer , independently of changes in blood pressure.9 , 10 there has been a concern around thiazide the potential association between diuretics and skin cancer risk due to the photosensitising properties of thiazides and harmful effects identified in several observational studies ; 7 however , our findings do not support an association between the use of thiazides and skin cancers . 
other studies have also suggested that blockade of the reninangiotensin system by aceis and arbs might have a protective effect against a broad range of cancer types , 77 including lung , breast , and prostate cancers , 78 by affecting cell proliferation , angiogenesis , and apoptosis.79 however , we found no significant associations between any of these drug classes and risk of any cancers . 
 our findings suggesting a potential increased risk of any , prostate , or skin cancers with use of calcium channel blockers and cancer death with thiazides were unexpected considering that no compelling evidence exists with regard to plausible mechanisms that would affect carcinogenesis in these parts of the body with use of these drugs.75 , 80 however , our detailed analyses and the absence of plausible mechanisms suggest that calcium channel blockers or thiazides are unlikely to cause such cancers . 
 comparison of a single drug class against all other groups is limited by uncertainty regarding whether the apparent excess risk is a true effect of the intervention or a reflection of a potentially beneficial effect of the drug class in the comparison group ( which by chance will differ for different classes )  . 
in the case of thiazide diuretics , a larger number of trials providing cancer death data is required to investigate this association further , since only two trials contributed data to this analysis . 
in the case of calcium channel blockers , the excess risks identified were primarily driven by the comparison of calcium channel blockers against arbs , which in turn seems to have been driven by data from a single trial ( value73 , 74 )  . 
although no significant heterogeneity was identified across trials with a calcium channel blocker comparison in two - stage meta - analysis , the value trial ( calcium channel blocker vs arb comparison ) , was an important driver of the excess risk for calcium channel blockers compared with all other comparators in the main analysis . 
because of the relatively small number of placebo - controlled trials available for most drug classes , we did individual participant data network meta - analyses to estimate these effects . 
this finding , together with the time - stratified analyses results , and the absence of heterogeneity in treatment effects across drug classes provide evidence against any class - specific effects on the risk of developing cancer . 
 however , these detailed and robust analyses have inadequate power to detect a statistical difference , particularly for site - specific cancers . a key strength of this study was the use of individual participant data from the largest dataset of randomised controlled trials of antihypertensive drug treatments available to date , to our knowledge . 
previously , a large meta - analysis of randomised controlled trials investigated the risk of cancer associated with antihypertensive treatment , but it was based on aggregate data12 and one study that analysed individual participant - level data only included 28 787 participants with 1823 cancer events.4 the number of participants included in our metaanalysis was nearly ten times higher and the number of cancer events was more than 13 000 higher than that the previous meta - analysis based on included individual participant - level data , enabling a more detailed analysis to be done than previously possible . 
another important strength of this study was that we had access to unpublished cancer event data collected during follow - up , and additional information from most trials on cancer subtypes , date of diagnosis , and information on multiple diagnoses in individual partici pants . 
since we had access to time - to - event data , we were able to assess any trend in cancer risk over time , an analysis that has not been possible previously using randomised data . 
 566 vol 22 april 2021 articles this analysis allowed us to account for the latency period between exposure to the antihypertensive drug and occurrence of cancer , since events diagnosed early during follow - up are less likely to be linked to the study medication . 
thus , our study provides the most compelling evidence to date for the safety of antihypertensive drugs with respect to cancer and cancer subtypes that we have considered . a limitation of this study was that we did not have access to individual participant data for all trials that were eligible for inclusion in the bplttc database . 
therefore , although we had access to a larger number of cancer events from randomly assigned participants than did previous studies , some analyses involving cancer mortality or site - specific cancer outcomes were based on relatively small numbers of events , resulting in greater uncertainty around the risk estimates . 
however , previous evidence81 , 82 has suggested that adjudication of common outcomes does not have an impact on relative treatment effects because any misclassification is expected to be consistent across treatment groups . 
 however , our sensitivity analysis , stratified by explicit exclusion of cancer patients at baseline , suggested that there were no differences in the relative treatment effects in trials that excluded cancer patients compared with those that did not . 
investigators across many trials were also allowed to prescribe additional non - study anti hypertensive treatments to participants whose blood pressure had not been controlled sufficiently with the study drug . 
in cases where the treatment and control groups were systemically prescribed different classes of drugs ( either by design or chance ) , this could lead to the underestimation of each drug class effect on the outcomes . 
hence , it would be prudent for future trials to continue collecting outcomes , including cancer , long after the trial has ended to allow the investigation of off - target effects of antihypertensive drugs . 
 in our analyses stratified by follow - up duration , we found no evidence of an increasing risk with more years of exposure to the treatment ; however , studies with longer durations might be necessary to rule out any association with long - term antihypertensive use . our study has addressed an ongoing controversy about the safety of blood pressure lowering medication with respect to cancer risk , using the largest sample of individual - level randomised evidence on blood pressure lowering treatment to date , to our knowledge . 
in our detailed analyses , we found no evidence that the use of antihypertensive medication has any substantial effect on cancer risk , although we could not rule out potential class - specific effects for calcium channel blockers and thiazide diuretics . 
it is estimated that between 30% and 50% of individuals have poor adherence to these drugs , partly because of concerns around the harmful effects that long - term use of antihypertensive medications might cause.2 , 3 the main implication of our study is that patients using antihypertensive medication should continue to take their medications because concerns about increased cancer risk seem to be unfounded . contributors kr and dc acquired the funding for the study . 
the corresponding author had the final responsibility to submit for publication . declaration of interests mw reports personal fees from amgen , kyowa kirin , and freeline , outside the submitted work . 
js reports ownership in companies providing services to itrim , amgen , janssen , novo nordisk , eli lilly , boehringer , bayer , pfizer , and astrazeneca outside the submitted work . 
kr reports grants from the british heart foundation , uk research and innovation global challenges research fund , oxford martin school , and national institute for health research oxford biomedical research centre , during the conduct of the study ; and personal fees from bmj heart and plos medicine , outside the submitted work . 
ec , zb , rr , kkt , cjp , and brd declare no competing interests . data sharing the bplttc is governed by the university of oxfords policies on research integrity and codes of practice and follows the universitys policy on the management of research data and records . 
requests for data should be made directly to the data custodians of individual trials . acknowledgments this study was funded by the british heart foundation ( pg / 18 / 65 / 33872 and fs / 19 / 36 / 34346 ) , the national institute for health research ( nihr ) oxford biomedical research centre , and the oxford martin school . 
 the views expressed in this article are those of the authors and not necessarily those of the national health service , nihr , or the uk department of health and social care . 
this manuscript was prepared using accord , allhat , peace , and shep research materials vol 22 april 2021 articles obtained from the national heart , lung and blood institute biologic specimen and data repository information coordinating centre and does not necessarily reflect the opinions or views of accord , allhat , peace and shep , or the nhlbi . 
this manuscript was not prepared in collaboration with investigators of the aask trial and does not necessarily reflect the opinions or views of aask , the niddk central repositories , or the niddk . 
 n a d o f a r a g e n e k u l k a r n i firadenovec : a new gold standard for bcg - unresponsive bladder cancer ? lancet oncol 2021 ; 22 : 89in this comment , the declaration of interests statement was incorrect and should have read as follows : i report personal fees from merck , ferring , biosyent , tersera , abbvie , roche , theralase , and janssen , outside the submitted work . 
 this correction has been made to the online version as of dec 30 , 2020 , and the printed version is correct . maringe c , spicer j , morris m , et al . 
 the impact of the covid - 19 pandemic on cancer deaths due to delays in diagnosis in england , uk : a national , population - based , modelling study . 
lancet oncol 2020 ; 21 : 154950in this comment , on the second and eleventh lines of paragraph two , the drug name has been corrected to gx - 188e . 
durvalumab alone and durvalumab plus tremelimumab versus chemotherapy in previously untreated locally patients with unresectable , advanced or metastatic urothelial carcinoma ( danube ) : a randomised , open - label , multicentre , phase 3 trial . 
 lancet oncol 2020 ; 21 : 157488 in this article , the affiliation for ignacio duran should have been hospital universitario virgen del roco , seville , spathis correction has been made to the online version as of dec 30 , 2020 . correction to lancet oncol 2020 ; 21 : 160210 pm , welt ens poortmans fortpied c , et al . 
internal mammary and medial supraclavicular lymph node chain irradiation in stage iiii breast cancer ( eortc 22922 / 10925 ) : 15 - year results of a randomised , phase 3 trial . 
 lancet oncol 2020 ; 21 : 160210 in this article , the funders of the study should have been ligue nationale contre le cancer and kwf kankerbestrijding in the funding and acknowledgments sections . 
org / health - professional / cancer - statistics / incidence#heading - four ( accessed oct 14 , 2020 )  . covid - 19 in patients with cancer lennard lee and colleagues 1 investi gated the associations of different tumour types and patient demographics with covid - 19 prevalence in patients with cancer in the uk as part of the uk coronavirus cancer monitoring project ( ukccmp )  . 
we would like to bring to the readers attention several methodological concerns that might undermine the validity of the findings . first , the study does not include some details about the cancer , such as whether incident or recurrent cancers were included and how cancer type was defined for individuals with multiple cancers . 
 furthermore , because the ukccmp enrols patients with cancer and covid - 19 without tracking covid - 19 incidence , an analysis of covid - 19 prevalence would be more appropriate than an analysis of covid - 19 risk . second , the proportions of the breast and prostate cancer for both the ukccmp and office for national statistics ( ons ) cohorts were underestimated because calculations did not use only individuals at risk ( women for breast cancer and men for prostate cancer ) as a denominator . 
although a very small number of men could have been diagnosed with breast cancer , it would be more appropriate to focus on breast cancer in women , which would have then show similar proportions in the ukccmp ( 143 [ 321% ] of 445 ) and the ons data ( 46 109 [ 335% ] of 137 844 )  . 
thus , analyses of covid - 19 prevalence stratified by sex would be more appropriate for breast and prostate tumours , as well as tumours of the female and male reproductive systems . third , the authors mentioned that the management of patients with cancer and covid - 19 was directed by the patients clinician tea although covid - 19 has promptly and drastically changed how medicine is practised , cancer care still could differ across hospitals and regions . 
most importantly , the risk of morbidity and mortality from covid - 19 is not uniform across the uk population , 2 with a substantially lower covid - 19 mortality rate in wales than in england . 
additionally , there is vast geographical variation in cancer type incidence.3 therefore , if the ukccmp has these data , the authors should have investigated the associations of different tumour types with covid - 19 prevalence by region . fourth , some other factors that might influence the outcomes of covid - 19 such as its severity and covid - 19 - specific treatment as well as cancer immunotherapy and timing of immunotherapy should be accounted for in the future studies . we declare no competing interests . * carmen smotherman , daniel norez , rebecca austin - datta , lusine yaghjyan carmen.smotherman@jax.ufl.edu department of epidemiology , college of public health and health professions and college of medicine , university of florida , gainesville , fl , usa ( cs , ra - d , ly ) ; center for data solutions , college of medicine , university of florida , jacksonville , fl 32206 , usa ( cs , dn ) lee lyw , cazier j - b , starkey t , et al . 
 andcommunity / birthsdeathsandmarriages / deaths / bulletins / deathsinvolvingcovid19 englandandwales / deathsoccurringinmarch202 0#characteristics - of - those - dying - fromcovid - 19 ( accessed oct 14 , 2020 )  . vol 21 december 2020 e539 correspondence 4 weeks before symptom onset , 9 ( 29% ) of 31 patients received other anticancer treatments , including targeted therapy or chest radiotherapy concurrently , which also might affect the odds of death . 
we suggest that the data might be further analysed to evaluate the association of chemotherapy with death after excluding these patients who had received additional treatments . third , advanced cancer stage has been identified as a risk factor of death for patients with cancer , 4 and increased odds of death ( or 338 ; 95% ci 133859 ; p = 0011 ) in patients with solid tumours and covid - 19 in univariable logistic regression analysis of this study . 
it would be interesting to know whether or not receiving chemotherapy within 4 weeks before symptom onset is related to death in patients with solid tumours and covid - 19 after adjusting for cancer stage . 
 we declare no competing interests . guosen zhang , yang an , lu zhang , longxiang xie , * xiangqian guo xqguo@henu.edu.cn department of predictive medicine , school of basic medical sciences , institute of biomedical informatics , bioinformatics center , henan provincial engineering center for tumor molecular medicine , henan university , kaifeng 475004 , china yang k , sheng y , huang c , et al . 
 risk factors for in - hospital mortality in patients with cancer and covid - 19 we read with great interest the excellent research by kunyu yang and colleagues1 in the lancet oncology . 
 the results indicated that receiving chemotherapy within 4 weeks before symptom onset was associated with increased odds of death ( odds ratio [ or ] 351 , 95% ci 1161059 ; p = 0026 ) in patients with cancer and covid - 19 , adjusted for sex , cancer type , and time since cancer diagnosis . 
 although we applaud the authors efforts , we have some questions for the authors and would appreciate some additional information about the research . first , older age ( 60 years ) has been proved as a significant independent predictor of mortality in both patients with cancer and patients with covid - 19.2 , 3 however , the authors excluded this risk factor because of no significant difference in age between the survival group and non - survival group , explaining that their study was comprised of an older population ( median age 63 years )  . 
we cannot completely accept this elucidation because we found that patients aged younger than 60 years accounted for 86 ( 42% ) of the 205 patients in this study , and they did not belong to the older age group . 
we think that the explanation might be that patients with haematological malignancies were younger ( median age 55 years vs 63 years ) but accounted for a higher proportion of mortality ( 41% vs 20% ) compared with the overall patient cohort . 
 therefore , age could be an important factor affecting the risk of mortality in this study , and the results should be presented after adjusting for age . second , in the group of patients receiving chemotherapy within vol 21 september 2020 e407 correspondence facilities are scarce , prioritisation should involve the patients managed with curative - intent therapeutic strategies , and those with a life expectancy of 5 years or more , acknowledging that final decisions lie with the referring clinicians . 
patients with cancer should be closely monitored owing to their susceptibility to sars - cov - 2 infection . ar reports grants , personal fees , and non - financial support from pfizer , merck , personal fees and non - financial support from merck , sharpe & dohme , astrazeneca , roche , ipsen , and novartis . 
cochrane database syst rev 2018 ; 2 : cd008983 . preparedness for covid - 19 in the oncology community in africa the world is experiencing an unprecedented health crisis with the coronavirus disease 2019 ( covid - 19 ) pandemic threatening human existence and livelihood . 
patients with cancer are thought to be more susceptible and have higher morbidity and mortality rates from covid - 19 than the general population.1 africa , with a heterogeneity of economies , cultures , and disease patterns , is thank fully the last continent to be hit by the pandemic . 
we acknowledge the points made by our colleagues from morocco.2 with many lessons learnt from other countries and the experiences within africa from the ebola and cholera epidemics , africa should be prepared for covid - 19 . 
unfortunately , poverty , low health literacy rates , and cultural practices that negatively affect cancer outcomes will result in poor assimilation of covid - 19 containment strategies in africa . the continent , despite many competing health challenges , is now finally implementing cancer prevention strategies , improving treatment access , and expanding the cancer workforce . 
weas oncologists in africafollow covid - 19 cancer care guidelines from other highincome countries.3 , 4 we realise the urgency to delay the start of adjuvant therapies and regular surveillance , reconsider switching to oral systemic therapies ( many of which are inaccessible to our patients ) , and rethink the effectiveness of further lines of palliative chemotherapy . 
we must weigh the consequences of exposing our susceptible patients and small cancer ignoring oncology workforce to covid - 19 while principles that we previously did not dare to disregard.5 we need to make critical decisions because many patients with cancer present with locally advanced disease in africa , and delaying treatment will result in progression and deterioration of their cancer as well as higher out - of - pocket expenditure for treatments , leading to further psychological distress . what do we do when a patient with cancer on chemotherapy develops a fever ? would we ignore the possibility of neutropenic fever , malaria , or typhoid ? should we call the overstretched and under - resourced covid - 19 team ? the paucity of protective gear and onsite testing kits for patients and health - care staff on the continent is a major flaw in delivering life - saving oncology care during this crisis . 
the availability of logistics ( which are greatly inadequate ) , institutional published online april 3 , 2020 s1470 - 2045 ( 20 ) 30220 - 5 vol 21 may 2020 comment guidelines , and the country - specific covid - 19 case burden will dictate our actions , most likely negatively . in west africa , covid - 19 protocols are defined by individual institutions . 
patients with a fever are referred to the emergency roo a minimum number of essential staff ( in protective gear when available ) will be rotated , prescriptions refilled remotely , and second - line and third - line palliative chemotherapy halted . 
of particular concern is the large population infected by hiv , which includes approximately 8 million people.6 while public hospitals prepare for the first wave of covid - 19 patients , oncology services at this point are still aiming to deliver full service when follow - up outpatient services possible , although have been severely curtailed . 
staff will be divided into teams consisting of core personnel . in sudan , despite the low covid - 19 burden , cancer centres have established a contingency plan by deferring new referrals except for emergency surgery , non - urgent intravenous cases . 
 medical teams and core support staff work as divided teams after having attended mandatory covid - 19 training sessions . oncologists in africa , in the absence of centralised and resource - appropriate covid - 19 guidelines , are pragmatically safeguarding patients and the workforce while providing essential cancer care . 
korle bu teaching hospital , accra gqqf + 6r , ghana ( vv ) ; the national cancer institute , university of gezira , wad madani , sudan ( mmae ) ; and stellenbosch university , stellenbosch , south africa ( hs ) yu j , ouyang w , chua mlk , xie c . 
countries / southafrica ( accessed march 29 , 2020 )  . the uk coronavirus cancer monitoring project : protecting patients with cancer in the era of covid - 19 published online april 15 , 2020 s1470 - 2045 ( 20 ) 30230 - 8 the uk coronavirus cancer monitoring project ( ukccmp ) aims to collect , analyse , and disseminate in real time data from the uk cancer centres about severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection rates in patients with cancer , and their outcomes in terms of coronavirus disease 2019 ( covid - 19 )  . 
this approach will enable oncologists to gain crucial insights to inform decision making . 622 vol 21 may 2020 comment covid - 19 and cancer : 1 year on it has been a year since the uk entered its first covid - 19 lockdown on march 23 , 2020 , with unprecedented consequences . 
although the pandemic is far from over , what have its impacts been on cancer care in the uk and globally , and what does the future hold ? have subsequently progressed and become harder to treat . 
moreover , lockdown - associated lifestyle habits eg , unhealthy diets and reduced physical activitycould cause a further increase in the prevalence of obesityrelated cancers in the years ahead . covid - 19 has had devastating effects on patients with cancer , with huge numbers of missed diagnoses and delayed treatments due to health systems under pressure and patient reluctance to seek medical care . 
 despite repeated reassurances from officials that the uks national health service ( nhs ) remained open for urgent care , a study estimated that 45% of those with potential cancer symptoms did not contact their doctor during the uks first wave of the pandemic ( marchaugust , 2020 ) , citing reasons including fear of contracting covid - 19 and avoiding placing extra strain on the nhs . 
combined with interruptions in cancer screening programmes and delays in scans and diagnostics , a spike in late cancer presentations and diagnoses is antici pated , making some previously curable tumours more difficult to treat and , unfortunately , further excess deaths unavoidable . 
this problem prevails internationally , even in countries praised for their management of covid - 19 ; a study estimated that in the state of victoria , australia , around 2500 cancer diagnoses were missed during the first 6 months of the pandemic . in the uk the pandemic has also caused major delays in cancer treatments . 
around 40 000 fewer people than normal started cancer treatment last year , and us hospitals have been deluged by covid - 19 cases , rendering patients with cancer unable to obtain timely care . 
the uks nhs currently has more than 46 million people on waiting lists for surgery and 300 000 people have been on hold for more than 12 monthsa wait time that is 100 - times higher than before the pandemic . 
a large proportion of these delays are for patients with cancer , and the royal college of surgeons is particularly concerned , stating that it could take several years to clear the backlog . 
moreover , uk cancer surgeons are increasingly fearful of a wave of compensation claims from patients unable to receive their treatment during the pandemic and whose cancers despite this gloomy narrative , perhaps some hope can be gleaned from the crisis . 
the uk medicines and healthcare products regulatory agency ( mhra ) s rapid approval of the biontech / pfizer and oxford / astrazeneca covid - 19 vaccines , enabling their swift rollout , could help to accelerate approvals of other new drugs , including cancer treatments . 
for example , belzutifan , a promising treatment for von hippel - lindau disease that causes renal cell carcinoma , has received a so - called innovation passport from the mhra , putting it on track to receive an approval decision within 150 days of the final submission of trial data . 
the developers of the oxford / astrazeneca vaccine have founded a new biotechnology company that will use the technology underpinning their vaccine to develop new cancer therapies , and a trial of a new treatment for nonsmall - cell lung cancer will begin soon . 
if these drugs can be administered at home to prevent severe illness and hospitalisation , pressures on health systems will be reduced , allowing other health services , including cancer care , to get back on track . to mitigate the devastating effects of the pandemic on cancer care , the uk and other countries need to capitalise on the scientific advances of the past 12 months to recoup some of the huge losses and setbacks . 
effective cooperation and collaboration within and between countries , unlike that regrettably displayed by some governments regarding vaccine distribution , is essential and must not stop once the pandemic response is scaled back . 
the incident , which killed at least 220 people and left more than 6000 injured , devastated huge areas of the city , including hospitals and health - care facilities , piling enormous new pressures on a health - care system whose resources were already stretched financially and by the ongoing covid - 19 pandemic . saint george hospital university medical center , located in the city centre and one of the biggest hospitals in beirut , was so badly damaged as a result of the explosions that it was forced to close and send its patients elsewhere . 
those affected included patients with cancer who were in the middle of their chemotherapy treatmentsome of whom panicked and fled without notifying medical staff . rabih said , a member of the oncology team at saint george hospital university medical center , described the challenges faced by staff in the chaos of evacuating patients from a hospital that had been demolished by the blasts . 
we lost some of our colleagues in the explosions , while patients witnessed the traumatic death and serious injury of family members and others within the hospital . it was particularly challenging to organise the evacuation of patients with cancer who were immunocompromised and cytopenic , raising the risk of bleeding and infection , especially during the covid - 19 pandemic . peter noun , a paediatric oncologist who works with more than 100 children in units at saint george and the lebanese hospital geitaouianother nearby hospital that was severely damaged and forced to closeis worried about the disruption this has caused to his patients treatment . our major concern now is where to continue the chemotherapy for our kids , noun explained . 
more than 45 of our patients have already missed one chemotherapy session , and it may be weeks before we are able to resume their treatment schedules . further to the damage and disruption caused to hospitals and medical centres , a warehouse containing large stocks of medicines was also destroyed near the site of the explosions . 
as well as vaccines and other essential medicines , it contained a supply of chemotherapy products to be distributed to patients across lebanon . although we do not yet know the extent of the damage , a significant number of cancer drugs were stored in a warehouse close to the explosion site , said confirmed . 
this is hugely concerning , as there was already a shortage of cancer treatments due to lebanons financial crisis and the cost of cancer drugs , making access to various expensive medications a challenge even before the blasts . there are also concerns over toxins released by the explosions , which could pose severe health risks in both the short and long term , including an increased incidence of cancer . 
lebanons health minister issued a warning about the potentially hazardous effects of toxic air pollutants , such as nitrogen dioxide , following the incident , advising those who were able to leave the area to do so . friends after months of severe economic crisis , our close from lebanon will have to survive another disaster , reflected benjamin besse ( gustave roussy institute , villejuif , france )  . 
with more than 6000 injured people , hospitals have to prioritise first aid over cancer diagnosis and care . enrique soto prez de celis ( national institute of medical science and nutrition , mexico city , mexico ) agreed : disasters such as this one can be extremely challenging for health - care systems , not only by causing direct loss of life , but also by compromising the availability of medical services to treat other diseases such as cancer . damage to clinics and hospitals can break the continuity of cancer therapy and jeopardise patient care , particularly for the most vulnerable , such as older adults or those receiving palliative or end - of - life care , who are in risk of losing access to urgent medications , he continued . 
this highlights the relevance of training first responders who are part of rapidresponse teams deployed to disaster areas to implement essential noncommunicable disease interventions , include essential cancer and to medications in emergency kits . meanwhile , richard penson ( harvard medical school , boston , ma , usa ) commented on the international relief response to the disaster : covid - 19 has distanced us from our patients and our neighbours , but somehow heightened an awareness of the need to meet injustice with action . 
we are traumatised together and must act together . elizabeth gourd vol 21 september 2020 1143 time to talk about planetary health and cancer care the 46th annual scientific meeting of the clinical oncology society of australia ( cosa ) was held on nov 1214 , 2019 , in adelaide , sa , australia . 
amid sessions on the meetings themes of urological cancers , age and gender issues , and digital health , was one that discussed the interface between cancer and environmental and political change . 
as many communities across australia were dealing with an unprecedented week of bush fires , the decision to set aside time to discuss cancer care in the context of the environment comes at a watershed moment . 
the fires brought to the fore a debate on what is thought to be a major cause of the drought conditions that have precipitated the worsening bush fire season climate change . lauded although some appear to question the link between climate change and the bush fires , it cannot be denied that the health of the planet affects that of human for reducing beings . 
australia should be greenhouse gas emissions by championing renewable energy ; however , it is also the third biggest exporter of fossil fuels , as measured by co2 potential , which is likely to have consequences on global and national scales . 
 a reluctance to acknowledge the potential effects of climate change on human health on a global scale will hinder progress to mitigate such consequences . designating climate change as a public health issue , the 2019 report of the lancet countdown on health and climate change , published in november , 2019 , suggests that a child born today will live in a world that is more than 4c warmer than that in the pre - industrial age , with health consequences evident throughout life . 
in addition to the general global deterioration in air quality , isolated events , such as the bush fires , can have an immediate and direct effect on air pollution . 
furthermore , with climate change in food leading to proposed changes potentially production and human diet ( for example , as explored in the eatlancet commission ) , resultant changes in the human microbiome resulting from changing diet might also affect disease outcomes , given the recognised effect of the microbiome on responses to anticancer treatment such as immunotherapy . 
in addition to the known longterm health consequences , the destruction caused by increasing climate change - related emergencies will have an acute effect on health and health services . oncology is particularly susceptible to disruption caused by events related to climate change because of the need for long - term treatments requiring multiple trips to specialist care at tertiary hospitals ; unique and highly specialised medicines , equipment , and training ; the susceptibility of patients with cancer to other health issues ; and existing comorbidities of the patients . 
road closures , destruction of infrastructure , and population displacement due to natural disasters can lead to an array of consequences resulting in patient hardelays in the delivery of essential medical supplies ( eg , cancer drugs or time - sensitive deliveries of radioactive isotopes for cancer imaging or treatment ) , a shortage of specialist staff to provide services or perform operations in hospitals or clinics , and reduced access to clinics for the patients themselves are just some of the disruptions to vital oncology services that patients might experience . 
this issue is true whether for small island nations devastated by a category 5 hurricanecompounding the challenge of the growing cancer burden in these regionsor a city cloaked in thick smoke from a nearby forest fire . 
in 2017 , flooding from a tropical storm forced the md anderson cancer center ( houston , tx , usa ) to cancel hospital appointments due to impassable nearby roads and flooded buildings . 
with the incidence of climate - related emergencies likely to increase over time , patients with cancer are likely to feel the effects . the consequences of many years of inaction on climate change are now rapidly taking their toll on the environment and on human health worldwide . 
the lancet oncology for more on cosa 2019 see fore more on the australian bush fires see reuters.com / article / us - australiabushfires / lack - of - forecast - rainsto - prolong - australian - bushfiresthreat - iduskbn1xo01c for discussion of climate change and the bush fires see politics / federal / raving - innercity - lunatics - michaelmccormack - dismisses - linkbetween - climate - change - andbushfires - 20191111 - p539ap . html for more on renewable energy in australia theguardian.com / australianews / 2019 / oct / 24 / australiasemissions - to - start - fallingthanks - to - renewables - boomresearchers - say for more on australian fossil fuel exports net.au / news / science / 2019 - 08 - 19 / australia - co2exports - third - highestworldwide / 11420654 for the lancet countdown on health and climate change see review lancet 2019 ; published online nov 13 . 
lancet oncol 2020 ; 21 : 101718in this news piece , the web links in the margin for the preamble to the iarc monographs and for the iarc declarations of interest were incorrect and have been amended . 
 lancet oncol 2020 ; 21 : 112526in this comment , the fourth paragraph should read one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
because overdiagnosis appears to increase with age , it is possible that overdiagnosis occurred in both groups after the age of 50 years , but could not be detected because of the design of the trial . 
 this correction has been made as of sept 1 , 2020 , and the printed version is correct . vol 21 september 2020 e418 corrections asbestos exposure : the dust cloud lingers exposure to asbestos fibres is to blame for most ( > 80% ) cases of the notoriously incurable cancer , malignant mesothelioma . 
con sequently , the most dangerous forms of asbestos ( blue and brown ) were banned in the uk in 1985 , and white asbestos was eventually barred in 1999 . 
the long lagtime between asbestos exposure and mesothelioma development ( around 2050 years ) means that the current uk peaks in mesothelioma deaths are probably a result of industrial exposure in the 20th century . 
 however , numbers of diagnoses and deaths in the uk have begun to plateau in the past 5 years , and are predicted to decline in the coming years due to the effects of the legislation implemented several decades ago . by contrast , in the usa , ten states and washington , dc , are suing the environmental protection agency for failing to enforce strict rules on the use of asbestos . 
an initial ban on asbestos in 1989 was overturned in 1991 , and federal law still allows some regulated use of asbestos ( eg , in roofing , ceiling , and flooring materials )  . 
around 3000 new mesothelioma cases and 2500 related deaths are recorded annually in the usa , with the highest incidence in states with a history of shipbuilding and industry , such as maine and alaska . the usa is not the only country that still uses asbestos . 
we can only expect the incidence of asbestos - related mesothelioma and other diseases in these countries to continue to rise unless governments act to address this highly preventable cause of premature death . 
nine of 17 trials assessed had a fragility index of 2 or less ; if two patients or fewer in the experimental group had had a progression or overall survival event instead of no event , the results would not have been significant . 
 these results highlight a worrisome potential weakness in the evidence used by the fda for approvals and beg the question : should more than one significant , positive phase 3 rct be mandated for cancer drug approvals ? arguments against requiring significant , positive results from multiple phase 3 rcts are substantive ( avoiding research waste ) , ethical ( ensuring patients receive the likely superior drug ) , practical ( survival endpoints have long follow - up , patient accrual is challenging , and high costs ) , and cynical ( sponsors might be resistant to funding more than one trial )  . 
if the quantity of evidence required for drug approval does not change , we should demand real - world effectiveness ( and not just toxicity ) data for all approved drugs , either from phase 4 post - marketing trials or through real - world data from patients , and act on these results if they differ substantially from those originally submitted as evidence . 
the addition of the fragility index to more traditional statistical approaches also challenges our ideas about clinical trial design , including statistical design , and whether we must redefine our notion of a positive result . 
the lancet oncology for the study by del paggio and tannock see articles lancet oncol 2019 ; 20 : 106569 vol 20 august 2019 1035 editorial new decade , new opportunities ? the arrival of a new decade , and the observance of world cancer day on feb 4 , 2020 , provide an opportunity to reflect on the progress achieved in oncology and to anticipate what lies ahead . 
great advances in cancer research , treatment , and survival have clearly been madefor example , in the uk , cancer mortality is now half that recorded in the 1970s . 
13 themes emerged , including cancer prevention ( eg , vaccination , screening , and public health interventions ) ; improved access to , and provision of , palliative care and opioids ; and monitoring of longterm toxicity and treatment sequelae in cancer survivors . 
 the high price of cancer care was also raised as a crucial issue , including the need for an honest debate on the true value of new drugs and other interventions . 
at the research level , an improved understanding of cancer biology , especially for refractory cancers , was noted as an urgent need , along with the identification of highrisk patients and early predictors of treatment response . 
 inclusion of neglected patient groups and rare cancers in research and policy initiatives featured in many responses , as did the need to reduce the administrative burden and barriers involved in cancer research and clinical studies alike . 
finally , the central role of big data , real - world data , and data sharing in artificial intelligence and digital health were highlighted as major step - change opportunities . 
for example , the uk spends just 01% of its gdp on anticancer drugs , and just 78% of nhs expenditure on cancer care , even though the disease causes almost a third of all deaths . 
 therefore , in addition to developing low - cost alternatives to existing cancer treatments and attempting to drive down current prices , correctly intentioned and strong political will is crucial to ensure provision ofand access toaffordable cancer treatment for all in appropriately funded , well organised , patient - centred health systems . as we move into an increasingly digital era , digital health will provide major opportunities for future cancer control . 
artificial intelligence is now being used to aid early diagnosis , as portrayed in numerous studies showing that artificial intelligence - based screening and imaging can outperform radiologists and pathologists . 
this is especially true for rare cancers and neglected patient groups , because data samples from many small populations can be combined , enabling and enhancing research in settings in which it might be difficult or even impossible to do traditional clinical trials . 
however , the explosion of data generation , data storage , and its use , demands the right expertise and governance to prevent misinterpretation and exploitation . despite the many opportunities that exist for cancer control over the next decade , we will not reap the benefits of such efforts without health system reform worldwide that delivers affordable cancer care for all . 
we also need structural change to ensure that cancer research funding and administration supports diverse and exploratory aims ; clinical trials are better designed to avoid the influence of vested interests and proprietary protectionism ; and oncologists have properly protected time to participate in research . 
all of this must also happen within the bigger context of an environmental catastrophe ; erosion of basic human rights ; and political extremis only with rational and ambitious actions can we make the 2020s a decade of possibility , rather than one of disappointment . 
indeed , they could be more likely to develop severe complications of covid - 19 , owing to their immunosuppressed status caused by both the cancer and anticancer therapies , such as radiotherapy , chemotherapy , and surgery.2 in this urgent situation , it is crucial to characterise the clinical features , risk factors , and outcomes of patients with cancer and covid - 19 . in the lancet oncology , results from two independent , multicentre studies on patients with cancer and covid - 19 have been publishedboth done in hubei , china , the initial epicentre of the pandemic . 
kunyu yang and colleagues investigated the clinical characteristics , outcomes , and risk factors for mortality in 205 patients with cancer and covid - 19.3 30 ( 15% ) patients were transferred to an intensive care unit and 40 ( 20% ) died while in hospital . 
receipt of chemotherapy within 4 weeks of symptom onset was a risk factor for in - hospital death ( odds ratio [ or ] 351 [ 95% ci 1161059 ] ; p = 0026 )  . 
 yang and colleagues also highlighted that compared with patients with solid tumours , those with haematological malignancies had a higher case - fatality rate ( nine [ 41% ] of 22 patients vs 31 [ 17% ] of 183 patients ) and had more severe events such as acute respiratory distress syndrome ( six [ 27% ] of 22 vs 17 [ 10% ] of 177 ) and acute renal failure ( four [ 18% ] of 22 vs nine [ 5% ] of 177 )  . 
faster disease progression , more frequent hospital admissions for chemotherapy , increased susceptibility to bacterial co infection , and greater myelosuppression and immunosuppression could explain the poorer prognosis patients with haematological malignancies compared with those with solid tumours . 
in the second study in the lancet oncology , jianbo tian and colleagues included 232 patients with cancer and covid - 19 during the same period , who were statistically matched to patients with covid - 19 without cancer.4 tian and colleagues found that patients with cancer had increased risk of developing severe or critical covid - 19 than patients without cancer ( or 361 [ 259504 ] ; p < 00001 )  . 
they also identified several novel predictors for poor prognosis , such as advanced tumour stage ( or 260 [ 95% ci 105643 ] ; p = 0039 ) , elevated tumour necrosis factor ( 122 [ 101147 ] ; p = 0037 ) and n - terminal pro - b - type natriuretic peptide ( 165 [ 103278 ] ; p = 0032 ) , and reduced cd4 + t cells ( 084 [ 071098 ] ; p = 0031 )  . it should be noted that the two studies have inherent limitations . 
moreover , the authors did not analyse the frequent thrombophilic complications in cancer as well as in covid - 19 : deep vein thrombosis and pulmonary embolisdespite these limitations , the two groups have provided information that can help to provide more appropriate care for patients with cancer and severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection and monitor reliable markers during the infection course . a few other short reports with small sample sizes have also focused on patients with cancer , describing clinical characteristics of patients with cancer and investigating their prognosis.57 the studies found higher risk of sarscov - 2 infection in patients with cancer compared with the general population in wuhan , 5 and higher risk of severe events in patients with cancer and covid - 19 , 6 particularly those who had received antitumour treatment recently.7 when taking all studies into consideration , patients with cancer and covid - 19 in china have a case fatality rate of up to 20% , which is much higher than that of the community ( 1872% ) , as reported in various countries ( figure )  . 
moreover , patients with cancer who had received chemotherapy , targeted therapy , or immunotherapy , or had undergone surgery 24 weeks before presenting with covid - 19 were found to have an approximately 4 - times higher risk for in - hospital death than patients who had not been recently treated with anticancer therapies 862 vol 21 july 2020 comment ( figure )  . 
in multivariable logistic regression analysis in the study by tian and colleagues , these therapies were found to confer a 329 times ( 95% ci 126861 ; p = 0015 ) increased risk of developing severe covid - 19.4 therefore , oncology teams should pay close attention to immunotherapy - related adverse effects , such as severe neurotoxicity , myocarditis , and pneumonitis , which might negatively affect survival of patients with covid - 19 . the data described above raise an important issue : should anticancer treatment be postponed during the covid - 19 pandemic ? we should keep in mind that the primary risk for patients with cancer during the pandemic is reduced access to hospitals and inability to receive necessary medications in a timely fashion . 
all aspects of cancer treatment have been affected : not only screening , referral , and clinical testing in symptomatic cancer diagnosis , but also treatment and follow - up of patients with cancer.8 a report from the netherlands has shown a decrease in cancer diagnoses during the covid - 19 pandemic , with the overall rate of cancer diagnosis decreasing by 27% from jan 6 to march 2 , 2020.9 patients might be anxious about being exposed to sars - cov - 2 in a health - care setting , and might struggle to consult with a general practitioner in the midst of strict social distancing and in this context , lockdown policies . 
extreme caution is required in delaying life - saving cancer therapies . some preliminary recommendations have been proposed to guide decisions on delaying or continuing cancer treatment during the covid - 19 pandemic . 
for some types of tumour including lung and pancreatic cancer , acute leukaemia , and highly aggressive lymphoma , timely diagnosis and yang et al ( 2020 ) 3 tian et al ( 2020 ) 4 yu et al ( 2020 ) 5 zhang et al ( 2020 ) 7 overall ( i = 00% , p = 0755 ) yang et al ( 2020 ) 3 liang et al ( 2020 ) 6 yu et al ( 2020 ) 5 zhang et al ( 2020 ) 7 overall ( i = 00% , p = 0815 ) 0495 0495 case - fatality rate ( 95% ci ) study weight * 020 ( 014025 ) 020 ( 015025 ) 025 ( 001049 ) 029 ( 012045 ) 4401% 4921% 216% 463% 020 ( 017024 ) 10000% odds ratio ( 95% ci ) 351 ( 1161059 ) 534 ( 1801618 ) 138 ( 0101964 ) 408 ( 1091532 ) study weight * 3461% 3510% 607% 2423% 399 ( 208764 ) 10000% 005 2000 figure : pooled analysis from the current published evidence ( a ) case - fatality rate of patients with cancer and covid - 19 . 
 ( b ) odds ratio for in - hospital death for patients receiving anticancer therapies within 24 weeks before onset of covid - 19 versus those who did not receive such anticancer therapies . 
these recommendations can be cautiously applied in current clinical practice until evidence - based guidelines are available.10 in conclusion , patients with cancer have worse clinical outcomes of covid - 19 than those without cancer . 
 further studies regarding comprehensive management of patients with cancer and covid - 19 are urgently needed to provide better health care to this patient population . we declare no competing interests . liang v tang , * yu hu dr_huyu@126.com institute of hematology , union hospital , tongji medical college , huazhong university of science and technology , wuhan 430022 , china bray f , ferlay j , soerjomataram i , siegel rl , torre la , jemal a . 
the discovery of driver mutations in the kit and pdgfra genes has led to clinical development of three tyrosine kinase inhibitors ( tkis ) imatinib , sunitinib , and regorafeniband has revolutionised treatment and prognosis of patients with advanced gastrointestinal stromal tumours . 
however , primary and secondary resistance to these drugs limit their activity and , eventually , almost all gastrointestinal stromal tumours progress , mainly due to acquired mutations.1 these tkis inhibit kit and pdgfra tyrosine kinases by competitively binding to their atp - binding domains with atp , thus , most acquired mutations are found in the atp - binding pocket or activation loop of the kit or pdgfra gene , resulting in reactivation of the corresponding kinase.2 acquired mutations after tki therapy are highly variable and are heterogeneous in a patient , even within a single lesion . 
furthermore , refractory gastrointestinal stromal tumours might potentially have different resistance mechanisms other than acquired mutations.3 hence , the activities of tkis with similar mode of action are limited after imatinib ; median progression - free survival of sunitinib in the second - line is 68 months and that of regorafenib in the third - line is 48 months.4 , 5 since the approval of regorafenib in 2012 , many agents have been evaluated for fourth - line therapy , but none of them were approved for patients with gastrointestinal stromal tumours that were refractory to three tkis until the end of 2019 . ripretinib is designed to stabilise kit and pdgfra tyrosine kinases in an inactive conformation by binding to switch pocket regions and is shown to specifically inhibit the wide spectrum of primary and secondary resistant mutations found in the atp - binding pocket or activation loop of kit and pdgfra , and also other mutated kinases ( eg , braf in in - vitro experiments and mouse models ) .6 in the lancet oncology , jean - yves blay and colleagues7 report the results of the invictus study , which examined the efficacy of ripretinib in patients with gastrointestinal stromal tumours that were refractory or intolerant to three available tkis in a placebo - controlled , double - blind , randomised phase 3 study . 
median progression - free survival , the primary endpoint , was longer in the ripretinib group than in the placebo group ( 63 months [ 95% ci 4669 ] vs 10 month [ 0917 ] , hazard ratio 015 , 95% ci 009025 , p < 00001 ) and the objective response rate , the key secondary endpoint , was higher in the group that received ripretinib ( 9% , 95% ci 418 ) than in the group that received placebo ( 0% , 08 ) by the central review , although this difference was not statistically significant ( p = 0050 )  . 
moreover , ripretinib had an improved overall survival , with a median overall survival of 151 months compared with 66 months in the placebo group despite crossover to riprecinib from placebo , which was permitted after disease progression . 
however , due to hierarchal testing , overall survival could not be formally tested 864 vol 21 july 2020 comment acting on misinformation to prevent patient harm a group of government ministers are in discussions to call for an expansion of the remit of the uks cancer act , according to a recent report . 
the aim is to broaden the scope of the act to include the regulation of clinically unproven diagnostic procedures , to prohibit dangerous treatments , and to introduce stricter controls of social media posts about purported cancer cures . 
 lockdown following an unprecedented national intro duced across the uk in march , 2020 , as a result of the initial covid - 19 outbreak , cancer screening services were suspended , routine diagnostic work was postponed , and urgent referrals for suspected cancer declined dramatically . 
the absence of national health service ( nhs ) - based cancer diagnosis and treatment , and fears about a huge backlog of patients with cancer in the uk , have left a vacuum that those peddling unproven and unapproved tests and interventions have tried to fill . 
thus , review and revision of the cancer act to address this emerging threat to patient safety is welcome . enacted by the uk houses of parliament in 1939 , the cancer act was introduced with the aim to make further provision for the treatment of cancer , to authorise the minister of health to lend money to the national radium trust , to prohibit particular advertisements relating to cancer , and for purposes connected with the matters aforesaid . 
although the act has since been revised , the remaining provision prohibiting any advertisements that offer to treat or cure cancer remains in effect to this day , and has led to the prosecution of many individuals guilty of advertising unproven cures for cancer , including in the past decade . 
crucially , the act does not cover advertising of purported cancer diagnostic tests ( eg , thermography ) or the undertaking of such tests that , although unapproved and often debunked , have been shown to lead to false hope for those with cancer and even the tragic deaths of some patients . 
tighter regulation is , therefore , needed to prevent the dissemination of misleading claims used to market health products or tests , especially online . online advertisements , and particularly social media , are largely responsible for the the widespread visibility of unapproved cancer diagnostic tests and false cancer cures . 
individuals preying on the vulnerability of patients to sell fake medical products is an age - old problem , but the advent of social media has led to an exponential proliferation of advertising of such products online . 
with the added challenge of covid - 19 lockdowns in various countries affecting cancer care , patients with cancer and their families might be even more susceptible to advertisements that offer hope for their illness . 
in some countries , such as the usa , advertisement of genuine and clinically proven cancer treatments are permitted , which can make the regulation of unproven so - called miracle cures for cancer particularly difficult in the absence of relevant regulations . fortunately , steps are being taken to combat this rise in misinformation . 
 but the rise in misleading information in relation to the covid - 19 pandemic suggests that existing measures are not suffi cient and further efforts are needed to halt this trend . increase vigilance are , of course , to reduce , if not eliminate , the promotion of fake cancer cures , a multifaceted approach is needed . 
 the lancet oncology for the report on the discussion on the cancer act see news / 2020 / 08 / 09 / cross - partycoalition - seeks - revamplegislation - crack - fake - cancer / for the cancer act 1939 see ukpga / geo6 / 2 - 3 / 13 for examples of prosecutions for breaching the cancer act 1939 in the past decade see uk / trading - standards - cancercure - claims - prosecuted for more on false hope given by cancer diagnostic tests see health - 53407636 for more on patients and groups tackling health misinformation see technology / healthmisinformation - online.html for more on social media measures to crack down on misinformation see youtube - overrun - with - boguscancer - treatmentclaims - 11562072401 for more on misleading information about covid - 19 see washingtonpost.com / technology / 2020 / 08 / 11 / facebook - covid - misinformationtakedowns / vol 21 september 2020 1123 editorial correction to lancet oncol 2019 ; 20 : 128694 correction to lancet oncol 2019 ; 20 : 1506517 correction to lancet oncol 2019 ; 20 : e616 burki tk . 
 ff l u c i c l o v i n e a n d ga - psma - 11 pet - ct in patients with early biochemical recurrence after prostatectomy : a prospective , single - centre , single - arm , comparative imaging trial . 
lancet oncol 2019 ; 20 : 128694in this article , in figure 2 , the f - fluciclovine detection rate for prostate bed has been corrected to 9 ( 18% )  . 
this correction has been made to the online version as of sept 23 , 2019 . correction to lancet oncol 2019 ; 20 : 160214 oscarsson n , mller b , rosn a , et al . 
lancet oncol 2019 ; 20 : 1602 14in the summary of this article , the first sentence of the findings section should have read of 223 patients screened between may 9 , 2012 , and dec 20 , 2017 , 87 patients were enrolled and randomly assigned to either hyperbaric oxygen therapy ( n = 42 ) or standard care ( n = 45 )  . 
 this correction has been made to the online version as of sept 23 , 2019 , and the printed article is correct . kato k , cho bc , takahashi m , et al . 
nivolumab versus chemotherapy in patients with advanced oesophageal squamous cell carcinoma refractory or intolerant to previous chemotherapy ( attraction - 3 ) : a multicentre , randomised , open - label , phase 3 trial . 
 lancet oncol 2019 ; 20 : 1506517in this article , the name of the funder should be ono pharmaceutical company , and in the results section , paragraph eight , the data for the comparison between groups for the utility index should have been 0076 , 00110142 ; p = 0023 . 
lancet oncol 2019 ; 20 : e52234in this series paper , the value 55% was missing from in the the following sentence first paragraph of the strategies for providing paediatric oncology services section : data from hospital - based registries in the english - speaking caribbean islands show a 2 - year survival rate of 55% compared with 85% in hics . 
this correction has been made to the online version as of oct 30 , 2019 . published online september 23 , 2019 s1470 - 2045 ( 19 ) 30594 - 7 vol 20 november 2019 e613 corrections correction to lancet oncol 2019 ; 20 : 38393 correction to lancet oncol 2019 ; 20 : 134959 correction to lancet oncol 2019 ; 20 : e64552 oar a , moraes fy , romero y , ilbawi a , yap ml . 
 lancet oncol 2019 ; 20 : 38393in table 2 of this article , data in the any adverse event , n ( % ) row were corrected for the grade 3 and grade 4 columns . 
these corrections have been made to the online version as of dec 2 , 2019 . correction to lancet oncol 2019 ; 20 : 134244 oladeru ot , perni s , williams b . 
 this correction has been made to the online version as of dec 2 , 2019 . correction to lancet oncol 2019 ; 20 : 154455 infante naing a , wong dj , jr , et al . 
the appendix has been updated as of dec 2 , 2019 . vol 20 december 2019 e663 correction correction to lancet oncol 2014 ; 15 : 150312 correction to lancet oncol 2019 ; 20 : 76980 correction to lancet oncol 2019 ; 20 : 98699 open - label phase 1 / 2 jg , niesvizky r , kumar sk , berdeja et al . 
 lancet oncol 2014 ; 15 : 150312in the eighth paragraph of the results section of this article , the first sentence should have been overall responses were noted in 59 ( 92% , 95% ci 8397 ) of 64 patients ( table 5 )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 765 ben - aharon i , goshen - lago t , fontana e , et al . 
this correction has been made to the online version as of july 1 , 2019 . 2018 jacob s , yap ml , wilson be , ferlay j , bray f , barton mb . 
 lancet oncol 2019 ; 20 : 76980 in the affiliations for this article , dr mei ling yap should have been affiliated with the university of new south wales ( sydney , nsw , australia )  . 
this correction has been made to the online version as of july 1 , 2019 . correction to lancet oncol 2019 ; 20 : 795805 randomised , controlled hofvind s , holen s , aase hs , et al . 
 lancet oncol 2019 ; 20 : 795805 in figure 1 , the number of patients with screen - detected breast cancer in the digital breast tomosynthesis group should have read 95 , and the number of patients in the digital mammography group should have read 87 . 
 quizartinib versus salvage chemotherapy in relapsed or refractory flt3 - itd acute myeloid leukaemia ( quantum - r ) : a multicentre , randomised , controlled , open - label , phase 3 trial . 
lancet oncol 2019 ; 20 : 98699in this article , the second sentence in the statistical analysis section should have read the sample size calculation wording in the original protocol specified a 5% , two - sided calculation ; however , this wording was inaccurate , and subsequently , a one - sided calculation at 25% was implemented to solely test for superiority of quizartinib , which is consistent with the primary aim of the study . 
this correction has been made to the online version as of july 1 , 2019 , and the printed article is correct . correction to lancet oncol 2019 ; 20 : e30212 hillengass j , usmani s , rajkumar sv , et al . 
these corrections have been made to the online version as of july 1 , 2019 . vol 20 july 2019 e346 corrections guidelines , and the country - specific covid - 19 case burden will dictate our actions , most likely negatively . in west africa , covid - 19 protocols are defined by individual institutions . 
patients with a fever are referred to the emergency roo a minimum number of essential staff ( in protective gear when available ) will be rotated , prescriptions refilled remotely , and second - line and third - line palliative chemotherapy halted . 
of particular concern is the large population infected by hiv , which includes approximately 8 million people.6 while public hospitals prepare for the first wave of covid - 19 patients , oncology services at this point are still aiming to deliver full service when follow - up outpatient services possible , although have been severely curtailed . 
staff will be divided into teams consisting of core personnel . in sudan , despite the low covid - 19 burden , cancer centres have established a contingency plan by deferring new referrals except for emergency surgery , non - urgent intravenous cases . 
 medical teams and core support staff work as divided teams after having attended mandatory covid - 19 training sessions . oncologists in africa , in the absence of centralised and resource - appropriate covid - 19 guidelines , are pragmatically safeguarding patients and the workforce while providing essential cancer care . 
korle bu teaching hospital , accra gqqf + 6r , ghana ( vv ) ; the national cancer institute , university of gezira , wad madani , sudan ( mmae ) ; and stellenbosch university , stellenbosch , south africa ( hs ) yu j , ouyang w , chua mlk , xie c . 
countries / southafrica ( accessed march 29 , 2020 )  . the uk coronavirus cancer monitoring project : protecting patients with cancer in the era of covid - 19 published online april 15 , 2020 s1470 - 2045 ( 20 ) 30230 - 8 the uk coronavirus cancer monitoring project ( ukccmp ) aims to collect , analyse , and disseminate in real time data from the uk cancer centres about severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection rates in patients with cancer , and their outcomes in terms of coronavirus disease 2019 ( covid - 19 )  . 
this approach will enable oncologists to gain crucial insights to inform decision making . 622 vol 21 may 2020 comment s for more on the uk coronavirus cancer monitoring project see ukcoronaviruscancermonitoring . identified in december , 2019 , several cases of acute respiratory syndrome in hubei province , china were identified ; these were the first described cases of covid - 19 . 
 the causative virus , sars - cov - 2 , is a new strain of betacoronavirus previously not humans and thought to be of zoonotic origin.1 the presentation of covid - 19 varies from no or minor symptoms akin to the common cold , to severe acute respiratory distress syndrome , resulting in severely impaired respiratory function.1 sars - cov - 2 is highly contagious through direct transfer of respiratory droplets during coughing and sneezing or indirect fomite spread via contaminated surfaces.2 this simple transmission , coupled with international travel , has enabled rapid spread of the virus with more than 870 000 cases and 43 000 deaths reported worldwide as of april 1 , 2020.3 approximately 25 million individuals live with , or have a history of , cancer in the uk , with 1000 new diagnoses each day.4 of these patients , a substantial proportion require , are undergoing , or are recovering from surgery and complex treatments . 
patients with cancer potentially have increased susceptibility to sars - cov - 2 infection and have more serious sequelae , resulting from impaired immune function due to cancer itself , cancer treatment , or both.5 , 6 wenhua liang and colleagues6 reported their identification of 18 patients with cancer in a cohort of 1590 patients with covid - 19 in china , indicating an increased incidence of covid - 19 in patients with cancer compared with the general chinese population ( 113% vs 029% )  . 
the incidence of covid - 19 in patients with cancer ( 12 [ 079% ] of 1524 patients ) was higher than in the general wuhan population ( 037% )  . patients with specific types of cancer might be at an increased risk of covid - 19 , with both these reports highlighting the high proportion of patients with lung cancer with confirmed diagnoses of covid - 19 ( five of 18 patients in liang et al , 6 and seven of 12 in yu et al7 )  . 
severe infection with sars - cov - 2 is associated with cytokine storm and increased concentrations of c - reactive protein and il - 6 pneumonitis , severe adverse events that are also lymphocyte associated with immune checkpoint inhibitor therapy.8 consequently , patients on immunotherapy could be at increased risk from covid - 19 . 
therefore , sars - cov - 2 inflammatory infection is highly unlikely to affect all patients with cancer equally . little effect on populations , the european society of medical oncology has published guidelines on how to mitigate the effect of covid - 19 on patients with cancer , by prioritisation of cancer treatment in patients expected to derive a substantial absolute survival benefit , reducing hospital visits , and converting from intravenous to oral regimens.9 however , these guidelines take a broad approach for a very heterogenous population . 
policies , including self - isolation and social distancing , are widely acknowledged to be required to suppress viral spread , both in the general and at - risk populations , thereby reducing pressure on already stretched healthreallocation care of resources away from cancer care services could potentially have unintended cancer - related implications , including increased morbidity and mortality . 
a local emergency response reporting group has been created at each uk cancer centre to ensure continued updating of the ukccmp live clinical data dissemination systethe project will collect data on patients with cancer who are positive for sars - cov - 2 infection , including tumour type and stage , patient age , present cancer treatment , and clinical outcomes , with the aim to enable oncologists to gain crucial insights to inform decision making . 
 data collection , analysis , and dissemination coordinated by the centre for computational biology at the university of birmingham , ( birmingham , uk ) through a dedicated workflow hosted by the compute and storage for life science infrastructure as part of vol 21 may 2020 comment the birmingham environment for academic research local cloud.10 ukccmp delivers meaningful real - time data to all uk cancer centres and clinicians to allow more personalised approaches to individual patient care and inform clinical decision making . 
this initiative will improve cancer care in the uk and beyond at this time of unprecedented global turmoil and reliance on health - care resources . we declare no other competing interests . 
the university of birmingham initiated this process , with the pro - vice - chancellor dedicating the computational and human resources of the universitys centre for computational biology , the institute of translational medicine , and scientists from the institute of cancer and genomic sciences . 
other academic institutions dedicating time and staff to the project include the university of oxford , university of leeds , university college london , edinburgh cancer centre , clatterbridge cancer centre , and kings college london . the uk coronavirus cancer monitoring project team lennard.lee@nhs.net huang c , wang y , li x , et al . 
 joint - mission - on - covid - 19 - final - report.pdf ( accessed april 9 , 2020 )  . coronavirus covid - 19 global cases by the center for systems science and engineering at johns hopkins university ( jhu )  . 
castles ( compute and storage for the life sciences ) : a collection of compute and storage resources for supporting research at the university of birminghabirmingham : birmingham environment for academic research , june 20 , 2019 . 
 ( accessed april 7 , 2020 )  . recommendations from national regulatory agencies for ongoing cancer trials during the covid - 19 pandemic clinical research has transformed cancer care and is often integrated seamlessly into routine oncology clinics , offering eligible patients additional treatment options or lines of therapy . 
typically , and particularly for diseases with poor prognoses or when trials entail biomarker - directed personalised treatment , clinical trial enrolment can be preferred ( by both doctors and patients ) over standard care.1 however , many barriers already preclude patients participation in clinical trials , with only a small proportion enrolled in interventional trials.2 the coronavirus disease 2019 ( covid - 19 ) pandemic presents an additional major barrier to patients enrolment and ongoing participation in clinical trials . 
institutions are adapting their oncology practice , considering alternative treat ment strategies to appropriately balance risks and benefits , despite the absolute individual risk increases from covid - 19 for patients being currently unknown.3 the us food and drug administration ( fda ) and other international bodies have released guidance for sponsors and study sites to ensure the safety of trial participants while maintaining compliance with good clinical practice and minimising risks to study integrity . 
this guidance is summarised in the panel.410 although this guidance is very welcome and helpful , specific considerations must be made for each trial , in view of the wide variety of study types , relative complexities , and perceived risks and benefits . 
many study sites and sponsors have already stopped study enrolment , and it is not clear when these studies will reopen because of the probable prolonged effects of the covid - 19 pandemic . 
for patients on study treatment , the difficult decision to stop or carry on with the investigational medical product or other study treatments should be discussed between see online for appendix members of the uk coronavirus cancer monitoring project team are listed in the appendix ( p 1 )  . 
 institute of cancer and genomic sciences , university of birmingham , birmingham b15 2tt , uk published online april 8 , 2020 s1470 - 2045 ( 20 ) 30226 - 6 624 vol 21 may 2020 comment correction to lancet oncol 2020 ; 21 : 26170 correction to lancet oncol 2020 ; 21 : 80820 correction to lancet oncol 2020 ; 21 : 92334 blay j - y , serrano c , heinrich mc , et al . 
quality of life in patients with cervical cancer after open versus minimally invasive radical hysterectomy ( lacc ) : a secondary outcome of a multicentre , randomised , open - label , phase 3 , noninferiority trial . 
this correction has been made to the online version as of june 29 , 2020 . vol 21 july 2020 e341 corrections circulating tumour dna analysis to direct therapy in advanced breast cancer ( plasmamatch ) : a multicentre , multicohort , phase 2a , platform trial nicholas c turner , belinda kingston , lucy s kilburn , sarah kernaghan , andrew m wardley , iain r macpherson , richard d baird , rebecca roylance , peter stephens , olga oikonomidou , jeremy p braybrooke , mark tuthill , jacinta abraham , matthew c winter , hannah bye , michael hubank , heidrun gevensleben , ros cutts , claire snowdon , daniel rea , david cameron , abeer shaaban , katrina randle , sue martin , katie wilkinson , laura moretti , judith m bliss * , alistair ring * summary background circulating tumour dna ( ctdna ) testing might provide a current assessment of the genomic profile of advanced cancer , without the need to repeat tumour biopsy . 
we aimed to assess the accuracy of ctdna testing in advanced breast cancer and the ability of ctdna testing to select patients for mutation - directed therapy . methods we did an open - label , multicohort , phase 2a , platform trial of ctdna testing in 18 uk hospitals . 
 patients were recruited into four parallel treatment cohorts matched to mutations identified in ctdna : cohort a comprised patients with esr1 mutations ( treated with intramuscular extended - dose fulvestrant 500 mg ) ; cohort b comprised patients with her2 mutations ( treated with oral neratinib 240 mg , and if oestrogen receptor - positive with intramuscular standard - dose fulvestrant ) ; cohort c comprised patients with akt1 mutations and oestrogen receptor - positive cancer ( treated with oral capivasertib 400 mg plus intramuscular standard - dose fulvestrant ) ; and cohort d comprised patients with akt1 mutations and oestrogen receptor - negative cancer or pten mutation ( treated with oral capivasertib 480 mg )  . 
 for cohort a , 13 or more responses among 78 evaluable patients were required to infer activity and three or more among 16 were required for cohorts b , c , and d . 
this trial is registered with clinicaltrials.gov , nct03182634 ; the european clinical trials database , eudract2015 - 003735 - 36 ; and the isrctn registry , isrctn16945804 . findings between dec 21 , 2016 , and april 26 , 2019 , 1051 patients registered for the study , with ctdna results available for 1034 patients . 
cohorts b and c met or exceeded the target number of responses , with five ( 25% [ 95% ci 949 ] ) of 20 patients in cohort b and four ( 22% [ 648 ] ) of 18 patients in cohort c having a response . 
 cohorts a and d did not reach the target number of responses , with six ( 8% [ 95% ci 317 ] ) of 74 in cohort a and two ( 11% [ 133 ] ) of 19 patients in cohort d having a response . 
17 serious adverse reactions occurred in 11 patients , and there was one treatment - related death caused by grade 4 dyspnoea ( in cohort c )  . interpretation ctdna testing offers accurate , rapid genotyping that enables the selection of mutation - directed therapies for patients with breast cancer , with sufficient clinical validity for adoption into routine clinical practice . 
our results demonstrate clinically relevant activity of targeted therapies against rare her2 and akt1 mutations , confirming these mutations could be targetable for breast cancer treatment . funding cancer research uk , astrazeneca , and puma biotechnology . copyright 2020 the author ( s )  . 
however , there has been uncertainty about the validity of ctdna testing in routine practice , as there have been few large prospective studies to assess the accuracy and utility of ctdna testing . 
in addition , sensitivity has not been perfect in previous retrospective studies , suggesting the potential for false negative ctdna results , and , in routine clinical practice , reflex testing of tumour tissue is advised to confirm negative results . 
in 2018 , the american society of clinical oncology and college of american pathologists guidelines committee on ctdna analysis concluded that the absence of prospective trials was one of the major weaknesses in the evidence for bringing ctdna testing to routine practice , with a need for trials that recruited patients solely on the basis of ctdna testing without tissue testing beforehand . added value of this study plasmamatch is , to our knowledge , the first large , prospective , multicentre study assessing the feasibility and clinical utility of ctdna analysis to direct therapy in patients with advanced breast cancer . 
patients with rare , potentially targetable mutations in her2 and akt1 in ctdna had clinically important responses with the her2 inhibitor neratinib and akt inhibitor capivasertib , respectively , similar to activity seen in previous tissue sequencing - directed trials . 
these findings confirm that these mutations are targetable for breast cancer therapy , and demonstrate the validity and clinical utility of using ctdna testing to screen patients for rare mutations . implications of all the available evidence these findings show that ctdna testing for mutations has sufficient accuracy for widespread adoption in clinical practice , with the assays used . 
the high sensitivity of ctdna testing for tissue mutations calls into question the need for reflex tissue testing for negative ctdna results , within the pretreated metastatic breast cancer patient population studied . 
 highly sensitive assays have been developed in the past 5 years to analyse circulating tumour dna ( ctdna ) , which is released into the plasma in small quantities as cancer cells die , providing the opportunity for a scalable , non - invasive approach to profile tumours for somatic mutations.10 retrospective studies show high agreement between ctdna analysis and tumour tissue - based analysis in patients with advanced cancer.11 however , previous prospective studies comparing commercially available ctdna assays have shown there might be substantial discordance in ctdna testing results , 12 , 13 raising concerns over whether ctdna testing is ready for widespread clinical adoption.14 we aimed to assess the clinical validity of ctdna testing , and to investigate the clinical utility of using ctdna to select targeted therapies for patients without previous tissue testing . methods study design and participants plasmamatch is a multicohort , open - label , nonrandomised , phase 2a clinical trial platform run across 18 uk hospitals ( appendix p 2 )  . 
those with potentially targetable mutations identified in ctdna testing ( esr1 , her2 , akt1 , or pten ) were offered entry into one of four parallel treatment cohorts ( ad ) according to the see online for appendix vol 21 october 2020 1297 articles identified , with therapies matched mutation mutations . 
a fifth cohort ( e ) recruiting patients with triple - negative breast cancer with no targetable mutation , designated to receive olaparib plus the atr inhibitor azd6738 , is ongoing and will be reported separately . 
 eligible patients were women at least 18 years of age with histologically confirmed advanced breast cancer that was not suitable for treatment with radical or curative intent , who had measurable disease , an eastern cooperative oncology group performance status of 02 , estimated life expectancy of more than 3 months , and were suitable for a baseline advanced disease biopsy or had an archival advanced disease biopsy available for subsequent retrospective sequencing and comparison with ctdna . 
 patients were required to have had disease progression on radiological or clinical assessment at registration ( with radiological confirmation required before treatment cohort entry ) , and to have completed at least one previous line of treatment for advanced breast cancer , or relapsed within 12 months of neoadjuvant or adjuvant chemotherapy . 
patients with her2 - positive breast cancer must have had at least two previous lines of her2 - targeted therapy in the advanced setting ( or one line if no further her2 - targeted therapies were available )  . 
an approved protocol amendment implemented on feb 19 , 2018 , after 515 patients had been recruited , required a maximum of two previous lines of chemo therapy , antibodydrug conjugate , or immunotherapy . 
exclusion criteria for ctdna testing included uncon trolled cns or cardiac disease , ongoing toxicities of grade 1 or higher from previous treatments , and malignancies of other types within the past 3 years . 
cohort - specific eligibility criteria are given in the protocol ( appendix )  . the study was co - sponsored by the institute of cancer research and the royal marsden national health service ( nhs ) foundation trust , london , uk , and approved by a research ethics committee ( 16 / sc / 0271 )  . 
digital droplet pcr was done at a central laboratory in the national institute for health research centre for molecular pathology at the royal marsden nhs foundation trust and institute of cancer research prospectively in all patients , for mutations in pik3ca , esr1 , her2 , and akt1 ( appendix p 4 )  . 
from july 10 , 2018 ( after recruitment of 680 patients ) , prospective testing also included error - corrected targeted sequencing with guardant360 ( guardant health ; redwood city , ca , usa ) for a panel of 73 genes including pik3ca , esr1 , her2 , akt1 , pten , and tp53 , with retro spective for previously enrolled patients . 
for sequencing results , tumour comparison with ctdna tissue sequencing using advanced disease tissue biopsies was done retro spectively for patients who entered a treatment cohort ( appendix p 5 )  . 
testing for pik3ca mutations was included to test the validity of the pik3ca ctdna testing , but was not used for entry to therapeutic cohorts as phase 3 studies of treatments for breast cancer with pik3ca mutations were ongoing when plasmamatch started recruitment.1 a positive result by either ctdna assay was sufficient for cohort entry . 
if more than one mutation was identified , entry to cohorts bd took preference to cohort a . received extended - dose 500 mg cohort a included individuals with esr1 mutations ; they fulvestrant ( a selective oestrogen receptor downregulator ) administered intramuscularly on days 1 , 8 , and 15 in cycle 1 , and days 1 and 15 in cycle 2 onwards , on a 28 - day cycle . 
in cohort a , as a prespecified exploratory analysis , esr1 mutations were determined to be clonally dominant or subclonal , with a clonally dominant mutation indicating a summed esr1 allele fraction of 50% or greater of maximum allele fraction detected in the sample by targeted sequencing to correct for variations in the purity of ctdna in plasma dna ( appendix p 5 )  . cohort b included individuals with her2 mutations ; they received 240 mg neratinib ( an irreversible pan - her tyrosine kinase inhibitor ) orally once a day on a continuous schedule . 
in patients with oestrogen receptorpositive breast cancer , this treatment was administered together with fulvestrant 500 mg intramuscularly at standard dosing ( days 1 and 15 in cycle 1 and day 1 in cycle 2 onwards on a 28 - day cycle )  . cohort c included individuals with akt1 mutations and oestrogen receptor - positive breast cancer ; they received 400 mg capivasertib ( selective akt inhibitor ) orally twice a day for 4 days on followed by 3 days off continuously with fulvestrant 500 mg intramuscularly at standard dosing . cohort d included individuals with an akt pathway activating mutation ( mutations in akt1 with oestrogen receptor - negative breast cancer , or pten inactivating mutations or homozygous deletion [ irrespective of oestrogen receptor status ] ; full criteria are described in the appendix p 6 )  . 
this cohort received 480 mg capivasertib monotherapy orally , twice a day for 4 days on , followed by 3 days off , continuously . in addition to the eligibility criteria for ctdna testing , for cohort assignment patients with a relevant targetable mutation had to have adequate haematological , renal , and hepatic function ( adequate defined as absolute neutrophil count 10 10 cells per l , platelet count 100 10 per l , 1298 vol 21 october 2020 articles haemoglobin 9 g / dl , serum crea tinine 15 the upper limit of normal [ uln ] , total bilirubin 15 uln , alanine aminotransferase and aspartate aminotransferase 3 uln [ or 5 uln in the presence of liver metastases ] )  . 
for cohorts c and d , patients were excluded if baseline glycated haemoglobin ( hba1c ) was 80% ( 64 mmol / mol ) or fasting plasma glucose was 70 mmol / l ( 126 mg / dl ) , or they had poorly controlled diabetes . 
patients were eligible for cohort entry with detection of a mutation at any allele fraction , and clonal dominance was not considered in eligibility . once enrolled into a cohort , treatment was given until disease progression , unacceptable toxicity , or pregnancy . 
laboratory assessments , adverse event recording , and vital signs were performed every 4 weeks at a minimu toxicity was assessed using national cancer institute common terminology criteria for adverse events version 4 . 
coding was done with use of the medical dictionary for regulatory activities version 22 . outcomes the primary endpoint for cohorts ad was confirmed objective response rate defined as a confirmed complete response or partial response according to recist criteria at any point during trial treatment . 
secondary endpoints included duration of response ( defined as time from the first documentation of complete response or partial response until date of disease progression or last date of follow - up ) , clinical benefit rate ( defined as complete response , partial response , or stable disease for more than 6 months during trial treatment ) , progression - free survival ( defined as time from cohort entry to first date of either confirmed progression of disease according to recist criteria or death from any cause ) , safety and tolerability of therapies , frequency of mutations , accuracy of ctdna testing by agreement between ctdna mutation status and tissue mutation status and the proportion of patients entering a cohort , and pharmacokinetics ( for cohorts a and b )  . 
prespecified exploratory endpoints included confirmed response rate in clonally dominant versus subclonal mutations in cohort a . statistical analysis all cohorts used a single - stage ahern design with 5% , to have 80% power . 
cohort a assumed an unacceptable response rate of 10% and a target response rate of 20% in the final design , requiring 13 or more responses from 78 evaluable patients to infer activity . 
this assumption was an approved amendment ( on may 1 , 2018 ) to the original two - stage design to account for the ctdna testing detecting subclonal mutations as well as clonal mutations where the response rate was expected to be lower ( appendix p 6 )  . 
cohorts b , c , and d each assumed an unacceptable response rate of 5% and a target response rate of 25% , requiring three or more responses from 16 evaluable patients . 
this number gave 85% probability of identifying 25 patients for a mutation with prevalence of 3% for each of cohorts b , c , and d individually , allowing for 36% attrition between ctdna screening and cohort entry . objective response rate , duration of response , and clinical benefit rate were measured in an evaluable population defined as those patients with measurable disease per recist at baseline and at least one on - treatment assessment ; patients who stopped treatment because of intolerable toxicity or death without having a scan after baseline were evaluable and recorded as non - responders . 
proportions and two - sided 95% cis for estimation purposes were reported for each cohort and in prespecified subgroup analyses ( by clonally dominant versus subclonal mutations in cohort a , compared using a fishers exact test , by hormone receptor status in cohort b , and by akt1 or pten mutation in cohort d )  . 
analysis of clonality of her2 mutations in cohort b and of akt1 in cohort c was a post - hoc analysis . in post - hoc exploratory analyses , response rates for each cohort were reported by pik3ca and tp53 mutation status and , for cohort a , tissue mutation status . 
for inference purposes , thus corresponding to the design characteristics underpinning the trials hypothesis testing ( ie , alpha 5% , one - sided ) , proportions and two - sided 90% cis are reported . progression - free survival was measured in the intentionto - treat population . 
patients who were alive and progression free were censored at date of last follow - up ; patients who had non - recist confirmed progression ( eg , clinically judged progression or radiologically confirmed but lesions not measured according to recist ) were censored at the date progression was reported . 
the safety population included all patients who had at least one dose of treatment , regardless of their eligibility , and treatment - emergent adverse events where more than 10% of patients reported any grade of the adverse event or any patients reported the adverse event at grade 3 or higher were presented . 
in addition , pharmacokinetics were reported as a percentage vol 21 october 2020 1299 articles change from an approved historical population pharmacokinetic model for standard - dosing 500 mg fulvestrant , in cohort a only . 
this study is registered with clinicaltrials.gov , nct03182634 ; the european clinical the trials database , eudract2015 - 003735 - 36 ; and isrctn registry , isrctn16945804 . role of the funding source the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
 the corresponding author had full access to all of the data and the final responsibility to submit for publication . results between dec 21 , 2016 , and april 26 , 2019 , 1051 patients were registered into the study ( 1044 via ctdna screening , seven via previous tumour sequencing ; figure 1 ; appendix p 17 ) with ctdna results available for 1034 patients ( 990% )  . 
digital pcr results were available for 1025 patients ( 982% ) and targeted sequencing results were available for 800 patients ( 766% ; 364 prospective and 436 retrospective )  . 
patients had a median of one ( iqr 02 ) previous lines of chemotherapy , and a median of two ( 13 ) previous lines of systemic therapy ( table )  . a somatic mutation was detected in 743 ( 93% ) of 800 patients with ctdna targeted sequencing results ( appendix p 18 )  . 
esr1 mutations were found almost exclusively in hormone receptor - positive breast cancer , were found at lower average allele fractions than other mutations , and were frequently polyclonal ( appendix pp 1718 )  . 
her2 mutations were found least frequently in triple - negative breast cancer , while akt1 mutations were found at a similar frequency in hormone receptorpositive her2 - negative breast cancer and triple - negative breast cancer ( appendix p 18 )  . gene - level agreement identification between ctdna digital pcr and targeted sequencing ( n = 800 ) was 9699% ( kappa 089093 ; figure 1 )  . 
 for mutation sensitivity ( or percent - positive agreement reflecting the absence of gold standard ) for digital pcr was 93% ( 95% ci 8398 ) overall and 98% ( 87100 ) in patients with contemporaneous biopsies ( appendix pp 17 , 20 )  . 
 specificity for both digital pcr and sequencing ( or percent - negative agreement reflecting the absence of gold standard ) was high for akt1 , her2 , and pik3ca , varying by gene ( appendix p 17 )  . 
esr1 mutations had lower percent - negative agreement . identified mutations were in 533 for ctdna ( 511% ) of 1044 patients registered testing and 357 ( 345% ) of 1034 with results had targetable mutations eligible for cohort entry , of whom 136 entered one of the five available cohorts . 
the most common reason for not entering a cohort was that the patient was ineligible based on the specific eligibility criteria for the relevant cohort , or in the case of cohort a ( esr1 mutation ) , 64 patients did not enter because of cohort a being suspended ( while the protocol amendment to change the design was ongoing ) or closed ( figure 1 ; appendix p 7 )  . 84 ( 38% ) of 222 patients with an esr1 mutation in ctdna identified while cohort a was open to recruitment were enrolled in cohort a ( figure 1 , table )  . 
the most common esr1 mutations detected in plasma were asp538gly ( 45 [ 54% ] of 84 ) , tyr537ser ( 31 [ 37% ] ) , and glu380gln ( 29 [ 35% ] )  . 
 six ( 8% [ 95% ci 317 ] ) of 74 patients had a confirmed partial response with a median duration of response of 70 months ( iqr 3783 ) and four patients continuing on treatment at data cutoff ( figure 2 )  . 
in a pre - planned exploratory analysis , five ( 12% [ 95% ci 426 ] ) of 41 patients with clonally dominant esr1 mutations , and none ( 0% [ 013 ] ) of 27 patients with subclonal mutations had a confirmed response ( p = 015 ; 27 [ 40% ] of 68 esr1 mutations were subclonal ) ; six patients had unknown clonality . 
the main reason for treatment increased 1300 vol 21 october 2020 articles 1051 met inclusion criteria and registered for plasmamatch 7 registered to cohort d with previous tumour tissue sequencing 10 results not available ( test failed or not done ) 501 with no mutation or amplication identied 176 not eligible for cohort 148 pik3ca mutation 20 her2 amplication 8 pik3ca mutation and her2 amplication 221 did not enter a cohort 67 ineligible 22 patient choice 40 clinician decision 64 cohort a suspended or closed 6 other cohort closed ( deadline passed for cohort entry ) 8 died before cohort entry 14 unknown 1044 registered for ctdna testing 1034 ctdna testing results available * 1025 digital pcr 364 targeted sequencing 533 with mutation or amplication identied 357 with targetable mutation ( s ) identied 136 entered a cohort via ctdna testing 18 entered cohort c ( akt1 mutation and oestrogen receptor - positive breast cancer ) 18 initiated treatment 18 were evaluable for response 84 entered cohort a ( esr1 mutation ) 21 entered cohort b ( her2 mutation ) 80 initiated treatment 74 were evaluable for response 20 initiated treatment 20 were evaluable for response 1 entered cohort e ; to be reported at a later date ( triplenegative breast cancer with no mutation ) 19 entered cohort d ( akt basket ; akt1 mutation with oestrogen breast cancer , or pten mutation ) receptor - negative 19 initiated treatment 19 were evaluable for response figure 1 : trial profile further detail on accuracy of ctdna testing is provided in the appendix ( p 17 )  . 
 * 436 additional samples were analysed by targeted sequencing retrospectively ; these were not used for determining cohort suitability ; agreement between digital pcr and targeted sequencing ( n = 800 ) was as follows : akt1 kappa 093 ( 95% ci 087099 ) , her2 kappa 0.89 ( 079098 ) , esr1 kappa 090 ( 086093 ) , and pik3ca kappa 092 ( 089095 )  . vol 21 october 2020 1301 articles discontinuation was disease progression ( 72 [ 95% ] of 76 patients ; appendix p 8 )  . 
fulvestrant activity was similar in patients with and without esr1 mutations in tissue sequencing ( appendix p 29 )  . 21 ( 58% ) of 36 patients with an her2 mutation in ctdna were enrolled in cohort b ( figure 1 , table )  . 
the ( ten most common her2 mutations detected in plasma were [ 48% ] of 21 patients ) , val777leu leu755ser ( four [ 19% ] ) , and ser310phe ( three [ 14% ] )  . 
five ( 25% [ 95% ci 949 ) of 20 patients had a confirmed response ( one complete and four partial ) , and an additional three patients had unconfirmed partial responses ( figure 3 )  . 
for patients with oestrogen receptor - negative breast cancer and akt1 mutation or pten mutation the denominator is patients with hr - positive disease only ( for those who entered cohort d n = 13 ; for those that did not enter cohort d n = 11 )  . 
||patients may be included in more than one type of systemic therapy , but patients are only included once in each category ( eg , if a patient had trastuzumab and pertuzumab they are counted once in the anti - her2 therapy category )  . 
in the subgroup of patients with hormone receptor - positive her2 - negative breast cancer treated with neratinib and fulvestrant , four ( 24% [ 95% ci 750 ] ) of 17 patients had a confirmed response ( figure 3 )  . 
the most common grade 3 or grade 4 adverse events were diarrhoea ( four [ 20% ] of 20 patients ) and hypertension ( three [ 15% ] ; appendix p 11 )  . 
ctdna = circulating tumour dna . previous fulvestrant therapy no previous fulvestrant therapy neratinib plus fulvestrant neratinib hr positive , her2 negative hr negative , her2 negative hr negative , her2 positive insertion ser310phe val777leu leu755ser val697leu figure 3 : neratinib in her2 - mutant breast cancer ( cohort b ) waterfall plot of maximum change in tumour size in individual patients with her2 mutations in ctdna treated with neratinib alone or neratinib plus fulvestrant . 
ctdna = circulating tumour dna . patients 18 ( 60% ) of 30 patients with an akt1 mutation in ctdna and oestrogen receptor - positive cancer were enrolled in cohort c ( figure 1 ; table )  . 
all 18 patients were evaluable ; four ( 22% [ 95% ci 648 ] ) patients had a confirmed partial response , and an additional four patients had unconfirmed partial responses ( figure 4a )  . 
in a post - hoc analysis , four ( 23% ) of 17 akt1 mutations ( clonality was assessable in 17 patients ) were subclonal ( appendix p 24 )  . 
the median relative dose intensity was 88% ( iqr 7099 , range 25101 ) for capivasertib and 99% ( iqr 97100 , range 94102 ) for fulvestrant . 19 patients were enrolled in cohort d , 12 following ctdna testing and seven following tumour testing ( figure 1 , table 1 )  . 
 the most common grade 3 or grade 4 adverse events were rash ( five [ 26% ] of 19 patients ) , hypertension ( two [ 11% ] ) , aminotransferase increase ( two [ 11% ] ) , gamma - glutamyltransferase increase ( two [ 11% ] ) , and vomiting ( two [ 11% ] ; appendix p 15 )  . 
 the median relative dose intensity of capivasertib was 94% ( iqr 63100 , range 42102 )  . 1304 vol 21 october 2020 articles previous fulvestrant therapy no previous fulvestrant therapy 100 100 in post - hoc analyses , the response rates in cohorts ad did not vary by pik3ca or tp53 co - mutational status ( appendix pp 2728 )  . discussion in this large , prospective trial of ctdna testing in advanced breast cancer , we found that ctdna testing was highly accurate , with high agreement between different ctdna testing techniques , and high sensitivity for mutations identified in advanced breast cancer tissue biopsies . 
ctdna testing identified patients with rare targetable mutations and these patients were recruited into cohorts that were given targeted therapies ( matched to mutations ) without confirmatory tumour testing , with activity comparable to previous studies involving tumour tissue testing.4 , 5 we enrolled more than 1000 patients across the uk in less than 3 years , and the dynamic trial platform design allowed for the simultaneous evaluation of multiple targeted treatment options . the availability and accuracy of ctdna testing shown in this study compares favourably with tissue - based mutation testing . 
nearly all patients ( 99% ) received a result from ctdna tumour testing , contrasting with previous sequencing studies where results were typically received in only 7090% of patients.15 , 16 in addition , previous tumour sequencing studies generally only included patients with disease that could be biopsied , which is not a constraint for ctdna testing . 
results were received relatively quickly after blood draw , compared with results for tissue - based testing , and this led to a high conversion rate of patients with ctdna mutations into the corresponding treatment cohort . 
the accuracy of ctdna testing was also similar to that achieved with tissue sequencing.17 discordance between ctdna results was still observed for patients at low allele frequency mutations , suggesting further potential for assay development . 
esr1 mutations had lower percent - negative agreement , probably reflecting the subclonality of acquired esr1 mutations , with ctdna detecting mutations present in metastasic sites other than the one biopsied . 
533 ( 511% ) of 1044 patients who underwent ctdna testing had a potentially targetable mutation ( pik3ca , esr1 , her2 , akt1 , or pten ) , indicating a potential value for ctdna testing . testing could replace akt1 leu52arg akt1 glu17lys entered trial on the basis of ctdna testing entered trial on the basis of tissue sequencing hr positive , her2 negative hr negative , her2 negative akt1 glu17lys akt1 leu52arg pten single nucleotide variant pten truncating pten deletion patients figure 4 : capivasertib in akt1 - mutant and pten - mutant breast cancer ( cohorts c and d ) ( a ) waterfall plot of maximum change in tumour size in individual patients with hr - positive cancer and akt1 mutations in ctdna , treated with capivasertib plus fulvestrant ( cohort c )  . 
 ( b ) waterfall plot of maximum change in tumour size in individual patients with akt1 mutations and hr - negative breast cancer , or with activating pten mutations , treated with capivasertib ( cohort d )  . 
in a previous phase 1 study with an expansion cohort of those with her2 - mutant breast cancer identified in tissue , who were given neratinib , there was a 32% unconfirmed response rate after 8 weeks of treatment.4 in our study , neratinib for her2 - mutant breast cancer identified by ctdna testing had comparable activity to that observed when guided by tissue testing , with durable responses . 
similarly , capivasertib had high activity in patients with ctdna - identified akt1 mutations , vol 21 october 2020 1305 articles both in hormone receptor - positive cancer with fulvestrant and in hormone receptor - negative cancer as a single agent , again con firming the results of a previous phase 1 study.5 these results confirm the high activity of these drugs against her2 and akt1 mutations , and strongly support the need for registration trials , facilitated by a ctdna testing programme . our study did not show benefit from increasing the dose of fulvestrant in patients with esr1 mutations in ctdna . 
previous research has suggested that fulvestrant at standard doses does not maximally inhibit or degrade mutated esr1 , 18 and we assessed whether more frequent administration of fulvestrant would increase therapeutic utility . 
although exposure was increased in later cycles , this was insufficient to enhance activity , with the response rate remaining similar to that previously reported.19 , 20 we note however that our study recruited a heavily pretreated population , and this might have reduced the activity of fulvestrant . 
more potent oestrogen receptor inhibitors , such as novel oral oestrogen receptor degraders and modulators , are also likely to be required.21 we found that patients with tyr537ser esr1 mutations were no less sensitive to fulvestrant than those with other that esr1 mutations were esr1 mutations , and frequently subclonal , with detection of esr1 mutations in ctdna that were not present in contemporaneous single site tissue biopsies , reflecting the limited sampling of single site tissue biopsies . 
inclusion of relatively heavily pretreated patients might reduce activity of the targeted drugs , especially in cohort a , and future ctdna selection trials might benefit from more restrictive entry criteria . 
 the study was designed to assess the activity of therapies against specific genomic events , but it did not target pik3ca mutations , 1 and as a result relatively few of the patients registered to the trial had a response to therapy ( 17 [ 16% ] of 1051 patients )  . 
although we identified low activity of capi vasertib in pten - mutant cancers when used as a single agent , akt inhibition in combination with paclitaxel chemotherapy might be efficacious in ptenmutant cancers.22 , 23 capivasertib plus fulvestrant might be efficacious in endocrine - resistant oestrogen receptorpositive breast cancer without mutation selection , as shown in the faktion trial.24 it is not possible to robustly compare plasmamatch with faktion , as patients enrolled in plasmamatch had more previous lines of treatment , and akt1 mutations were not assessed and would be few in number in faktion.24 in conclusion , we show that ctdna testing , with the assays employed in this study , has sufficient accuracy for widespread adoption in routine clinical practice to identify patients with breast cancer who are suitable for licensed targeted therapies , such as pik3ca - mutant breast cancer , with the transformative potential of efficient and rapid screening for clinical trials . 
a high proportion of patients with specific targeted mutations were able to enrol on the matching treatment cohort , with clinically important activity observed with therapies matched to akt1 and her2 mutations . 
with mutationmatching therapy now approved in breast cancer , with alpelisib for pik3ca - mutant disease , ctdna testing can be seen as a standard - of - care test for both common and rare targetable genetic events . contributors nct is the chief investigator , and ar is the coordinating investigator for the trial . 
jmb is the trials methodology lead within the institute of cancer research clinical trials and statistics unit ( icr - ctsu ) and provided oversight and guidance for trial management , statistics , and data interpretation throughout the trial . 
 amw , irm , rdb , rr , and ar are all cohort clinical leads responsible for the clinical oversight and safety review and evaluation for a defined treatment cohort within the trial . 
amw , irm , rdb , rr , ps , oo , jpb , mt , mcw , dr , dc , as , mh , and kr are members of the plasmamatch trial management group , which contributed to study design , was responsible for oversight throughout the trial , and contributed to data interpretation and manuscript preparation . 
ps , oo , jpb , mt , ja , mcw , and dc were involved in recruitment and treatment of participants and contributed to data collection and manuscript preparation . 
 all authors reviewed and approved the manuscript . declaration of interests nct , ar , jmb , lsk , cs , lm , sk , kw , sm , hb , mh , bk , and rc report grants from cancer research uk , grants and non - financial support in the form of study drug provision from astrazeneca and puma biotechnology , non - financial support in the form of ctdna sequencing from guardant health , and provision of reagents from biorad , during the conduct of the study . 
nct also reports grants and personal fees from astrazeneca , pfizer , and roche genentech , personal fees from bristolmyers squibb , lilly , merck sharpe & dohme , novartis , bicycle therapeutics , taiho pharmaceutical , zeno pharmaceuticals , and repare therapeutics , and grants from biorad , clovis , merck sharpe and dohme , and guardant health , outside the submitted work . 
 amw reports personal fees from roche , personal fees and other support from novartis , pfizer , lilly , daiichi sankyo , merck sharpe & dohme , astrazeneca , and athenex , and other support from seattle genetics , andrew wardley , and manchester cancer academy and outreach research and innovation group , outside the submitted work . 
irm reports personal fees and non - financial support from roche , eli lilly , and eisai , and personal fees from novartis , pfizer , daiichi sankyo , genomic health , pierre fabre , and merck sharpe & dohme , outside the submitted work . 
rr reports personal fees from novartis , eli lilly , and pfizer , personal fees and non - financial support 1306 vol 21 october 2020 articles from daiichi sankyo and g1 therapeutics , and non - financial support from roche and astrazeneca , outside the submitted work . 
oo reports grants and personal fees from pfizer and eisai , personal fees from roche genentech and tesaro , non - financial support from astrazeneca , personal fees and non - financial support from eli lilly , and grants from novartis , outside the submitted work . 
 mt reports personal fees from pfizer , novartis , roche , vaccitech , oxford vacmedix , lilly , astellas , genomic health , and eisai , personal fees and non - financial support from janssen , bristol - myers squibb , and ipsen , and non - financial support from eusa pharma , outside the submitted work . 
mcw reports personal fees and non - financial support from eisai , lilly , and roche , and personal fees from pfizer , genomic health , and novartis , outside the submitted work . 
dr reports personal fees from novartis , pfizer , roche , daiichi sankyo , lily , and genomic health , non - financial support from daiichi sankyo and eisai , and grants from celgene , roche , biotheranostics , and rna diagnostics , outside the submitted work . 
 dc reports other support from novartis , astrazeneca , pfizer , roche , eli lilly , puma biotechnology , daiichi sankyo , synthon , seagen , zymeworks , elsevier , european cancer organisation , celgene , succint medical communications , prima biomed , oncolytics biotech , celldex therapeutics , san antonio breast cancer consortium , highfield communication , samsung bioepis , prime oncology , merck sharp & dohme , rti health solutions , and eisai , and grants from cancer research uk , chief scientist office , breast cancer institute , pfs genomics , and national institute for health research health technology assessment , outside the submitted work . 
as reports grants from ventana roche , and genomic heath , personal fees from daiichi sankyo , hologic , genomic health , and ventana roche , outside the submitted work . 
jmb also reports grants and non - financial support from astrazeneca , novartis , janssen cilag , merck sharpe & dohme , pfizer , roche , and clovis oncology , and grants from medivation , outside the submitted work . 
 all other authors declare no competing interests . data sharing de - identified individual participant data , together with a data dictionary defining each field in the dataset , will be made available to other researchers on request , subject to approval of a formal data access request in accordance with the icr - ctsu data and sample access policy . 
trial data are collected , managed , stored , shared , and archived according to icr - ctsu standard operating procedures to ensure the enduring quality , integrity , and utility of the data . 
data recipients are required to enter a formal data sharing agreement , which describes the conditions for data release and requirements for data transfer , storage , archiving , publication , and intellectual property . 
data sharing is undertaken if proposed projects have a sound scientific or patient benefit rationale , as agreed by the trial management group and approved by the trial steering committee , as required . 
additional documents may be shared if approved by the trial management group and trial steering committeeeg , statistical analysis plan and informed consent form . acknowledgments plasmamatch is funded by cancer research uk ( cruk / 15 / 010 , c30746 / a19505 ) with additional support from astrazeneca , puma biotechnology , guardant health , and biorad . 
thanks also to staff at participating centres , the icr - ctsu trial team , the staff at central laboratories , and syed haider and his team in the breast cancer now toby robins research centre bioinformatics core facility for bioinformatics support . 
 plasmamatch is supported by the national institute for health research ( nihr ) manchester clinical research facility at the christie hospital , manchester , uk , and by the cancer research uk cambridge centre , the cambridge nihr biomedical research centre , and the cambridge experimental cancer medicine centre , cambridge , uk . 
 plasmamatch is supported at participating sites in england by the nihr clinical research network , in scotland by the chief scientist office , and in wales by health and care research wales . 
this study represents independent research supported by the nihr biomedical research centre at the royal marsden national health service foundation trust and the institute of cancer research , london , uk . 
the authors also acknowledge past and present colleagues on the plasmamatch trial management group , the independent data monitoring committee , and the trial steering committee , who provided oversight of the trial ( appendix p 3 )  . corrections correction to lancet oncol 2016 ; 17 : 738 correction to lancet oncol 2016 ; 17 : e310 correction to lancet oncol 2016 ; 17 : 1203 , 06 , 08 , 09 , 11 published online august 31 , 2016 s1470 - 2045 ( 16 ) 30438 - 7 wallington m , saxon eb , bomb m , et al . 
 also , in the patients with nsclc column in table 1 of this article , and in the 30 - day mortality columns in tables 2 , 3 , 5 and 7 of this article , some percentages were incorrect . 
dual - targeted therapy with trastuzumab and lapatinib in treatment - refractory , kras codon 12 / 13 wild - type , her2 - positive metastatic colorectal cancer ( heracles ) : a proof - ofconcept , multicentre , open - label , phase 2 trial . 
lancet oncol 2016 ; 17 : the declaration of interests section of this review , the declaration for rk should have included and has received lecture fees from japan vaccine co ltd and msd for lectures on the safety and e ectiveness of the hpv vaccine . 
 folfiri plus cetuximab versus folfiri plus bevacizumab for metastatic colorectal cancer ( fire - 3 ) : a post - hoc analysis of tumour dynamics in the final ras wild - type subgroup of this randomised open - label phase 3 trial . 
this correction has been made to the online version as of sept 1 , 2016 , and the printed version is correct . correction to lancet oncol 2016 ; 17 : e423 burki tk . 
this correction has been made to the online version as of oct 4 , 2016 . vol 17 october 2016 e420 published online july 30 , 2020 s1470 - 2045 ( 20 ) 30421 - 6 for the study reporting the new finger - stick test see sci transl med 2020 ; published online july 15 . 
sciencemag.org / content / 12 / 552 / eaaw5831.full for more on the links between the fukushima disaster and thyroid cancer see sci rep 2020 ; 10 : 4074 for more on the release of plutonium from fukushima see sciencedirect 2020 ; published online july 8 . 
sciencedirect.com / science / article / pii / s0048969720340614 ? via%3 dihub potential new method for rapid diagnosis of radiation sickness radiation sickness , or acute radiation syndrome , might now be identified within hours of radiation exposure using a new finger - stick blood test developed by researchers . 
this condition occurs as a consequence of nuclear radiation or radioactive fallouts due to a nuclear weapon detonation or reactor accidents and can affect several sensitive organs within the body . 
 in an attempt to create the first - inhuman approved biodosimetry assay for the estimation of absorbed ionising radiation dose , marshleen yadav and colleagues at the ohio state university ( columbus , oh , usa ) identified a pair of microrna molecules in the blood that can be used to determine the degree of radiation exposure and assess whether or not toxicity has occurred . 
 identified one biomarker , they microrna - 150 , which is highly expressed in blood cells and is sensitive to radiation ( its concentration in the bloodstream decrease as radiation exposure increases ) and another , microrna - 23a , which is abundant in the bloodstream but remains unchanged upon radiation exposure . 
 this breakthrough diagnostic method offers a promising alternative to the standard dicentric chromosome assay , which looks for signs of dna damage caused by radiation and can take several days to produce results . 
 because individuals who have been exposed to toxic amounts of radiation require urgent and aggressive treatment , and because the period immediately after exposure is the most important in terms of the identification and triaging of patients , this accelerated diagnosis from a few days to only a few hours has the potential to substantially improve individual prognosis and save lives . 
 in addition to the benefits of reducing this diagnostic timeframe on an individual basis , the ease and scalability of the new finger - stick test makes it an opportune tool for screening large numbers of people within a short period of time . 
this feature is particularly useful when considering major nuclear disasters , such as chernobyl and fukushima , in which entire populations might be affected and require immediate testing to assess the severity of their radiation exposure . 
persistent links between the meltdown of the fukushima daiichi nuclear power plant in 2011 and the increased incidence of thyroid cancer in children and young adults in the region , detected through a large - scale mass ultrasound thyroid screening programme put in place after the disaster , indicate the value of mass screening and monitoring for those overexposed to radiation . 
moreover , a study published in july , 2020 , showed that the fukushima disaster released not only radioactive cesium but also particles of plutonium into the atmosphere underlines the invisible dangers such incidents continue to pose to public health several years after the event . 
 the potential scalability of the finger - stick test is also a very important consideration in clinical oncology settings , in which large numbers of patients stand to benefit from precise , accelerated screening for radiation exposure . beyond its utility in preparedness for a nuclear disaster , the assay has potential applications in radiation oncology and bone marrow transplant clinics , study author naduparambil k jacob explained . 
 molecular assays like this will likely help in modifying the regimen during the fractionated radiation based on individuals physiological response . irradiated human we have shown dose response leukaemia patients during marrow ablation and reconstitution after bone marrow transplant and we have done baseline comparisons in healthy humans , he continued . 
however , additional pivotal validation studies following fda - 2 animal rule using non - human primates as a model is needed for potential regulatory approval . whatever the application , the speed and convenience of this new diagnostic tool is essential to its future uptake , as norman coleman ( national cancer institute , bethesda , md , usa ) observed : the importance of a rapid diagnostic tool has been demonstrated in the covid - 19 management , such that a persons medical needs can be determined rapidly and they can be directed to either required treatment or to appropriate reassurance . 
for a resource - limited situation when there is more need than resources for everyone , the benefit to knowing who does not require treatment allows the available resources to be utilized most effectively and for someone who does not require a treatment to avoid it and the potential toxicity . importantly , these assays are biomarkers that estimate some degree of damage to a person or an organ system , added coleman . 
a blood test does not progress to a treatment without a professional making the determination . elizabeth gourd 1142 vol 21 september 2020 news articles lancet oncol 2016 ; 17 : 120316 this online publication has been corrected . 
the systemic anti - cancer therapy ( sact ) dataset collated by public health england allows the assessment of factors a ecting 30 - day mortality in a national patient population . 
the aim of this rst study based on the sact dataset was to establish national 30 - day mortality benchmarks for breast and lung cancer patients receiving sact in england , and to start to identify where patient care could be improved . methods in this population - based study , we included all women with breast cancer and all men and women with lung cancer residing in england , who were 24 years or older and who started a cycle of sact in 2014 irrespective of the number of previous treatment cycles or programmes , and irrespective of their position within the disease trajectory . 
we did logistic regression analyses , adjusting for relevant factors , to examine whether patient , tumour , or treatment - related factors were associated with the risk of 30 - day mortality . 
for each cancer type and intent , we calculated 30 - day mortality rates and patient volume at the hospital trust level , and contrasted these in a funnel plot . findings between jan 1 , and dec , 31 , 2014 , we included 23 228 patients with breast cancer and 9634 patients with non - small cell lung cancer ( nsclc ) in our regression and trust - level analyses . 
30 - day mortality increased with age for both patients with breast cancer and patients with nsclc treated with curative intent , and decreased with age for patients receiving palliative sact ( breast curative : odds ratio [ or ] 1085 , 99% ci 10401132 ; p < 00001 ; nsclc curative : 1045 , 10131079 ; p = 000033 ; breast palliative : 0987 , 09770996 ; p = 000034 ; nsclc palliative : 0987 , 09760998 ; p = 00015 )  . 
30 - day mortality was also signi cantly higher for patients receiving their rst reported curative or palliative sact versus those who received sact previously ( breast palliative : or 2326 99% ci 16343312 ; p < 00001 ; nsclc curative : 3371 , 15547316 ; p < 00001 ; nsclc palliative : 2667 , 21093373 ; p < 00001 ) , and for patients with worse general wellbeing ( performance status 24 ) versus those who were generally well ( breast curative : 6057 , 133327513 ; p = 00021 ; breast palliative : 6241 , 41809319 ; p < 00001 ; nsclc palliative : 3384 , 22765032 ; p < 00001 )  . 
we identi ed trusts with mortality rates in excess of the 95% control limits ; this included seven for curative breast cancer , four for palliative breast cancer , ve for curative nsclc , and seven for palliative nsclc . interpretation our ndings show that several factors a ect the risk of early mortality of breast and lung cancer patients in england and that some groups are at a substantially increased risk of 30 - day mortality . 
furthermore , our results highlight the importance of collecting routine data beyond clinical trials to better understand the factors placing patients at higher risk of 30 - day mortality , and ultimately improve clinical decision making . 
they can also be given for palliative purposes , to improve the quality of life for patients with advanced incurable cancers for as long as possible by controlling cancer growth and providing vol 17 september 2016 1203 articles research in context evidence before this study we searched pubmed for articles published up to feb 29 , 2016 , reporting on 30 - day mortality after chemotherapy for breast and lung cancer . 
we also consulted leading clinicians in this specialty for relevant , recent published work . we identi ed four studies investigating the factors associated with high 30 - day mortality following anticancer treatment in patients with a range of cancers including breast and lung , and two recent clinical trials that reported on 30 - day mortality after treatment with current standard treatments for breast and lung cancer . the four studies identi ed were all regional rather than national , and the clinical trials were done in selected groups of patients ( restricted to certain age and performance status ranges or with limited comorbidities ) so the results do not necessarily apply to the national cancer patient population in england . 
we also identi ed previous published work that showed variation in 30 - day postoperative mortality between trusts using funnel plots . added value of this study this study reports on patient , tumour - related , and treatment - related factors associated with 30 - day mortality after systemic anticancer treatment . 
we studied the diverse populations of patients with breast and lung cancer in england throughout 2014 using data from the newly available systemic anti - cancer therapy ( sact ) dataset . 
to our knowledge , this is the rst time this topic has been investigated at a national level . implications of all the available evidence this study shows that the sact dataset provides insight into the factors a ecting early mortality of patients in england . 
 it suggests that treatment intent ( curative or palliative ) , age , performance status , whether patients had received sact before the qualifying treatment used for this study , and sex and stage ( lung cancer only ) all a ect the 30 - day mortality risk . 
for some patients , this approach might also increase survival time . patients dying within 30 days after beginning treatment with sact are unlikely to have gained the survival or palliative bene ts of the treatment , and in view of the side - e ects sometimes caused by sact , are more likely to have su ered harin particular , the risk of neutropenic sepsis ( infection resulting from low blood neutrophil count , probably the most important cause of sact - related death ) is highest in the 30 days after sact , peaking at around 1115 days after treatment.5 sact cycles are typically 21 or , less commonly , 28 days long , so death from neutropenic sepsis from the previous treatment is captured within the 30 - day mortality metric . 
simply reducing doses of or avoiding sact altogether would reduce or eliminate instances of treatment - related early mortality , but at the cost of some patients being denied e ective sact and hence the survival and palliation bene ts . to maximise the bene ts of sacts it is therefore important to gain a more detailed understanding of how the many di erent patient and tumour characteristics can predict patient outcomes , such as the risk of early mortality . 
only a small number of local observational studies have assessed 30 - day mortality after sact , but each has pointed to areas in which patient care could be improved.58 treatment - related early mortality is also commonly measured in clinical trials of sact , but , by necessity , patient cohorts are often selected on the basis of protocoldriven inclusion criteriaeg , within a certain age range , good performance status , or limited comorbidities.9 , 10 the ndings from these trials are therefore less reliable estimates of treatment - related early mortality in the groups not included from the general cancer patient population . 
 there is thus a clear need to make use of population - based data to establish 30 - day mortality benchmarks for the full range of patient types , to investigate how patient and treatment - related factors a ect the risk of 30 - day mortality , and to identify di erences between provider trusts to help improve clinical outcomes . here we examine factors that a ect the risk of 30 - day mortality in patients with breast and lung cancer in 2014 using data collected from nhs hospital trusts across england in the sact dataset . 
 we additionally characterised the extent of variation in 30 - day mortality rates between hospital trusts england , and identi ed those with signi cantly higher 30 - day mortality rates . 
this is the rst time , to our knowledge , that 30 - day mortality following recently reported sact has been investigated on a large scale in a population that re ects the real diversity of patients with breast and lung cancer being treated in the national health service ( nhs ) in england . 1204 vol 17 september 2016 articles see online for appendix methods study design and data this population - based , observational study11 included all breast and lung cancer patients aged 24 years and older reported to have received sact in england between jan 1 , and dec 31 , 2014 , according to the sact dataset , irrespective of the number of previous treatment cycles or programmes , and irrespective of their position within the disease trajectory . 
 the sact dataset is a new resource at public health england , which started a phased implementation in 2012 , and which collects information reported routinely by nhs hospital trusts about the treatment of cancer in england12 in four key areas : patient and tumour characteristics including age , sex , morphology , and performance status ; hospital and consultant details , including general medical council ( gmc ) number ; treatment characteristics including drug names and drug combinations ( regimens ) ; and outcome elds including date of most recent treatment and date of death ( when applicable )  . the appendix provides the full data standard , including a description of all 43 items recorded , with data eld formats as described in the nhs data dictionary13 ( appendix p 1 )  . 
these are primary patient and hospital trust identi ers ( nhs number , birth date , postcode , sact provider organisation code ) and key treatment details ( sact regimen name , regimen start date , and cycle number )  . phased introduction of data entry started in april , 2012 . 
by january , 2014 , 141 ( 95% ) of 148 trusts were routinely submitting at least the mandatory data items ; because of trust mergers , the total number of trusts expected reduced to 147 by july 2014 . 
we selected a reporting period of january to december , 2014 , because this was the most complete calendar year of data that was available at the time this analysis was completed.14 this reporting period also allowed linkage with the english national cancer registration and analysis service ( ncras ) , which improved data completeness when morphology , stage at diagnosis , and dates of death were missing from the sact dataset . treatment and patients we de ned sact as any cytotoxic chemotherapy , active anticancer therapies such as monoclonal antibodies ( eg , trastuzumab ) , and targeted biological treatments such as egfr tyrosine kinase inhibitors . 
 we did not distinguish between patients receiving combined chemo - radiotherapy and those receiving chemotherapy only , as this was poorly recorded in the sact dataset at this stage . we examined data for breast and lung cancer patients ( identi ed by the clinical codes in panel 1 ) because both had good data completeness in the sact dataset ; in 2014 , data had been submitted for 18 976 ( 94% ) of 20 265 patients with breast cancer and 13 405 ( 92% ) of 14 527 patients with lung cancer who were reported to have commenced chemotherapy.13 we provide descriptive statistics on small cell lung cancer ( sclc ) and non - small cell lung cancer ( nsclc ) separately , based on morphology data ( supplemented from cancer registry data where missing from the sact dataset ) because these cancer types generally require di erent treatment strategies . 
we excluded from our regression analysis all patients for whom the start date of their last reported cycle of sact was not reported because this precluded an assessment of 30 - day mortality . outcomes of the patients with breast or lung cancer reported to have received sact in england between jan 1 , 2014 , and dec 31 , 2014 , we identi ed those that died within 30 days of sact ( from all causes , including iatrogenic deaths or those due to disease progression ) by calculating the time between the start date of the most recently reported sact cycle in 2014 and , when relevant , the date of death for each patient . 
 from this , we calculated a national 30 - day mortality rate by dividing the number of patients that received sact within 30 days of their death by the total number of patients that received sact in the reporting period . 
we mainly used the date of death as reported for a patient through sact dataset returns , but when that was unavailable , we extracted it from records in the ncras . 
all patients were traced through the nhs demographics services using matched identi ers ( including nhs number , date of birth , and sex )  . there were 22 deaths for patients with breast cancer and 35 deaths for patients with lung cancer that were only recorded in ncras , not the sact dataset or the nhs demographics service . 
 608 patients with breast cancer and 732 patients with nsclc had con icting dates of death recorded in the sact versus ncras datasets ; this resulted in a con ict about 30 - day mortality status ( records agged as death within 30 days in one source but not the other ) for 16 patients with breast cancer and 20 with nsclc . for 26 patients who died within 30 days of receiving sact , death certi cate data could not be found . 
 one patient with lung cancer in the 30 - day mortality group had a di erent date of birth recorded in the cancer registry , so we used their date of birth recorded in the sact dataset . 
for all other patients , nhs number , date of birth , and sex were identical in both databases . some trusts reported a high proportion of patients as having received only the rst cycle of sact : 13 trusts that treated 574 patients with breast cancer , and 14 trusts that treated 302 patients with lung cancer , had a very high proportion ( > 80% ) of patients for whom only the rst cycle of sact was reported . 
 * these total numbers are patients treated with curative and palliative intents only , and do not include those for whom treatment intent was unknown . table 1 : patterns of missing values in the sact dataset for ps , stage , and bmi for all patients with breast or nsclc these patients might have had subsequent cycles of chemotherapy that were not recorded in the sact dataset . statistical analysis and explanatory variables we examined the association of age , performance status , income deprivation , whether patients had received previous sact ( as recorded in the sact dataset ) , and bmi with 30 - day mortality after sact for breast and nsclc patients . 
these variables are linked to patient care in a clinical setting in relation to sact treatment ; income deprivation , while not directly linked to patient care , re ects other factors that arefor example , those in low - income areas might be more likely to smoke and have higher levels of comorbidity . we also examined the association of sex and cancer stage at diagnosis with 30 - day mortality for nsclc patients only . 
we also did not examine the association of cancer stage at diagnosis with 30 - day mortality for breast cancer because there can be a substantial time interval between diagnosis and sact treatment for many breast cancer patients ( eg , patients who relapse with metastatic disease several years after the initial diagnosis ) , making this indicator less clinically relevant than for lung cancer . income deprivation was not reported directly by nhs hospital trusts in the sact dataset . 
instead , we used patient postcodes , as reported in the dataset , to derive each patients income deprivation score from the english indices of deprivation 2010 , 15 and assigned patients into ve groups from least ( group 1 ) to most ( group 5 ) income deprived . 
we chose income deprivation over health - related indices , which would have been interrelated with our 30 - day mortality outcome measure . the dataset this measure : there were missing values for performance status and bmi for patients with breast cancer or nsclc , and stage for nsclc ( table 1 )  . 
 inspection of the data showed that for performance status , this was mainly the result of a few trusts not reporting trusts reported no performance status data , one of which was a large trust , and 12 trusts had 10% or less completion of performance status data . 
we assumed data were missing completely at random ( mcar ) at the patient level because we found no evidence to the contrary , and these trusts provided care for a range of patients . four height and weight data ( used to calculate bmi ) are likely to be recorded for patients receiving less treatments with a xed dose ; however , many patients included in our study received treatments that were dosed according to body surface area or weight , some of whom also had missing height and weight data , which probably obscures this association between bmi and 1206 vol 17 september 2016 articles treatment regimen . 
additionally , some trusts with low patient volumes ( < 400 patients ) reported no height or weight data , giving some evidence for an association between bmi and treating trust , although this link is probably weak . data for stage at diagnosis were more complete : stage was reported for 10 408 ( 93% ) of 11 199 patients with lung cancer and 13 883 ( 89% ) of 15 626 patients with curative breast cancer , compared with 4159 ( 55% ) of 7602 patients with palliative breast cancer , suggesting that stage at diagnosis data were more likely to be reported when patients had a smaller time interval between diagnosis and last reported treatment . 
most patients with breast cancer receiving palliative treatment are likely to be stage iv ( the most advanced stage ) ; therefore , clinicians might be less likely to record stage at diagnosis for these patients because it is assumed to be stage iv . 
thus , there was evidence of an association between stage at diagnosis and treatment intent . because we assumed that performance status was mcar , and that bmi and stage seemed to be only weakly related to treatment regimen and intent , respectively , we hypothesised that there would be no variables upon which we could base multiple imputation . 
we tested this by attempting multiple imputation16 using the ice command in stata , based on variables of age , sex , intent of treatment , patients not having received any previous sact as recorded in the dataset from 201214 ( treatment naive ) , regimen , income deprivation group , cancer type ( breast or lung cancer ) , treating trust , and death within 30 days . we used a train - test approach to assess the accuracy of this imputed data , whereby from all known data , we used the multiple imputation algorithm to estimate 1% , 5% , 10% , and 20% of the data in multiple tests . 
these unknown categories were also used for risk adjustment in the funnel plot . regression analysis and risk - adjustment we used logistic regression analysis to assess any associations between the explanatory variables and 30 - day mortality . 
we present the results of these logistic regression analyses as adjusted odds ratios ( or ) that re ect the e ect of each variable in our multivariable regression model , alongside the unadjusted or and proportion of patients with 30 - day mortality . 
for each model , the mean variance in ation factor was lower than 104 , which suggests that there were no issues with co - linearity between model terms . we plotted the errors of the residuals in the model , which showed that the variables in our model were equally variable and indicated that the assumptions of our regression model were valid . 
 in addition to testing the main e ects presented here , we tested models with interactions modelled between age and performance status , age and bmi , and for nsclc only , sex and performance status , and sex and bmi . 
in each case , the model t was inferior . analyses were completed separately by cancer type ( breast or nsclc ) further separated by treatment intent ( curative or palliative ) in four regression analyses . 
in this rst analysis of the sact dataset , we did not do separate regression analyses for each mode of treatment we included as curative ( panel 2 ) , because this would have resulted in smaller group sizes and thus lower statistical power . we compared 30 - day mortality rates between the following groups for age , performance status , income deprivations , previous sact treatment , bmi , sex ( nsclc ) , and tumour stage at diagnosis ( nsclc )  . 
 for performance status , we recorded patients as ps 0 ( asymptomatic ) , ps 1 ( symptomatic , still able to carry out light activities ) , ps 24 ( symptomatic patients requiring any amount of bed rest during the day , or who were completely bed bound , grouped together because of small patient numbers ) , and performance status not recorded . 
for income deprivation , we compared patients panel 2 : typical de nitions of curative and palliative intent used in this study , as recorded by trusts in electronic prescribing systems curative modes of treatment 1 adjuvant : given after surgery to reduce the chance of the cancer spreading or coming back 2 neoadjuvant : given before surgery to shrink a tumour and make surgery possible or less dis guring 3 curative : given alone without other forms of treatment to try to cure the cancer completely palliative modes of treatment 1 palliative : given to maintain or improve the quality of life for patients with advanced incurable cancer for as long as possible , by controlling the growth of a cancer and providing symptom relief vol 17 september 2016 1207 articles patients receiving sact in 2014 29 112 women with breast cancer 15 545 patients with lung cancer 30 - day mortality patients dying within 30 days of most recently recorded cycle of sact in 2014 still alive > 30 days patients alive for 31 or more days after most recently recorded cycle of sact in 2014 700 women with breast cancer 1274 patients with lung cancer 867 patients with nsclc 27 664 patients with breast cancer 13 771 patients with lung cancer 10 332 patients with nsclc excluded patients for whom no sact cycle start date was present 748 patients with breast cancer 500 patients with lung cancer * figure 1 : study pro le for our analyses in this report nsclc = non - small cell lung cancer . 
 * the number of excluded patients with nsclc is not shown here , as the excluded patient group was not traced in the national cancer registration and analysis service for additional morphology data . breast , curative breast , palliative breast , not recorded total patients 30 - day mortality 15 626 / 28 364 ( 55% ) 41 ( < 1% ) 7602 / 28 364 ( 27% ) 5136 / 28 364 ( 18% ) breast , all intents combined 28 364 ( 100% ) lung ( all subtypes ) , curative lung ( all subtypes ) , palliative 2429 / 15 045 ( 16% ) 10 587 / 15 045 ( 70% ) lung ( all subtypes ) , not recorded 2029 / 15 045 ( 14% ) lung ( all subtypes ) , all intents combined 15 045 ( 100% ) data are n ( % ) of total patients by cancer type and treatment intent ; and n ( % ) of deaths occurring within 30 days of systemic anticancer therapy for each of those groups . 
sclc = small cell lung cancer . table 3 : 30 - day mortality rates in patients with lung cancer by morphology and treatment intent in income domain group 3 ( the middle level of socioeconomic deprivation based on household income ) with those in group 1 ( least deprived ) , 2 , 4 , and 5 ( most deprived )  . 
for previous sact treatment , we compared patients for whom one or more previous systemic anticancer treatments were recorded in the sact dataset before the qualifying treatment used in this study with patients for whom no previous systemic anticancer treatments were recorded in any year ( 201214 ) of the database ( treatment naive )  . 
for bmi , we compared patients with bmi scores in the healthy weight range ( bmi 185 to < 25 kg / m ) with those in the underweight range ( bmi < 185 kg / m ) , overweight ( bmi 25 to < 30 kg / m ) , and obese categories ( bmi > 30 kg / m ) , and those for whom bmi information was not recorded . 
the factors included in the risk adjustment were the same as those detailed for the logistic regression analyses ( eg , age , perfor mance status , bmi , and stage at diagnosis )  . as noted in the methods for multiple imputation , the large number of missing values for performance status were a result of a small number of trusts not providing any performance status information . 
we used the risk - adjusted mortality rate to create funnel plots using the funnelcompar command in stata , which gave the 95% and 998% control limits ( dashed lines on the graphs ) and the national risk - adjusted 30 - day mortality rate ( the horizontal line on each graph )  . role of the funding source there was no funding source for this study . 
the corresponding author had full access to all aggregated data and analyses and the nal responsibility to submit for publication . results of the patients in the sact database , 748 ( 3% ) of 29 112 patients with breast cancer and 500 ( 3% ) of 15 545 patients with lung cancer receiving sact were excluded from the analysis due to missing cycle start dates . 
treatment intent was not recorded for 5136 ( 18% ) of 28 364 patients with breast cancer and 2029 ( 14% ) of 15 045 patients with lung cancer ; these patients were excluded from the regression and trust - level analyses . 
because of lower patient numbers for sclc ( n = 3352 ) , we only did the regression and trust - level analyses for patients with nsclc ( 11 199 patients including those for whom treatment intent was not recorded )  . 
in view of the exclusions , the 1208 vol 17 september 2016 articles nal cohort for regression and trust - level analyses included 23 228 patients with breast cancer and 9634 patients with nsclc . the median patient age was 54 years ( iqr 4764 ) for patients with breast cancer treated with curative intent ; 61 years ( 5170 ) for patients with palliative breast cancer ; 67 years ( 6173 ) for patients with nsclc treated with curative intent ; and 68 years ( 6174 ) for patients with nsclc treated with palliative intent . 
the appendix shows the distribution of age , performance status , income deprivation , and bmi by age for patients with breast and nsclc treated with curative and palliative intent ( appendix pp 24 )  . data for performance status , a measure of patients level of cancer symptoms and general wellbeing , 20 was not reported for 6919 ( 30% ) of 23 228 patients with breast cancer and 2968 ( 31% ) of 9634 patients with nsclc , for whom treatment intent was recorded . 
a further 2139 ( 42% ) of 5136 patients with breast cancer and 530 ( 34% ) of 1565 patients with nsclc , were missing both performance status and treatment intent . overall , 30 - day mortality was higher for patients with lung cancer ( 1274 / 15 045 [ 9% ] ; table 2 ) than patients with breast cancer ( 700 / 28 364 [ 3% ] ; table 2 ) , and in each treatment intent category ( curative , palliative , and unknown ; table 2 )  . 
30 - day mortality was lowest for patients with breast or lung cancer receiving systemic anticancer therapy for curative rather than for palliative purposes : 41 / 15 626 ( < 1% ) versus 569 / 7602 ( 8% ) for breast cancer , and 70 / 2429 ( 3% ) versus 1061 / 10 587 ( 10% ) for lung cancer ( table 2 )  . 
for the remaining 105 ( 8% ) of patients , most death certi cates mentioned cancer . table 4 and the appendix ( p 4 ) show all results of the regression analysis for patients with breast cancer treated with curative intent . 
30 - day mortality was also higher for patients with ps 24 compared with those with ps 0 , though con dence intervals were large ( or 6057 , 99% ci 133327513 ; p = 00021 )  . table 5 and the appendix ( p 5 ) show results of the regression analysis for patients with breast cancer treated with palliative intent . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of breast cancer patients receiving curative sact who had 30 - day mortality . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of patients with breast cancer receiving palliative sact who had 30 - day mortality . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of patients with nsclc receiving curative sact who had 30 - day mortality . 
patients for whom performance status was not recorded also had a higher 30 - day mortality than those with ps 0 ( 2719 , 18883918 ; p < 00001 )  . 
 treatment - naive patients receiving palliative treatment had a signi cantly higher 30 - day mortality than those for whom previous sacts are recorded in the dataset between 2012 and 2014 ( or 2326 , 99% ci 16343312 ; p < 00001 )  . table 6 and the appendix ( p 6 ) show results of the regression analysis for patients with nsclc treated with curative intent . 
as with patients with breast cancer , 30 - day mortality signi cantly increased with age for patients with nsclc treated with curative intent ( or 1045 , 99% ci 10131079 ; p < 000033 )  . 
treatment - naive patients had signi cantly higher 30 - day mortality than those for whom previous systemic anticancer treatments were recorded in the dataset between 2012 and 2014 ( or 3371 , 99% ci 15547316 ; p = 000033 )  . table 7 and the appendix ( p 7 ) show results of the regression analysis for patients with nsclc treated with palliative intent . 
as for breast cancer patients , 30 - day mortality decreased with age for patients with nsclc treated with palliative intent ( or 0987 , 99% ci 09760998 ; p = 00015 )  . 
treatment - naive patients had signi cantly higher 30 - day mortality than those for whom previous sact was recorded in the dataset between 2012 and 2014 ( or 2667 , 99% ci 21093373 ; p < 00001 )  . 
30 - day mortality was also signi cantly higher for patients with stage iv ( advanced ) than stage iii tumours ( or 1438 , 95% ci 10991883 ; p = 000051 )  . figures 25 show risk - adjusted funnel plots for di erent modalities of treatment and cancer type , by hospital trust . 
this included seven trusts for breast curative , four for breast palliative , ve for nsclc curative , and seven for nsclc palliative . discussion in our population - based study of english breast and lung cancer patients , 30 - day mortality increased with age for both patients with breast cancer or nsclc receiving curative sact , and decreased with age for patients receiving palliative sact . 
patients with breast cancer or nsclc with worse general wellbeing ( indicated by higher ps scores ) had higher 30 - day mortality than those who were generally well ( ps 0 ) , and 30 - day mortality was also higher for treatment - naive patients than those who had any previously recorded cycles of sact between 2012 and 2014 . 
individual trust data will be discussed in a public health england report . to our knowledge , this is the rst time these benchmarks in 30 - day mortality after sact have been established on a national basis . 
the 2011 national cancer strategy for england proposed 30 - day mortality as a potential national clinical indicator of avoidable harm from sact21 and it has been used as a clinically relevant indicator for sact in previously published work.5 these benchmarks can provide a better understanding of the patient characteristics associated with increased 30 - day mortality and start improved clinical treatment decision making and identify those hospital trusts where clinical practice and data management should be reviewed . to support a particular strength of 30 - day mortality as an outcome measure is that it avoids issues with the details and coding of causes of death on death certi cates . 
 * for age , our analysis examined the e ect of each 1 - year increase on 30 - day mortality , so this is the total proportion of patients with nsclc receiving palliative sact who had 30 - day mortality . 
 table 7 : regression analysis results showing 30 - day mortality for patients with nsclc treated with palliative intent by age , ps , id , previous sact ( previously treated or treatment naive ) , bmi , sex , and cancer stage nearly all patients in our study , including those dying within 30 days of receiving sact . 
however , we know that patients who die within 30 days of receiving sact are very unlikely to receive any bene t from it irrespective of what their cause of death was . 
it is therefore not necessary to know whether death was caused by side - e ects from treatment , cancer progression , or any other causes to examine factors that increase the risk of experiencing net harm rather than net bene t from receiving sact . the large cohort of breast and lung cancer patients included in the sact dataset gives con dence that the associations we recorded between a number of variables and higher early mortality in england are real , despite some issues with data completeness , which we expect to improve in subsequent years of data collection . the large , signi cant increase in 30 - day mortality for treatment - naive patients suggests that particular care and an emphasis on the early reporting of toxic e ects should be undertaken in patients who are sact treatment naive . 
this approach is consistent with ndings of a previous study of the toxic e ects from lung cancer treatment.22 to our knowledge there are no previous studies of treatment - naive status in this context , so we are unable to identify the reasons behind the increased 30 - day mortality for these patients . there our identi cation of treatment - naive patients relied on treatment records taken from the sact dataset alone and there are two known data issues reducing the accuracy of this grouping . 
the database was only implemented in 2012 and made mandatory in april , 2014 , so data for previous sact treatments might be missing for some patients ( eg , those who received a previous issue will be most treatment before 2012 )  . 
 additionally , the challenge of some trusts only recording patients rst cycle of sact means we might be underestimating early mortality from sact and overestimating increased risk associated with the treatment - naive patients . 
as data completeness improves in subsequent years , a clearer understanding of the association between treatment - naive status and 30 - day mortality will be possible . is a 30 - day mortality increased with age for patients with breast cancer and nsclc treated with curative intent , figure 2 : funnel plot of variation in risk - adjusted 30 - day mortality in patients with breast cancer given systemic anticancer therapy with curative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . female male stage i stage ii stage iii stage iv vol 17 september 2016 1211 1000 1100 1200 number of patients receiving chemotherapy ( 2014 ) articles number of patients receiving chemotherapy ( 2014 ) figure 3 : funnel plot of variation in risk - adjusted 30 - day mortality in patients with breast cancer given systemic anticancer therapy with palliative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . the nding that 30 - day mortality increased with worsening performance status for patients with breast cancer or nsclc treated with palliative intent could be because patients with poorer general health are less able to tolerate the negative side - e ects of sact compared with healthier individuals , to an extent where the toxic e ects outweigh the bene cial e ects.5 these ndings suggest great care is required when advising chemotherapy in this patient group . we noted that 30 - day mortality was signi cantly higher for patients with breast cancer or nsclc receiving palliative sact for whom performance status was not recorded compared with those with ps 0 . 
this result might be because ps 0 is relatively easy to de ne , but it might be more di cult for clinicians to score the extent of reduced wellbeing . our nding that 30 - day mortality was lower in women with lung cancer than in men with lung cancer given palliative sact was expected . 
previous data suggest that women with lung cancer are generally diagnosed at an earlier age , with a more localised cancer , and have better survival.20 however , to our knowledge there have been no speci c investigations of early mortality in this context prior to our study , so we are unable at this stage to suggest why sex a ects 30 - day mortality risk in particular . 
 the increased 30 - day mortality for nsclc patients receiving palliative sact who had advanced cancers was also expected because these patients are typically less well ; although again , no previous studies have , to our knowledge , investigated the e ect of cancer stage on early mortality speci cally . the nding that overweight nsclc patients treated with palliative intent had a reduced 30 - day mortality compared with those in the healthy bmi group could be explained by dose - limitation practices . 
chemotherapy doses are calculated according to patient height and weight , but smaller doses than this are often given to patients with higher bmi.24 , 25 these practices might reduce short - term mortality in overweight patients . 
 however , long - term survival might be lower for these patients than those with a healthy bmi if the administered dose is not high enough to e ectively reduce tumour growth and spread . 
research into whether there are longer - term survival di erences between overweight and healthy weight patients could help to elucidate whether there is a problem with under - dosing for larger patients . 
 weight loss is an adverse prognostic factor in lung cancer26 and could explain this trend , though the di erence recorded was non - signi cant . the relative risk of overall mortality in obese and overweight patients with breast cancer is increased compared with healthy weight individuals , 27 which number of patients receiving chemotherapy ( 2014 ) figure 4 : funnel plot showing variation in risk - adjusted 30 - day mortality in patients with non - small cell lung cancer given systemic anticancer therapy with curative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . perhaps because older patients are generally more frail and less able to tolerate sact than are younger patients . 
 conversely , 30 - day mortality decreased with age for patients with breast cancer and nsclc treated with palliative intent , perhaps because older patients are less likely likely than younger patients to accept or be prescribed sact treatment that might extend their life in favour of other palliative care options to relieve pain or discomfort . 
alternatively younger patients might have more aggressive disease with a higher risk of noniatrogenic cancer mortality.23 1212 vol 17 september 2016 articles suggests that a high bmi itself does not generally confer a signi cant biological protective e ect against mortality . 
if the e ects we recorded are due to dose - limitation or patient weight loss , an association between bmi and 30 - day mortality will probably be noted for other cancer types in future reports on the sact dataset . for patients with nsclc treated palliatively with no recorded bmi , 30 - day mortality was signi cantly lower than for those with a healthy bmi , but this reduction in risk was smaller than for overweight and obese patients , suggesting the bmi unknown group is probably mainly a mix of healthy weight and overweight patients . 
as data completeness improves , we will better understand the distribution of bmi scores amongst patients receiving sact , and obtain improved estimates of 30 - day mortality for each bmi group . although we identi ed several factors a ecting 30 - day mortality risk , our population - based dataset included only patients that received sact , so we cannot con rm whether patients would have had better outcomes if they had not received sact . 
through more sophisticated links with audit data and other data sources in future , we intend to investigate treatment rates alongside mortality by trust , which would provide some information about outcomes for these patient groups . 
this cohort represents a large proportion of number of patients receiving chemotherapy ( 2014 ) figure 5 : funnel plot showing variation in risk - adjusted 30 - day mortality in patients with non - small cell lung cancer given systemic anticancer therapy with palliative intent , by hospital trust each circle represents a separate hospital trust ; blue and red circles represent outliers beyond the 95% and 998% con dence interval boundaries that are represented as grey lines . 
red line shows national risk - adjusted 30 - day mortality rate . patients with breast cancer with higher mortality than is typically reported in clinical trials : 26% of patients with breast cancer diagnosed in england in 2013 were older than 60 years , with incidence peaking between the ages of 65 and 69 years.29 this might be because clinical trials typically recruit a tter cohort of patients with a lower disease burden and better performance status than the overall patient population receiving treatment to clearly determine the e ects of the interventions under investigation , and to ensure older and less well patients are not put at risk . 
patients in trials also tend to receive more intensive support and follow up . therefore , our analysis highlights the value of investigating sact treatment outcomes on a national scale , and shows that ndings of clinical trials in selected age cohorts cannot readily be generalised to all patients . 
lung cancer often occurs in patients with signi cant smoking - related comorbidities , which are likely to increase the risk of 30 - day mortality , 6 although lack of available comorbidity data meant that we could not account for them in these analyses . 
future analyses will pool data for multiple years ( as it becomes available ) to provide su ciently large patient cohorts to examine the impact of patient and disease characteristics on 30 - day mortality from sclc . the we predicted higher 30 - day mortality for patients receiving palliative sact because these patients are not expected to recover from their cancer and the burden of vol 17 september 2016 1213 articles disease is generally high . 
however , it remains important to weigh up the important bene ts some patients receive from palliative treatment with emerging evidence suggesting that patients prescribed chemotherapy at the end of life overall experience a net reduction in their quality of life.30 , 31 patient choice is an important factor in these decisions ; previous ndings showed that patients with cancer were much more likely to accept intensive sact treatment with only a small chance of bene t compared with doctors and nurses.32 to help clinicians and patients to make treatment decisions that are most likely to produce the desired outcomes , we must understand the factors a ecting the balance between bene ts and harms of palliative sact , which we have started to investigate here . 
these factors should be a focus of discussions about treatment between patients and their clinicians to allow better informed decisions and improved outcomes . in future studies based on the sact dataset , we hope to examine di erences in the factors a ecting 30 - day mortality between subcategories of patients that received curative sact ( adjuvant , neoadjuvant , and curative ) , which we were unable to do in this initial analysis due to insu cient patient numbers in each sub - category . 
 this analysis will be possible once data on more patients become available in subsequent years . we also identi ed several trusts with signi cantly higher levels of 30 - day mortality . 
we have written to all trusts to inform them of their 30 - day mortality rates , and have speci cally encouraged outlier trusts to review both their clinical practice and also their data management systems . 
 analogously , simply because a hospital trust fell within the control limits of the funnel plots , it does not guarantee that each patient received optimal treatment , as data issues may be obscuring instances of suboptimal clinical decision making . 
it is also possible that hospitals with signi cantly lower 30 - day mortality rates are not tolerating any risk and are treating only the ttest patients , which may have the unintended consequence of not treating patients who could have potentially bene ted from receiving sact . 
more comprehensive case mix adjustment and better data completeness will , in time , allow national datasets such as the sact dataset to be used as a performance management tool . although we have made some important insights into 30 - day mortality using the sact dataset , some limitations and gaps in reporting still remathe sact dataset uses only routinely reported data with no clinical note or pro - forma review . 
therefore , the dataset does not include items such as laboratory indicator test resultseg , for liver and renal function , so we are unable to analyse any association between these indicators and 30 - day mortality , or use them in risk adjustment models . at this stage , we did not assess whether drug dosage was appropriate , and whether this was associated with 30 - day mortality because this was beyond the scope of our rst report . 
however , analyses of these data in future reports would be valuable , for example in assessing whether sact regimens are both clinically e ective and cost - e ective . 
subsequently , some of those patients probably received subsequent cycles that were not recorded in the dataset , whose absence from the sact dataset would arti cially increase the time between cycle start date and date of death , and lower 30 - day mortality . 
 this omission might also arti cially increase the risk of 30 - day mortality associated with being treatment naive , because later cycles of sact , and therefore any deaths within 30 days of those later cycles , were not recorded . 
 issues with missing data will be resolved through improvements in sact data reporting by trusts through e - prescribing systems in subsequent years . compared with the national cancer waiting times database , the sact dataset captured 94% and 92% of patients with breast and lung cancer , respectively , reported to have received sact in 2014.13 3% of both patients with breast cancer and with lung cancer receiving sact were also excluded from the analyses in this report due to missing cycle start dates . 
some of these missing data could be due to delayed or phased reporting because the dataset was only mandated from april , 2014 ( the proportion of trusts reporting on at least the mandatory data elds was 141 [ 95% ] of 148 in january , 2014 , but 147 [ 100% ] of 147 by july )  . some nhs trusts reported incorrect names for the combinations of sacts ( regimens ) given to some con rmed breast and lung cancer patients included in our analyses , which highlights the need for trusts to improve the quality of their regimen data reporting . 
this error could be because sact is recorded some time before its administration , and the record might not be updated if treatment is delayed or omitted , which is likely to falsely increase 30 - day mortality . we acknowledge that performance status might not have accurately re ected comorbidity status , which can be associated with socioeconomic deprivation ( eg , through a higher prevalence of smoking amongst more socioeconomically deprived patients ) , which might a ect whether these patients receive sact . 
therefore , improved data collection on comorbidity status would the association between enable us socioeconomic deprivation and 30 - day mortality more thoroughly in future . investigate for the rst time to our knowledge , our analysis of the for linkage and mortality sact dataset morphology , at diagnosis , the ncras ( with stage 1214 vol 17 september 2016 articles information ) gives us important insights into 30 - day mortality in a large , representative population of patients with breast or lung cancer receiving systemic anticancer therapy in england . 
our data suggest that treatment intent , patient age , performance status , whether patients had received previous systemic anticancer treatments , and sex all a ect 30 - day mortality risk in this context . 
some patients may not have bene ted from decisions to give sact ; accurate and complete reporting of sact data on a national scale is therefore crucial to provide real world information to support clinicians with decision making on treatment , complementing evidence from clinical trial data . contributors dd , mwa , mp , and sm led on study design and concept . 
dd , mwa , mp , sm as well as ebs , mb , rs , mwi , jr , dc , jd , dt , tp , and cw all actively and substantially contributed to the writing of this manuscript , performing literature searches , interpreting data and providing comment on multiple iterations of the manuscript . declaration of interests dd reports that public health england ( phe ) provided funding for the project team and are preparing a report on the subject of 30 - day mortality in england ( 2014 ) for publication . 
mp reports personal fees from roche pharmaceuticals ltd , personal fees from pierre fabre oncology ltd , personal fees from eli lilly , personal fees from astrazeneca , grants from msd , outside the submitted work . 
we thank the following colleagues for constructive comments and helpful discussions during the analysis of the data and drafting of this report : sara hiom ( cancer research uk ) , members from the chemotherapy clinical information and lung cancer site speci c clinical reference groups at phe , particularly michael lind , and eva morris ( university of leeds )  . 
 correction to lancet oncol 2016 ; 17 : 74756 correction to lancet oncol 2018 ; 19 : 153042 correction to lancet oncol 2019 ; 20 : 81626 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
lancet oncol 2016 ; 17 : 74756in results , median overall survival should have been median time of death ( after randomisation ) in eleven patients who died from progressive disease . 
prognostic value of end - of - induction pet response after first - line immunochemotherapy for ( gallium ) : follicular secondary analysis of a randomised , phase 3 trial . 
 lancet oncol 2019 ; 20 : 81626 the appendix of this article has been updated as of may 10 , 2019 . published online april 29 , 2019 s1470 - 2045 ( 19 ) 30280 - 3 published online may 10 , 2019 s1470 - 2045 ( 19 ) 30292 - x published online may 10 , 2019 s1470 - 2045 ( 19 ) 30293 - 1 correction to lancet oncol 2017 ; 18 : 106175 perl ae , altman jk , cortes j , et al . 
this correction has been made to the online version as of may 29 , 2019 . correction to lancet oncol 2019 ; 20 : 82736 shitara k , iwata h , takahashi s , et al . 
lancet oncol 2019 ; 20 : 82736the appendix of this article has been updated as of may 10 , 2019 . correction to lancet oncol 2019 ; 20 : 84961 eng c , kim tw , bendell j , et al . 
 atezolizumab with or without cobimetinib versus regorafenib previously treated metastatic colorectal cancer ( imblaze370 ) : a multicentre , open - label , phase 3 , randomised , controlled trial . 
this correction has been made to the online version as of may 29 , 2019 and the printed article is correct . correction to lancet oncol 2019 ; 20 : e26273 ngiam ky , khor iw . 
lancet oncol 2019 ; 20 : e26273tables 1 and 2 in this article have been corrected as of april 29 , 2019 . correction to lancet oncol 2019 ; 20 : 297310 cella d , grnwald v , escudier b , et al . 
this update has been made online as of may 29 , 2019 . vol 20 june 2019 e293 corrections nivolumab in children and young adults with relapsed or refractory solid tumours or lymphoma ( advl1412 ) : a multicentre , open - label , single - arm , phase 12 trial kara l davis , elizabeth fox , melinda s merchant , joel m reid , rachel a kudgus , xiaowei liu , charles g minard , stephan voss , stacey l berg , brenda j weigel , crystal l mackall summary background immune checkpoint inhibitors targeting pd - 1 have shown clinical benefit in adults with cancer , but data on these drugs in children are scarce . 
we did a phase 12 study of nivolumab , a pd - 1 blocking monoclonal antibody , to determine its safety , pharmacokinetics , and antitumour activity in children and young adults with recurrent or refractory non - cns solid tumours or lymphoma . methods we did a multicentre , open - label , single - arm , dose - confirmation and dose - expansion , phase 12 trial in 23 hospitals in the usa . 
eligible patients for part a ( dose - confirmation phase ) of the study were aged 118 years with solid tumours with measurable or evaluable disease ( by response evaluation criteria in solid tumors [ recist ] version 1.1 ) regardless of histology . 
eligible patients for part b ( dose - expansion phase ) were aged 130 years with measurable disease ( by recist criteria ) in the following disease cohorts : rhabdomyosarcoma , ewing sarcoma , osteosarcoma , neuroblastoma , hodgkin lymphoma , non - hodgkin lymphoma , and melanoma . 
patients in part a and were given nivolumab 3 mg / kg intravenously over 60 min on days 1 and 15 of a 28 - day cycle in a rolling 6 study design with de - escalation upon dose - limiting toxicities to establish the recommended phase 2 dose . 
the primary outcomes were the tolerability , systemic exposure , maximum tolerated dose , and the antitumour activity of nivolumab at the adult recommended dose in children and young adults . 
this trial is registered with clinicaltrials.gov , nct02304458 , with follow - up ongoing and is closed to new participants . findings 85 patients were enrolled between feb 22 , 2015 , and dec 31 , 2018 , and 75 patients were fully evaluable for toxicity . 
the most common overall toxicity was anaemia ( 35 [ 47% ] of 75 patients ; five patients had grade 3 or grade 4 ) and non - haematological toxicity was fatigue ( 28 [ 37% ] patients ; none had grade 3 or grade 4 )  . 
responses were observed in patients with lymphoma ( three [ 30% ] of ten with hodgkin lymphoma and one [ 10% ] of ten with non - hodgkin lymphoma ; all responders had pd - l1 expression )  . 
immune therapies have shown promising activity , including chimeric antigen receptor modified t cells68 and blinatumomab9 in relapsed or refractory paediatric b - cell precursor acute lymphoblastic leukaemia and dinutuximab in high - risk neuroblastoma , 10 as well as in combination with chemotherapy in recurrent and refractory neuro blastoma.11 immune checkpoint inhibitors block tumour - derived signals that inhibit immune responses , thus amplifying antitumour immunity . 
the search contained key terms checkpoint inhibitor , nivolumab , pd - l1 , pd - 1 , children , and pediatric with specific attention , but not exclusive , to phase 1 and phase 2 trials . 
our search highlighted the use of pd - 1 or pd - l1 blockers , including nivolumab , in a wide range of adult tumours , often with substantial clinical benefit . 
no phase 1 or phase 2 trials have been published that report on the safety or efficacy of pd - 1 targeting in sporadic paediatric cancers . added value of this study to our knowledge , our trial is the first to show safety and assess the antitumour activity of nivolumab in children and young adults with relapsed or refractory non - cns paediatric solid tumours or lymphoma . 
in the expanded phase 2 cohorts , no objective responses were observed except for patients with recurrent lymphoma . implications of all the available evidence nivolumab has similar immune adverse events and pharmacodynamic profiles in children as it does in adult patients . 
 used alone , nivolumab has preliminary activity for children and young adults with lymphoma and further study of this drug is warranted in this group , but the drug is not active in the sporadic paediatric solid tumour histotypes evaluated in this trial . have shown substantial benefit in several advanced cancers in adults12 and can induce tumour regression in children with solid tumours associated with germline mismatch repair deficiency.13 , 14 nivolumab , a humanised igg4 monoclonal pd - 1 blocking antibody , 15 administered once every 2 weeks ( 240 mg or approximately 3 mg / kg ) or once every 4 weeks ( 480 mg or approximately 6 mg / kg ) is approved by the us food and drug administration for adults and children ( aged > 12 years ) with microsatellite instability - high or mismatch repair deficient metastatic colon cancer and as second - line therapy in adults with advanced melanoma , renal cell carcinoma , urothelial carcinoma , hepatocellular carci noma , metastatic squamous cell non - small - cell lung cancer , head and neck cancer , small - cell lung cancer , and relapsed or progressed classical hodgkin lymphoma . 
we did a phase 12 trial of nivolumab in children and young adults with recurrent or refractory solid tumours , excluding cns tumours , or lymphoma , to characterise the toxicity and pharma cokinetics of nivolumab monotherapy in children , establish a recommended phase 2 dose , and evaluate clinical activity in common paediatric solid tumour and lymphoma cohorts . methods study design and participants we did a multicentre , open - label , single - arm , doseconfirmation and dose - expansion , phase 12 trial in 23 hospitals in the usa ( appendix p 10 )  . 
 eligible patients for part b ( dose - expansion phase ) were children and young adults aged 130 years with measurable disease ( by recist criteria ) in the following disease cohorts : rhabdomyo sarcoma , ewing sarcoma , infusion , or cellular osteosarcoma , neuroblastoma , hodgkin lymphoma , non - hodgkin lymphoma , and melanoma . 
all study participants were required to have adequate organ function ( neutrophils 075 ml , transfusion independent platelet count for 7 days 75 platelets / ml , bilirubin 15 times the upper limit of normal for age , alanine aminotransferase 135 000 u / ml , lipase equal to or lower than the upper limit of normal for age , no evidence of dyspnoea at rest , and pulse oximetry > 92% on room air ) , recovered from the acute toxic effects of previous anticancer therapies , and adequate performance status ( karnofsky 50% or lansky 60 )  . 
initially patients with allogenic stem - cell transplant were excluded ; however , the protocol was amended on sept 08 , 2016 ( version 4 ) , to include patients who had an allogenic stem - cell transplant at least 100 days before study enrolment and had no evidence of graft - versus - host disease . 
patients with known cns metastases or cns tumours , those requiring daily systemic corticosteroids , and those who had received systemic corticosteroids within 7 days before study enrolment were ineligible . 
additional detailed regarding pharmacokinetic statistical analyses , populations assessed for primary and secondary outcomes and planned interim analyses are contained in appendix pp 14 . evaluations , procedures part a was a dose - confirmation to establish the recommended phase 2 dose . 
six patients were planned to receive nivolumab 3 mg / kg intravenously over 60 min on see online for appendix 542 vol 21 april 2020 articles days 1 and 15 of a 28 - day cycle . 
if two of six patients experienced a dose - limiting toxicity ( appendix pp 48 ) during cycle 1 , dose de - escalation was planned to 1 mg / kg . 
if fewer than two patients in part a experienced a dose - limiting toxicity , then 3 mg / kg would be considered the recom mended phase 2 dose that would be tested in part b , as long as the pharmacokinetic analysis ensured that a minimum dose ( cmin ) of 10 g / ml or more occurred in at least five patients in which cmin was defined as the cycle 1 , day 15 pre - dose concentration , to confirm similar drug exposure to that observed in adults treated with the standard dose of 240 mg administered every 14 days . 
accumulation was calculated as the ratio of the area under the concentration time curve ( auc0168h ) for cycle 2 versus cycle 1 [ a : please state frequency and type of samples taken for pk analysis ]  . 
an additional six patients were planned to be enrolled in part a to complete a pharmacokinetic cohort . part b was done to test the recommended phase 2 dose determined in part a , identify signals of activity , and generate further information regarding toxicity of the drug in the following disease specific cohorts : rhabdomyosarcoma , ewing sarcoma , osteosarcoma , neurolymphoma , and non - hodgkin blastoma , hodgkin lymphoma . 
because of the activity of nivolumab in adults with melanoma , 15 patients younger than 18 years with recurrent , measurable melanoma were eligible for enrolment in part b as part of a nonstatistically powered cohort . patients in part a and part b were monitored for toxicity weekly during the first cycle , and then at the beginning of subsequent cycles . 
for part b , occurrence of a toxicity that met the definition of a dose - limiting toxicity affected subsequent treatment for that patient , but did not inform selection of the recommended phase 2 dose . 
review of symptoms , physical examination , and laboratory assessments ( electrolytes , complete blood count , liver enzymes , bilirubin , creatinine , and c - reactive protein ) were done weekly during cycle 1 , then before each cycle and as clinically indicated . 
patients were able to continue on study for up to 2 years unless they showed disease progression ( clinical or radiographic ) , experienced an adverse event requiring removal from therapy , refused further therapy , were non - compliant with therapy , or refused further participation . 
in general , protocol therapy was continued for grade 1 toxicities , with the exception of pneumonitis and cardiac toxicities in which case therapy was held for grade 1 toxicities . 
patients with measurable disease at baseline were evaluable for response if they received at least one dose of study drug and had a disease reevaluation done or clinical progression of disease was documented by the treating physician . 
response was evaluated using recist ( version 1.1 ) , except in patients with neuroblastoma whose response could be evaluated only by metaiodobenzylguanidine scintigraphy , in which response was assessed using curie scoring.16 , 17 due to the possibility of a delayed response following initial tumour progression , patients who experienced tumour growth greater than 20% but less than 40% were allowed to remain on the study for up to 12 weeks with more frequent disease monitoring as long as the patient showed no rapid disease progression or deterioration in performance status , had not experienced a diseaselimiting toxicity , or were otherwise showing clinical benefit . 
complete or partial responses required central radiographic review . pd - l1 expression , assessed by immunohistochemistry on tumour tissue obtained at initial diagnosis or subsequent biopsy , was evaluated centrally using the dako pd - l1 ihc 288 pharmdx assay ( agilent , santa clara , ca , usa ) in formalin - fixed , paraffin - embedded tumour samples.18 the percentage of tumour cells showing plasma membrane pd - l1 staining ( score 0 , 1 + , 2 + , or 3 + ; higher number indicates higher intensity ) was quantified in a minimum of 100 evaluable tumour cells . 
 the presence of tumour - associated immune cells , as well as the presence of pd - l1 membrane staining on associated lymphocytes or macrophages , were also assessed qualitatively . complete details on study design and execution are in the protocol . 
amendments to the study protocol are detailed in the appendix ( p 11 )  . outcomes primary objectives were to determine the tolerability and describe the toxicities of nivolumab at the adult recommended dose of 3 mg / kg in children and young adults with relapsed or refractory solid tumours or lymphoma ; to determine the systemic exposure of nivolumab in children compared to that in adults ; to determine the maximum tolerated dose of nivolumab in children ; to find out the antitumour activity of nivolumab vol 21 april 2020 articles in selected childhood solid tumours or lymphoma in seven expansion cohorts . secondary objectives included exploring the presence of infiltrating lymphocytes and expression of pd - l1 in tumour specimens from patients . 
the study is ongoing and other prespecified analyses ( immuno genicity of nivolumab , and nivolumab effects on circulating cytokines ) will be reported separately . statistical analysis part a was a phase 1 dose - finding study using the rolling 6 study design . 
if out of six evaluable patients , one or none experienced dose - limiting toxicity and at least five achieved a cmin of at least 10 g / ml , the 3 mg / kg nivolumab dose would be the recommended phase 2 dose because the dose is well tolerated and achieves the cmin associated with clinical activity in adults . 
if two or more of the six patients experienced dose - limiting toxicity at the 3 mg / kg dose , then the maximum treatment dose has been exceeded and the 1 mg / kg nivolumab dose would be evaluated . 
if one or none of six evaluable patients experienced a dose - limiting toxicity at the 1 mg / kg nivolumab dose and at least five patients achieve a cmin of at least 10 g / ml , then this dose level would be the recommended phase 2 dose . 
to establish whether nivolumab would be of sufficient interest for further evaluation in a disease category , part b defined a true response rate of 5% of insufficient interest for further evaluation and a response rate of 25% as sufficient for further evaluation . 
a simons optimal two - stage design for each cohort was used ( type 1 error of 007 and 88% power to detect the alternative hypothesis ) wherein each cohort would enrol ten patients in stage one . 
if three or more responses were observed in 20 evaluable patients , the treatment would be considered sufficiently active to warrant further study . for all parts of the study , any patient who received at least one dose of nivolumab and who experienced a doselimiting toxicity ( appendix p 5 ) during cycle 1 was considered evaluable for adverse events . 
in part a , patients who did not have dose - limiting toxicity and did not receive at least 85% of the prescribed dose within the first 28 days ( the observation period for dose - limiting toxicity ) for reasons other than toxicities ( eg , progressive disease ) were not considered evaluable for toxicity and their data were not be included in the study report and an additional patient was enrolled at that dose to replace the inevaluable patient . any patient who was enrolled and met eligibility criteria for part b and received at least one dose of protocol therapy would be considered evaluable for response provided the patient showed progressive disease or death while on protocol therapy , the patient was observed on protocol therapy for at least one cycle and the tumour was not removed surgically before the time complete response or partial response was confirmed , or the patient showed a complete or partial response as confirmed according to protocol criteria . 
 data from patients not evaluable for response were not included in the study report and an additional patient was enrolled at that dose to replace the inevaluable patient . the rolling 6 study design and simons two - stage study design were used for analysis of primary and secondary outcomes.20 , 21 the rolling 6 study design uses interim analyses to determine whether to increase the dose level , decrease the dose level , or define the maximum tolerated dose or the recommended phase 2 dose . 
all authors had full access to all of the data and the corresponding author had final responsibility for the decision to submit for publication . results enrolment occurred from feb 22 , 2015 , to july 30 , 2018 , and data cutoff for analysis was dec 31 , 2018 . 
before treatment with single - agent nivolumab , 71 ( 99% ) patients were treated with a median of three ( iqr 14 ) previous chemotherapy regimens , and 46 ( 64% ) had received radiotherapy with a median of one ( iqr 12 ) radiotherapy regimen . 
seven ( 10% ) patients did not receive the full dose of nivolumab ( five due to disease progression and two due to patient or physician preference ) and two ( 3% ) patients did not have all required laboratory evaluations . in part a , nivolumab 3 mg / kg was well tolerated and was confirmed as the paediatric recommended phase 2 dose ; no dose de - escalation was required and no dose - limiting toxicities were observed . 
in part b , white blood cell decreased neutrophil count decreased anaemia lymphocyte count decreased platelet count decreased 21 ( 28% ) 18 ( 37% ) 30 ( 40% ) 12 ( 16% ) 12 ( 16% ) 2 ( 3% ) 1 ( 1% ) 5 ( 7% ) 7 ( 9% ) investigations other , specify 20 ( 26% ) 1 ( 1% ) 3 ( 4% ) 3 ( 4% ) 2 ( 3% ) aspartate aminotransferase increased alanine aminotransferase increased fatigue nausea anorexia 21 ( 28% ) 1 ( 1% ) 28 ( 37% ) 17 ( 23% ) 1 ( 1% ) hypoalbuminemia 8 ( 11% ) 1 ( 1% ) 1 ( 1% ) 7 ( 9% ) 1 ( 1% ) 14 ( 19% ) 14 ( 19% ) 11 ( 15% ) 8 ( 11% ) 9 ( 12% ) 11 ( 15% ) 10 ( 13% ) 10 ( 13% ) 10 ( 13% ) 8 ( 11% ) 8 ( 11% ) 8 ( 11% ) 7 ( 9% ) 1 ( 1% ) 1 ( 1% ) 1 ( 1% ) 2 ( 3% ) 1 ( 1% ) 2 ( 3% ) 1 ( 1% ) 1 ( 1% ) 1 ( 1% ) 1 ( 1% ) 1 ( 1% ) 1 ( 1% ) 1 ( 1% ) 1 ( 1% ) fever hypokalaemia vomiting abdominal pain headache hypothyroidism hypocalcaemia hyponatremia hypophosphatemia rash maculopapular cough sinus tachycardia lipase increased febrile neutropenia pleural effusion arthralgia autoimmune disorder dyspnoea gastritis mucositis oral central nervous system dysfunction stevens - johnson syndrome tumour pain upper gastrointestinal haemorrhage adverse events that were definitely , possibly , and probably related to study treatment are presented . 
no deaths due to adverse events were reported . table 2 : haematological and non - haematological adverse events five ( 7% ) patients had protocol defined dose - limiting toxicities : grade 3 elevated lipase for more than 7 days ( n = 1 ) , grade 4 neutropenia ( n = 1 ) , grade 3 pain at tumour site ( n = 1 ) , grade 3 upper gastrointestinal haemorrhage ( n = 1 ) , and grade 2 enterocolitis infection ( n = 1 ; appendix p 6 )  . 
in part b , two ( 3% ) patients required dose modifications , one due to grade 2 wheezing that resolved and the patient was able to vol 21 april 2020 articles continue on therapy after one dose interruption and one due to grade 2 transaminitis that eventually necessitated coming off protocol . 
a complete listing of adverse events possibly , probably or definitely attributed to nivolumab is listed in the appendix ( pp 819 )  . grade 3 or 4 adverse events considered to be drugrelated occurred in 27 ( 36% ) of 75 patients . 
the most common immune - related adverse event was hepatic toxicity ( aspartate amino transferase increase in 22 [ 29% ] of 75 patients and alanine aminotransferase increase in 18 [ 24% ] ; table 3 )  . 
pleural or pericardial effusions were reported in 11 ( 15% ) of 75 evaluable patients , three of whom developed both ( we included all patients even if deemed unlikely or unrelated related to study therapy ; only four patients were attributed to study therapy ; table 4 )  . 
effusions developed during the first cycle of nivolumab in seven patients , during the second cycle in two patients , and after discontinuation of nivolumab in three patients ; severity ranged from moderate ( grade 2 in six patients ) to severe ( grade 3 in four ) and lifethreatening ( grade 4 in one )  . 
evaluation of the pleural fluid in one patient supported an inflammatory effusion because there was no evidence of malignant cells . in total , seven ( 10% ) of 72 patients in part b discontinued protocol therapy due to adverse events ( two had prolonged elevation of liver enzymes , one had prolonged elevated lipase , one had prolonged fever , one had gastrointestinal bleeding , one had infection , and one had an autoimmune disorder , including thyroiditis , elevated creatine kinase , elevated creatinine )  . 
37 ( 44% ) of 85 patients died on study or during the follow - up period , none were attributable to study therapy . 12 patients in part a and 64 patients in part b were evaluable for pharmacokinetics ( appendix p 7 )  . 
an accumulation ratio of 17 ( 04 ) was consistent with a half - life of 132 days . in this study , all patients with hodgkin lymphoma had classical hodgkin lymphoma and six were reported to be nodular sclerosing subtype . 
12 patients with hodgkin lymphoma were enrolled , but two patients did not start site cycle reported grade attribution to nivolumab received steroids intrathoracic disease at enrolment epithelioid sarcoma rhabdomyosarcoma , embryonal osteosarcoma neuroblastoma pleural pleural pleural pleural pleural rhabdomyosarcoma , nos rhabdomyosarcoma , alveolar pleural ewing sarcoma ewing sarcoma primary mediastinal large cell lymphoma 100 - day follow - up 100 - day follow - up possible unlikely unrelated possible unrelated possible 2 ; 2 2 ; 2 2 ; 2 paraoesophageal mass pulmonary metastasis pulmonary metastasis pulmonary metastasis none at enrolment pulmonary metastasis pleural and mediastinal metastasis pleural metastasis pulmonary metastasis pleural ; pericardial 2 ; 2 unlikely ; possible mediastinal and chest wall mass pleural ; pericardial 1 ; 100 - day follow - up possible ; possible no pleural metastasis pleural ; pericardial 1 ; 1 unlikely ; possible ewing sarcoma melanoma pericardial pleural 100 day follow - up unlikely unrelated nos = not otherwise specified . table 4 : incidence , timing , and attribution to nivolumab of pleural and pericardial effusions by patient diagnosis 546 vol 21 april 2020 articles t therapy due to changes in disease status following enrolment and therefore were not evaluable for response . 
 in ten patients with hodgkin lymphoma evaluable for response , one patient had a complete response , two had a partial response , five had stable disease ( median 128 cycles , iqr 618 ) , and two had a mixed response , with decrease in size of target lesions but appearance of new lesions during study . 
despite achieving the number of responses required to expand the hodgkin lymphoma cohort in the planned simons the hodgkin lymphoma cohort was not expanded in this trial so that we could evaluate nivolumab in a combination regimen for patients with relapsed hodgkin lymphoma in a separate trial ( ahod1712 ; nct02927769 )  . ten patients with non - hodgkin lymphoma were enrolled and evaluable for response ( table 1 )  . 
one patient with mediastinal large b - cell lymphoma had a metabolic complete response by pet and partial response by recist ( version 1.1 ) and remained on therapy for 11 cycles . 
the non - hodgkin lymphoma cohort was not expanded due to inadequate accrual to complete the expansion cohort . two stage design , as shown in the figure , no objective responses were observed in patients with solid tumours evaluated in this trial ( 74 patients were evaluable for response )  . 
stable disease was reported as best response in 11 ( 33% ) of 33 patients in the sarcoma cohorts and 5 ( 50% ) of 10 patients in the neuroblastoma ( measurable ) cohort . 
 among patients enrolled the neuroblastomametaiodo benzylguanidine cohort , four ( 40% ) of ten were deemed to have stable disease ( via central review ) after two cycles of therapy . 
this patient had metastatic disease at the time of enrolment and had progressed despite three surgical resections and previous therapy with interferonand dendritic cell therapy . 64 ( 75% ) of 85 patients had archival tumour evaluated for pd - l1 expression on tumour cells and on tumourinfiltrating leukocytes by immunochemistry . 
using a conservative cutoff of 1% pd - l1 expression on tumour cells to define positivity , only 750% ( seven of 47 total tested patients ) of non lymphoma tumour cohorts expressed pd - l1 on their tumour cells ( table 5 )  . 
by comparison , in the hodgkin lymphoma cohort , all nine patients tested had pd - l1 expression on their tumour cells , at levels ranging from 30% to 100% of cells ( table 5 )  . 
 in the non - hodgkin lymphoma cohort , pd - l1 expression was evaluated in eight ( 80% ) of ten patients and ranged from 1% to 100% of tumour cells ( table 5 )  . 
the patient intervention start did not start treatment progressive disease stable disease partial response complete response continued treatment neuroblastoma ( measurable ) neuroblastoma ( non - measurable ) rhabdomyosarcoma hodgkin lymphoma melanoma osteosarcoma ewing sarcoma non - hodgkin lymphoma time since enrolment ( months ) figure : response to nivolumab each bar represents one patient . 
for four patients who did not start treatment the bar represents the time from enrolment to withdrawal from study . tumour positivity for pd - l1 and with 100% pd - l1 tumour staining had a partial response . 
 a patient with diffuse large b - cell lymphoma showed 99% infiltrating lymphocytes expressing pd - l1 , but did not show a response to nivolumab ( table 5 )  . 
 pd - l1 membrane staining was most commonly observed on tumour - associated macrophages , although nine ( 16% ) of 58 patients , across various histologies ( three patients with non - hodgkin lymphoma , two with neuroblastoma , and four with sarcoma ) , showed predominant infiltration of lymphocytes expressing pd - l1 . 
together , these results vol 21 april 2020 articles patients who had tumour pd - l1 testing pd - l1 - positive tumour * range of pd - l1positive tumour cells tumours with infiltrating immune cells predominant pd - l1positive immune cell hodgkin lymphoma 9 / 12 ( 75% ) non - hodgkin lymphoma 8 / 10 ( 80% ) neuroblastoma osteosarcoma rhabdomyosarcoma ewing sarcoma 15 / 22 ( 68% ) 9 / 13 ( 69% ) 9 / 12 ( 75% ) 10 / 11 ( 91% ) malignant melanoma 9 / 9 ( 100% ) 7 / 8 ( 88% ) 1 / 15 ( 7% ) 2 / 9 ( 22% ) 1 / 9 ( 11% ) 1 / 10 ( 10% ) 30100% 1100% 13% 9 / 9 ( 100% ) 8 / 8 ( 100% ) 14 / 15 ( 93% ) 7 / 9 ( 78% ) 8 / 9 ( 89% ) 8 / 10 ( 80% ) macrophages macrophages or lymphocytes macrophages or lymphocytes macrophages or lymphocytes macrophages or lymphocytes macrophages other sarcoma 4 / 4 ( 100% ) 2 / 4 ( 50% ) 570% 4 / 4 ( 100% ) macrophages data are n / n ( % ) or % . 
malignant spindle cell and epithelioid neoplasm with focally rhabdoid features ( n = 1 ) , treated spindle and pleomorphic sarcoma ( n = 1 ) , proximal type epithelial sarcoma ( n = 1 ) , and metastatic epithelioid sarcoma ( n = 1 )  . table 5 : pd - l1 expression on tumour cells and infiltrating immune cells show an overall paucity of pd - l1 expression on the common childhood solid tumours evaluated here , excluding lymphomas , and a predominance of macrotumour microphages expressing pd - l1 environment . the discussion in this phase 12 trial , we found that nivolumab was well tolerated in children and the pharmacokinetics of the drug in children were similar to those reported in adults receiving the standard dose of 240 mg every 14 days.22 similar to findings in adults , 23 no clinically relevant effects on nivolumab clearance were observed across the age spectrum of paediatric patients and across the wide range of diseases enrolled on this trial . 
we observed greater frequency of grade 3 or grade 4 haematological toxicity in our cohort compared with that reported in adults , which we suspect is due to our patient population having received multiple myelotoxic chemotherapy or radiotherapy regimens before enrolment . 
 ten of these patients had neoplastic involvement of the lungs or chest at the time of treatment , suggesting that the effusions might be attributable to nivolumabinduced tumour associated inflammation . 
although management of nivolumab associated effusions could not be systematically assessed in this study , several patients were treated with supportive care and corticosteroids and showed symptomatic improve ment in the effusion . some patients with lymphoma experienced clinical benefit with nivolumab . 
despite this encouraging activity , the response rate appears lower than the 6687% overall response rate reported in adults with hodgkin lymphoma.24 , 25 the median age of patients with hodgkin lymphoma is our cohort was lower than the median of 35 years in a study by ansell and colleagues24 and a mean of 39 years in a study by younes and collagues25 in which they reported on 80 adults with classical hodgkin lymphoma.25 ansell and colleagues reported on 23 patients ( median age 35 years ) with hodgkin lymphoma and found that 22 ( 96% ) of 23 patients had a nodular sclerosing subtype of classical hodgkin lymphoma.24 overexpression of pd - l1 , associated with pd - l1 amplifi cation , is believed to contribute to the high response rate of hodgkin lymphoma to immune checkpoint inhibitors.24 , 26 although pd - l1 mutational status was not evaluated in this study , 100% of the hodgkin lymphoma tumours analysed showed high levels of pd - l1 expression as previously reported in adult trials.24 , 25 thus , the differences in histological subtypes treated or pd - l1 expression levels , compared with previous reports in adults , do not seem to account for the lower response rate observed . 
in a phase 2 trial in primary mediastinal b - cell lymphoma , anti - pd1 monotherapy showed a 41% overall response rate.27 in this study , of ten evaluable patients , we observed one partial response in a patient with primary mediatstinal b - cell lymphoma whose tumor showed pd - l1 positivity . 
future work is needed to investigate whether children with hodgkin lymphoma or primary mediastinal b - cell lymphoma experience a lower proportion of response compared with adults and whether this reflects ageassociated distinctions in immunobiology associated with hodgkin lymphoma or primary mediastinal b - cell lymphoma . in this study , there was no evidence for single - agent activity of nivolumab in non - lymphoma paediatric solid tumours , although some paediatric tumour histologies such as wilms tumour , malignant rhabdoid tumour , and germ - cell tumours were not evaluated in this study . 
 biological correlates used to predict response to immune checkpoint inhibitors are imperfect , although high 548 vol 21 april 2020 articles expression of pd - l1 on tumour cells or infiltrating t cells and high tumour mutational burden have been reported to correlate with response.2830 our data , consistent with previously published reports , 3133 show low pd - l1 expression on the histological tumour types enrolled in our study and a paucity of infiltrating t cells . 
given the that response to pd - 1 or pd - l1 blockade in nonlymphoma tumours is thought to reflect reinvigoration of t cells recognising neoantigens derived from tumour mutations , the absence of response might be indicative of the mutational burden in sporadic paediatric solid tumours.28 our study did not assess tumour mutational burden limiting assessment of its effect in the paediatric tumours studied here although previous studies have shown that approximately only 5% of sporadic paediatric solid tumours are classified as hypermutant , as defined by more than ten mutations per mb , 28 , 29 a minimum level that has been suggested to be associated with response to immune checkpoint inhibitors . 
of note , children with hypermutant tumours associated with germline mutations in mismatch repair genes show clinically significant responses to pd - 1 blockade , 13 , 14 providing evidence that paediatric patients are capable of mounting antitumour effects induced by pd - 1 in the presence of adequate antigens to drive t - cell responses . 
future studies are needed to investigate whether selected cohorts of children with hypermutant sporadic solid tumours would show clinical benefit following pd - 1 blockade . in summary , our results show that nivolumab 3 mg / kg every 14 days is tolerable in children . 
antitumour activity was observed in hodgkin lymphoma and in one patient with non - hodgkin lymphoma , but single agent activity was not observed for the common , non - lymphoma , noncns paediatric solid tumours studied here . 
future studies evaluating nivolumab , or other pd - 1 or pd - l1 blockers , alone or in combination with other immuno modulators , might be warranted in selected populations of patients with paediatric solid tumours whose tumours manifest higher mutational burden or other biomarkers that provide evidence for increased tumour immuno genicity . contributors kld , ef , msm , bjw , cgm , and clm contributed to the conception and design of the study . 
all authors contributed to the data interpretation , drafting , and revision of the manuscript and final approval to submit the manuscript for publication . declaration of interests clm is a founder of lyell immunopharma ; holds equity in lyell immunopharma and apricity ; receives consulting fees from lyell immunopharma ; is an advisory board member for neoimmune tech , nektar , pact pharma , bryologyx , allogene , and apricity . 
all other authors declare no competing interests . data sharing the childrens oncology group data sharing policy describes the release and use of childrens oncology groups individual subject data for use in research projects in accordance with national clinical trials network program and national cancer institute community oncology research program guidelines . 
data are available to researchers whose proposed analysis is found by childrens oncology group to be feasible and of scientific merit and who agree to the terms and conditions of use . acknowledgments the research reported is supported by bristol - myers squibb , the childrens oncology group , the national cancer institute of the national institutes of health ( award um1 ca228823 ) , and the cookies for kids cancer foundation . 
we thank the patients and their families for making this study possible . for more on kras mutations in pancreatic cancer see series lancet oncol 2020 ; 21 : e13545 for the 2013 study see nature 2013 ; 503 : 54851 for more on the discontinued kras inhibitor azd4785 see vantage / articles / news / trialresults / astras - first - attempt - failstheres - no - giving - kras for the phase 2 codebreak 100 trial results see iaslc.org / iaslc - news / pressrelease / sotorasib - providesdurable - clinical - benefit - patientsnsclc - and - kras for the phase 1 codebreak 100 trial results see n engl j med 2020 ; 383 : 120717 for more on the krystal - 1 study see issues / november - 25 - 2020 / krasinhibitor - adagrasib - showsactivity - in - non - small - cell - lungcancer / undruggable krastime to rebrand ? after decades of research into kras - mutant cancers , clinical development of drugs targeting this pervasive mutation is finally showing some much - awaited promise . ras proteins are a family of prototypical oncogenes that are mutated in many human cancers . 
kras is the most frequently mutated isoform of ras mutations ( 86% ) , and is mutated in 90% of pancreatic cancers , 40% of colorectal cancers , and 30% of lung cancers . 
compared with other proteins , the relatively smooth protein inhibitors to bind structure meant that designing to surface grooves was difficult , stalling progress in drug development for many years . 
but , in a major breakthrough in 2013 , a compound was developed that could bind to a small pocket in the mutant kras gly12cys protein , reinvigorating efforts to find an active inhibitor . 
development of inhibitors that were selective for mutant forms of kras also reduced the toxicity that might have been observed with widescale inhibition of a ubiquitous prote although recently developed kras inhibitors still failed to progress to latestage clinical trials ( eg , azd4785 ) , the advance in 2013 has led to new drugs reaching further stages of development , with recent data representing the first phase 2 evidence of clinical activity of a kras inhibitor . 
in the single - arm study , 124 patients with previously treated non - smallcell lung cancer ( nsclc ) with a centrally confirmed kras gly12cys mutation were enrolled and given sotorasib , which targets that mutation . 
in the phase 1 krystal - 1 study , presented at the eortc - nci - aacr symposium on molecular targets and cancer therapeutics in october , 2020 , 79 patients with nsclc were given adagrasib twice a day , resulting in objective responses in 23 ( 45% ) of 51 evaluable patients another encouraging result in patients with a high unmet clinical need . 
in view of previous , unsuccessful attempts to target kras mutations in cancer , and the fact that most of the patients included in these trials had already received previous lines of therapy , these results are a sign that barriers to targeting kras are surmountable . however , these are still early results . 
codebreak 100 is a registrational trial and , together with results from krystal - 1 , the outlook for kras inhibition in nsclc is good , but confirmatory studies in larger patient populations and comparison with the current standard of care are needed . 
 although the kras gly12cys mutation is highly prevalent , and potentially targetable , in lung cancers , other kras mutations , such as kras gly12asp , are prevalent in different cancer types . 
use of pan - kras inhibitors that block kras irrespective of mutation type , such as bbp - 454 ( in the preclinical phase ) , might open up kras inhibition to broader patient populations , but the safety of such an approach will be an important consideration . 
new drugs are showing encouraging results , and the goal of improving outcomes for patients with these difficultto - treat tumours seems more like a possibility than a mere pipe drea research in this area is finally gaining momentuon this wave of renewed enthusiasm from this rare story of hope in cancer drug discovery , the label of undruggable now seems unsuitable and unhopeful , and active therapies for some of the most deadly cancers are now potentially within our grasp . 
 the lancet oncology vol 22 march 2021 editorial correction to lancet oncol 2019 ; 20 : 128694 correction to lancet oncol 2019 ; 20 : 137085 correction to lancet oncol 2020 ; 21 : 75051 petct calais j , ceci f , eiber m , et al . 
 f - fluciclovine and ga - psma - 11 pet - ct in patients with early biochemical recurrence after prostatectomy : a prospective , single - centre , single - arm , comparative imaging trial . 
nivolumab plus ipilimumab versus sunitinib in first - line treatment for advanced renal cell carcinoma : extended follow - up of efficacy and safety results from a randomised , controlled , phase 3 trial . 
these corrections have been made to the online version as of may 4 , 2020 , and will be made to the printed version . published online may 4 , 2020 s1470 - 2045 ( 20 ) 30267 - 9 vol 21 june 2020 e304 corrections corrections correction to lancet oncol 2015 ; 16 : 522 correction to lancet oncol 2016 ; 17 : 553 correction to lancet oncol 2016 ; 17 : 733 philip , pa . 
 this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . eggermont amm , chiarion - sileni v , grob j - j , et al . 
this correction has been made to the online version as of june 1 , 2016 . correction to lancet oncol 2016 ; 17 : 751 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . vol 17 june 2016 e223 editorial for the series on us cancer survivorship see pages e11 , e19 , e30 , e39 and e51 for the us national institutes of health page on cannabis see cancer / treatment / cam / hp / cannabis - pdq for the study by whiting and colleagues see jama 2015 ; 313 : 245673 for the 2015 colorado report see com / pubs / mpg%20impact%20 of%20marijuana%20on%20 colorado - final.pdf cannabis : high time for evidence - based policies on nov 8 , while americans elected donald trump as their next president , those in california , maine , nevada , and massachusetts quietly voted for a di erent kind of change : legalisation of the use , sale , and consumption of recreational marijuana for adults over 21 years of age . 
an ongoing controversy , marijuana legislation in 30 us states now con icts with us federal law , in which marijuana is a schedule i controlled substance with no currently accepted medical use and high potential for abuse , but brings these states in line with a global trend . 
for individuals with chronic pain and treatment - induced side - e ectsboth common in patients with cancer and cancer survivorslegalisation of marijuana use could change the treatment landscape , but evidence - based , rational policies must be a top priority . 
 cannabis is legal for medicinal use or is decriminalised in more than 11 european countries , including the netherlands , belgium , and spa australia legalised medicinal cannabis on nov 1 , 2016 , and germany and the canadian federal government will follow in 2017 . 
 the us national institutes of health lists cannabis and cannabinoids ( of which tetrahydrocannabinol [ thc ] is the most notable ) as having potential for treating cancer - related symptoms caused by the disease itself or its treatment , although the evidence for its bene ts and harms is con icting . 
dronabinol and nabilone , synthetic versions of thc , have been approved by the fda to treat cancer - related and chemotherapy - induced nausea , but these are not derived from the native plant . 
 this is in part because research on marijuana in the usa is highly restricted : it requires approval from three separate federal agencies and the drug must only be supplied by the national institute on drug abuse . 
however , for a product rapidly becoming mainstream , clinical trials and basic research are crucial : the requirement for evidence of the bene ts and risks of marijuana use will grow as access increases and regulations , including clear guidelines for safe and e ective use , must be developed . 
and , is it possible , or ethical , to distinguish recreational users from patients with cancer who might have legitimate palliative care needs to ensure their access ? taxes from the regulated sale of marijuana could be enormous ; a 2015 report on the economic impact of legalisation in colorado , usa , since jan 2014 stated that legal marijuana activities generated $121 million in combined sales and excise tax revenues . 
government should , through judicious regulation , ensure that legal medicinal products are safe , e cacious , and cost - e ective ; that they are widely accessible ; and that any potential pro ts are used to develop and improve the health systecrucially , at a time when countries and governments are just starting to control the cancer epidemic caused by tobacco smoking , we must ensure that we do not legalise another inhalable product that could lead to another major public health crisis in 20 years time . 
 the lancet oncology vol 18 january 2017 correction to lancet oncol 2020 ; 21 : 101718 correction to lancet oncol 2020 ; 21 : 93546 correction to lancet oncol 2020 ; 21 : 112526 iarc monographs vol 127 group . 
lancet oncol 2020 ; 21 : 101718in this news piece , the web links in the margin for the preamble to the iarc monographs and for the iarc declarations of interest were incorrect and have been amended . 
 lancet oncol 2020 ; 21 : 112526in this comment , the fourth paragraph should read one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
because overdiagnosis appears to increase with age , it is possible that overdiagnosis occurred in both groups after the age of 50 years , but could not be detected because of the design of the trial . 
 this correction has been made as of sept 1 , 2020 , and the printed version is correct . vol 21 september 2020 e418 corrections published online september 24 , 2020 s1470 - 2045 ( 20 ) 30584 - 2 for more on the two online surveys see org / meetings / esmo - virtualcongress - 2020 / daily - reporter / daily - reporter - news / covid19cancer - research for more on burnout rates among oncology physician assistants in the usa see record / 185959 / abstract for more on oncologists burnout in russia see record / 191626 / abstract for more on us oncologists burnout see j clin oncol 2014 ; 32 : 67886 for more on the cost of physician burnout in the usa see sections / health - shots / 2019 / 05 / 31 / 728334635 / whatsdoctor - burnout - costing - america burnout among cancer professionals during covid - 19 results released newly from two online surveys done by the european society for medical oncology ( esmo ) resilience task force have outlined the extent to which the covid - 19 pandemic has affected burnout , job performance , and wellbeing in the global oncology workforce . 
38% of respondents stated that they had experienced feelings of burnout and 78% had felt increased concern for their personal safety since the onset of the pandemic . july 16 the follow - up survey , which was done from aug 6 , 2020 , found that the proportion of respondents reporting feelings of burnout had risen to 49% . 
 but whereas 66% of respondents in the first survey felt unable to do their job as well as they had done before the pandemic , by the time of the second survey , this proportion had decreased to 49% . these results suggest oncology professionals are adapting to the covid - 19 circumstances with a better ability to manage patients with cancer during the pandemic , but a higher risk of distress and burnout , commented susana banerjee ( royal marsden national health service foundation trust and institute of cancer research , london , uk ) , lead author of the two surveys . the investigators found that as national covid - 19 mortality rates increased , wellbeing and job performance decreased . 
feeling burnout can take time to manifest itself , so i would not expect higher crude covid - 19 mortality rate alone at one timepoint to drive burnout , explained banerjee . 
 there was a lot of uncertainty and unpredictability and , at the time , we had very limited knowledge on the risks of covid - 19 for individual patients with cancer . 
as health - care systems prioritised patients with covid - 19 , referrals for suspected cancer dwindled , increasing the fear of delayed diagnosis and a pending increase in mortality . i think there is a sense of failure and helplessness associated with the pandemic that we have never experienced before , said tara sanft ( yale school of medicine , new haven , ct , usa )  . 
we are trying to manage patients with many more restrictions than we have in the past , and navigate care and communicate with families and teams , all mostly over the phone or video . oncologists are already at heightened risk of burnout , because they have to discuss lifechanging treatment decisions with patients , deliver bad news , and supervise therapies that can have adverse effects , which is not easy , particularly in an era of constrained resources . 
a poster presented at the american society of clinical oncology 2020 meeting noted that rates of burnout among oncology physician assistants in the usa increased from 35% in 2015 , to 49% in 2019 . 
a 2014 survey of more than 1100 us oncologists concluded that 45% had at least one symptom of burnout , although interestingly the same survey found that more than 80% of respondents were satisfied with their career and a similar proportion were satisfied with their specialty . 
there is a real risk of colleagues leaving the profession or early retirement and this impact on the workforce could affect patient care , banerjee told the lancet oncology . the majority of respondents to the esmo surveys believed that counselling and psychological support services would be helpful . 
 covid - 19 has meant that we had to do away with a lot of bureaucracy and hone in on what was important ; i hope systems can learn from this reprioritisation , she said . 
if we really want to address burnout we have to cut through all the red tape and get back to the business of taking care of the patient . talha khan burki 1402 vol 21 november 2020 news forbes ljl , simon ae , warburton f , et al . 
differences in cancer awareness and beliefs between australia , canada , denmark , norway , sweden and the uk ( the international cancer benchmarking partnership ) : do they contribute to differences in cancer survival ? brit j cancer 2013 ; 108 : 292300 . llanwarne n , newbould j , burt j , campbell jl , roland m . 
covid - 19 and long term conditions : what if you have cancer , diabetes , or chronic kidney disease ? bmj 2020 ; 368 : m1174 . fewer cancer diagnoses during the covid - 19 epidemic in the netherlands published online april 30 , 2020 s1470 - 2045 ( 20 ) 30265 - 5 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on may 4 , 2020 for more on the challenges of cancer care during the covid - 19 pandemic see editorial lancet oncol 2020 ; 21 : 603 for more on the impact of covid - 19 on cancer diagnosis see comment page 748 see online for appendix the dreadful consequences of coronavirus disease 2019 ( covid - 19 ) put an unprecedented pressure on health - care services across the globe.1 the netherlands , a country with 174 million inhabitants that provides its citizens with universal access to essential healthcare serviceswith the general practitioner as the gatekeeper to secondary careis no exception in this regard . the first patient with covid - 19 in the netherlands was confirmed on feb 27 , 2020 , in the southern part of the country.2 thereafter , the disease spread rapidly throughout the country . 
subsequently , strict social distancing policies were implemented by the dutch government as of march 15 , 2020 , to mitigate the spread of covid - 19.3 , 4 all sites ( excluding skin cancer ) skin cancers ( excluding basal cell carcinoma ) first conrmed case of covid - 19 in the netherlands nationwide implementation of strict social distancing policies and temporary halt of national cancer screening programmes public awareness campaign about lesser cancer diagnoses 39% 40% 6 jan 13 jan 20 jan 27 jan 3 feb 10 feb 17 feb 24 feb 2 m arch 9 m arch 16 m arch 23 m arch 30 m arch 6 april calendar week in 2020 figure : number of cancer diagnoses by week in the netherlands in the period between jan 6 , 2020 ( calendar week 2 ) and april 12 , 2020 ( calendar week 15 ) basal cell carcinoma of the skin is not included in the statistics . 
the point estimates for the change in cancer diagnoses per calendar week are based on the mean total number of cancer diagnoses in the calendar weeks from 2 to 8 ; that is , the period before the covid - 19 outbreak in the netherlands . 
data from the nationwide netherlands cancer registry in the period between feb 24 , 2020 , and april 12 , 2020which are based on initial case ascertain ment through pathological cancer notifications from the nationwide network of histopathology and cytopathologyshow that there is a notable decrease in cancer diagnoses when compared with the period before the covid - 19 outbreak . 
this effect was most pronounced for skin cancers ( figure ) and observed across all age groups and geographical regions , and almost all cancer sites ( appendix )  . 
first , individuals with potential , non - specific symptoms of cancer might have barriers to consulting a general practitioner , including moral concerns about wasting the general practitioners time for non - covid - 19 - related symptoms , assumptions about insufficient capacity for essential noncovid - 19 - related health - care services , and anxiety about acquiring covid - 19 in a health - care setting . 
a general practitioner might , therefore , postpone initial investigations for symptoms that do not immediately hint towards a potential cancer diagnosis , resulting in delayed or postponed hospital referrals . 
third , hospitals might have postponed diagnostic evaluation or have longer turnaround times for diagnostic evaluation because many hospital - based resources are being allocated to tackle covid - 19 . 
lastly , national screening programmes for breast , colorectal , and cervical cancer are temporarily halted as of march 16 , 2020 , to alleviate the demand on the health - care system due to covid - 19 . 
collectively , fewer cancer diagnoses in the covid - 19 era will result from patient , doctor , and system factors.5 initially disseminated among the upsetting findings of fewer cancer diagnoses the dutch were community on april 2 , 2020 , and again on april 15 , 2020 , by the netherlands comprehensive cancer organisationwhich hosts the netherlands cancer registryto create awareness of this issue . 
lastly , misconceptions were eliminated about a heightened risk of contracting covid - 19 in a health - care setting because of inadequate policies for infection control at the institutional level and resource constraints in the delivery of essential oncological care . priorities for cancer care amid the covid - 19 pandemic will be meticulously triaged on the basis of a multitude of factors that are outside the scope of this comment . 
general frameworks to inform cancer treatment decisions during the covid - 19 pandemic it does merit brief are discussed elsewhere.69 acknowledgment that the effect of a reasonable delay in the management of particular low - risk malignancies ( eg , many skin cancers ) will only marginally affect the quantity and quality of life . 
conversely , the treatment for potentially curable cancers with an imminent risk of early death ( eg , acute leukaemias ) cannot be safely postponed . the data discussed here support the national oncology taskforce and the national coordination centre for patient distribution to safeguard optimal patient access to essential oncological care throughout all hospitals in the netherlands . 
these more detailed dataincluding various patient ( eg , covid - 19 positivity ) , tumour , follow - upwill and treatment characteristics , and ultimately establish the effect of the covid - 19 outbreak on oncological care in the netherlands . 
this information can also guide the public , policymakers , and physicians in the future whenever an outbreak of a similar magnitude occurs . rhav reports grants from bristol - myers squibb and roche , outside the submitted work . 
government.nl / latest / news / 2020 / 03 / 15 / additional - measures - in - schoolsthe - hospitality - sector - and - sport ( accessed april 23 , 2020 )  . dobson cm , russell aj , rubin gp . 
patient delay in cancer diagnosis : what do we really mean and can we be more specific ? bmc health serv res 2014 ; 14 : 387 . hanna tp , evans ga , booth cm . 
 ff l u c i c l o v i n e a n d ga - psma - 11 pet - ct in patients with early biochemical recurrence after prostatectomy : a prospective , single - centre , single - arm , comparative imaging trial . 
lancet oncol 2019 ; 20 : 128694in this article , in figure 2 , the f - fluciclovine detection rate for prostate bed has been corrected to 9 ( 18% )  . 
this correction has been made to the online version as of sept 23 , 2019 . correction to lancet oncol 2019 ; 20 : 160214 oscarsson n , mller b , rosn a , et al . 
lancet oncol 2019 ; 20 : 1602 14in the summary of this article , the first sentence of the findings section should have read of 223 patients screened between may 9 , 2012 , and dec 20 , 2017 , 87 patients were enrolled and randomly assigned to either hyperbaric oxygen therapy ( n = 42 ) or standard care ( n = 45 )  . 
 this correction has been made to the online version as of sept 23 , 2019 , and the printed article is correct . kato k , cho bc , takahashi m , et al . 
nivolumab versus chemotherapy in patients with advanced oesophageal squamous cell carcinoma refractory or intolerant to previous chemotherapy ( attraction - 3 ) : a multicentre , randomised , open - label , phase 3 trial . 
 lancet oncol 2019 ; 20 : 1506517in this article , the name of the funder should be ono pharmaceutical company , and in the results section , paragraph eight , the data for the comparison between groups for the utility index should have been 0076 , 00110142 ; p = 0023 . 
lancet oncol 2019 ; 20 : e52234in this series paper , the value 55% was missing from in the the following sentence first paragraph of the strategies for providing paediatric oncology services section : data from hospital - based registries in the english - speaking caribbean islands show a 2 - year survival rate of 55% compared with 85% in hics . 
this correction has been made to the online version as of oct 30 , 2019 . published online september 23 , 2019 s1470 - 2045 ( 19 ) 30594 - 7 vol 20 november 2019 e613 corrections correction to lancet oncol 2020 ; 21 : e57588 correction to lancet oncol 2021 ; 22 : 2942 correction to lancet oncol 2021 ; 22 : 8597 bahadoer rr , dijkstra ea , van etten b , et al . 
short - course radiotherapy followed by chemotherapy before total mesorectal excision ( tme ) versus preoperative chemoradiotherapy , tme , and optional adjuvant chemotherapy locally advanced rectal cancer ( rapido ) : a randomised , open - label , phase 3 trial . 
 lancet oncol 2021 ; 22 : 2942in figure 1 in this article , in the standard of care group , of the 187 patients who had adjuvant chemotherapy , 185 should have been indicated as having this chemotherapy according to hospital policy . 
fixeddose combination of pertuzumab and trastuzumab for subcutaneous injection plus chemotherapy in her2 - positive early breast cancer ( federica ) : a randomised , open - label , multicentre , non - inferiority , phase 3 study . 
lancet oncol 2021 ; 22 : 8597in table 2 of this article , the cycle 7 ( predose cycle 8 ) pertuzumab serum geometric mean auc 021 days ( percentage cv ) , g / ml per day should have been 2440 ( 242 ) for the intravenous infusion group and 2440 ( 262 ) for the fixed - dose combination group , and the cycle 7 ( predose cycle 8 ) trastuzumab serum geometric mean ( percentage cv ) , auc 021 days g / ml per day should have been 1640 ( 240 ) for the intravenous infusion group and 1700 ( 289 ) for the fixed - dose combination group . 
intermittent schedules of the oral rafmek inhibitor ch5126766 / vs - 6766 in patients with ras / raf - mutant solid tumours and multiple myeloma : a single - centre , open - label , phase 1 dose - escalation and basket dose - expansion study . 
also , sentence two of paragraph four of the discussion should have read these tumours harboured a range of ras and raf mutations , including kras gly12asp , kras gly12val , kras gly12arg , brafve , and hras gly13arg . 
 vol 22 february 2021 corrections valuing all lives equally : cancer surgery , covid - 19 , and the nhs in crisis as covid - 19 infections continue to increase at an unprecedented rate , and the uk enters the toughest phase of the pandemic so far , the national health service ( nhs ) finds itself under the most pressure seen in its 72 - year history . 
with the majority of intensive care beds occupied by patients with covid - 19 , kings college hospital in london was one of the first to take the drastic action to cancel urgent cancer surgeries . 
however , it is not alone , as other nhs hospitals in london , manchester , birmingham , cambridge , essex , scotland , and northern ireland , to name just a few , have also started to cancel urgent cancer surgeries . it would be prudent for the uk health secretary , matt hancock , to announce a regional approach to tackle cancelled surgeries in the various health trusts immediately . 
improving and connecting all referral pathways would help to facilitate an improved flow of patients to hospitals that are not yet at capacity . in addition to the hundreds of cancer operations being cancelled as hospitals are inundated with patients with covid - 19 , more than 3800 patients with cancer in london are already waiting beyond the 62 - day target for their first cancer treatment , and more than 1000 individuals needing urgent cancer surgery do not yet have a date for their treatment . 
estimates suggest that in london alone , more than 500 patients with cancer need to be treated per week to stay on top of demand , but most hospitals that were meant to remain covid - 19 - free are now compromised . 
despite the cancellation of urgent cancer surgery , they are now being earmarked for recovering patients who are not ready to be discharged from hospital , as well as for mass covid - 19 vaccination centres . 
if these emergency hospitals were staffed properly and used to their full potential , the impact of covid - 19 on cancer surgery might be reduced . faces while the nhs immense pressures from covid - 19 , and with all but the most urgent elective activities , including cancer surgery , postponed , it is shocking that some non - time - critical elective care is continuing in the private sector . 
when the first lockdown began in march , 2020 , all private providers in england were on an unprecedented national block contract with nhs england , to ensure that nhs patients who needed urgent surgery were prioritised over private patients with less urgent needs . 
with only a third of chemotherapy capacity used , despite grave concern about delays for some patients with cancer and general under - use , this arrangement ended in august , 2020 . 
regrettably , this partnership has not been renewed because the uk government is currently unwilling to fund nhs england to refer patients to a private sector that remains below capacity . the cost of cancelling urgent cancer surgery and the impact on lives cannot be underestimated . 
a covidsurg collaborative study published in may , 2020 , predicted that during the 12 - week peak disruption of hospital services caused by covid - 19 last year , at least 28 million elective operations were cancelled or postponed worldwide , including more than two million cancer operations . 
despite the ongoing extraordinary efforts of all nhs staff , it is imperative that the covid - 19 crisis does not cause unmitigated suffering for the many people with cancer in the uk . 
yet , older patients are undeniably under - represented and even discriminated against in cancer care . comorbidities in patients aged 65 years or older can preclude their inclusion in cancer clinical trials . 
 one analysis quantified this fact : people in this age group accounted for just 29% of patients included in colon cancer trials and 15% of those in breast cancer trials . 
another study showed larger age disparities between study participants and the incident disease population in trials with industry sponsorship than in those not sponsored by industrya bias that one could argue cynically encourages more positive results . when patient selection is so stringent , it calls into question whether the study population is representative . 
can results from such trials be truly representative of the average patient with cancer ? as an example , although the incidence of colorectal cancer is increasing in younger people , with an average age of onset of 68 years in men and 72 years in women , a standard upper limit of 65 years can lead to the exclusion of many diagnosed cases , leaving an atypical population with an earlier onsetand perhaps more aggressiveform of the disease . 
therefore , age inclusion criteria in trials that are dependent and relevant to the cancer type should be used . although a move away from paternalism in cancer care is essential , this shift has gone too far in some areas . 
the number of major upper - abdominal resections done in octogenarians with cancer ( aged 8089 years ) was found to have risen in 200111 , despite an increased morbidity risk . 
patient choice might be a factor in the rising incidence of complex surgeries , so it is vital that the risks and benefits of all clinical options are clearly communicated to patients , especially those at greater risk of complications , so that the best choice is made for each individual irrespective of chronological age . with under - representation in trials on one end of the scale and potential overuse of surgery on the other , the ideal scenario for older patients lies somewhere in between . 
increasingly , clinicians are realising that use of chronological age , created arbitrarily by sociolegal norms , can be poorly representative of an individuals health status , and instead are opting to use geriatric assessments tools to evaluate older patients health to inform cancer care . 
 the american college of surgeons coalition for quality in geriatric surgery have also developed a new geriatric surgery verification programme , which sets out standards that hospitals should meet to improve surgical outcomes for older patients . 
but with a report from the community oncology alliance showing that some 423 us community cancer clinics had closed between 2008 and 2018 , and that 45 practices reported sending medicare patients to other clinics for cancer care , neglect of older patients is clearly an ongoing concern . 
thus , better collaboration and coordination between all health - care providers is needed to develop personalised evidence - based treatment plans delivered in the right place at the right time . it can be easy to perceive those over a certain age as weak or frail . 
but remove two letters from the word elderly and you will arrive at an entirely different word , elder with its connotations of knowledge and wisdo older patients should not be viewed as fragile or side - lined , but should be recognised as a population from whom much can be learned . 
the lancet oncology for the lancet oncology series on geriatric oncology see series / geriatric - oncology for the study on geriatric patients in cancer clinical trials see proc am soc clin oncol 2019 ; 37 ( suppl ) : e23032 ( abstr ) for the study on age disparities in trial participants by industry sponsorship see jama oncol 2019 ; published online june 3 . 
 the cediranib in alveolar soft part sarcoma ( casps ) study was designed to discriminate the effect of cediranib from the intrinsically indolent nature of asps . methods in this double - blind , placebo - controlled , randomised , phase 2 trial , we recruited participants from 12 hospitals in the uk ( n = 7 ) , spain ( n = 3 ) , and australia ( n = 2 )  . 
patients were eligible if they were aged 16 years or older ; metastatic asps that had progressed in the previous 6 months ; had an ecog performance status of 01 ; life expectancy of more than 12 weeks ; and adequate bone marrow , hepatic , and renal function . 
participants were randomly assigned ( 2 : 1 ) , with allocation by use of computer - generated random permuted blocks of six , to either cediranib ( 30 mg orally , once daily ) or matching placebo tablets for 24 weeks . 
participants were unblinded at week 24 or sooner if they had progression defined by response evaluation criteria in solid tumors ( version 1.1 ) ; those on placebo crossed over to cediranib and all participants continued on treatment until progression or death . 
the primary endpoint was percentage change in sum of target marker lesion diameters between baseline and week 24 or progression if sooner , assessed in the evaluable population ( all randomly assigned participants who had a scan at week 24 [ or sooner if they progressed ] with target marker lesions measured )  . 
this study is registered with clinicaltrials.gov , number nct01337401 ; the european clinical trials database , number eudract2010 - 021163 - 33 ; and the isrctn registry , number isrctn63733470 recruitment is complete and follow - up is ongoing . findings between july 15 , 2011 , and july 29 , 2016 , of 48 participants recruited , all were randomly assigned to cediranib ( n = 32 ) or placebo ( n = 16 )  . 
four participants in the cediranib group were not evaluable for the primary endpoint ( one did not start treatment , and three did not have their scan at 24 weeks )  . 
median percentage change in sum of target marker lesion diameters for the evaluable population was 83% ( iqr 265 to 59 ) with cediranib versus 134% ( iqr 11 to 213 ) with placebo ( one - sided p = 00010 )  . 
the most common grade 3 adverse events on ( blinded ) cediranib were hypertension ( six [ 19% ] of 31 ) and diarrhoea ( two [ 6% ] )  . 
15 serious adverse reactions in 12 patients were reported ; 12 of these reactions occurred on open - label cediranib , and the most common symptoms were dehydration ( n = 2 ) , vomiting ( n = 2 ) , and proteinuria ( n = 2 )  . 
 one probable treatment - related death ( intracranial haemorrhage ) occurred 41 days after starting open - label cediranib in a patient who was assigned to placebo in the masked phase . interpretation given the high incidence of metastatic disease and poor long - term prognosis of asps , together with the lack of efficacy of conventional chemotherapy , our finding of significant clinical activity with cediranib in this disease is an important step towards the goal of long - term disease control for these young patients . 
 other studies involving asps , ongoing and completed , were identified using the clinicaltrials.gov website , searching for alveolar soft part sarcoma ; pubmed , searching for publications in english between jan 1 , 2000 , and dec 31 , 2018 , using the search terms tyrosine kinase inhibitor , anti - angiogenic agent , and alveolar soft part sarcoma ; via presentations at international meetings , and personal communications . 
other drugs with reported activity in asps include sunitinib , pazopanib , and anlotinib . added value of this study asps has a high metastatic potential , but usually slow disease progression , and sometimes spontaneous disease arrest and even , rarely , regression can occur . 
to our knowledge , this study is the only randomised trial to be reported in asps so far . implications of all the available evidence although the precise molecular targets of cediranib in asps are not known , this study has confirmed the value of this drug in the treatment of advanced asps . 
confirmation of the activity of cediranib in a randomised , placebo - controlled trial will provide a sound basis for future research with this and other drugs for asps . a slight predominance in women and a high incidence of metastatic disease at diagnosis.1 although metastases are intrinsically indolent , the long - term outlook is poor.2 lieberman and colleagues2 report that only 15% of patients with no metastases at diagnosis remained metastasis free after 20 years of follow - up , with a median metastasis - free period of 6 years and median survival after development of metastases of 2 years . 
if patients presented with metastases , median survival was 3 years , compared with 11 years for patients who were metastasis free at diagnosis , and survival tended to worsen with increasing age.2 unusually for a soft - tissue sarcoma , in addition to lung metastases , asps also metastasises to brain and bone.3 histologically , the disease is characterised by uniform polygonal cells arranged in a pseudoalveolar pattern separated by vascular septae , and molecular studies4 have shown a characteristic non - reciprocal translocation , t ( x ; 17 ) ( p112 ; q25 ) , resulting in the aspscr1tfe3 fusion gene that replaces the n - terminal portion of tfe3 in a manner consistent with transcriptional deregulation.4 asps cells have periodic acid - schiff ( pas ) - positive precrystalline granules that contain monocarboxylate transporter 1 ( mct1 ) and its chaperone basigin ( cd147 ) .5 in a genetically engineered mouse study6 that used the aspscr1tfe3 gene to drive oncogenesis , the mice developed tumours in the brain and orbitie , the cranial vaulta region known to have the highest lactate concentrations in the mouse . 
in addition to supplying energy , lactate acts to stimulate cell proliferation and angiogenesis because of the excess pyruvate , which upregulates hypoxia - inducible factor 1 inhibition of the prolyl hydroxylase ( hif1 - ) via responsible for its degradation , 7 raising the possibility that the lactate transporter mct1 could be a therapeutic target for inhibition of tumour angiogenesis.8 cediranib is a receptor tyrosine - kinase inhibitor , the targets of which include the vegf receptors vegfr1 , vegfr2 , and vegfr3 ; kit ; and platelet - derived growth factor receptors . 
after observation of a prolonged partial remission with cediranib in a patient with locally advanced and metastatic asps treated in a phase 2 , hypertension management study ( nct00264004 ) , 9 an opportunity arose to treat a further six patients with asps who were treated in a cediranib pharmacodynamic study of patients with soft - tissue sarcoma , most of whom had gastrointestinal stromal tumours ( d8480c00046 ) .10 strong evidence of the clinical activity of cediranib against asps , in terms of durable partial remissions and disease stabilisation , led to further studies including a single - arm , phase 2 trial of cediranib in asps by the us national cancer institute.11 other tyrosine - kinase inhibitors have also been shown to have activity in asps . 
a direct antitumour effect has been shown with sunitinib mediated by platelet - derived growth factor receptor ( pdgfrb ) , vegfr2 , and ret , with five partial responses in nine patients and median progression - free survival on treatment of 17 months ( range 233 ) .12 in adults , a retrospective study reported one complete response and seven partial responses in 30 patients treated with pazopanib , with a median progression - free survival of 136 months ( range 16322 ) and only little activity with trabectedin.13 in 40 patients with asps and a rearrangement of the tfe3 gene treated serine / threonine - protein kinase haspin with homolog alk1 and hepatocyte growth factor receptor the 1024 vol 20 july 2019 articles see online for appendix ( met ) inhibitor crizotinib , one patient had a partial response and 35 had stable disease as their best response , with 1 - year progression - free survival of 375% ( 95% ci 229521 ) .14 anlotinib has also been reported to have activity in a prospective basket study15 in which six of 13 patients with asps had partial responses and the median progression - free survival was 21 months . 
preliminary reports of immunomodulatory drugs have been activity with presented in the past 2 years.15 , 16 the cediranib in alveolar soft part sarcoma ( casps ) trial aimed to assess the efficacy of cediranib in the treatment of asps . 
the double - blind , placebo - controlled design was chosen because of the unusual biology of this cancer , which , although having strong metastatic potential , is characterised by indolent metastatic tumour growth and periods of spontaneous stabilisation , making single - group uncontrolled studies difficult to interpret.3 , 12 ethical challenges exist in placebo groups , which we mitigated by having a 2 : 1 randomisation favouring active treatment , restricting the no - treatment period to 24 weeks , and allowing crossover to active treatment on disease progression or , if no progression , after week 24 . 
 a preliminary report of casps was presented at the 2017 annual general meeting of the american society of clinical oncology.17 methods study design and participants in this multicentre , double - blind , placebo - controlled , randomised , phase 2 trial , participants were recruited from 12 hospitals in the uk ( n = 7 ) , spain ( n = 3 ) , australia ( n = 2 )  . 
patients were required to have measurable metastatic disease that had progressed according to the response evaluation criteria in solid tumors ( recist ) version 1.1 in the previous 6 months ; an ecog performance status of 01 ; life expectancy of more than 12 weeks ; and adequate bone marrow , hepatic , and renal function ( absolute neutrophil count > 15 10 per l ; platelet count > 10010 per l ; serum bilirubin < 15 upper limit of normal [ uln ] , unless proven gilberts syndrome ; alanine transaminase or aspartate transaminase < 25 uln or < 5 uln if liver metastases present ; serum creatinine < 15 uln or creatinine clearance > 50 ml per min )  . 
exclusion criteria included history of gastro intestinal disorder likely to impair absorption of cediranib ; poorly controlled hypertension ; any severe or uncon trolled comorbidityeg , active infection ; prolonged qt intervalie , qtc 480 msec ( using bazetts correction ) or family history of long qt syndrome ; substantial recent haemorrhage ( > 30 ml bleeding or episode in previous 3 months ) ; major thoracic or abdominal surgery in previous 14 days ; recent history of thrombosis ; pregnant or breastfeeding women ; unwillingness to use adequate birth control measures ; anticancer treatment in the previous 4 weeks , with the exception of palliative radiotherapy ; known hypersensitivity to any excipient of cediranib ; history of other malignancy except cancer in situ unless individual had been disease free for more than 2 years and with tissue diagnosis of asps from target lesion ; and any other concomitant anticancer therapy except steroids . 
 previous treatment with cediranib was added as an exclusion criterion and approved as a protocol amendment on the advice of the joint independent data monitoring and steering committee ( idmsc ) on sept 24 , 2014 . patients provided written , informed consent before enrolment . 
the study was approved by the south west london research ethics committee 4 ( rec reference 10 / h0806 / 118 ) in the uk ; the clinical research ethics committee of hospital de la santa creu i sant pau , barcelona ( 12 / 070 [ r ] ) , in spain ; and by the metro south health service district human research ethics committee , qld ( hrec / 12 / qpah / 10 ) , and the sydney local health district human research ethics committee ( hrec / 12 / rpah / 26 ) , in australia . 
the clinical trials and statistics unit at the institute of cancer research , london , uk ( icr - ctsu ) , had overall responsibility for trial coordination with two international trials groups ( grupo espaol de investigacin en sarcomas [ geis ] , madrid , spain , and australasian sarcoma study group [ assg ] , melbourne , australia ) having responsibility for regulatory and ethics submissions , monitoring , and safety reporting within their respective countries . 
the icr - ctsu undertook all central statistical monitoring , interim , and final analyses . randomisation and masking participants were randomly allocated ( 2 : 1 ) to cediranib or placebo by computer - generated random permuted block method ( block size of six ) derived by icr - ctsu , and the sequence centrally was generated random isation centrally at the icr - ctsu . 
both the participants and clinicians were masked to treatment allocation until week 24 or until disease progression if this occurred sooner.treatment was supplied in numbercoded bottles , masking participants and clinicians to assignment . procedures depending on treatment allocation , participants received cediranib or matching placebo 30 mg orally once daily , for the first 24 weeks of the study . 
participants could withdraw from the trial at any point and for any reason . review , and clinical assessments , including physical examination , symptom routine blood and urine investigations , took place at 2 and 4 weeks , then once every 4 weeks until week 24 , every 8 weeks up to 48 weeks , then every 12 weeks until progression or treatment discontin uation . 
tumour assessments ( ct or mri if indicated ) were done at baseline , every 8 weeks until week 48 , and then every 12 weeks until disease progression or death . 
 blood pressure was monitored at least weekly for the first 4 weeks , then monthly up to 24 weeks and thereafter as specified in the protocolie , every 8 weeks up to 48 weeks and every 12 weeks thereafter . 
masked radiology review was not planned as part of this study , although translational imaging studies are planned . toxicity was assessed using national cancer institute common terminology criteria for adverse events ( ctcae ) version 4 on the same schedule as the clinical assessments . 
coding was done by use of the medical dictionary for regulatory activities ( version 14 )  . treatment - related toxicities of grade 3 or worse , or repeated episodes of grade 2 toxicities not responding to adequate supportive measures were managed initially with dose interruptions of 25 days , with reintroduction on resolution at the same dose . 
longer interruptions up to 14 days were permitted for chronic problems such as nausea , diarrhoea , and palmar - plantar erythroto supportive dysaesthesia syndrome treatmenteg , antiemetics or loperamide . 
abnormal thyroid function was treated with l - thyronine as appropriate . if refractory outcomes the primary endpoint was percentage change in the sum of the longest diameters ( or shortest if nodal disease ) of target marker lesions , measured at 24 weeks ( or at progression if sooner ) from the date of treatment assignment . 
protocol - defined secondary endpoints were the proportion of participants with an objective response at week 24 , defined as the proportion of participants having either a partial or complete response at the end of blinded treatment ; best response up to week 24 , defined as best response at any point during blinded treatment ; best percentage reduction of target marker lesion size during blinded treatment ; progression - free survival defined as time from random assignment to disease progression ( defined by recist version 1.1 ) or death from any cause ; the proportion of patients alive and progression free at 12 months ; overall survival , defined as time from random assignment to death ( any cause ) ; and the safety and tolerability profile of cediranib in all participants . 
participants with non - recist confirmed progression ( eg , radio logically confirmed but lesions not measured according to recist , or participants with clinical evidence of progression only ) were censored at the date of their progression . exploratory endpoints included radiological responses using choi criteria , identification of predictive angiogenesis markers of response , to describe changes in angiogenesis markers and expression of angiogenesis regulatory genes in peripheral blood and optional tumour biopsies , and to explore changes in circulating endothelial cells and other rare cells events , including potential sarcoma circulating cells . 
in the previously mentioned cediranib pharmacodynamic phase 2 study ( d8480c00046 ) , 10 of 36 participants ( ten of whom had soft - tissue sarcoma and 26 had a gastrointestinal stromal tumour ) , six participants with metastatic asps had a mean decrease in tumour size at 8 weeks of 25% , with a coefficient of variation of 19% . 
 we assumed that a smaller effect and greater coefficient of variation than these results might be observed in a larger trial ; therefore , we determined that 36 participants would be required to detect a 20% decrease in the sum of the diameters of target marker lesions at 24 weeks between placebo and cediranib with a coefficient of variation of 25% , 80% power , and a one - sided significance level of 5% . 
we calculated this sample size for a twosample t test of the log transformation of the sum of the diameters of target marker lesions using the sampsi 1026 vol 20 july 2019 articles command in stata . 
we did a formal interim analysis after 18 participants ( 12 assigned to cediranib and six assigned to placebo ) had 24 weeks of follow - up data ( or had disease progression if sooner ) to determine early activity of cediranib . 
we chose to present the data as medians and iqrs and to use non - parametric tests a priori because of the uncertainty around whether or not the data would be normally distributed . 
for survival - related endpoints , we used the itt population ; thus , we still analysed participants allocated to placebo who subsequently crossed over as belonging to the placebo group . 
we calculated hazard ratios ( hrs ) and 90% cis from cox proportional hazards regression models for progression - free survival , with hrs of less than 1 favouring cediranib . 
similar to the primary endpoint , we did a sensitivity analysis for progression - free survival and overall survival , excluding two participants who had received cediranib before entering the study . 
we planned two additional sensitivity analyses for progression - free survival : one to include participants who had nonrecist confirmed progression , and the other was a landmark analysis , also including participants who had non - recist confirmed progressio , n but censoring participants 26 weeks after random assignment to provide insight into progression - free survival in the absence of crossover . the safety analysis population included all treated participants ( ie , all those who received at least one dose of study drug or placebo ) , and we summarise the worst grades of adverse events during the blinded treatment phase . 
 we present here any adverse event that was reported in at least 10% of participants in either treatment group , or in one or more participants for grade 3 and worse events . 
 we also report on the number of serious adverse reactions to cediranib . we also did an unplanned , exploratory analysis to explore the effect of previous tyrosine - kinase inhibitor therapy on progression - free survival . post hoc , we analysed duration of response ( calculated as time from first response , complete or partial response , to date of progression ) , and the proportion of participants in each group who had a clinical benefit at 24 weeks for completeness and to enable comparison with other studies . analyses are based on a database snapshot taken on april 11 , 2018 . 
 this study is registered with clinicaltrials.gov , number nct 0133740 ; on the isrctn registry , number isrctn 63733470 ; and on the european clinical trials database , number eudract 2010 - 021163 - 33 . role of the funding sources the funders of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all data in the study and final responsibility for the decision to submit for publication . results between july 15 , 2011 , and july 29 , 2016 , 48 patients recruited from 12 hospitals in three countries ( n = 31 from seven hospitals in the uk , n = 9 from three hospitals in spain , and n = 8 from two hospitals in australia ) were enrolled . 
more participants were recruited than were originally planned under the recommendation of the idmsc to account for the four participants who were not evaluable for the primary endpoint and two participants who had received cediranib previously . 
32 participants were randomly assigned to cediranib and 16 to placebo ( figure 1 ) and baseline characteristics were well balanced between the treatment groups ( table 1 )  . 
more than half of participants were diagnosed within 25 years of trial entry , the most common site of disease was the upper leg or groin and 11 ( 23% ) of 48 participants had known brain metastases at trial entry . 
20 ( 42% ) participants had previously received tyrosine - kinase inhibitor treatment , including two ( 4% ) with previous cediranib . a planned interim analysis was done of a snapshot of data taken on feb 4 , 2014 , and did not meet the stopping vol 20 july 2019 1027 articles 32 randomly assigned to cediranib 16 randomly assigned to placebo 31 started treatment 16 started treatment 48 patients recruited 48 enrolled 1 did not start treatment * 3 did not undergo scan at 24 weeks 1 due to early 2 due to other reasons discontinuation caused by toxicity 28 evaluable for primary analysis 16 evaluable for primary analysis 1 had previous cediranib 1 had previous cediranib 27 in cediranib naive population 15 in cediranib naive population figure 1 : trial profile * found to have a tumour infiltrating their heart after random assignment . 
one patient was subsequently found to be ineligible because of unconfirmed progression in the 6 months before trial entry , but was included in analyses . time on blinded criteria for the primary endpoint ( appendix p 57 ) , thus the study continued until the primary analysis . 
of 32 participants randomly assigned to cediranib , one ( 3% ) did not start treatment and three ( 6% ) did not have their scan at 24 weeks ( one of whom discontinued due to toxicity )  . 
of those who started treatment , 14 ( 45% ) in the cediranib group and four ( 25% ) in the placebo group had at least one dose modification , dose delay , or missed dose during blinded treatment because of adverse events . 
11 ( 35% ) of 31 who were given blinded cediranib did not continue to open - label treatment ; eight ( 26% ) because of disease progression , one ( 3% ) because of haematemesis , one ( 3% ) because of palmar - plantar erythrodysesthesia and fatigue , and one ( 3% ) because of general poor tolerance and planned surgery . 
of 36 ( 75% ) participants who started open - label cediranib , eight ( five from the cediranib group and three from the placebo group ) were still on treatment at the data cutoff for this analysis . 
reasons for discontinuation in the remaining 28 participants were disease progression ( n = 21 ) , adverse events ( n = 2 ) , patient choice ( n = 4 ) , and death ( n = 1 )  . 
 median time on open - label cediranib was 416 weeks ( iqr 210670 ) for the participants from the cediranib group and 403 weeks ( 1221086 ) for those from the placebo group . in the evaluable population ( 44 [ 92% ] of 48 enrolled patients ) , we found a significant difference in the median percentage change in the sum of the diameters of target marker lesions at 24 weeks of 83% ( iqr 265 to 59 ) in the cediranib group compared with 134% ( 11 to 213 ) in the placebo group ( one - sided p = 00010 ; figure 2 )  . best median percentage change in the sum of the diameters of target marker lesions by 24 weeks was 157% ( iqr 263 to 24 ) with cediranib and 12% ( 24 to 109 ) with placebo ( one - sided p < 00001 ; appendix p 2 )  . ( 42 the cediranib - naive population similar results were obtained in the sensitivity analysis [ 88% ] of 48 participants ) : median percentage change in the sum of the longest diameters ( or shortest if nodal disease ) of target marker lesions at 24 weeks was 44% ( iqr 263 to 60 ) with cediranib versus 144% ( 11 to 226 ) with placebo ( one - sided p = 00019 ) and best percentage change was 150% ( iqr 263 to 24 ) with cediranib versus 13% ( 25 to 118 ) with placebo ( onesided p = 000010 )  . the proportion of participants with an objective response , based on best response during the blinded treatment phase , was 19% , with six of 31 participants on cediranib having a partial response at any timepoint during the masked treatment phase . 
however , at week 24 , three of these participants no longer met recist criteria for partial response , and thus the proportion of participants with an objective response at week 24 was 11% ( three of 28 )  . 
14 ( 50% ) of 28 participants in the cediranib group and seven ( 44% ) of 16 in the placebo group had stable disease at 24 weeks ; thus the proportion of participants with clinical benefit at 24 weeks was 61% ( 17 of 28 ) for cediranib and 44% ( seven of 16 ) for placebo ( post - hoc analysis )  . 
of the seven participants in the placebo group who were stable at 24 weeks , three had received no treatment in the 6 months before randomisation , one had surgery to the primary disease site , and another three were on another tyrosine - kinase inhibitor until a month before randomisation . 
of the 14 patients randomly assigned to cediranib with stable disease or better at 24 weeks before therapy , three had no previous treatment ; eight had local therapy ( surgery or radiotherapy , or both ) only to primary or metastatic sites , or both ; two had local therapy and another tyrosine - kinase inhibitor ; and one had another tyrosine - kinase inhibitor only . 
of the 32 participants assigned to the cediranib group , two ( 6% ) who had stable disease up to week 24 subsequently achieved a partial response ( one by week 32 , the other by week 40 )  . 
notably , at the time of primary analysis with a minimum of 6 months follow - up after random assignment to treatment , four ( 25% ) of 16 participants in the placebo group had not progressed . 
we found no evidence of a significant difference in progression - free survival between the treatment groups ( unadjusted hr 082 , 90% ci 047143 ; p = 028 ; figure 3 ) , although , this analysis was probably confounded by the crossover to cediranib . 
in a sensitivity analysis excluding those participants with previous cediranib treatment , a similar result was achieved ( unadjusted hr 076 , 90% ci 043135 ; one sided p = 021 )  . 
we expect that with extended follow - up , the progression - free survival curves will increasingly converge due to the proportional effect of crossover to active therapy in those patients who were originally allocated to placebo . 
the first planned additional sensitivity analysis included three ( 6% ) of 48 participants ( one in the cediranib group and two in the placebo group ) who had non - recist confirmed progression ( appendix p 5 )  . 
 * patients who progressed had either progression of non - target lesions or appearance of new lesions despite a less than 20% decrease in the sum of target marker lesions . 
patient received cediranib before trial entry . cediranib median progression - free survival 101 months ( iqr 53190 ) placebo median progression - free survival 49 months ( iqr 19200 ) unadjusted hr 082 90% cl ( 047143 ) ; one - sided p = 028 overall survival between the groups ( figure 4 )  . 
excluding participants with previous cediranib treatment , the log rank p value ( one sided ) was 042 . the safety population included 47 ( 98% ) participants who had at least one dose of trial treatment . 
 most grade 3 adverse events on cediranib were hypertension and diarrhoea , which were managed by dose reduction ( adverse events that resulted in doses reductions are not shown separately in table 2 )  . 
as expected , we found no evidence of a difference in 1030 vol 20 july 2019 articles progression - free survival was difficult to assess because small numbers precluded formal comparisons ( appendix p 7 )  . discussion casps has confirmed the activity of cediranib in participants with advanced , metastatic asps , with a significant difference in the median percentage change in sum of the diameters of target marker lesions at 24 weeks compared with placebo . 
this endpoint was considered a more reliable index of treatment effect than progression - free survival in light of known indolent progression , spon taneous stabilisation , and spontaneous regression in this disease.12 additionally , this unconventional endpoint was considered more sensitive than progression - free survival and thus required fewer participants to show a significant difference between the two groupsan important con sideration for a trial in such a rare disease . 
the difference in median progression - free survival at the time of the analysis was not significant , with absolute values of 101 months ( iqr 53190 ) for cediranib and 49 months ( 19200 ) for placebo . 
some participants with stable disease and partial response had long - lasting disease control , with a median duration of response of 16 months ( iqr 157260 )  . we recognise that our analyses of secondary endpoints such as progression - free survival and overall survival are underpowered . 
however , the rarity and indolence of asps and the incorporation of crossover within the randomised trial dictated the use of an unconventional primary endpoint and acceptance that demonstration of superiority using more conventional criteria would not be possible . 
progression - free survival and overall survival data are reported to enable comparisons with other drugs , none of which have yet been studied in a prospective randomised trial ( eg , sunitinib , pazopanib , axitinib , axitinib plus pembrolizumab , anlotinib )  . 
most data on other tyrosine - kinase inhibitors are derived from reports on small single - centre studies or larger studies in soft - tissue sarcomas of which asps comprised only a small component . 
toxicity was as expected for a drug of this class and was generally manageable with dose interruptions or reductions , with few participants allocated to cediranib withdrawing due to treatment sideeffects . 
there were no grade 4 adverse events or deaths due to these causes . table 2 : adverse events reported during the blinded treatment phase the idea that inhibitors of angiogenesis , such as vegf receptor inhibitors like cediranib , might be active against asps was prompted by the observations of dormancy and spontaneous stabilisation , and the belief that some form of angiogenic switch might be responsible.18 an additional explanation , which is not mutually exclusive , is that this behaviour could be due to immune surveillance , for which supportive clinical data now exist from the use of immunomodulatory drugs ( eg , pembrolizumab ) .16 evidence of lactate as an energy source in asps , 6 with consequent upregulation of hif1 and vegf , might partially explain the activity of drugs that inhibit vegf receptors , although other targets could be involved . 
 spontaneous regression could be mediated via the immune systea study of the vegf receptor inhibitor axitinib in combination with pembrolizumab investigating in soft - tissue sarcomas ( nct02301039 ) is ongoing.16 in participants with asps , the proportion with an objective response was 455% ( 95% ci 181754 ) and with a 3 - month progression - free survival estimate of 909% ( 95% ci 508987 )  . immunomodulation to our knowledge , none of the molecularly targeted drugs discussed here have been studied as extensively as cediranib in asps or have shown superior activity . 
 this study does not have a no - treatment group , precluding control for spontaneous stabilisation or regression or variations in the rate of disease progression between the groups . in casps , the proportion of participants who had an objective response at week 24 ( 19% ) was lower than that reported overall by kummar and colleagues in a phase 2 trial of cediranib in metastatic asps ( 35% ) , 11 in which participants had a slightly lower median age than in this study ( 27 years vs 31 years ) , but a similar proportion had received antiangiogenic therapy previously ( 26% vs 33% in casps )  . 
although casps was open participants aged 16 years and older ( in kummar and colleagues study , the threshold was 18 years ) only one patient younger than 20 years was recruited , showing the predominance of participating centres only seeing adult patients . undertaking a randomised trial in such a rare disease , which has an incidence of less than one per million people per year , was challenging . 
the decision to undertake casps as a randomised trial was vindicated by the fact that seven ( 44% ) of 16 participants in the placebo group had stable disease at 24 weeks , despite all participants having documented progressive disease before study entry . 
at the time of primary analysis with a minimum of 6 months follow - up after random assignment to treatment , four ( 25% ) participants in the placebo group had still not progressed . 
this choice inevitably led to confounding in the interpretation of overall survival and long - term progression - free survival , as shown by the apparent convergence of the progression - free survival curves at 12 months . the findings of this study support the concept that antiangiogenic therapy is active against advanced asps . 
 whether or not the spectrum of receptor tyrosine kinases inhibited by cediranib is substantially different from that of other drugs that are active in this disease ( eg , sunitinib ) is unclear . 
 comparative data on relative potency in vitro against different receptor tyrosine kinases do not seem helpful in predicting toxicity profiles , and hypertension is not a reliable efficacy biomarker.19 given the high incidence of metastatic disease and poor long - term prognosis of asps , together with the lack 1032 vol 20 july 2019 articles of efficacy of conventional chemotherapy , the confirmation of significant clinical activity with cediranib in this disease is an important step towards the goal of longterm disease control for these young patients . 
further studies using cediranib in asps and other sarcomas , in conjunction with other drugs with potential activity in the disease , are warranted . contributors ij was chief investigator ; contributed to trial design , protocol development , participant recruitment , data collection , data interpretation , and writing ; and was a member of the trial management group . 
ml , vb , qc - h , rc , ad , ih , wj , alp , bs , mt , and jmt contributed to participant recruitment and data collection , and were members of the trial management group . 
all authors reviewed the manuscript prior to submission . declaration of interests ij , jpm , lk , lf , kj , sk , cs , ct , and jmb report grants and non - financial support in the form of study drug provision and distribution from astrazeneca during the conduct of the study . 
ij also reports personal fees from eli lilly , bayer , nektar , pharmamar , glaxosmithkline , ariad , and the institute of cancer research outside of the submitted work . 
 jmb also reports grants and non - financial support from astrazeneca , merck sharp & dohme , puma biotechnology , clovis oncology , and janssen - cilag ; grants , non - financial support , and travel support from pfizer ; and grants from medivation , novartis , and roche outside of the submitted work . 
all other authors declare no competing interests . data sharing the institute of cancer research , clinical trials and statistics unit ( icr - ctsu ) supports the wider dissemination of information from the research it conducts and increased cooperation between investigators . 
 trial data is collected , managed , stored , shared , and archived according to icr - ctsu standard operating procedures to ensure the enduring quality , integrity , and utility of the data . 
data recipients are required to enter a formal data sharing agreement that describes the conditions for release and requirements for data transfer , storage , archiving , publication , and intellectual property . 
 data sharing is undertaken if proposed projects have a sound scientific or patient benefit rationale as agreed by the tmg and approved by the independent data monitoring and steering committee as required . 
additionally , all indirect identifiers that could lead to deductive disclosures will be removed in line with cancer research uk data sharing guidelines . acknowledgments we thank the investigator - sponsored study collaboration between astrazeneca and the national institute for health research ( nihr ) clinical research network ( crn ) : cancer for their support , with funding from astrazeneca and for the study grant from cancer research uk ( cruk / 10 / 021 grant reference c2130 / a12118 )  . 
additionally , funding in australia was provided by the australasian sarcoma study group ( assg ) and funding in spain was provided by astrazeneca , spain , and the grupo espaol de investigacin en sarcomas ( geis ) to cover local costs . 
the institute of cancer research clinical trials and statistics unit ( icr - ctsu ) also receives programme grant funding from cancer research uk ( grant number c1491 / a15955 )  . 
we thank all the patients and their families who participated in this study , all staff involved at the 12 participating hospitals , and the staff involved in the trial at the icr - ctsu , assg , the centre for biostatistics and clinical trials at peter maccallum cancer centre ( which manages australian trial activities on behalf of assg ) , geis , and sofpromed investigacin clnica ( which manages spanish trial activities on behalf of geis )  . 
finally , we thank the past and present colleagues on the cediranib in alveolar soft part sarcoma ( casps ) trial management group , and the casps joint independent data monitoring and steering committee . 
 for example , the poster competition alone has resulted in nearly 100 submissions from 22 di erent countries , 74% of which report on research being done by groups in asia . 
furthermore , by drawing on the knowledge of a faculty of over 40 world - renowned speakers , the forum will focus on the ten most prevalent cancers in the asiapaci c region and will examine aspects of prevention , diagnosis , treatment , and palliation . 
opinion - leaders will discuss cancer aetiology , health - care systems , and the challenges of providing e ective disease management with limited resources , along with views on state - ofthe - art treatments in the areas of diagnostics , medical oncology , radiotherapy , and surgical oncology . 
finally , the forum will also host a didactic workshop on how to run a clinical trial ; a poster display of ongoing research relevant to asia ; and a poster discussion session in which authors of the three posters judged most in uential will have an opportunity to present their work orally . 
in this case report the second sentence of the rst paragraph ( she was given sirolimus and had complete remission of the disease . ) was included by error and should be ignored . 
additionally , the fth sentence of the second paragraph should have read : after a loading dose of 10 mg sirolimus , she received sirolimus once a day ; sirolimus doses were titrated to a trough sirolimus concentration of 512 ng / ml , attaining a nal maintenance dose of 2 mg once a day starting in may , 2004 . gerhard opelz , volker daniel , cord naujokat , et al . 
in this article the anti - epstein - barr virus immunoglobulin g reactivity should have read : 7735 1475 u / ml ( sandoglobulin ) , 1600 71 u / ml ( cytotect ) , and 1425 249 u / ml ( cytogam ) , as extrapolated from the results obtained at a one to ten dilution ( dade behring )  . vol 8 march 2007 levofloxacin prophylaxis in patients with newly diagnosed myeloma ( teamm ) : a multicentre , double - blind , placebo - controlled , randomised , phase 3 trial mark t drayson , stella bowcock , tim planche , gulnaz iqbal , guy pratt , kwee yong , jill wood , kerry raynes , helen higgins , bryony dawkins , david meads , claire t hulme , irene monahan , kamaraj karunanithi , helen dignum , edward belsham , jeff neilson , beth harrison , anand lokare , gavin campbell , michael hamblin , peter hawkey , anna c whittaker , eric low , janet a dunn , for the teamm trial management group and trial investigators summary background myeloma causes profound immunodeficiency and recurrent , serious infections . 
we aimed to assess whether patients newly diagnosed with myeloma benefit from antibiotic prophylaxis to prevent infection , and to investigate the effect on antibiotic - resistant organism carriage and health care - associated infections in patients with newly diagnosed myeloma . methods teamm was a prospective , multicentre , double - blind , placebo - controlled randomised trial in patients aged 21 years and older with newly diagnosed myeloma in 93 uk hospitals . 
we randomly assigned patients ( 1 : 1 ) to levofloxacin or placebo with a computerised minimisation algorith allocation was stratified by centre , estimated glomerular filtration rate , and intention to proceed to high - dose chemotherapy with autologous stem cell transplantation . 
patients were given 500 mg of levofloxacin ( two 250 mg tablets ) , orally once daily for 12 weeks , or placebo tablets ( two tablets , orally once daily for 12 weeks ) , with dose reduction according to estimated glomerular filtration rate every 4 weeks . 
this study is registered with the isrctn registry , number isrctn51731976 , and the eu clinical trials register , number 2011 - 000366 - 35 . findings between aug 15 , 2012 , and april 29 , 2016 , we enrolled and randomly assigned 977 patients to receive levofloxacin prophylaxis ( 489 patients ) or placebo ( 488 patients )  . 
597 serious adverse events were reported up to 16 weeks from the start of trial treatment ( 308 [ 52% ] of which were in the levofloxacin group and 289 [ 48% ] of which were in the placebo group )  . 
serious adverse events were similar between the two groups except for five episodes ( 1% ) of mostly reversible tendonitis in the levofloxacin group . interpretation addition of prophylactic levofloxacin to active myeloma treatment during the first 12 weeks of therapy significantly reduced febrile episodes and deaths compared with placebo without increasing health care - associated infections . 
these results suggest that prophylactic levofloxacin could be used for patients with newly diagnosed myeloma undergoing anti - myeloma therapy . funding uk national institute for health research . copyright 2019 the author ( s )  . 
we found that the risk of infection was greatest in the first 3 months after diagnosis of myeloma , with a third of patients suffering serious bacterial infection and infection , contributing to half of early mortality . 
despite this increasing concern about health care - associated infections , to our knowledge , there have been only two small inconclusive randomised controlled trials of antimicrobial prophylaxis in patients with myeloma , meaning a study of antimicrobial prophylaxis in patients with newly diagnosed myeloma was warranted . added value of this study to our knowledge , this is the first double - blind randomised placebo - controlled trial of antibiotic prophylaxis in patients with myeloma and the first trial to show improved survival and reduced infections . 
the trial was designed to map onto current standard practice in the uk , recruiting 977 patients from 93 hospitals and allowing a choice of anti - myeloma therapy , with most patients receiving newer anti - myeloma therapies . 
 examination of stool samples and nasal swabs every 4 weeks revealed no difference between the levofloxacin group and the placebo group for new acquisitions of clostridium difficile , meticillin - resistant staphylococcus aureus , and extended - spectrum - lactamase - positive gram - negative rods when assessed up to 16 weeks . 
the results of this study suggest that the benefits of levofloxacin prophylaxis outweigh the perceived risks in patients with newly diagnosed myeloma . implications of all the available evidence to our knowledge , this is the largest trial to date of levofloxacin prophylaxis in patients newly diagnosed with myeloma and provides the best available evidence to suggest that levofloxacin prophylaxis could be a standard of care in the first 12 weeks after diagnosis . reduce death from infections , since it has been shown to improve survival in patients with prolonged neutropenia.10 however , concerns about increased antibiotic resistance , 11 , 12 drug - related side - effects , and the risk of health care - associated infections13 mean the use of quinolone prophylaxis remains controversial.1417 although the profile of bacterial infections is similar to that seen in neutropenia , most infections in patients with myeloma are not associated with low neutrophil counts but arise because of immunodeficiency , encom passing reduced integrity of barriers and reduced competence of both innate and adaptive immunity . 
given this difference and there being , to our knowledge , only two small inconclusive randomised controlled trials of antimicrobial prophylaxis in myeloma so far , 18 , 19 and considering the increasing concern of health care - associated infections , there was ambivalence for the use of antimicrobial prophylaxis in patients newly diagnosed with myeloma in the uk.18 , 19 here , we report the results of the tackling early morbidity and mortality in myeloma ( teamm ) trial , which assessed the benefit of 12 weeks of levofloxacin prophylaxis and the effect on resistant organism carriage and health care - associated infections in patients with newly diagnosed myeloma . methods study design and participants teamm was a multicentre , double - blind , placebocontrolled , randomised , phase 3 trial done in 93 uk hospitals ( appendix pp 14 )  . 
eligible patients were aged [ excluding pneumocystis prophylaxis 21 years and older with newly diagnosed , symptomatic myeloma based on internationally agreed criteria , 20 , 21 within 14 days of starting a programme of anti - myeloma therapy . 
patients with the following characteristics were ineligible for this trial : contraindication to levofloxacin ( ie , known to have sensitivity or allergy to levofloxacin or other quinolones , a history of tendon disorders related to fluoroquinolone administration , receiving other pro phylactic antibiotic treatment regarded as essential ] , receiving amiodarone or arsenic trioxide , and on active antiepileptic treatment ) ; women of childbearing age who were not willing to use appropriate methods of contraception to prevent pregnancy ; women who were breastfeeding ; patients thought to have mandatory requirement for prophyl actic antibiotics ( with the exception of pneumocystis prophylaxis if regarded as essential ) ; and previous ( < 5 years since diagnosis ) or concurrent active malig nancies , except surgically removed basal or squamous cell carcinoma of the skin , treated carcinoma in - situ of the breast or cervix , or incidental histological finding of prostate cancer ( tnm stage t1a or 1b )  . 
patients were recruited by clinicians and research teams at their local hospitals . the study was approved by the uk coventry and warwickshire multi - research ethics committee on vol 20 december 2019 laboratory , heart of england nhs trust , birmingham , uk ( prof p hawkey md ) ; and patient advocacy , myeloma uk , edinburgh uk ( e low ba ) correspondence to : prof mark t drayson , school of immunity and infection , university of birmingham , birmingham b15 2tt , uk m.t.drayson@bham.ac.uk see online for appendix 1761 articles july 29 , 2011 . 
all patients provided written , informed consent . randomisation and masking we randomly assigned patients ( 1 : 1 ) to levofloxacin or placebo with a computerised minimisation algorithm that generated a trial number and drug pack allocation for each patient . 
allocation was stratified by centre , estimated glomerular filtration rate ( > 50 ml / min , 2050 ml / min , and < 20 ml / min ) , and intention to proceed to high - dose chemotherapy with autologous stem cell transplantation ( yes vs no )  . 
this list was then used to build the bespoke randomisation and drug inventory syste participants were enrolled by research staff at each centre who used a dedicated randomisation phone line at the clinical trials unit and after undergoing eligibility checks were allocated a drug pack number . 
sample drug packs were tested independently to confirm the active drug and placebo were correctly coded . procedures symptomatic myeloma was diagnosed according to british committee for standards in haematology and uk myeloma forum guidelines on the management and diagnosis of multiple myeloma20 , 21 with immunofixation of serum and urine to identify monoclonal immunoglobulin , measurement of bone marrow plasma cells , and identification of myeloma - related end organ damage . patients were given 500 mg of levofloxacin ( two 250 mg tablets ) , orally once daily for 12 weeks , or placebo tablets ( two tablets , orally once daily for 12 weeks ) , with dose reduction according to estimated glomerular filtration rate every 4 weeks . 
anti - myeloma therapy was given according to local practice . we assessed nasal swabs and stool samples collected at baseline , 4 weeks , 8 weeks , 12 weeks , and 16 weeks as per protocol for carriage of meticillin - resistant staphylococcus ( mrsa ) , clostridium difficile , and extendedaureus spectrum - lactamase ( esbl ) gram - negative coliforms . 
we identified esbl gram - negative coliforms from faecal screens and clinical specimens by culture on selective agar and genotyped for ctx - m - lactamase denaturing genes liquid chromatography . 
we cultured nasal swabs for mrsa and isolates were typed and stored . high - performance we assessed myeloma activity and markers of immunocompetence in blood and urine collected at baseline , 4 weeks , 8 weeks , 12 weeks , 16 weeks , and 1 year . 
markers of immunocompetence assessed were monoclonal and polyclonal immunoglobulins , antibodies specific to a range of bacterial and viral target antigens , markers of inflammation , and cytokines . capture of febrile episodes was via hospital records or patient diary cards as patients were asked to self - report temperature daily or when they felt unwell . 
management of neutropenic sepsis is relatively standardised across the uk according to national institute for health and care excellence guidelines.22 deaths were reviewed by a masked inde pendent clinical reviewer not linked to the trial . 
cause of death was ascertained from information sent by the centre regarding cause of death and disease status , and review of previous serious adverse events and myeloma response on blood samples received . 
assessments were done by two trial clinicians who were masked to the trial intervention . outcomes the primary outcome was time to first febrile episode or death from all causes within the first 12 weeks of trial treatment . 
a single febrile episode was defined as the initial febrile event and any subsequent fevers until that course of anti - infectives was stopped . secondary outcomes assessed from start of trial treatment to 12 weeks were the number of deaths and infection - related deaths ; number of non - febrile infections ( clinically suspected infections without a temperature 38c or higher and where anti - infectives were prescribed ) ; number of days in hospital ; number of days in hospital on anti - infective ; carriage and invasive infections with mrsa , c difficile , and esbl gramnegative coliforms ; patient characteristics , steroid usage , and indices of immunocompetence and their relation to colonisation by and development of infection from s aureus , c difficile , and esbl gram - negative coliforms and non - health care - associated infection and eastern cooperative oncology group performance status ; number of clinically documented infections , episodes of severe sepsis ( common terminology criteria for adverse events grade 3 or 4 ) , and suspected infections ; incidence of microbiologically proven infections , the pathogens , and their susceptibility to antibiotics ; days on infection ; and antibiotic therapy for treatment of response to anti - myeloma therapy and its relationship to total 1762 vol 20 december 2019 articles infection . 
secondary outcomes from randomisation to beyond 12 weeks were carriage and invasive infections with s aureus , c difficile , and esbl gram - negative coliforms between 12 weeks and 16 weeks to assess for delayed effects from the intervention that was stopped at 12 weeks ; response to anti - myeloma therapy at 16 weeks ; quality of life ( 4 - weekly questionnaires up to 16 weeks ) ; health economics ( daily diary card that captures elements of health resource use combined with information captured on the case report form ) ; and overall survival . 
 number of days in hospital , days on antibiotic therapy for treatment of infection , reponse to anti - myeloma therapy at 16 weeks , health economics and quality of life , more detailed microbiology , and in - depth analysis on patient measures of immunocompetence and relation to infection , and depth of myeloma response in relation to antibiotic use , will be reported separately . statistical analysis our power calculations assumed that 30% of patients would have a febrile episode or death in the first 12 weeks and levofloxacin would reduce this to 20% ; thus , 800 patients ( 400 in each study group ) would allow differences in excess of 10% to be detected with 90% power using a two - sided test at 5% significance . 
 a pre - planned early stopping guideline was applied for safety and reviewed by the data and safety monitoring committee , who endorsed the continuation of enrolment from 800 patients to up to 1000 patients . 
 recruiting 1000 patients into the trial ( 500 in each group ) would allow differences greater than 8% to be detected with 90% power using a two - sided test at 5% significance . 
1000 patients would also allow detection of a levofloxacin - induced three - times increase in c difficilepositive stools from 5% to 15% between entry to the trial and 12 weeks , with 95% power and 5% significance ( two - sided test )  . we analysed the primary endpoint with a log - rank comparison , beginning from the date the patient started trial treatment to the time of an event , or to censor date for those with no events up to 12 weeks . 
all randomly assigned patients were included in an intention - to - treat analysis of the primary endpoint , assessed using kaplan - meier curves and the log - rank test.23 we did prespecified exploratory analyses with cox proportional hazards models to compare trial groups after adjustment for stratification variables with assumptions for non - proportionality.24 proportionality assumptions were checked by visual inspection of kaplanmeier curves . 
we generated forest plots to examine the treatment effects in prespecified subgroups . we calculated overall survival from the date the patient started trial treatment to the date of death or censoring , as appropriate , with all - cause mortality . 
 this trial is registered with the isrctn registry , number 2183 patients assessed for eligibility 435 not meeting inclusion criteria 494 declined to participate 1206 excluded 66 other reasons 211 not known 977 randomly assigned 489 allocated to levooxacin 477 received allocated intervention 12 did not receive allocated intervention 488 allocated to placebo 475 received allocated intervention 13 did not receive allocated intervention 50 between 0 and 4 weeks 35 between 4 and 8 weeks 24 between 8 and 12 weeks 109 withdrew within treatment phase 46 participant choice 32 other reason 31 suspected drug toxicity 54 between 0 and 4 weeks 30 between 4 and 8 weeks 14 between 8 and 12 weeks 98 withdrew within treatment phase 48 participant choice 25 other reason 25 suspected drug toxicity 36 lost to follow - up 9 withdrew within the follow - up phase 36 lost to follow - up 3 withdrew within the follow - up phase 489 analysed for the primary endpoint 488 analysed for the primary endpoint figure 1 : trial profile isrctn51731976 , and the eu clinical trials register , number 2011 - 00366 - 35 . role of the funding source the funder and sponsors of the study had no role in study design , data collection , data analyses , data interpretation , or writing of the report . 
the corresponding author had full access to the data in the study and with sb , tp , gi , and jad had final responsibility for the decision to submit for publication , with the agreement of all other authors and the data monitoring and safety committee . results between aug 15 , 2012 , and april 29 , 2016 , we randomly assigned 977 patients to receive levofloxacin prophylaxis ( 489 patients ) or placebo ( 488 patients ; figure 1 ; appendix pp 14 )  . 
because 207 ( 21% ) of 977 patients withdrew during the trial treatment period and recruitment was faster than expected , the recruitment target was extended to 1000 patients ( figure 1 )  . 
the median patient age was 67 years ( iqr 5975 ) in the levofloxacin group and 67 years ( 6175 ) in the placebo group . 31 ( 6% ) of 489 patients in the levofloxacin group and 25 ( 5% ) of 488 patients in the placebo group withdrew because of suspected drug toxicity , and 15 ( 2% ) of these were unblinded . 
24 ( 2% ) of 977 total patients took an incorrect dose of levofloxacin ( or placebo ) during a 4 - week block of the 12 - week trial period according to their estimated glomerular filtration rate results . 
29 ( 9% ) of 308 serious adverse events in the levofloxacin group and 15 ( 5% ) of 289 serious adverse events in the placebo group were classed as possibly related to drug , eight ( 3% ) of 308 serious adverse events in the levofloxacin group and six ( 2% ) of 289 serious adverse events in the placebo group were classed as probably related to drug , and one ( < 1% ) case of delirium definitely related to drug was reported in the levofloxacin group . 
tendonitis was reported in five ( 1% ) of 489 patients in the levofloxacin group ( vs none in the placebo group ) and all episodes resolved , although three had sequelae reported in the short terone ( < 1% ) case of suspected levofloxacin - induced confusion reversed on stopping the drug . 
other categories of serious adverse events were similar between the study groups ( table 2 )  . in the levofloxacin group , 95 ( 19% ) first febrile episodes or deaths in 489 patients were reported versus 134 ( 27% ) in 488 patients in the placebo group ( hazard ratio for time to first event within 12 weeks [ hr ] 066 , 95% ci 051086 ; p = 00018 ; figure 2 )  . 
febrile episodes , deaths , and febrile episodes with death during the first 12 weeks were less frequent in the levofloxacin group than in the placebo group ( 87 [ 18% ] vs 112 [ 23% ] febrile episodes , four [ 1% ] vs seven [ 1% ] febrile episodes with death ; appendix p 6 )  . 
a prespecified subgroup analysis of time to first febrile episode or death within the first 12 weeks of treatment is shown in figure 3 . [ 3% ] deaths , and four [ 1% ] vs 15 cox regression analysis showed that treatment with levofloxacin was the most important factor in reducing febrile episodes or deaths and retained significance even when controlling for baseline characteristics . 
314 patients took co - trimoxazole 960 mg three times per week to prevent pneumocystis jirovecii pneumonia ( 155 in the placebo group and 159 in the levofloxacin group ; appendix p 10 )  . 
we recorded only one case of proven p jirovecii pneumonia and one possible microbiologically unproven case ( both in the levofloxacin group ) , and neither of these patients were receiving co - trimoxazole prophylaxis . 
use of prophylactic low dose co - trimoxazole also showed a significant benefit in reducing febrile episodes and deaths ( hr 059 , 95% ci 044080 ; p = 00007 ) and adjustment for co - trimoxazole made little difference to the levofloxacin benefit ( 066 , 051086 ; p = 00015 ) , indicating that these two variables have independent effects ( appendix p 10 )  . median follow - up was 12 months ( iqr 813 )  . 
log - rank analyses showed an overall survival benefit for the use of levofloxacin up to 12 weeks , with patients in the levofloxacin group having overall survival of 98% ( 95% ci 9799 , with 426 of 489 patients known to be surviving ) versus overall survival in the placebo group of 95% ( 9397 , with 405 of 488 patients known to be surviving ; p = 00081 ) , but no survival benefit at 12 months ( levofloxacin overall survival 90% , 95% ci 8793 vs placebo 8893 ; p = 094 ; appendix p 11 )  . 
during the 12 - week trial period , two ( 25% ) of eight patients in the levofloxacin group and ten ( 45% ) of 22 in the placebo group died while known to be responding to treatment . 
 five ( 63% ) of eight in the levofloxacin group and 14 ( 64% ) of 22 patients in the placebo group died with no evidence of infection at the time of death . 
at study entry , including chronic respiratory - related comorbidities obstructive pulmonary disease , asthma , and bronchiectasis were reported in 75 ( 15% ) of 489 patients in the levofloxacin group and 67 ( 14% ) of 488 patients in the placebo group . there were 323 non - febrile infections requiring antiinfective treatment . 
these non - febrile infections occurred in 249 patients116 ( 24% ) of 489 patients in the levofloxacin group versus 133 ( 27% ) of 488 patients in the placebo group ( p = 023 )  . 
59 ( 70% ) of 84 organisms isolated from the levofloxicin group versus 124 ( 73% ) of 170 organisms isoloated from the placebo group were sensitive to a range of antibiotics , although zero of three isolates in the levofloxacin group were sensitive to fluoroquinolones versus seven ( 88% ) of eight patients in the placebo group ( appendix p 9 )  . 
a case of suspected pneumocystis pneumonia and a case of microbiologically proven pneumocystis pneumonia were reported in most of the clinical isolates reported by two ( < 1% ) of 662 patients who had not taken cotrimoxazole in the levofloxacin group , and there was one case of c difficile infection in each of the two trial groups . local laboratories were bacterial , but 15 ( 13% ) of 112 were candida spp ( mainly upper airway or oral infections ) and 20 ( 18% ) of 112 were viral ( appendix p 8 )  . 
there were fewer streptococcus pneumoniae ( usually levofloxacin - sensitive ) than we anticipated , with three isolates reported in the placebo group and none in the levofloxacin group . infections 2595 stool and 2933 nasal samples were returned . 
 we observed similar acquisition rates for carriage of c difficile , esbl gram - negative coliforms , and mrsa between the levofloxacin group and placebo group over the 12 weeks of treatment and 4 weeks after treatment ( table 4 )  . 
this difference could not be accounted for by imbalance of baseline factors , by use of antibiotics in the month before diagnosis ( 75 [ 15% ] of 489 patients in the levofloxacin group vs 76 [ 16% ] of 488 patients in the placebo group ) , or by the use of steroids in the 14 days before trial entry ( 248 [ 51% ] patients in the levofloxacin group vs 246 [ 50% ] patients in the placebo group )  . 
nevertheless , new acquisitions of health care - associated infections were similar between the trial groups ( 40 in the levofloxacin group vs 45 in the placebo group )  . discussion levofloxacin prophylaxis resulted in significantly fewer deaths , febrile episodes , and a longer time to first febrile episode or death , than did treatment with placebo . 
this difference remained significant after adjustment for baseline prognostic factors , the use of prophylactic co - trimoxazole and when stratifying by various subgroups . including conventionally , studies on antibiotic prophylaxis in neutropenia use febrile episodes or infected patients as the primary endpoint , because studies are not usually powered to show a predicted 23% reduction in mortality.10 nevertheless , death is an important endpoint and should be captured . 
if febrile episodes alone is the primary endpoint , a higher number of deaths in one randomisation group might favour this group , since death prevents further febrile episodes occurring in this group . 
to our knowledge , no single large wellconducted study on antibiotic prophylaxis in neutropenia has shown a significant reduction in deaths , but metaanalysis showed a 3% reduction with fluoro quinolones and is the basis of several guidelines in patients with neutropenia.10 , 15 , 17 the reduction in deaths observed in the teamm study suggests that either the benefit of 1768 vol 20 december 2019 articles levofloxacin prophylaxis in newly diagnosed myeloma might be greater than in prolonged neutropenia , which could be shown in a future meta - analysis , or that our trial sample was just sufficient to show a benefit statistically and the real size of benefit might be similar to that in prolonged neutropenia . 
either way , to our knowledge this is the first time that the use of prophylactic antibiotics has shown a survival benefit in patients with newly diagnosed myeloma . the reduction in early deaths began within the first month and continued throughout the 3 - month treatment period , during which there were 30 deaths . 
if this were the case , continuing levofloxacin beyond 12 weeks might keep a patient who did not respond to first - line therapy alive long enough to respond to second - line therapy . a 12 - week prophylaxis period was chosen from data available at trial initiation . 
these data showed that the infection risk was highest in the first 2 months after diagnosis with myeloma and reduced as the disease responded to treatment and came under control.7 these data were from patients treated before the use of novel anti - myeloma agents . 
more recent studies have suggested that novel agents and high - dose steroids might contribute to a persistent risk of infection , even when myeloma is well controlled and this infection risk remains high during the first year after diagnosis.6 with the intro duction of immunotherapy , induction regimens might become even more immunosuppressive and be continued for longer periods than at present , increasing the risk of infectionrelated death . 
a continuing infection risk beyond 12 weeks raises the question of whether the absence of survival benefit at 12 months might be due to early stopping of the intervention12 months of prophylaxis might be beneficial . a limitation of our study is that the total number of deaths was small , reflecting a generally well and young patient population . 
201115 population data for england showed 792% net survival for newly diagnosed patients with myeloma at 12 months.9 12 - month overall survival in our study was 90% , and if adjusted for the risk of unrelated death as with net survival , the difference between our trial population and real - world population survival would be greater . 
since our subgroup analysis suggested that the benefit of levofloxacin was greatest in older and less fit patients , levofloxacin prophylaxis might exert a greater benefit once it is adopted in a real - world population . 
furthermore , since a benefit for prophylaxis was shown in a typical trial population that comprises a younger , more favourable myeloma prognosis group than does real - world patients , there is no patient subgroup for which levofloxacin prophylaxis should not be recommended . 
in the uk in 2017 , the prevalence of escherichia coli resistance to fluoroquinolones was reported to be 175% , but in italy resistance is 47%.25 however , such high resistance might not be observed for all relevant invasive organisms in myeloma . 
in such countries , patient subgroups showing the strongest benefit for levofloxacin prophylaxis , namely patients who are not eligible for stem cell transplantation and those with eastern cooperative oncology group performance status 24 , are still likely to benefit . febrile episodes with a temperature of 38c or greater are not a trivial event for patients with myeloma and have a major impact on quality of life and health - care costs , as patients are requested to attend hospital and are frequently admitted . 
we observed more non - febrile infections than febrile infections ( 323 non - febrile vs 264 febrile ) , showing such infections also have a substantial burden for patients and the health - care syste the clinically attributed sites of infection during febrile episodes were similarly distributed to those previously reported in the literature , 26 , 27 with most being in the respiratory tract . levofloxacin was well tolerated , and related serious adverse events were rare . 
european medicines agency17 and us food and drug administration alerts28 have highlighted the risk of long - term tendon damage , neuropsychiatric concerns , and hypo glycaemia following treatment with fluoro quinolones , especially in elderly people and largely occurring when the cause of such symptoms was not recognised and drug treatment continued . 
our data showed a less than 1% risk of tendonitis with no or mild sequelae after stopping levofloxacin , despite our median patient age being 67 years and most patients receiving high - dose steroids . 
patients who received 250 mg levofloxacin because of an estimated glomerular filtration important vol 20 december 2019 1769 articles rate of 50 ml / min or less did not derive a benefit of levofloxacin prophylaxis in our subgroup analyses . 
 although some hospitals might use levofloxacin 250 mg daily for patients with neutropenia , there is no evidence that this dose is sufficient and therefore we recommend the use of adjusted therapeutic doses of levofloxacin as per estimated glomerular filtration rate according to the manufacturers instructions . 314 patients were given co - trimoxazole 960 mg three times per week to prevent p jirovecii infection . 
a previous antibiotic prophylaxis study in patients with myeloma also reported no p jirovecii pneumonia in 212 patients , although twothirds of patients were not receiving co - trimoxazole.19 therefore , we conclude that the risk of p jirovecii pneumonia in patients with newly diagnosed myeloma is low and probably does not warrant routine treatment with prophylactic co - trimoxazole . 
however , the addition of a complementary antibiotic could be beneficial and should be investigated in future studies . the difference between our study and previous studies in patients with myeloma that reported no benefit for antibiotic prophylaxis might be due to the greater number of participants in the teamm trial and differences in the anti - myeloma treatments used . 
to our knowledge , the largest study to date took 10 years to recruit 212 patients and most of these patients did not receive novel anti - myeloma agents , although some received high - dose dexamethasone.19 our study recruited participants rapidly with broad entry criteria that allowed all forms of anti - myeloma treatment98% of our patient population received novel agents , which therefore reflects current practice . 
the use of total febrile episodes as a primary endpoint might also have contributed to a negative study , as previously discussed . the viral isolates reported in our study are probably an under - representation of viral infections , since taking specimens for viral identification was not routine practice in many district hospitals during the trial period . 
furthermore , there has been an increase in pneumococcal vaccination in the uk , with the 23 - valent polysaccharide pneumo coccal vaccine offered at 65 years of age since 2003 and herd immunity boosted by conjugate pneumococcal vaccines for children younger than 5 years with a seven - valent vaccine introduced in 2006 and 13 - valent vaccine introduced in 2010 . the perceived risks of increased carriage of antibioticresistant organisms and health care - associated infections were not evident in our study resultswe observed no increase in colonisation with antibiotic - resistant organisms or health care - associated infections in the levofloxacin groups , suggesting that there might be situations when the use of prophylactic antibiotics does not increase the carriage of antibiotic - resistant organisms . 
this observation is supported by large reviews and meta - analyses of prospective studies on antibiotic prophylaxis10 , 29 or selective digestive decontamination , 3032 which did not show increased carriage of resistant isolates com pared with placebo groups . 
our study group differs from previous studies because most patients were not admitted to hospital in our study . the main limitation of this study is the high number of withdrawals , despite the low toxicity . 
around half of the withdrawals occurred in the first 4 weeks , and the high numbers might reflect poor commitment of patients with newly diagnosed myeloma to a supportive care placebocontrolled trial , possibly because they prioritise focusing on disease control . 
myeloma xi33 was an open - label randomised trial of anti - myeloma therapies that ran concurrently with teamm , recruited at three times the rate of teamm , and had fewer withdrawals . 
a previous supportive care trial in patients with myeloma who received oral clodronic acid or placebo had higher withdrawal than the teamm trial ( 209 [ 39% ] of 536 patients ) .34 high withdrawal could be a feature of placebo - controlled supportive care trials and might require consideration in future recruitment targets . 
suspected drug toxic effects accounted for a quarter of withdrawals in the teamm trial and were balanced between the study groups , suggesting that perceived rather than actual toxic effects might have contributed to the large number of withdrawals . in summary , our study found a consistent benefit for the use of levofloxacin prophylaxis over 12 weeks in patients with newly diagnosed myeloma , without any increased in health care - associated infections . 
prolonged antibiotic prophylaxis after 12 weeks and combined 1770 vol 20 december 2019 articles antibiotic use for prophylaxis requires investigation in future studies . contributors mtd , sb , jad , tp , gi , gp , and ky originated the idea for the study and together with cth , ph , acw , and el were responsible for the study design , conduct of the trial , data collection , analysis , and write up . 
kk , hd , eb , jn , bh , al , gc , and mh were involved with the conduct of the trial , data collection , analysis , and write up . declaration of interests mtd reports personal fees from abingdon health , outside the submitted work . 
all other authors declare no competing interests . data sharing participant data is stored on a secure server at warwick clinical trials unit ( coventry , uk ) where each participant has been assigned a deidentified trial number . 
no identifiable data , such as name , address , hospital number , nhs number , date of birth , or any other identifying data , will be shared and should not be requested . 
any requests for access to the teamm trial data should be sent to the chief investigator ( m.t.drayson@bham.ac.uk ) who will inform the data custodians ( ie , warwick clinical trials unit ) and agreement will be made through the data access committee , which will comprise the principal investigators from the trial management group . 
for each data sharing request , it is essential that a proforma is completed that describes the purpose , scope , data items requested , analysis plan , and acknowledgment of the trial management tearequestors who are granted access to the data will be required to complete a data sharing agreement that will be signed by the requester , sponsor , and principal investigator ( s )  . 
the study protocol , statistical analysis plan , and consent forms are available upon request . acknowledgments this study was funded by the national institute for health research ( nihr ) health technology assessment programme ( grant no 08 / 116 / 69 )  . 
we thank the patients who were recruited into this study and their families , the clinicians and staff at each centre who looked after these patients , members of the independent trial steering committee chaired by mark wilcox , and members of the independent data monitoring committee ( anthony child , walter gregory , and tim boswell )  . 
the views expressed are those of the authors and not necessarily those of the uk national health service , the nihr , or the uk department of health . published online july 22 , 2019 s1470 - 2045 ( 19 ) 30416 - 4 see articles page 1273 garbay da , le cesne n , penel c , et al . 
j clin oncol 2009 ; 27 : 595864 . management of high - risk endometrial cancer : are we there yet ? endometrial cancer is a diverse disease that includes varying stages and histologies . 
as a result , the design , completion , and interpretation of large randomised trials comparing adjuvant therapies for this disease , even when well conducted and well analysed , is problematic . 
 this situation is especially true in the study of adjuvant therapy for advanced endometrial cancer , since many patients are diagnosed and treated surgically for early disease , with no indication for adjuvant treatment . the portec study group is to be commended for its work in refining the use of adjuvant therapy across various types of non - metastatic endometrial cancer . 
in the portec - 3 study , eligible patients included those with stages ii and iii and high - risk stage i endometrioid iiii serous and endometrial cancer and stages clear cell histologies.1 with more than 650 women enrolled , the combination of systemic chemotherapy and radiotherapy was shown to improve outcomes compared with radiotherapy alone . 
for example , 5 - year overall survival was 814% ( 95% ci 772858 ) with chemoradiotherapy versus 761% ( 716809 ) with radiotherapy alone ( adjusted hazard ratio [ hr ] 070 [ 95% ci 051097 ] , p = 0034 ) , and 5 - year failure - free survival was 765% ( 95% ci 715807 ) versus 691% ( 638738 ; hr 070 [ 052094 ] , p = 0016 )  . 
in the aftermath of these potentially practice - changing results , additional questions are raised . first , do these findings apply broadly to all subgroups included in the study ? in addition to the broad eligibility criteria of portec - 3 ( ie , different tumour stages and histologies ) , many clinicopathological variables have prognostic significance , such as tumour grade , depth of myometrial invasion , patient age , lymphovascular space invasion ( in the absence of positive lymph nodes ) , and the patients general condition . 
even within similar or identical subgroups , substantial differences exist among patients , such as extent of nodal dissection , which are potentially confounding variables . whether or not the results from portec - 3 are generally applicable across patient subgroups remains unknown . 
however , taking into account the statistical limitations of subgroup analyses , the therapeutic benefit of combined chemotherapy and radiotherapy ( vs radiotherapy alone ) appeared to remain confined to patients with stage iii disease and those with serous carcinomas of all stages . second , is chemotherapy alone a sufficient form of adjuvant therapy ? the gynecologic oncology group ( now nrg oncology ) did separate studies that overlap ( in terms of patient eligibility ) with portec 3 . 
in the nrg / gog 249 study , investigators randomly assigned high - risk patients with stage i and ii disease , including those with high - risk histologies , to chemotherapy plus vaginal cuff brachytherapy or pelvic radiotherapy with no chemotherapy . 
in the nrg / gog 249 study , the chemotherapy plus vaginal cuff brachytherapy group did not show improved overall survival or relapse - free survival compared with the group that received pelvic radiotherapy alone . 
however , the incidence of nodal failure was significantly higher in the absence of pelvic radiation therapy , and acute toxicity was greater in the vaginal cuff brachytherapy group.2 in the nrg / gog 258 trial , patients with stage iiiiva uterine cancer were randomly assigned to received adjuvant chemotherapy alone or combined chemotherapy with pelvic radiotherapy ( and para - aortic radiotherapy if nodal metastases were present )  . 
although recurrencefree survival and overall survival were not improved with the combined therapy , nodal and vaginal failures were significantly lower when radiotherapy was given.3 1192 vol 20 september 201 comment in these and other previous studies of adjuvant therapy within the portec - 3 eligibility groups , locoregional failure has been a notable and often predominant failure pattern in the absence of pelvic radiotherapy . the apparent complementarity of chemotherapy ( in limiting distant failure ) and radiotherapy ( in limiting local failure ) , is a consistent finding that is a reasonable basis for subsequent clinical investigation . 
several studies support the use of combined modality therapy rather than monotherapy.4 , 5 finally , is there a preferred way of combining chemotherapy with radiotherapy ? in both portec - 3 and nrg / gog 258 , the combined chemotherapy plus radiotherapy schedule was based on a phase 2 regimen piloted by the radiation therapy oncology group , rtog 9708.6 when nrg / gog 258 was designed , there was vigorous debate about the combined modality group , with various investigators favoring a sandwich regimen typically involving three cycles of chemotherapy , followed by involved - field radiotherapy , and then additional chemotherapy . 
however , multiple studies ( retrospective and prospective ) have demonstrated the safety and efficacy of the so - called sandwich approach.5 , 79 increasing evidence supports the use of upfront systemic therapy , when combined with radiotherapy , as a strategy to maximise both systemic and local control.10 many clinicians often use this regimen as a preferred adjuvant approach in locally advanced endometrial cancer . based on outstanding work done by the portec study group and others , we have made good progress in improving outcomes for women with high - risk and locally advanced endometrial cancers . 
however , we are not there yet . marcus randall department of radiation medicine , university of kentucky , lexington , ky 40536 , usa merand2@uky.edu i have received an honorarium from isoray medical within the past 2 years . copyright 2019 the author ( s )  . 
adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
gynecol oncol 2019 ; 153 : 4148 . the emerging role of pet - ct scan after radical prostatectomy : still a long way to go the management of biochemical recurrence after radical prostatectomy is a common challenge for urologists and radiation oncologists , because about 30% of patients have an increase in prostate - specific antigen ( psa ) concentrations after surgical treatment.1 however , the outcome of these patients is not always poor , varying substantially according to the site and the extent of recurrence.2 in this context , the role of imaging is of the utmost importance to establish the real burden of recurrent disease . 
the increasing use of pet - ct has led to a shift towards early detection of low - volume metastatic prostate cancer , 3 whereas several novel and promising pet tracers have been reported.4 however , no prospective clinical trials had tested the superiority of one tracer over the others in terms of diagnostic accuracy . published online july 30 , 2019 s1470 - 2045 ( 19 ) 30501 - 7 see articles page 1286 vol 20 september 201 9 1193 comment published online february 5 , 2020 s1470 - 2045 ( 19 ) 30857 - 5 see articles page 345 capivasertib inhibits a key pathway in metastatic breast cancer capivasertib in the pursuit of improved therapies for metastatic breast cancer , a succession of drugs have been approved that target a range of mechanisms . 
notable examples include the cdk4 / 6 inhibitors , such as palbociclib , abemaciclib , and ribociclib , several of which have been reported to confer a survival advantage upon addition to the selective oestrogen receptor degrader fulvestrant.1 , 2 inhibitor with is a potent pan - akt notable anti - proliferative activity in preclinical models.3 the pi3k / akt / mtor axis specifically has a central position in several pathways with key functions in promoting cell survival , growth , and proliferation . 
 substantial cross - talk between these pathways and mediators of oestrogen receptor signalling are well appreciated , and thus these mediators are logical targets in hormone - sensitive disease.4 previous attempts at inhibition of these downstream kinases are highlighted by the bolero - 2 trial , 5 which evaluated the addition of everolimus , a selective mtor inhibitor , to the aromatase inhibitor exemestane , and reported an improvement in progression - free survival but not in overall survival . 
 inhibition of pi3k , although particularly effective in patients with tumours with pik3ca mutations , has proved challenging owing to the toxicity profile of pi3k inhibitors.6 in the lancet oncology , robert jones and colleagues7 report a doubling of progression - free survival from 48 months ( 95% ci 3177 ) to 103 months ( 50132 ; hazard ratio 058 , 95% ci 039084 , p = 00044 ) with the addition of capivasertib to fulvestrant in oestrogen receptor - positive , her2 - negative , advanced breast cancer that had progressed or relapsed after treatment with an aromatase inhibitor . 
the addition of capivasertib to fulvestrant also increased the proportion of patients achieving an objective response by more than three times , to 29% ( compared with 8% with fulvestrant plus placebo )  . 
this benefit of the combination therapy was independent of pik3ca or pten alteration status , further highlighting the essential role of akt at the root of major intersecting signalling cascades . a combinatorial approach with agents targeting multiple converging sites along upregulated signalling pathways could potentially curb the development of resistance mechanisms . 
duration of response to therapy might be longer , although additive toxicities do remain a concern given the fundamental role that these kinases play in normal , non - cancerous cells . 
strategies with combinations of her2directed therapy might reveal a role for akt inhibition in the management of her2 - positive disease and triple - negative breast cancer , in which mutations in the pik3ca / akt / pten pathway occur in 1023% of tumours.8 , 9 two obvious questions that remain to be evaluated at this juncture are the possible first - line selection of capivasterib versus a cdk4 / 6 inhibitor and the everpresent question of drug sequencing . 
 although the overall survival data for capivasertib are not yet mature , the magnitude of improvement in outcomes between agents might shift current treatment standards . amb reports personal fees from eisai , myriad , merck , puma , genomic health , nanostring , biotheranostics , lilly , novartis , pfizer , celgene , agendia , bayer , genentech - roche , and astrazeneca , outside the submitted work . 
the effect of abemaciclib plus fulvestrant on overall survival in hormone receptor - positive , erbb2 - negative breast cancer that progressed on endocrine therapy monarch 2 : a randomized clinical trial . 
fulvestrant plus capivasertib versus placebo after relapse or progression on an aromatase inhibitor in metastatic , oestrogen receptor - positive breast cancer ( faktion ) : a multicentre , randomised , controlled , phase 2 trial . 
plos one 2015 ; 10 : e0141763 . adjuvant therapy for melanoma : how to choose ? compared with just 5 years ago , adjuvant therapy for stage iii melanoma has undergone a major transformation . 
immune checkpoint blockade and targeted therapies already approved in the metastatic stage iv melanoma setting have now been approved in the earlier adjuvant setting , providing long - awaited effective treatment options for patients for whom interferonalfa 2b was the mainstay of approved therapy since its approval in 1995.7 the decision about whether to prescribe a specific adjuvant therapy entails careful selection of patients on the basis of risk of disease relapse and likelihood of therapeutic efficacy , because , unlike in the metastatic setting , clinical response cannot be readily assessed , owing to the absence of measurable disease . in the lancet oncology , reinhard dummer and colleagues1 offer a large , comprehensive , exploratory , biomarker assessment study using patient samples and clinical outcomes from the phase 3 combi - ad trial , a double - blind , placebo - controlled study of adjuvant dabrafenib and trametinib versus two matching placebos in 870 patients with stage iii melanoma . 
in their study , they found low tumour mutational burden to have a strong association with favourable relapse - free survival in patients treated with targeted therapy versus placebo ( hazard ratio [ hr ] vs placebo 049 [ 95% ci 035068 ] , p < 00001 ) ; conversely , high tumour mutational burden seemed to identify a subset of patients showing little long - term efficacy with targeted treatment ( hr vs placebo 075 , 95% ci 044126 , p = 027 ) , especially when combined with an ( ifn ) gene expression signature lower than the median ( hr 088 [ 95% ci 040193 ] , p = 074 )  . 
these data contrast with a study of adjuvant pd - 1 therapy , 2 which showed more interferon favourable clinical outcomes in patients with high tumour mutational burden and concomitant ifn expression . 
 notably , biomarkers associated with response to braf and mek - targeted therapy did not involve amplifications in braf or examined mutations in the mapk pathway but rather apparent immune - related factors . although exploratory , as the authors acknowledge , and requiring prospective validation , data from this study provide a step towards identifying biomarkers that can guide clinicians in selecting the optimal therapy for patients with stage iii melanoma . 
the welcomed renaissance of new drug discovery for advanced melanoma has brought with it a multitude of unanswered questions with respect to optimal sequencing and selection of therapies , especially in patients whose tumours harbour a brafv600e / k mutation . 
although the eighth edition of the american joint commission on cancer staging system partitions patients with stage iii melanoma into further subgroups ( ad ) allowing for improved risk stratification , 3 much work remains for developing accurate prognostication models and nomograms for the individual patient . 
such efforts are already underway with prognostication tools incorporating clinical and other histological features beyond those already incorporated into the staging syste moreover , efforts towards gene expression profiling of the primary tumour and identifying new biomarkers of the tumour microenvironment that capture elements of the host immune response will no doubt further refine the accuracy of predicting the clinical behaviour of melanomas . published online january 30 , 2020 s1470 - 2045 ( 20 ) 30002 - 4 see articles page 358 vol 21 march 2020 comment digital oncology summary of international recommendations in 23 languages for patients with cancer during the covid - 19 pandemic patients with cancer are at high risk for serious illness and death from covid - 19 . 
their lives depend on their ability to receive medical care , but every visit to a health - care facility exposes them to the risk of contracting the virus ; therefore , concerns about getting infected might interfere with their continuity of care . 
in this difficult phase , these patients need guidance and support . professional guidance becomes of extreme importance for reducing the risk of contracting the virus , promoting patients safety , treatment , and compliance , and ameliorating patients stress . 
several medical centres and national and international oncology societies are attempting to provide guidance to patients , but their extent and content vary ; some national oncology societies have not provided any recommendations at all . 
we have developed an international scientific panel with the aim to review available guidelines from 63 oncology societies ( appendix p 2 ) and provide summarised comprehensive recommendations for patients with cancer . 
29 of 63 oncology societies provided some form of guidance for patients , either as their own recommendation statements or as a link to guidance from other societies ( we only considered links to guidelines written in the societys native language )  . 
as most patients worldwide do not speak english , the language of guidance delivery is a major barrier to the dissemination of recommendations in different countries ( figure )  . 
therefore , we have translated the summary of the comprehensive recommendations into 22 languages ( arabic , bulgarian , catalan , chinese , croatian , czech , dutch , english , french , german , greek , hungarian , italian , japanese , norwegian , polish , portuguese , romanian , serbian , slovenian , spanish , and swedish )  . 
this high risk is related to the immunosuppression caused by a variety of factors , such as the disease itself , low performance status , cachexia , and the effect of treatments ( surgery , chemotherapy , corticosteroids , radiotherapy , and bone marrow transplantation )  . 
the degree of immunosuppression depends on the type of cancer , the patients age , fitness , comorbidities , the type of therapy , and the time since last therapy . 
covid - 19 symptoms appear 214 days after exposure and include fever , cough , runny nose , sore throat , body aches , diarrhoea , and loss of smell or taste . 
immediate medical attention should be sought for more severe malay or bahasa , 61 marathi , 72 hindi , 72 persian , 57 english , 335 lahnda , 89 telgu , 74 vietnamese , 68 bengali , 189 turkish , 71 korean , 77 tamil , 69 javanese , 84 russian , 166 italian , 64 german , 78 french , 76 portuguese , 203 lahnda , 89 telgu , 74 vietnamese , 67 bengali , 189 turkish , 71 korean , 77 tamil , 69 javanese , 84 russian , 166 italian , 64 german , 78 french , 76 portuguese , 203 chinese , 1197 japanese , 128 urdu , 64 arabic , 242 spanish , malay or bahasa , 61 marathi , 72 hindi , 72 persian , 57 english , 335 chinese , 1197 japanese , 128 urdu , 64 arabic , 242 spanish , figure : number of people ( in millions ) whose native language is in the top 23 most spoken worldwide ( a ) comparison of the number of english speakers ( green ) with speakers of the remaining 22 languages ; the proportion of english speakers is 8% . 
 ( b ) number of people whose native language is covered by our multilanguage translation ( green ) ; the proportion of people able to access guidelines in their native language is 68% . published online may 13 , 2020 s1470 - 2045 ( 20 ) 30278 - 3 department of medical oncology , university hospital of ioannina , ioannina , greece ( d mauri ) ; department of medical oncology , the christie national health service foundation trust , manchester , uk ( k kamposioras ) ; department of radiotherapy / radiation oncology , university hospital of larissa , larissa , greece ( m tolia ) ; department of advanced radiation oncology , irccs sacro cuore don calabria hospital , verona , italy ( f alongi ) ; university of brescia , brescia , italy ( f alongi ) ; and blood and marrow transplant program , university of california san diego , la jolla , ca , usa ( d tzachanis ) dvd.mauri@gmail.com we declare no competing interests . 
patients with cancer should have a low threshold for seeking medical attention if they have any new symptoms . the second area of recommendation regards specific protocols or any special measure that people with cancer should take to avoid covid - 19 infection ( appendix p 6 )  . 
it should be worn when visiting a cancer centre or hospital . the third area of recommendation reflects on what to do if someone is symptomatic , and indicates to patients whether there are any vaccines , treatment , or dietary or other supplementations that are effective against covid - 19 infection ( appendix p 9 )  . 
patients with cancer should avoid people with a known exposure , infected asymptomatic people , and infected symptomatic people for at least 14 days and until their symptoms have resolved . 
there is no evidence that dietary interventions , complementary and alternative medicines , or supplements can treat or prevent covid - 19 . the fourth area of recommendation is related to mental health : guidance on managing anxiety and stress ( appendix p 11 )  . 
some suggestions to counteract these negative feelings include communication with friends and family , engaging in pleasant activities , meditation , yoga and physical exercise , eating healthily , avoiding excessive exposure to the news , and following good sleep hygiene . 
 patients who feel that they cannot cope with their stress should talk to their doctor . building trust between physicians and patients to enhance patients confidence in medical staff decisions and improve their compliance with medical advice is important , and is the fifth area of recommendation ( appendix p 13 )  . 
for all patients with cancer , the possibilities of delaying or holding treatment are being evaluated on a case - by - case basis , according to the overall clinical picture , the aggressiveness of the cancer , and the potential health risks from covid - 19 . 
 it is important that patients remain confident that their oncology teams are there to support thepatients need to be aware that a lot of misleading information circulates on the internet . 
the best sources of safe information online can be found on official websites provided by medical centres , oncology societies , and governments . finally , the sixth area of recommendation concerns the procedures at cancer centres ( appendix p 16 )  . 
patients and visitors who have symptoms or have been exposed to an infected person should not visit their cancer centre , but should first call their doctors office for further instruction . 
we believe that a summary of recommendations from different oncology societies across the globe and their multilanguage translation will provide useful guidance to patients and caregivers . * davide mauri , konstantinos kamposioras , maria tolia , filippo alongi , dimitrios tzachanis , on behalf of the international oncology panel and european cancer patient coalition collaborators vol 21 june 2020 members listed in the appendix 760 perspectives uk cancer care threatened by government incompetence on oct 6 , 2020 , in response to questions in parliament regarding cancer outcomes during covid - 19 , the uk health secretary , matt hancock , stated the best way to keep cancer services running is to suppress [ coronavirus ]  . 
cancer care cannot be put on hold ; cancer care during the pandemic should not be beyond the capacity of the uks ostensibly world - class health system ; and patients with suspected or prevalent cancer must not be denied timely access to care . the devastating effect of the first uk lockdown earlier this year on cancer screening , diagnosis , treatment , and supportive care has been widely documented . 
so far , an estimated 3 million people have missed cancer screenings , and between april and august , 2020 , suspected cancer referrals were down 350 000 compared with the same period in 2019 . 
delays in diagnosis and referral will indisputably lead to excess early cancer mortality ; although exact numbers are uncertain , upwards of 60 000 life - years could be lost during the next 510 years . 
early in the pandemic , most clinical cancer trials in the uk were halted , and although these are now starting to reopen , the impact on both novel treatment development and individual patient outcomes is incalculable . 
following loosening of the initial lockdown restrictions , referrals and treatment have returned to near - normal levels , but , with a second wave of covid - 19 looming , hancock admits that the ability of the national health service ( nhs ) to see patients for reasons other than covid - 19 is now once again at risk . 
it is incredulous that 9 months after the first case of covid - 19 in the uk , and despite ample data regarding the effect of covid - 19 policies on cancer care services , the uk governments solution during the impending second wave of covid - 19 over the winter , is to again reduce or pause cancer care , rather than to find answers to maintain services . 
other countries have managed to continue with provision of cancer care despite covid - 19 and will not have the devastating legacy the uk will endure in the years to come . 
for example , france has successfully handled workforce issues by drawing on a voluntary reserve force of medical professionals , and several countries , including australia and germany , have responded to localised outbreaks by coordinating the redistribution of medical resources . 
most notably , in new zealand , cancer treatment ( surgery , medical oncology , radiation oncology , and haematology ) continued during the covid - 19 lockdown and is still being provided at pre - covid - 19 levels . 
unfortunately , after years of austerity , the nhs entered the pandemic with fewer doctors , nurses , and capital assets than did health systems in many other highincome countries , which has severely hampered its ability to deal with the pandemic . fortunately , despite matt hancock and the uk governments incompetence , the nhs has been working hard under its own guidance to prepare differently for the second wave of covid - 19 . 
cancer research uk has set out additional recommendations for preserving high - quality cancer care , including ways to increase the workforce , harness new technologies , and other long - term ambitions for improvement . 
it is the governments responsibility to encourage and support nhs efforts , not undermine them with threats . governmental failures have contributed to a second wave of covid - 19failures in testing and track and trace strategy and implementation , inadequate attention to the vulnerability of care homes , insufficient guidance and support for school exams and reopenings , unequal application of lockdown measures , and high - profile flouting of safety rules have eroded public trust . 
hancock , and by extension , the uk government , have set up a false choice between covid - 19 and other life - threatening diseases ; the way forward must be to find an equitable and humane way to address both . 
however , in a brief four - page document outlining his health - care plans , the main points of focus are the immediate dismantling of the a ordable care act ( aca ) and a reduction in funding for medicaid and medicare . 
the most concrete point made in the document is that the free market should determine provision of health care , with insurers free to o er plans across state lines . 
he also calls for greater transparency on health - care costs , and explicitly stipulates that the us market should be open to cheaper drugs from international sources . the aca was introduced in an insurance - based system to enable the many millions of uninsured americans its access to health carean ambition that has been partially realised . 
while an attempted repeal of the aca now looks inevitable given trumps hardline stance and the republican partys control of both houses of congress , it should not be withdrawn until a workable substitute has been drawn up . 
although the aca is awedespecially implementation , rising premiums , decreasing coverage , and inability to provide cover for all noninsured americansit currently stands as the main barrier between poorer americans and the risk of either a premature death or being bankrupted by the worlds most expensive health - care systewhat is needed is strong , policy - driven leadership and a commitment of funds to tackle the fast - rising incidence of cancer and other non - communicable diseases in the american population . the lack of detail in trumps plans allows for exibility in their execution . 
 the lancet oncology drug approval by regulators : who watches the watchers ? randomised in this issue of the lancet oncology , ian tannock and colleagues discuss some important parameters controlled governing outcomes of trials . 
they note that this concept is , in part , a consequence of regulators such as the us food and drug administration and the european medicines agency requiring statistical signi cance versus a comparator for a speci c endpoint to license drugs , rather than an indication that a drug has greater clinical utility compared with those already available . 
also , drug approvals usually require full disclosure of toxicities to regulators , who then have the relevant data and in - house knowledge to undertake thorough meta - analyses across multiple trials to determine drug safety . 
while there is always a need to collect real - world data to ensure e cacy in an unselected patient population , these processes can sometimes lead to a duplication of e ort and a waste of taxpayers moneypublic grants and taxes fund agency operating costs and later analyses . 
 for regulatory agencies to truly serve the public that they are designed to protect , there should be greater transparency in the approval process , with approval being clearly made on clinical , not just statistical , e cacy . 
generic drugs ( or biosimilars ) might become newly available and the price of the originator rapidly falls ; therefore , in starting a pharmaceutical companies registration process at ema declines , or disappears altogether . 
the story of bisphosphonates as adjuvant treatment for early breast cancer roughly corresponds to this profile : convincing evidence coming mostly from academic studies , including the previously mentioned meta - analysis , arriving late to their goal , and also because of the good prognosis of the disease . academic groups have a important role in identifying treatment strategies that ultimately improve prognosis of patients.8 however , the results of academic trials might not translate into clinical practice , including in europe where country - level discussion about reimbursement for new drugs starts only after ema approval on request of pharmaceutical companies . 
 ema does allow for academic groups to act as medicine developers ; however , we suspect that either no or very few cancer drugs have been approved based on a request from the academic community . 
this situation is due to academic researchers leaving the agenda of registration trials to the pharmaceutical industry and not continuing to remain engaged through to the end of the drug development process . 
solving discrepancies between scientific recommendations and regulatory approval ( eg , in the case of bisphosphonates in early breast cancer ) should be a mission of academic researchers who contributed to developing scientific evidence . * francesco perrone , adriano gravina clinical trial unit , istituto nazionale per lo studio e la cura dei tumori irccs fondazione g pascale , naples 80131 , italy f.perrone@istitutotumori.na.it fp reports personal fees from bayer , janssen cilag , pierre fabre , astrazeneca , celgene , incyte , sandoz , bristol - myers squibb , ipsen , and eli lilly , outside of the submitted work . 
adjuvant denosumab in postmenopausal patients with hormone receptor - positive breast cancer ( abcsg - 18 ) : disease - free survival results from a randomised , double - blind , placebo - controlled , phase 3 trial . 
zoledronic acid combined with adjuvant endocrine therapy of tamoxifen versus anastrozol plus ovarian function suppression in premenopausal early breast cancer : final analysis of the austrian breast and colorectal cancer study group trial 12 . 
 j law med ethics 2019 ; 47 : 46567 . earlier diagnosis : the importance of cancer symptoms people diagnosed earlier with cancer are not only more likely to survive , but importantly also to have better experiences of care , lower treatment morbidity , and improved quality of life compared with those diagnosed late.1 efforts to improve earlier diagnosis of cancer are complex and multifaceted and have been at the forefront of international policy and charity ( eg , cancer research uk ) initiatives . 
these are attending cancer screening , which aims to detect cancer before it is symptomatic ( eg , mammography for breast cancer ) and presenting promptly to primary care with potential cancer symptoms . published online november 5 , 2019 s1470 - 2045 ( 19 ) 30658 - 8 see articles page 73 for be clear on cancer see on - cancer the fact that , in england , more than 90% of cancers are detected outside the three national screening programmes2 ( for cervical , breast , and bowel cancers ) highlights the importance of presenting promptly to primary care with potential cancer symptoms . 
in england , these campaigns come under the umbrella of be clear on cancer ; however , they are emulated across the world , including more recently in low - income and middle - income countries such as india , malaysia , and south africa . 
one challenge , which so far has remained largely unanswered , is whether these campaigns truly capture people with early - stage disease and thus provide a meaningful contribution to the early diagnosis effort . 
accumulating evidence vol 21 january 2020 comment shows that they increase public awareness , and the likelihood of visiting a doctor , being referred for investigations , and being diagnosed at an earlier stage of the disease.3 , 4 however , others have argued that the cancers detected are mainly advanced , 5 which would make awareness campaigns less worthy of the attention and investment they draw . in nearly 8000 patients and in their article in the lancet oncology , monica koo and colleagues6 present novel epidemiological evidence that tackles this issue head on . 
the data showed that the proportion of patients diagnosed with advanced disease ( ie , stage iv ) varied substantially by presenting sympto for example , a neck lump was associated with greater odds of advanced disease , while symptoms including abnormal mole , breast lump , post - menopausal bleeding , and rectal bleeding ( common symptoms that have already featured in public awareness campaigns ) were associated with lower odds of advanced disease . 
these findings provide support for the emphasis on factors that are important pre - presentation ( eg , knowledge of warning signs ) because understanding and responding to cancer symptoms can help to identify cancer before it has spread . koo and colleagues contribution is an essential jigsaw piece in the early diagnosis puzzle , although several questions remafor example , what symptoms should be featured ? who should the campaigns be targeted at ? what barriers ( other than poor knowledge of warning signs ) should they address ? how should the campaigns be evaluated ? it is also crucial to ensure campaigns do not serve to escalate persistent inequalities in cancer survival , 7 so understanding how barriers vary by sociodemographic characteristics including age , socioeconomic status , and ethnicity will be key . 
behavioural science has much to add here , in terms of identifying important barriers to symptomatic presentation such as worry about wasting a doctors time , fatalism , and fear , as well as designing appropriately tailored interventions or campaigns to address these barriers.8 in the readiness to their findings also have important implications for referral health - care professionals because prompt and investigation of potential cancer symptoms post - presentation is another step in ensuring timely diagnosis . 
research shows that international variation exists investigate or refer to secondary care for suspected cancer symptoms , and countries where health - care professionals demonstrate greater readiness observe the highest cancer survival rates.9 finallya message for policy makersadvocating more people going to the doctor , more referrals , and more investigations means it is imperative that health - care systems have a well equipped and well funded workforce to deal with this core and essential activity . although answers to many of these challenges will require an ongoing multidisciplinary and international effort , early diagnosis is likely to remain the holy grail of cancer care . 
with this in mind , it is reassuring and bolstering to see that global approaches to cancer control are on the right track . katriina whitaker school of health sciences , university of surrey , guildford , gu27xh , uk k.whitaker@surrey.ac.uk i declare no competing interests . copyright 2019 the author ( s )  . 
bmj 2018 ; 360 : k764 . vol 21 january 2020 comment m published online december 11 , 2019 s1470 - 2045 ( 19 ) 30715 - 6 see articles page 80 8 moriarty y , townson j , quinn - scoggins h , et al . 
improving cancer symptom awareness and help - seeking among adults living in socioeconomically deprived communities in the uk using a facilitated health check : a protocol for the awareness and beliefs about cancer ( abacus ) randomised control trial . 
bmj open 2015 ; 5 : e007212 . the role of self - management in cancer survivorship care is now earlier diagnosis of many cancers as well as more effective treatments are substantial contributors to increasing cancer survival . 
in 2016 in the usa alone , there were an estimated 155 million cancer survivors , with this number expected to increase to 203 million by 2026.1 cancer largely recognised as a chronic condition , and survivors continue to experience myriad symptoms , as well as late effects , well beyond the end of their cancer treatment . 
the challenges of delivering survivorship care through already overburdened health systems have increased our focus on research examining the acceptability , cost , and effectiveness of alternative models of follow - up care , such as follow - up care jointly provided with the patients general practitioner , with evidence of their effectiveness as well as acceptability to patients.2 another area gaining substantial research attention is self - management , in particular , equipping survivors with the skills and knowledge to manage the myriad cancer - related and treatment - related consequences.3 , 4 the paper by anja van der hout and colleagues in the lancet oncology5 reports the results of a randomised controlled trial evaluating the efficacy , reach , and usage of a fully automated self - management intervention oncokompas . 
although the key finding of the study was that oncokompas was not effective in improving the level of knowledge , skills , and confidence for self - management among cancer survivors ( difference in patient activation measure at 6 months 17 [ 95% ci 08 to 42 ] , p = 041 ) , this is possibly the largest randomised controlled trial ( n = 625 cancer survivors ) of self - management interventions reported in the literature to date and hence , contributes to that evidence base in a meaningful way . 
unlike previous studies , most of which focused on women with breast cancer , 3 the study by van der hout and colleagues5 included a range of survivors with prevalent and less prevalent solid and non - solid tumour types ( head and neck cancer , colorectal cancer , breast cancer , hodgkin lymphoma , and non - hodgkin lymphoma )  . 
this study therefore contributes substantial new knowledge on the reach and usage of self - management by a broader population of cancer survivors . supporting survivors to self - manage their symptoms and quality of life requires an understanding of the optimal timing for delivery of self - management interventions . 
self - management resources provided early in the cancer pathway might be more beneficial , longer - term survivors will probably have as many already found the information and support they need to build their skills and confidence to manage cancerrelated concerns . 
in the study in the lancet oncology , 5 only approximately half ( 167 [ 52% ] of 320 ) of the intervention group used the self - management platform at least once during the 6 - month follow - up period , and this group had a higher attrition rate ( 60 [ 19% ] participants withdrew from the study ) than the control group ( 36 [ 12% ] participants )  . 
the pilot work that informed this randomised controlled trial and which showed great promise for oncokompas , was done with survivors who were approximately 14 months post - diagnosis , so it is perplexing that the randomised controlled trial included a sample of predominantly much longer - term survivors . 
 as the authors suggested , the intervention might have been more beneficial if presented earlier . however , longer - term cancer survivors have unmet needs too and many will experience late effects of their vol 21 january 2020 comment correction to lancet oncol 2016 ; 17 : 28798 yock ti , yeap by , ebb dh , et al . 
 lancet oncol 2016 ; 17 : 28798 in this article , the curves for the intermediate - high - risk patients in figures 2 and 3 were incorrect and have been updated . 
this correction has been made to the online version as of march 2 , 2020 . vol 21 march 2020 e132 corrections fulvestrant plus capivasertib versus placebo after relapse or progression on an aromatase inhibitor in metastatic , oestrogen receptor - positive breast cancer ( faktion ) : a multicentre , randomised , controlled , phase 2 trial robert h jones * , angela casbard * , margherita carucci , catrin cox , rachel butler , fouad alchami , tracie - ann madden , catherine bale , pavel bezecny , johnathan joffe , sarah moon , chris twelves , ramachandran venkitaraman , simon waters , andrew foxley , sacha j howell summary background capivasertib ( azd5363 ) is a potent selective oral inhibitor of all three isoforms of the serine / threonine kinase akt . 
the faktion trial investigated whether the addition of capivasertib to fulvestrant improved progressionfree survival in patients with aromatase inhibitor - resistant advanced breast cancer . methods in this randomised , double - blind , placebo - controlled , phase 2 trial , postmenopausal women aged at least 18 years with an eastern cooperative oncology group performance status of 02 and oestrogen receptor - positive , her2 - negative , metastatic or locally advanced inoperable breast cancer who had relapsed or progressed on an aromatase inhibitor were recruited from 19 hospitals in the uk . 
enrolled participants were randomly assigned ( 1 : 1 ) to receive intramuscular fulvestrant 500 mg ( day 1 ) every 28 days ( plus a loading dose on day 15 of cycle 1 ) with either capivasertib 400 mg or matching placebo , orally twice daily on an intermittent weekly schedule of 4 days on and 3 days off ( starting on cycle 1 day 15 ) until disease progression , unacceptable toxicity , loss to follow - up , or withdrawal of consent . 
treatment allocation was done using an interactive web - response system using a minimisation method ( with a 20% random element ) and the following minimisation factors : measurable or non - measurable disease , primary or secondary aromatase inhibitor resistance , pik3ca status , and pten status . 
at the time of primary analysis for progression - free survival ( jan 30 , 2019 ) , 112 progression - free survival events had occurred , 49 ( 71% ) in 69 patients in the capivasertib group compared with 63 ( 89% ) of 71 in the placebo group . 
median progression - free survival was 103 months ( 95% ci 50132 ) in the capivasertib group versus 48 months ( 3177 ) in the placebo group , giving an unadjusted hazard ratio ( hr ) of 058 ( 95% ci 039084 ) in favour of the capivasertib group ( two - sided p = 00044 ; one - sided log rank test p = 00018 )  . 
 serious adverse reactions occurred only in the capivasertib group , and were acute kidney injury ( two ) , diarrhoea ( three ) , rash ( two ) , hyperglycaemia ( one ) , loss of consciousness ( one ) , sepsis ( one ) , and vomiting ( one )  . 
one further death in the capivasertib group had an unknown cause ; all remaining deaths in both groups ( 19 in the capivasertib group and 31 in the placebo group ) were disease related . interpretation progression - free survival was significantly longer in participants who received capivasertib than in those who received placebo . 
 the only other randomised phase 2 study of akt inhibition in patients with oestrogen receptor - positive , her2 - negative breast cancer showed no advantage of addition of capivasertib to paclitaxel chemotherapy . 
these studies have shown pan - pi3k and beta - sparing inhibitors to have an unfavourable toxicity profile and low clinical activity , and they are no longer in development for this indication . 
mtor inhibition with everolimus has shown activity , again at the cost of substantial toxicity , but the effect is agnostic to perturbation of the pi3k pathway . added value of this study to our knowledge , this study is the first randomised trial to report on the addition of an akt inhibitor to endocrine therapy in oestrogen receptor - positive metastatic breast cancer after previous aromatase inhibitor therapy . 
the results showed an improvement in progression - free survival and response rate with addition of capivasertib to endocrine therapy , suggesting synergy , in contrast to the poor efficacy in combination with chemotherapy . 
adverse events were common , but manageable with dose reduction , and did not seem to compromise efficacy . implications of all the available evidence several approaches to targeting the pi3k / akt / mtor pathway have been shown to be effective in metastatic oestrogen receptor - positive , her2 - negative breast cancer in combination with endocrine therapy . 
the intermittent scheduling of capivasertib in this study contrasts with the continuous treatment with pi3k and mtor inhibitors in the majority of previous publications , potentially resulting in improved tolerability . 
the faktion data support further investigation of akt inhibition with capivasertib in combination with fulvestrant in a phase 3 trial . identified , including alteration of the pi3k / akt pathway . 
 this pathway is altered in more than 50% of oestrogen receptorpositive advanced breast cancers , most frequently through somatic hotspot mutation in exons 9 and 20 of pik3ca , encoding the p110 isoform of pi3k.14 less frequently , pathway alteration is induced by loss of function mutation or deletion of the negative regulator pten or activating mutations in akt1 . 
pi3k pathway alteration is associated with endocrine therapy resistance through ligand inde pendent activation of the oestrogen receptor.5 , 6 conversely , preclinical data show compensatory increases receptor transcription following pi3k pathway inhibition.79 a rationale therefore exists for simultaneously targeting both the oestrogen receptor and pi3k pathways . liganddependent oestrogen reported several clinical improved trials have progressionfree survival with inhibitors of the pi3k pathway in combination with endocrine therapies . 
distal inhibition with the mtorc1 inhibitor everolimus improved progressionfree survival in combination with the aromatase inhibitor exemestane irrespective of the alteration status of the pi3k pathway , albeit at the cost of additional toxicity.3 , 10 by contrast , proximal pathway inhibition with the pi3ksubunit specific inhibitor alpelisib significantly enhanced the efficacy of fulvestrant , but only in tumours harbouring pik3ca hotspot mutations.11 this finding has led to selected approval for alpelisib , in combination with fulvestrant , in this specific subgroup of patients with oestrogen receptorpositive advanced breast cancer . 
an unmet need therefore remains for patients whose tumours do not carry pik3ca hotspot mutations . capivasertib ( azd5363 ) is a potent and selective inhibitor of the three akt isoforms . 
preclinical data show synergistic activity with fulvestrant in both endocrinesensitive and endocrineresistant models of oestrogen receptorpositive breast cancer.12 preliminary clinical activity was seen with capivasertib monotherapy in heavily pretreated patients with akt1mutant solid cancers , including oestrogen receptorpositive breast cancer , but very low singleagent activity in patients with pik3camutant breast and gynaeco logical cancers.13 , 14 in the phase 2 beech trial , capivasertib did not enhance the efficacy of paclitaxel in oestrogen receptorpositive advanced breast cancer , although endocrine therapy was not permitted in this study as is standard practice.15 in a phase 1b study , we determined the capivasertib dose to be used in combination with fulvestrant was 400 mg twice daily for 4 days then 3 days off in a weekly schedule.16 in the phase 2 faktion trial , we assessed the efficacy and safety of capivasertib plus fulvestrant in post menopausal women with aromatase inhibitorresistant , oestrogen receptorpositive , her2negative advanced or metastatic breast cancer . 
furthermore , the relative efficacy of the treatment combination in participants with and without alteration of the pi3k pathway was assessed . 346 vol 21 march 2020 articles see online for appendix methods study design and participants we did an investigatorinitiated , multicentre , randomised , doubleblind , placebocontrolled , biomarkeradaptive , phase 2 trial , in which patients were enrolled from 19 hospitals in the uk ( appendix p 20 )  . 
eligible patients were post menopausal women aged at least 18 years with locally confirmed oestrogen receptorpositive , her2 negative metastatic or locally advanced inoperable breast cancer and eastern cooperative oncology group performance status of 02 . 
participants cancers were required to have relapsed on or within 12 months of adjuvant aromatase inhibitor therapy or have progressed on an aromatase inhibitor in the metastatic setting ( although this did not need to be the most recent therapy )  . 
 primary resistance was defined as either disease relapse during or within 6 months of completing aromatase inhibitor treatment in the adjuvant setting , or disease progression within 6 months of starting aromatase inhibitor treatment and no response to aromatase inhibitor treatment in the metastatic setting . 
secondary resistance was defined as disease relapse more than 6 months after completion of aromatase inhibitor treatment in the adjuvant setting , or disease progression following achievement of clinical benefit with aromatase inhibitor treatment in the meta static setting . 
 participants were required to have a life expectancy of at least 12 weeks and adequate organ function ( absolute neutrophil count 10 10 per l ; platelet count 100 10 per l ; haemoglobin 9 g / dl ; international normalised ratio 15 ; potassium , calcium [ corrected for serum albumin ] , and magnesium within normal limits for the institution ; serum creatinine 15 times the upper limit of normal ; alanine aminotransferase and aspartate amino transferase 15 times the upper limit of normal [ or < 30 times if liver metastases ] ; total bilirubin 15 times fasting glucose the upper < 70 mmol / l )  . 
key exclusion criteria included previous treatment with fulvestrant or inhibitors of the pi3k / akt pathway , and clinically significant abnormalities of glucose meta bolis participants with well controlled type 2 diabetes with an hba1c of less than 42 mmol / mol limit of normal ; and ( < 8% ) and fasting blood glucose of less than 93 mmol / l could participate following a protocol amendment on june 11 , 2015 . 
a further protocol amendment on feb 27 , 2017 , was implemented to allow women with previous malignancy , in remission for at least 5 years , and those with bilateral oophorectomy ( to define menopause ) to participate . 
protocol deviations are outlined in the appendix ( p 4 ) , as are the full inclusion and exclusion criteria ( appendix pp 21116 )  . written , informed consent was obtained from all participants before trial screening procedures and enrolment . 
the trial was done in accordance with the principles of good clinical practice , the declaration of helsinki , and uk clinical trial regulations . randomisation and masking participants were randomly assigned ( 1 : 1 ) to receive fulvestrant plus capivasertib or fulvestrant plus placebo . 
 randomisation was done centrally , using minimisation with a 20% random element.17 minimisation factors were measurable versus nonmeasurable disease , pri mary versus secondary resistance to a thirdgeneration aromatase inhibitor , pik3ca mutation status ( mutated vs wildtype ) , and pten expression status ( null vs detected in 1% of tumour cells at moderate or strong intensity or 10% of cells at weak intensity )  . 
 participants were assigned sixdigit trial numbers and treatment groups and a confirmatory email including the participants trial number , initials , date of birth , and treatment kit numbers was sent to the investigator . 
participants , investigators , study site staff , and sponsor were masked to treatment assignment until database lock . procedures participant blood and tissue samples were obtained after consent and centrally tested at the all wales medical genetics service and the department of cellular pathology , university hospital of wales , cardiff , uk , for pik3ca and pten alteration status before random isation . 
if there was an incomplete dataset at the time of randomisation , the patient could still be randomly assigned using the unobtainable category . fulvestrant 500 mg was administered on day 1 of every cycle as two intramuscular injections , one into each buttock , and an additional loading dose was delivered at cycle 1 day 15 . 
capivasertib 400 mg or matching placebo was given orally twice daily on an intermittent weekly vol 21 march 2020 articles 183 patients assessed for eligibility at screening 38 ineligible 34 did not meet inclusion criteria 2 declined to participate 2 reasons missing 5 ineligible 2 for poor cardiac function 2 for abnormal liver function 1 her2 positive 145 consented and registered 140 eligible and randomly assigned 69 assigned to fulvestrant plus capivasertib 71 assigned to fulvestrant plus placebo 60 discontinued 51 owing to clinical disease progression or death 8 owing to intolerance to treatment due to toxicity and serious adverse events 1 reason missing 69 discontinued 67 owing to clinical disease progression or death 1 participant choice 1 reason missing 69 included in primary analysis 47 cases of recist progression 71 included in primary analysis 61 cases of recist progression 2 deaths ( counted as progression - free 2 deaths ( counted as progression - free survival event ) 2 deaths ( censored ) 7 active at data lock ( censored ) 11 lost to follow - up ( censored ) survival event ) 2 deaths ( censored ) 1 active at data lock ( censored ) 5 lost to follow - up ( censored ) figure 1 : trial profile schedule of 4 days on and 3 days off , starting on cycle 1 day 15 ( to facilitate testing of biomarkers before randomisation )  . 
fulvestrant and capivasertib were manu factured and provided by astrazeneca ( cambridge , uk ) and distributed by fisher clinical services ( horsham , uk )  . participants were reviewed in clinic for toxicities and laboratory monitoring on day 1 of every cycle , at the end of treatment , and 30 days after treatment . 
blood was drawn for analysis of sodium , potassium , urea , creatinine , albumin , alanine transaminase or aspartate transaminase , alkaline phos phatase , bilirubin , calcium and full blood count on day 1 of every cycle ( and day 15 of cycle 1 ) to cycle 7 and every three cycles thereafter . 
random blood glucose sampling followed the same pattern , but was replaced with fasting blood glucose on cycle 1 day 15 , cycle 2 day 1 , and cycle 3 day 1 . 
participants performed home urine dipstick for glucose on the third day of capivasertib or placebo dosing each week . participants completed drug diaries , which were returned to the study site at each study visit to aid data collection . the incidence and severity of adverse events and serious adverse events were recorded throughout the study period with haematological and biochemical laboratory tests recorded every 4 weeks . 
toxicities suspected to be related to capivasertib were managed by dose interruption or dose reduction to 320 mg , then 240 mg , then 160 mg at the same schedule . 
dose reduction of fulvestrant to 250 mg was allowed after discussion with the chief investigators if an investigator felt that unacceptable toxicity could reasonably be attributed to fulvestrant or if there were physical difficulties with administration of bilateral injections . ct scans of the chest , abdomen , and , if indicated , pelvis were done within 28 days before registration to confirm eligibility , and repeated every 8 weeks until cycle 7 , then every 12 weeks until disease progression . 
scans were assessed according to recist by local radiologists , without central review , to determine tumour response and date of progression . baseline pten status was assessed centrally at the university hospital wales cellular pathology department ( cardiff , uk )  . 
the first section was stained with haematoxylin and eosin to identify the area of greatest tumour density and tumour percentage , and the rest was made available for dna extraction and whole section immunohistochemistry . 
immunohistochemistry was prepared using dako ( ely , uk ) pten monoclonal mouse antihumanclone ( code m3627 ) , with antigen retrieval done with high ph dako target retrieval solution and the dako autostainer link 48 automated strainer with a predetection dilution of 1 : 100 . 
the the pten validation study and full protocol for immunohistochemistry detection have been published previously.18 the pten protein expression was docu mented using a numeric intensity score of the cyto plasmic staining in comparison with the surrounding stroma and macrophages ( 0 : null ; 1 : weak ; 2 : moderate ; and 3 : strong )  . 348 vol 21 march 2020 articles fulvestrant plus capivasertib group ( n = 69 ) fulvestrant plus placebo group ( n = 71 ) median age , years ( iqr ) ; range 62 ( 5568 ) ; 4281 61 ( 5368 ) ; 4082 eastern cooperative oncology group performance status ( physical examination ) 2 ( 23 ) ; 15 15 ( 22% ) 54 ( 78% ) 2 ( 13 ) ; 15 19 ( 27% ) 52 ( 73% ) the protocol definition of pten loss , for inclusion of a patient in the altered pathway subgroup , was either immunohistochemistry 0 or weak pten staining in less than 10% of cancer cells . baseline pik3ca mutational status was assessed centrally at the all wales genetics laboratory ( cardiff , uk )  . 
 cellfree dna was extracted using the qiagen ( hilden , germany ) qiaamp circulating nucleic acids kit ( 55114 )  . the protocol specified that pathway alteration was defined as either a hotspot mutation detected by digital droplet pcr ( ddpcr ) on pik3ca exons 9 or 20 in tumour tissue or blood or an immuno histochemistry null status for pten in tumour tissue ( primary tumour or metastatic biopsy )  . 
secondary endpoints were overall survival ( defined as the time from randomisation to death from any cause ) , the proportion of ( defined as objective response participants with a complete or partial response , according to recist version 1.1 ) and clinical benefit ( defined as the proportion of participants with an objective response or stable disease lasting 24 weeks )  . 
analysis of the effect of pi3k pathway alteration on these outcomes was planned prospectively and subgroup analyses of progressionfree survival , overall survival , and objective response by pi3k pathway alteration were additional secondary outcomes . 
also evaluated were tolerability and feasibility of the regimen , as shown by the number of participants discontinuing or requiring dose modifi cations ; fulvestrant pharmac okinetics , specifically whether capivasertib affected trough fulvestrant concentrations ; and safety , defined as the frequency and severity of adverse events reported during followup . a more extensive , preplanned , exploratory biomarker analysis is currently underway , and when completed , the results will be published in a followup paper . statistical analysis the hypothesis was that participants treated with fulvestrant plus capivasertib would have improved the assumption median progressionfree survival compared with those treated with fulvestrant plus placebo . 
the sample size was calculated for a phase 2 screening design , based on a primary outcome of progressionfree survival , assuming a timetoevent hazard ratio of 065 , 90% power , a one sided alpha of 020 , and an overall loss to followup of 10%.19 under the estimated progressionfree survival in the control group would be 54 months , a total of 98 events were required in 138 participants with 18month accrual and 6month minimum followup . 
if recruitment was restricted to participants with pik3ca mutations , 70 events in 98 participants would be required to provide 90% power to detect a hazard ratio of 06 in favour of the combination of fulvestrant with capisavertib . that an interim analysis of change in tumour size 8 weeks after randomisation in the first 40 participants without pathway alteration was planned to allow adaptation of recruitment according to participants pathway alteration status . 
this approach was designed to look for an early futility signal in the nonaltered participant group and to determine whether the trial should continue only in patients with tumours harbouring an altered pathway . 
this analysis showed that activity in the non altered group exceeded the prespecified threshold and the independent data monitoring committee determined that recruitment should remain open to all patients regardless of pathway alteration tumour status . efficacy analyses for progressionfree survival were done in the full analysis set , comprising all randomly assigned patients , on an intentiontotreat basis . 
participants without disease pro gression confirmed by recist and those who died or progressed after missing the last two recist assess ments were censored for progressionfree survival at the date of the last evaluable recist assessment or at the point of withdrawal of consent . 
 the proportion of patients with objective response and clinical benefit was summarised by trial group and analysed using logistic regression . two posthoc analyses were done to calculate the progressionfree survival of participants allocated to 350 vol 21 march 2020 articles capivasertib who discontinued or reported a dose reduction and the duration of response ( defined as the time from first documented objective response to the first documented progression or death ) for participants with measurable disease in both the capivasertib and placebo groups . 
the cofunder ( cancer research uk ) approved the study design , but had no role in the drafting of the report , or data collection , analysis , or interpretation . 
additionally , ac and cc had full access to the raw data . results between march 16 , 2015 , and march 6 , 2018 , 183 patients were screened for eligibility and 140 were randomly assigned to receive fulvestrant plus capivasertib ( n = 69 [ 49% ] ) or fulvestrant plus placebo ( n = 71 [ 51% ] ; figure 1 )  . 
 treatment groups were well balanced for baseline characteristics ( table 1 )  . ( 71% ) at the time of primary analysis , there had been 112 progressionfree survival events : 49 69 patients in the capivasertib group compared with 63 ( 89% ) in 71 in the placebo group . 
median progressionfree survival was 103 months ( 95% ci 50132 ) in the capivasertib group versus 48 months ( 3177 ) in the placebo group , giving an unadjusted hazard ratio ( hr ) of 058 ( 95% ci 039084 , 2sided p = 00044 ) and an adjusted hr of 058 ( 039085 , 2sided p = 00049 ; figure 2 ) in favour of fulvestrant plus placebo fulvestrant plus capivasertib hr 058 ( 95% ci 039084 ) ; p = 00044 time since randomisation ( months ) 71 ( 0 ) 29 ( 6 ) 19 ( 7 ) 8 ( 8 ) 4 ( 8 ) 1 ( 8 ) 1 ( 8 ) 0 ( 8 ) 0 ( 8 ) 69 ( 0 ) 38 ( 7 ) 28 ( 10 ) 13 ( 14 ) 8 ( 17 ) 5 ( 18 ) 2 ( 19 ) 0 ( 20 ) 2 ( 20 ) number at risk ( number censored ) fulvestrant plus placebo fulvestrant plus capivasertib figure 2 : progression - free survival hr = hazard ratio . the capivasertib plus fulvestrant group . 
the trial , therefore , met its primary endpoint . 99 ( 71% ) participants had measurable disease ( 49 in the capivasertib group and 50 in the placebo group )  . 
median progressionfree survival with the combination of fulvestrant and capivasertib was significantly longer than in the placebo group , both in patients with measurable disease ( 76 months [ 95% ci 48105 ] vs 32 months [ 3177 ] ) with a hr of 061 ( 95% ci 039095 , p = 0030 ) and those with nonmeasurable disease ( 134 months [ 95% ci 77301 ] vs 79 months [ 44108 ] ) with a hr of 047 ( 95% ci 022099 , 2sided p = 0046 )  . 20 ( 29% ) of 69 in the capivasertib group achieved an objective response compared with six ( 8% ) of 71 in the placebo group ( odds ratio [ or ] 442 , 95% ci 1651184 , 2sided p = 00031 )  . 
38 ( 55% ) of 69 in the capivasertib group had clinical benefit versus 29 ( 41% ) of 71 in the placebo group ( or 178 , 95% ci 091347 , 2sided p = 0093 )  . 20 ( 41% ) of 49 participants with measurable disease in the capivasertib group had an objective response compared with six ( 12% ) of 50 in the placebo group ( or 506 , 95% ci 1811411 , 2sided p = 00020 )  . 
in a posthoc analysis , the median duration of response in patients with measurable disease was 71 months ( 95% ci 3899 ) for participants in the capivasertib group and 50 months ( 27 to not reached ) for participants in the placebo group ( appendix p 5 )  . assessing the relative efficacy of capivasertib plus fulvestrant in participants with pi3k / pten pathway altered tumours versus those with nonaltered tumours was a prespecified objective of the trial . 
 59 ( 42% ) of 140 tumours were designated altered ( 31 [ 45% ] of 69 in the capivasertib group and 28 [ 39% ] of 71 in the placebo group ) and 81 ( 58% ) nonaltered ( 38 [ 55% ] of 69 in the capivasertib group and 43 ( 61% ) of 71 in the placebo group )  . 
the combined result of sequential analysis of plasma and tissue and the change to ddpcr led to a conversion from nonaltered to altered status in 21 participants ; 12 ( 17% ) of 69 patients in the capivasertib group and nine ( 13% ) of 71 patients in the placebo group were converted from nonaltered to altered , and three ( 4% ) in the capivasertib group and four ( 6% ) in the placebo group were converted from altered to nonaltered . in the pi3k / pten pathway nonaltered group , median progressionfree survival was 103 months ( 95% ci 32132 ) in the capivasertib group and 48 months ( 3086 ) in the placebo group . 
in the altered group , median progressionfree survival was 95 months ( 95% ci 66137 ) in the capivasertib group and 52 months ( 3184 ) in the placebo group ( figure 3 )  . 
 the significant improvement in progressionfree survival seen with fulvestrant and capivasertib versus placebo in the overall population was preserved in the nonaltered group ( 056 , 033096 , p = 0035 ) , but not in patients with pi3k / pten pathway altered ( 059 , 034103 , p = 0064 )  . 
in participants with measurable disease , nine ( 47% ) of 19 participants with pathway alteration in the capivasertib group had an objective response compared with two ( 11% ) of 19 in the placebo group ( or 765 , 95% ci 1374271 , 2sided p = 0020 )  . 
 in patients without pathway alteration , 11 ( 37% ) of 30 in the capivasertib group had an objective response compared with four ( 13% ) of 31 in the placebo group ( or 391 , 95% ci 1081414 , 2sided p = 0038 )  . tumours overall survival data are immature with a median followup for survival of 12 months ( iqr 617 )  . 
the median overall survival was 260 months ( 95% ci 184323 ) in the capivasertib group and 200 months ( 151212 ) in the placebo group with a hr of 059 ( 95% ci 034105 , 2sided p = 0071 ; figure 4 )  . 
in the nonaltered group , median overall survival was 237 months ( 95% ci 168 to not reached ) in the capivasertib group and 203 months ( 133234 ) in the placebo group ( hr 062 , 95% ci 030128 , 2sided p = 020 )  . 
in the altered group , median overall survival was 305 months ( 95% ci 176 to not reached ) in the capivasertib group and 187 months ( 95% ci 141212 ) in the placebo group ( hr 053 , 95% ci 021133 , 2sided p = 017 )  . the median duration of fulvestrant treatment was 92 months ( iqr 30141 ) in the capivasertib group compared with 46 months ( 28105 ) in the placebo group . 
the median duration of capivasertib treatment itself was slightly shorter than that of fulvestrant in the combined group at 77 months ( iqr 15135 ) due to discontinuation of capivasertib before disease progression in eight ( 12% ) patients . 
the median duration of placebo administration was 49 months ( iqr 23106 )  . overall , 28 ( 41% ) of 69 patients in the capivasertib group had a capivasertib dose reduction compared with one ( 1% ) of 71 in the placebo group ; more specifically , 22 had one , five had two , and one had three capivasertib dose reductions . 
of these eight participants , rash was reported in six , diarrhoea in three , and hypoglycaemia , nausea , vomiting , mouth ulcers , and sweating in one each . 
serious adverse reactions ( reported only in the capivasertib group ) were acute kidney injury ( two ) , diarrhoea ( three ) , hyperglycaemia ( one ) , loss of consciousness ( one ) , rash ( two ) , sepsis ( one ) , and vomiting ( one ; appendix p 7 )  . 
one death in the capivasertib treatment group had an unknown cause , and all remaining deaths in both groups ( 19 in the capivasertib group and 31 in the placebo group ) were disease related . in the pharmacokinetic analysis , there was no apparent difference in trough fulvestrant concentrations between participants assigned to capivasertib and those receiving placebo ( appendix p 19 )  . discussion the results of this study show that the addition of capivasertib to fulvestrant therapy significantly improved progressionfree survival in participants with oestrogen receptorpositive her2negative breast cancer that had progressed on an aromatase inhibitor . 
the trial met its primary objective and , to our knowledge , is the first study to show the efficacy of an akt inhibitor combined with fulvestrant in this setting . 
however , pi3k pathway alteration status , predefined in the protocol as pik3ca hotspot mutation in exons 9 or 20 or pten null by immunohistochemistry , did not seem to change the effect size of capivasertib , although there was not enough statistical power within the subgroups to confirm this finding . 
extended followup and a larger phase 3 study will be required to determine whether the trend for improved survival with capivasertib in faktion is a genuine finding . fulvestrant plus placebo fulvestrant plus capivasertib hr 059 ( 95% ci 034105 ) ; p = 0071 number at risk ( number censored ) fulvestrant plus placebo fulvestrant plus capivasertib time since randomisation ( months ) 71 ( 0 ) 69 ( 0 ) 57 ( 12 ) 56 ( 12 ) 44 ( 22 ) 42 ( 20 ) 24 ( 32 ) 24 ( 34 ) 14 ( 36 ) 13 ( 41 ) 3 ( 39 ) 9 ( 43 ) 2 ( 39 ) 5 ( 45 ) 2 ( 39 ) 0 ( 48 ) 0 ( 40 ) 0 ( 48 ) figure 4 : overall survival censored patients are marked on the curves with a vertical dash . 
the mtorc1 inhi bitor everolimus significantly improved progressionfree survival in combination with exemestane , 10 which was independent of pik3ca mutation and pi3k pathway alteration status.3 however , this improvement was at the expense of an increase in toxicity and overall survival was not significantly improved . 
two trials have shown significant improvements in progressionfree survival with everolimus versus placebo in combination with fulvestrant , although the relative benefits by pi3k pathway status are yet to be reported.20 , 21 the activity of the specific pi3k inhibitor , alpelisib , in combination with fulvestrant was confined to patients whose tumours harboured pik3ca mutations.11 therefore , the role of pathway alter ation in determining drug efficacy could be dependent on the specific target and its position in the pathway . the faktion data also contrast with the reported activity of capivasertib or ipatasertib ( another panakt inhibitor ) in combination with paclitaxel in the pakt22 and lotus23 studies in metastatic triplenegative breast cancer . 
both studies reported a significant improvement in progressionfree survival in the overall population , but the benefit was predominantly recorded in tumours with activating mutations in pik3ca or akt1 or inacti vating alterations in pten.22 , 23 however , deficient pten expression is a more frequent alteration in triplenegative breast cancer than in oestrogen receptorpositive , her2 negative breast cancer and is associated with increased akt pathway activation , 24 , 25 suggesting that the relative benefit of akt inhibition is context dependent . 
one patient in the treatment group had a grade 5 haemorrhage . 1 ( 1% ) 1 ( 1% ) of mutational status , provides a rational basis for effectiveness of the investigational combination beyond a mutant population . the pattern of adverse events observed with capivasertib was consistent with other pi3k / akt pathway inhibitors , with diarrhoea , rash , and hyperglycaemia being the most 354 vol 21 march 2020 articles prevalent . 
quality of life was not assessed in this phase 2 study , but will be key in future studies to assess the effect of such management strategies . the treatment environment is changing for patients with oestrogen receptorpositive , her2negative meta static breast cancer . 
cdk4 / 6 inhibitors are now routinely used in combination with aromatase inhibitors as first line therapy with improvements in overall survival.26 , 27 the value of continued cdk4 / 6 inhibition after pro gression is being tested in several clinical trials , but new , improved options are clearly needed in this setting . 
 notably , reduction or loss of pten has been implicated in resistance to both endocrine28 and cdk4 / 6 inhibitor therapy , 29 with such cancers responding to akt inhibition but not alphaspecific pi3k inhibition . 
elucidation of biomarkers of activity of akt inhibition in this population remains a research priority ; however , based on the results of the faktion trial , capivasertib is an attractive candidate for further development in this disease setting . analysis of efficacy by pathway alteration was limited to hotspot mutation detection in exon 9 and 20 of pik3ca as well as pten status by immunohistochemistry . 
 when the study was designed , akt1 mutation was reported in only 14% of oestrogen receptorpositive breast cancers ; 1 , 2 thus akt1 testing was not part of the original protocol . 
akt1 mutations have been identified in 67% of oestrogen receptorpositive breast cancer metastases , 3 and a more comprehensive biomarker analysis , including mutational status of all akt isoforms , is underway on faktion samples . 
the full dataset will inform future trial design and will help to identify the patient population with the greatest potential of benefit from capivasertib treatment . a strength of the study was the randomised nature of this phase 2 trial , which means that , although of modest size , it provides a rationale for a subsequent phase 3 trial . 
the design does increase the risk of obtaining a falsepositive result ; however , we were willing to accept this given that a phase 3 confirmatory trial was planned if there was a positive result . 
third , the modest size of the study did not allow meaningful subgroup analyses , such as for boneonly or visceral disease , but these should be evaluated in subsequent studies . 
 preclinical data suggest that akt inhibition might be superior to pi3k inhibition in this setting , 29 but formal confirmation of this theory in a randomised trial is required . that in conclusion , faktion met its primary outcome in showing the combination of fulvestrant and capivasertib is tolerable and produces a significant improvement in progressionfree survival for partici pants with advanced oestrogen receptorpositive her2negative breast cancer who have previously progressed on an aromatase inhibitor . 
these data indicate that capivasertib is active in combination with fulvestrant and provide the basis for a confirmatory phase 3 study . contributors rhj , sjh , ac , and af were responsible for study design , and rhj , sjh , ac , and mc for writing of the manuscript . 
rhj , sjh , cb , pb , jj , sm , ct , rv , and sw were responsible for patient accrual , trial conduct , and obtaining the data . 
all authors interpreted the data and reviewed the draft and final versions of the manuscript . declaration of interests the study sponsor ( vellindre ) and cardiff university are negotiating a contract with astrazeneca for exclusive access to the trial data . 
 rhj reports grants from astrazeneca and cancer research uk , during the conduct of the study , and personal fees from merck serono and roche , outside the submitted work . 
only requests that have scientifically and methodologically sound proposals will be considered and the usage vol 21 march 2020 articles of the shared trial data or supporting material will be limited to the approved proposal . 
the final decision as to whether data or supporting material might be shared and the exact data or supporting material to be shared will be made between the sponsor , trial team , and astrazeneca . 
 capivasertib ( azd5363 ) was discovered by astrazeneca after a collaboration with astex therapeutics ( and its collaboration with the institute of cancer research and cancer research technology limited )  . 
the trial management group contributed to the article revision . comment published online august 12 , 2016 s1470 - 2045 ( 16 ) 30365 - 5 see articles page 1363 leaky transporters and sphincters in barretts oesophagus ? barretts oesophagus is a metaplastic epithelial condition caused by chronic gastro - oesophageal re ux that predisposes to development of oesophageal adenocarcinoma . 
barretts oesophagus and oesophageal adenocarcinoma are not often thought of as hereditary diseasesie , a positive family history of either disease in rst - degree relatives or probands is usually not obtained.1 however , since these diseases could be polygenic locus contributing only weakly to disease development , clinical family history might underestimate the hereditary genetic component . 
estimates suggest that 24% of cases of oesophageal adenocarcinoma are hereditary and 76% are sporadic , 2 whereas up to 35% of cases of barretts oesophagus have a hereditary genetic component.3 therefore , several research groups have sought to identify disease loci using genome - wide association studies . 
in a review and meta - analysis of existing data , 9 17 germline markers of susceptibility to barretts oesophagus were identi ed , in addition to ve somatic markers of neoplastic progression and one marker of relapse after photodynamic therapy . in the lancet oncology , puya gharahkhani and the barretts and esophageal colleagues adenocarcinoma consortium ( beacon ) , the esophageal from adenocarcinoma genetics consortium ( eagle ) , and the wellcome trust case control consortium 2 ( wtccc2 ) 10 report their attempts to systematically prioritise genetic loci by doing a meta - analysis of all publicly available data from genome - wide association studies . 
nine new loci were identi ed from this meta - analysis , which were within or near the genes cftr , msra , linc00208 and blk , khdrbs2 , tppp and cep72 , tmod1 , satb2 , htr3c and abcc5 , and lpa . 
furthermore , for the rst time , a risk locus speci c to oesophageal adenocarcinoma and independent of risk for barretts oesophagus was foundrs9823696 , close to htr3c and abcc5 . relaxation of the muscular a pathway analysis showed an association of loci with muscle - cell di erentiation , these nine which is relevant because barretts oesophagus and oesophageal adenocarcinoma are caused proximally by defective lower locus with the oesophageal sphincter . 
gastro - oesophageal re ux has been associated with cystic brosis and is considered part of its phenotypic spectru thus , this particular locus is a candidate that potentially links two common syndromes previously thought to be unrelated . 
the cftr protein belongs to the atp - binding cassette ( abc ) class of transporters that transmits ions across cell membranes ; its defective function ( leakyie , permitting defective ion transport ) is pathogenic in patients with cystic brosis . 
 this association could represent a new area of research into the pathogenesis of barretts oesophagus and oesophageal adenocarcinoma . leaky link the research by gharahkhani and colleagues provides some much - needed perspective on the wealth of data now accumulating in this area of medicine . 
even if not proven to be disease causing , loci highlighted by this study might become valuable , singly or in aggregate , for the risk strati cation of patients re ux disorder , barretts with gastro - oesophageal 1336 vol 17 october 2016 comment published online september 1 , 2016 s1470 - 2045 ( 16 ) 30441 - 7 see articles page 1374 oesophagus , or perhaps those at risk of either of these two syndromes . 
moreover , if one or more of these variants prove to have a pathophysiological role in barretts oesophagus or oesophageal adenocarcinoma , they could become pivotal in the design of novel preventative or therapeutic strategies . stephen j meltzer the johns hopkins university school of medicine , baltimore , md 21287 , usa smeltzer@jhmi.edu i declare no competing interests . 
dig dis sci 2016 ; 61 : 2538 . 10 gharakhani p , fitzgerald rc , vaughan tl , et al , and the barretts and esophageal adenocarcinoma consortium ( beacon ) , the esophageal adenocarcinoma genetics consortium ( eagle ) , and the wellcome trust case control consortium 2 ( wtccc2 )  . 
 checkpoint inhibitors : a new standard of care for advanced merkel cell carcinoma ? merkel cell carcinoma represents a rare group of cutaneous malignancies , which typically develop in the sun - damaged skin of elderly individuals and often in immunosuppressed patients.1 locally advanced and metastatic merkel cell carcinoma have a grave prognosis , and until recently , the european inter - disciplinary consensus - based guidelines recommended clinical trials as a standard of care.2 however , in reality , patients with advanced merkel cell carcinoma receive platinum - based chemotherapies , which have a limited and short - lived clinical e cacy . 
 in the lancet oncology , howard kaufman and colleagues4 report results from a phase 2 study in which 88 patients with advanced merkel cell carcinoma were treated with the pd - l1 - blocking antibody avelumab . 
 eight ( 9% ) patients achieved a complete response and 20 ( 23% ) patients achieved a partial response.4 all patients had histologically con rmed stage iv ( advanced ) disease and had documented progression following at least one previous line of chemotherapy in the metastatic setting . 
tolerability of avelumab was excellent , with only one permanent treatment discontinuation.4 two patients discontinued treatment because of adverse e ects . these results in patients heavily pre - treated with chemotherapy indicate that avelumab has a high potential to change clinical practice in this aggressive cutaneous malignancy and led the us food and drug administration to award avelumab a breakthrough therapy designation for the treatment of metastatic merkel cell carcinoma in november , 2015 . 
there are vol 17 october 2016 1337 comment published online june 20 , 2016 s1470 - 2045 ( 16 ) 30150 - 4 see articles pages 1047 and 1061 hypofractionation for prostate cancer : tested and proven fractions of in the lancet oncology , results of two randomised phase 3 trials of hypofractionationie , fewer , larger , radiotherapeutic treatmentfor daily prostate cancer are reported.1 , 2 in the nal results from the conventional or hypofractionated high - dose intensity modulated radiotherapy in prostate cancer ( chhip ) trial , david dearnaley and colleagues advocate for hypofractionation , 1 whereas in the nal results from the hypofractionated irradiation for prostate cancer ( hypro ) trial , luca incrocci and colleagues recommend that hypofractionation not be adopted.2 how can we explain this apparent discordance ? the short explanation is that the two trials have di erent hypotheses . that what some postulated is the rationale for hypofractionation prostate cancer ? in 1999 , brenner and hall claimed that the fractionation sensitivity of prostate cancer was such that appropriately designed hypofractionation schemes would be expected to maintain current levels of tumor control and late sequelae...with the logistical and nancial advantages of fewer numbers of fractions.3 as a result , investigators across the globe designed prospective trials to test the hypofractionation hypothesis in prostate cancer . 
trials took two forms depending on the nature of the hypothesis : a superiority design or a non - inferiority design . investigators hypofractionation would increase e cacy compared with conventional fractionation , which in retrospect was an overinter pretation of brenner and halls paper . 
the increase in acute6 and late7 gastrointestinal and genitourinary toxic e ects recorded with the hypofractionation regimen used in hypro should temper enthusiasm for this fractionation schedule . comparing two hypofractionation other , perhaps more cautious , investigators designed trials with a non - inferiority hypothesis . 
 chhip is a large ( n = 3216 ) , three - arm , non - inferiority trial regimens ( 600 gy delivered as 20 fractions of 30 gy , ve fractions per week ; and 570 gy delivered as 19 fractions of 30 gy , ve fractions per week ) with a conventionally fractionated regimen ( 740 gy as 37 fractions of 20 gy , ve fractions per week ) .1 most patients enrolled in chhip had low - risk or intermediate - risk disease , although 12% had high - risk disease . 
after a median follow - up of 624 months ( iqr 539770 ) , 5 - year biochemical or clinical failure - free rates were 906% ( 95% ci 885923 ) in patients allocated the 600 gy hypofractionation schedule compared with 859% ( 834880 ) in those assigned the 570 gy hypofractionation schedule and 883% ( 860902 ) in those fractionation . 
the 600 gy hypofractionation schedule was judged non - inferior to the conventional regimen of 740 gy ( hr 084 , 90% ci 068103 ; pni = 00018 ) ; however , non - inferiority of the 570 gy hypofractionation schedule could not be claimed ( 120 , 099146 ; pni = 048 )  . 
results of the non - inferiority nrg oncology 0415 trial have also been reported.8 after a median follow - up of 58 years , researchers concluded that hypofractionation ( 28 fractions of 25 gy , ve fractions per week ) was non - inferior to conventional fractionation ( 41 fractions of 18 gy , ve fractions per week ) in men with low - risk prostate cancer ( hr for the primary endpoint of 5 - year disease - free survival 085 , 95% ci 064114 ) , which conventional allocated 1020 vol 17 august 2016 comment met the prede ned non - inferiority criterion ( critical hr < 152 )  . 
findings of a large non - inferiority trial of 1200 patients ( profit ; nct003046759 ) , comparing 600 gy hypofractionation ( the same regimen as in the chhip trial ) with 780 gy conventional fractionation are awaiting publication ( catton c , princess margaret cancer centre , personal communication )  . it is noteworthy that the hrs for the primary endpoint in the nrg oncology ( 085 ) and chhip ( 084 ) trials are similar . 
this consistency is noted despite the inclusion of patients with di erent risk groupings , varying durations of androgen suppression ( ranging from none to 6 months ) , and diverse radiotherapy regimens . 
these ndings together should reassure skeptical practitioners that hypofractionation can be introduced without a decrease in e cacy . sooner with hypofractionation on the other hand , the ndings of the non - inferiority studies are somewhat inconsistent with respect to toxic e ects . 
researchers on the nrg oncology trial also noted a slight increase in late grade 2 gastrointestinal and genitourinary toxic e ects , but no di erences in severe toxic e ects were recorded.8 the observation of increased late toxic e ects is perhaps not surprising , because the biological e ective dose of the hypofractionated regimen in nrg oncology 0415 ( 1280 gy ) is slightly greater than that of the hypofractionated regimen in chhip ( 1200 gy ) , assuming the / ratio of rectum and bladder to be 30 gy . and low - risk intermediate - risk including brachytherapy to put these results into context , it is important to acknowledge that there are several other radioin use for men therapeutic approaches currently prostate with rate cancer , and high - dose selected patients . 
preliminary results of extreme hypofractionation schedules ( four or ve fractions of rate ) , and active surveillance ( low - dose 70100 gy ) have been reported , 10 but no data from randomised trials of stereotactic body radiotherapy have been published up to now . 
although not technically stereotactic body radiotherapy , this trial is probably the closest comparison of extreme hypo fractionation with conventional fractionation that we will have in the short terevidence to support stereotactic body radiotherapy is growing but remains weak ( in quality and quantity ) compared with more moderate hypofractionation schedules . 
 in view of these reports , should radiation oncologists routinely abandon conventional fractionation and move to hypofractionation ? i do not think so ; i agree with the hypro investigators that the hypofractionation regimen used in their study ( 19 fractions of 34 gy ) should not be adopted . 
on the other hand , the results from nrg oncology 04158 and chhip1 suggest that hypofractionation will not result in any loss of e cacy and could make treatment less expensive and more convenient for patients when compared with conventionally fractionated radiotherapy . 
the nrg oncology trial investigators did note a slight increase in clinician - reported grade 2 gastrointestinal and genitourinary toxic e ects , and practitioners might use this nding as justi cation not to adopt this particular hypofractionation schedule , particularly in patients with large prostates or clinically signi cant pre - existing urinary dysfunction . 
i expect that future ancillary analyses of the nrg oncology study will de ne the appropriate dose constraints to keep grade 2 gastrointestinal and genitourinary toxic e ects low , as we learned with dose - escalation studies of conventional fractionation . 
 excess toxic e ects , however , were not recorded with 600 gy in 20 fractions in the chhip trial ; 1 the results of the profit trial will provide more information on the 4 - week schedule . 
conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
hypofractionated versus conventionally fractionated radiotherapy for patients with localised prostate cancer ( hypro ) : nal e cacy results from a randomised , multicentre , open - label , phase 3 trial . 
hypofractionated radiotherapy versus conventionally fractionated radiotherapy for patients with intermediate - risk localised prostate cancer : 2 - year patient - reported outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
radiother oncol 2013 ; 109 : 21721 . the case for informative phase 2 trials in osteosarcoma and high osteosarcoma is the most common malignant tumour of the bone but only ve cytotoxic chemotherapy drugsdoxorubicin , dose cisplatin , methotrexate ( map ) , and ifosfamide and etoposide have been shown to be of bene t . 
10 - year overall survival is about 60% and has not changed in more than 30 years.1 consequently , it is imperative to explore the activity of novel agents in osteosarcoma with the goal of improving outcome and , ultimately , if outcome is su ciently improved and a low - risk group can be identi ed , decreasing treatment - related morbidity . 
 in the lancet oncology , sophie piperno - neumann and colleagues2 present the results of os2006 , a randomised trial of zolendronate in addition to chemotherapy in newly diagnosed osteosarcoma . 
unfortunately , the trial showed an absence of improvement in 3 - year event - free survival in the zolendronate plus chemotherapy group ( 571% [ 95% ci 488650 ] ) compared with the chemotherapy alone group ( 634% [ 552709 ] , hr 136 [ 95% ci 095196 ] ; p = 0094 )  . 
as a consequence of the non - restrictive eligibility , there was heterogeneity in the evaluable population ; patients could have localised , possible , or de nite metastatic disease , axial or appendicular primary tumours , and metastatic sites restricted to the lung or in other sites . 
although sensitivity analyses support the authors conclusion that a negative trial result is not due to imbalances in the randomised population , it is preferable for outcome analysis to be restricted to a homogeneous patient population . heterogeneity of the patient population and the duration needed to enrol a su cient number of patients emphasise the importance of international collaboration for the undertaking of phase 3 trials in osteosarcoma . 
 the euramos - 1 trial enrolled 2260 patients over 6 years and outcome analyses were done in a homogenous patient population showing the feasibility in phase 3 trials of osteosarcoma.3 , 4 unfortunately , euramos - 1 , which tested the e ect on event - free survival of the addition of ifosfamide and etoposide to map in high - risk patients and the addition of interferon to map in low - risk patients , showed no bene t to either intervention.5 international cooperation os2006 and euramos - 1 show that a collaborative e ort and a 510 year time investment is required to do de nitive phase 3 trials in osteosarcoma . 
in view of 1022 vol 17 august 2016 clinical characteristics , outcomes , and risk factors for mortality in patients with cancer and covid - 19 in hubei , china : a multicentre , retrospective , cohort study kunyu yang * , yuhan sheng * , chaolin huang * , yang jin * , nian xiong * , ke jiang * , hongda lu * , jing liu , jiyuan yang , youhong dong , dongfeng pan , chengrong shu , jun li , jielin wei , yu huang , ling peng , mengjiao wu , ruiguang zhang , bian wu , yuhui li , liqiong cai , guiling li , tao zhang , gang wu summary background patients with cancer are a high - risk population in the covid - 19 pandemic . 
we aimed to describe clinical characteristics and outcomes of patients with cancer and covid - 19 , and examined risk factors for mortality in this population . methods we did a retrospective , multicentre , cohort study of 205 patients with laboratory - confirmed severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) infection and with a pathological diagnosis of a malignant tumour in nine hospitals within hubei , china , from jan 13 to march 18 , 2020 . 
risk factors for mortality were identified by univariable and multivariable logistic regression models . findings between jan 13 and mar 18 , 2020 , 205 patients with cancer and laboratory - confirmed sars - cov - 2 infection were enrolled ( median age 63 years [ iqr 5670 ; range 1496 ] ; 109 [ 53% ] women )  . 
patients with haematological malignancies had poorer prognoses than did those with solid tumours : nine ( 41% ) of 22 patients with haematological malignancies died versus 31 ( 17% ) of 183 patients with solid tumours ( hazard ratio for death 328 [ 95% ci 156691 ] ; log rank p = 00009 )  . 
multivariable regression analysis showed that receiving chemotherapy within 4 weeks before symptom onset ( odds ratio [ or ] 351 [ 95% ci 1161059 ] ; p = 0026 ) and male sex ( or 386 [ 95% ci 157950 ] ; p = 00033 ) were risk factors for death during admission to hospital . interpretation patients with cancer and covid - 19 who were admitted to hospital had a high case - fatality rate . 
it spread rapidly across the world during the following few weeks.1 , 2 as of may 27 , 2020 , 5 491 678 cases have been confirmed worldwide , with 349 190 deaths.3 , 4 in wuhan , the initial centre of the epidemic , 50 340 covid - 19 cases and 3869 deaths have been confirmed , as of may 26 , 2020.5 patients with cancer are a vulnerable population during the covid - 19 pandemic . 
therefore , they are at increased risk of opportunistic infections , developing severe complications , requiring admission to an intensive care unit ( icu ) , or even death.69 liang and colleagues10 analysed data from 18 patients with cancer , from a sample of 1590 patients with covid - 19 , and found a higher risk of covid - 19 and poorer outcomes in patients with cancer than in those without . 
large studies are needed to comprehensively describe the characteristics and outcomes of patients with cancer and covid - 19 . we collected and analysed data from patients with cancer and covid - 19 who were admitted to nine local hospitals in hubei , china . 
recent studies have shown that receiving antitumour treatments and patchy consolidation on ct scans were associated with development of severe events in covid - 19 ( requiring admission to the intensive care unit , the use of mechanical ventilation , or death )  . 
 however , we found no published multicentre study with a large sample size discussing clinical characteristics , outcomes , and risk factors of mortality of patients with cancer and a confirmed diagnosis of covid - 19 . diagnosed with covid - 19 , and to identify risk factors associated with in - hospital mortality . methods study design and participants this retrospective , multicentre , cohort study was led by wuhan union hospital ( wuhan , china )  . 
the list of participating hospitals is as follows : cancer center of wuhan union hospital , west branch of wuhan union hospital , jin yin - tan hospital , wuhan red cross hospital , the central hospital of wuhan , huanggang central hospital , the first peoples hospital affiliated to yangtze university , xianning central hospital , and suizhou central hospital ( appendix p 1 )  . 
diagnosis of covid - 19 followed who interim guidance.12 from jan 13 to march 18 , 2020 , we enrolled 205 patients with a history of cancer , irrespective of when the cancer had been diagnosed . 
 the inclusion criteria were strictly based on pathological diagnosis of a malignant tumour and laboratory confirmation of sars - cov - 2 infection ; patients clinically diagnosed with covid - 19 were excluded . 
 the presence of sars - cov - 2 infection was confirmed by rt - pcr and next - generation sequencing analysis of samples collected from nasopharyngeal swabs.4 , 13 we aimed to explore the clinical characteristics and outcomes of patients with covid - 19 who had malignant tumours . 
there was no formal determination added value of this study in this retrospective , multicentre , cohort study , we report demographic , clinical , laboratory , and radiological findings , as well as treatments and outcomes , for 205 patients with cancer and laboratory - confirmed severe acute respiratory distress syndrome coronavirus 2 ( sars - cov - 2 ) infection in hubei , china . 
 receiving chemotherapy within 4 weeks before symptom onset , and male sex were risk factors for death during admission to hospital . implications of all the available evidence patients with cancer are a vulnerable population with a higher case - fatality from covid - 19 than the general population . 
 male patients with cancer and those receiving chemotherapy within 4 weeks before symptom onset might require additional medical attention and supportive care once diagnosed with covid - 19 , as they appear to be at increased risk of in - hospital mortality . 8161 patients diagnosed with covid - 19 in electronic medical record system from nine hospitals in hubei , china , between jan 13 and march 18 , 2020 248 patients with a history of a tumour identied from the electronic medical record system 21 patients excluded 12 with benign tumours 9 without pathological conrmation 22 patients without laboratory conrmation of sars - cov - 2 infection excluded 205 patients included in the study figure : study profile sars - cov - 2 = severe acute respiratory syndrome coronavirus 2 . of sample size and all patients meeting the inclusion criteria were recruited . 
the cutoff date for our study was april 20 , 2020 . ethics approval was obtained from the ethics committee of wuhan union hospital , tongji medical college , huazhong university of science and technology , wuhan , china , at the beginning of the study . 
data on spo were missing for 17 patients . table 1 : demographics and baseline characteristics of patients with cancer and covid - 19 data collection we obtained information about demographic data , clinical manifestations , cancer histories , laboratory findings , chest ct examinations , treatments , and outcomes of all enrolled patients from electronic medical records and patients interviews . 
based on the tnm staging system , cancer stage was defined as early ( iii ) or late ( iiiiv ) stage for solid tumours ( staging information for brain cancer was not recorded )  . 
we also recorded information about treatments ( administration of anti biotics and for covid - 19 antivirals , oxygen therapy , and mechanical ventilation ) , compli cations , and outcomes during admission to hospital . definitions acute respiratory distress syndrome was defined according to the berlin definition.15 acute heart failure , acute kidney injury , septic shock , and secondary infection were defined according to previous studies.13 leucocytosis was defined as a white blood cell count of more than 10 cells per l . 
 * stroke , acute heart failure , myocardial ischaemia , electrolyte disturbance , and other complications . table 3 : treatments and complications of patients with cancer and covid - 19 00012 045 00014 069 094 034 0014 < 00001 < 00001 00011 < 00001 < 00001 00039 00004 < 00001 < 00001 < 00001 00001 < 00001 < 00001 00034 statistical analysis we hypothesised that differences exist in demographic , clinical , and laboratory characteristics , treatments , and cancer history between survivors and non - survivors of covid - 19 with cancer . 
quantitative variables were presented as medians ( iqr ) , and qualitative vari ables were presented by frequencies and percentages ( only available data were calculated )  . the mann - whitney u test , fishers exact test , test , and yates continuity correction were applied to analyse the differences between groups according to the type of data . 
we chose receiving chemotherapy within 4 weeks before symptom onset as the cutoff according to the number of patients within groupings and the significance of the logistic regression analysis ( appendix p 1 )  . 
for the multivariable logistic regression analysis , we chose four variables to avoid overfitting of the regression model because of the small number of endpoint events ( n = 40 ) in our research . 
variable selection was based on significance from the univariable logistic regression analysis ( p < 005 ) , the correlation between indicators , basic baseline clinical characteristics , and the accuracy and availability of data . 
other laboratory tests , including creatinine , lactate dehydrogenase , creatine kinase , d - dimer , interleukin - 6 , and c - reactive protein can be unavailable in emergency situations . 
the time period of hospital admission was not included because some patients might have been admitted to other hospitals and been given treatment ( eg , antibiotics , antiviral medication , oxygen therapy ) before they were transferred to the current hospital . 
therefore , receiving chemotherapy within 4 weeks before symptom onset , cancer type ( solid vs haematological ) , time since cancer diagnosis , and sex were chosen in our multi variable logistic regression model . 
the differences between groups were considered to be significant when the p value was less than 005 . role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication . results from jan 13 to march 18 , 2020 , 227 patients with cancer were screened from 8161 patients with covid - 19 admitted to nine hospitals in hubei province . 
184 ( 90% ) of 205 patients were identified from among the 6485 patients admitted to five hospitals designated for patients with covid - 19 in the city of wuhan . 
among 8161 patients with covid - 19 , 205 ( 25% ) had cancer . of the 205 patients with cancer included ( table 1 ) , 40 ( 20% ) had died as of april 20 , 2020 , and 34 ( 18% ) of 184 patients in wuhan city had died . 
no significant differences in age and other comorbidities were observed between survivors and non - survivors . data for abnormal blood cell counts in the 203 patients for whom these data were available included 25 ( 12% ) cases of leucocytosis , 54 ( 27% ) of leucopenia , 32 ( 16% ) of neutro penia , 102 ( 50% ) of lymphocytopenia , and 25 ( 12% ) of thrombocytopenia ( table 2 )  . 
129 ( 70% ) of 185 patients had elevated concentrations of d - dimer , 115 ( 60% ) of 192 patients had elevated concentrations of c - reactive protein , and 78 ( 49% ) of 160 patients had increased lactate dehydro genase . 
compared with survivors ( table 2 ) , non - survivors had higher nlr and higher concentrations of creatinine , blood urea nitrogen , lactate dehydrogenase , creatine kinase , d - dimer , c - reactive protein , procalcitonin , and interleukin - 6 , and lower lymphocyte and platelet counts , and albumin and calcium concentrations . of the 205 patients included , 144 ( 70% ) received intravenous antibiotics and 192 ( 94% ) received antiviral medications ( table 3 )  . 
compared with survivors ( table 3 ) , non - survivors were more likely to receive intravenous medication ( antibiotics , immunoglobulin , or corticosteroids ) , receive oxygen therapy , require mechanical ventilation , be transferred to the icu , and develop complications such as acute respiratory distress syndrome , secondary infection , acute renal failure , and septic shock ( table 3 )  . 38 ( 20% ) of 192 patients had been diagnosed with cancer within the past year , and 20 ( 12% ) of 162 patients had an ecog score higher than 1 before admission . 
54 ( 30% ) of 182 patients received antitumour therapy within 4 weeks before symptom onset , and 15 ( 8% ) of 182 received more than one treatment , including seven ( 4% ) of 182 who received both chemotherapy and targeted therapy . 
 910 vol 21 july 2020 articles the case - fatality rate in patients with haematological malignancies was 41% ( nine of 22 patients ) and that in solid tumours was 17% ( 31 of 183 patients ; hr 328 [ 95% ci 156691 ] ; log rank p = 00009 ; appendix p 3 )  . 
for example , two of three patients with multiple myeloma died ; case - fatality rates were lower for patients with breast cancer , thyroid cancer , and cervical cancer . we did a comparative analysis of clinical characteristics , treatments , laboratory data , and radiological data from patients with solid tumours and those with haematological malignancies ( appendix pp 46 )  . 
patients with haematological malignancies were younger than those with solid tumours ( median age 55 years [ iqr 2662 ] vs 64 years [ 5770 ] ) , and most ( 15 [ 68% ] of 22 ) were male . 
 [ 27% ] of acute respiratory distress syndrome ( six 22 patients vs 17 [ 10% ] of 177 patients ) and coagulopathy ( five [ 23% ] of 22 patients vs 13 [ 7% ] of 177 patients ) were more frequently seen in patients with haematological malig nancies than in those with solid tumours . 
14 ( 70% ) of 20 patients with haematological malignancies received antitumour treatments in the past 4 weeks before symptom onset , compared with 40 ( 25% ) of 162 patients with solid tumours . 
11 ( 55% ) of 20 patients with haematological malignancies and 20 ( 12% ) of 162 patients with solid tumours received chemotherapy within 4 weeks before symptom onset . in univariable logistic regression analysis , cancer type , time since cancer diagnosis , cancer stage , male sex , leuco cytosis , lymphopenia , high nlr , thrombocytopenia , lactate dehydrogenase , d - dimer , creatine kinase , c - reactive protein , creatinine , receipt of chemotherapy or targeted therapy within 4 weeks before symptom onset , and hospital admission were associated with death ( table 5 )  . 
we included 180 patients with complete data in the multivariable regression analysis ( 146 survivors and 34 non - survivors ) , in which we included four variables : sex , cancer type , receipt of chemotherapy within the previous 4 weeks , and time since cancer diagnosis . 
receiving chemotherapy within 4 weeks before symptom onset ( or 351 [ 95% ci 1161059 ] ; p = 0026 ) and male sex ( 386 [ 157950 ] ; p = 00033 ) were associated with increased odds of death during admission to hospital ( table 5 )  . 
similar results were shown after adjusting for study centre or different cancer types ( appendix p 8 )  . discussion patients with cancer are a vulnerable population in the ongoing covid - 19 pandemic . 
 to our knowledge , this is the first multicentre , retrospective , cohort study to describe the clinical features , outcomes , and risk factors for mortality in patients with cancer and diagnosed with covid - 19 . 
severe pneumonia occurred in 52 ( 25% ) patients and the in - hospital univariable or ( 95% ci ) p value multivariable or ( 95% ci ) p value ( continued from previous page ) cancer type solid tumour ecog score haematological malignancy 339 ( 133863 ) 0010 207 ( 068635 ) 020 1 ( ref ) 1 ( ref ) 1 ( ref ) 129 ( 050329 ) 177 ( 043726 ) 398 ( 0811953 ) 060 043 0088 100 hospital admission before feb 13 , 2020 807 ( 2752370 ) 00001 1 ( ref ) or = odds ratio . 
hospital admission before feb 13 , 2020 , is used as a factor to represent the time period of the covid - 19 pandemic . table 5 : bivariate logistic regression analysis of factors associated with death during admission to hospital case - fatality rate in patients with covid - 19 and cancer was 20% , which is much higher than the case - fatality rate for covid - 19 in the overall chinese population ( 1% ) .13 in wuhan , the case - fatality rate of patients with cancer in our study was 18% ( 34 of 184 patients ) , which was higher than the overall case - fatality rate reported for patients with covid - 19 ( 8% ) .5 in particular , male sex and receiving chemotherapy within 4 weeks before symptom onset were identified as risk factors for death in patients with cancer who were diagnosed with covid - 19 . the proportion of patients with cancer among those with covid - 19 who were admitted to the nine hospitals in our study was 25% , which was higher than that reported in the overall chinese population ( 029% ) 18 and in a previous report of patients with covid - 19 ( 1% ) .10 this finding suggests that patients with cancer are more susceptible to covid - 19 than the general population . 
by contrast with four other human coronaviruses ( hcov - nl63 , hcov - 229e , hcov - oc43 , and hku1 ) , which induce only mild upper respiratory diseases , 19 sars - cov - 2 behaves like sars - cov and middle east respiratory syndrome coronavirus ( mers - cov ) to some extent , and leads to higher rates of severe respiratory syndrome.20 similar to our study , fever and cough were the most common clinical manifestations among patients with covid - 19.16 although older age and underlying diseases have been found to be risk factors for severe events in a previous study , 10 this was not observed in our study . 
we found bilateral lung lesions in 91% of patients with available records , which was higher than the figure reported previously by xu and colleagues ( bilateral lung lesions in 53 [ 59% ] of vol 21 july 2020 articles 90 patients with laboratory - confirmed sars - cov - 2 infection ) , 21 sug gesting that patients with cancer were more vulnerable once they became infected with sars - cov - 2 . men were found to be at a higher risk of mortality than women in this study . 
in addition to sex differences in smoking rate , 22 differences in the immune and endocrine systems between men and women23 , 24 might exert different responses against sars - cov - 2 infection . 
62 ( 57% ) of 109 women in our study had one of these three types of cancers . lymphocytopenia is one of the clinical features of covid - 19 , 4 indicating that the virus tends to diminish the antiviral immunity of the host . 
since we do not yet have highly effective drugs targeting sars - cov - 2 , a patients inherent immunity might be a determining factor for their prognosis after effective supportive care . 
it has been recommended that the mode of admin istration ( from infusion to oral administration ) and intervals of chemotherapy should be adjusted according to patients conditions.25 although molecular - targeted therapy rarely impairs patients immunity , those receiving maintenance molecular - targeted therapy all had advanced disease , and seven ( 58% ) of 12 received chemotherapy concurrently within 4 weeks before symptom onset , which might have accounted for the increased risk of death . 
immunosuppressive treatments administered more than 4 weeks before symptom onset might not worsen the outcome of covid - 19 , which can be partially explained by the recovery of patients from side - effects of cytotoxic treatments . 
because of the small number of patients in our study who received chest radiotherapy 4 weeks before onset of covid - 19 , we were not able to analyse the effect of recent chest radiotherapy on patient outcomes . many haematological malignancies change how blood cells in the immune system function . 
lower respiratory tract diseases caused by human coronaviruses in patients with haematological malignancies have been associated with high rates of oxygen use and mortality.26 in our study , patients with haematological malignancies had poorer prognoses than those with solid tumours . 
besides the inherent differences between haematological malignancies and solid tumours , more patients with haematological malignancies received chemotherapy within 4 weeks before symptom onset ( 11 [ 55% ] of 20 vs 20 [ 12% ] of 162 ) , which might partly explain our finding of worse outcomes in these patients . in addition to lymphocytes , neutrophils are the mainstay in fighting off various infections . 
nlr is considered to reflect host inflammation and is a predictor of bacterial infection.27 it has also been found to be associated with clinical outcome and treatment efficacy in several cancers.28 in patients with covid - 19 , high neutrophil counts have frequently been seen in refractory disease.29 in line with a previous study , 30 we found a high nlr to be associated with poor prognosis in patients with cancer and covid - 19 . 
sars - cov - 2 infection and subsequent bacterial infection might have caused a deterioration of lung function and contributed to death , although this hypothesis requires further investigation . our study had some limitations . 
 additionally , we did not compare the case - fatality rate , characteristics , outcomes , and treatment strategies of patients with cancer against a control group of patients without cancer . 
dynamic changes in the titre of the igm and igg antibodies , sars - cov - 2 nucleic acid , and other laboratory tests such as tumour - related cytokines besides interleukin - 6 ( eg , tumour necrosis factorand interferon - ) in the course of disease should be further recorded and analysed . 
finally , the impact of covid - 19 on cancer needs to be evaluated with long - term follow - up of survivors . in conclusion , patients with cancer and covid - 19 require urgent and special attention , since they are a vulnerable population with a much higher case - fatality rate than the general population . 
receiving chemotherapy 4 weeks before symptom onset and male sex are two indicators that might help clinicians to identify patients with cancer who are at high risk of fatal outcomes at an early stage . contributors gw and ky had the idea for and designed the study and provided financial support . 
gw , ky , bw , ch , yj , nx , kj , and hl critically revised the manuscript for important intellectual content . declaration of interests we declare no competing interests . acknowledgments this work was supported by the national natural science foundation of china ( nsfc 81874218 , nsfc 81672978 )  . 
we thank all front - line healthcare workers for their efforts during the covid - 19 pandemic . long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial ian smith * , john robertson * , lucy kilburn , maggie wilcox , abigail evans , chris holcombe , kieran horgan , cliona kirwan , elizabeth mallon , mark sibbering , anthony skene , raghavan vidya , maggie cheang , jane banerji , james morden , kally sidhu , andrew dodson , judith m bliss , mitch dowsett summary background preoperative and perioperative aromatase inhibitor ( poai ) therapy has the potential to improve outcomes in women with operable oestrogen receptor - positive primary breast cancer . 
the poetic trial aimed to test these two hypotheses . methods poetic was an open - label , multicentre , parallel - group , randomised , phase 3 trial ( done in 130 uk hospitals ) in which postmenopausal women aged at least 50 years with who performance status 01 and hormone receptor - positive , operable breast cancer were randomly assigned ( 2 : 1 ) to poai ( letrozole 25 mg per day orally or anastrozole 1 mg per day orally ) for 14 days before and following surgery or no poai ( control )  . 
recruitment is complete and long - term follow - up is ongoing . findings between oct 13 , 2008 , and april 16 , 2014 , 4480 women were recruited and randomly assigned to poai ( n = 2976 ) or control ( n = 1504 )  . 
 434 ( 10% ) of 4480 women had a breast cancer recurrence ( 280 [ 9% ] poai ; 154 [ 10% ] control ) , hazard ratio 092 ( 95% ci 075112 ) ; p = 040 with the proportion free from breast cancer recurrence at 5 years of 910% ( 95% ci 899920 ) for patients in the poai group and 904% ( 887919 ) in the control group . 
within the poai - treated her2 - negative subpopulation , 5 - year recurrence risk in women with low ki67b and ki672w ( lowlow ) was 43% ( 95% ci 2963 ) , 84% ( 68105 ) with high ki67b and low ki672w ( highlow ) and 215% ( 171270 ) with high ki67b and ki672w ( highhigh )  . 
within the poai - treated her2 - positive subpopulation , 5 - year recurrence risk in the lowlow group was 101% ( 95% ci 32313 ) , 77% ( 34175 ) in the highlow group , and 157% ( 101244 ) in the highhigh group . 
the most commonly reported grade 3 adverse events were hot flushes ( 20 [ 1% ] of 2801 patients in the poai group vs six [ < 1% ] of 1400 in the control group ) and musculoskeletal pain ( 29 [ 1% ] vs 13 [ 1% ] )  . 
no treatment - related deaths were reported . interpretation poai has not been shown to improve treatment outcome , but can be used without detriment to help select appropriate adjuvant therapy based on tumour ki67 . 
we carried out a pubmed search for relevant clinical studies published from jan 1 , 1989 until dec 31 , 2019 using the terms neoadjuvant endocrine , breast cancer , clinical trial , and presurgical and endocrine therapy . 
before the initiation of poetic , two small clinical neoadjuvant trials , impact and z1031 , reported that tumour ki67 24 weeks after starting preoperative endocrine treatment predicted outcome better than baseline ki67 . 
another modestly sized trial used to triage patients with 24 week ki67 > 10% to chemotherapy and reporting the long - term outcome for those less than 10% , has led to a larger ongoing trial . 
the concept of complete cell cycle arrest has been developed as an additional possible cutoff for on - treatment ki67 . added value of this study results from poetic suggest that 2 weeks preoperative endocrine therapy makes no perceptible improvement in long - term outcome , but was nevertheless a safe treatment practice . 
in patients with a high baseline ki67 value ( > 10% ) a biopsy 2 weeks after starting preoperative endocrine therapy provides additional clinical utility by predicting long - term outcomes . 
the trial documents the relationship of 2 - week ki67 with risk of recurrence for estimating whether the prognosis of individual patients is sufficiently good on endocrine therapy alone or whether additional treatment such as chemotherapy or new targeted therapies should be considered . implications of all the available evidence the data show no reason for short - term presurgical treatment to be applied for its direct therapeutic potential , but support prescribing an aromatase inhibitor for the short - term period before breast cancer surgery in oestrogen receptor - positive tumours with a high proliferation rate to derive information on early endocrine responsiveness that can be used to predict a patients 5 - year prognosis on standard adjuvant therapy . 
the clinical manoeuvres to incorporate this in the patient pathway with reliable quality assured ki67 are straightforward and the measurement of ki67 is inexpensive , potentially making this an attractive approach to estimating the prognosis of patients with early breast cancer . introduction the poetic ( peri - operative endocrine therapy individualising care ) trial was designed to address two important hypotheses in the treatment of postmenopausal women with oestrogen receptor - positive early breast cancer . the first was that short duration presurgical endocrine therapy might improve clinical outcome . 
this hypothesis was plausible because 2 weeks preoperative endocrine therapy had been shown to markedly reduce proliferation in human breast cancer as measured by ki67.1 , 2 longstanding experimental evidence had shown that the stimulatory effect of surgery on the growth of metastases in mice could be inhibited by perioperative endocrine therapy.3 , 4 any improvement in long - term outcome following short exposure to preoperative or perioperative endocrine therapy would be achieved with no additional toxicity or resource implications and be of considerable clinical importance . the second hypothesis concerned identifying which patients with hormone receptor - positive early breast cancer have a sufficiently good prognosis such that standard of care medical treatment , often comprising adjuvant endocrine therapy alone , was sufficient and which group should be considered for additional therapies . 
traditional approaches to this problem had used standard prognostic parameters including size , grade , nodal involvement , and age , often integrated into a prognostic tool ( eg , nottingham prognostic index , 5 adjuvant online , 6 nhs predict7 ) , but these merely provided the predicted probability of benefit for a patient population with given tumour and demo - graphic characteristics . 
more recently , genomic platforms have been developed aimed at providing more accurate prognostic and predictive information for the individual patient.8 , 9 however , these genomic tests are expensive , by no means universally available , and differ among themselves in terms of the information they provide.10 a simple test which predicts outcome after short duration preoperative endocrine therapy could therefore be helpful in accurately selecting appropriate treatment in the individual patient , if it incorporated an in - vivo response to aromatase inhibitor . 
a small neoadjuvant trial ( impact ) had already suggested this might be feasible : results showed that tumour ki67 after 2 weeks ( ki672w ) of endocrine treatment predicted outcome better than at baseline ( ki67b ) , remaining significant multivariable analysis , whereas ki67b did not.11 , 12 similar 1444 vol 21 november 2020 articles see online for appendix results have subsequently been reported from another small trial comparing letrozole with tamoxifen13 and from a further trial comparing anastrozole , letrozole , and exemestane with one another.14 poetic , with a much larger patient population , aimed to build on these findings to provide the definitive clinical evidence to inform future practice . methods study design and participants this open - label , multicentre , parallel group , randomised , phase 3 trial recruited participants from 130 uk hospitals ( appendix p 2527 )  . 
eligible patients were postmenopausal women ( aged at least 50 years with amenorrhoea for more than 12 months , bilateral oophorectomy or hysterectomy , or had been on hormone replacement therapy within the previous 12 months , and with folliclestimulating hormone concentrations in the postmenopausal range if aged less than 55 years ) with oestrogen receptor - positive or progesterone receptorpositive ( allred 3 , h - score 2 , or 1% of positive cells , assessed in local pathology laboratories ) , her2 - positive or her2negative ( assessed locally ) , operable primary breast cancer and no evidence of metastatic spread investigated according to local guidelines . 
if palpable , a tumour of any size was sufficient , otherwise requiring an ultrasound size of at least 15 c women required who performance status 01 and an indication for standard adjuvant endocrine therapy . 
previous endocrine therapy or chemotherapy was not allowed , nor was concurrent use of hormone replacement therapy or any other oestrogen - containing medication ( within 4 weeks of randomisation )  . 
no previous use of oestrogen implants at any time , current , continuous , long - term systemic steroid usage , or treatment with an unlicensed or investigational drug within 4 weeks of randomisation was allowed . 
patients with invasive malignancy diagnosed within the previous 5 years or any severe co - incident medical disease were ineligible ( appendix p 1 )  . patients provided written informed consent before enrolment . 
poetic was sponsored by the institute of cancer research ( icr ) and royal marsden nhs foundation trust and approved by the londonsouth east research ethics committee ( reference 08 / h1102 / 37 ) and managed and analysed by the icr clinical trials and statistics unit ( icr - ctsu ; appendix p 1 for study oversight details )  . 
the protocol is in the appendix . randomisation and masking participants were randomly allocated ( 2 : 1 ) to perioperative aromatase inhibitor ( poai ) treatment or no perioperative treatment ( control ) by computer - generated permuted block method ( variable block size six or nine ) derived centrally by icr - ctsu using its dedicated randomisation system , stratified by hospital . 
no placebo was used ; clinicians and patients were not masked to treatment allocation , but central laboratory staff were masked . ratio weighted inhibitor procedures poai was a non - steroidal aromatase standard dosage ( oral anastrozole 1 mg per day or oral letrozole 25 mg per day ) ; choice of agent was declared by each participating hospital at trial outset . 
before randomisation , all patients had excisional surgery prebooked for around 2 weeks ( minimum 10 days ) later to ensure timing of surgery was not biased by treatment allocation . 
 treatment continued without interruption until 14 days after surgery . all non - trial adjuvant therapy , laboratory investigations , and disease staging were established on clinical grounds according to standard of care local practice ( appendix p 1 )  . 
in february , 2011 , a letter to investigators , followed by an approved protocol amendment , recommended that local multidisciplinary teams gave due consideration to other factors , including pretreatment grade on diagnostic core where available , when considering use of adjuvant chemotherapy . follow - up data were submitted annually to icr - ctsu ; disease - related events , second cancers and deaths were reported on occurrence . 
adverse event data were restricted three meno pausal symptoms ( hot flushes , sweating , and musculoskeletal pain ) at baseline , surgery , and at followup 2 weeks postsurgery ( assessed using national cancer institute common terminology criteria for adverse events version 3 ) as the safety profiles of the aromatase inhibitors used were well established . 
 participants were able to withdraw from the trial at any time for any reason . formalin - fixed paraffin - embedded tissue samples were required before randomisation ( baseline ) and at surgery . 
at surgery , samples could be either core biopsies or sections cut from the routine excision . vol 21 november 2020 1445 articles tissue samples were processed , stored , and analysed for ki67 staining centrally in the ralph lauren centre for breast cancer research at the royal marsden nhs foundation trust . 
ki67 was analysed immunohistochemically in a core biopsy taken at baseline ( ki67b ) , and in either a core biopsy or the excision biopsy taken at surgery ( ki672w ) , and was estimated as the percentage of cancer cells staining positive . 
we used mib1 as the primary antibody to ki67 and detection was done with the real envision system , both from dako ( glostrup , denmark until 2016 ; now agilent technologies , didcot , uk )  . 
scoring was according to methodology including between - batch quality control procedures as described by the international ki67 in breast cancer working group party.15 analysis of 2 - week samples from the control group was restricted to a randomly selected subset since minimal change from baseline was expected.16 outcomes the primary endpoint was time to recurrence ( time from randomisation to local , regional , or distant tumour recurrence or death from breast cancer without previous notification of relapse ) with second primary cancers and intercurrent deaths censored . 
secondary clinical endpoints included relapse - free survival ( as per time to recurrence but also including deaths from any cause as events ) , time to local recurrence ( time from randomisation to first confirmed local recurrence , censoring at previous distant recurrence , second primary cancer , or death ) , time to distant recurrence ( time from randomisation to first confirmed distant recurrence or breast cancer death without previous relapse , censoring at second primary cancer or intercurrent death ) and overall survival ( time from randomisation to death from any cause )  . 
breast cancer - free survival duplicated the definition of time to recurrence , and was listed in the protocol in error . ki67 was evaluated as a biomarker in relation to its effect on predicting disease outcomes ( one of the trials two key objectives ) and as the molecular secondary endpoint to assess proliferation rate at baseline ( ki67b ) and at surgery ( ki672w ) , thus assessing the impact of poai . 
the additional molecular secondary endpoint of gene expression profile at core biopsy and at surgical excision is not reported here as data analysis is ongoing . statistical analysis the sample size assumed the proportion of patients with recurrence by 5 years would be low ( approximately 10% ) given known recurrence rates for similar populations.17 , 18 with 4350 patients it would be possible to detect a 3% improvement in time to recurrence at 5 years ( 10% to 7% recurrences ) with 91% power ( two - sided of 5% )  . 
the sample size was increased originally from 4000 to 4350 patients to allow for underestimation of the relapse rate potentially owing to patients dying from other causes before breast cancer relapse . 
this change was endorsed by the trial steering committee and independent data monitoring committee and managed via a protocol amendment approved on dec 31 , 2012 . to modified analyses relating to clinical endpoints were done according intention - to - treatremoving patients who subsequently withdrew consent for use of data . 
patients who did not have primary breast surgery as planned were censored at the date of that decision . baseline demographic details , tumour characteristics , adjuvant treatment , and ki67 data are presented with descriptive statistics . 
protocol compliance between treatment groups ( time from randomisation to surgery and number of inpatient days for surgery ) was compared using wilcoxon rank - sum tests ; differences in tumour grade at surgery were assessed using a test for trend in prespecified analyses . 
in a post - hoc exploratory analysis , following initial planned analyses on the trial data , a multivariable logistic regression model was created , using a forward stepwise approach , to determine factors affecting chemotherapy use . for survival - related endpoints , kaplan - meier curves were plotted and treatment groups compared with the log - rank test . 
 comparisons between treatment groups were made with and without adjustment for progesterone receptor status ( positive , negative , unknown ) , her2 status ( positive , negative , unknown ) , presurgical tumour grade ( g1 , g2 , and g3 ) , pathological ( continuous ) , presurgical histological type ( ductal , lobular , special type ) , nodal status ( n0 , n13 , and n4 + ) , age at randomisation ( continuous ) and vascular invasion ( yes , no )  . 
subgroup analyses were done for baseline clinical characteristics and presented using a forest plot . tumour size associations between ki67b and ki672w and time to recurrence were done separately in the poai and control groups with the principal focus being to study the ontreatment effect of poai . 
assessment of ki67 in the control group was considered of low additional value because patients were not exposed to perioperative treatment and because of the lack of association between poai and time to recurrence . 
 to explore associations between ki67 and disease outcome in the poai group , ki67 scores were dichotomised and patients divided into four groups as follows : lowlow ( ki67b and ki672w < 10% ) ; highlow ( ki67b 10% , ki672w < 10% ) ; highhigh ( ki67b and ki672w 10% ) ; and lowhigh ( ki67b < 10% , ki672w 10% )  . 
in addition to the predefined 10% ki67 dichotomisation , chosen to ensure consistency with other neoadjuvant trials , 12 , 14 other cut - points were explored using harrells c coefficient19 including that for complete cell cycle arrest ( ccca ; ki67 27%20 )  . previous analyses21 of change in ki67 in 679 control group patients with paired samples available indicated that in patients with a core - cut surgery sample the median proportional reduction was 41% ( iqr 278 to 348 ) , whereas in those with a resection sample at surgery , the median proportional reduction in ki67 between baseline and surgery was 177% ( iqr 442 to 127 ) in contrast with an earlier small pilot study.16 from these findings , it was assumed that , for a given surgical sample , change in ki67 score would be proportionally approximately 15% less if the sample was core - cut rather than resection ( eg , 10% reduction with resection sample translated to 85% for core - cut )  . 
for cases where ki672w was 0% , no adjustment was made . this manuscript describes the primary endpoint analysis , time to recurrence after a 5 - year median followup for both hypotheses ; first by randomised poai allocation and second exploring the ability of ki67 to predict disease outcome . 
for this purpose , a database snapshot was taken on aug 8 , 2017 for data presented at the san antonio breast cancer conference 2017 and updated with a second database snapshot taken on feb 6 , 2018 . 
a p value of less than 005 was deemed to be significant . this study is registered with clinicaltrials.gov , nct02338310 ; the european clinical trials database , eudract2007 - 003877 - 21 ; and isrctn63882543 . the isrctn registry , role of the funding source the funder of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all of the data in the study and had final responsibility for the decision to submit for publication . results between oct 13 , 2008 , and april 16 , 2014 , 4486 patients were entered from 130 uk centres . 
six patients subsequently withdrew consent for data to be used and therefore 4480 patients ( 2976 poai , 1504 control ) were included in the modified intention - to - treat analysis ( figure 1 )  . median age at randomisation was 671 years ( iqr 615748 ) , 2536 ( 57% ) of 4480 patients had a tumour size up to 2 cm , and all but eight ( < 1% ) patients were confirmed locally to have hormone receptor - positive tumours ( table 1 )  . 
23 ( 1% ) of 4480 patients did not have surgery as planned ( 16 patients in the poai group and seven in the control group ; figure 1 )  . 
 177 ( 6% ) of 2976 patients did not have the protocol defined duration of poai ( preoperatively < 10 days or > 21 days , post operatively < 10 days )  . 
the most common reasons were 63 ( 2% ) had their surgery changed , 35 ( 1% ) had less owing to adverse events ( 16 were in the presurgical period ) , and 30 ( 1% ) had less owing to patient choice or omission . 
surgical details and postsurgery tumour characteristics were well balanced between groups with the exception of pathological tumour grade , which was higher in the control group ( p < 00001 ; table 1 )  . 
 adjuvant chemo therapy was given to 770 ( 26% ) of 2957 patients in the poai group and 460 ( 31% ) of 1493 patients in the control group ( appendix p 15 ) with multivariable analyses attributing this to differences observed in postsurgical grade ( appendix p 16 )  . 
following surgery , most ( poai 2507 [ 86% ] of 2960 patients ; control 1186 [ 81% ] of 1497 patients ) women were prescribed aromatase inhibitor monotherapy ( appendix p 17 )  . with 629 months median follow - up ( iqr 581741 ) , 434 ( 10% ) of 4480 women had a breast cancer recurrence ( poai 280 [ 9% ] of 2976 patients , control 154 [ 10% ] of 1504 patients ; table 2 ) with no significant difference observed between the treatment groups ( hr 092 , 95% ci 075112 ; p = 040 , adjusted hr 096 , 077119 ; p = 070 ; figure 2a ) with the proportion free from breast cancer recurrence at 5 years of 910% ( 899920 ) in the poai group and 904% ( 887919 ) in the control group . 
 likewise , no significant differences between treatment groups were observed for relapse - free survival , time to local recurrence , and time to distant recurrence ( table 3 )  . 
 second breast cancer primaries developed in 26 ( < 1% ) of 2976 women in the poai group compared with 24 ( 2% ) of 1504 in the control group . 
5 - year overall survival was 889% ( 95% ci 877901 ) in the poai group versus 889% ( 872905 ) in the control group ( unadjusted hr 094 , 95% ci 079112 ; p = 050 , adjusted hr 091 , 075110 ; p = 033 ; figure 2b )  . selected menopausal symptoms were assessed in 4201 ( 94% ) of 4480 women , with higher symptom rates observed for poai ( appendix p 18 )  . 
the most commonly reported grade 3 adverse events were hot flushes ( 20 [ 1% ] of 2801 patients in the poai group vs six [ < 1% ] of 1400 in the control group ) and musculoskeletal pain ( 29 [ 1% ] vs 13 [ 1% ] )  . 
the most 1448 vol 21 november 2020 articles common were pulmonary embolism musculoskeletal pain ( n = 3 )  . ( n = 3 ) and 3913 ( 87% ) of 4480 participants had ki67b data available . 
 2528 ( 85% ) of 2976 patients in the poai group and 678 ( 45% ) of 1504 in the control group had paired ki67b and ki672w data available ( figure 1 )  . 
in 2316 ( 72% ) of 3206 participants with paired ki67 data , the surgical sample was a resection ( 1834 [ 73% ] of 2528 patients in the poai group ; 474 [ 70% ] of 678 patients in the control group ) or the surgical sample type was unknown ( six in the poai group and two in the control group ) and the ki672w scores for these resections and unknown surgical sample types were corrected as described . 
688 ( 27% ) of 2528 poai and 202 ( 30% ) of 678 control patients surgical sample type was core - cut biopsy . the median ki67b score in the 3913 of 4480 patients with a sample available was 152% ( iqr 86260 ; poai 153% [ 85264 ] ; control : 149% [ 86251 ] )  . 
ki67b values were different between her2 - negative and her2positive tumours ( median 143% [ iqr 82246 ] in her2 - negative tumours , median 266% [ 170374 ] in her2 - positive tumours ; p < 00001 )  . 
women whose ki672w remained high ( highhigh group ) were significantly more likely to have a recurrence than those whose ki672w had dropped below 10% ( highlow group ; unadjusted hr 259 , 95% ci 193347 ; p < 00001 , adjusted hr 210 , 148298 ; p < 00001 ; figure 3a )  . 
within the poai - treated her2negative subpopulation , 5 - year recurrence risk in women with low ki67b and ki672w ( lowlow ) was 43% ( 95% ci 2963 ) , 84% ( 68105 ) with high ki67b and low ki672w ( highlow ) and 215% ( 171270 ) with high ki67b and ki672w ( highhigh )  . 
within the poai - treated her2positive subpopulation , 5 - year recurrence risk in the low low group was 101% ( 95% ci 32313 ) , 77% ( 34175 ) in the high - low group , and 157% ( 101244 ) in the highhigh group . 
adding a high versus low classification at 2 weeks segregated groups in relation to their baseline ki67 ( appendix p 21 )  . the her2 - negative poai - treated subpopulation posthoc exploratory analyses relating to the combined effects of age and chemotherapy use suggested that in patients with ki67b of at least 10% , who did not receive adjuvant chemotherapy , the residual ki672w ( high or low ) conferred demographics at randomisation and tumour characteristics from the diagnostic core surgery details and tumour characteristics from surgery perioperative aromatase inhibitor group ( n = 2976 ) control group ( n = 1504 ) perioperative aromatase inhibitor group ( n = 2960 ) control group ( n = 1497 ) ( continued from previous page ) definitive breast surgery mastectomy conservative surgery definitive axillary surgery sentinal lymph node biopsy nodal status missing clearance sampling missing n13 missing missing vascular invasion not reported missing multi - focal disease 1051 ( 36% ) 1902 ( 64% ) 7 ( < 1% ) 503 ( 34% ) 992 ( 66% ) 2 ( < 1% ) 2911 ( 98% ) 1470 ( 98% ) 916 ( 31% ) 287 ( 10% ) 1708 ( 58% ) 42 ( 1% ) 7 ( < 1% ) 1815 ( 61% ) 801 ( 27% ) 334 ( 11% ) 10 ( < 1% ) 813 ( 27% ) 1990 ( 67% ) 143 ( 5% ) 14 ( < 1% ) 468 ( 31% ) 150 ( 10% ) 852 ( 57% ) 25 ( 2% ) 2 ( < 1% ) 892 ( 60% ) 434 ( 29% ) 165 ( 11% ) 6 ( < 1% ) 445 ( 30% ) 981 ( 66% ) 63 ( 4% ) 8 ( 1% ) 381 ( 13% ) 223 ( 15% ) 2563 ( 87% ) 1266 ( 85% ) 16 ( 1% ) 8 ( 1% ) data are n ( % ) and median ( iqr )  . 
 * one patient ( perioperative aromatase inhibitor ) with hormone receptor status unknown was her2 negative ; the remaining two patients ( control ) with hormone receptor status unknown also had her2 status unknown . 
special types from surgery specimen include mucinous , papillary , tubular , endocrine cell carcinoma , pure special type , metaplastic carcinoma clear cell , and basaloid , tubular , and cribiform carcinoma . 
patients are eligible if they have either a palpable tumour ( clinical examination ) of any size or a tumour with an ultrasound size of 15 c618 patients had tumour size < 15 cm , of which 607 had a tumour confirmed as palpable . table 1 : baseline characteristics a differential effect on prognosis as assessed by time to recurrence for both those aged less than 70 years and aged at least 70 years ( appendix pp 49 )  . 
numbers were too small to fully define effects for the corresponding group ( ie , ki67b 10% ) who did receive chemotherapy . in patients with her2 - negative breast cancer in the control group , 56 time to recurrence events were reported in the 597 of 678 patients for whom ki672w was available . 
if more than one first event was reported on the same date , it was included in the row here according to the following order of priority : distant recurrence , local recurrence , breast second primary cancer , non - breast second primary cancer , and intercurrent death . 
 included 25 patients ( 18 perioperative aromatase inhibitor , seven in the control group ) with unknown cause of death and no previous event ; one patient had a second primary cancer before unknown cause of death and was not included here . 
 other causes in the perioperative aromatase inhibitor group ( n = 13 ) were accident ( n = 2 ) , acute kidney injury , alzheimers disease , ascending aortic aneurysm , haematemesis secondary to gastric ulcer , hepatic cirrhosis , multiorgan failure , myelofibrosis , old age with vascular deterioration and chronic kidney disease , portal hypertension , a fall , ascites , evidence of cirrhosis , postoperative complications relating to pituitary tumour operation , and renal failure ; other causes in the control group ( n = 6 ) were complications post laparotomy , dementia , diabetes , meningioma , subdural haematoma , and suicide . table 2 : disease - related first events and deaths a post - hoc sensitivity analysis in the her2 - negative subgroup combining the baseline data for poai and control gave a 5 - year recurrence risk of 47% ( 95% ci 3563 ) for low ki67b and 115% ( 95% ci 101131 ) for high ki67b ( appendix p 24 )  . prespecified exploratory analysis in the her2 - negative subgroup suggested an optimal cut - point around 1520% for ki67b and around 68% for ki672w and that using the ccca threshold for ki672w had prognostic discrimination ( appendix pp 1113 )  . in patients with hormone receptor - positive , her2positive breast cancer in the poai group ( 273 [ 10% ] of 2528 patients ) , 33 time to recurrence events were reported . 
143 women in the ki67 highhigh group had a recurrence compared with 94 in the highlow group , although the difference was not significant ( unadjusted hr 208 , 95% ci 088490 ; p = 0093 , adjusted hr 183 , 071473 ; p = 021 ; figure 3b )  . 
similar to the her2negative group , absolute risk of recurrence at 1 , 3 , and 5 years was higher in the high - high group than in the highlow group ( appendix p 23 )  . 
5 - year recurrence risk in the low - low group was 101% ( 95% ci 32313 ) , 77% ( 34175 ) in the highlow group , and 157% ( 101244 ) in the highhigh group . 
in the 70 women with her2 - positive breast cancer in the control group , nine time to recurrence events were reported . discussion poetic is , to our knowledge , the largest trial of its kind to assess the potential of poai therapy in patients with postmenopausal , hormone receptor - positive early breast cancer and it did not show any significant long - term improvement in disease outcomes with this approach . 
 this was despite preclinical experimental evidence in a mouse model suggesting the contrary.3 , 4 a smaller phase 3 clinical trial , which reported after poetic was initiated , randomly assigned operable breast cancer patients ( n = 976 , 50% hormone receptor - positive , 45% hormone receptor - negative , and 5% hormone receptor unknown ) to surgery or an intramuscular injection of depot hydroxyprogesterone 500 mg 514 days before surgery ; no significant benefit was observed in the overall population ( hr 087 , 95% ci 068109 ; p = 023 ) , but the results suggested a hypothesis - generating potential disease - free survival in node - positive subgroups ( hr 072 , 054097 ; p = 002 ) .22 in contrast , consistent with the overall finding , poetic showed no suggestion of long - term outcome improvement with poai overall or in the node - positive subgroup . improvement in poetic , the frequency of chemotherapy was slightly lower in patients in the poai group than in those in the control group . 
multivariable regression supported the suggestion that this was probably because of multidisciplinary teams being influenced by pathological tumour grade , which was on average lower in the patients in the poai group . 
this absolute difference was small however ( 5% ) , and since the overall event rate was less than 20% would have had an imperceptible effect on outcome comparisons . on a pragmatic note , it is common practice to start some patients on preoperative endocrine therapy if there has to be a significant delay in surgery for any reason . 
 despite not showing any statistical evidence of clinical benefit , our results provide reassurance that there is no detriment to this practice . the second aim of this trial was to explore whether the measurement of tumour ki67 2 weeks after starting treatment could predict disease outcome better than baseline ki67 alone , thus providing the basis of a simple and inexpensive test to personalise adjuvant treatment in patients with hormone receptor - positive , her2negative breast cancer . 
previously , impact had shown 1450 vol 21 november 2020 articles a control perioperative aromatase inhibitor unadjusted hazard ratio 092 ( 95% ci 075112 ) ; p = 040 number at risk ( number censored ) perioperative aromatase inhibitor control 2976 ( 57 ) 1504 ( 21 ) 2871 ( 93 ) 1451 ( 42 ) 2793 ( 153 ) 1404 ( 71 ) 2681 ( 400 ) 1349 ( 194 ) 2374 ( 1021 ) 1197 ( 509 ) 1711 ( 1833 ) 862 ( 909 ) 875 ( 2382 ) 450 ( 1202 ) 317 ( ) 150 ( ) unadjusted hazard ratio 094 ( 95% ci 079112 ) ; p = 050 time from randomisation ( years ) number at risk ( number censored ) perioperative aromatase inhibitor control 2976 ( 38 ) 1504 ( 11 ) 2914 ( 45 ) 1474 ( 17 ) 2850 ( 75 ) 1442 ( 23 ) 2756 ( 294 ) 1393 ( 136 ) 2443 ( 904 ) 1237 ( 452 ) 1768 ( 1728 ) 893 ( 859 ) 905 ( 2290 ) 466 ( 1153 ) 323 ( ) 155 ( ) figure 2 : kaplan - meier survival curve by randomised treatment group for time to recurrence ( a ) and overall survival ( b ) in part a test for proportionality , p = 058 . 
in part b test for proportionality , p = 082 . that 2 - week on - treatment ki67 predicted outcome better than baseline and , unlike baseline , was significant in multivariable analysis.12 poetic has provided evidence for the clinical validity of on - treatment aromatase inhibitor ki672w in addition to ki67b to predict those with high residual risk of recurrence in spite of standard - ofcare therapy . 
our results provide an early indication of endocrine sensitivity or resistance including for the large number of patients who are not routinely considered for adjuvant chemotherapy . separate clearly defined adjuvant treatment pathways for her2 - positive and her2 - negative breast cancers now exist and we therefore analysed these groups separately when considering prognostic risk . 
focus for exploratory analysis was therefore on the her2 - negative subgroup , which comprised approximately 90% of the poetic population . number of events unadjusted hazard ratio adjusted hazard ratio 5 - year survival estimate perioperative aromatase inhibitor group control group 385 ( 13% ) 207 ( 14% ) 41 ( 1% ) 24 ( 2% ) 262 ( 9% ) 147 ( 10% ) relapse - free survival time to local recurrence time to distant recurrence 094 ( 079111 ) ; 047 086 ( 052143 ) ; 057 090 ( 073110 ) ; 030 095 ( 079114 ) ; 059 092 ( 054156 ) ; 075 094 ( 075118 ) ; 059 perioperative aromatase inhibitor group control group 879% ( 866891 ) 876% ( 857892 ) 986% ( 981990 ) 985% ( 976990 ) 917% ( 905926 ) 909% ( 892923 ) data are n ( % ) , hazard ratio ( 95% ci ) ; p value , and % ( 95% ci )  . 
models adjusted for progesterone receptor status ( positive , negative , unknown ) , her2 status ( positive , negative , unknown ) , presurgical tumour grade ( g1 , g2 , and g3 ) , pathological tumour size ( continuous ) , presurgical histological type ( ductal , lobular , special type ) , nodal status ( n0 , n13 , and n4 + ) , age at randomisation ( continuous ) , and vascular invasion ( yes , no )  . 
28 patients with hormone receptor - positive breast cancer and her2 - negative breast cancer and four patients with hormone receptor - positive and her2 - positive breast cancer in the low - high group were omitted from the figure . previously , it had been shown that patients with a low ki67b have a better prognosis than those with a high ki67b value.23 poetic confirmed this in a larger prospective population , dichotomising ki67b at 10% with 5 - year recurrence risk in her2 - negative patients in the poai group of 44% for low ki67b and 118% for high ki67b . 
to our knowledge , this is the first large published dataset that makes use of the ki67 scoring methodology recommended by the international ki67 in breast cancer working group ; the strong association of ki67 at baseline with prognosis served as a clinical validation of that methodology.15 patients whose ki67b was low did well on standard of care , with approximately 85% of those receiving endocrine therapy alone . 
but irrespective of adjuvant treatment , it is reasonable to conclude that ki672w did not add significant prognostic or predictive information in this subgroup . in contrast , for patients whose tumours had a high baseline ki67 in the poai group , 73% had a low ki672w 2 weeks after starting treatment ; those patients had a better prognosis at 5 years than those who continued to have a high ki672w ( 84% vs 215% 5 - year recurrence risk )  . 
older age has already been shown to be an independent prognostic factor in breast cancer24 and poetic patients aged at least 70 years had poorer outcomes than those aged below 70 years . 
since a substantial minority ( 26% ) of poai patients had adjuvant chemotherapy , this could be a potential confounding factor in the interpretation of ki672w in relation to prognosis and prediction of the value of endocrine therapy alone . 
in the corresponding groups who received chemotherapy , numbers were insufficient to determine a prognostic ki67 effect or to define a plausible beneficial chemotherapy effect . in the two - thirds of patients below the age of 70 years not receiving chemotherapy , the overall outcome in terms of recurrence risk was better , probably reflecting the choice of omitting chemotherapy for better prognosis patients . 
but the key point was that in this population of patients non - confounded by chemotherapy , 21% with high ki67b remained high at surgery ( highhigh ) and those had 112% 5 - year recurrence risk ( arguably meriting chemotherapy in addition ) , compared with the lowlow groups in which recurrence by 5 years was only 16% and the highlow group in which recurrence by 5 years was only 29% ( indicating that additional chemotherapy would be of no clinically relevant benefit )  . 
 this exploratory outcome must be interpreted with caution but further supports the prognostic value of measuring ki67 at 2 weeks . similar findings were observed for patients aged at least 70 years . 
in those 1452 vol 21 november 2020 articles aged at least 70 years who did not receive chemotherapy , there was again a large difference in outcome between the highlow and highhigh groups ( 5 - year recurrence risk 123% vs 345% ) , again supporting the discriminatory power of measuring ki67 at 2 weeks , even though the absolute risks were greater . the prespecified ki672w 10% cut - point was chosen for consistency with ongoing clinical trials ( alternate [ nct01953588 ] ; adapt [ nct01779206 ] )  . 
the relationship of ki672w with recurrence risk is continuous and as illustrated by our analysis by means of ccca , other cutpoints might be selected if appropriate for a specific use ( eg , assessing the value of well - tolerated additional treatment )  . in conclusion , in poetic , giving perioperative endocrine therapy with an aromatase inhibitor had no significant effect on long - term outcome . 
first , we believe that we have identified a subgroup with a low baseline ki67 who have a sufficiently good prognosis that the majority will do well on standard endocrine therapy alone ( except perhaps for a minority as dictated by other clinicalpathological factors ) and who do not require a repeat 2 - week biopsy . 
second , giving poai to the subgroup with high baseline ki67 can differentiate two groups of patients according to their 2 - week ki67 value : those who convert to a low ki67 might not need anything beyond adjuvant endocrine therapy ( taking consideration of other clinical - pathological factors ) , whereas those with a high ki67 that has remained high , should be considered for further adjuvant treatments and trials . 
there are , of course , now several commercially available genomic platforms developed to provide the same kind of prognostic and predictive information for the individual patient.8 , 9 but these tests are expensive , they often involve central testing of tissue , which has to be sent long distances with inevitable time delay , and results can differ between the platforms . 
all authors reviewed the manuscript before submission . declaration of interests md reports grants from cancer research uk , during the conduct of the study ; and personal fees from radius , roche , myriad , orion , g1 therapeutics , nanostring , abbvie , h3 biomedicine , lilly , and the icr rewards for inventors scheme , outside the submitted work . 
 jmb reports grants from cancer research uk , during the conduct of the study ; grants from medivation ; grants and non - financial support from astrazeneca , merck sharp & dohme , puma biotechnology , clovis oncology , pfizer , janssen - cilag , novartis , and roche , outside the submitted work . 
all other authors declare no competing interests . data sharing de - identified data will be made available to other researchers on request , subject to approval of a formal data access request in accordance with the icr - ctsu data and sample access policy . 
trial data is collected , managed , stored , shared , and archived according to icr - ctsu standard operating procedures in order to ensure the enduring quality , integrity , and utility of the data . 
formal requests for data sharing are considered in line with the institute of cancer research clinical trials and statistics unit ( icr - ctsu ) procedures with due regard given to funder and sponsor guidelines . 
data recipients are required to enter a formal data sharing agreement which describes the conditions for release and requirements for data transfer , storage , archiving , publication and intellectual property . 
additional documents might be shared if approved by the tmg and trial steering committee ( eg , statistical analysis plan and informed consent form )  . acknowledgments poetic is co - sponsored by the institute of cancer research and the royal marsden nhs foundation trust . 
we are grateful for the support from the national institute for health research ( nihr ) clinical research network and for the study grant from cancer research uk ( cruk / 07 / 015 grant reference a8671 )  . 
the poetic trial represents independent research supported by the national institute for health research biomedical research centre at the royal marsden nhs foundation trust and the institute of cancer research , london . 
we thank all the patients and their families who participated in this study , all staff involved at the 132 participating hospitals , the staff involved in the trial at icr - ctsu , ralph lauren centre for breast cancer research at the royal marsden nhs foundation trust , and the centre for molecular pathology at the institute of cancer research . 
finally , we thank the past and present colleagues on the poetic trial management group , and the poetic independent data monitoring committee and trial steering committee . correction to lancet oncol 2020 ; 21 : 26170 correction to lancet oncol 2020 ; 21 : 80820 correction to lancet oncol 2020 ; 21 : 92334 blay j - y , serrano c , heinrich mc , et al . 
quality of life in patients with cervical cancer after open versus minimally invasive radical hysterectomy ( lacc ) : a secondary outcome of a multicentre , randomised , open - label , phase 3 , noninferiority trial . 
this correction has been made to the online version as of june 29 , 2020 . vol 21 july 2020 e341 corrections correction to lancet oncol 2019 ; 20 : 38393 correction to lancet oncol 2019 ; 20 : 134959 correction to lancet oncol 2019 ; 20 : e64552 oar a , moraes fy , romero y , ilbawi a , yap ml . 
 lancet oncol 2019 ; 20 : 38393in table 2 of this article , data in the any adverse event , n ( % ) row were corrected for the grade 3 and grade 4 columns . 
these corrections have been made to the online version as of dec 2 , 2019 . correction to lancet oncol 2019 ; 20 : 134244 oladeru ot , perni s , williams b . 
 this correction has been made to the online version as of dec 2 , 2019 . correction to lancet oncol 2019 ; 20 : 154455 infante naing a , wong dj , jr , et al . 
the appendix has been updated as of dec 2 , 2019 . vol 20 december 2019 e663 correction despite state of the art normal imaging , 37 ( 52% ) of 71 patients who underwent second - look laparotomy had macroscopic peritoneal disease reported by the surgeon , and in four patients this disease was not resectable . 
perhaps surprisingly , only 26 ( 70% ) of the 37 cases of metastases suspected by the surgeons were confirmed pathologically , presumably due to chemotherapy down staging or alternative diagnoses.9 the main finding in prophylochip was no difference in disease - free survival between patients receiving active surveillance versus second - look surgery plus hipec . 
after a median follow - up of 508 months ( iqr 470548 ) , 3 - year disease - free survival was 53% ( 95%ci 4164 ) in the surveillance group versus 44% ( 3356 ) in the second - look surgery group ( hazard ratio 097 [ 95% ci 061156 ] ; p = 082 )  . 
this trial has finally answered a longstanding question : should groups at high risk of colorectal peritoneal metastases have second - look surgery ? the answer is clearly no , provided that primary surgery has been optimal and complete . 
 recent results of randomised trials6 , 8 allows for important observations : complete tumour removal by surgeons experienced in the principles and practice of cytoreductive surgery is crucial ; low - volume imaging does not detect peritoneal disease ; and high - risk features can predict peritoneal recurrence . 
congratulations to my french colleagues for showing in two elegant complex trials that optimal surgery is the best treatment for colorectal peritoneal metastases and that second - look surgery is not required , provided that primary surgery is optimal . 
perhaps follow - up should be intensified for high - risk groups , but all oncologists , surgeons , and combining these two the multidisciplinary teams should be very aware that no imaging modality is sensitive , or specific , for peritoneal metastases . 
second - look surgery plus hyperthermic intraperitoneal chemotherapy versus surveillance in patients at high risk of developing colorectal peritoneal metastases ( prophylochipprodige 15 ) : a randomised , phase 3 study . 
proc am soc clin oncol 2018 ; 36 ( suppl ) : lba3503 . panagiotopoulou ig , shah n , rowaiye b , chandrakumaran k , carr nj , moran b . 
 colorectal dis 2019 ; 21 : 88693 . final results of the uk age trial on breast cancer screening age in the lancet oncology , the findings from a 23 - year follow - up of the uk age trial are presented by stephen duffy and colleagues.1 no difference mortality from breast cancer was found between the group that began yearly mammography screening at age 3941 years until they entered the national health service ( nhs ) breast screening programme at age 5052 years , and a group that did not begin mammography screening until they entered the nhs breast screening programme ( 126 deaths vs 255 deaths occurring after more than 10 years of follow - up ; relative rate 098 [ 95% ci 079122 ] ; p = 086 )  . the trial was well conducted , utilising the facilities of the centres already participating in the nhs breast screening programme that had the capacity to screen additional women . 
as participating women were flagged with the nhs central register , mortality from breast cancer in the compared groups could be accurately ascertained . unfortunately , the debate over whether to initiate breast screening at age 40 or 50 years will not have published online august 12 , 2020 s1470 - 2045 ( 20 ) 30428 - 9 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on september 1 , 2020 see articles page 1165 vol 21 september 2020 1125 comment been resolved by the uk age trial , as the lack of a control group who were not offered screening at any age precluded determining whether either group in the trial derived any benefit . 
although there is the possibility that in the intervention group ( screening initiated at age 3941 years ) some person - years were saved by the earlier detection of breast cancer than in the control group , overall there was no mortality reduction in the intervention group compared to the control group by the end of follow - up . 
those who favour screening will be left with a conundrum , but those who believe that mammography screening has little or no benefit will feel their views have been justified . one surprising aspect of the report by duffy and colleagues is the conclusion that no overdiagnosis of breast cancer occurred in either group beyond that which would occur when screening those aged 50 years and older . 
we also confirmed that adjuvant chemotherapy was used , but found no benefit from mammography screening , 6 and instead found a harmful effect , especially from overdiagnosis.7 thus , although duffy and colleagues should be com mended for providing long - term data from a well conducted study , it could be argued that breast screening with mammography should not be initiated at any age , but rather women should be encouraged to practise breast awareness , with mammography used as a diagnostic test , while always remembering that in young women mammography can be negative even in the presence of physically detectable breast cancer . 
geneva : world health organization , 2017 . chemoradiotherapy plus a smac mimetic for locally advanced squamous cell carcinoma of the head and neck published online august 3 , 2020 s1470 - 2045 ( 20 ) 30383 - 1 see articles page 1173 led to the availability of checkpoint inhibitors has substantial progress in the treatment of patients with recurrent or metastatic squamous cell carcinoma of the head and neck . 
 however , the treatment outcome of locoregionally advanced squamous cell carcinoma of the head and neck , traditionally associated with alcohol and nicotine 1126 vol 21 september 2020 comment olaparib in patients with metastatic castration - resistant prostate cancer with dna repair gene aberrations ( toparp - b ) : a multicentre , open - label , randomised , phase 2 trial joaquin mateo * , nuria porta * , diletta bianchini , ursula mcgovern , tony elliott , robert jones , isabel syndikus , christy ralph , suneil jain , mohini varughese , omi parikh , simon crabb , angus robinson , duncan mclaren , alison birtle , jacob tanguay , susana miranda , ines figueiredo , george seed , claudia bertan , penny flohr , berni ebbs , pasquale rescigno , gemma fowler , ana ferreira , ruth riisnaes , rita pereira , andra curcean , robert chandler , matthew clarke , bora gurel , mateus crespo , daniel nava rodrigues , shahneen sandhu , aude espinasse , peter chatfield , nina tunariu , wei yuan , emma hall , suzanne carreira , johann s de bono summary background metastatic castration - resistant prostate cancer is enriched in dna damage response ( ddr ) gene aberrations . 
the toparp - b trial aims to prospectively validate the association between ddr gene aberrations and response to olaparib in metastatic castration - resistant prostate cancer . methods in this open - label , investigator - initiated , randomised phase 2 trial following a selection ( or pick - thewinner ) design , we recruited participants from 17 uk hospitals . 
men aged 18 years or older with progressing metastatic castration - resistant prostate cancer previously treated with one or two taxane chemotherapy regimens and with an eastern cooperative oncology group performance status of 2 or less had tumour biopsies tested with targeted sequencing . 
patients with ddr gene aberrations were randomly assigned ( 1 : 1 ) by a computer - generated minimisation method , with balancing for circulating tumour cell count at screening , to receive 400 mg or 300 mg olaparib twice daily , given continuously in 4 - week cycles until disease progression or unacceptable toxicity . 
the primary endpoint of confirmed response was defined as a composite of all patients presenting with any of the following outcomes : radiological objective response ( as assessed by response evaluation criteria in solid tumors 1.1 ) , a decrease in prostate - specific antigen ( psa ) of 50% or more ( psa50 ) from baseline , or conversion of circulating tumour cell count ( from 5 cells per 75 ml blood at baseline to < 5 cells per 75 ml blood )  . 
recruitment for the trial has completed and follow - up is ongoing . findings 711 patients consented for targeted screening between april 1 , 2015 , and aug 30 , 2018 . 
161 patients had ddr gene aberrations , 98 of whom were randomly assigned and treated ( 49 patients for each olaparib dose ) , with 92 evaluable for the primary endpoint ( 46 patients for each olaparib dose )  . 
confirmed composite response was achieved in 25 ( 543% ; 95% ci 390691 ) of 46 evaluable patients in the 400 mg cohort , and 18 ( 391% ; 251546 ) of 46 evaluable patients in the 300 mg cohort . 
radiological response was achieved in eight ( 242% ; 111423 ) of 33 evaluable patients in the 400 mg cohort and six ( 162% ; 62320 ) of 37 in the 300 mg cohort ; psa50 response was achieved in 17 ( 370% ; 232525 ) of 46 and 13 ( 302% ; 172461 ) of 43 ; and circulating tumour cell count conversion was achieved in 15 ( 536% ; 339725 ) of 28 and 13 ( 481% ; 287681 ) of 27 . 
the most common grade 34 adverse event in both cohorts was anaemia ( 15 [ 31% ] of 49 patients in the 300 mg cohort and 18 [ 37% ] of 49 in the 400 mg cohort )  . 
one death possibly related to treatment ( myocardial infarction ) occurred after 11 days of treatment in the 300 mg cohort . interpretation olaparib has antitumour activity against metastatic castration - resistant prostate cancer with ddr gene aberrations , supporting the implementation of genomic stratification of metastatic castration - resistant prostate cancer in clinical practice . funding cancer research uk , astrazeneca , prostate cancer uk , the prostate cancer foundation , the experimental cancer medicine centres network , and the national institute for health research biomedical research centres . copyright 2019 the author ( s )  . 
before starting this study , several genomic landscape studies were published describing an enrichment for aberrations in dna repair genes in metastatic prostate cancers ( studies identified in pubmed , searching for prostate cancer , genomics , and biopsy , between jan 1 , 2010 and nov 1 , 2015 , with no language restrictions )  . 
preclinical and clinical studies identified in pubmed ( searching for cancer , parp , and brca or dna repair between jan 1 , 2005 and july 1 , 2019 , with no language restrictions ) have established a correlation between different dna repair defects and sensitivity to parp inhibition in different tumour types , leading to drug approvals in ovarian and breast cancer . 
in the toparp - a trial , we identified an association between somatic alterations in dna repair genes and antitumour activity of olaparib in 49 patients with metastatic prostate cancer . 
other clinical trials of parp inhibitors in prostate cancer were identified on the clinicaltrials.gov website , searching for prostate cancer and parp for studies published from database inception to july 1 , 2019 , without language restriction . added value of this study to our knowledge , toparp - b is the first prospective clinical trial in a genomically defined population of patients with metastatic prostate cancer . 
this study has confirmed the antitumour activity of olaparib against metastatic prostate cancer with defective dna repair secondary to either germline or somatic gene inactivation . implications of all the available evidence randomised phase 3 trials for dna repair - defective prostate cancers are now ongoing based on the toparp data . 
our results , if confirmed in registration studies , would support the implementation of tumour genomic testing in clinical practice for treatment stratification in advanced prostate cancer . these drugs have introduction molecular stratification for treatment is not currently the standard of care for metastatic prostate cancers despite evidence of substantial interpatient genomic hetero geneity . 
most therapeutic strategies for advanced prostate cancers target androgen receptor signalling ; taxane based chemotherapies and radiopharmaceuticals are also approved.1 although improved outcomes in the past decade , metastatic prostate cancer remains invariably fatal and new therapeutic strategies involving molecular stratification are urgently needed . 
 genomic studies of metastatic prostate cancer have identified a number of potentially actionable recurrent genomic lossoffunction alterations in dna repair genes in 2025% of cases , such as defects in homologous recombinationmediated repair genes.3 among these , germline or somatic alterations in brca2 are the most common , accounting for 612% of cases across studies.24 these data underpin the evaluation of poly ( adpribose ) polymerase ( parp ) inhibitors in metastatic prostate cancer.5 , 6 aberrations , 24 including olaparib is an orally bioavailable inhibitor of the catalytic activity of parp1 and parp2 , which have key roles in dna damage response ( ddr )  . 
olaparib is approved for the treatment of advanced ovarian and breast cancers associated with germline brca1 or brca2 mutations.7 it is also approved as a maintenance therapy after response to platinumbased chemotherapy for ovarian cancer , indicating benefit from parp inhibition beyond tumours with brca1 / 2 mutations.8 , 9 furthermore , olaparib has antitumour activity in vitro and in vivo in models that are defective in other ddr proteins , including palb2 , atm , fancd2 , rad51 , and rad54 , among others , although the magnitude of preclinical sensitisation varies between proteins , with brca2 loss being arguably the most potent sensitising event.10 , 11 to evaluate the antitumour activity of olaparib against metastatic castrationresistant prostate cancer , we designed toparp , an adaptive programme of serial phase 2 clinical trials aimed at identifying predictive biomarkers for response to parp inhibition in metastatic castrationresistant prostate cancer . 
in the first trial , toparpa , we identified an association between putatively deleterious ddr gene aberrations and res ponse to olaparib in 49 molecularly unselected patients.12 in this article , we present the results of toparpb , which was designed to validate the observed antitumour activity of olaparib in patients with metastatic castration resistant prostate cancer presenting with ddr gene aberrations . methods study design and participants toparpb is a multicentre , openlabel , investigator initiated , randomised phase 2 trial . 
patients were recruited from 17 uk hospitals ( appendix p 2 )  . patients with prostate cancer that had developed metastasis and castration resistance were first registered on the trial for molecular preselection by targeted next generation sequencing ( ngs ) of primary or metastatic prostate cancer biopsies . 
other inclusion criteria included : documented prostate cancer progres sion at trial entry , defined by either rising prostate specific antigen ( psa ) serum concentration ( according to the prostate cancer working group 2 [ pcwg2 ] criteria13 ) or radiologically ( according to modified response evaluation criteria in solid tumors [ recist ] version 1.114 or by bone scan as per pcwg2 criteria ) ; a castrate testosterone concentration of less than 50 ng / dl ; an eastern cooperative oncology group ( ecog ) perfor mance status of 2 or less ; and adequate organ function ( including haemoglobin 9 g / dl after a protocol amend ment on march 15 , 2018 [ previously 10 g / dl ] , platelets 100 10 per l , serum creatinine 15 times the institu tional upper limit of normal , and albumin > 25 g / l )  . 
 tumour cells the baseline count ( cellsearch system ; menarini silicon biosystems , castel maggiore , italy ) had to be five cells per 75 ml blood or higher except in patients with radiologically measurable target lesions of 2 cm or more in diameter on the baseline ct scan and a psa concentration of 2 ng / ml or higher on screening . 
the complete study protocol is available in the appendix . treated with parp for circulating the study was approved by the londonsurrey borders research ethics committee ( rec reference 11 / lo / 2019 ) , and cosponsored by the royal marsden nhs foundation trust and the institute of cancer research ( icr ) , london , uk . 
patients provided written informed consent before enrolment , both for the ngs prescreening and treatment stages . randomisation and masking eligible patients were randomly allocated ( 1 : 1 ) to receive olaparib at 300 mg ( approved dose for the tablet formulation in ovarian and breast cancer15 ) or 400 mg twice a day . 
the allocation sequence was generated centrally by a computergenerated mini misation algorithm derived by the icrctsu , with circulating tumour cell count at screening ( 5 cells per 75 ml blood vs < 5 cells per 75 ml blood ) as a balancing factor . 
further details on the sample processing , quality control , bioinformatics pipelines , and panel design are available in the appendix ( pp 57 ) .16 patients previously known to have germline aberrations were eligible only on confirmatory tumour testing by ngs . all patients received oral olaparib ( 300 mg or 400 mg , tablet formulation ) twice daily continuously in 4week cycles until evidence of radiographic progression ( based on recist 1.1 for soft tissue disease , or the appearance of 2 lesions on bone scan ) , unacceptable toxicity according to investigator review , or patient decision to discontinue . 
patients treated with 300 mg twice daily were offered the option of dose escalation to 400 mg twice daily on confirmation of radiographic progression , providing the escalation was considered to be clinically indicated by the treating physician and the patient had not previously required a dose reduction for management of toxicity . examination , routine blood clinical assessments , including reviews of adverse events ( according to the national cancer institute common terminology criteria for adverse events [ ctcae ] version 4.02 ) and ecog performance status , physical tests and ( haematology and biochemistry ) , took place 2 weeks after the start of treatment , and then at the start of every new 4week cycle . 
local radiological response assessments were used for the primary endpoint definition ; all recist 1.1 responses were confirmed by central review by radiologists at icr ( ac and nt )  . 
circulating tumour cell counts were centrally analysed at the cancer biomarkers laboratory at icr ( by pf , be , and gf ) and results were not made available to the treating physician . 
psa serum measure ments were collected every cycle if available , and every 164 vol 21 january 2020 articles 12 weeks at a minimu blood samples for correlative biomarker studies were taken every 4 weeks . 
to be judged a response confirmation in a second consecutive assessment at least 4 weeks later was required . secondary endpoints were : radiographic progression free survival , defined as the time from randomisation to first evidence of radiographic progression ( according to recist 1.1 or bone scan as per pcwg2 criteria ) or death ; time to radiographic progression , defined as the time from randomisation to first evidence of radiographic progression ; progressionfree survival , defined as the time from randomisation to radiographic progression , unequivocal clinical pro gression , or death ; overall survival , defined as the time from randomisation to death from any cause ; time to psa progression , defined as a confirmed increase of 25% or more and an absolute increase of 2 ng / ml or more in psa from the nadir ( pcwg2 ) ; duration of psa response , defined as the time from the first documented psa decrease of 50% or greater to psa progression ; best percentage change in psa from baseline while on treatment ; percentage change in psa from baseline at 12 weeks ( or earlier if therapy was discontinued ) ; proportion of patients with circulating tumour cell count conversion ; and the safety and tolerability profile of olaparib . a prespecified exploratory endpoint was response in patients in whom dose was escalated to 400 mg twice daily after progression on 300 mg twice daily . 
a pharma cokinetics substudy was planned but because of patients declining recruitment it was closed prematurely with no analyses pursued . statistical analysis this trial followed a selection ( or pickthewinner ) design.18 each dose cohort was assessed independently for the primary endpoint . 
the sample size needed to show the minimum desired antitumour activity was determined on the basis of aherns onestage design , with a response of 30% or less for the null hypothesis , and a response of more than 50% for the alternative hypothesis ( onesided level of 005 and a level of 015 )  . 
following the ahern design , if at least 19 ( 43% ) of 44 evaluable patients in a dose cohort responded , then the dose cohort would be considered successful . 
if the 400 mg twice daily dose cohort was deemed successful , the ddr biomarker identified in toparpa , in which all patients received 400 mg twice daily , would be considered validated as being predictive of response . 
no formal interim analyses were planned . for the primary endpoint , the evaluable population was defined as all randomly assigned patients who met all of the eligibility criteria and commenced trial treatment , unless they discontinued treatment prior to 12 weeks for reasons that were not related to the study drug or disease . 
sensitivity analyses of the primary endpoint were done in the intentiontotreat ( itt ) population ( all randomly assigned patients ) and per protocol population ( all evaluable patients who received at least one cycle of olaparib and had no eligibility violations )  . 
a posthoc sensitivity analysis in patients with a circulating tumour cell count of five or more cells per 75 ml blood at baseline was done for comparison with toparpa results . 
toxicity was analysed in all patients who received at least one dose of olaparib , and the worst grades of adverse events that occurred during treatment for each dose cohort are reported . 
serious adverse events and deaths observed within 30 days of the last dose of study treatment were summarised by dose cohort , as well as the exposure to study drug and reasons for discon tinuation , dose modification or interruption , and treatment delay . ( in for analysis of the primary endpoint was triggered when all patients had completed at least 6 months of treat ment the absence of prior discontinuation )  . 
for time to radiographic progression , patients who did not progress radiologically were censored at the last scheduled disease assessment during the study or date of death , whichever occurred first . 
 * non - mutually exclusive subgroups : one patient had brca1 / 2 , cdk12 , and other mutations , and two patients had both palb2 and other mutations ( included in each subgroup )  . 
assessment of ctc count at screening not possible due to ctc kit shortage ; the patient was allowed to be randomly assigned as he had recist 11 measurable disease ; for randomisation ctc count was assumed to be < 5 cells per 75 ml blood but the patient was unevaluable for ctc response . 
five nonmutually exclusive subgroups were predefined : patients with alterations in brca1 / 2 , atm , cdk12 , palb2 , and any other gene related to ddr or associated with parp inhibitor sensitivity . 
the corresponding author had full access to all data in the study and had final responsibility for the decision to submit for publication . to ngs prescreening results between april 1 , 2015 and aug 30 , 2018 , 711 patients consented ( figure 1a )  . 
from 681 patients with at least one sample available , 779 tumour samples were analysed ( 637 [ 82% ] primary tumour samples and 142 [ 18% ] postcastration resistance metastatic biopsies )  . 
 * non - mutually exclusive subgroups : one patient treated at 300 mg had brca1 / 2 , cdk12 , and other mutations , and two patients treated at 300 mg had both palb2 and other mutations . 
one - sided exact binomial 95% confidence intervals . table 2 : overall antitumour activity of olaparib in patients with dna damage response gene aberrations by dose cohort and gene subgroup sample or the sequencing data not fulfilling quality control parameters . of the 592 patients with evaluable tissue samples , 161 ( 27% ) had ddr gene aberrations on the basis of ngs . 
the most commonly detected ddr gene aberrations were mutations or homozygous deletions in brca2 ( 44 [ 7% ] of the 592 patients ) , atm ( 40 [ 7% ] ) , and cdk12 ( 33 [ 6% ] )  . 98 patients with ddr gene aberrations were randomly assigned and treated in the two dose cohorts ( 49 patients in each cohort )  . 
a greater number of participants were recruited than originally planned , at the recommendation of the independent data monitoring committee , to account for six participants ( three in each cohort ) who were deemed not evaluable ( ineligible post randomisation ) for the primary end point analyses . 
baseline features of each gene aberration subgroup are summarised in the appendix ( p 8 )  . 92 patients ( 46 in each dose cohort ) were evaluable for the primary endpoint . 
70 ( 76% ) patients were evaluable for the recist 1.1 response , 89 ( 97% ) for psa response , and 55 ( 60% ) for circulating tumour cell conversion . 
 a confirmed com posite response was observed in 25 ( 543% ; 95% ci 390691 ) of 46 patients in the 400 mg cohort and 18 ( 391% ; 251546 ) of 46 patients in the 300 mg cohort ( p = 014 ; table 2 )  . 
radiological response according to recist 1.1 was observed in eight ( 242% ; 95% ci 111423 ) of 33 evaluable patients in the 400 mg cohort and six ( 162% ; 62320 ) of 37 in the 300 mg cohort ; psa50 response was observed in 17 ( 370% ; 232525 ) of 46 and 13 ( 302% ; 172461 ) of 43 , respectively ; and circulating tumour cell count conversion was observed in 15 ( 536% ; 339725 ) of 28 and 13 ( 481% ; 287681 ) of 27 , respectively . 
based on the first 44 evaluable patients included in each cohort ( as planned initially ) , 25 ( 57% ) confirmed responses were recorded in the 400 mg cohort and 18 ( 41% ) in the 300 mg cohort ; thus , the predefined criteria for success was met for the 400 mg regimen but not for the 300 mg regimen . when including in the analysis only the 55 evalu able patients with a circulating tumour cell count of 5 cells per 75 ml blood at baseline , confirmed composite response was observed in 17 ( 607% ; 95% ci 406785 ) of 28 evaluable patients in the 400 mg cohort and 13 ( 481% ; 287681 ) of 27 in the 300 mg cohort ( appendix p 9 )  . 
in keeping with previous reports , 17 , 20 circulating tumour cell conversions posttreatment were significantly associated with longer radiographic progressionfree survival and overall survival in landmark analyses ( appendix p 15 )  . the best percentage change from baseline in psa concentration and in the sum of target lesions in each patient in the intentiontotreat population are pre sented in figure 2a and 2b . 
at the time of analysis , 45 ( 92% ) of 49 patients on 400 mg olaparib and 46 ( 94% ) of 49 patients on 300 mg olaparib had radio graphic progression or died ; median radiographic progressionfree survival was 55 months ( 95% ci 4483 ) in the 400 mg cohort and 56 months ( 3777 ) in the 300 mg cohort ( figure 2c )  . 
39 ( 80% ) patients on 400 mg and 38 ( 78% ) patients on 300 mg had died , with a median overall survival of 143 months ( 97189 ) in the 400 mg cohort and 101 months ( 90177 ) in the 300 mg cohort . 
 ( d ) swimmers plot of time on treatment for each patient , indicating periods of treatment interruptions , dose reductions , and , in the 300 mg cohort , dose escalations . 
a summary of treatment dose reductions , escalations ( 300 mg cohort ) , interruptions , and discontinuations in each dose cohort is presented in the appendix ( p 10 )  . dose escalation from 300 mg to 400 mg was pursued in 11 patients . 
none of these patients achieved a response after dose escalation . the confirmed composite response , and response by individual components , for each of the predefined gene subgroups are shown in table 2 . 
the brca1 / 2 subgroup had the highest number of responses both for the composite endpoint of confirmed response and across all its component outcomes ( table 2 ) and the longest median radiographic progressionfree survival ( figure 3c ) of all ddr gene aberration subgroups . 
of the 32 patients in the brca1 / 2 subgroup , 13 had germline mutations in brca2 , six somatic mutations in brca2 , 11 homozygous deletions in brca2 , and the remaining two cases had mutations in brca1 ( one germline and one somatic )  . 
 ten patients in the brca1 / 2 subgroup ( five allocated to 400 mg and five to 300 mg ) remained on treatment for more than 1 year . 21 patients with suspected deleterious atm aber rations were treated ( table 1 ; one patient with homozygous deletion and the rest with germline or somatic mutations that are predicted to result in either truncation or missense mutations affecting the kinase domain ) , and 19 were evaluable for response ( table 2 )  . 
conversely , four of seven patients with palb2 mutations responded to treatment ( table 2 )  . 20 patients were evaluated in the subgroup with other gene alterations associated with ddr or parp inhibitor sensitivity ( table 2 )  . 
psa50 responses were seen in two patients : one with a somatic nonsense mutation in fanca and one with a chek2 mutation . the safety population included all 98 patients treated ( table 3 )  . 
the tolerability profile was in line with what has been previously reported for olaparib and other parp inhibitors.2123 the most common grade 34 adverse event in both cohorts was anaemia ( 15 [ 31% ] in the 300 mg cohort and 18 [ 37% ] in the 400 mg cohort )  . 18 ( 37% ) patients in the 400 mg cohort and six ( 12% ) in the 300 mg cohort required at least one dose reduction ( appendix p 10 ) , with anaemia being the most common adverse event leading to dose reductions ( two patients in the 300 mg cohort and nine in the 400 mg cohort )  . 
 overall , 18 ( 19% ) of the 98 patients were permanently discontinued from olaparib treatment due to adverse events ( appendix p 10 ) the most common adverse events leading to discon tinuation were anaemia ( two of five patients who discontinued on 400 mg and five of 13 on 300 mg ) and fatigue ( three on 400 mg and four on 300 mg )  . 107 serious adverse events were 49 ( 50% ) patients ( 300 mg cohort : 49 events in 22 patients ; 400 mg cohort : 58 events in 24 patients ) with 19 serious reported 170 vol 21 january 2020 articles adverse reactions ( possibly related to study drug ; 11 in the 300 mg cohort and eight in the 400 mg cohort ) in 13 patients ( 8 patients in the 300 mg cohort and 5 in the 400 mg cohort )  . 
all other deaths were unrelated to treatment ( n = 76 ; 70 due to disease and six due to other causes )  . discussion the toparpb trial has confirmed the antitumour activity of olaparib against metastatic castrationresistant prostate cancer with specific ddr gene aberrations . 
the number of composite responses observed in the cohort of patients who received 400 mg tablets of olaparib twice daily met the predefined criteria for success , validating the ddr biomarker identified in toparpa as being predictive of response.12 overall , the data suggest that both drug dose and the specific type of ddr gene aberration might influence antitumour activity , given that the composite response at the 300 mg regimen was lower and did not reach the predefined criteria for success . 
the antitumour activity observed varied considerably for different ddr gene aberrations , with the greatest antitumour activity seen in the subgroup with brca1 / 2 alterations . despite randomisation , cdk12 aberrations were imbalanced between the cohorts , with an enrichment in the 300 mg cohort . 
this imbalance might explain , at least in part , the inferior composite response in the 300 mg cohort.4 , 24 the rationale to explore the two doses originated from prior clinical observations indicating a doseresponse relationship for olaparib between 100 mg and 400 mg at twice daily dosing , although 400 mg has been associated with enhanced toxicity.25 , 26 in keeping with this finding , 37% patients at 400 mg had to reduce their dose to 300 mg , most commonly because of anaemia . 
all of these data would need to be considered when assessing the optimal dose of olaparib for prostate cancer treatment . our results support the implementation of routine genomic testing of metastatic prostate cancer , to detect dna repair defects for targeting by parp inhibition . 
 * one death due to myocardial infarction ( grade 5 event deemed a suspected unexpected serious adverse reaction ) was reported ( not included in table )  . table 3 : treatment - emergent adverse events germline ngs testing in all men with metastatic prostate cancer per national comprehensive cancer network guidelines . 
the antitumour activity of olaparib indicated in this trial , in patients with metastatic castration resistant prostate cancer with both germline and somatic aberrations of brca2 , now supports the implementation of ngs testing of tumour samples . antitumour activity was also observed in other ddr gene aberration subgroups . 
circulating conversely , germline and somatic atm aberrations are common in metastatic prostate cancer ; atm functions as a cell cycle checkpoint , preventing cell cycle progression in the presence of dna damage rather than directly mediating repair , unlike brca2 and palb2 . 
in the toparpa trial , five patients had atm aberrations in tumour biopsies : two of these had a psa response , and two more had circulating tumour cell conversion . 
 preliminary results suggest that rucaparib , another parp inhibitor , results in few psa decreases in patients with atm aberrations.30 in toparpb , we treated 21 patients with suspected deleterious atm aberrations : two achieved a recist or psa response , and several others had circulating tumour cell count conversions following tumour cell count decreases seen in this subgroup were associated with increased duration on the trial , tumour shrinkage per recist , and a psa decrease , as was the case for the overall toparpb population , with circulating tumour cell conversions robustly associating with increased radiographic progressionfree survival and overall survival . 
overall , the data suggest that the antitumour activity of olaparib in metastatic castrationresistant prostate cancer with atm loss is less than that for brcaaltered tumours ; nevertheless , a subset of patients with atm - altered metastatic castrationresistant prostate cancer appear to derive benefit . 
further studies , as well as the study of rational drug combinations , are now needed to elucidate how to best evaluate and treat metastatic castrationresistant prostate cancer with atm alter ations . 
furthermore , because all patients in our study had ddr gene aberrations and received olaparib , we are not able to fully differentiate the predictive value versus the prognostic effect of the gene aberrations in terms of survival . 
randomised trials including patients with and without the biomarkers will be more able to clinically qualify putative predictive biomarkers . nonetheless , the results from toparpb have overall driven the design and conduct of several registration trials of parp inhibitors in metastatic castration resistant prostate cancer ( nct02987543 , nct02975934 , and nct03148795 ) , which are likely to guide the clinical use of parp inhibitors in metastatic prostate cancer in the future . 
other studies , in parallel , are exploring the addition of parp inhibitors to the standardofcare drugs targeting the androgen receptor ( nct03732820 and nct03395197 ) , on the basis of results from a phase 2 clinical trial indicating that a broader target population than just patients with gene aberrations might benefit from these drugs.31 in conclusion , the data from toparpb have confirmed the antitumour activity of olaparib against meta static prostate cancer with particular ddr gene aberrations . 
the high response observed in patients with metastatic castrationresistant prostate cancer with germline or somatic brca1 / 2 aberrations , and the durability of many of these responses , support the use of olaparib in this subpopulation . 
the antitumour activity observed against tumours with atm , palb2 , fanca , or chek2 aberrations suggest that parp inhibitors might have a role as single drug therapies or in rational combinations against these other subtypes of metastatic prostate cancer , although further data are needed to precisely assess the clinical relevance of each of these different ddr gene aberrations in prostate cancer . contributors jm , np , ss , eh , and jsdb designed the trial . 
rj reports grants and personal fees from astellas , astrazeneca , exelixis , and roche ; personal fees and nonfinancial support from bristolmyers squibb , janssen pharmaceutica , ipsen , and merck sharp & dohme ; grants , personal fees , and nonfinancial support from bayer ; and personal fees from merck serono , novartis , pfizer , sanofi genzyme , and eusa , outside of the submitted work . 
ab reports advisory board fees and speaker fees from sanofi and bayer , advisory board fees from astellas , speaker fees from janssen pharmaceutica , merck sharp & dohme , and roche , and provision of educational support to janssen pharmaceutica , outside of the submitted work . 
ss reports grants and consultancy honoraria from bristolmyers squibb , merck sharp & dohme , and roche , and grants from endocyte and astrazeneca , outside of the submitted work . 
she also reports grants and nonfinancial support from merck sharp & dohme , astrazeneca , and bayer ; and grants from janssen pharmaceutica , kyowa kirin , alliance pharma , sanofi , and accuray , outside of the submitted work . 
 he also reports personal fees and nonfinancial support from astellas pharma , sanofi , and menarini silicon biosystems ; grants , personal fees , and nonfinancial support from astrazeneca , daiichi , sierra oncology , and cellcentric ; personal fees from genentech , pfizer , bayer , boehringer ingelheim , merck serono , and merck sharp & dohme ; and nonfinancial support from genmab , glaxosmithkline , orion pharma , qiagen , taiho pharmaceutical , and vertex , outside of the submitted work . 
jsdb has an abiraterone rewards to inventors patent with royalties paid to the institute of cancer research ( icr ; london , uk ) , and a parp inhibitors and dna repair defects patent with royalties paid to icr . 
the authors affiliated to icr disclose that the institution is a joint applicant for the patent entitled dna damage repair inhibitors for treatment of cancer , which includes the granted application us8143241 . 
 all other authors declare no competing interests . data sharing the institute of cancer research clinical trials and statistics unit ( icrctsu ) , london , uk , supports the wider dissemination of information from the research it does , and increased cooperation between investigators . 
trial data is collected , managed , stored , shared , and archived according to icrctsu standard operating procedures to ensure the enduring quality , integrity , and use of the data . 
data recipients are required to enter a formal data sharing agreement that describes the conditions for release and requirements for data transfer , storage , archiving , publication , and intellectual property . 
data sharing is permitted if proposed projects have a sound scientific or patient benefit rationale as agreed by the trial management group and approved by the icrctsu independent data monitoring and steering committee as required . 
 additionally , all indirect identifiers that might lead to deductive disclosures will be removed in line with cancer research uk data sharing guidelines . acknowledgments we are grateful for the support and funding from astrazeneca , and for the study grants from cancer research uk ( cruk / 11 / 029 , c12540 / a12829 , c12540 / a13230 , and c12540 / a20447 ) , prostate cancer uk and the movember foundation through the london movember centre of excellence ( ceo13_2002 ) , and the prostate cancer foundation ( 20131017 )  . 
the institute of cancer research ( icr ) clinical trials and statistics unit ( icrctsu ) , london , uk , also receives programme grant funding from cancer research uk ( c1491 / a15955 and c1491 / a25351 )  . 
we also acknowledge support from the uk national institute for health research ( nihr ) cancer research network and the uk national health service ( nhs ) funding to the nihr biomedical research centre at the royal marsden nhs foundation trust and icr ( london , uk ) , and support from the uk experimental cancer medicine centres network . 
the views expressed in this article are those of the author ( s ) and not necessarily those of the uk national health service , the nihr , or the uk department of health . 
we thank all patients and their families for participating in this study , all staff involved at the vol 21 january 2020 articles 17 participating hospitals , and the staff involved in the trial at the cancer biomarkers group at icr , at the prostate cancer targeted therapy group at the royal marsden hospital ( london , uk ) , and at icrctsu . 
 finally , we thank the past and present colleagues of the toparp trial management group , the toparpb independent data monitoring committee , and the icrctsu steering committee for trials in metastatic castrationresistant prostate cancer . articles conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial david dearnaley , isabel syndikus , helen mossop , vincent khoo , alison birtle , david bloom eld , john graham , peter kirkbride , john logue , zafar malik , julian money - kyrle , joe m osullivan , miguel panades , chris parker , helen patterson * , christopher scrase , john sta urth , andrew stockdale , jean tremlett , margaret bidmead , helen mayles , olivia naismith , chris south , annie gao , clare cruickshank , shama hassan , julia pugh , clare gri n , emma hall , on behalf of the chhip investigators summary background prostate cancer might have high radiation - fraction sensitivity that would give a therapeutic advantage to hypofractionated treatment . 
we present a pre - planned analysis of the e cacy and side - e ects of a randomised trial comparing conventional and hypofractionated radiotherapy after 5 years follow - up . methods chhip is a randomised , phase 3 , non - inferiority trial that recruited men with localised prostate cancer ( pt1bt3an0m0 )  . 
patients were randomly assigned ( 1 : 1 : 1 ) to conventional ( 74 gy delivered in 37 fractions over 74 weeks ) or one of two hypofractionated schedules ( 60 gy in 20 fractions over 4 weeks or 57 gy in 19 fractions over 38 weeks ) all delivered with intensity - modulated techniques . 
randomisation was by computer - generated random permuted blocks , strati ed by national comprehensive cancer network ( nccn ) risk group and radiotherapy treatment centre , and treatment allocation was not masked . 
the chhip trial is registered as an international standard randomised controlled trial , number isrctn97182923 . findings between oct 18 , 2002 , and june 17 , 2011 , 3216 men were enrolled from 71 centres and randomly assigned ( 74 gy group , 1065 patients ; 60 gy group , 1074 patients ; 57 gy group , 1077 patients )  . 
the proportion of patients who were biochemical or clinical failure free at 5 years was 883% ( 95% ci 860902 ) in the 74 gy group , 906% ( 885923 ) in the 60 gy group , and 859% ( 834880 ) in the 57 gy group . 
there were no signi cant di erences in either the proportion or cumulative incidence of side - e ects 5 years after treatment using three clinician - reported as well as patient - reported outcome measures . 
the estimated cumulative 5 year incidence of radiation therapy oncology group ( rtog ) grade 2 or worse bowel and bladder adverse events was 137% ( 111 events ) and 91% ( 66 events ) in the 74 gy group , 119% ( 105 events ) and 117% ( 88 events ) in the 60 gy group , 113% ( 95 events ) and 66% ( 57 events ) in the 57 gy group , respectively . 
open access article distributed under the terms of cc by . introduction prostate cancer is the most common cancer in men in the uk , with 41 736 new cases in 2011.1 since the introduction of prostate - speci c antigen ( psa ) testing , most men diagnosed have localised disease . 
management options include external - beam radiotherapy , brachytherapy , radical prostatectomy , active surveillance ( for men with low - risk disease ) , and watchful waiting ( for those unsuitable for radical curative treatment ) , with management choices often a ected by potential treat ment - related toxic e ects . 
 prostate cancer and its treatment are the leading cause of cancer years lived with disability.2 lancet oncol 2016 ; 17 : 104760 published online june 20 , 2016 s1470 - 2045 ( 16 ) 30102 - 4 this online publication has been corrected . 
 before the chhip trial began , reports based on retrospective series of patients suggested that the / ratio for prostate cancer might be low , but only two small randomised trials had tested hypofractionation compared with conventional fractionation , both using relatively low doses of radiotherapy , and neither trial was large enough to conrm or refute a benet . 
 since chhip started , more recent results from a meta - analysis of ve small trials testing hypofractionation and retrospective reviews of large patient databases have been done , suggesting that the best estimates for the / ratio are between 14 gy and 19 gy , although estimates up to 83 gy have been calculated . 
meta - analyses of studies of dose - escalated radiotherapy and neoadjuvant androgen deprivation show improved disease control compared with standard radiotherapy doses , but dose escalation increases bowel side - e ects . 
 however , conformal and intensity - modulated radiotherapy improves dose distributions of radiotherapy and conformal radiotherapy reduces side - e ects . added value of this study the chhip trial is , to our knowledge , the largest randomised treatment study undertaken in localised prostate cancer . 
 we tested two experimental hypofractionated radiotherapy schedules using 3 gy per fraction to total doses of 60 gy and 57 gy compared with standard fractionation using 2 gy per fraction to a total dose of 74 gy . 
we have shown that the hypofractionated schedule of 60 gy in 20 fractions is non - inferior to a standard schedule of 74 gy in 37 fractions for the endpoint of biochemical and clinical disease control . 
 quality controlled imrt techniques were used and the side - e ect pro les were favourable and low in all three randomised groups . interpretation the ndings from this pre - planned analysis of the chhip trial show that the hypofractionated imrt schedule giving 60 gy in 3 gy fractions in 4 weeks is both e ective and safe and can be recommended as a new standard of care for patients with localised prostate cancer using the high - quality radiotherapy techniques described . 
the results are most robust for patients with intermediate - risk disease who received short - course androgen deprivation therapy . external - beam radiotherapy is most appropriate for men with intermediate - risk or high - risk disease , 3 and is associated with long - term disease control in most patients.4 about 15 800 men receive radical prostate radiotherapy in the uk every year ( ball c , national clinical analysis and specialised applications team , the clatterbridge cancer centre nhs foundation trust , personal communication )  . 
several phase 3 randomised controlled trials have shown the bene t of dose escalation5 , 6 and high - dose conformal radiotherapy with conventional 2 gy daily fractions to a total dose of 74 gy is the standard of care in the uk.7 however , a that high - dose radiotherapy meta - analysis showed ( 7480 gy ) is associated with an increased risk ( odds ratio 158 ) of late gastrointestinal toxicity of grade 2 or more compared with lower doses of radiotherapy ( 64702 gy ) .8 therefore , it is important to use advanced radiotherapy techniques that are able to sculpt dose distributions to the prostate target and avoid the organs at risk . additionally , there has been interest in the fraction sensitivity of prostate cancer.911 the association between total isoe ective radiation dose and fraction size is described by a linear quadratic model which uses two constants : and  . 
however , for prostate cancer , a value as low as 15 gy has been suggested , which is lower than the 3 gy reported for the late reactions of most normal tissues ( including rectum ) .12 these ndings have potentially important therapeutic implications . 
hypofractionated radiotherapy , giving fewer fractions each with a higher dose , might improve the therapeutic ratio , resource use , and patient convenience . the main aims of the chhip trial ( cruk / 06 / 016 ) were to compare the e cacy and toxicity of conventional and hypofractionated radiotherapy using high - quality radiation techniques . methods study design and participants chhip is an international , multicentre , randomised , phase 3 , non - inferiority trial comparing the conventionally fractionated schedule of 74 gy in 37 fractions with two experimental hypofractionated schedules of 60 gy in 20 fractions and 57 gy in 19 fractions in men with localised prostate cancer . 
safety of the 3 gy ( fraction ) schedules was reported after a pre - planned analysis of the rst 457 men recruited.13 here , we report primary e cacy results and further comparative safety data . men older than 16 years who had histologically con rmed t1bt3an0m0 prostate cancer and a who performance status of 0 or 1 were eligible . 
 1048 vol 17 august 2016 articles see online for appendix on aug 1 , 2006 , after 454 patients had been recruited , these criteria were revised to re ect the developing consensus on use of long - term androgen deprivation in locally advanced disease . 
other exclusion criteria included previous pelvic radiotherapy or radical prostatectomy , previous androgen suppression , another active malignancy in the past 5 years ( other than cutaneous basal - cell carcinoma ) , comorbid conditions precluding radical radiotherapy , hip prosthesis ( criterion amended to bilateral hip prosthesis jan 30 , 2009 ) , and full anticoagulation treatment ( criterion removed july 1 , 2009 )  . 
full details of trial design , eligibility , and treatment have been reported previously.13 the protocol is available in the appendix ( pp 2790 )  . the the study was approved in the uk by the london multi - centre research ethics committee ( 04 / mre02 / 10 ) and by institutional research board of each participating international site . 
the institute of cancer research clinical trials and statistics unit ( icr - ctsu ; london , uk ) coordinated the study and carried out central statistical data monitoring and all analyses . 
following registration , and within 46 weeks before radiotherapy , patients were randomly assigned ( 1 : 1 : 1 ) to receive conventional fractionation ( control ) or one of two hypofractionated schedules . 
computer - generated random permuted blocks of sizes six and nine were used , strati ed by ( nccn ) national comprehensive cancer network risk - classi cation ( low vs intermediate vs high ) 3 and radiotherapy treatment centre . 
it was not possible to mask patients or clinicians to treatment allocation . procedures short - course androgen deprivation treatment was given for 36 months before and during radiotherapy ; this was optional for patients with low - risk disease . 
 received individuals the experimental groups combined with every month , hypofractionated treatment with 3 gy daily fractions to a total dose of either 60 gy in 20 fractions in 40 weeks ( 28 days ) or 57 gy in 19 fractions in 38 weeks ( 27 days )  . 
 biological doses in the hypofractionated schedules were calculated to be equivalent to those in the conventional schedule assuming / ratios of 24 gy for the 60 gy group and 14 gy for the 57 gy group . 
treatment delays for toxic e ects , and for technical reasons of up to 5 days , were permitted . planning of radiotherapy treatment for all three groups was done with forward or inverse three - dimensional methods about 12 weeks after the start of hormonal treatment . 
 portal imaging was used to verify treatment accuracy , which was to be within 3 mm and was taken at least three times during week 1 and at least weekly intervals thereafter . 
the integral quality - assurance programme has previously been described.13 staging investigations included psa measurement , standard haematology and biochemistry , lymph node assessment by pelvic mri or ct , and bone scans for patients at intermediate or high risk . 
histology was locally assessed with diagnostic transrectal ultrasoundguided biopsies ( or specimens from transurethral resection of the prostate ) and reported with the gleason syste psa concentrations were recorded before commencement of androgen deprivation therapy and radiotherapy and subsequently at weeks 10 , 18 , and 26 after radiotherapy and then at 6 - month intervals for 5 years and subsequently annually . baseline , pre - radiotherapy treatment , acute , and late toxicity data were collected using physician - completed and patient - reported outcome questionnaires . 
instruments chosen re ected practice at the time of trial commencement , the desirability of assessing symptoms before radiotherapy to allow consideration of emergent events , and to facilitate comparison with other studies . 
 baseline bowel , bladder , and sexual function assessments were made before androgen deprivation therapy and radiotherapy and were graded using the late e ects on normal tissues : subjective / objective / management ( lent / som ) 17 and royal marsden hospital ( rmh ) 18 outcome scoring patient - reported systems and vol 17 august 2016 1049 articles questionnaires . 
when the sample size was increased ( see statistical analysis ) it was felt that su cient data had been collected on acute toxicity to allow robust conclusions to be drawn about comparisons between the three randomised groups . 
reactions were graded every week during radiotherapy and at weeks 10 , 12 , and 18 from radiotherapy start date using the radiation therapy oncology group ( rtog ) scoring system for acute toxicity.19 late side - e ects were then the start of assessed beginning 26 weeks after radiotherapy and every 6 months for 2 years and then yearly to 5 years , as previously described , 13 using the rtog grades late side - e ects , 19 rmh , and lent / som scoring systems . 
a quality - of - life substudy using patient - reported outcomes was included as previously described.20 from trial initiation to early 2009 , the ucla - pci , including the short form 36 ( sf - 36 ) , and the functional assessment of cancer therapy - prostate ( fact - p ) quality - of - life instruments were used . 
after a protocol amendment on march 12 , 2009 , the expanded prostate cancer index composite ( epic ) and short form 12 ( sf - 12 ) instruments replaced ucla - pci , sf - 36 , and fact - p due to epic becoming the patient - reported outcome measure of choice . 
patient - reported outcomes to 2 years after treatment have been reported.20 for outcomes the primary outcome measure was time to biochemical or clinical failure , de ned as the time from randomisation to biochemical failure or prostate cancer recurrence . 
 the initial de nition of biochemical failure ( psa > 2 ng / ml 6 months or more after the commencement of radiotherapy and a psa rising by 50% or more from the nadir ) was updated in 2007 , and applied retrospectively , to re ect the phoenix consensus guidelines as a psa concentration greater than nadir plus 2 ng / ml.21 the nadir psa was the lowest concentration recorded at any time after commencement of androgen deprivation therapy or radiotherapy . 
prostate cancer recurrence events were as reported by the investigator and included recommencement of androgen deprivation therapy , local recurrence , lymph node or pelvic recurrence , and distant metastases . secondary e cacy outcome measures were disease - free survival ( time from randomisation to any prostate cancer - related event or death from any cause ) ; overall survival ( time from randomisation to death from any cause ) ; development of metastases ; and recommencement of hormonal treatment for disease recurrence . 
cause of death was centrally reviewed by a panel of three trial investigators ( dd , jg , is ) , masked to treatment allocation . additional secondary endpoints were acute and late side - e ects . 
clinician - reported late toxicity outcomes were the proportion of patients with a grade 2 or worse toxic e ect at 2 and 5 years , and time to development of grade 1 , grade 2 , and grade 3 toxicity ( assessed using each scoring method )  . 
patient - reported outcomes included overall bowel , bladder , and sexual dysfunction bother reported as single items on the ucla - pci and epic - 50 instruments . and conventional statistical analysis the trial was powered to assess non - inferiority in biochemical or clinical failure - free rate between the hypofractionated radiotherapy schedules . 
 we assumed a 70% failure - free rate at 5 years in the control group and , with 2163 patients , initially wished to exclude a decrease of 6% in a hypofractionated group . 
 due to accrual exceeding expectations , a protocol amendment on nov 23 , 2009 , increased the sample size to allow a smaller non - inferiority margin of 5% , corresponding to a critical hazard ratio ( hr ) of 1208 , to be used . 
this analysis would require 349 events in the control group but , as agreed with the independent data monitoring committee , data could also be considered su ciently mature for analysis after a median follow - up of 5 years . 
a small allowance ( 15% ) for dropout or loss to follow - up was incorporated . analyses for all time - to - event endpoints were on an intention - to - treat basis . 
 for development of metastases and recommencement of hormonal treatment patients were censored at the date they were last seen or date of death . kaplan - meier methods were used to estimate event rates . 
estimates of treatment e ect were made using unadjusted and also adjusted cox regression models , with an hr less than 1 indicating a decreased risk of the event in the hypofractionated treatment group compared with control . 
covariates included in adjusted cox regression models were age ( 69 years vs > 69 years ) , nccn risk group ( low vs intermediate vs high ) , gleason score ( 6 vs > 6 ) , clinical stage , and pre - androgen deprivation therapy psa ( < 10 ng / ml vs 1020 ng / ml vs > 20 ng / ml )  . 
although the trial was not designed to 1050 vol 17 august 2016 articles directly compare the hypofractionated schedules , hypothesis generating comparisons have been made , with an hr less than 1 indicating a decreased risk of the event in the 60 gy group compared with the 57 gy group . 
 for time to biochemical or clinical failure , hrs are provided with two - sided 90% cis ( equivalent to one - sided 95% cis ) in accordance with the one - sided non - inferiority design . 
comparisons were made between the control group and each hypofractionated group using the log - rank test , with a p value less than 005 indicating statistical signi cance . ( ) time absolute treatment di erences biochemical or clinical failure have been calculated based on the kaplan - meier estimate of the failure - free rate in the control group and the hr . 
a competing risks analysis was done using the methods of fine and gray for the primary outcome measure , with death due to any cause as the competing event with consistent results ( data not shown )  . 
pre - planned subgroup analyses of the primary outcome by nccn risk group were done in addition to multivariable analyses adjusting for risk group and prespeci ed clinically prognostic factors . 
 * data presented for patients who received androgen deprivation therapy and a start and end date of treatment is known ( n = 950 in the 74 gy group , n = 966 in the 60 gy group , and n = 970 in the 57 gy group )  . 
data presented for patients who received androgen deprivation therapy and started radiotherapy ( n = 1008 in the 74 gy group , n = 1022 in the 60 gy group , and n = 1020 in the 57 gy group )  . 
data presented for patients who started radiotherapy ( n = 1043 in the 74 gy group , n = 1051 in the 60 gy group , and n = 1056 in the 57 gy group )  . table : baseline demographics , clinical characteristics , and treatment details by randomised group comparisons of the distribution of acute toxicity scores were compared using mann - whitney tests . 
 the proportion of small or worse patient - reported bother and time to rst very small , small , moderate , or worse late bother score were analysed as for late toxicity endpoints . 
to make some allowance for multiple testing of toxicity and patient - reported endpoints , a p value of less than 001 was considered statistically signi cant . for all time - to - event analyses the proportional hazards assumption of the cox model was tested using schoenfeld residuals and found to hold ( appendix pp 2526 )  . analyses were based on a database snapshot taken on sept 8 , 2015 , and were done using stata version 13 . 
the chhip trial is registered as an international standard randomised controlled trial , number isrctn97182923 . was estimated10 assuming a linear t for data from the hypofractionated groups . acute toxicity analyses were done in the safety population , including all patients who received at least one fraction of radiotherapy . 
all available data were used irrespective of timing of assessment , with the exception of comparisons at 18 weeks , where a 2 week window either side of the expected date was used . 
pairwise role of the funding source the funding source provided peer - reviewed approval for the trial , but had no other role in study design , collection , analysis , interpretation of data , or writing of the report . 
hmo , cg , and eh also had full access to the data . 1052 vol 17 august 2016 articles results between oct 18 , 2002 , and june 17 , 2011 , 3216 men were recruited from 71 centres in the uk , republic of ireland , switzerland , and new zealand ( appendix pp 1 , 45 )  . 
 1065 patients were assigned to the conventional 74 gy schedule , 1074 to the 60 gy schedule , and 1077 to the 57 gy schedule ; 64 patients received no radiotherapy ( gure 1 )  . 
at the time of analysis , median follow - up was 626 months ( 541772 ) in the 74 gy group , 622 months ( 539772 ) in the 60 gy group , and 624 months ( 537766 ) in the 57 gy group . by 5 years , the number of patients with biochemical or clinical events were 111 of 1065 in the 74 gy group , 88 of 1074 in the 60 gy group , and 132 of 1077 in the 57 gy group , respectively . 
with reference to the critical hr for non - inferiority , 60 gy was non - inferior to 74 gy with hr 084 ( 90% ci 068103 ) , pni = 00018 . 
since the upper limit of the 90% ci for the hr comparing 57 gy with 74 gy ( hr 120 [ 099146 ] ) exceeds 1208 ( pni = 048 ) , non - inferiority of the 57 gy schedule relative to 74 gy cannot be claimed . 
to facilitate comparison with other studies , 95% cis were estimated as 065107 for the hr in the 60 gy group and 096151 for the hr in the 57 gy group . 
the estimated absolute di erence in the proportion of patients in the hypofractionated groups free from biochemical or clinical failure compared with that in the control group at 5 years is = 180% ( 90% ci 034 to 358 ) for 60 gy versus 74 gy and = 220% ( 488 to 008 ) for 57 gy versus 74 gy . 
of 252 deaths reported , 40 ( 16% ) were prostate cancer related , 88 ( 35% ) were due to a second malignancy , 111 ( 44% ) were non - cancer causes , and 13 ( 5% ) were of unknown cause . 
 no signi cant di erences in overall survival were observed between the control group and either of the hypofractionated groups ( gure 2b ; appendix p 6 )  . progression events or death occurred in 209 ( 20% ) of 1065 patients in the 74 gy group , 179 ( 17% ) of 1074 in the 60 gy group , and 227 ( 21% ) of 1077 in the 57 gy group . 
 1054 vol 17 august 2016 articles compared with 74 gy , the hr for disease - free survival was 083 ( 95% ci 068101 ) in the 60 gy group and 108 ( 090131 ) in the 57 gy group . 
androgen deprivation therapy was recommenced in 80 ( 8% ) patients in the 74 gy group , 70 ( 7% ) in the 60 gy group , and 89 ( 8% ) in the 57 gy group . 
time to recommencement of androgen deprivation therapy and development of distant metastases were not signi cantly di erent between either of the hypo fractionated schedules and the 74 gy schedule ( appendix pp 6 , 17 )  . acute rtog bowel and bladder symptoms peaked sooner in the hypofractionated schedules than in the control , at 45 weeks compared with 78 weeks ( gure 4 , appendix p 18 )  . 
there was signi cantly more acute bowel toxicity at the peak in the hypofractionated schedules compared with the control ; the proportion of patients reporting rtog grade 2 or worse bowel toxicity was 176 ( 25% ) of 715 patients with available assessments in the 74 gy group , 277 ( 38% ) of 720 in the 60 gy group ( vs 74 gy , p < 00001 ) , and 270 ( 38% ) of 713 in the 57 gy group ( vs 74 gy , p < 00001 ; gure 4a )  . 
however , the distribution of bladder toxicity by grade was similar across all groups ; the proportion of patients with available assessments reporting rtog grade 2 or worse bladder toxicity was 331 ( 46% ) of 715 in the 74 gy group compared with 356 ( 49% ) of 720 in the 60 gy group ( p = 034 ) , and 327 ( 46% ) of 713 in the 57 gy group ( p = 090 ; gure 4b )  . 
of 592 patients treated with 74 gy with available assessments , 15 ( 3% ) and 34 ( 6% ) reported rtog grade 2 or worse bowel and bladder toxicity , respectively . 
corresponding proportions in the 60 gy group ( 607 patients treated with available assessments ) were 20 ( 3% ) bowel ( p = 038 ) and 30 ( 5% ) bladder ( p = 100 ) , and in the 57 gy group ( 508 patients treated with available assessments ) were 15 ( 3% ) bowel ( p = 060 ) and 30 ( 5% ) bladder ( p = 010 )  . all radiotherapy schedules showed a low frequency of late bowel and bladder side - e ects ( gure 5 , appendix pp 1922 )  . 
2 years from the start of treatment fewer assessable patients treated with 57 gy reported rtog grade 2 or worse bowel symptoms as compared with 74 gy control ( 74 gy , 35 [ 4% ] of 922 vs 57 gy , 17 [ 2% ] of 962 ; p = 00075 ) ; however , no di erence was observed between the 60 gy group ( 28 [ 3% ] of 959 ) and the 74 gy group ( p = 031 ) ; this was evident across all clinician - reported toxicity scales ( rtog , rmh , and lent - som ; gure 5a , appendix pp 8 , 1920 )  . 
sexual dysfunction was 74 gy , grade 1 + 74 gy , grade 2 + 74 gy , grade 3 + 60 gy , grade 1 + 60 gy , grade 2 + 60 gy , grade 3 + 57 gy , grade 1 + 57 gy , grade 2 + 57 gy , grade 3 + number of patients 74 gy 60 gy 57 gy time from start of radiotherapy ( weeks ) number of patients 74 gy 60 gy 57 gy figure 4 : acute rtog toxicity by timepoint and randomised treatment group ( a ) prevalence of bowel toxicity and ( b ) prevalence of bladder toxicity . 
grade 3 + = grade 3 or worse adverse event . common at baseline and increased with androgen deprivation therapy ; although this partially recovered after radiotherapy it remained higher than baseline in all groups ( appendix pp 10 , 13 , 2324 )  . 
the proportion of lent - som grade 2 or worse sexual symptoms at 2 years was similar in each treatment group ( 74 gy , 550 [ 67% ] of 826 assessable patients ; 60 gy , 562 [ 65% ] of 864 [ vs 74 gy , p = 054 ] ; 57 gy , 552 [ 64% ] of 859 , [ vs 74 gy , p = 033 )  . at 5 years post - radiotherapy , the frequency of grade 2 or worse bowel , bladder , and sexual toxicity across clinician - reported toxicity scales was similar across fractionation schedules ( appendix pp 810 )  . 
late toxicity data have been included in analyses if they were reported within 6 weeks of the 6 month visit , within 3 months of the 1224 month visit , and within 6 months of the 3660 month visit . 
for ucla / epic , before androgen deprivation therapy data were included if they were reported within 3 months before starting androgen deprivation therapy and within 1 month after starting androgen deprivation therapy . 
 estimated cumulative incidences of grade 2 or worse bowel toxicity at 5 years measured with the rtog scale were 137% ( 111 events ) for the 74 gy group , 119% ( 105 events ) for the 60 gy group ( hr compared with 74 gy 094 [ 95% ci 072123 ] , p = 065 ) and 113% ( 95 events ) for the 57 gy group ( hr compared with 74 gy 084 1056 vol 17 august 2016 articles [ 064111 ] , p = 022 )  . 
estimated cumulative incidences of grade 2 or worse bladder toxicity at 5 years measured with the rtog scale were 91% ( 66 events ) for the 74 gy group , 117% ( 88 events ) for the 60 gy group ( hr compared with 74 gy 134 [ 95% ci 098185 ] , p = 007 ) and 66% ( 57 events ) for the 57 gy group ( hr 085 [ 060121 ] , p = 037 ; gure 5 , appendix p 9 )  . 
there was a slightly higher frequency of grade 2 or worse bowel and bladder sidee ects in the 60 gy group compared with 57 gy at 2 and 5 years on most clinician - reported scales ( appendix pp 89 )  . 
cumulative incidence of lent - som grade 2 or worse bowel side - e ects was higher in the 60 gy group compared with the 57 gy group ( hr 139 [ 95% ci 114170 ] , p = 00010 ; appendix p 8 ) , but this di erence was not seen with other toxicity scales . 
cumulative incidence of grade 2 or worse rtog bladder toxicity was also greater in the 60 gy group versus the 57 gy group ( hr 158 [ 113220 ] , p = 00073 ; gure 5 , appendix p 9 ) , although this was not seen with other toxicity scales . 
at 5 years , the proportions of patients with rtog grade 3 or worse bowel events were none of 534 patients in the 74 gy group , two ( < 1% ) of 569 patients in the 60 gy group , and three of 549 ( < 1% ) in the 57 gy group ; rtog grade 3 or worse bladder events occurred in two ( < 1% ) of 534 patients in the 74 gy group , four ( < 1% ) of 569 patients in the 60 gy group , and ve ( 1% ) of 549 patients in the 57 gy group . 
the estimated cumulative incidence of grade 3 or worse bowel and bladder adverse events at 5 years was 2% ( 17 events ) and 3% ( 27 events ) in the 74 gy group , 3% ( 20 events ) and 6% ( 38 events ) in the 60 gy group , and 4% ( 23 events ) and 3% ( 21 events ) in the 57 gy group , respectively ( gure 5c , d )  . 
no treatmentrelated deaths were reported . patient - reported outcomes showed no signi cant di erences in the proportion of small or worse bowel , bladder , or sexual bother at 2 or 5 years ( gure 5 , appendix pp 813 )  . 
at 5 years , the proportion of assessable patients reporting small or worse bowel bother was 49 ( 14% ) of 341 in the 74 gy group , 57 ( 15% ) of 375 in the 60 gy group , and 59 ( 15% ) of 387 in the 57 gy group . 
the corresponding gures for bladder bother were 56 ( 17% ) of 333 , 63 ( 17% ) of 371 , and 60 ( 16% ) of 376 , respectively , and for sexual bother were 187 ( 52% ) of 357 , 184 ( 52% ) of 357 and 195 ( 53% ) of 370 , respectively . 
the cumulative incidence of late small or worse bother in each hypofractionated schedule was not signi cantly di erent from control for bowel , bladder , and sexual symptoms , and there were no signi cant di erences between the hypofractionated groups ( gure 5e , f , appendix pp 810 )  . discussion in this pre - planned analysis with a median follow - up of over 5 years , we found that the 60 gy hypofractionated schedule is non - inferior to the 74 gy conventionally fractionated schedule in terms of time to biochemical or clinical failure for patients with localised prostate cancer . 
 evaluation of the lower 57 gy hypofractionated schedule was inconclusive : it cannot be stated to be non - inferior to the 74 gy control group but it was inferior to the 60 gy group . 
notably , the proportion of patients free from biochemical or clinical failure at 5 years in all treatment groups ( 883% for the 74 gy group , 906% for the 60 gy group , and 859% for the 57 gy group ) were considerably higher than the 71% reported for the 74 gy group in the national mrc rt01 trial.6 recent meta - analyses5 , 22 identi ed ve relatively small phase 3 trials comparing modest hypofractionation with conventional 1820 gy fractions . 
there were no consistent the di erences between randomised groups , and investigators concluded that larger trials were required to establish the non - inferiority of hypofractionation for clinical e ectiveness . 
in the chhip trial , we estimate the / ratio to be 18 gy , which is in keeping with previous reports23 and recent large series and meta - analyses which have suggested the / ratio to be between 14 gy and 193 gy.2427 our estimate does not account for any time factor related to overall treatment duration and repopulation.26 the potential e ect of accelerated the improvement in 5 - year disease control for a 3 gy dose di erence between the 57 gy and 60 gy groups is in keeping with the review of the six randomised controlled dose - escalation trials previously reported5 , 6 and a recent meta - analysis of biologically equivalent dose escalation.28 five other contemporary phase 3 studies have reported side - e ects related to hypofractionated radiotherapy2933 ( appendix p 14 )  . 
we initially reported no di erences between the three randomised groups in the frequency of side - e ects in the rst 457 patients recruited to the chhip trial with 2 years follow - up.13 , 20 analysis of acute side - e ects in the full chhip cohort has con rmed no di erence in bladder side - e ects except that the wave of toxicity occurs earlier in the hypofractionated groups . 
however , we have now documented that the peak acute bowel toxicity is greater in patients receiving a hypofractionated schedule , although it is noteworthy that only 2% of patients had grade 3 or worse toxic e ects and only 1% had a prolongation of treatment time of more than 1 week , indicating the hypofractionated schedules . 
an increased acute gastrointestinal reaction in patients treated with hypofractionated radio therapy has been noted by other investigators29 , 32 but not by norkus and colleagues , 33 who treated patients using a 4 day per week schedule . 
the 57 gy group had less grade 1 or worse and grade 2 or worse lent - som bowel and grade 2 or worse rtog bladder side - e ects than the 60 gy group with outcomes on other toxicity scales supporting this e ect , although they were not tolerability of the vol 17 august 2016 1057 articles relate signi cant ; there were no signi cant di erences between the 57 gy and 60 gy groups in sexual function domains . 
 the results are in accord with a recent meta - analysis indicating the general tolerability of hypofractionated radiotherapy , 5 , 22 although two studies have reported approximate doublings of grade 2 gastro intestinal31 or genitourinary30 side - e ects compared with conventional 1820 gy fractions ( appendix p 14 )  . post - radiotherapy symptoms treatment methods , total dose , patient factors , and fractionation schedules . 
the favourable results in the chhip study re ect the mandated radiotherapy technique using an integrated simultaneous boost with relatively narrow planning target volume margins16 and normal tissue dose constraints . 
the cumulative rate of rtog grade 2 or worse gastrointestinal side - e ects observed by 5 years was 14% compared with 33% for the 74 gy group in the rt01 trial , 34 which used conformal radiotherapy without speci ed dose constraints . 
we previously reported complementary ndings from the chhip trial showing a greater than 50% reduction in bowel bother or distress compared with the rt01 trial using the ucla - pci instrument.20 additionally , the apparently more favourable bladder toxicity results reported in the chhip trial compared with other studies might relate to lower total delivered dose29 , 30 or amount of bladder and trigone included in the high - dose volume , 31 which would be in keeping with our observation of lower side - e ects in the 57 gy compared with 60 gy hypo fractioned groups . 
limitations are that results are primarily applicable to patients receiving short - course androgen deprivation therapy ( 97% of the men treated ) and might not be generalisable for populations who do not receive androgen deprivation therapy , and are most robust for patients with intermediate - risk disease ( 73% of the men treated ) , although there was no heterogeneity of e ect across all risk groups . 
because the hypofractionated and conventional radiotherapy were given over di erent lengths of time , the study does not address the issue of treatment duration and accelerated repopulation in prostate cancer and our estimate of the / ratio of 18 gy does not include a time factor . other complementary phase 3 studies treating patients with prostate cancer with radiotherapy alone without androgen deprivation therapy and using hypofractionated trial ( isrctn43853433 ) has radiotherapy with di erent treatment durations will clarify these issues . 
in the netherlands , the hypro study ( isrctn85133859 ) 32 randomised 820 patients with intermediate - risk or high - risk disease to high - dose conventional radiotherapy ( 78 gy in 39 fractions ) or dose - escalated hypofractionated radiotherapy of 646 gy in 19 fractions given over a period of 67 weeks with or without androgen deprivation therapy . 
in canada , the profit randomised 1204 men with intermediate - risk disease to receive either 60 gy in 20 fractions over 4 weeks or 78 gy in 39 fractions . 
 for the low - risk patient group , the rtog 0415 study recruited 1115 patients who were randomly assigned to receive 70 gy in 28 fractions over 55 weeks or 738 gy in 41 fractions over 81 weeks . 
 the hypo trial ( isrctn45905321 ) will shortly complete recruitment of 1200 men comparing 437 gy in seven fractions over 1519 days with 78 gy in 39 fractions over trial ( isrctn17627211 ) 78 weeks and compares 3625 gy in ve fractions over 12 weeks with 78 gy in 39 fractions over 78 weeks . 
 prostate , and might reduce outcome results will not be available for several years . the pace prostate cancer radiotherapy accounts for 27% of the workload of radiotherapy departments in the uk.35 radical external - beam radiotherapy was given 14 364 patients in 201415 in england and wales involving 455 638 attendances . 
before commencement of the chhip trial , 3 gy fraction schedules were rarely used , but by 201415 , after publication of initial safety results , 13 19% of patients received 3 gy hypofractionated schedules ( ball c , personal communication )  . 
the chhip trial results show that the combination of hypofractionation and high - quality radiotherapy tech niques gives excellent tumour control , a low level of side - e ects , and increased convenience for patients compared with a conventional fractionation schedule . 
high - dose modest hypo fractionation using high - quality treatment methods such as those used in this trial should become a new standard of care for external - beam radiotherapy . 
the trial results might act as a benchmark for comparison with other treatment approaches , including radical prostatec tomy , brach ytherapy , and external beam radiation therapy without androgen deprivation therapy or using extreme hypofractionation schedules . contributors dd is the chief investigator and was involved with study design , recruiting patients , data interpretation , and manuscript writing . 
we would also like to thank the chhip trial management group members past and present and the independent data monitoring committee ( matthew sydes [ chair ] , christopher tyrell , peter barrett - lee and , previously , peter hoskin , christopher nutting ) and trial steering committee ( anthony zietman [ chair ] , soren bentzen , vivian cosgrove , heather payne ) for overseeing the trial . 
we acknowledge support of cancer research uk ( c8262 / a7253 , c1491 / a9895 , c1491 / a15955 , sp2312 / 021 ) , the department of health , the national institute for health research ( nihr ) cancer research network , and nhs funding to the nihr biomedical research centre at the royal marsden nhs foundation trust and the institute of cancer research , london . 
we acknowledge the data supplied by chris ball ( national clinical analysis and specialised applications team , clatterbridge cancer centre nhs foundation trust ) from the national radiotherapy dataset ( rtds )  . 12 thames hd , bentzen sm , turesson i , overgaard m , van den bogaert w . 
the early toxicity of escalated versus standard dose conformal radiotherapy with neo - adjuvant androgen suppression for patients with localised prostate cancer : results from the mrc rt01 trial ( isrctn47772397 )  . 
hypofractionated radiotherapy versus conventionally fractionated radiotherapy for patients with intermediate - risk localised prostate cancer : 2 - year patient - reported outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
 int j radiat oncol biol phys 2006 ; 65 : 96574 . maria lucia reale , * massimo di maio massimo.dimaio@unito.it department of oncology , university of turin , turin 10128 , italy ; division of medical oncology , ordine mauriziano hospital , turin , italy us food and drug administration . 
europa.eu / en / documents / scientific - guideline / reflection - paperregulatory - guidance - use - healthrelated - quality - life - hrql - measuresevaluation_en.pdf ( accessed feb 23 , 2020 )  . schnipper le , davidson ne , wollins ds , et al . 
a standardised , generic , validated approach to stratify the magnitude of clinical benefit that can be anticipated from anti - cancer therapies : the european society for medical oncology magnitude of clinical benefit scale ( esmo - mcbs )  . 
quality of life assessment using patient - reported outcome ( pro ) measures : still a cinderella outcome ? ann oncol 2018 ; 29 : 228687 . bergman b , aaronson nk , ahmedzai s , kaasa s , sullivan m . 
a psychometric properties of the updated eortc module for assessing quality of life in patients with lung cancer ( qlq - lc29 ) : an international , observational field study . 
for patients with cancer infected with influenza , the risk of hospital admission for respiratory distress is four times higher , and the risk of death ten times higher than patients without cancer . 
this exacerbation seems to be particularly marked in those with neutropenia or lymphopenia , a feature commonly seen in patients with cancer treated with multiple therapies.2 a comment1 from wenhua liang and colleagues , published in the lancet oncology , on the situation in china suggests that patients with cancer are at higher risk of infection with sars - cov - 2 than the general population ( 1% of patients with covid - 19 in the study had cancer , whereas the incidence of cancer in the chinese population is 029% ) , which could be related to the closer medical follow - up of these patients . 
more concerning is the increased risk of severe respiratory complications requiring time in the intensive care unit in patients with cancer , as compared with patients without cancer ( 39% vs 8% , respectively ; p = 00003 )  . 
 a covariate signifi cantly associated with this risk was a history of chemotherapy or surgery in the month preceding infection ( odds ratio 534 , 95% ci 1801618 ; p = 00026 ) , a factor that includes the majority of patients with cancer . 
finally , patients with cancer deteriorated more rapidly than those without cancer ( median time to severe events 13 days vs 43 days ; p < 00001 ; hazard ratio 356 , 95% ci 165769 )  . the following guidelines apply to adult patients with solid tumours only , and should be considered complementary to the standard rules adopted by the french health authorities for the general population . first , some prevention measures can be implemented in oncology departments . 
the basic principle is published online march 25 , 2020 s1470 - 2045 ( 20 ) 30204 - 7 for hcsp guidelines see avisrapportsdomaine ? clefr = 775 vol 21 may 2020 comment for patients with cancer and oncology or radiotherapy departments to avoidas much as possibleany contact with people with coronavirus disease 2019 ( covid - 19 )  . 
if , despite this principle , such patients were admitted to hospital in oncology or radiotherapy departments , they should be isolated from other patients with cancer and referred to departments specialised in the fight against covid - 19 as quickly as possible . infrastructure and given the susceptibility of patients with cancer to sars - cov - 2 infection , their presence at hospitals should be minimised . 
this includes telemedicine and phone calls to replace safety visits , as well as replacement of intravenous drugs with oral drugs ( eg , chemotherapy and hormone therapies ) where possible , along with logistics to allow home administration of intravenous and subcutaneous anticancer agents . 
adjustment of dosing schedules of chemotherapy or radiotherapy treatments can be considered to reduce the frequency of hospital admissions ( eg , every 3 weeks , rather than weekly administration , of the same regimens or hypofractionated radiotherapy )  . 
moreover , some patients with slowly evolving metastatic cancers could be given temporary breaks in their treatment at the discretion of the referring oncologist , with disease assessment extended to every 23 months , to avoid hospital admissions . despite these measures , some patients with cancer will have to be admitted to hospital for systemic treatment or radiotherapy . 
the caregivers are advised to organise daily phone calls to patients with cancer planned to be admitted the following day , to ensure these patients do not present any symptoms compatible with covid - 19 before being admitted to oncology or radiotherapy wards . 
to protect patients with cancer , open - space chemotherapy outpatient centres should integrate separation measures ( eg , minimum space between seats , mobile walls , wearing of masks by patients and staff )  . infection and patients with cancer who do not have covid - 19 , or who have recovered , can continue treatment , with the aforementioned adjustments to limit their presence at the hospital . 
if access to hospital cancer care is reduced because of requisition of facilities for management of patients with covid - 19 , or if the likelihood of viral life - threatening complications were deemed too high , a selection of patients to be admitted to hospital for cancer treatment , prioritised by type of care or treatment , might be required . 
the prioritisation in the management of patients will integrate the essence of curative or non - curative intent therapeutic strategy , age of patients , life expectancy , time since diagnosis ( eg , early setting recently diagnosed or first - line treatment , or late setting in patients who have been treated with multiple lines of chemotherapy ) , and symptoms . 
the following priority order is proposed ( but remains at the discretion of the patients clinician and team ) : ( 1 ) patients with cancers managed with curative intent treatments ( favouring those patients aged 60 years or life expectancy 5 years , or both ) ; ( 2 ) patients with cancers managed with non - curative intent treatments , and aged 60 years or younger , or life expectancy of 5 years or more , or both , and in first - line of the therapeutic strategy ( early setting ) ; and ( 3 ) other patients with cancers managed with non - curative intent treatments , favouring those whose cancerous lesions extend or whose symptoms might jeopardise their lives quickly in the case of treatment discontinuation . 
patients with cancer who need to be hospitalised for supportive care ( eg , pain management , bacterial infection , or palliative care before death ) could be referred to non - specialised cancer departments , or home care . in summary , patients with cancer are at high risk of severe and urgent clinical complications and patients with cancer with covid - 19 should discontinue their systemic anticancer treatments until complete resolution of symptoms ( at clinician discretion )  . 
in a situation where available care departments involved remain 620 vol 21 may 2020 comment facilities are scarce , prioritisation should involve the patients managed with curative - intent therapeutic strategies , and those with a life expectancy of 5 years or more , acknowledging that final decisions lie with the referring clinicians . 
patients with cancer should be closely monitored owing to their susceptibility to sars - cov - 2 infection . ar reports grants , personal fees , and non - financial support from pfizer , merck , personal fees and non - financial support from merck , sharpe & dohme , astrazeneca , roche , ipsen , and novartis . 
cochrane database syst rev 2018 ; 2 : cd008983 . preparedness for covid - 19 in the oncology community in africa the world is experiencing an unprecedented health crisis with the coronavirus disease 2019 ( covid - 19 ) pandemic threatening human existence and livelihood . 
patients with cancer are thought to be more susceptible and have higher morbidity and mortality rates from covid - 19 than the general population.1 africa , with a heterogeneity of economies , cultures , and disease patterns , is thank fully the last continent to be hit by the pandemic . 
we acknowledge the points made by our colleagues from morocco.2 with many lessons learnt from other countries and the experiences within africa from the ebola and cholera epidemics , africa should be prepared for covid - 19 . 
unfortunately , poverty , low health literacy rates , and cultural practices that negatively affect cancer outcomes will result in poor assimilation of covid - 19 containment strategies in africa . the continent , despite many competing health challenges , is now finally implementing cancer prevention strategies , improving treatment access , and expanding the cancer workforce . 
weas oncologists in africafollow covid - 19 cancer care guidelines from other highincome countries.3 , 4 we realise the urgency to delay the start of adjuvant therapies and regular surveillance , reconsider switching to oral systemic therapies ( many of which are inaccessible to our patients ) , and rethink the effectiveness of further lines of palliative chemotherapy . 
we must weigh the consequences of exposing our susceptible patients and small cancer ignoring oncology workforce to covid - 19 while principles that we previously did not dare to disregard.5 we need to make critical decisions because many patients with cancer present with locally advanced disease in africa , and delaying treatment will result in progression and deterioration of their cancer as well as higher out - of - pocket expenditure for treatments , leading to further psychological distress . what do we do when a patient with cancer on chemotherapy develops a fever ? would we ignore the possibility of neutropenic fever , malaria , or typhoid ? should we call the overstretched and under - resourced covid - 19 team ? the paucity of protective gear and onsite testing kits for patients and health - care staff on the continent is a major flaw in delivering life - saving oncology care during this crisis . 
the availability of logistics ( which are greatly inadequate ) , institutional published online april 3 , 2020 s1470 - 2045 ( 20 ) 30220 - 5 vol 21 may 2020 comment corrections correction to lancet oncol 2016 ; 17 : 142634 stintzing s , modest dp , rossius l , et al . 
 folfiri plus cetuximab versus folfiri plus bevacizumab for metastatic colorectal cancer ( fire - 3 ) : a post - hoc analysis of tumour dynamics in the final ras wild - type subgroup of this randomised open - label phase 3 trial . 
 lancet oncol 2016 ; 17 : 142634in the appendix , page 9 , supplementary table 3 , the values for orr central independent review board should have read 113 / 157 ( 720% ) and for the difference 3 / 157 ( 19% ) in the folfiri plus cetuximab group . 
this correction has been made to the online version as of oct 31 , 2016 . vol 17 november 2016 e479 corrections correction to lancet oncol 2015 ; 16 : 522 correction to lancet oncol 2016 ; 17 : 553 correction to lancet oncol 2016 ; 17 : 733 philip , pa . 
 this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . eggermont amm , chiarion - sileni v , grob j - j , et al . 
this correction has been made to the online version as of june 1 , 2016 . correction to lancet oncol 2016 ; 17 : 751 carrie c , hasbini a , de laroche g , et al . 
salvage radiotherapy with or without short - term hormone therapy for rising prostate - specific antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
this correction has been made to the online version as of june 1 , 2016 , and the printed version is correct . vol 17 june 2016 e223 lancet oncol 2019 ; 20 : 121125 published online july 29 , 2019 s1470 - 2045 ( 19 ) 30339 - 0 this online publication has been corrected . 
the corrected version first appeared at thelancet.com / oncology on august 6 , 2019 . see comment page 1184 * collaborators listed at the end of the article and in the appendix correspondence to : dr lisa m force , department of oncology , st . 
jude childrens research hospital , memphis , tn 38105 , usa lisa.force@stjude.org see online for appendix the global burden of childhood and adolescent cancer in 2017 : an analysis of the global burden of disease study 2017 gbd 2017 childhood cancer collaborators * summary background accurate childhood cancer burden data are crucial for resource planning and health policy prioritisation . 
 although global incidence and mortality estimates are available , there are no previous analyses of the global burden of childhood cancer represented in disability - adjusted life - years ( dalys )  . methods using the global burden of diseases , injuries , and risk factors study ( gbd ) 2017 methodology , childhood ( ages 019 years ) cancer mortality was estimated by use of vital registration system data , verbal autopsy data , and population - based cancer registry incidence data , which were transformed to mortality estimates through modelled mortality - to - incidence ratios ( mirs )  . 
final point estimates are reported with 95% uncertainty intervals . findings globally , in 2017 , there were 115 million ( 95% uncertainty interval 106123 ) dalys due to childhood cancer , 973% ( 973973 ) of which were attributable to ylls and 27% ( 2727 ) of which were attributable to ylds . 
822% ( 821822 ) of global childhood cancer dalys occurred in low , low - middle , or middle socio - demographic index locations , whereas 503% ( 503503 ) of adult cancer dalys occurred in these same locations . 
cancers that are uncategorised in the current gbd framework comprised 265% ( 265265 ) of global childhood cancer dalys . interpretation the gbd 2017 results call attention to the substantial burden of childhood cancer globally , which disproportionately affects populations in resource - limited settings . 
the use of daly - based estimates is crucial in demonstrating that childhood cancer burden represents an important global cancer and child health concern . funding bill & melinda gates foundation , american lebanese syrian associated charities ( alsac ) , and st . 
 information on the burden of childhood cancer is crucial to informing these efforts and thus , model - based estimates are necessary to determine cancer burden in settings without data until cancer data coverage improves . the global burden of diseases , injuries , and risk factors study ( gbd ) 2017 provides estimates for 359 diseases and injuries , including cancers , and is therefore uniquely positioned to fill the gap in health planning data as countries work to expand their cancer surveillance systems.10 additionally , standard gbd outcomes include estimates of disability - adjusted lifeyears ( dalys ) , a useful composite metric that accounts for both the mortality and morbidity of a disease.11 dalys allow for cross - disease and cross - geography comparisons that contextualise disease burden . 
so far , however , no vol 20 september 2019 1211 articles research in context evidence before this study previous work to describe childhood cancer burden globally has focused on conventional metrics of cancer burden , such as incidence , mortality , and survival , either in a subset of countries ( eg , the third volume of the international incidence of childhood cancer and concord - 3 ) or globally ( eg , globocan 2018 )  . 
 we searched pubmed for english - language research articles describing the global burden of childhood cancer published between jan 1 , 2010 , and sept 30 , 2018 , using the terms pediatric or childhood or child and cancer or neoplasm or tumor or malignancy or oncology and global or international or worldwide or world and burden or metrics or incidence or mortality or prevalence or survival but did not find additional applicable work . 
while providing valuable information , no previous publications incorporated morbidity or provided disability - adjusted life - years ( dalys ) , a metric that allows policy makers to directly compare the lifelong implications of childhood cancer burden against other diseases for priority setting . added value of this study to our knowledge , we report for the first time the global and regional estimates of childhood cancer burden using global burden of diseases , injuries , and risk factors study ( gbd ) 2017 results , with dalys as the outcome measure , providing a new perspective on the global burden childhood cancer to that previously available in published literature . 
this burden is disproportionately high in low , low - middle , and middle socio - demographic index ( sdi ) settings , which together contribute 822% of global childhood cancer dalys . 
childhood cancers are a major cause of global disease burden , even when compared with other diseases of childhood or with adult cancers . implications of all the available evidence by presenting the global burden of childhood cancer in dalys , we identified that childhood cancer results in a substantial disease burden despite a relatively low absolute number of incident cases and deaths . 
this burden is particularly notable in resource - limited settings , where the ability to directly compare the burden of various diseases through dalys is particularly relevant for policy makers , who must consider a myriad of health priorities in addition to childhood cancers and can use these data to make evidence - based resource allocation and cancer - control planning decisions . 
as countries implement , monitor , and evaluate capacity - building programmes as part of the who global initiative for childhood cancer , refining the methodology of childhood cancer burden estimation in future gbd iterations will be crucial to identify high - impact interventions and provide the most useful information for cancer control efforts by governments , stakeholders , and the global health community . dedicated gbd analysis of childhood cancer burden has been done . 
previous research describing childhood cancer burden internationally has focused on traditional metrics of cancer burden , including incidence , mortality , and survival.6 , 7 , 12 we aimed to report the global burden of childhood cancer in 2017 using daly estimates from gbd 2017 , an approach that adds a new perspective to the assessment of childhood cancer burden than has been presented in previous analyses . methods overview the gbd study was created to establish comprehensive and comparable global health metrics . 
estimates of incidence , prevalence , mortality , years of life lost ( ylls ) , years lived with disability ( ylds ) , and dalys are generated for each disease and injury , with each metric reported by year , location , age group , and sex.13 each successive gbd iteration supersedes the results of previous gbd rounds for the entire newly estimated time series . 
gbd 2017 is compliant with the guidelines for accurate and transparent health estimates reporting ( appendix p 4 ) .14 data sources used in gbd 2017 are available online . estimation of cancer burden the gbd cancer estimation process focuses first on the estimation of cancer mortality ( see appendix pp 78 for ( mirs ) were used flow diagrams of the gbd 2017 cancer estimation process )  . 
cancer mortality data sources include vital registration systems , cancer registration systems , and verbal autopsy data ( a map of the site - years of childhood cancer data available in gbd 2017 is available on appendix p 10 )  . 
mirs for all age , sex , location , and year combinations were modelled using a spatiotemporal gaussian process regression with incidence data from cancer registries and mortality data from cancer registries or high - quality vital registration systems . 
 sdi categories do not sum to precisely the global total because gbd does not provide separate estimates for all locations globally and an adjustment factor is made between all estimated locations , which each have a corresponding estimated sdi value for 2017 , and the global aggregate . 
cancers without a detailed gbd cause . table : childhood cancer burden , 2017 mortality data even if data quality varies , tests individual as well as ensemble models , and is capable of selecting the optimal model or set of models on the basis of the out - of - sample predictive validity . 
cause - specific mortality estimates were subsequently scaled to independently modelled all - cause mortality.17 , 18 the mortality estimates for each cancer type were divided by the corresponding mir to obtain incidence estimates . 
 two sequelae were estimated for cohorts that survive 10 years after diagnosis : ( 1 ) diagnosis or treatment and ( 2 ) remission , after which disability risk is returned to that of the general population . 
four sequelae were estimated for cohorts that do not survive 10 years after diagnosis : ( 1 ) diagnosis or treatment , ( 2 ) remission , ( 3 ) metastatic or disseminated , and ( 4 ) terminal phases . 
 to generate yld estimates , each sequela prevalence was multiplied by a sequelae - specific disability weight , representing the magnitude of health loss associated with a specific health outcome , measured on a scale from 0 ( full health ) to 1 ( equivalent to death ; appendix p 39 ) .19 ylls were estimated by multiplying the difference between a standard life expectancy at the age of death and the estimated number of deaths at that age.17 the yld and yll estimates were summed to provide vol 20 september 2019 1213 articles for the gbd compare tool see gbd - compare / for the gbd results tool see results - tool daly estimates.13 more detailed descriptions of the methods for disease burden estimation can be found in the appendix for this paper and in the gbd 2017 capstone publications.13 , 1719 definitions the childhood age group in this analysis encompasses children and adolescents , defined as ages 019 years . 
the 014 - year age range is used to define paediatrics in some countries and global health organisations , and data for subsets of this age range are available online using the gbd compare tool and the gbd results tool . 
all cancers as defined in the 10th revision of the international classification of diseases , chapter ii ( neoplasms ) , are the gbd cancer estimation process included ( appendix p 10 )  . 
in this analysis , we restructured the cancer diagnostic categories to depict the most relevant childhood cancer information , categorising any cancer with less than 1000 global deaths annually as other rare cancers , and any cancer without a specific gbd cause as uncategorised cancers . 
all rates in this paper are reported per 100 000 person - years , with the gbd 2017 world standard population used for calculation of age - standardised rates.17 see the appendix for definitions of gbd world superregions ( p 54 ) and gbd world regions ( p 60 )  . gbd 2017 produced estimates at global , regional , national , and select subnational levels ; 13 this analysis focuses on the global and regional estimates . 
results are presented by socio - demographic index ( sdi ) quintile in a subset of tables and figures given the usefulness of sdi as a summary measure of where countries are on the development spectrum ( appendix p 47 )  . 
sdi is a composite measure of income per capita , total fertility rate under 25 years of age , and average educational attainment , and has been shown to correlate well with health outcomes.19 uncertainty analysis final point estimates are reported with 95% uncertainty intervals ( uis )  . 
the uis were calculated as the 25th and 975th percentile of the distribution of 1000 draws at each step in the cancer estimation process , with the uncertainty propagated through each step ( ui estimation is described in further detail in the appendix p 39 )  . role of the funding source the funders of this research had no role in the design of the gbd cancer estimation process , collection or analysis of data , interpretation of results , or in the writing of this manuscript . 
the corresponding author had full access to all data used in this study and had final responsibility for the decision to submit for publication . results childhood cancer resulted in 115 million ( 95% ui 106123 ) dalys globally in 2017 , of which 973% ( 973973 ) came from ylls and 27% ( 2727 ) came from ylds ( table )  . 
a substantial portion of the global burden of childhood cancer exists in low , low - middle , and middle sdi countries ( 822% [ 821822 ] of the global childhood cancer total dalys ; table ) , countries that are concentrated in asia , africa , and central and south america ( figure 1a )  . 
this geographical pattern of cancer burden distribution is noticeably different from that observed in adults ( figure 1b ) , with only 503% ( 503503 ) of the global adult cancer absolute daly burden affecting low , low - middle , and middle sdi countries ( appendix p 66 )  . of the childhood cancer age groups , the 04 - year age group had the greatest contribution to global childhood cancer dalys ( 43 million [ 95% ui 3847 ] , or 370% [ 369370 ] of the global 019 year childhood cancer absolute daly burden ; figure 2 )  . 
across all childhood cancer age groups , a consistently higher proportion of total dalys was made up by ylls ( 968% [ 968968 ] to 981% [ 981981 ] of the total age group - specific dalys ) than by ylds ( 19% [ 1919 ] to 32% [ 3232 ] of the total age group - specific dalys ; appendix p 68 )  . 
 leukaemias constituted the highest proportion of categorised childhood cancer daly burden globally , followed by brain and nervous system cancers , with 341% ( 340341 ) of all childhood cancer dalys globally attributable to leukaemias and 181% ( 181181 ) attributable to brain and nervous system cancers . 
in adolescents , other rare cancers , which include cancers such as those of the testes , ovaries , and thyroid , contributed the second highest proportional daly burden categorised ( 195% [ 194195 ] )  . 
there was a substantial proportion of uncategorised cancers , those neoplasms without a specific cancer type noted in the current gbd data structure , throughout the childhood and adolescent age range , representing 265% figure 1 : global map of age - standardised daly rates for ( a ) childhood cancers ( ages 019 years ) and ( b ) adult cancers ( 20 years or older ) , both sexes combined , 2017 quintiles are based on dalys per 100 000 person - years . 
for childhood cancers , quintile 1 indicates less than 222 , quintile 2 indicates 222 to less than 263 , quintile 3 indicates 263 to less than 346 , quintile 4 indicates 346 to less than 441 , and quintile 5 indicates 441 or more . 
for adult cancers , quintile 1 indicates less than 3314 , quintile 2 indicates 3314 to less than 3915 , quintile 3 indicates 3915 to less than 4407 , quintile 4 indicates 4407 to less than 4964 , and quintile 5 indicates 4964 or more . 
 vct = saint vincent and the grenadines . 1214 vol 20 september 2019 articles a caribbean age - standardised daly rate quintiles for childhood cancers quintile 1 ( 020% ) quintile 2 ( 2140% ) quintile 3 ( 4160% ) quintile 4 ( 6180% ) quintile 5 ( 81100% ) age - standardised daly rate quintiles for adult cancers quintile 1 ( 020% ) quintile 2 ( 2140% ) quintile 3 ( 4160% ) quintile 4 ( 6180% ) quintile 5 ( 81100% ) barbados comoros west africa eastern mediterranean dominica grenada maldives mauritius malta marshall isl kiribati solomon isl vanuatu samoa seychelles persian gulf singapore balkan peninsula fiji tonga barbados comoros west africa eastern mediterranean dominica grenada maldives mauritius malta marshall isl kiribati solomon isl vanuatu samoa caribbean seychelles persian gulf singapore balkan peninsula fiji tonga vol 20 september 2019 1215 articles a 12 000 000 4 500 000 9 000 000 3 375 000 6 000 000 2 250 000 3 000 000 1 125 000 childhood cancer type uncategorised cancers * other rare cancers renal cancers liver cancers brain and nervous system cancers hodgkin lymphoma non - hodgkin lymphoma leukaemias not otherwise specied acute myeloid leukaemia acute lymphoblastic leukaemia 019 age group ( years ) 59 1014 1519 59 1014 1519 age group ( years ) age group ( years ) figure 2 : global daly burden of childhood cancer types , both sexes combined , 2017 , in absolute and proportional burden in the 019 years age group ( a ) , and absolute and proportional burden by 5 - year childhood age group ( b , c ) daly = disability - adjusted life - year . 
the proportion of uncategorised cancers was highest in the 04 - year age group ( 340% [ 339340 ] ) , some of which might be attributable to cancers such as retinoblastoma and neuroblastoma , which are not currently separately estimated . when assessed by gbd world region ( figure 3 ) , there was substantial variability in the absolute and proportional daly burden of childhood cancers by cancer type . 
estimates of the proportion of childhood cancer dalys comprised by leukaemias and brain and nervous system cancers , the most common childhood cancer types in many high - resource settings , both varied by up to 27 times between world regions . 
the greatest proportional burden of leukaemias was in andean latin america ( 494% [ 95% ui 491497 ] of all childhood cancers ) and central latin america ( 487% [ 486489 ] of all childhood cancers ) , whereas the greatest absolute burden rested in south asia ( 954 000 [ 805 0001 119 000 ] dalys ) and east asia ( 695 000 [ 580 000763 000 ] dalys )  . 
 non - hodgkin lymphomas , which include subtypes such as burkitts lymphomas that are not separately estimated in the gbd study , varied by approximately three times between world regions , with the greatest proportional childhood cancer daly burden in eastern sub - saharan africa ( 165% [ 165166 ] of all childhood cancers ) and western sub - saharan africa ( 161% [ 160161 ] of all childhood cancers )  . 
the pro portion of childhood cancers that were uncategorised was prominent in all world regions , but disproportionately high in regions within sub - saharan africa ( eg , 420% [ 419421 ] in western sub - saharan africa )  . rankings of the relative burden of childhood cancers are shown in figure 4 , expressed in absolute dalys by sdi quintile , gbd super - region , and the 50 most populous countries for children in 2017 . 
the intercategory rankings show that the low - middle sdi quintile had the greatest daly burden for the majority of childhood cancer types , and the low sdi quintile had the most childhood cancer types that ranked second in daly burden . 
although four of the five countries with the highest childhood cancer dalys were in the gbd superregions ( 1 ) south asia and ( 2 ) southeast asia , east asia , and oceania , sub - saharan africa had the greatest daly burden for more childhood cancer types than any other super - region . 
the intra - category rankings highlight that for most countries , gbd super - regions , and sdi settings , uncategorised cancers had the highest estimated daly burden of all the childhood cancer types . focusing on the representation of childhood cancer burden in terms of dalys is not meant to devalue the importance of more standard cancer burden metrics . 
the incidence and mortality values and ageabsolute standardised rates for childhood cancers globally in 2017 are presented in the table , and the relationship between country - level age - standardised childhood cancer incidence or mortality rates and sdi are shown in figure 5 . 
with increasing sdi , age - standardised childhood cancer incidence rates generally increased , and age - standardised childhood cancer mortality rates decreased ( figure 5 )  . although the absolute incidence and mortality attributed to childhood cancers numbered in the hundreds of thousands globally , the burden as represented by ylls and dalys was substantially greater , in the millions globally ( table )  . 
compared with cancers of adulthood ( figure 6a ) , childhood cancers collectively ranked first in terms of daly contribution in low and low - middle sdi countries , higher than the daly burden attributable to any single adult cancer type . 
globally , childhood cancer 1216 vol 20 september 2019 articles south asia sub - saharan africa high income southeast asia , east asia , and oceania gbd super - regions latin america and caribbean north africa , and middle east central europe , eastern europe , and central asia childhood cancer type uncategorised cancers * other rare cancers renal cancers liver cancers brain and nervous system cancers hodgkin lymphoma non - hodgkin lymphoma leukaemias not otherwise specied acute myeloid leukaemia acute lymphoblastic leukaemia 3 000 000 2 500 000 2 000 000 1 500 000 1 000 000 500 000 south asia oceania central sub - saharan africa w estern sub - saharan africa tropical latin a m erica central latin a m erica eastern sub - saharan africa n orth africa and middle east southern sub - saharan africa southeast asia east asia andean latin a m erica w estern europe highinco m e n orth a m erica southern latin a m erica caribbean highinco m e asia pacic australasia eastern europe central asia central europe gbd regions figure 3 : the absolute ( a ) and proportional ( b ) dalys due to childhood ( 019 years ) cancer types by gbd world region , both sexes combined , 2017 see the appendix for definitions of gbd world super - regions ( p 54 ) and regions ( p 60 )  . 
included leukaemias not otherwise specified , chronic lymphocytic leukaemias , and chronic myeloid leukaemias . ranked sixth in terms of daly burden , with a daly burden lower only than the burden attributable to cancers of the lung , liver , stomach , colon , and breast . 
this ranking pattern was different when childhood cancers were compared with other diseases of childhood ( figure 6b ) , in which the highest childhood cancer daly burden ranking was in high - middle and middle sdi settingscountries that generally have transitioning development statusrather than the lowest sdi settings . 
 compared with other diseases of childhood , childhood cancer ranked ninth globally in terms of daly burden , lower than the global burden of lower respiratory infections , diarrhoeal diseases , malaria , and hiv or aids , but higher than the global burden of measles , typhoid , and tuberculosis . discussion to our knowledge , this paper is the first analysis to quantify the global burden of childhood cancer using dalys . 
the high - income gbd super - region includes the gbd regions of australasia , high - income asia pacific , high - income north america , western europe , and southern latin america . 
previous approaches to reporting the global burden of childhood cancers have focused on incidence , mortality , and survival ; each of these metrics , although essential , provide a limited assessment when reviewed individually.6 , 7 , 12 dalys can provide a useful summary measure of early mortality and treatment - related morbidity , especially for the childhood cancer population , in which early deaths contribute many ylls to dalys and in which children surviving cancer treatment often live for many years with chronic disability . 
in our analysis of gbd 2017 , we report that although the absolute numbers of global childhood cancer incident cases and deaths were relatively small , the global burden of childhood cancer as represented in dalys was substantial . 
the majority of these childhood cancer dalys affected countries with a lower sdi , probably due to both the younger population structure observed in lower - income settings as well as a disproportionately large yll burden , reflective of the lower survival rates observed in countries with frail health systems . as expected , lower sdi settings were noted to have the highest age - standardised overall childhood cancer the association between mortality rates . 
however , childhood cancer incidence rates and sdi represented in figure 5a is unexpected , given that there are few established environmental risk factors for the majority of childhood cancers and current evidence suggests that pathological germline cancer predisposition mutations affect less than 10% of the childhood cancer population.8 , 20 the cause of the trend between incidence and sdi is unknown but probably multifactorial . 
although there is heterogeneity in environmental exposures between world regions and much to learn regarding potential genetic variability between populations , these factors alone are unlikely to explain the estimated variation in childhood cancer incidence by sdi . 
limitations in access to health care and diagnostic capacity for children with cancer have been suggested to contribute to artificially low case ascertainment in resource - limited settings.21 missed diagnoses caused by poor access to health facilities , misdiagnoses as non - oncological diseases , and underregistration due to overburdened cancer registration systems all probably contribute to this phenomenon . 
the gbd 2017 results highlight that improving the accuracy of global childhood cancer burden assessment will require not only expanding the quantity and quality of populationbased cancer registration systems , but also increasing access to health care with the capacity to identify children with cancer regardless of where they live . treatment of childhood cancer in lmic settings has been shown to be very cost - effective according to who choosing interventions that are cost - effective criteria , but because of finite resources and competing health priorities in many lmic settings , an accurate appraisal of childhood cancer disease burden using comparable metrics is essential for health policy decision making.22 , 23 025 050 075 100 025 075 100 050 gbd regions east asia southeast asia oceania central asia central europe eastern europe high - income asia pacic australasia western europe southern latin america high - income north america caribbean andean latin america central latin america tropical latin america north africa and middle east south asia central sub - saharan africa eastern sub - saharan africa southern sub - saharan africa western sub - saharan africa figure 5 : the association between sdi and childhood cancer age - standardised incidence rate ( a ) and mortality rate ( b ) , 2017 both panels represent estimates for both sexes combined . 
each colour represents one of the seven gbd super - regions ( red represents southeast asia , east asia , and oceania ; blue represents central europe , eastern europe , and central asia ; green represents high - income ; purple represents latin america and the caribbean ; orange represents north africa and the middle east ; yellow represents south asia ; and grey represents sub - saharan africa )  . 
sdi = socio - demographic index . as low sdi countries develop , the burden of infectious diseases tends to decline and thus the relative burden of non - communicable diseases , including cancers , tends to risea phenomenon known as epidemiological transition . 
the use of dalys provides a unique ability to contextualise the burden of childhood cancers comparison with general diseases of childhood , and we found that childhood cancer ranks among the top five causes of daly burden in middle and high - middle sdi settings , with a lower ranking on either end of the sdi spectrum , particularly in low sdi settings . 
this is a markedly different concentration of burden than occurs in adult cancers , in which daly burden is heavily weighted towards countries 1220 vol 20 september 2019 articles with high and middle sdi status , and is probably due in part to the older population structure in higher sdi settings , as well as to lifestyle risk factors that are more prevalent in higher - resourced settings.24 this variation in the epidemiological patterns of cancer burden distribution in children and adults supports the view that the mechanisms of addressing cancer burden in adults , which focus on risk - reduction strategies and screening interventions , are not as relevant in the paediatric and adolescent age groups at this time . 
childhood cancers generally progress rapidly , are not amenable to screening , and are fatal without swift diagnosis and treatment.8 thus , improving childhood cancer outcomes will require well functioning health systems capable of early diagnosis and effective treatment . requested addressing the global burden of childhood cancer has gained greater relevance during the past 2 years since the world health assembly cancer resolution in may , 2017 , and the who global initiative for childhood cancer announced during the high level meeting on non - communicable diseases at the un general assembly in september , 2018.25 , 26 the world health assembly cancer resolution resourcestratified guidance for the development of cancer - control programmes , specifically calling for children and adolescents to be included in the design of these programmes . 
the who global initiative for childhood cancer is the first programme designed to address this resolution with a focus on childhood cancer and aims to increase the overall survival for six key childhood cancers ( acute lymphoblastic leukaemia , burkitts lymphoma , hodgkin lymphoma , low - grade glioma , retinoblastoma , and wilms tumour ) to 60% globally by 2030 through integration of childhood cancer into national cancer control policies and capacity - building interventions including the development of national centres of excellence and regional satellites.5 as initiatives such as these recommend countries develop and implement paediatric - specific cancer control plans over the next decade , country - specific and region - specific variations in disease burden and identification of high - yield opportunities for improvement in outcomes will be essential . 
the gbd study provides valuable estimates of childhood cancer epidemiology in areas where direct disease burden data are scarce or non - existent , provides the most comprehensive and contextualised global burden estimates to date through the use of dalys , and is updated annually . 
moreover , the gbd framework is already monitoring progress of the health - related un sustainable development goals.27 , 28 as the who global initiative for childhood cancer will develop indicators similar in structure to those used for tracking of sustainable development goal targets , the gbd study provides an ideal platform for monitoring global progress in childhood cancer by quantifying changes in burden and tracking proposed indicators over time . the deeper analyses of the gbd cancer estimation process described here highlight opportunities improve the currently applied methodology with regard to childhood cancers in particular . 
inclusion of data from paediatric - specific cancer registries would add key existing information for childhood cancer incidence not currently included in the gbd data sources.7 however , additional data sources alone will not resolve key structural limitations in the existing gbd approach . 
the present anatomical site - based system of reporting cancer types functions well for adult cancers , which are primarily carcinomas , but leaves 265% of childhood cancer dalys globally with a label of uncategorised cancers . 
morphology is crucial to appropriate diagnosis and treatment of childhood cancers , and thus the current gbd classification system inadequately communicates the burden of childhood cancers and represents a missed opportunity for actionable burden estimates . 
using the international classification of childhood cancer system as a framework for reporting childhood cancers would decrease the notable proportion that are uncategorised and should be prioritised in future gbd iterations.29 a separate limitation in the reporting is that although gbd 2017 provided estimates for benign tumour burden in aggregate , it did not specify the portion attributable to cns tumours . 
thus , the estimates reported here do not include these tumours , which are important contributors to childhood cancer morbidity and include one of the six indicator cancers ( low - grade gliomas ) proposed by the who global initiative for childhood cancer.25 furthermore , the current gbd approach to modelling the treatment and survivorship phases of childhood cancer care might lead to a systematic underestimation of ylds and dalys . 
this consideration is important because children in lmic settings tend to present to care later in their disease course , potentially leading to different distributions of cancer stage at diagnosis than are observed in hics.3 addressing this issue was not historically possible because of a paucity of childhood cancer staging information in population - based cancer registries.30 if the recently published toronto guidelines providing concrete staging recom mendations are adopted by registries in the coming years , however , opportunities to use staging data to improve the estimation of ylds might be possible in the near future.30 second , the current gbd estimation of ylds assumes that all children receive and complete treatment . 
unfortunately , many children with cancer in lmic settings have notable risk of therapy abandon ment.31 although global data on childhood cancer abandonment are limited , creating a method to account for the proportion of children who vol 20 september 2019 1221 articles abandon therapy upfront is imperative given that untreated childhood cancer is generally fatal . 
finally , the current gbd models do not incorporate the well established increased lifelong risk of multimorbidity and early death observed in childhood cancer survivors compared with the general population.3234 the existing modelling of disability in childhood cancer survivors is limited to 10 years after cancer diagnosis , with children surviving past 10 years presumed to have the same risk of morbidity and mortality as the general population . 
 substantial data have shown this assumption to be inaccurate , and incorporation of survivorship cohort data would improve the gbd estimation of childhood cancer survivor burden.33 , 34 these limitations suggest that the gbd 2017 estimates probably underestimate the dalys associated with childhood cancer . 
opportunities to improve on the current gbd methodology are both feasible and necessary to provide the most useful information to global health stakeholders interested in reducing disparities in global childhood cancer outcomes . in summary , this analysis of the global burden of childhood cancer produced by the gbd 2017 study demonstrates substantial daly burden , even when compared with cancers in adults and general diseases of childhood . 
all other authors provided data , reviewed results , or reviewed and contributed to the paper . declaration of interests njk reports personal fees and honorarium for discussing gbd anaemia findings from vifor pharmaceuticals , llc , outside the submitted work . 
all other authors declare no competing interests . acknowledgments the work in this paper was supported by the bill & melinda gates foundation , american lebanese syrian associated charities ( alsac ) , and st baldricks foundation . 
lmf acknowledges support from the us national institutes of health ( nih ) loan repayment progra aawa received funding from department of science and technology , government of india , new delhi , through the inspire faculty prografc acknowledges support from the european union ( feder funds poci / 01 / 0145 / feder / 007728 and poci / 01 / 0145 / feder / 007265 ) and national funds ( fct / mec , fundao para a cincia e a tecnologia and ministrio da educao e cincia ) under the partnership agreements pt2020 uid / multi / 04378 / 2013 and pt2020 uid / qui / 50006 / 2013 . 
ef acknowledges support from the european union ( feder funds poci / 01 / 0145 / feder / 007728 and poci / 01 / 0145 / feder / 007265 ) and national funds ( fct / mec , fundao para a cincia e a tecnologia and ministrio da educao e cincia ) under the partnership agreements pt2020 uid / multi / 04378 / 2013 and pt2020 uid / qui / 50006 / 2013 . 
 we are very grateful for the contributions of the cancer registries and individuals who collaborated in the gbd 2017 cancer estimates . corrections correction to lancet oncol 2015 ; 16 : 733 correction to lancet oncol 2016 ; 17 : 1055 correction to lancet oncol 2016 ; 17 : 1163 , 1165 basset - seguin n , hauschild a , grob jj , et al . 
 this correction has been made to the online version as of july 26 , 2016 . published online june 24 , 2016 s1470 - 2045 ( 16 ) 30273 - x dearnaley d , syndikus i , mossop h , et al . 
 conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
 lancet oncol 2016 ; 17 : 104760 in gure 4b of this article , the curves for 57 gy grade 1 + and 60 gy grade 1 + were incorrect . 
these corrections have been made to the online version as of june 24 , 2016 , and the printed version is correct . van maaren mc , de munck l , de bock gh , et al . 
lancet oncol 2016 ; 17 : 115870in gures 2b and 3b , the label for the bottom row of number at risk should have read t2n1 , and in gure 3b , the label for the top row should have read t1n0 . 
open access article distributed under the terms of cc by . vol 17 august 2016 e321 dramatic drop in new cancer drug trials during the covid - 19 pandemic data showing a 60% decrease in new clinical trials for cancer drugs and biological therapies during the pandemic further highlights the impact that covid - 19 is having on oncology research , leading organisations have warned . a comparison of trials launched between january and may , 2020 , using information from the medidata enterprise data store found a dramatic decline compared with the previous 5 years . during the 40 - month observation period , 1440 phase 14 oncology trials were launched in 91 countries , the us researchers reported in their study in jama network open . 
of these trials , 1249 were started in the years before the pandemic , but just 191 since covid - 19 hit . further calculations based on a month - by - month analysis showed an incidence rate ratio of 040 ( 95% ci 028055 ) compared with the pre - pandemic period . study leader elizabeth lamont , senior medical director of acorn ai at medidata ( boston , ma , usa ) , said that 29% of the worlds industry - sponsored interventional trials of oncology drugs or biological agents run on the platform they used for the analysis . 
their figures , the team say , raise concerns about the development of new cancer therapies . fareed melham , senior vice president at acorn ai labs , pointed out that they have previously reported a dip in patient enrolment . 
this is just another piece of data that adds to that story , so it wasnt just ongoing trials , but it was also new trial starts where we saw decline . logistical challenges in keeping existing trials running have been reported by several organisations . 
in july , 2020 , a survey by the american society of clinical oncology ( asco ) found that clinical trials had been halted or priorities shifted . vol 22 march 2021 at the start of 2021 , asco published a road to recovery report , setting out five goals for getting clinical research back on track , including designing more pragmatic and efficient trials , reducing regulatory burden , and improving accessibility . it is not surprising to see a decline in the launch of new trials , it is consistent with other work showing a 50% decline in enrolment during the early months of the pandemic , said richard schilsky , chief medical officer for asco . anecdotally at least , it seems that recruitment to trials has started to recover as sites adapt to new ways of working , even as cases have spiked once more in many countries , including the usa and across europe , he added . this pandemic will come to an end and when it does , cancer will still be with us . 
we had to redirect our focus , it had to be done , but we have to get cancer research back on track as soon as possible . aoife regan , head of clinical research at cancer research uk ( london , uk ) explained that at the start of the pandemic in early 2020 , 95% of cancer trials were halted . 
there followed a concerted effort to get the existing portfolio back up and running , but that does leave limited capacity for bringing in new studies , she says . it is likely to be a while before new study launches are back at the rate they once were , despite a handful of sites having now started new trials , she said . 
there is also countrywide variation in what trial sites are managing to do , as well as the global problem of a backlog of recruitment for existing studies , she added . a rapid drop in fundraising revenue also means that cancer research uk is planning for a decrease in research spending from 400 million to 250 million . 
the first thing we did was a rapid review of the entire portfolio because we wanted to be published online february 4 , 2021 s1470 - 2045 ( 21 ) 00067 - x for the medidata enterprise data store see medidata.com / en / clinical - trialsolutions / unified - platform / enterprise - data - store for the study report see jama netw open 2021 ; 4 : e2036353 for more on the american society of clinical oncology survey see jco oncol pract 2020 ; 16 : 41721 for more on the american society of clinical oncology road to recovery report see j clin oncol 2021 ; 39 : 15569 for more on cuts in cancer research funding due to covid - 19 see lancet oncol 2021 ; 22 : e6 really confident that our trials were still viable and feasible , said regan . some will take longer to complete , some of them may need more money to complete , and some of them may never meet their endpoints . 
they are still funding , and there is work happening to better embed research in uk national health service networks , take a look at contracts , and generally remove the barriers that slow trials down . 
it is going to be a challenge and we may need to think about how to make that room for those new studies coming through , but there is a real will to make it happen . lamont added that there are signs of recovery and that the industry is starting to learn how to work in this new world . 
in a way that , in the end , may leave us better off in our ability to carry out efficient trials that minimise the burden on patients . emma wilkinson news yang k , sheng y , huang c , et al . 
clinical characteristics , outcomes , and risk factors for mortality in patients with cancer and covid - 19 in hubei , china : a multicentre , retrospective , cohort study . 
 j hematol oncol 2020 ; 13 : 43 . risk factors for in - hospital mortality in patients with cancer and covid - 19 the covid - 19 pandemic is getting worse globally . 
we read with interest the recent article by kunyu yang and colleagues1 in the lancet oncology , which was , to our knowledge , the first to focus on the mortality of covid - 19 in patients with cancer . 
 the authors concluded that receiving chemotherapy within 4 weeks before symptom onset and male sex were independent prognostic factors for in - hospital mortality in patients with cancer and covid - 19 . first , the data in the article showed that 40 ( 20% ) of 205 patients with cancer and covid - 19 had died . 
 however , this finding is insufficient to conclude that patients with cancer and covid - 19 had a higher casefatality rate than did the general patient population with covid - 19 . 
 additionally , in wuhan , the mortality rate of inpatients with covid - 19 was 28% , regardless of whether or not they had cancer.2 second , we reviewed the cancer history of the 205 patients listed in the article.1 based on data availability , we found that 98 ( 77% ) of 127 survivors were at early cancer stage ( stage iii ) , 121 ( 82% ) of 148 survivors underwent surgery , and 73 ( 47% ) of 156 survivors survived for more than 5 years since their cancer diagnosis , 1 indicating that a substantial proportion of these patients might be clinically cured of their cancer . 
therefore , there was a large amount of heterogeneity among the patients with cancer and it would be better to study the association between mortality related to covid - 19 and primary or metastatic thoracic malig nancies . 
 third , the main causes of death for the general patient population with covid - 19 include sepsis , respiratory failure , and acute respiratory distress syndrome.2 older age , high sequential organ failure assessment score , and d - dimer concentration greater than 1 g / ml are potential risk factors for poor prognosis.2 although there were only 40 endpoint events in this article , 1 it is not appropriate to establish the multivariable logistic regression model by use of cancer - related variables , rather than these key risk factors . 
 because of scarce evidence of the correlation between these factors and mortality in patients with cancer and covid - 19 , as well as the small sample size , the conclusion that receiving chemotherapy within 4 weeks before symptom onset is an unfavourable prognostic factor for these patients should be interpreted with caution . 
 furthermore , biological sex affects immune responses and covid - 19 outcomes in all populations , not just patients with cancer.3 because the expression of angiotensin - converting enzyme 2 ( ace2 ) is also different in various cancers , 4 an analysis of the relation between case - fatality rate and ace2 expression in patients with cancer and covid - 19 would be of interest . overall , the available evidence might not strongly prove that patients with cancer and covid - 19 have a much higher case - fatality rate than do the general patient population with covid - 19 . 
the decision of whether or not to use chemotherapy should be especially cautious for patients with cancer and covid - 19 . we declare no competing interests . kaibo guo , leitao sun , li yuan , harpreet s wasan , * shanming ruan shanmingruan@zcmu.edu.cn joint first authors the first clinical medical college of zhejiang chinese medical university , hangzhou , zhejiang , china ( kg , ly ) ; department of medical oncology , the first affiliated hospital of zhejiang chinese medical university , hangzhou 310006 , zhejiang , china ( ls , sr ) ; and department of cancer medicine , hammersmith hospital , imperial college healthcare nhs trust , london , uk ( hsw ) vol 21 september 2020 e406 correspondence covid - 19 and the us health insurance conundrum the devastating effects of the covid - 19 pandemic go far beyond public health ; with many industries on hold and unemployment increasing worldwide , the global economy is approaching the deepest recession in living memory . 
in the usa , where health insurance is largely provided by employers and more than 30 million people have filed for unemployment in the past 2 months , such a recession could cause an unprecedented surge in uninsured or underinsured people . 
indeed , an analysis published on may 4 , 2020 , has estimated that if unemployment in the usa reaches 20% , 2543 million people could lose their health insurance . 
for patients with cancer , for whom care is already expensive and long lasting , this could be a fatal blow . a recent report has estimated a delay in more than 22 million cancer screening tests and a 20% decrease in the number of interactions between patients and their oncologists in the usa during the covid - 19 pandemic . 
although this approach is understandable at this time , delayed screening and reduced treatment of early stage disease could result in the need for longer and more complex treatments for more advanced stage disease . 
coupled with the anguish and mental health effects associated with the uncertainty of treatment plans and outcomes , the demands on cancer care will inevitably increase in the future , driving individual health - care costs even higher , just at a time when patients ability to pay is hugely compromised . the options for us patients with no health insurance are scarce . 
some companies and charities are fighting to improve health insurance access , but a large increase in out - of - pocket health expenses could drive many patients into bankruptcy . 
although some might find respite in opting for medicaid or cobra ( a federal insurance after mechanism employment ends ) , not everyone is eligible for the former , and the latter can be unaffordable . that extends health although efforts to fight the covid - 19 pandemic are of paramount importance , in the usa , measures are urgently needed to avoid severe economic and social outcomes , and a tighter regulation on health - care prices , with a particular focus on private community oncology providers , is needed urgently . 
 the lancet oncology cancer detection : the quest for a single liquid biopsy for all in an editorial published in 2016 , the lancet oncology commented on the plans of the company , grail , to create a universal blood test that would allow screening of asymptomatic people for several types of cancer . 
 we raised several questions , including the sensitivity and specificity of these tests , what tumours could be detected , the ethical implications for positive cases , and how to best inform clinical practice and guide the patient . 
one clear lesson from the covid - 19 pandemic is that , even in high - income countries , mass testing can quickly exacerbate existing funding frail ties in health systems . 
the case for long - term savings made by detecting and treating cancers earlier must be made more clearly to governments and insurers alike . 4 years after grails ambition was announced , we now see encouraging scientific progress . 
however , several of our previous questions remain unanswered , and importantly , can these tests be refined to have a costbenefit suitable for use worldwide ? the lancet oncology for more on the increase of unemployment in the usa see 30 / economy / unemploymentbenefits - coronavirus / index.html for more on the potential loss of health insurance in the usa see research / 2020 / 05 / how - thecovid - 19 - recession - could - affecthealth - insurance - coverage.html for the report on the impact of covid - 19 on the us health - care system see com / insights / the - iqvia - institute / covid - 19 / shifts - in - healthcaredemand - delivery - and - careduring - the - covid - 19 - era for more on the costs of cobra see org / 2020 / 05 / 13 / cobra - healthinsurance - covid - 19 - jobs / for more on grails plan see editorial lancet oncol 2016 ; 17 : 123 for more on the ccga study see org / article / s09237534 ( 20 ) 36058 - 0 / fulltext for more on the detect - a trial see org / content / early / 2020 / 04 / 27 / science.abb9601 for more on the increasing number of patients with cancer in low - income and middleincome countries see j glob oncol 2019 ; 5 : 18 vol 21 june 2020 editorial corrections published online june 24 , 2016 s1470 - 2045 ( 16 ) 30273 - x correction to lancet oncol 2015 ; 16 : 733 correction to lancet oncol 2016 ; 17 : 1055 correction to lancet oncol 2016 ; 17 : 1163 , 1165 basset - seguin n , hauschild a , grob jj , et al . 
 conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
 lancet oncol 2016 ; 17 : 104760 in gure 4b of this article , the curves for 57 gy grade 1 + and 60 gy grade 1 + were incorrect . 
these corrections have been made to the online version as of june 24 , 2016 , and the printed version is correct . van maaren mc , de munck l , de bock gh , et al . 
lancet oncol 2016 ; 17 : 115870in gures 2b and 3b , the label for the bottom row of number at risk should have read t2n1 , and in gure 3b , the label for the top row should have read t1n0 . 
these corrections have been made to the online version as of july 26 , 2016 , and the printed version is correct . vol 17 august 2016 e321 correction to lancet oncol 2020 ; 21 : 64554 correction to lancet oncol 2020 ; 21 : 144354 correction to lancet oncol 2020 ; 21 : e51927 smith i , robertson j , kilburn l , et al . 
 long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial . 
lancet oncol 2020 ; 21 : e51927in this review , the second sentence of the first paragraph of the section entitled cancer burden now describing the number of new cancer cases worldwide in 2017 should read according to analysis from the global burden of disease study , there were 168 million new cases of cancer . 
this correction has been made to the online version as of nov 30 , 2020 . correction to lancet oncol 2020 ; 21 : 156373 powles t , plimack er , soulires d , et al . 
pembrolizumab plus axitinib versus sunitinib monotherapy as firstline treatment of advanced renal cell carcinoma ( keynote - 426 ) : extended follow - up from a randomised , openlabel , phase 3 trial . 
lancet oncol 2020 ; 21 : 156373in table 1 of this article the n ( % ) for previous nephrectomy should read 357 ( 83% ) for the pembrolizumab plus axitinib group and 358 ( 83% ) for the sunitinib group . 
these corrections have been made to the online version as of nov 30 , 2020 , and the printed version is correct . correction to lancet oncol 2020 ; 21 : e30516 fangusaro j , witt o , herniz driever p , et al . 
these corrections have been made to the online version as of nov 30 , 2020 . vol 21 december 2020 e553 corrections correction to lancet oncol 2019 ; 20 : 155665 correction to lancet oncol 2019 ; 20 : e658 correction to lancet oncol 2020 ; 21 : e31729 bertelsen ca , neuenschwander au , jansen je , et al . 
lancet oncol 2019 ; 20 : 155665in this article , two patients ( one in the control group and one in the complete mesocolic excision group ) were incorrectly classified as not having recurrences , due to an error in data extraction . 
 the incorrect data have been updated in the summary findings , the results , figures 2a and 2c , table 3 , supplementary figures 2c and 2f in the appendix , and the discussion . 
complete mesocolic excision for colon cancer : is now the time for a change in practice ? lancet oncol 2019 ; 20 : 147476in this comment , the cumulative incidence of recurrence in each group has been amended , owing to these data being corrected in the linked article by bertelsen and colleagues . 
lancet oncol 2019 ; 20 : e658 in this correspondence , the absolute in risk of recurrence reduction has been amended , owing to this being corrected in the linked article by bertelsen and colleagues . 
this correction has been made to the online version as of aug 3 , 2020 . correction to lancet oncol 2020 ; 21 : e33036 cooney tm , cohen jk , guimaraes cv , et al . 
these corrections have been made to the online version as of aug 3 , 2020 . vol 21 august 2020 e372 corrections correction to lancet oncol 2020 ; 21 : 64554 correction to lancet oncol 2020 ; 21 : 144354 correction to lancet oncol 2020 ; 21 : e51927 smith i , robertson j , kilburn l , et al . 
 long - term outcome and prognostic value of ki67 after perioperative endocrine therapy in postmenopausal women with hormone - sensitive early breast cancer ( poetic ) : an open - label , multicentre , parallel - group , randomised , phase 3 trial . 
lancet oncol 2020 ; 21 : e51927in this review , the second sentence of the first paragraph of the section entitled cancer burden now describing the number of new cancer cases worldwide in 2017 should read according to analysis from the global burden of disease study , there were 168 million new cases of cancer . 
this correction has been made to the online version as of nov 30 , 2020 . correction to lancet oncol 2020 ; 21 : 156373 powles t , plimack er , soulires d , et al . 
pembrolizumab plus axitinib versus sunitinib monotherapy as firstline treatment of advanced renal cell carcinoma ( keynote - 426 ) : extended follow - up from a randomised , openlabel , phase 3 trial . 
lancet oncol 2020 ; 21 : 156373in table 1 of this article the n ( % ) for previous nephrectomy should read 357 ( 83% ) for the pembrolizumab plus axitinib group and 358 ( 83% ) for the sunitinib group . 
these corrections have been made to the online version as of nov 30 , 2020 , and the printed version is correct . correction to lancet oncol 2020 ; 21 : e30516 fangusaro j , witt o , herniz driever p , et al . 
these corrections have been made to the online version as of nov 30 , 2020 . vol 21 december 2020 e553 corrections articles lancet oncol 2005 ; 6 : 36976 published online may 10 , 2005 70175 - 3 see reection and reaction page 352 department of radiochemotherapy ( m reni md , p passoni md , e bonetto md , e villa md ) , department of radiology ( r nicoletti md ) , department of statistics ( l galli msc ) , and department of surgery ( a zerbi md , g balzano md , l aldrighetti md , prof c staudacher md , prof v di carlo md ) , s raffaele h scientic institute , milan , italy department of oncology , s luigi curr h catania , italy ( s cordio md , r bordonaro md ) ; department of oncology , pierantoni h forl , italy ( c milandri md , a passardi md ) ; department of oncology , azienda ospedaliera and university , verona , italy ( c oliani md ) ; department of medical oncology , azienda ospedaliera - policlinico , modena , italy ( g luppi md ) correspondence to : dr michele reni , department of oncology , san raffaele h scientic institute , via olgettina 60 , 20132 milan , italy reni.michele@hsr.it gemcitabine versus cisplatin , epirubicin , uorouracil , and gemcitabine in advanced pancreatic cancer : a randomised controlled multicentre phase iii trial michele reni , stefano cordio , carlo milandri , paolo passoni , elisa bonetto , cristina oliani , gabriele luppi , roberto nicoletti , laura galli , roberto bordonaro , alessandro passardi , alessandro zerbi , gianpaolo balzano , luca aldrighetti , carlo staudacher , eugenio villa , valerio di carlo summary background patients with advanced pancreatic adenocarcinoma have a poor response , progression - free survival , and overall survival with standard treatment . 
 methods in a randomised multicentre phase iii trial , 52 patients were randomly assigned to 40 mg / m2 cisplatin and 40 mg / m2 epirubicin both given on day 1 , 600 mg / m2 gemcitabine given intravenously over 1 h on days 1 and 8 , and 200 mg / m2 uorouracil a day given by continuous infusion on days 128 of a 4 - week cycle ( pefg regimen ) , and 47 were assigned to 1000 mg / m2 gemcitabine given intravenously over 30 min once a week for 7 of 8 consecutive weeks in cycle 1 and for 3 of 4 weeks thereafter . 
more patients allocated pefg than gemcitabine alone were alive without progressive disease at 4 months ( 60% [ 95% ci 4672 ] vs 28% [ 1742 ] ; hazard ratio [ hr ] 046 [ 026079 ] )  . 
1 - year overall survival in the pefg group was 385% ( 253517 ) and in the gemcitabine group was 213% ( 96330 ; hr 068 [ 042109 ] )  . 
more patients assigned pefg showed disease response than did those assigned gemcitabine ( 385% [ 253517 ] vs 85% [ 05165 ] ; odds ratio 660 [ 2112060 ] , p = 00008 )  . 
more patients in the pefg group had grade 34 neutropenia and thrombocytopenia than in the gemcitabine group ( p ( cid : 2 ) 00001 )  . interpretation the pefg regimen could be considered for treatment of advanced pancreatic adenocarcinoma . introduction pancreatic adenocarcinoma is associated with a poor prognosis . 
more than 80% of patients present with advanced disease at diagnosis , and mortality is high because tumours inltrate the abdominal blood vessels and spread to regional lymph nodes and liver at an early stage . 
gemcitabine the standard treatment for unresectable disease , and has led to an objective response in 426% of patients and a 1 - year overall survival of 1728% in phase iii trials.111 gemcitabine was licensed for treatment of advanced pancreatic cancer on the basis of improved clinical benet and increased overall survival compared with uorouracil.1 is regarded as improve several attempts the efcacy of gemcitabine in advanced pancreatic adenocarcinoma by use of new agents or by addition of a second cytotoxic agent or other drugs to a standard dose and schedule of gemcitabine have not shown a survival advantage.211 however , a signicant benet in median progressionfree survival has been noted for gemcitabine combined with uorouracil , 2 cisplatin , 7 or oxaliplatin , 11 which suggests that platinum - based agents and antifolates have a role in treatment of pancreatic cancer . 
moreover , although combination treatment did not increase overall survival compared with gemcitabine alone , whether salvage therapy affects the relation between progressionfree survival and overall survival is not known . 
strategies that have not included gemcitabine have been assessed , but have not shown better results.12 , 13 findings from a phase ii trial14 suggested that xed - dose gemcitabine improves survival , but phase iii data are not available . gemcitabine combined with erlotinib improved 1 - year overall survival compared with gemcitabine alone from 17% to 24%.15 cisplatin , epirubicin , uorouracil , and gemcitabine ( pefg ) an empirically derived treatment based on four agents that are active against pancreatic adenocarcinomashowed promising activity with regard to response rate and survival in a previous phase ii trial.16 we therefore did a multicentre randomised phase iii trial to compare standard treatment of gemcitabine with that of pefg by use of previously dened doses and schedules.16 methods patients between april , 2000 , and march , 2003 , 104 patients from ve institutions aged 1870 years with histovol 6 june 2005 articles 104 patients randomised 54 allocated pefg 50 allocated gemcitabine 2 ineligible ( inadequate liver function ) 3 ineligible 2 inadequate liver function 1 other cancer 52 analysed 47 analysed figure 1 : trial prole intensity score of 20 mm or more of a possible 100 mm on the memorial pain assessment card , 18 or a karnofsky performance status of 5070 . 
the study was done in accordance with the declaration of helsinki and approved by the local ethics committees of participating institutions ; written informed consent was obtained from all patients . 
 study objectives we chose 4 - month progression - free survival as the primary endpoint to avoid the potential effect of salvage treatment after progression on overall survival and the potential effect of surgery or radiotherapy ( allowed after 4 months in patients with stage iva disease ) on both overall survival and progression - free survival . 
secondary endpoints were overall survival , objective response , clinical benet , safety , and quality of life . randomisation patients who fullled all inclusion criteria were registered by the attending physician at the coordinating institution . 
patients were stratied by centre and stage ; the trial was unblinded . analysis was by intention to treat . treatment plan 54 patients were allocated to pefg regimens that were repeated every 28 days16 and that consisted of 40 mg / m2 cisplatin ( cisplatino - teva , pharmachemie bv , haarlem , netherlands ) and 40 mg / m2 epirubicin ( farmarubicina , pharmacia & upjohn spa , milan , italy ) given intravenously on day one , 600 mg / m2 gemcitabine ( gemzar , eli lilly , fegersheim , france ) given in 1 h on days 1 and 8 , and 200 mg / m2 uorouracil ( fluorouracile - teva , pharmachemie bv , haarlem , netherlands ) a day as protracted infusion for the duration of chemotherapy by use of an indwelling , catheter . guidelines for dose reduction and treatment delay have been reported previously.16 50 patients were allocated to 1000 mg / m2 gemcitabine a week given intravenously over 30 min for 7 consecutive weeks followed by 1 week of rest , and then subsequently for 3 of every 4 weeks . 
treatment was delayed if absolute neutrophil count was less than 1000 ( cid : 4 ) 106 cells / l , platelet count was less than 50 ( cid : 4 ) 109 / l , or if the patient developed grade 34 non - haematological toxic effects . patients were removed from the study if recovery was not evident within 2 weeks . 
patients who had ampullary tumours , other histological variants of pancreatic carcinoma , previous adjuvant chemotherapy , or previous malignant disease were ineligible for the study , with the exception of those who had had basalcell carcinoma of the skin , carcinoma in situ of the cervix , or other cancers for which the patient had been disease - free for at least 5 years . 
 eligibility criteria for assessment of clinical benet were baseline use of analgesics of at least two nonsteroidal anti - inammatory drugs , baseline pain pefg ( n = 52 ) gemcitabine ( n = 47 ) 62 ( 3769 ) 59 ( 2569 ) age ( years ) median ( range ) male female karnofsky performance status ( cid : 7 ) 70 ( cid : 5 ) 70 stage metastatic previous treatment pancreatic surgery radiotherapy or chemotherapy site of metastases liver lymph nodes lung table 1 : baseline characteristics vol 6 june 2005 articles pefg ( n = 52 ) gemcitabine ( n = 47 ) hazard ratio ( 95% ci ) progression - free survival ( months ) 4 - month ( 95% ci ) median ( iqr ) overall survival 1 - year ( 95% ci ) 2 - year ( 95% ci ) 60% ( 4672 ) 54 ( 2096 ) 28% ( 1742 ) 33 ( 2253 ) 046 ( 026079 ) 051 ( 033078 ) 0001 00033 385% ( 253517 ) 115% ( 28202 ) 213% ( 96330 ) 21% ( 0062 ) 068 ( 042109 ) 063 ( 042096 ) 01119 0033 table 3 : progression - free survival and overall survival time the dose of gemcitabine was lowered by 25% . both groups were allocated treatment for a maximum of 6 monthsie , six cycles of pefg and ve of gemcitabine . 
treatment was continued up to this time unless unacceptable side - effects developed , disease progressed , the patient refused treatment , or a medical decision was made to stop treatment . 
in patients with stage iva disease treatment was classied as complete after 4 months if no clinical benet was seen , the reduction in tumour size was less than 25% , or if ca19.9 concentration decreased to less than 50% of baseline . 
at the end of treatment , patients with operable stage iva disease were recommended for surgery and were allowed to receive radiotherapy . assessment of disease , including spiral ct of the abdomen and chest , was done at baseline , every 8 weeks during chemotherapy , and then every 3 months . 
for assessment of clinical benet , patients were asked to record pain intensity every day by completion of a memorial pain assessment card and a diary on the use of analgesics . 
performance status and bodyweight were assessed once a week . to dene outcome measures toxic effects were graded by the national cancer institute common toxicity criteria version 2.0.19 all scans were reviewed by a radiologist ( rn ) who was blinded to treatment assignment . 
standard who the best response criteria were used antitumour effects recorded.20 complete response was dened as the disappearance of all measurable and assessable disease in all disease sites ; partial response as a decrease of 50% or more in the sum of the products of the perpendicular diameters of all measurable lesions , with no new lesions or progression of assessable disease ; progressive disease as an increase of 25% or more of the product of the perpendicular diameters of all measurable lesions , the appearance of new lesions , or the reappearance of a lesion that had previously disappeared ; and stable disease as that which did not pefg ( n = 52 ) gemcitabine ( n = 47 ) 2 ( 16 ) 4 ( 06 ) 114 4 ( 18 ) 4 ( 17 ) 17 ( 925 ) 10 ( 816 ) number of cycles median ( range ) total number of cycles time between randomisation and treatment ( days ) median ( iqr ) duration of chemotherapy ( weeks ) median ( iqr ) table 2 : details of treatment meet the criteria for the above.20 the duration of complete response was dened as the time between the rst documentation of complete disease resolution and the rst documented observation of progressive disease , and the duration of partial response as the time between start of treatment and rst observation of progressive disease . 
 to have a clinical benet clinical benet was assessed on the basis of pain , karnofsky performance status , and change in bodyweight as described previously.1 briey , patients were thought they had an increase of 20 points or more from baseline karnofsky performance status score , a decrease of 50% or more in use of analgesics from baseline , or a reduction of 50% or more in baseline memorial pain assessment card score , without being negative for either of the other two criteria . 
 vol 6 june 2005 articles age ( continuous variable ) group ( pefg [ n = 52 ] vs gemcitabine [ n = 47 ] ) stage ( iva [ n = 29 ] vs metastatic [ n = 70 ] ) karnofsky performance status ( continuous variable ) table 4 : multivariate analyses progression - free survival hazard ratio ( 95 % ci ) 098 ( 096100 ) 050 ( 033077 ) 213 ( 133341 ) 099 ( 098101 ) 01080 00021 00020 04697 overall survival hazard ratio ( 95% ci ) 098 ( 095100 ) 063 ( 041096 ) 210 ( 129342 ) 099 ( 097100 ) 00717 00345 00035 01573 statistical analysis on the basis of progression - free survival curves for gemcitabine1 and pefg , 16 and in view of the idea that a large difference in progression - free survival could be found only in the direction of the pefg group and that the number of events would correspond to the number of patients because progressive disease or death for all patients was anticipated at the time of nal analysis , a sample size of 100 patients was planned to attain 90% probability of detecting ( with a one - sided 5% ( cid : 8 ) level ) a 30% absolute difference in 4 - month progression - free survival . 
no interim analysis was planned or done , and no early - stopping rule was planned for this trial . ( median follow - up 335 months results patients final analyses were done on feb 28 , 2005 , when all living patients had completed at least 24 months of follow - up [ range 240460 ] )  . 
23 patients in the pefg group and 20 patients in the gemcitabine group were assessable for assessment of clinical benet , and 37 ( 19 and 18 , respectively ) did not meet the eligibility criteria , and 19 ( 10 and 9 , respectively ) were not compliant . table 1 shows baseline characteristics of patients by treatment group . 
dose intensity was 95 mg / m2 a week ( 95% of intended dose ) for epirubicin and cisplatin , 1140 mg / m2 a week ( 81% ) for uorouracil , and 255 mg / m2 a week ( 85% ) for gemcitabine . 
treatment three discontinued was discontinued before completion in 27 patients : 20 had progressive disease , four refused to continue chemotherapy ( one with partial response and three with stable disease ) , and treatment because of doctors instructions ( two with partial response and one with stable disease )  . 
dose intensity was 734 mg / m2 a week ( 92% of intended dose )  . treatment was discontinued before completion in 37 patients : 32 had progressive disease , two had stable disease and refused to continue chemotherapy , two patients with stable disease discontinued treatment because of pneumonia and febrile jaundice , and one patient with a partial response discontinued treatment because of doctors instructions . after chemotherapy , radiotherapy ( median 54 gy , range 5456 ) was given to six of 15 patients in the pefg group with stage iva disease ( one of whom was admitted to surgery ) , and to ve of 14 patients in the gemcitabine group with stage iva disease . 
one patient ( allocated gemcitabine alone ) had a reduction in tumour size of more than 25% , absence of clinical benet , and a reduction in ca19.9 of more than 50% of baseline concentration after 4 months . 
this patient refused to continue chemotherapy and received radiotherapy . log - rank p = 0047 pefg gemcitabine follow - up ( months ) numbers at risk pefg gemcitabine figure 3 : overall survival * one patient died 1 week after randomisation before starting treatment . 
at the time of nal analysis two patients were progression free , one patient in the pefg group ( at ( cid : 7 ) 23 months ) and one patient in the gemcitabine group ( 31 months )  . 
 at follow - up , 95 patients had died of disease progression : three patients ( one with metastatic disease ) assigned pefg and one patient with stage iva disease assigned gemcitabine were alive at feb 28 , 2005 ( n = 2 ) , feb 3 , 2005 ( ( cid : 7 ) 33 months survival for one patient assigned pefg ) , and at feb 9 , 2005 ( ( cid : 7 ) 25 months survival for one patient assigned pefg )  . 
the hazard ratio for death in the pefg group compared with the gemcitabine group was 065 ( 95% ci 043099 , p = 0047 , log - rank test )  . 
the proportion of patients with 1 - year and 2 - year overall survival was greater in the pefg group than in the gemcitabine group ( table 3 , gure 3 )  . 
 radiological analyses showed that one patient had a complete response and 19 had partial responses after pefg treatment compared with four patients who had a partial response after gemcitabine treatment ( odds ratio 660 [ 2112060 ] , p = 00008 ; table 5 )  . 
median duration of partial response was 95 months ( iqr 63129 ) after pefg and 69 months ( 4387 ) after gemcitabine ; median duration of stable disease was 52 months ( 3888 ) after pefg and 56 months ( 4692 ) after gemcitabine . 
15 ( 65% [ 95% ci 4581 ] ) of 23 patients assigned pefg had a clinical benet compared with ve ( 25% [ 1147 ] ) of 20 patients assigned gemcitabine ( p = 00139 )  . table 6 shows treatment - related side - effects . 
growth factors chosen by the attending physician were used for 3 days in ve patients assigned pefg ( one patient at cycle one , one at cycle two , two at cycle three , and two at cycle ve ) , and in two patients assigned gemcitabine ( one patient at cycle one and one at cycle ve )  . 
red - cell transfusion was used in six patients assigned pefg ( one patient at cycle one , one at cycle two , two at cycle three , and two at cycle in four patients assigned gemcitabine ve ) , and ( four patients at cycle one and one at cycle six )  . erythropoietin chosen by the attending physician was given to three patients in the pefg group and to four patients in the gemcitabine group . 
there were no treatment - related deaths . findings of the quality - of - life analyses have been reported previously.24 our sample size was insufcient to obtain adequate statistical power to detect reliably differences between groups for multiple comparisons . although conventional statistical testing was not done , we noted that patients allocated pefg were 2044% more likely to obtain a clinically relevant improvement in scores for emotional functioning , overall quality of life , cognitive measures , pain , fatigue , indigestion , dyspnoea , appetite loss , and atulence than were those allocated gemcitabine . 
patients in the gemcitabine group had better scores for sexual function and body image than did those in the pefg group . than 86 patients had radiological documentation of progressive disease . 
22 of 45 patients assigned pefg and 25 of 41 patients assigned gemcitabine received salvage therapy with more ten different regimens . 17 patients in the gemcitabine group received salvage pefg . 
the median interval between progression and death was 39 months ( iqr 2171 ) in the pefg group and 38 months ( 2782 ) in the gemcitabine group ( p = 03536 )  . 
in the subset of patients who had salvage treatment , median interval between progression and death was 68 months ( 3791 ) in the pefg group and 70 months ( 4592 , p = 04301 )  . discussion we have shown that patients allocated pefg had a more favourable outcome in terms of progression - free survival and overall survival than did those allocated standard treatment with gemcitabine . 
after a minimum follow - up of 24 months , the survival advantage of pefg was maintained at 1 year and at 2 years , and was conrmed by multivariate analyses . 
 febrile neutropenia , use of growth gemcitabine was approved on the basis of data from a trial that used clinical benet as a primary endpoint.1 however , this measure was not validated and its use has been criticised because it did not take into account quality of life.25 we have shown that pefg is associated with a signicantly improved clinical benet compared with gemcitabine alone . 
furthermore , although conventional statistical testing for quality of life was not done , when all the descriptive data were taken into account quality of life for patients assigned pefg was at least equal to that for the gemcitabine group for most scales . 
this nding further supports the use of combination chemotherapy compared with gemcitabine in that improved clinical outcome with pefg is not achieved at the cost of impaired quality of life . favour the main drawbacks of our study are with regard to sample size and the generalisability of results . 
the sample size , which might seem combination group , was calculated on the basis of previous data1 , 16 that suggested an unusually large difference in progression - free survival between pefg and standard treatment . 
the choice to calculate sample size by a one - sided test was based on the idea that a large difference in outcome could be found only in the direction of the pefg group , and that treatment - related or catheter - related complications in this group could not worsen the outcome.16 , 2628 our ndings conrm the validity of both assumptions . 
however , if we had used a two - sided test , our sample size would have been about the same ( ie , 49 patients per group ) to achieve 80% probability of detecting , with a 5% ( cid : 8 ) level , a 30% difference from 35% to 65% . 
with regard to validity of the control group and generalisability of results , comparisons with different trials are difcult and remain speculative because of differences in selection criteria and imbalances in prognostic factors . 
the proportion of patients with a karnofsky performance status of more than 70 or with metastatic disease in our study is consistent with those in previous phase iii trials in pancreatic adenocarcinoma.111 by contrast , these trials included patients with a more favourable prognosis , 2 such as those with stage iii disease13 , 5 , 6 , 10 or patients older than 70 years , 13 , 5 , 6 , 810 which could have positively biased the outcome , as could have a dropout of more than 20% of patients during the lead - in period.1 nevertheless , the safety , dose - intensity , activity , and efcacy of our control group was consistent with other series , 111 suggesting that such factors had a negligible effect on outcome . we chose 4 - month progression - free survival as our primary endpoint . 
however , progression - free survival is associated with a risk of : assessment bias in unblinded trials ; unequal time interval of progression assessment across treatment groups ; asymmetrical censoring ; and inappropriate crediting of an unknown amount of additional progression - free time in patients who die without documentation of progressive disease and who have the date of death recorded as the progression date . 
in our trial , the timing of tumour assessment was identical in the two groups , and a radiologist blinded to treatment group centrally reviewed ct scans to keep the effects of biases on progression - free survival to a minimu furthermore , about 10% of patients were not assessable for the primary endpoint because scans were not done in time to document progression , and the comparison between progressionfree - survival curves was repeated with these patients omitted , with similar ndings ( p = 0005 , data not shown )  . furthermore , the time between progression and death was much the same for both groups , suggesting that salvage therapy had a similar effect on outcome in both groups , and that progression - free survival might be an adequate prediction of overall survival . 
previous trials have used 6 - month progression - free survival as the primary endpoint , and on the basis of previously reported data for 6 - month progression - free survival ( 52% for pefg vs 22% for gemcitabine ) , 16 if we had chosen this endpoint for our sample calculation , the number of patients would have been about the same ( 48 patients per group with ( cid : 8 ) = 005 and ( cid : 10 ) = 01 , one - sided test )  . 
nevertheless , our ndings are important because pefg had manageable toxic effects , did not negatively affect quality of life , and maintained a statistically and clinically relevant outcome advantage compared with standard treatment . 
accordingly , pefg might be a feasible and effective rst - line treatment for patients with locally advanced or metastatic pancreatic adenocarcinoma . contributors m reni and l galli were responsible for the study idea , study design , data analysis and interpretation , and drafting of the article . 
m reni , s cordio , c milandri , p passoni , e bonetto , c oliani , g luppi , r nicoletti , r bordonaro , a passardi , a zerbi , g balzano , l aldrighetti , c staudacher , e villa , and v di carlo participated in data acquisition . all authors were involved in critical review of the article . 
m reni had full access to all data in the study and had nal responsibility for the decision to submit for publication . conict of interest we declare no conicts of interest . acknowledgments no funding was received for this study . reection and reaction management of chemotherapy - induced side - effects ( 5 - ht3 ) antagonist developments summary of in their review , sharma and colleagues1 provided an excellent chemotherapy - induced nausea , management of vomiting , mucositis , and diarrhoeacommon sources of psychological and physical distress in patients with cancer . 
an important addition to this list is mirtazapine , a 5 - ht3 receptor antagonist , which has proven to be an effective antiemetic agent.26 specically , mirtazapine has been associated with relief of nausea , vomiting , and other common comorbidities related to cancer chemotherapy and radiotherapy.25 as well as having antiemetic effects , mirtazapine is also effective in treatment of depressive symptoms , pain , anorexia , anxiety , and insomnia comorbidities that are common in patients with cancer and have been linked to poor quality of life and compliance with treatment.25 , 7 receptors , opiate - like mirtazapine enhances noradrenergic and serotonergic neurotransmission via its antagonism of 5 - ht3 and central presynaptic ( cid : 2 ) 2 adrenergic enhanced agonism at the 5 - ht1 receptor , and its activities.810 possible important drawbacks of mirtazapine are the absence of induction of sedation at low doses . 
other sideeffects include constipation and weight ga intravenous formulation , and antinociceptive its because of its salutary effects on common cancerrelated complications , mirtazapine , as part of an antiemetic treatment regimen , might decrease the need for additional drugs for these complications , potentially leading to fewer adverse drugdrug interactions , lower costs , and improved overall quality of life for these patients . 
a large , controlled , clinically comparative trial of mirtazapine and other 5 - ht3 receptor antagonists could help dene the optimum and most cost - effective therapeutic regimen for nausea and vomiting in patients with cancer who are undergoing treatment . 
 mukaila a raji outpatient geriatrics clinics , sealy center on aging , department of internal medicine , university of texas medical branch , 301 university boulevard , galveston , tx , usa muraji@utmb.edu i declare no conicts of interest . sharma r , tobin p , clarke sj . 
lancet oncol 2005 ; 6 : 138the news in brief story , oestrogen and lung - cancer survival , should read : the investigators used getinib to block the epidermal - growthfactor - receptor pathway and fulvestrant to block the oestrogen pathway in mice with grafter lung tumours . polychronis a , sinnett hd , hadjiminas d , et al . 
preoperative getinib versus getinib and anastrozole in postmenopausal patients with oestrogen - receptor positive and epidermal - growth - factorreceptor - positive primary breast cancer : a double - blind placebocontrolled phase ii randomised trial . 
dose - response study of myo - inositol as an inhibitor of lung tumorigenesis induced in a / j mice by benzo [ a ] pyrene and 4 - ( methylnitrosamino ) - 1 ( 3 - pyridyl ) - 1 - butane . 
anticarcinogenic activities of organic isothiocyanates : chemistry and mechaniscancer res 1994 ; 54 ( suppl ) : 1976s81s . 64 sticha krk , staretz me , wang m , et al . 
effects of benzyl isothiocyanate and phenethyl isothiocyanate on benzyl [ a ] pyrene metabolism and dna adduct formation in the a / j mouse . carcinogenesis 2000 ; 21 : 171119 . 65 chen yr , wang w , kong ant , tan th . 
effects of phenethyl isothiocyanate and benzyl isothiocyanate , individually and in combination , on lung tumorigenesis induced in a / j mice by benzo [ a ] pyrene and 4 - ( methylnitrosamino ) - 1 - ( 3 - pyridyl ) - 1butanone . 
chemopreventive effects of myoinositol and dexamethasone on benzo [ a ] pyrene and 4 - ( methylnitrosamino ) - 1 - ( 3 - pyridyl ) - 1 - butanone - induced pulmonary carcinogenesis in female a / j mice . 
only reproduce with permission from the lancet publishing group . articles lancet oncol 2005 ; 6 : 36976 published online may 10 , 2005 70175 - 3 see reection and reaction page 352 department of radiochemotherapy ( m reni md , p passoni md , e bonetto md , e villa md ) , department of radiology ( r nicoletti md ) , department of statistics ( l galli msc ) , and department of surgery ( a zerbi md , g balzano md , l aldrighetti md , prof c staudacher md , prof v di carlo md ) , s raffaele h scientic institute , milan , italy department of oncology , s luigi curr h catania , italy ( s cordio md , r bordonaro md ) ; department of oncology , pierantoni h forl , italy ( c milandri md , a passardi md ) ; department of oncology , azienda ospedaliera and university , verona , italy ( c oliani md ) ; department of medical oncology , azienda ospedaliera - policlinico , modena , italy ( g luppi md ) correspondence to : dr michele reni , department of oncology , san raffaele h scientic institute , via olgettina 60 , 20132 milan , italy reni.michele@hsr.it gemcitabine versus cisplatin , epirubicin , uorouracil , and gemcitabine in advanced pancreatic cancer : a randomised controlled multicentre phase iii trial michele reni , stefano cordio , carlo milandri , paolo passoni , elisa bonetto , cristina oliani , gabriele luppi , roberto nicoletti , laura galli , roberto bordonaro , alessandro passardi , alessandro zerbi , gianpaolo balzano , luca aldrighetti , carlo staudacher , eugenio villa , valerio di carlo summary background patients with advanced pancreatic adenocarcinoma have a poor response , progression - free survival , and overall survival with standard treatment . 
 methods in a randomised multicentre phase iii trial , 52 patients were randomly assigned to 40 mg / m2 cisplatin and 40 mg / m2 epirubicin both given on day 1 , 600 mg / m2 gemcitabine given intravenously over 1 h on days 1 and 8 , and 200 mg / m2 uorouracil a day given by continuous infusion on days 128 of a 4 - week cycle ( pefg regimen ) , and 47 were assigned to 1000 mg / m2 gemcitabine given intravenously over 30 min once a week for 7 of 8 consecutive weeks in cycle 1 and for 3 of 4 weeks thereafter . 
more patients allocated pefg than gemcitabine alone were alive without progressive disease at 4 months ( 60% [ 95% ci 4672 ] vs 28% [ 1742 ] ; hazard ratio [ hr ] 046 [ 026079 ] )  . 
1 - year overall survival in the pefg group was 385% ( 253517 ) and in the gemcitabine group was 213% ( 96330 ; hr 068 [ 042109 ] )  . 
more patients assigned pefg showed disease response than did those assigned gemcitabine ( 385% [ 253517 ] vs 85% [ 05165 ] ; odds ratio 660 [ 2112060 ] , p = 00008 )  . 
more patients in the pefg group had grade 34 neutropenia and thrombocytopenia than in the gemcitabine group ( p ( cid : 2 ) 00001 )  . interpretation the pefg regimen could be considered for treatment of advanced pancreatic adenocarcinoma . introduction pancreatic adenocarcinoma is associated with a poor prognosis . 
more than 80% of patients present with advanced disease at diagnosis , and mortality is high because tumours inltrate the abdominal blood vessels and spread to regional lymph nodes and liver at an early stage . 
gemcitabine the standard treatment for unresectable disease , and has led to an objective response in 426% of patients and a 1 - year overall survival of 1728% in phase iii trials.111 gemcitabine was licensed for treatment of advanced pancreatic cancer on the basis of improved clinical benet and increased overall survival compared with uorouracil.1 is regarded as improve several attempts the efcacy of gemcitabine in advanced pancreatic adenocarcinoma by use of new agents or by addition of a second cytotoxic agent or other drugs to a standard dose and schedule of gemcitabine have not shown a survival advantage.211 however , a signicant benet in median progressionfree survival has been noted for gemcitabine combined with uorouracil , 2 cisplatin , 7 or oxaliplatin , 11 which suggests that platinum - based agents and antifolates have a role in treatment of pancreatic cancer . 
moreover , although combination treatment did not increase overall survival compared with gemcitabine alone , whether salvage therapy affects the relation between progressionfree survival and overall survival is not known . 
strategies that have not included gemcitabine have been assessed , but have not shown better results.12 , 13 findings from a phase ii trial14 suggested that xed - dose gemcitabine improves survival , but phase iii data are not available . gemcitabine combined with erlotinib improved 1 - year overall survival compared with gemcitabine alone from 17% to 24%.15 cisplatin , epirubicin , uorouracil , and gemcitabine ( pefg ) an empirically derived treatment based on four agents that are active against pancreatic adenocarcinomashowed promising activity with regard to response rate and survival in a previous phase ii trial.16 we therefore did a multicentre randomised phase iii trial to compare standard treatment of gemcitabine with that of pefg by use of previously dened doses and schedules.16 methods patients between april , 2000 , and march , 2003 , 104 patients from ve institutions aged 1870 years with histovol 6 june 2005 articles 104 patients randomised 54 allocated pefg 50 allocated gemcitabine 2 ineligible ( inadequate liver function ) 3 ineligible 2 inadequate liver function 1 other cancer 52 analysed 47 analysed figure 1 : trial prole intensity score of 20 mm or more of a possible 100 mm on the memorial pain assessment card , 18 or a karnofsky performance status of 5070 . 
the study was done in accordance with the declaration of helsinki and approved by the local ethics committees of participating institutions ; written informed consent was obtained from all patients . 
 study objectives we chose 4 - month progression - free survival as the primary endpoint to avoid the potential effect of salvage treatment after progression on overall survival and the potential effect of surgery or radiotherapy ( allowed after 4 months in patients with stage iva disease ) on both overall survival and progression - free survival . 
secondary endpoints were overall survival , objective response , clinical benet , safety , and quality of life . randomisation patients who fullled all inclusion criteria were registered by the attending physician at the coordinating institution . 
patients were stratied by centre and stage ; the trial was unblinded . analysis was by intention to treat . treatment plan 54 patients were allocated to pefg regimens that were repeated every 28 days16 and that consisted of 40 mg / m2 cisplatin ( cisplatino - teva , pharmachemie bv , haarlem , netherlands ) and 40 mg / m2 epirubicin ( farmarubicina , pharmacia & upjohn spa , milan , italy ) given intravenously on day one , 600 mg / m2 gemcitabine ( gemzar , eli lilly , fegersheim , france ) given in 1 h on days 1 and 8 , and 200 mg / m2 uorouracil ( fluorouracile - teva , pharmachemie bv , haarlem , netherlands ) a day as protracted infusion for the duration of chemotherapy by use of an indwelling , catheter . guidelines for dose reduction and treatment delay have been reported previously.16 50 patients were allocated to 1000 mg / m2 gemcitabine a week given intravenously over 30 min for 7 consecutive weeks followed by 1 week of rest , and then subsequently for 3 of every 4 weeks . 
treatment was delayed if absolute neutrophil count was less than 1000 ( cid : 4 ) 106 cells / l , platelet count was less than 50 ( cid : 4 ) 109 / l , or if the patient developed grade 34 non - haematological toxic effects . patients were removed from the study if recovery was not evident within 2 weeks . 
patients who had ampullary tumours , other histological variants of pancreatic carcinoma , previous adjuvant chemotherapy , or previous malignant disease were ineligible for the study , with the exception of those who had had basalcell carcinoma of the skin , carcinoma in situ of the cervix , or other cancers for which the patient had been disease - free for at least 5 years . 
 eligibility criteria for assessment of clinical benet were baseline use of analgesics of at least two nonsteroidal anti - inammatory drugs , baseline pain pefg ( n = 52 ) gemcitabine ( n = 47 ) 62 ( 3769 ) 59 ( 2569 ) age ( years ) median ( range ) male female karnofsky performance status ( cid : 7 ) 70 ( cid : 5 ) 70 stage metastatic previous treatment pancreatic surgery radiotherapy or chemotherapy site of metastases liver lymph nodes lung table 1 : baseline characteristics vol 6 june 2005 articles pefg ( n = 52 ) gemcitabine ( n = 47 ) hazard ratio ( 95% ci ) progression - free survival ( months ) 4 - month ( 95% ci ) median ( iqr ) overall survival 1 - year ( 95% ci ) 2 - year ( 95% ci ) 60% ( 4672 ) 54 ( 2096 ) 28% ( 1742 ) 33 ( 2253 ) 046 ( 026079 ) 051 ( 033078 ) 0001 00033 385% ( 253517 ) 115% ( 28202 ) 213% ( 96330 ) 21% ( 0062 ) 068 ( 042109 ) 063 ( 042096 ) 01119 0033 table 3 : progression - free survival and overall survival time the dose of gemcitabine was lowered by 25% . both groups were allocated treatment for a maximum of 6 monthsie , six cycles of pefg and ve of gemcitabine . 
treatment was continued up to this time unless unacceptable side - effects developed , disease progressed , the patient refused treatment , or a medical decision was made to stop treatment . 
in patients with stage iva disease treatment was classied as complete after 4 months if no clinical benet was seen , the reduction in tumour size was less than 25% , or if ca19.9 concentration decreased to less than 50% of baseline . 
at the end of treatment , patients with operable stage iva disease were recommended for surgery and were allowed to receive radiotherapy . assessment of disease , including spiral ct of the abdomen and chest , was done at baseline , every 8 weeks during chemotherapy , and then every 3 months . 
for assessment of clinical benet , patients were asked to record pain intensity every day by completion of a memorial pain assessment card and a diary on the use of analgesics . 
performance status and bodyweight were assessed once a week . to dene outcome measures toxic effects were graded by the national cancer institute common toxicity criteria version 2.0.19 all scans were reviewed by a radiologist ( rn ) who was blinded to treatment assignment . 
standard who the best response criteria were used antitumour effects recorded.20 complete response was dened as the disappearance of all measurable and assessable disease in all disease sites ; partial response as a decrease of 50% or more in the sum of the products of the perpendicular diameters of all measurable lesions , with no new lesions or progression of assessable disease ; progressive disease as an increase of 25% or more of the product of the perpendicular diameters of all measurable lesions , the appearance of new lesions , or the reappearance of a lesion that had previously disappeared ; and stable disease as that which did not pefg ( n = 52 ) gemcitabine ( n = 47 ) 2 ( 16 ) 4 ( 06 ) 114 4 ( 18 ) 4 ( 17 ) 17 ( 925 ) 10 ( 816 ) number of cycles median ( range ) total number of cycles time between randomisation and treatment ( days ) median ( iqr ) duration of chemotherapy ( weeks ) median ( iqr ) table 2 : details of treatment meet the criteria for the above.20 the duration of complete response was dened as the time between the rst documentation of complete disease resolution and the rst documented observation of progressive disease , and the duration of partial response as the time between start of treatment and rst observation of progressive disease . 
 to have a clinical benet clinical benet was assessed on the basis of pain , karnofsky performance status , and change in bodyweight as described previously.1 briey , patients were thought they had an increase of 20 points or more from baseline karnofsky performance status score , a decrease of 50% or more in use of analgesics from baseline , or a reduction of 50% or more in baseline memorial pain assessment card score , without being negative for either of the other two criteria . 
 vol 6 june 2005 articles age ( continuous variable ) group ( pefg [ n = 52 ] vs gemcitabine [ n = 47 ] ) stage ( iva [ n = 29 ] vs metastatic [ n = 70 ] ) karnofsky performance status ( continuous variable ) table 4 : multivariate analyses progression - free survival hazard ratio ( 95 % ci ) 098 ( 096100 ) 050 ( 033077 ) 213 ( 133341 ) 099 ( 098101 ) 01080 00021 00020 04697 overall survival hazard ratio ( 95% ci ) 098 ( 095100 ) 063 ( 041096 ) 210 ( 129342 ) 099 ( 097100 ) 00717 00345 00035 01573 statistical analysis on the basis of progression - free survival curves for gemcitabine1 and pefg , 16 and in view of the idea that a large difference in progression - free survival could be found only in the direction of the pefg group and that the number of events would correspond to the number of patients because progressive disease or death for all patients was anticipated at the time of nal analysis , a sample size of 100 patients was planned to attain 90% probability of detecting ( with a one - sided 5% ( cid : 8 ) level ) a 30% absolute difference in 4 - month progression - free survival . 
no interim analysis was planned or done , and no early - stopping rule was planned for this trial . ( median follow - up 335 months results patients final analyses were done on feb 28 , 2005 , when all living patients had completed at least 24 months of follow - up [ range 240460 ] )  . 
23 patients in the pefg group and 20 patients in the gemcitabine group were assessable for assessment of clinical benet , and 37 ( 19 and 18 , respectively ) did not meet the eligibility criteria , and 19 ( 10 and 9 , respectively ) were not compliant . table 1 shows baseline characteristics of patients by treatment group . 
dose intensity was 95 mg / m2 a week ( 95% of intended dose ) for epirubicin and cisplatin , 1140 mg / m2 a week ( 81% ) for uorouracil , and 255 mg / m2 a week ( 85% ) for gemcitabine . 
treatment three discontinued was discontinued before completion in 27 patients : 20 had progressive disease , four refused to continue chemotherapy ( one with partial response and three with stable disease ) , and treatment because of doctors instructions ( two with partial response and one with stable disease )  . 
dose intensity was 734 mg / m2 a week ( 92% of intended dose )  . treatment was discontinued before completion in 37 patients : 32 had progressive disease , two had stable disease and refused to continue chemotherapy , two patients with stable disease discontinued treatment because of pneumonia and febrile jaundice , and one patient with a partial response discontinued treatment because of doctors instructions . after chemotherapy , radiotherapy ( median 54 gy , range 5456 ) was given to six of 15 patients in the pefg group with stage iva disease ( one of whom was admitted to surgery ) , and to ve of 14 patients in the gemcitabine group with stage iva disease . 
one patient ( allocated gemcitabine alone ) had a reduction in tumour size of more than 25% , absence of clinical benet , and a reduction in ca19.9 of more than 50% of baseline concentration after 4 months . 
this patient refused to continue chemotherapy and received radiotherapy . log - rank p = 0047 pefg gemcitabine follow - up ( months ) numbers at risk pefg gemcitabine figure 3 : overall survival * one patient died 1 week after randomisation before starting treatment . 
at the time of nal analysis two patients were progression free , one patient in the pefg group ( at ( cid : 7 ) 23 months ) and one patient in the gemcitabine group ( 31 months )  . 
 at follow - up , 95 patients had died of disease progression : three patients ( one with metastatic disease ) assigned pefg and one patient with stage iva disease assigned gemcitabine were alive at feb 28 , 2005 ( n = 2 ) , feb 3 , 2005 ( ( cid : 7 ) 33 months survival for one patient assigned pefg ) , and at feb 9 , 2005 ( ( cid : 7 ) 25 months survival for one patient assigned pefg )  . 
the hazard ratio for death in the pefg group compared with the gemcitabine group was 065 ( 95% ci 043099 , p = 0047 , log - rank test )  . 
the proportion of patients with 1 - year and 2 - year overall survival was greater in the pefg group than in the gemcitabine group ( table 3 , gure 3 )  . 
 radiological analyses showed that one patient had a complete response and 19 had partial responses after pefg treatment compared with four patients who had a partial response after gemcitabine treatment ( odds ratio 660 [ 2112060 ] , p = 00008 ; table 5 )  . 
median duration of partial response was 95 months ( iqr 63129 ) after pefg and 69 months ( 4387 ) after gemcitabine ; median duration of stable disease was 52 months ( 3888 ) after pefg and 56 months ( 4692 ) after gemcitabine . 
15 ( 65% [ 95% ci 4581 ] ) of 23 patients assigned pefg had a clinical benet compared with ve ( 25% [ 1147 ] ) of 20 patients assigned gemcitabine ( p = 00139 )  . table 6 shows treatment - related side - effects . 
growth factors chosen by the attending physician were used for 3 days in ve patients assigned pefg ( one patient at cycle one , one at cycle two , two at cycle three , and two at cycle ve ) , and in two patients assigned gemcitabine ( one patient at cycle one and one at cycle ve )  . 
red - cell transfusion was used in six patients assigned pefg ( one patient at cycle one , one at cycle two , two at cycle three , and two at cycle in four patients assigned gemcitabine ve ) , and ( four patients at cycle one and one at cycle six )  . erythropoietin chosen by the attending physician was given to three patients in the pefg group and to four patients in the gemcitabine group . 
there were no treatment - related deaths . findings of the quality - of - life analyses have been reported previously.24 our sample size was insufcient to obtain adequate statistical power to detect reliably differences between groups for multiple comparisons . although conventional statistical testing was not done , we noted that patients allocated pefg were 2044% more likely to obtain a clinically relevant improvement in scores for emotional functioning , overall quality of life , cognitive measures , pain , fatigue , indigestion , dyspnoea , appetite loss , and atulence than were those allocated gemcitabine . 
patients in the gemcitabine group had better scores for sexual function and body image than did those in the pefg group . than 86 patients had radiological documentation of progressive disease . 
22 of 45 patients assigned pefg and 25 of 41 patients assigned gemcitabine received salvage therapy with more ten different regimens . 17 patients in the gemcitabine group received salvage pefg . 
the median interval between progression and death was 39 months ( iqr 2171 ) in the pefg group and 38 months ( 2782 ) in the gemcitabine group ( p = 03536 )  . 
in the subset of patients who had salvage treatment , median interval between progression and death was 68 months ( 3791 ) in the pefg group and 70 months ( 4592 , p = 04301 )  . discussion we have shown that patients allocated pefg had a more favourable outcome in terms of progression - free survival and overall survival than did those allocated standard treatment with gemcitabine . 
after a minimum follow - up of 24 months , the survival advantage of pefg was maintained at 1 year and at 2 years , and was conrmed by multivariate analyses . 
 febrile neutropenia , use of growth gemcitabine was approved on the basis of data from a trial that used clinical benet as a primary endpoint.1 however , this measure was not validated and its use has been criticised because it did not take into account quality of life.25 we have shown that pefg is associated with a signicantly improved clinical benet compared with gemcitabine alone . 
furthermore , although conventional statistical testing for quality of life was not done , when all the descriptive data were taken into account quality of life for patients assigned pefg was at least equal to that for the gemcitabine group for most scales . 
this nding further supports the use of combination chemotherapy compared with gemcitabine in that improved clinical outcome with pefg is not achieved at the cost of impaired quality of life . favour the main drawbacks of our study are with regard to sample size and the generalisability of results . 
the sample size , which might seem combination group , was calculated on the basis of previous data1 , 16 that suggested an unusually large difference in progression - free survival between pefg and standard treatment . 
the choice to calculate sample size by a one - sided test was based on the idea that a large difference in outcome could be found only in the direction of the pefg group , and that treatment - related or catheter - related complications in this group could not worsen the outcome.16 , 2628 our ndings conrm the validity of both assumptions . 
however , if we had used a two - sided test , our sample size would have been about the same ( ie , 49 patients per group ) to achieve 80% probability of detecting , with a 5% ( cid : 8 ) level , a 30% difference from 35% to 65% . 
with regard to validity of the control group and generalisability of results , comparisons with different trials are difcult and remain speculative because of differences in selection criteria and imbalances in prognostic factors . 
the proportion of patients with a karnofsky performance status of more than 70 or with metastatic disease in our study is consistent with those in previous phase iii trials in pancreatic adenocarcinoma.111 by contrast , these trials included patients with a more favourable prognosis , 2 such as those with stage iii disease13 , 5 , 6 , 10 or patients older than 70 years , 13 , 5 , 6 , 810 which could have positively biased the outcome , as could have a dropout of more than 20% of patients during the lead - in period.1 nevertheless , the safety , dose - intensity , activity , and efcacy of our control group was consistent with other series , 111 suggesting that such factors had a negligible effect on outcome . we chose 4 - month progression - free survival as our primary endpoint . 
however , progression - free survival is associated with a risk of : assessment bias in unblinded trials ; unequal time interval of progression assessment across treatment groups ; asymmetrical censoring ; and inappropriate crediting of an unknown amount of additional progression - free time in patients who die without documentation of progressive disease and who have the date of death recorded as the progression date . 
in our trial , the timing of tumour assessment was identical in the two groups , and a radiologist blinded to treatment group centrally reviewed ct scans to keep the effects of biases on progression - free survival to a minimu furthermore , about 10% of patients were not assessable for the primary endpoint because scans were not done in time to document progression , and the comparison between progressionfree - survival curves was repeated with these patients omitted , with similar ndings ( p = 0005 , data not shown )  . furthermore , the time between progression and death was much the same for both groups , suggesting that salvage therapy had a similar effect on outcome in both groups , and that progression - free survival might be an adequate prediction of overall survival . 
previous trials have used 6 - month progression - free survival as the primary endpoint , and on the basis of previously reported data for 6 - month progression - free survival ( 52% for pefg vs 22% for gemcitabine ) , 16 if we had chosen this endpoint for our sample calculation , the number of patients would have been about the same ( 48 patients per group with ( cid : 8 ) = 005 and ( cid : 10 ) = 01 , one - sided test )  . 
nevertheless , our ndings are important because pefg had manageable toxic effects , did not negatively affect quality of life , and maintained a statistically and clinically relevant outcome advantage compared with standard treatment . 
accordingly , pefg might be a feasible and effective rst - line treatment for patients with locally advanced or metastatic pancreatic adenocarcinoma . contributors m reni and l galli were responsible for the study idea , study design , data analysis and interpretation , and drafting of the article . 
m reni , s cordio , c milandri , p passoni , e bonetto , c oliani , g luppi , r nicoletti , r bordonaro , a passardi , a zerbi , g balzano , l aldrighetti , c staudacher , e villa , and v di carlo participated in data acquisition . all authors were involved in critical review of the article . 
m reni had full access to all data in the study and had nal responsibility for the decision to submit for publication . conict of interest we declare no conicts of interest . acknowledgments no funding was received for this study . reection and reaction use of endomyocardial biopsy to assess anthracyclineinduced cardiotoxicity a reection and reaction article , by young and colleagues1 has a few issues with regard to cumulative dose and endomyocardial assessment of cardiotoxicity that need to be corrected . 
none of the three articles quoted by these authors recorded a higher cumulative dose of liposomal doxorubicin than the dose in our report.2 only one of these publications included patients who had undergone endomyocardial biopsy assessment to exclude cardiotoxicity pathologically . 
 in the patients with kaposis sarcoma who were given a different anthracycline , liposomal daunorubicin , only 48% were assessed with at least one echocardiogram and none had histological assessment of anthracycline - induced cardiotoxicity . 
young and colleagues refer to the retrospective study comparing endomyocardial biopsy results ( by use of the billingham scale ) of patients given conventional and liposomal doxorubicin.1 however , the highest cumulative dose of 860 mg / m2 , in a patient who had no documentation of concomitant left - ventricular ejection fraction ( lvef ) , is much lower than the cumulative dose achieved by our patient . intervals furthermore , several important publications were not discussed in the commentary.1 a case series of 42 patients given pegylated liposomal doxorubicin were assessed at baseline and at specic for evidence of cardiotoxicity by use of multigated acquisition scans ( muga ) .3 some of these patients had received previous conventional anthracyclines . 
one patient in this series underwent three endomyocardial biopsies at cumulative liposomal doxorubicin doses of 600 mg / m2 , 900 mg / m2 , and 1320 mg / m2 , with no pathological evidence of cardiotoxicity on the billingham scale . 
a prospective study by gabizon and colleagues4 had enrolled eight patients with advanced malignant disease , all of whom had received previous chemotherapy ( four had been given conventional doxorubicin )  . 
in ve patients with kaposis sarcoma , liposomal doxorubicin cumulative doses ranged from 16802360 mg / m2 but no accompanying endomyocardial documentation of lack of cardiotoxicity was supplied.5 however , three patients had a decrease in lvef on echocardiography . endomyocardial biopsy is the most sensitive and specic investigation available for assessment of anthracyclineinduced cardiotoxicity , but the invasive nature of this test limits routine use.5 endomyocardial biopsy examination can detect cardiotoxicity before any ventricular dysfunction on muga or echocardiography.6 indication of leftcompared with our case , none of the publications described had a higher cumulative dose of liposomal doxorubicin with concurrent endomyocardial conrmation of the absence of cardiotoxicity . 
moreover , the dose achieved was much higher than the lifetime recommended cumulative dose of 450550 mg / m2 for conventional doxorubic this raises the interesting possibility of treatment with liposomal doxorubicin until progression in some circumstances . 
the use of liposomal anthracyclines in combination with other agents , especially trastuzumab , important message we hoped to reinforce . is another * robin l jones , david w miles * department of medical oncology , royal marsden hospital , london , uk . 
department of medical oncology , guys hospital , london , uk ; and breast unit , mount vernon hospital , northwood , middlesex , uk robin.jones@icr.ac.uk we declare no conicts of interest . young am , dhillon t , bower m . 
see - and - treat strategy for diagnosis and management of cervical squamous intraepithelial lesions . lancet oncol 2004 ; 6 : 4350 . in table 2 , data for ref 8 should have been cervical stenosis , 35 of 911 ( 38% )  . 
22 of 101 ( 218% ) occurred with lletz cone and 13 of 810 ( 16% ) with lletz . vol 6 february 2005 reflection & reaction truly informed the report . 
 honest patient - orientated information on survival for different types of cancer and options for palliative care must be made widely available to choices , ensure according it also demands the development of practice guidelines and standards with followup research to assess their effects . 
at a top policy level , the nci is urged to state - of - the - science convene meeting , include palliative care among its members , and to fund a high - profile research agenda to examine the quality of care , in addition for cures . searching specialist leadership of the nci should promote excellence and help produce the best possible practice guidelines . such guidance could help achieve a paradigm that patients palliative - care needs are assessed early in the course of their disease , while they are undergoing treatment , rather than waiting until death is very near . 
in the uk , increasing integration of hospices the national health service with ( nhs ) have continuity of good palliative care throughout the course of their disease . education and research in palliative techniques and psychosocial support now occur in several units in the uk . but charities cannot expect nhs funding to be standardised across the uk without the parameters of service provision being defined . 
the death in america project should be mirrored in europe , research and identifying more beacons of good practice . irene j higginson * and ilora g finlay facilitating * department of palliative care and policy , kings college london , weston education centre , cutcombe road , london , se5 9rj , uk . 
university of wales college of medicine section of oncology and palliative medicine , velindre hospital , whitchurch , cardiff , cf14 2tl . 1 esteve j , kricker a , ferlay j , parkin dm ( eds )  . 
facts and figures of cancer in the european community international agency for research on cancer commission of the european communities world health organization europe against cancer , 1993 . 2 foley km , gelband h . 
 3 lynn j , teno jm , phillips rs , et al . perceptions by family members of the dying experience of older and seriously ill patients : support investigators study to understand prognoses and preferences for outcomes and risks of treatments . 
 j clin oncol 2001 ; 19 : 20512 . erratum antisense therapy for cancerthe time of truth by burkhard jansen and uwe zangemeister - wittke . lancet oncol 2002 ; 3 : 67283 . the second paragraph on page 677 following the citation for figure 5 inferred that all patients survived beyond 1 year . 
policy analysis of cervical cancer screening strategies in low - resource settings : clinical benefits and cost - effectiveness . jama 2001 ; 285 : 310715 . 5 hartley p , daubenton jd . 
estimates of lung - cancer incidence in europe , 2000 women country crude rate asr cumulative risk * no of cases crude rate asr cumulative risk * no of cases eastern europe 872 877 belarus 742 bulgaria 984 czech republic 1361 hungary 490 moldova 943 poland romania 671 russian federation 880 800 slovakia 823 ukraine northern europe denmark estonia finland iceland ireland latvia lithuania norway sweden united kingdom 735 764 923 572 405 509 824 735 557 393 821 southern europe 959 albania 650 bosnia herzegovina 937 croatia greece italy macedonia malta portugal slovenia spain yugoslavia 1241 1006 1077 558 601 521 906 868 1105 western europe austria belgium france germany luxembourg netherlands switzerland 839 605 1257 796 834 904 927 739 697 710 489 689 955 471 782 507 749 685 615 443 468 699 368 315 395 615 577 351 214 476 588 792 812 825 558 594 469 445 339 644 532 809 532 421 764 535 502 605 620 485 * cumulative risks are for ages 064 years . 
only reproduce with permission from the lancet . reflection & reaction graham j caine and gregory yh lip haemostasis , thrombosis , and vascular biology unit , university department of medicine , city hospital , birmingham b18 7qh , uk . 1 nash gf , turner lf , scully mf , kakkar ak . 
incidence of cancer after prophylaxis with warfarin against recurrent venous thromboembolisn engl j med 2000 ; 342 : 195358 . 5 smorenburg sm , vink r , otten h - m , et al . the effects of vitamin k - antagonists on survival of patients with malignancy : a systematic analysis . 
clin exp metastasis 1991 ; 9 : 311 . 8 maurer lh , herndon je , hollis dr , et al . randomized trial of chemotherapy and radiation therapy with or without warfarin for limited - stage small - cell lung cancer : a cancer and leukaemia group b study . 
lancet 1994 ; 343 : 88689 . 10 chahinian ap , propert kj , ware jh , et al . a randomized trial of anticoagulation with warfarin and of alternating chemotherapy in extensive small - cell lung cancer by the cancer and leukaemia group b . 
in addition , the symptom duration for class iv should have read ( cid : 2 ) 3 months and the total radiation dose for class vi should have read ( cid : 2 ) 544 gy . 
only reproduce with permission from the lancet publishing group . aacr cancels annual meeting because of sars cases people have died from the disease , and there have been 111 probable and 95 suspected in ontario . 
 newsdesk the american association for cancer research cancelled its annual meeting 3 days before it was due to begin in toronto , canada ( april 59 , 2003 ) because of recent outbreak of severe acute respiratory syndrome ( sars )  . countrys the cancelling the meeting was a difficult decision to make , says the organisations chief executive officer margaret foti ( philadelphia , pa , usa )  . the aacr received 6900 abstracts , booked 400 speakers , and expected about 16 000 participants to attend the meeting , foti explains . 
ten torontos medical officer of health , sheela basrur , wrote a letter to the aacr emphasising the precautions that health - care providers should take while attending the meeting but did not advise the organisation to cancel the conference , says a spokesperson from toronto public health . 
however , we were still says foti . receiving cancellations , some cancer centres were advising their staff not to attend because of concerns about travelling to countries affected by sars and the potential transmission of the disease from health - care professionals to their immunocompromised patients with cancer , she explains . 
 the aacr contacted the world health organization , the us centers for disease control and prevention ( cdc ) , and toronto health officials , all of whom noted that there is not concern currently widespread transmission of sars to the community in toronto . 
 about india cuts budget for cancer treatment the indian government has cut financial support for cancer research and treatment , despite the country facing the massive challenge of nearly one million new cancer cases every year . 
in the central governments annual budget for 20032004 , allocation for the national cancer control programme ( nccp ) has been reduced to rs 520 million from rs 580 million . 
the nccp official approached by the lancet oncology preferred to remain anonymous but did say that the cut may be due to the fact that we were not able to absorb all the funds allotted to us in the past . jyotsna govil of the indian cancer society remarks : this is a prime example of tokenism in matters of health . the allocation has been so meagre that a state like delhi receives as little as rs15 million per annum for hospitals run by the local administration . 
govil points out that it is obvious the government has little use for a cancer education and prevention programme , despite every medical authority saying the incidence can be cut by 70% with screening and awareness programmes . experts say india needs rational budgeting for cancer programmes . 
at present , patients presenting with latestage disease , because of lack of awareness , prove to be a financial burden as scarce resources are used in their treatment without much outcome in terms of long - term survival . in addition to awareness and early detection , we need to spend money on treatment facilities to do away with lists . 
only reproduce with permission from the lancet publishing group . reection and reaction see extras / 04oncl0604webtable1.pdf november , 2004 , issue of the lancet oncology is an example of a report that fails to use rigorously standard , agreed criteria.5 these sorts of errors are most evident in webtable 1 of their review . 
 it is important that standard oncological criteria are used so that researchers can compare results and so that practicing physicians can make enlightened choices about how best to treat their patients . 
in oncology , the most commonly used criteria are those set forth by the international union against cancer and who , which dene an objective clinical response as a reduction of at least 50% in the sum of the product of perpendicular diameters of all tumours , without the growth of any tumour by more than 25% and without the appearance of any new tumours.6 another set of criteria , designated response evaluation criteria in solid tumours ( recist ) , is in many ways similar to the who criteria and designates that an objective response can be declared if there is at least a 30% reduction in the longest diameters of all target lesions . 
in the recist criteria , no target lesion can grow by 20% or more and no new lesions can appear.7 it is obvious that a clear - eyed perspective on cancer vaccines is needed if we are to make real progress . 
it is important with use of these standard criteria that responses cannot automatically be attributed to the effect of a cancer vaccine when patients are treated simultaneously with other surgery , known and effective chemotherapy , interleukin 2 , or radiotherapy . 
 symptoms and claims of benet to patients that include improvement longer - than - expected survival are subjective and generally uncontrolled.4 finally , use of surrogate endpoints such as the generation of anti - tumour t cells in vivo is of interest , but is not a substitute for tumour regression in assessment of the clinical effect of an experimental treatment . we think that progress will be made to improve cancer vaccines by the denition of ligands for toll - like receptors and of the way in which the innate and adaptive immune systems interact , as well as by the inhibition of negative regulatory signals , such as those provided by ctla4 and regulatory t cells . 
these and many other experimental approaches are being tested in preclinical and clinical trials . but perhaps cancer vaccines will be most effective when they are used in combination with adoptive cell - transferbased immunotherapeutic regimens . * nicholas p restifo , steven a rosenberg us national cancer institute , national institutes of health , bethesda , md 20892 , usa restifo@nih.gov we declare no conicts of interest . rosenberg sa , dudley me . 
cancer regression in patients with metastatic melanoma after the transfer of autologous antitumor lymphocytes . proc natl acad sci usa 2004 ; 101 ( suppl 2 ) : 1463945 . klebanoff ca , finkelstein se , surman dr , et al . 
part 1 : vaccines for solid tumours . lancet oncol 2004 ; 5 : 68189 . in webtable 1 : data for ref 29 should have been cr , 2 ; pr , 2 ; data for ref 31 should have been pr , 4 ; data for ref 79 should have been pr , 6 of 17 ; data for ref 86 should have been or , 1 of 34 ; and data for ref 61 should have read pr , 2 of 33 in patients with melanoma . vol 6 january , 2005 reection and reaction see extras / 04oncl0604webtable1.pdf november , 2004 , issue of the lancet oncology is an example of a report that fails to use rigorously standard , agreed criteria.5 these sorts of errors are most evident in webtable 1 of their review . 
 it is important that standard oncological criteria are used so that researchers can compare results and so that practicing physicians can make enlightened choices about how best to treat their patients . 
in oncology , the most commonly used criteria are those set forth by the international union against cancer and who , which dene an objective clinical response as a reduction of at least 50% in the sum of the product of perpendicular diameters of all tumours , without the growth of any tumour by more than 25% and without the appearance of any new tumours.6 another set of criteria , designated response evaluation criteria in solid tumours ( recist ) , is in many ways similar to the who criteria and designates that an objective response can be declared if there is at least a 30% reduction in the longest diameters of all target lesions . 
in the recist criteria , no target lesion can grow by 20% or more and no new lesions can appear.7 it is obvious that a clear - eyed perspective on cancer vaccines is needed if we are to make real progress . 
it is important with use of these standard criteria that responses cannot automatically be attributed to the effect of a cancer vaccine when patients are treated simultaneously with other surgery , known and effective chemotherapy , interleukin 2 , or radiotherapy . 
 symptoms and claims of benet to patients that include improvement longer - than - expected survival are subjective and generally uncontrolled.4 finally , use of surrogate endpoints such as the generation of anti - tumour t cells in vivo is of interest , but is not a substitute for tumour regression in assessment of the clinical effect of an experimental treatment . we think that progress will be made to improve cancer vaccines by the denition of ligands for toll - like receptors and of the way in which the innate and adaptive immune systems interact , as well as by the inhibition of negative regulatory signals , such as those provided by ctla4 and regulatory t cells . 
these and many other experimental approaches are being tested in preclinical and clinical trials . but perhaps cancer vaccines will be most effective when they are used in combination with adoptive cell - transferbased immunotherapeutic regimens . * nicholas p restifo , steven a rosenberg us national cancer institute , national institutes of health , bethesda , md 20892 , usa restifo@nih.gov we declare no conicts of interest . rosenberg sa , dudley me . 
cancer regression in patients with metastatic melanoma after the transfer of autologous antitumor lymphocytes . proc natl acad sci usa 2004 ; 101 ( suppl 2 ) : 1463945 . klebanoff ca , finkelstein se , surman dr , et al . 
part 1 : vaccines for solid tumours . lancet oncol 2004 ; 5 : 68189 . in webtable 1 : data for ref 29 should have been cr , 2 ; pr , 2 ; data for ref 31 should have been pr , 4 ; data for ref 79 should have been pr , 6 of 17 ; data for ref 86 should have been or , 1 of 34 ; and data for ref 61 should have read pr , 2 of 33 in patients with melanoma . vol 6 january , 2005 reflection & reaction system to deliever radiation intraoperatively . 
they describe their own low - energy orthovoltage equipment and state that a dose of 5 gy delivered to a depth of 1 cm in the tumour bed would be sufficient to destroy nonexcised , marginal cancer cells . 
for example , to reduce the amount of local recurrence in patients with early breast cancer by a factor of two , an extra dose of 16 gy to the tumour bed is needed.6 considering the physics and radiobiology , together with the infiltrative growth characteristics of breast cancer , it might be more effective to simply dissect a 1 - cm tissue margin around the tumour during surgery to obtain a similar outcome to that proposed for intraoperative radiotherapy . 
they quadrantectomy with quadrantectomy followed by whole - breast irradiation and showed a significant reduction in local recurrence by adding wholebreast irradiation to the treatment schedule . in conclusion , although some patients might benefit from intraoperative radiotherapy , at this time , we simply cannot identify who those patients are . 
and thus , intraoperative radiotherapy should not be rushed into routine clinical practice until the results of long - term endpoints in continuing clinical trials have been fully reported and appropriately assessed to ascertain the effect of intraoperative radiotherapy on local recurrence , survival , and late sideeffects . harry bartelink department of radiotherapy , netherlands cancer institute , amsterdam , netherlands . reflection & reaction system to deliever radiation intraoperatively . 
they describe their own low - energy orthovoltage equipment and state that a dose of 5 gy delivered to a depth of 1 cm in the tumour bed would be sufficient to destroy nonexcised , marginal cancer cells . 
for example , to reduce the amount of local recurrence in patients with early breast cancer by a factor of two , an extra dose of 16 gy to the tumour bed is needed.6 considering the physics and radiobiology , together with the infiltrative growth characteristics of breast cancer , it might be more effective to simply dissect a 1 - cm tissue margin around the tumour during surgery to obtain a similar outcome to that proposed for intraoperative radiotherapy . 
they quadrantectomy with quadrantectomy followed by whole - breast irradiation and showed a significant reduction in local recurrence by adding wholebreast irradiation to the treatment schedule . in conclusion , although some patients might benefit from intraoperative radiotherapy , at this time , we simply cannot identify who those patients are . 
and thus , intraoperative radiotherapy should not be rushed into routine clinical practice until the results of long - term endpoints in continuing clinical trials have been fully reported and appropriately assessed to ascertain the effect of intraoperative radiotherapy on local recurrence , survival , and late sideeffects . harry bartelink department of radiotherapy , netherlands cancer institute , amsterdam , netherlands . reflection & reaction hrpt2 and parathyroid cancer we read with interest the lancet oncologys news article entitled , vital gene linked to parathyroid carcinoma that highlighted a paper by shattuck and colleagues in the new england journal of medicine.1 , 2 the article by shattuck et al was accompanied by an editorial , 3 which clearly acknowledged an earlier publication in this field by howell and co - workers entitled , hrpt2 mutations are associated with malignancy in sporadic parathyroid tumors.4 in the linked - editorial , weinstein and simonds clearly refer to the study of howell et al : another recent study identified similar mutations in four of four tumours from patients with parathyroid carcinoma , but not in parathyroid adenomas , suggesting that such mutations are markers of cancer . 
while shattuck et al only screened parathyroid carcinomas for hrpt2 mutations , howell colleagues carried out a more extensive screening programme for hrpt2 in : benign parathyroid mutations lesions ( 25 sporadic adenomas , two lithium - associated tumours , 11 secondary , and six tertiary hyperplastic glands ) ; familial parathyroid tumours ( three with familial isolated hyperparathroidism , five with hyperparathyroidism jaw tumour syndrome , three with multiple endocrine neoplasia type 1 , and one with multiple endocrine neoplasia type 2 ) ; and sporadic parathyroid carcinomas . 
 in their series , howell and coworkers found the hrpt2 mutation was specific to the sporadic parathyroid cancer subtype ( in addition to the germline hrpt2 mutations already reported in a subset of families with hyperparathyroidism jaw tumour syndrome5 )  . 
shattuck et al were unable to draw this conclusion in their study because they did not include sporadic benign parathyroid tumours . in summary , prior to shattuck et al , howell and colleagues had clearly established the presence of a somatic hrpt2 mutation in sporadic parathyroid carcinoma . 
additionally , howell et al have previously shown that somatic hrpt2 mutations are specific to the carcinoma subtype in sporadic neoplastic parathyroid disease , with the exception of somatic hrpt2 mutation in 4% of sporadic adenomas with cystic features.5 deborah j marsh * , hans morreau , and bin t teh * kolling institute of medical research , royal north shore hospital , sydney , nsw , australia and department of molecular medicine , university of sydney , sydney , nsw , australia , department of pathology , leiden university medical center , leiden , netherlands , laboratory of cancer genetics , van andel research institute , grand rapids , mi , usa . aacr cancels annual meeting because of sars cases people have died from the disease , and there have been 111 probable and 95 suspected in ontario . 
 newsdesk the american association for cancer research cancelled its annual meeting 3 days before it was due to begin in toronto , canada ( april 59 , 2003 ) because of recent outbreak of severe acute respiratory syndrome ( sars )  . countrys the cancelling the meeting was a difficult decision to make , says the organisations chief executive officer margaret foti ( philadelphia , pa , usa )  . the aacr received 6900 abstracts , booked 400 speakers , and expected about 16 000 participants to attend the meeting , foti explains . 
ten torontos medical officer of health , sheela basrur , wrote a letter to the aacr emphasising the precautions that health - care providers should take while attending the meeting but did not advise the organisation to cancel the conference , says a spokesperson from toronto public health . 
however , we were still says foti . receiving cancellations , some cancer centres were advising their staff not to attend because of concerns about travelling to countries affected by sars and the potential transmission of the disease from health - care professionals to their immunocompromised patients with cancer , she explains . 
 the aacr contacted the world health organization , the us centers for disease control and prevention ( cdc ) , and toronto health officials , all of whom noted that there is not concern currently widespread transmission of sars to the community in toronto . 
 about india cuts budget for cancer treatment the indian government has cut financial support for cancer research and treatment , despite the country facing the massive challenge of nearly one million new cancer cases every year . 
in the central governments annual budget for 20032004 , allocation for the national cancer control programme ( nccp ) has been reduced to rs 520 million from rs 580 million . 
the nccp official approached by the lancet oncology preferred to remain anonymous but did say that the cut may be due to the fact that we were not able to absorb all the funds allotted to us in the past . jyotsna govil of the indian cancer society remarks : this is a prime example of tokenism in matters of health . the allocation has been so meagre that a state like delhi receives as little as rs15 million per annum for hospitals run by the local administration . 
govil points out that it is obvious the government has little use for a cancer education and prevention programme , despite every medical authority saying the incidence can be cut by 70% with screening and awareness programmes . experts say india needs rational budgeting for cancer programmes . 
at present , patients presenting with latestage disease , because of lack of awareness , prove to be a financial burden as scarce resources are used in their treatment without much outcome in terms of long - term survival . in addition to awareness and early detection , we need to spend money on treatment facilities to do away with lists . 
only reproduce with permission from the lancet publishing group . smoking and lung cancer review randomized trial of vitamin a and n - acetylcysteine in patients with head and neck cancer or lung cancer . 
dose - response study of myo - inositol as an inhibitor of lung tumorigenesis induced in a / j mice by benzo [ a ] pyrene and 4 - ( methylnitrosamino ) - 1 ( 3 - pyridyl ) - 1 - butane . 
anticarcinogenic activities of organic isothiocyanates : chemistry and mechaniscancer res 1994 ; 54 ( suppl ) : 1976s81s . 64 sticha krk , staretz me , wang m , et al . 
effects of benzyl isothiocyanate and phenethyl isothiocyanate on benzyl [ a ] pyrene metabolism and dna adduct formation in the a / j mouse . carcinogenesis 2000 ; 21 : 171119 . 65 chen yr , wang w , kong ant , tan th . 
effects of phenethyl isothiocyanate and benzyl isothiocyanate , individually and in combination , on lung tumorigenesis induced in a / j mice by benzo [ a ] pyrene and 4 - ( methylnitrosamino ) - 1 - ( 3 - pyridyl ) - 1butanone . 
chemopreventive effects of myoinositol and dexamethasone on benzo [ a ] pyrene and 4 - ( methylnitrosamino ) - 1 - ( 3 - pyridyl ) - 1 - butanone - induced pulmonary carcinogenesis in female a / j mice . 
 honest patient - orientated information on survival for different types of cancer and options for palliative care must be made widely available to choices , ensure according it also demands the development of practice guidelines and standards with followup research to assess their effects . 
at a top policy level , the nci is urged to state - of - the - science convene meeting , include palliative care among its members , and to fund a high - profile research agenda to examine the quality of care , in addition for cures . searching specialist leadership of the nci should promote excellence and help produce the best possible practice guidelines . such guidance could help achieve a paradigm that patients palliative - care needs are assessed early in the course of their disease , while they are undergoing treatment , rather than waiting until death is very near . 
in the uk , increasing integration of hospices the national health service with ( nhs ) have continuity of good palliative care throughout the course of their disease . education and research in palliative techniques and psychosocial support now occur in several units in the uk . but charities cannot expect nhs funding to be standardised across the uk without the parameters of service provision being defined . 
the death in america project should be mirrored in europe , research and identifying more beacons of good practice . irene j higginson * and ilora g finlay facilitating * department of palliative care and policy , kings college london , weston education centre , cutcombe road , london , se5 9rj , uk . 
university of wales college of medicine section of oncology and palliative medicine , velindre hospital , whitchurch , cardiff , cf14 2tl . 1 esteve j , kricker a , ferlay j , parkin dm ( eds )  . 
facts and figures of cancer in the european community international agency for research on cancer commission of the european communities world health organization europe against cancer , 1993 . 2 foley km , gelband h . 
 3 lynn j , teno jm , phillips rs , et al . perceptions by family members of the dying experience of older and seriously ill patients : support investigators study to understand prognoses and preferences for outcomes and risks of treatments . 
 j clin oncol 2001 ; 19 : 20512 . erratum antisense therapy for cancerthe time of truth by burkhard jansen and uwe zangemeister - wittke . lancet oncol 2002 ; 3 : 67283 . the second paragraph on page 677 following the citation for figure 5 inferred that all patients survived beyond 1 year . 
only reproduce with permission from the lancet publishing group . reflection & reaction hrpt2 and parathyroid cancer we read with interest the lancet oncologys news article entitled , vital gene linked to parathyroid carcinoma that highlighted a paper by shattuck and colleagues in the new england journal of medicine.1 , 2 the article by shattuck et al was accompanied by an editorial , 3 which clearly acknowledged an earlier publication in this field by howell and co - workers entitled , hrpt2 mutations are associated with malignancy in sporadic parathyroid tumors.4 in the linked - editorial , weinstein and simonds clearly refer to the study of howell et al : another recent study identified similar mutations in four of four tumours from patients with parathyroid carcinoma , but not in parathyroid adenomas , suggesting that such mutations are markers of cancer . 
while shattuck et al only screened parathyroid carcinomas for hrpt2 mutations , howell colleagues carried out a more extensive screening programme for hrpt2 in : benign parathyroid mutations lesions ( 25 sporadic adenomas , two lithium - associated tumours , 11 secondary , and six tertiary hyperplastic glands ) ; familial parathyroid tumours ( three with familial isolated hyperparathroidism , five with hyperparathyroidism jaw tumour syndrome , three with multiple endocrine neoplasia type 1 , and one with multiple endocrine neoplasia type 2 ) ; and sporadic parathyroid carcinomas . 
 in their series , howell and coworkers found the hrpt2 mutation was specific to the sporadic parathyroid cancer subtype ( in addition to the germline hrpt2 mutations already reported in a subset of families with hyperparathyroidism jaw tumour syndrome5 )  . 
shattuck et al were unable to draw this conclusion in their study because they did not include sporadic benign parathyroid tumours . in summary , prior to shattuck et al , howell and colleagues had clearly established the presence of a somatic hrpt2 mutation in sporadic parathyroid carcinoma . 
additionally , howell et al have previously shown that somatic hrpt2 mutations are specific to the carcinoma subtype in sporadic neoplastic parathyroid disease , with the exception of somatic hrpt2 mutation in 4% of sporadic adenomas with cystic features.5 deborah j marsh * , hans morreau , and bin t teh * kolling institute of medical research , royal north shore hospital , sydney , nsw , australia and department of molecular medicine , university of sydney , sydney , nsw , australia , department of pathology , leiden university medical center , leiden , netherlands , laboratory of cancer genetics , van andel research institute , grand rapids , mi , usa . reflection & reaction is a possibility of breast cancer as a result of smoking and that the risk is higher in those women who start to smoke while teenagers . 
 pankaj chaturvedi department of surgery , tata memorial hospital , mumbai , india . reection and reaction management of chemotherapy - induced side - effects ( 5 - ht3 ) antagonist developments summary of in their review , sharma and colleagues1 provided an excellent chemotherapy - induced nausea , management of vomiting , mucositis , and diarrhoeacommon sources of psychological and physical distress in patients with cancer . 
an important addition to this list is mirtazapine , a 5 - ht3 receptor antagonist , which has proven to be an effective antiemetic agent.26 specically , mirtazapine has been associated with relief of nausea , vomiting , and other common comorbidities related to cancer chemotherapy and radiotherapy.25 as well as having antiemetic effects , mirtazapine is also effective in treatment of depressive symptoms , pain , anorexia , anxiety , and insomnia comorbidities that are common in patients with cancer and have been linked to poor quality of life and compliance with treatment.25 , 7 receptors , opiate - like mirtazapine enhances noradrenergic and serotonergic neurotransmission via its antagonism of 5 - ht3 and central presynaptic ( cid : 2 ) 2 adrenergic enhanced agonism at the 5 - ht1 receptor , and its activities.810 possible important drawbacks of mirtazapine are the absence of induction of sedation at low doses . 
other sideeffects include constipation and weight ga intravenous formulation , and antinociceptive its because of its salutary effects on common cancerrelated complications , mirtazapine , as part of an antiemetic treatment regimen , might decrease the need for additional drugs for these complications , potentially leading to fewer adverse drugdrug interactions , lower costs , and improved overall quality of life for these patients . 
a large , controlled , clinically comparative trial of mirtazapine and other 5 - ht3 receptor antagonists could help dene the optimum and most cost - effective therapeutic regimen for nausea and vomiting in patients with cancer who are undergoing treatment . 
 mukaila a raji outpatient geriatrics clinics , sealy center on aging , department of internal medicine , university of texas medical branch , 301 university boulevard , galveston , tx , usa muraji@utmb.edu i declare no conicts of interest . sharma r , tobin p , clarke sj . 
lancet oncol 2005 ; 6 : 138the news in brief story , oestrogen and lung - cancer survival , should read : the investigators used getinib to block the epidermal - growthfactor - receptor pathway and fulvestrant to block the oestrogen pathway in mice with grafter lung tumours . polychronis a , sinnett hd , hadjiminas d , et al . 
preoperative getinib versus getinib and anastrozole in postmenopausal patients with oestrogen - receptor positive and epidermal - growth - factorreceptor - positive primary breast cancer : a double - blind placebocontrolled phase ii randomised trial . 
patients preferences for adjuvant chemotherapy in early stage breast cancer : is treatment available ? br j cancer 2001 ; 84 : 155785 . palda va , llewellyn - thomas ha , mackenzie rg , et al . 
clin therap 1998 ; 20 : c2025 . 14 cruzan v director , missouri department of health , 497 vs 261 : 1990 . errata migliorati ca , siegel ma , elting ls . 
in this personal view , the fth sentence of the second paragraph in the future directions section ( p 512 ) should have read : yet , in bisphosphonate - associated osteonecrosis , the maxilla is a ected much more than it is in osteoradionecrosis , suggesting occurrence of a di erent form of vascular pathogenesis or other mechanism . sobrero a , khne c - h . 
in this debate , the fourth sentence of the last paragraph in the argument for the proposal ( p 516 ) should have read : however , these data also mean that in patients who will probably relapse with no adjuvant treatment , one in ve will not relapse with uorouracil and leucovorin and one in three will not relapse with adjuvant folfox . azizi aa , haberler c , czech t , et al . 
in this case report , the rst sentence of the fth paragraph ( p 522 ) should have read : restaging in october , 2004 , revealed progression of the 15 known lesions as well as 12 new pulmonary lesions ( gure 2a , c )  . vol 7 july 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com re ection and reaction parameters and does not incorporate non - carcinoma variables , such as concomitant illnesses , which could also a ect patient outcome.2 however , in the midst of such uncertainty , fuzzy logic could have an important role in the decision - making process . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
in this review , the labelling of the four histological images in gure 2 should have been ( from left to right ) : dfsp , dsrct , mfh , and leio . 670 vol 8 august 2007 re ection and reaction panel : ten principles for a bill of rights for patients with cancer all patients , irrespective of domicile , have a right of access to : 1 high - quality , patient - focused cancer services that are commissioned , accredited , and monitored according to national standards 2 optimum cancer care , based on clinical needs and irrespective of means within the resources available 3 management by a multidisciplinary team of accredited cancer professionals in an environment of patientfriendly care 4 timely and sensitively delivered care according to national standards 5 evidence - based diagnostic treatment and supportive care that meet national standards at a location as close to place of domicile as is clinically appropriate 6 provision and maintenance of high - quality cancer registration , clinical notes , and clinical outcome data 7 equitable access to new developments in diagnosis and treatment 8 comprehensive information about treatment options 9 information about the compliance with quality standards of the commissioning and delivery of cancer services relating to the cancer network in which they are managed 10 right of redress if provision of care falls below national standards was adopted , alternative co - payment schemes and health insurance ( advocated by some commentators ) , 6 might also need to be considered to meet public expectation of cancer care as nhs investment falls beyond 2008 . how can the continued improvements in cancer services be sustained in the long - term , despite nhs reforms and changes in government and funding mechanisms ? one possibility would be a bill of rights for patients with cancer ( panel ) , which could apply to patients managed in either state or private sectors ( or both )  . 
since public support for cancer as a nhs priority is greater than that for any other disease , it is likely that such a bill would be supported by the electorate . 
the times ( london ) , april 4 , 2006 : 18 . erratum steven a narod , jan lubinski , parviz ghadirian , et al , for the hereditary breast cancer clinical study group . 
in this article , the authors surname domcheck should have been spelt domchek throughout . and their bene ts and risks i declare no con icts of interest . vol 7 june 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology re ection and reaction parameters and does not incorporate non - carcinoma variables , such as concomitant illnesses , which could also a ect patient outcome.2 however , in the midst of such uncertainty , fuzzy logic could have an important role in the decision - making process . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
in this review , the labelling of the four histological images in gure 2 should have been ( from left to right ) : dfsp , dsrct , mfh , and leio . 670 vol 8 august 2007 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com unfortunately , this benet will not be realised from meta - analyses because of the absence of stage stratication in existing studies . 
we agree that the use of endoluminal ultrasonography and possibly pet should be a requirement to stratify patients in future randomised trials of preoperative treatment oesophageal cancer . * bryan h burmeister , b mark smithers university of queensland , princess alexandra hospital , brisbane , 4102 , australia bryan_burmeister@health.qld.gov.au i declare no conicts of interest . burmeister bh , smithers bm , gebski v , et al . 
a step too far ? lancet oncol 2005 ; 6 : 731the rst sentence should have read on sept 13 , 2005 , the scottish medicines consortium ( smc ) approved anastrozole for postmenopausal women with early - stage invasive breast cancer . vol 6 november 2005 re ection and reaction moreover , our in - vitro calibrations suggested that at the high cell burdens often seen in cll , it was likely that , as a consequence of treatment with the usual dose of rituximab ( 375 mg / m2 , once a week for 4 weeks ) , complement would be consumed substantially , and complement - dependent cytotoxicity could be abrogated , thus compromising the e ectiveness of the treatment . 
we reported that complement was depleted for up to several weeks in several patients with cll as a consequence of rituximab treatment , thus leading us to propose that use of fresh frozen plasma could enhance the therapeutic action of rituximab in cll . 
 finally , use of large amounts of rituximab at these high cell burdens saturates a second e ector - cell mechanism that is important in the action of rituximabie , fcrmediated clearance of cll cells . 
this e ect leads to a second event in which almost all cd20 is removed ( shaved ) from the targeted cells , further compromising the treatment.2 , 6 the cd20 concentrations of the patient reported by klep sh and co - workers would have been interesting to follow to establish whether supplemental complement can modulate the shaving reaction . ronald taylor university of virginia school of medicine , charlottesville , va , usa rpt@virginia.edu the author declared no con icts of interest 1 . 
j immunol 2006 ; 177 : 743543 . paediatric oncology : a call for papers if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology submitted via the lancet oncologys online submission service , and all authors must clearly state in the covering letter that their submission is in response to the paediatric oncology call for papers . 
please note that the deadline for submission is may 21 , 2007 . to submit a paper , clearly marked with the phrase paediatric oncology call for papers , go to thelancetoncology cancer a ects about 1 in 500 children under 15 years of age.1 although great strides have been made in the treatment of paediatric cancer over the past few decades , in the uk about 20% of all deaths in children aged 1 to 14 years are still caused by cancer.1 the lancet oncology is therefore issuing a call for papers that address paediatric cancer . 
accepted papers will be published in the lancet oncology to coincide with the international society of paediatric oncology ( siop ) annual congress ( mumbai , india ; nov 13 , 2007 )  . 
if your submission describes , in part or wholly , a study accepted for presentation at the siop annual congress , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication in the lancet oncology can be scheduled to comply with siops embargo policies . 
articles should be lidia siemaszkiewicz the lancet oncology , london nw1 7by , uk charles stiller ( childhood cancer research group ) , mike quinn , steve rowan ( o ce for national statistics )  . 
the third sentence of the fourth paragraph should have read : alvin eisner ( oregon health & science university , portland , or , usa ) , whose group has recently shown that anastrozole does not produce the neurological changes detectable in the eyes of women who have received tamoxifen ( breast cancer res treat published online jan 27 , 2007 ; doi : 10.1007 / s10549 - 006 - 9486 - 3 ) does think , nevertheless , that further studies need to be done to compare side e ect pro les . vol 8 may 2007 reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com re ection and reaction debate . 
patients preferences for adjuvant chemotherapy in early stage breast cancer : is treatment available ? br j cancer 2001 ; 84 : 155785 . palda va , llewellyn - thomas ha , mackenzie rg , et al . 
clin therap 1998 ; 20 : c2025 . 14 cruzan v director , missouri department of health , 497 vs 261 : 1990 . errata migliorati ca , siegel ma , elting ls . 
in this personal view , the fth sentence of the second paragraph in the future directions section ( p 512 ) should have read : yet , in bisphosphonate - associated osteonecrosis , the maxilla is a ected much more than it is in osteoradionecrosis , suggesting occurrence of a di erent form of vascular pathogenesis or other mechanism . sobrero a , khne c - h . 
in this debate , the fourth sentence of the last paragraph in the argument for the proposal ( p 516 ) should have read : however , these data also mean that in patients who will probably relapse with no adjuvant treatment , one in ve will not relapse with uorouracil and leucovorin and one in three will not relapse with adjuvant folfox . azizi aa , haberler c , czech t , et al . 
we aimed to assess whether exposure to ionising radiation through mammography screening was associated with risk of breast cancer in brca1 or brca2 mutation carriers . methods we identi ed 1600 cases of breast cancer and 1600 controls without breast cancer who were matched for brca mutation , date of birth ( within 1 year ) , and country of residence from an international registry of brca1 and brca2 mutation carriers . 
 results we found no association between ever having screening mammography and risk of breast cancer ( odds ratio [ or ] 103 [ 95% ci 085125 ] , adjusted for parity , oral - contraceptive use , ethnic origin , and bilateral oophorectomy )  . 
 the association was much the same for brca1 mutation carriers and brca2 mutation carriers ( 104 [ 084129 ] vs 106 [ 067166 ] , respectively , adjusted for parity , oral - contraceptive use , ethnic origin , and bilateral oophorectomy )  . interpretation these ndings do not lend support to the idea that exposure to ionising radiation through routine screening mammography contributes substantially to the burden of breast cancer in brca1 and brca2 mutation carriers . 
prospective studies are needed to con rm the results of this initial report , and , where possible , these studies should assess a more appropriate endpoint of total exposure . introduction women with a germline mutation in brca1 or brca2 have increased risks of developing breast and ovarian cancer . 
because the risk of breast cancer rises substantially from age 25 years and peaks between age 3050 years , some researchers1 , 2 recommended that screening should start early ( ie , at age 25 years )  . 
current methods of screening for breast cancer include mammography , ultrasonography , clinical examination , and mri.3 at present , mammography is the most widely used imaging modality . screening mammography is associated with a small dose of radiation to the breast . 
this dose is not thought to be high enough to increase the risk of breast cancer in the general population , but women who are at increased genetic risk might be particularly sensitive to the dnadamaging e ects of ionising radiation.46 hereditary breast cancer typically occurs at a young age ( ie , women in their thrities and forties ) , and brca1 and brca2 have a role in the repair of dna damage.7 , 8 these two proteins help repair double - strand dna breaks , which are characteristic of lesions induced by ionising radiation . 
radiation is an established risk factor for early - onset breast cancer in the general population , 911 although exposure levels associated with this risk are many times greater than that associated with screening mammography . 
we aimed to assess whether screening mammography was associated with risk of breast cancer in brca1 and brca2 mutation carriers . methods participants women with a brca1 or brca2 mutation were identi ed through a registry of mutation carriers , which was located at the centre for research on womens health , university of toronto , ontario , canada . 
data for these women were gathered from women with known pathogenic brca1 and brca2 mutations during genetic counselling and mutation testing at 44 centres in six countries in north america , europe , and israel . 
when a mutation in brca1 or brca2 was found in a proband or in her relative , genetic testing was o ered to other at - risk women in her family . 
mutations were identi ed by use of various techniques during the course of genetic testing , but all 402 vol 7 may 2006 articles abnormal nucleotide sequences were con rmed by direct sequencing of dna . 
 from april 26 1992 , to july 12 2005 , data were submitted to the registry for 4951 women with a brca1 or brca2 mutation and with information on history of mammography , including age at rst mammography . 
41 women were excluded because they were diagnosed with ovarian cancer or any other cancer before diagnosis with breast cancer ; 165 women were excluded because they had had three women were prophylactic mastectomy ; and excluded because of missing data for important variables . 
 after exclusions , there were 4742 eligible brca mutation carriers2181 women with breast cancer ( ie , cases ) and 2561 women without breast cancer ( ie , con trols )  . 
cases and controls were matched for date of birth ( within 1 year ) , brca mutation ( brca1 vs brca2 ) , and country of residence ; matching was done by ps using a computer prograthe control could not have been diagnosed with any cancer before the age of diagnosis of breast cancer for the case . 
for this study , questionnaires were excluded if age at breast - cancer diagnosis or age at rst mammography were missing . the questionnaire inquired about whether participants had ever had screening mammography , and , if so , the age at which they rst had the procedure ; and about the total number of mammography procedures they had had in their lifetime ( ie , until the date of questionnaire completion )  . 
because of the di culty in distinguishing between screening mammography and diagnostic mammography for cases , we restricted our analyses to the rst mammography that took place at least 1 year before the year of diagnosis of breast cancerie , a mammography procedure was excluded from analyses if it was reported to have occurred in the same calendar year as breast - cancer diagnosis or in the year before breast - cancer diagnosis . 
information on cancer diagnoses were obtained from the questionnaire . information for family history was derived from pedigrees , which were drawn by research personnel at every centre ; pedigrees were sent to the study centre in toronto with , but separate from , questionnaires . 
 statistical analyses we analysed age at rst mammography for every case and matched control by classifying women into three age - groups : 30 years or younger ; 3140 years ; and 41 years age ( years ) median ( range ) year of birth year ( range ) mutation brca1 brca2 parity mean ( sd ) nulliparous oral contraceptives bilateral oophorectomy country of residence ever use ever usa canada poland norway israel austria ethnic origin jewish french - canadian other white other controls ( n = 1600 ) cases ( n = 1600 ) 467 ( 214832 ) 473 ( 189826 ) 011 * 1953 ( 19151981 ) 1953 ( 19151980 ) matched 1260 ( 79% ) 340 ( 21% ) 20 ( 14 ) 288 ( 18% ) 1260 ( 79% ) 340 ( 21% ) 20 ( 13 ) 249 ( 16% ) 945 ( 59% ) 941 ( 59% ) 76 ( 5% ) 51 ( 3% ) 520 ( 33% ) 474 ( 30% ) 461 ( 29% ) 71 ( 4% ) 50 ( 3% ) 24 ( 2% ) 330 ( 21% ) 128 ( 8% ) 1119 ( 70% ) 23 ( 1% ) 520 ( 33% ) 474 ( 30% ) 461 ( 29% ) 71 ( 4% ) 50 ( 3% ) 24 ( 2% ) 271 ( 17% ) 145 ( 9% ) 1144 ( 72% ) 40 ( 3% ) matched 03 * 007 09 002 matched 001 family history of breast cancer one or more rst - degree relatives with breast cancer 803 ( 59% ) 764 ( 57% ) || 037 data are number ( % ) , unless otherwise stated ; data might not add to 100% because of rounding . 
 * adjusted for parity , oral - contraceptive use , bilateral oophorectomy , and ethnic orig table 2 : association between age of rst mammography and risk of breast cancer for all women and by brca mutation , age at breast - cancer diagnosis , and cancer not identi ed by mammography or older . 
because ionising radiation is thought to be a risk factor for early - onset breast cancer in particular , analyses were repeated after strati cation of cases by age of diagnosis ( 40 years vs > 40 years )  . 
furthermore , because the intensity of screening mammography might a ect the age of breast - cancer diagnosis ( ie , women who have regular screening might have breast cancer diagnosed earlier than women who do not participate in a screening programme ) , we did a subgroup analysis of cases with breast cancer diagnosed by procedures other than mammographyie , by self - examination or physician examination . 
 role of the funding source the sponsor of this study had no role in the study design ; in the collection , analysis , or interpretation of the data ; or in the writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results table 1 shows the characteristics of the 1600 cases and 1600 matched controls . 
controls were signi cantly more likely to have had bilateral oophorectomy than were cases , but only 127 ( 4% ) of all participants had had a bilateral oophorectomy before the age of breast - cancer diagnosed in the case . 
we did not receive a pedigree for all participants for whom a questionnaire was available : detailed family history was available for 2706 ( 85% ) participants : 1367 ( 85% ) cases and 1339 ( 84% ) controls . 
 the mean age of breast - cancer diagnosis in cases was 405 years ( 81 ) for brca1 mutation carriers and 418 years ( 80 ) for brca2 mutation carriers . 
199 ( 12% ) cases were diagnosed by screening mammography , and 1281 ( 80% ) were diagnosed by other procedures ( usually palpation of a mass by physician or self - examination ) ; 120 ( 8% ) cases did not have information for method of diagnosis because of missing data or diagnosis by more than one method . 
 more brca2 mutation carriers were diagnosed by 404 vol 7 may 2006 articles mammo graphy compared with brca1 mutation carriers ( 77 [ 23% ] of 340 vs 122 [ 10% ] of 1260 , p < 00001 )  . 661 ( 41% ) cases and 729 ( 46% ) controls had at least one screening mammography procedure 1 year or more before the calendar year in which the case was diagnosed . 
 mean age at rst screening mammography was 353 years ( sd 78 ) for cases and 355 years ( 80 ) for controls ( p = 070 , t test )  . 
201 ( 13% ) cases and 234 ( 15% ) controls rst had mammography at age 30 years or younger ; 342 ( 21% ) cases and 355 ( 22% ) controls rst had mammography at age 3140 years ; and 118 ( 7% ) cases and 140 ( 9% ) controls rst had a mammography at age 41 years or older . 
for 760 ( 48% ) of the 1600 matched pairs , the case had her rst mammography at a younger age than the control ; for 706 ( 44% ) matched pairs , the control had her rst mammography at a younger age than the case ( p = 016 , t test ) ; and for 134 ( 8% ) matched pairs , the case and control had the same age at rst mammography or neither had mammography . after rst mammography , controls had a mean of 64 mammography procedures ( sd 038 ) every 10 years . 
 the frequency of mammography was much the same for controls who initiated the procedure in their thirties ( mean 67 [ 037 ] every 10 years ) and those who initiated it in their forties ( 68 mammograms [ 038 ] every 10 years )  . table 2 shows the association between age at rst mammography and risk of breast cancer for all women and for subgroups . 
the associations were much the same for subgroups with brca1 and brca2 mutations , and for those who were diagnosed at age 40 years or younger and at older than 40 years ( table 2 )  . 
 initiation of mammography in the thirties was associated with diagnosis of breast cancer at age 40 years or younger ( table 2 ) , but no association was noted for earlier initiation of mammography ( ie , at age 30 years , table 2 )  . 
subgroup analysis that excluded the 199 cases and their matched controls who had breast cancer identi ed by mammography showed no association between mammography and risk of breast cancer for women who had a breastcancer diagnosis by methods other than that of mammography . 
subgroup analysis showed that initiation of mammog raphy at age 3140 years was associated with an increased risk of breast - cancer diagnosis before age 40 years ; however , this nding might be due to chance . 
 we did a large study of 1600 matched pairs , and , on the basis of the 95% ci , were able to exclude an overall increase in risk associated with ever having mammography of higher than 125 . 
nevertheless , the numbers of women in some subgroups were small , and for women diagnosed with breast cancer before age 40 years , we could not exclude an increase in risk of 155 . we questioned cases and controls on the total number of mammography procedures they had had until the date of questionnaire completion , but we did not record the date of every mammography , only the rst procedure . 
however , in the absence of a comprehensive review of medical records , desticntion between diagnostic mammography ( ie , that initiated in response to an abnormal breast nding ) and screening mammography ( ie , that done only for the purpose of screening ) can be di cult . 
in the study reported here , we excluded all mammography that took place in the same calendar year as diagnosis of breast cancer in cases and controls and those done in the previous year to avoid any potential misclassi cation of screening and diagnostic mammography . 
although a young woman might have mammography only for assessment of a suspicious mass ( eg , a cyst ) , and thus the procedure might not be an indicator of long - term screening behaviour , we expect that such women will be a minority . 
in our study , the mean frequency of this for controls was mammography recommendationone mammography procedure every 19 months , or about 13 mammography procedures over a surveillance period of 20 years . than less a case - control study such as that reported here would be di cult to do in the general population because women at high risk of cancer are more likely to participate in a screening programme than are women at average risk or low risk . 
such selection bias would probably be a particular problem for assess ment of the e ect of early - onset mammography , which is generally recommended only for women at high risk of breast cancer . 
by contrast , self - selection for screening by inherent risk level is probably less important for mutation carriers because the main vol 7 may 2006 articles if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology determinant of risk is the mutation . 
furthermore , self - selection to have early mammography by women with a strong family history of breast cancer would lead to a spurious positive association between mammography exposure and breast - cancer risk , and not to the null nding that we recorded . the possibility of recall bias must be assessed in a casecontrol study . 
 women who have regular screening might be more likely to be diagnosed with breast cancer than unscreened women as a result of intensi ed surveillancea situation that would result in an excess of breast cancer identi ed by screening in the women under close surveillance . 
 therefore , we repeated our analysis on women who did not have cancer identi ed by mammography , and found that these women were not at increased risk of breast cancer . 
furthermore , only 199 ( 12% ) of the 1600 cases reported that the breast cancer was diagnosed as a result of breast - cancer screening . we planned this study on the premise that radiation exposure from a screening mammography might be su cient to raise the cancer risk in women with genetic susceptibility to the disease . 
on the basis of the similarities of radiation - induced breast cancer and hereditary breast cancer , we have previously raised caution that such screening might be hazardous.6 our ndings reported here do not lend support to the idea that brca1 or brca2 mutation carriers are at increased risk of breast cancer after exposure to mammography . 
 other studies12 , 13 of the e ects of radiation exposure in brca carriers have been negativeie , they reported12 , 13 no increase in the risk of second primary ipsilateral or contralateral breast cancer associated with radiotherapy as treatment for a rst breast cancer . 
our data should be reassuring to women and their physicians , and suggest that mammography is not a risk factor for breast cancer in carriers of brca1 or brca2 mutations . 
the decision of whether to o er mammography screening to high - risk women should be based rst on an assessment of the sensitivity of the screening tool and the potential bene ts of early detection in this high - risk group . 
we thank anna tulman and nicole phillips ( centre for research on womens health , university of toronto , ontario , canada ) for data management . con icts of interest we declare no con icts of interest . other members of the hereditary breast cancer clinical study group austriat wagner . canadap ainsworth , a chudley , a eisen , d gilchrist , e lemire , d provencher , w meschino , e warner . israelr gershoni - baruch , e friedman , g rennert . 
 italyb pasini , c bellati . usaf couch , m daly , c eng , d fishman , b karlan , j mclennan , w mckinnon , s merajver , s neuhausen , b pasche , o olopade , m osborne , k sweet , h saal , n tung , j weitzel , m wood . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology article appearing in the lancet oncology . 
in this article , the co - author magdalena b lasota should have been written as magdalena bielska - lasota . 868 vol 8 october 2007 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com unfortunately , this benet will not be realised from meta - analyses because of the absence of stage stratication in existing studies . 
we agree that the use of endoluminal ultrasonography and possibly pet should be a requirement to stratify patients in future randomised trials of preoperative treatment oesophageal cancer . * bryan h burmeister , b mark smithers university of queensland , princess alexandra hospital , brisbane , 4102 , australia bryan_burmeister@health.qld.gov.au i declare no conicts of interest . burmeister bh , smithers bm , gebski v , et al . 
a step too far ? lancet oncol 2005 ; 6 : 731the rst sentence should have read on sept 13 , 2005 , the scottish medicines consortium ( smc ) approved anastrozole for postmenopausal women with early - stage invasive breast cancer . vol 6 november 2005 reection and reaction information , how will individuals who give broad and future consent know that ethics review boards only approved research that met the conditions of this consent approach ? will an independent organisation be in place to ensure that the conditions are met ? for example , national legislation in estonia for the estonian genome project requires that a governing board be established to monitor the biobanks activities ; an independent national ethics committee provides general ethical oversight of the biobank.5 in the uk , the ethics and governance council , which is independent structurally and nancially from the uk biobank , has been established to ensure that the biobanks activities , protocol , and procedures comply with the projects ethics governance framework.5 both these projects require individuals to give blanket consent for future use of their biobank samples . the condentiality of personal legitimacy of alternative - consent approaches hinges on the adequacy of governance mechanisms to information , protect facilitate withdrawal of consent , and ensure that ethics review boards full their obligation to approve only studies that meet the conditions of these models . accountability , transparency , and proper monitoring are crucial to maintain public trust in biobank research , 5 especially individuals give consent for future research with their biobank samples before an ethics review board has approved specic studies . 
whether oversight mechanisms such as those for the estonian genome project and the uk biobank will ensure that alternative consent approaches do not undermine public trust in biobank research or render the principle of informed consent meaningless remains to be seen . karen j maschke the hastings center , 21 malcolm gordon road , garrison , new york , ny 10524 - 5555 , usa maschkek@thehastingscenter.org i declare no conicts of interest . hansson mg , dillner j , bartram cr , et al . 
research involving human biological materials : ethical issues and policy guidance , vol 1 : report and recommendations of the national bioethics advisory commission . rockville , md : national bioethics advisory commission , 1999 . 
protracted remission of metastatic epithelioid angiosarcoma with weekly infusion of doxorubicin , paclitaxel , and cisplatlancet oncol 2006 ; 7 : 9293the third paragraph should have read : the patient began hormone - ablative treatment with a monthly injection of 75 mg leuporelin intramuscularly for 3 months . al - terkait f , charalambous h . 
lancet oncol 2006 ; 7 : 188the third line should have read : resection of low anterior rectal cancer . if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com vol 7 march 2006 re ection and reaction panel : ten principles for a bill of rights for patients with cancer all patients , irrespective of domicile , have a right of access to : 1 high - quality , patient - focused cancer services that are commissioned , accredited , and monitored according to national standards 2 optimum cancer care , based on clinical needs and irrespective of means within the resources available 3 management by a multidisciplinary team of accredited cancer professionals in an environment of patientfriendly care 4 timely and sensitively delivered care according to national standards 5 evidence - based diagnostic treatment and supportive care that meet national standards at a location as close to place of domicile as is clinically appropriate 6 provision and maintenance of high - quality cancer registration , clinical notes , and clinical outcome data 7 equitable access to new developments in diagnosis and treatment 8 comprehensive information about treatment options 9 information about the compliance with quality standards of the commissioning and delivery of cancer services relating to the cancer network in which they are managed 10 right of redress if provision of care falls below national standards was adopted , alternative co - payment schemes and health insurance ( advocated by some commentators ) , 6 might also need to be considered to meet public expectation of cancer care as nhs investment falls beyond 2008 . how can the continued improvements in cancer services be sustained in the long - term , despite nhs reforms and changes in government and funding mechanisms ? one possibility would be a bill of rights for patients with cancer ( panel ) , which could apply to patients managed in either state or private sectors ( or both )  . 
since public support for cancer as a nhs priority is greater than that for any other disease , it is likely that such a bill would be supported by the electorate . 
the times ( london ) , april 4 , 2006 : 18 . erratum steven a narod , jan lubinski , parviz ghadirian , et al , for the hereditary breast cancer clinical study group . 
 for example , the poster competition alone has resulted in nearly 100 submissions from 22 di erent countries , 74% of which report on research being done by groups in asia . 
furthermore , by drawing on the knowledge of a faculty of over 40 world - renowned speakers , the forum will focus on the ten most prevalent cancers in the asiapaci c region and will examine aspects of prevention , diagnosis , treatment , and palliation . 
opinion - leaders will discuss cancer aetiology , health - care systems , and the challenges of providing e ective disease management with limited resources , along with views on state - ofthe - art treatments in the areas of diagnostics , medical oncology , radiotherapy , and surgical oncology . 
finally , the forum will also host a didactic workshop on how to run a clinical trial ; a poster display of ongoing research relevant to asia ; and a poster discussion session in which authors of the three posters judged most in uential will have an opportunity to present their work orally . 
in this case report the second sentence of the rst paragraph ( she was given sirolimus and had complete remission of the disease . ) was included by error and should be ignored . 
additionally , the fth sentence of the second paragraph should have read : after a loading dose of 10 mg sirolimus , she received sirolimus once a day ; sirolimus doses were titrated to a trough sirolimus concentration of 512 ng / ml , attaining a nal maintenance dose of 2 mg once a day starting in may , 2004 . gerhard opelz , volker daniel , cord naujokat , et al . 
in this article the anti - epstein - barr virus immunoglobulin g reactivity should have read : 7735 1475 u / ml ( sandoglobulin ) , 1600 71 u / ml ( cytotect ) , and 1425 249 u / ml ( cytogam ) , as extrapolated from the results obtained at a one to ten dilution ( dade behring )  . vol 8 march 2007 re ection and reaction causation of pathophysiological changes that ultimately lead to cancer , h pylori is frequently not detectable at the time of neoplasia development.24 moreover , in a large proportion of patients with gastric cancer who were classi ed as h - pylori negative by use of routine elisa , past infection could be proved by analysis of antibodies to caga igg , which persist longer after loss of infection than do igg antibodies identi ed by conventional testing.3 , 4 di culties in the identi cation of past h - pylori infection frequently lead to an underestimation of the cancer risk attributable this bacterium.3 , 4 in 1994 , the international agency for research on cancer classi ed h pylori as a type 1 carcinogena de nite cause of human cancer.2 meimarakis and colleagues nding1 that infection with the carcinogenic bacterium is bene cial once cancer has developed seems paradoxical at rst , but might have a biological basis . 
however , the supporting evidence they provide is not convincing : the assumption that patients negative for h pylori have increased regulatory - t - cell responses in tumour tissue is biased by the use of ox40 ( tumour necrosis factor receptor superfamily member 4 ) as a mar ker of cd4 - positive , cd25positive regulatory t cells . 
although ox40 is expressed on regulatory t cells , it is not speci c for this cell type and is expressed by other types of lymphocytes such as activated type 1 and type 2 t - helper ( th ) cells.7 nevertheless , a model in which a microbe - induced immune response a ects tumour growth is plausible . 
 several physiological processes necessary for tumour devel opment , such as angiogenesis , cell survival , and tissue remodelling , are regulated by leucocytic in ltrates in the neoplastic environment , either directly or by secreted products . 
in stomach cancer , the extent of in ltration by cytotoxic t cells and natural - killer cells into the neoplasticcell nest is a signi cant predictor of patient survival.8 , 9 thus , microbe - induced in ammation might modulate antitumour immunity and a ect immune surveillance in the stomach or lymph nodes . 
this idea is consistent with the nding that h - pylori infection inhibits the progression of chemically induced gastric carcinogenesis in mice.10 vol 7 may 2006 more than 15% of all human cancer is thought to be caused by infections , some of which indirectly promote carcinogenesis through induction of chronic in ammatory states . 
in animal studies , an in ammatory response induced by h pylori is of fundamental importance for the development of bacteria - related gastric malig nant disease.11 in human beings , proin ammatory polymorphisms in cytokine genes strongly enhance cancer risk associated with h - pylori infection.12 however , once cancer has developed , persistent h - pylori infection and in ltration with some leucocyte subsets seem to correlate with a favourable prognosis . 
the results of meimarakis and colleagues1 re ect the clinical implications of this multifaceted and complex biology of infection and disease . * roland rad , christian prinz , roland m schmid 2nd department of internal medicine and gastroenterology , technical university of munich , ismaningerstr 22 , 81675 munich , germany roland.rad@lrz.tum.de we declare no con icts of interest . helicobacter pylori as a prognostic indicator after curative resection of gastric carcinoma : a prospective study . 
is helicobacter pylori infection a necessary condition for noncardia gastric cancer ? am j epidemiol 2004 ; 159 : 25258 . uemura n , okamoto s , yamamoto s , et al . 
 for example , the poster competition alone has resulted in nearly 100 submissions from 22 di erent countries , 74% of which report on research being done by groups in asia . 
furthermore , by drawing on the knowledge of a faculty of over 40 world - renowned speakers , the forum will focus on the ten most prevalent cancers in the asiapaci c region and will examine aspects of prevention , diagnosis , treatment , and palliation . 
opinion - leaders will discuss cancer aetiology , health - care systems , and the challenges of providing e ective disease management with limited resources , along with views on state - ofthe - art treatments in the areas of diagnostics , medical oncology , radiotherapy , and surgical oncology . 
finally , the forum will also host a didactic workshop on how to run a clinical trial ; a poster display of ongoing research relevant to asia ; and a poster discussion session in which authors of the three posters judged most in uential will have an opportunity to present their work orally . 
in this case report the second sentence of the rst paragraph ( she was given sirolimus and had complete remission of the disease . ) was included by error and should be ignored . 
additionally , the fth sentence of the second paragraph should have read : after a loading dose of 10 mg sirolimus , she received sirolimus once a day ; sirolimus doses were titrated to a trough sirolimus concentration of 512 ng / ml , attaining a nal maintenance dose of 2 mg once a day starting in may , 2004 . gerhard opelz , volker daniel , cord naujokat , et al . 
in this article the anti - epstein - barr virus immunoglobulin g reactivity should have read : 7735 1475 u / ml ( sandoglobulin ) , 1600 71 u / ml ( cytotect ) , and 1425 249 u / ml ( cytogam ) , as extrapolated from the results obtained at a one to ten dilution ( dade behring )  . vol 8 march 2007 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology shows that change in breast appearance and palpable induration are highly sensitive to randomised dose.1 the irradiated breast looking and feeling the same as the contralateral breast 10 years after treatment is a valid outcome for patients . 
given the / value of 30 gy for late adverse e ects , by calculation of the biological equivalent dose , his schedule is equivalent to 616 gy in 20 gy fractions , a dose expected to generate a high incidence of late normal - tissue injuries . 
kunkler should not blame the fraction size ; eight fractions of 425 gy ( total 34 gy ) would have reproduced the late adverse e ects of 50 gy in 20 gy fractions in the breast . 
the sensitivity of late normal - tissue endpoints to changes in fraction size is well established , and means that a large total dose reduction is needed when the fraction size is increased . 
the trial has su cient power , as re ected in the 95% ci for the estimate , to support the hypothesis that the fractionation sensitivity of breast cancer is similar to that of late e ects . 
 john r yarnold , soren m bentzen , joanne haviland , j roger owen department of radiotherapy , royal marsden hospital , downs road , sutton , sm2 5pt , uk john.yarnold@icr.ac.uk we declare no con icts of interest . yarnold j , ashton a , bliss j , et al . 
radiother oncol 2005 ; 75 : 917 . case reports and clinical pictures in the lancet oncology following the introduction of original research in 2005 , the lancet oncology has decided to phase out the publication of case reports and clinical pictures , because we believe their value within the journal has diminished . 
this reduction in the number of article categories will enable us to increase the amount of content in other existing sections of the journal . lidia siemaszkiewicz the lancet oncology , london nw1 7by , uk erratum owen r , ashton a , bliss jm , et al . 
e ect of radiotherapy fraction size on tumour control in patients with early - stage breast cancer after local tumour excision : long - term results of a randomised trial . 
in this article , the last sentence of the 5th paragraph in the procedures section ( p 469 ) should have read : the proportion of patients who received a boost was almost identical in all three treatment groups : 350 ( 75% ) patients for 50 gy , 348 ( 75% ) for 42.9 gy , and 353 ( 75% ) for 39 gy . 620 vol 7 august 2006 reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com re ection and reaction parameters and does not incorporate non - carcinoma variables , such as concomitant illnesses , which could also a ect patient outcome.2 however , in the midst of such uncertainty , fuzzy logic could have an important role in the decision - making process . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
in this review , the labelling of the four histological images in gure 2 should have been ( from left to right ) : dfsp , dsrct , mfh , and leio . 670 vol 8 august 2007 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper , clearly marked with the phrase sabcs call for papers , go to elsevier.com / thelancetoncology in the twentieth century : cure for many diseases is now available and other diseases have been rendered chronic . 
quality of life comprises physical , psychological , emotional , and spiritual issues , which are also the cornerstones of palliative medicine . palliative - care specialists face a great opportunity : to share their knowledge of integrated palliative care with other specialists , so that the latter can learn how to provide integrated care and cure . 
the more physicians are involved in the cure and care of a patient , the greater the risk that information is not shared , which might hamper good medical care . 
in breast cancer : a call for papers in many countries the probability of developing a cancer before the age of 65 years is fast approaching 15%.1 this is a substantial risk and of all cancers , breast neoplasia is the most prevalent , not only in women but also overall.1 the lancet oncology is , therefore , issuing a call for papers that will o er major advances in the management of breast cancer . 
accepted papers will be published in the lancet oncology to coincide with the san antonio breast cancer symposium ( sabcs ; tx , usa , dec 1316 , 2007 )  . 
 aacn clin issues 2005 ; 16 : 54250 . presentation at the sabcs , please let us know the precise details of the type of presentation ( such as including dates and poster or oral presentation ) , times , so that publication in the lancet oncology can be scheduled to comply with sabcss embargo policies . 
 articles should be submitted via the lancet oncologys online submission service , and all authors must clearly state in the covering letter that their submission is in response to the sabcs call for papers . 
the deadline for submissions is oct 12 , 2007 . david collingridge the lancet oncology , london nw1 7by , uk 1 mackay j , jemal a , lee nc , parkin dm . 
atlanta : american cancer society , 2006 . published online june 22 , 2007 doi : 10.1016 / s14702045 ( 07 ) 70177 - 8 see articles page 603 erratum on june 4 , 2007 , the lancet oncology published results online of the zest trial by martin stockler and colleagues.1 this was an early online publication , with print publication scheduled for the july issue . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
in this review , the labelling of the four histological images in gure 2 should have been ( from left to right ) : dfsp , dsrct , mfh , and leio . 670 vol 8 august 2007 re ection and reaction study , patients were treated in many centres worldwide without a speci c histopathological protocol . 
therefore , our results seem applicable to the community at large . unfortunately , several known risk factors were not reported in many patients , and cross - tabulations showed di erences in the three treatment groups for detection method ( p = 0001 ) , tumour size ( p = 0002 ) , tumour grade ( p = 004 ) , margin status ( p < 00001 ) , and oestrogen receptor status ( p = 006 )  . 
when comparing patients receiving radiotherapy who were given boost with those who were not , we found that the distribution for detection method tumour grade , or oestrogen receptor status was very similar between the two groups . 
as expected , patients with a boost had more tumours of unknown size ( 49% vs 31% ) , and unknown margin ( 43% vs 25% ) than patients who did not receive a boost . 
for example , in the european organisation for research and treatment of cancer ( eortc ) study , poor di erentiation was ( illogically ) better in terms of local recurrence than intermediate di erentiation in multivariate analysis.2 as in our study , age , margin status , and radiotherapy were important variables , and the researchers concluded that young women and those with involved margins are at high risk of local recurrence , even after radiotherapy with 50 gy.2 we know that young women are at high risk for local failure , so why shouldnt we use a boost with a proven bene t3 to improve the results in dcis too ? furthermore , boost radiotherapy was well - tolerated in the eortc study , 3 with only 1% severe breast brosis ( similar to that in the standard group ) and led to only a small reduction in excellent or good cosmesis . in our retrospective study , a boost was probably given more often in the presence of adverse prognostic factors . 
i agree that results might have been even better with a radiotherapeutic quality programme , and that an improved de nition of the exact boost volume might have been achieved . our results indicate the situation in invasive breast cancer , and in the absence of other data , they justify boost radiotherapy in young patients with dcis . 
the attainment of level 1 evidence from adequately powered randomised trials with a quality assurance programme is desirable , and future research by the international breast cancer study group ( ibcsg ) and eortc might one day address this . 
the question of which treatment should be used as standard is debatable , but we think boost treatment is the most promising strategy . guenther gruber coordinator of the radiation oncology task force , ibcsg international breast cancer study group , institute of radiation oncology , kantonsspital , aarau , switzerland guenther.gruber@ksa.ch i declare no con icts of interest . omlin a , amichetti m , azria d , et al . 
breast - conserving treatment with or without radiotherapy in ductal carcinoma in situ : ten - year results of european organisation for research and treatment of cancer randomized phase iii trial 10853a study by the eortc breast cancer cooperative group and eortc radiotherapy group . 
in table 6 of this health - care research article ( p 592 ) , the estimated demand for megavoltage machines in 2002 for chile should have read 44 , and the total estimated demand for megavoltage machines in 2002 should have read 1060 . douillard j - y , rosell r , de lena m , et al . 
adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ibiiia non - smallcell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
the a liation for v lorusso should have read irccs oncologico , bari , italy ( v lorusso md ) in the author address list ( p 719 ) and m de lena , v lorusso ( irccs oncologico , bari ) in the investigator list ( p 726 )  . 
in the investigator list ( p 726 ) , e massa ( policlinico universitario , cagliari ) should have read g mantovani , e massa ( policlinico universitario , cagliari )  . gajjar a , chintagumpala m , ashley d , et al . 
risk - adapted craniospinal radiotherapy followed by high - dose chemotherapy and stem - cell rescue in children with newly diagnosed medulloblastoma ( st jude medulloblastoma96 ) : long - term results from a prospective , multicentre trial . 
the fourth sentence of the second paragraph in the results ( p 816 ) should have read : 5 - year event - free survival was 66% ( 4883 ) for the 42 patients with metastatic disease and 63% ( 4483 ) for the 33 patients with m23 disease . vol 7 october 2006 re ection and reaction richard g grundy childrens brain tumour research centre , university of nottingham , the medical school , queens medical centre , nottingham ng7 2uh , uk richard.grundy@nottingham.ac.uk the author declared no con icts of interest . grundy rg , wilne sa , weston cl , et al . 
pediatr neurosurg 1998 ; 28 : 21522 . bou et e , perilongo g , canete a , massimino m et al intracranial ependymoma in children ; a critical review of prognostic markers and a plea for cooperation . 
med pediatr oncol 1998 ; 40 : 3440 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zupancic m , shah pc , shah - khan f , nagendra s . 
in this review , the author list should have read : melanie zupancic , prabodh c shah , farheen shah - khan , sanjai nagendra . grundy rg , wilne sa , weston cl , et al . 
 full total resection less than full total resection 100 075 050 025 000 numbers at risk total resection 44 partial resection 45 time from surgery ( years ) 7 figure 5 : overall survival based on neurosurgical assessment of the extent of resection at the end of surgery vol 8 september 2007 re ection and reaction study , patients were treated in many centres worldwide without a speci c histopathological protocol . 
therefore , our results seem applicable to the community at large . unfortunately , several known risk factors were not reported in many patients , and cross - tabulations showed di erences in the three treatment groups for detection method ( p = 0001 ) , tumour size ( p = 0002 ) , tumour grade ( p = 004 ) , margin status ( p < 00001 ) , and oestrogen receptor status ( p = 006 )  . 
when comparing patients receiving radiotherapy who were given boost with those who were not , we found that the distribution for detection method tumour grade , or oestrogen receptor status was very similar between the two groups . 
as expected , patients with a boost had more tumours of unknown size ( 49% vs 31% ) , and unknown margin ( 43% vs 25% ) than patients who did not receive a boost . 
for example , in the european organisation for research and treatment of cancer ( eortc ) study , poor di erentiation was ( illogically ) better in terms of local recurrence than intermediate di erentiation in multivariate analysis.2 as in our study , age , margin status , and radiotherapy were important variables , and the researchers concluded that young women and those with involved margins are at high risk of local recurrence , even after radiotherapy with 50 gy.2 we know that young women are at high risk for local failure , so why shouldnt we use a boost with a proven bene t3 to improve the results in dcis too ? furthermore , boost radiotherapy was well - tolerated in the eortc study , 3 with only 1% severe breast brosis ( similar to that in the standard group ) and led to only a small reduction in excellent or good cosmesis . in our retrospective study , a boost was probably given more often in the presence of adverse prognostic factors . 
i agree that results might have been even better with a radiotherapeutic quality programme , and that an improved de nition of the exact boost volume might have been achieved . our results indicate the situation in invasive breast cancer , and in the absence of other data , they justify boost radiotherapy in young patients with dcis . 
the attainment of level 1 evidence from adequately powered randomised trials with a quality assurance programme is desirable , and future research by the international breast cancer study group ( ibcsg ) and eortc might one day address this . 
the question of which treatment should be used as standard is debatable , but we think boost treatment is the most promising strategy . guenther gruber coordinator of the radiation oncology task force , ibcsg international breast cancer study group , institute of radiation oncology , kantonsspital , aarau , switzerland guenther.gruber@ksa.ch i declare no con icts of interest . omlin a , amichetti m , azria d , et al . 
breast - conserving treatment with or without radiotherapy in ductal carcinoma in situ : ten - year results of european organisation for research and treatment of cancer randomized phase iii trial 10853a study by the eortc breast cancer cooperative group and eortc radiotherapy group . 
in table 6 of this health - care research article ( p 592 ) , the estimated demand for megavoltage machines in 2002 for chile should have read 44 , and the total estimated demand for megavoltage machines in 2002 should have read 1060 . douillard j - y , rosell r , de lena m , et al . 
adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ibiiia non - smallcell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
the a liation for v lorusso should have read irccs oncologico , bari , italy ( v lorusso md ) in the author address list ( p 719 ) and m de lena , v lorusso ( irccs oncologico , bari ) in the investigator list ( p 726 )  . 
in the investigator list ( p 726 ) , e massa ( policlinico universitario , cagliari ) should have read g mantovani , e massa ( policlinico universitario , cagliari )  . gajjar a , chintagumpala m , ashley d , et al . 
risk - adapted craniospinal radiotherapy followed by high - dose chemotherapy and stem - cell rescue in children with newly diagnosed medulloblastoma ( st jude medulloblastoma96 ) : long - term results from a prospective , multicentre trial . 
the fourth sentence of the second paragraph in the results ( p 816 ) should have read : 5 - year event - free survival was 66% ( 4883 ) for the 42 patients with metastatic disease and 63% ( 4483 ) for the 33 patients with m23 disease . vol 7 october 2006 newsdesk virus linked with prostate cancer new microarray technology has linked a previously unknown virus to prostate cancer , although the exact relation between the virus and prost ate cancer is not yet clear . the virus , tentatively named xmrv , is similar to leukaemia viruses that infect mice , but seems to infect only human beings . 
the lack of studies in animals will complicate e orts to determine the virus precise role in prostate cancer , says eric klein , ( cleveland clinic , cleveland , oh , usa ) who reported the study at the american society for clinical oncology prostate cancer symposium ( san francisco , ca , usa ; feb 2426 , 2006 )  . 
furthermore , the chip is a tool that can be used to invest igate any aetiology , disease of unknown especially when the epid em iol ogy of a disease suggests infec tion is a factor , says derisi . 
 virus was seen in tissues from patients with prostate cancer who were homozygous for a single nucleotide polymorphism , known as r462q , which codes for a variant , malfunctioning form of rnase l . 
the wildtype enzyme degrades single - strand ed rna in response to interferon or viral infection , preventing propaga tion of viruses once they have infected the cell , and trigg ering apoptosis in the host cell . the chip contains several thousand conserved sequences from every virus known to infect plants , animals , and humansa total of nearly 1000 viruses . 
 researchers use these sequences as probes to uncover previously unknown viruses in tissues . the researchers are also attempting to identify other viruses in cancers particularly those that occur in patients with compromised immune systems . 
 these include aids - related lymph omas and skin cancers associated with solidorgan transplantation . tabitha m powledge sentinel - node mapping for staging of colorectal cancer use of sentinel - node mapping to stage colorectal cancer can lead to increased detection of nodal metastases and lower recurrence compared with conventional procedures , according to new ndings ( am j surg 2006 ; 191 : 30510 )  . lymph - node status is one of the most important prognostic factors used to determine treatment after a diagnosis of colorectal cancer . 
patients with nodal disease are given adjuvant chemotherapy because of evidence of potential mortality red uctions of 33% with such treatment ; but there is no de nitive evidence for survival bene t with adjuvant chemo therapy in patients who are node - negative  . because conventional pathology under stages 1520% of patients with colo rectal cancer , sentinel - lymph - node map ping was developed to identify nodes most likely to harbour metastases . 
 it would be cost prohib itive to perform such ultra staging methods on all nodes harvested during conventional surg ery , says sukamal saha ( michigan state university , mi , usa )  . saha and co - workers compared outcomes of 500 consecutive patients who underwent sent inel - lymph - node mapping with 368 consecutive patients who underwent conventional surgery and pathological assessment . nodal positivity was 48% for the group assigned sentinel - lymph - node map ping , compared with 35% for the group assigned conventional staging ( p < 0001 )  . 
after a minimum of 2 years follow - up , patients assigned nodal mapping ( n = 153 ) had an overall recur rence of 7% , compared with 25% for the 162 patients assigned conven tional staging ( p = 0001 )  . sentinel - node biopsy in colorectal cancer is controversialstudies have found identi cation rates of 7799% , resulting in a false - negative rate of 360% . 
the volume of dye sentinel - node mapping : the route to increased identi cation of nodal metastasis they injected was according to the diameter of the tumour as opposed to a xed volume [ as ] in other studies , says markus zuber ( university of basel , switzerland )  . 
therefore , our results seem applicable to the community at large . unfortunately , several known risk factors were not reported in many patients , and cross - tabulations showed di erences in the three treatment groups for detection method ( p = 0001 ) , tumour size ( p = 0002 ) , tumour grade ( p = 004 ) , margin status ( p < 00001 ) , and oestrogen receptor status ( p = 006 )  . 
when comparing patients receiving radiotherapy who were given boost with those who were not , we found that the distribution for detection method tumour grade , or oestrogen receptor status was very similar between the two groups . 
as expected , patients with a boost had more tumours of unknown size ( 49% vs 31% ) , and unknown margin ( 43% vs 25% ) than patients who did not receive a boost . 
for example , in the european organisation for research and treatment of cancer ( eortc ) study , poor di erentiation was ( illogically ) better in terms of local recurrence than intermediate di erentiation in multivariate analysis.2 as in our study , age , margin status , and radiotherapy were important variables , and the researchers concluded that young women and those with involved margins are at high risk of local recurrence , even after radiotherapy with 50 gy.2 we know that young women are at high risk for local failure , so why shouldnt we use a boost with a proven bene t3 to improve the results in dcis too ? furthermore , boost radiotherapy was well - tolerated in the eortc study , 3 with only 1% severe breast brosis ( similar to that in the standard group ) and led to only a small reduction in excellent or good cosmesis . in our retrospective study , a boost was probably given more often in the presence of adverse prognostic factors . 
i agree that results might have been even better with a radiotherapeutic quality programme , and that an improved de nition of the exact boost volume might have been achieved . our results indicate the situation in invasive breast cancer , and in the absence of other data , they justify boost radiotherapy in young patients with dcis . 
the attainment of level 1 evidence from adequately powered randomised trials with a quality assurance programme is desirable , and future research by the international breast cancer study group ( ibcsg ) and eortc might one day address this . 
the question of which treatment should be used as standard is debatable , but we think boost treatment is the most promising strategy . guenther gruber coordinator of the radiation oncology task force , ibcsg international breast cancer study group , institute of radiation oncology , kantonsspital , aarau , switzerland guenther.gruber@ksa.ch i declare no con icts of interest . omlin a , amichetti m , azria d , et al . 
breast - conserving treatment with or without radiotherapy in ductal carcinoma in situ : ten - year results of european organisation for research and treatment of cancer randomized phase iii trial 10853a study by the eortc breast cancer cooperative group and eortc radiotherapy group . 
in table 6 of this health - care research article ( p 592 ) , the estimated demand for megavoltage machines in 2002 for chile should have read 44 , and the total estimated demand for megavoltage machines in 2002 should have read 1060 . douillard j - y , rosell r , de lena m , et al . 
adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ibiiia non - smallcell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
the a liation for v lorusso should have read irccs oncologico , bari , italy ( v lorusso md ) in the author address list ( p 719 ) and m de lena , v lorusso ( irccs oncologico , bari ) in the investigator list ( p 726 )  . 
in the investigator list ( p 726 ) , e massa ( policlinico universitario , cagliari ) should have read g mantovani , e massa ( policlinico universitario , cagliari )  . gajjar a , chintagumpala m , ashley d , et al . 
risk - adapted craniospinal radiotherapy followed by high - dose chemotherapy and stem - cell rescue in children with newly diagnosed medulloblastoma ( st jude medulloblastoma96 ) : long - term results from a prospective , multicentre trial . 
the fourth sentence of the second paragraph in the results ( p 816 ) should have read : 5 - year event - free survival was 66% ( 4883 ) for the 42 patients with metastatic disease and 63% ( 4483 ) for the 33 patients with m23 disease . vol 7 october 2006 reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com re ection and reaction richard g grundy childrens brain tumour research centre , university of nottingham , the medical school , queens medical centre , nottingham ng7 2uh , uk richard.grundy@nottingham.ac.uk the author declared no con icts of interest . grundy rg , wilne sa , weston cl , et al . 
pediatr neurosurg 1998 ; 28 : 21522 . bou et e , perilongo g , canete a , massimino m et al intracranial ependymoma in children ; a critical review of prognostic markers and a plea for cooperation . 
med pediatr oncol 1998 ; 40 : 3440 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zupancic m , shah pc , shah - khan f , nagendra s . 
in this review , the author list should have read : melanie zupancic , prabodh c shah , farheen shah - khan , sanjai nagendra . grundy rg , wilne sa , weston cl , et al . 
 full total resection less than full total resection 100 075 050 025 000 numbers at risk total resection 44 partial resection 45 time from surgery ( years ) 7 figure 5 : overall survival based on neurosurgical assessment of the extent of resection at the end of surgery vol 8 september 2007 newsdesk virus linked with prostate cancer new microarray technology has linked a previously unknown virus to prostate cancer , although the exact relation between the virus and prost ate cancer is not yet clear . the virus , tentatively named xmrv , is similar to leukaemia viruses that infect mice , but seems to infect only human beings . 
the lack of studies in animals will complicate e orts to determine the virus precise role in prostate cancer , says eric klein , ( cleveland clinic , cleveland , oh , usa ) who reported the study at the american society for clinical oncology prostate cancer symposium ( san francisco , ca , usa ; feb 2426 , 2006 )  . 
furthermore , the chip is a tool that can be used to invest igate any aetiology , disease of unknown especially when the epid em iol ogy of a disease suggests infec tion is a factor , says derisi . 
 virus was seen in tissues from patients with prostate cancer who were homozygous for a single nucleotide polymorphism , known as r462q , which codes for a variant , malfunctioning form of rnase l . 
the wildtype enzyme degrades single - strand ed rna in response to interferon or viral infection , preventing propaga tion of viruses once they have infected the cell , and trigg ering apoptosis in the host cell . the chip contains several thousand conserved sequences from every virus known to infect plants , animals , and humansa total of nearly 1000 viruses . 
 researchers use these sequences as probes to uncover previously unknown viruses in tissues . the researchers are also attempting to identify other viruses in cancers particularly those that occur in patients with compromised immune systems . 
 these include aids - related lymph omas and skin cancers associated with solidorgan transplantation . tabitha m powledge sentinel - node mapping for staging of colorectal cancer use of sentinel - node mapping to stage colorectal cancer can lead to increased detection of nodal metastases and lower recurrence compared with conventional procedures , according to new ndings ( am j surg 2006 ; 191 : 30510 )  . lymph - node status is one of the most important prognostic factors used to determine treatment after a diagnosis of colorectal cancer . 
patients with nodal disease are given adjuvant chemotherapy because of evidence of potential mortality red uctions of 33% with such treatment ; but there is no de nitive evidence for survival bene t with adjuvant chemo therapy in patients who are node - negative  . because conventional pathology under stages 1520% of patients with colo rectal cancer , sentinel - lymph - node map ping was developed to identify nodes most likely to harbour metastases . 
 it would be cost prohib itive to perform such ultra staging methods on all nodes harvested during conventional surg ery , says sukamal saha ( michigan state university , mi , usa )  . saha and co - workers compared outcomes of 500 consecutive patients who underwent sent inel - lymph - node mapping with 368 consecutive patients who underwent conventional surgery and pathological assessment . nodal positivity was 48% for the group assigned sentinel - lymph - node map ping , compared with 35% for the group assigned conventional staging ( p < 0001 )  . 
after a minimum of 2 years follow - up , patients assigned nodal mapping ( n = 153 ) had an overall recur rence of 7% , compared with 25% for the 162 patients assigned conven tional staging ( p = 0001 )  . sentinel - node biopsy in colorectal cancer is controversialstudies have found identi cation rates of 7799% , resulting in a false - negative rate of 360% . 
the volume of dye sentinel - node mapping : the route to increased identi cation of nodal metastasis they injected was according to the diameter of the tumour as opposed to a xed volume [ as ] in other studies , says markus zuber ( university of basel , switzerland )  . 
 janet fricker vol 7 april 2006 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com anne szarewski cancer research uk centre for epidemiology , mathematics , and statistics , wolfson institute of preventive medicine , london ec1m 6bq , uk anne.szarewski@cancer.org.uk i have been sponsored by various pharmaceutical companies that manufacture contraceptive drugs to attend or lecture at many conferences , to give expert testimonies , or to act in a consultancy capacity . 
london : chapman and hall , 1991 . authors reply iarc thanks samuel shapiro and anne szarewski for their remarks regarding the policy watch article on combined oestrogenprogestagen contraceptives and menopausal treatment.1 samuel shapiro participated in the monograph meeting at our invitation , and the discussions beneted from his knowledge . 
according to iarc rules , samuel shapiro did not participate in the assessments because of the conict of interest he declared before the meeting . samuel shapiro believes that the working group was restricted from the assessment of evidence for the carcinogenicity of oestrogen - only or progestagen - only products . 
all iarc working groups are free to consider any published studies they regard as pertinent , and iarc made the previous monograph on single - ingredient products2 available to the working group . 
however , the effects of combined oestrogen and progestagen products are complex , and to extrapolate from studies of singleingredient products to predict the carcinogenicity of combined products would have been difcult . 
the working group noted , for example , that the increased risk of breast cancer is higher with combined menopausal treatment than with oestrogen - only menopausal treatment , and that the increased risk of endometrial cancer with combined treatment depends on the number of days per cycle progestagens are taken . epidemiological studies on the combined products themselves were more informative in assessing their carcinogenicity and consequently the working group decided to specically focus on these studies . 
carcinogenicity of combined oestrogenprogestagen contraceptives and menopausal treatment . lancet oncol 2005 ; 6 : 55253 . iarc monographs on the evaluation of carcinogenic risks to humans , volume 72 , hormonal contraception and post - menopausal hormonal therapy . 
lancet oncol 2005 ; 6 : 263the rst sentence of the second paragraph should read : in the rst study , researchers from mayo clinic ( rochester , mn , usa ) analysed survival of 842 patients who had radical prostatectomy for ct3 prostate cancer . vol 6 october 2005 re ection and reaction many ovarian cancers are diagnosed as international federation of gynecology and obstetrics stage iii disease . 
women with this stage of disease have a 5 - year survival of only 302%57% , 8 therefore studies with these women needs to start at the time of diagnosis . 
the main advantage of a prospective study would be the accurate documentation of the use of oral contraceptives , and this could help establish the period of time a woman should be using oral contraceptives , for prevention of ovarian cancer . 
 given that oral contraception has been available for more than 45 years , it would be too draconian not to o er patients such an intervention for chemoprevention of ovarian cancer , especially because the management of high - risk women with a brca mutation is multimodal and includes intensi ed early detection and prophylactic surgery . 
in this article the a liations for prof f boccardo and prof a rubagotti should have read : university of genoa , italy , and national cancer research institute of genoa , italy ( prof f boccardo md , prof a rubagotti phd )  . 
 more work needs to be done on the assessment of the risks and bene ts of oral contraception in addition to the lowered risk of ovarian cancer , the increased risk of breast cancer among carriers of a brca mutation also needs to be discussed in this context . 
 from case - control studies we know that the relative risk for breast cancer is not increased5 or only modestly increased ( or 12 ; 95% ci 102140 ) , 6 by the use of oral contraceptives . 
in view of the fact that carriers of a brca mutation have a lifetime risk for the development of breast cancer of up to 84% , 7 an odds ratio of 12 is considerable and should to be taken into account in the risk management of these patients . 
conversely , the risk reduction for ovarian cancer noted in the study by mclaughin and co - workers2odds ratio of 056 ( 95% ci 045071 ) in carriers of a brca1 mutation and 039 ( 023066 ) in carriers of a brca2 mutationcan be o set against the potentially increased risk of breast cancer . 
what is needed is to be able to provide a risk pro le for an individual person to allow accurate risk management in an individual woman . case - control studies do have limitations because they do not acquire prospective data , such as real risks for the development of cancers , or disease - speci c survival data . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
such features are consistent with the evidence we have reported from japan.7 , 8 the us6 and uk5 studies suggest that at and depressed tumours are more likely to be underdiagnosed in western countries.9 routine use of chromoendoscopy would give a solution to this issue because about 60% of at and depressed tumours could be missed without use of this technique.6 tsuyoshi konishi , * toshiaki watanabe , tetsuichiro muto , kenjiro kotake , hirokazu nagawa , on behalf of the japanese society for cancer of the colon and rectum department of surgical oncology , university of tokyo , 7 - 3 - 1 , hongo , bunkyo - ku , tokyo 113 - 8655 , japan ( tk , tw , hn ) ; department of surgery , cancer institute hospital , 3 - 10 - 6 , ariake , koutou - ku , tokyo 135 - 8550 , japan ( tm ) ; and department of surgery , tochigi cancer center , 4 - 9 - 13 , yohnan , utsunomiya , tochigi 320 - 0834 , japan ( kk ) toshwatanabe@yahoo.co.jp we declare no conicts of interest . vol 7 february 2006 if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com re ection and reaction moreover , our in - vitro calibrations suggested that at the high cell burdens often seen in cll , it was likely that , as a consequence of treatment with the usual dose of rituximab ( 375 mg / m2 , once a week for 4 weeks ) , complement would be consumed substantially , and complement - dependent cytotoxicity could be abrogated , thus compromising the e ectiveness of the treatment . 
we reported that complement was depleted for up to several weeks in several patients with cll as a consequence of rituximab treatment , thus leading us to propose that use of fresh frozen plasma could enhance the therapeutic action of rituximab in cll . 
 finally , use of large amounts of rituximab at these high cell burdens saturates a second e ector - cell mechanism that is important in the action of rituximabie , fcrmediated clearance of cll cells . 
this e ect leads to a second event in which almost all cd20 is removed ( shaved ) from the targeted cells , further compromising the treatment.2 , 6 the cd20 concentrations of the patient reported by klep sh and co - workers would have been interesting to follow to establish whether supplemental complement can modulate the shaving reaction . ronald taylor university of virginia school of medicine , charlottesville , va , usa rpt@virginia.edu the author declared no con icts of interest 1 . 
j immunol 2006 ; 177 : 743543 . paediatric oncology : a call for papers if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology submitted via the lancet oncologys online submission service , and all authors must clearly state in the covering letter that their submission is in response to the paediatric oncology call for papers . 
please note that the deadline for submission is may 21 , 2007 . to submit a paper , clearly marked with the phrase paediatric oncology call for papers , go to thelancetoncology cancer a ects about 1 in 500 children under 15 years of age.1 although great strides have been made in the treatment of paediatric cancer over the past few decades , in the uk about 20% of all deaths in children aged 1 to 14 years are still caused by cancer.1 the lancet oncology is therefore issuing a call for papers that address paediatric cancer . 
accepted papers will be published in the lancet oncology to coincide with the international society of paediatric oncology ( siop ) annual congress ( mumbai , india ; nov 13 , 2007 )  . 
if your submission describes , in part or wholly , a study accepted for presentation at the siop annual congress , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication in the lancet oncology can be scheduled to comply with siops embargo policies . 
articles should be lidia siemaszkiewicz the lancet oncology , london nw1 7by , uk charles stiller ( childhood cancer research group ) , mike quinn , steve rowan ( o ce for national statistics )  . 
the third sentence of the fourth paragraph should have read : alvin eisner ( oregon health & science university , portland , or , usa ) , whose group has recently shown that anastrozole does not produce the neurological changes detectable in the eyes of women who have received tamoxifen ( breast cancer res treat published online jan 27 , 2007 ; doi : 10.1007 / s10549 - 006 - 9486 - 3 ) does think , nevertheless , that further studies need to be done to compare side e ect pro les . vol 8 may 2007 re ection and reaction many ovarian cancers are diagnosed as international federation of gynecology and obstetrics stage iii disease . 
women with this stage of disease have a 5 - year survival of only 302%57% , 8 therefore studies with these women needs to start at the time of diagnosis . 
the main advantage of a prospective study would be the accurate documentation of the use of oral contraceptives , and this could help establish the period of time a woman should be using oral contraceptives , for prevention of ovarian cancer . 
 given that oral contraception has been available for more than 45 years , it would be too draconian not to o er patients such an intervention for chemoprevention of ovarian cancer , especially because the management of high - risk women with a brca mutation is multimodal and includes intensi ed early detection and prophylactic surgery . 
in this article the a liations for prof f boccardo and prof a rubagotti should have read : university of genoa , italy , and national cancer research institute of genoa , italy ( prof f boccardo md , prof a rubagotti phd )  . 
 more work needs to be done on the assessment of the risks and bene ts of oral contraception in addition to the lowered risk of ovarian cancer , the increased risk of breast cancer among carriers of a brca mutation also needs to be discussed in this context . 
 from case - control studies we know that the relative risk for breast cancer is not increased5 or only modestly increased ( or 12 ; 95% ci 102140 ) , 6 by the use of oral contraceptives . 
in view of the fact that carriers of a brca mutation have a lifetime risk for the development of breast cancer of up to 84% , 7 an odds ratio of 12 is considerable and should to be taken into account in the risk management of these patients . 
conversely , the risk reduction for ovarian cancer noted in the study by mclaughin and co - workers2odds ratio of 056 ( 95% ci 045071 ) in carriers of a brca1 mutation and 039 ( 023066 ) in carriers of a brca2 mutationcan be o set against the potentially increased risk of breast cancer . 
what is needed is to be able to provide a risk pro le for an individual person to allow accurate risk management in an individual woman . case - control studies do have limitations because they do not acquire prospective data , such as real risks for the development of cancers , or disease - speci c survival data . 
 vol 8 january 2007 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com unfortunately , this benet will not be realised from meta - analyses because of the absence of stage stratication in existing studies . 
we agree that the use of endoluminal ultrasonography and possibly pet should be a requirement to stratify patients in future randomised trials of preoperative treatment oesophageal cancer . * bryan h burmeister , b mark smithers university of queensland , princess alexandra hospital , brisbane , 4102 , australia bryan_burmeister@health.qld.gov.au i declare no conicts of interest . burmeister bh , smithers bm , gebski v , et al . 
 for example , the poster competition alone has resulted in nearly 100 submissions from 22 di erent countries , 74% of which report on research being done by groups in asia . 
furthermore , by drawing on the knowledge of a faculty of over 40 world - renowned speakers , the forum will focus on the ten most prevalent cancers in the asiapaci c region and will examine aspects of prevention , diagnosis , treatment , and palliation . 
opinion - leaders will discuss cancer aetiology , health - care systems , and the challenges of providing e ective disease management with limited resources , along with views on state - ofthe - art treatments in the areas of diagnostics , medical oncology , radiotherapy , and surgical oncology . 
finally , the forum will also host a didactic workshop on how to run a clinical trial ; a poster display of ongoing research relevant to asia ; and a poster discussion session in which authors of the three posters judged most in uential will have an opportunity to present their work orally . 
in this case report the second sentence of the rst paragraph ( she was given sirolimus and had complete remission of the disease . ) was included by error and should be ignored . 
additionally , the fth sentence of the second paragraph should have read : after a loading dose of 10 mg sirolimus , she received sirolimus once a day ; sirolimus doses were titrated to a trough sirolimus concentration of 512 ng / ml , attaining a nal maintenance dose of 2 mg once a day starting in may , 2004 . gerhard opelz , volker daniel , cord naujokat , et al . 
in this article the anti - epstein - barr virus immunoglobulin g reactivity should have read : 7735 1475 u / ml ( sandoglobulin ) , 1600 71 u / ml ( cytotect ) , and 1425 249 u / ml ( cytogam ) , as extrapolated from the results obtained at a one to ten dilution ( dade behring )  . vol 8 march 2007 re ection and reaction richard g grundy childrens brain tumour research centre , university of nottingham , the medical school , queens medical centre , nottingham ng7 2uh , uk richard.grundy@nottingham.ac.uk the author declared no con icts of interest . grundy rg , wilne sa , weston cl , et al . 
pediatr neurosurg 1998 ; 28 : 21522 . bou et e , perilongo g , canete a , massimino m et al intracranial ependymoma in children ; a critical review of prognostic markers and a plea for cooperation . 
med pediatr oncol 1998 ; 40 : 3440 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zupancic m , shah pc , shah - khan f , nagendra s . 
in this review , the author list should have read : melanie zupancic , prabodh c shah , farheen shah - khan , sanjai nagendra . grundy rg , wilne sa , weston cl , et al . 
we aimed to assess whether exposure to ionising radiation through mammography screening was associated with risk of breast cancer in brca1 or brca2 mutation carriers . methods we identi ed 1600 cases of breast cancer and 1600 controls without breast cancer who were matched for brca mutation , date of birth ( within 1 year ) , and country of residence from an international registry of brca1 and brca2 mutation carriers . 
 results we found no association between ever having screening mammography and risk of breast cancer ( odds ratio [ or ] 103 [ 95% ci 085125 ] , adjusted for parity , oral - contraceptive use , ethnic origin , and bilateral oophorectomy )  . 
 the association was much the same for brca1 mutation carriers and brca2 mutation carriers ( 104 [ 084129 ] vs 106 [ 067166 ] , respectively , adjusted for parity , oral - contraceptive use , ethnic origin , and bilateral oophorectomy )  . interpretation these ndings do not lend support to the idea that exposure to ionising radiation through routine screening mammography contributes substantially to the burden of breast cancer in brca1 and brca2 mutation carriers . 
prospective studies are needed to con rm the results of this initial report , and , where possible , these studies should assess a more appropriate endpoint of total exposure . introduction women with a germline mutation in brca1 or brca2 have increased risks of developing breast and ovarian cancer . 
because the risk of breast cancer rises substantially from age 25 years and peaks between age 3050 years , some researchers1 , 2 recommended that screening should start early ( ie , at age 25 years )  . 
current methods of screening for breast cancer include mammography , ultrasonography , clinical examination , and mri.3 at present , mammography is the most widely used imaging modality . screening mammography is associated with a small dose of radiation to the breast . 
this dose is not thought to be high enough to increase the risk of breast cancer in the general population , but women who are at increased genetic risk might be particularly sensitive to the dnadamaging e ects of ionising radiation.46 hereditary breast cancer typically occurs at a young age ( ie , women in their thrities and forties ) , and brca1 and brca2 have a role in the repair of dna damage.7 , 8 these two proteins help repair double - strand dna breaks , which are characteristic of lesions induced by ionising radiation . 
radiation is an established risk factor for early - onset breast cancer in the general population , 911 although exposure levels associated with this risk are many times greater than that associated with screening mammography . 
we aimed to assess whether screening mammography was associated with risk of breast cancer in brca1 and brca2 mutation carriers . methods participants women with a brca1 or brca2 mutation were identi ed through a registry of mutation carriers , which was located at the centre for research on womens health , university of toronto , ontario , canada . 
data for these women were gathered from women with known pathogenic brca1 and brca2 mutations during genetic counselling and mutation testing at 44 centres in six countries in north america , europe , and israel . 
when a mutation in brca1 or brca2 was found in a proband or in her relative , genetic testing was o ered to other at - risk women in her family . 
mutations were identi ed by use of various techniques during the course of genetic testing , but all 402 vol 7 may 2006 articles abnormal nucleotide sequences were con rmed by direct sequencing of dna . 
 from april 26 1992 , to july 12 2005 , data were submitted to the registry for 4951 women with a brca1 or brca2 mutation and with information on history of mammography , including age at rst mammography . 
41 women were excluded because they were diagnosed with ovarian cancer or any other cancer before diagnosis with breast cancer ; 165 women were excluded because they had had three women were prophylactic mastectomy ; and excluded because of missing data for important variables . 
 after exclusions , there were 4742 eligible brca mutation carriers2181 women with breast cancer ( ie , cases ) and 2561 women without breast cancer ( ie , con trols )  . 
cases and controls were matched for date of birth ( within 1 year ) , brca mutation ( brca1 vs brca2 ) , and country of residence ; matching was done by ps using a computer prograthe control could not have been diagnosed with any cancer before the age of diagnosis of breast cancer for the case . 
for this study , questionnaires were excluded if age at breast - cancer diagnosis or age at rst mammography were missing . the questionnaire inquired about whether participants had ever had screening mammography , and , if so , the age at which they rst had the procedure ; and about the total number of mammography procedures they had had in their lifetime ( ie , until the date of questionnaire completion )  . 
because of the di culty in distinguishing between screening mammography and diagnostic mammography for cases , we restricted our analyses to the rst mammography that took place at least 1 year before the year of diagnosis of breast cancerie , a mammography procedure was excluded from analyses if it was reported to have occurred in the same calendar year as breast - cancer diagnosis or in the year before breast - cancer diagnosis . 
information on cancer diagnoses were obtained from the questionnaire . information for family history was derived from pedigrees , which were drawn by research personnel at every centre ; pedigrees were sent to the study centre in toronto with , but separate from , questionnaires . 
 statistical analyses we analysed age at rst mammography for every case and matched control by classifying women into three age - groups : 30 years or younger ; 3140 years ; and 41 years age ( years ) median ( range ) year of birth year ( range ) mutation brca1 brca2 parity mean ( sd ) nulliparous oral contraceptives bilateral oophorectomy country of residence ever use ever usa canada poland norway israel austria ethnic origin jewish french - canadian other white other controls ( n = 1600 ) cases ( n = 1600 ) 467 ( 214832 ) 473 ( 189826 ) 011 * 1953 ( 19151981 ) 1953 ( 19151980 ) matched 1260 ( 79% ) 340 ( 21% ) 20 ( 14 ) 288 ( 18% ) 1260 ( 79% ) 340 ( 21% ) 20 ( 13 ) 249 ( 16% ) 945 ( 59% ) 941 ( 59% ) 76 ( 5% ) 51 ( 3% ) 520 ( 33% ) 474 ( 30% ) 461 ( 29% ) 71 ( 4% ) 50 ( 3% ) 24 ( 2% ) 330 ( 21% ) 128 ( 8% ) 1119 ( 70% ) 23 ( 1% ) 520 ( 33% ) 474 ( 30% ) 461 ( 29% ) 71 ( 4% ) 50 ( 3% ) 24 ( 2% ) 271 ( 17% ) 145 ( 9% ) 1144 ( 72% ) 40 ( 3% ) matched 03 * 007 09 002 matched 001 family history of breast cancer one or more rst - degree relatives with breast cancer 803 ( 59% ) 764 ( 57% ) || 037 data are number ( % ) , unless otherwise stated ; data might not add to 100% because of rounding . 
 * adjusted for parity , oral - contraceptive use , bilateral oophorectomy , and ethnic orig table 2 : association between age of rst mammography and risk of breast cancer for all women and by brca mutation , age at breast - cancer diagnosis , and cancer not identi ed by mammography or older . 
because ionising radiation is thought to be a risk factor for early - onset breast cancer in particular , analyses were repeated after strati cation of cases by age of diagnosis ( 40 years vs > 40 years )  . 
furthermore , because the intensity of screening mammography might a ect the age of breast - cancer diagnosis ( ie , women who have regular screening might have breast cancer diagnosed earlier than women who do not participate in a screening programme ) , we did a subgroup analysis of cases with breast cancer diagnosed by procedures other than mammographyie , by self - examination or physician examination . 
 role of the funding source the sponsor of this study had no role in the study design ; in the collection , analysis , or interpretation of the data ; or in the writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results table 1 shows the characteristics of the 1600 cases and 1600 matched controls . 
controls were signi cantly more likely to have had bilateral oophorectomy than were cases , but only 127 ( 4% ) of all participants had had a bilateral oophorectomy before the age of breast - cancer diagnosed in the case . 
we did not receive a pedigree for all participants for whom a questionnaire was available : detailed family history was available for 2706 ( 85% ) participants : 1367 ( 85% ) cases and 1339 ( 84% ) controls . 
 the mean age of breast - cancer diagnosis in cases was 405 years ( 81 ) for brca1 mutation carriers and 418 years ( 80 ) for brca2 mutation carriers . 
199 ( 12% ) cases were diagnosed by screening mammography , and 1281 ( 80% ) were diagnosed by other procedures ( usually palpation of a mass by physician or self - examination ) ; 120 ( 8% ) cases did not have information for method of diagnosis because of missing data or diagnosis by more than one method . 
 more brca2 mutation carriers were diagnosed by 404 vol 7 may 2006 articles mammo graphy compared with brca1 mutation carriers ( 77 [ 23% ] of 340 vs 122 [ 10% ] of 1260 , p < 00001 )  . 661 ( 41% ) cases and 729 ( 46% ) controls had at least one screening mammography procedure 1 year or more before the calendar year in which the case was diagnosed . 
 mean age at rst screening mammography was 353 years ( sd 78 ) for cases and 355 years ( 80 ) for controls ( p = 070 , t test )  . 
201 ( 13% ) cases and 234 ( 15% ) controls rst had mammography at age 30 years or younger ; 342 ( 21% ) cases and 355 ( 22% ) controls rst had mammography at age 3140 years ; and 118 ( 7% ) cases and 140 ( 9% ) controls rst had a mammography at age 41 years or older . 
for 760 ( 48% ) of the 1600 matched pairs , the case had her rst mammography at a younger age than the control ; for 706 ( 44% ) matched pairs , the control had her rst mammography at a younger age than the case ( p = 016 , t test ) ; and for 134 ( 8% ) matched pairs , the case and control had the same age at rst mammography or neither had mammography . after rst mammography , controls had a mean of 64 mammography procedures ( sd 038 ) every 10 years . 
 the frequency of mammography was much the same for controls who initiated the procedure in their thirties ( mean 67 [ 037 ] every 10 years ) and those who initiated it in their forties ( 68 mammograms [ 038 ] every 10 years )  . table 2 shows the association between age at rst mammography and risk of breast cancer for all women and for subgroups . 
the associations were much the same for subgroups with brca1 and brca2 mutations , and for those who were diagnosed at age 40 years or younger and at older than 40 years ( table 2 )  . 
 initiation of mammography in the thirties was associated with diagnosis of breast cancer at age 40 years or younger ( table 2 ) , but no association was noted for earlier initiation of mammography ( ie , at age 30 years , table 2 )  . 
subgroup analysis that excluded the 199 cases and their matched controls who had breast cancer identi ed by mammography showed no association between mammography and risk of breast cancer for women who had a breastcancer diagnosis by methods other than that of mammography . 
subgroup analysis showed that initiation of mammog raphy at age 3140 years was associated with an increased risk of breast - cancer diagnosis before age 40 years ; however , this nding might be due to chance . 
 we did a large study of 1600 matched pairs , and , on the basis of the 95% ci , were able to exclude an overall increase in risk associated with ever having mammography of higher than 125 . 
nevertheless , the numbers of women in some subgroups were small , and for women diagnosed with breast cancer before age 40 years , we could not exclude an increase in risk of 155 . we questioned cases and controls on the total number of mammography procedures they had had until the date of questionnaire completion , but we did not record the date of every mammography , only the rst procedure . 
however , in the absence of a comprehensive review of medical records , desticntion between diagnostic mammography ( ie , that initiated in response to an abnormal breast nding ) and screening mammography ( ie , that done only for the purpose of screening ) can be di cult . 
in the study reported here , we excluded all mammography that took place in the same calendar year as diagnosis of breast cancer in cases and controls and those done in the previous year to avoid any potential misclassi cation of screening and diagnostic mammography . 
although a young woman might have mammography only for assessment of a suspicious mass ( eg , a cyst ) , and thus the procedure might not be an indicator of long - term screening behaviour , we expect that such women will be a minority . 
in our study , the mean frequency of this for controls was mammography recommendationone mammography procedure every 19 months , or about 13 mammography procedures over a surveillance period of 20 years . than less a case - control study such as that reported here would be di cult to do in the general population because women at high risk of cancer are more likely to participate in a screening programme than are women at average risk or low risk . 
such selection bias would probably be a particular problem for assess ment of the e ect of early - onset mammography , which is generally recommended only for women at high risk of breast cancer . 
by contrast , self - selection for screening by inherent risk level is probably less important for mutation carriers because the main vol 7 may 2006 articles if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology determinant of risk is the mutation . 
furthermore , self - selection to have early mammography by women with a strong family history of breast cancer would lead to a spurious positive association between mammography exposure and breast - cancer risk , and not to the null nding that we recorded . the possibility of recall bias must be assessed in a casecontrol study . 
 women who have regular screening might be more likely to be diagnosed with breast cancer than unscreened women as a result of intensi ed surveillancea situation that would result in an excess of breast cancer identi ed by screening in the women under close surveillance . 
 therefore , we repeated our analysis on women who did not have cancer identi ed by mammography , and found that these women were not at increased risk of breast cancer . 
furthermore , only 199 ( 12% ) of the 1600 cases reported that the breast cancer was diagnosed as a result of breast - cancer screening . we planned this study on the premise that radiation exposure from a screening mammography might be su cient to raise the cancer risk in women with genetic susceptibility to the disease . 
on the basis of the similarities of radiation - induced breast cancer and hereditary breast cancer , we have previously raised caution that such screening might be hazardous.6 our ndings reported here do not lend support to the idea that brca1 or brca2 mutation carriers are at increased risk of breast cancer after exposure to mammography . 
 other studies12 , 13 of the e ects of radiation exposure in brca carriers have been negativeie , they reported12 , 13 no increase in the risk of second primary ipsilateral or contralateral breast cancer associated with radiotherapy as treatment for a rst breast cancer . 
our data should be reassuring to women and their physicians , and suggest that mammography is not a risk factor for breast cancer in carriers of brca1 or brca2 mutations . 
the decision of whether to o er mammography screening to high - risk women should be based rst on an assessment of the sensitivity of the screening tool and the potential bene ts of early detection in this high - risk group . 
we thank anna tulman and nicole phillips ( centre for research on womens health , university of toronto , ontario , canada ) for data management . con icts of interest we declare no con icts of interest . other members of the hereditary breast cancer clinical study group austriat wagner . canadap ainsworth , a chudley , a eisen , d gilchrist , e lemire , d provencher , w meschino , e warner . israelr gershoni - baruch , e friedman , g rennert . 
 italyb pasini , c bellati . usaf couch , m daly , c eng , d fishman , b karlan , j mclennan , w mckinnon , s merajver , s neuhausen , b pasche , o olopade , m osborne , k sweet , h saal , n tung , j weitzel , m wood . re ection and reaction causation of pathophysiological changes that ultimately lead to cancer , h pylori is frequently not detectable at the time of neoplasia development.24 moreover , in a large proportion of patients with gastric cancer who were classi ed as h - pylori negative by use of routine elisa , past infection could be proved by analysis of antibodies to caga igg , which persist longer after loss of infection than do igg antibodies identi ed by conventional testing.3 , 4 di culties in the identi cation of past h - pylori infection frequently lead to an underestimation of the cancer risk attributable this bacterium.3 , 4 in 1994 , the international agency for research on cancer classi ed h pylori as a type 1 carcinogena de nite cause of human cancer.2 meimarakis and colleagues nding1 that infection with the carcinogenic bacterium is bene cial once cancer has developed seems paradoxical at rst , but might have a biological basis . 
however , the supporting evidence they provide is not convincing : the assumption that patients negative for h pylori have increased regulatory - t - cell responses in tumour tissue is biased by the use of ox40 ( tumour necrosis factor receptor superfamily member 4 ) as a mar ker of cd4 - positive , cd25positive regulatory t cells . 
although ox40 is expressed on regulatory t cells , it is not speci c for this cell type and is expressed by other types of lymphocytes such as activated type 1 and type 2 t - helper ( th ) cells.7 nevertheless , a model in which a microbe - induced immune response a ects tumour growth is plausible . 
 several physiological processes necessary for tumour devel opment , such as angiogenesis , cell survival , and tissue remodelling , are regulated by leucocytic in ltrates in the neoplastic environment , either directly or by secreted products . 
in stomach cancer , the extent of in ltration by cytotoxic t cells and natural - killer cells into the neoplasticcell nest is a signi cant predictor of patient survival.8 , 9 thus , microbe - induced in ammation might modulate antitumour immunity and a ect immune surveillance in the stomach or lymph nodes . 
this idea is consistent with the nding that h - pylori infection inhibits the progression of chemically induced gastric carcinogenesis in mice.10 vol 7 may 2006 more than 15% of all human cancer is thought to be caused by infections , some of which indirectly promote carcinogenesis through induction of chronic in ammatory states . 
in animal studies , an in ammatory response induced by h pylori is of fundamental importance for the development of bacteria - related gastric malig nant disease.11 in human beings , proin ammatory polymorphisms in cytokine genes strongly enhance cancer risk associated with h - pylori infection.12 however , once cancer has developed , persistent h - pylori infection and in ltration with some leucocyte subsets seem to correlate with a favourable prognosis . 
the results of meimarakis and colleagues1 re ect the clinical implications of this multifaceted and complex biology of infection and disease . * roland rad , christian prinz , roland m schmid 2nd department of internal medicine and gastroenterology , technical university of munich , ismaningerstr 22 , 81675 munich , germany roland.rad@lrz.tum.de we declare no con icts of interest . helicobacter pylori as a prognostic indicator after curative resection of gastric carcinoma : a prospective study . 
is helicobacter pylori infection a necessary condition for noncardia gastric cancer ? am j epidemiol 2004 ; 159 : 25258 . uemura n , okamoto s , yamamoto s , et al . 
lancet oncol 2006 ; 7 : 29596the fourth sentence in the third paragraph should have read : exposure to carbon - black particles occurs mainly in the form of aggregates ( ie , particle size , 50600 nm ) and agglomerates ( 27 m )  . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology re ection and reaction debate . 
patients preferences for adjuvant chemotherapy in early stage breast cancer : is treatment available ? br j cancer 2001 ; 84 : 155785 . palda va , llewellyn - thomas ha , mackenzie rg , et al . 
clin therap 1998 ; 20 : c2025 . 14 cruzan v director , missouri department of health , 497 vs 261 : 1990 . errata migliorati ca , siegel ma , elting ls . 
in this personal view , the fth sentence of the second paragraph in the future directions section ( p 512 ) should have read : yet , in bisphosphonate - associated osteonecrosis , the maxilla is a ected much more than it is in osteoradionecrosis , suggesting occurrence of a di erent form of vascular pathogenesis or other mechanism . sobrero a , khne c - h . 
in this debate , the fourth sentence of the last paragraph in the argument for the proposal ( p 516 ) should have read : however , these data also mean that in patients who will probably relapse with no adjuvant treatment , one in ve will not relapse with uorouracil and leucovorin and one in three will not relapse with adjuvant folfox . azizi aa , haberler c , czech t , et al . 
in this case report , the rst sentence of the fth paragraph ( p 522 ) should have read : restaging in october , 2004 , revealed progression of the 15 known lesions as well as 12 new pulmonary lesions ( gure 2a , c )  . vol 7 july 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology re ection and reaction study , patients were treated in many centres worldwide without a speci c histopathological protocol . 
therefore , our results seem applicable to the community at large . unfortunately , several known risk factors were not reported in many patients , and cross - tabulations showed di erences in the three treatment groups for detection method ( p = 0001 ) , tumour size ( p = 0002 ) , tumour grade ( p = 004 ) , margin status ( p < 00001 ) , and oestrogen receptor status ( p = 006 )  . 
when comparing patients receiving radiotherapy who were given boost with those who were not , we found that the distribution for detection method tumour grade , or oestrogen receptor status was very similar between the two groups . 
as expected , patients with a boost had more tumours of unknown size ( 49% vs 31% ) , and unknown margin ( 43% vs 25% ) than patients who did not receive a boost . 
for example , in the european organisation for research and treatment of cancer ( eortc ) study , poor di erentiation was ( illogically ) better in terms of local recurrence than intermediate di erentiation in multivariate analysis.2 as in our study , age , margin status , and radiotherapy were important variables , and the researchers concluded that young women and those with involved margins are at high risk of local recurrence , even after radiotherapy with 50 gy.2 we know that young women are at high risk for local failure , so why shouldnt we use a boost with a proven bene t3 to improve the results in dcis too ? furthermore , boost radiotherapy was well - tolerated in the eortc study , 3 with only 1% severe breast brosis ( similar to that in the standard group ) and led to only a small reduction in excellent or good cosmesis . in our retrospective study , a boost was probably given more often in the presence of adverse prognostic factors . 
i agree that results might have been even better with a radiotherapeutic quality programme , and that an improved de nition of the exact boost volume might have been achieved . our results indicate the situation in invasive breast cancer , and in the absence of other data , they justify boost radiotherapy in young patients with dcis . 
the attainment of level 1 evidence from adequately powered randomised trials with a quality assurance programme is desirable , and future research by the international breast cancer study group ( ibcsg ) and eortc might one day address this . 
the question of which treatment should be used as standard is debatable , but we think boost treatment is the most promising strategy . guenther gruber coordinator of the radiation oncology task force , ibcsg international breast cancer study group , institute of radiation oncology , kantonsspital , aarau , switzerland guenther.gruber@ksa.ch i declare no con icts of interest . omlin a , amichetti m , azria d , et al . 
breast - conserving treatment with or without radiotherapy in ductal carcinoma in situ : ten - year results of european organisation for research and treatment of cancer randomized phase iii trial 10853a study by the eortc breast cancer cooperative group and eortc radiotherapy group . 
in table 6 of this health - care research article ( p 592 ) , the estimated demand for megavoltage machines in 2002 for chile should have read 44 , and the total estimated demand for megavoltage machines in 2002 should have read 1060 . douillard j - y , rosell r , de lena m , et al . 
adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ibiiia non - smallcell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
the a liation for v lorusso should have read irccs oncologico , bari , italy ( v lorusso md ) in the author address list ( p 719 ) and m de lena , v lorusso ( irccs oncologico , bari ) in the investigator list ( p 726 )  . 
in the investigator list ( p 726 ) , e massa ( policlinico universitario , cagliari ) should have read g mantovani , e massa ( policlinico universitario , cagliari )  . gajjar a , chintagumpala m , ashley d , et al . 
risk - adapted craniospinal radiotherapy followed by high - dose chemotherapy and stem - cell rescue in children with newly diagnosed medulloblastoma ( st jude medulloblastoma96 ) : long - term results from a prospective , multicentre trial . 
the fourth sentence of the second paragraph in the results ( p 816 ) should have read : 5 - year event - free survival was 66% ( 4883 ) for the 42 patients with metastatic disease and 63% ( 4483 ) for the 33 patients with m23 disease . vol 7 october 2006 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology article appearing in the lancet oncology . 
in this article , the co - author magdalena b lasota should have been written as magdalena bielska - lasota . 868 vol 8 october 2007 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology shows that change in breast appearance and palpable induration are highly sensitive to randomised dose.1 the irradiated breast looking and feeling the same as the contralateral breast 10 years after treatment is a valid outcome for patients . 
given the / value of 30 gy for late adverse e ects , by calculation of the biological equivalent dose , his schedule is equivalent to 616 gy in 20 gy fractions , a dose expected to generate a high incidence of late normal - tissue injuries . 
kunkler should not blame the fraction size ; eight fractions of 425 gy ( total 34 gy ) would have reproduced the late adverse e ects of 50 gy in 20 gy fractions in the breast . 
the sensitivity of late normal - tissue endpoints to changes in fraction size is well established , and means that a large total dose reduction is needed when the fraction size is increased . 
the trial has su cient power , as re ected in the 95% ci for the estimate , to support the hypothesis that the fractionation sensitivity of breast cancer is similar to that of late e ects . 
 john r yarnold , soren m bentzen , joanne haviland , j roger owen department of radiotherapy , royal marsden hospital , downs road , sutton , sm2 5pt , uk john.yarnold@icr.ac.uk we declare no con icts of interest . yarnold j , ashton a , bliss j , et al . 
radiother oncol 2005 ; 75 : 917 . case reports and clinical pictures in the lancet oncology following the introduction of original research in 2005 , the lancet oncology has decided to phase out the publication of case reports and clinical pictures , because we believe their value within the journal has diminished . 
this reduction in the number of article categories will enable us to increase the amount of content in other existing sections of the journal . lidia siemaszkiewicz the lancet oncology , london nw1 7by , uk erratum owen r , ashton a , bliss jm , et al . 
e ect of radiotherapy fraction size on tumour control in patients with early - stage breast cancer after local tumour excision : long - term results of a randomised trial . 
in this article , the last sentence of the 5th paragraph in the procedures section ( p 469 ) should have read : the proportion of patients who received a boost was almost identical in all three treatment groups : 350 ( 75% ) patients for 50 gy , 348 ( 75% ) for 42.9 gy , and 353 ( 75% ) for 39 gy . 620 vol 7 august 2006 re ection and reaction recommended that , in developing a cancer plan , every country should assess its needs and resources and set priorities accordingly . 
this nding is similar to our experience in papua new guinea and suggests that the burden of cancer in developing countries and the need for radiotherapy is much greater than that estimated by the international agency for research on cancer.1 in response to williams and wakehams point that the cost of radiotherapy is too high for some sub - saharan african countries , and their reference to our cost gures for palliation , these australian gures were given to indicate the relative cost of palliative treatment . 
as we noted , the cost of radiotherapy varies substantially from place to place , with the major determinant being local workforce costs.2 finally , williams and wakeham note that reliable radiotherapy services depend on a stable electricity supply , which is certainly true for linear accelerators . 
 however , cobalt megavoltage machines are more robust ; as we state in our review , they are more suited to low - income countries . we appreciate williams and wakehams perspectives , but reiterate that our aim was to discuss the relevance and availability of radiotherapy services in low - income and middle - income countries . 
 * michael barton , michael frommer , jesmin sha q faculty of medicine , and collaboration for cancer outcomes , research and evaluation , liverpool health service , university of new south wales , liverpool bc , nsw , australia michael.barton@swsahs.nsw.gov.au we declare no con icts of interest . 
in this case report , the third sentence should have read : mri of neck , chest , abdomen , and pelvis showed enlarged lymph nodes in both the mediastinum and the left supraclavicular area ( gure 1 )  . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology 706 vol 7 september 2006 re ection and reaction recommended that , in developing a cancer plan , every country should assess its needs and resources and set priorities accordingly . 
this nding is similar to our experience in papua new guinea and suggests that the burden of cancer in developing countries and the need for radiotherapy is much greater than that estimated by the international agency for research on cancer.1 in response to williams and wakehams point that the cost of radiotherapy is too high for some sub - saharan african countries , and their reference to our cost gures for palliation , these australian gures were given to indicate the relative cost of palliative treatment . 
as we noted , the cost of radiotherapy varies substantially from place to place , with the major determinant being local workforce costs.2 finally , williams and wakeham note that reliable radiotherapy services depend on a stable electricity supply , which is certainly true for linear accelerators . 
 however , cobalt megavoltage machines are more robust ; as we state in our review , they are more suited to low - income countries . we appreciate williams and wakehams perspectives , but reiterate that our aim was to discuss the relevance and availability of radiotherapy services in low - income and middle - income countries . 
 * michael barton , michael frommer , jesmin sha q faculty of medicine , and collaboration for cancer outcomes , research and evaluation , liverpool health service , university of new south wales , liverpool bc , nsw , australia michael.barton@swsahs.nsw.gov.au we declare no con icts of interest . 
in this case report , the third sentence should have read : mri of neck , chest , abdomen , and pelvis showed enlarged lymph nodes in both the mediastinum and the left supraclavicular area ( gure 1 )  . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology 706 vol 7 september 2006 re ection and reaction debate . 
patients preferences for adjuvant chemotherapy in early stage breast cancer : is treatment available ? br j cancer 2001 ; 84 : 155785 . palda va , llewellyn - thomas ha , mackenzie rg , et al . 
clin therap 1998 ; 20 : c2025 . 14 cruzan v director , missouri department of health , 497 vs 261 : 1990 . errata migliorati ca , siegel ma , elting ls . 
in this personal view , the fth sentence of the second paragraph in the future directions section ( p 512 ) should have read : yet , in bisphosphonate - associated osteonecrosis , the maxilla is a ected much more than it is in osteoradionecrosis , suggesting occurrence of a di erent form of vascular pathogenesis or other mechanism . sobrero a , khne c - h . 
in this debate , the fourth sentence of the last paragraph in the argument for the proposal ( p 516 ) should have read : however , these data also mean that in patients who will probably relapse with no adjuvant treatment , one in ve will not relapse with uorouracil and leucovorin and one in three will not relapse with adjuvant folfox . azizi aa , haberler c , czech t , et al . 
in this case report , the rst sentence of the fth paragraph ( p 522 ) should have read : restaging in october , 2004 , revealed progression of the 15 known lesions as well as 12 new pulmonary lesions ( gure 2a , c )  . vol 7 july 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com authors reply jonathan knisely expresses concern about several features of our paper , 1 which leads him to qualify the paper and the data presented as potentially misleading and awed . 
the argument that we did not analyse data for patients in whom central pathology review did not conrm a diagnosis of low - grade glioma is incorrect because these individuals formed part of the sensitivity analysis presented in the paper . 
to cite the present who classication , the main histopathological features of anaplastic glioma are those of a diffusely inltrating astrocytoma with increased cellularity , distinct nuclear atypia , and marked mitotic activity.2 similar , far - from - precise descriptions are given to dene low - grade oligodendroglioma from their anaplastic counterparts . 
substantial variation between researchers in the area of neuro - oncology exists precisely because of such arbitrary descriptions inherent to microscopic classication of brain tumours.3 , 4 i would indeed hope that an expert pathologist is involved in the routine care of patients with glioma , but even these specialists might disagree with each other . 
we need trials instead of speculation : for too long treatment of this disease has been dominated by expert opinion . martin van den bent , on behalf of the eortc 22845 trialists department of neuro - oncology , daniel den hoed oncology centre , rotterdam , the netherlands m.vandenbent@erasmusmc.nl i declare no conicts of interest . van den bent mj , afra d , de witte o , et al . 
fertility preservation for young patients with cancer : who is at risk and what can be offered ? lancet oncol 2005 ; 6 : 20918sections on the preservation of male fertility and on the ethics of fertility preservation in this review had substantial similarity with that of a previously published paper . 
asian j andol 2003 ; 5 : 32537 . vol 6 december 2005 reection and reaction information , how will individuals who give broad and future consent know that ethics review boards only approved research that met the conditions of this consent approach ? will an independent organisation be in place to ensure that the conditions are met ? for example , national legislation in estonia for the estonian genome project requires that a governing board be established to monitor the biobanks activities ; an independent national ethics committee provides general ethical oversight of the biobank.5 in the uk , the ethics and governance council , which is independent structurally and nancially from the uk biobank , has been established to ensure that the biobanks activities , protocol , and procedures comply with the projects ethics governance framework.5 both these projects require individuals to give blanket consent for future use of their biobank samples . the condentiality of personal legitimacy of alternative - consent approaches hinges on the adequacy of governance mechanisms to information , protect facilitate withdrawal of consent , and ensure that ethics review boards full their obligation to approve only studies that meet the conditions of these models . accountability , transparency , and proper monitoring are crucial to maintain public trust in biobank research , 5 especially individuals give consent for future research with their biobank samples before an ethics review board has approved specic studies . 
whether oversight mechanisms such as those for the estonian genome project and the uk biobank will ensure that alternative consent approaches do not undermine public trust in biobank research or render the principle of informed consent meaningless remains to be seen . karen j maschke the hastings center , 21 malcolm gordon road , garrison , new york , ny 10524 - 5555 , usa maschkek@thehastingscenter.org i declare no conicts of interest . hansson mg , dillner j , bartram cr , et al . 
research involving human biological materials : ethical issues and policy guidance , vol 1 : report and recommendations of the national bioethics advisory commission . rockville , md : national bioethics advisory commission , 1999 . 
protracted remission of metastatic epithelioid angiosarcoma with weekly infusion of doxorubicin , paclitaxel , and cisplatlancet oncol 2006 ; 7 : 9293the third paragraph should have read : the patient began hormone - ablative treatment with a monthly injection of 75 mg leuporelin intramuscularly for 3 months . al - terkait f , charalambous h . 
lancet oncol 2006 ; 7 : 188the third line should have read : resection of low anterior rectal cancer . if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com vol 7 march 2006 re ection and reaction parameters and does not incorporate non - carcinoma variables , such as concomitant illnesses , which could also a ect patient outcome.2 however , in the midst of such uncertainty , fuzzy logic could have an important role in the decision - making process . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
in this review , the labelling of the four histological images in gure 2 should have been ( from left to right ) : dfsp , dsrct , mfh , and leio . 670 vol 8 august 2007 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com anne szarewski cancer research uk centre for epidemiology , mathematics , and statistics , wolfson institute of preventive medicine , london ec1m 6bq , uk anne.szarewski@cancer.org.uk i have been sponsored by various pharmaceutical companies that manufacture contraceptive drugs to attend or lecture at many conferences , to give expert testimonies , or to act in a consultancy capacity . 
london : chapman and hall , 1991 . authors reply iarc thanks samuel shapiro and anne szarewski for their remarks regarding the policy watch article on combined oestrogenprogestagen contraceptives and menopausal treatment.1 samuel shapiro participated in the monograph meeting at our invitation , and the discussions beneted from his knowledge . 
according to iarc rules , samuel shapiro did not participate in the assessments because of the conict of interest he declared before the meeting . samuel shapiro believes that the working group was restricted from the assessment of evidence for the carcinogenicity of oestrogen - only or progestagen - only products . 
all iarc working groups are free to consider any published studies they regard as pertinent , and iarc made the previous monograph on single - ingredient products2 available to the working group . 
however , the effects of combined oestrogen and progestagen products are complex , and to extrapolate from studies of singleingredient products to predict the carcinogenicity of combined products would have been difcult . 
the working group noted , for example , that the increased risk of breast cancer is higher with combined menopausal treatment than with oestrogen - only menopausal treatment , and that the increased risk of endometrial cancer with combined treatment depends on the number of days per cycle progestagens are taken . epidemiological studies on the combined products themselves were more informative in assessing their carcinogenicity and consequently the working group decided to specically focus on these studies . 
carcinogenicity of combined oestrogenprogestagen contraceptives and menopausal treatment . lancet oncol 2005 ; 6 : 55253 . iarc monographs on the evaluation of carcinogenic risks to humans , volume 72 , hormonal contraception and post - menopausal hormonal therapy . 
lancet oncol 2005 ; 6 : 263the rst sentence of the second paragraph should read : in the rst study , researchers from mayo clinic ( rochester , mn , usa ) analysed survival of 842 patients who had radical prostatectomy for ct3 prostate cancer . vol 6 october 2005 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology used in a more procedure - speci c assessment , such as in patients with colorectal cancer.2 , 3 this drawback has promoted the development of potentially more speci c scales , such as the colorectal possum ( cr - possum ) , which aims to predict more accurately the mortality associated with colorectal surgical procedures.4 in this issue of the lancet oncology , ferjani and colleagues5 compare a recently created speci c colorectal scoring system , developed by use of the association of coloproctology of great britain and ireland ( acpgbi ) database and named the acpgbi score , 6 with all of the above - mentioned scoring systems . 
the acpgbi scoring system is simpler to calculate than the other scoring systems , as it incorporates only ve operative variables rather than the 1218 variables of the other systems . 
the researchers postulate that this focused colorectal surgery mortality score would probably be more accurate in predicting mortality in patients undergoing surgery for colorectal cancer than the more general scoring scales . 
 ferjani and co - workers prospectively assessed all patients who underwent major surgical procedures for colorectal cancer at a single institution during the 3 - year period of 20022005 and compared the reported mortality with the predicted mortality based on the four separate scoring systems ( possum , p - possum , cr - possum , and acpgbi ) to assess their accuracy . 
in this study , the observed ( actual ) versus expected ( predicted ) mortality in 618 patients was analysed and compared by the various scoring systems with the actual reported overall mortality of 102% ( 95% ci 80129 )  . 
cr - possum gave the most accurate prediction for emergency cases and cases done by noncolorectal surgeons , whereas acpgbi gave better accuracy in elective cases and for cases done only by colorectal surgeons . 
 in discussing variance between scoring systems in di erent studies , 2 , 4 , 6 we should note they span di e rent decades and might not be entirely comparable . 
however , a criticism of the present study is the pur p ose ful exclusion of laparoscopic colorectal cancer pro cedures given the inc reasing use of this technique in colorectal cancer surgery . 
additionally , geo graphically speci c practice norms have the potential to a ect predictions ; in this instance , the acpgbi is a uk - based system that has not yet been valid ated for populations outside of the uk and , as such , its applicability to other health - care systems is not yet de ned . ferjani and colleagues have done a valuable study assessing prospectively an established scoring system that is focused on colorectal surgerythe acpgbi scoring systethe importance of developing such scoring indices is becoming more and more apparent as medicine as a whole becomes more data - driven . 
finally , although more focused scoring scales might ultimately prove to be the most accurate , the inevitable locoregional variation in di erent pop ulations and di erent medical systems might make it impossible for one single scoring system to be all - encompassing . madeleine poirier , n joseph espat * maisonneuve - rosemont hospital , montreal , quebec , canada ( mp ) ; hepatobiliary and oncologic surgery , university of illinois at chicago , chicago , il , usa ( nje ) jespat@uic.edu the authors declared no con icts of interest tez m , yoldas o , gocmen e , et al . 
on page 268 the last sentence of the rst paragraph of the second column should have read : the patient information sheets are now being reviewed to re ect the revised policy , in which surgeons are asked not to modify procedures carried out as part of the routine care of the child in order to obtain extra tissue for ukccsg tumour bank . vol 8 april 2007 reection and reaction if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com unfortunately , this benet will not be realised from meta - analyses because of the absence of stage stratication in existing studies . 
we agree that the use of endoluminal ultrasonography and possibly pet should be a requirement to stratify patients in future randomised trials of preoperative treatment oesophageal cancer . * bryan h burmeister , b mark smithers university of queensland , princess alexandra hospital , brisbane , 4102 , australia bryan_burmeister@health.qld.gov.au i declare no conicts of interest . burmeister bh , smithers bm , gebski v , et al . 
a step too far ? lancet oncol 2005 ; 6 : 731the rst sentence should have read on sept 13 , 2005 , the scottish medicines consortium ( smc ) approved anastrozole for postmenopausal women with early - stage invasive breast cancer . vol 6 november 2005 re ection and reaction study , patients were treated in many centres worldwide without a speci c histopathological protocol . 
therefore , our results seem applicable to the community at large . unfortunately , several known risk factors were not reported in many patients , and cross - tabulations showed di erences in the three treatment groups for detection method ( p = 0001 ) , tumour size ( p = 0002 ) , tumour grade ( p = 004 ) , margin status ( p < 00001 ) , and oestrogen receptor status ( p = 006 )  . 
when comparing patients receiving radiotherapy who were given boost with those who were not , we found that the distribution for detection method tumour grade , or oestrogen receptor status was very similar between the two groups . 
as expected , patients with a boost had more tumours of unknown size ( 49% vs 31% ) , and unknown margin ( 43% vs 25% ) than patients who did not receive a boost . 
for example , in the european organisation for research and treatment of cancer ( eortc ) study , poor di erentiation was ( illogically ) better in terms of local recurrence than intermediate di erentiation in multivariate analysis.2 as in our study , age , margin status , and radiotherapy were important variables , and the researchers concluded that young women and those with involved margins are at high risk of local recurrence , even after radiotherapy with 50 gy.2 we know that young women are at high risk for local failure , so why shouldnt we use a boost with a proven bene t3 to improve the results in dcis too ? furthermore , boost radiotherapy was well - tolerated in the eortc study , 3 with only 1% severe breast brosis ( similar to that in the standard group ) and led to only a small reduction in excellent or good cosmesis . in our retrospective study , a boost was probably given more often in the presence of adverse prognostic factors . 
i agree that results might have been even better with a radiotherapeutic quality programme , and that an improved de nition of the exact boost volume might have been achieved . our results indicate the situation in invasive breast cancer , and in the absence of other data , they justify boost radiotherapy in young patients with dcis . 
the attainment of level 1 evidence from adequately powered randomised trials with a quality assurance programme is desirable , and future research by the international breast cancer study group ( ibcsg ) and eortc might one day address this . 
the question of which treatment should be used as standard is debatable , but we think boost treatment is the most promising strategy . guenther gruber coordinator of the radiation oncology task force , ibcsg international breast cancer study group , institute of radiation oncology , kantonsspital , aarau , switzerland guenther.gruber@ksa.ch i declare no con icts of interest . omlin a , amichetti m , azria d , et al . 
breast - conserving treatment with or without radiotherapy in ductal carcinoma in situ : ten - year results of european organisation for research and treatment of cancer randomized phase iii trial 10853a study by the eortc breast cancer cooperative group and eortc radiotherapy group . 
in table 6 of this health - care research article ( p 592 ) , the estimated demand for megavoltage machines in 2002 for chile should have read 44 , and the total estimated demand for megavoltage machines in 2002 should have read 1060 . douillard j - y , rosell r , de lena m , et al . 
adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ibiiia non - smallcell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
the a liation for v lorusso should have read irccs oncologico , bari , italy ( v lorusso md ) in the author address list ( p 719 ) and m de lena , v lorusso ( irccs oncologico , bari ) in the investigator list ( p 726 )  . 
in the investigator list ( p 726 ) , e massa ( policlinico universitario , cagliari ) should have read g mantovani , e massa ( policlinico universitario , cagliari )  . gajjar a , chintagumpala m , ashley d , et al . 
risk - adapted craniospinal radiotherapy followed by high - dose chemotherapy and stem - cell rescue in children with newly diagnosed medulloblastoma ( st jude medulloblastoma96 ) : long - term results from a prospective , multicentre trial . 
the fourth sentence of the second paragraph in the results ( p 816 ) should have read : 5 - year event - free survival was 66% ( 4883 ) for the 42 patients with metastatic disease and 63% ( 4483 ) for the 33 patients with m23 disease . vol 7 october 2006 reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
 for example , the poster competition alone has resulted in nearly 100 submissions from 22 di erent countries , 74% of which report on research being done by groups in asia . 
furthermore , by drawing on the knowledge of a faculty of over 40 world - renowned speakers , the forum will focus on the ten most prevalent cancers in the asiapaci c region and will examine aspects of prevention , diagnosis , treatment , and palliation . 
opinion - leaders will discuss cancer aetiology , health - care systems , and the challenges of providing e ective disease management with limited resources , along with views on state - ofthe - art treatments in the areas of diagnostics , medical oncology , radiotherapy , and surgical oncology . 
finally , the forum will also host a didactic workshop on how to run a clinical trial ; a poster display of ongoing research relevant to asia ; and a poster discussion session in which authors of the three posters judged most in uential will have an opportunity to present their work orally . 
in this case report the second sentence of the rst paragraph ( she was given sirolimus and had complete remission of the disease . ) was included by error and should be ignored . 
additionally , the fth sentence of the second paragraph should have read : after a loading dose of 10 mg sirolimus , she received sirolimus once a day ; sirolimus doses were titrated to a trough sirolimus concentration of 512 ng / ml , attaining a nal maintenance dose of 2 mg once a day starting in may , 2004 . gerhard opelz , volker daniel , cord naujokat , et al . 
in this article the anti - epstein - barr virus immunoglobulin g reactivity should have read : 7735 1475 u / ml ( sandoglobulin ) , 1600 71 u / ml ( cytotect ) , and 1425 249 u / ml ( cytogam ) , as extrapolated from the results obtained at a one to ten dilution ( dade behring )  . vol 8 march 2007 reection and reaction sung jj , lau jy , goh kl , leung wk . 
prevalence and distinctive biologic features of at colorectal adenomas in a north american population . gastroenterology 2001 ; 120 : 165765 . muto t , kamiya j , sawada t , et al . 
dis colon rectum 2004 ; 47 : 146266 . flat and depressed tumour supercial tumour without or with depression of the surface polypoid pedunculated or sessile errata acharya s , hensley ml , montag ac , fleming gf . 
head circumference at birth linked to cancer in childhood . lancet oncol 2006 ; 7 : 45reference 1 should read : samuelsen so , bakketeig ls , tretli s , et al . 
 with regard to at and depressed colorectal tumours , sung and colleagues1 stated that : there have been few reports of at and de - novo tumours from western populations , except for one study from the uk , 5 and concluded that whether this feature is unique to eastern populations or merely reects underdiagnosis of the lesion in the west is not clear . however , a study6 by a japanese endoscopist in the usa showed that at and depressed lesions were found in up to 23% of the us patients who had dyeassisted colonoscopy . 
whether oversight mechanisms such as those for the estonian genome project and the uk biobank will ensure that alternative consent approaches do not undermine public trust in biobank research or render the principle of informed consent meaningless remains to be seen . karen j maschke the hastings center , 21 malcolm gordon road , garrison , new york , ny 10524 - 5555 , usa maschkek@thehastingscenter.org i declare no conicts of interest . hansson mg , dillner j , bartram cr , et al . 
research involving human biological materials : ethical issues and policy guidance , vol 1 : report and recommendations of the national bioethics advisory commission . rockville , md : national bioethics advisory commission , 1999 . 
protracted remission of metastatic epithelioid angiosarcoma with weekly infusion of doxorubicin , paclitaxel , and cisplatlancet oncol 2006 ; 7 : 9293the third paragraph should have read : the patient began hormone - ablative treatment with a monthly injection of 75 mg leuporelin intramuscularly for 3 months . al - terkait f , charalambous h . 
lancet oncol 2006 ; 7 : 188the third line should have read : resection of low anterior rectal cancer . if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com vol 7 march 2006 reection and reaction information , how will individuals who give broad and future consent know that ethics review boards only approved research that met the conditions of this consent approach ? will an independent organisation be in place to ensure that the conditions are met ? for example , national legislation in estonia for the estonian genome project requires that a governing board be established to monitor the biobanks activities ; an independent national ethics committee provides general ethical oversight of the biobank.5 in the uk , the ethics and governance council , which is independent structurally and nancially from the uk biobank , has been established to ensure that the biobanks activities , protocol , and procedures comply with the projects ethics governance framework.5 both these projects require individuals to give blanket consent for future use of their biobank samples . the condentiality of personal legitimacy of alternative - consent approaches hinges on the adequacy of governance mechanisms to information , protect facilitate withdrawal of consent , and ensure that ethics review boards full their obligation to approve only studies that meet the conditions of these models . accountability , transparency , and proper monitoring are crucial to maintain public trust in biobank research , 5 especially individuals give consent for future research with their biobank samples before an ethics review board has approved specic studies . 
whether oversight mechanisms such as those for the estonian genome project and the uk biobank will ensure that alternative consent approaches do not undermine public trust in biobank research or render the principle of informed consent meaningless remains to be seen . karen j maschke the hastings center , 21 malcolm gordon road , garrison , new york , ny 10524 - 5555 , usa maschkek@thehastingscenter.org i declare no conicts of interest . hansson mg , dillner j , bartram cr , et al . 
research involving human biological materials : ethical issues and policy guidance , vol 1 : report and recommendations of the national bioethics advisory commission . rockville , md : national bioethics advisory commission , 1999 . 
protracted remission of metastatic epithelioid angiosarcoma with weekly infusion of doxorubicin , paclitaxel , and cisplatlancet oncol 2006 ; 7 : 9293the third paragraph should have read : the patient began hormone - ablative treatment with a monthly injection of 75 mg leuporelin intramuscularly for 3 months . al - terkait f , charalambous h . 
lancet oncol 2006 ; 7 : 188the third line should have read : resection of low anterior rectal cancer . if you would like to respond to an article published in the lancet oncology , please email your submission to the editor at : david.collingridge@lancet.com vol 7 march 2006 re ection and reaction debate . 
patients preferences for adjuvant chemotherapy in early stage breast cancer : is treatment available ? br j cancer 2001 ; 84 : 155785 . palda va , llewellyn - thomas ha , mackenzie rg , et al . 
clin therap 1998 ; 20 : c2025 . 14 cruzan v director , missouri department of health , 497 vs 261 : 1990 . errata migliorati ca , siegel ma , elting ls . 
in this personal view , the fth sentence of the second paragraph in the future directions section ( p 512 ) should have read : yet , in bisphosphonate - associated osteonecrosis , the maxilla is a ected much more than it is in osteoradionecrosis , suggesting occurrence of a di erent form of vascular pathogenesis or other mechanism . sobrero a , khne c - h . 
in this debate , the fourth sentence of the last paragraph in the argument for the proposal ( p 516 ) should have read : however , these data also mean that in patients who will probably relapse with no adjuvant treatment , one in ve will not relapse with uorouracil and leucovorin and one in three will not relapse with adjuvant folfox . azizi aa , haberler c , czech t , et al . 
in this case report , the rst sentence of the fth paragraph ( p 522 ) should have read : restaging in october , 2004 , revealed progression of the 15 known lesions as well as 12 new pulmonary lesions ( gure 2a , c )  . vol 7 july 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology used in a more procedure - speci c assessment , such as in patients with colorectal cancer.2 , 3 this drawback has promoted the development of potentially more speci c scales , such as the colorectal possum ( cr - possum ) , which aims to predict more accurately the mortality associated with colorectal surgical procedures.4 in this issue of the lancet oncology , ferjani and colleagues5 compare a recently created speci c colorectal scoring system , developed by use of the association of coloproctology of great britain and ireland ( acpgbi ) database and named the acpgbi score , 6 with all of the above - mentioned scoring systems . 
the acpgbi scoring system is simpler to calculate than the other scoring systems , as it incorporates only ve operative variables rather than the 1218 variables of the other systems . 
the researchers postulate that this focused colorectal surgery mortality score would probably be more accurate in predicting mortality in patients undergoing surgery for colorectal cancer than the more general scoring scales . 
 ferjani and co - workers prospectively assessed all patients who underwent major surgical procedures for colorectal cancer at a single institution during the 3 - year period of 20022005 and compared the reported mortality with the predicted mortality based on the four separate scoring systems ( possum , p - possum , cr - possum , and acpgbi ) to assess their accuracy . 
in this study , the observed ( actual ) versus expected ( predicted ) mortality in 618 patients was analysed and compared by the various scoring systems with the actual reported overall mortality of 102% ( 95% ci 80129 )  . 
cr - possum gave the most accurate prediction for emergency cases and cases done by noncolorectal surgeons , whereas acpgbi gave better accuracy in elective cases and for cases done only by colorectal surgeons . 
 in discussing variance between scoring systems in di erent studies , 2 , 4 , 6 we should note they span di e rent decades and might not be entirely comparable . 
however , a criticism of the present study is the pur p ose ful exclusion of laparoscopic colorectal cancer pro cedures given the inc reasing use of this technique in colorectal cancer surgery . 
additionally , geo graphically speci c practice norms have the potential to a ect predictions ; in this instance , the acpgbi is a uk - based system that has not yet been valid ated for populations outside of the uk and , as such , its applicability to other health - care systems is not yet de ned . ferjani and colleagues have done a valuable study assessing prospectively an established scoring system that is focused on colorectal surgerythe acpgbi scoring systethe importance of developing such scoring indices is becoming more and more apparent as medicine as a whole becomes more data - driven . 
finally , although more focused scoring scales might ultimately prove to be the most accurate , the inevitable locoregional variation in di erent pop ulations and di erent medical systems might make it impossible for one single scoring system to be all - encompassing . madeleine poirier , n joseph espat * maisonneuve - rosemont hospital , montreal , quebec , canada ( mp ) ; hepatobiliary and oncologic surgery , university of illinois at chicago , chicago , il , usa ( nje ) jespat@uic.edu the authors declared no con icts of interest tez m , yoldas o , gocmen e , et al . 
on page 268 the last sentence of the rst paragraph of the second column should have read : the patient information sheets are now being reviewed to re ect the revised policy , in which surgeons are asked not to modify procedures carried out as part of the routine care of the child in order to obtain extra tissue for ukccsg tumour bank . vol 8 april 2007 re ection and reaction debate . 
patients preferences for adjuvant chemotherapy in early stage breast cancer : is treatment available ? br j cancer 2001 ; 84 : 155785 . palda va , llewellyn - thomas ha , mackenzie rg , et al . 
clin therap 1998 ; 20 : c2025 . 14 cruzan v director , missouri department of health , 497 vs 261 : 1990 . errata migliorati ca , siegel ma , elting ls . 
in this personal view , the fth sentence of the second paragraph in the future directions section ( p 512 ) should have read : yet , in bisphosphonate - associated osteonecrosis , the maxilla is a ected much more than it is in osteoradionecrosis , suggesting occurrence of a di erent form of vascular pathogenesis or other mechanism . sobrero a , khne c - h . 
in this debate , the fourth sentence of the last paragraph in the argument for the proposal ( p 516 ) should have read : however , these data also mean that in patients who will probably relapse with no adjuvant treatment , one in ve will not relapse with uorouracil and leucovorin and one in three will not relapse with adjuvant folfox . azizi aa , haberler c , czech t , et al . 
in this case report , the rst sentence of the fth paragraph ( p 522 ) should have read : restaging in october , 2004 , revealed progression of the 15 known lesions as well as 12 new pulmonary lesions ( gure 2a , c )  . vol 7 july 2006 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology re ection and reaction parameters and does not incorporate non - carcinoma variables , such as concomitant illnesses , which could also a ect patient outcome.2 however , in the midst of such uncertainty , fuzzy logic could have an important role in the decision - making process . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
in this review , the labelling of the four histological images in gure 2 should have been ( from left to right ) : dfsp , dsrct , mfh , and leio . 670 vol 8 august 2007 re ection and reaction study , patients were treated in many centres worldwide without a speci c histopathological protocol . 
therefore , our results seem applicable to the community at large . unfortunately , several known risk factors were not reported in many patients , and cross - tabulations showed di erences in the three treatment groups for detection method ( p = 0001 ) , tumour size ( p = 0002 ) , tumour grade ( p = 004 ) , margin status ( p < 00001 ) , and oestrogen receptor status ( p = 006 )  . 
when comparing patients receiving radiotherapy who were given boost with those who were not , we found that the distribution for detection method tumour grade , or oestrogen receptor status was very similar between the two groups . 
as expected , patients with a boost had more tumours of unknown size ( 49% vs 31% ) , and unknown margin ( 43% vs 25% ) than patients who did not receive a boost . 
for example , in the european organisation for research and treatment of cancer ( eortc ) study , poor di erentiation was ( illogically ) better in terms of local recurrence than intermediate di erentiation in multivariate analysis.2 as in our study , age , margin status , and radiotherapy were important variables , and the researchers concluded that young women and those with involved margins are at high risk of local recurrence , even after radiotherapy with 50 gy.2 we know that young women are at high risk for local failure , so why shouldnt we use a boost with a proven bene t3 to improve the results in dcis too ? furthermore , boost radiotherapy was well - tolerated in the eortc study , 3 with only 1% severe breast brosis ( similar to that in the standard group ) and led to only a small reduction in excellent or good cosmesis . in our retrospective study , a boost was probably given more often in the presence of adverse prognostic factors . 
i agree that results might have been even better with a radiotherapeutic quality programme , and that an improved de nition of the exact boost volume might have been achieved . our results indicate the situation in invasive breast cancer , and in the absence of other data , they justify boost radiotherapy in young patients with dcis . 
the attainment of level 1 evidence from adequately powered randomised trials with a quality assurance programme is desirable , and future research by the international breast cancer study group ( ibcsg ) and eortc might one day address this . 
the question of which treatment should be used as standard is debatable , but we think boost treatment is the most promising strategy . guenther gruber coordinator of the radiation oncology task force , ibcsg international breast cancer study group , institute of radiation oncology , kantonsspital , aarau , switzerland guenther.gruber@ksa.ch i declare no con icts of interest . omlin a , amichetti m , azria d , et al . 
breast - conserving treatment with or without radiotherapy in ductal carcinoma in situ : ten - year results of european organisation for research and treatment of cancer randomized phase iii trial 10853a study by the eortc breast cancer cooperative group and eortc radiotherapy group . 
in table 6 of this health - care research article ( p 592 ) , the estimated demand for megavoltage machines in 2002 for chile should have read 44 , and the total estimated demand for megavoltage machines in 2002 should have read 1060 . douillard j - y , rosell r , de lena m , et al . 
adjuvant vinorelbine plus cisplatin versus observation in patients with completely resected stage ibiiia non - smallcell lung cancer ( adjuvant navelbine international trialist association [ anita ] ) : a randomised controlled trial . 
the a liation for v lorusso should have read irccs oncologico , bari , italy ( v lorusso md ) in the author address list ( p 719 ) and m de lena , v lorusso ( irccs oncologico , bari ) in the investigator list ( p 726 )  . 
in the investigator list ( p 726 ) , e massa ( policlinico universitario , cagliari ) should have read g mantovani , e massa ( policlinico universitario , cagliari )  . gajjar a , chintagumpala m , ashley d , et al . 
risk - adapted craniospinal radiotherapy followed by high - dose chemotherapy and stem - cell rescue in children with newly diagnosed medulloblastoma ( st jude medulloblastoma96 ) : long - term results from a prospective , multicentre trial . 
the fourth sentence of the second paragraph in the results ( p 816 ) should have read : 5 - year event - free survival was 66% ( 4883 ) for the 42 patients with metastatic disease and 63% ( 4483 ) for the 33 patients with m23 disease . vol 7 october 2006 re ection and reaction parameters and does not incorporate non - carcinoma variables , such as concomitant illnesses , which could also a ect patient outcome.2 however , in the midst of such uncertainty , fuzzy logic could have an important role in the decision - making process . 
instead of assuming everything must be de ned in to black and white ( binary view ) , fuzzy logic is a method that captures and uses the concept of fuzziness in a computationally e ective manner . 
 the combination of neural networks and fuzzy logic has created a new term , a neurofuzzy systeneural networks , fuzzy systems , and the combination of both have already been successfully applied to computer - aided diagnosis eg , detection of microcalci cation , auto matic detection of distorted plethysmogram pulses in neonates and paediatric patients , detection of erythematosquamous diseases , and lung - nodule detectionand have been useful for predicting the presence of prostate cancer.3 , 4 resulting in parameters , slight variations from measurement errors , can change the tnm classi cation . 
 for example , neurofuzzy systems can incorporate data from many clinical , pathological , biological , and genetic variables . * mesut tez , selda tez department of general surgery , gazi university school of medicine , ankara , turkey ( mt ) ; department of radiology , 29 mayis hospital , ankara , turkey ( st ) mesuttez@yahoo.com the authors declared no con icts of interest . quirke p , williams gt , ectors n , ensari a , piard f , nagtegaal i . 
the future of the tnm staging system in colorectal cancer : time for a debate ? lancet oncol 2007 ; 8 : 65157 . sato f , shimada y , selaru fm , et al . 
urology 2006 ; 68 : 35761 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata blackhall f , ranson m , thatcher n . 
in this review , the rst sentence of the second paragraph in the erlotinib in nsclc section ( p 501 ) should have read : consistent with the intact trials , 24 , 25 the results for similarly designed trials of erlotinib26 , 27 in combination with chemotherapy were negative . 
in this world focus , the second sentence of the rst paragraph on page 372 should have read : championed by the programme for appropriate technology ( path ) , a sociocultural study has been launched in uganda on the feasibility of vaccinating girls against human papilloma virus ( hpv ) , the results of which could lead to the eventual vaccination of all girls with a course of three injections . 
the rst sentence of the fourth paragraph ( p 372 ) , the rst sentence of the last paragraph ( p 372 ) , and the rst sentence of the 16th paragraph ( p 373 ) should have referred to the feasibility study . 
the rst sentence of the second paragraph in the second column on page 373 should have read : therefore , the future trial of a vaccine that targets hpv 16 and 18 is unlikely to yield results consistent enough upon which a national full - scale vaccination programme can be based . 
in this article , in gure 3b on page 494 , the hazard ratio for study 16 should be 085 , and for study 17 should be 119 . wunder t , nielsen to , maki rg , osullivan b , alman ba . 
in this review , the labelling of the four histological images in gure 2 should have been ( from left to right ) : dfsp , dsrct , mfh , and leio . 670 vol 8 august 2007 re ection and reaction richard g grundy childrens brain tumour research centre , university of nottingham , the medical school , queens medical centre , nottingham ng7 2uh , uk richard.grundy@nottingham.ac.uk the author declared no con icts of interest . grundy rg , wilne sa , weston cl , et al . 
pediatr neurosurg 1998 ; 28 : 21522 . bou et e , perilongo g , canete a , massimino m et al intracranial ependymoma in children ; a critical review of prognostic markers and a plea for cooperation . 
med pediatr oncol 1998 ; 40 : 3440 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zupancic m , shah pc , shah - khan f , nagendra s . 
in this review , the author list should have read : melanie zupancic , prabodh c shah , farheen shah - khan , sanjai nagendra . grundy rg , wilne sa , weston cl , et al . 
 full total resection less than full total resection 100 075 050 025 000 numbers at risk total resection 44 partial resection 45 time from surgery ( years ) 7 figure 5 : overall survival based on neurosurgical assessment of the extent of resection at the end of surgery vol 8 september 2007 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper , clearly marked with the phrase sabcs call for papers , go to elsevier.com / thelancetoncology in the twentieth century : cure for many diseases is now available and other diseases have been rendered chronic . 
quality of life comprises physical , psychological , emotional , and spiritual issues , which are also the cornerstones of palliative medicine . palliative - care specialists face a great opportunity : to share their knowledge of integrated palliative care with other specialists , so that the latter can learn how to provide integrated care and cure . 
the more physicians are involved in the cure and care of a patient , the greater the risk that information is not shared , which might hamper good medical care . 
in breast cancer : a call for papers in many countries the probability of developing a cancer before the age of 65 years is fast approaching 15%.1 this is a substantial risk and of all cancers , breast neoplasia is the most prevalent , not only in women but also overall.1 the lancet oncology is , therefore , issuing a call for papers that will o er major advances in the management of breast cancer . 
accepted papers will be published in the lancet oncology to coincide with the san antonio breast cancer symposium ( sabcs ; tx , usa , dec 1316 , 2007 )  . 
 aacn clin issues 2005 ; 16 : 54250 . presentation at the sabcs , please let us know the precise details of the type of presentation ( such as including dates and poster or oral presentation ) , times , so that publication in the lancet oncology can be scheduled to comply with sabcss embargo policies . 
 articles should be submitted via the lancet oncologys online submission service , and all authors must clearly state in the covering letter that their submission is in response to the sabcs call for papers . 
the deadline for submissions is oct 12 , 2007 . david collingridge the lancet oncology , london nw1 7by , uk 1 mackay j , jemal a , lee nc , parkin dm . 
atlanta : american cancer society , 2006 . published online june 22 , 2007 doi : 10.1016 / s14702045 ( 07 ) 70177 - 8 see articles page 603 erratum on june 4 , 2007 , the lancet oncology published results online of the zest trial by martin stockler and colleagues.1 this was an early online publication , with print publication scheduled for the july issue . 
the argument that we did not analyse data for patients in whom central pathology review did not conrm a diagnosis of low - grade glioma is incorrect because these individuals formed part of the sensitivity analysis presented in the paper . 
to cite the present who classication , the main histopathological features of anaplastic glioma are those of a diffusely inltrating astrocytoma with increased cellularity , distinct nuclear atypia , and marked mitotic activity.2 similar , far - from - precise descriptions are given to dene low - grade oligodendroglioma from their anaplastic counterparts . 
substantial variation between researchers in the area of neuro - oncology exists precisely because of such arbitrary descriptions inherent to microscopic classication of brain tumours.3 , 4 i would indeed hope that an expert pathologist is involved in the routine care of patients with glioma , but even these specialists might disagree with each other . 
we need trials instead of speculation : for too long treatment of this disease has been dominated by expert opinion . martin van den bent , on behalf of the eortc 22845 trialists department of neuro - oncology , daniel den hoed oncology centre , rotterdam , the netherlands m.vandenbent@erasmusmc.nl i declare no conicts of interest . van den bent mj , afra d , de witte o , et al . 
fertility preservation for young patients with cancer : who is at risk and what can be offered ? lancet oncol 2005 ; 6 : 20918sections on the preservation of male fertility and on the ethics of fertility preservation in this review had substantial similarity with that of a previously published paper . 
asian j andol 2003 ; 5 : 32537 . vol 6 december 2005 articles extra - pleural pneumonectomy versus no extra - pleural pneumonectomy for patients with malignant pleural mesothelioma : clinical outcomes of the mesothelioma and radical surgery ( mars ) randomised feasibility study tom treasure , loic lang - lazdunski , david waller , judith m bliss , carol tan , james entwisle , michael snee , mary obrien , gill thomas , suresh senan , ken obyrne , lucy s kilburn , james spicer , david landau , john edwards , gill coombes , liz darlison , julian peto , for the mars trialists * summary background the e ects of extra - pleural pneumonectomy ( epp ) on survival and quality of life in patients with malignant pleural mesothelioma have , to our knowledge , not been assessed in a randomised trial . 
we aimed to assess the clinical outcomes of patients who were randomly assigned to epp or no epp in the context of trimodal therapy in the mesothelioma and radical surgery ( mars ) feasibility study . methods mars was a multicentre randomised controlled trial in 12 uk hospitals . 
the main endpoints were feasibility of randomly assigning 50 patients in 1 year ( results detailed in another report ) , proportion randomised who received treatment , proportion eligible ( registered ) who proceeded to randomisation , perioperative mortality , and quality of life . 
this trial is registered , number isrctn95583524 . findings between oct 1 , 2005 , and nov 3 , 2008 , 112 patients were registered and 50 were subsequently randomly assigned : 24 to epp and 26 to no epp . 
the main reasons for not proceeding to randomisation were disease progression ( 33 patients ) , inoperability ( ve patients ) , and patient choice ( 19 patients )  . 
the hazard ratio [ hr ] for overall survival between the epp and no epp groups was 190 ( 95% ci 092393 ; exact p = 0082 ) , and after adjustment for sex , histological subtype , stage , and age at randomisation the hr was 275 ( 121626 ; p = 0016 )  . 
 of the 49 randomly assigned patients who consented to quality of life assessment ( epp n = 23 ; no epp n = 26 ) , 12 patients in the epp group and 19 in the no epp group completed the quality of life questionnaires . 
although median quality of life scores were lower in the epp group than the no epp group , no signi cant di erences between groups were reported in the quality of life analyses . 
there were ten serious adverse events reported in the epp group and two in the no epp group . interpretation in view of the high morbidity associated with epp in this trial and in other non - randomised studies a larger study is not feasible . 
these data , although limited , suggest that radical surgery in the form of epp within trimodal therapy o ers no bene t and possibly harms patients . funding cancer research uk ( cruk / 04 / 003 ) , the june hancock mesothelioma research fund , and guys and st thomas nhs foundation trust . introduction time when deaths from malignant pleural at a mesothelioma were rising in the uk1 , 2 and europe , 3 data from the uk thoracic surgical register of the society for cardiothoracic surgery in great britain and ireland showed that few patients were being o ered surgery for their disease . 
encouraging results from large case series had been reported for extrapleural pneumonectomy ( epp ) , 47 in which the lung and ipsilateral parietal pleura , pericardium , and hemidiaphragm are resected . 
 epp = extra - pleural pneumonectomy . in 2004 , we did a systematic review to assess the available evidence for e ectiveness of epp.8 median survival ranged from 17 to 35 months in seven surgical follow - up studies reported from 1999 to 2004 . 
the available data had been reported retrospectively on the basis of completed treatment and so measurement of the extent to which survival was in uenced by epp itself rather than the initial selection of treatment and subsequent progressive continued treatment in patients with a favourable prognosis was not possible . selection for to establish the e cacy of epp , we designed the mesothelioma and radical surgery ( mars ) trial.9 epp , within the context of trimodal therapy , was to be compared with induction chemotherapy but no epp . 
at the start of the trial , a power calculation , on the basis of the di erence claimed for e ectiveness of epp8 and natural history data , 10 suggested that 670 patients would be needed to identify any statistically signi cant di erence between epp and no epp with overall survival as the primary outcome . 
because of the anticipated di culty in recruiting patients , an initial feasibility study was done with the objective of randomising 50 patients within 1 year to epp or no epp to assess patient acceptability and to gauge the potential recruitment rate that could be expected in a larger trial . 
 randomisation between groups was possible but took longer than would be feasible to recruit su cient numbers to a de nitive trial.11 here we report the survival and quality of life outcomes of mars 2 years after recruitment was completed . methods patients the mars feasibility study was a multicentre randomised controlled trial with a prerandomisation registration phase and a two - stage consent process ( gure 1 )  . 
patients were eligible for registration if they were aged 18 years or older with pathologically con rmed mesothelioma and no evidence on preoperative ct staging of unresectable disease or distant metastases . 
they also had to be deemed t enough to undergo preoperative chemotherapy followed by pneumonectomy ( according to british thoracic society criteria for lung cancer surgery ) 12 and the planned postoperative radiotherapy . after chemotherapy , patients underwent restaging by ct . 
this team was chaired by the chief investigator , coordinated by the trial team at the institute of cancer research clinical trials and statistics unit the radiologist from the trial management group , the surgical coordinator , a medical and a radiation oncologist , and the designated mars trial surgeon . 
for each patient deemed eligible by the referring clinical team , clinical data and imaging reports were circulated to mars virtual multidisciplinary team members , and a teleconference ( icr - ctsu ; sutton , uk ) and included 764 vol 12 august 2011 articles was held to provide a consensus on whether that patient should be o ered randomisation . study centres were also asked ( but were not obliged ) to complete a screening log of all patients with mesothelioma to document the eligible population and calculate the proportion who agreed to enter the registration phase of the study . 
patients who ful lled eligibility criteria and who received chemotherapy outside of the trial , but in a manner consistent with the protocol , could also be registered for assessment of eligibility for randomisation by the mars virtual multidisciplinary team . mars was approved by cambridgeshire 4 research ethics committee ( mrec / 04 / 5 / 008 ) and was locally approved at all participating centres . randomisation and masking patients were informed of the mars virtual multidisciplinary team decision , and those still deemed eligible were invited to consent to be randomly assigned ( 1 : 1 ) to either epp followed by radical radiotherapy or to no epp . 
 we used the tnm staging system proposed by the international mesothelioma interest group.13 patients were eligible for randomisation if they had completed preoperative chemotherapy and still had operable disease de ned as t13 , n01 , m0 . registration and randomisation were done by telephone to the icr - ctsu . 
patients and investigators were not masked to treatment allocation . procedures patients assigned to epp underwent surgery at one of the participating surgical centres in accordance with the trial surgical protocol ( webappendix pp 12 )  . 
three other centres were added later ( northern general hospital , she eld , and st jamess university hospital , leeds , opened to recruitment in 2006 , but did not randomly assign an epp patient until 2007 ) , although in one there was no surgery within mars . 
all randomly assigned patients , including those in the no epp group , received continued oncological management according to local policy , which could include chemotherapy , palliative radiotherapy , or further surgery . we monitored acute and late radiotherapy e ects ( de nded in the webappendix p 5 ) , and collected clinical 257 ( 246 ) patients screening logs received screening logs not received 108 ( 97 ) patients approached 149 patients not approached 106 ineligible 30 clinical decision 12 other 1 unknown 40 patients not registered 18 ineligible 3 clinical decision 18 patient decision 1 other ( no radiological staging ) 112 ( 57 ) patients registered 68 ( 57 ) patients registered 44 patients registered 55 registrations not completed 27 disease progression 18 patient withdrawal 5 inoperable 4 other 1 died 57 reviewed by mdt 50 ( 24 ) randomised 7 excluded 6 disease progression 1 patient withdrawal 24 ( 13 ) randomly assigned to epp ( with radical radiotherapy ) 26 ( 11 ) randomly assigned to no epp figure 2 : feasibility of registration and recruitment to mars numbers in brackets indicate those patients screened who did not have chemotherapy before registration . 
mdt = multidisciplinary teaepp = extra - pleural pneumonectomy . see online for webappendix follow - up data including quality - of - life assessment by the european organisation for research and treatment of cancer and qlq - lc13 questionnaires at registration , randomisation , 6 weeks , 3 , 6 , 9 , 12 , 18 ( quality of life only ) , and 24 months , and annually thereafter . ( eortc ) qlq - c30 the aim of the mars feasibility study was to quantify the proportion of eligible patients subsequently randomised , to assess the feasibility of randomising 50 patients within 1 year , 11 and to measure clinical outcomes in randomly assigned patients . 
deaths were reviewed by the independent data monitoring committee for relatedness to trial treatment . statistical analysis the main analyses of the mars feasibility study were descriptive and included summary information from the screening logs on reasons for loss or withdrawal , the proportions of eligible patients registered and randomly assigned to treatment , and the proportion of randomly assigned patients who completed epp surgery . 
we also assessed treatment compliance , complications , perioperative mortality and quality of life . all analyses of randomly assigned patients were by intention to treat and were censored at the date last known to be alive . 
 hrs and 95% cis were calculated by cox proportional hazards regression , adjusting for the prespeci ed prognostic factors of sex , histological subtype , stage at randomisation , and age at randomisation . 
clinicians were free to choose the chemotherapy regimen as long as it included a platinum - based drug . table 2 : characteristics of patients subsequently randomly assigned to epp or no epp proportions are reported with two - sided 95% cis . 
this trial is registered , number isrctn95583524 . 766 vol 12 august 2011 role of the funding source the sponsor of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between oct 1 , 2005 and nov 3 , 2008 , 112 patients were registered , of whom 50 were subsequently randomly assigned to epp ( n = 24 ) or to no epp ( n = 26 ; gure 2 )  . 
62 patients ( 554% ) did not proceed to random allocation , mainly because of disease progression ( 33 patients ) , inoperability ( ve patients ) , or patient choice ( 19 patients )  . 12 centres submitted screening logs for 257 patients . 
of the 246 who were screened before any chemotherapy , 97 ( 394% , 95% ci 331457 ) were invited to enter the registration phase , 57 ( 232% , 180288 ) were registered , and 24 ( 98% , 64142 ) were subsequently randomised . 
136 of 257 ( 53% ) patients were excluded for clinical reasons ( ineligibility , clinical decision , disease progression , and inoperability ) before the patient was approached , 21 of 108 ( 19% ) were excluded before registration , and 39 of 112 ( 35% ) were excluded before randomisation . 
these data suggest an unavoidable cumulative ( 95% ci 706813 ) independent of patient withdrawal or other reasons . loss of 763% during the recruitment period an increasing number of patients were referred to mars centres for assessment for eligibility . 
44 patients were registered in this way , bypassing the screening log process , and therefore came from an unknown denominator . table 1 shows patient characteristics at registration for all 112 registered patients and the 50 who were subsequently randomised . 
seven patients had more than three cycles , two of whom were deemed eligible by the mars virtual multidisciplinary team and subsequently randomly assigned , and four patients had fewer than three cycles of chemotherapy , one of whom was subsequently randomly assigned . 
the most common chemotherapy regimen given was cisplatin and gemcitabine ( 38 of 94 ; 40% ) , followed by cisplatin and pemetrexed ( 24 ; 26% ) , and mitomycin , vinblastine , and cisplatin ( 20 ; 21% )  . 38 ( 76% ) of 50 patients subsequently randomly assigned to epp ( n = 18 ) or no epp ( n = 20 ) had pet - ct scan vol 12 august 2011 24 randomly assigned to epp ( with radical radiotherapy ) 16 completed epp surgery 5 epp surgery not started 3 patient refusal 2 clinical decision 3 epp surgery abandoned 1 perioperative death 2 unexpected disease progression 11 postoperative complications 1 reoperation plus cardiac plus 1 cardiac plus pulmonary plus pulmonary infection 1 cardiac plus pulmonary * 1 cardiac plus urine retention 2 pulmonary plus other 1 reoperation * 1 cardiac 3 other 8 radical radiotherapy not received 1 clinical decision 2 toxicity 2 disease progression 3 died 8 received radical radiotherapy figure 3 : feasibility of epp surgery and radical radiotherapy treatment epp = extra - pleural pneumonectomy . 
other complications were exible bronchoscopy or drain infection in pneumonectomy cavity ; ischaemic right leg requiring femoropopliteal bypass and eventual below knee amputation with culture - positive pneumonia needing mini tracheostomy . 
postoperative pain , low blood pressure , and intraoperative bleeding and further bleeding from chest drains postoperatively . 0 / 24 0 / 26 number of events / at risk no epp figure 4 : overall survival epp = extra - pleural pneumonectomy . time from randomisation ( months ) 8 / 16 3 / 24 3 / 12 4 / 20 articles no epp 5 / 11 articles ten each before randomisation , one assigned three , and one assigned one . 
there were two further deaths within the protocolde ned perioperative period , giving a total of three perioperative deaths in 24 ( 125% , 95% ci 27324 ) in patients randomised to epp by intention to treat and three perioperative deaths in 19 ( 158% , 34396 ) patients in whom epp was attempted . 
11 of 16 patients who were assigned to and completed epp surgery had at least one postoperative complication ( gure 3 )  . eight of the 16 patients who completed epp received radical radiotherapy , ve of whom had complications . 
 severe ( grade 3 or 4 ) acute radical radiotherapy sidee ects were rare : two patients had grade 3 fatigue and one had grade 3 pasevere late side - e ects were fatigue ( n = 1 , grade 3 ) , pneumonitis or dyspnoea ( n = 2 , grade 3 ) , and ascites ( n = 1 , grade 3 )  . 
this patient also had coexisting herpes retinitis and progressive di use changes on mri of the spinal cord outside the irradiated region and thus the diagnosis of radiation - induced myelopathy was excluded . 
two patients who had completed epp operation had further surgery to deal with thoracic space infection . 16 of the 26 patients randomly assigned to no epp received further oncological management : one received radiotherapy alone ; seven had further chemotherapy alone ; one had epp surgery o trial ; one had radiotherapy and chemotherapy ; one had radiotherapy and non - epp surgery ; two had chemotherapy and epp surgery o trial ; one had chemotherapy and cediranib ( as part of a phase 1 trial ) ; and two had radiotherapy , chemotherapy , and nonepp surgery . 
thus , three patients had epp o trial , 13 had further chemotherapy , ve had some form of radiotherapy , three had non - epp surgery , and ten received no further treatment . at a median from randomisation of 247 months ( iqr 216322 ) , 30 of 50 patients had died ( epp n = 17 ; no epp n = 13 ) ; four of these deaths ( three in the epp group and one in the no epp group ) occurred more than 18 months after randomisation . 
of the perioperative deaths in patients randomly assigned to epp , one had a follow - up number of events / at risk 0 / 24 time from randomisation ( months ) 9 / 15 number of events / at risk 0 / 26 time from randomisation ( months ) 6 / 21 9 / 12 figure 5 : recurrence - free and progression - free survival recurrence - free survival in patients randomised to epp ( a ) and progression - free survival in patients randomly assigned to no epp ( b )  . 
epp = extra - pleural pneumonectomy . information available for the mars virtual multidisciplinary tea pet - ct scan results suggested that 23 patients ( ten epp and 13 no epp ) were resectable , ve ( four epp and one no epp ) were equivocal , and in ten patients ( four epp and six no epp ) this information was not available . 
no di erences in terms of stage or other patient - related features were noted between the two groups . of the 24 patients randomly assigned to epp , ve did not proceed to surgery : three by patient choice and two by clinician decision ( gure 3 )  . 
 four surgeons did the epp operations : two were assigned 768 vol 12 august 2011 articles no epp 833 800 833 833 750 1000 900 700 600 500 400 300 200 100 numbers with completed questionnaires returned / at risk no epp figure 6 : quality of life 750 333 667 667 542 583 750 583 708 667 667 583 500 417 registration randomisation 6 weeks 3 months 6 months 9 months 12 months 18 months 24 months time 20 / 23 19 / 26 12 / 23 19 / 26 5 / 21 6 / 26 11 / 17 22 / 25 9 / 13 17 / 22 8 / 10 15 / 18 5 / 10 10 / 13 rupture of the aortic isthmus ( multiple sites ) and died on the operating table ; one died at home ( cause unknown ) shortly after a further operation to have a diaphragm patch repaired ; and one died of bronchopneumonia 6 weeks after the epp operation . 
the perioperative death in the no epp group was one of the patients who underwent epp surgery outside the trial ; the patient died of multiple organ failure . 12 - month survival was 522% ( 95% ci 305700 ) in those allocated epp and 731% ( 517862 ) in those allocated to no epp ( di erence 180% , 18 to 439 ; gure 4 )  . 
the hazard ratio for overall survival in the epp group ( unadjusted ) versus the no epp group was 190 ( 95% ci 092393 ; exact p = 0082 )  . 
none of the three longterm survivors allocated to no epp crossed over to epp . 42 of 50 patients ( epp n = 19 , no epp n = 23 ; four from the no epp group had an event more than 18 months after random allocation ) had disease recurrence ( epp group ) , progression ( no epp group ) , or died before relapse or progression ( gure 5 )  . 
12 - month progression - free survival in the no epp group was 423% ( 235600 ) and median progression - free survival was estimated to be 90 months ( 72147 )  . 23 patients in the epp group and 26 in the no epp group consented to quality - of - life assessment and 12 and 19 patients completed the quality - of - life questionnaires , respectively . 
median quality - of - life scores seemed to be lower for the epp group than the no epp group , with the lowest median score shortly after surgery ( gure 6 ) ; however , there were no statistically signi cant di erences between treatment groups . 12 serious adverse events were reported during the study period : ten in the epp group and two in the no epp group . 
three were suspected unexpected serious adverse reactions ( two in the epp group and one in the no epp group ) , eight were serious adverse reactions ( all in the epp group ) , and there was one other serious adverse event in the no epp group . discussion in an intention - to - treat analysis of outcome data in the mars trial , we noted no survival advantage for the epp surgery group compared with the no epp group . 
in summary , the outcomes of mars provide no evidence of bene t therapy over chemotherapy alone , for survival or quality of life . from epp within trimodal survival data for epp were provided in a recent systematic review , 14 which allows us to put the epp survival data from mars in context ( panel )  . 
for 30 studies where data were given , 12 - month survival ranged from 36% to 83% , with an overall survival of 571% ( 1231 of 2155 patients ) compared vol 12 august 2011 articles panel : research in context systematic review in 2004 , we did a systematic review to assess the available evidence for e ectiveness of extra - pleural pneumonectomy ( epp ) .8 we identi ed seven publications of multimodal therapy but all were analysed on the basis of completed treatment , o ered no control data , and whether the most optimistic estimate of e ect size was su cient to outweigh the burden of treatment was debatable . 
during presentations of the available data to meetings at the british thoracic society and society for cardiothoracic surgery in great britain and ireland and in an editorial in the british medical journal9 we con rmed the uncertainty regarding the e ectiveness of epp was su cient to propose a randomised controlled trial . interpretation in the mesothelioma and radical surgery ( mars ) feasibility study , patients randomly assigned to no epp had better median and 1 - year survival than those assigned to epp . 
when compared with survival data from epp in a systematic review , 14 the mars surgical outcomes are in the middle of the reported range of median and 1 - year survival rates . 
in mars , survival was reported from randomisation to epp , which was after completion of three cycles of chemotherapy rather than from first chemotherapy as is customarily done for reports of epp within trimodal therapy . 
an allowance for this difference in starting time puts the survival of the patients in the no epp group in the upper part of the range of reported trimodal therapy outcomes . 
 the evidence from mars , in the context of external evidence from observational studies , suggests that the net effect of epp is to shorten survival without a gain in quality of life . 
a subset of four of these studies1518 plus an eortc phase 2 trial19 are most comparable with mars in that patients were all operated on since 2000 , had similar stage criteria for epp , and were planned for trimodal therapy in the same sequence , starting with chemotherapy with subsequent epp and then radiotherapy ( table 3 )  . 
in studies in which chemotherapy was the rst modality , the survival time was counted from the start of chemotherapy1518 or from registration.19 in mars , survival was calculated from the later timepoint of randomisation to epp or no [ iqr 2843 ] months between epp ( median 36 registration and randomisation )  . 
thus , to make any comparison , 36 months would have to be added to the 144 months median survival in the epp group of mars and the resulting estimated 18 months survival from the start of treatment becomes similar to these reported series ( table 3 )  . we cannot know from these non - controlled studies what survival might have been for similar patients to those having epp but who were managed without surgery . 
overall survival for the no epp group in mars was better than that used in the power calculations for the proposed phase 3 trial , for which 670 patients would be needed on the basis of the power calculation.9 in any subsequent planned phase 3 study of extirpative surgery , this non - surgical outcome would have to be taken into consideration in the power calculations of the number of patients needed overall to show superiority in the surgical arm . morbidity is di cult to compare between arms with two very di erent approaches to management but for epp morbidity has been consistently reported as high1921 and mars was no exception . 
in mars , no signi cant di erences were reported in the quality - of - life analyses between groups ; however , there seemed to be poorer quality of life , particularly just after surgery in patients randomly assigned to epp . 
the same consideration applies to any protocol that includes radical radiotherapy . in mars , most patients randomly assigned to epp had surgery in two centres with considerable experience in the surgery and perioperative care of these patients . 
in the systematic review of results of epp in 34 studies , 14 including 2320 patients , 30 - day mortality ranged from 0% to 118% and was 60% overall . 
for the 993 patents in 14 studies that were reported since 2008 when mars closed , and which therefore represent a similar era to when patients were recruited to mars , mortality was 56% ( range 0111% ) .14 one should note , however , that for a hypothetical study of 20 consecutive operations , an anticipated 5% mortality would shift to 10% or 0% with one additional or one fewer death . 
in doing so , a rigorous method of surgical quality assurance would be important . at the time mars was being planned , pemetrexed was not yet the standard of care in the uk . 
during recruitment , the chemotherapy standard of care for mesothelioma changed , and patients recruited later were more likely to receive cisplatin and pemetrexed than those recruited earlier in the study . 
there was no imbalance in the use of pemetrexed between the epp and no epp arms . the challenges of compliance with the trial protocol in this study should be taken into account when planning future phase 3 studies in which there is a large di erence in treatments between the two arms . 
some patients did not undergo surgery because , when reassessed after chemotherapy and when the risk : bene t balance of epp had been explained by the operating surgeon , they opted not to proceed . 
 nonetheless , although only 50 patients were randomised over the entire study period , rather than in the anticipated year , the fact that recruitment of these patients was possible suggests that the expected reluctance of patients to accept no radical surgery in a study with two very di erent to management of mesothelioma was not as marked as had been expected . treatment approaches to our knowledge , mars is the rst study to successfully randomly assign patients to epp and no radical surgery for mesothelioma . 
the mars trial was rigorously done , with the nal decision that a patient was eligible for randomisation within mars made in discussions by the mars virtual multidisciplinary team and the allocation to epp or no epp made within the icr - ctsu . 
although the study is small and the conclusions must be guarded , we believe the ndings are of relevance to guide practice . the median survival after epp within mars is consistent with 10 , 12 , 13 , and 14 months in larger observational studies , 2225 as was the proportion of complications . 
however , a much larger study with longer follow - up would be needed to provide reliable evidence on mortality patterns and long - term survival for any extirpative surgery for mesothelioma whether epp or lung - sparing surgery . 
a trial assessing the potential bene ts of total pleurectomy might be more practical in the future management of mesothelioma given the lower risk of perioperative mortality and morbidity in an ageing population with increasing comorbidities . 
recent data that compared and decortication with epp support the contention that this approach is unlikely to result in poorer survival than that associated with epp in mesothelioma.22 total pleurectomy lung - sparing contributors tt and jp were the mars chief investigators who , with dw and kob , instigated the trial . 
the trial management group was responsible for oversight of the day - to - day running of the trial under the guidance of the independent trial steering committee . con icts of interest ms has been a member of an advisory board for eli lilly . 
all other authors declare no con icts of interest . acknowledgments mars was supported by cancer research uk ( grant number cruk / 04 / 003 ) with additional support from the june hancock mesothelioma research fund . 
we acknowledge nancial support from the department of health via the nihr comprehensive biomedical research centre award to guys and st thomas nhs foundation trust in partnership with kings college london . 
travel and accommodation expenses for travel to the surgical centre for each trial participant and one relative ( or carer ) were met by the june hancock mesothelioma research fund . 
we thank all the patients who participated in this study ; and the surgeons , doctors , nurses , radiographers , physicists , pathologists , and data managers at the participating centres . 
we also thank all the trials unit sta at icr - ctsu , sutton , who contributed to the coordination of the trial and the trial management group , and independent data monitoring and trial steering committees for their oversight of the trial . vol 12 august 2011 articles correspondence computerised gave a more accurate assessment of prognosis than visual grading . 
 moreover , comparison of visual scores assessments with of the pten reaction product histological slides can show important discrepancies.6 thus , pten score values estimated by an observer should not be used as a simpli ed surrogate computerised optical density for measurement . 
a computer - assisted reassessment of the stained sections used by obyrne and colleagues , 1 followed by survival models based on continuous data for pten expression , would give more reliable results . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata kreimer ar , gonzlez p , katki ha , et al , for the cvt vaccine group . 
e cacy of a bivalent hpv 16 / 18 vaccine against anal hpv 16 / 18 infection among young women : a nested analysis within the costa rica vaccine trial . 
 lancet oncol 2011 ; 12 : 86270in the trial pro le of this study , virgins who were excluded from the restricted cohort were wrongly classi ed as missing cervical dna results . 
in the results section , the follow - up time for the hpv group should have been 542 months ( range 470748 ) and for the control group 542 months ( range 470744 ) , with a median follow - up time of 542 months and a p value for di erence by arm of 0975 . 
lancet oncol 2011 ; 12 : 98889contrary to the statement made in this comment , we have been subsequently alerted to the fact that translational studies associated with sch ski and colleagues trial had been undertaken but are not yet published . 1096 vol 12 november 2011 editorial published online april 26 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70100 - 0 see comment page 416 for more on health of workers at the fukushima plant see lancet 2011 ; doi : 10.1016 / s0140 - 6736 ( 11 ) 60519 - 9 japans nuclear crisis as the number of people dead or missing after the march 11 earthquake and tsunami in japan approaches 28 000 , e orts to control the crisis at fukushima daiichi nuclear power plant continue . 
government spokesman yukio edano said that the limit was based on shortterm radiation exposure , and that expansion would be considered as long - term exposure is taken into account . 
studies of survivors of atomic bombings and previous nuclear accidents have linked radiation exposure to leukaemia and many solid cancers , including thyroid , lung , gastrointestinal , and breast cancer . 
in a letter to the lancet , japanese doctors called for collection of peripheral - blood stem cells from workers , to allow access to autologous transplant in the event of major accidental radiation exposure . radioactive water used to cool the fukushima reactors has been released into the sea , causing concern about harm to marine life and contamination of the food cha although japanese authorities have banned shing near the plant , i has been found in small konago sh caught o the coast of ibaraki prefecture . 
i has been found in air , rainwater , and milk across the usa ; the us nuclear radiation commission and the environmental protection agency stressed that , at the low concentrations detected , the material poses no threat to public health . the japanese government and plant operator tokyo electric power have been criticised for a lack of clear information about the situation , particularly at the start of the crisis . 
early ratings of the severity of the disaster varied from level 5 to 7 on the international nuclear and radiological event scale of 17 ( the japanese nuclear safety agency initially rated the situation as level 5 , whereas helmut hirsch , a scientist commissioned by greenpeace , rated it as 7 ; chernobyl was rated as 7 )  . 
the chairman of the un scienti c committee on the e ects of atomic radiation ( unscear ) said that fukushima ranked between three mile island and chernobyl in terms of environmental outcomes , and stated that his organisation did not expect any serious long - term health e ects from events in japan . 
 a confused public response is perhaps not surprising in view of the comparisons being made to chernobyl ; little consensus has been reached over the estimated health e ects of the chernobyl accident . 
a 2008 unscear report concluded that over 6000 cases of thyroid cancer in young people could be linked to chernobyl , but that evidence was inconclusive for other cancers , while greenpeace claim that 93 000 cases of cancer will eventually be caused . 
in this issue of the lancet oncology , kirsten moysich and coauthors emphasise that those most likely to show longterm e ects of radiation from chernobyl are those who were children at initial exposure . 
according to the un chernobyl forum report , the accidents largest public - health e ect was on mental healthan e ect worsened by poor information about health risks associated with radiation exposure . 
the longterm consequences of events at fukushima remain to be seen , but as japan moves forward , clear and accessible dissemination of information is essential to ensure that adequate safeguards , monitoring , and support are provided in the years ahead . 
 the lancet oncology vol 12 may 2011 editorial for the acs letter see center / acs - can - requestssurgeon - generals - report - onsugar - sweetened - beverages / for more on overweight and obesity and cancer see n engl j med 2003 ; 348 : 162538 for more on the 2012 cancer prevention guidelines see ca cancer j clin 2012 ; 62 : 3067 for more on physical activity see comment lancet 2012 ; 380 : 18990 for more on the food industry see plos med 2012 ; 9 : e1001246 for more on cynical marketing and brand alignment see editorial lancet 2012 ; 380 : 188 for more on the un declaration on non - communicable diseases see editorial lancet oncol 2011 ; 12 : 981 healthy choice should be the easy choice on july 3 , 2012 , the american cancer society ( acs ) cancer action network asked the us surgeon general to initiate a comprehensive review of the consumption of sugarsweetened beverages and their e ects on healthwith the aim of raising public consciousness and changing behaviours in choices of food and beverages . 
 the acss request is in line with its recent guidelines on nutrition and physical activity for cancer prevention , which proposed individuals recommendations ( eg , limit consumption of high - calorie foods and beverages ) and for community action ( eg , decrease access to and marketing of food and beverages of low nutritional value , particularly to youth )  . for current trends towards increasing portion sizes , sugarsweetened drinks , additives , high - calorie convenience foods , and ready meals , compounded by decreased physical activity , have contributed to the obesity epidemic in the usa , and similar trends are now being seen in many other countries worldwide . 
 the availability of healthy choices are made by individuals , but they can be either facilitated or impeded by social , physical , and economic factors , and by the regulatory environment . 
 access to , and a ordability of healthy foods , compared inexpensive , extensively with marketed high - calorie foods and beverages of low nutritional value , and barriers to physical activity , all contribute to obesity . 
e orts are therefore essential to create an environment that encourages healthy choices , promoting physical activity and increasing access to a ordable , healthy food while decreasing access toand exposure to marketing of food and beverages of low nutritional value . 
 cynical marketing and brand alignment often culminate in the junk food and drink giantseg , mcdonalds , coca cola , and cadburys at the 2012 olympics games in londonacting as major sponsors of sporting and social events . 
corporate responsibility campaigns that deftly shift responsibility for overconsumption from corporations to individuals to forestall regulation and promote brandtactics similar to those employed by the tobacco industryare also worrying and should be strongly discouraged . 
for instance , companies could be incentivised to decrease additive content over longer periods of time to gradually acclimatise consumers to the di erence while not having a major e ect on the viability of their business . interventions and strategies should aim to make healthy choices the easiest choices . 
at both the individual and community level , health policies should aim to : improve awareness and information about bene ts of a healthy lifestyle ; introduce appropriate scal measures to make healthy food more a ordable ; and enhance regulatory mechanisms and measures that increase nutritional information or restrict marketing of unhealthy food . 
the 2004 who global strategy on diet , physical activity , and health , and the 2011 un highlevel summit political declaration on the prevention of non - communicable diseasesin response to the rapid changes in nutrition and physical activity all over the globeprovide a framework that should be implemented and strengthened . 
it took nearly ve decades from the us surgeon generals report on tobacco and cancer for e ective public health policies to be put in place ; we cannot wait that long this time . 
the number of patients reporting no pain from bone metastases , as measured by the bpi , increased from 39 of 149 ( 26% ) before sbrt to 55 of 102 ( 54% ) 6 months after sbrt ( p < 00001 )  . 
bpi - reported pain reduction from baseline to 4 weeks after sbrt was clinically meaningful ( mean 34 [ sd 29 ] on the bpi pain - at - its - worst item at baseline , 21 [ 24 ] at 4 weeks ; e ect size 047 , p = 000076 )  . 
these improvements were accompanied by signi cant reduction in opioid use during the rst 6 months after sbrt ( 43 [ 289% ] of 149 patients with strong opioid use at baseline vs 20 [ 200% ] of 100 at 6 months ; p = 0011 )  . 
ordinal regression modelling showed that patients reported signi cant pain reduction according to the mdasi during the rst 6 months after sbrt ( p = 000003 ) , and signi cant reductions in a composite score of the six mdasi symptom interference with daily life items ( p = 00066 )  . 
 only a few instances of non - neurological grade 3 toxicities occurred : nausea ( one event ) , vomiting ( one ) , diarrhoea ( one ) , fatigue ( one ) , dysphagia ( one ) , neck pain ( one ) , and diaphoresis ( one ) ; pain associated with severe tongue oedema and trismus occurred twice ; and non - cardiac chest pain was reported three times . 
signi cant reductions in patient - reported pain and other symptoms were evident 6 months after sbrt , along with satisfactory progression - free survival and no late spinal cord toxicities . funding national cancer institute of the us national institutes of health . 
 introduction almost 40% of patients with cancer develop spinal metastases during the course of their disease.1 , 2 inadequately treated spinal metastases can lead to pain and neurological complications , including metastatic epidural spinal cord compression . 
as a result , patients might experience severe symptom burden and diminished health - related quality of life ( hrqol ) .35 palliative radiotherapy e ectively controls pain for patients with spinal metastases ; 4 however , higher - dose radiotherapy might be needed for durable tumour control and prevention of bony destruction of the spinal column , which results in spinal instability . 
the spinal cords sensitivity to radiation generally precludes high radiation doses to the spine or re - irradiation using conventional techniques.6 accordingly , new techniques have been developed to optimise radiation dose delivery to bone metastases while sparing the spinal cord . 
 stereotactic body radiotherapy ( sbrt ) , an emerging technique , uses image guidance to deliver high - dose radiation precisely , creating a steep dose gradient at the interface between spinal cord and tumour . 
this approach increases the therapeutic window by lowering the risk for spinal cord myelopathy.68 delivered in high doses and one to ve fractions , spinal sbrt is available on various platforms , some of which include ct imageguided stereotaxy . 
sbrt can be used in combination with or in lieu of surgery and allows patients to avoid possible perioperative risk factors , such as general anaesthesia , bleeding , infection , or hospitalisation . 
in a preliminary report of a prospective phase 12 trial of sbrt , we detailed the safety , e cacy , and patterns of failure for sbrt using results from a vol 13 april 2012 articles subset of patients ( n = 63 ) with spinal metastases who were followed for up to 50 months.2 in the present analysis of the entire patient cohort , we investigated the symptomreduction bene t of spinal sbrt during the rst 6 months post - treatment , and clinical bene t for up to 2 years . 
we hypothesised that , for patients with mech an ically stable spinal metastases , sbrt is a clinically e ective therapy for tumour control ( evidenced by radio graphic depiction of tumour progression ) and sympto matic improvement ( evidenced by patient - reported outcomes )  . 
 methods patients this phase 12 trial was approved by the institutional review board of the university of texas md anderson cancer center ( houston , tx , usa )  . 
 eligibility requirements included a diagnosis of cancer ( excluding multiple myeloma ) , a karnofsky performance status score of at least 40 , and an mri scan documenting spinal or paraspinal metastasis within 4 weeks of enrolment . 
acceptable indications included oligometastatic disease arising from a known primary tumour , failure of previous conventional external beam radiotherapy or surgery , residual tumour after surgery , medical inoperability , and refusal to undergo surgery . 
 patients with mechanically unstable spine or epidural spinal cord compression were excluded ; however , patients with previously documented spinal cord compression that had been decompressed and stabilised were eligible . 
 patients were excluded if they had a pacemaker , were unable to undergo mri , or had received systemic radiotherapy ( strontium 89 ) or cytotoxic chemotherapy within 30 days of enrolment , or spinal external beam radiotherapy within 3 months of enrolment . 
 procedures all patients underwent intensity - modulated , nearsimultaneous , ct - guided sbrt ( ct - linac system [ exact targeting system , varian medical systems , palo alto , ca , usa ] or trilogy treatment delivery systems with on - board imager cone beam ct [ varian medical systems ] ) using a bluebag bodyfix total body immobilisation system ( elekta , stockholm , sweden ) , consisting of a whole - body vacuum cushion , carbon bre base plate , and plastic xation sheet . 
patients received a total dose of 2730 gy , typically delivered in three fractions given every other day , with 10 - gy radiation volume received by the spinal cord limited to 001 c gross target volume encompassed the lesion as visualised on the pretreatment ct scan . 
the clinical target volume encompassed the gross target volume and surrounding vertebral body ( including superior and inferior endplates and any existing paraspinal component ) , along with all additional spinal structures deemed to be at risk for recurrence , such as the pedicle , lamina , and posterior elements . 
in patients with postsurgical metallic artifacts near the area of interest , intrathecal contrast injection with iohexol ( ge healthcare canada inc , mississauga , on , canada ) was done 3060 min before ct image acquisition to assist with accurate spinal cord delineation . 
we measured pain at metastatic sites treated with sbrt via the brief pain inventory ( bpi ) .9 the bpi assesses pain at present and pain at its worst , least , and on average in the past 24 h , on a 010 scale . 
the bpi and mdasi are well validated in patients with various types of cancer.9 , 10 the medical outcomes study 12 - item shortform health survey ( sf - 12 ) was administered as an hrqol measure.11 patient - reported symptoms were assessed in the clinic via the bpi , mdasi , and sf - 12 pre - sbrt ( baseline ) and at 3 months and 6 months post - sbrt ; assessments at 2 weeks , 4 weeks , and 2 months were completed by the patient at home and returned by post , with a reminder call from a study nurse . 
 mri scans of the region treated were done at 3 , 6 , 9 , 12 , 18 , and 24 months post - sbrt and then every 6 months thereafter , as standard care . 
 history , neurological exam results , and mccormick functional classi cation12 were obtained at baseline and at each follow - up visit ( during the same timepoints as patient - reported outcomes assessments )  . 
toxicity was graded by the patients treatment team according to the national cancer institute common toxicity criteria for adverse events , version 2.0.13 statisticsmean , median , sd , statistical analysis descriptive and proportionsare used to describe patient and clinical characteristics . 
to account for multiple comparisons in the symptom and hrqol outcomes , which required eight modellings , we adjusted the individual type i error to be 005 / 8 = 000625 to maintain a conservative family - wise error rate of 005 . using pain cutpoints established by serlin and colleagues , 14 we categorised ratings of the bpis pain - atits - worst item as no pain ( 0 ) , mild pain ( 14 ) , moderate pain ( 56 ) , and severe pain ( 710 )  . 
concordance between bpi and mdasi painat - its - worst ratings , both scored on a 010 scale in the past 24 h , was examined using paired t tests . 
e ect sizes were calculated to estimate the magnitude of change in bpi and mdasi ratings ( composite score for all patients ) between baseline and 4 weeks post - treatment.15 , 16 for patient - reported outcomes measures , e ect sizes are clinically meaningful at roughly one - half sd or higher , the level often used in distribution - based methods of determining meaningful di erences.17 lowess curves , 18 which represent a smoothed estimate of average mdasi symptom severity and interference as a function of time , were constructed from baseline to 6 months post - sbrt . 
 ordinal regression models19 and generalised linear mixed models were tted to examine symptom development for the ve most - severe mdasi symptoms and the symptom - interference component score from baseline to 6 months post - sbrt . 
independent variables included weeks from start of therapy , age , sex , tumour volume of spinal metastasis at baseline , type of primary cancer , disease progression status 6 months after sbrt based on radiographic ( spinal mri ) results , opioid use , and karnofsky performance status at baseline . progression - free survival ( pfs ) and overall survival curves from date of enrolment were generated using the kaplan - meier method . 
spinal mris were done for 142 of 149 patients ( 95% ) at the 6 - month follow - up . baseline characteristics ( n = 149 ) 564 ( 125 ) 580 ( 200880 ) karnofsky performance status number of lesions age in years mean ( sd ) median ( range ) male female 8090 none primary histology breast cancer colon cancer melanoma thyroid cancer renal cancer sarcoma other unknown sbrt site cervical thoracic lumbar sacral previous therapy to spinal site radiotherapy alone surgery alone radiotherapy and surgery non - small - cell lung cancer 77 ( 52% ) 72 ( 48% ) 8 ( 5% ) 108 ( 72% ) 30 ( 20% ) 3 ( 2% ) 40 ( 27% ) 22 ( 15% ) 39 ( 26% ) 48 ( 32% ) 15 ( 10% ) 6 ( 4% ) 15 ( 10% ) 4 ( 3% ) 14 ( 9% ) 47 ( 32% ) 17 ( 11% ) 28 ( 19% ) 3 ( 2% ) 28 ( 19% ) 66 ( 44% ) 51 ( 34% ) 4 ( 3% ) metastatic tumour volume in cm , median ( range ) 382 ( 163579 ) data are number of patients ( % ) unless otherwise stated . 
sbrt = stereotactic body radiotherapy . at the time of analysis , 40 of 149 patients ( 27% ) were still alive , with a median follow - up of 159 months ( range 10916 ; iqr 95303 ) and mean 209 months ( sd 171 )  . 
median overall survival was 23 months ( 95% ci 186272 ) post - sbrt , with 1 - year and 2 - year actuarial survival of 685% ( 601754 ) and 464% ( 378547 ) , respectively . 
tumour progression was seen in 41 of 149 patients ( 28% ) and occurred at a median of 13 months ( range < 1101 ) , based on mri scans . 
actuarial pfs based on mri scans at 6 months , 1 year , and 2 years post - sbrt was 861% ( 95% ci 794907 ) , 805% ( 729861 ) , and 724% ( 631797 ) , respectively . 
 * no signi cant di erences between bpi pain - at - its - worst mean scores and mdasi pain item mean scores ( paired t tests ) were found at any timepoint other than the 6 - month assessment ( p = 0022 )  . 
the number of patients for whom analgesia data were available di ered slightly from the number of patients who provided symptom data . table 2 : pain severity scores and opioid use over time , before and after sbrt pain - at - its - worst ratings , at baseline and post - sbrt assessments . 
 the proportion of patients reporting no spine pain on the bpi increased signi cantly between baseline and 4 weeks post - sbrt , from 39 of 149 ( 26% ) to 43 of 109 ( 39% ) ( p = 0038 )  . 
this improvement continued throughout the study , with 53 of 120 ( 44% ) reporting no pain at 3 months ( p = 0004 ) and 55 of 102 ( 54% ) reporting no pain at 6 months ( p < 00001 )  . 
further , a signi cant decrease in the percentage of patients with moderate - tosevere bpi spine pain ( rated 5 on the 010 scale ) was noted from baseline to 4 weeks ( p = 0003 ) , 2 months ( p < 00001 ) , and 6 months ( p = 0002 ) post - sbrt . we noted clinically meaningful reductions in mean mdasi pain ratings between baseline and 4 weeks posttreatment ( from 34 [ sd 31 ] at baseline to 21 [ 26 ] at 4 weeks on the mdasis 010 scale ; e ect size 047 )  . 
 di erences in mean pain severity ratings between the bpi ( metastatic bone pain ) and mdasi ( general pain ) were noted only for the 6 - month assessment ( p = 0022 ; table 2 )  . 
we noted signi cant reduction in opioid use from baseline to 3 months ( p = 0021 ) and baseline to 6 months ( p = 0011 ) post - sbrt ( table 2 )  . 
 during the 6 months of observation , the ve most severe mdasi symptoms were fatigue , pain , disturbed sleep , 398 vol 13 april 2012 articles fatigue pain disturbed sleep drowsiness distress general activity normal work walking ability enjoyment of life mood relations with other people drowsiness , and distress . 
the lowess curves in gure 2 show that symptom interference lessened over time . reduction table 3 gives p values from ordinal regression modelling of mdasi symptom severity and interference , and sf - 12 physical and mental health component scores , adjusted for independent variables . 
patients reported signi cant pain ( p = 000003 ) 6 months after sbrt , and signi cant reduction in disturbed sleep , drowsiness , sadness ( all p < 00001 ) , fatigue , distress , lack of appetite , nausea , and di culty remembering ( all p < 005 )  . 
ordinal regression modelling showed that a composite score of all six interference items decreased signi cantly at each successive assess ment during the 6 months after sbrt ( p = 00066 )  . 
 patients whose lesions were categorised as progressive at the 6 - month follow - up examination ( 19 of 149 ; 13% ) reported signi cantly more - severe mdasi pain ( p < 00001 ) , fatigue ( p = 001 ) , and drowsiness ( p = 000008 ) than did patients with stable or smaller lesions . 
patients who received opioids during the 6 months after sbrt reported more severe mdasi pain , fatigue ( both p < 00001 ) , disturbed sleep , distress , and drowsiness ( allp < 0001 ) than did patients not using opioids . 
grade 3 toxicities were nausea ( one event ) , vomiting ( one event ) , diarrhoea ( one event ) , fatigue ( one event ) , non - cardiac chest pain ( three events ) , dysphagia ( one event ) , neck pain ( one event ) , diaphoresis ( one event ) , and pain associated with severe tongue oedema and trismus ( two events )  . 
 discussion this study incorporated validated single - symptom ( bpi ) and multisymptom ( mdasi ) assessments to measure patient - reported outcomes for pain and other symptoms in patients with metastatic spine lesions who received sbrt . 
in accordance with our previous report documenting the safety , e ectiveness , and patterns of failure of spinal sbrt , 2 here we showed signi cant reductions in the severity of pain and consistent reductions in other patient - reported symptoms and symptom interference 6 months after spinal sbrt , along with satisfactory pfs and no late spinal cord toxicities . 
 signi cant at p < 000625 , after adjusting for multiple comparisons ( eight models )  . table 3 : signi cance of reduced score for patient - reported outcomes during the rst 6 months after sbrt , adjusted for independent variables panel : research in context systematic review in recent years , spinal stereotactic body radiation therapy ( sbrt ) has become an increasingly established technique for the management of spinal metastases ; however , when this phase 12 trial was designed and activated in 2002 , spinal sbrt literature was in its infancy , consisting of preliminary technical reports with sparse outcomes data . 
drawing on previous experience in symptom research , 25 , 26 we applied well - established symptom - assessment methods to analyse outcomes data acquired from our prospective cohort . interpretation the results of this study show that sbrt is an e ective primary or salvage treatment for mechanically stable spinal metastasis . 
signi cant reduction in patient - reported pain and other symptoms was evident 6 months after sbrt , along with satisfactory progression - free survival and no late spinal cord toxicities . 
for patients with evidence of tumour progression 6 months after sbrt , such progression was signi cantly associated with more severe pain , as expected , suggesting a true ( non - placebo ) palliative e ect for sbrt . 
 this trial provides prospective data that support the careful use of spinal sbrt in selected patients , since sbrt safely and reliably halts the progression of disease while reducing patient symptoms and improving functioning in daily life , as measured by validated methods . 
this study also highlights the importance of integrating patient - reported symptom assessments with clinical outcome evaluations to fully demonstrate the bene t of sbrt in patients with metastatic spinal disease . 
between baseline and 4 weeks post - sbrt , we observed medium , but clinically meaningful , e ect sizes for pain reduction as reported on both the bpi pain - at - its - worst and mdasi pain items , along with signi cant increase in the number of patients reporting complete pain relief as early as 4 weeks post - sbrt . 
signi cant improvement in bpi pain ratings and e ect size relative to pre - sbrt scores was even larger 6 months after treatment ( e ect size 064 , p < 00001 ) , when only two patients had tumour progression and high pain severity and were receiving opioid therapy . 
the e ectiveness of sbrt for tumour and pain control was further evidenced by a reduction over time in the use of strong opioids , astandard of care for managing severe pa patient - reported data from the bpi and the mdasi , which use the same 010 pain - severity rating scale and 24 - h recall period ( table 2 ) , did not di er signi cantly in this cohort of patients with advanced cancer . 
this result suggests that researchers can use either scale in clinical studies when pain at its worst is the outcome of interest , and the same rating is expected with either scale . 
 the present study shows that pain reduction and functional improvement can also be re ected in the reduction of associated symptoms , such as fatigue , distress , and disturbed sleep.21 using a sensitive multiplesymptom assessment method ( the mdasi ) with a highly selective but comprehensive set of symptom items , 22 , 23 we not only prospectively identi ed pain and other major symptoms in a cohort of patients who received spinal sbrt , but also showed how multiple symptoms improved over time after treatment . 
signi cant reductions in the severity of several 400 vol 13 april 2012 articles symptoms in addition to metastatic pain suggest that spinal sbrt produces minimum symptom burden and toxic e ects for patients with late - stage cancer . 
we did not nd a signi cant di erence between renal - cell carcinoma and other primary histologies on patient - reported severity of any mdasi symptom ( data not shown )  . fatigue was consistently the most severe symptom over time , possibly as a result of advanced disease and continuous use of opioids . 
although fatigue improved over the 6 months post - sbrt ( p = 0037 ) , the physical and mental health component scores of the sf - 12 remained more or less constant in follow - up . 
these results are consistent with those of degen and colleagues , 24 who reported signi cant pain reduction 4 weeks after spinal sbrt that was durable to 1 year , but no signi cant change in physical or mental well - being data from the sf - 12 . 
in the present study , lower baseline karnofsky performance status was signi cantly associated with higher total symp tom interference on the mdasi and worsening physical well - being as measured by the sf - 12 ( table 3 )  . 
 the e cacy and safety of sbrt we report in this study are supported by the structured schedule with de ned assessment intervals and follow - up serial spinal mris , which permitted close assessment of the procedure . 
in this study , sbrt did not lead to any radiation - related spinal cord myelopathy ; the numbness reported by some patients was probably caused by pre - sbrt chemotherapy . 
in the present study , 24 patients did not return their paper - and - pencil symptom assessment results by post at the 2 - week assessment timepoint ; nonetheless , most of these patients contributed symptom data at subsequent timepoints . 
however , it is well accepted that sbrt has a quanti able clinical e ect on tumour growth with an accompanying reduction in pain at the radiation site , as shown in our previous report in a subset of this cohort of patients with stage iv cancer.2 one strength of the present study is that multiple symptoms were assessed simultaneously and longitudinally for each patient and compared with baseline , with each patient serving as his or her own control . 
such a trial is currently ongoing with the radiation therapy oncology group 06 - 31 study . in reviewing patient records , we found that 16 patients were positive for adrenal metastasis and 12 were positive for brain metastasis at enrolment . 
for this reason , although the protocol designated data collection up to 24 months , we did not use patient - reported outcomes data beyond 6 months , after which the symptomreduction bene t from sbrt could be confounded by increased pain from rapid disease progression at or near the end of life in this cohort with very advanced cancer . 
 further study of this data is warranted to determine the entire pro le of pain and other symptoms , from beyond 6 months post - sbrt to near the time of death . 
 radiation the role of sbrt in treating mechanically stable spinal metastases without spinal cord compression is continuing to develop in an era in which new tech nologies and treatments are being highly scrutinised . 
nonetheless , the current study provides additional data that support the clinical bene t of sbrt for carefully selected patients and suggests that sbrt reliably halts the progression of disease , reduces patient symptoms , and leads to improved functioning in daily lifethus demonstrating both symptomatic and clinical bene t ( panel )  . 
this study also highlights the importance of integrating patient - reported symptom assessments with clinical outcome evaluations to fully demonstrate the bene t of sbrt in patients with metastatic spinal disease . 
 all other authors declare that they have no con icts of interest . acknowledgments the researchers from the department of symptom research are partially funded by a grant from the national cancer institute ( nci ) of the us national institutes of health ( nih )  . 
this review summarises the present understanding of how mirnas operate at the molecular level ; how their dysregulation is a crucial part of tumour formation , maintenance , and metastasis ; how they can be used as biomarkers for disease type and grade ; and how mirna - based treatments could be used for diverse types of malignancies . introduction micrornas ( mirnas ) are small non - coding rnas ( 2123 nucleotides ) encoded in the genome of plants , invertebrates , and vertebrates . 
these small molecules mainly bind imperfectly to the 3 untranslated region of target messenger rnas ( mrnas ) .1 they negatively regulate gene expression post - transcriptionally by inhibiting translation and causing degradation of target mrna . 
additionally , they are key regulators in many diseaseseg , neurological disorders , heart disease , vascular diseases , viral infection , and cancer.1 the discovery of mirnas led to a worldwide research e ort to establish their roles in cancer . 
 mirnas regulate molecular pathways in cancer by targeting various oncogenes and tumour suppressors , 1 and have a role in cancer - stem - cell biology , angiogenesis , the epithelialmesenchymal transition , metastasis , and drug resistance . 
because mirna - based regulation is dependent on expression of its mrna targets , which are not always ubiquitously expressed , an mirna can have e ects speci c to cells types and conditions . researchers are beginning to uncover the complex role that mirnas have in malignant disease . 
 importantly , this knowledge could be used in the development of anticancer therapies . invaluable regulation of cancer pathways gene regulation and mutations in 2002 , the rst report about the role of mirnas in cancer established that the gene cluster containing the mirnas mir - 15 and mir - 16 is deleted in most people with chronic lymphocytic leukaemia ( cll ) .2 further studies have shown that mir - 15 and mir - 16 act as tumour suppressors by targeting the oncogene bcl2 , which encodes a protein involved in cell survival.3 conversely , mir - 21 is an excellent example of an oncogenic mirna ( a so - called oncomir )  . 
it is overexpressed in most cancerseg , breast cancer , colorectal cancer , lung cancer , pancreatic cancer , glioblastoma , neuroblastoma , leukaemia , and lymphoma.47 overexpression of this mirna can cause tumour growth , maintenance , and survival in vivo.8 importantly , these tumours are completely dependent on expression of mir - 21.8 mir - 21 targets several tumour - suppressor genes , including pten , to increase proliferation and decrease apoptosis.9 , 10 mir - 21 could also promote tumour migration by targeting pro - invasion genes.11 modulation of mirna expression is increasingly thought to be an important mechanism by which tumoursuppressor proteins and oncoproteins exert some of their e ects . 
the proto - oncogene myc transcriptionally activates the mir - 17 - 92 clustera polycistronic transcript of mirnas 17 , 18a , 19a , 20a , 19b - 1 , and 92a - 1.12 the oncogenicity of mir - 17 - 92 is attributed mainly to mir - 19 , which inhibits pten to activate akt signalling and promote cancer - cell survival ( gure 2 ) .13 myc also represses transcription of many tumour - suppressor mirnas , including the let - 7 family.14 reduced expression of let - 7 mirnas is recorded in many cancers , 1 and correlates with poor survival . 
let - 7a , let - 7c , and let - 7g are deleted in lung cancer tumours , and many mirnas of the let - 7 family are located in the genomic region frequently deleted in patients with lung cancer.15 involved the tumour suppressor p53 transcriptionally induces the mir - 34 family of mirnas in response to dna damage ( gure 2 )  . 
mir - 34a is expressed from one genomic site , but mir - 34b and mir - 34c are produced together from one primary transcript at another site.16 , 17 loss of mir - 34a expression is associated with metastasis and recurrence of prostate cancer.18 restoration of mir - 34 in pancreatic cancer cells substantially expression inhibited clonogenic cell growth and invasion , induced vol 13 june 2012 e249 review oncogenic mirnas tumour - suppressing mirnas additionally , genetic variation in the mir - 221 binding site in the 3 utr of kit is associated with a heightened risk of acral melanoma.24 mutations loss of function mutations loss of function oncogenic mirna tumour - suppressing mirna tumour - suppressor mrna oncogene mrna mirna resistance mirna resistance tumour - suppressor mrna oncogene mrna upregulation more transcription gene amplication hypomethylation downregulation less transcription genomic deletion hypermethylation tumour - supressor mrna tumorigenesis oncogene mrna figure 1 : regulation of tumorigenesis by mirnas tumorigenesis can be regulated by mirnas at di erent levels . 
upregulation of oncogenic mirnas reduces expression of tumour - suppressor protein , but downregulation of tumour - suppressing mirnas results in an increased production of oncogenic proteloss - of - function mutations in tumour - suppressing mirnas and mutation of the target section of oncogene mrna can cause tumorigenesis , because expression of oncogenic proteins is no longer regulated . 
similarly , studies of prostate cancer stem cells show that reintroduction of mir - 34a into tumours and cancer cell lines leads to corresponding reductions of cd44 and tumour size.19 expression of mir - 34b and mir34c is lost through deletion or hypermethylation , or is downregulated , in 90% of colorectal cancers.20 , 21 in their absence , both p53 - dependent and p38 - mapk - dependent responses to dna damage are attenuated , leading to oncogenesis.21 , 22 importantly , myc is a target of mir - 34b and mir - 34c , substantiating the inter connected nature of mirna expression in malignancies ( gure 2 )  . gene regulation is not the only way in which mirnas are implicated in malignancies ( gure 1 )  . 
for example , a single nucleotide polymorphism in the 3 utr of the kras oncogene signi cantly increases risk of non - small - cell lung cancer.23 cancer stem cells cancer stem cellsalso called tumour - initiating cells are a small population of cells within a tumour that are thought to arise from somatic stem cells . 
they have enhanced self - renewal capacities , tumorigenic potential , and expression of unique surface markers ; 25 and are often essential for tumour maintenance , treatment resistance , tumour progression , and distant metastasis . 
some mirnas involved in stem - cell regulation are mir - 296 , mir - 134 , mir - 470 , and the mir - 34 family , which targets genes essential for pluripotency and stem - cell function ( eg , oct4 , nanog , sox2 , notch , and bcl2 ) .26 let - 7 in vitro and regulation of cancer stem cells . 
 in breast cancer , let - 7 and mir - 30 are important for the downregulated in breast - cancer stem cells.27 when overexpressed in mice , it can reduce numbers of undi erentiated cells inhibit cell proliferation , tumour formation , and metastasis.28 mir - 30 expression is also low and can inhibit the selfrenewal ability of breast - cancer stem cells . 
the combination of both inhibits self - renewal and mammosphere formation in breast - cancer stem cells.28 let - 7 and mir - 30 angiogenesis promotion of angiogenesis by tumours necessitates activation of proliferation and migration pathways in vascular smooth muscle cells . 
in nasopharyngeal carcinoma cells , the mir - 15a / 16 - 1 cluster regulates angiogenesis ( gure 3 ) by targeting the angiogenic factors vegfa and met.29 mir - 145 blocks migration of vascular smooth muscle cells by inhibiting fli1 , 30 and mir - 143 by targeting the versican protein involved in migration induced by platelet - derived growth factor.31 the mir - 143 cluster is downregulated in cancers of the prostate , colon , gastric , and bladder , and in cll and b - cell lymphomas.32 transition the epithelialmesenchymal epithelialmesenchymal transition and metastasis epithelial cells undergo several molecular changes during assume a mesenchymal cell phenotype necessary for tumour metastasis and progression ( gure 3 ) .33 expression of e - cadherin ( cdh1 ) is essential for retaining an epithelial cell type . 
similarly , expression of mir - 200 in breast cancers is positively correlated with concen trations of e - cadher the e250 vol 13 june 2012 review importance of this association is supported by evidence that restoration of mir - 200 expression is su cient to reverse the transition ( ie , mesenchymal to epithelial ) in a kidney - derived cell line.34 however , other mirnas are needed epithelialmesenchymal the transition . 
in pancreatic epithe lial cells , the expression of mirnas from the mir - 30 family inversely correlates with the mesenchymal pheno type.35 in mesenchymallike ovarian cancer cell lines , overexpression of mir429 reverses the transition.36 to prevent the to supplement clinical potential diagnosis and classi cation the development of cytogenetic , immunological , and traditional molecular methods morphological classi cation systems has re ned the identi cation of cancer subtypes.37 for instance , transcriptome pro ling studies of di erent cancer types with large - scale genomic approaches showed that a 97 - gene expression pro le is better for classi cation of breast cancer histological grade than are lymph - node status and tumour size.37 gene - expression pro ling has also led to development of breast - cancer prognostic pro ling tests , which have been approved for clinical use.38 as with mrna , whole - genome mirna pro ling has shown that mirna expression changes substantially in most human cancers.39 mirna expression signatures provide a more accurate method of cancer subtype classi cation than does expression pro ling of an entire group of known protein - coding rnas.40 mirna pro les can contribute to the diagnostic and prognostic classication of human malignancies ( table ) .2 , 4148 the use of the traditional , gold standard , histological examination in the diagnosis and classi cation of cancers can be limited by availability of adequately preserved tissue and the possibility of subjective interpretation by pathologists . 
by contrast , mirnas show resistance to degradation and their expression levels can be established in a few hours with as little as 10 ng of total rna ; therefore , mirnas are ideal as both diagnostic and prognostic indicators in clinical settings . screenings of resected tumours and biopsy samples have identi ed mirna signatures that can be used to di erentiate between malignant and benign condi tions in several organs . 
seven mirnas are di erentially expressed in biopsied pancreatic ductal adenocarcinomas compared with benign and healthy tissues.49 a multi centre trial50 showed that use of signatures from these mirnas gives greater accuracy than does conventional cytology . 
one mirna was overexpressed in 19 of 20 malignant samples.51 mirna expression can also be used to identify well characterised genotypeseg , to distinguish between dna damage drosha mir - 34 carcinogenesis mirna processing mir - 17 - 92 cluster pten figure 2 : oncogenic and tumour - suppressing mirnas in the dna damage response dna damage can lead to the upregulation of the mir - 34 family through the activation of the p38 map - kinase and p53 pathways . 
 vol 13 june 2012 e251 review these two mirnas are deleted or down regulated in 68% of patients with cll.2 furthermore , cll can be classi ed into ve di erent categories according to genetic instabilities ( deletion of chromosomal regions 11q , 13q , and 17p ; trisomy 12 ; and normal karyotype )  . 
studies show that the speci c expression pattern of 32 individual mirnas can di erentiate between these di erent chromosomal abnormalities ( table ) .42 other forms of genomic instability can be inferred with mirna pro ling ( table )  . prognostic indicators many identi ed genotypes are associated with distinct prognoses ( table )  . 
by comparing two main groups of patients with good prognosis ( low zap70 expression , mutated immunoglobulin variable region genes ) and poor prognosis ( high zap70 , immunoglobulin variable region genes not mutated ) , they identi ed 13 mirnas with variable expression according to prognosis ( table ) .41 prognosis or outcome microrna expression reference chronic lymphocytic leukaemia high zap70 ; immunoglobulin variable region not mutated poor 13q14.3 deletion indolent 17p deletion aggressive calin41 calin2 visone42 mir - 15a mir - 16 - 1 mir - 16 - 2 mir - 195 mir - 221 mir - 23b mir - 155 mir - 24 - 1 mir - 146 mir - 223 mir - 29a - 2 mir - 29b - 2 mir - 29c mir - 15a mir - 16 - 1 mir - 130b mir - 129 - 3p mir - 632 mir - 768 - 5p mir - 638 mir - 453 mir - 29b / c mir - 181b / c / d mir - 342 - 3p mir - 223 mir - 181a mir - 367 mir - 205 mir - 96 mir - 182 mir - 183 down down down down down down down down down down down down disease progression mir - 181 visone42 trisomy 12 lung cancer non - squamous non - small - cell lung cancer ( stages ii , iii , and iv ) and lymph - node metastasis poor lebanony43 zhu44 zhu44 zhu44 ( continues on next page ) in lung cancer , researchers focusing on the mir - 183 family of mirnas ( mir - 183 , mir - 182 and mir - 96 ) have recorded a link between the expression of these mirnas and progression of non - small - cell lung cancer . 
expression of the mir - 183 family can also help to identify tumours with heightened lymph - node metastasis ; an increased likelihood of progression to stage ii , iii , or iv ; and poor survival ( table ) .44 many biomarkers are prognostic indicators for breast cancer . 
the two most common are the oestrogen receptor , expression of which predicts a good outcome ; and her2 , which when over expressed is associated with poor outcome , anti - oestrogen treatment resistance , and metastasis.53 although identi cation of these two markers has been invaluable for breast cancer management , other molecular methods are needed for classi cation of subtypes . 
analysis of 93 breast - cancer samples showed that speci c patterns of mirna expression were associated with breast - tumour subtypes of di erent clinical outcomes.45 one investigation45 showed that expression of 31 mirnas was signi cantly associated with clinical factors . 
14 were overexpressed in grade iii , oestrogen - receptor - negative malignancies of basal - like subtype , seven of which were also associated with her2 - overexpressing cancers.45 import antly , six were related to the same clinical outcomes in another independent dataset ( table ) .46 although the expression pattern of several mirnas can give useful information about stage and prognosis , one mirna alone can have accurate predictive power . 
 the predictive e ect of mir - 210 was so strong that the researchers noted that the overexpression of mir - 210 alone allowed prediction of prognosis to the same level as a 76 - gene mrna signature test ( gene76 )  . 
overexpression of mir - 210 is associated with an increased risk of recurrence and a reduced chance of relapse - free survival.46 in cll with trisomy 12 , when expression of immuno globulin variable region genes and zap70 does not predict clinical outcome , the overexpression of one mirna , mir - 181 , can predict disease progression ( table ) .42 to colorectal cancers resistant mirna pro ling can identify treatment - resistant cancers . 
as with overexpression of her2 in breast cancer , overexpression of four mirnas have been linked to egfr antagonists.48 screening for mirnas could enable treatment to be tailored to individual patients and thus increase the chances of survival . 
urine cytology of speci c markers can also be used but this method does not have the sensitivity biomarkers in body uids although mirna pro ling of tumours could be an excellent prognostic test , invasive procedures such as biopsy , aspiration biopsy , or excision surgery of alreadyexisting tumours are necessary to obtain samples . 
an ideal biomarker should be accessible with non - invasive methods , sensitive enough to detect early presence of tumours before clinical symptoms present , and absent or low in healthy , tumour - free individuals.54 stable , degradationresistant , extracellular mirnas could be detected in body uids such as serum , urine , saliva , tears , breast milk , seminal uid , and faecal matter . 
one breast cancer study comparing the circulating mirna pro le in healthy women with that of those with early - stage breast cancer62 showed that downregulation of mir - 181a and mir - 1304 is associated with the disease . 
mir - 195 and let - 7a concentrations are higher in the plasma of patients with breast cancer than in healthy individuals.62 after tumourexcision surgery , postoperative serum concentrations of both these mirnas return to values reported in the healthy control group.59 researchers investigating the plasma levels of mirnas in 74 patients diagnosed with di erent types of lung cancer63 identi ed three mirnas ( mir - 155 , mir - 197 , and mir - 182 ) that were at a higher concentration in patients with cancer than in control individuals . 
 the serum the investigators also reported that vol 13 june 2012 e253 review for detection of low - grade bladder cancer , 64 driving the search for new speci c and sensitive biomarkers . 
 a proof - of - concept study65 showed that mir - 126 , mir - 182 and mir - 199a concentrations are signi cantly increased in the urine of patients with stage 1 bladder cancer , as well as in those with stage 2 and stage 3 disease . 
 the concentration of these markers in urine continues to increase as malignancy progresses and decreases after tumour - excision operations.65 for those with a positive for colorectal cancer , patients older than 60 years are o ered screening every 2 years with non - invasive faecal occult blood testing , 66 with a subsequent colonoscopic result . 
 investigation unfortunately , the test has only 3350% sensitivity ; use of novel biomarkers would prevent many healthy individuals undergoing an expensive , painful procedure with the risk of serious medical complications.67 mir - 21 and mir - 106 are upregulated in the stool of patients with colorectal neoplasia ( colorectal cancer or adenoma )  . 
mir144 * is increased in the faeces of patients with colorectal cancer with a sensitivity of 74% and a speci city of 87% , and is thus another potential biomarker to help diagnosis of colorectal cancer.68 samples extracted with the faecal blood - test kits could also be used to extract mirnas ; clinicians could undertake both tests simultaneously to increase the sensitivity of diagnosis.67 mirnas as cancer treatment the development of new treatments has contributed substantially to increased 5 - year survival and the reduction in overall mortality rates.62 , 69 however , although the classi cation of cancers has become increasingly diver si ed , the variety and speci city of treatment options has lagged behind . 
more than 2000 gene - therapy - based clinical trials are in progress for various illnesses , but only one is of mirna treatment.32 treatment can be targeted to mirnas in two ways : mirna reduction and mirna replacement ( gure 4 )  . 
new mirna - based treatments would need to have selective and accurate delivery of the agents to the target tumours to increase the therapeutic potential and reduce possible side - e ects . two major di culties have impeded development of mirna - based treatments . 
first , rna has low stability in vivo ; mirna introduced into mice via the tail vein is cleared from the circulatory system in 30 min.70 unmodi ed , saline - formulated , double - stranded rna injected intravenously undergoes rnase - mediated degradation and rapid renal excretion . 
an increase could be achieved by improved mirna stability or by protection from rna - hostile environments . substitution of phosphodiester by phosphorothioate in the rna backbone , and of the ribose moieties to 2 - o - methyl or other 2 substitutions confer substantial nuclease resistance.71 locked nucleic acid ( lna ) is a modi ed rna nucleotide that has an extra bridge connecting the 2 oxygen and 4 carbon . 
these modi cations increase the thermostability of lna - rna duplexes , increase target speci city , and are resistant to exonucleases and endonucleases , thereby improving stability of mirnas in vitro and in vivo.72 finally , introduced rna can be conjugated to a cholesterol moiety , increasing stability in the circulation . 
for example , an antagonist of mir - 16 with 2o - methyl modi ed nucleotides and cholesterol linked to its end via a hydroxyprolinol linkage is stable and e ciently silences mirna expression.73 protection from hostile environ ments is typically achieved by encasing of lna or mirna mimics in nanoparticles to form micelle - like structures ( gure 4 )  . the second di culty is how to ensure tumour - speci c delivery and retention of mirnas . 
e orts to achieve targeted delivery could be further hindered by rst - pass metabolism and rapid localisation of small molecules delivered systemically to the kidney and liver.74 targeted delivery to speci c tissues can be done when tumour - speci c ligands are linked to nanoparticles , which can be directed to tumour cells via active or passive targeting . 
nanoparticles between 15 nm and 100 nm are the best for systemic delivery.76 active targeting of nanoparticles necessitates their conjugation with di erent compounds that have a speci c a nity to tumours . 
various cancer - associated cell - surface proteins ( eg , her2 , 77 egfr , 78 and ca - 12579 ) and hyaluronic acid80 could potentially be used for this conjugation . 
investigators have developed a poly ( ethylene glycol ) hyaluronic acid nanoparticle ( p - ha - np ) that can be used to deliver doxorubicin and camptothecin to mouse cells.81 the nanoparticles were internalised successfully into cancer cells ( scc7 and mda - 3t3 ) , but rarely taken up by normal broblasts ( nih - 3t3 )  . 
tumour - bearing mice were systemically treated with camptothecin de livered with p - ha - np , and tumour growth was success fully stopped for at least 35 days . 
these nanoparticles could e254 vol 13 june 2012 review mirna modied rna target mrna nanoparticle antibody cancer - specic ligands cell membrane figure 4 : mirna - based treatment in mirna reduction treatment ( a ) , single - stranded lna molecules ( anti - mirnas ) bind to mirnas complementarily , preventing the mirnas from binding to target mrnas . 
 possibly be modi ed to carry mirnas to speci cally targeted cancer stem cells.81 furthermore , integrin - - 3 - targeted nanoparticles used to deliver anti - mir - 132 had promising results in inhibition of angiogenesis and breast tumour metastasis.82 the goal of mirna replacement is the reintroduction of mirnas depleted in cancer cells and the reactivation of cellular pathways that drive a therapeutic response . 
 trang and co - workers70 concluded that a chemically synthesised mir - 34a packaged into a lipid - based delivery vehicle and given locally or systemically could block tumour growth in mouse models of non - small - cell lung cancer . 
systemic delivery of formulated mir - 34a did not induce a rise in cytokines or liver and kidney enzymes in serum , suggesting that the formulation is well tolerated and that side - e ects could be negligible . 
similar results were noted in another study of a mouse model of non - smallcell lung cancer with activated kras ; 70 an mir - 34a or let - 7 mimic mirna formed a complex with a neutral lipid emulsion , which led to a 60% reduction in tumour area.70 additionally , systemic delivery of atelocollagenconjugated mir - 16 in a mouse xenograft model of prostate cancer inhibited metastasis into bone.83 mirna reduction with lna has been done with antimir - 21 to treat autoimmune splenomegaly in mice with systemic lupus erythematosus ; 84 mir - 21 is upregulated in all subsets of lupus mouse lymphocytes . 
targeting of mir - 21 with an intraperitoneally injected lna - based antagonist decreases manifestation of cardinal systemic lupus erythematosus and leads to the reversal of splenomegaly.84 the only mirna - based treatment tested in people is anti - mir - 122 for the treatment of infection with hepatitis c virus ( hcv )  . 
mir - 122 is an essential mirna for hcv replication and is predominantly in the liver.85 in 2010 , data from a drug trial of an intravenously delivered lna to remove mir - 122 and stop infection in chimpanzees was reported.86 lna given to chronically infected chim panzees once a week for 12 weeks led to a reduction in viral load in the serum and the liver . 
a phase 1 trial87 in 77 healthy volunteers established that anti - mir - 122 is safe and vol 13 june 2012 e255 review search strategy and selection criteria data for this review were identi ed by searches of pubmed with the term microrna in combination with cancer , in vivo , circulating , systemic delivery , therapeutics , or lna . 
the subsequent phase 2a trial87 assessed the safety and antiviral activity of subcutaneous anti - mir - 122 given at doses of 3 mg / kg , 5 mg / kg , and 7 mg / kg every week for 29 days ; patients were followed up until week 18 . 
this trial87 drew attention to the potential of lnas for cancer treatment . conclusion the discovery of mirnas has changed the way control of gene expression is thought about and , perhaps more importantly , has set a precedent for the development of new diagnostic methods and treatments of diseases , including malignancies . 
in the long term , work to identify major mirna targets and to develop safe and speci c methods of delivery of mirna - based treatments could allow modulation of mirnas to become a central feature of cancer treatment and management . contributors ywk and df - m did the literature search , wrote and edited the report , and designed the gures . 
mb wrote and edited the report . con icts of interest ywk and mb have led a patent relating to microrna delivery with nanoparticles conjugated to cancer - targeting anti - cd4 antibodies . 
the animal and human clinical data on the low rate of neurotoxic e ects of eribulin compared with other anti - microtubule drugs may make it a step forward for the patients quality of life too . finally , a plea must be made again for closer examination of tumour samples in clinical trials , which was not done as part of this study . 
although very expensive , the comparison of tissue from responding patients with that of patients who progress could provide invaluable information for a more accurate determination of who will truly bene t from eribulif markers that rule out or enrich populations for treatment with eribulin can be identi ed , we will move clinical therapeutics forward with greater e ciency and parsimony . robert g maki mount sinai school of medicine , medicine and pediatrics , gustave l levy place , box 1208 , new york , ny 10029 - 6574 , usa bobmakimd@gmail.com vakifahmetoglu h , olsson m , zhivotovsky b . 
imatinib mesylate ( sti - 571 glivec , gleevec ) is an active agent for gastrointestinal stromal tumours , but does not yield responses in other soft - tissue sarcomas that are unselected for a molecular target . 
phase iii randomized , intergroup trial assessing imatinib mesylate at two dose levels in patients with unresectable or metastatic gastrointestinal stromal tumors expressing the kit receptor tyrosine kinase : s0033 . 
halichondrin b and homohalichondrin b , marine natural products binding in the vinca domain of tubuldiscovery of tubulin - based mechanism of action by analysis of di erential cytotoxicity data . 
interactions of halichondrin b and eribulin with tubulj chem inf model 2011 ; 51 : 1393404 . sch ski p , ray - coquard il , cio a , et al , for the european organisation for research and treatment of cancer ( eortc ) soft tissue and bone sarcoma group ( stbsg )  . 
nilotinib versus imatinib for the treatment of patients with newly diagnosed chronic phase , philadelphia chromosome - positive , chronic myeloid leukaemia : 24 - month minimum follow - up of the phase 3 randomised enestnd trial . 
 moreover , comparison of visual scores assessments with of the pten reaction product histological slides can show important discrepancies.6 thus , pten score values estimated by an observer should not be used as a simpli ed surrogate computerised optical density for measurement . 
a computer - assisted reassessment of the stained sections used by obyrne and colleagues , 1 followed by survival models based on continuous data for pten expression , would give more reliable results . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata kreimer ar , gonzlez p , katki ha , et al , for the cvt vaccine group . 
e cacy of a bivalent hpv 16 / 18 vaccine against anal hpv 16 / 18 infection among young women : a nested analysis within the costa rica vaccine trial . 
 lancet oncol 2011 ; 12 : 86270in the trial pro le of this study , virgins who were excluded from the restricted cohort were wrongly classi ed as missing cervical dna results . 
in the results section , the follow - up time for the hpv group should have been 542 months ( range 470748 ) and for the control group 542 months ( range 470744 ) , with a median follow - up time of 542 months and a p value for di erence by arm of 0975 . 
lancet oncol 2011 ; 12 : 98889contrary to the statement made in this comment , we have been subsequently alerted to the fact that translational studies associated with sch ski and colleagues trial had been undertaken but are not yet published . 1096 vol 12 november 2011 comment are more likely to opt for burdensome treatment with a small chance of improvement than are healthy people.6 , 7 following a deliberative model of patientphysician interaction , 8 the physician should explain his or her own assessment of bene ts and harms , including the underlying health - related values ( see question two ) , thereby empowering the patient to reconsider his or her own values , preferences , and the resulting decision . 
 if the patients choice to proceed with the intervention results from deeply held values coupled with a thorough understanding of the facts , the patient and the physician should proceed with the intervention . 
 although physicians should always minimise the required resources to achieve a speci c treatment goal , whether a high consumption of resources constitutes a legitimate reason to withhold an intervention that provides only a questionable or small net bene t to the patient is controversial.9 , 10 under the assumption that the setting of limits is unavoidable in any health - care system , we have included a fth question that asks doctors to take the resource implications of their decisions into account in an ethically justi ed way . 
the question becomes relevant in all health - care systems in which physicians have to ration care through budgets , waiting lists , or the application of rationing rules to individual cases . 
if the patient has a realistic understanding of the situation and there is persistent disagreement about the value of the intervention ( after answering question four ) , the physician should explicitly inform the patient that the requested intervention provides only a small or questionable net bene t at high costs . 
alternatively , if the patient does not have a realistic understanding of his or her medical situation and the bene tharm ratio of the intervention is at least questionable in the physicians judgment , question ve could guide the decision . 
however , if the treatment draws heavily on resources , considerations of equality might justify a unilateral decision to withhold the requested intervention , because the high resource consumption is not counterbalanced by a clear net bene t or sound autonomy - based arguments . 
beyond futility : to what extent is the concept of futility useful in clinical decision - making about cpr ? lancet oncol 2002 ; 3 : 63842 . consensus statement of the society of critical care medicines ethics committee regarding futile and other possibly inadvisable treatments . 
 motesanib , or open - label bevacizumab , in combination with paclitaxel , as rst - line treatment for her2 - negative locally recurrent or metastatic breast cancer : a phase 2 , randomised , double - blind , placebo - controlled study . 
lancet oncol 2011 ; 12 : 66372in the summary , the nal sentence of the findings section should have stated 12 208 ( 73% ) of the women positive by hpv testing had no cytological abnormality , and these women had 258 ( 35% ) of 747 cin3 or adenocarcinoma in situ , 25 ( 29% ) of 87 cancers , and 17 ( 63% ) of 27 adenocarcinomas . 
this long - awaited once in a generation opportunity to put ncds on the global agenda generated as many fears of a missed opportunity as it did hopes of a turning point for the health of millions around the world . 
the unanimous agreement by un member states to hold the summit on ncds signalled recognition of a growing global emergency and , at long last , a willingness to act . 
although often thought of as diseases of rich countries , ncds now disproportionately a ect more people in poorer nations , accounting for 80% of all ncd - related deaths . 
ncds include cancers , cardiovascular diseases , diabetes , and chronic respiratory diseases : all are largely preventable and share common risk factors , such as tobacco use , unhealthy diet , physical inactivity , and harmful use of alcohol . 
furthermore , the world economic forum identi ed ncds as a severe threat to economic development and put a price tag of $30 trillion on the expected burden of these diseases over the next 20 years . 
 the aim of the meeting was to secure commitment from heads of government for a coordinated global response , to raise awareness among the general public , and to adopt a comprehensive political declaration for health strategies . 
notably , governments decided to commit to multisectoral national and international policies to control ncds , to reduce individual exposure to ncd risk factors through international agreements such as the who framework convention on tobacco control , the who global strategy on diet , physical activity and health , and the who global strategy to reduce the harmful use of alcohol , to give greater priority to early detection , screening and diagnosis , to increase access to vaccines as part of national immunisation programmes , and to improve access to palliative care . 
 industry these commitments should be applauded as a good start in tackling the serious burden that ncds represent , and signal the start of attempts to reverse the undue long - term neglect the political arena has a orded such issues . 
 indeed , although the fundamental con ict of interest between the tobacco industry and public health is fully recognised in the declar ation , other groups from the food and drink industrywhich the un euphemistically refers to as civil society alongside organisations such as academiawere invited to participate in the meeting , although they were excluded from any decision - making . 
 in preparation for the meeting , the uiccas part of the ncd allianceproposed very speci c targets that could have been included , such as a commitment by 2025 to reduce avoidable deaths from ncds by 25%a target who believes is achievable . 
instead , the document calls on who simply to set up a comprehensive global monitoring framework and prepare recommendations for voluntarynot compulsoryglobal targets before the end of 2012 , and to report initial progress in 2013 . 
afatinib versus placebo for patients with advanced , metastatic non - small - cell lung cancer after failure of erlotinib , ge tinib , or both , and one or two lines of chemotherapy ( lux - lung 1 ) : a phase 2b / 3 randomised trial . 
lancet oncol 2012 ; 13 : 52838in this article ( published online march 26 ) , the rst sentence of the fourth paragraph on the fourth page should have read we measured progression - free survival from the date of randomisation to disease progression or death , whichever occurred rst . 
the coin trial assessed preplanned treatment holidays in advanced colorectal cancer to achieve this aim . methods coin was a randomised controlled trial in patients with previously untreated advanced colorectal cancer . 
in arm c , patients who had not progressed at their 12 - week scan started a chemotherapy - free interval until evidence of disease progression , when the same treatment was restarted . 
here , we compare arms a and c , with the primary objective of establishing whether overall survival on intermittent therapy was non - inferior to that on continuous therapy , with a prede ned non - inferiority boundary of 1162 . 
 median survival in the itt population ( n = 815 in both groups ) was 158 months ( iqr 94261 ) in arm a and 144 months ( 80247 ) in arm c ( hazard ratio [ hr ] 1084 , 80% ci 10081165 )  . 
preplanned subgroup analyses in the per - protocol population showed that a raised baseline platelet count , de ned as 400 000 per l or higher ( 271 [ 28% ] of 978 patients ) , was associated with poor survival with intermittent chemotherapy : the hr for comparison of arm c and arm a in patients with a normal platelet count was 096 ( 95% ci 080115 , p = 066 ) , versus 154 ( 117203 , p = 00018 ) in patients with a raised platelet count ( p = 00027 for interaction )  . 
in the per - protocol population , more patients on continuous than on intermittent treatment had grade 3 or worse haematological toxic e ects ( 72 [ 15% ] vs 60 [ 12% ] ) , whereas nausea and vomiting were more common on intermittent treatment ( 11 [ 2% ] vs 43 [ 8% ] )  . 
grade 3 or worse peripheral neuropathy ( 126 [ 27% ] vs 25 [ 5% ] ) and hand foot syndrome ( 21 [ 4% ] vs 15 [ 3% ] ) were more frequent on continuous than on intermittent treatment . interpretation although this trial did not show non - inferiority of intermittent compared with continuous chemotherapy for advanced colorectal cancer in terms of overall survival , chemotherapy - free intervals remain a treatment option for some patients with advanced colorectal cancer , o ering reduced time on chemotherapy , reduced cumulative toxic e ects , and improved quality of life . 
 introduction the treatment of advanced colorectal cancer has improved substantially during the past decade with the introduction of new and more e ective drugs and advances in our understanding of the diseases molecular biology . 
strategies that minimise time on treatment , reduce side - e ects , and improve quality of life , while maintaining duration of survival , are highly desirable . before the introduction of irinotecan and oxaliplatin into treatment schedules for advanced colorectal cancer , uorouracil - based chemotherapy was generally continued until unacceptable toxic e ects or disease progression . 
the resultant cumulative sensory neuropathy with oxaliplatin and handfoot syndrome with uoropyrimidines1 adversely a ect quality of life and overall dose intensity because of reduced dosing in subsequent treatment cycles . one potential method to reduce toxic e ects and improve quality of life is to consider alternatives to continuous chemotherapy . 
intermittent therapy given for a restricted period and then restarted , either after a prede ned interval ( prede ned treatment ) or at disease progression ( repeat therapy ) , are such alternatives . 
however , in breast and prostate cancer , intermittent hormones or cytotoxic agents have not reduced median overall survival.24 a previous medical research council ( mrc ) trial , cr06b , assessed 354 patients with advanced colorectal cancer treated with the de gramont ( uorouracil and folinic acid ) schedule , continuous infusional uorouracil , or raltitrexed.5 those with stable or responding disease at 12 weeks were further randomly assigned to continue therapy until progressive disease or to stop , with the option to restart the same chemotherapy at later progression . 
there was no evidence of a di erence in overall survival between the two strategies ( hazard ratio [ hr ] 087 , 95% ci 069109 , p = 023 ) , with the results even slightly favouring intermittent over continuous treatment . 
 although criticised for its small size and failure of randomly assigned patients to restart protocol treatment , this trial gave impetus to the notion of intermit tent therapy in advanced colorectal cancer and set a precedent for combination chemotherapy.6 intermittent trials of further with its cumulative sensory neuropathy , oxaliplatin is an appropriate drug to use in the exploration of intermittent therapy and has been assessed in two trials , optimox - 17 and optimox - 2.8 in optimox - 1 , 7 continuous oxaliplatin and uorouracil were compared with a novel strategy of planned oxaliplatin breaks , but with continuous uorouracil . 
neither trial showed a signi cant reduction in survival with intermittent therapy , although optimox - 2 showed a trend in favour of continuation of uorouracil during oxaliplatin breaks , and has been adopted as the benchmark for standard practice . 
this outcome is despite failure to recruit beyond phase 2 after the licensing of bevacizumab and that the trend in favour of continuous treatment was not statistically signi cant . the phase 3 coin trial ( continuous or intermittent ) was developed to conclusively address this issue . 
the coin trial also assessed the e ect of addition of cetuximab to continuous oxaliplatin and uoro pyrimidine combination chemo therapy ; the results of this comparison are reported in a companion paper.9 methods study design and participants the full protocol can be found on the mrc clinical trials unit website . 
 eligibility included written informed consent , age of at least 18 years , and histologically con rmed adenocarcinoma of the colorectum , inoperable metastatic or locoregional measurable disease ( response evaluation criteria in solid tumors [ recist ] version 1.0 ) , 10 no previous chemotherapy for metastatic disease , who per formance status 02 , and good end - organ function . 
 patients were excluded if they had previous or present malignant disease , uncontrolled medical comorbidity likely to interfere with coin treatment or response assessment , known brain metastases , or previous oxaliplatin exposure . coin was approved by the uk medicines and healthcare regulatory agency in june , 2004 , and southwest multicentre research ethics committee in december , 2004 . 
 approvals for the irish sites were obtained from the irish medicines board in november , 2006 , and st jamess hospital / adelaide & meath hospital , incorporating the national childrens hospital research ethics committee in december , 2006 . 
the trial was coordinated by the mrc clinical trials unit following the principles of international conference on harmonisation good clinical practice guidelines , undertaken with a trial management group , monitored at regular intervals by an independent data monitoring committee , and overseen by an independent trial steering committee . randomisation and masking central telephone randomisation was done by the mrc clinical trials unit , using the method of minimisation with a random element . 
patients were randomly assigned ( 1 : 1 : 1 ) to the control arm ( oxaliplatin plus capecitabine or oxaliplatin plus uorouracil and folinic acid ) chemotherapy ( arm a ) or one of two research arms : continuous chemotherapy plus cetuximab ( arm b ) or intermittent chemotherapy ( arm c ; gure 1 )  . 
treatment allocation was not masked . continuous oxaliplatin - based procedures two chemotherapy oncologists chose between regimens according to local hospital policy or patient the arm a ( n = 815 ) arm c ( n = 815 ) choice of chemotherapy at baseline capecitabine - based fluorouracil - based 536 ( 66% ) 279 ( 34% ) 533 ( 65% ) 282 ( 35% ) 525 ( 64% ) 290 ( 36% ) 523 ( 64% ) 292 ( 36% ) 63 ( 5669 ) 63 ( 5870 ) 74 ( 9% ) 69 ( 8% ) male female median ( years ) 75 years who performance status previous adjuvant chemotherapy none 16 months > 6 months yes ( unspeci ed ) site of primary tumour status of primary tumour resected unresected local recurrence metastases metachronous synchronous liver only liver and others non - liver more than two number of metastatic sites data are n ( % ) or median ( iqr )  . table 1 : baseline characteristics 375 ( 46% ) 378 ( 46% ) 62 ( 8% ) 608 ( 75% ) 36 ( 4% ) 128 ( 16% ) 43 ( 5% ) 445 ( 55% ) 331 ( 41% ) 39 ( 5% ) 249 ( 31% ) 552 ( 68% ) 174 ( 21% ) 436 ( 53% ) 198 ( 24% ) 283 ( 35% ) 326 ( 40% ) 199 ( 24% ) 375 ( 46% ) 378 ( 46% ) 62 ( 8% ) 608 ( 75% ) 36 ( 4% ) 131 ( 16% ) 40 ( 5% ) 419 ( 51% ) 350 ( 43% ) 46 ( 6% ) 241 ( 30% ) 567 ( 70% ) 179 ( 22% ) 430 ( 53% ) 200 ( 25% ) 284 ( 35% ) 329 ( 40% ) 196 ( 24% ) rectum 243 ( 30% ) 252 ( 31% ) preference . 
oxaliplatin plus capecitabine was given as a 3 - weekly regimen of intravenous oxaliplatin 130 mg / m over 2 h followed by oral capecitabine 1000 mg / m twice a day for 2 weeks . 
oxaliplatin plus uorouracil and folinic acid was given as a 2 - weekly regimen of intravenous l - folinic acid 175 mg or d , l - folinic acid 350 mg over 2 h given concurrently with oxaliplatin 85 mg / m over 2 h , followed by intravenous bolus uorouracil 400 mg / m , and nally uorouracil 2400 mg / m infusion over 46 h via an ambulatory pump . in arm a , treatment was continued until recistde ned progressive disease , development of cumulative toxic e ects ( precluding both oxaliplatin and uoropyrimidine use ) , or patients chose to stop . 
patients on arm c received chemotherapy for 12 weeks , after which treatment was stopped completely and the patients 644 vol 12 july 2011 articles 2445 patients enrolled 815 randomised to arm a 815 randomised to arm c 815 randomised to arm b 303 exclusions in the rst 12 weeks 69 deaths 104 progressive disease 60 came o trial for other specic reason 21 too few treatment cycles 49 no valid 12 - week assessment 290 exclusions in the rst 12 weeks 63 deaths 106 progressive disease 68 came o trial for other specic reason 17 too few treatment cycles 36 no valid 12 - week assessment a vs b comparison is reported in reference 9 512 had valid 12 - week assessment : result not progressive disease 525 had valid 12 - week assessment : result not progressive disease 45 excluded 14 excluded 2 one further cycle but only to complete original 12 - week period 1 lost to follow - up 13 protocol violation * 29 came o trial for other specic reason within 3542 days of 12 - week assessment 6 planned surgery 7 second - line therapy 3 clinician decision ( other than second - line ) 3 progression 4 toxic eects 3 intercurrent illness 3 patient decision 1 lost to follow - up 6 protocol violation * 7 came o trial for other specic reason within 3542 days of 12 - week assessment 2 planned surgery 2 second - line therapy 2 clinician decision ( other than second - line ) 1 other ( patient had bowel obstruction and needed a stent ) 467 pp analysis population 511 pp analysis population figure 2 : trial pro le pp = per - protocol . 
the intermittent strategy was that the same chemotherapy was to be restarted on con rmation of progressive disease ( with this scan becoming the new baseline measure ment )  . 
forms were scheduled to be completed at baseline ( before randomisation ) , 6 weeks , 12 weeks , and every 12 weeks thereafter ( before knowledge of ct scan results )  . the primary objective of this part of the coin trial was to establish whether intermittent therapy was noninferior to continuous therapy in terms of overall survival in patients with advanced colorectal cancer . 
the secondary aims were to evaluate failure - free survival ( of the treatment strategies ) , response , toxic e ects , quality of life , and cost - e ectiveness . 
the primary quality - of - life outcome measures were palliation , toxic e ects , functional scales , and global quality of life . statistical analysis the sample size for comparison of arm a versus c was 1614 patients ( 807 per arm )  . 
in the uk - based focus trial , 1 patients receiving continuous chemotherapy had 2 - year overall survival of 20% and a median overall survival of vol 12 july 2011 articles 100 075 050 025 100 075 050 025 arm a ( continuous ) arm c ( intermittent ) hr 1084 ( 80% ci 10081165 ; 95% ci 09701211 ) median survival ( months ) : arm a , 158 ; arm c , 144 ; one - sided 90% cl 136 ; non - inferiority limit 136 hr 1087 ( 80% ci 09861198 ; 95% ci 09361261 ) median survival ( months ) : arm a , 196 ; arm c , 180 ; one - sided 90% cl 163 ; non - inferiority limit 169 number at risk arm a 815 arm c 815 688 668 513 477 297 281 151 148 467 511 459 498 368 381 213 224 104 113 hr 1052 ( 80% ci 09821128 ; 95% ci 09471170 ) median survival ( months ) : arm a , 84 ; arm c , 74 hr 1075 ( 80% ci 09861173 ; 95% ci 09411229 ) median survival ( months ) : arm a , 92 ; arm c , 87 number at risk time ( months ) time ( months ) arm a 815 arm c 815 515 456 168 178 467 511 391 369 125 148 figure 3 : kaplan - meier curves for overall survival in ( a ) the itt population and ( b ) the per - protocol population , and strategy - failure - free survival in ( c ) the itt population and ( d ) the per - protocol population median survival in each arm is derived directly from the kaplan - meier curve . 
additionally , for overall survival we present median survival in arm c corresponding to the one - sided 90% ( ie , upper 80% ) con dence limit ( cl ) of the hazard ratio ( hr ) ; and for comparison , the limit of median survival regarded non - inferior with the pre de ned non - inferiority bound of hr 1162 . 
to show non - inferiority with a one - sided log - rank test with of 01 and power of 90% , 1420 patients would be needed ( 710 patients per arm )  . 
to account for the roughly 12% of patients who progress or who do not complete 12 weeks of treatment and therefore would not contribute to the comparison , the target sample size was increased to 807 patients per arm , and the analysis was timed to be done when at least 1168 overall survival events had occurred . 
stata were two - sided at a 95% signi cance ( version 11.1 ) was used for all statistical analyses . the primary question was one of non - inferiority , so both intention - to - treat ( itt ) and per - protocol analyses of overall survival were planned . 
the itt analysis included all patients randomly allocated to treatment groups , whereas the per - protocol analysis included patients who reached the point at which continuous and intermittent strategies divergedie , they received a full 12 weeks treatment ( allowing for one missed cycle ) , remained on trial , and had no evidence of progressive disease at 12 weeks ( within 4 weeks )  . 
 additionally , the patients included in the per - protocol analysis had to have adhered to the assigned protocol strategy at 12 weeksie , patients in arm a continuing treatment and those in arm c starting a chemotherapyfree interval . 
this population was de ned to correspond to the patient cohort who , when seen at the 12 - week timepoint ( outside a trial context ) , would bene t from discussion about whether to continue treatment or begin a chemotherapy - free interval . 
strategy - failure - free survival was de ned as the time from randomisation to failure time 646 vol 12 july 2011 articles equated this measure of the coin strategy to which a patient was randomly assigned ( webappendix p 3 )  . 
in the intermittent treatment group , a strategy - failure - free survival event occurred when a patient had progressive disease during a planned treatment period or within 8 weeks of starting a chemotherapy - free interval . 
 the primary analysis timepoint for quality of life was 24 weeks after randomisation , but baseline and 12 - week data were also analysed since these timepoints were milestones in the treatment strategy . 
ordinal logistic regression was used to predict 12 - week and 24 - week scores rounded into ve categories , adjusting for treatment arm and previous scores . we compared rates of toxic e ects between treatment groups using a test , or fishers exact test in case of low event rates ( n < 5 )  . 
to investigate the e ect of prespeci ed covariates on survival , we built prognostic models using a backward stepwise approach with critical value p = 005 for both removal from and re - entry into the model at each iteration . 
to investigate whether these covariates modi ed the treatment e ect , predictive models were tted that included the covariate , treatment arm , and a treatmentpredictive factor interaction term ; interaction tests were done with likelihood - ratio tests of the null hypothesis that the interaction coe cient is zero . this trial is registered , isrctn27286448 . role of the funding source the trial was conceived and developed by the national cancer research institute advanced colorectal clinical studies group . 
the corresponding author had full access to the data and had nal responsibility for the decision to submit for publication . results between march 9 , 2005 , and may 9 , 2008 , 2445 patients were randomly allocated to treatment groups at 111 centres in the uk and ireland , with 1630 patients assigned to the comparison of continuous versus intermittent treatment . 
 * in the coin dataset , the rst disease response assessment was at around 12 weeks ; therefore , patients with stable disease must have ( at least ) maintained this stability for that length of time . 
 table 2 : response at 12 weeks and best response in arms a and c and response after rechallenge ( arm c only ) 12 weeks 24 weeks or ( 95% ci ) p value or ( 95% ci ) p value functional scales impaired physical functioning impaired role functioning 113 ( 097130 ) 111 ( 097127 ) impaired cognitive functioning impaired social functioning 107 ( 092123 ) 105 ( 091120 ) impaired emotional functioning 114 ( 098131 ) 0086 101 ( 085120 ) 099 ( 083118 ) 089 082 ( 070096 ) 0015 090 024 090 ( 076107 ) 082 ( 070096 ) 0016 073 ( 062087 ) 000025 082 ( 068098 ) 0033 138 ( 116164 ) 000029 100 ( 084120 ) 094 ( 079111 ) 080 ( 067095 ) 082 ( 068099 ) 099 044 0012 0037 079 ( 066094 ) 0008 066 ( 055079 ) < 00001 011 013 037 052 075 065 066 040 019 028 028 079 062 016 083 046 102 ( 089117 ) 103 ( 090119 ) 103 ( 089120 ) 106 ( 092123 ) 110 ( 095126 ) 108 ( 094125 ) 109 ( 093128 ) 098 ( 085113 ) 104 ( 090119 ) problems eating or drinking 123 ( 100150 ) 0045 063 ( 047084 ) 00021 problems handling small objects 112 ( 096132 ) 054 ( 045065 ) < 00001 treatment interferes with daily activities 101 ( 089116 ) 062 ( 052073 ) < 00001 treatment felt to have been worthwhile 094 ( 080111 ) 120 ( 096150 ) 012 108 ( 093125 ) 030 098 ( 083115 ) 081 odds ratios ( ors ) are for arm c compared with arm a , and are from ordinal regression models adjusting for previous timepoints ( baseline , 12 weeks )  . 
ors greater than 1 indicate worse quality of life , and ors less than 1 indicate better quality of life . table 3 : quality of life at 12 and 24 weeks see online for webappendix and to arm c was 218 months ( 162295 )  . 
28 ( 7% ) of 383 surviving patients had no data returned for 12 months and were deemed lost to follow - up . 35 ( 2% ) patients did not start trial therapy because of clinical deterioration after randomisation , patient choice , or subsequent ineligibility after randomisation . 
in the per - protocol population , the geometric mean overall time on treatment in arm c was 52 months ( 95% ci 5054 ) versus 75 months ( 7378 ) in arm a ( p < 00001 )  . 
although total dose delivered of chemo therapeutic agents was greater in arm a than in arm c ( p < 00001 ) , dose intensity was in arm c during on - treatment periods greater ( p < 00001 )  . 
in treatment group , 325 ( 64% ) of 511 potentially eligible patients restarted a second 12 - week course of chemo therapy after a chemotherapy - free interval . intermittent the 1247 ( 77% ) deaths had occurred in the itt population at the time of analysis . 
median survival in the itt population was 158 months ( iqr 94261 ) in arm a and 144 months ( 80247 ) in arm c , and in the perprotocol population was 196 months ( 130281 ) in arm a and 180 months ( 121293 ) in arm c . 
the hr point estimates were 1084 ( 80% ci 10081165 ) in the itt population and 1087 ( 09861198 ) in the perprotocol population ; the upper limits were higher than the prede ned non - inferiority boundary ( gure 3 )  . 
 kaplan - meier overall survival in the itt population for arm a versus arm c was 287% versus 265% at 2 years and 130% versus 112% at 3 years . 1166 ( 94% ) of 1247 deaths in the itt population were due to colorectal cancer . 
22 ( 2% ) deaths were reported to be treatment - related , 52 ( 4% ) were from other causes , and the cause of death for the remaining seven ( < 1% ) is currently unknown . 
70 ( 6% ) deaths occurred within 60 days of randomisation , with no di erence between the two groups . median strategy - failure - free survival the itt population was 84 months ( iqr 53118 ) in arm a and 74 months ( 51121 ) in arm c , and in the perprotocol population was 92 months ( 70129 ) in arm a and 87 months ( 59134 ) in arm c . 
from the kaplan - meier plots ( gure 3 ) , intermittent therapy seemed to result in a greater loss of patients ( in terms of strategy ) early on , especially around 69 months , but at 2 years there was little di erence in number of patients remaining on strategy : 2 - year survival in the itt analysis was 74% ( n = 28 ) in the continuous treatment arm and 76% ( n = 35 ) in the intermittent treatment arm , and in the per - protocol analysis was 77% on continuous ( n = 18 ) and 76% on intermittent ( n = 24 ) treatment . among patients in the per - protocol population allocated intermittent treatment who commenced a chemotherapyfree interval ( n = 511 ) , the median time to progression was 129 weeks ( 30 months ; iqr 109240 weeks )  . 
among those who later restarted trial therapy ( n = 325 ) , the median overall length of the chemotherapy - free interval before progression was 160 weeks ( 37 months ; iqr 137260 weeks )  . 
the median number of chemotherapy - free intervals was two ( range one to six )  . protocol treatment in both treatment groups was identical up to 12 weeks ( the time of the rst scheduled radiological disease assessment )  . 
best overall response ( by recist criteria ) did not di er between treatment groups , suggesting that most patients achieve best response within the rst 12 weeks of therapy . 
grade 3 or worse peripheral neuropathy and hand foot syndrome were more frequent during continuous treatment ( webappendix p 4 )  . there were fewer eligible patients in arm c ( 79% , n = 647 ) than in arm a ( 89% , n = 724 ; p < 00001 ) , since more patients in arm c either remained on trial therapy ( 6% vs 1% in arm a , n = 46 vs nine , p < 00001 ) or died ( 14% vs 9% in arm a , n = 115 vs 74 , p = 00015 )  . 
among patients judged eligible to receive second - line therapy , this treatment was given to signi cantly fewer patients on intermittent therapy ( 52% , n = 336 ) than on continuous therapy ( 62% , n = 448 ; p = 000020 )  . quality of life in the per - protocol population at baseline , 12 weeks , and 24 weeks was assessable in 279 ( 60% ) patients on continuous treatment and 282 ( 55% ) patients on intermittent treatment . 
no clear evidence of di erences in baseline characteristics was identi ed between those patients who completed quality - of - life questionnaires and all patients randomly allocated to treatment groups , but the risk of such di erences cannot be eliminated . 
after adjustment for previous measurements , there were signi cant bene ts from intermittent therapy at 24 weeks for fatigue , dry or sore mouth , problems eating and drinking , di culty handling small objects , interference with daily activities , nausea or vomiting , appetite loss , constipation , and diarrhoea ( table 3 ; p < 005 for all )  . 
at 12 weeks , there was a nonsigni cant trend towards an adverse e ect of intermittent therapy on emotional functioning ( p = 0086 ) , but this result was not evident at 24 weeks ( p = 090 ; table 3 )  . we undertook a post - hoc exploratory analysis of the e ects of protocol adherence on overall survival . 
a cuto of 60% was chosen because this proportion formed a pragmatic and appropriate benchmark midway between the 40% and 80% of restarts reported in optimox - 1 and optimox - 2 , respectively . 
 however , this di erence lessens over time and the overall hr is non - signi cant ( gure 4 )  . favours intermittent therapy favours continuous therapy figure 5 : subgroup analyses of overall survival within the per - protocol population hr = hazard ratio . 
the nal model contained the following previously identi ed prognostic variables : previous adjuvant chemotherapy or surgery ; alkaline phosphatase ; body surface - area ; platelet count ; time from diagnosis to vol 12 july 2011 articles 100 075 050 025 normal platelet count ( < 400 000 per l ) raised platelet count ( 400 000 per l ) arm a ( continuous ) arm c ( intermittent ) hr 0961 ( 80% ci 08541080 ; 95% ci 08031150 ) , p = 0660 hr 1545 ( 80% ci 12921848 ; 95% ci 11752031 ) , p = 00018 number at risk time ( months ) time ( months ) arm a 332 arm c 371 327 365 265 295 158 185 133 138 130 131 101 figure 6 : kaplan - meier curves of overall survival within the per - protocol population , by baseline platelet subgroup interaction with treatment arm : hazard ratio ( hr ) 1646 ( 95% ci 11882279 ) ; p = 00027 . randomisation ; resection of primary tumour ; mutation present in any of kras , nras , or braf ; and number of metastatic sites . 
in particular , each of the four variables identi ed by khne and colleagues13 were present with the exception of white blood cell count ( in our data , platelet count was a stronger prognostic indicator ) , and the score de ned by khne was strongly prognostic ( p < 00001 for trend )  . 
a raised platelet count at baseline ( 400 000 per l , recorded for 271 [ 28% ] of 978 patients ) predicts a signi cant survival detriment from intermittent chemotherapy ( p = 00027 for interaction ; gure 6 )  . 
raised baseline platelet count had an even greater predictive e ect for a detriment from intermittent therapy on 24 - week quality of life , particularly for functional scales ( p < 005 for all ) , for which a consistent trend was noted towards bene t from intermittent therapy for patients with normal platelet count and an adverse e ect for patients with raised platelet count . 
additionally , the symptom scales of fatigue , pain , dyspnoea , appetite loss , constipation , and global quality of life followed this trend ( p < 005 for all )  . 
furthermore , patients on intermittent therapy were signi cantly more likely than were those on continuous therapy to report at 24 weeks that their treatment had not been worthwhile if their baseline platelet count was raised ( p = 0048 for interaction ; webappendix p 7 )  . 
other factors with interactions signi cant at the 10% level were presence of metastases in the liver only ( p = 0066 ) and tumoral kras status ( p = 0070 )  . discussion the goal of palliative chemotherapy is to increase overall survival with improvement or minimum de cit in quality of life . 
the trial did not meet its primary outcome objective , which was to show non - inferiority intermittent chemotherapy versus continuous chemotherapy as rst - line in advanced colorectal cancer . 
however , there seems to be a large subpopula tion of patients for whom intermittent therapy provides similar survival bene t and can be recommended . therapy that the coin trial has shown intermittent chemotherapy is associated with improved quality of life , shortened time on chemotherapy , reduced number of visits to hospital , and a minimum di erence in overall survival . 
in coin , we developed a statistical plan that set the outer bound of the hr for non - inferiority for overall survival at the rigorous level of 1162 ( for comparison , the outer bound in the comparison of uorouracil versus capecitabine in the x - act trial was 125 ) .14 the trial did not meet this strict criterion ( upper limit of hr in the itt group was 1165 )  . 
this 650 vol 12 july 2011 articles result does not suggest that continuous chemotherapy is superior to an intermittent strategy , but does translate into an observed di erence in median overall survival of around 6 weeks ( 14 months ) , favouring continuous therapy . 
our con dence intervals reliably exclude a detriment greater than 22 months ( itt analysis ) or 32 months ( per - protocol analysis ) in median overall survival with intermittent therapy . the striking outcome from the study is the signi cant correlation of a raised baseline platelet count as a predictive biomarker for use of a continuous or intermittent chemotherapy strategy . 
a quarter of patients had a raised platelet count at baseline and these patients had substantially inferior survival ( a 5 - month reduction in survival ; test for interaction p = 00027 ) when treated with intermittent chemotherapy and also impaired quality of life on almost all scales apart from those directly related to toxic e ects of chemotherapy . 
raised platelet count has previously been identi ed as a poor prognostic marker in advanced colorectal cancer.13 the mechanism could relate to paracrine feedback driven by cytokines including interleukin 6 , directly causing throm bocytosis.15 it could , alternatively , relate to an aspect of immunomodulation driven by t - regulatory cells and foxp3 epigenetic regulation.16 if con rmed in other datasets , the easily measurable marker of a raised platelet count at initiation of chemotherapy would be a helpful and cost - e ective predictive biomarker for identi cation of patients in whom continuous therapy might be preferable in order to maximise symptom control and survival . the shorter overall survival in this uk trial compared with some other trial settings is probably related to a combination of several factors , such as a more advanced distribution of disease at presentation , fewer available e ective treatments , or di erent attitudes of patients and clinicians to additional therapy . 
a recent report17 shows from registry data that survival for colorectal cancer is lower in the uk than for other comparable countries ( for 1 - year survival uk registries reported 75% compared with 8085% for the other registries in the comparable years 200507 ; 54% vs 5866% at 5 years )  . 
since coin recruited widely from 111 centres across the uk and ireland and had broad inclusion criteria , it is likely to be representative of outcomes for advanced colorectal cancer in the uk . failure to restart oxaliplatin - based chemotherapy after an interval has previously been identi ed as detrimental to survival.18 in the coin per - protocol population ( ie , patients clinically eligible to recommence chemotherapy ) , 325 ( 64% ) of 511 potentially eligible patients restarted a second 12 - week course of chemo therapy . 
this proportion compares with a reintroduction rate of 40% in optimox - 17 and 80% in optimox - 2 , which recruited patients from only 12 centres and in which high rates of reintroduction were protocol mandated.8 the gure of 64% from the coin trial could reason ably represent a good re ection of real practice in an incurable disease , in which chemotherapy must strike a balance between quality and length of life . 
the proportion of coin patients restarting oxaliplatin and the low numbers receiving second - line chemotherapy regimens compared with some other countries re ects a less aggressive approach that is characteristic of uk oncology and could also have contributed to the lower overall survival . additionally , the predominantly uk study setting is important in that bevacizumab was not reimbursed for rst - line treatment or subsequent use in routine nhs practice during the study period , and although its availability would probably have resulted in longer overall survival , the e ect of addition of this targeted agent on a chemotherapy - free interval strategy is unclear . 
in the aio trial , 20 patients are randomly allocated to one of three arms ( bevacizumab plus uoropyrimidine , bevacizumab alone , or no treatment after 24 weeks of induction oxaliplatin uoropyrimidine and bevacizumab ) and complete accrual is due in 2013 . 
however , our message that omission of chemotherapy for long periods in selected patients without overall survival interpreted cautiously vol 12 july 2011 articles panel : research in context systematic review conventional palliative chemotherapy for treatment of advanced colorectal cancer is given continuously until progressive disease or cumulative toxic e ects occur , or the patient chooses to discontinue . 
in a previous medical research council study , cr06b , 5 a shortened course of chemotherapy with reuse of the same treatment on progression showed an improvement in quality of life with no loss of survival . 
one consistent nding is that patients receiving short - course therapy can have a reduced time to disease progression , but several investigators have reported that at the time of progression patients can be successfully rechallenged with the same regimen . 
searches of medline and cancerlit for publications and pdq ( physicians data query ) and the ukcccr trial register for any additional open or closed trials in advanced colorectal cancer found no trials comparing these approaches when this trial was started . interpretation survival in coin is shorter than for many international trials in advanced colorectal cancer , which probably re ects a more advanced stage of disease at presentation in the uk . 
additionally , the lack of routine availability of biological agents in the uk national health service might contribute to shortened survival and therefore restrict direct application of the coin data in the most resource - rich health - care settings . 
the nding that intermittent chemotherapy is inferior in patients with raised platelet counts is novel and needs con rmation , but supports the conventional practice of continuous chemotherapy for this cohort . 
conversely , for most patients with normal platelet counts at baseline , this study suggests that chemotherapy - free intervals are associated with improved quality of life and no loss of overall survival and is therefore an option that clinicians should discuss with such patients . de cit could be even more relevant in such contexts . 
 potential bene ts from the continuation of such targeted agents with or without the addition of a uoropyrimidine , when oxaliplatin temporarily discontinued , have yet to be shown in terms of progression - free or strategy - failure - free survival or more importantly in terms of overall survival in any completed randomised controlled trials ; such data are eagerly awaited . standard uk practice is to image patients at 12 - week intervals . 
during treatment breaks , patients in arm c attended hospital as outpatients or day cases on an average of two occasions every 1224 weeks , whereas those in arm a would have been seen on at least eight occasions and possibly 12 depending on the chemotherapy regimen . 
this more frequent clinical review could have led to earlier identi cation of disease progression . the secondary and subgroup analyses of the trial are intended to o er some guidance to practising clinicians , patients , and patient advocates . 
the overall e ect on quality of life with time o treatment in arm c , as assessed at the speci c timepoints of 12 and 24 weeks , suggest an improvement in fatigue , nausea and vomiting , anorexia or loss of appetite , constipation , diarrhoea , dry or sore mouth , and di culty handling objects . 
however , pain seems to be slightly but consistently more frequent in those receiving the intermittent strategy , which could be accounted for by the increased likelihood of tumour progression or activity during a chemotherapy - free interval . 
yet this nding disappears at 24 weeks , when those on continuous therapy may be uncertain about continuing e ectiveness or tolerability of ongoing treatment . initial 12 - week period of in advanced colorectal cancer , for patients treated with palliative intent , as in most other malignancies , time o chemotherapy remains a treatment option . 
this study has shown and quanti ed the bene ts of a chemotherapyfree interval in terms of reduced time on chemotherapy , reduced cumulative toxic e ects , and improved quality of life after an induction chemotherapy . 
by contrast , the three - quarters of patients in coin with normal platelet counts at randomisa tion su ered no loss in overall survival and could reap potentially important bene ts of chemotherapyfree intervals . contributors raa was the trial fellow , member of trial management group , reviewed all safety events , and co - wrote the report . 
sf , sg , th , emb , and dp were the highest recruiting oncologists to the trial and mjk was the lead oncologist for the sites in ireland and contributed to trial management . 
all authors reviewed all the data and commented on the report . 652 vol 12 july 2011 articles con icts of interest raa and tsm have received travel , accommodation , and lecture fees from roche and merck serono . 
th has received travel expenses , meeting attendance , and lecture fees from glaxosmithkline , novartis , sano , roche , p zer , and abraxis and also payment for manuscript preparation from the british journal of healthcare . 
this long - awaited once in a generation opportunity to put ncds on the global agenda generated as many fears of a missed opportunity as it did hopes of a turning point for the health of millions around the world . 
the unanimous agreement by un member states to hold the summit on ncds signalled recognition of a growing global emergency and , at long last , a willingness to act . 
although often thought of as diseases of rich countries , ncds now disproportionately a ect more people in poorer nations , accounting for 80% of all ncd - related deaths . 
ncds include cancers , cardiovascular diseases , diabetes , and chronic respiratory diseases : all are largely preventable and share common risk factors , such as tobacco use , unhealthy diet , physical inactivity , and harmful use of alcohol . 
furthermore , the world economic forum identi ed ncds as a severe threat to economic development and put a price tag of $30 trillion on the expected burden of these diseases over the next 20 years . 
 the aim of the meeting was to secure commitment from heads of government for a coordinated global response , to raise awareness among the general public , and to adopt a comprehensive political declaration for health strategies . 
notably , governments decided to commit to multisectoral national and international policies to control ncds , to reduce individual exposure to ncd risk factors through international agreements such as the who framework convention on tobacco control , the who global strategy on diet , physical activity and health , and the who global strategy to reduce the harmful use of alcohol , to give greater priority to early detection , screening and diagnosis , to increase access to vaccines as part of national immunisation programmes , and to improve access to palliative care . 
 industry these commitments should be applauded as a good start in tackling the serious burden that ncds represent , and signal the start of attempts to reverse the undue long - term neglect the political arena has a orded such issues . 
 indeed , although the fundamental con ict of interest between the tobacco industry and public health is fully recognised in the declar ation , other groups from the food and drink industrywhich the un euphemistically refers to as civil society alongside organisations such as academiawere invited to participate in the meeting , although they were excluded from any decision - making . 
 in preparation for the meeting , the uiccas part of the ncd allianceproposed very speci c targets that could have been included , such as a commitment by 2025 to reduce avoidable deaths from ncds by 25%a target who believes is achievable . 
instead , the document calls on who simply to set up a comprehensive global monitoring framework and prepare recommendations for voluntarynot compulsoryglobal targets before the end of 2012 , and to report initial progress in 2013 . 
overall e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against grade 3 or greater cervical intraepithelial neoplasia : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 8999in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
cross - protective e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against cervical infection and precancer caused by non - vaccine oncogenic hpv types : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 10010in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
lancet oncol 2012 ; 13 : 1012in this comment ( published online nov 9 , 2011 ) , the last sentence of the sixth paragraph incorrectly lists hpv - 35 as one of the oncogenic hpv types covered by the new nine - type gardasil vaccine ; the list should include hpv - 45 instead . 
this correction has been made to the online version as of jan 3 , 2012 . vol 13 january 2012 editorial for more on the world cancer declaration see comment lancet oncol 2011 ; 12 : 109192 for more on global cancer transitions see articles lancet oncol 2012 ; 13 : 790801 cancer awareness campaigns : dispelling the myths feb 4 marks world cancer day 2013 , an annual event that aims to raise awareness of cancer and to encourage in prevention , detection , and treatment . 
 e orts this years theme focuses on item ve of the world cancer declaration , adopted by the united nations in 2011 , which aspires to dispel damaging myths and misconceptions about the disease . four key myths are highlighted . 
these changes a ect not only individuals , but also threaten the economic development of communities and countries and , in turn , progress towards achieving the 2015 millennium development goals . 
improvements in early detection and treatment mean that many patients diagnosed with the disease can be treated e ectively and survive indeed , there are nearly 30 million cancer survivors worldwide . 
better understanding of risk factors and increased prevention e orts o er cost - e ective and sustainable means to reduce the global cancer burden in the longer ter in 2013 that such erroneous beliefs persist alarming . 
in the wake of the adoption of the world cancer declaration , the union for international cancer control ( uicc ) and its members set out a number of actionable goals for each of the declarations items . 
 for item ve , they aimed to develop and implement , by 2015 , public awareness and education programmes that seek to eliminate any stigma associated with cancer and to provide information about the methods and e ectiveness of early cancer detection combined with e ective therapy . 
such aims are laudable , and their achievement essential if misconceptions about cancer are to be eliminated . however , the uicc plans to direct e orts at the primary health - care level . 
given that many of the myths they aim to tackle may discourage individuals from presenting to primary care in the rst place , and that barriers exist to access of such care in some countries , e orts must also be focused elsewhere . 
campaigns must be aimed at the general publicas exempli ed by the uk department of healths latest anti - smoking campaign , with adverts running on all of the major commercial television channels in the uk , which feature graphic images of tumours growing on cigarettes as individuals smoke thea further example is provided by change4life , a social marketing campaign run by the national health service in england and wales . 
in the wake of the festive period , the campaign has been expanded to advocate better eating habitscutting back on fat and salt intake , eating more fruit and vegetables , and swapping sugarladen treats for healthier alternatives . 
 although undoubtedly useful , both these population - level awareness campaigns serve as examples of a common problem with such exercisesthe link to cancer , heart disease , and other conditions is implied , but not stated explicitly . 
better attempts at educating the public as to the implications of making these changes might also alleviate the concerns of some individuals that such campaigns are a symptom of the government intervening unduly with personal choices . improvements in particular focusing on educationat all levels , from the a ected individual , through to communities , governments , and beyondis vital if we are to debunk misconceptions and improve awareness of cancer and its hidden costs . 
 the lancet oncology in communication , vol 14 february 2013 comment all authors have received grant support from novartis switzerland for clinical trials of blood - concentration testing of imatinib . 
additionally , nw has received travel and accommodation support from novartis switzerland , and lad has received honoraria from novartis for blood - concentration testing of imatinib . us food and drug administration . 
enforcementactions / warningletters / ucm210191.htm ( accessed oct 10 , 2010 )  . larson ra , druker bj , guilhot f , et al , for the iris ( international randomized interferon vs sti571 ) study group . 
population pharmacokinetics of imatinib and the role of 1 - acid glycoprotebr j clin pharmacol 2006 ; 62 : 97112 . petain a , kattygnarath d , azard j , et al , for the innovative therapies with children with cancer european consortiupopulation pharmacokinetics and pharmacogenetics of imatinib in children and adults . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zhao f - h , lin mj , chen f , et al . 
performance of high - risk human papillomavirus dna testing as a primary screen for cervical cancer : a pooled analysis of individual patient data from 17 population - based studies from china . 
 lancet oncol 2010 ; 11 : 116071on page 1165 of this article , the right hand panel of gure 1a should state pooled speci city = 864% ( 838890 ) and the right hand panel of gure 1b should state pooled speci city = 851% ( 823879 )  . 
in table 1 of this review , data from hertel et al ( 2006 ) for number of conceptions , rst trimester loss , and deliveries , and from shepherd et al ( 2006 and 2008 ) and dargent et al ( 2007 and 2008 ) for number of deliveries were incorrect . 
 vol 12 january 2011 articles cognitive behavioural treatment for women who have menopausal symptoms after breast cancer treatment ( menos 1 ) : a randomised controlled trial eleanor mann , melanie j smith , jennifer hellier , janet a balabanovic , hisham hamed , elizabeth a grunfeld , myra s hunter summary background hot ushes and night sweats ( hfns ) a ect 6585% of women after breast cancer treatment ; they are distressing , causing sleep problems and decreased quality of life . 
we investigated whether cognitive behavioural therapy ( cbt ) can help breast cancer survivors to e ectively manage hfns . methods in this randomised controlled trial , we recruited women from breast clinics in london , uk , who had problematic hfns ( minimum ten problematic episodes a week ) after breast - cancer treatment . 
randomisation was done in blocks of 1220 participants , stratifying by age ( younger than 50 years , 50 years or older ) , and was done with a computergenerated sequence . 
group cbt comprised one 90 min session a week for 6 weeks , and included psycho - education , paced breathing , and cognitive and behavioural strategies to manage hfns . 
the trial is registered , isrctn13771934 , and was closed march 15 , 2011 . findings between may 5 , 2009 , and aug 27 , 2010 , 96 women were randomly allocated to group cbt ( n = 47 ) or usual care ( n = 49 )  . 
group cbt signi cantly reduced hfns problem rating at 9 weeks after randomisation compared with usual care ( mean di erence 167 , 95% ci 243 to 091 ; p < 00001 ) and improvements were maintained at 26 weeks ( mean di erence 176 , 254 to 099 ; p < 00001 )  . 
we recorded no cbt - related adverse events . interpretation group cbt seems to be a safe and e ective treatment for women who have problematic hfns after breast cancer treatment with additional bene ts to mood , sleep , and quality of life . 
hfns are more severe in this population than they are in healthy women and have a negative e ect on quality of life , mood , and sleep.24 chemotherapy or adjuvant endocrine treatments can compromise or lead to failure of ovarian function , resulting in rapid reduction of oestrogen concentrations , which induces or exacerbates hfns . 
 hfns can in turn reduce adherence to endocrine therapy if left untreated.57 hormone replacement is an e ective treatment for hfns , but is generally contraindicated for patients with breast cancer because it can increase the risk of breast cancer recurrence , and hfns can return in women who discontinue hormone replacement therapy ( ssris ) , and therapy.8 a cochrane review of non - hormonal medical treatments concluded that clonidine ( an antihypertensive drug ) , gabapentin ( an anticonvulsant that works through an unknown mechanism ) , selective serotonin reuptake inhibitors serotonin - norepinephrine reuptake inhibitors ( snris ) showed a mild to moderate e ect on the frequency of hfns in women with a history of breast cancer ( reductions of between 15% and 58% ; average 37% ) .9 three trials done since the review was undertaken recorded similar reductions.1012 various side - e ects of medical treatments were reportedeg , dry mouth , sleep problems , and nauseaand short follow - up long - term conclusions outcomes.9 some ssris ( paroxetine and uoxetine ) , but not all , might reduce the e ectiveness of endocrine treatments.13 evidence of improvements to quality of life is mixed ; six of 12 studies of non - hormonal drugs reported no e ect.1012 , 14 moreover , many breast cancer survivors prefer treat ments.3 therapieseg , vitamins , for non - pharmacological magnetic devices , or acupuncturethe cochrane review to use non - medical limited about vol 13 march 2012 articles for the trial protocol see 2407 / 11 / 44 concluded that outcomes were either inconsistent or not statistically signi cant.9 consequently , a need exists for safe , acceptable , and e ective non - hormonal treatments that are free from side - e ects to help these women to manage hfns.15 , 16 an intervention based on cognitive behavioural therapy ( cbt ) has been developed , 17 including psychoeducation , paced breathing and relaxation , and cbt to help women to manage hfns . 
this intervention has been shown to be acceptable to women and has shown promise in exploratory trials of one - to - one and group cbt.17 , 18 the treatment is based on a model of the hypothesised causal mechanisms and maintaining factors of hfns , which include anxiety , stress , embarrassment , negative beliefs , catastrophic thoughts , and avoidance behaviours.19 , 20 in a pilot , uncontrolled trial of group cbt , 17 women who had been treated for breast cancer reported an average 49% reduction in hfns problem rating and a 38% reduction in self - reported hfns frequency.18 hfns frequency has generally been considered to be the target of treatments , but studies have suggested that problem rating ( ie , the extent to which hfns are bothersome and interfere with life ) should be the primary outcome in clinical trials because it is associated with help - seeking behaviour and quality of life to a greater extent than is frequency of hfns.21 , 22 sternal skin conductance ( ssc ) monitoring is the most valid physiological measure of hfns , but is rarely included in trials . 
subjective and physiological measures assess di erent aspects of hfns.23 menos 1 is a randomised controlled trial of group cbt compared with usual care with a 26 - week follow - up . 
we hypothesised that participants would report less problematic hfns and fewer hfns , improved mood , sleep , and health - related quality of life after group cbt compared with individuals who received usual care . 
we measured subjective frequency and problem rating of hfns and ssc monitoring of hfns frequency , to establish whether the treatment a ects physiological or psychological factors , or both . methods study design and participants the study design is described in detail in the trial protocol.20 brie y , recruitment took place between march 17 , 2009 , and aug 27 , 2010 . 
 they could also apply for inclusion by responding to lea ets and posters displayed in clinics . english - speaking women older than 18 years were eligible if they had had at least ten problematic hfns per week ( con rmed by a 2 - week diary and a screening interview ) for a duration of 2 months or more , had completed medical treatment for breast cancer ( surgery , radiotherapy , or chemotherapy ) , and had no evidence of other cancers or metastases . 
because many women use treatments for hfns but still have troublesome symptoms and seek further treatment , they were not excluded if they had been using the treatment consistently for 2 months or more , and planned to continue at the same dose during the trial . 
after base line assessment and receipt of consent from 1220 par ticipants , the trial clinical psychologist ( mjs ) sent participants identi cation details to a programmer at the clinical trials unit at kings college london , uk , for randomisation . 
the programmer created a computer - generated random isation sequence , allocating participants in a one - to - one ratio , strati ed by age ( < 50 years , 50 years ) , with randomly varying block size . 
 speci cally , at 9 - week and 26 - week assessments , women were met by a separate researcher who collected questionnaires and who also asked the women not to disclose their treatment allocation to the researcher who did the outcome assessments . 
to check whether the trial coordinator ( em ) was successfully masked , after 9 - week assessments for each cohort she noted which group she thought participants had been allocated to . 
the trial statistician was masked to group identity until analyses were complete . procedures assessments took place at baseline , 9 weeks after randomisation ( typically 2 weeks after treatment ) , and 26 weeks after randomisation . 
about 2 weeks before participants attended a baseline assessment , a researcher explained the study , assessed eligibility by telephone , and posted written information and a 2 - week diary to be updated on a daily basis to record hfns frequency . 
at baseline assessment , eligibility was con rmed ; participants were able to ask questions before signing a standard consent for women were asked about their breast cancer treatment history , menopause symptoms , and medical history . 
they completed a questionnaire covering 310 vol 13 march 2012 articles demographic characteristics and baseline measures and were given a small ssc monitor and a magnetic event marker bracelet worn for 24 h . 
they were asked to indicate when they had an hfns by passing the magnet over the monitor ; they were encouraged to do usual activities and were shown how to remove the monitor to shower or bathe . participants allocated to receive group cbt attended a 90 min session every week for 6 weeks , between june , 2009 , and october , 2010 ( panel 1 )  . 
all sessions were audio taped , then 10% were randomly selected ( with a computer - generated random number sequence ) and a psychologist ( msh ) experienced in cognitive behavioural therapy for hfns , rated them for adherence to the treatment manual , by indicating on coding sheets the extent to which the group leader covered each topic . 
coding sheets included speci c components of the intervention ( eg , reviewing home work , providing information about the role of stress , demonstrating paced breathing in the session , group discussion of behaviours relating to hfns ) developed for the trial ( appendix )  . all participants received usual carethey had access to clinical specialists and cancer support services , either through routine follow - up appointments or as part of a breast cancer survivorship programme in southeast london ( panel 1 )  . 
 at 26 weeks after randomisation , questionnaires were sent containing the same measures ; face to face or telephone interviews were done by an independent psychologist after nal measures were completed to obtain womens responses to being in the trial and their views about the treatment ( for those in the cbt group )  . 
follow - up was completed by march 15 , 2011 . outcomes the primary outcome was the hfns problem rating ( hot ush rating scale24 ) at 9 weeks after randomisation . 
 problem ratingie , the extent to which symptoms are bothersome and interfere with lifewas chosen , before the trial began , 20 as the primary outcome measure because problem rating , rather than frequency , is associated with help - seeking and quality of life , and it has been recommended as the most appropriate patientreported outcome measure in clinical trials of hfns panel 1 : intervention content group cognitive behavioural therapy ( cbt ) the group cbt was psycho - educational , structured , and interactive with presentations , group discussion , handouts , and weekly homework . 
paced breathing and relaxation were practised at each session and participants were given a relaxation and paced breathing audio cd to practise at home daily and during hot ushes and night sweats ( hfns )  . 
 women recorded their hfns in weekly diaries . session one introduced the cognitive behavioural model including physiological , cognitive , behavioural , and emotional components of hfns ; provided information about the physiology of hfns ; and introduced paced breathing . 
participants described their experiences of hfns in the context of breast cancer , outlined their goals for treatment , discussed and recorded particular triggers of hot ushes , and practised relaxation . session two focused on the role of stress in potentiating hfns and cbt strategies for the reduction of stress and anxiety . 
paced breathing was introduced and practised as homework . session three focused on cognitive ( eg , catastrophic thinking and overly negative beliefs about hot ushes ) and behavioural reactions ( eg , avoidance of activities ) to hot ushes . 
they also completed sleep diaries in preparation for the sleep sessions . session four focused on understanding night sweats and improving sleep habits and the application of behavioural strategies to reduce wakefulness after night sweats . 
 participants identi ed ways in which they could change sleep habits , which they implemented as homework . session ve focused on the cognitive component of sleep problems , including sleep - related anxieties or general worries leading to further wakefulness . 
cbt strategies were developed for the management of night sweats . session six was a review session and participants made action plans to maintain cognitive and behavioural changes , including dealing with setbacks . usual care all women had completed active breast cancer treatment and were typically followed up every 6 months by an oncologist or clinical nurse specialist , with additional appointments as needed . 
women were sent an information lea et produced by breast cancer care and o ered telephoned support every 2 weeks ( average seven telephone calls , maximum ten )  . 
the remainder were no longer attending follow - up appointments at the hospital ( n = 7 ) , or were not treated at hospitals in the southeast london cancer network ( n = 12 )  . 
therefore , individuals in the usual care group received information and had access to high quality support services . see online for appendix treatments.21 , 22 problem rating and severity tend to be associated with each otherneither are strongly associated with frequency of hfns.21 secondary outcomes included hfns problem rating at 26 weeks , and hfns frequency , mood , and healthrelated quality - of - life measures at 9 weeks and 26 weeks after randomisation . 
problem rating of hfns ( hot ush rating scale24 ) was calculated as the mean of three 10 - point items that assess the extent to which symptoms vol 13 march 2012 5 chose not to participate mean body - mass index ( kg / m ; sd ) 2713 ( 530 ) 2751 ( 690 ) articles 278 screened for eligibility 177 excluded 79 not meeting inclusion criteria 18 symptoms not problematic 5 cancers had metastasised 8 unable to attend cbt sessions 20 lived too far away 19 never had breast cancer 1 died 8 undergoing cancer treatment 98 chose not to participate 101 consented to take part and completed baseline assessment 96 randomly allocated to treatment 47 cognitive behavioural therapy 6 in cohort one 9 in cohort two 7 in cohort three 7 in cohort four 6 in cohort ve 6 in cohort six 6 in cohort seven 49 usual care 5 in cohort one 10 in cohort two 7 in cohort three 7 in cohort four 6 in cohort ve 7 in cohort six 7 in cohort seven 1 unable to attend 1 ill health 1 symptoms ceased 1 chose not to participate 1 chose not to participate 1 died 2 could not be contacted at week 9 43 completed hfrs at week 9 45 completed hfrs at week 9 40 completed hfrs at week 26 40 completed hfrs at week 26 43 analysed 45 analysed figure 1 : trial pro le cbt = cognitive behavioural therapy . 
a di erence of two points or more is regarded as clinically relevant.17 , 18 , 25 the scale has good internal consistency ( cronbach = 09 ) and testretest reliability ( r = 08 )  . 
 a 6 - cm by 6 - cm monitor measured ssc every 10 s by passing an electric current across two electrodes attached to the sternal region of the chest . 
this is the standard criteria used for ssc monitoring validated with ambulatory and laboratory equipment.23 the sum of physiological and participantreported ( event - marked ) hfns were extracted for analysis . 
hfns = hot ushes and night sweats . table 1 : demographic and clinical baseline characteristics 312 vol 13 march 2012 articles cognitive behavioural therapy ( mean [ sd ] ) usual care ( mean [ sd ] ) cbt vs usual care * ( adjusted mean di erence [ se , 95% ci ; p value ] ) baseline 9 weeks 26 weeks 652 ( 243 ) 353 ( 198 ) 313 ( 194 ) 612 ( 202 ) 495 ( 224 ) 460 ( 248 ) 167 ( 039 , 243 to 091 ; < 00001 ) 176 ( 040 , 254 to 099 ; < 00001 ) * adjusted analysis used cohort number as a random e ect and a covariate for the binary age strati cation factor . table 2 : hot ush and night sweats problem - rating scores usual care cognitive behavioural therapy week 9 week 26 time from randomisation figure 2 : changes in problem - rating scores for hot ushes and night sweats error bars show 95% cis . treat sample ( excluding those who contributed no data )  . 
 we assessed the primary outcome with a linear mixed model ; covariates were treatment group , baseline hfns problem rating score , the strati cation factor age ( as a dichotomous category , split at 50 years ) , and time . 
we also analysed secondary outcomes with mixed linear regression models with random participant and cohort group intercepts and a time - by - treatment interaction term ; covariates in the model were treatment group , baseline value of outcome , the stratication factor age , and time . 
 participants rate each item on a 4 - point scale , according to the extent to which they are experi encing each item , and subscale scores are calculated , ranging from 01 ( higher scores indicate poorer wellbeing )  . 
the depressed mood subscale has concurrent validity with the ghq and the whq has good internal reliability for subscales ( cronbach 070084 ) and test - retest reliability ( 078096 )  . 
we also included measures of process variables including beliefs , behaviours , and stress , which are described elsewhere.20 adherence to group cbt was measured by the number of sessions attended and the number of times that a participant practised relaxation or paced breathing each week . 
recurrence of breast cancer , skin irritation due to the hot ush monitor , and clinically signi cant deterioration in mood were identi ed as possible expected unrelated adverse events , and clinically signi cant deterioration in mood as a result of group cbt was identi ed as a potential treatment - related adverse event . 
recurrence of breast cancer or secondary cancers were classi ed as expected but unrelated serious adverse events.28 statistical analysis we calculated that a sample size of 96 women was needed to provide 90% power to detect a two - point di erence ( sd 24 ; standardised e ect size 08 ) in mean hfns problem rating for the comparison of cbt to usual care at 9 weeks after randomisation . 
this sample size allowed for 20% loss to follow - up , a variance in ation factor of 149 ( intraclass correlation 007 , 29 eight participants per group ) to power for expected clustering of outcomes , and an hfns problem rating baseline - to - outcome correlation of 04 on analysis of covariance with two - sided 5% signi cance levels . the statistical analysis plan was nalised and approved by the trial team before completion of data collection . 
analyses were based on modi ed intention - tovol 13 march 2012 24 h sternal skin conductance frequency ( n = 89 ) 24 h event - marker frequency ( n = 89 ) 1083 ( 896 ) 1000 ( 784 ) 911 ( 833 ) 776 ( 510 ) 191 ( 151 ) 104 to 487 articles total hfns frequency hot ush frequency night sweats frequency baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks whq depressed mood whq somatic symptoms whq anxiety or fears whq sleep problems whq memory and concentration sf - 36 physical functioning sf - 36 rolephysical 7284 ( 3789 ) 5772 ( 4373 ) 4533 ( 4593 ) 5864 ( 3216 ) 4560 ( 3800 ) 3746 ( 4141 ) 1631 ( 1484 ) 1212 ( 993 ) 848 ( 913 ) 938 ( 883 ) 1205 ( 803 ) 023 ( 026 ) 013 ( 016 ) 013 ( 019 ) 056 ( 026 ) 044 ( 024 ) 045 ( 023 ) 034 ( 025 ) 023 ( 027 ) 024 ( 031 ) 063 ( 030 ) 037 ( 031 ) 043 ( 037 ) 075 ( 034 ) 059 ( 036 ) 051 ( 037 ) 6617 ( 2289 ) 7538 ( 2424 ) 7413 ( 2496 ) 5372 ( 4329 ) 6000 ( 4035 ) 5577 ( 4310 ) 26 weeks with two - sided 95% cis . 
the trial is registered with current controlled trials , number isrctn13771934 . cognitive behavioural therapy ( mean [ sd ] ) usual care ( mean [ sd ] ) adjusted mean ( di erence [ se ] ) 95% ci role of the funding source the sponsor of the study had no role in the study design , data collection , data analysis , data interpretation , or writing of the report . 
 results we randomly allocated 96 women to treatment between may 5 , 2009 , and aug 27 , 2010 , most of whom remained in the trial ( gure 1 )  . 
withdrawal rates were much the same in both treatment groups ( p = 099 at 9 weeks ; p = 079 at 26 weeks ) , as were baseline demographic and clinical characteristics of participants ( table 1 )  . 
on starting the trial , hfns were frequent and problematic with a mean of 69 per woman ( sd 39 ) occurring per week for an average of 2 years , with a mean problem rating of 63 out of 10 ( table 1 )  . 
13 women were taking non - hormonal prescribed drugs ( table 1 ) : hormone replacement therapy ( one woman in each group ) , ssri ( two women in the cbt group and three in the usual care group ) , gabapentin ( one woman in each group ) , clonidine ( two women in the cbt group ) , gabapentin plus ssri ( one woman in the cbt group ) , and clonidine plus ssri ( one woman in the usual care group )  . problem rating scores at 9 weeks and 26 weeks were lower in the cbt group than they were in the usual care group ( table 2 )  . 
there was a signi cant di erence between groups the primary outcomehfns problem rating at 9 weeks following randomisation ( adjusted mean di erence of 167 , 95% ci 243 to 091 ; p < 00001 ) with a greater reduction from baseline in problem rating in the cbt group compared to the usual care group . 
at 9 weeks , the change in problem rating from baseline was 305 ( sd 23 ) in the cbt group , compared with 106 ( sd 17 ) in usual care group , equating to a 46% reduction in the cbt group and a 19% reduction in the usual care group . 
at 26 weeks , the problem rating had decreased from baseline by 52% ( mean change 339 , sd 23 ) in the cbt group and by 25% ( mean change 126 , sd 22 ) in the usual care group ( table 2 ; gure 2 )  . we recorded no signi cant di erence between groups in hfns frequency , or in the hot ush frequency and night sweat frequency subscales when analysed separately , at 9 weeks or 26 weeks ( table 3 and appendix )  . 
compared with baseline , both groups reported non - signi cantly fewer hfns at 9 weeks ( 21% in the cbt group and 24% in the usual care group ) and 26 weeks ( 38% in both groups )  . 
 table 3 : e ect of treatment on hot ushes and night sweats week 26 compared with those in the usual care group ( table 3 and appendix )  . 
women receiving cbt also reported less anxiety than did women in the usual care group at 9 weeks , but this di erence was not statistically signi cant at 26 weeks ( table 3 )  . 
we recorded small improvements in memory and concentration of participants in the cbt group compared with those in the usual care group , but no statistically signi cant di erences in somatic symptoms ( table 3 )  . 
at 26 weeks , women in the cbt group reported signi cantly better social functioning , physical functioning , and improved general health ( at both 9 weeks and 26 weeks ) than did women in the usual care group , according to the sf - 36 assessments ( table 3 )  . 
compared with women in the usual care group , women in the cbt group reported better mental health at 9 weeks and less bodily pain at 26 weeks ( table 3 )  . 
we recorded no signi cant di erences between the groups in emotional role functioning or vitality subscales ( table 3 )  . although we did not record a mean two - point difference between treatment groups ( gure 3 ) , a greater percentage of individuals had reached this two - point threshold in the cbt group than in the usual care group at both 9 weeks ( 65% [ 95% ci 5078 ] vs 38% [ 2552 ] ) and 26 weeks ( 78% [ 6288 ] vs 33% [ 2048 ] )  . 
this exploratory analysis suggests that improvement from baseline was clinically better in the cbt group than it was in the usual care group ( gure 3 )  . in the 10% of sessions assessed for quality assurance , cbt was delivered according to the treatment manual , with 98100% adherence . 
participant adherence to treatment was good ; 39 ( 91% ) of 43 participants who received cbt attended at least four of six sessions , and relaxation or paced breathing was practised , on average , 29 times each week ( sd 2693 )  . individuals taking prescribed drugs for hfns tended to continue them throughout the trial . 
three women started homoeopathy or herbal remedies ( one in the cbt group , two in the usual care group ) , and one woman in the usual care group started acupuncture . 
when the adjusted primary analyses were repeated excluding these ve participants , the estimates and cis remained within the same margins ( week 9 hot ush problem rating , cbt vs usual care mean di erence 158 , 95% ci 238 to 079 ; p < 00001 ; week 26 hot ush problem rating , cbt vs usual care mean di erence 177 , 259 to 095 ; p < 00001 )  . we recorded six adverse events , three in the cbt group and three in the usual care group . 
one participant died of an unrelated disorder before the treatment phase ( usual care group ) , we recorded two reoccurrences of breast cancer ( one in each group ) , and one woman reported low mood unrelated to the trial ( cbt group )  . 
 ( continued from previous page ) sf - 36 bodily pain sf - 36 general health sf - 36 vitality sf - 36 social functioning sf - 36 roleemotional sf - 36 mental health baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks 4615 ( 2273 ) 5368 ( 2398 ) 5100 ( 2250 ) 4810 ( 1594 ) 5184 ( 1458 ) 5034 ( 1542 ) 3533 ( 1610 ) 3963 ( 1523 ) 4031 ( 1748 ) 6702 ( 3143 ) 7530 ( 2539 ) 7750 ( 2718 ) 6739 ( 4245 ) 7561 ( 3802 ) 7350 ( 3760 ) 6757 ( 1789 ) 7463 ( 1422 ) 7070 ( 1924 ) cognitive behavioural therapy usual care week 9 week 26 figure 3 : proportion of patients with a reduction of two or more points in the hot ush problem - rating scale from baseline estimates are unadjusted . 
 vol 13 march 2012 articles two women ( both in the usual care group ) had mild reactions to the hot ush monitor ( a reaction to the adhesive used on the electrode patch )  . 
none of the adverse events were related to cbt . discussion our ndings suggest that cbt is safe , acceptable , and e ective in helping women to manage hot ushes and night sweats after breast cancer treatment , with additional bene ts to mood , sleep , and some aspects of quality of life . 
after group cbt , women reported less problematic hfns than did those receiving usual care , and these improvements were maintained at both the 9 - week and 26 - week follow - up . 
although the pre - speci ed endpoint of a between - group di erence of 2 points on the problemrating scale was not met , there was a statistically signi cant improvement in the cbt group , and a large proportion of women ( 78% ) who had received cbt achieved a reduction of 2 points compared with the usual care group ( 33% ) at 26 weeks . 
similarly , we recorded no signi cant di erences between groups in 24 h rate of hfns after the treatment phase , either physiologically ( ssc ) de ned or participant recorded ( event monitor )  . 
most women participating in group cbt reported reductions in problem rating that are regarded as clinically important , and there were sustained signi cant differences in problem rating between cbt and usual care . 
one study was the menos1 single - group pilot trial , 18 in which weekly 15 h sessions of cognitive behavioural therapy ( cbt ) for 6 weeks resulted in an average 49% reduction in problem rating and 38% reduction in hot ushes and night sweats ( hfns ) frequency , maintained at 3 months follow - up . 
a larger randomised controlled trial of cbt and exercise , 33 which used the group protocol manual developed for menos 1 , 18 reported preliminary ndings in which frequency and problem - rating reduced compared with usual care , although detailed ndings are not available . 
in another single - group trial , 34 an instructional dvd of paced breathing and distraction used over the course of 1 week resulted in small reductions in bothersomeness and interference of hfns and no change in physiologically measured hot ush frequency . 
cbt shows some promise but adequately powered randomised controlled trials are needed . interpretation our ndings show that group cbt can reduce the e ect of hot ushes and night sweats for women who have had breast cancer treatment . 
group cbt seems to be a safe , acceptable , and e ective treatment option which can be incorporated into breast cancer survivorship programmes and delivered by trained breast cancer nurses . 
at baseline , on average , participants had higher scores for sleep problems , somatic symptoms , and memory and concentration ( whq ) compared with norms for healthy women ( table 3 and data not shown ) .27 according the the sf - 36 scale , they had lower scores ( lower quality of life ) than did healthy women , especially for physical role functioning , general health , vitality , and bodily pa the signi cant improve ments in mood and sleep , as well as memory and concentration , after cbt are clinically important because di culties with mood sleep and cognitive functions are commonly reported by patients with breast cancer , particularly by those with hfns.30 moreover , the improve ment in social functioning after cbt is relevant because women report nding hot ushes especially di cult to deal with at work and in other social situations.18 although randomised controlled trials of non - hormonal drugs for hfns have shown moderate reductions in hfns frequency , they have recorded little evidence of improved quality of life.9 similarly , some studies show only weak relations between frequency of hfns and quality of life.21 , 22 the results of our study are very similar to the preliminary ndings of a parallel trial of cbt for hfns in a sample of healthy women ( menos2 ) .31 this consistent pattern of results suggests that the cbt might work by a ecting symptom perception and cognitive appraisal of hfns and possibly mood , rather than physiological mechanisms of hfns , such as temperature regulation or the thermoneutral zone in the hypothalamus.19 further analyses of moderators and mediators of hfns are planned to clarify this issue through identi cation of the underlying causal pathways to improvement on the hot ush problem rating scale.20 for example , changes in sleep after treatment might partly mediate the improvements in mood and quality of life . 
further studies should examine particular components of the intervention to test these analyses experimentally . we postulated that cbt would reduce hfns frequency to a greater extent than would usual care , especially because paced breathing has been shown to reduce hfns frequency measured both physiologically and subjectively.32 women receiving cbt reported practising paced breathing daily . 
paced breathing , once learnt , is practised for 25 min throughout the day and at the onset of a hot ush , so an average of 29 times per week is a realistic rate at which to practise . 
however , we controlled for usual care and assessment e ects and we should gain some insight into the placebo e ects of usual care through the planned mediator and moderator analysis.20 further research could compare di erent types of control conditions with di ering levels of information , advice , and support . 
the group cbt programme should be generalisable to other breast cancer settings because it is delivered in a hospital setting , is done by use of easily transferable guidelines ( the treatment manual ) , and adherence to the guidelines was high . 
the most cost - e ective method of delivering the group cbt would probably be to include it as part of survivorship support programme , delivered by trained and supervised breast - care nurses . to date , the best available treatments have been nonhormonal drugs including ssri and snris , clonidine , and gabapentin.9 these treatments have produced moderate reductions in hfns frequency ( averaging 37% across trials9 ) , but have had little e ect on quality - of - life measures . 
 by contrast our ndings suggest that both cbt and usual care resulted in a 38% reduction in frequency , and compared with the usual care group , those who received cbt showed statistically signi cant and lasting reductions in problem rating and improvements in quality of life . 
cbt could , therefore , be an important alternative or additional treatment option for patients with breast cancer ( panel 2 )  . limitations of this study include the frequency measures , which had high variability . 
however , ndings from another study show evidence of the validity of this scale compared with daily diary measures.24 estimation of the frequency of night sweats with the hot ush rating scale can be more di cult because women do not report night sweats that they sleep through , but this limitation is common to all self - report measures . 
the physiological measure was used for 24 h at baseline and at 9 weeks after randomisation ; in view of the variability of this measure , future studies might include a longer time of ssc monitoring and also include this measure at follow - up assessments . 
addition ally , we did not control for all potential confounding factors that could have an e ect on menopausal symptoms , such as the use of drugs to manage hfns and the use of adjuvant hormone therapy . 
however , treatment options are still restricted for these women , so a need still exists for nonhormonal interventions . our ndings suggest that this cognitive behavioural treatment , designed to be delivered by trained health professionals such as breast - care nurses , has the potential to improve long - term health outcomes for patients with breast cancer , and could be incorporated into breast cancer survivorship programmes . con icts of interest we declare that we have no con icts of interest . 
msh contributed to the search of published studies , study design , and data interpretation , and was the principle investigator and report guarantor . acknowledgments this work was funded by cancer research uk ( grant c8303 / a6130 ) ; msh was also supported by the national institute for health research biomedical research centre for mental health , south london and maudsley nhs foundation trust and the institute of psychiatry , kings college london , uk . 
trudie chalder , mark harries , ruth pickering , aleksandra gentry - maharaj , and caroline burgess contributed to development of the study , and participated in trial steering and data management committees . 
we would like to thank the clinical trials unit at kings college london for their advice and support , and team at the south east london cancer research network , gian gargaro at the guys surviving cancer , living life service , and the clinical sta at guys hospital , university hospital lewisham , kings college hospital , princess royal university hospital at bromley , queen marys sidcup , and queen elizabeth woolwich , for their help with participant recruitment . articles e ect of hiv on survival in patients with non - small - cell lung cancer in the era of highly active antiretroviral therapy : a population - based study ramesh rengan , nandita mitra , kaijun liao , katrina armstrong , anil vachani summary background hiv - infected patients with lung cancer have been reported to have poorer survival than uninfected patients . 
we examined the e ect of hiv infection on clinical outcome in patients with lung cancer who are also receiving haart . methods patients diagnosed with non - small - cell lung cancer ( nsclc ) from jan 1 , 2000 , to dec 31 , 2005 , with or without hiv infection were identi ed by querying the surveillance , epidemiology , and end results registry and the medicare lung cancer database . 
survival analysis by stage and treatment delivered comparing the hiv - infected patients with uninfected controls was done with kaplan - meier and cox models with propensity score adjustments . findings 71 976 patients with nsclc were identi ed as uninfected controls and 322 patients with nsclc were identi ed in the hiv group ; median age was 75 years for both groups . 
median overall survival for all stages was 70 months ( 95% ci 7070 ) for uninfected controls versus 80 months ( 60100 ) for the hiv group ( p = 016 ) ; for those with stage i / ii disease it was 370 months ( 360390 ) versus 430 months ( 260580 ; p = 037 ) ; for those with stage iiia / iiib disease it was 70 months ( 7070 ) versus 30 months ( 2080 ; p = 0051 ) ; and for those with stage iv disease it was 30 months for both groups ( 95% ci 3030 for controls ; 2050 for hiv group ; p = 077 )  . 
since the adoption of haart in the mid - 1990s , the expected survival of patients with hiv has improved substantially.21 , 22 although haart e ectively treats the immunosuppression associated with hiv infection , data also suggest that these drugs could diminish the e cacy of the antineoplastic regimens routinely used in the treatment of lung cancer.23 therefore , the clinical outcome of hiv - infected patients with lung cancer in the era of haart remains unclear . our study was designed to assess overall survival in hiv - infected patients with nsclc in the era of haart compared with uninfected patients . 
additionally , for patients with early stage nsclc , for whom surgical resection is the standard of care , we have assessed overall survival in hiv - infected patients after surgical resection as compared with uninfected patients . 
our goal was to establish whether nsclc displayed a more aggressive phenotype in hiv - infected individuals , to quantify the e ect of viral infection on clinical outcome in patients with nsclc . 
the broader objective was to establish the role that hiv infection should have in clinical decision making in patients with nsclc . methods study design the seer - medicare database is the result of a linkage of two population - based data sources : the surveillance , epidemiology and end results ( seer ) registry , sponsored by the us national cancer institute ( nci ) , and medicare , a federally funded us programme that hiv + ( n = 322 ) control ( n = 71 976 ) p value for more on seer see median age ( iqr ) 75 ( 6981 ) 75 ( 6981 ) stage i / ii stage iiia / iiib stage iv race white african american other comorbidities 2 or more median income in bottom two quartiles ( range in us dollars ) table : patient characteristics 3540% 2981% 3478% 20 016 22 793 29 167 7174% 2360% 466% 497% 870% 8634% 4317 ( 732 492 ) 62 859 6056 3061 6164 11 660 54 152 33 117 2781% 3167% 4050% 8733% 841% 425% 856% 1620% 7524% 4601 ( 732 492 ) 0002 048 004 099 < 00001 < 00001 072 002 00003 < 00001 065 pro vides health insurance for people of age 65 years and over , disabled , or have end - stage renal disease . 
the linkage to medicare provides longitudinal data for all claims from the center for medicare and medicaid services from the time of eligibility to death.24 , 25 patients younger than 65 years are excluded from this registry unless they are disabled or have end - stage renal disease . this study was approved by the institutional review board of the university of pennsylvania . study population we developed an analytic dataset from the seermedicare linked database , consisting of patients with a diagnosis of lung cancer ( icd - 9 code 162xx ) and nonsmall - cell histology ( adenocarcinoma , squamous cell carcinoma , large cell , bronchoalveolar carcinoma , or nsclc not otherwise speci ed ) contained in the seer registry who were diagnosed between jan 1 , 2000 , and dec 31 , 2005 . 
patients who were enrolled in medicare , but receive their bene ts through a third party , such as a health maintenance organisation , or private fee - forservice plan , were excluded from this analysis because of incomplete claims data in medicare for these patients . 
survival comparisons were also done after strati cation for disease stage . we used propensity score methods to account for imbalances between the two comparison groups on measured covariates.27 , 28 we chose propensity score adjustment in our cox model rather than traditional covariate adjustment , since recent ndings have suggested that this method is advantageous when analysing large observational datasets such as seer - medicare.29 our group has previously used this method to examine seer - medicare data.30 , 31 in an observational study such 1204 vol 13 december 2012 articles log - rank p = 037 hiv - infected control 95% ci for hiv patients 95% ci for controls log - rank p = 016 number at risk hiv - infected control 71 976 20 999 9615 4132 1225 20 016 13 006 6950 3205 log - rank p = 0051 log - rank p = 077 number at risk hiv - infected control 22 793 5313 time ( months ) 2007 29 167 2671 time ( months ) figure 1 : kaplan - meier comparative survival of hiv - infected and uninfected control nsclc patients : ( a ) all stages ; ( b ) stage i / ii ; ( c ) stage iiia / iiib ; and ( d ) stage iv as this one , covariate imbalances could potentially lead to biased survival estimates due to confounding . 
we calculated propensity scores using multivariable logistic regression with hiv infection as the outcome of interest , with adjustment for race , median income , stage , sex , and comorbidities . 
we then used multivariable cox proportional hazards models to compare death from any cause between the hiv - infected and control groups after adjustment for the propensity score as a continuous variable . 
to assess the proportional hazards assumption , we used the schoenfeld residuals test and complementary log - log plots . the kaplan - meier method was used to compare patients with stage i and ii disease with or without hiv infection who underwent de nitive surgical resection to assess the e ect of hiv infection in patients undergoing de nitive surgical resection for treatment of early stage nsclc . 
all statistical analyses were done with the statistical analysis system ( sas ) version 9.3. role of the funding source the sponsor did not have any role in study design , collection , analysis , or interpretation of the data , or in writing of this report . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results 322 patients were identi ed from jan 1 , 2000 , to dec 31 , 2005 , with a diagnosis of hiv ( hiv group ) and 71 976 individuals with a diagnosis of nsclc were identi ed who were not associated with a diagnosis of hiv ( control group )  . 
a similar proportion of patients were stage iiia / iiib and stage iv in both groups , but there was a signi cantly greater proportion of patients with stage i / ii disease in the hiv - infected group than the control group ( p = 0002 , table )  . 
there was a signi cant di erence in ethnic background between the two groups , with the hiv - infected group containing a higher proportion of african americans ( 236% vs 84% , p < 00001 )  . 
 the proportion of patients with their median income in vol 13 december 2012 1205 articles the bottom two quartiles was much the same between the two groups ( table )  . 
 the unadjusted median survival for uninfected control patients with nsclc was 70 months ( 95% ci 7070 ) com pared with 80 months ( 60100 ) for the hiv group ( p = 016 )  . 
when strati ed by stage , the unadjusted median survival for stage i / ii patients was 370 months ( 95% ci 360390 ) for uninfected controls compared with 430 months ( 260580 ) for the hiv group ( p = 037 ) , for those with stage iiia / iiib disease , it was 70 months ( 7070 ) for uninfected controls compared with 30 months ( 2080 ) for the hiv group ( p = 0051 ) , and for those with stage iv disease , it was 30 months ( 3030 for control group and 2050 for hiv group ) for un infected controls and the hiv group ( p = 077 ; gure 1 )  . 
after using propensity score adjustment to account for potential confounders , there remained no di erence in survival between uninfected controls and the hiv group across all stages ( hazard ratio 103 , 95% ci 091117 ) , stage i / ii ( 122 , 09316 ) , stage iiia / iiib ( 088 , 071109 ) , and stage iv ( 099 , 082121 )  . to examine the e ect of treatment on survival , we restricted our analysis to stage i and ii patients undergoing de nitive surgical resection alone , which is the standard of care.32 of the 114 hiv - infected patients with stage i or ii disease , 92 ( 807% ) underwent surgical resection . 
 the 5 - year survival was 47% for hiv - infected patients undergoing surgical resection versus 49% for the control group ( p = 088 )  . hiv - infected control 95% ci for hiv patients 95% ci for controls log - rank p = 088 discussion our results indicate that , across all stages , survival outcomes in hiv - infected patients with nsclc are not signi cantly di erent from uninfected patients . 
additionally , when assessing stage i / ii patients undergoing de nitive sur gical resection , survival was not signi cantly di erent in hivinfected patients undergoing surgery com pared with uninfected patients . 
taken together , these data suggest that nsclc does not display a more aggressive phenotype in hiv - infected patients . our ndings are in contrast to previously published reports that suggest that hiv - infected patients with lung cancer fare worse when compared with uninfected patients ( panel ) .17 , 18 notably , these previous studies included patients from the pre - haart era and spanned over three decades to identify adequate patient numbers . 
 these studies did not distinguish between nsclc and sclc , which have signi cantly di erent treatments and expected survival and as such cannot be grouped together for the purpose of examination of clinical outcome.1 , 2 , 33 a retrospective study by brock and colleagues18 examined the e ect of hiv infection across di erent stage subgroups in a combined cohort of sclc and nsclc and pre - haart and post - haart patients . 
although the authors did not note any signi cant di erence in stage - speci c survival , the overall survival of hivinfected patients with lung cancer was worse than hivindeterminate patients . 
their results may be due , in part , to the increased proportion of advanced stage patients ( iii and iv ) seen in the hiv - infected group relative to the hiv - indeterminate patients.18 in a report from the italian cooperative group on aids and tumors , spina and colleagues reported signi cantly poorer survival in 39 patients with hiv and lung cancer treated in the prehaart era ( 198697 ) than in matched controls ( median survival of 50 vs 100 months ; p < 00001 ) .34 , 35 a follow - up study36 com pared survival in hiv - infected patients with lung cancer from the pre - haart era to the haart era , demonstrating a signi cant improvement in survival ( from 38 to 70 months ; p = 001 )  . 
 although the exact reason for our observation is unclear , hiv - infected patients might have received regular medical care while on haart and therefore were diagnosed at an earlier stage . since the introduction of haart in 1996 , mortality from hiv / aids has decreased substantially . 
they further reported that this translated into an improvement in median survival of an hiv - infected patient in the haart era to 325 years from 76 years in the prehaart era.21 by contrast , the median survival of a patient with lung cancer across all stages is around 15 months.1 an analysis by persad and colleagues showed that 25% of all clinical trials for patients with nsclc and 29% of clinical trials for patients with sclc explicitly excluded patients with hiv.9 given the signi cant improvement in survival with hiv in the haart era , persad and coworkers argued for greater inclusion of patients with hiv in clinical trials across all cancers . there are several limitations to our analysis . 
although this study represents the largest study , to our knowledge , to date on the e ect of hiv on clinical outcome in nsclc , the number of hiv - infected patients identi ed is fairly small , leading to limited power to detect a small survival di erence . 
although there are data for the incidence of nsclc in patients with hiv , 16 there are limited data for the incidence of hiv in patients with nsclc , with reports ranging from 50 to 1800 hivinfected individuals per 100 000 patients with lung cancer.17 , 18 our data is concordant with these reports . 
although we restricted our analysis to patients treated between jan 1 , 2000 , and dec 31 , 2005 , when most hiv patients should have been receiving haart , we could not con rm that the patients included in our analysis were being treated with haart . 
a recent report assessing us trends in haart use showed widespread adoption of treatment during this period , with around 80% of hiv - infected therapy.40 seer - medicare patients on antiretroviral seer - medicare does not panel : research in context systematic review at the time that this study was designed , an increased incidence of nsclc in hiv - infected patients had been reported . 
before initiating our study , we searched the medical literature for comparative studies examining clinical outcome in hiv - infected lung cancer or hiv - infected patients with nsclc when compared with hiv - uninfected or indeterminate patients with lung cancer . 
we searched pubmed ( without any date or language restrictions ) using the following terms : hiv and survival and lung cancer , or hiv and survival and non - small cell lung cancer or hiv and lung cancer or hiv and non - small cell lung cancer and repeated these searches including the term antiretroviral therapy , highly active . 
we identi ed studies that had retrospectively examined the outcome of hiv - infected patients with lung cancer and reported this group to have poorer survival when compared to uninfected or hiv - indeterminate patients with lung cancer or historical benchmarks for survival . interpretation our data suggest that survival of hiv - infected patients with nsclc in the era of haart is comparable to hiv - uninfected patients with nsclc . 
haart regimens have previously been shown to interfere with the antineoplastic regimens that are routinely used in the treatment of lung cancer.23 the extent to which this interaction a ected the results seen in our study is unclear . 
the potential for drugdrug interactions must be taken into account when administering antineoplastic agents in patients with hiv / aids on haart.41 also , seer - medicare does not capture cd4 count data , a factor which has previously reported to correlate with survival in hiv - infected patients with lung cancer.19 seer - medicare does not capture in formation on the incidence of opportunistic infections or the administration of prophylactic regimens and therefore this is not included in this analysis . 
competing risks of death in hiv - infected patients with nsclc from opportunistic infec tions or complications from antineoplastic therapy , such as neutropenia , could not be quanti ed in our analysis . 
however , on the basis of our results , such an unmeasured confounder would have two to be signi cantly imbalanced between the vol 13 december 2012 1207 articles the hiv group comparison groups for to show signi cantly poorer survival than the uninfected controls.42 additionally , because the data in seer - medicare is mainly composed of people older than 65 years , we were unable to examine the e ect of hiv infection on survival in younger patients.1 notably , the median age of patients with hiv and lung cancer is generally reported to be younger than the average age of the lung cancer population.34 , 39 , 43 the clinical phenotype of lung cancer in younger patients with hiv could be distinct from that seen in patients over age 65 years . 
age has been shown to be an important prognostic factor for survival in lung can cer , with older patients faring more poorly.44 advanced age has also been shown to be an independent predictor of poor survival in hiv - infected patients initiating haart.45 however , since seer - medicare does not capture data for patients under the age of 65 years , whether the results reported in our trial are applicable to all hiv - infected patients with lung cancer is unclear . trials , where in conclusion , these data suggest that hiv infection alone in the era of haart should not play a role in clinical decision making in treatment of patients with nsclc . 
notably , the intergroupe francophone de cancerologie thoracique has recently initiated a phase 2 , multicentre prospective study evaluating the combination of pemetrexed plus carboplatin in hivpositive patients with lung cancer and accrual to this ( clinicaltrials.gov , number nct01296113 )  . 
additionally , these data suggest that improving access to modern diagnostic imaging and cancer therapies are likely to signi cantly bene t patients with nsclc with hiv since their outcome is similar to that of uninfected controls when treated with de nitive surgical resection . 
the clinical management of the hiv - infected patient with nsclc , as with all patients with lung cancer , requires a multidisciplinary approach to individualise and optimise therapy and to manage toxicities . is ongoing trial contributors rr , nm , kl , and av were responsible for the study concept and design . 
although not legally enforceable , the report is an essential step forward in guiding future drug development , highlighting novel treatment combinations that should speed up drug development , reduce costs , and give patients faster access to new treatments . 
 so what are the qualifying criteria ? the disease must be considered serious and only drugs that have a robust biological rationale for use in combination , as opposed to use individually , should be assessedie , combined agents should have more than additive e cacy or provide a more durable response . 
examples include agents that are inactive alone but potentiate the activity of another drug , drugs against which resistance occurs rapidly when used as a monotherapy but in combination remain e ective for longer , and drugs that target di erent , but complementary , biological pathways . 
two or more marketed drugs have been used very successfully in combination in patients with cancer , and this guidance is the next logical step to prompt novel treatments for drugs that have not been tested and marketed individually , enabling fast - track marketing approval and earlier patient access . 
as the report suggests , co - development will generally provide less data on safety and e cacy , and when safety cannot be tested in phase 1 studies of individual drugs ( eg , because of resistance ) , preclinical evidence , pharmacokinetic data , and biomarker evaluation should be sought . 
 indeed the guidance states that co - development could present a greater risk to the patient than if the drugs are developed initially as single agents . co - development allows innovative adaptive trial designs in which patients treated with single agents that prove ine ective can crossover to the more active combination treatment . 
however , the biggest advance in the development of new treatment regimens could be made if the fda now focused its attention wholeheartedly on facilitating head - to - head comparative e ectiveness studies of drugs already on the marketas called for by the obama administration . 
comparative e ectiveness studiesa current buzz phraserefers to many types of study and is described by the fda as intended to help make decisions more consistent , transparent , and rational , and useful in identifying gaps and uncertainties . 
however , these studies are often large randomised trials , and therefore expensive to complete , and can include a placebo control as well as the head - to - head comparison ( s ) , adding further to the time and e ort involved . 
unsurprisingly , therefore , these are a di cult sell to drug manufacturers who are likely to have little interest in an expensive trial of their latest topselling drug given their vested interests . 
it is now time , however , for the fda to use its considerable in uence more e ectively to incentivise manufacturers to complete such comparative research and provide speci c guidance as to what it expects in terms of the optimum trial design . 
 the rhetoric now needs to be translated into detailed speci cs of how such collaborative and comparative research might be achieved so patients are best served . the us national cancer institute ( nci ) has been at the forefront of cutting edge and practice - changing trial research and will be vital in complementing the fda in its e orts . 
the nci recently re - organised its clinical trials programme following recommendations from the institute of medicine report in april , 2010 , and has consolidated its nine trial groups for adult cancer into fourwith the aim of making the overall programme more cost e ective and e cient . 
by collaborating with the fda on combination drug trials for unmarketed agents , comparative e ectiveness studies for marketed drugs , as well as drug and diagnostic co - development strategies , the nci will ensure patients have access to more treatment options , better personalised treatment , and the latest magic bullets . 
we assessed the prognostic value of a prede ned cell cycle progression ( ccp ) score in two cohorts of patients with prostate cancer . methods we measured the expression of 31 genes involved in ccp with quantitative rt - pcr on rna extracted from formalinxed para n - embedded tumour samples , and created a prede ned score and assessed its usefulness in the prediction of disease outcome . 
the signature was assessed retrospectively in a cohort of patients from the usa who had undergone radical prostatectomy , and in a cohort of randomly selected men with clinically localised prostate cancer diagnosed by use of a transurethral resection of the prostate ( turp ) in the uk who were managed conservatively . 
the primary endpoint was time to biochemical recurrence for the cohort of patients who had radical prostatectomy , and time to death from prostate cancer for the turp cohort . findings after prostatectomy , the ccp score was useful for predicting biochemical recurrence in the univariate analysis ( hazard ratio for a 1 - unit change [ doubling ] in ccp 189 ; 95% ci 154231 ; p = 5610 ) and the best multivariate analysis ( 177 , 140222 ; p = 4310 )  . 
in the best predictive model ( nal multivariate analysis ) , the ccp score and prostate - speci c antigen ( psa ) concentration were the most important variables and were more signi cant than any other clinical variable . 
in the turp cohort , the ccp score was the most important variable for prediction of time to death from prostate cancer in both univariate analysis ( 292 , 238357 , p = 6110 ) and the nal multivariate analysis ( 257 , 193343 ; p = 8210 ) , and was stronger than all other prognostic factors , although psa concentration also added useful information . 
heterogeneity in the hazard ratio for the ccp score was not noted in any case for any clinical variables . interpretation the results of this study provide strong evidence that the ccp score is a robust prognostic marker , which , after additional validation , could have an essential role in determining the appropriate treatment for patients with prostate cancer . funding cancer research uk , queen mary university of london , orchid appeal , us national institutes of health , and koch foundation . introduction prostate cancer is a common diagnosis , especially when prostate - speci c antigen ( psa ) screening is used , 1 and its natural history is highly variable and di cult to predict . 
we therefore selected a set of ccp genes and retrospectively tested their prognostic value in prediction of disease outcome using a prede ned score , in a cohort of patients with prostate cancer who had been treated with radical prostatectomy and in a cohort of conservatively treated patients . methods ccp gene selection to reliably generate expression data from formalinxed para n - embedded ( ffpe ) tissue , we selected 126 ccp 804 consecutive patients with radical prostatectomy 775 with clinical data 442 with available tumour tissue 410 eligible for analysis 29 no clinical data 333 no available tissue 32 excluded because of treatment with neoadjuvant therapies 44 excluded because of poor - quality cell - cycle - progression scores 366 analysed for gene expression data figure 1 : flow chart of cohort with radical prostatectomy genes from the gene expression omnibus database and tested their performance with rna extracted from 96 commercially available ffpe prostate tumour sections ( asterand , detroit , mi , usa ) obtained from anonymous patients . 
 therefore , we selected genes for inclusion in the signature on the basis of their correlation with the mean expression of the entire set of ccp genes ( webappendix pp 14 )  . 
the nal signature consisted of 31 ccp genes ( foxm1 , cdc20 , cdkn3 , cdc2 , kif11 , kiaa0101 , nusap1 , cenpf , aspm , bub1b , rrm2 , dlgap5 , birc5 , kif20a , plk1 , top2a , tk1 , pbk , asf1b , c18orf24 , rad54l , pttg1 , cdca3 , mcm10 , prc1 , dtl , cep55 , rad51 , cenpm , cdca8 , and orc6l )  . 
these highly correlated genes were used to provide a robust and highly reproducible measurement of cell proliferation and were not intended factors to capture ( eg , invasive potential )  . information to other related radical prostatectomy cohort men who had undergone radical prostatectomy for prostate cancer from 198595 were identi ed through the tumour registry at the scott and white clinic , temple , tx , usa . 
the specimens were inked , and pathological ndings were recorded as positive for bladder neck or urethral margin , invasion into the capsule , extension through the capsule , positive margins , and the involvement of the seminal vesicles . 
 biochemical recurrence was de ned as a psa concentration greater than 03 ng / ml based on the management policy used in the 1990s , and was not changed for this analysis . 
we selected patients who had not been treated with neoadjuvant drugs and for whom clinical data and tumour tissue were available for inclusion in this study to create a retrospective cohort . 
 institutional review board approval was obtained from the scott and white clinic . transurethral resection of prostate ( turp ) cohort for the population - based retrospective watchful - waiting cohort , potential cases of prostate cancer were identi ed 246 vol 12 march 2011 articles 214 ( 156293 ) 132 ( 094185 ) 164 ( 088306 ) 145 ( 110193 ) 215 ( 153301 ) 143 ( 109189 ) 224 ( 167301 ) 165 ( 126217 ) 220 ( 170285 ) 155 ( 114211 ) 189 ( 154231 ) 833% * 619% * 445% * 237% * ccp score recurrence hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) from six cancer registries in great britawithin each region , cases from collaborating hospitals were reviewed , and full details of these cases have been reported.31 men were included in this study if they had clinically localised prostate cancer , which was diagnosed by use of turp between 1990 and 1996 ( inclusively ) , were younger than 76 years at the time of diagnosis , and had a baseline psa measurement . 
men who had hormone therapy before diagnostic biopsy were also excluded because of the e ects of hormone treatment on interpretation of the gleason score . original histological specimens from the diagnostic procedure were requested , collected , and centrally reviewed by a panel of expert urological pathologists to con rm the turp diagnosis and , when necessary , to reassign gleason scores for all the prostate cancers by use of a contemporary interpretation16 of the gleason scoring syste follow - up was through the cancer registries and the last review took place in december , 2006 . 
 deaths were divided into two categories , those from prostate cancer and those from other causes , according to whos standardised criteria.32 national ethics approval was obtained from the northern multicentre research ethics committee , followed by local ethics committee approval at each of the turp cohort the collaborating hospitals for ( webappendix p 6 )  . gene expression depending on tumour volume , ve to 12 consecutive 5 m ( turp ) or 10 m ( prostatectomy ) ffpe tumour sections were used to isolate tumour - derived rna . 
we switched from rneasy ffpe to mirneasy because the new kit consistently generated figure 2 : analysis of cell cycle progression ( ccp ) score in cohort with radical prostatectomy ( a ) distribution of the ccp scores for 366 patients . 
2 values were 5493 , 415 , and 841 in the univariate analysis , multivariate analysis , and nal model , respectively , when gleason scores were assessed as a three - group categorical variable with 2 degrees of freedo table 1 : summary of statistical analysis of prostatectomy cohort , by biochemical recurrence better rna yields . 
no di erence was noted between the kits in terms of the data for gene expression . total rna was treated with dnase i ( sigma - aldrich , st louis , mo , usa ) before cdna synthesis . 
however , most samples ( 90% of radical prostatectomy cohort and 85% of turp cohort ) could be used to generate ccp scores , and therefore , had rna of adequate quality . before measurement of gene expression , the cdna was preampli ed in a pooled reaction containing taqman assays ( applied biosystems )  . 
the ampli cation reaction was diluted 1 : 20 with the 1tris - edta bu er before it was loaded on taqman low density arrays ( applied biosystems ) to assess the ampli ed genes . 
a total of 31 prede ned ccp genes and 15 housekeeper genes were ampli ed on one taqman low density array . ccp score the ccp score for each individual was calculated . 
the values of each of three replicates of each of the 31 ccp genes were normalised by subtraction of the average of up to 15 non - failed housekeeper genes for that replicate ( centred with a prede ned value ) to give c * t . 
this quantity was then converted to a value that was proportional to the copy number , calculated as 2c * for missing c * t values , due to low expression , 2c * was set as equal to 0 . 
for each ccp gene , the mean 2c * of the qualifying replicatesie , those with expression of at least 13 housekeeper genes , was then averaged over the qualifying ccp genes . 
this is the normalised average of 2c * t and was converted back to create the ccp score by taking a base 2 logaritha ccp gene was judged as having failed if more than one replicate did not qualify , or if two replicates quali ed and one of them had 2c * equal to 0 , or if the standard deviation between the three 248 vol 12 march 2011 articles replicate c * t values exceeded 05 . 
ccp scores with the number of failing ccp genes greater than nine of 31 , or a high sd between scores calculated from the three replicates , were rejected and excluded from the analysis . 
 the interassay variability has been established in our laboratory and the sd of the ccp score for experimental replicates is 01 . statistical analysis survival analysis was done with cox proportional hazards models . 
the clinical variables recorded for the prostatectomy cohort were diagnostic gleason score , most recent prebiopsy psa concentration , clinical stage , clinical grade , primary treatment ( no preoperative or postoperative hormones , orchiectomy , or adjuvant radiation ) , age at surgery , pathological tumour stage , pathological grade , pathological gleason score , and invasion features . the primary endpoint for the turp cohort was time to death from prostate cancer . 
biochemical progression was not an appropriate outcome for this cohort , since baseline psa concentrations remain elevated and some patients will have chosen to start hormones or have radical treatment without evidence of increasing psa concentration . 
the variables recorded for the turp cohort were centrally reviewed gleason grade and score , baseline psa value , clinical stage , extent of disease ( proportion of turp chips with disease ) , age at diagnosis , and initial treatment ( no initial treatment or early hormone management )  . 
 the analysis set and a complete analysis plan were agreed , and all ccp scores were assigned , before the clinical and outcome data were unmasked . in both cohorts , psa concentration was modelled as the natural logarithm of 1 + psa ( ng / ml )  . 
 as indicated above , for the prostatectomy cohort , only a single pathological gleason score was recorded at diagnosis ; for the turp cohort , 3 + 4 and 4 + 3 were shown to have nearly identical prognosis.13 , 31 therefore , a total gleason score of 7 was analysed as one group . 
 for simplicity , gleason scores were grouped into less combined risk score combined risk score stratied by gleason score figure 3 : 10 - year predicted risk of recurrence for di erent combined risk scores in cohort with radical prostatectomy ( a ) , and distribution of the combined risk scores for di erent subgroups based on gleason scores ( b ) the probability of recurrence was estimated from a cox proportional hazard model by use of the combined risk score . than 7 , 7 , and greater than 7 ( radical prostatectomy cohort : less than 7 [ 56% with score 6 ] , greater than 7 [ 75% with score 8 , 19% with score 9 ] ; turp cohort : less than 7 [ 88% with score 6 ( all 3 + 3 ) ] , 7 [ 34% with score 4 + 3 ] , and greater than 7 [ 51% with score 8 , 46% with score 9 ] )  . 
all p values were twosided and 95% cis and p values were based on statistics with 1 degree of freedom obtained from partial likelihood models . the main assessment was a univariate analysis of the association between outcome and ccp score . 
this later e ect was measured by use of the decrease in the likelihood ratio when the ccp score was omitted from a model containing it and the other relevant baseline clinicopathological variables . 
in construction of the best prognostic model , the goal was to capture most of the prognostic information from the ccp score and the clinical covariates in a simple linear model without over tting the data . 
a multivariate proportional ( cox ) hazards model was used to achieve this goal and to create a combined score based on the major clinical variable and the ccp score . 
the ccp score was evaluated vol 12 march 2011 articles 1658 reviewed histology and assigned gleason score 747 diagnosed by use of needle biopsy 2333 eligible patients 675 excluded 203 not requested 472 excluded after review 283 unknown or missing histology slides 43 incorrect pathology specimen 135 histologically ungradeable gleason score 6 no tissue in block 5 histologically ungradeable gleason score 911 diagnosed by use of turp 429 unselected samples identied for analysis 482 not included in this study 7 previous hormone therapy 31 ineligible for study 9 psa > 100 ng / ml 6 missing baseline psa 4 previous cancer 4 metastases within 6 months 1 biopsy not between 199096 61 excluded because of poor - quality cell - cycle progression scores 398 available for analysis 337 eligible in nal analysis figure 4 : flow chart of cohort with transurethral resection of prostate ( turp ) psa = prostate - speci c antigen . as a linear and a quadratic term , and tested for interactions with individual covariates . 
we used a forward stepwise regression in which a new variable was added only if it had a p value of less than 002 for the prostatectomy study and 005 for the turp study ( since fewer variables were tested )  . 
the corresponding author had full access to the data ( as did ss , jer , and dm ) , and takes full responsibility in submitting the report for publication . the results for radical prostatectomy cohort , patients characteristics and treatment outcomes have been reported previously.33 figure 1 summarises the selection of 410 patients for this study who underwent radical prostatectomy . 
the median preoperative psa concentration was 69 ng / ml ( 46109 ) , and 281 ( 71% ) of 397 patients had psa concentrations less than 10 ng / ml . 
a unit change in the score corresponds to a doubling in expression level . that were the the univariate analysis showed that in the patients who had undergone radical prostatectomy , a high ccp score was predictive of biochemical recurrence ( table 1 )  . 
 addition of a quadratic term for ccp score was not signi cant ( p = 063 ) , indicating that a simple linear model would capture most of the prognostic information from the signature . 
 the ccp score was only weakly correlated with other variables , the highest correlation was with the gleason score and psa ( pearsons ( cid : 1 ) values , 022 and 021 respectively )  . 
however , patients with higher clinical 250 vol 12 march 2011 articles 276 ( 103740 ) 205 ( 105401 ) 213 ( 160285 ) 267 ( 159447 ) 351 ( 195635 ) 505 ( 289883 ) 208 ( 134324 ) 412 ( 1671021 ) 246 ( 182333 ) 292 ( 199429 ) 560 ( 2671175 ) 225 ( 177287 ) 292 ( 239357 ) 783% * 346% * 131% * 22% * risk ( ie , gleason score > 6 and psa concentrations > 10 ng / ml ) tended to have a reduced ccp hazard ratio ( hr )  . 
the ccp score was predictive for death after disease progression ( hr 299 , 95% ci 169528 ; p = 00007 )  . in the full multivariate analysis of the prostatectomy cohort , ccp and psa concentration were the most signi cant predictors of biochemical recurrence , and provided more prognostic information than did any other variable ( table 1 )  . 
the best multivariate model was developed by forward stepwise regression and is given by combined risk score 055 ccp + 081 log ( 1 + psa ) + 028 tstage + 064 margin + { 030 ( gleason score 7 ) + 099 ( gleason score > 7 ) } figure 3a shows how the risk of biochemical recurrence in the nal 10 years increased as a function of the combined risk score , and given the central prognostic role of the gleason score , gure 3b shows the distribution of combined risk score in di erent gleason score categories . for the turp cohort , the selection of patients is summarised in gure 4 . 
we report the results obtained with a randomly selected subset of 337 men diagnosed by use of turp for which we were able to compute the ccp score ( gure 4 )  . 
within 10 years of diagnosis , 171 ( 51% ) of 337 men had died , 68 ( 20% ) from prostate cancer and 103 ( 31% ) from other causes . figure 5a shows the distribution of the ccp score among the 337 patients in the turp cohort . 
by comparison with the gleason score , psa , cancer extent , and ki67 , the ccp score provided the most prognostic information in the univariate analysis , with the being slightly greater than that for the gleason score ( table 2 ) , and substantially larger than for all other variables . 
 compared with the prostatectomy cohort , the ccp score figure 5 : analysis of cell cycle progression ( ccp ) score in cohort with transurethral resection of prostate ( turp ) ( a ) distribution of the ccp scores ( n = 337 )  . 
2 values were 813 , 54 , and 71 in the univariate analysis , multivariate analysis , and nal model , respectively , when gleason score was assessed as a three - group categorical variable with 2 df ( when increased to ve groups , 2 values were 94 , 54 , and 72 , respectively )  . 
 table 2 : summary of statistical analysis of transurethral resection of the prostate cohort combined risk score in the full multivariate analysis , after adjustment for psa concentration , gleason score , ki67 expression , and extent of disease , the ccp score was dominant ( table 2 ) , providing more information than did any other variable . 
 none of the variables showed a signi cant interaction with the ccp score , and the hr for the ccp score was only slightly attenuated when other factors were added to the model ( table 2 )  . 
 hormone treatment was signi cant in a univariate model ( hr 381 , 95% ci 240605 ) , but did not add signi cant predictive information in the multivariate model ( 112 , 068184 ) , presumably because the decision to use this treatment was based on the known prognostic factors . 
 addition of a quadratic term for ccp was also not signi cant in the multivariate model ( p = 013 )  . in the forward stepwise regression model , with the variables ccp , psa concentration , and gleason score , the best predictor was the combined risk score calculated as function of figure 6a shows the predicted 10 - year death rate from prostate cancer the increases as a combined score ; gure 6b shows the distribution of the combined score in di erent gleason score categories . 
for men with a tumour that was gleason score 6 or less , use of the combined score identi ed 28 ( 16% ) of 172 patients with a 10 - year risk of death from prostate cancer that was less than 2% , and 102 ( 59% ) of 172 with a risk less than 5% , but also identi ed 25 ( 15% ) with a risk greater than 10% , indicating that not all gleason score 6 or less tumours are low risk . 
for gleason score 7 combined risk score stratied by gleason score 095 ccp + 061 log ( 1 + psa ) + { 090 ( gleason score 7 ) + 100 ( gleason score > 7 ) } figure 6 : 10 - year predicted risk of prostate cancer death for di erent combined risk scores in cohort with transurethral resection of prostate ( a ) , and distribution of the combined risk scores for di erent subgroups based on gleason scores ( b ) the probability of prostate cancer death was estimated from a cox proportional hazard model by use of the combined risk score . correlated more with gleason score ( pearsons ( cid : 1 ) = 061 ) , log ( 1 + psa ) ( ( cid : 1 ) = 027 ) , ki67 ( ( cid : 1 ) = 050 ) , and extent of disease ( ( cid : 1 ) = 051 )  . 
the prognostic value of the ccp score was similar in di erent gleason categories and when strati ed by psa , extent of disease , and ki67 ( gure 5b )  . 
figure 5c shows a kaplan - meier plot of the proportion of patients dying of prostate cancer at di erent follow - up times grouped by integer values of the ccp score . 252 vol 12 march 2011 articles ( either 3 + 4 or 4 + 3 ) , the corresponding data were none of 73 patients , eight ( 11% ) , and 59 ( 81% ) , respectively . 
in the whole cohort , the numbers and percentages were 28 ( 8% ) of 337 , 111 ( 33% ) , and 173 ( 51% ) , respectively . when we assessed deaths from other causes , the only signi cant factor was age . 
neither the ccp score nor other major prognostic factors for prostate cancer death were signi cant causes , indicating that confounding by other deaths cannot explain these ndings . discussion the ccp score was predictive of outcome in both cohorts and provided substantially more prognostic information than did clinical variables alone . 
expression of ccp genes is higher in actively growing cells , and presumably by measuring the expression of ccp genes , we are indirectly measuring the growth rate and inherent aggressiveness of the tumour , which ultimately a ects outcome . 
three of the genes in our signaturetop2a , rrm2 , and birc5have been previously associated with prostate cancer outcome , 14 , 15 but we believe the use of a larger panel will ensure robustness of the score . 
notably , many ccp genes are putative targets of cytotoxic or radiation therapies : rrm ( pemetrexed and gemcitabine ) , top 2a ( anthracyclines ) , kif11 and kif20a ( taxanes ) , tk1 ( uorouracil ) , and rad51 and rad54l ( radiation , alkylating drugs , and novel targeted drugs ) , and therefore ccp may be useful in predicting response to treatment . both cohorts have their strengths and weaknesses . 
the cohort of patients who had undergone radical prostatectomy were mainly screen detected , and had lower baseline gleason scores and psa concentrations , but a very low death rate from prostate cancer . 
the turp cohort had more aggressive disease , which meant that prostate cancer mortality could be reliably modelled , but was all based on symptomatic patients and turp samples , which is unusual in contemporary practice . 
in both settings , ccp score and psa concentration were the dominant variables , whereas other clinical variables ( including gleason score ) did not retain most of their univariate prognostic usefulness . 
by contrast ki67 , which is coded for by a ccp gene and by itself can be predictive of outcome in this dataset , 34 was eliminated from models that immunohistochemical score . 
 assessment of ki67 is dominated in the predictive models probably because measurement of the ccp score through rna concentrations is more quantitative and better represents the underlying biology . included ccp panel : research in context systematic review we searched pubmed through the national center for biotechnology information search engine with key terms prostate cancer , prognostic , and rna expression . 
also , the ndings of most studies were not shown to be robust in terms of patient composition or clinical setting . to develop the cell cycle progression ( ccp ) score , we downloaded and analysed every large publicly available expression dataset that was associated with cancer outcome ( gene expression omnibus database )  . 
as a result , we concluded that ccp genes were the key components in every validated prognostic signature , and this conclusion was in accord with mosley and colleagues.29 interpretation although the appropriate management of early prostate cancer is widely acknowledged to be a major clinical issue , none of the previously de ned prognostic signatures have had a major e ect on clinical care . 
in this study , we addressed all these issues , and the results indicate that the ccp score can be helpful in assessing prognosis in a range of settings , especially for patients with a good prognosis such as gleason score 6 . 
the ccp score is a robust measure of the proliferative activity in the tumour and might be useful in ascertaining which prostate cancers can be safely managed with a conservative strategy . 
further validation studies are needed , especially for screen - detected cancers that are diagnosed by use of needle biopsy when conservative management is an option . the evidence presented here indicates that the ccp score adds signi cantly to the predictive power of the clinical variables typically used to predict disease outcome after surgery and at the time of disease diagnosis . 
although potentially useful in both of these settings , the most pressing clinical need is to accurately separate indolent disease in men with newly diagnosed cancer , which is unlikely to be fatal , from the more aggressive cancers treatment . 
 currently , gleason score and baseline psa concentration are the strongest predictors , and extent of disease and ki67 add only a small additional discrimination.34 clinical stage , which was only available for some of the turp cohort , was only weakly predictive of outcome in previous analyses.31 results from the univariate analysis of the turp cohort have shown that the ccp score was a stronger predictor of death from prostate cancer than in need of radical vol 12 march 2011 articles were any of the other variables , and multivariate analysis indicated that this score added a substantial amount of prognostic information not captured by any other measure . 
this result is supported by an hr of 174 in the prostatectomy cohort and 257 in the turp cohort in the multivariate model for a 1 - unit increase in the ccp score . 
when the ccp score was adjusted for clinical variables , the hrs were 168 and 306 , respectively , for a change from the 25th to 75th percentiles of the ccp score distributions in each cohort . 
although the area under the receiver operating characteristic curve ( auc ) does not account for time - to - event information or censoring , it has become a common way to compare predictive scores for an event . 
for an event in the rst 5 years , the auc in the prostatectomy cohort for biochemical recurrence was 0825 for the clinical score , and 0842 for the combined score ( including the ccp score )  . 
 additionally , the added value of the ccp score to clinical variables can be noted by comparison of the outcomes of patients in the lowest quartile versus highest quartile of the clinical score versus the combined score . 
comparison of the 10 - year event proportions in the highest quartile showed that the kaplan - meier estimates were 843% ( clinical score ) versus 836% ( combined score ) for the cohort of patients who had under gone radical prostatectomy ( biochemical recurrence ) , and 626% versus 674% , respectively , for the turp cohort ( death from prostate cancer )  . 
therefore , addition of the ccp score to clinical variables allows more accurate prediction of which men can be safely managed by watchful waiting , and , of equal importance , which men with apparently low - risk disease actually are at high risk of death from prostate cancer and might bene t from radical treatment . 
 for example , 8% of the entire cohort and 15% of men with a gleason score of 6 or less could be identi ed with a 10 - year death rate from prostate cancer of less than 2% , and 17% of those with a gleason score of 6 or less still had a 10 - year death rate from prostate cancer of more than 10% . versus ccp genes have been shown to be prognostic in breast cancer.29 they have also proven to be prognostic in lung and brain cancers.35 , 36 the results of these previous studies led us to assess whether ccp genes would be useful in prostate cancer . 
 as a result , the interpretation of this study is not complicated by the extensive multiple testing inherent in more comprehensive discovery strategies , and , its measurement therefore , we can be highly con dent about the main conclusions of this report . 
we do not claim , however , that the ccp score contains every gene that might be prognostic in prostate cancer , and additional studies might uncover biomarkers that greatly improve the overall performance of our predictive models . 
assessment of the value of the ccp score in clinical trials of adjuvant radiation , androgen deprivation , and other systemic treatments is warranted to establish whether this signature can help in the decisions about treatments in that setting too . important step is an contributors all authors approved the nal report and contributed to the study . 
for the turp cohort study , jc and gf contributed to the experimental design , writing the report , and data analysis ; dmb and csf participated in the pathology review and interpretation ; hm was involved in coordinating cancer registry clinical data ; es participated in specimen preparation ; ps and hm were involved in the study plan and design . 
for the prostatectomy cohort study , gps and arb were involved in the experimental design , writing the report , and data analysis ; vos participated in the pathology review and interpretation ; and jer , ag , and ddf contributed to the statistical analysis . con icts of interest jsl , ag , ss , sw , ay , ddf , jp , jer , and jdw are employees of myriad genetics . 
the other authors declared that they have no con icts of interest . acknowledgments we gratefully recognise the patients who participated in this study and the support from cancer research uk , queen mary university of london , the orchid appeal , national institutes of health ( spore ca92629 ) , and the koch foundation and myriad genetics . 
we assessed the prognostic value of a prede ned cell cycle progression ( ccp ) score in two cohorts of patients with prostate cancer . methods we measured the expression of 31 genes involved in ccp with quantitative rt - pcr on rna extracted from formalinxed para n - embedded tumour samples , and created a prede ned score and assessed its usefulness in the prediction of disease outcome . 
the signature was assessed retrospectively in a cohort of patients from the usa who had undergone radical prostatectomy , and in a cohort of randomly selected men with clinically localised prostate cancer diagnosed by use of a transurethral resection of the prostate ( turp ) in the uk who were managed conservatively . 
the primary endpoint was time to biochemical recurrence for the cohort of patients who had radical prostatectomy , and time to death from prostate cancer for the turp cohort . findings after prostatectomy , the ccp score was useful for predicting biochemical recurrence in the univariate analysis ( hazard ratio for a 1 - unit change [ doubling ] in ccp 189 ; 95% ci 154231 ; p = 5610 ) and the best multivariate analysis ( 177 , 140222 ; p = 4310 )  . 
in the best predictive model ( nal multivariate analysis ) , the ccp score and prostate - speci c antigen ( psa ) concentration were the most important variables and were more signi cant than any other clinical variable . 
in the turp cohort , the ccp score was the most important variable for prediction of time to death from prostate cancer in both univariate analysis ( 292 , 238357 , p = 6110 ) and the nal multivariate analysis ( 257 , 193343 ; p = 8210 ) , and was stronger than all other prognostic factors , although psa concentration also added useful information . 
heterogeneity in the hazard ratio for the ccp score was not noted in any case for any clinical variables . interpretation the results of this study provide strong evidence that the ccp score is a robust prognostic marker , which , after additional validation , could have an essential role in determining the appropriate treatment for patients with prostate cancer . funding cancer research uk , queen mary university of london , orchid appeal , us national institutes of health , and koch foundation . introduction prostate cancer is a common diagnosis , especially when prostate - speci c antigen ( psa ) screening is used , 1 and its natural history is highly variable and di cult to predict . 
we therefore selected a set of ccp genes and retrospectively tested their prognostic value in prediction of disease outcome using a prede ned score , in a cohort of patients with prostate cancer who had been treated with radical prostatectomy and in a cohort of conservatively treated patients . methods ccp gene selection to reliably generate expression data from formalinxed para n - embedded ( ffpe ) tissue , we selected 126 ccp 804 consecutive patients with radical prostatectomy 775 with clinical data 442 with available tumour tissue 410 eligible for analysis 29 no clinical data 333 no available tissue 32 excluded because of treatment with neoadjuvant therapies 44 excluded because of poor - quality cell - cycle - progression scores 366 analysed for gene expression data figure 1 : flow chart of cohort with radical prostatectomy genes from the gene expression omnibus database and tested their performance with rna extracted from 96 commercially available ffpe prostate tumour sections ( asterand , detroit , mi , usa ) obtained from anonymous patients . 
 therefore , we selected genes for inclusion in the signature on the basis of their correlation with the mean expression of the entire set of ccp genes ( webappendix pp 14 )  . 
the nal signature consisted of 31 ccp genes ( foxm1 , cdc20 , cdkn3 , cdc2 , kif11 , kiaa0101 , nusap1 , cenpf , aspm , bub1b , rrm2 , dlgap5 , birc5 , kif20a , plk1 , top2a , tk1 , pbk , asf1b , c18orf24 , rad54l , pttg1 , cdca3 , mcm10 , prc1 , dtl , cep55 , rad51 , cenpm , cdca8 , and orc6l )  . 
these highly correlated genes were used to provide a robust and highly reproducible measurement of cell proliferation and were not intended factors to capture ( eg , invasive potential )  . information to other related radical prostatectomy cohort men who had undergone radical prostatectomy for prostate cancer from 198595 were identi ed through the tumour registry at the scott and white clinic , temple , tx , usa . 
the specimens were inked , and pathological ndings were recorded as positive for bladder neck or urethral margin , invasion into the capsule , extension through the capsule , positive margins , and the involvement of the seminal vesicles . 
 biochemical recurrence was de ned as a psa concentration greater than 03 ng / ml based on the management policy used in the 1990s , and was not changed for this analysis . 
we selected patients who had not been treated with neoadjuvant drugs and for whom clinical data and tumour tissue were available for inclusion in this study to create a retrospective cohort . 
 institutional review board approval was obtained from the scott and white clinic . transurethral resection of prostate ( turp ) cohort for the population - based retrospective watchful - waiting cohort , potential cases of prostate cancer were identi ed 246 vol 12 march 2011 articles 214 ( 156293 ) 132 ( 094185 ) 164 ( 088306 ) 145 ( 110193 ) 215 ( 153301 ) 143 ( 109189 ) 224 ( 167301 ) 165 ( 126217 ) 220 ( 170285 ) 155 ( 114211 ) 189 ( 154231 ) 833% * 619% * 445% * 237% * ccp score recurrence hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) from six cancer registries in great britawithin each region , cases from collaborating hospitals were reviewed , and full details of these cases have been reported.31 men were included in this study if they had clinically localised prostate cancer , which was diagnosed by use of turp between 1990 and 1996 ( inclusively ) , were younger than 76 years at the time of diagnosis , and had a baseline psa measurement . 
men who had hormone therapy before diagnostic biopsy were also excluded because of the e ects of hormone treatment on interpretation of the gleason score . original histological specimens from the diagnostic procedure were requested , collected , and centrally reviewed by a panel of expert urological pathologists to con rm the turp diagnosis and , when necessary , to reassign gleason scores for all the prostate cancers by use of a contemporary interpretation16 of the gleason scoring syste follow - up was through the cancer registries and the last review took place in december , 2006 . 
 deaths were divided into two categories , those from prostate cancer and those from other causes , according to whos standardised criteria.32 national ethics approval was obtained from the northern multicentre research ethics committee , followed by local ethics committee approval at each of the turp cohort the collaborating hospitals for ( webappendix p 6 )  . gene expression depending on tumour volume , ve to 12 consecutive 5 m ( turp ) or 10 m ( prostatectomy ) ffpe tumour sections were used to isolate tumour - derived rna . 
we switched from rneasy ffpe to mirneasy because the new kit consistently generated figure 2 : analysis of cell cycle progression ( ccp ) score in cohort with radical prostatectomy ( a ) distribution of the ccp scores for 366 patients . 
2 values were 5493 , 415 , and 841 in the univariate analysis , multivariate analysis , and nal model , respectively , when gleason scores were assessed as a three - group categorical variable with 2 degrees of freedo table 1 : summary of statistical analysis of prostatectomy cohort , by biochemical recurrence better rna yields . 
no di erence was noted between the kits in terms of the data for gene expression . total rna was treated with dnase i ( sigma - aldrich , st louis , mo , usa ) before cdna synthesis . 
however , most samples ( 90% of radical prostatectomy cohort and 85% of turp cohort ) could be used to generate ccp scores , and therefore , had rna of adequate quality . before measurement of gene expression , the cdna was preampli ed in a pooled reaction containing taqman assays ( applied biosystems )  . 
the ampli cation reaction was diluted 1 : 20 with the 1tris - edta bu er before it was loaded on taqman low density arrays ( applied biosystems ) to assess the ampli ed genes . 
a total of 31 prede ned ccp genes and 15 housekeeper genes were ampli ed on one taqman low density array . ccp score the ccp score for each individual was calculated . 
the values of each of three replicates of each of the 31 ccp genes were normalised by subtraction of the average of up to 15 non - failed housekeeper genes for that replicate ( centred with a prede ned value ) to give c * t . 
this quantity was then converted to a value that was proportional to the copy number , calculated as 2c * for missing c * t values , due to low expression , 2c * was set as equal to 0 . 
for each ccp gene , the mean 2c * of the qualifying replicatesie , those with expression of at least 13 housekeeper genes , was then averaged over the qualifying ccp genes . 
this is the normalised average of 2c * t and was converted back to create the ccp score by taking a base 2 logaritha ccp gene was judged as having failed if more than one replicate did not qualify , or if two replicates quali ed and one of them had 2c * equal to 0 , or if the standard deviation between the three 248 vol 12 march 2011 articles replicate c * t values exceeded 05 . 
ccp scores with the number of failing ccp genes greater than nine of 31 , or a high sd between scores calculated from the three replicates , were rejected and excluded from the analysis . 
 the interassay variability has been established in our laboratory and the sd of the ccp score for experimental replicates is 01 . statistical analysis survival analysis was done with cox proportional hazards models . 
the clinical variables recorded for the prostatectomy cohort were diagnostic gleason score , most recent prebiopsy psa concentration , clinical stage , clinical grade , primary treatment ( no preoperative or postoperative hormones , orchiectomy , or adjuvant radiation ) , age at surgery , pathological tumour stage , pathological grade , pathological gleason score , and invasion features . the primary endpoint for the turp cohort was time to death from prostate cancer . 
biochemical progression was not an appropriate outcome for this cohort , since baseline psa concentrations remain elevated and some patients will have chosen to start hormones or have radical treatment without evidence of increasing psa concentration . 
the variables recorded for the turp cohort were centrally reviewed gleason grade and score , baseline psa value , clinical stage , extent of disease ( proportion of turp chips with disease ) , age at diagnosis , and initial treatment ( no initial treatment or early hormone management )  . 
 the analysis set and a complete analysis plan were agreed , and all ccp scores were assigned , before the clinical and outcome data were unmasked . in both cohorts , psa concentration was modelled as the natural logarithm of 1 + psa ( ng / ml )  . 
 as indicated above , for the prostatectomy cohort , only a single pathological gleason score was recorded at diagnosis ; for the turp cohort , 3 + 4 and 4 + 3 were shown to have nearly identical prognosis.13 , 31 therefore , a total gleason score of 7 was analysed as one group . 
 for simplicity , gleason scores were grouped into less combined risk score combined risk score stratied by gleason score figure 3 : 10 - year predicted risk of recurrence for di erent combined risk scores in cohort with radical prostatectomy ( a ) , and distribution of the combined risk scores for di erent subgroups based on gleason scores ( b ) the probability of recurrence was estimated from a cox proportional hazard model by use of the combined risk score . than 7 , 7 , and greater than 7 ( radical prostatectomy cohort : less than 7 [ 56% with score 6 ] , greater than 7 [ 75% with score 8 , 19% with score 9 ] ; turp cohort : less than 7 [ 88% with score 6 ( all 3 + 3 ) ] , 7 [ 34% with score 4 + 3 ] , and greater than 7 [ 51% with score 8 , 46% with score 9 ] )  . 
all p values were twosided and 95% cis and p values were based on statistics with 1 degree of freedom obtained from partial likelihood models . the main assessment was a univariate analysis of the association between outcome and ccp score . 
this later e ect was measured by use of the decrease in the likelihood ratio when the ccp score was omitted from a model containing it and the other relevant baseline clinicopathological variables . 
in construction of the best prognostic model , the goal was to capture most of the prognostic information from the ccp score and the clinical covariates in a simple linear model without over tting the data . 
a multivariate proportional ( cox ) hazards model was used to achieve this goal and to create a combined score based on the major clinical variable and the ccp score . 
the ccp score was evaluated vol 12 march 2011 articles 1658 reviewed histology and assigned gleason score 747 diagnosed by use of needle biopsy 2333 eligible patients 675 excluded 203 not requested 472 excluded after review 283 unknown or missing histology slides 43 incorrect pathology specimen 135 histologically ungradeable gleason score 6 no tissue in block 5 histologically ungradeable gleason score 911 diagnosed by use of turp 429 unselected samples identied for analysis 482 not included in this study 7 previous hormone therapy 31 ineligible for study 9 psa > 100 ng / ml 6 missing baseline psa 4 previous cancer 4 metastases within 6 months 1 biopsy not between 199096 61 excluded because of poor - quality cell - cycle progression scores 398 available for analysis 337 eligible in nal analysis figure 4 : flow chart of cohort with transurethral resection of prostate ( turp ) psa = prostate - speci c antigen . as a linear and a quadratic term , and tested for interactions with individual covariates . 
we used a forward stepwise regression in which a new variable was added only if it had a p value of less than 002 for the prostatectomy study and 005 for the turp study ( since fewer variables were tested )  . 
the corresponding author had full access to the data ( as did ss , jer , and dm ) , and takes full responsibility in submitting the report for publication . the results for radical prostatectomy cohort , patients characteristics and treatment outcomes have been reported previously.33 figure 1 summarises the selection of 410 patients for this study who underwent radical prostatectomy . 
the median preoperative psa concentration was 69 ng / ml ( 46109 ) , and 281 ( 71% ) of 397 patients had psa concentrations less than 10 ng / ml . 
a unit change in the score corresponds to a doubling in expression level . that were the the univariate analysis showed that in the patients who had undergone radical prostatectomy , a high ccp score was predictive of biochemical recurrence ( table 1 )  . 
 addition of a quadratic term for ccp score was not signi cant ( p = 063 ) , indicating that a simple linear model would capture most of the prognostic information from the signature . 
 the ccp score was only weakly correlated with other variables , the highest correlation was with the gleason score and psa ( pearsons ( cid : 1 ) values , 022 and 021 respectively )  . 
however , patients with higher clinical 250 vol 12 march 2011 articles 276 ( 103740 ) 205 ( 105401 ) 213 ( 160285 ) 267 ( 159447 ) 351 ( 195635 ) 505 ( 289883 ) 208 ( 134324 ) 412 ( 1671021 ) 246 ( 182333 ) 292 ( 199429 ) 560 ( 2671175 ) 225 ( 177287 ) 292 ( 239357 ) 783% * 346% * 131% * 22% * risk ( ie , gleason score > 6 and psa concentrations > 10 ng / ml ) tended to have a reduced ccp hazard ratio ( hr )  . 
the ccp score was predictive for death after disease progression ( hr 299 , 95% ci 169528 ; p = 00007 )  . in the full multivariate analysis of the prostatectomy cohort , ccp and psa concentration were the most signi cant predictors of biochemical recurrence , and provided more prognostic information than did any other variable ( table 1 )  . 
the best multivariate model was developed by forward stepwise regression and is given by combined risk score 055 ccp + 081 log ( 1 + psa ) + 028 tstage + 064 margin + { 030 ( gleason score 7 ) + 099 ( gleason score > 7 ) } figure 3a shows how the risk of biochemical recurrence in the nal 10 years increased as a function of the combined risk score , and given the central prognostic role of the gleason score , gure 3b shows the distribution of combined risk score in di erent gleason score categories . for the turp cohort , the selection of patients is summarised in gure 4 . 
we report the results obtained with a randomly selected subset of 337 men diagnosed by use of turp for which we were able to compute the ccp score ( gure 4 )  . 
within 10 years of diagnosis , 171 ( 51% ) of 337 men had died , 68 ( 20% ) from prostate cancer and 103 ( 31% ) from other causes . figure 5a shows the distribution of the ccp score among the 337 patients in the turp cohort . 
by comparison with the gleason score , psa , cancer extent , and ki67 , the ccp score provided the most prognostic information in the univariate analysis , with the being slightly greater than that for the gleason score ( table 2 ) , and substantially larger than for all other variables . 
 compared with the prostatectomy cohort , the ccp score figure 5 : analysis of cell cycle progression ( ccp ) score in cohort with transurethral resection of prostate ( turp ) ( a ) distribution of the ccp scores ( n = 337 )  . 
2 values were 813 , 54 , and 71 in the univariate analysis , multivariate analysis , and nal model , respectively , when gleason score was assessed as a three - group categorical variable with 2 df ( when increased to ve groups , 2 values were 94 , 54 , and 72 , respectively )  . 
 table 2 : summary of statistical analysis of transurethral resection of the prostate cohort combined risk score in the full multivariate analysis , after adjustment for psa concentration , gleason score , ki67 expression , and extent of disease , the ccp score was dominant ( table 2 ) , providing more information than did any other variable . 
 none of the variables showed a signi cant interaction with the ccp score , and the hr for the ccp score was only slightly attenuated when other factors were added to the model ( table 2 )  . 
 hormone treatment was signi cant in a univariate model ( hr 381 , 95% ci 240605 ) , but did not add signi cant predictive information in the multivariate model ( 112 , 068184 ) , presumably because the decision to use this treatment was based on the known prognostic factors . 
 addition of a quadratic term for ccp was also not signi cant in the multivariate model ( p = 013 )  . in the forward stepwise regression model , with the variables ccp , psa concentration , and gleason score , the best predictor was the combined risk score calculated as function of figure 6a shows the predicted 10 - year death rate from prostate cancer the increases as a combined score ; gure 6b shows the distribution of the combined score in di erent gleason score categories . 
for men with a tumour that was gleason score 6 or less , use of the combined score identi ed 28 ( 16% ) of 172 patients with a 10 - year risk of death from prostate cancer that was less than 2% , and 102 ( 59% ) of 172 with a risk less than 5% , but also identi ed 25 ( 15% ) with a risk greater than 10% , indicating that not all gleason score 6 or less tumours are low risk . 
for gleason score 7 combined risk score stratied by gleason score 095 ccp + 061 log ( 1 + psa ) + { 090 ( gleason score 7 ) + 100 ( gleason score > 7 ) } figure 6 : 10 - year predicted risk of prostate cancer death for di erent combined risk scores in cohort with transurethral resection of prostate ( a ) , and distribution of the combined risk scores for di erent subgroups based on gleason scores ( b ) the probability of prostate cancer death was estimated from a cox proportional hazard model by use of the combined risk score . correlated more with gleason score ( pearsons ( cid : 1 ) = 061 ) , log ( 1 + psa ) ( ( cid : 1 ) = 027 ) , ki67 ( ( cid : 1 ) = 050 ) , and extent of disease ( ( cid : 1 ) = 051 )  . 
the prognostic value of the ccp score was similar in di erent gleason categories and when strati ed by psa , extent of disease , and ki67 ( gure 5b )  . 
figure 5c shows a kaplan - meier plot of the proportion of patients dying of prostate cancer at di erent follow - up times grouped by integer values of the ccp score . 252 vol 12 march 2011 articles ( either 3 + 4 or 4 + 3 ) , the corresponding data were none of 73 patients , eight ( 11% ) , and 59 ( 81% ) , respectively . 
in the whole cohort , the numbers and percentages were 28 ( 8% ) of 337 , 111 ( 33% ) , and 173 ( 51% ) , respectively . when we assessed deaths from other causes , the only signi cant factor was age . 
neither the ccp score nor other major prognostic factors for prostate cancer death were signi cant causes , indicating that confounding by other deaths cannot explain these ndings . discussion the ccp score was predictive of outcome in both cohorts and provided substantially more prognostic information than did clinical variables alone . 
expression of ccp genes is higher in actively growing cells , and presumably by measuring the expression of ccp genes , we are indirectly measuring the growth rate and inherent aggressiveness of the tumour , which ultimately a ects outcome . 
three of the genes in our signaturetop2a , rrm2 , and birc5have been previously associated with prostate cancer outcome , 14 , 15 but we believe the use of a larger panel will ensure robustness of the score . 
notably , many ccp genes are putative targets of cytotoxic or radiation therapies : rrm ( pemetrexed and gemcitabine ) , top 2a ( anthracyclines ) , kif11 and kif20a ( taxanes ) , tk1 ( uorouracil ) , and rad51 and rad54l ( radiation , alkylating drugs , and novel targeted drugs ) , and therefore ccp may be useful in predicting response to treatment . both cohorts have their strengths and weaknesses . 
the cohort of patients who had undergone radical prostatectomy were mainly screen detected , and had lower baseline gleason scores and psa concentrations , but a very low death rate from prostate cancer . 
the turp cohort had more aggressive disease , which meant that prostate cancer mortality could be reliably modelled , but was all based on symptomatic patients and turp samples , which is unusual in contemporary practice . 
in both settings , ccp score and psa concentration were the dominant variables , whereas other clinical variables ( including gleason score ) did not retain most of their univariate prognostic usefulness . 
by contrast ki67 , which is coded for by a ccp gene and by itself can be predictive of outcome in this dataset , 34 was eliminated from models that immunohistochemical score . 
 assessment of ki67 is dominated in the predictive models probably because measurement of the ccp score through rna concentrations is more quantitative and better represents the underlying biology . included ccp panel : research in context systematic review we searched pubmed through the national center for biotechnology information search engine with key terms prostate cancer , prognostic , and rna expression . 
also , the ndings of most studies were not shown to be robust in terms of patient composition or clinical setting . to develop the cell cycle progression ( ccp ) score , we downloaded and analysed every large publicly available expression dataset that was associated with cancer outcome ( gene expression omnibus database )  . 
as a result , we concluded that ccp genes were the key components in every validated prognostic signature , and this conclusion was in accord with mosley and colleagues.29 interpretation although the appropriate management of early prostate cancer is widely acknowledged to be a major clinical issue , none of the previously de ned prognostic signatures have had a major e ect on clinical care . 
in this study , we addressed all these issues , and the results indicate that the ccp score can be helpful in assessing prognosis in a range of settings , especially for patients with a good prognosis such as gleason score 6 . 
the ccp score is a robust measure of the proliferative activity in the tumour and might be useful in ascertaining which prostate cancers can be safely managed with a conservative strategy . 
further validation studies are needed , especially for screen - detected cancers that are diagnosed by use of needle biopsy when conservative management is an option . the evidence presented here indicates that the ccp score adds signi cantly to the predictive power of the clinical variables typically used to predict disease outcome after surgery and at the time of disease diagnosis . 
although potentially useful in both of these settings , the most pressing clinical need is to accurately separate indolent disease in men with newly diagnosed cancer , which is unlikely to be fatal , from the more aggressive cancers treatment . 
 currently , gleason score and baseline psa concentration are the strongest predictors , and extent of disease and ki67 add only a small additional discrimination.34 clinical stage , which was only available for some of the turp cohort , was only weakly predictive of outcome in previous analyses.31 results from the univariate analysis of the turp cohort have shown that the ccp score was a stronger predictor of death from prostate cancer than in need of radical vol 12 march 2011 articles were any of the other variables , and multivariate analysis indicated that this score added a substantial amount of prognostic information not captured by any other measure . 
this result is supported by an hr of 174 in the prostatectomy cohort and 257 in the turp cohort in the multivariate model for a 1 - unit increase in the ccp score . 
when the ccp score was adjusted for clinical variables , the hrs were 168 and 306 , respectively , for a change from the 25th to 75th percentiles of the ccp score distributions in each cohort . 
although the area under the receiver operating characteristic curve ( auc ) does not account for time - to - event information or censoring , it has become a common way to compare predictive scores for an event . 
for an event in the rst 5 years , the auc in the prostatectomy cohort for biochemical recurrence was 0825 for the clinical score , and 0842 for the combined score ( including the ccp score )  . 
 additionally , the added value of the ccp score to clinical variables can be noted by comparison of the outcomes of patients in the lowest quartile versus highest quartile of the clinical score versus the combined score . 
comparison of the 10 - year event proportions in the highest quartile showed that the kaplan - meier estimates were 843% ( clinical score ) versus 836% ( combined score ) for the cohort of patients who had under gone radical prostatectomy ( biochemical recurrence ) , and 626% versus 674% , respectively , for the turp cohort ( death from prostate cancer )  . 
therefore , addition of the ccp score to clinical variables allows more accurate prediction of which men can be safely managed by watchful waiting , and , of equal importance , which men with apparently low - risk disease actually are at high risk of death from prostate cancer and might bene t from radical treatment . 
 for example , 8% of the entire cohort and 15% of men with a gleason score of 6 or less could be identi ed with a 10 - year death rate from prostate cancer of less than 2% , and 17% of those with a gleason score of 6 or less still had a 10 - year death rate from prostate cancer of more than 10% . versus ccp genes have been shown to be prognostic in breast cancer.29 they have also proven to be prognostic in lung and brain cancers.35 , 36 the results of these previous studies led us to assess whether ccp genes would be useful in prostate cancer . 
 as a result , the interpretation of this study is not complicated by the extensive multiple testing inherent in more comprehensive discovery strategies , and , its measurement therefore , we can be highly con dent about the main conclusions of this report . 
we do not claim , however , that the ccp score contains every gene that might be prognostic in prostate cancer , and additional studies might uncover biomarkers that greatly improve the overall performance of our predictive models . 
assessment of the value of the ccp score in clinical trials of adjuvant radiation , androgen deprivation , and other systemic treatments is warranted to establish whether this signature can help in the decisions about treatments in that setting too . important step is an contributors all authors approved the nal report and contributed to the study . 
for the turp cohort study , jc and gf contributed to the experimental design , writing the report , and data analysis ; dmb and csf participated in the pathology review and interpretation ; hm was involved in coordinating cancer registry clinical data ; es participated in specimen preparation ; ps and hm were involved in the study plan and design . 
for the prostatectomy cohort study , gps and arb were involved in the experimental design , writing the report , and data analysis ; vos participated in the pathology review and interpretation ; and jer , ag , and ddf contributed to the statistical analysis . con icts of interest jsl , ag , ss , sw , ay , ddf , jp , jer , and jdw are employees of myriad genetics . 
the other authors declared that they have no con icts of interest . acknowledgments we gratefully recognise the patients who participated in this study and the support from cancer research uk , queen mary university of london , the orchid appeal , national institutes of health ( spore ca92629 ) , and the koch foundation and myriad genetics . 
we aimed to assess the value of her2 and top2a as predictive markers of response to anthracycline - based adjuvant therapy in patients with early breast cancer . methods we did a meta - analysis of individual patient data from ve randomised adjuvant trials that compared anthracycline - based regimens with cyclophosphamide , methotrexate , and uorouracil ( cmf ) regimens . 
we calculated hazard ratios ( hr ) to compare event - free survival ( efs ) and overall survival in patients receiving anthracycline - based treatment with those receiving cmf in two her2 cohorts ( her2 ampli ed and non - ampli ed tumours ) and in three top2a cohorts ( normal , ampli ed , and deleted tumours )  . findings we analysed data for 3452 patients for her2 and 3102 patients for top2a . 
for efs , hrs were 089 ( 95% ci 079101 ) for her2 non - ampli ed patients and 071 ( 058086 ) for her2 - ampli ed patients ( pinteraction = 00485 ) ; for overall survival , hrs were 091 ( 95% ci 079105 ) for her2 non - ampli ed patients and 073 ( 059089 ) for her2 - ampli ed patients ( pinteraction = 00718 )  . 
in analysis of top2a status , hrs for efs were 088 ( 078100 ) for normal , 063 ( 046087 ) for deleted , and 062 ( 043090 ) for ampli ed ( pinteraction = 00513 ) ; hrs for overall survival were 089 ( 078103 ) for normal , 068 ( 049095 ) for deleted , and 067 ( 046098 ) for ampli ed ( pinteraction = 01608 )  . 
 when patients with top2a - deleted and top2a - ampli ed tumours were grouped together ( altered cohort ) and compared with data from patients with normal top2a tumours , hrs for efs were 064 ( 050081 ) for altered and 088 ( 078100 ) for normal ( pinteraction = 00183 ) ; hrs for overall survival were 067 ( 052086 ) for altered and 089 ( 078103 ) for normal ( pinteraction = 00455 )  . interpretation although her2 ampli cation and combined top2a ampli cation and deletion may have some value in the prediction of responsiveness to anthracycline - based chemotherapy , our ndings do not support the use of anthracyclines only in patients with her2 - ampli ed or top2a - aberrated tumours . funding associazione italiana ricerca cancro , academy of finland , belgian federation against cancer , cancer research uk , les amis de linstitut bordet , scottish breast cancer trials group , ncic clinical trials group , canadian cancer society research institute , danish council for strategic research , pharmacia - upjohn ( now p zer ) , and abbott laboratories . from several introduction findings retrospective analyses of randomised trials have suggested that anthracyclinecontaining adjuvant therapy might be bene cial to only those patients with breast cancer who have her2 gene ampli cation or protein overexpression , 14 but this e ect cannot be explained by any biological rationale . 
one of the the topoisomerase ii proteinthe gene for which , top2a , is on chromosome 17q12 - q21.5 other retrospective analyses have suggested that anthracycline - containing adjuvant therapy might be most e ective in patients whose tumours carry ampli ed top2a.68 however , this association was not seen in a study reported in 2008.9 two studies suggested that top2a gene deletion might targets of anthracycline intracellular also confer increased sensitivity to anthracyclines , 10 , 11 although , as with her2 , this e ect cannot be explained by any biological rationale.5 these studies have lent support to the idea of a tailored approach to the use of anthracyclines . 
nevertheless , none of them alone could safely lead to rm conclusions for daily practice , because small study sample sizes have necessitated caution in application to routine care of patients . 
 national laboratories quality control an external laboratory ( laboratory of cancer biology , university of tampere , tampere , finland ) was originally going to do the central assessment of her2 and top2a for all tumour specimens with sections cut from tissue microarrays . 
however , in december , 2006 , the protocol was amended because preliminary data showed suboptimum concordance between results from the external laboratory and those from the four national laboratories that did the assessments for the original studies when the external laboratory tested her2 and top2a on tissue microarray sections . 
testing for both markers at the four national laboratories was done by uorescent in - situ hybridisation ( fish ) , as described in the individual publications.4 , 6 , 911 in the external laboratory , testing was done by fish with three probes for her2 , top2a , and the centromere of chromosome 17 ( abbott laboratories , abbott park , il , usa )  . 
for this analysis , a tumour was de ned as her2 ampli ed or top2a ampli ed if the ratio between her2 or top2a gene copy number and number of copies of chromosome 17 centromere was two or more ; we regarded top2a gene to be deleted if the ratio was 08 or lower and to be top2a normal if the ratio was greater than 08 but lower than two . 
we estimated concordance in her2 and top2a scores between the external and the four national laboratories by calculating the proportion of cases with the same de nition of gene status ( ie , ampli ed or non - ampli ed for her2 , and ampli ed , deleted , or normal for top2a )  . 
 during on - site monitoring visits , local data , sample ow , and fish protocols were collected and veri ed for at least 50 randomly selected patients in each national laboratory . 
 level of compliance to randomised interventions was veri ed for each individual trial . subgroup analysis we prospectively de ned four biologically homogeneous cohorts : ( 1 ) highly hormone - sensitive tumours , de ned as oestrogen - receptor and progesterone - receptor positive ( 10% of immunostained cells ) , her2 non - ampli ed , and grade 12 ; ( 2 ) moderately hormone - sensitive tumours , de ned as oestrogen - receptor positive and progesteronereceptor negative independent of grade and her2 gene status , or oestrogen - receptor and progesterone - receptor positive and grade 3 , or her2 gene ampli ed ; ( 3 ) her2ampli ed tumours which were oestrogen - receptor and progesterone - receptor negative ; and ( 4 ) triple - negative tumours , de ned as oestrogen - receptor and progesteronereceptor negative and her2 non - ampli ed . 
we identi ed these four cohorts on the basis of gene expression signature studies reported in the past decade.17 oestrogenreceptor , progesterone - receptor , and histological grading were assessed at either local pathology units ( piccart and colleagues , 14 ejlersten and colleagues , 15 and poole and colleagues [ neat and br9601 trials ] 16 ) or the national laboratory ( levine and colleagues13 )  . 
 considering this assump tion , we ran the analysis by molecular subgroups twiceie , with and without the data from the neat and br9601 trials.16 the two analyses gave very similar results , so the molecular subgroup analyses include data from the neat and br9601 trials.16 statistical analysis the primary study endpoint was the comparison in terms of efs and overall survival between patients who received anthracycline - based treatment and those who received cmf in the two her2 cohorts ( her2 ampli ed and non - ampli ed tumours ) and in the three top2a cohorts ( top2a normal , ampli ed , and deleted tumours )  . 
in a secondary efs and overall survival analysis , the log - rank test was adjusted by the main prognostic factorspathological tumour size ( 2 cm or > 2 cm ) and number of ipsilateral positive axillary nodes ( node - negative , 13 positive nodes , or 4 positive nodes )  . 
 the test for interaction had two degrees of freedom when patients were divided by top2a status into three cohorts ( ie , normal , ampli ed , or deleted ) and one degree of freedom when patients were allocated in two cohorts ( ie , normal or aberrated )  . 
we used sas version 9.1 and splus version 7 for statistical analyses . role of funding sources the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results 1003 ( 22% ) of 4558 of patients could not be assessed in the meta - analysis because of an absence of data for her2 or top2a gene status ( table 1 )  . 
when efs curves from patients who participated in the meta - analysis were compared with those from patients who did not , within each trial and by treatment group , we recorded no statistically signi cant di erences ( data not shown )  . 
in piccart and colleagues trial , 14 top2a gene status was assessed only within the her2 ampli ed cohort , which might explain why the rate of top2a gene ampli cation is more than double than that in the other trials . 
likewise , the high proportion of her2 gene ampli cation reported in the ejlertsen and colleagues trial15 might be explained by most patients having oestrogen - receptor - negative disease . 
 the bene t of treatment with anthracyclines over treatment with cmf was greater for individuals with her2 gene ampli cation than it was for individuals without her2 gene ampli cation when analysing efs ( pinteraction = 00485 ) , but not when analysing overall survival ( pinteraction = 00718 ; gure 1 and gure 2 )  . 
we recorded no signi cant di erence in the bene t of treatment with anthracyclines over treatment with cmf when assessing the three separate top2a cohorts in terms of either efs ( pinteraction = 00513 ) or overall survival ( pinteraction = 01608 ; 1138 vol 12 november 2011 articles hazard ratio ( 95% ci ) 139 ( 075257 ) 099 ( 063155 ) 176 ( 048642 ) 070 ( 033149 ) 123 ( 080188 ) 111 ( 087143 ) 122 ( 076196 ) 067 ( 047095 ) 177 ( 032969 ) 061 ( 031123 ) 090 ( 063127 ) 084 ( 069103 ) 043 ( 012147 ) 068 ( 030155 ) 068 ( 040114 ) 086 ( 035211 ) 076 ( 042139 ) 070 ( 051096 ) 134 ( 050362 ) 094 ( 050176 ) 072 ( 040131 ) 037 ( 015090 ) 089 ( 060131 ) 082 ( 063107 ) gure 1 and gure 2 )  . 
however , when top2a ampli cations and deletions were combined ( altered cohort ) , we recorded a signi cant di erence in the bene t of treatment with anthracyclines over treatment with cmf between patients with normal top2a status and those with altered top2a status when analysing both efs ( pinteraction = 00183 ) and overall survival ( pinteraction = 00455 ; gure 1 and gure 2 )  . 
 for when adjusted according to the main prognostic factors ( ie , pathological tumour size and number of positive the e ect of ipsilateral axillary nodes ) , hrs anthracyclines versus cmf in patients with her2 gene ampli cation were 070 ( 95% ci 057085 ; p = 00004 ) for efs and 073 ( 059090 ; p = 0003 ) for overall survival , and , for patients without her2 gene ampli cation , were 085 ( 075096 ; p = 0012 ) for efs and 087 ( 075101 ; p = 0061 ) for overall survival . 
after adjustment , the bene t of treatment with anthracyclines over treatment with cmf was not statistically di erent between individuals with her2 ampli cation and those without her2 ampli cation in either efs ( pinteraction = 010 ) or overall survival ( pinteraction = 017 )  . 
 for top2a , adjusted hrs were 062 ( 042092 ; p = 0019 ) for efs and 068 ( 045102 ; p = 0060 ) for overall survival for patients with top2a ampli cation , 057 ( 041081 ; p = 0002 ) for efs and 064 ( 045092 ; p = 0016 ) for overall survival for patients with top2a deletion , and 086 ( 076098 ; p = 0024 ) for efs and 087 ( 075 100 ; p = 0057 ) for overall survival for patients with top2a normal . 
after adjustment , the bene t of treatment with anthracyclines over treatment with cmf di ered signi cantly between the three groups in terms of efs ( pinteraction = 004 ) but not in overall survival ( pinteraction = 019 )  . 
when top2a ampli cations and deletions were combined , adjusted hrs were 060 ( 047077 ; p = 00001 ) for efs and 063 ( 048082 ; p = 00005 ) for overall survival in patients with top2a alterations , and 086 ( 076098 ; p = 0024 ) for efs and 087 ( 075100 ; p = 0056 ) for overall survival in patients with top2a - normal tumours . 
the bene t of treatment with anthracyclines over treatment with cmf di ered signi cantly between the two groups in terms of both efs ( pinteraction = 0013 ) and overall survival ( pinteraction = 0033 )  . of 2588 patients with data that could be assessed , 740 ( 29% ) were de ned as highly hormone - sensitive , 878 ( 34% ) as moderately hormone - sensitive , 311 ( 12% ) as her2 ampli ed and oestrogen - receptor and progesterone - receptor negative , and 659 ( 25% ) as triple negative ( gure 3 and gure 4 )  . 
we recorded no signi cant di erence treatment e ect of anthracyclines or cmf between molecular subgroups , but individuals with her2 - ampli ed tumours seemed to respond better to anthracyclines and those with highly hormone - sensitive tumours seemed to respond better to cmf ( gure 3 )  . 
we compared treatment groups by top2a gene status within the her2 positive molecular subgroup , and , in all three cohorts , anthracycline - based therapy seemed to be more e ective than cmf ( webappendix p 2 )  . 
 discussion our ndings show a greater bene t from anthracyclinebased adjuvant therapy in patients with her2 gene ampli cation than in patients without such ampli cation and in patients with top2a gene alterations than in patients with normal top2a status . 
however , our study also shows that patients with her2 non - ampli ed or top2a normal tumours might have some additional bene t from treatment with anthracyclines , which than a qualitative suggests a quantitative rather interaction between anthracycline activity and her2 or top2a status . 
 this meta - analysis we trials with di erences in the type of anthracycline - based regimens or in the cmf schedules used ( webappendix p 1 ) , which included vol 12 november 2011 1139 articles patients events risk group anthracycline - based patients events risk group anthracycline - based number at risk anthracycline - based year year patients events risk group anthracycline - based patients events risk group anthracycline - based number at risk anthracycline - based year year figure 4 : event - free survival analysis , by molecular subgroups survival in patients with ( a ) highly hormone - sensitive tumours , ( b ) moderately hormone - sensitive tumours , ( c ) her2 - ampli ed tumours , and ( d ) triple - negative tumours . is a potential limitation in the interpretation of the study results , although we recorded similar associations in the interaction between the activity of treatments and her2 or top2a status in each individual trial . 
 two pooled analyses of previously published data have investigated her2 , but not top2a , in the same setting with similar results.18 , 19 neither of these studies did an external quality control substudy for the testing of her2 or top2a . 
our study design chose the external laboratory as the gold standard , but because tumour samples assessed in the external laboratory were not tested in another laboratory , and because samples from the four national laboratories were not cross - compared , we cannot identify the reason behind the recorded discordance . 
in view of the retrospective nature of this assessment and the restricted sample size , the results of this subgroup analysis have to be regarded as merely hypothesis - generating and should not lead to changes in clinical practice . 
this analysis , prompted by the known molecular and clinical heterogeneity of breast cancer , 17 suggests that , in contradiction to previously reported studies that analysed the her2 non - ampli ed cohort as a homogeneous group , 14 , 6 , 9 , 10 , 18 , 19 di erential bene t from anthracyclines might exist within the her2 non - ampli ed cohort . 
in our analysis individuals with triple - negative or moderately hormone - sensitive tumours 1140 vol 12 november 2011 articles seemed to respond better to treatment with anthracyclines than to treatment with cmf . 
because all triple - negative tumours and almost 90% of moderately hormone - sensitive tumours from this study did not carry top2a gene ampli cation , other mechanisms of increased sensitivity to anthracycline might exist . 
we de ned triple - negative tumours as such if oestrogen - receptor and progesteronereceptor immunostaining was less than 10% , and not less than 1% as suggested in international guidelines.20 however we regard this discrepancy as irrelevant with regard to the suggested bene t from anthracyclines in patients who do not carry top2a gene ampli cation . 
 triple - negative tumours and moderately hormonesensitive tumours are often characterised by high proliferation rates.2123 proliferation signals can lead to topoisomerase ii protein over - expression independently of top2a gene status.24 , 25 indeed , data reported elsewhere2627 draw attention to the absence of concordance between top2a gene status and protein concentrations within the same tumour . 
ideally , quanti cation of nuclear concentrations of the topoisomerase ii protein ( ie , the active protein isoform ) might be the most appropriate way to investigate its predictive value.28 other biological factors not related to top2a have been investigated as potential markers of sensitivity to anthracyclines . 
among those , polysomy of chromosome 17 , which could be a marker of genomic instability and dna repair dysfunction , might play a part.29 moreover , factors involved in the regulation of the stromatumour interaction or in the immune response against a tumour might also be involved.3032 future studies looking at molecular markers to predict response to anthracyclines will have to take into account the fact that probably only a multifactorial system will predict responsiveness to anthracyclines . in conclusion , our ndings do not justify routine use of her2 and top2a as molecular markers to predict anthracycline activity , because women with non - her2 ampli ed and non - top2a altered tumours seem to derive bene ts from treatment with anthracyclines , and because problems exist with the reproducibility of top2a gene status assessment by fish . contributors adl , jmsb , be , kip , cp , ji , hm , fpom , dc , mjp , and mb had the idea for and designed the study . 
cd , jmsb , be , kip , dl , cp , he , hm , fpom , fc , am , cjt , cs , ls , dc , and mjp provided study materials . con icts of interest adl has a consultancy and advisory role for and has received honoraria from schering - plough . 
kip has a consultancy and advisory role for and has received honoraria from roche , abraxis , astrazeneca , p zer , novartis , and amgen , and has given expert testimony for novartis and astrazeneca . 
all other authors declare that they have no con icts of interest . acknowledgments we thank associazione italiana ricerca cancro , abbott laboratories , academy of finland , belgian federation against cancer , cancer research uk , les amis de linstitut bordet , p zer , scottish bc trials group , ncic clinical trials group , the canadian cancer society research institite ( ccsri ) , and the danish council for strategic research for funding . editorial for the acs letter see center / acs - can - requestssurgeon - generals - report - onsugar - sweetened - beverages / for more on overweight and obesity and cancer see n engl j med 2003 ; 348 : 162538 for more on the 2012 cancer prevention guidelines see ca cancer j clin 2012 ; 62 : 3067 for more on physical activity see comment lancet 2012 ; 380 : 18990 for more on the food industry see plos med 2012 ; 9 : e1001246 for more on cynical marketing and brand alignment see editorial lancet 2012 ; 380 : 188 for more on the un declaration on non - communicable diseases see editorial lancet oncol 2011 ; 12 : 981 healthy choice should be the easy choice on july 3 , 2012 , the american cancer society ( acs ) cancer action network asked the us surgeon general to initiate a comprehensive review of the consumption of sugarsweetened beverages and their e ects on healthwith the aim of raising public consciousness and changing behaviours in choices of food and beverages . 
 the acss request is in line with its recent guidelines on nutrition and physical activity for cancer prevention , which proposed individuals recommendations ( eg , limit consumption of high - calorie foods and beverages ) and for community action ( eg , decrease access to and marketing of food and beverages of low nutritional value , particularly to youth )  . for current trends towards increasing portion sizes , sugarsweetened drinks , additives , high - calorie convenience foods , and ready meals , compounded by decreased physical activity , have contributed to the obesity epidemic in the usa , and similar trends are now being seen in many other countries worldwide . 
 the availability of healthy choices are made by individuals , but they can be either facilitated or impeded by social , physical , and economic factors , and by the regulatory environment . 
 access to , and a ordability of healthy foods , compared inexpensive , extensively with marketed high - calorie foods and beverages of low nutritional value , and barriers to physical activity , all contribute to obesity . 
e orts are therefore essential to create an environment that encourages healthy choices , promoting physical activity and increasing access to a ordable , healthy food while decreasing access toand exposure to marketing of food and beverages of low nutritional value . 
 cynical marketing and brand alignment often culminate in the junk food and drink giantseg , mcdonalds , coca cola , and cadburys at the 2012 olympics games in londonacting as major sponsors of sporting and social events . 
corporate responsibility campaigns that deftly shift responsibility for overconsumption from corporations to individuals to forestall regulation and promote brandtactics similar to those employed by the tobacco industryare also worrying and should be strongly discouraged . 
for instance , companies could be incentivised to decrease additive content over longer periods of time to gradually acclimatise consumers to the di erence while not having a major e ect on the viability of their business . interventions and strategies should aim to make healthy choices the easiest choices . 
at both the individual and community level , health policies should aim to : improve awareness and information about bene ts of a healthy lifestyle ; introduce appropriate scal measures to make healthy food more a ordable ; and enhance regulatory mechanisms and measures that increase nutritional information or restrict marketing of unhealthy food . 
the 2004 who global strategy on diet , physical activity , and health , and the 2011 un highlevel summit political declaration on the prevention of non - communicable diseasesin response to the rapid changes in nutrition and physical activity all over the globeprovide a framework that should be implemented and strengthened . 
it took nearly ve decades from the us surgeon generals report on tobacco and cancer for e ective public health policies to be put in place ; we cannot wait that long this time . 
we report on whether selective focal ablation of unifocal and multifocal cancer lesions can reduce this treatment burden . methods men aged 4580 years were eligible for this prospective development study if they had low - risk to high - risk localised prostate cancer ( prostate speci c antigen [ psa ] 15 ng / ml , gleason score 4 + 3 , stage t2 ) , with no previous androgen deprivation or treatment for prostate cancer , and who could safely undergo multiparametric mri and have a general anaesthetic . 
patients received focal therapy using high - intensity focused ultrasound , delivered to all known cancer lesions , with a margin of normal tissue , identi ed on multiparametric mri , template prostate - mapping biopsies , or both . 
 nine men ( 22% , 95% ci 1138 ) had self - resolving , mild to moderate , intermittent dysuria ( median duration 50 days [ iqr 25185 ] )  . 
median overall international index of erectile function - 15 ( iief - 15 ) scores were similar at baseline and at 12 months ( p = 0060 ) , as were median iief - 15 scores for intercourse satisfaction ( p = 0454 ) , sexual desire ( p = 0644 ) , and overall satisfaction ( p = 0257 )  . 
there was an improvement in lower urinary tract symptoms , assessed by international prostate symptom score ( ipss ) , between baseline and 12 months ( p = 0026 ) , but the ipss - quality of life score showed no di erence between baseline and 12 months ( p = 0655 )  . 
no signi cant di erence was reported in median trial outcomes index scores between baseline and 12 months ( p = 0113 ) but signi cant improvement was shown in median functional assessment of cancer therapy ( fact ) - prostate ( p = 0045 ) and median fact - general scores ( p = 0041 )  . 
no histological evidence of cancer was identi ed in 30 of 39 men biopsied at 6 months ( 77% , 95% ci 6189 ) ; 36 ( 92% , 7998 ) were free of clinically signi cant cancer . 
after retreatment in four men , 39 of 41 ( 95% , 95% ci 8399 ) had no evidence of disease on multiparametric mri at 12 months . interpretation focal therapy of individual prostate cancer lesions , whether multifocal or unifocal , leads to a low rate of genitourinary side - e ects and an encouraging rate of early absence of clinically signi cant prostate cancer . funding medical research council ( uk ) , pelican cancer foundation , and st peters trust . introduction the management of localised prostate cancer remains controversial because the systematic over - diagnosis that accompanies the current diagnostic pathway results in over - treatment.1 at present , radical whole - gland surgery or radiotherapy can result in substantial side - e ects that are a consequence of damage to surrounding structures . 
 these include urinary incontinence ( 520% ) , erectile dysfunction ( 3070% ) , and bowel toxicity ( 510% ) .2 , 3 technological re ne ments do not seem to have reduced the burden of harm.4 , 5 apart from active surveillance for low - risk disease , few strategies are available to address the burden of treatment - related side - e ects in other risk categories . 
 one strategy that has shown promise relates to managing prostate cancer in the same manner as most other solid organ malignanciesby focusing injury to the the therapy to the cancer lesion , 622 vol 13 june 2012 articles the protocol was anonymously peer - reviewed by the national cancer research network ( ncrn ) , uk , and the medical research council , uk . for the study protocol see therapy / hifu / focal / focal - hifuprotocol bladder , rectum , and neurovascular bundles could be reduced.6 , 7 we have previously assessed hemi - ablation of patients with localised unilateral prostate cancer , 8 which included treatment of the entire half of the prostate associated with cancer . 
this strategy is the most straight forward to undertake , standardise , and train others to do , but is limited because only one in ve men have true unilateral disease on template biopsies . 
furthermore , hemi - ablation might represent overtreatment since a low - volume , lowgrade lesion would be treated in the same manner as a high - volume , high - grade cancer . 
in this study , we postulated that selective focal ablation of unifocal and multifocal cancer lesions with a margin of normal tissue could reduce genitourinary and rectal side - e ects for men with localised prostate cancer . methods study design and patients we undertook a two - centre , prospective development study , as de ned by the ideal ( idea , development , exploration , assessment , and long - term ) guidelines for assessing innovation in surgery.9 men could enter into the study if they had localised prostate cancer on multiparametric mri and templateprostate - mapping biopsies.10 transperineal we included men with low - risk to high - risk disease ( prostate - speci c antigen [ psa ] 15 ng / ml , gleason score 4 + 3 , stage t2 ) , aged 4580 years with a life expectancy of 5 years or more , a prostate volume of 40 ml or less or maximum anteriorposterior length of 40 mm or less who had undergone multiparametric mri and transperineal template ( 5 mm spaced ) biopsies in the 6 months before recruitment . 
we excluded men who had androgen suppression within the previous 6 months , previous radiation therapy or chemotherapy for prostate cancer , latex allergies , previous rectal surgery preventing insertion of transrectal probe , intraprostatic calci cations making high - intensity focused ultrasound ( hifu ) of focal areas of cancer di cult , previous transurethral resection of the prostate or laser prostatectomy in 5 years before recruitment , previous hifu , cryosurgery , or thermal or microwave therapy to the prostate at any point before recruitment . 
men who were not t for general anaesthesia or regional anaes thesia as assessed by a consultant anaesthetist , or were unable to have mri scanning ( eg , severe claustrophobia , permanent cardiac pacemaker , metallic to contribute implant signi cant artifact to images ) were also excluded . 
all men gave written informed consent . likely our trial was approved by the university college london hospitals local research ethics committee a , uk , which is under the auspices of the national research ethics service . 
additionally , contrast - enhance ment procedures to locate areas of cancer , multiparametric mri was done at 15 t magnetic eld strength with pelvic phased - array included t2 - weighting , dynamic coils . 
all biopsies were reported by a single uropathologist . men underwent focal ablation with a transrectal hifu device ( sonablate 500 ; focus surgery , indianapolis , in , usa )  . 
the dimensions of the target area were determined by the focal length of the transducer , the applied frequency , the intensity of the applied power ( w / cm ) , and the duration of the pulse . 
its long axis lies at right angles to the transducer and is greatest in length towards the transducer . this temperature tissue destruction is produced by thermal , mechanical , and cavitation e ects to produce a clearly demarcated region of coagulative necrosis surrounded by normal tissue on microscopic examination . 
adequate cell destruction can be produced by short exposure ( 1 s ) to temperatures of 60c or more , which has therefore been adopted as the minimum target temperature . 
cooling due to tissue perfusion in the focal zone is not a problem because the rate of heating is greater than that of cooling when the exposure time is within a window of 3 s . 
cavitation results from gas ( bubble ) formation within cells due to heat and mechanical energy deposition causing bubbles to oscillate . all patients had sterile urine on culture before treatment . 
if culture was positive for infection , men were treated with antibiotics and their treatment rescheduled ; prophy lactic intravenous gentamicin was given to all men at the time of general anaesthetic . 
the operator made judgments as to the location and boundaries of the cancer lesions for treatment planning on the basis of the information from both multiparametric mri ( when a lesion was visible ) and template - prostate - mapping biopsies . 
designation of individual lesions was usually straightforward but when positive biopsies were close together , lesions were labelled separately if there was at least one intervening normal biopsy . after ablation , the suprapubic catheter was placed on free drainage into a urinary leg - bag for 12 days and urethral voiding was encouraged thereafter by closure of a valve attached to the catheter . 
because many men travelled a long distance , the timing of catheter removal was delayed to coincide with the rst trial visit after the operation at 1014 days ( for an early mri ) even if urethral voiding was restored earlier . 
 a contrast - enhanced mri was done 1014 days after focal hifu to con rm the area of ablation , as shown by a con uent perfusion de cit . follow - up consisted of clinic visits at 1 month , 3 months , 6 months , 9 months , and 12 months for psa measurement and adverse event reporting . 
 questionnaires included the international prostate symptom score ( ipss ) , international index of erectile function - 15 ( iief - 15 ) , ucla - expanded prostate cancer index composite ( epic ) urinary incontinence scale , and the functional assessment of cancer therapyprostate ( fact - p ) score , which includes fact - general ( fact - g ) scores and the trials outcome index.1115 phosphodiesterase - 5 inhibitors were permitted at any timepoint during follow - up . 
at 6 months , another multiparametric mri followed by targeted biopsies of the treated areas were scheduled with a minimum requirement for sampling every 1 ml of residual tissue with one core . 
our justi cation for one biopsy for every ml of residual tissue re ects the biopsy density of the original template biopsies before focal hifu ( which was about 1 ml for every biopsy )  . 
as the purpose of the 6 - month biopsies was to determine whether the ablation was successful , our ethics com mittee did not permit sampling of untreated tissue due to the requirement for another general anaesthetic . 
however , biopsies of the untreated tissue were permitted if a new , potentially malignant lesion was seen on multiparametric mri . the primary outcomes were feasibility , patient acceptability , and side - e ect pro le of focal hifu . 
the iief - 15 was used to report the proportion of men capable of having erectile function su cient for penetration at 12 months as well as total iief - 15 score and domain scores on erectile function , intercourse satisfaction , orgasmic function , sexual desire , and overall satisfaction . 
the continence questionnaire included total scores as well as the proportion of patients who were pad - free , or leak - free and pad - free at 12 months . 
quality of life was measured with fact - p with summary measures of the trial outcome index score , fact - p score , and fact - g score . secondary outcomes were histological and imaging measures of cancer control . 
for this status to be met , we de ned trifecta as leak - free and padfree continence , erections su cient for penetration , and no evidence of clinically signi cant disease at 12 months multiparametric mri16 , 17 in those men with normal baseline genitourinary function . statistical analysis since the primary objective of the study was to determine the side - e ect pro le of focal ablation , the sample size was powered on a common event , namely erectile dysfunction . 
the sample size calculation was based on a comparison with a known rate of 40% erectile dysfunction , 18 which usually occurs when hifu is applied to the whole prostate.19 therefore , with an level of 005 and power of 90% ( 1 ) , the sample size required was at least 33 men with good baseline function . 
we adjusted the sample size to allow for the estimated rate of 25% of men having poor baseline erectile function in the general population , and therefore aimed to recruit 42 men in total . validated questionnaires were analysed with standard methods . 
missing values for patient - reported outcome 624 vol 13 june 2012 articles psa density ( ng / ml per ml prostate ) 018 ( 014022 ) age ( years ) serum psa ( ng / ml ) reason for psa test and biopsy psa screening ( patient request ) lower urinary tract symptoms * prostate volume ( ml ) initial biopsy trus biopsy tpm biopsy gleason ( trus - guided biopsy ) no trus biopsy gleason ( tpm biopsies ) clinical stage trus guided biopsies total cores total positive cores percent positive cores tpm biopsies total cores total positive cores positive cores ( % ) core density ( biopsies / ml ) number of lesions on tpm disease distribution bilateral ( midline lesion ) three unifocal unilateral multifocal unilateral bilateral high intermediate nccn risk category20 patients ( n = 41 ) 63 ( 580660 ) 66 ( 5477 ) 31 ( 76% ) 10 ( 24% ) 35 ( 290455 ) 35 ( 85% ) 6 ( 15% ) 24 ( 59% ) 7 ( 17% ) 5 ( 12% ) 5 ( 12% ) 13 ( 32% ) 24 ( 59% ) 4 ( 10% ) 37 ( 90% ) 4 ( 10% ) 15 ( 37% ) 6 ( 15% ) 5 ( 12% ) 15 ( 37% ) 11 ( 27% ) 26 ( 63% ) 4 ( 10% ) 100 ( 80120 ) 20 ( 1030 ) 110 ( 63338 ) 46 ( 355655 ) 5 ( 3090 ) 94% ( 46185 ) 14 ( 0919 ) variables ( between 2% and 10% missing values for individual questions ) were imputed with a fully conditional speci cation method and logistic regression model ( categorical data )  . 
the imputation was based on the observation of values missing completely at rando we classed the variables for which missing values were to be imputed ( questionnaires ) as categorical . 
 wilcoxon signed rank test ( two - tailed ) was used to assess di erences between continuous variables that were not normally distributed ( psa and questionnaire scores ) measured at baseline and at the 12 - month follow - up visit . 
the corresponding author had full access to all the data and had nal responsibility for the decision to submit for publication . results 42 men were recruited between june 27 , 2007 , and june 30 , 2010 . 
he had an uneventful recovery after hifu and had no respiratory symptoms immediately before treatment , or at 2 weeks and 6 weeks after treatment during the formal trial visits . 
 as a result , 41 men were included in analyses ; 30 ( 73% ) had intermediate and high - risk disease ( table 1 ) .20 three men had baseline mild stress urinary incontinence but required no pads ; 35 had good baseline sexual function with erections su cient for penetration . 
 * these men were opportunistically screened with a psa test when they presented with symptoms of lower urinary tract infection , rather than part of a formal request ( by their physician or by the men themselves ) for a psa test . 
a high number of positive cores were retrieved , despite only a maximum of three lesions , because large dominant lesions were sampled several times . table 1 : baseline characteristics see online for appendix vol 13 june 2012 articles neurovascular bundles figure 1 : schematic diagrams of the types of focal therapy unilateral one - area ablation ( a )  . 
grey transparent boxes represent ablation zones on the high - intensity focused ultrasound device . total anaesthetic time ( min ) procedure time ( suprapubic catheter + focal hifu ; min ) total hospitalisation time ( admission to discharge ; h ) discharge time ( end procedure to discharge ; h ) time with suprapubic catheter ( days ) * dysuria ( negative urine culture ) duration of dysuria ( days ) intermittent haematuria ( start of stream only ) duration of intermittent haematuria ( days ) urinary debris duration of urinary debris ( days ) urinary tract infection ( positive urine culture ) acute retention of urine value 1350 ( 11501500 ) 1050 ( 8701250 ) 120 ( 100270 ) 60 ( 50180 ) 85 ( 80150 ) 9 / 41 ( 22% , 1138 ) 5 ( 25185 ) 16 / 41 ( 39% , 2456 ) 15 ( 103150 ) 14 / 41 ( 34% , 2051 ) 145 ( 60165 ) 7 / 41 ( 17% , 732 ) 1 / 41 ( 2% , 013 ) data are median ( iqr ) or number of patients a ected / n ( % , 95% ci )  . 
 * suprapubic catheter was usually removed at the same time as the postoperative early contrast mri for convenience to reduce visits for men who travelled far to the study centre . 
 table 2 : perioperative outcomes in men undergoing focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer to moderate , urethra on the rst day after the operation with the suprapubic catheter clamped . 
he had multiparametric mri and urethrogram within 4 weeks , which showed extravasation of urine outside the prostate ; although the serosal layer of the rectum was a ected by treatment no de nitive rectourethral stula was seen . 
however , as a precautionary measure , he was managed conservatively with a suprapubic catheter and quinolone antibiotics , serial 2 monthly multiparametric mri , and a further repeat urethrogram until the extravasation had resolved by 6 months . 
at that point , he developed a stricture requiring endoscopic dilatation ; a further two limited endoscopic prostate - tissue resections to a prostate that had a total volume of 80 ml were done when voiding did not return to normal . overall iief - 15 scores initially decreased , indicating diminished erectile function but showed a gradual return to baseline by 12 months ( p = 0060 ; gure 2a )  . 
iief - 15 domain scores in intercourse satisfaction ( p = 0454 ) , sexual desire ( p = 0644 ) , and overall satisfaction ( p = 0257 ) all showed decreased scores at 1 month and 3 months , but there was no signi cant di erence between baseline and 12 months ( gure 2 c , f )  . 
iief - 15 erectile and orgasmic domains showed signi cant deteriorations from baseline to 12 months ( p = 0042 and p = 0003 , respectively ; gure 2 b , d )  . 
no formal programme of penile rehabilitation was available , but all men were o ered phosphodiesterase - 5 inhibitors ( eg , sildena l , tadala l ) if needed ; 14 of the 31 men required phosphodiesterase - 5 inhibitors . in a post - hoc analysis to explore whether type of ablation made any di erence to erectile dys function , we assessed the following factors . 
of those men who had erections su cient for penetration at baseline , 28 of 31 ( 90% , 95% ci 7498 ) of those who had unilateral nervesparing ablation and four of four ( 100% , 40100 ) who had bilateral nerve - sparing ablation had erections su cient for penetration at 12 months . 
ipss values increased initially although by 12 months showed signi cantly lower values , suggesting lower urinary - tract symptoms from baseline ( p = 0026 ; gure 4 )  . 
no signi cant di erence was seen in ipss - quality - of - life score between baseline and 12 months ( p = 0655 ; gure 4 )  . 
of 38 men with no urinary leak at baseline all ( 100% , 95% ci 91100 ) were leak - free and pad - free by 9 months ; 40 men pad - free at baseline were pad - free again by 3 months and maintained pad - free continence at 12 month ( 100% , 91100 ; one man did not report on this parameter at 12 months and was excluded )  . signi cant deterioration of health - related quality of life was shown between baseline and 12 months on the total fact - p and total fact - g scores ( p = 0045 and p = 0041 , respectively ; gure 5 )  . 
no signi cant di erence was seen between baseline and 12 months in the trial outcomes index between baseline and 12 months ( p = 0113 ; gure 5 )  . compared with baseline , a signi cant decrease in psa levels was reported at 12 months ( p < 00001 ; gure 6 )  . 
 the time to nadir was not calculated because the psa changes showed a pattern of ongoing small decreases in psa up to trial end at 12 months . one man refused to undergo biopsy at 6 months because of his concern over the e ect of further biopsies on sexual function . 
of the n = 41 n = 41 n = 41 n = 41 n = 41 n = 41 ( n = 2 ) ( n = 1 ) ( n = 3 ) ( n = 1 ) ( n = 1 ) ( n = 3 ) time ( months ) figure 4 : urinary function after focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer , measured with international prostate symptom score ( ipss ) questionnaire two - tailed p values were reported for wilcoxon signed ranks test comparing baseline and 12 - month median scores . 
median baseline versus 12 - month international prostate symptom score ( ipss ) : 80 ( iqr 55130 ) vs 70 ( 30120 , p = 0026 ; a )  . 
median baseline versus 12 - month ipss - quality of life : 10 ( 0020 ) vs 10 ( 1010 , p = 0655 ; b )  . 39 men biopsied , nine ( 23% , 95% ci 1139 ) had evidence of cancer while three ( 8% , 221 ) had evidence of clinically signi cant cancer ( epstein criteria21 , 22gleason > 3 + 3 , > 2 cores positive , > 2 mm cancer involve ment ; table 3 )  . 
median baseline versus 12 - month functional assessment of cancer therapy ( fact ) - prostate score : 1385 ( 13301470 ) vs 1453 ( 13701520 , p = 0045 ; b )  . 
as de ned by epstein criteria : gleason > 3 + 3 , > 2 cores positive , 3 mm cancer involvement . table 3 : histological outcomes at 6 months in men undergoing focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer 9 months and 29 ng / ml ( 1836 ) at 12 months . 
none of the four men undergoing repeat focal therapy consented to further biopsies but all had multiparametric mri at trial exit showing no evidence of clinically signi cant disease at 12 months . 
no man required adjuvant radiotherapy , prostate cancer surgery , or androgen deprivation therapy during the trial duration . vol 13 june 2012 articles 39 / 41 * ( 95% , 95% ci 8399 ) 26 / 31 * ( 84% , 95% ci 6695 ) pad - free continence leak - free / pad - free continence erections sucient for penetration no evidence of disease trifecta ( pad - free , leak - free , and erectile function satisfatory for penetration , and no evidence of clinically signicant disease ) any cancer on biopsy clinically signicant cancer on biopsy ( 3 mm and / or gleason > 3 + 3 ) time ( months ) 9 / 39 * ( 23% , 95% ci 1139 ) 3 / 39 ( 8% , 95% ci 221 ) functional outcome continence * pad - free and leak free pad - free erections satisfactory for penetration use of phosphodiesterase 5 inhibitors|| 26 ( 68% , 5183 ) 33 ( 83% , 6793 ) 19 ( 54% , 3771 ) 36 ( 95% , 8299 ) 38 37 ( 97% , 86100 ) ( 100% , 91100 ) ( 100% , 91100 ) 40 40 40 38 ( 100% , 91100 ) ( 100% , 91100 ) ( 100% , 91100 ) ( 100% , 91100 ) ( 83% , 6693 ) 29 ( 83% , 6693 ) 31 ( 89% , 7397 ) ( 89% , 7397 ) 3 / 35 ( 9% ) 4 / 19 ( 21% , 646 ) 14 / 29 ( 48% , 2967 ) 17 / 29 ( 59% , 3976 ) 17 / 31 ( 55% , 3673 ) 14 / 31 ( 45% , 2764 ) figure 7 : trifecta rate after focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer patient - reported trifecta outcomes were reported with validated questionnaires . 
proportion of men scoring 2 on question 2 of iief - 15 : over the past 4 weeks when you had erections with sexual stimulation , how often were your erections hard enough for penetration ?  . 
||phosphodiesterase - 5 inhibitors ( tadala l , sildena l , or vardena l ; percentage calculated with denominator as those achieving erections su cient for intercourse )  . of the 31 men with good baseline function , 26 ( 84% , 95% ci 6695 ) achieved the trifecta status of having leak - free and pad - free continence , erections su cient for intercourse , and no evidence of clinically signi cant disease on multipara metric mri at 12 months ( gure 7 )  . 
 discussion to our knowledge , our study is the rst to assess targeting of individual known cancer areas , with a margin of normal tissue , in men with multifocal as well as unifocal prostate cancer across all cancer - risk categories . 
almost 90% of men reported having erections satisfactory for intercourse at 12 months , and all were continent . there was a signi cant decrease in psa levels from baseline to 12 months , with concentrations of serum psa continuing to decline months after the initial treatment . 
conclusions from this nding should not be made , although if this decline in serum psa were to be reproduced , one possible reason for it might be the presentation of antigens to the immune response leading to a secondary immune response against the remaining prostate tissue.23 there are several limitations to our study . 
second , characterisation of disease with templateprostate - mapping biopsies before focal therapy was di erent to the 6 - month veri cation biopsy , because of research ethics committee stipulations to limit patient burden . 
the trial will assess focal hifu applied to clinically signi cant areas of prostate cancer identi ed on entry by multiparametric mri and template prostate - mapping biopsies25 , 26 followed by further multiparametric mri and template prostate - mapping biopsies applied to treated and untreated tissue at 3 years ( nct01194648 )  . 
destruction of some normal tissue is necessary to incorporate an adequate margin but because of the nature of the hifu therapy , our margins are likely to be larger than they need to be . 
furthermore , image - registration of preoperative mri to treatment delivery could further help to reduce destruction of normal tissue by allowing the clinician to more accurately de ne the boundaries of the target lesion . many retrospective series have reported case encouraging short - term functional and cancer - control outcomes of men treated in a focal manner with hifu and cryotherapy.2732 a prospective feasibility trial has reported on the use of focal interstitial laser therapy in a small cohort of 12 men with very low - risk unifocal disease.33 we have previously reported8 the outcomes from a prospective development study of 20 men with unilateral disease undergoing ablation of an entire prostate lobe using hifu . 
18 ( 90% ) were leak - free and pad - free continent while 19 ( 95% ) were pad - free after 630 vol 13 june 2012 articles panel : research in context systematic review in 2007 , we did a systematic review7 of reports on medline and pubmed databases using the terms focal therapy and prostate cancer and / or high intensity focused ultrasound and / or cryotherapy / cryoablation / cryosurgery . 
subsequent to this review , we started a health technology assessment of focal therapy , following the phased approach described by the medical research council complex interventions guidelines and subsequently formalised in the ideal guidelines for assessing surgical procedures.9 interpretation our study showed that the rate of genitourinary side - e ects associated with focal therapy is low , coupled with an encouraging rate of early absence of clinically signi cant prostate cancer . 
these ndings rea rm two other prospective development studies8 , 33 in which focal using high - intensity focused ultrasound and photothermal therapy was used . focal therapy could hold promise in mitigating the harms that result from current therapeutic strategies . 
any randomised controlled trial should be pragmatic in nature and adaptive in execution , so that actual clinical practice is re ected and new technological developments can be incorporated as they occur . 
furthermore , since the natural history of prostate cancer is long , timelines based on metastases and mortality , which would require a trial at least 15 years in duration , might not be feasible or warranted . 
subsequent linkage to national electronic registries will ensure that robust cancer - control outcomes are still reported at a later date . hemi - ablation ; 17 ( 89% ) of 19 achieved trifecta status at 12 months.8 the current study allowed user or operator determination of ablative zones within the prostate on an individual basis provided our standardised method of focal therapy was followed . 
however , the treatments invariably followed one of three patterns of ablation ( gure 1 ) , by contrast with our previous study , 8 whereby the treatment method was xed and standardised by mandating therapy to the entire half of the prostate associated with cancer ( hemi - ablation ) regardless of individual lesion grade , volume , or location and proximity to a neurovascular bundle . while our current study is not directly comparable to previous studies of focal therapy ( panel ) , it continues to support the proposition that tissue preservation leads to functional preservation . 
the histological outcomes in this study were slightly worse than those reported for hemiablation , perhaps because of the requirements for increased pre cision of focal ablationindividual areas of cancer were targeted as opposed to a standardised hemiablationwith a resulting reduction in margin around the cancer . 
image - registration software to accurately fuse , in real - time , pretreatment location data to intraoperative ultrasound images could improve histological outcomes.34 another reasonable explanation might relate to physical limitations of the ablative technology . 
new irreversible electroporation and platforms such as photodynamic therapy are theor etically more tissuespeci c and could allow neurovascular bundle preservation even if the ablative zone is close to the prostate capsule ; tissue speci city of these techniques has not yet been assessed . in conclusion , focal therapy of individual prostatecancer lesions , regardless of whether they are multifocal or unifocal , leads to a low rate of genitourinary sidee ects and an encouraging rate of early freedom from clinically signi cant prostate cancer . 
if the functional outcomes that we report are reproduced in larger studies and coupled with acceptable rates of cancer control in the medium to long term , focal therapy could o er a strategy by which the burden of treatmentrelated side - e ects are addressed for a substantial proportion of men with localised prostate cancer . 
the design and execution of comparative - e ectiveness research assessing long - term cancer control needs to be prioritised , especially at a pace than can match the potential for informal di usion . contributors me and hua conceived the study . 
all authors contributed to the drafting and editing of the manuscript and approved the nal version . con icts of interest me and hua received funding from ushifu , glaxosmithkline , and advanced medical diagnostics for clinical trials . 
me and hua are paid consultants to steba biotech and have received funding from ushifu , focused surgery , misonix ( manufacturers and distributors of the sonablate 500 high - intensity focused ultrasound device ) , and oncura and ge healthcare for medical consultancy and travel to conferences . 
 all other authors declared no con icts of interest . acknowledgments this study was funded by the uk medical research council , the pelican cancer foundation , and st peters trust , and sponsored by university college london hospitals nhs foundation trust . 
we thank the men vol 13 june 2012 articles who agreed to participate in this trial , and jane coe and victor abu for their invaluable help and support during the duration of the study . 
hua and me receive funding for other research projects from the wellcome trust , national institute of health research - health technology assessment programme , the us national institute of healthnational cancer institute , prostate action , and prostate cancer research centre . 
 me receives funding in part from the uk national institute of health research university college london hospitals / university college london comprehensive biomedical research centre . errata see articles page 528 errata miller va , hirsh v , cadranel j , et al . 
afatinib versus placebo for patients with advanced , metastatic non - small - cell lung cancer after failure of erlotinib , ge tinib , or both , and one or two lines of chemotherapy ( lux - lung 1 ) : a phase 2b / 3 randomised trial . 
lancet oncol 2012 ; 13 : 52838in this article ( published online march 26 ) , the rst sentence of the fourth paragraph on the fourth page should have read we measured progression - free survival from the date of randomisation to disease progression or death , whichever occurred rst . 
this correction has been made to the online version as of april 24 , 2012 . see news page e194 vol 13 may 2012 e186 editorial evolution : the lancet oncologyan online - enhanced journal long - standing readers of the lancet oncology will have noticed changes in the journal over the years . 
as a result , we strongly encourage print readers to activate their online accounts , and for all our online - only subscribers to check the website regularly for new content . why are we doing this ? since 2005 , the lancet oncology has seen a 70% increase in the number of articles submitted from the united states , europe , and asia . 
furthermore , because cancer is fast becoming the number one cause of death in many countries , there is an ever - pressing demand for more information and rapid dissemination of ndings . 
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 the lancet oncology budget cuts in the usa : a short - term win ? on nov 18 , 2011 , president barack obama signed a bill into law that will a ect the funding for several science agencies . 
the white house o ce of science and technology policy , which advices the executive o ce about the e ects of science and technology on domestic and international a airs , has had its funding cut by more than 30% , leaving just $45 million . 
the usas budget cuts to quell the national de cit of $12 trillion by 2021 mean that several key agencies such as the national institutes of health ( nih ) and national science foundation had below - in ation increases to their funding . 
such reductions in funding might not bode well for federally funded organisationsincluding the nih and centers for disease control and prevention ( cdc ) that fund much of the cancer research in the usa . the budget cuts also extend to preventive measures , which are needed in addition to funding for research into the causes of and treatments for cancers . 
the cdc has recommended a total of $37 billion in funding for tobacco prevention programmes , but collectively individual states have only budgeted $4567 million ( 12% ) of this amount . if the usa is to remain a world leader in terms of research , any budget cuts to cancer research and prevention programmes need to be implemented judiciously because although the short - term win of saving a few dollars will look good on a budget sheet , it will not translate into medium - term and long - term solutions of stopping the rising burden of cancer . 
the usa need only look at ireland , which even in austere times , is providing improved care for patients as a result of a reorganisation of its health structures into specialist centres . 
 the lancet oncology see news page 17 for more on cuts to tobacco prevention funding see releases / post / 2011_11_30_ state_report for more on the white house o ce of science and technology policy budget cut see chemistryworld / news / 2011 / november / 21111101.asp for more on the usas budget cuts see com / news / what - does - the - usbudget - stalemate - mean - forresearch - 1.9475 for more on the rising burden of cancer see the lancet oncology commission thelancet.com / commission / delivering - a ordable - cancercare - in - high - income - countries vol 13 january 2012 e ects of zoledronic acid versus clodronic acid on skeletal morbidity in patients with newly diagnosed multiple myeloma ( mrc myeloma ix ) : secondary outcomes from a randomised controlled trial gareth j morgan * , j anthony child * , walter m gregory , alex j szubert , kim cocks , sue e bell , nuria navarro - coy , mark t drayson , roger g owen , sylvia feyler , a john ashcroft , fiona m ross , jennifer byrne , huw roddie , claudius rudin , gordon cook , graham h jackson , ping wu , faith e davies , on behalf of the national cancer research institute haematological oncology clinical studies group summary background bisphosphonates are the standard of care for reducing the risk of skeletal - related events in patients with bone lesions from multiple myeloma . 
here , we report the secondary outcomes relating to skeletal events . methods patients ( 18 years ) with newly diagnosed multiple myeloma were enrolled from 120 centres in the uk and received intensive or non - intensive antimyeloma treatment . 
a computer - generated randomisation sequence was used to allocate patients in a 1 : 1 ratio , through an automated telephone service to intravenous zoledronic acid ( 4 mg every 2128 days ) or oral clodronic acid ( 1600 mg / day ) , and the drugs were continued at least until disease progression . 
at a median follow - up of 37 years ( iqr 2947 ) , patients in the zoledronic acid group had a lower incidence of skeletal - related events than did those in the clodronic acid group ( 265 [ 27% ] vs 346 [ 35% ] , respectively ; hazard ratio 074 , 95% ci 062087 ; p = 00004 )  . 
zoledronic acid was also associated with a lower risk of any skeletal - related event in the subsets of patients with ( 233 [ 35% ] of 668 vs 292 [ 43% ] of 682 with clodronic acid ; 077 , 065092 ; p = 00038 ) and without bone lesions at baseline ( 29 [ 10% ] of 302 vs 48 [ 17% ] of 276 with clodronic acid ; 053 , 033084 ; p = 00068 )  . 
fewer patients in the zoledronic acid group had vertebral fractures than did those in the clodronic acid group ( 50 [ 5% ] in the zoledronic acid group vs 88 [ 9% ] in the clodronic acid group ; p = 00008 ) , other fractures ( 45 [ 5% ] vs 66 [ 7% ] ; p = 004 ) , and new osteolytic lesions ( 46 [ 5% ] vs 95 [ 10% ] ; p < 00001 )  . 
 interpretation the results of this study support the early use of zoledronic acid rather than clodronic acid in patients with newly diagnosed multiple myeloma for the prevention of skeletal - related events , irrespective of bone disease status at baseline . funding medical research council ( london , uk ) , novartis , schering health care , chugai , pharmion , celgene , and ortho biotech . introduction multiple myeloma , which is diagnosed in more than 100 000 people every year , 1 is characterised by the growth of malignant plasma cells in the bone marrow.2 , 3 interactions between myeloma cells and bone marrow stromal cells are fundamental to the excessive activation and proliferation of osteoclasts , causing localised bone destruction.4 myeloma cells also secrete factors that inhibit osteoblasts , blocking the repair of osteolytic damage . 
results from this trial showed that patients given zoledronic acid had signi cantly improved progression - free survival ( hazard ratio [ hr ] 088 , 95% ci 080098 ; p = 00179 ) and a reduced risk of death ( 084 , 074096 ; p = 00118 ) versus clodronic acid , with overall survival prolonged by 55 months.12 importantly , improved overall survival with zoledronic acid remained signi cant after adjustment for the e ect of skeletal - related events that ( 085 , 074097 ; p = 0018 ) , suggesting zoledronic acid has direct antimyeloma activity . 
in this analysis , we investigated in detail the e ects of clodronic acid and zoledronic acid on skeletal - related events in patients with newly diagnosed multiple myeloma . methods trial design the mrc myeloma ix trial was a multicentre ( n = 120 ) , randomised , open - label , two - by - two factorial trial , with 1970 patients with newly diagnosed multiple myeloma randomly assigned to bisphosphonates 1960 analysed ( intention - to - treat population ) 979 clodrononic and cvad , ctd , mp , or ctda 981 zoledronic acid and cvad , ctd , mp , or ctda 917 started clodronic acid 11 started zoledronic acid 15 started pamidronic acid 0 started etidronic acid 31 bisphosphonate not initiated 5 bisphosphonate not conrmed 887 started zoledronic acid 25 started clodronic acid 14 started pamidronic acid 1 started etidronic acid 45 bisphosphonate not initiated 9 bisphosphonate not conrmed 820 randomly assigned to thalidomide maintenance or watchful waiting 2 excluded 1 no consent 1 withdrew consent 408 thalidomide 410 no thalidomide 195 clodronic acid 213 zoledronic acid 195 clodronic acid 215 zoledronic acid figure 1 : trial pro le the complete trial protocol is provided in morgan and colleagues.12 cvad = cyclophosphamide , vincristine , doxorubicin , and dexamethasone . 
full details have already been reported.12 patients adult patients ( 18 years ) with newly diagnosed and histologically con rmed symptomatic multiple myeloma were eligible for inclusion in the trial . 
 exclusion criteria included previous or concurrent active tumours , acute renal failure ( de ned as serum creatinine concentration > 500 mol / l that was unresponsive to 72 h of rehydration , urine output < 400 ml / day , or requirement for dialysis ) , and previous treatment for multiple myeloma ( except local radiotherapy for bone pain or spinal cord compression , bisphosphonates for hypercalcaemia of malignancy , or low - dose corticosteroids )  . the trial was approved by the north west multi - centre research ethics committee and local review committees at all participating centres . 
all patients provided written informed consent . randomisation and masking the methods of randomisation and masking for this study have been previously described in detail.12 brie y , a computer - generated randomisation sequence was used to allocate patients in a 1 : 1 ratio by use of an automated telephone service to zoledronic acid or clodronic acid . 
 no investigators , sta , or patients were masked to treatment allocation . treatment patients were allocated to two main treatment pathways ( intensive and non - intensive ) , as previously described in detail.12 in each pathway , patients were randomly assigned to oral clodronic acid ( 1600 mg / day ) or intravenous zoledronic acid ( 4 mg , 15 min infusion every 34 weeks with induction chemotherapy and every 4 weeks thereafter )  . 
dose adjustment for patients with impaired renal function at baseline and delays in administration of the dose in patients with increases in serum creatinine concentration during the study were implemented for zoledronic acid , per the prescribing information . 
data for skeletal - related events , de ned as vertebral fractures , other fractures , spinal cord compression , need for radiation or surgery for bone lesions , and new osteolytic lesions , were analysed until disease progression . 
 these included bone fracture , radiation to bone , surgery for bone lesions and spinal cord compression , and height loss ( as an indicator for further imaging follow - up )  . 
additional prespeci ed analyses of hypercalcaemia of malignancy and exploratory analyses of skeletal - related events , excluding the development of new osteolytic lesions , were undertaken . statistical analysis the primary endpoints of progression - free survival , overall survival , and overall response rate , and the secondary endpoint of safety have been reported previously.12 here , we report the secondary endpoint of skeletal - related events . 
in the intensive pathway , we aimed to recruit 1080 patients ( 540 per group ) to test the hypothesis that cyclophosphamide , thalidomide , and dexamethasone ( ctd ) was not inferior to cyclo phosphamide , vincristine , doxorubicin , and dexamethasone ( cvad ) , with a hazard ratio of 12 and 80% power at a 5% signi cance level . 
in the non - intensive pathway , we aimed to recruit 850 patients ( 425 per group ) to assess whether attenuated ctd ( ctda ) was superior to standard chemotherapy with melphalan plus prednisolone , with 80% power at a 5% signi cance level . 
we calculated that the sample size for the intensive and non - intensive pathways combined had su cient power ( > 80% ) to detect a reduction of 10% in the proportion of patients with skeletal - related events for zoledronic acid compared with clodronic acid . analyses were based on the treatment that patients with histologically con rmed multiple myeloma who provided written informed consent were randomly assigned to receive ( intention - to - treat population )  . 
data , in part , from morgan and colleagues.12 table 1 : baseline demographics and disease characteristics of the intention - to - treat population clodronic acid zoledronic acid hr 074 ( 95% ci 062087 ) ; p = 00004 * number at risk clodronic acid zoledronic acid time from randomisation ( months ) hr 053 ( 95% ci 033084 ) ; log - rank p = 00068 hr 077 ( 95% ci 065092 ) ; log - rank p = 00038 time from randomisation ( months ) time from randomisation ( months ) number at risk clodronic acid zoledronic acid figure 2 : time to rst skeletal - related event overall ( a ) , in patients with bone lesions at baseline ( b ) , and in patients without bone lesions at baseline ( c ) hr = hazard ratio . 
to reduce the potential e ects of related skeletal - related events ( eg , a fracture requiring surgery ) in multiple - event analyses , only one skeletal - related event per 21 days was included ( eg , skeletal - related events of possibly linked causality were counted only once , and judged to be one skeletal - related event )  . 
post - hoc analyses that included all skeletal - related events irrespective of whether they were the rst or subsequent skeletal - related events within 21 days ( not reported ) were done and provided results consistent with those in which the linked events were counted as one skeletal - related event . 
all hypothesis tests were the 5% signi cance level , without adjustment for multiplicity . this trial is registered , number isrctn68454111 . two - sided and undertaken at role of the funding source no funding organisation was involved in study design , data collection , data analysis or interpretation , writing , or decision about publication submission . 
all authors had full access to trial data ; gjm , jac , and ghj had nal responsibility for the decision to submit for publication . results 1970 patients were enrolled between may 14 , 2003 , and nov 20 , 2007 , and 1960 were the intention - to - treat population ( gure 1 )  . 
baseline demographics and disease characteristics of patients were well balanced between the zoledronic acid and clodronic acid groups ( table 1 ) .12 1898 ( 97% ) of 1960 patients were white , 1401 ( 71% ) had myeloma bone disease at baseline , 562 ( 29% ) had a history of vertebral fractures , 231 ( 12% ) had previous non - vertebral fractures , 1010 ( 52% ) had been diagnosed with osteolytic lesions , and 258 ( 13% ) had previous radiotherapy ( table 1 )  . 
median follow - up was 37 years ( iqr 2847 ) for patients in the zoledronic acid group and 38 years ( 2947 ) for those in the clodronic acid group ; 582 ( 30% ) patients had been given zoledronic acid or clodronic acid for at least 2 years ( 290 [ 30% ] of 981 in the zoledronic acid group and 292 [ 30% ] of 979 in the clodronic acid group )  . 
in the overall patient population , fewer patients assigned to zoledronic acid had a skeletal - related event than did those assigned to clodronic acid ( 265 [ 27% ] of 981 vs 346 [ 35% ] of 979 , respectively ) , with zoledronic acid signi cantly reducing the risk of skeletal - related events versus clodronic acid 746 vol 12 august 2011 articles skeletal - related events incidence ( 95% ci ) overall di erence ( 95% ci ) between clodronic acid and zoledronic acid * p value for preceding 12 months clodronic acid ( n = 979 ) zoledronic acid ( n = 981 ) clodronic acid ( n = 979 ) zoledronic acid ( n = 981 ) 12 months 24 months 36 months 48 months 60 months 451 ( 46% ) 333 ( 34% ) 043 ( 038048 ) 033 ( 028037 ) 011 ( 004018 ) 93 ( 9% ) 28 ( 3% ) 13 ( 1% ) 2 ( < 1% ) 54 ( 6% ) 16 ( 2% ) 4 ( < 1% ) 2 ( < 1% ) 060 ( 053066 ) 042 ( 036048 ) 018 ( 009026 ) 069 ( 061078 ) 047 ( 040053 ) 023 ( 012033 ) 080 ( 068091 ) 049 ( 042056 ) 030 ( 017044 ) 083 ( 070095 ) 051 ( 043058 ) 032 ( 018046 ) 00002 00024 00089 00510 05359 data are number ( % ) , unless otherwise indicated . 
unadjusted p value for the comparison of incidence of skeletal - related events in zoledronic acid group versus clodronic acid group per 12 months ( eg , 24 - month p value is for incidence between 12 months and 24 months )  . table 2 : cumulative annual incidence of rst and subsequent skeletal - related events for the intention - to - treat population after randomisation clodronic acid zoledronic acid ( gure 2a )  . 
the total number of skeletal - related events reported was also lower in the zoledronic acid group than in the clodronic acid group ( 419 vs 597 , respectively )  . 
the proportion of patients with at least one skeletal - related event was consistently lower in the zoledronic acid group versus the clodronic acid group at each timepoint ( p < 00001 overall ; table 2 )  . 
the di erence in incidences of skeletal - related events for zoledronic acid versus clodronic acid was signi cant for each of the rst 3 years separately , but the total number of skeletalrelated events was low at 48 months and 60 months , and reduced the statistical power for the respective 12 - month comparisons ( table 2 )  . 
similar distributions of skeletalrelated events were noted for patients treated with zoledronic acid and clodronic acid in the intensive ( zoledronic acid , 155 [ 28% ] of 555 ; clodronic acid , 202 [ 36% ] of 556 ; log - rank p = 0003 ) and non - intensive pathways ( zoledronic acid , 110 [ 26% ] of 426 ; clodronic acid , 144 [ 34% ] of 423 ; log - rank p = 0008 )  . 
the mean skeletal morbidity rate was lower with zoledronic acid versus clodronic acid in the intensive and non - intensive pathways ( 04 skeletal - related events per patient per year vs 08 per patient per year , respectively )  . 
however , patients who did not have myeloma bone disease at baseline had lower rates of bone pain ( 248 [ 43% ] of 578 vs 1136 [ 84% ] of 1350 ) , and higher rates of anaemia ( 330 [ 57% ] vs 523 [ 39% ] ) , renal failure ( 96 [ 17% ] vs 171 [ 13% ] ) , and infection ( 74 [ 13% ] vs 90 [ 7% ] ) than did patients with bone disease at baseline . in an exploratory analysis that excluded new osteolytic lesions from the de nition of skeletal - related event , the outcome was similar to the analysis that included new osteolytic lesions , and the reduction in risk of skeletalrelated events with zoledronic acid was still signi cant ( hr 076 , 95% ci 064089 ; log - rank p = 00011 )  . 
 further exploratory analysis by patients risk of skeletalrelated events , as identi ed in another assessment of the myeloma ix patients , 16 showed a reduced risk of p < 00001 p = 0070 any skeletal - related event except hypercalcaemia of malignancy p = 00031 p < 00001 p = 037 p = 00008 p = 0040 p = 029 radiotherapy lesion surgery to bone vertebral fracture other fracture spinal cord compresssion p = 00069 p = 022 p < 00001 p = 023 p = 0035 any skeletal - related event except hypercalcaemia of malignancy radiotherapy lesion radiotherapy lesion any skeletal - related event except hypercalcaemia of malignancy figure 3 : proportion of patients with an on - study skeletal - related event overall ( a ) , with bone lesions at baseline ( b ) , and without bone lesions at baseline ( c ) skeletal - related events with zoledronic acid versus clodronic acid in the high - risk and low - risk populations ( data not shown )  . 
analysis by cytogenetic markers ( poor prognosis de ned by use of uorescence in - situ hybridisation [ fish ] as adverse igh translocations , gain of 1q , and loss of 17p ) showed that the bene t vol 12 august 2011 articles ctda vs melphalan + prednisolone ( non - intensive pathway ) 075 ( 060094 ) zoledronic acid vs clodronic acid ctd vs cvad ( intensive pathway ) serum calcium concentration ( high vs low ) serum creatinine concentration ( high vs low ) haemoglobin concentration ( high vs low ) platelets ( high vs low ) skeletal - related events at baseline * no vs yes missing vs yes centre hazard ratio ( 95% ci ) p value 072 ( 062084 ) 091 ( 076110 ) 131 ( 111155 ) 093 ( 077112 ) 108 ( 092126 ) 119 ( 093153 ) 035 ( 028044 ) 083 ( 046152 ) < 00001 03399 00141 00012 04362 03489 01623 < 00001 05532 < 00001 ctd = cyclophosphamide , thalidomide , and dexamethasone . 
overall p value , but not hazard ratio , reported for 120 centres . table 3 : multivariate model for risk of skeletal - related events associated with zoledronic acid in terms of skeletalrelated events was attributable to the non - poor prognosis subset , 16 wherein the bene ts of zoledronic acid were especially meaningful ( log - rank p = 00012 ; data not the poor - prognosis subset , disease shown )  . 
 progression was fairly rapid , and very few patients were assessable for the time to rst skeletal - related - event endpoint at later timepoints ( 48 months and 60 months ; data not shown )  . 
 in an exploratory analysis , patients with osteolytic lesions at baseline showed a non - signi cantly longer progression - free survival than did those with no osteolytic lesions ( 20 months , 95% ci 1821 , vs 18 months , 1719 , hr 090 , 082100 ; p = 00535 )  . 
however , patients with bone disease at baseline had a higher incidence of skeletal - related events than did those without bone disease at baseline ( 525 [ 39% ] of 1350 vs 77 [ 13% ] of 578 , respectively ; p < 00001 )  . 
moreover , zoledronic acid , compared with clodronic acid , was associated with a signi cantly reduced risk of any skeletal - related event in patients with ( 233 [ 35% ] of 668 vs 292 [ 43% ] of 682 ; gure 2b ) and without bone disease at baseline ( 29 [ 10% ] of 302 vs 48 [ 17% ] of 276 ; gure 2c )  . 
zoledronic acid was associated with a reduced incidence of each type of skeletal - related event versus clodronic acid in the overall population ( gure 3a ) , and signi cant reductions were noted for any skeletal - related event ( 265 [ 27% ] of 981 vs 346 [ 35% ] of 979 for clodronic acid ; p < 00001 ) , new osteolytic lesions ( 46 [ 5% ] vs 95 [ 10% ] for clodronic acid ; p < 00001 ) , vertebral fractures ( 50 [ 5% ] vs 88 [ 9% ] for clodronic acid ; p = 00008 ) , and other fractures ( 45 [ 5% ] vs 66 [ 7% ] for clodronic acid ; p = 004 ) , but not radiotherapy ( 179 [ 18% ] vs 211 [ 22% ] for clodronic acid ; p = 007 ) , surgery to the bone ( 49 [ 5% ] vs 58 [ 6% ] for clodronic acid ; p = 037 ) , and spinal - cord compression ( 13 [ 1% ] vs 19 [ 2% ] for clodronic acid ; p = 029 )  . 
 zoledronic acid was associated with a signi cantly reduced incidence of any skeletal - related event in patients with ( gure 3b ) and without bone disease at baseline ( gure 3c )  . in a prespeci ed multivariate model of all on - study skeletal - related events , the reduction in such events with zoledronic acid versus clodronic acid remained signi cant ( table 3 )  . 
baseline serum calcium concentration , baseline skeletal - related event , melphalan plus prednisolone versus ctda ( in the non - intensive pathway ) , and treatment centre also showed signi cant correlations with risk of skeletalrelated events ( table 3 )  . 
overall , exclusion of new osteolytic lesions from the skeletal - related - events composite endpoint did not a ect model outcomes ( data not shown )  . results of further exploratory analyses showed that the proportion of patients with a skeletal - related event was signi cantly lower with zoledronic acid versus clodronic acid when the rst 12 months ( log - rank p = 00012 ) or 24 months ( log - rank p = 00102 ) were excluded from the analyses ( data not shown )  . 
furthermore , signi cantly fewer patients in the zoledronic acid group than in the clodronic acid group had at least one skeletal - related event after randomisation to maintenance thalidomide or no maintenance ( log - rank p = 00005 ; data not shown )  . 
 the incidences of most adverse events were similar in zoledronic acid and clodronic acid groups and have been previously reported.12 overall , the rates of acute renal failure were low and similar for patients in the zoledronic acid and clodronic acid groups ( 57 [ 6% ] of 983 [ two patients for whom con rmation of consent was not received were included in the safety population ] vs 60 [ 6% ] of 979 , respectively ; p = 078 )  . 
during the study , 47 ( 5% ) of 979 patients in the clodronic acid group and 43 ( 4% ) of 981 in the zoledronic acid group died of renal failure ( p = 067 ) , and 123 ( 13% ) patients in the clodronic acid group and 92 ( 9% ) in the zoledronic acid group died of multiple myeloma or treatmentrelated infections ( p = 0025 )  . 
28 ( 3% ) patients in the clodronic acid group and 28 ( 3% ) in the zoledronic acid group had hypercalcaemia , which was reported as a serious adverse event in six ( < 1% ) of 979 patients in the clodronic acid group and six ( < 1% ) of 983 in the zoledronic acid group . 
as previously reported , 12 con rmed osteonecrosis of the jaw was rare , but the rate was higher in the zoledronic acid group than in the clodronic acid group ( 35 [ 4% ] vs three [ < 1% ] , respectively ; p < 00001 )  . 
gastrointestinal serious adverse events were not signi cantly di erent with clodronic acid versus zoledronic acid ( 30 [ 3% ] vs 24 [ 2% ] , respectively ; p = 041 )  . 
 treatment - emergent serious adverse events that were suspected to be related to bisphosphonate use arose in 41 ( 45 events ) of 983 patients in the zoledronic acid group versus 33 ( 34 events ) of 979 patients in the clodronic acid group , and represented a subset of the overall treatmentemergent serious adverse events that were suspected to be 748 vol 12 august 2011 articles tenderness related to any of the study drugs as previously reported.12 in patients given zoledronic acid , treatment - emergent serious adverse events were musculoskeletal , connective tissue , and bone disorders ( n = 16 ) ; renal and urinary disorders ( n = 8 ) ; haematological disorders ( n = 5 ) ; gastrointestinal [ n = 1 ] , nausea and vomiting , disorders ( dehydration epigastric [ n = 1 ] , and nausea , vomiting , constipation , dehydration [ n = 1 ] ) ; endocrine , metabolism , or nutrition disorders ( n = 3 ) ; infections ( n = 3 ) ; cardiovascular disorders ( n = 2 ) ; skin and subcutaneous disorders ( n = 2 ) ; uid or electrolyte disturbance ( n = 1 ) ; general disorder or administration - site condition ( n = 1 ) ; and nervous system disorder ( n = 1 )  . 
in patients in the clodronic acid group , treatment - emergent events were gastrointestinal disorders ( diarrhoea [ n = 2 ] , abdominal pain and bloating [ n = 1 ] , nausea or vomiting [ n = 6 ] , oesophagitis [ n = 1 ] , haematemesis [ n = 1 ] , and gastrointestinal disturbance [ n = 1 ] ) ; renal and urinary disorders ( n = 9 ) ; infections ( n = 5 ) ; haematological disorders ( n = 2 ) ; skin and subcutaneous disorders ( n = 2 ) ; cardiovascular disorder ( n = 1 ) ; general disorder or administration - site condition ( n = 1 ) ; hepatic disorder ( n = 1 ) ; and reproductive system or breast disorder ( n = 1 )  . 
 adverse serious in progression - free discussion the results of the current analysis of the mrc myeloma ix trial show that zoledronic acid was associated with a signi cantly reduced risk of skeletal - related events versus clodronic acid in patients with newly diagnosed multiple myeloma irrespective of their bone disease status at baseline . 
additionally , zoledronic acid was associated with a reduced incidence of skeletal - related events in the intensive and non - intensive pathways , suggesting that all patients undergoing initial treatment for multiple myeloma could bene t from early use of zoledronic acid . 
 previous analyses showed that zoledronic acid was associated with a signi cant reduction in the risk of death ( hr 084 , 95% ci 074096 ; p = 00118 ) and a signi cant improvement ( 088 , 080098 ; p = 00179 ) , providing signi cant clinical bene ts and not just reduction in rates of skeletal - related events ( panel ) .12 although clinical guidelines recommend bisphosphonates for patients with documented bone lesions , 4 , 7 , 8 , 17 all patients ( ie , with or without bone disease at baseline ) could bene t when bisphosphonates are begun early in the course of multiple myeloma . 
moreover , the reductions in skeletal - related events with zoledronic acid versus clodronic acid noted throughout the course of the trial support the continued use of zoledronic acid in patients with multiple myeloma at least until disease progression , when patients went o study in this trial and data for skeletal - related events were no longer collected . 
however , the optimum duration of zoledronic acid is not known , and some patients might bene t from continuing zoledronic acid , possibly at a reduced dose , during disease remission . 
additional clinical trials are needed to further re ne these aspects of treatment . survival panel : research in context systematic review in addition to the experience obtained from previous mrc myeloma trials of clodronic acid , a review of the reports of clinical trials of a wide variety of combination chemotherapy regimens and bisphosphonates was undertaken and used to develop the 22 factorial trial design for the myeloma ix trial . 
at the time that the myeloma ix trial was initiated , most patients with symptomatic multiple myeloma in the uk were treated long - term with bisphosphonates ; however , there was no consensus for the optimum timing and duration of treatment with bisphosphonates , or the e cacy for prevention of skeletal - related events of all the available bisphosphonates and their potential to a ect disease outcomes and survival variables in patients with multiple myeloma . 
in the myeloma ix trial , we assessed the possible enhanced e ects on disease - related bone changes and survival of a third - generation bisphosphonate ( zoledronic acid ) in comparison with a standard older - generation oral agent ( clodronic acid )  . interpretation the results of the myeloma ix trial showed signi cant bene ts with zoledronic acid versus clodronic acid on progression - free survival , overall survival , and several variables for skeletal - related events , and , to our knowledge , for the rst time established the superiority of one bisphosphonate over another in patients with multiple myeloma . 
moreover , exploratory analyses have shown signi cant bene ts with treatment before the onset of bone lesions and also with long - term treatment ( eg , during maintenance therapy or long - term follow - up )  . 
the data from myeloma ix provide compelling evidence that zoledronic acid should be considered an essential component of therapeutic regimens for patients starting treatment for newly diagnosed multiple myeloma irrespective of whether bone lesions are already present , and support the continuation of zoledronic acid at least until disease progression . 
however , the results of this study do not provide insight into whether the frequency of dosing with zoledronic acid can be reduced after initial treatment , such as in patients with long - term remission of their disease . in patients with multiple myeloma , renal adverse events and osteonecrosis of the jaw are causes for concern and should be monitored and managed appropriately . 
indeed , because monitoring the concentrations of creatinine in vol 12 august 2011 articles ( ie , and reactions strategies that were colleagues13 ) the serum was less frequent for the clodronic acid group than for the zoledronic acid group ( ie , every 3 months vs monthly , respectively ) , any observation bias would be in favour of clodronic acid . 
this bias suggests that the renal adverse events reported in the myeloma ix trial were most likely a result of the disease , antimyeloma treatments , non - myeloma - related drugs , or other comorbidities rather than toxicity associated with bisphosphonates , validating the renal safety protocols for zoledronic acid . 
 recommendations for prevention and management of osteonecrosis of the jaw were implemented in myeloma ix from june , 2006 , onwards , 13 but further reductions in the risk of osteonecrosis of the jaw might be possible with prevention reported subsequently . 
the results of a study in postmenopausal women ( n = 7765 ) given intravenous zoledronic acid ( 5 mg per year ) for osteoporosis showed that the acutephase reaction lasted about 3 days and the incidence was similar to that with placebo by the third infusion.19 in myeloma ix , acute - phase reactions , which are thought to result from immune - cell activation after the rst infusion of zoledronic acid , might have been less frequent than in the postmenopausal osteoporosis setting because of the fairly high prevalence of disease and treatment - related myelosuppression in patients with multiple myeloma . 
gastrointestinal adverse events are generally more common in patients given oral bisphosphonates , as noted heregastrointestinal treatment - emergent serious adverse events arose more frequently with clodronic acid than with zoledronic acid ( 12 vs three events , respectively )  . 
 are serious , potentially debilitating complications a ecting most patients with multiple myeloma , especially those who do not receive bone - targeted therapy.6 bisphosphonates can e ectively reduce the risk of skeletal - related events in this population.2022 consequently , clinical practice guidelines and recommendations include bisphosphonates as a key component of disease treatment for patients with myeloma bone disease.4 , 78 , 17 in the previous mrc myeloma studies , 9 , 10 clodronic acid was of particular bene t ( ie , slowing progression of skeletal disease and reducing skeletal morbidity ) to patients without bone skeletal - related events lesions at treatment initiation.9 , 10 moreover , subgroup analysis suggested that clodronic acid might confer survival bene ts in patients without overt bone disease at diagnosis.10 three bisphosphonates have been approved for patients with osteolytic bone lesions from multiple myelomazoledronic acid and pamidronic acid in the usa and europe , and clodronic acid in europe . 
previous comparison of zoledronic acid with pamidronic acid in patients with multiple myeloma showed no signi cant di erence in the incidence of skeletal - related events ( 86 [ 47% ] of 183 vs 82 [ 49% ] of 167 , respectively ) , 20 or the time to rst skeletal - related event ( 380 days vs 286 days , respectively ; p = 0538 ) among patients with multiple lesions.21 the myeloma and established osteolytic more recently introduced nitrogen - containing bisphosphonates , pamidronic acid and zoledronic acid , are more potent inhibitors of osteoclastic activity than are the earlier , non - nitrogen - containing bisphosphonates ( eg , clodronic acid ) .23 however , pamidronic acid is more similar to clodronic acid in terms of antiresorptive potency than it is to zoledronic acid , which has more potent anticancer e ects in preclinical models of myeloma and other cancers.2325 because of the short infusion time and particular antiresorptive potency of zoledronic acid compared with pamidronic acid con rmed in preclinical and clinical investigationsit was adopted as the comparator for clodronic acid , a uk standard , in the myeloma ix trial . 
treatment regimens for multiple myeloma also changed between the completion of the trial of zoledronic acid versus pamidronic acid , 21 and the start of the myeloma ix trial . induction chemotherapy regimens used to treat patients with multiple myeloma are continually evolving as new drugs and new combinations are assessed in clinical trials . 
 in recent years , there has been interest in the potential for immunomodulatory drugs ( eg , lenalidomide ) and bortezomib to slow osteolytic bone destruction in multiple myeloma through inhibition of osteoclast activity , ( eg , bortezomib ) .2630 so far , these data are derived from preclinical clinical assessments of biochemical markers of bone resorption and bone mineral density and have not yet been correlated with a reduction in the risk of skeletal - related events . 
there is no evidence to suggest that antimyeloma treatment alone can replace bisphosphonates for treatment of multiple myeloma bone disease ; however , the potential for synergistic and between bisphosphonates is intriguing . 
on the basis of the data this study , for skeletal - related events obtained studies and osteoblast increased activity e ects drugs these and 750 vol 12 august 2011 articles zoledronic acid is very likely to provide clinically in combination with newer signi cant bene ts antimyeloma regimens because it has proved bene cial in the prevention of skeletal - related events in patients with solid tumours who were given a broad range of primary anticancer treatments.21 , 31 , 32 however , clinical studies are needed to con rm this theory . 
 the myeloma ix study is the rst large , independent clinical trial in patients with newly diagnosed multiple myeloma , and its results show unequivocal superiority of one bisphosphonate over another for reduction of the risk of skeletal - related events . 
overall , the data from this study support the early use of zoledronic acid for reduction in the risk of skeletal - related events in all patients with newly diagnosed multiple myeloma . contributors gjm , jac , and ghj were chief investigators . 
gjm , jac , wmg , kc , seb , ajs , nn - c , and pw contributed to writing the report , generation of tables and gures , or data interpretation . 
gjm developed an early draft , and all authors contributed to the review and amendments and approved the submitted report . con icts of interest gjm has participated on advisory boards for , received payment for lectures and development of educational presentations from , and received travel support from celgene , novartis , merck , and johnson and johnson . 
gc has received speakers fees from celgene and janssen - cilag , payment for the development of educational presentations from celgene , acted as a consultant for celgene , janssen - cilag , and novartis , and received travel support to attend meetings from celgene and janssen - cilag . 
 fed has participated on advisory boards and spoken at meetings for celgene , ortho biotech , and novartis , and has received travel support to attend meetings from celgene and ortho biotech . 
we thank all the patients , investigators , and sta who participated in the mrc myeloma ix trial ; sta at the clinical trials research unit , university of leeds , leeds , uk , for trial coordination and data management ; sta at the department of immunology , university of birmingham , birmingham , uk ; sta at wessex regional genetics laboratory , university of southampton , southampton , uk ; sta at haematological malignancy diagnostic service , leeds teaching hospitals nhs trust , leeds , uk ; sta at institute of cancer research , london , uk , for central laboratory investigations ; david bowen for independent safety oversight ; the mrc leukaemia data monitoring and ethics committee ; the mrc leukaemia trial steering committee ; the national cancer research institute haematological oncology clinical studies group ; myeloma uk ; the national institute for health research for support , through the national cancer research network ; the support of biomedical research centre at the royal marsden hospital ; lead investigators , as previously reported ; 12 and michael hobert ( proed communications , beachwood , oh , usa ) , for his medical editorial assistance with this report . 
 editorial for more on national cancer survivors day see ncsd.org / for more on the us national coalition for cancer survivorship see canceradvocacy.org for more on the profiles registry see pro lesregistry.nl cancer survivors : still room for improvement june 5 marked the 24th annual national cancer survivors day , with events hosted in 19 countries to raise awareness of issues a ecting cancer survivors , and to show that life after a diagnosis of cancer can be meaningful and productive . 
as the number of individuals diagnosed with cancer increases , and progress is made in successfully treating the disease , the population of cancer survivorsde ned by the us national coalition for cancer survivorship as any individual with cancer , from the time of diagnosis through the remainder of their lifewill inevitably swell . 
for instance , over 2 million people in the uk are currently living with the consequences of cancer and its treatment , and this gure is projected to grow at more than 3% per year . 
 and the e ects of cancer are not limited to the acute phase of disease ; according to a macmillan cancer support survey of over 4500 peoplea quarter of whom had rst been a ected by cancer more than 10 years previouslycancer survivors report poorer health than the general population . 
with the focus of healthcare professionals largely on treating the disease itself , is enough e ort being invested in individuals post - treatment ? survivors are often a ected by physical complicationseg , pain , sexual dysfunction , and nerve damageand emotional problemseg , depression , anxiety , and memory loss . 
while the raising practical and nancial emotional and physical burdens are highest in the rst year of treatment , another macmillan survey suggested that , 10 years after the end of treatment , as many as 54% of survivors are still a ected by emotional problems and 71% had been a ected by physical conditions related to their cancer and its treatment in the previous 12 months . 
such late e ects are particularly of concern with survivors of childhood cancer , with aggressive treatment protocols aimed at curing disease also running the risk of serious premature cardiovascular disease and second cancers later in life . 
 its own right , whilst childhood cancer survivors are often closely monitored in the longer termperhaps as a result of the fewer number of patients , and their treatment in specialist centresthe scenario for adults is less organised . 
little is known of the exact incidence and prevalence of many of the late side - e ects that could a ect a cancer survivor , nor what risk factors might be at play . 
a number of initiatives are underway to help address this knowledge gap ; for example , the dutch patient reported outcomes following initial treatment and long term evaluation of survivorship ( profiles ) registry is a growing population - based cohort following both short and longer term cancer survivors which aims to better understand the physical and psychosocial care needs of cancer survivors and to identify patients at high risk for poor physical and mental health outcomes . 
 until such time as the natural history of these complications is better understood , long - term care must focus on management of symptoms and means to prevent chronic disease . 
education is of paramount importancedata suggest that almost half of cancer survivors were not aware of long - term physical sidee ects , and less than a fth of survivors a ected by late symptoms had sought medical help . 
whilst long - term side - e ects are likely to be discussed while making treatment choices , perhaps the best time to reinforce this message is at the end of treatment , with key signs and symptoms outlined , and advice given on who to contact should the need arise . 
the example set by follow - up mechanisms in screening programmes could perhaps be adapted , with missed visits agged for attention , perhaps at the primary - care level , given that most survivors will present with late symptoms to their family doctor . 
 although often criticisedlargely on privacy and security groundscomprehensive individual electronic medical records , with information collated from the multiple specialty units that will have interacted with a patient along the treatment pathway , would ensure that the relevant information would be made available in a systematic manner to primary - care givers so that future symptoms can be more readily associated with previous exposures . 
afatinib versus placebo for patients with advanced , metastatic non - small - cell lung cancer after failure of erlotinib , ge tinib , or both , and one or two lines of chemotherapy ( lux - lung 1 ) : a phase 2b / 3 randomised trial . 
lancet oncol 2012 ; 13 : 52838in this article ( published online march 26 ) , the rst sentence of the fourth paragraph on the fourth page should have read we measured progression - free survival from the date of randomisation to disease progression or death , whichever occurred rst . 
we present a pre - planned preliminary safety analysis of side - e ects in stages 1 and 2 of a randomised trial comparing standard and hypo fractionated radiotherapy . methods we did a multicentre , randomised study and recruited men with localised prostate cancer between oct 18 , 2002 , and aug 12 , 2006 , at 11 uk centres . 
patients were randomly assigned in a 1 : 1 : 1 ratio to receive conventional or hypofractionated high - dose intensity - modulated radio therapy , and all were given with 36 months of neoadjuvant androgen suppression . 
this study is registered , number isrctn97182923 . findings 153 men recruited to stages 1 and 2 were randomly assigned to receive conventional treatment of 74 gy , 153 to receive 60 gy , and 151 to receive 57 gy . 
 for bladder toxicities , three ( 22% ; 0562 ) of 138 men , three ( 22% ; 0563 ) of 137 , and none ( 00% ; 975% ci 0026 ) of 143 had scores of grade 2 or worse on the rtog scale at 2 years . interpretation hypofractionated high - dose radiotherapy seems equally well tolerated as conventionally frac tionated treatment at 2 years . funding stage 1 was funded by the academic radiotherapy unit , cancer research uk programme grant ; stage 2 was funded by the department of health and cancer research uk . introduction prostate cancer is the most common cancer in men in the uk , usa , and western europe , with 37 000 men diagnosed in the uk and an estimated 913 000 cases worldwide in 2008.1 after the introduction of prostatespeci c antigen ( psa ) testing , most men diagnosed have localised disease . 
management options include externalbeam radiotherapy , brachytherapy , radical prostatectomy , active surveillance ( for men with low - risk disease ) , and watchful waiting ( for those unsuitable for radical curative treatment )  . 
external - beam radiotherapy might be most appropriate for men with disease features of intermediate or high risk , 2 , 3 and is associated with long - term disease control in most patients.4 about 10 000 men receive radical prostate radiotherapy in the uk every year.5 substantial technological advances over the past decade have improved both the ability to adjust dose distributions to the prostate target and treatment accuracy . 
several phase 3 randomised control trials have shown the bene t of dose escalation , 6 and high - dose conformal radiotherapy with conventional 2 gy daily fractions to a total dose of 74 gy has become the standard of care in the uk.7 additionally , there has been interest in the fraction sensitivity of prostate cancer.810 the ratio for most cancers is believed to be about 10 gy , but for prostate cancer values as low as 15 gy have been suggested , which is smaller than the roughly 3 gy reported for the late reactions of most normal tissues ( including rectum ) .11 these ndings have potentially important therapeutic implications . 
hypofractionated radiotherapy with fewer high - fraction - size treatments would be bene cial for prostate cancer because it would deliver a larger biological - equivalent dose to the tumour than would conventional treatment in 1820 gy fractions , while vol 13 january 2012 articles see online for appendix maintaining a similar or lower incidence of late normal tissue reactions . 
furthermore , improved resource use and patient convenience because of short treatment duration would be important gains . maintenance of few treatment - related side - e ects is of paramount importance , because they increase with dose escalation . 
in previous dose - escalation randomised controlled trials ( with di erences of 810 gy between groups ) , variations in side - e ects of 1015% have been reported.6 meta - analysis showed an odds ratio of 158 for late gastrointestinal toxicity of grade 2 or more , in favour of conventional rather than high - dose radiotherapy.6 we therefore aimed to compare a conventional radiotherapy schedule with hypofractionated schedules in prostate cancer . methods trial design we undertook a multistage , multicentre randomised trial ( conventional or hypofractionated controlled high - dose intensity modulated radiotherapy in prostate cancer ; chhip )  . 
we used a three - arm design to ensure that we would be able to extrapolate an isoe ective dose for a speci c rate of complications ( in a similar way to the large uk breast fractionation trials ) .12 biological doses in the experimental schedules were calculated to be equivalent to those in the conventional schedule ; equivalence was achieved with the assumptions that ratios were 25 gy for the 60 gy group and 15 gy for the 57 gy group.9 all treatment groups received conformal and intensity - modulated radiation techniques . 
 this report is a pre - planned analysis of stages 1 and 2 of this trial , with the object ive of establishing the safety of experimental hypofractionated radiotherapy schedules . patients patients were recruited to stage 1 between oct 18 , 2002 and april 27 , 2005 , at the royal marsden nhs trust ( london , uk ) and clatterbridge centre for oncology nhs foundation trust ( wirral , uk ) ; and to stage 2 between may 4 , 2005 , and aug 12 , 2006 , at 11 uk centres ( see appendix )  . 
men with histologically con rmed t1bt3a n0 m0 prostate cancer , 13 psa concentrations of less than 30 ng / ml , estimated risk of lymph - node involvement less than 30% , 14 and who performance status 0 or 1 were eligible . 
patients were excluded if they had t3 tumours and a gleason score of 8 or more , a life expectancy of less than 10 years , previous pelvic radiotherapy , previous androgen suppression , another active malignancy in the past 5 years ( other than cutaneous basal - cell carcinoma ) , comorbid conditions precluding radical radiotherapy , full anticoagulation treatment , or hip prosthesis . chhip ( cruk / 06 / 016 ) was approved by the london multi - centre research ethics committee ( 04 / mre02 / 10 ) and the local ethics committees of all participating centres . 
the trial was coordinated by the royal marsden hospital bob champion unit ( sutton , uk ) and the institute of cancer research clinical trials and statistics unit ( icr - ctsu ; sutton , uk ) , in which central statistical monitoring and all analyses were done . 
both committees approved reporting of this pre - planned analysis of side - e ect data to 2 years from patients recruited in stages 1 and 2 . randomisation and masking men were registered in the trial before or after starting initial hormone therapy . 
treatment allocation was not masked and , because of the trials size , assessors could not be blinded to toxicity or clinical assessments . treatment as part of standard treatment , men received short - course androgen suppression for 36 months before and during radiotherapy , although it was optional for men with low - risk disease . 
injections of a luteinising - hormonereleasing hormone ( lhrh ) analogue every month , combined with initial antiandrogen to reduce testosterone are , or an antiandrogen alone , were allowed . individuals in the control group received prostate radiotherapy with standard 2 gy daily fractions ( monday to friday treatment ) for 74 weeks to give a total dose of 74 gy in 37 fractions . 
patients in the experimental groups were given hypofractionated treatment with 3 gy daily fractions to a total dose of either 60 gy in 20 fractions in 40 weeks or 57 gy in 19 fractions in 38 weeks . 
a complex forward - planned multisegment technique was developed for the trial.15 target and treatment planning volumes have been previously described.15 treatment was planned and delivered using an integrated simultaneous - boost technique with target volumes designed to give the conventional 74 gy group : a dose of 59 gy ( 80% ) to the prostate and base or all seminal vesicles , with a uniform 10 cm margin ; a dose of 71 gy ( 96% ) to the prostate with a 10 cm margin , except posteriorly where the margin was reduced to 05 cm ; and 74 gy ( 100% ) to the prostate with a margin of 05 cm ( 00 cm posteriorly )  . 
pelvic lymph nodes were not included in the target volumes . for the hypofractionated groups , similar proportions of the prescribed dose ( ie , 60 gy or 57 gy ) were given to vol 13 january 2012 articles for more on the phantom see 457 patients randomised 153 allocated to 74 gy in 37 daily fractions of 2 gy 153 allocated to 60 gy in 20 daily fractions of 3 gy 151 allocated to 57 gy in 19 daily fractions of 3 gy 4 did not receive treatment 1 ineligible 1 technically unsuitable 2 patient choice 6 did not receive treatment 1 ineligible 4 technically unsuitable 1 unknown 3 did not receive treatment 2 ineligible 1 unknown 149 received allocated treatment 148 had planned dose 1 less than planned dose 147 received allocated treatment 147 had planned dose 148 received allocated treatment 148 had planned dose 11 not evaluable for rtog toxicity at 2 years 4 died 1 withdrew consent 5 missing forms 1 missing data 10 not evaluable for rtog toxicity at 2 years 1 died 1 withdrew consent 2 lost to follow - up 4 missing forms 2 missing data 5 not evaluable for rtog toxicity at 2 years 2 died 1 lost to follow - up 2 missing forms 138 evaluable for rtog toxicity at 2 years 132 complete set of follow - up forms 6 missed some assessments 137 evaluable for rtog toxicity at 2 years 134 complete set of follow - up forms 3 missed some assessments 143 evaluable for rtog toxicity at 2 years 138 complete set of follow - up forms 5 missed some assessments figure 1 : trial pro le for chhip stages 1 and 2 a complete set of follow - up forms means that the patient completed 6 , 12 , 18 , and 24 month follow - up forms ; follow - up forms completed after 2 years not included . 
portal imaging was used to verify treatment accuracy , which was to be within 3 m a quality - assurance programme was designed as an integral part of the study . 
before trial entry began , every centre completed a process document that de ned the methods to be used for ct simulation , treatment planning , and veri ed treatment accuracy and dosimetry . 
during the trial , on - site quality - assurance visits measured the accuracy of treatment delivery and dosimetry with a trial - speci c phanto details of target volumes , dose parameters , constraints , and the proforma used to record each patients dose distribution are given in the appendix . assessments staging included psa measurement , standard haematology and biochemistry , lymph - node assessment by pelvic mri or ct , and bone scan for patients investigations at intermediate or high risk.2 , 3 histology was locally assessed with diagnostic transrectal ultrasound - guided biopsies ( or specimens from transurethral resection of the prostate ) and reported with the gleason system . bowel , bladder , and sexual function assessments were made before hormone therapy ( when the patient was already registered for the trial ) ; before radiotherapy ; every week during radiotherapy ; and at weeks ten , 12 , and 18 to assess acute toxicity , with subsequent assessments at 26 weeks and every 6 months for 5 years . 
initial symptoms and radiotherapy side - e ects were graded with the late e ects on normal tissues : subjective / objective / management ( lent / som ) 16 and royal marsden hospital ( rmh ) 17 scoring systems . 
radiotherapy side - e ects were also graded with the radiation therapy oncology group ( rtog ) scoring system.18 statistical analysis stage 1 included 150 patients ( 50 per treatment group ) and was powered ( 878% power ; 0045 one - sided ) with a one - stage fleming - ahern design19 to rule out an upper limit of 25% of patients with rtog grade 2 or worse bladder or bowel complications at 2 years for each experimental group , with an expected rate of 10% in the control group . 
data presented for patients who started radiotherapy ( n = 149 in the 74 gy group , n = 147 in the 60 gy group , and n = 148 in the 57 gy group )  . table 1 : baseline demographic and clinical characteristics and treatment details by allocated treatment group 2 years . 
 the sample size ( stage 1 plus stage 2 ) was set at 450 patients ( 150 per group ) , with a 10% allowance for dropout . analyses of side - e ect data for prevalence were done according to treatment received andwith the exception of com parisons at 18 weeksincluded all available assessments from all patients who received at least one fraction of radiotherapy . 
the 18 week comparison was restricted to assessments done in a period 2 weeks either side of this time to consistently capture the end of the acute toxicity period across treatment groups . for the primary endpoint , only patients with an rtog assessment at 2 years were included in analyses , although we did a sensitivity analysis that included all patients . 
time to rst occurrence of late ( reported on follow - up forms from 6 months after the start of radiotherapy onwards ) side - e ects of di erent grades were compared with the kaplan - meier method used to calculate cumulative proportion of patients that had events by 2 years . 
analyses presented in this report have not been adjusted for strati cation factors , but sensitivity analyses adjusting for risk group showed the results to be robust ( data not shown )  . analyses were based on a database snapshot on april 1 , 2010 , and were done with stata version 112 . 
 this study is registered , number isrctn97182923 . role of the funding source the funding source provided peer - reviewed approval for the trial , but had no other role in study design , collection , analysis , interpretation of data , or writing of the report . 
13 patients received no radiotherapy : four were ineligible at trial entry , ve were shown to be technically unsuitable during the planning process , two patients chose to leave , and two for unknown reasons . 
overall , six patients were ineligible : one had abnormal blood counts , two were receiving warfarin , one had stage t3b disease , one had hip prostheses , and one had a perianal stula ( two ineligible patients did receive radiotherapy )  . 
of the 444 treated patients , all but one received the protocolassigned radiotherapy dose and schedule ; one patient in the 74 gy group stopped treatment after 70 gy because of acute urinary obstruction . median follow - up is 505 months ( iqr 435613 ) ; 426 of 457 patients randomly assigned and 424 of 444 treated have been followed up for at least 2 years . 
 most patients received lhrh analogues and short - term antiandrogens ( table 1 ) , similarly distributed across treatment groups and by risk group of the national comprehensive cancer network . acute bowel and bladder side - e ects , measured with the rtog scale , seemed to peak sooner in the experimental groups than in the control group ( gure 2 ) : at 45 weeks in the hypofractionated groups compared with 78 weeks in the control group . 
of 129 patients in the 74 gy group who were assessed 18 weeks after start of radiotherapy , three ( 23% ) reported bowel side - e ects of rtog grade 2 or worse and nine ( 70% ) had bladder side - e ects of grade 2 or worse . 
grade 3 bladder side - e ects were reported by two patients who received 57 gy , and one patient in the 74 gy group had a grade 4 event . 
no acute grade 3 bowel toxicity was reported . late side - e ect pro les by treatment group as reported on each scoring system are shown in gures 3 and 4 . 
cumulative proportion figures only include events occurring up to 2 years post - radiotherapy and are calculated with the kaplan - meier method . table 2 : total number of events , hazard ratios , and cumulative proportion with events by 2 years for bowel , bladder , and sexual dysfunction endpoints by allocated treatment group rtog toxicity scores at 2 years were available for 138 men given 74 gy , 137 given 60 gy , and 143 given 57 gy . 
none of the estimates of late toxicity suggested a doubling of sidee ects in the experimental groups compared with the standard group and , because the upper con dence limits are all less than 20% , the criteria for rejection of any of the treatment groups on the grounds of safety were not met . 
results from the sensitivity analysis that included all patients suggested that the ndings are robust to missing outcomes ( data not shown )  . vol 13 january 2012 articles 74 gy g1 + 74 gy g2 + 74 gy g3 + 60 gy g1 + 60 gy g2 + 60 gy g3 + 57 gy g1 + 57 gy g2 + 57 gy g3 + time from start of radiotherapy ( months ) number of patients assessable 74 gy 153 60 gy 153 57 gy 151 141 143 141 142 138 145 139 138 138 time from start of radiotherapy ( months ) 74 gy g1 + 74 gy g2 + 74 gy g3 + 74 gy g4 60 gy g1 + 60 gy g2 + 60 gy g3 + 60 gy g4 57 gy g1 + 57 gy g2 + 57 gy g3 + 57 gy g4 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy time from start of radiotherapy ( months ) grade 0 grade 3 grade 1 grade 4 grade 2 figure 5 : lent / som sexual dysfunction toxicity of the three treatment groups by assessment timepoint ( a ) cumulative proportion . 
the cumulative proportion of patients with late rtog bowel toxicity of grade 2 or worse at 2 years was 76% ( 95% ci 43132 ) in the 74 gy group , 69% ( 38125 ) in the 60 gy group , and 48% ( 2397 ) in the 57 gy group ( gure 3 ; table 2 )  . 
 for late rtog bladder toxicity , cumulative proportion values were 35% ( 1581 ) , 90% ( 54151 ) , and 48% ( 2398 ; gure 4 , table 2 )  . 
there were no statistically signi cant di erences in cumulative incidence of sidee ects between the groups . with the rmh symptom score , there was low prevalence of bowel scores of grade 2 or worse before radiotherapy on either of the baseline scores ( ie , before hormone or radiotherapy treatment ; eight of 451 patients )  . 
 at 2 years , eight ( 58% ) of 138 patients given 74 gy had rmh bowel scores of grade 2 or worse , four ( 29% ) of 138 patients given 60 gy , and one ( 07% ) of 143 patients given 57 gy . 
prevalences of bladder scores of grade 2 or worse were similar in the three groups before radiotherapy : 25 ( 172% ) of 145 men given 74 gy , 22 ( 151% ) of 146 given 60 gy , and 21 ( 147% ) of 143 given 57 gy . 
rmh bladder scores of grade 1 or worse were recorded in 61 ( 439% ) of 139 men given 74 gy , 39 ( 283% ) of 138 given 60 gy , and 50 ( 350% ) of 143 given 57 gy . with the lent / som assessment system and the maximum score for each normal tissue , the prevalence of bowel scores of grade 2 or worse before hormone or radiotherapy treatments was 39% ( 17 of 439 patients )  . 
 grade 1 scores or worse were reported in 19 ( 135% ) of 141 patients in the 74 gy group , 16 ( 110% ) of 146 in the 60 gy group , and 15 ( 106% ) of 142 in the 57 gy group at the assessment before radiotherapy . 
the prevalence of bowel symptoms at 2 years was higher in the 74 gy group than in the other two groups , with 31 ( 225% ) of 138 patients in the 74 gy group experiencing grade 1 events , 13 ( 94% ) experiencing grade 2 events , and two ( 14% ) experiencing grade 3 events versus 23 ( 168% ) of 137 men in the 60 gy group experiencing grade 1 events , seven ( 51% ) experi encing grade 2 events , and one ( 07% ) experiencing grade 3 events , and 22 ( 155% ) of 142 men in the 57 gy group experiencing grade 1 events , six ( 42% ) experi encing grade 2 events , and one ( 07% ) experiencing grade 3 events ( p = 0023 )  . 
the 6 , 12 , 18 , and 24 month scores after radiotherapy all showed signi cant to preradiotherapy levels ( p = 00001 for 6 month scores ; p < 00001 for other timepoints )  . increases compared before hormone treatment , 45 ( 188% ) of 239 patients had lent / som grade 1 bladder scores , 61 ( 255% ) had grade 2 scores , and 26 ( 109% ) had grades 3 or 4 . 
as expected , scores deteriorated during neoadjuvant hormone therapy , with 350 ( 835% ) of 419 men recording scores of grade 2 or worse before radiotherapy ( p < 00001 )  . 
partial recovery was reported : scores of grade 2 or worse were reported in 310 ( 754% ) of 411 patients 24 months after radiotherapy treatment ( gure 5 )  . 
lent / som sexual dysfunction scores were not signi cantly di erent in randomised groups at any point ( table 2 )  . discussion this planned interim analysis of stages 1 and 2 of the chhip trial has shown no clinically meaningful di erences in acute toxicity between standard and hypofractionated radiotherapy schedules . 
the safety criteria for stopping were not met and the trial completed accrual in june , 2011 . acute reactions occurred earlier in the hypofractionated groups than in the control group , in which the pattern of acute toxicity was very similar to that reported in the group of men randomised to receive 74 gy in a previous trial.17 however , the cumulative proportion of both bowel and bladder side - e ects at 2 years is lower in the chhip trial than in the 74 gy group in the previous trial ( in which incidence of rtog bowel toxicity of grade 2 or worse was 20% and bladder toxicity of grade 2 or worse was 8% ) .20 this di erence might be a result of patient selection factors ( although age and psa distributions are very similar ) , or of the favourable dose distributions panel : research in context systematic review before the chhip trial began , reports based on retrospective series of patients suggested that the ratio for prostate cancer might be low , 810 but only two small randomised trials ( with relatively low doses of radiotherapy ) existed and neither was large enough to con rm or refute a bene t.31 , 32 since chhip started , reviews33 , 34 of two large patient databases have been done , suggesting that the best estimates for the ratio are 37 gy and 14 gy . 
however , conformal and intensity - modulated radiotherapy improves dose distributions of radiotherapy and conformal radiotherapy reduces side - e ects . interpretation the ndings from this pre - planned safety analysis of the rst 457 patients enrolled in the chhip trial suggest that high - dose hypofractionated schedules using 3 gy fractions and intensity - modulated radiotherapy are safe . 
safety and e cacy data from the full trial is essential to fully assess hypofractionated schedules , but these safety results should enable investigators to safely pursue these avenues of research . 
clinicians and patients should be strongly encouraged to support trials using fractions of 3 gy or more . and adherence to normal tissue dose constraints with the forward - planning or inverse - planning methods used in the chhip trial.15 data from randomised controlled trials have shown that treatment technique , 21 planning target margin , 22 and dose , 2226 can all a ect outcomes of prostate cancer radiotherapy . 
therefore , meaningful assessment of the biological e ects of altered fractionation schedules can be made only by controlling for these other factors . although not included as part of this safety analysis , we have measured patient - reported outcomes with the same instruments as those used in the previous trial.17 this continuing longitudinal quality - of - life substudy that recruited 1958 men will help to establish whether altered fractionation a ects di erent symptom complexes27 and will be analysed and published separately . the choice of treatment in our control group was based on level 1 evidence and a meta - analysis of trials assessing dose escalation6 and the addition of hormonal therapy28 , 29 for men with intermediate - risk and high - risk disease . 
 the dose of 74 gy was preferred to a higher dose because it has become the standard dose in the uk7 after the mrc rt01 trial , 20 which is the largest reported study of dose escalation and the only study to routinely include shortcourse androgen suppression . 
the median duration of androgen suppression of 5 months is roughly what was recommended in the updated trog 96.01 trial that compared radiotherapy alone with the addition of either 3 or 6 months of androgen deprivation.30 the experimental high - dose hypofractionated groups were designed as they were because retrospective data reviews have suggested that the ratio might be low ( panel ) .8 , 10 large multicentre reviews and a metasummary3335 have suggested estimates of 37 gy , 34 and 14 gy.33 however , a 2008 review36 of studies that used altered hypofractionated treatments showed that evidence is insu cient to recommend a change to doses larger than 2 gy per fraction and that results from continuing randomised controlled trials were needed . 
4 week schedules with 3 gy fractions were chosen because there was some data and experience with similar , but lower dose schedules in the uk.37 other investigators of international studies of hypofractionated radiotherapy have also reported favourable toxicity . 
a small italian phase 3 trial38 included 168 men and was designed to establish whether a high - dose hypofractionation schedule ( 62 gy in 31 gy daily fractions ) was associated with lower radiation - related toxicity than was a high - dose conventional schedule ( 80 gy in 2 gy daily fractions )  . 
frequency of side - e ects after 3 years of follow - up and psa control was reported to be at least as good in the hypofractionated cohort as in the control group ( psa control 87% vs 79% , p = 004 ) .38 additionally , reports from phase 1 or 2 trials of high - dose hypofractionated radiotherapy treatments in prostate cancer are encouraging . 
late bowel side - e ects ( rtog grade 2 or worse ) have been reported in 4% , 55% , and 63% and late bladder side - e ects in 42% , 56% , and 43% of men after 25 years of follow - up.3941 a preliminary report37 of a dose - fractionation escalation study in 210 men ( 294 gy in 22 fractions to 43 gy in 12 fractions ) reported rectal bleeding in 88% of patients . 
in a large phase 2 study including 770 men treated with 25 gy fractions to a total of 70 gy in 55 weeks , 42 rates of late grade 2 or worse rectal and bladder toxicity were 45% and 52% . preliminary estimates of psa control rates in these studies3842 are comparable to those in standard fractionation schedules . 
a large single - institute series of 705 men in manchester , uk , is valuable , because it suggests that a schedule of 50 gy in 16 fractions ( 3125 gy per fraction ) was equivalent to a contem poraneously treated series with 6570 gy in 1820 gy fractions.43 previously reported randomised controlled trials of hypofractionation have used only modest radiation doses by present standards . 
results show a 7% reduction in psa control rate ( 5295% vs 5995% ) in the 20 fraction group with hr for failure of 118 ( 95% ci 099141 )  . 
after median follow - up of 44 months , 4 year psa control rates were alike ( 862% for hypofractionation vs 854% for standard fractionation ) ; rectal bleeding was more frequent in the hypofractionated group ( appendix )  . 
all these studies are compatible with an ratio for prostate cancer of 1530 gy.44 other phase 3 randomised controlled trials are underway : in canada , investigators are comparing 60 gy in 20 fractions with 78 gy in 39 fractions in a planned cohort of 1204 patients ( isrctn 43853433 ) ; and in the netherlands , researchers are comparing 646 gy in 19 fractions with 78 gy in 39 fractions , with a planned cohort of 800 patients ( isrctn 85138529 )  . 
after a pilot study , a scandinavian collaborative group is comparing increased hypofractionation with 427 gy in seven fractions given in 1519 days with 78 gy in 39 fractions in 78 weeks in a group of 592 men ( isrctn 45905321 )  . 
 the combination of studies should clearly de ne the clinical role of hypofractionation for prostate cancer and the fractionation sensitivity of both prostate cancer and normal tissues with improved precision . analyses in our study were not powered for formal comparisons and 84% of patients were from two sites , although the trial occurred in 11 centres overall . 
stage 3 of this trial aims to show non - inferiority of biochemical psa control between experimental and control groups and includes an additional 2759 patients recruited from 41 centres , and will provide an opportunity to validate the ndings presented here . 
planned associated translational research includes comparative dose - volume histograms and side - e ect analysis for the hypofractionated groups , collection of germline dna for radiogenomics , 45 and tissue microarray assessment of predictive factors for fraction sensitivity . contributors dd was the chief investigator and was involved with study design , recruitment of patients , data interpretation , and writing of the report . 
 ah , vk , rh , db , ag , pk , mr , js , hp , csc , and cp contributed to trial design , patient recruitment , data collection , follow - up , and reviewed the report . 
eh was responsible for central management of the trial at icr - ctsu and for all statistical analyses , is a member of the trial steering committee , and was involved in data interpretation and writing of the report . con icts of interest we declare that we have no con icts of interest . acknowledgments stage 1 of this study was supported by the academic radiotherapy units cancer research uk programme grant ( sp2312 / 021 ) , and stage 2 was additionally supported by the department of health . 
central trial management costs during follow - up and statistical analyses were supported by cancer research uk ( grant number c8262 / a7253 , trial reference number cruk / 06 / 016 ) , with quality assurance from the department of health . 
 recognition goes to all the trials unit sta at bob champion unit and at icr - ctsu , sutton , uk , who contributed to the central coordination of the trial . 
we would also like to thank the trial management group , independent data monitoring and trial steering committees ( appendix ) for overseeing the trial . editorial for the ntps 12th report on carcinogens see niehs.nih.gov / ntp / roc / twelfth / pro les / formaldehyde.pdf for the acc letter see policy / regulatory - reform / acc - letter - to - house - sciencecommittee - regarding - jointhearing - on - the - report - oncarcinogens.pdf for the addendum to the ntps 12th report see nih.gov / ntp / roc / twelfth / addendum.pdf for the iarc monograph on carginogens see iarc.fr / en / publications / pdfsonline / monographs / index.php for more on who and unicefs consultation see comment lancet 2012 ; 380 : 1214 carcinogenicity assessments : who decides ? a column in the new york times in september , 2012 , drew attention to an attempt by the american chemistry council ( acc ) , a body representing the interests of the chemical industry in the usa , to put funding for the national toxicology programs ( ntp ) 13th report on carcinogens on hold . 
the acc wrote a letter to congress in april , 2012 , contesting the change of listing in the 12th version of the report about formaldehyde , which is widely used in manufactured products , from reasonably anticipated to be a human carcinogen to known to be a human carcinogen , citing inconsistencies between various bodies in their methods of carcinogen reporting . 
 they state that some aspects of a similar classi cation by an environmental protection ag ency ( epa ) report was not found to be scienti cally justi ed by a government commissioned review . 
 this justi cation , based on inter - departmental incon sistencies , raises a wider question about the duplication of work by di erent organisations and who the reporting bodies should be accountable to . in their letter , the acc describe awed science and duplicative procedures that they claim lead to confusing messages . 
the epa report that listed formaldehyde as a carcinogen was reviewed by a panel from the national academy of sciences who , according to the acc , found that the epa had not justi ed its conclusion that formaldehyde causes leukaemia . 
the ntps 12th report has an addendum acknowledging the review , but state that the national academy had not been tasked to do an independent hazard assessment and their ndings had restricted applicability to the 13th report on carcinogens . 
in september , 2012 , 76 occupational and health scientists wrote a letter to congress to point out that whos international agency for research into cancer ( iarc ) monograph on carcinogens also describes formaldehyde as a human carcinogen , thus supporting the epa and ntp reports . 
the acc expresses concerns about the redundancy in a system that they claim has overlapping reporting of substances ( with di erent assessment methods ) between the ntp , epa , centers for disease control and prevention , and agency for toxic substances and disease registryall of which are under the control of di erent federal agencies . 
any methodological or report discrepancies can be exploited by lobbyists like the acc and because these agencies are all housed within us government agencies , they are vulnerable to lobbying organisations who can garner political in uence , in this case , to suppress fundings . the amount of duplicative reporting in the usa can be ampli ed across the world . 
although carcinogen research should certainly be undertaken by di erent institutions around the world , the review of carcinogen status only really needs to be done by a single international organisation with standardised , robust methods . 
 it is notable that the 76 scienti c experts supporting the epa and ntp reports emphasised the iarc monograph on carcinogens as de nitive evidence that the ntps report is scienti cally robust and in accordance with global authoritative bodies . 
this comes at a time when who is reforming itself to better de ne its role in the world and is actively engaging with the global community to shape its future through a consultation process . 
perhaps global responsibility for carcinogen reporting should be ceded to iarc , under a revised remit for who , and then government policy on cancer risk from substances can focus on how to safeguard health and not whether the method of the assessment was sound . 
combining , rather than duplicating , scienti c e orts in an environment independent from policy and industry lobbyists , should be a future aspiration in which who could take a central and leading role . 
here , we report long - term results of this trial . methods women with completely locally excised dcis were recruited into a randomised 22 factorial trial of radiotherapy , tamoxifen , or both . 
the recommended dose for radiation was 50 gy in 25 fractions over 5 weeks ( 2 gy per day on weekdays ) , and tamoxifen was prescribed at a dose of 20 mg daily for 5 years . 
this study is registered , number isrctn99513870 . findings between may , 1990 , and august , 1998 , 1701 women were randomly assigned to radiotherapy and tamoxifen , radiotherapy alone , tamoxifen alone , or to no adjuvant treatment . 
after a median follow - up of 127 years ( iqr 109147 ) , 376 ( 163 invasive [ 122 ipsilateral vs 39 contralateral ] , 197 dcis [ 174 ipsilateral vs 17 contralateral ] , and 16 of unknown invasiveness or laterality ) breast cancers were diagnosed . 
radiotherapy reduced the incidence of all new breast events ( hazard ratio [ hr ] 041 , 95% ci 030056 ; p < 00001 ) , reducing the incidence of ipsilateral invasive disease ( 032 , 019056 ; p < 00001 ) as well as ipsilateral dcis ( 038 , 022063 ; p < 00001 ) , but having no e ect on contralateral breast cancer ( 084 , 045158 ; p = 06 )  . 
tamoxifen reduced the incidence of all new breast events ( hr 071 , 95% ci 058088 ; p = 0002 ) , reducing recurrent ipsilateral dcis ( 070 , 051086 ; p = 003 ) and contralateral tumours ( 044 , 025077 ; p = 0005 ) , but having no e ect on ipsilateral invasive disease ( 095 , 066138 ; p = 08 )  . 
no data on adverse events except cause of death were collected for this trial . interpretation this updated analysis con rms the long - term bene cial e ect of radiotherapy and reports a bene t for tamoxifen in reducing local and contralateral new breast events for women with dcis treated by complete local excision . funding cancer research uk and the australian national health and medical research council . in situ ( dcis ) introduction ductal carcinoma is usually an asymptomatic disorder that is characterised by a clonal proliferation of epithelial cells con ned within the lumen of mammary ducts.1 , 2 screening has led to a substantial increase in the incidence of dcis over the past two decades ; the disorder represents 10% of all breast carcinomas and around 20% of screen - detected cancers.35 for dcis management options include surgery , radiotherapy , and hormonal therapy.6 the e ectiveness of radiotherapy in reducing recurrences has been examined in four clinical trials.711 in all these studies , radiotherapy reduced in - situ or invasive recurrences by about 50% . 
after just over 6 years of follow - up , a signi cant reduction in all new breast events was reported in the tamoxifen group compared with the placebo group ( rate ratio 063 , 95% ci 047083 ; p = 00009 )  . 
tamoxifen was weakly associated with a reduction in all new breast events compared with no tamoxifen ( hr 083 , 95% ci 064106 ) , but this was because of a reduction in all dcis ( 068 , 049096 ) ; no reduction in invasive cancer was reported ( 111 , 076163 )  . 
patients with lobular carcinoma in situ , atypical ductal hyperplasia in the absence of dcis , pagets disease of the nipple , and those in whom pathological margins of the disease were uncertain were life excluded , as were patients with a reduced expectancy . patients were included if their lesion or lesions could be completely excised , which was con rmed by radiology of the surgical specimen and free margins on histological examination . 
if dcis extended to the margin of the vol 12 january 2011 tamoxifen ( n / n ) no tamoxifen ( n / n ) hr ( 95% ci ) articles patients who did not receive radiotherapy 46 / 794 60 / 794 51 / 782 84 / 782 109 / 794 140 / 782 ipsilateral invasive dcis contralateral invasive dcis 6 / 794 2 / 794 20 / 782 9 / 782 8 / 794 29 / 782 all recurrences 122 / 794 171 / 782 patients who received radiotherapy ipsilateral invasive dcis contralateral invasive dcis 10 / 794 10 / 794 9 / 782 13 / 782 20 / 794 22 / 782 6 / 794 2 / 794 9 / 794 5 / 782 2 / 782 9 / 782 all recurrences 29 / 794 33 / 782 favours tamoxifen favours no tamoxifen figure 3 : forest plot for new breast events in the tamoxifen comparison strati ed by whether or not patients received radiotherapy hr = hazard ratio . 
the size of lesion , pathological type of disease , and if re - excision was done was recorded , and an estimate of the maximum diameter of the total lesion was made . 
 on an individual basis , surgeons in discussion with each patient decided whether to enter the patient into the fourway 22 randomisation , or one of two separate two - way randomisations with elective choice for the other treatment modality . patients were given information that described the disease , treatment options , and trial design . 
ethics approval was obtained from local ethics committees at all participating hospitals . randomisation and masking randomisation was done in one of three central trials o ces by fax or telephone contact . 
the their own centres each prepared central trial 089 ( 059133 ) 071 ( 051099 ) 077 ( 059098 ) 029 ( 012073 ) 022 ( 005101 ) 027 ( 012059 ) 071 ( 057087 ) 141 ( 054370 ) 068 ( 029159 ) 093 ( 050175 ) 118 ( 036387 ) 099 ( 014704 ) 099 ( 039249 ) 099 ( 061159 ) randomisation lists using a common algorithm , and these lists were available only to trial sta who were trained in the randomisation procedure . 
 procedures the recommended dose for radiotherapy was 50 gy in 25 fractions over 5 weeks ( 2 gy per day on weekdays ; tumour dose fractionation 82 ) at the isocentre or at the point of intersection of the two tangential elds . 
 tamoxifen was prescribed at a dose of 20 mg daily for 5 years . yearly bilateral mammography was recommended for the rst 7 years after treatment and every 2 years thereafter . 
dates and sites of histologically con rmed local new breast events ( dcis or invasive cancer ) , diagnosis of any new non - breast malignant disease , and causes of death were recorded . 
patients in the uk who were lost to follow - up were registered with the o ce for national statistics ( now the nhs information centre ) to nd out details of death ( date and cause ) and cancer registrations ( date of registration )  . the endpoints of primary interest were invasive ipsilateral new breast events for radiotherapy and any new breast event , including contralateral disease and dcis for tamoxifen . 
 no data on adverse events were routinely collected , except for cause of death . statistical analysis to assess the e ects of the two main treatment comparisons , analysis was restricted to patients who were randomly assigned to each main treatment comparison . 
all analyses were strati ed according to whether or not patients received the alternate treatment , and whether this was by choice or as a result of random treatment allocation . 
only the rst new breast event was recorded ; thus , for example , a distant new breast event that occurred after a local new breast event was not available for analysis . from analyses were by intention to treat . 
after randomisation , seven patients were excluded from the vol 12 january 2011 analysis because of protocol violations ; two patients had previous malignant disease , four patients underwent mastectomy before randomisation , and one patient had invasive cancer rather than dcis . 
thus , 1694 patients were eligible for analysis ( gure 1 )  . radiotherapy ( n / n ) no radiotherapy ( n / n ) hr ( 95% ci ) articles patients who did not receive tamoxifen ipsilateral invasive dcis contralateral invasive dcis ipsilateral invasive dcis contralateral invasive dcis 9 / 522 12 / 522 21 / 522 5 / 522 2 / 522 9 / 522 10 / 522 9 / 522 19 / 522 6 / 522 2 / 522 9 / 522 all recurrences 32 / 522 patients who received tamoxifen 28 / 508 29 / 508 59 / 508 7 / 508 6 / 508 13 / 508 72 / 508 22 / 508 22 / 508 46 / 508 5 / 508 3 / 508 8 / 508 all recurrences 28 / 522 59 / 508 follow - up was complete up to oct 1 , 2008 , and events after that time are not included in this analysis . 
1363 ( 80% ) of 1694 patients were 5064 years old and 160 ( 9% ) were under 50 years old at randomisation ; these patients had either symptomatic or mammographically detected dcis . 912 patients ( 54% ) chose to enter the 22 randomisation ( gure 1 )  . 
782 patients chose the two - way randomisation : 664 patients ( 39% ) were randomly assigned to receive tamoxifen or not , of whom 603 elected not to receive radiotherapy and 61 received elective radiotherapy ; 118 patients ( 7% ) were randomly assigned to receive radiotherapy or not , of whom 29 elected not to receive tamoxifen and 89 received elective tamoxifen . 376 ( 222% ) women had new breast events during the follow - up period ( table 1 ) : 197 ( 12% ) patients had ductal carcinoma in situ ( dcis ) , 163 ( 10% ) had invasive cancers , and the type of new breast events was unknown in 16 ( 1% )  . in total , 1576 patients were randomly assigned to receive tamoxifen or not ( gure 1 )  . 
fewer new breast events occurred in the patients randomly assigned to receive tamoxifen than in those who did not receive the drug ( p = 0002 ; table 2 ; gure 2 )  . 
 there was a signi cant reduction in all contralateral events in those randomly assigned to tamoxifen compared with tamoxifen those assigned ( p = 0005 ; table 2 ) , with an absolute 10 - year reduction of 23% . 
tamoxifen was associated with a reduction in the incidence of contralateral invasive events and there was weak evidence of a reduction in incidence of dcis ( table 2 )  . 
overall , an absolute 10 - year reduction of 65% for all new breast events was achieved with the use of tamoxifen . to no women who were randomly assigned to tamoxifen but who were not treated with radiotherapy had a signi cant overall reduction in new breast events ( p = 0001 ) , whereas 024 ( 011055 ) 041 ( 021081 ) 031 ( 018052 ) 071 ( 022223 ) 033 ( 010161 ) 068 ( 029159 ) 041 ( 030057 ) 044 ( 021093 ) 035 ( 016078 ) 037 ( 022064 ) 117 ( 036384 ) 066 ( 011396 ) 110 ( 043286 ) 044 ( 032060 ) favours radiotherapy favours no radiotherapy figure 5 : forest plot for new breast events in the radiotherapy comparison strati ed by whether or not patients received tamoxifen hr = hazard ratio . 
overall , those randomised to radiotherapy had fewer new breast events than did those not randomised to radiotherapy ( p < 00001 ; table 3 ; gure 4 ) , with an absolute reduction of 126% . 
radiotherapy signi cantly reduced all ipsilateral events ( p < 00001 ) whereas no e ect of radiotherapy was reported in relation to contralateral events ( p = 06 )  . 
in both patients who received tamoxifen and those who did not , a signi cant reduction in new breast events was reported with radiotherapy ( table 3 ; gure 5 )  . 
 in an analysis restricted to patients in the factorial randomisation , the combination treatment signi cantly reduced new breast events compared with no adjuvant treatment ( p < 00001 )  . 
tamoxifen plus radiotherapy signi cantly reduced all ipsilateral new breast events ( p < 00001 ) but had no e ect on contralateral new breast events ( p = 02 ; webappendix p 1 )  . 
patients randomised to radiotherapy and tamoxifen had signi cantly reduced ipsilateral new breast events compared with those randomised to tamoxifen alone ( p < 00001 ) but not contralateral new breast events ( p = 05 ; webappendix p 3 )  . 
 randomly assigned tumour blocks were not collected at trial entry , but diagnostic slides have now been collected retrospectively and centrally reviewed for 1224 of the 1694 patients , 16 which suggested that high grade , large size , and young age were signi cant predictors of a high recurrence rate.16 table 4 shows details of potential treatment interactions with age and tumour grade . 
no clear e ect of age was seen on tamoxifen e cacy , whereas radiotherapy was more e ective in women over 50 years old than in those under 50 years old . 179 women had died after a median of 127 years of follow - up ( table 5 )  . 
overall , there was no signi cant di erence in the death rate across treatment groups , but an increase cardiovascular deaths was reported in those randomised to radiotherapy , with or without tamoxifen ( p = 0008 ) , although the numbers were small . 
the clinically most relevant endpoints are invasive ipsilateral new breast events for radiotherapy because it is a local therapy , and all breast events for tamoxifen because it is a systemic therapy . 
 in our rst report , 10 there was no signi cant reduction in new breast events with tamoxifen ; however , in this longterm follow - up the reduction in new breast events was signi cant . 
the tamoxifen e ect seemed to be apparent only in patients who did not receive radiotherapy ; however , only 523 patients who received tamoxifen randomisation and a test for interaction between treatments was not signi cant ( data not shown )  . 
an e ect of tamoxifen was seen in irradiated patients in the only other trial that assessed its use in women with dcis.11 radiotherapy were the vol 12 january 2011 articles panel : research in context systematic review this trial was prompted by the introduction of mammographic screening in the uk , which greatly increased the incidence of ductal carcinoma in situ ( dcis )  . 
two overviews of the trials for dcis have been published.13 , 21 interpretation this long - term follow - up study con rms the e ect of radiotherapy on ipsilateral new breast events and reports an e ect of tamoxifen , which was not apparent in the previous analysis . 
this trial emphasises the importance of radiotherapy in high - grade dcis and also suggests a role for tamoxifen primarily for new contralateral disease . only 130 ( 8% ) patients were on hormone - replacement therapy at the time of randomisation . 
of these , 19 ( 292% ) of 65 randomised to tamoxifen developed a new breast event compared with 16 ( 246% ) of 65 who were not on tamoxifen . 
all women received radiotherapy and tamoxifen signi cantly reduced recurrences after just over 6 years of follow - up ( rate ratio 063 , 95% ci 047083 ) , with weak evidence of a reduction in recurrent dcis ( 069 , 046104 ) and a signi cant reduction in invasive breast cancer events ( 057 , 038085 )  . 
the european organisation for research and treatment of cancer ( eortc ) trial17 reported updated results on the use of radiotherapy in dcis in the absence of tamoxifen after a median of 105 years of follow - up . 
 a swedish study18 reported a relative risk of 040 for ipsilateral disease in women who received radiotherapy compared with those not irradiated , corresponding to an absolute 10 - year reduction of 16% . 
 the early breast cancer trialists collaborative group did a meta - analysis of the e ects of radiotherapy on local recurrences and 15 - year survival in women with early invasive breast cancer.22 overall , the recurrence rate ratio was about 03 in women receiving radiotherapy after breast - conserving surgery compared with those not receiving radiotherapy . 
this reduction is again similar to that reported in the present analysis . no signi cant e ects were reported on mortality , either from breast cancer or other causes for either treatment , except for a possible detrimental e ect of radiotherapy on cardiovascular deaths , but the numbers were small and further data are needed . contributors jc , jff , hb , isf , and wdg designed the trial . 
all authors contributed to the interpretation of the data , writing of the manuscript , and approved the nal version . con icts of interest hb has received travel grants from astrazeneca and roche . 
 acknowledgments the dcis trial was partially funded by the cancer research uk programme grant in the uk ( c569 - a10404 ) and the australian national health and medical research council . errata errata lehtinen m , paavonen j , wheeler cm , et al . 
overall e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against grade 3 or greater cervical intraepithelial neoplasia : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 8999in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
cross - protective e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against cervical infection and precancer caused by non - vaccine oncogenic hpv types : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 10010in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
lancet oncol 2012 ; 13 : 1012in this comment ( published online nov 9 , 2011 ) , the last sentence of the sixth paragraph incorrectly lists hpv - 35 as one of the oncogenic hpv types covered by the new nine - type gardasil vaccine ; the list should include hpv - 45 instead . 
this correction has been made to the online version as of jan 3 , 2012 . vol 13 january 2012 comment if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology as piration of mediastinal and hilar lymph nodes should be used to assess preoperative lung cancer status in countries where tuberculosis is endemic.10 finally , hiv infection is associated with increased lung cancer cases . 
can tuberculosis further increase this risk ? in a study11 that linked aids registry surveillance data for 322 675 patients with aids diagnosed between 1977 and 2002 , with cancer registries in 11 us regions , lung cancer risk over 10 years was unrelated to tuberculosis . 
 tuberculosis awareness in patients with cancer needs to be reinforced , especially in low - burden developed countries , and lung cancer awareness in patients with previous or suspected tuberculosis should be urgently strengthened in developing countries to increase the low numbers of potentially resectable tumours . * sandro vento , massimiliano lanzafame department of internal medicine , faculty of medicine and health sciences , university of botswana , gaborone , botswana ( sv ) ; and infectious diseases unit , gb rossi university hospital , verona , italy ( ml ) ventosandro@yahoo.it we declare that we have no con icts of interest . yu yh , liao cc , hsu wh , et al . 
lancet oncol 2011 ; 12 : 37786in this article ( april ) , on page 380 , the number of women with luminal a breast cancer tested for the kras variant should have been 478 in gure 2a and the percentage of premenopausal women diagnosed with luminal a breast cancer should have been 151% in gure 2b . 
lancet oncol 2011 ; 12 : 41516on page 415 , in the second column , it was stated that 17 variants showed moderate to strong evidence of a true association and were therefore candidates for clinical tests , this should have said 14 variants . 
this correction has been made to the online version as of may 18 , 2011 . published online may 18 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70127 - 9 522 vol 12 june 2011 reducing cancer risk in homosexual men increasing use and e cacy of combination antiretroviral treatment has rede ned hiv / aids as a chronic disease and decreased the number of aids - de ning cancers . 
furthermore , research published in cancer on may 9 , 2011 , suggests that men who have sex with men ( msm ) are twice as likely to have cancer than are heterosexual men . 
this statistic underscores two key questions : why is cancer risk so high in msm , and what can be done to reduce the threat ? the cancer study collated responses from 122 354 people ( 51 233 men , including 1493 msm ) , from interviews in california in 2001 , 2003 , and 2005 . 
 msm are more likely to smoke and abuse alcohol , have higher rates of hiv infection and immunosuppression , and have di erent transmission patterns of human papillomavirus ( hpv )  . 
additionally , co - infection plays a part : hiv - infected patients are at increased risk of developing malignancies associated with epstein - barr virus , human herpesvirus 8 , and hepatitis b and c viruses ( hbv and hcv , respectively )  . 
viral transmission is also not helped by increases in msm who serosort ( ie , have sex with a partner of the same perceived hiv serotype ) or seroguess ( ie , msm who estimate their partners hiv infection status based on sexual behaviour ) to have unprotected sex . as a consequence of antiretroviral treatment , nonaidsde ning cancers are now more prevalent than are aidsde ning cancers and prevalence continues to increase in msm . 
hiv - infected patients with cancer have a worse prognosis than do similarly staged non - hiv - infected patients with the same cancer , are more likely to have more advanced disease at presentation , and have a greater rate of recurrence . 
a reluctance to seek early medical help coupled with stereotypical male behaviours on compliance are likely contributing factors , but the underlying tumour biology and milieu might also have a role . 
 vol 12 june 2011 campaigns were common in the mainstream media and had a remarkable e ect on educating the general population , promoting condom use , and reducing risky behaviours , but such e orts have lost momentum in recent years . 
reinvigoration and innovation are needed at the population level and in targeted groups to better educate more recent generations of the dangers of unprotected sex , the wide range of health risks associated with infection , and the importance of smoking cessation and decreased alcohol use . 
the data in the cancer study further support the increasing evidence that suggests vaccinating boys against hpv could lead to substantial health bene ts in the population and might reduce numbers of many cancer types , including those of the head and neck , anus , and penis . 
an australian surveillance study published in the lancet infectious diseases in november , 2010 , showed a decline in the number of genital warts in young heterosexual men who had been vaccinated . 
consequently , if a comprehensive population - based vaccination programme in young boys were to be initiated , wart reduction would be seen in msm too , provided su cient numbers of men were vaccinated to promote herd immunity . although more research is needed to better understand the underlying biological , aetiological , and psychological di erences a ecting cancer prevalence and treatment response in msm , in the short - to - medium term , cancer risk could be reduced by improved education and lifestyle changes . 
 the ndings in cancer not only highlight the needs of a vulnerable group in society , but also act as a timely reminder that many cancers are preventable and , frustratingly , the tools needed for mass eradication available , but woefully underused . 
we aimed to assess the value of her2 and top2a as predictive markers of response to anthracycline - based adjuvant therapy in patients with early breast cancer . methods we did a meta - analysis of individual patient data from ve randomised adjuvant trials that compared anthracycline - based regimens with cyclophosphamide , methotrexate , and uorouracil ( cmf ) regimens . 
we calculated hazard ratios ( hr ) to compare event - free survival ( efs ) and overall survival in patients receiving anthracycline - based treatment with those receiving cmf in two her2 cohorts ( her2 ampli ed and non - ampli ed tumours ) and in three top2a cohorts ( normal , ampli ed , and deleted tumours )  . findings we analysed data for 3452 patients for her2 and 3102 patients for top2a . 
for efs , hrs were 089 ( 95% ci 079101 ) for her2 non - ampli ed patients and 071 ( 058086 ) for her2 - ampli ed patients ( pinteraction = 00485 ) ; for overall survival , hrs were 091 ( 95% ci 079105 ) for her2 non - ampli ed patients and 073 ( 059089 ) for her2 - ampli ed patients ( pinteraction = 00718 )  . 
in analysis of top2a status , hrs for efs were 088 ( 078100 ) for normal , 063 ( 046087 ) for deleted , and 062 ( 043090 ) for ampli ed ( pinteraction = 00513 ) ; hrs for overall survival were 089 ( 078103 ) for normal , 068 ( 049095 ) for deleted , and 067 ( 046098 ) for ampli ed ( pinteraction = 01608 )  . 
 when patients with top2a - deleted and top2a - ampli ed tumours were grouped together ( altered cohort ) and compared with data from patients with normal top2a tumours , hrs for efs were 064 ( 050081 ) for altered and 088 ( 078100 ) for normal ( pinteraction = 00183 ) ; hrs for overall survival were 067 ( 052086 ) for altered and 089 ( 078103 ) for normal ( pinteraction = 00455 )  . interpretation although her2 ampli cation and combined top2a ampli cation and deletion may have some value in the prediction of responsiveness to anthracycline - based chemotherapy , our ndings do not support the use of anthracyclines only in patients with her2 - ampli ed or top2a - aberrated tumours . funding associazione italiana ricerca cancro , academy of finland , belgian federation against cancer , cancer research uk , les amis de linstitut bordet , scottish breast cancer trials group , ncic clinical trials group , canadian cancer society research institute , danish council for strategic research , pharmacia - upjohn ( now p zer ) , and abbott laboratories . from several introduction findings retrospective analyses of randomised trials have suggested that anthracyclinecontaining adjuvant therapy might be bene cial to only those patients with breast cancer who have her2 gene ampli cation or protein overexpression , 14 but this e ect cannot be explained by any biological rationale . 
one of the the topoisomerase ii proteinthe gene for which , top2a , is on chromosome 17q12 - q21.5 other retrospective analyses have suggested that anthracycline - containing adjuvant therapy might be most e ective in patients whose tumours carry ampli ed top2a.68 however , this association was not seen in a study reported in 2008.9 two studies suggested that top2a gene deletion might targets of anthracycline intracellular also confer increased sensitivity to anthracyclines , 10 , 11 although , as with her2 , this e ect cannot be explained by any biological rationale.5 these studies have lent support to the idea of a tailored approach to the use of anthracyclines . 
nevertheless , none of them alone could safely lead to rm conclusions for daily practice , because small study sample sizes have necessitated caution in application to routine care of patients . 
 national laboratories quality control an external laboratory ( laboratory of cancer biology , university of tampere , tampere , finland ) was originally going to do the central assessment of her2 and top2a for all tumour specimens with sections cut from tissue microarrays . 
however , in december , 2006 , the protocol was amended because preliminary data showed suboptimum concordance between results from the external laboratory and those from the four national laboratories that did the assessments for the original studies when the external laboratory tested her2 and top2a on tissue microarray sections . 
testing for both markers at the four national laboratories was done by uorescent in - situ hybridisation ( fish ) , as described in the individual publications.4 , 6 , 911 in the external laboratory , testing was done by fish with three probes for her2 , top2a , and the centromere of chromosome 17 ( abbott laboratories , abbott park , il , usa )  . 
for this analysis , a tumour was de ned as her2 ampli ed or top2a ampli ed if the ratio between her2 or top2a gene copy number and number of copies of chromosome 17 centromere was two or more ; we regarded top2a gene to be deleted if the ratio was 08 or lower and to be top2a normal if the ratio was greater than 08 but lower than two . 
we estimated concordance in her2 and top2a scores between the external and the four national laboratories by calculating the proportion of cases with the same de nition of gene status ( ie , ampli ed or non - ampli ed for her2 , and ampli ed , deleted , or normal for top2a )  . 
 during on - site monitoring visits , local data , sample ow , and fish protocols were collected and veri ed for at least 50 randomly selected patients in each national laboratory . 
 level of compliance to randomised interventions was veri ed for each individual trial . subgroup analysis we prospectively de ned four biologically homogeneous cohorts : ( 1 ) highly hormone - sensitive tumours , de ned as oestrogen - receptor and progesterone - receptor positive ( 10% of immunostained cells ) , her2 non - ampli ed , and grade 12 ; ( 2 ) moderately hormone - sensitive tumours , de ned as oestrogen - receptor positive and progesteronereceptor negative independent of grade and her2 gene status , or oestrogen - receptor and progesterone - receptor positive and grade 3 , or her2 gene ampli ed ; ( 3 ) her2ampli ed tumours which were oestrogen - receptor and progesterone - receptor negative ; and ( 4 ) triple - negative tumours , de ned as oestrogen - receptor and progesteronereceptor negative and her2 non - ampli ed . 
we identi ed these four cohorts on the basis of gene expression signature studies reported in the past decade.17 oestrogenreceptor , progesterone - receptor , and histological grading were assessed at either local pathology units ( piccart and colleagues , 14 ejlersten and colleagues , 15 and poole and colleagues [ neat and br9601 trials ] 16 ) or the national laboratory ( levine and colleagues13 )  . 
 considering this assump tion , we ran the analysis by molecular subgroups twiceie , with and without the data from the neat and br9601 trials.16 the two analyses gave very similar results , so the molecular subgroup analyses include data from the neat and br9601 trials.16 statistical analysis the primary study endpoint was the comparison in terms of efs and overall survival between patients who received anthracycline - based treatment and those who received cmf in the two her2 cohorts ( her2 ampli ed and non - ampli ed tumours ) and in the three top2a cohorts ( top2a normal , ampli ed , and deleted tumours )  . 
in a secondary efs and overall survival analysis , the log - rank test was adjusted by the main prognostic factorspathological tumour size ( 2 cm or > 2 cm ) and number of ipsilateral positive axillary nodes ( node - negative , 13 positive nodes , or 4 positive nodes )  . 
 the test for interaction had two degrees of freedom when patients were divided by top2a status into three cohorts ( ie , normal , ampli ed , or deleted ) and one degree of freedom when patients were allocated in two cohorts ( ie , normal or aberrated )  . 
we used sas version 9.1 and splus version 7 for statistical analyses . role of funding sources the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results 1003 ( 22% ) of 4558 of patients could not be assessed in the meta - analysis because of an absence of data for her2 or top2a gene status ( table 1 )  . 
when efs curves from patients who participated in the meta - analysis were compared with those from patients who did not , within each trial and by treatment group , we recorded no statistically signi cant di erences ( data not shown )  . 
in piccart and colleagues trial , 14 top2a gene status was assessed only within the her2 ampli ed cohort , which might explain why the rate of top2a gene ampli cation is more than double than that in the other trials . 
likewise , the high proportion of her2 gene ampli cation reported in the ejlertsen and colleagues trial15 might be explained by most patients having oestrogen - receptor - negative disease . 
 the bene t of treatment with anthracyclines over treatment with cmf was greater for individuals with her2 gene ampli cation than it was for individuals without her2 gene ampli cation when analysing efs ( pinteraction = 00485 ) , but not when analysing overall survival ( pinteraction = 00718 ; gure 1 and gure 2 )  . 
we recorded no signi cant di erence in the bene t of treatment with anthracyclines over treatment with cmf when assessing the three separate top2a cohorts in terms of either efs ( pinteraction = 00513 ) or overall survival ( pinteraction = 01608 ; 1138 vol 12 november 2011 articles hazard ratio ( 95% ci ) 139 ( 075257 ) 099 ( 063155 ) 176 ( 048642 ) 070 ( 033149 ) 123 ( 080188 ) 111 ( 087143 ) 122 ( 076196 ) 067 ( 047095 ) 177 ( 032969 ) 061 ( 031123 ) 090 ( 063127 ) 084 ( 069103 ) 043 ( 012147 ) 068 ( 030155 ) 068 ( 040114 ) 086 ( 035211 ) 076 ( 042139 ) 070 ( 051096 ) 134 ( 050362 ) 094 ( 050176 ) 072 ( 040131 ) 037 ( 015090 ) 089 ( 060131 ) 082 ( 063107 ) gure 1 and gure 2 )  . 
however , when top2a ampli cations and deletions were combined ( altered cohort ) , we recorded a signi cant di erence in the bene t of treatment with anthracyclines over treatment with cmf between patients with normal top2a status and those with altered top2a status when analysing both efs ( pinteraction = 00183 ) and overall survival ( pinteraction = 00455 ; gure 1 and gure 2 )  . 
 for when adjusted according to the main prognostic factors ( ie , pathological tumour size and number of positive the e ect of ipsilateral axillary nodes ) , hrs anthracyclines versus cmf in patients with her2 gene ampli cation were 070 ( 95% ci 057085 ; p = 00004 ) for efs and 073 ( 059090 ; p = 0003 ) for overall survival , and , for patients without her2 gene ampli cation , were 085 ( 075096 ; p = 0012 ) for efs and 087 ( 075101 ; p = 0061 ) for overall survival . 
after adjustment , the bene t of treatment with anthracyclines over treatment with cmf was not statistically di erent between individuals with her2 ampli cation and those without her2 ampli cation in either efs ( pinteraction = 010 ) or overall survival ( pinteraction = 017 )  . 
 for top2a , adjusted hrs were 062 ( 042092 ; p = 0019 ) for efs and 068 ( 045102 ; p = 0060 ) for overall survival for patients with top2a ampli cation , 057 ( 041081 ; p = 0002 ) for efs and 064 ( 045092 ; p = 0016 ) for overall survival for patients with top2a deletion , and 086 ( 076098 ; p = 0024 ) for efs and 087 ( 075 100 ; p = 0057 ) for overall survival for patients with top2a normal . 
after adjustment , the bene t of treatment with anthracyclines over treatment with cmf di ered signi cantly between the three groups in terms of efs ( pinteraction = 004 ) but not in overall survival ( pinteraction = 019 )  . 
when top2a ampli cations and deletions were combined , adjusted hrs were 060 ( 047077 ; p = 00001 ) for efs and 063 ( 048082 ; p = 00005 ) for overall survival in patients with top2a alterations , and 086 ( 076098 ; p = 0024 ) for efs and 087 ( 075100 ; p = 0056 ) for overall survival in patients with top2a - normal tumours . 
the bene t of treatment with anthracyclines over treatment with cmf di ered signi cantly between the two groups in terms of both efs ( pinteraction = 0013 ) and overall survival ( pinteraction = 0033 )  . of 2588 patients with data that could be assessed , 740 ( 29% ) were de ned as highly hormone - sensitive , 878 ( 34% ) as moderately hormone - sensitive , 311 ( 12% ) as her2 ampli ed and oestrogen - receptor and progesterone - receptor negative , and 659 ( 25% ) as triple negative ( gure 3 and gure 4 )  . 
we recorded no signi cant di erence treatment e ect of anthracyclines or cmf between molecular subgroups , but individuals with her2 - ampli ed tumours seemed to respond better to anthracyclines and those with highly hormone - sensitive tumours seemed to respond better to cmf ( gure 3 )  . 
we compared treatment groups by top2a gene status within the her2 positive molecular subgroup , and , in all three cohorts , anthracycline - based therapy seemed to be more e ective than cmf ( webappendix p 2 )  . 
 discussion our ndings show a greater bene t from anthracyclinebased adjuvant therapy in patients with her2 gene ampli cation than in patients without such ampli cation and in patients with top2a gene alterations than in patients with normal top2a status . 
however , our study also shows that patients with her2 non - ampli ed or top2a normal tumours might have some additional bene t from treatment with anthracyclines , which than a qualitative suggests a quantitative rather interaction between anthracycline activity and her2 or top2a status . 
 this meta - analysis we trials with di erences in the type of anthracycline - based regimens or in the cmf schedules used ( webappendix p 1 ) , which included vol 12 november 2011 1139 articles patients events risk group anthracycline - based patients events risk group anthracycline - based number at risk anthracycline - based year year patients events risk group anthracycline - based patients events risk group anthracycline - based number at risk anthracycline - based year year figure 4 : event - free survival analysis , by molecular subgroups survival in patients with ( a ) highly hormone - sensitive tumours , ( b ) moderately hormone - sensitive tumours , ( c ) her2 - ampli ed tumours , and ( d ) triple - negative tumours . is a potential limitation in the interpretation of the study results , although we recorded similar associations in the interaction between the activity of treatments and her2 or top2a status in each individual trial . 
 two pooled analyses of previously published data have investigated her2 , but not top2a , in the same setting with similar results.18 , 19 neither of these studies did an external quality control substudy for the testing of her2 or top2a . 
our study design chose the external laboratory as the gold standard , but because tumour samples assessed in the external laboratory were not tested in another laboratory , and because samples from the four national laboratories were not cross - compared , we cannot identify the reason behind the recorded discordance . 
in view of the retrospective nature of this assessment and the restricted sample size , the results of this subgroup analysis have to be regarded as merely hypothesis - generating and should not lead to changes in clinical practice . 
this analysis , prompted by the known molecular and clinical heterogeneity of breast cancer , 17 suggests that , in contradiction to previously reported studies that analysed the her2 non - ampli ed cohort as a homogeneous group , 14 , 6 , 9 , 10 , 18 , 19 di erential bene t from anthracyclines might exist within the her2 non - ampli ed cohort . 
in our analysis individuals with triple - negative or moderately hormone - sensitive tumours 1140 vol 12 november 2011 articles seemed to respond better to treatment with anthracyclines than to treatment with cmf . 
because all triple - negative tumours and almost 90% of moderately hormone - sensitive tumours from this study did not carry top2a gene ampli cation , other mechanisms of increased sensitivity to anthracycline might exist . 
we de ned triple - negative tumours as such if oestrogen - receptor and progesteronereceptor immunostaining was less than 10% , and not less than 1% as suggested in international guidelines.20 however we regard this discrepancy as irrelevant with regard to the suggested bene t from anthracyclines in patients who do not carry top2a gene ampli cation . 
 triple - negative tumours and moderately hormonesensitive tumours are often characterised by high proliferation rates.2123 proliferation signals can lead to topoisomerase ii protein over - expression independently of top2a gene status.24 , 25 indeed , data reported elsewhere2627 draw attention to the absence of concordance between top2a gene status and protein concentrations within the same tumour . 
ideally , quanti cation of nuclear concentrations of the topoisomerase ii protein ( ie , the active protein isoform ) might be the most appropriate way to investigate its predictive value.28 other biological factors not related to top2a have been investigated as potential markers of sensitivity to anthracyclines . 
among those , polysomy of chromosome 17 , which could be a marker of genomic instability and dna repair dysfunction , might play a part.29 moreover , factors involved in the regulation of the stromatumour interaction or in the immune response against a tumour might also be involved.3032 future studies looking at molecular markers to predict response to anthracyclines will have to take into account the fact that probably only a multifactorial system will predict responsiveness to anthracyclines . in conclusion , our ndings do not justify routine use of her2 and top2a as molecular markers to predict anthracycline activity , because women with non - her2 ampli ed and non - top2a altered tumours seem to derive bene ts from treatment with anthracyclines , and because problems exist with the reproducibility of top2a gene status assessment by fish . contributors adl , jmsb , be , kip , cp , ji , hm , fpom , dc , mjp , and mb had the idea for and designed the study . 
cd , jmsb , be , kip , dl , cp , he , hm , fpom , fc , am , cjt , cs , ls , dc , and mjp provided study materials . con icts of interest adl has a consultancy and advisory role for and has received honoraria from schering - plough . 
kip has a consultancy and advisory role for and has received honoraria from roche , abraxis , astrazeneca , p zer , novartis , and amgen , and has given expert testimony for novartis and astrazeneca . 
the coin trial assessed preplanned treatment holidays in advanced colorectal cancer to achieve this aim . methods coin was a randomised controlled trial in patients with previously untreated advanced colorectal cancer . 
in arm c , patients who had not progressed at their 12 - week scan started a chemotherapy - free interval until evidence of disease progression , when the same treatment was restarted . 
here , we compare arms a and c , with the primary objective of establishing whether overall survival on intermittent therapy was non - inferior to that on continuous therapy , with a prede ned non - inferiority boundary of 1162 . 
 median survival in the itt population ( n = 815 in both groups ) was 158 months ( iqr 94261 ) in arm a and 144 months ( 80247 ) in arm c ( hazard ratio [ hr ] 1084 , 80% ci 10081165 )  . 
preplanned subgroup analyses in the per - protocol population showed that a raised baseline platelet count , de ned as 400 000 per l or higher ( 271 [ 28% ] of 978 patients ) , was associated with poor survival with intermittent chemotherapy : the hr for comparison of arm c and arm a in patients with a normal platelet count was 096 ( 95% ci 080115 , p = 066 ) , versus 154 ( 117203 , p = 00018 ) in patients with a raised platelet count ( p = 00027 for interaction )  . 
in the per - protocol population , more patients on continuous than on intermittent treatment had grade 3 or worse haematological toxic e ects ( 72 [ 15% ] vs 60 [ 12% ] ) , whereas nausea and vomiting were more common on intermittent treatment ( 11 [ 2% ] vs 43 [ 8% ] )  . 
grade 3 or worse peripheral neuropathy ( 126 [ 27% ] vs 25 [ 5% ] ) and hand foot syndrome ( 21 [ 4% ] vs 15 [ 3% ] ) were more frequent on continuous than on intermittent treatment . interpretation although this trial did not show non - inferiority of intermittent compared with continuous chemotherapy for advanced colorectal cancer in terms of overall survival , chemotherapy - free intervals remain a treatment option for some patients with advanced colorectal cancer , o ering reduced time on chemotherapy , reduced cumulative toxic e ects , and improved quality of life . 
 introduction the treatment of advanced colorectal cancer has improved substantially during the past decade with the introduction of new and more e ective drugs and advances in our understanding of the diseases molecular biology . 
strategies that minimise time on treatment , reduce side - e ects , and improve quality of life , while maintaining duration of survival , are highly desirable . before the introduction of irinotecan and oxaliplatin into treatment schedules for advanced colorectal cancer , uorouracil - based chemotherapy was generally continued until unacceptable toxic e ects or disease progression . 
the resultant cumulative sensory neuropathy with oxaliplatin and handfoot syndrome with uoropyrimidines1 adversely a ect quality of life and overall dose intensity because of reduced dosing in subsequent treatment cycles . one potential method to reduce toxic e ects and improve quality of life is to consider alternatives to continuous chemotherapy . 
intermittent therapy given for a restricted period and then restarted , either after a prede ned interval ( prede ned treatment ) or at disease progression ( repeat therapy ) , are such alternatives . 
however , in breast and prostate cancer , intermittent hormones or cytotoxic agents have not reduced median overall survival.24 a previous medical research council ( mrc ) trial , cr06b , assessed 354 patients with advanced colorectal cancer treated with the de gramont ( uorouracil and folinic acid ) schedule , continuous infusional uorouracil , or raltitrexed.5 those with stable or responding disease at 12 weeks were further randomly assigned to continue therapy until progressive disease or to stop , with the option to restart the same chemotherapy at later progression . 
there was no evidence of a di erence in overall survival between the two strategies ( hazard ratio [ hr ] 087 , 95% ci 069109 , p = 023 ) , with the results even slightly favouring intermittent over continuous treatment . 
 although criticised for its small size and failure of randomly assigned patients to restart protocol treatment , this trial gave impetus to the notion of intermit tent therapy in advanced colorectal cancer and set a precedent for combination chemotherapy.6 intermittent trials of further with its cumulative sensory neuropathy , oxaliplatin is an appropriate drug to use in the exploration of intermittent therapy and has been assessed in two trials , optimox - 17 and optimox - 2.8 in optimox - 1 , 7 continuous oxaliplatin and uorouracil were compared with a novel strategy of planned oxaliplatin breaks , but with continuous uorouracil . 
neither trial showed a signi cant reduction in survival with intermittent therapy , although optimox - 2 showed a trend in favour of continuation of uorouracil during oxaliplatin breaks , and has been adopted as the benchmark for standard practice . 
this outcome is despite failure to recruit beyond phase 2 after the licensing of bevacizumab and that the trend in favour of continuous treatment was not statistically signi cant . the phase 3 coin trial ( continuous or intermittent ) was developed to conclusively address this issue . 
the coin trial also assessed the e ect of addition of cetuximab to continuous oxaliplatin and uoro pyrimidine combination chemo therapy ; the results of this comparison are reported in a companion paper.9 methods study design and participants the full protocol can be found on the mrc clinical trials unit website . 
 eligibility included written informed consent , age of at least 18 years , and histologically con rmed adenocarcinoma of the colorectum , inoperable metastatic or locoregional measurable disease ( response evaluation criteria in solid tumors [ recist ] version 1.0 ) , 10 no previous chemotherapy for metastatic disease , who per formance status 02 , and good end - organ function . 
 patients were excluded if they had previous or present malignant disease , uncontrolled medical comorbidity likely to interfere with coin treatment or response assessment , known brain metastases , or previous oxaliplatin exposure . coin was approved by the uk medicines and healthcare regulatory agency in june , 2004 , and southwest multicentre research ethics committee in december , 2004 . 
 approvals for the irish sites were obtained from the irish medicines board in november , 2006 , and st jamess hospital / adelaide & meath hospital , incorporating the national childrens hospital research ethics committee in december , 2006 . 
the trial was coordinated by the mrc clinical trials unit following the principles of international conference on harmonisation good clinical practice guidelines , undertaken with a trial management group , monitored at regular intervals by an independent data monitoring committee , and overseen by an independent trial steering committee . randomisation and masking central telephone randomisation was done by the mrc clinical trials unit , using the method of minimisation with a random element . 
patients were randomly assigned ( 1 : 1 : 1 ) to the control arm ( oxaliplatin plus capecitabine or oxaliplatin plus uorouracil and folinic acid ) chemotherapy ( arm a ) or one of two research arms : continuous chemotherapy plus cetuximab ( arm b ) or intermittent chemotherapy ( arm c ; gure 1 )  . 
treatment allocation was not masked . continuous oxaliplatin - based procedures two chemotherapy oncologists chose between regimens according to local hospital policy or patient the arm a ( n = 815 ) arm c ( n = 815 ) choice of chemotherapy at baseline capecitabine - based fluorouracil - based 536 ( 66% ) 279 ( 34% ) 533 ( 65% ) 282 ( 35% ) 525 ( 64% ) 290 ( 36% ) 523 ( 64% ) 292 ( 36% ) 63 ( 5669 ) 63 ( 5870 ) 74 ( 9% ) 69 ( 8% ) male female median ( years ) 75 years who performance status previous adjuvant chemotherapy none 16 months > 6 months yes ( unspeci ed ) site of primary tumour status of primary tumour resected unresected local recurrence metastases metachronous synchronous liver only liver and others non - liver more than two number of metastatic sites data are n ( % ) or median ( iqr )  . table 1 : baseline characteristics 375 ( 46% ) 378 ( 46% ) 62 ( 8% ) 608 ( 75% ) 36 ( 4% ) 128 ( 16% ) 43 ( 5% ) 445 ( 55% ) 331 ( 41% ) 39 ( 5% ) 249 ( 31% ) 552 ( 68% ) 174 ( 21% ) 436 ( 53% ) 198 ( 24% ) 283 ( 35% ) 326 ( 40% ) 199 ( 24% ) 375 ( 46% ) 378 ( 46% ) 62 ( 8% ) 608 ( 75% ) 36 ( 4% ) 131 ( 16% ) 40 ( 5% ) 419 ( 51% ) 350 ( 43% ) 46 ( 6% ) 241 ( 30% ) 567 ( 70% ) 179 ( 22% ) 430 ( 53% ) 200 ( 25% ) 284 ( 35% ) 329 ( 40% ) 196 ( 24% ) rectum 243 ( 30% ) 252 ( 31% ) preference . 
oxaliplatin plus capecitabine was given as a 3 - weekly regimen of intravenous oxaliplatin 130 mg / m over 2 h followed by oral capecitabine 1000 mg / m twice a day for 2 weeks . 
oxaliplatin plus uorouracil and folinic acid was given as a 2 - weekly regimen of intravenous l - folinic acid 175 mg or d , l - folinic acid 350 mg over 2 h given concurrently with oxaliplatin 85 mg / m over 2 h , followed by intravenous bolus uorouracil 400 mg / m , and nally uorouracil 2400 mg / m infusion over 46 h via an ambulatory pump . in arm a , treatment was continued until recistde ned progressive disease , development of cumulative toxic e ects ( precluding both oxaliplatin and uoropyrimidine use ) , or patients chose to stop . 
patients on arm c received chemotherapy for 12 weeks , after which treatment was stopped completely and the patients 644 vol 12 july 2011 articles 2445 patients enrolled 815 randomised to arm a 815 randomised to arm c 815 randomised to arm b 303 exclusions in the rst 12 weeks 69 deaths 104 progressive disease 60 came o trial for other specic reason 21 too few treatment cycles 49 no valid 12 - week assessment 290 exclusions in the rst 12 weeks 63 deaths 106 progressive disease 68 came o trial for other specic reason 17 too few treatment cycles 36 no valid 12 - week assessment a vs b comparison is reported in reference 9 512 had valid 12 - week assessment : result not progressive disease 525 had valid 12 - week assessment : result not progressive disease 45 excluded 14 excluded 2 one further cycle but only to complete original 12 - week period 1 lost to follow - up 13 protocol violation * 29 came o trial for other specic reason within 3542 days of 12 - week assessment 6 planned surgery 7 second - line therapy 3 clinician decision ( other than second - line ) 3 progression 4 toxic eects 3 intercurrent illness 3 patient decision 1 lost to follow - up 6 protocol violation * 7 came o trial for other specic reason within 3542 days of 12 - week assessment 2 planned surgery 2 second - line therapy 2 clinician decision ( other than second - line ) 1 other ( patient had bowel obstruction and needed a stent ) 467 pp analysis population 511 pp analysis population figure 2 : trial pro le pp = per - protocol . 
the intermittent strategy was that the same chemotherapy was to be restarted on con rmation of progressive disease ( with this scan becoming the new baseline measure ment )  . 
forms were scheduled to be completed at baseline ( before randomisation ) , 6 weeks , 12 weeks , and every 12 weeks thereafter ( before knowledge of ct scan results )  . the primary objective of this part of the coin trial was to establish whether intermittent therapy was noninferior to continuous therapy in terms of overall survival in patients with advanced colorectal cancer . 
the secondary aims were to evaluate failure - free survival ( of the treatment strategies ) , response , toxic e ects , quality of life , and cost - e ectiveness . 
the primary quality - of - life outcome measures were palliation , toxic e ects , functional scales , and global quality of life . statistical analysis the sample size for comparison of arm a versus c was 1614 patients ( 807 per arm )  . 
in the uk - based focus trial , 1 patients receiving continuous chemotherapy had 2 - year overall survival of 20% and a median overall survival of vol 12 july 2011 articles 100 075 050 025 100 075 050 025 arm a ( continuous ) arm c ( intermittent ) hr 1084 ( 80% ci 10081165 ; 95% ci 09701211 ) median survival ( months ) : arm a , 158 ; arm c , 144 ; one - sided 90% cl 136 ; non - inferiority limit 136 hr 1087 ( 80% ci 09861198 ; 95% ci 09361261 ) median survival ( months ) : arm a , 196 ; arm c , 180 ; one - sided 90% cl 163 ; non - inferiority limit 169 number at risk arm a 815 arm c 815 688 668 513 477 297 281 151 148 467 511 459 498 368 381 213 224 104 113 hr 1052 ( 80% ci 09821128 ; 95% ci 09471170 ) median survival ( months ) : arm a , 84 ; arm c , 74 hr 1075 ( 80% ci 09861173 ; 95% ci 09411229 ) median survival ( months ) : arm a , 92 ; arm c , 87 number at risk time ( months ) time ( months ) arm a 815 arm c 815 515 456 168 178 467 511 391 369 125 148 figure 3 : kaplan - meier curves for overall survival in ( a ) the itt population and ( b ) the per - protocol population , and strategy - failure - free survival in ( c ) the itt population and ( d ) the per - protocol population median survival in each arm is derived directly from the kaplan - meier curve . 
additionally , for overall survival we present median survival in arm c corresponding to the one - sided 90% ( ie , upper 80% ) con dence limit ( cl ) of the hazard ratio ( hr ) ; and for comparison , the limit of median survival regarded non - inferior with the pre de ned non - inferiority bound of hr 1162 . 
to show non - inferiority with a one - sided log - rank test with of 01 and power of 90% , 1420 patients would be needed ( 710 patients per arm )  . 
to account for the roughly 12% of patients who progress or who do not complete 12 weeks of treatment and therefore would not contribute to the comparison , the target sample size was increased to 807 patients per arm , and the analysis was timed to be done when at least 1168 overall survival events had occurred . 
stata were two - sided at a 95% signi cance ( version 11.1 ) was used for all statistical analyses . the primary question was one of non - inferiority , so both intention - to - treat ( itt ) and per - protocol analyses of overall survival were planned . 
the itt analysis included all patients randomly allocated to treatment groups , whereas the per - protocol analysis included patients who reached the point at which continuous and intermittent strategies divergedie , they received a full 12 weeks treatment ( allowing for one missed cycle ) , remained on trial , and had no evidence of progressive disease at 12 weeks ( within 4 weeks )  . 
 additionally , the patients included in the per - protocol analysis had to have adhered to the assigned protocol strategy at 12 weeksie , patients in arm a continuing treatment and those in arm c starting a chemotherapyfree interval . 
this population was de ned to correspond to the patient cohort who , when seen at the 12 - week timepoint ( outside a trial context ) , would bene t from discussion about whether to continue treatment or begin a chemotherapy - free interval . 
strategy - failure - free survival was de ned as the time from randomisation to failure time 646 vol 12 july 2011 articles equated this measure of the coin strategy to which a patient was randomly assigned ( webappendix p 3 )  . 
in the intermittent treatment group , a strategy - failure - free survival event occurred when a patient had progressive disease during a planned treatment period or within 8 weeks of starting a chemotherapy - free interval . 
 the primary analysis timepoint for quality of life was 24 weeks after randomisation , but baseline and 12 - week data were also analysed since these timepoints were milestones in the treatment strategy . 
ordinal logistic regression was used to predict 12 - week and 24 - week scores rounded into ve categories , adjusting for treatment arm and previous scores . we compared rates of toxic e ects between treatment groups using a test , or fishers exact test in case of low event rates ( n < 5 )  . 
to investigate the e ect of prespeci ed covariates on survival , we built prognostic models using a backward stepwise approach with critical value p = 005 for both removal from and re - entry into the model at each iteration . 
to investigate whether these covariates modi ed the treatment e ect , predictive models were tted that included the covariate , treatment arm , and a treatmentpredictive factor interaction term ; interaction tests were done with likelihood - ratio tests of the null hypothesis that the interaction coe cient is zero . this trial is registered , isrctn27286448 . role of the funding source the trial was conceived and developed by the national cancer research institute advanced colorectal clinical studies group . 
the corresponding author had full access to the data and had nal responsibility for the decision to submit for publication . results between march 9 , 2005 , and may 9 , 2008 , 2445 patients were randomly allocated to treatment groups at 111 centres in the uk and ireland , with 1630 patients assigned to the comparison of continuous versus intermittent treatment . 
 * in the coin dataset , the rst disease response assessment was at around 12 weeks ; therefore , patients with stable disease must have ( at least ) maintained this stability for that length of time . 
 table 2 : response at 12 weeks and best response in arms a and c and response after rechallenge ( arm c only ) 12 weeks 24 weeks or ( 95% ci ) p value or ( 95% ci ) p value functional scales impaired physical functioning impaired role functioning 113 ( 097130 ) 111 ( 097127 ) impaired cognitive functioning impaired social functioning 107 ( 092123 ) 105 ( 091120 ) impaired emotional functioning 114 ( 098131 ) 0086 101 ( 085120 ) 099 ( 083118 ) 089 082 ( 070096 ) 0015 090 024 090 ( 076107 ) 082 ( 070096 ) 0016 073 ( 062087 ) 000025 082 ( 068098 ) 0033 138 ( 116164 ) 000029 100 ( 084120 ) 094 ( 079111 ) 080 ( 067095 ) 082 ( 068099 ) 099 044 0012 0037 079 ( 066094 ) 0008 066 ( 055079 ) < 00001 011 013 037 052 075 065 066 040 019 028 028 079 062 016 083 046 102 ( 089117 ) 103 ( 090119 ) 103 ( 089120 ) 106 ( 092123 ) 110 ( 095126 ) 108 ( 094125 ) 109 ( 093128 ) 098 ( 085113 ) 104 ( 090119 ) problems eating or drinking 123 ( 100150 ) 0045 063 ( 047084 ) 00021 problems handling small objects 112 ( 096132 ) 054 ( 045065 ) < 00001 treatment interferes with daily activities 101 ( 089116 ) 062 ( 052073 ) < 00001 treatment felt to have been worthwhile 094 ( 080111 ) 120 ( 096150 ) 012 108 ( 093125 ) 030 098 ( 083115 ) 081 odds ratios ( ors ) are for arm c compared with arm a , and are from ordinal regression models adjusting for previous timepoints ( baseline , 12 weeks )  . 
ors greater than 1 indicate worse quality of life , and ors less than 1 indicate better quality of life . table 3 : quality of life at 12 and 24 weeks see online for webappendix and to arm c was 218 months ( 162295 )  . 
28 ( 7% ) of 383 surviving patients had no data returned for 12 months and were deemed lost to follow - up . 35 ( 2% ) patients did not start trial therapy because of clinical deterioration after randomisation , patient choice , or subsequent ineligibility after randomisation . 
in the per - protocol population , the geometric mean overall time on treatment in arm c was 52 months ( 95% ci 5054 ) versus 75 months ( 7378 ) in arm a ( p < 00001 )  . 
although total dose delivered of chemo therapeutic agents was greater in arm a than in arm c ( p < 00001 ) , dose intensity was in arm c during on - treatment periods greater ( p < 00001 )  . 
in treatment group , 325 ( 64% ) of 511 potentially eligible patients restarted a second 12 - week course of chemo therapy after a chemotherapy - free interval . intermittent the 1247 ( 77% ) deaths had occurred in the itt population at the time of analysis . 
median survival in the itt population was 158 months ( iqr 94261 ) in arm a and 144 months ( 80247 ) in arm c , and in the perprotocol population was 196 months ( 130281 ) in arm a and 180 months ( 121293 ) in arm c . 
the hr point estimates were 1084 ( 80% ci 10081165 ) in the itt population and 1087 ( 09861198 ) in the perprotocol population ; the upper limits were higher than the prede ned non - inferiority boundary ( gure 3 )  . 
 kaplan - meier overall survival in the itt population for arm a versus arm c was 287% versus 265% at 2 years and 130% versus 112% at 3 years . 1166 ( 94% ) of 1247 deaths in the itt population were due to colorectal cancer . 
22 ( 2% ) deaths were reported to be treatment - related , 52 ( 4% ) were from other causes , and the cause of death for the remaining seven ( < 1% ) is currently unknown . 
70 ( 6% ) deaths occurred within 60 days of randomisation , with no di erence between the two groups . median strategy - failure - free survival the itt population was 84 months ( iqr 53118 ) in arm a and 74 months ( 51121 ) in arm c , and in the perprotocol population was 92 months ( 70129 ) in arm a and 87 months ( 59134 ) in arm c . 
from the kaplan - meier plots ( gure 3 ) , intermittent therapy seemed to result in a greater loss of patients ( in terms of strategy ) early on , especially around 69 months , but at 2 years there was little di erence in number of patients remaining on strategy : 2 - year survival in the itt analysis was 74% ( n = 28 ) in the continuous treatment arm and 76% ( n = 35 ) in the intermittent treatment arm , and in the per - protocol analysis was 77% on continuous ( n = 18 ) and 76% on intermittent ( n = 24 ) treatment . among patients in the per - protocol population allocated intermittent treatment who commenced a chemotherapyfree interval ( n = 511 ) , the median time to progression was 129 weeks ( 30 months ; iqr 109240 weeks )  . 
among those who later restarted trial therapy ( n = 325 ) , the median overall length of the chemotherapy - free interval before progression was 160 weeks ( 37 months ; iqr 137260 weeks )  . 
the median number of chemotherapy - free intervals was two ( range one to six )  . protocol treatment in both treatment groups was identical up to 12 weeks ( the time of the rst scheduled radiological disease assessment )  . 
best overall response ( by recist criteria ) did not di er between treatment groups , suggesting that most patients achieve best response within the rst 12 weeks of therapy . 
grade 3 or worse peripheral neuropathy and hand foot syndrome were more frequent during continuous treatment ( webappendix p 4 )  . there were fewer eligible patients in arm c ( 79% , n = 647 ) than in arm a ( 89% , n = 724 ; p < 00001 ) , since more patients in arm c either remained on trial therapy ( 6% vs 1% in arm a , n = 46 vs nine , p < 00001 ) or died ( 14% vs 9% in arm a , n = 115 vs 74 , p = 00015 )  . 
among patients judged eligible to receive second - line therapy , this treatment was given to signi cantly fewer patients on intermittent therapy ( 52% , n = 336 ) than on continuous therapy ( 62% , n = 448 ; p = 000020 )  . quality of life in the per - protocol population at baseline , 12 weeks , and 24 weeks was assessable in 279 ( 60% ) patients on continuous treatment and 282 ( 55% ) patients on intermittent treatment . 
no clear evidence of di erences in baseline characteristics was identi ed between those patients who completed quality - of - life questionnaires and all patients randomly allocated to treatment groups , but the risk of such di erences cannot be eliminated . 
after adjustment for previous measurements , there were signi cant bene ts from intermittent therapy at 24 weeks for fatigue , dry or sore mouth , problems eating and drinking , di culty handling small objects , interference with daily activities , nausea or vomiting , appetite loss , constipation , and diarrhoea ( table 3 ; p < 005 for all )  . 
at 12 weeks , there was a nonsigni cant trend towards an adverse e ect of intermittent therapy on emotional functioning ( p = 0086 ) , but this result was not evident at 24 weeks ( p = 090 ; table 3 )  . we undertook a post - hoc exploratory analysis of the e ects of protocol adherence on overall survival . 
a cuto of 60% was chosen because this proportion formed a pragmatic and appropriate benchmark midway between the 40% and 80% of restarts reported in optimox - 1 and optimox - 2 , respectively . 
 however , this di erence lessens over time and the overall hr is non - signi cant ( gure 4 )  . favours intermittent therapy favours continuous therapy figure 5 : subgroup analyses of overall survival within the per - protocol population hr = hazard ratio . 
the nal model contained the following previously identi ed prognostic variables : previous adjuvant chemotherapy or surgery ; alkaline phosphatase ; body surface - area ; platelet count ; time from diagnosis to vol 12 july 2011 articles 100 075 050 025 normal platelet count ( < 400 000 per l ) raised platelet count ( 400 000 per l ) arm a ( continuous ) arm c ( intermittent ) hr 0961 ( 80% ci 08541080 ; 95% ci 08031150 ) , p = 0660 hr 1545 ( 80% ci 12921848 ; 95% ci 11752031 ) , p = 00018 number at risk time ( months ) time ( months ) arm a 332 arm c 371 327 365 265 295 158 185 133 138 130 131 101 figure 6 : kaplan - meier curves of overall survival within the per - protocol population , by baseline platelet subgroup interaction with treatment arm : hazard ratio ( hr ) 1646 ( 95% ci 11882279 ) ; p = 00027 . randomisation ; resection of primary tumour ; mutation present in any of kras , nras , or braf ; and number of metastatic sites . 
in particular , each of the four variables identi ed by khne and colleagues13 were present with the exception of white blood cell count ( in our data , platelet count was a stronger prognostic indicator ) , and the score de ned by khne was strongly prognostic ( p < 00001 for trend )  . 
a raised platelet count at baseline ( 400 000 per l , recorded for 271 [ 28% ] of 978 patients ) predicts a signi cant survival detriment from intermittent chemotherapy ( p = 00027 for interaction ; gure 6 )  . 
raised baseline platelet count had an even greater predictive e ect for a detriment from intermittent therapy on 24 - week quality of life , particularly for functional scales ( p < 005 for all ) , for which a consistent trend was noted towards bene t from intermittent therapy for patients with normal platelet count and an adverse e ect for patients with raised platelet count . 
additionally , the symptom scales of fatigue , pain , dyspnoea , appetite loss , constipation , and global quality of life followed this trend ( p < 005 for all )  . 
furthermore , patients on intermittent therapy were signi cantly more likely than were those on continuous therapy to report at 24 weeks that their treatment had not been worthwhile if their baseline platelet count was raised ( p = 0048 for interaction ; webappendix p 7 )  . 
other factors with interactions signi cant at the 10% level were presence of metastases in the liver only ( p = 0066 ) and tumoral kras status ( p = 0070 )  . discussion the goal of palliative chemotherapy is to increase overall survival with improvement or minimum de cit in quality of life . 
the trial did not meet its primary outcome objective , which was to show non - inferiority intermittent chemotherapy versus continuous chemotherapy as rst - line in advanced colorectal cancer . 
however , there seems to be a large subpopula tion of patients for whom intermittent therapy provides similar survival bene t and can be recommended . therapy that the coin trial has shown intermittent chemotherapy is associated with improved quality of life , shortened time on chemotherapy , reduced number of visits to hospital , and a minimum di erence in overall survival . 
in coin , we developed a statistical plan that set the outer bound of the hr for non - inferiority for overall survival at the rigorous level of 1162 ( for comparison , the outer bound in the comparison of uorouracil versus capecitabine in the x - act trial was 125 ) .14 the trial did not meet this strict criterion ( upper limit of hr in the itt group was 1165 )  . 
this 650 vol 12 july 2011 articles result does not suggest that continuous chemotherapy is superior to an intermittent strategy , but does translate into an observed di erence in median overall survival of around 6 weeks ( 14 months ) , favouring continuous therapy . 
our con dence intervals reliably exclude a detriment greater than 22 months ( itt analysis ) or 32 months ( per - protocol analysis ) in median overall survival with intermittent therapy . the striking outcome from the study is the signi cant correlation of a raised baseline platelet count as a predictive biomarker for use of a continuous or intermittent chemotherapy strategy . 
a quarter of patients had a raised platelet count at baseline and these patients had substantially inferior survival ( a 5 - month reduction in survival ; test for interaction p = 00027 ) when treated with intermittent chemotherapy and also impaired quality of life on almost all scales apart from those directly related to toxic e ects of chemotherapy . 
raised platelet count has previously been identi ed as a poor prognostic marker in advanced colorectal cancer.13 the mechanism could relate to paracrine feedback driven by cytokines including interleukin 6 , directly causing throm bocytosis.15 it could , alternatively , relate to an aspect of immunomodulation driven by t - regulatory cells and foxp3 epigenetic regulation.16 if con rmed in other datasets , the easily measurable marker of a raised platelet count at initiation of chemotherapy would be a helpful and cost - e ective predictive biomarker for identi cation of patients in whom continuous therapy might be preferable in order to maximise symptom control and survival . the shorter overall survival in this uk trial compared with some other trial settings is probably related to a combination of several factors , such as a more advanced distribution of disease at presentation , fewer available e ective treatments , or di erent attitudes of patients and clinicians to additional therapy . 
a recent report17 shows from registry data that survival for colorectal cancer is lower in the uk than for other comparable countries ( for 1 - year survival uk registries reported 75% compared with 8085% for the other registries in the comparable years 200507 ; 54% vs 5866% at 5 years )  . 
since coin recruited widely from 111 centres across the uk and ireland and had broad inclusion criteria , it is likely to be representative of outcomes for advanced colorectal cancer in the uk . failure to restart oxaliplatin - based chemotherapy after an interval has previously been identi ed as detrimental to survival.18 in the coin per - protocol population ( ie , patients clinically eligible to recommence chemotherapy ) , 325 ( 64% ) of 511 potentially eligible patients restarted a second 12 - week course of chemo therapy . 
this proportion compares with a reintroduction rate of 40% in optimox - 17 and 80% in optimox - 2 , which recruited patients from only 12 centres and in which high rates of reintroduction were protocol mandated.8 the gure of 64% from the coin trial could reason ably represent a good re ection of real practice in an incurable disease , in which chemotherapy must strike a balance between quality and length of life . 
the proportion of coin patients restarting oxaliplatin and the low numbers receiving second - line chemotherapy regimens compared with some other countries re ects a less aggressive approach that is characteristic of uk oncology and could also have contributed to the lower overall survival . additionally , the predominantly uk study setting is important in that bevacizumab was not reimbursed for rst - line treatment or subsequent use in routine nhs practice during the study period , and although its availability would probably have resulted in longer overall survival , the e ect of addition of this targeted agent on a chemotherapy - free interval strategy is unclear . 
in the aio trial , 20 patients are randomly allocated to one of three arms ( bevacizumab plus uoropyrimidine , bevacizumab alone , or no treatment after 24 weeks of induction oxaliplatin uoropyrimidine and bevacizumab ) and complete accrual is due in 2013 . 
however , our message that omission of chemotherapy for long periods in selected patients without overall survival interpreted cautiously vol 12 july 2011 articles panel : research in context systematic review conventional palliative chemotherapy for treatment of advanced colorectal cancer is given continuously until progressive disease or cumulative toxic e ects occur , or the patient chooses to discontinue . 
in a previous medical research council study , cr06b , 5 a shortened course of chemotherapy with reuse of the same treatment on progression showed an improvement in quality of life with no loss of survival . 
one consistent nding is that patients receiving short - course therapy can have a reduced time to disease progression , but several investigators have reported that at the time of progression patients can be successfully rechallenged with the same regimen . 
searches of medline and cancerlit for publications and pdq ( physicians data query ) and the ukcccr trial register for any additional open or closed trials in advanced colorectal cancer found no trials comparing these approaches when this trial was started . interpretation survival in coin is shorter than for many international trials in advanced colorectal cancer , which probably re ects a more advanced stage of disease at presentation in the uk . 
additionally , the lack of routine availability of biological agents in the uk national health service might contribute to shortened survival and therefore restrict direct application of the coin data in the most resource - rich health - care settings . 
the nding that intermittent chemotherapy is inferior in patients with raised platelet counts is novel and needs con rmation , but supports the conventional practice of continuous chemotherapy for this cohort . 
conversely , for most patients with normal platelet counts at baseline , this study suggests that chemotherapy - free intervals are associated with improved quality of life and no loss of overall survival and is therefore an option that clinicians should discuss with such patients . de cit could be even more relevant in such contexts . 
 potential bene ts from the continuation of such targeted agents with or without the addition of a uoropyrimidine , when oxaliplatin temporarily discontinued , have yet to be shown in terms of progression - free or strategy - failure - free survival or more importantly in terms of overall survival in any completed randomised controlled trials ; such data are eagerly awaited . standard uk practice is to image patients at 12 - week intervals . 
during treatment breaks , patients in arm c attended hospital as outpatients or day cases on an average of two occasions every 1224 weeks , whereas those in arm a would have been seen on at least eight occasions and possibly 12 depending on the chemotherapy regimen . 
this more frequent clinical review could have led to earlier identi cation of disease progression . the secondary and subgroup analyses of the trial are intended to o er some guidance to practising clinicians , patients , and patient advocates . 
the overall e ect on quality of life with time o treatment in arm c , as assessed at the speci c timepoints of 12 and 24 weeks , suggest an improvement in fatigue , nausea and vomiting , anorexia or loss of appetite , constipation , diarrhoea , dry or sore mouth , and di culty handling objects . 
however , pain seems to be slightly but consistently more frequent in those receiving the intermittent strategy , which could be accounted for by the increased likelihood of tumour progression or activity during a chemotherapy - free interval . 
yet this nding disappears at 24 weeks , when those on continuous therapy may be uncertain about continuing e ectiveness or tolerability of ongoing treatment . initial 12 - week period of in advanced colorectal cancer , for patients treated with palliative intent , as in most other malignancies , time o chemotherapy remains a treatment option . 
this study has shown and quanti ed the bene ts of a chemotherapyfree interval in terms of reduced time on chemotherapy , reduced cumulative toxic e ects , and improved quality of life after an induction chemotherapy . 
by contrast , the three - quarters of patients in coin with normal platelet counts at randomisa tion su ered no loss in overall survival and could reap potentially important bene ts of chemotherapyfree intervals . contributors raa was the trial fellow , member of trial management group , reviewed all safety events , and co - wrote the report . 
sf , sg , th , emb , and dp were the highest recruiting oncologists to the trial and mjk was the lead oncologist for the sites in ireland and contributed to trial management . 
all authors reviewed all the data and commented on the report . 652 vol 12 july 2011 articles con icts of interest raa and tsm have received travel , accommodation , and lecture fees from roche and merck serono . 
th has received travel expenses , meeting attendance , and lecture fees from glaxosmithkline , novartis , sano , roche , p zer , and abraxis and also payment for manuscript preparation from the british journal of healthcare . 
our aim was to assess the strengths of their e ects and determine whether they depend on characteristics of the tumours or the a ected women . methods individual data from 117 epidemiological studies , including 118 964 women with invasive breast cancer and 306 091 without the disease , none of whom had used menopausal hormone therapy , were included in the analyses . 
 we calculated adjusted relative risks ( rrs ) associated with menarche and menopause for breast cancer overall , and by tumour histology and by oestrogen receptor expression . findings breast cancer risk increased by a factor of 1050 ( 95% ci 10441057 ; p < 00001 ) for every year younger at menarche , and independently by a smaller amount ( 1029 , 10251032 ; p < 00001 ) , for every year older at menopause . 
 premenopausal women had a greater risk of breast cancer than postmenopausal women of an identical age ( rr at age 4554 years 143 , 133152 , p < 0001 )  . 
all three of these associations were attenuated by increasing adiposity among postmenopausal women , but did not vary materially by womens year of birth , ethnic origin , childbearing history , smoking , alcohol consumption , or hormonal contraceptive use . 
the e ect of menopause in women of an identical age and trends by age at menopause were stronger for oestrogen receptor - positive disease than for oestrogen receptor - negative disease ( p < 001 for both comparisons )  . interpretation the e ects of menarche and menopause on breast cancer risk might not be acting merely by lengthening womens total number of reproductive years . 
 to assess reliably the strengths of these associations and whether they vary by tumour subtype or by characteristics of a ected women requires large numbers , and we address these questions by combining information from more than 100 epidemiological studies . 
combining individual participant data from many studies not only increases statistical power but also permits similar de nitions and similar analytical methods to be used across studies . methods search strategy and selection criteria this collaboration began in 1992 , and has published on breast cancer risk associated with use of hormonal therapies and childbearing practices.14 potentially eli gible epidemiological studies have been sought at regular intervals by computer - aided literature searches , by written communication and discussions with col leagues , and by discussions at scienti c meetings , including collaborators meetings in oxford in 1993 , 1995 , 2000 , 2005 , and 2011 ( appendix p 3 shows search strategy and selection criteria )  . 
so that similar analytical methods could be used across studies , we incorporated cohort studies using a nested case control design , in which up to four controls were selected at random , matched at follow - up to age of the case at cancer diagnosis and , where appropriate , by broad geographical region . 
data for a range of sociodemographic , reproductive , and other behavioural factors , covering the time period to onset of disease for cases and to an equivalent time for controls , were sought from principal investigators ( appendix p 3 )  . vol 13 november 2012 1141 articles we included studies in these analyses if individual data had been provided for womens menopausal status , age at menarche and , if appropriate , age at menopause , and whether or not they had had a hysterectomy or a bilateral oophorectomy . 
women who had had a natural menopause or who had had a bilateral oophorectomy before their natural menopause were classi ed as postmenopausal , but those who had had a hysterectomy without bilateral oophorectomy before their natural menopause were classi ed as being of unknown menopausal status ( because hysterectomy can mask cessation of ovarian activity )  . 
otherwise , we took de nitions used by principal investigators to classify each woman by her age at menarche , menopausal status and , for postmenopasual women , by her age at menopause . 
women with unknown menopausal status or unknown ages at menarche or menopause were excluded from analyses , as were women who had used menopausal hormone therapy , since such use can mask the onset of menopause and a age at menarche 9 10 11 12 13 14 15 16 17 18 19 20 age at menarche ( years ) b age at menopause age at natural menopause ( years ) figure 1 : cumulative distribution of ( a ) age at menarche and ( b ) age at natural menopause data are for women without breast cancerie , controls . 
results for age at menopause are based on data from 157 272 postmenopausal women aged older than 55 years at the time of reporting their age at menopause . modify associations between hormonal factors and breast cancer risk.1 we also sought information about tumour characteristicsie , about oestrogen receptor status and about tumour histology . 
we used information provided by principal investigators to classify tumours as oestrogen receptor - positive or oestrogen receptor - negative , and as ductal , lobular , or of other histology . from reports in previous statistical analysis we did all analyses using conditional logistic regression , similar in principle to the mantel - haenszel strati cation technique used this collaboration.16 when two groups were compared odds ratios ( ors , described as relative risks [ rrs ] when cases and controls are compared ) and standard cis are given . 
 when more than two groups were compared , we estimated variances for every group , treating the ors or rrs as oating absolute risks , 7 because this method enables valid comparisons between any two groups , even if neither is the baseline group . 
this method does not alter risk estimates , but yields variances for each nonbaseline group that are slightly smaller than the variances calculated with conventional methods ( because these include the variance of the baseline group ) and we used these variances to calculate group - speci c cis . 
any comparison between two risk estimates must take the variation in each group into account . analyses of the association between various factors and womens age at menarche and age at menopause were restricted to controls , and we calculated ors stratifying by study , by centre within study , and where appropriate by age at diagnosis ( 20 years , and then in 3 year age groups , 2123 years to 8789 years ) ; by year of birth ( < 1920 , 192029 , 193039 , 194049 , and 1950 ) ; by parity and age when rst child was born ( nulliparous women were a separate stratum and parous women were cross - classi ed by parity [ 12 , 3 ] and age at rst birth [ < 20 years , 2029 years , 30 years ] ) ; by current body - mass index ( bmi ; < 25 kg / m , 2529 kg / m , 30 kg / m ) ; by height ( < 160 cm , 160164 cm , 165 cm ) ; by smoking ( never , past , present ) ; and by alcohol consumption per week ( < 50 g and 50 g )  . 
we restricted analyses comparing breast cancer risk in premenopausal , perimenopausal , and postmenopausal women to women aged 4554 years ( since each category is represented in this narrow age band ) and we used the same strati cations as described above , except that age was strati ed by single years . 
or calculations were strati ed by study and , where appropriate , by age at diagnosis , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi ( results for bmi as a young adult are not strati ed by current bmi )  . 
bmi = body - mass index . vol 13 november 2012 1143 articles a age at menarche study , centre within study , age at diagnosis in single years , and year of birth , and adjusted by parity , age at rst birth , bmi , smoking , and alcohol consumption , also using the same categories as described previously . age at menarche ( years ) < 11 ( 97 ) 11 ( 110 ) 12 ( 120 ) 13 ( 130 ) 14 ( 140 ) 15 ( 150 ) 16 ( 166 ) 5511 / 11 685 119 ( 113125 ) 15 855 / 37 779 109 ( 106112 ) 25 806 / 61 512 107 ( 105109 ) 31 759 / 83 389 100 ( 098102 ) 20 599 / 53 212 098 ( 096100 ) 10 576 / 31 390 092 ( 089095 ) 8858 / 27 124 082 ( 079085 ) b age at menopause age group ( mean , years ) cases / controls ( 95% gs ci ) age group ( mean , years ) cases / controls ( 95% gs ci ) we calculated rrs for breast cancer per 1 year younger at menarche and per 1 year older at menopause by linear regression , using the mean age within each category . 
 signi cance tests for heterogeneity by tumour subtype were based on analyses within cases only ( because controls provide no additional information ) , strati ed by age , study , and bmi and adjusted for other variables listed previously . 
we did our analyses with stata ( version 11 )  . when results for large numbers of subgroups are presented in the gures 99% cis ( or group - speci c 99% cis ) are given , to take account of multiple testing . 
 in the text all cis quoted are 95% cis . role of the funding source the funders had no role in study design , data collection , analysis , or interpretation of data , preparation of the report , or decision to publish . 
all members of the analysis and writing committee ( vb , db , rp , kp , gr ) had access to the raw data and are responsible for the nal submission for publication . results overall 117 studies , together including 118 964 women with breast cancer ( cases ) and 306 091 without the disease ( controls ) , were included in these analyses . 
median age at cancer diagnosis was 54 years ( iqr 4464 )  . figure 1a shows the distribution of age at menarche reported by controlsie , women without breast cancer . 
 their mean age at menarche was 131 years ( sd 17 ) , with almost two - thirds ( 65% , 198 113 of 306 068 ) reporting menarche at ages 12 , 13 , or 14 years . 
only 16% ( 49 464 ) of the controls reported menarche at age 11 years or younger and 19% ( 58 514 ) reported menarche at age 15 years or older . 
having early menarche was associated with many factors known to a ect breast cancer risk , including parity , figure 4 : relative risk of breast cancer ( a ) per year younger at menarche and ( b ) per year older at menopause , in various subgroups and by tumour characteristics relative risks are calculated stratifying by study and age , and where appropriate , by year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi ( results for bmi as a young adult are not strati ed by current bmi )  . 
 * subgroup analyses for age at menarche are for age at menopause < 50 vs 50 years in postmenopausal women ; and for age at menopause are for age at menarche < 13 vs 13 years . 
case - case comparisons strati ed by study , age and year of birth , and adjusted by parity , age at rst birth , smoking , alcohol consumption , height , and current bmi . 
 age at menopause ( years ) < 40 ( 353 ) 4044 ( 419 ) 4549 ( 472 ) 5054 ( 515 ) 55 ( 561 ) 2397 / 7741 067 ( 062073 ) 5516 / 18 544 073 ( 070077 ) 17 336 / 52 040 086 ( 084089 ) 28 197 / 75 944 100 ( 098102 ) 6891 / 16 144 112 ( 107117 ) figure 3 : relative risk of breast cancer by ( a ) age at menarche and ( b ) age at menopause calculated stratifying by study , age , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current body - mass index . 
rrs strati ed by study , age at diagnosis in single years , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi . 
 * results for breast cancer risk are plotted against the time between menopause and the diagnosis of breast cancer for postmenopausal women , and against an estimate of that time for premenopausal and perimenopausal women . 
the premenopausal women aged 4554 years in these analyses would be expected to reach their menopause in the next 27 years , on average ( this estimate is based on the age distribution of the premenopausal women in these analyses and the age distribution of womens ages at menopause shown in gure 1b )  . 
perimenopausal women might be expected to reach their menopause in the next 6 months , on average . age at rst birth , height , and bmi ( gure 2a )  . 
associations with late menarche were generally the con verse of associations with an early menarche ( appendix p 7 )  . the younger women were at menarche , the greater was their subsequent risk of breast cancer , the rr increasing by a factor of 1050 ( 95% ci 10441057 , p < 00001 ) for every year younger at menarche ( gure 3a )  . 
results in figure 3a were strati ed by study , age , year of birth , parity and age at rst birth , height , current bmi , smoking , consumption . 
additional adjustment ( either individually or simultaneously ) by ethnic origin , hormonal contraceptive use , and family history of breast cancer , altered the excess rr estimate by less than 1% ( data not shown )  . alcohol and to assess consistency of ndings , we calculated the rr of breast cancer per year younger at menarche for 34 subgroups of women , subdivided by 14 of their personal characteristics : year of birth , age at diagnosis and menopausal status , ethnic origin , parity , age at rst birth , height , bmi as a young adult , current bmi , use of oral contraceptives , smoking , alcohol consumption , family history of breast cancer , menopausal status and , for their age at menopause postmenopausal women , ( gure 4a )  . 
both among premenopausal and among postmenopausal women , increasing bmi seemed to attenuate the relevance of age at menarche , but this attenuation was signi cant only among postmenopausal women ( hetero geneity p = 0006 )  . 
we noted some weakening of the association with age at menarche by attained age in postmenopausal women ( heterogeneity p = 004 ; trend p = 002 ) and family history of breast cancer ( heterogeneity p = 001 ) , but for all other personal characteristics examined heterogeneity across subgroups was not signi cant . 
the ndings were not dominated by the results in any particular study ( appendix pp 810 ) and there was no signi cant heterogeneity in the ndings by study design ( appendix p 6 )  . of the 117 contributing studies , 85 provided some information about tumour characteristics ( appendix pp 45 ) , and gure 4a shows the rrs per year younger at menarche for various tumour subtypes . 
the association with age at menarche was signi cantly stronger for lobular than ductal tumours ( heterogeneity p = 00001 ) , but there were no signi cant di erences by oestrogen receptor status . 
cross - classi cation by both oestrogen receptor status and tumour histology did not show any further interaction ( appendix p 6 )  . figure 1b shows the cumulative distribution of the reported age at natural menopause among postmenopausal controls . 
their mean age at natural menopause was 493 years ( sd 46 ) , with 15% ( 26 285 of 170 413 ) reporting menopause before age 45 years , 75% ( 127 984 ) between the ages 45 and 54 years , and 10% ( 16 144 ) at age 55 years or older . 
associations with an early meno pause were generally the converse of those associated with a late menopause ( appendix p 7 )  . ovarian production of hormones decreases rapidly at around the time of menopause , as is shown in gure 5a , using published data from a cohort study of women who were premenopausal at entry and who had repeated measures of serum oestradiol until after the menopause.8 the short - term e ect of these changes on breast cancer risk can be assessed by restricting analyses to the 31 000 cases and 70 000 controls aged 4554 years ( since pre menopausal , peri menopausal , and postmenopausal women are represented in this age group ) and by stratifying analyses by single years of age ( so that women of identical ages are being compared )  . 
among such women , breast cancer risk was greater among premeno pausal than postmenopausal women ( rr 143 , 95% ci 133152 , p < 00001 ) , with the risk for perimenopausal women being between the other two ( gure 5b ; p < 0001 for all comparisons )  . the consistency of the nding of a greater risk of breast cancer among premenopausal than post menopausal women of the same age was examined across 30 subgroups of women , subdivided by 13 of their characteristics ( appendix p 11 )  . 
this nding re ects , at least in part , known di erences between premenopausal and postmenopausal women in the relation between their current bmi and breast cancer risk , as shown in gure 5c . 
among premenopausal women , those who were overweight or obese ( bmi 25 kg / m ) had a lower risk of breast cancer than leaner women ( bmi < 25 kg / m ) , whereas the reverse was observed among postmenopausal women . 
however , at ages 4554 years , where both premenopausal and postmenopausal women are rep resented , a sudden decrease occurs at menopause in the proportion of oestrogen the proportion of tumours with lobular histology increases with age , with a sudden decrease around the time of menopause . 
after adjusting by single years of age and other potential confounding factors , the heterogeneity at ages and postmenopausal women is highly signi cant both for oestrogen receptor status ( hetero geneity p = 0003 ) and for tumour histology ( heterogeneity p < 00001 , appendix p 11 )  . in analyses restricted to postmenopausal women , the rr of breast cancer increased by a factor of 1029 ( 10251032 , p < 00001 ) for every year older at menopause ( gure 3b )  . 
the ndings in gure 3b were years between premenopausal 4554 b lobular breast cancers age at diagnosis ( years ) figure 6 : breast cancer by tumour characteristics and by womens age and menopausal status ( a ) oestrogen receptor - positive ( er + )  . 
results are shown for age groups < 40 years , 4044 years , 4554 years , 5559 years , 6064 years , and 65 years , and plotted against the mean age of women with breast cancer in each age group . strati ed by study , year of birth , age , parity and age at rst birth , height , current bmi , smoking , and alcohol consumption . 
additional adjustment by ethnic origin , age at menarche , family history of breast cancer , and hormonal contraceptive use ( both individually and simultaneously ) altered the excess rr estimate by less than 1% ( data not shown )  . 
rrs did not di er signi cantly between women with a natural menopause ( 1030 , 10261034 ) and bilateral oophor ectomy ( 1019 , 10041034 , heterogeneity p = 02 ; appendix p 12 )  . the association between age at menopause and breast cancer risk was examined in 30 subgroups and did not vary signi cantly across 11 of the 13 characteristics examined ( gure 4b )  . 
the relation between breast cancer risk and increasing age at vol 13 november 2012 1147 articles menopause was signi cantly greater for oestrogen receptor - positive disease than for oestrogen receptornegative disease ( p = 001 ) , and for lobular than for ductal tumours ( heterogeneity p = 0006 )  . 
the ndings were not dominated by the results in any particular study ( appendix pp 1315 ) and there was no signi cant variation by study design ( appendix p 6 )  . among postmenopausal women , for whom the e ect on breast cancer risk per year younger at menarche can be directly compared to the e ect per year older at menopause , breast cancer risk increased by a signi cantly greater amount per year of menarche than per year of menopause ( 1045 [ 10361054 ] vs 1029 [ 10251032 ] ; heterogeneity p = 0001 )  . discussion this worldwide collaboration has brought together and reanalysed individual participant data for 120 000 women with breast cancer and 300 000 controls without the disease from 117 epidemiological studies in 35 countries ( panel )  . while con rming that early menarche and late menopause increase breast cancer risk , we showed that these e ects were not equivalent , in that the excess risk panel : research in context systematic review the collaborative group on hormonal factors in breast cancer began in 1992 . 
since then published literature on epidemiological studies of breast cancer has been identi ed using electronic searches ( medline , embase , and pubmed , 19982011 ; using combinations of the search terms breast cancer , risk , epidem * , and hormones ) , supplemented by hand searching in review articles . 
eligible studies needed to have obtained individual information about reproductive factors and about use of hormonal therapies , from at least 400 women with breast cancer and similar information from controls without the disease . 
studies that had obtained relevant data , but had not published any results for breast cancer were sought by correspondence with colleagues , by discussions at collaborators meetings , and by electronic searches using additional terms cohort , prospective , women , and cancer risk . 117 eligible studies were included and principal investigators contributed information about almost 120 000 women with breast cancer who had never used menopausal hormonal therapies to this individual - participant meta - analysis . 
we report on the relation between menarche and menopause and breast cancer risk , overall , and by oestrogen receptor status and by histological subtypes of the tumours , adjusting for possible confounding factors . 
subgroup results are also shown by various sociodemographic and personal characteristics , including year of birth , ethnic origin , parity , age at rst birth , smoking , alcohol consumption , and body - mass index . interpretation breast cancer risk increased by a signi cantly greater factor for every year younger at menarche than for every year older at menopause , indicating that menarche and menopause may not a ect breast cancer risk merely by extending womens total reproductive years . 
endogenous ovarian hormones are more relevant for oestrogen receptor - positive disease than for oestrogen receptor - negative disease and for lobular than for ductal tumours . associated with lengthening womens reproductive years by one year at menarche was greater than the excess associated with one years lengthening at menopause . 
 we also found that oestrogen receptor - positive and lobular breast cancers are strongly a ected by womens menopausal status , and by their age . the production of steroid hormones by the ovary begins at around the time of menarche and decreases rapidly at around the time of menopause . 
 by restricting analyses to the 31 000 women with breast cancer in this narrow age range and stratifying by single years of age ( and by other potential confounding factors ) , valid comparisons can be made of the short - term e ect of the menopause , and breast cancer risk was about 40% higher in premenopausal than in postmenopausal women of the same age . 
since the postmenopausal women had reached their menopause only an average 46 years previously , the ndings indicate a rapid decline in breast cancer risk in women of identical ages soon after menopause . 
this nding probably explains the attening of the age - incidence curve at around age 50 years , the so - called clemmesens hook , 9 frequently observed in populations before the widespread use of hormonal therapies and screening . there is accumulating evidence that oestrogen receptorpositive and lobular breast cancers are more sensitive to ovarian hormones than are oestrogen receptor - negative and ductal cancers . 
not only are oestrogen receptorpositive and lobular tumours strongly a ected by the menopause , as we have shown , but postmenopausal women who use hormone therapy have a greater increase in oestrogen receptor - positive than oestrogen receptornegative tumours and in lobular than ductal breast cancers.10 , 11 furthermore , oestrogen - blocking treatments improve survival for oestrogen receptor - positive , but not for oestrogen receptor - negative breast cancer.12 womens adiposity was consistently shown to attenuate associations between menopause and breast cancer risk . 
 circulating oestradiol concentrations increase as postmenopausal womens bmi increases.13 that the rr of breast cancer risk falls more rapidly after the menopause in lean than in overweight and obese women is likely to re ect , at least in part , di erences in oestradiol concentrations between such women . 
oestradiol concentrations in postmenopausal women are greater the younger they were at menarche , 14 and this might , in part , account for the associations recorded between age at menarche and breast cancer risk . although a womans age at menarche does not coincide precisely with the onset of breast development , the two are highly correlated.15 breast cancer is almost unknown before menarche and extremely rare soon afterwards , making it e ectively impossible to study the short - term e ects of the hormonal changes associated with menarche by comparing breast cancer risk in women of identical ages before and soon after menarche . 1148 vol 13 november 2012 articles these ndings con rm that young age at menarche and old age at menopause increase breast cancer risk . 
many factors known to a ect breast cancer risk , including childbearing patterns , height , and bmi , are also associated both with womens age at menarche and with their age at menopause . 
to ensure as much comparability as possible between women with breast cancer and controls , and thus to minimise potential confounding , analyses were strati ed by these factors , and by study , age , year of birth , smoking , and alcohol consumption . 
the associations did not vary materially by womens personal characteristics , other than bmi among postmenopausal women . this meta - analysis of individual - participant data includes almost all available epidemiological evidence for the association between menarche and menopause and breast cancer risk . 
single studies do not have su cient power to examine these asso ciations in detail , so reviews based solely on the limited published evidence could well be susceptible to publication bias . 
although availability of information about oestrogen receptor status varied substantially over time , with most studies done before 1990 contributing relatively little information , analyses of all available data combined were su ciently powered to describe asso ciations separately within both oestrogen receptor - positive receptor - negative disease . 
another important advantage of this metaanalysis is that it seeks to review both published and unpublished ndings , thus avoiding unduly selective emphasis on published results or on only some studies . oestrogen and women included in these analyses generally reported their ages at menarche and at menopause many years after the events had occurred . 
comparisons of information recorded at around the time of menarche and menopause with that recalled many years later has shown substantial regression to the mean over time , especially for recalled age at menarche , 1623 which would dilute estimates of rr.23 , 24 the slight attenuation in the estimated rr with attained age thus relects , at least in part , misclassi cation of recalled ages at menarche and , to a lesser extent , of recalled age at menopause . 
 since sig ni cant associations were recorded at all ages , it is reasonable to conclude that the e ects of age at menarche and age at menopause on breast cancer risk persist throughout life . since the e ect on breast cancer risk of 1 year younger at menarche is signi cantly greater than that of 1 year older at menopause , these ndings suggest that the e ects of each may not be acting merely by lengthening the total duration of womens reproductive years . 
in most populations womens average age at menarche has been declining in successive birth cohorts , 25 contributing to increasing incidence of breast cancer worldwide . contributors vb , db , rp , kp , and gr analysed the data , had full access to the pooled data , wrote the rst draft of the report , and had nal responsibility for the decision to submit ; all are guarantors . 
funding for the contributing studies is described in the publications of those studies . corrections correction to lancet oncol 2012 ; 13 : 569 toh hc , ha tc , wee j . 
this correction has been made to the online version as of may 28 , 2012 , and the printed article is correct . vol 13 june 2012 e231 corrections correction to lancet oncol 2012 ; 13 : 983 , 986 correction to lancet oncol 2012 ; 13 : 1028 correction to lancet oncol 2012 ; 13 : e468 fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 this correction has been made as of oct 29 , 2012 . randomised , chemorefractory jfw , van den smits mlj , nijsen holmium - 166 bosch maaj , et al . 
lancet oncol 2012 ; 13 : 102534in table 1 of this article , the total number of patients with ocular melanoma should have been six , as should the total number of patients with colorectal carcinoma . 
lancet oncol 2012 ; 13 : e468in this news item , the second and third sentences of the second paragraph should have read : median pfs was 94 months ( 95% ci 86167 ) in the combination group compared with 58 months ( 4674 ) in the dabrafenib monotherapy group ( hazard ratio 039 , 95% ci 025062 ; p < 0001 )  . 
 lancet oncol 2012 ; 13 : 106465the rst author of this comment should have been listed as ankit i mehta and his in the a liations section should have been aim . 
these corrections have been made to the online version as of nov 23 , 2012 . initials vol 13 december 2012 e520 erratum fleischhauer k , shaw be , gooley t , et al . 
in the abstract , the rst line of the methods should have read hla and clinical data for unrelated - donor transplantations submitted to the international histocompatibility working group in haemopoietic - cell transplantation were analysed retrospectively . 
in this news article , the rst sentence of the fourth paragraph should have read the researchers found that a daily serving of unprocessed red meat increased the risk of cancer mortality by 10% , whereas a daily serving of processed meat was responsible for a 16% increased risk . 
this correction has been made as of march 26 , 2012 . published online march 26 , 2012 doi : 10.1016 / s14702045 ( 12 ) 70130 - 4 see news page e147 e135 vol 13 april 2012 articles lancet oncol 2012 ; 13 : 114151 published online october 17 , 2012 s1470 - 2045 ( 12 ) 70425 - 4 see comment page 1071 * collaborators listed at end of paper correspondence to : secretariat , cancer epidemiology unit , richard doll building , oxford ox3 7lf , uk collaborations@ceu.ox.ac.uk see online for appendix menarche , menopause , and breast cancer risk : individual participant meta - analysis , including 118 964 women with breast cancer from 117 epidemiological studies collaborative group on hormonal factors in breast cancer * summary background menarche and menopause mark the onset and cessation , respectively , of ovarian activity associated with reproduction , and a ect breast cancer risk . 
our aim was to assess the strengths of their e ects and determine whether they depend on characteristics of the tumours or the a ected women . methods individual data from 117 epidemiological studies , including 118 964 women with invasive breast cancer and 306 091 without the disease , none of whom had used menopausal hormone therapy , were included in the analyses . 
 we calculated adjusted relative risks ( rrs ) associated with menarche and menopause for breast cancer overall , and by tumour histology and by oestrogen receptor expression . findings breast cancer risk increased by a factor of 1050 ( 95% ci 10441057 ; p < 00001 ) for every year younger at menarche , and independently by a smaller amount ( 1029 , 10251032 ; p < 00001 ) , for every year older at menopause . 
 premenopausal women had a greater risk of breast cancer than postmenopausal women of an identical age ( rr at age 4554 years 143 , 133152 , p < 0001 )  . 
all three of these associations were attenuated by increasing adiposity among postmenopausal women , but did not vary materially by womens year of birth , ethnic origin , childbearing history , smoking , alcohol consumption , or hormonal contraceptive use . 
the e ect of menopause in women of an identical age and trends by age at menopause were stronger for oestrogen receptor - positive disease than for oestrogen receptor - negative disease ( p < 001 for both comparisons )  . interpretation the e ects of menarche and menopause on breast cancer risk might not be acting merely by lengthening womens total number of reproductive years . 
 to assess reliably the strengths of these associations and whether they vary by tumour subtype or by characteristics of a ected women requires large numbers , and we address these questions by combining information from more than 100 epidemiological studies . 
combining individual participant data from many studies not only increases statistical power but also permits similar de nitions and similar analytical methods to be used across studies . methods search strategy and selection criteria this collaboration began in 1992 , and has published on breast cancer risk associated with use of hormonal therapies and childbearing practices.14 potentially eli gible epidemiological studies have been sought at regular intervals by computer - aided literature searches , by written communication and discussions with col leagues , and by discussions at scienti c meetings , including collaborators meetings in oxford in 1993 , 1995 , 2000 , 2005 , and 2011 ( appendix p 3 shows search strategy and selection criteria )  . 
so that similar analytical methods could be used across studies , we incorporated cohort studies using a nested case control design , in which up to four controls were selected at random , matched at follow - up to age of the case at cancer diagnosis and , where appropriate , by broad geographical region . 
data for a range of sociodemographic , reproductive , and other behavioural factors , covering the time period to onset of disease for cases and to an equivalent time for controls , were sought from principal investigators ( appendix p 3 )  . vol 13 november 2012 1141 articles we included studies in these analyses if individual data had been provided for womens menopausal status , age at menarche and , if appropriate , age at menopause , and whether or not they had had a hysterectomy or a bilateral oophorectomy . 
women who had had a natural menopause or who had had a bilateral oophorectomy before their natural menopause were classi ed as postmenopausal , but those who had had a hysterectomy without bilateral oophorectomy before their natural menopause were classi ed as being of unknown menopausal status ( because hysterectomy can mask cessation of ovarian activity )  . 
otherwise , we took de nitions used by principal investigators to classify each woman by her age at menarche , menopausal status and , for postmenopasual women , by her age at menopause . 
women with unknown menopausal status or unknown ages at menarche or menopause were excluded from analyses , as were women who had used menopausal hormone therapy , since such use can mask the onset of menopause and a age at menarche 9 10 11 12 13 14 15 16 17 18 19 20 age at menarche ( years ) b age at menopause age at natural menopause ( years ) figure 1 : cumulative distribution of ( a ) age at menarche and ( b ) age at natural menopause data are for women without breast cancerie , controls . 
results for age at menopause are based on data from 157 272 postmenopausal women aged older than 55 years at the time of reporting their age at menopause . modify associations between hormonal factors and breast cancer risk.1 we also sought information about tumour characteristicsie , about oestrogen receptor status and about tumour histology . 
we used information provided by principal investigators to classify tumours as oestrogen receptor - positive or oestrogen receptor - negative , and as ductal , lobular , or of other histology . from reports in previous statistical analysis we did all analyses using conditional logistic regression , similar in principle to the mantel - haenszel strati cation technique used this collaboration.16 when two groups were compared odds ratios ( ors , described as relative risks [ rrs ] when cases and controls are compared ) and standard cis are given . 
 when more than two groups were compared , we estimated variances for every group , treating the ors or rrs as oating absolute risks , 7 because this method enables valid comparisons between any two groups , even if neither is the baseline group . 
this method does not alter risk estimates , but yields variances for each nonbaseline group that are slightly smaller than the variances calculated with conventional methods ( because these include the variance of the baseline group ) and we used these variances to calculate group - speci c cis . 
any comparison between two risk estimates must take the variation in each group into account . analyses of the association between various factors and womens age at menarche and age at menopause were restricted to controls , and we calculated ors stratifying by study , by centre within study , and where appropriate by age at diagnosis ( 20 years , and then in 3 year age groups , 2123 years to 8789 years ) ; by year of birth ( < 1920 , 192029 , 193039 , 194049 , and 1950 ) ; by parity and age when rst child was born ( nulliparous women were a separate stratum and parous women were cross - classi ed by parity [ 12 , 3 ] and age at rst birth [ < 20 years , 2029 years , 30 years ] ) ; by current body - mass index ( bmi ; < 25 kg / m , 2529 kg / m , 30 kg / m ) ; by height ( < 160 cm , 160164 cm , 165 cm ) ; by smoking ( never , past , present ) ; and by alcohol consumption per week ( < 50 g and 50 g )  . 
we restricted analyses comparing breast cancer risk in premenopausal , perimenopausal , and postmenopausal women to women aged 4554 years ( since each category is represented in this narrow age band ) and we used the same strati cations as described above , except that age was strati ed by single years . 
or calculations were strati ed by study and , where appropriate , by age at diagnosis , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi ( results for bmi as a young adult are not strati ed by current bmi )  . 
bmi = body - mass index . vol 13 november 2012 1143 articles a age at menarche study , centre within study , age at diagnosis in single years , and year of birth , and adjusted by parity , age at rst birth , bmi , smoking , and alcohol consumption , also using the same categories as described previously . age at menarche ( years ) < 11 ( 97 ) 11 ( 110 ) 12 ( 120 ) 13 ( 130 ) 14 ( 140 ) 15 ( 150 ) 16 ( 166 ) 5511 / 11 685 119 ( 113125 ) 15 855 / 37 779 109 ( 106112 ) 25 806 / 61 512 107 ( 105109 ) 31 759 / 83 389 100 ( 098102 ) 20 599 / 53 212 098 ( 096100 ) 10 576 / 31 390 092 ( 089095 ) 8858 / 27 124 082 ( 079085 ) b age at menopause age group ( mean , years ) cases / controls ( 95% gs ci ) age group ( mean , years ) cases / controls ( 95% gs ci ) we calculated rrs for breast cancer per 1 year younger at menarche and per 1 year older at menopause by linear regression , using the mean age within each category . 
 signi cance tests for heterogeneity by tumour subtype were based on analyses within cases only ( because controls provide no additional information ) , strati ed by age , study , and bmi and adjusted for other variables listed previously . 
we did our analyses with stata ( version 11 )  . when results for large numbers of subgroups are presented in the gures 99% cis ( or group - speci c 99% cis ) are given , to take account of multiple testing . 
 in the text all cis quoted are 95% cis . role of the funding source the funders had no role in study design , data collection , analysis , or interpretation of data , preparation of the report , or decision to publish . 
all members of the analysis and writing committee ( vb , db , rp , kp , gr ) had access to the raw data and are responsible for the nal submission for publication . results overall 117 studies , together including 118 964 women with breast cancer ( cases ) and 306 091 without the disease ( controls ) , were included in these analyses . 
median age at cancer diagnosis was 54 years ( iqr 4464 )  . figure 1a shows the distribution of age at menarche reported by controlsie , women without breast cancer . 
 their mean age at menarche was 131 years ( sd 17 ) , with almost two - thirds ( 65% , 198 113 of 306 068 ) reporting menarche at ages 12 , 13 , or 14 years . 
only 16% ( 49 464 ) of the controls reported menarche at age 11 years or younger and 19% ( 58 514 ) reported menarche at age 15 years or older . 
having early menarche was associated with many factors known to a ect breast cancer risk , including parity , figure 4 : relative risk of breast cancer ( a ) per year younger at menarche and ( b ) per year older at menopause , in various subgroups and by tumour characteristics relative risks are calculated stratifying by study and age , and where appropriate , by year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi ( results for bmi as a young adult are not strati ed by current bmi )  . 
 * subgroup analyses for age at menarche are for age at menopause < 50 vs 50 years in postmenopausal women ; and for age at menopause are for age at menarche < 13 vs 13 years . 
case - case comparisons strati ed by study , age and year of birth , and adjusted by parity , age at rst birth , smoking , alcohol consumption , height , and current bmi . 
 age at menopause ( years ) < 40 ( 353 ) 4044 ( 419 ) 4549 ( 472 ) 5054 ( 515 ) 55 ( 561 ) 2397 / 7741 067 ( 062073 ) 5516 / 18 544 073 ( 070077 ) 17 336 / 52 040 086 ( 084089 ) 28 197 / 75 944 100 ( 098102 ) 6891 / 16 144 112 ( 107117 ) figure 3 : relative risk of breast cancer by ( a ) age at menarche and ( b ) age at menopause calculated stratifying by study , age , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current body - mass index . 
rrs strati ed by study , age at diagnosis in single years , year of birth , parity , age at rst birth , smoking , alcohol consumption , height , and current bmi . 
 * results for breast cancer risk are plotted against the time between menopause and the diagnosis of breast cancer for postmenopausal women , and against an estimate of that time for premenopausal and perimenopausal women . 
the premenopausal women aged 4554 years in these analyses would be expected to reach their menopause in the next 27 years , on average ( this estimate is based on the age distribution of the premenopausal women in these analyses and the age distribution of womens ages at menopause shown in gure 1b )  . 
perimenopausal women might be expected to reach their menopause in the next 6 months , on average . age at rst birth , height , and bmi ( gure 2a )  . 
associations with late menarche were generally the con verse of associations with an early menarche ( appendix p 7 )  . the younger women were at menarche , the greater was their subsequent risk of breast cancer , the rr increasing by a factor of 1050 ( 95% ci 10441057 , p < 00001 ) for every year younger at menarche ( gure 3a )  . 
results in figure 3a were strati ed by study , age , year of birth , parity and age at rst birth , height , current bmi , smoking , consumption . 
additional adjustment ( either individually or simultaneously ) by ethnic origin , hormonal contraceptive use , and family history of breast cancer , altered the excess rr estimate by less than 1% ( data not shown )  . alcohol and to assess consistency of ndings , we calculated the rr of breast cancer per year younger at menarche for 34 subgroups of women , subdivided by 14 of their personal characteristics : year of birth , age at diagnosis and menopausal status , ethnic origin , parity , age at rst birth , height , bmi as a young adult , current bmi , use of oral contraceptives , smoking , alcohol consumption , family history of breast cancer , menopausal status and , for their age at menopause postmenopausal women , ( gure 4a )  . 
both among premenopausal and among postmenopausal women , increasing bmi seemed to attenuate the relevance of age at menarche , but this attenuation was signi cant only among postmenopausal women ( hetero geneity p = 0006 )  . 
we noted some weakening of the association with age at menarche by attained age in postmenopausal women ( heterogeneity p = 004 ; trend p = 002 ) and family history of breast cancer ( heterogeneity p = 001 ) , but for all other personal characteristics examined heterogeneity across subgroups was not signi cant . 
the ndings were not dominated by the results in any particular study ( appendix pp 810 ) and there was no signi cant heterogeneity in the ndings by study design ( appendix p 6 )  . of the 117 contributing studies , 85 provided some information about tumour characteristics ( appendix pp 45 ) , and gure 4a shows the rrs per year younger at menarche for various tumour subtypes . 
the association with age at menarche was signi cantly stronger for lobular than ductal tumours ( heterogeneity p = 00001 ) , but there were no signi cant di erences by oestrogen receptor status . 
cross - classi cation by both oestrogen receptor status and tumour histology did not show any further interaction ( appendix p 6 )  . figure 1b shows the cumulative distribution of the reported age at natural menopause among postmenopausal controls . 
their mean age at natural menopause was 493 years ( sd 46 ) , with 15% ( 26 285 of 170 413 ) reporting menopause before age 45 years , 75% ( 127 984 ) between the ages 45 and 54 years , and 10% ( 16 144 ) at age 55 years or older . 
associations with an early meno pause were generally the converse of those associated with a late menopause ( appendix p 7 )  . ovarian production of hormones decreases rapidly at around the time of menopause , as is shown in gure 5a , using published data from a cohort study of women who were premenopausal at entry and who had repeated measures of serum oestradiol until after the menopause.8 the short - term e ect of these changes on breast cancer risk can be assessed by restricting analyses to the 31 000 cases and 70 000 controls aged 4554 years ( since pre menopausal , peri menopausal , and postmenopausal women are represented in this age group ) and by stratifying analyses by single years of age ( so that women of identical ages are being compared )  . 
among such women , breast cancer risk was greater among premeno pausal than postmenopausal women ( rr 143 , 95% ci 133152 , p < 00001 ) , with the risk for perimenopausal women being between the other two ( gure 5b ; p < 0001 for all comparisons )  . the consistency of the nding of a greater risk of breast cancer among premenopausal than post menopausal women of the same age was examined across 30 subgroups of women , subdivided by 13 of their characteristics ( appendix p 11 )  . 
this nding re ects , at least in part , known di erences between premenopausal and postmenopausal women in the relation between their current bmi and breast cancer risk , as shown in gure 5c . 
among premenopausal women , those who were overweight or obese ( bmi 25 kg / m ) had a lower risk of breast cancer than leaner women ( bmi < 25 kg / m ) , whereas the reverse was observed among postmenopausal women . 
however , at ages 4554 years , where both premenopausal and postmenopausal women are rep resented , a sudden decrease occurs at menopause in the proportion of oestrogen the proportion of tumours with lobular histology increases with age , with a sudden decrease around the time of menopause . 
after adjusting by single years of age and other potential confounding factors , the heterogeneity at ages and postmenopausal women is highly signi cant both for oestrogen receptor status ( hetero geneity p = 0003 ) and for tumour histology ( heterogeneity p < 00001 , appendix p 11 )  . in analyses restricted to postmenopausal women , the rr of breast cancer increased by a factor of 1029 ( 10251032 , p < 00001 ) for every year older at menopause ( gure 3b )  . 
the ndings in gure 3b were years between premenopausal 4554 b lobular breast cancers age at diagnosis ( years ) figure 6 : breast cancer by tumour characteristics and by womens age and menopausal status ( a ) oestrogen receptor - positive ( er + )  . 
results are shown for age groups < 40 years , 4044 years , 4554 years , 5559 years , 6064 years , and 65 years , and plotted against the mean age of women with breast cancer in each age group . strati ed by study , year of birth , age , parity and age at rst birth , height , current bmi , smoking , and alcohol consumption . 
additional adjustment by ethnic origin , age at menarche , family history of breast cancer , and hormonal contraceptive use ( both individually and simultaneously ) altered the excess rr estimate by less than 1% ( data not shown )  . 
rrs did not di er signi cantly between women with a natural menopause ( 1030 , 10261034 ) and bilateral oophor ectomy ( 1019 , 10041034 , heterogeneity p = 02 ; appendix p 12 )  . the association between age at menopause and breast cancer risk was examined in 30 subgroups and did not vary signi cantly across 11 of the 13 characteristics examined ( gure 4b )  . 
the relation between breast cancer risk and increasing age at vol 13 november 2012 1147 articles menopause was signi cantly greater for oestrogen receptor - positive disease than for oestrogen receptornegative disease ( p = 001 ) , and for lobular than for ductal tumours ( heterogeneity p = 0006 )  . 
the ndings were not dominated by the results in any particular study ( appendix pp 1315 ) and there was no signi cant variation by study design ( appendix p 6 )  . among postmenopausal women , for whom the e ect on breast cancer risk per year younger at menarche can be directly compared to the e ect per year older at menopause , breast cancer risk increased by a signi cantly greater amount per year of menarche than per year of menopause ( 1045 [ 10361054 ] vs 1029 [ 10251032 ] ; heterogeneity p = 0001 )  . discussion this worldwide collaboration has brought together and reanalysed individual participant data for 120 000 women with breast cancer and 300 000 controls without the disease from 117 epidemiological studies in 35 countries ( panel )  . while con rming that early menarche and late menopause increase breast cancer risk , we showed that these e ects were not equivalent , in that the excess risk panel : research in context systematic review the collaborative group on hormonal factors in breast cancer began in 1992 . 
since then published literature on epidemiological studies of breast cancer has been identi ed using electronic searches ( medline , embase , and pubmed , 19982011 ; using combinations of the search terms breast cancer , risk , epidem * , and hormones ) , supplemented by hand searching in review articles . 
eligible studies needed to have obtained individual information about reproductive factors and about use of hormonal therapies , from at least 400 women with breast cancer and similar information from controls without the disease . 
studies that had obtained relevant data , but had not published any results for breast cancer were sought by correspondence with colleagues , by discussions at collaborators meetings , and by electronic searches using additional terms cohort , prospective , women , and cancer risk . 117 eligible studies were included and principal investigators contributed information about almost 120 000 women with breast cancer who had never used menopausal hormonal therapies to this individual - participant meta - analysis . 
we report on the relation between menarche and menopause and breast cancer risk , overall , and by oestrogen receptor status and by histological subtypes of the tumours , adjusting for possible confounding factors . 
subgroup results are also shown by various sociodemographic and personal characteristics , including year of birth , ethnic origin , parity , age at rst birth , smoking , alcohol consumption , and body - mass index . interpretation breast cancer risk increased by a signi cantly greater factor for every year younger at menarche than for every year older at menopause , indicating that menarche and menopause may not a ect breast cancer risk merely by extending womens total reproductive years . 
endogenous ovarian hormones are more relevant for oestrogen receptor - positive disease than for oestrogen receptor - negative disease and for lobular than for ductal tumours . associated with lengthening womens reproductive years by one year at menarche was greater than the excess associated with one years lengthening at menopause . 
 we also found that oestrogen receptor - positive and lobular breast cancers are strongly a ected by womens menopausal status , and by their age . the production of steroid hormones by the ovary begins at around the time of menarche and decreases rapidly at around the time of menopause . 
 by restricting analyses to the 31 000 women with breast cancer in this narrow age range and stratifying by single years of age ( and by other potential confounding factors ) , valid comparisons can be made of the short - term e ect of the menopause , and breast cancer risk was about 40% higher in premenopausal than in postmenopausal women of the same age . 
since the postmenopausal women had reached their menopause only an average 46 years previously , the ndings indicate a rapid decline in breast cancer risk in women of identical ages soon after menopause . 
this nding probably explains the attening of the age - incidence curve at around age 50 years , the so - called clemmesens hook , 9 frequently observed in populations before the widespread use of hormonal therapies and screening . there is accumulating evidence that oestrogen receptorpositive and lobular breast cancers are more sensitive to ovarian hormones than are oestrogen receptor - negative and ductal cancers . 
not only are oestrogen receptorpositive and lobular tumours strongly a ected by the menopause , as we have shown , but postmenopausal women who use hormone therapy have a greater increase in oestrogen receptor - positive than oestrogen receptornegative tumours and in lobular than ductal breast cancers.10 , 11 furthermore , oestrogen - blocking treatments improve survival for oestrogen receptor - positive , but not for oestrogen receptor - negative breast cancer.12 womens adiposity was consistently shown to attenuate associations between menopause and breast cancer risk . 
 circulating oestradiol concentrations increase as postmenopausal womens bmi increases.13 that the rr of breast cancer risk falls more rapidly after the menopause in lean than in overweight and obese women is likely to re ect , at least in part , di erences in oestradiol concentrations between such women . 
oestradiol concentrations in postmenopausal women are greater the younger they were at menarche , 14 and this might , in part , account for the associations recorded between age at menarche and breast cancer risk . although a womans age at menarche does not coincide precisely with the onset of breast development , the two are highly correlated.15 breast cancer is almost unknown before menarche and extremely rare soon afterwards , making it e ectively impossible to study the short - term e ects of the hormonal changes associated with menarche by comparing breast cancer risk in women of identical ages before and soon after menarche . 1148 vol 13 november 2012 articles these ndings con rm that young age at menarche and old age at menopause increase breast cancer risk . 
many factors known to a ect breast cancer risk , including childbearing patterns , height , and bmi , are also associated both with womens age at menarche and with their age at menopause . 
to ensure as much comparability as possible between women with breast cancer and controls , and thus to minimise potential confounding , analyses were strati ed by these factors , and by study , age , year of birth , smoking , and alcohol consumption . 
the associations did not vary materially by womens personal characteristics , other than bmi among postmenopausal women . this meta - analysis of individual - participant data includes almost all available epidemiological evidence for the association between menarche and menopause and breast cancer risk . 
single studies do not have su cient power to examine these asso ciations in detail , so reviews based solely on the limited published evidence could well be susceptible to publication bias . 
although availability of information about oestrogen receptor status varied substantially over time , with most studies done before 1990 contributing relatively little information , analyses of all available data combined were su ciently powered to describe asso ciations separately within both oestrogen receptor - positive receptor - negative disease . 
another important advantage of this metaanalysis is that it seeks to review both published and unpublished ndings , thus avoiding unduly selective emphasis on published results or on only some studies . oestrogen and women included in these analyses generally reported their ages at menarche and at menopause many years after the events had occurred . 
comparisons of information recorded at around the time of menarche and menopause with that recalled many years later has shown substantial regression to the mean over time , especially for recalled age at menarche , 1623 which would dilute estimates of rr.23 , 24 the slight attenuation in the estimated rr with attained age thus relects , at least in part , misclassi cation of recalled ages at menarche and , to a lesser extent , of recalled age at menopause . 
 since sig ni cant associations were recorded at all ages , it is reasonable to conclude that the e ects of age at menarche and age at menopause on breast cancer risk persist throughout life . since the e ect on breast cancer risk of 1 year younger at menarche is signi cantly greater than that of 1 year older at menopause , these ndings suggest that the e ects of each may not be acting merely by lengthening the total duration of womens reproductive years . 
in most populations womens average age at menarche has been declining in successive birth cohorts , 25 contributing to increasing incidence of breast cancer worldwide . contributors vb , db , rp , kp , and gr analysed the data , had full access to the pooled data , wrote the rst draft of the report , and had nal responsibility for the decision to submit ; all are guarantors . 
this prospective study aimed to validate reported associations between genotype and radiation toxicity in a large independent dataset . methods 92 ( of 98 attempted ) snps in 46 genes were successfully genotyped in 1613 patients : 976 received adjuvant breast radiotherapy in the cambridge breast imrt trial ( isrctn21474421 , n = 942 ) or in a prospective study of breast toxicity at the christie hospital , manchester , uk ( n = 34 )  . 
a further 637 received radical prostate radiotherapy in the mrc rt01 multicentre trial ( isrctn47772397 , n = 224 ) or in the conventional or hypofractionated high dose intensity modulated radiotherapy for prostate cancer ( chhip ) trial ( isrctn97182923 , n = 413 )  . 
at a type i error rate adjusted for multiple testing , this study had 99% power to detect a snp , with minor allele frequency of 035 , associated with a per allele odds ratio of 22 . findings none of the previously reported associations were con rmed by this study , after adjustment for multiple comparisons . 
the p value distribution of the snps tested against overall toxicity score was not di erent from that expected by chance . interpretation we did not replicate previously reported late toxicity associations , suggesting that we can essentially exclude the hypothesis that published snps individually exert a clinically relevant e ect . 
continued recruitment of patients into studies within the radio genomics consortium is essential so that su ciently powered studies can be done and methodological challenges addressed . funding cancer research uk , the royal college of radiologists , addenbrookes charitable trust , breast cancer campaign , cambridge national institute of health research ( nihr ) biomedical research centre , experimental cancer medicine centre , east midlands innovation , the national cancer institute , joseph mitchell trust , royal marsden nhs foundation trust , institute of cancer research nihr biomedical research centre for cancer . introduction late side - e ects from radiotherapy are often irreversible , can decrease health - related quality of life , and limit treatment intensity in radical radiotherapy regimens . 
 quanti cation of late toxicity is therefore crucial in assessment of the therapeutic bene t of radiotherapy , and recommendations for its reporting have been made.1 , 2 if the hypothesis that there is a sizeable subpopulation of patients who have a signi cantly increased risk of developing toxicity proves correct , it is likely that this subset of cases currently limits our ability to maximise toxicity - free local control through higher doses of radiation the remaining cases . 
the rapper ( radiogenomics : assessment of polymorphisms for predicting the e ects of radiotherapy ) study was designed to identify common genetic variation associated with the development of late radiation toxicity3 as a rst step in the process of identifying such a subset of toxicityprone patients . apart from one small genome - wide study , 4 single nucleotide polymorphism ( snp ) association studies of radiotherapy toxicity published to date have used a candidate gene approach . 
the focus of candidate gene studies has thus been on genes involved in dna damage recognition and repair ( eg , atm , brca1 , brca2 , and tp53 ) , free radical scavenging ( eg , sod2 ) , and anti - in ammatory response ( eg , tgfb1 )  . 
no individual snp or combined risk snp signature914 has yet been validated as a risk factor for radiation toxicity . we aimed to con rm reported associations between candidate snps or snp signatures and radiation toxicity in a large , well powered prospective study of patients with breast and prostate cancer . methods patients 1613 patients from four studies were included in this analysis . 
treatment was given according to the component study protocols and details were recorded for all patients . into the cambridge breast imrt samples were obtained from 942 of 1145 women recruited trial ( isrctn21474421 ) who underwent conservative surgery followed by adjuvant radiotherapy.15 in this study , patients with signi cant dose inhomogeneities , de ned by a volume of 2 cm or more exceeding 107% of the prescribed dose , were randomly assigned to receive either standard breast radiotherapy ( control ) or a straightforward method of forward - planned intensity modulated radiotherapy ( imrt ; intervention )  . 
34 samples were from patients enrolled in a prospective study of breast toxicity in women who received conservative surgery and adjuvant radiotherapy at the christie hospital ( manchester , uk )  . 
 blood samples were also obtained for 224 of the 843 patients with localised prostate cancer randomly assigned trial ( isrctn47772397 ) to standard - dose or escalated - dose the mrc rt01 multi - centre ( chhip ) conformal radiotherapy after neoadjuvant androgen suppression.1618 at the time of initial analysis in june , 2009 , for the study we report here , 647 patients had been recruited to both the conventional or hypo fractionated high dose intensity modulated radiotherapy for prostate the cancer rapper study , and 2 - year toxicity data were available for analysis for 413 patients . 
chhip patients with localised prostate cancer underwent imrt after neoadjuvant androgen suppression and were randomly assigned to one of three dose schedules.19 recruitment to both the chhip and rapper studies was ongoing at the date of data release . ( isrctn97182923 ) and trial the rapper study ( ukcrn1471 ) reported here is a large uk sample collection study , opened in 2005 , which recruits patients from clinical trials and other well designed studies . 
all patients in the cambridge imrt and manchester prospective trials were o ered recruitment to rapper when they enrolled in the component study ; blood samples were taken for rapper before radiotherapy . 
 patients recruited to the mrc rt01 trial and under continuing follow - up in 2005 were o ered participation in the rapper study at a follow - up appointment ; blood samples were therefore taken at least 2 years after the start of their radiotherapy . 
the distribution of toxicity in patients recruited to rt01 but not rapper was broadly similar to that seen in patients recruited to both rt01 and rapper ( data not shown )  . 
rapper is approved by the cambridgeshire 862 patients registered to rt01 trial 1145 patients recruited to cambridge imrt trial and underwent 3d imaging and dosimetry calculated with standard breast pain ongoing recruitment to manchester prospective toxicity study ongoing recruitment to chhip and rapper studies , data release june 17 , 2009 dosimetry adequate dose inhomogeneity 843 randomised 814 randomised * randomised 422 high dose ( 74 gy / 37 f ) 421 standard dose ( 64 gy / 32 f ) 410 allocated imrt ( intervention ; 40 gy / 15 f ) 44 standard radiotherapy ( 40 gy / 15 f ) 74 gy / 37 f 60 gy / 20 f 57 gy / 19 f 330 patients ineligible for randomisation : standard radiotherapy ( 40 gy / 15 f ) 404 allocated standard radiotherapy ( control ; 40 gy / 15 f ) 117 recruited to rapper 115 recruited to rapper 304 recruited to rapper 368 recruited to rapper 381 recruited to rapper 44 recruited to rapper 209 recruited to rapper 134 recruited to rapper 151 recruited to rapper 114 toxicity data available 110 toxicity data available 263 toxicity data available 335 toxicity data available 344 toxicity data available 34 toxicity data available 128 toxicity data available 134 toxicity data available 151 toxicity data available figure 1 : trial pro le imrt = intensity modulated radiotherapy . 
 * one patient was not randomised because the standard plan was unacceptable , owing to a signi cant region of low dose , so imrt was prescribed ; patient was withdrawn from the late toxicity analysis . 
in patients with breast cancer , body - mass index , use of tamoxifen and chemotherapy , breast boost , breast volume , ethnic origin , cardiovascular disease , and cosmesis after surgery were also recorded . 
in patients with prostate cancer , data for hypertension , previous surgery , clinical stage , risk of seminal vesicle involvement , prescribed dose , and baseline symptoms were also documented . toxicity was recorded with standardised scoring systems ; the scales and incidence of each toxicity endpoint used ( acute and late toxicity ) are shown in appendix 1 . 
an e ect of poor surgical cosmesis on clinical assessment of breast shrinkage or induration at 2 years has been reported for patients in the imrt trial ; 15 thus , endpoints that accurately re ect late toxicity , due to radiotherapy rather than surgery , were used ( appendix 1 )  . 
details of the methods used are available elsewhere.15 four urinary endpoints for patients with prostate cancer , ve rectal ( bleeding , proctitis , sphincter control , stool frequency , tenesmus ) and ( frequency , nocturia , incontinence , and decreased stream ) were chosen to represent the range of rectal and bladder toxicity reported by patients 2 years after radiotherapy to the prostate . 
the rectal endpoints have previously shown a dose - volume response for at least one dose level with the volume of rectum receiving between 30 gy and 70 gy expressed as a percentage of the total rectal volume.20 sexual dysfunction was not analysed because few men had adequate , selfreported , erectile function at baseline before hormone therapy was commenced.21 the symptoms of late toxicity after radiotherapy to the pelvis are non - speci c and might be present before treatment . 
we took the e ect of baseline function into account by calculating changes in scores from baseline ( pre - hormone treatment ) to those recorded at 2 years for each endpoint22 ( appendix 1 )  . 
if the nal symptom score was zero , then change in toxicity was also scored as zero if the pre - hormone or pre - radiotherapy scores were not recorded . 
desc = permissible dose escalation in non - carriers to maintain isotoxicity with unselected population . table 1 : e ect sizes , quanti ed as the or between carriers and non - carriers that can be resolved with 99% power and a nominal of 2710 scores to measure overall acute toxicity in patients with breast cancer and , by combining acute bladder and bowel toxicity , in those with prostate cancer . 
for an individual patient ( k ) , a standardised z score , zk , i , was derived for each toxicity endpoint ( i ) for which that patient had a valid ( non - missing ) score , sk , i : zk , i = ( sk , imeani ) / sdi , where meani and standard deviation ( sdi ) were taken over all cases in the study population for which toxicity data were available . 
 conversion of individual toxicity scores to z scores eliminated the problem of grades for one toxicity item not being directly comparable with grades for another ite z scores de ned , for a particular endpoint , whether a patients score was high or low relative to the distribution of the scores of other patients in the population . 
the stat score for patient k , statk , was the average of all nonmissing z scores for that patient : statk = mean zk , i . to select snps , we undertook a comprehensive literature search of medline and pubmed databases using the keywords radiotherapy , radiation , toxicity , adverse e ects , genetic variation , and poly morphis this search identi ed 69 in - vitro or in - vivo studies published up to dec 31 , 2009 . 
 additionally , we examined the most frequently studied genes , atm , tgfb1 , xrcc1 , xrcc3 , and hif1a , in more detail by choosing a set of tag snps to capture all common genetic variation in these ve genes with r greater than 08.24 six new candidate snps were also selected : two in atm ( rs1800054 , rs4986761 ) reported to be associated with breast cancer susceptibility ; two in mre11 ( rs569143 , rs2155209 ) reported to be associated with breast and bladder cancer susceptibility ; and rs1800734 in mlh1 and rs2303428 in msh2 , reported to be associated with acute myeloid leukaemia after chemotherapy . 
dna was genotyped for 95 snps with the fluidigm high - throughput platform and fluidigm 96.96 dynamic arrays according the manufacturers instructions and read with the fluidigm ep1 ( fluidigm corporation , san francisco , ca , usa )  . 
genotypes were automatically called with the biomark genotyping analysis software ( version 2.1.1 ) , but all cluster plots were also checked manually and adjusted as necessary . six snp assays failed quality control on the fluidigm system and so these , as well as three snps chosen later , were genotyped with the taqman 7900ht sequence detection system ( applied biosystems , warrington , uk )  . 
primer and probe details are available on request . for both fluidigm and taqman genotyping , 5% of all samples were duplicated as a reproducibility control and negative controls were also included on all plates . 
three snps ( rs3957356 , rs1805389 , and rs2333227 ) failed quality control on both platforms and genotype distributions of a further three deviated from those expected under hardyweinberg equilibrium with the bonferroni correction for multiple testing ( p < 000051 ) and so were excluded from further analysis ( rs2284999 , rs2293036 , rs4899056 )  . 
multivariable analysis of overall and individual endpoints of toxicity included all covariates , identi ed from univariate analyses , with p values of less than 005 ( appendix 1 ) .22 , 23 , 25 many of these factors are known to be associated with toxicity , but are unlikely to be confounders of any genotype - toxicity association . 
in genetics , a confounding variable is genetically determined and could lead to spurious associations with a phenotype eg , genetic variation associated with large breast size leading to a large volume of normal tissue irradiated and so increased toxicity . 
after multivariable analysis , residuals were calculated for each patient to quantify the toxicity not accounted for by available patient - related and treatment - related factors.23 , 26 patients with residuals of zero had toxicity entirely accounted for by the available patient - related and doserelated factors . 
for snps that were signi cantly associated with a particular toxicity endpoint , the endpoint was dichotomised to obtain a more clinically interpretable per - allele odds ratio ( or )  . a bonferroni correction was made to adjust for the e ects of multiple testing ; the nominal signi cance threshold ( p = 005 ) was divided by the number of tests done ( 92 snps20 endpoints ) to give a signi cance threshold of p = 2710 . 
q - q plots were created to assess the distribution of the 92 test statistics from that expected under the null hypothesis that no snp was associated with late radiotherapy toxicity . we undertook power calculations by specifying di erences to be detected between genotypes in the mean vol 13 january 2012 articles 102 101 102 101 of the toxicity endpoint and adjusting for groups of unequal size according to minor allele frequency ( maf ; appendix 1 )  . 
power of 99% and a type i error rate ( p value ) of 2710 were selected to reduce risk of false - negative and false - positive associations , respectively , and the detectable e ect sizes ( ors ) were estimated with stplan software ( version 4.3 ) downloaded from the department of biostatistics at the md anderson cancer center ( houston , tx , usa ; table 1 )  . 
if the incidence of toxicity in non - carriers ( p0 ) is assumed to be 20% , the incidence of toxicity in carriers ( pc ) will depend on the e ect size of that allele . 
 to estimate the clinical relevance of the detectable e ects , a hypothetical scenario was considered in which the snp was used to identify sensitive individuals and escalate the dose in the remaining , relatively more resistant , cases . 
 the permis sible dose escalation ( desc ) that would result in the same incidence of toxicity in the non - carriers as would be seen in the unselected population was calculated . 
to this end , a logistic doseresponse curve with a steepness of 50 = 3 was assumedie , at the steepest part of the doseresponse curve , corresponding to a 50% response level , there would be a 3% increase in response in percentage points for a 1% increase in dose , a typical value for late normal tissue e ects ( appendix 1 ) .27 the value at the 20% response level is 17.28 using this value and the di erence between p and p0 , we calculated desc using a linear approximation to the doseresponse curve . 
 this approximation was deemed adequate over the fairly narrow range of response probabilities considered . role of the funding source the funding sources had no role in the design of the study , collection , analysis , interpretation of the data , writing of the report , or in the decision to submit for publication . 
gcb had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results 66 snps previously reported to be associated with radiotherapy toxicity , either clinically or in in - vitro assays , 914 , 2968 were selected along with an additional 28 snps in atm , tgfb1 , xrcc1 , xrcc3 , and hif1a as tagging snps , designed to capture all common genetic variation within these genes , or because of evidence for direct functionality ( table 2 )  . 
appendix 2 shows the unadjusted results from regression analysis of all 92 analysed snps in 46 genes against all endpoints . some genetic variants , depending on their action , are likely to a ect toxicity in both breast and prostate cancer . 
in the combined cancer site analysis , we sought any such variants rst , using the stat score of overall late toxicity in the o o o oooooo oooooooooooooooooooooooooooooooooooooo o o o o o o oooooo ooooooooooooooooooooooooooooooooooooooo expected expected distribution : 2 ( 1 df ) figure 2 : q - q plots showing p values ( and corresponding values ) obtained from ( a ) univariate and ( b ) multivariable analyses of overall toxicity against genotype at the 92 snps the solid lines represent the identity line ( x = y )  . 
a quantile - quantile or q - q plot is obtained by ordering the p values obtained from association tests and plotting them against that which would be expected from chance alone . 
deviation from the identity line ( x = y ) at the tail of the distribution suggests deviation from the null distribution ( that expected under the null hypothesis that no snp is associated with the trait ) and the presence of true association . 
snps not in hapmap and therefore the linkage disequilibrium with snps genotypes in the present study could not be calculated ; xrcc1 and xrcc3 genes tagged completely in present study . 
the or ( per additional risk allele ) was 184 ( 95% ci 126270 ) for any increase in urinary frequency . if we attempt to con rm only snp associations with previously reported endpoints , a less stringent bonferroni correction threshold could be deemed appropriate . 
in this analysis , 196 tests were done because many of the previous studies looked at non - speci c outcomes , such as early or late adverse radiotherapy reaction , and therefore the threshold for signi cance after a bonferroni correction was 2610 . 
a few borderline signi cant associations were identi ed , but none reached this p - value threshold : the rad21 snp rs105083811 , 67 and sod2 snp rs488011 have previously been reported to be associated with severe radiosensitivity in various tumour types and were respectively associated with urinary incontinence ( p = 002 ) and proctitis ( p = 003 )  . 
xrcc1 snps rs1799782 and rs25487 were reported as being associated with adverse reactions to radiotherapy66 and here were associated with altered pigmentation ( p = 003 ) and telangiectasia ( p = 001 )  . where possible , we tested the associations of previously reported snp signatures , but not all the snps within such signatures were successfully genotyped in this study . 
we were unable to con rm association of increased toxicity with increasing number of risk alleles for any of the previously published signatures ( table 3 )  . discussion none of the previous reports of signi cant associations between radiation toxicity and snps in candidate genes have been con rmed with appropriate levels of con dence within the design and sample size of our study ( panel )  . 
the q - q plots show that there are no more signi cant associations among the 92 snps tested for overall late e ects than would have been expected by chance . 
this nding is despite the fact that all the variants had already been reported as signi cantly associated with radiotherapy toxicity or otherwise judged to have a high previous probability of involvement . 
our ndings suggest that the published literature on this subject is dominated by false - positive associations due to small sample sizes , multiple testing , and the absence of rigorous independent validation attempts in the original studies . for ve genes thought to be particularly good candidates ( atm , tgfb1 , xrcc1 , xrcc3 , and hif1a ) , we not only re - examined the previously reported snps but also examined a more comprehensive set of tag snps designed to represent all the known common variants ( maf > 005 ) within the genomic footprint of each gene . 
rs1801516 had previously been reported to be associated with several e ects including adverse radiotherapy reaction according to for research and rtog / european organisation treatment of cancer ( eortc ) , 36 late toxicity according to rtog , 38 severe radiation - induced sequelae ( common terminology criteria for adverse events version 3.0 grade 3 ) , 11 in - vitro clonogenic survival fraction , 69 and development of telangiectasia.34 it has been reported as a breast cancer susceptibility allele , 37 although not con rmed in subsequent studies.70 in view of this additional background , the association we noted could be a true - positive association . 
the relation between heterozygous truncating mutations in atm and radiosensitivity remains equivocal . a possible limitation of our study was our necessary reliance on 2 - year follow - up toxicity data in this still maturing study . 
normal tissue reactions , such as induration and telangiectasia , develop gradually after a latency period over many years.71 , 72 although there is evidence that late e ects at 2 years are predictive of those at 5 years , 73 we might not have detected the full severity of developing late toxicity in some patients . 
the only genome - wide association study undertaken so far into late toxicity from radiotherapy has reported an association that reached genome - wide panel : research in context systematic review we undertook a comprehensive search of medline and pubmed databases using the keywords radiotherapy , radiation , toxicity , adverse e ects , genetic variation , and polymorphisthis search identi ed 69 in - vitro or in - vivo studies published up to dec 31 , 2009 . 
studies to date have been underpowered , including fewer than 500 samples , have tested many single nucleotide polymorphisms without adjusting for multiple comparisons , and ndings have proved di cult to replicate.68 interpretation our failure to replicate the associations of most variants reported from candidate gene studies suggests that common variation in the genes studied is increasingly unlikely to be clinically important in determining individual variation in response to radiotherapy . signi cance between snp rs2268363 in the folliclestimulating hormone receptor gene ( fshr ; involved in testes development and spermatogenesis ) and erectile dysfunction in a small cohort of african american men.4 collaborations developed through the radiogenomics consortium are enabling replication studies to be done.74 , 75 we have aimed to minimise both false - positive and false - negative ndings in this validation study , since the need for multiple testing was generally ignored in the original hypothesis - generating studies . 
however , use of such a stringent p value is justi ed ; as table 1 shows , even with this conservative bonferroni correction , we have enough power to detect clinically relevant ors . if a bonferroni correction is made , the actual p value chosen to represent statistical signi cance can vary slightly according to estimates of the degree of correlation between the multiple hypotheses tested . 
the probability that we are actually interested in is the probability that the null hypothesis is true given the data , 76 which depends on the p value , the power of the study to detect the e ect , and the previous probability the null hypothesis is true . 
this estimate assumes there are 10 million snps in the human genome ; results from other vol 13 january 2012 articles genome - wide association studies suggest no more than 50 snps would be expected to account for 1% of the phenotypic variance with detectable e ect sizes and the previous probability is doubled for candidate gene selection . 
also , many of the previously reported endpoints were either nonspeci ceg , early or late adverse radiotherapy reaction according to rtog / eortc36or were in - vitro tests of radiosensitivity , which did not provide an e ect size to be tested here , and so we felt a form of correction was necessary . 
however , with increasing rarity of these radiosensitive cases , the clinical bene t of their removal from the risk set tends to zeroie , identi cation of such rare variants in a hypothetical subgroup is likely to be increasingly irrelevant for the treatment deliverable to most patients . 
table 1 shows that , if carriers of a snp with a maf of 5% associated with an increase in toxicity from 20% to 552% ( equal to an or of 49 ) could be advised not to receive radiotherapy , this approach would only allow an increase in dose to the remaining patients of 05 gy if we aim for isotoxicity in the non - carriers . 
 therefore we can essentially exclude the hypothesis that published snps individually exert a clinically relevant e ect . our failure to con rm ndings of candidate gene studies is by no means unprecedented in the eld of genetic studies ; in fact , this situation has been the norm for most candidate gene studies of cancer susceptibility . 
 before the development of genome - wide association studies , more than 500 snps were examined in more than 100 candidate genes for breast cancer susceptibility ; 77 many of those genes were examined in our study . 
none those associations were con rmed , although subsequently more than 30 genetic loci with unequivocal e ects on breast cancer risk have been identi ed and are continuing to be discovered through ever larger genomewide association studies.7880 a few of these loci lie close to genes that had already been considered in candidate studies ( eg , 8q24 upstream of myc , 6q25 upstream of esr1 , and 11q upstream of ccnd1 ) and are likely to be regulatory regions for these genes . 
genome - wide association studies have served to emphasise the poverty of our understanding of the biological basis of most complex traits and diseases and one of the earliest advances to come from this new technology will be the recognition of new biochemical pathways , and hence drug targets , for these traits . despite the failure to validate previously identi ed genetic determinants of radiotoxicity in our study , there remains evidence that genetic variation might account for a proportion of the patient - to - patient variability in response to radiation therapy . 
several recent studies have shown that chromosomal radiosensitivity of lymphocytes is largely determined by genetic factors.8185 rare radiosensitivity syndromes , such as ataxia telangi ectasia , certainly a ect radiosensitivity in individual mutation carriers , but the prevalence of such mutations is so low that they have little e ect on radiosensitivity in most patients with cancer . the ultimate goal of radiogenomics is to develop a genetic risk pro le including many snps for individualisation of radiation dose prescriptions to optimise tumour control while minimising normal tissue damage . 
 importantly , there is interest in identi cation of both individuals with low and those with high risk of toxicity , and there is no conceptual di erence between the two . 
 for example , if one allele of a polymorphic genetic locus is associated with a high risk of toxicity , by de nition the other allele can be regarded as a non - toxicity allele . 
 development of genetic risk pro les could , therefore , stratify patients into subgroups with di erent probabilities of developing toxicity ; this approach would allow individualised dose prescription , to increase survival and decrease the morbidity associated with cancer . 
the rst stage in development of such a pro le is to identify genetic variants that are unequivocally associated with di erences in radiation toxicity , even if their individual e ect size is small . 
the establishment of the radiogenomics consort ium in 2009 should provide a route to not only undertake large , su ciently powered studies , but also to address meth odological challenges associated with radiogenomics.74 , 75 the rapper study is continuing and a stage 1 genomewide analysis of stat score and individual late toxicity endpoints has been done . 
ultimately , the top 510% of snps showing the most signi cant association with toxicity will be genotyped across the radiogenomics consortium and included in a meta - analysis with other similar genome - wide association studies . in conclusion , our failure to replicate the associations of most variants reported from candidate gene studies suggests that common variation in the genes studied is increasingly unlikely to be important in determining individual variation in response to radiotherapy . 
we cannot yet exclude a role for variants in these genes with very low maf or small e ects , both of which would limit the clinical importance of these associations . vol 13 january 2012 articles contributors gcb , cmlw , ngb , pdpp , and amd were involved in the conception and design of the study . 
all authors were involved in writing or critical review of the draft report and all approved the nal version . con icts of interest we declare that we have no con icts of interest . acknowledgments we thank john barnett for help in preparation and proofreading of the article and kristy driver for help with database management . 
 moreover , comparison of visual scores assessments with of the pten reaction product histological slides can show important discrepancies.6 thus , pten score values estimated by an observer should not be used as a simpli ed surrogate computerised optical density for measurement . 
a computer - assisted reassessment of the stained sections used by obyrne and colleagues , 1 followed by survival models based on continuous data for pten expression , would give more reliable results . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata kreimer ar , gonzlez p , katki ha , et al , for the cvt vaccine group . 
e cacy of a bivalent hpv 16 / 18 vaccine against anal hpv 16 / 18 infection among young women : a nested analysis within the costa rica vaccine trial . 
 lancet oncol 2011 ; 12 : 86270in the trial pro le of this study , virgins who were excluded from the restricted cohort were wrongly classi ed as missing cervical dna results . 
in the results section , the follow - up time for the hpv group should have been 542 months ( range 470748 ) and for the control group 542 months ( range 470744 ) , with a median follow - up time of 542 months and a p value for di erence by arm of 0975 . 
lancet oncol 2011 ; 12 : 98889contrary to the statement made in this comment , we have been subsequently alerted to the fact that translational studies associated with sch ski and colleagues trial had been undertaken but are not yet published . 1096 vol 12 november 2011 corrections correction to lancet oncol 2012 ; 13 : 1045 woll pj , reichardt p , le cesne a , et al , for the eortc soft tissue and bone sarcoma group and the ncic clinical trials group sarcoma disease site committee . 
lancet oncol 2012 ; 13 : 104554in this article ( published online sept 4 , 2012 ) , in gure 5 , the total number of events in the control group should have been 499 . 
we investigated whether erlotinib improves clinical outcome in these patients . methods topical was a double - blind , randomised , placebo - controlled , phase 3 trial , done at 78 centres in the uk . 
 eligibility criteria were newly diagnosed , pathologically con rmed nsclc ; stage iiib or iv ; chemotherapy naive ; no symptomatic brain metastases ; deemed unsuitable for chemotherapy because of poor ( 2 ) eastern cooperative oncology group performance status or presence of several comorbidities , or both ; and estimated life expectancy of at least 8 weeks . 
patients were randomly assigned ( by phone call , in a 1 : 1 ratio , strati ed by disease stage , performance status , smoking history , and centre , block size 10 ) to receive oral placebo or erlotinib ( 150 mg per day ) until disease progression or unacceptable toxicity . 
this study is registered , number isrctn 77383050 . findings between april 14 , 2005 , and april 1 , 2009 , we randomly assigned 350 patients to receive erlotinib and 320 to receive placebo . 
657 patients died ; median overall survival did not di er between groups ( erlotinib , 37 months , 95% ci 3242 , vs placebo , 36 months , 3239 ; unadjusted hazard ratio [ hr ] 094 , 95% ci 081110 , p = 046 )  . 
59% ( 178 of 302 ) of patients assigned erlotinib and who were assessable at 1 month developed rst - cycle rash , which was the only independent factor associated with overall survival . 
 compared with placebo , overall survival seemed to be worse in the group that did not develop rst - cycle rash ( 130 , 105161 , p = 0017 )  . 
grade 3 or 4 diarrhoea was more common with erlotinib than placebo ( 8% [ 28 of 334 ] vs 1% [ four of 313 ] , p = 00001 ) , as was high - grade rash ( 23% [ 79 of 334 ] vs 2% [ ve of 313 ] , p < 00001 ) ; other adverse events were much the same between groups . interpretation patients with nsclc who are deemed unsuitable for chemotherapy could be given erlotinib . 
patients who develop a rst - cycle rash should continue to receive erlotinib , whereas those who do not have a rash after 28 days should discontinue erlotinib , because of the possibility of decreased survival . fundingcancer research uk , roche . introduction lung cancer , the main cause of cancer - related death , accounts for nearly 14 million deaths worldwide every year , and has an annual incidence of more than 41 000 in the uk ( age standardised incidence of 48 per 100 000 ) .1 mortality from lung cancer accounts for more than 452 000 deaths in china , 342 000 in europe , and 162 000 in the usa.1 the number of lung - cancer deaths in developing countries is expected to increase during the next few decades such that by 2030 about 70% of tobacco - related deaths will occur in these countries . 
however , most patients with advanced or metastatic nsclc are elderly ( median age 72 years2 ) and many receive only active supportive care , including palliative radiotherapy , because of physician choice , poor performance status , or presence of several comorbidities.2 , 3 therefore , despite the recom mendation to treat these patients with platinum - based chemo therapy , only about 25% of elderly ( age > 65 years ) us patients3 and 29% of newly diagnosed uk patients2 currently receive any cytotoxic treatment . erlotinib is an oral egfr inhibitor that is associated with a signi cant survival bene t among patients with nsclc when used as maintenance monotherapy after rst - line chemotherapy or as second - line or third - line monotherapy.46 in chemotherapy - naive patients with vol 13 november 2012 1161 articles activating egfr mutations , erlotinib signi cantly improved progression - free survival compared with chemotherapy.7 , 8 we did a large randomised trial to determine whether erlotinib monotherapy would be bene cial as rst - line therapy in unselected patients with advanced nsclc deemed unsuitable for chemotherapy . methods study design and participants topical was a superiority phase 3 , double - blind , randomised , placebo - controlled trial . 
eligibility criteria were newly diagnosed , pathologically con rmed nsclc ; stage iiib or iv disease ; chemotherapy naive ; no symptomatic brain metastases ; deemed unsuitable for chemotherapy because of poor eastern cooperative oncology group ( ecog ) performance status ( ps 2 ) or presence of several comorbidities ( including impaired renal function with creatinine clearance < 60 ml / min ) , or both ; and estimated life expectancy of at least 8 weeks . 
other inclusion criteria were age older than 18 years , diagnosis within the past 62 days , able to take oral medication , and using e ective contraception if appropriate . 
exclusion criteria were previous treatment with any biological anticancer therapy ; previous palliative radiotherapy ( except to bone metastases , within the previous 2 weeks ) ; pregnant or lactating women ; evidence of signi cant laboratory nding or concurrent uncontrolled medical illness judged to 670 patients randomised 350 patients assigned erlotinib 329 received erlotinib 16 did not start study treatment 5 missing data * 320 patients assigned placebo 311 received placebo 7 did not start study treatment 2 missing data * 39 ineligible 1 ecog 0 / 1 with crcl > 60 ml / min 38 > 62 days of diagnosis 40 ineligible 4 ecog 0 / 1 with crcl > 60 ml / min 36 > 62 days of diagnosis 350 analysed by intention to treat 320 analysed by intention to treat reasons for stopping 2 still on study drug at end of follow - up 14 completed 12 months 40 protocol toxicity 20 non - protocol toxicity 16 clinical morbidity 21 voluntary withdrawals ( not toxicity ) 84 progressive disease 126 died 6 other 16 never started study drug 5 missing data reasons for stopping 0 still on study drug at end of follow - up 6 completed 12 months 12 protocol toxicity 13 non - protocol toxicity 2 clinical morbidity 26 voluntary withdrawals ( not toxicity ) 119 progressive disease 119 died 1 unavailable 13 other 7 never started study drug 2 missing data figure 1 : trial pro le * patients with no recorded start date of study drug or dosing details . 
patients were randomised in a 1 : 1 ratio to either once daily oral erlotinib ( 150 mg tablets ) or matching placebo , with a computer generated sequence , strati ed by disease stage ( iiib , iv ) , performance status ( 01 , 2 , 3 ) , smoking history ( never , current / former ) , and centre ( 78 sites ) , with a block size of 10 . 
patients continued to receive active supportive care , including palliative radiotherapy , at the discretion of their clinician . the primary endpoint was overall survival , measured from the date of randomisation until death from any cause . 
secondary endpoints were progression - free survival ( time until progression or death from any cause ) , tumour response ( according to response evaluation criteria in solid tumours ) , adverse events , and quality of life . 
 within 4 weeks before randomisation patients had a physical examination , assessment of comorbidities with the charlson comorbidity index ( cci ) , blood count and biochemistry , chest radiograph , and ct of the chest and abdomen . 
 presence of several comorbidities was de ned as cci of 3 or more . clinicians did physical examinations , including assessment of performance status , development of rash , and adverse events ( with national cancer institute of canada common toxicity criteria for adverse events , version 3.0 ) , and a chest radiograph every month for the rst 12 months , and every 2 months thereafter . 
we graded rash with the criteria : erythema alone ( a ) , erythema with papules ( b ) , erythema with papules and pustules ( c ) , and erythema with papules 1162 vol 13 november 2012 and con uent pustules ( d )  . 
puri cation and assessment of quality and quantity of tumour dna were done with wizard genomic dna puri cation kit ( promega , madison , wi , erlotinib ( n = 350 ) placebo ( n = 320 ) age at randomisation median ( years ) 75 years 77 ( 7282 ) 220 ( 63% ) 77 ( 7281 ) 203 ( 63% ) usa )  . 
 * all patients with a performance score of 01 had comorbidities , ie , 92% ( 98 of 106 ) had cci scores of 3 , 95% ( 101 of 106 ) had creatinine clearance < 60 ml / min , and a median age of 81 years with 81% ( 86 of 106 ) aged > 75 years old . 
we calculated compliance to study treatment by dividing the total number of tablets taken ( equivalent to number of days on study drug ) by the number of days from randomisation to death , progression , or when treatment was stopped early , and expressed results as a percentage . 
preplanned subgroup analyses included sex , histological examination , activating egfr or kras mutation , stage , smoking status , ecog score , and development of rst - cycle rash . this study is registered , number isrctn 77383050 . role of the funding source the trial was funded by cancer research uk ( c1438 / a4147 ) , with an educational grant from roche for the translational studies , but neither were involved in trial design , data analyses or interpretation , or writing of this report . 
additional support came from the university college london and university college london hospital biomedical research centre , who had no role in study design , data collection , analysis , or interpretation , or writing of the report . 
the corresponding author had the nal responsibility for the decision to submit for publication . results we recruited 670 patients from 78 centres from the uk national cancer research network between april 14 , 2005 , and april 1 , 2009 . 
our randomisation procedure gave 936 cells and by chance the rst allocation in each cell for several centres was erlotinib , producing an imbalance in the number randomised to each group ; 350 participants were as signed to receive erlotinib and 320 placebo ( gure 1 )  . 
compliance to study treatment ( de ned as patients who took their tablets for 75% of the time that they were in the trial , until they died or stopped treatment early ) , was 58% ( 204 of 350 ) for erlotinib and 63% ( 203 of 320 ) for placebo ( median compliance was 88% [ iqr 098 ] for erlotinib and 86% [ 096 ] for placebo , appendix p 4 )  . 
 after discontinuation of study treatment , the most common subsequent therapy was palliative radiotherapy , which was given to 34% ( 119 of 350 ) of patients assigned erlotinib and 36% ( 114 of 320 ) of those assigned placebo . 
 only 2% ( 12 of 670 ) of patients received a tyrosinekinase inhibitor ( n = 3 ) or chemotherapy ( n = 9 ) after disease progression , seven in the placebo group and ve in the erlotinib group . 
the only tyrosine - kinase inhibitor used was erlotinib . 657 patients died ; 314 in the placebo group and 343 in the erlotinib group , with 93% ( 608 of 657 ) of deaths attributed to progressive disease . 
we identi ed no di erence in overall survival 1164 vol 13 november 2012 articles among all patients ; median overall survival was 37 months ( 95% ci 3242 ) in the erlotinib group versus 36 months ( 3239 ) in the placebo group ( unadjusted hr 094 , 95% ci 081110 , p = 046 ; adjusted hr 092 , 078107 , p = 031 )  . 
1 year overall survival was 14% ( 95% ci 1018 ) with placebo versus 15% ( 1219 ) with erlotinib . we identi ed a signi cant improvement in progression - free survival with erlotinib ( unadjusted hr 083 , 95% ci 071097 , p = 0019 ; adjusted hr 080 , 068093 , p = 00054 ) ; median progression - free survival was 28 months ( 95% ci 2630 ) with erlotinib versus 26 months ( 2429 ) with placebo ( gure 2b )  . 
tumour response rates are shown in the appendix ( p 5 ) ; 4% ( 15 of 350 ) of patients in the erlotinib group and 2% ( seven of 320 ) of those in the placebo group had a complete or partial tumour response . among the 647 patients who started study treatment , the occurrence of any grade 34 adverse event was 75% ( 252 of 334 ) with erlotinib and 70% ( 219 of 313 ) with placebo ( p = 012 , table 2 )  . 
more patients assigned erlotinib had rash at any time and of any grade than did those assigned placebo ( 56% [ 188 of 334 ] vs 15% [ 46 of 313 ] p < 00001 )  . 
 21% ( 69 of 334 ) of patients assigned erlotinib had diarrhoea of grade 12 versus 8% ( 24 of 313 ) for placebo ( p < 00001 ) , and rash and diarrhoea mainly occurred within the rst month of treatment . 
we recorded increased diarrhoea ( mean di erence 151 ) , hair loss ( 126 ) , sore mouth ( 64 ) , and decreased constipation ( 94 ) more frequently in patients assigned erlotinib than in those assigned placebo . [ p < 00001 ] , in prespeci ed subgroup analyses , rst - cycle rash among patients assigned erlotinib was the only signi cant independent factor ( hr 024 , 95% ci 016035 , p < 00001 ; table 3 ) associated with overall survival , from a stepwise selection multivariate analysis containing rash , sex , histological examination , ecog score , stage , and smoking status . 
patients were classi ed as having rst - cycle rash ( any grade ) when the rash occurred within the rst 28 days , which was when we made the rst assessment of rash . 
of the 647 patients who started study treatment , predictor variables for overall survival * rash women vs men ecog 01 vs 23 stage iiib vs iv ex - smoker vs smoker never smoker vs smoker hazard ratio ( 95% ci ) p value 024 ( 016035 ) < 00001 081 ( 059101 ) 087 ( 053140 ) 084 ( 061110 ) 092 ( 071118 ) 064 ( 036114 ) adenocarcinoma vs non - adenocarcinoma 092 ( 066129 ) predictor variables for progression - free survival rash women vs men 041 ( 027060 ) < 00001 074 ( 044103 ) 0058 adenocarcinoma vs non - adenocarcinoma 099 ( 071137 ) ecog 01 vs 23 stage iiib vs iv ex - smoker vs smoker never smoker vs smoker 091 ( 056148 ) 083 ( 059109 ) 098 ( 076127 ) 062 ( 035110 ) * for overall survival , p values from overall tests were p = 017 for sex , p = 062 for ecog , p = 084 for histological examination , p = 023 for stage , and p = 035 for smoking status . 
for progression - free survival , p values from overall tests were p = 006 for sex , p = 086 for ecog , p = 079 for histological examination , p = 021 for stage , and p = 028 for smoking status . 
result after a stepwise selection ; rash remained the only signi cant variable in the model for overall survival and progression - free survival . table 3 : summary of multivariate analysis for overall survival and progression - free survival 017 064 055 023 051 013 095 070 021 088 010 67 who died before this assessment were excluded from this subgroup analysis , to avoid bias by classi cation of them as not having rash . 
59% ( 178 of 302 ) of patients assigned erlotinib developed rst - cycle rash ( compared with 5% [ 15 of 278 ] assigned placebo ) , and we recorded a positive correlation between overall survival ( p < 00001 ) and progression - free survival ( p < 00001 ) with in creasing rash severity . among patients assigned erlotinib who developed rash ( compared with all those assigned placebo ) , overall survival was signi cantly longer ( hr 076 , 95% ci 063092 , p = 00058 ) , as was progression - free survival ( 066 , 054080 , p < 00001 )  . 
hazard ratios for patients assigned erlotinib who did not develop rash , compared with placebo , were 130 ( 95% ci 105161 , p = 0017 ) for overall survival , and 109 ( 089136 , p = 039 ) for progression - free survival , neither of which overlapped the corresponding intervals for patients who were treated with erlotinib and developed rash , indicating that they were signi cantly di erent ( ie , evidence for an interaction )  . 
 median overall survival was 62 months ( 95% ci 4872 ) for the erlotinib and rash group , 29 months ( 2337 ) for the erlotinib without rash group , and 41 months ( 3746 ) for placebo . 
1 year overall survival was 24% ( 95% ci 1729 ) for erlotinib and rash , 10% ( 516 ) for erlotinib without rash , and 18% ( 1221 ) for placebo . 
for erlotinib and rash compared with placebo , the number needed to treat to save one life at 6 months was seven and vol 13 november 2012 1165 articles erlotininb , no rash ( events 120 ) erlotininb , rash ( events 175 ) placebo ( events 272 ) erlotinib , no rash vs placebo hr 130 ( 95% ci 105161 ) p = 0017 erlotinib , rash vs placebo hr 076 ( 95% ci 063092 ) p = 00058 number at risk erlotinib , no rash erlotinib , rash placebo erlotininb , no rash ( events 122 ) erlotininb , rash ( events 173 ) placebo ( events 278 ) erlotinib , no rash vs placebo hr 109 ( 95% ci 089136 ) p = 039 erlotinib , rash vs placebo hr 066 ( 95% ci 054080 ) p < 00001 number at risk erlotinib , no rash erlotinib , rash placebo time since randomisation ( months ) figure 3 : overall survival and progression - free survival according to whether patients on erlotinib developed rst - cycle rash or not hr = hazard ratio . 
median progression - free survival was 34 months ( 95% ci 3140 ) for erlotinib and rash , 25 months ( 2228 ) for erlotinib without rash , and 29 months ( 2732 ) for placebo . we identi ed overall survival bene ts in patients who developed rst - cycle rash in all subgroups including those with the worst characteristics : ecog performance status 3 , overall survival hr 058 ( 95% ci 038089 , p = 0012 ) and progression - free survival hr 041 ( 026065 , p < 00001 ) ; stage iv , overall survival hr 066 ( 052084 , p < 00001 ) and progression - free survival hr 056 ( 044072 , p = 00009 ) ; and age 75 years or older , overall survival hr 077 ( 061097 , p = 0028 ) and progression - free survival hr 071 ( 056089 , p = 00032 )  . 
 kaplan - meier curves for overall survival were much the same for patients assigned placebo who did or did not develop rash ( p = 035 , data not shown )  . patients assigned erlotinib who developed rst - cycle rash had a higher occurrence of fatigue and diarrhoea than did those assigned erlotinib who did not develop rash ( appendix p 7 )  . 
the proportions with grade 34 fatigue were 30% ( 53 of 178 ) for erlotinib and rash , 19% ( 24 of 124 ) for erlotinib without rash , and 26% ( 72 of 278 ) for placebo . 
for grade 34 diarrhoea , the proportions were 11% ( 20 of 178 ) for erlotinib and rash , 6% ( eight of 124 ) for erlotinib without rash , and 1% ( four of 278 ) for placebo . 
when we excluded rst - cycle rash , the proportion of patients reporting at least four grade 34 adverse events was 47% ( 84 of 178 ) for erlotinib and rash , 19% ( 23 of 124 ) for erlotinib without rash , and 36% ( 99 of 278 ) for placebo ( appendix p 8 )  . 
among patients assigned erlotinib who developed rash , we recorded much the same e ects on quality of life as we did in the main analysis , with dyspnoea ( 93 ) and chest pain ( 67 ) signi cantly improved compared with patients without rash ( appendix p 9 )  . appendix p 2 shows the results of the other prespeci ed subgroup analyses , according to the presence or absence of rash in participants assigned erlotinib . 
among patients without rash , we identi ed no evidence of bene t , and overall survival might be worse for some subgroups , such as men ( hr 152 , 95% ci 113204 , p = 00046 ) , or ecog performance status 3 ( 169 , 111258 , p = 0014 )  . 
 patients assigned erlotinib who developed rash had longer overall survival and progression - free survival than did those assigned erlotinib who did not develop rash irrespective of baseline charac teristics , although some subgroups , including women ( overall survival hr 066 , 95% ci 048090 , p = 00090 ) and patients with adenocarcinoma ( 055 , 039077 , p = 000049 ) seemed to have a greater bene t than did other subgroups . 
 median overall survival for erlotinib and rash versus placebo was 81 months ( 95% ci 62104 ) versus 45 months ( 3956 ) for women , and 49 months ( 4163 ) versus 38 months ( 3344 ) for men . 
 however , the interaction test between sex and treatment was not signi cant ( p = 029 ) , and some of this di erence might be explained by a higher compliance to erlotinib in women ( 68% , 81 of 119 ) than in men ( 52% , 101 of 195 )  . 
 appendix p 10 shows further results for overall survival and progression - free survival according to sex and histological examination . in our biological substudy , dna was available for 390 patients out of 398 ( 58% of total study population ) who provided material . 
of the 28 egfr mutation - positive samples , 11 had exon 19 deletions , ten had a mutation at exon 21 ( 858leuarg ) , and seven had other mutations . 
in these patients , median overall survival was 104 months ( 95% ci 55151 ) for erlotinib ( n = 17 ) versus 37 months ( 03493 ) for pla cebo ( n = 11 )  . 
 among patients with wild - type egfr who were assigned erlotinib and developed rash ( n = 94 ) , hr for overall survival was 086 ( 95% ci 066112 , p = 027 ) and for progression - free survival was 069 ( 053090 , p = 00070 ; appendix p 2 )  . 
hr for those assigned erlotinib who did not develop rash ( n = 67 ) was 128 ( 095172 , p = 010 ) for overall survival and 105 ( 078141 , p = 074 ) for progression - free survival . kras mutation - positivity was not associated with overall survival or progression - free survival . 
among those who were kras mutation - positive , median overall survival was 42 months ( 95% ci 1862 ) for erlotinib ( n = 35 ) versus 36 months ( 1944 ) for placebo ( n = 38 ) ; median progression - free survival was 35 months ( 1748 ) versus 27 months ( 1839 )  . 
patients with wild - type kras had median overall survival of 37 months ( 2842 ) for erlotinib ( n = 210 ) versus 34 months ( 2743 ) for placebo ( n = 180 ) ; median progression - free survival was 27 months ( 2229 ) for erlotinib and 26 months ( 2329 ) for placebo . 
the presence or absence of rst - cycle rash did not a ect the results ( data not shown )  . discussion first - line treatment with erlotinib did not improve overall survival in all unselected patients with advanced nsclc deemed unsuitable for chemotherapy treatment , who usually have a poor prognosis ( about 34 months median overall survival10 )  . 
additionally , in prespeci ed subgroup analyses , com pared with placebo , erlotinib signi cantly improved both overall survival and progression - free survival for patients who developed a rst - cycle rash ; median overall survival in this group increased by 21 months , from 41 months to 62 months . 
however , few patients assigned placebo developed rst - cycle rash ( 5% compared with 59% assigned erlotinib ) , and we identi ed no di erence in survival in patients assigned placebo who had rash compared with those who did not . 
few patients were lost to follow - up because survival is short and patients with lung cancer in the uk are seen regularly and remain under the care of a hospital physician . a limitation of our study was that the incidence of egfr mutation was only 7% and a quarter of them were uncommon mutations . 
most egfr mutation studies focus on so - called hot spot analysis , looking only for common alterations , short deletions in exon 19 , or the 858leuarg point mutation in exon 21 . 
our population were mostly elderly , white , present or exsmokers , and such groups might have a di erent mutation spectrum pro le , which further studies could examine . 
never theless , although analyses were based on only 28 patients , overall survival and progressionfree survival were improved in patients with an egfr mutation who were assigned erlotinib , consistent with ge tinib in patients with poor performance status.13 however , patients with tumours showing wild - type egfr also showed bene t when they developed an erlotinib - related rash . 
in the ipass study , 14 only 56% ( 683 ) of patients provided samples with egfr mutation data available in 36% ( 437 ) of the 1217 patients randomised . 
this proportion was much the same as in our trial where samples from 58% of patients had su cient dna for analysis . another limitation of our study is that we did routine ct scans at 3 and 6 months , whereas some other studies have used ct scans every 68 weeks , so our schedule might be deemed suboptimum for assessment of progression - free survival . 
also , we included patients of performance status 2 , for whom , on the basis of evidence reported in 2005 , 15 chemotherapy could improve survival , and a phase 2 study16 has shown that doublet chemotherapy has a better survival than single agent chemotherapy . 
however , when topical was designed , provision of chemotherapy to such patients was not routine practice because many studies with second and third generation chemotherapy had not shown survival bene t , and many of these patients had serious adverse events.17 , 18 a limitation of many of the more recent chemotherapy trials is that median age of patients of performance status 2 is 65 years or younger , median survival is much the same as for patients of performance status 01 , and many go on to receive second - line treatment , suggesting that they are a highly selected group . 
by contrast , in topical median age was 77 years , 90% of participants had several comorbidities , and less than 2% were given second - line treatment , which is indicative of the real - world scenario that lung cancer is a disease of elderly people with comorbidities , and many of these patients still continue to be treated with best supportive care worldwide , including palliative radiotherapy.19 when topical was designed some evidence already suggested that development of a rash during erlotinib vol 13 november 2012 1167 articles panel : research in context systematic review we did not do a systematic review of scienti c literature before designing the topical trial ( in 2002 ) , because at the time there were no other studies of rst - line egfr inhibitors in patients with advanced non - small - cell lung cancer ( nsclc ) who were elderly or had poor performance status . 
these patients are often excluded from rst - line chemotherapy trials . lung cancer is predominantly a disease of elderly people , and elderly patients with advanced nsclc deemed unsuitable for chemotherapy with poor performance status ( 2 and 3 ) or several comorbidities , or both , remain a major challenge . 
since topical , no phase 3 trials of rst - line monotherapy for this group have been reported . interpretation the ndings of topical and other trials58 show that erlotinib is an important treatment for patients with nsclc in various clinical settings , including as maintenance after rst - line chemotherapy , as second - line or third - line monotherapy in unselected patients with advanced nsclc , and in chemotherapy - naive patients with activating egfr mutations . 
however , unlike the topical patients , most of the patients in other studies had good performance status . the clinical implications of the topical trial are that patients who are deemed unsuitable for chemotherapy could be given erlotinib . 
those who have egfr mutation - positive tumours could receive continuous erlotinib ; whereas those who have wild - type tumours should discontinue erlotinib after about 28 days if they do not develop a rash because of the possibility of decreased survival . therapy could be associated with improved outcomes across several cancers including nsclc.20 with this knowledge , we developed a scoring system for rash as part of the topical protocol , and speci ed a preplanned subgroup analysis . 
furthermore , retrospective analyses of two phase 3 nsclc trials show a positive correlation between rash and treatment e ect on survival : the br.21 trial12 of erlotinib and the flex trial11 of cetuximab , an anti - egfr antibody , when added to rst - line chemotherapy . 
researchers have recorded much the same ndings in trials of pancreatic cancer , locally advanced head and neck cancer , and metastatic colorectal cancer.12 , 21 , 22 currently no clear biological explanations link erlotinib activity with rash , but rash probably represents greater uptake of the drug . 
smokers have a lower plasma concentration of erlotinib than do non - smokers.23 , 24 smokers also have a lower incidence of skin rash and have less clinical bene t from egfr inhibitors compared with non - smokers.23 , 24 this nding was con rmed in topical because present smokers in the erlotinib group were less likely to develop rash when compared with former smokers ( odds ratio 029 , 95% ci 018048 ) or never - smokers ( 020 , 006066 )  . 
 increased occurrence of skin rash has been identi ed in a phase 2 dose escalation study of erlotinib , although another study suggested that dose - escalation does not improve incidence or out come.25 , 26 alternatively , skin rash might be a surrogate marker of patients able to mount antitumour immune response . 
data increasingly suggest the importance of the host immune system in control of cancer cell growth after tyrosine - kinase inhibitor treatments.27 , 28 as reported with other tyrosinekinase inhibitors , erlotinib could enhance cytotoxic t - cell in ltration . drug uptake and cytotoxic t - cell in ltration could be linked , with increased uptake of drug causing increased egfr blockade and cell killing , resulting in improved host immune response . 
future studies could examine whether combining erlotinib and immunomodulatory agents can further fuel a more robust immunological response , increase the severity and incidence of skin rash , and potentially further improve durability of response , progression - free survival , and overall survival in this group of patients who are deemed not suitable for chemotherapy . a phase 2 study10 of ge tinib ( n = 201 ) compared with placebo ( instep ) in a group of patients with similar characteristics to those in topical showed no statistical di erence in survival with a hr of 084 ( 95% ci 062115 ) , but we identi ed a suggestion of a bene t among patients with high egfr gene copy number determined by uorescence in - situ hybridisation ( hr 044 , 95% ci 017112 )  . 
the dose of ge tinib might have been sub therapeutic in patients with wild - type egfr tumours , and this notion is supported by the lower than expected proportion who developed rash . 
 another phase 2 trial29 of only patients of performance status 2 ( n = 103 ) with a median age of less than 70 years compared erlotinib with carboplatin and paclitaxel , and showed that progression - free survival was better with chemotherapy than with erlotinib but progression - free survival did not di er between patients assigned erlotinib who developed rash compared with those who were assigned chemotherapy ( hr 094 , 95% ci 056159 )  . 
in topical , erlotinib seemed to have a greater e ect in some subgroups than in others ( eg , median overall survival was improved by 36 months for women with rash and 11 months for men with rash )  . 
previous studies have also reported sextreatment interactions with tyrosine - kinase inhibitors and other chemotherapies , where female patients bene ted more than men.30 diarrhoea , hair loss , and fatigue were expected adverse events associated with erlotinib , and their severity was usually mild to moderate . 
overall , occur rence and severity of adverse events in topical were much the same as those in the saturn and br.21 trials despite our population being predominantly elderly patients with poor performance status ( ecog 23 ) .5 , 6 taking erlotinib tablets at home should be more convenient to patients compared with treatments that require administration in hospital . 
we believe that patients with poor performance status and activating egfr mutation tumours should 1168 vol 13 november 2012 articles receive erlotinib or ge tinib , in line with the established evidence in patients with good per formance status , and supported by the nding that the small number of these patients in topical all developed rash.7 , 8 , 14 our data suggest patients with egfr wild - type or unknown egfr status tumours could start erlotinib but they should discontinue if they do not develop rash within 28 days , because these patients had no bene t in overall survival or progression - free survival , and in some subgroups overall survival could be reduced if erlotinib were taken continuously ( panel )  . 
the reasons for this nding are unknown but for some of our patients ( especially men and those with ecog performance status of 3 ) , the disease might be so advanced that any toxic treatment could accelerate deaths . 
researchers have recorded deleterious e ects of anti - egfr in some patients treated with erlotinib or cetuximab.31 , 32 a strategy of use of rst - cycle erlotinib - induced rash to select patients with poor performance status for continued treatment could substantially improve cost e ectiveness . 
second and third line erlotinib is marginally cost - e ective compared with best supportive care , therefore rst - line erlotinib could be more cost - e ective.33 egfr testing has now become standard of care to select patients who are egfr mutation - positive for treatment with tyrosine - kinase inhibitors . 
if erlotinib is to become a standard therapy for patients who have egfr wild - type tumours and are unsuitable for chemotherapy ( 93% in our trial ) it should be in a selected population . 
prospective studies are needed to increase our understanding of the biological mechanism linking rash and erlotinib bene t , including dose - escalation studies or studies of the relation between rash and tumour egfr copy number.34 further translational research with our biological samples might identify candidate markers for erlotinib - induced rash that can preselect patients for treatment with a marker measured at baseline , without having to treat all patients for 4 weeks , and then discontinue those without rash . contributors sml had the initial trial concept ; sml , cb , rr , and ah designed the trial ; sml , su , cl , sf , gs , em , pjw , mh , rl , rj , et , dc , gm , and sb were centre investigators , and recruited and treated patients ; sml , ik , yn , and ah were involved in trial conduct ; sml , ik , cb , and ah analysed and interpreted the data ; ik did the statistical analyses ; sml , cb , and ah wrote the report . 
all authors reviewed and approved the nal report . con icts of interest cl , et , dc , gm , and sml have received travel grants and honoraria from roche uk for serving on advisory boards . 
all other authors declare that they have no con icts of interest . acknowledgments the trial was funded by cancer research uk ( c1438 / a4147 ) , with an educational grant from roche for the translational studies , and support from the university college london and university college london hospital biomedical research centre ( who part - fund sml )  . 
we report on whether selective focal ablation of unifocal and multifocal cancer lesions can reduce this treatment burden . methods men aged 4580 years were eligible for this prospective development study if they had low - risk to high - risk localised prostate cancer ( prostate speci c antigen [ psa ] 15 ng / ml , gleason score 4 + 3 , stage t2 ) , with no previous androgen deprivation or treatment for prostate cancer , and who could safely undergo multiparametric mri and have a general anaesthetic . 
patients received focal therapy using high - intensity focused ultrasound , delivered to all known cancer lesions , with a margin of normal tissue , identi ed on multiparametric mri , template prostate - mapping biopsies , or both . 
 nine men ( 22% , 95% ci 1138 ) had self - resolving , mild to moderate , intermittent dysuria ( median duration 50 days [ iqr 25185 ] )  . 
median overall international index of erectile function - 15 ( iief - 15 ) scores were similar at baseline and at 12 months ( p = 0060 ) , as were median iief - 15 scores for intercourse satisfaction ( p = 0454 ) , sexual desire ( p = 0644 ) , and overall satisfaction ( p = 0257 )  . 
there was an improvement in lower urinary tract symptoms , assessed by international prostate symptom score ( ipss ) , between baseline and 12 months ( p = 0026 ) , but the ipss - quality of life score showed no di erence between baseline and 12 months ( p = 0655 )  . 
no signi cant di erence was reported in median trial outcomes index scores between baseline and 12 months ( p = 0113 ) but signi cant improvement was shown in median functional assessment of cancer therapy ( fact ) - prostate ( p = 0045 ) and median fact - general scores ( p = 0041 )  . 
no histological evidence of cancer was identi ed in 30 of 39 men biopsied at 6 months ( 77% , 95% ci 6189 ) ; 36 ( 92% , 7998 ) were free of clinically signi cant cancer . 
after retreatment in four men , 39 of 41 ( 95% , 95% ci 8399 ) had no evidence of disease on multiparametric mri at 12 months . interpretation focal therapy of individual prostate cancer lesions , whether multifocal or unifocal , leads to a low rate of genitourinary side - e ects and an encouraging rate of early absence of clinically signi cant prostate cancer . funding medical research council ( uk ) , pelican cancer foundation , and st peters trust . introduction the management of localised prostate cancer remains controversial because the systematic over - diagnosis that accompanies the current diagnostic pathway results in over - treatment.1 at present , radical whole - gland surgery or radiotherapy can result in substantial side - e ects that are a consequence of damage to surrounding structures . 
 these include urinary incontinence ( 520% ) , erectile dysfunction ( 3070% ) , and bowel toxicity ( 510% ) .2 , 3 technological re ne ments do not seem to have reduced the burden of harm.4 , 5 apart from active surveillance for low - risk disease , few strategies are available to address the burden of treatment - related side - e ects in other risk categories . 
 one strategy that has shown promise relates to managing prostate cancer in the same manner as most other solid organ malignanciesby focusing injury to the the therapy to the cancer lesion , 622 vol 13 june 2012 articles the protocol was anonymously peer - reviewed by the national cancer research network ( ncrn ) , uk , and the medical research council , uk . for the study protocol see therapy / hifu / focal / focal - hifuprotocol bladder , rectum , and neurovascular bundles could be reduced.6 , 7 we have previously assessed hemi - ablation of patients with localised unilateral prostate cancer , 8 which included treatment of the entire half of the prostate associated with cancer . 
this strategy is the most straight forward to undertake , standardise , and train others to do , but is limited because only one in ve men have true unilateral disease on template biopsies . 
furthermore , hemi - ablation might represent overtreatment since a low - volume , lowgrade lesion would be treated in the same manner as a high - volume , high - grade cancer . 
in this study , we postulated that selective focal ablation of unifocal and multifocal cancer lesions with a margin of normal tissue could reduce genitourinary and rectal side - e ects for men with localised prostate cancer . methods study design and patients we undertook a two - centre , prospective development study , as de ned by the ideal ( idea , development , exploration , assessment , and long - term ) guidelines for assessing innovation in surgery.9 men could enter into the study if they had localised prostate cancer on multiparametric mri and templateprostate - mapping biopsies.10 transperineal we included men with low - risk to high - risk disease ( prostate - speci c antigen [ psa ] 15 ng / ml , gleason score 4 + 3 , stage t2 ) , aged 4580 years with a life expectancy of 5 years or more , a prostate volume of 40 ml or less or maximum anteriorposterior length of 40 mm or less who had undergone multiparametric mri and transperineal template ( 5 mm spaced ) biopsies in the 6 months before recruitment . 
we excluded men who had androgen suppression within the previous 6 months , previous radiation therapy or chemotherapy for prostate cancer , latex allergies , previous rectal surgery preventing insertion of transrectal probe , intraprostatic calci cations making high - intensity focused ultrasound ( hifu ) of focal areas of cancer di cult , previous transurethral resection of the prostate or laser prostatectomy in 5 years before recruitment , previous hifu , cryosurgery , or thermal or microwave therapy to the prostate at any point before recruitment . 
men who were not t for general anaesthesia or regional anaes thesia as assessed by a consultant anaesthetist , or were unable to have mri scanning ( eg , severe claustrophobia , permanent cardiac pacemaker , metallic to contribute implant signi cant artifact to images ) were also excluded . 
all men gave written informed consent . likely our trial was approved by the university college london hospitals local research ethics committee a , uk , which is under the auspices of the national research ethics service . 
additionally , contrast - enhance ment procedures to locate areas of cancer , multiparametric mri was done at 15 t magnetic eld strength with pelvic phased - array included t2 - weighting , dynamic coils . 
all biopsies were reported by a single uropathologist . men underwent focal ablation with a transrectal hifu device ( sonablate 500 ; focus surgery , indianapolis , in , usa )  . 
the dimensions of the target area were determined by the focal length of the transducer , the applied frequency , the intensity of the applied power ( w / cm ) , and the duration of the pulse . 
its long axis lies at right angles to the transducer and is greatest in length towards the transducer . this temperature tissue destruction is produced by thermal , mechanical , and cavitation e ects to produce a clearly demarcated region of coagulative necrosis surrounded by normal tissue on microscopic examination . 
adequate cell destruction can be produced by short exposure ( 1 s ) to temperatures of 60c or more , which has therefore been adopted as the minimum target temperature . 
cooling due to tissue perfusion in the focal zone is not a problem because the rate of heating is greater than that of cooling when the exposure time is within a window of 3 s . 
cavitation results from gas ( bubble ) formation within cells due to heat and mechanical energy deposition causing bubbles to oscillate . all patients had sterile urine on culture before treatment . 
if culture was positive for infection , men were treated with antibiotics and their treatment rescheduled ; prophy lactic intravenous gentamicin was given to all men at the time of general anaesthetic . 
the operator made judgments as to the location and boundaries of the cancer lesions for treatment planning on the basis of the information from both multiparametric mri ( when a lesion was visible ) and template - prostate - mapping biopsies . 
designation of individual lesions was usually straightforward but when positive biopsies were close together , lesions were labelled separately if there was at least one intervening normal biopsy . after ablation , the suprapubic catheter was placed on free drainage into a urinary leg - bag for 12 days and urethral voiding was encouraged thereafter by closure of a valve attached to the catheter . 
because many men travelled a long distance , the timing of catheter removal was delayed to coincide with the rst trial visit after the operation at 1014 days ( for an early mri ) even if urethral voiding was restored earlier . 
 a contrast - enhanced mri was done 1014 days after focal hifu to con rm the area of ablation , as shown by a con uent perfusion de cit . follow - up consisted of clinic visits at 1 month , 3 months , 6 months , 9 months , and 12 months for psa measurement and adverse event reporting . 
 questionnaires included the international prostate symptom score ( ipss ) , international index of erectile function - 15 ( iief - 15 ) , ucla - expanded prostate cancer index composite ( epic ) urinary incontinence scale , and the functional assessment of cancer therapyprostate ( fact - p ) score , which includes fact - general ( fact - g ) scores and the trials outcome index.1115 phosphodiesterase - 5 inhibitors were permitted at any timepoint during follow - up . 
at 6 months , another multiparametric mri followed by targeted biopsies of the treated areas were scheduled with a minimum requirement for sampling every 1 ml of residual tissue with one core . 
our justi cation for one biopsy for every ml of residual tissue re ects the biopsy density of the original template biopsies before focal hifu ( which was about 1 ml for every biopsy )  . 
as the purpose of the 6 - month biopsies was to determine whether the ablation was successful , our ethics com mittee did not permit sampling of untreated tissue due to the requirement for another general anaesthetic . 
however , biopsies of the untreated tissue were permitted if a new , potentially malignant lesion was seen on multiparametric mri . the primary outcomes were feasibility , patient acceptability , and side - e ect pro le of focal hifu . 
the iief - 15 was used to report the proportion of men capable of having erectile function su cient for penetration at 12 months as well as total iief - 15 score and domain scores on erectile function , intercourse satisfaction , orgasmic function , sexual desire , and overall satisfaction . 
the continence questionnaire included total scores as well as the proportion of patients who were pad - free , or leak - free and pad - free at 12 months . 
quality of life was measured with fact - p with summary measures of the trial outcome index score , fact - p score , and fact - g score . secondary outcomes were histological and imaging measures of cancer control . 
for this status to be met , we de ned trifecta as leak - free and padfree continence , erections su cient for penetration , and no evidence of clinically signi cant disease at 12 months multiparametric mri16 , 17 in those men with normal baseline genitourinary function . statistical analysis since the primary objective of the study was to determine the side - e ect pro le of focal ablation , the sample size was powered on a common event , namely erectile dysfunction . 
the sample size calculation was based on a comparison with a known rate of 40% erectile dysfunction , 18 which usually occurs when hifu is applied to the whole prostate.19 therefore , with an level of 005 and power of 90% ( 1 ) , the sample size required was at least 33 men with good baseline function . 
we adjusted the sample size to allow for the estimated rate of 25% of men having poor baseline erectile function in the general population , and therefore aimed to recruit 42 men in total . validated questionnaires were analysed with standard methods . 
missing values for patient - reported outcome 624 vol 13 june 2012 articles psa density ( ng / ml per ml prostate ) 018 ( 014022 ) age ( years ) serum psa ( ng / ml ) reason for psa test and biopsy psa screening ( patient request ) lower urinary tract symptoms * prostate volume ( ml ) initial biopsy trus biopsy tpm biopsy gleason ( trus - guided biopsy ) no trus biopsy gleason ( tpm biopsies ) clinical stage trus guided biopsies total cores total positive cores percent positive cores tpm biopsies total cores total positive cores positive cores ( % ) core density ( biopsies / ml ) number of lesions on tpm disease distribution bilateral ( midline lesion ) three unifocal unilateral multifocal unilateral bilateral high intermediate nccn risk category20 patients ( n = 41 ) 63 ( 580660 ) 66 ( 5477 ) 31 ( 76% ) 10 ( 24% ) 35 ( 290455 ) 35 ( 85% ) 6 ( 15% ) 24 ( 59% ) 7 ( 17% ) 5 ( 12% ) 5 ( 12% ) 13 ( 32% ) 24 ( 59% ) 4 ( 10% ) 37 ( 90% ) 4 ( 10% ) 15 ( 37% ) 6 ( 15% ) 5 ( 12% ) 15 ( 37% ) 11 ( 27% ) 26 ( 63% ) 4 ( 10% ) 100 ( 80120 ) 20 ( 1030 ) 110 ( 63338 ) 46 ( 355655 ) 5 ( 3090 ) 94% ( 46185 ) 14 ( 0919 ) variables ( between 2% and 10% missing values for individual questions ) were imputed with a fully conditional speci cation method and logistic regression model ( categorical data )  . 
the imputation was based on the observation of values missing completely at rando we classed the variables for which missing values were to be imputed ( questionnaires ) as categorical . 
 wilcoxon signed rank test ( two - tailed ) was used to assess di erences between continuous variables that were not normally distributed ( psa and questionnaire scores ) measured at baseline and at the 12 - month follow - up visit . 
the corresponding author had full access to all the data and had nal responsibility for the decision to submit for publication . results 42 men were recruited between june 27 , 2007 , and june 30 , 2010 . 
he had an uneventful recovery after hifu and had no respiratory symptoms immediately before treatment , or at 2 weeks and 6 weeks after treatment during the formal trial visits . 
 as a result , 41 men were included in analyses ; 30 ( 73% ) had intermediate and high - risk disease ( table 1 ) .20 three men had baseline mild stress urinary incontinence but required no pads ; 35 had good baseline sexual function with erections su cient for penetration . 
 * these men were opportunistically screened with a psa test when they presented with symptoms of lower urinary tract infection , rather than part of a formal request ( by their physician or by the men themselves ) for a psa test . 
a high number of positive cores were retrieved , despite only a maximum of three lesions , because large dominant lesions were sampled several times . table 1 : baseline characteristics see online for appendix vol 13 june 2012 articles neurovascular bundles figure 1 : schematic diagrams of the types of focal therapy unilateral one - area ablation ( a )  . 
grey transparent boxes represent ablation zones on the high - intensity focused ultrasound device . total anaesthetic time ( min ) procedure time ( suprapubic catheter + focal hifu ; min ) total hospitalisation time ( admission to discharge ; h ) discharge time ( end procedure to discharge ; h ) time with suprapubic catheter ( days ) * dysuria ( negative urine culture ) duration of dysuria ( days ) intermittent haematuria ( start of stream only ) duration of intermittent haematuria ( days ) urinary debris duration of urinary debris ( days ) urinary tract infection ( positive urine culture ) acute retention of urine value 1350 ( 11501500 ) 1050 ( 8701250 ) 120 ( 100270 ) 60 ( 50180 ) 85 ( 80150 ) 9 / 41 ( 22% , 1138 ) 5 ( 25185 ) 16 / 41 ( 39% , 2456 ) 15 ( 103150 ) 14 / 41 ( 34% , 2051 ) 145 ( 60165 ) 7 / 41 ( 17% , 732 ) 1 / 41 ( 2% , 013 ) data are median ( iqr ) or number of patients a ected / n ( % , 95% ci )  . 
 * suprapubic catheter was usually removed at the same time as the postoperative early contrast mri for convenience to reduce visits for men who travelled far to the study centre . 
 table 2 : perioperative outcomes in men undergoing focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer to moderate , urethra on the rst day after the operation with the suprapubic catheter clamped . 
he had multiparametric mri and urethrogram within 4 weeks , which showed extravasation of urine outside the prostate ; although the serosal layer of the rectum was a ected by treatment no de nitive rectourethral stula was seen . 
however , as a precautionary measure , he was managed conservatively with a suprapubic catheter and quinolone antibiotics , serial 2 monthly multiparametric mri , and a further repeat urethrogram until the extravasation had resolved by 6 months . 
at that point , he developed a stricture requiring endoscopic dilatation ; a further two limited endoscopic prostate - tissue resections to a prostate that had a total volume of 80 ml were done when voiding did not return to normal . overall iief - 15 scores initially decreased , indicating diminished erectile function but showed a gradual return to baseline by 12 months ( p = 0060 ; gure 2a )  . 
iief - 15 domain scores in intercourse satisfaction ( p = 0454 ) , sexual desire ( p = 0644 ) , and overall satisfaction ( p = 0257 ) all showed decreased scores at 1 month and 3 months , but there was no signi cant di erence between baseline and 12 months ( gure 2 c , f )  . 
iief - 15 erectile and orgasmic domains showed signi cant deteriorations from baseline to 12 months ( p = 0042 and p = 0003 , respectively ; gure 2 b , d )  . 
no formal programme of penile rehabilitation was available , but all men were o ered phosphodiesterase - 5 inhibitors ( eg , sildena l , tadala l ) if needed ; 14 of the 31 men required phosphodiesterase - 5 inhibitors . in a post - hoc analysis to explore whether type of ablation made any di erence to erectile dys function , we assessed the following factors . 
of those men who had erections su cient for penetration at baseline , 28 of 31 ( 90% , 95% ci 7498 ) of those who had unilateral nervesparing ablation and four of four ( 100% , 40100 ) who had bilateral nerve - sparing ablation had erections su cient for penetration at 12 months . 
ipss values increased initially although by 12 months showed signi cantly lower values , suggesting lower urinary - tract symptoms from baseline ( p = 0026 ; gure 4 )  . 
no signi cant di erence was seen in ipss - quality - of - life score between baseline and 12 months ( p = 0655 ; gure 4 )  . 
of 38 men with no urinary leak at baseline all ( 100% , 95% ci 91100 ) were leak - free and pad - free by 9 months ; 40 men pad - free at baseline were pad - free again by 3 months and maintained pad - free continence at 12 month ( 100% , 91100 ; one man did not report on this parameter at 12 months and was excluded )  . signi cant deterioration of health - related quality of life was shown between baseline and 12 months on the total fact - p and total fact - g scores ( p = 0045 and p = 0041 , respectively ; gure 5 )  . 
no signi cant di erence was seen between baseline and 12 months in the trial outcomes index between baseline and 12 months ( p = 0113 ; gure 5 )  . compared with baseline , a signi cant decrease in psa levels was reported at 12 months ( p < 00001 ; gure 6 )  . 
 the time to nadir was not calculated because the psa changes showed a pattern of ongoing small decreases in psa up to trial end at 12 months . one man refused to undergo biopsy at 6 months because of his concern over the e ect of further biopsies on sexual function . 
of the n = 41 n = 41 n = 41 n = 41 n = 41 n = 41 ( n = 2 ) ( n = 1 ) ( n = 3 ) ( n = 1 ) ( n = 1 ) ( n = 3 ) time ( months ) figure 4 : urinary function after focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer , measured with international prostate symptom score ( ipss ) questionnaire two - tailed p values were reported for wilcoxon signed ranks test comparing baseline and 12 - month median scores . 
median baseline versus 12 - month international prostate symptom score ( ipss ) : 80 ( iqr 55130 ) vs 70 ( 30120 , p = 0026 ; a )  . 
median baseline versus 12 - month ipss - quality of life : 10 ( 0020 ) vs 10 ( 1010 , p = 0655 ; b )  . 39 men biopsied , nine ( 23% , 95% ci 1139 ) had evidence of cancer while three ( 8% , 221 ) had evidence of clinically signi cant cancer ( epstein criteria21 , 22gleason > 3 + 3 , > 2 cores positive , > 2 mm cancer involve ment ; table 3 )  . 
median baseline versus 12 - month functional assessment of cancer therapy ( fact ) - prostate score : 1385 ( 13301470 ) vs 1453 ( 13701520 , p = 0045 ; b )  . 
as de ned by epstein criteria : gleason > 3 + 3 , > 2 cores positive , 3 mm cancer involvement . table 3 : histological outcomes at 6 months in men undergoing focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer 9 months and 29 ng / ml ( 1836 ) at 12 months . 
none of the four men undergoing repeat focal therapy consented to further biopsies but all had multiparametric mri at trial exit showing no evidence of clinically signi cant disease at 12 months . 
no man required adjuvant radiotherapy , prostate cancer surgery , or androgen deprivation therapy during the trial duration . vol 13 june 2012 articles 39 / 41 * ( 95% , 95% ci 8399 ) 26 / 31 * ( 84% , 95% ci 6695 ) pad - free continence leak - free / pad - free continence erections sucient for penetration no evidence of disease trifecta ( pad - free , leak - free , and erectile function satisfatory for penetration , and no evidence of clinically signicant disease ) any cancer on biopsy clinically signicant cancer on biopsy ( 3 mm and / or gleason > 3 + 3 ) time ( months ) 9 / 39 * ( 23% , 95% ci 1139 ) 3 / 39 ( 8% , 95% ci 221 ) functional outcome continence * pad - free and leak free pad - free erections satisfactory for penetration use of phosphodiesterase 5 inhibitors|| 26 ( 68% , 5183 ) 33 ( 83% , 6793 ) 19 ( 54% , 3771 ) 36 ( 95% , 8299 ) 38 37 ( 97% , 86100 ) ( 100% , 91100 ) ( 100% , 91100 ) 40 40 40 38 ( 100% , 91100 ) ( 100% , 91100 ) ( 100% , 91100 ) ( 100% , 91100 ) ( 83% , 6693 ) 29 ( 83% , 6693 ) 31 ( 89% , 7397 ) ( 89% , 7397 ) 3 / 35 ( 9% ) 4 / 19 ( 21% , 646 ) 14 / 29 ( 48% , 2967 ) 17 / 29 ( 59% , 3976 ) 17 / 31 ( 55% , 3673 ) 14 / 31 ( 45% , 2764 ) figure 7 : trifecta rate after focal high - intensity focused ultrasound for unifocal and multifocal localised prostate cancer patient - reported trifecta outcomes were reported with validated questionnaires . 
proportion of men scoring 2 on question 2 of iief - 15 : over the past 4 weeks when you had erections with sexual stimulation , how often were your erections hard enough for penetration ?  . 
||phosphodiesterase - 5 inhibitors ( tadala l , sildena l , or vardena l ; percentage calculated with denominator as those achieving erections su cient for intercourse )  . of the 31 men with good baseline function , 26 ( 84% , 95% ci 6695 ) achieved the trifecta status of having leak - free and pad - free continence , erections su cient for intercourse , and no evidence of clinically signi cant disease on multipara metric mri at 12 months ( gure 7 )  . 
 discussion to our knowledge , our study is the rst to assess targeting of individual known cancer areas , with a margin of normal tissue , in men with multifocal as well as unifocal prostate cancer across all cancer - risk categories . 
almost 90% of men reported having erections satisfactory for intercourse at 12 months , and all were continent . there was a signi cant decrease in psa levels from baseline to 12 months , with concentrations of serum psa continuing to decline months after the initial treatment . 
conclusions from this nding should not be made , although if this decline in serum psa were to be reproduced , one possible reason for it might be the presentation of antigens to the immune response leading to a secondary immune response against the remaining prostate tissue.23 there are several limitations to our study . 
second , characterisation of disease with templateprostate - mapping biopsies before focal therapy was di erent to the 6 - month veri cation biopsy , because of research ethics committee stipulations to limit patient burden . 
the trial will assess focal hifu applied to clinically signi cant areas of prostate cancer identi ed on entry by multiparametric mri and template prostate - mapping biopsies25 , 26 followed by further multiparametric mri and template prostate - mapping biopsies applied to treated and untreated tissue at 3 years ( nct01194648 )  . 
destruction of some normal tissue is necessary to incorporate an adequate margin but because of the nature of the hifu therapy , our margins are likely to be larger than they need to be . 
furthermore , image - registration of preoperative mri to treatment delivery could further help to reduce destruction of normal tissue by allowing the clinician to more accurately de ne the boundaries of the target lesion . many retrospective series have reported case encouraging short - term functional and cancer - control outcomes of men treated in a focal manner with hifu and cryotherapy.2732 a prospective feasibility trial has reported on the use of focal interstitial laser therapy in a small cohort of 12 men with very low - risk unifocal disease.33 we have previously reported8 the outcomes from a prospective development study of 20 men with unilateral disease undergoing ablation of an entire prostate lobe using hifu . 
18 ( 90% ) were leak - free and pad - free continent while 19 ( 95% ) were pad - free after 630 vol 13 june 2012 articles panel : research in context systematic review in 2007 , we did a systematic review7 of reports on medline and pubmed databases using the terms focal therapy and prostate cancer and / or high intensity focused ultrasound and / or cryotherapy / cryoablation / cryosurgery . 
subsequent to this review , we started a health technology assessment of focal therapy , following the phased approach described by the medical research council complex interventions guidelines and subsequently formalised in the ideal guidelines for assessing surgical procedures.9 interpretation our study showed that the rate of genitourinary side - e ects associated with focal therapy is low , coupled with an encouraging rate of early absence of clinically signi cant prostate cancer . 
these ndings rea rm two other prospective development studies8 , 33 in which focal using high - intensity focused ultrasound and photothermal therapy was used . focal therapy could hold promise in mitigating the harms that result from current therapeutic strategies . 
any randomised controlled trial should be pragmatic in nature and adaptive in execution , so that actual clinical practice is re ected and new technological developments can be incorporated as they occur . 
furthermore , since the natural history of prostate cancer is long , timelines based on metastases and mortality , which would require a trial at least 15 years in duration , might not be feasible or warranted . 
subsequent linkage to national electronic registries will ensure that robust cancer - control outcomes are still reported at a later date . hemi - ablation ; 17 ( 89% ) of 19 achieved trifecta status at 12 months.8 the current study allowed user or operator determination of ablative zones within the prostate on an individual basis provided our standardised method of focal therapy was followed . 
however , the treatments invariably followed one of three patterns of ablation ( gure 1 ) , by contrast with our previous study , 8 whereby the treatment method was xed and standardised by mandating therapy to the entire half of the prostate associated with cancer ( hemi - ablation ) regardless of individual lesion grade , volume , or location and proximity to a neurovascular bundle . while our current study is not directly comparable to previous studies of focal therapy ( panel ) , it continues to support the proposition that tissue preservation leads to functional preservation . 
the histological outcomes in this study were slightly worse than those reported for hemiablation , perhaps because of the requirements for increased pre cision of focal ablationindividual areas of cancer were targeted as opposed to a standardised hemiablationwith a resulting reduction in margin around the cancer . 
image - registration software to accurately fuse , in real - time , pretreatment location data to intraoperative ultrasound images could improve histological outcomes.34 another reasonable explanation might relate to physical limitations of the ablative technology . 
new irreversible electroporation and platforms such as photodynamic therapy are theor etically more tissuespeci c and could allow neurovascular bundle preservation even if the ablative zone is close to the prostate capsule ; tissue speci city of these techniques has not yet been assessed . in conclusion , focal therapy of individual prostatecancer lesions , regardless of whether they are multifocal or unifocal , leads to a low rate of genitourinary sidee ects and an encouraging rate of early freedom from clinically signi cant prostate cancer . 
if the functional outcomes that we report are reproduced in larger studies and coupled with acceptable rates of cancer control in the medium to long term , focal therapy could o er a strategy by which the burden of treatmentrelated side - e ects are addressed for a substantial proportion of men with localised prostate cancer . 
the design and execution of comparative - e ectiveness research assessing long - term cancer control needs to be prioritised , especially at a pace than can match the potential for informal di usion . contributors me and hua conceived the study . 
all authors contributed to the drafting and editing of the manuscript and approved the nal version . con icts of interest me and hua received funding from ushifu , glaxosmithkline , and advanced medical diagnostics for clinical trials . 
me and hua are paid consultants to steba biotech and have received funding from ushifu , focused surgery , misonix ( manufacturers and distributors of the sonablate 500 high - intensity focused ultrasound device ) , and oncura and ge healthcare for medical consultancy and travel to conferences . 
 all other authors declared no con icts of interest . acknowledgments this study was funded by the uk medical research council , the pelican cancer foundation , and st peters trust , and sponsored by university college london hospitals nhs foundation trust . 
we thank the men vol 13 june 2012 articles who agreed to participate in this trial , and jane coe and victor abu for their invaluable help and support during the duration of the study . 
hua and me receive funding for other research projects from the wellcome trust , national institute of health research - health technology assessment programme , the us national institute of healthnational cancer institute , prostate action , and prostate cancer research centre . 
 me receives funding in part from the uk national institute of health research university college london hospitals / university college london comprehensive biomedical research centre . editorial this online publication has been corrected . 
the corrected version rst appeared at thelancet.com / oncology on june 29 , 2012 for more on the lancet oncologys call for gps to receive better education see leading edge lancet oncol 2009 ; 10 : 97 for more on variation in gp referral patterns for patients with cancer see articles lancet oncol 2012 ; 13 : 35365 for more on the partnership between cancer research uk and the royal college of general practitioners see news lancet oncol 2012 : 12 : e232 for more on qcancer risk calculators see for more on the challenges of supporting patients with multiple morbidities see articles lancet 2012 ; published online may 10 . 
a third of all young cancer patients reported their gps took no action despite presentation with common cancer symptoms and a quarter of patients had to visit the gp four or more times before their symptoms were taken seriously . 
if a young person presents with the same symptoms three times , gps should automatically refer them for further investigation . although the tct survey was small ( collating the opinions of only 300 patients ) , the ndings mirror those of lyratzopoulos and colleagues published in the lancet oncology in april , 2012 , that analysed more than 41 000 patients with 24 types of cancer . 
in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
 so what can be done to restore trust ? usefully , cancer research uk and the royal college of general practitioners have launched an initiative to support gps by putting together models of best practice , and by reviewing care pathways and thresholds for further investigation to ensure gps have better access to diagnostics and secondary care . 
 additionally , the department of health has announced a pilot project within gp practices of cancer - risk prediction tools ( qcancer risk calculators ) developed by researchers at the university of nottingha these successful these partnerships are good examples of engagement between policy makers and physicians with organisations that have a perceptive understanding of the patient viewpoint and of research realities and possibilities . 
 initiatives will be whether transforming the e ectiveness of the gp and improving patient care will take time to assess , but it is unlikely that they will prove to be a broad panacea . 
it is becoming increasingly clear , for example , that the uk health - care system is not designed to cope with multiple comorbiditiesa common situation among patients with cancerand in the future gps will need to take a central and proactive role in coordinating patient care throughout their entire journey within the national health service . 
this will require rethinking of the current infrastructure , and might require adjustments to gps case burdens to ensure su cient time is available for more thorough consultations , especially in socioeconomically deprived areas . while the role of the gp in cancer diagnosis is undeniably important , it is essential not to forget interdependency on improved patient education , screening , secondary care and access to latest treatments , supportive and palliative care , and coordinated long - term follow - up . 
 improved understanding of the factors contributing to the di erences between the uks cancer outcomes and those of other countries will provide important clues and solutions . 800 000 people visit a gp every day in the uk , but questions are increasingly being asked about the competency of those doctors that undermine patient trust . 
however , implementation of this bill could be a fresh start in a process of restoring trust and ensuring gps have access to the best tools necessary to provide a rst - class service and to guarantee all patients receive the best possible care . 
overall e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against grade 3 or greater cervical intraepithelial neoplasia : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 8999in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
cross - protective e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against cervical infection and precancer caused by non - vaccine oncogenic hpv types : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 10010in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
lancet oncol 2012 ; 13 : 1012in this comment ( published online nov 9 , 2011 ) , the last sentence of the sixth paragraph incorrectly lists hpv - 35 as one of the oncogenic hpv types covered by the new nine - type gardasil vaccine ; the list should include hpv - 45 instead . 
this correction has been made to the online version as of jan 3 , 2012 . vol 13 january 2012 editorial evolution : the lancet oncologyan online - enhanced journal long - standing readers of the lancet oncology will have noticed changes in the journal over the years . 
as a result , we strongly encourage print readers to activate their online accounts , and for all our online - only subscribers to check the website regularly for new content . why are we doing this ? since 2005 , the lancet oncology has seen a 70% increase in the number of articles submitted from the united states , europe , and asia . 
furthermore , because cancer is fast becoming the number one cause of death in many countries , there is an ever - pressing demand for more information and rapid dissemination of ndings . 
having an online focus will also better align the journal with the majority of our readers main way of accessing content . what will change ? editorials , comment , cancer and society , and articles will continue in print and online . 
 correspondence , reviews , historical reviews , personal views , and health - care development articles will become online - only content , but the quantity will increase from the monthly current average of two to three , to four to ve . 
finally , podcasts will feature interviews with authors and will be published on the same day as the corresponding article . we hope you share our enthusiasm for the new feel of the journal and we look forward to bringing you even more of the high - quality material youve come to expect of the lancet oncology in the months and years ahead . 
 the lancet oncology budget cuts in the usa : a short - term win ? on nov 18 , 2011 , president barack obama signed a bill into law that will a ect the funding for several science agencies . 
the white house o ce of science and technology policy , which advices the executive o ce about the e ects of science and technology on domestic and international a airs , has had its funding cut by more than 30% , leaving just $45 million . 
the usas budget cuts to quell the national de cit of $12 trillion by 2021 mean that several key agencies such as the national institutes of health ( nih ) and national science foundation had below - in ation increases to their funding . 
such reductions in funding might not bode well for federally funded organisationsincluding the nih and centers for disease control and prevention ( cdc ) that fund much of the cancer research in the usa . the budget cuts also extend to preventive measures , which are needed in addition to funding for research into the causes of and treatments for cancers . 
the cdc has recommended a total of $37 billion in funding for tobacco prevention programmes , but collectively individual states have only budgeted $4567 million ( 12% ) of this amount . if the usa is to remain a world leader in terms of research , any budget cuts to cancer research and prevention programmes need to be implemented judiciously because although the short - term win of saving a few dollars will look good on a budget sheet , it will not translate into medium - term and long - term solutions of stopping the rising burden of cancer . 
the usa need only look at ireland , which even in austere times , is providing improved care for patients as a result of a reorganisation of its health structures into specialist centres . 
 the lancet oncology see news page 17 for more on cuts to tobacco prevention funding see releases / post / 2011_11_30_ state_report for more on the white house o ce of science and technology policy budget cut see chemistryworld / news / 2011 / november / 21111101.asp for more on the usas budget cuts see com / news / what - does - the - usbudget - stalemate - mean - forresearch - 1.9475 for more on the rising burden of cancer see the lancet oncology commission thelancet.com / commission / delivering - a ordable - cancercare - in - high - income - countries vol 13 january 2012 editorial for the ntps 12th report on carcinogens see niehs.nih.gov / ntp / roc / twelfth / pro les / formaldehyde.pdf for the acc letter see policy / regulatory - reform / acc - letter - to - house - sciencecommittee - regarding - jointhearing - on - the - report - oncarcinogens.pdf for the addendum to the ntps 12th report see nih.gov / ntp / roc / twelfth / addendum.pdf for the iarc monograph on carginogens see iarc.fr / en / publications / pdfsonline / monographs / index.php for more on who and unicefs consultation see comment lancet 2012 ; 380 : 1214 carcinogenicity assessments : who decides ? a column in the new york times in september , 2012 , drew attention to an attempt by the american chemistry council ( acc ) , a body representing the interests of the chemical industry in the usa , to put funding for the national toxicology programs ( ntp ) 13th report on carcinogens on hold . 
the acc wrote a letter to congress in april , 2012 , contesting the change of listing in the 12th version of the report about formaldehyde , which is widely used in manufactured products , from reasonably anticipated to be a human carcinogen to known to be a human carcinogen , citing inconsistencies between various bodies in their methods of carcinogen reporting . 
 they state that some aspects of a similar classi cation by an environmental protection ag ency ( epa ) report was not found to be scienti cally justi ed by a government commissioned review . 
 this justi cation , based on inter - departmental incon sistencies , raises a wider question about the duplication of work by di erent organisations and who the reporting bodies should be accountable to . in their letter , the acc describe awed science and duplicative procedures that they claim lead to confusing messages . 
the epa report that listed formaldehyde as a carcinogen was reviewed by a panel from the national academy of sciences who , according to the acc , found that the epa had not justi ed its conclusion that formaldehyde causes leukaemia . 
the ntps 12th report has an addendum acknowledging the review , but state that the national academy had not been tasked to do an independent hazard assessment and their ndings had restricted applicability to the 13th report on carcinogens . 
in september , 2012 , 76 occupational and health scientists wrote a letter to congress to point out that whos international agency for research into cancer ( iarc ) monograph on carcinogens also describes formaldehyde as a human carcinogen , thus supporting the epa and ntp reports . 
the acc expresses concerns about the redundancy in a system that they claim has overlapping reporting of substances ( with di erent assessment methods ) between the ntp , epa , centers for disease control and prevention , and agency for toxic substances and disease registryall of which are under the control of di erent federal agencies . 
any methodological or report discrepancies can be exploited by lobbyists like the acc and because these agencies are all housed within us government agencies , they are vulnerable to lobbying organisations who can garner political in uence , in this case , to suppress fundings . the amount of duplicative reporting in the usa can be ampli ed across the world . 
although carcinogen research should certainly be undertaken by di erent institutions around the world , the review of carcinogen status only really needs to be done by a single international organisation with standardised , robust methods . 
 it is notable that the 76 scienti c experts supporting the epa and ntp reports emphasised the iarc monograph on carcinogens as de nitive evidence that the ntps report is scienti cally robust and in accordance with global authoritative bodies . 
this comes at a time when who is reforming itself to better de ne its role in the world and is actively engaging with the global community to shape its future through a consultation process . 
perhaps global responsibility for carcinogen reporting should be ceded to iarc , under a revised remit for who , and then government policy on cancer risk from substances can focus on how to safeguard health and not whether the method of the assessment was sound . 
combining , rather than duplicating , scienti c e orts in an environment independent from policy and industry lobbyists , should be a future aspiration in which who could take a central and leading role . 
 the lancet oncology vol 13 november 2012 1063 corrections correction to lancet oncol 2011 ; 12 : 531 , 532 bonnefoi h , piccart m , bogaerts j , et al , on behalf of the eortc 10994 / big 1 - 00 study investigators . 
tp53 status for prediction of sensitivity to taxane versus non - taxane neoadjuvant chemotherapy in breast cancer ( eortc 10994 / big 1 - 00 ) : a randomised phase 3 trial . 
 lancet oncol 2011 ; 12 : 52739in this article , table 2 was incorrect and should have been as shown below . accordingly , the third paragraph of the results section should have read by february , 2010 , 675 primary had occurred , endpoint of which 420 ( 62% ) were distant recurrences ( table 2 )  . 
this correction has been made to the online version as of jan 28 , 2013 . events fec ( n = 361 ) * t - et ( n = 314 ) * progression while on neoadjuvant chemotherapy 56 ( 16% ) distant recurrence invasive locoregional recurrence invasive contralateral cancer death without previous report of progression 219 ( 61% ) 59 ( 16% ) 14 ( 4% ) 13 ( 4% ) progression treatment toxicity cancer ( non - breast ) cardiovascular other not known 49 ( 16% ) 201 ( 64% ) 42 ( 13% ) 13 ( 4% ) 9 ( 3% ) data are number ( % ) or number . 
deaths occurring during chemotherapy or within 30 days of chemotherapy completion and without disease relapse . table 2 : first events contributing to progression - free survival correction to lancet oncol 2013 ; 14 : 88 , 89 , 95 goss pe , smith ie , oshaughnessy j , et al , on behalf of the teach investigators . 
 lancet oncol 2013 ; 14 : 8896the second sentence of the methods in the summary should read women outpatients 33 countries with her2 - positive earlybreast cancer who had previously received chemotherapy but not trastuzumab were randomly from 405 centres adjuvant assigned ( 1 : 1 ) to receive daily lapatinib ( 1500 mg ) or daily placebo for 12 months , and the second sentence of the study design and participants section , should read participants were hospital outpatients at 405 centres in 33 countries worldwide . 
 the online version was corrected on jan 28 , 2013 . vol 14 february 2013 editorial for more on the fdas approval of bevacizumab in 2008 see leading edge lancet oncol 2010 ; 11 : 805 for more on the in uence of public debate on bevacizumabs approval see news lancet oncol 2011 ; 12 : 730 for more on the sharing of information between patients see cancer and society lancet oncol 2012 ; 13 : 13334 chasing the greenback and the decline in scienti c rigour the presentation of results from clinical trials at conferences and in the peer - reviewed literature is an important part of the scienti c process , serving as a venue to stimulate debate and to push research forward . 
what purpose does such early release of results serve , and should such practices be condoned ? a press release from roche on march 30 , 2012 , serves as an example of this approach , announcing headline results of the emilia trial , which compared the companys new drug , trastuzumab emtansine ( trastuzumab - dm1 ) , with lapatinib and capecitabine in women with her2 - positive breast cancer that had progressed after treatment with trastuzumab and a taxane - based chemotherapy regimen . 
however , this endpoint represents only one of three co - primary endpoints listed in the trials record on clinicaltrials.gov ( including safety and the clinically more important endpoint of overall survival , the data for which are apparently not yet mature )  . 
on the basis of these ndings , the company plans to submit for licensing to both the european medicines agency ( ema ) and the us food and drug administration ( fda ) , the latter of which refused accelerated approval of the drug in 2010 , led on the basis of phase 2 data . 
 while it is in the interests of the pharmaceutical industry to promote their new products and push for rapid licensing , particularly given the limits to the duration of patents and the need to recoup costs , one wonders who actually bene ts from prematurely releasing headline results . 
positive press releases also are serve to catch the attention of the public and patient advocacy movements , and in doing so , increase the pressure on regulatory agencies and governmental bodies to rush through approval of agents . 
this is a risky practicewithout disclosure of actual data or highlighting the full spectrum of endpoints , and bypassing the usual checks and balances of the peerreview process , hope can be falsely raised , without full awareness of the equilibrium between risks and bene ts . 
take , for instance , the decision of the fda to give the go - ahead to the use of bevacizumab for metastatic breast cancer on an accelerated approval programme in 2008 , counter to the recommendations of its oncology advisory panel , and the subsequent clash between public opinion and scienti c evidence that surrounded the withdrawal of this indication in 2011 as further data emerged showing insu cient e cacy . 
furthermore , the debate over the use of bevacizumab for patients with breast cancer still rages , providing confusion for patients and oncologists alike . early release of preliminary data may also affect the compliance of trial participants in adhering to longer term follow - up . 
for instance , discussion amongst patients via online communities and social media regarding the side - effect profiles of new drugs can result in educated guesses being made as to their treatment allocation . 
taken together with dripfed messages about positive findings , a patient might be encouraged to dropout of the trial follow - up in the pursuit of alternatives , or to crossover from the control arm to receive the experimental drug . 
 rapid access to the latest treatments is of paramount importance for patients , but not before agents are exposed to full scienti c rigour to ensure bene t and minimise harm for all concerned . 
the impact of data that have succeeded in convincing clinical peers will be sustainable beyond a short - lived bump in share prices , or worse , a later and potentially more costly disasterboth for patients and manufacturersif a drug is withdrawn as further data become available . 
 the lancet oncology vol 13 may 2012 editorial for the paho report see new.paho.org / hq / index.php ? option = com_docman&task = doc_ download&gid = 16836&itemid = for more on tobacco content in video games see cancer and society page 237 for the welsh government campaign see uk / newsroom / healthandsocial care / 2012 / 120206smoking / ? lang = en for the british medical associations policy brie ng see images / smokinginvehicles_v3_ tcm41 - 210651.pdf for more on laws banning smoking in vehicles carrying children see news / pdf / prevention.pdf tobacco control : time to protect children on feb 8 , 2012 , the pan american health organization ( paho ) published a report on tobacco control measures for the americas summarising the progress made in the implementation of the who framework convention on tobacco control ( fctc )  . 
signed by 168 countries in 2005 , the fctc requires state parties to apply a series of policies and measures aimed at reducing tobacco consumption , preventing young people from beginning to smoke , and protecting non - smokers from second - hand smoke ( shs )  . 
 although a growing number of south american countries are adopting e ective tobacco control policies , the paho report recommends further measures , particularly increases in tobacco taxes and bans on tobacco advertising . 
 such bans have reduced the amount of tobacco imagery in traditional media channels , but indirect advertising through new media is increasing ; targeting technology that has a large youth following . 
protection of children from smoking should be placed at the forefront of political agendas and , encouragingly , several countries , both within and outside the americas , have challenged the tobacco companies about such practices in recent years . tobacco advertising is known to be e ective in enticing new customers , and as traditional markets have shrunk , tobacco companies have used more inventive and under hand means to promote their products , increasingly targeting the child and teen markets . 
for example , as reported by barrientos - gutierrez and colleagues in this issue of the lancet oncology , the prevalence of tobacco content in video games in the usa , canada , and mexico , increased from 08% in 2005 to 126% in 2011 in games that are rated appropriate for 10 - year - olds and older . 
 however , while the protection of teenagers from indirect increased , protecting tobacco advertising should be children from tobacco smoke itself , and its associated carcinogens , should be placed even higher up national political agendas . 
article 8 of whos fctc calls for parties to take action to provide protection from exposure to tobacco smoke , and surely emphasis should be placed on the youngest members of societies , who perhaps are the most vulnerable biologically and psychologically . both the us environmental protection agency and the international agency for research on cancer have classi ed shs as a de nitive cause of cancer . 
the presence of shs in enclosed spaces , such as homes and vehicles , can result in signi cant morbidity for children , and increased hospital visits and health - care expenditures . 
since no level of shs exposure has been shown to be safe , parties should expand the scope of smoke - free legislation to include other locations where evidence exists to support such bans . 
 measures to protect children are gaining momentum and on feb 6 , 2012 , an educational campaign to stop people smoking in cars when children are present was launched by the welsh government . 
legislation will be considered depending on the success of the 3 - year campaign , although scant details on how success will be measured , or how this legislation will be enforced , have been provided . 
indeed , laws prohibiting smoking in vehicles carrying children have already been adopted in south africa , mauritius , bahrain , and puerto rico , and in several regions of canada , australia , and the usa . 
 the welsh proposal might be in the spirit of fctc recommendations , but it could be argued that the use of the law to enforce and legislate in this manner is the start of a slippery slope of state sanctions against peoples rights and freedoms . 
 furthermore , a broad range of antismoking initiatives has proved popular among the general population and has substantially reduced the numbers of individuals who smoke indoors , thereby decreasing shs in private spaces . 
 societies must protect those groups that are most vulnerable , whilst maintaining an individuals freedom of choice , and many countries have made great strides to achieve this di cult balancing act . 
 the lancet oncology vol 13 march 2012 e ects of zoledronic acid versus clodronic acid on skeletal morbidity in patients with newly diagnosed multiple myeloma ( mrc myeloma ix ) : secondary outcomes from a randomised controlled trial gareth j morgan * , j anthony child * , walter m gregory , alex j szubert , kim cocks , sue e bell , nuria navarro - coy , mark t drayson , roger g owen , sylvia feyler , a john ashcroft , fiona m ross , jennifer byrne , huw roddie , claudius rudin , gordon cook , graham h jackson , ping wu , faith e davies , on behalf of the national cancer research institute haematological oncology clinical studies group summary background bisphosphonates are the standard of care for reducing the risk of skeletal - related events in patients with bone lesions from multiple myeloma . 
here , we report the secondary outcomes relating to skeletal events . methods patients ( 18 years ) with newly diagnosed multiple myeloma were enrolled from 120 centres in the uk and received intensive or non - intensive antimyeloma treatment . 
a computer - generated randomisation sequence was used to allocate patients in a 1 : 1 ratio , through an automated telephone service to intravenous zoledronic acid ( 4 mg every 2128 days ) or oral clodronic acid ( 1600 mg / day ) , and the drugs were continued at least until disease progression . 
at a median follow - up of 37 years ( iqr 2947 ) , patients in the zoledronic acid group had a lower incidence of skeletal - related events than did those in the clodronic acid group ( 265 [ 27% ] vs 346 [ 35% ] , respectively ; hazard ratio 074 , 95% ci 062087 ; p = 00004 )  . 
zoledronic acid was also associated with a lower risk of any skeletal - related event in the subsets of patients with ( 233 [ 35% ] of 668 vs 292 [ 43% ] of 682 with clodronic acid ; 077 , 065092 ; p = 00038 ) and without bone lesions at baseline ( 29 [ 10% ] of 302 vs 48 [ 17% ] of 276 with clodronic acid ; 053 , 033084 ; p = 00068 )  . 
fewer patients in the zoledronic acid group had vertebral fractures than did those in the clodronic acid group ( 50 [ 5% ] in the zoledronic acid group vs 88 [ 9% ] in the clodronic acid group ; p = 00008 ) , other fractures ( 45 [ 5% ] vs 66 [ 7% ] ; p = 004 ) , and new osteolytic lesions ( 46 [ 5% ] vs 95 [ 10% ] ; p < 00001 )  . 
 interpretation the results of this study support the early use of zoledronic acid rather than clodronic acid in patients with newly diagnosed multiple myeloma for the prevention of skeletal - related events , irrespective of bone disease status at baseline . funding medical research council ( london , uk ) , novartis , schering health care , chugai , pharmion , celgene , and ortho biotech . introduction multiple myeloma , which is diagnosed in more than 100 000 people every year , 1 is characterised by the growth of malignant plasma cells in the bone marrow.2 , 3 interactions between myeloma cells and bone marrow stromal cells are fundamental to the excessive activation and proliferation of osteoclasts , causing localised bone destruction.4 myeloma cells also secrete factors that inhibit osteoblasts , blocking the repair of osteolytic damage . 
results from this trial showed that patients given zoledronic acid had signi cantly improved progression - free survival ( hazard ratio [ hr ] 088 , 95% ci 080098 ; p = 00179 ) and a reduced risk of death ( 084 , 074096 ; p = 00118 ) versus clodronic acid , with overall survival prolonged by 55 months.12 importantly , improved overall survival with zoledronic acid remained signi cant after adjustment for the e ect of skeletal - related events that ( 085 , 074097 ; p = 0018 ) , suggesting zoledronic acid has direct antimyeloma activity . 
in this analysis , we investigated in detail the e ects of clodronic acid and zoledronic acid on skeletal - related events in patients with newly diagnosed multiple myeloma . methods trial design the mrc myeloma ix trial was a multicentre ( n = 120 ) , randomised , open - label , two - by - two factorial trial , with 1970 patients with newly diagnosed multiple myeloma randomly assigned to bisphosphonates 1960 analysed ( intention - to - treat population ) 979 clodrononic and cvad , ctd , mp , or ctda 981 zoledronic acid and cvad , ctd , mp , or ctda 917 started clodronic acid 11 started zoledronic acid 15 started pamidronic acid 0 started etidronic acid 31 bisphosphonate not initiated 5 bisphosphonate not conrmed 887 started zoledronic acid 25 started clodronic acid 14 started pamidronic acid 1 started etidronic acid 45 bisphosphonate not initiated 9 bisphosphonate not conrmed 820 randomly assigned to thalidomide maintenance or watchful waiting 2 excluded 1 no consent 1 withdrew consent 408 thalidomide 410 no thalidomide 195 clodronic acid 213 zoledronic acid 195 clodronic acid 215 zoledronic acid figure 1 : trial pro le the complete trial protocol is provided in morgan and colleagues.12 cvad = cyclophosphamide , vincristine , doxorubicin , and dexamethasone . 
full details have already been reported.12 patients adult patients ( 18 years ) with newly diagnosed and histologically con rmed symptomatic multiple myeloma were eligible for inclusion in the trial . 
 exclusion criteria included previous or concurrent active tumours , acute renal failure ( de ned as serum creatinine concentration > 500 mol / l that was unresponsive to 72 h of rehydration , urine output < 400 ml / day , or requirement for dialysis ) , and previous treatment for multiple myeloma ( except local radiotherapy for bone pain or spinal cord compression , bisphosphonates for hypercalcaemia of malignancy , or low - dose corticosteroids )  . the trial was approved by the north west multi - centre research ethics committee and local review committees at all participating centres . 
all patients provided written informed consent . randomisation and masking the methods of randomisation and masking for this study have been previously described in detail.12 brie y , a computer - generated randomisation sequence was used to allocate patients in a 1 : 1 ratio by use of an automated telephone service to zoledronic acid or clodronic acid . 
 no investigators , sta , or patients were masked to treatment allocation . treatment patients were allocated to two main treatment pathways ( intensive and non - intensive ) , as previously described in detail.12 in each pathway , patients were randomly assigned to oral clodronic acid ( 1600 mg / day ) or intravenous zoledronic acid ( 4 mg , 15 min infusion every 34 weeks with induction chemotherapy and every 4 weeks thereafter )  . 
dose adjustment for patients with impaired renal function at baseline and delays in administration of the dose in patients with increases in serum creatinine concentration during the study were implemented for zoledronic acid , per the prescribing information . 
data for skeletal - related events , de ned as vertebral fractures , other fractures , spinal cord compression , need for radiation or surgery for bone lesions , and new osteolytic lesions , were analysed until disease progression . 
 these included bone fracture , radiation to bone , surgery for bone lesions and spinal cord compression , and height loss ( as an indicator for further imaging follow - up )  . 
additional prespeci ed analyses of hypercalcaemia of malignancy and exploratory analyses of skeletal - related events , excluding the development of new osteolytic lesions , were undertaken . statistical analysis the primary endpoints of progression - free survival , overall survival , and overall response rate , and the secondary endpoint of safety have been reported previously.12 here , we report the secondary endpoint of skeletal - related events . 
in the intensive pathway , we aimed to recruit 1080 patients ( 540 per group ) to test the hypothesis that cyclophosphamide , thalidomide , and dexamethasone ( ctd ) was not inferior to cyclo phosphamide , vincristine , doxorubicin , and dexamethasone ( cvad ) , with a hazard ratio of 12 and 80% power at a 5% signi cance level . 
in the non - intensive pathway , we aimed to recruit 850 patients ( 425 per group ) to assess whether attenuated ctd ( ctda ) was superior to standard chemotherapy with melphalan plus prednisolone , with 80% power at a 5% signi cance level . 
we calculated that the sample size for the intensive and non - intensive pathways combined had su cient power ( > 80% ) to detect a reduction of 10% in the proportion of patients with skeletal - related events for zoledronic acid compared with clodronic acid . analyses were based on the treatment that patients with histologically con rmed multiple myeloma who provided written informed consent were randomly assigned to receive ( intention - to - treat population )  . 
data , in part , from morgan and colleagues.12 table 1 : baseline demographics and disease characteristics of the intention - to - treat population clodronic acid zoledronic acid hr 074 ( 95% ci 062087 ) ; p = 00004 * number at risk clodronic acid zoledronic acid time from randomisation ( months ) hr 053 ( 95% ci 033084 ) ; log - rank p = 00068 hr 077 ( 95% ci 065092 ) ; log - rank p = 00038 time from randomisation ( months ) time from randomisation ( months ) number at risk clodronic acid zoledronic acid figure 2 : time to rst skeletal - related event overall ( a ) , in patients with bone lesions at baseline ( b ) , and in patients without bone lesions at baseline ( c ) hr = hazard ratio . 
to reduce the potential e ects of related skeletal - related events ( eg , a fracture requiring surgery ) in multiple - event analyses , only one skeletal - related event per 21 days was included ( eg , skeletal - related events of possibly linked causality were counted only once , and judged to be one skeletal - related event )  . 
post - hoc analyses that included all skeletal - related events irrespective of whether they were the rst or subsequent skeletal - related events within 21 days ( not reported ) were done and provided results consistent with those in which the linked events were counted as one skeletal - related event . 
all hypothesis tests were the 5% signi cance level , without adjustment for multiplicity . this trial is registered , number isrctn68454111 . two - sided and undertaken at role of the funding source no funding organisation was involved in study design , data collection , data analysis or interpretation , writing , or decision about publication submission . 
all authors had full access to trial data ; gjm , jac , and ghj had nal responsibility for the decision to submit for publication . results 1970 patients were enrolled between may 14 , 2003 , and nov 20 , 2007 , and 1960 were the intention - to - treat population ( gure 1 )  . 
baseline demographics and disease characteristics of patients were well balanced between the zoledronic acid and clodronic acid groups ( table 1 ) .12 1898 ( 97% ) of 1960 patients were white , 1401 ( 71% ) had myeloma bone disease at baseline , 562 ( 29% ) had a history of vertebral fractures , 231 ( 12% ) had previous non - vertebral fractures , 1010 ( 52% ) had been diagnosed with osteolytic lesions , and 258 ( 13% ) had previous radiotherapy ( table 1 )  . 
median follow - up was 37 years ( iqr 2847 ) for patients in the zoledronic acid group and 38 years ( 2947 ) for those in the clodronic acid group ; 582 ( 30% ) patients had been given zoledronic acid or clodronic acid for at least 2 years ( 290 [ 30% ] of 981 in the zoledronic acid group and 292 [ 30% ] of 979 in the clodronic acid group )  . 
in the overall patient population , fewer patients assigned to zoledronic acid had a skeletal - related event than did those assigned to clodronic acid ( 265 [ 27% ] of 981 vs 346 [ 35% ] of 979 , respectively ) , with zoledronic acid signi cantly reducing the risk of skeletal - related events versus clodronic acid 746 vol 12 august 2011 articles skeletal - related events incidence ( 95% ci ) overall di erence ( 95% ci ) between clodronic acid and zoledronic acid * p value for preceding 12 months clodronic acid ( n = 979 ) zoledronic acid ( n = 981 ) clodronic acid ( n = 979 ) zoledronic acid ( n = 981 ) 12 months 24 months 36 months 48 months 60 months 451 ( 46% ) 333 ( 34% ) 043 ( 038048 ) 033 ( 028037 ) 011 ( 004018 ) 93 ( 9% ) 28 ( 3% ) 13 ( 1% ) 2 ( < 1% ) 54 ( 6% ) 16 ( 2% ) 4 ( < 1% ) 2 ( < 1% ) 060 ( 053066 ) 042 ( 036048 ) 018 ( 009026 ) 069 ( 061078 ) 047 ( 040053 ) 023 ( 012033 ) 080 ( 068091 ) 049 ( 042056 ) 030 ( 017044 ) 083 ( 070095 ) 051 ( 043058 ) 032 ( 018046 ) 00002 00024 00089 00510 05359 data are number ( % ) , unless otherwise indicated . 
unadjusted p value for the comparison of incidence of skeletal - related events in zoledronic acid group versus clodronic acid group per 12 months ( eg , 24 - month p value is for incidence between 12 months and 24 months )  . table 2 : cumulative annual incidence of rst and subsequent skeletal - related events for the intention - to - treat population after randomisation clodronic acid zoledronic acid ( gure 2a )  . 
the total number of skeletal - related events reported was also lower in the zoledronic acid group than in the clodronic acid group ( 419 vs 597 , respectively )  . 
the proportion of patients with at least one skeletal - related event was consistently lower in the zoledronic acid group versus the clodronic acid group at each timepoint ( p < 00001 overall ; table 2 )  . 
the di erence in incidences of skeletal - related events for zoledronic acid versus clodronic acid was signi cant for each of the rst 3 years separately , but the total number of skeletalrelated events was low at 48 months and 60 months , and reduced the statistical power for the respective 12 - month comparisons ( table 2 )  . 
similar distributions of skeletalrelated events were noted for patients treated with zoledronic acid and clodronic acid in the intensive ( zoledronic acid , 155 [ 28% ] of 555 ; clodronic acid , 202 [ 36% ] of 556 ; log - rank p = 0003 ) and non - intensive pathways ( zoledronic acid , 110 [ 26% ] of 426 ; clodronic acid , 144 [ 34% ] of 423 ; log - rank p = 0008 )  . 
the mean skeletal morbidity rate was lower with zoledronic acid versus clodronic acid in the intensive and non - intensive pathways ( 04 skeletal - related events per patient per year vs 08 per patient per year , respectively )  . 
however , patients who did not have myeloma bone disease at baseline had lower rates of bone pain ( 248 [ 43% ] of 578 vs 1136 [ 84% ] of 1350 ) , and higher rates of anaemia ( 330 [ 57% ] vs 523 [ 39% ] ) , renal failure ( 96 [ 17% ] vs 171 [ 13% ] ) , and infection ( 74 [ 13% ] vs 90 [ 7% ] ) than did patients with bone disease at baseline . in an exploratory analysis that excluded new osteolytic lesions from the de nition of skeletal - related event , the outcome was similar to the analysis that included new osteolytic lesions , and the reduction in risk of skeletalrelated events with zoledronic acid was still signi cant ( hr 076 , 95% ci 064089 ; log - rank p = 00011 )  . 
 further exploratory analysis by patients risk of skeletalrelated events , as identi ed in another assessment of the myeloma ix patients , 16 showed a reduced risk of p < 00001 p = 0070 any skeletal - related event except hypercalcaemia of malignancy p = 00031 p < 00001 p = 037 p = 00008 p = 0040 p = 029 radiotherapy lesion surgery to bone vertebral fracture other fracture spinal cord compresssion p = 00069 p = 022 p < 00001 p = 023 p = 0035 any skeletal - related event except hypercalcaemia of malignancy radiotherapy lesion radiotherapy lesion any skeletal - related event except hypercalcaemia of malignancy figure 3 : proportion of patients with an on - study skeletal - related event overall ( a ) , with bone lesions at baseline ( b ) , and without bone lesions at baseline ( c ) skeletal - related events with zoledronic acid versus clodronic acid in the high - risk and low - risk populations ( data not shown )  . 
analysis by cytogenetic markers ( poor prognosis de ned by use of uorescence in - situ hybridisation [ fish ] as adverse igh translocations , gain of 1q , and loss of 17p ) showed that the bene t vol 12 august 2011 articles ctda vs melphalan + prednisolone ( non - intensive pathway ) 075 ( 060094 ) zoledronic acid vs clodronic acid ctd vs cvad ( intensive pathway ) serum calcium concentration ( high vs low ) serum creatinine concentration ( high vs low ) haemoglobin concentration ( high vs low ) platelets ( high vs low ) skeletal - related events at baseline * no vs yes missing vs yes centre hazard ratio ( 95% ci ) p value 072 ( 062084 ) 091 ( 076110 ) 131 ( 111155 ) 093 ( 077112 ) 108 ( 092126 ) 119 ( 093153 ) 035 ( 028044 ) 083 ( 046152 ) < 00001 03399 00141 00012 04362 03489 01623 < 00001 05532 < 00001 ctd = cyclophosphamide , thalidomide , and dexamethasone . 
overall p value , but not hazard ratio , reported for 120 centres . table 3 : multivariate model for risk of skeletal - related events associated with zoledronic acid in terms of skeletalrelated events was attributable to the non - poor prognosis subset , 16 wherein the bene ts of zoledronic acid were especially meaningful ( log - rank p = 00012 ; data not the poor - prognosis subset , disease shown )  . 
 progression was fairly rapid , and very few patients were assessable for the time to rst skeletal - related - event endpoint at later timepoints ( 48 months and 60 months ; data not shown )  . 
 in an exploratory analysis , patients with osteolytic lesions at baseline showed a non - signi cantly longer progression - free survival than did those with no osteolytic lesions ( 20 months , 95% ci 1821 , vs 18 months , 1719 , hr 090 , 082100 ; p = 00535 )  . 
however , patients with bone disease at baseline had a higher incidence of skeletal - related events than did those without bone disease at baseline ( 525 [ 39% ] of 1350 vs 77 [ 13% ] of 578 , respectively ; p < 00001 )  . 
moreover , zoledronic acid , compared with clodronic acid , was associated with a signi cantly reduced risk of any skeletal - related event in patients with ( 233 [ 35% ] of 668 vs 292 [ 43% ] of 682 ; gure 2b ) and without bone disease at baseline ( 29 [ 10% ] of 302 vs 48 [ 17% ] of 276 ; gure 2c )  . 
zoledronic acid was associated with a reduced incidence of each type of skeletal - related event versus clodronic acid in the overall population ( gure 3a ) , and signi cant reductions were noted for any skeletal - related event ( 265 [ 27% ] of 981 vs 346 [ 35% ] of 979 for clodronic acid ; p < 00001 ) , new osteolytic lesions ( 46 [ 5% ] vs 95 [ 10% ] for clodronic acid ; p < 00001 ) , vertebral fractures ( 50 [ 5% ] vs 88 [ 9% ] for clodronic acid ; p = 00008 ) , and other fractures ( 45 [ 5% ] vs 66 [ 7% ] for clodronic acid ; p = 004 ) , but not radiotherapy ( 179 [ 18% ] vs 211 [ 22% ] for clodronic acid ; p = 007 ) , surgery to the bone ( 49 [ 5% ] vs 58 [ 6% ] for clodronic acid ; p = 037 ) , and spinal - cord compression ( 13 [ 1% ] vs 19 [ 2% ] for clodronic acid ; p = 029 )  . 
 zoledronic acid was associated with a signi cantly reduced incidence of any skeletal - related event in patients with ( gure 3b ) and without bone disease at baseline ( gure 3c )  . in a prespeci ed multivariate model of all on - study skeletal - related events , the reduction in such events with zoledronic acid versus clodronic acid remained signi cant ( table 3 )  . 
baseline serum calcium concentration , baseline skeletal - related event , melphalan plus prednisolone versus ctda ( in the non - intensive pathway ) , and treatment centre also showed signi cant correlations with risk of skeletalrelated events ( table 3 )  . 
overall , exclusion of new osteolytic lesions from the skeletal - related - events composite endpoint did not a ect model outcomes ( data not shown )  . results of further exploratory analyses showed that the proportion of patients with a skeletal - related event was signi cantly lower with zoledronic acid versus clodronic acid when the rst 12 months ( log - rank p = 00012 ) or 24 months ( log - rank p = 00102 ) were excluded from the analyses ( data not shown )  . 
furthermore , signi cantly fewer patients in the zoledronic acid group than in the clodronic acid group had at least one skeletal - related event after randomisation to maintenance thalidomide or no maintenance ( log - rank p = 00005 ; data not shown )  . 
 the incidences of most adverse events were similar in zoledronic acid and clodronic acid groups and have been previously reported.12 overall , the rates of acute renal failure were low and similar for patients in the zoledronic acid and clodronic acid groups ( 57 [ 6% ] of 983 [ two patients for whom con rmation of consent was not received were included in the safety population ] vs 60 [ 6% ] of 979 , respectively ; p = 078 )  . 
during the study , 47 ( 5% ) of 979 patients in the clodronic acid group and 43 ( 4% ) of 981 in the zoledronic acid group died of renal failure ( p = 067 ) , and 123 ( 13% ) patients in the clodronic acid group and 92 ( 9% ) in the zoledronic acid group died of multiple myeloma or treatmentrelated infections ( p = 0025 )  . 
28 ( 3% ) patients in the clodronic acid group and 28 ( 3% ) in the zoledronic acid group had hypercalcaemia , which was reported as a serious adverse event in six ( < 1% ) of 979 patients in the clodronic acid group and six ( < 1% ) of 983 in the zoledronic acid group . 
as previously reported , 12 con rmed osteonecrosis of the jaw was rare , but the rate was higher in the zoledronic acid group than in the clodronic acid group ( 35 [ 4% ] vs three [ < 1% ] , respectively ; p < 00001 )  . 
gastrointestinal serious adverse events were not signi cantly di erent with clodronic acid versus zoledronic acid ( 30 [ 3% ] vs 24 [ 2% ] , respectively ; p = 041 )  . 
 treatment - emergent serious adverse events that were suspected to be related to bisphosphonate use arose in 41 ( 45 events ) of 983 patients in the zoledronic acid group versus 33 ( 34 events ) of 979 patients in the clodronic acid group , and represented a subset of the overall treatmentemergent serious adverse events that were suspected to be 748 vol 12 august 2011 articles tenderness related to any of the study drugs as previously reported.12 in patients given zoledronic acid , treatment - emergent serious adverse events were musculoskeletal , connective tissue , and bone disorders ( n = 16 ) ; renal and urinary disorders ( n = 8 ) ; haematological disorders ( n = 5 ) ; gastrointestinal [ n = 1 ] , nausea and vomiting , disorders ( dehydration epigastric [ n = 1 ] , and nausea , vomiting , constipation , dehydration [ n = 1 ] ) ; endocrine , metabolism , or nutrition disorders ( n = 3 ) ; infections ( n = 3 ) ; cardiovascular disorders ( n = 2 ) ; skin and subcutaneous disorders ( n = 2 ) ; uid or electrolyte disturbance ( n = 1 ) ; general disorder or administration - site condition ( n = 1 ) ; and nervous system disorder ( n = 1 )  . 
in patients in the clodronic acid group , treatment - emergent events were gastrointestinal disorders ( diarrhoea [ n = 2 ] , abdominal pain and bloating [ n = 1 ] , nausea or vomiting [ n = 6 ] , oesophagitis [ n = 1 ] , haematemesis [ n = 1 ] , and gastrointestinal disturbance [ n = 1 ] ) ; renal and urinary disorders ( n = 9 ) ; infections ( n = 5 ) ; haematological disorders ( n = 2 ) ; skin and subcutaneous disorders ( n = 2 ) ; cardiovascular disorder ( n = 1 ) ; general disorder or administration - site condition ( n = 1 ) ; hepatic disorder ( n = 1 ) ; and reproductive system or breast disorder ( n = 1 )  . 
 adverse serious in progression - free discussion the results of the current analysis of the mrc myeloma ix trial show that zoledronic acid was associated with a signi cantly reduced risk of skeletal - related events versus clodronic acid in patients with newly diagnosed multiple myeloma irrespective of their bone disease status at baseline . 
additionally , zoledronic acid was associated with a reduced incidence of skeletal - related events in the intensive and non - intensive pathways , suggesting that all patients undergoing initial treatment for multiple myeloma could bene t from early use of zoledronic acid . 
 previous analyses showed that zoledronic acid was associated with a signi cant reduction in the risk of death ( hr 084 , 95% ci 074096 ; p = 00118 ) and a signi cant improvement ( 088 , 080098 ; p = 00179 ) , providing signi cant clinical bene ts and not just reduction in rates of skeletal - related events ( panel ) .12 although clinical guidelines recommend bisphosphonates for patients with documented bone lesions , 4 , 7 , 8 , 17 all patients ( ie , with or without bone disease at baseline ) could bene t when bisphosphonates are begun early in the course of multiple myeloma . 
moreover , the reductions in skeletal - related events with zoledronic acid versus clodronic acid noted throughout the course of the trial support the continued use of zoledronic acid in patients with multiple myeloma at least until disease progression , when patients went o study in this trial and data for skeletal - related events were no longer collected . 
however , the optimum duration of zoledronic acid is not known , and some patients might bene t from continuing zoledronic acid , possibly at a reduced dose , during disease remission . 
additional clinical trials are needed to further re ne these aspects of treatment . survival panel : research in context systematic review in addition to the experience obtained from previous mrc myeloma trials of clodronic acid , a review of the reports of clinical trials of a wide variety of combination chemotherapy regimens and bisphosphonates was undertaken and used to develop the 22 factorial trial design for the myeloma ix trial . 
at the time that the myeloma ix trial was initiated , most patients with symptomatic multiple myeloma in the uk were treated long - term with bisphosphonates ; however , there was no consensus for the optimum timing and duration of treatment with bisphosphonates , or the e cacy for prevention of skeletal - related events of all the available bisphosphonates and their potential to a ect disease outcomes and survival variables in patients with multiple myeloma . 
in the myeloma ix trial , we assessed the possible enhanced e ects on disease - related bone changes and survival of a third - generation bisphosphonate ( zoledronic acid ) in comparison with a standard older - generation oral agent ( clodronic acid )  . interpretation the results of the myeloma ix trial showed signi cant bene ts with zoledronic acid versus clodronic acid on progression - free survival , overall survival , and several variables for skeletal - related events , and , to our knowledge , for the rst time established the superiority of one bisphosphonate over another in patients with multiple myeloma . 
moreover , exploratory analyses have shown signi cant bene ts with treatment before the onset of bone lesions and also with long - term treatment ( eg , during maintenance therapy or long - term follow - up )  . 
the data from myeloma ix provide compelling evidence that zoledronic acid should be considered an essential component of therapeutic regimens for patients starting treatment for newly diagnosed multiple myeloma irrespective of whether bone lesions are already present , and support the continuation of zoledronic acid at least until disease progression . 
however , the results of this study do not provide insight into whether the frequency of dosing with zoledronic acid can be reduced after initial treatment , such as in patients with long - term remission of their disease . in patients with multiple myeloma , renal adverse events and osteonecrosis of the jaw are causes for concern and should be monitored and managed appropriately . 
indeed , because monitoring the concentrations of creatinine in vol 12 august 2011 articles ( ie , and reactions strategies that were colleagues13 ) the serum was less frequent for the clodronic acid group than for the zoledronic acid group ( ie , every 3 months vs monthly , respectively ) , any observation bias would be in favour of clodronic acid . 
this bias suggests that the renal adverse events reported in the myeloma ix trial were most likely a result of the disease , antimyeloma treatments , non - myeloma - related drugs , or other comorbidities rather than toxicity associated with bisphosphonates , validating the renal safety protocols for zoledronic acid . 
 recommendations for prevention and management of osteonecrosis of the jaw were implemented in myeloma ix from june , 2006 , onwards , 13 but further reductions in the risk of osteonecrosis of the jaw might be possible with prevention reported subsequently . 
the results of a study in postmenopausal women ( n = 7765 ) given intravenous zoledronic acid ( 5 mg per year ) for osteoporosis showed that the acutephase reaction lasted about 3 days and the incidence was similar to that with placebo by the third infusion.19 in myeloma ix , acute - phase reactions , which are thought to result from immune - cell activation after the rst infusion of zoledronic acid , might have been less frequent than in the postmenopausal osteoporosis setting because of the fairly high prevalence of disease and treatment - related myelosuppression in patients with multiple myeloma . 
gastrointestinal adverse events are generally more common in patients given oral bisphosphonates , as noted heregastrointestinal treatment - emergent serious adverse events arose more frequently with clodronic acid than with zoledronic acid ( 12 vs three events , respectively )  . 
 are serious , potentially debilitating complications a ecting most patients with multiple myeloma , especially those who do not receive bone - targeted therapy.6 bisphosphonates can e ectively reduce the risk of skeletal - related events in this population.2022 consequently , clinical practice guidelines and recommendations include bisphosphonates as a key component of disease treatment for patients with myeloma bone disease.4 , 78 , 17 in the previous mrc myeloma studies , 9 , 10 clodronic acid was of particular bene t ( ie , slowing progression of skeletal disease and reducing skeletal morbidity ) to patients without bone skeletal - related events lesions at treatment initiation.9 , 10 moreover , subgroup analysis suggested that clodronic acid might confer survival bene ts in patients without overt bone disease at diagnosis.10 three bisphosphonates have been approved for patients with osteolytic bone lesions from multiple myelomazoledronic acid and pamidronic acid in the usa and europe , and clodronic acid in europe . 
previous comparison of zoledronic acid with pamidronic acid in patients with multiple myeloma showed no signi cant di erence in the incidence of skeletal - related events ( 86 [ 47% ] of 183 vs 82 [ 49% ] of 167 , respectively ) , 20 or the time to rst skeletal - related event ( 380 days vs 286 days , respectively ; p = 0538 ) among patients with multiple lesions.21 the myeloma and established osteolytic more recently introduced nitrogen - containing bisphosphonates , pamidronic acid and zoledronic acid , are more potent inhibitors of osteoclastic activity than are the earlier , non - nitrogen - containing bisphosphonates ( eg , clodronic acid ) .23 however , pamidronic acid is more similar to clodronic acid in terms of antiresorptive potency than it is to zoledronic acid , which has more potent anticancer e ects in preclinical models of myeloma and other cancers.2325 because of the short infusion time and particular antiresorptive potency of zoledronic acid compared with pamidronic acid con rmed in preclinical and clinical investigationsit was adopted as the comparator for clodronic acid , a uk standard , in the myeloma ix trial . 
treatment regimens for multiple myeloma also changed between the completion of the trial of zoledronic acid versus pamidronic acid , 21 and the start of the myeloma ix trial . induction chemotherapy regimens used to treat patients with multiple myeloma are continually evolving as new drugs and new combinations are assessed in clinical trials . 
 in recent years , there has been interest in the potential for immunomodulatory drugs ( eg , lenalidomide ) and bortezomib to slow osteolytic bone destruction in multiple myeloma through inhibition of osteoclast activity , ( eg , bortezomib ) .2630 so far , these data are derived from preclinical clinical assessments of biochemical markers of bone resorption and bone mineral density and have not yet been correlated with a reduction in the risk of skeletal - related events . 
there is no evidence to suggest that antimyeloma treatment alone can replace bisphosphonates for treatment of multiple myeloma bone disease ; however , the potential for synergistic and between bisphosphonates is intriguing . 
on the basis of the data this study , for skeletal - related events obtained studies and osteoblast increased activity e ects drugs these and 750 vol 12 august 2011 articles zoledronic acid is very likely to provide clinically in combination with newer signi cant bene ts antimyeloma regimens because it has proved bene cial in the prevention of skeletal - related events in patients with solid tumours who were given a broad range of primary anticancer treatments.21 , 31 , 32 however , clinical studies are needed to con rm this theory . 
 the myeloma ix study is the rst large , independent clinical trial in patients with newly diagnosed multiple myeloma , and its results show unequivocal superiority of one bisphosphonate over another for reduction of the risk of skeletal - related events . 
overall , the data from this study support the early use of zoledronic acid for reduction in the risk of skeletal - related events in all patients with newly diagnosed multiple myeloma . contributors gjm , jac , and ghj were chief investigators . 
gjm , jac , wmg , kc , seb , ajs , nn - c , and pw contributed to writing the report , generation of tables and gures , or data interpretation . 
gjm developed an early draft , and all authors contributed to the review and amendments and approved the submitted report . con icts of interest gjm has participated on advisory boards for , received payment for lectures and development of educational presentations from , and received travel support from celgene , novartis , merck , and johnson and johnson . 
gc has received speakers fees from celgene and janssen - cilag , payment for the development of educational presentations from celgene , acted as a consultant for celgene , janssen - cilag , and novartis , and received travel support to attend meetings from celgene and janssen - cilag . 
 fed has participated on advisory boards and spoken at meetings for celgene , ortho biotech , and novartis , and has received travel support to attend meetings from celgene and ortho biotech . 
we thank all the patients , investigators , and sta who participated in the mrc myeloma ix trial ; sta at the clinical trials research unit , university of leeds , leeds , uk , for trial coordination and data management ; sta at the department of immunology , university of birmingham , birmingham , uk ; sta at wessex regional genetics laboratory , university of southampton , southampton , uk ; sta at haematological malignancy diagnostic service , leeds teaching hospitals nhs trust , leeds , uk ; sta at institute of cancer research , london , uk , for central laboratory investigations ; david bowen for independent safety oversight ; the mrc leukaemia data monitoring and ethics committee ; the mrc leukaemia trial steering committee ; the national cancer research institute haematological oncology clinical studies group ; myeloma uk ; the national institute for health research for support , through the national cancer research network ; the support of biomedical research centre at the royal marsden hospital ; lead investigators , as previously reported ; 12 and michael hobert ( proed communications , beachwood , oh , usa ) , for his medical editorial assistance with this report . 
 articles extra - pleural pneumonectomy versus no extra - pleural pneumonectomy for patients with malignant pleural mesothelioma : clinical outcomes of the mesothelioma and radical surgery ( mars ) randomised feasibility study tom treasure , loic lang - lazdunski , david waller , judith m bliss , carol tan , james entwisle , michael snee , mary obrien , gill thomas , suresh senan , ken obyrne , lucy s kilburn , james spicer , david landau , john edwards , gill coombes , liz darlison , julian peto , for the mars trialists * summary background the e ects of extra - pleural pneumonectomy ( epp ) on survival and quality of life in patients with malignant pleural mesothelioma have , to our knowledge , not been assessed in a randomised trial . 
we aimed to assess the clinical outcomes of patients who were randomly assigned to epp or no epp in the context of trimodal therapy in the mesothelioma and radical surgery ( mars ) feasibility study . methods mars was a multicentre randomised controlled trial in 12 uk hospitals . 
the main endpoints were feasibility of randomly assigning 50 patients in 1 year ( results detailed in another report ) , proportion randomised who received treatment , proportion eligible ( registered ) who proceeded to randomisation , perioperative mortality , and quality of life . 
this trial is registered , number isrctn95583524 . findings between oct 1 , 2005 , and nov 3 , 2008 , 112 patients were registered and 50 were subsequently randomly assigned : 24 to epp and 26 to no epp . 
the main reasons for not proceeding to randomisation were disease progression ( 33 patients ) , inoperability ( ve patients ) , and patient choice ( 19 patients )  . 
the hazard ratio [ hr ] for overall survival between the epp and no epp groups was 190 ( 95% ci 092393 ; exact p = 0082 ) , and after adjustment for sex , histological subtype , stage , and age at randomisation the hr was 275 ( 121626 ; p = 0016 )  . 
 of the 49 randomly assigned patients who consented to quality of life assessment ( epp n = 23 ; no epp n = 26 ) , 12 patients in the epp group and 19 in the no epp group completed the quality of life questionnaires . 
although median quality of life scores were lower in the epp group than the no epp group , no signi cant di erences between groups were reported in the quality of life analyses . 
there were ten serious adverse events reported in the epp group and two in the no epp group . interpretation in view of the high morbidity associated with epp in this trial and in other non - randomised studies a larger study is not feasible . 
these data , although limited , suggest that radical surgery in the form of epp within trimodal therapy o ers no bene t and possibly harms patients . funding cancer research uk ( cruk / 04 / 003 ) , the june hancock mesothelioma research fund , and guys and st thomas nhs foundation trust . introduction time when deaths from malignant pleural at a mesothelioma were rising in the uk1 , 2 and europe , 3 data from the uk thoracic surgical register of the society for cardiothoracic surgery in great britain and ireland showed that few patients were being o ered surgery for their disease . 
encouraging results from large case series had been reported for extrapleural pneumonectomy ( epp ) , 47 in which the lung and ipsilateral parietal pleura , pericardium , and hemidiaphragm are resected . 
 epp = extra - pleural pneumonectomy . in 2004 , we did a systematic review to assess the available evidence for e ectiveness of epp.8 median survival ranged from 17 to 35 months in seven surgical follow - up studies reported from 1999 to 2004 . 
the available data had been reported retrospectively on the basis of completed treatment and so measurement of the extent to which survival was in uenced by epp itself rather than the initial selection of treatment and subsequent progressive continued treatment in patients with a favourable prognosis was not possible . selection for to establish the e cacy of epp , we designed the mesothelioma and radical surgery ( mars ) trial.9 epp , within the context of trimodal therapy , was to be compared with induction chemotherapy but no epp . 
at the start of the trial , a power calculation , on the basis of the di erence claimed for e ectiveness of epp8 and natural history data , 10 suggested that 670 patients would be needed to identify any statistically signi cant di erence between epp and no epp with overall survival as the primary outcome . 
because of the anticipated di culty in recruiting patients , an initial feasibility study was done with the objective of randomising 50 patients within 1 year to epp or no epp to assess patient acceptability and to gauge the potential recruitment rate that could be expected in a larger trial . 
 randomisation between groups was possible but took longer than would be feasible to recruit su cient numbers to a de nitive trial.11 here we report the survival and quality of life outcomes of mars 2 years after recruitment was completed . methods patients the mars feasibility study was a multicentre randomised controlled trial with a prerandomisation registration phase and a two - stage consent process ( gure 1 )  . 
patients were eligible for registration if they were aged 18 years or older with pathologically con rmed mesothelioma and no evidence on preoperative ct staging of unresectable disease or distant metastases . 
they also had to be deemed t enough to undergo preoperative chemotherapy followed by pneumonectomy ( according to british thoracic society criteria for lung cancer surgery ) 12 and the planned postoperative radiotherapy . after chemotherapy , patients underwent restaging by ct . 
this team was chaired by the chief investigator , coordinated by the trial team at the institute of cancer research clinical trials and statistics unit the radiologist from the trial management group , the surgical coordinator , a medical and a radiation oncologist , and the designated mars trial surgeon . 
for each patient deemed eligible by the referring clinical team , clinical data and imaging reports were circulated to mars virtual multidisciplinary team members , and a teleconference ( icr - ctsu ; sutton , uk ) and included 764 vol 12 august 2011 articles was held to provide a consensus on whether that patient should be o ered randomisation . study centres were also asked ( but were not obliged ) to complete a screening log of all patients with mesothelioma to document the eligible population and calculate the proportion who agreed to enter the registration phase of the study . 
patients who ful lled eligibility criteria and who received chemotherapy outside of the trial , but in a manner consistent with the protocol , could also be registered for assessment of eligibility for randomisation by the mars virtual multidisciplinary team . mars was approved by cambridgeshire 4 research ethics committee ( mrec / 04 / 5 / 008 ) and was locally approved at all participating centres . randomisation and masking patients were informed of the mars virtual multidisciplinary team decision , and those still deemed eligible were invited to consent to be randomly assigned ( 1 : 1 ) to either epp followed by radical radiotherapy or to no epp . 
 we used the tnm staging system proposed by the international mesothelioma interest group.13 patients were eligible for randomisation if they had completed preoperative chemotherapy and still had operable disease de ned as t13 , n01 , m0 . registration and randomisation were done by telephone to the icr - ctsu . 
patients and investigators were not masked to treatment allocation . procedures patients assigned to epp underwent surgery at one of the participating surgical centres in accordance with the trial surgical protocol ( webappendix pp 12 )  . 
three other centres were added later ( northern general hospital , she eld , and st jamess university hospital , leeds , opened to recruitment in 2006 , but did not randomly assign an epp patient until 2007 ) , although in one there was no surgery within mars . 
all randomly assigned patients , including those in the no epp group , received continued oncological management according to local policy , which could include chemotherapy , palliative radiotherapy , or further surgery . we monitored acute and late radiotherapy e ects ( de nded in the webappendix p 5 ) , and collected clinical 257 ( 246 ) patients screening logs received screening logs not received 108 ( 97 ) patients approached 149 patients not approached 106 ineligible 30 clinical decision 12 other 1 unknown 40 patients not registered 18 ineligible 3 clinical decision 18 patient decision 1 other ( no radiological staging ) 112 ( 57 ) patients registered 68 ( 57 ) patients registered 44 patients registered 55 registrations not completed 27 disease progression 18 patient withdrawal 5 inoperable 4 other 1 died 57 reviewed by mdt 50 ( 24 ) randomised 7 excluded 6 disease progression 1 patient withdrawal 24 ( 13 ) randomly assigned to epp ( with radical radiotherapy ) 26 ( 11 ) randomly assigned to no epp figure 2 : feasibility of registration and recruitment to mars numbers in brackets indicate those patients screened who did not have chemotherapy before registration . 
mdt = multidisciplinary teaepp = extra - pleural pneumonectomy . see online for webappendix follow - up data including quality - of - life assessment by the european organisation for research and treatment of cancer and qlq - lc13 questionnaires at registration , randomisation , 6 weeks , 3 , 6 , 9 , 12 , 18 ( quality of life only ) , and 24 months , and annually thereafter . ( eortc ) qlq - c30 the aim of the mars feasibility study was to quantify the proportion of eligible patients subsequently randomised , to assess the feasibility of randomising 50 patients within 1 year , 11 and to measure clinical outcomes in randomly assigned patients . 
deaths were reviewed by the independent data monitoring committee for relatedness to trial treatment . statistical analysis the main analyses of the mars feasibility study were descriptive and included summary information from the screening logs on reasons for loss or withdrawal , the proportions of eligible patients registered and randomly assigned to treatment , and the proportion of randomly assigned patients who completed epp surgery . 
we also assessed treatment compliance , complications , perioperative mortality and quality of life . all analyses of randomly assigned patients were by intention to treat and were censored at the date last known to be alive . 
 hrs and 95% cis were calculated by cox proportional hazards regression , adjusting for the prespeci ed prognostic factors of sex , histological subtype , stage at randomisation , and age at randomisation . 
clinicians were free to choose the chemotherapy regimen as long as it included a platinum - based drug . table 2 : characteristics of patients subsequently randomly assigned to epp or no epp proportions are reported with two - sided 95% cis . 
this trial is registered , number isrctn95583524 . 766 vol 12 august 2011 role of the funding source the sponsor of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between oct 1 , 2005 and nov 3 , 2008 , 112 patients were registered , of whom 50 were subsequently randomly assigned to epp ( n = 24 ) or to no epp ( n = 26 ; gure 2 )  . 
62 patients ( 554% ) did not proceed to random allocation , mainly because of disease progression ( 33 patients ) , inoperability ( ve patients ) , or patient choice ( 19 patients )  . 12 centres submitted screening logs for 257 patients . 
of the 246 who were screened before any chemotherapy , 97 ( 394% , 95% ci 331457 ) were invited to enter the registration phase , 57 ( 232% , 180288 ) were registered , and 24 ( 98% , 64142 ) were subsequently randomised . 
136 of 257 ( 53% ) patients were excluded for clinical reasons ( ineligibility , clinical decision , disease progression , and inoperability ) before the patient was approached , 21 of 108 ( 19% ) were excluded before registration , and 39 of 112 ( 35% ) were excluded before randomisation . 
these data suggest an unavoidable cumulative ( 95% ci 706813 ) independent of patient withdrawal or other reasons . loss of 763% during the recruitment period an increasing number of patients were referred to mars centres for assessment for eligibility . 
44 patients were registered in this way , bypassing the screening log process , and therefore came from an unknown denominator . table 1 shows patient characteristics at registration for all 112 registered patients and the 50 who were subsequently randomised . 
seven patients had more than three cycles , two of whom were deemed eligible by the mars virtual multidisciplinary team and subsequently randomly assigned , and four patients had fewer than three cycles of chemotherapy , one of whom was subsequently randomly assigned . 
the most common chemotherapy regimen given was cisplatin and gemcitabine ( 38 of 94 ; 40% ) , followed by cisplatin and pemetrexed ( 24 ; 26% ) , and mitomycin , vinblastine , and cisplatin ( 20 ; 21% )  . 38 ( 76% ) of 50 patients subsequently randomly assigned to epp ( n = 18 ) or no epp ( n = 20 ) had pet - ct scan vol 12 august 2011 24 randomly assigned to epp ( with radical radiotherapy ) 16 completed epp surgery 5 epp surgery not started 3 patient refusal 2 clinical decision 3 epp surgery abandoned 1 perioperative death 2 unexpected disease progression 11 postoperative complications 1 reoperation plus cardiac plus 1 cardiac plus pulmonary plus pulmonary infection 1 cardiac plus pulmonary * 1 cardiac plus urine retention 2 pulmonary plus other 1 reoperation * 1 cardiac 3 other 8 radical radiotherapy not received 1 clinical decision 2 toxicity 2 disease progression 3 died 8 received radical radiotherapy figure 3 : feasibility of epp surgery and radical radiotherapy treatment epp = extra - pleural pneumonectomy . 
other complications were exible bronchoscopy or drain infection in pneumonectomy cavity ; ischaemic right leg requiring femoropopliteal bypass and eventual below knee amputation with culture - positive pneumonia needing mini tracheostomy . 
postoperative pain , low blood pressure , and intraoperative bleeding and further bleeding from chest drains postoperatively . 0 / 24 0 / 26 number of events / at risk no epp figure 4 : overall survival epp = extra - pleural pneumonectomy . time from randomisation ( months ) 8 / 16 3 / 24 3 / 12 4 / 20 articles no epp 5 / 11 articles ten each before randomisation , one assigned three , and one assigned one . 
there were two further deaths within the protocolde ned perioperative period , giving a total of three perioperative deaths in 24 ( 125% , 95% ci 27324 ) in patients randomised to epp by intention to treat and three perioperative deaths in 19 ( 158% , 34396 ) patients in whom epp was attempted . 
11 of 16 patients who were assigned to and completed epp surgery had at least one postoperative complication ( gure 3 )  . eight of the 16 patients who completed epp received radical radiotherapy , ve of whom had complications . 
 severe ( grade 3 or 4 ) acute radical radiotherapy sidee ects were rare : two patients had grade 3 fatigue and one had grade 3 pasevere late side - e ects were fatigue ( n = 1 , grade 3 ) , pneumonitis or dyspnoea ( n = 2 , grade 3 ) , and ascites ( n = 1 , grade 3 )  . 
this patient also had coexisting herpes retinitis and progressive di use changes on mri of the spinal cord outside the irradiated region and thus the diagnosis of radiation - induced myelopathy was excluded . 
two patients who had completed epp operation had further surgery to deal with thoracic space infection . 16 of the 26 patients randomly assigned to no epp received further oncological management : one received radiotherapy alone ; seven had further chemotherapy alone ; one had epp surgery o trial ; one had radiotherapy and chemotherapy ; one had radiotherapy and non - epp surgery ; two had chemotherapy and epp surgery o trial ; one had chemotherapy and cediranib ( as part of a phase 1 trial ) ; and two had radiotherapy , chemotherapy , and nonepp surgery . 
thus , three patients had epp o trial , 13 had further chemotherapy , ve had some form of radiotherapy , three had non - epp surgery , and ten received no further treatment . at a median from randomisation of 247 months ( iqr 216322 ) , 30 of 50 patients had died ( epp n = 17 ; no epp n = 13 ) ; four of these deaths ( three in the epp group and one in the no epp group ) occurred more than 18 months after randomisation . 
of the perioperative deaths in patients randomly assigned to epp , one had a follow - up number of events / at risk 0 / 24 time from randomisation ( months ) 9 / 15 number of events / at risk 0 / 26 time from randomisation ( months ) 6 / 21 9 / 12 figure 5 : recurrence - free and progression - free survival recurrence - free survival in patients randomised to epp ( a ) and progression - free survival in patients randomly assigned to no epp ( b )  . 
epp = extra - pleural pneumonectomy . information available for the mars virtual multidisciplinary tea pet - ct scan results suggested that 23 patients ( ten epp and 13 no epp ) were resectable , ve ( four epp and one no epp ) were equivocal , and in ten patients ( four epp and six no epp ) this information was not available . 
no di erences in terms of stage or other patient - related features were noted between the two groups . of the 24 patients randomly assigned to epp , ve did not proceed to surgery : three by patient choice and two by clinician decision ( gure 3 )  . 
 four surgeons did the epp operations : two were assigned 768 vol 12 august 2011 articles no epp 833 800 833 833 750 1000 900 700 600 500 400 300 200 100 numbers with completed questionnaires returned / at risk no epp figure 6 : quality of life 750 333 667 667 542 583 750 583 708 667 667 583 500 417 registration randomisation 6 weeks 3 months 6 months 9 months 12 months 18 months 24 months time 20 / 23 19 / 26 12 / 23 19 / 26 5 / 21 6 / 26 11 / 17 22 / 25 9 / 13 17 / 22 8 / 10 15 / 18 5 / 10 10 / 13 rupture of the aortic isthmus ( multiple sites ) and died on the operating table ; one died at home ( cause unknown ) shortly after a further operation to have a diaphragm patch repaired ; and one died of bronchopneumonia 6 weeks after the epp operation . 
the perioperative death in the no epp group was one of the patients who underwent epp surgery outside the trial ; the patient died of multiple organ failure . 12 - month survival was 522% ( 95% ci 305700 ) in those allocated epp and 731% ( 517862 ) in those allocated to no epp ( di erence 180% , 18 to 439 ; gure 4 )  . 
the hazard ratio for overall survival in the epp group ( unadjusted ) versus the no epp group was 190 ( 95% ci 092393 ; exact p = 0082 )  . 
none of the three longterm survivors allocated to no epp crossed over to epp . 42 of 50 patients ( epp n = 19 , no epp n = 23 ; four from the no epp group had an event more than 18 months after random allocation ) had disease recurrence ( epp group ) , progression ( no epp group ) , or died before relapse or progression ( gure 5 )  . 
12 - month progression - free survival in the no epp group was 423% ( 235600 ) and median progression - free survival was estimated to be 90 months ( 72147 )  . 23 patients in the epp group and 26 in the no epp group consented to quality - of - life assessment and 12 and 19 patients completed the quality - of - life questionnaires , respectively . 
median quality - of - life scores seemed to be lower for the epp group than the no epp group , with the lowest median score shortly after surgery ( gure 6 ) ; however , there were no statistically signi cant di erences between treatment groups . 12 serious adverse events were reported during the study period : ten in the epp group and two in the no epp group . 
three were suspected unexpected serious adverse reactions ( two in the epp group and one in the no epp group ) , eight were serious adverse reactions ( all in the epp group ) , and there was one other serious adverse event in the no epp group . discussion in an intention - to - treat analysis of outcome data in the mars trial , we noted no survival advantage for the epp surgery group compared with the no epp group . 
in summary , the outcomes of mars provide no evidence of bene t therapy over chemotherapy alone , for survival or quality of life . from epp within trimodal survival data for epp were provided in a recent systematic review , 14 which allows us to put the epp survival data from mars in context ( panel )  . 
for 30 studies where data were given , 12 - month survival ranged from 36% to 83% , with an overall survival of 571% ( 1231 of 2155 patients ) compared vol 12 august 2011 articles panel : research in context systematic review in 2004 , we did a systematic review to assess the available evidence for e ectiveness of extra - pleural pneumonectomy ( epp ) .8 we identi ed seven publications of multimodal therapy but all were analysed on the basis of completed treatment , o ered no control data , and whether the most optimistic estimate of e ect size was su cient to outweigh the burden of treatment was debatable . 
during presentations of the available data to meetings at the british thoracic society and society for cardiothoracic surgery in great britain and ireland and in an editorial in the british medical journal9 we con rmed the uncertainty regarding the e ectiveness of epp was su cient to propose a randomised controlled trial . interpretation in the mesothelioma and radical surgery ( mars ) feasibility study , patients randomly assigned to no epp had better median and 1 - year survival than those assigned to epp . 
when compared with survival data from epp in a systematic review , 14 the mars surgical outcomes are in the middle of the reported range of median and 1 - year survival rates . 
in mars , survival was reported from randomisation to epp , which was after completion of three cycles of chemotherapy rather than from first chemotherapy as is customarily done for reports of epp within trimodal therapy . 
an allowance for this difference in starting time puts the survival of the patients in the no epp group in the upper part of the range of reported trimodal therapy outcomes . 
 the evidence from mars , in the context of external evidence from observational studies , suggests that the net effect of epp is to shorten survival without a gain in quality of life . 
a subset of four of these studies1518 plus an eortc phase 2 trial19 are most comparable with mars in that patients were all operated on since 2000 , had similar stage criteria for epp , and were planned for trimodal therapy in the same sequence , starting with chemotherapy with subsequent epp and then radiotherapy ( table 3 )  . 
in studies in which chemotherapy was the rst modality , the survival time was counted from the start of chemotherapy1518 or from registration.19 in mars , survival was calculated from the later timepoint of randomisation to epp or no [ iqr 2843 ] months between epp ( median 36 registration and randomisation )  . 
thus , to make any comparison , 36 months would have to be added to the 144 months median survival in the epp group of mars and the resulting estimated 18 months survival from the start of treatment becomes similar to these reported series ( table 3 )  . we cannot know from these non - controlled studies what survival might have been for similar patients to those having epp but who were managed without surgery . 
overall survival for the no epp group in mars was better than that used in the power calculations for the proposed phase 3 trial , for which 670 patients would be needed on the basis of the power calculation.9 in any subsequent planned phase 3 study of extirpative surgery , this non - surgical outcome would have to be taken into consideration in the power calculations of the number of patients needed overall to show superiority in the surgical arm . morbidity is di cult to compare between arms with two very di erent approaches to management but for epp morbidity has been consistently reported as high1921 and mars was no exception . 
in mars , no signi cant di erences were reported in the quality - of - life analyses between groups ; however , there seemed to be poorer quality of life , particularly just after surgery in patients randomly assigned to epp . 
the same consideration applies to any protocol that includes radical radiotherapy . in mars , most patients randomly assigned to epp had surgery in two centres with considerable experience in the surgery and perioperative care of these patients . 
in the systematic review of results of epp in 34 studies , 14 including 2320 patients , 30 - day mortality ranged from 0% to 118% and was 60% overall . 
for the 993 patents in 14 studies that were reported since 2008 when mars closed , and which therefore represent a similar era to when patients were recruited to mars , mortality was 56% ( range 0111% ) .14 one should note , however , that for a hypothetical study of 20 consecutive operations , an anticipated 5% mortality would shift to 10% or 0% with one additional or one fewer death . 
in doing so , a rigorous method of surgical quality assurance would be important . at the time mars was being planned , pemetrexed was not yet the standard of care in the uk . 
during recruitment , the chemotherapy standard of care for mesothelioma changed , and patients recruited later were more likely to receive cisplatin and pemetrexed than those recruited earlier in the study . 
there was no imbalance in the use of pemetrexed between the epp and no epp arms . the challenges of compliance with the trial protocol in this study should be taken into account when planning future phase 3 studies in which there is a large di erence in treatments between the two arms . 
some patients did not undergo surgery because , when reassessed after chemotherapy and when the risk : bene t balance of epp had been explained by the operating surgeon , they opted not to proceed . 
 nonetheless , although only 50 patients were randomised over the entire study period , rather than in the anticipated year , the fact that recruitment of these patients was possible suggests that the expected reluctance of patients to accept no radical surgery in a study with two very di erent to management of mesothelioma was not as marked as had been expected . treatment approaches to our knowledge , mars is the rst study to successfully randomly assign patients to epp and no radical surgery for mesothelioma . 
the mars trial was rigorously done , with the nal decision that a patient was eligible for randomisation within mars made in discussions by the mars virtual multidisciplinary team and the allocation to epp or no epp made within the icr - ctsu . 
although the study is small and the conclusions must be guarded , we believe the ndings are of relevance to guide practice . the median survival after epp within mars is consistent with 10 , 12 , 13 , and 14 months in larger observational studies , 2225 as was the proportion of complications . 
however , a much larger study with longer follow - up would be needed to provide reliable evidence on mortality patterns and long - term survival for any extirpative surgery for mesothelioma whether epp or lung - sparing surgery . 
a trial assessing the potential bene ts of total pleurectomy might be more practical in the future management of mesothelioma given the lower risk of perioperative mortality and morbidity in an ageing population with increasing comorbidities . 
recent data that compared and decortication with epp support the contention that this approach is unlikely to result in poorer survival than that associated with epp in mesothelioma.22 total pleurectomy lung - sparing contributors tt and jp were the mars chief investigators who , with dw and kob , instigated the trial . 
the trial management group was responsible for oversight of the day - to - day running of the trial under the guidance of the independent trial steering committee . con icts of interest ms has been a member of an advisory board for eli lilly . 
all other authors declare no con icts of interest . acknowledgments mars was supported by cancer research uk ( grant number cruk / 04 / 003 ) with additional support from the june hancock mesothelioma research fund . 
we acknowledge nancial support from the department of health via the nihr comprehensive biomedical research centre award to guys and st thomas nhs foundation trust in partnership with kings college london . 
travel and accommodation expenses for travel to the surgical centre for each trial participant and one relative ( or carer ) were met by the june hancock mesothelioma research fund . 
we thank all the patients who participated in this study ; and the surgeons , doctors , nurses , radiographers , physicists , pathologists , and data managers at the participating centres . 
we also thank all the trials unit sta at icr - ctsu , sutton , who contributed to the coordination of the trial and the trial management group , and independent data monitoring and trial steering committees for their oversight of the trial . vol 12 august 2011 articles editorial published online november 16 , 2012 s1470 - 2045 ( 12 ) 70526 - 0 for more on the patient protection and a ordable care act see world report lancet 2012 ; 380 : 172728 obama : health - care reform , part two the re - election of us president barack obama has surely eliminated the last serious threat to health - care reform in the usa . 
the patient protection and a ordable care act has already survived systematic opposition from republicans , a supreme court challenge , and nally , mitt romneys vow to repeal it if elected . 
the us healthcare system still faces many challenges and it may take more than insurance reform to address the the act can be seen as a health insurance reform packageover the next 2 years , medical insurance will almost certainly be extended to as many as 30 million americans who presently lack coverage . 
for most patients with cancerwho for decades have been discriminated against , denied coverage , and charged more that they could possibly a ord for life - saving treatmentsthe act has been an important step . 
it prohibits some of the health insurance industrys most notorious practiceseg , denying coverage to people who have pre - existing conditions or who participate in clinical trials , increasing premiums because of age or poor health , and insurance caps that restrict the amount that a patient can clai it also o ers free screening and preventive health care . although several measures have already been implemented , such as a requirement that insurance plans allow parents to cover their children aged up to 26 years in their policies , most aspects of the law are yet to be introduced . 
the biggest obstacles facing successful implementation of the act are the reliance on individual states to expand medicaid ( which guarantees health bene ts for the poorest americans ) , the budget cuts that the republicans will likely demand during upcoming negotiations , and the successful roll out by 2014 of insurance marketsso - called exchangesat the heart of the law , which enable people to buy individual coverage . 
that almost 50 million people have no health coverage in one of the richest countries in the world is a scandal that needs to be addressed , but the system is awed . 
the usa spends 16% of gdp on health versus 8% of gdp in europe , yet outcomes such as overall and cancer - speci c mortality are comparable between the two continents . 
the system will bankrupt itself unless major changes to funding and organisation are introducedtweaking medicares funding structure will not be su cient ; the entire health - care system needs an overhaul . 
the prevailing approach to paying for health care , based mainly on invidual services and products , encourages wasteful and ine ective care , creates incentives to overtest and overtreat while ignoring outcomes . 
he undoubtedly faces many di culties : the countrys trillion dollar de cit , the scal cli , and especially , the lack of a legislative majoritygiven that the democrats only control the senatewhich could lead to legislation bouncing from one chamber of congress to the other and nothing being done . 
but clinicians and societies also need to become more involved and lead such changes , otherwise others ( eg , politicians or insurers ) will make decisions that might later be judged inappropriate or unfair . 
 as obama cannot target another term in o ce , an opportunity exists to keep health high on the agenda and to o er americans the best medicine at the best cost . 
in the rst term of his presidency , obama set out important and necessary health insurance refor in his second term , he now needs to lead reform to make the health system fair , e cient , and sustainableif he can achieve this , he will leave an enduring legacy to be proud of . 
additionally , nw has received travel and accommodation support from novartis switzerland , and lad has received honoraria from novartis for blood - concentration testing of imatinib . us food and drug administration . 
enforcementactions / warningletters / ucm210191.htm ( accessed oct 10 , 2010 )  . larson ra , druker bj , guilhot f , et al , for the iris ( international randomized interferon vs sti571 ) study group . 
population pharmacokinetics of imatinib and the role of 1 - acid glycoprotebr j clin pharmacol 2006 ; 62 : 97112 . petain a , kattygnarath d , azard j , et al , for the innovative therapies with children with cancer european consortiupopulation pharmacokinetics and pharmacogenetics of imatinib in children and adults . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zhao f - h , lin mj , chen f , et al . 
performance of high - risk human papillomavirus dna testing as a primary screen for cervical cancer : a pooled analysis of individual patient data from 17 population - based studies from china . 
 lancet oncol 2010 ; 11 : 116071on page 1165 of this article , the right hand panel of gure 1a should state pooled speci city = 864% ( 838890 ) and the right hand panel of gure 1b should state pooled speci city = 851% ( 823879 )  . 
in table 1 of this review , data from hertel et al ( 2006 ) for number of conceptions , rst trimester loss , and deliveries , and from shepherd et al ( 2006 and 2008 ) and dargent et al ( 2007 and 2008 ) for number of deliveries were incorrect . 
 vol 12 january 2011 articles parotid - sparing intensity modulated versus conventional radiotherapy in head and neck cancer ( parsport ) : a phase 3 multicentre randomised controlled trial christopher m nutting , james p morden , kevin j harrington , teresa guerrero urbano , shreerang a bhide , catharine clark , elizabeth a miles , aisha b miah , kate newbold , maryanne tanay , fawzi adab , sarah j je eries , christopher scrase , beng k yap , roger p ahern , mark a sydenham , marie emson , emma hall , on behalf of the parsport trial management group * summary background xerostomia is the most common late side - e ect of radiotherapy to the head and neck . 
we assessed the hypothesis that parotid - sparing imrt reduces the incidence of severe xerostomia . methods we undertook a randomised controlled trial between jan 21 , 2003 , and dec 7 , 2007 , that compared conventional radiotherapy ( control ) with parotid - sparing imrt . 
we randomly assigned patients with histologically con rmed pharyngeal squamous - cell carcinoma ( t14 , n03 , m0 ) at six uk radiotherapy centres between the two radiotherapy techniques ( 1 : 1 ratio )  . 
 this study is registered with the international standard randomised controlled trial register , number isrctn48243537 . findings 47 patients were assigned to each treatment armedian follow - up was 440 months ( iqr 300597 )  . 
at 12 months xerostomia side - e ects were reported in 73 of 82 alive patients ; grade 2 or worse xerostomia at 12 months was signi cantly lower in the imrt group than in the conventional radiotherapy group ( 25 [ 74% ; 95% ci 5687 ] of 34 patients given conventional radiotherapy vs 15 [ 38% ; 2355 ] of 39 given imrt , p = 00027 )  . 
the only recorded acute adverse event of grade 2 or worse that di ered signi cantly between the treatment groups was fatigue , which was more prevalent in the imrt group ( 18 [ 41% ; 99% ci 2361 ] of 44 patients given conventional radiotherapy vs 35 [ 74% ; 5589 ] of 47 given imrt , p = 00015 )  . 
at 24 months , grade 2 or worse xerostomia was signi cantly less common with imrt than with conventional radiotherapy ( 20 [ 83% ; 95% ci 6395 ] of 24 patients given conventional radiotherapy vs nine [ 29% ; 1448 ] of 31 given imrt ; p < 00001 )  . 
at 12 and 24 months , signi cant bene ts were seen in recovery of saliva secretion with imrt compared with conventional radiotherapy , as were clinically signi cant improvements in dry - mouth - speci c and global quality of life scores . 
at 24 months , no signi cant di erences were seen between randomised groups in non - xerostomia late toxicities , locoregional control , or overall survival . interpretation sparing the parotid glands with imrt signi cantly reduces the incidence of xerostomia and leads to recovery of saliva secretion and improvements in associated quality of life , and thus strongly supports a role for imrt in squamous - cell carcinoma of the head and neck . funding cancer research uk ( cruk / 03 / 005 )  . introduction radiotherapy is the main non - surgical treatment for squamous - cell carcinoma of the head and neck ( hnscc ) .1 high rates of local tumour control can be achieved with 5 - year survival greater than 80% for stage 1 and 2 and 6070% for stage 3 and 4 tumours ; 2 however , long - term late sequelae of radiotherapy are highly prevalent and have severe adverse e ects on quality of life ( qol ) .3 , 4 radiation - induced xerostomia is the most commonly reported late side - e ect of radiotherapy to the head and neck . 
lack of saliva a ects speech and swallowing and can accelerate dental caries.5 ( imrt ) radiotherapy intensity - modulated conformal radiotherapy technique that can spare the major salivary glands . 
patients were required to attend regular follow - up , undergo salivary ow measurements , and complete self - assessed qol questionnaires . they were exclusion criteria included previous head or neck radiotherapy ; previous malignancy except non - melanoma skin cancer ; pre - existing salivary gland disease ; tumour involvement of the parotid glands ; or previous or concurrent illness that would compromise completion of treatment or follow - up . 
patients who had received neoadjuvant chemotherapy were eligible . 94 patients recruited 47 randomly assigned to conventional 47 randomly assigned to imrt radiotherapy 6 died before 12 months 6 died before 12 months 41 alive at 12 months 41 alive at 12 months 7 not assessed at 12 months 3 withdrew consent 2 did not attend 1 reason unknown 1 deviated and withdrew ( treated with chemoradiation ) 2 not assessed at 12 months 1 did not attend 1 not done because of disease recurrence at 8 months 34 evaluable for primary endpoint 39 evaluable for primary endpoint at 12 months 33 received treatment as per protocol 1 deviation ( imrt given , unable to cover target volume adequately ) at 12 months 37 received treatment as per protocol 2 deviations ( radiotherapy gap because of rectal bleeding , concomitant chemotherapy ) 29 alive and disease free 12 months after completion of radiotherapy 5 alive with recurrence or progressive disease 29 alive and disease free 24 months after completion of radiotherapy 5 died figure 1 : study pro le imrt = intensity - modulated radiotherapy . 37 alive and disease free 12 months after completion of radiotherapy 2 alive with recurrence 29 alive and disease free 24 months after completion of radiotherapy 7 alive with recurrence or progressive 3 died disease all patients provided written informed consent . 
 the parsport ( cruk / 03 / 005 ) was approved by national south - west multicentre research ethics committee ( mrec 03 / 6 / 79 ) and local ethics committees of all participating centres . 
our trial was sponsored by the royal marsden nhs foundation trust and undertaken in accordance with the principles of good clinical practice . the randomisation and masking patients were randomly assigned in a 1 : 1 ratio to parotidsparing imrt or conventional radiotherapy ( control )  . 
treatment allocation was not masked ; however , the patient was not informed of the treatment until they had completed the baseline qol questionnaires . procedures staging investigations included examination under anaesthetic , tumour biopsy , diagnostic ct or mri of head and neck , chest radiograph , full blood count , and biochemistry . 
in postoperative patients , histology reports that documented the extent of surgical resection were required . the protocol for target volume de nition and treatment planning has been previously described.9 all patients underwent ct - planned radiotherapy with either threedimensional conformal radiotherapy with parallel opposed lateral elds ( conventional radiotherapy ) or parotid - sparing imrt . 
nodal groups at risk of harbouring occult metastatic disease received a biologically equivalent dose of either 50 gy in 25 daily fractions ( conventional radiotherapy ) or 54 gy in 30 fractions ( imrt )  . 
for imrt patients a planning constraint of less than 24 gy to the whole contralateral parotid gland was used.9 , 10 for quality assurance , plans were assessed from all centres for protocol compliance and dosimetric consistency.10 , 11 acute side - e ects were graded weekly with national cancer institute common toxicity criteria ( version 3 ) 12 during radiotherapy and until 8 weeks after treatment . 
salivary ow 128 vol 12 february 2011 articles december , 2007 , both committees approved closure of recruitment after 94 patients had been randomly assigned to the study groups with the expectation that this would provide su cient evaluable patients to allow robust statistical analysis . 
our trial was not powered to reliably assess small di erences in locoregional pfs or overall survival , although these are reported for completeness . our analysis was done on an intention - to - treat basis , with all patients who had a 12 - month xerostomia assessment included . 
mann - whitney test p < 00001 . table 1 : baseline characteristics and treatment details measurements were done before radiotherapy , at week 4 of radiotherapy , and at 2 weeks , 3 , 6 , 12 , 18 , and 24 months after radiotherapy . 
unstimulated and sodium - citratestimulated parotid saliva from each parotid duct ori ce and oor of mouth saliva were collected by standard methods.7 , 8 after treatment , clinical follow - up was monthly in year 1 , every 8 weeks in year 2 , then every 36 months until the end of year 5 . 
assessments were not blinded to treatment allocation . patient - reported qol was collected with questionnaire booklets that contained the european organization for research and treatment of cancer ( eortc ) qlqc30 quality - of - life instrument16 ( which measures generic cancer - related qol ) , the associated head and neck speci c module hn35 , 17 xerostomia questionnaire.8 patients completed the baseline booklet in the clinic before randomisation . 
follow - up booklets were sent directly to the patients homes at 2 weeks , 3 , 6 , 12 , 18 , and 24 months after radiotherapy . the modi ed and our primary objective was to assess late side - e ects . 
this endpoint was chosen because it assesses an abnormal symptom ( ie , partial but persistent or complete dryness or worse ) measured by a reliable and sensitive method for scoring late side - e ects in hnscc.18 we decided on 12 months a priori as a clinically appropriate time at which to make a valid assessment of late e ects . xerostomia secondary endpoints were the proportion of patients with any measurable salivary ow after radiotherapy , acute and other late radiation side - e ects , qol that included xerostomia - related qol as measured by the modi ed locoregional progression - free survival ( pfs ) , and overall survival . 
in march , 2007 , the independent data monitoring committee and the trial steering committee approved an increase in the target sample size to 84 evaluable patients ( ie , alive 1 year after the end of radiotherapy ) that was anticipated to be achievable with 100 randomly assigned patients . 
in vol 12 february 2011 conventional radiotherapy imrt p = 0061 p = 00096 p = 00027 p = 00029 p < 00001 number at risk conventional radiotherapy imrt p = 0028 p = 000068 p = 0025 p < 00001 p < 00001 articles not presented these sensitivity analyses because they gave similar results to the main analysis . 
we present unadjusted odds ratios ( ors ) and ors adjusted for tumour site ( oropharynx or hypopharynx ) , stage of disease ( 1 and 2 or 3 and 4 ) , and radiotherapy indication ( radical or postoperative )  . 
all other analyses are unadjusted . we compared the proportions of patients with any measurable saliva ow and proportions ever reporting grade 2 or worse acute and late side - e ects between treatment groups with fishers exact tests . 
to make some adjustment for multiple testing we used a signi cance level of 1% for all secondary side - e ects , sialometry , and qol endpoints and accordingly we provide 99% cis . 
acute and late side - e ects in our report were those where sidee ects of grade 2 or worse were experienced by at least 20% of patients in either group or those where proportions were signi cantly di erent between treatment groups . we calculated qol scores with standard algorithms with a higher score suggesting poorer qol on all scales except eortc global health status , where a higher score suggests better qol.24 we deemed di erences in eortc qol scores of 10 points or more clinically signi cant in line with eortc guidelines.25 the primary qol analysis included all completed questionnaires . 
we compared in eortc qol and xerostomia mean changes questionnaire item scores from baseline between groups by two - sample t tests . we used generalised estimating equations ( gee ) , adjusting for the correlations in multiple measurements from the same patient ( with an exchangeable correlation matrix ) to account for the longitudinal nature of the xerostomia and qol data . 
a pragmatic approach to modelling was taken , with treatment - by - time interaction terms included if they were identi ed in advance as clinically relevant or they were statistically signi cant . 
qol gee models also included terms for baseline score for the item of interest . for survival - related endpoints , alive and disease - free patients were censored at date of last follow - up . 
rtog = radiation therapy oncology group . censored 1 month before any disease recurrence , in case recurrence could adversely a ect salivary ow , and by excluding patients whose side - e ect assessment was not within 2 months either side of its expected date . 
we have 130 vol 12 february 2011 articles our analyses were based on a database snapshot frozen on may 14 , 2010 , and were done in stata version 10 . 
 this study is registered as an international standard randomised controlled trial , number isrctn48243537 . role of the funding source the funding source provided peer - reviewed approval for the trial but had no other role in study design , collection , analysis , interpretation of data , or writing of the report . 
one patient assigned to the conventional radiotherapy group was deemed ineligible because they were due to be treated with chemoradiation ( no follow - up data are available for this patient )  . 
 * * worst of subjective ( pain , dysphagia , taste alteration ) , objective ( mucosal integrity , weight ) , and management ( pain , ulcer , dysphagia , taste alteration ) grades . 
worst of subjective ( dysphagia , pain ) , objective ( weight loss , stricture , ulceration , bleeding , anaemia ) , and management ( dysphagia / stricture , weight loss , pain / ulceration , bleeding ) grades . 
worst of subjective ( roughness , sensation ) , objective ( oedema , alopecia , pigmentation change , ulcer / necrosis , telangiectasia , brosis / scar , atrophy / contraction ) , and management ( dryness , sensation , ulcer , oedema , brosis / scar ) grades . 
worst of subjective ( pain , voice hoarseness , breathing ) , objective ( oedema , mucosal integrity , respiration ) , and management ( pain , hoarseness , respiration ) grades . 
worst of subjective ( pain , mastication , denture use , trismus ) , objective ( exposed bone , trismus ) , and management ( pain , bone , trismus / mastication ) grades . 
||||worst of subjective ( pain , tinnitus , hearing ) , objective ( skin , hearing ) , and management ( pain , skin , hearing loss ) grades . table 2 : maximum acute and late side - e ect grades by treatment group vol 12 february 2011 conventional radiotherapy imrt no measurable salivary ow * ( n = 25 ) measurable salivary ow ( n = 0 ) no measurable salivary ow ( n = 18 ) measurable salivary ow ( n = 16 ) subjective xerostomia better than grade 2 6 ( 24% ) subjective xerostomia grade 2 or worse 19 ( 76% ) 10 ( 56% ) 8 ( 44% ) 12 ( 75% ) 4 ( 25% ) fishers exact test for association ( treatment groups combined ) p = 0018 . 
eortc hn35 = european organization for research and treatment of cancer head and neck speci c module hn35 . contralateral parotid was signi cantly less in the imrt group ( p < 00001 ; table 1 )  . 
45 of 47 patients randomly allocated to receive conventional radiotherapy and 45 of 47 randomly assigned to receive imrt completed radiotherapy as per protocol ; 33 of the 34 patients evaluable for the primary outcome in the conventional radiotherapy group and 37 of 39 patients evaluable for the primary endpoint in the imrt group completed radiotherapy as per protocol ( gure 1 )  . 
at 12 months , there were signi cantly fewer cases of xerostomia in the imrt group ( 25 [ 74% , 95% ci 56 to 87 ] of 34 in the conventional radiotherapy group vs 15 [ 38% , 23 to 55 ] of 39 in the imrt group ) , and the absolute reduction was 35% ( 95% ci 14 to 56 ; p = 00027 )  . 
 at 24 months , 20 ( 83% , 63 to 95 ) of 24 patients in the conventional radiotherapy group reported xerostomia versus nine ( 29% , 14 to 48 ) of 31 in the imrt group , and the absolute reduction was 54% ( 32 to 76 ; p < 00001 )  . 
the proportion of patients that reported grade 2 or worse xerostomia at 12 months did not di er by tumour site , radiotherapy indication ( primary vs postoperative ) , stage of disease , or use of neoadjuvant chemotherapy ( data not shown )  . 
a similar pattern was seen over time and between treatment groups when xerostomia was scored with the rtog scale ( gure 2 )  . 132 vol 12 february 2011 articles conventional radiotherapy imrt the only recorded acute adverse event of grade 2 or worse to di er between treatment groups ( at the 1% signi cance level ) was fatigue ( table 2 ) : 18 ( 41% ; 99% ci 23 to 61 ) of 44 patients in the conventional radiotherapy group versus 35 ( 74% ; 55 to 89 ) of 47 in the imrt group ( p = 00015 )  . 
of note , at 12 months , grade 3 or worse dysphagia was reported by two ( 5% ) of 40 patients in the conventional radiotherapy group and four ( 9% ) of 46 in the imrt group . we recorded baseline sialometry in 80 patients , all of whom had measurable salivary ow . 
at 12 months unstimulated saliva ow from the contralateral parotid gland was noted in 16 ( 47% ) of 34 patients in the imrt group compared with none of 25 in the conventional radiotherapy group ( p < 00001 )  . 
corresponding data at 24 months were seven ( 44% ) of 16 in the imrt group versus none of 15 in the conventional radiotherapy group ( p = 00068 )  . 
strong concordance was noted between measurable contralateral saliva ow and grade 2 or worse xerostomia ( table 3 )  . mean changes in global health status from baseline to 12 months were 11 ( 99% ci 99 to 121 ) for conventional radiotherapy versus 30 ( 119 to 179 ; p = 078 ) for imrt . 
 changes at 24 months were 28 ( 171 to 116 ) for conventional radiotherapy versus 83 ( 66 to 232 ) for imrt , corresponding to a between group di erence in change scores of 111 ( 90 to 312 ; p = 014 )  . 
no in change from statistically signi cant di erences baseline between groups were noted for any qlqc30 subscale scores ( data not shown )  . in both study groups , hn35 subscale scores for dry mouth , senses , and sticky saliva were signi cantly worse than baseline at 12 months . 
mean increases from baseline at 12 months in the dry mouth subscale were 565 ( 99% ci 365 to 765 ; p < 00001 ) for conventional radiotherapy and 480 ( 318 to 642 ; p < 00001 ) for imrt . 
mean increases at 24 months were 593 ( 378 to 807 ; p < 00001 ) for conventional radiotherapy and 348 ( 138 to 559 ; p < 00001 ) for imrt . 
at both time points , smaller score changes were noted in the imrt group than in the conventional radiotherapy group , although these were not signi cant at the 1% level . in the gee model for dry mouth the main treatment coe cient was 66 ( 99% ci 215 to 83 ; p = 025 ) with a treatment - by - time interaction term of 003 ( 006 to 000 ; p = 0017 ) , suggesting the di erence in dry mouth between treatment groups increases over time . 
censoring at recurrence had a negligible e ect on qol results , although the interaction term from the gee analysis 0 / 47 0 / 47 number of events / at risk conventional radiotherapy imrt time from randomisation ( months ) 1 / 42 2 / 44 5 / 34 4 / 39 1 / 30 4 / 31 1 / 29 0 / 28 0 / 23 2 / 22 0 / 19 0 / 18 0 / 15 1 / 15 0 / 11 figure 4 : kaplan - meier plot of locoregional progression - free survival by treatment group hazard ratio 153 ( 95% ci 063 to 370 )  . 
2 - year locoregional progression - free survival estimates for conventional radiotherapy 80% ( 95% ci 65 to 90 ) and for imrt 78% ( 62 to 87 ) ; absolute di erence 3% ( 15 to 20 )  . 
 became less statistically signi cant ( coe cient 002 ; p = 0080 )  . the xerostomia questionnaire was only completed by 39 patients at baseline and 12 months and by 33 patients at baseline and 24 months ( compared with 73 reporting the primary endpoint at 12 months and 55 at 24 months )  . 
 in both treatment groups all eight xerostomia questionnaire items were signi cantly worse at 12 and 24 months than at baseline and although the changes were smaller in the imrt group , no statistically signi cant di erences between group changes were noted ( webappendix p 1 )  . overall , there were seven locoregional recurrences in the conventional radiotherapy group : ve in the highdose volume and two in both the high - dose volume and electively irradiated neck . 
2 - year locoregional pfs was 80% ( 95% ci 65 to 90 ) in the conventional radiotherapy group and 78% ( 62 to 87 ) in the imrt group ( absolute di erence 3% , 95% ci 15 to 20 ; hr 153 , 95% ci 063 to 370 ; log - rank p = 034 ; gure 4 )  . 32 deaths have been reported so far ( 18 in the conventional radiotherapy group vs 14 in the imrt group ; hr for overall survival 068 , 95% ci 034 to 137 )  . 
of these deaths , 20 were due to head and neck cancer ( ten in the conventional radiotherapy group vs ten in the imrt see online for webappendix vol 12 february 2011 articles group )  . 
other causes of death in the conventional radiotherapy group were second ( non - head - and - neck ) primary cancer ( four patients ) , cardiac ( two ) , gastrointestinal complications ( one ) , and suicide ( one ) ; and in the imrt group were infection ( two ) , second primary cancer ( one ) , and gastrointestinal complications ( one )  . 
a consistently higher qlqc30 global and hn35 dry mouth qol score was reported in patients who received imrt ; between group di erences at 24 months were clinically but not statistically signi cant . 
xerostomia questionnaire results showed changes in favour of imrt in all eight questions but these di erences were not large enough to reach statistical signi cance , probably because of the small number of patients that completed this questionnaire . 
we postulate that this could be because of di erences in patient perception of the xerostomia symptom or because of other factors such as submandibular gland or oral cavity dose or comorbidity . 
before the design of our randomised trial , a few small single centre experiences had been published and a review of the published work on imrt had been done.26 no randomised trials were identi ed . 
during the recruitment period of the parsport trial two smaller randomised trials were reported in nasopharyngeal cancer from centres in asia , and several other single institutional experiences were reported.27 , 28 interpretation our trial is the largest randomised trial of imrt in head and neck cancer , and the only trial addressing squamous - cell carcinoma , the predominant form seen worldwide . 
our trial shows that imrt reduces patient - reported xerostomia , allows recovery of salivary ow , and improves quality of life after treatment compared with conventional radiotherapy . detailed analyses of the distribution of dose to the salivary tissue including parotid glands and other minor salivary glands , and its correlation with clinical outcomes are ongoing . 
initial results suggest that there is no correlation between submandibular gland dose and xerostomia . a limitation of our trial was that it was not possible to mask the treatments from patients or clinicians because of di erences in treatment delivery . 
however , results that relate to multiple secondary endpoints support the primary analysis and the size of the observed e ect is unlikely to be due entirely to assessment or reporting bias . 
after our trial was designed , several small nonrandomised studies2935 and one case - control study36 of parotid - sparing imrt have been published with a range of endpoints including saliva ow rate , patient - reported symptoms , and qol . 
 qol was assessed with eortc qlqc30 , hn35 , and the sf36 health survey and although qol scores for some domains were better for imrt patients , no improvements in patient - reported dry mouth symptoms on the hn35 questionnaire were noted . 
kam and colleagues38 reported a reduction in observer - rated severe xerostomia ( rtog grade 2 or worse ) with imrt ( 39% vs 82% ; p = 0001 ) in 60 patients with early - stage nasopharyngeal cancer . 
the results of the parsport trial are thus likely to be generalisable to all head and neck tumours for which conventional radiotherapy is used . in our study , fewer cases of acute dermatitis were recorded in patients treated with imrt than in those treated with conventional radiotherapy , although di erences were not statistically signi cant at the 1% level , probably because of reduced dose to skthe proportions of patients that reported grade 2 or worse acute xerostomia and grade 2 or worse salivary gland changes also showed reductions , albeit not statistically signi cant ( table 2 )  . 
 in an unplanned dosimetry review in a subset of patients , mean radiation doses to the posterior fossa were 2030 gy in the patients treated with imrt compared with about 6 gy in patients treated with conventional 134 vol 12 february 2011 articles radiotherapy , which could account for the recorded di erence in acute radiation fatigue . 
apart from salivary gland changes and radiation - induced xerostomia , other late side - e ects of conventional radiotherapy were not altered by imrt . our trial was too small to detect small di erences in , or conclude non - inferiority of , locoregional pfs or overall survival . 
although patients continue to be followed up for long - term survival , to show non - inferiority in overall survival to no more than 5% at 2 years ( 80% power , onesided 5% signi cance ) would need a randomised controlled trial of more than 900 patients . 
 recurrences have not been noted in the spared parotid tissue in patients treated with imrt or surgery , 21 , 39 suggesting that a large study to show non - inferiority in this tumour type is probably both impractical and inappropriate . 
our trial has shown a clinically and statistically signi cant reduction in xerostomia , improved salivary ow , and improved qol , and thus strongly supports a role for imrt in hnscc . contributors cmn and eh were responsible for the trial design , trial management , data interpretation , and writing of the report . 
cc and eam were responsible for the design and conduct of the quality assurance programme and contributed to the trial management , data interpretation , and writing of the report . 
all authors reviewed and approved the nal version of the paper . con icts of interest the authors declared no con icts of interest . acknowledgments parsport was supported by cancer research uk ( grant numbers c8996 / a8684 , trial reference number cruk / 03 / 005 )  . 
the parsport trial team acknowledges the support of the national institute for health research , through the national cancer research network . comment information about non - speci c side - e ects from providers and written material , such as those on consent forms and labels , without consideration of the nocebo e ect . for this model to work on behalf of patients , the risks and bene ts of a speci c treatment have to be completely unrelated to the act of information disclosure to the patient.8 although this notion might be true for some treatments , it is not uniformly applicable . 
with surgery , the outcome of treatment is more likely to be related to patient anatomy and surgical technique and less likely to be a ected by information exchange during the consent process . 
for example , a patient who develops insulin de ciency after undergoing surgery for pancreatic cancer can be counselled quite objectively that this risk is likely to manifest on the basis of the size of the tumour and location within the pancreas and is unlikely to be a ected by the act of disclosure of this risk to the patient before surgery . 
 for patients with cancer who undergo non - invasive treatments or are prescribed drugs associated with non - speci c side - e ects , the act of disclosure itself could a ect the possibility of side - e ect manifestation . 
 rather , in many clinical circumstances in which the potential for non - speci c side - e ects is high , such as in the non - invasive treatment of cancer , the act of information disclosure could be more accurately viewed as part of the riskbene t analysis , thus dependent on real - time discussion , and personalised to the patient . 
theor med bioeth 2011 ; 32 : 22943 . published online november 16 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70332 - 1 errata adams c , torode j , henshall s , cazap e , ryel al , grey n . 
lancet oncol 2011 ; 12 : 109192in this comment , the fourth sentence of the third paragraph should have read : who has committed to produce targets for its so - called best - buy interventions in time for the world health assembly in 2012 . 
in this news article , the rst sentence of the fourth paragraph should have read the researchers found that a daily serving of unprocessed red meat increased the risk of cancer mortality by 10% , whereas a daily serving of processed meat was responsible for a 16% increased risk . 
this correction has been made as of march 26 , 2012 . published online march 26 , 2012 doi : 10.1016 / s14702045 ( 12 ) 70130 - 4 see news page e147 e135 vol 13 april 2012 editorial this online publication has been corrected . 
the corrected version rst appeared at thelancet.com / oncology on june 29 , 2012 for more on the lancet oncologys call for gps to receive better education see leading edge lancet oncol 2009 ; 10 : 97 for more on variation in gp referral patterns for patients with cancer see articles lancet oncol 2012 ; 13 : 35365 for more on the partnership between cancer research uk and the royal college of general practitioners see news lancet oncol 2012 : 12 : e232 for more on qcancer risk calculators see for more on the challenges of supporting patients with multiple morbidities see articles lancet 2012 ; published online may 10 . 
a third of all young cancer patients reported their gps took no action despite presentation with common cancer symptoms and a quarter of patients had to visit the gp four or more times before their symptoms were taken seriously . 
if a young person presents with the same symptoms three times , gps should automatically refer them for further investigation . although the tct survey was small ( collating the opinions of only 300 patients ) , the ndings mirror those of lyratzopoulos and colleagues published in the lancet oncology in april , 2012 , that analysed more than 41 000 patients with 24 types of cancer . 
in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
 so what can be done to restore trust ? usefully , cancer research uk and the royal college of general practitioners have launched an initiative to support gps by putting together models of best practice , and by reviewing care pathways and thresholds for further investigation to ensure gps have better access to diagnostics and secondary care . 
 additionally , the department of health has announced a pilot project within gp practices of cancer - risk prediction tools ( qcancer risk calculators ) developed by researchers at the university of nottingha these successful these partnerships are good examples of engagement between policy makers and physicians with organisations that have a perceptive understanding of the patient viewpoint and of research realities and possibilities . 
 initiatives will be whether transforming the e ectiveness of the gp and improving patient care will take time to assess , but it is unlikely that they will prove to be a broad panacea . 
it is becoming increasingly clear , for example , that the uk health - care system is not designed to cope with multiple comorbiditiesa common situation among patients with cancerand in the future gps will need to take a central and proactive role in coordinating patient care throughout their entire journey within the national health service . 
this will require rethinking of the current infrastructure , and might require adjustments to gps case burdens to ensure su cient time is available for more thorough consultations , especially in socioeconomically deprived areas . while the role of the gp in cancer diagnosis is undeniably important , it is essential not to forget interdependency on improved patient education , screening , secondary care and access to latest treatments , supportive and palliative care , and coordinated long - term follow - up . 
 improved understanding of the factors contributing to the di erences between the uks cancer outcomes and those of other countries will provide important clues and solutions . 800 000 people visit a gp every day in the uk , but questions are increasingly being asked about the competency of those doctors that undermine patient trust . 
however , implementation of this bill could be a fresh start in a process of restoring trust and ensuring gps have access to the best tools necessary to provide a rst - class service and to guarantee all patients receive the best possible care . 
additionally , nw has received travel and accommodation support from novartis switzerland , and lad has received honoraria from novartis for blood - concentration testing of imatinib . us food and drug administration . 
enforcementactions / warningletters / ucm210191.htm ( accessed oct 10 , 2010 )  . larson ra , druker bj , guilhot f , et al , for the iris ( international randomized interferon vs sti571 ) study group . 
population pharmacokinetics of imatinib and the role of 1 - acid glycoprotebr j clin pharmacol 2006 ; 62 : 97112 . petain a , kattygnarath d , azard j , et al , for the innovative therapies with children with cancer european consortiupopulation pharmacokinetics and pharmacogenetics of imatinib in children and adults . 
 if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata zhao f - h , lin mj , chen f , et al . 
performance of high - risk human papillomavirus dna testing as a primary screen for cervical cancer : a pooled analysis of individual patient data from 17 population - based studies from china . 
 lancet oncol 2010 ; 11 : 116071on page 1165 of this article , the right hand panel of gure 1a should state pooled speci city = 864% ( 838890 ) and the right hand panel of gure 1b should state pooled speci city = 851% ( 823879 )  . 
in table 1 of this review , data from hertel et al ( 2006 ) for number of conceptions , rst trimester loss , and deliveries , and from shepherd et al ( 2006 and 2008 ) and dargent et al ( 2007 and 2008 ) for number of deliveries were incorrect . 
 vol 12 january 2011 comment are more likely to opt for burdensome treatment with a small chance of improvement than are healthy people.6 , 7 following a deliberative model of patientphysician interaction , 8 the physician should explain his or her own assessment of bene ts and harms , including the underlying health - related values ( see question two ) , thereby empowering the patient to reconsider his or her own values , preferences , and the resulting decision . 
 if the patients choice to proceed with the intervention results from deeply held values coupled with a thorough understanding of the facts , the patient and the physician should proceed with the intervention . 
 although physicians should always minimise the required resources to achieve a speci c treatment goal , whether a high consumption of resources constitutes a legitimate reason to withhold an intervention that provides only a questionable or small net bene t to the patient is controversial.9 , 10 under the assumption that the setting of limits is unavoidable in any health - care system , we have included a fth question that asks doctors to take the resource implications of their decisions into account in an ethically justi ed way . 
the question becomes relevant in all health - care systems in which physicians have to ration care through budgets , waiting lists , or the application of rationing rules to individual cases . 
if the patient has a realistic understanding of the situation and there is persistent disagreement about the value of the intervention ( after answering question four ) , the physician should explicitly inform the patient that the requested intervention provides only a small or questionable net bene t at high costs . 
alternatively , if the patient does not have a realistic understanding of his or her medical situation and the bene tharm ratio of the intervention is at least questionable in the physicians judgment , question ve could guide the decision . 
however , if the treatment draws heavily on resources , considerations of equality might justify a unilateral decision to withhold the requested intervention , because the high resource consumption is not counterbalanced by a clear net bene t or sound autonomy - based arguments . 
beyond futility : to what extent is the concept of futility useful in clinical decision - making about cpr ? lancet oncol 2002 ; 3 : 63842 . consensus statement of the society of critical care medicines ethics committee regarding futile and other possibly inadvisable treatments . 
 motesanib , or open - label bevacizumab , in combination with paclitaxel , as rst - line treatment for her2 - negative locally recurrent or metastatic breast cancer : a phase 2 , randomised , double - blind , placebo - controlled study . 
lancet oncol 2011 ; 12 : 66372in the summary , the nal sentence of the findings section should have stated 12 208 ( 73% ) of the women positive by hpv testing had no cytological abnormality , and these women had 258 ( 35% ) of 747 cin3 or adenocarcinoma in situ , 25 ( 29% ) of 87 cancers , and 17 ( 63% ) of 27 adenocarcinomas . 
this correction has been made to the online version as of july 29 , 2011 . 722 vol 12 august 2011 editorial for niraula and colleagues meta - analysis see j clin oncol 2012 ; published online july 16 . 
these data raise the question whether the pursuit of improved survival outcomes comes with a trade - o in tolerability that is reaching an unsustainable level . leboulleux and colleagues study in the september issue of the lancet oncology serves to further illustrate this point . 
despite an improvement in progressionfree survival of more than 5 months , patients with di erentiated thyroid cancer given vandetanib were at substantially greater risk of side - e ects such as severe diarrhoea and were more than ve times more likely to discontinue treatment because of toxicity than were those in the control group . 
and in another article in the current issue , by ismael and colleagues , a novel subcutaneous formulation of trastuzumab increase treatment - related toxicity and mortality compared with the standard intravenous administrationwhich in turn suggests that the potential for increased patient convenience with the new formulation is not necessarily a clear - cut bene t . 
 is shown to one would have hoped that the advent of targeted therapythe premise of which revolves around an ability to more precisely direct treatments to disease would have lessened the amount of adverse e ects a patient might experience . 
in an analysis of the selectivity of various kinase inhibitors , in which a range of targeted agents were screened across a panel of more than 300 kinases , sorafenibas just one examplewas found to bind to 10% of o - target kinases with a similar a nity to its primary targets of vegfr and braf . 
the barrier for agents to proceed to later stage trials should be raised , and in some instances , when clinical bene t is marginaleg , bevacizumab for breast cancerone wonders whether the current accelerated approval processes might in fact have become too accelerated . 
given the marked increase in complications when targeted agents are combined with chemotherapeutic agents , greater emphasis should be placed on undertaking phase 1 trials of combinations of drugs , and only when there is a clear mechanistic rationale for the drugs co - administration . 
 more comparative phase 2 trials should be done , and should also incorporate extensive biomarker analyses not just for e cacy , but also for a better understanding of the molecular mechanisms of toxicity . 
in so doing , phase 3 trials can be better designed not only to enrol solely those patients most likely to bene t , but also those least likely to be harmed . 
greater attention must also be paid to collecting quality - of - life data , in particular patient - reported outcomes , to determine whether the quality of any lengthening of survival is not outweighed by toxicity . 
 finally , post - marketing phase 4 studies should be more widely done , and databases set up to rigorously and prospectively collect data for adverse events as they are reported in the community , so that a new drugs activity and toxicity can be better examined in a less selected patient population . 
indeed , an analysis of updated drug labels for anticancer drugs that had been approved by the fda showed that more than 40% of targeted agents gained one or more boxed warnings for serious adverse drug reactions within about 4 years of initial approval , with half of the additional adverse reactions potentially being fatal , highlighting the value of continued surveillance . 
radiat res 2006 ; 166 : 36774 . davis s , day rw , kopecky kj , et al , for the international consortium for research on the health e ects of radiation writing committee and study teachildhood leukaemia in belarus , russia , and ukraine following the chernobyl power station accident : results from an international collaborative population - based case - control study . 
 ( accessed april 13 , 2011 )  . published online april 1 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70082 - 1 erratum van hooft je , bemelman wa , oldenburg b , et al , for the collaborative dutch stent - in study group . 
 lancet oncol 2011 ; 12 : 34452in this article ( april ) , the fth sentence of the second paragraph of the introduction should have read in a systematic review of 54 uncontrolled trials and case reports , self - expandable metal stents were technically successful in 919% of patients and clinically successful in 717% of patients when used as a bridge to surgery.14 the second sentence of the fourth paragraph of the discussion should have read our technical success of 70% was rather low compared with the published data ( 919% ) .14 the fth sentence of the eighth paragraph of the discussion should have read in the four patients in whom the lesion seemed to be benign at endoscopy , the procedure was ceased and endoscopists did not attempt to place the stent . 
these corrections have been made to the online version as of april 1 , 2011 . 418 vol 12 may 2011 comment if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology as piration of mediastinal and hilar lymph nodes should be used to assess preoperative lung cancer status in countries where tuberculosis is endemic.10 finally , hiv infection is associated with increased lung cancer cases . 
can tuberculosis further increase this risk ? in a study11 that linked aids registry surveillance data for 322 675 patients with aids diagnosed between 1977 and 2002 , with cancer registries in 11 us regions , lung cancer risk over 10 years was unrelated to tuberculosis . 
 tuberculosis awareness in patients with cancer needs to be reinforced , especially in low - burden developed countries , and lung cancer awareness in patients with previous or suspected tuberculosis should be urgently strengthened in developing countries to increase the low numbers of potentially resectable tumours . * sandro vento , massimiliano lanzafame department of internal medicine , faculty of medicine and health sciences , university of botswana , gaborone , botswana ( sv ) ; and infectious diseases unit , gb rossi university hospital , verona , italy ( ml ) ventosandro@yahoo.it we declare that we have no con icts of interest . yu yh , liao cc , hsu wh , et al . 
lancet oncol 2011 ; 12 : 37786in this article ( april ) , on page 380 , the number of women with luminal a breast cancer tested for the kras variant should have been 478 in gure 2a and the percentage of premenopausal women diagnosed with luminal a breast cancer should have been 151% in gure 2b . 
lancet oncol 2011 ; 12 : 41516on page 415 , in the second column , it was stated that 17 variants showed moderate to strong evidence of a true association and were therefore candidates for clinical tests , this should have said 14 variants . 
this correction has been made to the online version as of may 18 , 2011 . published online may 18 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70127 - 9 522 vol 12 june 2011 articles conjugated equine oestrogen and breast cancer incidence and mortality in postmenopausal women with hysterectomy : extended follow - up of the womens health initiative randomised placebo - controlled trial garnet l anderson , rowan t chlebowski , aaron k aragaki , lewis h kuller , joann e manson , margery gass , elizabeth bluhm , stephanie connelly , f allan hubbell , dorothy lane , lisa martin , judith ockene , thomas rohan , robert schenken , jean wactawski - wende summary background by contrast with many observational studies , women in the womens health initiative ( whi ) trial who were randomly allocated to receive oestrogen alone had a lower incidence of invasive breast cancer than did those who received placebo . 
we aimed to assess the in uence of oestrogen use on longer term breast cancer incidence and mortality in extended follow - up of this cohort . methods between 1993 and 1998 , the whi enrolled 10 739 postmenopausal women from 40 us clinical centres into a randomised , double - masked , placebo - controlled trial . 
women aged 5079 years who had undergone hysterectomy and had expected 3 - year survival and mammography clearance were randomly allocated by a computerised , permuted block algorithm , strati ed by age group and centre , to receive oral conjugated equine oestrogen ( 0625 mg per day ; n = 5310 ) or matched placebo ( n = 5429 )  . 
using data from this extended follow - up ( to aug 14 , 2009 ) , we assessed long - term e ects of oestrogen use on invasive breast cancer incidence , tumour characteristics , and mortality . 
in subgroup analyses , we noted breast cancer risk reduction with oestrogen use was concentrated in women without benign breast disease ( p = 001 ) or a family history of breast cancer ( p = 002 )  . 
in the oestrogen group , fewer women died from breast cancer ( six deaths , 0009% per year ) compared with controls ( 16 deaths , 0024% per year ; hr 037 , 95% ci 013091 ; p = 003 )  . 
fewer women in the oestrogen group died from any cause after a breast cancer diagnosis ( 30 deaths , 0046% per year ) than did controls ( 50 deaths , 0076% ; hr 062 , 95% ci 039097 ; p = 004 )  . interpretation our ndings provide reassurance for women with hysterectomy seeking relief of climacteric symptoms in terms of the e ects of oestrogen use for about 5 years on breast cancer incidence and mortality . 
however , our data do not support use of oestrogen for breast cancer risk reduction because any noted bene t probably does not apply to populations at increased risk of such cancer . funding us national heart , lung , and blood institute ; wyeth . introduction elevated concentrations of endogenous oestrogen have been consistently associated with increased risk of breast cancer.1 exogenous oestrogen use has also been associated with higher breast cancer incidence in many25 but not all6 , 7 observational studies , especially in leaner women35 , 8 and those receiving oestrogen long term.4 , 5 , 8 , 9 oestrogen use has been linked to hormone - receptor positive and early stage disease , 3 , 5 suggesting a better prognosis , 10 although associations with breast cancer mortality are mixed.2 , 9 , 1017 during the intervention phase of the womens health initiative ( whi ) randomised trial17 of 10 739 post menopausal women who had undergone hysterectomy , a nonsigni cant reduction in incidence of breast cancer was noted after receipt of conjugated equine oestrogens compared with placebo ( hazard ratio [ hr ] 079 , 95% ci 061102 )  . 
after trial intervention was stopped in february , 2004 , because of an increased incidence of stroke , 18 follow - up continued until planned termination in 2005 and every year thereafter for participants who consented to extended surveillance . 
the reduced breast cancer risk in the oestrogen group persisted and reached statistical signi cance ( hr 077 , 95% ci 062095 ) .19 we aim to provide additional details about the e ects of oestrogen use on invasive breast cancer incidence during and after intervention with regard to tumour characteristics and previously identi ed e ect modi ers . 
we also present results for breast cancer - related mortality . methods study design and participants postmeno pausal women aged 5079 years who had under gone a hysterectomy were recruited into the whi randomised , double - masked , placebo - controlled trial at 40 clinical centres in the usa between 1993 and 1998 . 
eligible women were randomly allocated in a one - to - one ratio to receive oral conjugated equine oestrogen ( 0625 mg per day ) or matched placebo through use of a computerised , permuted - block algorithm , strati ed by age group and centre . 
details of study design , eligibility , and implementation have been published elsewhere.18 , 19 data collection participants previous hormone use was ascertained at baseline by an interviewer - administered questionnaire . 
adherence to study drug was assessed primarily by pill counts or weighing returned bottles ; self - report was used only rarely . until 2005 , participants vital and health status was assessed twice every year and mammography was done once per year throughout the trial . 
when the intervention ended on feb 29 , 2004 , after a mean follow - up of 71 ( sd 16 ) years , all participants were unmasked and asked to stop taking the study drug . 
during study close - out , end 7645 participants ( 78% of 9786 living participants in active follow - up at that time ; 3778 [ 779% ] of 4851 women allocated to oestrogen and 3867 [ 784% ] of 4935 allocated to placebo ) consented to extended follow - up.19 from 2005 , vital and health status updates have been obtained once per year . 
this report presents data until aug 14 , 2009 , after an overall median follow - up of 118 years ( iqr 91129 )  . breast cancers were documented by medical and pathological record review by centrally trained doctor adjudicators . 
tumour characteristics were coded at the whi clinical coordinating center according to surveillance , epidemiology , and end results ( seer ) guidelines.20 deaths were documented with death certi cates and medical records . 
all adjudicators were masked to randomisation assignment . intervention phase the post - intervention phase statistical analysis we compared incidence of breast cancer by treatment group with failure - time methods and the intention - totreat principle . 
we did analyses for three time phases : ( from randomisation until the feb 29 , 2004 ) ; ( from march 1 , 2004 , until the data cuto on aug 14 , 2009 ) ; and overall results . 
event times during the intervention phase were censored at date of death , last follow - up , or termination of the intervention phase ( feb 29 , 2004 ) , whichever occurred rst . 
participants were included in post - intervention phase incidence analyses if they were alive , in follow - up , and had not developed breast cancer by march 1 , 2004 . 
we compared slopes for each phase with wald tests . we examined the in uence of non - adherence to protocol - assigned censoring events treatment by 6 months after participants rst became non - adherent ( ie , took < 80% of study drugs or started non - study hormone therapy )  . 
some categories do not add up to total number of women who consented to extended follow - up due to missing data . table 1 : baseline characteristics of participants in the womens health initiative trial of conjugated equine oestrogen who consented to extended follow - up in secondary analyses , we tested interactions between randomisation assignment and 16 baseline charac teristics within the primary cox model , expanded to include the designated baseline factor , randomisation assignment , and interaction term ( s )  . 
we omitted partici pants with missing estimated probability of continued adherence , in the proportional - hazards models to adjust for changes in the distribution of sample characteristics during follow - up.21 478 vol 13 may 2012 articles vol 13 may 2012 values from the corresponding analysis . 
no adjustment for multiple testing was made ; at most , one interaction was expected to be signi cant by chance alone . all analyses were done with sas version 9.1.3 and gures were drawn with r 2.11. 
decisions about study design , data collection and analysis , result interpretation , manuscript preparation , and the decision to submit the manuscript for publication resided with committees comprised of whi investigators that included nhlbi representatives . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results baseline breast cancer risk factors in women who consented to extended follow - up were much the same as those of the original cohort18 and much the same between randomised groups , apart from a small imbalance in bilateral oophorectomy and benign breast disease ( table 1 )  . 
during the intervention phase , 8090% of par ticipants had mammograms every year with equivalent frequencies treatment groups.17 , 22 3894 ( 812% ) of 4794 of women in the oestrogen group and 3965 ( 813% ) of 4877 controls had at least one mammogram after the trial intervention was stopped . two the oestrogen placebo hr 077 ( 95% ci 062095 ) p = 002 hr 068 ( 95% ci 049095 ) p = 002 articles 0045 0030 0015 number at risk oestrogen placebo 5310 5429 time since randomisation ( years ) time since randomisation ( years ) 5166 5280 5007 5106 4840 4915 4261 4301 3620 3678 1696 1771 5310 5429 3513 3752 2752 2883 1862 1937 1506 1571 1270 1355 figure 1 : kaplan - meier estimates of cumulative hazards of invasive breast cancer in the whi randomised trial of conjugated equine oestrogen with the intention - to - treat principle ( a ) and with adjustments for adherence ( b ) background shading shows the distribution of the duration of intervention ( in quintiles )  . 
by that time , 57% of 5310 women in the oestrogen group and 91% of 5429 controls had started hormones provided by their health - care providers.18 of 7472 participants in extended follow - up with available data , 604 ( 81% ) reported use of hormones after intervention , with slightly more in the oestrogen group than the placebo group ( 334 [ 90% ] of 3699 in the oestrogen group vs 270 [ 72% ] of 3773 controls ; p = 0003 )  . in the intention - to - treat analyses , data were available for a median follow - up of 72 years ( iqr 6481 ) from randomisation until early termination of the trial intervention , a median follow - up of 47 years ( 3551 ) after intervention , and a median of 118 years ( 91129 ) follow - up overall . 
in these analyses , use of oestrogen was associated with lower overall invasive breast cancer incidence ( 151 events , 027% per year ) compared with placebo ( 199 events , 035% per year ; hr 077 , 95% ci 062095 ; p = 002 ; 19 table 2 , gure 1 ) , with no di erence between intervention and post - intervention hazard ratios ( pinteraction = 076 )  . 
we noted non - signi cant increasing trends in oestrogen hrs by time since randomisation ( pslope = 019 ) and by time since trial cessation ( pslope = 032 )  . median duration of study drug use was 59 years ( iqr 2573 ) and median time to non - adherence ( ie , taking < 80% of study pills or starting other hormone therapy ) was 35 years ( 1565 )  . 
sensitivity analyses adjusting for non - adherence yielded a stronger association between oestrogen use and lower breast cancer risk overall ( hr 068 , 95% ci 049095 ; gure 1 ) , which seemed even higher when restricted to the intervention period ( 058 , 039084 )  . in analyses of tumour characteristics ( table 2 ) , oestrogen use was associated with a reduced risk of in ltrating ductal carcinoma ( hr 067 , 95% ci 051088 ) compared with placebo but not in ltrating lobular cancers ; however , the test for heterogeneity was not signi cant ( p = 033 )  . 
 482 vol 13 may 2012 025 050 100 200 favours oestrogen favours placebo articles ratios for hormone receptor - positive tumours and hormone receptor - negative tumours were much the same . 
we noted a reduced risk for her2 - negative tumours ( 074 , 056097 ) but not her2 - positive tumours ( 150 , 079283 ) in women who received oestrogen compared with placebo ( pheterogeneity = 0045 ) , although missing her2 data were common . 
compared with placebo , we noted fewer small and node - negative tumours but no reduction in the number of large tumours ( 2 cm ) or node - positive tumours in the oestrogen group , but comparisons between subtypes did not reach signi cance . in analyses starting at randomisation ( table 2 and gure 2 ) , fewer women diagnosed with breast cancer died in the oestrogen group ( 30 deaths , 0046% per year ) compared with the placebo group ( 50 deaths , 0076% per year ; hr 062 , 95% ci 039097 ; p = 004 )  . 
of these deaths , six were directly attributed to breast cancer in the oestrogen group ( 0009% per year ) compared with 16 in the placebo group ( 0024% per year ; 037 , 013091 ; p = 003 )  . subgroup analyses provided a mostly consistent pattern of lower breast cancer incidence with oestrogen use ( gure 3 )  . 
of 16 interactions tested , two were nominally statistically signi cant : history of benign breast disease ( p = 001 ) and rst degree family history of breast cancer ( p = 002 )  . 
no interactions were reported with age ( p = 098 ) , body - mass index ( p = 049 ) , gail model risk score ( p = 022 ) , oophorectomy status ( p = 055 ) , years since menopause onset ( p = 068 ) , previous oestrogen use ( p = 095 ) , or vasomotor symptoms ( p = 074 )  . of women who rst used hormone therapy 5 years or more after menopause ( ie , gap time 5 years ) , the estimated e ect of oestrogen ( hr 065 , 95% ci 048089 ) seemed lower than that for women who started hormone therapy sooner after menopause ( 089 , 066120 ) but the interaction was not signi cant ( p = 013 )  . after discontinuation discussion use of oestrogen for a median of 59 years in postmenopausal women with hysterectomy in the whi randomised trial was associated with a signi cant reduction in incidence of invasive breast cancer , a reduction that continued for the median 47 years of follow - up intervention . 
potential e ect modi cation with benign breast disease ( p = 001 ) and family history of breast cancer ( p = 002 ) suggests that these reductions might not apply to women at increased risk . 
we noted a signi cant reduction in breast cancer - related mortality and all - cause mortality after breast cancer diagnosis with oestrogen use , but the number of such deaths was small . although many observational studies have reported an increased risk of breast cancer with oestrogen use , 25 some have reported lower risks.6 , 23 in previous studies reporting an adverse e ect of such therapy on breast cancer , most25 , 8 but not all , 5 , 9 showed an increased risk of breast cancer only after prolonged ( > 5 years ) oestrogen use . 
in this trial , with substantial variation in exposure length ( median duration of the intervention 59 years [ range < 110 years ] ; median adherent time 35 years ; and 2291 [ 21% ] of 10 739 partici pants reporting previous oestrogen use for > 5 years at baseline ) , we noted no time - trends in terms of duration of use or time since cessation and no interactions with previous oestrogen use , although the power for interaction tests was low ( panel )  . 
the continued , postintervention e ect of oestrogen on breast cancer incidence is akin to that reported for other hormone - targeted drugs shown to reduce breast cancer incidence.33 , 34 panel : research in context systematic review conjugated equine oestrogen was approved for management of climacteric symptoms in several countries in the early 1940s . 
by the 1990s , about 40% of postmenopausal women in the usa and uk were receiving hormone therapy ( oestrogen alone or oestrogen plus progesterone ) .2426 however , the risks and bene ts of this commonly used therapy had never been established in a clinical trial setting . 
against this background , scientists at the us national institutes of health , working in conjunction with experts in a number of disciplines , developed the womens health initiative ( whi ) hormone therapy programme to meet this unmet need with potential implications for a large number of postmenopausal women in the usa and around the world.27 the whi hormone therapy programme consisted of two full - scale randomised , placebo - controlled clinical trials to separately assess the e ect of oestrogen alone and oestrogen plus progesterone on chronic disease in postmenopausal women with and without previous hysterectomy , respectively , at 40 clinical sites in the usa . 
when the whi trials were developed , observational study evidence suggested that oestrogen , alone or with progesterone , would modestly increase breast cancer risks25 but the cancers would have a favourable prognosis.35 the results from the whi randomised , placebo - controlled trial of oestrogen alone contradicts most previous observational studies in that oestrogen use was associated with reduced breast cancer incidence and reduced breast cancer - associated mortality . 
 previous e orts to reconcile these results have pointed to the issue of timing of rst hormone therapy.28 , 29 additionally , some of the di erences between previous observational studies and the present randomised clinical trial results might re ect variation in mammography frequency in observational study populations . 
the whi oestrogen - alone ndings also di er from those seen in the whi randomised trial assessing oestrogen plus progesterone in women without previous hysterectomy in which combined hormone therapy signi cantly increased breast cancer incidence and breast cancer mortality.3032 interpretation our ndings provide reassuring evidence about breast safety of oestrogen use for climacteric symptom management in postmenopausal women with hysterectomy for durations consistent with those reported in this trial . 
although a reduced risk of breast cancer incidence and mortality was noted in recipients of oestrogen , these ndings do not support its use for breast cancer risk reduction in light of the lack of bene t for populations at higher risk , the adverse e ects on stroke and venous thromboembolism , 18 and the increased risk reduction available with other drugs . vol 13 may 2012 oestrogen and progesterone placebo ( in combined arm ) hr 125 ( 95% ci 107146 ) oestrogen alone placebo ( in oestrogen - alone arm ) hr 077 ( 95% ci 062095 ) articles 005 004 003 002 001 time since randomisation ( years ) number at risk combined arm oestrogen and progesterone placebo oestrogen - alone arm oestrogen alone placebo 8506 8102 5310 5429 8329 7914 5166 5280 8109 7721 5007 5106 7796 7466 4840 4915 7009 6692 4261 4301 6189 5889 3620 3678 2914 2648 1696 1771 figure 4 : cumulative hazards , adjusted for age and ethnic group , of invasive breast cancer by random allocation in the whi trials of conjugated equine oestrogen alone and conjugated equine oestrogen plus medroxyprogesterone acetate trials derived from chlebowski and colleagues32 hr = hazard ratio . many observational studies report increased breast cancer risk with oestrogen alone in normal weight but not overweight or obese women.4 , 5 , 8 we noted no e ect modi cation with body - mass index ; oestrogen hazard ratios were less than one in normal weight , overweight , and obese women . use of mammography is a potential source of confounding in observational studies.35 in clinical practice , women who take hormone therapy have mammograms more regularly than untreated women36 and screened populations have an increased rate of breast cancer detection , 37 , 38 potentially explaining the increased breast cancer risk in oestrogen users noted in previous studies that did not assess screening . 
controlling for ongoing screening in observational studies is unusual and not straightforward because it depends on adequate data collection and modelling , and the assumption that mammography use is not an intermediate variable of exposure and disease.39 , 40 detection bias is an unlikely explanation for our results . 
 mammography rates were protocol - de ned and very similar between randomisation groups.17 , 22 further more , little e ect on breast density41 oestrogen use has or detection of breast cancer.22 finally , the signi cant reduction in breast cancer mortality reported with oestrogen use provides strong evidence against the possibility that the risk reduction noted was an artifact of oestrogen e ects on screening , 40 because a delay in detection would be expected to increase mortality . favourable e ects of use of oestrogen alone on breast cancer survival , measured from cancer diagnosis , have been seen in some1012 but not all2 , 7 , 1316 reports . 
studies of mostly oestrogen alone use on breast cancer mortality , measured from start of hormone therapy have provided mixed results with favourable , 1012 neutral , 1315 and unfavourable2 , 7 associations reported . 
our results , measured from randomisation ( although still imprecise ) provide important new evidence that oestrogen use for about 5 years reduces breast cancer mortality , supporting a favourable association with breast cancer incidence . a reduction in breast cancer incidence with conjugated equine oestrogen is biologically plausible . 
although such oestrogen is a recognised mitogen that usually stimulates mammary cell proliferation and inhibits apoptosis through activation of the oestrogen receptor , 1 both preclinical4246 and clinical45 ndings suggest that after long - term oestrogen deprivation , adaptive changes in mammary tumour gene expression pro les render tumours paradoxically susceptible to oestrogen - induced apoptosis.43 , 44 although the mechanisms are complex and not wholly understood , 46 preclinical studies suggest involvement of the fas / fas l extrinsic ( receptor - mediated ) death regulatory pathway47 and the intrinsic ( mitochondrial ) apoptotic pathway , mediated through increased expression of several proapoptotic proteins including p53 - unregulated modulator of apoptosis.48 , 49 e orts to reconcile the original ndings of this trial17 with observational study results suggested that the time from menopause to rst hormone use ( gap time ) is a potential modulator of hormone therapys in uence on breast cancer risk.28 in the parallel whi randomised clinical trial29 and the observational million women study , 5 women starting oestrogen plus progesterone use with a short gap time were at increased breast cancer risk . 
for use of oestrogen alone , the million women study investigators reported no increased incidence in breast cancer with oestrogen use starting 5 years or more from menopause but an increased risk with a shorter gap time.5 in these analyses , oestrogen hazard ratios were lower than 1 for early initiation ( gap time < 5 years ) and late initiation ( 5 years )  . 
we noted a somewhat greater in women starting in uence oestrogen therapy 5 years or more after meno pause , but the interaction with gap time was not statistically signi cant . 484 vol 13 may 2012 articles although breast cancer incidence and related mortality were lower for women who took oestrogen alone than for controls , our ndings do not support oestrogen use for breast cancer risk reduction because subgroup analyses suggest the bene t might not apply to populations at increased breast cancer risk . 
additionally , other hormonetargeted drugs have a substantially greater in uence on breast cancer than does oestrogen.33 , 34 , 50 , 51 however , our ndings , together with a relatively balanced riskbene t pro le for clinical events , 18 , 52 provide reassurance about breast cancer safety for postmenopausal women with previous hysterectomy who receive unopposed oestrogen to reduce climacteric symptoms for durations equivalent to those reported in this trial . tamoxifen , raloxifene , and exemestane all provide greater breast cancer risk reduction than oestrogen , but have important limitations . 
the selective oestrogen receptor modulators tamoxifen and raloxifene reduce risk of breast cancer and fractures but increase climacteric symptoms and have adverse e ects on stroke , blood clots , and endometrial cancer , leading to an unfavourable riskbene t pro le in most postmenopausal women.33 , 53 exemestane , an aromatase lowers oestro gen concentrations , also substantially reduces breast cancer risk.34 however , aromatase inhibitors cause bone loss and increase climacteric symptoms and arthralgias , 54 exerting a greater in uence when started soon after menopause.55 the mechanisms through which exogenous oestrogens , tamoxifen , raloxifene , and aromatase inhibitors all reduce breast cancer risk are not known but clearly warrant further study . inhibitor that and study strengths include the randomised , doublemasked , placebo - controlled prospective design with breast cancer as the designated primary safety outcome , a large sample size , high - quality outcomes ascertainment , protocol - required mammography throughout most of the follow - up period . 
however , any bias arising from poor adherence would probably dilute the di erences between random isation groups over the duration of follow - up , as the adherence - adjusted analyses con rmed . 
small numbers of breast cancer deaths , some attrition associated with re - consenting for extended follow - up , and a median of only 47 years of post - intervention follow - up should also be noted . 
the trial assessed only one dose and schedule of oral conjugated equine oestrogens ; whether these ndings apply to lower doses , other oestrogen preparations , or longer durations of use is not known . major di erences exist in whi trial ndings between oestrogen only therapy in women with previous hysterectomy and those of the parallel whi randomised trial of oestrogen plus medroxyprogesterone acetate in women with an intact uterus . 
whereas oestrogen - alone treatment was associated with reduced breast cancer incidence and reduced breast cancer mortality , combined hormone therapy increased breast cancer incidence , 29 , 52 delayed breast cancer diagnosis , 56 and increased breast cancer mortality.48 the biological basis for this di erence is unknown . 
the comparability of breast cancer incidence rates for the placebo groups in the two trials ( gure 4 ) suggests that di erences in hormone therapy , rather than hysterectomy , is the primary determinant . 
 changes in the serum proteome in response to oestrogen and combined hormone therapies are generally quite similar but di erences have been identi ed that could in uence breast cancer risk , including those in notch2 and some igf binding proteins.57 contributors gla , rtc , and aka conceived the study design . 
gla and aka had full access to the data . con icts of interest rtc has been a consultant for astrazeneca , novartis , amgen , and p zer , received funding support from amgen , and served on speakers bureaus for astrazeneca and novartis . 
all other authors declare that they have no con icts of interest . acknowledgments the womens health initiative program is funded by the us national heart , lung , and blood institute , national institutes of health , and department of health and human services through contracts n01wh22110 , 24152 , 32100 - 2 , 32105 - 6 , 32108 - 9 , 32111 - 13 , 32115 , 32118 - 32119 , 32122 , 42107 - 26 , 42129 - 32 , and 44221 . editorial for more on the health - care bill see world report lancet 2010 ; 375 : 114950 supreme court asked to decide future of us health care the twists and turns of the journey of the new us health - care policy through the us legal system reached in september , its expected end destination when 2011 , the justice department asked the supreme court to review the governments health - care law . 
 the a ordable care act , signed into law on march 23 , 2010 , called for a number of changes that are focused around a central tenet mandating that most americans must be insured from 2014 , or face a tax penalty . 
however , an individual mandate is vehemently opposed by some , most notably the republican party , who argue it is unconstitutional , and the law has been repeatedly challenged ( but mainly upheld ) in the courts over the past 18 monthswith the requirement for individual insurance the main point of contention . 
and in a further twist , the 26 states that originally led the atlanta suit have also lodged an appeal in the supreme court claiming that without this individual mandate the health - care legislation will be unworkable . 
 the government is con dent that the mandate will not be struck from the law and argue that it does not exceed its powers of commerce but will save money by preventing cost - shiftingin which the costs of emergency treatment of uninsured individuals are covered by increases in the premiums of those with insurance . 
opponents say that enactment of the law will cost money , leading to raised taxes , and overburden health - care systems that will be unable to cope with the additional patients . 
certainly allowing more patients access to the system through insurance is only a rst step on the care pathway , with delivery of services an equally important , and perhaps the biggest , challenge for the reforms . 
 as a result of the subsequent community reaction and premium costs , questions remain about the obama administrations mandate on future insurance costs and on the capacity of the current health - care syste furthermore , businesses must also o er coverage under the reforms , with only those companies with fewer than 50 employees being exempt , and this has understandably sparked resistance within the business community . 
nevertheless , these uncertainties and squabbles aside , there are several notable and important aspects of the act , such as coverage for dependents up to 26 years of age and the removal of caps on insurance , that highlight why the legislation must not be overturned or gutted . 
previously insurers were able to deny this group coverage in a bid to increase their pro ts whereas the new law ensures temporary coverage for people with pre - existing conditions until the mandate is activated in 2014 . 
 however , does not all this legal wrangling and discussion of cost rather miss the point and fundamental philosophy behind the law ? who has not experienced a sudden , serious , and chronic illness in a family member or friend ? the law is trying to change a reactive health - care system to a proactive one , with improved access to care for all . 
surprisingly , no alternative proposals to replace obamas law have been suggested by detractors , with republicans simply calling for it to be repealed , despite many health experts calling the existing system broken . 
 so should universal health - care be a human right , and do those who oppose the law lack a moral compass , or is this a naive and rose - tinted view in the current nancial climate ? one thing is certaif the law is repealed , or the individual mandate is removedand if november , 2012 , sees a change of guard at the topa whole generation will rue a missed opportunity . 
although great progress has been made against many types of cancer ( as highlighted by recent mortality data from the american cancer society ) , treatment of others has shown little change in the past few decades . 
two phase 3 clinical trials published in december , 2011 , in the new england journal of medicine ( gog018 and icon7 ) showed that women with newly diagnosed advanced ovarian cancer given concomitant bevacizumab with a paclitaxel and carboplatin chemotherapy regimen following surgery , and then maintenance bevacizumab , had signi cantly longer progression - free survival compared with those who received chemotherapy alone . 
5 - year survival is just 30% , a figure that has not changed for the past 30 yearsthis contrasts with breast cancer , in which 5 - year survival has improved from 50% to 80% over the same period . 
for example , in this issue of the lancet oncology , gotlieb and colleagues show that aflibercept , a vegf - trap , can prolong time between repeat paracentesis to drain malignant ascites associated with the disease , compared with placebo . although these latest reports show promise for the treatment of ovarian cancer , a major hurdle towards reducing mortality continues to be the late presentation of the disease . 
less than a third of women are diagnosed with early - stage disease , for which survival at 5 years is 90%indicating that early diagnosis and treatment is central to reducing mortality . 
ovarian cancer has often been called a silent killer because of its subtle and nonspeci c symptoms ; however , it is perhaps not so much that the disease is silent , but rather that it is not being heard because of a lack of understanding of the biology of the disease . 
 in 2009 , the target ovarian cancer charity published the rst results of its path nder study , which surveyed women , family doctors , and specialists to identify gaps in the knowledge and treatment of those with ovarian cancer . 
a key nding was that many factors can lead to delays in diagnosis , from women not recognising symptoms and delaying an initial consultation with a doctor , through to misdiagnosis . 
since then , an online tool has been developed by researchers from the university of nottingham in the uk as a diagnostic aid that takes into account risk factors including age and family history , and the presence of persistent symptoms , such as abdominal swelling and loss of appetite . 
published in the british medical journal on jan 4 , 2012 , a study into the e ectiveness of the tool showed that the 10% of women with the highest predicted risks according to the algorithm had 63% of all ovarian cancers diagnosed over the next 2 years . 
this project enters its next phase later this year , with an increased number of specialist clinics being made available to women . after many years of disappointing results for women with ovarian cancer , on the eve of world cancer day on feb 4 , 2012 , there is at long last an opportunity to celebrate some improvements made in the diagnosis and treatment of this devastating cancer . 
world cancer day will undoubtedly be dominated by the more prominent cancer types , but it is imperative that continued e orts are made in rarer cancers and that these diseases are not ophaned by a disproportionate focus on easy wins . 
 the lancet oncology vol 13 february 2012 corrections correction to lancet oncol 2011 ; 12 : 531 , 532 bonnefoi h , piccart m , bogaerts j , et al , on behalf of the eortc 10994 / big 1 - 00 study investigators . 
tp53 status for prediction of sensitivity to taxane versus non - taxane neoadjuvant chemotherapy in breast cancer ( eortc 10994 / big 1 - 00 ) : a randomised phase 3 trial . 
 lancet oncol 2011 ; 12 : 52739in this article , table 2 was incorrect and should have been as shown below . accordingly , the third paragraph of the results section should have read by february , 2010 , 675 primary had occurred , endpoint of which 420 ( 62% ) were distant recurrences ( table 2 )  . 
this correction has been made to the online version as of jan 28 , 2013 . events fec ( n = 361 ) * t - et ( n = 314 ) * progression while on neoadjuvant chemotherapy 56 ( 16% ) distant recurrence invasive locoregional recurrence invasive contralateral cancer death without previous report of progression 219 ( 61% ) 59 ( 16% ) 14 ( 4% ) 13 ( 4% ) progression treatment toxicity cancer ( non - breast ) cardiovascular other not known 49 ( 16% ) 201 ( 64% ) 42 ( 13% ) 13 ( 4% ) 9 ( 3% ) data are number ( % ) or number . 
deaths occurring during chemotherapy or within 30 days of chemotherapy completion and without disease relapse . table 2 : first events contributing to progression - free survival correction to lancet oncol 2013 ; 14 : 88 , 89 , 95 goss pe , smith ie , oshaughnessy j , et al , on behalf of the teach investigators . 
 lancet oncol 2013 ; 14 : 8896the second sentence of the methods in the summary should read women outpatients 33 countries with her2 - positive earlybreast cancer who had previously received chemotherapy but not trastuzumab were randomly from 405 centres adjuvant assigned ( 1 : 1 ) to receive daily lapatinib ( 1500 mg ) or daily placebo for 12 months , and the second sentence of the study design and participants section , should read participants were hospital outpatients at 405 centres in 33 countries worldwide . 
 the online version was corrected on jan 28 , 2013 . vol 14 february 2013 editorial for niraula and colleagues meta - analysis see j clin oncol 2012 ; published online july 16 . 
these data raise the question whether the pursuit of improved survival outcomes comes with a trade - o in tolerability that is reaching an unsustainable level . leboulleux and colleagues study in the september issue of the lancet oncology serves to further illustrate this point . 
despite an improvement in progressionfree survival of more than 5 months , patients with di erentiated thyroid cancer given vandetanib were at substantially greater risk of side - e ects such as severe diarrhoea and were more than ve times more likely to discontinue treatment because of toxicity than were those in the control group . 
and in another article in the current issue , by ismael and colleagues , a novel subcutaneous formulation of trastuzumab increase treatment - related toxicity and mortality compared with the standard intravenous administrationwhich in turn suggests that the potential for increased patient convenience with the new formulation is not necessarily a clear - cut bene t . 
 is shown to one would have hoped that the advent of targeted therapythe premise of which revolves around an ability to more precisely direct treatments to disease would have lessened the amount of adverse e ects a patient might experience . 
in an analysis of the selectivity of various kinase inhibitors , in which a range of targeted agents were screened across a panel of more than 300 kinases , sorafenibas just one examplewas found to bind to 10% of o - target kinases with a similar a nity to its primary targets of vegfr and braf . 
the barrier for agents to proceed to later stage trials should be raised , and in some instances , when clinical bene t is marginaleg , bevacizumab for breast cancerone wonders whether the current accelerated approval processes might in fact have become too accelerated . 
given the marked increase in complications when targeted agents are combined with chemotherapeutic agents , greater emphasis should be placed on undertaking phase 1 trials of combinations of drugs , and only when there is a clear mechanistic rationale for the drugs co - administration . 
 more comparative phase 2 trials should be done , and should also incorporate extensive biomarker analyses not just for e cacy , but also for a better understanding of the molecular mechanisms of toxicity . 
in so doing , phase 3 trials can be better designed not only to enrol solely those patients most likely to bene t , but also those least likely to be harmed . 
greater attention must also be paid to collecting quality - of - life data , in particular patient - reported outcomes , to determine whether the quality of any lengthening of survival is not outweighed by toxicity . 
 finally , post - marketing phase 4 studies should be more widely done , and databases set up to rigorously and prospectively collect data for adverse events as they are reported in the community , so that a new drugs activity and toxicity can be better examined in a less selected patient population . 
indeed , an analysis of updated drug labels for anticancer drugs that had been approved by the fda showed that more than 40% of targeted agents gained one or more boxed warnings for serious adverse drug reactions within about 4 years of initial approval , with half of the additional adverse reactions potentially being fatal , highlighting the value of continued surveillance . 
 the lancet oncology vol 13 september 2012 corrections correction to lancet oncol 2012 ; 13 : 983 , 986 correction to lancet oncol 2012 ; 13 : 1028 correction to lancet oncol 2012 ; 13 : e468 fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 this correction has been made as of oct 29 , 2012 . randomised , chemorefractory jfw , van den smits mlj , nijsen holmium - 166 bosch maaj , et al . 
lancet oncol 2012 ; 13 : 102534in table 1 of this article , the total number of patients with ocular melanoma should have been six , as should the total number of patients with colorectal carcinoma . 
lancet oncol 2012 ; 13 : e468in this news item , the second and third sentences of the second paragraph should have read : median pfs was 94 months ( 95% ci 86167 ) in the combination group compared with 58 months ( 4674 ) in the dabrafenib monotherapy group ( hazard ratio 039 , 95% ci 025062 ; p < 0001 )  . 
our aim was to investigate these associations in a large uk prospective cohort with su cient information on incident cancer to allow direct comparison of height - associated risk across cancer sites and in relation to major potential confounding and modifying factors . methods information on height and other factors relevant for cancer was obtained in 19962001 for middle - aged women without previous cancer who were followed up for cancer incidence . 
we used cox regression models to calculate adjusted relative risks ( rrs ) per 10 cm increase in measured height for total incident cancer and for 17 speci c cancer sites , taking attained age as the underlying time variable . 
 findings 1 297 124 women included in our analysis were followed up for a total of 117 million person - years ( median 94 years per woman , iqr 84102 ) , during which time 97 376 incident cancers occurred . 
risk increased for 15 of the 17 cancer sites we assessed , and was statistically signi cant for ten sites : colon ( rr per 10 cm increase in height 125 , 95% ci 119130 ) , rectum ( 114 , 107122 ) , malignant melanoma ( 132 , 124140 ) , breast ( 117 , 115119 ) , endometrium ( 119 , 113124 ) , ovary ( 117 , 111123 ) , kidney ( 129 , 119141 ) , cns ( 120 , 112129 ) , nonhodgkin lymphoma ( 121 , 114129 ) , and leukaemia ( 126 , 115138 )  . 
the increase in total cancer rr per 10 cm increase in height did not vary signi cantly by socioeconomic status or by ten other personal characteristics we assessed , but was signi cantly lower in current than in never smokers ( p < 00001 )  . 
in current smokers , smokingrelated cancers were not as strongly related to height as were other cancers ( rr per 10 cm increase in height 105 , 95% ci 101109 , and 117 , 113122 , respectively ; p = 00004 )  . 
in a meta - analysis of our study and ten other prospective studies , height - associated rrs for total cancer showed little variation across europe , north america , australasia , and asia . interpretation cancer incidence increases with increasing adult height for most cancer sites . 
the relation between height and total cancer rr is similar in di erent populations . funding cancer research uk and the uk medical research council . introduction tall people are at increased risk of cancer . 
increasing cancer risk with increasing adult height has been reported for all cancers combined and for several common cancers , such as those of the breast , ovary , prostate , and large bowel.17 evidence is limited , however , for incident , rather than fatal , disease and for less common cancer sites . 
 moreover , it is not clear to what extent height - associated risks vary by cancer site , or how other factors , such as smoking and socioeconomic status , a ect these associations.8 , 9 because the range of height in a given population is usually narrow , large numbers of events are needed for reliable estimation of risk . 
we also did a meta - analysis of published results from prospective studies on the relation between height and total cancer incidence or mortality . methods participants between 1996 and 2001 , 13 million middle - aged women invited to attend the uks national health service ( nhs ) breast screening programme completed a million women study recruitment questionnaire , which asked , among other things , about social , demographic , and lifestyle factors , including current height and weight . 
of women who answered a study questionnaire in 200607 , a sample selected at random ( on the basis of day of birth ) were asked in 200609 to have their height measured by their family doctor : 3762 women did so . 
in this validation sample , the correlation between measured and reported heights was excellent ( pearson correlation coe cient 088 )  . vol 12 august 2011 articles all participants gave written consent to take part in our study , and approval was obtained from the oxford and anglia multi - centre research ethics committee . 
all study participants have a unique nhs number and are automatically followed up for death , emigration , and cancer registration through the nhs central registers with that number and other identifying details . 
the registers regularly provide study investigators with information on the date of any such event in participants , and code the underlying cause of death and cancer site with the international classi cation of diseases , 10th revision ( icd - 10 ) .10 follow - up is complete for over 99% of study participants . 
 procedures our main endpoints were incident invasive cancer at 17 individual sites with at least 1000 incident cases : mouth and pharynx ( icd - 10 c00 - c14 ) , oesophagus ( c15 ) , stomach ( c16 ) , colon ( c18 ) , rectum ( c19 - 20 ) , pancreas ( c25 ) , lung ( c34 ) , malignant melanoma ( c43 ) , breast ( c50 ) , endometrium ( c54 ) , ovary ( c56 ) , kidney ( c64 ) , bladder ( c67 ) , central nervous system ( c7072 , d32 , 33 , 42 , and 43 ) , non - hodgkin lymphoma ( c82 - 85 ) , multiple myeloma ( c90 ) , and leukaemia ( c91 - 95 )  . 
we included all other invasive cancers ( the remaining icd - 10 c codes , except non - melanoma skin cancer [ c44 ] ) as other and unspeci ed cancers . there concluded has su cient evidence of carcinogenicity in human beings in relation to active tobacco smoking : 11 , 12 of the sites listed above , mouth and pharynx , oesophagus , stomach , colorectum , pancreas , lung , mucinous tumours of the ovary , kidney , and myeloid leukaemia ( c92 ) , and , additionally , liver ( c22 ) , larynx , nasal cavity and nasal sinuses ( c30 - 32 ) , cervix ( c53 ) , and urinary tract , including renal pelvis and ureter ( c65 , 66 , 68 )  . 
when comparing smoking - related and other cancers , we excluded from our analysis cancers of ill - de ned and unspeci ed sites , which might include some smokingrelated cancers ( icd - 10 c26 , c39 , c57 , c76 - 80 and c95 - 96 ) , and cancers of the ovary ( for a substantial proportion of which histological subtype was not known , and which might have included mucinous tumours )  . cm , 1601649 height was reported by participants at recruitment in feet and inches , and converted to centimetres for our analysis . 
for the analyses , women were divided into six categories of reported height ( < 155 cm [ reference group ] , cm , 1551599 1701749 cm , and 175 cm and taller ) ; we took the average height in each of these categories to be the mean measured height in that category in the sample whose height was measured in 200609 . 
standardised to the distribution of categories of self - reported height in our whole analysis population . table 1 : baseline characteristics by height and follow - up for incident cancer in the million women study 786 vol 12 august 2011 articles women rr ( 95% fci ) incident cancers < 155 cm ( mean 1528 cm ) 233 516 15 792 100 ( 098102 ) 155 cm ( mean 1565 cm ) 196 773 14 213 108 ( 107110 ) 160 cm ( mean 1604 cm ) 388 515 28 806 112 ( 111114 ) 165 cm ( mean 1649 cm ) 288 893 22 571 120 ( 118122 ) 170 cm ( mean 1690 cm ) 143 289 11 902 128 ( 125130 ) 175 cm ( mean 1738 cm ) 46 138 4092 137 ( 133142 ) analysis strati ed by age at recruitment and region and adjusted for socioeconomic status , smoking , alcohol intake , body mass index , strenuous exercise , age at menarche , parity , and age at rst birth . table 2 : relative risks ( rrs ) and 95% oated cis ( fcis ) for total cancer incidence , by category of height reported at recruitment ( mean measured height ) cancer ( icd10 c44 ) registered before recruitment and if they did not have valid information on height at recruitment ( including a small proportion , about 005% whose reported height was < 120 cm or > 200 cm )  . 
for analyses including endometrial and / or cervical cancers , we excluded women if they reported a hysterectomy at recruitment , or if their hysterectomy status was unknown ; similarly , for analyses of ovarian cancer , we excluded women reported a bilateral they oophorectomy at recruitment , or if their oophorectomy status was unknown . from we calculated woman - years the date of recruitment to the date of rst cancer registration ( at any site ) , death , or the last date of follow - up , whichever was rst . 
for analyses of cancer incidence , the last date of follow - up was dec 31 , 2008 , for the uk regions of east anglia and south west ; june 30 , 2008 , for oxford , thames , west midlands , and north west ( mersey ) ; and dec 31 , 2007 , for northern and yorkshire , trent , north west ( manchester and lancashire ) , and scotland . statistical analysis we used cox regression models to estimate relative risks ( rrs ) and cis in relation to height at recruitment , taking attained age as the underlying time variable . 
we strati ed all analyses by age at recruitment ( < 52 , 5355 , 5658 , 5961 , 6264 , 65 years ) and region ( ten regions covered by ten cancer registries ) , and adjusted , as appropriate , for quintiles of socioeconomic group ( based on townsend deprivation score13 ) , body - mass index ( < 225 , 225249 , 250274 , 275299 , 30 kg / m ) , strenuous exercise ( less than once a week , once a week or more ) , alcohol consumption ( none , 2 units per week , 3 units per week ) , smoking ( never , past , current 114 cigarettes per day , current 15 cigarettes per day ) , age at menarche ( < 13 , 13 , 14 years ) , parity ( 0 , 12 , 3 full - term pregnancies ) , and age at rst birth ( < 25 , 25 years )  . 
 we calculated the rr per 10 cm increase in height as a trend across the six category means using the measured mean height in each category of reported height.14 we assessed heterogeneity of trends in rrs between di erent cancer sites with a ( ) contrast test , under the survival analysis assumptions that estimates at each cancer site are asymptotically normally distributed and , because of censoring at rst cancer diagnosis at any site , uncorrelated ( and that therefore site - speci c estimates account for competing risks of cancers at other sites ) .15 where two categories of exposure are compared ( as in the text ) conventional cis are given . 
for analyses of total cancer , where more than two categories are compared ( as in the gures ) , oated cis ( fcis ) were estimated by treating the rrs as oating absolute risks ( fars ) .16 , 17 use mean height ( cm ) figure 1 : relative risks ( rrs ) and 95% oated cis ( fcis ) for total incident cancer , by height rrs are adjusted for age , region , socioeconomic status , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth , and are plotted against the mean measured height in each category . 
all results are presented in the text with 95% cis , but for analyses by cancer site , when multiple rrs were estimated , 99% cis are given in the gures . where we present results in the form of plots , the rrs and their corresponding fcis or cis are represented by squares and lines with the area of each square inversely proportional to the variance of the logarithm of the corresponding rr . 
this shows the amount of statistical information involved . meta - analysis we identi ed published prospective studies of adult height and risk of total cancer ( incidence or mortality ) through electronic searches of published work ( medline and embase , up to april , 2011 ) with combinations of the search terms height , body size , anthropometr * , neoplasms , mortality , and risk factors , and vol 12 august 2011 articles number of incident cancers mouth and pharynx 1095 oesophagus 1167 stomach 1177 colon 6281 rectum 3190 pancreas 2044 lung 8074 melanoma 3583 breast 39 299 endometrium 5810 ovary 4830 kidney 1665 bladder 1354 cns 2328 non - hodgkin lymphoma 3411 1215 multiple myeloma leukaemias 1482 other and unspecifed 8997 total cancer 97 376 rr * & 99% ci 094 ( 082108 ) 104 ( 091119 ) 103 ( 090118 ) 125 ( 117132 ) 114 ( 105124 ) 105 ( 095117 ) 103 ( 098108 ) 132 ( 122142 ) 117 ( 114120 ) 119 ( 112126 ) 117 ( 109125 ) 129 ( 115145 ) 100 ( 088114 ) 120 ( 109132 ) 121 ( 112131 ) 113 ( 099129 ) 126 ( 111142 ) 115 ( 110121 ) 116 ( 114117 ) through cited references in identi ed papers . 
we included in our meta - analysis all identi ed studies with published age - adjusted rr and 95% cis for total cancer per 10 cm increase in height , or with su cient published data to allow estimation of such rrs . 
where only categorical results were published , we calculated the trend in rr per 10 cm increase in height using the mean height in each height category ( estimated , where necessary , as category midpoints , or by other methods ) , 18 assuming linearity of log rrs and with a summary trend estimate obtained by the method of generalised least squares.19 we combined results for subgroups of total cancer ( eg , smoking - related and other cancers ) by least squares , where necessary . 
where the mean year of birth of the study population was not given , we made an estimate with the average age at , and year of , study recruitment . 
 results the 1 297 124 women included in our analysis had a mean age at recruitment of 561 years ( sd 49 ) and an average year of birth of 1942 . 
the median length of follow - up was 94 years per woman ( iqr 84102 years ) , for a total of 117 million person - years , during which 97 376 incident cancers were noti ed . table 1 shows characteristics of the study population , including measured height , by six categories of height reported at recruitment . 
taller women tended to be of higher socioeconomic status , to drink more alcohol , to be more active , to have a later age at menarche , to have fewer children , and to have their rst child later in life than shorter women . 
based on heights measured in the validation sample , the mean height in the study population was 1609 cm ( sd 64 )  . total cancer incidence rose with increasing height ( table 2 )  . 
comparing women in the tallest group with 075 125 figure 2 : relative risks ( rrs ) and 99% cis per 10 cm increase in height for incident cancer at 17 speci c sites and for total cancer the doted line represents the rr per 10 cm increase in height for total cancer . 
 there is heterogeneity across cancer sites ( contrast test [ 17 degrees of freedom ] = 1152 ; p < 00001 ) mostly because of the greater than average increase in risk with increasing height for colon cancer and for malignant melanoma , and the lower than average risk for lung cancer . 
however , the overall rr of incident cancer in relation to height was not materially altered when we excluded breast cancer cases from our analysis ( rr per 10 cm increase in height 115 , 95% ci 113116 )  . 
 we adjusted our results in gures 1 and 2 and in table 2 by age , region , socioeconomic status , smoking , alcohol , body - mass index , physical activity , age at menarche , parity , and age at rst birth . 
table 3 shows the e ect of adjustment by potential confounding variables on the rr for total cancer per 10 cm increase in height in an analysis restricted to the 1 087 489 women with full information on all adjustment variables . 
compared with the risk with adjustment for age and region only ( rr 114 , 95% ci 113115 ) , additional adjustment by the remaining factors increases the rr slightly to 116 ( 115118 )  . figure 3 shows the rr for total cancer per 10 cm increase in height , and the mean measured height , in subgroups of women de ned by their year of birth , socioeconomic status , smoking status , alcohol con sumption , body - mass index , physical activity , age at menarche , parity , age at rst birth , menopausal status , and use of oral contraceptives and hormone replacement therapy . 
as we expected , women born before 1939 were shorter than women born in 1946 or later ( mean measured height 1599 vs 1615 cm ) , as were women from the lowest compared to the highest socioeconomic tertile ( 1601 vs 1614 cm )  . 
although the risk for total cancer is somewhat higher in women in the lowest tertile of socioeconomic 125 figure 3 : relative risks ( rrs ) and 99% cis per 10 cm increase in height for all incident cancer , by various characteristics at recruitment the dotted line represents the rr per 10 cm increase in height for all women . 
rrs are adjusted as appropriate for age , region , socioeconomic status , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
the rr per 10 cm greater height was 119 ( 95% ci 117121 ) in never smokers , but only 111 ( 108114 ) in current smokers ( p < 00001 for hetero geneity )  . 
 vol 12 august 2011 articles mouth and pharynx oesophagus stomach colon rectum pancreas lung melanoma breast ovary kidney bladder endometrium 2960 1493 1943 18 533 3192 2426 1194 non - hodgkin lymphoma 1630 multiple myeloma leukaemias other and unspecifed 3616 total cancer 42 244 highest socioeconomic third middle socioeconomic third lowest socioeconomic third mean height ( cm ) figure 4 : relative risks ( rrs ) and 95% oated cis ( fcis ) for all incident cancer in relation to height , and by socioeconomic status the baseline category ( rr = 10 ) is women shorter than 160 cm from the highest socioeconomic group . 
rrs are adjusted for age , region , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
rrs are plotted against the mean measured height in each category of height ( < 160 cm , 160165 cm , 165170 cm , 170 cm ) , within categories of socioeconomic status . never smokers number of incident cancers current smokers number of incident cancers figure 5 shows the rrs per 10 cm increase in height by cancer site in never smokers and in current smokers ( results in past smokers are uninterpretable , because they are a heterogeneous group with a wide range of times since last smoking )  . 
the mix of cancers di ers in the two groups with , as expected , a higher proportion of women with lung and other smoking - related cancers in current smokers than in never smokers . 
in never - smokers , heterogeneity across cancer sites was substantially weaker ( p = 0004 ) than in current smokers ( p < 00001 )  . for smoking - related cancers , the rr per 10 cm greater height was substantially smaller in current smokers than in never smokers ( 105 vs 117 , p for di erence = 00004 ; gure 6 )  . 
 * rrs are adjusted for age , region , socioeconomic status , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
the overall pattern of rrs remained similar , with lower risk for smoking - related cancers than for other cancers in current smokers , although the di erence between these risks was reduced ( rr per 10 cm height 102 , 95% ci 097106 , in current smokers and 110 , 103117 , in never smokers ; p for di erence = 005 ) ; for other speci ed cancers , risks remained similar to those in our main analysis ( rrs 118 , 114122 , in current smokers and 119 , 116121 , in never smokers )  . 
 because breast cancer dominates our ndings , we repeated our analyses shown in gure 3 separately for the ve most common cancers in our study : breast , lung , colon , endometrium , and ovary , and for the remaining cancers . 
overall , we did not identify signi cant heterogeneity , by the 12 factors we show in gure 3 , for these cancer sites ( test for heterogeneity aggregated across all characteristics : colon p = 07 , lung p = 02 , breast p = 03 , endometrium p = 05 , ovary p = 02 , remaining cancers p = 02 )  . because there was no strong variation by cancer site in our study except in smokers , we did a meta - analysis of published studies of all - cancer risk , noting for each study the proportion of current smokers in the study population . 
 figure 7 shows details of our study together with ten other prospective studies1 , 3 , 8 , 2128 that have published results in such a way as to allow estimation of the rr of total cancer incidence or mortality per 10 cm increase in height . 
the populations covered include men and women from asia , australasia , europe , and north america , with mean years of birth ranging over three decades ( 1917 to 1946 ) , and with mean heights ranging over 24 cm ( 155 to 179 cm )  . 
there was no signi cant heterogeneity between the results from studies in men ( i for heterogeneity 0% , p = 09 ) or between those in women ( i for heterogeneity 31% , p = 02 ) , but there was a slightly lower height - associated rr in men than in women ( 110 vs 115 , p for di erence < 00001 )  . 
when we excluded the ndings of our study , the summary rr in women was slightly reduced ( summary rr per 10 cm greater height 113 , 95% ci 110116 ; i for heterogeneity 25% ; p = 02 ) , and there was no longer signi cant heterogeneity between studies in men and those in women ( p for di erence = 01 )  . 
all of the mortality studies we included provided rrs adjusted for at least one measure of socioeconomic status , which should have minimised potential confounding due to the relation in many populations between socioeconomic status and cancer survival.29 discussion we identi ed a clear and highly signi cant trend of increasing cancer risk with increasing height in this large prospective study of uk women , with rr for total incident cancer of 116 ( 99% ci 114117 ) for every 10 cm greater height . 
the magnitude of the height - associated increase in cancer risk was similar for women with di erent years of birth , from di erent socioeconomic groups , and across subgroups de ned by alcohol intake , body - mass index , physical activity , age at menarche , parity , age at rst birth , menopausal status , and use of oral contraceptives or hormone replacement therapy . 
by contrast , current smokers had a lower rr for total cancer incidence per 10 cm increase in height than never smokers , and this was largely because the height - associated cancer rrs in smokers were lower for smoking - related than for other cancers . 
 each of the 17 most common speci c sites we assessed included 1000 or more cancers , and together they constitute some 90% of total incident cancers in our study population . 
most previous studies had limited statistical power to study site - speci c cancer risk and tended to focus on a few common cancer sites , and our results for the common cancers are consistent with their ndings.2 , 47 all study participants were routinely linked to records of the nhs central registers and details of every incident cancer and death were coded before noti cation to the study investigators , thus providing complete and nondi erential ascertainment of cancer incidence during follow - up . 
there was excellent correlation between self - reported and measured height , consistent with previous ndings for height and some this cohort.30 , 31 other anthropometric variables nevertheless , we corrected for measurement error , and for changes in height over time , by use of the mean measured height in each category to calculate rr per 10 cm increase in height . 
 as expected , the average height of women in this population was slightly greater the more recently they were born and with increasing socioeconomic status ( gure 3 )  . 
method of chne and thompson18 used to estimate mean heights in height categories . 075 group , age at menarche , parity , age at rst birth , bodymass index , physical activity , smoking status , and alcohol consumption . 
women in higher socioeconomic groups are on average taller ( table 1 ) , and socioeconomic status is related to total cancer incidence ( gure 4 ) , 29 yet the association between height and risk of cancer was similar for women of low , medium , and high socioeconomic status . 
as in other studies that could adjust for a range of potential confounding factors , our results suggest that the relation between height and cancer risk is not due to other known risk factors for cancer.9 our ndings show that the height - related rr of cancer was lower for smoking - related cancers than for other cancers , but only in current smokers . 
in accordance with our ndings kabat and colleagues32 have reported that lung cancer incidence in the womens health initiative study showed a stronger association with height in never smokers than in current or past smokers . 
smoking - related cancers are more common in current smokers than in never smokers , with agestandardised incidence rates of 599 and 176 , respectively per 100 000 women per year , in this cohort . 
the estimated excess age - standardised incidence rate for every 10 cm increase in height for smoking - related cancers is about 30 per 100 000 women per year , both in current and in never smokers ( 599 005 for current smokers and 176 017 for never smokers )  . we found no other modi cation of height - associated rr by the 11 other factors we assessed , either for total cancer , or separately for the ve most common cancers ( breast , lung , colon , endometrium , and ovary )  . 
 there was little variation in height - associated rrs at speci c cancer sites in never smokers , in whom the e ect of height on cancer risk is free from modi cation by smoking . 
in general , studies have found taller people to be at increased risk of a range of cancers with varying causes , with no individual cancer site consistently identi ed as showing no association.2 , 47 our nding of di erences in height - related rr between smokers and never smokers might provide an explanation for some reported inconsistencies in height - associated risk for smoking - related cancers.2 our meta - analysis of height and total cancer risk shows that ndings are very consistent for incidence and for mortality , and in populations from europe , north america , asia , and australasia with mean years of birth ranging over 30 years , and with mean heights ranging from 155 cm to 179 cwomen in these studies were less likely than men to be current smokers ( gure 7 ) and this might partly explain the slightly higher heightassociated rr in women than in men in our metaanalysis . 
the overall result in women is also strongly weighted by the results from the million women study , in which there has been allowance for measurement error , and more extensive adjustment than in the other studies , both of which tended to increase the estimated rr . 
as in any meta - analysis of published data , our ndings need to be interpreted in the knowledge that other studies with relevant data might not have published their results . 
 the similarity of the height - associated rr for di erent cancers and in di erent populations suggests that a basic common mechanism , possibly acting in early life , might be involved.8 adult height reaches its maximum between the ages of 20 and 30 years . 
variation in height relates to genetic and environmental in uences acting mostly in the rst 20 years , or so , of life ; environmental factors , including childhood nutrition and infections , are believed to predominate.3336 hormone levels , especially of growth factors such as insulin - like growth factors ( igfs ) , both in childhood and in adult life , might be relevant.2 , 9 circulating levels of igfs in adulthood and childhood a ect cancer risk ; 3740 igf - i levels in childhood and adolescence are strongly related to skeletal growth , 38 and levels in adulthood , although less strongly , to adult height.41 , 42 another possibility is that height predicts cancer risk because taller people have more cells ( including stem cells ) , and thus a greater opportunity for mutations leading to malignant transformation.43 , 44 height might thus be related to cancer risk through increased cell turnover mediated by growth factors , or through increased cell numbers . 
adult height in european populations has increased by about 1 cm per decade throughout the 20th century.33 , 45 , 46 the increase in adult height during the past century could thus have resulted in an increase in cancer incidence some 1015% above that expected if population height had remained constant . 
all authors approved the report . con icts of interest we declare that we have no con icts of interest . acknowledgments we thank all the women who participated in the study , sta from participating nhs breast screening centres , and family doctors , practice nurses , and other primary - care sta for help with validation measurements . 
we thank gary whitlock for helpful contributions to the manuscript . articles lancet oncol 2012 ; 13 : 94656 published online august 3 , 2012 s1470 - 2045 ( 12 ) 70322 - 4 see comment page 862 * collaborators listed at end of paper correspondence to : secretariat , collaborative group on epidemiological studies of ovarian cancer , cancer epidemiology unit , richard doll building , oxford ox3 7lf , uk collaborations@ceu.ox.ac.uk ovarian cancer and smoking : individual participant meta - analysis including 28 114 women with ovarian cancer from 51 epidemiological studies collaborative group on epidemiological studies of ovarian cancer * summary background smoking has been linked to mucinous ovarian cancer , but its e ects on other ovarian cancer subtypes and on overall ovarian cancer risk are unclear , and the ndings from most studies with relevant data are unpublished . 
 to assess these associations , we review the published and unpublished evidence . methods eligible epidemiological studies were identi ed by electronic searches , review articles , and discussions with colleagues . 
individual participant data for 28 114 women with and 94 942 without ovarian cancer from 51 epidemiological studies were analysed centrally , yielding adjusted relative risks ( rrs ) of ovarian cancer in smokers compared with never smokers . findings after exclusion of studies with hospital controls , in which smoking could have a ected recruitment , overall ovarian cancer incidence was only slightly increased in current smokers compared with women who had never smoked ( rr 106 , 95% ci 101111 , p = 001 )  . 
of 17 641 epithelial cancers with speci ed histology , 2314 ( 13% ) were mucinous , 2360 ( 13% ) endometrioid , 969 ( 5% ) clear - cell , and 9086 ( 52% ) serous . 
for mucinous cancers , incidence was increased in current versus never smokers ( 179 , 95% ci 160200 , p < 00001 ) , but the increase was mainly in borderline malignant rather than in fully malignant tumours ( 225 , 95% ci 191265 vs 149 , 128173 ; pheterogeneity = 001 ; almost half the mucinous tumours were only borderline malignant )  . 
both endometrioid ( 081 , 95% ci 072092 , p = 0001 ) and clear - cell ovarian cancer risks ( 080 , 95% ci 065097 , p = 003 ) were reduced in current smokers , and there was no signi cant association for serous ovarian cancers ( 099 , 95% ci 093106 , p = 08 )  . 
these associations did not vary signi cantly by 13 sociodemographic and personal characteristics of women including their body - mass index , parity , and use of alcohol , oral contraceptives , and menopausal hormone therapy . interpretation the excess of mucinous ovarian cancers in smokers , which is mainly of tumours of borderline malignancy , is roughly counterbalanced by the de cit of endometrioid and clear - cell ovarian cancers . 
the substantial variation in smoking - related risks by tumour subtype is important for understanding ovarian carcinogenesis . funding cancer research uk and mrc . introduction until recently , smoking was not thought to be a risk factor for ovarian cancer , but in 2009 the international agency for research on cancer added mucinous ovarian tumours ( which comprise about a tenth of all ovarian cancers ) to their list of tobacco - related cancers.1 we identi ed 56 epi demiological studies of ovarian cancer that obtained information about womens smoking history . 
some results have been published from 55 of the 56 studies , 256 but results on smoking - related risks have been pub lished from only about a third of these studies.4 , 5 , 10 , 15 , 16 , 18 , 20 , 23 , 27 , 32 , 34 , 35 , 43 , 44 , 46 , 50 , 53 , 54 , 56 almost all reported little or no association between smoking and overall risk of ovarian cancer ; some , but not all , reported an increased risk of mucinous tumours in smokers , but not for other subtypes of ovarian cancer . the collaborative group on epidemiological studies of ovarian cancer was set up to bring together and reanalyse the available epidemiological evidence , published and unpublished , on the association between various factors and ovarian cancer risk.57 to avoid selective emphasis on results from the few studies that have published their ndings , this report sought data from all studies larger than a speci c size that have obtained relevant information about the relation between ovarian cancer risk and womens smoking history , whether published or not . methods search strategy and selection criteria this collaboration began in 1998 , and since then potentially eligible epidemiological studies have been sought regularly by searches of review articles and from computer - aided literature searches in medline , embase , and pubmed , with combinations of the search terms ovarian cancer , ovary cancer , smok * , and tobacco . 
 to be eligible for these analyses , studies needed to have obtained individual data for womens reproductive history , use of hormonal therapies , and smoking history and to have studied at least 200 women with ovarian 946 vol 13 september 2012 the collaboration after 2009 , so reliable analyses of these aspects of smoking could not be done . 
apparent inconsistencies in the data were recti ed , where possible , number of cases / controls median year of diagnosis of cases median year of birth of cases mean age at diagnosis of cases ( years ) cancer ( before 2006 , studies with less than 200 cases of ovarian cancer had been eligible , so there are fewer cases in some early studies )  . 
studies that had obtained relevant data , but had not published on ovarian cancer and smoking , were sought by correspondence with colleagues , by discussions at collaborators meetings , and by electronic searches with additional terms cohort , prospective , women , and cancer risk . we identi ed 56 eligible studies and invited principal investigators from each to participate in the collaboration . 
thus , data from 51 of the 56 eligible studies identi ed are analysed in this report , and implications of the slight incompleteness are discussed later . data extraction cases were women with malignant epithelial ( borderline malignant or fully malignant ) or with non - epithelial ovarian cancer and controls were women without ovarian cancer who had not undergone bilateral oophorectomy . 
 information sought from principal investigators about each individual case and control included their age , ethnic group , education , alcohol and tobacco use , height , weight or body - mass index ( bmi ) , age at menarche , reproductive history , use of hormonal contraceptives , use of menopausal hormonal therapy , hysterectomy , and family history of ovarian or breast cancer . 
so that similar analytical methods could be used across studies , we incorporated cohort studies using a nested casecontrol design , in which up to four controls were selected at random , matched by age at cancer diagnosis and , where appropriate , by broad geographical region . 
in one cohort study , 21 cases were women with fatal ovarian cancer , whereas in all other studies cases were women with incident disease . principal investigators of the 51 epidemiological studies ( one of which is unpublished ) in these analyses251 provided individual information about smoking history for cases and controls . 
the information provided was used to classify all women as ever or never smokers , and in all but three studies7 , 14 , 45 ever smokers could be classi ed as either current or past smokers . 
after the records had been checked and corrected , investigators were sent summary tables and listings of the variables to be used in analyses for nal con rmation that their data had been correctly interpreted . information about histological classi cation and malignant potential of the ovarian cancers was sought from principal investigators . 
the epithelial cancers were then classi ed as clear - cell , endometrioid , mucinous , serous , other , mixed , or nos , and were further subdivided by their malignant potential as borderline malignant , fully malignant , and not known whether borderline or fully international investigators provided malignant . 
information about ovarian cancer histology was provided by investigators of all but ve9 , 10 , 12 , 21 , 36 of the 51 participating studies ; not all studies had included non - epithelial and borderline malignant ovarian cancer . statistical analysis we used conditional logistic regression to calculate the relative risk ( rr ) of ovarian cancer in relation to smoking history ( ie , the incidence rate ratio among otherwise similar women of the same age , calculated as the ratio of the odds of smoking among cases to the odds of smoking among controls )  . 
to ensure that women in one study were compared directly only with otherwise similar women in the same study , all analyses were routinely strati ed by study , by centre within study , by ne divisions of age ( 5 - year age groups up to 8589 years ) , ever use of menopausal hormonal therapy ( yes , no ) , menopausal status or hysterectomy ( premenopausal or perimenopausal , natural menopause before age 50 years , natural menopause at or after age 50 years , previous hysterectomy , other or unknown ) , and bmi ( < 25 kg / m , 25 kg / m ) and were routinely adjusted by parity ( 0 , 12 , 3 ) and use of oral contraceptives ( no or yes for durations of < 5 years and 5 years )  . 
for other potential confounding factors ( year of birth , ethnic origin , education , family history of ovarian or breast cancer , age at menarche , and alcohol use ) , we did sensitivity analyses comparing results before and after adjustment for each variable in turn and for all simultaneously . 
smoking status was treated as a dichotomous outcome ( current vs never ) and the term for tumour subtype was treated as the variable of interest in a conditional logistic regression , strati ed and adjusted as described previously . analyses were done using stata ( version 11 )  . 
the position of the square shows the value of the rr and its area is inversely proportional to the variance of the logarithm of the rr , thereby providing an indication of the amount of statistical information available for that particular estimate . 
when results from many studies , tumour subtypes , or many subgroups are many presented in the gures , the lines show 99% cis ( rather than 95% cis ) to help to allow for multiple testing . 
when the main results are given in the text , however , 95% cis are used . role of the funding source the funders had no role in study design , data collection , analysis or interpretation of data , preparation of the report , or the decision to publish . 
all members of the analysis and writing committee ( vb , kg , ch , km , rp , gr ) had access to the raw data and are responsible for the nal submission for publication . results table 1 shows details of the women in the 51 participating studies . 
 over all , the studies contributed 28 114 women with ovarian cancer ( cases ) and 94 942 women without ovarian cancer ( controls ) , with 10 362 ( 37% ) cases from europe and 12 817 ( 46% ) from north america . 
 * including one unpublished study ( guangzhou , china )  . women were younger than 35 years at diagnosis , 2696 ( 10% ) were aged 3544 years , 6467 ( 23% ) were 4554 years , 9206 ( 33% ) were 5564 years , and 8322 ( 30% ) were 65 years or older . 
 the ndings varied signi cantly by study design ( pheterogeneity < 00001 ) with a slightly increased risk of ovarian cancer in ever - smokers in prospective studies ( rr 106 , 95% ci 101111 , p = 002 ) and in casecontrol studies with population controls ( rr 108 , 95% ci 103114 , p = 0003 ) , but an apparent reduced risk in studies with hospital controls ( rr 081 , 95% ci 075089 , p < 00001 )  . 
we could not exclude the possibility that hospital controls were more likely to have vol 13 september 2012 articles number of cases in current / past / never smokers current smokers past smokers relative risk in current smokers vs never smokers ( 99% ci ) relative risk in past smokers vs never smokers ( 99% ci ) all women 4587 / 5835 / 12 040 all in studies with recorded histology 4057 / 5235 / 10 522 all epithelial 3803 / 4914 / 9819 clear - cell endometrioid mucinous 159 / 237 / 573 411 / 574 / 1375 735 / 545 / 1034 serous 1751 / 2494 / 4841 other or mixed 552 / 838 / 1522 epithelial nos non - epithelial 195 / 226 / 474 79 / 63 / 180 malignant tumour nos 175 / 258 / 523 106 ( 100113 ) 107 ( 100114 ) 107 ( 100114 ) 080 ( 063101 ) 081 ( 070094 ) 179 ( 147217 ) 099 ( 091108 ) 113 ( 096133 ) 117 ( 088156 ) 090 ( 062130 ) 119 ( 089159 ) 106 ( 100112 ) 105 ( 099111 ) 106 ( 100113 ) 091 ( 073113 ) 092 ( 080106 ) 116 ( 098137 ) 106 ( 098115 ) 114 ( 099131 ) 110 ( 085143 ) 084 ( 057123 ) 101 ( 080127 ) figure 2 : relative risk of subtypes of ovarian cancer in current and past smokers compared with never smokers strati ed by study , age at diagnosis , menopausal status or hysterectomy , body - mass index , and ever use of hormonal therapy and adjusted for parity and duration of oral contraceptive use . 
nos = not otherwise speci ed . conditions associated with smoking and thus not be representative of smoking habits the general population and so we omitted studies with hospital controls from all subsequent analyses . after excluding studies with hospital controls , we found a small increase in the risk of ovarian cancer in ever smokers compared with never smokers ( rr 107 , 95% ci 103110 , p < 00001 )  . 
there was no signi cant heterogeneity in the rr estimates between prospective studies and casecontrol studies with population controls , nor between studies within each of these designs ( p > 005 for all comparisons )  . 
all studies were of incident ovarian cancer except one ( of fatal ovarian cancer21 ) and results were similar for both incident and fatal disease ( gure 1 )  . 
 after further exclusion of the studies unable to di erentiate between current and past smokers , the rr of ovarian cancer in ever smokers was 106 ( 95% ci 103109 ) and was similar in current ( 106 , 95% ci 101111 , p = 001 ) and in past smokers ( 106 , 95% ci 102111 , p = 0003 ) ( gure 2 )  . 
of the 22 462 cases of ovarian cancer in gure 2 , almost 90% ( 19 814 ) were from studies that had recorded information about tumour histology , and the rr estimates for current and past smokers were similar when analyses were restricted to these women . 
there was a 10 - year range in mean age at diagnosis by subtype , from mean 586 ( sd 104 ) years in women with fully malignant serous tumours to 488 ( 135 ) years in those with borderline malignant serous tumours . in current versus never smokers , rrs varied substantially by histological subtype of the tumour ( gure 2 )  . 
 * fully malignant or borderline malignant status was not known for all cases ; there were only two borderline malignant clear - cell , 36 border line malignant endometrioid , and ve borderline malignant mixed tumours . table 2 : distribution and characteristics of subtypes of ovarian cancer in studies with recorded histology increased in current versus never smokers ( rr 179 , 95% ci 160200 , p < 00001 ) , but for endometrioid and for clear - cell tumours , there were signi cantly reduced risks ( rr 081 , 95% ci 072092 , p = 0001 , and rr 080 , 95% ci 065097 , p = 003 , respectively )  . 
the 950 vol 13 september 2012 articles number of cases in current / past / never smokers current smokers relative risk in current smokers vs never smokers ( 99% ci ) relative risk in past smokers vs never smokers ( 99% ci ) past smokers 107 ( 100114 ) 106 ( 100113 ) 3803 / 4914 / 9819 all epithelial fully malignant clear - cell endometrioid mucinous serous 159 / 229 / 563 406 / 555 / 1334 365 / 318 / 628 1383 / 2073 / 4042 borderline malignant 0 / 2 / 0 clear - cell 4 / 8 / 24 endometrioid 368 / 219 / 397 mucinous 351 / 343 / 695 serous 080 ( 063101 ) 082 ( 071095 ) 149 ( 117189 ) 096 ( 087106 ) insucient data insucient data 225 ( 164308 ) 115 ( 094141 ) 090 ( 072112 ) 091 ( 079105 ) 108 ( 088133 ) 105 ( 096115 ) insucient data insucient data 128 ( 098167 ) 108 ( 088132 ) figure 3 : relative risk of clear - cell , endometrioid , mucinous , and serous epithelial ovarian tumours by malignant potential and smoking history strati ed by study , age at diagnosis , menopausal status or hysterectomy , body - mass index , and ever use of hormonal therapy and adjusted for parity and duration of oral contraceptive use . 
the dotted line represents the overall result for all women . di erences in smoking - related risk across these four speci c subtypes of epithelial ovarian cancer were signi cant ( hetero geneity p < 00001 )  . the association between mucinous ovarian cancer and current smoking varied further when cancers were subdivided by their malignant potential ( gure 3 )  . 
the increased risk was much greater for borderline malignant ( rr 225 , 95% ci 191265 ) than for fully malignant mucinous cancers ( rr 149 , 95% ci 128173 ) ( heterogeneity p = 001 )  . 
neither the increased risk of borderline malignant nor that of fully malignant mucinous tumours in current smokers were driven by the ndings in any one study or groups of studies ( gure 4 )  . 
for serous tumours , the di erence in risk between borderline malignant and fully malignant cancers in current smokers was not signi cant ( rr 115 , 95% ci 099133 , and rr 096 , 95% ci 089104 ; heterogeneity p = 04 ; gure 3 )  . 
relative risk ( rr ) estimates were strati ed by study and age at diagnosis , and , where appropriate , menopausal status or hysterectomy , body - mass index , and ever use of menopausal hormone therapy , and adjusted by parity and duration of oral contraceptive use . 
there was no material increase or decrease in risk of other ovarian cancer subtypes in past versus never smokers ( gure 3 )  . all analyses in gures 24 were strati ed by age , study , use of menopausal hormone therapy , menopausal status or hysterectomy , and bmi and adjusted by parity and duration of oral contraceptive use . 
additional adjustment by year of birth , ethnic origin , education , family history of ovarian or breast cancer , age at menarche , and alcohol use changed the rr estimates by less than 2% . 
 952 vol 13 september 2012 articles furthermore , the observed associations between current smoking and overall risk of ovarian cancer , and the risk in the endometrioid , mucinous , and serous subtypes , did not vary substantially by year of birth , age at diagnosis , ethnic origin , education , alcohol use , bmi , parity , age at menarche , use of oral contraceptives , having a rstdegree relative with ovarian or breast cancer , menopausal status , hysterectomy , or use of menopausal hormone therapy ( table 3 )  . 
there were too few clear - cell tumours to compare reliably the association with smoking between subgroups . there was no signi cant heterogeneity between prospective studies and casecontrol studies with population controls in the association between current smoking and ovarian cancer risk overall ( heterogeneity p = 02 ) or when analyses were restricted to mucinous , endometrioid , and serous tumour subtypes ( hetero geneity : mucinous , p = 02 ; endometrioid , p = 04 ; serous , p = 007 )  . discussion this collaboration has brought together and reanalysed individual participant data for about 28 000 women with ovarian cancer from 51 studies of the e ect of smoking on ovarian cancer incidence . 
although current smoking was associated with an excess of mucinous ovarian cancer , as had been reported previously , 1 we found that the increase was mainly in tumours of borderline malignancy rather than in fully malignant tumours . 
the signi cant adverse and favourable e ects of current smoking were attenuated in past smokers , so past smoking had little net e ect on ovarian cancer incidence . to selectively results of casecontrol studies that used hospital controls di ered qualitatively from those of studies that used other designs . 
these di erences are unlikely to be due merely inaccurate retrospective reporting of smoking , since the results di er substantially between the retrospective studies using hospital controls and the retrospective studies using population controls . 
since smoking is associated with various diseases that could lead to hospital admission it is plausible that , on average , the hospital controls were more likely to smoke than were women in the general population . 
nevertheless , to ensure that all the epidemiological information is published , details of those studies are included in table 1 and in gure 1 . smoking history and the retrospective reporting of smoking might have been di erentially a ected by the cases knowledge that they had ovarian cancer . 
although these possibilities cannot be excluded , the similarity of the ndings in casecontrol studies with population controls and in studies with prospective recording of smoking suggests that they might not be a serious issue here . an advantage of seeking to review all epidemiological studies of ovarian cancer with information on smoking , published and unpublished , is that this helps to avoid unduly selective emphasis on published results or on just some studies . 
only a third of eligible studies have published on the association between smoking and risk of ovarian cancer , so reviews based solely on published studies could have been susceptible to publication bias . 
 eligible studies that did not contribute data to this collaboration , but had published on ovarian cancer risk associated with smoking , 53 , 54 , 56 together contain fewer than a tenth as many cases as are included in the present analyses . 
furthermore , to have completely up - to - date information from continuing prospective studies that are accumulating data beyond the time when information was contributed to this collaboration is not possible . 
ongoing prospective studies will continue to accrue women with ovarian cancer , but there is no good reason to expect that these additional data will materially change the evidence that is already available . a further advantage of bringing together worldwide evidence on the association between ovarian cancer and smoking is that large numbers of cases are needed to assess reliably whether the association varies by tumour subtype . 
misclassi cation of tumour subtype would tend to dilute rr estimates , and blur di erences between them , yet sharp di erences in the smoking - related risks were found ( similar di erences by tumour subtype were not found for other factors such as oral contraceptive use and adiposity57 , 59 )  . the ndings for di erent tumour subtypes were not driven by the results from any one study or group of studies and are unlikely to be due to confounding . 
all analyses were routinely strati ed by age , study , use of menopausal hormone therapy , menopausal status , and bmi and were adjusted by parity and oral contraceptive use ; additional adjustment for six other factors hardly changed the rr estimates . even in casecontrol studies with population controls there might have been some di erential participation by the large proportional increase in risk of mucinous ovarian tumours associated with current smoking , and vol 13 september 2012 articles the di erences between the proportional increases in fully malignant and in borderline malignant mucinous tumours , are both de nite ndings and could re ect a real e ect of smoking . 
although borderline malignant mucinous tumours are less aggressive than fully malignant mucinous tumours , they can have microinvasive or invasive components.60 the proportional reductions in smoking - related risks of clear - cell and endometrioid tumours , although not as great as the proportional increase in mucinous tumours , could also be a real e ect of smoking . 
since information about the amount smoked and the timing of exposure was not sought systematically for this collaboration , little could be done to examine these associations further . smoking is known to a ect the ovaries , in that smokers have an earlier menopause than do non - smokers , 61 but this e ect does not necessarily imply that smoking would a ect ovarian cancer incidence or have di erent e ects on di erent tumour subtypes . 
in particular , endometrial cancer risk is reduced in smokers62 and our nding of a reduced risk of endometrioid tumours in current smokers is consistent with the hypothesis that endometrioid ovarian cancers might have their origin in endometrial cells . 
no equivalent analogy exists for clearcell tumours . smoking has a wide range of adverse e ects resulting in large increases in mortality from many speci c causes.63 although the excess of mucinous tumours in smokers is de nite , it seems to be counterbalanced by a small de cit in clear - cell and endometrioid tumours . 
this study could not address survival , but since about half the mucinous tumours in smokers were of borderline malignancy , smoking is likely to have little net e ect on mortality from ovarian cancer . contributors vb , kg , ch , km , rp , and gr analysed the data , had full access to the pooled data , wrote the rst draft of the report , and had nal responsibility for the decision to submit for publication ; all are guarantors . 
funding for the contributing studies is described in the publications of those studies.251 corrections correction to lancet oncol 2012 ; 13 : 559 correction to lancet oncol 2012 ; 13 : 696 lancet oncology . 
 lancet oncol 2012 ; 13 : 559 the second sentence of the third paragraph of this editorial should read in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
pixantrone dimaleate versus other chemotherapeutic agents as a singleagent salvage treatment in patients with relapsed or refractory aggressive non - hodgkin lymphoma : a phase 3 , multicentre , open - label , randomised trial . 
this correction has been made to the online version as of june 29 , 2012 , and the printed article is correct . vol 13 july 2012 e285 corrections correction to lancet oncol 2012 ; 13 : 983 , 986 correction to lancet oncol 2012 ; 13 : 1028 correction to lancet oncol 2012 ; 13 : e468 fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 this correction has been made as of oct 29 , 2012 . randomised , chemorefractory jfw , van den smits mlj , nijsen holmium - 166 bosch maaj , et al . 
lancet oncol 2012 ; 13 : 102534in table 1 of this article , the total number of patients with ocular melanoma should have been six , as should the total number of patients with colorectal carcinoma . 
lancet oncol 2012 ; 13 : e468in this news item , the second and third sentences of the second paragraph should have read : median pfs was 94 months ( 95% ci 86167 ) in the combination group compared with 58 months ( 4674 ) in the dabrafenib monotherapy group ( hazard ratio 039 , 95% ci 025062 ; p < 0001 )  . 
the corrected version rst appeared at thelancet.com / oncology on june 29 , 2012 for more on the lancet oncologys call for gps to receive better education see leading edge lancet oncol 2009 ; 10 : 97 for more on variation in gp referral patterns for patients with cancer see articles lancet oncol 2012 ; 13 : 35365 for more on the partnership between cancer research uk and the royal college of general practitioners see news lancet oncol 2012 : 12 : e232 for more on qcancer risk calculators see for more on the challenges of supporting patients with multiple morbidities see articles lancet 2012 ; published online may 10 . 
a third of all young cancer patients reported their gps took no action despite presentation with common cancer symptoms and a quarter of patients had to visit the gp four or more times before their symptoms were taken seriously . 
if a young person presents with the same symptoms three times , gps should automatically refer them for further investigation . although the tct survey was small ( collating the opinions of only 300 patients ) , the ndings mirror those of lyratzopoulos and colleagues published in the lancet oncology in april , 2012 , that analysed more than 41 000 patients with 24 types of cancer . 
in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
 so what can be done to restore trust ? usefully , cancer research uk and the royal college of general practitioners have launched an initiative to support gps by putting together models of best practice , and by reviewing care pathways and thresholds for further investigation to ensure gps have better access to diagnostics and secondary care . 
 additionally , the department of health has announced a pilot project within gp practices of cancer - risk prediction tools ( qcancer risk calculators ) developed by researchers at the university of nottingha these successful these partnerships are good examples of engagement between policy makers and physicians with organisations that have a perceptive understanding of the patient viewpoint and of research realities and possibilities . 
 initiatives will be whether transforming the e ectiveness of the gp and improving patient care will take time to assess , but it is unlikely that they will prove to be a broad panacea . 
it is becoming increasingly clear , for example , that the uk health - care system is not designed to cope with multiple comorbiditiesa common situation among patients with cancerand in the future gps will need to take a central and proactive role in coordinating patient care throughout their entire journey within the national health service . 
this will require rethinking of the current infrastructure , and might require adjustments to gps case burdens to ensure su cient time is available for more thorough consultations , especially in socioeconomically deprived areas . while the role of the gp in cancer diagnosis is undeniably important , it is essential not to forget interdependency on improved patient education , screening , secondary care and access to latest treatments , supportive and palliative care , and coordinated long - term follow - up . 
 improved understanding of the factors contributing to the di erences between the uks cancer outcomes and those of other countries will provide important clues and solutions . 800 000 people visit a gp every day in the uk , but questions are increasingly being asked about the competency of those doctors that undermine patient trust . 
however , implementation of this bill could be a fresh start in a process of restoring trust and ensuring gps have access to the best tools necessary to provide a rst - class service and to guarantee all patients receive the best possible care . 
 the lancet oncology vol 13 june 2012 comment if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology as piration of mediastinal and hilar lymph nodes should be used to assess preoperative lung cancer status in countries where tuberculosis is endemic.10 finally , hiv infection is associated with increased lung cancer cases . 
can tuberculosis further increase this risk ? in a study11 that linked aids registry surveillance data for 322 675 patients with aids diagnosed between 1977 and 2002 , with cancer registries in 11 us regions , lung cancer risk over 10 years was unrelated to tuberculosis . 
 tuberculosis awareness in patients with cancer needs to be reinforced , especially in low - burden developed countries , and lung cancer awareness in patients with previous or suspected tuberculosis should be urgently strengthened in developing countries to increase the low numbers of potentially resectable tumours . * sandro vento , massimiliano lanzafame department of internal medicine , faculty of medicine and health sciences , university of botswana , gaborone , botswana ( sv ) ; and infectious diseases unit , gb rossi university hospital , verona , italy ( ml ) ventosandro@yahoo.it we declare that we have no con icts of interest . yu yh , liao cc , hsu wh , et al . 
lancet oncol 2011 ; 12 : 37786in this article ( april ) , on page 380 , the number of women with luminal a breast cancer tested for the kras variant should have been 478 in gure 2a and the percentage of premenopausal women diagnosed with luminal a breast cancer should have been 151% in gure 2b . 
lancet oncol 2011 ; 12 : 41516on page 415 , in the second column , it was stated that 17 variants showed moderate to strong evidence of a true association and were therefore candidates for clinical tests , this should have said 14 variants . 
this correction has been made to the online version as of may 18 , 2011 . published online may 18 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70127 - 9 522 vol 12 june 2011 errata errata lehtinen m , paavonen j , wheeler cm , et al . 
overall e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against grade 3 or greater cervical intraepithelial neoplasia : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 8999in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
cross - protective e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against cervical infection and precancer caused by non - vaccine oncogenic hpv types : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 10010in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
lancet oncol 2012 ; 13 : 1012in this comment ( published online nov 9 , 2011 ) , the last sentence of the sixth paragraph incorrectly lists hpv - 35 as one of the oncogenic hpv types covered by the new nine - type gardasil vaccine ; the list should include hpv - 45 instead . 
this correction has been made to the online version as of jan 3 , 2012 . vol 13 january 2012 editorial published online september 18 , 2012 s1470 - 2045 ( 12 ) 70422 - 9 for more on mortality and cancer incidence in 9 / 11 survivors and emergency services personnel see articles lancet 2011 ; 378 : 87987 , and articles lancet 2011 ; 378 : 898905 9 / 11 survivors to get free cancer treatment the us national institute for occupational safety and health ( niosh ) announced on sept 11 , 2012 , that emergency services workers and other survivors from the terrorist attacks on the twin towers of the world trade center in new york , ny , usa , will now be eligible for free cancer treatment in addition to the compensation announced previously for other diseases . the world trade center health program was established by the james zadroga 9 / 11 health and compensation act of 2010 , and signed in to law by president barack obama in january , 2011 . 
the law , named after a new york police o cer who died of a respiratory disease attributed to working among the devastation , provides us$42 billion of health - care coverage . 
survivors of the attacks on the pentagon and at the crash site in shanksville , pa , usa , will become eligible for the programme later this year . compensation for cancer treatment was held - up by a dispute over whether cancer could be caused by the atrocities . 
although this early conclusion was misguided in view of the well - established links between smoke , particulates , occupational risk , and cancer , such uncertainty was understandable on the basis of the equivocal nature of the emerging 9 / 11 data . 
 a study of mortality in survivors published in the lancet in 2011 , showed no excess ; in fact , it showed a de cit of mortality possibly attributable to the higher levels of tness among emergency workers . 
in a second article , also in the lancet in 2011 , rachel zeig - owens and colleagues looked speci cally at early cancer occurrence , and these data were again di cult to interpret . 
the standardised incident rate ( sir ) ratio for all cancers combined was 121 for re ghters deployed to the world trade center between sept 11 , 2001 , and july 25 , 2002 , indicating the possibility of an occupational hazard and higher than expected number of cancers , but the con dence intervals did not reach signi cance , and for individual malignancies ( eg , lung cancer ) there was no signi cant di erence , suggesting it was too soon to detect cancers associated with exposure to toxins . 
 long - term continued monitoring and research will be essential to establish the full extent of any associations . the analytical methods used in the cancer outcomes study also contributed to the confounding in the conclusions . 
however , for re ghters , an occupational health risk is already wellestablished , plus the nature of the job involves shift work and tends to attract tter and healthier people than in the normal population , which in turn modi es the risk of disease . 
thus , comparing cancer incidence in re ghters with that in the general population does not answer the very speci c question of whether deployment to the twin towers in the aftermath of the terrorist attacks added additional risk to their already underlying occupational risk . 
to answer this question , the denominator in the sir calculation needed to be the expected number of cancers among re ghters in major metropolitan cities in the usa . the slaughter of innocent people in the terrorist attacks in new york in 2001 has undeniably had a direct and profound e ect on the lives of many people : families , rst responders , volunteers , survivors , and manhattan residents . 
irrespective of the scienti c debate surrounding the robustness of the data linking cancer incidence to the world trade center devastation , su cient evidence exists from other settings to conclude that exposure to harmful chemicals and inhalation of noxious fumes and particles is not healthy , and on the precautionary principle alone , it is only right that all people directly a ected by 9 / 11 should be a orded free health care . 
to quote john feal , a campaigner for the treatment of 9 / 11 survivors : we dont need a phd to tell us that 9 / 11 and its aftermath cause cancer . 
 it is often said , the rst role of any government is to protect the safety of its peopleproviding free health care is a just and compassionate response irrespective of the data thus far . 
 the lancet oncology vol 13 october 2012 corrections correction to lancet oncol 2012 ; 13 : 983 , 986 correction to lancet oncol 2012 ; 13 : 1028 correction to lancet oncol 2012 ; 13 : e468 fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 this correction has been made as of oct 29 , 2012 . randomised , chemorefractory jfw , van den smits mlj , nijsen holmium - 166 bosch maaj , et al . 
lancet oncol 2012 ; 13 : 102534in table 1 of this article , the total number of patients with ocular melanoma should have been six , as should the total number of patients with colorectal carcinoma . 
lancet oncol 2012 ; 13 : e468in this news item , the second and third sentences of the second paragraph should have read : median pfs was 94 months ( 95% ci 86167 ) in the combination group compared with 58 months ( 4674 ) in the dabrafenib monotherapy group ( hazard ratio 039 , 95% ci 025062 ; p < 0001 )  . 
with surgery , the outcome of treatment is more likely to be related to patient anatomy and surgical technique and less likely to be a ected by information exchange during the consent process . 
for example , a patient who develops insulin de ciency after undergoing surgery for pancreatic cancer can be counselled quite objectively that this risk is likely to manifest on the basis of the size of the tumour and location within the pancreas and is unlikely to be a ected by the act of disclosure of this risk to the patient before surgery . 
 for patients with cancer who undergo non - invasive treatments or are prescribed drugs associated with non - speci c side - e ects , the act of disclosure itself could a ect the possibility of side - e ect manifestation . 
 rather , in many clinical circumstances in which the potential for non - speci c side - e ects is high , such as in the non - invasive treatment of cancer , the act of information disclosure could be more accurately viewed as part of the riskbene t analysis , thus dependent on real - time discussion , and personalised to the patient . 
theor med bioeth 2011 ; 32 : 22943 . published online november 16 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70332 - 1 errata adams c , torode j , henshall s , cazap e , ryel al , grey n . 
lancet oncol 2011 ; 12 : 109192in this comment , the fourth sentence of the third paragraph should have read : who has committed to produce targets for its so - called best - buy interventions in time for the world health assembly in 2012 . 
these corrections have been made to the online version as of nov 25 , 2011 . 1182 vol 12 december 2011 corrections published online october 24 , 2012 s1470 - 2045 ( 12 ) 70471 - 0 correction to lancet oncol 2012 ; 13 : 107678 correction to lancet oncol 2012 ; 13 : 1065 saghir ns . 
 lancet oncol 2012 ; 13 : 106465the rst author of this comment should have been listed as ankit i mehta and his in the a liations section should have been aim . 
these corrections have been made to the online version as of nov 23 , 2012 . initials vol 13 december 2012 e520 corrections correction to lancet oncol 2012 ; 13 : 559 correction to lancet oncol 2012 ; 13 : 696 lancet oncology . 
 lancet oncol 2012 ; 13 : 559 the second sentence of the third paragraph of this editorial should read in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
pixantrone dimaleate versus other chemotherapeutic agents as a singleagent salvage treatment in patients with relapsed or refractory aggressive non - hodgkin lymphoma : a phase 3 , multicentre , open - label , randomised trial . 
this correction has been made to the online version as of june 29 , 2012 , and the printed article is correct . vol 13 july 2012 e285 editorial for more on the health - care bill see world report lancet 2010 ; 375 : 114950 supreme court asked to decide future of us health care the twists and turns of the journey of the new us health - care policy through the us legal system reached in september , its expected end destination when 2011 , the justice department asked the supreme court to review the governments health - care law . 
 the a ordable care act , signed into law on march 23 , 2010 , called for a number of changes that are focused around a central tenet mandating that most americans must be insured from 2014 , or face a tax penalty . 
however , an individual mandate is vehemently opposed by some , most notably the republican party , who argue it is unconstitutional , and the law has been repeatedly challenged ( but mainly upheld ) in the courts over the past 18 monthswith the requirement for individual insurance the main point of contention . 
and in a further twist , the 26 states that originally led the atlanta suit have also lodged an appeal in the supreme court claiming that without this individual mandate the health - care legislation will be unworkable . 
 the government is con dent that the mandate will not be struck from the law and argue that it does not exceed its powers of commerce but will save money by preventing cost - shiftingin which the costs of emergency treatment of uninsured individuals are covered by increases in the premiums of those with insurance . 
opponents say that enactment of the law will cost money , leading to raised taxes , and overburden health - care systems that will be unable to cope with the additional patients . 
certainly allowing more patients access to the system through insurance is only a rst step on the care pathway , with delivery of services an equally important , and perhaps the biggest , challenge for the reforms . 
 as a result of the subsequent community reaction and premium costs , questions remain about the obama administrations mandate on future insurance costs and on the capacity of the current health - care syste furthermore , businesses must also o er coverage under the reforms , with only those companies with fewer than 50 employees being exempt , and this has understandably sparked resistance within the business community . 
nevertheless , these uncertainties and squabbles aside , there are several notable and important aspects of the act , such as coverage for dependents up to 26 years of age and the removal of caps on insurance , that highlight why the legislation must not be overturned or gutted . 
previously insurers were able to deny this group coverage in a bid to increase their pro ts whereas the new law ensures temporary coverage for people with pre - existing conditions until the mandate is activated in 2014 . 
 however , does not all this legal wrangling and discussion of cost rather miss the point and fundamental philosophy behind the law ? who has not experienced a sudden , serious , and chronic illness in a family member or friend ? the law is trying to change a reactive health - care system to a proactive one , with improved access to care for all . 
surprisingly , no alternative proposals to replace obamas law have been suggested by detractors , with republicans simply calling for it to be repealed , despite many health experts calling the existing system broken . 
 so should universal health - care be a human right , and do those who oppose the law lack a moral compass , or is this a naive and rose - tinted view in the current nancial climate ? one thing is certaif the law is repealed , or the individual mandate is removedand if november , 2012 , sees a change of guard at the topa whole generation will rue a missed opportunity . 
the number of patients reporting no pain from bone metastases , as measured by the bpi , increased from 39 of 149 ( 26% ) before sbrt to 55 of 102 ( 54% ) 6 months after sbrt ( p < 00001 )  . 
bpi - reported pain reduction from baseline to 4 weeks after sbrt was clinically meaningful ( mean 34 [ sd 29 ] on the bpi pain - at - its - worst item at baseline , 21 [ 24 ] at 4 weeks ; e ect size 047 , p = 000076 )  . 
these improvements were accompanied by signi cant reduction in opioid use during the rst 6 months after sbrt ( 43 [ 289% ] of 149 patients with strong opioid use at baseline vs 20 [ 200% ] of 100 at 6 months ; p = 0011 )  . 
ordinal regression modelling showed that patients reported signi cant pain reduction according to the mdasi during the rst 6 months after sbrt ( p = 000003 ) , and signi cant reductions in a composite score of the six mdasi symptom interference with daily life items ( p = 00066 )  . 
 only a few instances of non - neurological grade 3 toxicities occurred : nausea ( one event ) , vomiting ( one ) , diarrhoea ( one ) , fatigue ( one ) , dysphagia ( one ) , neck pain ( one ) , and diaphoresis ( one ) ; pain associated with severe tongue oedema and trismus occurred twice ; and non - cardiac chest pain was reported three times . 
signi cant reductions in patient - reported pain and other symptoms were evident 6 months after sbrt , along with satisfactory progression - free survival and no late spinal cord toxicities . funding national cancer institute of the us national institutes of health . 
 introduction almost 40% of patients with cancer develop spinal metastases during the course of their disease.1 , 2 inadequately treated spinal metastases can lead to pain and neurological complications , including metastatic epidural spinal cord compression . 
as a result , patients might experience severe symptom burden and diminished health - related quality of life ( hrqol ) .35 palliative radiotherapy e ectively controls pain for patients with spinal metastases ; 4 however , higher - dose radiotherapy might be needed for durable tumour control and prevention of bony destruction of the spinal column , which results in spinal instability . 
the spinal cords sensitivity to radiation generally precludes high radiation doses to the spine or re - irradiation using conventional techniques.6 accordingly , new techniques have been developed to optimise radiation dose delivery to bone metastases while sparing the spinal cord . 
 stereotactic body radiotherapy ( sbrt ) , an emerging technique , uses image guidance to deliver high - dose radiation precisely , creating a steep dose gradient at the interface between spinal cord and tumour . 
this approach increases the therapeutic window by lowering the risk for spinal cord myelopathy.68 delivered in high doses and one to ve fractions , spinal sbrt is available on various platforms , some of which include ct imageguided stereotaxy . 
sbrt can be used in combination with or in lieu of surgery and allows patients to avoid possible perioperative risk factors , such as general anaesthesia , bleeding , infection , or hospitalisation . 
in a preliminary report of a prospective phase 12 trial of sbrt , we detailed the safety , e cacy , and patterns of failure for sbrt using results from a vol 13 april 2012 articles subset of patients ( n = 63 ) with spinal metastases who were followed for up to 50 months.2 in the present analysis of the entire patient cohort , we investigated the symptomreduction bene t of spinal sbrt during the rst 6 months post - treatment , and clinical bene t for up to 2 years . 
we hypothesised that , for patients with mech an ically stable spinal metastases , sbrt is a clinically e ective therapy for tumour control ( evidenced by radio graphic depiction of tumour progression ) and sympto matic improvement ( evidenced by patient - reported outcomes )  . 
 methods patients this phase 12 trial was approved by the institutional review board of the university of texas md anderson cancer center ( houston , tx , usa )  . 
 eligibility requirements included a diagnosis of cancer ( excluding multiple myeloma ) , a karnofsky performance status score of at least 40 , and an mri scan documenting spinal or paraspinal metastasis within 4 weeks of enrolment . 
acceptable indications included oligometastatic disease arising from a known primary tumour , failure of previous conventional external beam radiotherapy or surgery , residual tumour after surgery , medical inoperability , and refusal to undergo surgery . 
 patients with mechanically unstable spine or epidural spinal cord compression were excluded ; however , patients with previously documented spinal cord compression that had been decompressed and stabilised were eligible . 
 patients were excluded if they had a pacemaker , were unable to undergo mri , or had received systemic radiotherapy ( strontium 89 ) or cytotoxic chemotherapy within 30 days of enrolment , or spinal external beam radiotherapy within 3 months of enrolment . 
 procedures all patients underwent intensity - modulated , nearsimultaneous , ct - guided sbrt ( ct - linac system [ exact targeting system , varian medical systems , palo alto , ca , usa ] or trilogy treatment delivery systems with on - board imager cone beam ct [ varian medical systems ] ) using a bluebag bodyfix total body immobilisation system ( elekta , stockholm , sweden ) , consisting of a whole - body vacuum cushion , carbon bre base plate , and plastic xation sheet . 
patients received a total dose of 2730 gy , typically delivered in three fractions given every other day , with 10 - gy radiation volume received by the spinal cord limited to 001 c gross target volume encompassed the lesion as visualised on the pretreatment ct scan . 
the clinical target volume encompassed the gross target volume and surrounding vertebral body ( including superior and inferior endplates and any existing paraspinal component ) , along with all additional spinal structures deemed to be at risk for recurrence , such as the pedicle , lamina , and posterior elements . 
in patients with postsurgical metallic artifacts near the area of interest , intrathecal contrast injection with iohexol ( ge healthcare canada inc , mississauga , on , canada ) was done 3060 min before ct image acquisition to assist with accurate spinal cord delineation . 
we measured pain at metastatic sites treated with sbrt via the brief pain inventory ( bpi ) .9 the bpi assesses pain at present and pain at its worst , least , and on average in the past 24 h , on a 010 scale . 
the bpi and mdasi are well validated in patients with various types of cancer.9 , 10 the medical outcomes study 12 - item shortform health survey ( sf - 12 ) was administered as an hrqol measure.11 patient - reported symptoms were assessed in the clinic via the bpi , mdasi , and sf - 12 pre - sbrt ( baseline ) and at 3 months and 6 months post - sbrt ; assessments at 2 weeks , 4 weeks , and 2 months were completed by the patient at home and returned by post , with a reminder call from a study nurse . 
 mri scans of the region treated were done at 3 , 6 , 9 , 12 , 18 , and 24 months post - sbrt and then every 6 months thereafter , as standard care . 
 history , neurological exam results , and mccormick functional classi cation12 were obtained at baseline and at each follow - up visit ( during the same timepoints as patient - reported outcomes assessments )  . 
toxicity was graded by the patients treatment team according to the national cancer institute common toxicity criteria for adverse events , version 2.0.13 statisticsmean , median , sd , statistical analysis descriptive and proportionsare used to describe patient and clinical characteristics . 
to account for multiple comparisons in the symptom and hrqol outcomes , which required eight modellings , we adjusted the individual type i error to be 005 / 8 = 000625 to maintain a conservative family - wise error rate of 005 . using pain cutpoints established by serlin and colleagues , 14 we categorised ratings of the bpis pain - atits - worst item as no pain ( 0 ) , mild pain ( 14 ) , moderate pain ( 56 ) , and severe pain ( 710 )  . 
concordance between bpi and mdasi painat - its - worst ratings , both scored on a 010 scale in the past 24 h , was examined using paired t tests . 
e ect sizes were calculated to estimate the magnitude of change in bpi and mdasi ratings ( composite score for all patients ) between baseline and 4 weeks post - treatment.15 , 16 for patient - reported outcomes measures , e ect sizes are clinically meaningful at roughly one - half sd or higher , the level often used in distribution - based methods of determining meaningful di erences.17 lowess curves , 18 which represent a smoothed estimate of average mdasi symptom severity and interference as a function of time , were constructed from baseline to 6 months post - sbrt . 
 ordinal regression models19 and generalised linear mixed models were tted to examine symptom development for the ve most - severe mdasi symptoms and the symptom - interference component score from baseline to 6 months post - sbrt . 
independent variables included weeks from start of therapy , age , sex , tumour volume of spinal metastasis at baseline , type of primary cancer , disease progression status 6 months after sbrt based on radiographic ( spinal mri ) results , opioid use , and karnofsky performance status at baseline . progression - free survival ( pfs ) and overall survival curves from date of enrolment were generated using the kaplan - meier method . 
spinal mris were done for 142 of 149 patients ( 95% ) at the 6 - month follow - up . baseline characteristics ( n = 149 ) 564 ( 125 ) 580 ( 200880 ) karnofsky performance status number of lesions age in years mean ( sd ) median ( range ) male female 8090 none primary histology breast cancer colon cancer melanoma thyroid cancer renal cancer sarcoma other unknown sbrt site cervical thoracic lumbar sacral previous therapy to spinal site radiotherapy alone surgery alone radiotherapy and surgery non - small - cell lung cancer 77 ( 52% ) 72 ( 48% ) 8 ( 5% ) 108 ( 72% ) 30 ( 20% ) 3 ( 2% ) 40 ( 27% ) 22 ( 15% ) 39 ( 26% ) 48 ( 32% ) 15 ( 10% ) 6 ( 4% ) 15 ( 10% ) 4 ( 3% ) 14 ( 9% ) 47 ( 32% ) 17 ( 11% ) 28 ( 19% ) 3 ( 2% ) 28 ( 19% ) 66 ( 44% ) 51 ( 34% ) 4 ( 3% ) metastatic tumour volume in cm , median ( range ) 382 ( 163579 ) data are number of patients ( % ) unless otherwise stated . 
sbrt = stereotactic body radiotherapy . at the time of analysis , 40 of 149 patients ( 27% ) were still alive , with a median follow - up of 159 months ( range 10916 ; iqr 95303 ) and mean 209 months ( sd 171 )  . 
median overall survival was 23 months ( 95% ci 186272 ) post - sbrt , with 1 - year and 2 - year actuarial survival of 685% ( 601754 ) and 464% ( 378547 ) , respectively . 
tumour progression was seen in 41 of 149 patients ( 28% ) and occurred at a median of 13 months ( range < 1101 ) , based on mri scans . 
actuarial pfs based on mri scans at 6 months , 1 year , and 2 years post - sbrt was 861% ( 95% ci 794907 ) , 805% ( 729861 ) , and 724% ( 631797 ) , respectively . 
 * no signi cant di erences between bpi pain - at - its - worst mean scores and mdasi pain item mean scores ( paired t tests ) were found at any timepoint other than the 6 - month assessment ( p = 0022 )  . 
the number of patients for whom analgesia data were available di ered slightly from the number of patients who provided symptom data . table 2 : pain severity scores and opioid use over time , before and after sbrt pain - at - its - worst ratings , at baseline and post - sbrt assessments . 
 the proportion of patients reporting no spine pain on the bpi increased signi cantly between baseline and 4 weeks post - sbrt , from 39 of 149 ( 26% ) to 43 of 109 ( 39% ) ( p = 0038 )  . 
this improvement continued throughout the study , with 53 of 120 ( 44% ) reporting no pain at 3 months ( p = 0004 ) and 55 of 102 ( 54% ) reporting no pain at 6 months ( p < 00001 )  . 
further , a signi cant decrease in the percentage of patients with moderate - tosevere bpi spine pain ( rated 5 on the 010 scale ) was noted from baseline to 4 weeks ( p = 0003 ) , 2 months ( p < 00001 ) , and 6 months ( p = 0002 ) post - sbrt . we noted clinically meaningful reductions in mean mdasi pain ratings between baseline and 4 weeks posttreatment ( from 34 [ sd 31 ] at baseline to 21 [ 26 ] at 4 weeks on the mdasis 010 scale ; e ect size 047 )  . 
 di erences in mean pain severity ratings between the bpi ( metastatic bone pain ) and mdasi ( general pain ) were noted only for the 6 - month assessment ( p = 0022 ; table 2 )  . 
we noted signi cant reduction in opioid use from baseline to 3 months ( p = 0021 ) and baseline to 6 months ( p = 0011 ) post - sbrt ( table 2 )  . 
 during the 6 months of observation , the ve most severe mdasi symptoms were fatigue , pain , disturbed sleep , 398 vol 13 april 2012 articles fatigue pain disturbed sleep drowsiness distress general activity normal work walking ability enjoyment of life mood relations with other people drowsiness , and distress . 
the lowess curves in gure 2 show that symptom interference lessened over time . reduction table 3 gives p values from ordinal regression modelling of mdasi symptom severity and interference , and sf - 12 physical and mental health component scores , adjusted for independent variables . 
patients reported signi cant pain ( p = 000003 ) 6 months after sbrt , and signi cant reduction in disturbed sleep , drowsiness , sadness ( all p < 00001 ) , fatigue , distress , lack of appetite , nausea , and di culty remembering ( all p < 005 )  . 
ordinal regression modelling showed that a composite score of all six interference items decreased signi cantly at each successive assess ment during the 6 months after sbrt ( p = 00066 )  . 
 patients whose lesions were categorised as progressive at the 6 - month follow - up examination ( 19 of 149 ; 13% ) reported signi cantly more - severe mdasi pain ( p < 00001 ) , fatigue ( p = 001 ) , and drowsiness ( p = 000008 ) than did patients with stable or smaller lesions . 
patients who received opioids during the 6 months after sbrt reported more severe mdasi pain , fatigue ( both p < 00001 ) , disturbed sleep , distress , and drowsiness ( allp < 0001 ) than did patients not using opioids . 
grade 3 toxicities were nausea ( one event ) , vomiting ( one event ) , diarrhoea ( one event ) , fatigue ( one event ) , non - cardiac chest pain ( three events ) , dysphagia ( one event ) , neck pain ( one event ) , diaphoresis ( one event ) , and pain associated with severe tongue oedema and trismus ( two events )  . 
 discussion this study incorporated validated single - symptom ( bpi ) and multisymptom ( mdasi ) assessments to measure patient - reported outcomes for pain and other symptoms in patients with metastatic spine lesions who received sbrt . 
in accordance with our previous report documenting the safety , e ectiveness , and patterns of failure of spinal sbrt , 2 here we showed signi cant reductions in the severity of pain and consistent reductions in other patient - reported symptoms and symptom interference 6 months after spinal sbrt , along with satisfactory pfs and no late spinal cord toxicities . 
 signi cant at p < 000625 , after adjusting for multiple comparisons ( eight models )  . table 3 : signi cance of reduced score for patient - reported outcomes during the rst 6 months after sbrt , adjusted for independent variables panel : research in context systematic review in recent years , spinal stereotactic body radiation therapy ( sbrt ) has become an increasingly established technique for the management of spinal metastases ; however , when this phase 12 trial was designed and activated in 2002 , spinal sbrt literature was in its infancy , consisting of preliminary technical reports with sparse outcomes data . 
drawing on previous experience in symptom research , 25 , 26 we applied well - established symptom - assessment methods to analyse outcomes data acquired from our prospective cohort . interpretation the results of this study show that sbrt is an e ective primary or salvage treatment for mechanically stable spinal metastasis . 
signi cant reduction in patient - reported pain and other symptoms was evident 6 months after sbrt , along with satisfactory progression - free survival and no late spinal cord toxicities . 
for patients with evidence of tumour progression 6 months after sbrt , such progression was signi cantly associated with more severe pain , as expected , suggesting a true ( non - placebo ) palliative e ect for sbrt . 
 this trial provides prospective data that support the careful use of spinal sbrt in selected patients , since sbrt safely and reliably halts the progression of disease while reducing patient symptoms and improving functioning in daily life , as measured by validated methods . 
this study also highlights the importance of integrating patient - reported symptom assessments with clinical outcome evaluations to fully demonstrate the bene t of sbrt in patients with metastatic spinal disease . 
between baseline and 4 weeks post - sbrt , we observed medium , but clinically meaningful , e ect sizes for pain reduction as reported on both the bpi pain - at - its - worst and mdasi pain items , along with signi cant increase in the number of patients reporting complete pain relief as early as 4 weeks post - sbrt . 
signi cant improvement in bpi pain ratings and e ect size relative to pre - sbrt scores was even larger 6 months after treatment ( e ect size 064 , p < 00001 ) , when only two patients had tumour progression and high pain severity and were receiving opioid therapy . 
the e ectiveness of sbrt for tumour and pain control was further evidenced by a reduction over time in the use of strong opioids , astandard of care for managing severe pa patient - reported data from the bpi and the mdasi , which use the same 010 pain - severity rating scale and 24 - h recall period ( table 2 ) , did not di er signi cantly in this cohort of patients with advanced cancer . 
this result suggests that researchers can use either scale in clinical studies when pain at its worst is the outcome of interest , and the same rating is expected with either scale . 
 the present study shows that pain reduction and functional improvement can also be re ected in the reduction of associated symptoms , such as fatigue , distress , and disturbed sleep.21 using a sensitive multiplesymptom assessment method ( the mdasi ) with a highly selective but comprehensive set of symptom items , 22 , 23 we not only prospectively identi ed pain and other major symptoms in a cohort of patients who received spinal sbrt , but also showed how multiple symptoms improved over time after treatment . 
signi cant reductions in the severity of several 400 vol 13 april 2012 articles symptoms in addition to metastatic pain suggest that spinal sbrt produces minimum symptom burden and toxic e ects for patients with late - stage cancer . 
we did not nd a signi cant di erence between renal - cell carcinoma and other primary histologies on patient - reported severity of any mdasi symptom ( data not shown )  . fatigue was consistently the most severe symptom over time , possibly as a result of advanced disease and continuous use of opioids . 
although fatigue improved over the 6 months post - sbrt ( p = 0037 ) , the physical and mental health component scores of the sf - 12 remained more or less constant in follow - up . 
these results are consistent with those of degen and colleagues , 24 who reported signi cant pain reduction 4 weeks after spinal sbrt that was durable to 1 year , but no signi cant change in physical or mental well - being data from the sf - 12 . 
in the present study , lower baseline karnofsky performance status was signi cantly associated with higher total symp tom interference on the mdasi and worsening physical well - being as measured by the sf - 12 ( table 3 )  . 
 the e cacy and safety of sbrt we report in this study are supported by the structured schedule with de ned assessment intervals and follow - up serial spinal mris , which permitted close assessment of the procedure . 
in this study , sbrt did not lead to any radiation - related spinal cord myelopathy ; the numbness reported by some patients was probably caused by pre - sbrt chemotherapy . 
in the present study , 24 patients did not return their paper - and - pencil symptom assessment results by post at the 2 - week assessment timepoint ; nonetheless , most of these patients contributed symptom data at subsequent timepoints . 
however , it is well accepted that sbrt has a quanti able clinical e ect on tumour growth with an accompanying reduction in pain at the radiation site , as shown in our previous report in a subset of this cohort of patients with stage iv cancer.2 one strength of the present study is that multiple symptoms were assessed simultaneously and longitudinally for each patient and compared with baseline , with each patient serving as his or her own control . 
such a trial is currently ongoing with the radiation therapy oncology group 06 - 31 study . in reviewing patient records , we found that 16 patients were positive for adrenal metastasis and 12 were positive for brain metastasis at enrolment . 
for this reason , although the protocol designated data collection up to 24 months , we did not use patient - reported outcomes data beyond 6 months , after which the symptomreduction bene t from sbrt could be confounded by increased pain from rapid disease progression at or near the end of life in this cohort with very advanced cancer . 
 further study of this data is warranted to determine the entire pro le of pain and other symptoms , from beyond 6 months post - sbrt to near the time of death . 
 radiation the role of sbrt in treating mechanically stable spinal metastases without spinal cord compression is continuing to develop in an era in which new tech nologies and treatments are being highly scrutinised . 
nonetheless , the current study provides additional data that support the clinical bene t of sbrt for carefully selected patients and suggests that sbrt reliably halts the progression of disease , reduces patient symptoms , and leads to improved functioning in daily lifethus demonstrating both symptomatic and clinical bene t ( panel )  . 
this study also highlights the importance of integrating patient - reported symptom assessments with clinical outcome evaluations to fully demonstrate the bene t of sbrt in patients with metastatic spinal disease . 
 all other authors declare that they have no con icts of interest . acknowledgments the researchers from the department of symptom research are partially funded by a grant from the national cancer institute ( nci ) of the us national institutes of health ( nih )  . 
 vol 13 april 2012 articles us cancer care : should insurers really be in the driving seat ? a number of health insurers in the usa have indicated their intent to adopt standardised cancer - care pathways in an e ort to improve patient outcomes and drive down spiralling costs . 
unitedhealthcare , the largest health insurer in the usa , has launched a pilot programme in which physicians will be paid an upfront fee at the start of treatment , based on the expected cost of a standard treatment regimen for a patients speci c condition . 
 each medical group participating in the pilot will choose a standard chemotherapy regimen for each particular disease setting , with continuous review of results with participating oncology groups designed to identify best practices . 
unitedhealthcares senior vice - president for oncology , lee newcomer , stated : by paying medical oncologists for a patients total cycle of treatment , rather than the number of visits and amount of chemotherapy drugs given , this program promotes better , more patientcentric , evidence - based care , with no loss of revenue for the physician . 
other insurers are exploring di erent models ; highmark blue cross blue shield , for instance , is thought to be considering a model that incorporates local preferences into standardised pathways , and o ering several pathways for each cancer . 
other companies are looking at models that identify the single best treatment option based on available clinical evidence . adoption of standardised patient pathways potentially o ers a rapid means of cost reduction by eliminating unnecessary care ( thought to account for up to 30% of health - care spending ) and o - label drug use . 
the current fee - for - service payment schema , in which physicians are paid more for scale than e ectiveness and outcomes , incentives to perform unnecessary o ers perverse represents a nancial procedures , and potentially con ict of interest for some physicians . 
however , there is little clarity on the mechanisms by which standardised pathways will be adopted and revised , and given that insurance companies also have vested interests and are accountable to shareholders , are they best placed to be driving such e ciencies ? furthermore , adoption of standardised pathways suggests that treatment courses are certain , whereas in practice they are likely to evolve with the patients response to treatmenthow , for instance , will unpredictable supportive - care needs be covered , particularly in schemes that adopt an upfront payment system ? indeed , there may be value in health - care providers marking - up chemotherapy prices when the mark - up is speci cally used to subsidise other areas of patient care or medical education , rather than simply to line the pockets of stakeholders . 
will patients nd themselves faced with large increases in out - of - pocket expenses ? the potential loss of revenue to community oncology practices could also drive such operations out of business ; with an estimated 40% of people in rural areas living at least an hour from urban areas , patients could be forced to travel to distant hospitals , with the ensuing extra costs and inconvenience . 
 whilst standardisation of care in an e ort to improve patient outcomes is a laudable e ort , the range of options being explored by di erent providers still represents a great deal of variation in treatment regimens . 
at present , there seems to be little evidence to suggest that insurers standardised treatment protocols do actually reduce costs , and indeed do so without a ecting patient outcomes . 
and how will the standardised pathways incorporate cutting - edgeand often hugely expensivenew treatments ? as has been seen in the uk when the national institute for health and clinical excellence has denied access to drugs on the basis of minimal advances in e ectiveness versus huge costs , controversy will no doubt ensue when patients are denied access to treatments that they feel they are entitled to . 
 despite the patient protection and a ordable care act facing possible dilution as a result of republican gains in the house of representatives in the last midterm elections , e orts to open up greater equality for all patients , to improve access to the best treatments , and to drive down health - care costs are needed . 
but are insurance - led schemes really the best option ? the patientcentered outcomes research instituteproposed as part of health - care reformand possibly the national cancer institute may be ideally situated to do the comparative e ectiveness studies needed to identify regimens and treatment guidelines that o er the best results for all vested interests , and in so doing avoid a zipcode lottery of care . 
 the lancet oncology editorial for more on the nci and comparative e ectiveness research see leading edge lancet oncol 2010 ; 11 : 499 vol 12 january 2011 editorial trips , an international agreement on trade related aspects of intellectual property rights for more on australias stance on tobacco and plain packaging see news lancet oncol 2011 ; 12 : 427 for more on the marketing of anticancer campaigns in developing countries see editorial lancet 2011 ; 378 : 200 for more on the australian bill see parlinfo / download / legislation / bills / r4613_ rst / toc_ pdf / 11136b01 . pdf ; letype = application%2fpdf cigarettes and plain packaging : the battle lines are drawn on july 6 , 2011 , australia became the rst country to send a bill to their parliament on plain packaging for cigarettes . 
the legislation aims to reduce the number of current and new smokers by increasing the e ectiveness of the health warnings and also by reducing the appeal of the product . 
 the legislation has been referred to the trips council and the technical barriers to trade committee in the world trade organisation ( wto ) in an intellectual property rights battle , but rather than being headed - up by the tobacco companies , this move is spearheaded by low - income and middle - income countries . momentum from antismoking advocates to tackle the tobacco epidemic is gathering pace , and it needs to . 
 however , at a trips council meeting on june 7 , 2011 , the dominican republic , with support or sympathy from honduras , nicaragua , ukraine , the phillipines , zambia , mexico , cuba , and ecuador , said it had serious and grave concerns about the australian draft law in that it violated trademark law and would drive down the costs of cigarettes thereby increasing consumption and paving the way for counterfeiting . 
by contrast , new zealand , uruguay , and norway all supported the proposed law , and india said that studies have shown that plain packaging is an e ective antismoking strategy . 
whether the law is a violation of trademark law remains a contentious issue , because the brand name will remain , albeit in a standard typeface and size , with the packets covered in large health warnings . 
legal supporters told the lancet oncology that they were con dent the proposed law was fully compliant with wto obligations and hoped the case would provide an endorsement under international law of the importance of the who framework convention on tobacco control . 
 that the dominican republic , and others , should align themselves with the tobacco industrys stance in what is clearly a corporate e ort to save industry pro ts might seem strange , but the tobacco industry is thought to be important economically for many of these countries in terms of tax revenue and jobs . 
intriguingly , in an echo of thoughts put to wto by the dominican republic , the industry has also suggested that plain packaging will lead to an increase in the australian counterfeit market . 
but this is a separate issue to helping smokers quit or preventing new smokers taking up the habit , and should not deter the australian government from making every e ort to break the addictive cycle that smokers endure . 
 other defensive strategies by the tobacco industry include advertising campaigns to win over the australian public with spoof sketches of popular television programmes and the labelling of australia as a nanny state . 
phillip morris asia has also made a peremptory strike by ling notice of a legal claim from the australian government citing a violation of a previous investment treaty between hong kong and australia , an odd strategy given any losses are currently unknown . 
furthermore , contrary to this claim , the tobacco industry has suggested there is no evidence to support the e ectiveness of plain packaging as a strategy to reduce smoking ; experts believe plain packets can break the a liation smokers have with a particular brand helping them to quit and can also prevent teenagers from becoming smokers . 
 the australian tobacco market is comparatively small , representing only a$998 billion in 2009 , but much e ort is being expended to stop this law because it will set a precedent with canada , the uk , and new zealand all predicted to follow australias lead . 
this correction has been made to the online version as of may 28 , 2012 , and the printed article is correct . vol 13 june 2012 e231 articles sensitivity of transvaginal ultrasound screening for endometrial cancer in postmenopausal women : a case - control study within the ukctocs cohort ian jacobs , aleksandra gentry - maharaj , matthew burnell , ranjit manchanda , naveena singh , aarti sharma , andy ryan , mourad w seif , nazar n amso , gillian turner , carol brunell , gwendolen fletcher , rani rangar , kathy ford , keith godfrey , alberto lopes , david oram , jonathan herod , karin williamson , ian scott , howard jenkins , tim mould , robert woolas , john murdoch , stephen dobbs , simon leeson , derek cruickshank , steven j skates , lesley fallow eld , mahesh parmar , stuart campbell , usha menon summary background the increase in the worldwide incidence of endometrial cancer relates to rising obesity , falling fertility , and the ageing of the population . 
we report the performance of tvs screening in a large cohort . methods we did a nested case - control study of postmenopausal women who underwent tvs in the united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) following recruitment between april 17 , 2001 , and sept 29 , 2005 . 
 our study is registered with clinicaltrials.gov , number nct00058032 , and with the international standard randomised controlled trial register , number isrctn22488978 . findings 48 230 women underwent tvs in the ukctocs prevalence screen . 
9078 women were ineligible because they had undergone a hysterectomy and 2271 because their endometrial thickness had not been recorded ; however , 157 of these women had an endometrial abnormality on tvs and were included in the analysis . 
the optimum endometrial thickness cuto for endometrial cancer or aeh was 515 mm , with sensitivity of 805% ( 95% ci 727868 ) and speci city of 862% ( 858866 )  . 
sensitivity and speci city at a 5 mm or greater cuto were 805% ( 727868 ) and 857% ( 854862 ) ; for women with a 5 mm or greater cuto plus endometrial abnormalities , the sensitivity and speci city were 853% ( 782908 ) and 804% ( 800808 ) , respectively . 
when our analysis was restricted to the 96 women with endometrial cancer or aeh who reported no symptoms of postmenopausal bleeding at the ukctocs scan before diagnosis and had an endometrial thickness measurement available , a cuto of 5 mm achieved a sensitivity of 771% ( 678843 ) and speci city of 858% ( 857859 )  . 
the logistic regression model identi ed 25% of the population as at high risk and 395% of endometrial cancer or aeh cases were identi ed within this high risk group . 
in this high - risk population , a cuto at 675 mm achieved sensitivity of 843% ( 714930 ) and speci city of 899% ( 893905 )  . interpretation our ndings show that tvs screening for endometrial cancer has good sensitivity in postmenopausal women . 
 additional factors are mortality greater than 30% within 10 years of diagnosis10 and a proven link between stage and survival raising the possibility of a mortality bene t from earlier detection.10 of note , stage for stage , survival rates for endometrial cancer are similar to ovarian cancera cancer for which large - scale screening trials are underway.11 , 12 to assess the endometrium in symptomatic women are tvs and endometrial sampling . 
other studies1416 have included smaller populations , making the to assess sensitivity of screening , or to achieve con dent estimates of speci city or positive predictive value . techniques commonly used impossible the the opportunity to study the performance of tvs in a large cohort of postmenopausal women was provided by data from the united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) .12 , 17 ukctocs is a prospective trial of ovarian cancer screening , one arm of which involved pelvic ultrasound during which endometrial thickness was measured and recorded . 
we report on the characteristics of endometrial cancer screening in postmenopausal women in the general population to inform on the potential of screening for endometrial cancer . methods participants we did a nested case - control study within the ukctocs cohort with ultrasound ndings recorded at yearly screening appointments as part of the ovarian cancer screening trial . 
the pre - identi ed scottish centres dropped out because of logistical issues ( lack of space , retirement of potential research leads , unwillingness of nhs trust management to commit to a 10 - year trial , involvement in other ovarian cancer screening trials ) .17 participants completed a recruitment questionnaire , which requested baseline data on lifestyle and reproductive factors , previous cancer history , and family history of breast or ovarian cancer.17 the focus of the recruitment questionnaire was on risk factors for ovarian cancer and the trial was not resourced to collect all variables related to endometrial cancer risk at the initial visit . 
 50 639 participants were randomly assigned to yearly screening with tvs ; 48 230 attended the initial prevalence screen and are included in our study . all women assigned to screening with tvs who had undergone the prevalence screen were included as cases or controls . 
cases were women with a con rmed diagnosis of endometrial cancer or atypical endometrial hyperplasia ( aeh ) , complex endometrial hyperplasia ( ceh ) , endometrial stromal sarcoma ( ess ) , or carcino sarcoma . 
we excluded from our study all women assigned to screening with tvs who had undergone hysterectomy before random assignment in ukctocs or who had no endometrial thickness measurement or endometrial abnormality on the relevant scan . 
 our study was covered by the ethical approval obtained for the main ukctocs ( mrec reference 00 / 8 / 34 , granted by north west mrec )  . recorded procedures tvs with kretz / medison sa9900 ( medison , seoul , south korea ) ultrasound machines was done by experienced ultrasonographers at the 13 trial centres in the uk . 
during the course of the trial , they completed an accreditation programme and attended yearly ultrasound days . the ultrasonographers were instructed to ask about and record symptoms of postmenopausal bleeding . 
we do not know how accurately postmenopausal bleeding was documented and there might have been a bias to better documentation in women who had an endometrial thickness above the level which prompted clinical referral ( > 5 mm ) according to current guidelines . 
in all women who reported that they had experienced any irregular bleeding to the sonographer , data were recorded on the ultrasound for during scanning , details of ovarian morphology and size were recorded . 
representative grey - scale images of each ovary and the uterus were archived at the coordinating centre.12 vol 12 january 2011 articles at tvs , endometrial thickness was measured at its thickest point from the anterior to the posterior in the sagittal plane of the uterus . 
callipers were placed perpendicular to the outer edge of the endometriuif there was uid in the endometrial cavity , the endometrial thickness was measured as above but with the inclusion of the cavity uid and the double endometrial stripe , then the uid diameter was subtracted at the same point . 
 for the purposes of our study , thickened , irregular , cystic , heterogeneous , distended endometrium ; uid in the endometrial cavity ; or polyp or other mass or lesion were included under the de nition of endometrial abnormality . abnormal , in clinical practice , asymptomatic women are not investigated . 
in the absence of any de nitive data at the start of the trial , a pragmatic decision to recommend referral of asymptomatic women with an endometrial thickness greater than 10 mm was agreed on the basis of extensive discussion and consultation with clinicians . 
we emphasise that there was no systematic protocol - driven intervention based on endometrial thickness . trial guidelines for the management of endometrial thickness stated that all women with thickness greater than 5 mm should be questioned about bleeding . 
in the this , uk national health service , postmenopausal bleeding prompts a 2 - week referral to assess for cancer , and all centres would have irrespective of followed measurements of endometrial thickness . 
data on any di erences between the centres are not yet available . all participants were followed up through a agging study with the nhs information centre for health and social care ( formerly o ce of national statistics ) in england and wales and via the central services agency and cancer registry in northern ireland as appropriate . 
 * includes those with personal history of breast cancer . table 1 : baseline characteristics of ukctocs participants who underwent the rst yearly scan vol 12 january 2011 articles women without ec or aeh n = 36 731 women with ec or aeh n = 133 relative risk ( 95% ci ) < 5 mm 30 664 ( 835% ) 5 to 10 mm 10 to 20 mm 20 mm mean ( sd ) 4878 ( 133% ) 1116 ( 30% ) 73 ( 02% ) 26 ( 195% ) 33 ( 248% ) 59 ( 444% ) 15 ( 113% ) median ( iqr ) 29 mm ( 2040 ) 110 mm ( 60145 ) 346 mm ( 259 ) 1153 mm ( 781 ) 793 ( 4771318 ) 5927 ( 37679336 ) 2012 ( 1106436063 ) data are n ( % ) unless otherwise indicated . 
aeh = atypical endometrial hyperplasia . table 2 : distribution of endometrial thickness measurements in women with or without endometrial cancer or atypical endometrial hyperplasia optimum = 515 mm optimum = 580 mm 1specicity 1specicity figure 1 : receiver operator curves for detection of endometrial cancer and atypical endometrial hyperplasia endometrial thickness measurements alone ( a ) and a combination of endometrial thickness measurements and endometrial abnormality ( b )  . 
data on the relevant variables for the ultrasound group were then inserted into the derived high - risk model and a prior risk probability of endometrial cancer was calculated solely on the basis of epidemiological data . 
these groups were based on the cuto s of the ordered prior risk probabilities : the highest risk ( rst ) quartile , the second quartile , the third quartile , and those at lowest risk ( fourth quartile )  . 
 relative risks ( rrs ) were used because the prevalence of endometrial cancer was virtually unchanged from the prevalence of endometrial cancer in the trial population for those without hysterectomy . ovarian volume was assessed as another variable to identify women at higher risk of endometrial cancer or aeh by comparing measurements of those who developed endometrial cancer or aeh and those who had not . the relative risk of endometrial cancer or aeh in women with thickness measurements of 5 mm or greater or 10 mm or greater were calculated to show the endometrial thickness cuto s suggested by the ukctocs guidelines . 
our study is registered with clinicaltrials.gov , number nct00058032 , and with the international standard randomised controlled trial register , number isrctn22488978 . follow - up , copies of operative notes , histopathology reports , cytology reports , discharge summaries , multidisciplinary team meeting notes , and other correspondence were obtained . 
the nal diagnosiswhich included the primary site , stage , and grade of any cancerwas made on review of the medical notes by an independent gynaecological oncologist ( rm )  . our primary outcome measure was endometrial cancer and aeh . 
aeh was included because 40% of cases of aeh might have concurrent ec , 18 there is limited concordance between pathologists on the diagnosis of aeh or endometrial cancer , 19 and aeh is a precancerous state with greater than 25% of patients progressing to endometrial cancer ( estimates range from 25% to 82% ) .2025 ess , carcinosarcoma , and ceh were also analysed separately . statistical analysis the distribution of endometrial thickness was compared in women who did and did not develop endometrial cancer or aeh . 
these data were used to construct a receiver operator characteristic ( roc ) curve to assess the speci city and sensitivity of various thickness cuto s for detecting endometrial cancer or aeh . 
a multivariate logistic - regression analysis was done that combined thickness with the baseline characteristics of the study participants to develop an algorithm incorporating epidemiological variables that would identify a high - risk group who might bene t from a targeted approach to screening . 
further roc curves were constructed to assess the speci city and sensitivity of various endometrial thickness cuto s for detecting endometrial cancer or aeh in the di erent risk groups . further analyses assessed the sensitivity and speci city pro le of endometrial thickness for the detection of endometrial cancers , either alone or combined with ceh , ess , or carcinosarcoma , with a scan done within a year of diagnosis . 
since systematic protocol - driven intervention based on endometrial thickness , we did not analyse the data by stage of endometrial cancer . to explore the possibility of re ning screening in a higher - risk group , the baseline characteristics recorded at recruitment for women diagnosed with endometrial cancer in the control and multimodal groups of the trial were modelled as epidemiological risk factors for endometrial cancer with forward stepwise logistic regression . 
these factors were weight ; age at menarche ; use of the oral contraceptive pill ; personal history of breast , ovarian , lung , bowel , or other cancer ; age at scan ; and any pregnancy of longer than 6 months vol 12 january 2011 articles role of the funding source the sponsor of the study and the funding sources had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
ag - m , mb , rm , ar , and um also had access to the raw data . results table 1 shows the baseline characteristics of the women with and without endometrial cancer or aeh . 
the inclusion criteria and details of the ukctocs trial have been described in detail elsewhere.12 , 17 50 639 study participants were randomly assigned to the ultrasound arm of ukctocs . 
the resulting group of 37 038 women were included in our study ( web appendix pp 56 )  . absence of endometrial median follow - up from the scan to cancer registration ( iqr 405595 )  . 
since update was 511 years information on cancers can take up to 3 years to be recorded on the national cancer registries , we explored other sources of follow - up data in detail in the 985 women for whom the time from scan to cancer registry followup on feb 9 , 2009 , was less than 3 years . 
in this cohort , we had additional con rmation of endometrial cancer status in 849 women because they had attended further screening and in 66 of the remaining women through returned follow - up questionnaires . 
in 70 of 37 038 women , the only source of information on endometrial cancer status was cancer registry follow - up of less than 3 years from the date of scan . [ 2% ] , three mixed subtype the cohort of 37 038 women includes 125 women who developed endometrial cancer after random assignment ( 100 endometrioid [ 80% ] , six papillary serous [ 5% ] , two clear cell [ 2% ] , one mucoid [ 1% ] , and 13 endometrial carcinoma without speci cation of histological subtype [ 10% ] ) , six with ess , six with carcinosarcomas or mixed mllerian tumours , 11 with aeh , and two with ceh . 
ess = endometrial stromal sarcoma . table 3 : performance characteristics of endometrial thickness as a screening tool for endometrial cancer with and without endometrial abnormality vol 12 january 2011 articles developed endometrial cancer after random assignment were stage 1 , 11 were stage 2 , nine were stage 3 , and one was stage 4 . 
overall , 112 of the 136 women with endometrial cancer or aeh were asymptomatic and 24 were symptomatic at the last ukctocs scan before diagnosis ( of 99 women with endometrial cancer or aeh who reported no postmenopausal bleeding , 96 had endometrial thickness measurements available )  . the remainder of the cohort is 36 888 controls , who are women without a diagnosis of endometrial cancer or aeh within 1 year of their last ukctocs scan . 
the control group includes six women who had either a leiomyosarcoma or breast cancer that was metastatic to the endometrium and 23 women who had endometrial cancer or aeh diagnosed more than 1 year after the last ukctocs scan . 
the 5% missing data rate is in keeping with what was anticipated for a study of this type and size . weight , age , and personal history of cancer were associated with an increased risk of endometrial cancer or aeh , although oral contraceptive pill , age at menarche , and parity were associated with a decreased risk ( webappendix p 1 )  . table 2 shows the distribution of endometrial thickness measurements in the 36 731 women who did not have a diagnosis of endometrial cancer or aeh . 
most of the women had an endometrial thickness of less than 5 m in the 133 women with a diagnosis of endometrial cancer or aeh who had endometrial thickness recorded , 107 ( 81% ) had an endometrial thickness of 5 mm or greater . 
the optimum cuto for endometrial thickness was 515 mm with a rr of 252 ( 95% ci 165385 )  . the webappendix ( p 2 ) shows the distribution of endometrial thickness measurements according to the use of hormone replacement therapy ( hrt ) in the overall cohort . 
the median endometrial thickness in women in the whole cohort who did not use hrt was 27 mm ( iqr 20395 ) versus 36 mm ( 2551 ) in women that did and these results were similar in the subgroup of women without endometrial cancer or aeh ( p < 00001 )  . 
by contrast , the median thickness was 110 mm ( 59148 without hrt ; 70145 with hrt ) in women with endometrial cancer or aeh , irrespective of the use of hrt . 1406 women reported breast cancer diagnosis before entry into the trial . 
these women were more likely to have an endometrial thickness of 5 mm or greater to less than 10 mm ( rr 191 ; 95% ci 168218 ) , 10 mm or greater to less than 20 mm ( 450 ; 385525 ) , and 20 mm or greater ( 1101 ; 8041447 ) than women with no history of breast cancer ( webappendix , p 3 )  . 
of the women with no history of breast cancer , 29 757 ( 839% ) of 35 460 had an endometrial thickness of less than 5 mm compared with 940 ( 669% ) of 1406 women with history of breast cancerthe median endometrial thickness was 29 mm versus 36 mm ( p < 00001 ; webappendix p 3 )  . 
 a large proportion of this measurement in women with breast cancer was probably related to tamoxifen use , but treatment data were not systematically captured as part of the trial . we did an analysis of endometrial thickness by screening centre in the women who did not develop endometrial cancer . 
the median endometrial thickness was 29 mthe median thickness varied from 21 mm number % ( 95% ci ) number % ( 95% ci ) number % ( 95% ci ) positive for bleeding negative for bleeding 5 mm cuto > 5 mm 5 mm sensitivity speci city > 10 mm 10 mm sensitivity speci city positive predictive value negative predictive value 10 mm cuto positive predictive value negative predictive value overall 31 464 35 746 805% ( 727868 ) 857% ( 854862 ) 20% ( 1821 ) 999% ( 999999 ) 541% ( 453628 ) 972% ( 970974 ) 64% ( 5474 ) 998% ( 998999 ) 892% ( 769956 ) 422% ( 386440 ) 308% ( 266331 ) 931% ( 852972 ) 649% ( 510767 ) 773% ( 734808 ) 453% ( 357535 ) 884% ( 838923 ) 31 410 35 586 771% ( 678843 ) 858% ( 857859 ) 14% ( 1215 ) 999% ( 999100 ) 500% ( 403597 ) 972% ( 971973 ) 45% ( 3654 ) 999% ( 998999 ) table 4 : performance characteristics of endometrial thickness as a screening tool for endometrial cancer in women with and without postmenopausal bleeding vol 12 january 2011 articles optimum = 675 mm optimum = 485 mm optimum = 575 mm optimum = 465 mm 1specicity 1specicity figure 2 : receiver operator curve for endometrial thickness measurements for detection of endometrial cancer in the high - risk group first quartile ( a ) , second quartile ( b ) , third quartile ( c ) , and fourth quartile ( d )  . 
when dichotomised as endometrial thickness less than 5 mm and 5 mm or greater , the proportion of measurements greater than 5 mm per centre varied from 104% to 224% ( overall proportion 168% ; median centre proportion 166% , iqr 147198 )  . to assess the sensitivity and speci city pro le for detection of endometrial cancer or aeh , a roc curve was constructed with cuto points for endometrial thickness with or without data for endometrial abnormalities ( gure 1 , webappendix p 4 )  . 
our subgroup analyses that included endometrial cancer and aeh or a combination of endometrial cancer , aeh , ceh , and ess or carcinosarcoma showed similar levels of sensitivity and speci city . given the di erence noted in endometrial thickness distribution in users of hrt and non - users , the optimum cuto in hrt users was as expected higher ( 685 mm ) than non - users ( 455 mm ; table 3 )  . at the ukctocs scan , postmenopausal bleeding was recorded in 165 women ( 37 cases and 128 controls )  . 
table 4 shows the performance characteristics for women with and without postmenopausal bleeding . the relation between ovarian volume and endometrial cancer or aeh was assessed and no statistically signi cant correlation was identi ed ( p = 0956 ; data not shown )  . we explored the possibility of optimising approaches to endometrial cancer screening by incorporating epidemiological information provided in the recruitment questionnaire . 
logistic regression showed that decreased endometrial cancer or aeh risk was associated with the use of the oral contraceptive pill , age at menarche , and pregnancies longer than 6 months , while increased risk was associated with rising weight , increasing age , and personal history of breast and other cancer ( multivariate and univariate analyses are shown in webappendix p 1 )  . 
 on the basis of the logistic regression model , the population could be divided into quartiles with rrs for endometrial cancer compared with the entire population of 198 ( 139280 ) for the rst quartile , 107 ( 073158 ) for the second , 076 ( 049116 ) for the third , and 049 ( 030079 ) for the fourth ( table 5 )  . 
the population in the highest quartile of risk ( rst quartile ) included 395% of women with endometrial cancer or aeh ; in this population an optimum endometrial thickness cuto at 675 mm achieved a sensitivity of 843% and speci city of 899% ( gure 2 , table 5 )  . if endometrial we also assessed the number of further interventions that would be predicted thickness measurements were used as a screen for endometrial cancer or aeh ( table 6 )  . 
if the entire population were screened , an endometrial thickness cuto of 5 mm or greater would result in 58 women undergoing further investigation per case of endometrial cancer or aeh detected for the diagnosis of 805% ( 107 of 133 ) of cancers . 
 a cuto of 10 mm or greater , would lead to 17 women being investigated to detect each case of endometrial cancer ( 556% [ 74 of 133 cancers diagnosed ] )  . 
if the proportion of the population screened was reduced by the use of our logistic regression model to limit screening to the top quartile risk group , 22 women would have to undergo investigation per endometrial cancer detected for the detection of 43 ( 323% ) cases in the entire population . vol 12 january 2011 articles number of cases / controls proportion of cases included rr of ec ( 95% ci ) area under curve ( 95% ci ) > 5 mm et cuto > 10 mm et cuto optimum cuto first quartile second quartile third quartile fourth quartile 51 / 9015 395% 34 / 9081 264% 26 / 9104 202% 18 / 9115 140% 198 ( 139 280 ) 107 ( 073 158 ) 076 ( 049 116 ) 049 ( 030 079 ) 0902 ( 0848 0957 ) 0878 ( 0808 0948 ) 0744 ( 0623 0865 ) 0969 ( 0947 0991 ) sensitivity ( 95% ci ) speci city ( 95% ci ) sensitivity ( 95% ci ) speci city ( 95% ci ) cuto sensitivity ( 95% ci ) speci city ( 95% ci ) 0863 ( 0737 0943 ) 0794 ( 0621 0913 ) 0615 ( 0406 0798 ) 0944 ( 0727 0999 ) 7546 0837 ( 0829 0845 ) 7846 0864 ( 0857 0871 ) 7839 0861 ( 0854 0868 ) 7948 0872 ( 0865 0879 ) 0627 ( 0481 0759 ) 0471 ( 0298 0649 ) 0385 ( 0202 0594 ) 0667 ( 0410 0867 ) 8654 8863 8867 8914 0960 ( 0956 0964 ) 0976 ( 0973 0979 ) 0974 ( 0970 0977 ) 0978 ( 0975 0981 ) 485 mm 28 7574 675 mm 43 465 mm 17 575 mm 17 0843 ( 0714 0930 ) 0824 ( 0655 0932 ) 0654 ( 0443 0828 ) 0944 ( 0727 0999 ) 8104 0899 ( 0893 0905 ) 0834 ( 0826 0842 ) 7456 0819 ( 0811 0827 ) 8194 0899 ( 0893 0905 ) n = number . 
when we assessed this in our cohort , we found that for the left ovary , the use of the suggested cuto of 3 cm , the p value was 0063 and for the right ovary p was 0218 . discussion ultrasound imaging of the endometrium has long been thought a possible screening test for endometrial cancer . 
however , there has been a dearth of data about the performance of potential tests and the largest study involved fewer than 2000 women and only one endometrial cancer was diagnosed.13 the ukctocs protocol enabled us to assess the performance of tvs for endometrial screening cancer 37 038 postmenopausal women . 
 when the analysis was restricted to women who reported no symptoms of postmenopausal bleeding at the scan and had an endometrial thickness measurement available , a cuto of 5 mm achieved a sensitivity of 771% and speci city of 858% ( table 4 )  . 
although the role of population screening for endometrial cancer remains uncertain , the ndings are of immediate value in the management of increased endometrial thickness in postmenopausal women undergoing pelvic scans for reasons other than vaginal bleeding . our ndings con rm the strong correlation between tvs ndings and subsequent diagnosis of endometrial cancer , as shown by the rrs ( table 2 )  . 
 this correlation was shown by the levels of sensitivity et cut - o ( mm ) number of cases of ea / aeh with positive result proportion of ec cases detected number of women with positive result risk of ec / aeh relative risk of ec / aeh ( 95% ci ) number of investigations per case detected whole population screened whole population screened whole population screened whole population screened first quartile ( highest risk ) screened second quartile screened third quartile screened fourth quartile ( lowest risk ) screened > 675 > 485 > 465 > 575 10000% 8045% 5564% 1128% 3233% 2105% 1278% 1278% 36 864 6174 1263 1535 1665 036% 173% 586% 1705% 451% 182% 102% 181% 100 2047 ( 13393130 ) 3537 ( 25844950 ) 5315 ( 32118500 ) 4373 ( 20999032 ) * 2263 ( 9645319 ) * 838 ( 3821840 ) * 14588 ( 248186025 ) * * relative risk within the risk quartile . 
as expected , the optimum cuto in asymptomatic women of 445 mm is similar but lower than the 5 mm cuto reported for symptomatic women.26 of note , our report shows that 26 women ( 195% ) who developed endometrial cancer within a year of their scan on ukctocs had an endometrial thickness of less than 5 min a theoretical model , based on the estimate that 15% of endometrial cancers occur in women without vaginal bleeding , smith - bindman and colleagues27 calculated the risk of endometrial cancer to be 67% for an endometrial thickness greater than 11 mm.27 this ts satisfactorily with 59% risk of endometrial cancer in our cohort where 96 ( 722% ) of 133 women were asymptomatic at an endometrial cuto of 10 mm . although the data show that tvs can detect endometrial cancer before symptoms are detected in a high proportion of postmenopausal women , there are a range of issues that need to be addressed before population screening for endometrial cancer can be proposed . 
if we assume an incidence of 60 per 100 000 per year and 30% mortality at 5 - year follow - up , a randomised controlled trial would need 500 000 participants to document a 50% reduction in mortality . 
since a trial on this scale is almost certainly not feasible , decisions about whether or not to screen for endometrial cancer will have to be made on the basis of surrogate measures of e cacy . 
we explored the possibility of reducing the overall burden of screening by focusing on a group of the population identi ed as being at higher risk on the basis of epidemiological criteria . 
our logistic regression model that used epidemiological variables of the use of the oral contraceptive pill , age at menarche , number of pregnancies , weight , age , and history of cancer was able to separate the population into quartile groups at di erent levels of risk . 
 this would reduce the burden of screening to 25% of the population with detection of about 40% of the cases . the strengths of our study include the large size of our cohort , prospective data collection with standardised measurement of endometrial thickness as part of the trial protocol , systematic follow - up , and information on epidemiological variables . 
consistent with earlier reports of the correlation of endometrial thickness and hrt , 28 the median endometrial thickness in users of hrt in the control group was 36 mm versus 27 mm in non - users . 
this probably relates to the use of tamoxifen , which is known to be associated both with increased endometrial thickness ( range 49117 mm ) in postmenopausal women2934 and increased risk of endometrial cancer ( rates of 03% vs 006% in women on placebo ) .35 we were , however , unable to con rm a recently reported correlation between ovarian volume and the risk of endometrial cancer of aeh reported by the plco trialists.36 one of the limitations of our study was that endometrial cancer screening was not an interventional endpoint in the ukctocs . 
detailed data on the variety of procedures done was not collected , but this is unlikely to alter the performance characteristics of endometrial thickness . a further limitation of our study is the accuracy of the reports of postmenopausal bleeding . 
therefore , there might be bias in the recording of these data for women who had an endometrial thickness above the level that triggered clinical referral ( > 5 mm )  . there was a di erence in median endometrial thickness measurements in healthy women across the 13 centres . 
in addition to slight variations for measuring endometrial thickness in 36 731 individuals across 13 centres , it is also probably related to variations in the demographics such as body - mass index of patients between centres . 
it highlights the need to have training and quality assurance measures in place if ultrasound were to be used as a screen for endometrial cancer . the scanning techniques the cis around parameter estimates were wide because of low numbers of endometrial cancers despite the large overall number of participants . 
some key variables that could a ect risk of endometrial cancer , such as smoking , 38 diabetes , and hypertension , 39 could not be used in model building because the main focus of the recruitment questionnaire was on risk factors for ovarian cancer . 
variables were collected on follow - up and a greater percentage of women with endometrial cancer reported a history or diagnosis of diabetes ( nine [ 102% ] of 88 ) compared with those without endometrial vol 12 january 2011 articles panel : research in context systematic review a systematic review of ovarian cancer screening41 was published by the nhs centre for reviews and dissemination before submission of the grant proposal to the uk medical research council for united kingdom collaborative trial of ovarian cancer screening . 
no systematic review of endometrial cancer screening was done . a detailed review of published work of endometrial cancer screening in an asymptomatic population was done as part of our analysis . 
other studies1416 have included smaller populations making it impossible to assess the sensitivity of screening or to achieve con dent estimates of speci city or positive predictive value . interpretation our study provides to our knowledge the only large - scale data on the performance characteristics of tvs in endometrial cancer screening , and provides evidence that ultrasonography can detect endometrial cancer in asymptomatic women with 8090% sensitivity and similar levels of speci city . 
 clinicians faced with ultrasound data on endometrial thickness from scans done in various disorders aside from vaginal bleeding will now have data to inform their daily practice . the likely bene t of detection of endometrial cancer by ultrasound screening would be conjecture . 
we have limited ourselves to reporting and discussing the performance characteristics . the rising incidence of endometrial cancer and the di culty of doing a randomised controlled trial large enough to specify mortality as an endpoint , suggests that the decision to introduce screening for all or a subgroup of asymptomatic women will rest on surrogate criteria such as the performance characteristics described in our report and future studies of acceptability , health economics , and risk strati cation . 
we do not advocate population screening for endometrial cancer until further data are available from these studies . contributors ijj , agm , mb , sc , and um contributed to the study design , analysis and interpretation of the data , and drafting and revision of the report . 
um and ij has a nancial interest through ucl business and abcodia ltd in the third party exploitation of clinical trials biobanks , which have been developed through the research at ucl . 
all other authors declared no con icts of interest . acknowledgments the trial was core funded by the uk medical research council , cancer research uk , and the uk department of health with additional support from the eve appeal , special trustees of barts and the london , and special trustees of uclh . 
a substantial portion of this work was done at uclh / ucl within the womens health theme of the nihr cancer ( 1429 [ 50% ] of 28 801 ; data not shown )  . 
furthermore , although there was an association with weight , we could not con rm the link between the risk of endometrial cancer and body - mass index.40 a paucity of detailed information on type of hrt and duration of use at scan also reduced our ability to do further subanalyses . false - positive results on tvs screening for endometrial cancer will require a form of endometrial sampling that , although not a major procedure , will generate anxiety , inconvenience , and cost . 
there are of course complications as well as costs of hysteroscopy that would need to be assessed carefully in a risk - bene t analysis if screening for endometrial cancer with tvs was to be introduced . 
another important consideration for future studies of endometrial cancer screening is acceptability of the screening strategy . a cuto at 5 mm or greater would result in 58 diagnostic procedures for each case of endometrial cancer detected . 
we are exploring the possibility of further re ning risk strati cation by incorporating sex - steroid hormone pro ling . laparoscopy or whether ovarian cancer screening will save lives is currently unclear and whether the primary screen should be with tvs or a serum biomarker is debated . 
the extra cost of incorporating endometrial cancer screening within the scope of an ovarian cancer screening trial could be marginal and add bene t to the screening strategy if properly modelled . our report is to our knowledge the rst large - scale report of the performance characteristics of tvs in endometrial cancer screening ( panel )  . 
in particular , issues of early detection , morbidity , acceptability , and health economics of intervening on the basis of endometrial thickness will need to be the subject of future studies . 
we thank the women throughout the uk who are participating in the trial and to the entire medical , nursing , and administrative sta who work on the ukctocs . 21 kurman rj , kaminski pf , norris hj . 
the biologic signi cance of cytologic atypia corrections correction to lancet oncol 2011 ; 12 : 531 , 532 bonnefoi h , piccart m , bogaerts j , et al , on behalf of the eortc 10994 / big 1 - 00 study investigators . 
tp53 status for prediction of sensitivity to taxane versus non - taxane neoadjuvant chemotherapy in breast cancer ( eortc 10994 / big 1 - 00 ) : a randomised phase 3 trial . 
 lancet oncol 2011 ; 12 : 52739in this article , table 2 was incorrect and should have been as shown below . accordingly , the third paragraph of the results section should have read by february , 2010 , 675 primary had occurred , endpoint of which 420 ( 62% ) were distant recurrences ( table 2 )  . 
this correction has been made to the online version as of jan 28 , 2013 . events fec ( n = 361 ) * t - et ( n = 314 ) * progression while on neoadjuvant chemotherapy 56 ( 16% ) distant recurrence invasive locoregional recurrence invasive contralateral cancer death without previous report of progression 219 ( 61% ) 59 ( 16% ) 14 ( 4% ) 13 ( 4% ) progression treatment toxicity cancer ( non - breast ) cardiovascular other not known 49 ( 16% ) 201 ( 64% ) 42 ( 13% ) 13 ( 4% ) 9 ( 3% ) data are number ( % ) or number . 
deaths occurring during chemotherapy or within 30 days of chemotherapy completion and without disease relapse . table 2 : first events contributing to progression - free survival correction to lancet oncol 2013 ; 14 : 88 , 89 , 95 goss pe , smith ie , oshaughnessy j , et al , on behalf of the teach investigators . 
 lancet oncol 2013 ; 14 : 8896the second sentence of the methods in the summary should read women outpatients 33 countries with her2 - positive earlybreast cancer who had previously received chemotherapy but not trastuzumab were randomly from 405 centres adjuvant assigned ( 1 : 1 ) to receive daily lapatinib ( 1500 mg ) or daily placebo for 12 months , and the second sentence of the study design and participants section , should read participants were hospital outpatients at 405 centres in 33 countries worldwide . 
 the online version was corrected on jan 28 , 2013 . vol 14 february 2013 corrections published online october 24 , 2012 s1470 - 2045 ( 12 ) 70471 - 0 correction to lancet oncol 2012 ; 13 : 107678 correction to lancet oncol 2012 ; 13 : 1065 saghir ns . 
 lancet oncol 2012 ; 13 : 106465the rst author of this comment should have been listed as ankit i mehta and his in the a liations section should have been aim . 
these corrections have been made to the online version as of nov 23 , 2012 . initials vol 13 december 2012 e520 corrections published online november 23 , 2012 s1470 - 2045 ( 12 ) 70533 - 8 correction to lancet oncol 2012 ; 13 : 549 , 554 from prostate hormone therapy alone james nd , sydes mr , mason md , et al , for the stampede investigators . 
lancet oncol 2012 ; 13 : 54958in the summary of this article , the second sentence of the findings section should read : at the preplanned analysis of the second intermediate activity stage , with 305 ffs events ( 209 in arm a , 96 in arm d ) , there was no evidence of an advantage for hormone therapy plus celecoxib over hormone therapy alone : hr 094 ( 95% ci 074120 )  . 
the rst sentence of the fth paragraph of the results should read at this second intermediate analysis , celecoxib showed insu cient evidence of activity , in terms of ffs , for continuation of accrual to this comparison : hr 094 from adjusted cox model ( 75% ci upper limit 103 ; 95% ci 074120 ; gure 3 )  . 
overall e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against grade 3 or greater cervical intraepithelial neoplasia : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 8999in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
cross - protective e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against cervical infection and precancer caused by non - vaccine oncogenic hpv types : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 10010in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
lancet oncol 2012 ; 13 : 1012in this comment ( published online nov 9 , 2011 ) , the last sentence of the sixth paragraph incorrectly lists hpv - 35 as one of the oncogenic hpv types covered by the new nine - type gardasil vaccine ; the list should include hpv - 45 instead . 
this correction has been made to the online version as of jan 3 , 2012 . vol 13 january 2012 corrections correction to lancet oncol 2012 ; 13 : 983 , 986 correction to lancet oncol 2012 ; 13 : 1028 correction to lancet oncol 2012 ; 13 : e468 fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 this correction has been made as of oct 29 , 2012 . randomised , chemorefractory jfw , van den smits mlj , nijsen holmium - 166 bosch maaj , et al . 
lancet oncol 2012 ; 13 : 102534in table 1 of this article , the total number of patients with ocular melanoma should have been six , as should the total number of patients with colorectal carcinoma . 
lancet oncol 2012 ; 13 : e468in this news item , the second and third sentences of the second paragraph should have read : median pfs was 94 months ( 95% ci 86167 ) in the combination group compared with 58 months ( 4674 ) in the dabrafenib monotherapy group ( hazard ratio 039 , 95% ci 025062 ; p < 0001 )  . 
the legislation aims to reduce the number of current and new smokers by increasing the e ectiveness of the health warnings and also by reducing the appeal of the product . 
 the legislation has been referred to the trips council and the technical barriers to trade committee in the world trade organisation ( wto ) in an intellectual property rights battle , but rather than being headed - up by the tobacco companies , this move is spearheaded by low - income and middle - income countries . momentum from antismoking advocates to tackle the tobacco epidemic is gathering pace , and it needs to . 
 however , at a trips council meeting on june 7 , 2011 , the dominican republic , with support or sympathy from honduras , nicaragua , ukraine , the phillipines , zambia , mexico , cuba , and ecuador , said it had serious and grave concerns about the australian draft law in that it violated trademark law and would drive down the costs of cigarettes thereby increasing consumption and paving the way for counterfeiting . 
by contrast , new zealand , uruguay , and norway all supported the proposed law , and india said that studies have shown that plain packaging is an e ective antismoking strategy . 
whether the law is a violation of trademark law remains a contentious issue , because the brand name will remain , albeit in a standard typeface and size , with the packets covered in large health warnings . 
legal supporters told the lancet oncology that they were con dent the proposed law was fully compliant with wto obligations and hoped the case would provide an endorsement under international law of the importance of the who framework convention on tobacco control . 
 that the dominican republic , and others , should align themselves with the tobacco industrys stance in what is clearly a corporate e ort to save industry pro ts might seem strange , but the tobacco industry is thought to be important economically for many of these countries in terms of tax revenue and jobs . 
intriguingly , in an echo of thoughts put to wto by the dominican republic , the industry has also suggested that plain packaging will lead to an increase in the australian counterfeit market . 
but this is a separate issue to helping smokers quit or preventing new smokers taking up the habit , and should not deter the australian government from making every e ort to break the addictive cycle that smokers endure . 
 other defensive strategies by the tobacco industry include advertising campaigns to win over the australian public with spoof sketches of popular television programmes and the labelling of australia as a nanny state . 
phillip morris asia has also made a peremptory strike by ling notice of a legal claim from the australian government citing a violation of a previous investment treaty between hong kong and australia , an odd strategy given any losses are currently unknown . 
furthermore , contrary to this claim , the tobacco industry has suggested there is no evidence to support the e ectiveness of plain packaging as a strategy to reduce smoking ; experts believe plain packets can break the a liation smokers have with a particular brand helping them to quit and can also prevent teenagers from becoming smokers . 
 the australian tobacco market is comparatively small , representing only a$998 billion in 2009 , but much e ort is being expended to stop this law because it will set a precedent with canada , the uk , and new zealand all predicted to follow australias lead . 
 the lancet oncology vol 12 august 2011 comment information about non - speci c side - e ects from providers and written material , such as those on consent forms and labels , without consideration of the nocebo e ect . for this model to work on behalf of patients , the risks and bene ts of a speci c treatment have to be completely unrelated to the act of information disclosure to the patient.8 although this notion might be true for some treatments , it is not uniformly applicable . 
with surgery , the outcome of treatment is more likely to be related to patient anatomy and surgical technique and less likely to be a ected by information exchange during the consent process . 
for example , a patient who develops insulin de ciency after undergoing surgery for pancreatic cancer can be counselled quite objectively that this risk is likely to manifest on the basis of the size of the tumour and location within the pancreas and is unlikely to be a ected by the act of disclosure of this risk to the patient before surgery . 
 for patients with cancer who undergo non - invasive treatments or are prescribed drugs associated with non - speci c side - e ects , the act of disclosure itself could a ect the possibility of side - e ect manifestation . 
 rather , in many clinical circumstances in which the potential for non - speci c side - e ects is high , such as in the non - invasive treatment of cancer , the act of information disclosure could be more accurately viewed as part of the riskbene t analysis , thus dependent on real - time discussion , and personalised to the patient . 
theor med bioeth 2011 ; 32 : 22943 . published online november 16 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70332 - 1 errata adams c , torode j , henshall s , cazap e , ryel al , grey n . 
lancet oncol 2011 ; 12 : 109192in this comment , the fourth sentence of the third paragraph should have read : who has committed to produce targets for its so - called best - buy interventions in time for the world health assembly in 2012 . 
these corrections have been made to the online version as of nov 25 , 2011 . 1182 vol 12 december 2011 comment if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology as piration of mediastinal and hilar lymph nodes should be used to assess preoperative lung cancer status in countries where tuberculosis is endemic.10 finally , hiv infection is associated with increased lung cancer cases . 
can tuberculosis further increase this risk ? in a study11 that linked aids registry surveillance data for 322 675 patients with aids diagnosed between 1977 and 2002 , with cancer registries in 11 us regions , lung cancer risk over 10 years was unrelated to tuberculosis . 
 tuberculosis awareness in patients with cancer needs to be reinforced , especially in low - burden developed countries , and lung cancer awareness in patients with previous or suspected tuberculosis should be urgently strengthened in developing countries to increase the low numbers of potentially resectable tumours . * sandro vento , massimiliano lanzafame department of internal medicine , faculty of medicine and health sciences , university of botswana , gaborone , botswana ( sv ) ; and infectious diseases unit , gb rossi university hospital , verona , italy ( ml ) ventosandro@yahoo.it we declare that we have no con icts of interest . yu yh , liao cc , hsu wh , et al . 
lancet oncol 2011 ; 12 : 37786in this article ( april ) , on page 380 , the number of women with luminal a breast cancer tested for the kras variant should have been 478 in gure 2a and the percentage of premenopausal women diagnosed with luminal a breast cancer should have been 151% in gure 2b . 
lancet oncol 2011 ; 12 : 41516on page 415 , in the second column , it was stated that 17 variants showed moderate to strong evidence of a true association and were therefore candidates for clinical tests , this should have said 14 variants . 
although great progress has been made against many types of cancer ( as highlighted by recent mortality data from the american cancer society ) , treatment of others has shown little change in the past few decades . 
two phase 3 clinical trials published in december , 2011 , in the new england journal of medicine ( gog018 and icon7 ) showed that women with newly diagnosed advanced ovarian cancer given concomitant bevacizumab with a paclitaxel and carboplatin chemotherapy regimen following surgery , and then maintenance bevacizumab , had signi cantly longer progression - free survival compared with those who received chemotherapy alone . 
5 - year survival is just 30% , a figure that has not changed for the past 30 yearsthis contrasts with breast cancer , in which 5 - year survival has improved from 50% to 80% over the same period . 
for example , in this issue of the lancet oncology , gotlieb and colleagues show that aflibercept , a vegf - trap , can prolong time between repeat paracentesis to drain malignant ascites associated with the disease , compared with placebo . although these latest reports show promise for the treatment of ovarian cancer , a major hurdle towards reducing mortality continues to be the late presentation of the disease . 
less than a third of women are diagnosed with early - stage disease , for which survival at 5 years is 90%indicating that early diagnosis and treatment is central to reducing mortality . 
ovarian cancer has often been called a silent killer because of its subtle and nonspeci c symptoms ; however , it is perhaps not so much that the disease is silent , but rather that it is not being heard because of a lack of understanding of the biology of the disease . 
 in 2009 , the target ovarian cancer charity published the rst results of its path nder study , which surveyed women , family doctors , and specialists to identify gaps in the knowledge and treatment of those with ovarian cancer . 
a key nding was that many factors can lead to delays in diagnosis , from women not recognising symptoms and delaying an initial consultation with a doctor , through to misdiagnosis . 
since then , an online tool has been developed by researchers from the university of nottingham in the uk as a diagnostic aid that takes into account risk factors including age and family history , and the presence of persistent symptoms , such as abdominal swelling and loss of appetite . 
published in the british medical journal on jan 4 , 2012 , a study into the e ectiveness of the tool showed that the 10% of women with the highest predicted risks according to the algorithm had 63% of all ovarian cancers diagnosed over the next 2 years . 
this project enters its next phase later this year , with an increased number of specialist clinics being made available to women . after many years of disappointing results for women with ovarian cancer , on the eve of world cancer day on feb 4 , 2012 , there is at long last an opportunity to celebrate some improvements made in the diagnosis and treatment of this devastating cancer . 
world cancer day will undoubtedly be dominated by the more prominent cancer types , but it is imperative that continued e orts are made in rarer cancers and that these diseases are not ophaned by a disproportionate focus on easy wins . 
 the lancet oncology vol 13 february 2012 shortages of cancer drugs in the usa on feb 7 , 2011 , senators amy klobuchar and robert casey introduced the preserving access to life saving medications act . 
this new legislation means that manufacturers of prescription drugs will be required to notify the us food and drug administration ( fda ) when a drug is going to be discontinued or if any di culties arise that might a ect manufacture of a drug . 
 drug shortages in the usa have steadily increased in recent years , with 211 new shortages identi ed in 2010 compared with 166 in 2009 , 149 in 2008 , 129 in 2007 , and 70 in 2006 . 
furthermore , shortages are not just restricted to drugs , but also extend to medical supplieseg , technetium - 99m was in short supply after a nuclear reactor in canada , where it was produced , was temporarily closed down for repairs . 
so where does this leave health - care services , in particular cancer treatment , in the usa , and will changes in the legislation introduced earlier this year help ? 150 drugs are judged to be medically necessary . 
substitution of one drug with another might result in worse side - e ects or reduced e cacy , violate the protocol of a clinical trial , or lead to a shortage of the alternative drug . 
asco suggested substitution of leucovorin with levofolinate , which is much more expensive and is only approved by the fda for use as a rescue drug after administration of high - dose methotrexate in patients with osteosarcoma . 
 levofolinate irinotecan and uorouracil seems e ective in patients with metastatic colorectal cancer , but it is unclear whether addition in combination with of this agent to other chemotherapy regimens would replicate the responses expected of leucovorin ; thus there is a risk attached to this strategy . since one or only a few manufacturers are likely to be producing a particular generic drug , shortages are perhaps inevitable . 
the production of sterile injectable drugs takes a long time and is a complex process ; therefore , if one manufacturer is unable to produce a drug for whatever reason , other manufacturers might not be able , or willing , to ramp - up production . 
the reasons for drug shortages include increased demand ; di culties in obtaining , or discontinuations in , the bulk materials ; halted production in response to the fdas enforcement of good manufacturing practices ; change in formulation ; discontinuation because of insu cient nancial returns ; patent expiration ; mergers leading to discontinuation of one of two similar products ; and antitrust laws that prevent manufacturers from sharing information . because of concern about drug shortages in the usa , a drug shortages summit was convened on nov 5 , 2010 , in bethesda , md , usa , by the american society of health - system pharmacists ( ashp ) , american society of anesthesiologists , asco , and the institute for safe medication practices . 
before the klobucharcasey bill , manufacturers were only encouraged , but not required , to inform the fda of any di culties in the supply chathere is a risk that healthcare providers , after nding out about an impending drug shortage , might now decide to stockpile , which would only exacerbate the proble whether the fda will be able to enforce alternative or extended production remains to be seen . drug shortages mean that patients are not given the best treatment or that their treatment might be delayed . 
legally , non - fda - approved drugs ( including foreign - made versions of usa - approved drugs ) cannot be imported into the usa , and perhaps a solution would be either to relax some of the laws ( with appropriate safeguards ) to allow the import of life - saving treatments or to incentivise increased production in us facilities . 
 ( cid : 1593 ) the lancet oncology editorial for the preserving access to life saving medications act see newsreleases_detail . cfm ? id = 330941& for more on drug shortages in the usa see com / oncology - times / fulltext / 2011 / 02250 / critical_drug_ shortages__who_s_minding_ the_store_.1.aspx for more on isotope shortage in the usa see org / imageuploads / asnc%20 recommendations%20for%20 isotope%20shortage%20 - %20 0603102.pdf see news lancet oncol 2008 ; 9 : 1027 see re ection and reaction lancet oncol 2010 ; 10 : 74546 for the american society of clinical oncologys clinical alert about leucovorin see department%20content / cancer%20policy%20and%20 clinical%20a airs / downloads / cancer%20policy%20news / cancer%20policy%20alert / leucovorin%20alert%208 - 52010.pdf for more on levofolinate combination therapy see clin drug investig 2010 ; 30 : 24349 for the drug shortages summit summary report see summitreport for a list of current drug shortages see gov / drugs / drugsafety / drugshortages / ucm050792.htm vol 12 april 2011 comment if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology as piration of mediastinal and hilar lymph nodes should be used to assess preoperative lung cancer status in countries where tuberculosis is endemic.10 finally , hiv infection is associated with increased lung cancer cases . 
can tuberculosis further increase this risk ? in a study11 that linked aids registry surveillance data for 322 675 patients with aids diagnosed between 1977 and 2002 , with cancer registries in 11 us regions , lung cancer risk over 10 years was unrelated to tuberculosis . 
 tuberculosis awareness in patients with cancer needs to be reinforced , especially in low - burden developed countries , and lung cancer awareness in patients with previous or suspected tuberculosis should be urgently strengthened in developing countries to increase the low numbers of potentially resectable tumours . * sandro vento , massimiliano lanzafame department of internal medicine , faculty of medicine and health sciences , university of botswana , gaborone , botswana ( sv ) ; and infectious diseases unit , gb rossi university hospital , verona , italy ( ml ) ventosandro@yahoo.it we declare that we have no con icts of interest . yu yh , liao cc , hsu wh , et al . 
lancet oncol 2011 ; 12 : 37786in this article ( april ) , on page 380 , the number of women with luminal a breast cancer tested for the kras variant should have been 478 in gure 2a and the percentage of premenopausal women diagnosed with luminal a breast cancer should have been 151% in gure 2b . 
lancet oncol 2011 ; 12 : 41516on page 415 , in the second column , it was stated that 17 variants showed moderate to strong evidence of a true association and were therefore candidates for clinical tests , this should have said 14 variants . 
this correction has been made to the online version as of may 18 , 2011 . published online may 18 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70127 - 9 522 vol 12 june 2011 articles imatinib after induction for treatment of children and adolescents with philadelphia - chromosome - positive acute lymphoblastic leukaemia ( esphall ) : a randomised , open - label , intergroup study andrea biondi , martin schrappe , paola de lorenzo , anders castor , giovanna lucchini , virginie gandemer , rob pieters , jan stary , gabriele escherich , myriam campbell , chi - kong li , ajay vora , maurizio aric , silja rttgers , vaskar saha , maria grazia valsecchi summary background trials of imatinib have provided evidence of activity in adults with philadelphia - chromosome - positive acute lymphoblastic leukaemia ( all ) , but the drug 's role when given with multidrug chemotherapy to children is unknown . 
this study assesses the safety and e cacy of oral imatinib in association with a berlinfrankfurtmunster intensive chemotherapy regimen and allo geneic stem - cell transplantation for paediatric patients with philadelphiachromosome - positive all . methods patients aged 118 years recruited to national trials of front - line treatment for all were eligible if they had t ( 9 ; 22 ) ( q34 ; q11 )  . 
good - risk patients were randomly assigned by a web - based system with permuted blocks ( size four ) to receive post - induction imatinib with chemotherapy or chemotherapy only in a 1 : 1 ratio , while all poor - risk patients received post - induction imatinib with chemotherapy . 
the chemotherapy regimen was modelled on a berlinfrankfurtmunster high - risk backbone ; all received four post - induction blocks of chemotherapy after which they became eligible for stem - cell transplantation . 
the primary endpoints were disease - free survival at 4 years in the good - risk group and event - free survival at 4 years in the poor - risk group , analysed by intention to treat and a secondary analysis of patients as treated . 
4 - year disease - free survival was 729% ( 95% ci 561841 ) in the good - risk , imatinib group versus 617% ( 450747 ) in the good - risk , no imatinib group ( p = 024 )  . 
the as - treated analysis showed 4 - year diseasefree survival was 752% ( 610849 ) for good - risk patients receiving imatinib and 559% ( 361717 ) for those who did not receive imatinib ( p = 006 )  . 
16 patients in the good - risk imatinib group versus ten in the good - risk , no imatinib group ( p = 064 ) , and 24 in the poor - risk group , had a serious adverse event . interpretation our results suggests that imatinib in conjunction with intensive chemotherapy is well tolerated and might be bene cial for treatment of children with philadelphia - chromosome - positive all . funding projet hospitalier de recherche clinique - cancer ( france ) , fondazione tettamanti - de marchi and associazione italiana per la ricerca sul cancro ( italy ) , novartis germany , cancer research uk , leukaemia lymphoma research , and central manchester university hospitals foundation trust . introduction although survival of children with acute lymphoblastic leukaemia is almost 85% , outcome for the 35% of patients with philadelphia - chromosome - positive acute lymphoblastic leukaemia ( all ) is poor.1 , 2 an inter national study3 reported results for 610 children treated with intensive chemotherapy without tyrosine - kinase inhibitors . 
many groups treating adults with philadelphiachromosome - positive acute lymphoblastic leukaemia have noted the safety and e ectiveness of imatinib4 , 5 when given with chemo therapy.620 in an observational study , 21 the childrens oncology group ( cog ) assessed increased exposure to imatinib combined with chemotherapy in ve cohorts . 
44 children who received continuous imatinib from consolidation to the end of treatment , had a 3 - year event - free survival of 80% , with acceptable toxic e ects . 
in a small number of patients treated with a high - risk chemotherapy protocol ( shop - 2005 ) plus imatinib in spain , outcome was good compared with historical controls.22 minimal residual disease at the end of induction is an independent predictor of outcome in childhood acute lymphoblastic leukaemia.23 however , in the cog study , minimal residual disease assessed by multiparameter ow cytometry at the end of induction treatment , before administration of imatinib , was not prognostic for survival . we report results of the european intergroup study of post - induction treatment of philadelphia - chromosomepositive all ( esphall ) , which is contemporary to the cog study . 
the aim was to test the safety and long - term e cacy of post - induction imatinib plus chemotherapy compared with the standard berlinfrankfurtmunster backbone intensive treatment , using a risk - strati ed approach for treatment of patients on the basis of early response to therapy.24 methods patients to provide adequate statistical power , the study was started as a large collaborative trial . 
patients were enrolled into this open - label , randomised trial by ten national study groups , mainly in europe ( aieop , bfm - g / ch , coall , fralle , nopho , mrc , dcog , cph , pinda , and hkphosg ) , which obtained ethics approval from their own institutions . patients aged 118 years recruited to national trials of front - line treatment for all were eligible if t ( 9 ; 22 ) ( q34 ; q11 ) was present according to cytogenetics tested at the participating institution and the presence of a bcrabl fusion transcript identi ed by real - time pcr detecting the transcripts for both the p190 and p210 isoformsor uorescence in - situ hybridisation ( fish )  . 
early response was de ned as blast cell count of less than 1000 cells per l in peripheral blood after 7 days of treatment with prednisone and a single intrathecal dose of meth otrexate , or 25% or less bone marrow blast cells at day 15 , or less than 5% bone marrow blast cells at day 21 , depending on national induction protocols . 
complete remission was de ned as less than 5% blast cells in bone marrow aspirate ( with absolute neutrophil count 1500 cells per l and 100 000 platelets per l ) and bone marrow puncture for assessment of minimal residual disease imatinib treatment reinduction reinduction reinduction reinduction allogeneic stem - cell transplantation allogeneic stem - cell transplantation allogeneic stem - cell transplantation maintenance and cranial irradiation maintenance and cranial irradiation maintenance and cranial irradiation reinduction reinduction good risk randomisation induction poor risk time ( weeks ) figure 1 : study design for details of the chemotherapy regimens see appendix . 
 vol 13 september 2012 see online for appendix articles 229 patients screened 178 enrolled 51 excluded 16 did not meet eligibility criteria * 35 did not enter 108 good risk 70 poor risk 90 randomly assigned 18 excluded 10 clinical decision 8 no consent given 46 allocated imatinib 46 received imatinib 44 allocated to no imatinib 31 did not receive imatinib 13 deviations 1 unknown 9 clinical decision 3 parents refusal 32 received allogeneic stem - cell transplantation 12 did not receive allogeneic stem - cell transplantation 2 early failure 10 clinical decision 37 received allogeneic stem - cell transplantation 9 did not receive allogeneic stem - cell transplantation 1 early failure 8 clinical decision 59 received allogeneic stem - cell transplantation 11 did not receive allogeneic stem - cell transplantation 4 early failure 7 clinical decision 0 lost to follow - up 1 lost to follow - up 0 lost to follow - up 44 analysed 46 analysed 70 analysed figure 2 : trial pro le * 12 not enrolled in front - line acute lymphoblastic leukaemia protocols , two did not have relevant data , one had abnormal renal function , and one had active fungal infection . 
for 24 patients trial protocol not approved by ethics committee , four because of clinical decision , three because of parents refusal , two because of late diagnosis of t ( 9 ; 22 ) , and two died during induction . 
one patient lost to follow - up because of infection with clostridium sp not related to imatinib ( patient had liver failure , disseminated intravascular coagulation , and lung consolidation )  . absence of leukaemia in other organs . 
poor - risk patients were those who did not have early response or complete remission at the end of induction , and received chemotherapy and imatinib . randomisation and masking patients classi ed as good - risk patients were randomly assigned to receive imatinib with chemo therapy or chemotherapy only . 
the study was open label . procedures chemotherapy was modelled on a berlinfrankfurt munster high - risk backbone , 24 with all patients receiving four post - induction blocks of treatmentprotocol ib , hr1 , hr2 , and hr3 ( appendix ) after which they became eligible for allogeneic stem - cell transplantation in complete remission ( gure 1 , appendix ) .1 stem - cell transplantation was recommended for all poor - risk patients and for good - risk patients with any genotypematched donor . 
transplant ation from both matched related and unrelated donors was allowed in good - risk patients because the two techniques seem to have much the same outcome in philadelphia - chromosome - positive all as a result of improved hla matching and supportive care.3 , 26 patients who did not have a transplant had cranial irradiation and two re - induction blocks before continuation of treatment . 
preliminary data from a phase 1 study27 show that daily oral imatinib is well tolerated in children at doses of 260570 mg / m per day , therefore we used an intermediate dose of 300 mg / m per day for our study . 
imatinib was given for 126 days , starting from the end of induction , concomitantly with chemotherapy during protocol ib and in an alternated regimen with the other protocols ( gure 1 ) , as done in contemporary studies of adults ( appendix ) .17 , 20 resistance to protocol was de ned as 5% blast cells or more in bone marrow aspirate at the end of the third consolidation block of treatment for those without previous complete remission . 
late response was de ned as less than 5% blast cells in bone marrow aspirate at the end of either protocol ib or one of three consolidation blocks , for patients who did not have complete remission at end of induction . 
bone marrow relapse was de ned as 25% blast cells or more in bone marrow , after remission . minimal residual disease was analysed in central laboratories ( one for each study group ) that agreed on standard procedures . 
it was assessed in bone marrow and peripheral blood cells collected at eight points ( gure 1 ) , by quantitative real - time pcr ampli cation of immunoglobulin , t - cell receptor gene , 28 and bcr - abl fusion gene , according to guidelines.29 few patients had data for the bcr - abl fusion gene and so they were not included in the analysis , mainly because of scarcity of rna for analysis . 
the main analyses were done by intention to treat ; a secondary analysis was done of patients as treated . from randomisation ( or date of complete remission for poor - risk patients ) until relapse at any site , death during complete remission , or development of a second malignant neoplas event - free survival was de ned as time from start of treatment ( ie , protocol ib ) to rst failure , de ned as resistance , relapse , death from any cause , or second malignant neoplasoverall survival was de ned by the time from start of treatment to death from any cause . time statistical analysis the international trial data centre checked the quality of data and produced blinded yearly reports for the trials steering committee and interim analyses for the data monitoring committee . the study aimed to recruit 140 good - risk patients , to provide 80% power to detect a 24% di erence in 4 - year disease - free survival , with an expected baseline diseasefree survival of 40% ( two - sided test , 5% type 1 error and a minimum of 2 years of follow - up ) , according to lachin and faulkes.32 during 2009 , the steering committee reviewed preliminary study results and external evidence for the bene t of imatinib21 and decided to prematurely stop enrolment . 
for the regressor in the model we included the variables treatment and post - induction minimal residual disease ( three categories : < 510 cells , 510 cells , and unknown ) because of an unexpected imbalance of minimal residual disease in the randomised groups . 
planned secondary analyses were by group at 2 years after censoring patients who had transplants at date of stem - cell transplantation , and as - treated analyses counting deviations from the assigned group and comparing patients who actually received imatinib with those who did not . 
we calculated the probabilities of relapse and of death in continuous complete remission with the cumulative incidence estimator , thus allowing for competing risks , and compared them with the gray test . 
all authors had full access to all the data in the study and had nal responsibility for decision to submit for publication . results recruitment started on jan 1 , 2004 , and ended on dec 31 , 2009 . 
the sponsors had no role in study design , data collection , data analysis , data table 1 : baseline characteristics * early response was assessed in bone marrow in coall , fralle , mrc , and nopho , and in peripheral blood in the other groups . 
up to 2008 ( when evidence for adults became fully available ) , eight of 90 good - risk patients ( 9% ) refused to be assigned , in 2009 , ten of 18 eligible good - risk patients ( 56% ) were not assigned , resulting in 90 good - risk patients being randomly assigned . 
more patients were older than 10 years in the poor - risk group than in the good - risk group and fewer patients had white blood cell counts of less than 50 cells per l at diagnosis ( table 1 )  . all patients except two had progenitor - b philadelphiachromosome - positive acute lymphoblastic leukaemia . 
of 85 patients for whom detection of p190 and p210 was possible , p210 was detected more often in poor - risk patients than in good - risk patients . four patients achieved early response but not complete response at the end of induction and were classi ed as poor risk . 
minimal residual disease at the end of induction was higher in poor - risk patients than in goodrisk patients . baseline characteristics were much the same in each good - risk group , except for post - induction minimal residual disease , with low levels ( < 510 ) more frequent in the good - risk , no imatinib than in the good - risk , imitinab ( table 1 )  . 
108 of 128 randomised patients ( 84% ) had allogeneic stem - cell transplantation after hr3 , eight ( 6% ) before hr3 , and seven ( 5% ) after additional consolidation ( data were unavailable for ve patients )  . 
 * includes patients who failed earlyie , relapsed or died in complete continuous remission within 5 months of complete remission ( one relapse in the good - risk , imatinib group ; one relapse and one death in the good - risk , no imatinib group ; and two relapses and two deaths in the poor - risk group )  . 
no second malignant neoplasms were reported during the follow - up . table 2 : relapses and deaths no imatinib imatinib relapse death no imatinib imatinib adjusted hr 063 , 95% ci 028141 ; p = 026 number at risk no imatinib 44 imatinib 46 time ( years ) time ( years ) figure 3 : disease - free survival and cumulative incidence of relapse and of death in continuous complete remission in good risk patients , analysed by intention to treat ( a ) disease - free survival . 
one event in a patient in the imatinib group at 6 years after randomisation is omitted ( died in continuous complete remission of pulmonary graft - versus - host disease after transplantation )  . 
 940 vol 13 september 2012 articles event - free survival overall survival no imatinib imatinib relapse death no imatinib imatinib adjusted hr 035 , 95% ci 014090 ; p = 003 number at risk no imatinib 31 imatinib 58 time ( years ) time ( years ) figure 4 : disease - free survival curves and cumulative incidence of relapse and of death in continuous complete remission for good - risk patients , analysed as treated ( a ) disease - free survival . 
one event in a patient in the imatinib group at 6 years after randomisation is omitted ( died in continuous complete remission of pulmonary graft - versus - host disease after transplantation )  . patients was 31 years ( 2046 )  . 
for these patients 4 - year event - free survival was 619% ( 95% ci 522698 ) and 4 - year overall survival was 721% ( 95% ci 645797 )  . 
 for the 160 patients who were randomly assigned or in the poor - risk group , 4 - year event - free survival was 610% ( 95% ci 530690 ) and overall survival was 722% ( 95% ci 644800 )  . allogeneic stem - cell transplantation was done in rst complete remission in 137 of 178 ( 77% ) patients ( 78 with good risk , 59 with poor risk ) at a median of 155 days from rst complete remission , and after the hr3 block for 112 ( 82% ) patients ( table 2 )  . 
the most common type of transplant was from hla - matched unrelated donors in both risk groups ( 44 [ 56% ] good risk , 27 [ 46% ] poor risk )  . at 4 years , disease - free survival was 729% ( 95% ci 561841 ) in the good - risk , imatinib group and 617% ( 450747 ) in the good - risk , no imatinib group ( p = 024 ) , with an absolute di erence of 112% ( 95% ci 92 to 316 ; gure 3a ) when calculated by intention to treat . 
 the hr for any event was 071 ( 95% ci 033154 ; p = 038 ) and was 063 ( 95% ci 028141 ; p = 026 ) when adjusted for minimal residual disease after induction . 
 4 - year overall survival was 851% ( 95% ci 696931 ) in the good - risk , imatinib group and 729% ( 539850 ) in the good - risk , no imatinib group ( p = 037 )  . 
the hr for death was 068 ( 95% ci 026181 ; p = 044 ) and 059 ( 021165 ; p = 031 ) when adjusted for minimal residual disease after induction . relapse was the most frequent event in both good - risk groups , involving the bone marrow in all except four patients and half of relapses occurred after stem - cell transplantation , which was done in 37 ( 80% ) of 46 patients in the good - risk , imatinib group versus 32 ( 73% ) of 44 patients in the good - risk , no imatinib group at a median time of 53 months ( iqr 4864 ) versus 54 months ( 4761 )  . 
cumulative incidence of relapse at number at risk 70 time ( years ) figure 5 : survival in the poor - risk group an event that occurred after roughly 6 years is not shown ( relapse in bone marrow and testis after transplantation in rst complete remission )  . 4 years was 248% ( 95% ci 111385 ) in the good - risk , imatinib group and 292% ( 149435 ) in the good - risk , no imatinib group ( p = 066 ) and all relapses occurred within 3 years of entry into the study ( gure 3b )  . 
more deaths remission occurred in patients in the good - risk , no imatinib group than in the good - risk , imatinib group and none were related to imatinib ( table 2 )  . when censored at stem - cell transplantation during rst complete remission , 2 - year disease - free survival was 812% ( 95% ci 307964 ) in the good - risk , imatinib group versus 654% ( 304860 ) in the good - risk , no imatinib group ( p = 097 )  . 
 table 3 : serious adverse events the as - treated analyses compared 58 good - risk patients who received imatinib ( including 12 assigned to the good - risk , no imatinib group ) , with 31 patients who did not . 
the cumulative incidence of relapse at 4 years was 212% ( 95% ci 98326 ) for patients receiving imatinib and 344% ( 164524 ) for those not receiving imatinib ( p = 021 ; gure 4b )  . of the 58 patients receiving imatinib , 11 did not have a transplant , of whom four relapsed . 
none relapsed and three died in continuous complete remission ( one after stem - cell transplantation in rst complete remission )  . of the 70 poor - risk patients , 35 ( 50% ) were not in complete remission at the end of induction . 
4 - year event - free survival was 535% ( 95% ci 404650 ) and 4 - year overall survival was 635% ( 95% ci 502742 ; gure 5 )  . 
35 patients who were in complete remission at the end of induction had a 4 - year event - free survival of 585% ( 95% ci 409761 ) versus 489% ( 95% ci 315491 ) for the remaining 35 who achieved complete remission at a later time ( p = 045 )  . 
 disease - free survival at 4 years from complete remission was the same as event - free survival , because no patient was resistant to protocol . 23 patients relapsed ( table 2 ) within 24 months of study entry , mostly involving bone marrow ( n = 21 )  . 
 proportions of patients with the most commonly reported serious adverse events did not di er substantially between groups ( p = 064 when comparing good - risk patients treated with imatinib to those without ) and were mainly related to myelosuppression ( table 3 )  . 
minor delays ( 1 week ) in administration of chemotherapy were more common in good - risk patients not receiving imatinib than those receiving imatinib ( 14 / 31 [ 452% ] vs 13 / 58 [ 224% ] ) whereas major delays ( > 1 week ) occurred in 25 of 58 ( 431% ) patients in the good - risk , imatinib group versus six of 31 ( 194% ) patients in the good - risk , no imatinib group . 
this cohort includes 319 patients , of whom 31 ( 97% ) were resistant and two ( 06% ) died in induction , leaving 286 patients in rst cr at the end of the protocol - speci ed induction period . 
for historical , good risk versus good risk , imatinib . table 4 : comparison of outcome from esphall with historical data discussion this study was designed to assess the e cacy and safety of imatinib when added to the berlinfrankfurtmunster chemotherapy backbone in paediatric patients with philadelphia - chromosome - positive all . 
enrolment was stopped in 2009 , because of the results of the cog study21 and unwillingness of clinicians and families to enrol after numerous publications on data for adults.19 although the study is not powered to fully address the primary study aim , important conclusions can be derived . all patients enrolled achieved complete remission , whereas previous reports of patients treated with the same chemotherapy backbone note that as many as 10% of patients were resistant to treatment.3 all poorrisk patients not in complete remission after induction had complete remission with imatinib during consolidation treatment . 
disease - free survival was better in the good - risk , imatinib group than in the no imatinib group , despite the di erence in minimal residual disease at baseline , which favoured patients not receiving imatinib . 
only the as - treated analysis showed a better outcome for imatinib - treated patients after adjustment for di erences in minimal residual disease ( although with the caveat of potential selection bias )  . 
detailed , graded data for adverse events were not collected . in a historical cohort of 286 patients , 4 - year disease - free survival was 423% ( 95% ci 364482 ) ; less than in our study ( table 4 )  . 
in the historical cohort , poor - risk patients who had early response assessed by peripheral blood had a worse outcome than those who were assessed by bone marrow early response.3 this nding is supported by data from the historical cohort and our study , although the di erence was not signi cant in our study ( table 4 )  . our results are concordant with those of the cog study21 and provide evidence of long - term bene t of treatment with imatinib for all patient groups ( panel )  . 
patients with poor response to monotherapy with steroids as measured by blast cell count in peripheral blood , compared with bone marrow assessment early in induction , have a worse outcome ( table 4 ) , supporting historical ndings.3 in view of the di erent induction protocols used in each study , inter pretation of this variation is di cult . 
whether starting imatinib ( or a second generation tyrosine - kinase inhibitor ) during induction would cancel the negative e ect of poor early response with steroids is still unclear . the central role of allogeneic stem - cell transplantation was established in a pre - imatinib large cohort of patients.3 however , cog reported21 that allogeneic stem - cell transplantation provides no bene t compared with treatment with intensive continuous imatinib ( cohort 5 )  . 
in esphall , about 80% of enrolled patients had allogeneic stem - cell transplantation , vol 13 september 2012 articles panel : research in context systematic review we searched original english language publications in pubmed to may 16 , 2012 , with the terms ph + all , children , and tki or imatinib . 
one was done by the childrens oncology study group ( cog ) 21 and the other by the sociedad espaola de hematologa y oncologa peditricas.22 in the cog study , an intensive chemotherapy regimen was given with imatinib ( 340 mg / m per day ) administered with increasing exposure in ve cohorts of patients , from 42 ( cohort 1 ) to 280 continuous days ( cohort 5 ) before maintenance . 
3 - year event - free survival improved signi cantly for 44 patients in cohort 5 compared with historical controls , with no important toxic e ects associated with imatinib . 
sociedad espaola de hematologa y oncologa peditricas has reported results of three consecutive trials since 1994.22 in the latest , ( shop - 2005 ) imatinib ( 260 mg / m per day ) was given from day 15 of induction . 
patients with an hla - identical sibling or unrelated donor had allogeneic stem - cell transplantation in rst complete remission ( 15 transplants in 16 imatinib patients vs 17 in 27 historical controls )  . 
3 - year event - free survival of patients who received imatinib was signi cantly higher than that of historical controls who received similar chemotherapy without imatinib . interpretation the results of our study con rm the ndings of previous observational studies , although imatinib resulted in an improvement only in the per - protocol analysis after adjustment for minimal residual disease and in patients with poor prognosis . 
the role of allogeneic stem - cell transplantation in rst complete remission is unclear for patient with philadelphia - chromosome - positive acute lymphoblastic leukaemia receiving imatinib , since most patients in our study had a transplant . the limitation that a common policy of with administration of tyrosine - kinase inhibitors after transplantation was not adopted . 
in both good - risk and poor - risk groups , the few patients who received imatinib but not stem - cell transplantation , excluding those who failed before the median time to transplantation , had a poorer outcome ( three of nine good - risk patients and ve of seven poor - risk patients relapsed )  . 
in this context , serial analysis of minimal residual disease might help to select patients who can be treated with intensive chemotherapy protocols including a tyrosine - kinase inhibitor but without allogeneic stem - cell transplantation . our data support further investigation of new tyrosinekinase inhibitors in conjunction with the established chemotherapy backbone for treatment of children with philadelphia - chromosome - positive all . 
possible next steps are assessments of whether exposure to tyrosine - kinase inhibitors can change the intensity of chemotherapy and the use of transplantation in rst remission . contributors ab , ms , vs , and mgv designed and planned the study . 
all authors coordinated the study in their own countries , were responsible for data in their group , and have revised and approved the nal version of the report . con icts of interest we declare that we have no con icts of interest . acknowledgments the study was supported by projet hospitalier de recherche cliniquecancer ( france ) , fondazione tettamanti - de marchi and associazione italiana per la ricerca sul cancro ( aircig 8666 to ab and aircig 5017 to mgv ; italy ) , central manchester university hospitals foundation trust ( uk ) novartis germany , which provided funds for data management , and cancer research uk . 
analysis of minimal residual disease was funded by a grant from leukaemia lymphoma research . corrections published online november 23 , 2012 s1470 - 2045 ( 12 ) 70533 - 8 correction to lancet oncol 2012 ; 13 : 549 , 554 from prostate hormone therapy alone james nd , sydes mr , mason md , et al , for the stampede investigators . 
lancet oncol 2012 ; 13 : 54958in the summary of this article , the second sentence of the findings section should read : at the preplanned analysis of the second intermediate activity stage , with 305 ffs events ( 209 in arm a , 96 in arm d ) , there was no evidence of an advantage for hormone therapy plus celecoxib over hormone therapy alone : hr 094 ( 95% ci 074120 )  . 
the rst sentence of the fth paragraph of the results should read at this second intermediate analysis , celecoxib showed insu cient evidence of activity , in terms of ffs , for continuation of accrual to this comparison : hr 094 from adjusted cox model ( 75% ci upper limit 103 ; 95% ci 074120 ; gure 3 )  . 
these corrections have been made as of nov 23 , 2012 . vol 14 january 2013 comment are more likely to opt for burdensome treatment with a small chance of improvement than are healthy people.6 , 7 following a deliberative model of patientphysician interaction , 8 the physician should explain his or her own assessment of bene ts and harms , including the underlying health - related values ( see question two ) , thereby empowering the patient to reconsider his or her own values , preferences , and the resulting decision . 
 if the patients choice to proceed with the intervention results from deeply held values coupled with a thorough understanding of the facts , the patient and the physician should proceed with the intervention . 
 although physicians should always minimise the required resources to achieve a speci c treatment goal , whether a high consumption of resources constitutes a legitimate reason to withhold an intervention that provides only a questionable or small net bene t to the patient is controversial.9 , 10 under the assumption that the setting of limits is unavoidable in any health - care system , we have included a fth question that asks doctors to take the resource implications of their decisions into account in an ethically justi ed way . 
the question becomes relevant in all health - care systems in which physicians have to ration care through budgets , waiting lists , or the application of rationing rules to individual cases . 
if the patient has a realistic understanding of the situation and there is persistent disagreement about the value of the intervention ( after answering question four ) , the physician should explicitly inform the patient that the requested intervention provides only a small or questionable net bene t at high costs . 
alternatively , if the patient does not have a realistic understanding of his or her medical situation and the bene tharm ratio of the intervention is at least questionable in the physicians judgment , question ve could guide the decision . 
however , if the treatment draws heavily on resources , considerations of equality might justify a unilateral decision to withhold the requested intervention , because the high resource consumption is not counterbalanced by a clear net bene t or sound autonomy - based arguments . 
beyond futility : to what extent is the concept of futility useful in clinical decision - making about cpr ? lancet oncol 2002 ; 3 : 63842 . consensus statement of the society of critical care medicines ethics committee regarding futile and other possibly inadvisable treatments . 
 motesanib , or open - label bevacizumab , in combination with paclitaxel , as rst - line treatment for her2 - negative locally recurrent or metastatic breast cancer : a phase 2 , randomised , double - blind , placebo - controlled study . 
lancet oncol 2011 ; 12 : 66372in the summary , the nal sentence of the findings section should have stated 12 208 ( 73% ) of the women positive by hpv testing had no cytological abnormality , and these women had 258 ( 35% ) of 747 cin3 or adenocarcinoma in situ , 25 ( 29% ) of 87 cancers , and 17 ( 63% ) of 27 adenocarcinomas . 
this correction has been made to the online version as of july 29 , 2011 . 722 vol 12 august 2011 corrections correction to lancet oncol 2012 ; 13 : 983 , 986 correction to lancet oncol 2012 ; 13 : 1028 correction to lancet oncol 2012 ; 13 : e468 fizazi k , scher hi , molina a , et al , for the cou - aa - 301 investigators . 
abiraterone acetate for treatment of metastatic castration - resistant prostate cancer : nal overall survival analysis of the cou - aa - 301 doubleblind , placebo - controlled phase 3 study . 
 this correction has been made as of oct 29 , 2012 . randomised , chemorefractory jfw , van den smits mlj , nijsen holmium - 166 bosch maaj , et al . 
lancet oncol 2012 ; 13 : 102534in table 1 of this article , the total number of patients with ocular melanoma should have been six , as should the total number of patients with colorectal carcinoma . 
lancet oncol 2012 ; 13 : e468in this news item , the second and third sentences of the second paragraph should have read : median pfs was 94 months ( 95% ci 86167 ) in the combination group compared with 58 months ( 4674 ) in the dabrafenib monotherapy group ( hazard ratio 039 , 95% ci 025062 ; p < 0001 )  . 
whether this will prove to be bene cialboth for the balance sheet and , more importantly , to the patientswill depend on the regional context and how the process is managed . on april 4 , 2012 , the community oncology alliance ( coa ) , a non - pro t organisation dedicated to community oncology in the usa , published an update to their practice impact report , showing that in the past 45 years , nearly 700 oncology practices and clinics across the usa closed or are struggling nancially , with many private oncology practices being bought out or consolidated into a hospital setting . 
the act changed the way in which medicare and medicaid pays for prescription drugs , with oncology practices seeing a signi cant reduction in payment for chemotherapy agents which often does not cover the cost of the drugs . 
the consequences of this act are far - reaching , with many private insurance companies following this lead , resulting in further di culties for cancer - care providers . for oncology services that are still being provided , those in a hospital setting potentially result in increased costs when compared with private clinics . 
a study by the healthcare research company avalere health , commissioned by the coa , found that treatment for patients receiving chemotherapy in a hospital outpatient environment costs an average of 24% more than those who receive the same treatment in a private oncology clinic . 
however , the study was unable to determine whether the level of care requirements were higher in hospitals . at the personal level in the usa , cancer patients often nd themselves left without a safety net if they eventually become too ill to work . 
 hospital closures in the uk and other countries have lead to a consolidation of care which has been blamed for increasing the nancial burden on cancer patients , mainly via increased transport costs to and from clinics to see oncologists . 
complaints about regional variation for the funding of cancer drugs and a lack of choice add further complexities to an over - burdened syste the uk charity macmillan cancer support has highlighted the concerns to patients in a recent report , and are working with the nhs in wales to ensure that all cancer patients are provided with advice to help them cope with increased nancial stra there can , however , be bene ts gained from a consolidation of care . 
in some health - care systems , organised groups of clinicians have better purchasing power to broker more favourable deals with drug companies and suppliers , and integration of care within a hospital group or within a private company does not necessarily mean a shrink in geographical coverage or levels of provision . 
the formation of the regional cancer care associates ( rc2a ) in new jersey , usa , is potentially an early indication on how consolidation can be done for the bene t of the patient . 
this large company works to one standard at all sites to provide a transparent standard of care , improve access for patients to clinical trials , and to reduce over - testing and over - treatment . it is clear that the consolidation of cancer care will continue , with both public and private health care systems a ected . 
although there are pros and cons to any structural reorganisation , it is imperative that all decisions are thought through carefully to ensure that above all patient care is not a ected , and second that any cost savings are not simply transferred to the patients own expenditure . 
overall e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against grade 3 or greater cervical intraepithelial neoplasia : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 8999in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
cross - protective e cacy of hpv - 16 / 18 as04 - adjuvanted vaccine against cervical infection and precancer caused by non - vaccine oncogenic hpv types : 4 - year end - of - study analysis of the randomised , double - blind patricia trial . 
lancet oncol 2012 ; 13 : 10010in this article ( published online nov 9 , 2011 ) , the author a liations for xavier castellsagu and f xavier bosch did not include all relevant information . 
lancet oncol 2012 ; 13 : 1012in this comment ( published online nov 9 , 2011 ) , the last sentence of the sixth paragraph incorrectly lists hpv - 35 as one of the oncogenic hpv types covered by the new nine - type gardasil vaccine ; the list should include hpv - 45 instead . 
in this personal view , we discuss why small , low - grade gleason pattern prostate lesions , which are currently designated as prostate cancer , could be regarded as non - malignant . 
these lesions either do not meet the criteria of the hallmarks of cancer or robust evidence that they do so is absent , by contrast with large lesions with a high gleason grade , which seem to cause most metastatic disease . introduction diagnosis and treatment of localised prostate cancer has been a much debated topic and as such is fraught with controversy . 
this situation has not been helpful for men who are at risk of prostate cancer or who have been diagnosed with the disease.1 the issues have been well described : over diagnosis , underdiagnosis , missed diagnosis , misclassi cation of risk , overtreatment , and under treatment . 
despite a general acceptance that these issues are both real and important , few recommendations have been suggested to help to mitigate them . one approach that merits some discussion is the reclassi cation of the generic term prostate cancer ( when applied to disease localised to the prostate ) into two subtypesone that can be safely ignored , or better , not diagnosed and another that , if left untreated , would compromise either quality or quantity of life . 
possible bene ts of not diagnosing a lesion that is unlikely to a ect a patients life include reduction of the anxiety of living with a cancer diagnosis and avoidance of potential radical surgery that might not be of clinical bene t and could cause substantial side - e ects . 
add itionally , esserman and colleagues3 have argued that minimal risk lesions should not be called cancer , with these lesions perhaps instead being called indolent lesions of epithelial origin ( idle )  . 
others have o ered similar opinions in the past year.4 , 5 not all prostate cancers are destined to progress the future behaviour of lesions that are identi ed early in the natural history of several cancers remains uncertasome will regress , others will remain stable , some will seem stable because of very long celldoubling times , and a few will progress . 
although lung cancer is one of the most lethal cancers in terms of the ratio of diagnoses to cancer - speci c deaths , one in six individuals who die of causes other than lung cancer will have apparently malignant lesions at autopsy ; these lesions are now termed pseudodisease in recognition of their non - malignant behaviour . 
had these lesions been diagnosed during life rather than at autopsy , treatment would have resulted , but with little bene t to the patient and some harms and costs.6 thyroid cancer is closer to prostate cancer in terms of the burden of subclinical disease . 
an familiar with pathologists are increasing recognition that progression , metastases , and death are rare events in small renal masses has led to similar discussion about whether such lesions should also be deemed pseudo disease.9 low - risk , noninvasive bladder lesions have also been successfully reclassi ed from bladder cancer to papillary urothelial neoplasia of low malignant potential.10 these we believe , as do many others , that it is time to apply the same reasoning to low - risk prostate cancer . 
 prostate cancer is generally multifocal and consists of a dominant focus ( as measured by tumour volume ) , deemed the index lesion , and one or more separate , secondary tumour foci of smaller volume ( gure 1 )  . 
 much laboratory and clinical evidence has shown that we need to rethink the nomenclature we apply to lowgrade and low - volume lesions.11 we believe that small , low - grade gleason pattern lesions , which are currently designated as prostate cancer , could be regarded as nonmalignant . 
using the framework provided by hanahan and weinberg , 12 we argue that these lesions either do not meet the criteria of the six hallmarks of cancer , or robust evidence that they do so is absent , by contrast with larger , high - grade lesions , which seem to cause most metastatic disease . vol 13 november 2012 e509 personal view insensitivity to antigrowth signals decreased expression cdkn1b increased methylation of cyclin d2 resisting apoptosis overexpression of bcl2 overexpression of dad1 index lesion low - grade , low - volume secondary lesions unlimited replicative potential decreased androgen signalling overexpression of erg sustained angiogenesis increased microvessel density increased expression of proangiogenic factors self - suciency in growth signals overexpression of egfr amplication of her2 / neu local tissue invasion and metastasis overexpression of cxcr4 monoclonal nature of invasion and metastases of lesions very low mortality in men with only low - risk lesions figure 1 : hallmarks of cancer as applied to the index and secondary lesions in prostate cancer the changing face of gleason grading in 1966 , donald gleason rst published his unique grading system for prostate cancer based solely on the architectural pattern of the tumour.13 he developed a 5 - point scale on the basis of the outcomes of 270 patients , in which patterns 1 , 2 , and 3 represented tumours that most closely resembled healthy prostatic glands , and patterns 4 and 5 represented tumours ( or parts of tumours ) that were increasingly anaplastic in appearance ( gure 2 , table ) .14 an innovative aspect of this system was that , rather than assigning the worst grade as the grade of the carcinoma , the sum of the two most common patterns is calculated and reported as the gleason sum score . 
since the gleason system was introduced , pathologists have adopted modi cations to the original grading system as described , to adapt it to modern needs ( table )  . redesignation of cancer to non - cancer within the gleason system is not new . 
gleason patterns 1 and 2 , originally described by gleason as changes consistent with malignant transformation , are now regarded as normal variants of the prostate architecture.15 the redesignation of gleason pattern 3 ( possibly quali ed by an upper threshold on volume ) could be the next incremental step on a 40 - year process of re nement of the gleason classi cation systefor example , there has been an accepted grading shift upwardsone element of the so - called will rogers phenomenon16with the changing de nition of gleason pattern 4 resulting in the regrouping of cases previously regarded as gleason score 6 into the gleason score 7 classi cation . 
in many cases of cancer in which the patterns would previously have been assigned to the lowest gleason pattern 1 , advances immunohistochemistry have shown the presence of basal cells , identifying such cases as atypical adenomatous hyperplasia , a benign mimic of cancer.17 moreover , lesions with patterns 1 and 2 have been recognised as biologically similar to pattern 3 , further discouraging their use ( table )  . hallmark one : self - su ciency in growth signals tumour cells can generate their own growth signals and reduce their dependence on stimulation from the surrounding normal tissue microenvironment . ross and colleagues18 used laser capture microdissection to extract cells from radical prostatectomy specimens from 23 men to create two subgroups , those with either exclusive gleason pattern 3 ( gleason score 6 ) or those with exclusive pattern 4 ( gleason score 8 )  . 
the investigators measured mrna expression of 18 344 unique genes in the extracted cells , and noted di erential expression of 670 of these genes between gleason pattern 3 and gleason pattern 4 lesions . 
overexpression of both of these genes is associated with independent cell proliferation and enhanced cell motility through several signal transduction mechanisms , including the mapk , akt , and ras pathways . 
as well as the upregulation of egfr , the investigators showed overexpression of map2k4 and the egf - activated promigratory gene rala , and downregulation of reps2 ( which negatively regulates egfr via endocytosis ) , phlpp , and pml ( both of which inactivate the protein kinase phospho - akt , which mediates growth - factor associated cell survival ) in gleason pattern 4 lesions . skacel and colleagues19 used a tissue microarray of more than 300 tissue cores derived from radical prostatectomy specimens to show that her2 / neu protooncogene ampli cation , as measured by uorescent in situ hybridisation , was associated with high tumour volume of greater than 20 cm ( p = 0004 )  . 
ampli cation of her2 / neu , a member of the egfr family , was almost exclusively con ned to gleason pattern 4 lesions rather than gleason pattern 3 lesions . hallmark two : insensitivity to antigrowth signals cancer cells must be able to resist the normal antigrowth signals that push them into a quiescent phase of the cell cycle or enter into postmitotic phases that ensure speci c cell di erentiation . e510 vol 13 november 2012 personal view score ( lesions that included gleason patterns 4 and 5 ) compared with those that were only pattern 3 . hallmark four : unlimited replicative potential mammalian cells seem to have an inherent autonomous function , independent of cell - to - cell signalling , that limits their replicative ability . 
we have some evidence that exclusive gleason pattern 3 prostate lesions have this brake preserved and that high - grade cancers are more likely to have evolved a mechanism to overcome it . 
they used radical prostatectomy specimens ( 101 micro dissected specimens from 44 individuals ) to develop two phenotype tissue poolsone low - risk ( exclusive gleason pattern 3 ) and one high - risk ( gleason pattern 4 or higher )  . 
the high gleason grade lesions showed decreased androgen signalling , similar to metastatic prostate cancer , which could re ect dedi erentiation and account for the clinical association of the grade of the high - grade lesions with prognosis . 
this nding was also reported by hendriksen and colleagues , 26 who noted lower androgen signalling in high - grade gleason pattern prostate cancer than in low - grade gleason pat tern lesions . 
the researchers suggested that localised prostate cancer cells become more aggressive by selectively downregulating androgen - responsive genes , which results in increased tumour cell replication and proliferation , dedi erentiation , or reduced apoptosis . another mechanism that is available to the cell to overcome the intrinsic brake on replication is gene translocation . 
the tmprss2erg translocation is one of the most prevalent genetic changes in prostate cancer , the presence of which results in overexpression of the erg transcription factor , and therefore promotes proliferation . 
this loss of cdkn1b was associated with an increase in the proliferative index of high - grade prostate cancers . hallmark three : resisting cell death the ability of cancer cells to resist programmed cell death ( apoptosis ) is key to ensuring continued growth and proliferation . true and colleagues23 used laser capture microdissection to acquire speci c subpopulations of prostate cancer cells consistent with lesions containing gleason patterns 3 , 4 , and 5 from 29 radical prostatectomy specimens . 
they pro led transcript abundance using cdna micro array analysis and developed an 86 - gene model capable of di erentiating between lesions that contain gleason pattern 3 and those that contain higher patterns ( 4 and 5 )  . 
one speci c discriminatory gene identi ed was dad1 , a gene encoding defender against cell death 1 , which is a downstream target of the nfb survival pathway and displays an antiapoptotic function . 
 dad1 protein concentrations showed a strong association with gleason grade , with tumours of patterns 4 and 5 more likely to stain intensely compared with gleason pattern 3 . tissue another more familiar antiapoptotic gene is bcl2 , the role of which in carcinogenesis and castrate resistance in prostate cancer is well established . 
 ( d ) gleason grade 4 ( increased stromal invasion ; white arrows show some areas of gland fusion and poorly de ned lumens ; green arrow shows one of a few areas in which gleason pattern 3 is present ; original magni cation 40 )  . 
 since tmprss2erg fusions lead to frequent changes in the erg proto - oncogene in early - stage prostate cancer , investigation of this fusion in preneoplastic cells and multifocal lesions from the same patient has the potential to de ne its role in prostate cancer onset , progression , and heterogeneity . 
in a cross - sectional study27 in which individual cancers from radical prostatectomy specimens with two to three tumour foci of various sizes and grades were analysed , the researchers established that erg protein expression is signi cantly increased in tumours with large volumes and high gleason grade , presumably as a result of this transcription factor promoting tumour growth and proliferation . however , other evidence emphasises the uncertainty about the role of this particular gene fusion in prostate cancer development and progression . 
others29 have shown a strong relation between expression of tmprss2erg fusion mrna isoforms and pathological measures of clinical outcome ( seminal vesicle invasion , extracapsular exten sion ) in lesions from radical prostatectomy specimens . 
the same researchers also reported expression of the gene fusion in benign glands of the prostate . hallmark ve : sustained angiogenesis neoangiogenesis is a normal physiological process that takes place during embryonic development and wound healing . 
the process is also necessary for tumours to break through the volume threshold of 1 mm diameter , since tumours larger than this cannot rely on the di usion of oxygen from existing vessels . angiogenesis is probably necessary to support accelerated tumour growth , since the metabolic needs of the tumour must be met by an adequate blood supply.30 prostate cancer cells have the ability to produce several factors that promote new vessel formation . 
so the question arises , does this forced vascular proliferation occur preferentially in high - grade lesions or is it a transformation that is permissive for proliferation and dedi erentiation of prostate cancer cells ? raised vegf and increased microvessel density are related to a poor prognosis in prostate cancer , 31 and a close association exists between the two . 
moreover , this association seems to be more pronounced in high - grade and large tumours than in low - grade and small tumours.32 in a well designed study , mucci and col leagues33 established that poorly di erentiated tumours showed increased microvessel density and irregularity of the blood vessel lumen with reduced vessel size . 
men with tumours that had the smallest vessel diameter at inclusion were six times more likely ( 95% ci 18200 ) to develop metastatic prostate cancer or to die from the disease . 
 additionally , another subgroup was identi ed that had even greater propensity for clinical progression ; men who had irregularity of vessel diameter were 17 times more likely ( 95% ci 23128 ) to reach the same two endpoints . 
microvessel density itself was not linked to cancer - speci c mortality after results were adjusted for clinical factors.33 in higher - grade other factors are either required or facilitate new vessel formation . 
pericyte distribution was mapped from e512 vol 13 november 2012 personal view - smooth - muscle - actin - positive immune - stained histological sections and quanti ed by image analysis . 
 exclusive gleason pattern 3 lesions had a microvessel pericyte density score that could not be distinguished from benign prostate tissue , by contrast with the scores of higher - grade lesions . hallmark six : tissue invasion and metastasis the potential for invasion into adjacent anatomical structures and spread to distant sites are key attributes of cancer cells . 
for example , when individual prostate lesions derived from one patients primary prostate cancer specimen were implanted into mice , only one lesion out of three showed characteristics of local invasion and eventually formed metastases.36 this work reminds us that as well as histological heterogeneity within any one prostate lesion there are , within the cancer , distinct elements with a range of biological potentials . 
this g - protein - coupled transmembrane receptor has a key role in the directional migration of cancer cells to speci c metastatic sites in response to its ligand cxcl12 . 
additionally , cxcr4 upregulation has been associated with lymph node and bone metastasis in prostate cancer , possibly through activation of the ras oncogene family member rap1a , the expression of which is also upregulated in gleason pattern 4 lesions relative to those containing only gleason pattern 3 . 
 investigators of other studies have suggested that hypoxia induces cxcr4 expression in tumour cells via hypoxiainducible factor 1.37 , 38 large volume tumours are much more likely to have central hypoxic areas than are small volume tumours . 
expres sion of cxcr4 on the tumour cell membrane allows the cancer cells to migrate or metastasise away from the area of low oxygen tension , down a cxcl12 concentration gradient , to areas of high oxygen concentration . 
the ligand cxcl12 is secreted at especially high concen trations by lymph node and bone marrow stromal cells . most men have two to three distinct tumour foci in their prostate at presentation . 
other researchers40 have noted that 80% of secondary foci are smaller than 05 cm and have the same volume distribution as do tumours found incidentally in patients that undergo cystoprostatectomy for bladder cancer . 
tumour volume has been proposed to be associated with prostate - speci c antigen ( psa ) recur rence41 and prostate lesions smaller than 05 cm are almost always clinically insigni cant because of the long doubling times of such lesions.42 several authors43 , 44 have proposed that the threshold for signi cance of volume be placed higher , at 12 cm , on the basis of data from the european large - scale ran domised prostate cancer screening trial , in which volume thresholds of insigni cant disease were calculated on the basis of models of lifetime risk estimates of prostate cancer diagnosis in screened and non - screened participants . 
however , after accounting for tumour stage and grade , the threshold volumes for the index tumour and total tumour were 13 cm and 25 cm , respectively.43 , 44 a strong association also seems to exist between pathological and staging measures of poor prognosis ( extracapsular invasion , seminal vesicle invasion , metastases ) and individual cancer lesion volumes . 
lesions measuring 05 cm or more had a one in ten chance of capsular invasion , whereas lesions measuring 40 cm or more had a one in ten chance of seminal vesicle invasion . 
lesions measuring 50 cm or more had a one in ten chance of metastases.45 volume is an important determinant of grade ( or vice versa ) ; gleason pattern 4 or higher is very rare in lesions that are not attributed index status.46 if the volume of a lesion is a key attribute of progression , as it seems to be , 47 then multiplicity for any given overall tumour volume within a prostate should be a good prognostic sign . 
in other words , if 2 cm of tumour is distributed fairly equally among ve separate lesions , the mean lesion volume will be less than 05 c if , on the other hand , the cancer was unifocal ( seen in about one in ve men who present with prostate cancer ) , then the mean tumour volume will equate to the overall tumour volumeie , 2 cthe primacy of the index lesion as a determinant of progression seems to hold . the next question in relation to the volume of speci c prostate cancer foci is about the biological potential of these small lesions . 
schmid and colleagues48 have reported that 79% of men with vol 13 november 2012 e513 personal view previously untreated prostate cancer of all clinical stages , who had serial psa measurements during a period of at least 12 months , had a tumour doubling time greater than 24 months . 
primary tumour volumes that theoretically lead to distant metastases tend to be at least 4 cm in volume.49 as such , with an estimated tumour volume doubling time of 2 years , it would take about 6 years for a 05 cm lesion to reach a volume of 4 cm . although overwhelming evidence suggests that small tumours are very safe from a biological perspective , there remain some anomalies that remind us that our understanding is far from complete . 
up to one in four tumours that show capsular invasion can be identi ed as non - index lesions , 50 and although tumours that are locally invasive do need to achieve some volume threshold , they do not necessarily have to be very large.51 in fact , circulating tumour cells and occasionally lymph - node metastases have been reported in men who have lesions of 02 cm in volume.52 in a series of 239 patients with tumour volumes of less than 05 cm , investigators showed that 43 were poorly di erentiated , 11 had extracapsular extension , six had positive surgical margins , two had positive lymph nodes , and seven progressed within 5 years.53 greene and coworkers54 assessed dna ploidy status , which is an independent prognostic factor for localised prostate cancer . 
thus , tumour volume in itself did not adequately predict the biological potential of prostate cancer and so should be combined with other factors , predominantly gleason grade . the molecular association of individual lesions with lymph node metastases has added more force to the argument that , despite multifocality , prostate cancer disease progression is likely to be related to lesions that meet some minimum grade and volume thresholds . 
 tmprsserg gene fusions seen in lymph node metastases are also found in the index lesion and not in small , low - grade satellite lesions55 or secondary highlesions.56 results of one grade and high - volume important study57 showed that metastatic deposits taken from men in a rapid autopsy protocol shared one common cell of orighowever , the question of whether the metastatic clone originated from the index lesion is something that was not possible to address in this study because of the nature of the men from whom the tissue samples were taken ( ie , they had been through rst - line and second - line hormonal therapies in addition to chemotherapy in some instances , so the prostates were small and brotic , which made the delineation of individual lesions impossible ) .58 grasso and colleagues59 also noted the monoclonal origin of lethal , castrateresistant prostate cancer by sequencing the exomes of metastatic deposits in 50 lethal , heavily pretreated metastatic cancers obtained at autopsy . epidemiological evidence also supports the assertion that most prostate lesions , especially those of low volume and low gleason grade , currently called cancer , do not show tissue invasion and eventual metastases . 
similar frequencies are seen on assessment of prostates taken from cystoprostatectomy specimens from men who have undergone surgery for high - risk or invasive bladder cancer.40 therefore , since a third of men have prostate cancer that will not a ect them in their lifetimes , it is unsurprising that small , low - grade lesions have low ( or possibly absent ) malignant potential . this argument is lent support by ndings from longterm radical prostatectomy outcome series . 
for example , eggener and coworkers60 showed that , of 9775 men who had gleason 3 pattern in isolation con rmed on radical whole - mount prostatectomy specimens , only three died of prostate cancer in a 15 year period . 
in fact , when these three patients were reviewed , a small amount of gleason pattern 4 was seen.1 this nding cannot merely be accounted for by the success of surgery itself and is strong evidence that exclusive gleason pattern 3 lesions are not a metastatic phenotype . 
 prostate others61 , 62 have reported similar ndings in smaller cohorts of patients , but using biochemical recurrence as a surrogate out come measure . the scienti c literature about the advantages and disadvantages of active surveillance also helps the understanding of whether low - volume , low - grade disease behaves in a malignant way . 
warlick and colleagues63 investigated whether curability after surgery , which they de ned as surgical pathological characteristics that would generally confer a greater than 75% chance of remaining biochemically recurrence - free at 10 years , was a ected if treatment was delayed.64 in other words , is the window of opportunity for curesomething that con cerns patients and physicians alike when considering active surveillancelost in men with small , low - grade disease who have delayed curative treatment ? after comparing the burden of supposedly incurable cancer among patients undergoing delayed surgery at a median time of 265 months after diagnosis with that in patients undergoing immediate surgery ( who would have been eligible for active surveillance ) the investigators reported no association between adverse pathological changes on whole - mount specimens and the time period between diagnosis and surgery . 
clinical experience with active surveillance suggests that an estimated risk of metastasis exists of less than 1% at 28 years64 and disease - speci c mortality of 1% at 8 years in men undergoing surveillance for low - risk disease as classi ed by a diagnostic transrectal ultrasound - guided biopsy . 
early outcomes in men with intermediate - risk disease managed by active surveillance have also been encouraging.65 results of research that has assessed active surveillance have shown that all prostate cancer - related mortality occurred e514 vol 13 november 2012 personal view in men who had been reclassi ed as higher risk and who were o ered radical treatment . 
in other words , when compared with a more rigorous sampling strategy , transrectal ultrasound - guided biopsy undergrades and understages disease as a result of random and systematic errors in sampling the prostate.66 clinical implications when prostate cancer is identi ed from biopsies , the psychological connotations associated with having cancer mean that many men choose or are advised to undergo radical treatment that they stand little chance of bene ting from.67 most clinicians advising patients know that exclusive gleason pattern 3 carries very little lifetime risk to the patient , but many still recommend radical treatments that carry high toxicity pro les . 
the absence of precision means that the attribution of low risk is insecure in about one in three men who are deemed to be at low risk ( exclusive gleason pattern 3 disease ) , but in fact are not . 
if we could accurately identify men with gleason pattern 3 lesions in isolation , these men would be very likely to be at much lower ( possibly negligible ) risk of death from prostate cancer than men previously attributed a gleason pattern 3 diagnosis of cancer . 
if this situation came to pass , we might be in a position to reclassify exclusive gleason pattern 3 lesions to a term that substitutes the word cancer for something else , such as idle.3 such a term would seem to be appropriate ; if low - volume , lowgrade lesions were reclassi ed as non - cancer or idle lesions and this change met with widespread professional acceptance , the immediate implications for clinical practice would be profound . first , research into novel detection strategies and therapies is likely to need substantial rethinking . 
in fact , hundreds of millions of pounds have been spent on the discovery of an elusive biomarker during the past two to three decades , on the premise that the outcomes from the transrectal ultrasound - guided biopsy are the gold standard . 
a third of all men diagnosed with prostate cancer are estimated to have clinically insigni cant disease.64 , 68 , 69 furthermore , transrectal prostate biopsies can miss a clinically signi cant cancer that is likely to progress and metastasise within a mans lifetime ( which incorrectly designates the patient a true negative )  . 
40% of men who test negative on biopsy are estimated to have cancer ; 68 , 70 of these , a third have clinically signi cant cancer based on lesion volume and presence of high grade.69 second , a recalibration of what is deemed cancer is likely to substantially reduce the overdiagnosis and overtreatment burdens with which we are all familiar . 
the performance characteristics of multiparametric mri , for example , coupled with an intensive sampling strategy , in being able to rule out 05 cm lesions with a negative predictive value of about 9095% , is arguably an ideal test.71 a large multicentre study is in progress that is assessing the reproducibility of such imaging in men at risk before any biopsy , against a reference standard that can be applied in all men and not only those who undergo surgery ( nct01292291 )  . 
the key with imaging is that it could provide an accurate volume with indicators of high gleason grade before biopsy and act as a triage test to identify men who need biopsies , which would allow men with no clinically signi cant cancer to avoid entering the diagnostic pathway altogether.72 third , when compared with other solid organ malignancies , prostate cancer is an outlier . 
treatments for breast , renal , thyroid , liver , and pancreatic cancers all include tissue - preserving therapies , if appropriate , which are dependent on location and burden of the cancer . 
 these specialties in oncological surgery de veloped tissue preservation , as opposed to halsted prin ciples for wide surgical margins , because of upstream diagnostic methods that rely on identifying measurable ( by palpation or imaging ) disease that can undergo targeted sampling followed by targeted treatment . 
random and blind sampling has forced our hands as clinicians , so that we have to apply radical whole - gland principles because the exact disease statuses of regions of the prostate are search strategy and selection criteria we searched pubmed and medline for relevant publications from the past 10 years ( jan 1 , 2002 to april 16 , 2012 ) , and supplemented the results of our search with key articles from before this period when appropriate . 
so , if multifocality is overlooked in other organs by targeting only the measurable index lesion that which is largest by size and has elements of the highest gradethat targeting these lesions in prostate cancer might be su cient to lead to acceptable , possibly equivalent , cancer control rates to whole - gland therapy is a reasonable hypothesis . 
focal therapy certainly leads to reduced genitourinary and rectal sidee ects , if the results of early prospective studies are reproducible and surgeons.7375 however , the key will be to design longitudinal cohort and comparative e ectiveness studies that assess medium - term and long - term cancer control . 
such research will need to focus on the natural history of untreated benign and low - volume , low - grade prostate lesions . populations , centres , across contributors hua conceived the personal view , and ma and hua did the database searches and identi ed relevant articles . 
all authors redrafted the report through several iterations and approved the nal submitted version . con icts of interest me and hua received funding from ushifu , glaxosmithkline , and advanced medical diagnostics for clinical trials . 
none of these funding sources had any input or role in the production of the report . acknowledgments me and hua acknowledge funding from the medical research council ( uk ) , pelican cancer foundation , prostate action , st peters trust , wellcome trust , national institute for health research health technology assessment programme ( uk ) , the us national institutes of healthnational cancer institute , and the prostate cancer research centre . 
me receives funding in part from the uk national institute for health research university college london hospitals / university college london comprehensive biomedical research centre . articles e ect of hiv on survival in patients with non - small - cell lung cancer in the era of highly active antiretroviral therapy : a population - based study ramesh rengan , nandita mitra , kaijun liao , katrina armstrong , anil vachani summary background hiv - infected patients with lung cancer have been reported to have poorer survival than uninfected patients . 
we examined the e ect of hiv infection on clinical outcome in patients with lung cancer who are also receiving haart . methods patients diagnosed with non - small - cell lung cancer ( nsclc ) from jan 1 , 2000 , to dec 31 , 2005 , with or without hiv infection were identi ed by querying the surveillance , epidemiology , and end results registry and the medicare lung cancer database . 
survival analysis by stage and treatment delivered comparing the hiv - infected patients with uninfected controls was done with kaplan - meier and cox models with propensity score adjustments . findings 71 976 patients with nsclc were identi ed as uninfected controls and 322 patients with nsclc were identi ed in the hiv group ; median age was 75 years for both groups . 
median overall survival for all stages was 70 months ( 95% ci 7070 ) for uninfected controls versus 80 months ( 60100 ) for the hiv group ( p = 016 ) ; for those with stage i / ii disease it was 370 months ( 360390 ) versus 430 months ( 260580 ; p = 037 ) ; for those with stage iiia / iiib disease it was 70 months ( 7070 ) versus 30 months ( 2080 ; p = 0051 ) ; and for those with stage iv disease it was 30 months for both groups ( 95% ci 3030 for controls ; 2050 for hiv group ; p = 077 )  . 
since the adoption of haart in the mid - 1990s , the expected survival of patients with hiv has improved substantially.21 , 22 although haart e ectively treats the immunosuppression associated with hiv infection , data also suggest that these drugs could diminish the e cacy of the antineoplastic regimens routinely used in the treatment of lung cancer.23 therefore , the clinical outcome of hiv - infected patients with lung cancer in the era of haart remains unclear . our study was designed to assess overall survival in hiv - infected patients with nsclc in the era of haart compared with uninfected patients . 
additionally , for patients with early stage nsclc , for whom surgical resection is the standard of care , we have assessed overall survival in hiv - infected patients after surgical resection as compared with uninfected patients . 
our goal was to establish whether nsclc displayed a more aggressive phenotype in hiv - infected individuals , to quantify the e ect of viral infection on clinical outcome in patients with nsclc . 
the broader objective was to establish the role that hiv infection should have in clinical decision making in patients with nsclc . methods study design the seer - medicare database is the result of a linkage of two population - based data sources : the surveillance , epidemiology and end results ( seer ) registry , sponsored by the us national cancer institute ( nci ) , and medicare , a federally funded us programme that hiv + ( n = 322 ) control ( n = 71 976 ) p value for more on seer see median age ( iqr ) 75 ( 6981 ) 75 ( 6981 ) stage i / ii stage iiia / iiib stage iv race white african american other comorbidities 2 or more median income in bottom two quartiles ( range in us dollars ) table : patient characteristics 3540% 2981% 3478% 20 016 22 793 29 167 7174% 2360% 466% 497% 870% 8634% 4317 ( 732 492 ) 62 859 6056 3061 6164 11 660 54 152 33 117 2781% 3167% 4050% 8733% 841% 425% 856% 1620% 7524% 4601 ( 732 492 ) 0002 048 004 099 < 00001 < 00001 072 002 00003 < 00001 065 pro vides health insurance for people of age 65 years and over , disabled , or have end - stage renal disease . 
the linkage to medicare provides longitudinal data for all claims from the center for medicare and medicaid services from the time of eligibility to death.24 , 25 patients younger than 65 years are excluded from this registry unless they are disabled or have end - stage renal disease . this study was approved by the institutional review board of the university of pennsylvania . study population we developed an analytic dataset from the seermedicare linked database , consisting of patients with a diagnosis of lung cancer ( icd - 9 code 162xx ) and nonsmall - cell histology ( adenocarcinoma , squamous cell carcinoma , large cell , bronchoalveolar carcinoma , or nsclc not otherwise speci ed ) contained in the seer registry who were diagnosed between jan 1 , 2000 , and dec 31 , 2005 . 
patients who were enrolled in medicare , but receive their bene ts through a third party , such as a health maintenance organisation , or private fee - forservice plan , were excluded from this analysis because of incomplete claims data in medicare for these patients . 
survival comparisons were also done after strati cation for disease stage . we used propensity score methods to account for imbalances between the two comparison groups on measured covariates.27 , 28 we chose propensity score adjustment in our cox model rather than traditional covariate adjustment , since recent ndings have suggested that this method is advantageous when analysing large observational datasets such as seer - medicare.29 our group has previously used this method to examine seer - medicare data.30 , 31 in an observational study such 1204 vol 13 december 2012 articles log - rank p = 037 hiv - infected control 95% ci for hiv patients 95% ci for controls log - rank p = 016 number at risk hiv - infected control 71 976 20 999 9615 4132 1225 20 016 13 006 6950 3205 log - rank p = 0051 log - rank p = 077 number at risk hiv - infected control 22 793 5313 time ( months ) 2007 29 167 2671 time ( months ) figure 1 : kaplan - meier comparative survival of hiv - infected and uninfected control nsclc patients : ( a ) all stages ; ( b ) stage i / ii ; ( c ) stage iiia / iiib ; and ( d ) stage iv as this one , covariate imbalances could potentially lead to biased survival estimates due to confounding . 
we calculated propensity scores using multivariable logistic regression with hiv infection as the outcome of interest , with adjustment for race , median income , stage , sex , and comorbidities . 
we then used multivariable cox proportional hazards models to compare death from any cause between the hiv - infected and control groups after adjustment for the propensity score as a continuous variable . 
to assess the proportional hazards assumption , we used the schoenfeld residuals test and complementary log - log plots . the kaplan - meier method was used to compare patients with stage i and ii disease with or without hiv infection who underwent de nitive surgical resection to assess the e ect of hiv infection in patients undergoing de nitive surgical resection for treatment of early stage nsclc . 
all statistical analyses were done with the statistical analysis system ( sas ) version 9.3. role of the funding source the sponsor did not have any role in study design , collection , analysis , or interpretation of the data , or in writing of this report . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results 322 patients were identi ed from jan 1 , 2000 , to dec 31 , 2005 , with a diagnosis of hiv ( hiv group ) and 71 976 individuals with a diagnosis of nsclc were identi ed who were not associated with a diagnosis of hiv ( control group )  . 
a similar proportion of patients were stage iiia / iiib and stage iv in both groups , but there was a signi cantly greater proportion of patients with stage i / ii disease in the hiv - infected group than the control group ( p = 0002 , table )  . 
there was a signi cant di erence in ethnic background between the two groups , with the hiv - infected group containing a higher proportion of african americans ( 236% vs 84% , p < 00001 )  . 
 the proportion of patients with their median income in vol 13 december 2012 1205 articles the bottom two quartiles was much the same between the two groups ( table )  . 
 the unadjusted median survival for uninfected control patients with nsclc was 70 months ( 95% ci 7070 ) com pared with 80 months ( 60100 ) for the hiv group ( p = 016 )  . 
when strati ed by stage , the unadjusted median survival for stage i / ii patients was 370 months ( 95% ci 360390 ) for uninfected controls compared with 430 months ( 260580 ) for the hiv group ( p = 037 ) , for those with stage iiia / iiib disease , it was 70 months ( 7070 ) for uninfected controls compared with 30 months ( 2080 ) for the hiv group ( p = 0051 ) , and for those with stage iv disease , it was 30 months ( 3030 for control group and 2050 for hiv group ) for un infected controls and the hiv group ( p = 077 ; gure 1 )  . 
after using propensity score adjustment to account for potential confounders , there remained no di erence in survival between uninfected controls and the hiv group across all stages ( hazard ratio 103 , 95% ci 091117 ) , stage i / ii ( 122 , 09316 ) , stage iiia / iiib ( 088 , 071109 ) , and stage iv ( 099 , 082121 )  . to examine the e ect of treatment on survival , we restricted our analysis to stage i and ii patients undergoing de nitive surgical resection alone , which is the standard of care.32 of the 114 hiv - infected patients with stage i or ii disease , 92 ( 807% ) underwent surgical resection . 
 the 5 - year survival was 47% for hiv - infected patients undergoing surgical resection versus 49% for the control group ( p = 088 )  . hiv - infected control 95% ci for hiv patients 95% ci for controls log - rank p = 088 discussion our results indicate that , across all stages , survival outcomes in hiv - infected patients with nsclc are not signi cantly di erent from uninfected patients . 
additionally , when assessing stage i / ii patients undergoing de nitive sur gical resection , survival was not signi cantly di erent in hivinfected patients undergoing surgery com pared with uninfected patients . 
taken together , these data suggest that nsclc does not display a more aggressive phenotype in hiv - infected patients . our ndings are in contrast to previously published reports that suggest that hiv - infected patients with lung cancer fare worse when compared with uninfected patients ( panel ) .17 , 18 notably , these previous studies included patients from the pre - haart era and spanned over three decades to identify adequate patient numbers . 
 these studies did not distinguish between nsclc and sclc , which have signi cantly di erent treatments and expected survival and as such cannot be grouped together for the purpose of examination of clinical outcome.1 , 2 , 33 a retrospective study by brock and colleagues18 examined the e ect of hiv infection across di erent stage subgroups in a combined cohort of sclc and nsclc and pre - haart and post - haart patients . 
although the authors did not note any signi cant di erence in stage - speci c survival , the overall survival of hivinfected patients with lung cancer was worse than hivindeterminate patients . 
their results may be due , in part , to the increased proportion of advanced stage patients ( iii and iv ) seen in the hiv - infected group relative to the hiv - indeterminate patients.18 in a report from the italian cooperative group on aids and tumors , spina and colleagues reported signi cantly poorer survival in 39 patients with hiv and lung cancer treated in the prehaart era ( 198697 ) than in matched controls ( median survival of 50 vs 100 months ; p < 00001 ) .34 , 35 a follow - up study36 com pared survival in hiv - infected patients with lung cancer from the pre - haart era to the haart era , demonstrating a signi cant improvement in survival ( from 38 to 70 months ; p = 001 )  . 
 although the exact reason for our observation is unclear , hiv - infected patients might have received regular medical care while on haart and therefore were diagnosed at an earlier stage . since the introduction of haart in 1996 , mortality from hiv / aids has decreased substantially . 
they further reported that this translated into an improvement in median survival of an hiv - infected patient in the haart era to 325 years from 76 years in the prehaart era.21 by contrast , the median survival of a patient with lung cancer across all stages is around 15 months.1 an analysis by persad and colleagues showed that 25% of all clinical trials for patients with nsclc and 29% of clinical trials for patients with sclc explicitly excluded patients with hiv.9 given the signi cant improvement in survival with hiv in the haart era , persad and coworkers argued for greater inclusion of patients with hiv in clinical trials across all cancers . there are several limitations to our analysis . 
although this study represents the largest study , to our knowledge , to date on the e ect of hiv on clinical outcome in nsclc , the number of hiv - infected patients identi ed is fairly small , leading to limited power to detect a small survival di erence . 
although there are data for the incidence of nsclc in patients with hiv , 16 there are limited data for the incidence of hiv in patients with nsclc , with reports ranging from 50 to 1800 hivinfected individuals per 100 000 patients with lung cancer.17 , 18 our data is concordant with these reports . 
although we restricted our analysis to patients treated between jan 1 , 2000 , and dec 31 , 2005 , when most hiv patients should have been receiving haart , we could not con rm that the patients included in our analysis were being treated with haart . 
a recent report assessing us trends in haart use showed widespread adoption of treatment during this period , with around 80% of hiv - infected therapy.40 seer - medicare patients on antiretroviral seer - medicare does not panel : research in context systematic review at the time that this study was designed , an increased incidence of nsclc in hiv - infected patients had been reported . 
before initiating our study , we searched the medical literature for comparative studies examining clinical outcome in hiv - infected lung cancer or hiv - infected patients with nsclc when compared with hiv - uninfected or indeterminate patients with lung cancer . 
we searched pubmed ( without any date or language restrictions ) using the following terms : hiv and survival and lung cancer , or hiv and survival and non - small cell lung cancer or hiv and lung cancer or hiv and non - small cell lung cancer and repeated these searches including the term antiretroviral therapy , highly active . 
we identi ed studies that had retrospectively examined the outcome of hiv - infected patients with lung cancer and reported this group to have poorer survival when compared to uninfected or hiv - indeterminate patients with lung cancer or historical benchmarks for survival . interpretation our data suggest that survival of hiv - infected patients with nsclc in the era of haart is comparable to hiv - uninfected patients with nsclc . 
haart regimens have previously been shown to interfere with the antineoplastic regimens that are routinely used in the treatment of lung cancer.23 the extent to which this interaction a ected the results seen in our study is unclear . 
the potential for drugdrug interactions must be taken into account when administering antineoplastic agents in patients with hiv / aids on haart.41 also , seer - medicare does not capture cd4 count data , a factor which has previously reported to correlate with survival in hiv - infected patients with lung cancer.19 seer - medicare does not capture in formation on the incidence of opportunistic infections or the administration of prophylactic regimens and therefore this is not included in this analysis . 
competing risks of death in hiv - infected patients with nsclc from opportunistic infec tions or complications from antineoplastic therapy , such as neutropenia , could not be quanti ed in our analysis . 
however , on the basis of our results , such an unmeasured confounder would have two to be signi cantly imbalanced between the vol 13 december 2012 1207 articles the hiv group comparison groups for to show signi cantly poorer survival than the uninfected controls.42 additionally , because the data in seer - medicare is mainly composed of people older than 65 years , we were unable to examine the e ect of hiv infection on survival in younger patients.1 notably , the median age of patients with hiv and lung cancer is generally reported to be younger than the average age of the lung cancer population.34 , 39 , 43 the clinical phenotype of lung cancer in younger patients with hiv could be distinct from that seen in patients over age 65 years . 
age has been shown to be an important prognostic factor for survival in lung can cer , with older patients faring more poorly.44 advanced age has also been shown to be an independent predictor of poor survival in hiv - infected patients initiating haart.45 however , since seer - medicare does not capture data for patients under the age of 65 years , whether the results reported in our trial are applicable to all hiv - infected patients with lung cancer is unclear . trials , where in conclusion , these data suggest that hiv infection alone in the era of haart should not play a role in clinical decision making in treatment of patients with nsclc . 
notably , the intergroupe francophone de cancerologie thoracique has recently initiated a phase 2 , multicentre prospective study evaluating the combination of pemetrexed plus carboplatin in hivpositive patients with lung cancer and accrual to this ( clinicaltrials.gov , number nct01296113 )  . 
additionally , these data suggest that improving access to modern diagnostic imaging and cancer therapies are likely to signi cantly bene t patients with nsclc with hiv since their outcome is similar to that of uninfected controls when treated with de nitive surgical resection . 
the clinical management of the hiv - infected patient with nsclc , as with all patients with lung cancer , requires a multidisciplinary approach to individualise and optimise therapy and to manage toxicities . is ongoing trial contributors rr , nm , kl , and av were responsible for the study concept and design . 
 lancet oncol 2012 ; 13 : 559 the second sentence of the third paragraph of this editorial should read in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
pixantrone dimaleate versus other chemotherapeutic agents as a singleagent salvage treatment in patients with relapsed or refractory aggressive non - hodgkin lymphoma : a phase 3 , multicentre , open - label , randomised trial . 
this correction has been made to the online version as of june 29 , 2012 , and the printed article is correct . vol 13 july 2012 e285 articles conjugated equine oestrogen and breast cancer incidence and mortality in postmenopausal women with hysterectomy : extended follow - up of the womens health initiative randomised placebo - controlled trial garnet l anderson , rowan t chlebowski , aaron k aragaki , lewis h kuller , joann e manson , margery gass , elizabeth bluhm , stephanie connelly , f allan hubbell , dorothy lane , lisa martin , judith ockene , thomas rohan , robert schenken , jean wactawski - wende summary background by contrast with many observational studies , women in the womens health initiative ( whi ) trial who were randomly allocated to receive oestrogen alone had a lower incidence of invasive breast cancer than did those who received placebo . 
we aimed to assess the in uence of oestrogen use on longer term breast cancer incidence and mortality in extended follow - up of this cohort . methods between 1993 and 1998 , the whi enrolled 10 739 postmenopausal women from 40 us clinical centres into a randomised , double - masked , placebo - controlled trial . 
women aged 5079 years who had undergone hysterectomy and had expected 3 - year survival and mammography clearance were randomly allocated by a computerised , permuted block algorithm , strati ed by age group and centre , to receive oral conjugated equine oestrogen ( 0625 mg per day ; n = 5310 ) or matched placebo ( n = 5429 )  . 
using data from this extended follow - up ( to aug 14 , 2009 ) , we assessed long - term e ects of oestrogen use on invasive breast cancer incidence , tumour characteristics , and mortality . 
in subgroup analyses , we noted breast cancer risk reduction with oestrogen use was concentrated in women without benign breast disease ( p = 001 ) or a family history of breast cancer ( p = 002 )  . 
in the oestrogen group , fewer women died from breast cancer ( six deaths , 0009% per year ) compared with controls ( 16 deaths , 0024% per year ; hr 037 , 95% ci 013091 ; p = 003 )  . 
fewer women in the oestrogen group died from any cause after a breast cancer diagnosis ( 30 deaths , 0046% per year ) than did controls ( 50 deaths , 0076% ; hr 062 , 95% ci 039097 ; p = 004 )  . interpretation our ndings provide reassurance for women with hysterectomy seeking relief of climacteric symptoms in terms of the e ects of oestrogen use for about 5 years on breast cancer incidence and mortality . 
however , our data do not support use of oestrogen for breast cancer risk reduction because any noted bene t probably does not apply to populations at increased risk of such cancer . funding us national heart , lung , and blood institute ; wyeth . introduction elevated concentrations of endogenous oestrogen have been consistently associated with increased risk of breast cancer.1 exogenous oestrogen use has also been associated with higher breast cancer incidence in many25 but not all6 , 7 observational studies , especially in leaner women35 , 8 and those receiving oestrogen long term.4 , 5 , 8 , 9 oestrogen use has been linked to hormone - receptor positive and early stage disease , 3 , 5 suggesting a better prognosis , 10 although associations with breast cancer mortality are mixed.2 , 9 , 1017 during the intervention phase of the womens health initiative ( whi ) randomised trial17 of 10 739 post menopausal women who had undergone hysterectomy , a nonsigni cant reduction in incidence of breast cancer was noted after receipt of conjugated equine oestrogens compared with placebo ( hazard ratio [ hr ] 079 , 95% ci 061102 )  . 
after trial intervention was stopped in february , 2004 , because of an increased incidence of stroke , 18 follow - up continued until planned termination in 2005 and every year thereafter for participants who consented to extended surveillance . 
the reduced breast cancer risk in the oestrogen group persisted and reached statistical signi cance ( hr 077 , 95% ci 062095 ) .19 we aim to provide additional details about the e ects of oestrogen use on invasive breast cancer incidence during and after intervention with regard to tumour characteristics and previously identi ed e ect modi ers . 
we also present results for breast cancer - related mortality . methods study design and participants postmeno pausal women aged 5079 years who had under gone a hysterectomy were recruited into the whi randomised , double - masked , placebo - controlled trial at 40 clinical centres in the usa between 1993 and 1998 . 
eligible women were randomly allocated in a one - to - one ratio to receive oral conjugated equine oestrogen ( 0625 mg per day ) or matched placebo through use of a computerised , permuted - block algorithm , strati ed by age group and centre . 
details of study design , eligibility , and implementation have been published elsewhere.18 , 19 data collection participants previous hormone use was ascertained at baseline by an interviewer - administered questionnaire . 
adherence to study drug was assessed primarily by pill counts or weighing returned bottles ; self - report was used only rarely . until 2005 , participants vital and health status was assessed twice every year and mammography was done once per year throughout the trial . 
when the intervention ended on feb 29 , 2004 , after a mean follow - up of 71 ( sd 16 ) years , all participants were unmasked and asked to stop taking the study drug . 
during study close - out , end 7645 participants ( 78% of 9786 living participants in active follow - up at that time ; 3778 [ 779% ] of 4851 women allocated to oestrogen and 3867 [ 784% ] of 4935 allocated to placebo ) consented to extended follow - up.19 from 2005 , vital and health status updates have been obtained once per year . 
this report presents data until aug 14 , 2009 , after an overall median follow - up of 118 years ( iqr 91129 )  . breast cancers were documented by medical and pathological record review by centrally trained doctor adjudicators . 
tumour characteristics were coded at the whi clinical coordinating center according to surveillance , epidemiology , and end results ( seer ) guidelines.20 deaths were documented with death certi cates and medical records . 
all adjudicators were masked to randomisation assignment . intervention phase the post - intervention phase statistical analysis we compared incidence of breast cancer by treatment group with failure - time methods and the intention - totreat principle . 
we did analyses for three time phases : ( from randomisation until the feb 29 , 2004 ) ; ( from march 1 , 2004 , until the data cuto on aug 14 , 2009 ) ; and overall results . 
event times during the intervention phase were censored at date of death , last follow - up , or termination of the intervention phase ( feb 29 , 2004 ) , whichever occurred rst . 
participants were included in post - intervention phase incidence analyses if they were alive , in follow - up , and had not developed breast cancer by march 1 , 2004 . 
we compared slopes for each phase with wald tests . we examined the in uence of non - adherence to protocol - assigned censoring events treatment by 6 months after participants rst became non - adherent ( ie , took < 80% of study drugs or started non - study hormone therapy )  . 
some categories do not add up to total number of women who consented to extended follow - up due to missing data . table 1 : baseline characteristics of participants in the womens health initiative trial of conjugated equine oestrogen who consented to extended follow - up in secondary analyses , we tested interactions between randomisation assignment and 16 baseline charac teristics within the primary cox model , expanded to include the designated baseline factor , randomisation assignment , and interaction term ( s )  . 
we omitted partici pants with missing estimated probability of continued adherence , in the proportional - hazards models to adjust for changes in the distribution of sample characteristics during follow - up.21 478 vol 13 may 2012 articles vol 13 may 2012 values from the corresponding analysis . 
no adjustment for multiple testing was made ; at most , one interaction was expected to be signi cant by chance alone . all analyses were done with sas version 9.1.3 and gures were drawn with r 2.11. 
decisions about study design , data collection and analysis , result interpretation , manuscript preparation , and the decision to submit the manuscript for publication resided with committees comprised of whi investigators that included nhlbi representatives . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results baseline breast cancer risk factors in women who consented to extended follow - up were much the same as those of the original cohort18 and much the same between randomised groups , apart from a small imbalance in bilateral oophorectomy and benign breast disease ( table 1 )  . 
during the intervention phase , 8090% of par ticipants had mammograms every year with equivalent frequencies treatment groups.17 , 22 3894 ( 812% ) of 4794 of women in the oestrogen group and 3965 ( 813% ) of 4877 controls had at least one mammogram after the trial intervention was stopped . two the oestrogen placebo hr 077 ( 95% ci 062095 ) p = 002 hr 068 ( 95% ci 049095 ) p = 002 articles 0045 0030 0015 number at risk oestrogen placebo 5310 5429 time since randomisation ( years ) time since randomisation ( years ) 5166 5280 5007 5106 4840 4915 4261 4301 3620 3678 1696 1771 5310 5429 3513 3752 2752 2883 1862 1937 1506 1571 1270 1355 figure 1 : kaplan - meier estimates of cumulative hazards of invasive breast cancer in the whi randomised trial of conjugated equine oestrogen with the intention - to - treat principle ( a ) and with adjustments for adherence ( b ) background shading shows the distribution of the duration of intervention ( in quintiles )  . 
by that time , 57% of 5310 women in the oestrogen group and 91% of 5429 controls had started hormones provided by their health - care providers.18 of 7472 participants in extended follow - up with available data , 604 ( 81% ) reported use of hormones after intervention , with slightly more in the oestrogen group than the placebo group ( 334 [ 90% ] of 3699 in the oestrogen group vs 270 [ 72% ] of 3773 controls ; p = 0003 )  . in the intention - to - treat analyses , data were available for a median follow - up of 72 years ( iqr 6481 ) from randomisation until early termination of the trial intervention , a median follow - up of 47 years ( 3551 ) after intervention , and a median of 118 years ( 91129 ) follow - up overall . 
in these analyses , use of oestrogen was associated with lower overall invasive breast cancer incidence ( 151 events , 027% per year ) compared with placebo ( 199 events , 035% per year ; hr 077 , 95% ci 062095 ; p = 002 ; 19 table 2 , gure 1 ) , with no di erence between intervention and post - intervention hazard ratios ( pinteraction = 076 )  . 
we noted non - signi cant increasing trends in oestrogen hrs by time since randomisation ( pslope = 019 ) and by time since trial cessation ( pslope = 032 )  . median duration of study drug use was 59 years ( iqr 2573 ) and median time to non - adherence ( ie , taking < 80% of study pills or starting other hormone therapy ) was 35 years ( 1565 )  . 
sensitivity analyses adjusting for non - adherence yielded a stronger association between oestrogen use and lower breast cancer risk overall ( hr 068 , 95% ci 049095 ; gure 1 ) , which seemed even higher when restricted to the intervention period ( 058 , 039084 )  . in analyses of tumour characteristics ( table 2 ) , oestrogen use was associated with a reduced risk of in ltrating ductal carcinoma ( hr 067 , 95% ci 051088 ) compared with placebo but not in ltrating lobular cancers ; however , the test for heterogeneity was not signi cant ( p = 033 )  . 
 482 vol 13 may 2012 025 050 100 200 favours oestrogen favours placebo articles ratios for hormone receptor - positive tumours and hormone receptor - negative tumours were much the same . 
we noted a reduced risk for her2 - negative tumours ( 074 , 056097 ) but not her2 - positive tumours ( 150 , 079283 ) in women who received oestrogen compared with placebo ( pheterogeneity = 0045 ) , although missing her2 data were common . 
compared with placebo , we noted fewer small and node - negative tumours but no reduction in the number of large tumours ( 2 cm ) or node - positive tumours in the oestrogen group , but comparisons between subtypes did not reach signi cance . in analyses starting at randomisation ( table 2 and gure 2 ) , fewer women diagnosed with breast cancer died in the oestrogen group ( 30 deaths , 0046% per year ) compared with the placebo group ( 50 deaths , 0076% per year ; hr 062 , 95% ci 039097 ; p = 004 )  . 
of these deaths , six were directly attributed to breast cancer in the oestrogen group ( 0009% per year ) compared with 16 in the placebo group ( 0024% per year ; 037 , 013091 ; p = 003 )  . subgroup analyses provided a mostly consistent pattern of lower breast cancer incidence with oestrogen use ( gure 3 )  . 
of 16 interactions tested , two were nominally statistically signi cant : history of benign breast disease ( p = 001 ) and rst degree family history of breast cancer ( p = 002 )  . 
no interactions were reported with age ( p = 098 ) , body - mass index ( p = 049 ) , gail model risk score ( p = 022 ) , oophorectomy status ( p = 055 ) , years since menopause onset ( p = 068 ) , previous oestrogen use ( p = 095 ) , or vasomotor symptoms ( p = 074 )  . of women who rst used hormone therapy 5 years or more after menopause ( ie , gap time 5 years ) , the estimated e ect of oestrogen ( hr 065 , 95% ci 048089 ) seemed lower than that for women who started hormone therapy sooner after menopause ( 089 , 066120 ) but the interaction was not signi cant ( p = 013 )  . after discontinuation discussion use of oestrogen for a median of 59 years in postmenopausal women with hysterectomy in the whi randomised trial was associated with a signi cant reduction in incidence of invasive breast cancer , a reduction that continued for the median 47 years of follow - up intervention . 
potential e ect modi cation with benign breast disease ( p = 001 ) and family history of breast cancer ( p = 002 ) suggests that these reductions might not apply to women at increased risk . 
we noted a signi cant reduction in breast cancer - related mortality and all - cause mortality after breast cancer diagnosis with oestrogen use , but the number of such deaths was small . although many observational studies have reported an increased risk of breast cancer with oestrogen use , 25 some have reported lower risks.6 , 23 in previous studies reporting an adverse e ect of such therapy on breast cancer , most25 , 8 but not all , 5 , 9 showed an increased risk of breast cancer only after prolonged ( > 5 years ) oestrogen use . 
in this trial , with substantial variation in exposure length ( median duration of the intervention 59 years [ range < 110 years ] ; median adherent time 35 years ; and 2291 [ 21% ] of 10 739 partici pants reporting previous oestrogen use for > 5 years at baseline ) , we noted no time - trends in terms of duration of use or time since cessation and no interactions with previous oestrogen use , although the power for interaction tests was low ( panel )  . 
the continued , postintervention e ect of oestrogen on breast cancer incidence is akin to that reported for other hormone - targeted drugs shown to reduce breast cancer incidence.33 , 34 panel : research in context systematic review conjugated equine oestrogen was approved for management of climacteric symptoms in several countries in the early 1940s . 
by the 1990s , about 40% of postmenopausal women in the usa and uk were receiving hormone therapy ( oestrogen alone or oestrogen plus progesterone ) .2426 however , the risks and bene ts of this commonly used therapy had never been established in a clinical trial setting . 
against this background , scientists at the us national institutes of health , working in conjunction with experts in a number of disciplines , developed the womens health initiative ( whi ) hormone therapy programme to meet this unmet need with potential implications for a large number of postmenopausal women in the usa and around the world.27 the whi hormone therapy programme consisted of two full - scale randomised , placebo - controlled clinical trials to separately assess the e ect of oestrogen alone and oestrogen plus progesterone on chronic disease in postmenopausal women with and without previous hysterectomy , respectively , at 40 clinical sites in the usa . 
when the whi trials were developed , observational study evidence suggested that oestrogen , alone or with progesterone , would modestly increase breast cancer risks25 but the cancers would have a favourable prognosis.35 the results from the whi randomised , placebo - controlled trial of oestrogen alone contradicts most previous observational studies in that oestrogen use was associated with reduced breast cancer incidence and reduced breast cancer - associated mortality . 
 previous e orts to reconcile these results have pointed to the issue of timing of rst hormone therapy.28 , 29 additionally , some of the di erences between previous observational studies and the present randomised clinical trial results might re ect variation in mammography frequency in observational study populations . 
the whi oestrogen - alone ndings also di er from those seen in the whi randomised trial assessing oestrogen plus progesterone in women without previous hysterectomy in which combined hormone therapy signi cantly increased breast cancer incidence and breast cancer mortality.3032 interpretation our ndings provide reassuring evidence about breast safety of oestrogen use for climacteric symptom management in postmenopausal women with hysterectomy for durations consistent with those reported in this trial . 
although a reduced risk of breast cancer incidence and mortality was noted in recipients of oestrogen , these ndings do not support its use for breast cancer risk reduction in light of the lack of bene t for populations at higher risk , the adverse e ects on stroke and venous thromboembolism , 18 and the increased risk reduction available with other drugs . vol 13 may 2012 oestrogen and progesterone placebo ( in combined arm ) hr 125 ( 95% ci 107146 ) oestrogen alone placebo ( in oestrogen - alone arm ) hr 077 ( 95% ci 062095 ) articles 005 004 003 002 001 time since randomisation ( years ) number at risk combined arm oestrogen and progesterone placebo oestrogen - alone arm oestrogen alone placebo 8506 8102 5310 5429 8329 7914 5166 5280 8109 7721 5007 5106 7796 7466 4840 4915 7009 6692 4261 4301 6189 5889 3620 3678 2914 2648 1696 1771 figure 4 : cumulative hazards , adjusted for age and ethnic group , of invasive breast cancer by random allocation in the whi trials of conjugated equine oestrogen alone and conjugated equine oestrogen plus medroxyprogesterone acetate trials derived from chlebowski and colleagues32 hr = hazard ratio . many observational studies report increased breast cancer risk with oestrogen alone in normal weight but not overweight or obese women.4 , 5 , 8 we noted no e ect modi cation with body - mass index ; oestrogen hazard ratios were less than one in normal weight , overweight , and obese women . use of mammography is a potential source of confounding in observational studies.35 in clinical practice , women who take hormone therapy have mammograms more regularly than untreated women36 and screened populations have an increased rate of breast cancer detection , 37 , 38 potentially explaining the increased breast cancer risk in oestrogen users noted in previous studies that did not assess screening . 
controlling for ongoing screening in observational studies is unusual and not straightforward because it depends on adequate data collection and modelling , and the assumption that mammography use is not an intermediate variable of exposure and disease.39 , 40 detection bias is an unlikely explanation for our results . 
 mammography rates were protocol - de ned and very similar between randomisation groups.17 , 22 further more , little e ect on breast density41 oestrogen use has or detection of breast cancer.22 finally , the signi cant reduction in breast cancer mortality reported with oestrogen use provides strong evidence against the possibility that the risk reduction noted was an artifact of oestrogen e ects on screening , 40 because a delay in detection would be expected to increase mortality . favourable e ects of use of oestrogen alone on breast cancer survival , measured from cancer diagnosis , have been seen in some1012 but not all2 , 7 , 1316 reports . 
studies of mostly oestrogen alone use on breast cancer mortality , measured from start of hormone therapy have provided mixed results with favourable , 1012 neutral , 1315 and unfavourable2 , 7 associations reported . 
our results , measured from randomisation ( although still imprecise ) provide important new evidence that oestrogen use for about 5 years reduces breast cancer mortality , supporting a favourable association with breast cancer incidence . a reduction in breast cancer incidence with conjugated equine oestrogen is biologically plausible . 
although such oestrogen is a recognised mitogen that usually stimulates mammary cell proliferation and inhibits apoptosis through activation of the oestrogen receptor , 1 both preclinical4246 and clinical45 ndings suggest that after long - term oestrogen deprivation , adaptive changes in mammary tumour gene expression pro les render tumours paradoxically susceptible to oestrogen - induced apoptosis.43 , 44 although the mechanisms are complex and not wholly understood , 46 preclinical studies suggest involvement of the fas / fas l extrinsic ( receptor - mediated ) death regulatory pathway47 and the intrinsic ( mitochondrial ) apoptotic pathway , mediated through increased expression of several proapoptotic proteins including p53 - unregulated modulator of apoptosis.48 , 49 e orts to reconcile the original ndings of this trial17 with observational study results suggested that the time from menopause to rst hormone use ( gap time ) is a potential modulator of hormone therapys in uence on breast cancer risk.28 in the parallel whi randomised clinical trial29 and the observational million women study , 5 women starting oestrogen plus progesterone use with a short gap time were at increased breast cancer risk . 
for use of oestrogen alone , the million women study investigators reported no increased incidence in breast cancer with oestrogen use starting 5 years or more from menopause but an increased risk with a shorter gap time.5 in these analyses , oestrogen hazard ratios were lower than 1 for early initiation ( gap time < 5 years ) and late initiation ( 5 years )  . 
we noted a somewhat greater in women starting in uence oestrogen therapy 5 years or more after meno pause , but the interaction with gap time was not statistically signi cant . 484 vol 13 may 2012 articles although breast cancer incidence and related mortality were lower for women who took oestrogen alone than for controls , our ndings do not support oestrogen use for breast cancer risk reduction because subgroup analyses suggest the bene t might not apply to populations at increased breast cancer risk . 
additionally , other hormonetargeted drugs have a substantially greater in uence on breast cancer than does oestrogen.33 , 34 , 50 , 51 however , our ndings , together with a relatively balanced riskbene t pro le for clinical events , 18 , 52 provide reassurance about breast cancer safety for postmenopausal women with previous hysterectomy who receive unopposed oestrogen to reduce climacteric symptoms for durations equivalent to those reported in this trial . tamoxifen , raloxifene , and exemestane all provide greater breast cancer risk reduction than oestrogen , but have important limitations . 
the selective oestrogen receptor modulators tamoxifen and raloxifene reduce risk of breast cancer and fractures but increase climacteric symptoms and have adverse e ects on stroke , blood clots , and endometrial cancer , leading to an unfavourable riskbene t pro le in most postmenopausal women.33 , 53 exemestane , an aromatase lowers oestro gen concentrations , also substantially reduces breast cancer risk.34 however , aromatase inhibitors cause bone loss and increase climacteric symptoms and arthralgias , 54 exerting a greater in uence when started soon after menopause.55 the mechanisms through which exogenous oestrogens , tamoxifen , raloxifene , and aromatase inhibitors all reduce breast cancer risk are not known but clearly warrant further study . inhibitor that and study strengths include the randomised , doublemasked , placebo - controlled prospective design with breast cancer as the designated primary safety outcome , a large sample size , high - quality outcomes ascertainment , protocol - required mammography throughout most of the follow - up period . 
however , any bias arising from poor adherence would probably dilute the di erences between random isation groups over the duration of follow - up , as the adherence - adjusted analyses con rmed . 
small numbers of breast cancer deaths , some attrition associated with re - consenting for extended follow - up , and a median of only 47 years of post - intervention follow - up should also be noted . 
the trial assessed only one dose and schedule of oral conjugated equine oestrogens ; whether these ndings apply to lower doses , other oestrogen preparations , or longer durations of use is not known . major di erences exist in whi trial ndings between oestrogen only therapy in women with previous hysterectomy and those of the parallel whi randomised trial of oestrogen plus medroxyprogesterone acetate in women with an intact uterus . 
whereas oestrogen - alone treatment was associated with reduced breast cancer incidence and reduced breast cancer mortality , combined hormone therapy increased breast cancer incidence , 29 , 52 delayed breast cancer diagnosis , 56 and increased breast cancer mortality.48 the biological basis for this di erence is unknown . 
the comparability of breast cancer incidence rates for the placebo groups in the two trials ( gure 4 ) suggests that di erences in hormone therapy , rather than hysterectomy , is the primary determinant . 
 changes in the serum proteome in response to oestrogen and combined hormone therapies are generally quite similar but di erences have been identi ed that could in uence breast cancer risk , including those in notch2 and some igf binding proteins.57 contributors gla , rtc , and aka conceived the study design . 
gla and aka had full access to the data . con icts of interest rtc has been a consultant for astrazeneca , novartis , amgen , and p zer , received funding support from amgen , and served on speakers bureaus for astrazeneca and novartis . 
all other authors declare that they have no con icts of interest . acknowledgments the womens health initiative program is funded by the us national heart , lung , and blood institute , national institutes of health , and department of health and human services through contracts n01wh22110 , 24152 , 32100 - 2 , 32105 - 6 , 32108 - 9 , 32111 - 13 , 32115 , 32118 - 32119 , 32122 , 42107 - 26 , 42129 - 32 , and 44221 . articles cognitive behavioural treatment for women who have menopausal symptoms after breast cancer treatment ( menos 1 ) : a randomised controlled trial eleanor mann , melanie j smith , jennifer hellier , janet a balabanovic , hisham hamed , elizabeth a grunfeld , myra s hunter summary background hot ushes and night sweats ( hfns ) a ect 6585% of women after breast cancer treatment ; they are distressing , causing sleep problems and decreased quality of life . 
we investigated whether cognitive behavioural therapy ( cbt ) can help breast cancer survivors to e ectively manage hfns . methods in this randomised controlled trial , we recruited women from breast clinics in london , uk , who had problematic hfns ( minimum ten problematic episodes a week ) after breast - cancer treatment . 
randomisation was done in blocks of 1220 participants , stratifying by age ( younger than 50 years , 50 years or older ) , and was done with a computergenerated sequence . 
group cbt comprised one 90 min session a week for 6 weeks , and included psycho - education , paced breathing , and cognitive and behavioural strategies to manage hfns . 
the trial is registered , isrctn13771934 , and was closed march 15 , 2011 . findings between may 5 , 2009 , and aug 27 , 2010 , 96 women were randomly allocated to group cbt ( n = 47 ) or usual care ( n = 49 )  . 
group cbt signi cantly reduced hfns problem rating at 9 weeks after randomisation compared with usual care ( mean di erence 167 , 95% ci 243 to 091 ; p < 00001 ) and improvements were maintained at 26 weeks ( mean di erence 176 , 254 to 099 ; p < 00001 )  . 
we recorded no cbt - related adverse events . interpretation group cbt seems to be a safe and e ective treatment for women who have problematic hfns after breast cancer treatment with additional bene ts to mood , sleep , and quality of life . 
hfns are more severe in this population than they are in healthy women and have a negative e ect on quality of life , mood , and sleep.24 chemotherapy or adjuvant endocrine treatments can compromise or lead to failure of ovarian function , resulting in rapid reduction of oestrogen concentrations , which induces or exacerbates hfns . 
 hfns can in turn reduce adherence to endocrine therapy if left untreated.57 hormone replacement is an e ective treatment for hfns , but is generally contraindicated for patients with breast cancer because it can increase the risk of breast cancer recurrence , and hfns can return in women who discontinue hormone replacement therapy ( ssris ) , and therapy.8 a cochrane review of non - hormonal medical treatments concluded that clonidine ( an antihypertensive drug ) , gabapentin ( an anticonvulsant that works through an unknown mechanism ) , selective serotonin reuptake inhibitors serotonin - norepinephrine reuptake inhibitors ( snris ) showed a mild to moderate e ect on the frequency of hfns in women with a history of breast cancer ( reductions of between 15% and 58% ; average 37% ) .9 three trials done since the review was undertaken recorded similar reductions.1012 various side - e ects of medical treatments were reportedeg , dry mouth , sleep problems , and nauseaand short follow - up long - term conclusions outcomes.9 some ssris ( paroxetine and uoxetine ) , but not all , might reduce the e ectiveness of endocrine treatments.13 evidence of improvements to quality of life is mixed ; six of 12 studies of non - hormonal drugs reported no e ect.1012 , 14 moreover , many breast cancer survivors prefer treat ments.3 therapieseg , vitamins , for non - pharmacological magnetic devices , or acupuncturethe cochrane review to use non - medical limited about vol 13 march 2012 articles for the trial protocol see 2407 / 11 / 44 concluded that outcomes were either inconsistent or not statistically signi cant.9 consequently , a need exists for safe , acceptable , and e ective non - hormonal treatments that are free from side - e ects to help these women to manage hfns.15 , 16 an intervention based on cognitive behavioural therapy ( cbt ) has been developed , 17 including psychoeducation , paced breathing and relaxation , and cbt to help women to manage hfns . 
this intervention has been shown to be acceptable to women and has shown promise in exploratory trials of one - to - one and group cbt.17 , 18 the treatment is based on a model of the hypothesised causal mechanisms and maintaining factors of hfns , which include anxiety , stress , embarrassment , negative beliefs , catastrophic thoughts , and avoidance behaviours.19 , 20 in a pilot , uncontrolled trial of group cbt , 17 women who had been treated for breast cancer reported an average 49% reduction in hfns problem rating and a 38% reduction in self - reported hfns frequency.18 hfns frequency has generally been considered to be the target of treatments , but studies have suggested that problem rating ( ie , the extent to which hfns are bothersome and interfere with life ) should be the primary outcome in clinical trials because it is associated with help - seeking behaviour and quality of life to a greater extent than is frequency of hfns.21 , 22 sternal skin conductance ( ssc ) monitoring is the most valid physiological measure of hfns , but is rarely included in trials . 
subjective and physiological measures assess di erent aspects of hfns.23 menos 1 is a randomised controlled trial of group cbt compared with usual care with a 26 - week follow - up . 
we hypothesised that participants would report less problematic hfns and fewer hfns , improved mood , sleep , and health - related quality of life after group cbt compared with individuals who received usual care . 
we measured subjective frequency and problem rating of hfns and ssc monitoring of hfns frequency , to establish whether the treatment a ects physiological or psychological factors , or both . methods study design and participants the study design is described in detail in the trial protocol.20 brie y , recruitment took place between march 17 , 2009 , and aug 27 , 2010 . 
 they could also apply for inclusion by responding to lea ets and posters displayed in clinics . english - speaking women older than 18 years were eligible if they had had at least ten problematic hfns per week ( con rmed by a 2 - week diary and a screening interview ) for a duration of 2 months or more , had completed medical treatment for breast cancer ( surgery , radiotherapy , or chemotherapy ) , and had no evidence of other cancers or metastases . 
because many women use treatments for hfns but still have troublesome symptoms and seek further treatment , they were not excluded if they had been using the treatment consistently for 2 months or more , and planned to continue at the same dose during the trial . 
after base line assessment and receipt of consent from 1220 par ticipants , the trial clinical psychologist ( mjs ) sent participants identi cation details to a programmer at the clinical trials unit at kings college london , uk , for randomisation . 
the programmer created a computer - generated random isation sequence , allocating participants in a one - to - one ratio , strati ed by age ( < 50 years , 50 years ) , with randomly varying block size . 
 speci cally , at 9 - week and 26 - week assessments , women were met by a separate researcher who collected questionnaires and who also asked the women not to disclose their treatment allocation to the researcher who did the outcome assessments . 
to check whether the trial coordinator ( em ) was successfully masked , after 9 - week assessments for each cohort she noted which group she thought participants had been allocated to . 
the trial statistician was masked to group identity until analyses were complete . procedures assessments took place at baseline , 9 weeks after randomisation ( typically 2 weeks after treatment ) , and 26 weeks after randomisation . 
about 2 weeks before participants attended a baseline assessment , a researcher explained the study , assessed eligibility by telephone , and posted written information and a 2 - week diary to be updated on a daily basis to record hfns frequency . 
at baseline assessment , eligibility was con rmed ; participants were able to ask questions before signing a standard consent for women were asked about their breast cancer treatment history , menopause symptoms , and medical history . 
they completed a questionnaire covering 310 vol 13 march 2012 articles demographic characteristics and baseline measures and were given a small ssc monitor and a magnetic event marker bracelet worn for 24 h . 
they were asked to indicate when they had an hfns by passing the magnet over the monitor ; they were encouraged to do usual activities and were shown how to remove the monitor to shower or bathe . participants allocated to receive group cbt attended a 90 min session every week for 6 weeks , between june , 2009 , and october , 2010 ( panel 1 )  . 
all sessions were audio taped , then 10% were randomly selected ( with a computer - generated random number sequence ) and a psychologist ( msh ) experienced in cognitive behavioural therapy for hfns , rated them for adherence to the treatment manual , by indicating on coding sheets the extent to which the group leader covered each topic . 
coding sheets included speci c components of the intervention ( eg , reviewing home work , providing information about the role of stress , demonstrating paced breathing in the session , group discussion of behaviours relating to hfns ) developed for the trial ( appendix )  . all participants received usual carethey had access to clinical specialists and cancer support services , either through routine follow - up appointments or as part of a breast cancer survivorship programme in southeast london ( panel 1 )  . 
 at 26 weeks after randomisation , questionnaires were sent containing the same measures ; face to face or telephone interviews were done by an independent psychologist after nal measures were completed to obtain womens responses to being in the trial and their views about the treatment ( for those in the cbt group )  . 
follow - up was completed by march 15 , 2011 . outcomes the primary outcome was the hfns problem rating ( hot ush rating scale24 ) at 9 weeks after randomisation . 
 problem ratingie , the extent to which symptoms are bothersome and interfere with lifewas chosen , before the trial began , 20 as the primary outcome measure because problem rating , rather than frequency , is associated with help - seeking and quality of life , and it has been recommended as the most appropriate patientreported outcome measure in clinical trials of hfns panel 1 : intervention content group cognitive behavioural therapy ( cbt ) the group cbt was psycho - educational , structured , and interactive with presentations , group discussion , handouts , and weekly homework . 
paced breathing and relaxation were practised at each session and participants were given a relaxation and paced breathing audio cd to practise at home daily and during hot ushes and night sweats ( hfns )  . 
 women recorded their hfns in weekly diaries . session one introduced the cognitive behavioural model including physiological , cognitive , behavioural , and emotional components of hfns ; provided information about the physiology of hfns ; and introduced paced breathing . 
participants described their experiences of hfns in the context of breast cancer , outlined their goals for treatment , discussed and recorded particular triggers of hot ushes , and practised relaxation . session two focused on the role of stress in potentiating hfns and cbt strategies for the reduction of stress and anxiety . 
paced breathing was introduced and practised as homework . session three focused on cognitive ( eg , catastrophic thinking and overly negative beliefs about hot ushes ) and behavioural reactions ( eg , avoidance of activities ) to hot ushes . 
they also completed sleep diaries in preparation for the sleep sessions . session four focused on understanding night sweats and improving sleep habits and the application of behavioural strategies to reduce wakefulness after night sweats . 
 participants identi ed ways in which they could change sleep habits , which they implemented as homework . session ve focused on the cognitive component of sleep problems , including sleep - related anxieties or general worries leading to further wakefulness . 
cbt strategies were developed for the management of night sweats . session six was a review session and participants made action plans to maintain cognitive and behavioural changes , including dealing with setbacks . usual care all women had completed active breast cancer treatment and were typically followed up every 6 months by an oncologist or clinical nurse specialist , with additional appointments as needed . 
women were sent an information lea et produced by breast cancer care and o ered telephoned support every 2 weeks ( average seven telephone calls , maximum ten )  . 
the remainder were no longer attending follow - up appointments at the hospital ( n = 7 ) , or were not treated at hospitals in the southeast london cancer network ( n = 12 )  . 
therefore , individuals in the usual care group received information and had access to high quality support services . see online for appendix treatments.21 , 22 problem rating and severity tend to be associated with each otherneither are strongly associated with frequency of hfns.21 secondary outcomes included hfns problem rating at 26 weeks , and hfns frequency , mood , and healthrelated quality - of - life measures at 9 weeks and 26 weeks after randomisation . 
problem rating of hfns ( hot ush rating scale24 ) was calculated as the mean of three 10 - point items that assess the extent to which symptoms vol 13 march 2012 5 chose not to participate mean body - mass index ( kg / m ; sd ) 2713 ( 530 ) 2751 ( 690 ) articles 278 screened for eligibility 177 excluded 79 not meeting inclusion criteria 18 symptoms not problematic 5 cancers had metastasised 8 unable to attend cbt sessions 20 lived too far away 19 never had breast cancer 1 died 8 undergoing cancer treatment 98 chose not to participate 101 consented to take part and completed baseline assessment 96 randomly allocated to treatment 47 cognitive behavioural therapy 6 in cohort one 9 in cohort two 7 in cohort three 7 in cohort four 6 in cohort ve 6 in cohort six 6 in cohort seven 49 usual care 5 in cohort one 10 in cohort two 7 in cohort three 7 in cohort four 6 in cohort ve 7 in cohort six 7 in cohort seven 1 unable to attend 1 ill health 1 symptoms ceased 1 chose not to participate 1 chose not to participate 1 died 2 could not be contacted at week 9 43 completed hfrs at week 9 45 completed hfrs at week 9 40 completed hfrs at week 26 40 completed hfrs at week 26 43 analysed 45 analysed figure 1 : trial pro le cbt = cognitive behavioural therapy . 
a di erence of two points or more is regarded as clinically relevant.17 , 18 , 25 the scale has good internal consistency ( cronbach = 09 ) and testretest reliability ( r = 08 )  . 
 a 6 - cm by 6 - cm monitor measured ssc every 10 s by passing an electric current across two electrodes attached to the sternal region of the chest . 
this is the standard criteria used for ssc monitoring validated with ambulatory and laboratory equipment.23 the sum of physiological and participantreported ( event - marked ) hfns were extracted for analysis . 
hfns = hot ushes and night sweats . table 1 : demographic and clinical baseline characteristics 312 vol 13 march 2012 articles cognitive behavioural therapy ( mean [ sd ] ) usual care ( mean [ sd ] ) cbt vs usual care * ( adjusted mean di erence [ se , 95% ci ; p value ] ) baseline 9 weeks 26 weeks 652 ( 243 ) 353 ( 198 ) 313 ( 194 ) 612 ( 202 ) 495 ( 224 ) 460 ( 248 ) 167 ( 039 , 243 to 091 ; < 00001 ) 176 ( 040 , 254 to 099 ; < 00001 ) * adjusted analysis used cohort number as a random e ect and a covariate for the binary age strati cation factor . table 2 : hot ush and night sweats problem - rating scores usual care cognitive behavioural therapy week 9 week 26 time from randomisation figure 2 : changes in problem - rating scores for hot ushes and night sweats error bars show 95% cis . treat sample ( excluding those who contributed no data )  . 
 we assessed the primary outcome with a linear mixed model ; covariates were treatment group , baseline hfns problem rating score , the strati cation factor age ( as a dichotomous category , split at 50 years ) , and time . 
we also analysed secondary outcomes with mixed linear regression models with random participant and cohort group intercepts and a time - by - treatment interaction term ; covariates in the model were treatment group , baseline value of outcome , the stratication factor age , and time . 
 participants rate each item on a 4 - point scale , according to the extent to which they are experi encing each item , and subscale scores are calculated , ranging from 01 ( higher scores indicate poorer wellbeing )  . 
the depressed mood subscale has concurrent validity with the ghq and the whq has good internal reliability for subscales ( cronbach 070084 ) and test - retest reliability ( 078096 )  . 
we also included measures of process variables including beliefs , behaviours , and stress , which are described elsewhere.20 adherence to group cbt was measured by the number of sessions attended and the number of times that a participant practised relaxation or paced breathing each week . 
recurrence of breast cancer , skin irritation due to the hot ush monitor , and clinically signi cant deterioration in mood were identi ed as possible expected unrelated adverse events , and clinically signi cant deterioration in mood as a result of group cbt was identi ed as a potential treatment - related adverse event . 
recurrence of breast cancer or secondary cancers were classi ed as expected but unrelated serious adverse events.28 statistical analysis we calculated that a sample size of 96 women was needed to provide 90% power to detect a two - point di erence ( sd 24 ; standardised e ect size 08 ) in mean hfns problem rating for the comparison of cbt to usual care at 9 weeks after randomisation . 
this sample size allowed for 20% loss to follow - up , a variance in ation factor of 149 ( intraclass correlation 007 , 29 eight participants per group ) to power for expected clustering of outcomes , and an hfns problem rating baseline - to - outcome correlation of 04 on analysis of covariance with two - sided 5% signi cance levels . the statistical analysis plan was nalised and approved by the trial team before completion of data collection . 
analyses were based on modi ed intention - tovol 13 march 2012 24 h sternal skin conductance frequency ( n = 89 ) 24 h event - marker frequency ( n = 89 ) 1083 ( 896 ) 1000 ( 784 ) 911 ( 833 ) 776 ( 510 ) 191 ( 151 ) 104 to 487 articles total hfns frequency hot ush frequency night sweats frequency baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks whq depressed mood whq somatic symptoms whq anxiety or fears whq sleep problems whq memory and concentration sf - 36 physical functioning sf - 36 rolephysical 7284 ( 3789 ) 5772 ( 4373 ) 4533 ( 4593 ) 5864 ( 3216 ) 4560 ( 3800 ) 3746 ( 4141 ) 1631 ( 1484 ) 1212 ( 993 ) 848 ( 913 ) 938 ( 883 ) 1205 ( 803 ) 023 ( 026 ) 013 ( 016 ) 013 ( 019 ) 056 ( 026 ) 044 ( 024 ) 045 ( 023 ) 034 ( 025 ) 023 ( 027 ) 024 ( 031 ) 063 ( 030 ) 037 ( 031 ) 043 ( 037 ) 075 ( 034 ) 059 ( 036 ) 051 ( 037 ) 6617 ( 2289 ) 7538 ( 2424 ) 7413 ( 2496 ) 5372 ( 4329 ) 6000 ( 4035 ) 5577 ( 4310 ) 26 weeks with two - sided 95% cis . 
the trial is registered with current controlled trials , number isrctn13771934 . cognitive behavioural therapy ( mean [ sd ] ) usual care ( mean [ sd ] ) adjusted mean ( di erence [ se ] ) 95% ci role of the funding source the sponsor of the study had no role in the study design , data collection , data analysis , data interpretation , or writing of the report . 
 results we randomly allocated 96 women to treatment between may 5 , 2009 , and aug 27 , 2010 , most of whom remained in the trial ( gure 1 )  . 
withdrawal rates were much the same in both treatment groups ( p = 099 at 9 weeks ; p = 079 at 26 weeks ) , as were baseline demographic and clinical characteristics of participants ( table 1 )  . 
on starting the trial , hfns were frequent and problematic with a mean of 69 per woman ( sd 39 ) occurring per week for an average of 2 years , with a mean problem rating of 63 out of 10 ( table 1 )  . 
13 women were taking non - hormonal prescribed drugs ( table 1 ) : hormone replacement therapy ( one woman in each group ) , ssri ( two women in the cbt group and three in the usual care group ) , gabapentin ( one woman in each group ) , clonidine ( two women in the cbt group ) , gabapentin plus ssri ( one woman in the cbt group ) , and clonidine plus ssri ( one woman in the usual care group )  . problem rating scores at 9 weeks and 26 weeks were lower in the cbt group than they were in the usual care group ( table 2 )  . 
there was a signi cant di erence between groups the primary outcomehfns problem rating at 9 weeks following randomisation ( adjusted mean di erence of 167 , 95% ci 243 to 091 ; p < 00001 ) with a greater reduction from baseline in problem rating in the cbt group compared to the usual care group . 
at 9 weeks , the change in problem rating from baseline was 305 ( sd 23 ) in the cbt group , compared with 106 ( sd 17 ) in usual care group , equating to a 46% reduction in the cbt group and a 19% reduction in the usual care group . 
at 26 weeks , the problem rating had decreased from baseline by 52% ( mean change 339 , sd 23 ) in the cbt group and by 25% ( mean change 126 , sd 22 ) in the usual care group ( table 2 ; gure 2 )  . we recorded no signi cant di erence between groups in hfns frequency , or in the hot ush frequency and night sweat frequency subscales when analysed separately , at 9 weeks or 26 weeks ( table 3 and appendix )  . 
compared with baseline , both groups reported non - signi cantly fewer hfns at 9 weeks ( 21% in the cbt group and 24% in the usual care group ) and 26 weeks ( 38% in both groups )  . 
 table 3 : e ect of treatment on hot ushes and night sweats week 26 compared with those in the usual care group ( table 3 and appendix )  . 
women receiving cbt also reported less anxiety than did women in the usual care group at 9 weeks , but this di erence was not statistically signi cant at 26 weeks ( table 3 )  . 
we recorded small improvements in memory and concentration of participants in the cbt group compared with those in the usual care group , but no statistically signi cant di erences in somatic symptoms ( table 3 )  . 
at 26 weeks , women in the cbt group reported signi cantly better social functioning , physical functioning , and improved general health ( at both 9 weeks and 26 weeks ) than did women in the usual care group , according to the sf - 36 assessments ( table 3 )  . 
compared with women in the usual care group , women in the cbt group reported better mental health at 9 weeks and less bodily pain at 26 weeks ( table 3 )  . 
we recorded no signi cant di erences between the groups in emotional role functioning or vitality subscales ( table 3 )  . although we did not record a mean two - point difference between treatment groups ( gure 3 ) , a greater percentage of individuals had reached this two - point threshold in the cbt group than in the usual care group at both 9 weeks ( 65% [ 95% ci 5078 ] vs 38% [ 2552 ] ) and 26 weeks ( 78% [ 6288 ] vs 33% [ 2048 ] )  . 
this exploratory analysis suggests that improvement from baseline was clinically better in the cbt group than it was in the usual care group ( gure 3 )  . in the 10% of sessions assessed for quality assurance , cbt was delivered according to the treatment manual , with 98100% adherence . 
participant adherence to treatment was good ; 39 ( 91% ) of 43 participants who received cbt attended at least four of six sessions , and relaxation or paced breathing was practised , on average , 29 times each week ( sd 2693 )  . individuals taking prescribed drugs for hfns tended to continue them throughout the trial . 
three women started homoeopathy or herbal remedies ( one in the cbt group , two in the usual care group ) , and one woman in the usual care group started acupuncture . 
when the adjusted primary analyses were repeated excluding these ve participants , the estimates and cis remained within the same margins ( week 9 hot ush problem rating , cbt vs usual care mean di erence 158 , 95% ci 238 to 079 ; p < 00001 ; week 26 hot ush problem rating , cbt vs usual care mean di erence 177 , 259 to 095 ; p < 00001 )  . we recorded six adverse events , three in the cbt group and three in the usual care group . 
one participant died of an unrelated disorder before the treatment phase ( usual care group ) , we recorded two reoccurrences of breast cancer ( one in each group ) , and one woman reported low mood unrelated to the trial ( cbt group )  . 
 ( continued from previous page ) sf - 36 bodily pain sf - 36 general health sf - 36 vitality sf - 36 social functioning sf - 36 roleemotional sf - 36 mental health baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks baseline 9 weeks 26 weeks 4615 ( 2273 ) 5368 ( 2398 ) 5100 ( 2250 ) 4810 ( 1594 ) 5184 ( 1458 ) 5034 ( 1542 ) 3533 ( 1610 ) 3963 ( 1523 ) 4031 ( 1748 ) 6702 ( 3143 ) 7530 ( 2539 ) 7750 ( 2718 ) 6739 ( 4245 ) 7561 ( 3802 ) 7350 ( 3760 ) 6757 ( 1789 ) 7463 ( 1422 ) 7070 ( 1924 ) cognitive behavioural therapy usual care week 9 week 26 figure 3 : proportion of patients with a reduction of two or more points in the hot ush problem - rating scale from baseline estimates are unadjusted . 
 vol 13 march 2012 articles two women ( both in the usual care group ) had mild reactions to the hot ush monitor ( a reaction to the adhesive used on the electrode patch )  . 
none of the adverse events were related to cbt . discussion our ndings suggest that cbt is safe , acceptable , and e ective in helping women to manage hot ushes and night sweats after breast cancer treatment , with additional bene ts to mood , sleep , and some aspects of quality of life . 
after group cbt , women reported less problematic hfns than did those receiving usual care , and these improvements were maintained at both the 9 - week and 26 - week follow - up . 
although the pre - speci ed endpoint of a between - group di erence of 2 points on the problemrating scale was not met , there was a statistically signi cant improvement in the cbt group , and a large proportion of women ( 78% ) who had received cbt achieved a reduction of 2 points compared with the usual care group ( 33% ) at 26 weeks . 
similarly , we recorded no signi cant di erences between groups in 24 h rate of hfns after the treatment phase , either physiologically ( ssc ) de ned or participant recorded ( event monitor )  . 
most women participating in group cbt reported reductions in problem rating that are regarded as clinically important , and there were sustained signi cant differences in problem rating between cbt and usual care . 
one study was the menos1 single - group pilot trial , 18 in which weekly 15 h sessions of cognitive behavioural therapy ( cbt ) for 6 weeks resulted in an average 49% reduction in problem rating and 38% reduction in hot ushes and night sweats ( hfns ) frequency , maintained at 3 months follow - up . 
a larger randomised controlled trial of cbt and exercise , 33 which used the group protocol manual developed for menos 1 , 18 reported preliminary ndings in which frequency and problem - rating reduced compared with usual care , although detailed ndings are not available . 
in another single - group trial , 34 an instructional dvd of paced breathing and distraction used over the course of 1 week resulted in small reductions in bothersomeness and interference of hfns and no change in physiologically measured hot ush frequency . 
cbt shows some promise but adequately powered randomised controlled trials are needed . interpretation our ndings show that group cbt can reduce the e ect of hot ushes and night sweats for women who have had breast cancer treatment . 
group cbt seems to be a safe , acceptable , and e ective treatment option which can be incorporated into breast cancer survivorship programmes and delivered by trained breast cancer nurses . 
at baseline , on average , participants had higher scores for sleep problems , somatic symptoms , and memory and concentration ( whq ) compared with norms for healthy women ( table 3 and data not shown ) .27 according the the sf - 36 scale , they had lower scores ( lower quality of life ) than did healthy women , especially for physical role functioning , general health , vitality , and bodily pa the signi cant improve ments in mood and sleep , as well as memory and concentration , after cbt are clinically important because di culties with mood sleep and cognitive functions are commonly reported by patients with breast cancer , particularly by those with hfns.30 moreover , the improve ment in social functioning after cbt is relevant because women report nding hot ushes especially di cult to deal with at work and in other social situations.18 although randomised controlled trials of non - hormonal drugs for hfns have shown moderate reductions in hfns frequency , they have recorded little evidence of improved quality of life.9 similarly , some studies show only weak relations between frequency of hfns and quality of life.21 , 22 the results of our study are very similar to the preliminary ndings of a parallel trial of cbt for hfns in a sample of healthy women ( menos2 ) .31 this consistent pattern of results suggests that the cbt might work by a ecting symptom perception and cognitive appraisal of hfns and possibly mood , rather than physiological mechanisms of hfns , such as temperature regulation or the thermoneutral zone in the hypothalamus.19 further analyses of moderators and mediators of hfns are planned to clarify this issue through identi cation of the underlying causal pathways to improvement on the hot ush problem rating scale.20 for example , changes in sleep after treatment might partly mediate the improvements in mood and quality of life . 
further studies should examine particular components of the intervention to test these analyses experimentally . we postulated that cbt would reduce hfns frequency to a greater extent than would usual care , especially because paced breathing has been shown to reduce hfns frequency measured both physiologically and subjectively.32 women receiving cbt reported practising paced breathing daily . 
paced breathing , once learnt , is practised for 25 min throughout the day and at the onset of a hot ush , so an average of 29 times per week is a realistic rate at which to practise . 
however , we controlled for usual care and assessment e ects and we should gain some insight into the placebo e ects of usual care through the planned mediator and moderator analysis.20 further research could compare di erent types of control conditions with di ering levels of information , advice , and support . 
the group cbt programme should be generalisable to other breast cancer settings because it is delivered in a hospital setting , is done by use of easily transferable guidelines ( the treatment manual ) , and adherence to the guidelines was high . 
the most cost - e ective method of delivering the group cbt would probably be to include it as part of survivorship support programme , delivered by trained and supervised breast - care nurses . to date , the best available treatments have been nonhormonal drugs including ssri and snris , clonidine , and gabapentin.9 these treatments have produced moderate reductions in hfns frequency ( averaging 37% across trials9 ) , but have had little e ect on quality - of - life measures . 
 by contrast our ndings suggest that both cbt and usual care resulted in a 38% reduction in frequency , and compared with the usual care group , those who received cbt showed statistically signi cant and lasting reductions in problem rating and improvements in quality of life . 
cbt could , therefore , be an important alternative or additional treatment option for patients with breast cancer ( panel 2 )  . limitations of this study include the frequency measures , which had high variability . 
however , ndings from another study show evidence of the validity of this scale compared with daily diary measures.24 estimation of the frequency of night sweats with the hot ush rating scale can be more di cult because women do not report night sweats that they sleep through , but this limitation is common to all self - report measures . 
the physiological measure was used for 24 h at baseline and at 9 weeks after randomisation ; in view of the variability of this measure , future studies might include a longer time of ssc monitoring and also include this measure at follow - up assessments . 
addition ally , we did not control for all potential confounding factors that could have an e ect on menopausal symptoms , such as the use of drugs to manage hfns and the use of adjuvant hormone therapy . 
however , treatment options are still restricted for these women , so a need still exists for nonhormonal interventions . our ndings suggest that this cognitive behavioural treatment , designed to be delivered by trained health professionals such as breast - care nurses , has the potential to improve long - term health outcomes for patients with breast cancer , and could be incorporated into breast cancer survivorship programmes . con icts of interest we declare that we have no con icts of interest . 
msh contributed to the search of published studies , study design , and data interpretation , and was the principle investigator and report guarantor . acknowledgments this work was funded by cancer research uk ( grant c8303 / a6130 ) ; msh was also supported by the national institute for health research biomedical research centre for mental health , south london and maudsley nhs foundation trust and the institute of psychiatry , kings college london , uk . 
trudie chalder , mark harries , ruth pickering , aleksandra gentry - maharaj , and caroline burgess contributed to development of the study , and participated in trial steering and data management committees . 
our aim was to investigate these associations in a large uk prospective cohort with su cient information on incident cancer to allow direct comparison of height - associated risk across cancer sites and in relation to major potential confounding and modifying factors . methods information on height and other factors relevant for cancer was obtained in 19962001 for middle - aged women without previous cancer who were followed up for cancer incidence . 
we used cox regression models to calculate adjusted relative risks ( rrs ) per 10 cm increase in measured height for total incident cancer and for 17 speci c cancer sites , taking attained age as the underlying time variable . 
 findings 1 297 124 women included in our analysis were followed up for a total of 117 million person - years ( median 94 years per woman , iqr 84102 ) , during which time 97 376 incident cancers occurred . 
risk increased for 15 of the 17 cancer sites we assessed , and was statistically signi cant for ten sites : colon ( rr per 10 cm increase in height 125 , 95% ci 119130 ) , rectum ( 114 , 107122 ) , malignant melanoma ( 132 , 124140 ) , breast ( 117 , 115119 ) , endometrium ( 119 , 113124 ) , ovary ( 117 , 111123 ) , kidney ( 129 , 119141 ) , cns ( 120 , 112129 ) , nonhodgkin lymphoma ( 121 , 114129 ) , and leukaemia ( 126 , 115138 )  . 
the increase in total cancer rr per 10 cm increase in height did not vary signi cantly by socioeconomic status or by ten other personal characteristics we assessed , but was signi cantly lower in current than in never smokers ( p < 00001 )  . 
in current smokers , smokingrelated cancers were not as strongly related to height as were other cancers ( rr per 10 cm increase in height 105 , 95% ci 101109 , and 117 , 113122 , respectively ; p = 00004 )  . 
in a meta - analysis of our study and ten other prospective studies , height - associated rrs for total cancer showed little variation across europe , north america , australasia , and asia . interpretation cancer incidence increases with increasing adult height for most cancer sites . 
the relation between height and total cancer rr is similar in di erent populations . funding cancer research uk and the uk medical research council . introduction tall people are at increased risk of cancer . 
increasing cancer risk with increasing adult height has been reported for all cancers combined and for several common cancers , such as those of the breast , ovary , prostate , and large bowel.17 evidence is limited , however , for incident , rather than fatal , disease and for less common cancer sites . 
 moreover , it is not clear to what extent height - associated risks vary by cancer site , or how other factors , such as smoking and socioeconomic status , a ect these associations.8 , 9 because the range of height in a given population is usually narrow , large numbers of events are needed for reliable estimation of risk . 
we also did a meta - analysis of published results from prospective studies on the relation between height and total cancer incidence or mortality . methods participants between 1996 and 2001 , 13 million middle - aged women invited to attend the uks national health service ( nhs ) breast screening programme completed a million women study recruitment questionnaire , which asked , among other things , about social , demographic , and lifestyle factors , including current height and weight . 
of women who answered a study questionnaire in 200607 , a sample selected at random ( on the basis of day of birth ) were asked in 200609 to have their height measured by their family doctor : 3762 women did so . 
in this validation sample , the correlation between measured and reported heights was excellent ( pearson correlation coe cient 088 )  . vol 12 august 2011 articles all participants gave written consent to take part in our study , and approval was obtained from the oxford and anglia multi - centre research ethics committee . 
all study participants have a unique nhs number and are automatically followed up for death , emigration , and cancer registration through the nhs central registers with that number and other identifying details . 
the registers regularly provide study investigators with information on the date of any such event in participants , and code the underlying cause of death and cancer site with the international classi cation of diseases , 10th revision ( icd - 10 ) .10 follow - up is complete for over 99% of study participants . 
 procedures our main endpoints were incident invasive cancer at 17 individual sites with at least 1000 incident cases : mouth and pharynx ( icd - 10 c00 - c14 ) , oesophagus ( c15 ) , stomach ( c16 ) , colon ( c18 ) , rectum ( c19 - 20 ) , pancreas ( c25 ) , lung ( c34 ) , malignant melanoma ( c43 ) , breast ( c50 ) , endometrium ( c54 ) , ovary ( c56 ) , kidney ( c64 ) , bladder ( c67 ) , central nervous system ( c7072 , d32 , 33 , 42 , and 43 ) , non - hodgkin lymphoma ( c82 - 85 ) , multiple myeloma ( c90 ) , and leukaemia ( c91 - 95 )  . 
we included all other invasive cancers ( the remaining icd - 10 c codes , except non - melanoma skin cancer [ c44 ] ) as other and unspeci ed cancers . there concluded has su cient evidence of carcinogenicity in human beings in relation to active tobacco smoking : 11 , 12 of the sites listed above , mouth and pharynx , oesophagus , stomach , colorectum , pancreas , lung , mucinous tumours of the ovary , kidney , and myeloid leukaemia ( c92 ) , and , additionally , liver ( c22 ) , larynx , nasal cavity and nasal sinuses ( c30 - 32 ) , cervix ( c53 ) , and urinary tract , including renal pelvis and ureter ( c65 , 66 , 68 )  . 
when comparing smoking - related and other cancers , we excluded from our analysis cancers of ill - de ned and unspeci ed sites , which might include some smokingrelated cancers ( icd - 10 c26 , c39 , c57 , c76 - 80 and c95 - 96 ) , and cancers of the ovary ( for a substantial proportion of which histological subtype was not known , and which might have included mucinous tumours )  . cm , 1601649 height was reported by participants at recruitment in feet and inches , and converted to centimetres for our analysis . 
for the analyses , women were divided into six categories of reported height ( < 155 cm [ reference group ] , cm , 1551599 1701749 cm , and 175 cm and taller ) ; we took the average height in each of these categories to be the mean measured height in that category in the sample whose height was measured in 200609 . 
standardised to the distribution of categories of self - reported height in our whole analysis population . table 1 : baseline characteristics by height and follow - up for incident cancer in the million women study 786 vol 12 august 2011 articles women rr ( 95% fci ) incident cancers < 155 cm ( mean 1528 cm ) 233 516 15 792 100 ( 098102 ) 155 cm ( mean 1565 cm ) 196 773 14 213 108 ( 107110 ) 160 cm ( mean 1604 cm ) 388 515 28 806 112 ( 111114 ) 165 cm ( mean 1649 cm ) 288 893 22 571 120 ( 118122 ) 170 cm ( mean 1690 cm ) 143 289 11 902 128 ( 125130 ) 175 cm ( mean 1738 cm ) 46 138 4092 137 ( 133142 ) analysis strati ed by age at recruitment and region and adjusted for socioeconomic status , smoking , alcohol intake , body mass index , strenuous exercise , age at menarche , parity , and age at rst birth . table 2 : relative risks ( rrs ) and 95% oated cis ( fcis ) for total cancer incidence , by category of height reported at recruitment ( mean measured height ) cancer ( icd10 c44 ) registered before recruitment and if they did not have valid information on height at recruitment ( including a small proportion , about 005% whose reported height was < 120 cm or > 200 cm )  . 
for analyses including endometrial and / or cervical cancers , we excluded women if they reported a hysterectomy at recruitment , or if their hysterectomy status was unknown ; similarly , for analyses of ovarian cancer , we excluded women reported a bilateral they oophorectomy at recruitment , or if their oophorectomy status was unknown . from we calculated woman - years the date of recruitment to the date of rst cancer registration ( at any site ) , death , or the last date of follow - up , whichever was rst . 
for analyses of cancer incidence , the last date of follow - up was dec 31 , 2008 , for the uk regions of east anglia and south west ; june 30 , 2008 , for oxford , thames , west midlands , and north west ( mersey ) ; and dec 31 , 2007 , for northern and yorkshire , trent , north west ( manchester and lancashire ) , and scotland . statistical analysis we used cox regression models to estimate relative risks ( rrs ) and cis in relation to height at recruitment , taking attained age as the underlying time variable . 
we strati ed all analyses by age at recruitment ( < 52 , 5355 , 5658 , 5961 , 6264 , 65 years ) and region ( ten regions covered by ten cancer registries ) , and adjusted , as appropriate , for quintiles of socioeconomic group ( based on townsend deprivation score13 ) , body - mass index ( < 225 , 225249 , 250274 , 275299 , 30 kg / m ) , strenuous exercise ( less than once a week , once a week or more ) , alcohol consumption ( none , 2 units per week , 3 units per week ) , smoking ( never , past , current 114 cigarettes per day , current 15 cigarettes per day ) , age at menarche ( < 13 , 13 , 14 years ) , parity ( 0 , 12 , 3 full - term pregnancies ) , and age at rst birth ( < 25 , 25 years )  . 
 we calculated the rr per 10 cm increase in height as a trend across the six category means using the measured mean height in each category of reported height.14 we assessed heterogeneity of trends in rrs between di erent cancer sites with a ( ) contrast test , under the survival analysis assumptions that estimates at each cancer site are asymptotically normally distributed and , because of censoring at rst cancer diagnosis at any site , uncorrelated ( and that therefore site - speci c estimates account for competing risks of cancers at other sites ) .15 where two categories of exposure are compared ( as in the text ) conventional cis are given . 
for analyses of total cancer , where more than two categories are compared ( as in the gures ) , oated cis ( fcis ) were estimated by treating the rrs as oating absolute risks ( fars ) .16 , 17 use mean height ( cm ) figure 1 : relative risks ( rrs ) and 95% oated cis ( fcis ) for total incident cancer , by height rrs are adjusted for age , region , socioeconomic status , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth , and are plotted against the mean measured height in each category . 
all results are presented in the text with 95% cis , but for analyses by cancer site , when multiple rrs were estimated , 99% cis are given in the gures . where we present results in the form of plots , the rrs and their corresponding fcis or cis are represented by squares and lines with the area of each square inversely proportional to the variance of the logarithm of the corresponding rr . 
this shows the amount of statistical information involved . meta - analysis we identi ed published prospective studies of adult height and risk of total cancer ( incidence or mortality ) through electronic searches of published work ( medline and embase , up to april , 2011 ) with combinations of the search terms height , body size , anthropometr * , neoplasms , mortality , and risk factors , and vol 12 august 2011 articles number of incident cancers mouth and pharynx 1095 oesophagus 1167 stomach 1177 colon 6281 rectum 3190 pancreas 2044 lung 8074 melanoma 3583 breast 39 299 endometrium 5810 ovary 4830 kidney 1665 bladder 1354 cns 2328 non - hodgkin lymphoma 3411 1215 multiple myeloma leukaemias 1482 other and unspecifed 8997 total cancer 97 376 rr * & 99% ci 094 ( 082108 ) 104 ( 091119 ) 103 ( 090118 ) 125 ( 117132 ) 114 ( 105124 ) 105 ( 095117 ) 103 ( 098108 ) 132 ( 122142 ) 117 ( 114120 ) 119 ( 112126 ) 117 ( 109125 ) 129 ( 115145 ) 100 ( 088114 ) 120 ( 109132 ) 121 ( 112131 ) 113 ( 099129 ) 126 ( 111142 ) 115 ( 110121 ) 116 ( 114117 ) through cited references in identi ed papers . 
we included in our meta - analysis all identi ed studies with published age - adjusted rr and 95% cis for total cancer per 10 cm increase in height , or with su cient published data to allow estimation of such rrs . 
where only categorical results were published , we calculated the trend in rr per 10 cm increase in height using the mean height in each height category ( estimated , where necessary , as category midpoints , or by other methods ) , 18 assuming linearity of log rrs and with a summary trend estimate obtained by the method of generalised least squares.19 we combined results for subgroups of total cancer ( eg , smoking - related and other cancers ) by least squares , where necessary . 
where the mean year of birth of the study population was not given , we made an estimate with the average age at , and year of , study recruitment . 
 results the 1 297 124 women included in our analysis had a mean age at recruitment of 561 years ( sd 49 ) and an average year of birth of 1942 . 
the median length of follow - up was 94 years per woman ( iqr 84102 years ) , for a total of 117 million person - years , during which 97 376 incident cancers were noti ed . table 1 shows characteristics of the study population , including measured height , by six categories of height reported at recruitment . 
taller women tended to be of higher socioeconomic status , to drink more alcohol , to be more active , to have a later age at menarche , to have fewer children , and to have their rst child later in life than shorter women . 
based on heights measured in the validation sample , the mean height in the study population was 1609 cm ( sd 64 )  . total cancer incidence rose with increasing height ( table 2 )  . 
comparing women in the tallest group with 075 125 figure 2 : relative risks ( rrs ) and 99% cis per 10 cm increase in height for incident cancer at 17 speci c sites and for total cancer the doted line represents the rr per 10 cm increase in height for total cancer . 
 there is heterogeneity across cancer sites ( contrast test [ 17 degrees of freedom ] = 1152 ; p < 00001 ) mostly because of the greater than average increase in risk with increasing height for colon cancer and for malignant melanoma , and the lower than average risk for lung cancer . 
however , the overall rr of incident cancer in relation to height was not materially altered when we excluded breast cancer cases from our analysis ( rr per 10 cm increase in height 115 , 95% ci 113116 )  . 
 we adjusted our results in gures 1 and 2 and in table 2 by age , region , socioeconomic status , smoking , alcohol , body - mass index , physical activity , age at menarche , parity , and age at rst birth . 
table 3 shows the e ect of adjustment by potential confounding variables on the rr for total cancer per 10 cm increase in height in an analysis restricted to the 1 087 489 women with full information on all adjustment variables . 
compared with the risk with adjustment for age and region only ( rr 114 , 95% ci 113115 ) , additional adjustment by the remaining factors increases the rr slightly to 116 ( 115118 )  . figure 3 shows the rr for total cancer per 10 cm increase in height , and the mean measured height , in subgroups of women de ned by their year of birth , socioeconomic status , smoking status , alcohol con sumption , body - mass index , physical activity , age at menarche , parity , age at rst birth , menopausal status , and use of oral contraceptives and hormone replacement therapy . 
as we expected , women born before 1939 were shorter than women born in 1946 or later ( mean measured height 1599 vs 1615 cm ) , as were women from the lowest compared to the highest socioeconomic tertile ( 1601 vs 1614 cm )  . 
although the risk for total cancer is somewhat higher in women in the lowest tertile of socioeconomic 125 figure 3 : relative risks ( rrs ) and 99% cis per 10 cm increase in height for all incident cancer , by various characteristics at recruitment the dotted line represents the rr per 10 cm increase in height for all women . 
rrs are adjusted as appropriate for age , region , socioeconomic status , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
the rr per 10 cm greater height was 119 ( 95% ci 117121 ) in never smokers , but only 111 ( 108114 ) in current smokers ( p < 00001 for hetero geneity )  . 
 vol 12 august 2011 articles mouth and pharynx oesophagus stomach colon rectum pancreas lung melanoma breast ovary kidney bladder endometrium 2960 1493 1943 18 533 3192 2426 1194 non - hodgkin lymphoma 1630 multiple myeloma leukaemias other and unspecifed 3616 total cancer 42 244 highest socioeconomic third middle socioeconomic third lowest socioeconomic third mean height ( cm ) figure 4 : relative risks ( rrs ) and 95% oated cis ( fcis ) for all incident cancer in relation to height , and by socioeconomic status the baseline category ( rr = 10 ) is women shorter than 160 cm from the highest socioeconomic group . 
rrs are adjusted for age , region , smoking , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
rrs are plotted against the mean measured height in each category of height ( < 160 cm , 160165 cm , 165170 cm , 170 cm ) , within categories of socioeconomic status . never smokers number of incident cancers current smokers number of incident cancers figure 5 shows the rrs per 10 cm increase in height by cancer site in never smokers and in current smokers ( results in past smokers are uninterpretable , because they are a heterogeneous group with a wide range of times since last smoking )  . 
the mix of cancers di ers in the two groups with , as expected , a higher proportion of women with lung and other smoking - related cancers in current smokers than in never smokers . 
in never - smokers , heterogeneity across cancer sites was substantially weaker ( p = 0004 ) than in current smokers ( p < 00001 )  . for smoking - related cancers , the rr per 10 cm greater height was substantially smaller in current smokers than in never smokers ( 105 vs 117 , p for di erence = 00004 ; gure 6 )  . 
 * rrs are adjusted for age , region , socioeconomic status , alcohol intake , body - mass index , strenuous exercise , age at menarche , parity , and age at rst birth . 
the overall pattern of rrs remained similar , with lower risk for smoking - related cancers than for other cancers in current smokers , although the di erence between these risks was reduced ( rr per 10 cm height 102 , 95% ci 097106 , in current smokers and 110 , 103117 , in never smokers ; p for di erence = 005 ) ; for other speci ed cancers , risks remained similar to those in our main analysis ( rrs 118 , 114122 , in current smokers and 119 , 116121 , in never smokers )  . 
 because breast cancer dominates our ndings , we repeated our analyses shown in gure 3 separately for the ve most common cancers in our study : breast , lung , colon , endometrium , and ovary , and for the remaining cancers . 
overall , we did not identify signi cant heterogeneity , by the 12 factors we show in gure 3 , for these cancer sites ( test for heterogeneity aggregated across all characteristics : colon p = 07 , lung p = 02 , breast p = 03 , endometrium p = 05 , ovary p = 02 , remaining cancers p = 02 )  . because there was no strong variation by cancer site in our study except in smokers , we did a meta - analysis of published studies of all - cancer risk , noting for each study the proportion of current smokers in the study population . 
 figure 7 shows details of our study together with ten other prospective studies1 , 3 , 8 , 2128 that have published results in such a way as to allow estimation of the rr of total cancer incidence or mortality per 10 cm increase in height . 
the populations covered include men and women from asia , australasia , europe , and north america , with mean years of birth ranging over three decades ( 1917 to 1946 ) , and with mean heights ranging over 24 cm ( 155 to 179 cm )  . 
there was no signi cant heterogeneity between the results from studies in men ( i for heterogeneity 0% , p = 09 ) or between those in women ( i for heterogeneity 31% , p = 02 ) , but there was a slightly lower height - associated rr in men than in women ( 110 vs 115 , p for di erence < 00001 )  . 
when we excluded the ndings of our study , the summary rr in women was slightly reduced ( summary rr per 10 cm greater height 113 , 95% ci 110116 ; i for heterogeneity 25% ; p = 02 ) , and there was no longer signi cant heterogeneity between studies in men and those in women ( p for di erence = 01 )  . 
all of the mortality studies we included provided rrs adjusted for at least one measure of socioeconomic status , which should have minimised potential confounding due to the relation in many populations between socioeconomic status and cancer survival.29 discussion we identi ed a clear and highly signi cant trend of increasing cancer risk with increasing height in this large prospective study of uk women , with rr for total incident cancer of 116 ( 99% ci 114117 ) for every 10 cm greater height . 
the magnitude of the height - associated increase in cancer risk was similar for women with di erent years of birth , from di erent socioeconomic groups , and across subgroups de ned by alcohol intake , body - mass index , physical activity , age at menarche , parity , age at rst birth , menopausal status , and use of oral contraceptives or hormone replacement therapy . 
by contrast , current smokers had a lower rr for total cancer incidence per 10 cm increase in height than never smokers , and this was largely because the height - associated cancer rrs in smokers were lower for smoking - related than for other cancers . 
 each of the 17 most common speci c sites we assessed included 1000 or more cancers , and together they constitute some 90% of total incident cancers in our study population . 
most previous studies had limited statistical power to study site - speci c cancer risk and tended to focus on a few common cancer sites , and our results for the common cancers are consistent with their ndings.2 , 47 all study participants were routinely linked to records of the nhs central registers and details of every incident cancer and death were coded before noti cation to the study investigators , thus providing complete and nondi erential ascertainment of cancer incidence during follow - up . 
there was excellent correlation between self - reported and measured height , consistent with previous ndings for height and some this cohort.30 , 31 other anthropometric variables nevertheless , we corrected for measurement error , and for changes in height over time , by use of the mean measured height in each category to calculate rr per 10 cm increase in height . 
 as expected , the average height of women in this population was slightly greater the more recently they were born and with increasing socioeconomic status ( gure 3 )  . 
method of chne and thompson18 used to estimate mean heights in height categories . 075 group , age at menarche , parity , age at rst birth , bodymass index , physical activity , smoking status , and alcohol consumption . 
women in higher socioeconomic groups are on average taller ( table 1 ) , and socioeconomic status is related to total cancer incidence ( gure 4 ) , 29 yet the association between height and risk of cancer was similar for women of low , medium , and high socioeconomic status . 
as in other studies that could adjust for a range of potential confounding factors , our results suggest that the relation between height and cancer risk is not due to other known risk factors for cancer.9 our ndings show that the height - related rr of cancer was lower for smoking - related cancers than for other cancers , but only in current smokers . 
in accordance with our ndings kabat and colleagues32 have reported that lung cancer incidence in the womens health initiative study showed a stronger association with height in never smokers than in current or past smokers . 
smoking - related cancers are more common in current smokers than in never smokers , with agestandardised incidence rates of 599 and 176 , respectively per 100 000 women per year , in this cohort . 
the estimated excess age - standardised incidence rate for every 10 cm increase in height for smoking - related cancers is about 30 per 100 000 women per year , both in current and in never smokers ( 599 005 for current smokers and 176 017 for never smokers )  . we found no other modi cation of height - associated rr by the 11 other factors we assessed , either for total cancer , or separately for the ve most common cancers ( breast , lung , colon , endometrium , and ovary )  . 
 there was little variation in height - associated rrs at speci c cancer sites in never smokers , in whom the e ect of height on cancer risk is free from modi cation by smoking . 
in general , studies have found taller people to be at increased risk of a range of cancers with varying causes , with no individual cancer site consistently identi ed as showing no association.2 , 47 our nding of di erences in height - related rr between smokers and never smokers might provide an explanation for some reported inconsistencies in height - associated risk for smoking - related cancers.2 our meta - analysis of height and total cancer risk shows that ndings are very consistent for incidence and for mortality , and in populations from europe , north america , asia , and australasia with mean years of birth ranging over 30 years , and with mean heights ranging from 155 cm to 179 cwomen in these studies were less likely than men to be current smokers ( gure 7 ) and this might partly explain the slightly higher heightassociated rr in women than in men in our metaanalysis . 
the overall result in women is also strongly weighted by the results from the million women study , in which there has been allowance for measurement error , and more extensive adjustment than in the other studies , both of which tended to increase the estimated rr . 
as in any meta - analysis of published data , our ndings need to be interpreted in the knowledge that other studies with relevant data might not have published their results . 
 the similarity of the height - associated rr for di erent cancers and in di erent populations suggests that a basic common mechanism , possibly acting in early life , might be involved.8 adult height reaches its maximum between the ages of 20 and 30 years . 
variation in height relates to genetic and environmental in uences acting mostly in the rst 20 years , or so , of life ; environmental factors , including childhood nutrition and infections , are believed to predominate.3336 hormone levels , especially of growth factors such as insulin - like growth factors ( igfs ) , both in childhood and in adult life , might be relevant.2 , 9 circulating levels of igfs in adulthood and childhood a ect cancer risk ; 3740 igf - i levels in childhood and adolescence are strongly related to skeletal growth , 38 and levels in adulthood , although less strongly , to adult height.41 , 42 another possibility is that height predicts cancer risk because taller people have more cells ( including stem cells ) , and thus a greater opportunity for mutations leading to malignant transformation.43 , 44 height might thus be related to cancer risk through increased cell turnover mediated by growth factors , or through increased cell numbers . 
adult height in european populations has increased by about 1 cm per decade throughout the 20th century.33 , 45 , 46 the increase in adult height during the past century could thus have resulted in an increase in cancer incidence some 1015% above that expected if population height had remained constant . 
all authors approved the report . con icts of interest we declare that we have no con icts of interest . acknowledgments we thank all the women who participated in the study , sta from participating nhs breast screening centres , and family doctors , practice nurses , and other primary - care sta for help with validation measurements . 
we thank gary whitlock for helpful contributions to the manuscript . comment if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology as piration of mediastinal and hilar lymph nodes should be used to assess preoperative lung cancer status in countries where tuberculosis is endemic.10 finally , hiv infection is associated with increased lung cancer cases . 
can tuberculosis further increase this risk ? in a study11 that linked aids registry surveillance data for 322 675 patients with aids diagnosed between 1977 and 2002 , with cancer registries in 11 us regions , lung cancer risk over 10 years was unrelated to tuberculosis . 
 tuberculosis awareness in patients with cancer needs to be reinforced , especially in low - burden developed countries , and lung cancer awareness in patients with previous or suspected tuberculosis should be urgently strengthened in developing countries to increase the low numbers of potentially resectable tumours . * sandro vento , massimiliano lanzafame department of internal medicine , faculty of medicine and health sciences , university of botswana , gaborone , botswana ( sv ) ; and infectious diseases unit , gb rossi university hospital , verona , italy ( ml ) ventosandro@yahoo.it we declare that we have no con icts of interest . yu yh , liao cc , hsu wh , et al . 
lancet oncol 2011 ; 12 : 37786in this article ( april ) , on page 380 , the number of women with luminal a breast cancer tested for the kras variant should have been 478 in gure 2a and the percentage of premenopausal women diagnosed with luminal a breast cancer should have been 151% in gure 2b . 
lancet oncol 2011 ; 12 : 41516on page 415 , in the second column , it was stated that 17 variants showed moderate to strong evidence of a true association and were therefore candidates for clinical tests , this should have said 14 variants . 
this correction has been made to the online version as of may 18 , 2011 . published online may 18 , 2011 doi : 10.1016 / s14702045 ( 11 ) 70127 - 9 522 vol 12 june 2011 editorial for the coa report see userfiles / les / community_ oncology_practice_impact_ report_4 - 4 - 12f%281%29%281 %29.pdf for the avalere study see communityoncology.org / userfiles / les / avalere_cost%20 of_cancer_care_studyf.pdf to nd out more about the macmillan campaign see getinvolved / campaigns / countingthecostofcancer / countingthecostofcancer.aspx for the regional cancer care association see rc2acancercare.com / are patients counting the cost of the economic downturn ? impossible to the continuing global economic crisis remains far reaching and ignore . 
whether this will prove to be bene cialboth for the balance sheet and , more importantly , to the patientswill depend on the regional context and how the process is managed . on april 4 , 2012 , the community oncology alliance ( coa ) , a non - pro t organisation dedicated to community oncology in the usa , published an update to their practice impact report , showing that in the past 45 years , nearly 700 oncology practices and clinics across the usa closed or are struggling nancially , with many private oncology practices being bought out or consolidated into a hospital setting . 
the act changed the way in which medicare and medicaid pays for prescription drugs , with oncology practices seeing a signi cant reduction in payment for chemotherapy agents which often does not cover the cost of the drugs . 
the consequences of this act are far - reaching , with many private insurance companies following this lead , resulting in further di culties for cancer - care providers . for oncology services that are still being provided , those in a hospital setting potentially result in increased costs when compared with private clinics . 
a study by the healthcare research company avalere health , commissioned by the coa , found that treatment for patients receiving chemotherapy in a hospital outpatient environment costs an average of 24% more than those who receive the same treatment in a private oncology clinic . 
however , the study was unable to determine whether the level of care requirements were higher in hospitals . at the personal level in the usa , cancer patients often nd themselves left without a safety net if they eventually become too ill to work . 
 hospital closures in the uk and other countries have lead to a consolidation of care which has been blamed for increasing the nancial burden on cancer patients , mainly via increased transport costs to and from clinics to see oncologists . 
complaints about regional variation for the funding of cancer drugs and a lack of choice add further complexities to an over - burdened syste the uk charity macmillan cancer support has highlighted the concerns to patients in a recent report , and are working with the nhs in wales to ensure that all cancer patients are provided with advice to help them cope with increased nancial stra there can , however , be bene ts gained from a consolidation of care . 
in some health - care systems , organised groups of clinicians have better purchasing power to broker more favourable deals with drug companies and suppliers , and integration of care within a hospital group or within a private company does not necessarily mean a shrink in geographical coverage or levels of provision . 
the formation of the regional cancer care associates ( rc2a ) in new jersey , usa , is potentially an early indication on how consolidation can be done for the bene t of the patient . 
this large company works to one standard at all sites to provide a transparent standard of care , improve access for patients to clinical trials , and to reduce over - testing and over - treatment . it is clear that the consolidation of cancer care will continue , with both public and private health care systems a ected . 
although there are pros and cons to any structural reorganisation , it is imperative that all decisions are thought through carefully to ensure that above all patient care is not a ected , and second that any cost savings are not simply transferred to the patients own expenditure . 
the corrected version rst appeared at thelancet.com / oncology on june 29 , 2012 for more on the lancet oncologys call for gps to receive better education see leading edge lancet oncol 2009 ; 10 : 97 for more on variation in gp referral patterns for patients with cancer see articles lancet oncol 2012 ; 13 : 35365 for more on the partnership between cancer research uk and the royal college of general practitioners see news lancet oncol 2012 : 12 : e232 for more on qcancer risk calculators see for more on the challenges of supporting patients with multiple morbidities see articles lancet 2012 ; published online may 10 . 
a third of all young cancer patients reported their gps took no action despite presentation with common cancer symptoms and a quarter of patients had to visit the gp four or more times before their symptoms were taken seriously . 
if a young person presents with the same symptoms three times , gps should automatically refer them for further investigation . although the tct survey was small ( collating the opinions of only 300 patients ) , the ndings mirror those of lyratzopoulos and colleagues published in the lancet oncology in april , 2012 , that analysed more than 41 000 patients with 24 types of cancer . 
in that study , researchers found that nearly a quarter of patients needed three or more consultations with their gp before a referral was made and the probability of an increased number of consultations was higher among young patients . 
 so what can be done to restore trust ? usefully , cancer research uk and the royal college of general practitioners have launched an initiative to support gps by putting together models of best practice , and by reviewing care pathways and thresholds for further investigation to ensure gps have better access to diagnostics and secondary care . 
 additionally , the department of health has announced a pilot project within gp practices of cancer - risk prediction tools ( qcancer risk calculators ) developed by researchers at the university of nottingha these successful these partnerships are good examples of engagement between policy makers and physicians with organisations that have a perceptive understanding of the patient viewpoint and of research realities and possibilities . 
 initiatives will be whether transforming the e ectiveness of the gp and improving patient care will take time to assess , but it is unlikely that they will prove to be a broad panacea . 
it is becoming increasingly clear , for example , that the uk health - care system is not designed to cope with multiple comorbiditiesa common situation among patients with cancerand in the future gps will need to take a central and proactive role in coordinating patient care throughout their entire journey within the national health service . 
this will require rethinking of the current infrastructure , and might require adjustments to gps case burdens to ensure su cient time is available for more thorough consultations , especially in socioeconomically deprived areas . while the role of the gp in cancer diagnosis is undeniably important , it is essential not to forget interdependency on improved patient education , screening , secondary care and access to latest treatments , supportive and palliative care , and coordinated long - term follow - up . 
 improved understanding of the factors contributing to the di erences between the uks cancer outcomes and those of other countries will provide important clues and solutions . 800 000 people visit a gp every day in the uk , but questions are increasingly being asked about the competency of those doctors that undermine patient trust . 
however , implementation of this bill could be a fresh start in a process of restoring trust and ensuring gps have access to the best tools necessary to provide a rst - class service and to guarantee all patients receive the best possible care . 
this review summarises the present understanding of how mirnas operate at the molecular level ; how their dysregulation is a crucial part of tumour formation , maintenance , and metastasis ; how they can be used as biomarkers for disease type and grade ; and how mirna - based treatments could be used for diverse types of malignancies . introduction micrornas ( mirnas ) are small non - coding rnas ( 2123 nucleotides ) encoded in the genome of plants , invertebrates , and vertebrates . 
these small molecules mainly bind imperfectly to the 3 untranslated region of target messenger rnas ( mrnas ) .1 they negatively regulate gene expression post - transcriptionally by inhibiting translation and causing degradation of target mrna . 
additionally , they are key regulators in many diseaseseg , neurological disorders , heart disease , vascular diseases , viral infection , and cancer.1 the discovery of mirnas led to a worldwide research e ort to establish their roles in cancer . 
 mirnas regulate molecular pathways in cancer by targeting various oncogenes and tumour suppressors , 1 and have a role in cancer - stem - cell biology , angiogenesis , the epithelialmesenchymal transition , metastasis , and drug resistance . 
because mirna - based regulation is dependent on expression of its mrna targets , which are not always ubiquitously expressed , an mirna can have e ects speci c to cells types and conditions . researchers are beginning to uncover the complex role that mirnas have in malignant disease . 
 importantly , this knowledge could be used in the development of anticancer therapies . invaluable regulation of cancer pathways gene regulation and mutations in 2002 , the rst report about the role of mirnas in cancer established that the gene cluster containing the mirnas mir - 15 and mir - 16 is deleted in most people with chronic lymphocytic leukaemia ( cll ) .2 further studies have shown that mir - 15 and mir - 16 act as tumour suppressors by targeting the oncogene bcl2 , which encodes a protein involved in cell survival.3 conversely , mir - 21 is an excellent example of an oncogenic mirna ( a so - called oncomir )  . 
it is overexpressed in most cancerseg , breast cancer , colorectal cancer , lung cancer , pancreatic cancer , glioblastoma , neuroblastoma , leukaemia , and lymphoma.47 overexpression of this mirna can cause tumour growth , maintenance , and survival in vivo.8 importantly , these tumours are completely dependent on expression of mir - 21.8 mir - 21 targets several tumour - suppressor genes , including pten , to increase proliferation and decrease apoptosis.9 , 10 mir - 21 could also promote tumour migration by targeting pro - invasion genes.11 modulation of mirna expression is increasingly thought to be an important mechanism by which tumoursuppressor proteins and oncoproteins exert some of their e ects . 
the proto - oncogene myc transcriptionally activates the mir - 17 - 92 clustera polycistronic transcript of mirnas 17 , 18a , 19a , 20a , 19b - 1 , and 92a - 1.12 the oncogenicity of mir - 17 - 92 is attributed mainly to mir - 19 , which inhibits pten to activate akt signalling and promote cancer - cell survival ( gure 2 ) .13 myc also represses transcription of many tumour - suppressor mirnas , including the let - 7 family.14 reduced expression of let - 7 mirnas is recorded in many cancers , 1 and correlates with poor survival . 
let - 7a , let - 7c , and let - 7g are deleted in lung cancer tumours , and many mirnas of the let - 7 family are located in the genomic region frequently deleted in patients with lung cancer.15 involved the tumour suppressor p53 transcriptionally induces the mir - 34 family of mirnas in response to dna damage ( gure 2 )  . 
mir - 34a is expressed from one genomic site , but mir - 34b and mir - 34c are produced together from one primary transcript at another site.16 , 17 loss of mir - 34a expression is associated with metastasis and recurrence of prostate cancer.18 restoration of mir - 34 in pancreatic cancer cells substantially expression inhibited clonogenic cell growth and invasion , induced vol 13 june 2012 e249 review oncogenic mirnas tumour - suppressing mirnas additionally , genetic variation in the mir - 221 binding site in the 3 utr of kit is associated with a heightened risk of acral melanoma.24 mutations loss of function mutations loss of function oncogenic mirna tumour - suppressing mirna tumour - suppressor mrna oncogene mrna mirna resistance mirna resistance tumour - suppressor mrna oncogene mrna upregulation more transcription gene amplication hypomethylation downregulation less transcription genomic deletion hypermethylation tumour - supressor mrna tumorigenesis oncogene mrna figure 1 : regulation of tumorigenesis by mirnas tumorigenesis can be regulated by mirnas at di erent levels . 
upregulation of oncogenic mirnas reduces expression of tumour - suppressor protein , but downregulation of tumour - suppressing mirnas results in an increased production of oncogenic proteloss - of - function mutations in tumour - suppressing mirnas and mutation of the target section of oncogene mrna can cause tumorigenesis , because expression of oncogenic proteins is no longer regulated . 
similarly , studies of prostate cancer stem cells show that reintroduction of mir - 34a into tumours and cancer cell lines leads to corresponding reductions of cd44 and tumour size.19 expression of mir - 34b and mir34c is lost through deletion or hypermethylation , or is downregulated , in 90% of colorectal cancers.20 , 21 in their absence , both p53 - dependent and p38 - mapk - dependent responses to dna damage are attenuated , leading to oncogenesis.21 , 22 importantly , myc is a target of mir - 34b and mir - 34c , substantiating the inter connected nature of mirna expression in malignancies ( gure 2 )  . gene regulation is not the only way in which mirnas are implicated in malignancies ( gure 1 )  . 
for example , a single nucleotide polymorphism in the 3 utr of the kras oncogene signi cantly increases risk of non - small - cell lung cancer.23 cancer stem cells cancer stem cellsalso called tumour - initiating cells are a small population of cells within a tumour that are thought to arise from somatic stem cells . 
they have enhanced self - renewal capacities , tumorigenic potential , and expression of unique surface markers ; 25 and are often essential for tumour maintenance , treatment resistance , tumour progression , and distant metastasis . 
some mirnas involved in stem - cell regulation are mir - 296 , mir - 134 , mir - 470 , and the mir - 34 family , which targets genes essential for pluripotency and stem - cell function ( eg , oct4 , nanog , sox2 , notch , and bcl2 ) .26 let - 7 in vitro and regulation of cancer stem cells . 
 in breast cancer , let - 7 and mir - 30 are important for the downregulated in breast - cancer stem cells.27 when overexpressed in mice , it can reduce numbers of undi erentiated cells inhibit cell proliferation , tumour formation , and metastasis.28 mir - 30 expression is also low and can inhibit the selfrenewal ability of breast - cancer stem cells . 
the combination of both inhibits self - renewal and mammosphere formation in breast - cancer stem cells.28 let - 7 and mir - 30 angiogenesis promotion of angiogenesis by tumours necessitates activation of proliferation and migration pathways in vascular smooth muscle cells . 
in nasopharyngeal carcinoma cells , the mir - 15a / 16 - 1 cluster regulates angiogenesis ( gure 3 ) by targeting the angiogenic factors vegfa and met.29 mir - 145 blocks migration of vascular smooth muscle cells by inhibiting fli1 , 30 and mir - 143 by targeting the versican protein involved in migration induced by platelet - derived growth factor.31 the mir - 143 cluster is downregulated in cancers of the prostate , colon , gastric , and bladder , and in cll and b - cell lymphomas.32 transition the epithelialmesenchymal epithelialmesenchymal transition and metastasis epithelial cells undergo several molecular changes during assume a mesenchymal cell phenotype necessary for tumour metastasis and progression ( gure 3 ) .33 expression of e - cadherin ( cdh1 ) is essential for retaining an epithelial cell type . 
similarly , expression of mir - 200 in breast cancers is positively correlated with concen trations of e - cadher the e250 vol 13 june 2012 review importance of this association is supported by evidence that restoration of mir - 200 expression is su cient to reverse the transition ( ie , mesenchymal to epithelial ) in a kidney - derived cell line.34 however , other mirnas are needed epithelialmesenchymal the transition . 
in pancreatic epithe lial cells , the expression of mirnas from the mir - 30 family inversely correlates with the mesenchymal pheno type.35 in mesenchymallike ovarian cancer cell lines , overexpression of mir429 reverses the transition.36 to prevent the to supplement clinical potential diagnosis and classi cation the development of cytogenetic , immunological , and traditional molecular methods morphological classi cation systems has re ned the identi cation of cancer subtypes.37 for instance , transcriptome pro ling studies of di erent cancer types with large - scale genomic approaches showed that a 97 - gene expression pro le is better for classi cation of breast cancer histological grade than are lymph - node status and tumour size.37 gene - expression pro ling has also led to development of breast - cancer prognostic pro ling tests , which have been approved for clinical use.38 as with mrna , whole - genome mirna pro ling has shown that mirna expression changes substantially in most human cancers.39 mirna expression signatures provide a more accurate method of cancer subtype classi cation than does expression pro ling of an entire group of known protein - coding rnas.40 mirna pro les can contribute to the diagnostic and prognostic classication of human malignancies ( table ) .2 , 4148 the use of the traditional , gold standard , histological examination in the diagnosis and classi cation of cancers can be limited by availability of adequately preserved tissue and the possibility of subjective interpretation by pathologists . 
by contrast , mirnas show resistance to degradation and their expression levels can be established in a few hours with as little as 10 ng of total rna ; therefore , mirnas are ideal as both diagnostic and prognostic indicators in clinical settings . screenings of resected tumours and biopsy samples have identi ed mirna signatures that can be used to di erentiate between malignant and benign condi tions in several organs . 
seven mirnas are di erentially expressed in biopsied pancreatic ductal adenocarcinomas compared with benign and healthy tissues.49 a multi centre trial50 showed that use of signatures from these mirnas gives greater accuracy than does conventional cytology . 
one mirna was overexpressed in 19 of 20 malignant samples.51 mirna expression can also be used to identify well characterised genotypeseg , to distinguish between dna damage drosha mir - 34 carcinogenesis mirna processing mir - 17 - 92 cluster pten figure 2 : oncogenic and tumour - suppressing mirnas in the dna damage response dna damage can lead to the upregulation of the mir - 34 family through the activation of the p38 map - kinase and p53 pathways . 
 vol 13 june 2012 e251 review these two mirnas are deleted or down regulated in 68% of patients with cll.2 furthermore , cll can be classi ed into ve di erent categories according to genetic instabilities ( deletion of chromosomal regions 11q , 13q , and 17p ; trisomy 12 ; and normal karyotype )  . 
studies show that the speci c expression pattern of 32 individual mirnas can di erentiate between these di erent chromosomal abnormalities ( table ) .42 other forms of genomic instability can be inferred with mirna pro ling ( table )  . prognostic indicators many identi ed genotypes are associated with distinct prognoses ( table )  . 
by comparing two main groups of patients with good prognosis ( low zap70 expression , mutated immunoglobulin variable region genes ) and poor prognosis ( high zap70 , immunoglobulin variable region genes not mutated ) , they identi ed 13 mirnas with variable expression according to prognosis ( table ) .41 prognosis or outcome microrna expression reference chronic lymphocytic leukaemia high zap70 ; immunoglobulin variable region not mutated poor 13q14.3 deletion indolent 17p deletion aggressive calin41 calin2 visone42 mir - 15a mir - 16 - 1 mir - 16 - 2 mir - 195 mir - 221 mir - 23b mir - 155 mir - 24 - 1 mir - 146 mir - 223 mir - 29a - 2 mir - 29b - 2 mir - 29c mir - 15a mir - 16 - 1 mir - 130b mir - 129 - 3p mir - 632 mir - 768 - 5p mir - 638 mir - 453 mir - 29b / c mir - 181b / c / d mir - 342 - 3p mir - 223 mir - 181a mir - 367 mir - 205 mir - 96 mir - 182 mir - 183 down down down down down down down down down down down down disease progression mir - 181 visone42 trisomy 12 lung cancer non - squamous non - small - cell lung cancer ( stages ii , iii , and iv ) and lymph - node metastasis poor lebanony43 zhu44 zhu44 zhu44 ( continues on next page ) in lung cancer , researchers focusing on the mir - 183 family of mirnas ( mir - 183 , mir - 182 and mir - 96 ) have recorded a link between the expression of these mirnas and progression of non - small - cell lung cancer . 
expression of the mir - 183 family can also help to identify tumours with heightened lymph - node metastasis ; an increased likelihood of progression to stage ii , iii , or iv ; and poor survival ( table ) .44 many biomarkers are prognostic indicators for breast cancer . 
the two most common are the oestrogen receptor , expression of which predicts a good outcome ; and her2 , which when over expressed is associated with poor outcome , anti - oestrogen treatment resistance , and metastasis.53 although identi cation of these two markers has been invaluable for breast cancer management , other molecular methods are needed for classi cation of subtypes . 
analysis of 93 breast - cancer samples showed that speci c patterns of mirna expression were associated with breast - tumour subtypes of di erent clinical outcomes.45 one investigation45 showed that expression of 31 mirnas was signi cantly associated with clinical factors . 
14 were overexpressed in grade iii , oestrogen - receptor - negative malignancies of basal - like subtype , seven of which were also associated with her2 - overexpressing cancers.45 import antly , six were related to the same clinical outcomes in another independent dataset ( table ) .46 although the expression pattern of several mirnas can give useful information about stage and prognosis , one mirna alone can have accurate predictive power . 
 the predictive e ect of mir - 210 was so strong that the researchers noted that the overexpression of mir - 210 alone allowed prediction of prognosis to the same level as a 76 - gene mrna signature test ( gene76 )  . 
overexpression of mir - 210 is associated with an increased risk of recurrence and a reduced chance of relapse - free survival.46 in cll with trisomy 12 , when expression of immuno globulin variable region genes and zap70 does not predict clinical outcome , the overexpression of one mirna , mir - 181 , can predict disease progression ( table ) .42 to colorectal cancers resistant mirna pro ling can identify treatment - resistant cancers . 
as with overexpression of her2 in breast cancer , overexpression of four mirnas have been linked to egfr antagonists.48 screening for mirnas could enable treatment to be tailored to individual patients and thus increase the chances of survival . 
urine cytology of speci c markers can also be used but this method does not have the sensitivity biomarkers in body uids although mirna pro ling of tumours could be an excellent prognostic test , invasive procedures such as biopsy , aspiration biopsy , or excision surgery of alreadyexisting tumours are necessary to obtain samples . 
an ideal biomarker should be accessible with non - invasive methods , sensitive enough to detect early presence of tumours before clinical symptoms present , and absent or low in healthy , tumour - free individuals.54 stable , degradationresistant , extracellular mirnas could be detected in body uids such as serum , urine , saliva , tears , breast milk , seminal uid , and faecal matter . 
one breast cancer study comparing the circulating mirna pro le in healthy women with that of those with early - stage breast cancer62 showed that downregulation of mir - 181a and mir - 1304 is associated with the disease . 
mir - 195 and let - 7a concentrations are higher in the plasma of patients with breast cancer than in healthy individuals.62 after tumourexcision surgery , postoperative serum concentrations of both these mirnas return to values reported in the healthy control group.59 researchers investigating the plasma levels of mirnas in 74 patients diagnosed with di erent types of lung cancer63 identi ed three mirnas ( mir - 155 , mir - 197 , and mir - 182 ) that were at a higher concentration in patients with cancer than in control individuals . 
 the serum the investigators also reported that vol 13 june 2012 e253 review for detection of low - grade bladder cancer , 64 driving the search for new speci c and sensitive biomarkers . 
 a proof - of - concept study65 showed that mir - 126 , mir - 182 and mir - 199a concentrations are signi cantly increased in the urine of patients with stage 1 bladder cancer , as well as in those with stage 2 and stage 3 disease . 
 the concentration of these markers in urine continues to increase as malignancy progresses and decreases after tumour - excision operations.65 for those with a positive for colorectal cancer , patients older than 60 years are o ered screening every 2 years with non - invasive faecal occult blood testing , 66 with a subsequent colonoscopic result . 
 investigation unfortunately , the test has only 3350% sensitivity ; use of novel biomarkers would prevent many healthy individuals undergoing an expensive , painful procedure with the risk of serious medical complications.67 mir - 21 and mir - 106 are upregulated in the stool of patients with colorectal neoplasia ( colorectal cancer or adenoma )  . 
mir144 * is increased in the faeces of patients with colorectal cancer with a sensitivity of 74% and a speci city of 87% , and is thus another potential biomarker to help diagnosis of colorectal cancer.68 samples extracted with the faecal blood - test kits could also be used to extract mirnas ; clinicians could undertake both tests simultaneously to increase the sensitivity of diagnosis.67 mirnas as cancer treatment the development of new treatments has contributed substantially to increased 5 - year survival and the reduction in overall mortality rates.62 , 69 however , although the classi cation of cancers has become increasingly diver si ed , the variety and speci city of treatment options has lagged behind . 
more than 2000 gene - therapy - based clinical trials are in progress for various illnesses , but only one is of mirna treatment.32 treatment can be targeted to mirnas in two ways : mirna reduction and mirna replacement ( gure 4 )  . 
new mirna - based treatments would need to have selective and accurate delivery of the agents to the target tumours to increase the therapeutic potential and reduce possible side - e ects . two major di culties have impeded development of mirna - based treatments . 
first , rna has low stability in vivo ; mirna introduced into mice via the tail vein is cleared from the circulatory system in 30 min.70 unmodi ed , saline - formulated , double - stranded rna injected intravenously undergoes rnase - mediated degradation and rapid renal excretion . 
an increase could be achieved by improved mirna stability or by protection from rna - hostile environments . substitution of phosphodiester by phosphorothioate in the rna backbone , and of the ribose moieties to 2 - o - methyl or other 2 substitutions confer substantial nuclease resistance.71 locked nucleic acid ( lna ) is a modi ed rna nucleotide that has an extra bridge connecting the 2 oxygen and 4 carbon . 
these modi cations increase the thermostability of lna - rna duplexes , increase target speci city , and are resistant to exonucleases and endonucleases , thereby improving stability of mirnas in vitro and in vivo.72 finally , introduced rna can be conjugated to a cholesterol moiety , increasing stability in the circulation . 
for example , an antagonist of mir - 16 with 2o - methyl modi ed nucleotides and cholesterol linked to its end via a hydroxyprolinol linkage is stable and e ciently silences mirna expression.73 protection from hostile environ ments is typically achieved by encasing of lna or mirna mimics in nanoparticles to form micelle - like structures ( gure 4 )  . the second di culty is how to ensure tumour - speci c delivery and retention of mirnas . 
e orts to achieve targeted delivery could be further hindered by rst - pass metabolism and rapid localisation of small molecules delivered systemically to the kidney and liver.74 targeted delivery to speci c tissues can be done when tumour - speci c ligands are linked to nanoparticles , which can be directed to tumour cells via active or passive targeting . 
nanoparticles between 15 nm and 100 nm are the best for systemic delivery.76 active targeting of nanoparticles necessitates their conjugation with di erent compounds that have a speci c a nity to tumours . 
various cancer - associated cell - surface proteins ( eg , her2 , 77 egfr , 78 and ca - 12579 ) and hyaluronic acid80 could potentially be used for this conjugation . 
investigators have developed a poly ( ethylene glycol ) hyaluronic acid nanoparticle ( p - ha - np ) that can be used to deliver doxorubicin and camptothecin to mouse cells.81 the nanoparticles were internalised successfully into cancer cells ( scc7 and mda - 3t3 ) , but rarely taken up by normal broblasts ( nih - 3t3 )  . 
tumour - bearing mice were systemically treated with camptothecin de livered with p - ha - np , and tumour growth was success fully stopped for at least 35 days . 
these nanoparticles could e254 vol 13 june 2012 review mirna modied rna target mrna nanoparticle antibody cancer - specic ligands cell membrane figure 4 : mirna - based treatment in mirna reduction treatment ( a ) , single - stranded lna molecules ( anti - mirnas ) bind to mirnas complementarily , preventing the mirnas from binding to target mrnas . 
 possibly be modi ed to carry mirnas to speci cally targeted cancer stem cells.81 furthermore , integrin - - 3 - targeted nanoparticles used to deliver anti - mir - 132 had promising results in inhibition of angiogenesis and breast tumour metastasis.82 the goal of mirna replacement is the reintroduction of mirnas depleted in cancer cells and the reactivation of cellular pathways that drive a therapeutic response . 
 trang and co - workers70 concluded that a chemically synthesised mir - 34a packaged into a lipid - based delivery vehicle and given locally or systemically could block tumour growth in mouse models of non - small - cell lung cancer . 
systemic delivery of formulated mir - 34a did not induce a rise in cytokines or liver and kidney enzymes in serum , suggesting that the formulation is well tolerated and that side - e ects could be negligible . 
similar results were noted in another study of a mouse model of non - smallcell lung cancer with activated kras ; 70 an mir - 34a or let - 7 mimic mirna formed a complex with a neutral lipid emulsion , which led to a 60% reduction in tumour area.70 additionally , systemic delivery of atelocollagenconjugated mir - 16 in a mouse xenograft model of prostate cancer inhibited metastasis into bone.83 mirna reduction with lna has been done with antimir - 21 to treat autoimmune splenomegaly in mice with systemic lupus erythematosus ; 84 mir - 21 is upregulated in all subsets of lupus mouse lymphocytes . 
targeting of mir - 21 with an intraperitoneally injected lna - based antagonist decreases manifestation of cardinal systemic lupus erythematosus and leads to the reversal of splenomegaly.84 the only mirna - based treatment tested in people is anti - mir - 122 for the treatment of infection with hepatitis c virus ( hcv )  . 
mir - 122 is an essential mirna for hcv replication and is predominantly in the liver.85 in 2010 , data from a drug trial of an intravenously delivered lna to remove mir - 122 and stop infection in chimpanzees was reported.86 lna given to chronically infected chim panzees once a week for 12 weeks led to a reduction in viral load in the serum and the liver . 
a phase 1 trial87 in 77 healthy volunteers established that anti - mir - 122 is safe and vol 13 june 2012 e255 review search strategy and selection criteria data for this review were identi ed by searches of pubmed with the term microrna in combination with cancer , in vivo , circulating , systemic delivery , therapeutics , or lna . 
the subsequent phase 2a trial87 assessed the safety and antiviral activity of subcutaneous anti - mir - 122 given at doses of 3 mg / kg , 5 mg / kg , and 7 mg / kg every week for 29 days ; patients were followed up until week 18 . 
this trial87 drew attention to the potential of lnas for cancer treatment . conclusion the discovery of mirnas has changed the way control of gene expression is thought about and , perhaps more importantly , has set a precedent for the development of new diagnostic methods and treatments of diseases , including malignancies . 
in the long term , work to identify major mirna targets and to develop safe and speci c methods of delivery of mirna - based treatments could allow modulation of mirnas to become a central feature of cancer treatment and management . contributors ywk and df - m did the literature search , wrote and edited the report , and designed the gures . 
mb wrote and edited the report . con icts of interest ywk and mb have led a patent relating to microrna delivery with nanoparticles conjugated to cancer - targeting anti - cd4 antibodies . 
we present a pre - planned preliminary safety analysis of side - e ects in stages 1 and 2 of a randomised trial comparing standard and hypo fractionated radiotherapy . methods we did a multicentre , randomised study and recruited men with localised prostate cancer between oct 18 , 2002 , and aug 12 , 2006 , at 11 uk centres . 
patients were randomly assigned in a 1 : 1 : 1 ratio to receive conventional or hypofractionated high - dose intensity - modulated radio therapy , and all were given with 36 months of neoadjuvant androgen suppression . 
this study is registered , number isrctn97182923 . findings 153 men recruited to stages 1 and 2 were randomly assigned to receive conventional treatment of 74 gy , 153 to receive 60 gy , and 151 to receive 57 gy . 
 for bladder toxicities , three ( 22% ; 0562 ) of 138 men , three ( 22% ; 0563 ) of 137 , and none ( 00% ; 975% ci 0026 ) of 143 had scores of grade 2 or worse on the rtog scale at 2 years . interpretation hypofractionated high - dose radiotherapy seems equally well tolerated as conventionally frac tionated treatment at 2 years . funding stage 1 was funded by the academic radiotherapy unit , cancer research uk programme grant ; stage 2 was funded by the department of health and cancer research uk . introduction prostate cancer is the most common cancer in men in the uk , usa , and western europe , with 37 000 men diagnosed in the uk and an estimated 913 000 cases worldwide in 2008.1 after the introduction of prostatespeci c antigen ( psa ) testing , most men diagnosed have localised disease . 
management options include externalbeam radiotherapy , brachytherapy , radical prostatectomy , active surveillance ( for men with low - risk disease ) , and watchful waiting ( for those unsuitable for radical curative treatment )  . 
external - beam radiotherapy might be most appropriate for men with disease features of intermediate or high risk , 2 , 3 and is associated with long - term disease control in most patients.4 about 10 000 men receive radical prostate radiotherapy in the uk every year.5 substantial technological advances over the past decade have improved both the ability to adjust dose distributions to the prostate target and treatment accuracy . 
several phase 3 randomised control trials have shown the bene t of dose escalation , 6 and high - dose conformal radiotherapy with conventional 2 gy daily fractions to a total dose of 74 gy has become the standard of care in the uk.7 additionally , there has been interest in the fraction sensitivity of prostate cancer.810 the ratio for most cancers is believed to be about 10 gy , but for prostate cancer values as low as 15 gy have been suggested , which is smaller than the roughly 3 gy reported for the late reactions of most normal tissues ( including rectum ) .11 these ndings have potentially important therapeutic implications . 
hypofractionated radiotherapy with fewer high - fraction - size treatments would be bene cial for prostate cancer because it would deliver a larger biological - equivalent dose to the tumour than would conventional treatment in 1820 gy fractions , while vol 13 january 2012 articles see online for appendix maintaining a similar or lower incidence of late normal tissue reactions . 
furthermore , improved resource use and patient convenience because of short treatment duration would be important gains . maintenance of few treatment - related side - e ects is of paramount importance , because they increase with dose escalation . 
in previous dose - escalation randomised controlled trials ( with di erences of 810 gy between groups ) , variations in side - e ects of 1015% have been reported.6 meta - analysis showed an odds ratio of 158 for late gastrointestinal toxicity of grade 2 or more , in favour of conventional rather than high - dose radiotherapy.6 we therefore aimed to compare a conventional radiotherapy schedule with hypofractionated schedules in prostate cancer . methods trial design we undertook a multistage , multicentre randomised trial ( conventional or hypofractionated controlled high - dose intensity modulated radiotherapy in prostate cancer ; chhip )  . 
we used a three - arm design to ensure that we would be able to extrapolate an isoe ective dose for a speci c rate of complications ( in a similar way to the large uk breast fractionation trials ) .12 biological doses in the experimental schedules were calculated to be equivalent to those in the conventional schedule ; equivalence was achieved with the assumptions that ratios were 25 gy for the 60 gy group and 15 gy for the 57 gy group.9 all treatment groups received conformal and intensity - modulated radiation techniques . 
 this report is a pre - planned analysis of stages 1 and 2 of this trial , with the object ive of establishing the safety of experimental hypofractionated radiotherapy schedules . patients patients were recruited to stage 1 between oct 18 , 2002 and april 27 , 2005 , at the royal marsden nhs trust ( london , uk ) and clatterbridge centre for oncology nhs foundation trust ( wirral , uk ) ; and to stage 2 between may 4 , 2005 , and aug 12 , 2006 , at 11 uk centres ( see appendix )  . 
men with histologically con rmed t1bt3a n0 m0 prostate cancer , 13 psa concentrations of less than 30 ng / ml , estimated risk of lymph - node involvement less than 30% , 14 and who performance status 0 or 1 were eligible . 
patients were excluded if they had t3 tumours and a gleason score of 8 or more , a life expectancy of less than 10 years , previous pelvic radiotherapy , previous androgen suppression , another active malignancy in the past 5 years ( other than cutaneous basal - cell carcinoma ) , comorbid conditions precluding radical radiotherapy , full anticoagulation treatment , or hip prosthesis . chhip ( cruk / 06 / 016 ) was approved by the london multi - centre research ethics committee ( 04 / mre02 / 10 ) and the local ethics committees of all participating centres . 
the trial was coordinated by the royal marsden hospital bob champion unit ( sutton , uk ) and the institute of cancer research clinical trials and statistics unit ( icr - ctsu ; sutton , uk ) , in which central statistical monitoring and all analyses were done . 
both committees approved reporting of this pre - planned analysis of side - e ect data to 2 years from patients recruited in stages 1 and 2 . randomisation and masking men were registered in the trial before or after starting initial hormone therapy . 
treatment allocation was not masked and , because of the trials size , assessors could not be blinded to toxicity or clinical assessments . treatment as part of standard treatment , men received short - course androgen suppression for 36 months before and during radiotherapy , although it was optional for men with low - risk disease . 
injections of a luteinising - hormonereleasing hormone ( lhrh ) analogue every month , combined with initial antiandrogen to reduce testosterone are , or an antiandrogen alone , were allowed . individuals in the control group received prostate radiotherapy with standard 2 gy daily fractions ( monday to friday treatment ) for 74 weeks to give a total dose of 74 gy in 37 fractions . 
patients in the experimental groups were given hypofractionated treatment with 3 gy daily fractions to a total dose of either 60 gy in 20 fractions in 40 weeks or 57 gy in 19 fractions in 38 weeks . 
a complex forward - planned multisegment technique was developed for the trial.15 target and treatment planning volumes have been previously described.15 treatment was planned and delivered using an integrated simultaneous - boost technique with target volumes designed to give the conventional 74 gy group : a dose of 59 gy ( 80% ) to the prostate and base or all seminal vesicles , with a uniform 10 cm margin ; a dose of 71 gy ( 96% ) to the prostate with a 10 cm margin , except posteriorly where the margin was reduced to 05 cm ; and 74 gy ( 100% ) to the prostate with a margin of 05 cm ( 00 cm posteriorly )  . 
pelvic lymph nodes were not included in the target volumes . for the hypofractionated groups , similar proportions of the prescribed dose ( ie , 60 gy or 57 gy ) were given to vol 13 january 2012 articles for more on the phantom see 457 patients randomised 153 allocated to 74 gy in 37 daily fractions of 2 gy 153 allocated to 60 gy in 20 daily fractions of 3 gy 151 allocated to 57 gy in 19 daily fractions of 3 gy 4 did not receive treatment 1 ineligible 1 technically unsuitable 2 patient choice 6 did not receive treatment 1 ineligible 4 technically unsuitable 1 unknown 3 did not receive treatment 2 ineligible 1 unknown 149 received allocated treatment 148 had planned dose 1 less than planned dose 147 received allocated treatment 147 had planned dose 148 received allocated treatment 148 had planned dose 11 not evaluable for rtog toxicity at 2 years 4 died 1 withdrew consent 5 missing forms 1 missing data 10 not evaluable for rtog toxicity at 2 years 1 died 1 withdrew consent 2 lost to follow - up 4 missing forms 2 missing data 5 not evaluable for rtog toxicity at 2 years 2 died 1 lost to follow - up 2 missing forms 138 evaluable for rtog toxicity at 2 years 132 complete set of follow - up forms 6 missed some assessments 137 evaluable for rtog toxicity at 2 years 134 complete set of follow - up forms 3 missed some assessments 143 evaluable for rtog toxicity at 2 years 138 complete set of follow - up forms 5 missed some assessments figure 1 : trial pro le for chhip stages 1 and 2 a complete set of follow - up forms means that the patient completed 6 , 12 , 18 , and 24 month follow - up forms ; follow - up forms completed after 2 years not included . 
portal imaging was used to verify treatment accuracy , which was to be within 3 m a quality - assurance programme was designed as an integral part of the study . 
before trial entry began , every centre completed a process document that de ned the methods to be used for ct simulation , treatment planning , and veri ed treatment accuracy and dosimetry . 
during the trial , on - site quality - assurance visits measured the accuracy of treatment delivery and dosimetry with a trial - speci c phanto details of target volumes , dose parameters , constraints , and the proforma used to record each patients dose distribution are given in the appendix . assessments staging included psa measurement , standard haematology and biochemistry , lymph - node assessment by pelvic mri or ct , and bone scan for patients investigations at intermediate or high risk.2 , 3 histology was locally assessed with diagnostic transrectal ultrasound - guided biopsies ( or specimens from transurethral resection of the prostate ) and reported with the gleason system . bowel , bladder , and sexual function assessments were made before hormone therapy ( when the patient was already registered for the trial ) ; before radiotherapy ; every week during radiotherapy ; and at weeks ten , 12 , and 18 to assess acute toxicity , with subsequent assessments at 26 weeks and every 6 months for 5 years . 
initial symptoms and radiotherapy side - e ects were graded with the late e ects on normal tissues : subjective / objective / management ( lent / som ) 16 and royal marsden hospital ( rmh ) 17 scoring systems . 
radiotherapy side - e ects were also graded with the radiation therapy oncology group ( rtog ) scoring system.18 statistical analysis stage 1 included 150 patients ( 50 per treatment group ) and was powered ( 878% power ; 0045 one - sided ) with a one - stage fleming - ahern design19 to rule out an upper limit of 25% of patients with rtog grade 2 or worse bladder or bowel complications at 2 years for each experimental group , with an expected rate of 10% in the control group . 
data presented for patients who started radiotherapy ( n = 149 in the 74 gy group , n = 147 in the 60 gy group , and n = 148 in the 57 gy group )  . table 1 : baseline demographic and clinical characteristics and treatment details by allocated treatment group 2 years . 
 the sample size ( stage 1 plus stage 2 ) was set at 450 patients ( 150 per group ) , with a 10% allowance for dropout . analyses of side - e ect data for prevalence were done according to treatment received andwith the exception of com parisons at 18 weeksincluded all available assessments from all patients who received at least one fraction of radiotherapy . 
the 18 week comparison was restricted to assessments done in a period 2 weeks either side of this time to consistently capture the end of the acute toxicity period across treatment groups . for the primary endpoint , only patients with an rtog assessment at 2 years were included in analyses , although we did a sensitivity analysis that included all patients . 
time to rst occurrence of late ( reported on follow - up forms from 6 months after the start of radiotherapy onwards ) side - e ects of di erent grades were compared with the kaplan - meier method used to calculate cumulative proportion of patients that had events by 2 years . 
analyses presented in this report have not been adjusted for strati cation factors , but sensitivity analyses adjusting for risk group showed the results to be robust ( data not shown )  . analyses were based on a database snapshot on april 1 , 2010 , and were done with stata version 112 . 
 this study is registered , number isrctn97182923 . role of the funding source the funding source provided peer - reviewed approval for the trial , but had no other role in study design , collection , analysis , interpretation of data , or writing of the report . 
13 patients received no radiotherapy : four were ineligible at trial entry , ve were shown to be technically unsuitable during the planning process , two patients chose to leave , and two for unknown reasons . 
overall , six patients were ineligible : one had abnormal blood counts , two were receiving warfarin , one had stage t3b disease , one had hip prostheses , and one had a perianal stula ( two ineligible patients did receive radiotherapy )  . 
of the 444 treated patients , all but one received the protocolassigned radiotherapy dose and schedule ; one patient in the 74 gy group stopped treatment after 70 gy because of acute urinary obstruction . median follow - up is 505 months ( iqr 435613 ) ; 426 of 457 patients randomly assigned and 424 of 444 treated have been followed up for at least 2 years . 
 most patients received lhrh analogues and short - term antiandrogens ( table 1 ) , similarly distributed across treatment groups and by risk group of the national comprehensive cancer network . acute bowel and bladder side - e ects , measured with the rtog scale , seemed to peak sooner in the experimental groups than in the control group ( gure 2 ) : at 45 weeks in the hypofractionated groups compared with 78 weeks in the control group . 
of 129 patients in the 74 gy group who were assessed 18 weeks after start of radiotherapy , three ( 23% ) reported bowel side - e ects of rtog grade 2 or worse and nine ( 70% ) had bladder side - e ects of grade 2 or worse . 
grade 3 bladder side - e ects were reported by two patients who received 57 gy , and one patient in the 74 gy group had a grade 4 event . 
no acute grade 3 bowel toxicity was reported . late side - e ect pro les by treatment group as reported on each scoring system are shown in gures 3 and 4 . 
cumulative proportion figures only include events occurring up to 2 years post - radiotherapy and are calculated with the kaplan - meier method . table 2 : total number of events , hazard ratios , and cumulative proportion with events by 2 years for bowel , bladder , and sexual dysfunction endpoints by allocated treatment group rtog toxicity scores at 2 years were available for 138 men given 74 gy , 137 given 60 gy , and 143 given 57 gy . 
none of the estimates of late toxicity suggested a doubling of sidee ects in the experimental groups compared with the standard group and , because the upper con dence limits are all less than 20% , the criteria for rejection of any of the treatment groups on the grounds of safety were not met . 
results from the sensitivity analysis that included all patients suggested that the ndings are robust to missing outcomes ( data not shown )  . vol 13 january 2012 articles 74 gy g1 + 74 gy g2 + 74 gy g3 + 60 gy g1 + 60 gy g2 + 60 gy g3 + 57 gy g1 + 57 gy g2 + 57 gy g3 + time from start of radiotherapy ( months ) number of patients assessable 74 gy 153 60 gy 153 57 gy 151 141 143 141 142 138 145 139 138 138 time from start of radiotherapy ( months ) 74 gy g1 + 74 gy g2 + 74 gy g3 + 74 gy g4 60 gy g1 + 60 gy g2 + 60 gy g3 + 60 gy g4 57 gy g1 + 57 gy g2 + 57 gy g3 + 57 gy g4 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy 74 gy 60 gy 57 gy time from start of radiotherapy ( months ) grade 0 grade 3 grade 1 grade 4 grade 2 figure 5 : lent / som sexual dysfunction toxicity of the three treatment groups by assessment timepoint ( a ) cumulative proportion . 
the cumulative proportion of patients with late rtog bowel toxicity of grade 2 or worse at 2 years was 76% ( 95% ci 43132 ) in the 74 gy group , 69% ( 38125 ) in the 60 gy group , and 48% ( 2397 ) in the 57 gy group ( gure 3 ; table 2 )  . 
 for late rtog bladder toxicity , cumulative proportion values were 35% ( 1581 ) , 90% ( 54151 ) , and 48% ( 2398 ; gure 4 , table 2 )  . 
there were no statistically signi cant di erences in cumulative incidence of sidee ects between the groups . with the rmh symptom score , there was low prevalence of bowel scores of grade 2 or worse before radiotherapy on either of the baseline scores ( ie , before hormone or radiotherapy treatment ; eight of 451 patients )  . 
 at 2 years , eight ( 58% ) of 138 patients given 74 gy had rmh bowel scores of grade 2 or worse , four ( 29% ) of 138 patients given 60 gy , and one ( 07% ) of 143 patients given 57 gy . 
prevalences of bladder scores of grade 2 or worse were similar in the three groups before radiotherapy : 25 ( 172% ) of 145 men given 74 gy , 22 ( 151% ) of 146 given 60 gy , and 21 ( 147% ) of 143 given 57 gy . 
rmh bladder scores of grade 1 or worse were recorded in 61 ( 439% ) of 139 men given 74 gy , 39 ( 283% ) of 138 given 60 gy , and 50 ( 350% ) of 143 given 57 gy . with the lent / som assessment system and the maximum score for each normal tissue , the prevalence of bowel scores of grade 2 or worse before hormone or radiotherapy treatments was 39% ( 17 of 439 patients )  . 
 grade 1 scores or worse were reported in 19 ( 135% ) of 141 patients in the 74 gy group , 16 ( 110% ) of 146 in the 60 gy group , and 15 ( 106% ) of 142 in the 57 gy group at the assessment before radiotherapy . 
the prevalence of bowel symptoms at 2 years was higher in the 74 gy group than in the other two groups , with 31 ( 225% ) of 138 patients in the 74 gy group experiencing grade 1 events , 13 ( 94% ) experiencing grade 2 events , and two ( 14% ) experiencing grade 3 events versus 23 ( 168% ) of 137 men in the 60 gy group experiencing grade 1 events , seven ( 51% ) experi encing grade 2 events , and one ( 07% ) experiencing grade 3 events , and 22 ( 155% ) of 142 men in the 57 gy group experiencing grade 1 events , six ( 42% ) experi encing grade 2 events , and one ( 07% ) experiencing grade 3 events ( p = 0023 )  . 
the 6 , 12 , 18 , and 24 month scores after radiotherapy all showed signi cant to preradiotherapy levels ( p = 00001 for 6 month scores ; p < 00001 for other timepoints )  . increases compared before hormone treatment , 45 ( 188% ) of 239 patients had lent / som grade 1 bladder scores , 61 ( 255% ) had grade 2 scores , and 26 ( 109% ) had grades 3 or 4 . 
as expected , scores deteriorated during neoadjuvant hormone therapy , with 350 ( 835% ) of 419 men recording scores of grade 2 or worse before radiotherapy ( p < 00001 )  . 
partial recovery was reported : scores of grade 2 or worse were reported in 310 ( 754% ) of 411 patients 24 months after radiotherapy treatment ( gure 5 )  . 
lent / som sexual dysfunction scores were not signi cantly di erent in randomised groups at any point ( table 2 )  . discussion this planned interim analysis of stages 1 and 2 of the chhip trial has shown no clinically meaningful di erences in acute toxicity between standard and hypofractionated radiotherapy schedules . 
the safety criteria for stopping were not met and the trial completed accrual in june , 2011 . acute reactions occurred earlier in the hypofractionated groups than in the control group , in which the pattern of acute toxicity was very similar to that reported in the group of men randomised to receive 74 gy in a previous trial.17 however , the cumulative proportion of both bowel and bladder side - e ects at 2 years is lower in the chhip trial than in the 74 gy group in the previous trial ( in which incidence of rtog bowel toxicity of grade 2 or worse was 20% and bladder toxicity of grade 2 or worse was 8% ) .20 this di erence might be a result of patient selection factors ( although age and psa distributions are very similar ) , or of the favourable dose distributions panel : research in context systematic review before the chhip trial began , reports based on retrospective series of patients suggested that the ratio for prostate cancer might be low , 810 but only two small randomised trials ( with relatively low doses of radiotherapy ) existed and neither was large enough to con rm or refute a bene t.31 , 32 since chhip started , reviews33 , 34 of two large patient databases have been done , suggesting that the best estimates for the ratio are 37 gy and 14 gy . 
however , conformal and intensity - modulated radiotherapy improves dose distributions of radiotherapy and conformal radiotherapy reduces side - e ects . interpretation the ndings from this pre - planned safety analysis of the rst 457 patients enrolled in the chhip trial suggest that high - dose hypofractionated schedules using 3 gy fractions and intensity - modulated radiotherapy are safe . 
safety and e cacy data from the full trial is essential to fully assess hypofractionated schedules , but these safety results should enable investigators to safely pursue these avenues of research . 
clinicians and patients should be strongly encouraged to support trials using fractions of 3 gy or more . and adherence to normal tissue dose constraints with the forward - planning or inverse - planning methods used in the chhip trial.15 data from randomised controlled trials have shown that treatment technique , 21 planning target margin , 22 and dose , 2226 can all a ect outcomes of prostate cancer radiotherapy . 
therefore , meaningful assessment of the biological e ects of altered fractionation schedules can be made only by controlling for these other factors . although not included as part of this safety analysis , we have measured patient - reported outcomes with the same instruments as those used in the previous trial.17 this continuing longitudinal quality - of - life substudy that recruited 1958 men will help to establish whether altered fractionation a ects di erent symptom complexes27 and will be analysed and published separately . the choice of treatment in our control group was based on level 1 evidence and a meta - analysis of trials assessing dose escalation6 and the addition of hormonal therapy28 , 29 for men with intermediate - risk and high - risk disease . 
 the dose of 74 gy was preferred to a higher dose because it has become the standard dose in the uk7 after the mrc rt01 trial , 20 which is the largest reported study of dose escalation and the only study to routinely include shortcourse androgen suppression . 
the median duration of androgen suppression of 5 months is roughly what was recommended in the updated trog 96.01 trial that compared radiotherapy alone with the addition of either 3 or 6 months of androgen deprivation.30 the experimental high - dose hypofractionated groups were designed as they were because retrospective data reviews have suggested that the ratio might be low ( panel ) .8 , 10 large multicentre reviews and a metasummary3335 have suggested estimates of 37 gy , 34 and 14 gy.33 however , a 2008 review36 of studies that used altered hypofractionated treatments showed that evidence is insu cient to recommend a change to doses larger than 2 gy per fraction and that results from continuing randomised controlled trials were needed . 
4 week schedules with 3 gy fractions were chosen because there was some data and experience with similar , but lower dose schedules in the uk.37 other investigators of international studies of hypofractionated radiotherapy have also reported favourable toxicity . 
a small italian phase 3 trial38 included 168 men and was designed to establish whether a high - dose hypofractionation schedule ( 62 gy in 31 gy daily fractions ) was associated with lower radiation - related toxicity than was a high - dose conventional schedule ( 80 gy in 2 gy daily fractions )  . 
frequency of side - e ects after 3 years of follow - up and psa control was reported to be at least as good in the hypofractionated cohort as in the control group ( psa control 87% vs 79% , p = 004 ) .38 additionally , reports from phase 1 or 2 trials of high - dose hypofractionated radiotherapy treatments in prostate cancer are encouraging . 
late bowel side - e ects ( rtog grade 2 or worse ) have been reported in 4% , 55% , and 63% and late bladder side - e ects in 42% , 56% , and 43% of men after 25 years of follow - up.3941 a preliminary report37 of a dose - fractionation escalation study in 210 men ( 294 gy in 22 fractions to 43 gy in 12 fractions ) reported rectal bleeding in 88% of patients . 
in a large phase 2 study including 770 men treated with 25 gy fractions to a total of 70 gy in 55 weeks , 42 rates of late grade 2 or worse rectal and bladder toxicity were 45% and 52% . preliminary estimates of psa control rates in these studies3842 are comparable to those in standard fractionation schedules . 
a large single - institute series of 705 men in manchester , uk , is valuable , because it suggests that a schedule of 50 gy in 16 fractions ( 3125 gy per fraction ) was equivalent to a contem poraneously treated series with 6570 gy in 1820 gy fractions.43 previously reported randomised controlled trials of hypofractionation have used only modest radiation doses by present standards . 
results show a 7% reduction in psa control rate ( 5295% vs 5995% ) in the 20 fraction group with hr for failure of 118 ( 95% ci 099141 )  . 
after median follow - up of 44 months , 4 year psa control rates were alike ( 862% for hypofractionation vs 854% for standard fractionation ) ; rectal bleeding was more frequent in the hypofractionated group ( appendix )  . 
all these studies are compatible with an ratio for prostate cancer of 1530 gy.44 other phase 3 randomised controlled trials are underway : in canada , investigators are comparing 60 gy in 20 fractions with 78 gy in 39 fractions in a planned cohort of 1204 patients ( isrctn 43853433 ) ; and in the netherlands , researchers are comparing 646 gy in 19 fractions with 78 gy in 39 fractions , with a planned cohort of 800 patients ( isrctn 85138529 )  . 
after a pilot study , a scandinavian collaborative group is comparing increased hypofractionation with 427 gy in seven fractions given in 1519 days with 78 gy in 39 fractions in 78 weeks in a group of 592 men ( isrctn 45905321 )  . 
 the combination of studies should clearly de ne the clinical role of hypofractionation for prostate cancer and the fractionation sensitivity of both prostate cancer and normal tissues with improved precision . analyses in our study were not powered for formal comparisons and 84% of patients were from two sites , although the trial occurred in 11 centres overall . 
stage 3 of this trial aims to show non - inferiority of biochemical psa control between experimental and control groups and includes an additional 2759 patients recruited from 41 centres , and will provide an opportunity to validate the ndings presented here . 
planned associated translational research includes comparative dose - volume histograms and side - e ect analysis for the hypofractionated groups , collection of germline dna for radiogenomics , 45 and tissue microarray assessment of predictive factors for fraction sensitivity . contributors dd was the chief investigator and was involved with study design , recruitment of patients , data interpretation , and writing of the report . 
 ah , vk , rh , db , ag , pk , mr , js , hp , csc , and cp contributed to trial design , patient recruitment , data collection , follow - up , and reviewed the report . 
eh was responsible for central management of the trial at icr - ctsu and for all statistical analyses , is a member of the trial steering committee , and was involved in data interpretation and writing of the report . con icts of interest we declare that we have no con icts of interest . acknowledgments stage 1 of this study was supported by the academic radiotherapy units cancer research uk programme grant ( sp2312 / 021 ) , and stage 2 was additionally supported by the department of health . 
central trial management costs during follow - up and statistical analyses were supported by cancer research uk ( grant number c8262 / a7253 , trial reference number cruk / 06 / 016 ) , with quality assurance from the department of health . 
 recognition goes to all the trials unit sta at bob champion unit and at icr - ctsu , sutton , uk , who contributed to the central coordination of the trial . 
we would also like to thank the trial management group , independent data monitoring and trial steering committees ( appendix ) for overseeing the trial . editorial published online november 16 , 2012 s1470 - 2045 ( 12 ) 70526 - 0 for more on the patient protection and a ordable care act see world report lancet 2012 ; 380 : 172728 obama : health - care reform , part two the re - election of us president barack obama has surely eliminated the last serious threat to health - care reform in the usa . 
the patient protection and a ordable care act has already survived systematic opposition from republicans , a supreme court challenge , and nally , mitt romneys vow to repeal it if elected . 
the us healthcare system still faces many challenges and it may take more than insurance reform to address the the act can be seen as a health insurance reform packageover the next 2 years , medical insurance will almost certainly be extended to as many as 30 million americans who presently lack coverage . 
for most patients with cancerwho for decades have been discriminated against , denied coverage , and charged more that they could possibly a ord for life - saving treatmentsthe act has been an important step . 
it prohibits some of the health insurance industrys most notorious practiceseg , denying coverage to people who have pre - existing conditions or who participate in clinical trials , increasing premiums because of age or poor health , and insurance caps that restrict the amount that a patient can clai it also o ers free screening and preventive health care . although several measures have already been implemented , such as a requirement that insurance plans allow parents to cover their children aged up to 26 years in their policies , most aspects of the law are yet to be introduced . 
the biggest obstacles facing successful implementation of the act are the reliance on individual states to expand medicaid ( which guarantees health bene ts for the poorest americans ) , the budget cuts that the republicans will likely demand during upcoming negotiations , and the successful roll out by 2014 of insurance marketsso - called exchangesat the heart of the law , which enable people to buy individual coverage . 
that almost 50 million people have no health coverage in one of the richest countries in the world is a scandal that needs to be addressed , but the system is awed . 
the usa spends 16% of gdp on health versus 8% of gdp in europe , yet outcomes such as overall and cancer - speci c mortality are comparable between the two continents . 
the system will bankrupt itself unless major changes to funding and organisation are introducedtweaking medicares funding structure will not be su cient ; the entire health - care system needs an overhaul . 
the prevailing approach to paying for health care , based mainly on invidual services and products , encourages wasteful and ine ective care , creates incentives to overtest and overtreat while ignoring outcomes . 
he undoubtedly faces many di culties : the countrys trillion dollar de cit , the scal cli , and especially , the lack of a legislative majoritygiven that the democrats only control the senatewhich could lead to legislation bouncing from one chamber of congress to the other and nothing being done . 
but clinicians and societies also need to become more involved and lead such changes , otherwise others ( eg , politicians or insurers ) will make decisions that might later be judged inappropriate or unfair . 
 as obama cannot target another term in o ce , an opportunity exists to keep health high on the agenda and to o er americans the best medicine at the best cost . 
in the rst term of his presidency , obama set out important and necessary health insurance refor in his second term , he now needs to lead reform to make the health system fair , e cient , and sustainableif he can achieve this , he will leave an enduring legacy to be proud of . 
 the lancet oncology vol 13 december 2012 1171 articles sensitivity of transvaginal ultrasound screening for endometrial cancer in postmenopausal women : a case - control study within the ukctocs cohort ian jacobs , aleksandra gentry - maharaj , matthew burnell , ranjit manchanda , naveena singh , aarti sharma , andy ryan , mourad w seif , nazar n amso , gillian turner , carol brunell , gwendolen fletcher , rani rangar , kathy ford , keith godfrey , alberto lopes , david oram , jonathan herod , karin williamson , ian scott , howard jenkins , tim mould , robert woolas , john murdoch , stephen dobbs , simon leeson , derek cruickshank , steven j skates , lesley fallow eld , mahesh parmar , stuart campbell , usha menon summary background the increase in the worldwide incidence of endometrial cancer relates to rising obesity , falling fertility , and the ageing of the population . 
we report the performance of tvs screening in a large cohort . methods we did a nested case - control study of postmenopausal women who underwent tvs in the united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) following recruitment between april 17 , 2001 , and sept 29 , 2005 . 
 our study is registered with clinicaltrials.gov , number nct00058032 , and with the international standard randomised controlled trial register , number isrctn22488978 . findings 48 230 women underwent tvs in the ukctocs prevalence screen . 
9078 women were ineligible because they had undergone a hysterectomy and 2271 because their endometrial thickness had not been recorded ; however , 157 of these women had an endometrial abnormality on tvs and were included in the analysis . 
the optimum endometrial thickness cuto for endometrial cancer or aeh was 515 mm , with sensitivity of 805% ( 95% ci 727868 ) and speci city of 862% ( 858866 )  . 
sensitivity and speci city at a 5 mm or greater cuto were 805% ( 727868 ) and 857% ( 854862 ) ; for women with a 5 mm or greater cuto plus endometrial abnormalities , the sensitivity and speci city were 853% ( 782908 ) and 804% ( 800808 ) , respectively . 
when our analysis was restricted to the 96 women with endometrial cancer or aeh who reported no symptoms of postmenopausal bleeding at the ukctocs scan before diagnosis and had an endometrial thickness measurement available , a cuto of 5 mm achieved a sensitivity of 771% ( 678843 ) and speci city of 858% ( 857859 )  . 
the logistic regression model identi ed 25% of the population as at high risk and 395% of endometrial cancer or aeh cases were identi ed within this high risk group . 
in this high - risk population , a cuto at 675 mm achieved sensitivity of 843% ( 714930 ) and speci city of 899% ( 893905 )  . interpretation our ndings show that tvs screening for endometrial cancer has good sensitivity in postmenopausal women . 
 additional factors are mortality greater than 30% within 10 years of diagnosis10 and a proven link between stage and survival raising the possibility of a mortality bene t from earlier detection.10 of note , stage for stage , survival rates for endometrial cancer are similar to ovarian cancera cancer for which large - scale screening trials are underway.11 , 12 to assess the endometrium in symptomatic women are tvs and endometrial sampling . 
other studies1416 have included smaller populations , making the to assess sensitivity of screening , or to achieve con dent estimates of speci city or positive predictive value . techniques commonly used impossible the the opportunity to study the performance of tvs in a large cohort of postmenopausal women was provided by data from the united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) .12 , 17 ukctocs is a prospective trial of ovarian cancer screening , one arm of which involved pelvic ultrasound during which endometrial thickness was measured and recorded . 
we report on the characteristics of endometrial cancer screening in postmenopausal women in the general population to inform on the potential of screening for endometrial cancer . methods participants we did a nested case - control study within the ukctocs cohort with ultrasound ndings recorded at yearly screening appointments as part of the ovarian cancer screening trial . 
the pre - identi ed scottish centres dropped out because of logistical issues ( lack of space , retirement of potential research leads , unwillingness of nhs trust management to commit to a 10 - year trial , involvement in other ovarian cancer screening trials ) .17 participants completed a recruitment questionnaire , which requested baseline data on lifestyle and reproductive factors , previous cancer history , and family history of breast or ovarian cancer.17 the focus of the recruitment questionnaire was on risk factors for ovarian cancer and the trial was not resourced to collect all variables related to endometrial cancer risk at the initial visit . 
 50 639 participants were randomly assigned to yearly screening with tvs ; 48 230 attended the initial prevalence screen and are included in our study . all women assigned to screening with tvs who had undergone the prevalence screen were included as cases or controls . 
cases were women with a con rmed diagnosis of endometrial cancer or atypical endometrial hyperplasia ( aeh ) , complex endometrial hyperplasia ( ceh ) , endometrial stromal sarcoma ( ess ) , or carcino sarcoma . 
we excluded from our study all women assigned to screening with tvs who had undergone hysterectomy before random assignment in ukctocs or who had no endometrial thickness measurement or endometrial abnormality on the relevant scan . 
 our study was covered by the ethical approval obtained for the main ukctocs ( mrec reference 00 / 8 / 34 , granted by north west mrec )  . recorded procedures tvs with kretz / medison sa9900 ( medison , seoul , south korea ) ultrasound machines was done by experienced ultrasonographers at the 13 trial centres in the uk . 
during the course of the trial , they completed an accreditation programme and attended yearly ultrasound days . the ultrasonographers were instructed to ask about and record symptoms of postmenopausal bleeding . 
we do not know how accurately postmenopausal bleeding was documented and there might have been a bias to better documentation in women who had an endometrial thickness above the level which prompted clinical referral ( > 5 mm ) according to current guidelines . 
in all women who reported that they had experienced any irregular bleeding to the sonographer , data were recorded on the ultrasound for during scanning , details of ovarian morphology and size were recorded . 
representative grey - scale images of each ovary and the uterus were archived at the coordinating centre.12 vol 12 january 2011 articles at tvs , endometrial thickness was measured at its thickest point from the anterior to the posterior in the sagittal plane of the uterus . 
callipers were placed perpendicular to the outer edge of the endometriuif there was uid in the endometrial cavity , the endometrial thickness was measured as above but with the inclusion of the cavity uid and the double endometrial stripe , then the uid diameter was subtracted at the same point . 
 for the purposes of our study , thickened , irregular , cystic , heterogeneous , distended endometrium ; uid in the endometrial cavity ; or polyp or other mass or lesion were included under the de nition of endometrial abnormality . abnormal , in clinical practice , asymptomatic women are not investigated . 
in the absence of any de nitive data at the start of the trial , a pragmatic decision to recommend referral of asymptomatic women with an endometrial thickness greater than 10 mm was agreed on the basis of extensive discussion and consultation with clinicians . 
we emphasise that there was no systematic protocol - driven intervention based on endometrial thickness . trial guidelines for the management of endometrial thickness stated that all women with thickness greater than 5 mm should be questioned about bleeding . 
in the this , uk national health service , postmenopausal bleeding prompts a 2 - week referral to assess for cancer , and all centres would have irrespective of followed measurements of endometrial thickness . 
data on any di erences between the centres are not yet available . all participants were followed up through a agging study with the nhs information centre for health and social care ( formerly o ce of national statistics ) in england and wales and via the central services agency and cancer registry in northern ireland as appropriate . 
 * includes those with personal history of breast cancer . table 1 : baseline characteristics of ukctocs participants who underwent the rst yearly scan vol 12 january 2011 articles women without ec or aeh n = 36 731 women with ec or aeh n = 133 relative risk ( 95% ci ) < 5 mm 30 664 ( 835% ) 5 to 10 mm 10 to 20 mm 20 mm mean ( sd ) 4878 ( 133% ) 1116 ( 30% ) 73 ( 02% ) 26 ( 195% ) 33 ( 248% ) 59 ( 444% ) 15 ( 113% ) median ( iqr ) 29 mm ( 2040 ) 110 mm ( 60145 ) 346 mm ( 259 ) 1153 mm ( 781 ) 793 ( 4771318 ) 5927 ( 37679336 ) 2012 ( 1106436063 ) data are n ( % ) unless otherwise indicated . 
aeh = atypical endometrial hyperplasia . table 2 : distribution of endometrial thickness measurements in women with or without endometrial cancer or atypical endometrial hyperplasia optimum = 515 mm optimum = 580 mm 1specicity 1specicity figure 1 : receiver operator curves for detection of endometrial cancer and atypical endometrial hyperplasia endometrial thickness measurements alone ( a ) and a combination of endometrial thickness measurements and endometrial abnormality ( b )  . 
data on the relevant variables for the ultrasound group were then inserted into the derived high - risk model and a prior risk probability of endometrial cancer was calculated solely on the basis of epidemiological data . 
these groups were based on the cuto s of the ordered prior risk probabilities : the highest risk ( rst ) quartile , the second quartile , the third quartile , and those at lowest risk ( fourth quartile )  . 
 relative risks ( rrs ) were used because the prevalence of endometrial cancer was virtually unchanged from the prevalence of endometrial cancer in the trial population for those without hysterectomy . ovarian volume was assessed as another variable to identify women at higher risk of endometrial cancer or aeh by comparing measurements of those who developed endometrial cancer or aeh and those who had not . the relative risk of endometrial cancer or aeh in women with thickness measurements of 5 mm or greater or 10 mm or greater were calculated to show the endometrial thickness cuto s suggested by the ukctocs guidelines . 
our study is registered with clinicaltrials.gov , number nct00058032 , and with the international standard randomised controlled trial register , number isrctn22488978 . follow - up , copies of operative notes , histopathology reports , cytology reports , discharge summaries , multidisciplinary team meeting notes , and other correspondence were obtained . 
the nal diagnosiswhich included the primary site , stage , and grade of any cancerwas made on review of the medical notes by an independent gynaecological oncologist ( rm )  . our primary outcome measure was endometrial cancer and aeh . 
aeh was included because 40% of cases of aeh might have concurrent ec , 18 there is limited concordance between pathologists on the diagnosis of aeh or endometrial cancer , 19 and aeh is a precancerous state with greater than 25% of patients progressing to endometrial cancer ( estimates range from 25% to 82% ) .2025 ess , carcinosarcoma , and ceh were also analysed separately . statistical analysis the distribution of endometrial thickness was compared in women who did and did not develop endometrial cancer or aeh . 
these data were used to construct a receiver operator characteristic ( roc ) curve to assess the speci city and sensitivity of various thickness cuto s for detecting endometrial cancer or aeh . 
a multivariate logistic - regression analysis was done that combined thickness with the baseline characteristics of the study participants to develop an algorithm incorporating epidemiological variables that would identify a high - risk group who might bene t from a targeted approach to screening . 
further roc curves were constructed to assess the speci city and sensitivity of various endometrial thickness cuto s for detecting endometrial cancer or aeh in the di erent risk groups . further analyses assessed the sensitivity and speci city pro le of endometrial thickness for the detection of endometrial cancers , either alone or combined with ceh , ess , or carcinosarcoma , with a scan done within a year of diagnosis . 
since systematic protocol - driven intervention based on endometrial thickness , we did not analyse the data by stage of endometrial cancer . to explore the possibility of re ning screening in a higher - risk group , the baseline characteristics recorded at recruitment for women diagnosed with endometrial cancer in the control and multimodal groups of the trial were modelled as epidemiological risk factors for endometrial cancer with forward stepwise logistic regression . 
these factors were weight ; age at menarche ; use of the oral contraceptive pill ; personal history of breast , ovarian , lung , bowel , or other cancer ; age at scan ; and any pregnancy of longer than 6 months vol 12 january 2011 articles role of the funding source the sponsor of the study and the funding sources had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
ag - m , mb , rm , ar , and um also had access to the raw data . results table 1 shows the baseline characteristics of the women with and without endometrial cancer or aeh . 
the inclusion criteria and details of the ukctocs trial have been described in detail elsewhere.12 , 17 50 639 study participants were randomly assigned to the ultrasound arm of ukctocs . 
the resulting group of 37 038 women were included in our study ( web appendix pp 56 )  . absence of endometrial median follow - up from the scan to cancer registration ( iqr 405595 )  . 
since update was 511 years information on cancers can take up to 3 years to be recorded on the national cancer registries , we explored other sources of follow - up data in detail in the 985 women for whom the time from scan to cancer registry followup on feb 9 , 2009 , was less than 3 years . 
in this cohort , we had additional con rmation of endometrial cancer status in 849 women because they had attended further screening and in 66 of the remaining women through returned follow - up questionnaires . 
in 70 of 37 038 women , the only source of information on endometrial cancer status was cancer registry follow - up of less than 3 years from the date of scan . [ 2% ] , three mixed subtype the cohort of 37 038 women includes 125 women who developed endometrial cancer after random assignment ( 100 endometrioid [ 80% ] , six papillary serous [ 5% ] , two clear cell [ 2% ] , one mucoid [ 1% ] , and 13 endometrial carcinoma without speci cation of histological subtype [ 10% ] ) , six with ess , six with carcinosarcomas or mixed mllerian tumours , 11 with aeh , and two with ceh . 
ess = endometrial stromal sarcoma . table 3 : performance characteristics of endometrial thickness as a screening tool for endometrial cancer with and without endometrial abnormality vol 12 january 2011 articles developed endometrial cancer after random assignment were stage 1 , 11 were stage 2 , nine were stage 3 , and one was stage 4 . 
overall , 112 of the 136 women with endometrial cancer or aeh were asymptomatic and 24 were symptomatic at the last ukctocs scan before diagnosis ( of 99 women with endometrial cancer or aeh who reported no postmenopausal bleeding , 96 had endometrial thickness measurements available )  . the remainder of the cohort is 36 888 controls , who are women without a diagnosis of endometrial cancer or aeh within 1 year of their last ukctocs scan . 
the control group includes six women who had either a leiomyosarcoma or breast cancer that was metastatic to the endometrium and 23 women who had endometrial cancer or aeh diagnosed more than 1 year after the last ukctocs scan . 
the 5% missing data rate is in keeping with what was anticipated for a study of this type and size . weight , age , and personal history of cancer were associated with an increased risk of endometrial cancer or aeh , although oral contraceptive pill , age at menarche , and parity were associated with a decreased risk ( webappendix p 1 )  . table 2 shows the distribution of endometrial thickness measurements in the 36 731 women who did not have a diagnosis of endometrial cancer or aeh . 
most of the women had an endometrial thickness of less than 5 m in the 133 women with a diagnosis of endometrial cancer or aeh who had endometrial thickness recorded , 107 ( 81% ) had an endometrial thickness of 5 mm or greater . 
the optimum cuto for endometrial thickness was 515 mm with a rr of 252 ( 95% ci 165385 )  . the webappendix ( p 2 ) shows the distribution of endometrial thickness measurements according to the use of hormone replacement therapy ( hrt ) in the overall cohort . 
the median endometrial thickness in women in the whole cohort who did not use hrt was 27 mm ( iqr 20395 ) versus 36 mm ( 2551 ) in women that did and these results were similar in the subgroup of women without endometrial cancer or aeh ( p < 00001 )  . 
by contrast , the median thickness was 110 mm ( 59148 without hrt ; 70145 with hrt ) in women with endometrial cancer or aeh , irrespective of the use of hrt . 1406 women reported breast cancer diagnosis before entry into the trial . 
these women were more likely to have an endometrial thickness of 5 mm or greater to less than 10 mm ( rr 191 ; 95% ci 168218 ) , 10 mm or greater to less than 20 mm ( 450 ; 385525 ) , and 20 mm or greater ( 1101 ; 8041447 ) than women with no history of breast cancer ( webappendix , p 3 )  . 
of the women with no history of breast cancer , 29 757 ( 839% ) of 35 460 had an endometrial thickness of less than 5 mm compared with 940 ( 669% ) of 1406 women with history of breast cancerthe median endometrial thickness was 29 mm versus 36 mm ( p < 00001 ; webappendix p 3 )  . 
 a large proportion of this measurement in women with breast cancer was probably related to tamoxifen use , but treatment data were not systematically captured as part of the trial . we did an analysis of endometrial thickness by screening centre in the women who did not develop endometrial cancer . 
the median endometrial thickness was 29 mthe median thickness varied from 21 mm number % ( 95% ci ) number % ( 95% ci ) number % ( 95% ci ) positive for bleeding negative for bleeding 5 mm cuto > 5 mm 5 mm sensitivity speci city > 10 mm 10 mm sensitivity speci city positive predictive value negative predictive value 10 mm cuto positive predictive value negative predictive value overall 31 464 35 746 805% ( 727868 ) 857% ( 854862 ) 20% ( 1821 ) 999% ( 999999 ) 541% ( 453628 ) 972% ( 970974 ) 64% ( 5474 ) 998% ( 998999 ) 892% ( 769956 ) 422% ( 386440 ) 308% ( 266331 ) 931% ( 852972 ) 649% ( 510767 ) 773% ( 734808 ) 453% ( 357535 ) 884% ( 838923 ) 31 410 35 586 771% ( 678843 ) 858% ( 857859 ) 14% ( 1215 ) 999% ( 999100 ) 500% ( 403597 ) 972% ( 971973 ) 45% ( 3654 ) 999% ( 998999 ) table 4 : performance characteristics of endometrial thickness as a screening tool for endometrial cancer in women with and without postmenopausal bleeding vol 12 january 2011 articles optimum = 675 mm optimum = 485 mm optimum = 575 mm optimum = 465 mm 1specicity 1specicity figure 2 : receiver operator curve for endometrial thickness measurements for detection of endometrial cancer in the high - risk group first quartile ( a ) , second quartile ( b ) , third quartile ( c ) , and fourth quartile ( d )  . 
when dichotomised as endometrial thickness less than 5 mm and 5 mm or greater , the proportion of measurements greater than 5 mm per centre varied from 104% to 224% ( overall proportion 168% ; median centre proportion 166% , iqr 147198 )  . to assess the sensitivity and speci city pro le for detection of endometrial cancer or aeh , a roc curve was constructed with cuto points for endometrial thickness with or without data for endometrial abnormalities ( gure 1 , webappendix p 4 )  . 
our subgroup analyses that included endometrial cancer and aeh or a combination of endometrial cancer , aeh , ceh , and ess or carcinosarcoma showed similar levels of sensitivity and speci city . given the di erence noted in endometrial thickness distribution in users of hrt and non - users , the optimum cuto in hrt users was as expected higher ( 685 mm ) than non - users ( 455 mm ; table 3 )  . at the ukctocs scan , postmenopausal bleeding was recorded in 165 women ( 37 cases and 128 controls )  . 
table 4 shows the performance characteristics for women with and without postmenopausal bleeding . the relation between ovarian volume and endometrial cancer or aeh was assessed and no statistically signi cant correlation was identi ed ( p = 0956 ; data not shown )  . we explored the possibility of optimising approaches to endometrial cancer screening by incorporating epidemiological information provided in the recruitment questionnaire . 
logistic regression showed that decreased endometrial cancer or aeh risk was associated with the use of the oral contraceptive pill , age at menarche , and pregnancies longer than 6 months , while increased risk was associated with rising weight , increasing age , and personal history of breast and other cancer ( multivariate and univariate analyses are shown in webappendix p 1 )  . 
 on the basis of the logistic regression model , the population could be divided into quartiles with rrs for endometrial cancer compared with the entire population of 198 ( 139280 ) for the rst quartile , 107 ( 073158 ) for the second , 076 ( 049116 ) for the third , and 049 ( 030079 ) for the fourth ( table 5 )  . 
the population in the highest quartile of risk ( rst quartile ) included 395% of women with endometrial cancer or aeh ; in this population an optimum endometrial thickness cuto at 675 mm achieved a sensitivity of 843% and speci city of 899% ( gure 2 , table 5 )  . if endometrial we also assessed the number of further interventions that would be predicted thickness measurements were used as a screen for endometrial cancer or aeh ( table 6 )  . 
if the entire population were screened , an endometrial thickness cuto of 5 mm or greater would result in 58 women undergoing further investigation per case of endometrial cancer or aeh detected for the diagnosis of 805% ( 107 of 133 ) of cancers . 
 a cuto of 10 mm or greater , would lead to 17 women being investigated to detect each case of endometrial cancer ( 556% [ 74 of 133 cancers diagnosed ] )  . 
if the proportion of the population screened was reduced by the use of our logistic regression model to limit screening to the top quartile risk group , 22 women would have to undergo investigation per endometrial cancer detected for the detection of 43 ( 323% ) cases in the entire population . vol 12 january 2011 articles number of cases / controls proportion of cases included rr of ec ( 95% ci ) area under curve ( 95% ci ) > 5 mm et cuto > 10 mm et cuto optimum cuto first quartile second quartile third quartile fourth quartile 51 / 9015 395% 34 / 9081 264% 26 / 9104 202% 18 / 9115 140% 198 ( 139 280 ) 107 ( 073 158 ) 076 ( 049 116 ) 049 ( 030 079 ) 0902 ( 0848 0957 ) 0878 ( 0808 0948 ) 0744 ( 0623 0865 ) 0969 ( 0947 0991 ) sensitivity ( 95% ci ) speci city ( 95% ci ) sensitivity ( 95% ci ) speci city ( 95% ci ) cuto sensitivity ( 95% ci ) speci city ( 95% ci ) 0863 ( 0737 0943 ) 0794 ( 0621 0913 ) 0615 ( 0406 0798 ) 0944 ( 0727 0999 ) 7546 0837 ( 0829 0845 ) 7846 0864 ( 0857 0871 ) 7839 0861 ( 0854 0868 ) 7948 0872 ( 0865 0879 ) 0627 ( 0481 0759 ) 0471 ( 0298 0649 ) 0385 ( 0202 0594 ) 0667 ( 0410 0867 ) 8654 8863 8867 8914 0960 ( 0956 0964 ) 0976 ( 0973 0979 ) 0974 ( 0970 0977 ) 0978 ( 0975 0981 ) 485 mm 28 7574 675 mm 43 465 mm 17 575 mm 17 0843 ( 0714 0930 ) 0824 ( 0655 0932 ) 0654 ( 0443 0828 ) 0944 ( 0727 0999 ) 8104 0899 ( 0893 0905 ) 0834 ( 0826 0842 ) 7456 0819 ( 0811 0827 ) 8194 0899 ( 0893 0905 ) n = number . 
when we assessed this in our cohort , we found that for the left ovary , the use of the suggested cuto of 3 cm , the p value was 0063 and for the right ovary p was 0218 . discussion ultrasound imaging of the endometrium has long been thought a possible screening test for endometrial cancer . 
however , there has been a dearth of data about the performance of potential tests and the largest study involved fewer than 2000 women and only one endometrial cancer was diagnosed.13 the ukctocs protocol enabled us to assess the performance of tvs for endometrial screening cancer 37 038 postmenopausal women . 
 when the analysis was restricted to women who reported no symptoms of postmenopausal bleeding at the scan and had an endometrial thickness measurement available , a cuto of 5 mm achieved a sensitivity of 771% and speci city of 858% ( table 4 )  . 
although the role of population screening for endometrial cancer remains uncertain , the ndings are of immediate value in the management of increased endometrial thickness in postmenopausal women undergoing pelvic scans for reasons other than vaginal bleeding . our ndings con rm the strong correlation between tvs ndings and subsequent diagnosis of endometrial cancer , as shown by the rrs ( table 2 )  . 
 this correlation was shown by the levels of sensitivity et cut - o ( mm ) number of cases of ea / aeh with positive result proportion of ec cases detected number of women with positive result risk of ec / aeh relative risk of ec / aeh ( 95% ci ) number of investigations per case detected whole population screened whole population screened whole population screened whole population screened first quartile ( highest risk ) screened second quartile screened third quartile screened fourth quartile ( lowest risk ) screened > 675 > 485 > 465 > 575 10000% 8045% 5564% 1128% 3233% 2105% 1278% 1278% 36 864 6174 1263 1535 1665 036% 173% 586% 1705% 451% 182% 102% 181% 100 2047 ( 13393130 ) 3537 ( 25844950 ) 5315 ( 32118500 ) 4373 ( 20999032 ) * 2263 ( 9645319 ) * 838 ( 3821840 ) * 14588 ( 248186025 ) * * relative risk within the risk quartile . 
as expected , the optimum cuto in asymptomatic women of 445 mm is similar but lower than the 5 mm cuto reported for symptomatic women.26 of note , our report shows that 26 women ( 195% ) who developed endometrial cancer within a year of their scan on ukctocs had an endometrial thickness of less than 5 min a theoretical model , based on the estimate that 15% of endometrial cancers occur in women without vaginal bleeding , smith - bindman and colleagues27 calculated the risk of endometrial cancer to be 67% for an endometrial thickness greater than 11 mm.27 this ts satisfactorily with 59% risk of endometrial cancer in our cohort where 96 ( 722% ) of 133 women were asymptomatic at an endometrial cuto of 10 mm . although the data show that tvs can detect endometrial cancer before symptoms are detected in a high proportion of postmenopausal women , there are a range of issues that need to be addressed before population screening for endometrial cancer can be proposed . 
if we assume an incidence of 60 per 100 000 per year and 30% mortality at 5 - year follow - up , a randomised controlled trial would need 500 000 participants to document a 50% reduction in mortality . 
since a trial on this scale is almost certainly not feasible , decisions about whether or not to screen for endometrial cancer will have to be made on the basis of surrogate measures of e cacy . 
we explored the possibility of reducing the overall burden of screening by focusing on a group of the population identi ed as being at higher risk on the basis of epidemiological criteria . 
our logistic regression model that used epidemiological variables of the use of the oral contraceptive pill , age at menarche , number of pregnancies , weight , age , and history of cancer was able to separate the population into quartile groups at di erent levels of risk . 
 this would reduce the burden of screening to 25% of the population with detection of about 40% of the cases . the strengths of our study include the large size of our cohort , prospective data collection with standardised measurement of endometrial thickness as part of the trial protocol , systematic follow - up , and information on epidemiological variables . 
consistent with earlier reports of the correlation of endometrial thickness and hrt , 28 the median endometrial thickness in users of hrt in the control group was 36 mm versus 27 mm in non - users . 
this probably relates to the use of tamoxifen , which is known to be associated both with increased endometrial thickness ( range 49117 mm ) in postmenopausal women2934 and increased risk of endometrial cancer ( rates of 03% vs 006% in women on placebo ) .35 we were , however , unable to con rm a recently reported correlation between ovarian volume and the risk of endometrial cancer of aeh reported by the plco trialists.36 one of the limitations of our study was that endometrial cancer screening was not an interventional endpoint in the ukctocs . 
detailed data on the variety of procedures done was not collected , but this is unlikely to alter the performance characteristics of endometrial thickness . a further limitation of our study is the accuracy of the reports of postmenopausal bleeding . 
therefore , there might be bias in the recording of these data for women who had an endometrial thickness above the level that triggered clinical referral ( > 5 mm )  . there was a di erence in median endometrial thickness measurements in healthy women across the 13 centres . 
in addition to slight variations for measuring endometrial thickness in 36 731 individuals across 13 centres , it is also probably related to variations in the demographics such as body - mass index of patients between centres . 
it highlights the need to have training and quality assurance measures in place if ultrasound were to be used as a screen for endometrial cancer . the scanning techniques the cis around parameter estimates were wide because of low numbers of endometrial cancers despite the large overall number of participants . 
some key variables that could a ect risk of endometrial cancer , such as smoking , 38 diabetes , and hypertension , 39 could not be used in model building because the main focus of the recruitment questionnaire was on risk factors for ovarian cancer . 
variables were collected on follow - up and a greater percentage of women with endometrial cancer reported a history or diagnosis of diabetes ( nine [ 102% ] of 88 ) compared with those without endometrial vol 12 january 2011 articles panel : research in context systematic review a systematic review of ovarian cancer screening41 was published by the nhs centre for reviews and dissemination before submission of the grant proposal to the uk medical research council for united kingdom collaborative trial of ovarian cancer screening . 
no systematic review of endometrial cancer screening was done . a detailed review of published work of endometrial cancer screening in an asymptomatic population was done as part of our analysis . 
other studies1416 have included smaller populations making it impossible to assess the sensitivity of screening or to achieve con dent estimates of speci city or positive predictive value . interpretation our study provides to our knowledge the only large - scale data on the performance characteristics of tvs in endometrial cancer screening , and provides evidence that ultrasonography can detect endometrial cancer in asymptomatic women with 8090% sensitivity and similar levels of speci city . 
 clinicians faced with ultrasound data on endometrial thickness from scans done in various disorders aside from vaginal bleeding will now have data to inform their daily practice . the likely bene t of detection of endometrial cancer by ultrasound screening would be conjecture . 
we have limited ourselves to reporting and discussing the performance characteristics . the rising incidence of endometrial cancer and the di culty of doing a randomised controlled trial large enough to specify mortality as an endpoint , suggests that the decision to introduce screening for all or a subgroup of asymptomatic women will rest on surrogate criteria such as the performance characteristics described in our report and future studies of acceptability , health economics , and risk strati cation . 
we do not advocate population screening for endometrial cancer until further data are available from these studies . contributors ijj , agm , mb , sc , and um contributed to the study design , analysis and interpretation of the data , and drafting and revision of the report . 
um and ij has a nancial interest through ucl business and abcodia ltd in the third party exploitation of clinical trials biobanks , which have been developed through the research at ucl . 
all other authors declared no con icts of interest . acknowledgments the trial was core funded by the uk medical research council , cancer research uk , and the uk department of health with additional support from the eve appeal , special trustees of barts and the london , and special trustees of uclh . 
a substantial portion of this work was done at uclh / ucl within the womens health theme of the nihr cancer ( 1429 [ 50% ] of 28 801 ; data not shown )  . 
furthermore , although there was an association with weight , we could not con rm the link between the risk of endometrial cancer and body - mass index.40 a paucity of detailed information on type of hrt and duration of use at scan also reduced our ability to do further subanalyses . false - positive results on tvs screening for endometrial cancer will require a form of endometrial sampling that , although not a major procedure , will generate anxiety , inconvenience , and cost . 
there are of course complications as well as costs of hysteroscopy that would need to be assessed carefully in a risk - bene t analysis if screening for endometrial cancer with tvs was to be introduced . 
another important consideration for future studies of endometrial cancer screening is acceptability of the screening strategy . a cuto at 5 mm or greater would result in 58 diagnostic procedures for each case of endometrial cancer detected . 
we are exploring the possibility of further re ning risk strati cation by incorporating sex - steroid hormone pro ling . laparoscopy or whether ovarian cancer screening will save lives is currently unclear and whether the primary screen should be with tvs or a serum biomarker is debated . 
the extra cost of incorporating endometrial cancer screening within the scope of an ovarian cancer screening trial could be marginal and add bene t to the screening strategy if properly modelled . our report is to our knowledge the rst large - scale report of the performance characteristics of tvs in endometrial cancer screening ( panel )  . 
in particular , issues of early detection , morbidity , acceptability , and health economics of intervening on the basis of endometrial thickness will need to be the subject of future studies . 
we thank the women throughout the uk who are participating in the trial and to the entire medical , nursing , and administrative sta who work on the ukctocs . 21 kurman rj , kaminski pf , norris hj . 
afatinib versus placebo for patients with advanced , metastatic non - small - cell lung cancer after failure of erlotinib , ge tinib , or both , and one or two lines of chemotherapy ( lux - lung 1 ) : a phase 2b / 3 randomised trial . 
lancet oncol 2012 ; 13 : 52838in this article ( published online march 26 ) , the rst sentence of the fourth paragraph on the fourth page should have read we measured progression - free survival from the date of randomisation to disease progression or death , whichever occurred rst . 
stampedean international , open - label , randomised controlled trialuses a novel multiarm , multistage design to assess whether the early additional use of one or two drugs ( docetaxel , zoledronic acid , celecoxib , zoledronic acid and docetaxel , or zoledronic acid and celecoxib ) improves survival in men starting rst - line , long - term hormone therapy . 
here , we report the preplanned , second intermediate analysis comparing hormone therapy plus celecoxib ( arm d ) with hormone therapy alone ( control arm a )  . methods eligible patients were men with newly diagnosed or rapidly relapsing prostate cancer who were starting long - term hormone therapy for the rst time . 
patients randomly allocated to arm d received celecoxib 400 mg twice daily , given orally , until 1 year or disease progression ( including prostate - speci c antigen [ psa ] failure )  . 
accrual of further patients was discontinued in any research arm showing safety concerns or insu cient evidence of activity ( lack of bene t ) compared with the control arthe minimum targeted activity at the second intermediate activity stage was a hazard ratio ( hr ) of 092 . 
this trial is registered with clinicaltrials.gov , number nct00268476 , and with current controlled trials , number isrctn78818544 . findings 2043 patients were enrolled in the trial from oct 17 , 2005 , to jan 31 , 2011 , of whom 584 were randomly allocated to receive hormone therapy alone ( control group ; arm a ) and 291 to receive hormone therapy plus celecoxib ( arm d )  . 
at the preplanned analysis of the second intermediate activity stage , with 305 ffs events ( 209 in arm a , 96 in arm d ) , there was no evidence of an advantage for hormone therapy plus celecoxib over hormone therapy alone : hr 094 ( 95% ci 074120 )  . 
there was no evidence of di erences in the incidence of adverse events between groups ( events of grade 3 or higher were noted at any time in 123 [ 23% , 95% ci 2027 ] patients in arm a and 64 [ 25% , 1930 ] in arm d )  . 
the most common grade 35 events adverse e ects in both groups were endocrine disorders ( 55 [ 11% ] of patients in arm a vs 19 [ 7% ] in arm d ) and musculoskeletal disorders ( 30 [ 6% ] of patients in arm a vs 15 [ 6% ] in arm d )  . 
the independent data monitoring committee recommended stopping accrual to both celecoxib - containing arms on grounds of lack of bene t and discontinuing celecoxib for patients currently on treatment , which was endorsed by the trial steering committee . interpretation celecoxib 400 mg twice daily for up to 1 year is insu ciently active in patients starting hormone therapy for high - risk prostate cancer , and we do not recommend its use in this setting . 
accrual continues seamlessly to the other research arms and follow - up of all arms will continue to assess e ects on overall survival . funding cancer research uk , p zer , novartis , sano - aventis , medical research council ( london , uk )  . introduction prostate cancer is a major health problem worldwide , accounting for nearly a fth of all newly diagnosed male cancers . 
in the uk , roughly 35 000 men are diagnosed with prostate cancer each year , and in 2008 almost 10 000 men died from the disease.1 globally , 913 000 cases were diagnosed in 2008.2 the current standard rst - line treatment for locally advanced or metastatic prostate cancer is hormone therapy , achieved either surgically with bilateral orchidectomy or medically with luteinising hormone releasing hormone ( lhrh ) agonists or antagonists , or oral antiandrogens , 3 with additional radiotherapy for locally advanced cases.4 , 5 hormone therapy produces responses in up to 95% of patients , but lancet oncol 2012 ; 13 : 54958 published online march 26 , 2012 doi : 10.1016 / s14702045 ( 12 ) 70088 - 8 this online publication has been corrected . 
at this point , patients are potentially tter and better able to tolerate treatment , and intervention in the hormone - naive setting might have a better and more durable e ect . innovative , multiarm , multistage the stampede trial ( systemic therapy for advanced or metastatic prostate cancer : evaluation of drug e cacy ; medical research council [ mrc ] pr08 ) is ( mams ) , multicentre , randomised controlled trial . 
we designed the trial to assess the e ects of a bisphosphonate ( zoledronic acid ) , a cytotoxic chemotherapy drug ( docetaxel ) , and a cyclo - oxygenase - 2 ( cox - 2 ) inhibitor ( celecoxib ) , as single agents or combinations , in patients locally advanced or starting hormone therapy for metastatic prostate cancer . 
the trial is designed with separate stages focusing on safety , activity , and e cacy data ; a research arm is only allowed to proceed to the nal stage of recruitment if the study treatment is shown to be acceptably safe and su ciently active . 
we refer to lack of su cient activity as lack of bene t . cox - 2 is an isoenzyme induced by various mitogens , cytokines , and growth factors that are associated with a range of processes including in ammation12 and carcinogenesis.13 , 14 various case - control studies have shown a reduction in risk of prostate cancer associated with the use of non - steroidal anti - in ammatory drugs ( nsaids ) , which include inhibition of cox - 2 among their mode of action.15 pathological studies show that cox - 2 is upregulated in carcinomas , 16 and one study suggested that nsaid use might delay progression from subclinical to clinical prostate cancer.17 this combination of preclinical and epidemiological data justi ed assessment of a cox - 2 inhibitor in the present trial . the trial development group ( including clinical researchers , statisticians , trialists , and patient representatives ) chose to assess the selective cox - 2 inhibitor , celecoxib , because data suggest that it is better tolerated than other nsaids , exhibits activity as a cancerpreventing agent , 18 and shows inhibition of angiogenesis and induction of apoptosis in human cancer cells including prostate cancer , 19 particularly at higher doses.20 this decision was taken after full consideration of the risks and bene ts , in view of reports of potential adverse cardiovascular e ects.21 no safety concerns were raised during the pilot phase and the rst intermediate activity analysis , and the celecoxib arms were permitted to continue accrual . 
here , we report the results of the second intermediate analysis comparing hormone therapy alone with hormone therapy plus celecoxib . methods study design and participants stampede uses an adaptive multiarm , multistage design.22 , 23 this seamless phase 23 design starts with several trial arms and uses an intermediate outcome to adaptively focus accrual away from the less encouraging research arms , continuing accrual only with the more active interventions . 
the intermediate primary outcome is failure - free survival ( ffs ) de ned as the rst of : psa failure ( psa > 4 ng / ml and psa > 50% above nadir ) ; local progression ; nodal progression ; progression of existing metastases or development of new metastases ; or death from prostate cancer . 
ffs is used as a screening method for activity on the assumption that any treatment that shows an advantage in overall survival will probably show an advantage in ffs beforehand , and that a survival advantage is unlikely if an advantage in ffs is not seen . 
it is not assumed that ffs is a surrogate for overall survival ; an advantage in ffs might not necessarily into a survival advantage . translate the trial is managed by a trial management group ( tmg ) chaired by the chief investigator . 
accumulating comparative data are reviewed by the independent data monitoring committee ( idmc ) and recommendations are made to the trial steering committee ( tsc ) , which includes independent members , who have the nal responsibility for decision making ( eg , on stopping arms )  . 
we included patients with newly diagnosed prostate cancer with metastases to bone , node - positive disease , or clinically localised disease with high - risk features ( at least two of the following : t category 3 or 4 , gleason sum score 810 , or psa 40 ng / ml )  . 
 additionally , men failing previous localised therapy were eligible ( subject to restrictions on prior hormone therapy ) if they had a psa concentration of 4 ng / ml or 550 vol 13 may 2012 articles higher and doubling time of less than 6 months , or psa 20 ng / ml or higher , or nodal or metastatic relapse . patients had to be t for any of the trial treatments , with adequate haematological , renal , and liver function , and have a who performance status of 0 or 1 . 
all patients provided written informed consent . randomisation and masking computer - based randomisation was done centrally ( via telephone ) using minimisation with a random element of 80% allocation towards minimising arms , balancing on minimisation factors of randomising centre , metastases , nodal involvement , age at randomisation , who performance status , type of hormone therapy , regular aspirin or nsaid use at baseline , and planned use of radiotherapy . 
patients could be allocated primary outcome hazard ratio power onesided alpha critical hazard ratio control events stage i : activity stage ii : activity stage iii : activity stage iv : e cacy os 075 075 075 075 0500 100 0250 092 0100 089 0025 ffs = failure - free survival . 
 further details on the design and conduct of the trial are presented elsewhere.24 , 25 procedures all patients were planned to receive long - term hormone therapy for at least 2 years , and were allowed to start longterm hormone therapy up to 12 weeks before randomisation . 
the permitted methods of hormone therapy were lhrh analogues ( with short - term antiandrogens to cover disease are when necessary ) , maximum androgen blockade , lhrh antagonists , orchidectomy , or , patients without metastasis , bicalutamide monotherapy ( 150 mg daily ) ; choice of hormone therapy was based on clinician and patient preference . 
radiotherapy was encouraged for men with n0m0 disease ( stratifying on intent ) , with a target window of 69 months after starting hormone therapy , so that radiotherapy could be given at the same time in all trial arms and patients would not have chemotherapy and radiotherapy concomitantly . 
 patients allocated to celecoxib were planned to receive one 400 mg capsule twice daily , taken orally , until 1 year or an ffs event . patients were followed up every 6 weeks for 6 months , then every 12 weeks for 2 years , then every 6 months for 5 years , and annually thereafter . 
 2043 men starting long - term hormone therapy for prostate cancer randomised 584 arm a ( control ht - alone ) 292 arm c ( ht + docetaxel ) 291 arm d ( ht + celecoxib ) 293 arm b ( ht + zoledronic acid ) 292 arm e ( ht + docetaxel + zoledronic acid ) 291 arm f ( ht + celecoxib + zoledronic acid ) intermediate data presented in this report data remain masked : excluded from this report data remain masked : excluded from this report intermediate data presented in this report data remain masked : excluded from this report data remain masked : excluded from this report 584 hormone therapy ( 100% ) 0 celecoxib ( 0% ) 582 activity analysis ( 100% ) * 527 safety analysis ( 90% ) 209 ffs events median ffs = 27 months 291 hormone therapy ( 100% ) 245 celecoxib ( 84% ) 291 activity analysis ( 100% ) 259 safety analysis ( 89% ) 96 ffs events median ffs = 24 months accrual continues follow - up ongoing accrual continues follow - up ongoing accrual continues follow - up ongoing accrual stopped follow - up ongoing accrual continues follow - up ongoing accrual stopped follow - up ongoing figure 1 : trial pro le ht = hormone therapy . 
this is because the control group is in every pairwise comparison and the power of these comparisons is improved by having more patients in this group . statistical analysis the sample size was calculated using - nstageand its predecessor programs . 
we targeted a 25% relative reduction in events ( hazard ratio [ hr ] 075 ) for both ffs and survival ; this translates to a 9% absolute improvement at the median time . 
these parameters were chosen to ensure that meaningful amounts of new data would be accumulated between intermediate analyses , which were triggered when speci c numbers of events had been reported in the control group ( table 1 )  . 
the overall alpha and power levels represent the values for each pairwise comparison of research arm against the common control arm , accounting for intermediate analyses and repeated use of the control arm . the statistical design parameters translate into a series of activity hurdles against which each research arm is compared at three prede ned intermediate analyses.24 at the end of the second activity stage , reported here , the hr cutpoint was 0924 , determined with 95% power and a one - sided alpha of 025 , with analyses planned for when roughly 216 ffs events had been reported in the control group . 
it was anticipated that research arms with an hr less favourable than the cutpoint would be considered as showing insu cient activity and accrual might therefore be stopped ; accrual would continue to the remaining trial arms to collect further evidence . there is no single sample size target for stampede ; the trial targets a total of 405 deaths in the control arm in comparisons with active research arms , but the number of patients required to observe these events depends on the accrual rate , actual event rate ( mix of patients joining the trial ) , and number of research arms shown the intermediate stages . 
the duration of accrual and follow - up are adjusted to obtain this target.24 we anticipated that around 25004000 patients would join stampede over 68 years , with around 1500 patients in comparisons of research arms showing encouraging evidence at each intermediate analysis . 
twice as many patients are recruited to the control group as to any of insu ciently active at to be standard survival analysis methods were used for time - to - event data . 
coxs proportional hazards models were used to estimate the relative treatment e ects , adjusting for key strati cation factors , with relative improvements expressed as hrs ; hr less than 100 favours a research ar the proportional hazards assumption was tested ; provision was made to report restricted mean survival times and to translate the stopping boundaries appropriately in the instance of a non - proportional treatment e ect over time.26 all cis are provided at the 95% level for tradition , but a one - sided 75% ci is also included for primary comparison of ffs , in line with the trial design . 
 analyses were done with stata ( version 11 )  . the trial is registered with clinicaltrials.gov , number nct00268476 , and with current controlled trials , number isrctn78818544 . role of the funding source the trial was sponsored by the mrc and conducted by the mrc clinical trials unit . 
 ( continues in next column ) table 2 : baseline characteristics vol 13 may 2012 articles months number of patients ( stopped ) 245 ( 28 ) 194 ( 25 ) 137 ( 19 ) 107 ( 32 ) 64 ( 52 ) 9 ( 7 ) figure 2 : time on celecoxib for patients in arm d ( hormone therapy plus celecoxib ) only patients who reported starting celecoxib treatment are included . 
the drop at 12 months re ects patients completing their trial treatment ; events before then represent patients stopping trial treatment sooner , for any reason . ht only ht + c time from randomisation ( months ) ( 160 ) ( 62 ) ( 35 ) ( 27 ) number of patients ( events ) ht only ht + c figure 3 : kaplan - meier curve of failure - free survival in arm a ( hormone therapy alone ) versus arm d ( hormone therapy plus celecoxib ) ht = hormone therapy . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results data were frozen on feb 1 , 2011 , for review by the idmc on march 31 , 2011 . 
figure 1 shows the ow of patients through the trial ; table 2 gives the baseline characteristics of patients in this comparison . in both arms , androgen - deprivation therapy was lhrh based in nearly all patients ( 574 of 584 [ 98% ] in the control group and 286 of 291 [ 98% ] in the hormone therapy plus celecoxib group ) , with radiotherapy planned for around a quarter of patients . 
the reason for stopping celecoxib was known for 107 of these patients : 45 ( 42% ) completed protocol treatment , 30 ( 28% ) had disease progression , 12 ( 11% ) had excessive toxicity , and 20 ( 19% ) stopped for other reasons . 
in the hormone therapy plus celecoxib group , median ffs was 24 months ( 95% ci 1733 ) , with an ffs at 2 years of 51% ( 95% ci 4358 )  . in the 209 patients in the control group who had an ffs event , the rst reported event was psa failure in 163 patients ( 78% ) , metastases in 33 ( 16% ) , local progression in ve ( 2% ) , lymph - node progression in ve ( 2% ) , and prostate - cancer - related death in three ( 1% )  . 
in the 96 patients in the hormone therapy plus celecoxib group who reported an ffs event , the rst event was psa failure in 75 ( 78% ) , metastases in 15 ( 16% ) , local progression in two ( 2% ) and prostate - cancer - related death in four ( 4% )  . at this second intermediate analysis , celecoxib showed insu cient evidence of activity , in terms of ffs , for continuation of accrual to this comparison : hr 094 from adjusted cox model ( 75% ci upper limit 103 ; 95% ci 074120 ; gure 3 )  . 
 because of the lack of bene t indicated by this analysis , the idmc recommended discontinuing recruitment to both celecoxib - containing groups ( hormone therapy plus celecoxib [ arm d ] , and hormone therapy plus celecoxib plus zoledronic acid [ arm f ] ) , and this was endorsed by the tsc . 
treatment with zoledronic acid continues in the combination group ( armf )  . there is some evidence of non - proportional hazards in the data , which is mostly explained by who performance status ( p = 0007 ) ; there was no evidence that the hazards for the treatment e ect are non - proportional over time ( p = 0387 )  . 
grade 35 tox icities were reported at any time by 123 ( 23% ; 95% ci 2027 ) patients in the control group and 64 ( 25% , 1930 ) in the hormone therapy plus celecoxib group . 
these data , including those for the hormone therapy plus celecoxib plus zoledronic acid group , remain con dential to the idmc and will only be available to the tsc after future analyses . discussion in the stampede trial , we are assessing several drugs in combination with hormone therapy in patients with high - risk localised or metastatic prostate cancer . 
 resources are focused on trial arms most likely to show a clinically meaningful survival bene t by using lack - of - bene t analyses and stopping intermediate accrual to arms showing insu cient activity or adverse safety pro les . the celecoxib arm continued accrual through the rst intermediate analysis ( target hr 100 ) , but accrual was stopped after the second intermediate analysis when the target hr was more di cult to pass , at 092 . 
although there were no safety concerns raised by the idmc , there was no evidence of bene t when the totality of the data were taken into consideration , and the tsc recommended that treatment with celecoxib stop for patients still receiving the drug . our premise is that an advantage in overall survival should be preceded by an advantage in ffs , so we do not anticipate a later bene t with celecoxib emerging ; however , this remains to be determined in subsequent analysis of overall survival after longer follow - up . 
in some crpc studies this assumption has not held up , particularly studies with the immunotherapy sipuleucel - t , where a survival advantage has been shown without a prior bene t in psa progression.10 the potential mechanisms of action of celecoxib are not androgen - linked , so it is reasonable to assume that they might not be re ected in psa - based measures of ffs ; on this basis , we continue long - term patient follow - up and avoid de nitive statements relating to the overall e cacy of cox - 2 inhibition and prostatecancer survival in this setting . recruitment was also stopped to the hormone therapy plus celecoxib plus zoledronic acid group ; data for this arm have not been revealed to avoid inappropriate in uence on recruitment in the other zoledronic acidcontaining arms . 
the patients in both celecoxib - containing groups remain in the trial and will continue to be followed vol 13 may 2012 articles up to provide data on overall survival . 
there would have been limited power for such a comparison at this stage . celecoxib , a selective cox - 2 inhibitor , was selected on the basis of preclinical13 , 14 , 19 and clinical1618 data suggesting possible utility in prostate cancer ( panel )  . 
the celecoxib dose and treatment duration chosen for the trial ( 400 mg twice daily for 12 months ) was based on the dose used for prevention of familial polyposis coli20 and the need to minimise potential for cardiovascular risk , which seems to present with treatment durations longer than 12 months.21 the dose and duration were selected after a comprehensive literature review followed by joint discussion with patient representatives on the tmg , emphasising the importance of such collaboration in the design and conduct of clinical trials . external clinical trial data that have emerged since the launch of stampede have been equivocal as to the value of cox - 2 inhibitors in prostate27 , 28 and colorectal29 , 30 cancers . 
so far , published trials have not supported the use of cox - 2 inhibitors unequivocally in any established cancer type ; our trial adds further evidence of their limited clinical utility in established tumours . 
we do note panel : research in context systematic review at the time of trial design , there was substantial epidemiological , laboratory , and clinical evidence that cox - 2 has a role in development and progression of a range of cancers , including prostate cancer . 
celecoxib was chosen for assessment in hormone - sensitive prostate cancer based on in - vitro evidence of activity and data in other cancers , particularly familial polyposis coli , where it has a role in prevention of progression from polyp to cancer . 
we assessed a range of drugs with cox - 2 - inhibitory properties and selected celecoxib based on the data in familial polyposis coli and its safety pro le in large - scale trials of other diseases . 
 data from trials of celecoxib in established cancers have been tracked through the registers ( including alerts and clinicaltrials.gov ) , and lead investigators have been contacted for information each time reviews are updated but registers do not include recent data . interpretation at the second preplanned intermediate analysis , we have shown that celecoxib given at 400 mg twice daily for 1 year is insu ciently active in high - risk , hormone - sensitive prostate cancer to signi cantly a ect failure - free survival . 
other trials in prostate cancer ( and other cancer types ) have not supported the use of cox - 2 inhibitors unequivocally in any setting , and our trial adds further evidence of the limited clinical utility of these drugs in established , advanced cancer . 
first , there could be lack of expression of the target molecule cox - 2 , which we could retrospectively assess by collecting tissue blocks and studying cox - 2 expression . 
second , there might be a lack of on - target activity ; celecoxib was chosen because of documented activity in the setting of familial polyposis coli , 20 thus it seems reasonable to assume that the drug dose and delivery are within the necessary therapeutic range . 
the initial planned duration of therapy was 2 years , but in view of the excess cardiovascular problems reported with rofecoxib29 just before accrual to stampede , a shorter duration was selected . 
even if the duration was too short for optimum e ect , we would still expect some e ect , particularly with a median time to progression of around 2 years . a key strength of stampede is that several therapeutic combinations are tested synchronously , thereby shortening the time to assess e cacy and toxicity in new drug combinations in hormone - naive patients undergoing hormone therapy . 
the entry criteria were intended to de ne a population with a poor prognosis , requiring long - term hormone therapy , and to test the hypothesis that interventions at the point of rst hormone manipulation improve long - term outcome . 
 the trial is predicated on the notion that high - risk prostate cancer includes a range of patients , from those with localised disease and poor prognostic characteristics ( based on t category , psa , and gleason score ) to those presenting with metastatic disease , and that current therapies have limited long - term e cacy in many cases . 
it seems likely that median survival will be higher than originally anticipated , which might be partly related to new , active therapies that patients can receive after their rst trial ffs event . 
further agents are emerging , including abiraterone , 34 cabazitaxel , 35 sipuleucel - t , 10 radium - 223 , 36 and mdv3100.37 , 38 with the recent demonstration of a 556 vol 13 may 2012 articles survival bene t with radical radiotherapy in patients with locally advanced disease , 4 , 5 we anticipate further improve ments in ffs and overall survival ; indeed , the trial was amended in november , 2011 , to mandate the use of radiotherapy in newly diagnosed n0m0 disease following these results.5 the accumulating event rate is monitored as part of trial oversight processes . the remaining trial arms continue to recruit new patients and their data remain masked . 
researchers might infer that there is at least some evidence of improved ffs in these arms , but such evidence is not su cient to stop or change the trial . 
a further change to the trial occurred in november , 2011 , with the intro duction of hormone therapy plus abiraterone as a new research arpatients in the new arm will only be compared with those randomised contemporaneously to the control group . 
the trial can adaptively introduce further research arms and stop early those arms showing a lack of bene t.24 further research arms are likely to be introduced into the trial . 
in conclusion , we have shown that celecoxib given 400 mg twice daily for 1 year is insu ciently active for men starting long - term therapy for high - risk prostate cancer , and we do not recommend its use in this setting . contributors ndj is chief investigator for the trial . 
all other authors declared that they have no con icts of interest . acknowledgments this work is partly funded by cancer research uk ( grant cruk / 06 / 019 )  . 
wededicate this report to the memory of jim stansfeld , patient representative on the trial management group at the design stage , who was crucial to the inclusion of celecoxib as a research arm in stampede . 
we thank members of the independent data monitoring committee ( christopher williams [ chair ] , doug altman , bertrand tombal , and reg hall ) , the trial steering committee ( jonathan ledermann [ chair ] , david kirk , and jim paul ) , and pamela bramble and altaf moledina from p zer , for providing technical advice on celecoxib . 
see appendix for the full list of investigators and sites , and for contributions from mrc sta members . editorial for more on cancer risk after organ transplantation see jama 2011 ; 306 : 1891901 for more on tg4010 see articles lancet oncol 2011 ; 12 : 112533 tapping our immune potential to realise the ultimate goal last month , the immune surveillance theorywhich proposes that the immune system continuously identi es , and removes , malignant cells as they arisewas lent further weight by an article in jama , which showed that recipients of organ transplants have an increased risk for an array of cancersboth related and unrelated to infection compared with the general population . 
an increase in infection - related cancers ( eg , non - hodgkin lymphoma , gastric cancer , anal cancer , and kaposis sarcoma ) might be anticipated , given that use of immunosuppression to reduce the risk of transplant rejection is likely to result in poor immune control of known oncogenic pathogens . 
 however , the increased risk of , for example , lung and kidney cancers after transplantation noted in a range of patients receiving di erent organs cannot be so easily explained . 
although underlying medical disorders or treatment - related toxicities might have a role , the dampening of the immune system is also likely to be a factor in the development of cancers that are seemingly unrelated to infection . harnessing the immune system to combat cancer has long been a major goal , potentially o ering a more targeted and thus safer means of treatment . 
early attempts to alter the immune milieu for therapeutic gain involved the use of various cytokines , but despite eliciting some durable responses , cytokine treatments can be associated with substantial toxicities , in part because of their non - speci c mode of action . 
further , haemopoietic stem - cell transplantation has long been used in the treatment of haematological malignancies to induce a graft versus disease e ect ; however , treatment - related mortality , availability of donors , and complications from graft versus host disease remain problematic . a more targeted immune approach is an attractive proposition . 
as a result of the successful development of many vaccines against infectious diseases , and their more speci c e ects on the immune system , much e ort has been expended on vaccination strategies against viruses associated with malignancies . 
successes have been achieved with prophylactic vaccines , such as the human papillomavirus ( hpv ) vaccines aimed at precursors of cervical cancer ; however , vaccines against infection by other cancer - associated viruses such as epsteinbarr virus have remained elusive , despite many decades of research and clinical e orts . 
 despite the notable achievement of e ective prophylactic hpv vaccines , less progress has been made in therapeutic vaccine design , both against hpv and other viruses , or in the development of immune - targeted vaccines , with many attempts yielding little evidence of clinical activity . 
 the e cacy of therapeutic vaccines is also limited by the fact that many tumour antigens are self - antigens , and as such the body has an inbuilt tolerance to them ; immunological responses elicited in response to vaccines are thus often insu cient to produce a clinical bene t . however , highlighting the potential usefulness of treatments that manipulate the immune system , several therapeutic strategies are in late - stage trials or entering the clinic . 
 immunomodulatory drugs , such as thalidomide and lenalidomide , are also an established part of the therapeutic armamentarium for various haematological malignancies , although these drugs have multiple modes of action , not only on the immune systefurthermore , combinations of immunotherapy with more conventional anticancer approaches are beginning to yield promising results , as exempli ed by the improvements in progression - free survival for patients with non - small - cell lung cancer seen with the combination of tg4010 , a muc1 - targeted vaccine , and chemotherapy . to fully realise the potential of an immune - based approach , our understanding of the immune systems complex machinery will need to continue to improve at an exponential rate . 
only then can our approaches to control and make use of the hosts immune system become more sophisticated and e cient , allowing us to develop more re ned approaches that tap into a patients natural defence mechanisms , with the ultimate goal of treating cancer without poisoning the patient . 
 the lancet oncology vol 12 december 2011 1175 editorial for more on cancer risk after organ transplantation see jama 2011 ; 306 : 1891901 for more on tg4010 see articles lancet oncol 2011 ; 12 : 112533 tapping our immune potential to realise the ultimate goal last month , the immune surveillance theorywhich proposes that the immune system continuously identi es , and removes , malignant cells as they arisewas lent further weight by an article in jama , which showed that recipients of organ transplants have an increased risk for an array of cancersboth related and unrelated to infection compared with the general population . 
an increase in infection - related cancers ( eg , non - hodgkin lymphoma , gastric cancer , anal cancer , and kaposis sarcoma ) might be anticipated , given that use of immunosuppression to reduce the risk of transplant rejection is likely to result in poor immune control of known oncogenic pathogens . 
 however , the increased risk of , for example , lung and kidney cancers after transplantation noted in a range of patients receiving di erent organs cannot be so easily explained . 
although underlying medical disorders or treatment - related toxicities might have a role , the dampening of the immune system is also likely to be a factor in the development of cancers that are seemingly unrelated to infection . harnessing the immune system to combat cancer has long been a major goal , potentially o ering a more targeted and thus safer means of treatment . 
early attempts to alter the immune milieu for therapeutic gain involved the use of various cytokines , but despite eliciting some durable responses , cytokine treatments can be associated with substantial toxicities , in part because of their non - speci c mode of action . 
further , haemopoietic stem - cell transplantation has long been used in the treatment of haematological malignancies to induce a graft versus disease e ect ; however , treatment - related mortality , availability of donors , and complications from graft versus host disease remain problematic . a more targeted immune approach is an attractive proposition . 
as a result of the successful development of many vaccines against infectious diseases , and their more speci c e ects on the immune system , much e ort has been expended on vaccination strategies against viruses associated with malignancies . 
successes have been achieved with prophylactic vaccines , such as the human papillomavirus ( hpv ) vaccines aimed at precursors of cervical cancer ; however , vaccines against infection by other cancer - associated viruses such as epsteinbarr virus have remained elusive , despite many decades of research and clinical e orts . 
 despite the notable achievement of e ective prophylactic hpv vaccines , less progress has been made in therapeutic vaccine design , both against hpv and other viruses , or in the development of immune - targeted vaccines , with many attempts yielding little evidence of clinical activity . 
 the e cacy of therapeutic vaccines is also limited by the fact that many tumour antigens are self - antigens , and as such the body has an inbuilt tolerance to them ; immunological responses elicited in response to vaccines are thus often insu cient to produce a clinical bene t . however , highlighting the potential usefulness of treatments that manipulate the immune system , several therapeutic strategies are in late - stage trials or entering the clinic . 
 immunomodulatory drugs , such as thalidomide and lenalidomide , are also an established part of the therapeutic armamentarium for various haematological malignancies , although these drugs have multiple modes of action , not only on the immune systefurthermore , combinations of immunotherapy with more conventional anticancer approaches are beginning to yield promising results , as exempli ed by the improvements in progression - free survival for patients with non - small - cell lung cancer seen with the combination of tg4010 , a muc1 - targeted vaccine , and chemotherapy . to fully realise the potential of an immune - based approach , our understanding of the immune systems complex machinery will need to continue to improve at an exponential rate . 
only then can our approaches to control and make use of the hosts immune system become more sophisticated and e cient , allowing us to develop more re ned approaches that tap into a patients natural defence mechanisms , with the ultimate goal of treating cancer without poisoning the patient . 
we investigated whether erlotinib improves clinical outcome in these patients . methods topical was a double - blind , randomised , placebo - controlled , phase 3 trial , done at 78 centres in the uk . 
 eligibility criteria were newly diagnosed , pathologically con rmed nsclc ; stage iiib or iv ; chemotherapy naive ; no symptomatic brain metastases ; deemed unsuitable for chemotherapy because of poor ( 2 ) eastern cooperative oncology group performance status or presence of several comorbidities , or both ; and estimated life expectancy of at least 8 weeks . 
patients were randomly assigned ( by phone call , in a 1 : 1 ratio , strati ed by disease stage , performance status , smoking history , and centre , block size 10 ) to receive oral placebo or erlotinib ( 150 mg per day ) until disease progression or unacceptable toxicity . 
this study is registered , number isrctn 77383050 . findings between april 14 , 2005 , and april 1 , 2009 , we randomly assigned 350 patients to receive erlotinib and 320 to receive placebo . 
657 patients died ; median overall survival did not di er between groups ( erlotinib , 37 months , 95% ci 3242 , vs placebo , 36 months , 3239 ; unadjusted hazard ratio [ hr ] 094 , 95% ci 081110 , p = 046 )  . 
59% ( 178 of 302 ) of patients assigned erlotinib and who were assessable at 1 month developed rst - cycle rash , which was the only independent factor associated with overall survival . 
 compared with placebo , overall survival seemed to be worse in the group that did not develop rst - cycle rash ( 130 , 105161 , p = 0017 )  . 
grade 3 or 4 diarrhoea was more common with erlotinib than placebo ( 8% [ 28 of 334 ] vs 1% [ four of 313 ] , p = 00001 ) , as was high - grade rash ( 23% [ 79 of 334 ] vs 2% [ ve of 313 ] , p < 00001 ) ; other adverse events were much the same between groups . interpretation patients with nsclc who are deemed unsuitable for chemotherapy could be given erlotinib . 
patients who develop a rst - cycle rash should continue to receive erlotinib , whereas those who do not have a rash after 28 days should discontinue erlotinib , because of the possibility of decreased survival . fundingcancer research uk , roche . introduction lung cancer , the main cause of cancer - related death , accounts for nearly 14 million deaths worldwide every year , and has an annual incidence of more than 41 000 in the uk ( age standardised incidence of 48 per 100 000 ) .1 mortality from lung cancer accounts for more than 452 000 deaths in china , 342 000 in europe , and 162 000 in the usa.1 the number of lung - cancer deaths in developing countries is expected to increase during the next few decades such that by 2030 about 70% of tobacco - related deaths will occur in these countries . 
however , most patients with advanced or metastatic nsclc are elderly ( median age 72 years2 ) and many receive only active supportive care , including palliative radiotherapy , because of physician choice , poor performance status , or presence of several comorbidities.2 , 3 therefore , despite the recom mendation to treat these patients with platinum - based chemo therapy , only about 25% of elderly ( age > 65 years ) us patients3 and 29% of newly diagnosed uk patients2 currently receive any cytotoxic treatment . erlotinib is an oral egfr inhibitor that is associated with a signi cant survival bene t among patients with nsclc when used as maintenance monotherapy after rst - line chemotherapy or as second - line or third - line monotherapy.46 in chemotherapy - naive patients with vol 13 november 2012 1161 articles activating egfr mutations , erlotinib signi cantly improved progression - free survival compared with chemotherapy.7 , 8 we did a large randomised trial to determine whether erlotinib monotherapy would be bene cial as rst - line therapy in unselected patients with advanced nsclc deemed unsuitable for chemotherapy . methods study design and participants topical was a superiority phase 3 , double - blind , randomised , placebo - controlled trial . 
eligibility criteria were newly diagnosed , pathologically con rmed nsclc ; stage iiib or iv disease ; chemotherapy naive ; no symptomatic brain metastases ; deemed unsuitable for chemotherapy because of poor eastern cooperative oncology group ( ecog ) performance status ( ps 2 ) or presence of several comorbidities ( including impaired renal function with creatinine clearance < 60 ml / min ) , or both ; and estimated life expectancy of at least 8 weeks . 
other inclusion criteria were age older than 18 years , diagnosis within the past 62 days , able to take oral medication , and using e ective contraception if appropriate . 
exclusion criteria were previous treatment with any biological anticancer therapy ; previous palliative radiotherapy ( except to bone metastases , within the previous 2 weeks ) ; pregnant or lactating women ; evidence of signi cant laboratory nding or concurrent uncontrolled medical illness judged to 670 patients randomised 350 patients assigned erlotinib 329 received erlotinib 16 did not start study treatment 5 missing data * 320 patients assigned placebo 311 received placebo 7 did not start study treatment 2 missing data * 39 ineligible 1 ecog 0 / 1 with crcl > 60 ml / min 38 > 62 days of diagnosis 40 ineligible 4 ecog 0 / 1 with crcl > 60 ml / min 36 > 62 days of diagnosis 350 analysed by intention to treat 320 analysed by intention to treat reasons for stopping 2 still on study drug at end of follow - up 14 completed 12 months 40 protocol toxicity 20 non - protocol toxicity 16 clinical morbidity 21 voluntary withdrawals ( not toxicity ) 84 progressive disease 126 died 6 other 16 never started study drug 5 missing data reasons for stopping 0 still on study drug at end of follow - up 6 completed 12 months 12 protocol toxicity 13 non - protocol toxicity 2 clinical morbidity 26 voluntary withdrawals ( not toxicity ) 119 progressive disease 119 died 1 unavailable 13 other 7 never started study drug 2 missing data figure 1 : trial pro le * patients with no recorded start date of study drug or dosing details . 
patients were randomised in a 1 : 1 ratio to either once daily oral erlotinib ( 150 mg tablets ) or matching placebo , with a computer generated sequence , strati ed by disease stage ( iiib , iv ) , performance status ( 01 , 2 , 3 ) , smoking history ( never , current / former ) , and centre ( 78 sites ) , with a block size of 10 . 
patients continued to receive active supportive care , including palliative radiotherapy , at the discretion of their clinician . the primary endpoint was overall survival , measured from the date of randomisation until death from any cause . 
secondary endpoints were progression - free survival ( time until progression or death from any cause ) , tumour response ( according to response evaluation criteria in solid tumours ) , adverse events , and quality of life . 
 within 4 weeks before randomisation patients had a physical examination , assessment of comorbidities with the charlson comorbidity index ( cci ) , blood count and biochemistry , chest radiograph , and ct of the chest and abdomen . 
 presence of several comorbidities was de ned as cci of 3 or more . clinicians did physical examinations , including assessment of performance status , development of rash , and adverse events ( with national cancer institute of canada common toxicity criteria for adverse events , version 3.0 ) , and a chest radiograph every month for the rst 12 months , and every 2 months thereafter . 
we graded rash with the criteria : erythema alone ( a ) , erythema with papules ( b ) , erythema with papules and pustules ( c ) , and erythema with papules 1162 vol 13 november 2012 and con uent pustules ( d )  . 
puri cation and assessment of quality and quantity of tumour dna were done with wizard genomic dna puri cation kit ( promega , madison , wi , erlotinib ( n = 350 ) placebo ( n = 320 ) age at randomisation median ( years ) 75 years 77 ( 7282 ) 220 ( 63% ) 77 ( 7281 ) 203 ( 63% ) usa )  . 
 * all patients with a performance score of 01 had comorbidities , ie , 92% ( 98 of 106 ) had cci scores of 3 , 95% ( 101 of 106 ) had creatinine clearance < 60 ml / min , and a median age of 81 years with 81% ( 86 of 106 ) aged > 75 years old . 
we calculated compliance to study treatment by dividing the total number of tablets taken ( equivalent to number of days on study drug ) by the number of days from randomisation to death , progression , or when treatment was stopped early , and expressed results as a percentage . 
preplanned subgroup analyses included sex , histological examination , activating egfr or kras mutation , stage , smoking status , ecog score , and development of rst - cycle rash . this study is registered , number isrctn 77383050 . role of the funding source the trial was funded by cancer research uk ( c1438 / a4147 ) , with an educational grant from roche for the translational studies , but neither were involved in trial design , data analyses or interpretation , or writing of this report . 
additional support came from the university college london and university college london hospital biomedical research centre , who had no role in study design , data collection , analysis , or interpretation , or writing of the report . 
the corresponding author had the nal responsibility for the decision to submit for publication . results we recruited 670 patients from 78 centres from the uk national cancer research network between april 14 , 2005 , and april 1 , 2009 . 
our randomisation procedure gave 936 cells and by chance the rst allocation in each cell for several centres was erlotinib , producing an imbalance in the number randomised to each group ; 350 participants were as signed to receive erlotinib and 320 placebo ( gure 1 )  . 
compliance to study treatment ( de ned as patients who took their tablets for 75% of the time that they were in the trial , until they died or stopped treatment early ) , was 58% ( 204 of 350 ) for erlotinib and 63% ( 203 of 320 ) for placebo ( median compliance was 88% [ iqr 098 ] for erlotinib and 86% [ 096 ] for placebo , appendix p 4 )  . 
 after discontinuation of study treatment , the most common subsequent therapy was palliative radiotherapy , which was given to 34% ( 119 of 350 ) of patients assigned erlotinib and 36% ( 114 of 320 ) of those assigned placebo . 
 only 2% ( 12 of 670 ) of patients received a tyrosinekinase inhibitor ( n = 3 ) or chemotherapy ( n = 9 ) after disease progression , seven in the placebo group and ve in the erlotinib group . 
the only tyrosine - kinase inhibitor used was erlotinib . 657 patients died ; 314 in the placebo group and 343 in the erlotinib group , with 93% ( 608 of 657 ) of deaths attributed to progressive disease . 
we identi ed no di erence in overall survival 1164 vol 13 november 2012 articles among all patients ; median overall survival was 37 months ( 95% ci 3242 ) in the erlotinib group versus 36 months ( 3239 ) in the placebo group ( unadjusted hr 094 , 95% ci 081110 , p = 046 ; adjusted hr 092 , 078107 , p = 031 )  . 
1 year overall survival was 14% ( 95% ci 1018 ) with placebo versus 15% ( 1219 ) with erlotinib . we identi ed a signi cant improvement in progression - free survival with erlotinib ( unadjusted hr 083 , 95% ci 071097 , p = 0019 ; adjusted hr 080 , 068093 , p = 00054 ) ; median progression - free survival was 28 months ( 95% ci 2630 ) with erlotinib versus 26 months ( 2429 ) with placebo ( gure 2b )  . 
tumour response rates are shown in the appendix ( p 5 ) ; 4% ( 15 of 350 ) of patients in the erlotinib group and 2% ( seven of 320 ) of those in the placebo group had a complete or partial tumour response . among the 647 patients who started study treatment , the occurrence of any grade 34 adverse event was 75% ( 252 of 334 ) with erlotinib and 70% ( 219 of 313 ) with placebo ( p = 012 , table 2 )  . 
more patients assigned erlotinib had rash at any time and of any grade than did those assigned placebo ( 56% [ 188 of 334 ] vs 15% [ 46 of 313 ] p < 00001 )  . 
 21% ( 69 of 334 ) of patients assigned erlotinib had diarrhoea of grade 12 versus 8% ( 24 of 313 ) for placebo ( p < 00001 ) , and rash and diarrhoea mainly occurred within the rst month of treatment . 
we recorded increased diarrhoea ( mean di erence 151 ) , hair loss ( 126 ) , sore mouth ( 64 ) , and decreased constipation ( 94 ) more frequently in patients assigned erlotinib than in those assigned placebo . [ p < 00001 ] , in prespeci ed subgroup analyses , rst - cycle rash among patients assigned erlotinib was the only signi cant independent factor ( hr 024 , 95% ci 016035 , p < 00001 ; table 3 ) associated with overall survival , from a stepwise selection multivariate analysis containing rash , sex , histological examination , ecog score , stage , and smoking status . 
patients were classi ed as having rst - cycle rash ( any grade ) when the rash occurred within the rst 28 days , which was when we made the rst assessment of rash . 
of the 647 patients who started study treatment , predictor variables for overall survival * rash women vs men ecog 01 vs 23 stage iiib vs iv ex - smoker vs smoker never smoker vs smoker hazard ratio ( 95% ci ) p value 024 ( 016035 ) < 00001 081 ( 059101 ) 087 ( 053140 ) 084 ( 061110 ) 092 ( 071118 ) 064 ( 036114 ) adenocarcinoma vs non - adenocarcinoma 092 ( 066129 ) predictor variables for progression - free survival rash women vs men 041 ( 027060 ) < 00001 074 ( 044103 ) 0058 adenocarcinoma vs non - adenocarcinoma 099 ( 071137 ) ecog 01 vs 23 stage iiib vs iv ex - smoker vs smoker never smoker vs smoker 091 ( 056148 ) 083 ( 059109 ) 098 ( 076127 ) 062 ( 035110 ) * for overall survival , p values from overall tests were p = 017 for sex , p = 062 for ecog , p = 084 for histological examination , p = 023 for stage , and p = 035 for smoking status . 
for progression - free survival , p values from overall tests were p = 006 for sex , p = 086 for ecog , p = 079 for histological examination , p = 021 for stage , and p = 028 for smoking status . 
result after a stepwise selection ; rash remained the only signi cant variable in the model for overall survival and progression - free survival . table 3 : summary of multivariate analysis for overall survival and progression - free survival 017 064 055 023 051 013 095 070 021 088 010 67 who died before this assessment were excluded from this subgroup analysis , to avoid bias by classi cation of them as not having rash . 
59% ( 178 of 302 ) of patients assigned erlotinib developed rst - cycle rash ( compared with 5% [ 15 of 278 ] assigned placebo ) , and we recorded a positive correlation between overall survival ( p < 00001 ) and progression - free survival ( p < 00001 ) with in creasing rash severity . among patients assigned erlotinib who developed rash ( compared with all those assigned placebo ) , overall survival was signi cantly longer ( hr 076 , 95% ci 063092 , p = 00058 ) , as was progression - free survival ( 066 , 054080 , p < 00001 )  . 
hazard ratios for patients assigned erlotinib who did not develop rash , compared with placebo , were 130 ( 95% ci 105161 , p = 0017 ) for overall survival , and 109 ( 089136 , p = 039 ) for progression - free survival , neither of which overlapped the corresponding intervals for patients who were treated with erlotinib and developed rash , indicating that they were signi cantly di erent ( ie , evidence for an interaction )  . 
 median overall survival was 62 months ( 95% ci 4872 ) for the erlotinib and rash group , 29 months ( 2337 ) for the erlotinib without rash group , and 41 months ( 3746 ) for placebo . 
1 year overall survival was 24% ( 95% ci 1729 ) for erlotinib and rash , 10% ( 516 ) for erlotinib without rash , and 18% ( 1221 ) for placebo . 
for erlotinib and rash compared with placebo , the number needed to treat to save one life at 6 months was seven and vol 13 november 2012 1165 articles erlotininb , no rash ( events 120 ) erlotininb , rash ( events 175 ) placebo ( events 272 ) erlotinib , no rash vs placebo hr 130 ( 95% ci 105161 ) p = 0017 erlotinib , rash vs placebo hr 076 ( 95% ci 063092 ) p = 00058 number at risk erlotinib , no rash erlotinib , rash placebo erlotininb , no rash ( events 122 ) erlotininb , rash ( events 173 ) placebo ( events 278 ) erlotinib , no rash vs placebo hr 109 ( 95% ci 089136 ) p = 039 erlotinib , rash vs placebo hr 066 ( 95% ci 054080 ) p < 00001 number at risk erlotinib , no rash erlotinib , rash placebo time since randomisation ( months ) figure 3 : overall survival and progression - free survival according to whether patients on erlotinib developed rst - cycle rash or not hr = hazard ratio . 
median progression - free survival was 34 months ( 95% ci 3140 ) for erlotinib and rash , 25 months ( 2228 ) for erlotinib without rash , and 29 months ( 2732 ) for placebo . we identi ed overall survival bene ts in patients who developed rst - cycle rash in all subgroups including those with the worst characteristics : ecog performance status 3 , overall survival hr 058 ( 95% ci 038089 , p = 0012 ) and progression - free survival hr 041 ( 026065 , p < 00001 ) ; stage iv , overall survival hr 066 ( 052084 , p < 00001 ) and progression - free survival hr 056 ( 044072 , p = 00009 ) ; and age 75 years or older , overall survival hr 077 ( 061097 , p = 0028 ) and progression - free survival hr 071 ( 056089 , p = 00032 )  . 
 kaplan - meier curves for overall survival were much the same for patients assigned placebo who did or did not develop rash ( p = 035 , data not shown )  . patients assigned erlotinib who developed rst - cycle rash had a higher occurrence of fatigue and diarrhoea than did those assigned erlotinib who did not develop rash ( appendix p 7 )  . 
the proportions with grade 34 fatigue were 30% ( 53 of 178 ) for erlotinib and rash , 19% ( 24 of 124 ) for erlotinib without rash , and 26% ( 72 of 278 ) for placebo . 
for grade 34 diarrhoea , the proportions were 11% ( 20 of 178 ) for erlotinib and rash , 6% ( eight of 124 ) for erlotinib without rash , and 1% ( four of 278 ) for placebo . 
when we excluded rst - cycle rash , the proportion of patients reporting at least four grade 34 adverse events was 47% ( 84 of 178 ) for erlotinib and rash , 19% ( 23 of 124 ) for erlotinib without rash , and 36% ( 99 of 278 ) for placebo ( appendix p 8 )  . 
among patients assigned erlotinib who developed rash , we recorded much the same e ects on quality of life as we did in the main analysis , with dyspnoea ( 93 ) and chest pain ( 67 ) signi cantly improved compared with patients without rash ( appendix p 9 )  . appendix p 2 shows the results of the other prespeci ed subgroup analyses , according to the presence or absence of rash in participants assigned erlotinib . 
among patients without rash , we identi ed no evidence of bene t , and overall survival might be worse for some subgroups , such as men ( hr 152 , 95% ci 113204 , p = 00046 ) , or ecog performance status 3 ( 169 , 111258 , p = 0014 )  . 
 patients assigned erlotinib who developed rash had longer overall survival and progression - free survival than did those assigned erlotinib who did not develop rash irrespective of baseline charac teristics , although some subgroups , including women ( overall survival hr 066 , 95% ci 048090 , p = 00090 ) and patients with adenocarcinoma ( 055 , 039077 , p = 000049 ) seemed to have a greater bene t than did other subgroups . 
 median overall survival for erlotinib and rash versus placebo was 81 months ( 95% ci 62104 ) versus 45 months ( 3956 ) for women , and 49 months ( 4163 ) versus 38 months ( 3344 ) for men . 
 however , the interaction test between sex and treatment was not signi cant ( p = 029 ) , and some of this di erence might be explained by a higher compliance to erlotinib in women ( 68% , 81 of 119 ) than in men ( 52% , 101 of 195 )  . 
 appendix p 10 shows further results for overall survival and progression - free survival according to sex and histological examination . in our biological substudy , dna was available for 390 patients out of 398 ( 58% of total study population ) who provided material . 
of the 28 egfr mutation - positive samples , 11 had exon 19 deletions , ten had a mutation at exon 21 ( 858leuarg ) , and seven had other mutations . 
in these patients , median overall survival was 104 months ( 95% ci 55151 ) for erlotinib ( n = 17 ) versus 37 months ( 03493 ) for pla cebo ( n = 11 )  . 
 among patients with wild - type egfr who were assigned erlotinib and developed rash ( n = 94 ) , hr for overall survival was 086 ( 95% ci 066112 , p = 027 ) and for progression - free survival was 069 ( 053090 , p = 00070 ; appendix p 2 )  . 
hr for those assigned erlotinib who did not develop rash ( n = 67 ) was 128 ( 095172 , p = 010 ) for overall survival and 105 ( 078141 , p = 074 ) for progression - free survival . kras mutation - positivity was not associated with overall survival or progression - free survival . 
among those who were kras mutation - positive , median overall survival was 42 months ( 95% ci 1862 ) for erlotinib ( n = 35 ) versus 36 months ( 1944 ) for placebo ( n = 38 ) ; median progression - free survival was 35 months ( 1748 ) versus 27 months ( 1839 )  . 
patients with wild - type kras had median overall survival of 37 months ( 2842 ) for erlotinib ( n = 210 ) versus 34 months ( 2743 ) for placebo ( n = 180 ) ; median progression - free survival was 27 months ( 2229 ) for erlotinib and 26 months ( 2329 ) for placebo . 
the presence or absence of rst - cycle rash did not a ect the results ( data not shown )  . discussion first - line treatment with erlotinib did not improve overall survival in all unselected patients with advanced nsclc deemed unsuitable for chemotherapy treatment , who usually have a poor prognosis ( about 34 months median overall survival10 )  . 
additionally , in prespeci ed subgroup analyses , com pared with placebo , erlotinib signi cantly improved both overall survival and progression - free survival for patients who developed a rst - cycle rash ; median overall survival in this group increased by 21 months , from 41 months to 62 months . 
however , few patients assigned placebo developed rst - cycle rash ( 5% compared with 59% assigned erlotinib ) , and we identi ed no di erence in survival in patients assigned placebo who had rash compared with those who did not . 
few patients were lost to follow - up because survival is short and patients with lung cancer in the uk are seen regularly and remain under the care of a hospital physician . a limitation of our study was that the incidence of egfr mutation was only 7% and a quarter of them were uncommon mutations . 
most egfr mutation studies focus on so - called hot spot analysis , looking only for common alterations , short deletions in exon 19 , or the 858leuarg point mutation in exon 21 . 
our population were mostly elderly , white , present or exsmokers , and such groups might have a di erent mutation spectrum pro le , which further studies could examine . 
never theless , although analyses were based on only 28 patients , overall survival and progressionfree survival were improved in patients with an egfr mutation who were assigned erlotinib , consistent with ge tinib in patients with poor performance status.13 however , patients with tumours showing wild - type egfr also showed bene t when they developed an erlotinib - related rash . 
in the ipass study , 14 only 56% ( 683 ) of patients provided samples with egfr mutation data available in 36% ( 437 ) of the 1217 patients randomised . 
this proportion was much the same as in our trial where samples from 58% of patients had su cient dna for analysis . another limitation of our study is that we did routine ct scans at 3 and 6 months , whereas some other studies have used ct scans every 68 weeks , so our schedule might be deemed suboptimum for assessment of progression - free survival . 
also , we included patients of performance status 2 , for whom , on the basis of evidence reported in 2005 , 15 chemotherapy could improve survival , and a phase 2 study16 has shown that doublet chemotherapy has a better survival than single agent chemotherapy . 
however , when topical was designed , provision of chemotherapy to such patients was not routine practice because many studies with second and third generation chemotherapy had not shown survival bene t , and many of these patients had serious adverse events.17 , 18 a limitation of many of the more recent chemotherapy trials is that median age of patients of performance status 2 is 65 years or younger , median survival is much the same as for patients of performance status 01 , and many go on to receive second - line treatment , suggesting that they are a highly selected group . 
by contrast , in topical median age was 77 years , 90% of participants had several comorbidities , and less than 2% were given second - line treatment , which is indicative of the real - world scenario that lung cancer is a disease of elderly people with comorbidities , and many of these patients still continue to be treated with best supportive care worldwide , including palliative radiotherapy.19 when topical was designed some evidence already suggested that development of a rash during erlotinib vol 13 november 2012 1167 articles panel : research in context systematic review we did not do a systematic review of scienti c literature before designing the topical trial ( in 2002 ) , because at the time there were no other studies of rst - line egfr inhibitors in patients with advanced non - small - cell lung cancer ( nsclc ) who were elderly or had poor performance status . 
these patients are often excluded from rst - line chemotherapy trials . lung cancer is predominantly a disease of elderly people , and elderly patients with advanced nsclc deemed unsuitable for chemotherapy with poor performance status ( 2 and 3 ) or several comorbidities , or both , remain a major challenge . 
since topical , no phase 3 trials of rst - line monotherapy for this group have been reported . interpretation the ndings of topical and other trials58 show that erlotinib is an important treatment for patients with nsclc in various clinical settings , including as maintenance after rst - line chemotherapy , as second - line or third - line monotherapy in unselected patients with advanced nsclc , and in chemotherapy - naive patients with activating egfr mutations . 
however , unlike the topical patients , most of the patients in other studies had good performance status . the clinical implications of the topical trial are that patients who are deemed unsuitable for chemotherapy could be given erlotinib . 
those who have egfr mutation - positive tumours could receive continuous erlotinib ; whereas those who have wild - type tumours should discontinue erlotinib after about 28 days if they do not develop a rash because of the possibility of decreased survival . therapy could be associated with improved outcomes across several cancers including nsclc.20 with this knowledge , we developed a scoring system for rash as part of the topical protocol , and speci ed a preplanned subgroup analysis . 
furthermore , retrospective analyses of two phase 3 nsclc trials show a positive correlation between rash and treatment e ect on survival : the br.21 trial12 of erlotinib and the flex trial11 of cetuximab , an anti - egfr antibody , when added to rst - line chemotherapy . 
researchers have recorded much the same ndings in trials of pancreatic cancer , locally advanced head and neck cancer , and metastatic colorectal cancer.12 , 21 , 22 currently no clear biological explanations link erlotinib activity with rash , but rash probably represents greater uptake of the drug . 
smokers have a lower plasma concentration of erlotinib than do non - smokers.23 , 24 smokers also have a lower incidence of skin rash and have less clinical bene t from egfr inhibitors compared with non - smokers.23 , 24 this nding was con rmed in topical because present smokers in the erlotinib group were less likely to develop rash when compared with former smokers ( odds ratio 029 , 95% ci 018048 ) or never - smokers ( 020 , 006066 )  . 
 increased occurrence of skin rash has been identi ed in a phase 2 dose escalation study of erlotinib , although another study suggested that dose - escalation does not improve incidence or out come.25 , 26 alternatively , skin rash might be a surrogate marker of patients able to mount antitumour immune response . 
data increasingly suggest the importance of the host immune system in control of cancer cell growth after tyrosine - kinase inhibitor treatments.27 , 28 as reported with other tyrosinekinase inhibitors , erlotinib could enhance cytotoxic t - cell in ltration . drug uptake and cytotoxic t - cell in ltration could be linked , with increased uptake of drug causing increased egfr blockade and cell killing , resulting in improved host immune response . 
future studies could examine whether combining erlotinib and immunomodulatory agents can further fuel a more robust immunological response , increase the severity and incidence of skin rash , and potentially further improve durability of response , progression - free survival , and overall survival in this group of patients who are deemed not suitable for chemotherapy . a phase 2 study10 of ge tinib ( n = 201 ) compared with placebo ( instep ) in a group of patients with similar characteristics to those in topical showed no statistical di erence in survival with a hr of 084 ( 95% ci 062115 ) , but we identi ed a suggestion of a bene t among patients with high egfr gene copy number determined by uorescence in - situ hybridisation ( hr 044 , 95% ci 017112 )  . 
the dose of ge tinib might have been sub therapeutic in patients with wild - type egfr tumours , and this notion is supported by the lower than expected proportion who developed rash . 
 another phase 2 trial29 of only patients of performance status 2 ( n = 103 ) with a median age of less than 70 years compared erlotinib with carboplatin and paclitaxel , and showed that progression - free survival was better with chemotherapy than with erlotinib but progression - free survival did not di er between patients assigned erlotinib who developed rash compared with those who were assigned chemotherapy ( hr 094 , 95% ci 056159 )  . 
in topical , erlotinib seemed to have a greater e ect in some subgroups than in others ( eg , median overall survival was improved by 36 months for women with rash and 11 months for men with rash )  . 
previous studies have also reported sextreatment interactions with tyrosine - kinase inhibitors and other chemotherapies , where female patients bene ted more than men.30 diarrhoea , hair loss , and fatigue were expected adverse events associated with erlotinib , and their severity was usually mild to moderate . 
overall , occur rence and severity of adverse events in topical were much the same as those in the saturn and br.21 trials despite our population being predominantly elderly patients with poor performance status ( ecog 23 ) .5 , 6 taking erlotinib tablets at home should be more convenient to patients compared with treatments that require administration in hospital . 
we believe that patients with poor performance status and activating egfr mutation tumours should 1168 vol 13 november 2012 articles receive erlotinib or ge tinib , in line with the established evidence in patients with good per formance status , and supported by the nding that the small number of these patients in topical all developed rash.7 , 8 , 14 our data suggest patients with egfr wild - type or unknown egfr status tumours could start erlotinib but they should discontinue if they do not develop rash within 28 days , because these patients had no bene t in overall survival or progression - free survival , and in some subgroups overall survival could be reduced if erlotinib were taken continuously ( panel )  . 
the reasons for this nding are unknown but for some of our patients ( especially men and those with ecog performance status of 3 ) , the disease might be so advanced that any toxic treatment could accelerate deaths . 
researchers have recorded deleterious e ects of anti - egfr in some patients treated with erlotinib or cetuximab.31 , 32 a strategy of use of rst - cycle erlotinib - induced rash to select patients with poor performance status for continued treatment could substantially improve cost e ectiveness . 
second and third line erlotinib is marginally cost - e ective compared with best supportive care , therefore rst - line erlotinib could be more cost - e ective.33 egfr testing has now become standard of care to select patients who are egfr mutation - positive for treatment with tyrosine - kinase inhibitors . 
if erlotinib is to become a standard therapy for patients who have egfr wild - type tumours and are unsuitable for chemotherapy ( 93% in our trial ) it should be in a selected population . 
prospective studies are needed to increase our understanding of the biological mechanism linking rash and erlotinib bene t , including dose - escalation studies or studies of the relation between rash and tumour egfr copy number.34 further translational research with our biological samples might identify candidate markers for erlotinib - induced rash that can preselect patients for treatment with a marker measured at baseline , without having to treat all patients for 4 weeks , and then discontinue those without rash . contributors sml had the initial trial concept ; sml , cb , rr , and ah designed the trial ; sml , su , cl , sf , gs , em , pjw , mh , rl , rj , et , dc , gm , and sb were centre investigators , and recruited and treated patients ; sml , ik , yn , and ah were involved in trial conduct ; sml , ik , cb , and ah analysed and interpreted the data ; ik did the statistical analyses ; sml , cb , and ah wrote the report . 
all authors reviewed and approved the nal report . con icts of interest cl , et , dc , gm , and sml have received travel grants and honoraria from roche uk for serving on advisory boards . 
all other authors declare that they have no con icts of interest . acknowledgments the trial was funded by cancer research uk ( c1438 / a4147 ) , with an educational grant from roche for the translational studies , and support from the university college london and university college london hospital biomedical research centre ( who part - fund sml )  . 
the report highlighted that nearly 13 million cancer deaths are predicted for europe this year , and thatwith the exception of lung cancer in womenage - standardised death rates for most cancers decreased or remained unchanged since 2007 . 
about 127 million cancer cases and 76 million cancer deaths are estimated to have occurred in 2008 , with 56% of the cases and 64% of the deaths in developing countries . 
but can developing countries learn from the experiences of wealthier nations ? an increasing proportion of cancer deaths in developing countries are attributable to lifestyle changes such as smoking , diet , and physical inactivityin addition to the well documented disproportionately high burden of cancers related to infection . 
populations in countries with emerging economies will be increasingly exposed to the known risk factors associated with a uence , whereas those from poorer countries will continue to have high rates of infection , and limited or no access to treatment . 
 lack of basic infrastructure , rurality , con icts , and political instability mean many africans have no access to screening , early diagnosis , treatment , or palliative care . 
the incidence of cancer is increasing , but it remains a low public - health priority that has to compete for attention with other pressing and devastating health issues such as aids , malaria , and tuberculosis . in the a sustainable cancer control programme adapted to resource - constrained countries is crucial to tackle this predicted epidemic . 
without substantially increased prevention programmes , and a focus on early detection , the cancer burden in developing countries will make treatment una ordable long ter cancer management can be tailored and adapted to the resource level of the country or region . 
 but complacency would be unwarrantedafrica is likely at the early stages of a tobacco epidemic since smoking prevalence among boys is higher than in adults in some african countries . e orts to control cancer should be synergised with collaborative health initiatives , such as vaccination for liver and cervical cancers and public - health campaigns promoting physical activity and healthy diets . 
other initiatives include promoting cancer prevention information to over 3000 youths in lagos national stadium and o ering free hpv vaccines to 5000 girls in nigeria on world cancer day . 
aortic ( african organisation for research and training in africa ) has announced an initiative to improve cancer prevention , control , and care in africa through the integration and facilitation of evidencebased interventions . 
these examples are encouraging , but implementation will be the crucial factor . so can the battle against cancernotably absent from the millennium development goalsmove up the global health agenda ? this september , the un will hold a high - level summit to develop a global response to the growing threat of non - communicable diseases . 
 the lancet oncology vol 12 march 2011 articles association between endometriosis and risk of histological subtypes of ovarian cancer : a pooled analysis of casecontrol studies celeste leigh pearce , claire templeman , mary anne rossing , alice lee , aimee m near , penelope m webb , christina m nagle , jennifer a doherty , kara l cushing - haugen , kristine g wicklund , jenny chang - claude , rebecca hein , galina lurie , lynne r wilkens , michael e carney , marc t goodman , kirsten moysich , susanne k kjaer , estrid hogdall , allan jensen , ellen l goode , brooke l fridley , melissa c larson , joellen m schildkraut , rachel t palmieri , daniel w cramer , kathryn l terry , allison f vitonis , linda j titus , argyrios ziogas , wendy brewster , hoda anton - culver , alexandra gentry - maharaj , susan j ramus , a rebecca anderson , doerthe brueggmann , peter a fasching , simon a gayther , david g huntsman , usha menon , roberta b ness , malcolm c pike , harvey risch , anna h wu , andrew berchuck , on behalf of the ovarian cancer association consortium summary background endometriosis is a risk factor for epithelial ovarian cancer ; however , whether this risk extends to all invasive histological subtypes or borderline tumours is not clear . 
we undertook an international collaborative study to assess the association between endometriosis and histological subtypes of ovarian cancer . methods data from 13 ovarian cancer casecontrol studies , which were part of the ovarian cancer association consortium , were pooled and logistic regression analyses were undertaken to assess the association between selfreported endometriosis and risk of ovarian cancer . 
age , ethnic origin , study site , parity , and duration of oral contraceptive use were included in all analytical models . findings 13 226 controls and 7911 women with invasive ovarian cancer were included in this analysis . 
self - reported endometriosis was associated with a signi cantly increased risk of clear - cell ( 136 [ 202% ] of 674 cases vs 818 [ 62% ] of 13 226 controls , odds ratio 305 , 95% ci 243384 , p < 00001 ) , low - grade serous ( 31 [ 92% ] of 336 cases , 211 , 139320 , p < 00001 ) , and endometrioid invasive ovarian cancers ( 169 [ 139% ] of 1220 cases , 204 , 167248 , p < 00001 )  . 
no association was noted between endometriosis and risk of mucinous ( 31 [ 60% ] of 516 cases , 102 , 069150 , p = 093 ) or high - grade serous invasive ovarian cancer ( 261 [ 71% ] of 3659 cases , 113 , 097132 , p = 013 ) , or borderline tumours of either subtype ( serous 103 [ 90% ] of 1140 cases , 120 , 095152 , p = 012 , and mucinous 65 [ 85% ] of 767 cases , 112 , 084148 , p = 045 )  . interpretation clinicians should be aware of the increased risk of speci c subtypes of ovarian cancer in women with endometriosis . 
future e orts should focus on understanding the mechanisms that might lead to malignant transformation of endometriosis so as to help identify subsets of women at increased risk of ovarian cancer . funding ovarian cancer research fund , national institutes of health , california cancer research program , california department of health services , lon v smith foundation , european communitys seventh framework programme , german federal ministry of education and research of germany , programme of clinical biomedical research , german cancer research centre , eve appeal , oak foundation , uk national institute of health research , national health and medical research council of australia , us army medical research and materiel command , cancer council tasmania , cancer foundation of western australia , mermaid 1 , danish cancer society , and roswell park alliance foundation . introduction endometriosis is a common gynaecological disorder that is characterised by ectopic growth of endometrial glands and stroma . 
the estimated prevalence in the general population , based on women undergoing tubal ligation , is about 4% ; however , the disease is much more common in women with pelvic pain or infertility.1 the disease process typically involves the surface of the ovaries and pelvic peritoneum and is commonly thought to be due to re ux of endometrial tissue through the fallopian tubes during menstruation . 
to estimate the consistency and magnitude of the association between endometriosis and risk of the ve major histological subtypes of invasive epithelial ovarian cancer and borderline tumours with greater statistical power than has been possible previously , we undertook a pooled analysis of 13 casecontrol studies . methods patients and procedures all studies included in this pooled analysis had approval from ethics committees , and written informed consent was obtained from all study participants . 
study characteristics are reported in the appendix . we used primary data from all studies in the ocac at the time this analysis was initiated ; the study questionnaires included questions about endometriosis . 
one study was undertaken in australia , 9 three in europe , 2628 and nine in the usa.5 , 8 , 2936 the characteristics of the 13 studies are presented in table 1 . 
subsets of data from ve studies have been reported previously ( australian cancer study , australian ovarian cancer study [ aus ] , 9 diseases of the ovary and their evaluation study [ dov ] , 5 hawaii ovarian cancer study [ haw ] , 7 malignant ovarian cancer study [ mal ] , 7 and university of southern california , study of lifestyle and womens health [ usc ] 8 )  . 
we excluded one ocac study ( from poland37 ) from this analysis because the investigators thought that the endometriosis data were not reliable . in each study , information was provided about potential confounding variables that were previously noted to be related to ovarian cancer risk : age , ethnic origin , parity , breastfeeding , duration of oral contraceptive use , family history of ovarian cancer , weight , height , and history of tubal ligation . 
all data were cleaned and checked for internal consistency and clari cations were requested from the original investigators when needed . statistical analysis we included age , ethnic origin , oral contraceptive use , and parity in all models irrespective of their e ect on the association between endometriosis and ovarian cancer risk because these factors were judged to be potentially important confounders a priori . 
age was grouped into 5 year categories ( < 39 years , 4044 years , 4549 years , 5054 years , 5559 years , 6064 years , 6569 years , 7074 years , and 75 years ) ; ethnic origin was categorised as non - hispanic white , hispanic white , black , asian , or other . 
 number of births was categorised as zero , one , two , three , and four or more ; and oral contraceptive use was categorised as never , less than 2 years , 2499 years , 5999 years , and at least 10 years of use . 
 when a study had a cell with zero ( table 2 ) , which occurred only in the cells for exposed cases , we used the peto method to calculate the or.38 we did not use the peto method to calculate 95% cis because this method is known to be biased with non - balanced data , instead we used the exact con dence intervals.38 the studyspeci c ors were then used to calculate the summary ors . 
data for timing of endometriosis available . table 1 : description of studies included in the analysis los angeles county , ca university of southern california , study of population based in - person interview 19932005 also analysed low - grade and high - grade endometrioid tumours separately because they might behave di erently based on grade.39 in the analysis of borderline tumours , only serous and mucinous borderline cancers were analysed since clear - cell and endometrioid borderline tumours are rare , with insu cient numbers for a mean ingful analysis . 
a series of outcome variables for each comparison of histological subtype was created for this analysiseg , serous high - grade compared with serous low - grade . a sensitivity analysis was also done to investigate whether the association between ovarian cancer risk and endo metriosis di ered based on the timing of diagnosis of endometriosis relative to diagnosis date of ovarian cancer for cases and reference date for controls . 
for this analysis , we coded study participants as not having endometriosis if they were diagnosed with endometriosis within 3 years , 5 years , or 10 years of their ovarian cancer diagnosis or reference date for controls in the seven studies ( aus , 9 dov , 5 german ovarian cancer study [ ger ] , 26 hormones and ovarian cancer prediction study [ hop ] , 31 north carolina ovarian cancer study [ nco ] , 33 new england case - control study of ovarian cancer [ nec ] , 34 usc8 , 36 ) where this information was available . 
all p values were two - sided . role of the funding source no funding agency or sponsor had any role in the design and conduct of the study , collection , management , analysis , and interpretation of the data , and preparation , review , or approval of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results in the pooled analysis , 738 ( 93% ) of 7911 women with invasive epithelial ovarian cancer and 168 ( 88% ) of 1907 with borderline ovarian cancer reported a history of endometriosis ( table 2 )  . 
a history of endometriosis was reported by 136 ( 202% ) of 674 women with clear - cell , 169 ( 139% ) of 1220 with endometrioid , 31 ( 60% ) of 516 with mucinous , 261 ( 71% ) of 3659 with high - grade serous , and 31 ( 92% ) of 336 with low - grade serous subtypes of invasive ovarian cancer . 
 breastfeeding , weight , height , body - mass index , tubal vol 13 april 2012 articles 388 vol 13 april 2012 articles crude strati ed only strati ed and adjusted or ( 95% ci ) p value or ( 95% ci ) * p value or ( 95% ci ) p value invasive 149 ( 134165 ) < 00001 153 ( 137170 ) < 00001 146 ( 131163 ) < 00001 clear - cell 373 ( 304458 ) < 00001 344 ( 278427 ) < 00001 305 ( 243384 ) < 00001 endometrioid 232 ( 194278 ) < 00001 220 ( 182266 ) < 00001 204 ( 167248 ) < 00001 mucinous 109 ( 076158 ) 104 ( 071151 ) 086 102 ( 069150 ) 111 ( 096129 ) 116 ( 100135 ) 0056 113 ( 097132 ) 202 ( 138297 ) < 00001 222 ( 148331 ) < 00001 211 ( 139320 ) < 00001 high - grade serous low - grade serous borderline 126 ( 105150 ) 119 ( 099143 ) 0062 112 ( 093135 ) mucinous 127 ( 097167 ) 119 ( 090157 ) 023 112 ( 084148 ) serous 131 ( 105163 ) 128 ( 102161 ) 0034 120 ( 095152 ) or = odds ratio . 
 * strati ed by age ( 5 year categories ) , ethnic origin ( non - hispanic white , hispanic white , black , asian , and other )  . 
strati ed by age ( 5 year categories ) , ethnic origin ( non - hispanic white , hispanic white , black , asian , and other ) , and adjusted for duration of oral contraceptive use ( never , < 2 years , 2499 years , 5999 years , 10 years ) , and parity ( 0 , 1 , 2 , 3 , 4 children )  . table 3 : association between history of endometriosis and the histological subtypes of ovarian cancer 063 016 0012 0078 0015 093 013 024 045 012 period between endometriosis diagnosis and ovarian cancer diagnosis for cases and reference date for controls was increased to 5 years or 10 years ( table 4 )  . discussion our ndings suggest that the association of a history of endometriosis with increased risk of ovarian cancer is only apparent for invasive low - grade serous , clear - cell , and endometrioid subtypes , thus providing information about the pathogenesis of these subtypes relative to other subtypes of invasive epithelial ovarian cancer and further emphasising the di erences between low - grade and high - grade serous cancers . the relation between endometriosis and serous ovarian cancer has generally been null ; however , this subtype has not been analysed according to grade in previous studies.5 , 9 , 14 by contrast , we note an association between endometriosis and increased risk of low - grade serous ovarian cancers . 
results of recent molecular genetic studies have suggested that low - grade and highgrade serous ovarian cancers are distincthigh - grade cases are characterised by tp53 mutations , whereas typically have kras or braf low - grade cases mutations.18 , 40 likewise , lends increasing evidence support to the hypothesis that a signi cant proportion from borderline precursors , whereas this is not the case for high - grade serous tumours.40 thus , the pathogenesis of low - grade and high - grade serous ovarian cancers might di er . 
although concomitant endometriosis is often noted in endo metrioid and clear - cell ovarian cancers , some endosalpingiosis ( benign glandular proliferations ) , which is thought to be of tubal orig because endosalpingiosis is asymptomatic , its presence can only be detected patho logically and its incidence cannot be low - grade serous cancers might arise tumours can develop low - grade serous ligation , and family history of ovarian cancer did not confound the association between endometriosis and ovarian cancer - risk ( coe cient changed by < 10% ) and were not considered further in the analysis ( data not shown )  . no association was noted between a history of endometriosis and borderline ovarian cancer ( both serous and mucinous subtypes ; table 3 )  . 
by contrast , a history of endometriosis was associated with an increased risk of invasive epithelial ovarian cancer , after taking study site , age , ethnic origin , oral contraceptive use , and parity into account ( table 3 )  . 
this result was consistently noted for the 13 studies ( gure 1 ) , although ger , which had very few exposed cases , had a summary estimate of less than one . association of endometriosis and risk di ered for the histological subtypes of invasive epithelial ovarian cancer . 
women who reported a history of endometriosis were more likely to develop invasive low - grade serous , endometrioid , and clear - cell ovarian cancer ( table 3 ; gure 2 ) relative to women without such a history . 
 a history of endometriosis was not associated with invasive mucinous ovarian cancer ( table 3 ; gure 2 ) or invasive serous high - grade ovarian cancer ( table 3 ; gure 2 )  . 
no signi cant heterogeneity of e ects was noted for any of the invasive histological subtypes ( gure 2 )  . casecase analyses showed that a history of endometriosis was more commonly reported by women with invasive clear - cell , serous low - grade , and endometrioid ovarian cancers than by women with invasive serous highgrade or invasive mucinous ovarian cancers ( all comparisons p < 002 )  . 
endometriosis was more strongly linked with invasive clear - cell ovarian cancer than with the invasive endometrioid subtype ( or 164 , 95% ci 121222 , p = 0001 )  . 
also , endometriosis was more strongly linked with invasive low - grade serous ovarian cancer than with its high - grade counterpart ( 194 , 121311 , p = 001 )  . additional analyses of histological subtypes to assess the role of stage and grade ( for clear - cell , endometrioid , and mucinous ovarian cancers ) in the endometriosis invasive epithelial ovarian cancer relation showed no di erences ( data not shown )  . we analysed whether the e ect was robust to exclusion of women who were diagnosed with endometriosis within close proximity ( calendar time ) to diagnosis of their ovarian cancer . 
information about the timing of the diagnosis of endometriosis relative to that of invasive epithelial ovarian cancer was available in seven studies ( 5674 cases , 8968 controls )  . 
when women with endometriosis who were diagnosed within 3 years of their ovarian cancer diagnosis for cases and reference date for controls were coded as not having endometriosis , the results were slightly attenuated versus those without restrictions on the timing of diagnosis of endometriosis relative to diagnosis of ovarian cancer , but remained strong ( table 4 )  . 
aus = australian cancer study , australian ovarian cancer study.9 ger = german ovarian cancer study.26 mal = malignant ovarian cancer study.27 uko = united kingdom ovarian cancer population study.28 con = connecticut ovary study.29 dov = diseases of the ovary and their evaluation study.5 haw = hawaii ovarian cancer study.30 hop = hormones and ovarian cancer prediction study.31 may = mayo clinic ovarian cancer study.32 nco = north carolina ovarian cancer study.33 nec = new england case - control study of ovarian cancer.34 uci = university of california , irvine ovarian cancer study.35 usc = university of southern california , study of lifestyle and womens health.8 , 36 or = odds ratio . endometriosis the processes ascertained in casecontrol studies . 
our ndings of an association with endometriosis suggest that we might have identi ed a second precursor lesion for low - grade serous ovarian cancer in addition to borderline serous precursors . although the risk associated with a history of endometriosis was increased for both invasive clear - cell and endometrioid ovarian cancers , casecase comparisons suggested a stronger association for endometriosis with clear - cell cancer than with the endometrioid subtype . 
the pathological slides from the cases in this study have not undergone a systematic rereview and thus some misclassi cation is likely to be present.17 in a systematic review of 176 endometrioid cases , 50 ( 28% ) were reclassi ed as high - grade serous.17 assuming our endometrioid cases also included 28% high - grade serous cases and assuming an or of 1 for high - grade serous disease and endometriosis , the association we noted between endometriosis and endometrioid ovarian cancers might have been attenuated from an or of 250 to 204 . 
additionally , misclassi cation of clear - cell tumours as low - grade invasive serous ovarian cancer might , partly , account for the association noted for this subtype with a history of endometriosis . 
sangoi and colleagues41 reported 13 cases of clear - cell cancer as being misclassi ed as serous borderline tumours ( ten cases ) and low - grade serous ( three cases ) ; 41 we did not note an association between endometriosis and serous borderline tumours and misclassi cation is unlikely to account for the magnitude of e ect with low - grade serous cancers . ness42 reviewed the evidence for endometriosis as a precursor lesion for ovarian cancer and proposed both in ammatory and hormonal pathways for this process . 
many of the same genes , such as catenin and pten , have been shown to be mutated in both endometrial cancers and endometrioid ovarian cancers , 39 suggesting a shared molecular pathogenesis . 
however , clear - cell ovarian tumours do not express oestrogen or progesterone receptors and therefore endometriosis that can transform into clear - cell ovarian cancer could become hormone independent during the transformation process.18 molecular similarities between synchronous endometriosis and ovarian cancer at the time of diagnosis have been described.42 mutations in the arid1a gene have been noted in clear - cell tumours and contiguous atypical endometriosis , but not in distant endometriotic lesions.43 however , to our knowledge , no studies have been reported in which endometriotic lesions excised years before the development of cancer have been compared with tissue obtained at the time of cancer diagnosis . 
although we have reported strong associations between endometriosis and risk of low - grade serous , clear - cell , and endometrioid ovarian cancers , most women with endometriosis do not develop ovarian cancer . 
aus = australian cancer study , australian ovarian cancer study.9 ger = german ovarian cancer study.26 mal = malignant ovarian cancer study.27 uko = united kingdom ovarian cancer population study.28 con = connecticut ovary study.29 dov = diseases of the ovary and their evaluation study.5 haw = hawaii ovarian cancer study.30 hop = hormones and ovarian cancer prediction study.31 may = mayo clinic ovarian cancer study.32 nco = north carolina ovarian cancer study.33 nec = new england case - control study of ovarian cancer.34 uci = university of california , irvine ovarian cancer study.35 usc = university of southern california , study of lifestyle and womens health.8 , 36 or = odds ratio . vol 13 april 2012 articles clear - cell endometrioid low - grade serous or ( 95% ci ) * p value or ( 95% ci ) * p value or ( 95% ci ) * p value exclusions none 3 years 5 years 307 ( 244386 ) < 00001 205 ( 168249 ) < 00001 231 ( 150355 ) < 00001 278 ( 206374 ) < 00001 170 ( 130224 ) < 00001 201 ( 120335 ) 0008 251 ( 184342 ) < 00001 160 ( 121213 ) 0001 197 ( 117334 ) 001 003 10 years 238 ( 171333 ) < 00001 149 ( 109203 ) 001 188 ( 106332 ) data reported for the seven studies with information about timing of diagnosis ( aus , dov , ger , hop , nco , nec , and usc )  . 
aus = australian cancer study , australian ovarian cancer study.9 dov = diseases of the ovary and their evaluation study.5 ger = german ovarian cancer study.26 hop = hormones and ovarian cancer prediction study.31 nco = north carolina ovarian cancer study.33 nec = new england case - control study of ovarian cancer.34 usc = university of southern california , study of lifestyle and womens health.8 , 36 * strati ed according to age ( 5 year categories ) , ethnic origin ( non - hispanic white , hispanic white , black , asian , and other ) , and adjusted for duration of oral contraceptive use ( never , < 2 years , 2499 years , 5999 years , and 10 years ) , and parity ( 0 , 1 , 2 , 3 , and 4 children )  . table 4 : sensitivity analysis for the association between endometriosis and risk of invasive ovarian cancer based on timing of diagnosis between the two diseases panel : research in context systematic review to assess the association between ovarian cancer - risk and endometriosis , we searched pubmed for english language papers published during 19732011 . 
additional reports identi ed from the articles found during the initial search were reviewed for relevance . interpretation based on our review of the literature , an association was noted between invasive ovarian cancer and endometriosis . 
we have reported precise estimates for these associations and have identi ed an association with low - grade serous ovarian cancer that , to our knowledge , was not reported previously . 
on the basis of evidence , including the results of molecular studies , endometriosis should be thought of as a precursor lesion for clear - cell and endometrioid ovarian cancers , whereas the type of association with low - grade serous ovarian cancers requires further follow - up . clinicians need to be aware of the increased risk of speci c ovarian cancer subtypes in women with endometriosis . 
the hope is that we will develop a risk strati cation model that combines genetic and epidemiological risk to better stratify women into high - risk , intermediate - risk , and low - risk categories , allowing better individualisation of prevention and early detection approaches such as risk - reduction surgery and screening . 
a better understanding of the cause of the various disease subsets is necessary if we hope to develop better prevention , screening , and treatment approaches for this heterogeneous disease . relevant population and potentially alter the treatment of their endometriosis . 
in this respect , rossing and colleagues5 reported increased risk of endometrioid and clear - cell ovarian tumours associated with endometriosis was reduced among women who that the underwent ovarian surgery after the endometriosis was diagnosed . the results in this report are from casecontrol studies in which the history of endometriosis was based on self reports . 
the frequency of endometriosis reported in the control participants in studies from australia and the usa was much higher than it was in those from europe ( 57127% vs 1042% ; table 2 )  . 
in two of three european studies ( ger and uko ) , data were collected by use of a self - completed questionnaire , and in the third european study ( mal ) a trained study nurse collected the data , which suggests that the method of data collection did not contribute to the di erence . 
endometriosis frequency in cases from the european studies was also low and overall the results of these studies did not contribute substantively to the weighted summary or . recall bias is a major concern in casecontrol studies , particularly with a self - reported exposure like endometriosis . 
however , there is little reason to believe that this over - reporting would be non - random with respect to histological subtype of ovarian cancer and therefore it is unlikely to be an explanation for these results . 
also , results from registrybased studies in sweden and denmark where endometriosis data were obtained from hospital discharge databases were similar to our results in invasive cases10 , 14 and by histological subtype.14 in this pooled analysis with primary data from 13 studies , a self - reported history of endometriosis was associated with a signi cantly increased risk of invasive low - grade serous , clear - cell , and endometrioid ovarian cancers . 
our results were consistent for studies from various locations in australia , europe , and the usa that were undertaken in the 1990s and 2000s and sensitivity analyses suggest that risk is increased even among women whose endo metriosis was diagnosed many years before their ovarian cancer ( table 4 )  . 
although cases might have over - reported a history of endometriosis compared with controls , any such over - reporting is unlikely to result in ndings of increased risk that is restricted to speci c histological subtypes . 
further , our epidemiological ndings are consistent with the existing laboratory evidence of the 392 vol 13 april 2012 articles co - occurrence of endometriosis with endometrioid and clear - cell ovarian tumours and molecular and genetic similarities between these disorders . 
future research should focus on identi cation of factors that are associated with malignant transformation of endometriosis and subsequent risk of low - grade serous , clear - cell , and endometrioid ovarian cancers to identify women for whom more de nitive endometriosis treatment and ovarian cancer surveillance would be appropriate ( panel )  . contributors all authors contributed to the design and execution of this work and to the preparation of this report . 
approval of the nal report was obtained from all authors . con icts of interest we declare that we have no con icts of interest . acknowledgments this work was supported with donations by the family and friends of kathryn sladek smith to the ovarian cancer research fund . 
it was also supported by the national institutes of health ( r01 ca136891 , ca14089 , ca17054 , ca61132 , n01 pc67010 , and r03 ca113148 [ usc ] , r01 ca112523 , and r01 ca87538 [ dov ] , r01 ca58598 , n01 cn67001 , and n01 pc35137 [ haw ] , 5r01 ca074850 [ con ] , r01 ca76016 [ nco ] , ca58860 , ca92044 , and psa 042205 [ uci ] , r01 ca54419 and p50 ca105009 [ nec ] , r01 ca61107 [ mal ] , r01 ca95023 and r01 ca126841 [ hop ] , and r01 ca122443 and p50 ca136393 [ may ] ) ; california cancer research program ( 0001389v20170 and 2110200 [ usc ] ) ; california department of health services ( subcontract 050e8709 [ usc ] ) ; lon v smith foundation ( lvs 39420 [ uci ] ) ; european communitys seventh framework programme ( health - f2 - 2009 - 223175 [ ger ] ) ; german federal ministry of education and research of germany , programme of clinical biomedical research ( 01gb9401 [ ger ] ) ; german cancer research centre ( ger ) ; eve appeal ( uko ) ; oak foundation ( uko ) ; womens health theme of the uk national institute of health research supported university college london hospital / university college london comprehensive biomedical research centre ( uko ) ; national health and medical research council of australia ( 199600 [ aus ] ) ; us army medical research and materiel command ( damd 170110729 and w81xwh0610220 [ aus ] , w81xwh1010280 [ nec ] , and damd17 - 02 - 1 - 0669 [ hop ] ) ; cancer council tasmania ( aus ) ; cancer foundation of western australia ( aus ) ; mermaid 1 ( mal ) ; danish cancer society ( mal ) ; and roswell park alliance foundation ( hop )  . 
we assume full responsibility for the analyses and interpretation of these data . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper to the lancet go to thelancet / to submit a paper to the lancet oncology go to ees.elsevier.com / thelancetoncology / recommendations in light of the new data presented by raaijmakers and colleagues.3 piet dirix * , sandra nuyts department of radiation oncology , university hospitals leuven , leuven , belgium , piet.dirix@uzleuven.be the authors declared no con icts of interest . raaijmakers cp , roesink jm , dijkema t , houweling ac , terhaard ch . 
first results of a phase iii multicenter randomized controlled trial of intensity modulated ( imrt ) versus conventional radiotherapy ( rt ) in head and neck cancer ( parsport : isrctn48243537 ; cruk / 03 / 005 )  . 
proc am soc clin oncol 2009 ; 27 : abstr lba6006 . call for papersoncology and haematology the lancet and the lancet oncology are announcing plans for issues of each journal to be devoted to speci c topics in oncology and also to haematology . 
the former will be timed to coincide with the european society of medical oncology ( esmo ) congress in milan , italy ( oct 812 , 2010 ) , and the latter with the american society of hematology ( ash ) annual meeting in orlando , fl , usa ( dec 47 , 2010 )  . 
we would like to invite submissions of high - quality original research about cancers of the breast , lung , prostate , and gastrointestinal tract , or on any topic in haematology or haematological oncology . 
accepted papers will be published in either the lancet or the lancet oncology via fast - track peer review to coincide with either the esmo or ash annual meetings , as appropriate . 
 submissions to coincide with the esmo annual meeting must be received by june 25 , 2010 , and those for the ash annual meeting by oct 1 , 2010 , via either the lancet or the lancet oncologys online submission systems . 
please state in your covering letter that the submission is in response to this call for papers . if your work is being presented at either meeting and falls under an embargo policy , please tell us the date and time of the presentation , and whether the study is to be presented orally or in a poster . 
if your paper is accepted , online publication can be scheduled to coincide with the presentation and comply with any press embargo . jane godsland , zo mullan , richard turner , david collingridge the lancet ( jg , zm , and rt ) and the lancet oncology ( dc ) , 32 jamestown road , london nw1 7by , uk errata relling mv , altman rb , goetz mp , evans we . 
clinical implementation of pharmacogenomics : overcoming genetic exceptionalislancet oncol 2010 ; 11 : 50709the acknowledgment in this comment ( published online first on april 21 , 2010 ) should have read we thank colleagues in nihs pharmacogenomics research network . 
in the second paragraph , the last sentence was misspelt and should have read despite evidence linking pharmacogenomic variation with drug exposure , toxic e ects , and e cacy , many clinicians , regulators , and payors hold pharmacogenetic evidence to excessively high standards . 
lancet oncol 2010 ; 11 : 42938in this article , the acknowledgments statement should also have included : the uk medical research council funded the original all97 / 99 trial and supported the childhood leukaemia working party . 
lancet oncol 2007 ; 8 : 31722in this article , the equation for acpgbi in panel 2 should read loge [ r / ( 1r ) ] = ( 4859 + total score )  . 
additionally , in table 3 , 158 was added in error next to the heading clinicopathological staging . 516 vol 11 june 2010 adjuvant capecitabine in combination with docetaxel and cyclophosphamide plus epirubicin for breast cancer : an open - label , randomised controlled trial heikki joensuu , pirkko - liisa kellokumpu - lehtinen , riikka huovinen , arja jukkola - vuorinen , minna tanner , raija asola , riitta kokko , johan ahlgren , pivi auvinen , akseli hemminki , outi paija , leena helle , lauri nuortio , kenneth villman , greger nilsson , sirpa - liisa lahtela , kaisa lehti , marjo pajunen , paula poikonen , paul nyandoto , vesa kataja , petri bono , mika leinonen , henrik lindman , on behalf of the finxx study investigators summary background standard adjuvant chemotherapy regimens for patients with moderate - to - high - risk early breast cancer typically contain a taxane , an anthracycline , and cyclophosphamide . 
we aimed to investigate whether integration of capecitabine into such a regimen enhances outcome . methods in this open - label trial , we randomly assigned ( centrally by computer ; strati ed by node status , her2 status , and centre ) 1500 women with axillary node - positive or high - risk node - negative breast cancer to either three cycles of capecitabine and docetaxel followed by three cycles of cyclophosphamide , epirubicin , and capecitabine ( capecitabine group , n = 753 ) , or to three cycles of docetaxel followed by three cycles of cyclophosphamide , epirubicin , and uorouracil ( control group , n = 747 )  . 
after a median follow - up of 35 months ( iqr 255436 ) , recurrence - free survival at 3 years was better with the capecitabine regimen than with control ( 93% vs 89% ; hazard ratio 066 , 95% ci 047094 ; p = 0020 )  . 
more patients discontinued planned treatment in the capecitabine group than in the control group ( 178 / 744 [ 24% ] vs 23 / 741 [ 3% ] )  . 
 four patients in the capecitabine group and two in the control group died from potentially treatment - related causes . interpretation the capecitabine - containing chemotherapy regimen reduced breast cancer recurrence compared with a control schedule of standard agents . 
 introduction adjuvant chemotherapy consisting of an alkylating agent , an anthracycline , and a taxane is typically administered for early breast cancer , although the regimens used can vary considerably.13 results from a few large randomised trials and a meta - analysis suggest that addition of a taxane to adjuvant regimens containing an anthracycline improves disease - free and overall survival.46 despite such advances in chemotherapy , many women diagnosed with early breast cancer still eventually succumb to the disease . 
main exclusion criteria were : presence of distant metastases ; node - negative mucinous , papillary , medullary , or tubular disease ; clinically signi cant cardiac disease ; and previous neoadjuvant chemotherapy . 
study safety was monitored by an independent data safety monitoring committee . 1500 enrolled and underwent randomisation for the trial protocol see 753 assigned to capecitabine group 747 assigned to control group 1 withdrew consent 1 had distant metastases 1 withdrew consent 1 had distant metastases 751 included in intention - to - treat population 744 included in safety population ( received 745 included in intention - to - treat population 741 included in safety population ( received study treatment ) 566 completed study treatment 1 had cancer recurrence 169 had adverse events 4 withdrew consent 4 discontinued for other reasons study treatment ) 718 completed study treatment 3 had cancer recurrence 19 had adverse events 0 withdrew consent 1 discontinued for other reasons 54 had cancer recurrence or died 80 had cancer recurrence or died 27 died 18 died from breast cancer 41 died 35 died from breast cancer figure 1 : trial pro le 1146 the study generated randomisation and masking we randomly assigned patients ( centrally and with computer - assisted masking ) , in a 1 : 1 ratio , to receive either a capecitabine - containing chemotherapy regimen ( capecitabine group ) or a control schedule . 
we did randomisation with permutated blocks : block size ( two , four , or six ) varied at rando we strati ed women at random allocation according to the number of axillary lymph nodes that contained cancer ( 3 vs > 3 ) , her2 status ( negative vs positive ; ascertained by either immunohistochemistry or in - situ hybridisation ) , and centre . 
a trained study nurse communicated the randomisation result to study sites by fax . procedures patients allocated to the capecitabine group received capecitabine ( 900 mg / m twice a day , days 115 ) plus docetaxel ( 60 mg / m as a 1 - h intravenous infusion on day 1 of every 3 - week cycle ) , followed by cyclophosphamide ( 600 mg / m on day 1 ) , epirubicin ( 75 mg / m on day 1 ) , and capecitabine ( 900 mg / m twice a day , days 115 , every 3 weeks )  . 
those assigned control received docetaxel ( 80 mg / m as a 1 - h intravenous infusion on day 1 of every 3 - week cycle ) followed by cyclophosphamide ( 600 mg / m ) , epirubicin ( 75 mg / m ) , and uorouracil ( 600 mg / m ) , all administered on day 1 of every 3 - week cycle . 
in the capecitabine group , the rst capecitabine dose of every cycle was given in the evening of day 1 and the last dose was administered on the morning of day 15 , followed by a 7 - day rest period . 
if they developed a second grade 2 event , or their rst grade 3 event , we terminology criteria vol 10 december 2009 articles stopped chemotherapy and , after resolution to grade 01 , resumed it at 80% of the starting dose . 
 when scheduled treatment was discontinued for toxic e ects , we replaced agents as follows : capecitabine and docetaxel by cyclophosphamide , epirubicin , and capecitabine , or cyclophosphamide , epirubicin , and uorouracil ; single - agent docetaxel by cyclophosphamide , epi rubicin , and uorouracil ; and cyclo phosphamide , epirubicin , and capecitabine by cyclophosphamide , epirubicin , and uorouracil , or cyclophosphamide and epirubic we regarded staging examinations ( chest ct or radiography ; bone scan ; and abdominal ct , mri , or ultrasound ) as mandatory at screening for patients with four or more positive axillary nodes , 15 , 16 but these procedures were undertaken at the discretion of the investigator for all other patients . 
we scheduled follow - up of study participants for a minimum of 5 years after randomisation . the primary endpoint was recurrence - free survival , de ned as the time between randomisation and date of diagnosis of invasive breast cancer recurrence , or death if the patient died before cancer recurrence . 
based on this assumption , a total of 205 events and 1500 patients were needed to achieve 80% power , assuming a 3% annual dropout rate , when = 0028 ( two - sided )  . 
to maintain a signi cance level of 5% , we set the signi cance level in interim and nal analyses at 0028.17 the interim analysis had 80% power to detect an improvement from 890% to 935% ( hr 058 ) after median follow - up of 3 years in 1500 patients ( = 0028 , two - sided testing ) and when about 120 recurrences had happened . 
suicide and depression ; suicide and intoxication ; unknown ; unknown ( breast cancer unlikely ) ; pulmonary embolus ; septicaemia , colitis , and multiorgan failure ; acute myocardial infarction ; alcohol intoxication ; cardiac and pulmonary failure . 
pulmonary embolus ( n = 2 ) ; septicaemia ; septic shock ; amyotrophic lateral sclerosis ; subdural haemorrhage . table 2 : breast cancer recurrence and survival in the modi ed intention - to - treat population a recurrence - free survival control capecitabine p = 0020 ( log rank ) number at risk control capecitabine b overall survival articles we analysed frequency tables with fishers exact test or the test , and we compared age and weight distributions with the t test . 
to compare survival between groups , we used the kaplan - meier life - table method and an unadjusted cox proportional - hazards model ; we implemented the log - rank test to con rm the robustness of the analysis . 
 results between jan 27 , 2004 , and may 29 , 2007 , 1500 patients were recruited from 15 finnish centres ( n = 1199 ) and ve swedish centres ( n = 301 )  . 
four women were excluded from the modi ed intention - to - treat population ( two withdrew informed consent before they received study treatments , two had overt distant metastases at the time of study entry ; gure 1 )  . 
respectively , 56 ( 7% ) and 50 ( 7% ) women received single - agent trastuzumab after discontinuation of chemotherapy for up to 12 months , 24 ( 3% ) and 21 ( 3% ) received trastuzumab concomitantly with docetaxel only , and 16 ( 2% ) and 12 ( 2% ) received plus trastuzumab single - agent trastuzumab for up to 12 months after chemotherapy . 
tamoxifen , anastrozole , and other hormonal treatments were administered , respectively , to 325 ( 43% ) , 316 ( 42% ) , and 29 ( 4% ) patients assigned to the capecitabine group , and to 287 ( 38% ) , 328 ( 44% ) , and 27 ( 4% ) women allocated to the control group . concomitantly with docetaxel at the time of data lock ( aug 31 , 2008 ) , median follow - up was 35 months ( iqr 255436 )  . 
134 events ( deaths , distant or local relapses ) had happened , 54 ( 7% ) in the capecitabine group and 80 ( 11% ) in the control group , which triggered the interim analysis . 
the hazard ratio for the capecitabinerecurrence - free survival favoured number at risk control capecitabine p = 0089 ( log rank ) years after randomisation figure 2 : kaplan - meier estimates of 3 - year recurrence - free and overall survival in the modi ed intention - to - treat population 1148 vol 10 december 2009 articles 070 ( 048101 ) 047 ( 018125 ) 081 ( 051129 ) 052 ( 031088 ) 060 ( 037096 ) 077 ( 046127 ) 156 ( 078314 ) 049 ( 033075 ) capecitabine group control group patients events patients events hazard ratio ( log scale ) hazard ratio ( 95% ci ) who performance status positive axillary nodes oestrogen receptor status 03 positive negative her2 status positive negative 661 547 204 580 171 146 605 662 537 208 563 182 139 606 capecitabine better control better figure 3 : forest plot of exploratory subgroup analyses for recurrence - free survival containing regimen ( 066 , 95% ci 047094 ; p = 0020 ; table 2 ; gure 2 )  . 
in the capecitabine group , three women developed invasive contralateral breast cancer and six had other cancers , compared with two and eight patients , respectively , in the control group . 
disease - free survival ( which includes invasive contralateral breast cancers and second cancers ) was longer in the capecitabine group than in the control group ( 068 , 049094 ; p = 0020 )  . 
when patients treated with trastuzumab were excluded from the main analysis , the hazard ratio for recurrence - free survival still favoured the capecitabine - containing regimen ( 064 , 044091 ; p = 0014 )  . in exploratory subgroup analyses , recurrence - free survival was better in the capecitabine group than in the control group , with the exception of patients with her2 - positive disease ( gure 3 )  . 
in this analysis , the interaction between treatment and her2 status was signi cant ( p = 00049 ) , whereas interactions between treatment and the other subgroups shown in gure 3 were not ( p > 010 )  . 
patients who received capecitabine had more occurrences of grade 3 or 4 hand - foot syndrome , diarrhoea , nail changes , and stomatitis than did those in the control group , whereas neutropenia , febrile neutropenia , infection with neutropenia , amenorrhoea , and myalgia were more frequent in the control group ( table 3 )  . 
four patients in the capecitabine group died during chemotherapy from possibly treatment - related causes ( septic colitis ; suicide ; myocardial infarction ; unknown cause [ suspected cardiac arrhythmia ] ) and two died in the control group ( pulmonary arterial embolism ; septicaemia )  . all six planned cycles of chemotherapy were administered to 566 ( 75% ) individuals assigned the compared with capecitabine - containing 718 ( 96% ) allocated control . 
 table 3 : adverse events in safety population treatment was most frequent in the capecitabine group ( 178 [ 24% ] vs 23 [ 3% ] assigned control ; p < 00001 )  . 
of those allocated to the capecitabine group , 98 ( 13% ) discontinued during docetaxel and capecitabine cycles and a further 80 ( 11% ) during cyclophosphamide , vol 10 december 2009 1149 articles epirubicin , and capecitabine cycles . 
 58 ( 8% ) and 139 ( 19% ) patients assigned to the capecitabine and control groups , respectively , had the docetaxel dose reduced because of toxic e ects . 
including replaced cycles , most patients ( 1461 [ 98% ] ) received a total of six cycles . discussion our ndings showed enhanced recurrence - free survival for patients who received a regimen containing capecitabine in addition to docetaxel , epirubicin , and cyclophosphamide compared with women who received docetaxel , epirubicin , cyclophosphamide , and uorouracil . 
single - agent capecitabine has been compared with combination chemotherapy in the adjuvant treatment of elderly patients with breast cancer , 18 but to our knowledge , finxx is the rst adjuvant trial to report e cacy of capecitabine in combination with other agents for treatment of early breast cancer . our results suggest that integration of capecitabine upfront with potentially synergistic chemotherapeutic agents and into several cycles might be an e ective treatment strategy . 
this hypothesis is supported by data of randomised studies undertaken in the neoadjuvant setting.19 , 20 inclusion of capecitabine in the taxane and anthracycline - containing parts regimen distinguishes finxx from other trials investigating incorporation of capecitabine into adjuvant regimens . 
 findings of a randomised trial in the neoadjuvant setting indicated a 20% pathological complete response rate with and capecitabine compared with 13% in patients receiving uorouracil , epirubicin , and cyclophosphamide.21 cyclophosphamide , epirubicin , the the enhanced e cacy we recorded in the capecitabine arm was gained at the cost of increased diarrhoea and hand - foot syndrome , although febrile neutropenia was less frequent than with the control regimen , which is probably attributable to the reduced docetaxel dose . 
cardiotoxicity is a known e ect of the uoropyrimidine class of chemotherapeutic agents , and individuals receiving uoropyrimidines need to be monitored for symptoms and signs of these cardiac e ects , although cardiotoxicity might be typical with capecitabine than with infused uorouracil.22 in our study , most patients who interrupted capecitabine administration could continue treatment with other study agents and complete six cycles of chemotherapy . 
 less the control arm in our study represents a regimen frequently used in finland and sweden , which is not dissimilar to the types of regimen administered in many other countries.8 , 23 , 24 docetaxel 80 mg / m is a lower dose than the 100 mg / m2 regarded as standard in some regions . 
we selected the dose of 80 mg / m for two reasons : ( 1 ) on the basis of toxic e ects recorded with docetaxel 100 mg / m in the finher trial , leading to protocol modi cation ; 25 and ( 2 ) because no di erence in time - to - progression or survival was recorded between starting doses of 75 mg / m and 100 mg / m in the intention - to - treat population of a randomised trial of docetaxel as second - line therapy for advanced breast cancer.26 adjuvant docetaxel administered at either 80 mg / m or 100 mg / m at 3 - week intervals before three and cyclophosphamide for early breast cancer might show similar survival.27 the docetaxel dose of 60 mg / m administered in the capecitabine group is fairly low , but this amount was e ective in combination with other agents and rarely needed to be reduced . 
 of uorouracil , epirubicin , cycles our results suggest that e cacy is maintained when capecitabine is given at a dose of 900 mg / m instead of 1250 mg / m twice a day in combination with docetaxel , 12 and these data are consistent with analyses of capecitabine dose - reduction in metastatic disease.28 the hypothesis that an even lower capecitabine dose could be appropriate is being tested in an ongoing us oncology group trial , in which capecitabine is given at a dose of 825 mg / m concomitantly with docetaxel . 
 retrospective analysis of one study suggests that docetaxel plus capecitabine might be more e ective than docetaxel alone for treatment of oestrogen receptorpositive advanced breast cancer in particular , but this idea needs con rmation.29 chemotherapy - induced amenorrhoea is unlikely to account for the high e ciency of capecitabine combinations , because persistent amenorrhoea was less frequent in women allocated to the capecitabine group compared with those assigned control . 
the e ect was substantial and could be comparable to or greater than that achieved with the introduction of taxanes to adjuvant treatment of early breast cancer.6 , 30 however , this possibility needs to be con rmed in ongoing trials of adjuvant capecitabine . 
hj , rh , and hl provided administrative support . 1150 vol 10 december 2009 articles con icts of interest p - lk - l , mp , pp , and pb have received honoraria or consulting fees from roche . 
 all other authors declared no con icts of interest . acknowledgments we thank members of the independent monitoring committee ; chairman of the independent monitoring committee pertti neuvonen ; trial monitor raija husa ; medical , nursing , and clerical sta at participating centres ; and all women taking part in the finxx trial . 
the aim of this study was to assess the relative importance of di erent risk factors for treatment - emergent joint symptoms in patients assigned to anastrozole or tamoxifen as adjuvant treatment for postmenopausal breast cancer . methods the arimidex tamoxifen alone or in combination ( atac ) trial randomly assigned 9366 postmenopausal women to anastrozole ( 1 mg / day ) , to tamoxifen ( 20 mg / day ) , or to a combination of both . 
our analyses were based on data from case reports of 5433 women who were randomly assigned to anastrozole or tamoxifen , who started with their allocated treatment , and who did not have joint symptoms at entry ( anastrozole group : n = 2698 ; tamoxifen group : n = 2735 )  . 
joint symptoms were de ned as any report of arthralgia , arthrosis , arthritis , or joint disorder on a case - report forjoint disorders were de ned as reports of cervical spondylosis , osteoarthritis , and disc herniation . 
the atac trial is registered as an international standard randomised controlled trial , number isrctn18233230 . findings 777 of 1914 women ( 406% ) who used hormone replacement therapy ( hrt ) before trial entry developed joint symptoms compared with 1001 of 3519 women ( 284% ) without previous hrt use ( odds ratio [ or ] 172 [ 95% ci 153193 ] )  . 
women with hormone - receptor - negative breast cancer developed signi cantly fewer joint symptoms compared with those with hormone - receptor - positive tumours ( 124 of 461 [ 269% ] vs 1556 of 4548 [ 342% ] ; or 071 [ 057088 ] )  . 
women for whom chemotherapy was part of their initial treatment developed signi cantly more joint symptoms than those who did not receive it ( 461 of 1219 women [ 378% ] vs 1317 of 4214 women [ 313% ] ; or 134 [ 117153 ] )  . 
all signi cant risk factors from the univariate analysis were included in a multivariate analysis and remained signi cant with little change . interpretation in this trial , the major risk factors for developing joint symptoms were previous hrt , hormonereceptor positivity , previous chemotherapy , obesity , and treatment with anastrozole . 
discussion of identi ed risk factors is appropriate when counselling women before initiation of adjuvant hormonal treatment . funding this study was funded by cancer research uk and astrazeneca ( maccles eld , uk )  . introduction oestrogen de ciency has been associated with joint symptoms ( eg , arthralgia and arthritis ) in several di erent settings . 
in the general population , postmenopausal status and low oestrogen concentrations are associated with the development of joint pain and joint symptoms.1 , 2 these symptoms are most prominent around the ages of 50 to 59 years , 1 , 2 are more common in postmenopausal women than in premenopausal and perimenopausal women of the same age , 3 and often improve during use of hormone replacement therapy ( hrt ) .4 , 5 further evidence linking joint symptoms with decreased oestrogen concentrations comes from adjuvant trials of aromatase inhibitors in patients with early breast cancer , where increased joint symptoms ( eg , arthralgia and arthritis ) have been noted for all three thirdgeneration aromatase inhibitors.68 women treated with chemotherapy for breast cancer have also shown joint symptoms and other joint or muscle - related problems.9 , 10 however , tamoxifen does not seem to have an e ect on joint symptoms . 
in the rst international breast cancer intervention study , 11 joint symptoms were similarly distributed between treatment groups in postmenopausal women ( 159 of 3579 women in the tamoxifen group vs 147 of 3575 women in the placebo group ; p = 05 )  . 
 table 1 : patients with joint symptoms by severity and treatment rst received for all women ( safety population ) and for those without joint symptoms at entry ( study population ) symptoms in the arimidex tamoxifen alone or in combination ( atac ) trial , 13 and assess whether these risk factors act di erently in the presence of anastrozole treatment . 
 methods the atac trial13 was a double - blind randomised clinical trial in which postmenopausal women with early breast cancer were randomly assigned to oral daily anastrozole ( 1 mg ) alone , tamoxifen ( 20 mg ) alone , or a combination of both in a double - blind fashion , so that each woman took two tablets , at least one of which was active . 
 only women who started with their randomly assigned treatment and who did not report joint symptoms at entry were included in this analysis ( anastrozole group : n = 2698 ; tamoxifen group : n = 2735 )  . 
our analysis was based on the 100 - month median follow - up data set , at which point all patients had completed their study medication.14 because most symptoms occurred relatively early , and the e ects of treatment and other variables were not constant with time , the analysis was restricted to the occurrence of joint symptoms at any time during active treatment or within 14 days of its discontinuation . 
joint symptoms were de ned as any report of arthralgia , arthrosis , arthritis , or joint disorder ( coding symbols for a thesaurus of adverse reaction terms ) 15 on a case - report for joint disorders were de ned as reports of cervical spondylosis , anastrozole tamoxifen number at risk anastrozole tamoxifen 2698 2735 follow - up time ( years ) 2239 2372 1950 2085 1710 1859 1534 1656 1354 1464 figure 1 : patients ( % ) developing joint symptoms at or before a speci ed follow - up time during active treatment according to treatment rst received in women without joint symptoms at entry ( study population ) osteoarthritis , and disc herniation . 
for the atac trial , all side - e ect data were the result of elicited responses recorded on case - report forms and a speci c symptom check list was not used . 
interactions between treatment and subgroups were based on likelihood ratio tests for an added interaction terhazard plots were smoothed by use of an epanechnikov kernel with the optimum bandwidth chosen by cross validation.16 all p values are two - sided , with level of signi cance set at 005 , and all con dence intervals are at the 95% level . 
394 women in the anastrozole group and 359 women in the tamoxifen group ( or 090 [ 077105 ] ) reported a history of joint symptoms at entry into the trial . 
figure 1 shows the higher prevalence of joint symptoms reported by women without a history of joint symptoms at study entry in the anastrozole group compared with the tamoxifen group . 
in both treatment groups , most joint symptoms were of mild or moderate severity , and the intensity of symptoms was similarly distributed in both treatment groups ( table 1 )  . 
1067 of 1778 patients ( 60% ) who reported joint symptoms received treatment , with 960 of these patients ( 90% ) using a non - steroidal anti - in ammatory drug alone or in combination with a mild analgesic . potential risk factors for developing joint symptoms are shown for each treatment group in table 2 . 
after exclusion of women with baseline joint symptoms , 949 of 2698 women ( 352% ) reported joint symptoms in the anastrozole group compared with 829 of 2735 women ( 303% ) in the tamoxifen group ( or 125 [ 95% ci 111140 ; p < 00001 ] ; table 3 )  . 
for women who previously used hrt , 777 of 1914 ( 406% ) developed joint symptoms compared with 1001 of 3519 women ( 284% ) without previous hrt use ( or 172 [ 153193 ] ; p < 00001 )  . 
joint symptoms were increased by a similar amount for women who stopped hrt less than 6 months before trial entry compared with those who stopped hrt more than 6 months before entry ( 502 of 1201 women ( 418% ) vs 142 of 335 women ( 424% ) ; or 108 [ 084140 ] ; p = 054 )  . 
 women with hormone - receptor - negative breast cancer developed signi cantly fewer joint symptoms than those with hormone - receptor - positive tumours ( 124 of 461 ( 269% ) vs 1556 of 4548 ( 342% ) ; or 071 [ 057088 ] ; p = 0002 ; table 3 )  . 
 * north america = usa and canada . table 2 : selected baseline characteristics ( % ) according to treatment group ( study population ) role of the funding source this study was funded by cancer research uk and astrazeneca ( maccles eld , uk )  . 
 when all signi cant variables in the univariate models were entered into a multivariate model , the odds ratios were similar to the univariate ndings , except for smoking status , which became non - signi cant ( table 3 )  . 
 similar ndings for the univariate and multivariate analyses of risk factors were obtained if the population was restricted to hormone - receptor - positive women ( data not shown )  . 
additionally , there were no signi cant interactions of any factors with treatment , except for a weak interaction between treatment and previous hrt use ( pinteraction = 005 ; table 4 )  . 
 women from the usa and canada ( grouped as north america ) reported signi cantly more joint symptoms than those from the uk or the reference group of the rest of the world ( 738 of 1611 ( 458% ; or 244 [ 212280 ] ; p < 00001 ) vs 523 of 1815 ( 288% ; or 117 [ 101135 ] ; p = 003 ) vs 517 of 2007 ( 258% ) ; table 3 )  . 
data missing for 245 patients . table 4 : number ( % ) of women reporting joint symptoms at any time during treatment according to treatment rst received and selected risk factors in women without joint symptoms at entry ( study population ) no signi cant interactions of key variables in the univariate model were seen with region in the multivariate model ( data not shown )  . 
 discussion in this trial , the major risk factors for developing joint symptoms in women not reporting them at entry were previous hrt use , hormone - receptor positivity , previous chemotherapy , obesity , and treatment with anastrozole versus tamoxifen , leading to signi cant absolute increases of 121% , 73% , 65% , 62% , and 49% , respectively . 
women with pre - existing joint symptoms were excluded from this analysis to focus on new treatment - emergent symptoms . the e ect of previous hrt was especially striking , which could be because most women previously using hrt , for whom we had data , came o it within 6 months before entry into the study ( 1201 of 1536 women [ 782% ] ) , although the e ect was similar in women who had stopped their hrt treatment earlier . 
furthermore , the e ects of hrt seemed to be additive , resulting in an 181% increase in joint symptoms in women who previously used hrt and were on anastrozole compared with those on tamoxifen with no previous hrt use . 
 recent users of hrt ( ie , those who stopped use less than 6 months ago ) are likely to have a greater decrease in oestrogen concen trations with endocrine treatment than those who stopped use more than 6 months ago , and most , 17 , 18 but not all studies , 19 have shown that they are more likely than never users to have oestrogen - receptorpositive tumours . 
in our study , women with hormonereceptor - positive tumours reported more joint symptoms than those with hormone - receptor - negative tumours , but , paradoxically , the few women with tumours of unknown hormone - receptor status had the lowest number of joint symptoms . 
several studies have shown that women with high oestrogen concentrations are more likely to develop oestrogen - receptor - positive tumours than those with low oestrogen concentrations.20 , 21 obese women tend to have higher oestrogen concentrations than non - obese women as a result of aromatisation from the adipose tissue , 22 so the decrease in oestrogen concentration is likely to be greater in this group as well . 
obesity itself is also a risk factor for joint symptoms independent of endocrine treatment.23 however , crew and colleagues24 reported that women with a bmi between 25 and 30 kg / m developed fewer joint symptoms than those with a lower bmi . 
 chemotherapy is well known to induce arthralgia or myalgia and has been reported in several trials independently of endocrine treatment.10 , 2527 chemo therapy is known to damage ovarian function in premeno pausal women , and the e ects seen here could be a result of the ablation of any residual ovarian production of oestrogen in these postmenopausal women . 
again , the ndings were additive in anastrozole users so that the use of previous chemotherapy and anastrozole together resulted in a 124% increase in joint symptoms when compared with women on tamoxifen without previous chemo therapy . reports have suggested that side - e ects , such as joint symptoms , are under - reported in clinical trials compared with patient - recorded side - e ects.28 , 29 the atac trial was an international study , involving 21 countries . 
because of the nature of the collection , in which uniform de nition of symptoms was not provided , subcategories of joint symptoms were not thought to be reliable and were , therefore , not reported during the atac trial . 
additionally , the duration of symptoms and date of resolution of symptoms could not be assessed in detail , because data were collected at 3 months , 6 months , and at 6 - monthly intervals thereafter , so dates within these intervals were not recorded . 
because the study was blinded , there would have been no bias in relative rates , but the overall reporting rates for speci c symptoms could have been a ected . 
however , this approach did seem to be sensitive , because known minor side - e ects , and some previously unknown ones , were clearly detectable.30 the symptoms were assessed by clinicians and mapped to the relevant costart 870 vol 9 september 2008 articles terms.15 this ascertainment of joint symptoms needs to be taken into account when interpreting these ndings . 
 by contrast , a higher drop - out rate caused by joint symptoms was reported in two smaller uncontrolled studies , 31 , 32 but it is di cult to attribute all these events to an aromatase inhibitor , because joint symptoms are common in postmenopausal women ( eg , 31% of women receiving tamoxifen in the atac trial reported joint symptoms )  . the increased incidence of joint symptoms in the north american population is most probably consistent with di erent practices for recording symptoms . 
 although more patients had previous hrt use , previous chemotherapy , and a higher bmi in north america , compared with the uk and the rest of the world , the e ects of region were only slightly diminished when they were adjusted for in the multivariate model . 
 no signi cant interactions between region and risk factors were identi ed , suggesting that the di erences noted between regions were most probably due to di erent thresholds for reporting these symptoms in north america , especially because adverse events overall were more often reported in north american participants . in conclusion , several factors other than treatment with anastrozole were associated with the development of joint symptoms in this trial . 
joint symptoms were generally of mild to moderate intensity and for most women they do not override the clear bene ts of anastrozole over tamoxifen in terms of decreased recurrence and fewer other major side - e ects , including and gynaecological complications ( eg , endometrial cancer ) .14 however , for women with serious side - e ects on anastrozole , remains a viable option . 
 awareness of risk factors for joint symptoms will help both clinicians and patients to anticipate and manage these symptoms and ensure optimum adherence to endocrine treatment . thromboembolic tamoxifen venous events con icts of interest is declared no con icts of interest . 
all contributors took part in writing the paper and approved the nal version . acknowledgments this research was supported by cancer research uk and astrazeneca ( maccles eld , uk )  . 
we also thank the trial investigators , other supporting sta , and the members of the international steering committee . re ection and reaction with endemic burkitts lymphoma in africa from poor families , and will gladly share more detailed information with interested colleagues . 
the socit franaise doncologie pdiatrique lmb89 protocol : highly e ective multiagent chemotherapy tailored to the tumor burden and initial response in 561 unselected children with b - cell lymphomas and l3 leukemia . 
follow - up is done by dedicated health - care workers who actively seek out patients in their villages . colleagues in kenya and uganda did not accept the invitation to join in the rst study supported by siop , 3 perhaps because the proposed treatment schedule might have been perceived at the time as being worse than established treatment schedules , such as cyclophosphamide , doxorubicin , vincristine , and pred nisolone . 
 however , the french - african pediatric oncology group has now used the same schedule of cyclophosphamide and intrathecal methotrexate in several sub - saharan francophone countries , with comparable e cacy ( jean lemerle , socit franaise doncologie pdiatrique , personal communication ) .6 patients with primary resistance to this treatment , or who relapsed after treatment , have been treated with a 15 - day schedule of cyclophosphamide ( 60 mg / kg ) , vincristine ( 15 mg / m2 ) , and standard - dose intrathecal methotrexate on days 1 , 8 , and 15.7 a third of these patients remain in continuous remission after more than a years follow - up and are considered cured.7 thus , this approach has lead to an overall 1 - year survival of 67% for the group of patients enrolled in these rst - line and refractory studies.4 , 5 , 7 we believe that we have established an e ective , welltolerated , and a ordable treatment option for patients erratum veldeman l , madani i , hulstaert f , de meerleer m , mareel m , de neve w . 
the corrected webtables have been republished online . see online for webtables vol 9 june 2008 articles cancer survival in ve continents : a worldwide population - based study ( concord ) michel p coleman , manuela quaresma , franco berrino , jean - michel lutz , roberta de angelis , riccardo capocaccia , paolo baili , bernard rachet , gemma gatta , timo hakulinen , andrea micheli , milena sant , hannah k weir , j mark elwood , hideaki tsukuma , sergio koifman , gulnar azevedo e silva , silvia francisci , mariano santaquilani , arduino verdecchia , hans h storm , john l young , and the concord working group * summary background cancer survival varies widely between countries . 
the concord study provides survival estimates for 19 million adults ( aged 1599 years ) diagnosed with a rst , primary , invasive cancer of the breast ( women ) , colon , rectum , or prostate during 199094 and followed up to 1999 , by use of individual tumour records from 101 populationbased cancer registries in 31 countries on ve continents . 
 methods to compensate for wide international di erences in general population ( background ) mortality by age , sex , country , region , calendar period , and ( in the usa ) ethnic origin , we estimated relative survival , the ratio of survival noted in the patients with cancer , and the survival that would have been expected had they been subject only to the background mortality rates . 
5 - year relative survival for breast , colorectal , and prostate cancer was generally higher in north america , australia , japan , and northern , western , and southern europe , and lower in algeria , brazil , and eastern europe . 
concord has provided the rst opportunity to estimate cancer survival in 11 states in usa covered by the national program of cancer registries ( npcr ) , and the study covers 42% of the us population , four - fold more than previously available . 
relative survival for all ethnicities combined was 24% lower in states covered by npcr than in areas covered by the surveillance epidemiology and end results ( seer ) prograage - standardised relative survival by use of the appropriate racespeci c and state - speci c life tables was up to 2% lower for breast cancer and up to 5% lower for prostate cancer than with the census - derived national life tables used by the seer prograthese di erences in population coverage and analytical method have both contributed to the survival de cit noted between europe and the usa , from which only seer data have been available until now . interpretation until now , direct comparisons of cancer survival between high - income and low - income countries have not generally been available . 
the ndings should eventually facilitate joint assessment of international trends in incidence , survival , and mortality as indicators of cancer control . funding centers for disease control and prevention ( atlanta , ga , usa ) , department of health ( london , uk ) , cancer research uk ( london , uk )  . 
 introduction international comparisons of population - based cancer survival have been rare , 15 but large and unexplained di erences in survival have been reported for many cancers from individual studies and cancer registries in europe and north america.6 for example , 5 - year relative survival for women diagnosed with breast cancer during 198589 was 73% in europe ( weighted mean for 17 countries ) 7 and 84% in the usa.8 the concord study provides a systematic comparison of survival between europe and north america , 916 extended to countries in all other continents . the rst international comparison of cancer survival , published in 1964 , 17 was a study of patients diagnosed with one of 15 common cancers in denmark , england , finland , france , norway , sweden , and the usa , mainly during 194554 . 
it was the rst study in which relative survival techniques , rst described in the 1950s , 1820 were used to correct the survival estimates for di erences in background mortality between participant countries . 
the ndings are mainly of historical interest , but survival in the usa ( represented by connecticut ) was generally higher than in the european countries . cancer survival is known to vary between the regions of the usa covered by the us national cancer institutes ( nci ) surveillance , epidemiology and end results ( seer ) program , 21 but the range of survival in europe is much wider . 
concord also enables comparison of cancer survival between ve states and four metropolitan areas in the usa covered by the seer program ( seer - 9 ) and 11 states covered by the centers for disease control and preventions ( cdc ) national program of cancer registries ( npcr )  . 
it also provides a wider comparison of cancer survival between black and white patients in the usa than has previously been possible . concord includes data from one or more countries on all ve continents . 
to our knowledge , it is the rst attempt at a global comparison of cancer survival . methods cancer registries in 1999 , we identi ed at international cancer meetings in atlanta ( usa ) and lisbon ( portugal ) , and from published studies , population - based cancer registries that had published survival data and were operational during 199099 . 
in total , we identi ed 112 registries , but 11 were withdrawn or excluded : no response ( one ) ; withdrawal for legal reasons ( one ) ; incomplete registration before 1995 ( four ) ; follow - up activity stopped be fore 1999 ( two ) ; data not supplied by the september , 2005 deadline ( three )  . a pilot study of 50 registries in 2000 obtained a 100% response . 
all registries were able to provide data for patients diagnosed during all or part of the period 199094 , and had access to various data sources to obtain follow - up information for all patients for at least 5 years or to the end of 1999 . 
after further recruitment , a detailed questionnaire was obtained for 100 of the 101 registries nally included in the analyses , covering data de nitions and methods of operation , including data collection , coding of tumour site , morphology , behaviour , and stage at diagnosis , tracing of registered patients to ascertain their vital status , and linkage between data on the incident tumour and data on subsequent death or loss to follow - up . 
the procedures and de nitions used , the stated quality and completeness of data on the registration of incident cancers , and of the follow - up of those patients over the next 5 years , were deemed adequate to attempt cancer - survival analysis , subject to central quality control of the data . 
we retained hawaii ( usa ) with north america rather than oceania . africa was represented by a single cancer registry , for the wilaya ( dpartement , or state ) of stif ( algeria )  . central and south america , including the caribbean , were represented by the national cancer registry of cuba and two regional registries in brazil : the goinia ( gois state ) registry is one of 20 registries in state capitals , whereas the campinas ( so paulo state ) registry is the only one in brazil that is not in a state capital . data from north america include ve of the seven largest provinces in canada ( british columbia , manitoba , nova scotia , ontario , and saskatchewan )  . 
data for the usa came from 22 registries covering 16 states ( california , colorado , connecticut , florida , hawaii , idaho , iowa , louisiana , michigan , nebraska , new jersey , new mexico , new york state , rhode island , utah , and wyoming ) and six metro politan areas ( atlanta , ga , los angeles , ca , san fran cisco , ca , detroit , mi , new york city , ny , and seattle , wa )  . population - based cancer registries in the usa receive sup port from either or both of the two federal cancersurveillance programmes , the ncis seer program and the cdcs npcr.36 as of 1990 , the seer program in cluded nine population - based cancer registries covering some 10% of the us population ( seer - 9 ) : the states of connecticut , hawaii , iowa , new mexico , and utah , and the metropolitan areas of atlanta , ga , detroit , mi , san francisco , ca , and seattle , wa . 
the los angeles cancer registry be came a seer registry in 1992 , but we opted to retain it with the npcr data , so that the seer grouping vol 9 august 2008 articles we used was identical with that for which seer data had been published in the past ( seer - 9 )  . 
we received separate datasets from detroit , mi , san francisco , ca ( seer registries ) , and los angeles , ca ( npcr ) , and these were included in the respective totals for seer and npcr . 
 however , the data from these metropolitan areas could not be separately identi ed in the state - wide datasets we received from california and michigan , therefore , the nonmetropolitan data for those states could not be included with the other npcr data . 
 table 1 : population coverage and number of adults ( aged 1599 years ) diagnosed with cancer of the breast , colon , rectum , or prostate during 199094 * and included in the analyses : continent , country , and region 734 vol 9 august 2008 articles npcr : colorado , florida , idaho , los angeles , ca , louisiana , nebraska , new jersey , new york , rhode island , and wyoming . 
for this comparison , data from the non - metropolitan areas of california and michigan were ex cluded to ensure that the two sets of data were mutually exclusive . in asia , japan was represented by three of the prefectural ( state ) registries : fukui , osaka , and yamagata . in europe , the 53 cancer registries that contributed data to eurocare - 328 on cancers of the breast , colon , rectum , or prostate all participated in the concord study . 
six other registries also provided data : two national registries ( northern ireland and ireland ) and four regional registries from the netherlands ( north ) and switzerland ( graubunden - glarus , st gallen - appenzell , valais )  . 
in england , both the national cancer registry and eight of the regional cancer registries submitted datasets . oceania was represented by the national cancer registry of australia , with data from each of the eight populationbased state or territorial registries . quality control procedures used in the eurocare - 3 study were applied to all datasets . 
tumour records were supplied with the anatomical site coded to the ninth revision of the international classi cation of diseases ( icd - 939 ) for four index tumours : cancers of the breast ( women ) ( icd - 9 174.0174.9 ) , colon ( 153.0153.9 ) , rectum ( including the anus , 154.0154.9 ) , and prostate ( 185 )  . 
tumour morph ology and behaviour were coded to the rst or second revision of icd - oncology ( icd - o , 40 icd - o - 241 )  . 
the duration of survival was taken from the date of diagnosis of the index tumour until death from any cause , or until the patient was censored from the analysis as alive , either at loss to follow - up or after dec 31 , 1999 , whichever came rst ; any subsequent tumour occurring in the same patient during that period was ignored . standard quality - control routines , based on those developed by the international agency for research on cancer , 42 were applied to each tumour record . 
corrected tumour records were checked again : those which still had missing , invalid or inconsistent values for sex , site , morphology , or dates were agged as major errors and excluded from analysis . 
 records for which an unlikely combination of age , site and morphology had nonetheless been con rmed as correct were agged as minor errors , and included in the analyses . 
 details of the approach have been published else where.43 detailed quality - control ndings are available online.34 follow - up all registries used more than one mechanism of follow - up to ascertain the vital status ( alive , dead , emigrated , lost to follow - up ) and the date of the last vital status for each registered patient . 
secure linkage of a tumour record and a record of death , based on a set of identi ers such as name , sex , date of birth , and personal identity number , enabled the registry to update the tumour record accordingly . 
 a wide variety of administrative data bases was also used , such as social insurance , health insurance , motor vehicle records , drivers licences , hospital discharge records , national primary - care databases , electoral registers ( those eligible to vote ) , and voter registration records ( those who voted in the last election )  . 
this is subject to administrative error ( failure to remove in timely fashion the record of a person known to be dead ) and fraud ( by someone seeking to retain access to bene ts received by the deceased ) , but in most instances the risks are small . 
 if coverage of the databases was known to be high , and especially if a person was present in more than one such database , the risk of error decreased further . in the usa , a match to an administrative database might show that an event occurred during a certain quarter of a year ( eg , an insurance claim paid , a licence renewed ) , but the exact date might not be known ; the date of last vital status was then set to the rst day of the quarter , ie , jan 1 , april 1 , july 1 , sept 1 . 
this approach can give rise to irregu lar distribu tions of the day of last known vital status , but it is a conservative approach to establishing when patients were last known to be alive , because patients are censored from sur vival analysis on the latest of any such dates in the record . the proportion of patients not known to be dead and for whom the registry could not be certain that the date of last vital status was at least 5 years after diagnosis was less than 1% overall . 
such patients are described as censored from the analysis . statistical analysis we estimated relative survival up to 5 years after diagnosis from the individual tumour data , using the hakulinen approach44 embedded in the us national cancer institutes publicly accessible seer * stat software.45 seer * stat is the standard tool used for cancer - survival estimation by the seer program cancer registries , and we used it to ensure that survival estimates for us registries would be seen as comparable with those already published by the seer prograsurvival estimates were also derived by race for the usa ( black and white )  . relative survival is the ratio of the survival noted in the patients with cancer and the survival that would have been expected had they been subject only to the mortality rates of the general population ( background mortality )  . 
it is a measure of the excess mortality in patients with cancer over and above the background mortality , and can be interpreted as survival from the cancer after correction for other causes of death . 
background mortality was taken from life tables developed specially for the concord study , speci c for sex , calendar year , region , and race.46 the probability of survival in successive years after diagnosis was estimated in survivors to the start of each year . 
95% cis were calculated by use of a logarithmic transformation ( see text )  . table 2 : 5 - year relative survival ( % ) , age - standardised to icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colon , rectum , or prostate during 199094 and followed up to dec 31 , 1999 : continent , country , and region 738 vol 9 august 2008 articles see online for webtable for heterogeneity in the withdrawal of patients from followup and consequent changes in the age - sex - race distribution of patients with cancer in successive calendar years , by use of the exact method.44 expected survival was derived from complete life tables that contained the probabilities of death or the central death rates for the general population of the registrys territory , by single year of age , sex and ( where possible ) race , and single calendar year between 1990 and 1999 . 
for some registries , complete life tables were constructed from raw data obtained from published sources on the numbers of deaths by age , sex , and race in the relevant year ( s ) or period , and the corresponding populations . 
race - speci c estimates of relative survival were produced with separate life tables for each race , constructed from the raw data on populations and the number of deaths.46 in the usa , race - speci c mortality in the general population also varies between states.36 we developed separate sets of complete life tables for each state and metropolitan area and for each sex . 
this approach was designed to enable the closest possible adjustment of relative survival estimates in the usa for geographic variation in background mortality in both blacks and whites , by age , sex , and calendar period . 
for ve less populous states ( hawaii , idaho , new mexico , utah , and wyoming : 6% of the 109 million population covered by participating registries ; webtable ) , only the life tables for whites were su ciently robust , and relative survival estimates for blacks are not separately presented . relative survival measures the extent to which patients with cancer have a higher death rate than the general population of the country or region in which they live.56 occasionally , despite use of the most appropriate life table , this excess death rate can be negative in a given time interval since diagnosis , implying that the death rate of cancer survivors during that interval is actually lower than that of the general population . 
this situation can arise from random variation in the death rate when the number of deaths in the interval is small , 57 either because the interval is very short , or because survival is poor and most patients have already died before the start of the interval , or because survival is high and there are very few deaths . 
in such situations , we present by default the estimate derived by use of the seer * stat option to constrain the excess mortality rate to zero , which imposes a plateau in the relative survival curve . 
the unconstrained estimate was also obtained for comparison . even though relative survival is already adjusted for agespeci c di erences in background mortality , robust international comparison of relative survival requires agestandard isation , 23 because the age distribution of patients with cancer varies between countries , and because relative survival also varies widely by age , at least in europe.27 conventional age - speci c weights used to standardise incidence or mortality rates ( eg , the national population or the hypothetical world standard population58 ) are unsuitable because patients with cancer have a very di erent age pro le from that of the general population . a cancer - survival comparison of such wide scope has not been done before and the choice of weights for agestandardisation was not straightforward . 
international stan dard cancer - patient populations have been proposed , with di erent sets of weights in 5 - year or 10 - year age bands for each of 20 common cancers , derived from their worldwide distribution.59 the weights used for the eurocare - 3 study were derived from the age distribution of all patients included in that study for each cancer , and were thus cancer - speci c.43 the disadvantage of these standards is either that a unique set of weights is required for each cancer ( cancer - speci c ) , or else that the standards are arbitrary ( study - speci c ) , vitiating comparison between studies . we chose the recently developed international cancer survival standard ( icss ) weights.60 these comprise just three sets of age weights , derived from discriminant analysis to nd the smallest number of sets of standard age weights that enable adequate standardisation of survival . 
where data were too sparse for standardisation , the raw ( unstandardised ) survival estimate is presented , agged with r . the same age weights were used for men and women , and for each race , enabling direct comparison of agestandardised relative survival between patient groups de ned by sex and race . 
this would not be possible if cancer - speci c weights were used . vol 9 august 2008 articles figure 1 : 5 - year relative survival ( % ) , agestandardised to the icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colorectum , or prostate during 199094 and followed up to dec 31 , 1999 : country vertical bar on the right of each graphic shows the contribution ( % ) of each continent to the total number of cases analysed ( contributions under 1% are not labelled )  . 
 * agestandardised to icss weights , except for stif , algeria ( all cancers ) , malta ( prostate ) , and portugal ( prostate ) , which were unstandardised values ( see text )  . 
 740 cuba canada sweden japan australia finland france italy iceland spain netherlands norway switzerland germany austria denmark malta portugal northern ireland scotland england ireland wales slovenia poland czech republic estonia brazil slovakia algeria cuba france canada australia japan sweden malta norway netherlands austria germany spain iceland finland italy ireland northern ireland denmark scotland england portugal brazil wales slovakia czech republic slovenia estonia poland algeria breast ( women ) prostate colorectum ( women ) colorectum ( men ) 417 507 430 469 austria canada australia germany france iceland cuba netherlands sweden italy norway finland ireland spain estonia scotland northern ireland england czech republic japan brazil wales portugal slovakia malta slovenia denmark poland algeria japan cuba australia france canada netherlands sweden austria spain finland norway italy germany iceland northern ireland brazil portugal ireland scotland denmark england wales estonia slovenia malta slovakia czech republic poland algeria 263 656 433 457 5 - year relative survival ( % ) 5 - year relative survival ( % ) africa america , central and south america , north asia europe oceania data covering less than 100% of country vol 9 august 2008 articles figure 2 : 5 - year relative survival ( % ) , using statespeci c and race - speci c life tables and age - standardised to the icss weights * for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colon , rectum , colon and rectum combined , or prostate during 199094 and followed up to dec 31 , 1999 : 16 us states and six metropolitan areas vertical lines represent mean survival for seer ( red ) and npcr ( green ) registries , agestandardised to icss weights ( see text )  . 
 problems with data quality might have led to overestimation ( see text )  . vol 9 august 2008 articles for countries represented by more than one regional cancer registry , we provide a survival estimate derived from the pooled data for all contributing registries , agestandardised in the same way . 
we used these standard errors to estimate cis on the logarithmic scale ( webpanel )  . for the usa , we constructed funnel plots of relative survival for each cancer and sex , to obtain further insight into the variability of survival by race and state , and to avoid spurious ranking of the survival estimates.62 the plots show how much a particular survival estimate deviates from the pooled us value , given the precision of for each estimate . 
the precision depends on the number of deaths included in the analysis , which depends in turn on the size of the popu lation and the frequency and lethality of the cancer in that population . 
5 - year relative survival estimates for each popu lation , age - standardised race - speci c and state - speci c and adjusted background mortality , were plotted against the precision of the estimates , taken as the inverse square of their standard errors ( webpanel )  . 
the horizontal line in each plot , the target , was estimated as the pooled 5 - year relative survival for all participating us populations , agestandardised to the same weights . 
see text for attribution of registries to npcr and seer . r = raw ( not age - standardised ) survival estimate : too few cases in one or more age groups . 
black populations are not shown separately for hawaii , idaho , new mexico , utah , or wyoming , because it was not possible to estimate relative survival for blacks in these states with race - speci c life tables ( see text )  . table 3 : 5 - year relative survival ( % ) by use of state - speci c and race - speci c life tables and age - standardised to icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colon , rectum , or prostate during 199094 and followed up to dec 31 , 1999 , by race : us populations vol 9 august 2008 articles di erences between survival estimates are presented as the absolute value , eg , 15% is given as 5% ( not 50% ) higher than 10% . we analysed individual data for almost 2 million adults who were diagnosed with a rst , primary , malignant , invasive neoplasm of the breast ( women ) , colon , rectum , or prostate during the period 199094 and who had been followed up to ascertain their vital status for at least 5 years after diagnosis until the end of 1999 or later . 
data were contributed by 101 population - based cancer regis tries covering a combined population of almost 300 million persons living in 31 countries ( table 1 and web gure 1 )  . 
 the 24 european countries contri buted 740 000 patients ( 37% ) from a population base of 126 million , indicating lower mean incidence of cancer than in north america . the smallest dataset came from stif ( algeria ) , covering a population of 11 million , some 4% of the national population . 
the registry could only provide data for the period 199294 , the population is young , and cancer risks are currently low on the global scale.63 the dataset was therefore small , a total of 300 patients . 
this decreases the statistical precision of survival estimates , but no patient was detected solely at death certi cation or autopsy , and the vital status of every patient was ascertained at a home visit by registry sta , something no other registry could deliver . 
california provided the largest single dataset of 240 000 patients diagnosed during 199094 in a population of 31 million ( 12% of the us population ) , with a very high cancer risk on the global scale ( table 1 )  . for 16 of the 31 countries , the data covered 100% of the national population ( table 1 )  . 
the proportion of the national population covered by the data for the other 15 countries ranged from less than 10% ( algeria , brazil , japan , austria , czech republic , france , germany , poland ) to 1029% ( italy , portugal , spain , switzerland ) and 30% or more ( canada , usa , the netherlands )  . most registries provided data on patients diagnosed during the entire 5 - year period 199094 , but ten registries provided data for shorter periods ( table 1 )  . data for all four index cancers were provided by 89 of the 101 registries . 
two specialised registries in cte - dor ( france ) only collect data on cancers of the breast or colorectum , respectively , whereas ten general registries that collect data for all cancers only contributed data for selected cancers : breast ( isre , france ; northern netherlands ; all ve swiss registries ) ; breast , colon , and prostate ( campinas , brazil ; nova scotia , canada ) , or breast , colon , and rectum ( granada , spain ; table 1 )  . ethical approval for the concord study33 was obtained from the istituto superiore di sanit , rome , italy ( ce - iss 02 / 03 , may 20 , 2002 ) and from the institutional review board of the cdc , atlanta , ga , usa ( irb #3551 , july 24 , 2002 )  . 
seer data were obtained from the public - use dataset.38 for other registries , anonymised data were transmitted to the concord data analysis centre at the istituto superiore di sanit by use of special courier delivery of encrypted and password - protected cd - roms with separate email transmission of the password , or preplanned deposition of password - protected les on a specially created file transfer protocol ( ftp ) site from which the data were immediately removed in rome . 
each tumour record included a serial number for the purposes of quality control with the originating cancer registry . role of the funding source the pilot study ( january , 2000 to march , 2000 ) was funded by the uk department of health ( 75 000 )  . 
the cdc funded data collection and the costs of linkage to the national death index for the phase i study in participating registries in the national program of cancer registries ( us$3 million )  . 
the cancer survival group ( including br , mq ) in the london school of hygiene and tropical medicine , london , uk , has been funded by cancer research uk ( grant c1336 / a5735 ) since april , 2005 . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results the background risk of death in the general population varied widely between the participating countries and regions . 
the mean life expectancy at birth during the decade 199099 ranged from 637 to 776 years in men and from 709 to 837 years in women.46 in the usa , the range of life expectancies in white and black populations did not overlap at all in the states and metropolitan areas for which life tables could be con structed for both groups . 
 the ranges for men were 640701 years in blacks and 711759 years in whites , whereas the ranges in women were 733765 years in blacks and 788809 years in whites . 
 the cumulative risk of death from all causes over the age range 1559 years in the general population of the participating countries and regions ranged widely , from 9% to 34% in men and from 5% to 17% in women . 
over the age range 6084 years , the cumulative risk of death ranged from 60% to 86% in men and from 40% to 75% in women.46 of 785 255 records of breast cancer submitted for analysis , 45 020 ( 6% ) related to women registered with a previous primary cancer , and were excluded ( available online34 ) of the 740 235 eligible rst primary invasive breast cancers , 9215 records were excluded as death - certi cateonly ( dco ) registrations ( 1% ) , 239 as autopsy - detected tumours ( < 1% ) and 2064 with major errors ( < 1% ) , leaving 728 717 patients for analysis ( 98% of those eligible ) , of whom 370 000 ( 51% ) were resident in north america and 304 000 ( 42% ) in europe ( table 1 )  . 
almost all ( 97% ) of the 744 vol 9 august 2008 articles see online for web gures 2 and 3 tumours included in the analyses were microscopically veri ed , less than 1% of patients were censored from the analysis within 5 years of diagnosis , and 23% died within 1 month of diagnosis . relative survival at 5 years , age - standardised to the international cancer survival standard weights , ranged from 80% or over in north america , sweden , japan , finland , and australia to less than 60% in brazil and slovakia , and below 40% in algeria ( table 2 and gure 1 )  . 
 survival in the 24 european countries that contributed to concord was mostly in the range 7079% . the survival estimate of 388% ( 95% ci 314462 ) for stif ( algeria ) is based on 180 patients , and it is not agestandardised because there were too few patients for analysis in some age groups , but age - standardisation for breast cancer in other datasets rarely altered the raw estimate by more than 5% in either direction ( data not shown ) , and survival from breast cancer was undoubtedly much lower in algeria than in all the other countries . the pooled estimate of 5 - year survival for the two brazilian registries was 584% , but the estimate for goinia ( 654% ) is more reliable than the very low gure for campinas ( 366% ) , where high proportions of patients were excluded as dco or with major errors ( available online34 )  . 
the 5 - year survival estimate for cuba was 840% , but this was likely to be an over - estimate : some 28% of records were excluded because they were registered solely from a death certi cate . the pooled estimate of 5 - year survival for canada was 825% , with a narrow range from 793% in nova scotia to 854% in british columbia ( table 2 and gure 1 )  . 
in the usa , 5 - year relative survival for all races combined ranged from 7881% in new york city , new york state , and louisiana to 8990% in hawaii and seattle , wa ( table 2 ) , but most of the estimates were within a fairly narrow range , from 82% to 87% ( gure 2 )  . 
survival in metropolitan areas covered by seer registries was similar to that in the respective states : detroit , mi 830% and michigan state 823% ; san francisco , ca 862% and california state 846% . 
5 - year survival was 774% for residents of new york city , ny ( with 40% of the state population ) , slightly lower than for new york state as a whole , 810% . survival was lower for blacks than for whites in all 17 populations in the usa for which this could be assessed with race - speci c life tables ( web gure 2 )  . 
the range in survival was wider for blacks ( 6083% ) , but the values at both extremes of the range were based on relatively few patients and have wider cis . 
within a given us population , the absolute di erence in age - adjusted relative survival between blacks and whites ranged from 2% ( rhode island , nebraska ) to 2527% ( iowa and seattle , wa ; table 3 and web gure 2 )  . 
even in areas where blacks comprise 25% or more of the population , survival for black women was 814% below the lowest estimate for white women ( 796% ) in any of the participating areas : atlanta , ga ( 711% ) , detroit , mi ( 717% ) , new york city , ny ( 658% ) , and louisiana ( 699% )  . 
the pooled estimate of 5 - year survival for the usa was 840% , with 861% in areas covered by seer and 831% in areas covered by npcr ( table 3 )  . survival in black women was always lower than the mean survival for all us populations included , and often more than three standard deviations below it ( below the 998% control limits ) , after controlling for the precision of the estimates . 
survival in white women is generally within or above the upper control limits , especially in territories covered by the seer prograa notable exception is for white women in new york state , including new york city , where the survival estimates are precise , but well below the lower control limits ( web gure 3 )  . the pooled estimate of 5 - year survival for breast cancer in japan was 816% . 
survival in osaka ( 794% ) was lower than in fukui ( 831% ) and yamagata ( 873% ; table 2 and gure 1 )  . 5 - year relative survival for breast cancer in europe , agestandardised to the icss weights , ranged from 579% in slovakia to 820% in sweden ( table 2 and gure 1 ) , whereas the pooled estimate derived from the data of 58 registries in the 24 participating european countries was 731% . 
 survival estimates for most of these countries have been reported.27 the concord study includes additional data from four countries : 5 - year survival was 696% in ireland and 720% in northern ireland , similar to the uk mean value of 697% ( table 2 )  . 
in switzerland , 5 - year survival in the cantons of st gallen - appenzell , graubunden - glarus , and valais was 7275% , about 47% lower than in geneva or basel . 
5 - year survival was 778% in northern netherlands , similar to that in amsterdam and southern netherlands ( 7678% )  . the national estimate of 5 - year survival for breast cancer in australia was 807% . 
survival was virtually identical in the six largest states ( 96% of the national population ) , in the range 8082% , but notably lower in the two smallest regions : 719% in northern territory ( 10% of the population ) and 771% in tasmania ( 26% )  . of 488 741 colon cancer records submitted for analysis , 45 862 records ( 9% ) were excluded for a previous cancer , leaving 442 879 rst , primary , invasive colon cancers eligible for analysis ( available online34 )  . 
a further 13 102 ( 3% ) were excluded as dco registrations , 1534 ( < 1% ) as autopsydetected tumours , and 1144 ( < 1% ) as major errors , leaving 427 099 patients for inclusion in the analyses ( 96% of those eligible )  . 
almost 11% of patients died within the rst month after diagnosis . relative survival at 5 years , age - standardised to the icss weights , ranged from about 60% in north america , japan , australia , and some western european countries down to vol 9 august 2008 articles see online for web gure 4 40% or less in algeria , brazil , czech republic , estonia , poland , slovenia , and wales ( table 2 and gure 3 )  . the survival estimates of 114% ( 95% ci 07409 ) for men and 306% ( 95561 ) for women in stif ( algeria ) were based on fewer than 20 patients , and are not agestandardised , but survival was clearly lower in algeria than in all the other countries . the estimate of 5 - year relative survival for goinia ( 481% in men , 448% in women ) was more plausible for brazil than the low estimates for campinas , where 26% of patients had to be excluded with errors.34 5 - year survival in cuba was about 60% in both sexes , although more than half the patients were excluded from analysis as dcos.34 in canada , the pooled estimate of 5 - year survival was 561% for men and 587% for women . 
in the usa , 5 - year relative survival for all races combined was 601% in both sexes , with a range from 536% for women in new york city to 679% for men in hawaii ( table 2 and gure 2 )  . 
again , most of the estimates were within a narrow range , 5964% . 5 - year survival for colon cancer among blacks in the usa was lower than among whites . 
in 34 paired observations of this di erence in survival ( men and women in 17 popu lations ) , only three exceptions were noted , in men and women in iowa and men in nebraska . 
the estimates for blacks in those three areas were based on fewer than 50 patients , have wide con dence intervals and were not age - standardised ( table 3 and web gure 4 )  . 
the pooled estimate of age - adjusted 5 - year relative survival for the usa was 61% for white men and women , and 5152% for black men and women . 
within a given population , the absolute di erence between blacks and whites ranged from 26% in men and 73% in women in los angeles , ca to 143172% in colorado . 
the geographical range in blackwhite di erences in survival is a ected by small populations to some extent , but even in areas where blacks comprise 25% or more of the population ( atlanta , ga , detroit , mi , new york city , ny , louisiana ) , 5 - year survival from colon cancer in blacks was 612% lower than for whites in the same population ( table 3 )  . 
the pooled estimate of 5 - year survival in areas covered by npcr was 598% for men and 596% for women , and 619% for men and 621% for women in seer areas . age - standardised survival in whites ranged from 549% to 679% ( table 3 and web gure 4 )  . 
 survival in blacks was generally lower than the mean value for all included us populations and often more than three standard deviations below the mean , after controlling for precision of the survival estimates . 
the main exception was for white women in new york state , including new york city , ny , where survival estimates were precise , but more than three standard deviations below the lower control limits around the pooled us estimate ( web gure 3 )  . in japan , the pooled survival estimate was 630% in men and 571% in women , although survival was about 10% lower in osaka prefecture than in fukui or yamagata ( table 2 and gure 3 )  . in europe , 5 - year relative survival for colon cancer in men ranged from 285% in poland to 5457% in spain , finland , austria , and france . 
in women , the lowest estimate was also for poland ( 309% ) , while survival was in the range 5560% in nine countries ( table 2 and gure 3 )  . 
the estimates for northern ireland were 473% in men and 490% in women , slightly higher than the pooled estimate for the uk , 435% in men and 444% in women ( table 2 )  . the national estimate of 5 - year survival for colon cancer in australia was 578% in men and 577% in women . 
 survival ranged from 5062% in the eight states and territories : it was highest in new south wales , the australian capital territory , and queensland , and lowest in tasmania , northern territory , and western australia ( 96% of the population ; table 1 )  . of 233 176 rectal - cancer records submitted for analysis , 15 731 records ( 7% ) were excluded for a previous cancer , leaving 217 445 rst , primary , invasive rectal cancers eligible for analysis ( available online34 )  . 
a further 3213 ( 1% ) were excluded as dco regis trations , 517 ( < 1% ) as autopsydetected tumours and 574 ( < 1% ) as major errors , leaving 213 141 patients for inclusion in the analyses ( 98% of those eligible )  . 
almost 8% died within the rst month after diagnosis . 5 - year relative survival from rectal cancer , agestandardised to the icss weights , ranged from about 60% to around 20% in both sexes , with japan , canada , the usa , france , the netherlands , sweden , and australia at the upper end of the range , and algeria , estonia , poland , and slovakia at the lower end ( table 2 and gure 3 )  . the 5 - year survival estimates of 259% ( 95% ci 114437 ) for men and 182% ( 66346 ) for women in stif ( algeria ) were each based on 30 patients , and were not age - standardised because data were too sparse in some age groups . 5 - year relative survival in goinia , brazil , was 493% in men and 384% in women . 
5 - year survival in cuba was 592% in men and 628% in women , based on analysis of about 700 patients 746 vol 9 august 2008 cuba france austria canada malta australia japan spain germany netherlands iceland sweden finland norway italy northern ireland denmark ireland scotland portugal england slovakia slovenia estonia wales czech republic brazil poland algeria france cuba australia canada sweden japan norway netherlands finland malta ireland germany spain italy iceland scotland denmark england austria portugal northern ireland wales czech republic brazil slovenia slovakia estonia poland algeria colon ( women ) colon ( men ) rectum ( women ) rectum ( men ) 402 493 399 japan cuba australia france austria canada finland spain netherlands sweden italy germany norway ireland portugal iceland northern ireland scotland denmark england slovakia wales estonia malta czech republic slovenia brazil poland algeria cuba japan netherlands australia canada sweden france iceland norway spain finland brazil northern ireland germany italy austria denmark portugal scotland ireland england wales malta slovenia estonia czech republic poland slovakia algeria 5 - year relative survival ( % ) 5 - year relative survival ( % ) africa america , central and south america , north asia europe oceania data covering less than 100% of country vol 9 august 2008 394 497 385 articles figure 3 : 5 - year relative survival ( % ) , agestandardised to the icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the colon or rectum during 199094 and followed up to dec 31 , 1999 : country vertical bar on the right of each graphic shows the contribution ( % ) of each continent to the total number of cases analysed ( contributions under 1% are not labelled )  . 
 * age - standardised to icss weights , except for stif , algeria ( all cancers ) , austria ( rectum [ women ] ) , iceland ( rectum [ men and women ] ) , ireland ( rectum [ women ] ) , malta ( colon [ men ] and rectum [ men and women ] ) , which were unstandardised values ( see text )  . 
 articles in each sex , although 782 ( 36% ) patients had been excluded as dco ( available online34 )  . in canada , the pooled estimate of 5 - year survival was 587% for women and 531% for men , slightly lower in the global range than for cancers of the breast , colon , or prostate in canada . 
in the usa , 5 - year relative survival for all races combined was 569% in men and 598% in women , with a range from 4667% in men and 5266% in women ( table 2 and gure 2 )  . 
by contrast with colon cancer , survival from rectal cancer was slightly higher in women than in men . 5 - year survival for rectal cancer in the usa was generally lower for blacks than for whites , in both sexes ( web gure 4 )  . 
 the overall estimate of 5 - year survival in men was 474% for blacks and 573% for whites ; for women , the estimates were 494% for blacks and 604% for whites ( table 3 )  . 
 when survival for blacks was above 60% , or higher than for whites in the same population ( colorado , connecticut , nebraska , rhode island ) , the estimates for blacks were based on around 50 or fewer patients , with wide cis , and were usually not age - standardised ( table 3 and web gure 4 )  . 
 even where blacks comprised 25% or more of the population ( atlanta , ga , detroit , mi , new york city , ny , louisiana ) , 5 - year survival was 616% lower than for whites in the same area . 
the pooled estimate of 5 - year survival in areas covered by npcr was 563% for men and 588% for women , some 23% lower than for seer areas ( 585% men , 618% women ; table 3 and gure 2 )  . 5 - year survival ranged from 462% to 679% in whites ; in blacks , the range of age - standardised survival was from 428% to 635% ( table 3 and web gure 4 )  . 
survival for whites was also generally within the control limits , with the exception of new york city , ny , where survival was below the control limits ( web gure 3 )  . in japan , the pooled survival estimate for colon cancer was 582% for men and 576% for women , although survival was lower in osaka ( 5455% ) than in fukui or yamagata ( 6064% ; table 2 and gure 3 )  . in europe , the geographical pattern for age - standardised 5 - year survival was similar to that for colon cancer . 
for men , the range was from 2830% in poland , west bohemia ( czech republic ) , and slovakia to 5355% in france , sweden , and the netherlands ; whereas for women , the range was from 3032% in poland , estonia , and slovakia up to 639% in france , where three of the four contributing registries ranked the highest in europe ( table 2 and gure 3 )  . 
the estimate for women is not age - standardised , but it is based on over 200 patients ( table 1 ) , and similarity between the raw and standardised estimates for cancers of the colon and colon and rectum combined ( less than 1% , data not shown ) suggests that an age - standardised estimate for rectal cancer would not have been very di erent . 
in northern ireland , the estimates were 482% in men and 438% in women ( pooled uk estimates were 406% in men and 453% in women ; table 2 )  . the national estimate of age - standardised 5 - year survival for rectal cancer in australia was 548% in men and 592% in women . 
survival ranged from 4557% in men and from 5561% in women . of 663 621 men with prostate cancer , 35 934 ( 5% ) were ex cluded for a previous cancer , leaving 627 687 eligible rst , primary , invasive cancers of the prostate ( available online34 )  . 
 after 11 163 ( 2% ) exclusions for dco , 1640 ( < 1% ) for autopsy - detection and 801 for major error , 614 083 men were included in the analyses ( 98% of those eligible )  . 
less than 1% of men were censored from the analysis within 5 years of diagnosis , but 32% died within 1 month of diagnosis . ( < 1% ) 5 - year relative survival , age - standardised to the icss weights , ranged from 80% or higher in the usa ( 92% ) , canada and austria to less than 40% in denmark , poland , and algeria ( table 2 and gure 1 )  . the 5 - year survival estimate of 214% ( 95% ci 87389 ) in stif ( algeria ) was based on 36 patients , and was not age - standardised . in brazil , 5 - year survival was 344% in campinas and 557% in goinia . 
notably , 20 ( 134% ) men in campinas and 71 ( 218% ) men in goinia died within 1 month of diagnosis , which are the highest proportions of any of the participating registries ( available online34 )  . 
this estimate was based on 4300 patients , but 54% of the original data set of 9500 patients had been excluded as dco ( table 1 and data available online34 )  . the pooled estimate of 5 - year survival for prostate cancer in canada was 851% , ranging from 775% in saskatchewan to 893% in british columbia ( table 2 and gure 1 )  . 
in the usa , 5 - year relative survival from prostate cancer was 919% for all races combined , with a range from 816% in new york city , ny up to 950% in seattle , wa ( table 2 and gure 2 ) , but most of the estimates were within a fairly narrow range , from 886% ( louisiana ) to 940% ( atlanta , ga )  . 
the relative survival estimate for the state of michigan was 100% , although in the city of detroit , mi , with 42% of the state population ( webtable ) , survival from prostate cancer in the same period was 938% . age - standardised 5 - year relative survival for prostate cancer in blacks was lower than for whites in all 748 vol 9 august 2008 articles populations for which this could be separately assessed with race - speci c life tables ( web gure 2 )  . 
the di erence in survival between blacks and whites ranged from 50% ( florida ) to 1416% ( nebraska , rhode island ) , and although the largest di erences arise where the black populations are smallest , each survival estimate was based on at least 70 patients ( webtable )  . 
the pooled estimate of 5 - year survival was 895% in areas covered by npcr , and 931% in seer areas ( table 3 )  . survival in blacks was usually lower than the pooled us estimate , and often more than three standard deviations below it , after controlling for precision ( web gure 3 )  . 
 5 - year survival for whites was above the upper 998% control limit in three seer populations ( atlanta , ga , seattle , wa , and detroit , mi )  . 
in new york state , including new york city , ny , survival estimates are precise , but 69% below the pooled us estimate of 923% and well below the lower control limit ( web gure 3 )  . the 5 - year relative survival estimates for michigan state ( 100% in both blacks and whites ) were too high , and they are not shown in web gure 3 , although the data were included in the pooled estimate . 
information about the death had not been linked to the tumour record for some of the apparent 5 - year survivors from prostate cancer in michigan state , leading to an in ated estimate . 
this error did not a ect the survival estimates for prostate cancer in detroit , mi or those for other cancers in michigan state . the pooled estimate of 5 - year survival in japan was 504% , much lower on the global scale than for cancers of the breast , colon , or rectum in japan . 
survival estimates were similar in all three prefectures ( table 2 and gure 1 )  . the range of 5 - year survival in europe was especially wide for prostate cancer , from less than 40% in poland and denmark to more than 80% in austria ( table 2 and gure 1 )  . 
data were not available for nine registries : switzerland ( ve registries ) , isre and cte dor ( france ) , granada ( spain ) , and northern netherlands . 
in northern ireland , the estimate was 540% , slightly higher than the pooled estimate of 511% for the uk ( table 2 )  . the national estimate of age - standardised 5 - year survival for prostate cancer in australia was 774% . 
 survival was closely similar in the six largest states , in the range 7680% , but notably lower in the two smallest regions : 637% ( based on 78 patients , estimate not age - standardised ) and 702% in tasmania ( 1321 patients )  . in northern territory discussion to our knowledge , the concord study is the rst attempt to provide directly comparable data on cancer survival from many countries around the world by use of central qualitycontrol procedures , standard analytic methods , and a single , centralised analysis of individual tumour records from population - based cancer registries . 
cancer - mortality statistics have often been used for international comparisons of progress against cancer , 6872 but they are also a ected by wellknown problems of comparability , both between countries and between successive revisions of the icd.7275 the ndings presented here should help joint consideration of trends in incidence , survival , and mortality as indicators of cancer control . 
none of these indicators is perfect , but none is adequate on its own.7678 around 2800 life tables were created to enable the estimation of relative survival by age , sex , country , and race.46 the life tables are available on the concord website.34 5 - year relative survival for breast , colorectal , and prostate cancers was generally higher in north america , australia , japan , and northern , western , and southern europe , and lower in algeria , brazil , and eastern europe . exclusions for a previous cancer ( 59% ) were not unexpected . 
population - based cancer survival analyses are usually restricted to patients with a rst , primary invasive cancer , therefore , to the extent that patients with a previous cancer have been completely excluded in this study , this improves the comparability of the ndings with other studies . 
the data from newer registries are more likely to include unrecognised second and subsequent cancers , because any previous cancer ( s ) in a given patient might have been diagnosed before the registry began operation . the main indices of data quality for cancer survival are the proportions of registered patients known to the registry by dco , or lost to follow - up , and histologically veri ed . 
the overall proportion of patients who died within 1 month of diagnosis was low for breast cancer ( 23% ) and prostate cancer ( 32% ) , but higher for colon ( 109% ) and rectal cancers ( 78% )  . 
fewer than 1% of patients were censored from the analysis within 5 years of diagnosis . three registries were excluded after quality control , because of high losses to follow - up or ine cient regional or national linkage of information on the deaths of patients with cancer . 
the data for three other registries , cuba , campinas ( brazil ) and , for prostate cancer , michigan state vol 9 august 2008 articles ( usa ) , are less reliable than those from other registries , although for di erent reasons , discussed below . 
as with the rst global compilation of cancer incidence data , in the 1960s , retention of the two registries from central and south america was partly prompted by the paucity of information on cancer survival from that region : in this situation , even incomplete data have value.64 overall , the exclusion of dco registrations accounted for only 1% ( 9215 ) of the eligible records for breast cancer , 3% ( 13 102 ) for colon cancer , 1% ( 3213 ) for rectal cancer , and 2% ( 11 163 ) for prostate cancer ( available online34 )  . 
 sweden does not use dcos because the registration of patients with cancer at the time of diagnosis is close to 100% ; by contrast , hospitals in cuba are not allowed to retain the clinical records of deceased persons for more than 5 years.80 the di erent proportions of dco records are unlikely to explain the di erences in survival between europe and north america , however . 
the survival of patients whose tumour is registered as a dco is generally lower than the mean for all registered cancer patients , 82 so if they could have been included , the transatlantic di erences in survival would have been slightly greater . 
furthermore , most dco records in the european data are for patients aged 75 years or over , 43 where the survival di erences are in any case more marked.9 by contrast , if a high proportion of dco records is taken to suggest under - registration of long - term survivors , this might produce lower survival esti mates . 
 adjustment for both dcos and incompleteness of registration in thames ( uk ) and finland had surprisingly little e ect on survival , however , even when 1020% of registrations were dcos , because the two corrections tended to o - set one another.83 under - reporting of incident tumours by up to 5% has been shown not to a ect international comparisons of survival greatly.84 a plateau was imposed on the relative survival curve at some point during the rst 5 years after diagnosis in about 7% of the 6500 age - speci c survival estimates by registry , cancer , sex , and race ( data not shown )  . 
the e ect on the age - standardised survival estimates at national level was almost always less than 1% . diagnostic variability between pathologists might contribute to international di erences in cancer survival . 
severe cytological or architectural changes con ned to the mucosa ( in situ or intramucosal carcinoma ) have no metastatic potential , and are often labelled high - grade dysplastic adenoma . 
japanese pathologists rely more on cytological features , however , and do not consider evidence of invasion into the submucosal layer as a mandatory requirement for the diagnosis of colorectal carcinoma.85 pathological practice on this issue might vary substantially between western pathologists . 
islands of dysplastic tissue might also be displaced or herniated beyond the muscularis mucosae without implying invasive potential ( pseudo - invasion ) , and di erential diagnosis can be very di cult.86 , 87 assessment of the extent to which international survival di erences might be attributable to di erences in the pathological de nition of disease would need blinded review of pathological diagnoses of a sample of patients by an international panel of expert pathologists . 
survival in stif was similar to or even lower than survival in blacks diag nosed during 199397 in harare , the zimbabwean capital , where the very low survival was attributed to inade quate access to facilities for early diagnosis , clinical investigation , and treatment.89 survival in the two brazilian registries was generally low , although rectal - cancer survival in goinia was close to the european mean . 
data quality issues prevented the inclusion of data from three of the 20 population - based registries in state capitals : these registries should be used to provide a broader picture of cancer survival in brazil . 
 relative survival reported here for patients with cancer diagnosed in cuba during 199094 was about 20% higher than estimates for those diagnosed during 198889 , just a few years earlier.80 cancer survival for children diagnosed in cuba during 198889 was lower than in more developed countries.90 the high proportion of dcos in the 198889 data was considered less likely to be biased with respect to survival than in other registries , because of the way data were collected , 80 but the survival estimates for cuba reported here are still likely to be considerably in ated , and should be interpreted accordingly . national estimates of survival for patients with cancer diagnosed in japan during 199396 were slightly higher than the estimates for 199094 reported here.79 they were based on data from seven prefectures , including the three reported here ( yamagata , fukui , and osaka )  . 
as in the concord data , survival in osaka was generally lower than the mean survival for japan . variation in survival between the provinces of canada and the states and territories of australia was generally small , and overall survival was high : this suggests health care of a high standard in most areas . 
variation between the countries of europe was much wider . 750 vol 9 august 2008 articles the substantial di erences in survival between australia and the uk have been noted before.91 they are unlikely to be because of di erences in data quality . 
more e ective treatment in australia is a plausible explanation.92 comparisons of cancer survival between europe and the usa since 2000 have identi ed wide di erences , with survival usually higher in the usa.9 closer assessment of these di erences with more detailed data , not routinely collected by all registries , has enabled the explanatory e ect of clinical variables such as stage at diagnosis , investigative approach , anatomical site , and morphology to be quanti ed for colorectal cancer12 , 93 and breast cancer , 10 and for a range of cancers in children.11 in those studies , the usa has always been represented by data from the seer program registries , representing some 10% of the us population at that time , because no other data have been available . 
the availability of data from a large number of state - wide population - based cancer registries that began oper ation around 1990 , and meet data quality standards comparable with those of the seer registries , now enables a larger proportion of the us population to be included in national and international comparisons of cancer survival . 
the concord study provided the rst opportunity for the cancer registries of 11 us states in the npcr to follow up all their patients for vital status and to undertake analyses of cancer survival , and 42% of the us population is included in these analyses . the survival di erences between us and european patients with cancer , especially in the oldest patients , seem unlikely to be attributable to artefacts of cancer registration . 
 the concord study has nonetheless identi ed two methodological issues that probably do explain some of the well - known di erences in survival between europe and the usa , from which only seer data have been available until now . first , relative survival was about 24% higher in seer - 9 areas than in participating npcr areas of the usa . 
 consequently , cancer survival in the 42% of the us population covered by the concord study was 13% lower than survival in the seer areas alone ( 10% of the us population )  . 
direct estimation of cancer survival for other areas of the usa would be desirable . second , census - derived us national life tables give higher estimates of all - cause mortality than are noted in the seer areas , especially with the gradual decline of mortality in the decade after a census.46 use of censusderived national life tables to estimate relative survival ( the seer approach ) therefore produces estimates that are almost always higher than those obtained with statespeci c life tables for each calendar year in the decade ( concord approach ) , which we believe to be more appropriate because it provides tighter control for changes over time in background mortality . 
with the concord approach , age - standardised 5 - year survival in the 22 participating areas of the usa was up to 3% lower than with the seer approach for breast cancer in women , up to 4% lower for colorectal cancer , and up to 5% lower for prostate cancer ( available online34 )  . the di erences in cancer survival between blacks and whites of both sexes in the usa are large , and remarkably consistent in 16 states and six metropolitan areasmore populations than it has been possible to study in the past.94 the di erences were adjusted for age and for di erences in background mortality between blacks and whites within each state or metropolitan area . 
it would be interesting to know if the di erences were attributable to artefact , or di erences between blacks and whites in tumour biology , in stage at diagnosis , in access to health care , or in compliance with treatment . 
the blackwhite di erences in relative survival that we report would have been even larger if we had used race - speci c national life tables instead of racestate life tables , because back ground mortality is higher ( and expected survival lower ) in blacks than in whites in all the populations studied.23 , 95 survival from cancers of the breast , colorectum , and prostate varied with the type of health insurance in a population - based study : 96 survival was highest in patients who had private insurance , intermediate with federal insurance , and lowest with no insurance . 
late stage , 98 less treatment , and higher mortality seem to be associated with black race , low socioeconomic status , and poor survival in the usa.99101 extensive reviews have led to the conclusion that racial disparities in cancer treatment , which are not explained by clinical factors , lead to worse outcomes in blacks.102 , 103 analysis of seer data suggested that some racial di erences in treatment and cause - speci c survival persist after adjustment for poverty.104 by contrast , the racial di erence in survival from colorectal cancer was almost absent in patients managed under the equal - access , integrated health - care veterans a airs system.105 finally , overviews of race , socioeconomic status , and cancer outcomes strongly suggest that equal treatment yields equal outcome , irrespective of race.53 , 106 the data presented here extend the evidence that cancer survival in the usa is lower in blacks than in whites . simple ranking of countries by overall survival can be misleading . 
survival is very similar in many european countries , at the centre of the global range , and a small shift in the survival estimate in either direction can entail a large change in the rank . 
thus , even the national survival estimates for iceland and malta have wide con dence intervals and unstable rankings because they are based on populations of around 250 000 ( gures 1 and 3 )  . 
the detailed data by country and region are tabulated by continent , country , and region , rather than ranked : some vol 9 august 2008 articles estimates , based on sparse data , could not be agestandardised ( table 2 )  . the numbers of patients included in the analysis varied widely , as did the proportion of the national population covered by the data . 
population coverage of participating registries in italy was about 15% , but they were concentrated in the wealthier north of the country.22 , 30 the same point also applies to the usa , however , because the data presented here con rm suggestions107 that cancer survival in the seer program areas ( 10% population coverage during the 1990s ) was higher than in other parts of the country . 
similarly , survival for 199094 in the four french dpartements reported here ( 6% national coverage ) was high on the european scale for most cancers , 27 and a much larger study for the same period in 14 dpartements ( 20% coverage ) showed similar patterns of survival.108 , 109 for countries with more than one contributing registry but less than 100% population coverage , we have presented estimates of survival derived from the pooled data , not weighted means of the regional estimates of survival . 
the question of whether pooled survival estimates derived from regional registries with less than 100% national coverage can properly be considered representative of cancer survival in the whole country has been discussed else where.22 if population - based estimates of cancer survival are deemed reliable , however , they do suggest a poten tially achievable level of survival , irrespective of whether the estimate is for a whole country or only one region in that country . 
the proportionate contributions from each continent to the concord study are very di erent from the worldwide distribution of cancers of the breast , colon , rectum , and prostate . 
the national data for australia alone represented 63% of the population of oceania in 1995 , 111 and the survival estimates for north america included 44% of the combined populations of usa and canada around 1992 , but for africa , asia , and south america , the population coverage of these data was much lower . 
the survival data for europe were based on 25% of the continental population of 512 million in 1992 , 112 but the eurocare study ( ongoing since 1989 ) is the largest and most widely cited international study of cancer survival , and all 57 cancer registries in that study , and six others , contributed to concord . 
to provide an international summary measure of cancer survival for visual comparison , we therefore used the overall estimates for 23 countries in eurocare - 3 , but age - standardised to the icss weights used in concord , instead of the weights used in eurocare - 3.113 we have presented pooled estimates of survival for europe and north america ( table 3 ) , but not for other continents . the size of the population covered by the data a ects the statistical precision of the survival estimates . 
this is shown by 95% cis , but ranked graphics do not provide visual appreciation of the extent to which the survival estimate for a given country or region falls outside the distribution of survival estimates that might be expected , under the hypothesis that survival should be the same in all areas . 
we used funnel plots62 to provide that visual e ect for geographical and racial variation in survival in the usa , with the target value as the pooled estimate for the usa , age - standardised to the icss weights.60 these plots display striking geographical and racial variation in survival . clinical practice has continued to evolve in the 15 years or so since the patients included in this study were diagnosed . 
changes in diagnosis , screening , and treatment have undoubtedly improved the prognosis for cancer patients , at least in wealthier countries . survival has increased substantially for cancers of the breast ( women ) , colon , rectum , and prostate in the 17 areas of the usa covered by the seer program during 19962003 , 114 and in canada ( 199698 ) 115 and australia ( 19942004 ) .116 , 117 smaller increases have been reported in 11 of the 47 japanese prefectures.118 these estimates of relative survival , published for national purposes , cannot be compared with the data reported here , however , because of di erences in the quality control of incidence data or completeness of follow - up , and in methods of analysis . 
 some estimates were not age - standardised for international comparison , whereas others were standard ised to countryspeci c age weights , rather than the icss age weights that we used . the only recent international study of cancer survival is eurocare - 4 , which included patients diagnosed in 23 countries during all or part of 19952002 and followed up to 2003.29 , 30 survival increased substantially in eastern european countries , where it was much lower than in other parts of europe during 199094 . 
the rise in breast cancer survival in several countries was associated with a fall in mortality , possibly because of improved care and screening programmes ; the rise in prostate - cancer survival ( and incidence ) might be a result of more widespread psa testing . 
in western europe , survival in the uk and denmark was still low for several cancers in the late 1990s . concord is , by chance , reasonably well - timed to provide a baseline for international comparisons of cancer survival to assess the e ect of several major public health initiatives for the control of breast , 752 vol 9 august 2008 articles screening for breast colorectal , and prostate cancers . 
at that time , intense early diagnostic activity with prostate - speci c antigen ( psa ) had recently become widespread in the usa , but was little used elsewhere . 
in denmark , for example , the 50year increase in prostate cancer incidence is considered real , 119 but the danish society for urology assessed the evidence in 1990120 and decided not to advocate psa testing in asymptomatic men , because the therapeutic bene t was very small ; 121 only sympto matic patients were o ered treatment . 
mass screening for colorectal cancer with faecal occult blood ( fob ) testing or endoscopy had not begun during 199094 in any contributing country as far as we are aware . 
opportunistic screening with the fob test began in japan in 1992 ; by 2004 , about 20% of people aged 40 years or over had been tested within the previous year.122 opportunistic endoscopy had already become widespread in some parts of the us population by 1990 . the concord study was planned in three phases . 
the study reported here ( phase i , low resolution ) was designed to quantify international di erences in population - based relative survival by age , sex , country , or region for patients diagnosed during 199094 with a cancer of the breast , colon , rectum , or prostate . 
phase ii ( high resolution ) was designed to help interpret those international di erences in survival , by use of a subset of registries that could reabstract detailed clinical data , including stage at diagnosis and treatment , from the original medical records for large random samples of patients diagnosed with one of the same cancers during 199698 . 
phase iii was designed as a blinded , expert review of the pathological diagnosis for a subset of patients from the phase ii study , to assess the extent to which international survival di erences might be attributable to di erences in the pathological de nition of disease in participating countries . the range of survival estimates for each cancer is very wide . 
population - based cancer registries are increasingly important in the comparative assessment of cancer outcomes , 123 and even allowing for di erences in data quality or statistical robustness , there is little doubt that the chances of survival after a cancer diagnosis vary hugely on a global scale . the comparability of cancer survival estimates between countries is criticised far more often than the comparability of cancer incidence data from the same registries . 
cancer survival is a measure of the overall e ectiveness of cancer treatment services , whereas cancer incidence is a measure of the long - term e ect of prevention policies , which are less visible on a day - to - day basis and can , incorrectly , be seen as less important . cancer survival is a valuable indicator for international comparison of progress in cancer control , 76 , 124 , 125 despite the fact that part of the variation in cancer survival identi ed in this study could be attributable to di erences in the intensity of diagnostic activity ( casending ) in participating populations . 
if overdiagnosiswhich depends on diagnostic intensityis more marked in one country than another , then it will certainly be harder for researchers to compare incidence , mortality , and survival in those countries . 
in each country , the health - care system will have to be funded , sta ed , and equipped to cope with the diagnostic and therapeutic burden of all patients with cancer , however they are diagnosed . 
the health - care system must make provision accordingly , and monitor the outcome of that provision ; cancer survival is one such overall indicator . furthermore , a patient with cancer is still a patient with cancer , whether or not they represent over - diagnosis . 
as it is , a cancer diagnosis represents the best that medicine has to o er in a given country at a given time , and that best is variable . 
no matter how a patient with cancer is diagnosed , they have to cope with the consequences , both psychological and physical , and will usually want to be treated . 
in this sense , cancer incidence and survival estimates describe as accurately as possible the occurrence and the outcome , respectively , of cancer as it is diagnosed and treated at a given time in a given population . most of the wide global range in survival is probably attributable to di erences in access to diagnostic and treatment services.3 , 82 , 89 , 91 , 126 international variation survival in europe has been associated with national levels of economic development , as measured by total national expenditure on health.29 survival is positively associated with gross domestic product and the amount of investment in health technology such as ct scanners.124 part of the international variation is thus probably attributable to under - investment in health resources.127 , 128 the variation in survival might be considered intuitively obvious , given wide global variation in expenditure on health care , whether that is expressed in absolute terms or as a proportion of national resources . 
a parallel could be drawn with di erences in survival between rich and poor patients with cancer in a given country , which have frequently been reported.129 , 130 in survival until now , however , direct international comparisons of cancer survival between high - income and low - income countries have not generally been available . 
rc , sf , rda , msantaquilani , mq , gg , msant , fb , jml , th , sk , and av were involved in data preparation and quality control . 
all authors revised the report . con icts of interest the authors declared no con icts of interest . acknowledgments we are grateful to the many cancer registry sta around the world whose meticulous and sustained e orts at data collection , linkage , and quality control have enabled the survival of patients to be analysed and compared in this study . 
we thank dee bhakta and adrian cousins ( london school of hygiene and tropical medicine , london , uk ) for help in undertaking the pilot study and for producing web gure 1 , respectively . 
the ndings and conclusions in this report are those of the authors and do not necessarily represent the views of the us cdc . adjuvant capecitabine in combination with docetaxel and cyclophosphamide plus epirubicin for breast cancer : an open - label , randomised controlled trial heikki joensuu , pirkko - liisa kellokumpu - lehtinen , riikka huovinen , arja jukkola - vuorinen , minna tanner , raija asola , riitta kokko , johan ahlgren , pivi auvinen , akseli hemminki , outi paija , leena helle , lauri nuortio , kenneth villman , greger nilsson , sirpa - liisa lahtela , kaisa lehti , marjo pajunen , paula poikonen , paul nyandoto , vesa kataja , petri bono , mika leinonen , henrik lindman , on behalf of the finxx study investigators summary background standard adjuvant chemotherapy regimens for patients with moderate - to - high - risk early breast cancer typically contain a taxane , an anthracycline , and cyclophosphamide . 
we aimed to investigate whether integration of capecitabine into such a regimen enhances outcome . methods in this open - label trial , we randomly assigned ( centrally by computer ; strati ed by node status , her2 status , and centre ) 1500 women with axillary node - positive or high - risk node - negative breast cancer to either three cycles of capecitabine and docetaxel followed by three cycles of cyclophosphamide , epirubicin , and capecitabine ( capecitabine group , n = 753 ) , or to three cycles of docetaxel followed by three cycles of cyclophosphamide , epirubicin , and uorouracil ( control group , n = 747 )  . 
after a median follow - up of 35 months ( iqr 255436 ) , recurrence - free survival at 3 years was better with the capecitabine regimen than with control ( 93% vs 89% ; hazard ratio 066 , 95% ci 047094 ; p = 0020 )  . 
more patients discontinued planned treatment in the capecitabine group than in the control group ( 178 / 744 [ 24% ] vs 23 / 741 [ 3% ] )  . 
 four patients in the capecitabine group and two in the control group died from potentially treatment - related causes . interpretation the capecitabine - containing chemotherapy regimen reduced breast cancer recurrence compared with a control schedule of standard agents . 
 introduction adjuvant chemotherapy consisting of an alkylating agent , an anthracycline , and a taxane is typically administered for early breast cancer , although the regimens used can vary considerably.13 results from a few large randomised trials and a meta - analysis suggest that addition of a taxane to adjuvant regimens containing an anthracycline improves disease - free and overall survival.46 despite such advances in chemotherapy , many women diagnosed with early breast cancer still eventually succumb to the disease . 
main exclusion criteria were : presence of distant metastases ; node - negative mucinous , papillary , medullary , or tubular disease ; clinically signi cant cardiac disease ; and previous neoadjuvant chemotherapy . 
study safety was monitored by an independent data safety monitoring committee . 1500 enrolled and underwent randomisation for the trial protocol see 753 assigned to capecitabine group 747 assigned to control group 1 withdrew consent 1 had distant metastases 1 withdrew consent 1 had distant metastases 751 included in intention - to - treat population 744 included in safety population ( received 745 included in intention - to - treat population 741 included in safety population ( received study treatment ) 566 completed study treatment 1 had cancer recurrence 169 had adverse events 4 withdrew consent 4 discontinued for other reasons study treatment ) 718 completed study treatment 3 had cancer recurrence 19 had adverse events 0 withdrew consent 1 discontinued for other reasons 54 had cancer recurrence or died 80 had cancer recurrence or died 27 died 18 died from breast cancer 41 died 35 died from breast cancer figure 1 : trial pro le 1146 the study generated randomisation and masking we randomly assigned patients ( centrally and with computer - assisted masking ) , in a 1 : 1 ratio , to receive either a capecitabine - containing chemotherapy regimen ( capecitabine group ) or a control schedule . 
we did randomisation with permutated blocks : block size ( two , four , or six ) varied at rando we strati ed women at random allocation according to the number of axillary lymph nodes that contained cancer ( 3 vs > 3 ) , her2 status ( negative vs positive ; ascertained by either immunohistochemistry or in - situ hybridisation ) , and centre . 
a trained study nurse communicated the randomisation result to study sites by fax . procedures patients allocated to the capecitabine group received capecitabine ( 900 mg / m twice a day , days 115 ) plus docetaxel ( 60 mg / m as a 1 - h intravenous infusion on day 1 of every 3 - week cycle ) , followed by cyclophosphamide ( 600 mg / m on day 1 ) , epirubicin ( 75 mg / m on day 1 ) , and capecitabine ( 900 mg / m twice a day , days 115 , every 3 weeks )  . 
those assigned control received docetaxel ( 80 mg / m as a 1 - h intravenous infusion on day 1 of every 3 - week cycle ) followed by cyclophosphamide ( 600 mg / m ) , epirubicin ( 75 mg / m ) , and uorouracil ( 600 mg / m ) , all administered on day 1 of every 3 - week cycle . 
in the capecitabine group , the rst capecitabine dose of every cycle was given in the evening of day 1 and the last dose was administered on the morning of day 15 , followed by a 7 - day rest period . 
if they developed a second grade 2 event , or their rst grade 3 event , we terminology criteria vol 10 december 2009 articles stopped chemotherapy and , after resolution to grade 01 , resumed it at 80% of the starting dose . 
 when scheduled treatment was discontinued for toxic e ects , we replaced agents as follows : capecitabine and docetaxel by cyclophosphamide , epirubicin , and capecitabine , or cyclophosphamide , epirubicin , and uorouracil ; single - agent docetaxel by cyclophosphamide , epi rubicin , and uorouracil ; and cyclo phosphamide , epirubicin , and capecitabine by cyclophosphamide , epirubicin , and uorouracil , or cyclophosphamide and epirubic we regarded staging examinations ( chest ct or radiography ; bone scan ; and abdominal ct , mri , or ultrasound ) as mandatory at screening for patients with four or more positive axillary nodes , 15 , 16 but these procedures were undertaken at the discretion of the investigator for all other patients . 
we scheduled follow - up of study participants for a minimum of 5 years after randomisation . the primary endpoint was recurrence - free survival , de ned as the time between randomisation and date of diagnosis of invasive breast cancer recurrence , or death if the patient died before cancer recurrence . 
based on this assumption , a total of 205 events and 1500 patients were needed to achieve 80% power , assuming a 3% annual dropout rate , when = 0028 ( two - sided )  . 
to maintain a signi cance level of 5% , we set the signi cance level in interim and nal analyses at 0028.17 the interim analysis had 80% power to detect an improvement from 890% to 935% ( hr 058 ) after median follow - up of 3 years in 1500 patients ( = 0028 , two - sided testing ) and when about 120 recurrences had happened . 
suicide and depression ; suicide and intoxication ; unknown ; unknown ( breast cancer unlikely ) ; pulmonary embolus ; septicaemia , colitis , and multiorgan failure ; acute myocardial infarction ; alcohol intoxication ; cardiac and pulmonary failure . 
pulmonary embolus ( n = 2 ) ; septicaemia ; septic shock ; amyotrophic lateral sclerosis ; subdural haemorrhage . table 2 : breast cancer recurrence and survival in the modi ed intention - to - treat population a recurrence - free survival control capecitabine p = 0020 ( log rank ) number at risk control capecitabine b overall survival articles we analysed frequency tables with fishers exact test or the test , and we compared age and weight distributions with the t test . 
to compare survival between groups , we used the kaplan - meier life - table method and an unadjusted cox proportional - hazards model ; we implemented the log - rank test to con rm the robustness of the analysis . 
 results between jan 27 , 2004 , and may 29 , 2007 , 1500 patients were recruited from 15 finnish centres ( n = 1199 ) and ve swedish centres ( n = 301 )  . 
four women were excluded from the modi ed intention - to - treat population ( two withdrew informed consent before they received study treatments , two had overt distant metastases at the time of study entry ; gure 1 )  . 
respectively , 56 ( 7% ) and 50 ( 7% ) women received single - agent trastuzumab after discontinuation of chemotherapy for up to 12 months , 24 ( 3% ) and 21 ( 3% ) received trastuzumab concomitantly with docetaxel only , and 16 ( 2% ) and 12 ( 2% ) received plus trastuzumab single - agent trastuzumab for up to 12 months after chemotherapy . 
tamoxifen , anastrozole , and other hormonal treatments were administered , respectively , to 325 ( 43% ) , 316 ( 42% ) , and 29 ( 4% ) patients assigned to the capecitabine group , and to 287 ( 38% ) , 328 ( 44% ) , and 27 ( 4% ) women allocated to the control group . concomitantly with docetaxel at the time of data lock ( aug 31 , 2008 ) , median follow - up was 35 months ( iqr 255436 )  . 
134 events ( deaths , distant or local relapses ) had happened , 54 ( 7% ) in the capecitabine group and 80 ( 11% ) in the control group , which triggered the interim analysis . 
the hazard ratio for the capecitabinerecurrence - free survival favoured number at risk control capecitabine p = 0089 ( log rank ) years after randomisation figure 2 : kaplan - meier estimates of 3 - year recurrence - free and overall survival in the modi ed intention - to - treat population 1148 vol 10 december 2009 articles 070 ( 048101 ) 047 ( 018125 ) 081 ( 051129 ) 052 ( 031088 ) 060 ( 037096 ) 077 ( 046127 ) 156 ( 078314 ) 049 ( 033075 ) capecitabine group control group patients events patients events hazard ratio ( log scale ) hazard ratio ( 95% ci ) who performance status positive axillary nodes oestrogen receptor status 03 positive negative her2 status positive negative 661 547 204 580 171 146 605 662 537 208 563 182 139 606 capecitabine better control better figure 3 : forest plot of exploratory subgroup analyses for recurrence - free survival containing regimen ( 066 , 95% ci 047094 ; p = 0020 ; table 2 ; gure 2 )  . 
in the capecitabine group , three women developed invasive contralateral breast cancer and six had other cancers , compared with two and eight patients , respectively , in the control group . 
disease - free survival ( which includes invasive contralateral breast cancers and second cancers ) was longer in the capecitabine group than in the control group ( 068 , 049094 ; p = 0020 )  . 
when patients treated with trastuzumab were excluded from the main analysis , the hazard ratio for recurrence - free survival still favoured the capecitabine - containing regimen ( 064 , 044091 ; p = 0014 )  . in exploratory subgroup analyses , recurrence - free survival was better in the capecitabine group than in the control group , with the exception of patients with her2 - positive disease ( gure 3 )  . 
in this analysis , the interaction between treatment and her2 status was signi cant ( p = 00049 ) , whereas interactions between treatment and the other subgroups shown in gure 3 were not ( p > 010 )  . 
patients who received capecitabine had more occurrences of grade 3 or 4 hand - foot syndrome , diarrhoea , nail changes , and stomatitis than did those in the control group , whereas neutropenia , febrile neutropenia , infection with neutropenia , amenorrhoea , and myalgia were more frequent in the control group ( table 3 )  . 
four patients in the capecitabine group died during chemotherapy from possibly treatment - related causes ( septic colitis ; suicide ; myocardial infarction ; unknown cause [ suspected cardiac arrhythmia ] ) and two died in the control group ( pulmonary arterial embolism ; septicaemia )  . all six planned cycles of chemotherapy were administered to 566 ( 75% ) individuals assigned the compared with capecitabine - containing 718 ( 96% ) allocated control . 
 table 3 : adverse events in safety population treatment was most frequent in the capecitabine group ( 178 [ 24% ] vs 23 [ 3% ] assigned control ; p < 00001 )  . 
of those allocated to the capecitabine group , 98 ( 13% ) discontinued during docetaxel and capecitabine cycles and a further 80 ( 11% ) during cyclophosphamide , vol 10 december 2009 1149 articles epirubicin , and capecitabine cycles . 
 58 ( 8% ) and 139 ( 19% ) patients assigned to the capecitabine and control groups , respectively , had the docetaxel dose reduced because of toxic e ects . 
including replaced cycles , most patients ( 1461 [ 98% ] ) received a total of six cycles . discussion our ndings showed enhanced recurrence - free survival for patients who received a regimen containing capecitabine in addition to docetaxel , epirubicin , and cyclophosphamide compared with women who received docetaxel , epirubicin , cyclophosphamide , and uorouracil . 
single - agent capecitabine has been compared with combination chemotherapy in the adjuvant treatment of elderly patients with breast cancer , 18 but to our knowledge , finxx is the rst adjuvant trial to report e cacy of capecitabine in combination with other agents for treatment of early breast cancer . our results suggest that integration of capecitabine upfront with potentially synergistic chemotherapeutic agents and into several cycles might be an e ective treatment strategy . 
this hypothesis is supported by data of randomised studies undertaken in the neoadjuvant setting.19 , 20 inclusion of capecitabine in the taxane and anthracycline - containing parts regimen distinguishes finxx from other trials investigating incorporation of capecitabine into adjuvant regimens . 
 findings of a randomised trial in the neoadjuvant setting indicated a 20% pathological complete response rate with and capecitabine compared with 13% in patients receiving uorouracil , epirubicin , and cyclophosphamide.21 cyclophosphamide , epirubicin , the the enhanced e cacy we recorded in the capecitabine arm was gained at the cost of increased diarrhoea and hand - foot syndrome , although febrile neutropenia was less frequent than with the control regimen , which is probably attributable to the reduced docetaxel dose . 
cardiotoxicity is a known e ect of the uoropyrimidine class of chemotherapeutic agents , and individuals receiving uoropyrimidines need to be monitored for symptoms and signs of these cardiac e ects , although cardiotoxicity might be typical with capecitabine than with infused uorouracil.22 in our study , most patients who interrupted capecitabine administration could continue treatment with other study agents and complete six cycles of chemotherapy . 
 less the control arm in our study represents a regimen frequently used in finland and sweden , which is not dissimilar to the types of regimen administered in many other countries.8 , 23 , 24 docetaxel 80 mg / m is a lower dose than the 100 mg / m2 regarded as standard in some regions . 
we selected the dose of 80 mg / m for two reasons : ( 1 ) on the basis of toxic e ects recorded with docetaxel 100 mg / m in the finher trial , leading to protocol modi cation ; 25 and ( 2 ) because no di erence in time - to - progression or survival was recorded between starting doses of 75 mg / m and 100 mg / m in the intention - to - treat population of a randomised trial of docetaxel as second - line therapy for advanced breast cancer.26 adjuvant docetaxel administered at either 80 mg / m or 100 mg / m at 3 - week intervals before three and cyclophosphamide for early breast cancer might show similar survival.27 the docetaxel dose of 60 mg / m administered in the capecitabine group is fairly low , but this amount was e ective in combination with other agents and rarely needed to be reduced . 
 of uorouracil , epirubicin , cycles our results suggest that e cacy is maintained when capecitabine is given at a dose of 900 mg / m instead of 1250 mg / m twice a day in combination with docetaxel , 12 and these data are consistent with analyses of capecitabine dose - reduction in metastatic disease.28 the hypothesis that an even lower capecitabine dose could be appropriate is being tested in an ongoing us oncology group trial , in which capecitabine is given at a dose of 825 mg / m concomitantly with docetaxel . 
 retrospective analysis of one study suggests that docetaxel plus capecitabine might be more e ective than docetaxel alone for treatment of oestrogen receptorpositive advanced breast cancer in particular , but this idea needs con rmation.29 chemotherapy - induced amenorrhoea is unlikely to account for the high e ciency of capecitabine combinations , because persistent amenorrhoea was less frequent in women allocated to the capecitabine group compared with those assigned control . 
the e ect was substantial and could be comparable to or greater than that achieved with the introduction of taxanes to adjuvant treatment of early breast cancer.6 , 30 however , this possibility needs to be con rmed in ongoing trials of adjuvant capecitabine . 
hj , rh , and hl provided administrative support . 1150 vol 10 december 2009 articles con icts of interest p - lk - l , mp , pp , and pb have received honoraria or consulting fees from roche . 
 all other authors declared no con icts of interest . acknowledgments we thank members of the independent monitoring committee ; chairman of the independent monitoring committee pertti neuvonen ; trial monitor raija husa ; medical , nursing , and clerical sta at participating centres ; and all women taking part in the finxx trial . 
 errata risk ratio lower limit upper limit z value p value risk ratio ( 95% ci ) meyer18 lee19 hull20 deitcher21 overall 0704 0509 0438 0690 0509 0121 0329 0188 0124 0351 4091 0789 1017 3832 0737 0391 3018 1920 0425 3571 0696 0003 0055 0671 < 00001 * noble sir , shelley md , coles b , et al . 
the group of patients with slow - growing tumours are clinically characterised by never - smokers or former smokers who have had little active exposure , are women , and have egfr - activating mutations . 
to improve lung - cancer outcome , we have to adopt a two - pronged approach : identify the population at risk of slow - growing tumours and target them for screening trials , while using coordinated antitobacco e orts to prevent aggressive tumours in others . 
j natl cancer inst 2005 ; 97 : 33946 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata jones lw , eves nd , haykowsky m , joy aa , douglas ps . 
the correct gure is shown . number at risk months vol 9 october 2008 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology department of radiation oncology , all india institute of medical sciences , new delhi , india sharmadn@hotmail.com the authors declared no con icts of interest . powell jw , dexter e , scalzetti em , bogart ja . 
long term results of endobronchial brachytherapy : a curative treatment ? int j radiat oncol biol phys 2007 ; 67 : 42530 . brach b , buhler c , hayman mh , joyner lr jr , liprie sf . 
 chest 2005 ; 127 : 223742 . screening newborns for tp53 in the september issue of the lancet oncology , achatz and colleagues1 discuss the possibility of screening newborns in southeast brazil for a highly prevalent tp53 mutation ( 1 : 300 individuals ) that predisposes to many cancers . 
the authors present the justi cations and the problems associated with such a screening e ort , and conclude that on the basis of current scienti c and medical knowledge the r337h mutation does not meet all the criteria for mass newborn screening . 
 in my opinion , this type of screening will never meet the criteria for newborn screening , which is intended to detect conditions for which the population is at risk but there is no other way to assess risk in newborns . 
newborn screening is done for sporadic diseases such as congenital hypothyroidism and autosomal recessive disorders , in which carrier detection is di cult or impossible , but never applies for a disorder caused by the presence of a founder dominant mutation . 
a founder mutation in a newborn will be carried by one of the parents , so the detection of the child can be done by knowing who the adult carrier is . 
cascade screening is the most economically e ective , o ering the screening test to rst - degree relatives of carriers of the mutation , and several countries have chosen this approach.2 the problem with this type of screening is that it involves the cooperation of relatives who are not always willing , and so an alternative has been the creation of databases to store information on patients.3 in my view , population screening of informed and consenting adults is much better suited for the tp53 mutation . 
 this approach identi es families at risk and has been implemented in pilot studies for haemochromatosis.4 as emphasised by achatz and colleagues , 1 such population screeningin the context of appropriate genetic counsellingallows at - risk families the informed decision of whether or not to test the probands o spring . joel zlotogora department of community genetics , ministry of health , jerusalem , israel joelz@cc.huji.ac.il the author declared no con icts of interest . achatz miw , hainaut p , ashton - prolla p . 
 clin genet 2004 ; 66 : 48387 . had eld sg , horara s , starr bj , et al ; steering group for the department of health familial hypercholesterolaemia cascade testing audit project . 
lancet oncol 2009 ; 10 : 940in this news report , the nal sentence of the 90y radioembolisation paragraph should have read only one patient experienced radiation - induced pneumonitis ; three had gastrointestinal ulcers that did not require surgical treatment , and radioembolisation - induced liver disease was noted in 24 patients ( fatal for four )  . huober j , thrlimann b . 
lancet oncol 2009 ; 10 : 102829in this re ection and reaction , the a liation for both authors should read breast center , kantonsspital st gallen , 9007 st gallen , switzerland . 
the authors would also like to thank karen price for her useful comments on the article . 1142 vol 10 december 2009 articles lancet oncol 2010 ; 11 : 53042 published online may 17 , 2010 doi : 10.1016 / s14702045 ( 10 ) 70095 - 4 see re ection and reaction page 501 * see end of paper for members and a liations . correspondence to : prof tim key , endogenous hormones and breast cancer collaborative group , cancer epidemiology unit , nu eld department of clinical medicine , university of oxford , richard doll building , roosevelt drive , oxford , ox3 7lf , uk tim.key@ceu.ox.ac.uk insulin - like growth factor 1 ( igf1 ) , igf binding protein 3 ( igfbp3 ) , and breast cancer risk : pooled individual data analysis of 17 prospective studies the endogenous hormones and breast cancer collaborative group * summary background insulin - like growth factor 1 ( igf1 ) stimulates mitosis and inhibits apoptosis . 
some published results have shown an association between circulating igf1 and breast - cancer risk , but it has been unclear whether this relationship is consistent or whether it is modi ed by igf binding protein 3 ( igfbp3 ) , menopausal status , oestrogen receptor status or other factors . 
 the endogenous hormones and breast cancer collaborative group was established to analyse pooled individual data from prospective studies to increase the precision of the estimated associations of endogenous hormones with breastcancer risk . methods individual data on prediagnostic igf1 and igfbp3 concentrations were obtained from 17 prospective studies in 12 countries . 
the odds ratios ( ors ) with 95% cis of breast cancer associated with increasing igf1 concentrations were estimated by conditional logistic regression in 4790 cases and 9428 matched controls , with strati cation by study , age at baseline , and date of baseline . 
all statistical tests were two - sided , and a p value of less than 005 was considered signi cant . findings igf1 concentrations , adjusted for age , were positively associated with height and age at rst pregnancy , inversely associated with age at menarche and years since menopause , and were higher in moderately overweight women and moderate alcohol consumers than in other women . 
the ors for a di erence in igf1 concentration between the highest and lowest fth were 138 ( 95% ci 114168 ) for oestrogen - receptor - positive tumours and 080 ( 057113 ) for oestrogen - receptor - negative tumours ( p for heterogeneity = 0007 )  . interpretation circulating igf1 is positively associated with breast - cancer risk . 
 oestrogens are important in the aetiology of breast cancer , and there is laboratory evidence for crosstalk in cells between the signalling pathways for oestrogens and igf1.24 it is therefore important to examine whether the association of igf1 with breast - cancer risk varies according to the oestrogen - receptor status of the tumour or circulating concentrations of oestradiol . 
 around 99% of igf1 circulates bound to igf binding proteins , with most bound to igf binding protein 3 ( igfbp3 ) in a ternary complex with an acid labile subunit . 
less than 1% of igf1 circulates unbound.1 most the endogenous hormones and breast cancer collaborative group was established to do pooled analyses of individual data from prospective studies to increase the precision of the estimated associations of endogenous 530 vol 11 june 2010 articles hormones with breast - cancer risk.25 in this study we undertook a collaborative analysis of data from 17 studies to investigate the associations of igf1 and igfbp3 with breast - cancer risk . 
we also examined consistency between studies , associations in subgroups including menopausal status at blood collection and oestrogen receptor status , the e ects of adjustment of igf1 and igfbp3 for each other and for other risk factors , and the joint associations of igf1 , oestradiol , and testosterone with breast cancer risk in postmenopausal women . methods data collection studies were eligible for the collaborative analysis if they had prospectively collected blood samples and data on circulating igf1 , igfbp3 , and breast - cancer risk . 
 potentially eligible studies were through pubmed using the terms igf1 , igfbp3 , and breast identi ed cancer , by searching the reference lists of identi ed studies , and by correspondence with study investigators . 
samples taken 07 : 3009 : 00 130c 130c 80c 80c originally a case - cohort study ; matched sets created for this analysis same year of birth same year of birth same month and year time of day , menopausal status at blood collection and diagnosis , fasting status same month and year time of day , menopausal status at diagnosis , fasting status , luteal day of sample 3 months 3 months menopausal status , phase of cycle in premenopausal 5 years 89 days menopausal status , daylight saving period , recruitment centre plco , usa22 19932001 non - fasting 80c 24 months 24 months originally a case - cohort study ; matched sets created for this analysis pphv , netherlands11 prospect - epic , netherlands11 sof , usa26 198791 199397 198688 non - fasting non - fasting fat - free overnight and morning diet 20c 1 year same month and year place of residence 80c initially 1 year same month and year none then - 196c 120c 24 months 24 months whi - os , usa21 199398 fasting 70c 24 months 24 months originally a case - cohort study ; matched sets created for this analysis originally a case - cohort study ; matched sets created for this analysis * stored in liquid nitrogen at 196c , except in denmark in nitrogen vapour at 150c , and in sweden in electric freezers at 80 c . 
 table 1 : description of studies vol 11 june 2010 articles ( pphv ) and prospect - epic , from the netherlands ; 11 study of osteoporotic fractures ( sof ) , from the usa ; 26 and the womens health initiative , observational study ( whios ) , from the usa.21 table 1 summarises the study designs . 
 details of the assay methods for igf1 and igfbp3 are shown in table 2 ; 10 studies used serum , six used plasma , and one used both , but for convenience we refer to plasma concentrations throughout this paper . 
menopausal status at the time of blood collection was de ned on the basis of questions about the number of menstrual periods in the previous year and details of any hysterectomy and ovariectomy ; the details varied slightly between studies and are in the original publications . 
women were excluded from the analyses if they were perimenopausal or of unknown menopausal status , if they were using hormonereplacement therapy or other exogenous sex hormones at the time of blood collection , or if data were missing for dates of birth , blood collection , or diagnosis ( for cases )  . 
 statistical analysis of the 17 studies that contributed data , 11 provided data for women who were premenopausal at blood collection , and 15 provided data for women who were postmenopausal at blood collection . 
for the cross - sectional analyses , data were included from all women in the original studies who had not been diagnosed with breast cancer ( n = 10 022 ) ; in the analyses of breast - cancer risk the data were arranged in matched sets , and some potential controls were not matched ; therefore , the number of controls with data on igf1 is less in the risk analyses ( n = 9428 )  . concentrations of igf1 and igfbp3 were positively skewed ; therefore , log - transformed concentrations were used for all parametric analyses . 
correlations between igf1 and igfbp3 among premenopausal and postmenopausal controls were calculated using standardised log - transformed concentrations within each study , the standardised values being calculated by subtracting the mean log concentration and dividing by the standard deviation of the log concentration . 
the associations of igf1 with risk factors for breast cancer were examined in the controls using linear regression , calculating geometric mean concentrations and 95% cis according to categories of these factors . 
the heterogeneity between studies in the associations of igf1 with risk factors was assessed by adding a study factor interaction term to the model and using the f test to calculate its signi cance . 
a similar approach was used to assess heterogeneity according to menopausal status . 11 of the original studies contributing to the collaborative analysis had used matched nested case - control designs , and the remaining six had used unmatched controls or a case - cohort design ( janus , 20 kkh denmark , 12 mccs , 19 plco , 22 sof , 26 and whi - os21 )  . 
some used density sampling , meaning that an individual participant could appear more than once in a data le ; in order to avoid double - counting women in the cross - sectional analyses , we created a pooled dataset in which duplicate observations were deleted , with the case observation retained where a participant appeared as both a case patient and a control . 
we retained the original matched sets where available , otherwise for the case - cohort studies we created new matched sets in which each case was matched with up to four controls , matching by study , date of blood collection ( plus or minus 24 months ) , age at blood collection ( plus or minus 24 months ) and , for janus only , 20 county of residence . 
 conditional logistic regression was used to calculate the odds ratio ( or ) for breast cancer in relation to the plasma concentrations of igf1 and igfbp3 , categorising women in each study according to the quintiles of hormone concentration for the controls in that study . 
study - speci c cut - points were used because the absolute concentrations of igf1 and igfbp3 vary between studies because of laboratory variation ; further explanation of this approach is provided in previous publications.25 , 27 to provide a summary measure of risk , we calculated a linear trend by scoring the fths of the plasma igf1 or igfbp3 concentrations as 0 , 025 , 05 , 075 , and 1 ; under the assumption of linearity , a unit change in this trend variable is equivalent to the or comparing the highest with lowest fth of hormone concentration.27 heterogeneity in linear trends among studies was assessed using a test , calculating the statistic as the di erence between the sum of the model values for each study and the model value from the all - studies analysis . 
we also used tests to examine whether there was evidence of heterogeneity in the associations of igf1 with breast - cancer risk according to subgroups de ned by menopausal status at blood collection and other factors . the we examined the e ect on the association with breastcancer risk of adjusting igf1 and igfbp3 for each other . 
 we also investigated the associations of igf1 with breastcancer risk after adjusting , one factor at a time , for various established reproductive and hormonal risk factors for breast cancer : age at menarche ( < 12 , 1213 , 14 years ) ; figure 1 : geometric mean igf1 concentrations ( nmol / l with 95% ci ) among controls by selected factors adjusted for study and age at blood collection , as appropriate . 
p < 005 for test of interaction with study . parity ( 0 , 1 , 2 , 3 , 4 full - term pregnancies ) ; age at rst fullterm pregnancy ( < 20 , 2024 , 2529 , 30 years ) ; body mass index ( bmi ; < 225 , 225249 , 250274 , 275299 , 300 kg / m ) ; previous use of oral contraceptives ( never or ever ) ; and , for postmenopausal women only , type of vol 11 june 2010 articles menopause ( natural or surgical ) ; time since menopause ( 04 , 514 , 15 years ; natural postmenopausal women only ) ; previous use of hormone - replacement therapy ( never or ever )  . 
for postmenopausal women , we also investigated the associations of igf1 with breast - cancer risk after adjustment for plasma concentrations of oestradiol and testosterone , and the associations of igf1 with breast - cancer risk with joint classi cation according to plasma oestradiol and testosterone concentrations . all statistical tests were two - sided , and statistical signi cance was set at the 5% level . 
 role of the funding source the funding source had no role in study design , data collection , data analysis , data interpretation , or the writing of the report . 
mean age at baseline ranged from 355 ( sd 78 ) to 477 ( sd 31 ) for premenopausal women , and from 543 ( sd 61 ) to 718 ( sd 49 ) for postmenopausal women . 
across the studies , mean bmi ranged from 231 ( sd 35 ) to 284 ( sd 63 ) kg / m , and the median time between blood collection and diagnosis ranged from 1 ( iqr 03 ) to 17 ( iqr 818 ) years . 
 table 3 : participant characteristics by study and case - control status vol 11 june 2010 hormone fifth cases / or ( 95% ci ) or and 95% ci p for trend igf1 pre - menopausal women 1 articles controls 374 / 829 392 / 831 367 / 814 390 / 822 414 / 800 100 105 ( 088126 ) 105 ( 087125 ) 110 ( 092132 ) 121 ( 100145 ) 558 / 1069 113 ( 098132 ) 573 / 1083 114 ( 098133 ) 596 / 1060 124 ( 107144 ) 618 / 1039 133 ( 114155 ) 950 / 1900 110 ( 098123 ) 940 / 1897 110 ( 098124 ) 986 / 1882 118 ( 105132 ) 1032 / 1839 128 ( 114144 ) 405 / 816 384 / 828 374 / 797 372 / 798 380 / 773 100 096 ( 080114 ) 097 ( 081117 ) 094 ( 078114 ) 100 ( 082122 ) 524 / 1051 581 / 1041 542 / 1034 625 / 1003 097 ( 084113 ) 110 ( 095128 ) 106 ( 090123 ) 123 ( 104145 ) 908 / 1879 097 ( 086108 ) 955 / 1838 105 ( 093117 ) 914 / 1832 101 ( 090114 ) 1005 / 1776 113 ( 099128 ) postmenopausal women 508 / 1081 100 all women 882 / 1910 100 igfbp3 premenopausal women postmenopausal women 544 / 1067 100 all women 949 / 1883 100 075 figure 2 : odds ratios ( or ) for breast cancer associated with igf1 and igfbp3 among premenopausal women ( at blood collection ) , postmenopausal women ( at blood collection ) , and all women the black squares indicate the ors and the horizontal lines show the 95% cis . 
geometric mean concentrations of igfbp3 ranged from 680 ( 95% ci 657704 ) for premenopausal women and from 697 ( 668727 ) to 1606 ( 15791633 ) nmol / l for postmenopausal women . 
 data on igf1 and igfbp3 were available for 10 022 and 9889 controls , respectively ( these numbers are larger than those for the matched - set analyses because data for unmatched controls were included in the cross - sectional analyses )  . 
igf1 and igfbp3 were associated with each other , with correlations of 038 and 050 ( data not shown ) in premenopausal and postmenopausal women , 0050 00002 < 00001 0921 0012 0062 respectively ( both p < 00001 )  . 
the associations of igf1 with selected reproductive and other factors in control women are shown in gure 1 ( equivalent analyses for igfbp3 are in the webappendix p 2 )  . 
geometric mean igf1 was 26% lower for women aged 65 years and above than for women aged less than 45 years ; the other results presented in gure 1 are adjusted for age . 
igf1 was 7% higher in women who were at least 170 cm tall than in women who were less than 155 cm tall , and was higher in women with a bmi of 250274 kg / m than in thinner or more overweight women . 
igf1 was higher in women who drank up to 19 g / d of alcohol than in women who did not drink or who drank at least 20 g / d of alcohol , and was 4% lower for women who had undergone menarche at ages 14 years and over than for women who had undergone menarche before age 12 years . 
 igf1 was weakly positively associated with breast - cancer risk for premenopausal women ( test for trend , p = 0050 ) and strongly positively associated with breast - cancer risk for postmenopausal women ( test for trend p = 00002 ; gure 2 ) ; the test for heterogeneity by menopausal status at blood collection was not statistically signi cant ( test for heterogeneity p = 0894 )  . 
in the individual studies , the ors for the linear trend for premenopausal women ranged from 072 to 269 , with an overall estimate of 118 ( 95% ci 100140 ) , and the median ratio of the igf1 concentration in the top versus the lowest fth was 23 for for ( gure 3a )  . 
the ors postmenopausal women ranged from 043 to 273 , with an overall estimate of 130 ( 95% ci 113149 ) , and the median ratio of the igf1 concentration in the top versus the lowest fth was 24 ( gure 3b )  . 
in the combined analysis of premenopausal and postmenopausal women , 536 vol 11 june 2010 articles those in the highest fth of igfbp3 had an or of 113 ( 95% ci 099128 ) compared with women in the lowest fth ( test for trend p = 0062 )  . 
adjustment of the association between igf1 and breast - cancer risk for igfbp3 had no signi cant e ect on the or ; the or for linear trend before adjustment was 124 ( 95% ci 111138 ) and after adjustment was 124 ( 110141 )  . 
by contrast , adjustment of the association between igfbp3 and breast - cancer risk for igf1 reduced the or for linear trend from 112 ( 95% ci 100126 ) to 099 ( 087114 )  . 
analyses of breast - cancer risk in relation to the molar ratio of igf1 to igfbp3 showed a signi cant positive association , but the magnitude was less than for the analyses of igf1 ; ors in increasing fths of the ratio were 117 ( 099126 ) , ( 95% ci 104132 ) , 112 114 ( 101129 ) and 123 ( 108140 ) ( test for trend p = 0009 )  . 
the ors varied according to oestrogen - receptor status ; the or for a linear trend in igf1 was signi cant among oestrogen - receptor positive cases ( or 138 , 95% ci 114168 ) , but not for oestrogenreceptor negative tumours ( or 080 , 057113 ) and the test for heterogeneity was signi cant ( p = 0007 )  . 
 we examined the e ect on the association of igf1 with breast - cancer risk of adjustment , one factor at a time , for height , age at menarche , number of full - term pregnancies , age at rst full - term pregnancy , use of hormonal contraceptives , type of menopause ( postmenopausal only ) , time since menopause ( postmenopausal only ) , previous use of hormonal therapy for menopause ( postmenopausal only ) , bmi ( premenopausal and postmenopausal analysed separately ) , plasma oestradiol concentration ( postmenopausal only ) , plasma testosterone concentration ( postmenopausal only ) , time of day of blood collection , and the phase of the menstrual cycle at blood collection ( premenopausal only )  . 
none of these adjustments altered the or for igf1 and breast cancer by more than 2% ( data not shown ) with the exception of adjustment for testosterone in postmenopausal women , which reduced the or for an 80 percentile di erence in igf1 from 130 ( 95% ci 108155 ) to 124 ( 104149 )  . 
whi - os = womens health initiative , observational study . was signi cantly positively associated with risk in three out of 15 studies of postmenopausal women ( webappendix pp 3 , 4 )  . 
there was signi cant heterogeneity in the association of igfbp3 with breast - cancer risk according to oestrogen receptor status ; igfbp3 was non - signi cantly positively associated with risk for oestrogen - receptorpositive breast cancer and non - signi cantly inversely associated with risk for oestrogen - receptor - negative breast cancer ( test for heterogeneity p = 0039 ; webappendix p 5 )  . discussion the results of this collaborative analysis show that plasma concentrations of igf1 are positively associated with breast - cancer risk . 
hrt = hormone replacement therapy . modi ed by menopausal status at blood collection or by igfbp3 concentrations , but seems to be con ned to oestrogen - receptor - positive tumours . factors , the strengths of our study are that the data and plasma samples were all collected prospectively , that it includes almost all the available data from published studies worldwide , and that we were able to adjust for other potential risk including endogenous sex hormones . 
this method assumes the true concentrations across the quintiles are similar in all the studies , and if this assumption is not correct then the estimates of ors might be biased.27 however , because heterogeneity between studies in risk estimates was not evident , this assumption does seem reasonable . 
there was some evidence of heterogeneity between studies in some of the cross - sectional analyses , suggesting that caution should be maintained in the interpretation of these analyses . previous studies have examined the associations of igf1 with other factors . 
relevant publications are cited below , but it should be noted that some of these are from the studies contributing to this collaborative analysis . igf1 was inversely associated with age , with no obvious additional decline in concentrations around age 50 years , suggesting that menopause itself does not have a marked e ect on igf1 . 
no signi cant association of igf1 with height was noted in two previous analyses in adults , 29 , 33 but these results might be compatible with the small association noted in the current analysis . 
igf1 was higher in women with a bmi of 250 to 274 kg / m than in thinner or more overweight women , as described previously.34 most circulating igf1 is produced by the liver , and it is possible that a low bmi is associated with low igf1 synthesis due to a relatively low supply of nutrients to the liver , whereas obesity is associated with low igf1 synthesis in the liver due to compromised liver function.35 igf1 was not associated with smoking , consistent with previous observations.29 , 30 , 36 in relation to alcohol , igf1 was higher for women who drank a small amount than for those who drank no alcohol or those who drank 20 g or more per day . 
other observational studies had similar results.29 , 3740 in randomised trials , 15 g / d of alcohol had no e ect on igf1 in postmenopausal women , whereas 30 g / d caused a decrease in igf1 by 95% for premenopausal women and by 49% for postmenopausal women.41 , 42 igf1 did not di er between women with or without a rst - degree family history of breast cancer . 
laboratory studies have shown that oestrogen increases igf receptor levels in breast - cancer cells , 51 whereas in oestrogen - receptor - negative breastcancer cells the levels of igf1 receptor are decreased , and igf1 is non - mitogenic.52 igfbp3 was positively associated with breast - cancer risk , but this association was weak , and was eliminated by adjustment for igf1 , suggesting that the association of igfbp3 with risk is due to its positive correlation with igf1 . 
it seems that , at least in the current dataset , the igfbp3 measures do not add substantial information in assessing the relationship of igf1 with breast - cancer risk . 
in addition to its role in transporting igf1 , laboratory studies have shown that igfbp3 can have direct e ects on cell behaviour which can promote apoptosis , but under other circumstances can act against apoptosis.53 data on igfbp - 1 and igfbp - 2 have also been contributed for our collaborative analyses , but currently there are too few data to provide robust analyses . 
better understanding of the roles of igfbinding proteins as potential modulators of the association between igf1 and breast - cancer risk might come from further data on igfbp1 and igfbp2 , from measures of intact igfbp3 , 54 or from measures of bioavailable igf1.55 the or for igf1 is smaller than the ors for both oestrogens and androgens and breast - cancer risk in postmenopausal women , which have been shown in data mostly from the same epidemiological studies ; high concentrations of oestradiol and testosterone are associated with around a doubling in breast - cancer risk.25 , 5658 in our analyses , adjustment for oestradiol and testosterone had little e ect on the association of igf1 with breast - cancer risk for postmenopausal women , and there was no evidence of an interaction between igf1 and oestradiol or testosterone in relation to breast - cancer risk . 
nevertheless , a better understanding of the joint e ects of hormones on breast - cancer risk is needed.59 association we observed between igf1 and age at menarche has been noted previously.43 , 44 we observed a non - linear association between igf1 and parity , with the lowest concentrations for women who had four or more full - term pregnancies ; previous studies have not reported any associations between igf1 and parity.30 , 4345 igf1 was also positively associated with age at rst full - term pregnancy . 
igf1 was marginally higher for women who had previously used hormonal contraceptives than for women who had not , but did not vary according to previous use of hormonal therapy for menopause . 
in future analyses we will examine the relationships of igf1 with endogenous sex hormones . the associations of igf1 with height , age at menarche , age at rst full - term pregnancy , and time since menopause are compatible with the possibility that these factors a ect breast - cancer risk partly through their relationships with igf1 . 
this association did not vary signi cantly according to menopausal status at blood collection or according to the risk factors for breast cancer examined , and was not attenuated by adjustment for other risk factors including igfbp3 , reproductive factors , and , for postmenopausal women , bmi , oestradiol , and testosterone . 
if the association was due to an e ect of preclinical tumours on igf1 ( reverse causality ) , 46 then it would be expected to be weaker in those with a greater time interval between blood collection and diagnosis . 
 a previous meta - analysis based on studies published up to 2006 concluded that the association of igf1 with breastcancer risk is limited to premenopausal women , 47 but our analysis includes four large more recent studies with over 1500 additional patients and shows a clear association of igf1 with breast - cancer risk in postmenopausal women . 
the correlations ( intra - class or spearman ) between baseline and repeat measures ranged from approximately 04 to 09 over 1 to 15 years.10 , 17 , 19 , 4850 it is therefore likely that the observed association between igf1 concentrations and breastcancer risk is an underestimate of the true association , but more reproducibility data are required . 
 vol 11 june 2010 articles the association of igf1 with breast - cancer risk was not altered by adjusting for age at menarche , parity , age at rst full - term pregnancy , use of exogenous hormones , and bmi , suggesting that the relationship of igf1 with breastcancer risk is not confounded by these other risk factors . 
it is not known whether this association is causal , but there are plausible biological mechanisms that could explain such an e ect.1 , 2 the magnitude of the observed association is modest , but the true association could be substantially larger because of measurement error , and further work is needed to reliably quantify the relationship . 
 co - authors from womens health initiative observational study : mj gunter , te rohan , hd strickler ( department of epidemiology and population health , albert einstein college of medicine , new york , ny , usa )  . con ict of interest statement for the writing committee , tjk , pna , and gkr declared no con icts of interest . 
we thank the women who participated in the collaborating studies , the research sta , the collaborating laboratories and the funding agencies in each of the studies . re ection and reaction cancer patterns in inuit populations i wish to congratulate friborg and melbye1 on their informative review of cancer patterns in inuit populations , published in the september issue of the lancet oncology . 
as a clinician working with inuit in the nunavik region of northern quebec , i believe there are a few additional points worth mentioning . individuals first , there are a few small , but noteworthy , caseseries describing kaposis sarcoma in hiv seronegative inuit from greenland and nunavik . 
 although classic kaposis sarcoma is associated with human herpesvirus - 8 and is usually seen in elderly male patients of mediterranian or jewish descent , this disease has been described in eight immunocompetent inuit patients since 1974.2 a similar combination of genetic susceptibility and viral factors , as described by the authors with respect to nasopharyngeal carcinoma and epstein - barr virus in the inuit , might be responsible . second , with respect to the high incidence of cancers of the nasopharynx and lung , two signi cant exposures were not mentioned . 
although modern housing conditions have decreased exposure to fumes from lamps and open res for cooking , it is important to recognise that many groups of inuit still spend substantial amounts of time out on the land , cooking on open stoves inside their tents . 
additionally , the epidemic of marijuana smoking in 85% of adults ( according to 2004 nunavik public - health data ) 3 might play a part in the high incidence of lung and nasopharyngeal cancers . last , but not least , it is important to recognise that inuit face substantial challenges with respect to access to healthcare , and that these challenges represent part of a more far - reaching social inequality . 
 public - health statistics from the last 5 - year case period in nunavik suggest that both cancer incidence and mortality are higher overall for the subarctic inuit of the region than for age - matched southern patients.4 , 5 with life expectancy for canadian inuit more than 12 years less than the national average , 6 we must not forget that documents such as the universal declaration of human rights and the recommendations for worldwide cancer life expectancy for inuit is less than national average control mentioned in a comment by john se rin7 need to be applied for minority populations within developed countries as well as throughout the global community . barbara m young general internal medicine division , mcgill university , montreal , quebec , canada barbara.young@mcgill.ca the author declared no con icts of interest . friborg jt , melbye m . 
resumes_nunavik / anglais / alcoholdruguseandgamblingamongtheinuito fnunavik.pdf ( accessed nov 7 , 2008 )  . taux dincidence pour lensemble des sieges , excluant le cancer de la peau sans melanoma 2000 2004 . 
msss fichier des decs ( qubec ) , october 2005 ( electronic version )  . 6 wilkins r , uppal s , fins p , sencal s , guimond e , dion r . 
 errata risk ratio lower limit upper limit z value p value risk ratio ( 95% ci ) meyer18 lee19 hull20 deitcher21 overall 0704 0509 0438 0690 0509 0121 0329 0188 0124 0351 4091 0789 1017 3832 0737 0391 3018 1920 0425 3571 0696 0003 0055 0671 < 00001 * noble sir , shelley md , coles b , et al . 
our aim was to study trends over time in prostate - cancer mortality and incidence in the usa and uk in 19752004 , and compare these patterns with trends in screening and treatment . 
 methods joinpoint regression analysis of cancer - mortality statistics from cancer research uk ( london , uk ) and from the us national cancer institute surveillance , epidemiology and end results ( seer ) programme from 1975 to 2004 was used to estimate the annual percentage change in prostate - cancer mortality in both countries and the points in time when trends changed . 
the ratio of usa to uk age - adjusted prostate - cancer incidence was also assessed . findings age - speci c and age - adjusted prostate - cancer mortality peaked in the early 1990s at almost identical rates in both countries , but age - adjusted mortality in the usa subsequently declined after 1994 by 417% ( 95% ci 434 to 399 ) each year , four - times the rate of decline in the uk after 1992 ( 114% [ 144 to 084 ] )  . 
the mortality decline in the usa was greatest and most sustained in patients aged 75 years or older ( 532% [ 823 to 232 ] ) , whereas death rates had plateaued in this age group in the uk by 2000 . 
the mean ratio of usa to uk age - adjusted prostate - cancer incidence rates in 19752003 was 25 , with a pronounced peak around the time that psa testing was introduced in the usa . 
numbers needed to treat to prevent one death from prostate cancer were 33 000 in the 5564 - year age group . interpretation the striking decline in prostate - cancer mortality in the usa compared with the uk in 19942004 coincided with much higher uptake of psa screening in the usa . 
explanations for the di erent trends in mortality include the possibility of an early e ect of initial screening rounds on men with more aggressive asymptomatic disease in the usa , di erent approaches to treatment in the two countries , and bias related to the misattribution of cause of death . 
speculation over the role of screening will continue until evidence from randomised controlled trials is published . funding prompt ( prostate cancer : mechanisms of progression and treatment ) collaborative ( uk national cancer research institute , london , uk , and uk medical research council , london , uk )  . introduction prostate - cancer screening based on the serum prostatespeci c antigen ( psa ) test was introduced in the usa around 1990 and is almost routine in the usa ; in 2001 , 57% of men aged 50 years or older reported having a psa test within the previous 12 months.1 by con trast , for each year between 1999 and 2002 , an esti mated 6% of men aged 4584 years were tested in the uk.2 there is no robust evidence that routine psa testing decreases prostate - cancer mortality.3 , 4 the overall decline in mortality from prostate cancer in the usa since the early 1990s might be attributable to screening or improved treatment for more advanced disease , 511 but other research has suggested that mortality trends cannot be attributed to di erences in screening intensity , either between or within countries.1216 the most recently published comparisons of prostate - cancer mortality trends in the usa and uk , based on data up to the late 1990s , noted that rates had begun to fall more rapidly in the usa than in the uk , but the changes seemed too early to attribute the more rapid decline in mortality in the usa to an e ect of psa screening.17 , 18 we assessed whether this pattern of di erential mortality decline continued , by comparing usa and uk prostate - cancer mortality and incidence rates up to 2004 . 
 we also assessed possible explanations for changes in these rates , by collecting data from both countries on the use of treatments ( surgery , radiotherapy , and hormone treatment )  . 
 methods data sources prostate and all - cancer mortality statistics in 19752004 and prostate - cancer incidence statistics in 19752003 were obtained from cancer research uk , london , uk ( compiled from data produced by the regional registries in england , wales , scotland , and northern ireland ) 19 and from the us national cancer institute ( nci ) surveillance , vol 9 may 2008 articles epidemiol ogy and end results ( seer ) programme ( mortality data from the national center for health statistics ; incidence data from seer 9 registries database ) .20 usa and uk cancer statistics were age - adjusted to the same european standard population ( 19 age groups )  . 
hes records were extracted by use of the o ce of population , censuses and surveys ( opcs ) procedure code m61 ( radical prostatectomy ) when the underlying diagnosis was prostate cancer ( international classi cation of diseases [ icd ] 9 185 , icd10 c61 )  . 
for the 6574 - years and 75 - years age groups , the models with the best t to usa data had two joinpoints , but models with three joinpoints were chosen to assist comparison with the uk . 
evidence at 5% level of signi cance that annual percentage change is greater than or less than zero . table 1 : usa and uk prostate - cancer mortality trends ( joinpoint analysis ) , by age group ( 19752004 ) 446 vol 9 may 2008 articles prescription data were obtained from 500 uk family doctors , projected to the whole of the uk by the use of regional weights ( ie , by dividing the total number of family doctors in a region by the number sampled in that region ) , and adjusted to estimate the total number of prescriptions dispensed in the uk , as suggested by data published by the uk prescription pricing authority . 
the ims health database contains about 2 million currently active anonymous patient records and over 95 million prescriptions , is subject to internal validation and quality checks , 22 and is widely used in drug - use studies.2328 hes and ims data were used to calculate annual radical prostatectomy and anti - androgen deprivation drug country year of peak mortality peak mortality ( per 100 000 person - years ) decline since peak , 5564 years uk 6574 years uk 75 years any age 1991 1990 1992 1990 1994 1993 1992 1991 246 263 1206 1219 4609 4696 301 300 251 398 219 453 338 116 363 table 2 : usa and uk age - speci c and age - adjusted prostate - cancer peak mortality and percentage decline since peak , by age group prescriptions per incident prostate cancer by the use of the denominator . 
we allowed a maximum of three joinpoints , and an overall signi cance level of 5% was used for the comparisons of models applied to each data series . role of the funding source the funding source had no role in the study design , data collection , data analysis , or interpretation of the ndings . 
 results trends in age - adjusted and age - speci c prostate - cancer mortality up to the mid - 1990s were similar in the usa age - adjusted incidence ( all ages ) age - specic incidence ( 4554 years ) age - specic incidence ( 5564 years ) usa 2000 1500 1000 2000 1500 1000 2000 1500 1000 age - specic incidence ( 6574 years ) age - specic incidence ( 7584 years ) age - specic incidence ( 85 years ) 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 year year year figure 2 : usa and uk prostate - cancer incidence rates ( 19752003 ) vol 9 may 2008 usa / uk age - adjusted incidence ( all ages ) usa / uk age - specic incidence ( 4554 years ) usa / uk age - specic incidence ( 5564 years ) usa / uk age - specic incidence ( 6574 years ) usa / uk age - specic incidence ( 7584 years ) usa / uk age - specic incidence ( 85 years ) articles 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 year year year figure 3 : ratios of usa / uk prostate - cancer incidence ( 19752003 ) usa radiotherapy usa radical prostatectomy uk anti - androgen prescriptions uk radical prostatectomy 1980 1985 1990 1995 2000 2005 year figure 4 : usa and uk prostate - cancer treatment trends * % of incident prostate cancer . 
age - adjusted prostate - cancer mortality declined in the usa by 417% each year between 1994 and 2004 ( table 1 ) , almost four - times the rate of decline in the uk ( 114% each year )  . 
age - speci c and ageadjusted mortality peaked at almost identical rates in both countries , but subsequent declines were much greater in the usa than in the uk ( table 2 ) , especially in men aged 75 years or older . 
in this age group , we did not note a change in uk prostate - cancer mortality rates between 2000 and 2004 , compared with a decline of 532% each year between 2002 and 2004 in the usa ( table 1 )  . long - term usa and uk age - adjusted and age - speci c prostate - cancer incidence rate trends were similar in 19752003 , although rates in the usa were consistently higher than in the uk ( gure 2 )  . 
the mean ratio of usa to uk age - adjusted prostate - cancer incidence rates in 19752003 was 25 , with a pronounced peak around the time that psa testing was introduced in the usa ( gure 3 )  . 
ratios of usa to uk age - speci c prostatecancer incidence were highest in men aged under 75 years ; in 1992 the ratio was 82 for men aged 4554 years and 67 for men aged 5564 years . 
 in the usa , the proportion of men with prostate cancer who underwent radical prostatectomy has increased dramatically from the mid - 1980s , reaching a plateau of around 30% of all incident prostate cancers in the early 1990s ( gure 4 )  . 
uk prescriptions of gonadotropin - releasing hormones increased 33 - times per patient with prostate cancer and anti - androgens increased 18 - times per patient with prostate cancer ( 26 - times overall ) between 1991 and 1999 , and have since remained the same ( gure 4 )  . 
joinpoint analysis of seer data for all cancers ( except non - melanoma skin cancer ) show a slight increase of 040% ( 95% ci 034 to 046 ) each year between 1975 and 1990 , then a decline of 125% ( 134 to 117 ) to 2004 . 
comparable uk data from cancer research uk show a similar slight increase of 027% ( 015 to 039 ) between 1975 and 1989 , then a decline of 134% ( 145 to 124 )  . to gauge the population balance of risk and bene t , a simple numbers needed to treat calculation was done based on the di erence between usa and uk in the number of deaths from prostate cancer in 2004 . 
this calculation showed that the number of middle - aged uk men needed to emigrate to the usa to prevent one death in the 5564 - year age group was around 33 000 . 
in the usa , around 50% of men ( 16 700 of our emigres ) have an annual psa test.1 of these , about 4200 ( 25% ) men would have a raised psa ( 3 ng / ml ) , and of these , about 1300 ( 31% ) men would be diagnosed with localised prostate cancer and 210 ( 5% ) men would be diagnosed with advanced prostate cancer . 
of those with localised prostate cancer , about half ( 650 ) would be treated by radical prostatectomy , 33 and if intra operative or postoperative mortality were to exceed 015% , then at least one man would die to prevent one death from prostate cancer in those aged 5564 years . 
of men receiving radical treatment , there would also be a substantial burden of erectile and urinary dysfunction.34 discussion this study has shown that trends in prostate - cancer mortality in the uk and usa have diverged in recent years , with the usa experiencing more rapidly declining mortality compared with the uk since the mid - 1990s , especially in men aged 75 years or over ( gure 1 )  . 
despite major di erences between usa and uk health - care systems , all - cancer mortality trends in the usa and uk were very similar , suggesting that the divergence in usa and uk prostate - cancer mortality trends could be attributable to di erences in detection or treatment ( or both )  . detection was markedly di erent between the usa and uk . 
there was a ten - times di erence in the uptake of psa testing between the usa ( 57% ) and uk ( 6% ) by 2001 , 1 , 2 and the corresponding shift in the usa towards detection of predominantly localised disease33 , 35 , 36 has not occurred in the uk.3739 at the end of the 1990s , it was too early to attribute decreasing usa mortality rates to the e ect of screening.17 one interpretation of the current data could be that the higher numbers of patients screened in the usa have decreased prostate - cancer mortality . 
however , the introduction of screening would not be expected to decrease prostate - cancer mortality so soon , because only a small proportion of those with earlystage cancer would be predicted to die of the disease in the following 20 years in the absence of screening , even if treated conservatively.40 screening aims to bring diagnosis forward ( ie , lead time ) by detecting preclinical disease . 
the lead time resulting from the introduction of prostate - cancer screening is crucial to understanding noted trends , 9 but cannot easily be estimated from empirical data because psa screening also detects men whose prostate cancer would not have become clinically apparent in their lifetimes ( over - diagnosis )  . 
in practice , these two groups of men cannot be distinguished , and consequently models have been developed to estimate lead time under assumptions about the proportion of over - diagnosis . 
one recent model , based on data from the european randomised study of prostate cancer ( erspc ) , 41 estimated mean lead times ranging from 99 to 133 years ; another , based on seer prostate - cancer mortality data , estimated a mean lead time for white people of 46 years ( 95% ci 3259 ) .42 the di erence between these estimates might be caused by : di erent screening contexts in erspc ( two mass screening rounds in men recruited to a trial ) and seer ( repeated psa testing made available to the general population of men ) ; use of trial data ( erspc ) , as compared with estimates of individual - level parameters from populationlevel secular trends ( seer ) ; and di erent assumptions being made in the models.41 , 42 because prostate - cancer screening was established in the usa around 1990 , evidence of improved survival due to screening would start to become apparent around 2000 if lead times were relatively short9 and survival of men with localised cancer in the absence of screening was worse than that recorded by albertsen and colleagues.40 however , because the decline in usa prostate - cancer mortality rates started around 1990 , much of this decline should be due to factors other than detection by screening vol 9 may 2008 articles of more men at an early stage of disease . 
uncertainty about lead time means that our data might precede the point at which a survival bene t of screening would become apparent . di erences in treatments between the countries might be important in explaining some of the divergence in trends . 
whereas bene ts for a small minority might have an e ect on overall prostatecancer mortality , most men whose cancer is detected by screening might be receiving unnecessary diagnosis and treatment to the detriment of their quality of life , 41 , 42 , 5759 as highlighted by our numbers needed to treat calculation . 
 decreases in cause - speci c mortality would also not necessarily mean longer life expectancy , especially in older men who might succumb to another cause of death in the same year in which they would have died of prostate cancer . 
similarly , greater decreases in deaths due to other major causes in the uk than in the usa could contribute to divergent trends in prostate - cancer mortality , but there is no evidence that this occurred in relation to the major causes of mortality ( all cancers and cardiovascular disease )  . our studys main limitations were that it was ecological , and comparisons of underlying trends in stage at diagnosis and type of treatment were restricted by paucity of data from the uk . 
changes in cause of death coding the might have a ected our ndings , although introduction of icd - 9 in 1979 improved between - country comparability of cancer - mortality data.60 in the uk , a change in interpretation of icd rule 3 for selecting cause of death triggered an artefactual increase in prostatecancer mortality in 1983.61 the partial reversal of this change in 1993 might have had a slight e ect on our analysis of usa and uk prostate - cancer mortality trends from the early 1990s , but tending towards an underestimate of di erences.31 it has been suggested that misattribution of the underlying cause of death to prostate cancer in the rising and then falling pool of newly diagnosed cancers might have explained at least part of the rise and fall in prostatecancer mortality in the usa.8 since the secular trend in incidence of prostate cancer in the uk showed a steady increase , rather than the large rise then fall seen in the usa , such misattribution bias in the uk would be expected to artefactually raise prostate - cancer mortality rates throughout the study period . 
therefore , the di ering patterns of prostate - cancer incidence , combined with a xed proportion of misattribution of cause of death to prostate cancer in those diagnosed by screening , might explain some of the di erences in mortality noted between the usa and uk . 
one report suggests biased 450 vol 9 may 2008 articles underattribution of prostate cancer as the underlying cause of death in men who underwent radical treatment ; 62 this observation might also partly explain the noted mortality di erences between the usa and uk , because of di erences between these countries in the proportion of men receiving radical treatment for localised prostate cancers . there are also some concerns about data reliability . 
 seer prostate - cancer mortality data have been assessed to be reasonably representative of the us population , in africanalthough under - representing mortality americans , 63 but the reliability of seer data on prostatecancer treatments has not been assessed . 
all authors were involved in revisions and approved the nal version . con icts of interest the authors declared no con icts of interest . acknowledgments this research was supported by the prompt ( prostate cancer : mechanisms of progression and treatment ) collaborative ( uk national cancer research institute and uk medical research council )  . 
our aim was to study trends over time in prostate - cancer mortality and incidence in the usa and uk in 19752004 , and compare these patterns with trends in screening and treatment . 
 methods joinpoint regression analysis of cancer - mortality statistics from cancer research uk ( london , uk ) and from the us national cancer institute surveillance , epidemiology and end results ( seer ) programme from 1975 to 2004 was used to estimate the annual percentage change in prostate - cancer mortality in both countries and the points in time when trends changed . 
the ratio of usa to uk age - adjusted prostate - cancer incidence was also assessed . findings age - speci c and age - adjusted prostate - cancer mortality peaked in the early 1990s at almost identical rates in both countries , but age - adjusted mortality in the usa subsequently declined after 1994 by 417% ( 95% ci 434 to 399 ) each year , four - times the rate of decline in the uk after 1992 ( 114% [ 144 to 084 ] )  . 
the mortality decline in the usa was greatest and most sustained in patients aged 75 years or older ( 532% [ 823 to 232 ] ) , whereas death rates had plateaued in this age group in the uk by 2000 . 
the mean ratio of usa to uk age - adjusted prostate - cancer incidence rates in 19752003 was 25 , with a pronounced peak around the time that psa testing was introduced in the usa . 
numbers needed to treat to prevent one death from prostate cancer were 33 000 in the 5564 - year age group . interpretation the striking decline in prostate - cancer mortality in the usa compared with the uk in 19942004 coincided with much higher uptake of psa screening in the usa . 
explanations for the di erent trends in mortality include the possibility of an early e ect of initial screening rounds on men with more aggressive asymptomatic disease in the usa , di erent approaches to treatment in the two countries , and bias related to the misattribution of cause of death . 
speculation over the role of screening will continue until evidence from randomised controlled trials is published . funding prompt ( prostate cancer : mechanisms of progression and treatment ) collaborative ( uk national cancer research institute , london , uk , and uk medical research council , london , uk )  . introduction prostate - cancer screening based on the serum prostatespeci c antigen ( psa ) test was introduced in the usa around 1990 and is almost routine in the usa ; in 2001 , 57% of men aged 50 years or older reported having a psa test within the previous 12 months.1 by con trast , for each year between 1999 and 2002 , an esti mated 6% of men aged 4584 years were tested in the uk.2 there is no robust evidence that routine psa testing decreases prostate - cancer mortality.3 , 4 the overall decline in mortality from prostate cancer in the usa since the early 1990s might be attributable to screening or improved treatment for more advanced disease , 511 but other research has suggested that mortality trends cannot be attributed to di erences in screening intensity , either between or within countries.1216 the most recently published comparisons of prostate - cancer mortality trends in the usa and uk , based on data up to the late 1990s , noted that rates had begun to fall more rapidly in the usa than in the uk , but the changes seemed too early to attribute the more rapid decline in mortality in the usa to an e ect of psa screening.17 , 18 we assessed whether this pattern of di erential mortality decline continued , by comparing usa and uk prostate - cancer mortality and incidence rates up to 2004 . 
 we also assessed possible explanations for changes in these rates , by collecting data from both countries on the use of treatments ( surgery , radiotherapy , and hormone treatment )  . 
 methods data sources prostate and all - cancer mortality statistics in 19752004 and prostate - cancer incidence statistics in 19752003 were obtained from cancer research uk , london , uk ( compiled from data produced by the regional registries in england , wales , scotland , and northern ireland ) 19 and from the us national cancer institute ( nci ) surveillance , vol 9 may 2008 articles epidemiol ogy and end results ( seer ) programme ( mortality data from the national center for health statistics ; incidence data from seer 9 registries database ) .20 usa and uk cancer statistics were age - adjusted to the same european standard population ( 19 age groups )  . 
hes records were extracted by use of the o ce of population , censuses and surveys ( opcs ) procedure code m61 ( radical prostatectomy ) when the underlying diagnosis was prostate cancer ( international classi cation of diseases [ icd ] 9 185 , icd10 c61 )  . 
for the 6574 - years and 75 - years age groups , the models with the best t to usa data had two joinpoints , but models with three joinpoints were chosen to assist comparison with the uk . 
evidence at 5% level of signi cance that annual percentage change is greater than or less than zero . table 1 : usa and uk prostate - cancer mortality trends ( joinpoint analysis ) , by age group ( 19752004 ) 446 vol 9 may 2008 articles prescription data were obtained from 500 uk family doctors , projected to the whole of the uk by the use of regional weights ( ie , by dividing the total number of family doctors in a region by the number sampled in that region ) , and adjusted to estimate the total number of prescriptions dispensed in the uk , as suggested by data published by the uk prescription pricing authority . 
the ims health database contains about 2 million currently active anonymous patient records and over 95 million prescriptions , is subject to internal validation and quality checks , 22 and is widely used in drug - use studies.2328 hes and ims data were used to calculate annual radical prostatectomy and anti - androgen deprivation drug country year of peak mortality peak mortality ( per 100 000 person - years ) decline since peak , 5564 years uk 6574 years uk 75 years any age 1991 1990 1992 1990 1994 1993 1992 1991 246 263 1206 1219 4609 4696 301 300 251 398 219 453 338 116 363 table 2 : usa and uk age - speci c and age - adjusted prostate - cancer peak mortality and percentage decline since peak , by age group prescriptions per incident prostate cancer by the use of the denominator . 
we allowed a maximum of three joinpoints , and an overall signi cance level of 5% was used for the comparisons of models applied to each data series . role of the funding source the funding source had no role in the study design , data collection , data analysis , or interpretation of the ndings . 
 results trends in age - adjusted and age - speci c prostate - cancer mortality up to the mid - 1990s were similar in the usa age - adjusted incidence ( all ages ) age - specic incidence ( 4554 years ) age - specic incidence ( 5564 years ) usa 2000 1500 1000 2000 1500 1000 2000 1500 1000 age - specic incidence ( 6574 years ) age - specic incidence ( 7584 years ) age - specic incidence ( 85 years ) 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 year year year figure 2 : usa and uk prostate - cancer incidence rates ( 19752003 ) vol 9 may 2008 usa / uk age - adjusted incidence ( all ages ) usa / uk age - specic incidence ( 4554 years ) usa / uk age - specic incidence ( 5564 years ) usa / uk age - specic incidence ( 6574 years ) usa / uk age - specic incidence ( 7584 years ) usa / uk age - specic incidence ( 85 years ) articles 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 1975 1980 1985 1990 1995 2000 2005 year year year figure 3 : ratios of usa / uk prostate - cancer incidence ( 19752003 ) usa radiotherapy usa radical prostatectomy uk anti - androgen prescriptions uk radical prostatectomy 1980 1985 1990 1995 2000 2005 year figure 4 : usa and uk prostate - cancer treatment trends * % of incident prostate cancer . 
age - adjusted prostate - cancer mortality declined in the usa by 417% each year between 1994 and 2004 ( table 1 ) , almost four - times the rate of decline in the uk ( 114% each year )  . 
age - speci c and ageadjusted mortality peaked at almost identical rates in both countries , but subsequent declines were much greater in the usa than in the uk ( table 2 ) , especially in men aged 75 years or older . 
in this age group , we did not note a change in uk prostate - cancer mortality rates between 2000 and 2004 , compared with a decline of 532% each year between 2002 and 2004 in the usa ( table 1 )  . long - term usa and uk age - adjusted and age - speci c prostate - cancer incidence rate trends were similar in 19752003 , although rates in the usa were consistently higher than in the uk ( gure 2 )  . 
the mean ratio of usa to uk age - adjusted prostate - cancer incidence rates in 19752003 was 25 , with a pronounced peak around the time that psa testing was introduced in the usa ( gure 3 )  . 
ratios of usa to uk age - speci c prostatecancer incidence were highest in men aged under 75 years ; in 1992 the ratio was 82 for men aged 4554 years and 67 for men aged 5564 years . 
 in the usa , the proportion of men with prostate cancer who underwent radical prostatectomy has increased dramatically from the mid - 1980s , reaching a plateau of around 30% of all incident prostate cancers in the early 1990s ( gure 4 )  . 
uk prescriptions of gonadotropin - releasing hormones increased 33 - times per patient with prostate cancer and anti - androgens increased 18 - times per patient with prostate cancer ( 26 - times overall ) between 1991 and 1999 , and have since remained the same ( gure 4 )  . 
joinpoint analysis of seer data for all cancers ( except non - melanoma skin cancer ) show a slight increase of 040% ( 95% ci 034 to 046 ) each year between 1975 and 1990 , then a decline of 125% ( 134 to 117 ) to 2004 . 
comparable uk data from cancer research uk show a similar slight increase of 027% ( 015 to 039 ) between 1975 and 1989 , then a decline of 134% ( 145 to 124 )  . to gauge the population balance of risk and bene t , a simple numbers needed to treat calculation was done based on the di erence between usa and uk in the number of deaths from prostate cancer in 2004 . 
this calculation showed that the number of middle - aged uk men needed to emigrate to the usa to prevent one death in the 5564 - year age group was around 33 000 . 
in the usa , around 50% of men ( 16 700 of our emigres ) have an annual psa test.1 of these , about 4200 ( 25% ) men would have a raised psa ( 3 ng / ml ) , and of these , about 1300 ( 31% ) men would be diagnosed with localised prostate cancer and 210 ( 5% ) men would be diagnosed with advanced prostate cancer . 
of those with localised prostate cancer , about half ( 650 ) would be treated by radical prostatectomy , 33 and if intra operative or postoperative mortality were to exceed 015% , then at least one man would die to prevent one death from prostate cancer in those aged 5564 years . 
of men receiving radical treatment , there would also be a substantial burden of erectile and urinary dysfunction.34 discussion this study has shown that trends in prostate - cancer mortality in the uk and usa have diverged in recent years , with the usa experiencing more rapidly declining mortality compared with the uk since the mid - 1990s , especially in men aged 75 years or over ( gure 1 )  . 
despite major di erences between usa and uk health - care systems , all - cancer mortality trends in the usa and uk were very similar , suggesting that the divergence in usa and uk prostate - cancer mortality trends could be attributable to di erences in detection or treatment ( or both )  . detection was markedly di erent between the usa and uk . 
there was a ten - times di erence in the uptake of psa testing between the usa ( 57% ) and uk ( 6% ) by 2001 , 1 , 2 and the corresponding shift in the usa towards detection of predominantly localised disease33 , 35 , 36 has not occurred in the uk.3739 at the end of the 1990s , it was too early to attribute decreasing usa mortality rates to the e ect of screening.17 one interpretation of the current data could be that the higher numbers of patients screened in the usa have decreased prostate - cancer mortality . 
however , the introduction of screening would not be expected to decrease prostate - cancer mortality so soon , because only a small proportion of those with earlystage cancer would be predicted to die of the disease in the following 20 years in the absence of screening , even if treated conservatively.40 screening aims to bring diagnosis forward ( ie , lead time ) by detecting preclinical disease . 
the lead time resulting from the introduction of prostate - cancer screening is crucial to understanding noted trends , 9 but cannot easily be estimated from empirical data because psa screening also detects men whose prostate cancer would not have become clinically apparent in their lifetimes ( over - diagnosis )  . 
in practice , these two groups of men cannot be distinguished , and consequently models have been developed to estimate lead time under assumptions about the proportion of over - diagnosis . 
one recent model , based on data from the european randomised study of prostate cancer ( erspc ) , 41 estimated mean lead times ranging from 99 to 133 years ; another , based on seer prostate - cancer mortality data , estimated a mean lead time for white people of 46 years ( 95% ci 3259 ) .42 the di erence between these estimates might be caused by : di erent screening contexts in erspc ( two mass screening rounds in men recruited to a trial ) and seer ( repeated psa testing made available to the general population of men ) ; use of trial data ( erspc ) , as compared with estimates of individual - level parameters from populationlevel secular trends ( seer ) ; and di erent assumptions being made in the models.41 , 42 because prostate - cancer screening was established in the usa around 1990 , evidence of improved survival due to screening would start to become apparent around 2000 if lead times were relatively short9 and survival of men with localised cancer in the absence of screening was worse than that recorded by albertsen and colleagues.40 however , because the decline in usa prostate - cancer mortality rates started around 1990 , much of this decline should be due to factors other than detection by screening vol 9 may 2008 articles of more men at an early stage of disease . 
uncertainty about lead time means that our data might precede the point at which a survival bene t of screening would become apparent . di erences in treatments between the countries might be important in explaining some of the divergence in trends . 
whereas bene ts for a small minority might have an e ect on overall prostatecancer mortality , most men whose cancer is detected by screening might be receiving unnecessary diagnosis and treatment to the detriment of their quality of life , 41 , 42 , 5759 as highlighted by our numbers needed to treat calculation . 
 decreases in cause - speci c mortality would also not necessarily mean longer life expectancy , especially in older men who might succumb to another cause of death in the same year in which they would have died of prostate cancer . 
similarly , greater decreases in deaths due to other major causes in the uk than in the usa could contribute to divergent trends in prostate - cancer mortality , but there is no evidence that this occurred in relation to the major causes of mortality ( all cancers and cardiovascular disease )  . our studys main limitations were that it was ecological , and comparisons of underlying trends in stage at diagnosis and type of treatment were restricted by paucity of data from the uk . 
changes in cause of death coding the might have a ected our ndings , although introduction of icd - 9 in 1979 improved between - country comparability of cancer - mortality data.60 in the uk , a change in interpretation of icd rule 3 for selecting cause of death triggered an artefactual increase in prostatecancer mortality in 1983.61 the partial reversal of this change in 1993 might have had a slight e ect on our analysis of usa and uk prostate - cancer mortality trends from the early 1990s , but tending towards an underestimate of di erences.31 it has been suggested that misattribution of the underlying cause of death to prostate cancer in the rising and then falling pool of newly diagnosed cancers might have explained at least part of the rise and fall in prostatecancer mortality in the usa.8 since the secular trend in incidence of prostate cancer in the uk showed a steady increase , rather than the large rise then fall seen in the usa , such misattribution bias in the uk would be expected to artefactually raise prostate - cancer mortality rates throughout the study period . 
therefore , the di ering patterns of prostate - cancer incidence , combined with a xed proportion of misattribution of cause of death to prostate cancer in those diagnosed by screening , might explain some of the di erences in mortality noted between the usa and uk . 
one report suggests biased 450 vol 9 may 2008 articles underattribution of prostate cancer as the underlying cause of death in men who underwent radical treatment ; 62 this observation might also partly explain the noted mortality di erences between the usa and uk , because of di erences between these countries in the proportion of men receiving radical treatment for localised prostate cancers . there are also some concerns about data reliability . 
 seer prostate - cancer mortality data have been assessed to be reasonably representative of the us population , in africanalthough under - representing mortality americans , 63 but the reliability of seer data on prostatecancer treatments has not been assessed . 
all authors were involved in revisions and approved the nal version . con icts of interest the authors declared no con icts of interest . acknowledgments this research was supported by the prompt ( prostate cancer : mechanisms of progression and treatment ) collaborative ( uk national cancer research institute and uk medical research council )  . 
 methods 1941 tumours from 2391 women recruited to neat / br9601 were analysed on tissue microarrays for her2 and top2a ampli cation and deletion , her13 and ki67 expression , and duplication of chromosome 17 centromere enumeration probe ( ch17cep )  . 
log - rank analyses identi ed factors a ecting relapse - free and overall survival , and regression models tested independent prognostic e ect of markers , with adjustment for known prognostic factors ( age , nodal status , oestrogen - receptor status , grade , and tumour size )  . 
in univariate analyses , only her2 ampli cation and top2a deletion were signi cant prognostic factors for relapse - free ( hazard ratio [ hr ] 159 , 95% ci 132192 , p < 00001 ; and 152 , 120192 , p = 00006 , respectively ) and overall survival ( 179 , 147219 , p < 00001 ; and 162 , 126208 , p = 00002 respectively )  . 
by contrast , in multivariate analyses , ch17cep duplication was associated with signi cant improvements in both relapse - free ( hr 092 , 95% ci 072118 for tumours with normal ch17cep vs 052 , 034081 for tumours with abnormal ch17cep ; p for interaction = 0004 ) and overall survival ( 094 , 072124 vs 057 , 036092 ; p for interaction = 002 ) with anthracycline use . interpretation in women with early breast cancer receiving adjuvant chemotherapy , the most powerful predictor of bene t from anthracyclines is ch17cep duplication . 
in view of the location of her2 / top2a on chromosome 17 , ch17cep duplication might explain the inconsistencies in previous studies of factors predicting bene t from anthracyclines . funding cancer research uk and the scottish breast cancer clinical trials group . introduction breast cancer is recognised as a disease of substantial molecular diversity.1 the search for predictive biomarkers that can be applied to guide selection of appropriate therapies for di erent patient subgroups is intensifying . 
 the her2 oncogene is frequently cited as a biomarker of sensitivity or resistance to endocrine treatment and chemotherapy.2 , 3 the her2 oncogene is ampli ed or overexpressed in about 25% of early breast cancer cases for which adjuvant anthracycline use is considered in the uk.4 several observational reports have linked anthracycline sensitivity to her2 positivity.5 , 6 her2 ampli cation is linked both to multiple mechanistic pathways ( proliferation , dedi erentiation , apoptosis , dna repair ) 7 and to several molecular events that are now viewed separately from her2 ampli cation , such as top2a alterations and chromosome 17 ( ch17 ) centromeric duplication.8 , 9 ch17 centromeric duplication indicates duplication of the ch17 centromere enumeration probe ( ch17cep ) 8 , 9 and is not necessarily an indicator of chromosomal duplication . 
data suggest polysomyde ned by duplication of the cepin fact represents duplication of subchromosomal regions , including the cep , rather than whole chromosome duplication.10 for this report , the term ch17cep duplication represents increased cep17 copies and should be interpreted in view of these emerging data . her2 might be the central focus or driver for a region of genomic instability centred around 17q12 , frequently being associated with ampli cation or deletion of other genes within this region including grb7 , rara ( retinoic acid receptor ) , thra1 , cdc6 , and top2a . 
her2 ampli cation is also closely associated with ch17cep duplication.9 ch17 is the second most gene - dense chromosome in the human genome , housing several genes with key roles in breast cancer ( brca1 , her2 ) and dna repair ( tp53 , rad51c , rad52b ) .11 however , 266 vol 11 march 2010 articles ch17cep duplication has not been mechanistically linked to these pathways , which makes the key molecular change associated with clinical bene t from anthracyclinebased chemotherapy di cult to identify . 
 research so far has focused almost exclusively on her2 and top2a , both of which have been linked to anthracycline sensitivity.6 , 12 nevertheless , genes such as brca1 , rad51c , and tp53 , all with a role in dna repair , might also modify response to chemotherapy . 
 the uk national epirubicin adjuvant trial ( neat / br9601 ) trials examined the addition of the anthra cycline epirubicin to cyclophosphamide , methotrexate , and uorouracil ( cmf )  . 
we planned prospectively to investigate markers predictive of anthracycline bene t , including type i receptor tyrosine kinase ( rtk ) signalling pathways ( epidermal growth factor receptor [ egfr ] , her1 , her2 , her3 ) , ki67 , top2a alterations , and ch17cep duplication . 
data for her13 , ki67 , and top2a in the br9601 study were reported previously.12 methods study design and patients neat and br9601 recruited 2391 pre - menopausal and post - menopausal women with completely excised , histologically con rmed breast cancer with a clear indication for adjuvant chemotherapy.14 the 2021 patients in neat were randomly assigned , in a 1 : 1 randomisation , to receive either epirubicin ( 100 mg / m intravenously every 3 weeks ) for four cycles followed by cmf ( cyclophosphamide 100 mg / m orally days 114 or cyclophosphamide 600 mg / m days 1 and 8 , intravenously ; methotrexate 40 mg / m days 1 and 8 ; uorouracil 600 mg / m days 1 and 8 every 4 weeks ) for four cycles or to receive cmf for six cycles . 
the 370 patients in br9601 were randomly assigned , in a 1 : 1 randomisation , to receive either epirubicin ( 100 mg / m every 3 weeks ) for four cycles ( cyclophosphamide 750 mg / m , methotrexate 50 mg / m , and uorouracil 600 mg / m every 3 weeks given intravenously ) for four cycles or to receive cmf for eight cycles.14 both protocols were approved by central and local ethics committees , and patients provided written informed consent before randomisation . 
there was a prospectively preplanned agreement for a joint analysis with the primary outcomes of relapse - free and overall survival.14 followed by cmf for the present study , routine pathology tissue blocks were retrieved from the neat / br9601 trials and tissue microarrays constructed according to current guidelines for breast tissue collections.15 blocks were retrieved and tissue microarrays constructed from 80% of neat samples ( 1623 / 2021 ) and from 86% of br9601 samples ( 318 / 370 ) for this study . 
 triple - colour uorescent in - situ hybridisation ( fish ) and immunohistochemistry fish was done with a triple - colour probe for her2 , top2a , and ch17 ( abbot vysis , maidenhead , uk ) as described previously.12 her2 ampli cation was de ned as a ratio of her2 to ch17cep of 20 or greater , top2a ampli cation as a ratio of top2a to ch17cep of more than 15 , and top2a deletion as a ratio of top2a to ch17cep of less than 08 . 
 table 1 : biomarker analysis and relation with overall and relapse - free survival 100 100 100 100 100 100 100 100 100 vol 11 march 2010 articles documented as previously described.16 , 17 ch17 copy number was assessed by counting all cells with a minimum of one ch17 signal per cell , and ch17cep duplication de ned as greater than 186 observed cep signals per cell.9 statistical analysis the 1941 eligible samples from this trial population would be adequate to identify , with at least 80% power , prognostic hazard ratios ( hrs ) of 15 and treatment by marker interactions of 20 , with the exception of top2a , for which the values would be 16 and 23 , respectively , owing to the lower frequency of top2a aberrations in this patient population.18 sas ( version 9.1 ) was used for statistical analysis . 
kaplan - meier and log - rank analysis were used to compare relapse - free and overall survival as described previously.19 hrs and their cis were calculated from log - rank statistics . 
graphical examination showed no clear departure from proportional hazards . the analysis planto assess the interaction of type i rtks ( her13 ) , ki67 , top2a , and ch17cepwas prospectively planned , before any statistical analysis and merging of biomarker and clinical data . 
 268 vol 11 march 2010 articles duplication , ki67 , and her13 were considered in univariate analyses , together with conventional prognostic factors ( age , nodal status , oestrogen - receptor status , grade , and tumour size )  . 
her2 , top2a , and ch17cep as individual markers were entered in a nal cox model together with the treatment term and each of the three treatment - by - marker interactions , with adjustment for conventional prognostic factors ( age , nodal status , oestrogen - receptor status , grade , and tumour size )  . 
 the study conformed to the remark guidelines.19 role of the funding sources the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results the population included in this tissue microarray study was representative of patient and tumour characteristics within the main trial ( webappendix p 1 )  . 
of the 1941 patients included in this analysis , 630 ( 32% ) relapsed and 516 ( 27% ) died during follow - up ( median 74 years , iqr 6386 ) ; data from one patient were lost . 
 vol 11 march 2010 articles number at risk ecmf 216 events ecmf 215 events 181 deaths 177 deaths 47 events 92 events 43 deaths 78 deaths number at risk ecmf years years figure 3 : relapse - free and overall survival for patients with tumours exhibiting ch17cep duplication and ch17cep normal ( a ) relapse - free survival for chcep17 normal . 
of the eligible cases , 367 of 1762 ( 21% ) were her2 ampli ed , and ch17cep duplication was recorded in 406 ( 23% )  . the prognostic e ect of each biological marker assessed in this study was rst tested with respect to relapse - free and overall survival in all 1762 patients , irrespective of their allocated adjuvant chemotherapy . 
in univariate analysis , her2 ampli cation , top2a deletion , and her13 and egfr expression were signi cantly associated with a worse outcome for both relapse - free and overall survival ( table 1 ) , although the e ect observed with egfr expression was of borderline signi cance . 
we noted no such relation with top2a ampli cation , ch17cep duplication , or ki67 expression ( table 1 )  . subsequent analyses focused on possible di erential e ects of markers on relapse - free and overall survival between patients receiving anthracycline treatment ( epirubicin and cmf ) and those given cmf alone . 
 figures 1 and 2 show hr estimates for relapse - free and overall survival by treatment and molecular biomarker subgroup , with biomarkers dichotomised as positive / high or negative / low . 
we detected no signi cant interactions between treatment with epirubicin and biomarker for ch17cep duplication was associated with increased bene t from epirubicin plus cmf compared with cmf ( gures 13 ) for both relapse - free and overall survival ( univariate treatment by marker interactions p = 0004 and p = 002 , respectively )  . 
for tumours with normal ch17cep copy number , very little or no bene t was derived from the addition of the anthracycline ( relapsefree survival hr 092 , 95% ci 076111 , gure 3a ; overall survival 094 , 077116 , gure 3c )  . 
conversely , for patients with tumours exhibiting ch17cep duplication , the relative risk of relapse and death was substantially lower for those receiving epirubicin and cmf than cmf ( relapse - free survival 051 , 95% ci 036 073 , gure 3b ; overall survival 056 , 039082 , gure 3d )  . 
 a single cox regression model was done to test the e ects of anthracyclines , her2 ampli cation , top2a alteration , and ch17cep duplication ( including interactions with treatment for each marker ) simultaneously after adjustment for age , nodal status , oestrogen - receptor status , grade , and tumour size ( table 2 )  . 
the interaction for ch17cep duplication and epirubicin therapy remained signi cant for both relapse - free and overall survival ( table 2 )  . 270 vol 11 march 2010 articles both her2 ampli cations and top2a alterations ( ampli cations or deletions ) measured by fish were signi cantly associated with ch17cep duplication ( p < 00001 )  . 
her2 - ampli ed tumours were twice as likely to exhibit ch17cep duplication as were those that were not ampli ed ( 37% [ 136 / 367 ] vs 19% [ 270 / 1395 ] , p < 00001 )  . 
 top2a ampli ed or deleted tumours were also signi cantly more likely to exhibit ch17cep duplication than were those that were not top2a altered ( 31% [ 52 / 169 ] vs 22% [ 354 / 1593 ] and 65% [ 124 / 191 ] vs 18% [ 282 / 1571 ] , respectively , webappendix p 2 )  . 
the hrs for relapse - free survival in patients with tumours exhibiting ch17cep duplication were 065 ( 95% ci 032129 ) with her2 ampli cation and 046 ( 026080 ) without ; similarly the hrs were 062 ( 033116 ) with top2a alterations and 046 ( 025 084 ) without . 
by contrast , in patients whose tumours did not show ch17cep duplication , hrs for relapse - free survival were 085 ( 050145 ) with her2 ampli cation and 0.91 ( 069121 ) without ; and 101 ( 051201 ) with top2a alteration and 091 ( 070119 ) without . 
this exploratory subgroup analysis ( gure 4 ) linked bene t from anthracyclines to ch17cep duplication irrespective of her2 ampli cation or top2a alterations . discussion in a prospectively planned and adequately powered analysis of biomarkers of anthracycline bene t within the neat / br9601 clinical trials , ch17cep duplication , but not her2 or top2a , was identi ed as a predictive biomarker of anthracycline bene t in early breast cancer . 
a signi cant treatment - by - marker interaction was recorded for both relapse - free and overall survival in multivariate analyses corrected for conventional pathological factors and also for treatment - by - marker interactions for her2 and top2a . 
a signi cant reduction in the risk of both relapse and death after treatment with anthracycline - containing chemotherapy regimens was noted in patients whose tumours showed evidence of ch17cep duplication . 
we also noted a signi cant treatment - by - marker interaction between treatment with anthracycline - containing polychemotherapy and ch17cep duplication . suggested ki67 previous evidence from smaller , underpowered , ( proliferation ) , her13 analyses expression , top2a , and her2 as potential biomarkers of anthracycline bene t ; 2 , 6 , 12 , 2023 however , these markers provided no signi cant predictive value in the present study . 
validation in a large meta - analysis is planned to con rm this e ect and to lend support to adoption of this biomarker in routine clinical practice . to the best of our knowledge , the data presented here represent the rst time that one can clearly de ne a hr ( 95% ci ) p value relapse - free survival age 50 years 112 ( 094133 ) breast conserving surgery 083 ( 069099 ) node involvement 183 ( 161207 ) < 00001 oestrogen - receptor negative 093 ( 073118 ) oestrogen - receptor positive 075 ( 060094 ) tumour grade tumour diameter ecmf her2 ampli cation top2a alteration ch17cep duplication her2 * ecmf interaction top2a * ecmf interaction ch17cep * ecmf interaction overall survival age 50 years 129 ( 110152 ) 101 ( 100101 ) 089 ( 072110 ) 161 ( 117221 ) 140 ( 099200 ) 143 ( 109187 ) 103 ( 066161 ) 090 ( 055149 ) 098 ( 081119 ) 054 ( 035083 ) 0005 breast conserving surgery 082 ( 067100 ) node involvement 173 ( 151198 ) < 00001 oestrogen - receptor negative 088 ( 069114 ) oestrogen - receptor positive 066 ( 052084 ) tumour grade tumour diameter ecmf her2 ampli cation top2a alteration ch17cep duplication her2 * ecmf interaction top2a * ecmf interaction ch17cep * ecmf interaction 134 ( 111160 ) 101 ( 100101 ) 092 ( 072116 ) 136 ( 093200 ) 137 ( 101184 ) 091 ( 056147 ) 085 ( 050145 ) 060 ( 038095 ) 184 ( 131258 ) 00005 022 004 053 001 0002 0002 027 0003 006 001 089 069 086 005 034 00008 0002 0005 047 012 004 070 054 003 adjusted for age group , surgery group , nodal group , oestrogen - receptor status , grade , and tumour size . 
ch17cep = chromosome 17 centromere enumeration probe . table 2 : e ect of her2 , top2a , and ch17cep on relapse - free and overall survival , adjusted by patient and tumour characteristics for whom subgroup of patientsthose with ch17cep duplication for whom adjuvant anthracyclines provide signi cant additional treatment bene t , while identifying a larger group alternative , non - anthracyclinecontaining regimens should be considered . 
these data remain of value at a time when trastuzumab is frequently used to treat patients with her2 - positive breast cancer , since about two - thirds of patients whose tumours have ch17cep duplication do not exhibit her2 ampli cation . 
by contrast with ndings reported here , ma5 indicated that bene t from anthracyclines was associated with her2 and top2a ampli cation.25 , 26 the reduction in risk of relapse was much the same for patients in both neat / br9601 and ma5 whose tumours exhibited ch17cep duplication when given an anthracycline rather than cmf alone ; no bene t was recorded in patients with tumours with normal ch17cep.24 no signi cant treatment - by - marker interaction for either her2 or top2a was detected in the multivariate regression analysis , although her2 gene ampli cation was , as expected , prognostic for both overall and relapse - free survival in both treatment groups . 
this nding strongly suggests that neither gene is of clinical signi cance in terms of predicting clinical bene t from adjuvant anthracyclines , and rea rms the strong prognostic e ect of her2 ampli cation . 
previous data from other groups22 , 2528 are , however , con icting , with some studies suggesting her2 and others her2 and top2a as potential predictive markers for anthracycline bene t . 
preliminary results of a meta - analysis30 using individual patient data in 1944 cases from four clinical trials , 12 , 22 , 26 , 27 including 295 of the br9601 trial patients reported here , also showed no signi cant predictive e ect with her2 , and only a marginally signi cant e ect for top2a for disease - free but not overall survival . 
we believe that many previous smaller studies lacked the power to robustly test interactions , and that neither her2 ampli cation nor top2a gene alterations can be regarded as predictive for response to anthracyclines . 
a review of previously published studies ( webappendix p 3 ) accords with these con icting results.22 , 2528 , 3133 only the ma5 trial shows a signi cant interaction with her2 ; an early study by paik and colleagues32 of similar size to our study , but using only immunohistochemistry , also did not show a signi cant interaction between her2 and anthracyclines . 
 ki67 was not associated with bene t from anthracyclines , a result that does not contradict previous results , suggesting highly proliferative tumours bene t preferentially from chemotherapy . of note , her2 and top2a ampli cation and top2a deletion were signi cantly associated with ch17cep duplication , but the bene t from the anthracycline seemed to be restricted to patients whose tumours exhibited ch17cep duplication ( gure 4 )  . 
patients whose tumours were either her2 ampli ed or top2a ampli ed or deleted , but were normal for ch17cep , gained no apparent bene t from addition of the anthracycline ( gure 4 )  . 
this result also suggests that in our own previous report , 12 on her13 expression in the br9601 subgroup within the current trial , the small sample size masked the e ect reported here . 
cmf = cyclophosphamide , methotrexate , uorouracil . 272 vol 11 march 2010 articles duplication in top2a deleted cases in particular could explain the previously paradoxical result that these patients bene t from anthracyclines when other data suggest that top2a deleted cell lines are anthracycline resistant.22 , 34 the results of the bcirg006 study6 suggest that in a population , all of whom have tumours that are her2 ampli ed , there might be an additional e ect of top2a ampli cation , although the role of ch17cep duplication has not been explored in bcirg006 so far . 
 our present data do not rule out such an additional e ect of top2a in her2 - positive cancers since our study was done in a mixed her2 population , and might be underpowered to detect any additional e ect of top2a above that seen for ch17cep in the her2ampli ed subgroup . 
we de ned ch17cep duplication as an increase in the relative mean copy number of the cep , which hybridises to the pericentromeric - satellite repeat on ch17 , above that observed in non - tumour breast tissues.9 although there are several di erent approaches used to identify cep17 duplication , only two have been validated against observations in non - neoplastic breast samples.9 , 35 the di erent cuto s in these studies relate solely to di erent counting assumptions ( watters and colleagues9 count all cells with at least one ch17cep signal ; wang and colleagues35 count cells with at least two ch17cep signals ) , but in all other aspects they are identical . 
our approach does not invalidate previous de nitions of her2 ampli cation since these de nitions were also based on the ratio of the her2 gene and the ch17 centromere , irrespective of the underlying chromosomal defect present . 
our de nition of her2 ampli cation still identi es patients with poor prognosis , her2 protein overexpression , and potential for response to trastuzumab . including the observation that ch17cep duplication is associated with bene t from anthracyclines could o er a pragmatic approach to selection of patients for such therapy . 
recent reports suggest that ch17 polysomy is far less common in early breast cancer than was previously suggested , and that ch17cep duplication does not simply indicate polysomy or tumour aneuploidy but also identi es cancers with subchromosomal duplication or ampli cation of the ch17cep region ( which is close to the her2 amplicon ) .10 , 36 at present we cannot distinguish which of these di erent chromosomal abnormalities might be associated with the underlying mech anism of anthracycline sensitivity . 
the many mechanistic explanations for the observations reported here should be explored before we can suggest strategies to improve the future potential of dna - damaging agents in populations who are resistant to anthracyclines . trial population in conclusion , in this large , adequately powered , ( neat / br9601 ) , ch17cep clinical duplication , but not her2 or top2a , was identi ed as a biomarker of anthracycline bene t in patients with early breast cancer . 
validation in a larger meta - analysis is needed to provide con rmatory evidence to support the adoption of this biomarker in routine clinical practice . contributors jmsb was responsible for translational study design , coordination , data collection , statistical analysis plan , management of biological data , and the writing of the report . 
afm was responsible for collection of tissue from br9601 , tissue microarray construction , doing the molecular analyses and scoring of samples , and coordinating the data collection ; and contributed to the writing of the report . 
 ep , he , pp , and cc were responsible for setting up pathological review of all the tumour samples from the neat trial , guiding tissue microarray construction , and development and maintenance of the associated translational research databases . 
all other authors declared that they have no con icts of interest . acknowledgments the scottish cancer therapy network and institute for statistics and disease coordinated the br9601 trial and provided funding for tissue collection of br9601 blocks ; the neat trial was coordinated by the cancer research uk clinical trials unit , birmingham , and funded by cancer research uk and an educational grant from pharmacia ; the translational research was funded by cancer research uk , and vysis provided fish kits at reduced price . 
abbott provided funding in kind via free or reduced price reagents . vol 11 march 2010 articles articles cancer survival in ve continents : a worldwide population - based study ( concord ) michel p coleman , manuela quaresma , franco berrino , jean - michel lutz , roberta de angelis , riccardo capocaccia , paolo baili , bernard rachet , gemma gatta , timo hakulinen , andrea micheli , milena sant , hannah k weir , j mark elwood , hideaki tsukuma , sergio koifman , gulnar azevedo e silva , silvia francisci , mariano santaquilani , arduino verdecchia , hans h storm , john l young , and the concord working group * summary background cancer survival varies widely between countries . 
the concord study provides survival estimates for 19 million adults ( aged 1599 years ) diagnosed with a rst , primary , invasive cancer of the breast ( women ) , colon , rectum , or prostate during 199094 and followed up to 1999 , by use of individual tumour records from 101 populationbased cancer registries in 31 countries on ve continents . 
 methods to compensate for wide international di erences in general population ( background ) mortality by age , sex , country , region , calendar period , and ( in the usa ) ethnic origin , we estimated relative survival , the ratio of survival noted in the patients with cancer , and the survival that would have been expected had they been subject only to the background mortality rates . 
5 - year relative survival for breast , colorectal , and prostate cancer was generally higher in north america , australia , japan , and northern , western , and southern europe , and lower in algeria , brazil , and eastern europe . 
concord has provided the rst opportunity to estimate cancer survival in 11 states in usa covered by the national program of cancer registries ( npcr ) , and the study covers 42% of the us population , four - fold more than previously available . 
relative survival for all ethnicities combined was 24% lower in states covered by npcr than in areas covered by the surveillance epidemiology and end results ( seer ) prograage - standardised relative survival by use of the appropriate racespeci c and state - speci c life tables was up to 2% lower for breast cancer and up to 5% lower for prostate cancer than with the census - derived national life tables used by the seer prograthese di erences in population coverage and analytical method have both contributed to the survival de cit noted between europe and the usa , from which only seer data have been available until now . interpretation until now , direct comparisons of cancer survival between high - income and low - income countries have not generally been available . 
the ndings should eventually facilitate joint assessment of international trends in incidence , survival , and mortality as indicators of cancer control . funding centers for disease control and prevention ( atlanta , ga , usa ) , department of health ( london , uk ) , cancer research uk ( london , uk )  . 
 introduction international comparisons of population - based cancer survival have been rare , 15 but large and unexplained di erences in survival have been reported for many cancers from individual studies and cancer registries in europe and north america.6 for example , 5 - year relative survival for women diagnosed with breast cancer during 198589 was 73% in europe ( weighted mean for 17 countries ) 7 and 84% in the usa.8 the concord study provides a systematic comparison of survival between europe and north america , 916 extended to countries in all other continents . the rst international comparison of cancer survival , published in 1964 , 17 was a study of patients diagnosed with one of 15 common cancers in denmark , england , finland , france , norway , sweden , and the usa , mainly during 194554 . 
it was the rst study in which relative survival techniques , rst described in the 1950s , 1820 were used to correct the survival estimates for di erences in background mortality between participant countries . 
the ndings are mainly of historical interest , but survival in the usa ( represented by connecticut ) was generally higher than in the european countries . cancer survival is known to vary between the regions of the usa covered by the us national cancer institutes ( nci ) surveillance , epidemiology and end results ( seer ) program , 21 but the range of survival in europe is much wider . 
concord also enables comparison of cancer survival between ve states and four metropolitan areas in the usa covered by the seer program ( seer - 9 ) and 11 states covered by the centers for disease control and preventions ( cdc ) national program of cancer registries ( npcr )  . 
it also provides a wider comparison of cancer survival between black and white patients in the usa than has previously been possible . concord includes data from one or more countries on all ve continents . 
to our knowledge , it is the rst attempt at a global comparison of cancer survival . methods cancer registries in 1999 , we identi ed at international cancer meetings in atlanta ( usa ) and lisbon ( portugal ) , and from published studies , population - based cancer registries that had published survival data and were operational during 199099 . 
in total , we identi ed 112 registries , but 11 were withdrawn or excluded : no response ( one ) ; withdrawal for legal reasons ( one ) ; incomplete registration before 1995 ( four ) ; follow - up activity stopped be fore 1999 ( two ) ; data not supplied by the september , 2005 deadline ( three )  . a pilot study of 50 registries in 2000 obtained a 100% response . 
all registries were able to provide data for patients diagnosed during all or part of the period 199094 , and had access to various data sources to obtain follow - up information for all patients for at least 5 years or to the end of 1999 . 
after further recruitment , a detailed questionnaire was obtained for 100 of the 101 registries nally included in the analyses , covering data de nitions and methods of operation , including data collection , coding of tumour site , morphology , behaviour , and stage at diagnosis , tracing of registered patients to ascertain their vital status , and linkage between data on the incident tumour and data on subsequent death or loss to follow - up . 
the procedures and de nitions used , the stated quality and completeness of data on the registration of incident cancers , and of the follow - up of those patients over the next 5 years , were deemed adequate to attempt cancer - survival analysis , subject to central quality control of the data . 
we retained hawaii ( usa ) with north america rather than oceania . africa was represented by a single cancer registry , for the wilaya ( dpartement , or state ) of stif ( algeria )  . central and south america , including the caribbean , were represented by the national cancer registry of cuba and two regional registries in brazil : the goinia ( gois state ) registry is one of 20 registries in state capitals , whereas the campinas ( so paulo state ) registry is the only one in brazil that is not in a state capital . data from north america include ve of the seven largest provinces in canada ( british columbia , manitoba , nova scotia , ontario , and saskatchewan )  . 
data for the usa came from 22 registries covering 16 states ( california , colorado , connecticut , florida , hawaii , idaho , iowa , louisiana , michigan , nebraska , new jersey , new mexico , new york state , rhode island , utah , and wyoming ) and six metro politan areas ( atlanta , ga , los angeles , ca , san fran cisco , ca , detroit , mi , new york city , ny , and seattle , wa )  . population - based cancer registries in the usa receive sup port from either or both of the two federal cancersurveillance programmes , the ncis seer program and the cdcs npcr.36 as of 1990 , the seer program in cluded nine population - based cancer registries covering some 10% of the us population ( seer - 9 ) : the states of connecticut , hawaii , iowa , new mexico , and utah , and the metropolitan areas of atlanta , ga , detroit , mi , san francisco , ca , and seattle , wa . 
the los angeles cancer registry be came a seer registry in 1992 , but we opted to retain it with the npcr data , so that the seer grouping vol 9 august 2008 articles we used was identical with that for which seer data had been published in the past ( seer - 9 )  . 
we received separate datasets from detroit , mi , san francisco , ca ( seer registries ) , and los angeles , ca ( npcr ) , and these were included in the respective totals for seer and npcr . 
 however , the data from these metropolitan areas could not be separately identi ed in the state - wide datasets we received from california and michigan , therefore , the nonmetropolitan data for those states could not be included with the other npcr data . 
 table 1 : population coverage and number of adults ( aged 1599 years ) diagnosed with cancer of the breast , colon , rectum , or prostate during 199094 * and included in the analyses : continent , country , and region 734 vol 9 august 2008 articles npcr : colorado , florida , idaho , los angeles , ca , louisiana , nebraska , new jersey , new york , rhode island , and wyoming . 
for this comparison , data from the non - metropolitan areas of california and michigan were ex cluded to ensure that the two sets of data were mutually exclusive . in asia , japan was represented by three of the prefectural ( state ) registries : fukui , osaka , and yamagata . in europe , the 53 cancer registries that contributed data to eurocare - 328 on cancers of the breast , colon , rectum , or prostate all participated in the concord study . 
six other registries also provided data : two national registries ( northern ireland and ireland ) and four regional registries from the netherlands ( north ) and switzerland ( graubunden - glarus , st gallen - appenzell , valais )  . 
in england , both the national cancer registry and eight of the regional cancer registries submitted datasets . oceania was represented by the national cancer registry of australia , with data from each of the eight populationbased state or territorial registries . quality control procedures used in the eurocare - 3 study were applied to all datasets . 
tumour records were supplied with the anatomical site coded to the ninth revision of the international classi cation of diseases ( icd - 939 ) for four index tumours : cancers of the breast ( women ) ( icd - 9 174.0174.9 ) , colon ( 153.0153.9 ) , rectum ( including the anus , 154.0154.9 ) , and prostate ( 185 )  . 
tumour morph ology and behaviour were coded to the rst or second revision of icd - oncology ( icd - o , 40 icd - o - 241 )  . 
the duration of survival was taken from the date of diagnosis of the index tumour until death from any cause , or until the patient was censored from the analysis as alive , either at loss to follow - up or after dec 31 , 1999 , whichever came rst ; any subsequent tumour occurring in the same patient during that period was ignored . standard quality - control routines , based on those developed by the international agency for research on cancer , 42 were applied to each tumour record . 
corrected tumour records were checked again : those which still had missing , invalid or inconsistent values for sex , site , morphology , or dates were agged as major errors and excluded from analysis . 
 records for which an unlikely combination of age , site and morphology had nonetheless been con rmed as correct were agged as minor errors , and included in the analyses . 
 details of the approach have been published else where.43 detailed quality - control ndings are available online.34 follow - up all registries used more than one mechanism of follow - up to ascertain the vital status ( alive , dead , emigrated , lost to follow - up ) and the date of the last vital status for each registered patient . 
secure linkage of a tumour record and a record of death , based on a set of identi ers such as name , sex , date of birth , and personal identity number , enabled the registry to update the tumour record accordingly . 
 a wide variety of administrative data bases was also used , such as social insurance , health insurance , motor vehicle records , drivers licences , hospital discharge records , national primary - care databases , electoral registers ( those eligible to vote ) , and voter registration records ( those who voted in the last election )  . 
this is subject to administrative error ( failure to remove in timely fashion the record of a person known to be dead ) and fraud ( by someone seeking to retain access to bene ts received by the deceased ) , but in most instances the risks are small . 
 if coverage of the databases was known to be high , and especially if a person was present in more than one such database , the risk of error decreased further . in the usa , a match to an administrative database might show that an event occurred during a certain quarter of a year ( eg , an insurance claim paid , a licence renewed ) , but the exact date might not be known ; the date of last vital status was then set to the rst day of the quarter , ie , jan 1 , april 1 , july 1 , sept 1 . 
this approach can give rise to irregu lar distribu tions of the day of last known vital status , but it is a conservative approach to establishing when patients were last known to be alive , because patients are censored from sur vival analysis on the latest of any such dates in the record . the proportion of patients not known to be dead and for whom the registry could not be certain that the date of last vital status was at least 5 years after diagnosis was less than 1% overall . 
such patients are described as censored from the analysis . statistical analysis we estimated relative survival up to 5 years after diagnosis from the individual tumour data , using the hakulinen approach44 embedded in the us national cancer institutes publicly accessible seer * stat software.45 seer * stat is the standard tool used for cancer - survival estimation by the seer program cancer registries , and we used it to ensure that survival estimates for us registries would be seen as comparable with those already published by the seer prograsurvival estimates were also derived by race for the usa ( black and white )  . relative survival is the ratio of the survival noted in the patients with cancer and the survival that would have been expected had they been subject only to the mortality rates of the general population ( background mortality )  . 
it is a measure of the excess mortality in patients with cancer over and above the background mortality , and can be interpreted as survival from the cancer after correction for other causes of death . 
background mortality was taken from life tables developed specially for the concord study , speci c for sex , calendar year , region , and race.46 the probability of survival in successive years after diagnosis was estimated in survivors to the start of each year . 
95% cis were calculated by use of a logarithmic transformation ( see text )  . table 2 : 5 - year relative survival ( % ) , age - standardised to icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colon , rectum , or prostate during 199094 and followed up to dec 31 , 1999 : continent , country , and region 738 vol 9 august 2008 articles see online for webtable for heterogeneity in the withdrawal of patients from followup and consequent changes in the age - sex - race distribution of patients with cancer in successive calendar years , by use of the exact method.44 expected survival was derived from complete life tables that contained the probabilities of death or the central death rates for the general population of the registrys territory , by single year of age , sex and ( where possible ) race , and single calendar year between 1990 and 1999 . 
for some registries , complete life tables were constructed from raw data obtained from published sources on the numbers of deaths by age , sex , and race in the relevant year ( s ) or period , and the corresponding populations . 
race - speci c estimates of relative survival were produced with separate life tables for each race , constructed from the raw data on populations and the number of deaths.46 in the usa , race - speci c mortality in the general population also varies between states.36 we developed separate sets of complete life tables for each state and metropolitan area and for each sex . 
this approach was designed to enable the closest possible adjustment of relative survival estimates in the usa for geographic variation in background mortality in both blacks and whites , by age , sex , and calendar period . 
for ve less populous states ( hawaii , idaho , new mexico , utah , and wyoming : 6% of the 109 million population covered by participating registries ; webtable ) , only the life tables for whites were su ciently robust , and relative survival estimates for blacks are not separately presented . relative survival measures the extent to which patients with cancer have a higher death rate than the general population of the country or region in which they live.56 occasionally , despite use of the most appropriate life table , this excess death rate can be negative in a given time interval since diagnosis , implying that the death rate of cancer survivors during that interval is actually lower than that of the general population . 
this situation can arise from random variation in the death rate when the number of deaths in the interval is small , 57 either because the interval is very short , or because survival is poor and most patients have already died before the start of the interval , or because survival is high and there are very few deaths . 
in such situations , we present by default the estimate derived by use of the seer * stat option to constrain the excess mortality rate to zero , which imposes a plateau in the relative survival curve . 
the unconstrained estimate was also obtained for comparison . even though relative survival is already adjusted for agespeci c di erences in background mortality , robust international comparison of relative survival requires agestandard isation , 23 because the age distribution of patients with cancer varies between countries , and because relative survival also varies widely by age , at least in europe.27 conventional age - speci c weights used to standardise incidence or mortality rates ( eg , the national population or the hypothetical world standard population58 ) are unsuitable because patients with cancer have a very di erent age pro le from that of the general population . a cancer - survival comparison of such wide scope has not been done before and the choice of weights for agestandardisation was not straightforward . 
international stan dard cancer - patient populations have been proposed , with di erent sets of weights in 5 - year or 10 - year age bands for each of 20 common cancers , derived from their worldwide distribution.59 the weights used for the eurocare - 3 study were derived from the age distribution of all patients included in that study for each cancer , and were thus cancer - speci c.43 the disadvantage of these standards is either that a unique set of weights is required for each cancer ( cancer - speci c ) , or else that the standards are arbitrary ( study - speci c ) , vitiating comparison between studies . we chose the recently developed international cancer survival standard ( icss ) weights.60 these comprise just three sets of age weights , derived from discriminant analysis to nd the smallest number of sets of standard age weights that enable adequate standardisation of survival . 
where data were too sparse for standardisation , the raw ( unstandardised ) survival estimate is presented , agged with r . the same age weights were used for men and women , and for each race , enabling direct comparison of agestandardised relative survival between patient groups de ned by sex and race . 
this would not be possible if cancer - speci c weights were used . vol 9 august 2008 articles figure 1 : 5 - year relative survival ( % ) , agestandardised to the icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colorectum , or prostate during 199094 and followed up to dec 31 , 1999 : country vertical bar on the right of each graphic shows the contribution ( % ) of each continent to the total number of cases analysed ( contributions under 1% are not labelled )  . 
 * agestandardised to icss weights , except for stif , algeria ( all cancers ) , malta ( prostate ) , and portugal ( prostate ) , which were unstandardised values ( see text )  . 
 740 cuba canada sweden japan australia finland france italy iceland spain netherlands norway switzerland germany austria denmark malta portugal northern ireland scotland england ireland wales slovenia poland czech republic estonia brazil slovakia algeria cuba france canada australia japan sweden malta norway netherlands austria germany spain iceland finland italy ireland northern ireland denmark scotland england portugal brazil wales slovakia czech republic slovenia estonia poland algeria breast ( women ) prostate colorectum ( women ) colorectum ( men ) 417 507 430 469 austria canada australia germany france iceland cuba netherlands sweden italy norway finland ireland spain estonia scotland northern ireland england czech republic japan brazil wales portugal slovakia malta slovenia denmark poland algeria japan cuba australia france canada netherlands sweden austria spain finland norway italy germany iceland northern ireland brazil portugal ireland scotland denmark england wales estonia slovenia malta slovakia czech republic poland algeria 263 656 433 457 5 - year relative survival ( % ) 5 - year relative survival ( % ) africa america , central and south america , north asia europe oceania data covering less than 100% of country vol 9 august 2008 articles figure 2 : 5 - year relative survival ( % ) , using statespeci c and race - speci c life tables and age - standardised to the icss weights * for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colon , rectum , colon and rectum combined , or prostate during 199094 and followed up to dec 31 , 1999 : 16 us states and six metropolitan areas vertical lines represent mean survival for seer ( red ) and npcr ( green ) registries , agestandardised to icss weights ( see text )  . 
 problems with data quality might have led to overestimation ( see text )  . vol 9 august 2008 articles for countries represented by more than one regional cancer registry , we provide a survival estimate derived from the pooled data for all contributing registries , agestandardised in the same way . 
we used these standard errors to estimate cis on the logarithmic scale ( webpanel )  . for the usa , we constructed funnel plots of relative survival for each cancer and sex , to obtain further insight into the variability of survival by race and state , and to avoid spurious ranking of the survival estimates.62 the plots show how much a particular survival estimate deviates from the pooled us value , given the precision of for each estimate . 
the precision depends on the number of deaths included in the analysis , which depends in turn on the size of the popu lation and the frequency and lethality of the cancer in that population . 
5 - year relative survival estimates for each popu lation , age - standardised race - speci c and state - speci c and adjusted background mortality , were plotted against the precision of the estimates , taken as the inverse square of their standard errors ( webpanel )  . 
the horizontal line in each plot , the target , was estimated as the pooled 5 - year relative survival for all participating us populations , agestandardised to the same weights . 
see text for attribution of registries to npcr and seer . r = raw ( not age - standardised ) survival estimate : too few cases in one or more age groups . 
black populations are not shown separately for hawaii , idaho , new mexico , utah , or wyoming , because it was not possible to estimate relative survival for blacks in these states with race - speci c life tables ( see text )  . table 3 : 5 - year relative survival ( % ) by use of state - speci c and race - speci c life tables and age - standardised to icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the breast ( women ) , colon , rectum , or prostate during 199094 and followed up to dec 31 , 1999 , by race : us populations vol 9 august 2008 articles di erences between survival estimates are presented as the absolute value , eg , 15% is given as 5% ( not 50% ) higher than 10% . we analysed individual data for almost 2 million adults who were diagnosed with a rst , primary , malignant , invasive neoplasm of the breast ( women ) , colon , rectum , or prostate during the period 199094 and who had been followed up to ascertain their vital status for at least 5 years after diagnosis until the end of 1999 or later . 
data were contributed by 101 population - based cancer regis tries covering a combined population of almost 300 million persons living in 31 countries ( table 1 and web gure 1 )  . 
 the 24 european countries contri buted 740 000 patients ( 37% ) from a population base of 126 million , indicating lower mean incidence of cancer than in north america . the smallest dataset came from stif ( algeria ) , covering a population of 11 million , some 4% of the national population . 
the registry could only provide data for the period 199294 , the population is young , and cancer risks are currently low on the global scale.63 the dataset was therefore small , a total of 300 patients . 
this decreases the statistical precision of survival estimates , but no patient was detected solely at death certi cation or autopsy , and the vital status of every patient was ascertained at a home visit by registry sta , something no other registry could deliver . 
california provided the largest single dataset of 240 000 patients diagnosed during 199094 in a population of 31 million ( 12% of the us population ) , with a very high cancer risk on the global scale ( table 1 )  . for 16 of the 31 countries , the data covered 100% of the national population ( table 1 )  . 
the proportion of the national population covered by the data for the other 15 countries ranged from less than 10% ( algeria , brazil , japan , austria , czech republic , france , germany , poland ) to 1029% ( italy , portugal , spain , switzerland ) and 30% or more ( canada , usa , the netherlands )  . most registries provided data on patients diagnosed during the entire 5 - year period 199094 , but ten registries provided data for shorter periods ( table 1 )  . data for all four index cancers were provided by 89 of the 101 registries . 
two specialised registries in cte - dor ( france ) only collect data on cancers of the breast or colorectum , respectively , whereas ten general registries that collect data for all cancers only contributed data for selected cancers : breast ( isre , france ; northern netherlands ; all ve swiss registries ) ; breast , colon , and prostate ( campinas , brazil ; nova scotia , canada ) , or breast , colon , and rectum ( granada , spain ; table 1 )  . ethical approval for the concord study33 was obtained from the istituto superiore di sanit , rome , italy ( ce - iss 02 / 03 , may 20 , 2002 ) and from the institutional review board of the cdc , atlanta , ga , usa ( irb #3551 , july 24 , 2002 )  . 
seer data were obtained from the public - use dataset.38 for other registries , anonymised data were transmitted to the concord data analysis centre at the istituto superiore di sanit by use of special courier delivery of encrypted and password - protected cd - roms with separate email transmission of the password , or preplanned deposition of password - protected les on a specially created file transfer protocol ( ftp ) site from which the data were immediately removed in rome . 
each tumour record included a serial number for the purposes of quality control with the originating cancer registry . role of the funding source the pilot study ( january , 2000 to march , 2000 ) was funded by the uk department of health ( 75 000 )  . 
the cdc funded data collection and the costs of linkage to the national death index for the phase i study in participating registries in the national program of cancer registries ( us$3 million )  . 
the cancer survival group ( including br , mq ) in the london school of hygiene and tropical medicine , london , uk , has been funded by cancer research uk ( grant c1336 / a5735 ) since april , 2005 . 
the corresponding author had full access to all of the data and the nal responsibility to submit for publication . results the background risk of death in the general population varied widely between the participating countries and regions . 
the mean life expectancy at birth during the decade 199099 ranged from 637 to 776 years in men and from 709 to 837 years in women.46 in the usa , the range of life expectancies in white and black populations did not overlap at all in the states and metropolitan areas for which life tables could be con structed for both groups . 
 the ranges for men were 640701 years in blacks and 711759 years in whites , whereas the ranges in women were 733765 years in blacks and 788809 years in whites . 
 the cumulative risk of death from all causes over the age range 1559 years in the general population of the participating countries and regions ranged widely , from 9% to 34% in men and from 5% to 17% in women . 
over the age range 6084 years , the cumulative risk of death ranged from 60% to 86% in men and from 40% to 75% in women.46 of 785 255 records of breast cancer submitted for analysis , 45 020 ( 6% ) related to women registered with a previous primary cancer , and were excluded ( available online34 ) of the 740 235 eligible rst primary invasive breast cancers , 9215 records were excluded as death - certi cateonly ( dco ) registrations ( 1% ) , 239 as autopsy - detected tumours ( < 1% ) and 2064 with major errors ( < 1% ) , leaving 728 717 patients for analysis ( 98% of those eligible ) , of whom 370 000 ( 51% ) were resident in north america and 304 000 ( 42% ) in europe ( table 1 )  . 
almost all ( 97% ) of the 744 vol 9 august 2008 articles see online for web gures 2 and 3 tumours included in the analyses were microscopically veri ed , less than 1% of patients were censored from the analysis within 5 years of diagnosis , and 23% died within 1 month of diagnosis . relative survival at 5 years , age - standardised to the international cancer survival standard weights , ranged from 80% or over in north america , sweden , japan , finland , and australia to less than 60% in brazil and slovakia , and below 40% in algeria ( table 2 and gure 1 )  . 
 survival in the 24 european countries that contributed to concord was mostly in the range 7079% . the survival estimate of 388% ( 95% ci 314462 ) for stif ( algeria ) is based on 180 patients , and it is not agestandardised because there were too few patients for analysis in some age groups , but age - standardisation for breast cancer in other datasets rarely altered the raw estimate by more than 5% in either direction ( data not shown ) , and survival from breast cancer was undoubtedly much lower in algeria than in all the other countries . the pooled estimate of 5 - year survival for the two brazilian registries was 584% , but the estimate for goinia ( 654% ) is more reliable than the very low gure for campinas ( 366% ) , where high proportions of patients were excluded as dco or with major errors ( available online34 )  . 
the 5 - year survival estimate for cuba was 840% , but this was likely to be an over - estimate : some 28% of records were excluded because they were registered solely from a death certi cate . the pooled estimate of 5 - year survival for canada was 825% , with a narrow range from 793% in nova scotia to 854% in british columbia ( table 2 and gure 1 )  . 
in the usa , 5 - year relative survival for all races combined ranged from 7881% in new york city , new york state , and louisiana to 8990% in hawaii and seattle , wa ( table 2 ) , but most of the estimates were within a fairly narrow range , from 82% to 87% ( gure 2 )  . 
survival in metropolitan areas covered by seer registries was similar to that in the respective states : detroit , mi 830% and michigan state 823% ; san francisco , ca 862% and california state 846% . 
5 - year survival was 774% for residents of new york city , ny ( with 40% of the state population ) , slightly lower than for new york state as a whole , 810% . survival was lower for blacks than for whites in all 17 populations in the usa for which this could be assessed with race - speci c life tables ( web gure 2 )  . 
the range in survival was wider for blacks ( 6083% ) , but the values at both extremes of the range were based on relatively few patients and have wider cis . 
within a given us population , the absolute di erence in age - adjusted relative survival between blacks and whites ranged from 2% ( rhode island , nebraska ) to 2527% ( iowa and seattle , wa ; table 3 and web gure 2 )  . 
even in areas where blacks comprise 25% or more of the population , survival for black women was 814% below the lowest estimate for white women ( 796% ) in any of the participating areas : atlanta , ga ( 711% ) , detroit , mi ( 717% ) , new york city , ny ( 658% ) , and louisiana ( 699% )  . 
the pooled estimate of 5 - year survival for the usa was 840% , with 861% in areas covered by seer and 831% in areas covered by npcr ( table 3 )  . survival in black women was always lower than the mean survival for all us populations included , and often more than three standard deviations below it ( below the 998% control limits ) , after controlling for the precision of the estimates . 
survival in white women is generally within or above the upper control limits , especially in territories covered by the seer prograa notable exception is for white women in new york state , including new york city , where the survival estimates are precise , but well below the lower control limits ( web gure 3 )  . the pooled estimate of 5 - year survival for breast cancer in japan was 816% . 
survival in osaka ( 794% ) was lower than in fukui ( 831% ) and yamagata ( 873% ; table 2 and gure 1 )  . 5 - year relative survival for breast cancer in europe , agestandardised to the icss weights , ranged from 579% in slovakia to 820% in sweden ( table 2 and gure 1 ) , whereas the pooled estimate derived from the data of 58 registries in the 24 participating european countries was 731% . 
 survival estimates for most of these countries have been reported.27 the concord study includes additional data from four countries : 5 - year survival was 696% in ireland and 720% in northern ireland , similar to the uk mean value of 697% ( table 2 )  . 
in switzerland , 5 - year survival in the cantons of st gallen - appenzell , graubunden - glarus , and valais was 7275% , about 47% lower than in geneva or basel . 
5 - year survival was 778% in northern netherlands , similar to that in amsterdam and southern netherlands ( 7678% )  . the national estimate of 5 - year survival for breast cancer in australia was 807% . 
survival was virtually identical in the six largest states ( 96% of the national population ) , in the range 8082% , but notably lower in the two smallest regions : 719% in northern territory ( 10% of the population ) and 771% in tasmania ( 26% )  . of 488 741 colon cancer records submitted for analysis , 45 862 records ( 9% ) were excluded for a previous cancer , leaving 442 879 rst , primary , invasive colon cancers eligible for analysis ( available online34 )  . 
a further 13 102 ( 3% ) were excluded as dco registrations , 1534 ( < 1% ) as autopsydetected tumours , and 1144 ( < 1% ) as major errors , leaving 427 099 patients for inclusion in the analyses ( 96% of those eligible )  . 
almost 11% of patients died within the rst month after diagnosis . relative survival at 5 years , age - standardised to the icss weights , ranged from about 60% in north america , japan , australia , and some western european countries down to vol 9 august 2008 articles see online for web gure 4 40% or less in algeria , brazil , czech republic , estonia , poland , slovenia , and wales ( table 2 and gure 3 )  . the survival estimates of 114% ( 95% ci 07409 ) for men and 306% ( 95561 ) for women in stif ( algeria ) were based on fewer than 20 patients , and are not agestandardised , but survival was clearly lower in algeria than in all the other countries . the estimate of 5 - year relative survival for goinia ( 481% in men , 448% in women ) was more plausible for brazil than the low estimates for campinas , where 26% of patients had to be excluded with errors.34 5 - year survival in cuba was about 60% in both sexes , although more than half the patients were excluded from analysis as dcos.34 in canada , the pooled estimate of 5 - year survival was 561% for men and 587% for women . 
in the usa , 5 - year relative survival for all races combined was 601% in both sexes , with a range from 536% for women in new york city to 679% for men in hawaii ( table 2 and gure 2 )  . 
again , most of the estimates were within a narrow range , 5964% . 5 - year survival for colon cancer among blacks in the usa was lower than among whites . 
in 34 paired observations of this di erence in survival ( men and women in 17 popu lations ) , only three exceptions were noted , in men and women in iowa and men in nebraska . 
the estimates for blacks in those three areas were based on fewer than 50 patients , have wide con dence intervals and were not age - standardised ( table 3 and web gure 4 )  . 
the pooled estimate of age - adjusted 5 - year relative survival for the usa was 61% for white men and women , and 5152% for black men and women . 
within a given population , the absolute di erence between blacks and whites ranged from 26% in men and 73% in women in los angeles , ca to 143172% in colorado . 
the geographical range in blackwhite di erences in survival is a ected by small populations to some extent , but even in areas where blacks comprise 25% or more of the population ( atlanta , ga , detroit , mi , new york city , ny , louisiana ) , 5 - year survival from colon cancer in blacks was 612% lower than for whites in the same population ( table 3 )  . 
the pooled estimate of 5 - year survival in areas covered by npcr was 598% for men and 596% for women , and 619% for men and 621% for women in seer areas . age - standardised survival in whites ranged from 549% to 679% ( table 3 and web gure 4 )  . 
 survival in blacks was generally lower than the mean value for all included us populations and often more than three standard deviations below the mean , after controlling for precision of the survival estimates . 
the main exception was for white women in new york state , including new york city , ny , where survival estimates were precise , but more than three standard deviations below the lower control limits around the pooled us estimate ( web gure 3 )  . in japan , the pooled survival estimate was 630% in men and 571% in women , although survival was about 10% lower in osaka prefecture than in fukui or yamagata ( table 2 and gure 3 )  . in europe , 5 - year relative survival for colon cancer in men ranged from 285% in poland to 5457% in spain , finland , austria , and france . 
in women , the lowest estimate was also for poland ( 309% ) , while survival was in the range 5560% in nine countries ( table 2 and gure 3 )  . 
the estimates for northern ireland were 473% in men and 490% in women , slightly higher than the pooled estimate for the uk , 435% in men and 444% in women ( table 2 )  . the national estimate of 5 - year survival for colon cancer in australia was 578% in men and 577% in women . 
 survival ranged from 5062% in the eight states and territories : it was highest in new south wales , the australian capital territory , and queensland , and lowest in tasmania , northern territory , and western australia ( 96% of the population ; table 1 )  . of 233 176 rectal - cancer records submitted for analysis , 15 731 records ( 7% ) were excluded for a previous cancer , leaving 217 445 rst , primary , invasive rectal cancers eligible for analysis ( available online34 )  . 
a further 3213 ( 1% ) were excluded as dco regis trations , 517 ( < 1% ) as autopsydetected tumours and 574 ( < 1% ) as major errors , leaving 213 141 patients for inclusion in the analyses ( 98% of those eligible )  . 
almost 8% died within the rst month after diagnosis . 5 - year relative survival from rectal cancer , agestandardised to the icss weights , ranged from about 60% to around 20% in both sexes , with japan , canada , the usa , france , the netherlands , sweden , and australia at the upper end of the range , and algeria , estonia , poland , and slovakia at the lower end ( table 2 and gure 3 )  . the 5 - year survival estimates of 259% ( 95% ci 114437 ) for men and 182% ( 66346 ) for women in stif ( algeria ) were each based on 30 patients , and were not age - standardised because data were too sparse in some age groups . 5 - year relative survival in goinia , brazil , was 493% in men and 384% in women . 
5 - year survival in cuba was 592% in men and 628% in women , based on analysis of about 700 patients 746 vol 9 august 2008 cuba france austria canada malta australia japan spain germany netherlands iceland sweden finland norway italy northern ireland denmark ireland scotland portugal england slovakia slovenia estonia wales czech republic brazil poland algeria france cuba australia canada sweden japan norway netherlands finland malta ireland germany spain italy iceland scotland denmark england austria portugal northern ireland wales czech republic brazil slovenia slovakia estonia poland algeria colon ( women ) colon ( men ) rectum ( women ) rectum ( men ) 402 493 399 japan cuba australia france austria canada finland spain netherlands sweden italy germany norway ireland portugal iceland northern ireland scotland denmark england slovakia wales estonia malta czech republic slovenia brazil poland algeria cuba japan netherlands australia canada sweden france iceland norway spain finland brazil northern ireland germany italy austria denmark portugal scotland ireland england wales malta slovenia estonia czech republic poland slovakia algeria 5 - year relative survival ( % ) 5 - year relative survival ( % ) africa america , central and south america , north asia europe oceania data covering less than 100% of country vol 9 august 2008 394 497 385 articles figure 3 : 5 - year relative survival ( % ) , agestandardised to the icss weights * with 95% cis for adults ( aged 1599 years ) diagnosed with cancer of the colon or rectum during 199094 and followed up to dec 31 , 1999 : country vertical bar on the right of each graphic shows the contribution ( % ) of each continent to the total number of cases analysed ( contributions under 1% are not labelled )  . 
 * age - standardised to icss weights , except for stif , algeria ( all cancers ) , austria ( rectum [ women ] ) , iceland ( rectum [ men and women ] ) , ireland ( rectum [ women ] ) , malta ( colon [ men ] and rectum [ men and women ] ) , which were unstandardised values ( see text )  . 
 articles in each sex , although 782 ( 36% ) patients had been excluded as dco ( available online34 )  . in canada , the pooled estimate of 5 - year survival was 587% for women and 531% for men , slightly lower in the global range than for cancers of the breast , colon , or prostate in canada . 
in the usa , 5 - year relative survival for all races combined was 569% in men and 598% in women , with a range from 4667% in men and 5266% in women ( table 2 and gure 2 )  . 
by contrast with colon cancer , survival from rectal cancer was slightly higher in women than in men . 5 - year survival for rectal cancer in the usa was generally lower for blacks than for whites , in both sexes ( web gure 4 )  . 
 the overall estimate of 5 - year survival in men was 474% for blacks and 573% for whites ; for women , the estimates were 494% for blacks and 604% for whites ( table 3 )  . 
 when survival for blacks was above 60% , or higher than for whites in the same population ( colorado , connecticut , nebraska , rhode island ) , the estimates for blacks were based on around 50 or fewer patients , with wide cis , and were usually not age - standardised ( table 3 and web gure 4 )  . 
 even where blacks comprised 25% or more of the population ( atlanta , ga , detroit , mi , new york city , ny , louisiana ) , 5 - year survival was 616% lower than for whites in the same area . 
the pooled estimate of 5 - year survival in areas covered by npcr was 563% for men and 588% for women , some 23% lower than for seer areas ( 585% men , 618% women ; table 3 and gure 2 )  . 5 - year survival ranged from 462% to 679% in whites ; in blacks , the range of age - standardised survival was from 428% to 635% ( table 3 and web gure 4 )  . 
survival for whites was also generally within the control limits , with the exception of new york city , ny , where survival was below the control limits ( web gure 3 )  . in japan , the pooled survival estimate for colon cancer was 582% for men and 576% for women , although survival was lower in osaka ( 5455% ) than in fukui or yamagata ( 6064% ; table 2 and gure 3 )  . in europe , the geographical pattern for age - standardised 5 - year survival was similar to that for colon cancer . 
for men , the range was from 2830% in poland , west bohemia ( czech republic ) , and slovakia to 5355% in france , sweden , and the netherlands ; whereas for women , the range was from 3032% in poland , estonia , and slovakia up to 639% in france , where three of the four contributing registries ranked the highest in europe ( table 2 and gure 3 )  . 
the estimate for women is not age - standardised , but it is based on over 200 patients ( table 1 ) , and similarity between the raw and standardised estimates for cancers of the colon and colon and rectum combined ( less than 1% , data not shown ) suggests that an age - standardised estimate for rectal cancer would not have been very di erent . 
in northern ireland , the estimates were 482% in men and 438% in women ( pooled uk estimates were 406% in men and 453% in women ; table 2 )  . the national estimate of age - standardised 5 - year survival for rectal cancer in australia was 548% in men and 592% in women . 
survival ranged from 4557% in men and from 5561% in women . of 663 621 men with prostate cancer , 35 934 ( 5% ) were ex cluded for a previous cancer , leaving 627 687 eligible rst , primary , invasive cancers of the prostate ( available online34 )  . 
 after 11 163 ( 2% ) exclusions for dco , 1640 ( < 1% ) for autopsy - detection and 801 for major error , 614 083 men were included in the analyses ( 98% of those eligible )  . 
less than 1% of men were censored from the analysis within 5 years of diagnosis , but 32% died within 1 month of diagnosis . ( < 1% ) 5 - year relative survival , age - standardised to the icss weights , ranged from 80% or higher in the usa ( 92% ) , canada and austria to less than 40% in denmark , poland , and algeria ( table 2 and gure 1 )  . the 5 - year survival estimate of 214% ( 95% ci 87389 ) in stif ( algeria ) was based on 36 patients , and was not age - standardised . in brazil , 5 - year survival was 344% in campinas and 557% in goinia . 
notably , 20 ( 134% ) men in campinas and 71 ( 218% ) men in goinia died within 1 month of diagnosis , which are the highest proportions of any of the participating registries ( available online34 )  . 
this estimate was based on 4300 patients , but 54% of the original data set of 9500 patients had been excluded as dco ( table 1 and data available online34 )  . the pooled estimate of 5 - year survival for prostate cancer in canada was 851% , ranging from 775% in saskatchewan to 893% in british columbia ( table 2 and gure 1 )  . 
in the usa , 5 - year relative survival from prostate cancer was 919% for all races combined , with a range from 816% in new york city , ny up to 950% in seattle , wa ( table 2 and gure 2 ) , but most of the estimates were within a fairly narrow range , from 886% ( louisiana ) to 940% ( atlanta , ga )  . 
the relative survival estimate for the state of michigan was 100% , although in the city of detroit , mi , with 42% of the state population ( webtable ) , survival from prostate cancer in the same period was 938% . age - standardised 5 - year relative survival for prostate cancer in blacks was lower than for whites in all 748 vol 9 august 2008 articles populations for which this could be separately assessed with race - speci c life tables ( web gure 2 )  . 
the di erence in survival between blacks and whites ranged from 50% ( florida ) to 1416% ( nebraska , rhode island ) , and although the largest di erences arise where the black populations are smallest , each survival estimate was based on at least 70 patients ( webtable )  . 
the pooled estimate of 5 - year survival was 895% in areas covered by npcr , and 931% in seer areas ( table 3 )  . survival in blacks was usually lower than the pooled us estimate , and often more than three standard deviations below it , after controlling for precision ( web gure 3 )  . 
 5 - year survival for whites was above the upper 998% control limit in three seer populations ( atlanta , ga , seattle , wa , and detroit , mi )  . 
in new york state , including new york city , ny , survival estimates are precise , but 69% below the pooled us estimate of 923% and well below the lower control limit ( web gure 3 )  . the 5 - year relative survival estimates for michigan state ( 100% in both blacks and whites ) were too high , and they are not shown in web gure 3 , although the data were included in the pooled estimate . 
information about the death had not been linked to the tumour record for some of the apparent 5 - year survivors from prostate cancer in michigan state , leading to an in ated estimate . 
this error did not a ect the survival estimates for prostate cancer in detroit , mi or those for other cancers in michigan state . the pooled estimate of 5 - year survival in japan was 504% , much lower on the global scale than for cancers of the breast , colon , or rectum in japan . 
survival estimates were similar in all three prefectures ( table 2 and gure 1 )  . the range of 5 - year survival in europe was especially wide for prostate cancer , from less than 40% in poland and denmark to more than 80% in austria ( table 2 and gure 1 )  . 
data were not available for nine registries : switzerland ( ve registries ) , isre and cte dor ( france ) , granada ( spain ) , and northern netherlands . 
in northern ireland , the estimate was 540% , slightly higher than the pooled estimate of 511% for the uk ( table 2 )  . the national estimate of age - standardised 5 - year survival for prostate cancer in australia was 774% . 
 survival was closely similar in the six largest states , in the range 7680% , but notably lower in the two smallest regions : 637% ( based on 78 patients , estimate not age - standardised ) and 702% in tasmania ( 1321 patients )  . in northern territory discussion to our knowledge , the concord study is the rst attempt to provide directly comparable data on cancer survival from many countries around the world by use of central qualitycontrol procedures , standard analytic methods , and a single , centralised analysis of individual tumour records from population - based cancer registries . 
cancer - mortality statistics have often been used for international comparisons of progress against cancer , 6872 but they are also a ected by wellknown problems of comparability , both between countries and between successive revisions of the icd.7275 the ndings presented here should help joint consideration of trends in incidence , survival , and mortality as indicators of cancer control . 
none of these indicators is perfect , but none is adequate on its own.7678 around 2800 life tables were created to enable the estimation of relative survival by age , sex , country , and race.46 the life tables are available on the concord website.34 5 - year relative survival for breast , colorectal , and prostate cancers was generally higher in north america , australia , japan , and northern , western , and southern europe , and lower in algeria , brazil , and eastern europe . exclusions for a previous cancer ( 59% ) were not unexpected . 
population - based cancer survival analyses are usually restricted to patients with a rst , primary invasive cancer , therefore , to the extent that patients with a previous cancer have been completely excluded in this study , this improves the comparability of the ndings with other studies . 
the data from newer registries are more likely to include unrecognised second and subsequent cancers , because any previous cancer ( s ) in a given patient might have been diagnosed before the registry began operation . the main indices of data quality for cancer survival are the proportions of registered patients known to the registry by dco , or lost to follow - up , and histologically veri ed . 
the overall proportion of patients who died within 1 month of diagnosis was low for breast cancer ( 23% ) and prostate cancer ( 32% ) , but higher for colon ( 109% ) and rectal cancers ( 78% )  . 
fewer than 1% of patients were censored from the analysis within 5 years of diagnosis . three registries were excluded after quality control , because of high losses to follow - up or ine cient regional or national linkage of information on the deaths of patients with cancer . 
the data for three other registries , cuba , campinas ( brazil ) and , for prostate cancer , michigan state vol 9 august 2008 articles ( usa ) , are less reliable than those from other registries , although for di erent reasons , discussed below . 
as with the rst global compilation of cancer incidence data , in the 1960s , retention of the two registries from central and south america was partly prompted by the paucity of information on cancer survival from that region : in this situation , even incomplete data have value.64 overall , the exclusion of dco registrations accounted for only 1% ( 9215 ) of the eligible records for breast cancer , 3% ( 13 102 ) for colon cancer , 1% ( 3213 ) for rectal cancer , and 2% ( 11 163 ) for prostate cancer ( available online34 )  . 
 sweden does not use dcos because the registration of patients with cancer at the time of diagnosis is close to 100% ; by contrast , hospitals in cuba are not allowed to retain the clinical records of deceased persons for more than 5 years.80 the di erent proportions of dco records are unlikely to explain the di erences in survival between europe and north america , however . 
the survival of patients whose tumour is registered as a dco is generally lower than the mean for all registered cancer patients , 82 so if they could have been included , the transatlantic di erences in survival would have been slightly greater . 
furthermore , most dco records in the european data are for patients aged 75 years or over , 43 where the survival di erences are in any case more marked.9 by contrast , if a high proportion of dco records is taken to suggest under - registration of long - term survivors , this might produce lower survival esti mates . 
 adjustment for both dcos and incompleteness of registration in thames ( uk ) and finland had surprisingly little e ect on survival , however , even when 1020% of registrations were dcos , because the two corrections tended to o - set one another.83 under - reporting of incident tumours by up to 5% has been shown not to a ect international comparisons of survival greatly.84 a plateau was imposed on the relative survival curve at some point during the rst 5 years after diagnosis in about 7% of the 6500 age - speci c survival estimates by registry , cancer , sex , and race ( data not shown )  . 
the e ect on the age - standardised survival estimates at national level was almost always less than 1% . diagnostic variability between pathologists might contribute to international di erences in cancer survival . 
severe cytological or architectural changes con ned to the mucosa ( in situ or intramucosal carcinoma ) have no metastatic potential , and are often labelled high - grade dysplastic adenoma . 
japanese pathologists rely more on cytological features , however , and do not consider evidence of invasion into the submucosal layer as a mandatory requirement for the diagnosis of colorectal carcinoma.85 pathological practice on this issue might vary substantially between western pathologists . 
islands of dysplastic tissue might also be displaced or herniated beyond the muscularis mucosae without implying invasive potential ( pseudo - invasion ) , and di erential diagnosis can be very di cult.86 , 87 assessment of the extent to which international survival di erences might be attributable to di erences in the pathological de nition of disease would need blinded review of pathological diagnoses of a sample of patients by an international panel of expert pathologists . 
survival in stif was similar to or even lower than survival in blacks diag nosed during 199397 in harare , the zimbabwean capital , where the very low survival was attributed to inade quate access to facilities for early diagnosis , clinical investigation , and treatment.89 survival in the two brazilian registries was generally low , although rectal - cancer survival in goinia was close to the european mean . 
data quality issues prevented the inclusion of data from three of the 20 population - based registries in state capitals : these registries should be used to provide a broader picture of cancer survival in brazil . 
 relative survival reported here for patients with cancer diagnosed in cuba during 199094 was about 20% higher than estimates for those diagnosed during 198889 , just a few years earlier.80 cancer survival for children diagnosed in cuba during 198889 was lower than in more developed countries.90 the high proportion of dcos in the 198889 data was considered less likely to be biased with respect to survival than in other registries , because of the way data were collected , 80 but the survival estimates for cuba reported here are still likely to be considerably in ated , and should be interpreted accordingly . national estimates of survival for patients with cancer diagnosed in japan during 199396 were slightly higher than the estimates for 199094 reported here.79 they were based on data from seven prefectures , including the three reported here ( yamagata , fukui , and osaka )  . 
as in the concord data , survival in osaka was generally lower than the mean survival for japan . variation in survival between the provinces of canada and the states and territories of australia was generally small , and overall survival was high : this suggests health care of a high standard in most areas . 
variation between the countries of europe was much wider . 750 vol 9 august 2008 articles the substantial di erences in survival between australia and the uk have been noted before.91 they are unlikely to be because of di erences in data quality . 
more e ective treatment in australia is a plausible explanation.92 comparisons of cancer survival between europe and the usa since 2000 have identi ed wide di erences , with survival usually higher in the usa.9 closer assessment of these di erences with more detailed data , not routinely collected by all registries , has enabled the explanatory e ect of clinical variables such as stage at diagnosis , investigative approach , anatomical site , and morphology to be quanti ed for colorectal cancer12 , 93 and breast cancer , 10 and for a range of cancers in children.11 in those studies , the usa has always been represented by data from the seer program registries , representing some 10% of the us population at that time , because no other data have been available . 
the availability of data from a large number of state - wide population - based cancer registries that began oper ation around 1990 , and meet data quality standards comparable with those of the seer registries , now enables a larger proportion of the us population to be included in national and international comparisons of cancer survival . 
the concord study provided the rst opportunity for the cancer registries of 11 us states in the npcr to follow up all their patients for vital status and to undertake analyses of cancer survival , and 42% of the us population is included in these analyses . the survival di erences between us and european patients with cancer , especially in the oldest patients , seem unlikely to be attributable to artefacts of cancer registration . 
 the concord study has nonetheless identi ed two methodological issues that probably do explain some of the well - known di erences in survival between europe and the usa , from which only seer data have been available until now . first , relative survival was about 24% higher in seer - 9 areas than in participating npcr areas of the usa . 
 consequently , cancer survival in the 42% of the us population covered by the concord study was 13% lower than survival in the seer areas alone ( 10% of the us population )  . 
direct estimation of cancer survival for other areas of the usa would be desirable . second , census - derived us national life tables give higher estimates of all - cause mortality than are noted in the seer areas , especially with the gradual decline of mortality in the decade after a census.46 use of censusderived national life tables to estimate relative survival ( the seer approach ) therefore produces estimates that are almost always higher than those obtained with statespeci c life tables for each calendar year in the decade ( concord approach ) , which we believe to be more appropriate because it provides tighter control for changes over time in background mortality . 
with the concord approach , age - standardised 5 - year survival in the 22 participating areas of the usa was up to 3% lower than with the seer approach for breast cancer in women , up to 4% lower for colorectal cancer , and up to 5% lower for prostate cancer ( available online34 )  . the di erences in cancer survival between blacks and whites of both sexes in the usa are large , and remarkably consistent in 16 states and six metropolitan areasmore populations than it has been possible to study in the past.94 the di erences were adjusted for age and for di erences in background mortality between blacks and whites within each state or metropolitan area . 
it would be interesting to know if the di erences were attributable to artefact , or di erences between blacks and whites in tumour biology , in stage at diagnosis , in access to health care , or in compliance with treatment . 
the blackwhite di erences in relative survival that we report would have been even larger if we had used race - speci c national life tables instead of racestate life tables , because back ground mortality is higher ( and expected survival lower ) in blacks than in whites in all the populations studied.23 , 95 survival from cancers of the breast , colorectum , and prostate varied with the type of health insurance in a population - based study : 96 survival was highest in patients who had private insurance , intermediate with federal insurance , and lowest with no insurance . 
late stage , 98 less treatment , and higher mortality seem to be associated with black race , low socioeconomic status , and poor survival in the usa.99101 extensive reviews have led to the conclusion that racial disparities in cancer treatment , which are not explained by clinical factors , lead to worse outcomes in blacks.102 , 103 analysis of seer data suggested that some racial di erences in treatment and cause - speci c survival persist after adjustment for poverty.104 by contrast , the racial di erence in survival from colorectal cancer was almost absent in patients managed under the equal - access , integrated health - care veterans a airs system.105 finally , overviews of race , socioeconomic status , and cancer outcomes strongly suggest that equal treatment yields equal outcome , irrespective of race.53 , 106 the data presented here extend the evidence that cancer survival in the usa is lower in blacks than in whites . simple ranking of countries by overall survival can be misleading . 
survival is very similar in many european countries , at the centre of the global range , and a small shift in the survival estimate in either direction can entail a large change in the rank . 
thus , even the national survival estimates for iceland and malta have wide con dence intervals and unstable rankings because they are based on populations of around 250 000 ( gures 1 and 3 )  . 
the detailed data by country and region are tabulated by continent , country , and region , rather than ranked : some vol 9 august 2008 articles estimates , based on sparse data , could not be agestandardised ( table 2 )  . the numbers of patients included in the analysis varied widely , as did the proportion of the national population covered by the data . 
population coverage of participating registries in italy was about 15% , but they were concentrated in the wealthier north of the country.22 , 30 the same point also applies to the usa , however , because the data presented here con rm suggestions107 that cancer survival in the seer program areas ( 10% population coverage during the 1990s ) was higher than in other parts of the country . 
similarly , survival for 199094 in the four french dpartements reported here ( 6% national coverage ) was high on the european scale for most cancers , 27 and a much larger study for the same period in 14 dpartements ( 20% coverage ) showed similar patterns of survival.108 , 109 for countries with more than one contributing registry but less than 100% population coverage , we have presented estimates of survival derived from the pooled data , not weighted means of the regional estimates of survival . 
the question of whether pooled survival estimates derived from regional registries with less than 100% national coverage can properly be considered representative of cancer survival in the whole country has been discussed else where.22 if population - based estimates of cancer survival are deemed reliable , however , they do suggest a poten tially achievable level of survival , irrespective of whether the estimate is for a whole country or only one region in that country . 
the proportionate contributions from each continent to the concord study are very di erent from the worldwide distribution of cancers of the breast , colon , rectum , and prostate . 
the national data for australia alone represented 63% of the population of oceania in 1995 , 111 and the survival estimates for north america included 44% of the combined populations of usa and canada around 1992 , but for africa , asia , and south america , the population coverage of these data was much lower . 
the survival data for europe were based on 25% of the continental population of 512 million in 1992 , 112 but the eurocare study ( ongoing since 1989 ) is the largest and most widely cited international study of cancer survival , and all 57 cancer registries in that study , and six others , contributed to concord . 
to provide an international summary measure of cancer survival for visual comparison , we therefore used the overall estimates for 23 countries in eurocare - 3 , but age - standardised to the icss weights used in concord , instead of the weights used in eurocare - 3.113 we have presented pooled estimates of survival for europe and north america ( table 3 ) , but not for other continents . the size of the population covered by the data a ects the statistical precision of the survival estimates . 
this is shown by 95% cis , but ranked graphics do not provide visual appreciation of the extent to which the survival estimate for a given country or region falls outside the distribution of survival estimates that might be expected , under the hypothesis that survival should be the same in all areas . 
we used funnel plots62 to provide that visual e ect for geographical and racial variation in survival in the usa , with the target value as the pooled estimate for the usa , age - standardised to the icss weights.60 these plots display striking geographical and racial variation in survival . clinical practice has continued to evolve in the 15 years or so since the patients included in this study were diagnosed . 
changes in diagnosis , screening , and treatment have undoubtedly improved the prognosis for cancer patients , at least in wealthier countries . survival has increased substantially for cancers of the breast ( women ) , colon , rectum , and prostate in the 17 areas of the usa covered by the seer program during 19962003 , 114 and in canada ( 199698 ) 115 and australia ( 19942004 ) .116 , 117 smaller increases have been reported in 11 of the 47 japanese prefectures.118 these estimates of relative survival , published for national purposes , cannot be compared with the data reported here , however , because of di erences in the quality control of incidence data or completeness of follow - up , and in methods of analysis . 
 some estimates were not age - standardised for international comparison , whereas others were standard ised to countryspeci c age weights , rather than the icss age weights that we used . the only recent international study of cancer survival is eurocare - 4 , which included patients diagnosed in 23 countries during all or part of 19952002 and followed up to 2003.29 , 30 survival increased substantially in eastern european countries , where it was much lower than in other parts of europe during 199094 . 
the rise in breast cancer survival in several countries was associated with a fall in mortality , possibly because of improved care and screening programmes ; the rise in prostate - cancer survival ( and incidence ) might be a result of more widespread psa testing . 
in western europe , survival in the uk and denmark was still low for several cancers in the late 1990s . concord is , by chance , reasonably well - timed to provide a baseline for international comparisons of cancer survival to assess the e ect of several major public health initiatives for the control of breast , 752 vol 9 august 2008 articles screening for breast colorectal , and prostate cancers . 
at that time , intense early diagnostic activity with prostate - speci c antigen ( psa ) had recently become widespread in the usa , but was little used elsewhere . 
in denmark , for example , the 50year increase in prostate cancer incidence is considered real , 119 but the danish society for urology assessed the evidence in 1990120 and decided not to advocate psa testing in asymptomatic men , because the therapeutic bene t was very small ; 121 only sympto matic patients were o ered treatment . 
mass screening for colorectal cancer with faecal occult blood ( fob ) testing or endoscopy had not begun during 199094 in any contributing country as far as we are aware . 
opportunistic screening with the fob test began in japan in 1992 ; by 2004 , about 20% of people aged 40 years or over had been tested within the previous year.122 opportunistic endoscopy had already become widespread in some parts of the us population by 1990 . the concord study was planned in three phases . 
the study reported here ( phase i , low resolution ) was designed to quantify international di erences in population - based relative survival by age , sex , country , or region for patients diagnosed during 199094 with a cancer of the breast , colon , rectum , or prostate . 
phase ii ( high resolution ) was designed to help interpret those international di erences in survival , by use of a subset of registries that could reabstract detailed clinical data , including stage at diagnosis and treatment , from the original medical records for large random samples of patients diagnosed with one of the same cancers during 199698 . 
phase iii was designed as a blinded , expert review of the pathological diagnosis for a subset of patients from the phase ii study , to assess the extent to which international survival di erences might be attributable to di erences in the pathological de nition of disease in participating countries . the range of survival estimates for each cancer is very wide . 
population - based cancer registries are increasingly important in the comparative assessment of cancer outcomes , 123 and even allowing for di erences in data quality or statistical robustness , there is little doubt that the chances of survival after a cancer diagnosis vary hugely on a global scale . the comparability of cancer survival estimates between countries is criticised far more often than the comparability of cancer incidence data from the same registries . 
cancer survival is a measure of the overall e ectiveness of cancer treatment services , whereas cancer incidence is a measure of the long - term e ect of prevention policies , which are less visible on a day - to - day basis and can , incorrectly , be seen as less important . cancer survival is a valuable indicator for international comparison of progress in cancer control , 76 , 124 , 125 despite the fact that part of the variation in cancer survival identi ed in this study could be attributable to di erences in the intensity of diagnostic activity ( casending ) in participating populations . 
if overdiagnosiswhich depends on diagnostic intensityis more marked in one country than another , then it will certainly be harder for researchers to compare incidence , mortality , and survival in those countries . 
in each country , the health - care system will have to be funded , sta ed , and equipped to cope with the diagnostic and therapeutic burden of all patients with cancer , however they are diagnosed . 
the health - care system must make provision accordingly , and monitor the outcome of that provision ; cancer survival is one such overall indicator . furthermore , a patient with cancer is still a patient with cancer , whether or not they represent over - diagnosis . 
as it is , a cancer diagnosis represents the best that medicine has to o er in a given country at a given time , and that best is variable . 
no matter how a patient with cancer is diagnosed , they have to cope with the consequences , both psychological and physical , and will usually want to be treated . 
in this sense , cancer incidence and survival estimates describe as accurately as possible the occurrence and the outcome , respectively , of cancer as it is diagnosed and treated at a given time in a given population . most of the wide global range in survival is probably attributable to di erences in access to diagnostic and treatment services.3 , 82 , 89 , 91 , 126 international variation survival in europe has been associated with national levels of economic development , as measured by total national expenditure on health.29 survival is positively associated with gross domestic product and the amount of investment in health technology such as ct scanners.124 part of the international variation is thus probably attributable to under - investment in health resources.127 , 128 the variation in survival might be considered intuitively obvious , given wide global variation in expenditure on health care , whether that is expressed in absolute terms or as a proportion of national resources . 
a parallel could be drawn with di erences in survival between rich and poor patients with cancer in a given country , which have frequently been reported.129 , 130 in survival until now , however , direct international comparisons of cancer survival between high - income and low - income countries have not generally been available . 
rc , sf , rda , msantaquilani , mq , gg , msant , fb , jml , th , sk , and av were involved in data preparation and quality control . 
all authors revised the report . con icts of interest the authors declared no con icts of interest . acknowledgments we are grateful to the many cancer registry sta around the world whose meticulous and sustained e orts at data collection , linkage , and quality control have enabled the survival of patients to be analysed and compared in this study . 
we thank dee bhakta and adrian cousins ( london school of hygiene and tropical medicine , london , uk ) for help in undertaking the pilot study and for producing web gure 1 , respectively . 
the ndings and conclusions in this report are those of the authors and do not necessarily represent the views of the us cdc . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology euthanasia ( destroyed brain activity after application ) and palliative sedation ( continued brain activity after application )  . 
however , palliative is only acceptable for the combination of both intolerable and refractory ( untreatable ) symptoms.2 although it is understandable that patients struggle with existential questions in the face of death , it is problematic to consider this struggle as a refractory symptom for palliative sedation , as the authors correctly note . 
 such an application of palliative sedation occurs only in exceptional circumstances ( it is mostly applied for severe delirium and dyspnoea ) and , therefore , should not be the example by which the entire practice is considered controversial.3 we have proposed that palliative sedation is morally acceptable only when excruciating and untreatable symptoms severely threaten a patients ability to be the further agent of his or her life.4 this precondition acknowledges that it should be the progressive disease , not the palliative sedation , which inhibits the patients ability to shape their own life . 
therefore , total sedation will be at one end of the spectrum of palliative sedation , and used in a restricted group of patients , with intermittent and super cial sedation at the other end . 
in this perspective , palliative sedation is not controversial but a well de ned medical last resort for intractable ( and irresolvable ) multidimensional needs and problems in human beings who are su ering . 
clinical guidelines and an obligatory expert consultation in palliative care will educate and strengthen a reliable practice.5 jeroen hasselaar * , stans verhagen , rob reuzel , evert van leeuwen , kris vissers department of anesthesia , pain and palliative medicine ( jh , sv , kv ) , department of epidemiology , bio - statistics , and health technology assessment ( rr ) , and section ethics , philosophy , and history of medicine , department of iq health care ( evl ) radboud university medical center , nijmegen , the netherlands j.hasselaar@anes.umcn.nl the authors declared no con icts of interest . 1 materstvedt lj , bosshard g . 
in this article , the number 169 in the mild dyskaryosis box on the right - hand side of gure 3 should have been given as 196 . 748 vol 10 august 2009 re ection and reaction the authors declared no con icts of interest . 
the authors are supported by the national council for scienti c and technological development ( cnpq ) , the south american o ce for anticancer drug development ( soad ) , and the childrens cancer institute ( ici - rs )  . jones kl , buzdar au . 
curr stem cell res ther 2009 4 : 30613 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata saito m , aogi k , sekine i , et al . 
palonosetron plus dexamethasone versus granisetron plus dexamethasone for prevention of nausea and vomiting during chemotherapy : a double - blind , double - dummy , randomised , comparative phase iii trial . 
lancet oncol 2009 ; 10 : 11524the role of the funding source for this article should read under agreement with the study sponsor , the medical adviser , medical statistical adviser , and coordinating investigators of the study worked on the design and conduct of this study , and in the analysis and interpretation of the data collaboratively with the principal investigators at the trial sites . 
the trial members should read mamoru tsukuda ( medical adviser ; yokahama city university school of medicine , yokahama , japan ) , chikuma hamada ( medical statistical adviser ; tokyo university of science , tokyo , japan ) , yutaka ariyoshi ( coordinating investigator ; aichi cancer center , aichi hospital , okazaki , japan ) , tomohide tamura ( coordinating investigator , national cancer center , tokyo , japan ) , toshiaki saeki ( coordinating investigator , saitama medical university , hidaka , japan )  . 
 the con icts of interest statement should read : mamoru tsukuda , chikuma hamada , yutaka ariyoshi , tomohide tamura , and toshiaki saeki have received consulting fees or honoraria from taiho pharmaceutical . 
lancet oncol 2010 ; 11 : 15564in this article , the third sentence of the methods section in the summary should read 217 patients with previously treated stage iii ( unresectable ) or stage iv melanoma were randomly assigned a xed dose of ipilimumab of either 10 mg / kg ( n = 72 ) , 3 mg / kg ( n = 72 ) , or 03 mg / kg ( n = 73 ) every 3 weeks for four cycles ( induction ) followed by maintenance therapy every 3 months . 
we report the nal analyses of long - term survival data with additional follow - up in both trials . methods 311 men with metastatic disease were recruited to pr05 between 1994 and 1998 , and 508 men with non - metastatic disease were recruited to pr04 from 1994 to 1997 . 
all men were treated according to the recruiting sites standard practice at the time : for metastatic disease , all men were starting or responding to long - term hormone therapy ; for non - metastatic disease , most men had radiotherapy , hormone therapy , or both . 
men were randomly assigned to take four tablets per day of sodium clodronate ( 2080 mg ) or matching placebo for up to 3 years ( metastatic disease ) or 5 years ( non - metastatic )  . 
long - term overall survival was assessed on an intention - to - treat basis in all men at sites in england and wales using data from the national health service information centre , which held data for 278 of 311 men in the pr05 trial and 471 of 508 men in the pr04 trial . 
these studies are registered international standardised randomised controlled trials , numbers isrctn38477744 ( pr05 ) and isrctn61384873 ( pr04 )  . findings of the 278 men with metastatic disease , 258 ( 93% ) were reported to have died . 
evidence of a bene t for those with metastatic disease from use of sodium clodronate compared with placebo was seen in overall survival ( hazard ratio [ hr ] 077 , 95% ci 060098 ; p = 0032 )  . 
the medical research council ( mrc ) pr051 and pr042 randomised controlled trials assessed the role of adjuvant sodium clodronate in men with metastatic ( m1 ) and non - metastatic ( m0 ) prostate cancer , respectively . 
 both trials have previously reported results on their primary outcome measures.1 , 2 overall survival was a secondary outcome measure in both trials , but the overall survival data were immature when the primary analyses were published . 
the metastatic trial , pr05 , previously showed some evidence of improvement in overall survival with clodronate ( hazard ratio [ hr ] 080 , 95% ci 062103 ) ; whereas the non - metastatic trial , pr04 , did not show evidence of a bene t in overall survival ( hr 102 , 95% ci 080130 )  . 
the aim of this paper is to report nal analyses of long - term survival data with additional follow - up in both trials . methods patients the methods for these two trials have been fully described previously.1 , 2 in summary , 311 men with bony metastases from prostate cancer ( m1 ) and 508 men with prostate cancer with out metastases ( m0 ) gave written informed consent to join these two multi centre , double - blind , placebo - controlled randomised controlled trials , which opened to recruit ment in june , 1994 , and successfully completed accrual in july , 1998 , and december , 1997 , respectively . 
the trial was run under a clinical trial marketing product licence from the regulatory authority . 872 vol 10 september 2009 articles long - term hormone randomisation and masking randomisation was done centrally using minimisation across a number of strati cation factors to ensure balanced groups . 
in the pr05 trial in men with metastatic disease , the strati cation factors were treatment centre , time since therapy ( 6 weeks vs starting > 6 weeks ) , type of hormone therapy ( monotherapy vs maximal androgen blockade ) , and who performance status . 
in the non - metastatic trial , pr04 , the strati cation factors were : treatment centre , tumour stage ( t2 vs t3 vs t4 ) , primary therapy ( given vs not given ) , time from primary therapy to trial entry ( none vs 12 months vs > 12 months ) , and prostate - speci c antigen ( psa ) concentration at study entry ( < 50 ng / ml vs 50 ng / ml )  . 
men were randomly assigned to supplement the usual treatment for their prostate cancer with four tablets each day of oral sodium clodronate ( 2080 mg ) , or a matching placebo . 
men with metastatic disease were just starting or were already responding to standard treatment with hormone therapy ( androgen suppression ) , which was maintained through out the trial period . 
the primary outcome measure was the progression of symptom atic bone metastases or death from prostate cancer in the metastatic setting , or the development of symptomatic bone metastases or death from prostate cancer in the non - metastatic setting . 
all patients from england and wales who were successfully agged are included in the analyses : 278 ( 89% ) of 311 men with metastatic disease , and 471 ( 93% ) of 508 men with non - metastatic disease . 
exploratory interaction analyses were done using either tests for interaction or trend , as appropriate , to examine the consistency of the treatment e ect in di erent subgroups ; the degrees of freedom are speci ed in each instance . 
the subgroups used were the same as those used for previous analyses.1 , 2 ci are given at the 95% level ; p values are given to two signi cant gures . 
these studies are registered international standardised randomised controlled trials , numbers isrctn38477744 ( pr05 ) and isrctn61384873 ( pr04 )  . role of funding source the sponsor and main funder of the trial had no role in the design and conduct of the trial or in the analysis of the data . 
roche products ltd were involved in the design of the study , but not the analysis ; they were invited to submit comments on an early version of this manuscript . 
all patients on pr04 were agged before the main , previously reported analyses , but agging was not done in 190 patients in the pr05 trial who were already known to have died by that point . 
the estimated 5 - year survival was 80% with placebo and 78% with clodronate ; 10 - year survival rates were 51% with placebo and 48% with clodronate ( gure 2b )  . 
tests for interaction showed some evidence of heterogeneity in treatment e ect on survival in subgroups de ned by alkaline phos phatase ( heterogeneity = 435 , df 1 ; p = 0037 ) and serum creatinine ( heterogeneity = 516 , df 1 ; p = 0023 ; gure 3a ) , with larger treatment e ects with higher concentrations of alkaline phosphatase and serum creatinine . 
tests for inter action also showed some evidence of an increased treatment e ect in men who had bone metastases for a shorter time before randomisation ( hetero geneity = 369 , df 1 ; p = 0055 ) , and in men who had a shorter time from diagnosis to trial entry ( heterogeneity = 361 , df 1 ; p = 0058 ; gure 3a )  . 
 in the pr04 trial of men with non - metastatic disease , exploratory interaction analyses focused on the choice of primary treatment , although the numbers are small in each of these groups . 
this analysis showed no evidence of an interaction of clodronate with primary therapy given as radio therapy , hormone therapy , or both in terms of overall survival ( gure 3b ; heterogeneity = 113 , df 2 ; p = 057 )  . 
there was no evidence of heterogeneity of the treatment e ect of clodronate in patients receiving clodronate with long - term hormone therapy in the metastatic trial and the non - metastatic trial ( gure 3b ; heterogeneity = 084 , df 1 ; p = 036 )  . discussion overall survival remains an important long - term outcome measure in both metastatic and non - metastatic disease . 
here , we report an advantage in overall survival conferred by clodronate in men with metastases who joined the pr05 trial , but no evidence of a di erence in survival in men without metastases in the pr04 trial . 
the numbers of events are presented in parentheses , representing the deaths during these intervals . had nal responsibility for the decision to submit the manuscript for publication . results over the 5 - year period since the previous results , maturity in the metastatic trial , pr05 , increased from 235 ( 76% ) reported deaths in 311 men at the previously reported analyses to 258 ( 93% ) deaths in 278 men here , with a median follow - up of 115 years , compared with 49 years previously . 
for overall survival , there is evidence that clodronate confers a bene t compared with placebo , with an hr of 077 ( 95% ci 060098 ; p = 0032 )  . 
the estimated 5 - year survival was 21% with placebo and 30% with clodronate ; the estimated 10 - year survival was 9% with placebo and 17% with clodronate ( gure 2a )  . 
they have an established role in the management of myeloma and metastatic breast cancer , and the treatment of hypercalcaemia related to malignancy.6 , 7 prostate cancer is characterised by osteoblastic metastases , and it remains controversial as to whether osteoclast activation is a necessary precursor for the development of these sclerotic skeletal metastases , or occurs as a consequence of their presence.810 the results of our pair of trials support the latter hypothesis , as the bene t of clodronate seemed to be restricted to the progression of established metastases . 
 never theless , the more potent amino - bisphosphonates might also have direct e ects on tumour cells ; inducing apop tosis and inhibiting invasion through the inhibition of the mevalonate pathway.11 indeed , a recent study in local ised breast cancer12 suggests an improvement in disease - free survival in patients treated with zoledronic acid compared with placebo ( hr 064 , 95% ci 046091 )  . 
 when the trials started in the early 1990s , chemotherapy was not routinely used in the uk to any extent to treat prostate cancer , and the options for treatment after rst - line hormone therapy were very limited . 
 why have these two trials given apparently contradictory resultsis this due to biological factors related to the development and progression of bone metastases or just the play of chance ? certainly , both trials are modestly sized , with just over 800 patients recruited in total . 
the power calculations were based around the previously reported primary outcome measures rather than overall survival and di erences in survival might be attributable to chance , even though these analyses are based on 281 deaths in the non - metastatic setting and 258 deaths in the metastatic setting . 
 however , in the metastatic setting ( pr05 ) we have previously reported other bene ts in terms of symptomaticbone - progression - free survival with an increase in time to deterioration of performance status ( hr 071 , 95% ci 056092 ) and biologically measured favourable e ects on both alkaline phosphatase and psa nadir levels in favour of clodronate therapy.1 exploratory interaction analyses for the metastatic trial , reported here and previously , 1 suggest greater relative bene t with prompt initiation of clodronate for men with poorer prognostic features such as raised alkaline phosphatase and creatinine . 
 patients with raised alkaline phosphatase would be expected to have increased osteoblastic activity , and we speculate that this patient population with an increased disease burden might also have a greater degree of osteoclast activation and bone lysis , which might be modi ed with early bisphosphonate treatment . 
a raised creatinine level might lead to decreased bisphosphonate excretion , and therefore relatively greater drug exposure and more biological e ect . in the trial in men with non - metastatic disease ( pr04 ) , exploratory interaction analyses focused on primary therapy , because the choice of primary therapy would have been a re ection of both disease stage and standard local practice . 
for the group treated with a combination of radiotherapy and androgen deprivation , which would now be regarded as the standard of care for men with intermediate and high - risk localised disease , 35 the hr was 095 ( 95% ci 057157 )  . the principal action of bisphosphonates is to decrease osteoclast activity , and therefore bone resorption . 
 additional e ects might include a secondary reduction of tumour - producing growth factors , inhibition of the vol 10 september 2009 articles alternative additional treatments in most cases in both trials , and these were previously summarised for the metastatic trial.1 there were also very few data to suggest that variations in second - line or third - line hormone treatment would make a di erence to survival . 
there is no good reason to think there is an imbalance of these treatments across the trial groups . in prostate cancer , trials with much more potent bisphosphonates such as zoledronic acid should help clarify the situation for men with hormone - sensitive prostate cancer in due course ; a non - statistically signi cant trend for improved survival has already been reported using zoledronic acid in men with castrate - resistant disease.13 in men with hormone - sensitive disease , ongoing randomised controlled trials for men with high - risk locally advanced disease include the european association of urologys zeus trial ( isrctn66626762 ) across europe , which compares standard treatment with or without 4 mg infusions of zoledronic acid every 3 months for a total of 4 years . 
additionally , the trans - tasman radiation oncology groups radar trial ( nct00193856 ) in australia and new zealand , which is a four - arm trial in men having standard radiotherapy for prostate cancer , is comparing the e ects on survival of duration of androgen suppression ( given for either 5 or 18 months ) and use of zoledronic acid ( not given or given as 4 mg every 3 months for 18 months )  . 
 additionally , the lead investigators from pr04 and pr05 have been involved in the design and conduct of the ongoing mrc - led stampede trial ( isrctn78818554 ) .14 , 15 stampede is a trial for men with locally advanced or metastatic disease , and recruits similar populations to the pr04 and pr05 trials . 
in this six - arm trial , men starting long - term hormone therapy for the rst time are randomly assigned to supplement this treatment with 4 mg zoledronic acid given intravenously every 34 weeks for 2 years . 
the other research drugs in stampede are the taxane chemotherapy docetaxel , which is given for six cycles , and the cox2 inhibitor celecoxib , which is given for 1 year . 
patients in stampede are randomly assigned to receive hormone therapy alone ( control group ) , or hormone therapy plus docetaxel ; hormone therapy plus zoledronic acid ; hormone therapy plus celecoxib ; hormone therapy plus docetaxel plus zoledronic acid ; or hormone therapy plus zoledronic acid plus celecoxib . 
between 2000 and 3000 men will join the trial ; over 1000 patients have already been enrolled . in conclusion , pr05 is the rst trial , to our knowledge , to show an overall survival bene t conferred by an oral bisphosphonate when given in addition to standard hormone therapy to men with bone metastases who are starting or responding to hormone therapy for prostate cancer . 
however , there is no evidence that clodronate is of any bene t when given as an adjuvant to treatment in men with non - metastatic prostate cancer . contributors dpd and mdm co - led the drafting of the manuscript , participated in the design of the trials , participated in the implementation of trials , and read and approved the nal manuscript . 
mrs led the drafting of the manuscript , participated in the implementation of the trial , did the analyses , and read and approved the nal manuscript . con icts of interest mkbp , ks , and ms are all employed by the medical research council , a publicly funded body in the uk , who sponsored the trial . 
the other authors declared that they have no con icts of interest . acknowledgments this study was funded by the uk medical research council , and an education grant and free drugs from roche products ltd . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology chosen as one of the endpoints.2 patients recruited in this trial were offered radiofrequency ablation , because they were considered by the treating physician to be unsuitable for surgery and unfit for radiotherapy or chemotherapy as a result of either underlying chronic obstructive pulmonary disease or major associated comorbidities . 
because the patients had small , asymptomatic pulmonary tumours , no improvement in quality of life was noted after treatment with radiofrequency ablation , despite the high number of complete responses . 
nevertheless , we think that the absence of any significant worsening in short form ( sf ) - 12 ( physical and mental summary ) scores and functional assessment of cancer therapylung ( fact - l ; lung - cancer scale and trial outcome index ) scores provides evidence that the minimallyinvasive treatment approach used in these patients did preserve their quality of life . 
the number at risk for part b of gures 3 and 4 of this article should have been interventional group ( top ) and control group ( bottom )  . 
also , the second sentence in the discussion should have read , however , preoperative chemoradiotherapy in patients undergoing surgery signi cantly increased the proportion of those with complete resection ; and in those with complete resection , preoperative chemoradiotherapy increased the proportion of patients with mediastinal downstaging and histopathological response . bo etta p , hecht s , gray n , gupta p , straif k . 
during the immediate months preceding submission of the review sh was acting in the capacity of an expert witness for the plainti in a future court case against a smokeless tobacco company . 
sh declares his participation in this case in no way in uenced his writing or involvement in the review . bonnefoi h , potti a , delorenzi m , et al . 
in the webpanel of this article , the headings for docetaxel should have been resistant cell lines ( rst ) and sensitive cell lines ( second )  . 822 vol 9 september 2008 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology department of radiation oncology , all india institute of medical sciences , new delhi , india sharmadn@hotmail.com the authors declared no con icts of interest . powell jw , dexter e , scalzetti em , bogart ja . 
long term results of endobronchial brachytherapy : a curative treatment ? int j radiat oncol biol phys 2007 ; 67 : 42530 . brach b , buhler c , hayman mh , joyner lr jr , liprie sf . 
 chest 2005 ; 127 : 223742 . screening newborns for tp53 in the september issue of the lancet oncology , achatz and colleagues1 discuss the possibility of screening newborns in southeast brazil for a highly prevalent tp53 mutation ( 1 : 300 individuals ) that predisposes to many cancers . 
the authors present the justi cations and the problems associated with such a screening e ort , and conclude that on the basis of current scienti c and medical knowledge the r337h mutation does not meet all the criteria for mass newborn screening . 
 in my opinion , this type of screening will never meet the criteria for newborn screening , which is intended to detect conditions for which the population is at risk but there is no other way to assess risk in newborns . 
newborn screening is done for sporadic diseases such as congenital hypothyroidism and autosomal recessive disorders , in which carrier detection is di cult or impossible , but never applies for a disorder caused by the presence of a founder dominant mutation . 
a founder mutation in a newborn will be carried by one of the parents , so the detection of the child can be done by knowing who the adult carrier is . 
cascade screening is the most economically e ective , o ering the screening test to rst - degree relatives of carriers of the mutation , and several countries have chosen this approach.2 the problem with this type of screening is that it involves the cooperation of relatives who are not always willing , and so an alternative has been the creation of databases to store information on patients.3 in my view , population screening of informed and consenting adults is much better suited for the tp53 mutation . 
 this approach identi es families at risk and has been implemented in pilot studies for haemochromatosis.4 as emphasised by achatz and colleagues , 1 such population screeningin the context of appropriate genetic counsellingallows at - risk families the informed decision of whether or not to test the probands o spring . joel zlotogora department of community genetics , ministry of health , jerusalem , israel joelz@cc.huji.ac.il the author declared no con icts of interest . achatz miw , hainaut p , ashton - prolla p . 
 clin genet 2004 ; 66 : 48387 . had eld sg , horara s , starr bj , et al ; steering group for the department of health familial hypercholesterolaemia cascade testing audit project . 
lancet oncol 2009 ; 10 : 940in this news report , the nal sentence of the 90y radioembolisation paragraph should have read only one patient experienced radiation - induced pneumonitis ; three had gastrointestinal ulcers that did not require surgical treatment , and radioembolisation - induced liver disease was noted in 24 patients ( fatal for four )  . huober j , thrlimann b . 
lancet oncol 2009 ; 10 : 102829in this re ection and reaction , the a liation for both authors should read breast center , kantonsspital st gallen , 9007 st gallen , switzerland . 
the authors would also like to thank karen price for her useful comments on the article . 1142 vol 10 december 2009 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper to the lancet go to thelancet / to submit a paper to the lancet oncology go to ees.elsevier.com / thelancetoncology / recommendations in light of the new data presented by raaijmakers and colleagues.3 piet dirix * , sandra nuyts department of radiation oncology , university hospitals leuven , leuven , belgium , piet.dirix@uzleuven.be the authors declared no con icts of interest . raaijmakers cp , roesink jm , dijkema t , houweling ac , terhaard ch . 
first results of a phase iii multicenter randomized controlled trial of intensity modulated ( imrt ) versus conventional radiotherapy ( rt ) in head and neck cancer ( parsport : isrctn48243537 ; cruk / 03 / 005 )  . 
proc am soc clin oncol 2009 ; 27 : abstr lba6006 . call for papersoncology and haematology the lancet and the lancet oncology are announcing plans for issues of each journal to be devoted to speci c topics in oncology and also to haematology . 
the former will be timed to coincide with the european society of medical oncology ( esmo ) congress in milan , italy ( oct 812 , 2010 ) , and the latter with the american society of hematology ( ash ) annual meeting in orlando , fl , usa ( dec 47 , 2010 )  . 
we would like to invite submissions of high - quality original research about cancers of the breast , lung , prostate , and gastrointestinal tract , or on any topic in haematology or haematological oncology . 
accepted papers will be published in either the lancet or the lancet oncology via fast - track peer review to coincide with either the esmo or ash annual meetings , as appropriate . 
 submissions to coincide with the esmo annual meeting must be received by june 25 , 2010 , and those for the ash annual meeting by oct 1 , 2010 , via either the lancet or the lancet oncologys online submission systems . 
please state in your covering letter that the submission is in response to this call for papers . if your work is being presented at either meeting and falls under an embargo policy , please tell us the date and time of the presentation , and whether the study is to be presented orally or in a poster . 
if your paper is accepted , online publication can be scheduled to coincide with the presentation and comply with any press embargo . jane godsland , zo mullan , richard turner , david collingridge the lancet ( jg , zm , and rt ) and the lancet oncology ( dc ) , 32 jamestown road , london nw1 7by , uk errata relling mv , altman rb , goetz mp , evans we . 
clinical implementation of pharmacogenomics : overcoming genetic exceptionalislancet oncol 2010 ; 11 : 50709the acknowledgment in this comment ( published online first on april 21 , 2010 ) should have read we thank colleagues in nihs pharmacogenomics research network . 
in the second paragraph , the last sentence was misspelt and should have read despite evidence linking pharmacogenomic variation with drug exposure , toxic e ects , and e cacy , many clinicians , regulators , and payors hold pharmacogenetic evidence to excessively high standards . 
lancet oncol 2010 ; 11 : 42938in this article , the acknowledgments statement should also have included : the uk medical research council funded the original all97 / 99 trial and supported the childhood leukaemia working party . 
lancet oncol 2007 ; 8 : 31722in this article , the equation for acpgbi in panel 2 should read loge [ r / ( 1r ) ] = ( 4859 + total score )  . 
additionally , in table 3 , 158 was added in error next to the heading clinicopathological staging . 516 vol 11 june 2010 re ection and reaction the authors declared no con icts of interest . 
the authors are supported by the national council for scienti c and technological development ( cnpq ) , the south american o ce for anticancer drug development ( soad ) , and the childrens cancer institute ( ici - rs )  . jones kl , buzdar au . 
curr stem cell res ther 2009 4 : 30613 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata saito m , aogi k , sekine i , et al . 
palonosetron plus dexamethasone versus granisetron plus dexamethasone for prevention of nausea and vomiting during chemotherapy : a double - blind , double - dummy , randomised , comparative phase iii trial . 
lancet oncol 2009 ; 10 : 11524the role of the funding source for this article should read under agreement with the study sponsor , the medical adviser , medical statistical adviser , and coordinating investigators of the study worked on the design and conduct of this study , and in the analysis and interpretation of the data collaboratively with the principal investigators at the trial sites . 
the trial members should read mamoru tsukuda ( medical adviser ; yokahama city university school of medicine , yokahama , japan ) , chikuma hamada ( medical statistical adviser ; tokyo university of science , tokyo , japan ) , yutaka ariyoshi ( coordinating investigator ; aichi cancer center , aichi hospital , okazaki , japan ) , tomohide tamura ( coordinating investigator , national cancer center , tokyo , japan ) , toshiaki saeki ( coordinating investigator , saitama medical university , hidaka , japan )  . 
 the con icts of interest statement should read : mamoru tsukuda , chikuma hamada , yutaka ariyoshi , tomohide tamura , and toshiaki saeki have received consulting fees or honoraria from taiho pharmaceutical . 
lancet oncol 2010 ; 11 : 15564in this article , the third sentence of the methods section in the summary should read 217 patients with previously treated stage iii ( unresectable ) or stage iv melanoma were randomly assigned a xed dose of ipilimumab of either 10 mg / kg ( n = 72 ) , 3 mg / kg ( n = 72 ) , or 03 mg / kg ( n = 73 ) every 3 weeks for four cycles ( induction ) followed by maintenance therapy every 3 months . 
additionally , the last sentence of the second paragraph of the results section should read median follow - up was for 107 ( iqr 36233 ) , 87 ( 40223 ) , and 83 ( 35153 ) months for 10 mg / kg , 3 mg / kg , and 03 mg / kg groups , respectively . 226 vol 11 march 2010 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper go to thelancetoncology for information for authors see authors / oncology / authorinfo goldhirsch a , wood wc , gelber rd , et al . 
ann oncol 2007 ; 18 : 113344 . arimidex , tamoxifen , alone or in combination ( atac ) trialists group.e ect of anastrozole and tamoxifen as adjuvant treatment for early - stage breast cancer : 100 - month analysis of the atac trial . 
skeletal e ects of exemestane on bone - mineral density , bone biomarkers , and fracture incidence in postmenopausal women with early breast cancer participating in the intergroup exemestane study ( ies ) : a randomised controlled study . 
eur j cancer 2006 ; 42 : 296875 . call for papers : lung cancer , storyboard , and from the archives in 2007 the lancet oncology published themed issues on paediatric oncology and on breast cancer . 
despite many advances in treatment over recent years , lung cancer is still the number one cause of death due to cancer in the world1 and mean relative 5 - year survival is only 126% in europe2 . 
accepted in the lancet oncology papers will be published to coincide with the international lung cancer conference ( [ ilcc ] liverpool , uk , july 912 , 2008 )  . 
if your study describes , in part or wholly , a study accepted for presentation at the ilcc , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication in the lancet oncology can be scheduled to comply with ilccs embargo policies . 
articles should be submitted via the lancet oncologys online submission service , and all authors must clearly state in the covering letter that their submission is in response to the lung cancer call for papers . 
 storyboard will provide and entertaining opportunity to present new oncological in pictorial form and will allow the techniques progressive accumulation of knowledge by leading a reader from panel - to - panel . 
from the archives will be a short report based on a reference of historical importance in oncology that has contributed to a substantial change in thinking in the era originally published . 
please see our information for authors for full details of these new sections . lidia siemaszkiewicz the lancet oncology , london nw1 7by , uk parkin dm , bray f , ferlay j , pisani b . 
the last two sentences of the summarys findings should have read st gallen guidelines identi ed 353 ( 83% ) patients with poor prognosis and discordance with the signature in 168 ( 39% ) patients . 
 nottingham prognostic index recorded 179 ( 42% ) patients with poor prognosis and discordance with the signature in 117 ( 27% ) patients . vol 9 january 2008 re ection and reaction is supportive never - smokers , and women.7 there evidence that patients with egfr - mutant tumours are biologically more indolent ( lim wt , national cancer centre , singapore , personal communication )  . i propose re ning the bipartite model by adding a clinical and biological dimension to it . 
the group of patients with slow - growing tumours are clinically characterised by never - smokers or former smokers who have had little active exposure , are women , and have egfr - activating mutations . 
to improve lung - cancer outcome , we have to adopt a two - pronged approach : identify the population at risk of slow - growing tumours and target them for screening trials , while using coordinated antitobacco e orts to prevent aggressive tumours in others . 
j natl cancer inst 2005 ; 97 : 33946 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata jones lw , eves nd , haykowsky m , joy aa , douglas ps . 
 methods in start trial a , 2236 patients were randomly assigned to receive either 39 gy or 416 gy delivered in 13 fractions over 5 weeks or a global standard of 50 gy in 25 fractions . 
in start trial b , 2215 women were randomly assigned to receive either 40 gy in 15 fractions over 3 weeks or the same control regimen ( 50 gy in 25 fractions ) as in trial a . 
2739 patients were eligible for the quality - of - life study of whom 2208 ( 81% ) were accrued ( 1129 patients from trial a and 1079 from trial b )  . 
the start trials are registered , isrctn59368779 . findings at 5 years , up to 40% women reported moderate or marked changes to the breast after radiotherapy , and arm and shoulder pain a ected up to a third of patients . 
 rates of radiotherapy adverse e ects were lower for the 39 gy regimen in trial a and the 40 gy regimen in trial b , compared with the 50 gy control regimen ; rates of radiotherapy adverse e ects were similar between the 416 gy and 50 gy regimens in trial a . 
adverse change in skin appearance was signi cantly lower for patients who received 39 gy compared with those who received 50 gy ( hr 063 , 95% ci 047084 ) and for those who received 40 gy compared with those who received 50 gy ( 076 , 060097 ) ; no signi cant di erence was observed between patients who received 416 gy and those who received 50 gy in trial a ( 083 , 063108 )  . 
up to a third of women reported moderate or marked pain in the arm and shoulder over 5 years whilst more than 10% experienced moderate or marked arm and hand swelling , with no signi cant di erence in arm / shoulder subscale scores between the regimens in trial a or trial b ; many baseline arm and shoulder symptoms were associated with prior surgery . 
 interpretation a substantial proportion of women report moderate or marked breast , arm , and shoulder symptoms over 5 years of follow - up after radiotherapy , but with no detriment to body image . 
nonetheless , most patients stand to gain from hypofractionated radiotherapy regimens with a potential for fewer adverse e ects ; this strengthens the evidence from the start trials for hypofractionated regimens for women requiring radiotherapy for early breast cancer . funding cancer research uk , uk medical research council , uk department of health . trials randomised introduction the safety and e ectiveness of radiotherapy schedules that deliver a lower total dose in fewer , larger fractions than the international standard regimen has long been uncertain , despite widespread use in early breast cancer . 
in the uk , two ( standardisation of breast radiotherapy [ start ] trials a and b ) were run concurrently to compare the international standard dose ( 50 gy delivered in 25 fractions over 5 weeks ) with alternative schedules based on fewer larger fractions . 
trial b2 was a pragmatic non - inferiority trial comparing the same standard dose with 40 gy in 15 fractions over 3 weeks , a commonly used regimen in the uk . 
the results of trial a showed that rates of late - occurring adverse e ects assessed from photographs were signi cantly lower for the 39 gy regimen compared with the 50 gy control . 
the 416 gy regimen was similar to 50 gy in terms of radiotherapy adverse e ects and local tumour control.1 in trial b , for the 40 gy regimen , local tumour control was at least as good as with 50 gy , and late adverse e ects were reduced.2 regimens with shorter schedules could have a positive e ect on radiotherapy resource use and patients convenience . 
however , over the years , concerns about lengthy treatments might have contributed to womens choice of mastectomy alone over breast - conserving surgery plus radiotherapy , 3 while age and geographic location have vol 11 march 2010 articles also been cited as predictors of mastectomy.4 this situation is not desirable , since good - to - excellent breast cosmesis for most patients has been reported after breast - conserving surgery and a range of radiotherapy schedules , 58 albeit with variable levels of functional morbidity.9 , 10 in a pilot study to the start trials , photographic assessments showed that a third of women had some change in breast appearance over 10 years of follow - up , with evidence of variation according to fractionation regimen over time.11 rates of marked radiation e ects assessed from photographs were signi cantly higher for patients allocated a 429 gy regimen delivered in 13 fractions compared with 50 gy in 25 fractions , with lowest rates for 39 gy in 13 fractions ( although not statistically signi cant )  . 
however , patients ratings of the e ect of radiotherapy on cosmesis and breast , arm , and shoulder symptoms were not recorded in the pilot study and are generally poorly documented in published work.3 , 12 the start trials built on the experience of the pilot study by making a minor adjustment to one of the radiotherapy doses for use in trial a and by including a detailed quality - of - life study in trials a and b.1 , 2 here , using data from each trial separately , we compare radiotherapy schedules with respect to patients selfassessments of normal tissue e ects on the basis of changes in breast , arm , shoulder symptoms and function , and body image over 5 years of follow - up . methods patients participation in the start trials quality - of - life study was open to all radiotherapy centres recruiting patients to the start trials , for which full details of patients and procedures have been published.1 , 2 women with earlystage invasive breast cancer needing radiotherapy after primary surgery were eligible for the start trials if they were older than 18 years , did not have breast reconstruction before radiotherapy , and were available for follow - up . 
all centres could choose at the outset whether or not to participate in the quality - of - life study , with the expectation that all patients in participant centres would be approached for the quality - of - life study . 
no di erences were recorded in terms of radiotherapy planning and delivery between centres opting in and out of the qualityof - life study ( data not shown )  . 
 we reached accrual targets for the quality - of - life study much earlier than expected , so we decided to continue beyond the target sample size to boost precision of estimates and to make the most of the opportunity to accumulate a unique dataset . 
in the last year of recruitment we focused accrual in the quality - of - life study on speci c subgroups those who had undergone mastectomy , had received chemotherapy or were intended to have lymph - node irradiation in trial a , and those who were intended to have lymph - node irradiation in trial b . 
 full details of the organisational aspects of the trials have been published previously.1 , 2 procedures women in start trial a were randomly assigned to radiotherapy over a 5 - week period at either 50 gy in 25 fractions of 20 gy ( control ) or 416 gy in 13 fractions of 32 gy or 39 gy in 13 fractions of 30 gy.1 treatment entailed ve fractions per week in the control group and ve treatments every 2 weeks in each of the 13 fraction schedules ( three fractions one week and two the next )  . 
in trial b , patients were randomly allocated radiotherapy at either 50 gy in 25 fractions of 20 gy over 5 weeks ( control ) or 40 gy in 15 fractions of 267 gy over 3 weeks ( ie , ve fractions per week for both schedules ) .2 randomisation was done via telephone at icr - ctsu . 
 computer - generated random permuted blocks were used as the method of allocation , with patients strati ed by hospital , type of surgery ( breast - conserving surgery or mastectomy ) , and intention to give a tumour - bed boost or not . 
full details of the radiotherapy planning and treatment are presented elsewhere.1 , 2 patients who consented to participate in the quality - oflife study completed a questionnaire booklet in the breast clinic before randomisation . 
we mailed subsequent questionnaires for completion at home at 6 , 12 , 24 , and 60 months post - randomisation ( after checking the individuals current health status with their hospital team or family doctor )  . 
full details of the quality - of - life study are available elsewhere.13 we assessed quality of life with the eortc ( european organisation for research and treatment of cancer ) general cancer scale qlq - c3014 and breast - cancer module ( br23 ) .15 both measures use a four - point response format for individual items ( not at all , a little , quite a bit , very much )  . 
br23 consists of six subscales , of which three were used in the analysis : breast symptoms subscale ( four items [ pain , swelling , oversensitivity , and skin problems in the breast ] ) , arm subscale ( three items [ swelling in arm or hand , arm or shoulder pain , and di culty moving the arm ] ) , and body image ( four items )  . 
 these items included change in skin appearance in the area of the a ected breast ( to account for telangiectasia and other e ects ) , overall change in breast appearance ( to account for asymmetry and distortion ) , rmness to touch of the a ected breast ( to account for brosis ) , and reduction in size of the a ected breast ( to account for shrinkage ) ; the last three items only applied to patients who had completed breast - conserving surgery . 
 included change we assessed body image with a validated , cancer - speci c , ten - item scale ( body image scale ) , 16 which includes the br23 body image subscale . 
 items in self - consciousness with appearance , feeling less physically attractive , less sexually attractive , less feminine , dissatisfaction with appearance when dressed , dissatisfaction with body or scars , body feeling less whole , di culty looking at self naked , and avoidance of people because of appearance . 
this number would allow estimation of the proportion of patients with a particular side - e ect or speci ed degree of morbidity on a qualityof - life domain with a precision of at least 7% ( maximum se 35% ) , and it would enable detection of di erences between every test regimen and the control schedule of at least 20% ( with 90% power and = 001 , allowing for testing of multiple endpoints )  . 
we categorised questionnaire item scores for br23 and protocol items according to whether or not a patient had ever recorded an item as quite a bit or very much , corresponding to moderate or marked e ects . 
we then used survival analysis to measure time to rst reporting of a moderate or marked event , using the date of completion of the questionnaire to calculate length of follow - up from randomisation . 
data are median ( iqr )  . table 1 : characteristics of patients included in quality - of - life study 234 vol 11 march 2010 articles response by direct comparison of the 416 gy and 39 gy regimens in trial a . 
 for continuous symptom scores ( breast and arm symptoms , body image ) , we summarised distributions at every timepoint according to radiotherapy regimen with medians and iqr , since data were skewed and no suitable transformation could be found . 
we compared subscale scores for breast and arm symptoms and body image scale summary scores over the 5 years of follow - up and between regimens with generalised estimating equations , which allow for correlation within repeated observations per individual.17 radiotherapy since patients were strati ed at randomisation by type of primary surgery and intention to give a radiotherapy boost to the tumour bed , we undertook strati ed analyses and tests for interaction to see whether the relative e ects of the radiotherapy regimens varied according to these subgroups . 
for the continuous subscales of breast and arm symptoms and body image , strati ed analyses included all follow - up data in the generalised estimating equation models , but only 5 - year data are presented for simplicity . 
we also did a secondary analysis of arm , shoulder , and hand symptoms , with adjustment for axillary surgery and lymphatic radiotherapy , but since this modi cation made almost no di erence to the treatment e ects , unadjusted results are presented . 
 analysis was on an intention - to - treat basis , which is appropriate for assessment of safety in a trial in which compliance with allocated treatment is high ( 2175 of 2208 [ 99% ] patients in the quality - of - life study received their allocated radiotherapy regimen ) because underestimation of adverse risks is not a concern . 
the start trials are registered , number isrctn59368779 . role of the funding source the funding sources provided peer - reviewed approval for the trials and were observers on the trial steering committee , but had no other role in the study . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results between january , 1999 , and december , 2002 , 4451 women were enrolled into the start trials ( 2236 from 17 centres in trial a and 2215 from 23 centres in trial b )  . 
 of these , 2208 patients were accrued into the quality - oflife study , with 1129 from 13 centres in trial a and 1079 from 21 centres in trial b ( gure 1 )  . 
higher scores indicate more symptoms or concerns . table 2 : breast , arm , or shoulder symptoms and body image scale scores , according to radiotherapy regimen , over time from randomisation photographic assessment study . 
over the whole accrual period , the median proportion per centre of trial patients entered into the quality - of - life study out of those eligible was 91% ( iqr 7597 )  . table 1 shows characteristics of patients accrued into the quality - of - life study . 
more women received adjuvant chemotherapy ( with or without tamoxifen ) in trial a ( 38% , 427 / 1129 ) than in trial b ( 31% , 334 / 1079 ) , consistent with di erences in the composition of patients in the two trials ( table 1 )  . 
 in each regimen in trial a , a radiotherapy boost to the tumour bed was given to just under three - quarters of women who had completed breast - conserving surgery . 
 in each regimen in trial b , about half of breast - conserving surgery patients received a boost . adherence to randomised treatment in each trial was very high ( 1110 / 1129 [ 98% ] in trial a and 1065 / 1079 [ 99% ] in trial b ) .1 , 2 the proportion of completed quality - of - life questionnaires ( based on the number of returned vs expected forms ) was high , with 99% at baseline , decreasing only slightly over time to 91% at year 5.. 
reasons for nonreturn of questionnaires included patients withdrawal from the quality - of - life study , change of address , recurrence , and death , although most patients chose to remain in the study after a recurrence ( gure 1 )  . 
squares to the left of the vertical line indicate when rates of adverse e ects are lower in the test schedule compared with control ; estimates to the right of the line indicate whether rates are higher in the test schedule . 
 ( c ) start trial b , 40 gy vs 50 gy . 236 vol 11 march 2010 articles assessments completed per patient ( including at baseline ) , approximately three - quarters of women returned all ve booklets and the remaining quarter returned at least two . 
 the number of women with a baseline and at least one follow - up assessment ( denominators for the analysis ) were 1080 in trial a and 1037 in trial b , representing 96% of the 2208 patients accrued into the quality - of - life study ( gure 1 )  . 
 with respect to breast , arm , and shoulder symptoms , the most frequently reported adverse e ects in women who had completed breast - conserving surgery were breast hardness and overall change in breast appearance after radiotherapy ( estimated 5 - year rates 41% and 39% , respectively , with moderate or marked symptoms in both trials )  . 
in all radiotherapy regimens , the br23 breast symptom subscale score declined signi cantly from baseline to 60 months ( p < 00001 ) , but no signi cant di erences between regimens were noted in trial a ( p = 05558 ) or trial b ( p = 08757 ; table 2 )  . 
the rate of moderate or marked change in skin appearance after radiotherapy in all women ( breast - conserving surgery and mastectomy ) was signi cantly lower for the 39 gy versus 50 gy regimen in trial a ( hazard ratio 063 , 95% ci 047084 ) and for the 40 gy versus 50 gy regimen in trial b ( 076 , 060097 ) , whereas the 416 gy and 50 gy regimens in trial a did not di er signi cantly ( 083 , 063108 ; gure 2 )  . 
although no further signi cant di erences were found , there was a similar pattern for other post - radiotherapy e ects in the breast , with lowest rates of adverse changes in the 39 gy regimen of trial a and the 40 gy regimen in trial b , and similar rates in the 416 gy regimen compared with 50 gy ( gure 2 )  . 
lower rates for some endpoints were noted in the 39 gy schedule ( eg , breast hardness since radiotherapy , hazard ratio 073 , 95% ci 056095 ; oversensitivity in area of a ected breast 072 , 052098 ; change in breast ap pear ance since radiotherapy 079 , 062102 ; and change in skin appearance since radiotherapy 076 , 056103 )  . pain in the arm and shoulder a ected up to a third of patients over 5 years across regimens , and the 5 - year rate of moderate or marked shoulder sti ness was about 20% ( gure 2 )  . 
baseline arm and shoulder symptoms were associated with axillary surgery ( p = 00129 for arm or shoulder pain ; p = 00319 for arm or hand swelling ) and breast - conserving surgery ( p = 00163 for arm or shoulder pain )  . 
within - patient analysis of individual items at every timepoint showed that many arm or shoulder e ects persisted from baseline ( of 705 patients with moderate or marked arm or shoulder pain during follow - up , 282 [ 40% ] had symptoms at baseline )  . 
results adjusted for baseline scores . table 3 : survival analyses of moderate or marked grade normal tissue e ects from patients self - assessments , according to fractionation schedule , type of primary surgery , and boost in start trial a arm and shoulder symptom subscale scores did not di er signi cantly between regimens ( p = 02071 for trial a and p = 03101 for trial b ; table 2 )  . 
in trial a there was some evidence of fewer arm and shoulder adverse e ects for the 416 gy and 39 gy regimens compared with 50 gy , although these were not statistically signi cant . 
 with respect to body image , 851 of 2117 ( 40% ) women with relevant data reported moderate or marked concerns on at least one body - image item over 5 years of follow - up . 
 vol 11 march 2010 articles 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy 50 gy 40 gy type of primary surgery radiotherapy boost * breast - conserving surgery ( n = 911 ) mastectomy ( n = 126 ) boost ( n = 470 ) no boost ( n = 437 ) change in skin appearance since radiotherapy 080 ( 063103 ) 048 ( 020116 ) 072 ( 052101 ) 088 ( 061127 ) skin problems on or in area of a ected breast 086 ( 065115 ) 226 ( 0431180 ) 076 ( 051114 ) 097 ( 064146 ) pain in area of a ected breast 097 ( 074126 ) 063 ( 022179 ) 105 ( 072153 ) 088 ( 059130 ) oversensitivity in area of a ected breast 118 ( 091153 ) 055 ( 019154 ) 133 ( 092190 ) 105 ( 072153 ) swelling in area of a ected breast 089 ( 062129 ) 418 ( 0612837 ) 094 ( 057153 ) 080 ( 045142 ) arm or shoulder pain shoulder sti ness 103 ( 083129 ) 092 ( 047180 ) 101 ( 074136 ) 104 ( 075144 ) 094 ( 070125 ) 110 ( 047258 ) 087 ( 058131 ) 101 ( 066154 ) di culty in raising or moving arm sideways 099 ( 073135 ) 079 ( 035177 ) 090 ( 060137 ) 103 ( 065164 ) arm or hand swelling 112 ( 078160 ) 065 ( 020217 ) 065 ( 040104 ) 229 ( 129407 ) data are crude hazard ratio ( 95% ci )  . 
results adjusted for baseline scores . table 4 : survival analyses of moderate or marked grade normal tissue e ects from patients selfassessments according to fractionation schedule , type of primary surgery , and boost in start trial b the most typically reported moderate or marked concerns were feeling physically less attractive ( 496 / 2111 [ 23% ] ) and dissatisfaction with body ( 483 / 2112 [ 23% ] )  . 
body image scale summary scores were similar in all regimens over time ( p = 09990 for trial a and p = 03405 for trial b ; table 2 )  . 
 in subgroup analyses , the relative e ects of the randomised radiotherapy schedules on patient - reported symptoms did not vary signi cantly according to type of primary surgery ( breast - conserving surgery or mastectomy ) or whether or not a radiotherapy boost to the tumour bed was given ( tables 35 )  . 
 discussion in our study , detailed self - assessments by patients in the start trials of normal tissue responses to breast radiotherapy over 5 years provided independent evidence that use of a lower overall radiotherapy dose in fewer larger fractions does not result in an increase in adverse e ects or worse body image for most women , compared with the international standard regimen of 50 gy in 25 fractions . 
breast pain has been implicated as a risk factor for poor long - term quality of life1820 and should be monitored by clinical teams , whereas functional symptoms such as shoulder sti ness could warrant early clinical attention . 
breast and arm pain and oedema might have stronger associations than cosmesis with long - term quality of life21 and , therefore , these are important outcomes to assess in clinical trials . 
 little investigation has been done of self - reported breast , arm , and shoulder symptoms and functional outcomes after radiotherapy , 21 , 22 and thus our results make a potentially important contribution to the discussion of the e ects of breast radiotherapy for informed consent . 
 patients reports of transient and short - term e ects of radiotherapy have been reported , with limited e ect on overall quality of life.3 , 22 , 25 , 26 in future trials , well - de ned , frequent , objective , and subjective assessments of relevant symptoms are desirable , 27 , 28 to establish the duration and functional outcomes of acute e ects with more precision . 
 we have reported adverse e ects up to 5 years after radiotherapy , but we acknowledge that follow - up beyond 5 years is needed to assess further the pattern and severity of normal tissue e ects , since they cannot be assumed to decrease over time , and some e ects arise much later on . 
 follow - up in the start trials is ongoing , to assess the long - term e ects of the fractionation schedules , although ndings of the pilot study showed ( with median follow - up of 10 years ) that relative di erences remained unchanged over time.11 interest in the late e ects of speci c treatments for breast - cancer survivors is growing , making clinical trials a suitable vehicle for gathering these data . 
 breast changes that showed variation between radiotherapy regimens did not translate directly into di erences in ratings of general body image concerns , suggesting that women did not experience breast changes in a way that a ected their overall body image . 
this nding contrasts with the important e ect on body image reported by these women before starting radiotherapy , when worse body image was associated with younger 238 vol 11 march 2010 articles age , having mastectomy , and chemotherapy.13 the absence of variation in scores for body image between regimens might also indicate that the body image scale is designed to assess a range of concerns about overall attractiveness and appearance rather than speci c aspects of breast appearance . 
use of a radiotherapy boost and type of primary surgery have an adverse e ect on cosmesis and patient - reported symptoms , 5 , 8 , 29 but they did not a ect the comparison of the randomised schedules in the start trials . 
 in two other randomised controlled trials , researchers have compared the long - term e ect of hypofractionated radiotherapy regimens at 5 years , but patient - reported normal tissue damage and cosmesis were not recorded.11 , 30 the sensitivity of radiation dose to observer - rated breast symptoms and appearance was con rmed in the pilot study to the start trials , 11 and adverse changes in breast appearance from photographic assessments were signi cantly lower in the 39 gy in 13 fractions regimen compared with the 50 gy in 25 fractions control , with highest rates in patients who received 429 gy in 13 fractions . 
by contrast , in a canadian randomised trial comparing 425 gy in 16 fractions against 50 gy in 25 fractions , observer - rated cosmesis did not di er between schedules.30 the start trials comprise a well - de ned cohort of patients , which is representative of women with early breast cancer in the uk . 
individuals in the quality - of - life study were recruited from all parts of the uk , although london and the south of england were over - represented by comparison with annual distribution of new breast cancer cases for these areas ( 46% vs 35% , respectively ) .31 data for ethnic origin were not obtained in the start trials , so a statement about generalisability of our ndings in that respect is not possible . 
 to our knowledge , our study is the rst in which selfreported breast symptoms have identi ed di erences over 5 years between alternative radiotherapy regimens in early breast cancer . 
our ndings accord with observer - rated photographic changes reported separately in the start trials , 1 , 2 which indicated that the di erence between the two test dose levels in trial a in 20 gy - fraction equivalents can be estimated to be 10% . 
in our study , change in skin appearance was the outcome over 5 years that best discriminated between radiotherapy schedules , but other post - radiotherapy e ects ( eg , breast shrinkage and hardness ) and breast symptoms showed comparable patterns . 
breast - conserving surgery patients only . table 5 : breast , arm , or shoulder symptoms and body image scale scores at 5 years * according to radiotherapy regimen , type of primary surgery , and boost where both the symptomatic impact of treatment and the extent of disruption to womens lives relating to length of treatment can a ect quality of life . in conclusion , considerable morbidity still arises due to e ects on normal tissues of treatments for early breast cancer , and patients self - assessments are important to ascertain the extent and duration of these e ects . 
 however , these ratings by patients in the start trials strengthen evidence in favour of hypofractionated regimens , with a potential for fewer adverse e ects on the normal breast tissues . 
jry ( chief investigator for vol 11 march 2010 articles the start trials and chair of the trial management group ) contributed to data interpretation and helped to write the report . 
all authors were members of the start trial management group . con icts of interest the authors declared no con icts of interest . acknowledgments we thank all patients who participated in this study ; the clinical leads who were co - investigators in the start trials and their teams ; and the research nurses and data managers at participating centres . 
we also acknowledge the contributions of former icr - ctsu sta who worked on the start quality - of - life study , including c dawson , l gamaldo , and c harper . 
we acknowledge the trial steering group ( chaired by a barrett , university of east anglia , norwich ) and consumers , current , or past representatives of the radiotherapy action group exposure ( rage ) , who were observers to the trial management group . 
we thank cancer research uk , the uk medical research council , and the uk department of health for providing funds to undertake this research ( grant g9600656 )  . 
the cancer research uk grant number for the start trial is cruk / 96 / 001 . re ection and reaction ms has received consultancy fees from glaxosmithkline , and payment for lectures from physicians educational resources . 
production of hyperpolarized [ 1 , 4 - 13c2 ] malate from [ 1 , 4 - 13c2 ] fumarate is a marker of cell necrosis and treatment response in tumors . 
isocitrate dehydrogenase - 1 mutations : a fundamentally new understanding of di use glioma ? lancet oncol 2010 ; published online july 7 , doi : 10.1016 / s1470 - 2045 ( 10 ) 70053 - xin table 1 , data cited for acute myelogenous leukaemia should read 1% not 0% of idh1 mutations . 
these corrections have been made to the online version as of october 4 , 2010 . isocitrate wild - type idh1 nadp + nadph + co2 + h + - ketoglutarate mutant - idh1 nadph + h + nadp + 2 - hydroxyglutarate wild - type 922 vol 11 october 2010 re ection and reaction 23 cycles . 
notably , this extension of treatment has translated into a durable remission , ongoing survival beyond 32 months , and maintenance of the patients quality of life and functional capacity . 
 to my knowledge , this case represents the rst , albeit anecdotal , report of preventing both cold - induced and cumulative psn in a patient receiving oxaliplat although dose - limiting toxicity has not yet been seen in this patient , his cumulative dose for second - line oxaliplatin already surpasses his rst use of the drug , and more than doubles the median of six cycles and 492 mg / m2 reported for the optimox ( oxaliplatin reintroduction ) strategy.8 , 9 such a de nitive and clinically meaningful bene t for the prevention of psn has not been possible by use of pharmacological measures , 6 which have been disappointing by comparison , or without risks to outcome , such as those associated with calcium - magnesium infusions.2 the challenge in con rming these ndings will be to design an appropriate trial . 
one that maximises use of the historical record of oxaliplatin - induced psn so as to avoid exposing patients to an inactive placebo might well be the most expedient route to improving the quality of life of thousands of patients who su er from this potentially preventable adverse event . 
 michael castro department of cancer medicine , st marys hospital , amsterdam , ny 12010 , usa mcastromd@yahoo.com the author declared no con icts of interest . gamelin l , boisdron - celle m , morel a , et al . 
e ect of intravenous ( iv ) calcium and magnesium ( ca / mg ) versus placebo on response to folfox + bevacizumab ( bev ) in the concept trial . 
2008 gastrointestinal cancers symposium ; orlando , fl , usa ; jan 2527 , 2008 ; abstract 280 . gamelin l , boisdron - celle m , delva r , et al . 
randomized double blind ( db ) placebo ( plcb ) controlled phase iii study assessing the e cacy of xaliproden ( x ) in reducing the cumulative peripheral sensory neuropathy ( psn ) induced by the oxaliplatin ( ox ) and 5 - fu / lv combination ( folfox4 ) in rst - line treatment of patients ( pts ) with metastatic colorectal cancer ( mcrc )  . 
 in this article , in tables 6 and 7 ( pages 78990 ) , some data for relative survival and 95% ci for prostate , kidney , and thyroid cancer , and nonhodgkin lymphoma were incorrect . 
 methods 1941 tumours from 2391 women recruited to neat / br9601 were analysed on tissue microarrays for her2 and top2a ampli cation and deletion , her13 and ki67 expression , and duplication of chromosome 17 centromere enumeration probe ( ch17cep )  . 
log - rank analyses identi ed factors a ecting relapse - free and overall survival , and regression models tested independent prognostic e ect of markers , with adjustment for known prognostic factors ( age , nodal status , oestrogen - receptor status , grade , and tumour size )  . 
in univariate analyses , only her2 ampli cation and top2a deletion were signi cant prognostic factors for relapse - free ( hazard ratio [ hr ] 159 , 95% ci 132192 , p < 00001 ; and 152 , 120192 , p = 00006 , respectively ) and overall survival ( 179 , 147219 , p < 00001 ; and 162 , 126208 , p = 00002 respectively )  . 
by contrast , in multivariate analyses , ch17cep duplication was associated with signi cant improvements in both relapse - free ( hr 092 , 95% ci 072118 for tumours with normal ch17cep vs 052 , 034081 for tumours with abnormal ch17cep ; p for interaction = 0004 ) and overall survival ( 094 , 072124 vs 057 , 036092 ; p for interaction = 002 ) with anthracycline use . interpretation in women with early breast cancer receiving adjuvant chemotherapy , the most powerful predictor of bene t from anthracyclines is ch17cep duplication . 
in view of the location of her2 / top2a on chromosome 17 , ch17cep duplication might explain the inconsistencies in previous studies of factors predicting bene t from anthracyclines . funding cancer research uk and the scottish breast cancer clinical trials group . introduction breast cancer is recognised as a disease of substantial molecular diversity.1 the search for predictive biomarkers that can be applied to guide selection of appropriate therapies for di erent patient subgroups is intensifying . 
 the her2 oncogene is frequently cited as a biomarker of sensitivity or resistance to endocrine treatment and chemotherapy.2 , 3 the her2 oncogene is ampli ed or overexpressed in about 25% of early breast cancer cases for which adjuvant anthracycline use is considered in the uk.4 several observational reports have linked anthracycline sensitivity to her2 positivity.5 , 6 her2 ampli cation is linked both to multiple mechanistic pathways ( proliferation , dedi erentiation , apoptosis , dna repair ) 7 and to several molecular events that are now viewed separately from her2 ampli cation , such as top2a alterations and chromosome 17 ( ch17 ) centromeric duplication.8 , 9 ch17 centromeric duplication indicates duplication of the ch17 centromere enumeration probe ( ch17cep ) 8 , 9 and is not necessarily an indicator of chromosomal duplication . 
data suggest polysomyde ned by duplication of the cepin fact represents duplication of subchromosomal regions , including the cep , rather than whole chromosome duplication.10 for this report , the term ch17cep duplication represents increased cep17 copies and should be interpreted in view of these emerging data . her2 might be the central focus or driver for a region of genomic instability centred around 17q12 , frequently being associated with ampli cation or deletion of other genes within this region including grb7 , rara ( retinoic acid receptor ) , thra1 , cdc6 , and top2a . 
her2 ampli cation is also closely associated with ch17cep duplication.9 ch17 is the second most gene - dense chromosome in the human genome , housing several genes with key roles in breast cancer ( brca1 , her2 ) and dna repair ( tp53 , rad51c , rad52b ) .11 however , 266 vol 11 march 2010 articles ch17cep duplication has not been mechanistically linked to these pathways , which makes the key molecular change associated with clinical bene t from anthracyclinebased chemotherapy di cult to identify . 
 research so far has focused almost exclusively on her2 and top2a , both of which have been linked to anthracycline sensitivity.6 , 12 nevertheless , genes such as brca1 , rad51c , and tp53 , all with a role in dna repair , might also modify response to chemotherapy . 
 the uk national epirubicin adjuvant trial ( neat / br9601 ) trials examined the addition of the anthra cycline epirubicin to cyclophosphamide , methotrexate , and uorouracil ( cmf )  . 
we planned prospectively to investigate markers predictive of anthracycline bene t , including type i receptor tyrosine kinase ( rtk ) signalling pathways ( epidermal growth factor receptor [ egfr ] , her1 , her2 , her3 ) , ki67 , top2a alterations , and ch17cep duplication . 
data for her13 , ki67 , and top2a in the br9601 study were reported previously.12 methods study design and patients neat and br9601 recruited 2391 pre - menopausal and post - menopausal women with completely excised , histologically con rmed breast cancer with a clear indication for adjuvant chemotherapy.14 the 2021 patients in neat were randomly assigned , in a 1 : 1 randomisation , to receive either epirubicin ( 100 mg / m intravenously every 3 weeks ) for four cycles followed by cmf ( cyclophosphamide 100 mg / m orally days 114 or cyclophosphamide 600 mg / m days 1 and 8 , intravenously ; methotrexate 40 mg / m days 1 and 8 ; uorouracil 600 mg / m days 1 and 8 every 4 weeks ) for four cycles or to receive cmf for six cycles . 
the 370 patients in br9601 were randomly assigned , in a 1 : 1 randomisation , to receive either epirubicin ( 100 mg / m every 3 weeks ) for four cycles ( cyclophosphamide 750 mg / m , methotrexate 50 mg / m , and uorouracil 600 mg / m every 3 weeks given intravenously ) for four cycles or to receive cmf for eight cycles.14 both protocols were approved by central and local ethics committees , and patients provided written informed consent before randomisation . 
there was a prospectively preplanned agreement for a joint analysis with the primary outcomes of relapse - free and overall survival.14 followed by cmf for the present study , routine pathology tissue blocks were retrieved from the neat / br9601 trials and tissue microarrays constructed according to current guidelines for breast tissue collections.15 blocks were retrieved and tissue microarrays constructed from 80% of neat samples ( 1623 / 2021 ) and from 86% of br9601 samples ( 318 / 370 ) for this study . 
 triple - colour uorescent in - situ hybridisation ( fish ) and immunohistochemistry fish was done with a triple - colour probe for her2 , top2a , and ch17 ( abbot vysis , maidenhead , uk ) as described previously.12 her2 ampli cation was de ned as a ratio of her2 to ch17cep of 20 or greater , top2a ampli cation as a ratio of top2a to ch17cep of more than 15 , and top2a deletion as a ratio of top2a to ch17cep of less than 08 . 
 table 1 : biomarker analysis and relation with overall and relapse - free survival 100 100 100 100 100 100 100 100 100 vol 11 march 2010 articles documented as previously described.16 , 17 ch17 copy number was assessed by counting all cells with a minimum of one ch17 signal per cell , and ch17cep duplication de ned as greater than 186 observed cep signals per cell.9 statistical analysis the 1941 eligible samples from this trial population would be adequate to identify , with at least 80% power , prognostic hazard ratios ( hrs ) of 15 and treatment by marker interactions of 20 , with the exception of top2a , for which the values would be 16 and 23 , respectively , owing to the lower frequency of top2a aberrations in this patient population.18 sas ( version 9.1 ) was used for statistical analysis . 
kaplan - meier and log - rank analysis were used to compare relapse - free and overall survival as described previously.19 hrs and their cis were calculated from log - rank statistics . 
graphical examination showed no clear departure from proportional hazards . the analysis planto assess the interaction of type i rtks ( her13 ) , ki67 , top2a , and ch17cepwas prospectively planned , before any statistical analysis and merging of biomarker and clinical data . 
 268 vol 11 march 2010 articles duplication , ki67 , and her13 were considered in univariate analyses , together with conventional prognostic factors ( age , nodal status , oestrogen - receptor status , grade , and tumour size )  . 
her2 , top2a , and ch17cep as individual markers were entered in a nal cox model together with the treatment term and each of the three treatment - by - marker interactions , with adjustment for conventional prognostic factors ( age , nodal status , oestrogen - receptor status , grade , and tumour size )  . 
 the study conformed to the remark guidelines.19 role of the funding sources the sponsors of the study had no role in study design , data collection , data analysis , data interpretation , or writing of the report . 
the corresponding author had full access to all the data in the study and had nal responsibility for the decision to submit for publication . results the population included in this tissue microarray study was representative of patient and tumour characteristics within the main trial ( webappendix p 1 )  . 
of the 1941 patients included in this analysis , 630 ( 32% ) relapsed and 516 ( 27% ) died during follow - up ( median 74 years , iqr 6386 ) ; data from one patient were lost . 
 vol 11 march 2010 articles number at risk ecmf 216 events ecmf 215 events 181 deaths 177 deaths 47 events 92 events 43 deaths 78 deaths number at risk ecmf years years figure 3 : relapse - free and overall survival for patients with tumours exhibiting ch17cep duplication and ch17cep normal ( a ) relapse - free survival for chcep17 normal . 
of the eligible cases , 367 of 1762 ( 21% ) were her2 ampli ed , and ch17cep duplication was recorded in 406 ( 23% )  . the prognostic e ect of each biological marker assessed in this study was rst tested with respect to relapse - free and overall survival in all 1762 patients , irrespective of their allocated adjuvant chemotherapy . 
in univariate analysis , her2 ampli cation , top2a deletion , and her13 and egfr expression were signi cantly associated with a worse outcome for both relapse - free and overall survival ( table 1 ) , although the e ect observed with egfr expression was of borderline signi cance . 
we noted no such relation with top2a ampli cation , ch17cep duplication , or ki67 expression ( table 1 )  . subsequent analyses focused on possible di erential e ects of markers on relapse - free and overall survival between patients receiving anthracycline treatment ( epirubicin and cmf ) and those given cmf alone . 
 figures 1 and 2 show hr estimates for relapse - free and overall survival by treatment and molecular biomarker subgroup , with biomarkers dichotomised as positive / high or negative / low . 
we detected no signi cant interactions between treatment with epirubicin and biomarker for ch17cep duplication was associated with increased bene t from epirubicin plus cmf compared with cmf ( gures 13 ) for both relapse - free and overall survival ( univariate treatment by marker interactions p = 0004 and p = 002 , respectively )  . 
for tumours with normal ch17cep copy number , very little or no bene t was derived from the addition of the anthracycline ( relapsefree survival hr 092 , 95% ci 076111 , gure 3a ; overall survival 094 , 077116 , gure 3c )  . 
conversely , for patients with tumours exhibiting ch17cep duplication , the relative risk of relapse and death was substantially lower for those receiving epirubicin and cmf than cmf ( relapse - free survival 051 , 95% ci 036 073 , gure 3b ; overall survival 056 , 039082 , gure 3d )  . 
 a single cox regression model was done to test the e ects of anthracyclines , her2 ampli cation , top2a alteration , and ch17cep duplication ( including interactions with treatment for each marker ) simultaneously after adjustment for age , nodal status , oestrogen - receptor status , grade , and tumour size ( table 2 )  . 
the interaction for ch17cep duplication and epirubicin therapy remained signi cant for both relapse - free and overall survival ( table 2 )  . 270 vol 11 march 2010 articles both her2 ampli cations and top2a alterations ( ampli cations or deletions ) measured by fish were signi cantly associated with ch17cep duplication ( p < 00001 )  . 
her2 - ampli ed tumours were twice as likely to exhibit ch17cep duplication as were those that were not ampli ed ( 37% [ 136 / 367 ] vs 19% [ 270 / 1395 ] , p < 00001 )  . 
 top2a ampli ed or deleted tumours were also signi cantly more likely to exhibit ch17cep duplication than were those that were not top2a altered ( 31% [ 52 / 169 ] vs 22% [ 354 / 1593 ] and 65% [ 124 / 191 ] vs 18% [ 282 / 1571 ] , respectively , webappendix p 2 )  . 
the hrs for relapse - free survival in patients with tumours exhibiting ch17cep duplication were 065 ( 95% ci 032129 ) with her2 ampli cation and 046 ( 026080 ) without ; similarly the hrs were 062 ( 033116 ) with top2a alterations and 046 ( 025 084 ) without . 
by contrast , in patients whose tumours did not show ch17cep duplication , hrs for relapse - free survival were 085 ( 050145 ) with her2 ampli cation and 0.91 ( 069121 ) without ; and 101 ( 051201 ) with top2a alteration and 091 ( 070119 ) without . 
this exploratory subgroup analysis ( gure 4 ) linked bene t from anthracyclines to ch17cep duplication irrespective of her2 ampli cation or top2a alterations . discussion in a prospectively planned and adequately powered analysis of biomarkers of anthracycline bene t within the neat / br9601 clinical trials , ch17cep duplication , but not her2 or top2a , was identi ed as a predictive biomarker of anthracycline bene t in early breast cancer . 
a signi cant treatment - by - marker interaction was recorded for both relapse - free and overall survival in multivariate analyses corrected for conventional pathological factors and also for treatment - by - marker interactions for her2 and top2a . 
a signi cant reduction in the risk of both relapse and death after treatment with anthracycline - containing chemotherapy regimens was noted in patients whose tumours showed evidence of ch17cep duplication . 
we also noted a signi cant treatment - by - marker interaction between treatment with anthracycline - containing polychemotherapy and ch17cep duplication . suggested ki67 previous evidence from smaller , underpowered , ( proliferation ) , her13 analyses expression , top2a , and her2 as potential biomarkers of anthracycline bene t ; 2 , 6 , 12 , 2023 however , these markers provided no signi cant predictive value in the present study . 
validation in a large meta - analysis is planned to con rm this e ect and to lend support to adoption of this biomarker in routine clinical practice . to the best of our knowledge , the data presented here represent the rst time that one can clearly de ne a hr ( 95% ci ) p value relapse - free survival age 50 years 112 ( 094133 ) breast conserving surgery 083 ( 069099 ) node involvement 183 ( 161207 ) < 00001 oestrogen - receptor negative 093 ( 073118 ) oestrogen - receptor positive 075 ( 060094 ) tumour grade tumour diameter ecmf her2 ampli cation top2a alteration ch17cep duplication her2 * ecmf interaction top2a * ecmf interaction ch17cep * ecmf interaction overall survival age 50 years 129 ( 110152 ) 101 ( 100101 ) 089 ( 072110 ) 161 ( 117221 ) 140 ( 099200 ) 143 ( 109187 ) 103 ( 066161 ) 090 ( 055149 ) 098 ( 081119 ) 054 ( 035083 ) 0005 breast conserving surgery 082 ( 067100 ) node involvement 173 ( 151198 ) < 00001 oestrogen - receptor negative 088 ( 069114 ) oestrogen - receptor positive 066 ( 052084 ) tumour grade tumour diameter ecmf her2 ampli cation top2a alteration ch17cep duplication her2 * ecmf interaction top2a * ecmf interaction ch17cep * ecmf interaction 134 ( 111160 ) 101 ( 100101 ) 092 ( 072116 ) 136 ( 093200 ) 137 ( 101184 ) 091 ( 056147 ) 085 ( 050145 ) 060 ( 038095 ) 184 ( 131258 ) 00005 022 004 053 001 0002 0002 027 0003 006 001 089 069 086 005 034 00008 0002 0005 047 012 004 070 054 003 adjusted for age group , surgery group , nodal group , oestrogen - receptor status , grade , and tumour size . 
ch17cep = chromosome 17 centromere enumeration probe . table 2 : e ect of her2 , top2a , and ch17cep on relapse - free and overall survival , adjusted by patient and tumour characteristics for whom subgroup of patientsthose with ch17cep duplication for whom adjuvant anthracyclines provide signi cant additional treatment bene t , while identifying a larger group alternative , non - anthracyclinecontaining regimens should be considered . 
these data remain of value at a time when trastuzumab is frequently used to treat patients with her2 - positive breast cancer , since about two - thirds of patients whose tumours have ch17cep duplication do not exhibit her2 ampli cation . 
by contrast with ndings reported here , ma5 indicated that bene t from anthracyclines was associated with her2 and top2a ampli cation.25 , 26 the reduction in risk of relapse was much the same for patients in both neat / br9601 and ma5 whose tumours exhibited ch17cep duplication when given an anthracycline rather than cmf alone ; no bene t was recorded in patients with tumours with normal ch17cep.24 no signi cant treatment - by - marker interaction for either her2 or top2a was detected in the multivariate regression analysis , although her2 gene ampli cation was , as expected , prognostic for both overall and relapse - free survival in both treatment groups . 
this nding strongly suggests that neither gene is of clinical signi cance in terms of predicting clinical bene t from adjuvant anthracyclines , and rea rms the strong prognostic e ect of her2 ampli cation . 
previous data from other groups22 , 2528 are , however , con icting , with some studies suggesting her2 and others her2 and top2a as potential predictive markers for anthracycline bene t . 
preliminary results of a meta - analysis30 using individual patient data in 1944 cases from four clinical trials , 12 , 22 , 26 , 27 including 295 of the br9601 trial patients reported here , also showed no signi cant predictive e ect with her2 , and only a marginally signi cant e ect for top2a for disease - free but not overall survival . 
we believe that many previous smaller studies lacked the power to robustly test interactions , and that neither her2 ampli cation nor top2a gene alterations can be regarded as predictive for response to anthracyclines . 
a review of previously published studies ( webappendix p 3 ) accords with these con icting results.22 , 2528 , 3133 only the ma5 trial shows a signi cant interaction with her2 ; an early study by paik and colleagues32 of similar size to our study , but using only immunohistochemistry , also did not show a signi cant interaction between her2 and anthracyclines . 
 ki67 was not associated with bene t from anthracyclines , a result that does not contradict previous results , suggesting highly proliferative tumours bene t preferentially from chemotherapy . of note , her2 and top2a ampli cation and top2a deletion were signi cantly associated with ch17cep duplication , but the bene t from the anthracycline seemed to be restricted to patients whose tumours exhibited ch17cep duplication ( gure 4 )  . 
patients whose tumours were either her2 ampli ed or top2a ampli ed or deleted , but were normal for ch17cep , gained no apparent bene t from addition of the anthracycline ( gure 4 )  . 
this result also suggests that in our own previous report , 12 on her13 expression in the br9601 subgroup within the current trial , the small sample size masked the e ect reported here . 
cmf = cyclophosphamide , methotrexate , uorouracil . 272 vol 11 march 2010 articles duplication in top2a deleted cases in particular could explain the previously paradoxical result that these patients bene t from anthracyclines when other data suggest that top2a deleted cell lines are anthracycline resistant.22 , 34 the results of the bcirg006 study6 suggest that in a population , all of whom have tumours that are her2 ampli ed , there might be an additional e ect of top2a ampli cation , although the role of ch17cep duplication has not been explored in bcirg006 so far . 
 our present data do not rule out such an additional e ect of top2a in her2 - positive cancers since our study was done in a mixed her2 population , and might be underpowered to detect any additional e ect of top2a above that seen for ch17cep in the her2ampli ed subgroup . 
we de ned ch17cep duplication as an increase in the relative mean copy number of the cep , which hybridises to the pericentromeric - satellite repeat on ch17 , above that observed in non - tumour breast tissues.9 although there are several di erent approaches used to identify cep17 duplication , only two have been validated against observations in non - neoplastic breast samples.9 , 35 the di erent cuto s in these studies relate solely to di erent counting assumptions ( watters and colleagues9 count all cells with at least one ch17cep signal ; wang and colleagues35 count cells with at least two ch17cep signals ) , but in all other aspects they are identical . 
our approach does not invalidate previous de nitions of her2 ampli cation since these de nitions were also based on the ratio of the her2 gene and the ch17 centromere , irrespective of the underlying chromosomal defect present . 
our de nition of her2 ampli cation still identi es patients with poor prognosis , her2 protein overexpression , and potential for response to trastuzumab . including the observation that ch17cep duplication is associated with bene t from anthracyclines could o er a pragmatic approach to selection of patients for such therapy . 
recent reports suggest that ch17 polysomy is far less common in early breast cancer than was previously suggested , and that ch17cep duplication does not simply indicate polysomy or tumour aneuploidy but also identi es cancers with subchromosomal duplication or ampli cation of the ch17cep region ( which is close to the her2 amplicon ) .10 , 36 at present we cannot distinguish which of these di erent chromosomal abnormalities might be associated with the underlying mech anism of anthracycline sensitivity . 
the many mechanistic explanations for the observations reported here should be explored before we can suggest strategies to improve the future potential of dna - damaging agents in populations who are resistant to anthracyclines . trial population in conclusion , in this large , adequately powered , ( neat / br9601 ) , ch17cep clinical duplication , but not her2 or top2a , was identi ed as a biomarker of anthracycline bene t in patients with early breast cancer . 
validation in a larger meta - analysis is needed to provide con rmatory evidence to support the adoption of this biomarker in routine clinical practice . contributors jmsb was responsible for translational study design , coordination , data collection , statistical analysis plan , management of biological data , and the writing of the report . 
afm was responsible for collection of tissue from br9601 , tissue microarray construction , doing the molecular analyses and scoring of samples , and coordinating the data collection ; and contributed to the writing of the report . 
 ep , he , pp , and cc were responsible for setting up pathological review of all the tumour samples from the neat trial , guiding tissue microarray construction , and development and maintenance of the associated translational research databases . 
all other authors declared that they have no con icts of interest . acknowledgments the scottish cancer therapy network and institute for statistics and disease coordinated the br9601 trial and provided funding for tissue collection of br9601 blocks ; the neat trial was coordinated by the cancer research uk clinical trials unit , birmingham , and funded by cancer research uk and an educational grant from pharmacia ; the translational research was funded by cancer research uk , and vysis provided fish kits at reduced price . 
abbott provided funding in kind via free or reduced price reagents . vol 11 march 2010 articles re ection and reaction lactic acid cycle and is used clinically for the treatment of lactic acidosis , has been shown to decrease lactic acid in the brain in rats , thereby decreasing ischaemic damage.5 this drug improves lactic acidosis after experimental arter ial blockade and might , therefore , also decrease neu ral damage due to ischaemia after radiotherapy . 
 dichloro acetate could also have a potential antitumour e ect , because many cancerseg , glioblastomause the glucose - lactic acid cycle in mitochondrial respiration.6 a phase ii trial has now opened to test the safety and e cacy of dichloroacetate for the treatment of malignant gliomas.7 a drug used in the prevention of delayed bowel injury might also be useful in the prevention of cognitive impairment after radiotherapy . 
haydont and co - workers8 have recently shown in rats that protection of the bowel from delayed radiation injury can be achieved by use of the anticholesterol drug pravastat however , this drug had limited bene t in acute - bowel injury . 
if cognitive impairment , which is likely to be a late reaction to radiotherapy in the brain , has a similar underlying mechanism to delayed - bowel injury , then this drug might have a use in the management of such injury in the brain . the prevention of neural impairment by other methods has also been assessed . 
from these sites , stem cells can migrate to damaged areas elsewhere in the bradue to the fact that only a small percentage of brain metastases occur in the dentate gyrus , the shielding of this area during radiotherapy might , in many situations , be possible , thereby preventing the damage of these repair cells themselves.9 clinical research on the prevention of neurological impairment after radiotherapy is already being done . 
 for example , in a small study of 15 patients with brain tumours , bevacizumab was shown to decrease capillary leakage and radiation necrosis.10 furthermore , erythropoietin has been used to modify irradiation damage to the spinal cord in patients with malignant spinal - cord compression , 11 and , thus , might have a role in modifying radiation damage to the brain . some of these drugs are already commonly used for other indications . 
 john healy 5 claremont villas , glenageary , county dublin , ireland healyjb@eircom.net the author declared no con icts of interest . schagen sb , vardy j , on behalf of the steering committee of the international cognition and cancer task force . 
lancet oncol 2007 ; 8 : 85253 . captopril in treating patients with non - small cell lung cancer or limitedstage small cell lung cancer that has been previously treated with radiation therapy with or without chemotherapy . 
e ect of bevacizumab on radiation necrosis of the braint j radiat oncol biol phys 2007 : 67 : 32326 . loblaw da , holden l , xenocostas a , et al . 
 1056 vol 8 december 2007 articles lancet oncol 2010 ; 11 : 53042 published online may 17 , 2010 doi : 10.1016 / s14702045 ( 10 ) 70095 - 4 see re ection and reaction page 501 * see end of paper for members and a liations . correspondence to : prof tim key , endogenous hormones and breast cancer collaborative group , cancer epidemiology unit , nu eld department of clinical medicine , university of oxford , richard doll building , roosevelt drive , oxford , ox3 7lf , uk tim.key@ceu.ox.ac.uk insulin - like growth factor 1 ( igf1 ) , igf binding protein 3 ( igfbp3 ) , and breast cancer risk : pooled individual data analysis of 17 prospective studies the endogenous hormones and breast cancer collaborative group * summary background insulin - like growth factor 1 ( igf1 ) stimulates mitosis and inhibits apoptosis . 
some published results have shown an association between circulating igf1 and breast - cancer risk , but it has been unclear whether this relationship is consistent or whether it is modi ed by igf binding protein 3 ( igfbp3 ) , menopausal status , oestrogen receptor status or other factors . 
 the endogenous hormones and breast cancer collaborative group was established to analyse pooled individual data from prospective studies to increase the precision of the estimated associations of endogenous hormones with breastcancer risk . methods individual data on prediagnostic igf1 and igfbp3 concentrations were obtained from 17 prospective studies in 12 countries . 
the odds ratios ( ors ) with 95% cis of breast cancer associated with increasing igf1 concentrations were estimated by conditional logistic regression in 4790 cases and 9428 matched controls , with strati cation by study , age at baseline , and date of baseline . 
all statistical tests were two - sided , and a p value of less than 005 was considered signi cant . findings igf1 concentrations , adjusted for age , were positively associated with height and age at rst pregnancy , inversely associated with age at menarche and years since menopause , and were higher in moderately overweight women and moderate alcohol consumers than in other women . 
the ors for a di erence in igf1 concentration between the highest and lowest fth were 138 ( 95% ci 114168 ) for oestrogen - receptor - positive tumours and 080 ( 057113 ) for oestrogen - receptor - negative tumours ( p for heterogeneity = 0007 )  . interpretation circulating igf1 is positively associated with breast - cancer risk . 
 oestrogens are important in the aetiology of breast cancer , and there is laboratory evidence for crosstalk in cells between the signalling pathways for oestrogens and igf1.24 it is therefore important to examine whether the association of igf1 with breast - cancer risk varies according to the oestrogen - receptor status of the tumour or circulating concentrations of oestradiol . 
 around 99% of igf1 circulates bound to igf binding proteins , with most bound to igf binding protein 3 ( igfbp3 ) in a ternary complex with an acid labile subunit . 
less than 1% of igf1 circulates unbound.1 most the endogenous hormones and breast cancer collaborative group was established to do pooled analyses of individual data from prospective studies to increase the precision of the estimated associations of endogenous 530 vol 11 june 2010 articles hormones with breast - cancer risk.25 in this study we undertook a collaborative analysis of data from 17 studies to investigate the associations of igf1 and igfbp3 with breast - cancer risk . 
we also examined consistency between studies , associations in subgroups including menopausal status at blood collection and oestrogen receptor status , the e ects of adjustment of igf1 and igfbp3 for each other and for other risk factors , and the joint associations of igf1 , oestradiol , and testosterone with breast cancer risk in postmenopausal women . methods data collection studies were eligible for the collaborative analysis if they had prospectively collected blood samples and data on circulating igf1 , igfbp3 , and breast - cancer risk . 
 potentially eligible studies were through pubmed using the terms igf1 , igfbp3 , and breast identi ed cancer , by searching the reference lists of identi ed studies , and by correspondence with study investigators . 
samples taken 07 : 3009 : 00 130c 130c 80c 80c originally a case - cohort study ; matched sets created for this analysis same year of birth same year of birth same month and year time of day , menopausal status at blood collection and diagnosis , fasting status same month and year time of day , menopausal status at diagnosis , fasting status , luteal day of sample 3 months 3 months menopausal status , phase of cycle in premenopausal 5 years 89 days menopausal status , daylight saving period , recruitment centre plco , usa22 19932001 non - fasting 80c 24 months 24 months originally a case - cohort study ; matched sets created for this analysis pphv , netherlands11 prospect - epic , netherlands11 sof , usa26 198791 199397 198688 non - fasting non - fasting fat - free overnight and morning diet 20c 1 year same month and year place of residence 80c initially 1 year same month and year none then - 196c 120c 24 months 24 months whi - os , usa21 199398 fasting 70c 24 months 24 months originally a case - cohort study ; matched sets created for this analysis originally a case - cohort study ; matched sets created for this analysis * stored in liquid nitrogen at 196c , except in denmark in nitrogen vapour at 150c , and in sweden in electric freezers at 80 c . 
 table 1 : description of studies vol 11 june 2010 articles ( pphv ) and prospect - epic , from the netherlands ; 11 study of osteoporotic fractures ( sof ) , from the usa ; 26 and the womens health initiative , observational study ( whios ) , from the usa.21 table 1 summarises the study designs . 
 details of the assay methods for igf1 and igfbp3 are shown in table 2 ; 10 studies used serum , six used plasma , and one used both , but for convenience we refer to plasma concentrations throughout this paper . 
menopausal status at the time of blood collection was de ned on the basis of questions about the number of menstrual periods in the previous year and details of any hysterectomy and ovariectomy ; the details varied slightly between studies and are in the original publications . 
women were excluded from the analyses if they were perimenopausal or of unknown menopausal status , if they were using hormonereplacement therapy or other exogenous sex hormones at the time of blood collection , or if data were missing for dates of birth , blood collection , or diagnosis ( for cases )  . 
 statistical analysis of the 17 studies that contributed data , 11 provided data for women who were premenopausal at blood collection , and 15 provided data for women who were postmenopausal at blood collection . 
for the cross - sectional analyses , data were included from all women in the original studies who had not been diagnosed with breast cancer ( n = 10 022 ) ; in the analyses of breast - cancer risk the data were arranged in matched sets , and some potential controls were not matched ; therefore , the number of controls with data on igf1 is less in the risk analyses ( n = 9428 )  . concentrations of igf1 and igfbp3 were positively skewed ; therefore , log - transformed concentrations were used for all parametric analyses . 
correlations between igf1 and igfbp3 among premenopausal and postmenopausal controls were calculated using standardised log - transformed concentrations within each study , the standardised values being calculated by subtracting the mean log concentration and dividing by the standard deviation of the log concentration . 
the associations of igf1 with risk factors for breast cancer were examined in the controls using linear regression , calculating geometric mean concentrations and 95% cis according to categories of these factors . 
the heterogeneity between studies in the associations of igf1 with risk factors was assessed by adding a study factor interaction term to the model and using the f test to calculate its signi cance . 
a similar approach was used to assess heterogeneity according to menopausal status . 11 of the original studies contributing to the collaborative analysis had used matched nested case - control designs , and the remaining six had used unmatched controls or a case - cohort design ( janus , 20 kkh denmark , 12 mccs , 19 plco , 22 sof , 26 and whi - os21 )  . 
some used density sampling , meaning that an individual participant could appear more than once in a data le ; in order to avoid double - counting women in the cross - sectional analyses , we created a pooled dataset in which duplicate observations were deleted , with the case observation retained where a participant appeared as both a case patient and a control . 
we retained the original matched sets where available , otherwise for the case - cohort studies we created new matched sets in which each case was matched with up to four controls , matching by study , date of blood collection ( plus or minus 24 months ) , age at blood collection ( plus or minus 24 months ) and , for janus only , 20 county of residence . 
 conditional logistic regression was used to calculate the odds ratio ( or ) for breast cancer in relation to the plasma concentrations of igf1 and igfbp3 , categorising women in each study according to the quintiles of hormone concentration for the controls in that study . 
study - speci c cut - points were used because the absolute concentrations of igf1 and igfbp3 vary between studies because of laboratory variation ; further explanation of this approach is provided in previous publications.25 , 27 to provide a summary measure of risk , we calculated a linear trend by scoring the fths of the plasma igf1 or igfbp3 concentrations as 0 , 025 , 05 , 075 , and 1 ; under the assumption of linearity , a unit change in this trend variable is equivalent to the or comparing the highest with lowest fth of hormone concentration.27 heterogeneity in linear trends among studies was assessed using a test , calculating the statistic as the di erence between the sum of the model values for each study and the model value from the all - studies analysis . 
we also used tests to examine whether there was evidence of heterogeneity in the associations of igf1 with breast - cancer risk according to subgroups de ned by menopausal status at blood collection and other factors . the we examined the e ect on the association with breastcancer risk of adjusting igf1 and igfbp3 for each other . 
 we also investigated the associations of igf1 with breastcancer risk after adjusting , one factor at a time , for various established reproductive and hormonal risk factors for breast cancer : age at menarche ( < 12 , 1213 , 14 years ) ; figure 1 : geometric mean igf1 concentrations ( nmol / l with 95% ci ) among controls by selected factors adjusted for study and age at blood collection , as appropriate . 
p < 005 for test of interaction with study . parity ( 0 , 1 , 2 , 3 , 4 full - term pregnancies ) ; age at rst fullterm pregnancy ( < 20 , 2024 , 2529 , 30 years ) ; body mass index ( bmi ; < 225 , 225249 , 250274 , 275299 , 300 kg / m ) ; previous use of oral contraceptives ( never or ever ) ; and , for postmenopausal women only , type of vol 11 june 2010 articles menopause ( natural or surgical ) ; time since menopause ( 04 , 514 , 15 years ; natural postmenopausal women only ) ; previous use of hormone - replacement therapy ( never or ever )  . 
for postmenopausal women , we also investigated the associations of igf1 with breast - cancer risk after adjustment for plasma concentrations of oestradiol and testosterone , and the associations of igf1 with breast - cancer risk with joint classi cation according to plasma oestradiol and testosterone concentrations . all statistical tests were two - sided , and statistical signi cance was set at the 5% level . 
 role of the funding source the funding source had no role in study design , data collection , data analysis , data interpretation , or the writing of the report . 
mean age at baseline ranged from 355 ( sd 78 ) to 477 ( sd 31 ) for premenopausal women , and from 543 ( sd 61 ) to 718 ( sd 49 ) for postmenopausal women . 
across the studies , mean bmi ranged from 231 ( sd 35 ) to 284 ( sd 63 ) kg / m , and the median time between blood collection and diagnosis ranged from 1 ( iqr 03 ) to 17 ( iqr 818 ) years . 
 table 3 : participant characteristics by study and case - control status vol 11 june 2010 hormone fifth cases / or ( 95% ci ) or and 95% ci p for trend igf1 pre - menopausal women 1 articles controls 374 / 829 392 / 831 367 / 814 390 / 822 414 / 800 100 105 ( 088126 ) 105 ( 087125 ) 110 ( 092132 ) 121 ( 100145 ) 558 / 1069 113 ( 098132 ) 573 / 1083 114 ( 098133 ) 596 / 1060 124 ( 107144 ) 618 / 1039 133 ( 114155 ) 950 / 1900 110 ( 098123 ) 940 / 1897 110 ( 098124 ) 986 / 1882 118 ( 105132 ) 1032 / 1839 128 ( 114144 ) 405 / 816 384 / 828 374 / 797 372 / 798 380 / 773 100 096 ( 080114 ) 097 ( 081117 ) 094 ( 078114 ) 100 ( 082122 ) 524 / 1051 581 / 1041 542 / 1034 625 / 1003 097 ( 084113 ) 110 ( 095128 ) 106 ( 090123 ) 123 ( 104145 ) 908 / 1879 097 ( 086108 ) 955 / 1838 105 ( 093117 ) 914 / 1832 101 ( 090114 ) 1005 / 1776 113 ( 099128 ) postmenopausal women 508 / 1081 100 all women 882 / 1910 100 igfbp3 premenopausal women postmenopausal women 544 / 1067 100 all women 949 / 1883 100 075 figure 2 : odds ratios ( or ) for breast cancer associated with igf1 and igfbp3 among premenopausal women ( at blood collection ) , postmenopausal women ( at blood collection ) , and all women the black squares indicate the ors and the horizontal lines show the 95% cis . 
geometric mean concentrations of igfbp3 ranged from 680 ( 95% ci 657704 ) for premenopausal women and from 697 ( 668727 ) to 1606 ( 15791633 ) nmol / l for postmenopausal women . 
 data on igf1 and igfbp3 were available for 10 022 and 9889 controls , respectively ( these numbers are larger than those for the matched - set analyses because data for unmatched controls were included in the cross - sectional analyses )  . 
igf1 and igfbp3 were associated with each other , with correlations of 038 and 050 ( data not shown ) in premenopausal and postmenopausal women , 0050 00002 < 00001 0921 0012 0062 respectively ( both p < 00001 )  . 
the associations of igf1 with selected reproductive and other factors in control women are shown in gure 1 ( equivalent analyses for igfbp3 are in the webappendix p 2 )  . 
geometric mean igf1 was 26% lower for women aged 65 years and above than for women aged less than 45 years ; the other results presented in gure 1 are adjusted for age . 
igf1 was 7% higher in women who were at least 170 cm tall than in women who were less than 155 cm tall , and was higher in women with a bmi of 250274 kg / m than in thinner or more overweight women . 
igf1 was higher in women who drank up to 19 g / d of alcohol than in women who did not drink or who drank at least 20 g / d of alcohol , and was 4% lower for women who had undergone menarche at ages 14 years and over than for women who had undergone menarche before age 12 years . 
 igf1 was weakly positively associated with breast - cancer risk for premenopausal women ( test for trend , p = 0050 ) and strongly positively associated with breast - cancer risk for postmenopausal women ( test for trend p = 00002 ; gure 2 ) ; the test for heterogeneity by menopausal status at blood collection was not statistically signi cant ( test for heterogeneity p = 0894 )  . 
in the individual studies , the ors for the linear trend for premenopausal women ranged from 072 to 269 , with an overall estimate of 118 ( 95% ci 100140 ) , and the median ratio of the igf1 concentration in the top versus the lowest fth was 23 for for ( gure 3a )  . 
the ors postmenopausal women ranged from 043 to 273 , with an overall estimate of 130 ( 95% ci 113149 ) , and the median ratio of the igf1 concentration in the top versus the lowest fth was 24 ( gure 3b )  . 
in the combined analysis of premenopausal and postmenopausal women , 536 vol 11 june 2010 articles those in the highest fth of igfbp3 had an or of 113 ( 95% ci 099128 ) compared with women in the lowest fth ( test for trend p = 0062 )  . 
adjustment of the association between igf1 and breast - cancer risk for igfbp3 had no signi cant e ect on the or ; the or for linear trend before adjustment was 124 ( 95% ci 111138 ) and after adjustment was 124 ( 110141 )  . 
by contrast , adjustment of the association between igfbp3 and breast - cancer risk for igf1 reduced the or for linear trend from 112 ( 95% ci 100126 ) to 099 ( 087114 )  . 
analyses of breast - cancer risk in relation to the molar ratio of igf1 to igfbp3 showed a signi cant positive association , but the magnitude was less than for the analyses of igf1 ; ors in increasing fths of the ratio were 117 ( 099126 ) , ( 95% ci 104132 ) , 112 114 ( 101129 ) and 123 ( 108140 ) ( test for trend p = 0009 )  . 
the ors varied according to oestrogen - receptor status ; the or for a linear trend in igf1 was signi cant among oestrogen - receptor positive cases ( or 138 , 95% ci 114168 ) , but not for oestrogenreceptor negative tumours ( or 080 , 057113 ) and the test for heterogeneity was signi cant ( p = 0007 )  . 
 we examined the e ect on the association of igf1 with breast - cancer risk of adjustment , one factor at a time , for height , age at menarche , number of full - term pregnancies , age at rst full - term pregnancy , use of hormonal contraceptives , type of menopause ( postmenopausal only ) , time since menopause ( postmenopausal only ) , previous use of hormonal therapy for menopause ( postmenopausal only ) , bmi ( premenopausal and postmenopausal analysed separately ) , plasma oestradiol concentration ( postmenopausal only ) , plasma testosterone concentration ( postmenopausal only ) , time of day of blood collection , and the phase of the menstrual cycle at blood collection ( premenopausal only )  . 
none of these adjustments altered the or for igf1 and breast cancer by more than 2% ( data not shown ) with the exception of adjustment for testosterone in postmenopausal women , which reduced the or for an 80 percentile di erence in igf1 from 130 ( 95% ci 108155 ) to 124 ( 104149 )  . 
whi - os = womens health initiative , observational study . was signi cantly positively associated with risk in three out of 15 studies of postmenopausal women ( webappendix pp 3 , 4 )  . 
there was signi cant heterogeneity in the association of igfbp3 with breast - cancer risk according to oestrogen receptor status ; igfbp3 was non - signi cantly positively associated with risk for oestrogen - receptorpositive breast cancer and non - signi cantly inversely associated with risk for oestrogen - receptor - negative breast cancer ( test for heterogeneity p = 0039 ; webappendix p 5 )  . discussion the results of this collaborative analysis show that plasma concentrations of igf1 are positively associated with breast - cancer risk . 
hrt = hormone replacement therapy . modi ed by menopausal status at blood collection or by igfbp3 concentrations , but seems to be con ned to oestrogen - receptor - positive tumours . factors , the strengths of our study are that the data and plasma samples were all collected prospectively , that it includes almost all the available data from published studies worldwide , and that we were able to adjust for other potential risk including endogenous sex hormones . 
this method assumes the true concentrations across the quintiles are similar in all the studies , and if this assumption is not correct then the estimates of ors might be biased.27 however , because heterogeneity between studies in risk estimates was not evident , this assumption does seem reasonable . 
there was some evidence of heterogeneity between studies in some of the cross - sectional analyses , suggesting that caution should be maintained in the interpretation of these analyses . previous studies have examined the associations of igf1 with other factors . 
relevant publications are cited below , but it should be noted that some of these are from the studies contributing to this collaborative analysis . igf1 was inversely associated with age , with no obvious additional decline in concentrations around age 50 years , suggesting that menopause itself does not have a marked e ect on igf1 . 
no signi cant association of igf1 with height was noted in two previous analyses in adults , 29 , 33 but these results might be compatible with the small association noted in the current analysis . 
igf1 was higher in women with a bmi of 250 to 274 kg / m than in thinner or more overweight women , as described previously.34 most circulating igf1 is produced by the liver , and it is possible that a low bmi is associated with low igf1 synthesis due to a relatively low supply of nutrients to the liver , whereas obesity is associated with low igf1 synthesis in the liver due to compromised liver function.35 igf1 was not associated with smoking , consistent with previous observations.29 , 30 , 36 in relation to alcohol , igf1 was higher for women who drank a small amount than for those who drank no alcohol or those who drank 20 g or more per day . 
other observational studies had similar results.29 , 3740 in randomised trials , 15 g / d of alcohol had no e ect on igf1 in postmenopausal women , whereas 30 g / d caused a decrease in igf1 by 95% for premenopausal women and by 49% for postmenopausal women.41 , 42 igf1 did not di er between women with or without a rst - degree family history of breast cancer . 
laboratory studies have shown that oestrogen increases igf receptor levels in breast - cancer cells , 51 whereas in oestrogen - receptor - negative breastcancer cells the levels of igf1 receptor are decreased , and igf1 is non - mitogenic.52 igfbp3 was positively associated with breast - cancer risk , but this association was weak , and was eliminated by adjustment for igf1 , suggesting that the association of igfbp3 with risk is due to its positive correlation with igf1 . 
it seems that , at least in the current dataset , the igfbp3 measures do not add substantial information in assessing the relationship of igf1 with breast - cancer risk . 
in addition to its role in transporting igf1 , laboratory studies have shown that igfbp3 can have direct e ects on cell behaviour which can promote apoptosis , but under other circumstances can act against apoptosis.53 data on igfbp - 1 and igfbp - 2 have also been contributed for our collaborative analyses , but currently there are too few data to provide robust analyses . 
better understanding of the roles of igfbinding proteins as potential modulators of the association between igf1 and breast - cancer risk might come from further data on igfbp1 and igfbp2 , from measures of intact igfbp3 , 54 or from measures of bioavailable igf1.55 the or for igf1 is smaller than the ors for both oestrogens and androgens and breast - cancer risk in postmenopausal women , which have been shown in data mostly from the same epidemiological studies ; high concentrations of oestradiol and testosterone are associated with around a doubling in breast - cancer risk.25 , 5658 in our analyses , adjustment for oestradiol and testosterone had little e ect on the association of igf1 with breast - cancer risk for postmenopausal women , and there was no evidence of an interaction between igf1 and oestradiol or testosterone in relation to breast - cancer risk . 
nevertheless , a better understanding of the joint e ects of hormones on breast - cancer risk is needed.59 association we observed between igf1 and age at menarche has been noted previously.43 , 44 we observed a non - linear association between igf1 and parity , with the lowest concentrations for women who had four or more full - term pregnancies ; previous studies have not reported any associations between igf1 and parity.30 , 4345 igf1 was also positively associated with age at rst full - term pregnancy . 
igf1 was marginally higher for women who had previously used hormonal contraceptives than for women who had not , but did not vary according to previous use of hormonal therapy for menopause . 
in future analyses we will examine the relationships of igf1 with endogenous sex hormones . the associations of igf1 with height , age at menarche , age at rst full - term pregnancy , and time since menopause are compatible with the possibility that these factors a ect breast - cancer risk partly through their relationships with igf1 . 
this association did not vary signi cantly according to menopausal status at blood collection or according to the risk factors for breast cancer examined , and was not attenuated by adjustment for other risk factors including igfbp3 , reproductive factors , and , for postmenopausal women , bmi , oestradiol , and testosterone . 
if the association was due to an e ect of preclinical tumours on igf1 ( reverse causality ) , 46 then it would be expected to be weaker in those with a greater time interval between blood collection and diagnosis . 
 a previous meta - analysis based on studies published up to 2006 concluded that the association of igf1 with breastcancer risk is limited to premenopausal women , 47 but our analysis includes four large more recent studies with over 1500 additional patients and shows a clear association of igf1 with breast - cancer risk in postmenopausal women . 
the correlations ( intra - class or spearman ) between baseline and repeat measures ranged from approximately 04 to 09 over 1 to 15 years.10 , 17 , 19 , 4850 it is therefore likely that the observed association between igf1 concentrations and breastcancer risk is an underestimate of the true association , but more reproducibility data are required . 
 vol 11 june 2010 articles the association of igf1 with breast - cancer risk was not altered by adjusting for age at menarche , parity , age at rst full - term pregnancy , use of exogenous hormones , and bmi , suggesting that the relationship of igf1 with breastcancer risk is not confounded by these other risk factors . 
it is not known whether this association is causal , but there are plausible biological mechanisms that could explain such an e ect.1 , 2 the magnitude of the observed association is modest , but the true association could be substantially larger because of measurement error , and further work is needed to reliably quantify the relationship . 
 co - authors from womens health initiative observational study : mj gunter , te rohan , hd strickler ( department of epidemiology and population health , albert einstein college of medicine , new york , ny , usa )  . con ict of interest statement for the writing committee , tjk , pna , and gkr declared no con icts of interest . 
we thank the women who participated in the collaborating studies , the research sta , the collaborating laboratories and the funding agencies in each of the studies . articles lancet oncol 2010 ; 11 : 6674 published online october 28 , 2009 doi : 10.1016 / s14702045 ( 09 ) 70306 - 7 * see webappendix for investigators department of clinical oncology , university college hospital , london , uk ( prof j tobias frcp ) ; cancer research uk sussex psychosocial oncology group , brighton and sussex medical school , brighton , uk ( k monson msc ) ; department of clinical oncology , the christie hospital , manchester , uk ( n gupta frcr ) ; faculty of medicine , bute medical school , university of st andrews , st andrews , uk ( prof h macdougall frcr ) ; department of oncology , queen elizabeth hospital birmingham , birmingham , uk ( prof j glaholm frcr ) ; department of oral and maxillofacial surgery , st bartholomews hospital , london , uk ( prof i hutchison frcs ) ; and cancer research uk and ucl cancer trials centre , university college london , london , uk ( a hackshaw msc , l kadalayil phd ) correspondence to : mr allan hackshaw , cancer research uk and ucl cancer trials centre , university college london , 90 tottenham court road , london w1t 4tj , uk ah@ctc.ucl.ac.uk chemoradiotherapy for locally advanced head and neck cancer : 10 - year follow - up of the uk head and neck ( ukhan1 ) trial je rey s tobias , kathryn monson , nirmal gupta , hugh macdougall , john glaholm , iain hutchison , latha kadalayil , allan hackshaw , on behalf of the uk head and neck cancer trialists group * summary background between 1990 and 2000 , we examined the e ect of timing of non - platinum chemotherapy when combined with radiotherapy . 
 methods between jan 15 , 1990 , and june 20 , 2000 , 966 patients were recruited from 34 centres in the uk and two centres from malta and turkey . 
patients with locally advanced head and neck cancer , and who had not previously undergone surgery , were randomly assigned to one of four groups in a 3 : 2 : 2 : 2 ratio , strati ed by centre and chemotherapy regimen : radical radiotherapy alone ( n = 233 ) ; radiotherapy with two courses of chemotherapy given simultaneously on days 1 and 14 of radiotherapy ( sim alone ; n = 166 ) ; or 14 and 28 days after completing radiotherapy ( sub alone , n = 160 ) ; or both ( sim + sub ; n = 154 )  . 
patients who had previously undergone radical surgery to remove their tumour were only randomised to radiotherapy alone ( n = 135 ) or sim alone ( n = 118 ) , in a 3 : 2 ratio . 
the primary endpoints were overall survival ( from randomisation ) , and event - free survival ( efs ; recurrence , new tumour , or death ; whichever occurred rst ) among patients who were disease - free 6 months after randomisation . 
among patients who did not undergo surgery , the median overall survival was 26 years ( 99% ci 1942 ) in the radiotherapy alone group , 47 ( 2678 ) years in the sim alone group , 23 ( 1635 ) years in the sub alone group , and 27 ( 1647 ) years in the sim + sub group ( p = 010 )  . 
for every 100 patients given sim alone , there are 11 fewer efs events ( 99% ci 121 ) , compared with 100 given radiotherapy , 10 years after treatment . 
among the patients who had previously undergone surgery , median overall survival was 50 ( 99% ci 1880 ) and 46 ( 2276 ) years in the radiotherapy alone and sim alone groups ( p = 070 ) , respectively , with corresponding median efs of 37 ( 99% ci 1159 ) and 30 ( 1256 ) years ( p = 085 ) , respectively . 
the percentage of patients who had a signi cant toxicity during treatment were : 11% ( radiotherapy alone , n = 25 ) , 28% ( sim alone , n = 47 ) , 12% ( sub alone , n = 19 ) , and 36% ( sim + sub , n = 55 ) among patients without previous surgery ; and 9% ( radiotherapy alone , n = 12 ) and 20% ( sim alone , n = 24 ) among those who had undergone previous surgery . 
the percentage of patients who had a signi cant toxicity at least 6 months after randomisation were : 6% ( radiotherapy alone , n = 13 ) , 6% ( sim alone , n = 10 ) , 4% ( sub alone , n = 7 ) , and 6% ( sim + sub , n = 9 ) among patients who had no previous surgery ; and 7% ( radiotherapy alone , n = 10 ) and 11% ( sim alone , n = 13 ) among those who had undergone previous surgery . 
the most common toxicity 6 months after treatment was xerostomia , but this occurred in 3% or less of patients in each group . interpretation concurrent non - platinum chemoradiotherapy reduces recurrences , new tumours , and deaths in patients who have not undergone previous surgery , even 10 years after starting treatment . 
patients who have undergone previous surgery for head and neck cancer do not bene t from non - platinum chemotherapy . funding cancer research uk , with support from university college london and university college london hospital comprehensive biomedical research centre . introduction head and neck cancers are relatively common ( about 7500 new cases in the uk and 45 000 in the us each year ) , and are increasing in incidence in some countries such as the uk , mainly because of smoking and excessive alcohol intake.13 standard treatment until 1990 was surgical resection or radical radiotherapy , sometimes both . 
toxicity is especially important since vol 11 january 2010 articles patients are typically un t , often with coexistent illness.4 , 5 over the past decade the role of chemotherapy has become clearer . 
the number of agents found to be active in squamous - cell carcinoma has increased , and the best ways of combining them continue to be investigated . the uk head and neck ( ukhan ) cancer group was established in 1990 to investigate the e ectiveness of chemotherapy used in conjunction with radiotherapy and surgery . 
at the time , it was believed that chemotherapy given at time as radical radiotherapy ( ie , concurrent ) and afterwards ( ie , maintenance ) could be e ective . 
other objectives were to assess the e ect of timing and duration of chemotherapyie , whether two courses should be given simultaneously with ( sim alone ) or subsequent to ( sub alone ) the radiotherapy course , or both simultaneously and following radiotherapy ( four courses , sim + sub )  . 
 the same methods patients patients with locally advanced squamous - cell carcinoma of the head and neck were included in a factorial randomised trial if they were judged to be suitable for initial treatment or radical radiotherapy as either following an operation ( generally patients at high risk of recurrence following surgery due to margin status or advanced stage of disease at presentation )  . 
patients were eligible if they satis ed the following criteria : age 18 years or over ; considered t enough to receive any of the trial treatments ; had histological con rmation of squamous - cell carcinoma , with t2 to t4 primary lesions ( including node - negative cases ) or were node positive ; had full normal blood count , and creatinine and urea levels within normal ranges ; showed no evidence of distant metastases ; and had no previous treatment for the cancer other than surgical excision . 
 all patients gave written informed consent . procedures the extent of previous surgery , radiotherapy regimen , and nutritional support with either nasogastric or percutaneous - endoscopic radiologically inserted gastrostomy feeding , were based on local policies to maximise recruitment . 
 surgery before randomisation was also determined by local practice , and could involve resection of the primary tumour alone with or without comprehensive neck - node resection , provided that the intention was to completely 713 patients had no surgery 253 patients had surgery 233 patients allocated to radiotherapy alone 166 patients allocated to 160 patients allocated to 154 patients allocated to sim alone sub alone sim + sub 135 patients allocated to radiotherapy alone 118 patients allocated to sim alone 5 patients ineligible 1 early stage disease 2 ineligible history 1 previous treatment 1 other 7 patients ineligible 1 early stage disease 3 ineligible history 1 previous treatment 2 other 1 patients ineligible 1 early stage disease 5 patients ineligible 1 early stage disease 2 previous treatment 2 other 9 patients ineligible 1 early - stage disease 2 occult primary 1 ineligible history 3 previous treatment 2 other 14 non - compliers to chemotherapy * 50 non - compliers to chemotherapy * 68 non - compliers to chemotherapy * 32 non - compliers to chemotherapy * 233 patients analysed 166 patients analysed 160 patients analysed 154 patients analysed 135 patients analysed 118 patients analysed 178 events for overall survival 115 events for overall survival 128 events for overall survival 122 events for overall survival 95 events for overall survival 79 events for overall survival 197 events for efs 125 events for efs 141 events for efs 132 events for efs 103 events for efs 89 events for efs figure 1 : trial pro le efs = event - free survival . 
only 26 patients did not fully meet the eligibility criteria , but they were included in the analysis . vol 11 january 2010 articles see online for webappendix age ( years ; median and range ) male female tumour stage unknown nodal status negative positive unknown stage stage ii stage iii stage iv unknown site of primary larynx oral cavity oropharynx nasopharynx hypopharynx other unknown surgery group margins cleared * neck dissection done 188 ( 81 ) 45 ( 19 ) 19 ( 8 ) 106 ( 46 ) 52 ( 22 ) 56 ( 24 ) 129 ( 55 ) 104 ( 45 ) 64 ( 27 ) 71 ( 30 ) 97 ( 42 ) 1 ( < 1 ) 73 ( 31 ) 41 ( 18 ) 78 ( 34 ) 14 ( 6 ) 22 ( 9 ) 5 ( 2 ) clear the tumour . 
usually at the outset these surgery patients were scheduled for adjunctive postoperative radiotherapy because of their advanced disease . although radical radiotherapy could be given according to local practice , it had to be approved by the trial steering committee , and investigators were asked to adhere to it for all patients within that centre , regardless of treatment allocation . 
the south - east co - operative oncology group regimen involved irradiation with planned elds to adequately cover the primary tumour in unresected cases , and in most cases lymph - node drainage area . 
another common regimen , used in birmingham , edinburgh , and some other centres , had the following schedule : 55 gy given in 20 fractions ( 275 gy per fraction ) over 4 weeks to the primary tumour and rst station lymphatic drainage , and 4125 gy in 15 fractions to the elective neck . 
50 gy given in 20 fractions ( 25 gy per fraction ) was given postoperatively . chemotherapy regimens were either methotrexate alone or vincristine , bleomycin , methotrexate , and uorouracil ( vbmf ) ; webappendix.8 , 9 sim started on days 1 and 14 concurrently with radiotherapy , and sub started 14 and 28 days after completing radiotherapy . 
 methotrexate was given intravenously in two doses of 100 mg / m : the rst dose was given 24 h before radiotherapy and the second dose was given on day 14 of radiotherapy . 
folinic acid rescue was given if serum methotrexate concentration at 24 h after treatment exceeded 04 mol / l.10 vbmf consisted of vincristine 14 mg / m ( maximum 2 mg ) , bleomycin 30 mg , uorouracil 500 mg , and methotrexate 100 mg / drugs were given intravenously by slow bolus injection except bleomycin , which was given by intramuscular injection . 
 other endpoints were control of local and regional disease ( ie , the complete remission rate ) at 6 months ; time to recurrence ; death from head and neck cancer ; and toxicity during and after treatment , which was classi ed as signi cant if hospitalisation was required during chemoradiation , therapy was required to alleviate chronic treatment - related toxicity ( eg , dilatations for oesophageal strictures ) , or clinicians recorded an event as severe after treatment . 
although toxicity was not recorded on a standardised scale during the trial , we compared the reported adverse - event grading and descriptions with the common terminology criteria for adverse events ( ctcae ) version 3 , as part of the statistical analysis . 
 * primary site resection margins were clear . table 1 : distribution of baseline characteristics according to trial group vol 11 january 2010 articles a non - complier was de ned as a patient who did not receive the full dose according to the trial protocol . 
in october , 2008 , an active data chase was completed to ascertain which patients had died or had a recurrence or new tumour , and the date patients were last seen alive . lists centrally at randomisation and masking block strati ed randomisation was used , and allocations were concealed from investigators and patients by generating random number the coordinating centre ( cancer research uk and university college london cancer trials centre )  . 
patients were to be allocated to radiotherapy alone , sim alone , sub alone or sim + sub if they had not had previous surgery , using a block size of nine ( allocation ratio 3 : 2 : 2 : 2 , which is 1 : 2 in favour of chemotherapy , to increase the total number of patients given chemotherapy ) ; or only to radiotherapy alone or sim alone if they had previously undergone surgery , using a block size of ve ( allocation ratio 3 : 2 )  . 
 randomisation strati cation factors were centre ( which automatically strati es for radiotherapy regimen and all other for patient management ) and chemotherapy regimen ( though all but two centres used a single regimen during the trial )  . 
hospital clinicians recruited patients , and centres telephoned the co - ordinating centre , who assigned each patient a treatment allocation after recording the eligibility and strati cation factors . local policies statistical analysis the sample size of about 1000 patients was based on detecting an increase in 5 - year survival from 25% in the radiotherapy - alone group to 35% in the chemotherapy groups combined , with 90% power and two - sided 5% level of statistical signi cance . 
all p values are two - sided , and 99% ci were used to allow for having multiple comparisons ( 95% for the primary objective of any chemotherapy versus radiotherapy alone )  . 
expressed as a percentage of the number disease free at 6 months . table 3 : the number and causes of death , and the number of rst events in patients who were disease free at 6 months after randomisation ( used to examine event - free survival ) , according to trial group 3 ( 3 ) 2 ( 2 ) 3 ( 3 ) 2 ( 2 ) 1 ( < 1 ) 10 ( 8 ) 4 ( 3 ) 1 ( < 1 ) 1 ( < 1 ) 14 ( 12 ) 6 ( 5 ) 6 ( 5 ) 2 ( 2 ) 32 ( 27 ) 55 ( 47 ) 21 ( 18 ) 3 ( 25 ) 25 ( 27 ) 18 ( 20 ) 19 ( 21 ) vol 11 january 2010 articles radiotherapy alone sim alone sub alone sim + sub p = 010 number at risk radiotherapy alone sim alone sub alone sim + sub p = 070 number at risk radiotherapy alone sim alone time from randomisation ( years ) figure 2 : overall survival according to treatment groups for patients who had no surgery ( a ) and those who had undergone surgery ( b ) before randomisation sim = radiotherapy with two courses of chemotherapy given simultaneously on days 1 and 14 of radiotherapy . 
the median length of follow - up was 10 years after censoring those who had died ( maximum of 17 years ) , with 4397 person - years in total . 
the trial pro le is shown in gure 1 ; baseline characteristics are shown in table 1 . 7% of patients ( 69 / 966 ) were known to have not completed the planned radiotherapy course ( table 2 )  . 
27% of patients ( 164 / 598 ) allocated to receive chemotherapy did not complete their full course of treatment , mainly due to disease progression , acute toxicity , or withdrawal from treatment . 
among patients without prior surgery , only 8% ( 14 / 166 ) of the sim alone group were non - compliers to chemotherapy , compared with 31% ( 50 / 160 ) and 44% ( 68 / 154 ) in the sub alone and sim + sub groups respectively . 
27% ( 32 / 118 ) of sim alone patients who had surgery did not complete their chemotherapy . 69% ( 662 / 966 ) of patients were disease - free at 6 months ( webappendix )  . 
among those without previous surgery , the proportion disease - free at 6 months was highest in the sim alone group ( 73% , 122 / 166 ) compared with the other groups : radiotherapy alone ( 63% , 146 / 233 ) , sub alone ( 66% , 106 / 160 ) , and sim + sub ( 62% , 95 / 154 )  . 
 there was little di erence among patients who had undergone previous surgery : radiotherapy alone ( 76% , 102 / 135 ) and sim alone ( 77% , 91 / 118 )  . there were 717 deaths among all 966 patients , and 483 efs events among the 662 patients who were disease free at 6 months ( table 3 )  . 
estimated 5 - year overall survival was 43% ( 95% ci 3848 ) and efs was 32% ( 2737 ) in the radiotherapy - alone group ( patients with or without previous surgery )  . 
the chemotherapy or radiotherapy regimen used did not a ect the results ( webappendix )  . kaplanmeier curves for overall survival and efs are shown in gures 2 and 3 . 
in patients without previous surgery , median overall survival was 26 ( 99% ci 1942 ) years for those allocated to radiotherapy alone , 47 ( 2678 ) years for sim alone , 23 ( 1635 ) years for sub alone , and 27 ( 1647 ) years in those allocated to sim + sub ( log - rank p = 010 )  . 
 compared with radiotherapy alone , sim alone was associated with an improvement in efs ( hr 072 , 99% ci 053096 ; p = 0004 ) , although the e ect on overall survival was not signi cant ( 082 , 060111 ; p = 009 )  . 
 estimated 5 - year overall survival and efs in the sim - alone group were 50% ( 95% ci 3959 ) and 42% ( 3252 ; the corresponding rates in the radiotherapy alone group were 39% [ 3148 ] and 24% [ 1731 ] )  . 
 106 comparing four with two courses of chemotherapy ( ie , sim + sub vs either sim alone or sub alone ) did not show a survival advantage ( webappendix )  . 
adding sub to sim seemed to reduce the bene t of sim , producing a higher rate of death and events : compared with sim alone , overall survival ( hr 129 ; 99% ci 092181 ; p = 0049 ) and efs ( hr 127 , 092175 ; p = 006 )  . 
hr from an analysis of the main e ects associated with a 22 factorial trial ( ie , any sim vs no sim , and any sub vs no sub [ test for the interaction between sim and sub p = 012 ] , as well as sim alone vs sub alone , and survival hr vol 11 january 2010 articles radiotherapy alone sim alone sub alone sim + sub radiotherapy alone vs sim alone or sub alone ) , are shown in the webappendix . adding chemotherapy to radiotherapy was not e ective in patients who had undergone surgery previously . 
the median overall survival was 46 ( 99% ci 2276 ) and 50 ( 1880 ) years in those allocated to sim alone or radiotherapy alone , respectively ( hr 094 , 99% ci 064140 ; p = 070 )  . 
the median overall survival associated with sim alone was similar to the corresponding sim group without previous surgery ( 46 vs 47 years ) , but the median efs was higher ( 30 vs 22 years )  . estimated absolute risk di erences for overall survival , efs , and recurrence at 5 and 10 years after randomisation are shown in table 4 . 
compared with radiotherapy alone , for every 100 patients given sim alone , there could be 106 fewer patients who have a recurrence , new tumour , or die by 10 years after treatment ( 99% ci 11212 fewer ) ; equivalent to a number needed to treat of nine patients to avoid one event at 10 years . 
there could be 71 fewer deaths at 10 years ( 99% ci 184 fewer to 35 more ) among 100 patients treated with sim alone ( number needed to treat of 14 )  . 
no bene t was seen with sub alone or sim + sub , consistent with the other results . the percentages of patients who had a signi cant toxicity during treatment requiring hospitalisation in patients without previous surgery was 11% ( 25 / 233 ) in patients allocated to radiotherapy alone , 28% ( 47 / 166 ) in patients allocated to sim alone , 12% ( 19 / 160 ) in patients allocated to sub alone , and 36% ( 55 / 154 ) in patients allocated to sim + sub ( table 5 )  . 
although 28% of patients in the sim - alone group had an acute toxicity , compliance to chemotherapy was high ( 92% , 152 / 166 ; table 2 ) , probably because being in hospital would have provided them with the appropriate care to continue treatment . 
for patients who had undergone previous surgery , sim alone was associated with a doubling in the acute toxicity rate : 20% ( 24 / 118 ) sim alone versus 9% ( 12 / 135 ) radiotherapy alone . 
patients in the sim + sub group who during chemoradiation were less likely to complete their allocated chemotherapy regimen ( table 2 )  . experienced toxicity acute signi cant late toxicity occurring 6 months or more after randomisation was reported in 62 patients in total ; 44% ( n = 27 ) of rst noti cations occurring in months 6119 , and 24% ( n = 15 ) occurring in months 1224 . 
the rates were similar between the trial groups : 6% ( 13 / 233 ) among patients without surgery allocated to radiotherapy alone , 6% ( 10 / 166 ) for those allocated to sim alone , 4% ( 7 / 160 ) for those allocated to sub alone , and 6% ( 9 / 154 ) for those assigned to sim + sub ( table 5 ) ; and 7% p = 00005 number at risk radiotherapy alone sim alone sub alone sim + sub p = 085 number at risk radiotherapy alone sim alone time from randomisation ( years ) figure 3 : event - free survival ( efs ) according to treatment groups for patients who had no surgery ( a ) and those who had undergone surgery ( b ) before randomisation sim = radiotherapy with two courses of chemotherapy given simultaneously on days 1 and 14 of radiotherapy . 
 sub = radiotherapy with two courses of chemotherapy given 14 and 28 days after completing radiotherapy . treatment - related deaths , ( 10 / 135 ) and 11% ( 13 / 118 ) among patients who had undergone surgery allocated to radiotherapy alone or sim alone , respectively . there were 12 largely associated with dehydration , necrosis , mucositis , dysphagia , and renal failure . 
the rst six deaths were sent for independent review , after which clearer instructions were given to patients regarding adequate hydration and , in some centres , the avoidance of non - steroidal anti - in ammatory agents ( recognised to reduce glomerular ltration rate )  . 
negative risk di erences indicate that the event rate is lower than in the comparison group ( ie , more bene cial ) ; positive di erences indicate that the event rate is higher . 
 discussion the ukhan1 trial is one of the largest in head and neck cancer , and , to our knowledge , the only study to examine the timing of chemotherapy ( concurrent or maintenance ) in a factorial design . 
compared with radiotherapy alone , two courses of non - platinum chemotherapy given concurrently with radiotherapy ( sim alone ) in patients without previous surgery signi cantly extended efs by 12 years ( median efs 22 vs 10 years ; p = 0004 )  . 
the di erence in overall survival of 21 years ( median 47 vs 26 years , p = 009 ) was not statistically signi cant , probably because there were fewer overall survival events compared with efs in the analysis of sim alone versus radiotherapy alone ( 293 deaths vs 322 efs events ) and the e ect size was smaller ( hr of 082 vs 072 )  . 
the outcomes for sim alone were achieved with only one treatment - related death ( 06% ) , high compliance ( 92% ) , and acceptable toxicity rate ( 28% ) during treatment . 
among every 100 patients treated with sim alone , there were an estimated 106 fewer patients with a recurrence , new tumour , or death , 10 years later , compared with alone . 
concurrent chemoradiotherapy used in our study did not bene t patients who had undergone previous surgery , and the acute toxicity rate doubled . radiotherapy chemotherapy after radiotherapy was ine ective , which could be due in part to the higher proportion of patients who did not comply with treatment . 
reasons for non - compliance ( table 2 ) were largely because of toxicity , deaths , or withdrawals ( perhaps because some felt too unwell after radiotherapy to continue with therapy )  . 
 chemotherapy non - compliance was highest in the sim + sub group , and might also be due to patients not wanting to continue treatment after two courses of vol 11 january 2010 articles chemotherapy , possibly because they had completely responded after simultaneous chemoradiation , or were too unwell to continue . 
furthermore , this was a pragmatic trial , so we wanted centres to give their normal radiotherapy to encourage clinicians to participate , and therefore the doses used represented those given in routine practice at the time . 
all the radiotherapy regimens were radical doses , and there was no evidence that the radiotherapy regimen used a ected efs ( webappendix )  . there is variation in how patients with head and neck cancer are treated , with no established and agreed policy on chemoradiation , including for patients judged un t for platinum therapy . 
however , in the recent update , based on 9615 patients and including older data from ukhan1 , concomitant chemotherapy led to statistically signi cant reductions in deaths and recurrences , 7 with point estimates similar to those from ukhan1 : hr for overall survival 081 in mach - nc versus 082 ( 99% ci 060111 ) in ukhan1 , and hr for efs 079 in mach - nc versus 072 ( 99% ci 053096 ) in ukhan1 ( mach - nc used recurrence - free survival instead of efs )  . 
the review was based on adding chemotherapy to any loco - regional treatment ( ie , a mixture of surgery , no surgery , radiotherapy using standard or hyperfractionated regimens , or pre - operative radiotherapy )  . 
ukhan1 clearly separates patients according to whether they had surgery or not , showing that concurrent non - platinum chemotherapy used in the trial was more e ective than radiotherapy alone in the non - surgical group , but not in the group that had undergone previous surgery . 
 the mach - nc meta - analysis showed that concurrent chemoradiation should now be the routine treatment of choice for all patients with non - surgically treated advanced head and neck cancer . 
the ukhan1 study con rms this , but it also shows that a long - term bene t in terms of recurrence and deaths could be achieved with non - platinum agents that are inexpensive , relatively easy to deliver , and have lower toxicity than platinum therapies . 
 very few randomised head and neck cancer trials have reported such long - term e ects of chemo - radiotherapy , and we are not aware of any that have also investigated concurrent platinum treatment . 
 cisplatin used concurrently with radical radiotherapy has been shown to be better than radiotherapy alone : in an eortc trial ( 334 post - surgical patients with locally advanced disease ) , the risk of death was reduced by 30% ( p = 002 ) .12 efs was improved with cisplatin in a rtog trial ( 459 high - risk patients who had complete resection ) , with a decrease in risk ( hr 078 , 95% ci 061099 ; p = 004 ) .13 however , acute toxicity rates were much higher in those receiving chemotherapy ( 77% rtog and 41% eortc ) , compared with that in our own trial using vbmf or methotrexate ( 28% )  . 
although cisplatin - based regimens are often used in the us , the mach - nc meta - analysis did not nd a survival di erence according to type of chemotherapy ( p = 042 )  . 
in trials of poly - chemotherapy , the hr for death was 075 ( 95% ci 067084 ; using both uorouracil and platinum ) , 083 ( 074094 ; using either uorouracil or platinum ) , and 073 ( 052101 ; using chemotherapy other than uorouracil or platinum ) ; the ukhan1 estimate was 082 . newer agents such as taxanes and targeted therapies might improve on the longer - established doublet of cisplatin and uorouracil.1416 bonner and colleagues were the rst to show the value of cetuximab in advanced head and neck cancer , with a 30% reduction in the number of patients who progress or die ( in a trial of 424 patients ) .16 similar therapy combinations continue to be investigated . 
our 10 - year follow - up is reassuring for the regimens used in the ukhan1 study , and should encourage other trials to follow patients for many years . secondary hyperfractionated radiotherapy , involving an increase in the daily number of administered doses , is currently di cult for many uk oncology departments to deliver , so the simpler two courses of chemotherapy with only one fraction per day using standard regimens seems more feasible . 
as with improved outcomes at other sites such as the cervix , anus and lung , radical simultaneous chemoradiation therapy for scc of the head and neck is an e ective way of treating these life - threatening and disabling diseases . human papillomavirus ( hpv ) status was not obtained during the trial because it was not recognised as being a useful factor in head and neck cancer at the time the study was designed . 
however , data are beginning to emerge suggesting that patients with hpv - positive tumours have a better prognosis.17 although most evidence comes from observational studies , the e ects have been seen in retrospective analyses of randomised vol 11 january 2010 articles trials.18 , 19 we plan to examine hpv status and its possible e ect on outcome in the ukhan1 trial in the future . in summary , ukhan1 showed that patients with head and neck cancer who had undergone previous surgery did not bene t from the addition of chemotherapy to adjunctive post - operative radiotherapy . 
however , there was a clear bene t on recurrences and deaths associated with two courses of simultaneous non - platinum chemoradiotherapy in patients who had not undergone previous surgery , and this bene t persisted after a long follow up . 
non - platinum - based chemotherapy could be considered an alternative to platinum - based regimens , as well as an e ective therapy for patients who are judged to be un t for cisplatwith this particular group of patients , characteristically with multiple comorbidity and relatively low compliance to chemo therapy , the inability to tolerate platinum - based regimens is often a serious barrier to radical chemoradiation . 
moreover , the avoidance of local recurrence , with its potentially devastating consequences for the patients quality of life , is of particular importance in this group , many of whom su er from social deprivation and poor domestic support . 
improving efs reduces the number of patients who later need radical salvage surgery , which can be associated with long - term or permanent dis gurement , impaired function ( eg , ability to speak or eat easily ) , or social exclusion.20 because this is a high risk and generally un t patient group , many of whom are excessive users of alcohol and tobacco throughout treatment , the availability of a relatively simple , inexpensive and low toxicity chemoradiation regimen considerably improves the likelihood of completing treatment , essential for improving the chance of cure . contributors jt , km , ng , hmd , jg , and ih , designed and conducted the trial . 
 all authors were involved in writing the paper . con icts of interest the authors declared no con icts of interest . acknowledgments this comment was funded by cancer research uk , with support from university college london and university college london hospital comprehensive biomedical research centre . 
we are most grateful to all the patients and clinical teams at the hospitals in the uk and abroad , without whom this trial would not have been possible . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology procedure . 
however , recurrencesa rare problem within conventional criteria and a more frequent event outside are disastrous both for the patient who has received the transplant , and for the graft that has been removed from the donor pool ( or o ered by a family )  . 
 the most rational way to explore the vast territory beyond accepted criteria has to start with the analysis of available data in a detailed and strict manner ( ie , su cient sample size , plots to see where patients are distributed with respect to conventional limits , and follow - up )  . 
 we believe that our study , despite its limitations , meets these prerequisites . data on pathology are suboptimal for prediction , but , unlike radiology , are not subject to the changes that result from evolving imaging techniques . 
indeed the discrepancy between ndings from radiology and from pathology is diminishing , and should never involve maximum tumour size , but only the number of nodules , as our study has shown . the prediction of vascular invasion is still uncertain ; however , our study highlights this point as the main subject for further investigation and , while we wait for the identi cation of molecular markers , evidence is accumulating that information from concentrations of alpha - fetoprotein ( peak or gradient ) could help . as for the 444 patients within the milan criteria , they were included in the database ( which asked only for pathological information ) at the discretion of the participating centres , and were not overstaged by preoperative radiology , as outlined in our methods section . 
 outcome in these patients was excellent , con rming that neither the population nor the care they received were heterogeneous . we are unable to comment on the allegedly poor results of transplantation in the correspondents region , other than stating that experience in our centres does not match theirs , and that this should be no reason to accept equally poor results for patients transplanted for hcc . illusive interpretations are frequent in surgery when innovative procedures are perceived as the sole way to solve a bewildering problewhile our survival prediction chart and calculator are improvements from the current yes or no approach , we believe that a yes for most policy is counterproductive for patients and programmes alike , and unjusti able given the demand for grafts and for their responsible use . 
 vincenzo mazzaferro and pietro majno , for the metroticket investigator study group gastrointestinal surgery and liver transplantation , national cancer institute , via venezian 1 , milan 20133 , italy ( vm ) and hpitaux universitaires de genve , geneva , switzerland ( pm ) vincenzo.mazzaferro@istitutotumori.mi.it the authors declared no con icts of interest . erratum kenemans p , bundred nj , foidart j - m , et al , on behalf of the liberate study group . 
the corrected panels are shown below . g tamoxifen use at baseline ( n = 2068 ) h aromatase inhibitor use at baseline ( n = 202 ) 020 015 010 005 time since randomisation ( days ) 1095 1460 time since randomisation ( days ) 1095 1460 number at risk tibolone 25 mg placebo 1037 1031 99 vol 10 march 2009 re ection and reaction ms has received consultancy fees from glaxosmithkline , and payment for lectures from physicians educational resources . 
production of hyperpolarized [ 1 , 4 - 13c2 ] malate from [ 1 , 4 - 13c2 ] fumarate is a marker of cell necrosis and treatment response in tumors . 
isocitrate dehydrogenase - 1 mutations : a fundamentally new understanding of di use glioma ? lancet oncol 2010 ; published online july 7 , doi : 10.1016 / s1470 - 2045 ( 10 ) 70053 - xin table 1 , data cited for acute myelogenous leukaemia should read 1% not 0% of idh1 mutations . 
these corrections have been made to the online version as of october 4 , 2010 . isocitrate wild - type idh1 nadp + nadph + co2 + h + - ketoglutarate mutant - idh1 nadph + h + nadp + 2 - hydroxyglutarate wild - type 922 vol 11 october 2010 articles lancet oncol 2008 ; 9 : 114348 published online october 30 , 2008 doi : 10.1016 / s14702045 ( 08 ) 70259 - 6 see re ection and reaction page 1117 * see webappendix for atac trialists group cancer research uk , centre for epidemiology , mathematics , and statistics , wolfson institute of preventive medicine , queen mary school of medicine and dentistry , university of london , london , uk ( prof j cuzick phd , i sestak phd ) ; evanston northwestern healthcare , centre outcome research education , evanston hospital , evanston , usa ( d cella phd ) ; and cancer research uk , sussex psychosocial oncology group , brighton and sussex medical school , university of sussex , falmer , uk ( prof l fallow eld phd ) correspondence to : prof jack cuzick , cancer research uk , centre for epidemiology , mathematics and statistics , wolfson institute of preventive medicine , queen mary school of medicine and dentistry , university of london , london ec1m 6bq , uk jack.cuzick@cancer.org.uk treatment - emergent endocrine symptoms and the risk of breast cancer recurrence : a retrospective analysis of the atac trial jack cuzick , ivana sestak , david cella , lesley fallow eld , on behalf of the atac trialists group * summary background when the mechanism of action behind treatment toxicity re ects the intended e ect on the treatment target , the toxicity might be a useful marker for e cacy . 
 in this retrospective analysis , the relation between the reported incidence of vasomotor or joint symptoms and breast cancer recurrence in the arimidex , tamoxifen , alone or in combination ( atac ) trial is assessed . methods women with hormone - receptor - positive tumours who reported vasomotor or joint symptoms at the rst follow - up visit ( 3 months ) in the atac trial , ( which assessed tamoxifen or anastrozole for adjuvant treatment of postmenopausal breast cancer ) , were compared with women without these symptoms to see if there was a relation between these symptoms and subsequent recurrence . 
the atac trial is registered as an international standard randomised controlled trial , number isrctn18233230 . findings 1486 of 3964 ( 375% ) eligible women reported newly emergent vasomotor symptoms at the 3 - month followup visit and had lower subsequent recurrence than those who did not report these symptoms ( 223 during 10 752 women - years of follow - up vs 366 during 11 573 woman - years of follow - up , respectively ; hazard ratio [ hr ] 084 [ 95% ci 071100 ] , p = 004 ; adjusted for age , body - mass index , previous hormone - replacement therapy , nodal status , tumour size , and tumour grade )  . 
a greater decrease in breast - cancer recurrence was seen for the 1245 of 3964 ( 314% ) eligible women who reported new joint symptoms at the 3 - month follow - up visit compared with those not reporting these symptoms ( 158 during 9242 women - years of follow - up vs 366 during 11 573 women - years of followup ; adjusted hr 060 [ 050072 ] , p < 00001 )  . interpretation the appearance of new vasomotor symptoms or joint symptoms within the rst 3 months of treatment is a useful biomarker , suggesting a greater response to endocrine treatment compared with women without these symptoms . 
awareness of the relation between early treatment - emergent symptoms and bene cial response to therapy might be useful when reassuring patients who present with them , and might help to improve long - term treatment adherence when symptoms cannot be alleviated e ectively . funding cancer research uk and astrazeneca . introduction side - e ects often limit the dose of drugs that can be delivered , especially for cytotoxic chemotherapy where bone marrow , neurological , or gastrointestinal toxic e ects sometimes limit the achievable dose . 
for example , the occurrence of graft - versus - host disease in patients receiving allogeneic bone - marrow transplantation for haematological malignancies predicts overall survival.14 the occurrence of an acnei - form skin rash during the use of epidermal growth factor receptor ( egfr ) antibodies ( eg , cetuximab , panitumumab , or matuzumab ) , and also the kinase inhibitors , ge tinib and erlotinib , is another example where a side - e ect is associated with a higher probability of treatment response.5 , 6 side - e ects triggered by the therapeutic mechanism of action can be dose - independent . 
for example , in hormone therapy for breast cancer , neither inhibitors have a steep tamoxifen nor aromatase doseresponse curve for either side - e ects or e cacy.7 , 8 the appearance of vasomotor symptoms or joint symptoms is more likely to be related to the individual response to these drugs than to the dose . vasomotor symptoms ( eg , hot ushes , night sweats , and cold sweats ) are common side - e ects of endocrine treatment in women with early breast cancer.9 additionally , treatment with aromatase inhibitors increases the incidence of arthralgia and other joint symptoms.1012 for tamoxifen , there have been a few reports that women who developed vasomotor symptoms1316 had a lower risk of breast cancer recurrence than those who did not have these side - e ects , but no data on vasomotor symptoms exist for aromatase inhibitors . 
additionally , the incidence of joint symptoms is increased by all three vol 9 december 2008 1143 articles inhibitors third - generation aromatase ( anastrozole , letrozole , and exemestane ) , and is probably , at least partly , the result of the profound decrease in oestrogen concentrations.10 , 1719 however , to our knowledge , no associ ation between the development of joint symptoms and breast cancer recurrence has been reported . here , we investigate whether the early occurrence of endocrine symptoms ( speci cally vasomotor symptoms or joint symptoms ) is associated with treatment e cacy . 
 thus , the occurrence of certain symptoms could be the ultimate bioassay , which might be a re ection of the degree of biologically relevant oestrogen suppression produced in individual women by a speci c treatment . methods the arimidex , tamoxifen , alone or in combination ( atac ) study was a double - blind randomised clinical trial in which postmenopausal women with histologically con rmed localised breast cancer were randomly assigned to receive daily anastrozole ( 1 mg ) alone , tamoxifen ( 20 mg ) alone , or the combination in a double blind , method for 5 years as adjuvant treatment . 
details of trial design , methods , and primary objectives have been published elsewhere.9 after the initial analysis at 33 months of follow - up , 9 the combination group was stopped because no bene t compared with tamoxifen alone was seen , in terms of either e cacy or tolerability , and follow - up data were not subsequently collected . 
 therefore , our current analysis does not include these women and ndings will be presented only for the monotherapy groups , with focus on women who started their initial therapy , who had a hormone - receptorpositive tumour ( oestrogen - receptor positive or progesterone - receptor positive or both positive ) , and who did not report vasomotor symptoms or joint symptoms at entry . 
vasomotor symptoms were de ned as hot ushes , night sweats , or cold sweats and joint symptoms included reports of arthralgia , arthritis , arthrosis , or joint disorder . 
most symptoms occur soon after women start endocrine treatment , 20 , 21 so we used the recording of these symptoms ( all severities ) at the initial 3 - month follow - up visit as our measure of symptom occurrence . 
symptoms reported after 3 - months of initiation of the study therapy are not included in this analysis . regulatory and ethics authorities for all participating centres in 21 countries approved the protocol before enrolment of participants . 
 statistical analysis the rate of breast cancer recurrence was calculated by dividing the number of observed events by the number of woman - years of follow - up for each group . 
follow - up accrued until a breast cancer recurrence , death , or the cut - o date for this analysis ( march 31 , 2007 ) , which was the same as for the most recent 100 - month followup analysis.11 odds ratios ( or ) were used to compare factors a ecting the occurrence of vasomotor symptoms or joint symptoms at the 3 - month visit . 
for the post3 - month period , hazard ratios ( hr ) and corresponding 95% cis were estimated by the proportional hazards regression model , both with and without adjustment for age , body - mass index ( bmi ) , previous use of hormone replacement therapy ( hrt ) , nodal status , tumour size , and tumour grade.22 time - to - recurrence curves were formed by use of the kaplan - meier method.23 all p values are two - sided . 
 results overall , 590 of 6186 women ( 95% ) who started treat ment had vasomotor symptoms and 577 women ( 93% ) had joint symptoms at baseline ( table 1 )  . 
the size of these groups was small so subsequent recurrences were few ( four women with vasomotor symptoms and three women with joint symptoms ) , but were not signi cantly di erent from those in patients who did not report baseline symptoms ( vasomotor symptoms : hr 092 [ 95% ci 02959 ] , p = 07 ; joint symptoms : 068 [ 016286 ] , p = 06 )  . 
women with baseline symptoms tended to report fewer new endocrine symptoms during the trial than those without baseline symptoms ( data not shown )  . 1144 vol 9 december 2008 articles anastrozole tamoxifen all randomised women , n 3125 3116 exclusions , n ( % ) did not start randomised treatment 33 ( 11 ) 22 ( 07 ) joint symptoms only hormone - receptor negative or unknown status 502 ( 161 ) 512 ( 164 ) vasomotor symptoms only joint symptoms only at baseline 303 ( 97 ) 274 ( 88 ) vasomotor symptoms only at baseline 300 ( 96 ) 290 ( 93 ) both side - e ects at baseline 20 ( 06 ) 21 ( 07 ) study population * 1967 1997 * started allocated treatment , hormone - receptor positive , and no endocrine symptoms reported at trial entry . table 1 : exclusions from the randomised population by treatment group to obtain the study population women with hormone - receptor - negative tumours or with unknown hormone - receptor status and those with pre - existing vasomotor symptoms or joint symptoms at entry were excluded from the main analysis , leaving 1967 women in the anastrozole group ( 13 824 womanyears ) and 1997 in the tamoxifen group ( 13 637 womanyears ; table 1 )  . 
676 of 1967 women ( 344% ) in the anastrozole group reported vasomotor symptoms ( with or without joint symptoms ) compared with 810 of 1997 ( 401% ) in the tamoxifen group ( or 077 [ 95% ci 067087 ] , p = 00001 )  . 
in the anastrozole group , 665 of 1967 women ( 338% ) reported joint symptoms ( with or without vasomotor symptoms ) compared with 580 of 1997 ( 290% ) in the tamoxifen group ( or 125 [ 109143 ] , p = 0001 )  . 
more patients in the tamoxifen group reported vasomotor symptoms , whereas more patients in the anastrozole group reported joint symptoms , leading to a similar overall percentage of women reporting at least one of these symptoms ( 55% in both groups ; 1092 of 1967 in the tamoxifen group vs 1096 of 1997 in the anastrozole group )  . 
 after adjustment for age , bmi , previous hrt use , nodal status , tumour size , and tumour grade , women in the study population who reported vasomotor symptoms ( with or without joint symptoms ) at the 3 - month followup visit had fewer breast cancer recurrences than those who did not report these symptoms ( hr 084 [ 95% ci 071100 ] , p = 004 ; table 3 )  . 
those reporting only vasomotor symptoms , but not joint symptoms , had a similar decrease in recurrence rates to those reporting vasomotor stymptoms with or without joint symptoms ( not signi cant ; table 3 )  . 
 anastrozole no symptoms both symptoms tamoxifen no symptoms joint symptoms only vasomotor symptoms only both symptoms data are n ( % )  . patients 875 ( 445 ) 416 ( 211 ) 427 ( 217 ) 249 ( 127 ) 901 ( 451 ) 286 ( 143 ) 516 ( 258 ) 294 ( 147 ) table 2 : women with hormone - receptor - positive tumours and who did not report either symptom at trial entry with vasomotor symptoms or joint symptoms at the 3 - month follow - up visit according to treatment group the decrease in breast cancer recurrences for those reporting vasomotor or joint symptoms was equally clear for patients with local or distant recurrences . 
 there was no evidence of heterogeneity for vasomotor symptoms ( local recurrence : hr 080 [ 95% ci 057112 ] ; distant recurrence : 083 [ 068102 ] ; pheterogeneity = 05 ) or joint symptoms ( local recurrence : hr 064 recurrence : 060 [ 048074 ] ; pheterogeneity = 03 )  . 
for the e ect size for vasomotor symptoms ( with or without joint symptoms ) was larger in an unadjusted analysis ( hr 075 [ 95% ci 063091 ] , p = 0003 ) , and of the adjustment factors , only previous hrt use was a signi cant confounding those without previous hrt use , the e ect of vasomotor symptoms on subsequent recurrence was small ( hr 093 [ 077113 ] , p = 05 ) and similar in both treatment groups ( anastrozole group : hr 091 [ 068122 ] ; tamoxifen group : 093 [ 072120 ] )  . 
for those with previous hrt use , the e ect was substantially larger ( hr 063 [ 046085 ] , p = 0003 ) and apparent in both treatment groups ( anastrozole group : hr 053 [ 031088 ] ; tamoxifen [ 045096 ] )  . 
 signi cantly fewer women in the study population reporting joint symptoms ( with or without vasomotor symptoms ) at the 3 - month follow - up visit had a recurrence of breast cancer than those not reporting these symptoms ( hr 060 [ 95% ci 050072 ] , p < 00001 ; table 3 )  . 
figure 1 presents the recurrence proportion as a function of follow - up time according to treatment group and joint symptoms at the 3 - month follow - up visit . 
for women reporting both side - e ects at the 3 - month followup visit , a signi cantly greater decrease in breast cancer recurrence was noted compared with those not reporting any of these symptoms ( table 3 and gure 2 )  . 
 compared with women who reported neither symptom at the 3 - month follow - up visit , women who reported both side - e ects had an absolute decrease in recurrence of 114% ( 95% ci 99125 ) after 9 years of follow - up , those with joint symptoms only had a 10% ( 87108 ) absolute decrease , those who reported either side - e ect had a 8% ( 8280 ) absolute decrease , and those with vasomotor symptoms had only a 6% ( 6272 ) absolute risk decrease . discussion we present a retrospective analysis of the atac trial , assessing whether the occurrence of treatment - related symptoms ( vasomotor symptoms or joint symptoms ) is associated with breast cancer recurrence . 
a signi cantly larger e ect was noted for joint symptoms , which was similar in all subgroups , whereas the e ect of vasomotor symptoms was smaller and of borderline signi cance overall . 
the di erence in recurrence in patients with vasomotor symptoms ( with or without joint symptoms ) was substantially decreased after adjustment for age , bmi , previous hrt , nodal status , tumour size , and tumour grade and was most apparent in women who had taken hrt before trial entry . 
 analyses were restricted to patients with hormonereceptor - positive breast cancer , but similar ndings were obtained if analyses were based on all eligible randomised patients ( data not shown )  . 
 the analysis showed no signi cant di erence in recurrence in women who reported these symptoms at entry into the trial compared with those who did not report symptoms at entry . 
this nding adds weight to the interpretation of these data as re ecting a causal treatmentpatient interaction and not just a patients predisposition to these endocrine symptoms in the 1146 vol 9 december 2008 articles neither side - eect vasomotor symptoms only either side - eect joint symptoms only both side - eects 025 number at risk neither side - eect vasomotor symptoms only either side - eect joint symptoms only both side - eects 2017 912 1947 696 539 1583 880 1555 676 533 follow - up time ( years ) 1416 821 1449 629 509 1172 702 1262 561 444 796 471 855 385 324 215 165 figure 2 : breast cancer recurrence for anastrozole and tamoxifen treatments combined at di erent follow - up times according to endocrine symptoms reported at the 3 - month follow - up visit in women with hormonereceptor - positive tumours and without endocrine symptoms at entry di erences in drug metabolism or end - organ response , but this notion has yet to be fully elucidated . 
they showed that women with a wild - type genotype had a lower risk of disease relapse and a higher incidence of vasomotor symptoms than those without a wild - type genotype in the italian tamoxifen cyp2d6 . 
researchers from prevention trial assessed the frequency of the variants cyp2d6 ( * 4 / * 4 ) and noted that women who developed breast cancer on tamoxifen had a higher frequency in cyp2d6 * 4 / * 4 than those without breast cancer.24 additionally , pharmacological managing vasomotor symptomseg , the selective serotonin reuptake inhibitorsinhibit cyp2d6 and therefore decrease the e cacy of tamoxifen . 
in our study , a relation between vasomotor symptoms and breast cancer recurrence was seen , not only for tamoxifen , but also for the aromatase inhibitor anastrozole , suggesting that factors other than the cyp2d6 polymorphism are also involved . 
one possibility is the cyp19 gene ( aromatase ) itself , 25 but the full picture is likely to be more complicated and might involve other genetic loci . interventions used this analysis supports an inverse association between the occurrence of vasomotor symptoms and breast cancer recurrence previously reported for tamoxifen , 16 and extends this association to the aromatase inhibitor anastrozole and also to the presence of joint symptoms . 
 both of these symptoms are believed to be related to lowered oestrogen concentrations , although the speci c underlying cause of aromatase - inhibitor - induced joint symptoms is , as yet , unknown . 
additionally , patients who reported symptoms at baseline had fewer subsequent reports of these symptoms , but this might re ect a reporting bias in favour of new versus continuing symptoms . the e ect size was similar in both treatment groups , and an overall lower recurrence rate in patients assigned anastrozole compared with those assigned tamoxifen was apparent , regardless of whether symptoms were present or not . 
however , the size of the e ect of symptoms on recurrence was similar to , or larger than , the di erence the between anastrozole and importance of this nding . 
a detailed symptom questionnaire was not used , so it is possible that a larger e ect might have been observed if details were fully recorded . tamoxifen , supporting because the study only included women who began their allocated treatment , and endocrine symptoms were measured at the rst follow - up visit , reported adherence to treatment in the rst 3 - month period was high ( 3952 of 3964 [ 997% ] ) and is unlikely to a ect the reports of these symptoms . 
women reporting either symptom took 88% ( 1925 of 2188 ) of their prescribed treatment ( up to recurrence ) compared with 84% ( 1492 of 1776 ) in those with neither symptoit seems unlikely that these small di erences could explain the di erences in recurrences , but the reported di erences in adherence might re ect larger real di erences , which could confound our ndings . additionally , the appearance of symptoms would lead to the use of medicines that could also decrease recurrence as an additional e ect . 
details of aspirin and other non - steroidal anti - in ammatory drugs were not collected accurately , but use of cyclo - oxygenase - 2 inhibitors was collected accurately and only 12% ( 476 of 3964 ) of our study population used these drugs at any stage during the treatment . 
usage was higher in patients who reported vasomotor or joint symptoms than those who did not report these symptoms ( data not shown ) , but the hr for recurrence was unchanged if use of cox - 2 inhibitors was added to the model . 
for those with joint symptoms , the hazard ratio was only slightly changed ( hr 059 [ 95% ci 049072 ] ) if the use of either of these drugs was added to the model . the correlation of side - e ects with response to treatment has been noted in a few other situations , notably graft - versus - host disease for allogeneic bonemarrow transplantation and skin rash for antibodies directed at the egfr or tyrosine - kinase inhibitors . 
 however , this is the rst example to our knowledge where side - e ects of relatively non - toxic drugs with at doseresponse curves ( for both e cacy and side - e ects ) have been useful in predicting treatment response . 
this e ect is likely to be mediated by individual genetic vol 9 december 2008 1147 articles further work in understanding the genetic basis for individual response to treatment , these ndings also have important implications for communication between health - care professionals and patients with symptoms caused by endocrine therapy . 
several reports2628 have documented poor adherence to long - term endocrine therapy and an appreciation that endocrine symptoms indicate a stronger treatment e ect should help to encourage better symptomatic management and improve adherence for women receiving endocrine treatment . 
 these ndings also raise questions about the e ect that drugs aimed at ameliorating endocrine symptoms might have on the e cacy of endocrine treatments , if they target the same mechanism of action . contributors jc was responsible for the conception and design of the study , and assembly and analysis of the data . 
all contributors took part in writing the paper and approved the nal version . con icts of interest jc has received research funds from astrazeneca and acted as a consultant to astrazeneca and novartis . 
we also thank the trial investigators , other supporting sta , and the members of the international steering committee . re ection and reaction we did in fact invite all women to write these in the 5 - year quality of life booklet , as many patients had already been doing spontaneously at earlier time - points . 
few women recorded radiotherapy - related comments ; the majority commented on non - breast cancer issues , which the women felt might a ect their quality of life rather than the cancer and treatment itself ( unpublished data )  . 
comparison of patient - reported breast , arm , and shoulder symptoms and body image after radiotherapy for early breast cancer : 5 - year follow - up in the randomised standardisation of breast radiotherapy ( start ) trials . 
 br j radiol 2004 ; 77 : 13742 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology erratum oonk mh , van hemel bm , hollema h , et al . 
size of sentinel - node metastasis and chances of non - sentinel - node involvement and survival in early stage vulvar cancer : results from groinss - v , a multicentre observational study . 
lancet oncol 2010 ; 11 : 64652in this article ( published online first on march 26 , 2010 ) the rst line in the third box in gure 1a should have read 20 no lymphadenectomy . 
we aimed to establish agreement between these ssps for identi cation of breast cancer molecular subtypes . methods previously described microarray - based ssps were applied to one in - house ( n = 53 ) and three publicly available ( n = 779 ) breast cancer datasets . 
the proportion of cases classi ed as basal - like in each cohort was consistent irrespective of the ssp used ; however , the proportion of each remaining molecular subtype varied substantially . 
 however , di erent ssps produced broadly similar survival curves . interpretation although every ssp identi es molecular subtypes with similar survival , they do not reliably assign the same patients to the same molecular subtypes . 
for molecular subtype classi cation to be incorporated into routine clinical practice and treatment decision making , stringent standardisation of methodologies and de nitions for identi cation of breast cancer molecular subtypes is needed . funding breakthrough breast cancer , cancer research uk . introduction breast cancers are a diverse and heterogeneous group of diseases , and clinicopathological features and the status of oestrogen receptor and her2 guide treatment of patients . 
microarray - based gene expression pro ling has led to a paradigm shift in the way breast cancer is perceived , and has shown conclusively that breast cancer is not a single disease at the molecular level.16 the molecular heterogeneity of breast cancer and its implications are gradually being incorporated into clinical trial design , 7 and treatment strategies are being tailored to speci c subgroups of patients with breast cancer whose tumours have particular molecular aberrations ( eg , trastuzumab or lapatinib for women with her2 - positive disease )  . 
breast cancers can be classi ed by hierarchical cluster analysis , using an intrinsic gene list , into one of ve molecular subtypes : luminal a , luminal b , basal - like , her2 , and normal breast - like.15 , 8 however , this approach can only be applied retrospectively to su ciently sized cohorts of patients.8 an alternative strategy for classi cation of single samples into one of these molecular subtypes is the single sample predictor ( ssp ) , 35 which is based on similarities between a given case and molecular subtype centroids.3 , 4 breast cancer molecular subtypes identi ed by these approaches have been clinical presentations , 9 sites of relapse , 10 histological features , 11 responses to chemotherapy , 5 , 12 and outcomes.2 , 4 , 8 , 13 to have distinct suggested for consistent and clinically applicable molecular subtype assignment of breast cancers , a standardised methodology with reproducible results is fundamental.13 in the past 10 years , ve distinct intrinsic gene lists15 and three di erent ssps35 have been described to classify breast cancers into molecular subtype classes . 
molecular subtypes identi ed in separate studies with di erent ssps are assumed to be similar , if not identical , with respect to their clinical , biological , and prognostic characteristics ( ie , luminal a cancers in study a identi ed by the ssp - a are synonymous with luminal a cancers in study b identi ed by the ssp - b )  . 
nevertheless , some researchers have advocated that this molecular taxonomy should be used to design clinical studies6 , 14 and to guide decision - making regarding therapy.14 this assumption has not been the aims of this study were to assess the clinical usefulness of ssps by establishing agreement between di erent methods of breast cancer molecular subtype vol 11 april 2010 articles for the r code used see rock.icr.ac.uk / collaborations / mackay / for arrayexpress see see online for webappendix assignment ( ie , do di erent ssps assign the same patients to the same molecular subtype ? ) , and to ascertain whether each ssp identi es molecular subtypes with similar associations with outcome . 
to address these objectives , we analysed a cohort of consecutive invasive ductal carcinomas of no special type of histological grade iii , which were microdissected to minimise the e ect of varying amounts of stromal contamination , 15 and three cohorts of breast cancer samples the public domain.1618 methods sample collection we obtained 64 anonymised samples of consecutively accrued grade iii invasive ductal carcinomas of no special type from hospital la paz , madrid , spadetails of this cohort are described elsewhere.15 we de ned her2 status with us food and drug administration ( fda ) - approved methods for immuno histochemistry and dual - colour uorescence in - situ hybridisation ( fish ) as previously described , 19 and we scored status according to guidelines of the american society of clinical oncology and college of american pathologists ( webappendix pp 14 ) .20 we micro dissected representative frozen sections of tumours to ensure a consistent proportion of at least 90% tumour cells , and we extracted rna with trizol ( invitrogen , paisley , uk ) as previously described.15 53 cases produced su cient rna of optimum quality and underwent geneexpression pro ling with the illumina human wg6 version 2 array ( illumina inc , san diego , usa )  . 
the local research ethics committees approved this project . we analysed breast cancers from the publicly available nki - 295 ( n = 295 ) , 16 wang ( n = 286 ) , 17 and transbig ( n = 198 ) 18 datasets for molecular subtype classes and association with outcome . 
we obtained normalised microarray - based gene - expression data and clinical ndings from the ( nki - 295 , 22 wang internet or public repositories [ geo : gse2034 ] , transbig [ geo : gse7390 ] )  . 
details for the cohorts are provided in the webappendix ( p 5 )  . procedures methods related to mapping of centroid / ssp gene lists and breast cancer datasets and molecular subtype assignment are described in detail in the webappendix ( pp 14 )  . 
we have attempted to follow details for ssp analysis described in published work.35 to minimise the need to make assumptions , we tested several methods of gene and probe annotations and of handling of multiple probes for the same gene ( webappendix pp 14 )  . 
 table 1 : molecular subtype classi cations of breast cancers 340 vol 11 april 2010 articles for ensembl see ensembl.org previously published23 , 24 molecular subtype assignments of the nki - 295 dataset cancers with ssps described by sorlie and colleagues3 and hu and coworkers.4 in brief , annotations of centroid / ssp gene lists and breast cancer datasets were comprehensively updated and mapped to build 36 of the human genome ( ensembl assembly 54 ) ; annotation overlays were done with human genome organisation ( hugo ) gene symbols . 
to de ne whether a tumour pertained to the basal - like , her2 , luminal a , luminal b , or normal breastlike molecular subtype class , we correlated the gene expression of each tumour with 500 gene centroids by sorlie and colleagues3 ( sorlies ssp ) , 306 gene centroids by hu and coworkers4 ( hus ssp ) , and 50 gene centroids ( pam50 ) by parker and colleagues5 ( parkers ssp )  . 
we judged values of 001020 slight agreement , 021040 fair agreement , 041060 moderate agreement , 061080 substantial agreement , and 081099 almost - perfect agreement.26 survival curves were calculated by the kaplan - meier method and compared with the log - rank test . 
we applied a proportional - hazards model by coxs regression analysis to estimate hazard ratios and 95% ci for overall survival ( nki - 295 and transbig datasets ) and metastasis - free survival ( wang cohort , in addition to nki - 295 and transbig cohorts )  . 
in a multivariate analysis , tumour size was tted as continuous variable , tumour grade was tted as an ordinal variable , and oestrogen - receptor status and nodal status were tted as binary variables ( positive vs negative )  . 
in this case , we strati ed the cox model by dataset ; this process allowed baseline hazard functions to di er in each dataset but constrained the estimated hazard ratios to be the same across the datasets . 
it reduces the e ect of confounding on hazard ratio estimates caused by prognosis between di erent datasets but , similar to metainherent di erences 0740 ( 05660913 ) 0238 ( 01480328 ) sorlie ssp hu ssp basal luminal a luminal b normal her2 ( 95% ci ) basal luminal a luminal b normal her2 ( 95% ci ) 53 grade iii invasive ductal carcinomas 0274 ( 01730375 ) nki - 295 dataset hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 0532 ( 04620603 ) 0528 ( 04560601 ) 0656 ( 05920721 ) ( continues on next page ) vol 11 april 2010 articles ( continued from previous page ) wang dataset transbig dataset hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 hu ssp basal luminal a luminal b normal her2 parker ssp basal luminal a luminal b normal her2 sorlie ssp hu ssp basal luminal a luminal b normal her2 ( 95% ci ) basal luminal a luminal b normal her2 ( 95% ci ) 0439 ( 03550522 ) 0393 ( 03310455 ) 0459 ( 03940524 ) 0404 ( 03280480 ) 0488 ( 03880587 ) 0475 ( 03980553 ) ssp = single sample predictor . table 2 : agreement between single sample predictors for molecular subtype assignments analysis , it uses all co horts in one analysis , maximising the power to detect e ects . statistical analyses were done with r version 2.9.0 and spss version 11.5. 
 role of the funding source the sponsors had no role in study design , data collection , data analysis , data interpretation , writing of the report , or in the decision to submit for publication . 
bw , am , md , aa , and jsr - f took nal responsibility for the decision to submit the report for publication . results first , we sought to de ne the exact methods used previously to classify breast cancers according to three ssps . 
in the ssp analysis process , parameters and procedures were not described in su cient detail in the original publications.35 to minimise the need to make assumptions on methodology for assignment of molecular subtypes and to reduce inconsistencies in analysis methods , we aimed to reproduce the molecular the same gene subtype predictions of the nki - 295 dataset of breast cancers , which were previously classi ed into molecular subtypes by the sorlie or hu ssps ( webappendix pp 68 ) .23 , 24 agreement in molecular subtype assignment between the methods tested here and those previously published was 07150940 and depended on three factors : ( 1 ) use of di erent gene annotations for mapping of centroid / ssp gene lists and datasets ; ( 2 ) use of all probes identifying a gene versus averaging of multiple probes representing to establish correlations to a centroid / ssp gene list ; and ( 3 ) inclusion or exclusion of unclassi ed cases with a correlation less than 01 to any centroid.3 , 23 this cut - o was described by sorlie and colleagues3 as a conservative approach to include only cases with a strong correlation to a molecular subtype ( webappendix pp 14 , 9 )  . 
substantial agreement was noted ( 0646 [ 05650727 ] ) after exclusion of 109 unclassi ed cases with weak correlation ( < 01 ) to any centroids by sorlie and colleagues3 , 23 ( webappendix pp 68 )  . 
 we next ascertained molecular subtype classes ( table 1 ) and agreement between subtype assignments produced by the three distinct ssps in the four breast cancer cohorts ( table 2 , webappendix pp 1020 )  . 
we recorded only fair - to - moderate agreement between classi cations provided by sorlies and hus ssps ( 02740532 ; table 2 ) , moderate - to - substantial agreement between sorlies and parkers ssps ( 04390740 , table 2 ) , and fair - to - substantial agreement between hus and parkers ssps ( 02380656 ; table 2 , webappendix pp 1920 )  . 
 tables 1 and 2 show that in all four cohorts , the number of cases assigned to her2 , luminal a , luminal b , and normal breast - like molecular subtypes di ered remarkably , as did the number of unclassi ed cases with a correlation less than 01 to any centroid ( table 1 , gures 13 , webappendix pp 3137 )  . 
of the ve molecular subtypes , only the proportion of basal - like tumours was similar between the three distinct ssps tested . none of the microdissected grade iii invasive ductal carcinomas with a tumour - cell content of at least 90% nki - 295 dataset sorlie ssp 20033 patients er positive er negative grade 1 grade 2 grade 3 node positive node negative 2 cm > 2 cm basal - like her2 luminal a luminal b normal breast - like hu ssp 20064 parker ssp 20095 basal - like her2 luminal a luminal b normal breast - like patients at risk 29 p < 00001 sorlie ssp3 hu ssp4 parker ssp5 er status histological grade lymph - node status tumour size patients at risk 56 37 133 48 21 years patients at risk 25 years p < 00001 p < 00001 figure 1 : molecular subtype classi cation of nki - 295 breast cancers and overall survival of patients assigned to molecular substypes according to three single sample predictors er = oestrogen receptor . 
ssp = single sample predictor . vol 11 april 2010 articles sorlie ssp3 hu ssp4 parker ssp5 er status patients er positive er negative basal - like her2 luminal a luminal b normal breast - like patients at risk 53 basal - like 42 her2 171 luminal a 19 luminal b normal breast - like 1 wang dataset sorlie ssp 20033 hu ssp 20064 parker ssp 20095 p = 00372 patients at risk 49 104 124 0 patients at risk 54 15 65 139 13 years years p = 00017 p = 00133 figure 2 : molecular subtype classi cation of wang breast cancers and metastasis - free survival of patients assigned to molecular subtypes according to three single sample predictors er = oestrogen receptor . 
seven of 13 her2 - ampli ed grade iii invasive ductal carcinomasas indicated by immuno histochemistry and fishwere assigned to the molecular her2 subtype group with hus ssp , whereas the sorlie and parker ssps assigned all her2ampli ed cases to the luminal b subtype class ( webappendix p 10 )  . 
agreement between her2 , luminal a , and luminal b subtypes classi ed with sorlies , hus , or parkers ssps was generally only fair to moderate ( table 3 , webappendix p 21 )  . 
in the wang and transbig cohorts , concordance in assignment of tumours to luminal b class between sorlies and hus ssps , and between hus and parkers ssps , was only slight . 
almost - perfect concordance was noted only for classi cation of the basal - like subtype by all three ssps ( 08121000 ) , which was also recorded when unclassi ed cases were included in the analysis ( webappendix p 21 )  . 
our ndings show that , for assignment of her2 , luminal a , luminal b , and normal breast - like subtype classes , agreement between distinct ssps is only modest , but concordance for basal - like class is high . 
independent of the ssp used , molecular classi cation was associated signi cantly with overall survival survival ( webappendix p 31 ) in the nki - 295 dataset and with metastasis - free survival ( no information on overall survival is available publicly for this cohort ; gure 2 )  . 
these associations were also noted when unclassi ed cases ( ie , correlation < 01 to any centroid / ssp gene list ) were included in the analysis , with the exception of the assignment by sorlies ssp in the wang dataset ( webappendix pp 3234 )  . 
in the transbig data set , molecular subtypes were only associated signi cantly with overall survival ( gure 3 ) and metastasis - free survival ( webappendix pp 3537 ) when classi cations were made with hus ssp ; similar ndings were seen when un classi ed cases were included in the the wang dataset 344 vol 11 april 2010 articles transbig dataset sorlie ssp 20033 basal - like her2 luminal a luminal b normal breast - like patients er positive er negative grade 1 grade 2 grade 3 2 cm > 2 cm patients at risk 30 basal - like 11 her2 64 luminal a 90 luminal b 3 normal breast - like p = 00547 hu ssp 20064 parker ssp 20095 sorlie ssp3 hu ssp4 parker ssp5 er status histological grade tumour size patients at risk 40 30 119 0 years years p = 00067 p = 01118 figure 3 : molecular subtype classi cation of transbig breast cancers and overall survival of patients assigned to molecular subtypes according to three single sample predictors er = oestrogen receptor . 
importantly , the number and identity of cases assigned to molecular sub types in each cohort di ered by the ssp used , with the exception of basal - like subtype ( gures 13 , tables 1 and 2 )  . survival multivariate coxs hazard analysisincluding histological grade , tumour size , lymph node status , and oestrogen receptor statusshowed that , in the nki - 295 dataset , molecular subtypes only added independent prognostic information when assigned by the parker ssp for overall survival and by the hu and parker ssps for ( webappendix pp 2225 )  . 
 metastasis - free multivariate coxs hazard analysis of the transbig dataset ( lymph - node negative patients only ) , which included histological grade , tumour size , and oestrogen receptor status , indicated that molecular subtypes only added independent prognostic information when assigned by the hu ssp for overall survival and metastasis - free survival ( webappendix pp 2225 )  . 
for the wang dataset , no information on tumour size and histological grade was available publicly . to assess associations with outcome of each molecular subtype individually , circumventing the few samples assigned to each molecular subtype and maximising power to detect e ects , the nki - 295 , wang , and transbig cohorts were combined into one dataset ( table 4 )  . 
this analysis indicated that all ssps were prognostic for metastasis - free survival , and they were all prognostic for overall survival in the nki - 295 and transbig cohorts ( no overall survival data were available for the wang dataset )  . 
however , the signi cance of the association between luminal b and normal breast - like groups and metastasis - free survival was dependent on the ssp used for their assignment ( table 4 )  . discussion our ndings show that di erent ssps and methods used for molecular subtype assignment35 produce inconsistent results . 
the number of cases assigned to each molecular subtype di ered depending on the ssp used , and agreement for each class was modest ( ranging from fair to substantial ) , with the exception of the basal - like subtype . 
these results indicate that assignment of a given patient to a molecular subtype other than basal - like is strongly dependent on the ssp used and that results from studies of a speci c ssp cannot necessarily be generalised . 
this result could be accounted for in part by associations between molecular subtypes and clinico patho logical features linked to outcome ( webappendix pp 2629 ) and with expression levels of oestrogen receptor , her2 , and proliferationrelated genes ( webappendix pp 3861 )  . 
however , they suggest that the use of current ssps to allocate cases into her2 , luminal a , luminal b , and normal breast - like subtypes might be premature for strati cation of patients or in the context of clinical trials . the luminal b subtype was not identi ed reproducibly by di erent ssps . 
since distinction between luminal a and luminal b tumours seems to be driven by expression of proliferation - related genes , 4 , 14 the absence of consistency in allocation of these two subtypes should perhaps not come as a surprise . 
findings of several studies have shown that proliferation in oestrogen receptor - positive breast cancers is a continuum , 27 and allocation of speci c subgroups ( eg , luminal a and b ) might be arbitrary . one criticism levelled at molecular classi cation of breast cancer is that normal breast - like tumours could be an artifact derived from analysis of tumour specimens with a high proportion of normal tissue contamination.4 , 5 , 8 , 14 indeed , none of the microdissected breast cancer specimens with a tumour - cell content of at least 90% was assigned to the normal breast - like group ; however , the cases included in this study were all histological grade iii , and normal breast - like cancers were reported less frequently to be of grade iii in the nki - 295 series ( gure 1 , webappendix p 27 ) .11 despite several lines of evidence to suggest that the proportion of stromal cells has a substantial e ect on results of expression pro ling analysis and on gene classi ers , and that variable amounts of stromal cells in tumours introduce a confounding factor in interpretation of results of microarray analysis , 28 no previous study of molecular taxonomy of breast cancer has taken the degree of stromal contamination into account . 
 standardisation of tissue composition is needed if expression pro ling is to be used for breast cancer classi cation in clinical practice . several groups , including ours , have attempted to develop surrogate immunohistochemical markers for the molecular subtypes of breast cancer as de ned by microarrays ; 2931 however , results from these studies should be interpreted with caution , in view of the low stability of classes other than basal - like . 
in fact , validity of multiple surrogate markers for luminal b subtypes ( oestrogen receptor ( er ) - positive and / or progesterone receptor ( pr ) - positive , and her2 - positive ; 9 , 31 or er - positive and / or pr - positive and either her2positive and / or high ki67 expression ) 30 remains to be established . 
 table 4 : univariate and multivariate coxs regression analysis of overall and metastasis - free survival for the nki - 295 , wang , and transbig datasets combined metastasis - free survival overall basal - like her2 luminal b luminal a luminal b vs luminal a histological grade * oestrogen receptor status tumour size overall survival overall basal - like her2 luminal b luminal a luminal b vs luminal a histological grade * oestrogen receptor status tumour size between proposed immuno histochemical surrogates and microarray - de ned molecular subtypes.34 based subtyping should not be used to decide treatment for this group of patients . the pam50 method5 has provided an approach for breast cancer molecular classi cation , which is possibly clinically applicable ; however , reported agreement between the her2 pam50 - de ned subtype and her2 clinically positive cases ( as ascertained by immunohistochemistry and fish ) was only moderate.5 consistent with this observation , of cases classi ed as her2 - positive by fda - approved methods in our in - house dataset of grade iii invasive ductal carcinomas , just over half were assigned to the her2 molecular subtype by hus ssp , whereas all these cases were assigned to the luminal b subtype class by the other two ssps . 
these results show that the her2 group , as de ned by microarray gene pro ling analysis , does not equate with the clinical subgroup of her2 - positive breast cancers . 
since patients with her2 - positive cancers are eligible for targeted treatments ( ie , trastuzumab or lapatinib ) , extensive misassignment of these cases indicates that microarrayalthough microarray - based gene expression pro ling analysis has been reported as able to provide reasonably reproducible results for molecular classi cation of breast cancer , 3 , 4 our ndings show that without thorough standardisation , these tumours cannot be classi ed reliably by this approach . 
as emphasised by ioannidis and colleagues , 35 other investigators might only be able to predict molecular subtypes accurately when a detailed description of data processing and analytical methods is provided . 
 cancer molecular furthermore , careful standardisation of preanalytical variables that have a direct e ect on expression pro les , such as stromal component28 and tissue processing , 37 are equally crucial for development of reliable and reproducible classi ers . taxonomy vol 11 april 2010 articles limitations of our study include use of retrospectively accrued cohorts , the fact that three cohorts were retrieved from public repositories and some clinicopathological features were not available in one of the cohorts ( ie , tumour size and grade in the wang dataset ) , 17 and varied follow - up length in di erent datasets.1618 these limitations are also applicable to other studies of molecular taxonomy of breast cancer.13 for translation of current knowledge on the molecular features of breast cancer , the mechanisms of action of chemotherapy agents , and the availability of many compounds that target speci c molecular pathways or networks , molecular classi cations should have direct functional implications and be predictive of response to speci c therapeutic agents , rather than being descriptive and prognostic.8 , 38 , 39 this requirement is likely to need an integrative approach , combining descriptive data from su ciently powered cohorts40 and many sources , including clinicopathological features , massively parallel dna and rna sequencing , and proteomics , with detailed functional data from large panels of cancer models ( eg , high throughput rna interference and chemical screens ) .8 , 38 , 39 , 41 , 42 in conclusion , although ssps identify molecular subtypes with similar trends for association with outcome , they do not assign reliably the same patients to the same molecular subtypes . 
before molecular subtype classi cation can be incorporated into routine clinical practice and treatment decision making , standardisation of methodologies and stringent de nitions for identi cation of breast cancer molecular subtypes is needed . 
we also acknowledge nhs funding to the nihr biomedical research centre . re ection and reaction cancer patterns in inuit populations i wish to congratulate friborg and melbye1 on their informative review of cancer patterns in inuit populations , published in the september issue of the lancet oncology . 
as a clinician working with inuit in the nunavik region of northern quebec , i believe there are a few additional points worth mentioning . individuals first , there are a few small , but noteworthy , caseseries describing kaposis sarcoma in hiv seronegative inuit from greenland and nunavik . 
 although classic kaposis sarcoma is associated with human herpesvirus - 8 and is usually seen in elderly male patients of mediterranian or jewish descent , this disease has been described in eight immunocompetent inuit patients since 1974.2 a similar combination of genetic susceptibility and viral factors , as described by the authors with respect to nasopharyngeal carcinoma and epstein - barr virus in the inuit , might be responsible . second , with respect to the high incidence of cancers of the nasopharynx and lung , two signi cant exposures were not mentioned . 
although modern housing conditions have decreased exposure to fumes from lamps and open res for cooking , it is important to recognise that many groups of inuit still spend substantial amounts of time out on the land , cooking on open stoves inside their tents . 
additionally , the epidemic of marijuana smoking in 85% of adults ( according to 2004 nunavik public - health data ) 3 might play a part in the high incidence of lung and nasopharyngeal cancers . last , but not least , it is important to recognise that inuit face substantial challenges with respect to access to healthcare , and that these challenges represent part of a more far - reaching social inequality . 
 public - health statistics from the last 5 - year case period in nunavik suggest that both cancer incidence and mortality are higher overall for the subarctic inuit of the region than for age - matched southern patients.4 , 5 with life expectancy for canadian inuit more than 12 years less than the national average , 6 we must not forget that documents such as the universal declaration of human rights and the recommendations for worldwide cancer life expectancy for inuit is less than national average control mentioned in a comment by john se rin7 need to be applied for minority populations within developed countries as well as throughout the global community . barbara m young general internal medicine division , mcgill university , montreal , quebec , canada barbara.young@mcgill.ca the author declared no con icts of interest . friborg jt , melbye m . 
resumes_nunavik / anglais / alcoholdruguseandgamblingamongtheinuito fnunavik.pdf ( accessed nov 7 , 2008 )  . taux dincidence pour lensemble des sieges , excluant le cancer de la peau sans melanoma 2000 2004 . 
msss fichier des decs ( qubec ) , october 2005 ( electronic version )  . 6 wilkins r , uppal s , fins p , sencal s , guimond e , dion r . 
in this article , the header of the second column in table 2 should have read : time since diagnosis ( months )  . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology 1124 vol 9 december 2008 re ection and reaction panel : concepts applicable to various histologies ( excluding small - cell carcinoma , germ - cell tumors , and lymphoma ) in the analysis of brain metastasis trials involving radiosurgery and adjuvant wbrt patients eligible for radiosurgery have brain metastases less than 34 cm in diameter adjuvant wbrt probably decreases the risk of distant brain tumour recurrence for most histologies including melanoma adjuvant wbrt probably does not improve overall survival adjuvant wbrt is associated with a greater decline in learning and memory function at 4 to 6 months in a heterogenous population of primary cancer types wbrt causes acute fatigue and hair loss wbrt frequently delays the prompt initiation of systemic therapy a substantial proportion of patients with brain metastases do not need adjuvant wbrt in their lifetime a substantial proportion of patients with brain metastases initially treated with radiosurgery can be salvaged with additional radiosurgery delaying , or obviating the need for giving wbrt completely radiosurgery , like wbrt , can be used to address uncontrolled brain metastases in patients seeking to enroll on and qualify for clinical trials who would be otherwise excluded di culty inherent in accruing su cient numbers of patients to a site - speci c brain metastasis trial . 
however , there are common elements and fundamental concepts that seem to be valid across various histologies ( excluding small - cell carcinoma , germ - cell tumours , and lymphoma ) involving in the analysis of brain metastasis trials radiosurgery and adjuvant whole brain radiation therapy ( wbrt ; panel )  . 
perhaps in the future , the combination of advanced functional neuro - imaging and gene - expression pro ling techniques will enable us to identify better the subgroup of patients who are at greatest risk for developing distant brain metastases . 
the current preference and practice of medical oncologists in the department of melanoma medical oncology at md anderson cancer is to refer patients with oligo brain metastases to undergo radiosurgery alone to facilitate rapid enrolment on systemic therapy protocols . 
it is agreed that specialised brain metastasis trials focused exclusively on melanoma patients would help further elucidate the respective roles of surgery , radiosurgery , adjuvant wbrt , and systemic treatments . 
a phase 2 eastern cooperative oncology group ( e 6397 ) study of radiosurgery alone in patients with one to three brain metastases from renalcell carcinoma , melanoma , or sarcoma concluded that delaying wbrt might be appropriate for some subgroups of patients.2 in the meantime , the management of patients with melanoma brain metastases relies on the extrapolation of data gleaned from existing reports on brain metastasis , rst - hand knowledge of the patient history , and multidisciplinary discussion to provide the best treatment plan individualised for each patient . eric l chang * , patrick hwu department of radiation oncology ( elc ) , department of melanoma medical oncology ( ph ) , the university of texas md anderson cancer center houston , tx , usa echang@mdanderson.org the authors declared no con icts of interest . chang el , wefel js , hess kr , et al . 
phase ii trial of radiosurgery for one to three newly diagnosed brain metastases from renal cell carcinoma , melanoma , and sarcoma : an eastern cooperative oncology group study ( e 6397 )  . 
radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
lancet oncol 2010 ; 11 : 2128in gure 3 of this article ( published online first on nov 7 , 2009 ) , the data presented for unknown in the sex subgroup should have been in the egfr - positive cells subgroup . 
these corrections have been made to the printed article in this issue , and to the online version as of jan 6 , 2010 . rajkumar sv , jacobus s , callander ns , et al , for the eastern cooperative oncology group . 
lancet oncol 2010 ; 11 : 2937the webappendix of this article ( published online first on oct 22 , 2009 ) has been corrected as of jan 6 , 2010 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology vol 11 january 2010 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology euthanasia ( destroyed brain activity after application ) and palliative sedation ( continued brain activity after application )  . 
however , palliative is only acceptable for the combination of both intolerable and refractory ( untreatable ) symptoms.2 although it is understandable that patients struggle with existential questions in the face of death , it is problematic to consider this struggle as a refractory symptom for palliative sedation , as the authors correctly note . 
 such an application of palliative sedation occurs only in exceptional circumstances ( it is mostly applied for severe delirium and dyspnoea ) and , therefore , should not be the example by which the entire practice is considered controversial.3 we have proposed that palliative sedation is morally acceptable only when excruciating and untreatable symptoms severely threaten a patients ability to be the further agent of his or her life.4 this precondition acknowledges that it should be the progressive disease , not the palliative sedation , which inhibits the patients ability to shape their own life . 
therefore , total sedation will be at one end of the spectrum of palliative sedation , and used in a restricted group of patients , with intermittent and super cial sedation at the other end . 
in this perspective , palliative sedation is not controversial but a well de ned medical last resort for intractable ( and irresolvable ) multidimensional needs and problems in human beings who are su ering . 
clinical guidelines and an obligatory expert consultation in palliative care will educate and strengthen a reliable practice.5 jeroen hasselaar * , stans verhagen , rob reuzel , evert van leeuwen , kris vissers department of anesthesia , pain and palliative medicine ( jh , sv , kv ) , department of epidemiology , bio - statistics , and health technology assessment ( rr ) , and section ethics , philosophy , and history of medicine , department of iq health care ( evl ) radboud university medical center , nijmegen , the netherlands j.hasselaar@anes.umcn.nl the authors declared no con icts of interest . 1 materstvedt lj , bosshard g . 
in this article , the number 169 in the mild dyskaryosis box on the right - hand side of gure 3 should have been given as 196 . 748 vol 10 august 2009 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology procedure . 
however , recurrencesa rare problem within conventional criteria and a more frequent event outside are disastrous both for the patient who has received the transplant , and for the graft that has been removed from the donor pool ( or o ered by a family )  . 
 the most rational way to explore the vast territory beyond accepted criteria has to start with the analysis of available data in a detailed and strict manner ( ie , su cient sample size , plots to see where patients are distributed with respect to conventional limits , and follow - up )  . 
 we believe that our study , despite its limitations , meets these prerequisites . data on pathology are suboptimal for prediction , but , unlike radiology , are not subject to the changes that result from evolving imaging techniques . 
indeed the discrepancy between ndings from radiology and from pathology is diminishing , and should never involve maximum tumour size , but only the number of nodules , as our study has shown . the prediction of vascular invasion is still uncertain ; however , our study highlights this point as the main subject for further investigation and , while we wait for the identi cation of molecular markers , evidence is accumulating that information from concentrations of alpha - fetoprotein ( peak or gradient ) could help . as for the 444 patients within the milan criteria , they were included in the database ( which asked only for pathological information ) at the discretion of the participating centres , and were not overstaged by preoperative radiology , as outlined in our methods section . 
 outcome in these patients was excellent , con rming that neither the population nor the care they received were heterogeneous . we are unable to comment on the allegedly poor results of transplantation in the correspondents region , other than stating that experience in our centres does not match theirs , and that this should be no reason to accept equally poor results for patients transplanted for hcc . illusive interpretations are frequent in surgery when innovative procedures are perceived as the sole way to solve a bewildering problewhile our survival prediction chart and calculator are improvements from the current yes or no approach , we believe that a yes for most policy is counterproductive for patients and programmes alike , and unjusti able given the demand for grafts and for their responsible use . 
 vincenzo mazzaferro and pietro majno , for the metroticket investigator study group gastrointestinal surgery and liver transplantation , national cancer institute , via venezian 1 , milan 20133 , italy ( vm ) and hpitaux universitaires de genve , geneva , switzerland ( pm ) vincenzo.mazzaferro@istitutotumori.mi.it the authors declared no con icts of interest . erratum kenemans p , bundred nj , foidart j - m , et al , on behalf of the liberate study group . 
the corrected panels are shown below . g tamoxifen use at baseline ( n = 2068 ) h aromatase inhibitor use at baseline ( n = 202 ) 020 015 010 005 time since randomisation ( days ) 1095 1460 time since randomisation ( days ) 1095 1460 number at risk tibolone 25 mg placebo 1037 1031 99 vol 10 march 2009 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a manuscript to the lancet oncology visit thelancetoncology to submit a manuscript to the lancet neurology visit ees.elsevier.com / thelancetneurology 1 mosterd k , krekels gam , nieman fhm , et al . 
surgical excision versus mohs micrographic surgery for primary and recurrent basal - cell carcinoma of the face : a prospective randomised controlled trial with 5 - years follow - up . 
however , it is also explained by the fact that some patients were lost to follow - up after 30 months , and were therefore unable to visit our department at that time , but returned into follow - up when they visited our department after a longer period . 
there was no di erence in the method of follow - up between our rst and second publications . regarding the second question raised , we agree that perineural tumour invasion is an important risk factor . 
 finally , although the netherlands indeed an ethnically diverse country , the patients included in our study were people with fitzpatrick skin type i ( 11% ) , ii ( 44% ) , iii ( 35% ) , and iv ( 10% )  . 
 k mosterd * , n kelleners - smeets department of dermatology , maastricht university medical centre , po box 5800 , 6202 az , maastricht , netherlands k.mosterd@mumc.nl the authors declared no con icts of interest . neuro - oncology : a call for papers despite considerable research and the introduction of new therapies , long - term positive outcomes for patients with brain tumours are rare , and most patients experience a recurrence or progression of their cancer irrespective of the intervention . 
we are speci cally interested in the results of randomised controlled trials and other original clinical studies that will have a profound e ect on clinical practice , or on the fundamental understanding of tumour or cns biology , or on the management of neurological sequelae . accepted papers will be published in either the lancet oncology or the lancet neurology , and publication will coincide with the quadrennial meeting of the world federation of neuro - oncology and 6th meeting of the asian society for neuro - oncology ( wfno / asno ) , to be held in yokohama , japan , on may 1114 , 2009 . 
if your submission describes , in part or wholly , a study accepted for presentation at the wfno / asno meeting , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication can be scheduled to comply with wfno / asno embargo policies . 
 articles can be submitted via either the lancet oncologys or the lancet neurologys online submission services , but all authors must clearly state in the covering letter that their submission is in response to the tlo / tln call for papers . 
the closing date for this call for papers is march 13 , 2009 . david collingridge , helen frankish the lancet oncology ( dc ) , the lancet neurology ( hf ) , london nw1 7by , uk erratum kubota k , kawahara m , ogawara m , et al . 
vinorelbine plus gemcitabine followed by docetaxel versus carboplatin plus paclitaxel in patients with advanced non - small - cell lung cancer : a randomised , open - label , phase iii study . 
in this article , the hr for overall survival in table 2 should have read : 0996 ( 078127 )  . vol 10 january 2009 re ection and reaction we did in fact invite all women to write these in the 5 - year quality of life booklet , as many patients had already been doing spontaneously at earlier time - points . 
few women recorded radiotherapy - related comments ; the majority commented on non - breast cancer issues , which the women felt might a ect their quality of life rather than the cancer and treatment itself ( unpublished data )  . 
comparison of patient - reported breast , arm , and shoulder symptoms and body image after radiotherapy for early breast cancer : 5 - year follow - up in the randomised standardisation of breast radiotherapy ( start ) trials . 
 br j radiol 2004 ; 77 : 13742 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology erratum oonk mh , van hemel bm , hollema h , et al . 
size of sentinel - node metastasis and chances of non - sentinel - node involvement and survival in early stage vulvar cancer : results from groinss - v , a multicentre observational study . 
lancet oncol 2010 ; 11 : 64652in this article ( published online first on march 26 , 2010 ) the rst line in the third box in gure 1a should have read 20 no lymphadenectomy . 
this correction has been made to the online version as of june 28 , 2010 , and to the printed article . vol 11 july 2010 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper to the lancet go to thelancet / to submit a paper to the lancet oncology go to ees.elsevier.com / thelancetoncology / recommendations in light of the new data presented by raaijmakers and colleagues.3 piet dirix * , sandra nuyts department of radiation oncology , university hospitals leuven , leuven , belgium , piet.dirix@uzleuven.be the authors declared no con icts of interest . raaijmakers cp , roesink jm , dijkema t , houweling ac , terhaard ch . 
first results of a phase iii multicenter randomized controlled trial of intensity modulated ( imrt ) versus conventional radiotherapy ( rt ) in head and neck cancer ( parsport : isrctn48243537 ; cruk / 03 / 005 )  . 
proc am soc clin oncol 2009 ; 27 : abstr lba6006 . call for papersoncology and haematology the lancet and the lancet oncology are announcing plans for issues of each journal to be devoted to speci c topics in oncology and also to haematology . 
the former will be timed to coincide with the european society of medical oncology ( esmo ) congress in milan , italy ( oct 812 , 2010 ) , and the latter with the american society of hematology ( ash ) annual meeting in orlando , fl , usa ( dec 47 , 2010 )  . 
we would like to invite submissions of high - quality original research about cancers of the breast , lung , prostate , and gastrointestinal tract , or on any topic in haematology or haematological oncology . 
accepted papers will be published in either the lancet or the lancet oncology via fast - track peer review to coincide with either the esmo or ash annual meetings , as appropriate . 
 submissions to coincide with the esmo annual meeting must be received by june 25 , 2010 , and those for the ash annual meeting by oct 1 , 2010 , via either the lancet or the lancet oncologys online submission systems . 
please state in your covering letter that the submission is in response to this call for papers . if your work is being presented at either meeting and falls under an embargo policy , please tell us the date and time of the presentation , and whether the study is to be presented orally or in a poster . 
if your paper is accepted , online publication can be scheduled to coincide with the presentation and comply with any press embargo . jane godsland , zo mullan , richard turner , david collingridge the lancet ( jg , zm , and rt ) and the lancet oncology ( dc ) , 32 jamestown road , london nw1 7by , uk errata relling mv , altman rb , goetz mp , evans we . 
clinical implementation of pharmacogenomics : overcoming genetic exceptionalislancet oncol 2010 ; 11 : 50709the acknowledgment in this comment ( published online first on april 21 , 2010 ) should have read we thank colleagues in nihs pharmacogenomics research network . 
in the second paragraph , the last sentence was misspelt and should have read despite evidence linking pharmacogenomic variation with drug exposure , toxic e ects , and e cacy , many clinicians , regulators , and payors hold pharmacogenetic evidence to excessively high standards . 
lancet oncol 2010 ; 11 : 42938in this article , the acknowledgments statement should also have included : the uk medical research council funded the original all97 / 99 trial and supported the childhood leukaemia working party . 
lancet oncol 2007 ; 8 : 31722in this article , the equation for acpgbi in panel 2 should read loge [ r / ( 1r ) ] = ( 4859 + total score )  . 
the aim of this study was to assess the relative importance of di erent risk factors for treatment - emergent joint symptoms in patients assigned to anastrozole or tamoxifen as adjuvant treatment for postmenopausal breast cancer . methods the arimidex tamoxifen alone or in combination ( atac ) trial randomly assigned 9366 postmenopausal women to anastrozole ( 1 mg / day ) , to tamoxifen ( 20 mg / day ) , or to a combination of both . 
our analyses were based on data from case reports of 5433 women who were randomly assigned to anastrozole or tamoxifen , who started with their allocated treatment , and who did not have joint symptoms at entry ( anastrozole group : n = 2698 ; tamoxifen group : n = 2735 )  . 
joint symptoms were de ned as any report of arthralgia , arthrosis , arthritis , or joint disorder on a case - report forjoint disorders were de ned as reports of cervical spondylosis , osteoarthritis , and disc herniation . 
the atac trial is registered as an international standard randomised controlled trial , number isrctn18233230 . findings 777 of 1914 women ( 406% ) who used hormone replacement therapy ( hrt ) before trial entry developed joint symptoms compared with 1001 of 3519 women ( 284% ) without previous hrt use ( odds ratio [ or ] 172 [ 95% ci 153193 ] )  . 
women with hormone - receptor - negative breast cancer developed signi cantly fewer joint symptoms compared with those with hormone - receptor - positive tumours ( 124 of 461 [ 269% ] vs 1556 of 4548 [ 342% ] ; or 071 [ 057088 ] )  . 
women for whom chemotherapy was part of their initial treatment developed signi cantly more joint symptoms than those who did not receive it ( 461 of 1219 women [ 378% ] vs 1317 of 4214 women [ 313% ] ; or 134 [ 117153 ] )  . 
all signi cant risk factors from the univariate analysis were included in a multivariate analysis and remained signi cant with little change . interpretation in this trial , the major risk factors for developing joint symptoms were previous hrt , hormonereceptor positivity , previous chemotherapy , obesity , and treatment with anastrozole . 
discussion of identi ed risk factors is appropriate when counselling women before initiation of adjuvant hormonal treatment . funding this study was funded by cancer research uk and astrazeneca ( maccles eld , uk )  . introduction oestrogen de ciency has been associated with joint symptoms ( eg , arthralgia and arthritis ) in several di erent settings . 
in the general population , postmenopausal status and low oestrogen concentrations are associated with the development of joint pain and joint symptoms.1 , 2 these symptoms are most prominent around the ages of 50 to 59 years , 1 , 2 are more common in postmenopausal women than in premenopausal and perimenopausal women of the same age , 3 and often improve during use of hormone replacement therapy ( hrt ) .4 , 5 further evidence linking joint symptoms with decreased oestrogen concentrations comes from adjuvant trials of aromatase inhibitors in patients with early breast cancer , where increased joint symptoms ( eg , arthralgia and arthritis ) have been noted for all three thirdgeneration aromatase inhibitors.68 women treated with chemotherapy for breast cancer have also shown joint symptoms and other joint or muscle - related problems.9 , 10 however , tamoxifen does not seem to have an e ect on joint symptoms . 
in the rst international breast cancer intervention study , 11 joint symptoms were similarly distributed between treatment groups in postmenopausal women ( 159 of 3579 women in the tamoxifen group vs 147 of 3575 women in the placebo group ; p = 05 )  . 
 table 1 : patients with joint symptoms by severity and treatment rst received for all women ( safety population ) and for those without joint symptoms at entry ( study population ) symptoms in the arimidex tamoxifen alone or in combination ( atac ) trial , 13 and assess whether these risk factors act di erently in the presence of anastrozole treatment . 
 methods the atac trial13 was a double - blind randomised clinical trial in which postmenopausal women with early breast cancer were randomly assigned to oral daily anastrozole ( 1 mg ) alone , tamoxifen ( 20 mg ) alone , or a combination of both in a double - blind fashion , so that each woman took two tablets , at least one of which was active . 
 only women who started with their randomly assigned treatment and who did not report joint symptoms at entry were included in this analysis ( anastrozole group : n = 2698 ; tamoxifen group : n = 2735 )  . 
our analysis was based on the 100 - month median follow - up data set , at which point all patients had completed their study medication.14 because most symptoms occurred relatively early , and the e ects of treatment and other variables were not constant with time , the analysis was restricted to the occurrence of joint symptoms at any time during active treatment or within 14 days of its discontinuation . 
joint symptoms were de ned as any report of arthralgia , arthrosis , arthritis , or joint disorder ( coding symbols for a thesaurus of adverse reaction terms ) 15 on a case - report for joint disorders were de ned as reports of cervical spondylosis , anastrozole tamoxifen number at risk anastrozole tamoxifen 2698 2735 follow - up time ( years ) 2239 2372 1950 2085 1710 1859 1534 1656 1354 1464 figure 1 : patients ( % ) developing joint symptoms at or before a speci ed follow - up time during active treatment according to treatment rst received in women without joint symptoms at entry ( study population ) osteoarthritis , and disc herniation . 
for the atac trial , all side - e ect data were the result of elicited responses recorded on case - report forms and a speci c symptom check list was not used . 
interactions between treatment and subgroups were based on likelihood ratio tests for an added interaction terhazard plots were smoothed by use of an epanechnikov kernel with the optimum bandwidth chosen by cross validation.16 all p values are two - sided , with level of signi cance set at 005 , and all con dence intervals are at the 95% level . 
394 women in the anastrozole group and 359 women in the tamoxifen group ( or 090 [ 077105 ] ) reported a history of joint symptoms at entry into the trial . 
figure 1 shows the higher prevalence of joint symptoms reported by women without a history of joint symptoms at study entry in the anastrozole group compared with the tamoxifen group . 
in both treatment groups , most joint symptoms were of mild or moderate severity , and the intensity of symptoms was similarly distributed in both treatment groups ( table 1 )  . 
1067 of 1778 patients ( 60% ) who reported joint symptoms received treatment , with 960 of these patients ( 90% ) using a non - steroidal anti - in ammatory drug alone or in combination with a mild analgesic . potential risk factors for developing joint symptoms are shown for each treatment group in table 2 . 
after exclusion of women with baseline joint symptoms , 949 of 2698 women ( 352% ) reported joint symptoms in the anastrozole group compared with 829 of 2735 women ( 303% ) in the tamoxifen group ( or 125 [ 95% ci 111140 ; p < 00001 ] ; table 3 )  . 
for women who previously used hrt , 777 of 1914 ( 406% ) developed joint symptoms compared with 1001 of 3519 women ( 284% ) without previous hrt use ( or 172 [ 153193 ] ; p < 00001 )  . 
joint symptoms were increased by a similar amount for women who stopped hrt less than 6 months before trial entry compared with those who stopped hrt more than 6 months before entry ( 502 of 1201 women ( 418% ) vs 142 of 335 women ( 424% ) ; or 108 [ 084140 ] ; p = 054 )  . 
 women with hormone - receptor - negative breast cancer developed signi cantly fewer joint symptoms than those with hormone - receptor - positive tumours ( 124 of 461 ( 269% ) vs 1556 of 4548 ( 342% ) ; or 071 [ 057088 ] ; p = 0002 ; table 3 )  . 
 * north america = usa and canada . table 2 : selected baseline characteristics ( % ) according to treatment group ( study population ) role of the funding source this study was funded by cancer research uk and astrazeneca ( maccles eld , uk )  . 
 when all signi cant variables in the univariate models were entered into a multivariate model , the odds ratios were similar to the univariate ndings , except for smoking status , which became non - signi cant ( table 3 )  . 
 similar ndings for the univariate and multivariate analyses of risk factors were obtained if the population was restricted to hormone - receptor - positive women ( data not shown )  . 
additionally , there were no signi cant interactions of any factors with treatment , except for a weak interaction between treatment and previous hrt use ( pinteraction = 005 ; table 4 )  . 
 women from the usa and canada ( grouped as north america ) reported signi cantly more joint symptoms than those from the uk or the reference group of the rest of the world ( 738 of 1611 ( 458% ; or 244 [ 212280 ] ; p < 00001 ) vs 523 of 1815 ( 288% ; or 117 [ 101135 ] ; p = 003 ) vs 517 of 2007 ( 258% ) ; table 3 )  . 
data missing for 245 patients . table 4 : number ( % ) of women reporting joint symptoms at any time during treatment according to treatment rst received and selected risk factors in women without joint symptoms at entry ( study population ) no signi cant interactions of key variables in the univariate model were seen with region in the multivariate model ( data not shown )  . 
 discussion in this trial , the major risk factors for developing joint symptoms in women not reporting them at entry were previous hrt use , hormone - receptor positivity , previous chemotherapy , obesity , and treatment with anastrozole versus tamoxifen , leading to signi cant absolute increases of 121% , 73% , 65% , 62% , and 49% , respectively . 
women with pre - existing joint symptoms were excluded from this analysis to focus on new treatment - emergent symptoms . the e ect of previous hrt was especially striking , which could be because most women previously using hrt , for whom we had data , came o it within 6 months before entry into the study ( 1201 of 1536 women [ 782% ] ) , although the e ect was similar in women who had stopped their hrt treatment earlier . 
furthermore , the e ects of hrt seemed to be additive , resulting in an 181% increase in joint symptoms in women who previously used hrt and were on anastrozole compared with those on tamoxifen with no previous hrt use . 
 recent users of hrt ( ie , those who stopped use less than 6 months ago ) are likely to have a greater decrease in oestrogen concen trations with endocrine treatment than those who stopped use more than 6 months ago , and most , 17 , 18 but not all studies , 19 have shown that they are more likely than never users to have oestrogen - receptorpositive tumours . 
in our study , women with hormonereceptor - positive tumours reported more joint symptoms than those with hormone - receptor - negative tumours , but , paradoxically , the few women with tumours of unknown hormone - receptor status had the lowest number of joint symptoms . 
several studies have shown that women with high oestrogen concentrations are more likely to develop oestrogen - receptor - positive tumours than those with low oestrogen concentrations.20 , 21 obese women tend to have higher oestrogen concentrations than non - obese women as a result of aromatisation from the adipose tissue , 22 so the decrease in oestrogen concentration is likely to be greater in this group as well . 
obesity itself is also a risk factor for joint symptoms independent of endocrine treatment.23 however , crew and colleagues24 reported that women with a bmi between 25 and 30 kg / m developed fewer joint symptoms than those with a lower bmi . 
 chemotherapy is well known to induce arthralgia or myalgia and has been reported in several trials independently of endocrine treatment.10 , 2527 chemo therapy is known to damage ovarian function in premeno pausal women , and the e ects seen here could be a result of the ablation of any residual ovarian production of oestrogen in these postmenopausal women . 
again , the ndings were additive in anastrozole users so that the use of previous chemotherapy and anastrozole together resulted in a 124% increase in joint symptoms when compared with women on tamoxifen without previous chemo therapy . reports have suggested that side - e ects , such as joint symptoms , are under - reported in clinical trials compared with patient - recorded side - e ects.28 , 29 the atac trial was an international study , involving 21 countries . 
because of the nature of the collection , in which uniform de nition of symptoms was not provided , subcategories of joint symptoms were not thought to be reliable and were , therefore , not reported during the atac trial . 
additionally , the duration of symptoms and date of resolution of symptoms could not be assessed in detail , because data were collected at 3 months , 6 months , and at 6 - monthly intervals thereafter , so dates within these intervals were not recorded . 
because the study was blinded , there would have been no bias in relative rates , but the overall reporting rates for speci c symptoms could have been a ected . 
however , this approach did seem to be sensitive , because known minor side - e ects , and some previously unknown ones , were clearly detectable.30 the symptoms were assessed by clinicians and mapped to the relevant costart 870 vol 9 september 2008 articles terms.15 this ascertainment of joint symptoms needs to be taken into account when interpreting these ndings . 
 by contrast , a higher drop - out rate caused by joint symptoms was reported in two smaller uncontrolled studies , 31 , 32 but it is di cult to attribute all these events to an aromatase inhibitor , because joint symptoms are common in postmenopausal women ( eg , 31% of women receiving tamoxifen in the atac trial reported joint symptoms )  . the increased incidence of joint symptoms in the north american population is most probably consistent with di erent practices for recording symptoms . 
 although more patients had previous hrt use , previous chemotherapy , and a higher bmi in north america , compared with the uk and the rest of the world , the e ects of region were only slightly diminished when they were adjusted for in the multivariate model . 
 no signi cant interactions between region and risk factors were identi ed , suggesting that the di erences noted between regions were most probably due to di erent thresholds for reporting these symptoms in north america , especially because adverse events overall were more often reported in north american participants . in conclusion , several factors other than treatment with anastrozole were associated with the development of joint symptoms in this trial . 
joint symptoms were generally of mild to moderate intensity and for most women they do not override the clear bene ts of anastrozole over tamoxifen in terms of decreased recurrence and fewer other major side - e ects , including and gynaecological complications ( eg , endometrial cancer ) .14 however , for women with serious side - e ects on anastrozole , remains a viable option . 
 awareness of risk factors for joint symptoms will help both clinicians and patients to anticipate and manage these symptoms and ensure optimum adherence to endocrine treatment . thromboembolic tamoxifen venous events con icts of interest is declared no con icts of interest . 
all contributors took part in writing the paper and approved the nal version . acknowledgments this research was supported by cancer research uk and astrazeneca ( maccles eld , uk )  . 
extent of tumour hypoxia in localised prostate cancer is comparable to that in other cancers , but few data exist on the association of extent of tumour hypoxia with treatment outcome . 
we aimed to study the predictive value of intrinsic markers of tumour hypoxia and angiogenesis in localised prostate cancer , both in patients treated with radiotherapy and in those treated surgically . methods we applied a new , needle biopsy tissue microarray ( tma ) technique to study diagnostic samples from men with localised , previously untreated prostate cancer treated in two randomised controlled trials of radiotherapydose escalation . 
multivariate analysis by cox proportional hazards was done to assess the association between clinical outcome , in terms of biochemical control , and immunohistochemical staining of hypoxia inducible factor1 alpha ( hif - 1 alpha ) , vascular endothelial growth factor ( vegf ) , and osteopontin expression . 
the main outcome was time to biochemical ( ie , prostate - speci c antigen [ psa ] ) failure . findings between oct 12 , 1995 , and feb 5 , 2002 , 308 patients were identi ed from two prospective , randomised trials at the royal marsden hospital , london and sutton , uk , for the radiotherapy cohort and diagnostic biopsies were available for 201 of these patients . 
between june 6 , 1995 , and nov 4 , 2005 , 329 patients were identi ed from the aarhus university hospital , skejby , denmark , for the prostatectomy cohort ; of these , 40 patients were excluded because the tumour was too small to sample ( 19 patients ) , because the para n block was too thin ( 19 patients ) , or because the blocks were missing ( two patients ) , leaving 289 patients for analysis . 
for patients treated with radiotherapy , increased staining for vegf ( p = 0008 ) and hif - 1 alpha ( p = 002 ) expression , but not increased osteopontin expression ( p = 0978 ) , were signi cant predictors of a shorter time to biochemical failure on multivariate analysis , independent of clinical tumour stage , gleason score , serum psa concentration , and dose of radiotherapy . 
for patients treated with surgery , increased staining for vegf ( p < 00001 ) and hif - 1 alpha ( p < 00001 ) expression , and increased osteopontin expression ( p = 00005 ) were each signi cantly associated with a shorter time to biochemical failure on multivariate analysis , independent of pathological tumour stage , gleason score , serum psa concentration , and margin status . interpretation to our knowledge , this is the largest study of intrinsic markers of hypoxia and angiogenesis in relation to the outcome of radical treatment of localised prostate cancer . 
increased expression of vegf , hif - 1 alpha , and , for patients treated with surgery , osteopontin , identi es patients at high risk of biochemical failure who would be suitable for enrolment into trials of treatment intensi cation . 
 funding prostate cancer research foundation , london , uk ; danish cancer society , copenhagen , denmark ; cancer research uk , london , uk ; and national cancer research institute south of england prostate cancer collaborative , london , uk . introduction prostate cancer is the most commonly diagnosed cancer in men.1 established prognostic factors , such as tumour ( t ) stage according to the tumour , nodes , metastases ( tnm ) staging system , gleason score , and serum concentration of prostate - speci c antigen ( psa ) , are indicators of the natural history of disease2 , 3 and risk of recurrence after treatment.4 however , these factors explain only a moderate proportion of the variation in outcome , and there is an unmet need for better markers of prostate - cancer behaviour . 
markers are needed to identify high - risk patients , for whom standard radical treatment has poor outcomes and who would be suitable for clinical trials of more aggressive treatments . 
 identi cation of such markers of prostate cancer behaviour might provide insight into the molecular 342 vol 9 april 2008 articles mechanisms underpinning disease progression , and therefore inform the search for new therapeutic targets . 
 hypoxia in human tumours has long been linked to radioresistance.5 thomlinson and gray6 rst proposed the existence of hypoxia in human tumours more than 50 years ago and described the radioresistance of hypoxic mammalian cells . 
hypoxia has also been shown to be a potent stimulus for tumour progression , mediated via e ects on angiogenesis , genetic instability , glycolysis , inhibition of apoptosis , and upregulation of growth factors.7 , 8 in several cancers , including those of the head and neck , 9 , 10 cervix , 11 and soft - tissue sarcoma , 12 extent of tumour hypoxia is an important determinant of freedom from metastasis and overall survival . 
this nding is very well - established for patients treated with radiotherapy , but is less certain for those treated with surgery alone.13 the importance of hypoxia and angiogenesis in tumour biology has been underlined by the proven e ectiveness of treatments that exploit these abnormalities.14 , 15 a key e ect of hypoxia is the induction of gene expression mediated via hypoxia inducible factor 1 alpha ( hif - 1 alpha ) , a transcription factor that is stabilised under hypoxic conditions , and which induces a number of pathways important in tumour progression , such as angiogenesis , glycolysis , and proliferation.16 expression of hif - 1 alpha , assessed by immunohistochemistry , has been shown to predict radiotherapy outcome in several cancers.17 , 18 transcription of the angiogenic factor vascular endothelial growth factor ( vegf ) is directly controlled by hif - 1 alpha . 
tissue expression of vegf has been reported to predict treatment outcome in many cancers , including breast cancer , 19 osteosarcoma.21 osteopontin is a multifunctional secreted phosphoglycoprotein that is also induced by hypoxia , and has and been metastasis.22 while its transcriptional regulation is not fully understood , osteopontin is known to be regulated by factors other than hif - 1 alpha.23 in head and neck cancer , tumour expression of osteopontin , assessed by immuno histochemistry , correlates signi cantly with tumour oxygenation measured by polarographic electrodes , 24 and plasma osteopontin concentration is a predictor of radiotherapy outcome.10 tumour development cancer , 20 and implicated colorectal extent of tumour hypoxia in localised prostate cancer has been shown to be comparable to that in other cancers , 25 and hif - 1 alpha , 26 vegf , 27 and osteopontin28 are each overexpressed in prostate - cancer tissue in comparison with benign prostatic tissue . 
three small clinical studies , with a combined total of 147 patients , have suggested that tumour hypoxia measured by use of polarographic electrodes , 29 or immunohistochemical expression of vegf30 , 31 are tumour - osteopontin associated with treatment failure after radical treatment . 
 expression was increased signi cantly associated with decreased survival in a study of 70 patients with prostate cancer.28 these considerations provide a rationale for more de nitive studies to assess the role of tumour hypoxia and angiogenesis in terms of the outcome of radical treatment for patients with localised prostate cancer . 
 our speci c aims were to identify a high - risk group of patients who would be suitable candidates for clinical trials of more aggressive treatment , and to test whether markers of hypoxia and angiogenesis were predictive of outcome in patients treated with radiotherapy and in patients treated surgically . 
the second aim is pertinent to localised prostate cancer , because , if hypoxia is a determinant of radiotherapeutic outcome , but not surgical outcome , assessment of tumour oxygenation in individual patients could inform the choice between these two treatment modalities . 
 methods patients and procedures radiotherapy cohort between oct 12 , 1995 , and feb 5 , 2002 , 308 patients with clinically localised or locally advanced ( according to the tnm staging system : t13 , n0 or nx , m0 or mx ) , histologically proven , previously untreated prostate cancer were treated with radical radiotherapy in one of two prospective , randomised dose - escalation trials32 , 33 at the royal marsden hospital , london and sutton , uk . 
the randomised phase ii dose - escalation pilot study ( n = 127 ) and the randomised phase iii medical research council rt01 trial ( a trial of 843 patients of whom 181 patients were treated at the royal marsden academic urology unit , london and sutton , uk ) were of almost identical design , and have been described elsewhere.32 , 33 patients received 36 months of neoadjuvant androgen deprivation with subcutaneous goserelin 36 mg or leuprorelin 375 mg monthly , followed by radical radiotherapy to the prostate . 
 308 patients were eligible ; for those who gave written informed consent and who had diagnostic biopsies , biopsy tissue microarray ( tma ) was made by use of the checkerboard technique described by jhavar and colleagues.34 this technique reorientates cancer tissue from needle - biopsy than longitudinally , in para n blocks , thereby allowing many more sections to be taken for analysis . 
initial tissue vertically , rather vol 9 april 2008 articles figure 1 : scoring of immunohistochemical staining ( a ) hif - 1 alpha score 4 ( 40 )  . 
in the radical - prostatectomy group , two patients had missing pathological t stage and two patients had missing gleason scores . * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . 
 includes one t4 patient in the radiotherapy cohort . table 1 : characteristics of patients sections ( 4 m ) cut on to superfrost glass slides ( ultima , superfrost ultra slides [ lsl , rochdale , uk ] ) were stained by haematoxylin and eosin to identify the tissue samples ( ie , location and morphology of checkers ) within the microarray block . 
the tma included a total of 1164 tumour checkers , with a median of six checkers for each patient ( range 421 )  . radical prostatectomy cohort between june 6 , 1995 , and nov 4 , 2005 , 329 men with histologically proven , previously untreated , clinically localised prostate cancer were treated by radical prostatectomy ( rrp ) at the department of urology , aarhus university hospital , skejby , denmark . 
a conventional tma was constructed from tissue obtained at the time of surgery as described elsewhere.35 the most representative tumour areas were selected and marked on the haematoxylin and eosin - stained slides . 
by contrast to the tma for the radiotherapy cohort described above , for each patient only a single core ( diameter 06 mm ) was taken from the donor block with the tissue microarrayer ( beecher instruments , silver spring , md , usa )  . 
sections of 3 m were cut on a microtome and transferred to glass 344 vol 9 april 2008 articles hif - 1 alpha vegf osteopontin radiotherapy , n ( % ) radical prostatectomy , n ( % ) slides ( menzel - glser , superfrost plus , braunschweig , germany )  . 6 ( 3 ) 52 ( 26 ) 89 ( 44 ) 54 ( 27 ) 37 ( 18 ) 61 ( 30 ) 69 ( 34 ) 34 ( 17 ) 4 ( 2 ) 62 ( 31 ) 85 ( 42 ) 45 ( 22 ) 5 ( 3 ) 24 ( 8 ) 132 ( 46 ) 96 ( 34 ) 23 ( 8 ) 10 ( 4 ) 57 ( 21 ) 50 ( 18 ) 64 ( 23 ) 60 ( 22 ) 33 ( 12 ) 14 ( 5 ) 14 ( 5 ) 27 ( 10 ) 56 ( 20 ) 81 ( 28 ) 93 ( 33 ) 14 ( 5 ) immunohistochemistry the tmas were sectioned , and immunohistochemical staining done for hif - 1 alpha , vegf , and osteopont staining for hif - 1 alpha was done by use of the mouse monoclonal anti - hif - 1 alpha antibody , h1alpha67 ( novus biologicals , littleton , co , usa ) at a dilution of 1 : 1000 , according to the method described by koukourakis and coworkers.36 about 100 cancer cells were assessed for cytoplasmic hif - 1 - alpha expression , and scored as : 0 = no staining ; 1 = less than 1% of cells ; 2 = 110% of cells ; 3 = 1050% of cells ; and 4 = more than 50% of cells ( gure 1 ) .26 hif - 1 alpha was assessed in terms of cytoplasmic , rather than nuclear , staining , in accordance with the method published by zhong and colleagues , 26 who reported that cytoplasmic staining was a better predictor of outcome . 
staining for vegf was done by use of the rabbit anti - vegf polyclonal antibody ( a - 20 sc - 152 ; santa cruz biotechnology , santa cruz , ca , usa ) at a dilution of 1 in 400 , as described elsewhere.37 healthy tonsil tissue was used as a positive control . 
staining for osteopontin was done by use of the anti - osteopontin rabbit a nity isolated due to insu cient tissue on the radical prostatectomy tma section , vegf was not assessed in 11 patients , hif - 1 alpha was not assessed in four patients , and osteopontin was not assessed in four patients . 
 table 2 : distribution of molecular marker expression radiotherapy , n hazard ratio ( 95% ci ) p radical prostatectomy , n hazard ratio ( 95% ci ) p initial psa concentration , ng / ml 102 ( 101103 ) < 00001 101 ( 100101 ) 0023 initial psa concentration , ng / ml 1020 t stage * gleason score margin positive negative radiotherapy dose , gy hif - 1 alpha vegf osteopontin 217 ( 120394 ) 529 ( 292959 ) < 00001 001 117 ( 060228 ) 251 ( 124509 ) 065 001 136 ( 079237 ) 401 ( 196821 ) 0269 00001 173 ( 109 - 274 ) 002 179 ( 133243 ) 158 ( 124200 ) 149 ( 115194 ) 00001 00002 0003 144 ( 081255 ) 315 ( 180552 ) 0215 < 00001 257 ( 168394 ) < 00001 313 ( 182537 ) 334 ( 169662 ) < 00001 00005 266 ( 175404 ) < 00001 223 ( 184271 ) 175 ( 151204 ) 168 ( 137207 ) < 00001 < 00001 < 00001 * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . 
six patients had missing information on surgical - margin status . table 3 : univariate analysis of freedom from biochemical failure vol 9 april 2008 articles hif - 1 alpha vegf osteopontin score 02 score 3 score 4 score 02 score 3 score 4 score 5 score 02 score 3 score 4 score 5 hif - 1 alpha vegf osteopontin time from randomisation ( years ) score 0 score 3 score 1 score 4 score 2 time from randomisation ( years ) score 0 score 3 score 1 score 4 score 2 score 5 time from randomisation ( years ) score 0 score 3 score 1 score 4 score 2 score 5 figure 2 : freedom from biochemical failure ( % ) against time ( years ) with respect to expression of intrinsic markers of tumour hypoxia and angiogenesis * ( a ) radiotherapy cohort . 
 * marker categories pooled where fewer than ten patients in one category . monoclonal antibody ( sigma , gillingham , uk ) , at a dilution of 1 in 1000 , according to the method described by coppola.38 colon adenocarcinoma tissue was used as a positive control . 
 cytoplasmic staining for vegf and osteopontin in up to 100 , and not less than 20 , tumour cells was classi ed by use of a semiquantitative scoring method38 , 39 as : 0 = no staining ; 1 = less than 1% of cells ; 2 = 110% of cells ; 3 = 1133% of cells ; 4 = 3467% of cells ; and 5 = more than 67% of cells ( gure 1 )  . 
in patients who had intrapatient heterogeneity in scoring between di erent checkers , the worst score for each patient was used , based on the a - priori assumption that tumour behaviour would be more closely associated with the presence of highly hypoxic regions than with the average oxygenation . 
for all markers , experiments were repeated without the primary antibody as a negative control . scoring was done by a single expert prostate - cancer histopathologist ( cmc ) , blinded to patient outcome . 
all areas of benign glands , equivocal areas , prostatic intraepithelial neoplasia , or stromal tissue , were not scored . statistical analysis the main outcome measure was time to biochemical ( psa ) failure . 
in the radiotherapy cohort , biochemical failure was de ned by use of the houston criteria , 40 ie , an increase in serum psa concentration of at least 2 ng / ml greater than the nadir . 
these were gleason score ( < 7 , 7 , or > 7 ) , t stage ( t1 , t2 , or t3 ) , and initial the serum psa concentration radiotherapy cohort , clinical t stage was used , and the dose of radiotherapy ( 64 or 74 gy ) was also included in the xed baseline model . 
for 346 vol 9 april 2008 articles radiotherapy radical prostatectomy radiotherapy radical prostatectomy hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) hazard ratio ( 95% ci ) initial psa concentration 102 ( 101103 ) 0001 104 ( 102105 ) < 00001 initial psa concentration 117 ( 106129 ) 101 ( 099103 ) 0171 t stage * t stage * gleason score gleason score margin positive negative radiotherapy dose , gy 133 ( 068262 ) 219 ( 104460 ) 110 ( 062193 ) 215 ( 091505 ) 0406 0039 0750 0080 195 ( 121315 ) 0006 138 ( 077246 ) 0282 248 ( 143430 ) 186 ( 089386 ) 170 ( 097296 ) 0001 0097 0061 * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . table 4 : baseline multivariate analysis of freedom from biochemical failure 0002 0374 0041 0964 0328 0014 002 0008 0978 133 ( 078229 ) 0299 149 ( 084264 ) 136 ( 061303 ) 179 ( 106304 ) 0172 0459 0030 172 ( 135220 ) 145 ( 123172 ) 149 ( 119186 ) < 00001 < 00001 00005 margin positive negative radiotherapy dose , gy hif - 1 alpha vegf osteopontin 137 ( 069271 ) 220 ( 103467 ) 099 ( 054181 ) 155 ( 065370 ) 182 ( 113293 ) 146 ( 105204 ) 145 ( 110190 ) 100 ( 074136 ) the tissue - marker scores as discrete level factors rather than as continuous covariates . 
p values less than 005 were deemed statistically signi cant . * t stage is clinical for radiotherapy cohort and pathological for surgery cohort . table 5 : multivariate analysis of freedom from biochemical failure with expression of molecular markers included role of the funding source the prostate cancer research foundation , london , uk , contributed to funding of laboratory consumables . 
the sponsors had no role in study design , data collection , data analysis , data interpretation , writing of the report , or in the decision to submit for publication . 
cp had full access to all the data in the study and had nal responsibility for the decision to submit for publication . for results of the 308 patients who were identi ed for the radiotherapy cohort , 248 patients gave written informed their prostate biopsies and clinical consent information to be used in this study . 
for the 329 patients who were identi ed for the prostatectomy cohort , 40 patients were excluded because the tumour was too small to sample ( 19 patients ) , because the para n block was too thin ( 19 patients ) , or because the blocks were missing leaving 289 patients for analysis . 
expression of all three markers was signi cantly correlated with the other two : vegf and hif - 1 alpha , r = 022 , p = 0002 ; vegf and osteopontin , r = 032 , p < 00001 ; osteopontin and hif - 1 alpha , r = 031 , p < 00001 . 
 signi cant correlations were noted between higher hif - 1 alpha expression and higher initial serum psa concentration ( p = 0014 ) , and between higher vegf expression and higher gleason score ( p = 0043 )  . 
no signi cant correlation was noted between osteo pontin expression and any of the baseline clinical charac ter istics ( t stage , gleason score , and serum psa concentration )  . vol 9 april 2008 articles univariate analysis of the radiotherapy cohort baseline factors in relation to biochemical control is shown in table 3 . 
increased expression of hif - 1 alpha ( p = 00001 ) , vegf ( p = 00002 ) , and osteopontin ( p = 0003 ) were each signi cantly associated with decreased freedom from biochemical failure . 
 figure 2 shows freedom from biochemical failure in terms of each of the immunohistochemical markers . multivariate analysis of the baseline clinical characteristics of the radiotherapy cohort in relation to biochemical control showed that high initial serum psa concen tration ( p = 0001 ) , high t stage ( p = 0039 ) , and low radiotherapy dose ( p = 0006 ) were signi cant independent determin ants of decreased freedom from biochemical failure ( table 4 )  . 
addition of the molecular markers to this baseline model showed that increased vegf ( p = 0008 ) and hif - 1 alpha ( p = 002 ) expression , but not osteopontin expression ( p = 0978 ) , were each signi cant determinants of decreased freedom from biochemical failure , independent of clinical characteristics ( table 5 )  . 
 analysis of the marker scores as discrete level factors , rather than as continuous covariates , gave similar ndings ( data not shown )  . median follow - up of the radical prostatectomy cohort was 2 years ( range 07 ) , and 91 ( 32% ) of the 289 patients developed biochemical failure . 
expression of vegf and hif - 1 alpha were signi cantly correlated with each other ( r = 034 , p < 00001 ) , but not with osteopontin expression . 
higher expression of hif - 1 alpha was signi cantly correlated with higher pathological t stage ( p = 0001 ) and higher initial serum psa concentration ( p = 001 )  . 
a signi cant correlation with higher vegf expression was noted for higher pathological t stage ( p = 0009 ) and higher gleason score ( p = 0038 )  . 
figure 2 shows freedom from biochemical failure in terms of each of the molecular markers . ( p < 00001 ) , vegf ( p < 00001 ) were each multivariate analysis of the baseline clinical characteristics of the radical prostatectomy cohort in relation to biochemical control showed that initial serum psa concentration ( p < 00001 ) , and higher gleason score ( p = 0001 ) were signi cant independent determin ants of decreased freedom from biochemical failure ( table 4 )  . 
on multivariate analysis that incorporated the baseline clinical characteristics and increased expression of all three molecular markers , ( p < 00001 ) , and vegf ( p < 00001 ) , hif - 1 alpha osteopontin ( p = 00005 ) was signi cantly associated with decreased freedom from biochemical failure ( table 5 )  . 
analysis of the marker scores as discrete level factors , rather than as continuous covariates , gave similar ndings ( data not shown )  . discussion to our knowledge , this is the largest study of intrinsic markers of hypoxia and angiogenesis in relation to the outcome of radical treatment of localised prostate cancer . 
increased expression of hif - 1 alpha and vegf were each signi cant predictors of worse freedom from biochemical failure , independent of t stage , gleason score , initial psa concentration , and each other . 
additionally , increased osteopontin expression was a signi cant , independent determinant of worse treatment outcome for surgically treated those who underwent patients , but not radiotherapy . for for treated with advanced disease these ndings are consistent with the data available on the role of tumour hypoxia and angiogenesis in progression of prostate cancer . 
a polarographic electrode study29 of 57 patients with localised disease treated with brachytherapy showed a signi cant association between tumour oxygenation and time to biochemical recurrence ; however , that study had only nine failure events for analysis . 
the expression of vegf in prostate cancer is associated with the extent of tumour hypoxia , 39 and in a study of 50 patients with locally radical radiotherapy , green and co - workers30 reported a correlation between higher vegf expression and worse disease - speci c survival ( p = 0035 )  . 
furthermore , in a study31 that compared 17 patients who developed bone metastases after radical prostatectomy with 23 patients who remained disease - free , expression of vegf - a was signi cantly higher in those who developed bone metastases after radical prostatectomy . 
higher plasma concentrations of vegf have also been associated with biochemical progression after radical prostatectomy.41 the concentration of osteopontin in serum is associated with tumour hypoxia , 42 and , in a study of 90 patients with prostate cancer , increased serum osteopontin concentration was associated with higher gleason score , presence of bone metastases , and increased disease - speci c mortality.43 several studies , 44 , 45 although not all , 46 have shown an association between microvessel densitya measure of angiogenesisand outcome in patients with prostate cancer . 
first , there is a need for markers to identify high - risk patients , for whom standard radical treatment has poor outcomes , who 348 vol 9 april 2008 articles immuno histochemical would be suitable for clinical trials of more aggressive treatment . 
analysis of expression of hif - 1 alpha , vegf , and osteopontin in diagnostic biopsies by use of simple widely available techniques used in addition to the conventional risk factors of serum psa concentration , t stage , and gleason score , could identify such a high - risk group . 
further studies are warranted of mature cohorts managed by watchful waiting to assess whether hif - 1 alpha , vegf , and osteopontin could improve our ability to identify indolent prostate cancer . 
the association we recorded between treatment outcome and expression of hif - 1 alpha , vegf , and osteopontin , raises the possibility that these markers , or other components of the hypoxia angiogenesis axis , could represent valid therapeutic targets . 
androgen deprivation has been shown to decrease angiogenesis in prostate cancer in animals , 47 and improve tumour oxygenation in patients with prostate cancer , 48 making adjuvant hormone treatment a promising option for study in this group . 
 additionally , taken together with evidence of bene t from drugs that target hypoxia and proangiogenic proteins in other tumour types , 14 , 15 , 49 , 50 our ndings strengthen the rationale for trials of such drugs in patients with high - risk localised prostate cancer . 
by use of the technique described by jhavar and colleagues , we used tmas constructed from specimens from diagnostic needle biopsies , which enabled tma technology to be applied for the rst time , to our knowledge , to patients managed by radiotherapy . 
this study con rms the feasibility and use of this technique , which should now be applied to other candidate markers and to tissue samples from other prospective trials of prostate cancer radiotherapy . 
 the same technique could also be applied to patients managed by active surveillancefor whom diagnostic biopsies are typically the only tissue availableto identify markers that distinguish between patients that need radical treatment and those that could be safely monitored . 
the observation also lends support to the view that tumour hypoxia does not just cause radioresistance , but is also associated with an aggressive tumour phenotype.7 , 8 the study also has some limitations : rst , the duration of follow - up was relatively short , and there were insu cient clinical failure events for analysis . 
however , biochemical failure is a major concern to patients who have increased serum psa concentrations because it leads to the morbidity associated with salvage treatment , and patients with biochemical failure are at signi cant risk of death from prostate cancer ; 52 second , although , to our knowledge , this is the largest study of its kind , the 201 patients who had radiotherapy might not have been representative of the 308 patients from which they were taken , and analysis of the radiotherapy cohort was not adequately powered to detect any interaction between marker expression and radiotherapy dose with respect to treatment outcome . 
further studies will be needed to address this important issue and to assess the predictive role of expression of hif - 1 alpha , vegf , and osteopontin in patients treated with radiotherapy alone without neoadjuvant androgen deprivation . 
fourth , we noted a signi cant di erence in the distribution of marker expression between the radiotherapy and the surgical cohorts , for which the explanation is uncerta undoubtedly , the single core per patient on the tma from the surgical cohort , by contrast with a median of six checkers per patient on the tma from the radiotherapy cohort , would have contributed to this observation . 
last , the associations noted between clinical outcome and staining for hif - 1 alpha , vegf , and osteopontin are not su cient to conclude that expression , improves vol 9 april 2008 articles tumour hypoxia and angiogenesis adversely a ect treatment e cacy , and that these markers constitute therapeutic targets . 
staining for hif - 1 alpha , vegf , and osteopontin might only serve as a marker for an aggressive tumour phenotype . con icts of interest the authors declared no con icts of interest . 
rv , cmc , arn , mb , ah , rh , re , vk , ms , cc , dd , cp took part in writing the report . acknowledgments this work was undertaken in the royal marsden nhs foundation trust , london and sutton , uk , who received a proportion of its funding from the uk national health service executive ; the views expressed in this publication are those of the authors and not necessarily those of the uk national health service executive . 
this work was supported by the institute of cancer research , the cancer research uk section of radiotherapy ( cruk ) grant number c46 / a2131 , the ncri south of england prostate cancer collaborative and the prostate cancer research foundation . 
cp was funded by cruk and by the national cancer research institute south of england prostate cancer collaborative . re ection and reaction is supportive never - smokers , and women.7 there evidence that patients with egfr - mutant tumours are biologically more indolent ( lim wt , national cancer centre , singapore , personal communication )  . i propose re ning the bipartite model by adding a clinical and biological dimension to it . 
the group of patients with slow - growing tumours are clinically characterised by never - smokers or former smokers who have had little active exposure , are women , and have egfr - activating mutations . 
to improve lung - cancer outcome , we have to adopt a two - pronged approach : identify the population at risk of slow - growing tumours and target them for screening trials , while using coordinated antitobacco e orts to prevent aggressive tumours in others . 
j natl cancer inst 2005 ; 97 : 33946 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata jones lw , eves nd , haykowsky m , joy aa , douglas ps . 
the correct gure is shown . number at risk months vol 9 october 2008 re ection and reaction panel : concepts applicable to various histologies ( excluding small - cell carcinoma , germ - cell tumors , and lymphoma ) in the analysis of brain metastasis trials involving radiosurgery and adjuvant wbrt patients eligible for radiosurgery have brain metastases less than 34 cm in diameter adjuvant wbrt probably decreases the risk of distant brain tumour recurrence for most histologies including melanoma adjuvant wbrt probably does not improve overall survival adjuvant wbrt is associated with a greater decline in learning and memory function at 4 to 6 months in a heterogenous population of primary cancer types wbrt causes acute fatigue and hair loss wbrt frequently delays the prompt initiation of systemic therapy a substantial proportion of patients with brain metastases do not need adjuvant wbrt in their lifetime a substantial proportion of patients with brain metastases initially treated with radiosurgery can be salvaged with additional radiosurgery delaying , or obviating the need for giving wbrt completely radiosurgery , like wbrt , can be used to address uncontrolled brain metastases in patients seeking to enroll on and qualify for clinical trials who would be otherwise excluded di culty inherent in accruing su cient numbers of patients to a site - speci c brain metastasis trial . 
however , there are common elements and fundamental concepts that seem to be valid across various histologies ( excluding small - cell carcinoma , germ - cell tumours , and lymphoma ) involving in the analysis of brain metastasis trials radiosurgery and adjuvant whole brain radiation therapy ( wbrt ; panel )  . 
perhaps in the future , the combination of advanced functional neuro - imaging and gene - expression pro ling techniques will enable us to identify better the subgroup of patients who are at greatest risk for developing distant brain metastases . 
the current preference and practice of medical oncologists in the department of melanoma medical oncology at md anderson cancer is to refer patients with oligo brain metastases to undergo radiosurgery alone to facilitate rapid enrolment on systemic therapy protocols . 
it is agreed that specialised brain metastasis trials focused exclusively on melanoma patients would help further elucidate the respective roles of surgery , radiosurgery , adjuvant wbrt , and systemic treatments . 
a phase 2 eastern cooperative oncology group ( e 6397 ) study of radiosurgery alone in patients with one to three brain metastases from renalcell carcinoma , melanoma , or sarcoma concluded that delaying wbrt might be appropriate for some subgroups of patients.2 in the meantime , the management of patients with melanoma brain metastases relies on the extrapolation of data gleaned from existing reports on brain metastasis , rst - hand knowledge of the patient history , and multidisciplinary discussion to provide the best treatment plan individualised for each patient . eric l chang * , patrick hwu department of radiation oncology ( elc ) , department of melanoma medical oncology ( ph ) , the university of texas md anderson cancer center houston , tx , usa echang@mdanderson.org the authors declared no con icts of interest . chang el , wefel js , hess kr , et al . 
phase ii trial of radiosurgery for one to three newly diagnosed brain metastases from renal cell carcinoma , melanoma , and sarcoma : an eastern cooperative oncology group study ( e 6397 )  . 
radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
lancet oncol 2010 ; 11 : 2128in gure 3 of this article ( published online first on nov 7 , 2009 ) , the data presented for unknown in the sex subgroup should have been in the egfr - positive cells subgroup . 
these corrections have been made to the printed article in this issue , and to the online version as of jan 6 , 2010 . rajkumar sv , jacobus s , callander ns , et al , for the eastern cooperative oncology group . 
lancet oncol 2010 ; 11 : 2937the webappendix of this article ( published online first on oct 22 , 2009 ) has been corrected as of jan 6 , 2010 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology vol 11 january 2010 re ection and reaction chargari c , toillon ra , macdermed d , castadot p , magn n . 
concurrent hormone and radiation therapy in patients with breast cancer : what is the rationale ? lancet oncol 2009 ; 10 : 5360 . toledano a , azria d , garaud p , et al . 
in table 1 , a ten - fold discrepancy in tumour size was caused by a conversion error of the cyst size from cm to mfurthermore , the patients with squamous - cell carcinoma in situ should have been excluded ( peuchmaur et al , 1989 ; tobon et al , 1991 ; dadhwal et al , 2002 ) : these publications provided only limited data and exclusion does not change results signi cantly . 
data are mean ( sd , range ) or number ( % )  . table 1 : preoperative data for patients with mature cystic teratoma 446 vol 10 may 2009 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper to the lancet go to thelancet / to submit a paper to the lancet oncology go to ees.elsevier.com / thelancetoncology / recommendations in light of the new data presented by raaijmakers and colleagues.3 piet dirix * , sandra nuyts department of radiation oncology , university hospitals leuven , leuven , belgium , piet.dirix@uzleuven.be the authors declared no con icts of interest . raaijmakers cp , roesink jm , dijkema t , houweling ac , terhaard ch . 
first results of a phase iii multicenter randomized controlled trial of intensity modulated ( imrt ) versus conventional radiotherapy ( rt ) in head and neck cancer ( parsport : isrctn48243537 ; cruk / 03 / 005 )  . 
proc am soc clin oncol 2009 ; 27 : abstr lba6006 . call for papersoncology and haematology the lancet and the lancet oncology are announcing plans for issues of each journal to be devoted to speci c topics in oncology and also to haematology . 
the former will be timed to coincide with the european society of medical oncology ( esmo ) congress in milan , italy ( oct 812 , 2010 ) , and the latter with the american society of hematology ( ash ) annual meeting in orlando , fl , usa ( dec 47 , 2010 )  . 
we would like to invite submissions of high - quality original research about cancers of the breast , lung , prostate , and gastrointestinal tract , or on any topic in haematology or haematological oncology . 
accepted papers will be published in either the lancet or the lancet oncology via fast - track peer review to coincide with either the esmo or ash annual meetings , as appropriate . 
 submissions to coincide with the esmo annual meeting must be received by june 25 , 2010 , and those for the ash annual meeting by oct 1 , 2010 , via either the lancet or the lancet oncologys online submission systems . 
please state in your covering letter that the submission is in response to this call for papers . if your work is being presented at either meeting and falls under an embargo policy , please tell us the date and time of the presentation , and whether the study is to be presented orally or in a poster . 
if your paper is accepted , online publication can be scheduled to coincide with the presentation and comply with any press embargo . jane godsland , zo mullan , richard turner , david collingridge the lancet ( jg , zm , and rt ) and the lancet oncology ( dc ) , 32 jamestown road , london nw1 7by , uk errata relling mv , altman rb , goetz mp , evans we . 
clinical implementation of pharmacogenomics : overcoming genetic exceptionalislancet oncol 2010 ; 11 : 50709the acknowledgment in this comment ( published online first on april 21 , 2010 ) should have read we thank colleagues in nihs pharmacogenomics research network . 
in the second paragraph , the last sentence was misspelt and should have read despite evidence linking pharmacogenomic variation with drug exposure , toxic e ects , and e cacy , many clinicians , regulators , and payors hold pharmacogenetic evidence to excessively high standards . 
lancet oncol 2010 ; 11 : 42938in this article , the acknowledgments statement should also have included : the uk medical research council funded the original all97 / 99 trial and supported the childhood leukaemia working party . 
lancet oncol 2007 ; 8 : 31722in this article , the equation for acpgbi in panel 2 should read loge [ r / ( 1r ) ] = ( 4859 + total score )  . 
additionally , in table 3 , 158 was added in error next to the heading clinicopathological staging . 516 vol 11 june 2010 re ection and reaction with endemic burkitts lymphoma in africa from poor families , and will gladly share more detailed information with interested colleagues . 
the socit franaise doncologie pdiatrique lmb89 protocol : highly e ective multiagent chemotherapy tailored to the tumor burden and initial response in 561 unselected children with b - cell lymphomas and l3 leukemia . 
follow - up is done by dedicated health - care workers who actively seek out patients in their villages . colleagues in kenya and uganda did not accept the invitation to join in the rst study supported by siop , 3 perhaps because the proposed treatment schedule might have been perceived at the time as being worse than established treatment schedules , such as cyclophosphamide , doxorubicin , vincristine , and pred nisolone . 
 however , the french - african pediatric oncology group has now used the same schedule of cyclophosphamide and intrathecal methotrexate in several sub - saharan francophone countries , with comparable e cacy ( jean lemerle , socit franaise doncologie pdiatrique , personal communication ) .6 patients with primary resistance to this treatment , or who relapsed after treatment , have been treated with a 15 - day schedule of cyclophosphamide ( 60 mg / kg ) , vincristine ( 15 mg / m2 ) , and standard - dose intrathecal methotrexate on days 1 , 8 , and 15.7 a third of these patients remain in continuous remission after more than a years follow - up and are considered cured.7 thus , this approach has lead to an overall 1 - year survival of 67% for the group of patients enrolled in these rst - line and refractory studies.4 , 5 , 7 we believe that we have established an e ective , welltolerated , and a ordable treatment option for patients erratum veldeman l , madani i , hulstaert f , de meerleer m , mareel m , de neve w . 
the corrected webtables have been republished online . see online for webtables vol 9 june 2008 articles lancet oncol 2010 ; 11 : 45058 published online april 14 , 2010 doi : 10.1016 / s14702045 ( 10 ) 70038 - 3 see re ection and reaction page 406 kings college london , school of medicine , division of cancer studies , cancer epidemiology group , london , uk ( m van hemelrijck msc , h garmo phd , prof l holmberg md ) ; oncological centre , clintec department , karolinska institutet , stockholm , sweden ( j adolfsson md ) ; regional oncologic centre , uppsala university , uppsala , sweden ( h garmo , m lambe md , l holmberg ) ; department of urology , uppsala university , uppsala , sweden , and department of clinical cancer epidemiology , karolinska institutet , stockholm , sweden ( a bill - axelson md ) ; department of urology , helsingborg hospital , lund university , sweden ( o bratt md ) ; department of medical epidemiology and biostatistics , karolinska institutet , stockholm , sweden ( e ingelsson md , m lambe ) ; and department of surgical and perioperative sciences , urology and andrology , ume university , ume , sweden ( prof p stattin ) correspondence to : ms m van hemelrijck , kings college london , school of medicine , division of cancer studies , cancer epidemiology group , research oncology , 3rd floor , bermondsey wing , guys hospital , london se1 9rt , uk mieke.vanhemelrijck@kcl.ac.uk risk of thromboembolic diseases in men with prostate cancer : results from the population - based pcbase sweden mieke van hemelrijck , jan adolfsson , hans garmo , anna bill - axelson , ola bratt , erik ingelsson , mats lambe , pr stattin , lars holmberg summary background cancer is associated with an increased risk of thromboembolic diseases , but data on the association between prostate cancer and thromboembolic diseases are scarce . 
we investigated the risk of thromboembolic disease in men with prostate cancer who were receiving endocrine treatment , curative treatment , or surveillance . methods we analysed data from pcbase sweden , a database based on the national prostate cancer register , which covers over 96% of prostate cancer cases in sweden . 
standardised incidence ratios ( sir ) of deep - venous thrombosis ( dvt ) , pulmonary embolism , and arterial embolism were calculated by comparing observed and expected ( using the total swedish male population ) occurrences of thromboembolic disease , taking into account age , calendar - time , number of thromboembolic diseases , and time since previous thromboembolic disease . 
 findings between jan 1 , 1997 , and dec 31 , 2007 , 30 642 men received primary endocrine therapy , 26 432 curative treatment , and 19 526 surveillance . 
for men on endocrine therapy , risks for dvt ( sir 248 , 95% ci 225273 ) and pulmonary embolism ( 195 , 181215 ) were increased , although this was not the case for arterial embolism ( 100 , 082120 )  . 
similar patterns were seen for men who received curative treatment ( dvt : 173 , 147201 ; pulmonary embolism : 203 , 179230 ; arterial embolism : 095 , 069127 ) and men who were on surveillance ( dvt : 127 , 108147 ; pulmonary embolism : 157 , 138178 ; arterial embolism : 108 , 087133 )  . 
 increased risks for thromboembolic disease were maintained when patients were strati ed by age and tumour stage . interpretation all men with prostate cancer were at higher risk of thromboembolic diseases , with the highest risk for those on endocrine therapy . 
 introduction cancer is a risk factor for thromboembolic disease , and patients with cancer are estimated to be around four times more likely to develop a thrombosis than a similar individual without cancer.1 treatments for cancer might also increase the risk of thromboembolic disease . 
for prostate cancer , deep - venous thrombosis ( dvt ) and thromboembolism are common complications after prostatectomy , with risks ranging from 05% to 40% in the 30 days after the operation.25 additionally , the risk of thromboembolic disease increases exponentially with age.6 while several studies have investigated whether patients with prostate cancer treated with endocrine treatment are at higher risk for cardiovascular disease , few populationbased studies have investigated the risk of thromboembolic disease following endocrine treatment.79 during the 1980s , varenhorst and colleagues8 , 9 reported a positive association between the use of cyproterone acetate ( a steroidal antiandrogen ) and brinolytic activity , suggesting a decreased risk of thromboembolisa more recent study , including 11 199 men with prostate cancer , of whom 229 had a venous thromboembolism after diagnosis , showed a greater risk of venous thrombosis associated with cyproterone acetate than with gonadrotropin releasing - hormone ( gnrh ) agonists or orchiectomy.7 thought to have investigation of the risk of thromboembolic disease after endocrine treatment is important for several reasons . 
testosterone cardioprotective e ect , since androgen receptors have been identi ed on the cardiomyocytes and the valves of the heart.1015 preliminary experimental ndings have suggested that androgens might have a role in the regulation of arterial thrombosis through their e ect on platelet activation.16 endocrine treatment is used in a large proportion of men with prostate cancer during the course of the disease , and is the cornerstone treatment for men with locally advanced or metastatic prostate cancer.17 , 18 the indications for endocrine treatment have been widening because of more active treatment in men with advanced disease , and because of neoadjuvant and adjuvant use in men with localised high - risk tumours , resulting in more men of all ages and with all types of prostate tumour receiving endocrine treatment for longer periods.19 we studied a comprehensive population - based cohort with complete follow - up through record linkage of pertinent registers , to assess the risk of thromboembolic disease in men with prostate cancer who had received curative treatment , surveillance , or endocrine treatment . 
 450 vol 11 may 2010 articles methods data collection pcbase sweden is based on the national prostate cancer register ( npcr ) of sweden , which started in 1996 and captures more than 96% of all newly diagnosed , biopsycon rmed prostate cancers . 
this compares favourably with the swedish cancer registry , 20 which misses less than 37% of prostate cancer cases.21 the npcr includes date of diagnosis , age at diagnosis , tumour stage , tumour di erentiation , serum concentration of prostate cancerspeci c antigen ( psa ) at the time of diagnosis , and primary treatment given or planned up to 6 months after the date of diagnosis . 
the validity of primary treatment registered in npcr is more than 90% for curative treatment and surveillance , and more than 95% for endocrine treatment ( stattin p , unpublished )  . 
because of psa screening , the rate of curative treatment increased dramatically during the period of study , whereas the rate of primary endocrine treatment was more or less constant over the same period . 
 the proportion of men with localised disease put on surveillance decreased during this time.22 most endocrine treatment was with gnrh agonists or orchiectomy , although anti - androgens ( not combined with other endocrine treatment ) were prescribed in about 10% of cases . 
 for hormone - resistant prostate cancers , oestrogens and estramustine phosphate were prescribed most often.22 for information by using the swedish 10 - digit personal identity number , pcbase was linked to other national registers , demographics , allowing comorbidities , socio economic status , and causes of death to be collected.23 , 24 in 1987 , the hospital discharge register started collecting information regarding inpatient care . 
each record contains medical information on surgical and anaesthetic procedures , hospital department , and discharge diagnoses coded according to the who international classi cation of diseases 10 ( icd10 ) .23 for heart diseases , the primary diagnoses have been shown to be correct in around 95% of cases , as judged by the european society of cardiology diagnosis guidelines.2527 socioeconomic characteristics were assessed by record linkages to the 196090 5 - yearly census databases , and based on socioeconomic status . 
 socioeconomic status is based on occupational group , and strati es men into white - collar worker ( salaried professionals or educated workers who perform a semiprofessional o ce , administrative , or sales coordination ) , blue - collar worker ( manual workers ) , not gainfully employed , and unknown.24 as of 1997 , the cause of death register collected date and underlying cause of death coded according to icd10.23 detailed information on the data content of pcbase is given elsewhere.28 for our analyses , the following information was taken from pcbase : age , serum concentrations of psa , and treatment information at time of diagnosis , tumour grade and stage , socioeconomic status , history of thromboembolic disease ( primary diagnoses ) , and date of death . 
if who tumour grade was reported primarily instead of gleason score ( 25% of men ) , conversion to gleason score was done as follows : g1 = gleason 26 , g2 = gleason 7 , and g3 = gleason 810 . 
prostate cancer stage was de ned based on the tumour , node , metastasis ( tnm ) stages used in the npcr ( panel ) .22 men with prostate cancer were selected if they received curative treatment , surveillance , or endocrine treatment as primary treatment . 
endocrine treatment was grouped into anti - androgens , oestrogens , orchiectomy , gnrh agonists , gnrh agonist combined with long - term anti - androgens , and other types of endocrine treatment . 
 the swedish central ethics committee ( dnr 14 - 2007 ) the ethics committee at ume university and ( dnr 07 - 049m ) approved this study . statistical analysis we analysed the relation between the di erent types of prostate cancer treatment and subtypes of thromboembolic disease : dvt ( icd10 : i8082 ) , pulmonary embolism ( icd10 : i26 ) , and arterial embolism ( icd10 : k55 , i74 )  . 
 since pcbase is based on the entire swedish population , standardised incidence ratios ( sir ) could be calculated by comparing observed events in the selected cohort ( men with prostate cancer ) with the expected events in the swedish male population . 
the number of events for this standard population was based on the number of men in sweden each year on dec 31 ( register of the total population 19972007 ) .23 , 24 all numbers of events were based on the rst event of thromboembolic disease after a diagnosis of prostate cancer . panel : prostate cancer stage grouping in the national prostate cancer register ( npcr ) of sweden 1 localised ( prostate - speci c antigen [ psa ] < 20 ng / ml ) t02 , n0 or nx , m0 or mx , all grades , psa < 20 ng / ml 2 localised ( psa 20 ng / ml but < 50 ng / ml ) : t02 , n0 or nx , m0 or mx , all grades , psa 20 ng / ml but < 50 ng / ml 3 locally advancedt34 , n0 or nx , m0 or mx , all grades , 4 intermediate groupm0 or mx , psa 100 ng / ml , not in psa < 50 ng / ml stage group 1 , 2 , or 3 5 metastatic diseasem1 or psa > 100 ng / ml 6 missing datamissing t or n or m category / categories or missing grade or missing psa vol 11 may 2010 articles see online for webappendix total ( n ) mean follow - up time ( sd ) age group ( years ) 6574 date period 199799 200002 200306 gleason score 810 missing data prostate cancer stage group localised : psa < 20 ng / ml locally advanced intermediate missing data civil status married single missing data socioeconomic status white collar blue collar 452 the sirs were thus de ned as the ratio of the observed number of a particular thromboembolic disease to the expected number of that thromboembolic disease . 
time of follow - up was taken from the observed numbers of thromboembolic disease , and age - speci c and period - speci c incidence rates were calculated as the incidence of thromboembolic disease in the background population divided by the corresponding person - time in took this background population . 
all calculations thromboembolic disease history into account , since men with a history of previous thromboembolism are at an increased risk for being diagnosed with prostate cancer or a subsequent thromboembolic disease.29 the 95% ci for the sirs were estimated by assuming that the observed cases had a poisson distribution using byars normal approximation.30 , 31 to take comorbidities into account before prostate cancer diagnosis , sir calculations were also strati ed by history of ischaemic heart disease ( icd10 : i20 - 25 ) , circulatory disease ( icd10 : i00 - i99 ) , and stroke ( icd10 : i6064 , g45 )  . 
the absolute risk di erences by di erent types of thromboembolic disease and prostate cancer treatment were calculated , and sensitivity analyses were done to test the assumption of intention - to - treat . 
 finally , we calculated the bias in the sirs due to using the general population rates to estimate the expected numbers of thromboembolic disease , based on the formulas by jones and swerdlow.32 statistical analyses were done with sas version 9.1.3 , and r version 2.7.2. 
 role of the funding source the funding organisations had no in uence on the design and conduct of the study , data collection , management , analysis , interpretation , and preparation , review , or approval of the manuscript . 
the corresponding author had full access to all data , and the nal responsibility to submit the manuscript for publication . results between jan 1 , 1997 , and dec 31 , 2007 , pcbase registered 76 600 men diagnosed with prostate cancer , of whom 30 642 received endocrine treatment as their primary treatment . 
speci cally , 3391 men received anti - androgen therapy ; 5340 underwent orchiectomy ; 9066 received a gnrh agonist ; and 11 646 men received gnrh agonists combined with short - term anti - androgen therapy ( table 1 )  . 
18 446 ( 602% ) of the men given endocrine treatment were aged 75 years or more , compared with 9465 ( 485% ) of those on surveillance , and 1799 ( 68% ) of those who received curative treatment . 
in the endocrine treatment group , 4298 ( 140% ) patients had a localised tumour and psa concentration less than 20 ng / ml , compared with 12 879 ( 660% ) in the surveillance group , and 18 850 ( 713% ) in the curative treatment group . 
 in the group treated with anti - androgens , 838 ( 247% ) men had localised tumours , compared with 643 ( 190% ) with locally advanced disease , and 671 ( 198% ) with metastatic disease . 
 1881 men developed a thromboembolic disease after being diagnosed with prostate cancer : 767 men had a dvt , 873 a pulmonary embolism , and 241 an arterial embolis in the total group with prostate cancer , the sir was 190 ( 95% ci 177204 ) for dvt , 185 ( 173197 ) for pulmonary embolism , and 102 ( 089115 ) for arterial embolis when analysed according to prostate cancer treatment , the risks for dvt and pulmonary embolism were increased irrespective of whether patients received endocrine treatment , were treated curatively , or were on surveillance ( table 2 )  . 
results according to prostate cancer treatment were also analysed for di erent strata of comorbidities before prostate cancer diagnosis , but there was no indication of e ect modi cation by history of any circulatory disease ( data not shown )  . detailed analysis showed that adjustment for gleason score or civil status did not alter the sirs appreciably ( data not shown ) , but di erent e ects by age and tumour stage at time of diagnosis were found . 
age - strati ed and tumour - strati ed analyses showed a larger sir for men younger than 75 years , and for those with metastatic disease , in each treatment group ( table 3 )  . 
overall , the sirs for dvt were larger for men on endocrine treatment than for men who had undergone curative treatment or men who were on surveillance , but there was not such a distinct pattern for pulmonary embolism ( table 3 )  . 
 in age - strati ed analyses for di erent types of endocrine treatment , the smallest sir for both dvt and pulmonary embolism was noted for men treated with anti - androgens , whereas the largest was seen for orchiectomy ( table 4 )  . 
the age e ect seen for the overall endocrine treatment group in table 3 was also noted for each type of endocrine treatment , although it was less strong because endocrine treatment preferences vary by agearound 20% of the men in the two younger age groups received anti - androgens , and 9% underwent orchiectomy , whereas in men aged 75 years and over a higher proportion underwent orchiectomy ( 20% ) and a lower proportion received anti - androgens ( 10% )  . 
 sensitivity analyses excluding men who had an event of thromboembolic disease within 31 days after prostate patients with prostate cancer on endocrine treatment patients with prostate cancer on curative treatment patients with prostate cancer on surveillance sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp sir ( 95% ci ) deep - venous thrombosis 248 ( 225273 ) pulmonary embolism arterial embolism 195 ( 181215 ) 100 ( 082120 ) 436 / 1756 380 / 1952 108 / 1085 173 ( 147201 ) 203 ( 179230 ) 095 ( 069127 ) 160 / 927 248 / 1221 44 / 464 127 ( 108147 ) 157 ( 138178 ) 108 ( 087133 ) obs / exp 171 / 1351 245 / 1556 89 / 821 obs = observed . 
 table 3 : standard incidence ratios ( sir ) for di erent groups of thromboembolic diseases in patients with prostate cancer according to their treatment and strati ed by age and tumour stage cancer diagnosis did not alter the previous ndings signi cantly : changes in sirs ranged between 0% and 050% ( data not shown )  . 
increased risks for thromboembolic events for all treatment groups seem to be dominated by events occurring during the rst 18 months after diagnosis , but an increased risk was still noted after more than 4 years . 
a more detailed analysis of curative treatment indicated that the risks were highest during the rst 6 months , and were higher for radical prostatectomy than for radiotherapy ( data not shown )  . 
for the general population , it can be seen that the absolute risk for dvt was higher among men aged 75 years and over than for those aged under 75 years ( table 7 ) ; by contrast , the absolute risk for dvt in men treated with endocrine 454 vol 11 may 2010 articles anti - androgens orchiectomy gnrh agonists gnrh agonists plus short - term anti - androgen therapy sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp sir ( 95% ci ) obs / exp all ages 156 ( 103227 ) 27 / 173 281 ( 226345 ) 90 / 321 242 ( 204286 ) 142 / 586 251 ( 213294 ) 154 / 613 deep - venous thrombosis < 65 years * 114 ( 021636 ) 6574 years 069 ( 027173 ) 75 years 098 ( 047207 ) pulmonary embolism < 65 years * 023 ( 003173 ) 6574 years 046 ( 016136 ) 75 years 081 ( 039167 ) 176 ( 0231351 ) 136 ( 054342 ) 181 ( 103 318 ) 065 ( 008550 ) 077 ( 025236 ) 117 ( 062218 ) 403 ( 0941732 ) 096 ( 041223 ) 149 ( 089250 ) 063 ( 010408 ) 083 ( 031220 ) 084 ( 047151 ) 232 ( 0531016 ) 138 ( 060317 ) 130 ( 076222 ) 036 ( 005242 ) 082 ( 031221 ) 098 ( 054 177 ) all ages 135 ( 091194 ) 29 / 214 226 ( 177284 ) 73 / 324 184 ( 152220 ) 118 / 641 200 ( 168236 ) 141 / 706 obs = observed . 
gnrh = gonadotropin - releasing hormone . table 4 : standard incidence ratios ( sir ) for di erent groups of thromboembolic disease by type of endocrine treatment treatment was comparable for younger and older men . 
 therefore , the absolute risk increase after exposure to endocrine treatment was larger for those in the youngest age groups ( < 65 years and 6574 years ) than those in the oldest age group . 
the pattern was similar for pulmonary embolism ( data not shown )  . finally , we calculated the possible bias in the sirs due to using general population rates to estimate expected numbers of thromboembolic disease . 
the true relative risk ( rr ) of dvt was de ned as sir ( 1prev ) / ( 1 ( prevsir ) ) , where the prevalence ( prev ) of men with prostate cancer receiving endocrine treatment was estimated to be 560 / 100 000.33 this resulted in the following bias : [ ( rrsir ) / sir ] 100 = [ ( 250248 ) / 248 ] 100 = 084% , indicating that including men with prostate cancer in the general population only resulted in a deviation of less than 1% from the so - called true sir estimates . 
the size of the bias was similar for other thromboembolic diseases and other treatment groups ( data not shown )  . discussion in this large population - based study , we compared the risk of thromboembolic disease between swedish men with prostate cancer and swedish men in the background population . 
additionally , the relative risk of thromboembolic disease in men treated with endocrine therapy was higher for younger men ( < 65 years ) and for men with metastatic disease , while the absolute risk was similar for all three age groups ( < 65 , 6574 , and 75 years )  . 
 first , a baseline risk might be present because of physiological alterations due to the tumour , which seems to be supported by the fact that the risk of thromboembolic disease increases as tumour stage increases . 
second , the di erent patterns of risk associated with di erent types of treatment indicate that treatments , and the selection of these treatments , can a ect the risk of thromboembolic disease . 
curative treatment , such as prostatectomy , and surveillance are also associated with an increased risk of thromboembolic disease , and indicate that some men might have received surveillance because of ongoing comorbidities.34 third , the higher risks , through each vol 11 may 2010 articles absolute risk for men with prostate cancer absolute risk for men in the general population absolute risk di erence ( 95% ci ) deep - venous thrombosis endocrine treatment curative treatment surveillance pulmonary embolism endocrine treatment curative treatment surveillance 408 140 189 355 217 270 164 081 149 183 107 172 244 ( 205282 ) 059 ( 037080 ) 039 ( 011068 ) 173 ( 137209 ) 110 ( 083137 ) 099 ( 065133 ) table 6 : absolute risk and absolute risk di erence for deep - venous thromboembolism and pulmonary embolism disease by prostate cancer treatment in pcbase sweden absolute risk for men with prostate cancer absolute risk for men in the general population absolute risk di erence ( 95% ci ) endocrine treatment curative treatment < 65 years 6574 years 75 years < 65 years 6574 years 75 years surveillance < 65 years 6574 years 75 years 443 405 404 123 144 284 066 066 340 072 039 258 055 061 529 062 041 277 371 ( 246 to 496 ) 366 ( 300 to 431 ) 145 ( 094 to 196 ) 067 ( 039 to 095 ) 083 ( 049 to 117 ) 245 ( 384 to 106 ) 004 ( 041 to 050 ) 025 ( 001 to 051 ) 064 ( 007 to 121 ) table 7 : absolute risk and absolute risk di erence of deep - venous thrombosis by prostate cancer treatment and age group in pcbase sweden stage of the analysis , for men primarily treated with endocrine treatment indicate a risk conferred by endocrine treatment over and above the other treatments and indications for treatment . people with cancer have an increased risk of thromboembolic disease . 
even though this association has long been recognised in clinical practice , few studies have quanti ed this risk for men with prostate cancer in detail.7 , 35 , 36 high rates of thrombosis have been reported in other cancers , especially in people with advanced disease receiving antitumour treatment . 
clinical trials on breast cancer reported a rate of thrombosis of 110% in women with node - positive breast cancer , whereas development of venous thrombosis was reported in 10% of women with advanced ovarian cancer and in up to 28% of people with malignant gliomas.36 treatment for prostate cancer can also be associated with an increased risk of thromboembolic disease . 
 a cohort study based on 5951 patients undergoing prostatectomy showed an incidence of 05% ( 95% ci symptomatic dvt and pulmonary 0407 ) embolism.35 additionally , a british study including 11 199 men with advanced prostate cancer showed that patients treated with cyproterone acetate had a signi cantly higher risk for venous thromboembolism than did men for who underwent orchiectomy or were prescribed gnrh agonists ( adjusted odds ratio 523 , 95% ci 312879 ) .7 than lower all - cause mortality we caution that the observed contrasts in thromboembolic disease between di erent treatment groups should be interpreted as how treatment and treatment selection modify the risk of thromboembolic disease in men with prostate cancer . 
for several reasons , this study cannot directly quantify how much the observed di erences in thromboembolic disease risk between treatment groups are due to the treatments themselves.1 factors taken into account during the process of selecting treatment might also be associated with risk of thromboembolic disease . 
most men receiving curative treatment were recommended surgery , and had to be healthy enough to undergo radical prostatectomy.34 we made a similar observation in our study : men 75 years or older who had undergone curative treatment had a much lower absolute risk for dvt than men of the same age in the standard population , illustrating a selection bias towards healthy men for radiotherapy and prostatectomy . 
 the increased risk of thromboembolism in the group treated with curative intent occurred mainly during the rst 6 months of follow - up , indicating that the surgical intervention was important . 
however , a selection phenomenon might lead to a wrong conclusion about the e ect of surgery in a direct comparison with the rst period of follow - up in , for example , men under surveillance.2 there might have been di erences in diagnostic activity ( frequency of check - ups and di erences in the types of testing used ) for thromboembolic disease between the groups . 
vigilance for thromboembolic disease is likely to have been similar in men with advanced cancer and those o ered curative treatment , but might have been less intense in men under surveillance . 
it is also possible that a rapidly fatal pulmonary embolism in patients with advanced cancer could be interpreted as the fatal end - stage of the cancer , and therefore not coded in hospital charts . 
however , this misclassi cation would only a ect a smaller number of patients , and mainly those on endocrine treatment , biasing their estimates towards null.3 the comparison between the treatment groups might be confounded by the introduction of second - line treatment eg , men treated with curative intent or surveillance will have been exposed to endocrine treatment when the disease progressed . 
 babiker and colleagues37 showed that the early release of 456 vol 11 may 2010 articles into suggested from prostate cancer cells prostasomes the circulation might evoke blood - clotting e ects causing thromboembolic disease . 
another study by li and colleagues16 showed a possible link between endocrine treatment and thromboembolic disease , in which they noted that the prevention of experimental arterial thrombosis by the use of androgens at physiological concentrations is mediated by the androgen receptor through modulation of platelet activation . 
some studies have also testosterone has an that antithrombotic e ect , because higher concentrations are associated with an increase in antithrombin 3.9 , 38 , 39 this possible antithrombotic e ect of testosterone is supported by our treatment - speci c analyses of endocrine treatment , which showed that men treated with anti - androgens have the lowest sir . 
because of the e ect of anti - androgens in the hypothalamus , the testosterone concentrations in serum might even be increased , and thus androgen - dependent pathways in other organs can still function.40 the higher sirs in the youngest age group ( table 3 ) can be explained by a lower absolute thromboembolic disease risk for younger men than for older men in the general population , and similar absolute risks for younger and older men with prostate cancer . 
this age e ect was seen within each tumour stage ; however , a stronger e ect was seen for those with metastatic disease at time of diagnosis , suggesting that advanced cancer potentiates the risk due to the associated predisposition for thromboembolic disease . 
 that allow for detailed the npcr database contains data from more than 76 000 men with prostate cancer , and provides complete follow - up for each patient , as well as linkage to other registers information on thromboembolic disease morbidity . 
the bias in the sirs due to the use of general population rates , which included men with prostate cancer , to estimate expected numbers of thromboembolic disease was found to be negligible . 
however , as suggested by miettinen , 41 the physician or patients choice of endocrine treatment primarily constitutes a confounder for the study of the intended e ect ( palliative treatment for prostate cancer ) , but not for the study of side - e ects such as thromboembolic disease . 
this is because at the time the data were collected , the literature did not suggest a strong association between endocrine treatment and cardio vascular side - e ects , thus it was not standard clinical practice to take thromboembolic disease history into account when initiating treatment . 
 the diagnosis of prostate cancer itself can also bias the results , because these men receive more intensive medical care ( eg , increased number of clinical visits ) , and are therefore more likely to be diagnosed with a thromboembolic disease event when it occurs . 
based on the swedish drug registry , it was shown that it takes about 1 month before men with prostate cancer start taking their endocrine treatment ( stattin p , unpublished )  . 
the e ect of delayed start of treatment was assessed with a sensitivity analysis excluding cardiovascular disease events that occurred within 1 month of the prostate cancer diagnosis , and showed almost no change in sir estimates ( data not shown )  . 
furthermore , an unknown proportion of men treated curatively , on surveillance , or on anti - androgens , subsequently changed to gnrh agonists , which could dilute a true di erence in risk between anti - androgens and gnrh agonists . 
we had no information about smoking habits , diabetes , body - mass index , or hypertension , but none of these factors are strongly associated with prostate - cancer risk , and are therefore unlikely to explain the current ndings.42 no information was available on history of comorbidities other than circulatory diseases . our ndings indicate that it is important to consider thromboembolic side - e ects when treating patients with prostate cancer , especially those who require endocrine treatment . 
risk patterns for thromboembolic disease that di er according to prostate - cancer treatment , age , and tumour stage , are probably explained by the physiological e ects of prostate cancer , treatments for prostate cancer , and the factors taken into consideration when selecting these treatments . 
all other authors declared no con icts of interest . vol 11 may 2010 articles acknowledgments funding came from the swedish research council 825 - 2008 - 5910 , stockholm cancer society , and cancer research uk . 
this project was made possible by the continuous work of the national prostate cancer register of sweden steering group : pr stattin ( chairman ) , anders widmark , lars egevad , magnus trnblom , jan adolfsson , anna bill - axelson , jan - erik johanssson , david robinson , jonas hugosson , jan - erik damber , ola bratt , gran ahlgren , and roy ehrnstrm . articles sensitivity and speci city of multimodal and ultrasound screening for ovarian cancer , and stage distribution of detected cancers : results of the prevalence screen of the uk collaborative trial of ovarian cancer screening ( ukctocs ) usha menon , aleksandra gentry - maharaj , rachel hallett , andy ryan , matthew burnell , aarti sharma , sara lewis , susan davies , susan philpott , alberto lopes , keith godfrey , david oram , jonathan herod , karin williamson , mourad w seif , ian scott , tim mould , robert woolas , john murdoch , stephen dobbs , nazar n amso , simon leeson , derek cruickshank , alistair mcguire , stuart campbell , lesley fallow eld , naveena singh , anne dawnay , steven j skates , mahesh parmar , ian jacobs summary background ovarian cancer has a high casefatality ratio , with most women not diagnosed until the disease is in its advanced stages . 
 methods between 2001 and 2005 , a total of 202 638 post - menopausal women aged 5074 years were randomly assigned to no treatment ( control ; n = 101 359 ) ; annual ca125 screening ( interpreted using a risk of ovarian cancer algorithm ) with transvaginal ultrasound scan as a second - line test ( multimodal screening [ mms ] ; n = 50 640 ) ; or annual screening with transvaginal ultrasound ( uss ; n = 50 639 ) alone in a 2 : 1 : 1 ratio using a computer - generated random number algorithall women provided a blood sample at recruitment . 
 the main reasons for withdrawal were death ( two mms , 28 uss ) , non - ovarian cancer or other disease ( none mms , 66 uss ) , removal of ovaries ( ve mms , 29 uss ) , relocation ( none mms , 39 uss ) , failure to attend three appointments for the screen ( 72 mms , 757 uss ) , and participant changing their mind ( 483 mms , 1490 uss )  . 
 overall , 4355 of 50 078 ( 8.7% ) women in the mms group and 5779 of 48 230 ( 120% ) women in the uss group required a repeat test , and 167 ( 03% ) women in the mms group and 1894 ( 39% ) women in the uss group required clinical evaluation . 
28 ( 16 mms , 12 uss ) of 58 ( 483% ; 95% ci 350618 ) of the invasive cancers were stage i / ii , with no di erence ( p = 0396 ) in stage distribution between the groups . 
the sensitivity , speci city , and positive - predictive values for all primary ovarian and tubal cancers were 894% , 998% , and 433% for mms , and 849% , 982% , and 53% for uss , respectively . 
for primary invasive epithelial ovarian and tubal cancers , the sensitivity , speci city , and positive - predictive values were 895% , 998% , and 351% for mms , and 750% , 982% , and 28% for uss , respectively . 
there was a signi cant di erence in speci city ( p < 00001 ) but not sensitivity between the two screening groups for both primary ovarian and tubal cancers as well as primary epithelial invasive ovarian and tubal cancers . interpretation the sensitivity of the mms and uss screening strategies is encouraging . 
 although advances in therapy have improved median survival during the past decade , there has been little or no change in the overall mortality rate.1 , 2 women are commonly diagnosed with stage iii / iv disease , for which 5 - year survival rates are around 27% and 16% , respectively.35 this has led to e orts over the past two decades to develop early detection strategies using serum ca125 and ultrasound.6 , 7 preliminary evidence from a previous randomised controlled trial suggests that screening sequentially with ca125 and ultrasound ( multimodal screening ) can result in a survival bene t.8 median survival was signi cantly increased in women who developed ovarian cancer in the screened group compared with the control group ( 729 vs 418 months , p = 00112 )  . 
improved survival has also been reported in a single - arm ultrasound - based study.9 re nements have been made to screening since the two previous studies , including the introduction of transvaginal ultrasound , 10 improvements in the interpretation of ultrasound ndings using morphology - based indices , 9 , 1113 and the development of a risk of ovarian cancer algorithm for the interpretation of serial ca125 results.14 , 15 the multicentre united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) is a randomised controlled trial designed to provide de nitive data on the e ect of ovarian cancer screening on mortality , as well as comprehensively addressing the cost , acceptance , physical and psychosocial morbidity , and performance characteristics of multimodal screening and ultrasoundbased screening . methods participants women were recruited through 13 regional trial centres located in national health service ( nhs ) trusts in england , wales , and northern ireland.16 all women provided written consent . 
eligibility criteria included age panel 1 : classi cation of ovarian morphology on ultrasound normal ovary of uniform hypoechogenicity and with a smooth outline with or without a single inclusion cyst or spots of calci cations inclusion cyst must be single , less than 10 mm in diameter and not distort the outline of the ovary simple cyst a single , thin walled , anechoic cyst with no septa or papillary projections complex any case in which the ovary has any non - uniform ovarian echogenicity , excluding single simple or inclusion cysts 5074 years , and postmenopausal status de ned as greater than and including 12 months , amenorrhoea following a natural or surgical menopause , or greater than and including 12 months of hormone - replacement therapy commenced for menopausal symptoms.17 women were excluded if they had a history of bilateral oophorectomy , active malignancy ( women with a past history of malignancy were eligible if they had no documented persistent or recurrent disease and had not received treatment for > 12 months ) , previous history of ovarian cancer , participation in other ovarian cancer screening trials , or increased risk of familial ovarian cancer . 
high - risk women were eligible for a separate trial : the united kingdom familial ovarian cancer screening study ( ukfocss ) .18 the study was approved by the uk north west multicentre research ethics committee ( 00 / 8 / 34 ) , with site - speci c approval from the local regional ethics committees and the caldicott guardians ( data controllers ) of the participating primary care trusts . scanned electronically using procedures invitations to participate in the trial were sent to women aged 5074 years whose details were obtained from the age and sex registers of the participating 27 primary care trusts.16 on enrolment at the trial centres , women viewed an information video and participated in a group discussion before completing a datasheet , consent forms , and undergoing venepuncture . 
the recruitment questionnaires were sent to the coordinating centre , where they were com puterised intelligent character - reading and optical - mark - reading software ( teleform elite version 8.1.1 , cardi software inc , vista , ca , usa )  . 
any inconsistency or information not recognised by the data - capture software was veri ed manually by trained data - entry sta , who validated the computer - interpreted data . 
once the custom - built trialmanagement system con rmed eligibility , participants were randomly assigned to either no treatment ( control ) ; annual ca125 screening ( interpreted using a patented risk - of - ovarian - cancer algorithm ) with transvaginal ultrasound scan as a second - line test ( multimodal screening ; mms ) ; or annual screening with transvaginal ultrasound ( uss ) alone in a 2 : 1 : 1 ratio with a computergenerated random number algorith randomisation was done as follows : rst , the trial management system allocated a set of 32 random numbers to each trial centre ; second , the lowest eight were allocated to the mms group , the next eight to the uss group , and the remaining 16 to the control group ; third , each successive volunteer within the trial centre was randomly allocated one of the random numbers and so randomly assigned a group ; and nally , when all 32 random numbers had been used up a further set of 32 was generated . 
randomisation was accomplished by the trial - management system using the visual basic randomisation statement and the rnd function . 328 vol 10 april 2009 articles following randomisation , letters were automatically printed and sent to each woman and their general practitioner con rming eligibility and randomisation status . 
blood samples were taken in gel tubes ( 8 ml gel separation serum tubes ; greiner bio - one 455071 , stonehouse , uk ) at the trial centres and transported overnight at ambient temperature to the central laboratory . 
serum ca125 electroconcentrations were chemiluminescence sandwich immunoassay on an elecsys 2010 ( roche diagnostics , burgess hill , uk ) using two monoclonal antibodies ( oc125 and m11 ; fujirebio diagnostics ab , gteborg , sweden )  . 
the rst scan ( level 1 scan ) , and any repeat level 1 scans needed because of an type 1 unsatisfactory rst scan , were done by sonographers , who were certi ed sonographers , trained midwives , or doctors with experience in gynaecological scanning who were working in the nhs . 
detailed description of all features the number and size of cysts , wall regularity , presence and thickness of septae , size of papillations , and echogenicity of the uid contentswere recorded . 
cysts and complex morphology were classi ed pictorially , initially using the format reported in the kentucky screening trial , 19 and from 2003 onwards using the ( iota ) international ovarian tumour analysis classi cation.13 measurement of the ovary was important to con rm that it had been visualised , and for audit purposes . 
only cyst volume panel 2 : possible outcomes after level 1 and level 2 screens in the mms group level 1 screen normal risk of ovarian cancer score : women returned to annual screening , with the next level 1 blood test scheduled on the next anniversary of the randomisation date intermediate risk of ovarian cancer score : women were recalled for a repeat ca125 measurement 12 weeks after the screen . 
any women whose risk of ovarian cancer remained intermediate after three ca125 tests were referred for a level 2 screen elevated risk of ovarian cancer score : women were recalled for a level 2 screen in 68 weeks , with earlier screens arranged where there was a high index of suspicion level 2 screen women with a normal transvaginal ultrasound scan result and normal or intermediate risk of ovarian cancer returned to annual screening , with the next level 1 test on the next anniversary of the randomisation date women with a normal transvaginal ultrasound scan result but an elevated risk of ovarian cancer , or an unsatisfactory scan irrespective of risk of ovarian cancer status , underwent a repeat level 2 screen in 6 weeks and were triaged again on the basis of the results to annual screening or clinical assessment women with an abnormal transvaginal ultrasound scan were referred for clinical assessment irrespective of their risk of ovarian cancer status panel 3 : possible outcomes after level 1 and level 2 screens in the uss group level 1 screen women with a normal scan returned to annual screening , with the next level 1 transvaginal ultrasound scan on the next anniversary of the randomisation date women with an unsatisfactory scan result attended a repeat level 1 scan in 12 weeks . 
women were returned to annual screening following two unsatisfactory scans women with an abnormal level 1 scan were referred for a level 2 scan in 68 weeks , with earlier scans arranged where there was a high index of suspicion level 2 screen women with a normal level 2 scan returned to annual screening , with the next level 1 transvaginal ultrasound scan on the next anniversary of the randomisation date an unsatisfactory level 2 scan led to a repeat level 2 scan in 6 weeks or earlier , and women were triaged on the basis of the ndings to annual screening or clinical assessment women with an abnormal scan were referred for clinical assessment vol 10 april 2009 articles was used for scan classi cation . 
when ovaries were not visualised , the sonographers speci ed whether a good view of iliac vessels had been obtained or a poor view owing to obstruction by the bowel , broids , pelvic varicosities , or for other reasons . 
ascites was de ned as a maximum vertical pool measurement of greater than or equal to 10 m based on the visualisation and morphology of the ovaries , the scan was classi ed as either a normal scan , in which both ovaries had normal morphology or simple cysts less than 60 cm , or were not visualised but a good view of the iliac vessels was obtained ; an unsatisfactory scan , in which one or both ovaries were not visualised owing to a poor view ; or an abnormal scan , in which one or both ovaries had complex morphology or simple cysts greater than 60 cm , or ascites . scan images were transferred weekly on magnetooptical discs for central archiving . 
trial centres were able to request central review of ultrasound images . cancer using screening strategies in the level 1 screen in the mms group , women underwent venepuncture and serum ca125 measurement . 
the assay results were uploaded directly into the trial - management system , which calcu lated the risk of ovarian algorithm developed previously.15 , 17 the rst risk of ovarian cancer determination was based on a single measurement of ca125 and the womans age - speci c incidence of ovarian cancer . 
women were triaged into three risk groups on the basis of their risk of ovarian cancer , which determined whether they returned to annual screening or went on to have a repeat ca125 measurement or level 2 screen ( panel 2 )  . 
level 2 change rate and the the 202 638 women all had a blood sample taken at recruitment screening involved venepuncture for repeat ca125 assay and a transvaginal ultrasound scan . 
the results of the level 2 screen triggered three possible courses of action , as shown in panel 2 . the initial cuto s used for intermediate and elevated risk of ovarian cancer were greater than or equal to 1 / 1818 and greater than or equal to 1 / 500 , respectively . 
as the proportion of women classi ed into these risk categories were less than the proposed 15% and 2% , respectively , the cuto s were revised on april 1 , 2005 , to greater than or equal to 1 / 3500 and greater than or equal to 1 / 1000 after extensive data review by the independent data monitoring and ethics and trial steering committees . 
 there were three possible courses of action depending on the results of the level 1 scan , including referral for a level 2 scan , the results of which triggered one of a further three courses of action , as shown in panel 3 . 
 all clinicians were provided written information on the risk estimates for malignancy associated with the various morphological classi cations from the iota series once the estimates had been presented at the annual european society of gynaecological oncology meeting in 2003 . 
 additionally , clinicians were made aware that women who had previously undergone a hysterectomy had an incidence of adhesions and peritoneal increased pseudocysts that may be reported as multilocular adnexal cysts . clinical assessment this was undertaken by a designated clinician and included clinical evaluation and investigations as appropriate . 
these included serum ca125 in women in the ultrasound group , repeat transvaginal scans and doppler studies , ct / mri of the abdomen and pelvis , and occasionally assessment of other tumour markers . 
 for women in the mms group with a normal transvaginal ultrasound scan but elevated risk of ovarian cancer , clinical assessment included ruling out other causes of increased ca125 concentrations . 
the management plan took the views of the individual into account , and also accounted for any signi cant comorbidity , the speci c morphological features of the detected lesion , and history of a previous hysterectomy or major pelvic surgery that could be responsible for false - positive ultrasound appearances . for women who underwent surgery , the recommendation was removal of both ovaries and fallopian tubes for histopathological examination , even if the ovaries appeared macroscopically normal . 
where pelvic adhesions were present and there was an increased risk of complications , the clinician could opt to remove only the ovary found to have an abnormality on ultrasound and not proceed to remove the contra lateral ovary . 
a laparotomy was undertaken if clinical ndings or laparoscopy led to a strong suspicion of ovarian cancer , or if a laparoscopic procedure was not felt to be appropriate for other reasons . 
women found to have ovarian or tubal cancer at a primary laparoscopic procedure underwent a subsequent staging pro cedure . bilateral a follow - up plan was drawn up if , after clinical assessment , investigation , and discussion with the woman , a decision was made to manage the ndings conservatively . 
most women were followed up with a transvaginal ultrasound scan and a serum ca125 assessment at 3 months with a possible repeat at 6 months , and returned to annual screening if the ndings were unchanged at this review . 
 follow - up all participants are being followed up through a agging study with the nhs information centre for health and social care ( formerly o ce for national statistics , ons ) in england and wales , and with the central services agency and cancer registry in northern ireland . 
 additionally , women continued to attend for subsequent annual screens , and those who had been in the trial for 35 years following randomisation were sent follow - up questionnaires . 
 statistical analysis the primary outcome measure in ukctocs is ovarian cancer mortality and the primary comparison is based on an intention - to - treat analysis between the control group and both screened groups combined ( mms plus uss )  . 
 however , as the operating characteristics of the two screening groups are di erent a comparison between the control group and an individual screen group ( mms or uss ) is of equal interest . 
the design provides greater than 90% power to detect a 30% reduction in ovarian cancer mortality between the control and combined screening groups , and greater than 80% power to detect a 30% reduction in mortality between the control and either one of the individual screening groups , with both comparisons tested at a signi cance level of 005 . 
it is important to note that if one of the comparisons ( control vs mms or uss ) is signi cant and the other is not , the result would not necessarily imply that one method is signi cantly better than the other . 
if , as anticipated , the di erence in ovarian cancer mortality between the two screened groups is modest , then this study will have limited power to detect such di erences . 
the choice of screening strategy will then be based on other outcome measures such as sensitivity , positive - predictive value , morbidity , quality of life , and health economics . this paper presents the outcome of the prevalence screen in women randomly assigned to either mms or uss . 
the prevalence screen was de ned as a single or series of serum ca125 assays with or without transvaginal ultrasound scan ( mms ) or transvaginal ultrasound scan alone ( uss ) culminating in surgery or a return to annual screening . 
the screen was considered positive ( screen positive ) if the woman was referred for surgery and negative ( screen negative ) if the woman was returned to annual screening . 
the primary outcome measure was primary ovarian or fallopian tube cancer ( icd - 10 code c56 and c57.0 , respectively ) diagnosed within 12 months of the last scan or serum ca125 test in the prevalence screen . 
women with primary peritoneal cancer ( icd - 10 code c48.2 ) and those with ovarian neoplasms of uncertain behaviour ( icd - 10 code d39.1 ) were not included in the outcome measure . 
the most common reasons for withdrawal were death ( two mms ; 28 uss ) , non - ovarian cancer or other disease ( 66 uss ) , removal of ovaries ( ve mms ; 29 uss ) , relocation ( 39 uss ) , failure to attend three appointments for the screen ( 72 mms ; 757 uss ) , and participant changing her mind ( 483 mms ; 1490 uss )  . 
in accordance with good practice for randomised controlled trials we did not statistically compare the baseline characteristics of the women assigned to the two groups ; 20 , 21 the groups were well balanced ( table 1 )  . of the 50 078 women who underwent a prevalence screen in the mms group , 45 523 ( 909% ) were classi ed as low risk by the risk of ovarian cancer algorithm and returned to annual screening . 
in the course of the screen , ve women in the mms group died from unrelated causes , 24 were diagnosed with cancers other than ovarian cancer , and 215 withdrew from the trial . of the 48 230 women randomly assigned to the uss group , 42 416 ( 879% ) had transvaginal ultrasound scans , 4325 ( 90% ) had transabdominal ultrasound scans , and 1489 ( 31% ) had both . 
 six women in the uss group died from unrelated causes during the course of screening , seven were diagnosed with cancers other than ovarian cancer , and 252 withdrew from the trial . overall , 942 ( 095% ) of the 98 308 women screened underwent surgery as a result of the prevalence screen , with 87 women in the uss group undergoing surgery for every one woman from the mss group who underwent surgery . 
 there was a di erence in surgical approach between the two groups , with 75 of 97 ( 773% ) operations in the mms group involving laparotomy versus 397 of 845 ( 469% ) in the uss group ( table 2 )  . 
834 ( 47 mms , 787 uss ) women who underwent surgery were found to have benign pathology or normal ovaries ( table 3 ) , of whom 24 ( 29% ; 95% ci 1740 ) experienced a major complication . 
 * * three breast cancers , one endometrial cancer , and one cancer of the appendix . table 3 : histology in women who underwent surgery as a result of screening ( screen positives ) nodule and residual ovary in left pelvic side wall , one pulmonary embolism , two cases of deep - vein thrombosis , four cases of wound dehiscence , one wound haematoma , two hernias , one signi cant ileus , one bowel obstruction , one bowel stula , and two cases of signi cant infection . ovarian or tubal malignancies were detected in 87 women : 42 in the mms group and 45 in the uss group ( table 3 )  . 
there was no signi cant di erence ( fishers exact test p = 0229 ) in the number of stage iii borderline cancers in the mms ( two of eight ) compared with the uss group ( one of 20 )  . 
 in the mms group , 33 ( 786% ) of the 42 women with ovarian or tubal malignancies had ovarian cancer detected as a result of an elevated risk of ovarian cancer on the level 1 screen ( rst blood test )  . 
in the uss group , all 45 ( 100% ) women had ovarian cancer detected as a result of an abnormal scan on the level 1 screen ( rst scan )  . 
the median time to surgery from level 1 scan in these women was similar to that for women in the mms group : 815 days ( iqr 6031125 )  . 
 however , nine ( 214% ) of the women in the mms group with ovarian or tubal malignancies had ovarian cancer detected after an intermediate risk of ovarian cancer at the level 1 screen that led to repeat tests . 
the median time to surgery from the level 1 screen in these women was 2739 days ( iqr 22003310 ) , since the protocol for managing intermediate risk was to repeat ca125 tests 334 vol 10 april 2009 articles over a period of 810 months ( gure 2 )  . 
one woman initially had a normal level 2 scan , and one woman had two normal level 2 scans but was operated on based on a severe risk of ovarian cancer classi cation . 
they include one woman in the mms group and two from the uss group who withdrew from the trial after their level 1 screen and had an ovarian cancer diagnosed more than 1 year later . 
at an incident screen 22 months later , an increase in size of the mass on ultrasound prompted bilateral salpingo - oophorectomy , and she was diagnosed with stage ic papillary serous cystadenocarcinoma . 
as information on cancers can take up to 3 years to be recorded by the national cancer registries , we explored in detail the other sources of follow - up data in the 12 658 women for whom time from censorship ( 1 year from the date of the last scan or ca125 test on the prevalence screen ) to cancer registry follow up on june 13 , 2008 , was less then 3 years . 
in this cohort , after the censorship date , we had additional con rmation of ovarian cancer status in 11 336 women , as they had attended for further screening , and in an additional 17 women through returned follow - up questionnaires . 
 the source of veri cation of ovarian cancer status was limited to cancer registry follow up that was less than 3 years from the date of censorship in only 1275 women ( 13% of the entire cohort ; table 5 )  . 
this included one primary borderline and four invasive epithelial ovarian cancers in the mms group , and eight primary invasive epithelial ovarian cancers in the uss group ( table 3 )  . 
the ca125 concentrations at the prevalence screen ranged from 7 to 24 iu / l in the ve women with ovarian and tubal cancers in the mms group , and the cancers were diagnosed at 92 , 204 , 254 , 294 , and 329 days after the screen . 
all of the prevalence scans were normal in the uss group , and the cancers were diagnosed at 30 , 203 , 255 , 267 , 278 , 293 , 301 , and 341 days after the screen . for all primary ovarian and tubal cancers , the sensitivity , speci city , and positive - predictive values for mms and uss screening are shown in table 6 . 
there were 23 ( 42 of 97 ) operations per case of ovarian cancer in the mms and 188 ( 45 of 845 ) operations per case of early ( i / ii ) stage cancers ( % ) 471% 298% 649% 500% 291% 709% 483% 350% 618% 750% 194% 994% 00% 00% 410% 250% 55% 572% stage lower 95% ci upper 95% ci morphology serous endometrioid clear cell carcinosarcoma adenocarcinoma grade not graded screen positive screen negative overall overall * in two cases a diagnosis was made on the basis of ascitic uid cytology , omental biopsy , and imaging : primary surgery was not undertaken . table 4 : characteristics of primary invasive epithelial ovarian and tubal cancers ( icd - 10 c56 and c57.0 ) ons follow - up > 3 years from censorship date or when death certi cate was available number of women who have had an appointment after censorship date * number of women who have completed a follow - up questionnaire after censorship date * mms ( n = 50 078 ) uss ( n = 48 230 ) overall ( n = 98 308 ) 45 544 ( 909% ) 40 106 ( 832% ) 85 650 ( 871% ) 4071 ( 81% ) 7295 ( 182% ) 11 366 ( 116% ) 4 ( 001% ) 13 ( 003% ) 17 ( 002% ) remaining * 459 ( 09% ) 816 ( 17% ) 1275 ( 13% ) * in women with ons follow - up < 3 years from censorship date . 
censorship date is 1 year from the date of the last scan or ca125 in the prevalence screen . table 5 : details of follow - up of women who underwent screening the in speci city between ovarian cancer in the uss group . 
 when the analysis was restricted to primary invasive epithelial ovarian and tubal cancers , sensitivity was , compared with values when all cancers were included ( table 6 ) , much the same in the mms group , but lower in the uss group , although the di erence in sensitivity between mms and uss was still not statistically signi cant ( p = 0126 )  . 
 vol 10 april 2009 articles total number of women number of surgeries screen positives screen negatives sensitivity 95% ci speci city 95% ci 95% ci positive - predictive value screen positives screen negatives sensitivity 95% ci speci city 95% ci 95% ci positive - predictive value primary ovarian and tubal malignancies ( icd - 10 c56 and c57.0 ) within 1 year of prevalence screen number of operations per screen positive 188 108 primary invasive epithelial ovarian and tubal malignancies within 1 year of prevalence screen overall p value * 48 230 98 308 50 078 894% 849% 870% 0564 769965 724933 788929 998% 982% 990% < 00001 998998 981984 990991 433% 333538 53% 3971 92% 75113 895% 750% 829% 0126 752971 566885 720908 998% 982% 990% < 00001 998998 981984 990991 351% 256454 28% 1842 62% 4779 162 number of operations per screen positive 352 * fishers exact test . 
 borderline epithelial ovarian cancers and ovarian neoplasms of uncertain behaviour treated as false positives . table 6 : performance characteristics for detection of malignant ovarian and tubal neoplasms ( icd - 10 c56 and c57.0 ) in the prevalence screen speci city was higher in the mms than in the uss group , resulting in fewer repeat tests and almost nine times fewer operations per cancer detected . 
the main strengths of the study are recruitment by random invitation using the health - authority registers of 27 primary care trusts , the multicentre design involving recruitment and screening through 13 nhs trusts , the scale of the trial , high compliance with screening , randomisation to two well - de ned screening strategies , and an independent review of surgical outcomes and detailed follow - up of the entire cohort . 
although primary peritoneal cancers are treated similarly to advanced primary ovarian carcinomas , neither the mms nor the uss screening strategies were developed to detect thehowever , data on these cancers would be interesting , so primary peritoneal cancers are listed separately in table 3 . 
however , we have ( low malignant potential ) ovarian neoplasms , since they share the same icd - 10 code ( c56 ) as primary invasive epithelial ovarian cancers . 
 included primary borderline problem 84 primary ovarian ( icd - 10 c56 ) and three tubal cancers ( icd - 10 c57.0 ) were detected on screening , with a further 13 primary ovarian cancers diagnosed clinically in the ensuing year . 
19% ( eight of 42 ) of the primary ovarian cancers detected were borderline in the mms group , compared with 15% reported in clinical series.24 however , 44% ( 20 of 45 ) of the primary ovarian cancers detected in the uss group were borderline . 
this highlights an issue that has already become a signi cant cancer - screening strategiesthe detection of cancers that may never have been diagnosed in an individuals lifetime had they not been screened . 
in cancer screening , estimates of overdetection range from 3 to 50% of cases in breast cancer screening26 and 22 to 34% in prostate cancer screening.27 a similar rate of 25% overdetection has been reported with chest radiography for lung cancer , with the use of ct expected to result in higher rates.28 in ovarian cancer , such false positives may include ovarian neoplasms of uncertain behaviour ( icd - 10 d39.1 ) and borderline disease . 
once borderline cancers are detected during screening , it is di cult not to operate given that borderline and stage i invasive other 336 vol 10 april 2009 articles results indicate inherent strategies . 
the ovarian cancers share common morphological features on ultrasound imaging.29 the novel design of ukctocs , which randomly assigns women to two very di erent screening strategies , provides some insight into the in the di erent extent of overdiagnosis that screening pseudodisease will be less apparent with a serum ca125based ovarian cancer screening strategy than with uss screening . 
this accords with results from the prevalence screen of the prostate lung colon ovarian cancer ( plco ) screening trial , in which only one of nine borderline ovarian neoplasms were detected by ca125 screening , whereas all nine were detected by ultrasound.23 there is a possibility that some of these borderline tumours may progress to invasive cancers if undetected , although there is little evidence to support this . 
 di erences between the screening groups on later follow - up should help to elucidate the issue , and allow de nite estimates of overdiagnosis to be calculated . given the issues surrounding borderline disease , a separate analysis was done excluding borderline lesions , e ectively treating such lesions as false positives . 
this resulted in a fall in the sensitivity of the uss screen from about 85% to 75% , with an attendant increase in the ratio of operations per true positive from 19 : 1 to 35 : 1 . 
the detection rates in the mms group remained at around 89% , with a small increase in the ratio of operations per true positive from 23 : 1 to 29 : 1 . 
however , the clinical e ect of this di erence will depend on the mortality e ect on follow up , and on issues such as patient satisfaction and acceptability . various factors may contribute to the detection of more primary invasive epithelial cancers in the mms group than in the uss group . 
it is possible that a transvaginal ultrasound scan done at the time of the level 1 screen , 75 months earlier than when the transvaginal ultrasound scan was actually done in these women , would not have detected an abnormality . 
 although an unsatisfactory scan in the uss group does lead to a repeat level 1 scan in 3 months , the follow - up is not equivalent to that of an intermediate risk of ovarian cancer , as women are returned to annual screening after two unsatisfactory scans but have continued follow - up with ca125 after two intermediate risk of ovarian cancer results . 
ultrasound , unlike ca125 , has a subjective element , and it is possible that the heightened awareness of a sonographer in view of rising ca125 concentrations contributed to a positive diagnosis . 
however , it is noteworthy that two of the nine women in the mms group who were diagnosed after initially being classi ed as intermediate risk had normal scans initially . 
by contrast , ultrasound has a subjective element , and accuracy is correlated with the experience of the sonographer.30 , 31 there are no described qualityassurance measures for scanning postmenopausal ovaries in asymptomatic women . 
more than 100 sonographers were required to deliver the scan load of 55 000 scans per year ; these individuals were fully certi ed sta working in ultrasound departments in the uk nhs . 
until then , it should be noted that the number of interval cancers and sensitivity in the uss group is in keeping with other large single - centre and multicentre series ( table 7 ) for which systematic follow - up and tracing of interval cancers has been undertaken . 
a previous ultrasound and autopsy study that 154% of 234 post menopausal women who had died from nongynaecological diseases had ovarian cysts.32 here , 1894 ( 39% ) of women were found to have abnormal scans . 
 clinical assessment in the uss group , which included the use of morphological features detected during ultrasound , serum ca125 , and other imaging modalities , decreased surgical rates to 446% ( 845 of 1894 ) of those found to have abnormalities compared with 581% ( 97 of 167 ) of those with abnormalities in the mms group ( table 2 )  . 
the lack of follow - up data on the outcome of pelvic masses with benign ultrasound morphology33 means that a proportion of women and clinicians will opt for surgery once a complex adnexal lesion is detected , even if it is more likely to be benign . 
this is exempli ed in this series , in which a lesion detected on ultrasound was not removed on laparoscopy because it was thought to be an ovarian broma ( table 2 )  . 
the higher proportion of laparoscopic procedures in the uss group than in the mms group ( 624% vs 286% ) re ects the lower suspicion of malignancy among clinicians for certain ultrasounddetected lesions . 
however , such decisions are not straightforward , as the risk of malignancy associated with lesions such as multilocular cysts in clinical series is 18% , rising to 49% if a solid component is also present.29 during further rounds of screening there is likely to be a substantial fall in the number of women undergoing surgery for benign lesions in the uss group , as most will have been removed or detected and managed conservatively during the prevalence screen . 
it is therefore important to wait for the results of incidence screening before drawing de nite conclusions about the positive - predictive value and speci city characteristics of the two screening strategies . 
in the ultrasound screening trial by van nagell and colleagues , 9 the number of operations per case of invasive epithelial ovarian cancer detected was 93 : 1 ( table 7 ) after a mean of 48 annual screens . 
29% of women undergoing surgery which resulted in benign pathology or normal ovaries being detected , experienced a major complication involving injury to a hollow viscus or signi cant haemorrhage . 
 there was no di erence in the complication rates in the two screening groups . the proportion of primary invasive ovarian and fallopian tube cancers diagnosed with stage i / ii disease ( 48% ) was encouraging compared with the 26% rate in the clinical series34 and 22% in the prevalence screen of the plco screening trial in the usa ( table 7 ) .23 the highest reported proportion of early - stage cancers detected on screening is from the university of kentucky screening programme , 9 where 82% of primary invasive epithelial ovarian cancers detected were stage i / ii . 
the overall number of ovarian cancers reported in the university of kentucky study was also lower ( table 7 ) .9 the e ect of this apparent stage shift on mortality will not be known until su cient events have accrued for a comparison with mortality in the control group , when the trial is completed in december , 2014 . 
 the di erences in the uptake of the initial screen between women randomly assigned to the mms group and uss group ( gure 1 ) must be interpreted with care . 
 it is important not to interpret this as indicating that women preferred a blood test to a scan , as a signi cant proportion of this di erence re ects trial design . 
analysis of the psychosocial data and compliance with annual screening will provide better measures of womens preferences . a limitation of trial design could be that the criteria used to classify scans did not incorporate one of the many weighted morphological indices that have been 338 vol 10 april 2009 articles proposed to improve discrimination between benign and malignant masses.29 , 35 however , it is important to note that most of these indices were derived from clinical series in symptomatic patients , in whom advanced cancers are the nordata on morphological characteristics of early ovarian cancers in asymptomatic long - term follow - up of patients and outcome on ultrasound - detected limited . 
simple lesions are unilocular cysts are an exception , for which long - term follow - up of women has shown that they are invariably benign.36 this was incorporated into the ukctocs trial design , with simple cysts less than 60 cm in size classi ed as normal and the women returned to annual screening with no further review . 
all clinicians were provided with pictorial depictions of complex morphology , initially using the kentucky format19 until the adoption in 2003 of the iota format , 13 and all clinicians were aware of the risk of malignancy associated with the features in the clinical series . 
 serum ca125 and transvaginal ultrasound remain at the core of all new screening and diagnostic strategies being proposed for ovarian cancer , and although many new markers have been discovered since 1999 , none have so far been validated in a prospective screening trial . 
the trial serum bank , which currently has over 350 000 samples , will make the retrospective testing of new markers possible . a nal limitation of this report is that no data are available on cancers in the control group . 
however , in line with other ovarian cancer screening randomised controlled trials , 23 it was felt by the overseeing committees that the release of such information when screening is ongoing would compromise the overall outcome of the trial . 
although this maximises external validity by excluding biases related to advertisement and self - referral , the cohort is still likely to be healthier than the general uk population because of the characteristics of the women who chose to respond . 
the multicentre design , nhs hospital setting , use of standard tests ( ca125 and transvaginal ultrasound ) done by sta those who would deliver a national similar programme , and the management of women with abnormalities in nhs clinics using national guidelines ensures that the ndings of the trial are applicable to the wider population . 
there are inherent di erences between the two strategies being tested , with a more subjective element inherent in the ultrasound - based strategy than with the ca125 test , for which it is easy to implement stringent quality control . 
mms has signi cantly better speci city than does uss , resulting in fewer repeat tests and less surgery ; sensitivity for the detection of primary epithelial cancers of the ovaries and fallopian tubes seems better with mms than with uss , although is not statistically signi cant . 
the results of ongoing screening are required before a conclusion can be drawn regarding the e ect of screening on mortality . the di erence contributors ij , um , mp , sjs , sc , lf , and am were involved in study design . 
none of the other authors declared any con icts of interest . acknowledgments we are particularly grateful to the women throughout the uk who are participating in the trial , to the entire medical , nursing , and administrative sta who work on the ukctocs and to the independent members of the numerous oversight committees . 
the trial was core funded by the medical research council , cancer research uk , and the department of health , with additional support from the eve appeal , special trustees of barts and the london , and special trustees of university college london hospital ( uclh )  . 
a large portion of this work was done at uclh / ucl within the womens health theme of the national institute for health research uclh / ucl comprehensive biomedical research centre supported by the department of health . 
 news upcoming meetings sept 29oct 6 , 2009 lifestyle factors oct 2027 , 2009 chemical agents and related occupations special report : policy a review of human carcinogenspart d : radiation in june 2009 , 20 scientists from nine international countries met at the agency for research on cancer ( iarc ) to reassess the carcinogenicity of the types of radiation previously classi ed as carcinogenic to humans ( group 1 ) and to identify additional tumour sites and mechanisms of carcinogenesis ( table and panel )  . 
these assessments will be published as part d of volume 100 of the iarc monographs.1 less alpha particles , consisting of two protons and two neutrons , are a densely ionising type of radiation with low capacity to penetrate living tissue ( less than 01 mm )  . 
 carcinogenicity of emit after the chernobyl accident , a sharp increase in the risk of thyroid cancer was found with exposure to radioiodines , particularly iodine - 131 , during childhood and adolescence.2 , 3 this increased risk might be due to higher milk intake per unit of body weight among children ; a higher thyroid dose per unit of iodine - 131 intake from milk ; a higher susceptibility per unit of thyroid dose ; or a combination of these . 
combined analyses of casecontrol studies now estimate that residential exposure to radon gas is the leading cause of lung cancer after tobacco smoke ( 815% attributable risk in europe and north america ) .4 , 5 gamma - rays and ionising are x - rays sparsely electromagnetic radiation that penetrate living tissue , typically producing fast electrons that deposit energy , resulting in tissue damage . 
extensive study of atomicbomb increased cancer risks at multiple anatomical sites.6 current evidence adds to the list of tumours caused by x - rays survivors shows and gamma - rays ( table ) , and also in - utero exposure establishes that increases the risk of cancer at multiple sites.7 , 8 the working group rea rmed the carcinogenicity of x - radiation and gamma - radiation ( group 1 )  . and traversed neutrons are produced by nuclear reactions and are a main component of cosmic radiation . 
however , the evidence of cancer in experimental animals is su cient , and mechanistic data show that neutrons transfer their energy in clusters of ionising events resulting in similar , but more severe , local damage than that induced by x - rays or gamma - rays . 
 each type of ionising radiation ( panel ) the transfers energy form of highly structured tracks of radiation type major study populations tumour sites ( and types ) on which su cient evidence is based alpha - particle and beta - particle emitters radon - 222 and decay products general population ( residential exposure ) , underground miners radium - 224 and decay products medical patients radium - 226 , radium - 228 , and decay products radium - dial painters thorium - 232 and decay products medical patients plutonium phosphorus - 32 plutonium - production workers medical patients fission products , including strontium - 90 general population , following nuclear reactor accident solid cancers , leukaemia radioiodines , including iodine - 131 children and adolescents , following nuclear reactor accident thyroid x - radiation or gamma - radiation atomic - bomb survivors , medical patients ; in - utero exposure ( o spring of pregnant medical patients and of atomic - bomb survivors ) lung bone lung , liver , bone acute leukaemia bone , paranasal sinus and mastoid process ( radium - 226 only ) liver , extrahepatic bile ducts , gall bladder , leukaemia ( excluding cll ) salivary gland , oesophagus , stomach , colon , lung , bone , skin ( bcc ) , female breast , urinary bladder , brain and cns , leukaemia ( excluding cll ) , thyroid , kidney ( atomic - bomb survivors , medical patients ) ; multiple sites ( in - utero exposure ) skin ( bcc , scc , melanoma ) skin ( melanoma ) , eye ( melanoma , particularly choroid and ciliary body ) solar radiation uv - emitting tanning devices general population general population cll = chronic lymphocytic leukaemia . 
scc = squamous - cell carcinoma . table : radiation exposures with su cient evidence in humans vol 10 august 2009 news monograph working group members b armstrongco - chair ( australia ) , e cardisco - chair ( spain ) ; a green ( australia ) ; d krewski , r mitchel , n priest ( canada ) ; l tomaek ( czech republic ) ; k baverstock ( finland ) ; j - f dor , j hall , l sabatier ( france ) ; m sokolnikov ( russian federation ) ; m hill , m little , m marshall , c muirhead , a riddell ( uk ) ; d brenner [ unable to attend ] , r guilmette , d hoel , d richardson , r ullrich ( usa ) con icts of interest np works for , and rm is a consultant to , atomic energy of canada ltd . 
 invited specialists none panel : types of radiation classi ed in group 1 ionising radiation alpha - particle emitters beta - particle emitters x - rays and gamma - rays neutron radiation solar radiation ultraviolet radiation ( wavelengths 100400 nm , encompassing uva , uvb , and uvc ) cell killing , ionisation and excitation events that can produce a variety of molecular lesions and clustered , complex dna damage.9 subsequent processing of this damage induces many responses chromosomal ( eg , aberrations , mutations , genomic instability , cell transformation , and bystander e ects ) that contribute to carcinogenesis . 
based on these mechanistic considerations , all types of ionising radiation were classi ed by the working group as carcinogenic to humans ( group 1 )  . solar radiation is the main source of human exposure to ultraviolet ( uv ) radiation , which is further subdivided into uva , uvb , and uvc . 
the working group rea rmed the carcinogenicity of solar radiation ( group 1 )  . exposure to solar radiation causes speci c mutation ngerprint ( cytidine to thymidine transition ) , as a result of cyclobutane pyrimidine dimers in dna . 
this pattern had long been attributed to uvb.10 however , this same cytidine to thymidine transition has been detected the skin of uva - treated mice11 and in the tp53 gene of uva - induced or uvb - induced skin tumours hairless mice.10 in humans , this is widespread transition has been seen in tp53 in premalignant solar keratosis and in malignant skin tumours.12 based on these mechanistic data , the working group classi ed uv radiation as carcinogenic to humans ( group 1 )  . the use of uv - emitting tanning devices in many developed countries , especially among young women . 
a comprehensive meta - analysis concluded that the risk of cutaneous melanoma is increased by 75% when use of tanning devices starts before 30 years of age.13 additionally , casecontrol several studies provide consistent evidence of a positive association between the use of uv - emitting tanning devices and ocular melanoma.14 , 15 therefore , the working group raised the classi cation of the use of uvemitting tanning devices to group 1 , carcinogenic to humans . 
 exposure , while reviewing the studies of occupational uv the working group concluded that there is su cient evidence for ocular melanoma in welders.16 , 17 however , because welders are also exposed to other harmful agents , this association could not be attributed speci cally to uv radiation . 
 fatiha el ghissassi , robert baan , kurt straif , yann grosse , batrice secretan , vronique bouvard , lamia benbrahim - tallaa , neela guha , crystal freeman , laurent galichet , vincent cogliano , on behalf of the who international agency for research on cancer monograph working group international agency for research on cancer , lyon , france the iarc authors declared no con icts of interest . grosse y , baan r , straif k , et al . 
bmj 2005 ; 330 : 223 . national research council , committee to assess health risks from exposure to low levels of ionizing radiation , board on radiation e ects , and research division on earth and life studies . 
 6 national research council , committee to assess health risks from exposure to low levels of ionizing radiation , board on radiation e ects , and research division on earth and life studies . 
uva1 genotoxicity is mediated not by oxidative damage but by cyclobutane pyrimidine dimers in normal mouse skj invest dermatol 2008 ; 128 : 228996 . 12 agar ns , halliday gm , barnetson rs , ananthaswamy hn , wheeler m , jones am . 
ophthalmology 2005 ; 112 : 1599607 . 752 vol 10 august 2009 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology aware of the di erence in standards of cancer care in the 1980s , 2 i applauded the introduction of an organisation that would provide evidence - based assessment of new technologies backed up by compulsory compliance by those holding the pursestrings to implement de nitive recommendations . 
so why does controversy still surround nice recommendations ? and why do many nd nice unhelpful ? nice cannot choose what they reviewa drug has to have a license for its use in certain settings before the institute can provide guidance . 
fair enough , but nice should have enough nous to know which drugs are likely to be political hot potatoes and to gather preliminary trial evidence to form a view without interference from the government as experienced for trastuzumab . 
this development has been exploited by some drug companies who fund support and information materials for patients , thus encouraging popular demand for a drug that might not be considered were these materials to come from the company directly . probably the biggest criticism is the time taken to produce guidance , especially when compared with the faster ( and cheaper ) scottish systethis delay , or nice blight as it is known , is being addressed by the expansion of the organisation and the introduction of singletechnology appraisals . 
currently costing 33 million a year , what will the institute cost when fully expanded ? other criticisms include the arbitrary gure of 20 00030 000 that nice has attached to a quality - adjusted life - year for the approval of drugs . 
a recent article by john appleby , 3 senior economist at the kings fund , and colleagues asks the question whether it is up to nice to set this gure . littlejohns and colleagues paper attests to the prodigious output of nice , and the institute has an impressively active press o ce . 
trying to contact nice for advice is , however , problematicthis may be the sign of an organisation that is growing fast and cant keep up with its adolescence , but nice must strive to be accessible and not aloof . 
where are the nice audits of the uptake of their guidance ? the cancer tsar , mike richards , has published three audits showing increasing adherence to nice guidance and narrowing of the inequality gap , but should this not be a role for nice ? where are the data on timely implementation of their recommendations ? nice inherited the service guidance reports and completed the set by publishing guidance on skin cancers . 
but are there plans to revisit them , or is the excitement of tackling new drugs too diverting ? where are the recommendations that might now be superseded by the development of new treatments ? in 2003 , the lancet oncology published an article by littlejohns and co - workers4 assessing nice then . 
we , as a society , have to decide the size of our health budget and where we want to send itnice provides guidance and should be encouraged to continue to do so impartially and speedily , and the government should undertake to fund these changing recommendations rather than expect already stretched nhs budgets to swallow them . so , happy birthday nicekeep polishing , avoid the tarnish , and try to engage more . richard sainsbury royal free and university college medical schools , london , uk r.sainsbury@ucl.ac.uk the author declared no con icts of interest . littlejohns p , garner s , doyle n , macbeth f , barnett d , longson c . 
on page 12 of this special report , the installation and calibration of a new particle accelerator at the toulouse - rangueil hospital , toulouse , france , was actually done by a physicist with assistance from brainlab . 
additionally , only 145 patients were treated ( not 5500 as stated ) , and all are currently being followed for any adverse e ects . 316 vol 10 april 2009 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper to the lancet go to thelancet / to submit a paper to the lancet oncology go to ees.elsevier.com / thelancetoncology / recommendations in light of the new data presented by raaijmakers and colleagues.3 piet dirix * , sandra nuyts department of radiation oncology , university hospitals leuven , leuven , belgium , piet.dirix@uzleuven.be the authors declared no con icts of interest . raaijmakers cp , roesink jm , dijkema t , houweling ac , terhaard ch . 
first results of a phase iii multicenter randomized controlled trial of intensity modulated ( imrt ) versus conventional radiotherapy ( rt ) in head and neck cancer ( parsport : isrctn48243537 ; cruk / 03 / 005 )  . 
proc am soc clin oncol 2009 ; 27 : abstr lba6006 . call for papersoncology and haematology the lancet and the lancet oncology are announcing plans for issues of each journal to be devoted to speci c topics in oncology and also to haematology . 
the former will be timed to coincide with the european society of medical oncology ( esmo ) congress in milan , italy ( oct 812 , 2010 ) , and the latter with the american society of hematology ( ash ) annual meeting in orlando , fl , usa ( dec 47 , 2010 )  . 
we would like to invite submissions of high - quality original research about cancers of the breast , lung , prostate , and gastrointestinal tract , or on any topic in haematology or haematological oncology . 
accepted papers will be published in either the lancet or the lancet oncology via fast - track peer review to coincide with either the esmo or ash annual meetings , as appropriate . 
 submissions to coincide with the esmo annual meeting must be received by june 25 , 2010 , and those for the ash annual meeting by oct 1 , 2010 , via either the lancet or the lancet oncologys online submission systems . 
please state in your covering letter that the submission is in response to this call for papers . if your work is being presented at either meeting and falls under an embargo policy , please tell us the date and time of the presentation , and whether the study is to be presented orally or in a poster . 
if your paper is accepted , online publication can be scheduled to coincide with the presentation and comply with any press embargo . jane godsland , zo mullan , richard turner , david collingridge the lancet ( jg , zm , and rt ) and the lancet oncology ( dc ) , 32 jamestown road , london nw1 7by , uk errata relling mv , altman rb , goetz mp , evans we . 
clinical implementation of pharmacogenomics : overcoming genetic exceptionalislancet oncol 2010 ; 11 : 50709the acknowledgment in this comment ( published online first on april 21 , 2010 ) should have read we thank colleagues in nihs pharmacogenomics research network . 
in the second paragraph , the last sentence was misspelt and should have read despite evidence linking pharmacogenomic variation with drug exposure , toxic e ects , and e cacy , many clinicians , regulators , and payors hold pharmacogenetic evidence to excessively high standards . 
lancet oncol 2010 ; 11 : 42938in this article , the acknowledgments statement should also have included : the uk medical research council funded the original all97 / 99 trial and supported the childhood leukaemia working party . 
lancet oncol 2007 ; 8 : 31722in this article , the equation for acpgbi in panel 2 should read loge [ r / ( 1r ) ] = ( 4859 + total score )  . 
additionally , in table 3 , 158 was added in error next to the heading clinicopathological staging . 516 vol 11 june 2010 articles assessment of an rna interference screen - derived mitotic and ceramide pathway metagene as a predictor of response to neoadjuvant paclitaxel for primary triple - negative breast cancer : a retrospective analysis of ve clinical trials nicolai juul * , zoltan szallasi * , aron c eklund * , qiyuan li , rebecca a burrell , marco gerlinger , vicente valero , eleni andreopoulou , francisco j esteva , w fraser symmans , christine desmedt , benjamin haibe - kains , christos sotiriou , lajos pusztai , charles swanton summary background addition of taxanes to preoperative chemotherapy in breast cancer increases the proportion of patients who have a pathological complete response ( pcr )  . 
however , a substantial proportion of patients do not respond , and the prognosis is particularly poor for patients with oestrogen - receptor ( er ) / progesterone - receptor ( pr ) / human epidermal growth factor receptor 2 ( her2 ; erbb2 ) - negative ( triple - negative ) disease who do not achieve a pcr . 
we previously identi ed genes involved in mitosis or ceramide metabolism that in uenced sensitivity to paclitaxel , with an rna interference ( rnai ) screen in three cancer cell lines , including a triple - negative breast - cancer cell line . 
we used area under the curve ( auc ) analysis and multivariate logistic regression to retrospectively assess the metagene in six cohorts of patients with triple - negative breast cancer treated with neoadjuvant chemotherapy ; two cohorts treated with paclitaxel ( n = 27 , 30 ) and four treated without paclitaxel ( n = 88 , 28 , 48 , 39 )  . 
 findings the metagene was associated with pcr in paclitaxel - treated cohorts ( auc 079 [ 95% ci 053093 ] , 072 [ 048090 ] ) but not in non - paclitaxel treated cohorts ( 053 [ 031077 ] , 059 [ 022082 ] , 053 [ 036071 ] , 064 [ 043081 ] )  . 
in multivariate logistic regression , the metagene was associated with pcr ( or 1992 , 26215157 ; p = 00039 ) with paclitaxel - containing chemotherapy . interpretation the paclitaxel response metagene shows promise as a paclitaxel - speci c predictor of pcr in patients with triple - negative breast cancer . 
these results highlight the potential for functional genomics to accelerate development of drug - speci c predictive biomarkers without the need for training clinical trial cohorts . funding uk medical research council ; cancer research uk ; the national institutefor health research ( uk ) ; the danish council for independent research - medical sciences ( fss ) ; breast cancer research foundation ( new york ) ; fondation luxembourgeoise contre le cancer ; the fonds national de la recherche scienti que ; brussels region ( irsib - ip , life sciences 2007 ) and walloon region ( biowin - keymarker ) ; sally pearson breast cancer fund ; and the european commission . introduction despite the use of modern cytotoxic agents , the proportion of patients who achieve a complete pathological response ( pcr ) to preoperative chemotherapy remains low , at 1525% for all breast - cancer histopathological subtypes.1 rates of pcr in sporadic oestrogen - receptor ( er ) / progesterone - receptor ( pr ) / human epidermal growth factor receptor 2 ( her2 ; erbb2 ) - negative ( triple - negative ) breast cancer range from 12% for taxane monotherapy to 45% with combination neoadjuvant chemotherapy regimens.24 patients who achieve a pcr after chemotherapy have excellent disease - free and overall survival.1 the outcome for patients who do not achieve a pcr varies , and the prognosis for patients with triple - negative cancers and residual disease after preoperative chemotherapy is particularly poor.2 better understanding of breast - cancer biology is likely to expand the list of potentially e ective chemotherapeutic agents in the neoadjuvant setting , and will help identify tailored chemotherapy schedules for distinct patient cohorts based on tumour molecular characterisation . 
if it can be reliably established that patients resistant to one type of therapy are sensitive to a di erent agent , then robust predictors of chemotherapy response will have an essential role in selecting the optimum treatment in the neoadjuvant setting . 
predictive geneexpression signatures derived from an associative analysis approach are susceptible to chance associations which lead to overestimation of true clinical accuracy ; therefore , two separate trial cohorts are required to train and validate the predictive signature.5 , 6 associative strategies developed from genomics signatures that are predictive of drug response in cell lines might circumvent the need for training and validation of trial cohorts.7 quantifying distinct biological processes within gene - expression datasets , instead of a gene - by - gene based associative analysis , may further avoid these problems and accelerate biomarker development.8 however , potentially relevant biological processes or functional modules must be identi ed in advance for such an analysis to be possible . 
to test this hypothesis , we revisited results of our previous study9 of an rnai drugresistance screen across three cancer cell lines , including a triple - negative breast - cancer cell line , mda - mb - 231 . 
in this screen , we identi ed two distinct gene sets regulating sensitivity to paclitaxel.9 the rst set of genes is involved in mitosis and the mitotic spindle assembly checkpoint ( sac ) , and the second set is involved in metabolism of the proapoptotic lipid , ceramide . 
 an activated sac orchestrates a paclitaxel - induced mitotic arrest , and in our rnai screen , silencing several genes implicated in sac control impaired the accumulation of cells in mitosis and subsequent cell death in response to paclitaxel . 
identi cation of ceramide pathway genes as regulators of paclitaxel sensitivity9 is consistent with published evidence that overexpression of glucosylceramide synthase ( ugcg ) promotes resistance to paclitaxel and repression promotes paclitaxel sensitivity.1012 we created a metagene using established methodology8 , 13 to quantify the activity of these two biological pathways identi ed by our rnai screen , and tested its paclitaxelpredictive value in patients with triple - negative breast cancer who were treated in clinical trials with either a paclitaxel - containing combination regimen , t - fac ( paclitaxel followed by uorouracil , doxorubicin , and cyclophosphamide ) or by regimens without paclitaxel . methods patients and procedures treatment - response data were gene - expression and retrieved from six cohorts in ve neoadjuvant clinical trials , referred to in this study as mda1 , mda / maqc - ii , top , eortcfec , eortctet , and dfci . 
 * * triple - negative breast cancer subtype inferred by expression when insu cient data by immunohistochemistry / fish . table 1 : clinical and histopathological characteristics of the cohorts analysed vol 11 april 2010 articles rna interference a mechanism by which small double - stranded rnas can reduce expression of any mrna having a similar sequence . 
two clinical trial cohorts were treated with paclitaxel - containing regimens ( t - fac ) : the mda1 cohort14 and the mda / maqc - ii cohort ( geo accession number gse16716 )  . 
patients in the top cohort ( gse16446 ) were treated with neoadjuvant epirubicthe gene expression substudy of the eortc 10994 trial7 , 8 randomised patients to fec ( uorouracil , epirubicin , and cyclophosphamide ) or tet ( docetaxel followed by epirubicin and docetaxel ) , corresponding to the eortcfec ( gse6861 ) and eortctet ( gse4779 ) subgroups , respectively . 
in the dfci cohort ( gse18864 ) , triple - negative patients were treated with neoadjuvant cisplatin.15 patient characteristics for all cohorts are summarised in table 1 , and characteristics for the subset of patients with triple - negative disease are shown in the webappendix p 1 . 
in addition , we identi ed three genes from the ceramide pathway ( col4a3bp , gba1 , gba3 ) that together with the published gene ugcg , 1012 encode proximal regulators of ceramide metabolism and in uence paclitaxel sensitivity . 
of these 14 genes ( gure 1 ) , six mitotic genes and three ceramide genes could be assayed on the a ymetrix hgu133a platform , and these were combined into the mitotic and the ceramide gene sets . 
 the number of genes within each gene set was further reduced to the mitotic module ( four genes ) and the ceramide module ( two genes ) by only including genes that were signi cantly correlated with each other across four independent breast cancer datasets.1619 the expression of the genes within each module was compressed by taking the mean . 
since the two modules were expected to predict direction ( high mitotic expression = sensitivity , high ceramide expression = resistance ) , the paclitaxel response metagene was de ned as the mitotic module minus the ceramide module . 
as a comparison , 10 000 random combinations of nine - gene sets were subjected to the same correlative approach , across four clinical datasets , and the mean expression of signi cantly correlated genes were tested for their ability to predict pcr in t - fac - treated cohorts . 
these genes were subjected to the same correlation analysis as the paclitaxel response metagene , and the reported direction of expression relating to paclitaxel sensitivity was included as weights ( minus 1 if the gene induced sensitivity when repressed , 1 if the gene induced sensitivity when overexpressed )  . 
the genomic grade index and the stroma signatures were calculated as described previously.8 , 20 sensitivity opposite the statistical analysis a binomial test was used to test for enrichment in genes that predicted response to treatment with paclitaxelcontaining neoadjuvant chemotherapy , among the genes that substantially a ected paclitaxel sensitivity across three cell lines . 
the signi cance of association between module or metagene scores and pcr was estimated with the one - sided wilcoxon signed - rank test and plotted with receiver operating characteristics curves . 
we used a one - sided wilcoxon test because we had a prior expectation about the direction of association , based on the rnai screening results.9 the e ect size was estimated with auc and logistic regression . 
since the mda1 and mda / maqc - ii trials were done by the same investigators , at the same site , with identical geneexpression platforms , we combined the two t - fac figure 1 : process to derive the paclitaxel response metagene ( a ) flow chart describing the derivation of the gene modules and the paclitaxel response metagene . 
 ( b ) proximal regulators of the proapoptotic lipid , ceramide , that alter paclitaxel sensitivity through conversion to sphingomyelin ( via col4a3bp ceramide transporter ) or glucosylceramide ( ugcg glucosylceramide synthase ) and conversion of glucosylceramide to ceramide ( gba1 and gba3 beta - glucosidase )  . 
 role of the funding source the funding sources and sponsors of the trials had no role in the design of the study ; collection , analysis , or interpretation of the data ; or writing of this report . 
the corresponding author had full access to all data and had the nal responsibility to submit for publication . results to develop an analytical framework based on experimentally established functional links instead of associative correlations , we revisited our previously published functional genomic rnai screen that identi ed genes which either promote resistance or sensitivity to paclitaxel.9 based on this screen and previously published data , we identi ed two gene modules of tightly correlated genes : a four - gene mitotic module where higher expression predicted sensitivity , and a two - gene ceramide module where higher expression predicted resistance . 
we then used the mean expression of the genes within each module as a single predictive value ; an approach previously improve reliability across many tumour shown to samples.8 , 13 finally , we combined the mitotic and ceramide modules into a single functionally derived paclitaxelresponse metagene by subtracting the mean expression of the genes in the ceramide module from the mean expression of the genes in the mitotic module ( gure 1 )  . 
 therefore , this summary measure re ects the di erence in the mean expression of the two modules and is predicted to correlate with paclitaxel sensitivity . in the t - fac treated triple - negative cohorts , the paclitaxel response metagene was highly predictive of pcr , with an auc of 079 in mda1 ( p = 00053 ; 95% ci 053093 ; n = 27 ) , an auc of 072 in mda / maqc ( p = 0031 ; 048090 ; n = 30 ) , and an auc of 074 when the two cohorts were combined ( p = 00013 ; 058086 ; n = 57 ; table 2 , gure 2 a and b , webappendix p 2 )  . 
 consistent with these data , the paclitaxel response metagene was also predictive of response across all patients in each cohort : for mda1 , auc was 079 ( p < 00001 ; 069087 ; n = 133 ) ; for mda / maqc - ii , auc was 076 ( p = 000061 ; 061087 ; n = 100 ) ; and for the combined cohort , auc was 077 ( p < 10 ; 069084 ; n = 233 ; data not shown )  . measurements of gene expression in the cohorts treated with neoadjuvant paclitaxel were consistent with in - vitro functional observations ; repression of genes in the mitotic module was associated with resistance to t - fac therapy , and repression of genes in the ceramide module was associated with sensitivity to t - fac . 
these values predict resistance to paclitaxel , all others predict sensitivity . table 2 : association between gene sets and treatment response for all patients and for triple - negative patients for each cohort vol 11 april 2010 mitotic module ceramide module paclitaxel response metagene articles 070 065 * 079 050 055 * 053 063 * 064 064 * 1specicity 1specicity figure 2 : receiver operating characteristic ( roc ) curves for the gene modules and the paclitaxel response metagene roc curve in triple - negative patients in the t - fac - treated cohorts mda1 ( a ) and mda / maqc - ii ( b ) , the epirubicin - treated top cohort ( c ) , the fec - treated eortc cohort ( d ) , the tet - treated eortc cohort ( e ) , and in the cisplatin - treated dfci cohort ( f )  . 
these data suggest that the concordance of the functional genomic and clinical trial genomics datasets is unlikely to result from a chance association . for multivariate analysis , we combined the two t - factreated mda1 and mda / maqc - ii cohorts to increase 063 067 * 072 054 050 * 053 057 056 * 059 statistical power . 
we found that the paclitaxel response metagene was the covariate most signi cantly associated with pcr ( p = 00039 ; odds ratio 1992 ; 95% ci 26215157 ) in t - fac - treated patients with triple - negative breast cancer , more than nodal status , t stage , tumour grade , and ki67 ( table 3 )  . 
the paclitaxel response metagene also did better than the genomic grade index and the stroma signature in both univariate and multivariate analysis of the combined t - fac clinical trials , when all patients were considered and in the triple - negative cohorts ( table 4 ) .8 , 20 these data support the conclusion that the paclitaxel response metagene derived from an rnai screen has predictive power in two paclitaxel clinical trial cohorts that had no role in the discovery of the genes included in the metagene . 
the response metagene was not signi cantly associated with recurrence - free survival in two untreated triple - negative breast cancer cohorts , indicating the predictive rather than prognostic power of the metagene ( webappendix p 4 ) .16 , 18 to further validate the functional importance of the genes contained within the metagene and limit the possibility that the correlation step would arti cially enrich for genes predictive of pcr , we tested the ability to predict for pcr of 10 000 random nine - gene sets subjected to the same correlative approach . 
we addressed the relevance of the rnai screening process to select genes for inclusion in the metagene by performing the same analysis with 24 genes reported to be associated with paclitaxel or docetaxel resistance . 
 although the nine - gene set ( gure 1 ) selected before the expression correlation step was still predictive of pcr with t - fac , this gene set did not do as well as the paclitaxel response metagene . 
 to assess the paclitaxel speci city of the paclitaxel response metagene , we assessed its predictive power in four cohorts that did not receive paclitaxel ( table 1 , webappendix p 5 ) : the eortc 10994 fec trial cohort , eortc 10994 tet trial cohort , the top epirubicin trial cohort , and the triple - negative dfci cisplatin - treated cohort . 
the triple - negative tumours analysed were somewhat homogeneous ( re ecting the neoadjuvant setting of these trials ) , with similar nodal status , t stage , and were higher grade tumours ( webappendix p 5 ) , indicating that tumour heterogeneity is unlikely to account for this result . triple - negative subtype the 362 vol 11 april 2010 articles using a meta - analysis , we combined the odds ratios of the paclitaxel response metagene to pcr in the two paclitaxel - treated cohorts and in the four non - paclitaxel treated cohorts . 
we found that the summary odds ratio of the paclitaxel treated cohorts was 565 ( 95% ci 1671911 ; p = 00053 ) , whereas the summary odds ratio of the non - paclitaxel ( 95% ci 044 to 167 ; p = 067 ) , consistent with improved predictive power of the paclitaxel response metagene in paclitaxel treated cohorts ( gure 3 )  . 
 treated cohorts was 087 finally , we combined paclitaxel - treated with nonpaclitaxel - treated triple - negative cohorts and did logisticregression analysis using a mixed e ects model , considering paclitaxel treatment , binary metagene status , interaction . 
we observed a signi cant and interaction term between paclitaxel treatment and binary metagene status ( or 59 , 95% ci 1612318 ; p = 00089 ) , indicating that the paclitaxel response metagene has paclitaxel - speci c predictive power . their discussion this study supports the use of high - throughput rnai functional genomics screening to accelerate discovery of predictive biomarkers in cancer medicine . 
by ltering for common paclitaxel resistance pathways through rnai screening across three cell lines of di erent tumour origin , and selecting genes which correlate across independent cohorts , we derived a paclitaxel response metagene that is predictive of t - fac response in two clinical trial datasets , but not in cohorts treated without paclitaxel . 
data reported here support a model whereby expression of genes that regulate mitotic arrest and chromosomal stability , mediated through spindle assembly checkpoint signalling , and genes that in uence ceramide conversion to sphingomyelin or glucosylceramide , are associated with altered response to t - fac therapy in vivo ( gure 4 ) .9 , 21 since the metagene was derived from an rnai screen in a triple - negative breast - cancer cell line , we investigated the power of the metagene to predict response to paclitaxel in clinical trials that include patients with this histological subtype . 
the patient demographics in the four nonpaclitaxel trials included in this study are typical of the neoadjuvant setting and similar to mda1 and mda / maqcii , with a bias towards node positive , higher grade ( g2g3 ) and larger tumours ( t2 and above ) , indicating that tumour heterogeneity across the trial cohorts is unlikely to contribute to the observed results . 
however , although the paclitaxel response metagene performs better than the genomic grade index and the stromal signature in multivariate analysis , both of which have predictive value in patients treated with t - fac , 8 , 20 the aucs reported in the mda1 cohort result in false negatives and denial of active therapy in two of 13 ( 15% ) of the responding patients , to spare suboptimal treatment in ten of 14 patients with resistant disease . 
a false negative proportion of one in univariate analysis multivariate analysis oestrogen receptor 0084 ; 004019 ; < 00001 * 018 ; 007047 ; 000039 * 384 ; 184801 ; 000037 * 235 ; 101547 ; 0048 * 107 ; 055208 ; 084 360 ; 179723 ; 000032 * 624 ; 2771404 ; < 00001 * 242 ; 107548 ; 0034 * 728 ; 3231641 ; < 00001 * 079 ; 026244 ; 068 079 ; 027229 ; 066 346 ; 0671783 ; 014 346 ; 0671783 ; 014 067 ; 029152 ; 034 117 ; 045307 ; 075 199 ; 073544 ; 018 198 ; 077506 ; 015 179 ; 056570 ; 032 039 ; 009160 ; 019 010 ; 001080 ; 0030 * 659 ; 0765736 ; 0088 962 ; 1029028 ; 0048 * all patients her2 t stage ki67 grade node t stage ki67 grade node metagene triple - negative metagene 451 ; 1411443 ; 0011 * 1992 ; 26215157 ; 00039 * data are odds ratio ; 95% ci ; p value . 
tet = docetaxel followed by epirubicin and docetaxel . 13 ( 8% ) would be possible by sacri cing speci city , resulting in the sparing of suboptimal therapy in seven of 14 patients with resistant disease . 
 conversely , decreased levels of the ceramide transporter , col4a3bp ( cert ) , and glucosylceramide synthase , ugcg , may lead to an increase in the ceramide pool and potentiate paclitaxel - induced cytotoxicity . performance of the paclitaxel response metagene approach might be improved through gene selection from genomewide rnai screening approaches targeting more than 21 000 genes across multiple cell lines , by contrast with the 829 genes assessed in this study . sources of random and systematic error should be considered when interpreting these data . 
although no patients enrolled in the t - fac trials were known to have germline brca mutations , the same dna repair - pathway mechanisms may be disrupted in sporadic breast cancers that have also been implicated in taxane resistance in vitro.22 , 23 also , it should be noted that the t - fac clinical trial datasets were acquired from ne needle aspirations whereas the nonpaclitaxel datasets were acquired from core biopsies . 
rna yield and expression pro ling are similar using both techniques , 24 but we cannot exclude the possibility that the enrichment of stromal elements in the core biopsy datasets contribute to the lack of predictive power of the paclitaxel response metagene . 
the ve trials examined here varied in chemotherapy exposure from 12 to 24 weeks , and two trials used monotherapy schedules that might a ect the proportion of patients achieving a pcr . 
while these results support the rnai approach to biomarker discovery and argue against the role of chance in these ndings , the modest cohort sizes and the heterogeneity of the nonpaclitaxel trials require replication in larger prospective studies to con rm the relevance of this method with a clinically applicable gene - expression assay . 
experience with the oncotype dx assay has shown that rna - based expression measurements ( real - time pcr ) from para nxed tumour material can inform clinical decision making . 
with this assay , exact thresholds of mitotic and ceramide module expression should be de ned retrospectively with tumours from the t - fac trial before testing the de ned threshold in a prospective trial . 
a randomised clinical trial comparing a paclitaxel with a non - paclitaxel regimen will be required to formally support the paclitaxel - speci city of the metagene and the relevance of rnai to the biomarker discovery process . 
the usefulness of this approach in routine clinical practice should then be assessed , since patients enrolled in clinical trials may not accurately re ect the demographics and clinical stage of patients diagnosed with primary breast cancer . 
 notably , the paclitaxel response metagene was not predictive of pcr in the eortctet cohort ( docetaxel then epirubicin and docetaxel ) , which may be explained by the non - overlapping pathways of drug resistance to the two taxanes . 
the metagene was derived from a screen to identify mediators of paclitaxel not docetaxel resistance across three cell lines , and preclinical data has shown that docetaxel binds to - tubulin with greater a nity than paclitaxel and has increased interphase ( g1 / s / g2 ) cell - cycle activity , mediating cell death through the induction of bcl2 phosphorylation.25 , 26 finally , 1931% of patients respond to paclitaxel having progressed on or after docetaxel , 27 , 28 supporting the divergent drugresistance mechanisms of these two taxanes . we cannot be certain that the paclitaxel response metagene is paclitaxel speci c , despite the test for interaction , since silencing of col4a3bp and ugcg has been shown to promote doxorubicin sensitisation.9 , 29 consistent with this hypothesis , we note that the paclitaxel response metagene is weakly predictive of pcr in the eortcfec dataset across all patients ( auc 062 ; 95% ci 049072 ; p = 0025 )  . 
the ceramide module is likely the main contributor , since col4a3bp expression alone predicts for pcr in all patients ( 059 ; 048071 ; p = 0061 ) ; this would support the role of the ceramide pathway in the regulation of multidrug sensitivity in vivo . in summary , we used in - vitro functional genomics analyses to guide the development of a metagene to predict paclitaxel response in patients with breast cancer . 
 although we cannot conclude that our approach is better than associative predictive strategies , the latter strategy 364 vol 11 april 2010 articles requires training of two large cohorts and validation of such signatures . 
the functional genomics approach used in this study could be an e cient method to accelerate biomarker development for experimental therapies in single - cohort early phase clinical trials , where strati cation of response according to tumour expression of a functional metagene could be considered . contributors nj , zs , and csw designed the study and the research concept . 
the top trial was supported by the fondation luxembourgeoise contre le cancer , the fonds national de la recherche scienti que , brussels region ( irsib - ip , life sciences 2007 ) and walloon region ( biowin - keymarker ) , and the european commission ( fp6 - 2005 - ist - 026996 )  . 
national data on cancer patient survival in england and wales up to 2007 thus o er the opportunity for a rst formal assessment of the cancer plan in england , by comparing survival trends in england with those in wales before , during , and after the implementation of the plan . methods we analysed population - based survival in 22 million adults diagnosed with one of 21 common cancers in england and wales during 19962006 and followed up to dec 31 , 2007 . 
we estimated year - onyear trends in 1 - year relative survival for patients diagnosed during each period , and changes in those trends between successive periods in england and separately in wales . 
life tables for single year of age , sex , calendar year , deprivation category , and government o ce region were used to control for background mortality in all analyses . findings 1 - year survival in england and wales improved for most cancers in men and women diagnosed during 19962006 and followed until 2007 , although not all trends were signi cant . 
northsouth di erences in survival trends for the four most common cancers were not striking , but the north west region and wales showed the smallest improvements during 200103 and 200406 . interpretation the ndings indicate slightly faster improvement in 1 - year survival in england than in wales during 200406 , whereas the opposite was true during 200103 . 
these di erent patterns of survival suggest some bene cial e ect of the nhs cancer plan for england , although the data do not so far provide a de nitive assessment of the e ectiveness of the plan . funding o ce for national statistics ( contract nt - 04 / 2355a ) ; cancer research uk ( programme grant c1336 / a5735 )  . introduction in 1995 , the expert advisory group on cancer published the calman - hine report , 1 in which they recommended that strategic improvements be made to cancer services in england and wales . 
by 1999 , progress in improving cancer services was seen as inadequate.2 the national health service ( nhs ) cancer plan for late 2000.3 it was a england was published comprehensive 10 - year strategy , designed to improve prevention , early diagnosis , and screening , and to provide optimal thus improving survival and quality of life . 
 annual funding for cancer services rose by about 35% in real terms over the three nancial years from 2001 to 2004 . in wales , the cancer services expert group recommended substantial changes to cancer services in 1996.4 changes included the creation of mdts and the designation of specialist clinicians , but the approach relied heavily on clinical collaboration , supported by directives from the devolved administration , rather than on a formal strategy . 
the full national cancer plan for wales , designed to tackle cancer , 5 was not published until late 2006 . 3 - year progress reports on the nhs cancer plan were published in october , 2003 , 6 , 7 when , despite substantial progress , it was acknowledged that it would take time vol 10 april 2009 articles the di culty of before the e ects of the plan could be assessed . 
 given introducing systematic , nationwide changes in the nhs , it would be surprising if survival trends for patients diagnosed in england during 200103 were to di er much from earlier trends as a direct result of the plan . 
however , for patients diagnosed during 200406 , at least 3 years after implementation of the plan , any marked improvements in the overall e ectiveness of cancer services might reasonably be expected to show an e ect on trends in short - term survival . given the later implementation of a strategic cancer plan in wales , comparison of survival trends in england and wales over the same calendar periods could be instructive . 
but an observational comparison of outcomes before and after the introduction of a plan in one of two adjacent countries , with similar societies and health systems , seemed to be a reasonable alternative . 
1 - year survival trends might be expected to accelerate more rapidly in successive calendar periods in england than in wales after the introduction of the plan , if the plan was e ective . 
3 - year survival trends might also be di erent in england and wales . on dec 10 , 2008 , the o ce for national statistics ( ons ) published the o cial national statistics on survival for patients diagnosed with one of 21 common cancers in england during 200004 and followed up to 2005.8 national statistics on survival for cancer patients diagnosed in england during 200106 and followed up to dec 31 , 2007 , were published on march 20 , 2009.9 we have used these data , and the data for all cancer patients diagnosed in wales , to study national and regional trends in survival up to the end of 2007 . methods data collection population - based cancer registries collect a small standard dataset for all cancer patients in a de ned population . 
since 1971 , the national health service central register ( nhscr ) has provided noti cation of the deaths of all cancer patients whose record was successfully agged with details of the initial cancer registration . data for this study were extracted from the national cancer registry at the ons after the linkage of cancer records with data on the patients vital status ( alive , emigrated , dead , not traced ) at nhscr . 
after powers to legislate on health policy were devolved to uk national assemblies from 1997 , cancer registration in wales passed to the welsh cancer intelligence and surveillance unit , but the national cancer registry at the ons continues to receive cancer data from wales , and the vital status of all cancer patients in england and wales is updated by the ons . 
when the data were extracted on oct 17 , 2008 , the vital status at dec 31 , 2007 , was known for 996% of patients diagnosed with cancer during 19962006 , without regional variation . 
the data were received on dec 15 , 2008 . cancers were de ned by their anatomical location ( site ) , morphology , and behaviour ( benign , in situ , or invasive )  . 
tumour site was coded according to the tenth revision of the international classi cation of diseases ( icd - 10 ) .10 morphology and behaviour were coded according to the second edition of the international classi cation of diseases for oncology ( icd - o - 2 ) .11 we examined data for 21 common cancers , 17 in men and 18 in women . 
 standard criteria were used to decide whether a tumour record was eligible for inclusion in the analyses.12 records were excluded if they contained data of inadequate quality or were for patients not resident in england or wales . 
125 million of 84 million patients registered with benign tumours ( behaviour code 0 ) , tumours of uncertain behaviour ( code 1 ) , in - situ neoplasms ( code 2 ) or a metastasis ( code 6 ) were not included . 
of 7 043 765 patients with an invasive primary malignancy eligible for survival analysis during 19712006 , 6 436 299 ( 914% ) had one of the 21 cancers selected for analysis , of whom 2 338 785 were diagnosed during 19962006 . 
62% of patients were excluded because their survival was either zero or unknown ( tumour registered from a death certi cate only [ dco ] ) , and 14% of patients were excluded because of unknown vital status or sex , duplicate registration , synchronous tumours , or invalid dates or sequences of dates . 
 352 vol 10 april 2009 articles the government o ce regions of england have provided a geographic focus for public - health policy in england since 1999 , and have been closely linked with the new nhs strategic health authorities since 2006.13 we analysed the cancer data for each region , for england as a whole , and separately for wales . statistical analysis survival trends were quanti ed as the year - on - year rate of change within each calendar period . 
the di erence in survival trends between successive calendar periods provides a measure of any acceleration ( or deceleration ) in the rate of change in survival between successive periods . 
di erences or trends are given as the simple arithmetic values ; so 12% is reported as 2% ( not 20% ) higher than 10% , and a rise from 10% to 14% over 4 years is reported as an increase of 1% per year . we estimated relative survival for england , for wales , and for the nine government o ce regions of england , for each cancer , each sex , and by year or period of diagnosis . 
relative survival is the ratio of the observed probability of survival and the probability that would have been expected if the cancer patients had only experienced the normal ( background ) mortality of the general population in which they live , 14 , 15 given the same distribution of factors such as age , sex , geographic area , calendar period , and deprivation . 
it does not rely on accurate reporting of the cause of death , 16 and it enables the estimation of longterm survival from cancer , when competing causes of death become more important.17 it can be interpreted as survival from cancer after adjustment for other causes of death . expected survival is derived from population life tables . 
background mortality rates by age and sex di er widely between socioeconomic groups and geographic regions in england and wales , 18 and these di erences have changed over time . 
we therefore constructed life tables ( available online19 ) of all - cause death rates by single year of age ( 099 years ) , sex , deprivation category , and government o ce region for 1991 , 2001 , and 2005 , using the mid - year population estimates and the mean annual number of deaths during the 3 years centred on the index year . 
life tables for 2006 and 2007 could not be constructed because the relevant data ( deaths during 200708 ) were unavailable , so life tables for 2005 were used for those years without extrapolation . 
national and regional analyses for england were all done with life tables speci c for sex , government o ce region , deprivation category , and calendar year from 1996 . five deprivation categories were de ned from quintiles of the income domain score of the indices of multiple deprivation ( imd2004 ) , 20 and the equivalent indices for wales , 21 using administrative data for the icd - 10 * code exclusions ( % ) eligible for analysis number of patients included ( % ) dco zero survival other c19c21 c33 , c34 c54 , c55 c56 , 570577 c64c66 , c68 71 205 88 637 213 077 125 458 70 897 17 281 366 597 74 004 411 299 29 077 59 567 66 383 300 301 18 679 63 650 112 712 39 220 13 655 oesophagus stomach colon rectum pancreas larynx ( men ) lung melanoma breast ( women ) cervix uterus ovary prostate testis kidney bladder brain hodgkins disease non - hodgkin lymphoma myeloma leukaemia c91c95 total 36 866 67 034 2 338 785 106 66 829 ( 939 ) 81 517 ( 920 ) 195 108 ( 916 ) 120 023 ( 957 ) 59 272 ( 836 ) 16 624 ( 962 ) 323 157 ( 882 ) 71 935 ( 972 ) 384 442 ( 935 ) 27 998 ( 963 ) 57 306 ( 962 ) 61 385 ( 925 ) 284 310 ( 947 ) 18 194 ( 974 ) 57 536 ( 904 ) 107 398 ( 953 ) 36 171 ( 922 ) 13 305 ( 974 ) 33 865 ( 919 ) 59 692 ( 890 ) 2 163 274 ( 925 ) c82c85 93 186 87 207 ( 936 ) all patients were aged 1599 years . 
aged 100 years or over at diagnosis , vital status or sex unknown , sex - site error , invalid dates , duplicate registration , synchronous tumours , or a previous cancer of the same organ or tissue at some time since 1971 . table 1 : number of patients eligible and included for analysis , and percentage exclusions , for adults diagnosed with one of 21 common cancers in england and wales between 19962006 and followed up to 2007 lower super - output areas ( lsoas , mean 34 378 population 1500 ) 22 in england ( 2001 ) and wales ( 200204 )  . 
cancer patients were assigned to the deprivation category of their lsoa , using the postcode of residence at diagnosis and a combined historic le of 21 million unique full postcodes , each linked to a complete set of geographic area codes for each year that the postcode was active . 
death records were assigned to deprivation categories using the postcode and lsoa in the same way as the cancer cases , so that background mortality was precisely matched to the small areas of residence and deprivation categories of the cancer patients . 
although socioeconomic inequalities ( the socalled deprivation gap ) in survival have been widening for many adult cancers in england and wales , 23 tending to reduce the overall national gain in survival , recent trends in the deprivation gap in survival will be reported separately . survival probabilities were estimated at short ( for example , 1 - month ) intervals in the rst few months vol 10 april 2009 articles calendar years within which follow - up probabilities are used to estimate survival 1996 1997 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 1996 1997 1998 1999 2000 2001 2002 2003 2004 2005 2006 survival data used in cohort analysis survival data used in hybrid analysis 1996 1997 1998 1999 2000 2001 2002 2003 2004 2005 2006 survival data used in complete analysis figure 1 : structure of survival analyses in relation to nhs cancer plan , patients diagnosed 19962006 and followed up to 2007 numbers in the cells indicate the minimum number of years of follow - up completed by patients surviving to the end of a given calendar year ( columns ) who were diagnosed in the index year ( rows )  . 
conditional 5 - year survival is restricted to those who had survived at least 1 year ; ie , excluding follow - up in shaded cells . after diagnosis , then at progressively longer intervals up to 10 years after diagnosis , using the maximumlikelihood approach for individual data.24 we report the cumulative probabilities of relative survival at 1 , 3 , 5 , and 10 years after diagnosis . 
we also report 5 - year survival for patients who survived at least 1 year after their diagnosis ( conditional survival )  . given the structure of the data , various analytical approaches were required . 
the classical ( cohort ) approach was suitable for the analysis of year - on - year trends in 1 - year survival , since all patients were followed up at least that long ( gure 1 )  . 
short - term prediction of survival for patients diagnosed during 2007 was made with the hybrid approach , 25 combining the 1 - year survival probability for patients diagnosed during 2006 with the survival probabilities for the second and later years after diagnosis for patients who were alive and followed up for at least part of 2007 . 
conditional 5 - year survival was available with the cohort approach for 19962000 , the complete approach for 200103 , and the period approach26 for 200406 ( gure 1 )  . year - on - year trends in survival were estimated within a single variance - weighted linear regression27 model covering all 11 years and each calendar period , including two extra parameters in addition to the baseline trend , to allow for di erent trends in successive periods . 
we report changing survival trends as the absolute di erence between the regression slopes for each calendar period : a positive value implies acceleration of the upward trend in survival and a negative value implies deceleration ( see webappendix )  . 
 survival analyses were done with the publicly available stata program strel.28 other analyses were programmed in stata version 10.29 we constructed funnel plots30 to visualise the regional variability of 1 - year survival in england and wales for cancer patients diagnosed during 200406 . 
the plots allowed us to estimate how much a particular estimate of survival deviates from the pooled england value ( the target ) , given the precision of each estimate . 
the target value , taken as the estimate of 1 - year relative survival pooled across the nine regions of england for all patients diagnosed during 200406 , is represented by the horizontal line in each plot . 
the 95% and 998% control limits , derived from the complementary loglog transformation of the target estimate for england across the observed range of precision of the regional estimates , 31 represent approximately three standard deviations , respectively , from the target value at each level of precision ( webappendix )  . 
estimates that lie inside the control limits were considered as within the geographical variation that could be expected by chance . two and funnel plots were also constructed to show regional variation in the year - on - year trend in 1 - year survival during 200406 . 
the target value in each plot was set as the mean absolute change per year between the 1 - year relative survival estimates for all patients in england diagnosed in the single years 2004 , 2005 , and 2006 . 
the control limits were constructed on the assumption that the target value for the year - on - year change in survival follows a normal distribution ( see webappendix )  . this analytical strategy , including de nition of the calendar periods , the cancers , life tables , approaches to estimation of survival and survival trends , and the structure of the tables and graphics , was speci ed in advance , after data preparation was complete but before the start of any analyses . 
this was done to pre - empt any concerns regarding possible data - dredging in favour of a particular conclusion , whether for or against the e ectiveness of the nhs cancer plan . legal authority to hold the cancer data derives from a contract with the ons to produce the o cial national statistics32 on cancer survival . 
approval to analyse the data was obtained from the ons medical research service ( mr1101 , nov 20 , 2007 ) and from the statutory patient information advisory group ( piag ; now the ethics and con dentiality committee of the national information governance board ) under section 61 of the health and social care act 2001 ( piag 1 - 05 ( c ) / 2007 , july 31 , 2007 )  . 
the cancer survival group ( br , un , mq , le ) at the lshtm has been funded by cancer research uk ( grant c1336 / a5735 ) since april , 2005 . 
neither cancer research uk nor the ons had any role in study design , data collection , analysis , interpretation of the data , or the writing of this article . 
the corresponding author had full access to all the data and the nal responsibility to submit for publication . results 1 - year survival improved for most cancers in patients diagnosed during 19962006 and followed until 2007 , for both sexes and in england and wales . 
for patients diagnosed in 2006 , 1 - year survival was over 60% for 25 of the 35 cancersex combinations , both in england and wales ( table 2 )  . 
for cancers of the oesophagus , stomach , pancreas , lung , and brain , 1 - year survival was poor , in the range 1520% ( pancreas ) and rarely over 40% , despite noticeable improvement for some cancers ( oesophagus , stomach , brain among men in england , oesophagus in wales )  . 
table 2 summarises temporal trends in 1 - year survival , both for the entire period 19962007 and in each of the three calendar periods . for patients diagnosed in england during 19962000 , before the nhs cancer plan , 1 - year survival increased signi cantly ( p < 005 ) for eight of 17 cancers in men and for 12 of 18 cancers in women . 
the annual increase was about 1% for cancers of the oesophagus , stomach , and prostate in men , and for cancers of the oesophagus , stomach , and kidney among women . 
the pattern was similar in wales , but the trends were statistically signi cant less often because of the much smaller population . during 200103 , survival for most cancers did not increase , or else the upward trends observed for 19962000 were attenuated . 
the steep increase in 1 - year survival for non - hodgkin lymphoma is a notable exception : in wales , 1 - year survival rose by about 1% a year during 19962000 , and by 2% a year during 200103 ( 1% a year in england )  . for patients diagnosed during 200406 , 1 - year survival in england increased again for most cancers . 
||not enough data to be estimated . table 3 : national trends in relative survival ( % ) at 3 , 5 , and 10 years after diagnosis , and 5 - year conditional survival , by sex and calendar period of diagnosis , and predicted survival for 2007 were not always statistically signi cant . 
in wales , by contrast , survival fell for 19 of the 35 cancersex combinations , although none of the declines were signi cant . another way to summarise the contrast is to examine the di erences between england and wales in survival trends within each of the three periods . 
during 19962000 , the annual increase in 1 - year survival was greater in wales than in england for 14 of 17 cancers in men and eight of 18 cancers in women . 
the situation was similar during 200103 , with survival trends for eight of 17 cancers in men and 16 of 18 cancers in women in wales slightly more favourable than in england and only seven less favourable . 
however , this pattern was reversed during 200406 , when annual trends in england were more favourable than in wales for 11 of 17 cancers in men and 12 of 18 cancers in women . longer - term survival was estimated for each calendar period and predicted for 2007 , as was the change in ( table 3 )  . 
 survival between in england , both 3 - year and 5 - year survival improved successive periods 362 vol 10 april 2009 between 19962000 and 200103 for most tumours , except those of the bladder and brain ( both sexes ) , and hodgkins disease ( men only )  . 
the picture in wales was similar , but there was no improvement for tumours of the bladder or brain in men , or for tumours of the kidney or brain in women . 
the improvements in longer - term survival are similar to the earlier increases in 1 - year survival in both countries . changes in 3 - year survival between 200103 and 200406 in both england and wales were similar to those observed between 19962000 and 200103 , with no clear trend emerging . 
between the periods 19962000 and 200103 , survival increased more quickly in wales than in england for 12 of 17 cancers in men and 13 of 18 cancers in women . 
the di erent timing of increases in 3 - year survival between england and articles england 19962000 wales 19962000 england 200406 wales 200406 oesophagus stomach colon rectum pancreas larynx lung melanoma prostate testis kidney bladder brain hodgkins disease non - hodgkin lymphoma myeloma leukaemia women oesophagus stomach colon rectum pancreas lung melanoma breast cervix uterus ovary kidney bladder brain hodgkins disease non - hodgkin lymphoma myeloma leukaemia 3 - year relative survival ( % ) 3 - year relative survival ( % ) figure 2 : 3 - year relative survival ( % ) for adults diagnosed with 21 common cancers during 19962000 and 200406 in england and wales vol 10 april 2009 articles 05 10 1 - year relative survival ( % ) 200406 annual trend ( % ) 200406 colon ( men ) colon ( men ) colon ( women ) colon ( women ) breast ( women ) breast ( women ) lung ( men ) lung ( men ) precision of the survival estimate precision of the annual trend estimate figure 3 : funnel plots of 1 - year relative survival ( % ) and year - on - year trend ( % ) during 200406 : selected cancers , by sex , in the nine government o ce regions of england , and wales all patients were adults aged 1599 years , and were diagnosed during 200406 . 
control limits are shown by coloured curves : the inner limits are for 95% , the outer limits are for 998% . wales produced similar overall changes during 19962006 , as shown for each sex in gure 2 . the northsouth gradient in cancer survival in england31 is only partially con rmed . 
the gradient was present in the case of colon cancer , but it has been attenuated by increases in survival in so - called lowsurvival regions over the period 19962006 ( table 4 )  . 
 even so , the funnel plots show that the south west region ( gure 3 , symbol k ) was still a high - survival outlier in 200406 , while the north west region ( gure 3 , symbol b ) was still a low - survival outlier . very little regional variation in breast - cancer survival was seen in england , where 1 - year survival was close to 95% for women diagnosed during 19962000 and 96% for those diagnosed in 200103 , and 92% and 94% , respectively , in wales ( table 4 )  . 
 survival in the north west ( gure 3 , symbol b ) is lower than the pooled english value : the di erence is small , but the value is below the 998% control limits , and the downward annual trend during 200406 is outside the control limit . 
1 - year survival in wales ( gure 3 , symbol w ) during 200406 was also below the control limits , but the year - on - year trend during that period was positive , and within the control limits . despite gradual improvement , 1 - year relative survival from lung cancer remains poor , around 27% for men diagnosed during 200406 ( table 4 )  . 
1 - year survival in the yorkshire and humber region ( gure 3 , symbol d ) and wales ( gure 3 , symbol w ) was below the lower 95% control limit in that period , whereas survival in the london region ( gure 3 , symbol h ) was above the upper limit . 
again , the annual trend in the north west region ( gure 3 , symbol b ) during 200406 was just below the lower 95% control limit , whereas the trend in the west midland region ( gure 3 , symbol f ) was above the upper limit . discussion cancer survival , especially at 1 year after diagnosis , improved for most of the 21 cancers examined , both in england and wales , during the period 19962007 . 
 the rst group , with a generally poor prognosis , consists of ve cancers for which 1 - year survival is often below 40% in men and women : cancers of the oesophagus , stomach , pancreas , lung , and bra survival from cancers of the pancreas and lung has hardly improved at all between 19962007 , and 1 - year survival for pancreatic cancer remains below 20% . 
 the range of survival in the group of cancers with higher survival has tended to narrow over time , because of a ceiling e ect among malignancies for which 1 - year survival is already 90% or higher : melanoma of the skin and cancers of the breast , uterus , prostate , and testis , and in england only , hodgkins disease . 
part of the increase in survival for prostate cancer may be attributable to the diagnosis of more indolent tumours as a result of widespread prostate - speci c antigen ( psa ) testing . a key aim of the nhs cancer plan for england , published in september , 2000 , was to improve the prospects of survival for cancer patients . 
the availability of 6 years of data on incident cancers in both england and wales since the publication of the cancer plan provided an early opportunity to examine its e ect . 
for a number of cancers including stomach , colon , rectum , cervix , uterus , ovary , and kidney , survival trends in england improved between 200103 and 200406 in the absence of screening or the widespread delivery of more e ective new treatments . 
the di erent time trends in england and wales suggest that those recent gains might be attributable to improvements in cancer care , including earlier diagnosis and more widespread adherence to treatment guidelines . 
although cancer services in wales undoubtedly improved after the publication of the cameron report , clinical cancer outcomes and cancer information were not given such high priority by hospital trusts as in england after the publication of the nhs cancer plan . we identi ed no di erence between england and wales in survival trends at 3 years or more after diagnosis for patients diagnosed up to 2003 . 
the more rapid increase in shortterm survival in england than in wales since 2004 could be interpreted as related to the cancer plan , but we do not have evidence of the extent to which the various initiatives in the cancer plan were fully implemented by that time . 
 even so , predicted 3 - year survival for cancers diagnosed in 2007 in england was generally higher than for 200406 , suggesting that survival is likely to continue to increase . 
 by contrast , there are fewer predicted improvements in survival in wales . one aspect that suggests the results are plausible is the similarity of survival patterns between men and 366 vol 10 april 2009 articles women in each country . 
thus , the recent upward trend in 1 - year survival in england occurred in both sexes , while a levelling o of the trends was also seen in both sexes in wales . 
the use in all analyses of region - speci c and deprivation - speci c life tables for each calendar year and each sex ensured that the background mortality used to estimate relative survival corresponded as closely as is feasible to that of each cancer patient . socioeconomic inequalities in survival have been widening for many adult cancers in england and wales.8 the nhs cancer plan aimed to reduce socioeconomic inequalities ( the deprivation gap ) in survival . 
although that objective has not yet been fully assessed , and despite real recent improvements in 1 - year survival in some of the more deprived regions , the previously described northsouth gradient for cancer survival33 and other socioeconomic and health - related parameters18 is still present , and relative survival for most cancers in the more a uent southern regions is generally higher than the mean survival for england . 
 the funnel plots presented in gure 3 ( and webappendix ) provide insight into regional variation in survival and whether recent trends will enable regions with low survival to catch up . 
to the extent that gains in survival are less marked among more deprived groups than more a uent groups , this will reduce the overall national trends in survival , and thus the overall e ectiveness of the plan . the survival estimates reported here are not agestandardised because the age distribution of cancer patients was fairly stable for most cancers during this short period ( 11 years )  . 
a notable exception was hodgkins disease , for which the marked fall in survival during 200406 was partly due to an increase in the age at diagnosis of patients diagnosed with this malignancy : the mean age at diagnosis increased by about 3 years between 1998 and 2005 . 
 incidence of the 21 cancers examined was generally stable over the period 19962006 , except for a rise in cancers of the prostate and breast , and melanoma of the skin , and a fall in cancers of the lung and stomach in men . 
 the fall in survival in england is mainly attributable to progressive change in the recorded spectrum of urothelial malignancies , pathological classi cation and coding34 that have not yet occurred to the same extent in wales . following changes patients who had previously had a primary malignancy in a di erent organ or tissue were included in these analyses , by contrast with our previous work.23 , 35 this was done mainly because of the marked increase of asymptomatic prostate cancer detected by psa , since these men have extremely high survival , which would arti cially raise the proportion of patients excluded for a previous primary cancer . 
survival estimates were virtually identical with and without the exclusion of patients with more than one tumour ( data not shown )  . in the past , patients who died on the date of diagnosis could not be distinguished in the national cancer registry data from dco registrations , for which the true duration of survival is unknown.9 a ag to indicate dco status is now available for more than 90% of cancers registered since 1996 in england and wales , but we excluded both dco registrations and other cases with zero recorded survival , for consistency with most other publications on cancer survival . 
inclusion of those patients who do appear to have died on the same day as the diagnosis ( no dco ag ) would have reduced the estimates of 1 - year survival for some cancers by up to 1% , but it had no e ect on the estimated trends in survival ( data not shown )  . successive eurocare studies have shown that cancer survival in both england and wales has lagged behind other countries in western and northern europe , despite encouraging recent results showing that both countries have tended to approach the levels of survival in other european countries during 19952002.36 the eurocare studies formed part of the impetus to create the nhs cancer plan.2 a recent editorial37 questioned whether the uk really has an e ective cancer plan , on the basis of ndings in the eurocare - 4 study , 36 which included patients diagnosed up to 2002 . 
however , the nhs cancer plan only dates from 2000 , so the eurocare - 4 study cannot o er a fully viable european comparison of survival trends after its implementation . 1 - year survival is the only cohort - based measure of outcome that is available for the whole period up to 2006 . 
even 3 - year survival can only be estimated for patients diagnosed during 200406 by using the complete approach , and no estimation of 5 - year survival for 200406 is currently possible without using the hybrid approach to incorporate follow - up data for patients who were diagnosed ( and whose treatment will have begun ) in earlier periods ( gure 1 )  . 
 international di erences38 and , in england and wales , socioeconomic di erences23 in 5 - year survival are largely attributable to higher cancer - related mortality soon after diagnosis . implementation of the data analysed here represent the earliest period from which an overall assessment of survival trends after the cancer plan could reasonably be attempted . 
recent survival trends in england , more favourable than those in wales , do indicate that the nhs cancer plan is having some bene cial e ect in england . our ndings do not , however , provide a de nitive verdict on the overall e ectiveness of the cancer plan . 
 vol 10 april 2009 articles the national data include over 2 million cancer patients and they are remarkably up to date , with follow - up data available to dec 31 , 2007 . 
but even with a large and timely dataset , and the latest techniques to assess recent survival trends , it seems we will need at least 3 years of follow - up data for all patients diagnosed during the period 200406 , up to the end of 2009 . 
incorporation of survival trends in scotland and northern ireland in the same analytical strategy might improve the evaluation of national cancer plans in the uk . finally , it is essential to do more detailed analyses to investigate the e ect on time trends and regional inequalities in cancer survival of some of the more speci c measures listed in the cancer plan and the cancer reform strategy , 40 such as mdts , shorter waiting times for investigation and treatment , and the training and specialisation of surgeons and other specialists . 
such studies will require more prompt and e cient linkage of the national cancer dataand linkage to a wider range of health datasetsthan is currently possible , as well as new ways of using this information to improve health policy . contributors mpc and br led the study design . 
all authors revised the report . con icts of interest the authors declared no con icts of interest . acknowledgments we thank the cancer registry sta in england and wales : their sustained data collection and quality control have enabled the survival of patients to be analysed and compared in this study . 
we also thank nicola cooper , susan westlake , and domenica rasulo of the cancer team at the ons for extensive work in preparing the data in the national cancer registry . 
227 of 249 women approached completed a comprehensive set of standardised cognitive tasks at baseline and were randomly assigned to receive anastrozole ( 1 mg / day for 5 years ) or placebo . 
by 6 months , 13 women in both groups reported changes to their memory and this had decreased to ve women in the placebo group and three women in the anastrozole group by the 24 - month assessment . 
signi cantly more women in the anastrozole group complained of hot ushes at 24 months ( 23 of 76 [ 30% ] vs 11 of 73 [ 15% ] , p = 0032 , not corrected for multiple comparison ) , but this was the only di erence in reported endocrine symptoms . interpretation these ndings show little or no impairment of cognitive performance with the use of anastrozole compared with placebo in postmenopausal women at high risk of developing breast cancer who were able to tolerate endocrine - related side - e ects . 
future studies assessing cognition should be done within randomised trials with baseline assessments to ascertain the true extent of the putative e ects that treatments for breast cancer might have on memory and attention . funding cancer research uk , london , uk ( grant numbers c6280 / a3162 and c6280 / a6764 )  . 
depletion of oestrogen with aromatase inhibitors in otherwise healthy women trial of vol 9 october 2008 articles 227 women randomised at baseline assessment 116 women assigned to placebo 111 women assigned to anastrozole 10 women excluded 2 intolerable endocrine symptoms 3 did not like cognitive tests 2 family problems 2 forgot to take medication 1 lost to follow - up 10 women excluded 5 intolerable endocrine symptoms 2 did not like cognitive tests 2 family problems 1 lost to follow - up 106 available for 6 - month assessment 101 available for 6 - month assessment 32 women excluded 15 intolerable endocrine symptoms 4 did not like cognitive tests 5 other medical condition 2 other cancer diagnosis 6 lost to follow - up 24 women excluded 12 intolerable endocrine symptoms 3 did not like cognitive tests 1 family problems 2 other cancer diagnosis 1 same risk as general population 5 lost to follow - up 74 available for 24 - month assessment 77 available for 24 - month assessment figure 1 : study pro le could prove unacceptable in terms of an increase in menopausal - type symptoms and might have detrimental e ects on cognitive function . 
studies assessing the e ect of endocrine treatments alone on cognition in women at risk of or treated for breast cancer are rare.7 , 8 most published studies tried unsuccessfully to separate the potential e ects of endocrine treatment in patients with breast cancer who had already received chemo therapy.9 the topic is confounded by previous use of chemotherapy , inappropriate sample sizes , and other methodological issues.10 treatments because of the very low oestradiol concentrations in women who take aromatase inhibitors , we did a preliminary cross - sectional study of cognitive function in the anastrozole , tamoxifen , alone or combined ( atac ) adjuvant trial . 
we assessed memory and attention in women ( n = 94 ) who had been in the atac trial for a median of 36 months , and who had not received chemotherapy . 
patients data were compared with those from an age - matched control group.7 findings showed a signi cantly poorer performance on tasks of verbal memory and processing speed in the patients with breast cancer . 
however , the numbers of patients allo cated to the di erent treatment arms were too small to do any between - group analyses to establish whether tamoxifen or anastrozole , or the combination , was implicated . 
also no pre - treatment baseline assessment of the patients performance was done to be able to establish whether or not the e ect was a result of endocrine treatment . 
 bender and colleagues8 assessed cognitive function , depression , anxiety , and fatigue in a small group of postmenopausal women with early - stage breast cancer who were treated with tamoxifen or anastrozole for at least 3 months . 
the researchers reported that women who received anastrozole ( n = 15 ) had poorer verbal and visual learning and memory than those who received tamoxifen ( n = 16 )  . 
 methods patients between jan 3 , 2003 , and dec 21 , 2005 , postmenopausal women at increased risk of developing breast cancer ( determined from family history [ rst - degree relatives with breast cancer at age < 50 years or two or more second - degree relatives with breast cancer ] ; previous benign disease with evidence of proliferation or atypia ; mammographic dysplasia ; or nulliparity plus any rstdegree family history ) were recruited into the cognitive subprotocol from ve uk centres ( royal bolton hospital , bolton ; breast care centre , frenchay hospital , bristol ; department of surgery , university hospital of wales , cardi ; nightingale centre and genesis prevention centre , university hospital of south manchester , manchester ; and royal marsden hospital , london )  . 
the primary endpoint of the prevention trial was to ascertain if anastrozole ( 1 mg / day for 5 years ; astrazeneca , maccles eld , uk ) was e ective in preventing invasive and non - invasive breast cancer in postmenopausal women at increased risk of the disease . 
 the secondary endpoints were to study the role of anastrozole in preventing oestrogen - receptor - positive breast cancer , breast - cancer mortality , assess the e ect of anastrozole on other cancers , cardiovascular disease , fracture rates , and non - breast - cancer deaths . 
the cognitive study is a separate protocol from the main clinical trial . women were invited to join the cognitive subprotocol by the clinician , research nurse , or researcher from cancer research uk psychosocial oncology group before randomisation . 
the randomisation tables were drawn up strati ed by country and the randomisation was balanced in blocks , with sizes randomly selected to be 6 , 8 , or 10 . 
 baseline 6 months 24 months * assessments the standardised cognitive assessments and interviews were done by one of four experienced psychologists ( vaj , la , hh , bm ) trained in the administration of neuropsychological tests . 
the assessments ( webpanel ) were done at baseline , 6 months , and 24 months , apart from the measure of intelligence , which was done only once at baseline . 
the cognitive test assessed several broad areas and comprised nine objective tasks ( yielding 17 measures for analysis ) covering the functional areas of verbal and visual memory with both immediate and delayed recall , working memory , processing speed and executive function . 
where alternative versions of tasks were available these were presented in a counterbalanced order between participants across the three timepoints , eg , word uency , logical memory , complex gure , and word lists . 
these standardised neuropsychological tasks are sensitive and have shown changes between patient groups in previous breast - cancer studies described elsewhere.7 , 11 self - reported measures at each timepoint , participants also completed the general health questionnaire 12 the broadbent cognitive failures questionnaire ( cfq ) , 13 and the endocrine symptoms subscale ( es ) .14 the ghq12 is a 12 - item general health measure designed to screen for probable , non - psychotic psychiatric disorder in com ( ghq12 ) , 12 * restricted to the 151 participants who completed all three assessments ( n = 74 for placebo group and n = 77 for anastrozole group )  . table 2 : details of the 207 participants in the main analysis munity and medical settings . 
it is an important factor to measure as self - reported memory complaints correlate strongly with increased anxiety.15 the cfq was developed to assess explicitly propensity for committing a cognitive failure related to perception , memory , and motor function . 
 it comprises 25 questions relating to lapses in attention in everyday life , and responses are ranged as : 0 = never , 1 = very rarely , 2 = occasionally , 3 = quite often , 4 = very often . 
also , as part of a structured interview , patients were asked at 6 months and 24 months whether they had noticed any changes in their memory or concentration and at 24 months about adherence to trial drugs . 
 statistical analyses all statistical analyses were done by use of stata software , version 9.2. psychiatric morbidity , self - reports of memory changes , concentration changes , and scores from the cognitive failures questionnaire were compared at each timepoint among treatment groups by use of pearsons 2 test ( or fishers exact test when appropriate ) for categorical variables and wilcoxon rank - sum test for interval variables . 
 the independent variables were treatment group , age , vol 9 october 2008 articles auditory verbal learning immediate recall total recall 15 delayed recall 7 logical memory immediate recall delayed recall complex gure immediate delayed letter cancellation eciency letter number sequencing spatial span forwards backwards total digit span forward backwards total executive function stroop total verbal uency placebo anastrozole reliable change index ( rci ) with a correction for observed practice e ects on each measure.16 by using this method , an rci was calculated for each measure by use of the baseline and 6 - month , and the baseline and 24 - month data of the placebo participants . 
this study is registered as an international standard randomised controlled trial , number isrctn31488319 . role of the funding source cancer research uk funded the cognitive subprotocol ( grant numbers c6280 / a3162 and c6280 / a6764 ) and had no involvement in the study design , collection , analysis , or interpretation of the data or in the writing of the report . 
the corresponding author had nal responsibility to submit for publication . results 227 of 249 ( 91% ) women approached agreed to participate in the cognitive function subprotocol , 207 ( 91% ) of whom completed both the baseline and 6 - month assessments , and of those interviewed at 6 months , 151 ( 67% ) also completed a 24 - month assessment ( gure 1 )  . 
we did not note a signi cant di erence at baseline between those who were and those who were not excluded in terms of age , iq , previous hrt use or ghq12 scores ( data not shown )  . 
 however , 34 of the 76 ( 45% ) women cited endocrine symptoms as the main reason for withdrawing , seven before the 6 - month assessment ( ve anastrozole , two placebo ) and 27 before the 24 - month assessment ( 12 anastrozole , 15 placebo )  . the baseline characteristics of all participants and of those included in the main analysis are shown in table 1 . 
 the characteristics were similar across treatments ( data not shown ) , with the exception of hrt use , which was greater in the placebo group ( 77 / 116 [ 66% ] vs 46 / 109 [ 42% ] for all participants , and 72 / 106 [ 68% ] vs 42 / 99 [ 42% ] for the participants in main analysis )  . 
the psychological characteristics of the groups were similar at trial entry with 20 of 101 ( 20% ) women in the anastrozole group and 24 of 106 ( 23% ) women in the placebo group scoring above the threshold on the ghq12 ( table 2 )  . 
these proportions were only slightly higher than the 18% of above threshold scores recorded in healthy populations.17 there was also no signi cant di erence on the baseline characteristics and baseline scores between those who did and did not complete the 24 - month assessment ( data not shown )  . treatment group was unrelated to cognitive performance at baseline on any of the objective measures 20 15 10 05 30 figure 2 : mean changes and 95% cis from baseline for each cognitive task by treatment group intelligence quotient ( iq ) , psychological distress ( ghq12 ) , and previous hormone replacement therapy ( hrt ) use . after checking that the 17 objective cognitive measures had similar values at 6 months and 24 months by use of the wilcoxon signed ranks test , a mean of the two values was calculated . 
for each patient and for each cognitive measure , the change from baseline was calculated as the di erence between the mean value at 6 months and 24 months and the baseline value . 
to test for a signi cant change from baseline , the mean change from baseline of each measure was compared to 0 by use of the wilcoxon signed ranks test . 
the di erence between treatment groups was tested by comparing the mean changes the placebo and anastrozole groups by use of the wilcoxon rank - sum test . such group comparisons can mask impairment in subgroups of the population . 
therefore , to study performance for an individual woman , we used the from baseline between 956 vol 9 october 2008 articles independent of age , intelligence , menopausal status , cfq , and ghq12 scores . 
to calculate the mean change from baseline when there were missing values at baseline , the baseline values were imputed by use of a linear regression analysis of the measure on age and intelligence . the potential e ect of hrt use on cognitive function at baseline was assessed for both groups combined . 
higher mean scores for logical memory immediate , logical memory delayed , letter number sequencing , and improved performance on a task of executive function were in favour of the non - hrt users ( non - hrt vs hrt , mean [ sd ] : 1455 [ 400 ] vs 1294 [ 421 ] , p = 0007 ; 1310 [ 414 ] vs 1181 [ 410 ] , p = 0020 ; 1178 [ 233 ] vs 1067 [ 247 ] , p = 0003 ; 4259 [ 876 ] vs 3833 [ 820 ] , p < 0001 , not corrected for multiple comparison , respectively )  . figure 2 shows the mean change from baseline with 95% cis for each task by treatment group . 
 for both groups combined , there was a signi cant e ect of time for two tasks having an increased value from baseline ( mean change from baseline [ se ] : complex gure immediate recall 124 [ 036 ] ; complex gure delayed recall 133 [ 033 ] ; table 4 )  . 
when the analysis was restricted to the baseline and 6 - month data , there were no signi cant di erences between the anastrozole and placebo groups , and no e ect of time for any of the objective cognitive tasks ( table 5 )  . 
at baseline , data missing from 1 placebo patient and 2 anastrozole patients ; at 6 months , data missing from 2 placebo patients and 2 anastrozole patients ; at 24 months , data missing from 2 placebo patients and 1 anastrozole patient . 
at baseline , data missing from 2 placebo patients and 2 anastrozole patients ; at 6 months , data missing from 3 placebo patients and 3 anastrozole patients ; at 24 months , data missing from 3 placebo patients and 2 anastrozole patients . 
we tested if there was a di erence between treatment groups for these four factors and noted no signi cant di erence ( webtable 1 ) group comparisons do not identify impairment in subgroups of the population or account for practice e ects . 
 to assess performance of individual women , we used the rci with a correction for observed practice e ects on each measure.16 few women showed a reliable decline on three or more tasks at 6 months ( 3 anastrozole , 3 placebo ) or at 24 months ( 2 anastrozole , 2 placebo ) , and there were no signi cant di erences between the groups ( webtable 2 )  . 
 see online for webtables 13 there were no di erences between groups in the proportions of women experiencing psychological distress as measured by the ghq12 at each timepoint ( table 3 )  . 
 the baseline ghq12 score signi cantly correlated with the cfq score ( z = 2748 , p = 0006 , wilcoxon rank - sum test ) , data not shown . 
the women who were anxious reported more lapses in attention in everyday life ( data not shown )  . few women complained of changes in their attention and memory at 6 months or 24 months , and there were no di erences between the treatment groups ( table 2 )  . 
70 of 141 ( 50% ) reported forgetting to take their tablets during the study period ( 31 anastrozole , 39 placebo ) , but most ( 53 of 70 ; 76% ) rarely forgot . 
clinicians or research nurses suggested drug holidays ( ie , temporary cessation of trial medication ) for some women who experienced marked side - e ects during the study period . 
by the 6 - month assessment , ve women in the anastrozole and one woman in the placebo group had been told to take a drug holiday ( table 2 )  . 
from 6 months to 24 months , one woman in the anastrozole group did not take her tablets for an unknown duration . women also self - initiated drug holidays ; by 6 months , four women in the anastrozole and three in the placebo groups reported taking a drug holiday . 
from 6 months to 24 months , three women in the anastrozole group and one woman in the placebo group self - initiated drug holidays ( table 2 )  . 
the main analysis was also done without these patients and there was no di erence in the ndings ( webtable 3 )  . there was no signi cant e ect of time or treatment group on the total endocrine symptom score ( data not shown )  . 
to assess changes in individual endocrine symptoms from baseline , responses were dichotomised into those who reported , somewhat , a little bit , not at all or quite a bit or very much . 
 although our ndings con ict with other published work , 8 , 9 , 23 they are similar to data reported in clinical trials of raloxifene , a benzothiophene member of the selective oestrogen - receptor - modulator class of compounds used in the treatment and prevention of osteoporosis . 
the multiple outcomes of raloxifene study ( more ) 24 was a randomised clinical trial of raloxifene ( 60 mg or 120 mg ) versus placebo in 7478 postmenopausal women . 
although there was a tendency towards a decline in performance on verbal memory and attention tasks , there were no signi cant di erences between the three groups at baseline or after 3 years.24 hot ushes at 24 months ( 23 of 76 [ 30% ] vs 11 of 73 [ 15% ] , p = 0032 , not corrected for multiple comparison )  . discussion the ndings from this comprehensive , prospective neuropsychological study show that anastrozole does not seem to impair any aspect of cognitive function in postmenopausal women at increased lifetime risk of breast cancer who were participating in a placebocontrolled trial . 
 the strength of this study is that it is part of a large double - blind randomised clinical trial , which provides a better assessment of putative cognitive impairment than previous cross - sectional or observational cognitive studies . 
as this was a double - blind study , we can be in cognitive con dent that any noted di erences performance are true and not a ected by women knowing which treatment they were receiving . 
the weakness is that the study sample was relatively small compared with therapeutic trials ( n = 227 ) , and by 24 months attrition might have caused a loss of power to detect changes . 
this proportion was much lower than that reported in a prospective study of women with breast cancer who received endocrine treatment with or without chemotherapy.20 77 of 93 ( 83% ) of those who received both treatments complained of memory prob lems at 6 months compared with 24 of 49 ( 49% ) who received endocrine treatment only . 
it is well documented that self - reported cognitive problems are associated with high levels of anxiety , but this cannot explain the di erence because similar proportions of women scored above threshold on the ghq12 in both studies . 
one suggestion is that some women who have breast cancer experience post - traumatic stress disorders.21 a diagnosis of breast cancer plus ensuing treatment interrupts normal life and might sensitise patients to make inaccurate objective judgments about the way they function cognitively before and after diagnosis . our ndings lend support to the view that depletion of oestradiol concentrations once a woman is postmenopausal does not notably interfere with the processes of memory and attention over a 24 - month period . 
performance was poorer for previous hrt users on tasks requiring sustained attention and verbal memory , ie , logical memory immediate , letter number sequencing , and on a task of executive function . 
these ndings are interesting in the light of the data from the womens health initiative memory study ( whims ) , 25 which suggested that use of hrt is detrimental in the older postmenopausal woman . 
we know that from other work in an adjuvant setting that most side - e ects of endocrine treatments tend to develop within the rst 3 months and thereafter plateau or improve . 
complaints of arthralgia were not di erent between the groups with 26 of 100 ( 26% ) women in the anastrozole group and 30 of 106 ( 28% ) of those in the placebo group reporting this symptom as quite a bit or very much at 6 months . 
although surprising , the endocrine symptom pro le resembles those from an earlier chemoprevention study of tamoxifen versus placebo , where the only signi cant di erence between groups was for vasomotor complaints.28 patientreported outcomes from standard ised assessments are reliable and several published studies have shown that they represent better the side - e ects of drugs than those reported by clinicians on case report forms.29 poor adherence merits further study for the low reporting of menopausal - type symptoms , but self - rated and clinicianreported adherence was better than that in previous chemoprevention studies . 
an international task force has been proposed to provide guidelines for future research to address these issues.30 contributors vaj designed and supervised the study , did the neuropsychological assessments , and wrote and revised the report . 
 articles lancet oncol 2008 ; 9 : 33141 published online march 19 , 2008 doi : 10.1016 / s14702045 ( 08 ) 70077 - 9 see lancet online / articles doi : 10.1016 / s01406736 ( 08 ) 60348 - 7 see lancet online / comment doi : 10.1016 / s01406736 ( 08 ) 60349 - 9 * trialists listed at end of paper correspondence to : prof john yarnold , department of clinical radiotherapy , royal marsden hospital , sutton , surrey sm2 5pt , uk the uk standardisation of breast radiotherapy ( start ) trial a of radiotherapy hypofractionation for treatment of early breast cancer : a randomised trial the start trialists group * summary background the international standard radiotherapy schedule for breast cancer treatment delivers a high total dose in 25 small daily doses ( fractions )  . 
however , a lower total dose delivered in fewer , larger fractions ( hypofractionation ) is hypothesised to be at least as safe and e ective as the standard treatment . 
we tested two dose levels of a 13 - fraction schedule against the standard regimen with the aim of measuring the sensitivity of normal and malignant tissues to fraction size . methods between 1998 and 2002 , 2236 women with early breast cancer ( pt1 - 3a pn0 - 1 m0 ) at 17 centres in the uk were randomly assigned after primary surgery to receive 50 gy in 25 fractions of 20 gy versus 416 gy or 39 gy in 13 fractions of 32 gy or 30 gy over 5 weeks . 
the protocol - speci ed principal endpoints were local - regional tumour relapse , de ned as reappearance of cancer at irradiated sites , late normal tissue e ects , and quality of life . 
 this study is registered as an international standard randomised controlled trial , number isrctn59368779 . findings 749 women were assigned to the 50 gy group , 750 to the 416 gy group , and 737 to the 39 gy group . 
the estimated absolute di erences in 5 - year local - regional relapse rates compared with 50 gy were 02% ( 95% ci 13% to 26% ) after 416 gy and 09% ( 95% ci 08% to 37% ) after 39 gy . 
photographic and patient self - assessments suggested lower rates of late adverse e ects after 39 gy than with 50 gy , with an hr for late change in breast appearance ( photographic ) of 069 ( 95% ci 052091 , p = 001 )  . 
from a planned meta - analysis with the pilot trial , the adjusted estimates of / value for tumour control was 46 gy ( 95% ci 1181 ) and for late change in breast appearance ( photographic ) was 34 gy ( 95% ci 2345 )  . 
416 gy in 13 fractions was similar to the control regimen of 50 gy in 25 fractions in terms of local - regional tumour control and late normal tissue e ects , a result consistent with the result of start trial b . 
a lower total dose in a smaller number of fractions could o er similar rates of tumour control and normal tissue damage as the international standard fractionation schedule of 50 gy in 25 fractions . introduction in women with early breast cancer prescribed radiotherapy after tumour excision or mastectomy , the e ective dose of radiation is adjusted to balance the risk of local cancer recurrence against the risk of harmful e ects on healthy tissues . 
radiotherapy reduces the risk of local relapse by about 70% and reduces breast cancer mortality.1 such treatment is o ered to nearly all patients after local tumour excision and to selected patients after mastectomy . 
this schedule has evolved pragmatically , and is based on an assumption that a high total dose delivered in small fractions of 20 gy keeps the amount of normal tissue damage to a minimum while gaining the maximum level of tumour control . 
this perception was strengthened when early studies of hypofractionation , which did not use adequate reductions in total dose , reported unacceptably high rates of normal tissue injury.2 normal and malignant tissues vary in their responses to radiotherapy fraction size , termed fractionation sensitivity . 
responses are described by a model in which the sensitivity ( measured by the degree of tissue damage for normal tissues , and tumour recurrence rates for malignant tumours ) to fraction size is represented by the ratio of two constants and .3 the lower the ratio of to ( expressed in gy ) , the greater the e ect on normal and malignant tissues of changes in fraction size . 
healthy tissues of the breast and ribcage are sensitive to fraction size , with / values 5 gy or less , 4 so small changes in fraction size can produce relatively large changes in the e ects of radiotherapy on these tissues . 
this sensitivity is typical vol 9 april 2008 articles of so - called late - reacting normal tissues that take months or years to develop atrophy or brosis after radiotherapy . 
in head and neck cancer , radiotherapy delivered in small fractions ( 20 gy ) to a high total dose spares late - responding normal tissues relative to tumour.5 breast cancer has previously been thought to be insensitive to fraction size and best treated with fractions of 20 gy or less . 
however , some trials have tested the hypothesis that breast cancer is as sensitive to fraction size as the normal tissues of the breast and underlying rib cage.68 if con rmed , these ndings could indicate that small fraction sizes of 20 gy or lower o er no therapeutic advantage , and that a more e ective strategy would be to deliver fewer , larger fractions to a lower total dose . between 1986 and 1998 at the royal marsden hospital ( rmh ) and gloucestershire oncology centre ( goc ) in the uk , 1410 patients prescribed whole breast radiotherapy after breast conservation surgery were randomised to 50 gy in 25 fractions or to two dose levels of a 13 - fraction regimen over 5 weeks39 gy in 30 gy fractions and 429 gy in 33 gy fractions.7 , 8 the primary endpoint was late normal tissue e ects , with local tumour control as a secondary endpoint , and the results were consistent with breast cancer having a similar sensitivity to fraction size as the late - reacting healthy tissues . 
based on this pilot study , the standardisation of breast radiotherapy ( start ) trials were initiated by the uk coordinating committee for cancer research ( now national cancer research institute ) to extend the testing of radiotherapy schedules using fraction sizes larger than 20 gy , in terms of local - regional tumour control , normal tissue e ects , quality of life , and health economic consequences . 
trial a maintained the explanatory design of the rmh / goc trial , with a reduction in one of the test group doses from 429 gy in 33 gy fractions to 416 gy in 32 gy fractions , following advice from the independent data monitoring committee . 
 the trial was designed to allow interpolation between two 13 - fraction regimens in order to identify the schedule equivalent to 50 gy in 25 fractions in terms of late normal tissue e ects , and to compare local tumour control at this test - dose level . 
the protocol - speci ed intent was to combine the datasets of the pilot trial and start trial a under guidance of the independent data monitoring committee to more precisely estimate the fractionation sensitivity of breast cancer . 
by contrast , start trial b9 was a more pragmatic trial that compared a commonly used schedule in the uk ( 40 gy in 15 fractions in 3 weeks ) with a control group of 50 gy in 25 fractions over 5 weeks . 
 this paper presents the results of trial a . ( continues on next page ) methods participation was open to all uk centres that provided radiotherapy treatment to patients with early breast 332 vol 9 april 2008 articles cancer . 
due to earlier completion of recruitment in trial b , those centres were invited to join trial a after accrual to trial b was complete . operable invasive breast patients women with cancer ( international union against cancer pt1 - 3a pn0 - 1 m0 ) requiring radiotherapy after surgery ( breast - conserving surgery or mastectomy , with clear tumour margins 1 mm ) were eligible for the trial if they were aged over 18 years , did not have an immediate surgical reconstruction , and were available for follow - up . 
unlike the pilot study , which had normal tissue e ects as the primary endpoint , mastectomy patients were included in trial a , since tumour control was one of the principal endpoints . 
patients from 13 centres participating in trial a were also recruited into the quality of life and health economics studies ( health economics data not reported here , baseline quality of life data have been published elsewhere10 )  . 
13 centres recruited patients who had breast - conserving surgery into the photographic assessment substudy ( 12 centres were in both the quality of life and photographic studies )  . 
patients from 12 centres also consented to donate a 20 ml blood sample for the study and to complete an associated family history questionnaire ( substudy not reported here )  . 
written informed consent was obtained for all patients . procedures start trial a patients were randomised to either 50 gy in 25 fractions ( control group ) or 416 gy in 13 fractions or 39 gy in 13 fractions ( experimental schedules )  . 
this treatment involved ve fractions per week in the control group and ve treatments per fortnight ( monday , wednesday , friday one week , tuesday and thursday the next week ) in each of the two experimental schedules . randomisation was arranged via telephone at the clinical trials and statistics unit at the institute of cancer research ( icr - ctsu ) , sutton , uk , where patient details were recorded and treatment was allocated . 
computer - generated random permuted blocks were used as the method of allocation , with patients strati ed by hospital , type of surgery ( breast conserving surgery or mastectomy ) , and intention to give a tumour bed boost dose or not . 
use of adjuvant systemic treatment was recorded , with a requirement of at least a 2 - week gap between exposure to chemotherapy and radiotherapy . patients lay in a supine treatment position . 
the planning target volume was de ned as the whole breast the total dose administered with a 1 cm margin to palpable breast tissue ; where regional radiotherapy was indicated , the planning target volume was supraclavicular nodes with or without axillary chain with a 1 cm margthe decision to give regional radiotherapy was made before randomisation and was only used in 14% of patients ( table 1 )  . 
in two patients prescribed radiotherapy to the breast and supraclavicular fossa and randomised to the 416 gy schedule , the supraclavicular fossa was reduced to 39 gy because of the sensitivity of brachial plexus to fraction size . 
most patients were treated with 6 mv x - rays , although treatment with higher energies or cobalt - rays was allowed after discussion with the start trial radiotherapy quality assurance teaplanning protocols were speci ed at the time of noti cation of participation into the study and had to conform to the minimum quality criteria described in the start trial a protocol . 
other endocrine therapies include combinations of tamoxifen / anastrozole / letrozole / exemestane / goserelin , mostly within randomised trials . table 1 : demographic and clinical characteristics at randomisation of the 2236 patients in start trial a vol 9 april 2008 articles 2236 patients randomised 749 allocated 50 gy in 750 allocated 416 gy in 737 allocated 39 gy in 25 fractions over 5 weeks 13 fractions over 5 weeks 13 fractions over 5 weeks 735 received allocated treatment * 8 refused allocated treatment 1 whole breast treatment 741 received allocated treatment * 4 given non - allocated treatment 1 whole breast treatment 731 received allocated treatment * 4 given non - allocated treatment 1 refused to complete not given 1 recurrence found 3 severe skin reactions , treatment stopped after 23 fractions 1 withdrew after randomisation due to depression not given 1 withdrew after randomisation 1 continual wound infection ( given 50 gy ) ( given 50 gy ) 1 treatment delayed for 18 days 1 found to have metastases requiring further surgery , so radiotherapy suspended treatmentiridium implant given 1 withdrew after randomisation ( given 40 gy in 20 fractions ) 5 with baseline data only 3 withdrew consent to follow - up after randomisation 2 moved 2 with baseline data only 1 moved 1 unknown 2 with baseline data only 2 withdrew consent to follow - up after randomisation 749 included in analysis 750 included in analysis 737 included in analysis figure 1 : trial pro le for start trial a * only major treatment deviations listed . 
minor deviations due to public holidays , machine service days , and machine breakdowns not included . all centres submitted details of the standard radiotherapy technique , after which a visit by the quality assurance team checked dosimetric measurements in a 2d and 3d breast phantom , including the junction region between supraclavicular fossa and tangential breast or chest wall elds.1215 the mean di erence between prescribed and measured dose in a phantom was 21% . 
additionally , a third of the radiotherapy treatment plans were collected and analysed by the quality assurance team to ensure compliance with the protocol terms of prescription point , dose homogeneity , and lung depth . 
a random sample of patients had in - vivo thermoluminescent dosimeter measurements taken.1618 the protocol allowed for a dose variation ( in the planning target volume ) between 95% and 105% of that at the reference point on the central axis . 
these results con rmed a good compliance with the technical aspects of the trial protocol . the principal endpoints speci ed in the protocol were local - regional relapse , normal tissue e ects , and quality of life . 
local - regional tumour relapse was de ned as local relapse in breast or chest wall , and regional relapse in ipsilateral axilla or supraclavicular fossa if it had been within an irradiated target volume . 
disease - free survival was de ned as time to any breast cancer - related event ( local - regional or distant relapse , contralateral breast cancer , or death from breast cancer )  . 
brachial and plexopathy was reported if damage to the brachial plexus was suspected and the patient had symptoms of pain , parasthesia , numbness , or other sensory symptoms ( graded on a 4 - point scale )  . 
photographs were taken at baseline ( post - surgery and pre - radiotherapy ) and then at 2 and 5 years to assess changes to the breast based on change in size , shrinkage , and shape , and scored on a 3 - point graded scale . 
changes in breast appearance ( photographic ) were scored by three observers blind to patient identity , treatment allocation , and year of follow - up , and a nal agreed score reached by consensus . 
the assessment of change in breast appearance from photographs was fully validated in the pilot study.7 breast size and surgical de cit were both de ned from the baseline photographs by the same three observers applying 3 - point graded scales . 
post - baseline quality of life questionnaires included an additional four protocolspeci c items relating to changes in the a ected breast after radiotherapy ( skin changes in the area of the a ected breast , overall change in breast appearance , rmness to touch of the a ected breast , and reduction in size of the a ected breast )  . 
 the trial was overseen by a steering committee of several 334 vol 9 april 2008 articles independent experts joined by members of the icr - ctsu , start trial management group , and representatives of the funding bodies ( as observers )  . 
the trial management group was responsible for the day - to - day management of the trial , and the emerging safety and e cacy data was reviewed regularly by the independent data monitoring committee . 
central statistical monitoring of data was done by icr - ctsu , supplemented by selected on - site source document veri cation . statistical analysis the sample size was estimated with the intent of measuring di erences in local - regional tumour relapse between each 13 - fraction schedule and the control group . 
a 5 - year local - regional tumour relapse rate of 10% in the 50 gy group was predicted , based on the rmh / goc pilot target sample size of 2000 patients was de ned in trial a to provide 80% power to detect a di erence of 5% in the local - regional relapse rate between the control group and each test group ( two - sided = 005 )  . 
 kaplan - meier estimates of 5 - year relapse rates , rates of normal tissue e ects , rates of any breast - cancer related event , and mortality rates were calculated ( with 95% cis )  . 
 for the patient quality of life self - assessments of normal tissue e ects an event was de ned as the rst occurrence of a moderate or marked symptom ( graded quite a bit or very much )  . 
the scores from the photographic assessments of change in breast appearance at 2 and 5 years were dichotomised as none versus mild or marked change , and the rst occurrence of such a change was taken as the endpoint for the survival analysis . 
there were too few patients with marked change in breast appearance ( photographic ) to be able to analyse this category separately . the wald test was used to compare between pairs of fractionation schedules . 
since point estimates of di erences in event rates can , by chance , be atypical of the overall pattern of di erences between schedules , estimates of the absolute di erence in 5 - year event rates taking the whole range of observation times into account were obtained by applying the hazard ratios obtained from the cox model to the kaplan - meier estimate of the rate in the 50 gy control group.23 both one - sided and two - sided 95% cis were calculated for the absolute di erence in local - regional relapse rates at 5 years , since the upper limit is of greater clinical interest , in view of concern about a possible excess risk caused by hypofractionated schedules . 
plots were censored at the median length of follow - up ( rounded to nearest year )  . a direct estimate of the / value for breast cancer was obtained by tting a cox proportional hazards regression model containing terms for total dose , and total dose multiplied by dose per fraction , to the local - regional relapse data . 
similarly , an estimate of the / value for dose - limiting normal tissues was obtained by tting the same regression model to the photographic data for change in breast appearance . 
in each case , the / ratio was calculated by dividing the two parameter estimates ( estimate for total dose / estimate for total dose dose per fraction )  . 
where appropriate , the cox models included covariates associated with relapse and late normal tissue e ects , so the resulting / value estimates ( and 95% ci ) were adjusted for prognostic factors . 
local relapse de ned as ipsilateral local tumour relapse in breast parenchyma / breast skin / chest wall skbreast cancer - related events : local , regional , or distant relapse , breast cancer death , contralateral breast cancer ( disease - free survival )  . table 2 : survival analyses of relapse and mortality according to fractionation schedule in start trial a vol 9 april 2008 articles 006 005 004 003 002 001 role of the funding source the funding sources provided peer - reviewed approval for the trial and have had representation ( as observers ) on the trial steering committee , but had no other role in the design , conduct , data collection , data analysis or the results . 
the the study or interpretation of corresponding author had full access to all the data in the study , and had nal responsibility for the decision to submit for publication . 1999 , january , results between and december , 2002 , 2236 patients were enrolled in start trial a at 17 centres in the uk ( gure 1 )  . 
a total of 1129 patients enrolled in the quality of life study and 1306 in the photographic assessment study ( with 878 patients enrolled in both substudies )  . and clinical demographic characteristics randomisation were well balanced between treatment groups ( table 1 )  . 
of the women prescribed chemotherapy , many ( 555 / 793 , 700% ) received an anthracyclinecontaining regimen , which was balanced between randomised radiotherapy schedules ( 178 / 259 [ 687% ] for 50 gy ; 185 / 264 [ 701% ] for 416 gy ; and 192 / 270 [ 711% ] for 39 gy )  . 
cyclophosphamide , methotrexate , and uorouracil combination therapy alone was prescribed in 227 women ( 286% of those receiving chemotherapy ) , which was similarly balanced between randomised groups ( 77 [ 297% ] for 50 gy ; 78 [ 295% ] for 416 gy ; and 72 [ 267% ] for 39 gy )  . 
 of the 1805 women prescribed tamoxifen or another endocrine therapy , most ( 1790 , 992% ) were continuing treatment at randomisation ( 603 / 606 [ 995% ] for 50 gy ; 611 / 618 [ 989% ] for 416 gy ; and 576 / 581 [ 991% ] for 39 gy )  . 
 data for oestrogen receptor status was not collected as part of start trial a , but routine policy in most of the centres during the accrual period was to prescribe tamoxifen only to patients who were oestrogen - receptor positive or whose oestrogen receptor status was unknown . 
there were only 29 major treatment deviations ( including early stopping of treatment , patient refusal of allocated treatment , and patients found to be ineligible for reasons including presence of relapses ) , resulting in 987% compliance with allocated treatment ( gure 1 )  . 
compliance with completion of quality of life questionnaires over 5 years was more than 90% . unadjusted / = 48 gy ( 95%ci 0163 ) number at risk 50 gy 416 gy 39 gy 50 gy ( 28 / 749 ) 41.6 gy ( 30 / 750 ) 39 gy ( 35 / 737 ) years since randomisation 50 gy 41.6 gy 39 gy figure 2 : kaplan - meier plot ( a ) and nelson - aalen cumulative hazard plot ( b ) of local - regional tumour relapse in 2236 patients / ratios were truncated at zero when the calculated limit was negative . the protocol speci ed that the start trial a data would be combined with the rmh / goc pilot study data8 to obtain a combined estimate of the adjusted / values for breast cancer and for normal tissues . 
in view of the di erences between the trials in terms of absolute rates of local relapse and patient characteristics , a meta - analysis was subsequently considered more appropriate , on the advice of the independent data monitoring committee . 
repeating the meta - analysis by pooling the adjusted estimates from each trial ( rather than using individual patient data ) made little di erence to the combined estimates ( data not shown )  . analysis included all randomised patients on an intention - to - treat basis . 
this study is registered as an international standard randomised controlled trial , number isrctn59368779 . median follow - up of surviving patients was 51 years ( iqr 4460 ) , with a maximum follow - up of 80 years . 
at the time of analysis , 1881 patients ( 841% ) were alive and without relapse , 36 ( 16% ) were alive with local - regional 336 vol 9 april 2008 articles relapse ( without distant relapse ) , 54 ( 24% ) were alive with distant relapse ( including 14 with local - regional relapse ) , 256 ( 114% ) had died ( including 43 with local - regional relapse ) , and nine ( 04% ) had no follow - up . at the time of analysis , 93 ( 42% ) patients had had local - regional tumour relapse , and the hazard ratios relative to the 50 gy group were 105 ( 95% ci 063175 ) after 416 gy and 126 ( 95% ci 077208 ) after 39 gy ( table 2 )  . 
 the estimated absolute di erences in local - regional relapse rates compared with 50 gy at 5 years were 02% ( 95% ci 13% to 26% ) after 416 gy and 09% ( 95% ci 08% to 37% ) after 39 gy . 
since the main concern over hypofractionation is an excess risk rather than a possible bene t , a more precise estimate of the potential excess risk of local - regional relapse was obtained from the upper limit of the one - sided 95% ci for the absolute di erence in 5 - year local - regional relapse rates for each 13 - fraction schedule compared with 50 gy . 
 the kaplan - meier and cumulative hazard rate plots for local - regional relapse according to fractionation schedule ( gure 2 ) illustrate the low event rate in all randomised groups . the unadjusted / value for local - regional relapse estimated from a cox proportional hazards regression model was 48 gy ( 95% ci 0163 )  . 
adjusting for prognostic factors resulted in extremely wide con dence limits , since the main e ects for total dose and total dose x dose per fraction were not independently predictive of local - regional relapse in the regression model . 
hence , the / value for local - regional relapse was left as a crude estimate . rates of distant relapse , disease - free survival , and overall survival were similar between the fractionation schedules , with no evidence of a clinically signi cant detriment for either of the hypofractionated schedules compared with 50 gy ( table 2 )  . change in breast appearance ( photographic ) was assessed in 1055 patients with both a baseline and at least one follow - up image ( 354 for 50 gy , 357 for 416 gy , and 344 for 39 gy )  . 
not all patients had photographs available at both 2 and 5 years , for reasons including the 5 - year assessment not yet being due at the time of scoring and analysis , patient refusal , and withdrawal from the photographic study due to relapse . 
there were no associations between score for change in breast appearance ( photographic ) at 2 years or patient demographic or treatment characteristics and whether or not the patient had a 5 - year assessment ( data not shown )  . 
the hazard ratios for any ( mild or marked ) change in breast appearance compared with the 50 gy group were 109 ( 95% ci 085140 , p = 062 ) after 416 gy and 069 ( 95% ci 052091 , p = 001 ) after 39 gy ( gures 3 and 4 )  . 
reported cases include three with rib fracture after bone metastases and nine after trauma . table 3 : incidence of ischaemic heart disease , symptomatic rib fracture , and symptomatic lung brosis according to fractionation schedule and persisted to 5 years . 
the / estimate for any change in breast appearance ( photographic ) was 31 gy ( 95% ci 1646 ) adjusted for age , adjuvant therapy , lymphatic radiotherapy , breast size , and surgical de cit . for least one completed patient quality of life self - assessments of late normal tissue e ects were available 1080 patients ( 957% of all patients in the quality of life study ) with a baseline and at follow - up questionnaire ( 359 for 50 gy , 364 for 416 gy , and 357 for 39 gy )  . 
according to patient quality of life self - assessments of ve key normal tissue e ects on the breast or breast area , rates of moderate or marked e ects by 5 years were similar after 416 gy and 50 gy . 
 rates of moderate or marked normal tissue e ects tended to be lower after 39 gy than after 50 gy , with a signi cantly lower rate of change in skin appearance after 39 gy than after 50 gy ( p = 0004 )  . 
in the 416 gy group , there was one case of pneumonitis 9 months after treatment and one patient who developed mild symptoms and signs of brachial plexopathy 2 years after treatment . 
the remaining 24 incidences of second primary cancers consisted of one or two cases of several di erent types . when all patients in the rmh / goc trial ( 1410 patients ) and start trial a ( 2236 ) were included in a meta - analysis , the unadjusted estimate of the / value for local - regional relapse was 41 gy ( 95% ci 0974 )  . 
adjusting for known prognostic factors ( age , chemotherapy , tamoxifen , lymphatic radiotherapy , type of primary surgery , boost , and pathological tumour size ) gave an adjusted / value for local - regional relapse of 46 gy ( 95% ci 1181 )  . 
 including all the 1202 rmh / goc trial and 1055 start trial a patients with available photographic assessment data in a meta - analysis , the unadjusted estimate of the / value for any change in breast appearance was 36 gy ( 95% ci 2449 )  . 
adjusting for age , chemotherapy , tamoxifen , breast size , and surgical de cit gave an adjusted / value of 34 gy ( 95% ci 2345 )  . discussion the results of start trial a are consistent with the hypothesis that breast cancer is as sensitive to fraction size as the normal tissues . 
the rst indication that breast cancer could be safely and e ectively treated using fraction sizes above 20 gy was rst raised more than 20 years ago , when biological models were applied to retrospective clinical data.24 , 25 in start trial a , 416 gy in 13 fractions was similar to the control regimen of 50 gy in 25 fractions in terms of normal tissue e ects and also in terms of local tumour control.24 , 25 this result is consistent with that of the start trial b , in which 40 gy in 15 fractions over 3 weeks seemed at least as safe and e ective as 50 gy in 25 fractions . 
 the fractionation sensitivity of breast cancer quanti ed by an / ratio of 48 gy , but the small number of local - regional tumour relapse events ( n = 93 ) limits precision ( 95% ci 0163 gy )  . 
statistical power is enhanced by considering the results of start trial a together with a larger number of local - regional relapses ( n = 185 ) recorded by the pilot trial over a 15 - year period.8 a meta - analysis of the pilot data and start trial a generates an / ratio for breast cancer of 46 gy ( 95% ci 1181 )  . 
the con dence limits of such an estimate are still fairly wide but closer to the estimate of / ratio for 338 vol 9 april 2008 articles normal tissue e ects of 34 gy ( 95% ci 2345 ) from the meta - analysis of the photographic assessments . 
 despite the residual imprecision in estimating fraction size sensitivity , breast cancer seems to respond di erently to human squamous carcinomas of the bronchus and head and neck region , and to experimental animal tumours characterised by / values of 10 gy or more.5 this distinction is important , not only because it has potential implications for breast cancer treatment , but also because it contributes to accumulating evidence that cancers vary in their sensitivity to fraction size.26 the molecular mechanisms fractionation sensitivity are not yet understood , but the cellular correlates include recovery from sub - lethal and potentially lethal damage.27 the ability to predict fractionation sensitivity from the tumour phenotype or genotype might allow fraction size to be adjusted more accurately to the individual cancer . governing that time , adhering the initial estimate of a 10% rate of local - regional relapse at 5 years in the 50 gy control group was based on the pilot trial started in 1986 . 
since then , improvements in surgery , radiotherapy techniques , systemic therapy , and more e ective multidisciplinary working have reduced risks of both local and metastatic breast cancer relapse . 
at to appropriate governance procedures , the potential e ects of the predicted lower than expected relapse rates were discussed by the independent trial steering committee and the independent data monitoring committee . 
since the local - regional relapse rate was lower than expected ( < 4% ) , the study actually has greater power than originally planned to detect a 5% absolute di erence ( 97% power , assuming 4% in the control group ) , which represents a much larger relative treatment e ect ( 4% in control group vs 9% in test group compared with 10% vs 15% as speci ed in the protocol )  . 
for example , with a 4% local - regional relapse rate in the control group , the study is able to detect an absolute di erence of 35% with a similar level ( 82% ) of power as originally planned . the photographic assessments of normal tissue e ects con rm a dose - response relation between the two test doses , from which a precise estimate of / value has been derived , consistent with previous published work.27 assuming a conservative / value of 3 gy for all normal tissue e ects except nerve injury , the 39 gy and 416 gy test doses are equivalent to 468 gy and 516 gy in 20 gy equivalents , respectively . 
the fractionation sensitivity of underlying lung tissue or heart might di er from that of ribcage and breast , but this uncertainty is less relevant now that the heart can usually be physically shielded when advanced techniques of radiotherapy planning and delivery are applied.28 the results of patient quality of life self - assessments of normal tissue e ects in start trial a are largely consistent with the dose response e ect seen in the photographic assessments . physician assessments of normal tissue e ects have not been presented in this paper . 
preliminary analysis of these data produce estimates of the relative e ects of the fractionation schedules which seem similar to those assessed by the photographic and patient self - assessments . 
since the level of detail included in the hospital case notes varied within and between centres , this practice , although unbiased between treatment groups , could have led to underreporting of physician - assessed normal tissue e ects . 
the results of the physician assessments will thus be the subject of a separate paper , reporting also the sensitivity of the endpoints according to method of completion of case report forms . the 115% absolute di erence in breast appearance at 5 years between the two test regimens generates a value of 14 at the steepest part of the dose - response curve ( the value measures the gradient of the dose response curve as the percent increase in e ect per percent increase in total dose delivered in 20 gy fractions29 ) , which converts into a 52% absolute increase in normal tissue e ects per 20 gy fraction . 
the local - regional relapse data from start trial a generate a value of 02 , which gives some indication of the small gains expected from dose escalation when tumour control is more than 95%.30 this nding has implications for modelling the imprecision in the estimate of breast cancer fractionation sensitivity . 
taking into account the higher 10 - year local - regional relapse rates in the rmh / goc pilot trial , the current precision of the / estimate can be shown by estimating a 95% ci for the 10 - year local - regional relapse rate of a speci c fractionation schedule . 
if the / value for tumour control is as high as 81 gy ( the upper 95% con dence limit ) , a 13 - fraction regimen matched to 50 gy in 25 fractions for late normal tissue e ects would have an anti - tumour e ect equivalent to 473 gy in 20 gy fractions , accounting for 15% more local - regional relapses compared with 50 gy in 25 fractions . 
 if the / value for tumour control is as low as 11 gy ( the lower 95% con dence limit ) , the same schedule would be responsible for 43% fewer local - regional relapses at 10 years compared with 50 gy in 25 fractions . 
with the lower 5 - year local - regional relapse rates in start ( 34% ) compared with the rmh / goc pilot trial ( 8% ) , the absolute excess local - regional is roughly half in the start patient population . vol 9 april 2008 articles a median follow - up of 5 years is too short to allow assessment of all the potential late normal tissue e ects such as cardiac damage . 
however , the rmh / goc pilot data ( median follow - up 10 years ) showed that the relative e ects of di erent fractionation schedules remain unchanged over time . 
the short - term priority is to protect the heart from exposure to radiotherapy ; something that is now possible with advanced radiotherapy technologies . is unlikely in conclusion , our data are consistent with the hypothesis that breast cancer shows similar responsiveness to fraction size as the late responding normal tissues of the breast , as indicated by the / estimates . 
 independent data monitoring committee : h lucraft ( chair , newcastle general hospital ) , m parmar ( mrc clinical trials unit , london ) , i turesson ( akadamiska sjukhuset , uppsala , sweden )  . consumers ( observers to trial management group ) : m carling ( rage ) , j pritchard ( independent ) , m king ( ex - member of rage , deceased ) , e parkin ( ex - member of rage )  . funders ( observers to trial steering committee ) : k law ( cancer research uk ) , s perkins ( medical research council ) , u wells ( department of health )  . con ict of interest statement j brown is an employee of eli lilly & company , who are not a sponsor . 
 we declare that we have no con ict of interest . acknowledgments we thank all the patients who participated in this study , and the doctors , nurses , radiographers , physicists , and data managers at the participating centres . 
we acknowledge the support of the royal college of radiologists ( uk ) and radiotherapy action group exposure ( rage ) , especially margaret king , deceased , to whom this manuscript is dedicated . 
we acknowledge the contributions of colleagues who previously worked on the trial , including c cruickshank , c dawson , e marriage , l gamaldo , c harper , d hussey ( all ex - icr - ctsu ) and a deighton , s gri ths , e miles ( all ex - trial management group )  . 
we thank cancer research uk , the uk medical research council , and the department of health for providing the funds to undertake this research ( grant g9600656 )  . 
the cancer research uk number for the start trial is cruk / 96 / 001 . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology chosen as one of the endpoints.2 patients recruited in this trial were offered radiofrequency ablation , because they were considered by the treating physician to be unsuitable for surgery and unfit for radiotherapy or chemotherapy as a result of either underlying chronic obstructive pulmonary disease or major associated comorbidities . 
because the patients had small , asymptomatic pulmonary tumours , no improvement in quality of life was noted after treatment with radiofrequency ablation , despite the high number of complete responses . 
nevertheless , we think that the absence of any significant worsening in short form ( sf ) - 12 ( physical and mental summary ) scores and functional assessment of cancer therapylung ( fact - l ; lung - cancer scale and trial outcome index ) scores provides evidence that the minimallyinvasive treatment approach used in these patients did preserve their quality of life . 
the number at risk for part b of gures 3 and 4 of this article should have been interventional group ( top ) and control group ( bottom )  . 
also , the second sentence in the discussion should have read , however , preoperative chemoradiotherapy in patients undergoing surgery signi cantly increased the proportion of those with complete resection ; and in those with complete resection , preoperative chemoradiotherapy increased the proportion of patients with mediastinal downstaging and histopathological response . bo etta p , hecht s , gray n , gupta p , straif k . 
during the immediate months preceding submission of the review sh was acting in the capacity of an expert witness for the plainti in a future court case against a smokeless tobacco company . 
sh declares his participation in this case in no way in uenced his writing or involvement in the review . bonnefoi h , potti a , delorenzi m , et al . 
 errata risk ratio lower limit upper limit z value p value risk ratio ( 95% ci ) meyer18 lee19 hull20 deitcher21 overall 0704 0509 0438 0690 0509 0121 0329 0188 0124 0351 4091 0789 1017 3832 0737 0391 3018 1920 0425 3571 0696 0003 0055 0671 < 00001 * noble sir , shelley md , coles b , et al . 
the aim of this study was to con rm the validity of these geneexpression signatures in a large series of patients with oestrogen - receptor - negative breast tumours who were treated in a phase iii neoadjuvant clinical trial . 
 methods this trial compares a non - taxane regimen ( uorouracil , epirubicin , and cyclophosphamide [ fec ] for six cycles ) with a taxane regimen ( docetaxel for three cycles followed by epirubicin plus docetaxel [ tet ] for three cycles ) in women with oestrogen - receptor - negative breast cancer . 
pathological complete response , de ned as complete disappearance of the tumour with no more than a few scattered tumour cells detected by the pathologist in the resection specimen , was used to assess chemosensitivity . 
this study is registered on the clinical trials site of the us national cancer institute website findings of 212 patients with oestrogen - receptor - negative tumours assessed , 87 patients were excluded . 
125 oestrogenreceptor - negative tumours ( 55 that showed pathological complete responses ) were tested : 66 in the fec group ( 28 that showed pathological complete responses ) and 59 in the tet group ( 27 that showed pathological complete responses )  . 
the fec predictor had a sensitivity of 96% ( 27 of 28 patients [ 95% ci 8299 ] ) , speci city of 66% ( 25 of 38 patients [ 5079 ] ) , positive predictive value ( ppv ) of 68% ( 27 of 40 patients [ 5280 ] ) , and negative predictive value ( npv ) of 96% ( 25 of 26 patients [ 8199 ] )  . 
analysis of tumour size , grade , nodal status , age , and regimen - speci c signatures showed that the genomic signatures were the only independent variables predicting pathological complete response at p < 001 . 
the high npv of both signatures may allow early selection of patients with breast cancer who should be considered for trials with new drugs . introduction systemic chemotherapy for the treatment of breast cancer improves overall survival , whether given preoperatively or as postoperative adjuvant treatment.1 newer chemotherapy regimens containing taxanes further improve survival compared with standard regimens , 2 but taxanes are expensive , toxic , and might bene t only a small number of patients . 
several single - arm neoadjuvant chemotherapy trials have reported geneexpression signatures obtained from tumour biopsies taken at diagnosis.39 most of these studies described signa tures that predict clinical or pathological response , although one failed to identify any genes that predicted response.9 these studies have two weaknesses that restrict their use in routine practice . 
 we have previously reported gene - expression signatures that predict the response of cell lines and tumours to a range of chemotherapeutic drugs.15 the aim of the present study was to con rm the ability of these signatures to predict the response of oestrogen - receptor - negative breast tumours to chemotherapy in a large series of patients enrolled in a phase iii neoadjuvant trial . 
 methods patient selection and sample processing this substudy was restricted to patients with oestrogenreceptor - negative tumours because studies that contain both patients with oestrogen - receptor - positive tumours and pa tients with oestrogen - receptor - negative tumours are easily confounded by genes linked to oestrogen - receptor status ; additionally , pathological complete response is so rare after treatment with either regimen in patients with oestrogen - receptor - positive tumours that better selection of patients will have the greatest e ect in oestrogenreceptor - negative disease . 
pathological com plete response was used as a surrogate measure of chemosensitivity because this measure consistently predicts better survival after neoadjuvant chemotherapy.1114 , 16 , 17 we undertook this study in the context of a prospective phase iii intergroup trial of neoadjuvant chemotherapy ( european organisation for research and treatment of cancer [ eortc ] 10994 / breast international group [ big ] 00 - 01 ) , the design of which is shown in gure 1 . 
eligible patients had no evidence of distant metastatic disease ( ie , m0 , as de ned by the tumour , nodes , and metastasis [ tnm ] staging system ) , and had a histologically con rmed large , operable , invasive tumour ( tumour size t2 or t3 , node status n0 or n1 ) 18 or locally advanced breast cancer ( any t , n2 ; or t4 )  . 
this substudy was restricted to all patients who were assessed at the eortc data centre on april 1 , 2005 , who met the following criteria : oestrogenreceptor - negative tumours by immuno histochemistry of the pretreatment formalinxed biopsy ; completion of the planned chemotherapy regimen with no major protocol violation ; non - t4 tumours ; and good - quality and more than 200 ng yield of rna available from a pretreatment frozen biopsy . 
 in this substudy , patients were randomly assigned to a european non - taxane regimen of six cycles of 500 mg / m uor ouracil , 100 mg / m epirubicin , and 500 mg / m cyclophosphamide ( fec ) treatment , or to three cycles of 100 mg / m docetaxel followed by three cycles of 90 mg / m epirubicin plus 70 mg / m docetaxel ( tet )  . 
pathological complete response was used as the outcome measure , and was de ned as disappearance of the invasive component of the primary tumour after treatment , with at most a few scattered tumour cells detected by the pathologist in the resection specimen . 
the a ymetrix cel les were normalised breast cancer : large operable , or locally advanced , or inammatory randomisation non - taxane regimen : fec 100x6 surgery * taxane regimen : tx3 followed by etx3 surgery * first sample : standard xation histology and oestrogen - receptor status core biopsy second sample : snap frozen microarray figure 1 : study design of eortc 10994 / big 00 - 01 trial fec = uor ouracil , epirubicin , and cyclo phosphamide . 
 * surgery was followed by radiotherapy or hormonal therapy ( or both ) according to each centres policy . 1072 vol 8 december 2007 retracted articles for information on the robust multi - array average ( rma ) algorithm see bioconductor.org see online for webappendix , webpanel and webtable 1 with the robust multi - array average ( rma ) algorithto infer the presence of erbb2 amplicons , 40 genes from trip3 to rapgefl in the erbb2 region on chromosome 17q were clustered by use of euclidian distance and wards linkage method . 
the anthracycline used in the eortc clinical study was epirubic since data on epirubicin sensitivity were not available , we used the cell - line signature for doxorubicin , an anthracycline very similar to epirubicweights generated by binaryregression analysis were applied to the expression values and summed to create metagene scores that were converted to probabilities by applying a probit function ( webappendix , webpanel , and webtable 1 )  . 
the singledrug probabilities were combined to yield the predicted probabilities of pathological complete response to fec and tet regimens as previously described.15 receiver operating characteristic ( roc ) curves were used to test the quality of the predictions . 
bootstrapping fec group ( n = 66 ) tet group ( n = 59 ) 2670 3470 with 100 000 resampled datasets was used to nd 95% ci of the area under the curve ( auc ) of the roc curves . 
the youden index20 ( sensitivity + speci city1 ) was used to select a threshold for estimation of sensitivity , speci city , positive predictive value ( ppv ) , negative predictive value ( npv ) , and overall accuracy . 
when a category of an ordinal variable had too few observations , these were pooled with an adjacent ( consecutive ) category ( grade 1 and 2 , tumour size t1 and t2 , node status n1 and n2 )  . 
 binary estimates of age and the signatures , cut at the median of the tested population , were used for fishers exact test ; age was dichotomised as a surrogate indicator of menopausal status ( median age was 495 years )  . 
missing values for grade were fec group fec predictor tet group fec predictor age , years median range histology invasive ductal invasive lobular other * tnm stage grade hormone receptor status pr negative erbb2 status ampli ed response no pcr p < 00001 ( wilcoxon ) , n = 66 p = 0302 ( wilcoxon ) , n = 59 no pcr no pcr fec group tet predictor tet group tet predictor na = not available . 
pr and oestrogen receptor ( er ) were assessed locally in each centre ; cases where less than 10% of tumour cells stained positive for pr by immunohistochemistry were deemed negative . 
 table 1 : clinical and demographic characteristics of patients p = 0044 ( wilcoxon ) , n = 66 p < 00001 ( wilcoxon ) , n = 59 no pcr no pcr figure 2 : prediction of pathological complete response with genomic signatures strati ed by trial group pcr = pathological complete response . 
black dashed lines show maximum empirical youden index ; those in the upper - left and lower - right panels were used to calculate the performance metrics in table 2 . 
classi cation statistics at the optimum threshold ( maximum empirical youden index ) with 95% ci are shown . see online for webtable 2 table 2 : performance metrics of genomic regimen - speci c signatures fec group tet group auc ( 95% ci ) auc ( 95% ci ) doxorubicin fluorouracil 066 ( 053079 ) 073 ( 059085 ) 0023 0002 076 ( 063088 ) 040 ( 025056 ) cyclophosphamide 094 ( 088099 ) < 00001 056 ( 041071 ) docetaxel fec signature tet signature 037 ( 024051 ) 0068 090 ( 081097 ) 086 ( 076094 ) < 00001 058 ( 042073 ) 065 ( 051077 ) 0044 085 ( 074094 ) 00004 0211 0401 < 00001 0302 < 00001 auc by group , approximate 95% ci ( 100 000 bootstrap samples ) , and p value ( two - sided wilcoxon rank sum test ) for the null hypothesis of no di erence . table 3 : area under roc curves of genomic signatures ( single agents and regimen - speci c signatures ) by group fec group fec predictor tet group fec predictor auc = 086 ( n = 66 ) auc = 058 ( n = 59 ) maximum youden index = 062 maximum youden index = 029 1specicity 1specicity fec group tet predictor tet group tet predictor auc = 065 ( n = 66 ) auc = 085 ( n = 59 ) maximum youden index = 03 maximum youden index = 061 1specicity 1specicity figure 3 : roc analysis of the ability of genomic signatures to discriminate patients with a pathological complete response from patients with residual disease auc , number of cases ( n ) , and location of the maximum empirical youden index ( green point ) are shown . 
 to model the potential bene t from selecting the treatment regimen according to the predicted probabilities of pathological complete response to the individual regimens , a regimen preference score was calculated by subtracting the predicted probability of pathological complete response to tet from the predicted probability of pathological complete response to fec . 
use of zero as the threshold for allocation to one or other regimen assumes that the predicted probabilities of pathological complete response to the two regimens are perfectly matched , but this is unlikely because they were independently derived from cell - line data . 
hypothetical pathological complete response rates for the entire group of 125 patients were calculated at di erent regimen allocation thresholds by taking into account the observed pathological complete response rate and the number of patients in each group at that threshold . 
this study is registered on the clinical trials site of the us national cancer institute website role of the funding source the sponsor of the trial ( eortc ) designed and coordinated the trial . 
the funding sources of the study had no role in the design of the study ; collection , analysis , or interpretation of the data ; or in the writing of this report . 
the corresponding author had full access to all of the data and had the nal responsibility to submit for publication . results of 212 patients with oestrogen - receptor - negative tumours assessed at the data centre on april 1 , 2005 , 87 patients were excluded because of major protocol violation ( two patients ) , t4 tumours ( 30 patients ) , below 20% tumour - cell content in pretreatment incisional or core biopsy ( 25 patients ) , or poor quality rna or less than 200 ng yield of rna , or both ( 30 patients )  . 
biopsies from 66 tumours in the fec group and 59 tumours in the tet group of the eortc 10994 / big 00 - 01 study were tested on a ymetrix x3p microarrays . 
response predictors were constructed by taking genes that predict the response of cell lines to uorouracil , cyclophos phamide , docetaxel , and epirubicin given as single drugs , then combining these single - drug signatures to form regimen - speci c genomic signatures , as previously described.15 figure 2 shows the predicted probability of pathological complete response to fec and tet calculated with the regimen - speci c genomic signatures in the two treatment groups . 
the signatures signi cantly predict response in patients that received 1074 vol 8 december 2007 retracted articles fec group or ( 95% ci ) size t3 vs t1 and t2 077 ( 025233 ) grade 1 and 2 vs 3 039 ( 011135 ) nodal status 1 and 2 vs 0 087 ( 029264 ) erbb2 status a vs n * 176 ( 044733 ) age older vs younger 163 ( 055495 ) 062 011 081 037 046 tet group or ( 95% ci ) 026 ( 006096 ) 067 ( 016254 ) 057 ( 017187 ) 095 ( 028321 ) 141 ( 045449 ) 210 ( 067687 ) 003 056 042 100 060 020 fec signature tet signature 865 ( 2553384 ) 272 ( 090861 ) 00001 008 1476 ( 3787024 ) < 00001 or = odds ratio . 
univariate and multivariate linear regression models including age and the genomic signatures as continuous variables are shown in webtables 3 and 4 . table 4 : two - sided fishers exact tests for association of clinical variables and genomic signatures with pathological complete response by group fec group pcr fec group no pcr tet group pcr tet group no pcr predicted probability of pcr to tet figure 4 : predicted probabilities of pathological complete response to fec and tet treatments pcr = pathological complete response . 
as would be expected given the absence of e ect of the clinical or pathological variables in univariate analysis , the genomic signatures remain signi cant in formal multivariate testing ( webtable 4 )  . a plot of the predicted probabilities of pathological complete response to the two regimens can be divided the appropriate drugs ( p < 00001 )  . 
to assess the ability of the signatures to identify responders , we did a roc analysis ; the youden index was used to identify the threshold for calculation of the performance . 
the accuracy of prediction for the regimen - speci c signatures is 79% ( 52 of 66 patients [ 95% ci 6787 ] ) for patients in the fec group and 80% ( 47 of 59 patients [ 6888 ] ) for patients in the tet group ( table 2 )  . 
furthermore , the signatures are speci c to the two regimens ; table 3 and gure 3 show that the sign atures predict response in the correct group ( ie , the fec signature predicts response to fec treatment , and the tet signature predicts response to tet treatment ) , but not in the wrong group ( ie , fec to tet , or tet to fec )  . 
both treatment regimens in the eortc study contain epirubicin , albeit in di ering schedules and total doses , therefore a small amount of crossover between the predictors in the opposing groups might be anticipated . 
we noted a weak prediction by the tet signature in the fec group ( albeit the lower boundary of the ci of the auc [ 051 ] barely exceeds the 050 value for a random classi er ) but none with the fec signature in the tet group ( the ci of the auc overlaps 050 )  . 
the design of the study called for exposure of tumours to three cycles of full - dose docetaxel ( t ) before giving combined anthracycline plus ( et )  . 
to further study the role of individual drugs in the two groups , roc analysis was used to assess the performance of the singledrug predictors ( table 3 and web gure )  . 
we conclude that the regimen - speci c signatures predict pathological complete response because they are built from individual drug signatures that predict pathological complete response . taxane tumour size , and the clinical variables age at diagnosis , node status , the pathological variables and histological grade and erbb2 status were tested for their ability to predict pathological complete response by use of fishers exact test ( table 4 ) and by univariate logistic regression ( webtable 3 )  . 
tumour size in patients in the tet group showed a borderline signi cant association with response ( p = 003 ; this would not be signi cant the 14 comparisons in table 4 or the 18 comparisons in webtable 2 )  . 
the upper - right quadrant contains many patients who responded well to treatment ( triangles ) ; the undesirable side - e ects of taxanes mean these patients are candidates for conventional fec treatment . 
the lowerright quadrant contains many patients who failed to respond to fec ( green circles ) , but have a high predicted probability of pathological complete response to tet ; the upper - left quadrant contains some patients who failed to respond to tet ( blue circles ) , but have a high predicted probability of pathological complete response to fec . 
 inspection of the plot shows that dividing it with a diagonal line might form the basis of a rule to allocate patients to di erent regimens : patients below the diagonal line should receive tet , and patients above the line should receive fec . 
 at least two reasons exist for asking what might happen if this threshold were altered ( ie , the diagonal line were displaced vertically ) : rst , it might be desirable to decrease the number of patients receiving taxanes because of their side - e ects ; second , the predicted probabilities of pathological complete response to the two regimens are independently derived and unlikely to be matched precisely . 
to do this , we rst calculated a regimen preference score ; this was simply the predicted probability of pathological complete response to fec treatment minus the predicted probability of pathological complete response to tet treatment . 
in the treatment allocation model , patients were assigned to fec treatment when the regimen preference score was above the threshold ( above the diagonal line ) and to tet when the regimen preference score was below the threshold ( below the diagonal line )  . 
the diagonal line in gure 4 corresponds to a threshold of zero in gure 5 ; the patient marked by the arrow would be allocated to treatment with tet because their regimen preference score ( 02 ) was below zero . 
the ratio of green triangles to green circles above the diagonal line gives the pathological complete response rate for fec treatment ; this number multiplied by the total number of points above the line gives the number of responders in the group allocated to fec treatment ; likewise , the ratio of blue triangles to blue circles below the line gives the pathological complete response rate for tet treatment ; this number multiplied by the total number of points below the line gives the number of responders in the group allocated to tet treatment ; these are combined to calculate the hypothetical pathological complete response rate for both groups together . 
 when the threshold is lowered ( ie , the diagonal line in gure 4 is moved vertically down ) , more patients are assigned to fec treatment ( green dashed line in gure 5 ) , whereas when it is raised more patients are assigned to tet treatment ( blue dashed line )  . 
for example , for the point marked by an arrow ( regimen preference score of 02 ) , decreasing the regimen allocation threshold to 03 would mean that the score was now above the threshold and the patient would receive fec treatment . 
 generally , the lower the score the more likely a patient is to receive tet treatment ; conversely , the lower the threshold the more likely a patient is to receive fec treatment . 
for a wide range of thresholds the hypothetical pathological complete response rate ( red line ) is 6570% , well above the 42% and 46% pathological complete response rates noted in the fec and tet groups in the clinical trial . 
the peak of the red curve is displaced to the left of zero , suggesting that fec treatment could be safely used more frequently if treatment were selected by use of the signatures described here . 
we conclude that clinical application of these regimen - speci c genomic signatures could have a useful e ect on overall treatment success and decrease the number of patients exposed to the side - e ects of taxanes . 1076 vol 8 december 2007 retracted articles discussion this study con rms that gene - expression signatures based on cell lines can be used to predict pathological complete response of breast tumours to chemotherapy . 
 to our knowledge , this is the rst study in which genomic predictors for two di erent treatments have been studied in a large cohort of patients enrolled in a multicentre randomised phase iii clinical trial . 
long - term follow - up will be required to establish whether regimen - speci c genomic signatures also predict long - term survival , but this is likely since most previous studies have noted that patients achieving a pathological complete response indeed have longer survival , and this remains true after multivariate analysis.11 , 16 , 17 the ndings reported here used a doxorubicin signature instead of an epirubicin signature . 
the a ymetrix x3p chip we used was developed for analysis of para n - embedded material , so only small modi cations to the protocol might be needed to test para n - embedded material . 
alternatively , pcr techniques developed by gianni and colleagues4 could be used to measure the expression of the genes in our genomic signatures . there it necessitates is no universally accepted de nition of pathological complete response . 
pathological complete response de ned as disappearance of the invasive component of the primary tumour after treatment , with at most a few scattered tumour cells detected by the pathologist in the resection specimen , is standardisation of proof that a large mass of tumour cells has disappeared . 
killing large numbers of tumour cells is desirable , but does not guarantee long - term survival of patients , possibly because rare tumour stem cells are the crucial determinants of relapse.21 hence , validation of the clinical relevance of the signatures reported here will best be done by showing regimen - speci c prediction of improved survival of patients in a large adjuvant study , where the de nition of pathological complete response is not relevant . 
indeed , the pathological complete response rate is so low in this group in the neoadjuvant setting that a study ten times larger than the one we have undertaken would be needed to identify con dently a signature with similar predictive power in the oestrogen - receptor - positive group . to neoadjuvant the treatment allocation model explored in gures 4 and 5 suggests that selection of the treatment regimen with our genomic signatures has the potential to increase the pathological complete response rate from 44% to around 70% . 
an important caveat is that this will apply only to patients with oestrogen - receptor - negative the oestrogen - receptor - negative group there are two major tumours with radically di erent geneclasses of expression pro les ( called the erbb2 and basal - like classes in the stanford classi cation22 )  . 
 this makes it feasible to identify at an early stage patients who are unlikely to respond to fec or tet treatment and hence have the most to bene t from new drugs . 
 organising clinical trials on this basis would have important implications for the subsequent use of new drugs being tested , because the information obtained would apply only to a narrowly de ned group , albeit one vol 8 december 2007 1077 retracted articles with a poor outcome with conventional treatment . 
we thank the european commission sixth framework programme active p53 grant , fondation widmer , fondation medic , oncosuisse , swiss national science foundation nccr molecular oncology , eortc translational research fund , swedish cancer society , king gustav the fifth jubilee fund , swedish research council , us national institute for health , the american association for cancer research ( aacr ) , and the v foundation for cancer research for nancial support . re ection and reaction panel : concepts applicable to various histologies ( excluding small - cell carcinoma , germ - cell tumors , and lymphoma ) in the analysis of brain metastasis trials involving radiosurgery and adjuvant wbrt patients eligible for radiosurgery have brain metastases less than 34 cm in diameter adjuvant wbrt probably decreases the risk of distant brain tumour recurrence for most histologies including melanoma adjuvant wbrt probably does not improve overall survival adjuvant wbrt is associated with a greater decline in learning and memory function at 4 to 6 months in a heterogenous population of primary cancer types wbrt causes acute fatigue and hair loss wbrt frequently delays the prompt initiation of systemic therapy a substantial proportion of patients with brain metastases do not need adjuvant wbrt in their lifetime a substantial proportion of patients with brain metastases initially treated with radiosurgery can be salvaged with additional radiosurgery delaying , or obviating the need for giving wbrt completely radiosurgery , like wbrt , can be used to address uncontrolled brain metastases in patients seeking to enroll on and qualify for clinical trials who would be otherwise excluded di culty inherent in accruing su cient numbers of patients to a site - speci c brain metastasis trial . 
however , there are common elements and fundamental concepts that seem to be valid across various histologies ( excluding small - cell carcinoma , germ - cell tumours , and lymphoma ) involving in the analysis of brain metastasis trials radiosurgery and adjuvant whole brain radiation therapy ( wbrt ; panel )  . 
perhaps in the future , the combination of advanced functional neuro - imaging and gene - expression pro ling techniques will enable us to identify better the subgroup of patients who are at greatest risk for developing distant brain metastases . 
the current preference and practice of medical oncologists in the department of melanoma medical oncology at md anderson cancer is to refer patients with oligo brain metastases to undergo radiosurgery alone to facilitate rapid enrolment on systemic therapy protocols . 
it is agreed that specialised brain metastasis trials focused exclusively on melanoma patients would help further elucidate the respective roles of surgery , radiosurgery , adjuvant wbrt , and systemic treatments . 
a phase 2 eastern cooperative oncology group ( e 6397 ) study of radiosurgery alone in patients with one to three brain metastases from renalcell carcinoma , melanoma , or sarcoma concluded that delaying wbrt might be appropriate for some subgroups of patients.2 in the meantime , the management of patients with melanoma brain metastases relies on the extrapolation of data gleaned from existing reports on brain metastasis , rst - hand knowledge of the patient history , and multidisciplinary discussion to provide the best treatment plan individualised for each patient . eric l chang * , patrick hwu department of radiation oncology ( elc ) , department of melanoma medical oncology ( ph ) , the university of texas md anderson cancer center houston , tx , usa echang@mdanderson.org the authors declared no con icts of interest . chang el , wefel js , hess kr , et al . 
phase ii trial of radiosurgery for one to three newly diagnosed brain metastases from renal cell carcinoma , melanoma , and sarcoma : an eastern cooperative oncology group study ( e 6397 )  . 
radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
lancet oncol 2010 ; 11 : 2128in gure 3 of this article ( published online first on nov 7 , 2009 ) , the data presented for unknown in the sex subgroup should have been in the egfr - positive cells subgroup . 
these corrections have been made to the printed article in this issue , and to the online version as of jan 6 , 2010 . rajkumar sv , jacobus s , callander ns , et al , for the eastern cooperative oncology group . 
lancet oncol 2010 ; 11 : 2937the webappendix of this article ( published online first on oct 22 , 2009 ) has been corrected as of jan 6 , 2010 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology vol 11 january 2010 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper to the lancet go to thelancet / to submit a paper to the lancet oncology go to ees.elsevier.com / thelancetoncology / recommendations in light of the new data presented by raaijmakers and colleagues.3 piet dirix * , sandra nuyts department of radiation oncology , university hospitals leuven , leuven , belgium , piet.dirix@uzleuven.be the authors declared no con icts of interest . raaijmakers cp , roesink jm , dijkema t , houweling ac , terhaard ch . 
first results of a phase iii multicenter randomized controlled trial of intensity modulated ( imrt ) versus conventional radiotherapy ( rt ) in head and neck cancer ( parsport : isrctn48243537 ; cruk / 03 / 005 )  . 
proc am soc clin oncol 2009 ; 27 : abstr lba6006 . call for papersoncology and haematology the lancet and the lancet oncology are announcing plans for issues of each journal to be devoted to speci c topics in oncology and also to haematology . 
the former will be timed to coincide with the european society of medical oncology ( esmo ) congress in milan , italy ( oct 812 , 2010 ) , and the latter with the american society of hematology ( ash ) annual meeting in orlando , fl , usa ( dec 47 , 2010 )  . 
we would like to invite submissions of high - quality original research about cancers of the breast , lung , prostate , and gastrointestinal tract , or on any topic in haematology or haematological oncology . 
accepted papers will be published in either the lancet or the lancet oncology via fast - track peer review to coincide with either the esmo or ash annual meetings , as appropriate . 
 submissions to coincide with the esmo annual meeting must be received by june 25 , 2010 , and those for the ash annual meeting by oct 1 , 2010 , via either the lancet or the lancet oncologys online submission systems . 
please state in your covering letter that the submission is in response to this call for papers . if your work is being presented at either meeting and falls under an embargo policy , please tell us the date and time of the presentation , and whether the study is to be presented orally or in a poster . 
if your paper is accepted , online publication can be scheduled to coincide with the presentation and comply with any press embargo . jane godsland , zo mullan , richard turner , david collingridge the lancet ( jg , zm , and rt ) and the lancet oncology ( dc ) , 32 jamestown road , london nw1 7by , uk errata relling mv , altman rb , goetz mp , evans we . 
clinical implementation of pharmacogenomics : overcoming genetic exceptionalislancet oncol 2010 ; 11 : 50709the acknowledgment in this comment ( published online first on april 21 , 2010 ) should have read we thank colleagues in nihs pharmacogenomics research network . 
in the second paragraph , the last sentence was misspelt and should have read despite evidence linking pharmacogenomic variation with drug exposure , toxic e ects , and e cacy , many clinicians , regulators , and payors hold pharmacogenetic evidence to excessively high standards . 
lancet oncol 2010 ; 11 : 42938in this article , the acknowledgments statement should also have included : the uk medical research council funded the original all97 / 99 trial and supported the childhood leukaemia working party . 
lancet oncol 2007 ; 8 : 31722in this article , the equation for acpgbi in panel 2 should read loge [ r / ( 1r ) ] = ( 4859 + total score )  . 
additionally , in table 3 , 158 was added in error next to the heading clinicopathological staging . 516 vol 11 june 2010 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a paper go to thelancetoncology for information for authors see authors / oncology / authorinfo goldhirsch a , wood wc , gelber rd , et al . 
ann oncol 2007 ; 18 : 113344 . arimidex , tamoxifen , alone or in combination ( atac ) trialists group.e ect of anastrozole and tamoxifen as adjuvant treatment for early - stage breast cancer : 100 - month analysis of the atac trial . 
skeletal e ects of exemestane on bone - mineral density , bone biomarkers , and fracture incidence in postmenopausal women with early breast cancer participating in the intergroup exemestane study ( ies ) : a randomised controlled study . 
eur j cancer 2006 ; 42 : 296875 . call for papers : lung cancer , storyboard , and from the archives in 2007 the lancet oncology published themed issues on paediatric oncology and on breast cancer . 
despite many advances in treatment over recent years , lung cancer is still the number one cause of death due to cancer in the world1 and mean relative 5 - year survival is only 126% in europe2 . 
accepted in the lancet oncology papers will be published to coincide with the international lung cancer conference ( [ ilcc ] liverpool , uk , july 912 , 2008 )  . 
if your study describes , in part or wholly , a study accepted for presentation at the ilcc , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication in the lancet oncology can be scheduled to comply with ilccs embargo policies . 
articles should be submitted via the lancet oncologys online submission service , and all authors must clearly state in the covering letter that their submission is in response to the lung cancer call for papers . 
 storyboard will provide and entertaining opportunity to present new oncological in pictorial form and will allow the techniques progressive accumulation of knowledge by leading a reader from panel - to - panel . 
from the archives will be a short report based on a reference of historical importance in oncology that has contributed to a substantial change in thinking in the era originally published . 
please see our information for authors for full details of these new sections . lidia siemaszkiewicz the lancet oncology , london nw1 7by , uk parkin dm , bray f , ferlay j , pisani b . 
the last two sentences of the summarys findings should have read st gallen guidelines identi ed 353 ( 83% ) patients with poor prognosis and discordance with the signature in 168 ( 39% ) patients . 
national data on cancer patient survival in england and wales up to 2007 thus o er the opportunity for a rst formal assessment of the cancer plan in england , by comparing survival trends in england with those in wales before , during , and after the implementation of the plan . methods we analysed population - based survival in 22 million adults diagnosed with one of 21 common cancers in england and wales during 19962006 and followed up to dec 31 , 2007 . 
we estimated year - onyear trends in 1 - year relative survival for patients diagnosed during each period , and changes in those trends between successive periods in england and separately in wales . 
life tables for single year of age , sex , calendar year , deprivation category , and government o ce region were used to control for background mortality in all analyses . findings 1 - year survival in england and wales improved for most cancers in men and women diagnosed during 19962006 and followed until 2007 , although not all trends were signi cant . 
northsouth di erences in survival trends for the four most common cancers were not striking , but the north west region and wales showed the smallest improvements during 200103 and 200406 . interpretation the ndings indicate slightly faster improvement in 1 - year survival in england than in wales during 200406 , whereas the opposite was true during 200103 . 
these di erent patterns of survival suggest some bene cial e ect of the nhs cancer plan for england , although the data do not so far provide a de nitive assessment of the e ectiveness of the plan . funding o ce for national statistics ( contract nt - 04 / 2355a ) ; cancer research uk ( programme grant c1336 / a5735 )  . introduction in 1995 , the expert advisory group on cancer published the calman - hine report , 1 in which they recommended that strategic improvements be made to cancer services in england and wales . 
by 1999 , progress in improving cancer services was seen as inadequate.2 the national health service ( nhs ) cancer plan for late 2000.3 it was a england was published comprehensive 10 - year strategy , designed to improve prevention , early diagnosis , and screening , and to provide optimal thus improving survival and quality of life . 
 annual funding for cancer services rose by about 35% in real terms over the three nancial years from 2001 to 2004 . in wales , the cancer services expert group recommended substantial changes to cancer services in 1996.4 changes included the creation of mdts and the designation of specialist clinicians , but the approach relied heavily on clinical collaboration , supported by directives from the devolved administration , rather than on a formal strategy . 
the full national cancer plan for wales , designed to tackle cancer , 5 was not published until late 2006 . 3 - year progress reports on the nhs cancer plan were published in october , 2003 , 6 , 7 when , despite substantial progress , it was acknowledged that it would take time vol 10 april 2009 articles the di culty of before the e ects of the plan could be assessed . 
 given introducing systematic , nationwide changes in the nhs , it would be surprising if survival trends for patients diagnosed in england during 200103 were to di er much from earlier trends as a direct result of the plan . 
however , for patients diagnosed during 200406 , at least 3 years after implementation of the plan , any marked improvements in the overall e ectiveness of cancer services might reasonably be expected to show an e ect on trends in short - term survival . given the later implementation of a strategic cancer plan in wales , comparison of survival trends in england and wales over the same calendar periods could be instructive . 
but an observational comparison of outcomes before and after the introduction of a plan in one of two adjacent countries , with similar societies and health systems , seemed to be a reasonable alternative . 
1 - year survival trends might be expected to accelerate more rapidly in successive calendar periods in england than in wales after the introduction of the plan , if the plan was e ective . 
3 - year survival trends might also be di erent in england and wales . on dec 10 , 2008 , the o ce for national statistics ( ons ) published the o cial national statistics on survival for patients diagnosed with one of 21 common cancers in england during 200004 and followed up to 2005.8 national statistics on survival for cancer patients diagnosed in england during 200106 and followed up to dec 31 , 2007 , were published on march 20 , 2009.9 we have used these data , and the data for all cancer patients diagnosed in wales , to study national and regional trends in survival up to the end of 2007 . methods data collection population - based cancer registries collect a small standard dataset for all cancer patients in a de ned population . 
since 1971 , the national health service central register ( nhscr ) has provided noti cation of the deaths of all cancer patients whose record was successfully agged with details of the initial cancer registration . data for this study were extracted from the national cancer registry at the ons after the linkage of cancer records with data on the patients vital status ( alive , emigrated , dead , not traced ) at nhscr . 
after powers to legislate on health policy were devolved to uk national assemblies from 1997 , cancer registration in wales passed to the welsh cancer intelligence and surveillance unit , but the national cancer registry at the ons continues to receive cancer data from wales , and the vital status of all cancer patients in england and wales is updated by the ons . 
when the data were extracted on oct 17 , 2008 , the vital status at dec 31 , 2007 , was known for 996% of patients diagnosed with cancer during 19962006 , without regional variation . 
the data were received on dec 15 , 2008 . cancers were de ned by their anatomical location ( site ) , morphology , and behaviour ( benign , in situ , or invasive )  . 
tumour site was coded according to the tenth revision of the international classi cation of diseases ( icd - 10 ) .10 morphology and behaviour were coded according to the second edition of the international classi cation of diseases for oncology ( icd - o - 2 ) .11 we examined data for 21 common cancers , 17 in men and 18 in women . 
 standard criteria were used to decide whether a tumour record was eligible for inclusion in the analyses.12 records were excluded if they contained data of inadequate quality or were for patients not resident in england or wales . 
125 million of 84 million patients registered with benign tumours ( behaviour code 0 ) , tumours of uncertain behaviour ( code 1 ) , in - situ neoplasms ( code 2 ) or a metastasis ( code 6 ) were not included . 
of 7 043 765 patients with an invasive primary malignancy eligible for survival analysis during 19712006 , 6 436 299 ( 914% ) had one of the 21 cancers selected for analysis , of whom 2 338 785 were diagnosed during 19962006 . 
62% of patients were excluded because their survival was either zero or unknown ( tumour registered from a death certi cate only [ dco ] ) , and 14% of patients were excluded because of unknown vital status or sex , duplicate registration , synchronous tumours , or invalid dates or sequences of dates . 
 352 vol 10 april 2009 articles the government o ce regions of england have provided a geographic focus for public - health policy in england since 1999 , and have been closely linked with the new nhs strategic health authorities since 2006.13 we analysed the cancer data for each region , for england as a whole , and separately for wales . statistical analysis survival trends were quanti ed as the year - on - year rate of change within each calendar period . 
the di erence in survival trends between successive calendar periods provides a measure of any acceleration ( or deceleration ) in the rate of change in survival between successive periods . 
di erences or trends are given as the simple arithmetic values ; so 12% is reported as 2% ( not 20% ) higher than 10% , and a rise from 10% to 14% over 4 years is reported as an increase of 1% per year . we estimated relative survival for england , for wales , and for the nine government o ce regions of england , for each cancer , each sex , and by year or period of diagnosis . 
relative survival is the ratio of the observed probability of survival and the probability that would have been expected if the cancer patients had only experienced the normal ( background ) mortality of the general population in which they live , 14 , 15 given the same distribution of factors such as age , sex , geographic area , calendar period , and deprivation . 
it does not rely on accurate reporting of the cause of death , 16 and it enables the estimation of longterm survival from cancer , when competing causes of death become more important.17 it can be interpreted as survival from cancer after adjustment for other causes of death . expected survival is derived from population life tables . 
background mortality rates by age and sex di er widely between socioeconomic groups and geographic regions in england and wales , 18 and these di erences have changed over time . 
we therefore constructed life tables ( available online19 ) of all - cause death rates by single year of age ( 099 years ) , sex , deprivation category , and government o ce region for 1991 , 2001 , and 2005 , using the mid - year population estimates and the mean annual number of deaths during the 3 years centred on the index year . 
life tables for 2006 and 2007 could not be constructed because the relevant data ( deaths during 200708 ) were unavailable , so life tables for 2005 were used for those years without extrapolation . 
national and regional analyses for england were all done with life tables speci c for sex , government o ce region , deprivation category , and calendar year from 1996 . five deprivation categories were de ned from quintiles of the income domain score of the indices of multiple deprivation ( imd2004 ) , 20 and the equivalent indices for wales , 21 using administrative data for the icd - 10 * code exclusions ( % ) eligible for analysis number of patients included ( % ) dco zero survival other c19c21 c33 , c34 c54 , c55 c56 , 570577 c64c66 , c68 71 205 88 637 213 077 125 458 70 897 17 281 366 597 74 004 411 299 29 077 59 567 66 383 300 301 18 679 63 650 112 712 39 220 13 655 oesophagus stomach colon rectum pancreas larynx ( men ) lung melanoma breast ( women ) cervix uterus ovary prostate testis kidney bladder brain hodgkins disease non - hodgkin lymphoma myeloma leukaemia c91c95 total 36 866 67 034 2 338 785 106 66 829 ( 939 ) 81 517 ( 920 ) 195 108 ( 916 ) 120 023 ( 957 ) 59 272 ( 836 ) 16 624 ( 962 ) 323 157 ( 882 ) 71 935 ( 972 ) 384 442 ( 935 ) 27 998 ( 963 ) 57 306 ( 962 ) 61 385 ( 925 ) 284 310 ( 947 ) 18 194 ( 974 ) 57 536 ( 904 ) 107 398 ( 953 ) 36 171 ( 922 ) 13 305 ( 974 ) 33 865 ( 919 ) 59 692 ( 890 ) 2 163 274 ( 925 ) c82c85 93 186 87 207 ( 936 ) all patients were aged 1599 years . 
aged 100 years or over at diagnosis , vital status or sex unknown , sex - site error , invalid dates , duplicate registration , synchronous tumours , or a previous cancer of the same organ or tissue at some time since 1971 . table 1 : number of patients eligible and included for analysis , and percentage exclusions , for adults diagnosed with one of 21 common cancers in england and wales between 19962006 and followed up to 2007 lower super - output areas ( lsoas , mean 34 378 population 1500 ) 22 in england ( 2001 ) and wales ( 200204 )  . 
cancer patients were assigned to the deprivation category of their lsoa , using the postcode of residence at diagnosis and a combined historic le of 21 million unique full postcodes , each linked to a complete set of geographic area codes for each year that the postcode was active . 
death records were assigned to deprivation categories using the postcode and lsoa in the same way as the cancer cases , so that background mortality was precisely matched to the small areas of residence and deprivation categories of the cancer patients . 
although socioeconomic inequalities ( the socalled deprivation gap ) in survival have been widening for many adult cancers in england and wales , 23 tending to reduce the overall national gain in survival , recent trends in the deprivation gap in survival will be reported separately . survival probabilities were estimated at short ( for example , 1 - month ) intervals in the rst few months vol 10 april 2009 articles calendar years within which follow - up probabilities are used to estimate survival 1996 1997 1998 1999 2000 2001 2002 2003 2004 2005 2006 2007 1996 1997 1998 1999 2000 2001 2002 2003 2004 2005 2006 survival data used in cohort analysis survival data used in hybrid analysis 1996 1997 1998 1999 2000 2001 2002 2003 2004 2005 2006 survival data used in complete analysis figure 1 : structure of survival analyses in relation to nhs cancer plan , patients diagnosed 19962006 and followed up to 2007 numbers in the cells indicate the minimum number of years of follow - up completed by patients surviving to the end of a given calendar year ( columns ) who were diagnosed in the index year ( rows )  . 
conditional 5 - year survival is restricted to those who had survived at least 1 year ; ie , excluding follow - up in shaded cells . after diagnosis , then at progressively longer intervals up to 10 years after diagnosis , using the maximumlikelihood approach for individual data.24 we report the cumulative probabilities of relative survival at 1 , 3 , 5 , and 10 years after diagnosis . 
we also report 5 - year survival for patients who survived at least 1 year after their diagnosis ( conditional survival )  . given the structure of the data , various analytical approaches were required . 
the classical ( cohort ) approach was suitable for the analysis of year - on - year trends in 1 - year survival , since all patients were followed up at least that long ( gure 1 )  . 
short - term prediction of survival for patients diagnosed during 2007 was made with the hybrid approach , 25 combining the 1 - year survival probability for patients diagnosed during 2006 with the survival probabilities for the second and later years after diagnosis for patients who were alive and followed up for at least part of 2007 . 
conditional 5 - year survival was available with the cohort approach for 19962000 , the complete approach for 200103 , and the period approach26 for 200406 ( gure 1 )  . year - on - year trends in survival were estimated within a single variance - weighted linear regression27 model covering all 11 years and each calendar period , including two extra parameters in addition to the baseline trend , to allow for di erent trends in successive periods . 
we report changing survival trends as the absolute di erence between the regression slopes for each calendar period : a positive value implies acceleration of the upward trend in survival and a negative value implies deceleration ( see webappendix )  . 
 survival analyses were done with the publicly available stata program strel.28 other analyses were programmed in stata version 10.29 we constructed funnel plots30 to visualise the regional variability of 1 - year survival in england and wales for cancer patients diagnosed during 200406 . 
the plots allowed us to estimate how much a particular estimate of survival deviates from the pooled england value ( the target ) , given the precision of each estimate . 
the target value , taken as the estimate of 1 - year relative survival pooled across the nine regions of england for all patients diagnosed during 200406 , is represented by the horizontal line in each plot . 
the 95% and 998% control limits , derived from the complementary loglog transformation of the target estimate for england across the observed range of precision of the regional estimates , 31 represent approximately three standard deviations , respectively , from the target value at each level of precision ( webappendix )  . 
estimates that lie inside the control limits were considered as within the geographical variation that could be expected by chance . two and funnel plots were also constructed to show regional variation in the year - on - year trend in 1 - year survival during 200406 . 
the target value in each plot was set as the mean absolute change per year between the 1 - year relative survival estimates for all patients in england diagnosed in the single years 2004 , 2005 , and 2006 . 
the control limits were constructed on the assumption that the target value for the year - on - year change in survival follows a normal distribution ( see webappendix )  . this analytical strategy , including de nition of the calendar periods , the cancers , life tables , approaches to estimation of survival and survival trends , and the structure of the tables and graphics , was speci ed in advance , after data preparation was complete but before the start of any analyses . 
this was done to pre - empt any concerns regarding possible data - dredging in favour of a particular conclusion , whether for or against the e ectiveness of the nhs cancer plan . legal authority to hold the cancer data derives from a contract with the ons to produce the o cial national statistics32 on cancer survival . 
approval to analyse the data was obtained from the ons medical research service ( mr1101 , nov 20 , 2007 ) and from the statutory patient information advisory group ( piag ; now the ethics and con dentiality committee of the national information governance board ) under section 61 of the health and social care act 2001 ( piag 1 - 05 ( c ) / 2007 , july 31 , 2007 )  . 
the cancer survival group ( br , un , mq , le ) at the lshtm has been funded by cancer research uk ( grant c1336 / a5735 ) since april , 2005 . 
neither cancer research uk nor the ons had any role in study design , data collection , analysis , interpretation of the data , or the writing of this article . 
the corresponding author had full access to all the data and the nal responsibility to submit for publication . results 1 - year survival improved for most cancers in patients diagnosed during 19962006 and followed until 2007 , for both sexes and in england and wales . 
for patients diagnosed in 2006 , 1 - year survival was over 60% for 25 of the 35 cancersex combinations , both in england and wales ( table 2 )  . 
for cancers of the oesophagus , stomach , pancreas , lung , and brain , 1 - year survival was poor , in the range 1520% ( pancreas ) and rarely over 40% , despite noticeable improvement for some cancers ( oesophagus , stomach , brain among men in england , oesophagus in wales )  . 
table 2 summarises temporal trends in 1 - year survival , both for the entire period 19962007 and in each of the three calendar periods . for patients diagnosed in england during 19962000 , before the nhs cancer plan , 1 - year survival increased signi cantly ( p < 005 ) for eight of 17 cancers in men and for 12 of 18 cancers in women . 
the annual increase was about 1% for cancers of the oesophagus , stomach , and prostate in men , and for cancers of the oesophagus , stomach , and kidney among women . 
the pattern was similar in wales , but the trends were statistically signi cant less often because of the much smaller population . during 200103 , survival for most cancers did not increase , or else the upward trends observed for 19962000 were attenuated . 
the steep increase in 1 - year survival for non - hodgkin lymphoma is a notable exception : in wales , 1 - year survival rose by about 1% a year during 19962000 , and by 2% a year during 200103 ( 1% a year in england )  . for patients diagnosed during 200406 , 1 - year survival in england increased again for most cancers . 
||not enough data to be estimated . table 3 : national trends in relative survival ( % ) at 3 , 5 , and 10 years after diagnosis , and 5 - year conditional survival , by sex and calendar period of diagnosis , and predicted survival for 2007 were not always statistically signi cant . 
in wales , by contrast , survival fell for 19 of the 35 cancersex combinations , although none of the declines were signi cant . another way to summarise the contrast is to examine the di erences between england and wales in survival trends within each of the three periods . 
during 19962000 , the annual increase in 1 - year survival was greater in wales than in england for 14 of 17 cancers in men and eight of 18 cancers in women . 
the situation was similar during 200103 , with survival trends for eight of 17 cancers in men and 16 of 18 cancers in women in wales slightly more favourable than in england and only seven less favourable . 
however , this pattern was reversed during 200406 , when annual trends in england were more favourable than in wales for 11 of 17 cancers in men and 12 of 18 cancers in women . longer - term survival was estimated for each calendar period and predicted for 2007 , as was the change in ( table 3 )  . 
 survival between in england , both 3 - year and 5 - year survival improved successive periods 362 vol 10 april 2009 between 19962000 and 200103 for most tumours , except those of the bladder and brain ( both sexes ) , and hodgkins disease ( men only )  . 
the picture in wales was similar , but there was no improvement for tumours of the bladder or brain in men , or for tumours of the kidney or brain in women . 
the improvements in longer - term survival are similar to the earlier increases in 1 - year survival in both countries . changes in 3 - year survival between 200103 and 200406 in both england and wales were similar to those observed between 19962000 and 200103 , with no clear trend emerging . 
between the periods 19962000 and 200103 , survival increased more quickly in wales than in england for 12 of 17 cancers in men and 13 of 18 cancers in women . 
the di erent timing of increases in 3 - year survival between england and articles england 19962000 wales 19962000 england 200406 wales 200406 oesophagus stomach colon rectum pancreas larynx lung melanoma prostate testis kidney bladder brain hodgkins disease non - hodgkin lymphoma myeloma leukaemia women oesophagus stomach colon rectum pancreas lung melanoma breast cervix uterus ovary kidney bladder brain hodgkins disease non - hodgkin lymphoma myeloma leukaemia 3 - year relative survival ( % ) 3 - year relative survival ( % ) figure 2 : 3 - year relative survival ( % ) for adults diagnosed with 21 common cancers during 19962000 and 200406 in england and wales vol 10 april 2009 articles 05 10 1 - year relative survival ( % ) 200406 annual trend ( % ) 200406 colon ( men ) colon ( men ) colon ( women ) colon ( women ) breast ( women ) breast ( women ) lung ( men ) lung ( men ) precision of the survival estimate precision of the annual trend estimate figure 3 : funnel plots of 1 - year relative survival ( % ) and year - on - year trend ( % ) during 200406 : selected cancers , by sex , in the nine government o ce regions of england , and wales all patients were adults aged 1599 years , and were diagnosed during 200406 . 
control limits are shown by coloured curves : the inner limits are for 95% , the outer limits are for 998% . wales produced similar overall changes during 19962006 , as shown for each sex in gure 2 . the northsouth gradient in cancer survival in england31 is only partially con rmed . 
the gradient was present in the case of colon cancer , but it has been attenuated by increases in survival in so - called lowsurvival regions over the period 19962006 ( table 4 )  . 
 even so , the funnel plots show that the south west region ( gure 3 , symbol k ) was still a high - survival outlier in 200406 , while the north west region ( gure 3 , symbol b ) was still a low - survival outlier . very little regional variation in breast - cancer survival was seen in england , where 1 - year survival was close to 95% for women diagnosed during 19962000 and 96% for those diagnosed in 200103 , and 92% and 94% , respectively , in wales ( table 4 )  . 
 survival in the north west ( gure 3 , symbol b ) is lower than the pooled english value : the di erence is small , but the value is below the 998% control limits , and the downward annual trend during 200406 is outside the control limit . 
1 - year survival in wales ( gure 3 , symbol w ) during 200406 was also below the control limits , but the year - on - year trend during that period was positive , and within the control limits . despite gradual improvement , 1 - year relative survival from lung cancer remains poor , around 27% for men diagnosed during 200406 ( table 4 )  . 
1 - year survival in the yorkshire and humber region ( gure 3 , symbol d ) and wales ( gure 3 , symbol w ) was below the lower 95% control limit in that period , whereas survival in the london region ( gure 3 , symbol h ) was above the upper limit . 
again , the annual trend in the north west region ( gure 3 , symbol b ) during 200406 was just below the lower 95% control limit , whereas the trend in the west midland region ( gure 3 , symbol f ) was above the upper limit . discussion cancer survival , especially at 1 year after diagnosis , improved for most of the 21 cancers examined , both in england and wales , during the period 19962007 . 
 the rst group , with a generally poor prognosis , consists of ve cancers for which 1 - year survival is often below 40% in men and women : cancers of the oesophagus , stomach , pancreas , lung , and bra survival from cancers of the pancreas and lung has hardly improved at all between 19962007 , and 1 - year survival for pancreatic cancer remains below 20% . 
 the range of survival in the group of cancers with higher survival has tended to narrow over time , because of a ceiling e ect among malignancies for which 1 - year survival is already 90% or higher : melanoma of the skin and cancers of the breast , uterus , prostate , and testis , and in england only , hodgkins disease . 
part of the increase in survival for prostate cancer may be attributable to the diagnosis of more indolent tumours as a result of widespread prostate - speci c antigen ( psa ) testing . a key aim of the nhs cancer plan for england , published in september , 2000 , was to improve the prospects of survival for cancer patients . 
the availability of 6 years of data on incident cancers in both england and wales since the publication of the cancer plan provided an early opportunity to examine its e ect . 
for a number of cancers including stomach , colon , rectum , cervix , uterus , ovary , and kidney , survival trends in england improved between 200103 and 200406 in the absence of screening or the widespread delivery of more e ective new treatments . 
the di erent time trends in england and wales suggest that those recent gains might be attributable to improvements in cancer care , including earlier diagnosis and more widespread adherence to treatment guidelines . 
although cancer services in wales undoubtedly improved after the publication of the cameron report , clinical cancer outcomes and cancer information were not given such high priority by hospital trusts as in england after the publication of the nhs cancer plan . we identi ed no di erence between england and wales in survival trends at 3 years or more after diagnosis for patients diagnosed up to 2003 . 
the more rapid increase in shortterm survival in england than in wales since 2004 could be interpreted as related to the cancer plan , but we do not have evidence of the extent to which the various initiatives in the cancer plan were fully implemented by that time . 
 even so , predicted 3 - year survival for cancers diagnosed in 2007 in england was generally higher than for 200406 , suggesting that survival is likely to continue to increase . 
 by contrast , there are fewer predicted improvements in survival in wales . one aspect that suggests the results are plausible is the similarity of survival patterns between men and 366 vol 10 april 2009 articles women in each country . 
thus , the recent upward trend in 1 - year survival in england occurred in both sexes , while a levelling o of the trends was also seen in both sexes in wales . 
the use in all analyses of region - speci c and deprivation - speci c life tables for each calendar year and each sex ensured that the background mortality used to estimate relative survival corresponded as closely as is feasible to that of each cancer patient . socioeconomic inequalities in survival have been widening for many adult cancers in england and wales.8 the nhs cancer plan aimed to reduce socioeconomic inequalities ( the deprivation gap ) in survival . 
although that objective has not yet been fully assessed , and despite real recent improvements in 1 - year survival in some of the more deprived regions , the previously described northsouth gradient for cancer survival33 and other socioeconomic and health - related parameters18 is still present , and relative survival for most cancers in the more a uent southern regions is generally higher than the mean survival for england . 
 the funnel plots presented in gure 3 ( and webappendix ) provide insight into regional variation in survival and whether recent trends will enable regions with low survival to catch up . 
to the extent that gains in survival are less marked among more deprived groups than more a uent groups , this will reduce the overall national trends in survival , and thus the overall e ectiveness of the plan . the survival estimates reported here are not agestandardised because the age distribution of cancer patients was fairly stable for most cancers during this short period ( 11 years )  . 
a notable exception was hodgkins disease , for which the marked fall in survival during 200406 was partly due to an increase in the age at diagnosis of patients diagnosed with this malignancy : the mean age at diagnosis increased by about 3 years between 1998 and 2005 . 
 incidence of the 21 cancers examined was generally stable over the period 19962006 , except for a rise in cancers of the prostate and breast , and melanoma of the skin , and a fall in cancers of the lung and stomach in men . 
 the fall in survival in england is mainly attributable to progressive change in the recorded spectrum of urothelial malignancies , pathological classi cation and coding34 that have not yet occurred to the same extent in wales . following changes patients who had previously had a primary malignancy in a di erent organ or tissue were included in these analyses , by contrast with our previous work.23 , 35 this was done mainly because of the marked increase of asymptomatic prostate cancer detected by psa , since these men have extremely high survival , which would arti cially raise the proportion of patients excluded for a previous primary cancer . 
survival estimates were virtually identical with and without the exclusion of patients with more than one tumour ( data not shown )  . in the past , patients who died on the date of diagnosis could not be distinguished in the national cancer registry data from dco registrations , for which the true duration of survival is unknown.9 a ag to indicate dco status is now available for more than 90% of cancers registered since 1996 in england and wales , but we excluded both dco registrations and other cases with zero recorded survival , for consistency with most other publications on cancer survival . 
inclusion of those patients who do appear to have died on the same day as the diagnosis ( no dco ag ) would have reduced the estimates of 1 - year survival for some cancers by up to 1% , but it had no e ect on the estimated trends in survival ( data not shown )  . successive eurocare studies have shown that cancer survival in both england and wales has lagged behind other countries in western and northern europe , despite encouraging recent results showing that both countries have tended to approach the levels of survival in other european countries during 19952002.36 the eurocare studies formed part of the impetus to create the nhs cancer plan.2 a recent editorial37 questioned whether the uk really has an e ective cancer plan , on the basis of ndings in the eurocare - 4 study , 36 which included patients diagnosed up to 2002 . 
however , the nhs cancer plan only dates from 2000 , so the eurocare - 4 study cannot o er a fully viable european comparison of survival trends after its implementation . 1 - year survival is the only cohort - based measure of outcome that is available for the whole period up to 2006 . 
even 3 - year survival can only be estimated for patients diagnosed during 200406 by using the complete approach , and no estimation of 5 - year survival for 200406 is currently possible without using the hybrid approach to incorporate follow - up data for patients who were diagnosed ( and whose treatment will have begun ) in earlier periods ( gure 1 )  . 
 international di erences38 and , in england and wales , socioeconomic di erences23 in 5 - year survival are largely attributable to higher cancer - related mortality soon after diagnosis . implementation of the data analysed here represent the earliest period from which an overall assessment of survival trends after the cancer plan could reasonably be attempted . 
recent survival trends in england , more favourable than those in wales , do indicate that the nhs cancer plan is having some bene cial e ect in england . our ndings do not , however , provide a de nitive verdict on the overall e ectiveness of the cancer plan . 
 vol 10 april 2009 articles the national data include over 2 million cancer patients and they are remarkably up to date , with follow - up data available to dec 31 , 2007 . 
but even with a large and timely dataset , and the latest techniques to assess recent survival trends , it seems we will need at least 3 years of follow - up data for all patients diagnosed during the period 200406 , up to the end of 2009 . 
incorporation of survival trends in scotland and northern ireland in the same analytical strategy might improve the evaluation of national cancer plans in the uk . finally , it is essential to do more detailed analyses to investigate the e ect on time trends and regional inequalities in cancer survival of some of the more speci c measures listed in the cancer plan and the cancer reform strategy , 40 such as mdts , shorter waiting times for investigation and treatment , and the training and specialisation of surgeons and other specialists . 
such studies will require more prompt and e cient linkage of the national cancer dataand linkage to a wider range of health datasetsthan is currently possible , as well as new ways of using this information to improve health policy . contributors mpc and br led the study design . 
all authors revised the report . con icts of interest the authors declared no con icts of interest . acknowledgments we thank the cancer registry sta in england and wales : their sustained data collection and quality control have enabled the survival of patients to be analysed and compared in this study . 
we also thank nicola cooper , susan westlake , and domenica rasulo of the cancer team at the ons for extensive work in preparing the data in the national cancer registry . 
the ndings and conclusions in this report are those of the authors and do not necessarily represent the views of the ons or the welsh assembly . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology department of radiation oncology , all india institute of medical sciences , new delhi , india sharmadn@hotmail.com the authors declared no con icts of interest . powell jw , dexter e , scalzetti em , bogart ja . 
long term results of endobronchial brachytherapy : a curative treatment ? int j radiat oncol biol phys 2007 ; 67 : 42530 . brach b , buhler c , hayman mh , joyner lr jr , liprie sf . 
 chest 2005 ; 127 : 223742 . screening newborns for tp53 in the september issue of the lancet oncology , achatz and colleagues1 discuss the possibility of screening newborns in southeast brazil for a highly prevalent tp53 mutation ( 1 : 300 individuals ) that predisposes to many cancers . 
the authors present the justi cations and the problems associated with such a screening e ort , and conclude that on the basis of current scienti c and medical knowledge the r337h mutation does not meet all the criteria for mass newborn screening . 
 in my opinion , this type of screening will never meet the criteria for newborn screening , which is intended to detect conditions for which the population is at risk but there is no other way to assess risk in newborns . 
newborn screening is done for sporadic diseases such as congenital hypothyroidism and autosomal recessive disorders , in which carrier detection is di cult or impossible , but never applies for a disorder caused by the presence of a founder dominant mutation . 
a founder mutation in a newborn will be carried by one of the parents , so the detection of the child can be done by knowing who the adult carrier is . 
cascade screening is the most economically e ective , o ering the screening test to rst - degree relatives of carriers of the mutation , and several countries have chosen this approach.2 the problem with this type of screening is that it involves the cooperation of relatives who are not always willing , and so an alternative has been the creation of databases to store information on patients.3 in my view , population screening of informed and consenting adults is much better suited for the tp53 mutation . 
 this approach identi es families at risk and has been implemented in pilot studies for haemochromatosis.4 as emphasised by achatz and colleagues , 1 such population screeningin the context of appropriate genetic counsellingallows at - risk families the informed decision of whether or not to test the probands o spring . joel zlotogora department of community genetics , ministry of health , jerusalem , israel joelz@cc.huji.ac.il the author declared no con icts of interest . achatz miw , hainaut p , ashton - prolla p . 
 clin genet 2004 ; 66 : 48387 . had eld sg , horara s , starr bj , et al ; steering group for the department of health familial hypercholesterolaemia cascade testing audit project . 
lancet oncol 2009 ; 10 : 940in this news report , the nal sentence of the 90y radioembolisation paragraph should have read only one patient experienced radiation - induced pneumonitis ; three had gastrointestinal ulcers that did not require surgical treatment , and radioembolisation - induced liver disease was noted in 24 patients ( fatal for four )  . huober j , thrlimann b . 
lancet oncol 2009 ; 10 : 102829in this re ection and reaction , the a liation for both authors should read breast center , kantonsspital st gallen , 9007 st gallen , switzerland . 
the authors would also like to thank karen price for her useful comments on the article . 1142 vol 10 december 2009 articles sensitivity and speci city of multimodal and ultrasound screening for ovarian cancer , and stage distribution of detected cancers : results of the prevalence screen of the uk collaborative trial of ovarian cancer screening ( ukctocs ) usha menon , aleksandra gentry - maharaj , rachel hallett , andy ryan , matthew burnell , aarti sharma , sara lewis , susan davies , susan philpott , alberto lopes , keith godfrey , david oram , jonathan herod , karin williamson , mourad w seif , ian scott , tim mould , robert woolas , john murdoch , stephen dobbs , nazar n amso , simon leeson , derek cruickshank , alistair mcguire , stuart campbell , lesley fallow eld , naveena singh , anne dawnay , steven j skates , mahesh parmar , ian jacobs summary background ovarian cancer has a high casefatality ratio , with most women not diagnosed until the disease is in its advanced stages . 
 methods between 2001 and 2005 , a total of 202 638 post - menopausal women aged 5074 years were randomly assigned to no treatment ( control ; n = 101 359 ) ; annual ca125 screening ( interpreted using a risk of ovarian cancer algorithm ) with transvaginal ultrasound scan as a second - line test ( multimodal screening [ mms ] ; n = 50 640 ) ; or annual screening with transvaginal ultrasound ( uss ; n = 50 639 ) alone in a 2 : 1 : 1 ratio using a computer - generated random number algorithall women provided a blood sample at recruitment . 
 the main reasons for withdrawal were death ( two mms , 28 uss ) , non - ovarian cancer or other disease ( none mms , 66 uss ) , removal of ovaries ( ve mms , 29 uss ) , relocation ( none mms , 39 uss ) , failure to attend three appointments for the screen ( 72 mms , 757 uss ) , and participant changing their mind ( 483 mms , 1490 uss )  . 
 overall , 4355 of 50 078 ( 8.7% ) women in the mms group and 5779 of 48 230 ( 120% ) women in the uss group required a repeat test , and 167 ( 03% ) women in the mms group and 1894 ( 39% ) women in the uss group required clinical evaluation . 
28 ( 16 mms , 12 uss ) of 58 ( 483% ; 95% ci 350618 ) of the invasive cancers were stage i / ii , with no di erence ( p = 0396 ) in stage distribution between the groups . 
the sensitivity , speci city , and positive - predictive values for all primary ovarian and tubal cancers were 894% , 998% , and 433% for mms , and 849% , 982% , and 53% for uss , respectively . 
for primary invasive epithelial ovarian and tubal cancers , the sensitivity , speci city , and positive - predictive values were 895% , 998% , and 351% for mms , and 750% , 982% , and 28% for uss , respectively . 
there was a signi cant di erence in speci city ( p < 00001 ) but not sensitivity between the two screening groups for both primary ovarian and tubal cancers as well as primary epithelial invasive ovarian and tubal cancers . interpretation the sensitivity of the mms and uss screening strategies is encouraging . 
 although advances in therapy have improved median survival during the past decade , there has been little or no change in the overall mortality rate.1 , 2 women are commonly diagnosed with stage iii / iv disease , for which 5 - year survival rates are around 27% and 16% , respectively.35 this has led to e orts over the past two decades to develop early detection strategies using serum ca125 and ultrasound.6 , 7 preliminary evidence from a previous randomised controlled trial suggests that screening sequentially with ca125 and ultrasound ( multimodal screening ) can result in a survival bene t.8 median survival was signi cantly increased in women who developed ovarian cancer in the screened group compared with the control group ( 729 vs 418 months , p = 00112 )  . 
improved survival has also been reported in a single - arm ultrasound - based study.9 re nements have been made to screening since the two previous studies , including the introduction of transvaginal ultrasound , 10 improvements in the interpretation of ultrasound ndings using morphology - based indices , 9 , 1113 and the development of a risk of ovarian cancer algorithm for the interpretation of serial ca125 results.14 , 15 the multicentre united kingdom collaborative trial of ovarian cancer screening ( ukctocs ) is a randomised controlled trial designed to provide de nitive data on the e ect of ovarian cancer screening on mortality , as well as comprehensively addressing the cost , acceptance , physical and psychosocial morbidity , and performance characteristics of multimodal screening and ultrasoundbased screening . methods participants women were recruited through 13 regional trial centres located in national health service ( nhs ) trusts in england , wales , and northern ireland.16 all women provided written consent . 
eligibility criteria included age panel 1 : classi cation of ovarian morphology on ultrasound normal ovary of uniform hypoechogenicity and with a smooth outline with or without a single inclusion cyst or spots of calci cations inclusion cyst must be single , less than 10 mm in diameter and not distort the outline of the ovary simple cyst a single , thin walled , anechoic cyst with no septa or papillary projections complex any case in which the ovary has any non - uniform ovarian echogenicity , excluding single simple or inclusion cysts 5074 years , and postmenopausal status de ned as greater than and including 12 months , amenorrhoea following a natural or surgical menopause , or greater than and including 12 months of hormone - replacement therapy commenced for menopausal symptoms.17 women were excluded if they had a history of bilateral oophorectomy , active malignancy ( women with a past history of malignancy were eligible if they had no documented persistent or recurrent disease and had not received treatment for > 12 months ) , previous history of ovarian cancer , participation in other ovarian cancer screening trials , or increased risk of familial ovarian cancer . 
high - risk women were eligible for a separate trial : the united kingdom familial ovarian cancer screening study ( ukfocss ) .18 the study was approved by the uk north west multicentre research ethics committee ( 00 / 8 / 34 ) , with site - speci c approval from the local regional ethics committees and the caldicott guardians ( data controllers ) of the participating primary care trusts . scanned electronically using procedures invitations to participate in the trial were sent to women aged 5074 years whose details were obtained from the age and sex registers of the participating 27 primary care trusts.16 on enrolment at the trial centres , women viewed an information video and participated in a group discussion before completing a datasheet , consent forms , and undergoing venepuncture . 
the recruitment questionnaires were sent to the coordinating centre , where they were com puterised intelligent character - reading and optical - mark - reading software ( teleform elite version 8.1.1 , cardi software inc , vista , ca , usa )  . 
any inconsistency or information not recognised by the data - capture software was veri ed manually by trained data - entry sta , who validated the computer - interpreted data . 
once the custom - built trialmanagement system con rmed eligibility , participants were randomly assigned to either no treatment ( control ) ; annual ca125 screening ( interpreted using a patented risk - of - ovarian - cancer algorithm ) with transvaginal ultrasound scan as a second - line test ( multimodal screening ; mms ) ; or annual screening with transvaginal ultrasound ( uss ) alone in a 2 : 1 : 1 ratio with a computergenerated random number algorith randomisation was done as follows : rst , the trial management system allocated a set of 32 random numbers to each trial centre ; second , the lowest eight were allocated to the mms group , the next eight to the uss group , and the remaining 16 to the control group ; third , each successive volunteer within the trial centre was randomly allocated one of the random numbers and so randomly assigned a group ; and nally , when all 32 random numbers had been used up a further set of 32 was generated . 
randomisation was accomplished by the trial - management system using the visual basic randomisation statement and the rnd function . 328 vol 10 april 2009 articles following randomisation , letters were automatically printed and sent to each woman and their general practitioner con rming eligibility and randomisation status . 
blood samples were taken in gel tubes ( 8 ml gel separation serum tubes ; greiner bio - one 455071 , stonehouse , uk ) at the trial centres and transported overnight at ambient temperature to the central laboratory . 
serum ca125 electroconcentrations were chemiluminescence sandwich immunoassay on an elecsys 2010 ( roche diagnostics , burgess hill , uk ) using two monoclonal antibodies ( oc125 and m11 ; fujirebio diagnostics ab , gteborg , sweden )  . 
the rst scan ( level 1 scan ) , and any repeat level 1 scans needed because of an type 1 unsatisfactory rst scan , were done by sonographers , who were certi ed sonographers , trained midwives , or doctors with experience in gynaecological scanning who were working in the nhs . 
detailed description of all features the number and size of cysts , wall regularity , presence and thickness of septae , size of papillations , and echogenicity of the uid contentswere recorded . 
cysts and complex morphology were classi ed pictorially , initially using the format reported in the kentucky screening trial , 19 and from 2003 onwards using the ( iota ) international ovarian tumour analysis classi cation.13 measurement of the ovary was important to con rm that it had been visualised , and for audit purposes . 
only cyst volume panel 2 : possible outcomes after level 1 and level 2 screens in the mms group level 1 screen normal risk of ovarian cancer score : women returned to annual screening , with the next level 1 blood test scheduled on the next anniversary of the randomisation date intermediate risk of ovarian cancer score : women were recalled for a repeat ca125 measurement 12 weeks after the screen . 
any women whose risk of ovarian cancer remained intermediate after three ca125 tests were referred for a level 2 screen elevated risk of ovarian cancer score : women were recalled for a level 2 screen in 68 weeks , with earlier screens arranged where there was a high index of suspicion level 2 screen women with a normal transvaginal ultrasound scan result and normal or intermediate risk of ovarian cancer returned to annual screening , with the next level 1 test on the next anniversary of the randomisation date women with a normal transvaginal ultrasound scan result but an elevated risk of ovarian cancer , or an unsatisfactory scan irrespective of risk of ovarian cancer status , underwent a repeat level 2 screen in 6 weeks and were triaged again on the basis of the results to annual screening or clinical assessment women with an abnormal transvaginal ultrasound scan were referred for clinical assessment irrespective of their risk of ovarian cancer status panel 3 : possible outcomes after level 1 and level 2 screens in the uss group level 1 screen women with a normal scan returned to annual screening , with the next level 1 transvaginal ultrasound scan on the next anniversary of the randomisation date women with an unsatisfactory scan result attended a repeat level 1 scan in 12 weeks . 
women were returned to annual screening following two unsatisfactory scans women with an abnormal level 1 scan were referred for a level 2 scan in 68 weeks , with earlier scans arranged where there was a high index of suspicion level 2 screen women with a normal level 2 scan returned to annual screening , with the next level 1 transvaginal ultrasound scan on the next anniversary of the randomisation date an unsatisfactory level 2 scan led to a repeat level 2 scan in 6 weeks or earlier , and women were triaged on the basis of the ndings to annual screening or clinical assessment women with an abnormal scan were referred for clinical assessment vol 10 april 2009 articles was used for scan classi cation . 
when ovaries were not visualised , the sonographers speci ed whether a good view of iliac vessels had been obtained or a poor view owing to obstruction by the bowel , broids , pelvic varicosities , or for other reasons . 
ascites was de ned as a maximum vertical pool measurement of greater than or equal to 10 m based on the visualisation and morphology of the ovaries , the scan was classi ed as either a normal scan , in which both ovaries had normal morphology or simple cysts less than 60 cm , or were not visualised but a good view of the iliac vessels was obtained ; an unsatisfactory scan , in which one or both ovaries were not visualised owing to a poor view ; or an abnormal scan , in which one or both ovaries had complex morphology or simple cysts greater than 60 cm , or ascites . scan images were transferred weekly on magnetooptical discs for central archiving . 
trial centres were able to request central review of ultrasound images . cancer using screening strategies in the level 1 screen in the mms group , women underwent venepuncture and serum ca125 measurement . 
the assay results were uploaded directly into the trial - management system , which calcu lated the risk of ovarian algorithm developed previously.15 , 17 the rst risk of ovarian cancer determination was based on a single measurement of ca125 and the womans age - speci c incidence of ovarian cancer . 
women were triaged into three risk groups on the basis of their risk of ovarian cancer , which determined whether they returned to annual screening or went on to have a repeat ca125 measurement or level 2 screen ( panel 2 )  . 
level 2 change rate and the the 202 638 women all had a blood sample taken at recruitment screening involved venepuncture for repeat ca125 assay and a transvaginal ultrasound scan . 
the results of the level 2 screen triggered three possible courses of action , as shown in panel 2 . the initial cuto s used for intermediate and elevated risk of ovarian cancer were greater than or equal to 1 / 1818 and greater than or equal to 1 / 500 , respectively . 
as the proportion of women classi ed into these risk categories were less than the proposed 15% and 2% , respectively , the cuto s were revised on april 1 , 2005 , to greater than or equal to 1 / 3500 and greater than or equal to 1 / 1000 after extensive data review by the independent data monitoring and ethics and trial steering committees . 
 there were three possible courses of action depending on the results of the level 1 scan , including referral for a level 2 scan , the results of which triggered one of a further three courses of action , as shown in panel 3 . 
 all clinicians were provided written information on the risk estimates for malignancy associated with the various morphological classi cations from the iota series once the estimates had been presented at the annual european society of gynaecological oncology meeting in 2003 . 
 additionally , clinicians were made aware that women who had previously undergone a hysterectomy had an incidence of adhesions and peritoneal increased pseudocysts that may be reported as multilocular adnexal cysts . clinical assessment this was undertaken by a designated clinician and included clinical evaluation and investigations as appropriate . 
these included serum ca125 in women in the ultrasound group , repeat transvaginal scans and doppler studies , ct / mri of the abdomen and pelvis , and occasionally assessment of other tumour markers . 
 for women in the mms group with a normal transvaginal ultrasound scan but elevated risk of ovarian cancer , clinical assessment included ruling out other causes of increased ca125 concentrations . 
the management plan took the views of the individual into account , and also accounted for any signi cant comorbidity , the speci c morphological features of the detected lesion , and history of a previous hysterectomy or major pelvic surgery that could be responsible for false - positive ultrasound appearances . for women who underwent surgery , the recommendation was removal of both ovaries and fallopian tubes for histopathological examination , even if the ovaries appeared macroscopically normal . 
where pelvic adhesions were present and there was an increased risk of complications , the clinician could opt to remove only the ovary found to have an abnormality on ultrasound and not proceed to remove the contra lateral ovary . 
a laparotomy was undertaken if clinical ndings or laparoscopy led to a strong suspicion of ovarian cancer , or if a laparoscopic procedure was not felt to be appropriate for other reasons . 
women found to have ovarian or tubal cancer at a primary laparoscopic procedure underwent a subsequent staging pro cedure . bilateral a follow - up plan was drawn up if , after clinical assessment , investigation , and discussion with the woman , a decision was made to manage the ndings conservatively . 
most women were followed up with a transvaginal ultrasound scan and a serum ca125 assessment at 3 months with a possible repeat at 6 months , and returned to annual screening if the ndings were unchanged at this review . 
 follow - up all participants are being followed up through a agging study with the nhs information centre for health and social care ( formerly o ce for national statistics , ons ) in england and wales , and with the central services agency and cancer registry in northern ireland . 
 additionally , women continued to attend for subsequent annual screens , and those who had been in the trial for 35 years following randomisation were sent follow - up questionnaires . 
 statistical analysis the primary outcome measure in ukctocs is ovarian cancer mortality and the primary comparison is based on an intention - to - treat analysis between the control group and both screened groups combined ( mms plus uss )  . 
 however , as the operating characteristics of the two screening groups are di erent a comparison between the control group and an individual screen group ( mms or uss ) is of equal interest . 
the design provides greater than 90% power to detect a 30% reduction in ovarian cancer mortality between the control and combined screening groups , and greater than 80% power to detect a 30% reduction in mortality between the control and either one of the individual screening groups , with both comparisons tested at a signi cance level of 005 . 
it is important to note that if one of the comparisons ( control vs mms or uss ) is signi cant and the other is not , the result would not necessarily imply that one method is signi cantly better than the other . 
if , as anticipated , the di erence in ovarian cancer mortality between the two screened groups is modest , then this study will have limited power to detect such di erences . 
the choice of screening strategy will then be based on other outcome measures such as sensitivity , positive - predictive value , morbidity , quality of life , and health economics . this paper presents the outcome of the prevalence screen in women randomly assigned to either mms or uss . 
the prevalence screen was de ned as a single or series of serum ca125 assays with or without transvaginal ultrasound scan ( mms ) or transvaginal ultrasound scan alone ( uss ) culminating in surgery or a return to annual screening . 
the screen was considered positive ( screen positive ) if the woman was referred for surgery and negative ( screen negative ) if the woman was returned to annual screening . 
the primary outcome measure was primary ovarian or fallopian tube cancer ( icd - 10 code c56 and c57.0 , respectively ) diagnosed within 12 months of the last scan or serum ca125 test in the prevalence screen . 
women with primary peritoneal cancer ( icd - 10 code c48.2 ) and those with ovarian neoplasms of uncertain behaviour ( icd - 10 code d39.1 ) were not included in the outcome measure . 
the most common reasons for withdrawal were death ( two mms ; 28 uss ) , non - ovarian cancer or other disease ( 66 uss ) , removal of ovaries ( ve mms ; 29 uss ) , relocation ( 39 uss ) , failure to attend three appointments for the screen ( 72 mms ; 757 uss ) , and participant changing her mind ( 483 mms ; 1490 uss )  . 
in accordance with good practice for randomised controlled trials we did not statistically compare the baseline characteristics of the women assigned to the two groups ; 20 , 21 the groups were well balanced ( table 1 )  . of the 50 078 women who underwent a prevalence screen in the mms group , 45 523 ( 909% ) were classi ed as low risk by the risk of ovarian cancer algorithm and returned to annual screening . 
in the course of the screen , ve women in the mms group died from unrelated causes , 24 were diagnosed with cancers other than ovarian cancer , and 215 withdrew from the trial . of the 48 230 women randomly assigned to the uss group , 42 416 ( 879% ) had transvaginal ultrasound scans , 4325 ( 90% ) had transabdominal ultrasound scans , and 1489 ( 31% ) had both . 
 six women in the uss group died from unrelated causes during the course of screening , seven were diagnosed with cancers other than ovarian cancer , and 252 withdrew from the trial . overall , 942 ( 095% ) of the 98 308 women screened underwent surgery as a result of the prevalence screen , with 87 women in the uss group undergoing surgery for every one woman from the mss group who underwent surgery . 
 there was a di erence in surgical approach between the two groups , with 75 of 97 ( 773% ) operations in the mms group involving laparotomy versus 397 of 845 ( 469% ) in the uss group ( table 2 )  . 
834 ( 47 mms , 787 uss ) women who underwent surgery were found to have benign pathology or normal ovaries ( table 3 ) , of whom 24 ( 29% ; 95% ci 1740 ) experienced a major complication . 
 * * three breast cancers , one endometrial cancer , and one cancer of the appendix . table 3 : histology in women who underwent surgery as a result of screening ( screen positives ) nodule and residual ovary in left pelvic side wall , one pulmonary embolism , two cases of deep - vein thrombosis , four cases of wound dehiscence , one wound haematoma , two hernias , one signi cant ileus , one bowel obstruction , one bowel stula , and two cases of signi cant infection . ovarian or tubal malignancies were detected in 87 women : 42 in the mms group and 45 in the uss group ( table 3 )  . 
there was no signi cant di erence ( fishers exact test p = 0229 ) in the number of stage iii borderline cancers in the mms ( two of eight ) compared with the uss group ( one of 20 )  . 
 in the mms group , 33 ( 786% ) of the 42 women with ovarian or tubal malignancies had ovarian cancer detected as a result of an elevated risk of ovarian cancer on the level 1 screen ( rst blood test )  . 
in the uss group , all 45 ( 100% ) women had ovarian cancer detected as a result of an abnormal scan on the level 1 screen ( rst scan )  . 
the median time to surgery from level 1 scan in these women was similar to that for women in the mms group : 815 days ( iqr 6031125 )  . 
 however , nine ( 214% ) of the women in the mms group with ovarian or tubal malignancies had ovarian cancer detected after an intermediate risk of ovarian cancer at the level 1 screen that led to repeat tests . 
the median time to surgery from the level 1 screen in these women was 2739 days ( iqr 22003310 ) , since the protocol for managing intermediate risk was to repeat ca125 tests 334 vol 10 april 2009 articles over a period of 810 months ( gure 2 )  . 
one woman initially had a normal level 2 scan , and one woman had two normal level 2 scans but was operated on based on a severe risk of ovarian cancer classi cation . 
they include one woman in the mms group and two from the uss group who withdrew from the trial after their level 1 screen and had an ovarian cancer diagnosed more than 1 year later . 
at an incident screen 22 months later , an increase in size of the mass on ultrasound prompted bilateral salpingo - oophorectomy , and she was diagnosed with stage ic papillary serous cystadenocarcinoma . 
as information on cancers can take up to 3 years to be recorded by the national cancer registries , we explored in detail the other sources of follow - up data in the 12 658 women for whom time from censorship ( 1 year from the date of the last scan or ca125 test on the prevalence screen ) to cancer registry follow up on june 13 , 2008 , was less then 3 years . 
in this cohort , after the censorship date , we had additional con rmation of ovarian cancer status in 11 336 women , as they had attended for further screening , and in an additional 17 women through returned follow - up questionnaires . 
 the source of veri cation of ovarian cancer status was limited to cancer registry follow up that was less than 3 years from the date of censorship in only 1275 women ( 13% of the entire cohort ; table 5 )  . 
this included one primary borderline and four invasive epithelial ovarian cancers in the mms group , and eight primary invasive epithelial ovarian cancers in the uss group ( table 3 )  . 
the ca125 concentrations at the prevalence screen ranged from 7 to 24 iu / l in the ve women with ovarian and tubal cancers in the mms group , and the cancers were diagnosed at 92 , 204 , 254 , 294 , and 329 days after the screen . 
all of the prevalence scans were normal in the uss group , and the cancers were diagnosed at 30 , 203 , 255 , 267 , 278 , 293 , 301 , and 341 days after the screen . for all primary ovarian and tubal cancers , the sensitivity , speci city , and positive - predictive values for mms and uss screening are shown in table 6 . 
there were 23 ( 42 of 97 ) operations per case of ovarian cancer in the mms and 188 ( 45 of 845 ) operations per case of early ( i / ii ) stage cancers ( % ) 471% 298% 649% 500% 291% 709% 483% 350% 618% 750% 194% 994% 00% 00% 410% 250% 55% 572% stage lower 95% ci upper 95% ci morphology serous endometrioid clear cell carcinosarcoma adenocarcinoma grade not graded screen positive screen negative overall overall * in two cases a diagnosis was made on the basis of ascitic uid cytology , omental biopsy , and imaging : primary surgery was not undertaken . table 4 : characteristics of primary invasive epithelial ovarian and tubal cancers ( icd - 10 c56 and c57.0 ) ons follow - up > 3 years from censorship date or when death certi cate was available number of women who have had an appointment after censorship date * number of women who have completed a follow - up questionnaire after censorship date * mms ( n = 50 078 ) uss ( n = 48 230 ) overall ( n = 98 308 ) 45 544 ( 909% ) 40 106 ( 832% ) 85 650 ( 871% ) 4071 ( 81% ) 7295 ( 182% ) 11 366 ( 116% ) 4 ( 001% ) 13 ( 003% ) 17 ( 002% ) remaining * 459 ( 09% ) 816 ( 17% ) 1275 ( 13% ) * in women with ons follow - up < 3 years from censorship date . 
censorship date is 1 year from the date of the last scan or ca125 in the prevalence screen . table 5 : details of follow - up of women who underwent screening the in speci city between ovarian cancer in the uss group . 
 when the analysis was restricted to primary invasive epithelial ovarian and tubal cancers , sensitivity was , compared with values when all cancers were included ( table 6 ) , much the same in the mms group , but lower in the uss group , although the di erence in sensitivity between mms and uss was still not statistically signi cant ( p = 0126 )  . 
 vol 10 april 2009 articles total number of women number of surgeries screen positives screen negatives sensitivity 95% ci speci city 95% ci 95% ci positive - predictive value screen positives screen negatives sensitivity 95% ci speci city 95% ci 95% ci positive - predictive value primary ovarian and tubal malignancies ( icd - 10 c56 and c57.0 ) within 1 year of prevalence screen number of operations per screen positive 188 108 primary invasive epithelial ovarian and tubal malignancies within 1 year of prevalence screen overall p value * 48 230 98 308 50 078 894% 849% 870% 0564 769965 724933 788929 998% 982% 990% < 00001 998998 981984 990991 433% 333538 53% 3971 92% 75113 895% 750% 829% 0126 752971 566885 720908 998% 982% 990% < 00001 998998 981984 990991 351% 256454 28% 1842 62% 4779 162 number of operations per screen positive 352 * fishers exact test . 
 borderline epithelial ovarian cancers and ovarian neoplasms of uncertain behaviour treated as false positives . table 6 : performance characteristics for detection of malignant ovarian and tubal neoplasms ( icd - 10 c56 and c57.0 ) in the prevalence screen speci city was higher in the mms than in the uss group , resulting in fewer repeat tests and almost nine times fewer operations per cancer detected . 
the main strengths of the study are recruitment by random invitation using the health - authority registers of 27 primary care trusts , the multicentre design involving recruitment and screening through 13 nhs trusts , the scale of the trial , high compliance with screening , randomisation to two well - de ned screening strategies , and an independent review of surgical outcomes and detailed follow - up of the entire cohort . 
although primary peritoneal cancers are treated similarly to advanced primary ovarian carcinomas , neither the mms nor the uss screening strategies were developed to detect thehowever , data on these cancers would be interesting , so primary peritoneal cancers are listed separately in table 3 . 
however , we have ( low malignant potential ) ovarian neoplasms , since they share the same icd - 10 code ( c56 ) as primary invasive epithelial ovarian cancers . 
 included primary borderline problem 84 primary ovarian ( icd - 10 c56 ) and three tubal cancers ( icd - 10 c57.0 ) were detected on screening , with a further 13 primary ovarian cancers diagnosed clinically in the ensuing year . 
19% ( eight of 42 ) of the primary ovarian cancers detected were borderline in the mms group , compared with 15% reported in clinical series.24 however , 44% ( 20 of 45 ) of the primary ovarian cancers detected in the uss group were borderline . 
this highlights an issue that has already become a signi cant cancer - screening strategiesthe detection of cancers that may never have been diagnosed in an individuals lifetime had they not been screened . 
in cancer screening , estimates of overdetection range from 3 to 50% of cases in breast cancer screening26 and 22 to 34% in prostate cancer screening.27 a similar rate of 25% overdetection has been reported with chest radiography for lung cancer , with the use of ct expected to result in higher rates.28 in ovarian cancer , such false positives may include ovarian neoplasms of uncertain behaviour ( icd - 10 d39.1 ) and borderline disease . 
once borderline cancers are detected during screening , it is di cult not to operate given that borderline and stage i invasive other 336 vol 10 april 2009 articles results indicate inherent strategies . 
the ovarian cancers share common morphological features on ultrasound imaging.29 the novel design of ukctocs , which randomly assigns women to two very di erent screening strategies , provides some insight into the in the di erent extent of overdiagnosis that screening pseudodisease will be less apparent with a serum ca125based ovarian cancer screening strategy than with uss screening . 
this accords with results from the prevalence screen of the prostate lung colon ovarian cancer ( plco ) screening trial , in which only one of nine borderline ovarian neoplasms were detected by ca125 screening , whereas all nine were detected by ultrasound.23 there is a possibility that some of these borderline tumours may progress to invasive cancers if undetected , although there is little evidence to support this . 
 di erences between the screening groups on later follow - up should help to elucidate the issue , and allow de nite estimates of overdiagnosis to be calculated . given the issues surrounding borderline disease , a separate analysis was done excluding borderline lesions , e ectively treating such lesions as false positives . 
this resulted in a fall in the sensitivity of the uss screen from about 85% to 75% , with an attendant increase in the ratio of operations per true positive from 19 : 1 to 35 : 1 . 
the detection rates in the mms group remained at around 89% , with a small increase in the ratio of operations per true positive from 23 : 1 to 29 : 1 . 
however , the clinical e ect of this di erence will depend on the mortality e ect on follow up , and on issues such as patient satisfaction and acceptability . various factors may contribute to the detection of more primary invasive epithelial cancers in the mms group than in the uss group . 
it is possible that a transvaginal ultrasound scan done at the time of the level 1 screen , 75 months earlier than when the transvaginal ultrasound scan was actually done in these women , would not have detected an abnormality . 
 although an unsatisfactory scan in the uss group does lead to a repeat level 1 scan in 3 months , the follow - up is not equivalent to that of an intermediate risk of ovarian cancer , as women are returned to annual screening after two unsatisfactory scans but have continued follow - up with ca125 after two intermediate risk of ovarian cancer results . 
ultrasound , unlike ca125 , has a subjective element , and it is possible that the heightened awareness of a sonographer in view of rising ca125 concentrations contributed to a positive diagnosis . 
however , it is noteworthy that two of the nine women in the mms group who were diagnosed after initially being classi ed as intermediate risk had normal scans initially . 
by contrast , ultrasound has a subjective element , and accuracy is correlated with the experience of the sonographer.30 , 31 there are no described qualityassurance measures for scanning postmenopausal ovaries in asymptomatic women . 
more than 100 sonographers were required to deliver the scan load of 55 000 scans per year ; these individuals were fully certi ed sta working in ultrasound departments in the uk nhs . 
until then , it should be noted that the number of interval cancers and sensitivity in the uss group is in keeping with other large single - centre and multicentre series ( table 7 ) for which systematic follow - up and tracing of interval cancers has been undertaken . 
a previous ultrasound and autopsy study that 154% of 234 post menopausal women who had died from nongynaecological diseases had ovarian cysts.32 here , 1894 ( 39% ) of women were found to have abnormal scans . 
 clinical assessment in the uss group , which included the use of morphological features detected during ultrasound , serum ca125 , and other imaging modalities , decreased surgical rates to 446% ( 845 of 1894 ) of those found to have abnormalities compared with 581% ( 97 of 167 ) of those with abnormalities in the mms group ( table 2 )  . 
the lack of follow - up data on the outcome of pelvic masses with benign ultrasound morphology33 means that a proportion of women and clinicians will opt for surgery once a complex adnexal lesion is detected , even if it is more likely to be benign . 
this is exempli ed in this series , in which a lesion detected on ultrasound was not removed on laparoscopy because it was thought to be an ovarian broma ( table 2 )  . 
the higher proportion of laparoscopic procedures in the uss group than in the mms group ( 624% vs 286% ) re ects the lower suspicion of malignancy among clinicians for certain ultrasounddetected lesions . 
however , such decisions are not straightforward , as the risk of malignancy associated with lesions such as multilocular cysts in clinical series is 18% , rising to 49% if a solid component is also present.29 during further rounds of screening there is likely to be a substantial fall in the number of women undergoing surgery for benign lesions in the uss group , as most will have been removed or detected and managed conservatively during the prevalence screen . 
it is therefore important to wait for the results of incidence screening before drawing de nite conclusions about the positive - predictive value and speci city characteristics of the two screening strategies . 
in the ultrasound screening trial by van nagell and colleagues , 9 the number of operations per case of invasive epithelial ovarian cancer detected was 93 : 1 ( table 7 ) after a mean of 48 annual screens . 
29% of women undergoing surgery which resulted in benign pathology or normal ovaries being detected , experienced a major complication involving injury to a hollow viscus or signi cant haemorrhage . 
 there was no di erence in the complication rates in the two screening groups . the proportion of primary invasive ovarian and fallopian tube cancers diagnosed with stage i / ii disease ( 48% ) was encouraging compared with the 26% rate in the clinical series34 and 22% in the prevalence screen of the plco screening trial in the usa ( table 7 ) .23 the highest reported proportion of early - stage cancers detected on screening is from the university of kentucky screening programme , 9 where 82% of primary invasive epithelial ovarian cancers detected were stage i / ii . 
the overall number of ovarian cancers reported in the university of kentucky study was also lower ( table 7 ) .9 the e ect of this apparent stage shift on mortality will not be known until su cient events have accrued for a comparison with mortality in the control group , when the trial is completed in december , 2014 . 
 the di erences in the uptake of the initial screen between women randomly assigned to the mms group and uss group ( gure 1 ) must be interpreted with care . 
 it is important not to interpret this as indicating that women preferred a blood test to a scan , as a signi cant proportion of this di erence re ects trial design . 
analysis of the psychosocial data and compliance with annual screening will provide better measures of womens preferences . a limitation of trial design could be that the criteria used to classify scans did not incorporate one of the many weighted morphological indices that have been 338 vol 10 april 2009 articles proposed to improve discrimination between benign and malignant masses.29 , 35 however , it is important to note that most of these indices were derived from clinical series in symptomatic patients , in whom advanced cancers are the nordata on morphological characteristics of early ovarian cancers in asymptomatic long - term follow - up of patients and outcome on ultrasound - detected limited . 
simple lesions are unilocular cysts are an exception , for which long - term follow - up of women has shown that they are invariably benign.36 this was incorporated into the ukctocs trial design , with simple cysts less than 60 cm in size classi ed as normal and the women returned to annual screening with no further review . 
all clinicians were provided with pictorial depictions of complex morphology , initially using the kentucky format19 until the adoption in 2003 of the iota format , 13 and all clinicians were aware of the risk of malignancy associated with the features in the clinical series . 
 serum ca125 and transvaginal ultrasound remain at the core of all new screening and diagnostic strategies being proposed for ovarian cancer , and although many new markers have been discovered since 1999 , none have so far been validated in a prospective screening trial . 
the trial serum bank , which currently has over 350 000 samples , will make the retrospective testing of new markers possible . a nal limitation of this report is that no data are available on cancers in the control group . 
however , in line with other ovarian cancer screening randomised controlled trials , 23 it was felt by the overseeing committees that the release of such information when screening is ongoing would compromise the overall outcome of the trial . 
although this maximises external validity by excluding biases related to advertisement and self - referral , the cohort is still likely to be healthier than the general uk population because of the characteristics of the women who chose to respond . 
the multicentre design , nhs hospital setting , use of standard tests ( ca125 and transvaginal ultrasound ) done by sta those who would deliver a national similar programme , and the management of women with abnormalities in nhs clinics using national guidelines ensures that the ndings of the trial are applicable to the wider population . 
there are inherent di erences between the two strategies being tested , with a more subjective element inherent in the ultrasound - based strategy than with the ca125 test , for which it is easy to implement stringent quality control . 
mms has signi cantly better speci city than does uss , resulting in fewer repeat tests and less surgery ; sensitivity for the detection of primary epithelial cancers of the ovaries and fallopian tubes seems better with mms than with uss , although is not statistically signi cant . 
the results of ongoing screening are required before a conclusion can be drawn regarding the e ect of screening on mortality . the di erence contributors ij , um , mp , sjs , sc , lf , and am were involved in study design . 
none of the other authors declared any con icts of interest . acknowledgments we are particularly grateful to the women throughout the uk who are participating in the trial , to the entire medical , nursing , and administrative sta who work on the ukctocs and to the independent members of the numerous oversight committees . 
the trial was core funded by the medical research council , cancer research uk , and the department of health , with additional support from the eve appeal , special trustees of barts and the london , and special trustees of university college london hospital ( uclh )  . 
a large portion of this work was done at uclh / ucl within the womens health theme of the national institute for health research uclh / ucl comprehensive biomedical research centre supported by the department of health . 
concurrent hormone and radiation therapy in patients with breast cancer : what is the rationale ? lancet oncol 2009 ; 10 : 5360 . toledano a , azria d , garaud p , et al . 
in table 1 , a ten - fold discrepancy in tumour size was caused by a conversion error of the cyst size from cm to mfurthermore , the patients with squamous - cell carcinoma in situ should have been excluded ( peuchmaur et al , 1989 ; tobon et al , 1991 ; dadhwal et al , 2002 ) : these publications provided only limited data and exclusion does not change results signi cantly . 
data are mean ( sd , range ) or number ( % )  . table 1 : preoperative data for patients with mature cystic teratoma 446 vol 10 may 2009 articles lancet oncol 2010 ; 11 : 6674 published online october 28 , 2009 doi : 10.1016 / s14702045 ( 09 ) 70306 - 7 * see webappendix for investigators department of clinical oncology , university college hospital , london , uk ( prof j tobias frcp ) ; cancer research uk sussex psychosocial oncology group , brighton and sussex medical school , brighton , uk ( k monson msc ) ; department of clinical oncology , the christie hospital , manchester , uk ( n gupta frcr ) ; faculty of medicine , bute medical school , university of st andrews , st andrews , uk ( prof h macdougall frcr ) ; department of oncology , queen elizabeth hospital birmingham , birmingham , uk ( prof j glaholm frcr ) ; department of oral and maxillofacial surgery , st bartholomews hospital , london , uk ( prof i hutchison frcs ) ; and cancer research uk and ucl cancer trials centre , university college london , london , uk ( a hackshaw msc , l kadalayil phd ) correspondence to : mr allan hackshaw , cancer research uk and ucl cancer trials centre , university college london , 90 tottenham court road , london w1t 4tj , uk ah@ctc.ucl.ac.uk chemoradiotherapy for locally advanced head and neck cancer : 10 - year follow - up of the uk head and neck ( ukhan1 ) trial je rey s tobias , kathryn monson , nirmal gupta , hugh macdougall , john glaholm , iain hutchison , latha kadalayil , allan hackshaw , on behalf of the uk head and neck cancer trialists group * summary background between 1990 and 2000 , we examined the e ect of timing of non - platinum chemotherapy when combined with radiotherapy . 
 methods between jan 15 , 1990 , and june 20 , 2000 , 966 patients were recruited from 34 centres in the uk and two centres from malta and turkey . 
patients with locally advanced head and neck cancer , and who had not previously undergone surgery , were randomly assigned to one of four groups in a 3 : 2 : 2 : 2 ratio , strati ed by centre and chemotherapy regimen : radical radiotherapy alone ( n = 233 ) ; radiotherapy with two courses of chemotherapy given simultaneously on days 1 and 14 of radiotherapy ( sim alone ; n = 166 ) ; or 14 and 28 days after completing radiotherapy ( sub alone , n = 160 ) ; or both ( sim + sub ; n = 154 )  . 
patients who had previously undergone radical surgery to remove their tumour were only randomised to radiotherapy alone ( n = 135 ) or sim alone ( n = 118 ) , in a 3 : 2 ratio . 
the primary endpoints were overall survival ( from randomisation ) , and event - free survival ( efs ; recurrence , new tumour , or death ; whichever occurred rst ) among patients who were disease - free 6 months after randomisation . 
among patients who did not undergo surgery , the median overall survival was 26 years ( 99% ci 1942 ) in the radiotherapy alone group , 47 ( 2678 ) years in the sim alone group , 23 ( 1635 ) years in the sub alone group , and 27 ( 1647 ) years in the sim + sub group ( p = 010 )  . 
for every 100 patients given sim alone , there are 11 fewer efs events ( 99% ci 121 ) , compared with 100 given radiotherapy , 10 years after treatment . 
among the patients who had previously undergone surgery , median overall survival was 50 ( 99% ci 1880 ) and 46 ( 2276 ) years in the radiotherapy alone and sim alone groups ( p = 070 ) , respectively , with corresponding median efs of 37 ( 99% ci 1159 ) and 30 ( 1256 ) years ( p = 085 ) , respectively . 
the percentage of patients who had a signi cant toxicity during treatment were : 11% ( radiotherapy alone , n = 25 ) , 28% ( sim alone , n = 47 ) , 12% ( sub alone , n = 19 ) , and 36% ( sim + sub , n = 55 ) among patients without previous surgery ; and 9% ( radiotherapy alone , n = 12 ) and 20% ( sim alone , n = 24 ) among those who had undergone previous surgery . 
the percentage of patients who had a signi cant toxicity at least 6 months after randomisation were : 6% ( radiotherapy alone , n = 13 ) , 6% ( sim alone , n = 10 ) , 4% ( sub alone , n = 7 ) , and 6% ( sim + sub , n = 9 ) among patients who had no previous surgery ; and 7% ( radiotherapy alone , n = 10 ) and 11% ( sim alone , n = 13 ) among those who had undergone previous surgery . 
the most common toxicity 6 months after treatment was xerostomia , but this occurred in 3% or less of patients in each group . interpretation concurrent non - platinum chemoradiotherapy reduces recurrences , new tumours , and deaths in patients who have not undergone previous surgery , even 10 years after starting treatment . 
patients who have undergone previous surgery for head and neck cancer do not bene t from non - platinum chemotherapy . funding cancer research uk , with support from university college london and university college london hospital comprehensive biomedical research centre . introduction head and neck cancers are relatively common ( about 7500 new cases in the uk and 45 000 in the us each year ) , and are increasing in incidence in some countries such as the uk , mainly because of smoking and excessive alcohol intake.13 standard treatment until 1990 was surgical resection or radical radiotherapy , sometimes both . 
toxicity is especially important since vol 11 january 2010 articles patients are typically un t , often with coexistent illness.4 , 5 over the past decade the role of chemotherapy has become clearer . 
the number of agents found to be active in squamous - cell carcinoma has increased , and the best ways of combining them continue to be investigated . the uk head and neck ( ukhan ) cancer group was established in 1990 to investigate the e ectiveness of chemotherapy used in conjunction with radiotherapy and surgery . 
at the time , it was believed that chemotherapy given at time as radical radiotherapy ( ie , concurrent ) and afterwards ( ie , maintenance ) could be e ective . 
other objectives were to assess the e ect of timing and duration of chemotherapyie , whether two courses should be given simultaneously with ( sim alone ) or subsequent to ( sub alone ) the radiotherapy course , or both simultaneously and following radiotherapy ( four courses , sim + sub )  . 
 the same methods patients patients with locally advanced squamous - cell carcinoma of the head and neck were included in a factorial randomised trial if they were judged to be suitable for initial treatment or radical radiotherapy as either following an operation ( generally patients at high risk of recurrence following surgery due to margin status or advanced stage of disease at presentation )  . 
patients were eligible if they satis ed the following criteria : age 18 years or over ; considered t enough to receive any of the trial treatments ; had histological con rmation of squamous - cell carcinoma , with t2 to t4 primary lesions ( including node - negative cases ) or were node positive ; had full normal blood count , and creatinine and urea levels within normal ranges ; showed no evidence of distant metastases ; and had no previous treatment for the cancer other than surgical excision . 
 all patients gave written informed consent . procedures the extent of previous surgery , radiotherapy regimen , and nutritional support with either nasogastric or percutaneous - endoscopic radiologically inserted gastrostomy feeding , were based on local policies to maximise recruitment . 
 surgery before randomisation was also determined by local practice , and could involve resection of the primary tumour alone with or without comprehensive neck - node resection , provided that the intention was to completely 713 patients had no surgery 253 patients had surgery 233 patients allocated to radiotherapy alone 166 patients allocated to 160 patients allocated to 154 patients allocated to sim alone sub alone sim + sub 135 patients allocated to radiotherapy alone 118 patients allocated to sim alone 5 patients ineligible 1 early stage disease 2 ineligible history 1 previous treatment 1 other 7 patients ineligible 1 early stage disease 3 ineligible history 1 previous treatment 2 other 1 patients ineligible 1 early stage disease 5 patients ineligible 1 early stage disease 2 previous treatment 2 other 9 patients ineligible 1 early - stage disease 2 occult primary 1 ineligible history 3 previous treatment 2 other 14 non - compliers to chemotherapy * 50 non - compliers to chemotherapy * 68 non - compliers to chemotherapy * 32 non - compliers to chemotherapy * 233 patients analysed 166 patients analysed 160 patients analysed 154 patients analysed 135 patients analysed 118 patients analysed 178 events for overall survival 115 events for overall survival 128 events for overall survival 122 events for overall survival 95 events for overall survival 79 events for overall survival 197 events for efs 125 events for efs 141 events for efs 132 events for efs 103 events for efs 89 events for efs figure 1 : trial pro le efs = event - free survival . 
only 26 patients did not fully meet the eligibility criteria , but they were included in the analysis . vol 11 january 2010 articles see online for webappendix age ( years ; median and range ) male female tumour stage unknown nodal status negative positive unknown stage stage ii stage iii stage iv unknown site of primary larynx oral cavity oropharynx nasopharynx hypopharynx other unknown surgery group margins cleared * neck dissection done 188 ( 81 ) 45 ( 19 ) 19 ( 8 ) 106 ( 46 ) 52 ( 22 ) 56 ( 24 ) 129 ( 55 ) 104 ( 45 ) 64 ( 27 ) 71 ( 30 ) 97 ( 42 ) 1 ( < 1 ) 73 ( 31 ) 41 ( 18 ) 78 ( 34 ) 14 ( 6 ) 22 ( 9 ) 5 ( 2 ) clear the tumour . 
usually at the outset these surgery patients were scheduled for adjunctive postoperative radiotherapy because of their advanced disease . although radical radiotherapy could be given according to local practice , it had to be approved by the trial steering committee , and investigators were asked to adhere to it for all patients within that centre , regardless of treatment allocation . 
the south - east co - operative oncology group regimen involved irradiation with planned elds to adequately cover the primary tumour in unresected cases , and in most cases lymph - node drainage area . 
another common regimen , used in birmingham , edinburgh , and some other centres , had the following schedule : 55 gy given in 20 fractions ( 275 gy per fraction ) over 4 weeks to the primary tumour and rst station lymphatic drainage , and 4125 gy in 15 fractions to the elective neck . 
50 gy given in 20 fractions ( 25 gy per fraction ) was given postoperatively . chemotherapy regimens were either methotrexate alone or vincristine , bleomycin , methotrexate , and uorouracil ( vbmf ) ; webappendix.8 , 9 sim started on days 1 and 14 concurrently with radiotherapy , and sub started 14 and 28 days after completing radiotherapy . 
 methotrexate was given intravenously in two doses of 100 mg / m : the rst dose was given 24 h before radiotherapy and the second dose was given on day 14 of radiotherapy . 
folinic acid rescue was given if serum methotrexate concentration at 24 h after treatment exceeded 04 mol / l.10 vbmf consisted of vincristine 14 mg / m ( maximum 2 mg ) , bleomycin 30 mg , uorouracil 500 mg , and methotrexate 100 mg / drugs were given intravenously by slow bolus injection except bleomycin , which was given by intramuscular injection . 
 other endpoints were control of local and regional disease ( ie , the complete remission rate ) at 6 months ; time to recurrence ; death from head and neck cancer ; and toxicity during and after treatment , which was classi ed as signi cant if hospitalisation was required during chemoradiation , therapy was required to alleviate chronic treatment - related toxicity ( eg , dilatations for oesophageal strictures ) , or clinicians recorded an event as severe after treatment . 
although toxicity was not recorded on a standardised scale during the trial , we compared the reported adverse - event grading and descriptions with the common terminology criteria for adverse events ( ctcae ) version 3 , as part of the statistical analysis . 
 * primary site resection margins were clear . table 1 : distribution of baseline characteristics according to trial group vol 11 january 2010 articles a non - complier was de ned as a patient who did not receive the full dose according to the trial protocol . 
in october , 2008 , an active data chase was completed to ascertain which patients had died or had a recurrence or new tumour , and the date patients were last seen alive . lists centrally at randomisation and masking block strati ed randomisation was used , and allocations were concealed from investigators and patients by generating random number the coordinating centre ( cancer research uk and university college london cancer trials centre )  . 
patients were to be allocated to radiotherapy alone , sim alone , sub alone or sim + sub if they had not had previous surgery , using a block size of nine ( allocation ratio 3 : 2 : 2 : 2 , which is 1 : 2 in favour of chemotherapy , to increase the total number of patients given chemotherapy ) ; or only to radiotherapy alone or sim alone if they had previously undergone surgery , using a block size of ve ( allocation ratio 3 : 2 )  . 
 randomisation strati cation factors were centre ( which automatically strati es for radiotherapy regimen and all other for patient management ) and chemotherapy regimen ( though all but two centres used a single regimen during the trial )  . 
hospital clinicians recruited patients , and centres telephoned the co - ordinating centre , who assigned each patient a treatment allocation after recording the eligibility and strati cation factors . local policies statistical analysis the sample size of about 1000 patients was based on detecting an increase in 5 - year survival from 25% in the radiotherapy - alone group to 35% in the chemotherapy groups combined , with 90% power and two - sided 5% level of statistical signi cance . 
all p values are two - sided , and 99% ci were used to allow for having multiple comparisons ( 95% for the primary objective of any chemotherapy versus radiotherapy alone )  . 
expressed as a percentage of the number disease free at 6 months . table 3 : the number and causes of death , and the number of rst events in patients who were disease free at 6 months after randomisation ( used to examine event - free survival ) , according to trial group 3 ( 3 ) 2 ( 2 ) 3 ( 3 ) 2 ( 2 ) 1 ( < 1 ) 10 ( 8 ) 4 ( 3 ) 1 ( < 1 ) 1 ( < 1 ) 14 ( 12 ) 6 ( 5 ) 6 ( 5 ) 2 ( 2 ) 32 ( 27 ) 55 ( 47 ) 21 ( 18 ) 3 ( 25 ) 25 ( 27 ) 18 ( 20 ) 19 ( 21 ) vol 11 january 2010 articles radiotherapy alone sim alone sub alone sim + sub p = 010 number at risk radiotherapy alone sim alone sub alone sim + sub p = 070 number at risk radiotherapy alone sim alone time from randomisation ( years ) figure 2 : overall survival according to treatment groups for patients who had no surgery ( a ) and those who had undergone surgery ( b ) before randomisation sim = radiotherapy with two courses of chemotherapy given simultaneously on days 1 and 14 of radiotherapy . 
the median length of follow - up was 10 years after censoring those who had died ( maximum of 17 years ) , with 4397 person - years in total . 
the trial pro le is shown in gure 1 ; baseline characteristics are shown in table 1 . 7% of patients ( 69 / 966 ) were known to have not completed the planned radiotherapy course ( table 2 )  . 
27% of patients ( 164 / 598 ) allocated to receive chemotherapy did not complete their full course of treatment , mainly due to disease progression , acute toxicity , or withdrawal from treatment . 
among patients without prior surgery , only 8% ( 14 / 166 ) of the sim alone group were non - compliers to chemotherapy , compared with 31% ( 50 / 160 ) and 44% ( 68 / 154 ) in the sub alone and sim + sub groups respectively . 
27% ( 32 / 118 ) of sim alone patients who had surgery did not complete their chemotherapy . 69% ( 662 / 966 ) of patients were disease - free at 6 months ( webappendix )  . 
among those without previous surgery , the proportion disease - free at 6 months was highest in the sim alone group ( 73% , 122 / 166 ) compared with the other groups : radiotherapy alone ( 63% , 146 / 233 ) , sub alone ( 66% , 106 / 160 ) , and sim + sub ( 62% , 95 / 154 )  . 
 there was little di erence among patients who had undergone previous surgery : radiotherapy alone ( 76% , 102 / 135 ) and sim alone ( 77% , 91 / 118 )  . there were 717 deaths among all 966 patients , and 483 efs events among the 662 patients who were disease free at 6 months ( table 3 )  . 
estimated 5 - year overall survival was 43% ( 95% ci 3848 ) and efs was 32% ( 2737 ) in the radiotherapy - alone group ( patients with or without previous surgery )  . 
the chemotherapy or radiotherapy regimen used did not a ect the results ( webappendix )  . kaplanmeier curves for overall survival and efs are shown in gures 2 and 3 . 
in patients without previous surgery , median overall survival was 26 ( 99% ci 1942 ) years for those allocated to radiotherapy alone , 47 ( 2678 ) years for sim alone , 23 ( 1635 ) years for sub alone , and 27 ( 1647 ) years in those allocated to sim + sub ( log - rank p = 010 )  . 
 compared with radiotherapy alone , sim alone was associated with an improvement in efs ( hr 072 , 99% ci 053096 ; p = 0004 ) , although the e ect on overall survival was not signi cant ( 082 , 060111 ; p = 009 )  . 
 estimated 5 - year overall survival and efs in the sim - alone group were 50% ( 95% ci 3959 ) and 42% ( 3252 ; the corresponding rates in the radiotherapy alone group were 39% [ 3148 ] and 24% [ 1731 ] )  . 
 106 comparing four with two courses of chemotherapy ( ie , sim + sub vs either sim alone or sub alone ) did not show a survival advantage ( webappendix )  . 
adding sub to sim seemed to reduce the bene t of sim , producing a higher rate of death and events : compared with sim alone , overall survival ( hr 129 ; 99% ci 092181 ; p = 0049 ) and efs ( hr 127 , 092175 ; p = 006 )  . 
hr from an analysis of the main e ects associated with a 22 factorial trial ( ie , any sim vs no sim , and any sub vs no sub [ test for the interaction between sim and sub p = 012 ] , as well as sim alone vs sub alone , and survival hr vol 11 january 2010 articles radiotherapy alone sim alone sub alone sim + sub radiotherapy alone vs sim alone or sub alone ) , are shown in the webappendix . adding chemotherapy to radiotherapy was not e ective in patients who had undergone surgery previously . 
the median overall survival was 46 ( 99% ci 2276 ) and 50 ( 1880 ) years in those allocated to sim alone or radiotherapy alone , respectively ( hr 094 , 99% ci 064140 ; p = 070 )  . 
the median overall survival associated with sim alone was similar to the corresponding sim group without previous surgery ( 46 vs 47 years ) , but the median efs was higher ( 30 vs 22 years )  . estimated absolute risk di erences for overall survival , efs , and recurrence at 5 and 10 years after randomisation are shown in table 4 . 
compared with radiotherapy alone , for every 100 patients given sim alone , there could be 106 fewer patients who have a recurrence , new tumour , or die by 10 years after treatment ( 99% ci 11212 fewer ) ; equivalent to a number needed to treat of nine patients to avoid one event at 10 years . 
there could be 71 fewer deaths at 10 years ( 99% ci 184 fewer to 35 more ) among 100 patients treated with sim alone ( number needed to treat of 14 )  . 
no bene t was seen with sub alone or sim + sub , consistent with the other results . the percentages of patients who had a signi cant toxicity during treatment requiring hospitalisation in patients without previous surgery was 11% ( 25 / 233 ) in patients allocated to radiotherapy alone , 28% ( 47 / 166 ) in patients allocated to sim alone , 12% ( 19 / 160 ) in patients allocated to sub alone , and 36% ( 55 / 154 ) in patients allocated to sim + sub ( table 5 )  . 
although 28% of patients in the sim - alone group had an acute toxicity , compliance to chemotherapy was high ( 92% , 152 / 166 ; table 2 ) , probably because being in hospital would have provided them with the appropriate care to continue treatment . 
for patients who had undergone previous surgery , sim alone was associated with a doubling in the acute toxicity rate : 20% ( 24 / 118 ) sim alone versus 9% ( 12 / 135 ) radiotherapy alone . 
patients in the sim + sub group who during chemoradiation were less likely to complete their allocated chemotherapy regimen ( table 2 )  . experienced toxicity acute signi cant late toxicity occurring 6 months or more after randomisation was reported in 62 patients in total ; 44% ( n = 27 ) of rst noti cations occurring in months 6119 , and 24% ( n = 15 ) occurring in months 1224 . 
the rates were similar between the trial groups : 6% ( 13 / 233 ) among patients without surgery allocated to radiotherapy alone , 6% ( 10 / 166 ) for those allocated to sim alone , 4% ( 7 / 160 ) for those allocated to sub alone , and 6% ( 9 / 154 ) for those assigned to sim + sub ( table 5 ) ; and 7% p = 00005 number at risk radiotherapy alone sim alone sub alone sim + sub p = 085 number at risk radiotherapy alone sim alone time from randomisation ( years ) figure 3 : event - free survival ( efs ) according to treatment groups for patients who had no surgery ( a ) and those who had undergone surgery ( b ) before randomisation sim = radiotherapy with two courses of chemotherapy given simultaneously on days 1 and 14 of radiotherapy . 
 sub = radiotherapy with two courses of chemotherapy given 14 and 28 days after completing radiotherapy . treatment - related deaths , ( 10 / 135 ) and 11% ( 13 / 118 ) among patients who had undergone surgery allocated to radiotherapy alone or sim alone , respectively . there were 12 largely associated with dehydration , necrosis , mucositis , dysphagia , and renal failure . 
the rst six deaths were sent for independent review , after which clearer instructions were given to patients regarding adequate hydration and , in some centres , the avoidance of non - steroidal anti - in ammatory agents ( recognised to reduce glomerular ltration rate )  . 
negative risk di erences indicate that the event rate is lower than in the comparison group ( ie , more bene cial ) ; positive di erences indicate that the event rate is higher . 
 discussion the ukhan1 trial is one of the largest in head and neck cancer , and , to our knowledge , the only study to examine the timing of chemotherapy ( concurrent or maintenance ) in a factorial design . 
compared with radiotherapy alone , two courses of non - platinum chemotherapy given concurrently with radiotherapy ( sim alone ) in patients without previous surgery signi cantly extended efs by 12 years ( median efs 22 vs 10 years ; p = 0004 )  . 
the di erence in overall survival of 21 years ( median 47 vs 26 years , p = 009 ) was not statistically signi cant , probably because there were fewer overall survival events compared with efs in the analysis of sim alone versus radiotherapy alone ( 293 deaths vs 322 efs events ) and the e ect size was smaller ( hr of 082 vs 072 )  . 
the outcomes for sim alone were achieved with only one treatment - related death ( 06% ) , high compliance ( 92% ) , and acceptable toxicity rate ( 28% ) during treatment . 
among every 100 patients treated with sim alone , there were an estimated 106 fewer patients with a recurrence , new tumour , or death , 10 years later , compared with alone . 
concurrent chemoradiotherapy used in our study did not bene t patients who had undergone previous surgery , and the acute toxicity rate doubled . radiotherapy chemotherapy after radiotherapy was ine ective , which could be due in part to the higher proportion of patients who did not comply with treatment . 
reasons for non - compliance ( table 2 ) were largely because of toxicity , deaths , or withdrawals ( perhaps because some felt too unwell after radiotherapy to continue with therapy )  . 
 chemotherapy non - compliance was highest in the sim + sub group , and might also be due to patients not wanting to continue treatment after two courses of vol 11 january 2010 articles chemotherapy , possibly because they had completely responded after simultaneous chemoradiation , or were too unwell to continue . 
furthermore , this was a pragmatic trial , so we wanted centres to give their normal radiotherapy to encourage clinicians to participate , and therefore the doses used represented those given in routine practice at the time . 
all the radiotherapy regimens were radical doses , and there was no evidence that the radiotherapy regimen used a ected efs ( webappendix )  . there is variation in how patients with head and neck cancer are treated , with no established and agreed policy on chemoradiation , including for patients judged un t for platinum therapy . 
however , in the recent update , based on 9615 patients and including older data from ukhan1 , concomitant chemotherapy led to statistically signi cant reductions in deaths and recurrences , 7 with point estimates similar to those from ukhan1 : hr for overall survival 081 in mach - nc versus 082 ( 99% ci 060111 ) in ukhan1 , and hr for efs 079 in mach - nc versus 072 ( 99% ci 053096 ) in ukhan1 ( mach - nc used recurrence - free survival instead of efs )  . 
the review was based on adding chemotherapy to any loco - regional treatment ( ie , a mixture of surgery , no surgery , radiotherapy using standard or hyperfractionated regimens , or pre - operative radiotherapy )  . 
ukhan1 clearly separates patients according to whether they had surgery or not , showing that concurrent non - platinum chemotherapy used in the trial was more e ective than radiotherapy alone in the non - surgical group , but not in the group that had undergone previous surgery . 
 the mach - nc meta - analysis showed that concurrent chemoradiation should now be the routine treatment of choice for all patients with non - surgically treated advanced head and neck cancer . 
the ukhan1 study con rms this , but it also shows that a long - term bene t in terms of recurrence and deaths could be achieved with non - platinum agents that are inexpensive , relatively easy to deliver , and have lower toxicity than platinum therapies . 
 very few randomised head and neck cancer trials have reported such long - term e ects of chemo - radiotherapy , and we are not aware of any that have also investigated concurrent platinum treatment . 
 cisplatin used concurrently with radical radiotherapy has been shown to be better than radiotherapy alone : in an eortc trial ( 334 post - surgical patients with locally advanced disease ) , the risk of death was reduced by 30% ( p = 002 ) .12 efs was improved with cisplatin in a rtog trial ( 459 high - risk patients who had complete resection ) , with a decrease in risk ( hr 078 , 95% ci 061099 ; p = 004 ) .13 however , acute toxicity rates were much higher in those receiving chemotherapy ( 77% rtog and 41% eortc ) , compared with that in our own trial using vbmf or methotrexate ( 28% )  . 
although cisplatin - based regimens are often used in the us , the mach - nc meta - analysis did not nd a survival di erence according to type of chemotherapy ( p = 042 )  . 
in trials of poly - chemotherapy , the hr for death was 075 ( 95% ci 067084 ; using both uorouracil and platinum ) , 083 ( 074094 ; using either uorouracil or platinum ) , and 073 ( 052101 ; using chemotherapy other than uorouracil or platinum ) ; the ukhan1 estimate was 082 . newer agents such as taxanes and targeted therapies might improve on the longer - established doublet of cisplatin and uorouracil.1416 bonner and colleagues were the rst to show the value of cetuximab in advanced head and neck cancer , with a 30% reduction in the number of patients who progress or die ( in a trial of 424 patients ) .16 similar therapy combinations continue to be investigated . 
our 10 - year follow - up is reassuring for the regimens used in the ukhan1 study , and should encourage other trials to follow patients for many years . secondary hyperfractionated radiotherapy , involving an increase in the daily number of administered doses , is currently di cult for many uk oncology departments to deliver , so the simpler two courses of chemotherapy with only one fraction per day using standard regimens seems more feasible . 
as with improved outcomes at other sites such as the cervix , anus and lung , radical simultaneous chemoradiation therapy for scc of the head and neck is an e ective way of treating these life - threatening and disabling diseases . human papillomavirus ( hpv ) status was not obtained during the trial because it was not recognised as being a useful factor in head and neck cancer at the time the study was designed . 
however , data are beginning to emerge suggesting that patients with hpv - positive tumours have a better prognosis.17 although most evidence comes from observational studies , the e ects have been seen in retrospective analyses of randomised vol 11 january 2010 articles trials.18 , 19 we plan to examine hpv status and its possible e ect on outcome in the ukhan1 trial in the future . in summary , ukhan1 showed that patients with head and neck cancer who had undergone previous surgery did not bene t from the addition of chemotherapy to adjunctive post - operative radiotherapy . 
however , there was a clear bene t on recurrences and deaths associated with two courses of simultaneous non - platinum chemoradiotherapy in patients who had not undergone previous surgery , and this bene t persisted after a long follow up . 
non - platinum - based chemotherapy could be considered an alternative to platinum - based regimens , as well as an e ective therapy for patients who are judged to be un t for cisplatwith this particular group of patients , characteristically with multiple comorbidity and relatively low compliance to chemo therapy , the inability to tolerate platinum - based regimens is often a serious barrier to radical chemoradiation . 
moreover , the avoidance of local recurrence , with its potentially devastating consequences for the patients quality of life , is of particular importance in this group , many of whom su er from social deprivation and poor domestic support . 
improving efs reduces the number of patients who later need radical salvage surgery , which can be associated with long - term or permanent dis gurement , impaired function ( eg , ability to speak or eat easily ) , or social exclusion.20 because this is a high risk and generally un t patient group , many of whom are excessive users of alcohol and tobacco throughout treatment , the availability of a relatively simple , inexpensive and low toxicity chemoradiation regimen considerably improves the likelihood of completing treatment , essential for improving the chance of cure . contributors jt , km , ng , hmd , jg , and ih , designed and conducted the trial . 
 all authors were involved in writing the paper . con icts of interest the authors declared no con icts of interest . acknowledgments this comment was funded by cancer research uk , with support from university college london and university college london hospital comprehensive biomedical research centre . 
we are most grateful to all the patients and clinical teams at the hospitals in the uk and abroad , without whom this trial would not have been possible . re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology chosen as one of the endpoints.2 patients recruited in this trial were offered radiofrequency ablation , because they were considered by the treating physician to be unsuitable for surgery and unfit for radiotherapy or chemotherapy as a result of either underlying chronic obstructive pulmonary disease or major associated comorbidities . 
because the patients had small , asymptomatic pulmonary tumours , no improvement in quality of life was noted after treatment with radiofrequency ablation , despite the high number of complete responses . 
nevertheless , we think that the absence of any significant worsening in short form ( sf ) - 12 ( physical and mental summary ) scores and functional assessment of cancer therapylung ( fact - l ; lung - cancer scale and trial outcome index ) scores provides evidence that the minimallyinvasive treatment approach used in these patients did preserve their quality of life . 
the number at risk for part b of gures 3 and 4 of this article should have been interventional group ( top ) and control group ( bottom )  . 
also , the second sentence in the discussion should have read , however , preoperative chemoradiotherapy in patients undergoing surgery signi cantly increased the proportion of those with complete resection ; and in those with complete resection , preoperative chemoradiotherapy increased the proportion of patients with mediastinal downstaging and histopathological response . bo etta p , hecht s , gray n , gupta p , straif k . 
during the immediate months preceding submission of the review sh was acting in the capacity of an expert witness for the plainti in a future court case against a smokeless tobacco company . 
sh declares his participation in this case in no way in uenced his writing or involvement in the review . bonnefoi h , potti a , delorenzi m , et al . 
in the webpanel of this article , the headings for docetaxel should have been resistant cell lines ( rst ) and sensitive cell lines ( second )  . 822 vol 9 september 2008 re ection and reaction is supportive never - smokers , and women.7 there evidence that patients with egfr - mutant tumours are biologically more indolent ( lim wt , national cancer centre , singapore , personal communication )  . i propose re ning the bipartite model by adding a clinical and biological dimension to it . 
the group of patients with slow - growing tumours are clinically characterised by never - smokers or former smokers who have had little active exposure , are women , and have egfr - activating mutations . 
to improve lung - cancer outcome , we have to adopt a two - pronged approach : identify the population at risk of slow - growing tumours and target them for screening trials , while using coordinated antitobacco e orts to prevent aggressive tumours in others . 
j natl cancer inst 2005 ; 97 : 33946 . if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology errata jones lw , eves nd , haykowsky m , joy aa , douglas ps . 
the correct gure is shown . number at risk months vol 9 october 2008 news upcoming meetings sept 29oct 6 , 2009 lifestyle factors oct 2027 , 2009 chemical agents and related occupations special report : policy a review of human carcinogenspart d : radiation in june 2009 , 20 scientists from nine international countries met at the agency for research on cancer ( iarc ) to reassess the carcinogenicity of the types of radiation previously classi ed as carcinogenic to humans ( group 1 ) and to identify additional tumour sites and mechanisms of carcinogenesis ( table and panel )  . 
these assessments will be published as part d of volume 100 of the iarc monographs.1 less alpha particles , consisting of two protons and two neutrons , are a densely ionising type of radiation with low capacity to penetrate living tissue ( less than 01 mm )  . 
 carcinogenicity of emit after the chernobyl accident , a sharp increase in the risk of thyroid cancer was found with exposure to radioiodines , particularly iodine - 131 , during childhood and adolescence.2 , 3 this increased risk might be due to higher milk intake per unit of body weight among children ; a higher thyroid dose per unit of iodine - 131 intake from milk ; a higher susceptibility per unit of thyroid dose ; or a combination of these . 
combined analyses of casecontrol studies now estimate that residential exposure to radon gas is the leading cause of lung cancer after tobacco smoke ( 815% attributable risk in europe and north america ) .4 , 5 gamma - rays and ionising are x - rays sparsely electromagnetic radiation that penetrate living tissue , typically producing fast electrons that deposit energy , resulting in tissue damage . 
extensive study of atomicbomb increased cancer risks at multiple anatomical sites.6 current evidence adds to the list of tumours caused by x - rays survivors shows and gamma - rays ( table ) , and also in - utero exposure establishes that increases the risk of cancer at multiple sites.7 , 8 the working group rea rmed the carcinogenicity of x - radiation and gamma - radiation ( group 1 )  . and traversed neutrons are produced by nuclear reactions and are a main component of cosmic radiation . 
however , the evidence of cancer in experimental animals is su cient , and mechanistic data show that neutrons transfer their energy in clusters of ionising events resulting in similar , but more severe , local damage than that induced by x - rays or gamma - rays . 
 each type of ionising radiation ( panel ) the transfers energy form of highly structured tracks of radiation type major study populations tumour sites ( and types ) on which su cient evidence is based alpha - particle and beta - particle emitters radon - 222 and decay products general population ( residential exposure ) , underground miners radium - 224 and decay products medical patients radium - 226 , radium - 228 , and decay products radium - dial painters thorium - 232 and decay products medical patients plutonium phosphorus - 32 plutonium - production workers medical patients fission products , including strontium - 90 general population , following nuclear reactor accident solid cancers , leukaemia radioiodines , including iodine - 131 children and adolescents , following nuclear reactor accident thyroid x - radiation or gamma - radiation atomic - bomb survivors , medical patients ; in - utero exposure ( o spring of pregnant medical patients and of atomic - bomb survivors ) lung bone lung , liver , bone acute leukaemia bone , paranasal sinus and mastoid process ( radium - 226 only ) liver , extrahepatic bile ducts , gall bladder , leukaemia ( excluding cll ) salivary gland , oesophagus , stomach , colon , lung , bone , skin ( bcc ) , female breast , urinary bladder , brain and cns , leukaemia ( excluding cll ) , thyroid , kidney ( atomic - bomb survivors , medical patients ) ; multiple sites ( in - utero exposure ) skin ( bcc , scc , melanoma ) skin ( melanoma ) , eye ( melanoma , particularly choroid and ciliary body ) solar radiation uv - emitting tanning devices general population general population cll = chronic lymphocytic leukaemia . 
scc = squamous - cell carcinoma . table : radiation exposures with su cient evidence in humans vol 10 august 2009 news monograph working group members b armstrongco - chair ( australia ) , e cardisco - chair ( spain ) ; a green ( australia ) ; d krewski , r mitchel , n priest ( canada ) ; l tomaek ( czech republic ) ; k baverstock ( finland ) ; j - f dor , j hall , l sabatier ( france ) ; m sokolnikov ( russian federation ) ; m hill , m little , m marshall , c muirhead , a riddell ( uk ) ; d brenner [ unable to attend ] , r guilmette , d hoel , d richardson , r ullrich ( usa ) con icts of interest np works for , and rm is a consultant to , atomic energy of canada ltd . 
 invited specialists none panel : types of radiation classi ed in group 1 ionising radiation alpha - particle emitters beta - particle emitters x - rays and gamma - rays neutron radiation solar radiation ultraviolet radiation ( wavelengths 100400 nm , encompassing uva , uvb , and uvc ) cell killing , ionisation and excitation events that can produce a variety of molecular lesions and clustered , complex dna damage.9 subsequent processing of this damage induces many responses chromosomal ( eg , aberrations , mutations , genomic instability , cell transformation , and bystander e ects ) that contribute to carcinogenesis . 
based on these mechanistic considerations , all types of ionising radiation were classi ed by the working group as carcinogenic to humans ( group 1 )  . solar radiation is the main source of human exposure to ultraviolet ( uv ) radiation , which is further subdivided into uva , uvb , and uvc . 
the working group rea rmed the carcinogenicity of solar radiation ( group 1 )  . exposure to solar radiation causes speci c mutation ngerprint ( cytidine to thymidine transition ) , as a result of cyclobutane pyrimidine dimers in dna . 
this pattern had long been attributed to uvb.10 however , this same cytidine to thymidine transition has been detected the skin of uva - treated mice11 and in the tp53 gene of uva - induced or uvb - induced skin tumours hairless mice.10 in humans , this is widespread transition has been seen in tp53 in premalignant solar keratosis and in malignant skin tumours.12 based on these mechanistic data , the working group classi ed uv radiation as carcinogenic to humans ( group 1 )  . the use of uv - emitting tanning devices in many developed countries , especially among young women . 
a comprehensive meta - analysis concluded that the risk of cutaneous melanoma is increased by 75% when use of tanning devices starts before 30 years of age.13 additionally , casecontrol several studies provide consistent evidence of a positive association between the use of uv - emitting tanning devices and ocular melanoma.14 , 15 therefore , the working group raised the classi cation of the use of uvemitting tanning devices to group 1 , carcinogenic to humans . 
 exposure , while reviewing the studies of occupational uv the working group concluded that there is su cient evidence for ocular melanoma in welders.16 , 17 however , because welders are also exposed to other harmful agents , this association could not be attributed speci cally to uv radiation . 
 fatiha el ghissassi , robert baan , kurt straif , yann grosse , batrice secretan , vronique bouvard , lamia benbrahim - tallaa , neela guha , crystal freeman , laurent galichet , vincent cogliano , on behalf of the who international agency for research on cancer monograph working group international agency for research on cancer , lyon , france the iarc authors declared no con icts of interest . grosse y , baan r , straif k , et al . 
bmj 2005 ; 330 : 223 . national research council , committee to assess health risks from exposure to low levels of ionizing radiation , board on radiation e ects , and research division on earth and life studies . 
 6 national research council , committee to assess health risks from exposure to low levels of ionizing radiation , board on radiation e ects , and research division on earth and life studies . 
uva1 genotoxicity is mediated not by oxidative damage but by cyclobutane pyrimidine dimers in normal mouse skj invest dermatol 2008 ; 128 : 228996 . 12 agar ns , halliday gm , barnetson rs , ananthaswamy hn , wheeler m , jones am . 
ophthalmology 2005 ; 112 : 1599607 . 752 vol 10 august 2009 re ection and reaction lactic acid cycle and is used clinically for the treatment of lactic acidosis , has been shown to decrease lactic acid in the brain in rats , thereby decreasing ischaemic damage.5 this drug improves lactic acidosis after experimental arter ial blockade and might , therefore , also decrease neu ral damage due to ischaemia after radiotherapy . 
 dichloro acetate could also have a potential antitumour e ect , because many cancerseg , glioblastomause the glucose - lactic acid cycle in mitochondrial respiration.6 a phase ii trial has now opened to test the safety and e cacy of dichloroacetate for the treatment of malignant gliomas.7 a drug used in the prevention of delayed bowel injury might also be useful in the prevention of cognitive impairment after radiotherapy . 
haydont and co - workers8 have recently shown in rats that protection of the bowel from delayed radiation injury can be achieved by use of the anticholesterol drug pravastat however , this drug had limited bene t in acute - bowel injury . 
if cognitive impairment , which is likely to be a late reaction to radiotherapy in the brain , has a similar underlying mechanism to delayed - bowel injury , then this drug might have a use in the management of such injury in the brain . the prevention of neural impairment by other methods has also been assessed . 
from these sites , stem cells can migrate to damaged areas elsewhere in the bradue to the fact that only a small percentage of brain metastases occur in the dentate gyrus , the shielding of this area during radiotherapy might , in many situations , be possible , thereby preventing the damage of these repair cells themselves.9 clinical research on the prevention of neurological impairment after radiotherapy is already being done . 
 for example , in a small study of 15 patients with brain tumours , bevacizumab was shown to decrease capillary leakage and radiation necrosis.10 furthermore , erythropoietin has been used to modify irradiation damage to the spinal cord in patients with malignant spinal - cord compression , 11 and , thus , might have a role in modifying radiation damage to the brain . some of these drugs are already commonly used for other indications . 
 john healy 5 claremont villas , glenageary , county dublin , ireland healyjb@eircom.net the author declared no con icts of interest . schagen sb , vardy j , on behalf of the steering committee of the international cognition and cancer task force . 
lancet oncol 2007 ; 8 : 85253 . captopril in treating patients with non - small cell lung cancer or limitedstage small cell lung cancer that has been previously treated with radiation therapy with or without chemotherapy . 
e ect of bevacizumab on radiation necrosis of the braint j radiat oncol biol phys 2007 : 67 : 32326 . loblaw da , holden l , xenocostas a , et al . 
 1056 vol 8 december 2007 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology aware of the di erence in standards of cancer care in the 1980s , 2 i applauded the introduction of an organisation that would provide evidence - based assessment of new technologies backed up by compulsory compliance by those holding the pursestrings to implement de nitive recommendations . 
so why does controversy still surround nice recommendations ? and why do many nd nice unhelpful ? nice cannot choose what they reviewa drug has to have a license for its use in certain settings before the institute can provide guidance . 
fair enough , but nice should have enough nous to know which drugs are likely to be political hot potatoes and to gather preliminary trial evidence to form a view without interference from the government as experienced for trastuzumab . 
this development has been exploited by some drug companies who fund support and information materials for patients , thus encouraging popular demand for a drug that might not be considered were these materials to come from the company directly . probably the biggest criticism is the time taken to produce guidance , especially when compared with the faster ( and cheaper ) scottish systethis delay , or nice blight as it is known , is being addressed by the expansion of the organisation and the introduction of singletechnology appraisals . 
currently costing 33 million a year , what will the institute cost when fully expanded ? other criticisms include the arbitrary gure of 20 00030 000 that nice has attached to a quality - adjusted life - year for the approval of drugs . 
a recent article by john appleby , 3 senior economist at the kings fund , and colleagues asks the question whether it is up to nice to set this gure . littlejohns and colleagues paper attests to the prodigious output of nice , and the institute has an impressively active press o ce . 
trying to contact nice for advice is , however , problematicthis may be the sign of an organisation that is growing fast and cant keep up with its adolescence , but nice must strive to be accessible and not aloof . 
where are the nice audits of the uptake of their guidance ? the cancer tsar , mike richards , has published three audits showing increasing adherence to nice guidance and narrowing of the inequality gap , but should this not be a role for nice ? where are the data on timely implementation of their recommendations ? nice inherited the service guidance reports and completed the set by publishing guidance on skin cancers . 
but are there plans to revisit them , or is the excitement of tackling new drugs too diverting ? where are the recommendations that might now be superseded by the development of new treatments ? in 2003 , the lancet oncology published an article by littlejohns and co - workers4 assessing nice then . 
we , as a society , have to decide the size of our health budget and where we want to send itnice provides guidance and should be encouraged to continue to do so impartially and speedily , and the government should undertake to fund these changing recommendations rather than expect already stretched nhs budgets to swallow them . so , happy birthday nicekeep polishing , avoid the tarnish , and try to engage more . richard sainsbury royal free and university college medical schools , london , uk r.sainsbury@ucl.ac.uk the author declared no con icts of interest . littlejohns p , garner s , doyle n , macbeth f , barnett d , longson c . 
on page 12 of this special report , the installation and calibration of a new particle accelerator at the toulouse - rangueil hospital , toulouse , france , was actually done by a physicist with assistance from brainlab . 
additionally , only 145 patients were treated ( not 5500 as stated ) , and all are currently being followed for any adverse e ects . 316 vol 10 april 2009 re ection and reaction if you would like to respond to an article published in the lancet oncology , please submit your correspondence online at : com / thelancetoncology to submit a manuscript to the lancet oncology visit thelancetoncology to submit a manuscript to the lancet neurology visit ees.elsevier.com / thelancetneurology 1 mosterd k , krekels gam , nieman fhm , et al . 
surgical excision versus mohs micrographic surgery for primary and recurrent basal - cell carcinoma of the face : a prospective randomised controlled trial with 5 - years follow - up . 
however , it is also explained by the fact that some patients were lost to follow - up after 30 months , and were therefore unable to visit our department at that time , but returned into follow - up when they visited our department after a longer period . 
there was no di erence in the method of follow - up between our rst and second publications . regarding the second question raised , we agree that perineural tumour invasion is an important risk factor . 
 finally , although the netherlands indeed an ethnically diverse country , the patients included in our study were people with fitzpatrick skin type i ( 11% ) , ii ( 44% ) , iii ( 35% ) , and iv ( 10% )  . 
 k mosterd * , n kelleners - smeets department of dermatology , maastricht university medical centre , po box 5800 , 6202 az , maastricht , netherlands k.mosterd@mumc.nl the authors declared no con icts of interest . neuro - oncology : a call for papers despite considerable research and the introduction of new therapies , long - term positive outcomes for patients with brain tumours are rare , and most patients experience a recurrence or progression of their cancer irrespective of the intervention . 
we are speci cally interested in the results of randomised controlled trials and other original clinical studies that will have a profound e ect on clinical practice , or on the fundamental understanding of tumour or cns biology , or on the management of neurological sequelae . accepted papers will be published in either the lancet oncology or the lancet neurology , and publication will coincide with the quadrennial meeting of the world federation of neuro - oncology and 6th meeting of the asian society for neuro - oncology ( wfno / asno ) , to be held in yokohama , japan , on may 1114 , 2009 . 
if your submission describes , in part or wholly , a study accepted for presentation at the wfno / asno meeting , please let us know the precise details of the type of presentation ( such as poster or oral presentation ) , including dates and times , so that publication can be scheduled to comply with wfno / asno embargo policies . 
 articles can be submitted via either the lancet oncologys or the lancet neurologys online submission services , but all authors must clearly state in the covering letter that their submission is in response to the tlo / tln call for papers . 
the closing date for this call for papers is march 13 , 2009 . david collingridge , helen frankish the lancet oncology ( dc ) , the lancet neurology ( hf ) , london nw1 7by , uk erratum kubota k , kawahara m , ogawara m , et al . 
vinorelbine plus gemcitabine followed by docetaxel versus carboplatin plus paclitaxel in patients with advanced non - small - cell lung cancer : a randomised , open - label , phase iii study . 
in this article , the hr for overall survival in table 2 should have read : 0996 ( 078127 )  . vol 10 january 2009 strahlentherapie und onkologie originalarbeit ct - gesteuerte brachytherapie eine neue perkutane technik zur interstitiellen ablation von lebermetastasen jens ricke , peter wust , anna stohlmann , alexander beck , chie hee cho , maciej pech , gero wieners , birgit spors , michael werk , christian rosner , enrique lopez hnninen , roland felix1 ziel : analyse der sicherheit und effektivitt ct - gesteuerter brachytherapie zur ablation von lebermalignomen . 
alle patienten wiesen umstnde auf , die eine bildgefhrte thermische ablation mit radiofrequenz oder laserinduzierter thermotherapie ( litt ) einschrnkten : tumordurchmesser 5 cm bei sieben , enge lagebeziehung zu pfortader oder groen lebervenen bei zehn , enge lagebeziehung zur hepatikusgabel bei vier patienten . 
 patients and methods : 21 patients with 21 liver malignancies ( 19 metastases , two primary liver tumors ) were treated with interstitial ct - guided brachytherapy applying a 192ir source . 
in all patients , the use of image - guided thermal tumor ablation such as by radiofrequency or laser - induced thermotherapy ( litt ) was impeded either by tumor size 5 cm in seven , adjacent portal or hepatic vein in ten , or adjacent bile duct bifurcation in four patients . 
als minimalinvasive alternative zu offen - chirurgischen anstzen haben sich thermische lebermetastasenablationen wie radiofrequenz oder laserinduzierte thermotherapie ( litt ) etabliert [ 5 , 25 , 26 , 28 , 31 ]  . 
fr alle thermischen verfahren gelten jedoch limitationen hinsichtlich der maximal mglichen tumorausdehnung ( < 5 cm ) sowie mangelhafter wirksamkeit der methoden bei hyperperfundierten tumoren oder benachbarten khlenden gefen [ 3 , 9 , 20 ]  . 
 patienten und methodik zwischen januar 2001 und dezember 2002 wurden 21 konsekutive patienten in diese studie eingeschlossen , die mit 21 lebermalignomen einer chirurgischen therapie nicht zugnglich waren oder eine chirurgische leberteilresektion abgelehnt hatten . 
weitere einschlusskriterien umfassten die zurckliegende sanierung des primarius , einen karnofsky - index 80% , leberfunktion child a , quick 50% , partielle thromboplastinzeit ( ptt ) < 50 s , thrombozyten > 100 000 . 
 alle patienten wiesen besonderheiten auf , die eine bildgefhrte thermische ablation mittels litt oder radiofrequenz ungnstig beeinflusst oder unmglich gemacht htten . sieben patienten hatten tumoren 5 czehn tumoren zeigten eine enge lagebeziehung zu oder eine infiltration der linken oder rechten pfortaderste oder groen lebervenen . weitere vier patienten demonstrierten eine enge lagebeziehung zur hepatikusgabel oder eine infiltration des rechten oder linken ductus hepaticus . 
ber einen steifen angiographischen fhrungsdraht ( amplatz , boston scientific , usa ) wurde nach entfernung der nadel eine 6 - f - angiographieschleuse eingesetzt ( radiofocus , terumo , japan )  . 
 nach positionierung der brachytherapiekatheter wurde ein kontrastmittelgesttztes spiral - ct der leber in atemanhaltetechnik akquiriert ( 100 ml iopromid [ ultravist - 370 ] , flussrate : 1 ml / s ; startverzgerung : 80 s )  . 
fr jeden einzelnen katheter wurden dann die abstnde zum tumorrand anhand von referenzpunkten kodiert . die angestrebte minimale zieldosis fr den einsatz eines 192irbrachytherapieapplikators betrug 20 gy am tumorrand und wurde als einzeitdosis festgelegt . 
vor und nach dem eingriff wurden folgende laborparameter erhoben : bilirubin , ap , - gt , alt , ast , albumin , hmoglobin , blutbild , quick - wert und ptt . 
tumorvolumetrie sowie zur volumetrischen erfassung der leberparenchymanteile , die einer dosis > 5 gy ausgesetzt worden waren . die lokale tumorkontrolle , das gesamtberleben , das progressionsfreie berleben sowie das progressionsfreie berleben mit unterscheidung von intraund extrahepatischem progress wurde anhand der kaplan - meier - methode ermittelt . 
zum ausschluss einer korrelation zwischen laborparametervernderungen und dem umfang bestrahlten tumoroder lebervolumens wurde der ( cid : 2 ) 2 - test verwendet . abbildung 1a figure 1a abbildung 1b figure 1b abbildung 1c figure 1c abbildung 1d figure 1d abbildungen 1a bis 1d . 
fusionsbild aus einem ct - schnitt und dem aus dem dreidimensionalen datensatz errechneten bestrahlungsplan an identischer position in der z - achse . die offenen pfeile markieren die 5 - gy - isodose , die geschlossenen pfeile die 20 - gy - isodose . 
ct - gesteuerte brachytherapie ergebnisse die durchschnittliche gre der mittels ct - gesteuerter brachytherapie behandelten lebermalignome betrug 4 , 6 cm ( 2 , 511 cm ; median : 4 , 8 cm )  . 
 die minimale dosis , die innerhalb des tumorvolumens appliziert wurde , betrug 20 gy bei sieben , 18 gy bei sieben , 15 gy bei fnf und 12 gy bei zwei patienten ( mittlere dosis : 17 gy )  . 
der anteil gesunden leberparenchyms , der einer dosis > 5 gy exponiert wurde , belief sich im mittel auf 18% ( 539% ; durchschnittlich 286 ml [ 59624 ml ] )  . 
 sechs von 21 patienten ( 28% ) zeigten geringfgige komplikationen im sinne von belkeit und erbrechen . ein patient ( 5% ) erlitt eine versptete schwerwiegende komplikation durch eine 2 wochen post interventionem auftretende obstruktion des ductus choledochus bei hilusnah im linken leberlappen gelegener , 8 cm messender metastase . 
der einsatz computertomographischer dosimetrie erlaubt grte genauigkeit der strahlenexposition des tumorvolumens bei gleichzeitiger schonung benachbarter risikoorgane wie leberparenchym auch im sinne hepatischer reserve , gallenwege oder darm [ 13 , 16 , 22 , 32 ]  . 
 die mittels ct - gesteuerter brachytherapie erzielten lokalen kontrollraten lagen bei 87% und 70% nach 6 und 12 monaten und waren damit den ergebthermischer tumorablationen nissen mindestens ebenbrtig [ 30 ]  . 
aus onkologischer sicht bemerkenswert sind die ergebnisse des gesamtberlebens nach 1 jahr mit einer berlebenswahrscheinlichkeit von 65% . die durch brachytherapie behandelten leberherde waren in der regel therapierefraktr und stellten damit einen limitierenden prognostischen faktor dar . die hlfte der patienten erhielt im anschluss an die brachytherapie eine begleitende systemische chemotherapie , die in allen fllen als zweitoder drittlinientherapie anzusehen war . 
selbst wenn ein teil klinisch stummer oder in der radiologischen standardnachsorge verdeckter extrahepatischer tumormanifestationen in unserer studienpopulation dem nachweis entgangen sein drfte , scheint eine aggressive therapie der leberherde damit onkologisch bei patienten in gutem allgemeinzustand ( karnofsky - index 80% ) durchaus gerechtfertigt . 
die verlaufskontrollen ergaben jedoch einen lokalen progress bei 42% der patienten [ 1 ]  . neben der methodenbedingt ungenauen dosimetrie geht durch die laparotomie der vorteil der minimalen invasivitt bei bildfhrung und perkutanem vorgehen verloren [ 6 ]  . 
 fr die eigene studie nehmen wir an , dass der einsatz dreidimensionaler ct - datenstze und die damit verbundene hohe genauigkeit der dosimetrie entscheidend fr die guten resultate hinsichtlich lokaler tumorkontrolle gewesen sind [ 2 , 14 , 15 , 21 , 23 , 27 ]  . 
ct - gesteuerte brachytherapie die ergebnisse dieser studie demonstrieren , dass die ctgesteuerte brachytherapie sicher eingesetzt werden kann . nur in einem fall kam es zu einer schwerwiegenden komplikation mit einer galleabflussbehinderung durch obstruktion des ductus choledochus 2 wochen nach bestrahlung einer unmittelbar benachbarten metastase . 
 hinsichtlich der strahlenexposition gesunden leberparenchyms und der damit verbundenen gefhrdung der leberfunktion nach dem eingriff ist zu bemerken , dass die funktionelle kapazitt der leber direkt proportional der anzahl intakter hepatozyten sein drfte [ 10 , 11 , 17 , 18 ]  . 
zur planung der brachytherapie wurde von uns in anlehnung an die allgemein akzeptierte mglichkeit der chirurgischen zweidrittelresektion festgelegt [ 19 ] , dass ein drittel der leber maximal 5 gy als einzeitdosis erhalten drfte . 
wir gingen hierfr von der erkenntnis aus , dass bei fraktionierten schemata mit 1 , 82 gy eine toleranzdosis gesunden leberparenchyms von 30 gy ermittelt wurde [ 4 ]  . 
da uns eine zu erwartende geringe einschrnkung der hepatischen funktion auch unterhalb der toleranzdosis von 10 gy nicht kalkulierbar erschien , wurde zur erhhung der sicherheit eine halbierung des werts als grenzwert fr die bestrahlungsplanung festgelegt ( entsprechend 5 gy )  . 
die von den autoren nach der applikatoreinbringung fr die dosimetrie eingesetzten durchleuchtungsaufnahmen erlauben jedoch keine genaue planung , wie sie mit dreidimensionalen datenstzen erreicht wird ( abbildung 1b ) [ 12 ]  . 
bercksichtigt werden sollte fr die bewertung unserer eigenen ergebnisse , dass die minimale dosis im tumorvolumen bei zwei patienten nur 12 gy , die durchschnittliche minimale dosis 17 gy betrug . 
jens ricke klinik fr strahlenheilkunde charit virchow - klinikum augustenburger platz 1 13353 berlin deutschland telefon ( + 49 / 30 ) 4505 - 57001 , fax - 57901 e - mail : jens.ricke@charite.de strahlenther onkol 2004 no . 
5 urban & vogel strahlentherapie und onkologie original article linac radiosurgery versus whole brain radiotherapy for brain metastases a survival comparison based on the rtog recursive partitioning analysis martin kocher1 , mohammad maarouf2 , mark bendel1 , juergen voges2 , rolf - peter mller1 , volker sturm2 background and purpose : for patients with inoperable brain metastases , whole brain radiotherapy ( wbrt ) has been the standard treatment for decades . 
the prognostic factors derived from the rtog recursive partitioning analysis ( rpa ) provide a framework that allows a nonrandomized comparison of the two modalities . patients and methods : from 1991 to 1998 , 117 patients with one to three previously untreated cerebral metastases underwent single - dose linac radiosurgery ( median dose 20 gy ) without adjuvant wbrt . 
after radiosurgery , 26 / 117 patients ( 22% ) had salvage wbrt , radiosurgery or neurosurgical resection of recurrent ( 4 / 117 ) and / or new ( 24 / 117 ) metastases . 
survival of these patients was compared to a historical group of 138 patients with one to three lesions treated by wbrt ( 3036 gy / 3 - gy fractions ) from 1978 to 1991 ; only nine of these patients ( 7% ) had salvage wbrt . 
 conclusion : radiosurgery in patients with one to three cerebral metastases results in a substantial survival benefit only in younger patients with a low systemic tumor burden when compared to wbrt alone . 
 key words : stereotactic radiosurgery whole brain radiotherapy cerebral metastases strahlenther onkol 2004 ; 180 : 2637 doi 10.1007 / s00066 - 004 - 1180 - y radiochirurgie versus ganzhirnbestrahlung bei hirnmetastasen . 
 patienten und methodik : von 1991 bis 1998 erhielten 117 nicht vorbehandelte patienten mit ein bis drei hirnmetastasen eine linac - radiochirurgie ( mediane dosis 20 gy ) ohne adjuvante wbrt . 
zustzlich wurden 26 / 117 patienten ( 22% ) wegen eines lokalen metastasenrezidivs ( 4 / 117 ) oder neu aufgetretener hirnmetastasen ( 24 / 117 ) erneut mittels radiochirurgie , wbrt oder neurochirurgischer resektion behandelt . 
das berleben dieser patienten wurde mit einer historischen gruppe verglichen ( n = 138 ) , die von 1978 bis 1991 bei ein bis drei hirnmetastasen eine alleinige ganzhirnbestrahlung ( 3036 gy / 3 - gy - fraktionen ) erhielt . hiervon wurden nur neun patienten ( 7% ) wegen eines rezidivs erneut mit einer wbrt behandelt . 
 ergebnisse : in der rpa - klasse i ( karnofsky - index 70 , primrtumor kontrolliert , keine weiteren metastasen , alter < 65 jahre ) fhrte die radiochirurgie zu einem medianen berleben von 25 , 4 monaten ( n = 23 , konfidenzintervall [ ci ] 5 , 845 , 0 ) und war so1 department of radiation oncology , and 2 department of stereotaxy and functional neurosurgery , university of cologne , germany . 
in der rpa - risikoklasse ii ( alle anderen patienten ) fhrte die radiochirurgie nur zu einem geringen , aber signifikanten berlebensvorteil ( radiochirurgie : n = 74 , 5 , 9 monate , ci 3 , 28 , 5 , wbrt : n = 61 , 4 , 1 monate , ci 3 , 44 , 9 ; p < 0 , 04 )  . schlussfolgerung : im vergleich zur alleinigen wbrt fhrt die radiochirurgie bei patienten mit ein bis drei hirnmetastasen nur in jngerem alter und bei geringer systemischer tumorausbreitung zu einer prognoseverbesserung . 
mglicherweise spielt hierfr die hhere verfgbarkeit von salvage - therapien eine rolle . schlsselwrter : stereotaktische radiochirurgie ganzhirnbestrahlung hirnmetastasen introduction radiosurgery is , nowadays , a widely accepted treatment modality for inoperable brain metastases . 
several retrospective studies [ 7 , 8 , 10 , 18 , 23 ] and one randomized study [ 4 ] have shown increased local control rates of the irradiated lesions when compared to whole brain radiotherapy ( wbrt ) alone [ 15 ] , and most of these studies also suggested an increase in median survival from 34 months ( wbrt ) to 712 months ( radiosurgery ) [ 1 , 5 , 7 , 8 , 10 , 12 , 18 , 20 , 23 ]  . 
randomized trials , however , have failed to demonstrate a general survival benefit of radiosurgery so far [ 4 , 11 ] , probably because these metastatic patients have a high risk to die from extracranial tumor spread and intercurrent death , such that only about 3040% will eventually experience neurologic death . 
the classification is mainly based on the patients general ability to resist the malignant disease ( age , performance score ) and on the presence of extracranial tumor ( primary tumor , other extracranial metastases )  . 
this analysis provides a framework that allows to group patients and analyze treatment effects in a nonrandomized manner . for the present investigation , it was used to compare the survival times in patients with inoperable brain metastases treated by radiosurgery to those of a historical collective treated by wbrt alone . 
only patients with one to three metastases were studied , because , according to institutional policy , only up to three metastases were treated by radiosurgery and , in addition , evidence exists that in case of four or more metastases , the rpa loses its predictive power [ 14 ]  . 
 patients and methods treatment groups from 1991 to 1998 , 117 previously untreated patients ( 41 females , 76 males , median age 60 years ) with one to three cerebral metastases were treated by single - dose linac radiosurgery ( median marginal dose 20 gy , range 1525 gy ) without adjuvant wbrt . 
the most frequent primary tumor type was non - small - cell lung cancer ( 30% ) , followed by malignant melanoma ( 27% ) , hypernephroma ( 13% ) , breast carcinoma ( 12% ) , and other types ( 18% )  . 
patients with singular metastases in this group had either deep - situated tumors not suitable for resection or were referred for radiosurgery rather than surgery because of the physicians or patients preference . 
 survival of these patients was compared to a historical group ( 19781991 ) of 138 patients ( 58 females , 80 males , median age 58 years ) with one to three otherwise untreated brain metastases who received wbrt ( 3036 gy / 3 - gy fractions in 80% , 40 gy / 2 - gy fractions or boost up to 50 gy in 20% ) in the same institution . 
in this group , non - small - cell lung cancer ( 28% ) was also dominant , but breast cancer ( 19% ) which is thought to have a slightly better prognosis [ 9 ] was more frequent ( melanoma 6% , hypernephroma 5% , others 42% )  . 
the rpa demonstrated that all other known prognostic factors such as histology , primary site , time interval , number of lesions , and neurologic function are of minor importance . 
in twelve patients , wbrt ( 3036 gy / 3 - gy fractions ) was used , seven patients had salvage radiosurgery , five received both wbrt and radiosurgery , and four had their recurrences resected . 
linac radiosurgery versus wbrt for brain metastases local control ( radiosurgery targets ) outfield metastases 0.0f class iii class ii class i class iii class ii class i months months figure 2 . 
in rpa class ii ( all other patients ) , radiosurgery produced a small , but significant survival advantage ( radiosurgery : n = 74 , 5.9 months , ci 3.28.5 , wbrt : n = 61 , 4.1 months , ci 3.44.9 ; p < 0.04 ; figure 1 )  . 
 discussion while it seems unequivocal that radiosurgery improves local control of the irradiated metastases when compared to wbrt [ 4 ] , a substantial survival benefit has not been demonstrated yet . 
probably , the reason for this observation stems from the fact that patients with brain metastases have , in addition to local brain recurrence , competing risks , namely systemic progression , distant intracranial failure , and intercurrent death . obviously , radiosurgery of the visible brain metastases solves only part of the problem these metastatic patients have . 
 therefore , one can expect a survival advantage as a result of an increased local control rate of the irradiated brain metastases only in patients in good condition with a low systemic tumor burden and for whom effective means to control intracranial distant relapses are available . 
 in the radiosurgery group , 6 / 117 patients ( 5% ) had evidence of radiation necrosis [ 13 ] indicated by ct and / or mri scans 15 comparable retrospective and randomized analyses have been conducted for the combined treatment with radiosurgery side effects strahlenther onkol 2004 no . 
the addition of adjuvant wbrt to radiosurgery seems to increase local control and to decrease the frequency of new intracranial failures , but survival by rpa class remains unchanged [ 3 , 4 , 21 ]  . 
the addition of radiosurgery to wbrt resulted in a survival benefit for patients of all rpa classes in one retrospective study [ 19 ] , but a phase iii trial that has recently been published in abstract form showed a survival advantage ( 2 months ) only for rpa class i patients [ 22 ]  . 
in the radiosurgery group , 7 / 22 ( 30% ) of all patients had subsequent salvage radiosurgery ( n = 1 ) , wbrt ( n = 3 ) , radiosurgery and wbrt ( n = 2 ) , or neurosurgery ( n = 1 ) , while only 1 / 9 patients in the wbrt group had another wbrt . 
therefore , the purpose of this study was to document the changes of the oxygenation status in spontaneous canine tumors during fractionated radiation therapy using polarographic needle electrodes . material and methods : tumor oxygen partial pressure ( po2 ) measurements were performed with the eppendorf - po2 - histograph . the measurements were done under general anesthesia , and probe tracks were guided with ultrasound . 
oxygenation status of the palliative patient group was examined before each fraction of radiation therapy up to five times ( total dose : 2430 gy )  . results : 15 / 26 tumors had a pretreatment median po2 mors during fractionated radiation therapy . 
 1 section of diagnostic imaging and radiation oncology , veterinary school , university of zurich , switzerland , 2 institute for veterinary physiology , university of zurich , switzerland , 3 institute for social and preventive medicine , university of zurich , switzerland . 
the assessment of pretreatment oxygenation status has been shown to be of prognostic relevance for tumor recurrence , metastases , and survival [ 9 , 15 , 21 , 36 ]  . 
according to the oxygen fixation hypothesis , the radiation - induced damage to the dna can be fixed in the presence of oxygen but repaired under hypoxic conditions [ 20 ]  . 
proposed mechanisms thought to be responsible for the process of reoxygenation are changes in tumor blood flow and vascular architecture , reduced interstitial pressure , and a decrease in cellular oxygen consumption [ 5 , 26 , 28 , 33 , 44 ]  . 
an increase of mean oxygen tension after irradiation has been reported in early clinical studies in the 1960s describing oxygen partial pressure ( po2 ) measurements during fractionated radiation therapy [ 2 , 10 ]  . 
because of limited patient compliance , measurements often could only be performed pre - , midand posttreatment ; therefore , interpretation of these results is difficult [ 11 , 13 , 17 , 31 ]  . 
 [ 7 ] performed a second set of po2 measurements in 27 human patients suffering from head and neck squamous cell carcinoma and reported no changes in oxygenation after exposure to 1015 gy . 
furthermore , information on the oxygenation status may play an important role when adjuvant anti - angiogenetic agents or hypoxic cell toxins are considered to be used in combination with radiation therapy , because tumor oxygenation status represents the most important stimulus for angiogenesis [ 14 ]  . 
the mean value of mean corpuscular volume ( mcv ) was 65.9 fl ( range : 5470.7 fl ; normal : 6077 fl ) , the mean level of corpuscular hemoglobin ( mch ) 23.1 pg ( range : 1925 pg ; normal : 19.524.5 pg ) , and mean corpuscular hemoglobin concentration ( mchc ) 35.1 g / dl ( range : 3336.6 g / dl ; normal : 3236 g / dl )  . 
the initial tumor response at the end of fractionated radiation therapy was defined as no response ( unchanged tumor volume ) , partial response ( decreased tumor volume ) , or complete response ( no macroscopic tumor disease )  . 
intravenously , midazolam ( dormicum , roche pharma ag , reinach , switzerland ) was injected at a dosage of 0.125 mg / kg immediately followed by propofol ( propofol , fresenius kabi ag , stans , switzerland ) , slowly administered to effect . 
po2 changes in canine tumors during radiotherapy ments were initiated when focal bleeding was under control . tumor oxygen partial pressure measurements were performed with the eppendorf - po2 - histograph ( helzel medical system , kaltenkirchen , germany , previous eppendorf netheler hinz gmbh , hamburg , germany )  . 
the dogs scheduled for curative radiation therapy had oxygen measurements before fraction 1 , 3 , 6 , 8 , 10 , 12 , 14 , and 16 . the irradiation protocol for the curatively treated dogs was 1417 ( cid : 1 ) 3.5 gy ( n = 6 ) given on a monday / tuesday / thursday / friday schedule or daily 3 - gy fractions 1517 times ( n = 4 )  . 
tumor response at the end of fractionated radiation therapy was defined as no response ( nr ) : unchanged tumor volume ; partial response ( pr ) : decreased tumor volume ; complete response ( cr ) : no macroscopic tumor disease . 
therapieerfolg am ende der radiotherapie wurde definiert als kein ansprechen ( nr ) : unverndertes tumorvolumen ; partielles ansprechen ( pr ) : vermindertes tumorvolumen ; komplettes ansprechen ( cr ) : tumor makroskopisch nicht mehr nachweisbar . 
po2 changes in canine tumors during radiotherapy thews & vaupel [ 43 ] : statistical parameters were minimum of po2 , median po2 , mean po2 , standard deviation of po2 , the inter - quantile range ( iqr ) of po2 , and the maximum of po2 . the biological relevance was given by the relative frequency of values 2.5 mmhg , 5 mmhg , and 10 mmhg . 
quality parameters were the minimum po2 , maximum po2 , count and percentage of measurements < 0 mmhg and > 100 mmhg , and the total count of recorded values ( data not completely shown )  . 
furthermore , dose intervals were defined ( 69 gy , 1215 gy , 1621 gy , 2427 gy , 3033 gy , 38.539 gy , and 4545.5 gy ) to compare the different curative and palliative irradiation protocols . 
two tumors showed no response at the end of fractionated radiation therapy , in 18 tumors a partial response was seen , and four dogs had a complete response after radiaton therapy . 
the packed cell volume ( pcv ) negatively correlated with the tumor volume as well as with the hsv . the other blood parameters reported did not correlate with po2 parameters . 
in individual tumors , a combination of increase and decrease of po2 was observed as well as constantly hypoxic po2 courses ( figure 1 )  . when all measured tumors were combined , a decrease of the median po2 during the initial phase of radiation therapy was followed by an increase and again a decrease toward the end of therapy . 
however , since confidence intervals overlapped , the changes were not statistically significant ( figure 2 ) .when the study population was grouped into initially hypoxic and initially normoxic tumors , a significant difference was seen ( figure 3 )  . 
deskriptive statistische analyse des prtherapeutischen sauerstoffpartialdruckes ( po2 ) in 26 spontanen caninen tumoren . % 2 , 5 , 5 , 10 mmhg : relative frequenz der messwerte 2 , 5 , 5 , 10 mmhg ; iqr : bereich quantile 2575% ; sd : standardabweichung ; se : standardfehler . 
% 2 , 5 , 5 , 10 mmhg : relative frequenz der messwerte 2 , 5 , 5 , 10 mmhg ; hsv : hypoxisches subvolumen ; mcv : mittleres korpuskulres volumen ; pcv : hmatokrit . 
 the dose per fraction ( high [ 68 gy ] = palliative ; low [ 33.5 gy ] = curative ) had no influence on tumor oxygenation . there was no statistical difference . 
 discussion squamous cell carcinoma ( dog 13 ) fibrosarcoma ( dog 9 ) oral melanoma ( dog 25 ) it is well established that tumor oxygenation has an impact on tumor growth , tumor recurrence and development of metastases . 
the phenomenon of reoxygenation plays a major role in clinical radiotherapy , because it increases the cell kill of initially hypoxic tumor cells during fractionated radiotherapy [ 24 ]  . 
primarily based on laboratory work [ 19 ] , one assumes reoxygenation does also take place in human patients [ 31 ]  . therefore , we wanted to investigate first the pretreatment oxygenation status in spontaneous canine tumors and then obtain serial oxygen measurements in these tumor in order to describe the oxygen changes over the course of radiation therapy . 
the high percentage of hypoxia in these tumors could , in part , be explained by the fact , that 20 of the 26 tumors analyzed were of soft tissue origfrom human medicine it is known that sarcomas tend to be severely hypoxic [ 8 , 9 ]  . 
only a negative correlation between the hypoxic fraction and mcv was observed.this negative correlation between the mcv and the hypoxic fraction found in this study has already been reported previously [ 1 ]  . 
in human patients , a hemoglobin level between 12 and 14 g / dl was found to be optimal for tumor oxygenation [ 46 ]  . repeated po2 measurements were done very carefully . 
 oxygen levels in individual tumors were seen to increase , decrease or undulate over the course of radiation therapy . this is in agreement with a study on human head and neck carcinomas , where a significant increase as well as a decrease in oxygenation were found [ 31 ]  . 
other studies reported either an indose ( gy ) crease or a decrease of po2 in head and neck or cervical carcinoma [ 11 , 17 , 29 ]  . 
interestingly , a periodicity of the blood flow as well as of the po2 ( range : 1.338.5 mmhg ) of four to seven cycles in 1 h was found . 
however , when a single dose of 40 gy versus 20 gy was applied in a c3h mouse mammary carcinoma , tumors reoxgenated , but it took 12 rather than 4 h [ 18 ]  . 
however , at this moment in time , the median for kaplan - meier survival analysis has not been reached . acknowledgment we would like to thank professor martin meuli , childrens hospital , university of zurich , switzerland , for providing of the eppendorfpo2 - histograph . strahlentherapie und onkologie aktuelles forum rechtsfragen in der radioonkologie anforderungen an das aufklrungsgesprch und die dokumentation der behandlung mit fallbeispielen aus der aktuellen rechtsprechung fr das fachgebiet strahlentherapie radioonkologie * stefan hesselmann1 , leonie strauss2 , oliver micke1 , stefan knemann1 , andreas schuck1 , normann willich1 hintergrund : in den letzten jahren sind die rztliche aufklrung , die rztliche behandlung und deren folgen , u.a. 
eine folge dieses neuen ffentlichen bewusstseins um das einzelschicksal betroffener ist , dass die anforderungen an die rztliche aufklrung vor und im rahmen einer behandlung immer anspruchsvoller werden , damit der behandelnde arzt sich nicht schadenersatzpflichtig oder gar strafbar macht . 
in der praxis werden arzthaftungsflle aufgrund von beweisschwierigkeiten bei behandlungsfehlern in der regel nicht auf den vorwurf eines behandlungsfehlers , sondern gewissermaen als auffangtatbestand auf den vorwurf der fehlerhaften aufklrung gesttzt . 
denn lsst sich einem arzt kein behandlungsfehler nachweisen , so doch ( fast ) immer eine aufklrungspflichtverletzung . methodik : methodische darstellung der grundstze , die bei der aufklrung und der dokumentation einer strahlentherapeutischen behandlung erforderlich sind , unter bercksichtigung von fallbeispielen aus der aktuellen rechtsprechung . 
 schlussfolgerung : jeder arzt ist gezwungen , sich intensiv mit medizinrechtlichen fragen und problemen zu beschftigen , obgleich die rechtsprechung zum inhalt und umfang der aufklrungspflicht so vielschichtig und komplex ist , dass sie sich einem nichtjuristen , also auch einem mediziner , nicht ohne weiteres erschliet . 
nur so kann der einzelne arzt die problematik der zunehmenden tendenz , aus einer scheinbar nicht ordnungsgem durchgefhrten aufklrung finanziellen gewinn zu schlagen , entgegenwirken und einen arzthaftungsprozess , wenn er denn nicht zu vermeiden ist , zumindest fr sich entscheiden . 
demands on patient information and documentation of the therapy with examples of current legal cases concerning the specialization radiotherapy radiooncology background : in recent years , also due to the media , the medical information a physician gives to his patients , the methods of medical treatment and their consequences have increasingly come to the attention of the general public . 
as a result , to avoid claims for compensation because of faulty treatment or even to evade prosecution , the demands on medical information given before or during treatment are getting greater and greater . 
as a rule as a way out of difficulties these claims for compensation are based on the accusation of mistaken or incomplete information , because if one cannot prove any wrong treatment , faulty information can ( nearly ) always be proven . 
 methods : methodically , showing the principles that must be followed when giving information on radiotherapy and when documenting it , also taking examples of current legal cases into account . 
 conclusion : every attending physician should feel obliged to pay attention to legal questions concerning medical subjects , though judgments on the contents and the extent of the information that must be given to patients are complex and difficult to understand for anybody not experienced in law . 
only so the ever - increasing tendency of people to try to make financial profit on information that they consider mistaken or incomplete can be opposed and a lawsuit can be won , if it cannot be avoided . 
defensivmedizeine folge dieses neuen ffentlichen bewusstseins um das einzelschicksal betroffener geschdigter ist , dass die anforderungen an die rztliche aufklrung vor und im rahmen einer behandlung immer anspruchsvoller werden , damit der behandelnde arzt sich nicht schadenersatzpflichtig oder gar strafbar macht . dadurch ist die rzteschaft gezwungen , sich selbst intensiv mit medizinrechtlichen fragen und problemen zu beschftigen , obgleich die rechtsprechung zum inhalt und umfang der aufklrungspflicht so vielschichtig ist , dass die annahme nicht gerechtfertigt scheint , sie sei einem nichtjuristen , also auch einem mediziner , ohne weiteres verstndlich ( kg versr 79 , 260 [ 261 ] ) [ 1 , 2 , 4 , 5 , 79 , 1113 , 15 , 17 ]  . 
mai 1894 ( rgst 25 , 375ff . ) herrschende rechtsprechung , dass auch ein erfolgreich abgelaufener rztlicher eingriff in den krper des erkrankten patienten den tatbestand der krperverletzung erfllt , der schon kraft gesetzes rechtswidrig ist . 
 die aufklrung des patienten wer klrt auf ? grundstzlich hat der behandelnde arzt den patienten ber die mit der behandlung verbundenen risiken aufzuklren ( hamm versr 94 , 815 ; oldenburg versr 99 , 1422 )  . 
da im laufe einer behandlung meist mehrere rzte den patienten behandeln , ist es empfehlenswert , dass der jeweils fr die behandlung zustndige arzt darber aufklrt , welche manahmen er beabsichtigt . 
 wird die aufklrung ber verschiedene behandlungsschritte auf einen arzt bertragen , der in die behandlung des patienten involviert ist , so haftet dieser , wenn die aufklrung nicht umfassend war und damit in teilen unwirksam ist ( olg schleswig njw - rr 94 , 1052 )  . 
geschieht dies nicht , gehen alle fehler des tatschlich aufklrenden arztes zu lasten des delegierenden arztes . ein arzt im praktikum darf ber behandlungen aufklren , die er unter der verantwortung und der aufsicht des ausbildenden arztes durchfhrt , sowie auch ber solche , die er nicht selbst durchfhrt . 
 bei auslndischen , der deutschen sprache nicht ( ganz ) mchtigen patienten muss der arzt zum aufklrungsgesprch sprachkundige personen ( angehrige , pflegepersonal , ggf . einen vereidigten dolmetscher ) hinzuziehen , wenn unklar ist , ob der patient den erklrungen folgen kann . 
ist also ein sofortiger rztlicher eingriff geboten , um die gesundheit des patienten zu erhalten , kann auf die aufklrung verzichtet werden ( beweislast diesbezglich liegt beim arzt )  . 
 inhalt und umfang der aufklrung die aufklrung des patienten umfasst die aufklrung ber die notwendige rztliche behandlung grundund risikoaufklrung sowie die sicherung einer sachgerechten nachbehandlung sicherungsund nachsorgeaufklrung ( olg stuttgart medr 96 , 81 )  . 
laut einem urteil des olg hamm vom 24.4.1991 darber aufzuklren , dass bei einer relativen indikation fr eine adjuvante strahlentherapie nach der operation eines mammakarzinoms nur einem nicht gnzlich auszuschlieenden risiko eines lokalrezidivs vorgebeugt werden kann ( az . : 3 u 186 / 90 )  . der arzt darf durch die art der gesprchsfhrung dem patienten die entscheidung nicht abnehmen oder vorgeben , aber durchaus einen eindeutigen rat erteilen ( keine stellvertreterentscheidung )  . erforderliche untersuchungen einschlielich deren aussagekraft und der damit verbundenen risiken sind zu erklren . 
 stehen mehrere medizinisch indizierte und bliche behandlungsmethoden zur verfgung , die unterschiedliche erfolgschancen haben oder auch unterschiedliche belastungen und risiken mit sich bringen , so besteht eine echte wahlmglichkeit fr den patienten . 
 eine aufklrungspflichtige behandlungsalternative in form einer echten wahlmglichkeit liegt nicht vor , wenn sich ein alternatives verfahren erst in der erprobung befindet bzw . lediglich in form eines forschungsprojektes erprobt wird ( lg koblenz versr 94 , 1349 ) [ 14 , 16 ]  . 
 ob ein gesetzlich versicherter patient ber eine behandlungsalternative aufzuklren ist , die ihm nur als selbstzahler zur verfgung steht , weil die gesetzliche krankenversicherung sie aus ihrem leistungskatalog ausklammert , hat der bundesgerichtshof bisher nicht entschieden [ 14 ]  . 
 wenn die technischen behandlungsmglichkeiten ( z.b. nur telekobaltgert oder linearbeschleuniger mit niedriger energie vorhanden , simulationsgert nicht vorhanden ) fr eine bestimmte erkrankung nicht mehr dem medizinischen standard entsprechen , so ist darauf hinzuweisen , dass die behandlung in einem anderen , besser ausgestatteten zentrum durchgefhrt werden sollte ( olg mnchen versr 93 , 607 )  . falls der patient dieses nicht wnscht , ist dieses gesondert zu dokumentieren ( olg mnchen versr 93 , 607 )  . 
 wenn die gewhlte bestrahlungstechnik ( zweifeld - telekobaltbestrahlung nach brustkrebsoperation ) zum behandlungszeitpunkt ( 1983 ) dem behandlungsstandard entsprach , ist es nicht erforderlich , ber alternative techniken ( einfeldbestrahlung ) an grokliniken aufzuklren ( olg oldenburg versr 96 , 1023 )  . 
 risikoaufklrung im rahmen der risikoaufklrung soll der patient ber mgliche vorbergehende und bleibende folgen informiert werden . die einwilligung ist nur wirksam , wenn der patient ein allgemeines bild von der schwere und richtung des konkreten risikospektrums hat ( olg kln versr 88 , 384 )  . 
 der bgh hat ausgefhrt , dass es bei der verwirklichung eines risikos , ber das ein patient aufgeklrt worden ist , keine rolle mehr spielt , ob daneben auch andere risiken , die sich nicht verwirklicht haben , der erwhnung im aufklrungsgesprch bedurft htten . 
 nachsorgeaufklrung zu den pflichten eines radioonkologen zhlt es , die ergebnisse seiner behandlung kontinuierlich selbst zu verfolgen und sich einen eigenen eindruck ber die auftretenden nebenwirkungen und heilungschancen zu verschaffen . 
rztliche aufzeichnungen sind nicht nur gedchtnissttze fr den arzt , sie dienen auch dem interesse des patienten an einer ordnungsgemen dokumentation [ 3 , 6 , 16 , 19 ]  . 
 eine nachtrgliche auch eine ergnzende oder berichtigende vernderung ist ab dem moment unzulssig , wenn der patient zu erkennen gibt , dass er von seinem einsichtsrecht gebrauch oder schadenersatzansprche geltend machen will bzw . 
 art und weise der aufzeichnung und dauer der aufbewahrung die form ist zunchst in das belieben des arztes gestellt . sie muss nicht sofort leserlich erfolgen , stichwrter sind zunchst ausreichend ( tonband oder schriftform )  . 
 rechtspflicht zur offenbarung ? es ist zur zeit umstritten , ob rzte , hnlich wie rechtsanwlte , steuerberater und architekten , verpflichtet sind , den patienten auf einen von ihnen mglicherweise begangenen fehler ungefragt hinzuweisen , selbst wenn dieser nicht mit nachteilen fr den patienten verbunden ist . 
die derzeit vorherrschende rechtsansicht ist , dass eine rechtspflicht zur offenbarung nur dann besteht , wenn es erforderlich ist , einen entstandenen gesundheitsschaden zu beheben oder die entstehung eines weiteren schadens zu verhindern . 
 wer haftet ? grundstzlich trgt der behandelnde arzt die direkte verantwortung fr fehler in der diagnose , die falsche wahl der behandlungsart , das nichteinholen erforderlicher kontrollbefunde , fehler in der behandlungsdurchfhrung und eine fehlende oder fehlerhafte aufklrung ( horizontale haftung )  . 
 ein rztlicher urlaubsvertreter kann ebenfalls fr eine vom vertretenen arzt nach dessen bestrahlungsplanung begonnene therapie mitverantwortlich gemacht werden , zumindest dann , wenn er die behandlung ungeprft fortfhrt , obgleich ausreichende anhaltspunkte fr ernste zweifel an deren richtigkeit fr ihn erkennbar sind ( bgh 19.11.97 3 str 271 [ lg dsseldorf ] )  . 
medizinische wissenschaft und praxis besttigen , verbessern und entwickeln diese standards . die evidenzbasierte medizin wird hier in der lage gesehen , den stand des wissens so aufzuarbeiten , dass sie eine entscheidungshilfe fr den arzt in form von leitlinien erarbeiten kann . 
bis jetzt hat sich der bundesgerichtshof in seiner rechtsprechung ebenfalls noch nie an einer leitlinie orientiert , sondern immer am stand des aktuellen wissens in der medizhier bleibt abzuwarten , ob eine vom mglicherweise entstehenden rztlichen zentrum fr qualitt in der medizin zertifizierte leitlinie demnchst nicht als rechtlich verbindliche handlungsanleitung angesehen wird . 
 fazit jeder arzt ist gezwungen , sich intensiv mit medizinrechtlichen fragen und problemen zu beschftigen , obgleich die rechtsprechung zum inhalt und umfang der aufklrungspflicht so vielschichtig und komplex ist , dass sie sich einem nichtjuristen , also auch einem mediziner , nicht ohne weiteres erschlie . 
nur so kann der einzelne arzt der problematik der zunehmenden tendenz , aus einer scheinbar nicht ordnungsgem durchgefhrten aufklrung finanziellen gewinn zu schlagen , entgegenwirken und einen arzthaftungsprozess , wenn er nicht zu vermeiden ist , dennoch fr sich entscheiden . 
 korrespondenzanschrift stefan hesselmann klinik und poliklinik fr strahlentherapie radioonkologie albert - schweitzer - strae 33 48129 mnster deutschland telefon ( + 49 / 251 ) 83 - 47384 , fax - 47355 e - mail : hessels@uni - muenster.de strahlenther onkol 2004 no . 
5 urban & vogel strahlentherapie und onkologie original article impact of various parameters in detecting chromosomal aberrations by fish to describe radiosensitivity ulrike keller1 , alma kuechler2 , 3 , thomas liehr3 , elisabeth mller1 , gerhard grabenbauer1 , rolf sauer1 , luitpold distel1 background and purpose : analysis of radiation - induced chromosomal aberrations is regarded as the gold standard for classifying individual radiosensitivity . 
 patients and methods : in this study , five patients with severe radiation - induced late effects of at least grade 3 , classified according to the radiation therapy oncology group ( rtog ) , and eleven healthy individuals were examined retrospectively . 
the detailed analysis was focused on the number of breaks per metaphase , on breaks from complex chromosomal rearrangements per metaphase , as well as on the percentage of translocations , dicentric chromosomes , breaks , and excess acentric fragments each in comparison with the total number of mitoses analyzed . 
 results : using the number of breaks from complex chromosomal rearrangements after 2.0 gy , radiosensitive patients as endpoint were clearly to be distinguished ( p = 0.001 ) from healthy individuals . 
the parameters percentage of dicentric chromosomes , breaks , and excess acentric fragments in comparison to the total number of mitoses analyzed could neither serve as meaningful nor as significant criteria , since they showed a strong interindividual variability . 
 conclusion : to detect a difference in chromosomal aberrations between healthy and radiosensitive individuals , the parameters frequency of breaks per metaphase , complex chromosomal rearrangements , and translocations are most suitable . 
 key words : hypersensitivity ionizing radiation chromosomal aberrations complex aberrations fluorescence in situ hybridization ( fish ) strahlenther onkol 2004 ; 180 : 28996 doi 10.1007 / s00066 - 004 - 1200 - y bedeutung verschiedener parameter bei der detektion von chromosomalen aberrationen mit hilfe der fish - technik zur beschreibung der radiosensibilitt hintergrund und ziel : die analyse chromosomaler aberrationen wird als goldstandard angesehen , um individuelle strahlenempfindlichkeit zu detektieren . 
die frage stellt sich , welche parameter die unterschiede zwischen patienten mit erhhter strahlenempfindlichkeit und kontrollpersonen am besten detektieren . patienten und methodik : retrospektiv wurden fnf patienten mit klinisch manifestem strahlenempfindlichkeitssyndrom ( rtoggrad 3 ) und elf gesunde kontrollpersonen untersucht . 
dabei wurden periphere blutlymphozyten vor der kultivierung mit 0 , 7 gy und 2 , 0 gy bestrahlt und mittels drei - farb - fluoreszenz - in - situ - hybridisierung ( fish ) angefrbt . 
die analyse bezog sich auf die anzahl der brche pro metaphase , die anzahl der komplexen aberrationen pro metaphase sowie auf den anteil von translokationen , dizentrischen chromosomen , brchen und zustzlichen azentrischen fragmenten an der gesamtzahl der analysierten mitosen . 
 ergebnisse : mit hilfe des parameters brche aus komplexen aberrationen pro metaphase bei 2 gy konnten erhht strahlenempfindliche patienten als endpunkt klar von kontrollen unterschieden werden ( p = 0 , 001 )  . 
des weiteren waren sowohl translokationen ( p = 0 , 001 ) als auch brche pro mitose ( p = 0 , 002 ) geeignete indikatoren fr die unterscheidung von kontrollpersonen und erhht strahlenempfindlichen patienten . 
die parameter anteil der dizentrischen chromosomen , anteil der brche und anteil der zustzlichen azentrischen fragmente alle bezogen auf die gesamtzahl der analysierten mitosen konnten nicht als signifikante kriterien herangezogen werden , da sie eine groe interindividuelle variabilitt zeigten . 
 1 division of radiobiology , department of radiotherapy , erlangen , germany , 2 division of radiotherapy , department of radiology , jena , germany , 3 institute for human genetics and anthropology , jena , germany . received : june 4 , 2003 ; accepted : december 19 , 2003 strahlenther onkol 2004 no . 
chromosomal aberrations and radiosensitivity schlussfolgerung : um einen unterschied in den chromosomalen aberrationen zwischen kontrollpersonen und erhht strahlenempfindlichen individuen darzustellen , sind die parameter brche pro metaphase , komplexe chromosomale aberrationen und translokationen am besten geeignet . 
 schlsselwrter : erhhte strahlensensibilitt ionisierende strahlung chromosomale aberrationen komplexe aberrationen fluoreszenz - in - situ - hybridisierung ( fish ) introduction despite intensive research [ 1 , 5 , 17 , 21 , 35 ] on individual radiosensitivity , there is still no reliable test available which can be employed predictively in clinical everyday use to describe the individual degree of radiosensitivity . 
 the technique of fluorescence in situ hybridization ( fish ) provides the possibility to paint whole chromosomes . by using various fluorescence - labeled chromosome - painting probes [ 32 ] , metaphases can be examined for aberrations quickly and efficiently . 
 [ 16 , 17 ] analyzed the rate of cells containing aberrations , the percentage of normal and aberrant metaphases , the average rate of breaks per mitosis as well as the average rate of complex chromosomal rearrangements ( ccrs ) per mitosis , the frequency distribution of different aberration types , and the proportion of breaks involved in the formation of ccrs in comparison to the total number of breaks . 
 however , the question that still remains to be settled is which of the parameters used for analyzing chromosomal aberrations by application of three - color fish are most appropriate to distinguish hypersensitive patients from healthy individuals and , furthermore , which of these parameters would show the difference between hypersensitive patients and healthy individuals most clearly , since there is a strong interindividual variability [ 5 , 6 , 36 ]  . 
 the aim of this paper was , therefore , to evaluate various fish parameters regarding their sensitivity in detecting highly sensitive patients compared to healthy individuals at a relatively low dose of 2 gy . 
 patients and methods the study included a sample of five patients with severe radiation - related chronic toxicity of grade 3 according to the radiation therapy oncology group ( rtog ) , and eleven healthy individuals as controls . 
all patients were examined regularly during followup visits and were free of recurrence at the time of evaluation . in each case , late reaction was estimated and classified by the same physician . 
lymphocytes were irradiated in g0 cell cycle phase . x - irradiation was generated by a 6 - mv linear accelerator ( mevatron ; siemens , germany ) with a dose rate of 2.2 gy / min [ 19 ]  . 
each culture consisted of 1 ml whole blood and 9 ml rpmi medium supplemented with 1% penicillin - streptomycin , 2.5% phytohemagglutinin and 15% fetal calf seru3 h before harvesting , colcemid ( 0.1 g / ml ) was added to each culture for mitotic block . 
then , whole chromosome - painting probes ( wcp ) for chromosomes #1 , #2 , and #4 , which together account for approximately 22% of the human genome , were simultaneously hybridized for 48 h at 37 c . 
the biotinylated ( #2 , #4 ) and digoxigenin - labeled ( #1 , #4 ) target chromosomes were detected applying streptavidin - conjugated fluorescein - isothiocyanate ( fitc ) and anti - digoxigenin - rhodamine , painting chromosome #1 in red , #2 in green , and #4 in yellow . 
for scoring , the fish slides fluorescence microscope ( zeiss axioplan ; zeiss , oberkochen , germany ) with a suitable filter combination ( dapi , fitc , texas red ) was used . 
the following parameters were scored separately : the total number of break events ( breaks per metaphase ) , the frequency of breaks per aberrant metaphase , and the number of breaks involved in the formation of ccrs related to the total number of metaphases . 
furthermore , the frequency of aberrant metaphases per total number of metaphases , the frequency of translocations which included reciprocal as well as nonreciprocal translocations , the frequency of dicentrics which were associated with one acentric fragment , the frequency of open breaks and excess acentric fragments which are not related to dicentric chromosomes were recorded . 
the parameters breaks per aberrant metaphase ( p = 0.115 ) , number of aberrant metaphases per total number of metaphases ( p = 0.090 ) , frequency of dicentrics ( p = 0.145 ) , and frequency of open breaks per metaphase ( p = 0.090 ) were not suited to distinguish healthy individuals from patients using the mann - whitney u - test . for the five patients with elevated radiosensitivity , 658 break events were scored , of which 55.2% or 363 breaks derived from complex aberrations , whereas in cells from eleven healthy individuals , 857 breaks occurred and only 25.4% or 218 were breaks derived from ccrs ( table 3 )  . 
additionally , each ccr in cells from hypersensitive patients was more complex with 4.3 breaks per ccr in comparison to 3.6 breaks per ccr in healthy individuals ( data not shown )  . 
 the ratio of ccrs per metaphase to dicentrics and translocations for each single person is presented in figure 2 . the interindividual variability was very high among the hypersensitive patients proven by the standard deviation . 
the mean values of the mis were quite similar to values for healthy individuals of 2.9% mi at 0 gy and 2.0% mi at 2 gy compared to the hypersensitive patients with 3.3% mi at 0 gy and 2.5% mi at 2 gy . 
however , the coefficient of variation ( cv 0 gy = 97% , 2 gy = 99% ) had a much higher variation compared to the healthy individuals ( cv 0 gy = 21% , 2 gy = 45% )  . 
the correlation between mitotic rates in unirradiated and irradiated cells was quite constant with a ratio of 0.72 mitosis at 2 gy per 1 mitosis at 0 gy and a correlation of 94% ( figure 3 )  . 
 discussion three - color fish offers the possibility to evaluate most of the chromosomal aberrations occurring in the painted chromosomes [ 8 , 10 , 13 , 17 , 20 , 21 , 33 ]  . 
therefore , it enables us to judge the predictive power of the different aberration types or scores , and it allows a comparison of aberrations commonly identified using fish with those types found in conventional cytogenetics . 
a dose of 2 gy reduced the mitosis by 28% . however , there was an interindividual scattering including two of the sensitive patients , one having a reduced mitotic level and one having a highly elevated level . 
radiation - induced chromosomal aberrations of lymphocytes from eleven control persons ( control ) and five hypersensitive patients ( sensitive ) at 2 gy corrected for spontaneous aberration frequency at 0 gy . 
strahleninduzierte chromosomale aberrationen in lymphozyten bei elf kontrollpersonen ( control ) und fnf erhht strahlenempfindlichen patienten ( sensitive ) bei 2 gy , korrigiert um die spontane aberrationsfrequenz bei 0 gy . 
a significant value was reached to distinguish between hypersensitive patients and healthy individuals , which has already been proven [ 20 ]  . as the incidence of chromosomal rearrangements in nonirradiated peripheral blood cells is low , most ccrs have been induced by in vitro irradiation . 
similarly , ataxia - telangiectasia ( at ) patients , known to be associated with enhanced radiosensitivity , responded with a high frequency of ccrs after irradiation [ 19 ]  . 
therefore , we hypothesize that ccrs are a suitable marker for the identification of individual hypersensitivity . the frequent occurrence of ccrs in these individuals may particularly reflect the incompetence of the hypersensitive cell to handle dna damage including dna damage repair and post - repair processing . 
number of cells with n breaks per metaphase analyzed for five hypersensitive patients ( sensitive ) and eleven control persons ( healthy individuals ) by a dose of 2 gy . 
control persons ( * ) and hypersensitive patients ( ) are displayed including the region of the single standard deviation for healthy individuals ( area between lines ) and patients ( gray area )  . 
ccrs per metaphase in dependence on dicentrics per metaphase ( a ) , ccrs per metaphase in dependence on translocations per metaphase ( b ) , and translocations per metaphase in dependence on dicentrics per metaphase ( c )  . 
kontrollpersonen ( * ) und erhht strahlenempfindliche patienten ( ) sind mit der einfachen standardabweichung der kontrollen ( flche zwischen den linien ) und der patienten ( graues areal ) aufgetragen . 
since this metric parameter differs significantly between the two groups , it is understandable that this is a parameter frequently used for analyzing hypersensitive patients [ 17 , 19 , 20 , 31 ]  . 
although dicentric chromosomes are known as an excellent biomarker for acute radiation exposure [ 9 , 11 ] , fish , especially scoring translocations , seems to be superior to the analysis of dicentric chromosomes . 
since the blood analyzed in the study was freshly drawn from the patients and irradiated in vitro , neither the previous radiotherapy nor the chemotherapy could have been the reason for the broad scattering of excess acentric fragments . 
the radiation dose of 2 gy had been chosen for the study in order to compare in vitro with in vivo data , since a single dose of 2 gy is usually given in clinical radiotherapy regimens . 
a higher dose of 3 gy up to 6 gy will generate more excess acentric fragments and , therefore , may result in a better determination by excess fragments [ 3 , 4 , 25 ]  . 
 [ 3 , 4 ] scored excess acentric fragments in giemsa - stained preparations ( genomic yields ) , whereas in this work partial yields of painted chromosomes were scored . 
 other parameters other parameters analyzed in the study such as the yield of aberrant mitoses , the frequency of breaks per aberrant metaphase , and the open breaks display such a broad scattering that a clear distinction between the groups cannot safely be made . 
aberrant metaphases can only be used as additional information , since they seem to be not precise enough to differentiate between two groups . furthermore , the total number of aberrant metaphases displays a high interindividual variability and is not a distinctive indicator . 
open breaks are a relatively rare event using the g0 assay . one consideration was that the highly sensitive patients had a defect repair mechanis so , the incidence for open breaks would increase . 
best distinction between healthy individuals and hypersensitive patients can be achieved analyzing breaks per mitosis , translocations and complex aberrations , if a dose region equivalent to fractionated radiotherapy is used . these aberration types can only be detected by fish technique , and , therefore , a fish approach may be the best choice for detection of individual hypersensitivity toward ionizing irradiation . 
 strahlentherapie und onkologie originalarbeit einfluss einer properativen ( hyperthermen ) radiochemotherapie auf die manometrisch erfasste analsphinkterfunktion beim lokal fortgeschrittenen rektumkarzinom johannes fritzmann1 , michael hnerbein1 , wassilij slisow1 , johanna gellermann2 , peter wust2 , beate rau1 hintergrund und ziel : bei lokal fortgeschrittenen rektumkarzinomen ist die properative radiochemotherapie ( rct ) mit anschlieender kurativer chirurgie eine akzeptierte therapeutische option . 
alle patienten wurden mit 45 gy ( 5 ( cid : 1 ) 1 , 8 gy ) sowie zwei zyklen chemotherapie mit 5 - fluorouracil ( 5 - fu ) und leucovorin ( folinsure ) vorbehandelt . 
 ergebnisse : beim gesamtkollektiv aller 102 patienten kam es zu einer signifikanten reduktion des durchschnittlichen maximalen ruhedrucks von 97 auf 89 mmhg ( p = 0 , 02 )  . 
bei tief gelegenen tumoren ( 7 , 5 cm ab anokutanlinie [ acl ] ) fiel der maximale ruhedruck noch etwas deutlicher von 92 auf 79 mmhg ab ( p = 0 , 01 )  . 
 schlsselwrter : manometrie rektumkarzinom sphinkter strahlenther onkol 2004 ; 180 : 2818 doi 10.1007 / s00066 - 004 - 1173 - x influence of preoperative ( hyperthermic ) radiochemotherapy on manometric anal sphincter function in locally advanced rectal cancer background and purpose : preoperative radiochemotherapy ( rct ) followed by curative surgery is a well - accepted therapeutic option in the treatment of advanced rectal cancer . 
the aim of this study is to evaluate the influence of preoperative rct on anal sphincter function . patients and methods : between 1994 and 2000 , 102 patients with rectal cancer stage ut3 / ut4 were analyzed . 
all patients underwent radiotherapy with 45 gy ( 5 ( cid : 1 ) 1.8 gy ) including two cycles of 5 - fluorouracil ( 5 - fu ) / leucovorin ( folinic acid ) chemotherapy . 
verschiedene studien zeigten , dass speziell in dieser risikogruppe durch eine properative strahlentherapie eine verringerung des rezidivrisikos sowie eine verbesserung des gesamtberlebens erreicht werden knnen [ 17 , 18 , 23 , 26 , 27 ]  . 
dennoch kommt es bei fast allen patienten postoperativ zu einer beeintrchtigung der anorektalen funktion , die sich in erhhtem stuhldrang , erhhter stuhlfrequenz sowie inkontinenz uert [ 12 ]  . 
 der einfluss der properativen bestrahlung des beckens auf die anale sphinkterfunktion ist weitgehend unbekannt . die fixierte anatomische position des rektums im becken macht es empfindlicher gegen die effekte der bestrahlung . manche symptome lassen sich auf die begleitende proktitis sowie die vernderte rektumphysiologie ( endotheldefekt , fibroblastenproliferation der lamina propria etc . ) zurckfhren [ 16 , 27 , 28 , 30 ]  . 
ob die perkutane radiotherapie darber hinaus einen direkten einfluss auf die sphinkterfunktion hat , wurde bisher nur an wenigen studien mit geringer fallzahl evaluiert [ 1 , 4 , 29 , 31 ]  . 
 sphinktermanometrie nach der reinigung des rektums mittels klysma wurden die durchzugsmanometrie und vektorvolumenbestimmung mit dem pc - poligraf ( synectics gmbh , frankfurt / main ) in linksseitenlage der patienten durchgefhrt . 
daraus wurden die folgenden parameter extrahiert : sphinkterlnge , lnge der hochdruckzone ( lnge des sphinkteranteils , dessen druckwert > 50% des maximaldrucks liegt ) und maximaldruck ( ber basislinie ) [ 5 ]  . 
whrend des ersten zyklus erfolgte die chemotherapie mit leucovorin ( folinsure ; 50 mg ) und 5 - fluorouracil ( 5 - fu ; 300 mg / m2 )  . 
 die bestrahlung wurde in konformaler dreidimensional geplanter mehrfeldertechnik ( typischerweise drei felder ) mit einer zielvolumendosis von 5 ( cid : 1 ) 1 , 8 gy bis zu 45 gy ber einen zeitraum von 5 wochen durchgefhrt . 
auf der grundlage dieser klassifikation wurden die patienten entsprechend dem auftreten von nebenwirkungen in folgende zwei gruppen eingeteilt : gruppe 1 = patienten mit nebenwirkungen grad iii und gruppe 2 = patienten mit nebenwirkungen grad iiiiv . 
 zur ermittlung der ansprechrate des tumors auf die properative therapie wurden das stadium bei der initialen endosonographie ( ut ) mit dem histopathologischen stadium ( pt ) verglichen , der verlauf der tumorgre bestimmt und so zwischen kompletter remission ( cr ) , partieller remission ( pr ) , keiner vernderung ( nc ) und fortschreitender erkrankung ( pd ) unterschieden . 
 ergebnisse vergleich der manometriewerte des gesamtkollektivs beim vergleich der sphinktermanometrisch ermittelten maximalen ruhedruckwerte vor und nach properativer therapie zeigte sich fr das gesamte kollektiv von 102 patienten ein statistisch signifikanter abfall von durchschnittlich 97 38 ( 13199 ) auf 89 36 ( 24261 ) mmhg ( p = 0 , 02 )  . 
radiochemotherapie und sphinkterfunktion beim rektumkarzinom * p = 0 , 02 post post druck hier prtherapeutisch im mittel bei 99 mmhg ( 40 ) und posttherapeutisch bei 88 mmhg ( 37 )  . 
 pr post ruhewerte sphinkterlnge ( mm ) lnge der hochdruckzone ( mm ) maximaldruck ( mmhg ) lage des maximaldrucks ( mm ) kneifwerte sphinkterlnge ( mm ) lnge der hochdruckzone ( mm ) maximaldruck ( mmhg ) lage des maximaldrucks ( mm ) 39 15 17 8 97 38 17 9 40 17 17 8 89 36 18 9 50 20 19 9 178 71 21 11 51 24 18 8 176 67 22 11 0 , 02 n ( % ) gesamt [ n ( % ) ] responder komplette remission ( cr ) partielle remission ( pr ) nonresponder unverndert ( nc ) fortschreiten ( pd ) 12 ( 12 ) 51 ( 50 ) 35 ( 34 ) 3 ( 3 ) 63 ( 62 ) 38 ( 38 ) tabelle 4 . 
besonderes augenmerk wurde auf patienten mit proktitis gelegt , bei denen sich kein statistisch signifikanter unterschied zwischen der gruppe mit leichten und jener mit schweren symptomen zeigte ( differenz ruhedruck : p = 0 , 4 , differenz kneifdruck : p = 0 , 7 )  . 
whrend es bei den hheren tumorlokalisationen lediglich zu einem abfall des ruhedrucks von durchschnittlich 102 38 auf 100 41 mmhg kam ( p = 0 , 5 ) , zeigte sich bei den 7 , 5 cm gelegenen tumoren eine statistisch relevante reduktion von 92 37 auf 79 26 mmhg ( p = 0 , 01 ; abbildung 2 )  . 
 die betrachtung des remissionsausmaes in abhngigkeit von der tumorlokalisation ergab eine hhere ansprechrate fr die tiefer gelegenen tumoren ( 83% ) im gegensatz zu den hher gelegenen tumoren mit nur 41% respondern ( abbildung 3 )  . 
 hyperthermie bei einer zustzlichen behandlung mit regionaler hyperthermie zeigt sich bei den 46 patienten ( 45% ) mit hyperthermie eine grenzwertig signifikante verminderung des maximalen ruhedrucks von 105 40 auf 93 40 mmhg ( p = 0 , 05 )  . 
bei den 56 patienten ( 55% ) ohne hyperthermie in der vorbehandlung sank dieser von 91 35 auf 86 31 mmhg ( p = 0 , 3 )  . beim maximalen kneifdruck zeigt sich keine verminderung durch die vorbehandlung mit hyperthermie . 
hierbei lie sich kein strkerer abfall der drcke in der patientengruppe mit ausgeprgter proktitis nachweisen , so dass davon auszugehen ist , dass die akute radiogene proktitis nicht den entscheidenden einfluss auf den abfall der sphinkterdrcke hat . 
 te weder fr das gesamte patientenkollektiv ( p = 0 , 7 ) noch fr die mit einer hheren ansprechrate vergesellschafteten tiefen tumoren ( p = 0 , 5 ) nachgewiesen werden . 
 alter bei einem durchschnittsalter von 58 , 4 jahren ( 3074 ) korreliert der maximale ruhedruck sowohl vor als auch nach properativer rct mit einer signifikanz von p = 0 , 02 mit dem alter des patienten . 
in mehreren studien haben sich sowohl eine erhhte rate an r0 - resektionen [ 6 ] und folglich eine verringerung des lokalrezidivrisikos als auch ein verbessertes gesamtberleben gezeigt [ 26 ]  . 
gerade im anorektalen bereich wurden daher nach bestrahlung von rektumkarzinomen eine beeintrchtigung der sphinkterfunktion mit konsekutiver stuhlinkontinenz und erhhter stuhlfrequenz [ 7 , 12 , 13 , 29 ] sowie weitere nicht unerhebliche begleiterscheinungen beschrieben . 
zur einschtzung des einflusses der bestrahlung im vergleich zum operativen vorgehen auf die analsphinkterfunktion sind weitere untersuchungen nach operativer therapie notwendig . zur beurteilung der sphinkterfunktion ist die sphinktermanometrie eine valide methode [ 14 , 15 ]  . 
 bei den in unsere studie eingeschlossenen 102 patienten , die alle einer perkutanen bestrahlung von 45 gy unterzogen wurden , zeigte sich lediglich ein signifikanter unterschied bei der messung des maximalen ruhetonus , was auf einen verminderten tonus des m . 
in der von uns untersuchten patientengruppe fiel gerade der deutliche abfall ( von 92 auf 79 mmhg ) des maximalen ruhedrucks bei 53 patienten mit einem tumor 7 , 5 cm ab acl auf ( p = 0 , 01 )  . oberhalb 7 , 5 cm konnte eine solche differenz nicht aufgezeigt werden . 
man beachte , dass bei den nonrespondern schon initial ein herabgesetzter sphinktertonus besteht ( pr , tabelle 6 ) , also durch die therapie keine weitere verschlechterung ( eher eine verbesserung ) entsteht . 
 beim vergleich der maximalen kneifdrcke stimmen unsere ergebnisse mit denen der vorgenannten studien berein , in denen es zu keiner signifikanten reduktion gekommen ist . dies steht im gegensatz zu einer studie von kim et al . , die 24 patientinnen mit unterschiedlich schwerer proktitis nach bestrahlung mit 45 gy bei zervixkarzinom mit einer kontrollgruppe verglichen [ 13 ]  . 
in unserer wie auch in anderen studien [ 4 ] lie sich eine signifikante vernderung der hochdruckzone und damit der sphinkterlnge nicht nachweisen . allerdings sind diese ergebnisse kritisch zu bewerten , da sie bei der durchzugsmanometrie im gegensatz zu den absoluten druckwerten von der durchzugsgeschwindigkeit und somit vom untersucher abhngig sind . 
beim vergleich der patientengruppe mit hyperthermie mit der gruppe ohne hyperthermie war in unseren daten kein unterschied bezglich der postoperativen sphinkterfunktion darstellbar . angesichts der vergleichbarkeit unserer ergebnisse mit denen , die sich auf eine alleinige strahlentherapie sttzten , ist davon auszugehen , dass der entscheidende , die sphinkterfunktion beeinflussende faktor die strahlentherapie ist . 
auch die ( scheinbare ) korrelation von akuten nebenwirkungen und sphinkterbeeintrchtigung ( tabelle 4 ) erweist sich als indirekter effekt , da die tief sitzenden rektumkarzinome mit weniger dnndarmanteilen bestrahlt werden knnen , was mit weniger akuttoxizitt verbunden ist . 
 inwieweit dies von einem noch bestehenden schleimhautdem abhngt und welchen einfluss die sphinktererhaltende operation auf eine weitere schdigung des sphinkterapparates mit nachfolgender anorektaler funktionsstrung hat , mssen weitere untersuchungen der sphinkterfunktion nach abschluss der tumorspezifischen therapie zeigen . 
beate rau klinik fr chirurgie und chirurgische onkologie robert - rssle - klinik am mdc universittsklinikum charit , campus berlin - buch humboldt - universitt zu berlin lindenberger weg 80 13125 berlin deutschland telefon ( + 49 / 30 ) 9417 - 1425 , fax - 1404 e - mail : rau@rrk - berlin.de strahlenther onkol 2004 no . 
5 urban & vogel strahlentherapie und onkologie original article prognostic factors for brain metastases after whole brain radiotherapy data from a single institution * katharina fleckenstein1 * * , holger hof2 * * , frank lohr1 , frederik wenz1 , michael wannenmacher2 purpose : prognostic factors for overall survival of patients treated for brain metastases with whole brain radiotherapy ( wbrt ) at a single institution were retrospectively evaluated , and the validity of the rtog recursive partitioning analysis ( rpa ) for prognostic classes was assessed . patients and methods : the data of all patients ( n = 268 ) with brain metastases from solid tumors homogeneously treated between 01 / 1997 and 09 / 1999 at the university of heidelberg , germany , with wbrt without surgery or radiosurgery were reviewed . 13 different patientand therapy - related variables were evaluated for prognosis . 
 key words : brain metastases whole brain irradiation prognostic factors rpa class strahlenther onkol 2004 ; 180 : 26873 doi 10.1007 / s00066 - 004 - 1234 - 1 prognostische faktoren bei patienten mit zerebralen metastasen nach ganzhirnbestrahlung . 
daten einer einzelnen institution ziel : es wurden prognosefaktoren fr patienten mit hirnmetastasen , die an einer einzelnen institution mit einer ganzhirnbestrahlung ( wbrt ) behandelt wurden , retrospektiv ausgewertet . 
gleichzeitig wurde die gltigkeit der prognoseeinteilung der rtog auf der basis der rekursiven partitionsanalyse ( rpa ) fr dieses patientenkollektiv berpr patienten und methodik : die daten aller patienten mit hirnmetastasen solider malignome ( n = 268 ) , die zwischen 01 / 1997 und 09 / 1999 mit einer wbrt ohne resektion oder radiochirurgie am universittsklinikum heidelberg behandelt worden waren , wurden ausgewertet . 
in case of multiple brain metastases , whole brain radiotherapy ( wbrt ) is of special importance , since surgery or stereotactic radiotherapy is usually limited to a small number of lesions and most chemotherapy protocols are not effective in treating intracerebral malignant tumors . 
aiming at palliation , wbrt is the most effective tool for delaying intracerebral progression and for reducing neurologic symptoms [ 4 ]  . also , wbrt shows no significant effect on cognitive function [ 22 ]  . 
however , despite numerous studies designed to improve treatment outcome , median survival rates continue to be within a range of 36 months [ 2 , 3 , 5 , 13 , 15 , 17 , 23 , 25 ]  . 
due to the high incidence and morbidity of brain metastases , the aim of this retrospective observational study was to evaluate prognostic factors for survival in patients treated at a single institution with wbrt for brain metastases without surgery or radiosurgery and no further salvage therapy and to possibly identify long - term survivors . 
second , we assessed the validity of the recursive partitioning analysis ( rpa ) prognostic classes , which have been described by the radiation therapy oncology group ( rtog ) in 1997 [ 7 ] ( class i : karnofsky performance status [ kps ] 70% , age < 65 years , no extracranial metastases , controlled primary tumor ; class iii : kps < 70% ; class ii : others )  . 
 patients and methods patients with two or more brain metastases or a solitary brain metastasis and an underlying primary implying more occult cerebral metastases ( like breast cancer or small - cell lung cancer ) received wbrt instead of radiosurgery . 
for this analysis , only the records of patients ( n = 268 ) who underwent wbrt without surgery or radiosurgery and no further salvage therapy at the department of radiation oncology , university of heidelberg , gremany , between january 1997 and september 1999 were reviewed . 
200 patients ( 86% ) received a total dose between 3040 gy , and in 225 patients ( 97.8% ) fraction doses of 2 or 3 gy were administered , respectively . 
additionally , a grouping of the study population was performed according to the rpa prognostic classes , which have been described by the rtog in 1997 [ 7 ]  . 
prognostic factors for brain metastases in that same group , 69% had a controlled primary as opposed to only 42% in the total population . the total dose applied and the single dose per fraction were significant prognostic factors in univariate analysis ( p < 0.0001 ) , but could not be confirmed on multivariate analysis , if table 1 . 
remarkably , almost all patients surviving 1 year belonged to the group with only one or two brain metastases . on univariate analysis , the spatial extension of metastases within the brain had a significant effect on survival ( p = 0.0006 ) , if patients with supraor infratentorial manifestation only were compared to those with both - sided lesions . 
as to patients surviving 1 year , 18 had lung cancer , 13 breast cancer , four renal cancer , two malignant melanoma , and seven other cancers ( table 2 )  . 
neither did the size of brain metastases ( measuring the most extended one ) , although the majority of patients surviving 1 year had brain metastases < 2 cm in size . 
 on multivariate analysis , however , only a kps 70% , control of the primary tumor and no extracranial metastases were independent prognostic factors for overall survival ( table 3 )  . 
patients in rpa class ii had a median survival of 4.2 months ( n = 55 ) , and in rpa class iii , median survival was 1.8 months ( n = 28 )  . 
 primary tumor lung cancer breast cancer cancer of the kidney malignant melanoma other patients a two - sided significance probability for the log rank test b variable measured before start of whole brain radiotherapy a proportion of patients surviving 1 year according to primary tumor strahlenther onkol 2004 no . 
 since common practice for treating brain metastases varies from 10 ( cid : 1 ) 3 gy to 20 ( cid : 1 ) 2 gy , we tried to evaluate the influence of different fractionation regimens on a patients survival . 
neurologic symptom - free survival might have been a better endpoint but could not sufficiently be evaluated retrospectively . the optimal dose fractionation schedules for patients with brain metastases have been evaluated in several randomized trials [ 3 , 9 , 10 , 17 ]  . 
in general , patients treated over the shortest period of time and with larger fractions responded more quickly , but the duration of clinical response and time to progression were similar in various dose fractionation schedules . 
actuarial survival according to the recursive partioning analysis ( rpa ) class ( rpa class i : n = 9 , rpa class ii : n = 117 , rpa class iii : n = 46 ) ; + censored data . 
aktuarische darstellung der berlebenskurven in abhngigkeit von der rpaklasse ( rekursive partitionsanalyse ; rpa - klasse i : n = 9 , rpa - klasse ii : n = 117 , rpa - klasse iii : n = 46 ) ; + zensierte daten . 
some studies also indicate that patients with brain metastases , with breast as the primary site , have a better chance of survival than those with lung as the primary [ 2 , 3 , 5 , 7 , 8 , 10 , 12 ]  . 
 the median survival of the studied patient cohort ( 3.8 months ) was within the range of other previously published data [ 2 , 3 , 5 , 13 , 15 , 17 , 23 ]  . 
the median survival times for rpa class iii and ii are comparable to those published earlier [ 6 , 7 , 15 , 16 , 18 , 19 ]  . 
for rpa class i , survival seems slightly higher in the present study , but only 5% fell into the most favorable group , rpa class i ( 68% fell into class ii and 27% into class iii )  . 
 [ 18 ] question the predictability of the rpa classification for patients with four or more brain metastases , we grouped a selected subset of our total patient population , patients with four or more brain metastases , into the rpa classes . 
 therefore , it is necessary to validate the rpa classes on several populations to obtain a better understanding of the robustness of this syste whole population 19.1 conclusion based on the retrospective analysis of 232 out of 268 consecutive patients homogeneously treated at a single institution , one may conclude that : 1 . 
 strahlentherapie und onkologie original article pentoxifylline enhances tumor oxygenation and radiosensitivity in rat rhabdomyosarcomas during continuous hyperfractionated irradiation friedrich zywietz1 , lothar bhm2 , christoph sagowski3 , wolfgang kehrl3 purpose : to examine the influence of the hemorrheologic agent pentoxifylline ( ptx ) on tumor oxygenation and radiosensitivity . material and methods : tumor oxygenation in rat rhabdomyosarcomas r1h after ptx administration ( 50 mg / kg body weight ) was measured using interstitial po2 probes ( licox cmp system and eppendorf po2 - histograph )  . 
tumors were irradiated with 60co ( cid : 1 ) irradiation using single doses ( 15 and 30 gy ) , conventional fractionation ( 60 gy / 30 fractions / 6 weeks ) , and continuous hyperfractionation ( 54 gy / 36 fractions / 18 days ) in combination with ptx or an equivalent volume of physiological saline . 
however , in continuous hyperfractionated irradiation with 18 ( cid : 2 ) 50 mg / kg of ptx , the dmf with respect to tumor growth delay was found to be 1.37. 
 key words : pentoxifylline tumor oxygenation radiotherapy rat rhabdomyosarcoma strahlenther onkol 2004 ; 180 : 30614 doi 10.1007 / s00066 - 004 - 1198 - 1 pentoxifyllin stimuliert die tumoroxygenierung und strahlensensibilitt von rhabdomyosarkomen der ratte whrend kontinuierlicher hyperfraktionierter bestrahlung ziel : der einfluss der hmorrheologisch aktiven substanz pentoxifyllin ( ptx ) wurde in hinblick auf die tumoroxygenierung und strahlensensibilitt untersucht . 
 material und methodik : in rhabdomyosarkomen r1h der ratte wurde die tumoroxygenierung nach ptx - applikation ( 50 mg / kg krpergewicht ) mit invasiven po2 - sonden ( licox - cmp - system und eppendorf - po2 - histograph ) gemessen . 
tumoren wurden mit einzeldosen ( 15 und 30 gy ) , konventioneller fraktionierung ( 60 gy / 30 fraktionen / 6 wochen ) und kontinuierlicher hyperfraktionierung ( 54 gy / 36 fraktionen / 18 tage ) in kombination mit ptx oder quivalenten volumina physiologischer kochsalzlsung bestrahlt . 
einzeldosen von 15 und 30 gy in kombination mit ptx erhhten die strahlensensibilitt des r1h - tumors nur gering und ergaben dosismodifizierende faktoren ( dmf ) von 1 , 11 bzw . 
eine kontinuierliche hyperfraktionierte bestrahlung mit 18 ( cid : 2 ) 50 mg / kg ptx ergab jedoch einen dmf von 1 , 37 in bezug auf den tumor growth delay . in der lokalen tumorkontrolle gab es keine unterschiede . 
 1 institute for biophysics and radiobiology , university hospital hamburg - eppendorf , hamburg , germany , 2 department of pharmacology , university of stellenbosch , tygerberg , south africa , 3 department of oto - rhino - laryngology , university hospital hamburg - eppendorf , hamburg , germany . 
 schlsselwrter : pentoxifyllin tumoroxygenierung bestrahlung rhabdomyosarkom der ratte introduction the chaotic tumor vascular network and a chaotic tumor blood supply are generally recognized as major factors in the poor response of hypoxic tumors to irradiation [ 2 , 9 , 14 , 17 , 30 , 31 , 42 , 44 ]  . 
the methylxanthine derivative 3 , 7 - dimethyl - 1 - ( 5 - oxohexyl ) xanthine , known as pentoxifylline ( ptx ) , is a promising drug , since it increases the deformability of red cells , prevents platelet aggregation and reduces blood viscosity [ 11 , 35 ]  . 
the efficacy of the drug in improving tumor perfusion and tumor oxygenation [ 7 , 18 , 19 , 22 , 23 , 26 , 36 , 38 ] while showing minimal effect on other tissues is well documented [ 8 , 24 , 36 ]  . 
it has recently been reported that ptx has antimetastatic potential [ 1 , 16 ] and an inibitory effect on tumor angiogenesis , which is related to its antiproliferative action on endothelial cells [ 15 ]  . 
 studies on experimental tumors with single doses of radiation have shown that ptx , indeed , is capable of enhancing radiosensitivity [ 7 , 19 , 25 , 27 , 37 , 43 ]  . 
the objective of this study was to examine the effectiveness of ptx in a conventional fractionated radiotherapy and in continuous hyperfractionated irradiation using the rat rhabdomyosarcoma model and total doses of 60 and 54 gy , respectively . 
tumor volume ( vt ) was determined by measuring three orthogonal diameters a , b , and c and was calculated using an ellipsoid approximation : vt = / 6 ( a ( cid : 2 ) b ( cid : 2 ) c )  . 
dosemodifying factors ( dmfs ) were calculated as ratio of dose without to dose with ptx for the same level of 2vo assuming a linear relationship between tumor growth delay and radiation dose . 
the studies had been approved by the hamburg ministry of health ethics committee , and were conducted in accordance with the german law for animal protection and the united kingdom co - ordinating committee on cancer research guidelines . 
xylazine ( rompun , bayer , germany )  . the anesthetized animals breathing room air were placed prone on a small temperature - controlled irradiation table ( 37 c ) at a 60co radiotherapy facility ( gammatron 2 , siemens , germany )  . 
the radiation field size was 3 ( cid : 2 ) 3 cm2 and the dose rate 0.8 gy / mtumors were irradiated with 60 gy , given in 30 fractions of 2 gy , five times per week , for 6 weeks . 
hyperfractionated irradiation was continuously performed for 18 days up to a total dose of 54 gy , applied in 36 fractions , twice daily at a time interval of 6 h . 
 drug administration ptx ( 3 , 7 - dimethyl - 1 - [ 5 - oxohexyl ] xanthine ) was purchased as trental ( hoechst marion roussel , germany ) in 5 - ml ampoules of 20 mg . 
pentoxifylline : tumor oxygenation and radiation histography system ( eppendorf - netheler - hinz , hamburg , germany ) [ 33 ] and the licox cmp - system ( gms , kielmielkendorf , germany )  . 
changes in oxygenation were recorded for 80 m the eppendorf - po2 - histography system was used to measure the distribution of the oxygen partial pressure in the tumor as described previously [ 33 ]  . 
since tumor po2 depends on arterial oxygenation [ 33 ] , tumor po2 measurements were taken only when the oxygen partial pressure of the femoral artery was in the range of 115 12 mmhg as assessed by arterial blood gas analysis ( chiron blood gas analyzer 248 , bayer vital , germany )  . 
from the pooled po2 histograms the following parameters were derived : mean and median tumor po2 , the relative frequency of po2 values falling into the two lowest classes ( 05.0 mmhg ) , a parameter for tumor hypoxia . 
negative po2 values were excluded from the calculation using the eppendorf po2 read progra statistical analysis of the data was by the mann - whitney test ( u - test ) and the commercially available program spss for windows 11.0. 
 cell survival assays rhabdomyosarcoma r1h cells were grown in rpmi medium with 10% fbs 2 g / l l - glutamine , 100 u / l penicillin and 100 g / ml streptomycin in 75 - cm2 flasks incubated at 37 c in 95% o2 / 5% co2 . 
ptx at 2 mm was added immediately before irradiation at doses of 0 , 1 , 2 , 4 , 6 , 8 , and 10 gy and removed 1 h after irradiation . 
of ptx as measured with the licox systeit is apparent that ptx injection results in a gradual improvement of tumor po2 which rises from 21 ( t = 0 ) to 37 mmhg 60 min after drug administration ( channel 2 )  . 
this indicates that intraperitoneal application of ptx selectively improves tumor oxygenation . since the licox system measures the tumor oxygenation at a channel 1 : rat subcutis channel 2 : tumor r1h figure 1 . 
continuous monitoring of oxygenation in r1h rhabdomyosarcoma ( channel 2 ) and in the subcutis ( channel 1 ) of the rat after intraperitoneal injection of 50 mg / kg body weight pentoxifylline ( ptx ) using the licox cmp syste abbildung 1 . 
kontinuierliche registrierung der oxygenierung im rhabdomyosarkom r1h ( kanal 2 ) und in der subkutis ( kanal 1 ) der ratte nach intraperitonealer injektion von 50 mg / kg krpergewicht pentoxifyllin ( ptx ) , gemessen mit dem licox - cmp - syste strahlenther onkol 2004 no . 
pentoxifylline : tumor oxygenation and radiation single location in traumatized tumor tissue , we used the eppendorf system to determine the oxygen distribution in the whole tumor in 15 - min intervals . 
tumor oxygenation ( po2 ) and frequency of po2 values < 5 mmhg in rat r1h rhabdomyosarcomas after intraperitoneal injection of pentoxifylline ( 50 mg / kg body weight ) measured with the eppendorf - po2 - histograph . 
tumoroxygenierung ( po2 ) und hufigkeit der po2 - werte < 5 mmhg in rhabdomyosarkomen r1h der ratte nach intraperitonealer injektion von pentoxifyllin ( 50 mg / kg krpergewicht ) , gemessen mit dem eppendorf - po2 - histographen . 
relative changes in median tumor po2 and in the frequency of po2 values < 5 mmhg after intraperitoneal injection of 50 mg / kg body weight pentoxifylline measured by eppendorf po2 - histography . the corresponding arterial oxygen tensions ( pao2 ) which apply to the tumor po2 measurements are given on top of the figure . 
relative nderungen im medianen tumor - po2 und in der hufigkeit der po2 - werte < 5 mmhg nach intraperitonealer injektion von 50 mg / kg krpergewicht pentoxifyllin , gemessen mit dem eppendorf - po2 - histographen . 
the relative changes in median tumor oxygenation , in the frequency of po2 values < 5 mmhg , and the corresponding arterial blood ( pao2 ) are given in figure 2 . 
administration of 50 mg / kg of ptx ( i.p. ) was also associated with a rapid decrease of the initial mean arterial blood pressure ( mabp ) from 102 15 mmhg ( sd ) to 82 14 mmhg within 34 min and was followed by a full recovery to initial values 812 min later ( n = 10 )  . 
administration of 1 ( cid : 2 ) 50 mg / kg or 5 ( cid : 2 ) 50 mg / kg / 5 days of ptx alone had no influence on tumor growth as compared to untreated controls . 
the individual tumor growth curves demonstrated that the rate of tumor partial remission ( > 50% vo ) was 77% in the ptx - treated animals as compared to saline controls where it amounted to 50% . 
pentoxifylline : tumor oxygenation and radiation rate of tumor partial remissions indicate that ptx induces an enhancement of radiosensitivity of r1h tumors in a fractionated radiation treatment with radiotherapeutically relevant dose fractions . 
relative changes of tumor volume after irradiation with single doses of 15 and 30 gy in combination with pentoxifylline ( ptx : 50 mg / kg body weight ) or an equivalent volume of saline ( nacl ) in comparison to untreated controls . 
relative nderungen des tumorvolumens nach bestrahlung mit einzeldosen von 15 und 30 gy in kombination mit pentoxifyllin ( ptx : 50 mg / kg krpergewicht ) oder einem quivalenten volumen physiologischer kochsalzlsung ( nacl ) im vergleich zu unbehandelten kontrollen . 
relative changes of tumor volume after 60 gy given in 30 fractions over 6 weeks ( conventional fractionation ) in combination with 30 ( cid : 2 ) 50 mg / kg body weight of pentoxifylline ( ptx ) or with saline controls ( nacl : 30 equivalent volumes of ptx )  . 
relative nderungen des tumorvolumens nach 60 gy , 30 fraktionen in 6 wochen ( konventionelle fraktionierung ) , in kombination mit 30 ( cid : 2 ) 50 mg / kg krpergewicht pentoxifyllin ( ptx ) oder mit kochsalzlsung ( nacl : 30 quivalente volumina von ptx )  . 
 ( mittelwerte sem , n = 8 . ) in previous studies on r1h tumors , we have shown that tumor capillaries are progressively damaged during fractionated irradiation [ 45 ] ; especially after a total dose of 45 gy , a significant decrease in tumor oxygenation [ 46 ] and in the bioenergetic status of the tumors occurs [ 41 ]  . 
 in conventional or hyperfractionated irradiation , we noticed that ptx had an influence on body weight of the rats . animals of 312 13 g given conventional irradiation and ptx showed a lower weight gain as compared to animals in the saline group ( figure 6a )  . 
it is also interesting to note that the first 2 weeks of hyperfractionation induced an 8% loss in body weight , but this was followed by a rapid increase in subsequent weeks . 
total doses of 1 , 500 mg / kg ptx applied over 6 weeks in conventional irradiation and of 900 mg / kg given within 18 days for hyperfractionation were well tolerated . 
from these survival data it must be concluded that presence of ptx of 118 h post irradiation has no significant influence on radiotoxicity in the 0to 10 - gy treatment t = 6h r1h tumor nacl 54 gy / 36f / 18 d plus pentoxifylline ( ( cid : 127 ) ) plus nacl ( o ) sem 100 120 days after start of irradiation figure 5 . 
tumor volume curves of r1h rhabdomyosarcomas after continuous hyperfractionated irradiation ( 54 gy / 36 fractions / 18 days ) in combination with pentoxifylline ( ptx : 18 ( cid : 2 ) 50 mg / kg body weight ) or equivalent volumes of saline ( nacl : 18 equivalent volumes of ptx ) administered 45 min before the first daily irradiation . 
tumorvolumenkurven von rhabdomyosarkomen r1h nach kontinuierlicher hyperfraktionierter bestrahlung ( 54 gy / 36 fraktionen / 18 tage ) in kombination mit pentoxifyllin ( ptx : 18 ( cid : 2 ) 50 mg / kg krpergewicht ) oder quivalenten volumina kochsalzlsung ( nacl : 18 quivalente volumina von ptx ) , injiziert vor der ersten tglichen bestrahlung . 
tumor oxygenation ( po2 ) and frequency of po2 values < 5 mmhg in rat r1h rhabdomyosarcomas during a continuous hyperfractionated irradiation with 54 gy , given in 36 fractions for 18 days , in combination with 18 fractions of pentoxifylline ( ptx : 18 ( cid : 2 ) 50 mg / kg body weight ) or 18 equivalent volumes of saline ( nacl )  . 
tumoroxygenierung ( po2 ) und hufigkeit der po2 - werte < 5 mmhg in rhabdomyosarkomen r1h der ratte whrend einer kontinuierlichen hyperfraktionierten bestrahlung mit 54 gy , gegeben in 36 fraktionen in 18 tagen , in kombination mit 18 fraktionen pentoxifyllin ( ptx : 18 ( cid : 2 ) 50 mg / kg krpergewicht ) bzw . 
dna histograms recorded for r1h cells after exposure to a dose of 7 gy indicated a pronounced g1 block and a stable g1 / g2 peak ratio of 1.3 at 10 h post irradiation and reentry of cells into cycle at 3440 h post irradiation ( not shown )  . 
relative changes in body weight of male wag / rijh rats after conventional irradiation ( a ) or continuous hyperfractionated irradiation ( b ) in combination with pentoxifylline ( ptx ) or equivalent volumes of saline ( nacl )  . 
relative nderungen des krpergewichts von mnnlichen wag / rijh - ratten nach konventioneller bestrahlung ( a ) oder kontinuierlicher hyperfraktionierter bestrahlung ( b ) in kombination mit pentoxifyllin ( ptx ) bzw . 
 ( cid : 2 ) r1h und ptx , vor der bestrahlung gegeben und 18 h nach der bestrahlung entfernt . controls before and removed 1 h later before and removed 18 h later dose ( gy ) with the expression of a g1 block after irradiation ( not shown )  . 
mouse fsaii tumors exhibit increased blood flow 1090 min after administration of 100 mg / kg ptx [ 26 ] , while rif - 1 mouse tumors seem to be much more sensitive and only require 20 mg of ptx / kg to produce a maximum tumor po2 and minimum of tumor hypoxia only 15 min after drug application [ 18 ]  . 
ds sarcomas of sprague - dawley rats have been found to show a continuous increase of tumor oxygenation after 50 mg ptx / kg up to 45 min [ 22 ]  . 
the r1h rhabdomyosarcoma is a subline of the ba1112 tumor , and our eppendorf po2 measurements also show the 15 - min lag period ( figure 2 ) and maximum of tumor oxygenation 45 min after ptx injection . 
we also observed that the ptx - induced increase of tumor oxygenation depends upon tumor size in that larger r1h tumors ( vo > 3 cm3 ) show less oxygenation . 
pentoxifylline : tumor oxygenation and radiation using two different po2 methods we found that ptx improves tumor oxygenation in r1h tumors and that the drug acts as an effective radiosensitizer . 
it is possible that the necrotic fraction in the tumor size chosen here is still rather large and that the disappointing statistical outcome is due to this proble radiosensitization by pentoxifylline changes in tumor volume after irradiation with single doses of 15 and 30 gy in the presence of ptx produced rather modest dmfs in the range of 1.041.11 ( figure 3 ) , which did not improve when a total dose of 60 gy was given in 30 fractions for 6 weeks ( figure 4 )  . 
while it is clear that the 45 - min time delay between ptx injection and irradiation is optimal from the oxygenation point of view ( figure 2 ) , it is rather surprising that the enhancement in tumor growth delay remains rather small . 
it is possible that in the single - dose experiments , the positive effect of ptx on tumor oxygenation may be lost by the relatively long times of irradiation ( 15 gy : 18.8 min , 30 gy : 37.5 min ) with regard to the pharmacokinetics of tumor oxygenation after ptx application and , in part , by the effects of anesthesia ( figure 2 )  . 
we have previously demonstrated that fractionated irradiation produces progressive damage of tumor capillaries , especially a total dose > 45 gy induces severe and irreversible vascular damages and a substantial increase of tumor hypoxia [ 45 , 46 ]  . 
the fact that local tumor control 180 days post irradiation is nearly identical to the nacl controls may be attributed to the growth kinetics of the tumor which compensates for the initial cell loss at the end of irradiation . 
a similar decline and disappearance of the initial benefit of ptx to tumor growth in the late post - irradiation period have also been observed in rhabdomyosarcomas grown in mice [ 43 ]  . 
it is clear that a higher tumor growth delay occurred after continuous hyperfractionated irradiation and under conditions , where the hypoxic fraction ( frequency of po2 values < 5 mmhg ) is considerably reduced ( table 2 )  . 
 effects of pentoxifylline on tumor parenchyma it is known that ptx is an effective g2 block abrogator [ 28 , 34 , 39 , 40 ] , which promotes early mitosis [ 4 , 5 , 40 ] thereby restricting the time of repair [ 10 , 20 , 32 ] and repair in general [ 6 , 39 ]  . 
we calculated that the ptx dose of 50 mg / kg would give rise to 5 mm ptx in a 250 - g rat which is well in the effective range for g2 abrogation . 
experiments on p53 wildtype and p53 mutant cell pairs in squamous carcinoma and melanoma lines [ 4 , 39 ] and mcf7 cells [ 13 ] have shown that only p53 mutant cells undergo radiosensitization . 
for these reasons it appears that the enhanced cell kill seen in the presence of ptx in animal tumors is not due to abrogation of cell cycle check points and shortened repair time . 
a repair effect has been noted in a human glioma model using p53 mutant t98g cells , where the long interfraction spacing generates conditions for ptx to diminish repair [ 12 ]  . 
 strahlentherapie und onkologie original article thta - cream versus bepanthol lotion in breast cancer patients under radiotherapy a new prophylactic agent in skin care ? barbara rper , danielle kaisig , florian auer , ertan mergen , michael molls1 background and purpose : in radiotherapy of the breast following breast - conserving surgery , the adverse reaction predominantly found is confined to the skafter phase ii studies , thta - cream , containing cm glucan , hydroxyprolisilan c und matrixyl as active substances , was said to have prophylactic properties of preventing acute radiation side effects in skin tissue . 
at 0 , 30 , and 50 gy , acute skin toxicity was scored with a modified rtog scoring systethe patients content with the skin care and the technical assistants content with the skin marks were recorded . 
mild itchiness and sporadic efflorescences were more frequently seen with thta - cream . according to a ranking of anonymized breast photos at 50 gy by independent investigators , side effects were equal . 
 key words : skin care thermoluminescent dosimetry radiation injuries breast cancer randomized controlled trials strahlenther onkol 2004 ; 180 : 31522 doi 10.1007 / s00066 - 004 - 1174 - 9 thta - creme versus bepanthol - lotion bei brustkrebspatientinnen whrend strahlentherapie . 
 ein neues prophylaktisches mittel zur verhinderung akuter hautreaktionen ? hintergrund und ziel : bei insgesamt guter vertrglichkeit der postoperativen strahlentherapie an der brust stehen hautreaktionen im vordergrund der akuten nebenwirkungen . 
 schlsselwrter : hautpflege thermolumineszenzdosimetrie strahlentherapie akute nebenwirkungen mammakarzinom randomisierte studien introduction breast cancer is the most common type of cancer in women , which approximately every tenth woman will experience in her lifetime . 
according to epidemiologic studies , management is dominated by breast - conserving surgery in 8085% of patients treated in german tumor centers [ 7 ] , of which 90% will eventually receive radiotherapy [ 20 ]  . 
irradiation of the breast is generally well tolerated , but side effects of the skin are a common proble skin reaction to radiation is a well - known phenomenon . as early as 1924 miescher accurately described the course of radiation - induced skin erythema [ 19 ] , and its use for dosimetric purposes was widespread . 
with the development of linear accelerators and high - voltage photon beams , the skin surface dose could be significantly reduced , but not eliminated . namely in breast cancer and cancer of the head and neck , radiation - induced skin reactions still play a major role . 
in order to improve the therapeutic ratio , the search for agents with prophylactic properties to prevent acute radiation dermatitis is going on [ 4 , 8 , 10 , 11 , 1518 , 21 , 25 , 31 , 35 ]  . 
 recently , french scientists have presented their development of thta - cream ( theracosm gmbh , germany ) , a new formulation containing three active substances that are believed to influence radiation dermatitis . 
according to the product information , cm glucan is a biological response modifier , promoting phagocytosis of macrophages and production of cytolytic / cytostatic factors reducing oxidative stress ; hydroxyprolisilan c is said to help in the rearrangement of lipids and collagen fibers decreasing the skins sensitivity to free radicals , and matrixyl should stimulate the synthesis of collagen i , iii and iv , thus participating in the skins regenerative process . 
in phase ii studies , thta - cream was shown to be feasible in the prophylactic approach in breast cancer patients under radiotherapy , but randomized controlled studies are missing so far . 
 according to surveys in germany [ 38 ] and the united kingdom [ 14 ] , there is no consensus about best supportive skin care , as at least 15 different agents were in use for prophylactic and more than 50 for therapeutic purposes . 
after having forbidden to wash the irradiated skin for many decades , attitude has changed recently [ 37 ] , when skin washing was found to be of no harm [ 34 ] or even favorable in randomized studies [ 5 , 26 ]  . 
 considering hints of a beneficial effect on desquamation in the literature [ 16 , 30 ] , we chose a dexpanthenol - containing product for the control group : bepanthol lotion is an oil - inwater emulsion containing dexpanthenol , the alcohol derivate of panthothenic acid which is a component of coenzyme a . 
 study plan according to the chronological order of presenting for radiation treatment planning , patients were alternately assigned into two groups without further stratification , receiving either thta - cream ( arm a , n = 10 ) or bepanthol lotion ( arm b , n = 10 )  . 
patients were requested to wash the irradiated skin gently with due attention to skin marks ( water - resistant edding marks , covered by transparent tapes ) ; no other prophylactic topical treatment was allowed . skin care was in accordance with german recommendations [ 36 ]  . 
 factors that might affect acute skin toxicity in breast cancer patients [ 9 , 24 ] like age , tumor stage , chemotherapy , hormonal therapy , smoking , skin type , weight , breast size , and irradiated volume were recorded . 
bepanthol lotion for skin care in breast cancer under radiotherapy radiotherapy was delivered in supine position with 6mev photons of a linear accelerator with tangential half - beam fields and wedge filters according to an individual ct - based helax treatment plan . 
all patients had thermoluminescent dosimeter ( tld ) measurements of the actual dose delivered to the skin surface once during their radiotherapy series , in two thirds of the patients reproducibility was checked with a second set of measurements . 
tlds were fixed on the skin with a light tape in three locations : ( i ) in the upper inner quadrant ( uiq ) , ( ii ) in the upper outer quadrant ( uoq ) , and ( iii ) in the midline between lower quadrants ( submammary fold , mlq ) , each 2 cm away from the closer field borders ( see figure 1 )  . 
for assessment of acute skin toxicity , the rtog scoring system was modified to allow for further discrimination of low scores : five different aspects of skin toxicity were scored separately with 03 points ( see table 1 )  . 
tldmlq : 2 cm above the lower field border in midline between the lower quadrants ; tlduiq : 2 cm below the upper field border and 2 cm lateral from the medial field border ; tlduoq : 2 cm below the upper field border and 2 cm medial from the lateral field border . 
tldmlq : 2 cm kranial der unteren feldgrenze mittig zwischen den unteren quadranten ; tlduiq : 2 cm kaudal der oberen und lateral der medialen feldgrenze ; tlduoq : 2 cm kaudal der oberen und medial der lateralen feldgrenze . 
mlq : midline between lower quadrants ; ms : maximal score of one aspect anywhere in the breast ; sum : sum score of the different aspects in a defined area ; ts : total score ; uiq : upper inner quadrant ; uoq : upper outer quadrant . 
mlq : mittig zwischen unteren quadranten ; ms : maximalscore eines aspekts an beliebiger lokalisation ; sum : summenscore der verschiedenen aspekte an einer definierten lokalisation ; ts : gesamtscore ; uiq : oberer innerer quadrant ; uoq : oberer uerer quadrant . 
after anonymization , the photos were ranked from highest to lowest overall skin toxicity by two independent investigators unaware of the skin care product in use . interobserver agreement was quantified with the help of a pearson correlation . 
groups were well balanced with respect to tumor stage , chemotherapy , smoking , skin type , breast size , and fractionation of radiotherapy ( see table 2 )  . 
there was no difference for maximal scores in every single aspect of skin toxicity for both groups at 30 gy ; the median erythema was faint , elevation of skin temperature between none and faint , and all other aspects none in both arms . 
 at 50 gy , both arms showed , as a median , a moderate erythema , a faint elevation of skin temperature , and none desquamation , but differed slightly in itchiness and efflorescences ( thta - cream : faint / sporadic , bepanthol lotion : none )  . 
concerning the question what would you say , how pleasant is the use of your skin care product ? , the median vas score at 50 gy was 1 ( range 03 ) for patients in arm a and 1.75 ( range 02 ) in arm b ( vas : 0 = very pleasant , 10 = very unpleasant )  . 
 in one patient of arm a , an allergic reaction to thta - cream was suspected , occuring at 38 gy with a rush , efflorescences and strong itching exactly in the area the cream was applied to . 
a reduction by 3 points in our primary endpoint median total score ( e.g. , faint versus moderate erythema in all localizations with equal scores for all other aspects ) would be clinically relevant . 
instead , we found a median total score of 8 in favor of bepanthol lotion versus 11 for thta - creathis is not significant with ten patients per arm , uiq - 1 uiq - 2 uoq - 1 uoq - 2 mlq - 1 mlq - 2 location of tld measurement figure 2 . 
skin surface dose as measured by tld in percent of prescribed dose in three different locations for patients under skin care with thta - cream ( 1 ) and bepanthol lotion ( 2 )  . 
boxand - whisker plot : 50% of values within the box ; the mark in the box indicates the median , the whiskers mark the maximum and minimum of the values . 
hautoberflchendosis laut tld - messung in prozent der zielvolumendosis fr drei verschiedene lokalisationen bei patientinnen unter hautpflege mit thta - creme ( 1 ) und bepanthol - lotion ( 2 )  . 
box - and - whisker - plot : 50% der werte liegen innerhalb der box ; die markierung darin zeigt den median , die vertikalen linien die spannweite der werte . 
mlq : mittig zwischen unteren quadranten ; uiq : oberer innerer quadrant ; uoq : oberer uerer quadrant . uiq - 1 uiq - 2 uoq - 1 uoq - 2 mlq - 1 mlq - 2 ts - 1 ts - 2 sum scores and total score figure 3 . 
skin reaction at 50 gy according to sum score and total score for patients under skin care with thta - cream ( 1 ) and bepanthol lotion ( 2 )  . 
box - and - whisker plot : 50% of values within the box , the mark in the box indicates the median , the whiskers mark the maximum and minimum of the values . 
box - and - whisker - plot : 50% der werte liegen innerhalb der box , die markierung darin zeigt den median , die vertikalen linien die spannweite der werte . 
to increase the power to 80% , 17 patients were needed per arm . considering our results so far , a 6 - point reduction of the median total score for thta - cream with just another seven patients is extremely unlikely . 
in any case , the data leads to the conclusion that there is no superiority of thta - cream at 50 gy in the given setting and can hardly be expected with a larger study . 
 in awareness of the literature about factors affecting acute skin toxicity like radiation technique , target volume , breast size [ 9 ] and weight , lymphocele aspiration , smoking , age , skin cancer , tumor stage and radiation dose [ 24 ] , our treatment groups were well balanced ( table 2 )  . 
similarly , the differing number of patients under hormonal treatment is unlikely to influence the results ; tamoxifen has been hypothesized to enhance the risk of lung fibrosis after radiotherapy [ 3 ] , but an enhancement of skin reaction has not been reported . 
tld measurements at 2 cm distance from field edges resulted in around 65% of prescribed dose in the upper quadrants and 81% in the submammary fold with an intraindividual variation smaller than interindividually . 
further verification derives from clinical results : the follow - up of 270 breast cancer patients with 56 gy whole breast irradiation revealed the submammary fold as the most predominant site for late skin toxicity with a telangiectasia rate of 36% [ 2 ]  . 
 the scoring of acute skin toxicity at 50 gy revealed no statistically significant difference between study arms ( figure 3 )  . treatment was generally well tolerated ; at 50 gy , we observed on average moderate erythema , faint elevation of skin temperature , and no desquamation . 
ranking of photographs due to the side effects visible at 50 gy showed a high congruence between independent observers and confirmed the lack of difference between study arms ( figure 4 )  . 
porock & kristjanson stated that the majority of 126 breast cancer patients in their study did not require application of a topical agent during radiotherapy due to low side effects , but these topical agents were found to promote comfort [ 23 ]  . 
in twelve head and neck cancer patients serving as their own control , skin care with cream on one side of the neck was compared to powder on the other side [ 31 ]  . 
 topical agents have rarely been shown to produce significantly lower skin toxicity in randomized studies ( see table 3 )  . there are negative findings for creams containing dexpanthenol [ 16 ] , aloe vera [ 35 ] , chamomile or almond [ 18 ] , for topical vitamin solution [ 12 ] , lipiderm and biafine [ 8 , 10 , 32 ] , though again , patients content was higher with cream comstrahlenther onkol 2004 no . 
 [ 18 ] 1991 chamomile cream almond oil head and neck , chest , abdomen breast cancer 19 left / right side of area treated 48 above / below scar trend for chamomile no difference year 1982 halperin et al . 
 [ 15 ] 1997 hyaluronic acid cream placebo cream no difference no difference no difference no difference no difference no difference 65 right / left side of head 97 : 97 79 left / right ; breast : upper / lower half 83 : 89 25 : 24 : 25 12 right / left side of neck 44 above / below scar 70 : 64 head and neck , breast , pelvic cancer breast cancer t3 / 4 head and neck cancer 24 : 25 50 : 50 skin reaction later , shorter , less severe reduced incidence of high - grade epithelitis skin reaction less severe skin reaction later , shorter , less severe bostrm et al . 
historically , dna damage with cell deaths and changes in proliferation have been in the center of interest . following conventionally fractionated radiotherapy ( 2 gy 5 ( cid : 1 ) / week ) in bovine skin , first changes in basal cell densities appear at 2025 gy with cell loss reaching a nadir at 50 gy and rapid repopulation with return to control levels at 60 gy [ 1 ]  . dilated microvessels in the underlying dermis and progressive loss of lumen numbers have been reported with single high fractions ; these may initially account for erythema [ 22 , 31 ] and later for chronic changes like the development of telangiectasia [ 1 ]  . 
 trott & liu reported an overexpression of the cytokines tumor necrosis factor ( tnf - ) , interleukin - ( il - ) 1 and inducible nitrous oxide synthase after high single radiation doses in skin of mice , that could be suppressed by anti - inflammatory drugs , thus diminishing the subsequent moist desquamation [ 33 ]  . 
measured the transepidermal water loss ( tewl ) as a sign of epidermal barrier dysfunction during conventionally fractionated radiotherapy to 5060 gy in breast cancer patients [ 29 ]  . 
they found a rise of tewl starting day 11 preceding erythema , and a maximum of tewl around day 27 preceding peak skin changes with normalization of tewl on day 66 . 
apart from a possible explanation for the beneficial effect of hydrolytic enzymes in the prophylaxis of radiation dermatitis [ 11 ] , these considerations may as well be helpful in the development of new treatment strategies such as barrier repair agents [ 6 ]  . 
it could be speculated that thta - cream , even if capable of supporting the lipid metabolism under physiological conditions , may not be able to prevent barrier dysfunction triggered by radiationinduced cytokines . 
bepanthol lotion for skin care in breast cancer under radiotherapy acknowledgments we wish to thank all patients participating in the study and our technical assistants for their assessment of skin marks , as well as the companies theracosm and roche for the disposal of their products . 
kaulich1 , jens zurheide2 , thomas haug3 , wilfried budach2 , fridtjof nsslin1 , michael bamberg2 background : in radiotherapy of intraocular tumors , e.g. , in the case of malign choroid melanomas , episcleral brachytherapy with 106ru ophthalmic plaques has proven to be successful . 
in a study , the authors reported on the discovery of the following shortcomings in industrial quality assurance , which are relevant to therapy , during the course of an internal clinical acceptance test of 106ru ophthalmic plaques , manufactured by the company bebig from berlin , germany . 
moreover , the requested traceability of the calibration of activity and dose rate of the 106ru ophthalmic plaques to standards of the federal authorities in charge of measurement procedures has been implemented . 
 results : in the year 2002 , bebig updated , among other things , the asmw ( gdr ) calibration of the dose rate of the 106ru ophthalmic plaques from the years 19871989 by a calibration of the nist ( usa )  . 
the current nist calibration , together with the new equipment for the measurement of the depth dose curves , led to the consequence that the new nist 2001 dose rate values show , in the mean , a deviation of 0.75 times ( plaque type ccc ) up to 2.06 times ( plaque types ccx , ccy , and ccz ) compared to the dose rate values that had been indicated so far in bebigs certificate , based on the asmw 1987 calibration . 
if one takes into consideration the minimal and maximal values in such 95% confidence intervals , it follows that the new nist 2001 dose rate values deviate between 0.56 times ( plaque type ccc ) and 2.58 times ( plaque types ccx , ccy , and ccz ) from the bebig certificate ( asmw calibration 1987 )  . 
 conclusion : legislation has to make sure that the use of radioactive material on humans be , among other things , permitted as a matter of principle only , if the dose rate calibration can be traced to standards of a federal authority of measurement procedures . 
a historical retrospect reveals that the greatest changes have taken place in the indication of the dose rates of 125i sources . since the beginning of the use of 125i sources in brachytherapy in the late 1960s , the dose rate indications , so far , have had to be reduced in small steps over a period of about 35 years by nearly a factor of 2 . 
as regards the 106ru ophthalmic plaques , the nist 2001 calibration has resulted in a comparable reduction of the dose rate indications of up to a factor of 2 within the period of about several months . 
thus , in the previous history of radiotherapy this case must be regarded as unique , because for the first time ever , an urgently needed recalibration has been protracted for such an unduly long period of time . 
 key words : brachytherapy intraocular tumors 106ru ophthalmic plaques quality assurance dosimetry leakage test strahlenther onkol 2004 ; 180 : 35864 doi 10.1007 / s00066 - 004 - 1183 - 8 zum aktuellen stand der industriellen qualittssicherung von 106ru - augenapplikatoren hintergrund : die episklerale brachytherapie mit 106ru - augenapplikatoren hat sich bei der strahlentherapeutischen behandlung von intraokularen tumoren , z.b. 
in einer studie berichteten die autoren , dass bei der klinikinternen eingangsprfung von 106ru - augenapplikatoren der firma bebig , berlin , folgende therapierelevante schwachstellen der industriellen qualittssicherung festgestellt wurden : inkonsistente dosisleistungsangaben im herstellerzertifikat bis zu einer spannweite von 111% und mangelhafte dichtheit . 
industrial quality assurance procedures for 106ru plaques material und methodik : die firma bebig hat inzwischen die produktion von 106ru - applikatoren modernisiert und alle qualittssicherungsmanahmen bernommen , die von den autoren vorgeschlagen wurden . 
auerdem wurde die angemahnte rckfhrbarkeit der kalibrierung von aktivitt und dosisleistung der 106ru - augenapplikatoren auf bundesbehrden , die fr das messwesen zustndig sind , umgesetzt . ergebnisse : im jahr 2002 hat die firma bebig u.a. 
die aktuelle kalibrierung durch das nist und die neue ausstattung zur messung der tiefendosisverlufe fhrten dazu , dass die neuen nist - 2001 - dosisleistungswerte im mittel vom 0 , 75fachen ( applikator typ ccc ) bis zum 2 , 06fachen ( applikator - typen ccx , ccy and ccz ) von den bisher in den zertifikaten der firma bebig ( asmw - 1987 - kalibrierung ) angegebenen dosisleistungswerten abweichen . 
betrachtet man die minimalen und die maximalen werte im 95% - konfidenzintervall , so ergibt sich , dass die neuen nist - 2001 - dosisleistungswerte vom 0 , 56fachen ( applikator typ ccc ) bis zum 2 , 58fachen ( applikator typen ccx , ccy and ccz ) von den bisherigen zertifikatswerten der firma bebig ( asmw - 1987 - kalibrierung ) abweichen . 
bezglich der dichtheit gab es bei den 106ru - augenapplikatoren , die nach den neuen qualittsmastben produziert wurden , keine beanstandungen . schlussfolgerung : der gesetzgeber muss dafr sorgen , dass die anwendung von radioaktivem material am menschen grundstzlich u.a. 
seit dem beginn der anwendung von 125i - quellen in der brachytherapie in den spten 60er jahren mussten die dosisleistungsangaben bis heute in kleinen schritten innerhalb eines zeitraums von ca . 
however , in the case of recurrent pterygium perioperative 20 - kv soft xray irradiation [ 21 ] is now an effective alternative to 90sr ( cid : 1 ) irradiation . 
in radiotherapy of intraocular tumors , e.g. , in the case of malign choroid melanomas , episcleral brachytherapy with 106ru ophthalmic plaques has proven to be successful [ 14 , 1620 ]  . 
in a study [ 12 ] , the authors reported that in the course of an internal clinical acceptance test of 106ru ophthalmic plaques , manufactured by the company bebig , berlin , germany , the following shortcomings of industrial quality assurance , which are relevant to therapy , were discovered : risk of leakage as well as inconsistent dose rate specifications in the manufacturers certificates , covering a range of 111% . 
in the said study [ 12 ] , bebig was requested to eliminate these shortcomings and to adapt production and the internal quality assurance system of 106ru ophthalmic plaques to state - of - the - art methods . 
this included especially an overdue calibration of the 106ru ophthalmic plaques by a federal authority in charge of measurement procedures that was to replace the calibration of the years 19871989 carried out in those days by the amt fr standardisierung , messwesen und warenprfung ( asmw ) of the now defunct gdr . 
 according to the duty of notification imposed by 3 of the german medizinprodukte - betreiberverordnung the decree on the use of medical products the relevant authority in germany , the bundesinstitut fr arzneimittel und medizinprodukte ( bfarm ) , was informed by the authors in the year 2001 on the results of the internal clinical acceptance test concerning leakage and dose rate of the 106ru ophthalmic plaques [ 6 ]  . 
neither at its own institute nor at the german federal authority for radiation protection ( bundesamt fr strahlenschutz [ bfs ] ) was the bfarm able to come up with a qualified expert on the shortcomings in industrial quality assurance of 106ru ophthalmic plaques , which are relevant to therapy and described in [ 12 ]  . 
 in the meantime , bebig has largely adopted the recommendations published in [ 12 ] , and in a twelve - page customer information of may 15 , 2002 [ 3 ] , it informed users as well as the bfarm that production techniques and the internal quality assurance system of the company had been improved . thereupon , the bfarm asked the authors for a statement on this customer information . 
in this connection , it should be noted that currently , only a consistency check of the dose rate values according to the method described in [ 12 ] can be carried out in the internal clinical acceptance test . 
therefore , the authors advise the bfarm to ensure that an official check of the dose rate values given by bebig is carried out by the relevant german authority before closing the case [ 6 ]  . 
in this regards , the highest authority responsible for measurement procedures in the federal republic of germany is the physikalisch - technische bundesanstalt ( ptb ) in braunschweig , germany . 
 a large part of the results could only be achieved since following the introduction of its new quality management , bebig had five 106ru ophthalmic plaques from tbingen certified again , that had been certified according to the old asmw 1987 quality assurance procedures . 
consequently , besides the leakage test methods and the surface contamination test methods that conform to iso 9978 [ 11 ] and ansi n43.6 [ 1 ] , the companys certificate for sealed radioactive sources delivered with each new applicator under the heading leakage test methods also mentions the following : special immersion test in ringers solution at 20 c for 48 h , the activity in the liquid has been determined and was < 5 bq . contrary to this , in a special one - page customer information regarding test in ringer solution of bebig [ 4 ] , the user is advised against a leakage test in ringers solution as proposed in [ 12 ] with the argument that this will lead to an ugly discolouration of the 106ru plaques . 
instead of this , the user is advised by bebig : if you would like to carry out a leakage test we recommend the wet wipe test with alcohol or distilled and deionised water according to iso 9978 or din 25426 part 4 [ 7 ]  . in [ 12 ] , it was proven that this is not sufficient . 
furthermore , under the heading surface contamination test methods , the companys certificate now also includes the following notice : special contamination test : one millilitre of water was rinsed all over the source , which was repeated 2 times . 
 in january 2002 , four ophthalmic plaques of the types ccd , ccb , cgd , and cib - 2 , and in october 2002 , another two ophthalmic plaques of the types ccc and cib - 2 were submitted to an internal clinical acceptance test according to the leakage test procedure described in [ 12 ]  . 
in addition , random samples of wet wipe tests after moved water bath in ringers solution as well as samples of the ringers solution before application to the patient were examined . 
 in mid - 2002 , the authors noticed , that after the cleansing of a 106ru ophthalmic plaque of the type cib - 2 ( delivery january 2002 ) in an ultrasound bath , the cleansing liquid was contaminated . 
ultrasound cleansing is recommended by bebig in its instructions for the use of 106ru ophthalmic plaques as a possible method of processing after application and was carried out with a us cleansing apparatus that was acquired from bebig . 
the official analysis of a sample from the ultrasound bath of this ophthalmic plaque of the type cib - 2 was entrusted to the tv ( energieund systemtechnik gmbh badenwrttemberg )  . 
as described in [ 12 ] , the authors therefore use a scintillator [ 8 ] with a volume of about 0.8 mm3 ( diameter of 1 mm and height of 1 mm ) for the measurement of the depth dose curves . 
in [ 12 ] , the measurement system that was formerly used by bebig for the measurement of depth dose curves was criticized , since a scintillator whose size was 2 ( cid : 1 ) 2 ( cid : 1 ) 2 mm and of which volume was thus 8 mm3 was used . 
in the measurement protocol , only three depth dose measurement values at depths of 2 mm , 3.5 mm and 5 mm as well as an extrapolated depth dose value at a depth of 0 mm were formerly indicated . 
as regards measurement methods of the activity of 106ru ophthalmic plaques , the certificate for sealed radioactive sources now specifies as well : measurement of activity : the activity has been determined by measuring the resultant radiation and comparing it to a calibrated source , traceable to a national standard . 
in may 2002 , bebig replaced the asmw ( gdr ) calibration of the 106ru ophthalmic plaques dose rate of the years 19871989 by a calibration , which is traceable to standards of the national institute of standards and technology ( nist ; gaithersburg , md , usa ) of december 2001 . 
correct details the user only found in the protocol of measurements under the heading description of the measurement : the energy dose rate of the ( cid : 1 ) - radiation in tissueequivalent material has been measured with a scintillator ( diameter : 1 mm , height : 0.5 mm ) in a water phantothe results are traceable to nist standard ( 12 / 2001 )  . 
 retrospective estimation of the applied dose from the dose prescription the new calibration by the nist in the year 2001 showed that it is not sufficient to determine a calibration factor for all 106ru ophthalmic plaques . 
this means that a retrospective estimation of the applied dose from the dose prescription depends on two factors , i.e. , on the type of ophthalmic plaque and on the depth of the applied dose . 
 results leakage the measurement values of the internal clinical acceptance test concerning leakage , i.e. , wet wipe tests before and after a moved bath in ringers solution as well as evaluation of the samples of each ringers solution , were always < 5 bq . 
accordingly , the wet wipe tests after each application as well as the additional random measurements of the wet wipe tests and the samples of the ringers solutions after moved baths in ringers solution before application to the patients resulted in values < 5 bq for all six ophthalmic plaques . 
this means that in this respect the new specifications of the manufacturer were also fulfilled . for the four ophthalmic plaques that were delivered in january 2002 these results were confirmed by the legally prescribed leakage test of sealed radioactive sources according to 66 strlschv ( ordinance governing radiation protection ) carried out by the tv ( energieund systemtechnik gmbh baden - wrttemberg , germany ) in july 2002 . 
 the evaluation of a sample from the 20 - ml ultrasound bath of the ophthalmic plaque of the type cib - 2 ( delivered january 2002 ) undertaken by the tv in july 2002 ( energieund systemtechnik gmbh baden - wrttemberg ) and meas - ured with a calibrated - spectroscopy unit ( ultra pure germanium crystal ) resulted in a 106ru / 106rh activity of 118 1 bq per ml cleansing liquid h2o . 
after the authors had notified bebig of this complication , bebig informed the authors that a 30 - min ultrasound bath at a temperature of 70 c as an additional quality assurance measure in the future will be carried out . 
the 100% standardization refers to the calibration reference point [ 13 ] , related to the system , and which is situated on the central axis at a distance of 2 mm from the surface of the concave inside of the 106ru ophthalmic plaque . 
the depth dose curves of bebig have been computed from the data of the relevant certificates of bebig based on the asmw 1987 calibration and on the new nist 2001 calibration , respectively . 
the two depth dose curves of the company bebig have been computed from the data of the relevant certificates of bebig based on the asmw 1987 calibration ( measured with an 8 - mm3 scintillator ) and on the new nist 2001 calibration ( measured with an 0.4mm3 scintillator ) , respectively . 
die beiden tiefendosiskurven der firma bebig wurden mit hilfe der entsprechenden firmenzertifikate berechnet , die auf der asmw - 1987 - kalibrierung ( gemessen mit einem 8 - mm3 - szintillator ) bzw . 
in the case of five ophthalmic plaques , the activity indications of the asmw 1987 could be compared with the activity indications of the ptb 2002 , since company certificates for both calibrations exist . 
this contradicts bebigs customer information [ 3 ] , where it is stated in essence on page 7 , that after the new calibration the activity values of the applicators , with the exception of the types ccx , ccy , and ccz , have increased . 
table 1 shows that the activity of the ophthalmic plaques of the types ccd , ccb , and cgd , i.e. , the larger applicators , have , so far , been systematically and significantly underestimated . 
relative dose rate measurements carried out as internal clinical acceptance tests as described in [ 12 ] resulted for seven nist 2001 - calibrated 106ru ophthalmic plaques ( types ccx , cca , ccd , ccb , cgd , ccc , and cib2 ) in a variation coefficient of 3.2%. 
exemplary demonstration of the changes in the activity values of different 106ru ophthalmic plaques following a new calibration at the ptb ( braunschweig , deutschland ) in the year 2002 that replaced the asmw calibration of the year 1987 . 
exemplarische darstellung der nderungen der aktivittswerte verschiedener 106ru - augenapplikatoren durch eine neue kalibrierung bei der ptb ( braunschweig ) im jahr 2002 , die die asmw - kalibrierung aus dem jahr 1987 ablste . 
the results of the acceptance test of the 106ru ophthalmic plaques , of which the dose rate values are now traceable to the nist 2001 calibration , correspond very well with the indications of the manufacturer . 
 retrospective estimation of the applied dose from the dose prescription after the recalibration by the nist in the year 2001 , bebig computed conversion factors f ( plaque type , z ) that are dependent on the type of applicator and on the distance from the middle of the concave inside of the 106ru ophthalmic plaques . 
the conversion factors given to the user in tabular form in bebigs customer information [ 3 ] allow the conversion of the dose rate values , which until that time had been indicated in bebigs certificate , into those values that apply now . 
from this conversion factor f ( plaque type , z ) the following becomes evident : calibration by the nist and the new equipment for the measurement of the depth dose curves led to the consequence that the new nist 2001 dose rate values show , in the mean , a deviation of 0.75 times ( plaque type ccc ) up to 2.06 times ( plaque types ccx , ccy , and ccz ) from the dose rate values that had been indicated so far in bebigs certificate and which were based on the asmw calibration of 1987 . 
if one takes into consideration the minimal and the maximal values in this 95% confidence intervals , it follows that the new nist 2001 dose rate values deviate between 0.56 ( plaque type ccc ) and 2.58 times ( plaque types ccx , ccy , and ccz ) from the bebig certificate ( asmw calibration 1987 )  . 
with regards to , for instance , the ophthalmic plaques of the types ccx , ccy , and ccz , and supposing a scleral thickness of 1 mm and a tumor prominence of 4 mm , i.e. , an apex height of 5 mm , the followstrahlenther onkol 2004 no . 
industrial quality assurance procedures for 106ru plaques ing results occur : at a prescribed dose of 100 gy , a mean dose of 206 gy was applied , using as a basis an old bebig certificate ( asmw calibration 1987 )  . 
 it is striking that the conversion factor f ( plaque type , z ) indicates , for the ophthalmic plaque of type cca , an equal conversion factor for the distance of 3.5 mm and for the distance of 5 mm , i.e. , f ( cca , 3.5 mm ) = f ( cca , 5 mm ) = 1.54. the manufacturer should review these two conversion factors . if one is attentive to the tendencies in the conversion factor f ( plaque type , z ) , it is evident that the conversion factors in all other plaques increase with an increasing distance from the applicator surface . 
 it is also to be noted that with the help of the manufacturers conversion factors it is only possible to estimate dose values for tumors whose prominence is 4 m discussion the results of this article constitute an important up - to - date interim report for the rightly confused user of 106ru ophthalmic plaques as well as for the bfarm . 
in its statement in [ 5 ] , bebig contested the results of the authors in [ 12 ] concerning the shortcomings in the industrial quality assurance of 106ru ophthalmic plaques , which are relevant to therapy . 
but the results presented here demonstrate very patently that the the authors criticism was justified and that there was an urgent need for action on behalf of bebigs quality management . 
the general adoption of the proposals from tbingen concerning the quality assurance of 106ru ophthalmic plaques enabled bebig to catch up with the state of the art that is common in brachytherapy nowadays . 
a quick accomplishment by bebig of the few remaining tasks , such as the correction of the company certificates and the indication of a conversion factor for the calculation of the contained activity of the 106ru ophthalmic plaques , would be satisfying indeed . 
 with the help of table 1 in the bebigs customer information [ 3 ] , the dose - finding studies for intraocular tumors undertaken so far could , in principle , be corrected and reevaluated up to a tumor prominence of 4 mm using the conversion factors f ( plaque type , z )  . 
 future legislation should see to it that the use of radioactive material should only be permitted , among other things , if the dose rate calibration of the radioactive material can be traced to standards of a federal authority of measurement procedures . 
 recent experiences with 106ru ophthalmic plaques , which have been in use for more than 40 years [ 20 ] , have clearly shown that the medical physicist has to act in a very critical and committed way while carrying out internal clinical acceptance tests of radioactive material that is to be used on humans . 
as the penultimate authority , the medical physicist bears an especially high responsibility in tracking down shortcomings in industrial quality assurance , which are relevant to therapy , as well as for the identification of corresponding legal insufficiencies . 
 historical dimension for all radionuclides that were or are still used in brachytherapy , measurement methods as well as computing procedures of the dose rate have been continually improved over the course of time . 
since the beginning of 125i source usage in brachytherapy in the late 1960s , the dose rate indications , so far , have had to be reduced nearly by a factor of 2 [ 15 ]  . 
with regard to the 106ru ophthalmic plaques , a comparable reduction of the dose rate indications of up to a factor of about 2 has resulted due to the nist 2001 calibration . 
yet , the greatest difference to the recalibration of the 106ru ophthalmic plaques consists in the fact that in the case of the recalibration of 125i sources , this process took place in small steps over a period of about 35 years while in stark contrast to this , the dosimetry of the 106ru ophthalmic plaques has been corrected within the period of several months . 
thus , in the previous history of radiotherapy this case must be regarded as unique , since for the first time ever , an urgently needed recalibration has been protracted for such an unduly long period of time . 
virginia : strahlentherapie und onkologie original article verification of imrt : techniques and problems ludwig bogner , josef scherer , marius treutwein , matthias hartmann , franz gum , axel amediek1 purpose : imrt ( intensity - modulated radiotherapy ) verification techniques are reviewed together with investigations demonstrating the intrinsic verification problems . 
among the latter are techniques like fluence or three - dimensional ( 3 - d ) dose distribution verification within a transfer phantodifferent radiographic films and absolute dose probes are investigated for their suitability . 
in addition , simple tests have shown that dose calculation approximations in the imrt option of tms are one major source of the dose deviation . xvmc / vef does not use such approximations . 
later on , a minimal program could consist of a fluence or relative dose verification procedure with few films and absolute dose measurement , followed by an intensive mlc quality assurance ( qa )  . 
 key words : imrt verification qa monte carlo tps commissioning strahlenther onkol 2004 ; 180 : 34050 doi 10.1007 / s00066 - 004 - 1219 - 0 verifikation der imrt : techniken und probleme ziel : neben einem berblick ber verifikationstechniken der imrt ( intensittsmodulierten radiotherapie ) werden untersuchungen zu intrinsischen verifikationsproblemen dargestellt . material und methodik : verschiedene verifikationsmethoden fr klassenlsungen sowie fr individuelle patientenplne werden demonstriert , wie etwa fluenzund dreidimensionale dosisverteilungen in einem ersatzphantodazu werden verschiedene radiographiefilme und absolutdosissonden auf ihre eignung untersucht . 
monte - carlo - techniken ( xvmc / vef ) werden zur fehleranalyse eingesetzt und auf ihre tauglichkeit zur verifikation untersucht . ergebnisse : bei der klinischen einfhrung der imrt bei kopf - hals - tumoren wurden parallel fluenz - , relativund absolutdosimetrische verfahren zur verifikation angewandt . 
verification of imrt introduction while imrt ( intensity - modulated radiotherapy ) treatments of patients started some years ago in the usa , the introduction into clinical routine has proceeded much slower in germany . 
there is a critical review within a report of the imrt collaborative working group of the national cancer institute of the usa [ 5 ] , which contains a summary of imrt verification methods and their problems . 
the investigations have revealed weak links in the entire chain of therapy planning system ( tps ) commissioning treatment planning delivery verification and yield a critical assessment of what can be used to minimize errors in imrt dose delivery . 
 material and methods imrt method the treatment of h&n cancers by means of imrt was started in 2002 , using a seven - beam technique equally spaced in the posterior hemisphere according to hunt et al . 
one or both parotid glands , the spinal cord , the brain stem , and the unspecified tissue outside the eptv plus oars ( organs at risk ) are included in the optimization as oars . 
one applies a sequential boost technique with the same seven - field imrt technique used in the preceding large - volume imrt treatment ( the latter being shown in figure 6 )  . 
 imrt verification strategies since imrt is a sophisticated task for treatment planning as well as for realization of the treatment , a reliable quality assurance ( qa ) of the dose distribution within the patient is of extraordinary importance . 
the authors of the aforementioned report [ 5 ] stress that imrt dose distributions are characterized by complex three - dimensional ( 3 - d ) dose gradients and a time - dependent fluence delivery , placing severe limitations on the dosimeters and techniques . 
first of all , dose calculation by means of pencil beam model with imrt - specific approximations and disregarding small - field problems [ 1 ] ( ahnesj 2002 , personal communication ; murman 2003 , personal communication ) is possibly too inaccurate to achieve reliable results in an inhomogeneous medium in case of very small fields or field segments , which results from a high - resolution fluence segmentation . 
 another issue regarding the accuracy of treatment planning systems is the inappropriate modeling of treatment head details , which , in fact , turns out to strongly influence the accuracy of output factors and beam profiles in case of small irregular fields , especially in off - axis positions . 
simple multileaf modulated beams should be generated and the absolute dose verified in a slab phantothese subbeams should be calculated as single fields as well , because different algorithms are often used for modulated as opposed to unmodulated beams . these are some reasons why careful and multiple verification methods of imrt treatment plans must be done to try to separate the different sources of inaccuracies and to correlate them to tps , verificationor delivery - associated problems . from such a study , reliable verification techniques can presumably be derived , and the remaining tps - associated errors can be explained and regarded for corrections . imrt plan verification would require , in principle , an inhomogeneous anthropomorphic phantom identical to the patient . 
 verification of class solutions a classic method for verification of class solutions is the application of the treatment technique to a rando phantom and applying tlds , in combination with radiographic film dosimetry , to it ( e.g. , [ 23 ] )  . 
 another technique of dose verification is becoming interesting , as computer hardware gets more and more powerful : the monte carlo ( mc ) dose simulation [ 15 , 20 , 22 ]  . 
mc techniques are said to be the most precise dose engines , because , in principle , their accuracy depends only on the number of photons sampled [ 9 ]  . 
a remaining problem is , as in the case of convolution - based algorithms , the necessity of a very detailed treatment head model and its commissioning in order to correctly describe output factors and beam profiles of small irregfigure 1 . 
the possibly easier way consists of the measurement of the fluence distribution separately for each modulated treatment field , but the task group report [ 5 ] stresses that as no mechanism currently exists for independently verifying that the delivered fluence yields the desired dose distribution , an independent determination of the measured and calculated dose distribution coordinates is essential . 
in any case , even after succeeding to prove that it is sufficient to verify the fluence distributions of all fields , an absolute dose determination in at least one suitable point within a smoothly modulated area of each field by ionization chamber ( ic ) dosimetry or another reliable probe is mandatory . 
because of the remaining inaccuracies of the tps , described above , comparisons of these point doses with the correlated calculated doses must be regarded within an accuracy evaluation concept . moreover , as pointed out by the task group report , the calculated dose distribution must be accessed by an appropriate measurement . 
the shape and size of this phantom should be somewhat correlated with the shape of the treated area of the patient . this can be , in case of h&n tumors , a solid water cylinder with a diameter of approximately 20 csuch a phantom is easily accessible to dosimetry by radiographic films and absolute dose measurements by suitable probes for dose comparisons with calculated data ( figure 1 )  . 
the dose was then measured with 0.3 cm3 ic ( m23332 , ptw ) , diamond ( m60003 , ptw ) , and dosimetry diode ( m60008 , ptw ) in a slab phantom ( rw3 , ptw ) at the isocenter in 10 cm depth . 
one of the reasons is that most film materials , which are not water - equivalent , are very sensitive to low - energy photons , produced in the process of depth penetration of a photon . 
 measurements of fluence distributions by means of film dosimetry are usually done in a water - equivalent slab phantom in a distinct depth , with the beam direction perpendicular to the plane of the filthe measurement within a phantom beyond the depth dose maximum as opposed to in - air measurements seems to be mandatory . 
in addition , the optical density of the film after irradiation only correlates with the dose , which itself is only proportional to the photon fluence , when a local secondary electron equilibrium exists [ 18 ]  . 
yet , comparisons of in - air and in - phantom investigations of fluence distributions , measured by means of a radiographic film ( edr2 , kodak ) , reveal only a minor difference in the order of < 2% . 
for this kind of investigation , with perpendicular beam entrance to film plane , the choice of film type is not really essential , as long as one properly corrects the dependence of the optical density to the dose . 
 the situation changes completely when applying film dosimetry to 3 - d dose investigations within a transfer phantom , because , in coplanar imrt techniques , all beam angles are parallel to the plane of the filit is well known that in such a situation low - energy photons , increasingly produced with increased depth , result in a higher response of the film , such leading to dose errors of up to 20% . 
in an earlier study , we have investigated filter methods for parallel beam angles by use of a 0.6 mm thick lead filter , positioned symmetrically 5 mm from the film within the water - equivalent slab phantom , such yielding fairly good agreement within 7% with ionization chamber curves in the range > 1.5 c on the other hand , much better agreement without any filter at all is shown by the edr2 film , in the depth range of 118 cm with a dose deviation to ionization chamber measurement < 4% ( figure 4 )  . additionally , edr2 can be used as an absolute dosimeter within an accuracy of about 3% . 
die optische dichte als funktion der dosis fr den edr2film in verschiedenen tiefen . to one filit is important , during the corresponding ionization chamber measurement , to apply the complete sequence for the measurement of each individual subfield to account for scatter contributions from the remaining fields . 
for this reason , we investigated the output factor variation with field size by means of edr2 film dosimetry , measured in a depth of 5 cm rw3 , and compared it to ionstrahlenther onkol 2004 no . 
dosisdifferenzen zwischen der ionisationskammer und edr2 ( unten )  . determination of the absolute dose in a dose reference point by means of ionization chamber dosimetry was done using a 0.3 cm3 thimble chamber ( m23332 / unidos , ptw )  . 
for our own investigations , we defined a cylindrical volume of interest ( voi ) in a highly homogeneous region of the dose cube with an appropriate size to account for chamber volume and setup errors . 
this is not only for class solution verifications , but also for individual dosimetry within a transfer phantothe method is , in principle , capable of delivering a true 3 - d dose distribution within any phantom shape , filled with a homogeneous polymer gel , such avoiding the danger of undetected hot or cold spots ( e.g. , [ 6 , 12 ] )  . 
we use xvmc , including the monte carlo ( mc ) treatment head model vef , as described by fippel et al . [ 911 ] , which we commissioned with data from our linac ( primus , siemens ) for 6 - mv photons . 
for verification purposes , the optimization is switched off , and xvmc / vef is used for forward calculations of all beam segments , as determined by the pencil beam - based imrt treatment plan ( tms , nucletron b.v. ) and transferred via dicom - rt . 
 finally , all verification work requires the comparison of calculations with measurements of fluence in a slab phantom or dose distributions in a suitable transfer phanto to be highly flexible in redefining evaluation goals , we have developed our own verification software ( imrt - verif ) by means of matlab ( mathworks ) similar to others [ 29 ]  . 
it accepts data in the dicom - rt standard , using fiducial points ( figure 1 ) for matching , tilting , and rescaling picture resolution and normalization of pixel contents , etc . 
the evaluation procedure delivers a comparison of the processed raw data , its absolute and relative dose difference , and , additionally , a modified plot of absolute gamma values [ 21 ] , with arrows per pixel indicating the direction and size of distance - to - agreement deviation . 
comparison of edr2 film dosimetry and ic - based output factors of quadratic field sizes , measured in a depth of 5 cm ( top ) and of difference ( bottom )  . 
verification of imrt results when starting with imrt treatment of patients in our clinics in 2002 , we preferred to use different and independent verification methods to reveal any possible sources of error . 
figure 7 shows the result of a comparison between the measured and calculated fluence - proportional profiles of one modulated beam of the treatment plan , shown in figure 6 . 
at first , an absolute dose determination in one point of the transfer phantom , using ic or diode dosimetry , was done , yielding a measured dose about 57% too low in all cases investigated so far . 
the evaluation of the differences in this slice to tms calculation in terms of relative dose difference ( figure 8b ) and gamma plot ( figure 8c ) with a distance of agreement of 3 mm and 3% of dose shows a relative good agreement , with the exception of edge effects and hot spots . the absolute dose correction factor has been applied to the monitor units ( mus ) of the patient treatment plan , as well . 
 the evaluation of the verification of five patient treatment plans , three of which had been calculated with a sequential boost and two with an sib technique [ 27 , 31 ] , showed absolute dose deviations , which seemed to depend on the number of segments . 
in five imrt plans with about 70 segments , we found deviations of 6% ( 1% ) , whereas two boost cases with 30 segments somehow resulted in lower deviations of 5% ( 1% )  . 
the external segmentation software imfast ( siemens , [ 28 ] ) was used to investigate if any dependence of absolute dose deviation from the number of segments for the same treatment plan exists . 
starting from a tms calculation with the built - in segmentation algorithm switched off , the resulting fluence distribution was externally segmented by imfast with different restrictions to the number of segments . these plans were then transferred to the transfer phantom , followed by a comparison of absolute dose measurement to calculation . 
 9 ( cid : 1 ) 9 cm2 field also showed a lower dose , when calculated as imrt beathe closer intercomparison of tms 6.1a calculation as modulated rather than as normal beams revealed a 2.63.4% ( for two different siemens primus linacs ) dose error due to approximations made for imrt beams . 
the calculation deviates up to 2.5% for pb and 5% for cc , respectively . small - field dosimetry on quadratic fields showed that tms compares well with diamond measurements down to 2 ( cid : 1 ) 2 cm2 ( figure 10 )  . 
at 1 ( cid : 1 ) 1 cm2 , the tms 6.1a result gives a 23% lower output when compared to the diamond probe . diode shows a 11% higher dose response , the 0.3 cm3 ionization chamber is completely off due to the detector size . 
verification of imrt application of the new model to a patient case for comparison with the old model , strongly supports that small - field problems play a minor role , but instead , it is additional dose calculation approximations , which are only applied in imrt ( murman 2003 , personal communication ) , which seem to play the major role . 
since mlc tolerance tables allow a 2 mm deviation of the nominal leaf position , we looked for the differences in absolute dose of the 70 - segment patient plan when adding or subtracting 2 mm to every leaf within every segment as a worst case by means of an mc calculation . 
in doing so , we could detect a rather high influence of leaf position errors on the mean dose of about 8% ( low by smaller and high by larger aperture ) between both extremes ( figure 12 )  . 
the simultaneous application of relative fluence and dose verification in a transfer phantom in combination with absolute dose verification by ic or diode dosimetry is time - consuming , but it demonstrated its sensitivity for the detection of errors which can occur in the imrt chawhereas the fluence distributions of the modulated beams and the relative dose are in general good agreement with the calculated ones , we revealed systematic deviations in the absolute dose at a reference point . 
our search for the causes of these deviations can be divided into four parts : ( 1 ) investigations of the probes used for the verification process showed clearly that for relative film dosimetry in a transfer phantom the edr2 film is the only suitable one , whereas for relative fluence verification other films like xomat , ec - v are good as well . 
dose profile for the shown small irregular field , measured by diode , pin - point ic , ic15 , and edr2 film , normalized to 10 ( cid : 1 ) 10 cm2 . 
dosisprofile fr ein kleines irregulres feldsegment , gemessen mit diode , pin - point - ic , ic15 und edr2 - film , normiert auf 10 ( cid : 1 ) 10 cm2 . 
the commissioning data set consists of profiles using a 0.13 - cm3 ic and output factors down to minimal field sizes of 5 ( cid : 1 ) 5 cm2 according to tms recommendations in version tms 6.1a. ofs for smaller fields are extrapolated due to missing dastrahlenther onkol 2004 no . 
mc verification of the imrt treatment plan of figure 6 by means of xvmc / vef by dose - volume histograms of planning target volume , spinal cord , and right parotid gland . 
the focal spot size evaluation is based on the measurements of the 10 ( cid : 1 ) 10 cm2 field , which is usually done with a medium - volume chamber , although a high - resolution detector would be required for this purpose . 
a new head model with elliptic source size ( tms 6.1b ) commissioned by diamond - based ofs down to 1 ( cid : 1 ) 1 cm2 yields a rather good agreement . 
high deviations could also be found in the investigation of extremely small irregular field sizes ( but within tms default imrt settings ) with respect to beam profiles and ofs , showing again the necessity to measure data down to smaller field sizes with suitable probes like diamond or diodes for tps commissioning . 
 ( 3 ) our investigations strongly support that small - field problems play a minor role , but instead there are additional dose calculation approximations , which are only applied in imrt ( murman 2003 , personal communication ) which seem to play the major role . 
in addition to the calibration of the leaves at gantry zero position , it should be checked whether the mlc alignment depends on the gantry angle or on the moving direction of the leaf . 
it has to be emphasized that the manufacturer of a tps must disclose all approximations of the imrt algorithm , together with recommendations for base data measurement being sensifigure 12 . 
mc simulations of the mlc misalignment , demonstrated by means of the treatment plan of figure 6 : the histogram of [ 100 ( cid : 1 ) ( dose with deviating leaf positions dose with optimal leaf positions ) / dose with optimal leaf positions ] is shown . 
mc - simulationen zur mlc - dejustierung am beispiel der dosisverteilung des plans aus abbildung 6 : dargestellt ist die histogrammverteilung der gre [ 100 ( cid : 1 ) ( dosis bei abweichenden mlc - positionen dosis bei optimalen mlc - positionen ) / dosis bei optimalen mlc - positionen ]  . 
moreover , he must provide for a very detailed pre - release commissioning of the tps , together with his beta test sites , and supply the customer with the results of this . 
it must be sufficient for a hospital physicist to restrict himself to a post - release tps commissioning , which only can be a subset . in spite of the discussed problems , imrt is a method to spare the organs at risk and to get a sufficient dose in the ptv in one session [ 24 , 30 ]  . 
the classic irradiation technique for h&n tumors , on the other hand , claims multiple fields with overor underdosage at field matchlines of electron and photon fields and does not allow sparing the parotids . 
another source of error , relativizing the problems discussed in that paper , originates from the uncertainty of positioning , even when using a stereotactic mask syste conclusion the process of finding the most reliable verification process is perhaps close to its end . 
then , as a minimal individual verification concept , one should be able to reduce the procedure to either fluence or dose verification , but in both cases an absolute dose determination should be included for safety reasons . 
both methods are sensitive to detect delivery problems . an mc system like xvmc / vef is extremely useful as a tool to detect different sources of errors during the imrt introduction phase of a distinct tumor site . 
on the other hand , an mc system cannot be a verification tool for a pb - based tps , as dose differences are a priori to be expected . so the only way to avoid the well - known problems of pb algorithm is to use inverse mc systems like imco + + / iko [ 3 ] or hyperion [ 2 ] for imrt . 
 strahlentherapie und onkologie original article effect of the hypoxic cell sensitizer isometronidazole on local control of two human squamous cell carcinomas after fractionated irradiation andreas schreiber1 , 2 * , mechthild krause1 * , daniel zips1 , annegret drfler1 , klaus richter3 , sophie vettermann1 , cordula petersen1 , bettina beuthien - baumann4 , daniela thmmler5 , michael baumann1 , 6 background and purpose : hypoxia of clonogenic tumor cells is a major reason for radioresistance and hence local failure in radiotherapy . 
the objective of the present study was to test the efficacy of the hypoxic cell sensitizer isometronidazole ( iso ) during fractionated irradiation in two different human squamous cell carcinomas . 
 material and methods : local control was evaluated for fadu ( radiobiological hypoxic fraction [ rhf ] 7% ) and gl tumors ( rhf 0.1% ) after single - dose ( sd ) irradiation under ambient conditions and after 30 fractions within 6 weeks ( 30 f / 6 w )  . 
iso significantly decreased the sd - tcd50 in fadu tumors ( dose - modifying factor [ dmf ] = 1.2 ; p = 0.01 ) but not in the better oxygenated gl tumor . 
also significantly improved local control of fadu tumors after 30 fractions in 6 weeks ( dmf = 1.2 ; p = 0.01 ) , indicating that hypoxic clonogenic cells in fadu tumors are not only present before start of irradiation but also limit the efficacy of treatment during a fractionated course of radiotherapy . 
this , in light of the fact that other well - tolerable hypoxic cell sensitizers such as nimorazole with clinically proven efficacy at daily oral doses of < 3 g are available , limits the potential usefulness of iso for radiation oncology . key words : hypoxic cell sensitizer fractionated irradiation hypoxia local tumor control squamous cell carcinoma human tumor xenografts isometronidazole strahlenther onkol 2004 ; 180 : 37582 doi 10.1007 / s00066 - 004 - 1206 - 5 effektivitt des hypoxic cell sensitizer isometronidazol whrend fraktionierter strahlentherapie zweier humaner plattenepithelkarzinome in nacktmusen hintergrund und ziel : hypoxie klonogener zellen ist eine wichtige ursache fr die strahlenresistenz von tumoren und damit fr lokalrezidive nach strahlentherapie . 
das ziel der vorliegenden studie war die berprfung der effektivitt des hypoxic cell sensitizer isometronidazol ( iso ) whrend einer fraktionierten strahlentherapie in zwei unterschiedlichen menschlichen plattenepithelkarzinomen . material und methodik : die lokale kontrolle wurde fr fadu ( radiobiologische hypoxische fraktion [ rhf ] 7% ) und gl - tumoren ( rhf 0 , 1% ) nach einzeldosis - ( sd - ) bestrahlung unter normalen blutflussbedingungen und nach 30 fraktionen in 6 wochen ( 30 f / 6 w ) bestimmt . 
iso wurde bei beiden tumoren 60 min vor der sd - bestrahlung in einer konzentration von 100 mg / kg krpergewicht ( kg ) oder 750 mg / kg kg appliziert . 
whrend der fraktionierten bestrahlung erfolgte die applikation von iso tglich 60 min vor jeder fraktion ( 100 mg / kg kg , bei fadu zustzlich 750 mg / kg kg )  . 
 1 department of radiation oncology , medical faculty carl gustav carus , university of technology , dresden , germany , 2 department of radiotherapy , hospital dresden - friedrichstadt , dresden , germany , 3 department of clinical pharmacology , medical faculty carl gustav carus , university of technology , dresden , germany , 4 department of nuclear medicine , medical faculty carl gustav carus , university of technology , dresden , germany , 5 apogepha arzneimittel gmbh , dresden , germany , 6 experimental center , medical faculty carl gustav carus , university of technology , dresden , germany . 
efficacy of isometronidazole in fractionated irradiation ergebnisse : in beiden tumormodellen konnte weder nach sd - bestrahlung noch nach fraktionierter bestrahlung eine verbesserung der lokalen tumorkontrolle durch die applikation von iso 100 mg / kg kg gezeigt werden . 
iso in einer dosis von 750 mg / kg kg fhrte auch zu einer signifikanten verbesserung der lokalen kontrolle von fadu - tumoren nach 30 fraktionen in 6 wochen ( dmf = 1 , 2 ; p = 0 , 01 )  . 
dies deutet darauf hin , dass fadu - tumoren nicht nur vor beginn der behandlung hypoxische klonogene zellen enthalten , sondern dass diese auch whrend einer fraktionierten bestrahlung die effizienz der therapie limitieren . 
 schlussfolgerung : iso zeigt in einer konzentration von 750 mg / kg kg eine effektivitt als hypoxic cell sensitizer im ausgeprgt hypoxischen fadu - tumor , aber nicht im weniger hypoxischen gl - tumor . 
die tatsache , dass gut vertrgliche hypoxic cell sensitizer wie nimorazol , deren wirksamkeit bei tglichen dosen von < 3 g per os bereits klinisch nachgewiesen wurde , zur verfgung stehen , limitiert den potentiellen nutzen von iso fr die radioonkologie . 
 schlsselwrter : hypoxic cell sensitizer fraktionierte bestrahlung hypoxie lokale tumorkontrolle plattenepithelkarzinom humane tumorxenografts isometronidazol introduction anoxic and severely hypoxic cells are by a factor of approximately 3 more radioresistant than well - oxygenated cells [ 16 , 45 ]  . 
it is widely accepted that the presence of hypoxic clonogenic cells in tumors is an important determinant of the outcome of radiotherapy [ 19 , 21 , 27 ]  . 
the fraction of severely hypoxic , radioresistant clonogenic tumor cells , i.e. , the radiobiological hypoxic fraction ( rhf ) , can be determined in experimental tumors using colony - forming assays , or comparisons of tumor growth delay or tumor control under ambient and clamped hypoxic conditions . 
these assays are not applicable in the clinical situation , however , indirect evidence , e.g. , results of measurements of the intratumoral oxygen partial pressure using microelectrodes , supports that radiobiological hypoxic cells also negatively impact local control of tumors in patients treated with radiotherapy [ 6 , 7 , 12 , 14 , 15 , 20 , 28 , 37 , 42 , 43 ]  . 
possible approaches include correction of anemia by transfusion [ 9 ] or erythropoietin [ 17 , 41 ] , application of hyperbaric oxygen or normobaric carbogen [ 36 , 38 ] , application of drugs that improve tumor perfusion [ 22 ] , and use of hypoxia - specific cytotoxins [ 8 , 10 ]  . another possibility that has been widely tested in experimental and clinical studies is the use of electron - affinic substances , so - called hypoxic cell sensitizers . 
these drugs mimic the effect of oxygen but are not rapidly metabolized by tumor cells and therefore can diffuse further into the tissue than oxygen [ 29 , 31 ]  . 
the most potent of the electron - affinic substances is the 2nitroimidazole misonidazole , with sensitizer enhancement ratios ( ser ) of > 2 in animal tumors irradiated with single doses [ 11 , 32 ]  . 
the toxicity and efficacy of nitroimidazoles are linked to the pharmacological characteristics of the substances with 2 - nitroimidazoles and lipophilic substances being more toxic but also more efficient than other compounds [ 31 ]  . 
it has therefore been suggested that an improved therapeutic ratio may be achieved by application of less effective but at the same time much better tolerable nitroimidazoles during each fraction of the course of radiotherapy [ 11 , 31 ]  . 
a randomized trial testing nimorazole in head and neck cancer supports this approach [ 30 ] , while two trials testing etanidazole did not improve outcome of radiotherapy [ 13 , 23 ]  . isometronidazole ( iso ) , a 4 - nitroimidazole derivative , is a weak water - soluble hypoxic sensitizer with low lipophilicity . the tissue distribution of iso compares favorably to other nitroimidazoles showing only 50% of the tumor dose being reached in the cerebral tissue , whereas in metronidazole the same distribution of the substance was found in all organs [ 25 ]  . studies on v79 cells demonstrated an activity of iso as a hypoxic cell sensitizer in vitro [ 26 ]  . 
the experiments were performed using two human squamous cell carcinomas ( hscc ) in nude mice that previously have been shown to differ in their rhf before and during fractionated radiotherapy [ 2 ]  . 
 material and methods animals the experiments were performed using 7to 14 - week - old male and female nmri ( nu / nu ) mice from the specific pathogenfree breeding facility of the experimental center of the medical faculty carl gustav carus , university of dresden , germany . 
the animals were fed a commercial laboratory animal diet and water ad libituto immunosuppress the nude mice further , they were whole - body irradiated 13 days before tumor transplantation with 4 gy using 200 - kv x - rays ( 0.5 mm cu ) at a dose rate of about 1 gy / m tumors fadu is an established human hypopharyngeal squamous cell carcinoma line , kept in high passage by the american type culture collection ( rockville , md , usa )  . 
in extensive series of quantitative tumor transplantation and of radiation tumor control assays , fadu tumors have been shown to evoke no or only a very low level of residual immune reactivity in nude mice [ 3 , 46 ]  . 
 gl was established as a permanent tumor line in nude mice in this laboratory from a surgical specimen of a patient suffering from laryngeal carcinoma in 1991 [ 33 ]  . 
 cryoconserved tumor tissue from our tumor bank was transplanted subcutaneously ( s.c. ) to the back of nude mice . the originating tumors were passaged to a second group of nude mice before transplantation into experimental animals . for the experiments , source tumors were excised , cleaned from necrotic tissue , cut into small pieces , and transplanted s.c. into the right hind leg of the recipient mice . 
tumor volumes were determined by the formula of a rotational ellipsoid / 6 ( cid : 1 ) a ( cid : 1 ) b2 , where a is the longest and b the perpendicular shorter tumor axis . 
 to investigate whether the pharmacokinetics of iso during fractionated irradiation is different compared to untreated tumors , the tumor concentration as a function of time was determined prior to treatment , after application of ten fractions in 2 weeks , and after 20 fractions in 4 weeks ( 2.0 gy per fraction in fadu , 1.5 gy per fraction in gl )  . 
the concentration of iso in tumor tissue and in serum was investigated in a total of 150 mice at 5 , 30 , 60 , 90 , 120 , 180 , 240 , and 300 min after injection of the drug using reverse - phase high - performance liquid chromatography ( hplc )  . 
for this , the tumors were excised , homogenized ( 1 g in 9 ml sodium chloride solution / 1 , 000 ml water ) and centrifuged at 10 , 000 g . 
 local tumor irradiation and experimental design local irradiations were given with 200 - kv x - rays ( 0.5 mm cu ) at a dose rate of 1.11.2 gy / min using a specially designed jig allowing irradiation of up to five animals at the same time . 
fadu or gl tumors were irradiated either with single doses ( sd ) under ambient or clamp conditions or with 30 fractions in 6 weeks ( 30 f / 6 w ) under ambient conditions . isometronidazole ( iso ) was applied in a concentration of 100 mg / kg b.w. 
faduoder gl - tumoren wurden entweder mit einzeldosen ( sd ) unter normalem oder abgeklemmtem blutfluss oder mit 30 fraktionen in 6 wochen ( 30 f / 6 w ) unter normalem blutfluss bestrahlt . 
isometronidazol ( iso ) wurde in einer konzentration von 100 mg / kg kg ( iso 100 ) oder 750 mg / kg kg ( iso 750 ) 1 h vor jeder fraktion oder vor einzeldosisbestrahlung appliziert . 
 the animals were randomized over the experimental matrix in groups of three to four , aiming for about ten animals ( range : seven to 15 animals ) for each of the six to eight dose groups in each experimental arthe tumor control assays include data from 912 irradiated and 163 untreated control tumors . 
 determination of the tcd50 values and dose - modifying factors local tumor control rates were analyzed 120 days ( fadu ) or 180 days ( gl ) after the end of treatment . 
this time is adequate to detect virtually all regrowing tumors , as judged from asymptomatic curves of the incidence of recurrence versus time , approaching plateau values at day 60 in fadu and day 120 in gl [ 2 , 4 , 33 , 34 ]  . 
 dose - response curves for local tumor control , tcd50 values , i.e. , the radiation dose necessary to control 50% of the tumors locally , and dose - modifying factors ( dmf ) were calculated from the local control rates using a poisson - based inactivation model and maximum likelihood analysis as previously described in detail [ 2 ]  . 
 efficacy of iso after single - dose irradiation in vivo figure 2 shows the tcd50 values for fadu and gl tumors irradiated with single doses under ambient or clamped conditions 1 h after i.p. 
in the better oxygenated gl tumor , the tcd50 values were not significantly different compared to nacl injection after irradiation under ambient conditions and application of iso both in concentrations of 100 mg / kg b.w. 
die intratumorale konzentration des medikaments wurde in unbestrahlten tumoren ( ( cid : 1 ) ) , nach zehn fraktionen mit 2 gy ( 1 , 5 gy bei gl ) pro fraktion in 2 wochen ( ( cid : 2 ) ) und nach 20 fraktionen mit 2 gy ( 1 , 5 gy bei gl ) pro fraktion in 4 wochen ( ( cid : 3 ) ) gemessen . 
 efficacy of iso during fractionated irradiation in vivo figure 3 shows the dose - response curves for fadu and gl tumors irradiated with 30 fractions under ambient conditions in 6 weeks . 
for the experiments , two hscc lines ( fadu and gl ) that previously have been shown to differ in their rhf before and during fractionated radiotherapy [ 2 ] were selected . 
using the equation given by moulder & rockwell [ 27 ] , the single - dose tcd50 values under ambient and clamp hypoxic conditions ( table 2 ) , the d0 values of 1.1 gy for fadu cells [ 1 ] and 0.9 gy for gl cells ( drfler & baumann , unpublished data ) in vitro , and assuming an oxygen enhancement ratio ( oer ) of 2.7 , an rhf of 7% for fadu tumors and 0.1% for gl tumors can be estimated . 
was selected , since , based on pharmacokinetic and - dynamic data [ 18 , 2426 , 39 ] , this would be the initial dose level for a phase i clinical trial . 
however , application of iso at this dose level in both tumors did neither decrease the sinclamp ambient ambient iso 100 ambient iso 750 nacl clamp ambient nacl ambient iso 100 ambient iso 750 figures 2a and 2b . 
tcd50 values ( ( cid : 1 ) ) and 95% confidence interval after single - dose irradiation under ambient and clamped conditions and under ambient conditions after application of isometronidazole 100 mg / kg ( iso 100 ) b.w. 
tcd50 - werte ( ( cid : 1 ) ) und 95% - vertrauensbereiche nach einzeldosisbestrahlung unter normalem und abgeklemmtem blutfluss und unter normalem blutfluss bei vorheriger applikation von isometronidazol 100 mg / kg kg ( iso 100 ) oder 750 mg / kg kg ( iso 750 ) in fadu ( a ) und gl - tumoren ( b )  . 
tcd50 values , dose - modifying factors ( dmf ) , and p - values for fadu and gl tumors after single - dose ( sd ) and fractionated irradiation with 30 fractions in 6 weeks ( 30 f / 6 w )  . 
dmf was defined as the ratio of tcd50 under ambient conditions over the tcd50 under clamp hypoxic conditions or over the tcd50 under ambient conditions after application of isometronidazole ( iso )  . 
tcd50 - werte , dosismodifizierende faktoren ( dmf ) und p - werte fr faduand gl - tumoren nach einzeldosis ( sd ) und fraktionierter bestrahlung mit 30 fraktionen in 6 wochen ( 30 f / 6 w )  . 
iso wurde 1 h vor jeder bestrahlungsfraktion in einer konzentration von 100 mg / kg kg ( iso 100 ) oder 750 mg / kg kg ( iso 750 ) appliziert . 
this finding confirms the principal efficacy of iso as a hypoxic cell sensitizer and indicates that hypoxic clonogenic cells in fadu tumors are not only present before the start of irradiation but also limit the efficacy of treatment during a fractionated course of radiotherapy [ 2 , 35 ]  . 
lokale tumorkontrollraten ( symbole ) und tumorkontrollwahrscheinlichkeiten ( linien ) nach bestrahlung von fadu ( a ) oder gl - tumoren ( b ) mit 30 fraktionen in 6 wochen . 
isometronidazol ( durchgezogene linien ) wurde 60 min vor den bestrahlungen in einer konzentration von 100 mg / kg kg ( ( cid : 5 ) ) oder 750 mg / kg kg ( ( cid : 6 ) ) appliziert . 
local tumor control rates ( symbols ) and tumor control probability ( lines ) after irradiation of fadu ( a ) or gl tumors ( b ) with 30 fractions in 6 weeks . 
this , in light of the fact that other well - tolerable hypoxic cell sensitizers such as nimorazole with clinically proven efficacy at daily oral doses of < 3 g are available [ 29 ] , limits the potential usefulness of iso for radiation oncology . 
 strahlentherapie und onkologie aktuelles forum antitumorale wirkung von interferonen und interleukinen in kombination mit strahlentherapie teil ii : strahlenbiologische und immunologische strategien carsten herskind1 , 2 , katharina fleckenstein2 , jens lohr3 , chuan - yuan li4 , frederik wenz2 , frank lohr2 hintergrund : die kombinierte tumorbehandlung mit zytokinen wie interferonen ( ifn ) und strahlentherapie wurde zunchst phnomenologisch , zunehmend aber auf strahlenbiologischer grundlage durchgefhrt . 
in den letzten jahren ist das verstndnis fr die komplexen interaktionen des zytokinnetzwerkes im rahmen des immunsystems allerdings stark gestiegen , so dass das rational solcher studien neu bewertet werden sollte . 
 methodik : auf grundlage publizierter klinischer studien werden die bisherigen ergebnisse der kombinationsbehandlung mit ifn - ( cid : 1 ) , ifn - ( cid : 2 ) bzw . 
insbesondere die toxizitt war bei systemischer gabe oft ein probleneue immunologische erkenntnisse haben allerdings gezeigt , dass lokale interaktionen zwischen antigenprsentierenden zellen und effektorzellen wie natrlichen killerzellen ( nk - zellen ) und t - lymphozyten wichtig fr eine effektive immunreaktion gegen tumoren sind . 
neue prklinische studien weisen auf die bedeutung der zellulren produktion von zytokinen bei der interaktion zwischen den komponenten des immunsystems hin . gentherapeutische verfahren knnten dazu beitragen , die toxizitt der behandlung mit zytokinen zu reduzieren . schlsselwrter : strahlentherapie biological response modifiers zytokine interferon interleukin immunreaktion tumorassoziierte antigene ( taa ) strahlenther onkol 2004 ; 180 : 3319 doi 10.1007 / s00066 - 004 - 8119 - 1 antitumoral action of interferons and interleukins in combination with radiotherapy . 
part ii : radiobiological and immunologic strategies background : combined tumor treatment with cytokines , e.g. , interferons ( ifn ) , and radiotherapy was initially of phenomenological nature but has increasingly been based on a radiobiological rationale . 
 results : the initially high expectations regarding the antitumoral action of ifn - ( cid : 1 ) , ifn - ( cid : 2 ) and ifn - ( cid : 3 ) in combination with radiotherapy have , with few exceptions , not been fulfilled . 
recent advances in immunology , however , have emphasized the importance of local interactions between antigen - presenting cells and effector cells such as natural killer ( nk ) cells and cytotoxic t - lymphocytes in the immune reaction against tumors . 
 1 department of experimental clinical oncology , aarhus university hospital , aarhus , dnemark , 2 institut fr klinische radiologie , sektion strahlentherapie , mannheim , 3 department of pathology , university of california san francisco school of medicine , san francisco , california , usa , 4 department of radiation oncology , duke university medical center , durham , north carolina , usa . 
antitumorale wirkung von zytokinen und radiotherapie teil ii conclusion : a few positive clinical studies give cause for hope that a therapeutic benefit may be achieved by targeted , local application of cytokines . 
recent preclinical studies indicate the importance of cellular cytokine production in the interaction between the components of the immune systegene therapy might contribute to reduce the toxicity associated with cytokine treatment . key words : radiotherapy biological response modifiers cytokines interferon interleukin immune response tumorassociated antigens ( taa ) einleitung zu verbesserung der strahlentherapie von strahlenresistenten tumoren bzw . 
von tumoren , die aufgrund des umgebenden strahlenempfindlichem normalgewebes nicht mit hohen strahlendosen effektiv behandelt werden knnen , ist die erweiterung des therapeutischen fensters zwischen tumorheilung und normalgewebsreaktion von essentieller bedeutung . 
 groe hoffnungen verbanden sich in den letzten beiden jahrzehnten mit den interferonen ( ifn ) und interleukinen ( il ) als biologische agenzien , die die strahlentherapie ergnzen oder sogar die strahlenempfindlichkeit der tumoren erhhen knnten . 
als spter klar wurde , dass sich auch auf tumorzellen zytokinrezeptoren befinden und dass zytokine die strahlenempfindlichkeit von tumorzellen modulieren knnen , wurden prklinische und klinische studien zunehmend auf strahlenbiologischer basis durchgefhrt . mit dem wachsenden verstndnis fr die regelund steuerfunktionen , die zytokine vor allem im rahmen des immunsystems , aber auch im rahmen anderer prozesse wie z.b. der angiogenese bernehmen , kommt derzeit der modulation der immunreaktion gegenber tumorzellen eine immer grere bedeutung als rational fr den einsatz von zytokinen in kombination mit strahlentherapie zu . 
prklinische strategien zur verbesserung der gezielten antitumoralen wirkungen der zytokine werden am beispiel von il - 2 und il - 12 unter besonderer bercksichtigung der immunologischen zusammenhnge und anderen bisher untersuchten wirkungsweisen dargestellt und deren klinischer einsatz diskutiert . 
die grte effizienz zeigte ifnbisher bei haarzellleukmie , chronischer myeloischer leukmie ( cml ) und follikulren lymphomen , wenn auch eher eine protrahierung des krankheitsverlaufs als eine verbesserte heilung zu beobachten war . 
bei metastasierten kopf - hals - tumoren war in phase iii die modulation von cisplatin / 5 - fluorouracil ( 5 - fu ) durch ifn - 2b wirkungslos [ 65 ] ; bei metastasierten blasenkarzinomen erwies sich in phase iii die kombination cisplatin / 5 - fu mit ifn - 2b gegenber mvac ( methotrexat , vinblastin , doxorubicin , cisplatin ) sogar als nachteilig [ 69 ]  . 
die kombination von interferonen mit strahlentherapie schien eine gewisse effizienz zu haben , allerdings waren die untersuchungen mehr kasuistischer natur . systematisch kam ifn - ( cid : 2 ) in kombination mit chemound strahlentherapie bei npc nur in einer nicht randomisierten pdiatrischen studie zum einsatz . 
die therapieassoziierte toxizitt blieb moderat [ 49 ]  . zunehmend wurde der einsatz von interferonen in kombination mit strahlung aber auch in der erhhten strahlensensibilitt von gegenber ifnoder ifn - ( cid : 2 ) exponierten tumorzelllinien in vitro begrndet [ 3 , 11 , 23 , 64 ]  . 
als erhhung des verhltnisses letaler zu subletalen schden verstanden werden , was dagegen interessanterweise bei normalen diploiden mrc - 5 - fibroblasten nicht der fall war [ 64 ]  . 
zervix wurde interferon fter in kombination mit retinoiden ( retinoic acid [ ra ] ) zunchst ohne bestrahlung eingesetzt , was durch den synergistischen effekt ihrer nicht berlappenden wirkungsweisen begrndet wurde [ 40 , 41 , 68 ]  . 
dies fhrte bald zu klinischen phase - i / ii - studien mit ifn und 13 - cis - ra kombiniert mit strahlentherapie an verschiedenen tumorentitten , wobei von der haut bzw . 
viral ist , deutete sich in phase i / ii eine wirksamkeit der kombination ifn - 2a / 13 - cis - ra mit strahlentherapie an [ 55 ]  . 
ifn - 2b in kombination mit strahlentherapie , allerdings ohne ra , zeigte in einer phase - ii - studie an fortgeschrittenen zervixkarzinomen eine mgliche verbesserung des langzeit - berlebens in einer subgruppe der patientinnen ; die behandlung war jedoch mit erheblich mehr sptfolgen ( proktitiden ) verbunden [ 75 ]  . eine phase - i / ii - studie , die radiotherapie und ifn - ( cid : 2 ) bei 32 patienten mit fortgeschrittenen nichtkleinzelligen bronchialkarzinomen ( nsclc ) kombinierte , wartete mit exzellenten ergebnissen auf ( 81% ansprechen gegenber 35% historisch ) , wobei insbesondere auch das berleben verbessert zu werden schien [ 47 ]  . 
in der anschlieenden randomisierten phase - iii - studie ( rtog 93 - 04 ) konnte die hohe ansprechrate jedoch nicht reproduziert werden , und die ergebnisse von ifn - ( cid : 2 ) in kombination mit radiotherapie waren gegenber der alleinigen radiotherapie nicht verbessert [ 7 ]  . 
obwohl fr gliomzellen in vitro ein strahlensensibilisierender effekt der kombination von ifnund 13 - cis - ra beschrieben wurde [ 46 ] , zeigte eine klinische phase - ii - studie keinen effekt bei hochgradigen gliomen [ 16 ]  . 
die ermittelten 2 - jahres - berlebensraten lagen bei 84% fr die untersuchte kombination mit ifngegenber 54% fr die alleinige radiochemotherapie bei einer kontrollgruppe aus retrospektiven fllen [ 53 ]  . 
diese ergebnisse sollten deshalb baldmglichst in randomisierten phase - iii - studien unter standardisierten bedingungen berprft werden , um abzuklren , ob diese gezielte kombination verschiedener agenzien unter einbindung von ifn die erhoffte verbesserung der berlebensrate herbeifhren kann . 
 in einer phase - iii - studie bei hochgradigen gliomen konnte ifnadjuvant in kombination mit bcnu ( carmustin ) nach induktionsbehandlung mit strahlentherapie / bcnu die erwartungen aus prklinischen bzw . 
in einer phase - ii / iii - studie bei metastasierten melanomen war ifnbei 81 patienten mit nur einer kompletten und drei partiellen remissionen allenfalls gering wirksam und ohne eine erkennbare dosis - wirkungs - beziehung [ 63 ]  . 
eine phase - iii - studie mit adjuvanter ifn - - behandlung von patienten mit kleinzelligen bronchialkarzinomen ( sclc ) in komplettremission nach radiochemotherapie zeigte keinen signifikanten unterschied fr tumorprogression und berleben und war sogar tendenziell schlechter fr die ifn - - behandlung [ 31 ]  . 
 die insgesamt inkonsistenten antitumoralen effekte von ifnfhrten zu der schlussfolgerung , dass ifnnicht systemisch , sondern nur bei produktion durch bestimmte zellpopulationen , wie natrliche killerzellen ( nk - zellen ) und t - zellen , effektiv ist [ 9 , 22 ]  . 
antitumorale wirkung von zytokinen und radiotherapie teil ii toxizitt der kombination interferon / strahlentherapie ein gravierender nachteil der systemischen behandlung mit interferonen sind die zytokinassoziierten nebenwirkungen . diese umfassen im wesentlichen vier kategorien : konstitutionelle ( fieber , schttelfrost , krmpfe , gewichtsverlust , mdigkeit / schwche ) , neuropsychiatrische ( schlfrigkeit , verwirrtheit , neuropathien , depression ) , hmatologische und hepatische . 
berhaupt stellt die potentielle neurotoxizitt die grte gefahr dar [ 48 ] , vor allem wenn ifnmit der bestrahlung groer volumina von nervengewebe kombiniert wird [ 25 ]  . hnlich wie bei chemotherapeutika wurden auch recallphnomene beobachtet , so z.b. 
mit ifn ( pneumonitis ) [ 67 ] und ifn ( haut ) [ 73 ]  . zusammenfassung der klinischen studien die oben dargestellten studien zur systemischen ifn - gabe als adjuvans zur strahlentherapie sind in tabelle 1a bis 1c zusammengefasst . 
die ergebnisse zeigen , dass die erwartungen aus den prklinischen und frhen klinischen studien bisher nicht in greren randomisierten studien besttigt werden konnten . einen hoffnungsschimmer stellen die vorlufigen positiven ergebnisse einer studie mit ifn - - gabe in kombination mit radiochemotherapie bei pankreastumoren dar [ 53 ]  . 
 interleukine und radiatio : prklinische studien zytokine in der immunreaktion gegen tumorzellen vor dem hintergrund der klinischen erfahrungen mit interferon scheint es sinnvoll , gewonnene erkenntnisse ber das zusammenspiel zwischen zytokinen , dem immunsystem und tumorzellen bei der weiteren entwicklung einer kombinationstherapie einzusetzen . 
interferon stimuliert die expression von major - histocompatibility - complex - moleklen der klasse i ( mhc - i ) auf tumorzellen , die fr die antigenprsentation und wechselwirkung mit t8 - killerlymphozyten ( cd8 + ) erforderlich ist . 
 il - 2 und radiatio il - 2 spielt zusammen mit ifneine zentrale rolle fr die zellulre immunantwort und knnte deshalb potentiell die antitumorale immunreaktion durch bestrahlung untersttzen . die experimentelle therapie mit il - 2 und strahlentherapie in murinen tumormodellen war erfolgreich hinsichtlich der behandlung von lungenmetastasen und primrtumoren kurz nach inokulation , whrend bezglich grerer primrtumoren keine synergie erreicht wurde [ 29 ]  . 
in prostatatumoren sowohl der ratte [ 32 ] als auch der maus [ 26 ] wurde jedoch das ansprechen auf strahlentherapie durch il - 2 verbessert . im renca - tumormodell konnte die systemische gabe von il - 2 die immunstimulation durch unilaterale bestrahlung verstrken , so dass auch das wachstum unbestrahlter kontralateraler tumoren gehemmt wurde [ 77 ]  . 
sowohl cd4 + und cd8 + - t - lymphozyten als auch nk - zellen schienen dabei beteiligt zu seuntersuchungen in sl2 - lymphomen zeigten , dass die peritumorale injektion von il - 2 zusammen mit lokaler bestrahlung von nur einem tumor auch zur regression eines kontralateralen unbehandelten tumors fhrte [ 33 ]  . 
 mittels inokulation von unbestrahlten il - 2 berexprimierenden renca - tumorzellen konnte die antitumorale wirkung von il - 2 sowohl in wildtypwirten als auch in athymischen ( nackt - ) musen nachgewiesen werden [ 52 ]  . 
da il - 2 nicht nur t - lymphozyten , sondern auch nk - zellen aktiviert , deutet dies auf nk - zellen als effektorzellen h ifnberexprimierende zellen wurden dagegen nur in wildtypmusen , nicht aber in nacktmusen gehemmt , so dass in letzteren nk - zellen anscheinend nicht durch ifnaktiviert werden . 
weil ifneine hochregulierung von mhc - i und mhc - ii sowie die rekrutierung von antigenprsentierenden zellen ( apc ) hervorruft , liegt es nahe , dass die zytotoxische antwort in wildtypwirten in diesem fall von t - zellen vermittelt werden knnte . 
multiple vakzinierungen mit bestrahlten zytokinproduzierenden zellen kombiniert mit lungenbestrahlungen im renca - lungenmetastasenmodell zeigten synergistische antitumorale effekte mit lokaler bestrahlung fr beide zytokine [ 52 ]  . il - 12 und radiatio in prklinischen studien mit murinen lewis - lung - tumoren wurde eine synergie zwischen systemischer applikation von il - 12 und lokaler strahlentherapie beobachtet [ 72 ]  . 
brther : brachytherapie ( dosis in punkt a angegeben ) ; 13 - cis - ra : 13 - cis - retinsure ; cr : komplette remission ; gd : gesamtdosis ; k.a. : keine angaben ; n.s. : nicht signifikant ; nsclc : nichtkleinzelliges bronchialkarzinom ; pr : partielle remission . 
brther : brachytherapy ( dose in point a given ) ; 13 - cis - ra : 13cis retinoic acid ; cr : complete remission ; gd : total dose ; k.a. : not available ; n.s. : not significant ; nsclc : non - small - cell lung carcinoma ; pr : partial remission . 
 tumorentitt studienrandomipatienten phase siert zytokin fraktionierung chemo ergebnis , endpunkt signifi kanz literatur pankreas glioblastom iii a gegenber historischer kontrolle nein ifn - ( cid : 1 ) 25 ( cid : 4 ) 1 , 82 , 2 gy 5 - fu , cispt 84% , 2 - jahres p = 0 , 04a 383 / 275 ifn - ( cid : 1 ) 36 ( cid : 4 ) 1 , 8 gy bcnu berleben 10 monate , med . 
nach heilung des primrtumors wurde sogar eine cd8 + - abhngige immunitt gegenber einer zweiten inokulation beobachtet [ 66 ]  . untersuchungen zu den zellulren effektoren der immunreaktion gegenber dem primrtumor wurden in dieser studie nicht durchgefhrt . ein gentherapeutischer ansatz mit intratumoraler injektion von fr il - 12 / b7.1 kodierendem adenovirus in murine 4t1 - mammakarzinome und b16 - melanome ergab hnliche synergien mit fraktionierter strahlentherapie [ 43 ]  . 
nach hoch dosiertem il - 2 in kombination mit autologen tumor - infiltrating lympocytes ( til ) und ohne bestrahlung wurde bei 86 patienten mit metastasierten malignen melanomen eine ansprechrate von 34% beobachtet [ 60 ]  . eine randomisierte studie bei 113 patienten mit nsclc zeigte eine signifikante verbesserung des berlebens und der lokalen kontrolle bei verwendung von il - 2 und til in der adjuvanten postoperativen situation gegenber radiochemotherapie , aber keinen effekt auf die inzidenz von fernmetastasen [ 56 ]  . 
in einer randomisierten phase - iii - studie mit insgesamt 174 resezierten primren lungentumoren waren das 5und 9 - jahresberleben nach il - 2 / lak - immuntherapie ( lak : lymphokine - activated killer cells ) in kombination mit adjuvanter chemooder strahlentherapie mit 54% bzw . 
 in kombination mit chemotherapie mit cisplatin , vinblastin und dacarbazin , die allein bisher keinen positiven einfluss auf das berleben von patienten mit metastasierten malignen melanomen hatte , wurde nach il - 2 / ifn - - behandlung eine ansprechrate in hhe von 60% beobachtet , davon sogar 20% mit kompletten remissionen [ 38 ]  . 
 auf basis der oben und im ersten teil dieser bersicht ( strahlenther onkol 2004 ; 180 : 18793 ) beschriebenen prklinischen untersuchungen zum effekt von il - 2 in kombination mit bestrahlung im renca - modell [ 77 , 78 ] wurde eine klinische phase - ii - studie initiiert , die die kombination von einzeitbestrahlung ( 8 gy ) und il - 2 - injektionen bei 16 patienten mit metastasierten nierenzellkarzinomen untersuchte . 
 die intravense systemische applikation von il - 12 war , hnlich wie bei il - 2 , mit teils ausgeprgter toxizitt verbunden , die vom verwendeten zeitlichen schema abhing [ 39 , 58 ]  . die subkutane gabe wurde besser toleriert [ 50 ]  . 
vakzination mit il - 12 - gen - transduzierten melanomzellen zeigte in einer phase - i - studie nur milde toxizitt und fhrte bei drei von sechs patienten zu einem stabilen krankheitsverlauf [ 71 ]  . 
ber studien zur behandlung mit il - 12 in kombination mit strahlentherapie wurde unseres wissens bisher nicht berichtet . die problematische kurze halbwertszeit ( von il - 2 ) und die hohe systemische toxizitt der interleukine knnen mglicherweise mit gentherapeutischen verfahren und lokaler applikation kompensiert bzw . 
reduziert werden [ 1 , 35 ]  . physiologische effekte der zytokine : oxygenierung und vaskularisierung klinische studien weisen darauf hin , dass hypoxie mit einer verschlechterung der prognose verbunden ist [ 20 , 62 ] und die angiogenese durch expression von vascular endothelial growth factor ( vegf ) stimulieren kann [ 17 ]  . 
die initialen daten bezglich dieses endpunkts besttigten sich in einer anschlieenden randomisierten studie ( haensgen & dunst , manuskript in vorbereitung ) , ohne sich jedoch bisher eindeutig im klinischen ergebnis niederzuschlagen ( haensgen & dunst , persnliche mitteilung )  . 
mit il - 2 transfizierte emt6 - mammakarzinome waren gegenber bestrahlung empfindlicher als wildtyptumoren , was auf eine reduzierte hypoxische fraktion infolge der verbesserten vaskularisierung der tumoren zurckgefhrt wurde [ 36 ]  . 
die oben beschriebenen untersuchungen zu adenoviraler il - 12 - expression kombiniert mit bestrahlung eines murinen fibrosarkoms zeigten eine gefrarefizierung des primrtumors , die eine antiangiogene wirkung von il - 12 nahe legt [ 66 ]  . 
insbesondere die erhebliche toxizitt fgt sich zu einer wachsenden skepsis gegenber interferonen als biologische therapeutika in kombination mit chemotherapie bei epithelialen tumoren [ 2 , 12 ]  . dennoch lassen wenige lichtblicke die hoffnung zu , dass eine verbesserte lokale applikation bzw . 
eine gezielte kombination verschiedener modalitten zum erfolg fhren knnte . es wird allerdings hier deutlich , dass anstelle eines phnomenologischen ansatzes ein verstndnis der komplexen interaktionen der zytokine mit den verschiedenen komponenten des immunsystems , mit den tumorzellen und mit der bestrahlung erforderlich ist . 
insgesamt gestatten die daten die schlussfolgerung , dass die antitumoralen effekte fr il - 2 und il - 12 , hnlich wie fr die meis - ten anderen zytokine , vom untersuchten tumormodell und von der applikationsart abhngen und sowohl immunologisch - spezifischer als auch unspezifischer natur sind . 
neue einsichten in die mechanismen , die zur immunologischen toleranz gegenber tumoren fhren , ermglichen einen differenzierteren , gezielten einsatz der zytokine , der einen multidisziplinren ansatz unter einbeziehung immunologischer , gentechnischer und strahlenbiologischer erkenntnisse und verfahren erfordert . die enwicklung von einer zunchst berwiegend empirischen basis hin zu einem auf strahlenbiologischen und immunologischen mechanismen bauenden rational gibt anlass zur hoffnung , die lokale wirksamkeit der strahlentherapie weiter zu verbessern und dabei evtl . 
a phase iii comparison of radiation therapy with or without recombinant beta - interferon for poor - risk patients with locally advanced non - small - cell lung cancer ( rtog 93 - 04 )  . 
acquired immunity in nude mice induced by expression of the il - 2 or il - 4 gene in human pancreatic carcinoma cells and anti - tumor effect generated by in vivo gene transfer using retrovirus . 
13 - cis - retinoic acid and interferon alpha - 2a : effective combination therapy for advanced squamous cell carcinoma of the skj natl cancer inst 1992 ; 84 : 23541 . 
interferon - alpha 2a , 13 - cis - retinoic acid and radiotherapy for locally advanced carcinoma of the cervix : a pilot study . eur j gynaecol oncol 1998 ; 19 : 358 . 
prospective randomized trial of the treatment of patients with metastatic melanoma using chemotherapy with cisplatin , dacarbazine , and tamoxifen alone or in combination with interleukin - 2 and interferon alfa - 2b . 
phase iii trial of fluorouracil , interferon alpha - 2b , and cisplatin versus methotrexate , vinblastine , doxorubicin , and cisplatin in metastatic or unresectable urothelial cancer . j clin oncol 2002 ; 20 : 13617 . 
6 urban & vogel strahlentherapie und onkologie kasuistik frhzeitiger zahnverlust nach leukmiebehandlung im kindesalter fallbericht und literaturbersicht thomas herrmann1 , wolfgang drr1 , susanne koy2 , aquina lesche1 , dietmar lehmann1 hintergrund : ber die auswirkungen einer bestrahlung im kindesalter am zahnapparat gibt es bisher nur wenige mitteilungen . ursache fr einen frhzeitigen zahnverlust scheint eine verkleinerung der wurzeloberflche nach strahleneinwirkung zu sedie schdigung des zahnhalteapparats ist in der regel eine folge der bei neoplasien im kindesalter blicherweise angewandten radiochemotherapien . 
 fallbericht : es wird ber einen 33 - jhrigen patienten berichtet , der im alter von 11 jahren wegen einer akuten lymphatischen leukmie mit rezidiv eine intensive chemotherapie und eine neuroachsenund hirnschdelbestrahlung erhielt . 
der patient wurde in der implantationssprechstunde der klinik und poliklinik fr mund - , kieferund gesichtschirurgie vorstellig , da er schwere zahnvernderungen mit zahnverlust trotz guter zahnrztlicher betreuung und mundhygiene aufwies . 
 schlussfolgerung : eine intensive lebenslange zahnrztliche nachbetreuung von patienten mit durchgemachten tumorerkrankungen im kindesalter muss gefordert werden , um einerseits die therapiefolgen an den zhnen durch geeignete pflegemanahmen zu verringern , zum anderen aber auch rechtzeitig die notwendigen zahnrztlichen prothetischen manahmen einzuleiten . 
 schlsselwrter : strahlenfolgen an zhnen bei kindern kindliche neoplasien prophylaktische zns - bestrahlung bei kindlichen leukmien radiogene wachstumsstrungen strahlenther onkol 2004 ; 180 : 3714 doi 10.1007 / s00066 - 004 - 1244 - z early loss of teeth after treatment for childhood leukemia background : only few reports of effects of radiotherapy in childhood on the dental apparatus are available in the literature . 
 case report : a 33 - year - old patient is reported , who , at the age of 11 years , received high - dose chemotherapy and radiotherapy of neuroaxis and cranium for acute lymphatic leukemia with relapse . 
radiation doses given to the superior maxilla and mandible at the age of 11 were estimated to be in the range of 825 gy . conclusion : intense , life - long dental care and follow - up of patients cured from malignant disease in childhood must hence be postulated in order to minimize dental treatment sequelae by supportive measures , but also to initiate timely adequate dental and prosthetic management . 
 key words : dental radiation effects in children childhood neoplasia prophylactic cranial irradiation for childhood leukemia radiation - induced growth impairment 1 klinik und poliklinik fr strahlentherapie und radioonkologie , medizinische fakultt der technischen universitt dresden , 2 klinik und poliklinik fr mund - , kieferund gesichtschirurgie , medizinische fakultt der technischen universitt dresden . 
zahnverlust nach leukmiebehandlung im kindesalter fallbericht ein 33 - jhriger patient wurde von seiner hauszahnrztin in der interdisziplinren implantationssprechstunde der klinik und poliklinik fr mund - , kieferund gesichtschirurgie des universittsklinikums dresden vorgestellt . 
 zur intraoralen dentalen rehabilitation des patienten wurde bei der vorstellung in der implantationssprechstunde eine implantatinsertion regio 35 , 36 , 37 , 45 , 46 und 47 geplant . die motivation fr eine intensive mundhygiene und eine engmaschige zahnrztliche berwachung als voraussetzung fr eine implantatversorgung sind bei dem patienten gegeben . 
die behandlung erfolgte mit chemotherapie ( vincristin , cyclophosphamid , cytarabin [ alexan ] , thioguanin , l - asparaginase , methotrexat [ mtx ] , bcnu ) sowie einer prophylaktischen bestrahlung von schdel und neuroachse mit jeweils 18 gy ( einzeldosis 1 , 5 gy ) unter telecobaltbedingungen . 9 monate spter wurde ein rezidiv mit meningeosis leucaemica diagnostiziert . 
neben einer systemischen chemotherapie ( mercaleukin ) erfolgten intrathekal die gabe von mtx , cytarabin ( alexan ) und prednisolon sowie eine zweite bestrahlung mit nochmals 24 gy ( 1 , 5 gy pro fraktion ) auf cerebrum und neuroachse , wiederum als telecobalttherapie . die intrathekale cytarabin ( alexan ) und prednisolongabe wurde ber 3 jahre fortgesetzt . 
unter enerbol - gabe kam es zu einer langsamen befundbesserung , so dass 1 , 5 jahre nach der rezidivtherapie das eeg als normalisiert beschrieben wurde und alle klinischen symptome verschwunden waren . 
die damalige bestrahlung mit einer additiven dosis von 42 gy in zwei serien an der neuroachse wurde anhand eines gegenwrtig ( 2003 ) in behandlung befindlichen 10 - jhrigen kindes mit den heute zur verfgung stehenden mglichkeiten der bestrahlungsplanung rekonstruiert , wobei besonders die belastung im unterund oberkieferbereich betrachtet wurde . 
zahnverlust nach leukmiebehandlung im kindesalter im gegensatz dazu sind folgen am gebiss von patienten , bei denen eine tumorerkrankung im kindesalter erfolgreich therapiert wurde und die im erwachsenenalter vernderungen an ihrem zahnstatus aufweisen , nur in wenigen publikationen beschrieben worden . 
 [ 9 ] verglichen 1987 die entwicklung des zahnstatus von kindern , die wegen einer malignen erkrankung eine kombinierte radiochemotherapie erhalten hatten , mit 49 gleichaltrigen geschwistern und stellten fest , dass in der behandelten gruppe zahnschmelzvernderungen hufiger auftraten als in der kontrollgruppe , obwohl beide populationen keine unterschiede in oraler hygiene , gingivitishufigkeit und kariesmorbiditt aufwiesen . 
in einer untersuchung an 45 leukmiekranken kindern kamen pajari & lanning [ 10 ] 1995 zu der aussage , dass die chemotherapie die zahnschmelzentwicklung , nicht jedoch das wurzelwachstum strte . 
es trat eine statistisch signifikante verkleinerung dieser oberflche gegenber derselben anzahl gesunder gleichaltriger kinder auf . die patienten hatten im kindesalter eine chemotherapie und eine prophylaktische schdelbestrahlung ( maximal 22 gy ) wegen einer all erhalten . 
eine ganzkrperbestrahlung mit 10 gy war deutlich wirksamer in bezug auf die beeintrchtigung des zahnhalteapparats als eine chemotherapie mit prophylaktischer schdelbestrahlung , was auf die niedrigeren dosen am bestrahlten kiefer zurckgefhrt werden kann . 
 im fall unseres patienten scheint eine solche kompensation nicht ausreichend wirksam gewesen zu sein , so dass bereits in einem lebensalter von 33 jahren und nach dosen von additiv etwa 1825 gy am kiefer ein ausgeprgter zahnverlust konstatiert werden muss . 
diese schtzung scheint auf den europischen raum bertragbar zu sein und lsst erwarten , dass eine problematik wie bei unserem patienten in zukunft hufiger auftreten drfte , auch wenn neue strahlenarten und bestrahlungstechniken insbesondere bei kindlichen patienten die normalgewebe in umgebung des tumors entlasten knnen [ 6 , 8 ]  . 
darber hinaus sollte eine adquate zahnrztliche versorgung dieser patienten auch bei zahnverlusten im jugendlichen erwachsenenalter gesichert se neben einer intensiven zahnrztlichen berwachung der patienten , welche lebenslange fluoridierung sowie mundhygieneinstruktionen und ernhrungsberatung beinhaltet , mssen bei chirurgischen manahmen nach bestrahlung im kieferbereich von kindern manahmen zur prophylaxe einer osteoradionekrose auch im erwachsenenalter ergriffen werden . 
 dem radioonkologen drfte durch die kostentrger in zukunft hufiger die frage gestellt werden , ob es sich bei vernderungen am zahnapparat bei diesen patienten um eine radiogene nebenwirkung der neoplasiebehandlung handeln knnte . 
beim gegenwrtigen kenntnisstand wird man bei in der kindheit bestrahlten patienten selbst wenn nur eine prophylaktische bestrahlung der neuroachse und des schdels erfolgte diese frage in der regel bejahen mssen . 
6 urban & vogel strahlentherapie und onkologie original article intraoperative radiotherapy of soft tissue sarcoma of the extremity annette kretzler1 , michael molls1 , reiner gradinger2 , peter lukas3 , hans - ullrich steinau4 , florian wrschmidt1 purpose : evaluation of treatment outcome after intraoperative radiotherapy ( iort ) external - beam irradiation ( ebrt ) in patients with localized soft tissue sarcoma of the extremity at high risk for local recurrence after limb - sparing surgery . 
surgical margin status , primary versus recurrent tumor and tumor stage did not show any statistically significant influence ( univariate analysis ) on local recurrence rates . patients with t1 tumors exhibited a borderline significant ( p = 0.053 ) better distant disease - free survival ( 83% ) compared to t2 tumors ( 43% )  . 
 key words : soft tissue sarcoma intraoperative radiotherapy radiotherapy functional outcome local tumor control strahlenther onkol 2004 ; 180 : 36570 doi 10.1007 / s00066 - 004 - 1191 - 8 intraoperative strahlentherapie von weichteilsarkomen der extremitten ziel : beurteilung der behandlungsergebnisse nach intraoperativer strahlentherapie ( iort ) perkutane strahlentherapie ( ebrt ) bei patienten mit nicht metastasierten weichteilsarkomen der extremitten , die ein hohes lokalrezidivrisiko nach extremittenerhaltender operation hatten . patienten und methodik : zwischen 1989 und 1999 wurden daten von 28 patienten retrospektiv ausgewertet . 
alle patienten wurden einer extremittenerhaltenden operation und einer iort ( mediane dosis 15 gy ) unterzogen , die entweder als highdose - rate - brachytherapie oder mittels linac appliziert wurde . 
 schlsselwrter : weichteilsarkom intraoperative strahlentherapie strahlentherapie funktionales behandlungsergebnis lokale tumorkontrolle 1 department of radiotherapy and radiation oncology , klinikum rechts der isar , technical university munich , germany , 2 department of orthopedics and orthopedic surgery , klinikum rechts der isar , technical university munich , germany , 3 radiotherapy & radiation oncology , leopold franzens university innsbruck , austria 4 department of plastic surgery , university hospital bergmannsheil , bochum , germany . 
intraoperative radiotherapy of soft tissue sarcoma introduction in patients with soft tissue sarcoma of the extremity at high risk for local recurrence , the current standard treatment consists of limb - sparing surgery and external - beam radiotherapy ( ebrt ; either preor postoperatively ) achieving 5 - year actuarial local control rates of 7487% [ 8 , 9 , 14 , 27 ]  . 
therapists are faced with the dilemma of minimizing the risk of local recurrence , which negatively affects prognosis [ 5 , 16 ] , and at the same time preserving maximal function of the extremity . 
the rationale behind intraoperative radiotherapy ( iort ) is the possibility to apply a single high dose with enhanced biological effectiveness resulting in sterilization of microscopic disease of the tumor bed . 
in a prospective randomized trial of retroperitoneal sarcomas it has been shown that local tumor control rates could be significantly improved combining iort with low doses of ebrt [ 24 ]  . 
 the aim of this study was to evaluate patients with soft tissue sarcoma of the extremity , combining intraand postoperative radiotherapy , with special regard to local control , side effects , and limb function . 
 patients and methods from june 1989 to june 1999 , 28 patients with localized soft tissue sarcoma of the extremity without evidence of distant disease received iort as part of an interdisciplinary treatment protocol of the departments of radiation oncology , orthopedic surgery and plastic surgery . 
iort was applied in patients in whom close or positive margins were expected , in recurrent tumors or tumors adjacent to joints with the aim of extremity - preserving treatment . 
patient demographics , tumor characteristics , treatment factors , and course of disease were evaluated retrospectively by reviewing the patients hospital files and interviewing the patients , their relatives and primary care physicians . 
 characteristics 56 ( 2084 ) age ( years ) mean ( range ) gender male female tumor primary locally recurrent histology malignant fibrous histiocytoma liposarcoma schwannoma synovial sarcoma fibrosarcoma leiomyosarcoma extraosseous osteosarcoma chondrosarcoma t - stage tumor volume ( ml ) median ( range ) grade unknown surgical margins microscopically negative microscopically positive ( < 2 mm ) macroscopically positive 119 ( 42 , 153 ) 10.5 the most common histological subtype was malignant fibrous histiocytoma ( eleven patients )  . 
 between 1989 and 1993 , 16 patients received iort with a moulage technique ( flab method ) , a high - dose - rate afterloading technique developed in our department . 
for an optimal dose distribution , close contact of the flab with the tumor bed was mandatory with regard to the steep dose fall - off . this technique is different from intraoperatively placed plastic catheters which are loaded postoperatively [ 4 ]  . 
 iort doses were 1215 gy with a mean of 14.5 gy , calculated to the flab surface ( 15 gy at flab surface correspond to approximately 10 gy at 5 mm tissue depth ) or the 90% isodose , respectively . 
25 patients received postoperative radiotherapy with a mean of 50.6 gy ( range : 30.660 gy ) within a mean of 39 days ( range : 2183 days ) after surgery and iort . three patients did not receive any ebrt . 
in two patients this was due to previous treatment with 60 gy to the primary tumor site ; one patient underwent compartment resection and no further treatment was considered necessary . 
 follow - up and statistics the time of follow - up was calculated from the end of the entire treatment , i.e. , the last day of ebrt or the day of surgery and iort . 
 5 - year actuarial rates for local disease - free survival , overall survival and overall distant disease - free survival were evaluated using the kaplan - meier method with calculation of the 95% ci . 
statistical differences in local recurrences as well as differences in survival rates were tested with the log rank . p - values were two - sided ; a p - value < 0.05 was considered statistically significant . 
 results local control and survival the actuarial 5 - year overall and distant disease - free survival rates are 66% ( 47% , 85% ) and 54% ( 34% , 74% ; figure 1 ) , respectively . 
6 urban & vogel the overall actuarial recurrence rate after 5 years is 16% ( 1% , 31% ) and after 8 years 24% ( 4% , 44% )  . 
 patients with t1 tumors exhibited a borderline significant ( p = 0.053 ) better distant disease - free survival ( 83% ) compared to t2 tumors ( 43% ) without any statistically significant difference in overall survival ( table 3 )  . 
 as for late side effects , evaluable in 21 patients , eight presented with grade 12 contracture , eleven with grade 12 pain , one with neuropathy , and two with pathologic fractures . 
 one patient suffering a neuropathy and a pathologic fracture was an 84 - year - old woman with a recurrent tumor of the distal upper extremity , who declined an amputation and in 0 12 24 36 48 60 72 84 96 108 120 132 144 months pts . 
the second patient with a pathologic fracture was a 60 - year - old man , also with a recurrent distal upper extremity tumor , who underwent a compartment resection and received 15 gy intraoperatively and 60 gy ebrt . 
 side effect grade impaired wound healing acute lymphedema skin reactions chronic lymphedema fibrosis contracture contracture pain neuropathy pathologic fractures functional outcome the function of the treated extremity could be judged in 22 patients . 
eight patients ( 36% ) had no functional limitations , neither recreational nor occupational , and were able to participate in prolonged activities , i.e. , going on longer hiking tours , skiing , swimming , etc . 
five patients ( 23% ) with minor restrictions required infrequent support in daily life . nine patients ( 41% ) showed limitations necessitating regular help in daily life , i.e. , orthotic devices ( walking canes or braces ) or assistance for tasks like buttoning , writing , or lifting . 
 [ 19 ] recently published results of a prospective study of 39 patients with soft tissue sarcoma treated with the same flab technique intraoperatively , combined with preor postoperative ebrt . 
 after limb - sparing surgery with intraoperative brachytherapy or intraoperative electron - beam radiotherapy and ebrt , local control rates of 90100% have been reported [ 1 , 6 , 7 ]  . 
 [ 26 ] found 36% skin reactions , especially associated with application of chemotherapy , 6% bone fractures , 20% contractures associated with joint irradiation , 7% pain requiring narcotics , 19% edema ( grade 2 + ) , and 57% tissue indurations . 
 [ 20 ] found 72% of patients with significant limitations in joint movement , 65% suffering from moderate pain requiring no or low - dose analgetic treatment , 39% swelling of the leg , and 69% fibrosis depending on radiotherapy dose and treatment volume . 
 in two older patients , a pathologic fracture developed after periosteal excision with or without partial bone resection . this phenomenon is attributed to both periosteal excision and radiation compromising vascularity and removing osteoprogenitor cells . 
the incidence of neuropathy described in the literature is 212% with 7% after surgery alone [ 2 ] , 23% after surgery and ebrt [ 3 , 14 ] , 7% after surgery and adjuvant brachytherapy [ 2 ] , and 412% after surgery , iort and ebrt [ 6 , 7 ]  . 
due to the small number of patients and the insufficient or nonuniform description of side effects in other studies , however , the comparison with published data of the incidence of late side effects is difficult . 
 acknowledgment this paper is dedicated to our former colleague rolf stepan ( deceased ) , who built up the intraoperative radiotherapy facility and was involved in most of the radiation treatments . 
greiner1 background and purpose : analyses of permanent brachytherapy seed implants of the prostate have demonstrated that the use of a preplan may lead to a considerable decrease of dosimetric implant quality . 
preplans were compared with the respective postplans assessing the following parameters : coverage index , minimum target dose , homogeneity index , and dose exposure of organs at risk . the prostate geometries ( volume , width , height , length ) were compared as well . 
 results : at the first brachytherapy , the matching between the preplan and actual implant geometry was sufficient in 47% of the patients , and the preplan could be applied . 
 key words : hdr brachytherapy preplan implant quality prostate cancer strahlenther onkol 2004 ; 180 : 3517 doi 10.1007 / s00066 - 004 - 1225 - 2 anwendbarkeit und dosimetrische konsequenzen des ultraschallbasierten preplanning in der hdrbrachytherapie des prostatakarzinoms hintergrund und ziel : die anwendung eines preplan bei der prostata - brachytherapie mit radioaktiven seeds geht hufig mit einer relevanten abnahme der dosimetrischen qualitt des implantats einher . 
die implantatqualitt nahm deutlich 1 department of radiation oncology with division of medical radiation physics , university of bern , inselspital , bern , switzerland , 2 department of urology , university of bern , inselspital , bern , switzerland , 3 kantonsspital , lucerne , switzerland . 
preplanning in hdr brachytherapy of the prostate ab ( tabelle 1 ) : der mittlere coverage - index sank um 0 , 11 , die mittlere target - dosis um 0 , 15 , der mittlere homogenittsindex um 0 , 09 . 
die unterschiede der geometrischen parameter waren betrchtlich ( 8 , 0 bis 13 , 8 cm3 betreffend volumen ; 1 , 1 bis 1 , 0 cm betreffend breite , hhe und lnge ; abbildung 2 und tabelle 3 )  . 
 schlsselwrter : hdr - brachytherapie preplan qualitt prostatakarzinom introduction clinical data have emerged suggesting that prostate cancer patients treated with radiation therapy have a significantly better outcome , when the dose to the gland is escalated [ 10 , 12 , 17 , 22 ]  . 
besides improvements in external - beam radiation techniques such as intensity - modulated radiotherapy , high - doserate ( hdr ) brachytherapy has been shown to be a valuable treatment technique for dose escalation to the prostate gland [ 10 , 11 , 18 ] : by placing hdr afterloading needles directly into the prostate under real - time transrectal ultrasound ( trus ) guidance , a steep dose gradient between the prostate and adjacent normal tissues can be generated . 
at the brachytherapy session , the patient along with the ultrasound probe have to be repositioned according to the preplan trus in order to reinstall the same ultrasound geometry . furthermore , the needles are to be positioned as accurately as possible according to the preplan . 
however , as it has been reported from analyses in permanent brachytherapy seed implants , the prostate geometry and the position of the needles may considerably deviate from the preplan , potentially leading to a substantial decrease of the dosimetric implant quality [ 3 ]  . 
 the aim of the present study was to analyze the applicability of preplanning in fractionated hdr brachytherapy of the prostate and its impact on implant quality , measured by parameters such as planning target volume ( ptv ) coverage index , minimal target dose , homogeneity index [ 9 , 21 ] , as well as dose exposure of organs at risk . 
 patients and methods patients and preplanning we analyzed 15 consecutive patients with intermediateor high - risk prostate cancer who had undergone combined radiotherapy : the external - beam radiotherapy was given in standard fractions of 2 gy during 5 weeks with a total dose of 50 gy ; hdr brachytherapy boost was concomitantly delivered in two separate fractions with a gap of 2 weeks ( for overview see figure 1 )  . 
the second implant was done either by use of a preplan based on the prostate contouring from the first implant session ( six patients ) or by use of the initial preplan based on the pretherapeutic trus ( not evaluated )  . 
the ptv was defined as the entire prostate without the central area around the urethra . needle positions were required to be located within the prostate and were defined on the basis of a typical u - like geometry as has been previously described [ 6 , 13 ]  . 
a preplan was generated using the geometric optimization option with manual geometric adjustments according to the following requirements : the prescribed dose to the ptv was 9.5 gy ; the maximally tolerated dose to the rectum was 6.65 gy ( 70% of prescribed dose ) and to the urethra 11.875 gy ( 125% of prescribed dose )  . 
the matching of the actual geometry with the preplan geometry was judged to be acceptable , when the following requirements were fulfilled : ( a ) change in prostate volume estimated to be < 15% , ( b ) deviation of the actual needle position from the planned position ( x / y grid coordinate system at reference plane ) < 5 min cases where the matching was acceptable , the applicators were immediately connected to the 192ir brachytherapy system ( nucletron ) , and radiation was delivered according to the preplan . 
preplanning in hdr brachytherapy of the prostate evaluation of plans in all patients which were treated with a preplan , a postplan was done to assess the real isodose distribution . 
to calculate the postplan , the actual implant geometry including prostate geometry and needle positions was assessed by trus and sent to the treatment planning systethe 192ir source dwell positions and dwell times were then manually entered as determined by the preplan . 
based on dose - volume histogram data , the quality of plans and implants was evaluated by use of the following indicators which were reported by other authors in the literature [ 9 , 21 ] : ptv coverage index , determining the fraction of the ptv receiving the prescribed dose ; minimum target dose , which represents the minimal dose found anywhere within the target ; homogeneity index , determining the fraction of the target volume receiving doses in the range of 1.01.5 times the prescribed dose . 
to assess dose exposure of organs at risk , the values of v70 of the rectum and of v125 of the urethra were determined along with the maximal dose ( dmax )  . 
 results applicability of preplans at the first brachytherapy , the matching between the preplan geometry and the actual geometry was judged to be sufficient in seven out of 15 patients ( 47% ) and the preplan was applied ( figure 1 )  . eight out of 15 patients ( 53% ) were treated by on - line planning at the first brachytherapy . 
at the second brachytherapy , the matching between the preplan based on the first implant and the actual implant geometry was judged to be sufficient in all six patients ( 100% )  . changes of parameters of dosimetric implant quality the mean coverage index of the preplans for the first brachytherapy was 0.81 ( table 1 )  . 
the mean coverage index of the respective postplans decreased to 0.70 , the average difference being 0.11. this impairment of the implant quality was evident also in terms of the minimum target dose , which decreased at an average of 0.15 , and with respect to the mean homogeneity index , which was reduced at an average of 0.09. 
flow chart of the planning procedure for two high - dose - rate ( hdr ) brachytherapy implants in combination with external - beam radiation therapy ( ebrt )  . 
for the second brachytherapy implant , patients were either treated by use of a preplan based on the trus from the first implant session as indicated , or by use of preplan based on the pretherapeutic trus ( not shown )  . 
anlsslich der zweiten brachytherapiesitzung wurden die patienten entweder mittels eines preplans , der auf der ersten brachytherapiesitzung basierte , wie angegeben , oder mittels eines preplans bestrahlt , der auf dem prtherapeutischen trus beruhte ( nicht gezeigt )  . 
there was a trend toward an overall increase in the prostate volume between the pretherapeutic trus and the first brachytherapy ( mean absolute increase 3.2 cm3 , mean relative increase 9% ; table 3 )  . 
the individual differences of the three dimensions were considerable , ranging from a few millimeters up to 1 cthis is also illustrated in figure 2a , where contours from each trus ( pretherapeutic , first and second implant session ) are superimposed . 
according to the selection criteria for acceptance or rejection of geometry matching , the changes in dimensions were much more pronounced among the patients who were treated with an on - line plan . 
due to its high conformality , it allows one not only to increase the total dose , but also to shorten the overall treatment time by use of large single doses in parallel to external - beam radiation therapy . many centers split the dose delivered by hdr brachytherapy to two or three fractions in order to reduce toxicity [ 1 , 6 , 10 , 18 ]  . 
preplanning based on a pretherapeutic trus examination has been proposed to be helpful in this regard by two main reasons : ( a ) by temporal splitting of the preplan calculation from the actual implantation , the time spent within the surgery room may be reduced , potentially allowing to increase the number of patients being treated per day ; ( b ) pretherapeutic trus might allow to identify patients with unimplantable prostate and to spare them from undergoing unnecessary anesthesia . 
in order to reduce the probability of a major decrease of the dosimetric implant quality , we selected the patients undergoing preplan - based brachytherapy according to the matching of the preplan geometry to the actual prostate volume and needle positions . 
we assume that this was the case due to the relative stability of the distance between the rectum and the dorsal part of the prostate as well as due to our efforts to maximally spare the central area around the urethra . 
in a single patient , an increase of the v125 of urethra exposure by 0.34 did , however , occur , indicating that even overexposure of organs at risk is unpredictable in individual preplan - treated patients . 
 quality parameters ( coverage index , minimum target dose , homogeneity index ) between preand postplans were noticeably smaller ( around 50% less in average with a smaller range of individual differences ) in the setting of the second brachytherapy . 
moreover , in all six patients who were supposed to be treated with the preplan based on the first implant session , the matching criteria concerning prostate geometry and needle positions were fulfilled at the second brachytherapy . 
these results are consistent with the finding of some centers that trus under anesthesia facilitates reproduction of the position of the prostate in the subsequent brachytherapy [ 2 ]  . 
 given the result of a suboptimal implant dosimetry if preplanning is used in hdr brachytherapy , the question arises whether preplanning should be completely abandoned and replaced by on - line planning as it has been suggested for permanent brachytherapy seed implants [ 14 , 15 ]  . 
based on our and other institutions experience , the main problem in using a preplan is the need to reinstall the geometry of the planning ultrasound and reproduce the planned needle positions during implantation . 
 the decrease of dosimetric quality of permanent brachytherapy implants by use of preplanning has been attributed to several reasons including seed displacement [ 5 , 16 ] , changes of prostate volume [ 19 ] , and / or changes of prostate shape [ 3 ]  . 
even though the allowed deviations of needle positions were required to be < 5 mm in order to accept the use of the preplan , the deviations in the range of a few millimeters may have further contributed to the decrease of implant quality . 
selection of patients with severe pubic interference is claimed to be another argument to perform a pretherapeutic trus . indeed , in some patients it is impossible to reach an acceptable ptv coverage with the usual prescribed dose without excessive dose exposure of the urethra and / or the rectum . however , if hdr brachytherapy is implemented as a boost , the prescribed brachytherapy dose may be lowered in such cases along with an increase of the dose delivered by external - beam radiotherapy . 
this implies that patients with problematic conditions for optimal needle geometry may still receive a possibly reduced hdr brachytherapy boost and will not undergo spinal anesthesia in va therefore , pretherapeutic trus is not justified to spare unnecessary anesthesia . 
 conclusion we found that preplanning in hdr brachytherapy of the prostate is followed by a substantial decrease of dosimetric implant quality , specifically if the preplan is based on a pretherapeutic trus without anesthesia . 
we therefore propose to abandon pretherapeutic trus and to use intraoperative on - line planning based on the actual prostate geometry and needle positions at least for the first brachytherapy implant . 
preplanning in hdr brachytherapy of the prostate strahlentherapie und onkologie original article oxygenation of tumor recurrences following fractionated radiotherapy of primary tumors studies on the rhabdomyosarcoma r1h of the rat wolfgang kehrl1 , christoph sagowski2 , sren wenzel2 , friedrich zywietz3 background and purpose : tumor oxygenation is well recognized as a major factor of tumor response to radiotherapy . 
this observation has to be taken into account in cases of tumor recurrences where repeated radiotherapy , chemotherapy or combined treatment modalities are used . key words : rhabdomyosarcoma of the rat recurrence tumor oxygenation microvessel density strahlenther onkol 2004 ; 180 : 38390 doi 10.1007 / s00066 - 004 - 1224 - 3 oxygenierung von tumorrezidiven nach fraktionierter strahlentherapie . 
die oxygenierung wurde in r1h - tumoren vor und am ende der bestrahlung und in r1h - rezidiven gemessen ( abbildung 1 ) , wenn diese die gleiche gre wie 1 department of oto - rhino - laryngology , marienkrankenhaus hamburg , germany , 2 department of oto - rhino - laryngology , university hospital hamburg - eppendorf , germany , 3 institute of biophysics and radiobiology , university hospital hamburg - eppendorf , germany . received : august 25 , 2003 ; accepted : february 4 , 2004 strahlenther onkol 2004 no . 
whrend in primrtumoren ein medianer po2 von 17 7 mmhg gemessen wurde , betrug dieser in den tumorrezidiven nur 5 5 mmhg ( p < 0 , 05 )  . 
der prozentuale anteil der po2 - werte < 5 mmhg zeigte , dass die hypoxie in r1h - rezidiven signifikant grer war ( 58 5% ) im vergleich zu den unbestrahlten primrtumoren ( 22 4% ; tabelle 1 )  . 
dies knnte fr die behandlung von tumorrezidiven mit bestrahlung oder / und chemotherapie von bedeutung sein . schlsselwrter : rhabdomyosarkom der ratte rezidiv tumoroxygenierung gefdichte introduction it is well known that hypoxia of tumors is regarded as an important factor for radioresistance of tumors and , generally , of tumor response to radiotherapy [ 3 , 5 , 7 , 9 , 10 , 12 , 18 , 21 ]  . 
tumors tend to be anoxic as the result of a chaotic vascular network , showing poor patency and large temporal fluctuations of tumor blood flow [ 4 , 18 ]  . 
most experimental and human tumors therefore consist of varying proportions of hypoxic cells [ 6 , 8 , 13 , 23 , 26 , 28 , 30 ] , which are radioresistant . 
based on this limited knowledge about oxygenation in tumor recurrences after radiotherapy , it was the aim of the present study to investigate the oxygenation and changes in vascularization of recurrences of rat rhabdomyosarcomas , which had been treated with fractionated irradiation with a total dose of 75 gy prior to their recurrence . 
 material and methods tumor model the studies were performed on isotransplanted rhabdomyosarcomas r1h growing subcutaneously in the right flank of male adult wag / rijh rats ( 301 20 g )  . 
tumor volume ( vt ) was determined by measuring three orthogonal diameters a , b , and c and was calculated using an ellipsoid approximation : vt = / 6 ( a ( cid : 1 ) b ( cid : 1 ) c )  . 
 the studies had previously been approved by the hamburg ministry of health ethics committee , and were conducted in accordance with the german law for animal protection and the united kingdom co - ordinating committee on cancer research guidelines . 
 irradiation rats were anesthetized by intramuscular injections of xylazine ( 6 mg / kg body weight [ b.w. ] , rompun , bayer , germany ) in combination with ketamine ( 50 mg / kg b.w. , ketavet , parkedavis , germany ) and placed prone on a small temperaturecontrolled irradiation table ( 37 c )  . 
tumors were irradiated at a 60co radiotherapy facility ( gammatron 2 , siemens comp . , germany ) with a total dose of 75 gy , given in 30 fractions , five times a week , for 6 weeks . 
the radiation field was 3 ( cid : 1 ) 3 cm , the dose rate 1.0 gy / m measurement of tumor oxygenation oxygenation ( po2 ) of tumors and of recurrences was measured in anesthetized animals using o2 - sensitive needle electrodes ( outer diameter 350 m , diameter of the cathode 12 m ) and the eppendorf po2 histograph ( eppendorf nethler - hinz , hamburg , germany ) [ 22 ]  . 
to minimize the effects of anesthesia , the po2 measurements were carried out under controlled mechanical ventilation and continuous monitoring of hemodynamic parameters [ 22 , 31 ]  . after a preceding anesthesia with ketamine and xylazine ( see above ) , anesthesia was continued by an infusion of fentanyl strahlenther onkol 2004 no . 
 data evaluation pooled po2 histograms of the po2 measurements were used , from which the mean and median po2 and the relative frequency of the two lowest po2 classes ( 05 mmhg ) were obtained . 
 results irradiation figure 1 shows the relative changes in tumor volume of primary r1h tumors in the course of radiation treatment with a total dose of 75 gy and in the r1h recurrences . 
at the end of irradiation , a significant decrease in median tumor po2 ( 4 3 mmhg ) and an enhanced frequency of po2 values < 5 mmhg ( tumor hypoxia ) were ascertained ( figure 2b )  . 
oxygenation in tumor recurrences ( 0.050.1 mg / kg b.w. / h , fentanyl - janssen , janssen - cilag , germany ) and midazolam ( 0.91.8 mg / kg b.w. / h , dormicum , hoffmann - la roche , germany ) into the left femoral vein . artificial ventilation was at an inspired oxygen fraction ( fio2 ) of 33% maintaining the arterial po2 of the rats within the range of spontaneous breathing rats ( 98 29 mmhg ) [ 22 ]  . after the po2 measurements , arterial blood ( 60 l ) for blood gas analysis was taken ( chiron diagnostics 264 , bayer vital , germany )  . 
 the po2 measurements were carried out in seven to twelve radial tracks in each tumor with a step length of 0.7 mdepending on tumor size , 120200 po2 measurements were recorded . 
from the pooled histograms the following parameters were derived : the mean and the median po2 , and the relative frequency of po2 values falling in the two lowest classes ( 05 mmhg )  . 
 tumor histology and microvessel density tissue slices ( 2 mm ) of the equatorial plane of the r1h tumor were obtained , fixed in phosphate - buffered formaldehyde and processed using routine paraffin histology . 
mvd was determined by projecting the tissue section on a screen at a magnification of 40 and counting the events on the counting grid ( videoplan , mitsubishi company , japan )  . 
the mean distance a of the vessels was calculated with the formula given by lierse [ 17 ] : a = f / n , where a determines the distance from the middle of one blood vessel to the other , f calculates the scored days after start of irradiation figure 1 . 
relative nderungen des tumorvolumens von rhabdomyosarkomen r1h der ratte whrend und nach fraktionierter 60co - ( cid : 2 ) - bestrahlung ( 75 gy / 30 fraktionen / 6 wochen ) und den rezidiven ( vo = 3 , 1 0 , 5 cm3 ; n = 27 , mittelwerte sem )  . 
in tumor recurrences the number of po2 values < 5 mmhg was significantly increased to 58 5% in comparison to 22 4% in the primary tumors ( figure 3 )  . 
the lower median tumor po2 and the high frequency of po2 values < 5 mmhg clearly demonstrated a much poorer oxygenation in the recurrences as compared to the primary tumors . 
the status of oxygenation in the recurrences appears to be comparable to the tumor oxygenation of primary tumors after a radiation dose of 75 gy , although the tumor sizes differ considerably ( table 1 )  . 
 histomorphological findings figure 4 shows the morphological changes in the tissue of r1h rhabdomyosarcoma before , at the end of irradiation ( 75 gy ) , and in the r1h recurrence . 
the structure of blood vessels is very heterogeneous , with vessel diameters varying from tiny capillaries to blood vessels of sinusoidal type . after completion of irradiation ( figure 4b ) , the tumor tissue shows histopathomorphological signs of severe cellular damage as well as a high fraction of pleomorphic cells , cells with enlarged nuclei , and pyknotic cells . 
6 urban & vogel figure 2a abbildung 2a tumor po2 ( mmhg ) figure 2b abbildung 2b tumor po2 ( mmhg ) figure 2c abbildung 2c tumor po2 ( mmhg ) figures 2a to 2c . 
median tumor po2 ( dark columns ) and frequency of po2 values < 5 mm hg ( white columns ) of primary rhabdomyosarcomas r1h before and after irradiation , and of r1h recurrences . 
medianer tumor - po2 ( schwarze sulen ) und hufigkeit von po2 - werten < 5 mm hg ( weie sulen ) von primren rhabdomyosarkomen r1h vor und nach bestrahlung sowie von r1h - rezidiven . 
 r1h primary tumors r1h primary tumors after 75 gy r1h recurrences figure 3 abbildung 3 mvd was assessed in the periphery and center of primary r1h tumors before irradiation , at the end ( 75 gy ) , and of r1h recurrences . 
tumor oxygenation ( po2 ) and frequency of po2 values < 5 mm hg in primary rat rhabdomyosarcomas r1h before , after irradiation with 75 gy of 60co ( cid : 2 ) - rays , and in r1h recurrences , measured with the eppendorf po2 histograph . 
tumoroxygenierung ( po2 ) und hufigkeit der po2 - werte < 5 mm hg in primren rhabdomyosarkomen r1h der ratte vor und nach bestrahlung mit 75 gy 60co - ( cid : 2 ) - strahlen sowie in den r1h - tumorrezidiven , gemessen mit dem eppendorf - po2 - histographen . 
mikrogefdichte ( mvd ) und mittlerer gefabstand in primren und bestrahlten rhabdomyosarkomen r1h ( 75 gy ) sowie in tumorrezidiven r1h , bestimmt in peripheren und zentralen arealen des tumors . 
lichtmikroskopische aufnahmen von tumorgewebe aus der peripherie von primren rhabdomyosarkomen r1h und nach bestrahlung ( 75 gy ) sowie von r1h - rezidiven ( vergrerung 100fach , hale )  . 
c : tumorkapsel ; n : nekrose ; v : blutgef . r1h with those of r1h recurrences occurring after a conventional fractionated irradiation with a total dose of 75 gy . 
as far as the distance of tumor blood vessels is concerned , r1h recurrences show a greater distance between the blood vessels than primary r1h tumors ( table 2 )  . 
the higher vascularization of the recurrences in comparison to the irradiated tumors is an indication for the regrowth of the recurrences , though the vascularization does not achieve the level of the primary tumors . 
 so far , our findings of r1h recurrences are in agreement with the results of pelvic recurrences [ 11 ] , although big differences between human cervical tumors and rat rhabdomyosarcomas exist . 
the very rapid cell proliferation in experimental tumors may occur in excess of the development of tumor vascularization giving rise to hypoxia , whereas this imbalance may be less pronounced in human tumors with a slow growth rate . 
 our previous studies on r1h tumors have shown that tumor oxygenation in experimental tumors strongly depends on tumor size [ 22 , 24 , 25 , 27 , 36 ]  . 
since in this study r1h primary tumors and recurrences were of comparable size at the time of measurement , the impact of tumor volume can be excluded to have an influence on oxygenation . therefore , the differences in oxygenation can be attributed to variations in tumor morphology and pathophysiology between primary tumors and recurrences . 
 the morphological investigations by lightmicroscopy have shown that r1h recurrences have a modified angioarchitecture in comparison to primary tumors showing greater variations among the blood vessels in regard to length , dilatation , and vascular density . 
if larger intercapillary distances are present , a reliable evidence of insufficient tumor oxygenation has to be expected . moreover , a lower vascular density , a lower tumor oxygenation and the tumor bed effect [ 2 , 13 , 17 , 32 , 33 ] might explain the slower growth of the r1h recurrences in comparison to the primary tumors . 
again , our findings on mvd and intercapillary distance can only broadly be compared outline with those described for various human neoplasms [ 1 , 16 ] , bearing again in mind the differences between experimental and human tumors . 
in this context , our study again stresses the importance of the vascular density as a putative variable that may affect the results of clinical trials in the outcome of radiation treatment . 
 conclusion our study has shown that recurrences of r1h rhabdomyosarcomas occurring in the radiation field show higher grades of hypoxia and lower levels of vascularization in comparison to primary r1h tumors of the same size . 
jereczek - fossa1 , anna morra1 , filippo debraud2 , daniela alterio1 , chiara mazzetta3 , andrea rocca2 , gianpiero catalano1 , livia bianchi1 , marcella pasetti1 , fausto chiesa4 , roberto bruschini4 , roberto orecchia1 , 5 background : despite numerous randomized trials suggesting a benefit of unconventional fractionation in locally advanced head and neck cancer , the role of this approach in nasopharyngeal carcinoma is debatable . 
irradiation was delivered using a shrinking - field technique up to a total dose of 74.4 gy in 62 fractions of 1.2 gy twice daily ( minimum 6 - h interval ) / 5 days / week . 
at 6 weeks after completion of radiotherapy , complete response was seen in 35 patients ( 81% ) , partial response in five ( 12% ) , stable disease in one , and progressive disease in two . 
 conclusion : hyperfractionated radiotherapy seems a feasible and active regimen in locally advanced nasopharyngeal carcinoma . accompanying acute and late toxicity is acceptable and does not compromise delivery of the planned irradiation dose . 
this regimen is associated with a high local control rate ; relatively high nodal and distant failure , however , call for further treatment modifications , e.g. , optimization of irradiation technique and / or dose escalation as well as improved systemic therapies . 
 key words : nasopharyngeal carcinoma radiotherapy hyperfractionation altered / unconventional fractionation chemotherapy strahlenther onkol 2004 ; 180 : 42533 doi 10.1007 / s00066 - 004 - 1202 - 9 hyperfraktionierte strahlentherapie bei lokal fortgeschrittenem nasopharynxkarzinoeine analyse von 43 patienten hintergrund : obwohl zahlreiche randomisierte studien zugunsten unkonventioneller fraktionierungsschemata bei lokal fortgeschrittenenen kopf - hals - tumoren sprechen , ist der stellenwert dieses vorgehens beim nasopharynxkarzinom umstritten . 
auf der basis gngiger klinischer erfahrung fhrten die autoren die hyperfraktionierte bestrahlung in die therapie lokal fortgeschrittener kopf - hals - tumoren , einschlielich nasopharynxkarzinome , eerste ergebnisse dieses therapieansatzes bei patienten mit nasopharynxkarzinom werden vorgestellt und insbesondere grenzen des verfahrens und seine toxizitt diskutiert . 
 1 department of radiation oncology , european institute of oncology , milan , italy , 2 department of medical oncology , european institute of oncology , milan , italy , 3 department of epidemiology and biostatistics , european institute of oncology , milan , italy , 4 department of head and neck surgery , european institute of oncology , milan , italy , 5 faculty of medicine , university of milan , italy . * presented in part at the xith annual conference of the italian association of radiation oncology ( airo ) , grado , italy , 2001 , and at the annual conference of the american association of clinical oncology ( asco ) 2003 . 
die strahlentherapie wurde im rahmen einer shrinking - field - technik bis zu einer gesamtdosis von 74 , 4 gy in 62 fraktionen mit 2 ( cid : 1 ) tglich 1 , 2 gy ( minimum 6 - h - interval ) an 5 tagen pro woche durchgefhrt . 
6 wochen nach abschluss der strahlentherapie , wurde eine komplette remission bei 35 patienten ( 81% ) beobachtet , partielles ansprechen bei fnf ( 12% ) , krankheitsstillstand bei einem und fortschreiten der erkrankung bei zwei patienten . 
in the last decades , several innovative treatment strategies have been investigated including irradiation and comcomitant chemotherapy [ 2 , 68 , 11 , 12 , 21 , 26 , 29 , 43 , 44 , 54 ] as well as altered fractionation of radiotherapy [ 3 , 9 , 28 , 29 , 34 , 35 , 38 , 42 , 6670 ]  . 
unlike other locally advanced head and neck cancers where altered regimens have been widely tested within large prospective phase iii trials [ 18 , 22 , 23 , 49 , 53 , 56 , 59 ] , reports on altered fractionation in nasopharyngeal carcinoma are scarce . 
 patients and methods between december 1996 and november 2002 , 43 patients with locally advanced nasopharyngeal cancer were treated with hyperfractionated radiotherapy at the european institute of oncology , milan , italy . 
pretreatment staging included chest x - ray or computed tomography ( ct ) , abdominal ultrasound examination or ct scan , bone scan , and primary tumor evaluation with clinical examination including fiber optic endoscopy and ct or magnetic resonance imaging ( mri )  . 
 hyperfractionated radiotherapy was delivered in two daily fractions of 1.2 gy at an interval of at least 6 h , for 5 days a week without any interruptions being planned . 
the planned total dose to the tumor / involved lymph nodes was 74.4 gy in 62 fractions , prescribed to the icru ( international committee of radiation units ) reference point ( in case of complete remission of lymph nodes , a 10% reduction of the dose to nodal areas was permitted )  . 
bilateral electron fields ( 69 mev ) were used to deliver a boost of up to 52.8 gy to the posterior cervical lymph nodes ( in case of elective irradiation )  . 
the maximum total doses to the spinal cord and optic nerves were set at 42 and 50 gy , respectively , the maximum total dose to the brain stem at 50 gy ( or 60 gy to a very limited volume )  . 
the lower cervical and supraclavicular lymph nodes were treated with an anterior photon beam up to 50 gy prescribed at a depth of 3 celective irradiation of strahlenther onkol 2004 no . 
all areas including tumor and involved lymph nodes were irradiated using two fractions a day . in all patients , head immobilization ( with mask ) , simulation of all treatment phases and fields , orthogonal laser beams ( to ensure positioning reproducibility during simulation , dosimetric ct scan and therapy ) , ct - based treatment planning ( cadplan , ct scan with 0.5 - cm slice thickness ) , beams eye views ( bevs ) , customized shielding / multileaf collimator , half - beam blocks for field matching , in vivo dosimetry , and electronic portal verification were employed . 
chemotherapy was administered at the discretion of treating physician / team ( in general , chemotherapy was not performed in patients with an early stage of disease ; of nine patients who did not receive chemotherapy , five were in stage ii and four in stage iii / iv )  . 
in two of these patients , fbec was administered as second - line therapy , because they did not respond ( stable disease ) to two cycles of cf regimen , and in the other two patients , fbec was the only induction chemotherapy performed . 
all examinations were also performed 6 weeks after the completion of radiotherapy and then according to the follow - up schedule ( at 2or 3 - month intervals in the following 2 years , and every 4 months thereafter )  . 
all patients were to be followed up by a multidisciplinary tea clinical examination including fiber optic endoscopy was performed at every follow - up visit , whereas radiologic evaluation was undertaken 6 weeks after the completion of radiotherapy and every second visit thereafter . 
regarding mucositis , rtog grade 3 is defined as confluent fibrinous mucositis which may cause severe pain requiring narcotics , and grade 4 as ulceration , hemorrhage , or necrosis . 
for statistical analysis , tumor grade ( as described in the pathologic report ) was classified into 23 versus 4 and tumor stage into ii and iii versus iv . given the small number of patients available , the association between factors at baseline was assessed through fishers exact test , and confidence intervals for proportions were built using the exact binomial distribution . 
duration of follow - up , time to progression , and survival time were calculated from the beginning of therapy until the last observation , progression and death / last observation , respectively . 
 results we analyzed a total of 43 patients , 34 males and nine females , with a median age of 51 years ( range , 1576 years ; table 1 )  . only five patients ( 12% ) had a karnofsky score < 90 . 
in two cases radiotherapy was completed at lower doses , and the patients were hospitalized due to severe acute toxicity ( grade 4 mucositis and pneumonia ) and deterioration of general status / concomitant disorders , respectively . 
in three cases radiotherapy was interrupted for 2 , 2 , and 7 days , respectively , due to acute toxicity ( grade 3 subclinical hypothyroidism hypoacusis chronic otitis media caries / parodontopathy mandible rarefaction dysgeusia a assessed in 41 patients b pretreatment hypoacusis present in two cases or 4 mucositis associated with weight loss )  . 
to control mucositis - related pain , oral morphine and percutaneous fentanyl were administered to three and one patient , respectively ( once , morphine was introduced before irradiation to control tumorrelated pain )  . 
 late toxicity was evaluated in 41 patients with a follow - up > 3 months after treatment ( one patient died 10 days after irradiation due to disease progression , and only a 2 - month follow - up is available in one patient )  . 
 response to treatment and pattern of failure of the 34 patients who underwent induction chemotherapy , five ( 15% ) achieved a complete ( 95% confidence interval [ ci ] , 531% ) and 25 ( 74% ) a partial response ( 95% ci , 5687% ) , four ( 12% ) had stable disease ( 95% ci , 327% )  . 
 the global response ( assessed at 6 weeks after the completion of radiotherapy ) included complete response in 35 patients ( 81% ; 95% ci , 6792% ) , partial response in five ( 12% ; 95% ci , 425% ) , stable disease in one , and progressive disease in two patients . 
primary tumor progression was observed in three patients ( in all cases an initial t4 stage was diagnosed ) , and seven patients each showed regional lymph node progression and distant metastases . 
all but one patient with exclusive neck relapse have been alive with no evidence of disease at a median of 16 months ( range , 119 months ) from the diagnosis of progression . 
in two cases external - beam irradiation was performed ( 30 gy and 39.6 gy , respectively ) and in one case highdose - rate brachytherapy up to 24 gy ( prescribed at 10 mm from the applicators ) in six fractions . 
of the two patients treated with external - beam irradiation , one is alive with no evidence of disease at 29 months , and one died of disease 18 months after reirradiation . 
one patient with metastatic failure is alive with no evidence of disease 33 months after chemotherapy , surgical removal of liver metastasis , and radiotherapy for subsequent paraaortic lymph node metastases . 
 survival after a median follow - up of 32 months , 30 patients ( 70% ) have been alive and free of disease ( n = 8 after salvage therapy )  . 
median values for both outcomes have not been reached ; after 2 years , however , the estimated proportion of patients without progression was 58% ( 95% ci , 4476% ) and of patients alive 84% ( 95% ci , 7397% )  . 
 when fitting a cox model , after adjusting for age and treatment , no patient - , tumorand treatment - related factor was associated with time to progression or overall survival . 
reports on accelerated / hyperfractionated radiotherapy schedules [ 3 , 35 , 42 , 68 , 69 ] , show promising results , yet at the expense of increased acute and late toxicity rates . 
theoretically , pure hyperfractionation should increase the therapeutic ratio of irradiation by exploiting the difference in the / ( cid : 2 ) - ratio of tumor / acute - reacting tissues and of latereacting tissue ( including nervous tissue )  . 
however , both groups ( conventional and twice - daily ) had a similar incidence of late complications , except for three cases of temporal lobe necrosis in the twice - daily group treated with 1.6 gy per fraction ( accelerated hyperfractionation )  . in our patients , like in those treated with the same regimen by jenet al . 
 [ 28 ] , no severe late neurologic complication occurred . the low dose per fraction , generous interfraction interval and use of 3 - d conformal technique seem essential to limit late neurologic toxicity accompanying hyperfractionated regimens for nasopharyngeal carcinoma [ 33 , 34 , 38 ]  . 
 [ 65 ] reported a significantly increased neurologic toxicity rate ( temporal lobe , cranial nerves , optic nerve / chiasm , and brain stem / spinal cord ) in patients treated with a 2 - d irradiation regimen employing two daily fractions of 1.6 gy 4 h apart . these complications have also been described in other studies figure 2 . 
 of accelerated radiotherapy with multiple daily fractions [ 22 , 34 ] , but not with accelerated schedules of six daily fractions per week [ 35 ] or with pure hyperfractionation [ 67 ]  . 
literature data show that the brain may be very sensitive to a change in fraction size , and the / ( cid : 2 ) - ratio for brain necrosis may be considerably less than 3 gy [ 27 ]  . 
 the results of salvage therapies following radiotherapy for nasopharyngeal carcinoma are not satisfactory [ 30 , 35 , 40 ]  . moreover , locoregional failure is associated with an increased risk of systemic failure [ 31 ]  . 
in the retrospective comparison by jen et al . [ 28 ] , the overall locoregional control rate was nonsignificantly higher with hyperfractionation than once - daily irradiation ( 83% and 67% for the twiceand once - daily group , respectively )  . 
according to the authors , a sample size of 140 patients for both the twiceand the once - daily groups is needed to detect a 10% difference in locoregional control favoring the twice - daily group . 
numerous authors report a better target / normal tissue dose distribution using intensity - modulated radiation therapy ( imrt ) , stereotactic irradiation ( srt ) , or two - step intensity - modulated arch therapy ( two - step imat ) [ 4 , 5 , 16 , 20 , 24 , 41 , 47 , 58 , 64 , 70 ]  . 
a brachytherapy ( brt ) boost is reserved to limited initial disease ( t1t2 tumors ) or very limited residual disease after externalbeam radiotherapy [ 39 , 41 ] , although some authors did not strahlenther onkol 2004 no . 
welldesigned prospective studies are warranted to clarify the role of innovative approaches in nasopharyngeal carcinoma . moreover , particular attention should be paid to the differences in histological types , ethnic composition and stage distribution , since treatment results may differ in function of these characteristics [ 10 , 61 ]  . 
 [ 14 ] , in a series of 447 nasopharyngeal cancer patients treated with conventional radiotherapy with or without chemotherapy , demonstrated that t - stage , total radiation dose and the use of chemotherapy were independent prognostic factors for local response , whereas age , t - stage , n - stage , radiation dose and chemotherapy were correlated with overall survival . 
similarly , other investigators reported high rates ( up to 30% ) of distant metastases even in the series with very high local control [ 14 , 29 , 37 , 62 ]  . 
however , the role of such an approach is still controversial , since a benefit of chemotherapy has only been demonstrated in two [ 2 , 43 ] of the ten randomized studies comparing chemoradiotherapy with irradiation alone [ 2 , 68 , 11 , 21 , 26 , 43 , 44 , 54 ]  . 
a recent meta - analysis of six randomized trials ( 1 , 582 patients ) has shown that addition of chemotherapy to standard radical irradiation for locally advanced nasopharyngeal carcinoma increases both disease - free and overall survival at 4 years by 35% and 21% , respectively , when compared to exclusive irradiation [ 25 ]  . 
in his excellent recent review , al - sarraf [ 1 ] suggests that the optimal results can be obtained by using total chemoradiotherapy ( induction chemotherapy followed by concomitant chemoradiotherapy )  . 
for example , use of conformal multiple photon beams has shown a better compliance with dose homogeneity requirements and a reduced risk of dose inhomogeneity related to field matching and patient positioning ( when compared to conventional technique of mixed photon and electron fields ) [ 13 , 17 ]  . 
satisfactory local control was observed ; the relatively high nodal and distant failure rates , however , indicate the need for further protocol modifications . these may include optimization of irradiation technique and / or dose escalation ( with use of imrt , srt etc . ) as well as administration of concomitant chemotherapy . 
 strahlentherapie und onkologie original article immediate postoperative radiotherapy or watch and wait in the management of adult low - grade glioma ? rolf - dieter kortmann1 , branislav jeremic2 , michael weller3 , johannes lutterbach4 , frank paulsen1 , michael bamberg1 background : the eortc trial 22845 on the role of immediate postoperative radiotherapy in patients with supratentorial lowgrade glioma revealed an advantage of immediate postoperative radiotherapy for progression - free survival , but not for overall survival . 
 material and methods : reports in the literature spanning 60 years of radiation therapy were reviewed with respect to timing of radiotherapy , prognostic factors , dose prescriptions , modern treatment techniques , and late effects . 
 conclusion : the arguments for immediate postoperative irradiation include : low - grade gliomas respond to radiotherapy ; the tumors often display an aggressive pathobiological behavior ; patients with high risk profile may benefit from immediate radiotherapy in terms of progression - free and overall survival ; modern focal radiotherapy is far less toxic than feared ; radiotherapy might be more effective at diagnosis than at progression . 
 key words : low - grade glioma adults radiotherapy chemotherapy neurosurgery late effects prognostic factors strahlenther onkol 2004 ; 180 : 40818 doi 10.1007 / s00066 - 004 - 1221 - 6 sofortige postoperative strahlentherapie oder abwartende haltung bei der behandlung niedrigmaligner gliome im erwachsenenalter ? hintergrund : die krzlich publizierte eortc - studie 22845 , die den stellenwert der sofortigen strahlentherapie bei patienten mit supratentoriellen niedrigmalignen gliomen randomisiert untersuchte , zeigte , dass die sofortige postoperative strahlenbehandlung einen vorteil fr das progressionsfreie berleben zeigt , dass sich dieser zugewinn jedoch nicht in einem vorteil bezglich des gesamtberlebens widerspiegelt . 
ist die chemotherapie eine ntzliche alternative ? material und methodik : literaturberichte , die 60 jahre strahlentherapie umfassen , wurden unter den aspekten zeitpunkt der radiotherapie , prognostische faktoren , dosisverschreibungen , moderne bestrahlungstechniken und sptfolgen analysiert . 
die strahlentherapie verursacht keine wesentlichen neurokognitiven strungen , vorausgesetzt , dass moderne bestrahlungstechniken und moderate dosisverschreibungen angewandt werden . neuere serien mit geringen patientenzahlen lassen vermuten , dass die chemotherapie nach dem pcv - schema oder mit temozolomid das mediane berleben verlngert und zumindest bei oligodendroglialen tumoren ansprechraten von 50% erreicht . 
 1 department of radiooncology , university of tuebingen , germany , 2 department of radiotherapy , klinikum rechts der isar , technical university of munich , germany , 3 clinic for neurology , university of tuebingen , germany , 4 department of radiation oncology , university of freiburg , germany . 
therapie niedrigmaligner gliome bei erwachsenen schlussfolgerung : die argumente fr eine sofortige postoperative strahlenbehandlung lauten : niedrigmaligne gliome sprechen auf bestrahlung an ; die tumoren zeigen hufig ein aggressives pathobiologisches verhalten ; patienten mit hochrisikoprofil werden von einer sofortigen strahlentherapie profitieren ; moderne lokale strahlentherapien sind deutlich weniger toxisch als von vielen autoren befrchtet ; die strahlenbehandlung knnte zum zeitpunkt der diagnose effektiver sedie chemotherapie ist mglicherweise eine alternative zur sofortigen postoperativen behandlungssituation . 
 schlsselwrter : niedrigmaligne gliome erwachsene strahlentherapie chemotherapie operation sptfolgen prognostische faktoren introduction the therapeutic strategies in adult low - grade glioma include surgery and radiotherapy , but also wait and see . 
the past 3 decades have provided increasing evidence that postoperative radiotherapy improves survival in subtotally resected low - grade glioma , but these data are mainly based on numerous retrospective reports ( tables 1 and 2 )  . 
the recently published eortc trial 22845 showed that immediate postoperative radiotherapy possesses an advantage in terms of progressionfree survival ; this benefit , however , did not translate into overall survival [ 22 ]  . 
are there any patient subgroups with a defined risk profile that will benefit from immediate treatment ( radiotherapy or chemotherapy ) in terms of progression - free and overall survival ? 2 . 
are the chances for a benefit from radiotherapy at progression worse in terms of decreased tumor and symptom control , and is radiotherapy associated with a higher risk of radiotherapy - induced acute and long - term side effects ( larger tumor burden leading to larger treatment fields and , consequently , to a higher proportion of patients with deficits ) ? timing of postoperative radiotherapy the outcome of surgery alone and surgery plus radiation therapy including patients treated between 1956 and 2002 is summarized in tables 1 and 2 . 
although not specifically addressing the problem , several retrospective studies have indicated an advantage for immediate postoperative radiotherapy regarding overall survival and progression - free survival [ 15 , 29 , 30 , 57 , 60 ]  . 
in several other series comprising varying patient numbers and in which postoperative radiotherapy was retrospectively compared with no further treatment , overall survival rates ranged between 49% and 54% after radiotherapy and were superior to a wait and see policy with survival rates ranging from 21% to 32% at 5 years ( table 1 )  . 
observed 5and 10 - year survival rates for the irradiated group ( n = 101 ) of 60% and 41% , respectively . these were significantly better than those for the 18 patients treated with surgery alone ( 37% and 11% , respectively ; p = 0.048 ) [ 60 ]  . 
 author year patients ( n ) 5 - year survival ( % ) surgery surgery + rt 10 - year survival ( % ) surgery surgery + rt bouchard [ 3 ] stage & stein [ 65 ] leibel et al . 
 eortc / mrc study recently , preliminary results of an eortc / mrc study have shown that immediate postoperative radiotherapy in lowgrade glioma improved progression - free survival over that seen with observation only [ 22 ]  . 
 author year patients ( n ) 5 - year survival ( % ) surgery surgery + rt 10 - year survival ( % ) surgery surgery + rt chin et al . 
of 290 eligible and assessable patients , the irradiated group showed a significant ( p = 0.02 ) improvement in progression - free survival , but not in overall survival , with a median follow - up of 5 years . 
the 5 - year estimate was 63% versus 66% ( overall survival ) and 44% versus 37% ( time to progression ) for the treated and control arms , respectively . 
however , the results should be interpreted cautiously , as overall survival and progression - free survival may eventually become differentiated with longer follow - up , because these tumors are known to grow slowly . 
examined 139 patients [ 58 ] who received postoperative radiotherapy and found 5and 10 - year survival rates of 68% and 39% after higher doses ( > 53 gy ) , compared with 47% and 21% , after lower doses ( < 53 gy )  . whitton & bloom analyzed their data from 1960 to 1985 and found a trend toward improved survival for doses > 55 gy [ 74 ]  . a similar finding was also made by medbery et al . 
in the study of celli et al . on oligodendrogliomas , no difference in outcome was found for doses < 50 gy when compared to 50 gy [ 6 ] , which was confirmed by lindegaard et al . 
survival at 2 and 5 years was nonsignificantly better with low - dose radiotherapy ; it amounted to 94% and 72% , respectively , with low - dose irradiation and 85% and 64% , respectively , with high - dose radiotherapy . 
in a prospective phase ii study , hyperfractionated radiotherapy was investigated in a total of 37 adults , with histologically proven supratentorial low - grade ( grade ii ) glioma after incomplete resection [ 21 ]  . 
the results of this study compare favorably to those of other contemporary studies ( 7 - year survival : 69% ; 7 - year progression - free survival : 70% at median follow - up of 74 months )  . 
investigated the role of dose escalation with proton / photon radiotherapy in 20 patients with lower - grade gliomas in a prospective phase i / ii trial [ 12 ]  . 
therapie niedrigmaligner gliome bei erwachsenen the authors concluded that tumor recurrence was neither prevented nor noticeably delayed relative to published series on photon irradiation and that dose escalation failed to improve outcome . 
 response to treatment radiographically determined response to radiotherapy has not been well documented , because it has been assumed that low - grade gliomas are often indolent and unresponsive to radiotherapy . 
determined the rate of response of lowgrade ( who grade ii ) gliomas to radiotherapy and analyzed the relationship between radiographic response , symptom control and patient survival in 21 patients [ 2 ]  . 
retrospectively analyzed 379 patients and found that performance status , contrast enhancement on imaging , mental changes , and initial steroid dependence were significant independent prognostic factors , while histological subgroup , focal deficits , presence of seizures , prediagnostic symptom duration , tumor category , or tumor stage were not [ 34 ]  . 
although using different criteria , these observations were in part confirmed by grabenbauer et al . , who assessed clinically relevant prognostic factors in a retrospective series comprising 77 patients [ 16 ]  . 
univariate analyses identified the total radiation dose , duration of symptoms , the presence of seizures , and contrast enhancement on ct imaging as significant prognostic factors for overall survival . 
stable or decreasing uptake of 11c - methionine in tumor area after radiotherapy during follow - up seemed to be a favorable sign in a series of 14 patients in whom pet was investigated [ 42 ]  . 
on univariate analysis , age 1840 , presence of seizures at presentation , karnofsky performance status ( kps ) 70 , treating institution , and absence of contrast enhancement were associated with improved overall survival . 
in the prospective rtog study comparing two different dose prescriptions , multivariate analysis in 203 patients identified histological subtype , tumor size , and age as the most significant prognostic factors . 
 the eortc analyzed the data of 610 patients treated in their prospective trials in order to identify prognostic factors for survival in adults [ 22 , 23 , 46 ]  . 
a cohort of 322 patients who all received postoperative radiotherapy was investigated , and the results were validated against 288 patients in whom half of the patients received immediate postoperative radiotherapy . 
multivariate analysis showed that age 40 years , astrocytoma histology subtype , largest diameter of the tumor 6 cm , tumor crossing the midline , and presence of neurologic deficit before surgery were unfavorable prognostic factors for survival . 
an average ki - 67 value of 5% was prognostically significant for reduced cause - specific survival , and a level 10% was strongly significant of a poor survival outcome , but not for progression - free survival , and did not remain an independent statistically significant factor on multivariate analysis . 
used a three - tiered system to find progression toward higher grade in 33% of their cases , with an additional 38% of patients progressing to glioblastoma [ 39 ]  . 
a higher incidence of progression was noted in several other series , but mainly in those with up to only 25 patients [ 35 , 44 , 45 , 70 ] ( table 3 )  . 
observed a contrast enhancement of low - grade gliomas in ct in 22 of 24 patients ( 92% ) suggesting malignant transformation [ 37 ]  . of seven reoperated recurrences in this series , six ( 86% ) had progressed to highgrade malignancy . 
in the series of wallner et al . , six out of ten patients with pure oligodendrogliomas who underwent either surgical reresection or postmortem sampling , progressed to high - grade malignancy [ 73 ] , while in the series of nijjar et al . , progression of oligodendroglioma to glioblastoma occurred in eight of 22 patients ( 36% ) [ 40 ]  . a summary of these reports is given in table 3 . 
 [ 21 ] chemotherapy unlike in children , the role of chemotherapy in low - grade glioma is unclear , and data on efficacy are scarce and maintotal ly relate to oligodendroglial tumors and on the combination of procarbazine , lomustine ( ccnu ) , and vincristine ( pcv )  . 
treated nine symptomatic patients harboring low - grade oligodendroglioma with pcv ( eight at presentation and one was treated for a recurrence after radiotherapy had failed ) [ 36 ]  . 
nine adults with progressive oligodendroglioma were treated with carboplatin at a dose of 560 mg / m2 administered at 4 - week intervals in the series of friedman et al . 
investigated the clinical relevance of molecular genetic testing at the time of diagnosis for 50 patients with anaplastic oligodendrogliomas , treated with a chemotherapeutic regimen as the principal initial therapy [ 19 ]  . 
 patients ( n ) ( resection or biopsy ) progression patients with malignant transformation year 1975 1977 1984 1988 1989 1991 1992 1993 1993 1994 1996 1998 strahlenther onkol 2004 no . 
cr : complete remission ; nd : no data ; pcv : procarbazine , lomustine ( ccnu ) , vincristine ; pd : progressive disease ; pfs : progression - free survival ; pr : partial remission ; sd : stable disease . 
cr : komplette remission ; nd : keine angaben ; pcv : procarbazin , lomustin ( ccnu ) , vincristin ; pfs : progressionsfreies berleben ; pd : progrediente erkrankung ; pr : partielle remission ; sd : stabile erkrankung . 
 [ 4 ] 2003 carboplatin oligodendrogliomas ii oligodendrogliomas ii 17 oligodendropcv followed gliomas ii 11 oligoastrocytomas ii all subtypes by rt ( 54 / 59.4 gy ) temozolomide 8 / 9 sd 8 pr , 17 sd , 3 pd before rt quinn et al . 
 [ 49 ] 2003 11 cr , 17 pr , 16 sd median pfs 35 months median pfs 622 months 5 year os median 4.83 years median pfs 22 months 11.2 months alone or additional ccnu every 6 weeks . 
the disease was stable in 6466% of patients , and three patients ( 11% ) had disease progression . chemotherapy was followed by radiotherapy , and the 5 - year overall survival was 89% . 
the toxicity of this treatment was considerable : 75% of the patients had grade 3 or 4 neutropenia , and eight of 28 patients were unable to complete the protocol due to toxicity . 
the activity was assessed in larger series of patients with high - grade glioma and is currently under investigation in a randomized trial of the eortc [ 26 ]  . 
treated 46 patients with progressive low - grade glioma ( 16 astrocytomas and 20 oligodendrogliomas , five mixed gliomas , and five pilocytic astrocytomas ) with temozolomide and obtained 24% complete responses and 37% partial responses with 35% of patients having stable disease [ 49 ]  . 
toxicity was mild , and the authors concluded that this substance is active and tolerable . of note , 70% of these tumors showed contrast enhancement when temozolomide was started , suggesting a bias toward contamination by anaplastic lesions in that series . 
the role of temozolomide as primary treatment will be tested in a randomized setting against radiotherapy in a forthcoming eortc trial with respect to genetic subtypes for the group of oligodendroglioma . 
postirradiation changes include a wide spectrum of abnormalities from subclinical changes detectable only by mri to focal neurologic deficits and intellectual impairment due to brain necrosis or diffuse white matter injury , respectively . the risk of necrosis following radiotherapy is low when applying contemporary dose prescription . 
in the rtog study , 50.4 gy were compared with 64.8 gy using localized fields . radiation necrosis occurred in 1% and 5% of patients , respectively [ 56 ]  . 
observed radiotherapy - induced late effects in 28 long - term survivors who had received postoperative radiotherapy and were retrospectively compared with 23 patients who had undergone surgery alone [ 66 ]  . 
however , 19 of 28 patients received whole - brain irradiation with 40 gy followed by a boost to the tumor site up to a cumulative dose often > 60 gy . 
in the series of reijneveld et al . , 24 unoperated patients scored better on most quality - of - life items and functional status than 24 patients with surgically proven low - grade glioma [ 51 ]  . 
investigated 41 patients with low - grade glioma who underwent surgery , 20 of whom received additional immediate postoperative radiotherapy [ 68 ]  . none of the survivors had significant neurologic impairment when compared to control subject . 
these observations were confirmed by vigliani et al . who evaluated the effects of limited - field irradiation on cognitive functions in 17 patients as compared to 14 patients without radiotherapy [ 71 ]  . 
unlike in children , the presumed benign histological character of low - grade glioma is in sharp contrast to its biologically aggressive manner , despite surgery and radiotherapy and the absence of plateau in survival figures observed at long follow - up intervals [ 18 , 27 , 28 ]  . 
dose escalations do not add therapeutic efficacy [ 12 , 23 , 56 ] and are only associated with an increased risk for late neurotoxic side effects [ 24 , 56 , 66 ]  . 
 the role of postoperative radiotherapy now appears clearer following a report from the eortc study showing that an improvement in progression - free survival but not overall survival is obtained after immediate postoperative radiotherapy . 
given the eortc results demonstrating equivalent overall survival for both immediate and deferred radiation treatments , selecting the timing of radiotherapy on the basis of clusters of prognostic factors may be an attractive strategy [ 1 , 46 ]  . 
by contrast , among the unfavorable patients , immediate postoperative radiotherapy may be appropriate , as the disease may be expected to run a more aggressive course with a shorter expected interval to progression and shorter overall survival . 
the selection criteria for the forthcoming eortc trial are based on these experiences . preliminary data show that ccnu alone , pcv and temozolomide might be effective [ 8 , 9 , 26 , 36 , 69 ]  . 
therapie niedrigmaligner gliome bei erwachsenen arm a ( control arm ) : radiotherapy ( tumor site ) 50 gy , standard fractionation ( 1.672.0 gy fractions ) , conformal techniques [ 67 ]  . 
12 cycles * risk categories : requiring treatment as demonstrated by at least one of the following criteria : radiologically proven progressive lesion ; neurological symptoms others than seizures only ( focal deficits , signs of raised intracranial pressure , mental deficits ) ; intractable seizures ; age 40 years figure 1 . 
repeat biopsies are often not available at the time of clinical or radiographic progression , and , therefore , it is not known whether a lowor a high - grade tumor was treated , especially if contrast enhancement has appeared . 
 the studies in which adverse effects of radiotherapy were observed had used higher dose prescriptions and larger treatment fields , which are outdated today [ 43 , 66 ]  . 
 the dangers of deferring radiotherapy are largely unknown and the risk for severely compromising clinical conditions in case of progressive disease is often disregarded in the debate about timing of radiotherapy ( and chemotherapy , respectively )  . 
in a watch and wait strategy it can be assumed that these patients will be posed at a risk for a lesser chance of symptom and tumor control , if the tumor progresses early in the course of disease . 
 strahlentherapie und onkologie short communication iodine - 125 brachytherapy of brain stem tumors jen julow1 , rpd viola1 , 2 , tibor major3 , istvn vallik1 , sarolta sgi4 , lszl mangel3 , beta r . 
in case 1 , the tumor volume was 1.98 cm3 on the control ct , indicating a 65.5% shrinkage as compared to a target volume of 5.73 cm3 at the time of brachytherapy . 
after irradiation , the cyst volume was 0.16 cm3 on the control mri , indicating a 97.4% shrinkage as compared to a target volume of 6.05 cm3 at the time of brachytherapy , i.e. , the metastasis had virtually disappeared . 
 key words : brachytherapy brain stem tumors brain stem glioma 125i interstitial irradiation tumor shrinkage image fusion strahlenther onkol 2004 ; 180 : 44954 doi 10.1007 / s00066 - 004 - 1228 - z jod - 125 - brachytherapie von hirnstammtumoren ziel : beschreibung der interstitiellen jod - 125 - ( 125i - ) brachytherapie bei der behandlung von hirnstammtumoren . 
 schlsselwrter : interstitielle 125i - brachytherapie hirnstammtumoren schrumpfung fusionsbild introduction today , the treatment of brain gliomas is an interdisciplinary challenge [ 5 , 25 , 47 ] , and especially the cure of brain stem tumors proves to be a difficult task . 
johns hospital , budapest , hungary , 2 semmelweis university doctoral school , budapest , hungary , 3 department of radiotherapy , national institute of oncology , budapest , hungary , 4 department of radiology , st . 
johns hospital , budapest , hungary , 6 diagnostic and oncoradiologic institute , pannon university , kaposvr , hungary . received : august 18 , 2003 ; accepted : march 25 , 2004 strahlenther onkol 2004 no . 
surgical resection is the most efficient treatment for cervicomedullar cysts and exophytic tumors ; however , the 5 - year survival rates of 2343% in endophytic brain stem gliomas are mainly ensured by conventional fractionated radiation therapy [ 24 , 10 , 15 , 30 , 39 ]  . 
interstitial irradiation as a supplement to external irradiation dramatically improves the survival rate of patients with nonresectable low - grade brain stem gliomas which have been verified histologically [ 16 , 3339 ]  . 
 here , we report the results of iodine - 125 ( 125i ) interstitial irradiation in two patients with brain stem tumors ( one glioma and one carcinoma metastasis )  . 
due to an appropriate geometric arrangement of the sources , the three - dimensional isodose surface of the reference dose follows the tumor contours , even in irregularly shaped tumors . 
in april 1999 , the neurologic examination revealed a right - sided central paresis of the facial nerve , paresis of the trochlear nerve , and partial paresis of the oculomotor nerve . 
in april 1999 , following a stereotactic biopsy , which supported the presence of grade ii astrocytoma , a catheter was inserted into the tumor via a frontal drill hole , and its position was verified by intraoperative ct - ct image fusion ( figures 1a and 1b )  . 
within the mesencephalon , the black line contours the glioma ( a , b ) , while the white contour line marks the border of a necrotic cyst following irradiation ( b )  . 
brachytherapy of brain stem tumors ct and mri examinations confirmed a space - occupying lesion , 20 ( cid : 1 ) 20 ( cid : 1 ) 15 mm in size , localized in the pons . 
two catheters were inserted into the tumor via two frontal drill holes , and their position was verified by intraoperative ct - ct image fusion ( figures 2a to 2c )  . 
three - three 125i seeds with an activity of 3.7 mci each were placed in the two catheters without spacers . according to the treatment plan , 94% of the tumor ( 6.05 cm3 ) was irradiated with a dose of 54 gy . 
 the patients dysphagia , torpidity of palatal and pharyngeal reflexes had disappeared 2 months following irradiation . in march 2003 , the patients general state corresponded to 100 on the karnofsky scale . 
in november 2002 , the post - irradiation cyst volume measured on the control mri was 0.16 cm3 , indicating a 97.4% reduction of the target volume of 6.05 cm3 at the time of brachytherapy , i.e. , the metastasis had virtually disappeared . 
stereotactic biopsy , which is the basis of brachytherapy , proves a safe and minimally invasive intervention providing sufficient information for definitive diagnosis of brain stem tumors in 97% of cases ( table 1 ) [ 1 , 79 , 14 , 18 , 24 , 26 , 44 ]  . 
according to kondziolka & lunsford [ 24 ] , injury to brain vessels , hemorrhage after biopsy , and cranial nerve injuries can be avoided by keeping the biopsy needle away from the pial and ependymal surfaces and advancing with it intraparenchymally as long as possible . 
 radiation dose , patients age , and combination of different treatment modalities ( surgery , chemotherapy , immunotherapy , conformal external - beam irradiation , hyperfractionated radiation therapy , linac and gamma - knife stereotactic radiosurgery , conformal proton radiation therapy ) did not significantly influence the survival of patients with brain stem tumors ( table 2 ) [ 6 , 12 , 13 , 17 , 20 , 21 , 27 , 29 , 42 , 43 , 46 ]  . 
within a period of 2 years , the mortality rate is as high as 90100% in patients having diffuse brain stem gliomas treated with external - beam irradiation to a total dose of 54 gy [ 8 , 12 , 31 ]  . 
tc : transzerebellar ; tcla : transkoronal durch die achse des hirnstamms ; tcr : transkoronal ; tf : transfrontal . author ( year ) biopsies entry point of biopsies morbidity successful diagnosis ( n ) boviatsis et al . 
unwanted side effects ( vasogenic edema , radionecrosis of normal tissues ) can be prevented or reduced by precise dosimetry , cortisone therapy , and temporary implantation of catheters [ 37 , 3941 ]  . 
bt : brachytherapy ; cebrt : conformal external - beam radiation therapy ; ch : chemotherapy ; cprt : conformal proton radiation therapy ; gk : gamma - knife stereotactic radiosurgery ; hfrt : hyperfractionated radiation therapy : i : immunotherapy ; linac : linac stereotactic radiosurgery ; s : surgery ; wbrt : whole - brain irradiation . 
bt : brachytherapie ; cebrt : konformale teletherapiebestrahlung ; ch : chemotherapie ; cprt : konformale protonenbestrahlung ; gk : gamma - knife stereotaktische radiochirurgie ; hfrt : hyperfraktionierte strahlentherapie : i : immuntherapie ; linac : stereotaktische radiochirurgie mit dem linearbeschleuniger ; s : chirurgie ; wbrt : ganzhirnbestrahlung . 
a : astrocytoma ; aa : anaplastic astrocytoma ; cac : cystic adenocarcinoma ; hg : high - grade glioma ; lg : low - grade glioma ; pnet : primitive neuroectodermal tumor . 
a : astrozytome ; aa : anaplastische astrozytome ; cac : zystische adenokarzinome ; hg : high - grade - gliom ; lg : lowgrade - gliom ; pnet : primitiver neuroektodermaler tumor . 
 ( 1991 ) [ 39 ] hood & mckeever ( 1989 ) [ 19 ] 2 aa , 1 a median survival for 8 diffuse pontine tumors 8.4 months follow - up for 2 midbrain tumors > 40 months follow - up 18 months 192ir 29 125i , 26 192ir actual survival at 5 years after diagnosis 54.8% in 125i group , and 26.9% in 192ir group survival 7 , 8 , 10 months after brachytherapy matsumoto et al . 
 [ 32 ] performed 192ir interstitial irradiation ( with 30 gy marginal dose ) and linac boost therapy with 20 gy in a patient with an adenocarcinoma located within the mesencephalon . 
after an 18 - month follow - up period , the control mri examination showed stabilization of the tumor volume . this case suggests that brachytherapy can delay cyst recurrence , suppress tumor growth , and prolong survival in patients with cystic brain stem metastasis . 
if cytology proves the presence of a tumor , interstitial irradiation of the tumor can be performed during the same biopsy session , thus obviating the need for another stereotactic intervention . in agreement with the experiences of other brachytherapy centers ( table 3 ) , we recommend interstitial irradiation of primary infiltrating brain stem tumors and metastases . 
 strahlentherapie und onkologie review article radiotherapy for high - grade gliomas does altered fractionation improve the outcome ? carsten nieder1 , nicolaus andratschke1 , nicole wiedenmann1 , raymonde busch2 , anca l . 
grosu1 , michael molls1 background and purpose : the publication of radiation therapy oncology group ( rtog ) study 83 - 02 in 1996 stimulated further investigations of altered fractionation , i.e. , application of more than one fraction per day , in high - grade gliomas . 
 material and methods : to identify suitable trials , a medline search was performed by use of the following key words : brain tumors / astrocytoma / glioma / high - grade glioma / malignant glioma / glioblastoma multiforme and accelerated radiotherapy / hyperfractionated radiotherapy / altered fractionation . 
in addition , the search was extended to reference lists of articles and textbooks . whenever possible , data were extracted from the original papers on an intention - to - treat basis , i.e. , patients with protocol violations were not excluded for the purpose of this analysis . 
studies in brain stem gliomas , pediatric patients and studies which achieved acceleration by radiosurgery , stereotactic radiotherapy , or brachytherapy rather than conventional external - beam treatment were not included . 
the total number of 2 - year survivors was then calculated for each treatment strategy and compared by use of the ( cid : 1 ) 2 - test . results : the authors identified 1 , 414 patients from 21 studies ; two of these were randomized phase iii studies . 
none of the studies reported a significant improvement in survival by altered fractionation in comparison to either institutional historical controls or their respective randomized control ardoses of 6070 gy do not appear to improve survival compared to 5060 gy . 
 material und methodik : um entsprechende studien zu identifizieren , erfolgte eine medline - suche mit folgenden schlsselwrtern : brain tumors / astrocytoma / glioma / high - grade glioma / malignant glioma / glioblastoma multiforme und accelerated radio1 department of radiation oncology , klinikum rechts der isar , technical university of munich , germany , 2 institute for medical statistics and epidemiology , klinikum rechts der isar , technical university of munich , germany . received : august 7 , 2003 ; accepted : december 18 , 2003 strahlenther onkol 2004 no . 
wenn mglich , wurden die daten aus den originalarbeiten im sinne einer intention - to - treat - analyse extrahiert , d.h. , patienten mit protokollverletzungen wurden fr diese auswertung nicht ausgeschlossen . 
die gesamtzahl der 2 - jahres - berlebenden fr die verschiedenen therapieanstze wurde errechnet und mittels ( cid : 1 ) 2 - test verglichen . ergebnisse : die autoren identifizierten 1 414 patienten in 21 studien , darunter zwei randomisierte phase - iii - studien . 
die anderen studien sind sehr heterogen , da eine vielzahl von medikamenten und applikationsschemata benutzt wurde . sieben studien schlossen nur patienten mit glioblastoma multiforme ein , zwei nur patienten mit anaplastischen gliomen . 
die alleinige bestrahlung fhrte zu einer 2 - jahres - berlebensrate von 13% , die kombinierte radiochemotherapie oder die gabe sensibilisierender substanzen zu 23% ( p < 0 , 0001 )  . 
die studien zur konventionellen strahlentherapie plus chemotherapie oder radiosensibilisierung schlossen 1 115 patienten ein ( medianes berleben 11 monate , 2 - jahres - berlebensrate 18 , 5% )  . 
 schlsselwrter : strahlentherapie astrozytom gliom malignes gliom glioblastoma multiforme introduction despite considerable efforts , in the last years no clear trend toward improvement in outcome was achieved for high - grade gliomas [ 17 , 31 , 32 ]  . 
patients prognosis is mainly determined by several tumorand patient - related factors , whereas changes in treatment so far have contributed less than expected to increase median survival beyond approximately 912 months [ 20 ]  . 
the publication of radiation therapy oncology group ( rtog ) study 83 - 02 in 1996 suggested a therapeutic gain from altered fractionation , i.e. , application of more than one fraction per day , in high - grade gliomas and stimulated further investigations [ 37 ]  . 
whenever possible , data were extracted from the original papers on an intention - to - treat basis , i.e. , patients with protocol violations were not excluded for the purpose of our analysis . 
studies in brain stem gliomas , pediatric patients and studies which achieved acceleration by radiosurgery , stereotactic radiotherapy , or brachytherapy rather than conventional external - beam treatment were not included . 
for comparison , studies where conventional fractionation was used and which were published during the same time frame were selected ( tables 3 and 4 [ 4 , 5 , 7 , 8 , 13 , 18 , 22 , 26 , 35 , 36 ] )  . material and methods statistical methods to identify suitable trials , a search strategy was defined . 
the database medline was used by entering all possible combinations of one of the following key words : brain tumors / astrocytoma / glioma / high - grade glioma / malignant glioma / glioblastoma multiforme , with one of these key words : accelerated radiotherapy / hyperfractionated radiotherapy / altered fractionation . 
in addition , the search was extended to reference in order to decrease the confounding effects of additional use of chemotherapy and radiosensitizers , separate analyses were performed for groups with or without such treatment . 
cge : cobalt - gray - quivalent ; ecog : eastern cooperative oncology group ; gbm : glioblastoma multiforme ; kps : karnofsky - status ; rt : radiotherapie ; tesm : tumor + dem + sicherheitsabstand von cm ; wbrt : ganzhirnbestrahlung ; ? : daten lassen sich der originalpublikation nicht entnehmen . 
2000 [ 10 ] single institution phase ii single institution phase ii single institution phase ii single institution phase ii single institution phase ii single institution phase ii single institution phase ii single institution phase ii 51 20 eortc phase i / ii miralbell et al . 
 none of the studies reported a significant improvement in survival by altered fractionation in comparison to either institutional historical controls or their respective randomized control ardoses of 6070 gy do not appear to improve survival compared to 5060 gy . 
regarding 2 - year survival rates , radiotherapy alone resulted in 13% , combined chemoradiation or use of sensitizers in 23% ( p < 0.0001 ; table 5 )  . 
2001 [ 36 ] phase ii single institution phase ii 21 100 a 501 patients with an intended dose of 60 gy in 30 fractions , 135 patients with an intended dose of 45 gy , and 38 patients with an accelerated 55 - gy schedule as used by brada et al . 
the other authors did not evaluate this question . however , it must be noted that most of the studies started radiotherapy quite soon , i.e. , within 4 weeks from resection . 
 in our opinion , doses > 60 gy are not justified outside of well - defined clinical studies due to the lack of a clear doseresponse relationship and an increasing risk of toxicity . 
however , a different study of dose escalation to 90 gy ( photon irradiation , [ 5 ] ) reported a median survival of 12 months , which is very similar to numerous results of standard - dose trials . 
a recent meta - analysis of 3 , 004 patients from twelve randomized controlled trials also suggested a small but statistically significant improvement of survival from chemotherapy [ 34 ]  . 
rbe1 , falk wilfert1 , jan palm1 , jochem knig2 , susanne burdak - rothkamm1 , li liu1 , 3 , andreas schuck4 , normann willich4 , christian rbe1 background and purpose : the precise pathophysiological mechanisms of radiation - induced lung injury are poorly understood , but have been shown to correlate with dysregulation of different cytokines . 
the purpose of this study was to evaluate the time course of the pro - inflammatory cytokines tumor necrosis factor - ( tnf - ) ( cid : 1 ) , interleukin - ( il - ) 1 ( cid : 1 ) and il - 6 after whole - lung irradiation . 
real - time multiplex rt - pcr ( reverse transcriptase polmyerase chain reaction ) was established to evaluate the expression of tnf - ( cid : 1 ) , il - 1 ( cid : 1 ) and il - 6 in the lung tissue of the mice . 
for histological analysis , lung tissue sections were stained by hematoxylin and eos results : multiplex rt - pcr analysis revealed a biphasic expression of these pro - inflammatory cytokines in the lung tissue after irradiation . 
during the pneumonic phase , tnf - ( cid : 1 ) , il - 1 ( cid : 1 ) and il - 6 were significantly elevated and revealed their maximum at 8 weeks p.i. 
 key words : pneumonitis pro - inflammatory cytokines lung biphasic cytokine expression strahlenther onkol 2004 ; 180 : 4428 doi 10.1007 / s00066 - 004 - 1265 - 7 biphasische expression proinflammatorischer zytokine im rahmen der radiogenen lungenreaktion hintergrund und ziel : die genaue pathophysiologie der strahleninduzierten lungenschdigung ist bislang nur unvollstndig geklrt , scheint aber mit einer dysregulation verschiedener zytokine assoziiert zu sedas ziel dieser experimentellen studie war es , den zeitlichen expressionsverlauf der proinflammatorischen zytokine tumor - nekrose - faktor - ( tnf - ) ( cid : 1 ) , interleukin - ( il - ) 1 ( cid : 1 ) und il - 6 nach lungenbestrahlung zu untersuchen . 
im lungengewebe wurde die mrna - expression von tnf - ( cid : 1 ) , il - 1 ( cid : 1 ) und il - 6 mit hilfe der realtime - multiplex - rt - pcr ( reverse - transkriptase - polymerase - kettenreaktion ) quantifiziert . 
nach einem initialen anstieg bereits 1 h nach bestrahlung fr tnf - ( cid : 1 ) und nach 6 h fr il - 1 ( cid : 1 ) und il - 6 ging die zytokinexpression auf ausgangswerte zurck . 
whrend der pneumonitisphase war die mrna - expression von tnf - ( cid : 1 ) , il - 1 ( cid : 1 ) und il - 6 signifikant erhht und ereichte 8 wochen nach bestrahlung ihr maximuwhrend sich bis zu 4 wochen nach bestrahlung histopathologisch nur eine geringe lungenschdigung in 530% des gesamtlungengewebes beobachten lie , waren nach 8 , 16 bzw . 
 1 department of radiotherapy radiooncology , saarland university , homburg / saar , germany , 2 institute of medical biometrics , epidemiology and medical informatics , saarland university , homburg / saar , germany , 3 cancer center , union hospital tongji medical college , huazhong university of science and technology , wuhan , peoples republic of china , 4 department of radiotherapy radiooncology , university of mnster , germany . 
radiation - induced lung damage may arise depending on the total dose of irradiation , the fractionation schedule , the volume of lung tissue irradiated , the existence of prior lung disease , and the use of chemotherapeutic drugs in the treatment of the disease [ 14 , 15 , 17 , 25 ]  . 
acute pneumonitis is characterized by an enhanced vascular permeability with edema of the interstitium and exudation into air spaces and an influx and selective accumulation of different inflammatory and immune cells from the peripheral blood at the site of injury . 
a number of cytokines , known collectively as pro - inflammatory cytokines because they accelerate inflammation , regulate these inflammatory reactions and are released predominantly by recruited and resident inflammatory cells as well as pulmonary epithelial cells upon activation . 
 in the present study , we investigated the kinetics of radiation - induced upregulation of the pro - inflammatory cytokines tumor necrosis factor - ( tnf - ) , interleukin - ( il - ) 1 and il - 6 in whole - lung - irradiated c57bl / 6j mice . 
these pro - inflammatory cytokines are probably key mediators for the pathogenesis of radiation pneumonitis , because they show the following spectrum of biological activities : tnfenhances phagocytosis and cytotoxicity in neutrophilic granulocytes and modulates the expression of other cytokines including il - 1 and il - 6 . 
tnfand il - 1 are strong chemoattractants for leukocytes and they also increase their adherence to the endothelium by enhancing the expression of molecules such as intercellular adhesion molecule - ( icam - ) 1 and endothelial leukocyte adhesion molecule ( elam ) [ 9 ]  . 
il - 1 and il - 6 influence antigen - specific immune responses by an activation of t - cells ( induction of the differentiation of immature t - cells into cytotoxic t - cells , stimulation of t - helper cells ) and b - cells ( induction of the final maturation of b - cells into immunglobulin - secreting plasma cells and stimulation of the secretion of antibodies ) [ 5 ]  . 
glucocorticoids synthesized in response to acth inhibit the production of tnf - , il - 1 and il - 6 in vivo , thus establishing a sort of negative feedback loop between the immune system and neuroendocrine functions [ 18 ]  . 
 there are two functionally almost equivalent forms of il1 , il - 1 and il - 1 ( cid : 2 ) , that are encoded by two different genes but bind to the same receptor and therefore show similar if not identical biological activities . 
in the present study , we evaluated il - 1 , because it is the predominant form in mice , while il - 1 ( cid : 2 ) predominates in humans [ 8 ]  . 
in the present paper , we describe the principle of the method employed and the validation of this technique for those proinflammatory cytokines playing a role in radiation - induced pneumonitis . 
adult female mice , 8 weeks old and approximately 20 g in weight , were housed four to six per cage and allowed to acclimatize from shipping for 1 week prior to treatment . 
 radiation schedule a dose of 12 gy to the midplane of the lungs was delivered in a single fraction via a posterior field using a linear accelerator . a plastic jig was used to restrain the mice without anesthesia , and lead strips were placed to shield the head and abdomen . the irradiation characteristics were as follows : beam energy , 10 - mv photons ; dose rate , 2.4 gy / min ; sourcesurface distance ( ssd ) , 1 m ; size of the radiation field , 18 ( cid : 2 ) 10 ca film was taken to confirm that the entire lung was irradiated . 
23 mm thickness displaces the build - up region of the 10 - mv photon beam into the plastic material , thus achieving an acceptable dose uniformity throughout the thorax of individual mice . 
radiation - induced biphasic cytokine expression in the lung following irradiation the mice were maintained four to six per cage in laminar flow hoods in pathogen - free rooms to minimize pulmonary infections and supplied with standard laboratory diet and water ad libituage - matched controls were maintained under identical conditions for the course of the experiment . 
the left lobes were placed in fixative ( 4% neutral buffered formalin ) for histological analysis and the right lobes were quickly frozen in liquid nitrogen for rna isolation and subsequent pcr analyses . 
total rna preparations were performed using the rneasy total rna kit ( qiagen , hilden , germany )  . the lung tissue ( a right lobe is equivalent to 75 mg tissue ) was homogenized in 1.2 ml lysis buffer using a rotor - stator homogenizer ( ultra - turrax , ika , staufen , germany )  . 
the tnf - , il - 1 and il - 6 mrna expression in the lung tissue was quantified by realtime multiplex rt - pcr ( abi prism 7700 sequence detection system )  . 
in this multiplex rt - pcr one fluorogenic probe labeled with vic dye was used to detect the target amplicon ( tnfor il - 1 or il - 6 ) and another fluorogenic probe , labeled with fam dye , was used to detect the endogenous control gene ( gapdh )  . 
pcr primers and fluorogenic probes for murine tnf - , il - 1 and il - 6 and the reference gene gapdh were designed using the computer program primer express ( perkin elmer / applied biosystems , foster city , ca , usa )  . 
primer and probe sequences for tnf - ( cid : 1 ) , il - 1 ( cid : 1 ) , il - 6 , and gapdh . pcr primers and fluorogenic probes for murine tnf - ( cid : 1 ) , il - 1 ( cid : 1 ) and il - 6 and the reference gene gapdh were designed using the computer program primer express . 
die primer und fluoreszenzmarkierten sonden fr murinen tnf - ( cid : 1 ) , murines il - 1 ( cid : 1 ) und il - 6 sowie das referenzgen gapdh wurden mit der software primer express konstruiert . 
 pcr amplifications were performed in a total volume of 25 l , containing 3 l cdna sample , 50 mm kcl , 10 mm trishcl ( ph 8.3 ) , 60 nm passive reference 1 ( rox ) , 200 m datp , dctp , dgtp and 400 m dutp , 5.5 mm mgcl2 , 0.05% gelatine , for each target gene ( tnf - / il - 1 / il - 6 ) 300 nm of each primer , for the reference gene ( gapdh ) 80 nm ( forward primer ) and 60 nm ( reverse primer ) , 1.25 u amplitaq gold , and 0.25 u amperase uracil n - glycosylase ( taqman pcr core reagent kit ; perkin elmer / applied biosystems )  . 
radiation - induced biphasic cytokine expression in the lung and 10 min at 95 c , followed by a total of 40 two - temperature cycles : 15 s at 95 c and 1 min at 60 c . 
 histology for histological analysis , the left lobes were fixed in 4% neutral buffered formalin , paraffin - embedded , and sectioned at an average thickness of 5 the mounted sections were stained by hematoxylin and eos tnf - ( cid : 1 ) statistical methods the 14 groups ( corresponding to the 14 assessment time points ) and the control group were tested for mean difference on a logarithmic scale of the five mediator parameters by simple analysis of variance followed by two - sided pairwise comparisons versus control according to dunnett . 
in the il - 1 data with values < 2 ( cid : 2 ) 104 were excluded prior to statistical testing . the statistical calculations were performed by spss statistical software . 
in brief , the histopathologic alterations that contributed to the pleomorphic picture of radiation - induced lung injury included macrophage infiltration in air spaces , edema in the alveolar walls and / or air spaces , desquamation of epithelial cells from the alveolar walls , thickening of the alveolar septa by infiltration of inflammatory cells , collagen deposition , progressive fibrosis of alveolar septa , and obliteration of the alveoli . 
 pcr analysis the results of the quantitative assessment of tnf - , il - 1 and il - 6 mrna expression in lung tissue after thoracic irradicontrol 0.5h 1h 3h 6h 12h 24h 48h 72h 1w 2w 4w 8w 16w 24w time figure 1 . 
time course of the tnf - ( cid : 1 ) mrna expression in the lung tissue of mice that underwent thoracic irradiation with 12 gy ( data are mean sd of triplicate determinations from three different mice ; * : statistically significant )  . 
zeitlicher verlauf der tnf - ( cid : 1 ) - mrna - expression im lungengewebe von musen nach ganzlungenbestrahlung mit 12 gy ( mittelwert standardabweichung von dreifachbestimmungen an drei verschiedenen musen ; * : statistisch signifikant )  . 
current concepts of the pathogenesis of pulmonary fibrosis propose an initial inflammatory stage involving an influx of inflammatory cells into the interstitium , which together with activated resident cells are thought to release a variety of cytokines [ 24 , 6 , 10 , 11 , 1921 , 26 ] and other polypeptide mediators such as chemokines [ 12 ] that stimulate fibroblast proliferatsion and collagen secretion . while pulmonary fibroblasts are probably the most central cell populations in this process , because of their ability to produce collagen , it is obvious that the regulation of the fibroblast responses in injury is influenced by specific interactions among multiple cell types . 
cytokine expression by recruited and resident inflammatory cells , as well as by pulmonary epithelial and endothelial cells , has been implicated in the development of radiation - induced lung injury [ 4 , 19 , 20 ]  . 
time course of the il - 1 ( cid : 1 ) mrna expression in the lung tissue of mice that underwent thoracic irradiation with 12 gy ( data are mean sd of triplicate determinations from three different mice ; * : statistically significant )  . 
zeitlicher verlauf der il - 1 ( cid : 1 ) - mrna - expression im lungengewebe von musen nach ganzlungenbestrahlung mit 12 gy ( mittelwert standardabweichung von dreifachbestimmungen an drei verschiedenen musen ; * : statistisch signifikant )  . 
the second peak increase in tnf - , il - 1 and il - 6 mrna levels was associated with the onset of acute pneumonitis visible in the histological changes associated with organizing alveolitis . 
 discussion for the present study , we designed and optimized an accurate multiplex rt - pcr for the relative quantification of inflammatory cytokines playing a role in radiation - induced pneumonitis . 
to compensate for variations in input rna amounts and efficiency of reverse transcription , an endogenous control gene ( gapdh ) was quantified , and results were normalized to its values . 
in this multiplex rt - pcr , one fluorogenic probe , labeled with vic dye , was used to detect the target amplicon ( tnf - / il - 1 / il - 6 ) , and another fluorogenic probe , labeled with fam dye , was used to detect the endogenous control gene ( gapdh )  . 
as this method combines pcr amplification and product detection in one single step , the technique is very fast and easy to perform , compared to classic rt - pcr techniques . 
the use of internal fluorogenic probes the present work is a detailed study on the temporal release of the pro - inflammatory cytokines tnf - , il - 1 and il - 6 in the lung tissue of c57bl / 6j mice after thoracic irradiation . 
inflammatory cytokines are of key interest for modulating and ameliorating the effects of inflammatory reactions after lung irradiation ( acute radiation pneumonitis ) and their sequelae ( late radiation fibrosis )  . 
our results demonstrate a complex pattern of elevation of cytokine mrna levels following total - lung irradiation but with a clear indication of a two - phase mechanism in the molecular pathology . 
we observed an immediate release of pro - inflammatory cytokines in the first hours after lung irradiation with no detectable appearance of histological changes and a second long - lasting increase in pro - inflammatory cytokine mrna levels correlating with the onset of organizing alveolitis . 
since tnfenhances the production of different cytokines , including il - 1 and il - 6 , which are thought to further promote the inflammatory process , the authors presume that tnfmay induce the expression of il - 1 and il - 6 in irradiated lung tissue , therefore having a prominent role in the initiation of the cytokine cascade . 
in the first hours after thoracic irradiation , the bronchiolar epithelium revealed an intense and homogeneous staining for tnf - ; in lung parenchyma , resting alveolar macrophages stained positive . during the stage of acute pneumonitis , the lung tissue revealed an accumulation of positive inflammatory cells particularly in perivascular and peribronchial areas , as well as in subpleural regions . 
time course of the il - 6 mrna expression in the lung tissue of mice that underwent thoracic irradiation with 12 gy ( data are mean sd of triplicate determinations from three different mice ; * : statistically significant )  . 
zeitlicher verlauf der il - 6 - mrna - expression im lungengewebe von musen nach ganzlungenbestrahlung mit 12 gy ( mittelwert standardabweichung von dreifachbestimmungen an drei verschiedenen musen ; * : statistisch signifikant )  . 
human alveolar macrophages have been shown to release il - 1 , predominantly il - 1 ( cid : 2 ) , within hours after irradiation in vitro [ 16 ]  . 
no published data are available evaluating the cellular source of increased il - 1 and il - 6 expression after lung irradiation in vivo . therefore , immunohistochemical detection methods were established in our laboratory to evaluate the protein expression of il - 1 and il - 6 in the lung tissue after thoracic irradiation . our preliminary results seem to confirm the presented mrna expression data , with the bronchiolar epithelium becoming a significant source of these pro - inflammatory cytokines especially in the first hours after irradiation ; at the onset of radiation pneumonitis , the bronchiolar epithelium as well as inflammatory cells in the lung parenchyma produce high amounts of these inflammatory cytokines . 
these results are in contrast to our observation of a long - lasting increase of tnfon mrna and protein level during the acute phase of pneumonitis , predominantly secreted by inflammatory cells in the lung parenchyma [ 20 ]  . 
 previous reports of cytokine expression following lung irradiation focused on the remodeling phase but not the initial response within the first hours after irradiation [ 3 , 11 , 21 ]  . 
 [ 6 ] that tnfand il - 1 mrna levels ( measured by rnase protection assay ) were induced in the lung tissue of c57bl / 6j mice within 24 h after irradiation . 
radiation - induced biphasic cytokine expression in the lung conclusion this study demonstrates that irradiation induces a biphasic expression of pro - inflammatory cytokines in the lung : an initial transitory cytokine response within the first hours after lung irradiation and a second , more persistent cytokine elevation which coincides with the onset of acute pneumonitis . 
 strahlentherapie und onkologie original article early effects of irradiation on [ 123i ] - imt and [ 18f ] - fdg uptake in rat c6 glioma cells burkhard riemann1 , stefan knemann2 , daniel ppping1 , klaus kopka1 , matthias weckesser1 , normann willich2 , otmar schober1 background : single - photon emission computed tomography ( spect ) using 3 - [ 123i ] - iodo - l - ( cid : 1 ) - methyltyrosine ( [ 123i ] - imt ) and positron emission tomography ( pet ) using 2 - [ 18f ] - fluoro - 2 - deoxy - d - glucose ( [ 18f ] - fdg ) are valuable tools for the distinction between viable tumor and radionecrosis in patients receiving radiotherapy for high - grade gliomas . 
 material and methods : to determine the early effects of irradiation on [ 123i ] - imt and [ 18f ] - fdg uptake in gliomas , in vitro studies were performed using rat c6 glioma cells . 
 conclusion : rat c6 glioma cells show an early increase in [ 123i ] - imt and [ 18f ] - fdg uptake following irradiation which may be partly due to giant cell formation . 
 material und methodik : um die frhen effekte einer radiotherapie auf die [ 123i ] - imtund [ 18f ] - fdg - aufnahme in gliomen zu bestimmen , wurden in - vitro - studien an c6 - gliomzellen der ratte durchgefhrt . 
ferner fand sich ein leichter anstieg der [ 18f ] - fdg - aufnahme whrend der ersten 3 tage nach der strahlentherapie bezogen auf 105 lebendige gliomzellen ( p < 0 , 05 )  . 
dabei war die maximale zunahme der [ 123i ] - imt - aufnahme 1 h nach applikation insgesamt grer als die der [ 18f ] - fdg ( p < 0 , 01 )  . schlussfolgerung : c6 - gliomzellen zeigen nach einer strahlentherapie einen frhen anstieg der [ 123i ] - imtund [ 18f ] - fdg - aufnahme , der u.a. 
die ergebnisse dieser studie legen eine bedeutung der [ 123i ] - imt - spect und der [ 18f ] - fdg - pet in der frhen erfassung des ansprechens der gliome auf eine strahlentherapie nahe . 
 [ 123i ] - imt and [ 18f ] - fdg uptake in glioma cells following irradiation introduction it is well known that primarily morphological imaging techniques such as computed tomography ( ct ) or magnetic resonance imaging ( mri ) often fail to discriminate between viable tumor and radionecrosis . 
in recent years , functional imaging modalities like single - photon emission computed tomography ( spect ) and positron emission tomography ( pet ) have attracted considerable attention in the detection of residual / recurrent gliomas following different therapeutic interventions [ 12 , 42 , 44 ]  . 
it is generally accepted that pet using 2 - [ 18f ] - fluoro - 2 - deoxy - d - glucose ( [ 18f ] - fdg ) is a valuable tool for detecting the therapeutic efficiency of irradiation in gliomas , which is reflected by a decline in [ 18f ] - fdg uptake several weeks after radiotherapy [ 6 , 7 ]  . 
they reported that brain tumors that responded well to the treatment showed an early increase in [ 18f ] - fdg uptake , which correlated with the degree of the response . 
by contrast , nonresponders did not show any early changes in glucose metabolism . to date , the mechanisms underlying the early increase in glucose metabolism of the irradiated brain tumors are not known [ 37 , 52 ]  . 
introduced the radiolabeled amino acid 3 - [ 123i ] - iodo - l - - methyltyrosine ( [ 123i ] - imt ) for the spect examination of brain tumors [ 5 , 39 ]  . 
therefore , the kinetics of [ 123i ] - imt and [ 18f ] - fdg uptake were monitored in rat c6 glioma cells for 3 days following a single irradiation with 20 gy . 
 material and methods chemicals and reagents [ 123i ] - imt was synthesized from l - - methyltyrosine by radioiodination of the c3 position of the benzene ring as described previously [ 27 ]  . 
 linear accelerator irradiation experimental tumor cells were exposed to a single radiation dose of 20 gy at room temperature 1 day after subculture using a linear accelerator ( varian clinac 2100c , darmstadt , germany ) and 6 - mv photons . 
 uptake measurements uptake measurements were performed before and 1 , 2 , and 3 days after radiotherapy and sham irradiation , respectively . first , monolayers were washed twice with pbs and incubated for 10 min at 37 c with krebs - ringer bicarbonate - buffered mediusubsequently , 100 l of 0.9% nacl solution supplemented with [ 123i ] - imt and [ 18f ] - fdg ( 2 ci [ 74 kbq ] ) , respectively , were added [ 51 ]  . 
subsequently , cells were homogenized with 1 ml 0.1 n naoh for 30 min , and small samples ( 200 l ) were extracted for determination of radioactivity by - scintillation ( 1480 wallac wizard 3 , perkinelmer , boston , ma , usa ) [ 51 ]  . 
finally , tracer uptake , expressed as percent dose per 105 viable cells or percent dose per tissue culture well , was determined . dna flow cytometry study c6 cells ( approximately 106 cells ) cultured as described above were trypsinized and washed with pbs at 0 , 24 , 48 , and 72 h post strahlenther onkol 2004 no . 
histograms from the epics c printout were used to estimate the cell fractions in the g0 / 1 - , sand g2 / m - phases [ 20 ]  . 
the percent dose of [ 18f ] - fdg uptake per tissue culture well increased linearly in control cells between the 1st and 3rd day ( p < 0.001 ; figure 2a )  . 
 [ 123i ] - imt uptake the percent dose of [ 123i ] - imt uptake per tissue culture well increased conspicuously over time in the control group , with a 1 , 452% increase from day 0 through day 3 ( p < 0.001 ; figure 3a )  . 
there was a moderate but significant increase in [ 123i ] control irradiated 800 , 000 600 , 000 400 , 000 200 , 000 days after irradiation figure 1 . 
 by contrast , [ 123i ] - imt uptake per 105 viable control cells remained constant for 2 days and decreased on day 3 , when confluence was achieved ( p < 0.001 ; figure 3b )  . 
the results of a micromorphometric study showed that the giant cells increased in volume to about ten times that of control cells on the 3rd day after irradiation ( figures 4a and 4b )  . 
the cell fractions in the g0 / 1 - , sand g2 / m - phases determined by dna flow cytometry showed a clearly apparent synchronization with an arrest of cells in the s - phase and a significant decrease in g2 / m - phase cells ( p < 0.05 ) in the irradiated group ( data not shown )  . 
 [ 123i ] - imt and [ 18f ] - fdg uptake in glioma cells following irradiation 1 , 500 1 , 000 control ( [ 18f ] - fdg ) irradiated ( [ 18f ] - fdg ) days after irradiation control ( [ 18f ] - fdg ) irradiated ( [ 18f ] - fdg ) days after irradiation figure 2a abbildung 2a figure 2b abbildung 2b figures 2a and 2b . 
1 tag nach der scheinbestrahlung zeigt sich bei den kontrollzellen ein linearer anstieg der [ 18f ] - fdg - aufnahme pro zellkultur ( p < 0 , 001 )  . 
darber hinaus findet sich eine mige zunahme der [ 18f ] fdg - aufnahme pro zellkultur nach der strahlentherapie mit 20 gy ( p < 0 , 05 )  . 
bei den scheinbestrahlten zellen lsst sich ber einen zeitraum von 3 tagen nach der strahlentherapie eine abnahme der [ 18f ] - fdg - aufnahme in 105 lebendigen zellen nachweisen . 
im gegensatz dazu zeigt sich in den ersten 3 tagen nach der strahlentherapie eine signifikante zunahme der [ 18f ] - fdg - aufnahme ( p < 0 , 05 )  . 
 control ( [ 123i ] - imt ) irradiated ( [ 123i ] - imt ) control ( [ 123i ] - imt ) irradiated ( [ 123i ] - imt ) 1 , 500 1 , 000 days after irradiation days after irradiation figure 3a abbildung 3a figure 3b abbildung 3b figures 3a and 3b . 
they reported that tumors that responded well to the treatment showed an early increase in [ 18f ] - fdg uptake which correlated with the degree of the response , whereas nonresponders did not show any early changes in glucose metabolisthese findings suggest that both the early increase as well as the late decrease in [ 18f ] - fdg uptake may be correlated with a favorable response of brain tumors to radiation . therefore , maruyama et al . 
in order to explain the early increase in [ 18f ] - fdg uptake , they speculated that irradiated tumor cells require more glycolytic metabolism for energy - consuming processes such as deoxyribonucleic acid ( dna ) repair [ 41 ]  . 
 [ 64 ] who showed that cellular stress increases glucose transport by promoting the accumulation of glucose transporter molecules at the cell surface in vitro [ 58 , 64 ]  . 
in addition to the appearance of giant cells , the dna flow cytometry study showed an arrest of c6 glioma cells in the s - phase and a significant decrease in the g2 / m - phase cells , which indicates that cells are prohibited from further cell divisions . 
according to higashi et al . , irradiated tissue culture wells represent a simplified model for the tumor in vivo , since they contain viable as well as nonviable cells [ 20 ]  . 
inflammatory cells like macrophages , lymphocytes and leukocytes lead to a prominent increase in [ 18f ] - fdg uptake comparable to that of tumor cells [ 17 , 22 , 30 , 53 , 57 , 66 ]  . 
they also found an early increase in [ 18f ] - fdg uptake reaching its maximum between the 1st and 3rd day during radiotherapy applied in fractions of 2 gy per day . 
however , using this combined spect and pet approach , they could not quantify the portions of [ 18f ] - fdg uptake which were caused by the tumor and by the inflammation , respectively . 
in addition , the influence of different parameters , such as the total irradiation dose , the fractional application of these doses and their time dependence can be investigated under standardized conditions in vitro . 
according to the literature , very few investigative studies have been performed to document the early kinetics of amino acid uptake in tumor cells or tissues after irradiation [ 20 , 28 , 29 , 55 ]  . 
in contrast to our study using c6 glioma cells and [ 123i ] - imt , [ 3h ] - methionine uptake per 1 , 000 cells was already significantly increased within the 1st day following irradiation . 
therefore , it is of particular interest whether the irradiation - induced increase in [ 3h ] - methionine uptake in viable cells of tumor spheroids is also accompanied by giant cell formation . 
found a modest increase in [ 3h ] - methionine uptake per tissue culture well post irradiation with 30 gy in a human ovary cell line ( htb77ip3 ) [ 20 ]  . 
this is consistent with the present study showing a moderate increase in [ 123i ] - imt uptake per tissue culture well in rat c6 glioma cells after irradiation with 20 gy . 
in contrast to [ 3h ] - methionine , [ 123i ] - imt is not incorporated into proteins and is not metabolized further in quantitative terms [ 23 ]  . 
thus , [ 123i ] imt uptake does not reflect tumor metabolism but the expression of amino acid transport systems on the cell surface [ 25 , 34 , 35 , 49 ]  . 
recently , it could be shown that [ 123i ] - imt uptake in rat c6 glioma cells is principally mediated by the l - system for large , neutral amino acids ( 72% ) and to a minor extent by the b0 , + - system for cationic and zwitterionic amino acids ( 17% ) [ 51 ]  . 
 there are two studies that have investigated the uptake of [ 14c ] - methionine in vivo following irradiation using a rat ah109a tumor model [ 28 , 29 ]  . 
it is well known that many parameters such as radiation dose and fractionation , individual tumor radiosensitivity , oxidative status and vascular supply have to be taken into account when monitoring the effects of radiotherapy in the in vivo situation [ 26 , 36 ]  . however , in vitro models offer the advantage of studying the influence of single parameters in a standardized and less complex tumor model [ 11 ]  . 
 conclusion irradiation of rat c6 glioma cells with 20 gy induced giant cell formation and an increase in cellular [ 123i ] - imt and [ 18f ] fdg uptake within 2 days after irradiation . 
bechrakis2 , martin nausner1 , klaus - martin kreusel2 , heinz kluge3 , jrgen heese3 , jens heufelder3 , dino cordini3 , heinz homeyer3 , hermann fuchs2 , peter martus4 , michael h . 
foerster2 , thomas wiegel1 , wolfgang hinkelbein1 background and purpose : in june 1998 , proton - beam therapy of ocular tumors started at the hahn - meitner institute berlin , germany . 
 patients and methods : 245 consecutive patients with primary melanoma of the uvea were treated from june 1998 to april 2003 with a 68 - mev proton beain 96.2% of all patients , a uniform fractionation scheme was applied : single dose 15 cge ( cobalt gray equivalent ) , total dose 60 cge on 4 consecutive days . 
 conclusion : proton - beam irradiation of uveal melanomas at the hahn - meitner institute after the first 5 years of its initiation reveals local tumor control and eye retention rates in the range of other centers with larger experience . 
 key words : uveal melanoma proton therapy strahlenther onkol 2004 ; 180 : 41924 doi 10.1007 / s00066 - 004 - 1222 - 5 bestrahlung von aderhautmelanomen mit protonen in berl5 jahre behandlung am hahn - meitner - institut hintergrund und ziel : im juni 1998 wurde am hahn - meitner - institut in berlin mit der protonentherapie von augentumoren begonnen . 
bei 96 , 2% der behandelten kam ein einheitliches fraktionierungsschema zur anwendung : einzeldosis 15 cge ( cobalt - gray - quivalent ) , gesamtdosis 60 cge an 4 aufeinander folgenden tagen . 
 schlussfolgerung : die ergebnisse fr die lokale tumorkontrolle und den augenerhalt sind vergleichbar mit denen anderer zentren . damit ist es gelungen , in der hadronentherapie von beginn an eine behandlung auf hohem qualitativem niveau zu etablieren . schlsselwrter : aderhautmelanom protonentherapie introduction uveal melanoma is a rare disease with < 2 , 000 new patients per year treated in the usa and canada [ 30 ]  . 
a variety of therapeutic options is available ranging from careful observation in small melanocytic lesions of uncertain malignant potential to enucleation or exenteration of the orbital content for large tumors with extraocular extension . 
since the early 1980s , radiation therapy plays a very important role in all approaches of organ conservation , and many different modalities are in clinical use for ocular tumors , namely plaque ther1 department of radiation oncology and radiotherapy , charit universittsmedizin berlin , campus benjamin franklin , berlin , germany , 2 department of ophthalmology , charit universittsmedizin berlin , campus benjamin franklin , berlin , germany , 3 ocular tumor therapy , hahn - meitner institute berlin , germany , 4 institute of medical informatics , biometry and epidemiology , charit universittsmedizin berlin , campus benjamin franklin , berlin , germany . 
proton therapy of uveal melanomas in berlin apy with 125i , 106ru / 106rh , 198au [ 24 , 27 , 36 , 37 , 40 ] , stereotactic radiotherapy or radiosurgery [ 31 , 42 , 44 ] , and hadron therapy with proton or helium beams [ 3 , 11 , 16 , 17 , 32 ]  . 
 tumors in close proximity to the optic disk and fovea are most difficult to treat , due to the expected high complication rate related to the irradiation of structures that are vital for visual function . 
therefore , the steep distal fall - off of hadron namely proton beams offers the best chance to avoid unnecessary radiation exposure to optic disk , fovea and optic nerve , and thereby preserve visual acuity . 
 the first proton - beam facility in germany at the hahnmeitner institute in berlin - wannsee started routine therapy of ocular tumors in close collaboration with the departments of ophthalmology and radiation oncology of the charit medical school campus benjamin franklin in june 1998 . 
as of july 2003 , > 350 patients have been treated , and herein we report our results in 245 consecutive patients with primary uveal melanomas irradiated from june 1998 to april 2003 . 
 patients and methods diagnosis of uveal melanoma was established or confirmed in all 245 patients at the department of ophthalmology of the charit medical school campus benjamin frankldetails of the patient population are listed in table 1 . 
planning treatment volume ( ptv ) delineation was done by correlating photograph montages of the tumor and the ocular fundus with intraoperative measurements of clip distances , aand b - scan ultrasound measurements of the eye and the clip distances as well as high - resolution computed tomography of the involved eye in each case . 
orthogonal x - ray verifications of the clip positions are digitally superimposed to the expected clip positions from the eyeplan treatment program . eyelid retractors are used in all patients , and care is taken to avoid irradiation of the eyelids whenever possible . 
therapy with a 68 - mev proton beam generated by a cyclotron was given homogeneously for all but eight patients with four fractions of 15 cge ( cobalt gray equivalent ) on 4 consecutive days , almost all of the remainders were treated with eight fractions of 7.5 gy delivered twice daily on 4 consecutive days . 
all patients were followed after treatment at 3 - , 6 - , 9 - month and thereafter at yearly intervals in the department of ophthalmology , charit medical school campus benjamin franklfollowup data were prospectively recorded by uniform diagnostic procedures : measurements of visual acuity and intraocular pressure , slit - lamp biomicroscopy , indirect ophthalmoscopy , aand b - scan ultrasound measurements , and fundus photography . 
standard report forms were recorded for all patients . radiation retinopathy was recorded in the presence of cottonwool spots , retinal vasculopathy , retinal exudations or hemorrhages , with or without neovascularization . 
optic nerve neuropathy was recorded in the case of optic disk hyperemia or hemorrhages , peripapillary exudation , central retinal artery vasculopathy , or late optic disk pallor or atrophy . 
to reduce the influence of extreme values , each continuous variable was grouped into small , medium and large values according to the 33% and 67% percentile in the data ( table 1 )  . 
for the analysis of visual acuity during follow - up , a linear mixed model ( verbeke , molenbergh ) with random intercept and linear and quadratic effects of the time variable was applied . 
 results with a median follow - up of 18.4 months , seven local recurrences were diagnosed , resulting in a tumor control probability of 96.4% at that point of time and a 3 - year tumor control probability of 95.5% ( figure 1 )  . 
the rate of eye retention was somewhat lower with 92.6% at the time of the median followup for that parameter ( 20 months ) and 87.5% at 3 years ( figure 2 ) , due to complications such as severe neovascular glaucoma and / or vitreous hemorrhage , resulting in a blind and painful eye . 
the development of side effects namely , radiation retinopathy , optic nerve neuropathy , rubeosis iridis , secondary glaucoma and cataract over time is displayed in figures 3 to 7 . a steady increase was noted for all side effects apart from glaucoma and rubeosis iridis , where a plateau might evolve , due to adequate complication treatment options , such as retinal laser photocoagulation or cryocoagulation . 
 in univariate analysis , tumor size ( volume , tumor thickness , largest tumor basal diameter ) and tumor location ( distance to fovea and optic disk ) were significantly associated with local tumor control and complications ( table 2 )  . 
multivariate analysis revealed that tumor thickness was the most important prognostic factor for the development of treatment complications ( radiation retinopathy , optic nerve neuropathy , glaucoma , and cataract ) , followed by the distance to the optic disk . 
the change of visual acuity during follow - up was strongly inversely correlated with the distance of the tumor to the fovea , but not with the distance to the optic disk ( data not shown )  . 
various approaches to deliver radiation are available , but not all of them are suitable for tumors located at the posterior pole of the globe , where plaque therapy is associated with largely increased morbidity or is even impossible in case of tumors surrounding the optic disk . 
aiming to avoid enucleation with all the inherent consequences for vision and psychological selfestimate , stereotactic radiotherapy and hadron therapy both are established treatment modalities , with the latter owing the advantage of far more patients treated and evaluated over decades [ 2 , 16 , 17 , 21 ]  . 
 local control of malignant disease is the mainstay of therapy but given excellent tumor control rates achievable , further aspects of treatment outcome gain importance : reduction of side effects and preservation of a useful vision [ 8 , 15 , 20 , 29 ]  . the steep distal fall - off of proton - beam irradiation with typical values of about 1 mm distance from 90% to 10% isodoses for beam energies in the range of 6090 mev is superior to any other irradiation technique nowadays available . 
knowledge about the impacts of certain therapeutic strategies on outcome in patients with melanoma of the uveal tract has increased considerably by the collaborative ocular melanoma study group reports , as well as by large single - center series [ 2 , 6 , 10 , 11 , 18 , 26 , 40 ]  . 
although we do not yet have median 5 - year follow - up data , our kaplan - meier estimates for local control and eye retention compare quite well with other established centers ( table 4 ) , and we do not expect a significant deterioration in our results with longer follow - up available as , obviously , there is a learning curve [ 18 , 19 , 21 ]  . 
meticulous repeated self - assessment and follow - up of treatment results , as well as adoption of treatment experiences of others are of paramount importance in achieving this goal . 
proton - beam therapy for uveal melanoma has been established several decades ago , and institutions like mgh in boston , ma , usa , and psi in switzerland have largely contributed to the therapeutic concepts nowadays adopted by us and others . 
 scoring and evaluating side effects of therapy is difficult especially in uveal melanoma , as there are various interrelated parameters that have to be considered , some of them disease - related , others depending on treatment factors [ 8 , 10 , 12 , 13 , 20 , 21 , 28 , 29 , 33 ]  . 
the vast majority of all tumors treated were situated in direct proximity to the fovea and / or the optic disk ( see percentiles in table 1 ) , areas well known for an increased rate of side effects . 
even if in the long run visual acuity will decrease significantly in the majority of the patients treated , there is a substantial benefit in terms of binocular vision and cosmesis , and many patients maintain some significant degree of function for long periods after treatment . 
 conclusion within the time period which is evaluable until now , our results achieved after proton - beam therapy for uveal melanoma are well in the range of more experienced centers . 
hainfellner4 , daniela prayer5 , christine marosi1 background : extracranial seeding of glioblastoma multiforme ( gbm ) is very rare and its development depends on several factors . this case report describes two patients suffering from gbm with spinal seeding . 
 key words : glioblastoma multiforme spinal seeding cerebrospinal fluid strahlenther onkol 2004 ; 180 : 4557 doi 10.1007 / s00066 - 004 - 1293 - 3 glioblastom mit spinalen absiedelungen hintergrund : die extrakraniale ausbreitung eines glioblastoma multiforme ( gbm ) ist sehr selten und hngt von mehreren faktoren ab . 
the prognosis remains dismal : 8290% of the patients suffering from gbm die within the first 2 years , mostly after local recurrence of the tumor [ 57 , 9 , 12 ]  . 
not only is the extracranial seeding of gbm very rare [ 2 , 3 , 13 ] ( regional lymph nodes , lung , pleura , seldom bone and liver ) [ 11 , 14 ] , but there is also little information about spreading within the cerebrospinal fluid ( csf )  . 
a number of reasons are responsible 1 clinical division of oncology , department of medicine i , university of vienna , austria , 2 department of neurosurgery , university of vienna , austria , 3 department of radiooncology , university of vienna , austria , 4 clinical institute for neurology , university of vienna , austria , 5 department of neuroradiology , university of vienna , austria . 
glioblastoma and spinal seeding for the rare incidence of spinal seeding : first , patient survival is too short [ 14 ] ; second , there are no lymphatic vessels present in the cerebrum [ 16 ] ; furthermore , there is usually compression of the vascular system by the lesion itself as well as , lastly , the patients own immune response against malign cells [ 4 ]  . 
on the other hand , there are factors that promote spinal seeding : for one , surgical procedure can aid in the dissemination of tumor cells ; second , the long - term survival of patients has an influence and , furthermore , therapies that suppress the immune response in patients suffering from gbm ( radiation therapy , corticosteroid therapy , chemotherapy ) can also increase the risk of spinal seeding [ 8 ]  . 
after surgery , the patient underwent radiation therapy with 1.8 gy / fraction to a total of 66 gy and concomitant intravenous cytostatic chemotherapy with fotemustine 100 mg / m2 and dacarbazine 200 mg / m2 for five cycles . 
a stereotactic boost was given with a total of 3 ( cid : 1 ) 3 gy , and chemotherapy with ccnu 100 mg / m2 was administered for three cycles . 
a neuroradiosurgical boost with the gamma - knife was given , and chemotherapy was changed to temozolomide , 250 mg / day from day 1 to 5 , every 4 weeks . 
the neurologic examination remained normal until june 2000 , when palliative radiation therapy of the entire spinal cord with 1.8 gy / fraction to a total of 46 gy was planned . 
 case report 2 a 39 - year - old man was admitted to the intensive care unit through the emergency ward in a somnolent state with a history of 8 weeks with nausea and emesis . 
the mri of the cerebrum showed a temporomesial girlandiform contrast - enhancing lesion of up to 5 cm in diameter within the left hemisphere giving the impression of a gbm . 
radiation therapy was administered in the area from c3 to c7 together with concomitant chemotherapy consisting of carboplatin ( cbdca ) 350 mg / m2 on day 1 and etoposide 120 mg / m2 days 13 , of which the patient only received one cycle . 
both tumors initially showed close contact to the csf and thereby anatomic localization being favorable for the dissemination into the csf . furthermore , prior administration of immunosuppressive therapy is still active at the time of relapse and hereby also favors spinal seeding . 
the published cases and the two patients presented in this report confirm that patients with spinal seeding via csf from gbm are symptomatic from their spinal metastasis and that , besides witham et al . [ 17 ] and nakagawa et al . 
 strahlentherapie und onkologie original article anatomic variations due to radical prostatectomy impact on target volume definition and dose - volume parameters of rectum and bladder giuseppe sanguineti1 , pietro castellone2 , 3 , franca foppiano4 , paola franzone5 , michela marcenaro5 , piero tognoni6 , angelo bolognesi7 , giovanni luca ceresoli7 , claudio fiorino2 background and purpose : a quantitative estimate of the impact of prostatectomy on pelvic anatomy is unavailable , even if it would be an important prerequisite for a precise definition of clinical target volume ( ctv ) in post - prostatectomy radiotherapy . 
each patient underwent a planning ct between 1 week and 1 month before surgery ( ctpre ) , and then ct was repeated in the same positioning 12 months after surgery ( ctpost )  . 
two different ctvs were contoured : ctv1 : prostate + seminal vesicles in ctpre ; prostate + seminal vesicles surgical bed in ctpost ; ctv2 : prostate in ctpre ; prostate surgical bed in ctpost . 
preand post - surgery dose - volume histograms ( dvhs ) of rectum and bladder were compared together with the fraction of rectum / bladder receiving at least 95% of the icru dose ( v95 ) , the treated volume ( tv , body included in the 95% isodose ) and the irradiated volume ( iv , body included in the 50% isodose )  . 
the average reduction of v95 for the rectum was relatively small ( 2.5 cm3 of rectal wall )  . conclusion : the impact of prostatectomy on ctv definition is high . 
a significant reduction of ctv , ptv , tv and iv may be expected after surgery with a consequent reduction of the portions of rectum / bladder irradiated with adjuvant radiotherapy . key words : post - prostatectomy radiotherapy salvage radiotherapy adjuvant radiotherapy dose - volume histograms prostate strahlenther onkol 2004 ; 180 : 56372 doi 10.1007 / s00066 - 004 - 1245 - y anatomische vernderungen infolge radikaler prostatektomie . 
auswirkungen auf zielvolumendefinition und dosisvolumen - parameter von rektum und blase hintergrund und ziel : eine methode zur quantitativen bestimmung der auswirkungen einer prostatektomie auf die anatomie des beckenraums gibt es nicht , obwohl dies eine wichtige voraussetzung fr eine genaue festlegung des klinischen zielvolumens ( ctv ) fr die postoperative radiotherapie wre . 
 1 department of radiation oncology , university of texas medical branch , galveston , texas , usa , 2 department of medical physics , san raffaele hospital , milan , italy , 3 faculty of physics , university of naples federico ii , naples , italy , 4 department of medical physics , national institute for cancer research , genoa , italy , 5 department of radiotherapy , national institute for cancer research , genoa , italy , 6 department of urology , san martino hospital , genoa , italy , 7 department of radiochemotherapy , san raffaele hospital , milan , italy . 
impact of prostatectomy on ctv and dvhs patienten und methodik : sechs patienten , bei denen eine radikale retropubische prostatektomie indiziert war , unterzogen sich einer planungs - ct 1 woche bis 1 monat properativ ( ctpre ) ; die ct wurde in der gleichen positionierung 12 monate postoperativ wiederholt ( ctpost )  . 
es wurden unterschiedliche ctvs eingetragen : ctv1 : prostata + samenblschen in ctpre ; operationsfeld von prostata + samenblschen in ctpost ; ctv2 : prostata in ctpre ; prostataoperationsfeld in ctpost . 
prund postoperative dosis - volumen - histogramme ( dvhs ) von rektum und blase wurden verglichen und der anteil von rektum und blase , die mindestens 95% der icru - dosis ( v95 ) erhielten , sowie das behandlungsvolumen ( tv , innerhalb der 95% - isodose ) und das bestrahlungsvolumen ( iv , innerhalb der 50% - isodose )  . 
diese reduktion war im wesentlichen einer weiter kaudalen lage des kranialen ctv - randes nach prostatektomie ( durchschnittliche abweichung fr ctv2 : 1 , 5 cm ; spannweite 02 , 5 cm ) zuzuschreiben . 
postoperativ ist eine signifikante abnahme von ctv , ptv , tv und iv zu erwarten mit der folge einer verminderung der bei der adjuvanten radiotherapie von strahlung erfassten anteile von rektum und blase . 
 schlsselwrter : radiotherapie nach prostatektomie salvage - radiotherapie adjuvante radiotherapie dosis - volumen - histogramme prostata introduction the use of adjuvant or salvage radiotherapy after radical prostatectomy ( rp ) is still a source of controversy [ 14 , 9 , 1820 , 23 , 24 , 29 , 30 , 32 , 33 ]  . 
a number of retrospective single - institution studies confirmed a beneficial role for adjuvant radiotherapy [ 46 , 21 , 22 , 25 , 27 , 29 , 34 , 36 ] , while the final results of two phase iii trials addressing the question of the validity of adjuvant postoperative radiotherapy are awaited ( eortc 22911 , aro 96 - 02 )  . 
recently , the issue of the optimal dose of radiotherapy has been also raised with some retrospective data suggesting a potential increased benefit from the escalation of the dose [ 6 , 28 ]  . 
 however , no quantitative studies investigated the impact of prostatectomy on the anatomy of the pelvis , which is an important prerequisite for a precise definition of clinical target volume ( ctv )  . 
 moreover , no investigations tried to quantify possible systematic shifts of the bladder and the rectum due to prostatectomy and their possible impact on dose - volume histograms ( dvhs )  . 
 more in general , a number of points concerning the definition of ctv and planning target volume ( ptv ) in post - operative prostate radiotherapy have still to be addressed like interand intraobserver variability and the impact of organ motion . 
 a project involving two institutions ( national institute for cancer research in genoa and san raffaele hospital in milan , italy ) on the definition of target volumes in post - prostatectomy radiotherapy was started trying to give some answers to these questions . 
 here , we report the results of a study about the impact of rp on ctv definition and on the position of bladder and rectum and their implications for 3 - d crt . 
 imaging and co - registration procedures each patient underwent a planning ct between 1 week and 1 month before surgery ( ctpre ) ; ct was repeated in the same position 12 months after surgery ( ctpost )  . 
in spite of the attempt to keep rectum and bladder filling in a similar situation , large variations in bladder and rectum filling were evident in four of six patients each . 
however , no systematic trends between ctpre and ctpost were seen ( mean bladder volume ctpre : 77 23 cm3 ; ctpost : 65 29 cm3 ; mean rectum volume ctpre : 69 32 cm3 ; ctpost 64 26 cm3 ) , suggesting that the variation of filling between the two series was prevalently random for both rectum and bladder . 
 contouring ctv , rectum and bladder rectum , bladder and ctv were contoured on both ct scans ( pre and post ) for each patient by one observer ( gs )  . 
according with a definition previously followed by the authors [ 11 ] , the cranial and caudal limits of the rectum were assessed at the point where the rectum turns into the sigmoid and just above the anal verge , respectively . 
both rectum ( including filling ) and rectal wall were drawn . two different ctvs were contoured for each ct scan of each patient : ( 1 ) ctv1 : prostate + seminal vesicles in ctpre ; prostate + seminal vesicles bed in ctpost ; ( 2 ) ctv2 : prostate in ctpre ; prostatic bed in ctpost . at first , the observer defined the contours on ctpre ; after 1 week he defined the contours on ctpost , without knowing the patients name . 
its boundaries were : anteriorly , the pubic symphysis ; laterally , to include the levator ani muscle and some periprostatic fat with maximum extension up to the medial edge of the obturator internus muscle ; posteriorly , the rectal wall ; superiorly , the bladder ; inferiorly , 0.5 cm above the penile bulb . 
a : national institute for cancer research ; b : san raffaele hospital ; gls : gleason score ; ot : operative treatment ; psa : pros tate - specific antigen ; rp : radical prostatectomy ; turp : transurethral resection of the prostate . 
impact of prostatectomy on ctv and dvhs above and below the flexure , shown in figure 1 ; the location of the flexure was assessed by an independent observer without the information if the rectum referred to ctpre or ctpost scan . 
 this choice was suggested by the attempt to define two parts of the rectum with small ( caudal half ) or high ( cranial half ) impact of variable air / filling content in the rectum [ 13 ]  . 
 for the bladder ( figure 1 ) the analysis was restricted to the most caudal portion ( bottom ) in correspondence with the region of interface between the prostate and the bladder in the presurgical setting . 
this was due to the fact that in the upper portion of the bladder the deviations are expected to mostly depend on the random variable filling and not on the impact of prostatectomy . 
 dvhs of rectum and bladder ; irradiated ( iv ) and treated volume ( tv ) once the dose distribution of each planning for each ptv had been calculated , the cumulative dvhs referred to a single 2 - gy fraction were recovered for bladder , rectum ( solid organ ) and rectal wall . 
 in particular , we focused our attention on the fraction of rectum / bladder receiving > 95% of the icru dose [ 14 ] , once the dose is normalized to the isocenter dose in both situations ( pre and post ) , named v95 . 
 according to icru we calculated the fraction of body in cubic centimeters receiving > 95% and 50% of the icru dose , corresponding to the tv and the iv , respectively . 
 correlation between shifts of ctv / bladder / rectum , cranial / caudal limits of ctv and rectum / bladder v95 , tv and iv were also tested ( spearman test )  . 
 dose distribution : spatial variations in order to visualize the differences between preand post - surgery conformal planning on the ct images , the two dose distributions were subtracted ( pre post ) using an appropriate tool available on the cadplan tps ; a qualitative estimate of the spatial distribution of these differences relative to bony anatomy and location of the rectum and bladder before and after surgery could be appreciated on axial , coronal and sagittal slices . 
analyse der unterschiede zwischen prund postoperativer position von rektum und blase : unterschiede ergaben sich in den grau unterlegten regionen , nmlich den am weitesten kaudalen anteilen von rektum und blase . 
 the volumes of ctv1 , ctv2 , ptv1 , ptv2 , rectum and bladder preand post - rp were compared and deviations between preand post - surgery were tested through the wilcoxon matched - pair test . 
 spatial variations of ctv , rectum and bladder ( bev ) quantitative analysis in order to compare the shifts of ctv1 , ctv2 , rectum and bladder relative to the bony anatomy due to rp , beams eye view ( bev ) images of anterior and lateral beams were plotted . 
 for each patient average shifts of the posterior / anterior / lateral edges were then assessed ; mean values on the population were also considered , and statistical significance was tested ( wilcoxon matched - pair test )  . 
 for bladder and rectum different subanalyses were done : the rectum was considered to be composed of two portions , for ctv1 the average reduction was around 30% , while for ctv2 it amounted to around 50% . 
 in figure 2 we plotted the volumes of ctv1 / 2pre / post for the cranial border of ctvpost resulted to be more caudal on average of 1 and 1.5 cm for ctv1 and ctv2 , respectively , with a maximum difference up to 2.5 cm ; on the other hand , no systematic differences were found at the caudal border . 
no significant deviations could be appreciated on anterior - posterior bev images even if in two of six patients the ctv2post resulted to be symmetrically shrunk with respect to the ctv2pre of about 810 m concerning the bladder , a systematic large posterior shift of the bladder ( 1.5 cm on average ) in the region shown in figure 1 ( i.e. , interface between prostate and bladder in ctpre ) was found together with a relatively small shift in the caudal direction of the caudal border of the bladder . 
summary of the most significant differences between pre and postsurgical setting : differences were estimated by beam 's eye view ( bev ) lateral images ( wilcoxon test )  . 
zusammenfassung der bedeutendsten unterschiede zwischen prund postoperativer situation , ermittelt mit hilfe lateraler bev - ( beam 's - eye - view - ) darstellungen ( wilcoxon - test )  . 
percent and absolute ( cm3 ) reduction of clinical target volume ( ctv ) and planning target volume ( ptv ) after prostatectomy : mean values , range of variation , p - values ( wilcoxon test )  . 
prozentuale und absolute ( cm3 ) abnahme von klinischem zielvolumen ( ctv ) und planungszielvolumen ( ptv ) nach prostatektomie : mittelwerte , spannweite , p - werte ( wilcoxontest )  . 
 dvhs of rectum and bladder ; v95 , iv and tv table 4 gives a summary of v95 values ( % or cm3 of organs included in the 95% isodose ) , tv and iv ( cm3 of body included in the 95% and 50% isodose , respectively )  . 
 in particular , the reduction of v95 values for the rectal wall was more significant than for the rectum regarded as a solid , probably because the dvh of the wall was less affected than the dvh of the solid rectum by different status of filling . 
example of the different shapes of dose - volume histograms of the rectum wall ( cm3 ) before and after surgery ( four - field three - dimensional conformal radiotherapy technique )  . 
 as an example , the dvh of the rectal wall ( in cm3 ) referred to ctpre and ctpost for ctv1 and ctv2 of one patient is shown in figure 4 ; in general , a clear sparing of rectum and bladder could be appreciated even if considering the whole dvh . 
percent and absolute ( cm3 ) reduction of v95 for rectum ( solid and wall ) and bladder ; absolute reduction of the fraction of body included in the 95% isodose ( treated volume [ tv ] ) and in the 50% isodose ( irradiated volume [ iv ] ) : mean values , range of variation , p - values ( wilcoxon test )  . 
prozentuale und absolute ( cm3 ) abnahme von v95 von rektum und blase ; absolute verminderung des anteils innerhalb der 95% - isodose ( behandlungsvolumen [ tv ] ) und innerhalb der 50% - isodose ( bestrahlungsvolumen [ iv ] ) : mittelwerte , spannweite , p - werte ( wilcoxon - test )  . 
 we tried to find possible correlations between a number of dose / volume parameters ( ctv / ptv reduction , v95 , tv , iv ) and between these parameters and the shifts found through the bev - based analysis . 
a significant correlation between the previously reported posterior shift of the bladder in the lower part and v95 of the bladder ( when considering ctv2 ) was found ( figure 6 )  . 
 dose distribution : spatial variations when subtracting the dose distributions ( pre post ) , the obtained distribution of the differences seems to be have a characteristic shape ( figure 8 )  . 
 in particular , when looking at the central sagittal slice the plot of hot spots ( corresponding to regions irradiated in ctpre and unirradiated in ctpost ) and cold spots ( corresponding to regions irradiated in ctpost and unirradiated in ctpre ) , we could find a hot region at the cranial border in five of six patients for both ctv1 and ctv2 . 
 at the upper posterior border , in correspondence with the upper portion of rectum more affected by variable rectal filling , in three of six patients a hot spot was found , while in the remaining three a cold spot was detected , which was consistent with the random effect of variable filling . in the lower part , for most patients hot spots were evident at the posterior and cold spots at the anterior border , which was consistent with the previously reported anterior shift of ctv2 . 
 discussion and conclusion although the exact role of radiotherapy after prostatectomy is still unknown , a number of single - institution studies suggested some benefit for patients undergoing radiotherapy both in the adjuvant and salvage setting [ 19 , 23 ]  . 
 anyway , the increasing interest in postoperative radiotherapy concomitantly with the advent of 3 - d conformal techniques raise many questions on the problem of defining reliable and accurate ctvs and ptvs . 
 in the attempt to investigate this point , a number of studies were activated by our groups ( national institute for cancer research , genoa , and san raffaele hospital , milan , italy ) , including studies of the impact of interand intra observer / institute variability in defining the ctv , the im pact of organ motion and the current one of the impact of radical prostatectomy on the treated volume and on the dose distribution within rectum and bladder in a conformal approach . 
however , it has been our choice not to include pelvic lymph node stations ( typically obturator and external iliac ) , even if these had been sampled ( and then violated ) by the surgeon . 
 ive patients and where the prostate and seminal vesicles were before surgery for the operated patients , that represents our present clinical approach to postoperative patients regardless of pn stage . 
 positive deviations correspond to areas irradiated in the pre - surgery setting and not irradiated in the post - surgery setting ; negative deviations correspond to areas irradiated in the post - surgery setting and not irradiated in the pre - surgery setting . 
positive abweichungen entsprechen in der properativen situation bestrahlten , in der postoperativen situation nicht bestrahlten arealen ; negative abweichungen entsprechen in der postoperativen situation bestrahlten , in der properativen situation nicht bestrahlten arealen . 
our data show that the position of the rectum is relatively unchanged before and after surgery , upper border ( sigmoid flexure ) included ; therefore , no major changes in both rectal delineation and volume should be expected as a result of rp . 
since we were in a half - full / - empty situation and all patients were continent after rp , we observed only a slight nonsignificant reduction of mean bladder volume after surgery , and this fact should be taken into account when interpreting our findings . 
postoperatively , patients are often unable to fill their bladder for several weeks after surgery ( because of both the prolonged use of a catheter and possible problems with continence ) , and if this scenario is compared to a preoperative one in which the bladder was full , findings different from ours might be obtained . 
 finally , the upper margin of the ctv was more caudally defined in the postoperative setting and this can be due , at least in part , to the lack of preoperative ct scan [ 12 ]  . 
recently showed a tendency to underestimate the initial extension of the organs removed with a 1020% mean reduction of ptv length without the use of preoperative ct scans [ 12 ]  . 
on the other hand , based on the low yield of positive findings and the extra costs , the routine use of preoperative ct scan has been questioned by several authors [ 16 , 17 ] , and our approach reflects a realistic , though not desirable , scenario . 
 the anatomic variation of the bladder together with the smaller ctv leads to a reduction of tv and iv and , consequently , to a reduction of the portion of rectum and bladder included in the treatment fields . 
this fact should depend on the fact that it may be considered reasonably safe to include the whole prostatic fossa and periprostatic tissue taking the symphysis as the anterior limit . 
 intraobserver variability of the physician who contoured the volumes was investigated and found to be almost insignificant with respect to the large differences between the ctv before and after surgery . 
 on the other hand , preliminary results concerning interobserver variability indicate that the observer who contoured the ctv in this investigation did not have any systematic tendency to draw a more caudal ctv with respect to other observers . 
impact of prostatectomy on ctv and dvhs and possible postoperative radiotherapy against definitive radiotherapy , since this is only one minor aspect of a complex decision where other factors , such as control of disease and surgical morbidity , are likely to play a major role . 
while the rectum is spared by surgery , variable portions of the bladder ( neck , base ) are subject to surgery , and this may predispose to a reduced tolerance to radiotherapy . 
 within these limitations , our data suggest that dose es calation should be a more easily achievable goal in the postoperative setting with respect to the radical one , as we provided direct evidence that surgery brings a more favorable organ setup with a consequent reduction of the irradiated volume . 
 this investigation also clearly indicates that the treated volumes with and without the prostate are quite different , so that caution should be taken when interpreting toxicity data coming from experiences including naive and operated patients that do not take individual information on dose - volume coverage of organs at risk into consideration . 
wirth2 , thomas herrmann1 background and purpose : permanent interstitial brachytherapy by seed implantation is a treatment alternative for low - volume low - risk prostate cancer and a complex interdisciplinary treatment with a learning curve . 
the authors evaluated their learning curve based on dose - volume histograms and analyzed factors influencing implantation quality . patients and methods : since 1999 , 38 patients with a minimum follow - up of 6 months were treated at the authors institution with seed implantation using palladium - 103 or iodine - 125 , initially using the preplan method and later real - time planning . 
the dose - volume indices d90 , v100 , v150 , the dmax of preand postplans , and the size and position of the volume receiving the prescribed dose ( high - dose volume ) of the postplans were evaluated . 
the first five patients were treated under external supervision . results : patients were divided into three consecutive groups for analysis of the learning curve ( group 1 : n = 5 patients treated under external supervision ; group 2 : n = 13 patients ; group 3 : n = 20 patients )  . 
the relationship between high - dose volume and prostate volume showed a similar increase as the d90 , while the relationship between high - dose volume lying outside the prostate and prostate volume remained constant . 
an important factor influencing the learning curve in addition to the precision of seed positioning is organ volume definition on postimplant imaging . key words : prostate cancer brachytherapy permanent implants treatment planning dvh strahlenther onkol 2004 ; 180 : 5506 doi 10.1007 / s00066 - 004 - 1337 - 8 auswertung von dosis - volumen - histogrammen nach seed - implantation der prostata . 
die autoren nutzten dosis - volumen - histogramme der postplne , um die qualitt der behandlung im zeitverlauf zu beurteilen und zu analysieren . patienten und methodik : seit 1999 wurden am universittsklinikum dresden 38 patienten mit einer minimalen beobachtungszeit von 6 monaten mit palladium - 103und jod - 125 - seeds therapiert . 
ausgewertet wurden die dosis - volumen - kenngren d90 , v100 , v150 und dmax der prund postplne sowie die gre und lage des von der verschriebenen dosis umfassten volumens ( hochdosisvolumen ) der postplne . 
das verhltnis von hochdosisvolumen zu prostatavolumen zeigte einen hnlichen verlauf wie d90post , das verhltnis des auerhalb der prostata liegenden hochdosisvolumens zum prostatavolumen war im zeitverlauf konstant ( abbildung 2 )  . 
das verhltnis der prostatavolumina aus ct und transurethralem ultra1 department of radiotherapy and radiooncology , university hospital carl gustav carus at the technical university of dresden , dresden , germany , 2 department of urology , university hospital carl gustav carus at the technical university of dresden , dresden , germany . 
 eine wichtige ursache ist neben der przision der seed - positionierung die volumendefinition der prostata in den postplanbildern . schlsselwrter : prostatakarzinom brachytherapy permanentimplantate bestrahlungsplanung dvh introduction today , prostate cancer is the most common malignancy affecting men in north america and germany . 
with the widespread availability of prostate - specific antigen ( psa ) measurement and refined prostate biopsy techniques , there has been a marked stage shift together with an increase in the total number of cases diagnosed . 
for the treatment of localized prostate cancer in patients with a life expectancy of 10 years , definitive curative treatment options are recommended , since watchful waiting ( no treatment ) has been shown to lead to reduced cancer - specific survival . 
 interstitial brachytherapy with implantation of iodine - 125 ( 125i ) or palladium - 103 ( 103pd ) seeds is a minimally invasive curative treatment for organ - confined prostate cancer . 
while earlier uses of open prostatic seed implantation were disappointing [ 32 ] , technical refinements of transrectal ultrasound ( us ) have led to the development of us - guided perineal seed implantation [ 10 ]  . 
 a joint commission of the urologic and radiotherapeutic specialist societies in germany has recommended the application of permanent interstitial brachytherapy for patients with organ - confined disease and low - risk tumors only [ 31 ]  . 
according to these recommendations men with wellor moderately differentiated and low - volume tumors ( psa < 10 ng / ml , only one of six biopsies positive , gleason score < 7 ) should receive permanent interstitial brachytherapy as the only treatment . 
 furthermore , for reasons of technical feasibility and in order to reduce the risk of posttreatment voiding problems , further selection criteria concerning lower urinary tract function were recommended : ipss ( international prostatic symptom score ) < 10 points , maximum flow rate > 15 ml / s , residual urine volume < 50 ml , prostate volume < 50 ml [ 7 ]  . 
disease - free 5 - year and 10 - year survival rates of 71% and 60% have been reported for interstitial brachytherapy with or without ebrt [ 24 ]  . 
in this article our experience with postimplant dosimetry for the evaluation of implant quality in view of the learning curve involved in establishing this complex interdisciplinary treatment modality is reported . 
 the aforementioned stringent criteria for permanent interstitial brachytherapy by seed implantation were published in 2002 [ 32 ] , and some patients treated prior to the definition of these recommendations retrospectively did not fulfill these cri teria ( four patients had psa values between 10 and 20 ng / ml , five patients had ct2b disease )  . 
furthermore , three patients were deliberately treated by brachytherapy despite not fulfilling the recommended criteria , because no other curative treatment option was feasible ( two patients after surgery and radiotherapy for advanced testicular cancer ) or acceptable to the patient . 
prophylactic treatment by an - blocker for 4 weeks , an antibiotic for 10 days , and a nonsteroidal anti - inflammatory drug ( nsaid ) for 6 days was given . 
 in agreement with international recommendations [ 4 , 17 , 19 ] , patients implanted with 103pd ( patients 127 ) received a prostate - confined dose of 124 gy ( corresponding to the recommended 115 gy before correction of activity and air kerma strength by nist in 1999 [ 29 ] ) and patients implanted with 125i received 145 gy ( patients 2838 )  . 
the following criteria for the planning optimization of preplans were applied : v100pre ( prostate volume receiving the prescribed dose ) should be at least 98% of the prescribed dose ; dmax , pre for the urethra should not exceed 200 gy ( patients 112 ) or 300 gy ( patients 1338 ) ; dmax , pre for the rectal wall should not exceed 130 gy ( for palladium ) or 150 gy ( for iodine )  . 
approximately 2 weeks be fore implantation transrectal us for the establishment of the geometric prostatic data was performed ( volume study ) followed by computer - aided dosimetry planning ( brachy pro , prowess ) in order to determine the number , activity and position of seeds required . 
the position of the implanted peripheral seeds was marked in an intraoperative planning software system ( variseed , varian medical systems inc . ) , and the remaining 25% of total activity was then implanted into the inner prostatic regions according to the isodose distribution calculated by intraoperative planning . 
patients were discharged 24 h after catheter removal , if voiding clinical follow - up routine follow - up consisted of one visit after 4 weeks , 3monthly visits during the first 2 years , and 6 - monthly visits thereafter for another 2 years with assessment of psa , residual urine , digital rectal examination and assessment of symptoms according to the rtog / eortc score [ 27 ]  . 
 dosimetric evaluation of treatment all patients underwent ct scanning 4 weeks after seed implantation following the recommendations of the american brachytherapy society concerning postimplantation prostate edema and resulting changes in prostate volume [ 18 ]  . 
slice thickness and distance of ct planes were 4 m dose - volume histograms ( dvhs ) of prostate , rectum and in part of the urethra were calculated for the postplans with a planning system ( brachy pro , prowess )  . 
depending on ct slice thickness , seed marker design , distance between seeds and seed position ( straight vertical , tilted or angled ) , seeds were often visible on more than one ct slice . 
therefore , in order to identify possible seed overlap , the total number of seeds was also counted on additional pelvic anterior - posterior and oblique plain radiographs [ 18 ]  . 
 the cutoff between patient group 2 and 3 was set arbitrarily according to the d90post results ( patient number 19 , who was treated 19 months after the first patient )  . 
the obviously higher dmax , pre of the rectal wall in group 3 occurred after the change in nuclide from 103pd to 125i after patient 27 and the consecutive increase in the prescribed dose from 124 gy to 145 gy . 
corresponding figures were seen for the mean v100post ( 73.5% for group 2 , 88.2% for group 3 ) and for the mean v150post ( 43.1% in group 2 and 59.6% in group 3 , respectively )  . 
 in order to investigate the influence of implanted total activity and prostate volumes on the d90post , the activity per prostate volume was correlated with the d90post for those patients of group 2 and 3 who were treated with 103pd ( figure 4 )  . 
 [ 25 ] , in their series , reported a cutoff of d90post values of 88% of the prescribed dose of 145 gy ( nist - corrected ) using iodine . 
patients with d90post values above the cutoff value were significantly more likely to remain free from biochemical failure ( defined as a psa nadir > 1.0 ng / ml or two consecutive psa increases )  . 
 [ 20 ] reported a d90post cutoff of 90% ( for a prescribed dose of 120 gy using palladium or 144 gy using iodine ) and a relapse definition of three consecutive psa rises . 
suggest that a value of about 90% of the prescribed dose for 90% of the prostate volume represents a good implant quality and correlates with significantly better progression - free survival . 
gruppe 1 ( ( cid : 1 ) ) : fnf patienten , die unter anleitung von externem personal geplant und implantiert wurden ( vier patienten mit postplan ) ; gruppe 2 ( ( cid : 2 ) ) : erste 13 patienten , die von internem personal behandelt wurden ( definiert als lernphase ) ; gruppe 3 ( ( cid : 3 ) ) : folgende 20 patienten . ume definition in ct in comparison with mri and preplan us was taken . 
an opposite progression of d90post and the ratio of prostate volume on ct and transrectal us ( vct / vus ) was apparent in group 2 , indicating the contribution of con0 2 4 6 8 10 12 14 16 18 20 22 24 26 28 30 32 34 36 38 patient number 0 2 4 6 8 10 12 14 16 18 20 22 24 26 28 30 32 34 36 38 patient number figure 2 . 
high - dose volumes ( volume receiving the prescribed dose ) relative to prostate volumes ( closed symbols ) and percentage of high - dose volume lying outside the prostate ( open symbols ) for consecutive patients . 
hochdosisvolumen ( volumen , das die verschriebene dosis erhlt ) relativ zum prostatavolumen ( geschlossene symbole ) und anteil des hochdosisvolumens , das auerhalb der prostata liegt ( offene symbole ) fr alle patienten . 
ratio of prostate volumes by different imaging modalities : ct versus transrectal ultrasound ( us ; same groups as in figure 1 ) and mri versus us ( ) for six patients . 
the proportion of patients whose d90post exceeded 88% of the prescribed dose improved from 12% ( first 3 years ) to 26% ( 4th year ) , 66% ( 5th year ) , 67% ( 6th year ) , and 97% ( 7th year )  . 
 [ 12 ] analyzing the prostate volume receiving the prescribed dose ( v100post ) also support the existence of a learning curve and are in good agreement with data demonstrated here . 
the authors reported v100post values of 76% ( sd 12% ) for the first 30 patients versus 85% ( sd 7% ) for the following 33 patients as compared to 74% ( sd 13% ) in our group 2 versus 88% ( sd 8% ) in our group 3 . 
19 analyzed patients had a mean v100post of 47% in the postimplant ct performed several weeks after implantation , while postplans based on transrectal us performed directly after implantation had given an average v100post of 74% . 
in their series , the preplan method was inferior to the results obtained by intraoperative planning : the d90post increased from 53% to 113% and v100post from 58% to 95% . 
 the results of d90post depend on ( a ) the implanted total activity relative to the prostate volume , and ( b ) the position of the seeds relative to the contoured prostate . 
factor ( a ) can be excluded as a possible explanation for increasing d90post values during the learning phase , because no significant increase in the mean implanted activity per us prostate volume was seen ( figure 4 )  . 
the additional comparison of prostate volumes on ct and mr images for six patients ( figure 3 ) demonstrates the same probleall mri volumes matched well with the preimplant us volume . 
this can be interpreted as an indication that by 4 weeks after implantation the prostatic edema had resolved and that the ct prostate volumes were contoured too large during the learning phase . 
on the other hand , from the progression of the high - dose volume one would also expect an increasing percentage of the high - dose volume lying outside the prostate , which was not the case ( figure 2 )  . 
this , however , is probably not of importance , as no significant differences were found between the first nine ( palladium ) and the last eleven patients ( iodine ) of group 3 . 
evaluation of dvh in prostate cancer though the follow - up time is short , the clinical urethral and rectal side effects were much lower than expected on the basis of the postplans . 
 conclusion after analyzing the results and comparing them to data reported in the literature it can be concluded , that a learning phase has transformed into a technique with stable dosimetric results after the first 13 patients . 
as a consequence , the performance of an mri scan is now routinely integrated into the postplan procedure with the fusion of ct and mr images , which became possible due to a new planning software . 
combs1 , 2 , daniela schulz - ertner1 , 2 , christoph thilmann1 , 2 , lutz edler3 , jrgen debus1 , 2 background and purpose : the role of stereotactic radiosurgery ( srs ) alone or in combination with whole brain radiotherapy ( wbrt ) in the treatment of cerebral metastases from breast carcinoma is discussed controversially . 
 ten patients received srs alone ( group 1 ) , 13 patients were treated with wbrt and srs as a focal boost ( group 2 ) , and 39 patients received wbrt and salvage srs ( group 3 ) for recurrent metastases at a later time point . 
median local control intervals were 9 months for all patients , 6.5 months in group 1 , 4 months in group 2 , and 9 months in group 3 , respectively . 
 key words : brain metastases breast cancer whole brain radiation therapy stereotactic radiosurgery local control overall survival strahlenther onkol 2004 ; 180 : 5906 doi 10.1007 / s00066 - 004 - 1299 - x behandlung zerebraler metastasen des mammakarzinoms mit stereotaktischer radiochirurgie hintergrund und ziel : die behandlung zerebraler metastasen des mammakarzinoms mit stereotaktischer radiochirurgie ( srs ) allein oder in kombination mit einer ganzhirnbestrahlung ( wbrt ) wird derzeit kontrovers diskutiert . 
um die vorteile der srs in diesem kontext und den einfluss von prognostischen faktoren auf das gesamtberleben zu evaluieren , wurde eine retrospektive analyse durchgefhrt . patienten und methodik : zwischen 1986 und 2003 wurden 62 patientinnen mit 103 hirnmetastasen bei brustkrebs behandelt . 
 zehn patientinnen erhielten eine alleinige srs ( gruppe 1 ) , 13 patientinnen wurden mit wbrt und srs ( fokaler boost ) behandelt ( gruppe 2 ) , und 39 patientinnen erhielten eine wbrt und eine salvage - srs ( gruppe 3 ) bei progredienz der metastasen zu einem spteren zeitpunkt . ergebnisse : das mediane gesamtberleben war in der gruppe , die mit alleiniger srs behandelt wurde , tendenziell erhht im vergleich zu der gruppe , die eine wbrt mit srs als fokalem boost erhalten hatte . 
die mediane lokale kontrolle lag bei 9 monaten fr alle patientinnen , 6 , 5 monaten in gruppe 1 , 4 monaten in gruppe 2 and 9 monaten in gruppe 3 . 
es gab keine signifikanten unterschiede zwischen den einzelnen gruppen . schlussfolgerung : die alleinige srs ist eine effektive behandlungsmethode fr patientinnen mit ein bis drei hirnmetastasen bei mammakarzinoeine randomisierte studie zur weiteren evaluation der notwendigkeit einer wbrt bei diesen patientinnen sollte durchgefhrt werden . 
 schlsselwrter : hirnmetastasen mammakarzinom ganzhirnbestrahlung stereotaktische radiochirurgie lokale kontrolle gesamtberleben 1 department of radiation oncology , german cancer research center ( dkfz ) , heidelberg , germany , 2 department of radiation oncology , university of heidelberg , heidelberg , germany , 3 department of biostatistics , german cancer research center ( dkfz ) , heidelberg , germany . received : march 12 , 2004 ; accepted : june 30 , 2004 strahlenther onkol 2004 no . 
srs for brain metastases from breast cancer introduction breast cancer is the second most common cause of brain metastases with approximately 1015% of patients presenting with clinically overt cerebral metastases , whereas 30% of cerebral metastases are detected in autopsies [ 11 , 47 ]  . 
radiotherapy is the standard treatment of cerebral metastases , considering the patients prognosis and quality of life , resulting in transitory amelioration of the neurologic deficits in 6086% of patients . 
neurosurgical resection is a treatment alternative that is limited to a small number of intracranial metastases only in patients without extracerebral manifestations or controlled extracerebral disease [ 32 , 54 ]  . 
 stereotactically performed radiosurgery ( srs ) is an alternative in patients with one to three brain metastases , a patient collective with favorable outcome compared to patients with four or more brain metastases [ 27 ]  . 
by srs , high single doses of radiation can be applied by precise focal delivery to brain metastases , while side effects and complications are minimized [ 10 , 19 , 36 ]  . 
 very few postradiologic complications occur after srs , which include transient perifocal edema , delayed intratumoral hemorrhage or necrosis requiring neurosurgical intervention . in the past , the effectiveness of srs has been evaluated in patients with brain metastases from different primaries . 
the present analysis focuses on the role of srs in the management of patients with cerebral lesions from breast cancer , who represent a subgroup of patients with favorable outcome [ 3 , 35 , 53 ]  . 
until now , the indication for wbrt alone , srs alone as a primary treatment or wbrt with srs as a salvage treatment , or a combination of both in the primary situation is not strictly set up in the case of cerebral metastases from breast cancer . 
the first group ( group 1 ) consisted of ten patients with one to three brain metastases who received srs alone , the second group ( group 2 , 13 patients ) received wbrt and srs as a focal boost to one to three brain metastases , and the third group ( group 3 ) contained 39 patients treated with wbrt as an initial treatment who received srs for recurrent metastases at a later time point . 
in some patients the choice for one of the treatment schedules was based on certain patient - specific factors such as number of metastases , size of the lesion ( s ) , and karnofsky performance score . 
using the recursive partitioning analysis ( rpa ) classification for brain metastases , rpa score was 1 in 21 , 2 in 38 , and 3 in three patients , respectively [ 15 ]  . 
the initial tumor stage was stage i in twelve patients , stage iia and iib in twelve patients each , iiia and iiib in one patient each , and stage iv in seven patients . 
for srs , the target was defined as contrast - enhanced areas , adding a 1to 2 - mm safety marg patients in group 1 received srs alone with single doses between 15 and 20 gy ( median single dose 20 gy ) dependent on tumor size and location . 
total survival time was defined as the time from first diagnosis of breast cancer to death or end of follow - up , cerebral metastases - free time was collected as the time from first diagnosis of breast cancer to the first diagnosis of brain metastases . 
 statistical analysis statistical analysis included overall survival , local control ( freedom from progression of lesions treated with srs ) , locoregional control ( freedom from development of new brain metastases ) , and progression - free survival . 
 age and stage at primary diagnosis of breast cancer , karnofsky performance score , size and number of cerebral lesions , extracerebral disease , previous neurosurgical resection , and clinical symptoms before srs were determined using the log - rank test and the univariate and multivariate cox proportional hazards model , respectively [ 7 ]  . 
ten patients developed perifocal edema without clinical symptoms ( ctc1 ) , in one patient nausea and vomiting developed , and one patient suffered from intermittent neurologic deficits ( reduction of visual acuity )  . 
48 deaths were tumor - associated , i.e. , extraand / or intracranial tumor progression , two non - tumor - related deaths could be recorded , one due to pulmonary embolism and one of pneumonia . 
the median time from primary diagnosis to brain metastases was 47 ( range 0216 ) months , the median total survival time from primary diagnosis 64 ( range 14408 ) months . 
srs for brain metastases from breast cancer group 1 group 2 group 1 group 2 5 10 15 20 25 30 35 40 45 50 55 5 10 15 20 25 30 35 40 45 50 55 figure 1a abbildung 1a time ( months ) figure 1b abbildung 1b time ( months ) figures 1a and 1b . 
 we evaluated the statistical significance of prognostic factors on overall survival including age , karnofsky performance score , initial stage of disease , extracerebral manifestations , number and size of brain metastases , presence of neurologic symptoms , and neurosurgery prior to radiotherapeutic treatment ( table 2 )  . 
patients treated with srs only showed an increase in overall survival compared to wbrt with a focal boost ( p = 0.036 ) ( figures 1a and 1b )  . 
 tumor control median local and locoregional tumor control times were comparable for the three groups with a median local control of 9 months , while the median locoregional tumor control was 6 months . 
the difference between group 1 and 2 was not the median overall locoregional brain control was 6.5 months for group 1 , 4 months for group 2 , and 7 months for group 3 , respectively . 
 in all patients developing tumor progression , 53% suffered from cerebral tumor progression , 19% from extracerebral tumor progression , and 28% of all patients showed tumor progression extracranially and intracranially . 
lokoregionre kontrolle bei patientinnen , die wegen ein bis drei hirnmetastasen bei brustkrebs nur mit srs ( gruppe 1 ) oder mit wbrt und srs als fokalem boost ( gruppe 2 ) behandelt wurden ( p = 0 , 66 )  . 
patients with brain metastases from breast cancer treated with focal therapy , e.g. , surgery , have the longest survival rates of all cancer groups [ 3 , 20 , 35 , 53 ]  . 
second , relatively long 2 - year survival rates of 25% have been reported in contrast to patients with cerebral metastases from lung cancer , colon cancer or melanoma [ 52 , 53 ]  . 
our data with a median overall survival after srs of 15 months supports this finding that breast cancer patients with brain metastases have a favorable outcome as compared to patients with brain metastases from other primaries [ 20 ]  . 
patients with breast cancer very rarely present with brain metastases before primary diagnosis , the median interval between primary diagnosis and brain metastases being about 34 months [ 11 , 49 ]  . 
commonly , the presence of brain metastases is highly associated with very aggressive disease , a negative hormone receptor status , with relatively young age , and the presence of extracranial metastases , mainly to lung , liver and bones [ 43 , 46 ]  . 
 historically , all patients with brain metastases were treated with wbrt , resulting in overall survival times after diagnosis of brain metastases between 4 and 6 months [ 14 , 23 , 25 ]  . 
a commonly used wbrt regimen in the usa for the treatment of brain metastases is 30 gy in ten fractions , but due to high early and late toxicity fractionation should be tailored to the individual patient depending on overall performance status and overall prognosis . 
 long - term risks in cases of prolonged survival after wbrt are subacute leukoencephalopathy , progressive dementia , and ataxia [ 2 , 8 , 9 , 33 ]  . 
in patients with a solitary brain metastasis , surgical resection can be a possible treatment , the main goal being the immediate relief of symptoms , histological confirmation of diagnosis , and local control [ 49 ]  . 
a combination of neurosurgical resection of accessible metastases with postoperative wbrt has been shown to have a significant impact on overall survival [ 31 , 32 , 48 ]  . 
reported that neurosurgical resection followed by wbrt with 40 gy and a 10 - gy boost to the metastatic site increased local control and survival as compared to neurosurgery and wbrt alone [ 38 ]  . 
a recent study comparing surgical resection and srs in the treatment of solitary brain metastasis has revealed no significant difference in overall survival between these two therapeutic options supporting the idea , that srs is another effective treatment alternative for solitary brain metastases [ 30 ]  . 
considering the patients disease and medical condition and respecting the approximate time of life left , time - saving treatments , especially with very few side effects should be considered . 
especially in the case of patients with breast cancer , commonly associated with a favorable outcome , it should be evaluated whether wbrt with all known side effects should be the treatment of choice as compared to srs in patients with one to three brain metastases . 
in accordance with data found in the literature [ 12 ] , we could show that in patients with one to three cerebral lesions , the number of brain metastases does not significantly influence overall survival . 
however , a number of studies found in the literature support the idea , that patients with a single brain metastasis survive longer than patients with multiple lesions [ 28 , 34 , 50 ]  . 
 a main hallmark of srs is the application of high doses to the affected area and clinically insignificant doses to the surrounding brain [ 13 , 36 , 49 ]  . 
 recent randomized trials have shown that srs in combination with wbrt results in significantly increased median survival times and local control as compared to wbrt alone [ 44 , 45 ]  . 
report that local tumor control is reduced in patients receiving srs only compared to wbrt and srs , although no significant difference in overall survival has been found [ 42 ]  . 
 the same group added cyclophosphamide and doxorubicin in 26 further patients , leading to a survival of 12 months for responders but only 2.4 months for nonresponders [ 39 ]  . 
a phase ii trial showed partial response and disease stabilization rates of 4% and 17% , respectively , in heavily pretreated patients with brain metastases from solid tumors [ 5 ]  . 
 in the future , controlled randomized prospective studies are recommended to compare srs alone with wbrt and srs in patients with one to three brain metastases with equivalent clinical characteristics . 
a randomized multicenter clinical phase iii trial of the eortc is currently investigating the question whether wbrt can be omitted in patients with one to three brain metastases and controlled extracranial disease after srs or surgical resection . 
investigated gamma knife radiosurgery for patients with brain metastases from breast cancer who were candidates for high - dose chemotherapy and bone marrow transplantation because of advanced breast cancer [ 24 ]  . 
 they concluded from their experience in twelve patients that srs can be used effectively for the initial management of brain metastases to avoid or delay wbrt in patients treated previously with high - dose chemotherapy . 
the authors concluded from their results that patients with one to three brain metastases should be considered for stereotactic radiosurgery , and that wbrt as a palliative treatment might be delayed . 
 although wbrt is the standard treatment for brain metastases in patients with more than four brain metastases , an srs boost might be considered for one to three brain metastases . 
however , as to whether srs alone in patients with one to three brain metastases and an overall good performance status yields similar control probability compared to wbrt is still unclear . 
however , due to the retrospective nature of this study it cannot be excluded that a selection bias is responsible for the favorable outcome in patients of group 1 and 2 . 
es ist von besonderer klinischer bedeutung , inwieweit sich eine strahleninduzierte lokale zytokinproduktion im lungengewebe in erhhten zytokinspiegeln im blut widerspiegelt und mglicherweise die entwicklung einer radiogenen lungenschdigung vorherzusagen erlaubt . 
 ergebnisse und schlussfolgerung : die wichtigsten inflammatorischen zytokine der strahlenreaktion der lunge umfassen tumornekrose - faktor ( tnf - ) , interleukin - 1 ( il - 1 ) und interleukin - 6 ( il - 6 )  . 
klinische studien zur bedeutung von zytokinplasmaspiegeln fr die prdiktion einer radiogenen lungenschdigung zeigen viel versprechende erste ergebnisse : erhhte tgf - - plasmaspiegel whrend der radiotherapie scheinen eine prognostische bedeutung fr die entwicklung einer klinisch apparenten radiogenen pneumonitis zu besitzen . 
 schlsselwrter : radiogene lungenreaktion pneumonitis zytokine radiotherapie strahlenther onkol 2004 ; 180 : 5419 doi 10.1007 / s00066 - 004 - 1279 - 1 the relevance of cytokines in the radiation - induced lung reaction . 
it is of special clinical significance , how far local radiation induced cytokine production in the lung tissue may be reflected in increased cytokine blood levels in patients during radiotherapy and may predict the later development of radiation - induced lung damage . 
 results and conclusion : the major pro - inflammatory cytokines in the radiation response of the lung include tumor necrosis factor ( tnf - ) , interleukin - 1 ( il - 1 ) , and interleukin - 6 ( il - 6 )  . 
first approaches with radioprotective agents and gene therapy to modify radiation - induced cytokine expression have been investigated for prevention of late effects of irradiation lung damage in animal experiments . 
the biological impacts of endogenous radiation - induced cytokine production by tumor cells in respect of tumor behavior , potential damage to normal tissue , and clinical status of the host still need to be determined more precisely . 
 key words : radiation - induced lung reaction pneumonitis cytokines radiotherapy 1 abteilung fr strahlentherapie , radiologische klinik , universitt des saarlandes , homburg / saar , 2 sektion fr strahlenbiologie und molekulare umweltforschung , universittsklinik fr radioonkologie , tbingen . 
zytokine und radiogene lungenreaktion radiogene lungenreaktion bei der radiotherapie im brustraum gelegener tumoren ist es trotz des einsatzes moderner konformaler bestrahlungsplanungsund applikationstechniken unumgnglich , gesundes lungengewebe mit einer bedeutenden strahlendosis zu erfassen . 
 klassifikationssysteme das klassifikationssystem der radiation therapy oncology group ( rtog ) und der european organization for research in the treatment of cancer ( eortc ) basiert sowohl auf klinischen symptomen und deren ansprechen auf therapeutische manahmen als auch auf radiologischen kriterien . 
die stadieneinteilung nach morgan & seaton basiert auf einer einfachen klinischen schweregradeinteilung der kurzatmigkeit und korreliert dementsprechend mit dem ausma der klinischen beeintrchtigung des patienten infolge der lungenschdigung [ 40 ]  . 
 pathophysiologie und histopathologie wenngleich vielfltige vernderungen in smtlichen lungenkomponenten zur strahleninduzierten lungenschdigung beitragen , scheint die schdigung der typ - ii - pneumozyten und der endothelzellen eine zentrale pathophysiologische bedeutung fr die radiogene lungenreaktion zu besitzen . 
entscheidend fr die effektivitt der atmung ist die funktion der alveolokapillren membran , zusammengesetzt aus auslufern der typ - iund - ii - pneumozyten ( alveolarepithel ) und dem kapillarendothel . 
in der histopathologischen einteilung der radiogenen lungenreaktion von rubin & casarett wider [ 39 , 54 ] : ( cid : 127 ) latenzphase ( bis zu 4 wochen nach bestrahlung ) whrend der latenzphase der pneumonitis lassen sich elektronenmikroskopisch typische ultrastrukturelle lsionen der typ - iund - ii - pneumozyten sowie des endothels beobachten . 
der durch eine verminderte sekretion hervorgerufene mangel an surfactant bewirkt eine exsudation von fibrin in den alveolarrau darber hinaus kommt es zu einem ablsen der die alveolen auskleidenden typ - i - pneumozyten . 
sie sind gekennzeichnet durch eine weitere exsudation von proteinen in den alveolarraum , eine verdickung der alveolarsepten , ein interstitielles dem , eine obstruktion der kapillaren durch thrombozytenaggregate , fibrinund kollagenablagerungen , einen weiteren verlust von typ - i - pneumozyten , eine hyperplasie und zunahme der typ - ii - pneumozyten sowie eine infiltration des lungenparenchyms mit inflammatorischen zellen . 
 ( cid : 127 ) sptphase ( ab 6 monaten nach bestrahlung ) die sptphase der bestrahlungsreaktion , die dem klinischen bild der pulmonalen fibrose entspricht , ist durch einen verlust von kapillaren , eine ausgeprgte verdickung der alveolarsepten , eine verkleinerung des alveolarraums sowie eine generalisierte fibrosierung infolge vermehrter kollagenablagerung charakterisiert . 
zytokine sind lsliche proteine und peptide , die als hochspezifische mediatorsubstanzen bereits in nanobis pikomolaren konzentrationen biologisch wirksam werden und die interaktionen zwischen unterschiedlichen zellen vermitteln und regulieren [ 11 ]  . 
 in tierexperimentellen studien wurde die mrna - expression verschiedener zytokine ( tumor nekrose faktor [ tnf - ] , interleukin - 1 [ il1 ] , il - 1 , transforming growth factor [ tgf - ] ) und kollagengene ( kollagen i , iii , iv und fibronektin ) im lungengewebe zu verschiedenen zeitpunkten ( 1 tag bis 26 wochen ) nach ganzlungenbestrahlung untersucht [ 19 , 30 , 31 ]  . 
in diesen studien konnte gezeigt werden , dass bereits in den ersten tagen nach bestrahlung von lungengewebe eine kaskade von zytokinen initiiert wird , die fr wochen bis monate persistiert und schlielich zu einer histologisch nachweisbaren fibrosierung fhrt [ 55 ]  . 
zeigen , dass die inflammatorischen zytokine tnf , il - 1 und il - 1 bereits in den ersten stunden ( 1 , 2 , 4 , 8 h ) nach bestrahlung induziert werden und dass eine fraktionierte bestrahlung diese zytokinexpression prolongiert ; durch die gabe von kortikosteroiden konnte die strahleninduzierte zytokinexpression reduziert werden [ 29 ]  . 
die tgf - - mrna - expression im gesamtlungengewebe und die tgf - - proteinexpression in der bal - flssigkeit ( bronchoalveolre lavage ) bei ratten nach thorakaler bestrahlung mit 15 bzw . 
die bestrahlung bewirkte sowohl eine vermehrte tgf - - mrna - expression im lungengewebe als auch eine erhhung der tgf - - proteinproduktion in der bal - flssigkeit mit einem maximum nach 36 wochen ; dieses maximum der tgf - - expression korrelierte zeitlich mit dem einstrmen inflammatorischer zellen in die bal - flssigkeit bei den versuchstieren und ging einer fibrosierung des lungengewebes voraus [ 68 ]  . 
zu beginn der histologisch nachweisbaren pneumonitis ( 2 und 4 wochen nach bestrahlung ) erreichte die tgf - - mrnaexpression maximale werte und nahm im weiteren verlauf ( 8 , 16 und 24 wochen nach bestrahlung ) allmhlich ab . 
die erhhte tgf - - mrna - expression in den ersten stunden nach der lungenbestrahlung mit 12 gy korrelierte mit dem immunhistochemischen nachweis positiver alveolarmakrophagen im lungenparenchywhrend der radiogenen pneumonitis waren neben inflammatorischen zellen auch typ - iipneumozyten und vereinzelt fibroblasten positiv fr tgf -  . 
die differierenden zytokinexpressionsmuster bei diesen mausstmmen lassen den schluss zu , dass die zytokine tgf - , tnfund il - 1 zur fibrosierungsreaktion beitragen , whrend il - 1 mglicherweise eine protektive wirkung besitzt . 
zytokine und radiogene lungenreaktion eine geringe tgf - - mehrexpression ( auf mrnaund proteinebene ) 24 h nach bestrahlung nachweisbar ; diese geringe tgf - - mehrexpression korrelierte mit nur geringen histopathologischen vernderungen whrend des gesamten untersuchungszeitraums [ 50 ]  . 
 bereits 1 h nach bestrahlung mit 12 gy war eine erhhte tnf - mrna - expression im lungengewebe nachweisbar ; die zu diesem zeitpunkt durchgefhrten immunhistochemischen untersuchungen zeigten ein intensiv und homogen fr tnf gefrbtes bronchialepithel . 
darber hinaus konnten wir in weiteren immunhistochemischen untersuchungen zeigen , dass bereits in den ersten stunden nach bestrahlung sowie im rahmen der weiteren entzndungsreaktion nicht nur tnf - , sondern auch il - 1 und il - 6 im bronchialepithel stark exprimiert werden . 
 genetische grundlage der strahlensensitivitt : vergleich der zytokinexpression bei fibroseresistenten und - sensiblen mausrassen quantitative histologische untersuchungen im tiermodell konnten zeigen , dass die ausprgung und das ausma einer strahleninduzierten lungenschdigung von der jeweils untersuchten mausrasse abhngig sind . 
whrend bei den cba und c3h - mausrassen die akute entzndungsreaktion des lungengewebes nach strahlenexposition ohne nachfolgende fibrosierung abklingt , findet man bei c57 - mausstmmen eine ausgeprgte fibrosierungsreaktion der lunge [ 14 , 20 , 22 , 59 , 60 ]  . 
 whrend die tnf - - proteinexpression keine bedeutenden unterschiede zwischen den beiden mausrassen aufwies , wurde bei der fibrosesensiblen mausrasse eine erhhte tgf - produktion in der latenzund intermedirphase beobachtet . 
so zeigen beispielsweise lungenfibroblastenpopulationen des menschen [ 47 ] , der ratte [ 26 ] und der maus [ 43 ] in vitro eine stimulation der tgf - - produktion um den faktor 23 nach strahlenexposition im einzeldosisbereich von 25 gy . 
im kontext dieser untersuchungen konnte darber hinaus dargestellt werden , dass die strahleninduzierte expression von tgf1 den terminalen differenzierungsprozess von progenitorfibroblasten zu hochgradig kollagen synthetisierenden postmitotischen funktionsfibrozyten reguliert [ 26 , 43 ]  . 
hierbei wird allerdings derzeit diskutiert , inwiefern die strahleninduzierte neusyn1 ( ltgfthese von latentem tgf1 ) und / oder die nachgewiesene , durch strahlung induzierte aktivierung des extrazellulren ltgf1 erforderlich sind , um die tgf1 - abhngige regulation der zellzykluskontrolle und differenzierung von fibroblasten in gang zu setzen [ 18 , 25 ]  . 
 1 zu aktivem tgfmodifikation der strahleninduzierten zytokinexpression im lungengewebe in aktuellen tierexperimentellen untersuchungen wurden verschiedene substanzen hinsichtlich ihrer mglichen pharmakologischen modifikation der strahleninduzierten zytokinexpression im lungengewebe untersucht , mit dem ziel , die radiogene zytokinvermittelte lungenschdigung zu reduzieren . 
konnten in einem tiermodell mit hemithorakaler einzeitbestrahlung bei ratten zeigen , dass durch die zytoprotektive substanz ethyol { amifostin ; ethanthiol , 2 - [ ( 3 - amino - propyl ) - amino ] - dihydrogenphosphat ( ester ) } sowohl die expression und als auch die aktivierung von tgf1 im lungengewebe der versuchstiere supprimiert wird und dass infolgedessen die tgf1 - plasmaspiegel im vergleich zu den kontrolltieren erniedrigt waren . 
in eigenen tierexperimentellen untersuchungen mit ganzlungenbestrahlung bei c57bl6 - musen konnten wir zeigen , dass durch pentoxifyllin , einen tnf - - synthese - inhibitor , nicht nur die tnf - - expression auf mrnaund proteinebene , sondern auch die inflammatorische zellinfiltration des lungenparenchyms reduziert werden kann [ 53 ]  . 
erste untersuchungen zur radioprotektiven gentherapie mit der intratrachealen injektion eines magnesium superoxide dismutase ( mnsod ) plasmid / liposome - komplexes bei c57bl / 6 - musen zeigten eine leicht reduzierte mrna - expression von tnf - , il - 1 und tgfim lungengewebe . 
 klinische bedeutung von zytokinblutspiegeln fr die ermittlung einer radiogenen lungenschdigung die ermittelten toleranzdosen und - volumina sowie die pneumonitisinzidenzen bei den verschiedenen bestrahlungsindikationen basieren auf empirisch gewonnenen daten unter bercksichtigung der physikalischen bestrahlungsparameter . 
wie bereits im vorherigen abschnitt referiert , belegen die in den letzten jahren auf der molekularen ebene gewonnenen erkenntnisse , dass zytokine als mediatoren mageblich an der regulation inflammatorischer und fibrogener reaktionen der strahleninduzierten lungenschdigung beteiligt sind . 
daher werden zytokine , deren unterschiedliche expression mglicherweise fr die zu beobachtende heterogenitt der normalgewebsreaktion verantwortlich ist , im blutplasma / - serum bei patienten bestimmt , die sich aufgrund maligner erkrankungen einer radiound / oder chemotherapie unterziehen . 
zytokine und radiogene lungenreaktion tgfist im hinblick auf die bestrahlungsinduzierte fibrosierung wahrscheinlich das wichtigste zytokin , da er eine ganze reihe verschiedener prozesse initiiert , die letztendlich zu einer kollagenakkumulation fhren [ 36 ]  . 
darber hinaus stimuliert tgfindirekt ber die induktion von platelet derived growth factor ( pdgf ) die fibroblastenproliferation und bewirkt eine vorzeitige differenzierung der fibroblasten zu postmitotischen fibrozyten mit erhhter kollagensynthese [ 46 , 47 ]  . 
es ist folglich von besonderer klinischer bedeutung , inwieweit tgf - - blutspiegel whrend der radiotherapie strahleninduzierte lokale vernderungen der tgf - - expression im lungengewebe widerspiegeln und somit die entwicklung einer radiogenen lungenschdigung vorherzusagen erlauben . 
im klinischen bereich wurde eine korrelation zwischen zirkulierenden tgf - - blutspiegeln und der inzidenz pulmonaler komplikationen erstmals bei pa tientinnen beobachtet , die aufgrund eines fortgeschrittenen mammakarzinoms mit hochdosischemotherapie und nachfolgender autologer knochenmarktransplantation behandelt wurden [ 5 ]  . 
in spteren klinischen studien konnte dieselbe arbeitsgruppe zeigen , dass bei patienten , die sich aufgrund eines bronchialkarzinoms einer radiotherapie unterzogen , anhaltend erhhte tgf - - plasmaspiegel whrend der radiotherapie mit einer deutlich erhhten pneumonitisinzidenz korrelierten [ 1 , 2 , 4 , 33 , 68 ]  . 
in folgenden studien wurden von dieser arbeitsgruppe patienten mit nichtkleinzelligem bronchialkarzinom aufgrund entsprechend niedriger tgf - - plasmaspiegel fr eine dosiseskalation selektioniert , ohne dass bei diesen patienten pulmonale komplikationen auftraten [ 3 ]  . 
die kombinierte erfassung der tgf - - serumkonzentration am ende der radiotherapie sowie der v30 ( = anteil des gesamtlungenvolumens in prozent , das mit 30 gy bestrahlt wurde ) erlaubte eine prognostische einteilung der patienten in unterschiedliche risikogruppen ( low , intermediate , high risk ) mit entsprechend signifikant unterschiedlichen pneumonitisinzidenzen [ 24 ]  . bislang liegen klinische studien zur prognostischen bedeutung von zytokinplasmaspiegeln berwiegend fr tgf vor , obwohl tierexperimentelle untersuchungen belegen , dass offensichtlich verschiedene zytokine an der strahleninduzierten lungenschdigung beteiligt sind ; inwieweit sich eine strahleninduzierte expression weiterer zytokine im lungengewebe auch in erhhten blutkonzentrationen widerspiegelt , ist gegenstand aktueller forschung . 
wurden die il - 6und tnf - konzentrationen im blutplasma bei patienten mit berwiegend nichtkleinzelligem bronchialkarzinom vor , whrend und nach der bestrahlungsbehandlung bestimmt und mit dem auftreten einer klinisch apparenten pneumonitis korreliert [ 12 ]  . 
eine korrelation zwischen erhhten tnf - - plasmaspiegeln und dem auftreten einer radiogenen pneumonitis wurde nicht beobachtet . tumoreigene strahleninduzierte zytokinproduktion : klinische bedeutung fr die radiogene lungenschdigung ? die nach radiotherapie einsetzende fibrogenese des normalgewebes ist mglicherweise nicht allein auf eine lokale bestrahlungsinduzierte produktion von tgfzurckzufhren . 
so lie sich bei transgenen musen , die in der leber tgfberexprimieren , nicht nur in der leber , sondern insbesondere auch in extrahepatischen organen eine fibrosierung infolge erhhter tgf - - blutkonzentrationen nachweisen [ 56 , 58 ]  . 
im vergleich zu normalen , nicht transformierten zellen sezernieren viele tumorzellen , insbesondere auch bronchialkarzinomzellen , erhebliche mengen tgfnicht nur in vitro [ 42 ] , sondern auch in vivo [ 6 , 7 ]  . 
dagegen war in frhen stadien des mammakarzinoms ( stadium i und ii ) der tgf - - plasmaspiegel nur bei 25% der patientinnen erhht ; eine verringerung der tgf - plasmaspiegel nach chirurgischer exzision wurde nicht beob achtet [ 62 ]  . 
darber hinaus knnen sie als serologische marker fr die frhzeitige erkennung des hepatozellulren karzinoms eingesetzt werden , mit einer im vergleich zum - fetoprotein hheren sensitivitt und einer vergleichbaren spezifitt [ 61 , 63 ]  . 
 fr die tumorgenese ist tgfaufgrund folgender aspekte von bedeutung : er reguliert die zellproliferation in zellspezifischer weise ; fr die meisten epithelialen , endothelialen und hmatopoetischen zellen ist er der strkste bekannte wachstumsinhibitor ( reversibler g1 - arrest )  . 
da die hauptmenge des im blutserum / - plasma zirkulierenden tgfin einer biologisch inaktiven form an 2 - makroglobulin gebunden vorliegt , bewirken erhhte blutspiegel per se nicht unbedingt eine gewebsfibrosierung . 
 die auswirkungen einer mglichen tumorzelleigenen tgf - - produktion sowohl auf den tumor selbst als auch auf das umliegende gewebe und ihre systemischen manifestationen sind insbesondere vor dem hintergrund , dass durch ionisierende strahlung ltgfaktiviert wird , bisher nur unzureichend untersucht . 
zeigen , dass bei fnf von insgesamt 13 verschiedenen knochenund weichteilsarkomzelllinien die tnf - - expression sowohl auf proteinals auch auf mrna - ebene nach einer einzeitbestrahlung mit 5 gy hochreguliert wurde [ 27 ]  . 
von unserer arbeitsgruppe wurden zwlf verschiedene aus ewing - sarkomen sowie peripheren primitiven neuroektodermalen primrtumoren ( ppnet ) und metastasen isolierte tumorzelllinien hinsichtlich ihrer bestrahlungsinduzierten tnf - - expression zunchst in vitro und , nach ihrer etablierung als xenograft - tumoren auf der nacktmaus , in vivo untersucht [ 49 , 52 ]  . 
da tnfals proinflammatorisches zytokin entzndungsreaktionen induziert und darber hinaus ausgeprgte systemische wirkungen aufweist , folgern wir , dass eine bestrahlungsinduzierte tnf - produktion im tumorgewebe mglicherweise nicht nur fr den tumor selbst , sondern auch hinsichtlich einer mglichen schdigung des umliegenden normalgewebes und fr den klinischen status des patienten von wesentlicher bedeutung ist . abbildung 2 zeigt schematisch , dass durch die bestrahlung nicht nur im normalen lungengewebe , sondern auch im tumorgewebe zytokine induziert werden , die die strahlenreaktion auch des normalen lungengewebes beeinflussen knnen . 
increased cytokine blood levels as a result of radiation - induced cytokine expression in normal and tumor tissue : after irradiation cytokines are locally produced in normal lung tissue and possibly in the tumor and mediate the radiation - induced tissue reaction . 
a tumor - derived cytokine production may have effects not only on the tumor itself but also on the surrounding normal tissue and the whole organisincreased cytokine blood levels result from the cytokine expression in the normal and tumor tissue . 
zytokine und radiogene lungenreaktion schlussfolgerung die in den letzten jahren gewonnenen daten belegen , dass die strahlungsinduzierte lungenschdigung ein multizellulrer prozess ist , bei dem die interzellulre kommunikation zwischen den verschiedenen zellarten ber ein komplexes netzwerk interagierender zytokine erfolgt . 
klinische studien zur prognostischen bedeutung von zytokinplasmaspiegeln fr die ermittlung einer radiogenen lungenschdigung zeigen viel versprechende erste ergebnisse : erhhte tgf - - plasmaspiegel whrend der radiotherapie scheinen eine prognostische bedeutung fr die entwicklung einer klinisch apparenten radiogenen pneumonitis zu besitzen . 
magnesium superoxide dismutase ( mnsod ) plasmid / liposome pulmonary radioprotective gene therapy : modulation of irradiation induced mrna for il - 1 , tnf - , and tgfcorrelates with delay of organizing alveolitis / fibrosis . 
early and persistent alterations in the expression of interleukin - 1 , interleukin - 1 and tumor necrosis factor mrna levels in fibrosis resistant and sensitive mice after thoracic irradiation . 
a little to a lot or a lot to a little ? an analysis of pneumonitis risk from dose volume histogram parameters of the lung in pa tients with lung cancer treated with 3 - d conformal radiotherapy . 
9 urban & vogel strahlentherapie strahlentherapie und onkologie und onkologie original article health - related quality of life measurement in long - term survivors and outcome following radical radiotherapy for localized prostate cancer razvan m . 
galalae1 , tillmann loch2 , birgit riemer1 , peter rzehak3 , thomas kchler4 , bernhard kimmig1 , gyrgy kovcs1 purpose : to report long - term outcomes in terms of health - related quality of life ( hrqol ) and survival of a dose - escalating radiotherapy protocol and to validate a new disease - specific hrqol instrument . 
 patients and methods : 189 consecutive men with prostate cancer were analyzed ; 127 patients had t12 ( 1% t1 , 66% t2 ) and 62 patients ( 33% ) t3 tumors . 
the fraction dose was 15 gy in the mcneal zone ( planning target volume [ ptv ] 1 ) , while 89 gy were applied in the entire prostate ( ptv 2 )  . 
univariate analyses of variance by t - stage , grading , prostata - specific antigen ( psa ) status after therapy and adjuvant androgen suppression ( as ) revealed that psa elevation after irradiation and as were associated with significantly diminished hrqol . 
 key words : health - related quality of life ( hrqol ) hdr brachytherapy elective pelvic irradiation conformal radio therapy prostate cancer strahlenther onkol 2004 ; 180 : 5829 doi 10.1007 / s00066 - 004 - 1254 - x messung der gesundheitsbezogenen lebensqualitt bei langzeitberlebenden nach radikaler radiotherapie des lokalisierten prostatakarzinoms ziel : bericht von langzeitergebnissen in bezug auf gesundheitsorientierte lebensqualitt ( lq ) und berleben nach dosiseskalierter strahlentherapie und validierung eines neuen krankheitsspezifischen lq - instruments . 
 patienten und methodik : 189 konsekutive patienten mit prostatakarzinom wurden analysiert : 127 patienten hatten einen t12 ( 1% t1 , 66% t2 ) und 62 patienten ( 33% ) einen t3 - tumor . 
univariate varianzanalysen in bezug auf t - stadium , grading , posttherapeutischen status 1 department of radiation therapy ( radiooncology ) , university hospital schleswig - holstein , campus kiel , kiel , germany , 2 department of urology , university of homburg / saar , homburg / saar , germany , 3 department of epidemiology , university of ulm , ulm , germany , 4 reference center quality of life , department of surgery , university hospital schleswig - holstein , campus kiel , kiel , germany . received : november 5 , 2003 ; accepted : may 21 , 2004 strahlenther onkol 2004 no . 
quality of life following hdr brachytherapy for prostate cancer des prostataspezifischen antigens ( psa ) und adjuvante androgensuppression ( as ) ergaben , dass posttherapeutische psa - erhhung und as mit einer signifikant reduzierten lq assoziiert waren . 
 introduction pretreatment psa the world health organization ( who ) defines health as the absence of disease or infirmity , a state of complete physical , mental and social well - being [ 22 ]  . 
just as this broad and inclusive definition of health describes the medical model , so , too , does the term quality of life define all aspects of patients well - being including physical , psychological , social , spiritual and economic health . 
this seems to be the case especially in men with localized prostate cancer , since the debate on the appropriate indication for radical prostatectomy or definitive dose - escalated conformal radiotherapy is still ongoing . 
spe < 10 ng / ml 1019 ng / ml 20 ng / ml unknown mean psa ( ng / ml ) total cific instruments are likely to be more responsive to change , but are not comprehensive and do not allow across - condition comparisons . 
 scale abbrevianumber item version 1.0 tion of items range item numbers sexuality disease - related pain pa miction partnership flush general symptoms continence total number of items 5 4 3 2 2 4 2 40 , 56 , 57 , 58 , 59 45 , 46 , 47 , 48 36 , 37 , 42 55 , 60 38 , 39 32 , 33 , 34 , 35 43 , 44 strahlenther onkol 2004 no . 
this study was designed to measure the outcome of patients treated by combined high - dose - rate ( hdr ) brachytherapy and external - beam radiotherapy for localized prostate cancer clinically staged t1t3 n0 m0 according to uicc ( union internationale contre le cancer ) in terms of hrqol in survivors at long - term follow - up . 
 furthermore , this study was part of a validation project of a new disease - specific hrqol instrument ( psm - g version 1.0 [ prostate - specific module german )  . 
 patients and methods patient population , tumor characteristics , and treatment 189 consecutive patients with clinically localized prostate cancer ( ct1bt3 n0 m0 ) were treated since february 1986 with a combined protocol using external - beam elective irradiation ( ebir ) of the pelvic lymphatics and interstitial conformal high - dose - rate brachytherapy ( hdr - cbt ) for significant local dose escalation in the prostate . 
the locoregional pelvic lymph nodes were treated to 50 gy with a dose limitation in the prostate to 40 gy using intensity modulation of the beam by individually customed compensators . 
 instruments used for hrqol assessment the eortc core instrument qlq - c30 , which has been validated in large international studies , was used as a generic protocol [ 19 ]  . 
the operability of the five functional scales , physical functioning , role functioning , emotional functioning , cognitive functioning and social functioning , is described in the eortc scoring manual [ 6 ]  . 
 the functional scale scores were calculated using the formula : s = { 1 } 100 . ( rs 1 ) range raw score : i = item ; n = number of items per scale . 
the peripheral zone of the prostate was carried to the cumulative dose of nominal 70 gy by transrectal ultrasound - ( trus - ) planned , interstitial hdr - cbt . 
the minimum target dose ( mtd ) at the periphery of the ptv 1 according to the icru report 58 [ 5 ] was defined as reference dose and was equal to 15 gy per fraction . 
androgen deprivation therapy ( adt ) was given to 45% of the patients : neoadjuvant / concurrent adt as part of the initial management , and / or adt for prostate - specific antigen ( psa ) or clinical relapse during the further course of disease . 
 r ole functioning global health e m otional functioning c ognitive functioning s ocial functioning p hysical functioning financial difficulties n ausea and vo miting fatigue d yspnea pain c onstipation inso m nia diarrhea a ppetite loss figure 1 . 
nine single items completed the module exploring dimensions like performance / efficiency , stool , drug regulation , future perspective , erection , burdening by therapy , further difficulties / problems . 
however , aspects of quality of life are this study included 189 patients , who ranged in age from 47 to 86 years at the time of hrqol measurement ( range 4784 at radiotherapy begin ) with a mean of 73 years ( mean 69 years at radiotherapy begin )  . 
according to kaplan - meier product limits the calculated overall survival ( os ) at 5 years was 80% , and 67.2% at 10 years , respectively , while these estimates for bned survival were 74% and 64.7% ( figure 2 )  . 
univariate survival analyses revealed that low stage ( uicc ct12a ) , low tumor grading ( g12 ) , low initial psa ( < 20 ng / ml ) , no adjuvant hormonal treatment , and psa normalization ( < 1 ng / ml ) following radiotherapy were associated with longer survival ( table 9 )  . 
however , the observed survival differences according to t - stage and adjuvant hormonal treatment were not statistically significant , while those regarding grading , initial psa ( figure 3 ) and postirradiation psa kinetics were significant . 
there was a significant decrease of hrqol in two of four physical health domains , in one category of the mental health domain and sexual function for patients with psa recurrence versus those without , which confirms the current study results . 
we recognize this limitation of our trial , which was primarly designed to assess quality of life of survivors after definitive treatment for prostate cancer , and secondly to further validate a prostate - specific instrument . 
 however , in multivariate ( manova ) analyses , adjuvant hormonal treatment alone remains significant in terms of predicting quality of life impairment , while it was proven not to be significant in multivariate survival cox regression models . 
 from the clinical perspective , however , the results of the current study cannot be interpreted as proof of ineffectivity of hormone - ablative treatments as adjuncts to a dose - escalated radiotherapy regimen , although a number of theories speak against an assumed effectivity [ 23 ]  . 
these findings should be tested in future trials or in pooled retrospective data with a larger number of patients and discriminated by risk factors ( e.g. , initial psa , lesion grading , and uicc tumor stage )  . 
 [ 11 ] investi gated 114 patients with localized prostate cancer , who underwent ultrasound - transperineal brachytherapy as well as a control group of 142 age - matched control men . 
 the long - term outcome analysis of the accelerated hypofractionated prostate radiotherapy protocol reported in the current study demonstrates that hdr - cbt is an excellent method to deliver a high radiation dose to the prostate . 
this paper is the first specifically adressing hrqol in survivors at long - term follow - up ( 6.5 years ) following a dose - escalated , definitive radiotherapy for prostate cancer . 
the same is true for the prostate - specific questionnaire , which has been newly developed in cooperation with urologists and psychologists as a disease - specific but therapy - independent instrument [ 2 ]  . 
however , the reliability does not reach the level of 0.7 in the scales cognitive functioning of qlq - c30 ( cronbachs 0.61 ) , and general symptoms ( cronbachs 0.52 ) and continence ( cronbachs 0.63 ) of the prostate - specific protocol only . 
in the published data by ringdal & ringdal [ 21 ] a lower reliability was also observed in the scale cognitive functioning of qlq - c30 ( cronbachs 0.65 ) , while aaronson et al . 
the calculated mean scores of the current study are comparable with pooled results of the eortc [ 7 ] in 1 , 314 patients with prostate cancer prior to any therapy ( figure 4 )  . 
 conclusion results of hrqol measurement in long - term survivors and survival outcomes confirm that hdr brachytherapy combined with external - beam irradiation is a curative and well - tolerated treatment method for localized prostate cancer . 
the incidence of overlap between the sigmoid colon and / or small bowel and the planning target volume ( ptv ) as well as the dose to sigmoid colon and small bowel were investigated . 
the ptv was defined as a three - dimensional expansion of the ctv with a 10 - mm margin in craniocaudal and a 7 - mm margin in the other directions . 
 conclusion : when systematically investigating the anatomic position of sigmoid colon and small bowel in patients accepted for prostate irradiation , parts of both organs were often observed in close vicinity to the ptv . 
 key words : prostate cancer conformal radiotherapy dose - volume histogram sigmoid colon small bowel strahlenther onkol 2004 ; 180 : 57381 doi 10.1007 / s00066 - 004 - 1267 - 5 die berlappung von sigma und dnndarm mit dem planungszielvolumen bei der radiotherapie des prostatakarzinoms hintergrund und ziel : bei der radiotherapie des prostatakarzinoms wird das rektum als das limitierende organ fr die gesamtdosis angesehen . 
untersucht wurden die inzidenz der berlappung zwischen colon sigmoideum ( sigma ) und / oder dnndarm und dem planungszielvolumen ( ptv ) sowie die dosis an sigma und dnndarm . patienten und methodik : die ct - daten von 75 patienten mit prostatakarzinom wurden analysiert . 
 ergebnisse : das ptv berlappte sich in 60% der flle mit dem sigma und in 19% mit dem dnndarbei diesen patienten betrugen die mittlere maximaldosis fr das sigma 76 , 2 gy ( einfache standardabweichung : 70 , 080 , 7 gy ) und fr den dnndarm 74 , 9 gy ( einfache standardabweichung : 68 , 080 , 0 gy )  . schlussfolgerung : bei patienten , die fr eine bestrahlung eines prostatakarzinoms vorgesehen waren , wurde die anatomische lage von sigma und dnndarm untersucht . 
 schlsselwrter : prostatakarzinom konformale radiotherapie dosis - volumen - histogramm sigmoid dnndarm 1 department of radiation oncology , gent university hospital , gent , belgium , 2 department of radiology , gent university hospital , gent , belgiu received : december 4 , 2003 ; accepted : may 21 , 2004 strahlenther onkol 2004 no . 
incidence of overlap between sigmoid colon / small bowel and ptv in prostate irradiation introduction patients and methods 75 patients with histologically proven adenocarcinoma of the prostate , stage t3 , t4 or having a psa + [ ( gleason score 6 ) 10 ] > 15% underwent a ct scan 712 days ( mean 10 days ) prior to radiotherapy . 
patients were instructed to drink 500 ml of dilute contrast medium ( 30 ml gastrografin [ schering , berlin , germany ] in 1 l water ) the evening before and the morning of the ct scan procedure to increase the visibility of the small bowel ( figure 1 ) and sigmoid colon . 
approximately 30 min prior to the ct scan procedure , all patients received a rectal laxative ( microlax , sanofi - winthrop , colomiers , france ) and were instructed to drink 500 ml of water . 
to improve visualization of the bladder wall , intravenous contrast material ( ultravist , schering ) was administered 10 min prior to the ct scan procedure [ 7 ]  . 
5 mm thick contiguous slices were obtained in the supine position from the level of the umbilicus to a level 10 cm caudal to the testes using a helical ct scanner ( siemens somatom 4 + , siemens , erlangen , germany ) [ 7 ]  . 
 additional data on prostate , seminal vesicles and surrounding tissues were obtained using 2 mm thick contiguous slices from the superior border of both femoral heads to the distal border of the ischial tuberosity [ 7 ]  . 
a growing body of evidence is coming from the literature that dose escalation to the prostate improves local control [ 1315 , 22 , 27 , 37 , 39 ]  . 
both conformal and intensity - modulated radiotherapy ( imrt ) increase the radiation dose to the prostate and seminal vesicles while reducing the volume of normal surrounding tissue irradiated at high doses . 
with imrt , the dose in the volume of overlap between normal tissue and planning target volume ( ptv ) can be lowered selectively , providing a more favorable toxicity profile when compared to conventional and conformal approaches [ 24 , 36 ]  . 
the rectum is the distal portion of the intestinal tract , about 12 cm in length , and extends from the sigmoid colon to the pelvic diaphragm [ 22 ]  . 
late rectal toxicity above grade 2 has been correlated with the percentage of rectal volume [ 2 ] or rectal wall surface irradiated above a selected dose level [ 39 ]  . 
the extent of distal bowel that is defined as rectum may be investigator dependent , as there is no generally accepted computed tomography ( ct ) definition of the transition between rectum and sigmoid colon . 
 in our department , localized prostate cancer is irradiated with the prostate and , in patients with intermediate or poor prognosis , also the seminal vesicles as clinical target volume ( ctv )  . 
in practice , the seminal vesicles are included for t3 and t4 stage and if the result of the formula psa + [ ( gleason 6 ) 10 ] , wherein psa is prostate - specific antigen , is > 15% [ 10 ]  . 
b : blase ; r : rektum ; s : sigma ; sb : dnndarm ; t : bergang des rektums ins sigma ( anfang der horizontalen schlinge in der transversalen ebene )  . 
 we categorized the ct data sets according to four groups for the ptv : ( cid : 127 ) category a : sigmoid colon and / or small bowel overlapping the ptv on one or more ct slice ; figure 2 . 
the prostate ( p ) , seminal vesicles ( sv ) , rectum ( r ) , sigmoid colon ( s ) , and rectosigmoid junction ( j ) are presented . 
the beam aperture covered the beams eye view projection of the ptv with an 8 - mm isotropic margthis latter margin accounts for beam penumbra . femoral heads , bladder and penile bulb were contoured . 
incidence of overlap between sigmoid colon / small bowel and ptv in prostate irradiation mum sigmoid colon dose ( smax ) as well as the percentage of the sigmoid colon volume receiving 50 gy ( s50 ) , 60 gy ( s60 ) , 65 gy ( s65 ) , and 70 gy ( s70 ) are reported . 
for small bowel , the results on mean ( sbmean ) and maximum dose ( sbmax ) as well as the percentage of the small bowel volume receiving 50 gy ( sb50 ) , 60 gy ( sb60 ) , 65 gy ( sb65 ) , and 70 gy ( sb70 ) are reported . 
 together with the calculation of the dose to relative volumes of sigmoid colon and small intestine , we also calculated the dose to absolute volumes using the total volume and dose - volume histograms . 
 ( cid : 127 ) category b : sigmoid colon and / or small bowel and the ptv simultaneously visible on one or more ct slice , but not overlapping with the ptv ; ( cid : 127 ) category c : sigmoid colon and / or small bowel visible on the ct slice immediately above the ptv but not at lower slices ; ( cid : 127 ) category d : cases that do not fit the criteria ac . 
the results on mean ( smean ) and maxithere was a significant difference between category a and all other categories for s50 ( p 0.04 ) , s60 ( p 0.01 ) , s65 table 1 . 
svol : sigmoid colon volume ; smean : mean sigmoid colon dose ; smax : maximal sigmoid colon dose ; s50 , s60 , s65 , s70 : volume percent of sigmoid colon receiving a dose of 50 gy , 60 gy , 65 gy , and 70 gy , respectively . 
svol : sigmavolumen ; smean : mittlere sigmadosis ; smax : maximale sigmadosis ; s50 , s60 , s65 , s70 : prozentualer anteil des sigmavolumens , der mit 50 gy , 60 gy , 65 gy bzw . 
incidence of overlap between sigmoid colon / small bowel and ptv in prostate irradiation ( p < 0.01 ) , s70 ( p 0.02 ) , smean ( p 0.01 ; table 1 )  . 
absolute sigmoid colon volume receiving a dose of 50 gy ( svol50 ) , 60 gy ( svol60 ) , 65 gy ( svol65 ) , and 70 gy ( svol70 ) , respectively . 
absolutes sigmavolumen , das mit 50 gy ( svol50 ) , 60 gy ( svol60 ) , 65 gy ( svol65 ) und 70 gy ( svol70 ) bestrahlt wurde . 
 as for each patient the small bowel volume was available , we recalculated the percentages of small bowel volume into absolute volumes of small bowel ( presented as sbvol )  . 
sbvol : small bowel volume ; sbmean : mean small bowel dose ; sbmax : maximal small bowel dose ; sb50 , sb55 , sb60 , sb65 , sb70 : volume percent of small bowel receiving a dose of 50 gy , 55 gy , 60 gy , 65 gy , and 70 gy , respectively . 
sbvol : das dnndarmvolumen ; sbmean : mittlere dnndarmdosis ; sbmax : maximale dnndarmdosis ; sb50 , sb55 , sb60 , sb65 , sb70 : prozentulaer anteil des dnndarmvolumens , der mit 50 gy , 55 gy , 60 gy , 65 gy bzw . 
absolute small bowel volume receiving a dose of 50 gy ( sbvol50 ) , 55 gy ( sbvol55 ) , 60 gy ( sbvol60 ) , 65 gy ( sbvol65 ) , and 70 gy ( sbvol70 ) , respectively . 
absolutes dnndarmvolumen , das mit 50 gy ( sbvol50 ) , 55 gy ( sbvol55 ) , 60 gy ( sbvol60 ) , 65 gy ( sbvol65 ) und 70 gy ( sbvol70 ) bestrahlt wurde . 
there was a significant difference for sbvol50 , sbvol60 , sbvol65 , and sbvol70 ( p < 0.0001 ; t - test )  . there was no correlation between previous laparotomy and sigmoid or small bowel location ( table 5 )  . 
 discussion conformal and intensity - modulated radiotherapy ( imrt ) for prostate cancer are hot topics [ 3 , 7 , 13 , 24 , 36 ] , but detailed information on the delineation of the rectum and / or sigmoid colon and presence of sigmoid colon and small bowel in the treatment fields is generally unavailable [ 13 , 24 , 25 , 36 , 39 ]  . 
first , the ctv consisted of prostate and seminal vesicles , because the patients presented in this study all had t3 / t4 tumors or tumors with a high probability of seminal vesicle invasion . 
we are fully aware of the fact that a reduction of the cranial margin from ctv to ptv could reduce the incidence of overlap between sigmoid colon / small bowel and the ptv . 
 both rectal dose and rectal volume included in the high - dose region ( small volume high dose ) contribute to late rectal toxicity [ 19 , 24 , 27 , 30 ]  . 
but in a time period where dose escalation is routinely performed ( with doses to the prostate > 81 gy ) , we hypothesize that the strahlenther onkol 2004 no . 
 in most papers , the cranial border of the rectum is defined by the upper border of the treatment fields [ 31 , 35 ] or by the transition into the sigmoid colon [ 2 , 24 ] , which is located at the level of the third sacral vertebra . 
 considering the almost identical histological features of rectum and sigmoid colon [ 21 ] , it is reasonable to assume a similar toxicity profile and to regard the sigmoid colon as a serial organ , consisting of functional units arranged in series . 
high maximum dose to the rectal wall has been shown to correlate significantly with late rectal bleeding [ 18 , 19 ]  . small bowel is sensitive to radiation in a volume - dependent fashion [ 12 , 20 ]  . 
loops of small bowel may descend into douglas pouch or even adhere in the pelvis , especially after abdominopelvic surgery [ 20 ] , although we found no correlation between surgical history and presence of small bowel in the vicinity of the ptv ( table 5 )  . 
zelefsky & harrison reported on 32 of a total of 45 patients in which the small bowel would receive > 65% of the prescription dose ( at least 70.2 gy ) [ 38 ]  . 
incidence of overlap between sigmoid colon / small bowel and ptv in prostate irradiation egory a series , on average 66 cm3 and 57 cm3 of small bowel received 55 gy ( table 6 ) and 60 gy ( table 4 ) , respectively . 
 conclusion apart from the rectum , both the sigmoid colon and small bowel are potentially dose - limiting organs when treating prostate and seminal vesicles with high - dose conformal or intensity - modulated radiotherapy . 
 patients and methods : 67 patients with t1b2 n0 m0 prostate cancer were randomized to receive amifostine intrarectally ( group a , n = 33 ) or not ( group b , n = 34 ) before irradiation . 
 two different toxicity scales were used : eortc / rtog rectal and urologic toxicity criteria along with a subjective - rectosigmoid ( s - rs ) scale based on the endoscopic terminology of the world organization for digestive endoscopy . 
 key words : randomized amifostine intrarectal radiotherapy strahlenther onkol 2004 ; 180 : 55762 doi 10.1007 / s00066 - 004 - 1226 - 1 topische intrarektale verabreichung von amifostin zur verhinderung akuter rektaler strahlentoxizitt : eine randomisierte phase - ii - studie ziel : untersuchung des zytoprotektiven effekts von intrarektal verabreichtem amifostin zur verhinderung akuter rektaler strahlentoxizitt . 
 patienten und methodik : 67 patienten mit einem prostatakarzinom im stadium t1b2 n0 m0 wurden randomisiert zwei gruppen zugeteilt : gruppe a ( n = 33 ) mit und gruppe b ( n = 34 ) ohne intrarektale verabreichung von amifostin vor der bestrahlung . 
zwei verschiedene toxizittsskalen wurden verwendet , die rektalen und urologischen toxizittskriterien der eortc / rtog und die auf der endoskopischen terminologie der wode ( world organization for digestive endoscopy ) basierende s - rs - skala ( subjective - rectosigmoid scale )  . 
der bereich unter der kurve ( auc ) fr den zeitlichen verlauf einer mukositis ( rtog - kriterien ) whrend der bestrahlung stellte den mukositis - index ( mi ) dar . 
gem der rtog - toxizittsskala zeigten fnf von 33 patienten der gruppe a eine mukosi1 department of radiation oncology , aretaieion university hospital , university of athens medical school , athens , greece , 2 department of electrical and computer engineering , institute of communication and computer systems , national technical university of athens , athens , greece , 3 center of radiation oncology , ygeia diagnostic and therapeutic center of athens , athens , greece , 4 radiotherapy department , agios savvas anticancer hospital , athens , greece , 5 gastroenterology unit , alexandra general hospital , athens , greece , 6 urology department , sismanoglio hospital , university of athens medical school , athens , greece . 
 schlsselwrter : randomisiert amifostin intrarektal strahlentherapie introduction the close proximity of the target volume of prostate tumors to the anterior rectal wall makes it impossible to totally eliminate the dose to the rectal wall . 
since conformal radiotherapy in pelvic tumors has the objective to reduce irradiation to organs at risk such as the rectum [ 15 , 16 ] , it is important to evaluate the side effects as comprehensively as possible . 
it has already been approved for use as a radioprotector in the usa and the european union , after publication of an important multicenter randomized study in head and neck cancer patients [ 4 ]  . 
in a previous publication , the cytoprotective efficacy of amifostine against radiation - induced mucositis in the rectal mucosa has been analytically studied using toxicity scales as well as endoscopic objective findings [ 13 ]  . 
initial animal experiments demonstrated that topical administration of the radioprotector wr - 2721 ( amifostine , ethyol ) on the rectal surface results in high concentrations of wr - 2721 and its dephosphorylated active metabolite wr - 1065 in the rectal mucosa [ 2 , 21 ]  . 
patients previously treated with radioor chemotherapy or showing hemoglobin levels < 11 g / dl or white blood cell ( wbc ) counts < 2 , 500 / l and platelet counts < 100 , 000 / l were excluded . 
complete blood cell count , serum urea and creatinine levels as well as liver enzyme levels were assessed once every 2 weeks during the radiotherapy period and for 4 weeks thereafter . 
the objective findings of acute rectal toxicity were assessed and scored using a subjective - rectosigmoid ( s - rs ) toxicity scale described in detail in a previous publication [ 13 ]  . 
beyond this , in order to monitor the radiation - induced morbidity by time , we also performed a mucositis index ( mi ) for rectal and urinary toxicity as described below according to the trapezoid function [ 20 ] : mi = ( xn xn1 ) ( yn1 + yn ) where x = week ( s ) of treatment post - baseline , y = toxicity grade according to rtog criteria , n = certain time point of measurements . 
they were treated in supine position with a four - field - box technique using parallel opposed anterior and posterior and parallel opposed lateral portals with individualized blocks derived from beams eye view . 
in all patients , a three - dimensional treatment planning was performed in conjunction with dose - volume histograms ( dvhs ) for the target and the rectum ( organ at risk ) as well . 
the appropriate scaling factor was adjusted ( 10 cm = 100% of prescribed dose at x - axis and 10 cm = 100% of delineated rectum volume at y - axis ) to ensure reproducibility and comparability between different plots . 
 the application was feasible and well tolerated , while the enema remained in the rectal - anal canal for nearly 2 h without producing any symptom of nonpreferable bowel movement . 
intrarectal administration of amifostine pooled over grade : p = 0.76 ( 2 ) toxicity grade urinary group a group b 55.9% in group b ( p = 0.015 , fishers test )  . 
 however , the incidence of urinary toxicity grade 1 / 2 was equal in both groups in terms of ten out of 33 patients ( 30.3% ) in group a versus nine out of 34 ( 26.5% ) patients in group b ( p = 0.76 ) , while two patients in group a and three patients in group b experienced grade 2 toxicity with nycturia and dysuria requiring an anesthetic . 
concerning the auc - dvh , no significant differences were assessed between the two groups ( table 1 ) , confirming the homogeneity of the study in terms of the irradiated rectal volume . 
 lower gastro intestinal group a group b none 23 / 33 25 / 34 none 28 / 33 19 / 34 discussion the mechanism by which amifostine exerts its selective protection of normal tissue is based on the ability of free thiol to be taken up in higher concentrations in normal organs than in tumor tissue . 
the differential uptake of wr - 1065 is due to differences in the microenvironment at the tissue level resulting in the slow entry of the free thiol into tumor masses [ 5 , 26 ]  . 
in addition , the distribution of alkaline phosphatase in normal and malignant tissue differs , with higher concentrations of this enzyme found in capillaries and arterioles of normal cells and lower levels of alkaline phosphatase observed in tumor tissue . 
thus , selective protection is afforded normal tissues by reduced metabolism of amifostine to the active protector wr - 1065 and low uptake of wr - 1065 by tumors [ 30 ]  . 
the end result is as much as a 100 - fold higher steady concentration of the free thiol in normal organs such as bone marrow , kidney , salivary glands , frequency of urination or nycturia twice pretreatment habit dysuria , urgency not requiring medication 8 / 33 6 / 34 frequency of urination or nycturia which is less frequent than every hour dysuria , urgency , bladder spasm requiring local anesthetic 2 / 33 3 / 34 increased frequency change diarrhea requiring parasymin quality of bowel habits not requiring medication rectal discomfort not requiring analgesics 5 / 33 13 / 34 patholytic drugs mucous discharge not necessitating sanitary pads rectal or abdominal pain requiring analgesics 2 / 34 and heart , compared with tumor tissue . 
once the free thiol wr - 1065 has entered a normal cell , it is available to bind directly to , and thus detoxify , the active species of alkylating agents , platinum agents , or ionizing radiation [ 25 ]  . 
 [ 17 ] reported the results of a randomized clinical study conducted in china that evaluated the use of amifostine and radiotherapy in 100 patients with locally advanced rectal cancer . 
the first reason for this might be related to the high interindividual variation of chromosomes in the relatively small number of patients entered into the study : variation has quite an impact and could have masked a possible protective or modulating effect of amifostine . 
 the topical application of amifostine has been a challenge , since the intravenous or subcutaneous application of this substance is associated with systemic toxicity as already reported in the literature [ 10 ]  . 
by studying the topical application of wr - 2721 in the rectum of male copenhagen rats , reported significantly high concentrations preferentially in the rectal wall [ 2 ]  . 
second , the acute radiation - induced toxicity was evaluated by blind investigators who group b ( rt alone ) group a ( rt + amifostine ) weeks post baseline figure 1 . 
mukositis - index ( mi ) der rektalen strahlentoxizitt nach rtog - kriterien berechnet fr gruppe a ( unter amifostin ) und fr gruppe b ( ohne amifostin )  . 
according to our analysis , no significant differences between amifostine and control arm were monitored in the auc - dvh concerning the rectum as organ at risk , indicating that the impact of dose - volume effect on normal tissue complication probability ( ntcp ) was homogeneous between the treatment arms [ 18 ]  . 
 the latter report may probably explain the fact that no grade 4 toxicity ( rectal bleeding ) was tracked for all patients during the radiotherapy schedule , since due to conformal treatment planning the above limitations were not reached . 
the relative risk of bleeding was increased fivefold when 75 gy was delivered to 30% of the rectal wall volume or when lower doses ( 65 gy ) were delivered to 70% of the rectal wall volume . 
 [ 28 ] observed a statistically significant improvement in freedom from grade 23 rectal complications when the volume of rectum treated to doses > 70 gy was kept to 25% . 
beyond the small number of patients , this prospective randomized study has demonstrated that daily intrarectal administration of amifostine can successfully reduce the incidence and severity of acute rectal mucositis in pelvic irradiated areas , while the duration of mucositis as expressed by the mi is also significantly reduced . 
however , our results have also shown that intrarectal administration of amifostine has no effect on the cytoprotection of the urinary systethis can be easily explained by the lack of systemic absorption of intrarectally located wr - 2721 . 
phase iii randomized trials with more sufficient number of patients stand in need for further evaluation and confirmation of the best way of administering amifostine in patients undergoing pelvic irradiation . 
however , the fact that there is no cytoprotection to the urinary system should not be underestimated , since the only cytoprotection noted in our study was concerning the rectal mucosa . strahlentherapie und onkologie technical note evaluation of a laser system for ct software simulation ( exomio ) in patients with breast cancer gerd stramann1 , peter vacha1 , torsten osterhaus1 , anke battmann2 , detlev richter3 , kamal nashwan1 , hans otto neidel1 , klaus jochen klose2 , rita engenhart - cabillic1 purpose : to develop a manually movable laser system connected to the ct table for alignment of the isocenter cross of irradiation fields on the patients skin directly after ct software simulation . 
 material and methods : the specially designed laser system was constructed in the authors department , and the mean focusing accuracy of isocenter translations was analyzed using alderson phantom measurements . 
the mean overall accuracy from setup to treatment of the whole procedure of ct software simulation was measured by the comparison of bone structures and mamma contour of the digitally reconstructed radiograph ( drr ) with the verification filthe time taken for the different setup procedure steps was evaluated for 70 breast cancer patients who were treated using tangential fields . 
 material und methodik : ein in der abteilung der autoren speziell entwickeltes lasersystem zur einzeichnung des isozentrums wurde in hinblick auf seine fokussierungsgenauigkeit zunchst mittels alderson - phantom geprdanach erfolgte der einsatz bei der einstellung von tangentialen feldern bei 70 patientinnen mit mammakarzinodie durchschnittliche einstellgenauigkeit der gesamten prozedur der computerbasierten simulation einer ct - planung und die zeitrume der einzelnen schritte wurden ermittelt . 
 ergebnisse : die durchschnittliche fokussierungsgenauigkeit zur einzeichnung eines isozentrums nach einer definierten verschiebung des lasersystems betrug 0 , 8 0 , 5 mm , die durchschnittliche patientenbewegung whrend der liegezeit auf dem ct - tisch 2 , 0 1 mm und die mittlere positionierungsgenauigkeit des patienten bei der ersten bestrahlung nach der positionierung entsprechend den hauteinzeichnungen 3 , 9 1 , 5 mdie zeitdauer der gesamten prozedur lag bei 35 , 8 3 , 3 m schlussfolgerung : der wichtigste vorteil der computerbasierten simulation einer ct - planung gegenber der konventionellen simulation ist die entlastung des rntgensimulators , die auch durch eine schnelle planungssoftware ( exomio ) und das vorgestellte bewegliche lasersystem erreicht werden kann . 
 schlsselwrter : virtuelle simulation ct - simulation mammakarzinom 1 department of radiation oncology , university of marburg , marburg , germany , 2 department of radiology , university of marburg , marburg , germany , 3 department of computer science , university of applied sciences wiesbaden , wiesbaden , germany . received : october 24 , 2003 ; accepted : march 25 , 2004 strahlenther onkol 2004 no . 
ct software simulation in breast cancer introduction current clinical routine for external - beam radiotherapy starts with ct data acquisition and is then followed by individualized three - dimensional ( 3 - d ) treatment planning , conventional simulation and , finally , treatment delivery . 
 several software systems have been designed for ct simulation [ 3 , 4 , 1214 , 17 ] , with currently most of the published experience referring to acqsim [ 13 , 5 , 7 , 8 , 11 , 15 ]  . 
 ct simulation software development has proven to be a significant technological advance because it provides a tool to shorten the time required for 3 - d treatment planning and to simplify the treatment delivery process . 
the major improvement has been brought about by the ability to generate excellent digitally reconstructed radiographs ( drrs ) and to be able to perform a time - sparing 3 - d preplanning relevant to a range of planning features , including shielding block positioning and multileaf collimator ( mlc ) orientation . 
at present , the implementation of exomio ( medintec , bochum , germany ) requires isocenter and field alignment on the patients skin with the isocenter projection functionality and the light field of the accelerator to abandon the use of the conventional simulator . we have therefore developed a manually movable laser system which is connected to the ct table for alignment of the isocenter of the irradiation fields on the patients sk this alignment is performed after 3 - d preplanning described above which ensures that time constraints on the use of the linear accelerator for planning purposes are significantly reduced , which results in a faster setup process . 
the treatment consisted of two tangential 6 - mv linear accelerator phofigure 1a abbildung 1a ton beams whose positions were checked using an electronic online portal imaging system ( elekta , iview , hamburg , germany )  . 
 description of the procedure the patient is placed in a comfortable and reproducible position on the ct table with the support of an arm - holding device and knee padding . 
after the alignment of the laser beam on the patients skin in areas that are unlikely to have much movement , two lateral and one ventral ct markers are positioned on the crosses . 
the preliminary isocenter is placed cranially or caudally to the nipple on the breast surface depending on the tumor localization on the patients skin and using the different available ct planes , observers eye view ( oev ) and beams eye view ( bev )  . 
 after this step has been taken , the patient leaves the ct table and returns to the clinic for the treatment delivery to be given without any additional simulation procedure . 
 after ct software simulation preplanning , the structure set and the plan are exported to our helax treatment planning system : wedge angles , the isodose distribution and the monitor units are then obtained . 
the semiautomatic comparison between the drr and the portal image is made using the imaging operating system iview gt ( elekta , crawley , uk ) to evaluate the setup to treatment accuracy before dose delivery . to evaluate the accuracy of the manually movable laser system , an alderson phantom was used in the procedure as a phantom patient . 
however , in 12 / 60 cases the patient movement during the planning ct with ct simulation was > 3 mwe consider this to be significant , and figure 2 . 
a correction of the positioning was performed in six patients with positioning accuracies > 6 mm using the verification syste statistically , the overall accuracy is given by the square root of the sum of the squares of the craniocaudal and ventrodorsal individual accuracies . 
the time periods for the different steps of the ct software simulation process are given in table 1 . discussion compared to the results of setup to treatment accuracy for conventional simulation [ 6 , 10 , 18 ] our method showed that a similar overall accuracy was obtained using the described method for ct software simulation . 
 [ 16 ] we did not find repositioning errors > 1 cone reason is the detailed explanation of the procedure before ct simulation and the correction of inaccuracies > 3 mm after ct simulation before the marking of the isocenter . 
 the main advantage of additional ct simulation to real x - ray simulation is the possibility of time - sparing management of the complete simulation procedures . conclusion with the aid of a simple design of movable laser system connected to the ct table and implemented within the ct software simulation procedure , complete treatment delivery in breast cancer is possible . 
in general , the main advantage of well - known ct software simulation when compared to conventional simulation is the relief of the real x - ray simulator which is feasible with fast planning software ( exomio ) and our movable laser system . strahlentherapie und onkologie original article effects of paclitaxel in combination with ionizing radiation on angiogenesis in the chick embryo chorioallantoic membrane a radiobiological study dimitrios kardamakis1 , christos hadjimichael2 * , panagiotis ginopoulos3 , stamatis papaioannou2 purpose : to investigate the combined effects of paclitaxel and single or fractionated doses of ionizing radiation on the angiogenesis process , using as a model the chick embryo choriallantoic membrane ( cam )  . 
 material and methods : experiments were performed on 9 - day cam , when membranes were irradiated with various single or fractionated doses of x - rays , either alone or in combination with paclitaxel ( 6.4 g / disk )  . 
fractionated doses of x - rays ( two doses of 2.5 , 5 , or 7.5 gy , each 12 h apart ) exerted a dose - dependent reduction of the vascular density index . 
 conclusion : these data confirm that the cam system can be conveniently and properly used for radiobiological studies and indicate that paclitaxel in combination with ionizing radiation does not inhibit further angiogenesis in the system used . 
 key words : chorioallantoic membrane paclitaxel angiogenesis radiobiology strahlenther onkol 2004 ; 180 : 1526 doi 10.1007 / s00066 - 004 - 1140 - 6 auswirkungen von paclitaxel kombiniert mit ionisierender strahlung auf die angiogenese der chorioallantoismembran des hhnerembryos . 
fraktionierte bestrahlungen ( 2 - mal 2 , 5 , 5 oder 7 , 5 gy jeweils im abstand von 12 stunden ) fhrten dosisabhngig zu einem rckgang des blutgefdichte - index . 
 schlussfolgerung : diese ergebnisse besttigen , dass das cam - modell zweckmig fr radiobiologische untersuchungen eingesetzt werden kann , und belegen , dass paclitaxel kombiniert mit ionisierender strahlung im verwendeten modell die angiogenese nicht inhibiert . 
 schlsselwrter : chorioallantoismembran paclitaxel angiogenese radiobiologie 1 department of radiology and radiotherapy , university of patras school of medicine , greece , 2 department of molecular pharmacology , university of patras school of pharmacy , greece , 3 department of internal medicine , general hospital of patras , greece . 
combined effects of paclitaxel and ionizing radiation on angiogenesis introduction irradiation angiogenesis , the process of new vessel generation which leads to neovascularization in tumors , is increasingly appreciated as an alternative strategy in cancer treatment . 
this vessel - rich membrane originates from the embryo , grows outward and is the principal organ of respiratory gaseous exchange for the avian embryo until close to hatching [ 2 , 21 ]  . 
the preference for this system in assessing morphological and functional changes in vessels under normal or experimental conditions is due to its advantages , such as simplicity , reproducibility and usefulness [ 20 , 29 , 31 ]  . 
it is a model which has been widely used for studying the mechanisms of embryotoxicity , teratogenicity and systemic toxicity of chemicals [ 2 , 6 , 17 ] , for investigating the role of the nitric oxide pathway in the antiangiogenic and cytotoxic effects of ionizing radiation [ 20 ] , and for assessing new methods designed to quantitatively evaluate angiogenesis in vivo [ 41 ]  . 
 despite the fact that radiotherapy remains an important component in the management of malignant diseases , only a relatively small number of papers deal with the action of ionizing radiation either on angiogenesis [ 8 , 10 , 14 , 37 , 45 ] , or on endothelial cells in vitro [ 7 , 30 , 36 ]  . 
the results from these studies are variable and reveal that endothelial cells differ in their sensitivity to ionizing radiation , probably because of their heterogenicity and different cell kinetics [ 11 ]  . 
 paclitaxel , a microtubular inhibitor blocking and / or prolonging cells in g2 / m - phase , has been described for its radiosensitizing effects on many cell lines , including the leukemia cell line hl60 [ 5 ] , the breast cell line mcf - 7 and the ovarian cell lines of ovg - 1 and bg - 1 [ 22 ] and has been used in a number of clinical studies with promising results [ 25 , 35 , 39 , 42 , 43 , 48 ]  . 
 in the present study , we investigated the effects of a single concentration of paclitaxel on angiogenesis , in combination with various doses of ionizing radiation , using the chick embryo cam syste material and methods material fresh fertilized eggs ( gallus domesticus ) were obtained from pindos co . 
the window was covered with cellophane tape and the incubation continued until embryo development on day 9 , when part of the cam was irradiated at room temperature with x - rays ( 20 kv , 0.1 mm al ) , using a field of 1 cm diameter . day 9 was chosen as the irradiation day , because previous studies have shown that angiogenesis in the cam system reaches a maximum rate between days 912 , whereas , on day 14 , it reaches a plateau [ 20 , 29 ]  . 
after irradiation , sterile plastic disks of 1 cm diameter were used to cover the irradiated area of cam , as well as an adjacent second area ( nonirradiated ) , which served as a control . 
the assessment for morphological evaluation , made 24 h after irradiation , was based on previous results , which have shown that the maximum antiangiogenic effect of ionizing radiation on the cam occurred 24 h following irradiation [ 29 ]  . 
 morphological evaluation for morphological evaluation , the control and the test cam sites ( irradiated paclitaxel ) were flooded with 10% buffered formalin , the plastic disks removed , and the eggs kept at 37 c until dissection . 
a large cam area around the two disk sites was cut off , placed on a glass slide , and the vascular density index ( vdi ) was determined with the method of harris - hooker et al . 
 [ 19 ] , by counting the number of vessels crossing three concentric circles of 4 , 5 , and 6 mm diameter of a plastic mesh ( which was adopted above each glass side ) using a stereoscope ( olympus sz40 ) under a magnification of 34 ( cid : 1 )  . 
this method was repeatedly and extensively validated using indexes such as collagenous protein synthesis and computer - assisted image analysis in the cam [ 28 , 45 , data on file ]  . 
the shell - less model ( ex vivo ) was not preferred , because the absence of the shell disturbs the o2 / co2 exchange , increases the deaths of the chick embryos , and introduces other parameters during irradiation [ 2 ]  . 
effects of fractionated doses of x - rays with paclitaxel ( added after the first fraction ) on the vascular density index ( vdi ) of 9 - day cam . 
effects of fractionated doses of x - rays with paclitaxel ( added after the second fraction ) on the vascular density index ( vdi ) of 9 - day cam . 
differences with a level of p 0.05 were assumed to be statistically significant . results dose effect of paclitaxel on the cam system preliminary experiments were carried out in order to estimate the effect of various doses of paclitaxel on the vdi of the 9 - day cam . 
doses of paclitaxel up to 6.4 g / disk did not change the vdi significantly , while doses ranging from 11 to 55 g / disk produced early embryonic death of the chick and so their effect on angiogenesis was difficult to be determined ( data not shown )  . 
the reductions of the vdi were also significant ( p 0.01 ) , but it is obvious that paclitaxel failed to further increase the x - ray - induced antiangiogenicity ( table 1 )  . 
further statistical analysis showed that the above data from the three experiments of fractionation were not significantly different . discussion the present study was undertaken to investigate the effects of paclitaxel on angiogenesis , in combination with single or fractionated doses of ionizing radiation , using the chick embryo cam syste the three single doses of 5 , 10 , and 15 gy significantly reduced the vdi of the 9 - day cam suggesting that ionizing radiation has an antiangiogenic effect on the rapidly proliferating cam . 
this finding is in accordance with the basic concept of radiobiology that highly proliferating cell populations are more vulnerable to the effects of ionizing radiation [ 1 , 18 ] , although the effect was not dose - dependent . 
a possible explanation of this phenomenon is the fact that large vessels of the cam are relatively radioresistant to ionizing radiation ; experiments with radiation doses between 2 and 5 gy have shown a proportional decrease of vdi , without any additional decrease at higher doses ( data not shown )  . 
in the present study , fractionated doses of x - rays within an interval of 12 h produced a dose - dependent antiangiogenic effect and confirmed that the cam model can be used in radiobiological experiments . 
recent papers have shown that the yolk sac ( not the cam ) blood vessel system of chick embryo represents a useful model of in vivo measurements of angiogenesis in radiobiology [ 34 ]  . 
the authors have used only single or fractionated irradiation without the combination of any other agent and they have found that a single - dose irradiation with 10 gy induces endothelial cell proliferation [ 33 , 44 ]  . 
it may not at all be surprising that a microtubule - disrupting agent will be embryotoxic prior to being selectively antiangiogenic . other investigators , by contrast , used controlled release of paclitaxel from microspheres and provided evidence that the drug induces vascular regression and inhibits angiogenesis [ 9 , 46 ]  . 
therefore , paclitaxel at a dose of 6.4 g / disk was added either following irradiation or 12 h before irradiation . in the first case , paclitaxel failed to further increase the x - rayinduced antiangiogenicity at all radiation doses used , whereas in the second case , this was true only for the doses of 10 and 15 gy . 
when paclitaxel was added 12 h before irradiation , the dose of 5 gy produced no significant reduction in the vdi . a similar observation was made by withers & elkind [ 49 ] , who found that radiation delivered after the peak of mitotic arrest ( 4 h after paclitaxel treatment ) did not lead to enhancement in radiation response , but rather a slight radioprotection in crypt epithelial cells . 
data from either in vitro or animal studies have shown that , while not cytotoxic alone , paclitaxel caused a progressive reduction of surviving tumor cells after irradiation , and this effect was mainly attributed to inhibition of regeneration of surviving cells between the radiation dose fractions [ 26 , 47 ]  . 
in fact , the nature of the radiation - paclitaxel interaction is not only cell line - dependent ( block and / or prolongation in g2 / m - phase ) , but also dependent on paclitaxel concentration and duration of treatment , radiation dose and the scheduling of the two agents [ 15 , 23 ]  . 
using a carcinoma cell line , ingram & redpath have recently shown that pretreatment with paclitaxel ( 7.5 nm for 12 h ) induced a g2phase block which was maintained during 6 h postirradiation holding either in the presence or absence of paclitaxel , and that no modification of radiosensitivity in the low - dose region was seen [ 23 ]  . 
results from the same study as well as from other studies are consistent with a dual mechanism of action involving paclitaxel - induced radiation resistance , possibly as a consequence of postirradiation holding in phase g2 , and radiation - induced paclitaxel resistance through an unknown mechanisdespite the fact that paclitaxel has been tested in several clinical trials in combination with ionizing radiation with promising results [ 48 ] , there are no studies on possible morphological effects of this combined treatment on the vasculature . 
the present work demonstrates that the cam system of angiogenesis can be conveniently and properly used in radiobiological experiments and may become an important tool for radiobiological and radiopharmacological research . 
combined effects of paclitaxel and ionizing radiation on angiogenesis strahlentherapie und onkologie original article treatment of solitary brain metastasis resection followed by whole brain radiation therapy ( wbrt ) and a radiation boost to the metastatic site dirk rades , annette raabe , amira bajrovic , winfried alberti1 background : whole brain radiation therapy ( wbrt ) is reported to improve local control after resection of brain metastases . 
two therapies were compared for local control and survival : surgery followed by 40 gy wbrt ( group a ) versus surgery followed by 40 gy wbrt and a 10 gy boost ( group b )  . 
17 / 17 patients ( 100% ) of group a and 13 / 16 patients ( 81% ) of group b showed progression of brain metastasis , 8 / 17 and 3 / 16 patients in the area of metastatic surgery . 
 key words solitary brain metastasis resection of metastasis whole brain radiation therapy radiation boost strahlenther onkol 2004 ; 180 : 1447 doi 10.1007 / s00066 - 004 - 1159 - 8 behandlung von solitren hirnmetastasen . 
zwei therapien wurden fr die lokale kontrolle und das gesamtberleben verglichen : metastasenresektion mit anschlieender ganzhirnbestrahlung bis 40 gy ( gruppe a ) versus resektion mit anschlieender ganzhirnbestrahlung bis 40 gy und einem boost von 10 gy ( gruppe b )  . 
der vergleich beider gruppen ergab eine bessere lokale kontrolle ( p = 0 , 0087 ) und ein besseres gesamtberleben ( p = 0 , 0023 ) fr gruppe b ( abbildung 1 )  . 
bei 17 / 17 patienten ( 100% ) in gruppe a und 13 / 16 patienten ( 81% ) in gruppe b zeigte sich ein intrazerebraler progress , bei 8 / 17 und 3 / 16 patienten im bereich der resezierten metastase . 
in gruppe a verstarben 17 / 17 patienten ( 100% ) nach median 9 ( 326 ) monaten tumorbedingt , in gruppe b 9 / 16 patienten ( 56% ) nach median 14 ( 446 ) monaten . 
 schlsselwrter : solitre hirnmetastase metastasenresektion ganzhirnbestrahlung boost 1 department of radiotherapy and radiooncology , university hospital hamburg - eppendorf , germany . received : february 18 , 2003 ; accepted : september 29 , 2003 strahlenther onkol 2004 no . 
treatment of solitary brain metastasis including a postoperative radiation boost introduction in radiation oncology , motor dysfunction may be caused by a variety of malignant or benign lesions including brain metastases , primary brain tumors , and metastatic spinal cord compression [ 6 , 7 , 9 , 13 , 1618 ]  . 
three prognostic classes could be defined : rpa class i ( kps 70% , age < 65 years , controlled primary , no systemic metastases ) , rpa class ii ( kps 70% , age 65 years and / or uncontrolled primary and / or systemic metastases ) , and rpa class iii ( kps < 70% )  . 
 following selection criteria for this retrospective analysis : solitary brain metastasis , kps 70% , controlled disease regarding the primary tumor and further systemic metastases ( rpa class i and class ii )  . 
therefore , for inclusion in our analysis , a progression of brain metastasis had to be confirmed by magnetic resonance imaging ( mri ) or computed tomography ( ct )  . 
 the patients of group a ( n = 17 ) were treated by surgery and subsequent wbrt ( total dose 40 gy , dose per fraction 2 gy , five fractions per week )  . 
stereotactic radiosurgery ( srs ) may be indicated for the treatment of up to three metastases of a suitable size ( 4 cm ) [ 2 , 19 ]  . 
although it has been used for a long time , its value for improvement of local control and overall survival has only been investigated in randomized trials since 1990 [ 10 , 15 , 20 ]  . 
however , the optimum radiation schedule has still to be defined . we present results of a combined approach for the treatment of solitary brain metastasis consisting of surgery followed by radiation therapy . 
patient characteristics ( age , gender , type of primary tumor , * interval between first diagnosis of cancer and detection of brain metastasis , resection status of brain metastasis , controlled extracranial metastases , recursive partitioning analysis [ rpa ] class , further cancer treatment for the primary tumor or metastases ) for the whole series , for group a ( surgery followed by 40 gy whole brain radiation therapy [ wbrt ] ) , and for group b ( surgery followed by 40 gy wbrt and a 10 gy boost to the metastatic site )  . 
patientencharakteristika ( alter , geschlecht , art des primrtumors , * intervall zwischen erstdiagnose der erkrankung bis zum auftreten der hirnmetastase , resektionsstatus der hirnmetastase , kontrollierte extrakraniale metastasen , rpa - klasse [ recursive partitioning analysis ] , weitere tumortherapie des primrtumors oder von metastasen ) fr das gesamtkollektiv , fr gruppe a ( metastasenresektion gefolgt von 40 gy ganzhirnbestrahlung ) und fr gruppe b ( resektion gefolgt von 40 gy ganzhirnbestrahlung und 10 gy boost der metastasenregion )  . 
in the 4 / 16 patients treated before 07 / 1999 , metastatic surgery was incomplete . the fractionation schedules were selected , because the prognosis of our patients was expected to be comparably good [ 21 ]  . 
studies comparing different fractionation schedules of wbrt ranging from 10 gy / one fraction to 40 gy / 20 fractions did not reveal any specific schedule to be superior to others for local control and overall survival [ 3 ]  . 
doses per fraction > 2 gy should not be applied in patients with a comparably good prognosis [ 4 ]  . statistical analysis for comparison of groups a and b was performed using the kaplan - meier method [ 8 ] and the logrank test . 
 results comparison of groups a and b suggested a better progressionfree survival ( p = 0.0087 ) and a better overall survival ( p = 0.0023 ) for the patients of group b ( figure 1 )  . 
during the followup period , 30 / 33 patients ( 91% ) of the whole series developed cerebral progression , 17 / 17 patients ( 100% ) of group a and 13 / 16 patients ( 81% ) of group b . 
in group a , 47% ( 8 / 17 ) of the recurrences occurred in the area , where metastatic surgery was performed , and 53% ( 9 / 17 ) in other areas of the brain group b , the rates were 23% ( 3 / 13 ) and 77% ( 10 / 13 ) , respectively . 
 regarding the patients with local failure , the median time to progression was 8 ( 142 ) months for the whole series , 7 ( 122 ) months for group a and 12 ( 342 ) months for group b . 
26 / 33 patients ( 79% ) of the whole series , 17 / 17 patients ( 100% ) of group a and 9 / 16 patients ( 56% ) of group b , died due to progression of malignant disease . 
in 11 / 26 patients , it was caused by progression of brain metastases and additional lung ( n = 8 ) or liver ( n = 3 ) metastases . 
death occurred after a median interval of 11 ( 346 ) months in the whole series , after 9 ( 326 ) months in group a and after 14 ( 446 ) months in group b . 
all of these nine patients showed cerebral progression after a median interval of 12 ( 242 ) months , and 9 / 9 patients died due to brain metastasis after a median interval of 13 ( 646 ) months . 
median time to death in these patients was 10 ( 617 ) months in group a and 18 ( 1346 ) months in group b . discussion radiation therapy is the most frequently applied treatment modality for brain metastasis . 
surgery plays an important role in the treatment of solitary brain metastasis . three randomized studies compared resection of metastasis followed by wbrt and wbrt alone [ 10 , 15 , 20 ]  . 
other studies showed that wbrt improved local control after surgery , whereas improvement of overall survival could only be demonstrated for patients without extracranial disease [ 4 , 14 ]  . 
 according to these studies , we applied a combined regimen with surgery and postoperative radiation therapy only to rpa class i patients and rpa class ii patients with controlled systemic disease . two different approaches were used , a combined schedule consisting of surgery and postoperative wbrt ( group a ) and a regimen consisting of surgery , wbrt and a radiation boost resulting in a relatively high total dose of 50 gy to the metastatic site ( group b )  . 
kaplan - meier - kurven [ 8 ] fr das gesamtberleben ( a ) und das progressionsfreie berleben ( b ) : die unteren kurven entsprechen gruppe a ( metastasenresektion gefolgt von 40 gy ganzhirnbestrahlung ) , die oberen kurven entsprechen gruppe b ( resektion gefolgt von 40 gy ganzhirnbestrahlung und 10 gy boost der metastasenregion )  . 
 in our series , median overall survival of the patients of group a was 9 months , which was well in the range of the published randomized trials ( 910 months )  . 
 comparison of the two groups for parameters such as age , gender , type of primary tumor , interval between first diagnosis of cancer and detection of brain metastasis , controlled extracranial metastases , rpa class , and further cancer treatment for the primary tumor or metastases , did not reveal a significant difference . 
therefore these parameters had no relevant impact on our results , nor did the extent of metastatic surgery , as both groups were comparably balanced for completely and incompletely resected lesions . 
according to the literature , the treatment effect of srs for solitary brain metastasis is comparable to the effect of surgery followed by wbrt without a radiation boost [ 2 , 11 ]  . 
median overall survival after srs alone was reported to be 712 months for patients with controlled systemic disease [ 2 , 19 ] , which was worse than in the patients of our series who had received the radiation boost ( group b )  . 
 conclusion our results suggest that after resection of a solitary brain metastasis , patients seem to benefit from postoperative radiation therapy consisting of wbrt and an additional boost to the former metastatic site . 
 strahlentherapie und onkologie original article backscattered dose perturbation effects at metallic interfaces irradiated by high - energy xand gammaray therapeutic beams manickam ravikumar , ramamoorthy ravichandran , saminathan sathiyan , sanjay sudhakar supe1 purpose : to analyze backscattered dose enhancements near different metallic interfaces for cobalt - 60 ( 60co ) gamma rays and 6and 18 - mv photon beams . 
 results : it can be noticed that the backscatter dose factor ( bsdf ) reaches the saturation value within few millimeters of all inhomogeneities and the thickness at which the saturation value is reached depends on the atomic number of the inhomogeneity . the amount of backscattered radiation was noticed to be greater with lesser - energy photons ( 60co ) compared to the higherenergy photons . 
the backscattered electrons from lead inhomogeneity have a range in the order of 57 m conclusion : higher atomic number inhomogeneities result in an increase in bsdf , as they have higher scattering cross section for the secondary electrons . 
 key words : backscatter metallic interface beam quality perturbation range strahlenther onkol 2004 ; 180 : 1738 doi 10.1007 / s00066 - 004 - 1162 - 0 rckstreudosiseffekte an metallgrenzflchen unter hochenergie - rntgenund gammabestrahlung ziel : analyse der verstrkung der rckstreudosis an unterschiedlichen metallischen grenzflchen fr kobalt - 60 - ( 60co - ) gammastrahlen sowie fr 6und 18mv - photonen - strahlung . 
 ergebnisse : es wurde festgestellt , dass der rckstreudosisfaktor ( bsdf ) seinen sttigungswert innerhalb weniger millimeter aller grenzflchenmaterialien erreicht , wobei die dicke , bei der der sttigungswert erreicht wird , von der kernladungszahl des grenzflchenmaterials abhngt . 
die elektronen , die von der blei - grenzflche rckgestreut werden , haben eine reichweite von 57 m schlussfolgerung : grenzflchenmaterialien mit hherer kernladungszahl bewirken eine zunahme des bsdf , da sie fr die sekundrelektronen einen hheren streuquerschnitt aufweisen . 
backscattered dose enhancements at metallic interfaces introduction material and methods when a patient is treated with high atomic number metallic inhomogeneities embedded in body tissues , the dose at the metal - tissue interface increases significantly [ 9 , 10 , 30 , 33 , 35 ]  . the metallic interfaces within the patient are formed by metallic prosthesis , metal tubes and pins placed after surgery , permanent metal implants , and the dental materials in teeth . 
the significant increase in dose observed is mainly due to the scatter of secondary electrons across the interface , where a nonequilibrium zone of secondary electron fluence exists during photon irradiation . 
 the presence of metallic inhomogeneity in the electron beam results in an enhancement of dose at the tissue - metal interface due to the backscattered electrons [ 12 , 18 , 19 , 25 , 29 , 32 , 37 ]  . 
the dose enhancement at orthovoltage x - rays and cobalt - 60 ( 60co ) gamma rays due to the backscattered secondary electrons in cell irradiation procedures was reported by murthy & lakshmanan [ 23 ]  . 
a backscatter factor of 15% was reported [ 21 ] at 1.25 mev and a slightly less increase for high - energy x - rays at bone - titanium interface . 
das & khan [ 6 ] have studied the dose perturbation effects at some metallic interfaces and pointed out that the backscatter effect can be considered independent of field size , thickness of the medium overlying the interface , and width of the inhomogeneity . 
in many of the commercially available treatment planning systems , only the attenuation of the photon beam in the inhomogeneities is considered , whereas the backscattering effect at the interfaces is usually not taken into account . 
the backward scattering of secondary electrons from the metallic inhomogeneities depends on many parameters such as photon energy , width and thickness of the inhomogeneity , distance from the inhomogeneity , thickness of the medium overlying the interface , atomic number of the inhomogeneity , and field size of the photon beam [ 3 , 11 ]  . 
in our present study , backward scattering effects for 6and 18 - mv photon beams and 60co gamma radiation were investigated with five different materials of inhomogeneities of varying thickness embedded in a polystyrene phanto the dose above or below the inhomogeneity can be found out by multiplying the dose in the homogeneous medium with the forward or backscatter dose factors . 
the backscatter dose factor ( bsdf ) can be defined as bsdf ( e , t , x , d , z , f , ( cid : 1 ) , ( cid : 2 ) ) = di\dh ( 1 ) , where di is the dose at the interface between the metallic inhomogeneity and the polystyrene phantom , dh is the dose at the same point in the homogeneous polystyrene phantom material without the metallic layer , e is the energy of the megavoltage photon beam , t is the thickness of the metallic inhomogeneity , x is the distance of the point of measurement above the interface , d is the thickness of the phantom material placed over the metallic inhomogeneity , z is the atomic number of the inhomogeneity , f is the field size at the point of measurement , ( cid : 1 ) is the angle of beam incidence , and ( cid : 2 ) is the density of the metallic inhomogeneity . 
the chamber has a sensitive volume of 0.2 cm3 with an electrode separation of 1.5 m the resultant ionization was recorded using an rdm - 1f electrometer ( therados ) with a digital readout . 
the parallel - plate chamber was positioned in a polystyrene phantom of 25 ( cid : 3 ) 25 cm2 that was machined to provide a close fit for both the chamber and the sleeve . 
all the measurements were made with a field size of 8 ( cid : 3 ) 8 cm with 100 mu set on accelerator control for 6and 18 - mv photons and 1 min of irradiation time set in 60co unit . 
 during the measurements , the front window of the parallel - plate chamber was positioned at 5.2 cm depth in the polystyrene phantom and was maintained at 100 cm focus to surface distance ( fsd ) for 6and 18 - mv photons and at 80 cm for 60co with the gantry of the machines positioned under the couch . 
for dose measurement at the metal - polystyrene interface di , the parallel - plate chamber front window was placed directly in contact with the metallic inhomogeneities ( figure 1 )  . 
since the dose conversion factors are the same for both measurements , it is assumed that the ratio of the collected charges is equal to the ratio of the doses di and dh expressed in equation ( 1 )  . 
the validity of positioning the chamber in the reverse geometry was confirmed by measuring the percentage depth dose for a 10 ( cid : 3 ) 10 cm field with the chambers positioned at both sides . 
 the therapeutic photon beam qualities are usually represented in terms of ionization ratio ( ir ) , which is defined as the ratio of ionization measured at 20 cm depth in phantom to that of ionization measured at 10 cm , when the source - chamber distance is maintained at 100 cm [ 1 , 2 , 16 , 17 ]  . 
in the accelerator - produced photon beams , the quality of the beam at points off the central axis changes significantly due to the variation of flattening filter material thickness across the beam away from the central axis [ 13 , 14 , 22 , 24 ]  . 
the change in beam quality across the beam can be noted by observing the variation in ir across the beathough the change in ir is significant at lower photon energies , it was shown not to vary much at higher photon energies . 
an attempt was made earlier to show the difference in beam quality across the beam by measuring the forward dose scatter factors at points off the central axis [ 7 , 28 ]  . in this study , we have attempted to quantify the change in beam quality at off - axis by measuring the bsdfs . 
 since the backscattered electrons from the metallic inhomogeneities are of very low energies [ 6 , 15 , 33 , 36 ] , they are expected to have least range as they pass through the mediuin order to find out the range of backscattered electrons from lead and aluminum inhomogeneities , thin polystyrene sheets of varying thickness were placed between the chamber and the inhomogeneity materials . 
from the graph it can be seen that the bsdf variation with lead inhomogeneity has a slope comparable to that of ir curves for both 6and 18 - mv photons . 
it was also noticed that the variation in bsdf with high z - inhomogeneity ( lead ) has a greater slope compared to low z - inhomogeneity ( aluminum )  . 
hence it can be concluded that the quality specification by bsdf from high z - inhomogeneity is more sensitive to spectral changes in the photon bea figure 4 shows the variation of relative ionization with the thickness of the polystyrene placed over the interface for lead and aluminuit can be noticed that for all the energies investigated the relative ionization decreases drastically within few millimeters of the polystyrene indicating that the energy of the backscattered electrons is very low . 
the backscattered electrons from lead inhomogeneity have a range in the order of 57 mm . when the thickness of the polystyrene exceeds the range of backscattered electrons , the measured ionization remains constant thereafter . 
the tail portion of the curve could be due to the bremsstrahlung produced within the inhomogeneities as a result of interaction of secondary electrons with the atoms of the inhomogeneity material . 
the backscattered photons at the inhomogeneities can also lead to an increase in dose , but the amount of photons getting scattered reduces with energy , and it will be negligible at the energies studied . 
since the scattering cross section is higher with high z - materials , the minimum thickness of the inhomogeneity to produce the saturation value of bsdf is lesser for high z - metals compared to the low z - inhomogeneities . 
since the range of backscattered electrons from the inhomogeneities is higher with high - energy photons , the minimum thickness to reach the saturation value of bsdf is greater for 18 - mv photons compared to 60co gamma rays . 
though the range of backscattered electrons is higher from high - energy photons , the amount getting scattered from the inhomogeneities is less and this results in less bsdf for 18 - mv photons compared to 1.25 mev 60co gamma rays . 
 higher atomic number inhomogeneities result in an increase in bsdf as they have higher scattering cross section for the secondary electrons which might result in higher characteristic x - rays being produced . 
the backscattered electrons produced by higher - energy photons have higher range in polystyrene . the range of backscattered electrons from higher z - inhomoco 6 mv 18 mv thickness of perspex ( mm ) thickness of perspex ( mm ) figure 4a abbildung 4a figure 4b abbildung 4b figures 4a and 4b . 
backscattered dose enhancements at metallic interfaces geneity is higher compared to that from lower z - materials . the relatively small and long tail of the curve could be due to bremsstrahlung produced within the inhomogeneity . 
since the factors affecting the bsdf at the interface are energy - dependent , it is expected that the variation in bsdf will also be sensitive to the beam energy . 
the results from this study are clinically useful in predicting the increase in dose upstream at high z - interfaces and the same could be incorporated in the treatment planning procedures [ 20 ]  . 
 strahlentherapie und onkologie original article direct segment aperture and weight optimization for intensity - modulated radiotherapy of prostate cancer gert de meerleer1 * , luc vakaet1 * , werner de gersem1 , geert villeirs2 , wilfried de neve1 background and purpose : to describe the implementation and to evaluate the results of direct segment aperture optimization using the segment outline and weight adapting tool ( sowat ) in intensity - modulated radiotherapy ( imrt ) for prostate cancer . patients and methods : 14 consecutive , unselected patients with localized prostate cancer were entered in a planning study comparing imrt without and with the use of sowat . 
to create the planning target volume ( ptv ) , a three - dimensional anisotropic margin ( 10 mm in craniocaudal direction , 7 mm in both other directions ) was used . 
to compare both plans , physical as well as biological endpoints were considered . results : considering the ctv , sowat resulted in a significantly higher minimal dose together with a higher dose to 95% ( d95 ) and 90% ( d90 ) of the ctv volume ( p < 0.05 ; figure 2 )  . 
for rectum , the volumes receiving 50 gy ( rvol50 ) , 60 gy ( rvol60 ) , or 65 gy ( rvol65 ) as well as the mean dose were significantly lowered after sowat ( p = 0.0001 ; figure 3 )  . 
it leaves the delivery time unchanged , so that treatments can still be delivered within a time slot of 8 m key words : prostate cancer imrt leaf optimization planning strahlenther onkol 2004 ; 180 : 13643 doi 10.1007 / s00066 - 004 - 1209 - 2 direkte segment - apertur und gewichtsoptimierung bei intensittsmodulierter strahlenbehandlung ( imrt ) von prostatakrebs hintergrund und ziel : beschreibung der durchfhrung und bewertung der ergebnisse einer direkten segment - apertur - optimierung ( sowat ) durch verwendung eines segmentumschreibenden und gewichtsanpassenden planungsmittels bei intensittsmodulierter strahlenbehandlung ( imrt ) von prostatakrebs . 
physikalische wie auch biologische endpunkte fanden zum vergleich beider plne bercksichtigung . ergebnisse : bezglich des ctv erzielte sowat eine signifikant hhere minimaldosis sowie eine hhere dosis bis 95% ( d95 ) und 90% ( d90 ) des ctv - volumens ( p < 0 , 05 ; abbildung 2 )  . 
fr das rektum waren die volumina , die mit 50 gy ( rvol50 ) , 60 gy ( rvol60 ) oder 65 gy ( rvol65 ) bestrahlt wurden , wie auch die mittlere dosis nach sowat signifikant niedriger ( p = 0 , 0001 ; abbildung 3 )  . 
 gert de meerleer is a postdoctoral fellow of the fwo ( fonds voor wetenschappelijk onderzoek ) vlaanderen . 1 department of radiotherapy , and 2 department of radiology , gent university hospital , belgium . received : july 9 , 2003 ; accepted : september 29 , 2003 strahlenther onkol 2004 no . 
optimization for imrt of prostate cancer introduction intensity - modulated radiotherapy ( imrt ) has been implemented clinically at gent university hospital ( guh ) , belgium , since 1998 . 
with regard to prostate cancer , the goal was to escalate the dose to both clinical target volume ( ctv ) and the part of the planning target volume ( ptv ) that does not overlap organs at risk ( oars ) such as rectum , sigmoid colon or small bowel . 
sufficient literature exists that such dose escalation improves local control and is possible without increased radiation toxicity [ 10 , 12 , 21 , 22 , 27 , 30 , 33 ]  . 
in a previous planning study , we have shown that imrt plans significantly increased the ratio of tumor control probability ( tcp ) over normal tissue complication probability ( ntcp ) of the rectum [ 8 ]  . 
at guh , a segmented imrt planning technique , called anatomy - based segmentation , was developed in which segment shapes were directly derived from the geometry of ptv and oars in beams eye view ( bev )  . 
developed a tool ( sowat [ segment outline and weight adapting tool ] ) that , starting from arbitrarily shaped segments , optimizes their shapes and weights directly using biophysical objective functions [ 7 ]  . 
sowat proved to be performant in plan optimization for head and neck cancer [ 3 ]  . the purpose of this study was to assess the value of sowat in prostate cancer plan optimization . 
patients were instructed to drink dilute contrast medium ( 15 ml gastrografin [ schering , berlin , germany ] in 500 ml water ) the evening before and the morning of the ct scan in order to improve the visibility of small bowel . the patients were asked to drink 500 ml of water 30 min before the ct scan [ 23 ] and received a rectal laxative ( microlax , sanofi - winthrop , colombiers , france )  . 
the ct data on prostate , seminal vesicles and surrounding tissues were obtained by means of a helical ct scanner ( siemens somatom 4 + , siemens , erlangen , germany ) using 2 - mm slices at 2 - mm increments from the superior border of both femoral heads to the inferior border of the ischial tuberosity , and 5 - mm slices at 5 - mm increments from the level of the umbilicus to a level 10 cm caudal to the testis . 
the ctv , oars , and skin were contoured on each sequential ct slice in consensus reading between a radiation oncologist ( gdm ) and a radiologist , specialized in pelvic imaging ( gv )  . 
surrounding structures ( surs ) were defined as the whole patient excluding the ptv and the region within 25 mm of the ptv in order to limit high dose deposits in tissues outside the ptv and all oars ( e.g. , gluteal muscle ) [ 3 , 20 ]  . 
the dose constraints of 74 gy to the rectum and sigmoid colon and 80 gy to the bladder , as well as a softer dose restriction of 55 gy to surs were applied by a normal tissue optimization factor [ 7 ]  . 
 for rectum and sigmoid colon , the physical endpoints dmean and dmax as well as the volumes receiving a dose of 50 gy ( rvol50 and svol50 ) , 60 gy ( rvol60 and svol60 ) , 65 gy ( rvol65 and svol65 ) , 70 gy ( rvol70 and svol70 ) , 72 gy ( rvol72 and svol72 ) , and 74 gy ( rvol74 and svol74 ) were calculated . 
for bladder , the following physical endpoints were calculated : dmean and dmax as well as the bladder volume receiving a dose of 60 gy ( bvol60 ) , 65 gy ( bvol65 ) , 70 gy ( bvol70 ) , and 75 gy ( bvol75 )  . 
for rectum , sigmoid colon and bladder , ntcp was the biological endpoint and calculated using the lyman model [ 18 ] combined with the dosevolume histogram ( dvh ) reduction scheme of kutcher & burman [ 16 ]  . 
dose distributions for all plans were calculated using a grid with 3 ( cid : 1 ) 3 ( cid : 1 ) 3 mm voxels . criteria for plan acceptance are presented in table 3 . 
each normal tissue optimization factor ( ntof ) is computed according to the normal tissue complication probability ( ntcp ) model of lyman [ 18 ] , and kutcher & burman [ 16 ] , for which n is the volume factor , m is the slope factor , and td50 is the 50% complication probability dose level . 
jeder optimierungsfaktor fr normales gewebe wird entsprechend dem modell von lyman [ 18 ] fr die komplikationswahrscheinlichkeit von normalem gewebe berechnet , wie auch dem modell von kutcher & burman [ 16 ] , wofr gilt : n ist der volumenfaktor , m der verlaufsfaktor , und td50 das 50% komplikationswahrscheinlichkeitsniveau . 
by this term , the dose maximum to the rectal wall converges to 74 gy for all plans ( see figure 3 )  . one could consider the dose being normalized to 74 gy to a point that is located in the overlap volume between ptv and rectal wall and coincides with the dose maximum in the rectal wall . 
in an ideal plan , the whole ctv could exceed a dose of 74 gy , since ctv does not intersect with rectal wall , the latter being constrained to a dmax of 74 gy . 
this observation is consistent with a sharpening of the dose gradient by sowat at the edge of the ptv inside the rectusowat was originally designed to increase dose gradients nearby contoured structures . 
 figure 4 shows the dvh statistics for sigmoid colon that is modeled the same way as rectum in the objective function . in only five patients , the ptv overlapped with sigmoid . 
in the pre - sowat period , imrt beams were defined by the generation of an auto - beam of 8 mm around the ptv ( open beam ) and the generation of beam segments , based on the patients anatomy [ 8 ]  . 
there was no additional possibility to create a sharp dose gradient around the ptv . this imrt technology has been clinically implemented in over 130 patients with a very favorable toxicity profile . 
this results in a sharpening of the dose gradient at the overlap between ptv and oars , but avoiding sharp dose fall - off at regions , where this is unnecessary . 
as shown by the results , although a broader structure is included in the optimization , sowat reduces the volume of the rectum irradiated to high dose levels . we have pointed out the danger of allowing high levels of tdi at equal median ptv dose . 
physical endpoints concerning sigmoid colon for both plans . svol50 , svol60 , svol65 , svol70 , svol72 , svol74 , and smax are presented as dose - volume histograms ( mean sem )  . 
physikalische endpunkte fr das sigma in beiden plnen . svol50 , svol60 , svol65 , svol70 , svol72 , svol74 , and smax sind als dosis - volumenhistogramme angegeben ( mittelwert sem )  . 
physikalische endpunkte fr die blase in beiden plnen . bvol60 , bvol65 , bvol70 , bvol75 , and bmax sind als dosis - volumen - histogramme angegeben ( mittelwert sem )  . 
optimization for imrt of prostate cancer ctv dose of the swot plan was < 70 gy , sowat increased it by at least 2 gy , while this was only the case in five out of ten patients with a minimal dose of 70 gy . 
consequently , only a limited dose difference between the bladder base , and therefore , no dose gradient between bladder base and prostate base could be created in the swot plans . 
there is strong evidence that both rectal dose and volume of rectum included in the high - dose region are the major determinants [ 13 , 17 , 19 , 22 , 25 , 26 , 29 , 33 ]  . sowat generated a decrease in rvol50 , rvol60 , and rvol65 . 
we used the anatomic definition of the rectum ( and , consequently , sigmoid colon ) for its delineation , and a rectal laxative was used prior to the ct scan procedure . 
this explains the very small sem of the rectal volume in our study . we feel that the rectum should be considered an anatomically defined entity and that its volume should not depend on field sizes , rectal filling , or prostate volume . 
indeed , several authors stated that the probability of rectal bleeding was higher , if > 2530% of the rectal wall received > 70 gy [ 1 , 22 , 26 ] , or if the absolute volume of rectum receiving 70 gy was > 15 cm3 [ 15 ]  . 
sowat decreased rvol70 in eight patients , with the largest decreases seen in patients with rvol70 > 30% ( decreases of 9% , 12% , 16% , and 30% )  . 
 for four out of the five patients in whom an increase of rvol70 after sowat was seen , a lower ntcp was noted together with a lower rvol50 , rvol60 , and rvol65 . 
in the remaining patient , the 8% increase in rvol70 was countered by a lower rvol50 ( 7% ) , rvol60 ( 4% ) , and rvol65 ( 1% ) , but not by a lower ntcp . 
in the paper by skwarchuk et al . , the lowest maximal rectal dose at which a rectal bleeding occurred was 78 gy ( i.e. , 103% of prescription dose of 75.6 gy ) [ 25 ]  . 
sowat decreased it to 2% , by reducing bvol60 and bvol70 with 8% and 7% , respectively . sowat obviously did no effort in reducing physical bladder parameters , when the biological endpoint ( ntcp ) was already very low after swot . 
although the predicted percentage of p + may not be an exact predictor of uncomplicated control of disease , it allows comparison and ranking of different treatment plans [ 8 ]  . 
however , the sowat plan was considered better by the staff and implemented clinically because the homogeneity after sowat was better ( 3% and 4% improvement for ctv and ptv , respectively )  . 
since we have no in - house developed statistics on prostate margin ( research is going on ) , we have derived the expansion from ctv to ptv from literature . 
the overall effect of sowat can be summarized as ( 1 ) an increase in dmin to ctv and ptv ; ( 2 ) a reduction of the unwanted underdosage in ctv ; ( 3 ) a reduction of the volume of rectum irradiated to doses < 70 gy ; and ( 4 ) preservation of safe dose levels to sigmoid and bladder . 
 strahlentherapie und onkologie original article low - dose x - irradiation of adjuvant - induced arthritis in rats efficacy of different fractionation schedules andr liebmann1 , marion hindemith1 , jutta jahns1 , petra madaj - sterba2 , sigrid weisheit2 , friedrich kamprad1 , guido hildebrandt1 background and purpose : low - dose radiotherapy is widely accepted as a very effective treatment option for inflammatory symptoms associated with painful degenerative joint disorders . 
the efficacy of low - dose x - irradiation on adjuvant induced arthritis in rats using different fractionation schemes was investigated in vivo , in order to explore whether there is a dose and fractionation dependence . 
 results : a significant decrease of the clinical arthritis parameters was observed following 5 ( cid : 1 ) 0.5 gy or 5 ( cid : 1 ) 1.0 gy during the acute maximum of the inflammatory response ( days 1519 )  . 
the most pronounced treatment effect was reached after two daily fractionated series of 5 ( cid : 1 ) 0.5 gy with an early treatment onset ( days 1014 ) and repetition in interval ( days 2226 )  . 
after the application of 5 ( cid : 1 ) 1.0 gy on days 1014 or in a protracted scheme ( days 10 , 12 , 14 , 16 , and 18 ) , only a nonsignificant positive trend could be detected . 
two series of 5 ( cid : 1 ) 0.5 gy with an early treatment onset ( days 1014 ) and repetition in interval ( days 2226 ) were the most effective treatment schedule in this experimental study . 
 key words : low - dose radiotherapy anti - inflammatory radiotherapy fractionation adjuvant arthritis rat model strahlenther onkol 2004 ; 180 : 16572 doi 10.1007 / s00066 - 004 - 1197 - 2 niedrig dosierte strahlentherapie der adjuvansarthritis in einem rattenmodell . 
das ziel dieser studie war die beurteilung der klinischen wirksamkeit verschiedener fraktionierungsschemata und einzeldosen in einem experimentellen arthritismodell der ratte , um zu berprfen , ob eine dosisoder fraktionierungsabhngigkeit vorliegt . material und methodik : bei weiblichen lewis - ratten ( n = 128 ) wurde durch intradermale injektion von hitzeinaktiviertem mycobacterium tuberculosis am tag 0 eine adjuvansarthritis induziert . 
low - dose x - irradiation of adjuvant arthritis ergebnisse : nach 5 ( cid : 1 ) 0 , 5 gy oder 5 ( cid : 1 ) 1 , 0 gy whrend des akuten entzndungsmaximums ( tage 1519 ) konnte eine signifikante reduktion der klinischen arthritisparameter beobachtet werden . 
der gnstigste behandlungseffekt wurde mit zwei tglich fraktionierten serien von 5 ( cid : 1 ) 0 , 5 gy bei frhzeitigem behandlungsbeginn ( tage 1014 ) und wiederholung im intervall ( tage 2226 ) erreicht . 
nach 5 ( cid : 1 ) 1 , 0 gy an den tagen 1014 oder in einem protrahierten schema ( tage 10 , 12 , 14 , 16 und 18 ) war lediglich ein nichtsignifikanter positiver trend nachweisbar . 
 schlussfolgerung : eine niedrig dosierte strahlentherapie ist in der lage , die volle ausprgung einer arthritischen reaktion zu verhindern , wenn sie whrend der floriden phase der adjuvansarthritis appliziert wird . 
in dieser studie waren zwei bestrahlungsserien von 5 ( cid : 1 ) 0 , 5 gy mit frhzeitigem behandlungsbeginn ( tage 1014 ) und wiederholung im intervall ( tage 2226 ) das effektivste behandlungsschema . 
 schlsselwrter : niedrig dosierte strahlentherapie antiinflammatorische strahlentherapie fraktionierung adjuvansarthritis rattenmodell introduction the first publication about the successful treatment of inflammatory joint disorders with x - rays appeared already in 1898 , just 3 years after the discovery of x - rays by roentgen [ 21 ]  . clinical empirical observations about analgesic and antiinflammatory efficacy of low x - ray doses have existed for > 100 years [ 7 , 21 ] , and low - dose x - irradiation has been widely accepted as a very effective treatment option for inflammatory symptoms associated with painful degenerative joint disorders for decades [ 12 ]  . 
 recently , a pattern - of - care study in germany on radiation therapy for benign diseases , initiated by the german working group on radiotherapy of benign diseases , showed significant geographic and institutional differences [ 19 , 20 ]  . based on this survey , consensus guidelines to standardize radiation treatment of benign diseases have been suggested for the first time [ 13 ]  . 
 radiation doses in clinical use for the treatment of painful degenerative joint disorders are commonly single doses of 0.51.0 gy , two or three fractions a week , and total doses of 312 gy [ 13 , 20 ]  . 
 however , single doses , total doses , and fractionation schedules currently used in clinical practice are empirical and mainly based on clinical observations established by von pannewitz [ 15 , 16 ]  . 
 we investigated in vivo the effects of low - dose x - irradiation on adjuvant - induced arthritis in rats , in order to explore whether there is a dose , time or fractionation dependence of its anti - inflammatory efficacy . 
recently , we could clinically and histomorphologically demonstrate that low - dose x - irradiation exerts anti - inflammatory efficacy in adjuvant arthritis when given during the acute maximum of the inflammatory response [ 8 , 18 ]  . 
based on these results using the adjuvant arthritis model , three dose and fractionation experiments were performed ( in the years 1999 , 2001 , and 2002 ) to evaluate the anti - inflammatory efficacy of low - dose x - irradiation depending on treatment onset , fractionation scheme , and dose . 
 material and methods animals female lewis rats ( supplied by lewis rats probstheida , germany ) were housed two per case , with available food and water ad libitum in the medical - experimental center of the university of leipzig , germany ( n = 128 ; 1999 : n = 50 , 2001 : n = 30 , 2002 : n = 48 )  . 
 induction of adjuvant arthritis on day 0 ( day of induction ) , 0.5 mg of heat - inactivated mycobacterium tuberculosis ( r37 ra ; difco , detroit , mi , usa ) in 0.1 ml of paraffin oil ( riedel de haen ag , seelze , germany ) was injected intradermally into the base of the tail . special efforts were undertaken to assure a homogeneous suspension , and to exclude any intravenous injection . 
bersicht aller gruppen und therapieschemata ( ( cid : 1 ) scheinbestrahlung ; ( cid : 1 ) einzeldosis 1 , 0 gy ; ( cid : 2 ) einzeldosis 0 , 5 gy )  . 
for the second trial ( 2001 ) , 30 animals in three groups were treated ( group 3 : sham irradiation ; groups 8 and 9 : treatment regimes ) , and for the third trial ( 2002 ) , four groups with twelve animals each were treated ( group 1 : sham irradiation ; groups 4 , 11 , and 12 : treatment regimes )  . 
 prior to irradiation , animals were anesthetized with ketamine / xylazine intraperitoneally ( 8085 mg ketanest [ ketamine ] / kg body weight , 510 mg rompun [ xylazine ] / kg body weight )  . 
the anesthetized animals were fixed onto a custommade wooden jig , and their hind paws were placed into plastic boxes containing tissue - equivalent material to ensure a homogeneous dose distribution . 
 the hind paws were irradiated at 150 kv and 11.2 ma using a 150 - kv x - ray unit ( darpac 150 - mc , ray technologies ltd , swindon , wiltshire , uk )  . 
the beam was filtered with 0.3 mm cu and 1.1 mm al , yielding an hvl ( half - value layer ) equivalent of 6.71 mm al , and vertically directed . 
the irradiation field was adapted by a round tube ( diameter 4 cm , sourceto - surface distance 15 cm ) to include the hind paw up to 0.5 cm proximal of the ankle . 
the hind paw of the unanesthetized animal was placed into the water - filled chamber exactly as far as the inner hairline of the paw to ensure a reproducible borderline for hpv estimation . 
to avoid interobserver variability , the same person did all measurements , and another investigator the reading without knowing the treatment group of the animal or the previously measured hpv . 
 [ 25 ] using a scale of 04 , where 0 = no inflammation , 1 = unequivocal inflammation of one joint of the paw , 2 = unequivocal inflammation of at least two joints of the paw or moderate inflammation of one joint , 3 = severe inflammation of one or more joints , and 4 = maximum inflammation of one or more joints of the paw . thus , the maximum possible score for both hind paws was 8 . 
die bestrahlungstage sind mit pfeilen gekennzeichnet ( schwarz : tage 1014 [ gruppe 5 ] ; grau : tage 1519 [ gruppen 6 und 7 ] ; wei : tage 10 , 12 , 14 , 16 und 18 [ gruppe 10 ] )  . 
 the application of 5 ( cid : 1 ) 1.0 gy in the protracted scheme on days 10 , 12 , 14 , 16 , and 18 ( group 10 ) led just to a positive trend toward a reduction of hpv , but this did not reach statistical significance as compared with sham - irradiated hind paws ( figure 1 )  . 
 arthritis score ( as ) the analysis of the semiquantitative parameter as was performed to obtain a second clinical parameter for the evaluation of the arthritic reaction in sham - irradiated and locally x - irradiated animals during the observation period . 
only a nonsignificant trend for a reduction of hpv after 5 ( cid : 1 ) 1.0 gy on days 2226 ( group 8 ) was observed ( figure 2 )  . 
 following 5 ( cid : 1 ) 1.0 gy on days 1014 ( group 4 ) , a somewhat slower increase of hpv was measured as compared to sham - treated animals ( group 1 )  . 
 after the application of 5 ( cid : 1 ) 0.5 gy in the protracted scheme on days 10 , 12 , 14 , 16 , and 18 ( group 11 ) , a slightly reduced increase of hind paw swelling was observed . 
die behandlungstage sind mit pfeilen gekennzeichnet ( schwarz : tage 1014 [ gruppe 4 ] ; grau : tage 10 , 12 , 14 , 16 und 18 [ gruppe 11 ] ; wei : tage 1014 und 2226 [ gruppe 12 ] )  . 
 as for hpv , two courses of 5 ( cid : 1 ) 0.5 gy on days 1014 and 2226 ( group 12 ) resulted in the most pronounced positive effect on as . 
 in summary , over the three trials we found a significant decrease of the clinical arthritis parameters following 5 ( cid : 1 ) 0.5 gy ( figure 4 ) or 5 ( cid : 1 ) 1.0 gy ( figure 5 ) during the florid phase of the inflammatory response . 
the most pronounced treatment effect was reached after two daily fractionated series of 5 ( cid : 1 ) 0.5 gy with an early treatment onset ( days 1014 ) and repetition in interval ( days 2226 ; figure 4 )  . 
 after the application of 5 ( cid : 1 ) 1.0 gy on days 1014 or in a protracted scheme ( days 10 , 12 , 14 , 16 , and 18 ; group 10 ) , only a nonsignificant positive trend could be detected . 
klinische wirksamkeit von 5 ( cid : 1 ) 0 , 5 gy in abhngigkeit vom behandlungsbeginn . dargestellt ist der verlauf des hinterpfotenvolumens ( hpv ) nach applikation von 5 ( cid : 1 ) 0 , 5 gy an tagen 1014 ( gruppe 5 ) , tagen 1519 ( gruppe 7 ) , tagen 2226 ( gruppe 9 ) , tagen 10 , 12 , 14 , 16 und 18 ( gruppe 11 ) oder in zwei serien an den tagen 1014 sowie 2226 ( gruppe 12 ) nach arthritisinduktion . 
3 urban & vogel chronic granulomatous tissue in vivo [ 11 ] and the reduced inos activity of inflammatory macrophages in vitro [ 9 , 11 ] after low - dose x - irradiation . 
 experimental investigations to prove the efficacy of different fractionation schemes , different radiation doses , and the relevance of the treatment onset in animal models of arthritis are almost absent . 
first , it might confirm the empirically established clinical knowledge that low - dose x - irradiation during the florid phase of arthritis is able to exert antiinflammatory activity , and that an early treatment onset ( day 10 ) with five daily fractionated single dose of 0.5 gy ( group 5 ) seems to be more effective than 5 ( cid : 1 ) 1.0 gy ( group 4 )  . 
additionally , treatment onset at the same time in a protracted manner ( days 10 , 12 , 14 , 16 , and 18 ) with the same single and total doses ( groups 10 and 11 ) did not improve the clinical signs of experimental arthritis . 
 second , in agreement with our previous findings [ 8 ] daily fractionated x - irradiation during the acute maximum of the inflammatory response ( days 1519 ) with either 5 ( cid : 1 ) 0.5 gy ( group 7 ) or 5 ( cid : 1 ) 1.0 gy ( group 6 ) is equally effective . 
 third , two series of 5 ( cid : 1 ) 0.5 gy with an early treatment onset ( days 1014 ) and repetition in interval ( days 2226 ) were liebmann a , et al . 
in acute situations , these single doses are applied four to five times a week up to total doses of 35 gy , and in chronic situations , two to three fractions a week are given up to total doses of 612 gy [ 20 ]  . however , single doses , total doses , and fractionation schedules currently used in clinical practice are empirical and mainly based on clinical observations established by von pannewitz [ 15 , 16 ]  . 
 several studies using animal models of arthritis have shown that low - dose x - irradiation with single doses of 0.51.5 gy and total doses of 2.57.5 gy demonstrates antiinflammatory efficacy both clinically and histologically [ 3 , 6 , 8 , 14 , 24 ]  . 
 recently , we demonstrated , in the adjuvant arthritis model using an experimental setup closely related to the treatment schedules clinically used in radiotherapy of osteoarthritis , that daily fractionated doses of 5 ( cid : 1 ) 1.0 gy or 5 ( cid : 1 ) 0.5 gy during the maximum of the acute inflammatory response ( days 1519 ) significantly reduced the inflammatory and destructive signs usually characteristic of this macrophage - driven arthritis model [ 8 ]  . 
especially , the histopathologic analysis revealed highly significant reduction of cartilage and bone destruction during the chronic stage of the arthritic disease ( day 30 ) with minimal or almost absent effect on the number of inflammatory cells in the periarticular tissue in both irradiated groups [ 8 ]  . 
inos is locally increased in arthritic joints of patients , which through synthesis of no plays a pathophysiological role in arthritic disease progression [ 1 , 2 , 4 , 5 ]  . 
in macrophage - driven experimental arthritis models , pharmacological inhibition of no production clinically and histologically attenuates arthritis , and , furthermore , considerably reduces important catabolic factors [ 17 ]  . 
klinische wirksamkeit von 5 ( cid : 1 ) 1 , 0 gy in abhngigkeit vom behandlungsbeginn . dargestellt ist der verlauf des hinterpfotenvolumens ( hpv ) nach applikation von 5 ( cid : 1 ) 1 , 0 gy an tagen 1014 ( gruppe 4 ) , tagen 1519 ( gruppe 6 ) , tagen 2226 ( gruppe 8 ) oder an den tagen 10 , 12 , 14 , 16 und 18 ( gruppe 10 ) nach arthritisinduktion . 
low - dose x - irradiation of adjuvant arthritis the most effective treatment schedule in our experimental study , and , finally , treatment onset during the chronic phase ( days 2226 ) with either 5 ( cid : 1 ) 0.5 gy or 5 ( cid : 1 ) 1.0 gy did not show any significant positive clinical effect . 
 the time dependence of the effectiveness of low - dose radiotherapy for adjuvant - induced arthritis is in line with our observations that low - dose irradiation directly interferes with the signaling processes involved in the development of inflammation [ 18 ]  . 
two series of 5 ( cid : 1 ) 0.5 gy with an early treatment onset ( days 1014 ) and repetition in interval ( days 2226 ) were the most effective treatment schedule in our experimental study . 
 acknowledgments this work was partially supported by the research commission of the medical faculty of the university of leipzig and the bmbf within the framework of the nbl - 3 - program ( 01zz0106 ; formel1 - project )  . 
 strahlentherapie und onkologie original article irradiation and various cytotoxic drugs enhance tyrosine phosphorylation and ( cid : 1 ) in human a549 lung cancer cells in a substratum - dependent manner in vitro nils cordes1 , christina beinke1 , ludwig plasswilm2 , dirk van beuningen1 1 - integrin clustering background and purpose : interactions of cells with a substratum , especially extracellular matrix proteins , initiate clustering of integrin receptors in the cell membrane . 
this process represents the initial step for the activation of signaling pathways regulating survival , proliferation , differentiation , adhesion , and migration , and could , furthermore , be important for cellular resistancemediating mechanisms against radiation or cytotoxic drugs . 
colony formation assays , immunofluorescence staining in combination with activation of integrin clustering using anti - ( cid : 1 ) 1 - integrin antibodies ( k20 ) , and western blotting for tyrosine phosphorylation under treatment of cells with the ic50 for irradiation ( 2 gy ; ic50 = 2.2 gy ) , cisplatin ( 2 m ) , paclitaxel ( 5 nm ) , or mitomycin ( 7 m ) were performed . 
the clustering of ( cid : 1 ) 1 - integrins examined by immunofluorescence staining was only stimulated by irradiation , cisplatin , paclitaxel , or mitomycin in case of cell attachment to fn . 
by contrast , tyrosine phosphorylation , as one of the major events following ( cid : 1 ) 1 - integrin clustering , showed a 3.7 - fold , fn - related enhancement , and treatment of cells with the ic50 of radiation , cisplatin , paclitaxel , or mitomycin showed a substratum - dependent induction . 
 conclusion : for the first time , a strong influence of irradiation and a variety of cytotoxic drugs on the clustering of ( cid : 1 ) 1 - integrins could be shown . 
these data are not only important for the understanding of cellular resistance against cytotoxic agents but , furthermore , for tumor progression , anchorage - independent cell growth , and , possibly , the optimization of radiochemotherapeutic strategies . 
 key words : ( cid : 1 ) 1 - integrin clustering extracellular matrix ionizing radiation drugs strahlenther onkol 2004 ; 180 : 15764 doi 10.1007 / s00066 - 004 - 1144 - 2 bestrahlung sowie unterschiedliche zytostatika verstrken die tyrosinphosphorylierung und das ( cid : 1 ) in humanen a549 - bronchialkarzinomzellen in einer substratabhngigen weise in vitro 1 - integrin - clustering hintergrund und ziel : interaktionen von zellen mit einem substrat , insbesondere spezifischen proteinen der extrazellulren matrix , initiieren ein zusammenballen ( clustering ) von integrinrezeptoren in der zellmembran . 
 material und methodik : humane , auf polystyrol oder fibronectin ( fn ) wachsende a549 - bronchialkarzinomzellen wurden mit aufsteigenden dosen von 08 gy bestrahlt oder mit cisplatin ( 0 , 150 m ) , paclitaxel ( 0 , 150 nm ) oder mitomycin ( 0 , 150 m ) behandelt . 
koloniebildungsassays , immunfluoreszenzfrbungen in kombination mit der aktivierung des integrinclusterings sowie western - blotting zum nachweis der tyrosinphosphorylierung wurden unter behandlung mit den ic50 fr die bestrahlungsdosis und die zytostatikakonzentrationen durchgefhrt . 
 1 institute of radiobiology , german armed forces , munich , germany , 2 department of radiation oncology , university hospital basel , switzerland received : january 13 , 2003 ; accepted : august 6 , 2003 strahlenther onkol 2004 no . 
das clustering von ( cid : 1 ) 1 - integrinen , mittels immunfluoreszenzfrbung untersucht , wurde durch bestrahlung , cisplatin , paclitaxel und mitomycin lediglich in zellen , die auf fn wuchsen , stimuliert . 
im gegensatz hierzu zeigte die untersuchung der tyrosinphosphorylierung , als eines der hauptereignisse im anschluss an ein ( cid : 1 ) 1 - integrin - clustering , eine 3 , 7fache , fn - bedingte verstrkung . 
 schlsselwrter : ( cid : 1 ) 1 - integrin clustering extrazellulre matrix ionisierende strahlung zytostatika introduction cell attachment to proteins of the extracellular matrix ( ecm ) is a physiological process involving various cell adhesion molecules . 
interactions between cells and ecm proteins are not only adhesion - related but , furthermore , participate in the regulation of critical cell functions , i.e. , survival , proliferation , differentiation , and migration [ 7 , 21 , 41 , 47 ]  . 
several ten to 100 integrin receptors in combination with growth factor receptors are recruited to discrete sites within the cell membrane forming an area termed focal adhesion site [ 3 ]  . 
subsequent to cell attachment , specific intracellular effectors couple integrins and growth factor receptors to specific downstream signaling targets [ 28 ] such as integrinlinked kinase ( ilk ) [ 23 ] , protein kinase b / akt ( pkb / akt ) [ 15 , 30 ] , glycogen synthase kinase - 3 ( gsk - 3 ) [ 16 , 25 , 45 ] , focal adhesion kinase ( fak ) [ 40 ] , or protein kinases of the rasmitogen - activated protein kinase ( mapk ) pathway [ 27 ]  . 
in agreement with findings of other groups [ 20 , 38 ] , we have previously shown that the cellular sensitivity to radiation [ 8 , 10 ] as well as to a combined drug - radiation exposure [ 9 ] is greatly reduced at the presence of specific ecm proteins . 
a number of chemotherapy agents that are able to enhance the effectiveness of rt , such as cisplatin , paclitaxel , and mitomycin , are considered the standard treatment for patients with a number of cancer types . 
this process causes interstrand dna cross - links . treatment of head and neck cancer , cervical cancer , esophageal cancer as well as lung cancer is a major clinical indication [ 1 , 19 , 35 , 36 , 43 , 46 ]  . 
paclitaxel extracted from the bark of the pacific yew taxus brevifolia has shown cytotoxic activity in vitro and in vivo [ 11 , 31 , 37 , 39 ]  . 
major clinical indications of radiochemotherapy based on mitomycin administration are the treatment of patients with head and neck cancer , epidermoid carcinoma of the anal canal , or lung cancer [ 13 , 17 , 18 , 22 , 44 ]  . 
 since detailed studies concerning the possible molecular mechanisms involved in this radioand chemosensitivity - reducing phenomenon have not been performed so far , we focused on the influence of irradiation and treatment with various cytotoxic drugs on the initial step in cell - ecm adhesion , the event of integrin clustering , and the subsequent phosphorylation of tyrosine amino acid residues . 
dulbeccos modified eagles medium ( dmem ; gibco , karlsruhe , germany ) supplemented with 10% fetal bovine serum ( paa , linz , austria ) and 1% nonessential amino acids ( gibco ) was applied to cultivate the cells . 
 radiation exposure irradiation was delivered at room temperature using single doses of 240 - kv x - rays ( isovolt 320 / 10 ; seifert , ahrensburg , germany ) filtered with 3 mm berylliuthe absorbed dose was measured using a duplex dosimeter ( ptw , freiburg , germany )  . 
 drug exposure cisplatin ( platinex ; bristol - myers squibb gmbh , germany ) , paclitaxel ( taxol ; bristol arzneimittel gmbh , germany ) , and mitomycin ( mitomycin medac ; medac , germany ) were obtained as 10.0 mg / 20 ml infusion solution , 6.0 mg / 5 ml infusion solution , and 10.0 mg / 10 ml infusion solution , respectively . 
exponentially growing cells were plated onto noncoated or fibronectin - ( fn - ) precoated ( 1 g / cm2 ; becton dickinson , heidelberg , germany ) six - well dishes ( becton dickinson ) 24 h prior to irradiation or cisplatin ( 0.150 m 1 h ) , paclitaxel ( 0.150 nm , 3 h ) , or mitomycin ( 0.150 m , 1 h ) exposure . 
 immunofluorescence staining and confocal scanning microscopy 5 ( cid : 2 ) 103 a549 cells were seeded on noncoated or fn - precoated lab tek chamber slides ( nalge nunc international , hamburg , germany )  . 
1 h after irradiation or the specific drug exposure times , cells were stimulated with specific anti - ( cid : 1 ) 1 - integrin antibodies ( k20 ; 1 : 100 ; dako , hamburg , germany ) for ( cid : 1 ) 1 - integrin clustering for 30 min at 37 c 10% co2 . 
subsequently , secondary antibodies , cy2 - conjugated affinipure goat antimouse igg , were used at a dilution of 1 : 100 ( dianova , hamburg , germany ) to visualize ( cid : 1 ) 1 - integrin clusters . 
 total protein extraction 24 h after plating cells on fn or polystyrene , irradiation ( 2 gy ) or treatment with cisplatin ( 2 m , 1 h ) , paclitaxel ( 5 nm , 3 h ) , or mitomycin ( 7 m , 1 h ) was performed . 
cells were lysed using 50 mm tris - hcl ( ph 7.4 ) , 1% np - 40 , 0.25% sodium deoxycholate , 150 mm nacl , 1 mm edta supplemented with protease inhibitor cocktail complete ( roche , mannheim , germany ) , 5 mm sodium vanadate , and 5 mm sodium fluoride . 
 western blot 25 g total protein extracts were separated by sds - polyacrylamide electrophoresis , transferred onto a nitrocellulose membrane ( schleicher and schuell gmbh , dassel , germany ) , blocked using 5% nonfat dry milk powder in pbs and probed overnight at 4 c with monoclonal mouse anti - phosphotyrosine antibodies ( 4g10 ; 1 : 1 , 500 ; upstate , hamburg , germany )  . three independent experiments were performed . 
the protein detection was accomplished using specific hrp - conjugated goat anti - mouse antibodies in combination with the enhanced chemiluminescence detection systems ( ecl ; amersham , freiburg , germany )  . 
 results colony formation assay the presence of fn resulted in a significantly decreased radioand chemosensitivity of a549 cells in comparison with the treatment of cells on polystyrene ( figure 1 )  . 
for irradiation , cisplatin , paclitaxel , or mitomycin , the clonogenic survival was significantly improved at doses 4 gy or for concentrations 0.1 m , 5 nm , or 10 m , respectively . 
enhanced integrin clustering 101 102 103 dose ( gy ) concentration of cddp ( m ) concentration of paclitaxel ( nm ) concentration of mitomycin ( m ) figure 1 . 
cells plated on polystyrene ( p , ( cid : 1 ) ) or fibronectin ( fn , ( cid : 2 ) ) were exposed to irradiation , cisplatin ( cddp ) , paclitaxel , or mitomycin at various doses or concentrations , and the clonogenic survival was determined . 
zur messung des klonogenen berlebens nach bestrahlung , cisplatin ( cddp ) , paclitaxeloder mitomycingabe wurden zellen auf polystyrol ( p , ( cid : 1 ) ) oder fibronectin ( fn , ( cid : 2 ) ) ausgest . 
 analysis of tyrosine phosphorylation plating of cells on fn , in contrast to polystyrene , greatly induced ( 3.7 - fold ) basal tyrosine phosphorylation in untreated a549 controls in the molecular range of mr ~ 60 , 000 , 63 , 00068 , 000 , 120 , 000160 , 000 , and ~ 220 , 000 ( figures 3a and 3b )  . 
 although ( cid : 1 ) 1 - integrin clustering was only observed at fn presence under the different treatment regimes , substratumdependent changes in tyrosine phosphorylation were detected after irradiation ( 1.8 - fold ) , cisplatin ( 1.2 - fold ) , and paclitaxel ( 1.45 - fold ) in cells on polystyrene and after irradiation ( 1.2fold ) and paclitaxel ( 1.2 - fold ) in cells on fn ( figure 3b )  . 
 discussion as cells adhere to a substratum coated with ecm proteins , integrins become localized on the ventral surface of the cell in membrane structures known as focal adhesion sites [ 4 , 6 ]  . 
in our investigations , antibodies against ( cid : 1 ) 1 - integrins were used to mimic the early events of focal adhesion site formation , particularly the clustering of integrins in discrete patches . 
the use of specific anti1 - integrin antibodies allowed ( cid : 1 ) ( cid : 1 ) 1 - integrin - mediated signaling events to be studied in a controlled manner . 
our findings demonstrate that antibody - mediated ( cid : 1 ) 1 - integrin clustering led to enhanced tyrosine phosphorylation of protein complexes of 6068 , 120160 , and ~ 200 kda in the presence but not in the absence of the ecm protein fn . 
although the identities of the proteins of these complexes are currently unknown , especially the proteins between 120160 kda are clearly not integrin subunits . thus , integrin - stimulated phosphorylation of protein complexes may reflect a biochemical signaling process , although the exact nature of that process awaits elucidation . 
most interestingly , the clustering of ( cid : 1 ) 1 - integrins was enhanced by irradiation and the mechanistically different - functioning cytotoxic drugs cisplatin , paclitaxel , and mitomycin in a substratum - dependent manner . 
concomitant tyrosine phosphorylation , however , was induced by cell attachment to fn as well as radiation and paclitaxel exposure in cells on polystyrene . generally , cells on fn responded less sufficiently to the different cytotoxic agents in terms of tyrosine phosphorylation , which was due to the fn - related high basal levels . 
 findings regarding cell adhesion - mediated radioresistance ( cam - rr ) have been reported by a few groups during the last 10 years [ 20 , 38 ]  . 
recently , we were able to corroborate these observations in a variety of tumor and normal cell lines , and , furthermore , to uncover a central role of ( cid : 1 ) 1 - integrins within the cellular response to ionizing radiation and radiation - mediated improvement of cell adhesion to ecm proteins [ 8 , 10 , 33 ]  . 
immunofluorescence images show the enhanced clustering phenomenon of ( cid : 1 ) 1 - integrins ( arrows ) after treatment of cells grown on fibronectin ( a ) or polystyrene ( b ) with irradiation ( ir , 2 gy ) , cisplatin ( cddp , 2 m , 1 h ) , paclitaxel ( 5 nm , 3 h ) , or mitomycin ( 7 m , 1 h ) using specific clustering - inducing anti - ( cid : 1 ) 1 - integrin antibodies ( clone k20 ) in comparison with untreated controls . 
die immunfluoreszenzbilder zeigen das verstrkte , durch spezifische ( cid : 1 ) 1 - integrin - antikrper ( klon k20 ) induzierte clusterphnomen von ( cid : 1 ) 1 - integrinen ( pfeile ) nach einer behandlung der zellen auf fibronectin ( a ) oder polystyrol ( b ) mit bestrahlung ( ir , 2 gy ) , cisplatin ( cddp , 2 m , 1 h ) , paclitaxel ( 5 nm , 3 h ) oder mitomycin ( 7 m , 1 h ) im vergleich zu unbehandelten kontrollen . 
in the present study , the impact of the ecm protein fn on the cytotoxic potential of three different drugs , each with a unique mechanism of action , could be shown . 
cell adhesion - mediated drug resistance ( cam - dr ) is a wellknown phenomenon [ 14 , 24 , 42 ] , but detailed insights into the complex cellular networks , which accomplish this improved resistance , are rare . 
in fact , although the degree of resistance to cytotoxic drugs induced by cell adhesion is lower than that seen with many acquired mechanisms of drug resistance , e.g. , p - glycoprotein overexpression , cam - dr represents a novel intrinsic pathway for evading drug - induced cell death , especially apoptosis in leukemia cell lines [ 14 , 24 ]  . 
since even very small surviving tumor fractions < 1% have the potential to generate a large drug - resistant cell population after initial treatment with either irradiation or drugs , the importance of de novo mechanisms of radiation and drug resistance may be greatly underestimated . 
generally , high - level cellular resistance mechanisms cannot be found in a heterogeneous tumor cell population , and de novo resistance mechanisms such as cam - rr or cam - dr may provide sufficient figure 2b abbildung 2b cytoprotective ability to allow the emergence of these acquired mechanisms . 
 ( cid : 1 ) 1 - integrins seem to have the ability to protect cells from different forms of cell death , which suggests a block in the initiation or execution of cell death events at a point of general convergence . 
 elucidating the initial event upon cell attachment to a substratum , the integrin clustering activates the aforementioned biochemical pathways , which then participate in the regulation of various cell functions . 
regarding the lack of data on this issue , our findings clearly show that the physiological cell substratum fn plays an important role within this cellular responsiveness , which again questions cytotoxicity data of former studies only performed on polystyrene . 
 ( cid : 1 ) 1 - integrin clustering could only be performed on the physiological substratum and , thus , may be in part responsible for the observed fn - dependent improvement of survival via specific yet unknown pathways that seem to be substratum - specific and are also highly affected by the cytotoxic agents delivered . 
the most likely interpretation is that the clustering process causes the integrin to interact with another protein , which itself is a kinase or a phosphatase involved in downstream signaling . 
additionally , diverse forms of cross talk between tyrosine kinases or phosphatases and other signaling cascades reported [ 5 , 48 ] have to be taken into consideration for the differential effects observed in cells grown on fn or polystyrene . 
 for the first time , a strong influence of irradiation and a variety of cytotoxic drugs on the clustering of ( cid : 1 ) 1 - integrins is shown . 
although the exact mechanism mediating cam - rr and cam - dr remains elusive , these data strongly support different mechanisms of action to be proceeded in case of cell attachment to specific ecm proteins such as fn . 
besides the important impact on cellular resistance against cytotoxic agents , our results might also provide insights into tumor progression , anchorage - independent cell growth , and the optimization of radiochemotherapeutic strategies . 
 strahlentherapie und onkologie original article phyllodes tumor : an unexpected tumor of the breast a report on six patients heidi stranzl1 , florentia peintinger2 , arnulf hackl1 background and purpose : to evaluate the role of adjuvant radiotherapy for an unexpected malignancy of the breast , known as phyllodes tumor , a retrospective study was undertaken . patients and methods : between 1994 and 2002 , six female patients with a phyllodes tumor ( borderline , n = 2 ; malignant , n = 4 ) were irradiated after modified radical mastectomy at our institution . 
 key words : phyllodes tumor breast adjuvant radiotherapy strahlenther onkol 2004 ; 180 : 14851 doi 10.1007 / s00066 - 004 - 1182 - 9 phylloidestumor : ein seltener tumor der brust . 
 patienten und methodik : sechs patientinnen mit einem phylloidestumor ( borderline n = 2 ; maligne n = 4 ) wurden zwischen 1994 und 2002 nach modifizierter radikaler mastektomie bestrahlt . 
the internationally accepted name now is phyllodes tumor and accurately de1 department of radiotherapy , university medical school , graz , austria , 2 division of gynecology , leoben , austria . received : april 9 , 2003 ; accepted : september 29 , 2003 strahlenther onkol 2004 no . 
in contrast to fibroadenoma , stroma of a phyllodes tumor contains marked cellularity , nuclear atypia , increased mitotic figures , and overgrowth of the stromal elements [ 7 , 18 ]  . 
 the entity produces a spectrum of diseases that range from benign phyllodes tumors , which very rarely metastasize , over borderline to malignant phyllodes tumors , in which metastases have been estimated to occur in up to 25% of patients [ 6 , 7 , 14 ]  . 
 six patients treated postoperatively with adjuvant radiotherapy were identified as having borderline ( n = 2 ) and malignant ( n = 4 ) phyllodes tumors and are the subject of our report . 
in all six patients , computer - aided tomography treatment planning was done , which allowed to quantify the volume and dose delivered to the organs at risk [ 19 ]  . 
the only patient who failed distantly with multiple pulmonary age ( years ) histology size ( mm ) site surgery margins palpable ln no involved ln no td ( gy ) pulmonary fu ( months ) 29 outcome metastases received an ifosfamide - containing chemotherapy regimen . patients were routinely observed for tumor control in 3to 4 - month intervals during the first 3 years , and in 6 - month intervals thereafter . 
 results median follow - up was 33.8 months ( range 2942 months )  . four out of six patients are alive and free of disease 25 , 31 , 35 , and 41 months postoperatively . 
one patient initially presenting with a malignant phyllodes tumor failed locally after 17 months and died due to a cause unrelated to the tumor . she presented a resection margin of 7 mm postoperatively and refused recommended reexcision . 
the other patient with a borderline phyllodes tumor relapsed after 23 months with a malignant phyllodes tumor and died because of multiple pulmonary metastases , diagnosed 3 months after local failure . details are given in table 1 . 
ad : axillary dissection ; dm : distant metastases ; dod : dead of disease ; fu : follow - up ; ln : lymph nodes ; loq : lower outer quadrant ; lr : local recurrence ; m : modified radical mastectomy ; ned : no evidence of disease ; td : total dose ; uiq : upper inner quadrant ; uoq : upper outer quadrant . 
ad : axillre dissektion ; dm : fernmetastasen ; dod : tod am tumor ; fu : follow - up ; ln : lymphknoten ; loq : unterer uerer quadrant ; lr : lokalrezidiv ; m : modifizierte radikale mastektomie ; ned : kein hinweis auf tumor ; td : gesamtdosis ; uiq : oberer innerer quadrant ; uoq : oberer uerer quadrant . 
however , some individuals present masses with a rapid growth in a previously stable lump causing increased pressure in the skthis can lead to shiny stretched skin , dilated veins and even ulcerations over the tumor mass , though the skin itself is not involved [ 12 , 17 ]  . 
25% of phyllodes tumors are verified histologically to be malignant [ 7 , 23 ]  . benign tumors very rarely metastasize , in contrast to malignant specimens , which show systemic failure in approximately 25% of patients [ 6 , 7 , 14 ]  . 
in an overview of the literature [ 5 ] in patients with borderline and malignant tumors , the average local failure rate associated with mastectomy was only 18% , in contrast to 31% after conservative breast surgery . 
therefore , we conclude that a margin of at least 10 mm is recommended . phyllodes tumors are surrounded by a pseudocapsule of dense , compressed , normal tissue that may contain microscopic lesions . 
to obtain a microscopic clear margin of almost 10 mm , surgical intervention requires > 10 mm gross marg because of the rarity of disease , the adequacy of margins has never been subject of randomized trials . 
 metastatic disease is generally rare , even in large tumors , and has been reported in 520% of all phyllodes tumors [ 6 , 7 ]  . distant metastases will be observed in approximately 30% of malignant phyllodes tumors [ 6 , 7 , 14 ]  . 
the most common site of the initially diagnosed distant failure is the lung ( 66% ) , in a roughly decreasing frequency followed by bones ( 28% ) and liver in 15% of cases [ 7 , 10 ]  . 
 some authors describe the average time interval to local relapse to be 32 months for benign , 22 months for malignant , and 18 months for borderline phyllodes tumors [ 23 ]  . 
yet , postoperative adjuvant radiotherapy is recommended in highrisk ( i.e. , borderline , malignant , large tumors , close or uncertain surgical margins ) phyllodes tumors [ 3 , 5 , 8 , 9 ]  . 
based on our analysis and other existing data , we conclude that postoperative local radiotherapy is indicated for borderline and malignant phyllodes tumors of the breast , if there are any adverse factors , such as large preoperative tumors and close or uncertain resection margins . 
 strahlentherapie und onkologie original article late effects of post - high - dose - rate brachytherapy for oropharyngeal carcinoma : are they severer than post - low - dose - rate ? takayuki nose1 , didier peiffert2 , michel lapeyre2 , sylvette hoffstetter2 , masahiko koizumi1 , kinji nishiyama1 background : late effects by high - dose - rate ( hdr ) brachytherapy have been believed severer than low - dose - rate ( ldr ) provided tumor control was constant . 
the hdr schedule was 21 gy / 3.5 fractions / 2 days following 46 gy / 23 fractions external beam , while 25 gy / 3 days following 50 gy / 25 fractions external beam was for ldr . 
lokale kontrollen von im osaka medical center mit hdr behandelten patienten mit oropharyngealkarzinom wurden mit einer im centre alexis vautrin durchgefhrten studienserie mit ldr ( jeweils 82% und 79 , 9% ) verglichen . 
 patienten und methoden : die daten von 29 mit hdr und 24 mit ldr behandelten patienten ( durchschnittliche beobachtungszeit jeweils 27 und 29 , 5 monate ( p = 0 , 89 ) ) wurden gesammelt . 
das hdr - protokoll umfasste 21 gy / 3 , 5 fraktionen / 2 tage , gefolgt von 46 gy in 23 fraktionen durch externe bestrahlung , whrend fr die ldr 25 gy / 3 tage , gefolgt von 50 gy in 25 fraktionen durch externe bestrahlung , eingesetzt wurden . 
hinsichtlich frequenz , schwere und dauer der mukosaschden fanden sich keine unterschiede in den sptfolgen ( p = 0 , 90 , 0 , 12 , 0 , 40 )  . 
although considerable anatomical sites were treated with high - dose - rate ( hdr ) 192ir interstitial brachytherapy at several centers , radioexposure to medical personnel is an obstacle to the widespread use of this modality [ 2 , 6 , 7 , 14 , 16 ]  . 
 in our institutes ( osaka medical center [ omc ] and osaka university hospital [ ouh ] ) , more than 80 oropharyngeal carcinoma patients have been treated by hdr . 
 hdr group between february 2002 and june 2002 , a total of 46 oropharyngeal carcinoma patients , who had been treated by hdr brachytherapy , visited omc for follow - up . 
implants were performed with the plastic tube technique , which was developed in the 1970s mostly at cav and have been in clinical use at many centers for more than 20 years [ 13 ]  . 
the standard schedule was 1836 gy ( median 21 ) / 36 fractions / 13 days hdr following median 46 gy / 23 fractions / 4.5 weeks external radiotherapy ( 4546 gy , 22 patients ) with a 23 weeks gap . 
 ldr group between april 1999 and july 1999 , a total of 27 oropharyngeal carcinoma patients , who had been treated by ldr brachytherapy , visited cav for follow - up . 
the standard schedule was 2035 gy ( median 25 ) / 24 days following median 50 gy / 25 fractions / 5 weeks external radiotherapy ( 4050 gy , 23 patients ) with a 23 weeks gap . 
 dose specification planning computers used were cadplanbt ( varian tem , uk ) , plato ( nucletron , the netherlands ) , and dosigray ( dosigray , france ) for omc , ouh , and cav , respectively . 
ensuring clinical target volume coverage as well as keeping hyperdose sleeves diameter 810 mm was the common principle for both groups at omc and cav [ 10 , 11 ]  . 
median maximum diameter of hyperdose sleeve was 7.3 mm ( range 4.116.5 mm ) at omc , and 6 mm ( range 118.8 mm ) at cav , respectively ( p = 0.03 , smaller for cav )  . 
for hdr group , median volume irradiated with 0 prescribed dose ( v100 ) and that with 1.5 times prescribed dose ( v150 ) were 21.7 cm3 ( range 3.459.3 cm3 ) and 9.4 cm3 ( range 1.220.8 cm3 ) , respectively . 
 late changes : musculo - mucosal changes evaluation at follow - up exam , mucosal conditions were evaluated using the rtog / eortc late morbidity scoring scheme for mucous membrane ( table 2 )  . 
at least two photos for each patient ( resting and protrusion / phonation ) were sent to cav , france , and the scores were checked by two of the authors ( dp , ml )  . 
 * * subsite group a : tonsil , soft palate and uvula ; subsite group b : anterior pillar and glossotonsillar sulcus ; subsite group c : base of tongue and vallecula . 
 rtog / eortc late radiation morbidity scoring scheme ( mucous menbrane ) grade 0 modified dische score grade 0 erythema ulceration edema thinning of mucosa pallor of mucosa telangiectasia mobility impairment of the tonque mobility impairment of the faucial pillars none slight atrophy and dryness moderate atrophy and telangiectasia / little mucous marked atrophy with complete dryness / severe telangiectasia ulcerations fistular nil none nil nil nil none symmetrical / not impaired symmetrical / not impaired slight superficial tissue slight slight slight < 1 cm2 asymmetrical during protrusion asymmetrical during phonation moderate deep / soft moderate moderate moderate 14 cm2 asymmetrical at resting position asymmetrical at resting position severe bony severe severe severe 4 cm2 < fixed fixed ( dp , ml , sh ) at cav . 
 follow - up intervals the routine follow - up interval was 1 month for the first year , 2 months for the second year , and 36 months thereafter for hdr patients . 
for both cohorts , no attempt was made to modify follow - up intervals to collect neither more nor better results for this study and all patients came to follow - up clinic properly according to planned reservations . 
for mucosal change evaluation , when the patients came more than twice for routine follow - up during the study periods ( hdr : 12 of 29 , ldr : 5 of 24 ) , the latest evaluation was employed for the study . 
the frequency for ldr ( 29.2% ) in this study was comparable with the previously reported frequency of 26.6% among 277 patients from the same institute [ 13 ]  . 
the consistency for hdr patients was as follows : consistent 63% , one - grade difference 34% , two - grade difference 3% ; no 3or 4 - grade difference was found . 
the consistency for ldr patients was as follows : consistent 68% , 1 - grade difference 27% , 2 - grade difference 5% ; no 3or 4 - grade difference was observed . 
 none < 3 months < 12 months 12 months < mucosal damage duration ( p = 0.40 ) modified dische score figure 2b represents the distribution of the modified dische score . 
 discussion evaluation of late effects should be based on reproducible systefor the two systems used in the current study , the scoring consistency including one - grade difference among authors was excellent ( 97% for hdr patients and 95% for ldr patients ) with no 3or 4 - grade differences . 
 the current study suggested hdr and the standard ldr treatment resulted in comparable late effects while achieving comparable local control ( 82% for 82 patients at omc , 79.5% for 277 patients at cav ) [ 10 , 13 ]  . 
fractionated hdr schedule of osaka was originally determined based on clinical observations of hdr dose that induced equivalent acute mucositis induced by standard ldr dose , independently of linear - quadratic model [ 19 ]  . 
recently , based on the continuously hyperfractionated accelerated radiotherapy ( chart ) results , repair half - time was predicted as 3.84.9 h , which was considerably longer than previously assumed [ 1 ]  . 
 to replace 20 gy ldr , fractions / 1035 h 20 gy / 3 or 20 gy / 4 fractions / 35 h and more were predicted as the best hdr regimens with superior therapeutic ratio to ldr assuming repair half - time = 4 h . 
interestingly , these regimens were similar to the schedules used in the present study such as 18 gy / 3 fractions / 24 h or 24 gy / 4 fractions / 42 h . 
in that trial , 25 patients treated by exclusive hdr ( 60 gy / 10 fractions / 69 days ) and 26 patients by exclusive ldr ( 70 gy / 49 days ) were compared . 
while local control was equivalent ( 87% for hdr and 84% for ldr ) , tongue ulcer frequency was also comparable ( 1 / 25 for hdr and 1 / 26 for ldr )  . 
considering oropharyngeal cancer incidence in japan ( < 1% ) , it may take longer than decades . in conclusion , following the current dose schedules , late normal tissue effects showed no significant difference between hdr and ldr while tumor effects were also comparable . 
although more patient accrual is necessary to confirm the present findings , this study suggested that hdr is as safely applicable as ldr with the advantage of eliminating radioexposure to medical personnel . 
 strahlentherapie und onkologie original article radiation - induced changes of brain tissue after radiosurgery in patients with arteriovenous malformations : dose / volume - response relations sabine levegrn1 , holger hof2 , marco essig3 , wolfgang schlegel1 , jrgen debus2 purpose : to evaluate late radiation effects in the brain after radiosurgery of patients with cerebral arteriovenous malformations ( avms ) and to quantify dose / volume - response relations for radiation - induced changes of brain tissue identified on follow - up neuroimaging . patients and methods : data from 73 avm patients who had stereotactic linac radiosurgery at dkfz ( german cancer research center ) , heidelberg , germany , were retrospectively analyzed . 
the endpoint of radiation - induced changes of brain tissue on follow - up magnetic resonance ( mr ) neuroimaging ( i.e. , edema and blood - brain - barrier breakdown [ bbbb ] ) was evaluated . 
a previous analysis of the data found correlation of the endpoints with several dose / volume variables ( dv ) derived from each patients dose distribution in the brain , including the mean dose in a volume of 20 cm3 ( dmean20 ) and the absolute brain volume ( including the avm target ) receiving a dose of at least 12 gy ( v12 )  . 
to quantify dose / volume - response relations , patients were ranked according to dv ( i.e. , dmean20 and v12 ) and classified into four groups of equal size . 
 the dose / volume - response curves were fitted with a sigmoid - shape logistic function and characterized by dv50 , the dose for a 50% incidence , and the slope parameter k . results : dose / volume - response relations , based on two alternative , but correlated , dose distribution variables that are a function of both dose and volume , were observed for radiation - induced changes of brain tissue . 
this knowledge will eventually help to optimize radiosurgical treatments in avm patients . key words : arteriovenous malformation radiosurgery late radiation effect brain dose / volume response volume effect strahlenther onkol 2004 ; 180 : 758767 doi 10.1007 / s00066 - 004 - 1266 - 6 strahleninduzierte normalgewebevernderungen im gehirn nach stereotaktischer einzeit - hochdosisbestrahlung von patienten mit arteriovensen malformationen : dosis / volumen - wirkungs - beziehungen ziel : untersuchung spter strahlenfolgen im gehirn nach stereotaktischer einzeit - hochdosisbestrahlung von patienten mit zerebralen arteriovensen malformationen ( avm ) und quantifizierung der dosis / volumen - wirkungs - beziehungen von strahleninduzierten normalgewebevernderungen anhand von magnetresonanz - ( mr - ) bildgebung whrend der nachsorge . 
eine vorangegangene analyse der daten konnte eine korrelation der endpunkte mit verschiedenen dosis / volumen - variablen ( dv ) aufzeigen , die fr jeden patienten aus der dosisverteilung im gehirn berechnet wurden , wie z.b. 
die mittlere dosis in einem volumen von 20 cm3 1 department of medical physics , german cancer research center ( dkfz ) , heidelberg , germany , 2 department of radiation oncology , german cancer research center ( dkfz ) , heidelberg , germany , 3 department of radiology , german cancer research center ( dkfz ) , heidelberg , germany , received : december 3 , 2003 ; accepted : june 2 , 2004 strahlenther onkol 2004 no . 
dose / volume - response relations for changes of brain tissue after avm radiosurgery ( dmean20 ) und das absolute hirnvolumen ( einschlielich des avm - targets ) , das eine dosis von mindestens 12 gy erhlt ( v12 )  . 
der sigmoidale verlauf der dosis / volumen - wirkungs - kurven wurde mit hilfe einer logistischen funktion angepasst und durch dv50 , die dosis fr eine 50%ige inzidenz , sowie den steigungsparameter k charakterisiert . ergebnisse : strahleninduzierte normalgewebevernderungen im gehirn zeigten eine dosis / volumen - wirkungs - beziehung , wobei die abhngige variable eine funktion von dosis und volumen war . 
die genaue kenntnis der dosis / volumen - wirkungs - beziehungen kann zuknftig zur optimierung der strahlentherapie bei avm - patienten beitragen . schlsselwrter : arteriovense malformation radiochirurgie spte strahlenfolgen gehirn dosis / volumen - wirkungs - beziehung volumeneffekt introduction late radiation injury is the main dose - limiting factor for radiotherapy of lesions of the central nervous system ( cns )  . 
 although adverse effects after brain irradiation have been reported for several decades , there is still a critical need for more accurate information about the tolerance of the brain to radiation . 
 however , there is still a lack of reliable clinical data from both radiosurgery and fractionated radiotherapy on the volume effect in the bratolerance doses for specific partial volumes and endpoints have been suggested [ 3 , 18 ] , but the relationships of dose and volume to complications after irradiation of lesions in the brain have yet to be quantitatively assessed . 
the quantification of volume effects and the modeling of normal tissue response to partial irradiation of the brain are particularly demanding because of the highly differentiated and complex structure of the brain and the variety of endpoints after radiotherapy for cns diseases . since it is often difficult to separate the effect of the tumor from the effect of radiation on normal tissue reactions , an outcome analysis of benign malignancies such as arteriovenous malformations ( avms ) is of particular interest . 
radiosurgery today is known as successful modality to treat unresectable cerebral av however , follow - up neuroimaging in avm patients frequently shows the development of postradiosurgical changes of brain tissue , depending on the irradiated volume and the dose administered [ 69 , 13 , 14 , 20 ]  . 
in this study , we investigated late radiation effects in the brain for one specific avm data set in which both outcome information and dose distributions in the brain are available for each individual patient . 
we found that radiation - induced tissue changes after avm radiosurgery are well predicted by single dose distribution variables that are a function of both dose and volume , such as the mean dose in a specified volume of 20 cm3 and the volume receiving a dose of at least 12 gy . 
in this study , a continuation of our previous work , we described the radiologically observed dose / volume - response relationships by fitting a phenomenological normal tissue complication probability ( ntcp ) model based on dose / volume variables previously shown to correlate with the considered endpoints to the outcome data . 
the results will eventually help to guide dose prescriptions for individual avm patients treated with radiosurgery . patients and methods patient treatment between june 1993 and december 1998 , 108 patients with cerebral avms received stereotactic linac - based radiosurgery delivered using a micro - multileaf collimator ( stryker - leibinger ag , freiburg , germany ) , including the patients analyzed in this study . 
precise patient positioning was achieved using a specially designed mr - compatible ceramic ring attached to a stereotactic head frame which was fixed invasively to the skull , strahlenther onkol 2004 no . 
dose / volume - response relations for changes of brain tissue after avm radiosurgery enabling a positioning accuracy of < 1 mthree - dimensional ( 3 - d ) treatment planning was based mainly on computed tomography ( ct ) and mri , high - resolution ct angiography , and angiography in stereotactic setup . 
treatment planning was performed with the voxelplan system , enabling access to the full dose distribution information [ 11 ]  . the patients were treated with eleven to fourteen non - coplanar static fields delivered with 6or 15 - mv photons . 
a micro - multileaf collimator with a leaf width of 1 mm ( corresponding to 1.6 mm at isocenter distance ) was used to enable optimum field forming , especially for large , irregularly shaped av patients were followed in intervals of 3 months in the 1st year and then every 6 months with mri and neurologic examinations . 
today , brain necrosis is a rare complication after radiosurgery with an incidence of about 4% [ 4 , 8 ] , because clinical experience on underlying dose - response relationships is now available to guide the physicians prescriptions . 
these endpoints may not be dose - limiting , but may act as a precursor of more severe injuries occurring with higher doses and / or larger irradiated volumes . in this study , the endpoint of radiation - induced tissue changes on follow - up neuroimaging ( e.g. , edema , breakdown of the blood - brain barrier [ bbbb ] ) was evaluated . 
the assessment of bbbb was performed by the detection of hyperintense signals in the avm region on contrast - enhanced t1 - weighted images in comparison to the nonenhanced sequences . 
both changes occur as hyperintensities on t2 and flair , and the differentiation may be difficult in some cases [ 5 ]  . mri is one method which is recommended for the analysis of side effects with the lent / soma criteria [ 15 ] , since it very sensitively allows the detection and characterization of radiation - related morphological changes . 
the lent / soma scale for mri , however , provides only a coarse measure of normal brain tissue changes , with grade 0 indicating no morphological changes at all and grade ii already implicating cerebral necrosis . 
therefore , to further quantify the normal tissue reactions , a descriptive way was chosen to categorize the tissue changes according to their extent , differentiating between no reaction , small perifocal , intermediate perifocal and figure 1a abbildung 1a figure 1b abbildung 1b figures 1a and 1b . 
pretreatment ( left panel ) and postradiosurgery ( right panel ) t2 - weighted mri scans of two avm patients showing radiation - induced edema of different extent , classified as small ( a ) , and large ( b ) , respectively . 
pr ( links ) und posttherapeutische ( rechts ) t2 - gewichtete mr - schnittbilder von zwei avm - patienten mit strahleninduzierten demen unterschiedlicher ausdehnung , welche als klein ( a ) bzw . 
the definition of clinically relevant and reproducible endpoints is a crucial step in the quantitative analysis of dose / volume - effect relationships of adverse effects following radiotherapy of the brato ensure a consistent scoring and classification of radiation effects throughout the analysis , two mr - experienced physicians ( me , hh ) together reviewed the pretreatment and follow - up imaging studies for all patients included in the analysis . 
any possible bias or subjective element in the scoring process was thereby reduced to a minimuexamples of postradiosurgery edema and bbbb with different extent are shown in figures 1 and 2 , respectively . 
 predictors of radiation - induced brain tissue changes , such as the total volume of tissue ( including the avm target ) receiving a dose of at least 12 gy [ 79 ] or 10 gy [ 20 ] ( v12 and v10 , respectively ) , or the mean dose in a specified volume of 20 cm3 that was given the highest dose ( dmean20 ) [ 13 , 14 ]  . in a previous analysis , we compared these different parameters , all derived from the dose - volume histogram of the brain of each individual patient , with respect to their ability to predict radiation - induced brain tissue changes [ 16 ]  . 
we found that radiation - induced changes of brain tissue assessed through posttreatment neuroimaging are equally well predicted by the dose distribution variables v12 ( or v10 ) and figure 2a abbildung 2a data sample a total of 108 avm patients had stereotactic linac - based radiosurgery using a micro - multileaf collimator between 1993 and 1998 . 
excluded from this analysis were all patients treated for multiple avms , those who received reirradiation , and all patients with incomplete pretreatment or follow - up clinical or neuroimaging information . 
to ensure a consistent scoring of both endpoints edema and bbbb for every patient , we also excluded all patients without contrast - enhanced t1 - weighted mri either before treatment or during follow - up . 
 a total of 73 patients with full pretreatment and follow - up neuroimaging were included in the analysis . a median dose of 19 gy ( mean value : 18.6 gy , range : 13.322 gy ) was prescribed to the 80% isodose ( minimum dose to the target ) which completely encompassed the target volume . 
details about the patient characteristics can be found in a previous publication [ 16 ]  . fitting of dose / volume - response curves radiation - induced changes of normal brain tissue after avm radiosurgery have been reported in the literature to depend on dose and irradiated volume . 
pr ( links ) und posttherapeutische ( rechts ) kontrastmittelverstrkte t1 - gewichtete mr - schnittbilder von zwei avm - patienten mit strahleninduzierten strungen der blut - hirn - schranke unterschiedlicher ausdehnung , welche als klein ( a ) bzw . 
in this study , we will derive two alternative sets of dose / volume - response relations , one based on v12 , and one based on dmean20 . to quantify dose / volume - response relations , patients were ranked according to the value of the dose / volume variable dv ( i.e. , v12 or dmean20 ) and classified into four groups of equal size ( quartile )  . 
for each group , the actuarial rates ( with corresponding standard errors ) of developing the considered endpoints within 2.5 years after radiosurgery were determined from kaplan - meier estimates [ 12 ]  . 
the dose - response curves were fitted with a simple phenomenological ntcp model based on dv ( i.e. , v12 and dmean20 ) to assess the dose / volume - response of avm patients . 
parameter k characterizes the slope of the dose / volume - response curve . we fitted separate dose / volume - response curves for all combinations of endpoints ( i.e. , edema , bbbb , combined endpoint edema and / or bbbb ) and categories characterizing the extent of the image change ( i.e. , small , intermediate , and large )  . 
a commercial statistics software package was used to perform the curve fit ( s - plus 2000 professional , mathsoft inc . , seattle , wa , usa )  . goodness of fit for the different models was assessed by performing ( cid : 1 ) 2 - tests for grouped patient data . 
we then determined agreement between predicted and observed actuarial rates at 2.5 years after radiosurgery in each group by calculating a ( cid : 1 ) 2 - statistics ( defined as the sum of the squares of the differences between the observed and the predicted p2.5y ( dv ) in each group , weighted with the inverse of the squared standard errors on the actuarial rates )  . 
cumulative incidence of radiation - induced changes of brain tissue ( edema and / or breakdown of the blood - brain barrier [ bbbb ] ) as function of follow - up time after avm radiosurgery . 
figure 3 shows the relative cumulative incidence of small , intermediate , and large tissue changes ( edema and / or bbbb ) as function of follow - up time . 
characteristics dv50 and k of the dose / volume - response curves relating the actuarial rate of observing each endpoint within 2.5 years after radiosurgery to the dose distribution variables v12 and dmean20 are given along with the ( cid : 1 ) 2 - statistics of each fit . 
dose / volume - response relations were observed for variables v12 and dmean20 for all evaluated endpoints except for bbbb with intermediate and large extent , for which the fits of the logistic function based on v12 did not converge . 
dose / volume - response curves based on v12 and dmean20 fitted the data equally well , and neither of the two variables could be favored over the other in describing the observed response relations . 
 fitted dose / volume - response curves based on v12 for the endpoints small , intermediate , and large edema , small bbbb , as well as for the combined endpoint edema and / or bbbb with small , intermediate , and large extent are shown in figures 4a to 4c , respectively . 
 for all endpoints , a clear shift of the dose / volume - response curves toward higher values of the dose distribution variable ( i.e. , v12 or dmean20 ) was observed going from tissue changes with small extent to those with large extent . 
the mean dose in 20 cm3 , dmean20 , corresponding to a 50% actuarial rate of the combined endpoint edema and / or bbbb was by 10 gy higher for tissue changes with large extent compared to small extent ( see table 3 )  . discussion we fitted a phenomenological ntcp model using a sigmoid - shape logistic function to the radiologically observed actuarial rate of radiation - induced changes of brain tissue ( i.e. , edema , bbbb , edema and / or bbbb ) after radiosurgery of avm patients . 
alternative sets of dose / volume - response relations were derived , based on two variables characterizing the 3 - d dose distribution in the brain , v12 and dmean20 . 
 these variables represent different approaches to reduce the full 3 - d dose distribution in the brain to a single number , which is a function of both dose and volume . 
a previous analysis of our avm data sample demonstrated that these two dose / volume variables are correlated with the investigated endpoints and hence suited to quantify dose / volume - response relations [ 16 ]  . 
dose / volume - response relations for changes of brain tissue after avm radiosurgery endpoint : edema endpoint : bbbb small large intermediate figure 4a abbildung 4a figure 4b abbildung 4b v12 ( cm3 ) endpoint : edema and / or bbbb small large intermediate v12 ( cm3 ) figures 4a to 4c . 
 observed actuarial rates of developing radiation - induced changes of brain tissue with small , intermediate , and large extent within 2.5 years after radiosurgery are shown by closed squares , open triangles , and closed circles , respectively . 
die klinisch beobachteten aktuarischen hufigkeiten strahleninduzierter normalgewebevernderungen mit geringer , mittlerer und groer ausdehnung innerhalb von 2 , 5 jahren nach strahlenchirurgie sind als schwarze quadrate , offene dreiecke bzw . 
 small large intermediate figure 4c abbildung 4c v12 ( cm3 ) v12 and dmean20 fitted our data equally well , and neither of the two variables could be favored clearly over the other in describing the observed response relations . 
there is a slight preference , however , toward the use of dmean20 , because this variable allowed quantifying dose / volume relations for the endpoints of intermediate and large bbbb , in contrast to v12 . 
except for bbbb with intermediate and large extent and variable v12 , dose / volume - response relations were observed for every other combination of endpoint and dose / volume variable . 
a 50% actuarial rate of observing the combined endpoint edema and / or bbbb within 2.5 years is caused by v12 values of 4 and 22 cm3 for small and large tissue changes , respectively , differing by as much as 18 cm3 . 
dose / volume - response relations for changes of brain tissue after avm radiosurgery endpoint : edema endpoint : bbbb small large intermediate small large intermediate figure 5a abbildung 5a figure 5b abbildung 5b dmean20 ( gy ) dmean20 ( gy ) endpoint : edema and / or bbbb small large intermediate figures 5a to 5c . 
 observed actuarial rates of developing radiation - induced changes of brain tissue with small , intermediate , and large extent within 2.5 years after radiosurgery are shown by closed squares , open triangles , and closed circles , respectively . 
die klinisch beobachteten aktuarischen hufigkeiten strahleninduzierter normalgewebevernderungen mit geringer , mittlerer und groer ausdehnung innerhalb von 2 , 5 jahren nach strahlenchirurgie sind als schwarze quadrate , offene dreiecke bzw . 
 figure 5c abbildung 5c dmean20 ( gy ) the parametrizations of dose / volume - response curves that we provide ( equation 1 with parameters dv50 and k taken from tables 2 and 3 ) allow the calculation of any point on the response curve . 
in addition to dv50 , which we have chosen to quote throughout the paper , for instance dv10 , the value of the dose / volume variable corresponding to an actuarial rate of 10% for observing the respective endpoint within 2.5 years after radiosurgery , or any other point of clinical interest can be easily derived . dose / volume - response curves after radiosurgery of avm patients have been previously reported in the literature . 
they analyzed the endpoints of all imaging changes and symptomatic imaging changes [ 9 ] , symptomatic imaging changes as function of the avm location [ 8 ] , as well as permanent symptomatic imaging changes as function of location [ 7 ]  . 
dose / volume - response relations for changes of brain tissue after avm radiosurgery sponse curve for edema with intermediate extent , suggesting that their analysis may not have included tissue changes with small extent . 
 lax & karlsson evaluated the endpoint of new or aggravated neurologic symptoms or signs together with radiologic evidence of tissue changes following gamma knife radiosurgery of avm patients at karolinska hospital , stockholm , sweden . 
they have fitted an ntcp model ( a relative seriality model with a combined serial - parallel functional architecture ) using dmean20 as independent variable to the data [ 14 ]  . 
separate dose / volume - response curves were derived differentiating central versus peripheral location of the avm and the impact of previous hemorrhage on the development of symptomatic imaging changes [ 13 ]  . 
 the direct quantitative comparison of these previously determined dose / volume - response relations [ 79 , 13 , 14 ] with our parametrizations of late radiation effects in the brain after avm radiosurgery , however , is difficult . 
for future studies of volume effects in the brain , the definition of reliable and reproducible endpoints and the precise reporting of the applied scoring criteria are of utmost importance . 
 it is important to note that the parametrizations of dose / volume - response curves that we provide should only be applied to assess radiation - induced tissue changes after avm radiosurgery for radiologic endpoints . 
in this case , it might not be useful to avoid this response by applying strict dose / volume constraints in the treatment planning of avm patients , especially in light of the fact that the majority of brain tissue changes are temporary and often entirely asymptomatic . 
 conclusion dose / volume - response relations were derived that allow to quantitatively assess the risk of radiation - induced changes of brain tissue after avm radiosurgery from each patients dose distribution in the brahowever , further understanding of the mechanism leading to brain tissue changes and their correlation with the desired obliteration is required before one can decide which dose / volume constraints should be applied in clinical practice of avm radiosurgery . 
studies of this nature will eventually help to quantitatively assess the tolerance of the brain to partial irradiation . strahlentherapie und onkologie original article response of rat prostate and lung tumors to ionizing radiation combined with the angiogenesis inhibitor amca henk b . 
voest2 aim : to determine whether radiation combined with trans - 4 - aminomethyl cyclohexane carboxylic acid ( amca , or tranexamic acid , cyklokapron ) results in a better tumor response than radiation alone . 
 materials and methods : we evaluated the responses of the l44 lung tumor in bn rats and r3327 - matlylu ( mll ) prostate tumor in copenhagen rats , to single and fractionated x - ray doses with and without amca ( 1.5 g / kg )  . 
 conclusion : the enhancement ratio of 1.41.7 for the l44 tumor , but not for the mll tumor , due to amca treatment , indicates that amca may potentiate the anti - tumor effect of ionizing radiation in distinct tumor types . 
 key words : angiogenesis tranexamic acid growth delay rat tumors strahlenther onkol 2004 ; 180 : 798804 doi 10.1007 / s00066 - 004 - 1276 - 4 ansprechen von prostataund lungentumoren der ratte auf ionisierende strahlung kombiniert mit dem angiogeneseinhibitor amca ziel : untersuchung , ob strahlung kombiniert mit trans - 4 - aminomethyl - cyclohexancarbonsure ( amca oder tranexamsure , cyklokapron ) zu einem besseren tumoransprechen fhrt als strahlung alle material und methodik : wir berprften das ansprechen des l44 - lungentumors bei bn - ratten und des r3327 - matlylu - ( mll - ) prostatatumors bei kopenhagen - ratten auf einzelund fraktionierte rntgenstrahlendosen mit und ohne amca ( 1 , 5 g / kg )  . 
l44 - tumoren , die 4 tage lang fraktionierte strahlungsdosen von 2 , 5 gy erhielten , reagierten mit einer signifikanten relativen und spezifischen wachstumsverzgerung , wenn sie mit amca behandelt wurden ; der verstrkungsfaktor lag bei 1 , 61 , 7 . 
 schlussfolgerung : der verstrkungsfaktor von 1 , 41 , 7 des l44 - tumors , jedoch nicht des mll - tumors , infolge der amca - gabe , spricht dafr , dass amca bei bestimmten tumoren den antiproliferativen effekt ionisierender strahlung potenzieren kann . 
 schlsselwrter : angiogenese tranexamsure wachstumsverzgerung tumoren der ratte 1 department of radiotherapy , university medical centre utrecht , the netherlands , 2 department of medical oncology , university medical centre utrecht , the netherlands , 3 department of radiotherapy , medical centre haaglanden , westeinde hospital , the hague , the netherlands . 
response of two rat tumors to radiation combined with amca introduction an abundance of preclinical models has demonstrated the dependency of tumor growth on the formation of a new vascular network . 
based on these findings inhibition of angiogenesis is considered to be one of the most promising novel strategies in the treatment of cancer [ 8 , 14 , 40 , 47 ]  . 
current research with antiangiogenics investigates whether these agents can be combined with conventional treatment modalities such as chemotherapy and radiation therapy . several angiogenesis inhibitors when administered with ionizing radiation , potentiated the effects of radiation therapy [ 16 , 18 , 20 , 36 , 41 ]  . 
administration of the angiogenesis inhibitor angiostatin after radiotherapy of the primary tumor prevented outgrowth of metastases [ 7 ]  . trans - 4 - aminomethyl cyclohexane carboxylic acid ( amca , also tranexamic acid , cyklokapron ) is a lysine analogue that blocks the interaction between lysine residues and the lysine binding sites that are present in the kringle domains of plasminogen . 
several preclinical as well as clinical studies have reported promising effects of this drug on endothelial cell invasion , angiogenesis , tumor growth and metastasis [ 1 , 3 , 5 , 6 , 11 , 28 , 29 , 32 , 43 , 44 ]  . 
 tumor volume was based on two orthogonal cross - sectional diameter measurements ( v = 0.5a2b with a the smallest diameter )  . radiation treatment x - ray doses ( 200 kv , 20 ma , 0.5 mm cu , dose rate 4 gy / min ) ( philips orthovolt rt250 ) were administered locally under hypnorm / dormicum anaesthesia . 
excess growth delay , egd , for a treated tumor is t4t minus the time interval for control tumors ( with the same volume as the pretreatment volume of the treated tumor ) to reach four times that volume ( t4 ) : egd = t4t - t4 . 
kaplan - meier analysis was performed by scoring egd or sgd as events and with which the means , standard deviations and 95% confidence limits were calculated . the l44 is a radiation - induced anaplastic tumor , originally diagnosed as an adenosquamous lung carcinoma , and grows in the brown norway rat ( bn ( orl ) ico , charles river , maastricht , the netherlands ) with a tumor volume doubling time of about 4 days [ 2527 ]  . 
the r3327 - matlylu prostate tumor ( mll ) in male copenhagen rats ( cop / hsd , harlan world head quarters , indianapolis , indiana , usa ) is a fast growing , androgen insensitive , anaplastic tumor and highly metastatic to lymph nodes and lungs [ 22 ] with a tumor volume doubling time of about 2 days . 
response of two rat tumors to radiation combined with amca approval the animal experiments ethical committee of the university medical center utrecht approved the animal experiments . results treatment with amca only amca was well tolerated : bn rats experienced a slight growth retardation as compared to control rats ; copenhagen rats had a 6% body weight loss at the end of the period in which amca was applied . 
l44 tumors ( n = 15 ) treated with 4 daily dose fractions of 2.5 gy had a mean excess growth delay egd of 6.5 days , and tumors treated with the same fractionation scheme and amca had a mean egd of 11.1 days ( table 1 )  . 
in figure 1a examples of growth curves of a control tumor and those of tumors treated with 4 fractions of 2.5 gy alone and 4 fractions of 2.5 gy combined with amca are shown . 
 after the dose of 20 gy the tumor volume hardly increased in size in the 10 days post treatment ; thereafter tumor voltime after start of treatment ( d ) time after start of treatment ( d ) figure 1a abbildung 1a figure 1b abbildung 1b figures 1a and 1b . 
dreiecke : kontrolltumor ; quadrate : 4 tage fraktionierte strahlungsdosen von 2 , 5 gy ; rauten : 4 tage fraktionierte strahlungsdosen von 2 , 5 gy kombiniert mit amca . 
 enhancement ratio er the mean egd values for the l44 tumors derived from the three experiments in which 4 2.5 gy amca was administered were 6.5 days ( 4 2.5 gy ) and 11.1 days ( 4 2.5 gy + amca )  . 
 [ 36 ] described that angiostatin , a fragment of plasminogen and potent inhibitor of angiogenesis , combined with radiation showed anti - tumor interaction in four distinct tumor types . 
the egd and sgd values observed in earlier and the present experiments were plotted as a function of bed ( figures 2a , 2b , 3a , 3b , and table 2 )  . 
the dose - response curves tend to be straightened ( as compared to the dose - response curve of egd versus single doses for the l44 tumor e.g. ) and a linear regression was applied . 
the er observed for the l44 tumor is comparable with those found for several cytostatics such as gemcitabine [ 35 , 38 , 42 ] , cisplatin [ 24 ] , the camptothecin analogue rfs - 2000 [ 2 ] , 5 - fluorouracil [ 33 ] and two taxane analogues [ 31 ]  . 
 however , for the mll tumor , the er was not significantly different from 1 , hence no potentiation was observed in conthe two tumor types l44 and mll show large differences in responsiveness to radiation and amca . 
for example , the sgd at a biologically effective dose ( bed ) of 50 gy is 6.5 for the l44 tumor ( figure 2b ) , it is 2.0 for the mll tumor ( figure 3b )  . 
 [ 19 ] demonstrated that amongst the five dunning prostatic tumor lines the mll tumor showed a high vessel density and a high tissue vascular endothelial growth factor ( vegf ) level . 
however , the concave upward dose - response curve of egd versus single doses for the l44 tumor as can be made from the single - dose data presented in table 2 indicates a moderate hypoxic fraction . 
it is also known that hypoxic conditions create a microenvironment in which tumor cells become less angiogenesis - dependent , more apoptosis - resistant and more malignant because of the development of genomic instability and mutant genotypes impacting on apoptosis / survival signalling pathways . 
 conclusion the enhancement ratio of 1.41.7 for the l44 tumor , but not for the mll tumor , observed for the combined treatment irradiation and amca versus irradiation alone , indicates that amca may potentiate the anti - tumor effect of ionizing radiation in distinct tumor types . 
brunner1 , dieter schwab2 , thomas meyer3 , rolf sauer1 purpose : this study compared stenting and chemoradiation ( crt ) and attempted to identify factors that are predictive of response to crt . material and methods : a retrospective analysis identified 98 patients treated . 
two patients ( 2 / 25 ) with unresectable tumors at diagnosis had pathohistological complete response at resection after crt . conclusion : inclusion criteria for future crt trials should be based on tumor size at diagnosis : patients otherwise eligible for crt should only be included with an inoperable tumor 40 mm , while patients with larger tumors may only benefit from palliation by stenting . key words : cholangiocarcinoma chemoradiation stenting strahlenther onkol 2004 ; 180 : 7517 doi 10.1007 / s00066 - 004 - 1315 - 1 radiochemotherapie kann die berlebenszeit von patienten mit irresektablen extrahepatischen biliren karzinomen ohne tumorbulk verlngern . 
 die toxizittskriterien der rtog / nci - ctc wurden angewendet . ergebnisse : die mediane berlebenszeit fr alle patienten betrug 11 , 8 monate , 9 , 3 monate fr patienten mit alleinigem stenting und 16 , 5 monate mit radiochemotherapie ( p = 0 , 22 )  . 
zwei patienten ( 2 / 25 ) mit irresektablen tumoren zum diagnosezeitpunkt hatten eine pathologisch gesicherte komplette remission zum zeitpunkt der resektion nach radiochemotherapie . schlussfolgerung : die einschlusskriterien fr zuknftige studien sollten die tumorgre zum diagnosezeitpunkt bercksichtigen : patienten , die alle einschlusskriterien fr eine radiochemotherapie erfllen , sollten diese nur dann erhalten , wenn die tumorgre 40 mm nicht berschreitet , wohingegen patienten mit greren tumoren von alleinigem palliativen stenting zu profitieren scheinen . 
 schlsselwrter : cholangiokarzinom radiochemotherapy stenting 1 department of radiation oncology , friedrich - alexander university of erlangen - nuremberg , erlangen , germany , 2 department of gastroenterology and hepatology , friedrich - alexander university of erlangen - nuremberg , erlangen , germany , 3 department of abdominal surgery , friedrich - alexander university of erlangen - nuremberg , erlangen , germany . received : may 5 , 2004 ; accepted : september 30 , 2004 strahlenther onkol 2004 no . 
patients with btc have a poor prognosis with median survival time ( st ) between 624 months and 5 - year overall survival ( os ) rates of 1525% [ 7 ]  . 
complete resection remains the only therapy that offers the possibility of long - term survival , but most patients present with unresectable disease ( about 90% ) and more than half of the resected patients relapse within 1 year [ 9 , 13 , 23 ]  . 
radiotherapy ( rt ) alone , including external - beam rt ( ebrt ) and intraluminal brachytherapy ( ibt ) [ 28 ] , may relieve symptoms and contribute to biliary decompression but do not substantially increase survival rates in unresectable disease ( reviewed in [ 12 ] )  . 
5 - fluorouracil - ( 5 - fu - ) based chemoradiation ( crt ) has been performed in the adjuvant [ 14 , 29 , 30 ] definitive setting [ 1 , 6 , 9 , 23 ] for patients with btc , and improved survival has been reported . it is controversial whether chemotherapy alone is able to improve survival . 
 the only randomized trial tested a combination of 5 - fu , leucovorin and etoposide versus best supportive care and was not able to produce a significant prolongation of os [ 11 ]  . 
 accumulating data from recent phase ii trials suggest that single - agent gemcitabine represents an active and very well tolerated treatment option in btc ( reviewed in [ 27 ] )  . 
preclinical studies have shown that gemcitabine is a potent radiosensitizer [ 19 , 20 , 33 ] and that there is a synergistic interaction between gemcitabine and cisplatin [ 31 ]  . 
while we are far from understanding potential biological prognostic factors like hypoxia known to play a role in other tumors when crt is given [ 22 , 26 ] , our study contributes to the data favoring crt for btc . 
 material and methods study population and eligibility the hospital records of 98 patients with the diagnosis of unresectable biliary cancer referred to this university hospital between january 1994 and june 2001 were reviewed ( figure 1 )  . 
patients with gallbladder carcinoma were excluded from the control group , because stenting was often required only later during their course of disease progression precluding comparison of survival with patients who had crt ( figure 1 )  . 
stage was classified according to the uicc 1997 and had the following stage distribution : stage ii : four patients , stage iii : twelve patients , stage iva : twelve patients , stage ivb ( nonregional enlarged lymphatics ) : seven patients . 
unresectability was defined as ( 1 ) recurrent local disease ; ( 2 ) involvement of the tumor with the main portal vein ; ( 3 ) involvement of the secondary biliary radicals ; ( 4 ) invasion into adjacent liver tissue not permitting partial hepatectomy . 
initial laboratory requirements included white blood cell ( wbc ) count referred to university hospital n = 98 eligible for crt n = 27 n = 2 mhep . only cx n = 25 other primary n = 7 other therapy study group n = 25 study group palliative stenting n = 20 bile duct carcinoma n = 5 gall bladder carcinoma figure 1 . 
 characteristics chemoradiation stenting total number gender ( male / female ) age ( years ) median follow - up ( months ) tumor location klatskin ( bismuth stage i / ii / iii / iv / xa ) proximal / middle third distal third gallbladder recurrent after clear resectionb relapse after positive marginsc 16 / 9 median 60 ( range 3476 ) ( 1 / 0 / 5 / 6 / 1 ) 5 2 5 4 2 a x : stage not available b klatskin : n = 1 , distal third of choledochus : n = 1 , gallbladder : n = 2 c proximal third of choledochus : n = 1 , distal third of choledochus : n = 1 17 / 22 median 74 ( 4585 ) ( 2 / 3 / 6 / 12 / 14 ) starting in 1997 , 14 patients received concurrent crt containing gemcitabine ( iv 300 mg / m2 ) and cisplatin ( iv 30 mg / m2 ) as a pilot study both on days 1 , 8 , 22 , and 29 of rt [ 5 , 34 ]  . 
three - dimensional ( 3 - d ) conformal ebrt to the tumor region and the lymphatics was given with single doses of 1.8 gy / d up to a total dose of 4550.4 gy ( 10 - mev photons ) as previously described for pancreatic tumors [ 4 ]  . 
the total dose to the planning target volume ( ptv ) depended on the calculated normal tissue toxicity for the liver which was not allowed to receive > 30 gy to 30% of the total volume of the organ . 
the clinical target volume ( ctv ) of radiation included the primary tumor , regional lymph nodes in the hepatoduodenal ligament , porta hepatis and celiac axis with a 1.5 - cm margin ( figure 2 )  . 
based on a computed tomography ( ct ) scan matched with magnetic resonance imaging ( mri ) , cholangiography and ultrasound findings , 3 - d treatment planning with consecutive conformal rt using a multileaf collimator ( kd2 , siemens ) was performed . 
a remote afterloading system ( hdr microselector , nucletron b.v. , the netherlands ) with a high - dose - rate ( hdr ) iridium - 192 ( 192ir ) source was used and the source transfer tube was placed in a 12 - f catheter . 
 chemotherapy in ten patients concurrent chemotherapy consisted of 5 - fu ( iv 1 g / m2 / 24 h for 120 h ; days 15 and days 2933 of rt ) and mitomycin c ( rapid iv infusion , 10 mg / m2 ; day 1 and day 29 ) similar to a schedule we reported earlier for pancreatic carcinoma [ 4 ]  . 
transverse ct scan views with ptv delineations ( blue contour ) for the tumor and the regional lymphatics using a 1.5 - cm margin around the clinical target volume ( four - field approach )  . 
planungszielvolumen ( ptv ) fr ein hilres gallenwegskarzinotransversale ct - bilder mit angabe des ptv fr den tumor und die regionren lymphabflussgebiete mit einem 1 , 5 - cm - sicherheitssaum um das klinische zielvolumen ( blaue kontur ; vierfeldertechnik )  . 
for reasons of homogeneity , survival analysis for the six patients with recurrent tumor after surgery was calculated from the diagnosis of relapse and not from primary diagnosis on in the crt group . 
survival was calculated according to the kaplan - meier method from the time of diagnosis and from the time of treatment ( crt ) initiation to avoid a bias by patients treated for recurrent carcinoma . 
the differences between the survival curves were tested with the log - rank test . results patients selection of the therapy in the 25 patients treated with crt , a median dose of 45.0 gy ( range 30.454.0 gy ) was delivered to the ctv . 
 survival and prognostic factors at the time of this analysis ( december 2003 ) , 11 / 39 patients with stenting and 6 / 25 patients with crt are alive . 
if the survival calculation was performed using date of initial diagnosis , the median st for patients with crt was 22.7 months ( range 5.659 months ) and median st for stenting alone was 9.3 months as indicated above ( p = 0.058 ; figure 3a )  . 
 resection after chemoradiation tumor characteristics were not as detailed for patients of the control group as for the crt group , because imaging was not an absolute requirement for stenting . 
one of them had primary sclerosing cholangitis and a hilar cholangiocarcinoma with a diameter of 3.7 cm , a 2.5 - cm paraaortic lymph node metastasis and an associated portal vein thrombosis at the time of presentation . 
 this patient was not unresectable because of tumor size but crt was started because of the risk of intraoperative tumor cell spill and because of the presence of peripancreatic lymph nodes on ct scan . 
grade 3 nausea and toxicity were infrequent with two patients in each group of chemotherapy ( two patients : 5 - fu / mitomycin ; two patients : gemcitabine / cisplatin )  . 
the most severe nonhematologic dose - limiting toxicity ( dlt ) observed was a mallory - weiss rupture at 43.2 gy in one patient with concurrent 5 - fu / mitomycin c . 
patienten mit einem maximalen tumordurchmesser 4 cm ( durchgezogene linie ) wurden solchen mit einem durchmesser > 4 cm ( unterbrochene linie ; p = 0 , 01 ) gegenbergestellt . 
since a complete course of crt takes about 6 weeks including a minimum of 2 weeks of hospitalization in our experience , an outpatient - based therapeutic option like systematic chemotherapy or palliative stenting is preferable . 
similarly , tumor size was the only independent prognostic factor at multivariate analysis in a study of patients with inoperable malignant distal biliary strictures treated by palliative stenting alone [ 25 ]  . 
median st for patients with crt was 16.5 months in our study , though patient characteristics were unfavorable compared to other reports on crt in unresectable btc : nodal metastasis and grading were highest in this study compared to the literature [ 1 , 6 , 9 , 23 ]  . 
the reasons for good survival results in our study are most likely due to the treatment characteristics : ( 1 ) high total radiation dose is important in the light of the description of a dose - response relationship [ 1 ] ; ( 2 ) continuous - infusion ( civ ) 5 - fu is considered to be superior to bolus [ 24 ] , and combined mitomycin c has previously been described in a study with prolonged survival [ 21 ]  . 
reported a high median st of 21.2 months for unresectable biliary carcinoma ( 5 - fu at 1 , 000 mg / m2 / day civ over 96 h on days 14 ) in patients with less advanced stage than our study [ 23 ]  . 
taken together , retrospective , nonrandomized data suggest a prolongation of survival after crt compared to stenting alone or rt alone . the high frequency of cholangitis in patients with percutaneous stenting in our experience is both a serious complication and a problem for administration of chemotherapy . 
 of note , in pancreatic cancer a reciprocal correlation between the size of the target volume and the maximum tolerated dose ( mtd ) was described [ 5 , 6 , 34 ]  . 
intensity - modulated rt ( imrt ) techniques as recently reported for gastric carcinoma where the same organs at risk are dose - limiting for radiation [ 18 ] could be another step to improve therapeutic outcomes for btc . 
the addition of mucosa - protecting agents should also be considered [ 16 ]  . conclusion crt can safely be administered using recently established gemcitabineand cisplatin - based schedules for pancreatic carcinoma . 
crt in bile tract cancer strahlentherapie und onkologie original article radiation response in vitro of fibroblasts from a fanconi anemia patient with marked clinical radiosensitivity cholpon djuzenova1 , michael flentje1 , pierce nicholas plowman2 background : fanconi anemia ( fa ) is an autosomal recessive chromosome instability disorder characterized by progressive pancytopenia and cancer susceptibility . 
by contrast , her in vitro irradiated skin fibroblasts revealed nearly normal radiosensitivity as determined by the colony survival assay . material and methods : in view of this discrepancy , the radiation response of this particular fa fibroblast strain ( designated 425br ) was further analyzed in the present study by means of the alkaline single - cell gel electrophoresis ( comet ) assay , and also by the cytochalasin - blocked micronuclei ( mn ) test . 
in addition , the expression levels of dna repair proteins , hmre11 , rad50 , and rad51 , were investigated using western blot and foci immunofluorescence staining . results : the comet assay revealed that the initial dna fragmentation in irradiated fa cells was two times higher and the dna rejoining process was three times slower than that in control ( 1br3 ) fibroblasts . 
moreover , although the baseline level of mns was lower in fa cells than in controls , the fa fibroblasts were more prone ( about two times ) to mn production than control cells when irradiated with 24 gy . 
western blot analysis of the dna repair proteins ( hmre11 , rad50 , and rad51 ) did not reveal any abnormalities in protein expression levels or their migration patterns in the fibroblasts derived from an fa patient either before or after irradiation . 
at the same time , in vitro irradiated cells from the fa patient exhibited a significantly reduced number of nuclei with focally concentrated dna repair rad51 protein than in control cells . conclusion : the increased dna damage and mn induction in irradiated fa fibroblasts , and the reduction of the formation of dna repair foci containing rad51 suggest a possible link to the profound clinical radiosensitivity reported earlier for this fa patient . 
 the findings on this particular fa cell strain presented in the study point toward the difficulties involved in the prediction of the radiation response of cell lines and tumors based solely on the colony survival test . key words : comet assay dna damage dna repair fanconi anemia micronuclei x irradiation strahlenther onkol 2004 ; 180 : 78997 doi 10.1007 / s00066 - 004 - 1250 - 1 in - vitro - strahlensensibilitt der fibroblasten bei einem patienten mit fanconi - anmie mit auergewhnlicher klinischer strahlenreaktion hintergrund : die seltene , autosomal - rezessive fanconi - anmie ( fa ) ist durch progressives knochenmarkversagen und ein erhhtes krebsrisiko gekennzeichnet . 
 ( 2001 ) ber einen fall mit auergewhnlicher klinischer radiosensibilitt bei einer fa - patientin mit tonsillenkarzinogleichzeitig wiesen ihre in vitro bestrahlten hautfibroblasten eine fast normale strahlenempfindlichkeit auf , wie durch den koloniebildungsassay festgestellt . 
 material and methodik : aufgrund dieser diskrepanz wurde die strahlenempfindlichkeit dieser fa - fibroblastenlinie in der vorliegenden untersuchung mit der alkalischen einzelzell - gelelektrophorese ( comet - assay ) sowie dem cytochalasinblockierten mikrokerntest weiter analysiert . 
gleichzeitig war die induktion der mikrokerne in den fa - zellen um den faktor 2 hher als in kontrolllinien nach einer in - vitro - bestrahlung mit 24 gy rntgenstrahlen . 
mittels western - blot konnte gezeigt werden , dass die kontrollund 1 department of radiotherapy , university of wrzburg , wrzburg , germany 2 radiotherapy / clinical oncology , st . 
demgegenber zeigten bestrahlte zellen der fa - patientin eine gegenber den kontrollzellen verringerte anzahl von rad51 - foci - haltigen kernen . schlussfolgerung : die erhhte in - vitro - strahlenempfindlichkeit der hautfibroblasten , die hier durch den comet - assay , den mikrokerntest und die rad51 - immunfluoreszenz nachgewiesen wurde , kann mit den frher bei dieser fa - patientin berichteten starken klinischen strahlennebenwirkungen korrelieren . 
die dargestellten daten weisen auch auf die schwierigkeiten hin , die mit der vorhersage der strahlenempfindlichkeit des normalgewebes und der tumoren verbunden sind , wenn sie nur auf dem koloniebildungsassays basiert . 
 schlsselwrter : comet - assay dna - schaden dna - reparatur fanconi - anmie mikrokerne rntgenstrahlung introduction fanconi anemia ( fa ) is a genomic instability disorder characterized by developmental abnormalities and progressive bone marrow failure [ 9 ]  . 
 the hallmark of the fa cellular phenotype is a high level of spontaneous chromosomal breakage [ 44 ] , which can be increased by exposure of these cells to dna cross - linking agents , such as mitomycin c and diepoxybutane . 
irradiated fa fibroblasts were found ( with one exception [ 4 ] ) to exhibit the same colony - forming ability as irradiated normal cells [ 19 , 22 , 23 , 31 , 50 ]  . 
 [ 52 ] demonstrates a ninefold decrease in the repair of restriction enzyme - induced dna double - strand breaks ( dsbs ) by homologous recombination in fancg mutant cells , as well as elevated chromosomal aberrations at 3 - h intervals after radiation exposure . 
bone marrow grafting of patients with fa is characterized by uncommonly severe complications [ 47 ] , e.g. , cardiac failure , hemorrhagic cystitis , mucositis , an early skin rash , esophagitis , etc . 
 recently , a 32 - year - old female fa patient with tonsillar squamous cell carcinoma , treated by radiotherapy ( discontinued after 34 gy ) , was found to exhibit severe clinical radiosensitivity with profound mucositis , deep necrotic ulcer in the tonsil , septicemia , etc . 
however , the striking clinical radiotoxicity contrasts with the nearly normal response of her in vitro irradiated skin fibroblasts ( strain 425br ) , as assessed by the colony - forming assay [ 31 ]  . 
the apparent discrepancy between clinical and in vitro findings encouraged the present study of the radiation response of this fa fibroblast strain using the following experimental techniques : the alkaline single - cell gel electrophoresis ( comet ) assay , western blot and foci immunofluorescence analysis of the expression of dna repair proteins , and also the cytochalasin - blocked micronuclei ( mn ) test . 
 the dna dsbs are proposed to be the principal lesions for radiogenic cell killing [ 27 , 48 ] for which multiple repair pathways in mammalian cells exist [ 29 ]  . 
unfortunately , the relative yield of dsbs is low , and high radiation doses need to be applicated to produce measurable levels of dsbs , and these doses are far greater than those used clinically . 
by contrast , the yield of radiation - induced single - strand breaks ( ssbs ) is far greater [ 48 ] , and they can be readily measured at much lower clinically relevant doses of radiation . 
furthermore , the mechanisms that are proposed to vary the yield of radiation - induced dsb formation are also expected to vary the yield of radiation - induced ssbs [ 49 ]  . 
consequently , the extent of radiation - induced ssb formation measured by the alkaline comet assay can be considered a valid surrogate marker of radiogenic dsb formation [ 32 ]  . 
the comet assay is widely regarded as a fast and informative method for the measurement of dna strand breaks at the single - cell level immediately after dna damage [ 45 ] and also the restoration of high molecular dna as a function of time after treatment [ 37 ]  . 
the comet assay is also useful for the prediction of dna repair in cancer patients [ 2 , 38 ] , prenatal diagnosis of xeroderma pigmentosum and trichothiodystrophy [ 1 ] , and for the discrimination of carriers of fa [ 16 ] or ataxia telangiectasia [ 17 ]  . 
fanconi anemia and cellular radiosensitivity evaluated by the cytochalasin - blocked mn test [ 21 ] , which is well established in the biomonitoring of human populations as an indicator of radiation damage [ 33 ]  . 
 the two fibroblast strains used here initiated from skin biopsies of a control donor ( designated 1br3 ) and an fa patient ( 425br ) were kindly provided by p . 
 subjects cells monolayer cultures of each strain were grown in dulbeccos modified eagles medium ( sigma , d - 6046 ) supplemented with 10% fetal calf serum , glutamine ( 1 mm ) , and penicillin - streptomycin ( 100 u / ml and 100 g / ml , respectively ) , hereafter denoted as complete growth medium ( cgm )  . 
equal loading and transfer were assessed by reprobing the blots with anti - - actin antibody ( sigma a - 5316 ) and ponceau red ( sigma 19 , 976 - 1 ) , respectively . 
for hmre11 , rad51 or rad50 detection , membranes were incubated with respective primary and species - specific peroxidase - labeled secondary antibodies for 12 h at room temperature according to standard procedure . 
the levels of protein expression were quantified using the kodak 1d image analysis software and normalized to - actin levels . hmre11 , rad51 and rad50 foci formation fibroblasts were cultured on microscope glass slides for at least 24 h . 
subconfluent cells were irradiated with 8 gy on slides , fixed at 2 h post - irradiation in ice - cold ethanol at 20 c , and permeabilized with triton x - 100 ( 1% solution in phosphate - buffered saline [ pbs ] ) for 5 m slides were washed three times for 5 min in pbs and blocked in 4% fbs - pbs for 1 h at room temperature . 
slides were incubated for 1 h at room temperature with anti - hmre11 , - rad50 , or - rad51 primary antibodies , followed by incubation with respective secondary antibodies conjugated with alexa fluor 488 nm or 568 nslides were counterstained with 0.2 g / ml of dapi ( 4 ' , 6 ' - diamidino - 2 - phenylindole ) in antifade solution ( 1.5% n - propyl - gallate , 60% glycerol in pbs ) and examined using a leica dmlb epifluorescence microscope coupled to a cooled ccd camera ( colorview 12 )  . 
for each experimental point , at least 100 nuclei were examined , and hmre11 , rad51 or rad50 foci were scored by eye at a magnification of 1 , 000 . 
 x - ray irradiation irradiation was performed at room temperature using a 6 - mv siemens linear accelerator ( siemens , concord , ca , usa ) at a dose rate of 2 gy / mafter irradiation , cells were recovered in cgm for the indicated time until harvested . 
 western blot analysis 2 h after irradiation subconfluent control and fibroblasts irradiated with 8 gy were detached by trypsinization , lysed in ripa buffer ( 10 mm tris - hcl , ph 7.4 , 150 mm nacl , 1% sodium deoxycholate , 1% triton x - 100 ) containing protease inhibitors ( 2 g / ml aprotinin , 2 g / ml leupeptin , 5 g / ml pepstatin , 1 mm phenylmethane sulfonyl fluoride ) for 30 min on ice and subsequently centrifuged 10 min at 500 g . 
samples equivalent to 20 g of protein were separated using either 412% ( for hmre11 and rad51 ) or 38% ( for rad50 ) sodium - dodecyl - sulphate - polyacrylamide precast gels ( invitrogen , karlsruhe , germany ) and transferred to nitrocellulose x - ray treatment prior to comet assay in our earlier study [ 38 ] , fibroblast cultures were kept as monolayers during irradiation , however , the subsequent trypsinization and centrifugation lasts at least 10 min , so the given repair times in that study covered the time period between trypsinization and cell lysis , with 10 min being the earliest possible time point . 
therefore , in order to be able to study the fast component of the dna repair kinetics and to avoid trypsin - induced dna damage , in the present study fibroblasts were irradiated in a suspension . 
1 h prior to irradiation cell monolayers were rinsed with ca2 + and mg2 + - free physiological pbs ( sigma d - 8537 ) , detached by incubation for 5 min with 1 ml pbs supplemented with trypsin / edta , washed , and resuspended in cgm . 
dakin fully frosted microscope slides ( richardson supply company ltd . , london , uk ) were each covered with 400 l of 0.75% normal - melting - point agarose ( roth , 2268.2 , karlsruhe , germany ) in pbs prewarmed to 45 c . 
the coverglass was then removed , and 85 l of cell / agarose suspension ( 10 l of cell suspension containing about 104 cells was mixed with 75 l of 0.5% low - melting - point agarose , roth , 6351.1 , in pbs ) was placed over the first agarose layer and allowed to solidify under a fresh coverglass . 
after the coverglass was removed , the slides were gently immersed in a cold lysis solution ( 2.5 m nacl , 100 mm edta , 10 mm tris , 1% sodium sarcosinate , 10% dimethyl sulfoxide and 1% triton x - 100 added just before use ; ph was adjusted to 10 with naoh ) for 1 h at 4 c to lyse the cells and to permit dna unfolding . 
the microscope slides were transferred to the horizontal gel electrophoresis unit filled with fresh , chilled electrophoresis buffer ( 300 mm naoh , 1 mm edta , ph 13.5 ) to a level of about 0.25 cm above the slides and left for 20 min to allow unwinding of dna before electrophoresis . 
the slides were then drained , placed on a tray and flooded slowly with three changes of a neutralization buffer ( 0.4 m tris , ph 7.5 ) , each for 5 min , to remove alkali and detergents . 
the slides were stained with propidium iodide ( pi , sigma , p - 4170 , 10 g / ml solution in pbs ) , 50 l / slide , covered with a coverglass , and placed in a humidified air - tight container to prevent drying of the gel . 
for each cell sample , the tm data were fitted to a monoexponential function : tm ( t ) = tm0 exp + tmr ( 1 ) , ( 0.693 t ) where t is the incubation time after x - ray exposure ; tm0 and tmr are the initial reparable tm and residual ( i.e. , irreparable ) tm , respectively ; 0.5 is the repair half - time , i.e. 
the total initial tmi ( t = 0 ) is given by the sum : tmi = tm0 + tmr . micronucleus test mns were scored in binucleated cells ( bncs ) of cytochalasin b - blocked cultures according to fenech & morley [ 21 ]  . 
cytochalasin b allows division of the cell nucleus ( karyokinesis ) , but inhibits cell division ( cytokinesis ) , so cells that undergo nuclear division are easily recognized by their binucleated appearance [ 21 ]  . 
at 48 h post - incubation cells were trypsinized , placed on glass slides by cytospin centrifugation , fixed in cold methanol ( 20 c , 1 h ) , and stained with acridine orange ( sigma , a - 4921 , 20 g / ml )  . 
mn scoring was performed in 1 , 000 bncs according to the published criteria [ 21 ] using a leica dmlb fluorescence microscope ( wetzlar , germany )  . statistics data are presented as mean ( sd or se )  . 
 comet capture and analysis pi - stained electropherograms were examined in an epifluorescent microscope ( leica , wetzlar , germany ; dmlb , excitation filter : 515560 nm ; barrier filter : 590 nm ) attached to a black and white ccd video camera ( cohu electronics , san diego , ca , usa ) , that was connected to a computer equipped with the image analysis software komet 3.1 ( kinetic imaging ltd . , liverpool , uk )  . 
 superimposed and dead cells , as well as the cells on the edge of the gels were avoided . results short - term response to x - irradiation studied by the comet assay as we pointed out in the introduction , the major lesions associated with ionizing radiation are the dna dsbs for which multiple repair pathways in mammalian cells exist [ 29 ]  . 
 moreover , the mechanisms that are proposed to vary the yield of radiation - induced dsbs are also expected to vary the yield of radiation - induced ssbs [ 49 ]  . 
as clearly seen from the representative microphotographs in figure 1 , the tails are more pronounced in the irradiated sample obtained from the fa patient ( figure 1 , right panel ) than in that isolated from the control individual ( figure 1 , left panel )  . 
the mean ( se ) tm data of the two cell samples , each consisting of 75100 cells , were plotted as functions of time ( figure 2 , symbols ) and fitted to equation 1 using the least - square method ( figure 2 , smooth curves )  . 
in order to facilitate visual comparison of the fa and control data , the tm values were normalized to the corresponding initial dna damage values ( inset in figure 2 )  . 
it is clearly seen from the inset that the normalized curves are not identical , and the initial slopes ( and so the rates of dna repair ) are very different in the two cell strains . 
 expression of hmre11 , rad50 and rad51 a lot of experimental evidence supports the idea that an intact rad50 - mre11 - nbs1 complex is essential for a normal cellular response to dsbs [ 40 , 41 ]  . 
on the other hand , although no human genetic syndrome has been associated with rad51 , rad52 , rad54 , etc . , recent observations show that the rad51 protein was elevated tenfold above normal levels in fa group a , c and g fibroblasts [ 18 ] ; however , in group d2 the rad51 level was identical to that in normal cells . 
 in our study , we proposed that the dna repair proteins , namely , hmre11 , rad50 and rad51 , could be good candidates for screening for abnormalities in the repair of radiafigures 1a to 1j . 
 the cells were exposed in vitro to 5 gy of x - rays and then subjected to the alkaline single - cell gel electrophoresis ( comet ) assay either immediately ( a , b ) or at the indicated time after irradiation ( cj )  . 
after staining with propidium iodide , the comets were examined using an epifluorescence microscope ( leica , wetzlar , germany ; dmlb , magnification : 400 ) , attached to a colorview 12 ccd camera that was connected to a computer equipped with the image analysis software analysis 3.1 ( softimaging system gmbh , mnster , germany )  . 
die zellen wurden in vitro mit 5 gy bestrahlt und unmittelbar anschlieend ( a , b ) oder zur angezeigten zeit nach bestrahlung ( cj ) dem alkalischen comet - assay unterworfen . 
typical western blot analysis of the expression of the hmre11 and rad51 ( a ) , and rad50 ( b ) dna repair proteins in nonirradiated and irradiated control and fa cells . 
western - blot - analyse von hmre11 ( a , obere reihe ) , rad50 ( a , mittlere reihe ) und rad51 - proteinen ( b , obere reihe ) in normalen und fa - hautfibroblasten . 
however , in the irradiated cells derived from an fa patient we found a significant reduction in the fraction of rad51 ( 67 15% ) foci - positive cells compared with that ( 97 14% ) in control cells . 
 analysis of the immunofluorescence data by counting both foci - positive cells ( figure 4 ) and the number of foci per nucleus ( data not shown ) indicated that fibroblasts derived from an fa patient differ in their rad51 foci - forming response to irradiation compared with control cells . 
there were consistently more cells displaying rad51 foci after irradiation in the control cell line , and moreover , the number of irradiation - induced rad51 foci per nucleus was also significantly higher in control cells . 
the slow rate of mn induction in control cell lines irradiated with doses in the range of 13 gy was somewhat unusual , however , such radiation response was already observed in several fibroblast strains [ 34 ]  . 
comparison of the mean mn data reveals that x - irradiation led to an increased accumulation of mns ( by a factor of 1.51.7 ) in fa fibroblasts compared with control cells . 
in addition , the comparison of the proliferative ability ( rate of binucleation ) shown in the inset in figure 5 revealed the higher inhibition of proliferation in irradiated fa cells than in control cells . 
 the results of the comet assay ( figures 1 and 2 ) revealed that the initial dna fragmentation in the irradiated fa cells was two times higher and the dna rejoining process three times slower than in control fibroblasts . 
the findings on irradiated fa skin fibroblasts obtained here with the comet assay ( figure 2 ) agree with our previous results on peripheral mononuclear cells from fa patients and carriers [ 16 ]  . 
at the moment , there is no explanation for such a pronounced difference ; however , it is noteworthy that the recognition of dna damage by means of the comet assay is influenced by a number of factors that can alter the release of dna from the nuclear protein matrix . 
preexisting intrinsic alterations in chromatin conformation , a decreased condensation of supercoiled dna or higher degree of inhibition of loop rewinding in radiosensitive cells [ 12 , 36 , 51 ] might well determine the extent of dna migration in irradiated cells . 
furthermore , the increased radiation response of fa cells is consistent with the notion that fa might be a chromatin disease in which a defective complex of fa proteins does not adequately fulfill its role in chromatin remodeling in situation of cellular stress [ 26 ]  . 
 hmre11 rad50 rad51 p < 0.05 discussion in the present study , two strains of skin fibroblasts isolated from an fa patient with severe clinical radiosensitivity , described elsewhere [ 31 ] , and from an apparently healthy donor were evaluated for their in vitro radiosensitivity using 0 gy 8 gy 0 gy 8 gy 0 gy 8 gy 0 gy 8 gy 0 gy 8 gy 0 gy 8 gy control control control figure 4 . 
micronucleus ( mn ) expressions induced by in vitro irradiation in fibroblasts from the fa patient ( filled symbols ) are shown in comparison with the cells from the control subject ( open symbols )  . 
 each data point represents the mean number ( sd ) of mn in binucleated cells ( bncs ) of two slides from two experiments with at least 1 , 000 bncs scored per slide . 
induktion der mikrokerne ( mn ) nach in - vitro - bestrahlung in den fibroblasten der fa - patientin ( schwarze symbole ) im vergleich mit den zellen des kontrollspenders ( offene symbole )  . 
 the slow kinetics of the restitution of dna damage in irradiated fa cells shown here by the comet assay ( figure 2 ) is in line with the defects of the dna repair mechanism earlier reported for fa cells [ 13 , 42 ]  . 
therefore , we tested whether defects in the dna repair proteins , such as hmre11 , rad50 and rad51 , could account for the observed alteration in the kinetics of dna repair in fa cells after irradiation . 
 our data on the normal expression of hmre11 and rad51 in fa strain 425br are in line with those published in [ 14 ] , where it was demonstrated that fa fibroblasts express the same amounts of hmre11 and rad51 as normal cells do . 
 [ 18 ] who found tenfold elevated above normal level of rad51 in fa fibroblasts of group a , c and g , but normal level in group fa d2 fibroblasts . 
as shown previously [ 30 ] , the fa fibroblast strain 425br used in our study belongs to fa subtype a , so one of the underlying sources of the discrepancy between our data and those of donahue et al . 
 [ 18 ] could be the fact , that we measured protein distribution in the whole cell extracts , and not in the nuclear extracts as it was reported in donahue et al . 
 the increased induction of mns in fa cells after x - irradiation ( figure 5 ) is in accord with the data of maluf & erdtmann [ 30 ] who report an increased frequency of mn in nonirradiated leukocytes from fa patients . 
a forthcoming study from our own laboratory shows an increased frequency of chromosome aberrations in irradiated ( with 0.7 gy ) lymphoblastoid cells from another fa patient ( 30% of metaphases are aberrant ) compared with control ( 0% of aberrant metaphases ) and ataxia telangiectasia ( 7% of aberrant metaphases ) cells ( djuzenova & flentje , unpublished observation ) detected by 24 - color fish [ 28 ]  . 
 therefore , the findings on this particular fa cell strain presented in our report point toward the difficulties involved in the prediction of the radiation response of cell lines and tumors based solely on the colony survival test . 
 in summary , the increased dna fragmentation revealed by the alkaline comet assay and altered formation of foci containing rad51 dna repair protein , as well as the increased mn production in irradiated fa fibroblasts shown in our study can be correlated with the marked clinical radiosensitivity reported previously for this fa patient [ 31 ]  . 
the ptv , the ipsilateral lung ( il ) and the contralateral lung ( cl ) were defined in each axial ct slice ( slice thickness 1 cm )  . 
the dvhs were analyzed relating the minimum , maximum , median and mean dose to the volumes of interest ( voi )  . results : median ptv amounted to 774 cm3 . 
since it is generally accepted that the cc algorithm describes secondary particle transport more exactly than pb models , the use of the latter should be critically evaluated in the treatment planning of lung cancer . key words : lung cancer radiotherapy calculation algorithms collapsed cone algorithm pencil beam algorithm strahlenther onkol 2004 ; 180 : 7838 doi 10.1007 / s00066 - 004 - 1268 - 4 der einfluss des rechenalgorithmus auf die dosisverteilung bei der bestrahlung des nichtkleinzelligen bronchialkarzinoms ( nsclc )  . 
das ptv , die ipsilaterale lunge ( il ) und die kontralaterale lunge ( cl ) wurden in jeder axialen ct - schicht definiert ( schichtdicke 1 cm )  . 
unter verwendung von cc wurden lediglich 76 , 5% des ptv von der 95% - isodose umschlossen , whrend dies unter verwendung des pb bei 90 , 1% der fall war ( p = 0 , 01 )  . 
das volumen der il innerhalb der 1department of radiotherapy , university of wuerzburg , wuerzburg , germany . received : december 11 , 2003 ; accepted : september 30 , 2004 strahlenther onkol 2004 no . 
calculation algorithms for radiotherapy of lung cancer 80% - isodose betrug 19 , 6% fr den ccund 24 , 1% fr den pb - algorithmus ( p < 0 , 01 )  . 
das volumen der cl innerhalb der 80% - isodose war 3 , 3% fr den ccund 4 , 1% fr den pb - algorithmus ( p = 0 , 03 )  . schlussfolgerung : die berechnung der dosisverteilung mit dem ccbzw . 
da der cc - algorithmus die tatschlichen streuungsverhltnisse im gewebe unterschiedlicher dichte genauer bercksichtigt als der pb - algorithmus , sollte die verwendung des pb - algorithmus fr die bestrahlungsplanung des bronchialkarzinoms sehr kritisch beurteilt werden . schlsselwrter : bronchialkarzinom radiotherapie rechenalgorithmen collapsed - cone - algorithmus pencil - beamalgorithmus certainties like patient movements , setup displacements and organ movements ; ( cid : 127 ) the volume of the ipsilateral lung ( il ) ; ( cid : 127 ) the volume of the contralateral lung ( cl )  . treatment planning was done by a three - dimensional planning system ( helax , tms , v.6.01 ) using 18 - mv photon beams to be delivered by a primus ( siemens ) linear accelerator . 
a conformal multiple - beam technique was planned for each patient using a pb algorithnumber of beams , beam angles , wedges and position of collimator leaves arranged in beams eye view technique were individually selected to encompass the ptv as conformal as possible . 
subsequently , each treatment plan was recalculated using a point kernel model , which is implemented in the tms in an analytical collapsed tumor ( white water ; rw3 ) 0.7 cm chest wall ( white water ; rw3 ) lung parenchyma ( styrofoam ) lung parenchyma ( styrofoam ) chest wall ( white water ; rw3 ) 6 cm 5 cm 2 cm 5 cm 6 cm introduction lung cancer is the most common cancer in the world and we expected about 375 , 000 new cases in europe for 2000 [ 21 ]  . 
since only 2030% of patients with non - small cell lung cancer ( nsclc ) are suitable for curative surgery , primary radiotherapy plays an important role in therapy of nsclc . 
in contrast to conventional radiotherapy , three - dimensional conformal radiotherapy ( 3drt ) based on a three - dimensional treatment planning system ( 3dps ) provides the possibility to deliver higher radiation doses to the tumor simultaneously sparing normal tissues [ 2 , 5 , 7 , 9 , 13 , 15 , 16 , 20 ]  . 
the purpose of this paper was to analyze the influence of different algorithms on dose distributions in radiotherapy of nsclc . material and methods ten consecutive patients ( nine male , one female ; median age 64.9 years ) receiving definitive radiotherapy because of nsclc were studied . 
the following volumes of interest ( voi ) were defined in each axial ct slice : ( cid : 127 ) planning target volume ( ptv ) : including the tumor and the ipsilateral hilar and mediastinal lymph node region including a margin to encompass subclinical disease and treatment - related unfigure 1 . 
schematic illustration of the lung phantothe outer dimensions of the phantom are 30 30 24 cthe position of ionization chamber measurement ( point a ) was at 150 mm depth and is marked by x . 
exemplary dose distribution in an axial slice calculated by the pencil beam algorithin the calculated dose distribution the 20% ( 1 ) , 40% ( 2 ) , 60% ( 3 ) , 80% ( 4 ) , 90% ( 5 ) , 95% ( 6 ) , and 100% ( 7 ) isodose lines are displayed . 
exemplary dose distribution in an axial slice calculated by the collapsed cone algorithin the calculated dose distribution the 20% ( 1 ) , 40% ( 2 ) , 60% ( 3 ) , 80% ( 4 ) , 90% ( 5 ) , 95% ( 6 ) , and 100% ( 7 ) isodose lines are displayed . 
grid size of dose matrix geometry was 2.5 mm for dose calculation . phantom measurements were implemented to validate the planning syste a special phantom was designed for this study ( figure 1 )  . 
it consists of solid white water ( rw3 ) and styrofoathe geometry characteristics and density of the phantom were inserted into the planning systethe isocenter was located at point a at 150 mm depth in the phanto dose at point a was calculated for a 20 20 cm field for 18 - mv photons using the pb and the cc algorithadditionally , an ionization chamber measurement was performed at point a . 
the phantom was irradiated by 100 monitor units using 18 - mv photons . the statistical significance of comparing cc and pb algorithm was determined using the t - test for dependent samples . 
volume of il within the 80% isodose was 19.6% for the cc and 24.1% for the pb algorithm ( p < 0.01 ; table 2 )  . median volume of cl was 1 847 cm3 . 
pb algorithm overestimates the dose at point a by 11.4% , whereas there was only a difference of 1.2% between the measured dose and the dose calculated by cc algorithm . discussion in the past , several studies compared the treatment technique devised with conventional planning techniques to those devised with 3drt [ 2 , 5 , 13 ]  . 
additionally , 3dpss lead to an improved quantification of doses resulting in a more precise dose prescription to the tumor and a better definition of normal tissue tolerances in terms of dvhs [ 6 , 18 , 19 , 23 ]  . 
while the effect of inhomogeneities on the primary photon fluence is mostly well predicted , their influence on the dose delivered by scattered radiation is often approximated in a less accurate way . 
however , due to a large demand of computational power monte carlo algorithms were not in widespread use for clinical treatment planning in the past . instead , 3dps of the last generation generally used pb algorithms for dose calculation . 
the clinical studies evaluating the benefit of 3drt or correlating lung complication like pneumonitis with dose distributions mostly used pb or even less accurate algorithms [ 4 , 17 , 19 ]  . 
as a consequence , the dose calculation yields precise results as long as there is lateral charged particle equilibriu but this condition fails for irradiation of tumors near air cavities like head and neck cancer and lung cancer . 
the dose at the 95% isodose level , as calculated with a pb algorithm for 15 - mv photons , was actually 21.2% lower when measured in the phantoseen from this angle , the results of the studies using pb algorithms for correlation of tumor control probability and normal tissue complication probability with dose distribution should be considered critically . because of the limitations of the pb algorithms some 3dps of the newer generation implemented point kernel - based models like the cc approach . 
in a comparison of pb and cc algorithms for radiotherapy of head and neck cancer , the cc algorithm best estimates the buildup effect at the air - tissue boundary [ 14 ]  . 
 [ 4 ] verified the lung dose in an anthropomorphic phantom calculated by the cc algoriththey described an up to 5% variation between doses calculated at the center and near the edge of the phantom and concluded the cc algorithm accurately calculates dose within inhomogeneous lung regions . 
 but what are the consequences for the clinical practice ? an option to countervail the lower dose at the air - tissue boundary could be a technical modification , e.g. , an enlargement of the beam sizes toward the lung . 
the knowledge of the dose - effect relation of an irradiation - induced pneumonitis based on the great clinical experience with treatment planning systems using the pb algorithan enlargement of beam sizes could result in an increased incidence of pneumonitis . 
 conclusion the calculation algorithm used for the clinical situation of radiotherapy of lung cancer influences the dose distribution especially for a ptv situated in or at the boundary of an air cavity . 
for clinical studies and the publication of their results it is not sufficient to describe the prescribed dose at the normalization point and the dvhs , but it is also necessary to describe the algorithm used for dose calculation as well . strahlentherapie und onkologie original article interstitial high - dose - rate brachytherapy in the treatment of base of tongue carcinoma zoltn takcsi - nagy1 , csaba polgr1 , ferenc oberna2 , andrs somogyi1 , tibor major1 , va remenr3 , jnos fodor1 , mikls ksler3 , gyrgy nmeth1 background and purpose : to date none of the studies examined the feasibility and efficacy of interstitial high - dose - rate ( hdr ) brachytherapy in the treatment of carcinoma of the tongue base . 
therefore the aim of this study was to contribute to this issue . patients and methods : between 1992 and 2000 37 patients ( mean age 55 years ) with t14 and n03 carcinoma of the base of tongue were presented . 
30 patients with advanced stage received brachytherapy boost after 5066.5 gy ( mean , 60 gy ) locoregional external beam irradiation ( ebi ) and 7 patients with early stage ( t12 , n0 ) were managed locally with wide tumor excision and sole brachytherapy . 
the mean dose of boost and sole brachytherapy was 18 gy and 28 gy , respectively . results : the median follow - up time for surviving patients was 51 months . 
for patients treated with ebi and brachytherapy boost , the 5 - year actuarial rate of local , locoregional recurrence - free and overall survival was 60% , 52% and 46% , respectively . 
none of the sole brachytherapy patients experienced severe late radiation toxicity . conclusion : ebi combined with interstitial hdr brachytherapy boost result in acceptable local tumor control with low incidence of late side effects in patients with advanced disease . 
 key words : base of tongue high - dose - rate brachytherapy strahlenther onkol 2004 ; 180 : 76875 doi 10.1007 / s00066 - 004 - 1238 - x interstitielle high - dose - rate - brachytherapie in der behandlung des zungengrundkarzinoms hintergrund und ziel : zurzeit liegt keine internationale studie vor , die die anwendbarkeit und wirksamkeit der interstitiellen high - dose - rate - ( hdr - ) brachytherapie in der behandlung des zungengrundkarzinoms untersucht . 
ziel dieser arbeit ist es , unser petientenkollektiv retrospektiv zu analysieren und unsere therapiestrategien vorzustellen . patienten und methode : zwischen 1992 und 2000 wurden 37 patienten ( durchschnittsalter : 55 jahre ) mit zungengrundkarzinomen im stadium t14 n03 behandelt . 
die rate bezglich der 5 - jhrigen lokalen , lokoregionalen rezidivfreiheit und der gesamtberlebenszeit bei patienten , die mit ebi und brachytherapie - boost behandelt wurden , betrug 60% , 52% bzw . 
bei patienten , die mit einer alleinigen brachytherapie behandelt wurden , traten keine sptnebenwirkungen auf . 1 department of radiotherapy , national institute of oncology , budapest , hungary , 2 department of maxillofacial surgery , st . 
rokus hospital , budapest , hungary , 3 department of head and neck , maxillofacial and reconstructive plastic surgery , national institute of oncology , budapest , hungary . received : september 24 , 2003 ; accepted : april 1 , 2004 strahlenther onkol 2004 no . 
interstitial hdr brachytherapy in base of tongue carcinoma schlussfolgerung : ebi gefolgt von interstitieller hdr - brachytherapie fhrt zu einer annehmbaren lokalen tumorkontrolle bei patienten mit fortgeschrittenen karzinomen , wobei das risiko chronischer sptfolgen gering ist . 
 schlsselwrter : zungengrundkarzinom high - dose - rate brachytherapie introduction carcinomas of tongue base are often diagnosed when the disease is already advanced and lymph node metastases are present in 50% of the patients [ 3 ]  . 
both early and advanced lesions can be treated with partial or total glossectomy with or without radiotherapy or irradiation alone [ 4 , 13 , 16 , 17 , 20 , 28 , 31 ]  . 
organ preservation treatment modalities are recently emphasized to maintain good speech and swallowing function with high locoregional control [ 8 , 16 , 35 , 36 , 39 ]  . 
low - dose - rate ( ldr ) interstitial brachytherapy has been reported as the most effective technique to increase target volume dose and to reduce the risk of normal tissue complications [ 8 , 16 , 35 , 36 ]  . 
the use of ldr brachytherapy in the treatment of base of tongue cancer is well established , however , none of the studies examined the feasibility and efficacy of high - dose - rate ( hdr ) brachytherapy . 
the other 30 patients ( 81% ) with advanced ( stage iiiiv ) disease were managed with primary radiotherapy , external beam irradiation ( ebi ) + interstitial hdr brachytherapy boost to the primary site , neck dissection . 
28 ( mean , 5 ) flexible plastic tubes ( 27 patients ) or 24 ( mean , 4 ) rigid steel needles ( 10 patients ) were inserted into the tumor or tumor bed under general anesthesia [ 38 ]  . 
the ends of the flexible tubes were fixed with plastic buttons either on the submental skin for loop technique or on the surface of the base of tongue for non - loop technique . 
in case of rigid needle technique implants were inserted through the oral cavity ( 1 patient ) or submental area ( 9 patients )  . the rules of the paris system were used for the planning of the implant geometry [ 34 ]  . 
at the beginning years of our study ( 19921995 ) flexible implant tubes were not available at our department , thus only rigid needles were used with their known technical limitations . 
 in case of ct images the ptv was defined as the primary tumor ( or tumor bed ) plus a margin of 0.51 cthe active source positions and reference dose points were defined individually in each catheter / needle . 
dose optimization on dose points and geometry was performed and the dose was prescribed to the 100% isodose surface [ 10 ]  . for all patients v100 , v150 and dose non - uniformity ratio were applied for quantitative dose assessment of the interstitial implants . 
the v100 reference volume is the volume receiving equal to or greater dose than the reference dose , the v150 high dose volume is a volume that receives equal to or greater dose than the reference dose multiplied by 1.5. 
the coverage index , which is the fraction of the target volume receiving a dose equal to or greater than the prescribed dose , was calculated for patients ( n = 10 ) planned with ct images . 
 surgery + sole hdr brachytherapy primary ebi + hdr brachytherapy boost 7 patients with t12n0 , exophytic ( n = 6 ) or infiltrating ( n = 1 ) cancer underwent tumor excision with ( n = 4 ) or without ( n = 3 ) elective unilateral neck dissection . 
the tumor bed was implanted intraoperatively ( n = 3 ) or 3 weeks after surgery ( n = 4 ) to treat the primary site with interstitial sole hdr brachytherapy . 
ebi : external beam irradiation ; bt : brachytherapy ; s : surgery ; ajcc : american joint committee on cancer [ 15 ] ; na : not applicable ( for patients treated without surgery )  . 
 in case of flexible tube technique ( n = 20 ) , the dose was delivered except with four cases , when the dose was 12 gy in one fraction on 34 consecutive days , given in five to eight fractions of 35 gy up to a total dose of 1530 gy ( mean , 21 gy )  . 
 the mean brachytherapy dose using the rigid needle technique was 14.2 gy ( range , 1222 gy ) given in a single fraction of 12 gy ( n = 6 ) , or in two or three fractions of 611 gy ( n = 4 ) using two or three separated implantations . 
neck dissections ( six unilateral and two bilateral ) were performed in 8 ( 27% ) patients , in five cases at the time of brachytherapy implant and in three cases 1 month after completing brachytherapy , because of palpable and biopsy proven residual nodal disease with complete remission of the primary . 
initial tumor response for the primary radiotherapy group ( n = 30 ) was assessed at the first follow - up visit using conventional volume change categories ( complete response [ cr ] , partial response [ pr ] , no change [ nc ] )  . 
 results the 5 - year actuarial overall survival , locoregional tumor control , and local tumor control for all patients was 56% , 61% and 68% , respectively . surgery + sole hdr brachytherapy all 7 patients treated with surgery + sole brachytherapy were alive and controlled loco - regionally during the follow - up period without evidence of distant metastasis . 
 uniand multivariate analysis of prognostic factors for local and locoregional tumor control and survival results of univariate cox regression analysis of possible prognostic factors for local and locoregional failure rate are sumtable 2 . 
the other 6 patients 5 of them received chemotherapy died of further local and regional ( n = 3 ) or regional ( n = 2 ) progression , except 1 patient who died of gastric ulceration . 
both of them died of disease with a postmetastatic survival of 3 and 2 months . during the follow - up period 5 ( 14% ) of 37 patients died of other causes ( 2 lung cancer , 1 hypopharyngeal tumor and 2 cardial disease )  . 
 dosimetric evaluation of implants mean and median v100 were 59 and 61 cm3 ( range , 12.594 cm3 ) , mean and median v150 were 24 and 28 cm3 ( range , 5.253.2 cm3 ) , respectively . 
5 - jahres - berlebensraten gem kaplan - meier - berechnung bei patienten , die mit ebi + hdr - brachytherapie - boost behandelt wurden ( n = 30 )  . 
12 urban & vogel a n = number of events / patients ; b infiltrating + ulcerative morphology together in multivariate analysis both t status ( p = 0.032 ; rr : 3.68 ; 95% ci : 1.1212.11 ) and nodal status ( p = 0.007 ; rr : 17.52 ; 95% ci : 2.18140.76 ) remained significant risk factors of overall survival . 
interstitial hdr brachytherapy in base of tongue carcinoma discussion the standard treatment of early stage ( t12 ) base of tongue cancer is surgery or radiotherapy alone or surgery with postoperative radiotherapy [ 17 , 20 , 21 , 22 , 31 , 32 , 36 ]  . 
local control for patients with early stage ( t12 ) disease treated with surgery ( adjuvant radiotherapy ) or radiotherapy ( ebi brachytherapy ) have been reported in the range of 77100% and 56100% , respectively , in a retrospective , nonrandomized , multi - institutional , pooled analysis [ 32 ]  . 
 some authors treated early stage ( t12 ) base tongue tumor with radiotherapy ( ebi and brachytherapy ) alone , and the local control varied from 50100% ( table 4 )  . 
in our series 7 patients with t12 base of tongue cancer after tumor excision were treated with hdr brachytherapy alone and the local control was 100% without serious late radiation toxicity at a median follow - up time of 47 months ( range , 2778 months )  . 
 in the treatment of locally advanced base tongue cancer radiotherapy using modern techniques is recommended recently instead of radical surgery to improve results without functional and esthetic deficit [ 9 , 27 , 30 , 40 ]  . 
 [ 23 ] study with sole radiotherapy the 2 - year local control rate was 45% for t3 , and 23% for t4 lesions with a 5 - year overall survival of 27% for all cases . 
ebi : external beam irradiation ; bt : brachytherapy ; fup : follow - up period ; lc : local control ; os : overall survival ; ldr : low - dose - rate ; nr : not reported ; uk : unknown . 
in spite of the high proportion of t4 cases ( 53% ) in our series , the results were appropriate : complete response rate of 80% , local control rate of 60% ( 48% for t4 ) , and 5 - year overall survival of 46% . 
it is also to be noted , that 2 / 10 ( 20% ) patients with local failure were successfully salvaged and cured , yielding an ultimate crude local tumor control of 73% ( 22 / 30 )  . successful radiation therapy of base of tongue carcinomas requires total dose above 70 gy , which , however , increases the risk of osteoradionecrosis and xerostomia [ 2 , 11 , 29 , 33 ]  . 
the low incidence of serious late side effects in our series ( only 1 osteoradionecrosis ; 3% ) also justifies the feasibility of hdr interstitial brachytherapy as a boost treatment . in summary ebi combined with interstitial hdr brachytherapy boost results in acceptable local tumor control with low incidence of late side effects in patients with advanced disease . 
 strahlentherapie und onkologie short communication phase ii trial of hyperfractionated accelerated splitcourse radiochemotherapy with 5 - fu and cis - ddp in advanced head and neck cancer results and toxicity antje ernst - stecken1 , gerhard grabenbauer1 , heinrich iro2 , ludwig plasswilm3 , rolf sauer1 background : simultaneous radiochemotherapy resulted in a significant benefit improving both local control and overall survival in advanced head and neck cancer . 
in this phase ii study the efficacy and toxicity of a hyperfractionated accelerated split course radiotherapy with simultaneous application of 5 - fu and cisplatin were evaluated in patients with locally advanced tumors of the oral cavity , oroand hypopharynx . 
 results : overall survival , cause - specific survival , locoregional tumor - free survival and distant metastasis - free survival were 53% , 65% , 77% and 73% , respectively , at 3 years . 
 key words : squamous cell carcinoma advanced head and neck cancer altered fractionation combined modality treatment strahlenther onkol 2004 ; 180 : 80510 doi 10.1007 / s00066 - 004 - 1307 - 1 ergebnisse einer phase - ii - studie zur hyperfraktionierten akzelerierten radiochemotherapie mit 5 - fu und cisplatin bei fortgeschrittenen kopf - hals - tumoren hintergrund : die simultane radiochemotherapie hat bei fortgeschrittenen kopf - hals - tumoren eine signifikante verbesserung von lokaler kontrolle und gesamtberleben erreicht . 
die vorliegende phase - ii - studie hat die effektivitt und toxizitt einer hyperfraktionierten akzelerierten simultanen radiochemotherapie mit 5 - fu und cisplatin bei fortgeschrittenen tumoren der mundhhle , des hypound oropharynx gepr patienten und methode : von 1991 bis 2002 wurden 45 patienten zweimal tglich mit einer einzeldosis von 1 , 5 gy bis zu einer medianen dosis von 72 gy bei einer 1 - wchigen pause nach 30 gy bestrahlt . 
behandlungswoche wurden simultan 5 - fu ( 800 mg / m2 kof / d kontinuierlich ) und cisplatin ( 20 mg / m2 kof / d als bolus ) appliziert . 
 ergebnisse : gesamtberleben , tumorspezifisches berleben , lokoregionre kontrolle und fernmetastasenfreies berleben nach drei jahren betrugen 53% , 65% , 77% und 73% mit einem medianen follow - up von 21 monaten . 
zuknftige protokolle mssen den einsatz neuer chemotherapeutika beinhalten , eventuell auch mit prfung der durchfhrbarkeit einer erhaltungschemotherapie . schlsselwrter : plattenepithelkarzinom fortgeschrittene kopf - hals - tumoren alternative fraktionierung simultane radiochemotherapie 1 department of radiation therapy at the university of erlangen - nrnberg , germany , 2 department of head and neck surgery at the university of erlangen - nrnberg , germany , 3 department of radiation therapy at the university of basle , basle , switzerland . 
phase ii trial of radiochemotherapy in head and neck cancer introduction most of the patients with head and neck cancer present with advanced stages of disease not amenable for resection . 
the basis of these efforts is obvious : conventionally fractionated radiation therapy alone is only able to provide local tumor control rates of about 30% and , in addition , most of the squamous cell carcinomas are sensitive to chemotherapy . 
a significant improvement of local tumor control has been shown for concurrent 5 - fu , cddp , carboplatin , mitomycin c and methotrexate and radiotherapy [ 3 , 31 , 45 , 47 ]  . 
the aim of accelerated radiotherapy is to reduce tumor proliferation by shortening overall treatment time whereas hyperfractionated radiotherapy may increase the therapeutic ratio by taking advantage of different fractionation sensitivities between tumor and normal tissue and thereby reducing late morbidity [ 5 , 18 ]  . 
the rtog phase iii randomized study 9003 comparing standard fractionation radiotherapy to accelerated and hyperfractionated radiotherapy showed a significantly better locoregional outcome for the accelerated treatment schedules [ 19 ]  . 
 however , side effects of hyperfractionated , accelerated radiotherapy regimes with simultaneous application of chemotherapy may increase both early and late treatment related toxicities [ 7 , 19 ]  . 
on the other hand , a frequently underestimated problem is the high rate of comorbidities in many patients with advanced head and neck cancer representing an important prognostic indicator and factor influencing therapeutic decisions [ 2022 , 33 ]  . 
 for hypopharyngeal cancer , patients with carcinoma of the pyriform sinus showed an overall survival rate of 25% after 3 years and a cause - specific survival rate of 4050% [ 23 ]  . 
 with a median age between 50 and 70 years significant risk factors such as congestive heart disease , cardiac arrhythmia , peripheral vascular disease , pulmonary disease and renal disease may exist [ 32 ]  . 
 the aim of this trial was to determinate the efficacy and toxicity of a hyperfractionated accelerated split course radiotherapy regime with simultaneous application of 5 - fu and cisplat patients and methods between 1991 and 2002 , 45 consecutive patients with pathologically confirmed irresectable squamous cell carcinoma of the oral cavity , oropharynx and hypopharynx were treated at the department of radiation therapy at the university of erlangen - nrnberg . 
 of the patients with t1 and t2 cancer , 5 presented with carcinoma of the hypopharynx , 1 with oropharyngeal cancer and 1 with a tumor of the oral cavity . 
further inclusion criteria were : karnofsky performance status 70% , age 18 years , no distant metastatic disease , dental examination and therapy if necessary prior to treatment , adequate bone marrow function defined as an absolute peripheral granulocyte count 2 , 000 cells / mm3 , platelet count of 100 , 000 cells / mm3 , adequate hepatic function with bilirubin 1.5 mg% , serum cretable 1 . 
phase ii trial of radiochemotherapy in head and neck cancer atinine 1.5 mg% , sgot 2 the upper limit of normal , normal serum calcium ( without intervention ) , creatinine clearance > 50 ml / min determined by 24 - hour collection , no clinically significant heart disease , no significant ventricular arrhythmia requiring medication with antiarrythmics , no symptomatic coronary artery disease ( angina ) , no myocardial infarction within the last 6 months , no second or third degree heart block . 
patients had to sign a study - specific informed consent forexclusion criteria were : histology other than squamous cell carcinoma , evidence of distant metastases , prior chemotherapy or prior radiotherapy to the head and neck , initial surgical treatment excluding diagnostic biopsy , patients with simultaneous primaries , pregnant women ; patients with a history of non - melanoma skin cancer were eligible . 
 radiotherapy all patients were irradiated twice daily to the primary tumor region and the clinically involved lymph nodes , including the whole regional lymphatic drainage of the neck using a pair of parallel opposed portals . 
 in 41 ( 91% ) patients an additional boost was given up to a median total dose of 72 gy ( 6674 gy ) to all sites of clinical involvement with a safety margin of 12 cin all patients primary and boost treatment planning was based on ct - scans . 
 chemotherapy chemotherapy consisting of 5 - fluorouracil ( 5 - fu ) as continuous intravenous infusion and cisplatin ( cis - ddp ) as intravenous bolus was simultaneously administered from day 1 to 5 and day 29 to 33 using doses of 800 mg / m2 / d ( 5 - fu ) and 20 mg / m2 / d ( cis - ddp ) , respectively . 
 supportive care and standard medication all patients received an endoscopically controlled percutaneous gastrostomy prior to treatment in order to ensure enteral feeding in case of mucositis and to enable enteral medication during treatment in case of fungal or bacterial infections . 
patients were examinated by the head - and - neck surgeon and the radiotherapist 68 weeks after treatment , afterwards each 3 months during the first 2 years and then each 6 months for the whole follow - up . 
 cause - specific survival ( css ) , locoregional tumor - free survival ( lrc ) and distant metastasis - free survival ( dmf ) were calculated using product limit estimates as defined by the kaplan and meier method . 
 results restaging procedures 6 weeks after rct showed complete clinical remission in 36 ( 80% ) and partial remission in 8 ( 18% ) patients ; 1 had no change . 
 survival and prognostic factors overall survival ( os ) , cause - specific survival ( css ) , locoregional tumor - free survival ( lrc ) and distant metastasis - free survival ( dmf ) at 3 years were 49% , 65% , 77% and 73% , respectively ( figures 1 and 2 )  . 
4 ( 9% ) patients died without evidence of tumor , 13 ( 29% ) patients died from distant metastases , 1 died from toxic death , 2 died from secondary head and neck tumors . 
 toxicity grade - 2 dermatitis with moderate erythema and erosive skin lesions below 50% of the irradiated skin requiring local ointment therapy occurred in 35 ( 78% ) , grade - 3 dermatitis with intense erythema , erosive lesions of more than 50% and massive edema in 8 ( 18% ) patients . 
 intensity grade 01 acute toxicity ( ctc ) mucositis dermatitis anemia wbc platelets creatinine skin mucosa xerostomia swallowing kidney mandibula late toxicity ( rtog ) 4 58 36 87 15 24 22 29 44 97 6 discussion had permanent mild dysphagia and painful swallowing ; 23 ( 51% ) patients are continuously depending on an enteral feeding tube . 
 a recently published meta - analysis showed that there is a small but statistically significant benefit of 4% on survival for chemotherapy simultaneously added to locoregional radiation treatment in patients with nonmetastatic head and neck squamous cell carcinomas [ 34 ]  . 
the combination of radiotherapy and chemotherapy had a profound impact on locoregional recurrence [ 9 , 11 , 17 , 25 , 34 , 46 ] , on survival with local control [ 46 ] and on overall survival , as shown in the aro 95 - 6 trial [ 10 ]  . 
the combination of carboplatin and paclitaxel showed a relatively high response rate of 87% after induction and an overall survival rate of 70% at 3 years with a median follow - up of 28 months [ 43 ]  . 
the intensity of simultaneous chemotherapy with 5 - fluorouracil , hydroxyurea and paclitaxel to radiotherapy had to be reduced in more than 20% of the patients and there is no information , how many patients had a delayed start of locoregional therapy [ 43 ]  . 
 karnofsky performance status during therapy was unchanged in 4 ( 9% ) patients , 36 ( 80% ) patients developed mild fatigue , 4 ( 9% ) patients had severe weariness and 1 patient had to be admitted to hospital for rehydration . 
clinical trials have been frequently performed in patients who had adequate performance status , motivation towards treatment , adequate compliance and who allow continuous monitoring during followup to ensure early and adequate salvage therapy in case of recurrence . 
showed that there was a significant death rate due to comorbid conditions : a consecutive series of 591 patients with advanced head and neck cancer treated by surgery and / or radio ( chemo ) therapy , excluding distant metastases and nasopharyngeal tumors , was analyzed [ 20 ]  . 
previous studies could show that the impact of total tumor volume mainly results from the hypoxic volume and that endogenous markers like hypoxiainducible factor 1 - alpha ( hif - 1alpha ) have the potential to indicate therapeutically relevant levels of hypoxia within tumors [ 16 , 44 ]  . 
these factors have not been taken into account in most of the large radiochemotherapy studies and probably could help to identify subgroups of patients who might have a benefit with regards to distant metastasis - free survival by chemotherapy intensification efforts . 
 altered fractionation regimens like accelerated and hyperfractionated radiation therapy are capable to improve local - regional control in advanced head and neck cancer patients [ 19 ] and may , however , cause a significant increase in acute toxicity [ 20 , 35 ] , which is a particular problem following simultaneous radiochemotherapy . 
cause - specific survival rates of 50% and an actuarial locoregional failure rate of 35% at 5 years showed that cisplatin and 5 - fluorouracil given simultaneously to radiotherapy was an effective treatment approach . 
nevertheless , there is evidence of tumor cell repopulation during a gap with a lag period of at least 2 weeks from the beginning of radiotherapy [ 42 ]  . 
on the other hand , hyperfractionation or moderately accelerated fractionation seem to provide an advantage according to late toxicity : similar to the results of studer et al . , we also observed no case of osteoradionecrosis in the long - term follow - up [ 41 ]  . 
 strahlentherapie und onkologie case study radiotherapy of benign diseases scleredema adultorum buschke stefan knemann1 , stefan hesselmann1 , tobias blling1 , stephan grabbe2 , andreas schuck1 , christos moustakis1 , daniela de simoni1 , normann willich1 , oliver micke1 background : scleredema adultorum buschke is a rare disorder characterized by thickening of the dermis of the neck , head and upper trunk . 
in these cases therapeutic options are poor , with only case reports and small series supporting their use . case report : a 58 - year - old patient with a scleredema of the neck and upper trunk is described , who was treated twice within 6 months by electron - beam radiation therapy . 
a review of the literature of radiation treatment of this disease is given . conclusion : regardless of the possible mechanisms in pathogenesis and treatment of scleredema adultorum buschke , the application of ionizing radiation is an important , effective and well - tolerated therapy option in the treatment of severe cases and may candidate as the first - line treatment of this disease . key words : scleredema adultorum buschke electron - beam radiation therapy radiotherapy of benign diseases strahlenther onkol 2004 ; 180 : 8114 doi 10.1007 / s00066 - 004 - 1286 - 2 radiotherapie gutartiger erkrankungen scleroedema adultorum buschke hintergrund : das skleroedema adultorum buschke ist eine seltene erkrankung , die u.a. 
therapieserien mit kleinen fallzahlen , die einen behandlungsvorteil in der jeweiligen individuellen situation zeigten . fallbericht : beschrieben wird ein 58 - jhriger patient mit sklerdem des nackens und des oberen stammes , der innerhalb von 6 monaten zweimal mittels schneller elektronen bestrahlt wurde . 
eine literaturbersicht ber die behandlung der erkrankung mittels radiotherapie wird gegeben . schlussfolgerung : unabhngig von dem mglichen mechanismus der pathogenese und der therapie der erkrankung stellt die applikation ionisierender strahlung in schwerwiegenden fllen eine wichtige , effektive und gut vertrgliche therapie dar und sollte bei diesen patienten als therapie der ersten wahl diskutiert werden . schlsselwrter : skleroedema adultorum buschke elektronenbestrahlung radiotherapie gutartiger erkrankungen 1 department of radiotherapy , university hospital muenster , muenster , germany , 2 department of dermatology , university hospital muenster , muenster , germany . received : february 20 , 2004 ; accepted : july 23 , 2004 strahlenther onkol 2004 no . 
scleredema adultorum buschke introduction scleredema adultorum buschke is an uncommon scleroderma - like syndrome which predominantly affects young adults and must be differentiated from scleroderma in childhood [ 7 ]  . 
to date , approximately 400 cases have been reported in the literature which have illustrated different aspects of the disease , but the exact etiology , pathogenesis and prognosis remain uncerta clinically , it is characterized by skin thickening and tightening which begins in the cervical region and spreads symmetrically over the upper part of the body . 
several publications describe radiation therapy as an effective treatment option [ 3 , 4 , 20 , 33 ]  . case report in 2001 , a 58 - year - old caucasian male patient with the histologically confirmed diagnosis of scleredema adultorum buschke was referred to the department of radiotherapy radiooncology , university hospital muenster , germany , for treatment . 
the patient had no antecedent febrile illness , but he reported a bite of a tick in the neck 4 years before diagnosis , with following livid skin reactions in this area . 
in april 2001 , the patient was referred to our department for electron - beam radiation therapy . from august 8 until august 21 , 2001 , a fractionated electron radiation therapy was performed with a single posterior portal and an electron energy of 9 mev . 
ct - dokumentation der hautinfiltration ( pfeil )  . a second irradiation course was performed with the same radiation parameters and fractionation scheme from february 18 until march 5 , 2002 . 
to our knowledge , skin induration was unchanged until the patients death due to severe complications after a surgical intervention in march 2003 . discussion nowadays , we observe a renewed interest in the treatment of benign diseases with radiotherapy [ 1 , 11 , 13 , 24 , 2931 ]  . 
the classic type ( type i ) , described by buschke [ 5 ] , follows a febrile infection [ 7 ] often streptococcal or viral , of otorhinolaryngeal or respiratory orig type i has a tendency toward spontaneous yet inconstant resolution in a few weeks or months . 
in these difficult cases many different treatments have been proposed for scleredema , including systemic , topical or intralesional corticosteroids [ 15 ] , thyroid hormones , pituitary extract , high - dose penicillin [ 19 ] , immunosuppressants [ 12 ] , different chemotherapies [ 23 , 28 , 32 ] , antifibrotic therapy , and radiotherapy [ 3 , 4 , 15 , 20 , 22 , 33 ]  . 
cr : komplette remission ; pr : partielle remission . author diagnosis patients ( n ) energy total dose / fraction outcome lichen myxedematosus and squamous cell carcinoma lichen myxedematosus scleredema adultorum buschke hill et al . 
 [ 3 ] report a remarkable functional improvement and stabilization of the illness using electron - beam therapy to a total dose of 20 gy ( 10 2 gy )  . 
 [ 33 ] reported that 2 years after receiving electron - beam therapy twice a week for 36 days ( 20 gy , 2 gy per fraction ) after treatment failure with intralesional and systemic corticosteroids , the patient remained free of disease . 
because of these encouraging results in the literature concerning electron - beam radiation therapy of scleredema adultorum buschke , our patient was also treated with localized electron - beam radiation . 
a review on literature concerning the cases of radiation treatment of scleredema is given in table 1 . the biological effects of ionizing radiation on the pathogenesis of benign diseases [ 13 , 31 ] , especially scleredema adultorum buschke , are still unclear . 
abnormal expression of extracellular matrix genes in skin fibroblasts [ 34 ] as well as increased procollagen production in fibroblast cultures established from the lesional skin [ 26 ] have been observed . 
 if inflammatory mechanisms of normal dermis and subdermal cells or immunocompetent cells are coincident in etiology of this kind of diseases , the anti - inflammatory and anti - proliferative effect of radiation may be one explanation for response to therapy . 
the key to radiation therapys effect in scleredema may also lie in its ability to induce apoptosis in abnormal dermal fibroblasts or otherwise , to interfere with their cell signaling , thereby decreasing collagen and mucin production [ 4 ]  . because of the rare frequency and the extreme heterogeneity [ 16 ] of this family of diseases it will be very difficult to define an individualized experimental radiation treatment concept taking regard of simultaneous or subsequent systemic strahlenther onkol 2004 no . 
however , the therapies clinically applied up to now provide satisfactory results . conclusion in an uncommon disease with such few therapeutic options , regardless of the possible mechanisms in pathogenesis and treatment of scleredema adultorum buschke , the application of ionizing radiation can be considered an important , effective and well - tolerated therapy option . strahlentherapie und onkologie original article postmastectomy radiotherapy of the chest wall comparison of electron - rotation technique and common tangential photon fields thomas hehr1 , johannes classen1 , marco huth1 , ilona durst1 , gunter christ2 , michael bamberg1 , wilfried budach1 background and purpose : different radiotherapy techniques are being used for postmastectomy irradiation . 
a retrospective analysis of patterns of locoregional failure ( lrf ) after modified radical mastectomy and axillary lymph node dissection followed by locoregional radiotherapy with or without systemic treatment was performed . 
 patients and methods : 287 evaluable patients with locally advanced disease and / or adverse pathologic features ( pt3 17% of patients , pt4 35% , multicentricity 25% , pn more than three positive nodes and / or pn1biii 70% , close margins 29% , infiltration of pectoral fascia 20% ) with or without adjuvant chemo - hormonal treatment were included between 1989 and 2000 . 
the median follow - up of patients at risk was 43 months ( average 54 months )  . results : the 5 - year locoregional tumor control ( lrc ) , lrc first event , disease - free , and overall survival were 85% , 91% , 61% , and 70% ( kaplan - meier analysis ) , respectively . 
cox regression analysis showed that stage iii ( relative risk [ rr ] 1.7 ) , more than three involved axillary lymph nodes ( rr 5.1 ) , and infiltration of the pectoral fascia ( rr 3.2 ) increased the risk of locoregional failure , while positive estrogen receptor status ( rr 0.3 ) was associated with a reduced risk . 
 key words : electron - beam - rotation irradiation radiotherapy locally advanced breast cancer mastectomy prognostic and predictive factors strahlenther onkol 2004 ; 180 : 62936 doi 10.1007 / s00066 - 004 - 1264 - 8 einfluss der bestrahlungstechnik der thoraxwand auf die lokoregionre tumorkontrolle des lokal fortgeschrittenen mammakarzinoms nach mastektomie ziel : retrospektiver vergleich zweier bestrahlungstechniken der thoraxwand nach modifizierter radikaler mastektomie und axillrer lymphonodektomie hinsichtlich lokoregionrer tumorkontrolle ( lrc ) beim lokal fortgeschrittenen mammakarzinom . patienten und methodik : von 1989 bis 2000 wurden 287 patientinnen mit lokal fortgeschrittenem mammakarzinom und / oder pathohistologischen risikofaktoren ( pt3 17% der patientinnen , pt4 35% , multizentrizitt 25% , pn mehr als drei positive lymphknoten und / oder pn1biii 70% , knappe resektion [ < 1 cm im gesunden ] 29% , infiltration der faszie des musculus pectoralis 20% ) postoperativ an der thoraxwand entweder mit der tangentialen photonen - gegenfeldoder mit der elektronenrotationstechnik bestrahlt . 
die postoperative strahlentherapie wurde in konventioneller 1 department of radiation oncology , university of tuebingen , tuebingen , germany , 2 department of medical physics , university of tuebingen , tuebingen , germany . received : november 28 , 2003 ; accepted : july 23 , 2004 strahlenther onkol 2004 no . 
in abhngigkeit vom resektionsund lymphknotenstatus erhielten die patientinnen eine lymphabflussbestrahlung mit 50 gy gesamtdosis ( supra - / infraklavikularregion 80% , mammaria - interna - region 60% der patientinnen ) und / oder einen boost des tumorbetts von 10 gy gesamtdosis ( 25% der patientinnen )  . 
die mediane nachbeobachtungszeit betrug 43 monate ( durchschnittlich 54 monate )  . ergebnisse : das aktuarische 5 - jahres - berleben betrug 70% , das krankheitsfreie berleben 61% , die lrc 85% , die lrc first event 91% . 
in der multivariaten cox - regressionsanalyse ( stepwise backward - verfahren ) prognostisch relevant bezglich der lrc waren uicc - stadium iii ( relatives risiko [ rr ] 1 , 7 ) , mehr als drei axillre lymphknotenfiliae ( rr 5 , 1 ) , infiltration des musculus pectoralis ( rr 3 , 2 ) und positiver strogenrezeptorstatus ( rr 0 , 3 )  . 
bei primrtumoren mit durchmessern von 5 cm betrug die lrc nach elektronenrotationsbestrahlung 71% und nach tangentialer photonen - gegenfeldbestrahlung 83% ( p = 0 , 1 )  . schlussfolgerung : die lrc beim lokal fortgeschrittenen mammakarzinom ist nach modifizierter radikaler mastektomie , axillrer lymphonodektomie und radiatio der thoraxwand mit oder ohne lymphabfluss vergleichbar mit ergebnissen aus den randomisierten studien . 
 schlsselwrter : elektronen - bewegungsbestrahlung strahlentherapie lokal fortgeschrittenes mammakarzinom mastektomie prognosefaktoren introduction postmastectomy irradiation of the chest wall markedly reduces the risk of locoregional failure ( lrf ) in advanced breast cancer , defined as t3 tumors ( especially node - positive ) , any t4 tumor , histologically proven positive margins , gross residual disease , more than three positive lymph nodes , or gross extracapsular lymph node involvement [ 3 , 9 , 10 , 13 , 31 , 35 ]  . 
 specifically , three recent trials demonstrated a 9% benefit in survival at 1015 years in patients randomized to comprehensive postmastectomy radiotherapy who also received systemic therapy [ 2426 ]  . 
 although radiation - associated pneumonitis is not commonly reported , the risk of lung damage can limit the choice of irradiation techniques depending on body habitus and in - field lung volumes . 
the risks of cardiac and pulmonary toxicities are highly technique - dependent , so appropriate estimates of these risks could aid in clinical decision - making for selection of the treatment field arrangements . it was thought that electron - rotation irradiation in patients with homogeneous chest wall thickness , in mediolateral and craniocaudal dimension , provides sufficient dose to the chest wall , skin and underlying soft tissue , especially in tumors with lymphangiosis cutis [ 15 , 18 ]  . 
moreover , the scattered dose to the lung and heart could be kept low , by choosing electron energies between 412 mev , depending on minimal chest wall thickness , which , in contrast , might partly spare deep intercostal spaces . 
 the primary goal of this retrospective analysis was to compare two irradiation techniques for the treatment of the postmastectomy chest wall with respect to equivalence in locoregional tumor control ( lrc ) and patterns of lrf in locally advanced breast cancer . 
 patients and methods all records of patients treated between 1989 and 2000 with electron - beam - rotation irradiation or tangential opposed photon fields after modified radical mastectomy with or without adjuvant chemo - hormonal treatment have been reviewed ( table 1 )  . 
287 patients with one or more adverse pathology features pt3 17% , pt4 35% , multicentricity 25% , more than three positive axillary lymph nodes and / or gross extracapsular lymph node involvement 70% , close margins 29% , infiltration of the pectoral fascia 20% were included . 
in tumors with infiltration of the skin , the standard tangential opposed photon fields needed a bolus material , so - called superflab of 0.51.0 cm , to have the full dose at the surface . 
 conventionally fractionated postmastectomy radiotherapy with daily fractions of 1.8 gy five times per week or 2.5 gy four times per week resulting in a median total dose of 50 gy ( range 4656 gy ) to the chest wall was started between 26 and 306 days after surgery ( median 68 days ) ; the course of irradiation was not prolonged for > 5 days . 
the electron - beamrotation technique was designed for treating the whole chest wall ( average chest wall thickness in the range of 1.04.0 cm ) ; patients with a substantial difference of the minimal and maximal thickness of the chest wall after mastectomy received tangential opposed photon fields . 
electron energies between 4 and 10 mev were used , according to the minimal thickness of the chest wall ( skin - surface to lung ) , and the change in contour in the cephalad to caudal dimension , as derived from the planning computed tomography . 
indication for supra - / infraclavicular lymph node irradiation in 80% of patients was gross ( more than three or extracapsular ) lymph node involvement ( median 50.4 gy , range 4455.8 gy total dose ) , and inclusion of the cranial axilla in the supra - / infraclavicular anterior irradiation field depended on the completeness of axillary lymph node dissection . 
in centrally or medially located , lymph node - positive breast cancer , irradiation of the ipsilateral internal mammary lymph nodes was indicated ( 60% of all patients ) , and given by a separate mixed - beam anterior field ( 4to 10 - mev electrons , 19.820 gy total dose , and 6 - mv photons , 27.530.6 gy total dose ) with daily fractions of 1.82.5 gy to a median total dose of 50 gy ( range 4554.4 gy , table 3 )  . 
the distance between isocenter and endframe amounts to 26 cm , so that the rotation with an air gap between endframe and patient skin from 6 cm up to 16 cm is usable . 
the angular addition depends on the width of air gap and was measured in a cylinder phantom of pmma in which also the depth dose curve under rotation and the dose monitor calibration was performed . 
this is especially necessary when an additional parasternal field is provided but is also applied when the desired field length is < 20 cthe thickness of lead rubber is adjusted to the electron energy to ensure slowing table 3 . 
this changes the known depth dose curve of electrons in that way that the skin dose is a little less , the depth of maximum dose is deeper , and therefore the slope of the fall - off is steeper . 
the dose per rotational degree is in contrast to common radiologic thinking increasing with increasing air gap , because any point in the target volume sees radiation from a larger angle range . 
so for each electron energy and each width of air gap ( in steps of 1 cm ) a table of monitor units per rotational degree for a prescribed dose is used to calculate monitor units . 
at the time of analysis , median follow - up of all patients from the start of radiotherapy was 40 months ( average 51 months , range 2148 months ) , the median follow - up of patients at risk was 43 months ( average 54 months )  . 
the parameters uicc stage < / iii , n - stage ( more than three involved axillary lymph nodes ) , maximum tumor diameter ( < / 5 cm ) , resection status ( < / close margins ) , infiltration of the pectoral fascia , lymphangiosis cutis ( histopathology ) , estrogen receptor ( er ) status , histopathologic tumor grading ( < / giibiii ) , multicentricity , and irradiation technique ( electron - beam - rotation irradiation / tangential opposed 6 - mv photon fields ) were tested . 
all parameters with a univariate p - value 0.05 were taken into consideration for the multivariate cox regression model , and a stepwise backward procedure was used to identify independent significant parameters for lrc . 
the level of significance locoregional tumor control first event electron - rotation irradiation photon - based irradiation 108 120 132 144 156 time from start of treatment ( months ) figure 1 . 
 results the 5 - year local tumor control rate , the local tumor control rate first event ( local failure without preceding distant metastasis ) , the disease - free survival rate , and the overall survival rate were 85% ( standard error 3% ) , 91% ( 2% ) , 61% ( 3% ) , and 70% ( 3% ) , respectively . 
in the multivariate analysis ( cox regression analysis ) of all patients stage iii ( relative risk [ rr ] 1.7 ) , more than three involved axillary lymph nodes ( rr 5.1 ) and infiltration of the pectoral fascia ( rr 3.2 ) were independent predictors of inferior lrc , while positive er status ( rr 0.3 ) predicted long - term lrc . 
 overall , the comparison of the two different irradiation techniques of the chest wall did not reveal significant differences in lrc for patients treated either with the electron - rotation technique ( 5 - year lrc 92% ) or with the photon - based technique ( lrc 89% ; p = 0.9 ; figure 1 )  . 
however , in a subgroup of patients whose tumors were resected with close margins , a statistically significant increase in lrf rates of 25% at 5 years was observed with the electron - beam - rotation technique , whereas the lrf with tangential opposed 6 - mv photon fields was 13% ( p < 0.05 ; figure 2 )  . 
postmastectomy radiotherapy of the chest wall in locally advanced breast cancer tumors with lymphangiosis cutis / infiltrated skin ( n = 71 , lrf at 5 years 26% 6% ) , with peritumoral lymphangiosis ( n = 155 , lrf 17% 4% ) , or with infiltration of the pectoral fascia ( n = 57 , 27% 7% )  . 
the latest follow - up of patients without local recurrence revealed an inconspicuous chest wall in 65% of patients , persistent pigmentation in 19% , telangiectasia in 7% , and late normal tissue estimates were missing in 4% . 
there is no agreement as to the question of an adequate or optimal radiotherapy regimen for postmastectomy radiotherapy , as stated in the asco guidelines [ 31 ]  . this retrospective report assessed the clinical equivalence of two postmastectomy radiotherapy techniques with regard to lrc and treatment - related toxicities . 
applying these endpoints , the use of either electron - beam - rotation technique or tangential opposed photon fields for the treatment of the chest wall yielded equivalent 5 - year results , with a long - term lrc rate of 91% ( first event )  . 
the lrc in our patient population is comparable to the results reported from randomized trials of chest wall irradiation with or without adjuvant systemic therapy ( long - term lrc in the range of 8196% ) [ 7 , 5 - year locoregional tumor control photon - based irradiation electron - rotation irradiation 75% , p < 0.05 108 120 132 144 156 time from start of treatment ( months ) figure 2 . 
 reported that the relative effectiveness of photonand electron - based postoperative treatment schemes was similar in the only ( retrospective ) study comparing the two techniques [ 1 ]  . 
their multivariate analysis of 55 patients with locally advanced breast cancer revealed no differences in local tumor control due to the interval between surgery and irradiation , technique of irradiation , or irradiation modality . three - dimensional treatment planning allows to compare different irradiation techniques for the treatment of the postmastectomy chest wall and regional lymph nodes with respect to coverage of the target volume and to estimate the risk of radiation - associated pneumonitis or heart disease ( figure 3 )  . 
stated , that with most of the common techniques it was not possible to achieve adequate dose coverage of the chest wall and lymph nodes and optimal sparing of lung and heart at the same time , and that , therefore , the choice of technique should be based on clinical discretion and the technical expertise available to implement these complex plans . 
 of the seven techniques studied , their analysis supported partial wide tangential fields as the most appropriate balance of target coverage and normal tissue sparing when irradiating the chest wall and internal mammary lymph nodes [ 27 ]  . 
 in retrospective and prospective trials prognostic factors for poor local tumor control after mastectomy have been confirmed : axillary lymph node involvement , large primary tumor , skin involvement , high histopathologic grade , incomplete tumor resection , and local recurrence . 
postmastectomy radiotherapy of the chest wall in locally advanced breast cancer even with postmastectomy radiotherapy [ 7 , 14 , 16 , 18 , 25 , 26 , 28 , 34 , 3739 ]  . 
 furthermore , the rate of supraclavicular and especially internal mammary irradiation ( table 3 ) was higher in the group of patients who received the electron - beam - rotation technique . 
this potentially reflects a selection bias due to match line problems , e.g. , use of the hanging block technique or dose inhomogeneities between the tangential chest wall fields and an anterior internal mammary artery field . 
a careful interpretation of these findings should consider that the group of patients treated with the photon - based technique had comparable tand n - stage classifications to the group of patients treated with the electron - based technique , but the rates of lymphangiosis cutis , infiltration of the pectoral fascia , or negative er status were markedly higher in the latter group . 
with regard to the irradiation technique , the local control rates at 5 years in tumors with lymphangiosis cutis / skin involvement of 74% , with peritumoral lymphangiosis of 83% , or with infiltration of the pectoral fascia of 73% were not significantly different . univariate analysis of lrc in the total patient population confirmed former findings in patients with more than one negative prognostic factor in addition to the tand n - stage categories . 
locally advanced tumors exhibiting negative er status and poor differentiation grade , had a 30% lrf rate at 5 years after irradiation compared to 6% recurrences in tumors exhibiting none of these risk factors [ 15 ]  . radiation pneumonitis develops in the first few months after radiotherapy and is characterized by a chronic cough , fever , and nonspecific infiltrate on chest x - ray . 
both the combined use of chemoand radiotherapy , irradiation technique ( which affects the volume of lung treated ) , and the drugs used may be important in determining this effect . 
these data compare favorably with the reported rate of 3% radiation - induced pneumonitis in our group of patients receiving photon - based therapy of the chest wall plus mixedbeam irradiation of the internal mammary lymph nodes . 
however , the rate of 9% ( 15 / 172 patients ; p = 0.055 ) symptomatic pneumonitis with the electron - beam - rotation technique seems to be higher than expected . 
this irradiation technique was designed for treating the whole chest wall and electron energies between 4 and 15 mev were used , according to the minimal thickness of the chest wall ( skin - surface to lung )  . 
higher incidences of symptomatic radiation pneumonitis have also been reported in series in which a photon hockey - stick field was used to treat the internal mammary lymph nodes concurrently with chemotherapy [ 2 ]  . 
in our series , no correlation of the incidence of symptomatic pneumonitis was found using or not using sequential chemotherapy , or irradiating or not irradiating the regional figure 3 . 
the electron - beam - rotation irradiation of the chest wall seems to be less effective due to lrc after marginal resection ( histopathologic close margins ) compared to tangential opposed 6 - mv photon fields , and the electron - based therapy incorporates a trend to an increased symptomatic pneumonitis rate , but a negative patient selection bias ( higher rate of negative prognostiv factors ) has to be considered . strahlentherapie und onkologie original article po2 polarography versus positron emission tomography ( [ 18f ] fluoromisonidazole , [ 18f ] - 2 - fluoro - 2 ' - deoxyglucose ) an appraisal of radiotherapeutically relevant hypoxia bernd gagel1 , patrick reinartz2 , ercole dimartino3 , michael zimny2 , michael pinkawa1 , payam maneschi1 , sven stanzel4 , kurt hamacher5 , heinz h . 
 eine bewertung der strahlentherapeutisch relevanten hypoxie hintergrund und ziel : ziel dieser untersuchung war die validierung von [ 18f ] - fluormisonidazol - ( fmiso - ) und [ 18f ] - fluordeoxyglucose - ( fdg - ) positronenemissionstomographie ( pet ) zur erfassung der strahlentherapeutisch relevanten hypoxie durch das computergesttzte polarographische nadelelektrodensystem ( po2 - histographie ) , das den goldstandard zur festlegung der gewebeoxygenierung in menschlichen tumoren darstellt . patienten und methodik : bis jetzt wurden bei insgesamt 16 patienten mit metastatisch befallenen halslymphknoten eines plattenepithelkarzinoms der kopf - hals - region po2und pet - messungen durchgefhrt . 
die nadelelektrode wurde ct - gesteuert ohne 1 department of radiotherapy , university of aachen , aachen , germany , 2 department of nuclear medicine , university of aachen , aachen , germany , 3 department of otorhinolaryngology , university of aachen , aachen , germany , 4 institute for medical statistics , university of aachen , aachen , germany , 5 institute for nuclear chemistry , nuclear research center , jlich , germany . received : september 16 , 2003 ; accepted : march 25 , 2004 strahlenther onkol 2004 no . 
unter verwendung eines ganzkrperprotokolls mit einer emissionsmessung von 8 min und einer transmissionsmessung von 4 min pro bettposition durchgefhrt . ergebnisse : um mgliche korrelationen zwischen den verschiedenen relevanten , polarographisch gemessenen parametern der tumorhypoxie und den mittels fmiso - pet gewonnenen messdaten zu detektieren , wurde der pearson - korrelationskoeffizient berechnet . 
es zeigte sich eine mittlere ( r > 0 , 5 ) bis hohe korrelation ( r > 0 , 7 ) zwischen dem tumor / muskel - quotienten der fmisoaufnahme 2 h p.i. 
und den verschiedenen hypoxieparametern ( po2 - messwerte 2 , 5 , 5 , 0 , 10 , 0 mmhg sowie mittelwert und median der po2 - messwerte )  . 
keine korrelation konnte zwischen den fdg - pet - parametern und dem polarographisch bestimmten tumoroxygenierungsstatus aufgezeigt werden . schlussfolgerung : die mit pet gemessene fmiso - aufnahme gibt einen globalisierten messwert fr makroskopische anteile des tumors wieder . 
in addition , the hypoxic fraction in solid tumors also reduces their sensitivity to conventional treatment modalities modulating response to ionizing radiation or certain chemotherapeutic agents [ 9 , 19 ]  . 
for example , an approximately twice to three times higher radiation dose is necessary to kill hypoxic cells , compared to well - oxygenated cells [ 5 , 6 ]  . the computerized polarographic needle electrode system ( po2 histography ) has been suggested as gold standard for measuring tissue oxygenation in human malignancies [ 23 ]  . 
 however , it represents an invasive method being confined to superficial , well - accessible tumors or metastatic lymph nodes . with positron emission tomography ( pet ) , radiolabeled hypoxia - avid compounds can be applied to evaluate oxygenation status in experimental or human tumors [ 3 ]  . 
because of the fact that only seven patients were treated by primary radio - / chemotherapy , an analysis of radiosensitivity due to tumor hypoxia or tumor extension was not done . 
 the distances between the measurement points were 0.7 mm including an automatic probe movement of 1.0 mm forward and 0.3 mm backward to minimize compression effects caused by the forward motion of the needle electrode . 
the tumor was defined according to the image data of fdg pet . mean and maximum standardized uptake values ( suvs ) of the fmiso and fdg uptake of the tumor were calculated after normalization of the radioactivity concentration to the injected radioactivity and the body weight . 
additionally , the mean suv was corrected for partial volume effects by applying recovery coefficients obtained from phantom studies [ 26 ]  . statistical methods data are given as means with corresponding 95% cis for the mean as well as range . 
the scatter plots in figure 2 reflect the relationship between different parameters of polarographically measured tumor oxygenation and tumor - to - muscle ratio of fmiso as a parameter of tumor hypoxia . 
 however , the enhanced binding of nitroimidazoles is related to the hepatic metabolism of the drug [ 16 ] as well as to the fact that liver functions at a significant lower tissue po2 than other normally oxygenated tissues [ 13 ]  . 
fdg : [ 18f ] - 2 - fluoro - 2 ' - deoxyglucose ; fmiso : [ 18f ] fluoromisonidazole ; pet : positron emission tomography ; suv : standardized uptake value . 
po2 polarography versus pet ( fmiso , fdg ) : an appraisal of radiotherapeutically relevant hypoxia cell were counted reflecting low binding of 3h - miso in the outer sandwich cells which are near the oxygen and nutrient source , in contrast to heavy binding in interior sandwich cells bordering the necrotic center representing radiobiological hypoxia . 
these facts suggest that miso binding is proportional to cell size and cells in the inner noncycling portion are more nearly uniform in size , being still viable if restored to good nutrient and oxygen conditions . 
found an accumulation of miso next to necrosis but describing an on - off phenomenon and no inverse relationship of miso uptake to decreased polarographically measured po2 [ 15 ]  . 
these results taken together still put in question whether fmiso uptake allows to detect hypoxic therapy resistance in any given human tumor , and so far , no patient data exist . 
graphische darstellung der abhngigkeiten zwischen der polarographischen und mit hilfe der fmiso - pet ( tumor / muskel - quotient ) bestimmten oxygenierung in halslymphknotenmetastasen ( n = 16 )  . 
showed that the tumor uptake of fmiso was constant between 30 min and 2 h and that the tumor - to - blood and tumor - to - muscle fmiso uptake ratios were stable 24 h after injection using rats with ah109a tumors suggesting some retention mechanisms of fmiso within the tumor but not within any normal tissue [ 11 ]  . 
this problem of value distribution is also reflected by the correlations between the different parameters of polarographic po2 measurements showing only moderate correlations between the fraction of po2 values 2.5 mmhg and the mean or median po2 ( figure 1 )  . 
whereas , at present , the target volume is characterized by the concepts of gross tumor volume ( gtv ) , clinical target volume ( ctv ) , and planning target volume ( ptv ) , biological images as shown in figure 3 may provide information for defining a biological target volume ( btv ) to improve dose targeting to certain regions of target volume . 
nevertheless , additional patient data is required for a better validation of this method by the well - established po2 polarography resulting in regression curves that allow prediction of tissue po2 with satisfactory accuracy . strahlentherapie und onkologie original article radiation - induced plexopathy and fibrosis is magnetic resonance imaging the adequate diagnostic tool ? ulrike hoeller1 , michael bonacker2 , amira bajrovic1 , winfried alberti1 , gustav adam2 purpose : to investigate magnetic resonance imaging ( mri ) features of radiation - induced plexopathy ( rip ) and radiation - induced fibrosis frequently associated with rip . 
 patients and methods : seven patients with late radiation sequelae in the supraclavicular region were examined with mri after a median interval of 7 years ( range , 518 years ) following radiotherapy and 47 years after the onset of rip . 
four patients had rip plus severe soft - tissue fibrosis , two rip without soft - tissue fibrosis ( n = 2 / 6 ) , and one patient fibrosis without rip . 
mri was performed with a 1.5 - t unit including coronal stir , coronal and transversal t2 - weighted , transversal t1 - weighted and fat - saturated post - contrast ( gadolinium - dtpa ) spin echo sequences . results : the brachial plexus appeared normal in all patients , but subtle changes of adjoining tissue ( slight , linear signal intensity in t2 - weighted images or contrast enhancement surrounding the plexus ) were detected in patients with rip ( n = 4 / 6 ) and the patient without rip ( n = 1 )  . 
however , alterations of the soft tissue ( marked signal intensity in t2 - weighted sequences ) correlated well with the clinical degree of fibrosis and were restricted to areas of marked to severe fibrosis ( n = 3 / 3 )  . conclusion : reliable mri signs of rip could not be identified . 
the role of mri in the diagnostic work - up of rip is , therefore , the exclusion of tumor relapse . key words : mri radiation - induced plexopathy fibrosis breast cancer strahlenther onkol 2004 ; 180 : 6504 doi 10.1007 / s00066 - 004 - 1240 - 3 radiogene plexopathie und fibrose . 
ist die magnetresonanztomographie das verfahren der wahl ? ziel : die darstellung der radiogenen schdigung des plexus brachialis ( rp ) und der hufig mit der rp assoziierten weichteilfibrose mit der magnetresonanztomographie ( mrt ) wurde untersucht . patienten und methodik : sieben patientinnen mit ausgeprgten strahlenreaktionen in der supraklavikularregion wurden median 7 jahre nach therapie untersucht . 
nach exzision eines brustwandrezidivs ( n = 1 ) wurde die supraklavikularregion mit 60co in einzeldosen von 1 , 72 , 6 gy bis zu einer gesamtdosis von 4351 , 6 gy in 3 cm tiefe bestrahlt . 
 die mrt - untersuchung wurde an einem 1 , 5 - t - gert mit koronaren und transversalen t2 - gewichteten sequenzen , koronaren stir , transversalen t1 - gewichteten sequenzen und fettgesttigten spinechosequenzen nach kontrastmittelgabe ( gadolinium - dtpa ) durchgefhrt . ergebnisse : der plexus brachialis selbst stellte sich unauffllig dar , aber die perineuralen strukturen zeigten eine geringe lineare hyperintensitt in der t2 - gewichteten sequenz oder nach kontrastmittelgabe ( n = 4 / 6 )  . 
dagegen korrelierte die klinisch miggradige und ausgeprgte fibrose gut mit einer hyperintensitt des fettund bindegewebes in den t2 - gewichteten sequenzen ( n = 3 / 3 )  . schlussfolgerung : zuverlssige kriterien einer rp wurden nicht gefunden . 
 schlsselwrter : mrt radiogene plexopathie fibrose mammakarzinom 1 department of radiotherapy and radiooncology , center of radiology , university hospital eppendorf , hamburg , germany , 2 department of diagnostic and interventional radiology , center of radiology , university hospital eppendorf , hamburg , germany . received : october 20 , 2003 ; accepted : april 29 , 2004 strahlenther onkol 2004 no . 
the appearance of fibrosis in mri varies widely from low to highly reduced signal intensity and post - contrast enhancement [ 1 , 3 , 9 , 13 , 21 ]  . 
 brachial plexus was considered normal if it appeared as linear structures of low signal intensity similar to that of muscle surrounded by fat on all sequences [ 15 ]  . 
 results the clinical examination revealed mild to moderate soft - tissue fibrosis of the supraclavicular fossa in four patients including the upper axilla in three ( table 2 )  . 
however , subtle changes of the adjacent tissue were noted in four patients : slight and linear signal intensity in t2 - weighted images and stir was observed in three cases and interpreted as edema . 
 magnetic resonance imaging of soft tissue the alterations of the soft tissue were much more impressive and correlated well with the clinical degree of fibrosis of the patients and methods from june 1999 to july 2000 , six patients with rip and one patient with radiation - induced fibrosis were evaluated with mri . 
in a follow - up study of breast carcinoma patients treated to the supraclavicular region , six of 16 patients with rip and one of 21 patients with fibrosis consented to mri . four patients had mastectomy and three patients breastconserving surgery . 
adjuvant radiotherapy was given to the intact breast or thoracic wall in five patients with cobalt or 6 - mv photons to 5060 gy total reference dose ( table 1 )  . 
the median interval from radiotherapy to mri was 7 years ( range , 518 years ) , the interval from mri to the onset of rip ranged from 4 to 7 years . 
we acquired coronal stir ( fat - suppressed inverted t1 ) , coronal and transversal t2 - weighted , transversal t1 - weighted and fat - saturated post - contrast ( gadolinium dtpa ) spin echo sequences with a slice thickness of 46 m mri was evaluated by a radiologist ( mb ) blinded to the severity of clinical symptoms . 
 patient clinical late radiation effecta : rip fibrosis supraclavicular axilla fossa fibrosis mri findings : brachial plexus supraclavicular soft tissue axillary soft tissue extensive signal intensity ( edema ) extensive signal intensity ( edema ) ( stir ) , distorted and close structures ( fibrosis ) marked signal intensity , post - contrast enhancement post - contrast enhancement ( spin echo sequence ) marked signal intensity ( edema ) , no enhancement ( t2 ) marked signal intensity , ( spin echo sequence ) slightly distorted surrounded by slight signal intensity ( t2 , stir ; edema ) surrounded by slight linear slight signal intensity ( edema ) and contrast signal intensity ( t2 , stir ; enhancement ( t2 ) edema ) surrounded by slight linear post - contrast enhancement ( fat - saturated sequence only ) surrounded by slight linear signal intensity ( t2 , stir ; edema ) a 0 : none , 1 : mild , 2 : moderate , 3 : marked , 4 : severe b high signal intensity in bursa deltoidea / shoulder joint capsule interpreted as inflammatory exudation supraclavicular fossa and axilla . 
marked signal intensity in t2weighted sequences and stir was restricted to the only three regions of clinically marked to severe ( grade 23 ) fibrosis and was described as edema by mri criteria ( figures 1 and 2 )  . 
 discussion rip is a rare but severe complication of radiation therapy that results from direct neurotoxic effects of irradiation and / or secondary effects on regional vasculature ( vasa vasculature )  . 
 in studies on dogs nerves and autopsy studies , the principal histological lesion was loss of large nerve fibers and fibrosis of the epineurium without significant vascular injury [ 10 , 17 ]  . 
 case studies in humans and experimental studies found vascular lesions consisting of necrosis and hyalinization of the media of small arteries and extensive thickening of epiand perineurium [ 2 , 8 , 13 ]  . 
fibrotic lesions contain infiltrating inflammatory cells , fibroblasts and large amounts of various extracellular matrix components [ 16 ]  . if patients present with brachial plexopathy after treatment for breast cancer , mri is performed to distinguish rip and / or fibrosis from local relapse [ 3 , 11 , 13 ]  . 
mri showed swelling of the plexus and hyperintensity within the trunks on t2 - weighted images [ 21 ] , diffuse infiltration and slight hyperintensity ( t2 - weighted images ) of the brachial plexus [ 15 ] , or replacement of perineural fat by structures with a low signal intensity on both t1and t2 - weighted images [ 21 ]  . 
rip was not distinguished from fibrosis . in our study of patients with a similar long - term surveillance period after radiotherapy and onset of rip , the previously reported features were not observed , but in four of seven patients , increased perineural signal intensity on t2 - weighted images or contrast enhancement was detected . 
by comparison , in a study of patients with rip or tumor - associated plexopathy , increased t2 signals adjacent to or , rarely , in the brachial plexus and a loss of fat planes was found in the majority of patients ( 17 / 21 rip , 25 / 42 tumor plexopathies without and 14 / 19 with previous radiotherapy ) [ 19 ]  . 
interestingly , this phenomenon did not discriminate tumor from rip and was present in irradiated and nonirradiated patients as well , suggesting a correlation with plexopathy itself . radiation - induced fibrosis of supraclavicular and axillary soft tissues was described in a significant number of patients as a reduction of signal intensity of the fat in t1and t2 - weighted sequences , often resulting in a loss of clarity strahlenther onkol 2004 no . 
 two explanations were offered : either enhancement by microscopic fibrosis or a persistent vasculative leak related to radiotherapy [ 14 ]  . in our study group , there was a striking correlation of mri features and the severity of fibrosis . 
all areas of clinically moderate to marked fibrosis corresponded with increased signal intensity ( t2 - weighted sequence and stir ) and , in two cases , with post - contrast enhancement . 
a similar close correlation of severity of clinical induration and increased signals on stir images and post - contrast enhancement was found after radiotherapy of the breast [ 14 ]  . conclusion reliable mri signs of rip could not be identified in this study . 
mri in the diagnosis of radiation - induced plexopathy strahlentherapie und onkologie current discussion impact of hypoxia and the metabolic microenvironment on radiotherapy of solid tumors introduction of a multiinstitutional research project daniel zips1 , markus adam2 , michael flentje3 , axel haase4 , michael molls2 , wolfgang mueller - klieser5 , cordula petersen1 , christine philbrook2 , peter schmitt4 , oliver thews5 , stefan walenta5 , michael baumann1 , 6 background : recent developments in imaging technology and tumor biology have led to new techniques to detect hypoxia and related alterations of the metabolic microenvironment in tumors . 
however , whether these new methods can predict radiobiological hypoxia and outcome after fractionated radiotherapy still awaits experimental evaluation . material and methods : the present article will introduce a multiinstitutional research project addressing the impact of hypoxia and the metabolic microenvironment on radiotherapy of solid tumors . 
the four laboratories involved are situated at the universities of dresden , mainz , munich and wrzburg , germany . results : the joint scientific project started to collect data obtained on a set of ten different human tumor xenografts growing in nude mice by applying various imaging techniques to detect tumor hypoxia and related parameters of the metabolic microenvironment . 
these techniques include magnetic resonance imaging and spectroscopy , metabolic mapping with quantitative bioluminescence and single - photon imaging , histological multiparameter analysis of biochemical hypoxia , perfusion and vasculature , and immunohistochemistry of factors related to angiogenesis , invasion and metastasis . 
to evaluate the different methods , baseline functional radiobiological data including radiobiological hypoxic fraction and outcome after fractionated irradiation will be determined . conclusion : besides increasing our understanding of tumor biology , the project will focus on new , clinically applicable strategies for microenvironment profiling and will help to identify those patients that might benefit from targeted interventions to improve tumor oxygenation . key words : hypoxia microenvironment fractionated radiotherapy tumor xenografts strahlenther onkol 2004 ; 180 : 60915 doi 10.1007 / s00066 - 004 - 1285 - 3 bedeutung der hypoxie und des metabolischen mikromilieus fr die strahlentherapie solider tumoren . 
die experimentelle evaluierung , inwieweit diese methoden mit der radiobiologischen hypoxie und dem ergebnis der fraktionierten bestrahlung korrelieren , steht bislang aus . material und methodik : im vorliegenden artikel wird ein multiinstitutionelles forschungsprojekt zwischen arbeitsgruppen an den universitten in dresden , mainz , mnchen und wrzburg zur bedeutung der hypoxie und des metabolischen mikromilieus fr die strahlentherapie solider tumoren vorgestellt . ergebnisse : im gemeinsamen forschungsprojekt werden an zehn verschiedenen humanen tumorxenografts in der nacktmaus unterschiedliche methoden zur darstellung und quantifizierung der hypoxie und von parametern des metabolischen mikromilieus angewandt . 
diese methoden umfassen die magnetresonanztomographie und - spektroskopie , die histographische darstellung metabolischer parameter mittels quantitativer biolumineszenz , die multiparametrische analyse von biochemischer hypoxie , perfusion und gefnetz sowie immunhistochemische untersuchung von faktoren , die bei der angiogenese , invasion und metastasierung eine 1 department of radiotherapy and radiation oncology , medical faculty , university of technology , dresden , germany , 2 department of radiotherapy and radiation oncology , technical university of munich , munich , germany , 3 department of radiotherapy , university of wrzburg , wrzburg , germany , 4 department of experimental physics v , university of wrzburg , wrzburg , germany , 5 institute of physiology and pathophysiology , university of mainz , mainz , germany , 6 experimental center , medical faculty , university of technology , dresden , germany . received : february 17 , 2004 ; accepted : july 1 , 2004 strahlenther onkol 2004 no . 
diese sollen helfen , jene patienten herauszufinden , die von einer gezielten verbesserung der tumoroxygenierung profitieren . schlsselwrter : hypoxie mikromilieu fraktionierte strahlentherapie tumorxenografts introduction viable tumor cells within areas of insufficient oxygen and nutrient supply are characteristic of solid tumors . 
clinical data demonstrate that hypoxic clonogenic tumor cells and their potential to reoxygenate are important for the outcome after fractionated radiotherapy [ 1719 , 23 , 35 , 48 , 60 , 61 , 67 ]  . 
besides the effect of oxygen on radiation sensitivity , tumor hypoxia and related parameters of the metabolic microenvironment are associated with increased malignant progression , metastatic potential and therapy resistance by clonal selection , increased genetic instability and alterations of gene expression , translation or posttranslational processes [ 13 , 19 , 51 , 60 , 68 ]  . the radiobiological hypoxic fraction ( rhf ) , that is the proportion of severely hypoxic and therefore radioresistant tumor cells , can be determined by tumor control experiments , tumor growth delay assays and by the paired - survival curve test [ 21 , 43 ]  . 
all assays are based on the comparison of results obtained after irradiation either under artificial , homogeneous hypoxia ( using a clamp to block tumor perfusion ) or under normal blood flow conditions . 
the tumor control assay is the most relevant method to determine the rhf , because the tumor cells remain in their irradiated environment during follow - up , whereas with the paired - survival curve test tumor cells are transferred after in vivo irradiation to cell culture dishes [ 3 , 25 , 57 , 70 ]  . 
in contrast to the growth delay assay , using the tumor control as an experimental endpoint allows the measurement of very small proportions of hypoxic clonogenic cells within the tumor . 
animal studies on murine and human tumors revealed a considerable heterogeneity of rhf between different models [ 3 , 22 , 26 , 4143 , 49 , 56 , 58 ]  . 
it is unclear , whether the rhf in untreated tumors is of prognostic value for the outcome after fractionated irradiation , which also depends on other parameters such as number of clonogenic tumor cells and their intrinsic sensitivity , recovery from sublethal damage , repopulation , reoxygenation , and cell cycle distribution . unfortunately , none of the radiobiological methods to measure rhf are applicable to tumors in patients . 
during the last years , great efforts were undertaken to develop methods to quantify hypoxia and the metabolic microenvironment in clinical tumors [ 8 , 10 , 28 , 30 , 37 ]  . 
these techniques include po2 histography , magnetic resonance imaging ( mri ) and spectroscopy ( mrs ) , positron emission tomography ( pet ) , metabolic mapping with bioluminescence imaging , application of endogenous and exogenous hypoxia markers , and expression analysis of hypoxia - induced genes . 
establishing potentially clinically applicable methods to quantify hypoxia and the metabolic microenvironment in tumors and evaluating whether or not these techniques can predict rhf , is of great importance for radiation oncology . 
such interventions would include breathing high oxygen - content gas mixtures and application of hypoxic cell radiosensitizers . aim of the multiinstitutional research project the object of the joint research project , launched in 2003 and funded by the deutsche forschungsgemeinschaft , is to apply different methods to measure hypoxia and parameters of the metabolic microenvironment in different human squamous cell carcinoma lines growing subcutaneously in nude mice . 
all four groups will not only be able to use the same tumor models , but also to apply their methods to samples from the same tumor or even to the same tumor cross section ( figure 1 )  . 
10 urban & vogel tumor - bearing animals tumors after mri wrzburg : mri and mrs oxygenation , ph , lactate , perfusion d atabas e tumors after mri zips d , et al . 
hypoxia and microenvironment in radiotherapy of solid tumors in the following sections the different techniques to measure tumor hypoxia and parameters of the microenvironment that will be applied in the joint research project will shortly be described . 
 high - resolution magnetic resonance imaging and spectroscopy dresden : radiobiological hypoxic fraction , fractionated irradiation , multiparameter analysis of hypoxia , perfusion and vasculature tumor samples recent developments in mri and mrs have led to techniques that include high spatial resolution and functional imaging of vasculature and microenvironment in tumors . 
these methods have been incorporated into experimental and clinical investigations to assess information about oxygenation , vasculature , perfusion , ph , and metabolites [ 12 , 36 , 40 , 53 , 59 ]  . 
the protocol will include quantification of the oxygenation - related parameter r2 * while tumor - bearing animals breath air or carbogen ( see figure 2 for results obtained at 2 t ) , spin - labeling and contrast media - enhanced techniques to investigate microcirculation and 1h - mrs for assessment of extracellular ph and metabolites such as lactate . 
it is important to note that the evaluamunich : analysis of vegf and the plasminogen activation system mainz : metabolic mapping with bioluminescence imaging , endogenous hypoxia markers tumor samples figure 1 . 
 tion of all mri and mrs techniques will be done on the same different human squamous cell carcinoma xenografts that are used in all other parts of the joint research project . 
histological hematoxylin - eosin - ( he - ) stained section ( a ) and relative change of the oxygenation - related mr parameter r2 * when the breathing gas is switched from air to carbogen ( b )  . 
histologischer hmatoxylin - eosin - ( he - ) gefrbter schnitt ( a ) und relative nderung des oxygenierungsabhngigen mr - parameters r2 * bei umstellung des atemgases von luft auf carbogen ( b )  . 
hypoxia and microenvironment in radiotherapy of solid tumors glucose and lactate have led to metabolic mapping of histological tumor samples , a method that has been developed at the mainz laboratory ( see figure 3 ) [ 3133 ]  . 
clinical investigations utilizing this method revealed that a high lactate level in the primary lesion is associated with a high risk of metastasis and poor outcome [ 6 , 50 , 6365 ]  . 
mapping of glucose metabolism and expression analysis of glycolytic enzymes combined with detection of hypoxia - related markers , e.g. , hif - 1 and carboanhydrase 9 , will be performed on serial cross sections from the human squamous cell carcinomas . 
besides correlation with the radiobiological baseline data , co - localization studies will include images from the same individual tumor generated either by other histological methods ( see below ) or mri and mrs . 
serial cryosections of one biopsy were used for staining of the tissue structure ( he : hematoxylin and eosin ; cytokeratin : staining of epithelial tumor tissue ) and for quantitative imaging of the metabolite distribution ( pseudocolor - calibrated : atp , lactate , glucose )  . 
serielle kryoschnitte der biopsie wurden fr strukturfrbungen ( he : hmatoxylin - eosin ; cytokeratin : darstellung epithelialen tumorgewebes ) und fr die quantitative darstellung der metabolitverteilung ( falschfarbenkalibriert : atp , lactat , glukose ) verwendet . 
 sults from mr investigations can be correlated not only with radiobiological functional data but also with data obtained by histological methods , e.g. , by comparison of lactate levels and distribution assessed by both mrs and quantitative bioluminescence ( see below )  . 
 bioluminescence imaging of glucose metabolism and intrinsic hypoxia markers in tumors malignant cells exhibit an increased glycolytic flux caused by an overexpression of glucose transporters such as glut - 1 and enzymes that are involved in the glycolytic pathway , e.g. , lactate dehydrogenase ( ldh ) and phosphofructokinase ( pfk - 1 ) [ 9 , 52 ]  . 
the transcription factor hif - 1 is upregulated under hypoxic conditions and plays an important role in the overexpression of glucose transporters and glycolytic enzymes [ 52 , 66 ]  . 
quantitative bioluminescence imaging - based measurements of levels of adenosine triphosphate ( atp ) , multiparameter analysis of hypoxia , perfusion and vasculature in tumor sections fluorescence microscopy coupled with automated quantitative image analysis offers the possibility to detect and quantify biochemical hypoxic tumor cells , perfusion and vasculature in the same whole - tumor cross section ( see figure 4 ) [ 7 , 38 , 39 , 62 , 70 ]  . 
a standardized protocol to detect biochemical hypoxic tumor cells after injection of the exogenous hypoxic marker pimonidazole to the tumor - bearing animals adapted from a protocol originally developed at the university of nijmegen [ 39 ] has been established in the dresden laboratory [ 70 ]  . 
whereas the immunohistochemical hypoxic fraction , as determined by pimonidazole binding , correlated with rhf when oxygenation was manipulated in a murine tumor system [ 37 ] , no correlation was found comparing four different human melanoma xenografts [ 44 ]  . 
hypoxia and microenvironment in radiotherapy of solid tumors analysis of plasminogen activation system and vascular endothelial growth factor expression in tumors the plasminogen activation system ( pas ) , a family of proteases including upar , pai - 1 and upa , as well as the vascular endothelial growth factor ( vegf ) , both play a key role in tumor angiogenesis , invasion and metastasis [ 1 , 27 , 46 ]  . 
in a previous investigation , the munich group was able to relate the increase in hypoxic subvolume to a worse prognosis in patients with head and neck cancer [ 54 ]  . 
 retrospective investigations on tumor samples show that pas and vegf are overexpressed in tumors and might be related to clinical prognosis [ 2 , 5 , 34 , 47 ]  . 
in fact , the munich laboratory has previously shown a definite increase in the expression of upa and pai - 1 in hypoxic tumors of patients with squamous cell carcinomas [ 55 ]  . 
these comparisons will provide new insights into the complex interactions of vegf , pas and hypoxia and their role in tumor response to radiotherapy . outlook recent developments in imaging technology and tumor biology have led to advanced , sophisticated methods to detect tumor hypoxia and related parameters of the metabolic microenvironment in patients . 
considering these aspects , a multiinstitutional research project , funded by the deutsche forschungsgemeinschaft , between four laboratories at the universities of dresden , mainz , munich and wrzburg has been started . 
pseudocolored composite image reconstructed after scanning for the hoechst 33342 signal ( perfusion , blue ) , vascular structures ( 9f1 mab , red ) , and hypoxia ( pimonidazole , green ) of a cross section of an untreated fadu tumor ( 6 mm diameter )  . 
rekonstruierter tumorquerschnitt mit falschfarben fr perfusion ( hoechst 33342 , blau ) , blutgefe ( 9f1 mab , rot ) und hypoxie ( pimonidazol , grn ) eines unbehandelten fadu - tumors ( 6 mm durchmesser )  . 
der bildanalytisch bestimmte flchenanteil betrgt 13 , 9% fr hypoxie , 29 , 6% fr perfusion und 6 , 6% fr gefstrukturen , von denen 16 , 3% perfundiert sind . 
 our understanding of tumor biology , the project will focus on clinically applicable strategies for microenvironment profiling that will help to identify those patients that might benefit from targeted interventions to improve tumor oxygenation . 
 acknowledgment the joint research project is supported by the deutsche forschungsgemeinschaft grants ad 132 / 3 - 1 , ba 1433 / 4 - 1 , fl 225 / 2 - 1 , mu 576 / 14 - 1 . strahlentherapie strahlentherapie und onkologie und onkologie original article accelerated partial breast irradiation with iridium - 192 multicatheter pdr / hdr brachytherapy preliminary results of the german - austrian multicenter trial oliver j . 
beckmann5 , rolf sauer1 , vratislav strnad1 purpose : to evaluate perioperative morbidity , toxicity , and cosmetic outcome in patients treated with interstitial brachytherapy to the tumor bed as the sole irradiation modality after breast - conserving surgery . 
 patients and methods : from november 1 , 2000 to january 31 , 2004 , 176 women with early - stage breast cancer became partakers in a protocol of tumor bed irradiation alone using pulsed - dose - rate ( pdr ) or high - dose - rate ( hdr ) interstitial multicatheter implants . 
patients became eligible , if their tumor was an infiltrating carcinoma 3 cm in diameter , the surgical margins were clear by at least 2 mm , the axilla was surgically staged node - negative , the tumor was estrogen and / or progesterone receptor - positive , well or moderately differentiated ( g1 / 2 ) , the tumor did not contain an extensive intraductal component ( eic ) and the patients age was > 35 years . 
implants were positioned using a template guide , delivering either 49.8 gy in 83 consecutive hours ( pdr ) or 32.0 gy in two daily fractions over 4 days ( hdr )  . 
interim findings of the first 69 patients , who were treated in this multicenter trial , after a median follow - up of 24 months ( range , 1539 months ) are presented . 
late toxicity : hypersensation / mild pain 7.2% ( 5 / 69 ) , intermittent but tolerable pain 1.4% ( 1 / 69 ) , mild dyspigmentation 10.1% ( 7 / 69 ) , mild fibrosis 11.6% ( 8 / 69 ) , moderate fibrosis 1.4% ( 1 / 69 ) , mild telangiectasia ( < 1 cm2 ) 11.6% ( 8 / 69 ) , and moderate teleangiectasia ( 14 cm2 ) 1.4% ( 1 / 69 )  . 
 conclusion : this analysis indicates that accelerated partial breast irradiation with iridium - 192 interstitial multicatheter pdr / hdr implants is feasible with low perioperative morbidity , low acute and mild late toxicity , and does not significantly affect cosmetic results at a median follow - up of 24 months . 
 key words : accelerated partial breast irradiation brachytherapy pdr strahlenther onkol 2004 ; 180 : 6429 doi 10.1007 / s00066 - 004 - 1294 - 2 akzelerierte teilbrustbestrahlung mit iridium - 192 - multikatheter - pdr / hdr - brachytherapie . 
prliminre ergebnisse der deutsch - sterreichischen multizenter - studie ziel : evaluierung von perioperativer morbiditt , akutund spttoxizitt sowie des kosmetischen ergebnisses nach alleiniger interstitieller pulsed - dose - rate - ( pdr - ) / high - dose - rate - ( hdr - ) multikatheter - brachytherapie des tumorbetts mit 192 - iridium nach brusterhaltender operation . 
ein maximaler tumordurchmesser von 3 cm , ein negativer nodalstatus ( pn0 ) , eine r0 - resektion mit mindestens 2 mm sicherheitssaum , nur gut oder mig differenzierte karzinome ( g1 / 2 ) , strogenund / oder progesteronrezeptorpositive tumoren , kein nachweis einer eic ( extensive intraductal component ) und ein patientinnenalter von mindestens 35 jahren . 
die pdr - brachytherapie wurde mit 49 , 8 gy in 83 aufeinander folgenden stndlichen pulsen , die hdr - brachytherapie bis 32 , 0 gy in zwei tglichen fraktionen ber 1 department of radiation oncology , university hospital erlangen , erlangen , germany , 2 department of radiotherapy and radiobiology , university hospital akh wien , vienna , austria , 3 department of radiation oncology , barmherzige schwestern hospital linz , linz , austria , 4 department of radiation oncology , university hospital leipzig , leipzig , germany , 5 department of gynecology , university hospital erlangen , erlangen , germany . received : march 11 , 2004 ; accepted : july 27 , 2004 strahlenther onkol 2004 no . 
spttoxizitt : berempfindlichkeit / gelegentliches stechen im narbenareal 7 , 2% ( 5 / 69 ) , intermittierende , aber tolerable schmerzen 1 , 4% ( 1 / 69 ) , milde dyspigmentation 10 , 1% ( 7 / 69 ) , milde fibrosierung 11 , 6% ( 8 / 69 ) , moderate fibrosierung 1 , 4% ( 1 / 69 ) , milde teleangiektasiebildung ( < 1 cm2 ) 11 , 6% ( 8 / 69 ) und moderate teleangiektasiebildung ( 14 cm2 ) 1 , 4% ( 1 / 69 )  . 
 schlussfolgerung : diese analyse zeigt , dass die alleinige interstitielle pdr - / hdr - multikatheter - brachytherapie des tumorbetts nach brusterhaltender operation mit niedriger perioperativer komplikationsrate , geringer akuttoxizitt und milder spttoxizitt bei einer medianen nachbeobachtungszeit von 24 monaten durchfhrbar ist und das kosmetische ergebnis bislang nicht signifikant beeinflusst . 
 schlsselwrter : mammakarzinom alleinige brachytherapie teilbrustbestrahlung introduction in the context of broad interdisciplinary acceptance of whole - breast irradiation ( wbi ) as a standard radiation treatment , as indicated in all patients after breast - conserving surgery ( bcs ) , the concept of sole tumor bed irradiation or so - called partial breast irradiation ( pbi ) has become increasingly accepted in recent years for the treatment of patients with a genuine low risk of local recurrence . 
several radiotherapy techniques have been developed , for example , based on the experiences with interstitial boost irradiation [ 21 , 48 ] via brachytherapy with multicatheter [ 1 , 2 , 4 , 8 , 27 , 28 , 3033 , 3739 , 4143 , 45 , 47 , 49 , 6466 , 68 , 69 ] or single - catheter implants [ 3 , 14 , 25 , 26 , 29 , 56 , 70 ] , with three - dimensional conformal external - beam radiotherapy [ 5 , 18 , 67 ] or intraoperative radiotherapy ( iort ) with either electrons [ 9 , 19 , 23 , 40 , 45 , 6062 ] or with a low - kv x - ray source [ 13 , 58 , 59 ] , to prove the hypothesis that pbi can result in local control rates comparable to wbi in a carefully selected subgroup of patients . 
although first results for multicatheter brachytherapy investigations have been very encouraging [ 1 , 4 , 8 , 27 , 28 , 3032 , 49 , 6466 , 68 , 69 ] , pbi is not a standard treatment yet . 
each of the pbi modalities has to prove its efficiency and feasibility in respect of local control rates , acute and late side effects , as well as cosmetic outcome . in this paper we are presenting the 2 - year results of the german - austrian multicenter multicatheter brachytherapy apbi trial . patients and methods between november 2000 and january 2004 , 176 patients were registered for accelerated partial breast irradiation ( apbi ) in four study centers ( erlangen , leipzig , germany ; linz , vienna , austria )  . 
 eligibility and exclusion criteria patients were eligible for sole brachytherapy of the tumor bed , if they had histologically confirmed breast cancer , a maximum tumor diameter of 3 cm , complete resection with clear margins of at least 2 mm , postsurgical negative axillary lymph nodes ( pn0 ) , or singular nodal micrometastasis ( pn1 mi ) , with at least nine lymph nodes removed , no distant metastasis or contralateral breast cancer , ecog performance status 2 , estrogen and / or progesterone receptor - positive tumors , were at least 35 years of age , and after giving written consent . patients were excluded from the protocol , if they showed a multicentric invasive growth pattern , poorly differentiated or undifferentiated tumors , had postoperative residual microcalcifications , an extensive intraductal component ( eic ) , lymph vessel invasion ( l1 ) , unclear margins ( r1 / rx ) , or were pregnant . 
because of a general low - risk profile these patients had not been excluded from pbi and this analysis . breast - conserving surgery patients received different types of bcs ( see table 1 ) and conventional dissection of the ipsilateral axilla . 
the median diameter of the tumors was 13 mm ( range , 226 mm ) ; the median size of the safety margin amounted to 7 mm ( range , 12 20 mm )  . 
 in some cases the median value of the safety margin has been underestimated , because pathologists did not mention the exact extent of the resection margin , if it was > 10 msafety margins > 10 mm were indicated as 10 mm for evaluation . 
apbi : accelerated partial breast irradiation ; bcs : breast - conserving surgery ; dhi : dose homogeneity index ; eic : extensive intraductal component ; hdr : high dose rate ; pdr : pulsed dose rate ; sd : standard deviation ; volumeref : volume encompassed by reference isodose ( usually 85% ) ; volume 150 : volume encompassed by 150% of the reference dose ; volumemax : volume encompassed by 150% of the mean central dose ( mcd )  . 
 brachytherapy after bcs , an interval of 46 weeks was designated for wound healing and for proper histological analysis of the tumor specimen to guarantee the selection of the appropriate patients . 
in case of closed - cavity surgery , ct - based planning often does not lead to a clear delineation of the target volume ; therefore , it was not stipulated in the protocol . 
tamoxifen was administered to 78.3% ( 54 / 69 ) , anastrozole to 8.7% ( 6 / 69 ) , goserelin acetate to 11.6% ( 8 / 69 ) ; one patient ( 1.4% ) received bilateral ovarectomy . 
survival rates and local control rate parameters , as well as acute and late toxicity and cosmetic outcome , were assessed . local control was validated by physical examination every 3 / 6 months and ipsilateral mammography with ultrasound examination of the breast every 6 months after apbi . 
no other perioperative complications , for example bleeding or hematoma , were observed . acute toxicity was low : only 2.9% of the patients ( 2 / 69 ) experienced mild radiodermatitis . late toxicity was mild : 7.2% of the women ( 5 / 69 ) experienced hypersensation / mild pain related to the tumor bed , and 1.4% ( 1 / 69 ) intermittent but tolerable pamild dyspigmentation of the skin above the brachytherapy implant was found in 10.1% of the cases ( 7 / 69 )  . 
mild fibrosis was palpated in 11.6% ( 8 / 69 ) and moderate fibrosis in 1.4% of the patients ( 1 / 69 ) in the region of the surgical scar . 
accelerated partial breast irradiation with pdr / hdr brachytherapy ( < 1 cm2 ) of the involved skin was found in 11.6% ( 8 / 69 ) , and moderate telangiectasia ( 14 cm2 ) in 1.4% of the women ( 1 / 69 )  . 
this means good to excellent cosmetic results were observed in 92.4% of the evaluated patients ( 61 / 66 )  . patients subjectively judged the cosmetic outcome as follows : excellent in 53.0% ( 35 / 66 ) , good in 36.4% ( 24 / 66 ) , fair in 7.6% ( 5 / 66 ) , and poor in 3.0% ( 2 / 66 )  . 
patients judged the cosmetic results as good to excellent in 89.4 of the evaluated cases ( 59 / 66 )  . immediately before the beginning of brachytherapy , physicians declared cosmetic outcome as good to excellent in 90.9% ( 60 / 66 ) of the cases , and patients in 87.9% ( 58 / 66 ) , respectively . 
cosmetic outcome : sehr gutes / gutes kosmetisches ergebnis ; ebi : perkutane strahlentherapie ; lrr : lokalrezidivrate ; n : anzahl der behandelten patientinnen ; na : daten nicht verfgbar . 
cosmetic outcome : sehr gutes / gutes kosmetisches ergebnis ; ebi : perkutane strahlentherapie ; lrr : lokalrezidivrate ; n : anzahl der behandelten patientinnen ; ns : daten nicht erwhnt . 
problems were , for example , no proper localization of the excision cavity with surgical clips or by ct - based target volume planning [ 36 , 50 , 51 ] , the inclusion of patients with tumor diameters up to 4.5 cm [ 15 , 36 , 4244 , 50 , 51 ] , no exclusion of node - positive patients by omitting the surgical staging of the axilla [ 12 , 37 , 50 , 51 ] , no exclusion in case of positive nodes [ 15 , 4244 ] , the presence of an eic in some cases [ 15 , 4244 ] , the involvement of the surgical margins [ 12 , 15 , 36 , 50 , 51 , 54 ] , comparably small treatment volumes with a high portion of single - plane implants [ 4244 ] , or the nonavailability of detailed histological reports in many cases [ 12 ]  . 
a summary of the results of these trials is given in table 2 . based on the controversial results of earlier studies , strict patient selection criteria and systematic quality assurance procedures [ 20 , 46 , 66 ] were a significant factor in later clinical trials using multicatheter brachytherapy with various dose rates as the sole radiation treatment [ 1 , 4 , 23 , 25 , 27 , 29 , 3032 , 37 , 46 , 47 , 50 , 55 , 62 , 63 , 66 , 67 ]  . 
accelerated partial breast irradiation with pdr / hdr brachytherapy local control rates the results of various clinical investigations clearly underline the benefit of wbi in local control after bcs [ 16 , 17 , 53 , 63 ] , even in highly selected low - risk subgroups of patients [ 10 , 11 , 22 , 34 , 35 ]  . 
publications further indicate ( see table 3 ) that in apbi multicatheter brachytherapy trials with appropriate patient selection and optimal quality assurance , the risk of local recurrence is low and comparable to modern standard wbi , which usually leads to annual local failure rates of about 1% [ 6 , 7 , 34 , 35 ]  . 
 this would result in an annual ipsilateral in - breast recurrence rate of 0.44% , which is surely underestimated because of comparably short follow - up periods in the majority of the mentioned studies . to date , none of the patients treated in our study ( n = 176 ) have shown local , locoregional or distant failure . 
our data with limited follow - up but a comparatively large patient number seems to support the hypothesis that accelerated pbi with multicatheter brachytherapy implants is a safe treatment in a highly selected subgroup of patients . perioperative complications and side effects the surgical procedure of tube implantation was safe . 
besides the infectious complications , some authors described low incidences ( 24% ) of bleeding at the time of catheter removal [ 33 , 49 ] , of hematoma [ 27 , 33 , 49 ] , or complicated wound healing [ 27 , 33 ]  . 
the explanations for this difference in comparison to our results are a significantly higher total dose ( see table 3 ) and large implant volumes up to 204 cm2 [ 33 ]  . 
in this trial , the total dose ( 37.2 gy in ten fractions of hdr brachytherapy , prescribed as a minimal peripheral dose encompassing the target volume ) was also significantly higher . reviewing the publications it transpires that acute skin toxicity is clearly related to the prescribed total dose as well as to the implant volume , which , in our opinion , should only exceed 120150 cm3 for the reference isodose in very exceptional cases . to compare late toxicities using publications is very difficult , as the incidence of late complications is a matter of time . 
 at a medium follow - up period of 24 months , the evaluated late toxicities ( postimplant breast pain , dyspigmentation , fibrosis , telangiectasia , fat necrosis ) were acceptably mild or absent , as outlined above . other authors confirm our results , reporting mainly grade 1 / 2 late toxicities after apbi [ 1 , 4 , 33 , 49 ]  . 
 [ 27 ] describe , in a series with both ldr and hdr implants , a proportion of 24% with fat necrosis , two of the patients ( 4% ) needing surgical intervention , and wazer et al . 
in this study , no patient had combined clinical and mammographic signs of fat necrosis , which could be due to the high portion of pdr implants used in the study . 
in our experience , clinically evident fat necrosis seemed not to be a major problem of apbi . cosmetic outcome in this study the cosmetic results were independently evaluated by the responsible physician and the patient . 
no impact of brachytherapy on cosmetic outcome was found . as outlined in table 3 , the majority of multicatheter brachytherapy trials showed good to excellent cosmetic results in 8894% of the treated patients [ 33 , 37 , 47 , 49 , 52 , 66 , 68 , 69 ]  . 
longer follow - up periods of 46.5 years reported in other trials with around 90% good to excellent cosmetic results [ 33 , 37 , 47 , 49 , 52 , 66 ] give us the hope that our patients will not be surprised in the future by unexpected cosmetic events . conclusion this analysis shows that apbi with iridium - 192 multicatheter interstitial implants is feasible with very low perioperative morbidity , low acute and ( at a median follow - up of 24 months ) mild late toxicity , and does not significantly affect cosmetic results . 
accelerated partial breast irradiation with pdr / hdr brachytherapy strahlentherapie und onkologie original article virtual simulation of a boost field in adjuvant radiotherapy of the breast andreas kaiser1 , lutz moser1 , wolf kuschke1 , margit hinkelbein1 , andr buchali2 , volker budach1 background and purpose : in ct - based adjuvant radiotherapy of the breast , virtual simulation techniques have been developed . 
 conclusion : virtual simulation of a boost field has the potential to elegantly link the simplicity of a conventional simulation with the accurate tumor bed identification provided by a ct data set . 
 key words : virtual simulation ct simulation breast cancer radiotherapy boost tumor bed strahlenther onkol 2004 ; 180 : 63741 doi 10.1007 / s00066 - 004 - 1275 - 5 virtuelle simulation eines boostfeldes bei der adjuvanten strahlentherapie der brust hintergrund und ziel : fr die ct - geplante adjuvante strahlentherapie der brust sind techniken der virtuellen simulation entwickelt worden . 
in dieser arbeit wird eine einfache virtuelle simulation eines boostfeldes demonstriert . material und methodik : 41 felder wurden virtuell geplant , 26 als elektronenfelder , 15 als tangentiale photonenfelder ( abbildung 1 )  . ergebnisse : fr erfahrene anwender war die geometrische genauigkeit hoch ; mgliche fehlerquellen werden illustriert . 
differierende fokus - haut - abstnde mit konsekutiven divergenzeffekten und teilvolumeneffekte waren als urschlich zu diskutieren . schlussfolgerung : die virtuelle simulation eines boostfeldes hat das potential , die einfache technik einer konventionellen simulation mit der genauigkeit der tumorbettidentifizierung im ct - datensatz elegant zu verbinden . 
 darber hinaus ermglichte sie eine visualisierung der dosisverteilung , die in einigen fllen als hilfreich empfunden wurde ( abbildung 2 )  . schlsselwrter : virtuelle simulation ct - simulation brustkrebs strahlentherapie boost tumorbett 1 department of radiotherapy , campus mitte , charit universittsmedizin berlin , germany , 2 department of radiotherapy , ruppiner kliniken gmbh , neuruppin , germany . received : february 4 , 2004 ; accepted : july 27 , 2004 strahlenther onkol 2004 no . 
target areas in difficult anatomic regions could reliably be included , and organs at risk , e.g. , lung and heart , could be spared at the same time [ 7 , 12 ]  . 
 in radiotherapy of the breast , a boost dose is widely accepted to improve local control , particularly in patients 40 years of age [ 20 , 23 , 27 , 29 ]  . 
cosmetic results depend on boost field size and dose homogeneity with only mild late skin and soft - tissue changes and no substantial deterioration of cosmetic outcome [ 16 , 28 ]  . 
it is the objective of this paper to introduce the virtual simulation of a boost field based on the initial ct data set , analyze geometric accuracy and field size compared to a conventional simulation , and illustrate aspects of verification . 
using the acqsim software , an isocenter was defined as described before [ 4 , 5 ] , which then could be projected on the patients skin via adjustable lasers . 
for treatment verification and documentation , the radiographs were scanned into the on - line portal imaging system varis vision . approximately 80% of the breast cancer patients had tumor bed clips , and only those patients were included in this investigation to allow for a reliable verification and an analysis of geometric accuracy . 
the target volume included the clips and a safety margin of at least 2 cm with special regard to the initial tumor size ( refer also to [ 11 ] )  . 
preferentially , the boost dose was delivered via a direct electron bea the first step of the virtual simulation was to shift the isocenter toward the geometric center of the tumor bed , to enable table and gantry position alteration during preparation and treatment without missing the target . 
the software calculated the offset from the isocenter of the preceding series of tangential beam irradiation , which was marked on the patients sksecond , gantry , table and collimator position were chosen with regard to restrictions of the treatment machine such as interactions between gantry and table position or length and diameter of the electron tubus . 
in some cases , isodose distributions were generated using the cadplan treatment planning systeverification took place during week 5 of the tangential breast irradiation using a conventional varian ximatron simulator . 
 41 patients were investigated , 15 received a tangential electron beam ( group 1a ) , eleven an orthogonal electron beam ( group 1b ) , and 15 had opposed tangential photon beams ( group 2 )  . 
 results time expenditure the additional planning process took approximately 7 min : 3 min to identify and delineate additional structures , and about 4 min to define the boost field and generate a drr . 
a conventional simulation on the other hand could have taken up to 20 min depending on the physicians expertise and ease of identifying the tumor bed : up to 10 min for the physician , 15 min for the medical assistant , and 20 min for the patient . 
patient characteristics ( all values are means standard deviations ) : fsd : difference of the focus - skin distance at verification from the virtually planned distance ; isocenter : difference of the isocenter position at verification from the virtually planned position ; field size at vs : field size at virtual simulation ; verification : difference of the virtually planned field size from the field size modified at verification ; calculated : expected difference of the field size at verification from the size planned virtually with divergence effects calculated . 
 fsd : differenz zwischen dem fokus - haut - abstand bei der verifikation und bei der virtuellen simulation ; isocenter : abweichung der position des isozentrums bei der verifikation von der virtuell geplanten position ; field size at vs : virtuell geplante feldgre ; verification : differenz zwischen der virtuell geplanten feldgre zur genderten feldgre nach verifikation ; calculated : unter bercksichtigung der divergenzeffekte erwartete feldgrenunterschiede bei der verifikation . 
illustration of time expenditure of patient , medical staff , and at the machines ; one unit is equivalent to about 5 m : conventional simulation ; : virtual simulation . 
 divergence effects because of differing focus - skin distances have contributed concerning the electron beams , as well as partial volume effects due to the rather generous slice thickness of the planning ct scan . 
 as expected , an electron beam included the scar in most cases , whereas a tangential photon beam could include only a few . techniques using a ct and tumor bed clips for target volume definition have been published before as part of a three - dimensional planning procedure , which proved to be advantageous over a clinically guided conventional simulation [ 2 , 9 , 14 ]  . 
regarding recent discussions of a postoperative radiotherapy confined to the tumor bed [ 19 ] , it is important to understand the limitations of a virtual simulation , since a geographic miss could be deleterious . virtual simulation of a boost field links the simplicity of a conventional simulation with the three - dimensional information of a ct data set . 
breast boost : are we missing the target ? strahlentherapie und onkologie original article regional nodal recurrence in the management of breast cancer patients with one to three positive axillary lymph nodes outcome of patients following tangential irradiation without a separate nodal field heidi stranzl1 , florentia peintinger2 , petra ofner3 , ulrike prettenhofer1 , ramona mayer1 , arnulf hackl1 purpose : to examine the prognosis of breast cancer patients ( t13 , one to three positive axillary lymph nodes ) and locoregional failure rate after breast - conserving therapy / modified radical mastectomy and adequate axillary dissection following tangential radiotherapy without irradiation of the regional lymph nodes . patients and methods : from 1994 to 2002 , the medical records of 183 breast cancer patients ( t13 , one to three involved axillary lymph nodes ) were examined in order to identify those experiencing regional nodal recurrence , with or without local recurrence . 
chemotherapy was administered to 101 patients ( 55% ) , hormonal therapy to 124 ( 60% ) , and combined systemic treatment to 47 ( 26% )  . results : the median observation time was 44.4 months ( range , 11102 months )  . 
of the 14 patients ( 7.7% ) with a relapse , six ( 3.3% ) had a local recurrence , five ( 2.8% ) a regional relapse , and three ( 1.6% ) a simultaneous recurrence . 
nine out of 14 patients with locoregional relapse developed distant failure subsequently and seven of them ( 78% ) died of the disease . conclusion : regional recurrence is uncommon among patients with one to three positive axillary lymph nodes treated with surgery , adequate axillary dissection , and tangential field irradiation only . 
the authors conclude that regional nodal irradiation should not routinely be given following adequate axillary dissection when only one to three lymph nodes are positive . key words : breast cancer adjuvant irradiation one to three positive lymph nodes strahlenther onkol 2004 ; 180 : 6238 doi 10.1007 / s00066 - 004 - 1241 - 2 das lokoregionre rezidiv bei patientinnen mit mammakarzinom und ein bis drei positiven axillren lymphknoten . 
 ergebnisse nach tangentialer bestrahlung ohne separates nodales feld ziel : prognose und lokoregionre rezidivrate von patientinnen mit mammakarzinom ( t13 , ein bis drei positive axillre lymphknoten ) nach brusterhaltender therapie bzw . 
von den 14 patientinnen ( 7 , 7% ) mit rezidiven hatten sechs ( 3 , 3% ) ein lokales , fnf ( 2 , 8% ) ein isoliertes regionres und drei ( 1 , 6% ) ein simultanes lokales und regionres rezidiv ( tabelle 2 )  . 
 1 department of radiotherapy , university medical school , graz , austria , 2 division of gynecology , leoben , austria , 3 department of medical informatics , statistics and documentation , university medical school , graz , austria . received : september 25 , 2003 ; accepted : april 29 , 2004 strahlenther onkol 2004 no . 
outcome of breast cancer patients following adjuvant irradiation schlussfolgerung : das lokoregionre rezidiv ist bei patientinnen mit mammakarzinom ( t1t3 , ein bis drei positive lymphknoten ) nach chirurgischer intervention mit adquater axillrer dissektion und tangentialer bestrahlung ein seltenes ereignis . 
adjuvant radiotherapy , including the regional lymph nodes , is a significant issue in the multimodal therapeutic approach to breast cancer , as it has been extensively documented in several reports [ 1114 ]  . 
moreover , the benefits of adjuvant irradiation must be carefully balanced against the potential radiation - related complications of such treatment . for breast carcinoma , involvement of the axillary lymph nodes is the single most important prognostic factor [ 4 ]  . 
 since in the larger danish studies limited axillary dissections were undertaken , the ability to generalize these results has been questioned [ 8 ]  . the purpose of our study was to reevaluate the prognosis of female breast cancer patients ( t13 , one to three positive axillary lymph nodes ) with locoregional failure after breast - conserving therapy or modified radical mastectomy and adequate axillary dissection following tangential radiotherapy without irradiation of the regional lymph nodes . patients and methods the medical records of 1 , 075 women with pathologic stage ii or iii breast cancer treated between 1994 and 2002 were examined in order to identify those experiencing a regional nodal recurrence , with or without local recurrence and with or without distant metastases . 
all 183 patients underwent surgical treatment of the primary lesion , either breast - conserving therapy ( n = 146 ) or modified radical mastectomy ( n = 37 )  . 
patients were identified to have between one to three involved lymph nodes and were irradiated postoperatively after written approval [ 18 , 19 ]  . external - beam irradiation ( 4or 6 - mv photon / 60co ) was given to the breast alone using opposed tangential fields . 
the dose to the entire breast ( n = 146 , 79.8% ) was usually 50 gy ( range , 4654 gy ) , delivered at 1.82 gy per fraction , given five times weekly . 
cyclophosphamide , methotrexate , 5 - fluorouracil - based ( cmf ) and / or doxorubicin - containing regimens were given to 90% of patients receiving chemotherapy . hormonal therapy ( tamoxifen , 20 mg / day , 5 years ) was initiated in 124 patients ( 60% ) as a component of their primary treatment . 
outcome of breast cancer patients following adjuvant irradiation local recurrence was classified as detection of cancer within the conserved breast or chest wall and was documented pathologically in all cases . 
 for all patients the routine evaluation , until diagnosis of progression or last visit to our clinic / physician or death , provided careful clinical examination and complete blood count in 3to 6 - month intervals until the end of the 5th year , annually thereafter . 
statistical analysis of overall survival ( os ) , recurrence - free survival ( rfs ) , disease - free survival ( dfs ) , and metastases - free survival ( mfs ) , as well as analysis of follow - up , was calculated by the method of kaplan - meier . 
all p - values reported are two - sided . results by may 2003 , there was a median observation time of 44.4 months ( range , 11102 months ) for all patients . 
 age ( years ) 40 > 4055 > 5570 > 70 tumor location central lateral medial multicentric t - stage t1 t2 t3 tumor size ( cm ) 2 > 2 histologic grade 1 2 3 x estrogen receptor positive negative unknown margin status clear close lymphatic invasion present absent chemotherapy yes no hormonal therapy yes no 19 56 66 42 28 110 21 24 106 58 19 106 77 6 73 103 1 140 42 1 179 4 55 128 101 82 124 59 there were no patients identified with simultaneous local , regional and distant metastases . 
the pattern of regional nodal failure included supraclavicular nodes only ( n = 3 , 60% ) , axillary lymph nodes only ( n = 1 , 20% ) , or multiple nodal sites ( n = 1 , 20% )  . 
an analysis of the potential risk factors contributing to locoregional failure was performed , and only two risk factors were identified that significantly increased the risk of recurrence on univariate analysis ( table 1 )  . 
outcome of breast cancer patients following adjuvant irradiation with a tumor size 2 cm and 6.5% of the patients with a tumor size > 2 cm developed a local recurrence . 
 1 year ( % ) 3 years ( % ) 5 years ( % ) overall survival recurrence - free survival disease - free survival metastases - free survival 100 98 98 99 four of five ( 80% ) patients who developed regional nodal failure without any local relapse experienced recurrence in the supraclavicular nodes . 
nine patients with locoregional relapse developed distant metastases subsequently and seven of them ( 78% ) died of disease ; the remaining two patients were alive with distant metastases at the time of last follow - up in may 2003 , with a 95and 98 - month follow - up interval after first recurrence . 
 kaplan - meier estimates of os , rfs , dfs , and mfs at 1 year , 3 years , and 5 years are provided in detail in table 3 . 
 discussion time to failure ( months ) in demonstrating the power of adequate axillary dissection for both staging and survival , the number of nodes removed by the surgeon and examined by the pathologist plays an important role [ 6 , 14 , 23 ]  . 
 [ 10 ] found that in treating patients with early t - stage breast cancer and one to three positive lymph nodes , 1920 must be examined to assess stage with 90% accuracy . 
 13 in a study by the eastern cooperative oncology group [ 14 ] , the median number of nodes retrieved was 15 , and 13% of unirradiated patients with one to three positive nodes presented with recurrence . 
outcome of breast cancer patients following adjuvant irradiation most importantly , the danish and british columbian prospective randomized trials [ 1113 ] demonstrated a significant reduction in locoregional failure in patients irradiated postoperatively and a subsequent improvement in os . 
these findings were supported by others [ 9 ] and initiated changes in treatment recommendations [ 16 ]  . a recent retrospective analysis with node - positive women ( t1 / 2 , one to three positive axillary lymph nodes ) focused on the results in subgroups of patients defined by tumor size [ 7 ]  . 
as a consequence of this analysis , patients with t2 tumors and one to three positive nodes are at high risk of isolated locoregional recurrence without irradiation , and therefore the authors support the routine use of postmastectomy irradiation in these patients , especially in those aged 45 years . 
 our study suggests that primary tumor size > 2 cm is associated with an increased risk of locoregional recurrence following surgery of the primary tumor , adequate axillary dissection , and tangential irradiation only . 
as all female patients had seven or more axillary lymph nodes recovered at dissection , it is unlikely that an increased risk of failure seen among such patients was due to less extensive axillary clearance , responsible for inadequate primary treatment of the axilla . 
 currently , there are no sufficient data available to justify the routine application of a separate irradiation field to the supraclavicular fossa in node - positive patients ( one to three positive lymph nodes ) with an adequately dissected axilla . 
a number of studies have focused attention on the need of regional nodal irradiation in patients with four or more positive lymph nodes [ 2 , 3 , 22 ]  . 
 [ 14 ] , examining specific sites of recurrence , the results of the current study demonstrate that irradiation to the internal mammary nodes should not be considered mandatory at present . the axillary failure rate ( n = 1 , 0.6% ) in our study population is consistent with prior studies [ 3 ] which have also demonstrated the extremely low risk of developing an isolated axillary recurrence ( n = 1 , 0.6% ) in patients with one to three positive lymph nodes . 
in our study population , 64% of patients ( n = 9 ) with locoregional failure ( n = 14 ) subsequently suffered from distant metastases , which in turn determined the course of the disease . 
 a limitation of our study was that the number of patients in particular subgroups is low , especially those with t3 and those who had undergone modified radical mastectomy as initial surgical procedure , and therefore data must be interpreted with caution . 
 conclusion based on the findings of our study and other existing reports , we conclude that regional recurrence is an infrequent event in patients with t13 tumors and one to three positive axillary lymph nodes after surgery of the primary tumor , adequate axillary dissection , and tangential irradiation only . 
further randomized studies may determine the impact of regional nodal irradiation and may identify subgroups of patients with one to three positive nodes at high risk of regional nodal failure who might benefit from additional nodal irradiation . 
 strahlentherapie und onkologie original article analysis of the action of the restriction endonuclease alui using three different comet assay protocols wolfgang - ulrich mller1 , jens ciborovius1 , thomas bauch1 , christian johannes2 , christian schunck2 , ulrike mallek1 , wilfried bcker1 , gnter obe2 , christian streffer1 background and purpose : the comet assay offers the opportunity to measure the amount of dna damage and the effectiveness of dna repair in single cells . 
in a first part , experiments are presented comparing three different protocols of the comet assay technique with respect to the analysis of the induction of dna damage after x - irradiation in isolated human lymphocytes and cho cells . 
in a second part , the restriction enzyme alui , an agent producing dna double - strand breaks exclusively , was introduced into cho cells by electroporation and the effects were analyzed using the different comet assay protocols . 
the experiments were carried out in order to test the assertion that comet assay techniques can measure different types of dna damages at different ph conditions of lysis and electrophoresis . material and methods : three different comet assay protocols were used for the analysis of dna damage in lymphocytes and cho cells . 
 results : the results clearly indicate that among the three protocols the modified comet assay technique used by the authors showed the highest sensitivity in the radiotherapy - relevant dose range between 0 and 2 gy . 
whereas after radiation exposure all cell nuclei show a dose - dependent increase in dna content in the comet tail , most of the cell nuclei were unaffected by an alui uptake . 
nevertheless , there was an effect by alui that could be detected in all three assay versions : between 5% and 15% of the nuclei showed clearly abnormal comet morphologies . conclusion : neither the strictly alkaline nor the strictly neutral comet assay is applicable in the radiation dose range of about 2 gy . 
the restriction enzyme results show that other factors than just dna strand breaks contribute to dna migration into the tail of the comets . key words : comet assay lymphocytes cho cells dna damage x - rays restriction endonuclease alui strahlenther onkol 2004 ; 180 : 65564 doi 10.1007 / s00066 - 004 - 1255 - 9 analyse der wirkung der restriktionsendonuklease alui unter verwendung von drei verschiedenen kometentest - protokollen hintergrund und ziel : der kometen - test liefert die mglichkeit , das ausma von dna - schden und dna - reparatur in einzelzellen zu messen . 
in einem ersten teil werden experimente vorgestellt , in denen drei verschiedene protokolle des kometen - tests auf ihre fhigkeit berprft wurden , dna - schden nach rntgenbestrahlung in isolierten menschlichen lymphozyten und cho - zellen zu erfassen . 
die experimente wurden durchgefhrt , um die behauptung zu testen , dass durch vernderung der ph - bedingungen bei der lyse und der elektrophorese unterschiedliche dna - schadenstypen erfasst werden knnen . material und methodik : es wurden drei verschiedene kometen - test - protokolle ( tabelle 1 ) zur analyse von dna - schden in lymphozyten und cho - zellen verwendet . ergebnisse : die ergebnisse zeigen eindeutig , dass von den drei protokollen die von den autoren verwendete modifizierte fassung des kometen - tests die hchste empfindlichkeit im fr die strahlentherapie relevanten dosisbereich von 02 gy aufweist ( abbildungen 1 und 2 )  . 
dennoch gab es einen alui - effekt , der in allen drei versionen des tests nachweisbar war : zwischen 5 und 15% aller kerne zeigten deutlich anormale kometenstrukturen ( abbildungen 3 und 4 )  . 
 1 institute for medical radiobiology , university hospital essen , essen , germany , 2 institute for genetics , university of duisburg - essen , essen , germany . received : november 11 , 2003 ; accepted : july 23 , 2004 strahlenther onkol 2004 no . 
 schlsselwrter : kometen - test lymphozyten cho - zellen dna - schaden rntgenstrahlen restriktionsendo nuklease alui introduction since its introduction in 1984 by ostling & johanson [ 26 ] , the interest in the comet assay or single - cell gel electrophoresis as a useful tool for measuring dna damage and dna repair in individual cells has increased rapidly . 
although the assay basically remained unchanged ( embedding of single cells in agarose on microscope slides , lysis of the cells and electrophoresis in a weak electric field ) , a lot of modifications in the experimental conditions have been introduced ( for a review see [ 9 ] )  . 
it was assumed that one could measure either dna double - strand breaks ( dsb ) or dna single - strand breaks ( ssb ) plus alkali - labile lesions with high specificity just by changing the ph conditions for lysis and electrophoresis ( neutral protocols : [ 19 , 24 , 25 ] ; alkaline protocols : [ 18 , 2023 , 25 ] )  . 
the difference in sensitivity between these two versions seems to correlate with the different amounts of dna lesions the assay focuses on [ 29 ] : relationship between ssb plus alkali - labile sites and dsb is ~ 25 : 1 ( number of ssb per gy : 5001 , 000 , number of alkali - labile sites : 200300 ; number of dsb : 40 )  . in essen , germany , we have developed a comet assay ( lysis at ph 9.5 , electrophoresis at ph 8.3 ) which follows neither a strictly neutral nor an alkaline protocol . 
although some similarities to olives neutral assay are obvious , the essen protocol is much more sensitive ( statistically significant differences in initial dna damage can be measured after 0.1 gy x - rays at p < 0.01 [ 19 ] )  . 
additionally , we found that shifting the ph conditions for lysis and electrophoresis in our protocol to more neutral or alkaline ph values had no or little effect on the sensitivity of the assay . 
using the three different comet assay protocols , the induction of dna damage after x - irradiation was analyzed in isolated lymphocytes of two donors and in cho cells ( essen protocol : dose range 010 gy ; olives alkaline version : dose range 020 gy ; olives neutral version : dose range 050 gy )  . a major problem with most of the studies using the comet assay is the lack of specificity of the agent which was chosen for the induction of various dna damages . 
the cho cells were grown in mccoys 5a medium ( gibco ) supplemented with 10% newborn calf serum ( ncs , gibco ) and antibiotics ( penicillin 100 u / ml , streptomycin 0.1 mg / ml )  . 
 radiation exposure the cells were irradiated in suspension on ice using a stabilipan x - ray machine ( siemens , erlangen , germany ; 15 ma , 240 kvp , 0.5 mm cu filter ) at a dose rate of 1 gy / min ( for the experiments with the essen comet assay and the alkaline protocol ) or 2 gy / min ( for the experiments with the neutral assay )  . 
comet assay and alui comet assay protocols in the restriction enzyme experiments , the comet assay was carried out after 1 h of incubation on ice in the presence or absence of alui . 
100 l of a cell suspension ( optimum cell density approximately 35 104 / 100 l ) were mixed with 500 l of warm agarose ( 45 c ; 0.75% in pbs without ca2 + and mg2 + ; serva low melting for preparative isolation of dna / rna fragments , heidelberg , germany ) and spread on slides already precoated with 500 l agarose ( 0.1% in pbs without ca2 + and mg2 + )  . 
microscope slides were precovered with 500 l of 0.1% agarose and dried at 45 c for 4560 m100 l of the cell suspension was mixed with 500 l of 0.75% agarose and spread on the slides . 
after precoating with 500 l of 0.1% agarose and drying at 45 c for 4560 min , slides were covered with 500 l of 0.75% agarose plus 100 l cell suspension and transferred to a cooling plate for 1015 min at 4 c . 
the dna was allowed to unwind in 30 mm naoh , 1 mm edta at ph 12.3 for 30 min at room temperature in the dark before the electrophoresis was carried out in 200 ml of the unwinding buffer at ph 12.3 and room temperature in an electric field of 1.0 v / cm for 20 mafter washing in distilled water for 25 min , the gels were dried at 45 c on a warming plate . 
 table 1 presents a brief summary of the experimental steps of the three comet assay protocols in order to allow a direct comparison of the differences and similarities of the techniques used . 
after that procedure the slides were covered with 150 l of a solution of the fluorescent dye propidium iodide ( pi ) corresponding to 1.5 g pi per slide ( stock solution : 2.5 105 m ; serva , heidelberg , germany )  . 
three to four independent experiments were run for each dose - response relationship , and in each experiment 35 comets were measured per dose point . dose - response relationships were fitted using graphpad prism 4.0 ; as there is no biological model available that suggests , how the fit should look like , no specific model was applied consistently to all data points . 
after electroporation cells were kept on ice for 10 mfor recovery , cells were washed once with prewarmed medium and incubated in complete medium containing 10% fcs for 18 h including a 2 - h treatment with colcemid ( 0.08 g / ml )  . 
the dose - response curves of the lymphocytes of both donors and of cho cells show a steep increase in the amount of initial dna damage up to 2 gy ( figure 1a )  . 
for the neutral comet assay , the amount of dna damage measured after irradiation with 50 gy is comparable to the amount of dna damage after 2 gy when analyzed with the essen protocol . 
in the dose range between 020 gy the dose - response curves are close to linearity for both donors and for cho cells , although the sensitivity of the assay is limited to doses 2 gy ( figure 1c )  . comparison of the results of the three protocols . 
whereas the essen approach shows a steep increase in dna damage up to about 2 gy , neither the alkaline nor the neutral version detect significant amounts of damage in this dose range . 
at higher doses , the alkaline assay shows a steep increase , whereas the essen approach is leveling off and the neutral version starts to identify significant amounts of dna damage only at doses exceeding 510 gy . 
comparison of the essen ( a ) , neutral ( b ) and alkaline ( c ) comet assay approach applied to peripheral blood lymphocytes of two donors and to cho cells after exposure to x - rays . 
vergleich des essener ( a ) , neutralen ( b ) und alkalischen ( c ) kometen - test - ansatzes in peripheren lymphozyten zweier spender und in cho - zellen nach exposition mit rntgenstrahlen . 
die fehlerbalken stellen den standardfehler aller experimente dar , die mit den lymphozyten der beiden spender durchgefhrt wurden . effects of the restriction enzyme alui experiments with the restriction enzyme alui were performed with cho cells . 
in order to have a control on the activity of the restriction enzyme in cells of the same experiment , the scoring of chromosomal aberrations was carried out in parallel to the comet assay analysis . 
remarkably , in the comet assay analysis the only effect which could be attributed to the enzymatic activity of the restriction endonuclease was the induction of so - called abnormal comet structures . 
we defined abnormal comets as structures with either extremely long comet tails ( figures 3c and 3d ) and / or with extremely oversized , bulky tail proportions ( figures 3e and 3f ) which can easily be distinguished from typical normal comet shapes ( figures 3a and 3b )  . 
 dose ( gy ) results of the essen and the neutral version are surprising , because many features of both assays are very similar ( see table 1 )  . 
comet assay and alui using the essen comet assay protocol , these abnormal comets appear at a frequency far less than 5% and this value does not increase by x - ray doses 10 gy . 
for the analysis with the essen protocol and the neutral comet assay , nearly no abnormal comets could be detected in untreated samples or in cells just running through the electroporation procedure ( figures 4a and 4b )  . 
obviously , abnormal comets were generated by enzymatic treatment in a concentration - dependent manner , no matter which comet assay protocol was used for analysis ( figure 4 )  . 
obviously , the alui action is so fast , that the comparatively short times of electroporation ( which is done at room temperature ) and cooling down afterwards are sufficient for inducing dsb ; perhaps , some activity is even present on ice . 
prozentsatz anormaler kometen nach exposition von cho - zellen mit alui und anwendung des essener ( a ) , neutralen ( b ) oder alkalischen ( c ) ansatzes . electroporation c ontrol strahlenther onkol 2004 no . 
 discussion we compared three different protocols of the comet assay technique , the essen approach [ 17 ] , the neutral [ 24 ] and the alkaline assay [ 25 ] of olive et al . 
the induction of dna damage after x - irradiation was measured in isolated human lymphocytes and in cho cells resulting in three different doseresponse relationships ( figures 1 and 2 )  . quite a number of techniques are intended to be used in the detection of individual radiosensitivities , such as chromosomal aberrations [ 8 , 11 ] , 24 - color fish [ 14 , 15 ] , micronuclei [ 32 ] , dna - pkcs and ku ( p70 / p80 ) [ 3 ] , to name just some of the approaches . 
as our major interest with regard to the application of the comet assay is also directed at the monitoring of individual radiosensitivities , in particular , of tumor patients who received a radiotherapy , our test was optimized to have maximum sensitivity in the dose range between 02 gy and to allow the measurement of dna repair after a single dose of 2 gy ( corresponding to the dose per fraction in conventional radiotherapy )  . 
while neutral conditions should allow the measurement of dsb , alkaline ph values lead to single - stranded dna ( by cleavage of the hydrogen bonds between the two dna strands ) shifting the balance to the ssb plus alkali - labile lesions [ 2125 ]  . 
kohn & grimek - ewig [ 13 ] introduced the alkaline elution method for the analysis of dna single - strand interruptions by lysing the cells on filters using alkaline buffers . 
the induction and repair of dsb can be measured with the use of the neutral filter elution technique [ 6 ] and pulsed - field gel electrophoresis [ 30 ]  . 
therefore , the idea was supported that the comet assay is able to measure dsb under neutral conditions [ 19 , 24 , 25 ] and ( dsb plus ) ssb plus alkali - labile lesions under alkaalul ( u ) 0 u 10 u 20 u 40 u figures 5a and 5b . 
die fehlerbalken stellen den standardfehler des mittelwerts dar . line conditions [ 18 , 2023 , 25 ] , thus resulting in an increase in sensitivity due to the higher numbers of lesions covered ( for a review see [ 9 ] )  . 
 the results presented in this publication clearly indicate that one has to be careful with the assumption that for the comet assay only the ph conditions during lysis and electrophoresis are responsible for the type of dna damage being measured afterwards ( see figures 1 and 2 and table 1 )  . 
 [ 9 , 1825 ] , but the whole method itself was modified introducing , e.g. , different time schedules for the preparative steps and new buffer systems for lysis and electrophoresis . assuming that the neutral assay of olive et al . 
in particular , the composition of the buffers is almost the same and the ph values for electrophoresis are quite comparable ( ph 8.3 for the essen approach and ph 7.6 for the neutral comet assay )  . 
nevertheless , the dose - response curves are dramatically different ( figure 2 ) , pointing to the conclusion that it is not only ph that decides on the amount of dna released into the comet tail . 
 in addition , for the essen comet assay previous studies have shown that a change in the ph value of the lysis and electrophoresis buffer or the duration of the electrophoresis has no or just minor effects on the sensitivity [ 2 ]  . there are , however , other factors that should be kept in mind . 
a reduction in the electric field strength from 2.5 v / cm to 1.2 v / cm leads to a marked decrease in sensitivity of the comet assay itself ( approximately by a factor of 2 ; data not shown )  . 
analyzing the influence of lysis time in that context shows that the only effect of a longer lysis period ( 2 h instead of 15 min ) seems to be an increase in dna damage in the unirradiated samples by a factor of 1.6 ( unpublished results )  . 
we think that certain methodological features ( such as duration of lysis and electrophoresis and electric field strength ) have an effect on the morphology ( in particular , length and shape ) of the comet and may interfere with the analysis of the specific dna damage . 
therefore , besides the influence of the ph value on the nature of the dna damage being measured , effects of other methodological features on the morphology of the comet have to be considered . 
 [ 24 ] , that the original ostling & johanson approach [ 26 ] retains the intact loop structure of dna , thus making the assay sensitive to the release of dna supercoiling caused by ssb , might well apply . 
taking into consideration that the essen protocol uses ph values close to those used in the neutral version , we assume that ssb might be of less importance in our assay than in the alkaline version , but that release of dna supercoiling markedly amplifies the damage induced by the ssb . 
while in former experiments x - irradiation was used , known to induce a spectrum of different types of dna damage , the introduction of the restriction enzyme alui results in dsb only . 
only those experiments showing the generation of chromosomal aberrations by the restriction enzyme were analyzed with the comet assay . the study of the effects of alui with the comet assay led to surprising results . 
according to the proposed action of the enzyme in inducing dsb one would expect that alui increases the amount of measurable dna damage resulting in comets with a higher tail / head ratio than controls . 
if the strand break concept behind the comet assay is correct ( the comet assay is measuring dsb , ssb and alkali - labile sites dependent on the ph conditions ) , then all three approaches should give the same amount of dna in the comet tails . surprisingly , no increase in the tail / head ratio of regular comets could be measured with any comet assay protocol after enzymatic action . 
 in the alkaline comet assay of olive et al . , the so - called abnormal comets are typical structures after irradiation due to the methodological features of the technique [ 12 ]  . 
an increase in the frequency of abnormal comets in dependence on the concentration of alui was obtained with all three assays . our experience with the essen comet assay protocol suggests that the existence and a possible increase in the frequency of abnormal comets can normally be related to disturbances in cell culture conditions ( such as lower ph , serum starvation ) , cell death in general or apoptosis ( unpublished results )  . 
thus , it looks as if most cells did not take up alui at all , and that the dna of those cells which took up alui , was heavily degraded resulting in abnormal comets . 
 the problem with this explanation , however , is that the analysis of chromosomal aberrations argues against it , because markedly more cells showed at least one dicentric ( figure 5b ) , when compared with the number of abnormal comets ( figure 4 )  . 
one could argue that in those cells with , for example , only one dicentric the alui concentration might be too low to induce sufficient numbers of dsb to be detected in the comet assay . 
it is true that the average dispersion index of the dicentrics was 1.6 ( range , 1.12.0 without any relation to the alui activities applied ) , indicating that there were more cells with more than one dicentric than expected from a pure poissonian distribution . 
and due to the many sites that are potential points of attack in the genome by alui , penetration of alui will most probably result in a sufficient number of dsb to be detected in the comet assay . 
in addition , there is another aspect strongly indicating that it is not just a matter of too low alui concentrations and insufficient frequencies of dsb : if after alui penetration it might happen that the activity of the enzyme is too low to induce sufficient amounts of dsb to be detected in the comet assay , then one has to expect all transitions between almost no comet , short comets , long comets , and , perhaps , abnormal comets . 
thus , the discrepancy between the number of cells with at least one dicentric and the number of abnormal comets cannot be explained by too few dsb induced by alui . all these results taken together demonstrate that other factors , in addition to dna strand breaks , contribute to the outcome of the comet assay . 
 strahlentherapie und onkologie original article the influence of ca 125 and cea levels on the results of 18f - deoxyglucose positron emission tomography in suspected recurrence of epithelial ovarian cancer christian menzel , natascha dbert , nadja hamscho , konstantin zaplatnikov , sotirios vasvatekis , vanja matic , nicola wrdehoff , frank grnwald1 background and purpose : the follow - up of epithelial ovarian cancer ( oca ) consists of clinical investigation , sonography , and tumor markers ( tms ) , especially ca 125 . 
while there is still no consensus about the method of choice and the timing of its application , this study aims to find a tm threshold at which a pet would be appropriate . 
 material and methods : a total of 90 pet studies and the associated ca 125 values ( normal value < 35 u / ml ) were available in 71 patients during the follow - up after primary therapy for oca . 
in 67 / 90 studies the pet indicated a potential recurrence of oca and the median ca 125 was 166.7 u / ml ( range 13.34 , 060 u / ml )  . the tm levels were significantly different ( p < 0.001 , u - test )  . 
with one exception , there were no normal pet scans above ca 125 levels of 30 u / ml ; between 20 and 30 u / ml pet was positive in 4 / 7 studies . 
 material und methodik : es wurden insgesamt 90 pet - studien von 71 patientinnen in die untersuchung eingeschlossen , bei denen der aktuelle ca - 125 - wert ( normalwert < 35 u / ml ) vorlag . 
die pet liefert dabei offenbar in abhngigkeit von der hhe des ca - 125 - spiegels auf die tumorlokalisation hinweisende befunde , wobei die pet berwiegend bereits bei werten zwischen 20 und 30 u / ml positive befunde erbringt und ab einem schwellenwert von 30 u / l nahezu bei jeder patientin einen rezidivhinweis darstellen kann . 
ca 125 levels related to pet results in epithelial ovarian cancer introduction cancer of the ovaries ( oca ) predominantly occurs in postmenopausal women with a peak over the age of 60 . 
 after primary therapy they suffer an increased risk of an oca recurrence and must therefore be monitored closely . since conventional diagnostic imaging has only limited sensitivity to detect early oca recurrence , most patients are generally followed by endovaginal sonography , especially focusing on intraperitoneal fluids , and the evaluation of a tumor marker ( tm ) [ 14 ]  . 
 the concept of tms employs the detection of tumoror differentiation - specific proteins which may occur in the serum and have the potential to respond to therapy [ 17 , 18 , 22 ]  . these tms require relatively large numbers of tumor cells to become positive and thus lack high sensitivity . 
these problems are likely to be overcome by molecular tms , which consider tumor cells to be phenotypically different from normal cells and thus use the expression of different genes or the lack thereof and the consequences on protein syntheses , to target malignant clones . 
 ca 125 turns positive in approximately 80% of patients with epithelial oca , and its course reflects the patients tumor burden in > 90% of cases [ 9 ]  . 
it is generally agreed upon that a threshold level for ca 125 of 3540 u / ml being connected with rising levels during follow - up , is an indicator of oca recurrence . 
 material and methods we retrospectively analyzed the results of pet according to its ability to detect tumor remnants or recurrences of oca in relation to the most frequently evaluated ca 125 and cea in our patients . 
 there were 71 patients who underwent a total of 90 pet studies because of an otherwise unexplained elevation of the ca 125 , and this includes 19 patients who were investigated twice . 
this device allows the simultaneous acquisition of 47 contiguous slices at a thickness of 3.37 mm each , thus resembling an axial field of view of 16.2 c the patients were scanned between the base of the skull and the proximal femora , representing five to seven individual bed positions per patient . 
 all patients fasted for > 6 h prior to the examination to assure optimal conditions for the metabolism of the 18f - fdg , which was provided by commercial sources . 
blood glucose levels were checked as being within normal limits before the substance was administered . per bed position a 7 - min emission scan followed by a 3min transmission scan was done starting at the femoral / pelvic region . 
ergebnisse der positronenemissionstomographie ( pet ) bei ovarialkarzinom in bezug auf den ca - 125 - wert ( fr patientinnen mit ca - 125 - werten < 100 u / ml )  . menzel c , et al . 
even though the mean cea levels in those patients with positive oca detection were slightly higher , there was no true correlation between cea levels and the probability of a positive pet scan ( figure 2 )  . 
 pet negative pet positive positive negative discussion there is still no agreement on the most rational approach to further follow - up after primary therapy of epithelial oca , and in addition there is also still ongoing controversy about the initiation and selection of therapies once a recurrence is detected . 
limited data of the available studies , however , strengthen a thesis that treatment , especially chemotherapy , for oca recurrences is more effective in patients with a limited number of small lesions [ 4 ]  . 
the use of x - ray computed tomography ( ct ) or magnetic resonance imaging ( mri ) allows the detection of oca recurrences with a sensitivity of < 50% , while the specificity is about 75% or more . 
ca 125 levels related to pet results in epithelial ovarian cancer follow - up , the pet correctly identified 19 / 20 oca recurrences and 7 / 8 benign causes . 
 pet may thus detect recurrent disease at an earlier time than conventional and noninvasive techniques can do . however , there is yet no consensus regarding the true value of such findings , since earlier treatment does not necessarily lead to an overall increase in long - term survivors . 
such problems eventually may be overcome by an early diagnosis and a better characterization of patients regarding their biological tumor characteristics , since it could be shown that , e.g. , there is a negative effect of p53 overexpression on the outcome of treatment with radiochemotherapy [ 15 ]  . it is another limitation of our current study that no verification of pet findings could be obtained due to a lack of follow - up or the consequent initiation of therapy in pet - positive patients . 
in our current study , however , a rule of thumb for setting an indication for a pet could be a history of increasing ca 125 levels finally reaching levels close to or > 30 u / ml . 
in this situation pet seems to be the superior imaging modality as has also been suggested in other tumors , e.g. , in recurrent rectal carcinoma [ 6 ]  . 
 strahlentherapie und onkologie original article incidence , therapy and prognosis of colorectal cancer in different age groups a population - based cohort study of the rostock cancer registry rainer fietkau1 , heike zettl1 , sabine klcking1 , gnther kundt2 purpose : determination of frequency , treatment modalities used and prognoses of colorectal cancer in a population - specific analysis in relation to age . 
 in older patients with stage iii carcinomas , adjuvant treatment was done less frequently in accordance with the treatment recommendations ( < 60 years 8389% ; 6074 years 6777% ; 75 years 2936% according to stage and tumor localization ) ; in stage iv , the use of chemotherapy was reduced ( < 60 years 87.5100% ; 6074 years 3847% ; 75 years 3337% )  . 
 in the univariate analysis , age 75 years ( 4 - year survival rates : < 60 years 68 4.1% ; 6074 years 58 2.8% ; 75 years 38 3.7% ) , uicc stage and surgical treatment had a significant effect on prognosis . 
 key words : colorectal cancer elderly patients radiotherapy radiochemotherapy chemotherapy strahlenther onkol 2004 ; 180 : 47887 doi 10.1007 / s00066 - 004 - 1260 - z inzidenz , therapie und prognose kolorektaler tumoren in verschiedenen altersgruppen . 
eine bevlkerungsbasierte kohortenstudie des krebsregisters rostock ziel : bestimmung der hufigkeit , der therapiemodalitten und der prognose von patienten mit kolorektalen tumoren in einer bevlkerungsspezifischen analyse in bezug auf das alter . 
 ergebnisse : der relative anteil kolorektaler karzinome steigt mit zunehmendem alter ( < 60 jahre 7% ; 6074 jahre 12% ; 75 jahre 15% ; p = 0 , 001 )  . 
 mit zunehmendem alter wurden im stadium iii die behandlungen weniger hufig in bereinstimmung mit den therapieempfehlungen durchgefhrt ( < 60 jahre 8389% ; 6074 jahre 6777% ; 75 jahre 2936% gem stadium und tumorlokalisation ) ; im stadium iv nahm der anteil der patienten , die eine chemotherapie erhielten , mit zunehmendem alter ab ( < 60 jahre 87 , 5100% ; 6074 jahre 3847% ; 75 jahre 3337% )  . 
 in der univariaten analyse hatten das alter 75 jahre ( 4 - jahres - berlebensraten : < 60 jahre 68 4 , 1% ; 6074 jahre 58 2 , 8% ; 75 jahre 38 3 , 7% ) , das uicc - stadium und die chirurgische therapie einen signifikanten effekt auf die prognose . 
 1 cancer registry of rostock , department of radiotherapy , university of rostock , germany , 2 institute of medical informatics and biometry , university of rostock , germany . received : november 20 , 2003 ; accepted : april 29 , 2004 strahlenther onkol 2004 no . 
colorectal cancer in different age groups in der multivariaten analyse sind dagegen nur das alter 75 jahre ( p = 0 , 001 ) ; die durchfhrung einer chemotherapie ( kolonkarzinom ) oder radiochemotherapie ( rektumkarzinom ; p = 0 , 0040 , 001 ) und das tumorstadium ( p = 0 , 0450 , 001 ) unabhngige prognostische parameter . 
precise data on the incidence or on the therapeutic procedures and the prognosis of the different tumor entities depending upon the patients age at the onset of the disease are , however , scarce . 
however , these studies have the disadvantage that , in almost all cases , an age limit is specified and the patients under study were , for the most part , selected [ 9 ] ; as a consequence , usually only older patients in particularly good general state of health were reported . 
institutional results in this regard are difficult to interpret , as in these cases only those patients who were actually sent to a therapy are included , i.e. , were seen to be eligible for the respective therapy by the primary therapist . 
 the goal of this work was therefore to acquire more detailed data on frequency , therapy and prognosis of a selected malignant tumor in different age groups by means of a population - based cancer registry . 
furthermore , the treatment of colorectal cancer in its different stages is , by means of the recommendations of the german cancer society [ 16 ] , widely and comparatively well defined in germany [ 13 ] , and is therefore probably only subject to slight deviations . 
 material and methods as a basis for the data of the present study , the data documented for the diagnosis years 1999 and 2000 in the cancer registry of rostock were used . 
the catchment area for the cancer registry of rostock encompasses 600 , 000 inhabitants , i.e. , the cities of rostock and wismar , the rural districts of bad doberan and gstrow as well as parts of the rural districts of nordwestmecklenburg and nordvorpommern . 
the completeness of the data ( as compared to the estimated indices given by the robert koch institute ) was approximately 88% for the year 1999 , 91% for the year 2000 . 
 in addition to the master data of the patients , the kind of tumor , including the tumor stage or category ( according to the uicc classification of 1997 [ 21 ] ) , as well as the treatment modalities conducted are recorded . 
the rate of side effects of the respective treatment modalities as well as the exact execution of the respective chemotherapies can , due to the data acquisition , only be estimated , so that an evaluation in this regard was forgone . 
within the framework of the posttreatment care data , all of the patients death data , also in exchange with the central cancer registry of the new federal states in berlin , are reconciled . 
the information on local recurrences and the occurrence of distant metastases as well as the therapies for these are taken from the posttreatment reports of the practicing colleagues as well as from the individual outpatient tumor clinics . 
 for an exact analysis , the patients were divided into three age groups : patients < 60 years of age , patients between 60 and 74 years of age , and patients 75 years . 
colorectal cancer in different age groups second , variables yielding p - values 0.10 in the bivariate analysis were entered into the multivariate models to highlight some possible associations between the outcome and some covariates which were of borderline significance . 
 in all of the patients recorded , a semiannual inquiry is done by the central cancer registry of the new federal states of germany , by the colleagues involved , and by the registry offices in respect of the potential death data . 
in 1999 and 2000 , 6 , 016 patients were recorded in the cancer registry of rostock with tumor diseases ; of these , 644 carcinomas were localized in the colorectal tract . 
 in contrast to the age distribution of all tumors ( < 60 years : 34% ; 6074 years : 46% ; 75 years : 20% ) , there is a significant table 1 . 
characteristics of the patients with colorectal cancer diagnosed in the area of the cancer registry of rostock between 1999 and 2000 ( p - values for the comparison of different age groups )  . 
patientencharakteristik fr die kolorektalen tumorerkrankungen , die im bereich des tumorregisters rostock zwischen 1999 und 2000 diagnostiziert wurden ( p - werte zum vergleich zwischen den verschiedenen altersgruppen )  . 
in uicc stage i , the sole operation is standard therapy ; in uicc stages ii and iii , the german cancer society recommends operation in combination with a chemotherapy and irradiation . 
use of different treatment modalities for patients with rectal cancer by the different uicc stages : absolute number , percentages in brackets ( p - values for the comparison of different age groups )  . 
einsatz der verschiedenen therapiemodalitten bei patienten mit einem rektumkarzinom in verschiedenen tumorstadien : absolute zahlen , prozentangaben in klammern ( p - werte zum vergleich zwischen den verschiedenen altersgruppen )  . 
use of different treatment modalities for patients with colon cancer by the different uicc stages : absolute number , percentages in brackets ( p - values for the comparison of different age groups )  . 
einsatz der verschiedenen therapiemodalitten bei patienten mit einem kolonkarzinom in verschiedenen tumorstadien : absolute zahlen , prozentangaben in klammern ( p - werte zum vergleich zwischen den verschiedenen altersgruppen )  . 
univariate analysis of 4 - year survival ( with standard difference [ sd ] ) comparing uicc stage , age , localization , sex , and treatment of the primary tumor . 
univariate analyse der 4 - jahres - berlebensraten ( mit standardabweichungen [ sd ] ) zum vergleich der uicc - stadien , der altersgruppen , der tumorlokalisation , des geschlechts und der tumorbehandlung . 
colorectal cancer in different age groups if the entire population was analyzed ( tables 4 and 5 , figure 3 ) , there was no significant improvement of prognosis for the patients receiving adjuvant chemotherapy ( bivariate cox regression analysis : hazard ratio = 0.858 ; p = 0.313 ; log - rank test p = 0.715 ) or radiochemotherapy ( bi - variate cox regression analysis : hazard ratio = 0.783 ; p = 0.187 ; log - rank test p = 0.339 ) compared to the patients treated only surgically . 
 of course , adjuvant chemotherapy was mostly applied to patients with colon cancer , and radiochemotherapy to patients with rectal cancer ; therefore , a subgroup analysis was performed for uicc stages iii and iv ( figure 3 )  . 
the logrank test showed a significant difference between the survival curves of stage iii patients who received an adjuvant chemotherapy ( colon cancer ) or radiochemotherapy ( rectum cancer ) compared to patients treated only operatively ( p < 0.001 ) as well as for stage iv patients ( log - rank adjuvant chemotherapy [ p < 0.001 ] ; colon cancer or radiochemotherapy [ p = 0.02 ] ; rectum cancer )  . 
 as expected , uicc tumor stage was an independent prognostic parameter : compared to the reference group of patients with uicc stage i tumors , patients with uicc stage ii tumors ( adjusted hazard ratio = 1.768 ; p = 0.045 ) as well as patients with uicc stage iii tumors ( adjusted hazard ratio = 4.061 ; p < 0.001 ) and patients with uicc stage iv tumors ( adjusted hazard ratio = 13.550 ; p < 0.001 ) had a significantly worse prognosis . 
the latter means that the estimated risk of dying is 13.550 times greater for a patient with uicc stage iv compared to a patient with uicc stage i , adjusting for the other factors in the model . 
 age 75 years was an independent prognostic parameter in the multivariate model : compared to the reference group of patients < 60 years , patients 75 years ( adjusted hazard ratio = 2.544 ; p < 0.001 ) had a significantly worse prognosis . 
 discussion the data presented are based on a population - based cancer register ; they can be considered representative for the population in the cities and districts of the state mecklenburg - vorpommern examined due to the high data acquisition rate of 8892% . 
colorectal cancer in different age groups stage i stage ii 36 48 36 48 survival in months survival in months stage iii colon cancer stage iii rectal cancer figure 3 . 
the percentage of colorectal carcinomas in 40to 49 - yearolds is about 8% of all tumors ; the percent rate rises to 14% in 70to 79year - olds and climbs to 17% in patients 80 years . 
of course , it can not be excluded that individual treatment modalities for elderly patients were not reported ; however , for the younger patients the therapy procedures were registered completely , and there strahlenther onkol 2004 no . 
colorectal cancer in different age groups that patients > 70 years of age in good general state of health profit just as much from a palliative chemotherapy as younger patients . 
however , these results are based on seven randomized phase iii studies in which the percentage of patients > 70 years of age was only 15% of the total recruited [ 18 ] , or on a compilation of the literature [ 7 ] which showed that just 20% of all patients studied were > 75 years of age . this indicates a positive selection of patients in recruiting for the study . 
thus , our data indicates that , as in the population as a whole , the prognosis of patients worsens with advancing age , because , in contrast to the randomized studies , 27% of the patients in our study were 75 years . 
this view is supported by the data of the eurocare study [ 4 ] ; in this study , the 5 - year survival rate for rectal cancer patients as well as for colon cancer patients decreased with advancing age : from 49% to 57% ( rectal or colon cancer ) for patients aged 1544 years to 37% to 42% for patients > 75 years . 
there is , in fact , even a tendency to overtherapy , as in about 50% of the patients displaying uicc stage ii colon cancer an additional chemotherapy was applied which , according to the guidelines , would not have been indicated . 
whereas the majority of the patients up to 60 years of age ( 100% of all colon cancer patients , 87.5% of the rectal cancer patients ) at least received chemotherapy ( operation , radiotherapy ) , patients who exceed this age received chemotherapy only in considerably smaller numbers . most of these patients were either only operated on or retable 6 . 
this means that , especially in respect of adjuvant or palliative treatments which are standard for younger patients , the older patients did without . these results correspond to the literature data [ 5 ]  . 
 [ 19 ] examined the medicare data of 6 , 262 patients who were 65 years of age and who had developed a uicc stage iii colorectal carcinoma . an adjuvant chemotherapy was performed in the group of 65to 69 - year - old patients in 78% of the cases , in the group of 80to 84 - year - old patients it was only given to 34% , and amongst the 85to 89 - year - old patients 11% were administered this treatment . 
corresponding results were found by this same group of authors for rectal cancer [ 20 ] in 1 , 411 of the retrospectively charted patients who had contacted medicare because of a rectal cancer in uicc stages ii and iii . 
73% of the female patients between 65 and 69 years of age , 66% between the ages of 70 and 75 , 52% between 75 and 79 years of age , 39% between 80 and 84 years as well as 21% between 85 and 89 years of age received radiotherapy . 
colorectal cancer in different age groups how far this data corresponds to the actually applied therapy cannot be judged from this data alone , as not all americans are insured with medicare , i.e. , some have no insurance or are privately insured . 
 [ 2 ] also found that the use of chemotherapy or radiotherapy in the treatment of uicc stage iii colon cancer was reduced from 88% in patients < 55 years of age to 11% in patients > 85 years . 
because of fears that the patients will tolerate the chemotherapy / irradiation less well , it is preferred not to implement the patients of an advanced age suffer under increasing comorbidity , and there is the fear that complications will be less well tolerated in old age . 
 [ 10 ] came to similar conclusions for older patients with stage iii colon cancer by means of the data from the cancer registry of the jersey shore medical center . 
 strahlentherapie und onkologie original article radioprotective effects of amifostine in vitro and in vivo measured with the comet assay arndt - christian mller1 , steffi pigorsch1 , claus beyer2 , christine lautenschlger3 , jrgen dunst1 purpose : the authors investigated whether a potential radioprotective effect of amifostine ( wr - 2721 ) after in vitro or in vivo administration can be detected with the comet assay . 
moreover , it was determined whether radioprotection by wr - 2721 is dependent on the concentration of amifostine or alkaline phosphatase ( ap , the enzyme which activates the prodrug )  . 
 material and methods : in vitro administration of amifostine : freshly isolated lymphocytes from two healthy volunteers were incubated with different concentrations of ap ( 0210 u / ml ) and amifostine ( 05 , 000 g / ml )  . 
in vivo administration of amifostine : blood samples were collected from six postoperative rectal cancer patients before and after intravenous administration of amifostine 500 mg ( no pretreatment with radioor chemotherapy )  . 
a significant radioprotective effect ( p < 0.05 ) was seen after administration of amifostine in vitro for all concentrations investigated ( 2505 , 000 g / ml , initial dna damage )  . 
 key words : radioprotection amifostine comet assay alkaline phosphatase lymphocytes strahlenther onkol 2004 ; 180 : 51725 doi 10.1007 / s00066 - 004 - 1216 - 3 in - vivound in - vitro - quantifizierung radioprotektiver effekte von amifostin mit dem comet - assay ziel : die autoren untersuchten , ob ein potentieller radioprotektiver effekt von amifostin ( wr - 2721 ) nach in - vitround in - vivogabe mit dem comet - assay detektierbar ist . 
zudem wurde berprft , ob eine abhngigkeit der radioprotektion durch wr - 2721 von den konzentrationen an amifostin und alkalischer phosphatase ( ap , das enzym , welches das prodrug aktiviert ) besteht . 
des weiteren wurde die radioprotektion durch amifostin bezglich mglicher vorhandener interindividueller unterschiede untersucht . material und methodik : in - vitro - applikation von amifostin : frisch isolierte lymphozyten zweier gesunder spender wurden bei unterschiedlichen konzentrationen von ap ( 0210 u / ml ) und amifostin ( 05 000 g / ml ) inkubiert . 
in - vivo - applikation von amifostin : untersucht wurden leukozyten von sechs postoperativen rektumkarzinompatienten vor und nach infusion von 500 mg amifostin ( ohne radiooder chemotherapeutische vorbehandlung )  . 
zur beurteilung der radioprotektiven wirkung wurden dosismodifizierende faktoren ( dmf ) berechnet und der gepaarte t - test durchgefhrt . ergebnisse : der dna - schaden nach bestrahlung wurde durch alleinigen zusatz von amifostin in vitro nicht verndert . 
der comet - assay ist geeignet , kleine vernderungen der radiosensitivitt durch amifostin zu quantifizieren . schlsselwrter : radioprotektion amifostin comet assay alkalische phosphatase lymphozyten 1 department of radiotherapy , martin luther university of halle - wittenberg , halle , germany , 2 institute of clinical chemistry and pathobiochemistry , martin luther university of halle - wittenberg , halle , germany , 3 institute of biomathematics , martin luther university of halle - wittenberg , halle , germany . 
radioprotective effects of amifostine measured with the comet assay introduction amifostine is a selective radioprotector of normal tissues and was developed by the walter reed army institute of research of the us army to prevent their soldiers from a radioactive fallout . 
the radioprotective efficacy of the thiol amifostine ( wr - 2721 ) has been demonstrated in a recent randomized trial in which the drug significantly reduced the risk of radiation - induced xerostomia in head and neck cancer patients [ 4 ]  . 
the selectivity for normal tissue compared with tumors is explained by a better distribution of the drug to normal cells because of a normal ( not chaotic ) vessel architecture , a higher concentration of ap in the most tissues , and facilitated ( instead of passive ) diffusion by a polyamine transporter [ 14 ]  . 
 the single - cell gel electrophoresis ( scge , also called comet assay ) was established by stling & johanson [ 16 ] to assess dna damage in individual cells , embedded in agarose on a microscope slide [ 11 ]  . 
 [ 22 ] , is capable of detecting single - strand breaks ( ssbs ) , alkali - labile sites , and incomplete excision repair sites in individual cells [ 1 , 18 ]  . 
 reliable determination of intrinsic radiosensitivity in individual patients is a serious need in radiation oncology [ 13 ]  . the comet assay has been demonstrated to detect radiation damage even after relatively small radiation doses and can therefore be used in a clinical setting with conventional fraction sizes of about 2 gy . 
the experiments were created to test this hypothesis by using an intraindividual comparison , i.e. , the radiosensitivity of one individuals cells was measured before and after administration of amifostine . 
the first part of the experiments was performed under in vitro conditions to determine a possible dose dependency in the radioprotective effect of amifostine and to investigate the role of ap , the activating enzyme which converts the inactive prodrug amifostine into its active metabolite . 
peripheral blood cells were collected in citrate tubes from two healthy volunteers ( donor 1 : male , 24 years ; donor 2 : female , 27 years )  . 
the lymphocytes were separated from whole blood on sterile conditions using a ficoll hypaque technique [ 3 ] with a modified protocol of the institute of clinical chemistry and pathobiochemistry . 
 irradiation conditions and dna repair ice - cold sandwich - layer cells attached to microscope slides were irradiated with doses ranging from 0 to 8 gy of x - rays placed on piacryl plates ( tube size 15 ( cid : 1 ) 20 cm2 )  . 
for dna repair studies , cells attached to slides were incubated for 15 , 60 , and 120 min in complete medium ( 85% rpmi , 15% fcs ) at 37 c and processed as described below . 
a temporary layer of normal - melting - point agarose ( 1 , 000 l , 1% in pbs ) was utilized because of better adhesion of the other three layers and removed after solidification . 
radioprotective effects of amifostine measured with the comet assay single cells were suspended in low - melting - point agarose ( 85 l , 0.5% ) in pbs ( without repair ) or rpmi 1640 ( repair ) at the middle layer . 
after solidification , the top layer of lowmelting - point agarose was added ( 85 l , 0.5% in pbs or rpmi 1640 , depending on repair investigation )  . 
 estimation of radioprotection the radioprotective effect was expressed as dose - modifying factor ( dmf ) : dmf = ( % tail dna with amifostine ) : ( % tail dna without amifostine ) multiplication of a radiation dose with the factor results in the effective dose delivered to the tissue . 
to insure the activation of amifostine , the drug was first incubated with ap from calf for 15 min in 0.9% sodium chloride solution and then given to freshly isolated lymphocytes taken from two healthy donors . 
 the dna damage of isolated lymphocytes after irradiation with 6 gy was measured in the presence of amifostine alone , in the presence of ap alone , and in the presence of both at different durations of incubation time . 
there was no difference between samples with different incubation times suggesting that the duration of incubation had no influence on the amount of radioprotection . this experiment therefore clearly demonstrates that neither the prodrug amifostine itself nor the activating enzyme ap exert any radioprotection and that the activation of the prodrug occurs very rapidly . 
a radioprotective dose of amifostine ( 50 l / ml , final concentration ) was added to twelve increasing concentrations of ap for 15 min , mixed with lymphocytes ( proportion 1 : 1 ) and incubated again for 15 mthe final concentrations were 0.0150 u / ml for ap . 
initial dna damage after 6 gy ( expressed as % tail dna ) in control lymphocytes ( sample 1 ) , after addition of 1 , 000 g / ml amifostine ( sample 2 ) or 210 u / ml alkaline phosphatase ( sample 3 ) or both substances ( samples 46 , different incubation times of 0 , 15 , and 30 min )  . 
initialer dna - schaden nach 6 gy ( in % dna im schweif dargestellt ) in kontroll - lymphozyten ( probe 1 ) , nach zugabe von 1 000 g / ml amifostin ( probe 2 ) oder 210 u / ml alkalischer phosphatase ( probe 3 ) bzw . 
radioprotective effects of amifostine measured with the comet assay ever , yielded a significant radioprotection ( p < 0.05 ; figure 2 )  . higher concentrations did not further increase the radioprotective effect ; the differences in dna damage between a concentration of 0.5 u / ml ap and the maximum concentration were not significant . 
 impact of amifostine concentration on radioprotection . the amount of radioprotection in lymphocytes was examined at increasing concentrations of amifostine ( final concentrations 05 , 000 g / ml ) in the presence of ap . 
in the exponential repair phase ( 10 min ) , no significant change of the radiosensitivity was seen ; it is not clear whether this might be due to the technique or reflects a biological phenomenon . 
a definite radioprotective dose of amifostine ( final concentration 250 l / ml ) was incubated with a clearly activating concentration of ap ( final concentration 35 u / ml ) for 15 min , mixed with lymphocytes from two donors ( proportion 1 : 3 ) , and incubated again for 15 mafter irradiation with doses from 0 to 8 gy , the initial damages ( 0 min repair time ) and residual damages after 10 and 60 min of repair were measured with the comet assay . 
the statistical significance ( paired t - test ) and corresponding dmf were calculated for initial ( 0 min ) and residual dna damages ( 10 and 60 min )  . 
impact of concentration of alkaline phosphatase ( ap ) on initial dna damage ( in % tail dna ) after incubation with 50 g / ml amifostine and in vitro irradiation with 6 gy . 
 when the radiation damage was measured after repair of 10 or 60 min , a radioprotective effect was also visible . however , response to amifostine and irradiation in the lymphocytes of both volunteers did not appear unifora radioprotective trend in donor 1 ( average dmf of residual damage 0.91 ) and a significant effect in almost all samples of the other donor ( average dmf of residual damage 0.76 ) were observed ( figure 2 )  . 
 radioprotection after intravenous administration of amifostine in a clinical phase ii study , rectal cancer patients ( stage ii and iii ) who received standard postoperative radiochemotherapy were treated with amifostine 500 mg intravenously on days 15 and 2933 ; the clinical results of this study have recently been published in this journal [ 7 ]  . 
impact of amifostine concentration ( activated with 140 u / ml alkaline phosphatase ) and repair time on dna damage ( % tail dna ) in lymphocytes of donor 1 after in vitro irradiation with 6 gy . 
einfluss der konzentration von amifostin ( aktiviert mit 140 u / ml alkalischer phosphatase ) und der reparaturzeit auf den dna - schaden ( % dna im schweif ) von lymphozyten von spender 1 nach in - vitro - bestrahlung mit 6 gy . 
 discussion the comet assay is a rapid and highly reproducible technique for the evaluation of dna damage and can be used for measurement of radiosensitivity of normal and malignant cells under changing conditions ( cytotoxic drugs , hypoxia , radiomodulators )  . 
our present study was ( to our knowledge ) the first investigation in which the assay was used to determine small changes in individual radiosensitivity caused by the radioprotector amifostine . 
average values of dmf ( summary of experimental data from table 1 , donor 1 ) are represented related to amifostine concentration ( g / ml ) and repair time ( min )  . 
amifostine does not only reduce the initial dna damage ( repair time 0 min ) , but is even radioprotective during repair ( after 60 and 120 min , table 1 )  . 
mittelwerte des dmf ( zusammenfassung der experimentell gewonnenen daten aus tabelle 1 , spender 1 ) sind in abhngigkeit von der jeweiligen amifostinkonzentration ( g / ml ) und der reparaturzeit ( min ) dargestellt . 
the concentration of membrane - bound enzyme is not determinable , but indirect pharmacokinetic data like the fast plasma clearance ( 2.17 l / min ) of amifostine are available [ 19 ]  . 
it therefore remains questionable without amifostine , 0 min repair time with amifostine , 0 min repair time without amifostine , 10 min repair time with amifostine , 10 min repair time without amifostine , 60 min repair time with amifostine , 60 min repair time figure 3 . 
both diagrams show dna damages in % tail dna and increasing radiation doses for isolated lymphocytes with activated amifostine ( final concentrations were 250 l / ml for amifostine and 35 u / ml for alkaline phosphatase ) or without ( control experiments )  . the upper diagram represents the data of donor 1 , the lower of donor 2 . 
donor - specific mean dosemodifying factors ( dmfs ) were calculated for both volunteers ( donor 1 : 0.87 ; donor 2 : 0.78 ; mean dmf for both : 0.82 at 250 g / ml amifostine )  . 
significant radioprotection ( paired t - test , p 0.05 ) was investigated for initial damages in both , and for repair in most samples ( except for 6 gy 60 min repair ) of donor 2 . 
beide diagramme zeigen die dna - schden im schweif ( % ) bei steigenden energiedosen fr isolierte lymphozyten mit aktiviertem amifostin ( die endkonzentration fr amifostin betrug 250 l / ml , fr alkalische phosphatase 35 u / ml ) oder ohne amifostin ( kontrollexperimente )  . 
personenspezifische mittlere dosismodifizierende faktoren ( dmf ) wurden fr beide spender berechnet ( spender 1 : 0 , 87 ; spender 2 : 0 , 78 ; mittlerer dmf beider spender : 0 , 82 bei 250 g / ml amifostin )  . 
eine signifikante radioprotektion ( gepaarter t - test , p 0 , 05 ) wurde bei allen initialschden beider probanden und in der reparatur bei den meisten proben von spender 2 ( auer 6 gy 60 min ) gemessen . 
8 urban & vogel radiation dose ( gy ) without amifostine , 0 min repair time with amifostine , 0 min repair time without amifostine , 10 min repair time with amifostine , 10 min repair time without amifostine , 60 min repair time with amifostine , 60 min repair time radiation dose ( gy ) mller a - c , et al . 
radioprotective effects of amifostine measured with the comet assay without amifostine with amifostine without amifostine with amifostine radiation dose ( gy ) radiation dose ( gy ) without amifostine , with amifostine , without amifostine , with amifostine , without amifostine , with amifostine , 0 min repair time 0 min repair time 10 min repair time 10 min repair time 60 min repair time 60 min repair time without amifostine , with amifostine , without amifostine , with amifostine , without amifostine , with amifostine , 0 min repair time 0 min repair time 10 min repair time 10 min repair time 60 min repair time 60 min repair time radiation dose ( gy ) radiation dose ( gy ) without amifostine , with amifostine , without amifostine , with amifostine , without amifostine , with amifostine , 0 min repair time 0 min repair time 10 min repair time 10 min repair time 60 min repair time 60 min repair time without amifostine , with amifostine , without amifostine , with amifostine , without amifostine , with amifostine , 0 min repair time 0 min repair time 10 min repair time 10 min repair time 60 min repair time 60 min repair time radiation dose ( gy ) radiation dose ( gy ) figure 4 . 
the blood samples of the other four patients were irradiated with 2 , 4 , and 8 gy , and additional repair studies for 10 and 60 min were performed . 
blood samples were taken before and after infusion , irradiated in vitro ( on slide ) , and analyzed with the comet assay . dna damage was measured using % tail dna ( n = 50 per sample )  . 
the transition from cell survival to cell death ( necrotic and apoptotic fraction , 80% and 95% tail dna , respectively [ 2 , 15 ] ) is relatively small , and the dmf would become lower ( higher radioprotection ) , if it were calculated as a qualitative question . 
comparisons of protection factors calculated from survival fractions with dmfs measured by comet assay are very limited in their conclusion , because a qualitative endpoint ( lethality or no lethality ) is compared with a quantitative parameter ( different % tail dna )  . 
by contrast , in chinese hamster cells ( v79 - 171 ) a limiting value for surviving fraction after radiation doses of 240 gy was investigated which could not be increased by further elevation of the intracellular drug level corresponding with data from other human tumor cells ( ht - 29 / sp - ld , hela , me - 180vcii and ov - 2008 - vi ) [ 5 ]  . 
the results substantiate that small changes ( 1020% change in dna damage by amifostine ) in radiosensitivity are clearly detectable with the comet assay . clinical consequences include , that a single absolute dose of amifostine 500 mg ( corresponding to about 250300 mg / m2 ) yields an adequate radioprotective concentration in vivo and the restricted scope of application of amifostine to tumors with rare concentrations of ap is questionable . 
we have measured mean dmfs of about 0.87 in vivo ( table 3 ) which were only marginally improved by extremely higher concentrations of amifostine in vitro ( average dmf at 5 , 000 mg / ml in vitro : 0.80 , table 2 )  . 
comparing the efficacy of 500 mg amifostine with a recently published study concerning pelvic irradiation , it is indicated , that the same dose of amifostine leads to significant cytoprotective effects on rectal mucosa [ 12 ] supporting our results . 
radioprotective effects of amifostine measured with the comet assay strahlentherapie und onkologie aktuelles forum qui nescit simulare nescit curare wer nicht tuschen kann , kann nicht heilen anmerkungen zur aufklrung von patienten in der ( radio - ) onkologie johannes lutterbach1 , christian weissenberger1 , klaus hitzer2 , almut helmes3 hintergrund und ziel : die aufklrung von patienten , insbesondere in der onkologie , wird meist unter hervorhebung juristischer gesichtspunkte diskutiert . 
der vorliegende artikel verfolgt zwei ziele : die darstellung der aufklrung aus einem umfassenden kulturhistorischen verstndnis heraus und die diskussion der sich damit erffnenden chancen fr gegenwart und zukun material und methodik : analyse von historischer primrund sekundrliteratur sowie deutscher rechtsliteratur . 
 ergebnisse : anhand der begriffe aufklrung und einwilligung lassen sich die vergangenen 2500 jahre medizingeschichte schematisch in drei epochen unterteilen : epoche i : beginnend mit der griechischen antike bis weit in das 19 . 
 schlsselwrter : radiotherapie aufklrung informed consent prognose gesundheitskonomie strahlenther onkol 2004 ; 180 : 46977 doi 10.1007 / s00066 - 004 - 1253 - y on past practices and future directions of informed consent in ( radiation ) oncology background and purpose : informed consent , especially in oncology , is predominantly seen from a legal point of view . 
such a limited perspective runs the risk of reducing informed consent to some tiresome formalisthe present article highlights how the relationship between patient and physician might be enriched by a comprehensive historicocultural understanding of informed consent . 
 results : with the terms information and consent the last 2500 years of medical history can schematically be divided in three epochs : the first epoch started around 500 years bc , lasted until the 19th century ac and was dominated by the principle of " salus aegroti suprema lex . 
systematic requirements regarding patient information on planned medical interventions were not 1 klinik fr strahlenheilkunde , universittsklinikum freiburg , 2 rechtsanwalt , hamburg , 3 abteilung fr rehabilitationspsychologie , institut fr psychologie , freiburg . 
 nowadays , the debate regarding informed consent is dominated by the continuing differentiation of modern medicine , the development of medical practice as part of the service sector , and the changing ways how patients see themselves . 
the importance of informed consent will continue to rise in the future , while the emphasis of the physicians task will shift from information to counseling . informed consent will be increasingly established as independent service . 
 key words : radiotherapy informed consent prognosis health care management einleitung die aufklrung von patienten nimmt breiten raum in der tglichen arbeit des onkologisch ttigen arztes edies gilt insbesondere fr die gefahrengeneigte fachrichtung der strahlentherapie . 
es sind insbesondere die erst nach jahren oder sogar jahrzehnten auftretenden sptnebenwirkungen , die eine grndliche aufklrung angezeigt erscheinen lassen . das rztliche herangehen an die aufklrungsthematik ist wesentlich von forensischen aspekten geprgt . 
auch im schrifttum sowie bei wissenschaftlichen zusammenknften dominiert die medikolegale sichtweise der aufklrung : im september 1997 nur knapp 2 jahre nach ihrer grndung veranstaltete die deutsche gesellschaft fr radioonkologie ( degro ) in essen eine arbeitstagung mit dem titel radioonkologie und recht [ 14 ]  . 
spezifische anforderungen an die aufklrungspraxis des eigenen faches wurden ausfhrlich mit vertretern der rechtskunde diskutiert . im mrz 2001 errterte ein vorsitzender richter am oberlandesgerichts mnchen an dieser stelle in 22 thesen anforderungen an die patientenaufklrung am beispiel der strahlentherapie [ 17 ]  . 
 anhand der gerade genannten begriffe aufklrung und einwilligung lassen sich die vergangenen 2 500 jahre medizingeschichte schematisch , fr diesen berblick aber ausreichend , in drei epochen unterteilen : epoche i : griechische antike bis 19 . 
jahrhundert der auch heute noch hufig zitierte lateinische satz salus aegroti suprema lex ! bersetzt das wohl des patienten sei das oberste gebot ! lsst sich wie eine berschrift ber viele jahrhunderte medizinischen wirkens stellen . 
der oben zitierte satz msste also eher heien : das , was ich als arzt fr das wohl des patienten halte , sei oberstes gebot ! allerdings galt dies nur fr den umgang des arztes mit patienten aus der armen bevlkerungsschicht . 
aber fr die stadtphysici , die verpflichtet waren , sich um das wohl der armen zu kmmern , lsst sich eine solch paternalistische haltung belegen . welche rolle spielten in dieser situation aufklrung , wahrhaftigkeit und einwilligung ? das gesprch zwischen patient und arzt war zu damaliger zeit nicht selbstverstndlich . 
mit blick auf den sozial besser gestellten kranken hie es allerdings : der arzt belehrt den patienten und verordnet ihm nicht eher etwas , bis er ihn irgendwie davon berzeugt hat . 
wie dieser ihn zu einem erneuten eingriff bringen wollte , schildert der feinsinnige knstler in seinen lebenserinnerungen so : kurz vor meiner abreise lie mich herr hunter ersuchen , dringender ursache wegen zu ihm zu kommen . 
ich schrie , schlug blaue flecke und trat so lange mit meinen fen , bis ich mich befreite und herrn hunter , der schon mit seinen instrumenten zu operation in beabbildung 2 . 
der arzt karl johann osterhausen ergnzte 1798 den bekannten satz des fhrenden deutschen aufklrungsphilosophen immanuel kant mit blick auf die medizin folgendermaen : aufklrung ist der ausgang eines menschen aus seiner unmndigkeit in sachen , welche sein physisches wohl betreffen . 
so vertrat der internist karl ludolf von krehl die auffassung : wenigstens ist das der anfang vom ende unserer thtigkeit , sobald man alles erklren und [ den patienten ] wegen jeder einzelheit womglich fragen soll . 
der chirurg bernhard von langenbeck sagte 1885 : um eine operation zulssig zu machen , bedarf es des entschlusses des operateurs , sie zu unternehmen , und des freien entschlusses des kranken , sie zu erdulden . 
aber immerhin lautete die empfehlung eines chirurgischen lehrbuches von 1884 noch , unvernnftige und bertrieben ngstliche patienten , welche sich zu einer operation durchaus nicht verstehen wollen , zu narkotisieren , um auch gegen ihren willen die operation durchzusetzen . 
otto von bismarck berichtet in seinen memoiren : die behandelnden rzte waren entschlossen , den kronprinzen bewusstlos zu machen und die entfernung des kehlkopfes auszufhren , ohne ihm ihre absicht vorher angekndigt zu haben . 
ich erhob einspruch , verlangte , dass nicht ohne die einwilligung des patienten vorgegangen und , da es sich um den thronfolger handele , auch die zustimmung des familienhauptes eingeholt werde . 
 was dem rztlichen stand aus eigener kraft nicht gelang , nmlich den umgang mit dem kranken von sich aus neu zu gestalten , wurde ihm schlielich ber die rechtsprechung aufgezwungen . 
1894 entschied das reichsgericht in einem aufsehenerregenden urteil , dass ein rztlicher eingriff ohne einwilligung des patienten eine krperverletzung im sinne des ( heutigen ) 223 des strafgesetzbuches darstellt , selbst wenn die manahme medizinisch indiziert , nach den regeln der kunst durchgefhrt und im ergebnis erfolgreich ist [ 3 ]  . 
so bemerkte der zu seiner zeit berhmte und einflussreiche schottische arzt john gregory ( abbildung 4 ) zur aufklrung von ernsthaft erkrankten patienten : a deviation from truth strahlenther onkol 2004 no . 
es galt als inhuman , patienten mit der last des wissens ber eine ernste erkrankung zu beschweren , weil man es damals als sicher ansah , dass die aus dieser mitteilung folgende hoffnungslosigkeit und depressivitt lebensverkrzend und leidensvermehrend wirken mussten . 
der kranke empfahl sich unter aufrichtigen danksagungen , verlie das zimmer und strzte sich sofort vom gangfenster des ersten stockes herab , wobei er sich tdlich verletzte und beinahe einen assistenten der klinik erschlagen htte . 
storm nahm die nachricht mit freude zur kenntnis , begann wieder zu schreiben , vollendete im frhjahr des darauf folgenden jahres seinen schimmelreiter und starb im sommer 1887 [ 11 ]  . 
es ging also nicht mehr nur um das einfache recht des patienten , geplante eingriffe im sinne eines negativen abwehrrechts ablehnen zu drfen , sondern es wurde dem patienten das viel weitergehende recht auf ausfhrliche information zugesprochen , das fortan als voraussetzung fr eine selbstbestimmte entscheidung angesehen wurde . 
erstmalig in der medizingeschichte taucht in der urteilsbegrndung der uns so gelufige begriff des informed consent auf , was wrtlich mit informierte zustimmung oder freier mit einwilligung nach aufklrung bersetzt werden kann . 
die richter betonten ausdrcklich : der arzt verletzt seine pflichten gegenber seinem patienten und macht sich strafbar , wenn er fakten verschweigt , deren kenntnis fr eine einwilligung in eine geplante manahme von bedeutung ist . 
 das argument , dass die autonome entscheidung des einzelnen respektiert werden msse , wurde in der folgezeit von der modernen medizinethik , aber auch von den verschiedenen brgerrechtsbewegungen der 60er und 70er jahre aufgegriffen [ 12 ]  . 
in der viel gelesenen fachzeitschrift der american medical association formulierte der onkologe spaeth 1979 : the patient is the captain of his body , and decisions affecting that body can properly be made only by the patient himself . 
im vorwort heit es : wer als patient ber seine rechte informiert ist , kann sich aktiv am behandlungsprozess beteiligen ; wer als arzt seine pflichten kennt , kann patienten besser untersttzen . 
 die gegenwart der aufklrung im zweiten teil dieses artikels sollen zunchst bersichtsartig die wesentlichen inhalte dargestellt werden , ber die nach heutigem deutschen rechtsverstndnis bei der aufklrung mit dem patienten gesprochen werden muss . 
 die rechtsprechung verlangt die aufklrung des patienten ber den rztlichen befund ( diagnoseaufklrung ) : der patient muss erfahren , dass er krank ist und an welcher krankheit er leidet . 
 ber den zeitlichen verlauf seiner erkrankung : der patient muss erfahren , wie sich seine krankheit ohne behandlung entwickelt und ob die geplante behandlung vornehmlich auf die heilung oder auf die symptomlinderung zielt . 
 ber den verlauf der beabsichtigten behandlung ( verlaufsaufklrung ) : der patient muss erfahren , wie die behandlung abluft : anzahl der bestrahlungen , intervalle zwischen den chemotherapiezyklen , dauer des krankenhausaufenthalts etc . 
 ber das verhalten whrend der therapie ( therapeutische oder sicherungsaufklrung ) : der patient muss erfahren , wie er selbst zu einem komplikationslosen verlauf der behandlung beitragen kann , beispielsweise bei einer bestrahlung im mund - rachen - bereich durch verzicht auf das rauchen und eine konsequent durchgefhrte mundpflege . 
wenn ein patienten ber eine intensive krebstherapie mit hufig schwerwiegenden nebenwirkungen aufgeklrt wird , dann fragt der kranke fast zwangslufig zumindest nach dem grund fr diese therapie und dem zeitlichen verlauf des leidens also nach diagnose und prognose . 
hat der patient die notwendigkeit einer eingreifenden therapie akzeptiert , werden nicht selten alternative therapiemglichkeiten angesprochen , wobei sich der fragehorizont von etablierten schulmedizinischen verfahren bis weit in den paramedizinischen bereich erstreckt . 
 es stellt sich an diesem punkt die frage , ob dem zwang zur umfassenden aufklrung auf medizinischer seite ein ebenso umfassendes informationsbedrfnis auf seiten des patienten gegenbersteht [ 15 ]  . 
schrfer formuliert : befriedigt die geforderte aufklrungspraxis eher den juristen , oder begegnet sie tatschlich den wnschen der kranken [ 18 ] ? in einem interdisziplinren projekt untersuchen die ( nicht juristischen ) autoren derzeit systematisch die bedrfnisse von krebspatienten hinsichtlich der aufklrung . 
in der von januar bis juni 2003 dauernden pilotphase wurden 213 patienten der klinik fr strahlenheilkunde am universittsklinikum freiburg gebeten , zu beginn der strahlentherapie einen insgesamt 36 items umfassenden fragebogen auszufllen . 
 ein hnliches ergebnis ergab sich bei der frage wie wichtig sind ihnen informationen zur prognose ihrer erkrankung ? auch hier antworteten > 90% der befragten mit sehr wichtig oder wichtig . 
 auf die frage wie schtzen sie die fhigkeit ihres arztes ein , die prognose ihrer erkrankung zu beurteilen ? antworteten ber 80% der patienten : er beurteilt sie genau richtig . 
 die umfrageergebnisse belegen , dass dem rztlichen informationsangebot offensichtlich eine mindestens ebenso groe patientenseitige informationsnachfrage gegenbersteht . die rztliche kompetenz wird auch in schwierigen fragen als hoch eingestuman wird schlussfolgern drfen , dass das vom arzt gesagte deshalb auch ernst genommen wird . 
je nach zugrunde liegender fragestellung knnen diese wiederum in verschiedener technik ausgefhrt werden , z.b. durch variation der fensterung , der schichtdicke , des kontrastmittels , der schnittfhrung , des tracers etc . 
einen wesentlichen beitrag hierzu liefert das internet , das auf zahllosen websites in einer fr laien verstndlichen weise onkologisches wissen prsentiert [ 5 ]  . jenseits der virtualitt bieten z.b. 
 medizinische informationen stehen also heutzutage und ein ende der entwicklung ist vor allem mit blick auf die neuen medien nicht absehbar in groer flle , vielfach unabhngig von raum und zeit und kostenlos zur verfgung . 
rztliche aufgabe ist nun , dem bereits gut informierten patienten orientierungshilfen zu geben , daten zu wichten , prioritten zu setzen , um auf diese weise ein selbstbestimmtes handeln zu ermglichen . 
 noch bis vor wenigen jahrzehnten war es selbstverstndlich , dass der patient vom hausarzt an den niedergelassenen facharzt oder krankenhausarzt berwiesen , von diesem aufgeklrt und anschlieend auch behandelt wurde . 
aufklrung und behandlung gehrten deshalb untrennbar zusammen , aufklrer und behandler waren hufig identisch . diese verknpfung wird heute zunehmend hinterfragt . nicht nur in der krebsmedizin steigt die zahl von patienten und auch angehrigen , die sich zunchst unverbindlich informieren mchten . 
qualittsdemonstrierende ersatzindikatoren eine wichtige rolle . hierzu gehrt neben dem ansprechenden erscheinungsbild des krankenhauses oder der praxis und gut abgestimmten organisatorischen ablufen ganz entscheidend eine auf den einzelnen patienten zugeschnittene kommunikation des arztes . diese wird sich mehr und mehr an den wnschen des patienten orientieren . 
besteht klarheit , dass der patient die behandlung in einer konkreten einrichtung durchfhren lassen mchte , kann das aufklrungsgesprch dort in beiderseitigem interesse zielgerichtet gefhrt und auf die fr die geplante manahme relevanten aspekte fokussiert werden . 
 der gesteigerte aufwand , den solche unterredungen mit hufig von weit her anreisenden und gewhnlich gut vorinformierten patienten mit sich bringen , wird durch die gngigen gebhrenordnungen bislang nicht adquat abgebildet . 
8 urban & vogel strahlentherapie und onkologie original article prospective study on exclusive , nonsurgical strontium - / yttrium - 90 irradiation of pterygia bojan pajic1 , andreas pallas1 , daniel aebersold2 , guenther gruber2 , richard h . 
greiner2 purpose : prospective study to evaluate consecutive treatment results and to demonstrate safety and efficacy of nonsurgical , exclusive strontium - / yttrium - 90 ( cid : 1 ) - irradiation of nonoperated pterygia . 
 patients and methods : between november 1999 and march 2002 , 20 patients with 21 primary pterygia and six patients with recurrent pterygia after former surgery were treated with exclusive strontium - / yttrium - 90 irradiation up to a total dose of 3 , 600 cgy ( six fractions ) and 4 , 800 cgy ( eight fractions ) , respectively . 
 results : prior to irradiation the mean horizontal diameter of all pterygia was 2.6 mm and shrank to a mean diameter of 1.6 mm after treatment ( p = 0.0011 , students t - test )  . 
as to the therapeutic management , it is suggested to apply ( cid : 1 ) - irradiation prior to the development of an astigmatism - relevant pterygium , which requires excision . 
 key words : pterygium exclusive ( cid : 1 ) - irradiation irradiation for benign disease strahlenther onkol 2004 ; 180 : 5106 doi 10.1007 / s00066 - 004 - 1230 - 5 prospektive studie zur ausschlielichen nichtchirurgischen strontium - / yttrium - 90 - bestrahlung des pterygiums ziel : prospektive studie zur klinischen evaluation der wirksamkeit und sicherheit der ausschlielichen strontium - / yttrium - 90 - bestrahlung des nicht operierten pterygiums . 
 patienten und methodik : zwischen november 1999 und mrz 2002 wurden 20 patienten mit 21 primren pterygien und sechs patienten mit sechs nach exzision rezidivierenden pterygien mit einer ausschlielichen strontium - / yttrium - 90 - bestrahlung , gesamtdosis 3 600 cgy ( sechs fraktionen ) bzw . 
 ergebnisse : der durchschnittliche durchmesser der pterygien betrug vor der bestrahlung 2 , 6 mm und nahm nach bestrahlung signifikant auf 1 , 6 mm ab ( p = 0 , 0011 , student - t - test )  . 
 schlsselwrter : pterygium ausschlieliche strontium - / yttrium - 90 - bestrahlung bestrahlung gutartiger erkrankungen 1 ophthalmologic clinic pallas , olten , switzerland , 2 department of radiation oncology , university of bern , inselspital , bern , switzerland . received : september 4 , 2003 ; accepted : april 29 , 2004 strahlenther onkol 2004 no . 
exclusive strontium - / yttrium - 90 irradiation of pterygia introduction clinically , the pterygium is a rather well - perfused , gray tissue which expands , proliferating from the limbal epithelial stem cells , invading and destroying toward the center of the cornea , using the bowmans membrane pannus as a leading structure and destroying it progressively . 
 risk factors for a recurrence after resection are former surgery on the pterygium , especially in younger age , unprotected exposure to sunlight , and a positive family history [ 2 ]  . 
 the growth factors fibroblast growth factor ( fgf ) , vascular endothelial growth factor ( vegf ) , transforming growth factor - ( tgf - ) ( cid : 1 ) , and stem cell factor ( scm ) are increased in the pterygium [ 21 , 42 ]  . 
surgery alone did not always achieve satisfactory results [ 43 , 46 ] because of the provocation of reactive recurrences , which may show a more aggressive growth pattern [ 5 ]  . 
after the implementation of postoperative irradiation and / or intraoperative mitomycin c drops and thiotepa , very low recurrence rates were achieved [ 9 , 16 , 19 , 3234 , 39 , 45 ]  . 
while postoperative strontium - / yttrium - 90 ( cid : 1 ) - irradiation was very common during the third quarter of the last century , referral of patients from the ophthalmologist became rather rare following the routine integration of mitomycin c treatment and the successive standardization and amelioration of operative techniques [ 19 ]  . 
 the presumed etiology of the pterygia with its origin in limbal epithelial stem cells , whose replication is disturbed by sunlight , and its reactive inflammatory fibroblast proliferation has its analogies in intimal hyperplasia and further reactive diseases , which are successfully treated with irradiation [ 17 , 26 , 36 ]  . 
our study group has at its disposal data from 49 patients with 58 pterygia , who were exclusively treated with strontium - / - yttrium - 90 irradiation > 20 years earlier and are still followed up . 
in order to follow the immediate reaction of the pterygium and the surrounding tissue after irradiation , we initiated a prospective study of patients with early but symptomatic pterygia who did not undergo prior surgery and of patients with recurrences after recently performed excision and mitomycin treatment . the goal of this study was to demonstrate that pterygia are definitely prevented from proliferating by exclusive irradiation , that no surgery is needed to achieve this result , and that the indication for radiotherapy is given as in other benign diseases [ 17 , 26 , 36 ]  . 
 patients and methods from november 1999 to march 2002 , 26 patients ( 16 female and ten male ) with 27 pterygia were recruited and treated with exclusive strontium - / yttrium - 90 irradiation . 
five patients were immigrated from mediterranean countries and one from vietnam , i.e. , 23% of all patients came from a southern country with a more intensive sun exposure . all 27 pterygia infiltrated from the nasal limbus . 
 the patients , who were selected for treatment , had a progressively growing pterygium with moderate signs of activity , ocular irritation and signs of a beginning astigmatism with consecutive reduction of visual acuity . 
furthermore , the size of the pterygium , the distance of the corneal limbus to the head of the pterygium , was measured with a slit - lamp to control digital measuring . the photographs were taken with the fundus - camera ff 450 / ff 450 ir ( zeiss ) , which served for the digitized photomeasuring process of the eyes surface . 
with the videokeratoscope orbscan ii version 3.0 , a corneatopography was performed , which served for registration of the corneal astigmatis the strontium - / yttrium - 90 applicator used in our study is a convex plate of 12 mm diameter with the radioactive material at the inner surface . 
in this study , all patients with a primary pterygium had a fraction dose of 600 cgy and a treatment time of approximately 115 s ; the patients with recurrent pterygia had a fraction dose of 800 cgy and a treatment time of about 134 s . 
the changes of the pterygias size , the visual acuity and the astigmatism prior to and after treatment were evaluated on the basis of a two - tailed students t - test . 
tiefendosis der strontium - / yttrium - 90 - strahlung im gewebe . at the cornea , a gray and flat pannus remains , which shrinks continuously during the months following radiotherapy . 
the mean size of all pterygia was 2.6 1 mm ( range 15 mm ) before treatment , and 1.6 1 mm ( range 14.7 mm ) 10 months after treatment ( figure 2 )  . 
 discussion exclusive irradiation of a pterygium without prior surgical excision is still a widely unknown therapeutic approach , and it is not mentioned as a treatment option in the recent major review by hirst [ 19 ] either . 
 this prospective study therefore presents , for the first time , a new method of pterygium treatment , which was exclusively performed with strontium / yttrium ( cid : 1 ) - irradiation . 
the total dose of 3 , 600 cgy was given in six fractions for primary pterygia , and the total dose of 4 , 800 cgy in eight fractions for recurrent pterygia . 
 recurrences are well known to occur after excision and postoperative irradiation by means of the strontium applicator ( table 1 ) and also depend on the time interval between resection and first application . 
 in his study , hilgers [ 18 ] assumed that a dose up to 2 , 790 cgy may be associated with a recurrence rate of 20% . with an increased total dose up to 3 , 720 cgy , the rate of recurrence fell to 3% . 
 brenner & merriam [ 7 ] calculated the parameter / ( cid : 1 ) by means of a linear - quadratic formula and defined a value of 2 , 500 cgy , with a 90% confidence interval of 900 cgy . 
this fact was also recognized by van den brenk [ 44 ] , when he postulated that a fractioned large total dose is better tolerated by the tissue than the application of a single high dose . 
 considering the patients convenience and based on the data from the literature for other benign diseases and the data of postoperative pterygium irradiation , we presumed the optimal total dose for exclusive irradiation of a pterygium not yet treated surgically to be 3 , 600 cgy divided into six fractions . 
these reflections were the indication for postoperative irradiation . contrary to this indication , pterygia were not prevented after prior surgery in our study , but patients with existing pterygia were treated and progression had to be prevented . 
if stimulation and proliferation of fibroblasts are inhibited , this will presumably lead to a blocking of the angiogenesis and further obliteration of the vessels . we have never seen new vessels during and after treatment . 
telangiectasia of the conjunctiva , opacity of the cornea , corneal scarring , opacity of the lens , cataracts due to radiation , granuloma formation , atrophy and ulceration of the sclera are moderate and more severe late effects most often described after postoperative radiotherapy [ 4 , 13 , 14 , 18 , 23 , 30 , 38 , 40 ]  . 
the distance between the lens and the limbus corneae is 4 mm ; the effective dose at the lens is < 4% of the surface dose [ 4 , 14 ]  . 
nevertheless , several authors described opacity of the lens as a possible late side effect after ( cid : 1 ) - irradiation [ 4 , 15 , 18 , 23 , 40 ]  . 
very serious and often accumulated complications , combined with the probability of a higher rate of recurrence , are more frequently found in patients , who were treated with a single dose > 2 , 000 cgy [ 6 , strahlenther onkol 2004 no . 
in the literature , serious treatment complications such as edema and perforation of the cornea , infections , acute mature cataracts , scleral calcification and pain are described [ 37 ]  . 
 for the 26 patients in our study , exclusive strontium - / yttrium - 90 irradiation of the pterygium was a very efficient treatment method , which has proven to be successful without prior surgery . 
our procedure concerning the handling of the applicator , the selection of the single and total dose and the time schedule has also proven to prevent recurrences and to avoid side effects during a follow - up period of at least 24 months . 
immunohistochemical localization of basic fibroblast growth factor , platelet derived growth factor , transforming growth factor - ( cid : 1 ) and tumor necrosis factor - ( cid : 2 ) in the pterygiuacta histochem 1996 ; 98 : 195201 . 
 patients and methods : from january 2000 to october 2000 , 62 patients ( 73 heels ) with painful plantar heel spurs and a minimum pain history of 3 months were treated and evaluated in a prospective study . 
by means of a visual analog scale ( vas ) the patients had to self - assess the quantity of their heel pain once before , three times during and four times after rt at a longterm median follow - up of 28 and 40 months . 
older patients ( p = 0.04 ) and patients who avoided heel stress during the period of rt ( p < 0.01 ) demonstrated a better short - term response ( fu 1 ) ; both effects were lost 28 and 40 months after rt . 
moreover , significant differences in the extent of heel pain reduction by rt were observed in dependence on previous pain duration ( at fu 23 )  . conclusion : the results confirm the high efficacy of rt in painful plantar spur and add new aspects to formerly published data concerning the time course of changes in heel pain reduction . 
in addition , the initial success can be transformed into effective long - term results > 2 years after rt ; however , further improvement is not to be expected . 
as a new prognostic factor , the reduction of mechanical heel stress during rt may ameliorate the short - term results , whereas short heel pain history improves the long - term results . 
 key words : painful plantar heel spur low - dose radiotherapy benign disease analgesic therapy prognostic factors long - term results strahlenther onkol 2004 ; 180 : 5029 doi 10.1007 / s00066 - 004 - 1204 - 7 effektivitt und prognostische faktoren bei der radiotherapie schmerzhafter plantarer fersensporne hintergrund und ziel : die effektivitt der radiotherapie ( rt ) bei der behandlung des plantaren fersensporns wurde wiederholt beschrieben . 
die daten bezglich der schmerzlinderung , der langzeitergebnisse und der prognostischen faktoren variieren jedoch . in dieser arbeit wurden die effektivitt der rt ( schmerzreduktionsrate und langzeitergebnisse ) und prognostische faktoren bei der behandlung plantarer fersensporne untersucht . 
 patienten und methodik : in einer prospektiven studie wurden von januar bis oktober 2000 62 patienten ( 73 fersen ) mit einem schmerzhaften plantaren fersensporn und einer minimalen schmerzanamnese von 3 monaten behandelt und ausgewertet . 
eine quantitative selbsteinschtzung der fersenschmerzen mittels einer visuellen analogskala ( vas ) erfolgte vor , dreimal whrend und viermal nach abschluss der rt mit einer medianen nachbeobachtung von 28 und 40 monaten . 
patienten , die whrend der rt eine belastung der ferse vermieden , zeigten ebenfalls 6 wochen nach rt signifikant bessere behandlungsergebnisse ( p < 0 , 01 ; abbildung 4 ) ; beide effekte waren 28 und 40 monate nach rt nicht mehr nachweisbar . 
 schlsselwrter : schmerzhafter plantarer fersensporn radiotherapie gutartige erkrankung schmerztherapie prognostische faktoren langzeitergebnisse introduction the painful plantar heel spur is part of the heterogeneous group of degenerative benign diseases concerning the osseous and tendinous structures of spurs . 
due to microtraumatic changes and mechanical stress in the insertion of the plantar aponeurosis corresponding to increasing pressure and tractive force of the calcaneus , the osseous heel spur starts to grow toward the trajectories of the spongiosa in the base of the plantar aponeurosis [ 6 , 23 ]  . 
 using anti - inflammatory effects , radiotherapy ( rt ) of the painful plantar heel spur has been reported to be clinically effective at low costs [ 28 ]  . 
showed a higher rate of complete and partial remissions after a total dose of 5 gy in comparison to a total dose of 3 gy , whereas no further improvement was achieved by increasing the dose to 12 gy [ 27 ]  . 
 patients and methods from january 2000 to october 2000 , 62 patients ( 49 female , 13 male ) with refractory painful heel spurs were treated to a standard rt and evaluation protocol in our department . 
sufficient pain relief ( > 80% of initial pain extent ) was recognized in 18 / 73 heels ( 24.6% ) , partial improvement ( 5080% pain reduction ) in 27 / 73 heels ( 37.0% ) , and minor partial improvement ( 2050% pain reduction ) in 15 / 73 heels ( 20.5% ; figures 2a and 2b )  . 
inclusion criteria were a radiologically proven plantar heel spur , plantar heel pain with a minimum pain history of 12 weeks , age 25 years , and written consent of the patient . 
 all patients were treated according to a standard protocol , using high - voltage photons ( 10 mv , linear accelerator saturne i ; cgr , buc , france ; source - skin distance [ ssd ] 100 cm and one lateral field , sized 12 ( cid : 1 ) 17 cm )  . 
in 43 heels pain history was between 36 months , in eleven heels between 612 months , and 19 heels had a pain history of > 12 months . patients were divided into these three groups with regard to their duration of pain anamnesis . 
 plantar heel pain was evaluated during the rt series ( in the 1st , 2nd and 3rd week ) , shortly after rt ( immediately and 6 weeks after rt [ fu 1 ] ) , and during the long - term follow - up in august 2002 ( median 28 months after rt [ fu 2 ] ) and in august 2003 ( median 40 months after rt [ fu 3 ] ) , including a quantitative self - assessment of heel paquantitative assessment included duration of heel pain before rt , prior treatment , and intensity of pain , specified by a visual analog scale ( vas ; from 0 [ no pain ] to 10 [ maximal pain ] )  . 
radiotherapy of painful plantar heel spurs 100% 8099% 5079% 2049% < 20% 100% 8099% 5079% 2049% < 20% relative pain reduction ( end of rt ) relative pain reduction ( 6 weeks after rt ) figure 2a abbildung 2a figure 2b abbildung 2b 100% 8099% 5079% 2049% < 20% 100% 8099% 5079% 2049% < 20% relative pain reduction ( 28 months after rt ) relative pain reduction ( 40 months after rt ) figure 2c abbildung 2c figure 2d abbildung 2d figures 2a to 2d . 
radiotherapy of painful plantar heel spurs the evaluation at fu 2 revealed a plantar pain reduction in 64 heels ( 91.4% ; n = 70 ) , complete pain relief in 39 / 70 heels ( 55.7% ) , sufficient pain reduction in 42 / 70 heels ( 60.0% ) , partial improvement in 14 / 70 heels ( 20.0% ) , minor improvement in 8 / 70 heels ( 11.4% ) , and no improvement in 6 / 70 heels ( 8.6% ; figure 2c )  . 
within the 28 months of follow - up ( fu 2 ) pain progression was observed in nine cases ( 12.9% ) , which included four cases ( 5.5% ) with complete pain reduction after 6 weeks . 
61 / 68 heels ( 89.7% ) showed a pain reduction at fu 3 , complete pain relief was achieved in 36 / 68 heels ( 52.9% ) , sufficient pain reduction in 37 / 68 heels ( 54.4% ) , partial improvement in 15 / 68 heels ( 22.1% ) , minor improvement in 9 / 68 heels ( 13.2% ) , and no improvement in 7 / 68 heels ( 10.3% ; figure 2d )  . 
 patients who suffered from bilateral painful heel spurs ( n = 11 ) showed significant differences in the extent of heel pain , the duration of pain history , and the rate of pain relief between the right and the left heel . 
in three of these patients pain duration before rt was equal in both feet , in six patients the pain extent before rt was equal , and in four of these patients pain reduction after rt was identical . 
besides , patients avoiding heel stress during the periodof rt demonstrated also a significantly better treatment result 6 weeks after rt ( pearsons correlation coefficient = 0.467 ; p < 0.01 ) , albeit both effects were lost 28 and 40 months after rt ( figure 4 )  . 
die boxplots zeigen den median , die standardabweichung und die 25%und 75% - perzentilen der relativen fersenschmerzreduktion 6 wochen nach rt in abhngigkeit vom alter der patienten ( p < 0 , 05 )  . 
die boxplots zeigen den median , die standardabweichung und die 25%und 75% - perzentilen der relativen fersenschmerzreduktion 6 wochen nach rt in abhngigkeit von der subjektiven mechanischen fersenbelastung der patienten whrend der rt ( p < 0 , 01 )  . 
 discussion in germany , rt is a well - accepted and common indication to treat osteoarthritis and periarthritis , and although it is an acknowledged treatment for painful heel spurs [ 26 ] , no results of randomized trials evaluating rt against a control population are available [ 4 ]  . 
 further indications of low - dose rt besides osteoarthritic diseases were published , and positive effects on other inflammatory diseases such as chronic otitis media , hyperproliferative or fibrosing diseases such as ledderhoses , dupuytrens or peyronies disease were demonstrated [ 1 , 13 , 24 , 25 ]  . 
the synovial membrane may be the critical target of rt for osteoarthritis [ 29 ]  . the empirically based anti - inflammatory rt of benign diseases appears to act through specific modulation of different pathways of inflammatory reactions such as the nitric oxide ( no ) pathway in stimulated macrophages with reduction of no production and inos expression [ 8 ]  . 
low - dose rt shows interacting effects like downregulation of tumor necrosis factor - ( tnf - ) , increased expression of interleukin - ( il - ) 10 and induction of transforming growth factor - ( tgf - ) ( cid : 2 ) 1 , increased apoptosis , and reduction of expression of selectin [ 18 ]  . 
due to significant differences in the extent of heel pain and the duration of pain history between the right and the left heel of the eleven patients suffering from bilateral painful heel spurs , the individual heel was evaluated in itself and not to the single patient . 
we used high - voltage rt ( 10 mv ) and found a short - term response rate ( 6 weeks after rt ) of 82% and a rate of complete pain relief of 18% . 
the effect increased and heel pain decreased significantly until the follow - up visits 6 weeks and > 2 years ( 28 months ) after rt , showing that initial success can be transformed into effective long - term results . 
 [ 28 ] reported a delayed complete pain relief of 58% ( at median 41.5 months ) as well as 67% ( 12 gy ) and 72% ( 3 gy / 5 gy ; at median 3 years ) , respectively . 
37% of the patients reported slightly higher or lower pain extent during fu 2 to fu 3 ; the mean difference on the vas in the patients concerned , however , was only 0.6 in both directions and referred mainly to changes in pain extent of patients with persistent and chronic 36 months 612 months > 12 months pain history before rt figure 5 . 
radiotherapy of painful plantar heel spurs heel pareal pain recurrence was reported by 13% of the patients in the interval 6 weeks to 28 months after rt and by 5.9% in the interval 2840 months after rt . 
the latter data specify the observation of lindner & freislederer who found no further change in the results after a follow - up of 4 years and that of seegenschmiedt et al . who noticed 09% recurrences of heel pain after a median follow - up of 3.5 years [ 11 , 28 ]  . 
both effects , age and stress , were linked in our study and might be explained by the fact that older patients found it easier to take care of their heels , as they were often retired . nevertheless , these effects are only short - term ones and could not be observed in the follow - up evaluation 28 and 40 months after rt . 
 in accordance with several authors [ 5 , 15 , 28 ] and with some of our own previous data [ 22 ] , we can confirm the duration of heel pain history as a prognostic factor concerning heel pain relief . 
reduction of mechanical heel stress during rt may improve the short - term treatment results , whereas a short pain history ( < 6 months ) might influence the long - term results positively . 
 strahlentherapie und onkologie original article survival of patients in clinical stages iiiib of non - small - cell lung cancer treated with radiation therapy alone results of a population - based study in southern saxony - anhalt anja bollmann1 , thomas blankenburg2 , johannes haerting3 , oliver kuss3 , wolfgang schtte2 , jrgen dunst4 , heinz neef5 on behalf of the halluca study group * background and purpose : up to now , evidence about survival of patients with non - small - cell lung cancer treated with radiation therapy alone is only available from clinical studies . 
1 , 183 patients were diagnosed as having non - small - cell lung cancer , and 188 in clinical stages iiiib ( 15.9% ) were treated with radiation therapy alone . 
 key words : non - small - cell lung cancer radiation therapy alone clinical cancer registry halluca study strahlenther onkol 2004 ; 180 : 48896 doi 10.1007 / s00066 - 004 - 1184 - 7 berleben von patienten mit nichtkleinzelligem bronchialkarzinom in den klinischen tumorstadien iiiib nach primrer alleiniger strahlentherapie . 
ergebnisse einer versorgungsepidemiologischen studie im sdlichen sachsen - anhalt hintergrund und ziel : bisher existieren daten zum berleben von patienten mit nichtkleinzelligem bronchialkarzinom nach alleiniger strahlentherapie nur aus klinischen studien . 
deshalb wurde auf der basis einer epidemiologischen studie das berleben in einem unselektierten patientengut in abhngigkeit von verschiedenen prognosefaktoren analysiert und mit den berlebensdaten aus der literatur verglichen . patienten und methodik : zwischen april 1996 und september 1999 wurden im zuge der halleschen lungenkrebsstudie ( halluca - studie ) , einer multizentrischen feldstudie zur versorgungsqualitt von patienten mit bronchialkarzinom in den regie1 clinical cancer registry , martin luther university of halle - wittenberg , halle , germany , 2 martha maria hospital halle - dlau , halle , germany , 3 institute of medical epidemiology , biostatistics , and informatics , martin luther university of halle - wittenberg , halle , germany , 4 department of radiotherapy , martin luther university of halle - wittenberg , halle , germany , 5 cancer centre , martin luther university of halle - wittenberg , halle , germany . 
group : heinz neef , cancer center , martin luther university of halle - wittenberg ; johannes haerting , institute of medical epidemiology , biostatistics and informatics , martin luther university of halle - wittenberg ; wolfgang schtte , city hospital martha maria , halle - dlau ; jrgen dunst , department of radiotherapy , martin luther university of halle - wittenberg ; wolfram rosendahl , division of medical psychology , martin luther university of halle - wittenberg ; peter schmidt , clinical cancer registry , martin luther university of halle - wittenberg ; wolfgang slesina , department of medical sociology , martin luther university of halle - wittenberg ; mathias lange , social worker , martin luther university of halle - wittenberg . 
nach gesamtherddosen von < 50 gy , 50 bis < 60 gy und 60 gy wurden mediane berlebenszeiten von 4 , 2 , 10 , 7 und 18 , 9 monaten sowie 2 - jahres - berlebensraten von 8 , 7% , 13 , 4% und 35 , 2% erzielt ( tabelle 3 , abbildung 2 )  . 
 schlussfolgerung : patienten , die unter potentiell kurativer intention mit herddosen von 50 bis < 60 gy bestrahlt wurden , berlebten im vergleich zu den mit 60 gy bestrahlten patienten signifikant schlechter . 
conventional thoracic radiation therapy alone , however , has been the treatment of choice for patients with either locally advanced tumors , mainly stage iii , and also an alternative to surgery in patients with early stages who are unfit for major surgery . 
 currently , the role of radiation therapy is under investigation particularly due to multimodality approaches including radiation therapy [ 5 , 9 , 18 , 32 ] on one hand , and to new concepts in radiation therapy like hyperfractionated , accelerated radiotherapy [ 3 , 15 , 27 ] and dose escalation based on threedimensional conformal radiation therapy [ 1 , 13 , 29 , 34 ] or intensity - modulated radiotherapy [ 14 , 20 ] on the other . 
as a result of this , in recent clinical trials for assessing those new treatment strategies radiation therapy alone has degenerated to the mere control treatment [ 2 , 19 , 27 , 28 ]  . 
 to investigate current quality of care of patients treated with radiation therapy alone , we analyzed data from the halle lung cancer ( halluca ) study , a population - based multicenter study on treatment of patients with lung cancer in the districts of halle and dessau . 
 patients and methods study population between april 1996 and september 1999 , we performed a prospective population - based study in patients with lung cancer to evaluate patterns of care in this tumor type in a well - defined region . 
this halluca study recruited all newly diagnosed lung cancer patients in the districts of halle and dessau , a region of about 1.5 million inhabitants in the eastern part of germany . 
228 of them were treated with conventional radiation therapy alone . 28 patients with stage iv disease were excluded from this analysis , because they received thoracic radiation therapy with palliative intent only in order to improve symptoms . 
 data collection and analysis all tumor - relevant data were collected and managed by the clinical cancer registry of the cancer center halle , germany , by a modified version of the gieen tumor documentation system ( gtds )  . 
in spite of the considerable efforts taken some missing values remained , actually unavoidable in a register study . however , information on those is given in all of the displayed analyses . 
 concerning statistical methods we used absolute and relative frequencies for describing distributions and the standard methods in survival analysis ( kaplan - meier curves , log - rank test , cox regression ) for inference on survival times . 
day of diagnosis was preferably identified by day of histological confirmation of the tumor , or , in a descending order of evidence , by day of cytological confirmation , day of tumor staging or day of clinical diagnosis , if no information on a higher level was available . 
to validate and complement survival information , the data from the clinical cancer registry were compared to the death certificates collected by the local health institutions for the years 1996 / 1997 , 1998 / 1999 , and 2000 , and , additionally , each year ( since 1999 ) compared to the data from the common cancer registry of eastern germany in berl minimal follow - up was 12 months , the median follow - up time 33 months . 
median time between diagnosis of lung cancer and therapy onset was 22 days ; in 67.6% ( n = 123 ) of the cases , radiation therapy started within the first 4 weeks after diagnosis . 
within the group of patients curatively radiated we found a strikingly high number of doses between 50 and < 60 gy ( n = 78 ) compared to the number of patients radiated with 60 gy ( n = 41 )  . 
 overall treatment time is an important determinant for the effectiveness of fractionated radiation therapies , because under the assumption of a constant dose increasing treatment time reduces local tumor control . 
under the assumption that within a conventional regimen ( 1.82.0 gy per day , five times a week ) radiation therapy needs at last 28 days for a dose of 30 gy and 56 days for 60 gy , figure 1 shows the proportion of patients treated in time . 
it can be seen that 71.4% of the patients ( n = 130 ) were treated in time , whereas 28.6% ( n = 52 ) had a prolonged dose delivery . 
 to assess the influence of prognostic factors on survival , we investigated tumor stage , performance status at time of diagnosis , radiation dose , age , and sex in univariate as well as in multivariate analyses . 
for univariate analysis dose groups of < 30 gy , 30 to < 40 gy and 40 to < 50 gy were amalgamated to a dose group of < 50 gy , because these were observed to reflect palliative treatments and therapy ceasings ( n = 29 )  . 
the number of therapy ceasings in the dose groups of 50 to < 60 gy and 60 gy was low ( n = 2 and n = 1 , respectively ) , which enables a solid comparison of the latter two , curatively intended dose regimens . 
median survival times stratified by tumor stage ranged between 18.8 months in tumor stage i and 7.3 months in stage iiib , 2 - year survival rates between 24.2% dose 60 gy 50 to < 60 gy < 50 gy figure 2 . 
information about performance status , in general considered also an important prognostic factor for survival in lung cancer patients , was available only in 63.8% ( n = 120 ) of our patients with radiation therapy alone . 
 as the categories of the single ecog classes would comprise not enough cases , we amalgamated ecog classes 0 and 1 to describe patients with good performance status , and ecog classes 24 to describe patients with poor performance status . 
 multivariate survival analysis ( cox regression ) in a multivariate survival model the influence of the radiation dose as the prognostic factor of main interest was adjusted for tumor stage , performance status , age , and sex ( table 7 )  . 
as it is virtually impossible to achieve complete documentation in epidemiologic studies , the halluca study succeeded at last in improving data quality to a level that allows detailed population - based analyses of the current status of therapy in lung cancer patients and delivered valid information about the actual situation of quality of care . by contrast , clinical trials use strict inclusion criteria , resulting in a selection of patients . 
the differences in survival compared to data from major single institutions or prospective studies suggest a referral bias in this tumor type . we assume that there might be differences in treatment modalities with a certain proportion of patients with localized nsclc who receive no immediate specific treatment . 
this assumption is supported by the fact that we have observed , on one hand , a relatively high frequency of patients in poor general condition , and on the other , a high number of therapy ceasings , especially in low - dose groups . 
under the assumption that combined - modality therapy is mainly administered in patients with better general condition , such treatment selection criteria would necessarily lead to a more unfavorable selection of patients who undergo definitive radiation therapy alone . 
 comparison with data from clinical studies , as detailed population - based data in treatment of lung cancer are missing , and it should always be kept in mind that comparability is limited by the differing study designs . 
additionally , most of the clinical trials we discuss were conducted before the current international system for staging lung cancer was established by mountain and used the older classifications of uicc or ajcc [ 21 ]  . 
also , diagnostic , radiation , and treatment modes frequently do not obey to nowadays standards ; for example , thoracic ct was used for staging not before the mid 1980s ; the three - dimensional treatment planning has been used only recently . 
stadienabhngige berlebenszeit in monaten ( adjustiert nach alter , geschlecht , leistungszustand und gesamtherddosis )  . the second important observation in our investigation concerns the variation in dose prescription and the impact of radiation dose on survival of potentially curatively irradiated patients . 
an improvement of the effect of radiation therapy with increasing dose was already found as early as in the 1970s by the rtog studies 73 - 01 and 73 - 02 [ 23 , 24 ]  . 
only 3and 5 - year survival rates could be extracted from the rtog protocols 73 - 01 and 73 - 02 which are based on 707 patients in all localized tumor stages : 3 - year survival rates after total doses of 40 , 50 , and 60 gy were 6% , 10% , and 15% , respectively , this superiority of the 60 gy group vanishing after 5 years where survival rates of 6% were observed in all dose groups [ 23 ]  . 
this could be due to the large variation of radiation dose in our three groups , whereas in the rtog studies doses were fixed to the reported values in advance . 
 a further explanation for the differing results might be a bias in our study that could have been coming in because the physicians have determined the applied dose in the course of therapy depending on tumor response and the patients state . thus it can be speculated that especially the patients with a good prognosis received higher doses . 
this thesis is supported by the observation that , compared to the literature , survival rates in our study are inferior in the low - dose groups but superior in the 60 - gy group . 
statistical adjustment for tumor response and patients state in the course of treatment , however , was not possible , as this information was not collected in the halluca study . 
 there is no recent evidence from clinical studies about survival time with doses of < 60 gy , because with the results from the rtog studies a dose of 60 gy became the international standard for curative radiation therapy . 
the first , originally initiated to compare radiation therapy alone to combined radiochemotherapy , showed a median survival of 10 months and 2and 3 - year survival rates of 14% and 5% , respectively , in 177 patients mainly with locally advanced lesions after a dose of 65 gy [ 19 ]  . 
survival of patients with nsclc treated with radiation therapy alone ated radiation therapy to standard radiation therapy ( 60 gy ) , reported a median survival of 13 months and 1 - , 2 - , and 3 - year survival rates of 55% , 21% , and 13% , respectively , in 225 patients with approximately 60% in stage iiia / iiib [ 27 ]  . 
stage - dependent survival has rarely been investigated [ 4 , 26 ] ; most studies were restricted to only early ( i and ii ) or only locally advanced tumors . 
showed that survival was significantly longer in the tumor stages i and ii , in comparison to stages iiia and iiib , but no difference was seen between stages i and ii [ 26 ]  . 
saw no statistically significant influence of tumor stage in a univariate analysis ; however , 95 of the 148 patients in stages iiia oder iiib had received , either sequentially or concurrently , an additional chemotherapy [ 4 ]  . 
 most of our own data on stage - dependent survival are below those from the literature which can be most probably explained by the different study designs and the issues on patient selection already discussed . 
 in the literature , median survival in stage i is reported to be between 15 and 27.9 months , and 2 - year survival rates range between 35% and 56% [ 4 , 10 , 16 , 22 , 26 , 30 ] ; in stage ii these figures amount to 17.9 months and 3344% , respectively [ 4 , 26 ]  . 
gave median survival times of 11.3 months , and 2 - year survival rates of 22% ; in stage iiib these were 9.8 months and 18% [ 26 ]  . 
 our study , according to its main goal of investigating medical care in our region , was not a randomized intervention trial , and therefore we expect a certain mixing of distinct effects caused by dose changes in the course of treatment , that are subsumed under the dose effect . 
 conclusion in summary , our results suggest that the survival of patients with nsclc after radiation therapy alone in routine daily practice might be inferior to that observed in clinical trials and retrospective analyses of major single institutions . 
the most likely explanations for low survival figures are a decreasing use of radiation therapy alone with restriction of single - modality therapy to very unfavorable subgroups and a selection bias in prospective investigations . 
furthermore , in patients potentially curatively treated we found a significant impact of dose on survival in multivariate analysis suggesting that , if radiotherapy is administered , any attempt should be undertaken to achieve a dose of 60 gy , thus mirroring the established therapeutic recommendations from clinical trials . 
grabenbauer2 , franz rdel2 , kerstin amann3 , stefan schultze - mosgau1 1 influences tgf - ( cid : 1 ) r - iiibackground and purpose : following preoperative radiotherapy prior to ablative surgery of squamous epithelial cell carcinomas of the head and neck region , wound - healing disorders occur . 
altered levels of tgf - ( cid : 1 ) 1 are reported to promote fibrosis and to suppress vascularization during wound healing , whereas expression of tgf - ( cid : 1 ) receptor - iii ( tgf - ( cid : 1 ) r - iii ) is associat1 treatment on tgf - ( cid : 1 ) r - iii - associated ed with vascularization . 
the aim of the study was to analyze the influence of anti - tgf - ( cid : 1 ) vascularization in the transition area between irradiated graft bed and graft . material and methods : wistar rats ( male , weight 300500 g ) underwent preoperative irradiation of the head and neck region with 40 gy ( four fractions of 10 gy each ; n = 16 animals )  . 
on days 3 , 7 , 14 , 28 , 56 , and 120 , skin samples were taken from the transition area between transplant and graft bed and from the graft bed itself . 
 results : a significantly higher expression of tgf - ( cid : 1 ) r - iii was seen in the irradiated and anti - tgf - ( cid : 1 ) 1 - treated graft bed in comparison to the group receiving preoperative irradiation followed by transplantation alone . 
the percentage of tgf - ( cid : 1 ) r - iii positively staining capillaries from the total amount of capillaries in the anti - tgf - ( cid : 1 ) 1 - treated graft bed was higher than in the group irradiated only . 
the total area of capillaries was also higher in the tgf - ( cid : 1 ) 1 activity in irradiated tissue undergoing surgery leads to a higher expression of tgf - ( cid : 1 ) r - iii and conclusion : neutralizing of tgf - ( cid : 1 ) increased vascularization . 
 key words : wound healing tgf - ( cid : 1 ) 1 tgf - ( cid : 1 ) r - iii radiation free grafts in vivo experiment vascularization exogene modulation von tgf - ( cid : 1 ) von bestrahltem gewebe 1 beeinflusst die tgf - ( cid : 1 ) r - iii - assoziierte vaskularisation bei der wundheilung 1 , 2 nach chirurgie im vorbestrahlten transplantatlager . 
die erhhte tgf - ( cid : 1 ) hintergrund und ziel : nach properativer strahlentherapie und chirurgie zur behandlung von plattenepithelkarzinomen im kopf - hals - bereich treten wundheilungsstrungen auf . 
experimentelle voruntersuchungen zeigten eine erhhte expression der transforming growth factor - ( tgf - ) ( cid : 1 ) - isoformen tgf - ( cid : 1 ) 1 - expression frdert die fibrosierung und vermindert die vaskularisation ; der rezeptor tgf - ( cid : 1 ) r - iii ist hingegen mit einer neovaskularisation assoziiert . 
ziel der untersuchung war die analyse des einflusses einer anti - tgf - ( cid : 1 ) 1 - antikrper - behandlung auf die ausprgung der tgf - ( cid : 1 ) r - iii - assoziierten kapillarneubildung im bergangsbereich zwischen bestrahltem transplantatlager und transplantat . 
 material und methodik : wistar - ratten ( mnnlich , 300500 g ) wurden mit einer dosis von 4 ( cid : 2 ) 10 gy im halsbereich properativ bestrahlt ( 16 tiere )  . 
an den tagen 3 , 7 , 14 , 28 , 56 und 120 nach operation wurden hautbiopsien aus dem bergangsbereich zwischen transplantat und transplantatlager gewonnen und immunhistochemisch gefrbt ( abc - pox - methode )  . 
 strahlenther onkol 2004 ; 180 : 52633 doi 10.1007 / s00066 - 004 - 1212 - 7 1 department of oral and maxillofacial surgery , university of erlangen - nuremberg , germany , 2 department of radiation oncology , university of erlangen - nuremberg , germany , 3 institute of pathology , university of erlangen - nuremberg , germany . 
role of tgf - ( cid : 1 ) 1 and tgf - ( cid : 1 ) r - iii in wound healing and vascularization ergebnisse : eine signifikant erhhte expression von tgf - ( cid : 1 ) r - iii wurde in der properativ bestrahlten und anti - tgf - ( cid : 1 ) 1 - behandelten gruppe im vergleich zur ausschlielich vorbestrahlten gruppe nachgewiesen . 
der anteil tgf - ( cid : 1 ) r - iii - positiver kapillaren an der gesamtkapillarflche war in der anti - tgf - ( cid : 1 ) 1 - behandelten gruppe grer . 
die vaskularisation ( gefanzahl je flche ) war in der anti - tgf - ( cid : 1 ) schlussfolgerung : die postoperative applikation von neutralisierenden antikrpern gegen tgf - ( cid : 1 ) 1 im vorbestrahlten gewebe fhrt zu einer erhhten tgf - ( cid : 1 ) r - iii - expression und zu einer vermehrten vaskularisation . 
 schlsselwrter : wundheilung tgf - ( cid : 1 ) sation 1 tgf - ( cid : 1 ) r - iii bestrahlung freie transplantate in - vivo - experimente vaskulariintroduction radiochemotherapy and surgery represent the treatment options for patients with advanced head and neck carcinomas [ 14 ]  . 
besides the direct cellular damages to fibroblasts , endothelial cells and leukocytes , radiation substantially influences the expression of cytokines , such as transforming growth factor - ( tgf - ) ( cid : 1 ) , vascular endothelial growth factor ( vegf ) and fibroblast growth factor 2 ( fgf2 ) [ 16 ]  . 
tgf - ( cid : 1 ) comprises a family of pleiotropic cytokines which are involved in regulation of vascularization and synthesis of the extracellular matrix ( ecm ) components [ 23 ]  . 
pathologic tissue responses may be due to the aberration in the regulation of the tgf - ( cid : 1 ) isoforms . our own in vivo studies showed long - lasting altered suprabasal expression levels of tgf - ( cid : 1 ) 1 in the irradiated graft bed following free flap transplantation [ 31 , 32 ]  . 
it is not known if tgf - ( cid : 1 ) r - iii could serve as a control parameter for an angiogenic therapy with the aim of increased vascularization . 
irradiation leads to impairment of microvessels in the affected skin ; therefore , an experimental approach to improve wound healing and vascularization in irradiated tis1 and tgf - ( cid : 1 ) sue should be evaluated by staining of microvessels [ 30 ]  . 
e - selectin has been shown to be expressed on microvessels , whereas detection of von willebrand factor ( vwf ) fails [ 15 , 22 ]  . mature vascular endothelium does not necessarily express endothelial cell markers like cd31 , cd34 and vwf simultaneously [ 38 ]  . 
does local application of anti - tgf - ( cid : 1 ) 1 following free flap transplantation in preirradiated tissues influence expression of tgf - ( cid : 1 ) r - iii at endothelial cells ? material and methods experimental design 16 male wistar rats ( weight 300500 g , age 2.5 1 months ; charles river wiga , sulzfeld , germany ) were used . 
the rats were kept in pairs in polycarbonate cages in accordance with the requirements of the german animal welfare act ( animal experiment application 621 - 2531.31 - 3 / 99 ) at a temperature of 22 0.5 c , 55% humidity , and a 12 - h light / dark cycle . 
 preoperative irradiation , transplantation of the free myocutaneous gracilis flap , and application of anti - tgf - ( cid : 1 ) 1 antibodies were carried out under inhalation anesthesia with strahlenther onkol 2004 no . 
role of tgf - ( cid : 1 ) 1 and tgf - ( cid : 1 ) r - iii in wound healing and vascularization isoflurane ( forene , abbott , wiesbaden , germany ) following modification of the circulation system of the anesthesia unit ( tiberius 19 , draeger , bremen , germany )  . 
time interval between end of irradiation and grafting was 28 1 days . transplantation of a free myocutaneous gracilis flap into the preirradiated neck region a free myocutaneous gracilis flap measuring 2.5 ( cid : 2 ) 2.5 cm was taken from the right groin and used as the flap model . 
 exogenous application of anti - tgf - ( cid : 1 ) daily intracutaneous injection of anti - tgf - ( cid : 1 ) 1 antibodies ( 1 mg / 500 ml pbs , af 101 - na , r&d , minneapolis , mn , usa ) between graft and graft bed was carried out on days 17 after transplantation . 
intraoperatively and on days 0 , 3 , 7 , 14 , 28 , 56 , and 120 following free flap transplantation , biopsies ( 1 ( cid : 2 ) 1 ( cid : 2 ) 0.5 cm ) were taken from each rats graft bed and the transition area between graft and graft bed . one biopsy each from the preirradiated neck region and the nonirradiated right groin region served as an intraindividual control . 
the biopsies on days 3 and 7 were taken before a renewed application of anti - tgf - ( cid : 1 ) group 2 served as a control group without antibody treatimmunohistochemical analysis of tgf - ( cid : 1 ) r - iii and e - selectin preparation of formalin - fixed samples and immunohistochemical staining of the epitopes using the avidin - biotin - peroxidase complex ( abc - pox ) were carried out as previously described ment . 
a protease solution consisting of trypsin - cacl2 solution 0.1% ( swine pancreas trypsin , icn biomedicals inc , eschwege , germany ; 0.2 g cacl2 , 200 ml tbs , ph > 7.8 ; in a water bath at 37 c ) was used to demask the epitopes . 
to prevent nonspecific binding , the slides were incubated with the blocking solution ( 500 mg skimmed milk powder , merck , darmstadt , germany ; 50 ml tbs , 50 ml tween 20 ) for 30 min at room temperature . 
the secondary antibody consisted of a polyclonal , biotinylated rabbit - anti - goat for tgf - ( cid : 1 ) r - iii staining and goat - anti - rabbit for e - selectin staining ( dako , glostrup , denmark , dilution 1 : 250 in tbs / bsa 2.5% , 30 min , room temperature )  . 
 subsequent chromogenic assay was carried out using avidin - biotin / horseradish - peroxidase complex ( abc / hrp complex , dako , 30 min , room temperature )  . 
 from each tissue sample three sections were obtained consecutively and processed on microscopic slides , with one serving as a negative control in each case ( identical treatment , but replacement of the incubation step with a primary antibody by incubation with pure bsa )  . 
 qualitative and quantitative analysis slides were examined qualitatively under a bright - field microscope ( aristoplan , leitz , wetzlar , germany ) at 1040 ( cid : 2 ) magnification for changes in the extent and localization of tgf ( cid : 1 ) r - iii and e - selectin expression in the antibody - treated and the nontreated transition area and in the irradiated graft bed . this was determined and compared with the control checks . three visual fields per section for each sample , animal , day , and group were digitized with 40 ( cid : 2 ) magnification using a ccd camera ( hamamatsu c2400 , bridgewater , nj , usa ) and the program optimas 6.5 ( stemmer , puchheim , germany )  . 
role of tgf - ( cid : 1 ) 1 and tgf - ( cid : 1 ) r - iii in wound healing and vascularization selectin - positive capillaries in figure 2b . 
tgf - ( cid : 1 ) r - iii and e - selectin staining in the transition area of the irradiated graft bed of animals without antibody treatment at day 7 after surgery : following irradiation and transplantation ( group 2 ) , a capillary - associated staining of tgf - ( cid : 1 ) r - iii ( a ) and e - selectin - associated staining ( b ) were observed in the transition area between the grafted tissue and the graft bed . 
postoperativen tag ohne anti - tgf - ( cid : 1 ) therapie : nach bestrahlung und transplantation ( gruppe 2 ) wurden eine tgf - ( cid : 1 ) r - iii - expression ( a ) und eine e - selectin - expression ( b ) im kapillarendothel im bergangsbereich gesehen . originalvergrerung 40 ( cid : 2 ) ; die spezifitt der frbung wurde durch die mitgefhrten negativkontrollen belegt . 
in order to analyze the kinetics of expression , the value of relative capillaryarea from total capillary area labeling per visual field was analyzed separately for the antibody - treated and the nontreated transition area between graft and irradiated graft bed . 
confirmatory comparisons between treatment and control groups were made using generalized estimating equations ( gees ) with day , treatment , and subject id as independent factors for appropriate analysis of repeated measurements per individual . 
all calculations were made using spss 10.0 for windows ( spss inc , chicago , il , usa ) and sas 8.1 ( sas institute , carey , ca , usa )  . 
strongest expression was observed between day 1 and 7 after transplantation ( figures 1a and 1c )  . staining was stronger in the anti - tgf ( cid : 1 ) 1 - treated group and could be detected in the later phase of wound healing compared to the nontreated group . 
vascular endothelial cells showed strong e - selectin staining without any diminished expression over time ( figures 1b and 1d )  . staining of e - selectin on nonendothelial cells was stronger and more intense than tgf - ( cid : 1 ) r - iii staining . 
 quantitative analysis the number of tgf - ( cid : 1 ) r - iii - positive capillaries is given in figure 2a and for efigure 1c abbildung 1c figure 1d abbildung 1d figures 1c and 1d . 
tgf - ( cid : 1 ) r - iii and e - selectin staining in the transition area of the irradiated graft bed of animals with anti - tgf - ( cid : 1 ) 1 antibodies at day 7 after surgery : following irradiation , transplantation and antibody treatment ( group 1 ) , an increased capillary - associated staining of tgf - ( cid : 1 ) r - iii ( c ) and increased staining of e - selectin ( d ) were observed in the transition area between the grafted tissue and the graft bed compared to the nontreated animals ( group 2 )  . original magnification 40 ( cid : 2 ) ; specificity of staining was confirmed by the shown negative control checks to each sample . 
postoperativen tag nach anti - tgf - ( cid : 1 ) therapie : nach bestrahlung , transplantation und antikrpertherapie ( gruppe 1 ) wurde eine erhhte anzahl tgf - ( cid : 1 ) r - iii exprimierender kapillaren ( c ) und e - selectin exprimierender kapillaren ( d ) im bergangsbereich im vergleich zur kontrollgruppe ( gruppe 2 ) gesehen . 
anzahl tgf - ( cid : 1 ) r - iiiund e - selectin - positiver kapillaren im bergangsbereich nach bestrahlung und transplantation : nach applikation von anti - tgf - ( cid : 1 ) 1 - antikrpern ( gruppe 1 ) war die anzahl tgf - ( cid : 1 ) r - iii - positiver kapillaren am 28 . 
die anzahl e - selectin - positiver kapillaren war ebenfalls erhht ( gruppe 1 ) und zeigte eine zunahme im zeitlichen verlauf ( p < 0 , 005 ) im vergleich zur unbehandelten kontrollgruppe ( gruppe 2 ; b )  . 
 capillaries per visual field regarding tgf - ( cid : 1 ) r - iii - expressing endothelial cells was seen in the transition area until the 28th postoperative day between the anti - tgf - ( cid : 1 ) 1 and the control group . 
the relative area was higher in the anti - tgf - ( cid : 1 ) 1 - treated transition area until the 28th postoperative day than in the nontreated group . 
the relative capillary area of e - selectin - expressing endothelium was higher in the anti - tgf - ( cid : 1 ) 1 - treated group than in the control group ( figure 2d )  . 
 discussion this study shows that exogenous administration of tgf - ( cid : 1 ) neutralizing antibodies to tgf - ( cid : 1 ) 1 is capable of influencing endogenous tgf - ( cid : 1 ) r - iii expression . 
these findings are consistent with the observations of shah who also reported an influence of neutralizing anti - tgf - ( cid : 1 ) 1 treatment on endogenous expression profile and biological changes in skin architecture in an excisional wound - healing model [ 34 ]  . different experimental studies reporting contradictory results after anti - tgf - ( cid : 1 ) treatment during wound healing in nonirradiated tissue may be explained by the pleiotropic and dosestrahlenther onkol 2004 no . 
e - selectin - positive relative capillary area was significantly higher ( p < 0.005 ) at the 56th and 120th day postoperatively compared to the nontreated animals ( group 2 ; d )  . 
relative kapillarflche tgf - ( cid : 1 ) r - iiiund e - selectin - positiver kapillaren im bergangsbereich nach bestrahlung und transplantation : nach applikation von anti - tgf - ( cid : 1 ) 1 - antikrpern ( gruppe 1 ) konnte am 28 . 
die e - selectin - positive relative kapillarflche in gruppe 1 war ebenfalls gegenber der unbehandelten kontrollgruppe ( gruppe 2 ) an den untersuchungstagen 56 und 120 signifikant erhht ( p < 0 , 005 ; d )  . 
therefore , a suitable experimental model to study the influences of modulation of tgf - ( cid : 1 ) - impaired wound healing should include a lack or suprabasal expression of tgf - ( cid : 1 )  . 
the animal model used in this experimental study showed significant activation and de novo synthesis of tgf - ( cid : 1 ) 1 following irradiation and surgery [ 32 ]  . 
it has been shown that total reference doses between 30 and 50 gy caused lesions in tissues that are comparable to those found in humans after radiotherapy [ 3 ]  . 
with regard to the three to four times higher turnover rate in rats , the time interval of 28 days between irradiation and transplantation corresponds to the clinical practice with a time interval of 68 weeks between radiotherapy and surgical oncology . 
 vascularization during wound healing in irradiated tissue was improved in the transition area of anti - tgf - ( cid : 1 ) 1 - treated rats , as shown by histomorphometry using markers of vascular endothelial cells , tgf - ( cid : 1 ) r - iii and e - select anti - tgf - ( cid : 1 ) treatment resulted in an increased total number of capillaries per visual field and an increased relative capillary area . 
reported an increased angiogenesis following anti - tgf - ( cid : 1 ) 1 treatment in gallbladder tumors of mice [ 13 ]  . however , eskild - jensen et al . 
experimental results in our model indicate that tgf - ( cid : 1 ) r - iii expression is a marker of neovascularization during wound healing in nontransformed tissue . comparing the amounts of capillaries per visual field , a decreasing number of tgf - ( cid : 1 ) r - iii - positive and an increasing number of e - selectin - positive capillaries were observed over time . 
tgf - ( cid : 1 ) r - iii - associated capillaries could not be detected after the 28th postoperative day even in the anti - tgf - ( cid : 1 ) treated group , whereas the number and relative area of e - selectin - positive capillaries were still increased . 
besides the well - characterized strong tgf - ( cid : 1 ) r - iii staining of tumor vessels , a variety of studies showed the presence of tgf - ( cid : 1 ) r - iii in nontransformed vessels [ 10 , 33 ]  . 
role of tgf - ( cid : 1 ) 1 and tgf - ( cid : 1 ) r - iii in wound healing and vascularization weaker than in tumor tissues , all tissues were found to be positive , at least in microvessels [ 4 , 33 ]  . 
the group described a strong increase of microvessel - associated tgf - ( cid : 1 ) r - iii expression during dermal wound healing in an in vivo model . 
eselectin was chosen as the reference marker of vascularization , because it is expressed very early during angiogenesis and is still expressed on mature vessels [ 21 ] especially in irradiated tissue following high - dose radiotherapy , e - selectin is a suitable marker for vascularization because of its long - sustained alteration of expression [ 25 ]  . 
our experimental findings reveal that in the early phase of wound healing , until the 7th postoperative day , the contribution of tgf - ( cid : 1 ) r - iii - positive vessels to the total vascularization is higher than the contribution of e - selectin - expressing vessels . experimental and clinical studies on healing of microsurgically anastomosed flaps showed sufficient perfusion of the transplant from graft bed at the 7th postoperative day . 
tgf - ( cid : 1 ) r - iii may be a suitable marker to control efficacy of the angiogenic therapy in the early phase . in contrast to the detection of newly formed microvessels by staining with e - selectin in the early wound - healing phase , tgf - ( cid : 1 ) r - iii staining is not influenced by the inflammation process itself and shows high specificity for endothelial structures , whereas e - selectin is expressed by different cell types during inflammation and angiogenesis [ 8 ]  . 
 acknowledgments this research project was supported by the federal ministry of education and research ( bmbf ) and the interdisciplinary center for clinical research ( izkf ) at the university hospital of the university of erlangen - nuremberg , project no . 
 strahlentherapie und onkologie original article neoadjuvant radiochemotherapy in locally advanced gastric carcinoma gunther klautke1 , thomas foitzik2 , kaja ludwig3 , peter ketterer4 , ernst klar2 , rainer fietkau1 background and purpose : gastric carcinoma is characterized by a high rate of local recurrences and distant metastases and is often not resectable due to locally advanced stage . 
the aim of this study was to examine feasibility and effectiveness of neoadjuvant radiochemotherapy ( rct ) for locally advanced , primarily nonresectable gastric carcinoma and to achieve curative resection . 
 patients and methods : 21 patients with locally advanced gastric cancer located in cardia ( n = 17 ) and corpus ( n = 4 ; seven ct3 ; 14 ct4 ; 18 cn + ; all cm0 ) with a median age of 61 years were scheduled to receive neoadjuvant rct . 
therapy consisted of a conventionally fractionated , conformal radiotherapy using the shrinking - field technique ( 1.8 gy to 45 gy + 5.4 gy ) and chemotherapy using cisplatin ( 20 mg / m2 , d15 , 2933 ) , 5 - fluorouracil ( 5 - fu ; 800 mg / m2 , d15 , 2933 ) or paclitaxel ( 135 mg / m2 , d1 , 29 )  . 
following rct , tumors were classified resectable in 16 / 21 patients ( 76% ) ; 12 / 21 patients ( 58% ) were operated on , 11 / 12 achieved clear margins ( r0 )  . 
local control ( 4 years ) for patients following r0 resection was 89% . conclusion : neoadjuvant rct is feasible and locally highly effective but must be further investigated involving a higher number of patients . 
 key words : gastric cancer radiochemotherapy neoadjuvant therapy strahlenther onkol 2004 ; 180 : 695700 doi 10.1007 / s00066 - 004 - 9194 - z neoadjuvante radiochemotherapie bei lokal fortgeschrittenem magenkarzinom hintergrund und ziel : das magenkarzinom ist durch eine hohe rate an lokalrezidiven und fernmetastasen gekennzeichnet und im lokal fortgeschrittenen stadium oftmals irresektabel . 
ziel dieser studie war die berprfung der durchfhrbarkeit und effektivitt einer neoadjuvanten radiochemotherapie ( rct ) beim lokal fortgeschrittenen , primr nicht resektablen magenkarzinom mit dem ziel , die resektabilitt zu erreichen . 
 patienten und methodik : 21 patienten mit lokal fortgeschrittenen kardia ( n = 17 ) und korpuskarzinomen ( n = 4 ) des magens ( sieben ct3 ; 14 ct4 ; 18 cn + ; alle cm0 ) im alter von median 61 jahren wurden zur neoadjuvanten rct vorgestellt . 
die therapie bestand aus einer konventionell fraktionierten , konformalen strahlentherapie in shrinking - field - technik ( 1 , 8 gy bis 45 gy + 5 , 4 gy ) und einer cisplatinhaltigen ( 20 mg / m2 , d15 , 2933 ) chemotherapie mit 5 - fluorouracil ( 5 - fu ; 800 mg / m2 , d15 , 2933 ) oder paclitaxel ( 135 mg / m2 , d1 , 29 )  . 
 ergebnisse : die hmatotoxizitt war mit leukopenien grad 3 bei 10 / 21 patienten und thrombopenien grad 3 nach ctc bei 5 / 21 patienten moderat ; nichthmatologische toxizitten waren in 5 / 21 fllen fieber sowie eine pilzsepsis . 
nach der rct wurden die tumoren bei 16 / 21 patienten ( 76% ) als resektabel eingestuft ; 12 / 21 patienten ( 58% ) wurden operiert , 11 / 12 wurden r0 - reseziert . 
neoadjuvant radiochemotherapy in gastric carcinoma betrugen nach r0 - resektion 18 monate und 42% im vergleich zu 10 monaten und 0% bei den brigen patienten ( p = 0 , 035 )  . 
die lokale kontrolle ( 4 jahre ) nach r0 - resektion lag bei 89% . schlussfolgerung : die neoadjuvante radiochemotherapie ist durchfhrbar und lokal hocheffektiv , muss aber an greren patientenzahlen weiter berprft werden . 
this method allows patients with locally confined tumors without lymph node metastases to achieve 5 - year survival rates of 5090% [ 8 , 27 , 33 ] ; in stages iii and iv , however , the 5 - year survival rate rapidly drops to 1520% [ 23 ]  . 
in particular patients with a tumor located at the gastroesophageal junction ( global 5 - year survival rate of 27% ) display a poorer prognosis as compared to other localizations ( all other localizations : 61% [ 9 ] )  . 
randomized studies are presently being conducted on preoperative chemotherapy . for a long time gastric carcinoma in general has been regarded as a radiation - resistant tumor , so that patients with advanced tumors or locoregional recurrences were not even presented for radiotherapy . 
in a randomized chinese study [ 38 ] it was shown , however , that preoperative irradiation as compared to operation alone can improve the prognosis of patients with gastric carcinoma . 
even if reservations are called for in regard to the surgical technique [ 10 ] , it was indeed the same for both arms and the results at least prove the effectiveness of radiotherapy for gastric carcinoma . 
 female ( n ) male ( n ) age ( years ) tumor stage ut3 ( n ) ut4 ( n ) lymph node status un0 ( n ) un + ( n ) tumor localization cardia ( n ) corpus ( n ) 3171 ( median 61 ) radiochemotherapy ( rct ) has proven effective against gastrointestinal tumors in other localizations [ 7 , 17 , 18 , 19 , 24 , 28 , 31 , 36 ] , we submitted patients with advanced carcinoma of the cardia and stomach , in whom a curative resection was not indicated , to neoadjuvant rct within the framework of a phase ii study . 
the aim of this first data analysis is the representation of feasibility and effectiveness of this method of treatment . patients and methods patient characteristics from july 1 , 1997 to december 31 , 2003 , 21 patients ( three women , 18 men ) were given neoadjuvant treatment for locally advanced , histologically proven gastric carcinoma . 
the lymph node stations along the esophagus , up to the tracheal bifurcation , the small curvature of the stomach , and paraaortally to the height of lumbar vertebra ii were covered . 
dose - volume histograms were created separately for both lungs , the liver , the spinal cord as well as for each kidney , and the usual tolerances were taken into account . 
as it was a case of a preoperative treatment approach , a cumulative dose in the lung of maximum 14 gy was accepted , in the area of the spinal cord over short stretches a maximum dose of 44 gy was accepted . 
thereafter , therapy was changed to a combination of paclitaxel ( d1 , 29 ; 135 mg / m2 ; 3 - h infusion ) with cisplatin ( d15 , 2933 ; 20 mg / m2 ; 30 - min infusion ) with the goal of increasing local and systemic effectiveness . 
the evaluation of data and the survival according to kaplan - meier were calculated using the pc program relative to the date of securing the histology to the patients death or to the last time point of the follow - up period . 
the time between securing the histology and the proof of new lesions is given as the progression - free interval . results toxicity and feasibility preoperative rct could be completely administered to all patients . 
in addition to the usual prophylaxis of emesis with 5 - ht3 antagonists during chemotherapy , the patients received oral 5 - ht3 antagonists in the sole radiotherapy phase as well and , thus , had no problems with nausea or vomiting worth mentioning . 
one of these patients , however , refused surgery ; another patient had reduced lung function and a further two patients were not operated on due to a reduced general condition . 
one patient did not undergo surgery due to the occurrence of liver metastases ; another patient was diagnosed as having a second tumor in the pancreas and was also not operated on ( table 3 )  . 
 of the twelve patients operated on , three ( 25% ) displayed a pathohistologically confirmed complete remission ( pcr ) ; in a further two patients ( 17% ) only microfocal tumor residuals were to be found . 
thus , the rate of objectifiable remissions is 76% ( n = 16 / 21 ; table 3 )  . local recurrence rate , distant metastases , survival until now , 2 / 21 patients have developed an isolated local recurrence and 2 / 21 a local recurrence with distant metastases . 
for the remaining patients , local control is only 33% ( 25% )  . 8 / 21 patients developed distant metastases , representing a rate of distant metastasization after 4 years of 68% ( 13% )  . 
 hemotoxicity leukopenia grade 3 ( n ) thrombopenia grade 3 ( n ) nonhematologic toxicity fever ( n ) esophagitis grade 3 , 4 ( n ) fungal sepsis ( n ) table 3 . 
for the r0 - resected patients , the median total survival amounted to 18 months ( 4 months ) , and the 2 - year survival rate to 42% , as compared to a median survival of 10 months and a 2 - year survival rate of 0% for r1 and for patients not operated on ( p = 0.035 ; figure 1 )  . 
 comparison of both chemotherapy schemes a total of ten patients were treated with rct comprising 5fu and cisplatin and eleven patients with a combination of paclitaxel and cisplatin the 5 - fu group there were six t3 and four t4 tumors , in the paclitaxel group one t2 , one t3 and nine t4 tumors . 
in the 5 - fu and paclitaxel groups leukopenia grade 3 according to ctc occurred in 4 / 10 and 6 / 11 patients , respectively , and grade 3 thrombopenia according to ctc in 2 / 10 and 3 / 11 patients , respectively . 
even if these results cannot be accepted without criticism due to the different operative standards in germany in respect to lymph node dissection [ 1 ] , this study does , in principle , prove the feasibility and effectiveness of adjuvant rct in cases of gastric carcinoma . 
in this way , 16 of our 21 gastric carcinomas ( 76% ) which were primarily not assuredly resectable were translated into a resectable stage through neoadjuvant rct , and of the twelve patients who were actually operated on , eleven ( n = 11 / 21 ; 52% ) could have a curative resection . patients who could not be translated into an operable stage profited from simultaneous rct as well . 
it should , however , be taken into account here that our patients showed mainly t4 tumors and , for the most part , carcinomas of the cardia , which , per se , have a worse prognosis than other tumors localized in the stomach [ 9 ]  . 
even though this data is very heterogeneous , the authors were able to show that a dose of > 54 gy is important in order to achieve a locoregional control . 
here , an induction chemotherapy and subsequent rct with 30 gy were administered to patients with squamous carcinoma of the lower esophagus ( n = 10 ) and adenocarcinoma of the gastroesophageal junction ( n = 15 )  . 
similar to our group , this working group was able to submit 13 / 27 patients to an operative exploration , which led to an r0 resection in 10 / 27 ( 37% )  . 
in this respect , the median survival of patients not operated on was 10 months and of those operated on 18 months ; the 2 - year survival rate amounted to 0% and 42% , respectively ( p = 0.035 ; figure 1 )  . 
more recent studies show response rates of 2550% [ 3 , 25 , 37 ] ; the response rates are likely to be better with the use of more modern chemotherapy agents such as taxanes or irinotecan . 
neoadjuvant radiochemotherapy in gastric carcinoma be achieved , although shown only in small phase i / ii studies [ 15 ] ; nevertheless , these rates are still below those observed after rct . 
by comparison , the cr rates after chemotherapy are between 0% and a maximum of 7% [ 3 , 16 , 25 ] ; our patients achieved a rate of 14% after neoadjuvant rct . 
the prognostic importance of cr in gastric carcinoma is unclear ; in carcinoma of the esophagus , however , patients with cr after neoadjuvant rct have a higher median survival [ 4 , 6 , 35 ]  . 
although the paclitaxel group had mostly t4 tumors only , we were nevertheless able to achieve operability for just as many patients as in the 5 - fu group in which more than half had t3 tumors only . 
certainly , no precise statement can be made on the effectiveness due to the small number of patients , but the trend seems to speak for the use of paclitaxel . at a median follow - up time of 39 months , only one local recurrence has occurred in the group of operated patients . 
in our patient group , the local recurrence rate is 11% in the patients who underwent surgery as compared to 19% in the adjuvant rct arm of the study by macdonald et al . 
it must not be overlooked that we mainly treated patients with prognostically unfavorable carcinoma of the cardia ; even so , the rate of distant metastases in the operated patients as well , and in particular in lymph node - positive patients , was very high . 
at least for these patients it is to be discussed whether two to four courses of chemotherapy should be applied postoperatively , similarly to the treatment strategy for rectal carcinoma . 
a problem still unsolved in these patients is the high rate of distant metastases , which cannot be sufficiently improved by two courses of chemotherapy administered within the framework of neoadjuvant rct . 
postoperative adjuvant chemotherapy must be examined , at least for lymph node - positive patients . strahlentherapie und onkologie review article ductal carcinoma in situ of the breast increasing importance of radiotherapy as a part of the therapy approach rainer fietkau1 background : the treatment of ductal carcinoma in situ of the breast ( dcis ) has changed dramatically during the last decade . 
retrospective studies evaluated prognostic factors ( tumor size ; age ; margin width , presence of necrosis ; grading ) in order to define subgroups of patients whom adjuvant radiotherapy can be safely spared . 
 key words : ductal carcinoma in situ / dcis breast cancer radiotherapy strahlenther onkol 2004 ; 180 : 6829 doi 10.1007 / s00066 - 004 - 9192 - 1 duktales carcinoma in situ der brust . 
retrospektive untersuchungen bewerteten prognostische faktoren ( tumorgre ; alter ; weite des resektionsrandes ; nekrosen ; differenzierungsgrad ) , um subgruppen zu definieren , bei denen auf eine adjuvante bestrahlung ohne erhhung der lokalen rezidivrate verzichtet werden kann . 
 schlsselwrter : duktales carcinoma in situ / dcis brustkrebs strahlentherapie introduction ductal carcinoma in situ ( dcis ) of the breast is characterized by a proliferation of malignant epithelial cells without perforation of the basal membrane in the glandular duct of the breast . 
since the work done , among others , by rolf sauer [ 3234 ] showed that , in the case of invasive carcinoma , breast - conserving therapy was equivalent to mastectomy in early stages and therefore more and more patients with invasive cancer were treated by breast - conserving therapy [ 16 , 23 ] , this method was also tested for noninvasive dcis . 
 consequently , on the basis of the results of these studies and the current discussion in the literature an overview of the possibilities , indications and problems of radiotherapy in the treatment of dcis will be presented here . 
the few recurrences after mastectomy were traced back to either the presence of an undetected invasive carcinoma , the development of a new mammary carcinoma in the glandular tissue of the breast which remained behind after mastectomy , or a residual dcis focus . the treatment of dcis using mastectomy has never been compared in prospective randomized studies of breast - conserving therapy . 
using additional irradiation , the recurrence rate after breast - conserving therapy was able to be decreased to 8.9% ( 95% ci 6.811% ) ; the low level after mastectomy could , however , not be achieved . 
presumably , the patients prognosis would not be compromised by the higher local recurrence rate ; in randomized studies survival rates following breast - conserving therapy of 9899% after 5 years and 86% after 12 years were determined [ 12 , 20 , 46 ] , and after 15 years a survival rate of 92% following operation and irradiation was found in retrospective studies [ 42 ]  . 
therefore , it will also be impossible in the future to conduct a suitable randomized study . breast - conserving therapy and radiotherapy the goal of radiotherapy is a reduction of the local recurrence rate , which can amount to up to 40% after excision alone . 
by contrast , in the eortc study only patients with a tumor diameter of up to 5 cm and without evidence of an invasive carcinoma or pagets cancer were included . 
 the ukcccr study took in patients with a dcis that had been detected within the framework of preventive mam mography , as well as patients with a microinvasive carcinoma ( < 1 mm )  . 
 authors patients follow - up treat ment ( years ) ( n ) invasive recurrences ( % ) noninvasive recurrences ( % ) overall ipsilateral contralateral breast cancer recurrences ( % ) remarks fisher et al . 
the ukcccr study refers to very precise instructions on the histopathologic procedures and therefore assumes the percentage of affected resection margins to be minimal ; precise figures are not given . 
in particular , the 12 - year results of the nsabp study indicate that this advantage remains constant . expectedly , the survival rates and the frequency of distant metastases were not changed by radiotherapy . 
in the further course of the study this difference was balanced out again . in summary , the three randomized studies show that the local recurrence rate of invasive and noninvasive carcinoma can be significantly reduced by radiotherapy . arguments against radiotherapy even if radiotherapy does improve the local recurrence rate in randomized studies , the following arguments are brought forward against radiation treatment : ( cid : 127 ) the dcis is not a malignant underlying disease , but is typified by an excellent long - term prognosis . 
 [ 15 ] examined 134 , 501 patients with invasive carcinoma or dcis that had been taken up into the national cancer institutes seer prograof these patients , 37 , 379 were submitted to irradiation . 
the authors of the study cited above proceed from the assumption of a small increase which , in their opinion , should not influence the clinical decision for radiotherapy . ( cid : 127 ) irradiation could lead to a fibrosis of the breast , so that the posttreatment follow - up is more difficult and the evaluation of the mammogram is impeded . 
however , experienced radiologists only rarely have problems in this respect due to their experience with breast - conserving therapy nowadays . ( cid : 127 ) other side effects of irradiation in respect to the heart or the lungs should no longer be an argument , as these organs are not or only minimally affected by three - dimensional radiotherapy [ 37 , 44 ]  . ( cid : 127 ) because of the irradiation , necessary operations arising in the case of a recurrence such as a skin - sparing mastectomy with subsequent reconstruction are more difficult . 
this may be true for individual cases ; from the large randomized studies on breast - conserving therapy with irradiation there was , however , no report of more difficult healing processes after surgery for recurrence . ( cid : 127 ) in the case of an invasive recurrence , radiotherapy is no longer available . 
the therapy of choice in invasive recurrences is mastectomy ; in regulated follow - up these tumors are detected mostly < 5 cm , so that a postoperative irradiation is generally not necessary . 
irradiation of the lymphatic drainage areas is not affected by this [ 1 , 14 , 17 , 35 ]  . ( cid : 127 ) another argument against radiotherapy is the 6 - week treatment time and the cost of the treatment at about d 2 , 000 4 , 000.. 
however , the treatment period in comparison to the utility of radiotherapy plays only a subordinate role , as some of the patients , on the long run , are spared renewed therapy by irradiation . 
must be seen in comparison to the potential costs of a treatment for recurrences or the costs of a drug treatment , for instance chemotherapy or hormone therapy , which are significantly higher than those of a radiation treatment . in summary , most of the arguments are easy to rebut ; the potential carcinogenicity of irradiation must be taken seriously . 
there are too little long - term data in this regard for a definitive statement and we are obligated to gather this information . prognostic factors for the occurrence of local recurrences in retrospective and prospective studies different parameters were investigated which might be connected to the frequency of the local recurrence risk . tumor size the tumor size is not a sure prognostic parameter for a local recurrence in most of the studies . 
however , both randomized studies [ 4 , 13 ] found no significant difference between the local recurrence rate for tumors < and > 1 cm , whether irradiated or not . 
 [ 6 ] , wherein a local recurrence rate without irradiation of 18.1% for tumors with a size of 01 cm and 21.3% for tumors > 10 mm was reported . 
the restricting point must be made , however , that nearly all of the studies only covered tumors up to a size of 2 cm , whereby the percentage of tumors < 1 cm in the histopathologic evaluations of the randomized studies was approximately 70% . 
it is conspicuous in both randomized studies that patients whose tumors were > 1 cm profited more from irradiation , as the reduction of the local recurrence rates for tumors < 1 cm was 3040% ; for tumors > 1 cm , however , it was 5070% . 
 resection margin many authors consider the resection margin to be the most important prognostic parameter for a local recurrence as it is for invasive breast cancer [ 36 ] ; many questions remain unanswered , though . 
silverstein et al [ 40 ] reported that patients with a resection margin > 10 mm had a local recurrence rate of 4% at 8 years independently of whether they had been irradiated . 
 [ 25 ] observed a recurrence rate of 10.9% after excision alone and with a resection margin of > 1 mm ; after irradiation the figure was 4.9% ( not significant at this small number of cases )  . 
 [ 42 ] observed a lower local recurrence rate after additional irradiation at 9% for free resection margins as compared to 24% for afflicted resection margins ( p = 0.03 ) , which was confirmed by two french studies [ 8 , 45 ]  . 
 in summary , the resection margin after surgery is an important parameter for the evaluation of the local recurrence risk ; it is , however , unclear how large the resection margin must be : 1 or 10 mthrough an additional irradiation , the negative effect of an afflicted resection margin does remain , but becomes less or , in some part , no longer measurable . 
some work groups use an interstitial or percutaneous boost for tumor - afflicted resection margins [ 24 ] as usual in invasive breast cancer [ 18 , 19 , 28 ] or recurrent tumors [ 21 ]  . 
whether this actually leads to a further reduction of the local recurrence rate , as it does for invasive carcinoma , has not yet been proven . as in the experience of invasive mammary carcinoma , younger women have a higher local recurrence rate . 
in an overview , vicini & recht [ 48 ] found that younger women also more often have other unfavorable prognostic factors such as necroses , that they display unfavorable degrees of differentiation and have more advanced tumors . 
 the question therefore arises whether all patients should indeed undergo radiotherapy , or whether the choice of specific parameters ( see above ) allows to select patients with a particularly low risk of local recurrences , so that irradiation is not necessary . for this reason , the work group associated with silverstein [ 3841 ] proposed the van nuys prognostic index in 1995 . 
in this index the decisive parameters were , originally , the size of the tumor , the width of the resection margin , and the presence of comedo necroses as well as the grading . 
the data on the development of these scores are based on a total of 1 , 115 patients that were determined either with a mastectomy ( n = 401 ) , a breast - conserving therapy without irradiation ( n = 433 ) , or a conservative therapy with irradiation ( n = 281 )  . 
 in the analysis the tumor size , the age , the resection width , the degree of differentiation , and the presence of necroses were shown to be independent prognostic parameters . 
in the group with a medium probability of recurrence , the tumor - free survival rate after 10 years was 60% with excision alone and 80% with excision and radiotherapy . 
the adoption of this score into daily routine is problematic for a number of reasons . ( cid : 127 ) it is a case of retrospective data which has never been tested in prospective studies . 
the tumor sizes also differ : for a resection margin > 10 mm , the median tumor size was 12.5 mm in the radiotherapy arm but 9 mm after tumorectomy alone . 
in the case of smaller resection margins of 13 mm , the difference in median tumor size was between 14.5 mm ( tumorectomy and radiotherapy ) and 8 mm ( tumorectomy alone )  . 
in addition , an interstitial boost was administered in the early years , especially when the tumor margins were involved [ 24 ]  . ( cid : 127 ) other work groups which used the van nuys score on their collectives were not able to reproduce the data . 
 in the nsabp study [ 13 ] there were no differences in the rate of local recurrences according to the van nuys pathologic classification . ( cid : 127 ) all three randomized studies show that patients with an increased risk of recurrence ( e.g. , young women ; tumor - afflicted resection margins , appearance of comedo necrosis ) especially benefit from an adjuvant irradiation . 
however , the local recurrence risk is also significantly reduced in patients with a favorable risk profile . the extent to which patients with a low risk of local recurrences can do without an adjuvant irradiation is being determined within the framework of an rtog study . 
in this study patients with a dcis grade 1 or 2 , a tumor size < 2.5 cm , and a resection margin of at least 1 cm were included . 
 after 7 years the event free survival in the op + rt + tamoxifen arm was 83% as opposed to 77.1% in the op + rt arm ( p = 0.002 ) , corresponding to a reduction of 27% . 
the tamoxifen effect was especially pronounced when the margins of the incision were afflicted with tumors or the dcis displayed comedo necroses , i.e. , collectively in patients with a high risk of local recurrences . 
further analyses revealed that only patients whose tumors had estrogen receptors showed a benefit [ 2 ]  . contradictory results were yielded by the ukcccr study [ 46 ] , which randomized 1 , 576 patients with regard to tamoxifen . 
 in summary , both studies indicate that tamoxifen can reduce the risk in patient groups with a high risk of local recurrences , i.e. , age < 50 years , comedo necroses , tumor - afflicted incision margins , and estrogen receptor - positive tumors . 
how ever , there is no indication that the other patient groups , in particular women > 50 years of age with good prognostic parameters , benefit from adjuvant administration of tamoxifen in addition to radiotherapy . 
 details in the guidelines for the use of radiotherapy in the guidelines of the nci ( goc / cdr0000062787.html ) , breast - conserving therapy and irradiation without tamoxifen are named at the top of the list ; second on the list is mastectomy without the application of tamoxifen . 
this was also confirmed in a recently published review [ 7 ]  . in the guidelines of the german cancer society ( krebsgesellschaft.de ) postoperative irradiation is in general seen as being indicated . 
however , it is pointed out that in the case of a tumor size < 2 cm , a low grade and a 10 - mm safety clearance , irradiation can be forgone . 
the guidelines of the german cancer society are , in this sense , more restrictive than the nci recommendations . in the guidelines of the ago ( ago - online.de ) , postoperative irradiation is confirmed as having an evidence level of ib . 
according to these guidelines , the value of radiotherapy is questionable in cases of a tumor < 23 cm in diameter , a resection margin > 10 mm and a low nuclear grading or a van nuys prognostic index 4 . 
these guidelines point out explicitly that side effects and disadvantages of irradiation are to be weighed against the risk reduction . on a critical note it must be pointed out that the german guidelines rely on retrospective data and not on prospective randomized studies in their choice of the criteria dictating when irradiation can be forgone . 
this does not apply , however , to the tumor size ; here , there are hardly any data on tumors > 2 cm ; the randomized studies did not find any influence of tumor size . 
in addition , at least 70% of the tumors in the randomized studies were uniformly of a size < 2 cunfortunately , the patients age , which displayed a clear influence in almost all other studies , was not taken into account here ; patients < 40 years of age should , on the basis of their high rate of recurrence , always be irradiated . 
patients with an increased risk of recurrences ( e.g. , women < 50 years , tumor - afflicted resection margins , appearance of comedo necroses ) especially strahlenther onkol 2004 no . 
questions still open are : ( cid : 127 ) for which patient group , given prognostically favorable parameters , can treatment be performed without irradiation ? how large must the tumor - free resection margin be ? 1 or 10 mm ? ( cid : 127 ) as currently investigated for invasive breast cancer [ 27 ] , can the treatment volume be confined to the tumor bed in some patients with favorable prognostic factors ? ( cid : 127 ) to which patients should additional tamoxifen be prescribed ? to all patients with estrogen receptor - positive tumors , or only if additional risk factors are present ( e.g. , age < 50 years ; comedo necroses ) ? ( cid : 127 ) should patients with unfavorable risk parameters ( e.g. , tumor - afflicted resection margin ) be given an interstitial or percutaneous boost ? strahlentherapie und onkologie original article radiation therapy for nonmalignant diseases in germany current concepts and future perspectives m . 
heinrich seegenschmiedt1 , 2 , oliver micke2 , norman willich2 , and the german cooperative group on benign diseases ( gcg - bd ) background : radiotherapy ( rt ) of nonmalignant diseases has a long - standing tradition in germany . 
this development is reflected in a national patterns - of - care study ( pcs ) conducted during the years 20012002 . material and methods : in 2001 and 2002 , a questionnaire was mailed to all rt facilities in germany to assess equipment , patient accrual , rt indications , and treatment concepts . 
146 of 180 institutions ( 81% ) returned all requested data : 23 university hospitals ( uni ) , 95 community hospitals ( com ) , and 28 private institutions ( priv )  . 
all data were compared to the first pcs in 19941996 . results : in 137 institutions ( 94% ) 415 megavoltage units ( mean 1.7 ; range 14 ) , and in 78 institutions ( 53% ) 112 orthovoltage units ( mean 1.1 ; range 02 ) were available . 
a mean of 37 , 410 patients were treated per year in all institutions : 503 ( 1.3% ) for inflammatory disorders , 23 , 752 ( 63.5% ) for degenerative , 1 , 252 ( 3.3% ) for hypertrophic , and 11 , 051 ( 29.5% ) for functional , other and unspecified disorders . 
in comparison to the first pcs there was a significant increase of patients per year ( from 20 , 082 to 37 , 410 ; + 86.3% ) in most nonmalignant diseases during the past 78 years . 
most disorders were treated in accordance with the national consensus guidelines : the prescribed dose concepts ( single and total doses ) varied much less during the period 20012002 in comparison with the previous pcs in 19941996 . 
univariate analysis detected significant institutional differences in the use of rt for various disorders . conclusion : rt is increasingly accepted in germany as a reasonable treatment option for many nonmalignant diseases . 
the long - term perspective and research plan will have to include various updates of pcs , rewriting of consensus guidelines , introduction of registries for rare nonmalignant disorders , and clinical controlled studies even for so - called established indications , as international acceptance is based on the criteria of evidence - based medicine . keywords : radiotherapy of nonmalignant diseases patterns - of - care study quality assurance inflammatory / degenerative / hyperproliferative / functional disorders strahlenther onkol 2004 ; 180 : 71830 doi 10.1007 / s00066 - 004 - 9197 - 9 radiotherapie nichtmaligner erkrankungen in deutschland . 
die positive entwicklung sttzt die jngste patterns - of - care - studie ( pcs ) der jahre 20012002 . material und methodik : im jahr 2001 und 2002 wurden anhand eines fragebogens an allen deutschen strahlentherapeutischen institutionen die technische ausstattung , patientenzuweisung , indikationen und rt - konzepte bei nichtmalignen erkrankungen erfasst . 
146 von 180 institutionen ( 81% ) machten vollstndige angaben : 23 universittskliniken ( uni ) , 95 versorgungskrankenhuser ( com ) und 28 private praxen ( priv )  . 
die einzelnen krankheitsgruppen und erkrankungen pro institution und die rt - konzepte wurden nach hufigkeit und verhltnis zwischen den institutionen analysiert und mit der ersten pcs aus den jahren 19941996 verglichen . 
radiation therapy for nonmalignant diseases in germany ergebnisse : in 137 institutionen ( 94% ) standen 415 megavolt - gerte ( mittel 1 , 7 ; spanne 14 ) und in 78 institutionen ( 53% ) 112 orthovolt - gerte ( mittel 1 , 1 ; spanne 02 ) zur verfgung . 
im mittel wurden insgesamt 37 410 patienten pro jahr behandelt : 503 ( 1 , 3% ) wegen entzndlicher , 23 752 ( 63 , 5% ) wegen degenerativer , 1 252 ( 3 , 3% ) wegen hyperproliferativer und 11 051 ( 29 , 5% ) wegen funktioneller , anderer und nicht spezifizierter erkrankungen . 
die meisten erkrankungen wurden gem den nationalen konsensus - leitlinien behandelt : die dosierungskonzepte ( einzelund gesamtdosis ) schwankten im zeitabschnitt 20012002 weit weniger als bei der vorherigen pcs von 19941996 . 
 die langfristige perspektive und forschung auf diesem gebiet mssen neben der aktualisierung von pcs auch die berarbeitung der konsensus - leitlinien , die einfhrung von registern fr seltene erkrankungen und die durchfhrung kontrollierter studien auch bei etablierten indikationen zum ziel haben , da die internationale akzeptanz allein auf den kriterien der evidenzbasierten medizin aufbaut . schlsselwrter : radiotherapie nichtmaligner erkrankungen patterns - of - care - studie qualittssicherung entzndliche / degenerative / hyperproliferative / funktionelle erkrankungen introduction the use of radiotherapy ( rt ) for nonmalignant disorders has a long tradition in germany , but according to an international survey the clinical acceptance varies worldwide [ 14 ] ; a low acceptance rate and level of professional practice have been observed in anglo - american countries [ 21 ] , as old fears for tumor induction are still not resolved  . 
moreover , legal restrictions ( threat of malpractice ) , organizational and institutional reasons ( availability of rt equipment only in cancer centers ) , and competing treatment options prevent a broader acceptance . 
 a first general patterns - of - care study ( pcs ) was conducted during the period of 19941996 to assess the clinical potential of these indications in germany [ 28 ]  . since 1996 the german society for radiation oncology ( degro ) and the german cooperative group on benign diseases ( gcg - bd ) coordinate the scientific , clinical and practical exchange of knowledge and experience in the field of nonmalignant diseases . 
major goals of the group are the development and improvement of quality assurance ( qa ) measures and consensus guidelines for rt of nonmalignant diseases [ 16 ] , the coordination of controlled clinical trials and implementation of rt as accepted therapeutic option in medical specialties such as general medicine , internal medicine , surgery , orthopedics , etc . 
starting out from a first and general pcs in all german rt facilities [ 28 ] , other national pcs have been conducted on specific disease entities such as heterotopic ossification prophylaxis [ 20 , 33 ] , keloids [ 13 ] , graves orbitopathy [ 7 ] , plantar fasciitis [ 19 ] , and desmoids or aggressive fibromatosis [ 17 ]  . 
other specific national pcs and registries for rare nonmalignant disorders are planned ( table 1 )  . nevertheless , progress and changes are best assessed , if the first general pcs between 19941996 [ 16 ] is compared with an update of the quality of rt equipment , range of clinical indications , number of patients treated per institution , and specific rt prescriptions for each nonmalignant disease in various german rt institutions . 
a perspective is provided on further steps and initiatives to advance the field in the near future . material and methods a questionnaire ( see appendix ) was mailed to all german rt departments in 2001 and 2002 in order to identify their specific institutional experience with rt for nonmalignant diseases . 
 similar to our first published questionnaire and a european questionnaire [ 14 ] single disease entities and four traditional disease categories were assessed : inflammatory , degenerative , hyperproliferative , and functional disorders . 
data from institutions , which did only provide the numbers for the single disease categories , but not for the specific diseases themselves , were grouped as not specified within the respective diseases . 
for clarification additional statements were requested for each disease entity or category leaving some results without comparison to the former pcs . the mean annual values for each disease were calculated from the consecutive numbers of patients provided by the different institutions between the years 20012002 . 
 year nonmalignant disease status publications [ strahlentherapie und onkologie review article management of anemia in patients undergoing curative radiotherapy erythropoietin , transfusions , or better nothing ? jrgen dunst1 abstract background and results : anemia is a well - known risk factor for decreased local control and survival in patients undergoing curative radiotherapy . 
there is clear evidence from recent clinical investigations that anemia is an independent risk factor and hemoglobin ( hb ) levels during radiotherapy are important ( and not pretreatment hb levels )  . 
an optimal hb range with regard to tumor oxygenation seems to exist , and hb levels < 11 g / dl and > ~15 g / dl impair tumor oxygenation but have ( over a broader range ) no significant impact on normal tissue oxygenation . 
 there is some evidence from retrospective and prospective studies that the response to radiotherapy and the prognosis , especially in cervical cancers , might be improved if the hb levels during radiotherapy can be maintained in the optimal range , either by transfusions or by erythropoietthe effect of any antianemic therapy should be analyzed according to whether or not treatment was successful with regard to achieving optimal hb levels during irrradiation . 
 conclusions : treatment of anemia with the objective of improving local control and survival in radiotherapy patients is probably more difficult and sophisticated than coping with symptoms of anemia or improving quality of life . 
 key words : radiotherapy anemia prognosis erythropoietin transfusions strahlenther onkol 2004 ; 180 : 67181 doi 10.1007 / s00066 - 004 - 9191 - 2 behandlung der anmie unter kurativer strahlentherapie : erythropoietin , transfusionen oder besser nichts ? zusammenfassung hintergrund und ergebnisse : eine anmie ist ein risikofaktor bei patienten , die mit kurativer intention bestrahlt werden . 
zahlreiche klinische untersuchungen der letzten jahre haben gezeigt , dass die anmie ein unabhngiger risikofaktor ist und dass vor allem niedrige hmoglobin - ( hb - ) werte whrend einer mehrwchigen strahlentherapie von bedeutung sind . 
es scheint ein optimaler hb - bereich fr die tumoroxygenierung zu bestehen , denn hb - werte < 11 g / dl und > ~ 15 g / dl verschlechtern die tumoroxygenierung , haben aber keinen einfluss auf die oxygenierung des normalgewebes . 
 zahlreiche retrospektive und prospektive studien deuten darauf hin , dass sich die prognose vor allem bei patientinnen mit zervixkarzinomen verbessern lsst , wenn die hb - werte whrend der strahlentherapie im optimalen bereich gehalten werden . 
erythropoetin scheint gegenber transfusionen sicherer zu wirken , wenn ein stabiler anstieg der hb - werte erreicht werden soll ; andererseits birgt erythropoetin das risiko einer berkorrektur des hb - werts . 
 schlussfolgerungen : die behandlung der anmie bei tumorpatienten mit dem ziel , das ansprechen auf eine strahlentherapie und die prognose zu verbessern , ist wahrscheinlich komplizierter als die symptomatische behandlung der anmie oder die verbesserung der lebensqualitt . 
 the objective of this article is to summarize the experimental and clinical data with regard to the question whether or not the radiation oncologist should carefully look at and treat or prevent anemia during radiotherapy . 
 clinical aspects of anemia in patients with cancer frequency of anemia the frequency of anemia varies among cancer patients and is mainly dependent on site and extent of disease and type of treatment . 
anemia is more frequent in patients with systemic diseases and bone marrow infiltration ( e.g. , leukemias , plasmocytomas , lymphomas ) and in solid cancers of advanced stages [ 11 , 35 , 46 ]  . 
 according to own data , about 60% of patients treated with curative intent for head and neck , cervical , esophageal or rectal cancer have hemoglobin ( hb ) levels in the normal range ( > 13 g / dl )  . 
moderate to severe anemia ( hb between 9 and 11 g / dl ) has been noticed in about 1520% of patients with head and neck and cervical cancers but was not observed in a smaller group of patients with esophageal and rectal cancers . 
severe , transfusion - requiring anemia ( hb < 9 g / dl ) was noted only in a minority of patients , < 1% of all patients and 4% of patients with cervical cancers [ 20 ]  . 
in the first publication that has highlighted the impact of hb levels on treatment outcome , evans and bergsj analyzed 880 patients with stage iiv cancer of the cervix [ 23 ]  . 
anemia ( hb < 11 g / dl ) increased with stage ( 13% in stage i , 21% in stage ii , 34% in stage iii , 73% in stage iv , and 20% in patients treated postoperatively )  . 
42 patients ( 10% ) received transfusions prior to ( 6% also during ) treatment and additional 56 patients ( 15% ) were transfused during treatment [ 28 ]  . 
prior to treatment , anemia ( hb < 12 g / dl ) was present in 41% of all patients , and this percentage increased up to 54% during treatment . 
it is not likely that these differences result only from tumor bleeding , because clinically relevant bleeding is rarely observed in most head and neck cancers and a prognostic impact of anemia has been demonstrated in early glottic cancers which do not bleed [ 10 ]  . 
 laboratory findings and pathophysiology anemia in cancer patients may result from the malignant disease itself , or can be caused by specific tumor therapies such as chemotherapy , radiotherapy or surgery or may result from independent concomitant diseases . 
 anemia caused by tumor tumor - related anemia ( cytokine - mediated anemia comparable to anemia in chronic inflammatory diseases ) acute blood loss due to tumor bleeding chronic blood loss due to subclinical bleeding bone marrow infiltration anemia caused by cancer therapy hematologic toxicity of chemotherapy and / or radiotherapy blood loss during surgery patient - related causes of anemia concomitant medical illness ( e.g. , renal failure , esophageal varicosis , rheumatoid arthritis ) concomitant medication ( e.g. , nsars ) hereditary anemias strahlenther onkol 2004 no . 
a further characteristic finding are the relatively low serum levels of erythropoietin ( epo ) which are , with regard to the hb levels , lower than in anemic patients with blood loss [ 54 ]  . 
this finding suggests that insufficient endogeneous epo production is a major causative factor for anemia in patients with solid cancers [ 58 ]  . the serum concentrations of a variety of cytokines such as interleukin - 6 ( il - 6 ) or vascular endothelial growth factor ( vegf ) are increased in patients with solid cancers and anemia [ 18 ]  . 
with regard to the mentioned laboratory findings , anemia in patients with solid cancers resembles the anemia of chronic inflammatory disease ( acd , e.g. , in rheumatoid arthritis or crohns disease )  . prognostic impact of anemia pretreatment anemia as compared to patients with normal hb levels , patients with anemia at diagnosis have a worse prognosis , especially patients treated with radiotherapy in curative intent . 
the first and most comprehensive report on this topic by evans & bergsj has already demonstrated that there is a more or less linear relationship between decrease in hb and decrease in overall survival below a certain hb threshold [ 23 ]  . 
various other large analyses [ 10 , 24 , 25 , 28 , 34 , 39 , 42 , 49 , 53 , 59 , 6163 , 67 , 69 , 83 ] and three recent systematic reviews [ 11 , 27 , 41 ] have supported these findings . decreased hb levels are important for prognosis in malignancies with frequent and intensive bone marrow involvement such as leukemias and plasmocytomas ; in these malignancies , anemia reflects tumor burden and the extent of marrow infiltration . 
 hasenclever & diehl have proposed a prognostic model for localized ( stage iiii ) hodgkins disease in which a decreased hb ( < 10.5 g / dl ) is a major clinical factor besides elevated erythrocyte sedimentation rate ( esr ) and tumor bulk [ 36 ]  . 
in inoperable bladder cancer treated with radiotherapy , a combination of anemia , increased esr and age can better predict prognosis than clinical t - category [ 34 ]  . 
our own results in cervical cancer also support these findings [ 19 ]  . it should be noted that the poor prognosis in anemic patients if treated with radiotherapy mainly results from poor local control [ 32 ]  . 
anemia is strongly correlated with local failure rate and has no or only a small impact on distant metastases [ 19 ]  . anemia during radiotherapy most of the investigations in the literature that have analyzed the impact of anemia on treatment outcome have concentrated on pretreatment hb levels , probably because this information is routinely obtained during pretreatment staging procedures and can be easily extracted from the patients records even in retrospective investigations . 
however , all studies that looked at hb levels prior to and during radiotherapy have demonstrated that hb levels during radiotherapy are more important than pretreatment hb levels [ 19 , 33 , 56 , 75 , 79 ]  . an impact of nadir hb levels during radiation therapy for local control and survival in cervical cancers was observed by logsdon & eifel as well [ 52 ]  . 
another recent investigation has also found a significant impact of hb at the end of radiotherapy but not pretreatment hb on the response of locally advanced head and neck cancers . 
the radiochemotherapy regimen produced profound anemia in a high proportion of patients at the end of treatment , and the hb levels at the end of therapy were a significant prognostic factor for local control and survival , together with tumor size and histological response to radiochemotherapy . the current data , therefore , suggest that hb levels during a course of fractionated radiotherapy or even at the end of treatment may be more crucial than pretreatment hb levels . 
 according to these findings , the prognostic impact of pretreatment hb levels probably results from the strong correlation between hb levels prior to therapy and at the end of radiotherapy [ 19 , 33 ]  . 
these data are the theoretical basis for preventing and / or correcting anemia during radiotherapy . explanations for the prognostic impact association between anemia and tumor hypoxia the most attractive explanation for the impact of anemia is the association between anemia and tumor hypoxia . 
investigated 133 patients with head and neck squamous cell cancers , and an hb level < 11 g / dl was significantly associated with poor tumor oxygenation but had no impact on normal tissue oxygenation [ 4 ]  . 
from a pathophysiological point of view , it is not astonishing that tumor oxygenation is more sensitive to changes in hb than normal tissue oxygenation for two main reasons [ 55 ]  . 
there is indeed no association between hb and tumor oxygenation in patients with hb levels in the normal range , and tumor hypoxia may be present in about 3050% of tumors in nonanemic patients . 
 as anemia is a major cause of tumor hypoxia , it is reasonable to assume that treating or preventing anemia during radiotherapy may , via avoidance of tumor hypoxia , improve radiation response . 
 impaired immune function the association between anemia and tumor oxygenation cannot sufficiently explain the prognostic impact of anemia in patients with systemic malignancies or patients undergoing chemotherapy with oxygen - independent drugs . 
 therefore , anemia might be a symptom of an aggressive tumor or a symptom of a systemic disease which by itself is characterized by an impaired immune function with subsequent increased risk of tumor progression and distant metastases [ 26 , 42 ]  . 
15 out of 87 patients with stage iib to iva squamous cell cancers presented with moderate to severe anemia ( hb < 11 g / dl ) prior to radiotherapy . 
all were treated with definitive radiotherapy ( external - beam radiation plus high - dose - rate [ hdr ] brachytherapy ) in the period from 1995 through 1999 ; concurrent chemotherapy was not used in the treatment period . 
 five out of 18 primarily anemic patients had an increase in hb levels during radiotherapy ; we assume that the improvement of anemia in this subgroup was a consequence of the effective radiation treatment . 
we therefore assume that anemia in these patients behaves like an independent disease and would have required a specific antianemic therapy besides tumor treatment . anemia and quality of life the impact of anemia on quality of life is clearly established . 
 a huge number of studies have demonstrated a strong correlation between hb levels on the one hand and overall quality of life and especially some items of quality of life on the other hand . 
the data have led to evidence - based recommendations on the use of epo in oncology patients [ 64 ]  . treatment of anemia historical development of treatment guidelines prior to the 1980s , anemia with hb levels < ~10 g / dl was considered an indication for blood transfusions . 
the indications for blood transfusions , mainly perioperative blood transfusions , however , were restricted later in the 1980s due to possible risks of transfusions in the hiv era and due to a relative deficiency of donated blood . 
in the 1990s , the availability of recombinant human erythropoietin ( rhepo ) offered the chance to treat anemic patients without transfusion risks , and epo was introduced in nephrology and later in oncology . 
 theoretical considerations the key issue for radiation oncology concerns the question whether or not an optimal hb range exists and whether keeping the hb during radiation treatment within this range improves survival . 
with regard to the mentioned association between hb levels and tumor oxygenation , we propose the hypothesis that there is indeed an optimal hb range which is , however , smaller than expected from earlier investigations [ 81 ]  . 
critical hb values which may impair tumor oxygenation have been found to be values < 11 g / dl on the one hand and high values > ~15 g / dl on the other hand . 
from a theoretical point of view , the design of any interventional study with the objective of treating or preventing anemia should aim at trying to keep the hb during radiotherapy in this optimal range . experimental data in animal models the positive impact of correcting low hb levels on tumor oxygenation is well proven in animal models . 
 clearly demonstrated that induction of anemia led to impaired tumor oxygenation in tumor - bearing mice with a reduced median po2 and increased hypoxic fraction with po2 values < 5 mm hg [ 45 ]  . 
 there are no systematic studies on the impact of transfusions or epo on tumor oxygenation in human tumors in vivo due to ethical problems associated with repeated invasive po2 measurements . 
some casuistic observations with transfusions suggest that tumor oxygenation may be partly improved [ 20 , 73 ]  . clinical results with transfusions the question whether transfusions might improve or impair survival has been debated over long periods ( for review see [ 14 ] )  . 
some retrospective studies have reported decreased survival figures in patients with gastrointestinal cancers receiving transfusions during surgery ; the interpretation of these data is difficult , because the prognostic difference might result from the underlying anemia , specific therapy - related factors ( blood loss during surgery , indicating locally advanced or not curatively resectable disease ) or the transfusion itself ( e.g. , by immunosuppressive effects of donated blood )  . 
there is , on the other hand , evidence that the donation of allo genic blood may ( probably transiently ) alter immune function parameters [ 6 , 68 ]  . 
although it was the strategy to transfuse anemic patients with the objective of keeping the hb > 11 g / dl , only 19% of 54 transfused patients achieved this desired hb range ; the prognosis of this successfully transfused subgroup with regard to pelvic control and survival was identical to primarily nonanemic , nontransfused patients . 
tumor - related anemia was significantly associated with stage , tumor size and lymph node involvement , and this association was stronger in patients who did not sufficiently respond to transfusions . 
in a subgroup of anemic patients whose anemia was not tumor - related but resulted from other medical reasons ( e.g. , renal insufficiency or esophageal varicosis ) , anemia and success of transfusions were not related to outcome , and none of these anemic patients failed with regard to cervical cancer . 
second , however , it is difficult to maintain hb levels within the desired range with transfusions , because only 19% of patients were successfully transfused despite a well - defined transfusion strategy . 
epo : erythropoet experimental question and design results in normemic / anemic animals ; impact of epo or transfusions on tumor oxygenation epo in anemic , tumor - bearing animals , single - dose irradiation with 10 gy , growth delay effect of epo in anemic , tumor bearing animals , treatment with cyclophosphamide , growth delay partial restoration of tumor oxygenation after correction of anemia decreased growth delay in anemic animals , nearly full restoration of normal radiosensitivity after treatment with epo decreased growth delay in anemic animals , full restoration of sensitivity to cyclophosphamide after treatment with epo kelleher et al . 
2003 [ 72 ] effect of epo in anemic nude mice , decreased radiosensitivity in anemic animals , restoration of treatment of xenografted tumors with fractionated irradiation , impact radiosensitivity after treatment on growth delay and local control treatment of xenografted glio blastomas with fractionated irra diation , impact on growth delay and local control anemic animals , restoration of radiosensitivity after treatment with epo with epo strahlenther onkol 2004 no . 
11 urban & vogel transfused if the hb dropped < 12 g / dl ; however , transfusions were administered in case of an hb < 10 g / dl . 
this study , from a todays point of view , was not well planned and has therefore been criticized because of its design and the resulting imbalance between the treatment groups [ 26 ]  . 
 phase iii randomized study 132 patients with stage ii / iii cervical cancer , definitive radio therapy with external - beam irradiation lowest failure rate ( 6 / 38 ) in plus brachytherapy subgroup in experimental arm endpoint local control control arm : transfusions , if hb drops < 10 g / dl experimental arm : transfusions , if hb drops < 12.5 g / dl bush 1986 [ 9 ] grogan et al . 
in the nontransfusion group , patients were not clinical results with erythropoietin epo is a cytokine which increases erythropoiesis via prevention of apoptosis of erythrogenic precursor cells [ 31 , 47 ]  . 
 epo has primarily been used in patients with renal anemia , but its use was extended to oncology patients in the mid 1990s . the impact of epo on quality of life has clearly been demonstrated in a variety of large prospective and randomized trials ( table 4 )  . 
impact of recombinant human erythropoietin ( rhepo ) on transfusion requirements and quality of life ( qol ) in prospective randomized studies of patients receiving myelosuppressive chemotherapy for hematologic or nonhematologic malignancies . 
2002 [ 60 ] myeloma , lymphoma 262 343 solid tumors myelosuppressive nonplatinum 5 - fu - based chemotherapy myelosuppressive chemotherapy myelosuppressive chemotherapy increase in hb , reduced need for transfusions qol benefit for patients with hb increase increase in hb , reduced need for transfusions qol benefit for patients with hb increase increase in hb , reduced need for transfusions qol benefit for patients with hb increase strahlenther onkol 2004 no . 
it is worth mentioning that the hb levels at the beginning of treatment were in the range of about 910 g / dl in the majority of patients and that most of the patients were treated with myelosuppressive chemotherapy . 
 hb response transfusion requirements solid cancers hematologic malignancies tumor response mortality a recent cochrane review has analyzed all randomized controlled studies in which epo was used as experimental therapy against a null arm or placebo [ 7 ]  . 
studies that had been published until 2001 were incorporated in the meta - analysis , and a total number of 27 randomized controlled trials with a total number of 3 , 284 patients were analyzed . 
there was a significant impact of epo on hb levels and transfusion requirements , no effect on tumor response , and a trend toward reduced mortality in the epo group ( table 5 )  . 
transfusions lead to a rapid increase in hb , but most patients have slowly decreasing hb levels within the next weeks and there is some evidence that in daily clinical practice only a minority of transfusion - requiring patients can be successfully transfused with keeping the hb above a certain threshold [ 43 ]  . 
by contrast , epo yields a significant hb response in the majority of patients treated with radiotherapy patients ( n ) trials ( n ) relative risk ( 95% ci ) epo vs . 
one retrospective analysis and two further randomized ( but not yet fully published ) studies suggest a benefit in terms of local control [ 2 , 5 , 29 ]  . 
one study ( enhance study ) used epo as radiosensitizer in head and neck cancer patients treated with definitive or postoperative radiotherapy , the other ( int - 076 or best study ) used epo in patients treated with palliative chemotherapy for metastatic breast cancer [ 38 , 50 ]  . 
both studies demonstrated a transient ( best study ) or long - lasting ( enhance study ) increase in mortality in patients in the epo arwhen interpreting the data , there table 6 . 
hb : hmoglob authors rhepo dose iron supplementation mean hb at start mean hb at end of study ( g / dl ) of study ( g / dl ) average hb increment per % target hb per week ( g / dl ) reached target hb ( g / dl ) lavey & dempsey 1993 [ 48 ] dusenbery et al . 
2003 [ 38 ] 0.51.0 g / dl per month baseline hb 910 g / dl in most studies standard doses about 3 weekly 150 iu / kg epo , iron supplementation in some studies meta - analysis of 27 randomized trials epo as supportive drug in anemic patients receiving chemotherapy hb < 1112 g / dl placebo - controlled phase iii baseline hb 11.7 g / dl trial in patients treated with 3 weekly 300 iu / kg epo whole study period , 3.2 g / dl in 1st month curative xrt for head and neck cancer epo as radiosensitizer endpoint locoregional tumor progression hb < 1213 g / dl + i.v. 
iron reduced need for transfusions no impact on tumor response trend toward reduced mortality in patients with epo small increase in hb in placebo group increased rate of tumor progression in epo group as compared to placebo 1.8 g / dl per month over rapid increase in hb in epo group are some obvious differences between the studies in the cochrane review and the enhance and best studies which might explain the discrepancies in clinical results ( table 7 )  . 
 in the enhance and best studies , the inclusion criteria with regard to baseline hb levels were much broader than in other studies ; therefore , the average hb at start of therapy was nearly normal and only slightly reduced . 
in the enhance study , a high dose of epo ( three times weekly 300 iu / kg body weight , the double dose as compared to standard dosing regimens ) was used with the objective of surely and rapidly increasing hb levels during radiotherapy . 
if one assumes that there is an optimal hb range for tumor oxygenation , the placebo group had a radiobiologically favorable course of hb during radiotherapy , whereas the hb in the epo group might have been overcorrected ( figure 1 )  . 
these receptors probably have a physiological function and seem to play a role in protecting some tissues ( e.g. , glial cells ) from hypoxia - induced apoptosis [ 11 , 12 ]  . 
in most of these cell lines , they have no functional role because there is no effective downstream signaling , although increased proliferation of tumor cells by epo has been described [ 66 , 70 , 84 ]  . 
neuroectodermal tumor cells have been shown to upregulate the epo receptor and the secretion of epo under hypoxia , and it is assumed that cells thereby try to escape hypoxia - induced cell death figure 1 . 
the hb increased slightly in the placebo group ( from 11.8 g / dl at baseline to 12.9 g / dl at the end of radiotherapy ) and extremely in the epo group ( from 11.7 g / dl at baseline to 15.4 g / dl at the end of radiotherapy )  . 
under the assumption , that the optimal hb range with regard to tumor oxygenation and prevention of tumor hypoxia is between 11 and 15 g / dl , the placebo group had the radiobiologically better hb course . 
unter der annahme , dass der optimale hb - bereich fr die tumoroxygenierung zwischen 11 und 15 g / dl liegt , war der hb - verlauf whrend der radiotherapie in der plazebogruppe strahlenbiologisch gnstiger . 
in animal models , the use of epo alone ( in the control arms of studies ) has not promoted tumor growth [ 71 , 72 , 76 , 77 ]  . 
in clinical studies in humans , the meta - analysis has not found any evidence for enhanced tumor progression or decreased response to chemotherapy by the use of epo [ 7 ]  . 
 only two studies ( enhance and best studies ) have found an increase in tumor progression in the epo arm , but the results of these studies , as mentioned , can also be explained by other factors . in summary , there is currently no evidence that epo , in a clinical setting , increases the risk of tumor progression if used according to standard guidelines . 
the role of epo receptors is unclear and should be further investigated in translational research programs . possible risks of transfusions mainly depend on the type of donated blood ( for review see [ 14 ] )  . 
the risk of transmitting infectious agents ( mainly hepatitis virus , hiv ) has been reduced in the past 2 decades and is in the range of < 1 case per 1.5 million units of blood and about 1 / 220 , 000 units for hepatitis b . 
there is a small , but significant risk of thromboembolic events ; the absolute difference between patients treated with epo versus control patients is about 2% according to data from meta - analyses . 
so far , rca has only been observed in patients treated with epo for renal failures , and no cases have been described in cancer patients ( who receive the drug in higher doses , but only over relatively short periods as compared to renal failure patients )  . 2 a red blood unit contains red blood cells , buffy coat ( white blood cells and platelets ) and plasma . 
when interpreting the data , it should be noted that any antianemic therapy ( in contrast to anticancer therapies like radioor chemotherapy ) will not directly impinge on cancer control , but indirectly via its effect on hb levels . 
therefore , the effect of transfusions or epo is dependent on whether or not the hb levels of treated patients can be successfully kept within a certain ( optimal ) hb range . 
therefore , preventing and correcting anemia ( with the objective of keeping the hb level between 1115 g / dl during radiotherapy ) is an attractive treatment option to improve radiation response and survival . on the basis of the mentioned clinical and experimental data , the major conclusions for the radiation oncologist are : ( cid : 127 ) the association between anemia and outcome is clearly evi ( cid : 127 ) anemia during radiation therapy ( and not prior to therapy ) is a major risk factor for local failure and , as a consequence , decreased survival . 
the association between anemia and treatment response is clearly evident in patients undergoing radiotherapy . ( cid : 127 ) the critical threshold below which low hb levels have a significant impact on local control and prognosis in radiotherapy patients is probably about 11 g / dl . ( cid : 127 ) keeping the hb level above this threshold seems to be associated with better local control and survival . ( cid : 127 ) the most likely explanation for the association between anemia and decreased radiation response is anemia - induced tumor hypoxia . 
low ( < 11 g / dl ) and high ( > 15 g / dl ) hb levels can impair tumor oxygenation . ( cid : 127 ) in animal models , anemia decreases radiosensitivity , but response to single - dose and fractionated irradiation can be restored by correcting hb levels with epo . ( cid : 127 ) a possible impact of preventing or correcting anemia on survival is not yet clearly established . 
however , the subgroup of patients who will benefit most from antianemic therapies in terms of survival are probably patients who are undergoing radiotherapy with curative intent in cancer sites where the impact of anemia is well proven ( e.g. , cervix , head and neck , lung , bladder cancers )  . ( cid : 127 ) whenever correcting anemia by specific therapies , hb levels should be kept within the optimal range . further clinical studies with optimized antianemic treatment strategies are required . 
anemia in radiotherapy patients strahlentherapie und onkologie review article treatment of oral cavity and oropharyngeal cancer indications , technical aspects , and results of interstitial brachytherapy vratislav strnad1 abstract excellent local control rates of interstitial brachytherapy in oral cavity cancer and oropharyngeal carcinoma have been demonstrated in different retrospective studies . 
compared to external - beam radiation therapy the high local control rates with a low rate of side effects obtained by interstitial brachytherapy are the result of a steep dose reduction in the implant - surrounding normal tissues . 
low - dose - rate ( ldr ) and pulsed - dose - rate ( pdr ) interstitial brachytherapy with 0.40.55 gy / h / 24 h for tumors of the oral cavity and oropharynx in selected patients is a proven , effective and safe treatment method with excellent long - term data both as a sole treatment modality and a postoperative method , as well as a unique treatment method of head and neck tumors in previously irradiated areas . 
this paper deals with the technical aspects of interstitial brachytherapy , that seem to be relevant to high - quality outcome , and gives an overview of indications as well as past and recent results of interstitial brachytherapy in head and neck cancer . key words : head and neck cancer brachytherapy strahlenther onkol 2004 ; 180 : 7107 doi 10.1007 / s00066 - 004 - 9196 - x therapie von mundhhlenund oropharynxkarzinomen . 
indikationen , technische aspekte und ergebnisse der interstitiellen brachytherapie zusammenfassung in einer ganzen reihe von retrospektiven studien wurden ausgezeichnete lokale kontrollraten der interstitiellen brachytherapie bei karzinomen der mundhhle und des oropharynx demonstriert . 
die interstitielle low - dose - rate - ( ldr - ) und pulsed - dose - rate ( pdr - ) brachytherapie mit 0 , 40 , 55 gy / h / 24 h bei ausgewhlten patienten mit mundhhlenund oropharynxkarzinomen ist eine bewhrte , effektive und sichere methode mit ausgezeichneten langzeitergebnissen , sowohl als alleinige behandlungsmethode als auch als postoperative therapie und ebenfalls als eine einzigartige behandlungsmethode von vorbestrahlten hals - nasenohren - ( hno - ) tumoren . 
brachytherapy of oral cavity and oropharyngeal cancer introduction the standard treatment approach to squamous cell carcinomas of the oral cavity and oropharynx depends on tumor size and location , and consists in different types of radical surgery followed by external - beam radiation therapy with or without brachytherapy yielding different survival rates . 
surgical tumor resection , mostly together with lymph node neck dissection , often involves partial or total glossectomy or amputation of the soft palate and therefore frequently leads to swallowing incompetence and other serious effects following mutilating surgery . 
as a consequence of high radiation doses to salivary glands , the entire oropharynx and / or oral cavity and mandibular joints , external - beam radiation therapy causes quite a number of late effects , such as xerostomia , severe mucositis , mucosa atrophy , severe radiodermatitis , and trismus [ 1 , 6 , 7 , 1113 , 15 , 2123 , 31 , 33 , 43 , 61 , 62 , 64 , 79 , 8083 , 92 , 95 , 98 , 99 ]  . 
 by contrast , brachytherapy is able to deliver high doses to small volumes confined to the tumor / tumor bed , while surrounding tissues including salivary glands , mandibular joint , mucosa , and the overlying skin can be spared maximally . 
poor - quality brachytherapy will lead to an unacceptable outcome in terms of local control and serious side effects as well [ 72 , 90 ]  . this paper provides an overview of the current role of interstitial brachytherapy in oral cavity and oropharyngeal cancer . 
we will critically evaluate the indications for interstitial brachytherapy , localization procedures of planning target volume ( ptv ) , describe implant techniques , and analyze treatment results . indications for brachytherapy interstitial brachytherapy alone of the primary tumor site the main indications for brachytherapy alone in cancer of the oral cavity are tumors < 3040 mm in diameter without bone infiltration . 
to omit neck lymph node dissection as well , external - beam therapy of neck lymph nodes is possible in exceptional cases only . boost brachytherapy of the primary tumor site after external radiotherapy another indication for interstitial brachytherapy is a boost irradiation of the primary tumor site after external - beam radiation therapy in tumors not amenable to primary surgery . 
this approach is feasible in tumors 3040 mm in diameter at the time of implantation . if the tumor was treated with primary surgery and subsequent external - beam therapy , brachytherapy should be used as boost especially in the following cases : initial tumor size > 2030 mm , positive lymph nodes , and particularly resection margins that are unclear or < 5 mm , vessel invasion , or a histologically poor grading . postoperative interstitial brachytherapy alone postoperative interstitial irradiation alone of the primary tumor site is indicated particularly in case of a high risk of local recurrence ( e.g. , in instances of positive resection margins ) or if at least one of following risk factors is present : tumor infiltration depth > 5 mm , l1 , v1 or g3 grading . 
brachytherapy is feasible , if gingiva infiltration proves < 1 cm in width . technical aspects of brachytherapy clinical work - up clinical examination , with measurement and documentation of the localization of the tumor mass by ct or mr images , if meaningful , is important to document local tumor extension . 
the head and neck surgeon and radiation oncologist jointly make the decision on the appropriate modalities of head and neck cancer treatment . definition of the clinical target volume the ptv for interstitial brachytherapy is defined by a 5to 10 - mm margin of normal tissue surrounding the primary tumor or tumor bed . 
adjacent bone tissue , e.g. , the mandible , is never to be included in the clinical target volume ( ctv ) for brachytherapy . localization of the planning target volume in contrast to external - beam irradiation using ct and / or mr images as basis for treatment planning and delivery , ct and mri methods are sometimes of limited value in interstitial brachytherapy for head and neck cancer . 
first of all , deformation of varying degrees of tongue , soft palate , and floor of mouth during the implant procedure results in a completely different situation as seen on ct or mri before implantation . 
moreover , in case of small primaries or in the postoperative situation ( no macroscopic tumor ) neither ct nor mri allows to delineate the tumor / tumor bed surface with sufficient safety . 
implantation in local anesthesia and premedication with 2.510 mg midazolam ( dormicum ) given 1530 min before implantation is possible in some situations , but we do not recommend it . implantation techniques , design of the implant geometry the number of and spacing between needles is chosen to adequately cover the width and thickness of the ptv . 
 in principle , we use two different techniques , one for the implantation of tongue and floor of mouth , and the second for implantation of faucial arch or soft palate . for implantation of the tongue or floor of mouth under bimanual palpation of the tumor or tumor bed , hollow thin - walled stainless - steel needles are inserted below the chin and advanced into the tumor bed and surrounding tissue ( target volume )  . 
 similar results ( see table 1 ) were reported from other centers [ 17 , 32 , 34 , 35 , 36 , 39 , 75 ]  . using ldr brachytherapy after tumor resection as postoperative treatment modality , we found a slightly different situation . 
 for postoperative treatment , brachytherapy as boost ( pt1 / 2 pn + patients ) and , in particular , postoperative brachytherapy alone ( pt1 / 2 pn0 patients ) offer the patients the same 5 - year strnad v . 
in this way , the length and width of the target volume are well encompassed by peripheral catheters , the depth being presumed to extend from the dorsum of the tongue distally up to 0.51 cm from the maximal tumor depth stated in pathologic review or ct / mr imaging . 
 in principle , the posterior tube should be implanted first , and it is useful to mark the entry points for the guide needles on the skin surface by palpating the hyoid bone and carotid artery . 
typical insertion points are near the hyoid bone and in one line with the palatoglossal and palatopharyngeal arch ( for more technical details see also [ 72 , 90 ] )  . 
 prescription of dose , dose rate , fractionation both low - dose - rate ( ldr ) and pulsed - dose - rate ( pdr ) brachytherapy are feasible in interstitial brachytherapy for oral cavity and oropharyngeal cancer . 
dose prescription rules of icru 58 report and principles of the paris system should be respected [ 72 , 90 ]  . we recommend to perform curatively intended interstitial brachytherapy of oral cavity and oropharyngeal cancer strictly as ldr or pdr brachytherapy . 
if the center is only equipped with an hdr machine , interstitial brachytherapy should be done outside of controlled studies as fractionated brachytherapy only with a fraction dose 3 gy . results of brachytherapy local control rates trial results show a large similarity between oral tongue and floor of mouth cancers and important differences for oropharynx carcinomas ( see table 1 )  . 
first of all , it is important to distinguish between primary brachytherapy alone and brachytherapy as boost after external - beam therapy and postoperative brachytherapy as well as brachytherapy for local recurrences , particularly in previously irradiated areas . for cancers of the oral tongue treated with primary ldr brachytherapy , large retrospective series show ( table 1 ) , that time ( months ) figure 1 . 
5 - year local recurrence - free survival ( 78% ) after pulsed - dose rate brachytherapy in all patients with oral cavity carcinoma and oropharyngeal cancer ( n = 234 ) treated in our department between 1997 and 2003 . 
fnf jahre rezidivfreies berleben ( 78% ) nach einer brachytherapie mit gepulster dosisleistung bei patienten mit mundhhlenund oropharynxkarzinomen ( n = 234 ) , die in unserer klinik zwischen 1997 und 2003 behandelt wurden . 
brachytherapy of oral cavity and oropharyngeal cancer 36 48 36 48 time ( months ) time ( months ) figure 2a abbildung 2a figure 2b abbildung 2b figures 2a and 2b . 
4 - year local recurrence - free survival after pulsed - dose - rate brachytherapy in patients with oral cavity carcinoma and oropharyngeal cancer in previously irradiated areas ( n = 43 ) treated in our department between 1997 and 2001 . 
vier jahre rezidivfreies berleben nach einer brachytherapie mit gepulster dosisleistung in der vorbestrahlten region bei mundhhlenund oropharynxkarzinom - patienten ( n = 43 ) , die in unserer klinik zwischen 1997 und 2001 behandelt wurden . 
 brachytherapy avoids xerostomia , excessive mucositis in the whole oral cavity , and trismus and also permits future radiation therapy of secondary tumors in the head and neck area in spared nonirradiated tissues without any problems . 
also , the analysis of our data by 234 patients showed that , using pdr brachytherapy , the 5 - year local control rates after minimal , nonmutilating surgery varied between the same values as with ldr brachytherapy , with minimal side effects ( figure 1 , table 1 )  . 
until now , hdr brachytherapy as sole treatment modality or as postoperative treatment for head and neck carcinomas can only be used with caution and should be performed in controlled trials . 
the standard strategy of surgical salvage for failed radiation therapy as radical tumor resection with clear resection margins is difficult to accomplish , a repeated external - beam therapy is afflicted with a higher risk of severe side effects . 
to perform a salvage therapy for patients with secondary or recurrent tumors in previously irradiated areas , it is necessary to apply high doses ( 60 gy ) using brachytherapy techniques . 
in our analysis [ 89 ] , we achieved a permanent local control in 79% of patients ( 34 / 43 ) and a 4 - year local recurrence - free survival of 68% in all patients and 80% in patients treated with curative intent ( figure 2 )  . 
if simultaneous hyperthermia or concomitant chemotherapy can improve the results of brachytherapy still remains unclear [ 24 , 27 , 30 , 84 , 89 , 93 ]  . side effects after brachytherapy , nearly all of our patients show a mucositis grade 23 in the implanted area . 
in 234 patients with oral cavity cancer or oropharyngeal carcinoma treated between 1997 and december 2003 in our department in erlangen , using pdr brachytherapy , we have observed a soft - tissue necrosis rate of only 6.6% and an osteoradionecrosis rate of 5.5%. 
our results [ 89 ] regarding the rate of side effects ( soft - tissue necrosis 4.6% and , in particular , osteoradionecrosis 0% ) are quite comparable with those of peiffert et al . 
in our opinion , the low complication rates in our patients are due to the pdr brachytherapy , a method , which unites the biological advantages of ldr brachytherapy with the technological advantages of hdr afterloading . 
 conclusion ldr and pdr interstitial brachytherapy with 0.40.55 gy / h / 24 h for tumors of the oral cavity and the oropharynx in selected patients is a proven , effective and safe treatment method with excellent long - term data both as a sole treatment modality and a postoperative method , as well as a unique treat ment method of head and neck tumors in previously irradiated areas . strahlentherapie und onkologie review article current status of radiation therapy and combined modality treatment for bladder cancer claus rdel1 background : standard treatment for muscle - invasive bladder cancer is radical cystectomy . 
combined - modality treatment ( cmt ) , including transurethral resection ( turbt ) , radiation therapy ( rt ) and systemic chemotherapy , has been shown to produce survival rates comparable to those of radical cystectomy . 
with these programs , cystectomy has been reserved for patients with incomplete response or local relapse after trimodality treatment . methods : this review summarizes series of radical rt with different fractionation schedules and focuses on cmt for muscle - invasive bladder cancer . 
current protocols of the bladder - sparing approach will be discussed and the background of future developments , including incorporation of promising new chemotherapeutic agents as well as the role of predictive and prognostic factors in selecting patients for the respective treatment alternatives , will be given . results : there is moderate evidence that hyperfractionated and accelerated regimens are superior to conventional rt at least in situations where no concomitant chemotherapy is applied . 
in modern series of cmt , 5 - year survival rates in the range of 5060% have been published , and about three quarters of the surviving patients maintained their own bladder . 
clinical criteria helpful in determining patients for bladder preservation include such variables as early tumor stage , unifocal tumor , a visibly and microscopically complete turbt , and absence of ureteral obstruction . conclusion : cmt for bladder cancer is a reasonable treatment option for patients who are deemed medically unfit for cystectomy and for those seeking an alternative to radical cystectomy . 
 key words : bladder cancer radiotherapy combined - modality treatment strahlenther onkol 2004 ; 180 : 7019 doi 10.1007 / s00066 - 004 - 9195 - y aktueller stand der radiotherapie und der multimodalen organerhaltenden therapie des blasenkarzinoms hintergrund : die standardbehandlung des muskelinvasiven harnblasenkarzinoms ist die radikale zystektomie . 
bei diesen behandlungskonzepten erfolgt die zystektomie nur bei inkomplettem tumoransprechen oder bei invasiven lokalrezidiven . methodik : dieser bersichtsartikel beschreibt verschiedene fraktionierungsschemata der radikalen radiotherapie und konzepte der multimodale therapie des muskelinvasiven harnblasenkarzinoms . 
zuknftige entwicklungen der chemotherapie sowie die rolle prdiktiver und prognostischer faktoren fr eine rationale patientenselektion werden diskutiert . ergebnisse : bei der radikalen radiotherapie sind hyperfraktionierte und akzelerierte regime der konventionell fraktionierten radiotherapie wahrscheinlich berlegen . 
moderne serien einer multimodalen behandlung der blasenkarzinoms zeigen 5 - jahres - berlebensraten in einer grenordnung von 5060% ; drei viertel der berlebenden patienten behalten ihre eigene , gut funktionierende blase . 
patienten mit frhen tumorstadien und unifokalen tumoren , bei denen die initiale transurethrale resektion eine r0 - resektion schafft , sind ideale kandidaten fr eine blasenerhaltende therapie . schlussfolgerung : die multimodale behandlung des blasenkarzinoms ist eine adquate therapiealternative fr patienten , bei denen eine radikale zystektomie nicht durchfhrbar ist oder die eine radikale operation ablehnen . 
combined modality treatment for bladder cancer introduction treatment of invasive bladder cancer remains a triple challenge : first , the eradication of local disease , second , the elimination of potential micrometastases , and , third , the maintenance of the best quality of life possible without compromising survival . 
organ preservation which has been successful in cancers such as breast cancer [ 1 , 16 ] , soft - tissue sarcomas [ 43 ] , and laryngeal carcinoma [ 30 ] , among others has been the subject of recent investigations in bladder cancer as well . 
with these programs , cystectomy has been reserved for patients with incomplete response or local relapse following cmt . radioand chemosensitivity of transitional cell carcinoma of the bladder urothelial cancers are relatively radiosensitive . 
 macroscopic disease will require 5560 gy to achieve complete regression in 50% of cases , doses > 60 gy are necessary for long - term local control in 50% of cases . transitional cell carcinomas of the bladder are also sensitive to chemotherapy . 
newer cytotoxic drugs with promising activity include gemcitabine , the taxanes , and ifosfamide . what is currently the best radiation prescription for treating bladder cancer ? standard fractionation a large variation in total dose , fractionation and overall treatment time have been reported . 
overall , no clear dose - response relationship could be established from retrospective analyses , however , two [ 20 , 35 ] of six nonrandomized studies [ 19 , 40 , 42 , 52 ] have found a poorer outcome in multivariate analysis when total doses < 57.560 gy have been applied . hypofractionation using hypofractionation ( common in the uk ) doses of 48.657.5 gy in fractions of 2.53.5 gy have been applied . 
there is only one small randomized study reporting on curative rt where increased dose per fraction ( 3 gy 3 days per week to 30 gy , 4 weeks break , than 1.5 gy to a total dose of 60 gy ) was compared with conventionally fractionated rt ( 1.5 gy ) to the same total dose [ 29 ]  . 
studies with larger fractions sizes of 5.76 gy once weekly to a total dose of 3039 gy suggested good treatment tolerance for elderly patients with poor performance status [ 32 , 46 ]  . 
randomized 168 patients to receive 1 gy three times daily to a total dose of 84 gy versus 2 gy once daily to a total dose of 66 gy [ 36 ]  . 
a meta - analysis based on the pooled data of these two studies gives moderate evidence of a survival benefit at 5 and 10 years and an increased local control rate of hyperfractionation compared with conventional fractionation [ 55 ]  . acceleration given the short potential doubling time for most transitional cell carcinomas of the bladder ( 58 days ) , accelerated rt may overcome radioresistance due to tumor cell repopulation . 
in a retrospective analysis , maciejewski & majewski reported a significant loss of local control for an estimated tcd50 of 63.3 gy when treatment was prolonged from 40 to 55 days [ 31 ]  . 
in 147 patients , no significant relation between overall treatment time and local control was found for patients treated by continuous - course rt [ 11 , 35 ]  . 
however , in the analysis of de neve et al . , split - course rt with a gap of 1 month and an overall treatment time > 75 days was associated with the worst local control rates . 
combined modality treatment for bladder cancer twice - daily fractions of 1.82.0 gy 5 days a week to total doses between 54 and 64 gy resulted in 80% complete responders and a local control rate of 56% at 2 years [ 9 ]  . 
used a concomitant boost technique to shorten the overall treatment time ( 40 gy in 2 - gy fractions to the small pelvis and 15 gy to the bladder tumor area concomitantly in 0.75 - gy fractions , yielding a total tumor dose of 55 gy in 20 fractions in 4 weeks ) : 74% of patients showed a complete remission , the actuarial 3 - year freedom of local progression was 55% [ 41 ]  . 
 four other phase ii studies of accelerated rt have shown acceptable toxicity and encouraging locoregional control rates ; however , no randomized study is available as yet [ 34 , 39 , 60 , 65 ]  . thus , three conclusions can be drawn from the data and literature with respect to total radiation doses and fractionation for bladder cancer : ( 1 ) for radical rt with standard fractionation without concomitant chemotherapy total doses > 57.560 gy should be applied to the bladder tumor . ( 2 ) hypofractionated rt ( e.g. , twice weekly 6 gy ) should be restricted to situations with palliative intent in elderly patients in order to relieve symptoms in patients with a short life expectancy . ( 3 ) there is moderate evidence that hyperfractionated and accelerated regimens are superior to conventional rt at least in situations where no concomitant chemotherapy is applied . radiotherapy as part of combined - modality treatment with selective bladder preservation the rationale for combining rt with chemotherapy after conservative surgery of the bladder tumor is twofold . 
first , certain cytotoxic agents may have the potential of sensitizing tumor cells to radiation and to inhibit ( accelerated ) repopulation during rt , thus increasing local cure rates . 
second , the high rate of occult metastases necessitates an attempt to eradicate occult metastases that have already developed in as many as 50% of muscle - invasive tumors . the centers to pioneer modern bladder preservation therapy using the multimodality therapeutic approach included the university of paris , france , university of erlangen , germany , and harvard university , cambridge , ma , usa . 
from paris began a prospective trial of preoperative radiochemotherapy ( rct ) , using 5 - fluorouracil ( 5 - fu ) and cisplatin and concomitant bifractionated split - course rt followed by cystectomy or additional rct [ 25 ]  . 
over the past 10 years , the concept of organ preservation by conservative surgery and combined rt and chemotherapy has been investigated in several prospective series from single centers and cooperative groups . 
 components of combined - modality treatment transurethral resection of the bladder tumor it has become increasingly clear in recent years that any component of the trimodality therapy contributes considerably to the overall success . 
 series clinical induction treatment stage neoadjuvant treatment concurrent treatment complete consolidation rct regimen response for complete responders ( % ) ( adjuvant chemotherapy ) 5 - year overall survival ( % ) 5 - year overall survival with bladder ( % ) sauer et al . 
11 urban & vogel transurethral resection ( r0 , if possible ) radiochemotherapy restaging turbt superficial residual tumor 2 4 weeks 4 6 weeks complete remission follow up rdel c . 
if a patient is now conferred to our department with a turbt performed externly , reresection biopsies of the periphery and the tumor bed and , if necessary , reresection of residual tumor are mandatory . 
 salvage cystectomy muscleinvasive residual tumor concurrent radiochemotherapy in the erlangen series , rt to the pelvic lymph nodes will deliver a total dose adequate to control microscopic disease ( 50.4 gy with conventional fractionation )  . 
the addition of concurrent chemotherapy in our series not only increased the rate of completely responding patients at restaging turbt as compared to rt alone , but was also associated with a significantly improved overall survival ( table 3 )  . 
this is in line with the only prospective , randomized comparison of rt alone versus rct in bladder cancer : an improved local control rate was reported when cisplatin was given in conjunction with rt [ 10 ]  . 
it is noteworthy , that the improved survival rates in the erlangen series with combined rct compared to rt alone were primarily an effect of the higher initial response and local control rates . 
the addition of chemotherapy did not show any impact on the development of distant metastases , which is also reflected in the contradictory , albeit mostly negative results of adjuvant and neoadjuvant chemotherapy in cystectomy - based series [ 12 , 59 ]  . the optimal regimen and combination of rt and chemotherapy remains to be established . 
the intensification of the erlangen concurrent chemotherapy protocols over the past 18 years clearly yielded an increasing rate of complete response rates with 61% of patients treated with rt alone , 66% after rct with carboplatin , 82% after rct with cisplatin , and 87% after rct with 5 - fu / cisplatin ( table 3 )  . 
this remains also true if adjusted to the most important prognostic factor , the completeness of the initial turbt , with the rate of complete response after incomplete turbt ( r1 / 2 resection ) being 46% after rt alone , 57% after rct with carboplatin , 78% after rct with cisplatin , and 82% after rct with 5 - fu / cisplatin . newer chemotherapeutic agents , particularly gemcitabine and the taxanes , have shown significant single - agent activity against urothelial tumors and both have exhibited higher response rates and acceptable toxicity when used in combistrahlenther onkol 2004 no . 
impact of completeness of the initial transurethral resection ( r0 , r1 , r2 resection ) on overall survival after combined - modality treatment for bladder cancer ( results from the erlangen series )  . 
 treatment period n clinical stage rt / rct complete response ( % ) , overall ( after incomplete turbt ) 5 - year overall survival ( % ) 5 - year overall survival with bladder ( % ) 19821985 19851993 19851993 19932000 126 95 145 49 t1 ( high risk ) to t4 t1 ( high risk ) to t4 t1 ( high risk ) to t4 t1 ( high risk ) to t4 rt alone rt plus carboplatin rt plus cisplatin rt plus 5 - fu / cisplatin 61 ( 46 ) 66 ( 57 ) 82 ( 78 ) 87 ( 82 ) tively , have also recently been published [ 14 , 37 , 58 ]  . 
the rtog started a trial using paclitaxel and cisplatin concomitantly with twice - daily irradiation followed by either selective bladder preservation or radical cystectomy and adjuvant chemotherapy with gemcitabine and cisplatin ( rtog 99 - 06 )  . 
 future aspects of radiosensitization relate to the potential inhibition of oncogene products frequently activated and overexpressed in bladder cancer , such as h - ras and c - erbb - 1 . 
 treatment of mice expressing activated h - ras bladder cancer cell line tumors with farnesyltransferase inhibitors ( which inhibit the posttranslational modifications of h - ras ) before irradiation significantly decreased tumor cell clonogenicity and tumor regrowth [ 8 ]  . 
inhibition of epidermal growth factor ( egf ) receptor activity with small molecule tyrosin kinase inhibitors or antibodies against receptors may also markedly increase tumor radiosensitization in bladder cancer [ 3 ]  . salvage treatment for nonresponding and recurrent carcinomas salvage treatment plays an important and integrative role in any bladder - preserving treatment approach . 
only complete responders are considered good candidates for bladder preservation , and procede with a consolidation therapy with a total dose to the bladder tumor volume of up to 64 gy . both strategies have theoretical advantages . 
the late response evaluation may theoretically increase the chance of bladder preservation , because some slow responders whose tumors have not yet completely regressed after 40 gy may maintain their bladder with a delayed response evaluation . 
so far , however , both approaches seem to be equally effective in terms of long - term survival and bladder preservation . of patients who undergo turbt + rt / rct , approximately 2030% will present with residual tumor at restaging turbt and further 2030% of patients with completely responding tumors will develop de novo or recurrent disease in the preserved bladder . 
these tumors can be successfully managed by conservative surgery again , either alone or in combination with intravesical chemoor immunotherapy [ 62 ]  . muscle - invasive persistent or recurrent tumors require a salvage cystectomy . 
in the erlangen series , 83 of 415 patients ( 20% ) underwent salvage cystectomy for invasive residual or recurrent tumor : 41 of 110 non - complete responders ( 37% ) and 42 of 288 patients ( 15% ) with initial complete response , who experienced a local relapse . 
salvage cystectomy was radical ( r0 ) in all but five patients ( in four patients with nonresponding tumors and in one patient with an invasive relapse only r1 / r2 resections were achieved )  . 
disease - specific survival rates at 5 and 10 years ( as calculated from the time of salvage cystectomy ) for patients treated by salvage cystectomy for an invasive relapse were 51% and 45% . 
thus , close follow - up of patients after organ - preserving treatment is clearly indicated to maintain a second curative approach by salvage surgery in case of local failure . 
we recommend that patients should be followed at 3 - month intervals for the first 2 years and every 6 months thereafter . acute toxicity and chronic sequelae of combinedmodality treatment typical acute radiation - induced side effects , such as transient urocystitis and enteritis , are common and easily managed by symptomatic treatment . 
in our own experience , patients with a history of multiple turbts or multiple courses of intravesical chemoor immunotherapy prior to rct are predisposed to develop some kind of acute radiation cystitis , and are also at greater risk ( although low overall ) to suffer from bladder shrinkage thereafter . 
combined modality treatment for bladder cancer the total doses in current protocols lie in the range of about 60 gy to the whole bladder , and 64 gy to parts of the organ . 
 these doses , if administered in conventional fractionation with single doses of 1.82 gy , can be considered safe with regard to late bladder toxicity . a survey among 71 long - term survivors after radical rt for bladder cancer as well as 251 cystectomized patients and 310 population controls using an anonymously answered postal questionnaire revealed that three quarters of the irradiated patients had a functioning bladder with little or no distress from the urinary tract [ 23 ]  . 
the boston group has recently performed functional urodynamic studies and a validated quality of life questionnaire in 32 long - term survivors of their 19862000 trimodality protocols [ 63 ]  . 
 predictive and prognostic factors patient selection as more experience is acquired with organ - sparing treatment , it is clear , that future directions of clinical and basic research will focus on two main topics : ( a ) the optimization of the treatment modalities , including incorporation of new cytotoxic agents , and ( b ) the proper selection of patients who will most probably benefit from the respective treatment alternatives . 
 clinical criteria helpful in determining patients for bladder preservation include such variables as early tumor stage , unifocal tumor , a visibly and microscopically complete turbt , and absence of ureteral obstruction or associated carcinoma in situ . to further optimize patient selection , it should be of pivotal interest to recognize the subgroup of tumors which do not respond to rt / rct . 
in the erlangen series , patients with nonresponding tumors showed a 5 - year disease - specific survival rate of only 21% , even when salvage cystectomy could be performed , and > 40% developed distant metastases within the first 2 years . 
evidently , these tumors have a biologically less favorable profile , and prompt cystectomy , possibly combined with more aggressive adjuvant chemotherapy , might be more effective in these patients . 
in our analysis , the presence of histopathologic markers that indicate more aggressive tumors , like associated tis , g3 / g4 , multifocality and lymph vessel involvement , revealed no impact on initial response to rt / rct . 
translational research to identify molecular markers that may better determine a tumors true malignant potential as well as its response to specific cytotoxic therapies are sorely needed . overall , the findings on molecular markers do not yet confirm that abnormal expression of any of these proteins unequivocally predicts tumor response with possibly one exception : higher rates of spontaneous apoptosis were significantly related to better initial response and better local control with bladder preservation in most studies [ 7 , 22 , 33 , 45 ]  . 
 it is now becoming increasingly clear , that the inability to undergo apoptosis due to overexpression of bcl - 2 or survivin , a member of the inhibitor of apoptosis family , may predict local failure after irradiation and chemotherapy . 
reported excellent overall survival rates which , according to the authors , should be considered the surgical standard to which other treatment modalities should be compared [ 54 ]  . 
 this cystectomy series , however , included 213 patients ( 20% ) with noninvasive ( t0 , ta , tis ) bladder cancer and excluded 112 patients with inoperable tumor , unradical surgery or intraoperative detection of distant metastases . 
conversely , the erlangen , boston and rtog series did not include superficial noninvasive tumors and did not exclude patients who were , for different reasons , unsuitable for surgery . 
if comparison is restricted to the respective groups , the 5 - year overall survival rates of this radical cystectomy series and the bladder - sparing approaches become equal : 74% and 75% , respectively , for t1 tumors , and 47% and 45% , respectively , for muscle - invasive disease . notwithstanding the limitations of nonrandomized comparison , this analysis indicates that selective bladder preservation by trimodality treatment may result in long - term cure and survival rates comparable to the best cystectomy series , allowing this treatment to be considered a reasonable treatment option for patients who are deemed medically unfit for cystectomy and for those seeking an alternative to radical cystectomy . 
grabenbauer1 background and purpose : according to recent data medial location of early breast cancer was associated with a higher risk of systemic relapse and breast cancer death compared with lateral location . 
this paper will focus on literature data and will also present own data on the prognostic impact of radiation therapy ( rt ) to internal mammary nodes ( imns ) in early breast cancer patients with medial hemisphere tumor location . 
at the department of radiation oncology , university of erlangen , germany , a total of 822 patients ( 492 with lateral and 330 with medial lesions ) with early breast cancer were treated by surgery and postoperative rt with or without chemotherapy ( 19851996 )  . 
according to our data , rt with a total dose of 50 gy to imns in breast cancer patients with medial lesions was associated with os and sdfs rates comparable to patients with lateral tumors . 
 key words : medial breast cancer radiotherapy internal mammary nodes strahlenther onkol 2004 ; 180 : 6904 10.1007 / s00066 - 004 - 9193 - 0 parasternale lymphknoten beim invasiven mammakarzinobedeutung der radiotherapie hintergrund und ziel : nach neueren daten scheint ein in den medialen quadranten lokalisiertes mammakarzinom mit einem eindeutig erhhten risiko fr fernmetastasen und einem hheren sterberisiko einherzugehen als der laterale tumorsitz . 
fr den endpunkt fernmetastasierung wurde eine hazard - ratio ( hr ) von 1 , 29 ( zucali et al . ) , fr das tumorspezifische berleben eine hr von 1 , 311 , 46 1 department of radiation oncology , university of erlangen , erlangen , germany . 
von 80 , 8% auf 75 , 7% ab ( lohrisch et al . ) , wenn laterale mit medialen tumoren verglichen wurden . bei den 822 in erlangen therapierten patientinnen betrug das 5 - jahres - berleben fr laterale tumoren 76 , 2% , fr mediale tumoren dagegen 79 , 1% . 
die bestrahlung der medialen lymphabflsse mit 50 gy bei patientinnen mit medialem tumorsitz fhrte im eigenen krankengut zu einer prognoseverbesserung mit berlebensraten , die denen bei patientinnen mit lateralem tumorsitz vergleichbar sind . schlsselwrter : medialer tumorsitz mammakarzinom parasternale lymphknoten strahlentherapie the fact : diminished survival in patients with inner versus outer quadrant tumors recent studies have implicated a medial or central breast tumor location as a negative prognostic factor on risk of relapse and overall survival ( os ) [ 7 , 10 , 17 , 37 ]  . 
 [ 37 ] who evaluated a total of 2 , 396 patients , a subgroup of 777 women with medial tumors had an excess risk of 30% for distant metastases and , additionally , an excess mortality rate of 20% . 
 women with low - risk cancer did not experience any impact of tumor location on outcome , whereas patients with high - risk factors , such as tumor diameter > 20 mm , nodal disease , negative receptors or invasion of lymphatic or blood vessels , had an excess risk of 50% for both distant metastases and tumor - associated death . 
the most recent study evaluated a total of 45 , 880 patients with invasive breast cancer using the surveillance , epidemiology , and end results ( seer ) registries in the usa [ 7 ]  . 
both for node - negative and node - positive patients , inner versus outer quadrant tumor location was predictive for os and breast cancer - specific survival ( bcss ) rates . 
 reasons for increased risk of metastases and death from breast cancer in medial and central tumors a proposed mechanism for the increased risk of metastases and death from breast cancer from medial tumors is occult involvement of internal mammary lymph nodes ( imns ) that are not systematically treated with either surgery or radiation therapy ( rt )  . 
with the advent of sentinel lymph node biopsies , primary drainage to the imns occurs in 945% of breast cancers ; however , the rates of histological positivity seem to be lower . 
imn irradiation in invasive breast cancer the rate of positive imns for patients with negative and positive axillary lymph nodes ranged from 8% to 13.7% and 28% to 48% , respectively . 
a review of > 7 , 000 patients has shown that isolated , clinically detectable imn metastases occurred only in 5% of the patients during the course of disease progression [ 11 , 16 , 34 , 35 ]  . 
this is currently being investigated in a national cancer institute of canada trial in intact breast cancer patients and in a european organization for research and treatment of cancer ( 22922 ) trial of postmastectomy patients . 
 by contrast , one retrospective analysis evaluating treatment to the imns and three recent randomized trials in axillary node - positive postmastectomy patients revealed a relatively large impact on os in favor of the patient groups receiving rt , with an improved hr similar to the magnitude of systemic chemotherapy or tamoxifen [ 3 , 2022 ]  . 
a modest overall improvement in survival would be expected because isolated metastases to imns occur only in approximately 5% of patients . rt is a possible mechanism for a promotion of improved survival . 
in the danish 82b trial , there was a 12% improvement in survival at 10 years in node - negative patients that received rt [ 21 ]  . significant controversy surrounds targeting of the imns with rt [ 1 , 2 , 4 , 6 , 8 , 9 , 12 , 13 , 18 , 19 , 24 , 25 , 2833 ]  . 
recent analysis of patients treated in the danish randomized trials who received rt to the chest wall and regional lymphatics including imns did not show an adverse effect on cardiovascutable 2 . 
hufigkeit von befallenen mammaria - interna - lymphknoten ( imn ) beim operablen mammakarzino population patients ( n ) positive imns pn0 ( axilla ) operable , imn biopsy cn + and / or inner location < 7 cm , n01 m0 outer > 2 cm or cn + , inner and < 70 years of age 1 , 000 455 703 1 , 119 pn1 ( axilla ) 187 99 105 8 13.7 9 162 authors handley [ 11 ] urban [ 34 ] lacour et al . 
imn irradiation in invasive breast cancer patients with medial tumors ( n = 330 ) patients with medial tumors ( n = 330 ) patients with lateral tumors ( n = 492 ) p = 0.2 patients with lateral tumors ( n = 492 ) p = 0.3 time ( years ) time ( years ) figure 1 . 
overall survival for 822 patients with early breast cancer including 330 patients with medial tumors and radiotherapy to internal mammary nodes ( imns ) compared to 492 patients with lateral tumors without radiotherapy to imns . 
gesamtberleben von 822 patientinnen mit einem frhen mammakarzinom ; eingeschlossen sind 330 patientinnen mit medialen tumoren und bestrahlung der mammaria - interna - lymphknoten im vergleich zu 492 patientinnen mit lateralen tumoren , die keine bestrahlung der mammaria - interna - lymphknoten erhielten . 
metastasen - freies berleben von 822 patientinnen mit einem frhen mammakarzinom ; eingeschlossen sind 330 patientinnen mit medialen tumoren und bestrahlung der mammaria - internalymphknoten im vergleich zu 492 patientinnen mit lateralen tumoren , die keine bestrahlung der mammaria - interna - lymphknoten erhielten . 
however , in the past and probably even today rt to imns per se has been regarded as a potentially harmful treatment being associated with an excess risk of late cardiac morbidity and mortality ; e.g. , the stockholm trial demonstrated an increase in cardiovascular deaths in patients that received photons to the left chest wall [ 27 ]  . 
a recent seer registry - based study demonstrated an increase in cardiovascular deaths in women < 60 years of age who received adjuvant rt for left - sided breast cancer compared with patients treated for right - sided lesions [ 23 ]  . 
 the fiction : radiation therapy to internal mammary nodes may improve survival in medial and central tumors ( data from the university of erlangen , germany ) since 1980 , it has been the ongoing and continuing policy of our department to offer all patients with breast cancer involving the medial quadrants an additional rt to imns irrespective of the axillary nodal status . 
rt with a total dose of 50 gy and single fractions of 2 gy was applied by a mixed - beam technique using 6 - mv photons and electrons between 712 mev in an alternating fashion . 
this section will specifically focus on the outcome of 822 patients with early breast cancer treated between 1985 and 1996 and compare both the risk for distant metastases and death among patients with lateral and medial tumors . 
 the following inclusion criteria for this retrospective analy sis were selected : t1 or t2 category , primary unilateral breast cancer , complete surgery ( no residual tumor ) including axillary dissection , complete rt , complete follow - up , absence of distant metastases at diagnosis . 
 both os and systemic disease - free survival ( sdfs ) rates were consistently superior for the group of patients with medial tumor location as compared to patients with outer quadrant tumors . 
imn irradiation in invasive breast cancer conclusion literature data on > 50 , 000 patients with invasive breast cancer treated by surgery , rt to the breast / chest wall only with or without systemic therapy strongly indicate a negative impact of medial tumor location on both survival and the development of distant metastases . 
this article reviews preclinical and phase i clinical studies that reported on combining inhibition of activated ras and downstream effectors of ras with radiotherapy . material and methods : transfection studies and rna interference were used to check the role of the ras isoforms for intrinsic radiation sensibility . 
simultaneous treatment with l - 778 , 123 and irradiation was performed in non - small cell lung cancer , head and neck cancer , and pancreatic cancer patients . results : radiation sensitization was achieved in vitro and in vivo blocking the prenylation of ras proteins in cell lines with ras activated by mutations or receptor signaling . 
combined treatment in a phase i study was safe and effective . conclusion : the rational combination of ftis with radiotherapy may improve the clinical results of patients with tumors who bear mutant or receptor - signaling activated ras . key words : ras radiation pi3 kinase farnesyltransferase strahlenther onkol 2004 ; 180 : 73140 doi 10.1007 / s00066 - 004 - 9198 - 8 strahlensensibilisierung durch inhibition von aktiviertem ras hintergrund und ziel : ras wurde als signifikanter faktor der strahlenresistenz erkannt . 
dieser artikel gibt einen berblick ber prklinische studien und klinische phase - i - studien zur kombinierten inhibierung von aktiviertem ras und von ras - effektoren mit radiotherapie . material und methodik : transfektionsstudien und rna - interferenz kamen zur anwendung , um die rolle der ras - isoformen fr die intrinsische radiosensibilitt zu untersuchen . 
patienten mit nichtkleinzelligem bronchialkarzinom , kopf - hals - tumoren und pankreaskarzinom wurden simultan mit l - 778 , 123 und radiotherapie behandelt . ergebnisse : strahlensensibilisierung wurde in vitro and in vivo nach blockade der prenylierung von ras - proteinen in zelllinien mit ras - aktivierung durch mutationen oder rezeptorsignalaktivitt erreicht . 
unter den vielen ras - downstream - signalwegen wurde die bedeutung des beitrags des phosphoinositol - 3 - ( pi3 - ) kinase - akt - weges zur strahlenresistenz identifiziert . 
die kombinationsbehandlung war in einer phase - i - studie sicher und wirksam . schlussfolgerung : die kombination von ftis mit bestrahlung ist ein ansatz , der die klinischen ergebnisse von patienten mit tumoren verbessern knnte , bei denen ras mutiert oder ber rezeptorsignale aktiviert ist . schlsselwrter : ras strahlen pi3 - kinase farnesyltransferase 1 department of radiation oncology , university hospital , erlangen , germany , 2 department of radiation oncology , university of pennsylvania , philadelphia , pa , usa . 
radiation sensitization by inhibition of activated ras introduction the combination of irradiation with chemotherapy has been a major step forward to achieve responses and prolongation of survival in many tumor entities . 
combined treatment has become standard in tumors such as gastrointestinal tumors [ 76 ] , lung cancer [ 69 ] , head and neck cancer ( hnc ) [ 42 ] , and bladder cancer [ 60 ]  . 
radiation resistance has been shown to be increased by ras activation in rodent and tumor cells [ 49 ]  . the understanding of the posttranslational modifications of ras together with the identification of the responsible enzymes involved led to the synthesis of farnesyltransferase inhibitors ( ftis ) , compounds that inhibit farnesyltransferase ( ftase )  . 
cysteine palmitoylation sites are contained in h - ras , n - ras , and k - ras4a or a polylysine domain in k - ras4b as depicted by positive charges in the figure . 
nach der prenylierung sind die nchsten schritte der posttranslatorischen modifikation eine aax - proteolyse durch rce1 und dann eine - carboxymethylierung von farnesylierten cysteinresten durch die isoprenylcystein - carboxyl - methyltransferase . 
 h - ras ist exemplarisch fr die drei palmitoylierten formen gezeigt . the three mammalian ras genes yield four ras proteins : h - ras , n - ras , k - ras4a , and k - ras4b . 
the hypervariable region ( hvr ) after amino acid 165 ( c - terminal region ) can be divided into two domains : the linker domain and the membrane - targeting domathe membrane - targeting domain consists of a c - terminal caax box ( c : cysteine , a : aliphatic , x : any amino acid )  . 
 it is common to all ras proteins and serves as the primary membrane - targeting domaa secondary membrane - targeting domain , also situated in the hvr , contains cysteine palmitoylation sites in h - , n - , and k - ras4a or a polylysine domain in k - ras4b [ 30 , 31 , 77 ] ( figure 1 )  . 
prenyltransferases recognize the caax box [ 21 ] , and the transforming activity of ras proteins is lost when mutations in the caax sequence block prenylation and attachment to the plasma membrane [ 8 , 35 , 77 , 78 ]  . 
these findings led to the development of pharmacological compounds that inhibit prenyltransferases . functions and pathways of ras the binding of gtp ( guanosine triphosphate ) activates cellular ras proteins for signaling ( figure 2 )  . 
this is a common finding in many tumors including lung and breast cancers [ 51 , 54 ]  . ras proteins are hubs in signal transduction from receptor tyrosine kinases . 
two well - characterized pathways are the raf - map ( mitogen - activated protein ) kinase pathway and the phosphoinositide 3 ( pi3 ) kinase pathway ( reviewed in [ 28 ] )  . 
 this complex of transcription factors regulates genes as for instance matrix metalloproteinases , a heparin - binding form of egf and gm - csf ( granulocyte - macrophage colony - stimulating factor )  . 
thus , ras signaling can induce genes involved in the process of tumor invasion , tumor stroma formation , and growth control . ras proteins also stimulate pi3 kinases , which have multiple direct and indirect targets such as phosphoinositide - dependent kinases ( pdks ) , p70s6k , rac , and guanine exchange factors [ 9 ]  . 
 the inhibition of prenyltransferases prenylation by ftase is the first and obligate step in h - ras processing that results in a functional ras protein ( reviewed in [ 4 ] ) ( figure 1 )  . 
since the addition of a prenyl side chain is required for ras membrane localization , which is in turn necessary for oncogenic ras - mediated transformation , several groups have developed inhibitors specific for one of the two prenyltransferases involved in ras processing . 
by inhibiting its posttranslational processing , these compounds inhibit h - ras activity , whose processing is inhibited by ftis alone . by contrast , k - ras is prenylated at its enzyme recognition caax site with a 20 - carbon geranylgeranyl group by the enzyme geranylgeranyltransferase - i when farnesylation is blocked . 
inc. , r115777 from janssen pharmaceuticals , fti - 276 , and its methyl ester fti - 277 , additionally , the ggtis ggti 297 and its methyl ester ggti - 298 from drs . 
 effects of farnesyltransferase inhibitors in preclinical models initial studies of ftase inhibitor activity demonstrated reversion of morphological transformation and inhibition of tumor growth of cells transformed by oncogenic h - ras . however , these inhibitors had no effect on the behavior of cells transformed by other oncogenes such as raf - 1 , or of cells transformed by h - ras genetically modified to be attached to the membrane via myristylation or by prenylation by a geranylgeranyl group [ 14 , 56 , 57 ]  . 
the expected picture of fti specificity was significantly changed when subsequent studies of human tumor cells showed that these inhibitors are effective in blocking the growth of a wide variety of tumor cell lines both with and without ras mutation . 
it was also shown that they block the growth of rodent tumors and human tumor xenografts in vivo , some of which express wild - type - ( wt - ) ras . 
radiation sensitization by inhibition of activated ras cally target ras , it is apparent that this class of compounds has activity on prenylated proteins other than ras that are involved in promoting transformed cell growth . 
it now appears that growth inhibition by ftase inhibitors cannot be predicted , either by the mutation status of tumor cells , or by their tissue of origin this context it is the more surprising that fti treatment had little effect on the growth of normal cells , and both preclinical data and phase i clinical trials have demonstrated a relatively low level of normal cell and tissue toxicity associated with fti treatment [ 64 ]  . activated ras imparts radiation resistance many studies have shown that radiation resistance is influenced by ras activation . 
more evidence for the influence of the different isoforms of ras ( h - , k - , and n - ras ) on intrinsic radiation resistance came from transfection experiments with activating mutations in the respective genes coding for the isoforms of ras in several human tumor cell lines [ 3 , 5 , 32 ]  . 
changes in cell cycle distribution were excluded to be relevant for these effects , because no differences in cell cycle distribution were observed between parental cells and cells with loss of the activated ras allele , but radiation resistance correlated with expression of activated ras [ 5 ]  . farnesyltransferase inhibitors diminish ras - induced radiation resistance the discovery that activated ras goes along with increased radiation resistance led to the question of whether ras inhibition would lead to specific radiation sensitization of cells with activation of ras signaling . 
the fact that it is theoretically easier to shut off an activated oncogene than to restore lost activity of a tumor suppressor prompted molecular targeting of ras and the development of prenyltransferase inhibitors . in contrast to the aforementioned studies of tumor growth inhibition we have focused on the effects of prenyltransferase inhibitors on radiosensitivity in terms of survival while controlling for growth inhibition . 
in this respect it is important to point out the way we combined fti and radiation treatment , because methodological problems could have attributed at least in part to negative results in recently reported studies where ftis were combined with irradiation [ 46 , 50 ] : to test the influence of ras on radiation sensitivity , ras function needs to be blocked at the time of irradiation and therefore cells were exposed to ftis 24 h before radiation treatment . 
other assays like the mtt ( 3 - ( 4 , 5dimethylthiazol - 2 - yl ) - 2 , 5 - diphenyltetrazolium bromide ) assay [ 46 ] or apoptosis assays , while useful for determining growth inhibition , are not adequate for measuring clonogenic survival after irradiation [ 7 ]  . farnesyltransferase inhibitors and radiosensitivity synergistic radiation - induced cell killing after prenyltransferase inhibitor treatment was observed in both rodent and human tumor cells with ras mutations [ 3 , 12 ]  . 
radiation sensitization was not unique to certain tissues of orig testing cells from bladder ( t24 ) , breast ( hs578t ) , colon ( sw480 ) , lung ( a549 ) , and fibroblasts ( ht1080 ) gave consistent results of sensitization allowing a generalization of the observation for all cells independent of their origin with activated ras status . 
the correct balance of ftase and ggtase inhibition for blocking k - ras prenylation in vivo has not yet been established , and therefore in vivo radiosensitization of tumors expressing k - ras mutations has been more difficult to demonstrate . 
more recent work implies that in some tumors with k - ras activation by mutation , inhibition of h - ras may be sufficient for radiosensitization ( brunner tb , manuscript in preparation , [ 63 ] )  . tumor cell lines with ras activity stimulated by receptor tyrosine kinase activation were also radiosensitized by farnesyltransferase inhibition as demonstrated by gupta et al . 
the line with wt - ras status was isolated from one of the responding patients participating in the phase i trial with combined l - 778 , 123 and radiation therapy ( see below , [ 29 ] )  . 
radiation sensitization by inhibition of activated ras our laboratory radiosensitization by prenyltransferase inhibitors in preclinical tests is specific to tumor cells with oncogenic or activated ras , others have noted effects in cells where ras is not thought to be activated [ 13 ]  . 
possible candidate targets in the context of cancer treatment include rhob [ 43 ] , the phosphatases prl - 1 , - 2 , and - 3 [ 79 ] , and cenp - e and - f centromeric proteins ( reviewed in [ 72 ] )  . 
an important argument against the role of these proteins as targets for radiosensitization is that radiosensitization would also be expected for normal cells and not only cells with ras activation , which has not been the case in our studies [ 2 , 12 ]  . more confirmation for ras as the relevant target of ftis in the context of radiosensitization comes from different approaches to inhibit ras expression or activity . 
recently , small interfering rna ( sirna ) experiments have been performed in our laboratory to shut down gene expression by rna interference ( rnai ; reviewed in [ 66 ] , [ 17 ] )  . 
we have targeted specific ras isoforms such as k - ras ( figure 2 ) and shown that in the sw480 colon cancer cell line , downregulation of oncogenic k - ras expression by k - ras allele - specific sirna treatment reduces radiation survival [ 40 ]  . 
taken together , the studies cited above strongly implicate ras signaling in promoting the radiation survival of tumor cells and at the same time ras as the target of prenyltransferase inhibitors treatment when combined with irradiation . since many of the human tumor models we have studied as xenografts contain extensive regions of hypoxia and hypoxic cells are markedly more resistant to killing by radiation [ 73 , 74 ] , we investigated the effects of ftis on tumor xenograft hypoxia [ 11 ]  . 
l - 744 , 832 treatment resulted in a reduction in hypoxia in tumors that expressed activated h - ras ( cell lines t24 , 141 - 1 ) , but not in tumors with normal ras ( cell lines ht - 29 , rt - 4 )  . 
in these tumors , egf receptor is overexpressed leading in turn to pi3 kinase - driven vegf ( vascular endothelial growth factor ) overexpression similar to that seen in cells with ras mutations [ 47 ]  . 
this finding could be of significance to combined treatment with ftis and chemotherapeutics as well , since hypoxic tumors show resistance to these agents [ 73 ]  . in search for the missing link ( s ) connecting ras to radioresistance many downstream pathways of ras signaling have been described and their implications for survival after radiation are under investigation . 
pharmacological inhibitors of mek ( pd98059 , in later studies u0126 ) , pi3 kinase ( ly294002 ) , p70s6k ( rapamycin ) , and p38 ( sb203580 , pd169316 ) and an fti ( l - 744 , 832 ) were used in activated h - ras t24 bladder cancer cells . 
this approach was used to confirm the effects of the specific inhibitors on the respective pathways by immunoblotting the activated proteins or phosphorylated forms of the proteins mapk , akt , p70s6k , and p38 . 
whereas the pi3 kinase inhibitor ly294002 sensitized t24 cells to a similar extent as obtained after l - 744 , 832 treatment , none of the other inhibitors modified radiation sensitivity . 
to exclude that the observation of the significance of pi3 kinase in ras - mediated radiation resistance was unique to this cell line , 3.7 refs with activated h - ras , dld - 1 colon carcinoma cells with activated k - ras and two cells lines with wt - ras ( rt4 bladder carcinoma and mr4 ref ) were tested in the following experiments . 
subsequently , rt4 and mr4 cell lines transfected with the constitutively active pi3 kinase p110 subunit under control of a dexamethasone - sensitive promoter were more radioresistant after addition of dexamethasone . 
the significance of the pi3 kinase pathway in radiation resistance has been confirmed by transfecting ht1080 - expressing activated n - ras with a plasmid - encoding pten ( phosphatase and tensin homoloque deleted on chromosome ten ) phosphatase . 
overexpression of this phosphatase which antagonizes pi3 kinase activity by dephosphorylating ip3 [ 52 ] rendered ht1080 cells more sensitive to radiation compared to the parental cells with normal pten expression ( unpublished observations )  . 
 the contribution of pi3 kinase signaling to radiation survival has been demonstrated in a number of cell lines and by several groups [ 23 , 34 , 44 , 71 ]  . 
probing signaling pathways with the highly specific tool of rnai will probably allow to define new potential targets for molecular interventions in combination with radiotherapy . other ras downstream pathways have been implicated in radiation survival . 
induction of map kinase signaling by radiation exposure [ 39 ] , radiosensitization of mda mb231 breast carcinoma cells after mek inhibition [ 58 ] , and similar findings in prostate and myeloid cells [ 10 , 27 ] have been reported . 
upstream of ras receptor tyrosin kinases ( rtk ) like epidermal growth factor receptor ( egfr ) or platelet - derived growth factor receptor ( pdgfr ) are stimulated by an extracellular signal leading to dimerization and autophosphorylation of src - homology - 2 ( sh2 ) domains on the intracellular surface of the proteconsequently , grb , an adapter protein , binds via its sh2 domains . 
activated gtp - ras stimulates proliferative cellular processes through the activation of multiple pathways ( e.g. , raf ; mitogen - activated erk kinase [ mek ] ; jun n - terminal kinase [ jnk ] ; rac / rho , phospholipase c [ plc ] and phosphoinositide 3 kinase [ pi3k ] )  . 
akt has multiple downstream targets ( e.g. , gsk3 ; fkhr ; p21waf1 ; cyclin d / e ; p27kip1 , nos ; bad ; p70s6k ; mtor )  . 
egfr ( epidermal growth factor receptor ) oder pdgfr ( platelet - derived growth factor receptor ) durch ein extrazellulres signal stimuliert , was zur bildung von dimeren und autophosphorylierung von src - homologie - 2 - ( sh2 - ) domnen an der intrazellulren oberflche des proteins fhrt . 
radiation sensitization by inhibition of activated ras groups did not observe radiosensitization upon inhibition of this pathway [ 1 , 23 , 25 ]  . raf is another member within the signaling cascades of the ras oncogene . 
an activated raf allele was shown to result in radiation resistance , and antisense c - raf - 1 was able to cause sensitization to radiation in vitro [ 3638 , 55 , 70 ] and in vivo [ 22 ]  . 
similarly , contribution of raf to radiation survival was shown by a constitutively active form of raf or expression of an oncogenic h - ras effector mutant that retains the ability to promote raf activation in a rat intestinal epithelial cell model [ 75 ]  . 
the authors of this report concluded that the contribution of raf is map kinase - independent as map signaling did not contribute to radiation survival in this study [ 23 ]  . taking into consideration all these results , ( 1 ) ras activation by mutation or upstream signaling can increase intrinsic radiation resistance of tumor cells through activation of pi3 kinase . 
 ( 3 ) the relatively high activity of ftis in combination with irradiation in vivo can be explained in part by enhancement of both apoptosis and oxygenation in these tumors . 
these changes could contribute significantly to tumor radiosensitization , even if the mechanisms for these observations are not yet fully understood . it is possible that differences in the signal transduction specificity of the different isoforms of ras could be significant in this regard . 
since k - ras is the most frequently mutated form of ras in human malignancies , a perceived problem in the development of ftis has been their poor activity against k - ras because of its ability to be alternately prenylated . 
the fti used in this trial , l - 778 , 123 ( merck research laboratory , rahway , nj , usa ) , is a peptidomimetic inhibitor of farnesyltransferase . 
the recommended phase ii dose was found to be 560 mg / m2 / day by continuous infusion over 2 weeks in a phase i trial of prolonged continuous infusion of l - 778 , 123 alone . 
the dose - limiting toxicities ( dlts ) of this regimen were grade 4 neutropenia and prolongation of the corrected qt interval ( qtc ) on electrocardiogram ( ecg )  . the primary endpoint of this phase i trial was to establish the maximally tolerated dose and dlts of l - 778 , 123 in combination with radiation . 
response reporting was based upon the best response achieved observed in any follow - up scan . a total of nine patients were enrolled , six patients had nsclc : two with unresectable stage iiia disease and four with stage iiib disease . 
comparison of the observed toxicities with those seen with concurrent chemo - radiation treatment at these sites was favorable . response assessment was not the primary endpoint of this trial , but nevertheless responses were evaluated after the completion of therapy . 
the second patient had a stroke and was lost to follow - up . one of the six patients with nsclc had dlts and distant metastatic disease and , therefore , was taken off study . 
 a second stratum of this phase i trial enrolled twelve patients with pancreatic cancer treated with l - 778 , 123 at the same two dose levels than above and concomitant radiotherapy to 59.4 gy in standard fractions [ 48 ]  . 
 other common toxicities were mild neutropenia , dehydration , hyperglycemia , and nausea / vomiting . therapy was completed in eight patients and all of them had evaluable disease by radiologic measurements within 12 weeks of completion of radiotherapy . 
radiosensitization of a study patient - derived cell line was demonstrated in the presence of l - 778 , 123 and went along with reduction of high baseline phospho - akt and phospho - map kinase levels after fti treatment . conclusion in summary , ras activation has been identified as a contributor to radiation resistance of tumor cells in a series of studies from multiple laboratories . 
likewise , inhibiting ras by a variety of techniques including prenylation inhibition has been shown to sensitize tumors cells with mutant or wild - type but activated ras through upstream signaling for radiation in vitro and in vivo . 
further preclinical work will have to show if different tumors share one common signaling pathway or if variants of signaling exist that require specific targeting for radiosensitization . strahlentherapie und onkologie original article long - term results after external radiotherapy in age - related macular degeneration a prospective study ulrike prettenhofer1 , anton haas2 , ramona mayer1 , heidi stranzl1 , astrid oechs1 , arnulf hackl1 purpose : to prospectively evaluate the shortand long - term efficacy of external radiotherapy ( rt ) in patients with age - related macular degeneration ( amd ) by comparing two different dose schedules . 
 patients and methods : in this prospective , nonrandomized , comparative study including 80 patients , the efficacy of external rt with a total dose of 14.4 gy ( group a , n = 40 ) and 25.2 gy ( group b , n = 40 ) was compared . 
 conclusion : external rt of amd with 14.4 gy as well as with the escalated dose of 25.2 gy showed a poor beneficial outcome after 6 and 12 months , respectively . 
 key words : age - related macular degeneration external radiotherapy prospective study long - term results strahlenther onkol 2004 ; 180 : 915 doi 10.1007 / s00066 - 004 - 1177 - 6 langzeitergebnisse nach externer strahlentherapie der altersabhngigen makuladegeneration . 
 patienten und methodik : in dieser prospektiven , nicht randomisierten , vergleichenden studie , die 80 patienten einschloss , wurde die effektivitt der externen rt mit einer gesamtdosis von 14 , 4 gy ( gruppe a , n = 40 ) einer dosis mit 25 , 2 gy ( gruppe b , n = 40 ) gegenbergestellt . 
 schlussfolgerung : die externe rt der amd sowohl mit 14 , 4 gy als auch nach dosiserhhung mit 25 , 2 gy zeigte einen nur geringen positiven effekt nach 6 bzw . 
external radiotherapy in age - related macular degeneration introduction in 1929 , holloway & verhoeff were the first to report about loss of visual acuity in patients > 50 years of age that was due to degenerative changes of the retinal pigment epithelium [ 13 ]  . 
age - related macular degeneration ( amd ) manifests itself in many ways but is mainly categorized into two subgroups : the exudative form which is characterized by choroidal neovascularization ( cnv ) , and the atrophic or nonneovascular forapproximately 1020% of patients present with exudative amd caused by growth of new vessels from the choriocapillaris through breaks in bruchs membrane beneath the retina , overlying blood , exudates and pigmentary changes . cnv is usually accompanied by the ingrowth of scar tissue resulting in a disciform scar . 
untreated patients with the exudative form of amd can be expected to lose vision within 23 years . histopathologic factors concerning initiation and continuance of cnv in amd have been documented in the literature . 
several trials using external radiotherapy ( rt ) were started and up to now , a number of controversial results have been published [ 13 , 5 , 8 , 21 , 24 , 28 ]  . 
 in this prospective , nonrandomized , comparative study including 80 patients , the efficacy of external rt with a total dose of 14.4 gy ( group a , n = 40 ) and 25.2 gy ( group b , n = 40 ) was compared . 
 baseline evaluation all patients were referred from the department of ophthalmology , karl franzens university , graz , austria , after full ophthalmologic assessment including visual acuity testing , fundus photography , contrast sensitivity , and fluorescein angiography . 
 eligibility criteria : 60 years of age , classic or occult form of amd including drusen and characteristic retinal pigment epithelium changes , cnv lesions that were unsuitable for laser photocoagulation , a best - corrected visual acuity not worse than 20 / 200 , cnv lesions that were subfoveal and less than twelve disk areas in size , symptoms of < 4 weeks duration . 
 exclusion criteria : additional eye disease compromising visual acuity , any concurrent retinal disease ( angioid streaks , multifocal choroiditis ) , a history of any dry eye disorder , pretreatment head and neck irradiation , diabetes , hypertension , any treatment for malignancy , systemic corticosteroid treatment within 4 weeks before enrollment , any anticoagulants other than aspir patients characteristics a total of 80 patients ( 63 female , 17 male ) were recruited . 
 group a : mean age was 74 years ( range : 6183 years )  . eight patients presented with the classic and 32 with the occult form of cnv ( table 1 )  . 
five patients had classic and 35 occult cnv ( table 1 )  . all patients were adequately informed by physicians experienced in ocular rt and gave written informed consent [ 20 , table 1 . 
 during the treatment period , a portal film was taken weekly and verified by the radiation oncologist using the previous simulation fil follow - up all patients underwent regular follow - up at the departments of radiotherapy and ophthalmology . 
at each visit , complete ophthalmologic investigation , including fluorescein and indocyanine green angiography , was performed . changes in visual acuity , morphological characteristics of the disciform lesion and central visual field as well as possible radiation side effects like cataract or retinopathy were evaluated . 
due to the advanced age of our patients with an increased risk of intercurrent illness and death as well as lack of compliance in some cases , only 46 out of 80 patients could be followed over a minimum period of 48 months ( maximum 78 months )  . 
among 25 patients who could be observed after 48 months , 22 ( 88% ) did deteriorate and only three ( 12% ) had no change in their vision ( figure 1 )  . 
at 48 months , data of 21 patients were available and showed a decrease in 20 ( 95.2% ) and maintenance in one ( 4.8% ; figure 2 )  . 
 subjective evaluation of patients reading vision differed in the way that after 6 months , patients stated an improvement in 14 ( 34% ) and 17 cases ( 42% ) , respectively . 
 transpupillary thermotherapy ( hyperthermia treatment ) as used for uveal melanomas was thought to succeed in occluding neovascular vessels as well as reducing late leakage and subretinal fluid [ 18 ]  . 
in contrast to laser treatment , the effects produced by coagulation should be spared ; nevertheless , it is a treatment option for a subgroup of patients with occult lesions . 
 in a prospective study of gamma knife radiosurgery , investigators have demonstrated the effectiveness of a margin dose of 10 gy in reducing visual loss in patients with classic subfoveal cnv , but they could not see any beneficial influence on growth control of the neovascular complex [ 10 ]  . 
 more recently , intravitreal injections of an antivascular endothelial growth factor , which acts as an antipermeability and antiangiogenic agent , seem to be a promising new avenue for cnv [ 6 ]  . 
 macular translocation as well as macular rotation are surgical options which succeeded in restoring reading vision [ 4 ]  . however , there are still problems with postoperative complications like disorientation caused by diplopia and cyclotropia . although the use of roentgen therapy had been extended for retinal diseases by guyton & reese > 50 years ago , it was in 1993 when chakravarthy et al . 
published a study in which they determined whether low - dose irradiation ( 10 or 15 gy in five fractions ) could influence the natural course of amd according to data concerning irradiation of ocular choroidal hemangiomas [ 3 , 9 ]  . 
suggested that externalbeam irradiation with 16 gy slows down visual loss for only a few months , but patients reading vision could not be saved in the long run [ 24 ]  . 
reported that low - dose fractionated rt with 16 gy was well tolerated , vision and reading ability , however , were not preserved in most patients [ 8 ]  . 
another german study of 27 patients concluded that rt with a total dose of 20 gy failed to control growth in membrane size both in classic and occult cnv [ 5 ]  . 
 strahlentherapie und onkologie original article impaired quality of life in patients commencing radiotherapy for cancer monika janda1 , 2 , beth newman2 , andreas obermair3 , hedwig woelfl1 , michael trimmel4 , heidi schroeckmayr1 , joachim widder1 , richard poetter1 background : this study tested a three - item questionnaire to measure global quality of life ( qol ) and pain in patients commencing radiotherapy , based on items from the european organization for research and treatment of cancer ( eortc ) qlq - c30 instrument . 
 conclusion : this brief questionnaire addresses important aspects of qol , is feasible to use in a clinical setting and therefore represents a potentially useful tool for detecting those patients who may benefit from further evaluation and / or psychosocial support . 
 key words : cancer radiotherapy quality of life screening psychosocial support strahlenther onkol 2004 ; 180 : 7883 doi 10.1007 / s00066 - 004 - 1160 - 2 prvalenz reduzierter lebensqualitt zu beginn der strahlentherapie hintergrund : im rahmen dieser studie wurde ein kurzfragebogen zur erfassung der lebensqualitt , basierend auf dem lebensqualittsfragebogen der european organization for research and treatment of cancer ( eortc ) qlq - c30 , entwickelt . 
patienten mit niedriger lebensqualitt waren < 60 jahre und erhielten berdurchschnittlich hufig eine behandlung wegen eines bronchialkarzinoms , kolorektalen karzinoms , kopf - hals - tumors oder in palliativer absicht ( tabelle 2 )  . 
die in der vorliegenden stichprobe gemessenen lebensqualittswerte wurden des weiteren mit normen , welche fr die deutsche bevlkerung fr den eortc - qlq - c30 vorliegen , verglichen ( abbildungen 1a und 1b )  . 
 schlussfolgerung : der hier prsentierte kurze lebensqualittsfragebogen misst wichtige aspekte der lebensqualitt , ist auch in der arbeitsreichen atmosphre einer tagesklinik anwendbar und knnte sich daher als wichtiges screeninginstrument der lebensqualitt fr die strahlentherapie erweisen . 
patienten mit schlechter lebensqualitt zu beginn der bestrahlung knnten in besonderem ausma von zustzlicher betreuung und / oder information profitieren . schlsselwrter : krebs strahlentherapie lebensqualitt screening psychosoziale untersttzung 1 department of radiotherapy and radiobiology , medical school , university of vienna , general hospital , vienna , austria , 2 school of public health , queensland university of technology , brisbane , australia , 3 queensland centre for gynaecological cancer , royal womens hospital , herston , australia , 4 department of environmental psychology and experimental medical psychology , institute of environmental hygiene , university of vienna , vienna , austria . 
quality of life ( qol ) is affected by the diagnosis itself [ 22 ] as well as the diagnostic procedures , and often deteriorates further due to treatment - related side effects [ 7 , 14 ]  . 
in a recent meta - analysis , psychological interventions appeared to be more effective if patients were selected for therapy rather than if they were just included on the basis of their cancer diagnosis [ 26 ]  . 
early psychological treatment might be especially important for patients undergoing radiotherapy [ 32 ] , because patients are distressed before commencement of radiotherapy [ 13 ] and throughout treatment [ 25 ] , and early intervention is effective in reducing patient distress [ 20 ]  . 
 previous reports indicate that qol measures might carry independent prognostic information [ 2 , 3 , 6 , 28 ] , but others could not confirm these results and found only pain to be predictive of the outcome of lung cancer patients [ 10 ]  . 
single - item scales like the spitzer uniscale were compared with other qol tools and were shown to be equally sensitive and prognostically relevant as the more time - consuming methods [ 28 ]  . 
it was then the aim of this study to test the feasibility of using the three - item questionnaire in an unselected group of patients commencing radiotherapy and to compare our results to those available in the literature [ 11 , 16 , 18 , 23 , 31 ]  . 
 patients and methods patients all patients who were referred to the new patient clinic of the radiotherapy department of the university hospital , medical school of vienna , austria , between august 1998 and november 1999 were considered for this trial . 
eligible patients had to meet the following criteria : histologically proven malignancy , age > 18 years , first contact with our department , prior to receiving first radiotherapy treatment , not requiring constant hospital care , and able to understand german well enough to answer the questions . 
group 1 consisted of patients with breast cancer ( breast ) , group 2 comprised women with gynecologic cancer and patients with urogenital cancer ( gu / gyn )  . 
to allow comparison with normative data , a score for global qol was computed by combining oqol and opc and linearly transforming the resulting summary score to a 0100 scale with higher scores representing better global qol [ 1 ]  . 
this score was also transformed to a 0100 scale , with higher scores representing higher levels of pain the absence of an established cutoff level for impaired qol , patients with a score of 1 or 2 in at least one of the three items were classified as impaired qol . 
 data analysis ( cid : 1 ) 2 - tests were conducted to compare patients characteristics with satisfactory and impaired qol status ( impaired qol was defined by a raw score of 2 in at least one of the three questionnaire items )  . 
to investigate the independent influence of sex , age , and treatment subgroup on global qol and pain , multivariate logistic regression analyses were performed . variables were collapsed using reference coding to detect those characteristics independently associated with impaired qol . 
when compared to patients with satisfactory qol , patients with impaired qol were significantly more likely to be of younger age ( 17% of those 1829 years compared to 10.3% of those 70 years reported impaired qol )  . 
the patient groups with the highest proportion of reporting impaired qol was treated for advanced cancer ( 31.4% ) or cancer of the lung / gi / h&n ( 17.7% with impaired qol ; table 2 )  . 
as expected , cancer patients , on average , report lower global qol and higher pain than the general population ; however , for both men and women , there is a noteworthy crossover at older ages , and cancer patients actually report higher global qol and lower pain on average . 
for evaluation of treatment subgroup adjusted for age and sex , patients treated for lung / gi / h&n were selected as a reference group , since men and women are equally represented in this treatment subgroup . 
research , largely in the context of chemotherapy , indicates that patients with impaired qol are not only more likely to experience marked side effects during treatment [ 33 ] , but that qol furthermore provides independent prognostic information [ 2 , 3 , 6 , 16 , 28 ]  . 
an ideal screening test for qol should be inexpensive , easy to administer , present results to the medical staff immediately and impose minimal inconvenience to the patient , while covering relevant aspects of the patients experience [ 9 , 24 ]  . 
 in the present study , we report on the feasibility and usefulness of a very short screening instrument consisting of only three questions on qol and pain based on the eortc qlqc30 questionnaire . 
characteristics of patients ( n = 1 , 837 ) and multivariate logistic regression analysis of factors predicting impaired quality of life ( qol )  . ci : confidence interval ; for other abbreviations see table 1 . 
impaired quality of life in radiotherapy patients global qol score in german population global qol score in present austrian study / cancer patients pain score in german population pain score in present austrian study / cancer patients < 29 3039 4049 5059 6069 70 < 29 3039 4049 5059 6069 70 age ( years ) age ( years ) figure 1a abbildung 1a figure 1b abbildung 1b figures 1a and 1b . 
mean global quality of life ( qol ) scores ( higher scores representing higher qol ) and pain scores ( higher scores representing more pain ; general german population data compared to data obtained within the present austrian study ) in men ( a ) and women ( b )  . 
mittlere globale lebensqualitts - ( qol - ) werte ( hhere were entsprechen besserer lebensqualitt ) und schmerzwerte ( hhere werte entsprechen strkeren schmerzen ; normwerte der deutschen allgemeinbevlkerung im vergleich mit werten gemessen in der vorliegenden untersuchung ) bei mnnern ( a ) und frauen ( b )  . 
overall , the incidence of impaired qol by this definition was almost 14% , which compares favorably with previous studies carried out using more time - consuming methods [ 12 , 21 , 29 ]  . 
the utility of these three questions as a screening tool is evident from the mean global qol score of 32.6 for patients identified as having impaired qol , which is significantly lower than the 72.4 among patients reporting satisfactory qol . 
women aged 1829 reported a global qol score of 64.2 in our study compared to 78.9 in the general population , a reduction of 14.7 points and representing lower qol levels than seen for men . 
pain scores in these younger groups were considerably higher ( representing more pain ) than in the general population ( e.g. , male cancer patients aged 1829 reported a pain score of 23.6 , compared to 3.7 in the general population pain )  . 
however , pain scores in the older groups of cancer patients were somewhat lower than in the general population ( e.g. , women aged 6069 reporting a mean score of 22.6 , compared to 23.9 for the general population )  . 
as fayers points out , the expectation with which people are comparing their actual qol might be an explanation for the relatively low qol scores found in the older general population [ 5 ] compared to the cancer patients in the present study . 
men were more likely to report impaired qol in unadjusted analysis ; however , there was no significant difference in qol between men and women in the adjusted multivariate analysis . 
 looking at the results of the multivariate modeling reveals that those patients treated for lung / gi / h&n cancer , or for advanced cancer were more likely to report worse qol prior to commencing radiotherapy compared to other patients . 
however , as an aid to clinical practice , this three - item questionnaire offers a useful way to identify patients who may be referred for specialist , psychosocial support [ 4 ]  . 
bart1 , chris zurcher1 , 3 , jan wondergem1 background and purpose : von willebrand factor ( vwf ) , a glycoprotein involved in blood coagulation , is synthesized by endothelial cells . 
increased amounts of vwf in blood plasma or tissue samples are indicative of damaged endotheliuin the present study , mrna expression and localization of vwf were determined in irradiated rat heart tissue . material and methods : sprague - dawley rats received local heart irradiation with a single dose of 0 , 15 , or 20 gy . 
at mrna level , no changes in vwf could be observed at all time points after irradiation , suggesting that vwf deposition was not due to increased biosynthesis of the protein sections of amifostine - treated rat hearts , vwf staining was increased to a lesser extent . 
these increases in vwf accumulation precede development of fibrosis in the subendocardial layer and myocardium of the left ventricles , right ventricles , and atria . key words : ionizing radiation rat heart von willebrand factor fibrosis amifostine strahlenther onkol 2004 ; 180 : 10916 doi 10.1007 / s00066 - 004 - 1138 - 0 erhhte einlagerung des von - willebrand - faktors in rattenherzen nach lokaler ionisierender bestrahlung hintergrund und ziel : das glykoprotein von - willebrand - faktor ( vwf ) spielt eine wichtige rolle bei der blutgerinnung und wird durch endothelzellen synthetisiert . 
erhhte vwf - konzentrationen im blutplasma oder in gewebeproben weisen auf geschdigtes endothel hin der hier vorgestellten studie werden die mrna - expression und vwf - lokalisation im gewebe bestrahlter rattenherzen bestimmt . material und methodik : sprague - dawley - ratten erhielten eine lokale bestrahlung des herzens mit einer dosis von 0 , 15 oder 20 gy . 
nach zeitrumen von 3 monaten lie sich auch eine frbung der extrazellulren matrix ( ecm ) innerhalb fibrotischer bereiche beobachten . bezglich des mrna - levels konnten unabhngig vom zeitpunkt der untersuchung nach der bestrahlung keine vernderungen fr den vwf festgestellt werden . 
 schlussfolgerung : die von der strahlendosis und zeit abhngige zunahme der vwf - einlagerung deutet auf das vorliegen von geschdigtem endothel in den bestrahlten rattenherzen hdie zunahme der vwf - akkumulation geht der fibrosierung in der subendokardschicht und im myokard der linken und rechten ventrikel sowie im atrium voraus . 
 schlsselwrter : ionisierende strahlung ratte herz von - willebrand - faktor fibrose amifostin 1 department of clinical oncology ( k1 - p ) , leiden university medical center , the netherlands , 2 department of experimental therapy ( h6 ) , netherlands cancer institute , amsterdam , the netherlands , 3 department of pathology , faculty of veterinary medicine , university of utrecht , the netherlands . 
increased von willebrand factor in irradiated rat hearts introduction radiotherapy for treatment of breast cancer or hodgkins disease , as well as total body irradiation , may induce damage to the heart tissue , which , in the long term , results in cardiac complications for the patient [ 6 , 8 , 29 , 34 ]  . 
radiation - induced damage of endothelial cells may lead to a cascade of changes in blood vessels , resulting in an impaired blood supply to the surrounding tissue [ 3 , 10 ]  . 
in several heart studies , elevated expression of vwf in tissue specimens was suggested to be a marker of endothelial cell damage during allograft rejection [ 9 , 35 ] and other cardiac diseases , amongst which were aortic valvular disease and coronary artery disease [ 7 ]  . 
in a previous study , radiation - induced functional impairment and development of fibrosis were shown to be less severe after treatment of rats with amifostine ( ethyol ) [ 19 ] , a compound that has radioprotective effects [ 17 , 36 ]  . 
the animals were housed two per cage in a temperature - controlled room with a 12 - h light - dark cycle . food and water were provided ad libituthe irradiation procedure was performed as described by wondergem et al . 
local heart irradiation with a single dose of 0 , 15 , or 20 gy was performed , using an rt250 x - ray generator operated at 250 kv and 15 ma , with a dose rate of 1.95 gy / mrats were irradiated individually using plan - parallel opposed fields ( anterior - posterior 1 : 1 )  . 
the 15 - gy group consisted of 32 rats , the 20 - gy group comprised 33 rats , and 26 rats were nonirradiated controls . the experiments were performed with permission of the local committee on animal experiments , installed by the university of leiden according to the dutch law . 
 surgical procedure at seven different time points after irradiation ( 1 day to 16 months ) , three to five animals per radiation dose or control treatment were anesthetized by inhalation of fluothane ( inn : halothane ) ( astrazeneca , zoetermeer , the netherlands )  . 
 histopathology to determine total collagen accumulation , 5 - m sections were deparaffinized and subsequently incubated in phosphomolybdic acid ( 10 g / l ) for 5 min , in sirius red ( 5 g / l in a 1.2% picric acid solution ) for 90 min , and in 0.01 n hcl for 2 min , as described by junqueira et al . 
 immunohistochemistry after perfusion , hearts were incubated overnight in ethanol , 2% acetic acid ( or methanol - carnoys , in the amifostine experiment ) and embedded in paraffserial longitudinal sections ( 5 m ) were deparaffinized , and endogenous peroxidases were blocked with 1% h2o2 in methanol for 30 min at room temperature . 
nonspecific binding sides were blocked by a 10% bsa solution , and sections were incubated overnight at 5 c with a polyclonal rabbit anti - vwf antibody ( dako , glostrup , denmark ) 1 : 500 in 1% bsa in pbs , or a monoclonal anti - rat endothelial cell antigen antibody ( reca - 1 , monosan , uden , the netherlands ) 1 : 100 in 1% bsa in pbs . 
after washing , slides were incubated for 30 min at room temperature with a biotinylated swine anti - rabbit igg antibody ( dako ) 1 : 300 in 1% bsa in pbs , or a biotinylated horse anti - mouse igg antibody ( vector laboratories , burlingame , ca , usa ) 1 : 200 in 1% bsa in pbs and subsequently incubated with a streptavidin - biotin - peroxidase complex ( vector laboratories ) for 1 h . 
 after vwf staining , atria , left ventricles and right ventricles were divided in optical areas ( magnification 20 ( cid : 1 ) ) and each optical area was given a score as listed in table 1 . 
 rna isolation and pcr total rna was isolated from the left ventricles of irradiated and nonirradiated rats at different time points using rnazol b ( bioteck laboratories , houston , tx , usa )  . 
 pcr products were separated on a 1.5% agarose gel containing ethidium bromide and visualized by ultraviolet light . band intensities were determined by image quant software ( molecular dynamics , sunnyvale , ca , usa )  . 
 amifostine treatment to determine the effect of amifostine on vwf deposition , heart tissue specimens were used of a previous study on cardiac function and histopathology after irradiation in amifostinetreated rats [ 19 ]  . 
at 3 months after irradiation with a single dose of 15 or 20 gy , increased picrosirius red staining was observed in the epicardium , and at 6 months within the myocardium of the left ventricle , as compared to age - matched controls . 
fibrosis was first observed in the epicardial layer at 1 month after irradiation . fibrosis then developed in the myocardial layer at 6 months and , finally , in the subendocardial layer at 9 months . 
 immunohistochemistry in hearts from age - matched controls , all endocardial endothelium aligning the atrial and ventricular cavities , and the endothelial cells of approximately 80% of the coronary arteries were positively stained with the anti - vwf antibodies . 
3 months after irradiation , staining was observed within the extracellular matrix ( ecm ) of the myocardium , mainly in the left ventricle and often also in the subendocardial layer , near the cardiac valves or near the apex of the heart . 
staining for von willebrand factor ( vwf , a1 , b1 ) , endothelial antigen ( reca - 1 , a2 , b2 ) , and collagen ( picrosirius red , a3 , b3 ) in consecutive sections of left ventricles at 9 months after 20 gy . 
frbung auf von - willebrand - faktor ( vwf ) ( a1 , b1 ) , endothelantigen ( reca - 1 , a2 , b2 ) und kollagen ( picrosirius - rot , a3 , b3 ) in konsekutiven schnitten von linken ventrikeln 9 monate nach bestrahlung mit 20 gy . 
increased von willebrand factor in irradiated rat hearts 0 gy , n = 26 15 gy , n = 32 20 gy , n = 33 0 gy , n = 23 15 gy , n = 30 20 gy , n = 31 time after irradiation ( months ) time after irradiation ( months ) figure 2a abbildung 2a figure 2b abbildung 2b figures 2a to 2c . 
individual scores of von willebrand factor ( vwf ) staining in left ventricles ( a ) , right ventricles ( b ) , and atria ( c ) of rat hearts at different time points after irradiation with a single dose of 0 , 15 , or 20 gy . 
individuelle ergebnisse der von - willebrandfaktor - ( vwf - ) frbung in linken ventrikeln ( a ) , rechten ventrikeln ( b ) und atria ( c ) von rattenherzen zu verschiedenen zeitpunkten nach bestrahlung mit dosen von 0 , 15 oder 20 gy . 
in areas showing immunoreactive ecm , the number of capillaries was decreased , while remaining capillaries had a very irregular shape compared to nonirradiated myocardial capillaries ( reca - 1 staining )  . 
staining was absent in control preparations with pre - immune rabbit serum or a nonrelevant rabbit polyclonal antibody ( raised against the human camel protein ) , suggesting that in the vwf staining positive ecm was not a result of nonspecific binding of the polyclonal rabbit anti - vwf antibodies . 
 in order to quantify the presence of vwf in atria and left and right ventricles , immunoreactivity in the different cardiac regions was scored ( as described in the material and methods section )  . 
figures 2a to 2c show individual vwf scores for each animal and the mean of all animals in a radiation dose group . scores of nonirradiated animals did not exceed 1 , with one exception of an atrium at 6 months . 
although a variety was observed in individual scores of irradiated animals , mean scores of animals irradiated with 20 gy demonstrated an increase in vwf score from 3 months onward , and mean scores of animals irradiated with 15 gy showed an increase from 6 months onward . 
 vwf pcr to investigate if increases in vwf deposition in left ventricular tissue specimens coincided with increases in vwf gene expression , amounts of vwf mrna in left ventricle at different time points after irradiation were determined by pcr . 
amounts of von willebrand factor ( vwf ) mrna in pooled samples of three to five irradiated left ventricles sd over three independent pcrs , relative to time - related controls . 
menge an von - willebrand - faktor - ( vwf - ) mrna in proben von drei bis fnf bestrahlten linken ventrikeln sd , bestimmt in drei unabhngigen pcrs in relation zu zeitlich korrelierten kontrollproben . 
 vwf in amifostine - treated rat hearts a single dose of amifostine , administered prior to irradiation , led to a reduction of fibrotic lesions in the rat heart [ 19 ]  . 
in atria and left and right ventricles , at all radiation doses , vwf in amifostine - treated animals was lower than in irradiated animals without amifostine ( figures 3a to 3c )  . 
when combining all animals of the three radiation dose groups ( 15 gy , 20 gy and 22.5 gy ) , analysis of variance revealed that this difference was significant ( p < 0.05 ) in each of the three investigated cardiac regions . 
 with amifostine , n = 19 without amifostine , n = 22 without amifostine , fig 2 , n = 10 with amifostine , n = 19 without amifostine , n = 23 without amifostine , fig 2 , n = 10 22.5 radiation dose ( gy ) 22.5 radiation dose ( gy ) figure 3a abbildung 3a figure 3b abbildung 3b with amifostine , n = 18 without amifostine , n = 22 without amifostine , fig 2 , n = 10 figures 3a to 3c . 
individual scores of von willebrand factor ( vwf ) staining in left ventricles ( a ) , right ventricles ( b ) , and atria ( c ) of rat hearts , treated with or without amifostine , against radiation dose . 
individuelle ergebnisse der von - willebrandfaktor - ( vwf - ) frbung in linken ventrikeln ( a ) , rechten ventrikeln ( b ) und atria ( c ) von rattenherzen mit und ohne amifostinbehandlung gegen strahlendosen . 
increased von willebrand factor in irradiated rat hearts discussion in the present study , a timeand dose - dependent accumulation of vwf was shown in myocardial tissue after irradiation of the rat heart . 
this was due to the appearance of immunoreactive capillaries in irradiated left ventricles , right ventricles , and atria , starting at 1 month after irradiation , and deposition of vwf in ecm , mainly in left ventricles and atria , from 3 months onward . 
in the present study and in studies on silica - induced rat lung fibrosis and porcine serum - induced liver fibrosis , deposition of vwf was localized to fibrotic areas [ 14 , 31 ] , suggesting a role of vwf in the development of fibrosis . 
in the irradiated rat heart , a decrease in the number of capillaries ( as observed in former studies [ 30 ] and in the reca - 1 staining of the present study ) contributes to a decreased blood supply . 
the presence of vwf in the vascular subendothelial region may play a role in migration of fibromuscular cells [ 16 ] , a cell type which is associated with fibrosis . 
in these studies , increases in vwf deposition preceded the onset of functional renal impairment [ 37 ] or were limited to fibrotic areas in the lung [ 13 ]  . 
 to investigate whether increases in vwf deposition coincided with increases in vwf gene expression , amounts of vwf mrna in left ventricle tissue specimens were determined at different time points after irradiation . 
this is in accordance with studies on the irradiated kidney mentioned above , in which immunohistochemical increases in vwf were not associated with increased gene expression [ 21 ]  . 
in vivo , vwf , released to the luminal side , might be lost in the circulation , while release in the abluminal direction results in entrapment of vwf in the pericapillary and more remote ecm . 
together with the decreased vwf staining observed in the present study , these results suggest that amifostine has a radioprotective effect on the endothelium . moreover , the present data indicate that endothelial cell damage plays an important role in radiation - induced late cardiac damage . 
however , from this study it cannot be excluded that a radioprotective effect of amifostine on myocardial nonendothelial cells also contributes to the decrease in fibrosis and loss of cardiac function . 
berichtet wird ber mglichkeiten und chancen einer strahlentherapeutischen beteiligung an der weiterentwicklung dieses zukunftweisenden zweiges rztlichen , pflegerischen und psychosozialen handelns . material und methodik : erfahrungen aus der interdisziplinren zusammenarbeit zwischen palliativmedizin und strahlentherapie in deutschland werden dargestellt und entwicklungspotentiale diskutiert . ergebnisse : eine palliativeinheit kann effektiv nur interdisziplinr und interprofessionell arbeiten , d.h. 
zum einen machen die wirkungsweise , ap - plikationsart und effektivitt der radiotherapie sowie ein umfassender erfahrungsschatz in der betreuung von patienten mit fortgeschrittenen tumoren die strahlentherapie fr palliativeinheiten sehr attraktiv . 
zum anderen hat umgekehrt auch die strahlentherapie vorteile von den anderen fachgruppen der palliativeinheit zu erwarten . schlussfolgerung : bei einem wachsenden bedarf an palliativmedizinischer versorgung sollte sich der fachbereich der strahlentherapie aktiv an der entwicklung palliativmedizinischer einrichtungen in deutschland beteiligen . 
das ziel dieser beteiligung sollte es sein , in angemessenem rahmen die therapie unheilbar kranker menschen von seiten der strahlentherapie mitzugestalten und gleichzeitig die ganzheitliche versorgung der klassischen eigenen strahlentherapeutischen patienten zu verbessern . die weiterentwicklung der palliativmedizin in deutschland sollte vorangetrieben werden . 
 schlsselwrter : strahlentherapie palliativmedizin interdisziplinre zusammenarbeit strahlenther onkol 2004 ; 180 : 737 doi 10.1007 / s00066 - 004 - 1227 - 0 participation of radiotherapy in interdisciplinary palliative care units challenge and chance background : in germany , a sufficient system of palliative care does not exist . 
 results : a palliative care unit can only work in a team of different professions , which means different physicians , but also nurses , social workers , psychologists or pastors . 
this will meet the interests of palliative care and radiotherapy and most importantly the patients interests . key words : radiotherapy palliative care interdisciplinary work * beide autoren leisteten den gleichen beitrag . 
br. , 3 klinik fr strahlentherapie ( radioonkologie ) , universittsklinikum schleswig - holstein , campus kiel , 4 medizinische direktion , steiermrkische krankenanstaltenges.m.b.h. , graz , sterreich , 5 klinik fr strahlentherapie und radio - onkologie , marienhospital herne universittsklinik . 
interdisziplinre zusammenarbeit zwischen strahlentherapie und palliativmedizin einleitung nach der who - definition von 1990 ist palliativmedizin die angemessene medizinische versorgung von patienten mit einer nicht heilbaren , progredienten und weit fortgeschrittenen erkrankung bei begrenzter lebenserwartung , fr die das hauptziel der begleitung die lebensqualitt ist . 
 palliativmedizin ist kein neues fachgebiet , sondern im grunde die lteste form der medizin berhaupt , denn frher gab es bei nur wenigen erkrankungen einen kurativen behandlungsansatz [ 10 ]  . 
1997 wurde der anspruch auf eine angemessene palliativmedizinische versorgung schwerkranker und sterbender im sozialgesetzbuch v festgeschrieben ; 1998 wurden in den grundstzen zur sterbebegleitung palliativmedizinische manahmen als rztliche pflicht benannt . 
in europa gibt es neben internationalen ( european association for palliative care [ eapc ] ) und zahlreichen nationalen fachgesellschaften seit 1994 auch die deutsche gesellschaft fr palliativmedizin ( dgp )  . 
 palliativmedizin in der strahlentherapie wie cicely saunders , eine der begrnderinnen der englischen hospizbewegung , in einem rckblick schrieb , hatten u.a. ideen und entwicklungen der strahlentherapie wesentlichen einfluss auf die grndung des st . 
 wo knnten die grnde fr die zurckhaltung der strahlentherapeutischen kollegen bei der beteiligung an palliativmedizinischen einrichtungen liegen ? der wichtigste grund hierfr drfte eine im verhltnis zu anderen disziplinen relativ knappe personelle besetzung der bestehenden abteilungen fr strahlentherapie sein [ 7 ]  . 
ein weiterer grund fr die zurckhaltung knnte in der befrchtung liegen , mit einer palliativstation den schwerpunkt der abteilung wie bei einem hospiz von der therapie auf die sterbebegleitung zu verlagern . 
 palliativstationen und stationre hospize ein stationres hospiz ist ein betreuungsangebot fr schwer kranke und sterbende menschen mit hohem betreuungsaufwand , die nicht zu hause versorgt werden knnen , eine begrenzte lebenserwartung haben und keiner behandlung im akutkrankenhaus bedrfen . 
techniken der protonenbestrahlung oder der intensittsmodulierten radiotherapie fr noch mehr tumorpatienten verfgbar machen . dies bedeutet auch fr palliativ zu behandelnde patienten effektive therapiemglichkeiten mit weniger nebenwirkungen und somit besserer lebensqualitt . 
das fach verfgt ber gut ausgebildete rzte fr die beurteilung der gesamtsituation eines patienten , denn die indikationsstellung zu einer strahlentherapie und die therapieplanung erfordern viel umsicht und die beachtung vielschichtiger faktoren , welche den zustand des patienten und den verlauf der therapie beeinflussen . 
sie ist gezielt und sehr flexibel anwendbar , so dass auch dort , wo flexibilitt besonders wichtig ist , die therapien individuell an die bedrfnisse des patienten angepasst werden knnen , beispielsweise durch einfache vernderungen der fraktionierung und der dosis . 
da palliativstationen als zielsetzung die entlassung des patienten in seine husliche umgebung haben und die durchschnittliche liegezeit auf einer palliativstation nach erhebungen in nordrhein - westfalen nur 13 , 4 tage betrgt [ 11 ] , kann man solche stationen durchaus auch an ein onkologisches zentrum mit der mglichkeit zur strahlentherapie anbinden . 
da sich die strahlentherapie nicht ber ein organsystem definiert und mit fast allen anderen disziplinen der medizin kooperiert , knnen bereits bestehende strukturen durch eine palliativstation genutzt werden . vorteile der strahlentherapeutischen beteiligung an einer interdisziplinren palliativstation fr die strahlentherapie fr eine strahlentherapieabteilung ist eine palliativstation von groem wert . 
da die leitung der station in der regel interdisziplinr erfolgt oder die station zumindest ein enges netz von konsiliarrzten verknpft , wird fr die strahlentherapie spezialwissen aus anderen disziplinen sehr viel unkomplizierter und schneller verfgbar , was die qualitt der medizinischen versorgung auf den eigenen stationen zustzlich steigern kann . 
 eine palliativstation bietet fr die strahlentherapeutischen stationen ebenso wie fr alle anderen abteilungen des betreffenden krankenhauses die mglichkeit einer verlegung von patienten in einen bereich , der ber die notwendige strukturqualitt verfgt , um schwerstkranke patienten und deren angehrige adquat zu betreuen . 
 durch den besseren personalschlssel und das unmittelbare vorhandensein anderer berufsgruppen , wie physiotherapeuten , psychologen , seelsorger , sozialarbeiter und kunstoder musiktherapeuten , kann eine palliativstation auch die arbeit strahlentherapeutischer stationen und ambulanzen strahlenther onkol 2004 no . 
einstimmig ( ! ) wurde nicht nur die aufnahme der palliativmedizin in die ( muster - ) weiterbildungsordnung untersttzt , sondern auch nachhaltig der ausbau ambulanter und stationrer palliativmedizinischer versorgungsstrukturen gefordert . 
ber die bereits erfolgte aufnahme der palliativmedizin in die rztliche approbationsordnung im zuge der letzten novellierung im frhjahr 2002 hinaus forderte der deutsche rztetag einstimmig die aufnahme der palliativmedizin als querschnittsfach bzw . 
investitionen in die palliativmedizin zahlen sich nicht nur durch die verbesserte versorgung der patienten , sondern auch durch den gezielteren einsatz anderer ressourcen aus : ein bezglich des symptommanagements gut eingestellter palliativpatient bentigt weniger stationre einweisungen oder notfallversorgungen . 
 grundstze einhalten von aufnahmekriterien : patienten mit inkurablen fort geschrittenen erkrankungen und symptomen oder psychosozialen problemen , die einer krankenhausbehandlung bedrfen ganzheitlicher behandlungsansatz ziel : schmerztherapie und symptomkontrolle , psychosoziale betreuung von patienten und angehrigen verpflichtung zum interdisziplinren arbeiten personal krankenpflege : patient = 1 , 4 : 1 rztliche betreuung 24 h verfgbar sozialdienst , psychologischer dienst , seelsorge , physiotherapie raum gre : 812 betten mit entsprechenden funktionsrumen einund zweibettzimmer wohnliche gestaltung der gesamten rumlichkeiten wohnzimmer mit kochgelegenheit nach mglichkeit balkon oder terrasse bernachtungsmglichkeit fr angehrige strahlenther onkol 2004 no . 
interdisziplinre zusammenarbeit zwischen strahlentherapie und palliativmedizin groer teil der erbrachten leistungen im ops - katalog nicht erfasst , und es gibt derzeit keine mglichkeit , diese patientengruppe ber prozedurenmuster zu charakterisieren [ 16 ]  . 
diese beschrnken sich nicht nur auf die einzelnen fachbereiche der medizsie beziehen sich vor allem auch auf die zusammenarbeit mit anderen disziplinen wie der psychologie , der seelsorge , der sozialarbeit und natrlich auch der stationren und ambulanten pflege . 
2 urban & vogel strahlentherapie und onkologie original article development and evaluation of a skin organ model for the analysis of radiation effects viktor meineke1 , kerstin mller1 , roland ridi1 , nils cordes1 , frank - michael khn2 , artur mayerhofer3 , johannes ring2 , dirk van beuningen1 background and purpose : the reaction of tissues to ionizing radiation involves alterations in cell - cell and cell - matrix interactions mediated by cellular adhesion molecules . 
 material and methods : a human co - culture system consisting of the spontaneously immortalized keratinocyte cell line hacat and primary hdfa fibroblasts embedded into a collagen sponge was established . 
for that purpose , expression of ( cid : 1 ) 1 - integrin following irradiation was compared in the skin organ model and in hacat monolayer cells ( facscan and immunohistochemistry )  . 
a single dose of 5 gy x - irradiation induced an upregulation of ( cid : 1 ) 1 - integrin expression both in the skin organ model and in hacat cells . 
following irradiation , ( cid : 1 ) 1 - integrin immunoreactivity was intensified in the upper layers of the epidermis equivalent whereas it was almost absent in the deeper layers . 
 key words : ionizing radiation organ model skin ( cid : 1 ) 1 - integrin cellular adhesion molecules strahlenther onkol 2004 ; 180 : 1028 doi 10.1007 / s00066 - 004 - 1134 - 4 entwicklung und evaluierung eines hautorganmodells zur analyse von strahleneffekten hintergrund und ziel : die reaktion von gewebe auf ionisierende strahlung bewirkt nderungen in zell - zellund zell - matrix - interaktionen und wird durch zellulre adhsionsmolekle vermittelt . 
das ziel dieser studie bestand darin , ein geeignetes modell zur untersuchung kutaner strahlenreaktionen zu entwickeln und zu evaluieren . material und methodik : es wurde ein humanes kokultursystem etabliert , das aus der spontan immortalisierten keratinozytenzelllinie hacat und primren fibroblasten ( hdfa ) besteht , welche in einen speziellen kollagenschwamm eingebettet sind . 
hierzu wurde die expression von ( cid : 1 ) 1 - integrin nach ionisierender bestrahlung vergleichend im organmodell und an hacat - zellen untersucht ( facscan und immunhistochemie )  . 
des weiteren wurde der einfluss von ionisierender strahlung auf die dna - fragmentierung im organmodell analysiert ( tunel - assay )  . ergebnisse : das neue hautorganmodell zeigte charakteristika menschlicher haut , wie durch immunhistochemische frbungen von zytokeratin und ki - 67 sowie durch elektronenmikroskopische untersuchungen demonstriert werden konnte . 
sowohl im hautorganmodell als auch in hacat - zellen wurde die expression von ( cid : 1 ) 1 - integrin durch ionisierende strahlung ( 5 gy ) heraufreguliert . im hautorganmodell fanden sich darber hinaus nach bestrahlung umverteilungsphnomene des ( cid : 1 ) 1 - integrin - signals in die oberen schichten des epidermisquivalents . 
des weiteren konnte gezeigt werden , dass die bestrahlung einen deutlichen anstieg der dna - fragmentierung im hautorganmodell bewirkte . schlussfolgerung : die vorliegenden ergebnisse zeigen , dass das neue hautorganmodell gut geeignet ist , um zellulre strahleneffekte unter dreidimensionalen bedingungen zu analysieren . 
es knnen effekte untersucht werden , die sich in monolayerzellkulturen nicht darstellen lassen . schlsselwrter : ionisierende strahlung organmodell haut ( cid : 1 ) 1 - integrin zellulre adhsionsmolekle 1 institute of radiobiology of the german armed forces , munich , germany , 2 clinic of dermatology and allergology at biederstein , technical university of munich , germany , 3 anatomic institute , university of munich , germany . 
skin organ model for analysis of radiation effects introduction the molecular pathogenesis of the reaction of skin to ionizing radiation , also known as the cutaneous radiation syndrome , is still widely unknown [ 9 ]  . 
cams are transmembrane proteins , that are crucial for cell - cell and cell - matrix adhesion and involved in many cellular reactions and signaling events [ 4 ]  . 
one of particular importance is cd29 , the ( cid : 1 ) 1 - integrin subunit , which modulates cell - cell contact and interacts with extracellular matrix proteins such as fibronectin [ 7 , 18 ]  . in the skin , ( cid : 1 ) 1 - integrins ensure tissue integrity and regulate keratinocyte adhesion and differentiation [ 16 ]  . 
in the past , other skin models have been developed successfully for different purposes [ 10 , 1315 , 29 ]  . however , to our knowledge no organ model has been described for the study of radiation effects yet . 
it was not the objective of the present study to rebuild a complete human epidermis with all its special characteristics , but rather to get a three - dimensional test systethe second aim was to evaluate the suitability of this artificial skin organ model for the investigation of radiation effects . we started with the qualitative evaluation of parameters , which are known to be involved in radiation reactions , namely cell surface expression of adhesion molecules ( cams ) and dna damage . 
the data derived from flow cytometric analysis of ( cid : 1 ) 1 - integrin expression on hacat monolayer cell cultures were the basis to determine an appropriate time interval for immunohistochemical detection of ( cid : 1 ) 1 - integrin expression in the skin model . 
flow cytometric analysis of monolayer cells should demonstrate if there are any discrepancies between ( cid : 1 ) 1 - integrin expression in a monolayer cell culture and in a three - dimensional tissue culture . 
hacat and hdfa cells were cultured in dulbeccos modified eagles medium ( dmem , paa laboratories , linz , austria ) supplemented with 10% fetal bovine serum ( fbs , paa laboratories ) at 37 c in a humidified atmosphere with 10% co2 ; ph was maintained at 7.4. 
as recommended by the suppliers , 5 ( cid : 2 ) 105 cells were incubated with 5 l of an fitc - conjugated monoclonal cd29 ( ( cid : 1 ) 1 - integrin ) antibody ( dianova , hamburg , germany ) or an fitc - conjugated igg1 antibody ( serotec , kidlington , uk ) as an isotype control for 30 min on ice in the dark . 
after two final washings , flow cytometric analysis was performed using a bectondickinson facscan flow cytometer and cell quest software ( becton - dickinson , heidelberg , germany )  . 
the mean channel fluorescence ( mcf ) served as an indicator of the cell surface amount of ( cid : 1 ) 1 - integrmcf intensity distributions were plotted as relative expression of ( cid : 1 ) 1 - integrin as a function of time , and mcf of nonirradiated cells was defined as 100 . 
another decisive modification in our novel skin model was the growth of cells in a special freeze - dried collagen sponge matrix with a well - defined pore size of 10 m [ 26 ] which was a kind gift from the helmholtz institute for biomedical engineering . 
next , hacat cells ( 5 ( cid : 2 ) 105 cells / 0.5 ml medium ) were added on top of the sponge to build up an artificial epidermislike structure as a second layer . 
nach penetration des schwamms wurden 1 woche spter hacat - zellen auf die oberflche der gemischten kollagen - fibroblasten - matrix transferiert , um eine knstliche epidermishnliche struktur zu bilden . 
the basal ( cid : 1 ) 1 - integrin expression of nonirradiated hacat cells was defined as 100% and the ( cid : 1 ) 1 - integrin expression of irradiated hacat cells was normalized against it . 
 irradiation experiments hacat cells and the skin equivalent co - culture system were irradiated with 240 kv x - rays ( isovolt 320 / 10 , seifert , ahrensburg , germany ) filtered through 3 mm be with a focus to culture distance of 40 cthe dose rate was 1 gy / mthe dose used was 5 gy x - rays corresponding to the single dose applied in soft x - ray therapy for malignant skin diseases in the clinic of dermatology and allergy of the technical university of munich , germany . 
 immunohistochemistry for microscopic analysis , 7 - m cryosections ( leitz kryostat 1720 digital , bensheim , germany ) were mounted onto superfrost plus slides ( menzel - glser , braunschweig , germany ) , air - dried and rehydrated . 
sections were incubated with a primary antibody for ( cid : 1 ) 1 - integrin ( dako , hamburg , germany ) , ki - 67 antigen ( dako ) or cytokeratin ( polyvalent , detecting keratins 5 , 6 , 8 , 17 , dako ) for 60 min at room temperature followed by labeling with the apaap technique [ 5 ]  . 
the task of the study was to investigate qualitative changes of ( cid : 1 ) 1 - integrin expression in the whole epidermis equivalent following irradiation , irrespective of morphology . 
thin sections were viewed with a zeiss em10 . 1 - integrin expression results effect of ionizing radiation on ( cid : 1 ) of hacat cells we investigated whether ( cid : 1 ) 1 - integrin cell surface expression on hacat cells is altered by ionizing radiation . 
after reaching a maximum ( about 60% increase ) at 24 h following radiation , ( cid : 1 ) 1 - integrin expression declined without returning to basal levels at the end of the observed period of 48 h ( figure 2 )  . 
since a single dose of 5 gy caused a significant upregulation of ( cid : 1 ) 1 - integrin expression on hacat keratinocytes , the skin model was subjected to the same dose . 
immunohistochemistry was performed at 24 h after irradiation corresponding to the transient maximum of ( cid : 1 ) 1 - integrin expression observed in flow cytometric analysis of irradiated hacat cells . as demonstrated in figure 5a , an equal distribution of ( cid : 1 ) 1 - integrin throughout the whole epidermis equivalent was observed in the nonirradiated skin model . 
in the nonirradiated control skin model , only a few cells stained positive for dna damage ( labeling index 5.9% ) which corresponds to the normal process of cell differentiation of keratinocytes ( figure 6a )  . 
cell proliferation was demonstrated using the proliferation marker ki - 67 [ 21 ] and differentiation was shown by cytokeratin expression [ 24 ] and desmosomal cell contacts [ 23 ]  . 
as an example for its applicability , an upregulation of ( cid : 1 ) 1 - integrin expression after ionizing radiation as also observed in irradiated monolayer skin cells could be demonstrated implying its usefulness and potential for future strahlenther onkol 2004 no . 
skin organ model for analysis of radiation effects findings that keratinocytes with characteristics of stem cells show a higher ( cid : 1 ) 1 - integrin expression [ 12 ] may be transferred to our organ model . 
the noticed downregulation of ( cid : 1 ) 1 - integrin expression in the deeper layers of the epidermis equivalent after ionizing radiation may correspond to a radiation - induced inhibition of stem - cell - like keratinocytes . 
interestingly , the expression of ( cid : 1 ) 1 - integrin in the same monolayer cells , as demonstrated here and published elsewhere [ 17 ] , showed , overall , the same qualitative aspect of an upregulation by ionizing radiation . 
the effects observed in the novel skin model cannot be shown for monolayer cells alone and are strong arguments to investigate interactions between cells under three - dimensional co - culturing conditions . 
besides the functions listed above , ( cid : 1 ) 1 - integrins are known to be involved in the multistep process of transendothelial migration of leukocytes [ 31 ]  . 
there is evidence that blocking of ( cid : 1 ) 1 - integrins can inhibit migration of lymphocytes in inflamed lacrimal glands in nonirradiated tissue [ 20 ]  . 
 recently , it could be shown that apoptosis is an important parameter for the prognosis of cancer after radiation therapy figure 6a abbildung 6a figure 6b abbildung 6b figures 6a and 6b . 
 thus , organ models for the study of the radiation reaction of the skin might be a link between in vitro and in vivo experiments without the need for animal studies or human biopsies . skin organ cultures gained from skin biopsies also proved to be a useful tool to study the radiation reaction both after ionizing and uv irradiation [ 1 , 11 ]  . 
these split skin cultures show the advantage of a real three - dimensional structure and of interactions as in vivo skthe disadvantage , however , is a timely limited opportunity of culturing due to a reduced survival time of the explants . 
in addition , during preparation there is a traumatic disruption and damage to vital structures like blood vessels and the nervous system with effects hard to estimate . tissue engineering of a complete artificial skin organ model , by contrast , allows to study cellular interactions among monolayer cells under reproducible conditions . 
 in an initial set of experiments , we observed a radiationinduced upregulation of ( cid : 1 ) 1 - integrin expression in the novel three - dimensional skin organ model . 
our results , for the first time , show that these alterations of ( cid : 1 ) 1 - integrin expression levels are also detectable in a threedimensional human skin model . 
dna damage in irradiated cells ( tunel assay and electron microscopy ) observed using our novel organ model verifying apoptotic cells indicates that this model can be useful in estimating radiation response in a complex three - dimensional tissue - like syste up to now , no human skin organ model has been described for the evaluation of the effects of ionizing radiation . the present study , for the first time , provides such a model . initial experiments indicate its suitability and usefulness . 
 strahlentherapie und onkologie original article proton therapy for head and neck malignancies at tsukuba koichi tokuuye1 , yasuyuki akine1 , kenji kagei1 , masaharu hata1 , takayuki hashimoto1 , takashi mizumoto1 , yoshiko ohshiro1 , shinji sugahara1 , kiyoshi ohara1 , toshiyuki okumura2 , jun kusakari3 , hiroshi yoshida4 , fujio otsuka5 purpose : to evaluate the effectiveness and feasibility of proton therapy for head and neck cancers . 
 patients and methods : from 1983 to 2000 , 33 patients with head and neck malignancies but no history of surgical resection were treated with 250 - mev protons with or without x - ray irradiation . 
one ( 3% ) and six patients ( 18% ) suffered from treatment - related acute and late toxicity > grade 3 ( rtog / eortc acute and late radiation morbidity scoring criteria )  . 
 conclusion : proton therapy appeared to offer high local control rates with few toxicities relative to conventional radiotherapy . however , late toxicity was seen in areas where large radiation doses had been given . 
 key words : proton therapy head and neck carcinoma treatment - related toxicity strahlenther onkol 2004 ; 180 : 96101 doi 10.1007 / s00066 - 004 - 1132 - 6 protonentherapie bei kopf - hals - malignomen in tsukuba ziel : prfung der wirksamkeit und durchfhrbarkeit einer protonentherapie bei kopf - hals - malignomen . 
 patienten und methodik : von 1983 bis 2000 wurden 33 patienten mit kopf - hals - malignomen , aber ohne chirurgische vorbehandlung mit 250 - mev - protonen mit oder ohne rntgenstrahlung behandelt . 
die mediane gesamtdosis bei anwendung von protonen mit oder ohne rntgenstrahlung betrug 76 gy ( spanne 4299 gy ) , und die mediane protonenfraktionsdosis war 2 , 8 gy ( spanne 1 , 56 , 0 gy )  . ergebnisse : die fnf - jahres - berlebensund lokalkontrollraten betrugen 44% bzw . 
1 ( 3% ) und 6 ( 18 % ) patienten litten unter therapiebedingten akutund langzeitnebenwirkungen hher als grad 3 ( rtog / eortc - kriterien fr akutund langzeitstrahlennebenwirkungen )  . 
 schlsselwrter : protonentherapie kopf - hals - malignome therapiebedingte nebenwirkungen introduction primary therapy for head and neck malignancies generally involves either surgery or radiotherapy for early - stage tumors , extensive surgery combined with radiotherapy for more advanced but resectable tumors , and radiotherapy and / or chemotherapy for locally advanced tumors . 
the majority of these patients die of locoregionally persistent or recurrent disease , and only < 30% of them remain under control [ 14 , 1 department of radiation oncology , university of tsukuba hospital , tsukuba , japan , 2 department of radiology , central hospital of ibaraki prefecture , ibaraki , japan , 3 department of otolaryngology , university of tsukuba hospital , tsukuba , japan , 4 department of oral and maxillofacial surgery , university of tsukuba hospital , tsukuba , japan , 5 department of dermatology , university of tsukuba hospital , tsukuba , japan . 
some examples include intensity - modulated radiotherapy ( imrt ) [ 22 ] , conformal multisegmental field therapy [ 5 ] , and particle radiotherapy [ 11 , 17 , 18 ]  . 
these were patients who could not be treated otherwise due to advanced status of disease and / or recurrence after surgery , or to refusal of surgery because of expected postoperative disfigurement and / or dysfunction . 
only patients who had malignant tumors in the head and neck regions and who refused surgery before and / or after proton treatment or were inoperable were included in the study . 
ten of the 43 patients were excluded from this analysis : six received proton therapy postoperatively , three had proton irradiation preoperatively , and one discontinued treatment because of rapid deterioration in general status . 
 patient number age ( years ) sites pathology prior therapy female male male male male male male male male male female female male male female male male male male female male female male female male female male female male female female male female tongue tongue oral cavity parotid gland oral cavity parotid gland tongue oral cavity parotid gland oral cavity base of tongue hypopharynx oral cavity nasal cavity hypopharynx nasopharynx paranasal sinus nasopharynx middle ear paranasal sinus nasopharynx paranasal sinus nasal cavity nasopharynx paranasal sinus larynx parotid gland paranasal sinus paranasal sinus hypopharynx paranasal sinus nasal cavity paranasal sinus t3 n0 m0 t4 n0 m0 t1 n1 m1 recurrence t4 n2 mx t3 n0 m0 recurrence t3 n0 mx t3 n0 m0 t1 n0 mx t4 n0 m0 t2 n0 mx t2 n0 mx not applicable t2 n0 m0 t4 n0 m0 t4 n0 mx t4 n0 m0 not applicable recurrence t4 n2c m0 recurrence not applicable t4 n2c m0 t3 n0 m0 t4 n2c m0 t2a n0 m0 t4 n0 m0 t2 n0 m0 t2 n2c m0 t4 n0 m0 not applicable t4 n0 m0 squamous cell carcinoma squamous cell carcinoma adenocarcinoma squamous cell carcinoma anaplastic carcinoma squamous cell carcinoma mucoepidermoid carcinoma adenoid cystic carcinoma squamous cell carcinoma melanoma squamous cell carcinoma squamous cell carcinoma adenoid cystic carcinoma squamous cell carcinoma squamous cell carcinoma squamous cell carcinoma spindle cell carcinoma undifferentiated carcinoma squamous cell carcinoma epithelial - myoepithelial carcinoma spindle cell carcinoma squamous cell carcinoma adenoid cystic carcinoma squamous cell carcinoma squamous cell carcinoma squamous cell carcinoma epithelial - myoepithelial carcinoma melanoma squamous cell carcinoma none none none resection , rt cryotherapy , ctx cryotherapy , ctx none cryotherapy none cryotherapy none none resection resection none none none none none none none resection ctx strahlenther onkol 2004 no . 
proton therapy for head and neck malignancies 12 women , with a median age of 65 years ( range : 1783 years )  . patients characteristics are shown in table 1 . 
there were eight patients with paranasal tumors , four with nasopharyngeal tumors , and four with oral florid papillomatosis ( ofp ) classified as verrucous - type low - grade malignant lesions [ 8 ]  . the four ofp patients opted for proton therapy to avoid disfigurement after surgical resection . 
since the proton beams were shared with physics groups , the 250 - mev beams were available for medical use for 4 h / day , about 120 days / year . 
there were two treatment rooms , each supplied with a fixed vertical or a horizontal beam line with a maximum field size of 10 ( cid : 1 ) 10 cm2 at a dose rate of 2 gy / mthe proton therapy protocol was reviewed and approved by the institutional medical ethics committee . 
 prior to treatment planning , computed tomography ( ct ) studies were carried out to obtain 5 - mm transverse images of the patients head and neck region including the tumor immobilized by an individually manufactured thermoplastic mask . 
the treatments given are shown in table 2 . the rbe ( relative biological effectiveness ) value of 1.0 was used according to the data measured using fibrosarcoma nfsa cells [ 1 ]  . 
treatment - related toxicity was retrospectively categorized according to acute and late radiation morbidity scoring criteria described by the radiation therapy oncology group ( rtog ) [ 4 ]  . 
to compare the various treatment regimens employed , biologically effective doses ( bed ) were calculated using a linear - quadratic model with / ( cid : 2 ) ratios of 3 and 10 [ 6 ]  . 
the overall 2and 5 - year local control rates after treatment were 87% and 74% , respectively , the median survival time amounted to 49 months , and the 5 - year survival rates to 44% . 
median survival time and 5 - year survival rates were 44 months and 41% , respectively , and median progression - free survival time and 5 - year progression - free survival rates 28 months and 32% , respectively . 
the patient developed tongue ulcer necessitating tube feeding after completion of proton therapy ; this was followed by oral fistula formation at 28 months , bone necrosis and fistula formation at 8 years , and atrophic skin changes at 13 years . 
acute and late treatment - related toxicities were observed in seven patients ( 21% ) , resulting in 22.8% for both 3and 5 - year toxicity rates ; two patients had osteonecroses , four ulcerations in the irradiated area ( mucosa n = 3 , skin n = 1 ) , and one esophageal stenosis ( table 3 )  . 
no risk factor was found for late treatmentrelated toxicities such as osteonecrosis and fistula formation among performance status , age , treatment volume , history of surgical intervention and chemotherapy , and bed ( / ( cid : 2 ) = 3 and / ( cid : 2 ) = 10 ) values ( table 4 )  . out of 21 deaths , 15 ( 71% ) resulted from cancer progression : seven from distant metastases and eight from primary tumor extension . 
according to table 3 , there is a trend in which a bed ( / ( cid : 2 ) = 3 ) value > 130 is apparently associated with late toxicity , though it is not shown to be statistically significant . 
 discussion in the treatment of locally advanced head and neck cancer , increased locoregional control appears to be associated with improved survival , improved quality of life , and a reduction in the incidence of distant metastases [ 14 , 21 ]  . 
in our series which was limited to patients who did not undergo surgical resection , the overall local control rate was > 70% when relatively large proton doses were given with or without additional photon therapy . one and six patients suffered from acute and late treatmentrelated toxicities > grade 3 , respectively [ 4 ]  . 
the results are as follows : 2 - year overall and progression - free survival , and locorelocal control overall survival progression - free survival ( months ) figure 1 . 
 patient locally control number controlled ( c ) / period recurred ( r ) ( months ) treatment related toxicity time to toxicity ( months ) alive ( a ) / observation dead ( d ) period survival , and locoregional control rates without increasing the probability of late treatment - related toxicity . 
since our results seem quite comparable to the data shown above , we feel encouraged to continue the current treatment . recently , imrt has been found to offer better dose distributions than three - dimensional conformal radiotherapy [ 20 ]  . 
have described their clinical results on 35 patients with nasopharyngeal cancer treated with imrt [ 19 ]  . they achieved a 100% local control rate for a median followup period of 22 months and a 94% 4 - year overall survival rate after 6570 gy in 2.2 gy / fraction using imrt . 
have reported that proton therapy can deliver higher radiation doses with substantial dose reduction to the parotid gland , spinal cord , and brain stem in the treatment of nasopharyngeal carcinoma . 
 ( months ) ulceration osteonecrosis none ulceration , osteonecrosis ulceration none none none none ulceration none none none none none none none none none none none none none ulceration osteonecrosis none none none none esophageal stenosis none none none in a dose fractionation study , hayashi et al . 
33% of patients developed radiation - induced tongue ulcer . this high incidence of ulcer depended significantly on fraction size > 10 gy and 2 gy - equivalent total dose > 100 gy converted using an / ( cid : 2 ) ratio of 3 . 
have reported clinical results of 131 patients with early glottic carcinoma subjected to conventional daily fractionation of 2 gy compared to a hypofractionation scheme using a daily fraction size of 6 gy [ 9 ]  . 
high survival and low treatment - related toxicity rates were obtained in the conventional therapy group . according to lin et al . , proton radiotherapy is safe and effective in patients with recurrent nasopharyngeal carcinoma when a fraction dose of 1.82.0 is given [ 15 ]  . 
 acknowledgment this study was supported by a grant - in - aid for cancer research ( 1125 ) from the ministry of health , labor and welfare of the japanese government . 
 strahlentherapie und onkologie original article decreased local control following radiation therapy alone in early - stage glottic carcinoma with anterior commissure extension * abderrahim zouhair1 , david azria1 , philippe coucke1 , oscar matzinger1 , luc bron2 , raphael moeckli3 , huu - phuoc do3 , ren - olivier mirimanoff1 , mahmut ozsahin1 purpose : to assess the patterns of failure in the treatment of early - stage squamous cell carcinoma of the glottic larynx . 
 patients and methods : between 19832000 , 122 consecutive patients treated for early laryngeal cancer ( uicc t1n0 and t2n0 ) by radical radiation therapy ( rt ) were retrospectively studied . 
salvage treatment consisted of surgery in 17 patients ( one patient refused salvage and one was inoperable ; total laryngectomy in eleven , and partial laryngectomy or cordectomy in six patients )  . 
among the factors analyzed , multivariate analysis ( cox model ) demonstrated that anterior commissure extension , arytenoid protection , and male gender were the worst independent prognostic factors in terms of local control . 
 key words : glottic cancer radiotherapy surgery anterior commissure local relapse strahlenther onkol 2004 ; 180 : 8490 doi 10.1007 / s00066 - 004 - 1164 - y verminderte lokale kontrolle nach alleiniger strahlentherapie bei glottiskarzinom im frhstadium mit ausbreitung zur vorderen kommissur ziel : ergrndung der versagensmechanismen bei der therapie des larynxkarzinoms im frhstadiu patienten und methodik : zwischen 1983 und 2000 wurden 122 konsekutive patienten , die wegen eines larynxkarzinoms ( uicc t1n0 und t2n0 ) eine strahlentherapie erhielten , retrospektiv untersucht . 
es handelte sich um 68 patienten mit t1a - , 18 mit t1bund 36 mit t2 - tumoren . die diagnose wurde bei 104 patienten mit hilfe einer biopsie und bei 18 patienten mit laservaporisation oder stripping gestellt . bei 49 patienten ( 40% ) bestand die behandlungsplanung aus einer dreidimensionalen konformalen strahlentherapie , einschlielich neun patienten , die unter arytnoidprotektion bestrahlt wurden . 
sechs patienten starben an ihrem larynxkarzinoeine einseitige varianzanalyse zeigte , dass die ausbreitung auf die vordere kommissur , die arytnoidprotektion 1 department of radiation oncology , and 2 department of otorhinolaryngology , centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland , 3 institute of applied radiophysics ( ira ) , lausanne , switzerland . 
eine multivarianzanalyse ( cox - modell ) belegte , dass unter den bercksichtigten faktoren die ausbreitung auf die vordere kommissur , die protektion des aryknorpels und mnnliches geschlecht die schlechtesten unabhngigen prognosefaktoren im hinblick auf lokalrezidive sind . 
however , there is also substantial amount of literature indicating a very good local control when using rt alone in cases of anterior commissure infiltration [ 42 , 68 ]  . 
 in this retrospective single - center experience , we aimed at assessing the patterns of failure and prognostic factors , including anterior commissure extension and arytenoid protection in the treatment of early - stage squamous cell carcinoma of the glottic larynx . 
 patients and methods patients 122 patients with previously untreated t1n0 and t2n0 biopsy - proven squamous cell carcinoma of the glottic larynx , who were treated with rt alone at the centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland , between 1983 and 2000 , were included in this study . 
male - to - female ratio was 106 : 16 , and median age 62 years ( range : 3592 years )  . all patients underwent complete clinical examination and panendoscopy , and anterior commissure infiltration was always assessed , including the use of computed tomography ( ct )  . 
recent patients ( n = 15 ) received 70 gy in 6 weeks using a slightly accelerated schedule starting with a concomitant boost every friday from the beginning of treatment ( monday to thursday 2 gy / fraction / day ; 2 ( cid : 1 ) 2 gy on fridays )  . 
65 patients were treated with a 60co unit , and 57 with linear accelerators , either with 6 - mv photons ( n = 21 ) or 10to table 1 . 
 factor smoking alcohol dysphonia ( months ) t - classification histological differentiation localization anterior commissure extension group male female 612 > 12 well moderate poor glottic ( t1 ) glottic - supraglottic glottic - subglottic all 3 stages strahlenther onkol 2004 no . 
the typical borders for a t1 lesion would be the prevertebral fascia posteriorly , below the hyoid bone superiorly , below the cricoid cartilage inferiorly , and at the fall - off ( 12 cm ) anteriorly . 
t2n0 tumors were irradiated with ( n = 10 ) or without ( n = 12 ) elective nodal irradiation ( subdigastric and midjugular nodes ) , depending on the physicians decision . 
all patients were followed in a special head and neck consultation unit at chuv . the follow - up visits were repeated every other month during the first 2 years , every 6 months until the 5th year , and once a year thereafter . 
the events were death ( all causes of death included ) for overall survival , larynx cancer - related mortality for cause - specific survival , death ( including all causes of death ) or any relapse for disease - free survival , local recurrence for local control ( patients dying from any causes without local recurrence were censored ) , and metachronous second cancer for second cancer probability . 
differences between groups were assessed using the log - rank test [ 50 ]  . multivariate analyses were done using the cox stepwise - regression analysis to determine the independent contribution of each prognostic factor [ 11 ]  . 
 univariate analyses ( table 4 ) revealed that prognostic factors negatively influencing local control were anterior commissure extension ( figure 2 ) , arytenoid protection , and total rt dose < 66 gy . 
cancer - specific survival ( css ; ) , local control ( lc ; ) , and disease - free survival ( dfs ; ) in 122 patients with t1t2n0 glottic cancer treated with radiation therapy alone . 
tumorspezifische berlebensrate ( css ; ) , lokale kontrolle ( lc ; ) und krankheitsfreie berlebenszeit ( dfs ; ) bei 122 patienten mit t1t2n0 - glottistumoren , die nur mit strahlentherapie behandelt wurden . 
 site of failure in field in + out of field out of field extension , arytenoid protection , and male gender were the worst independent prognostic factors in terms of local control ( table 5 )  . 
total laryngectomy ( tl ) was realized in eleven patients , and partial laryngectomy ( pl ; n = 4 ) or cordectomy ( n = 2 ) in six . 
the ultimate larynx preservation rate was , therefore , 88% ( 107 out of 122 patients : eleven salvage tl , progression after salvage pl in one and cordectomy in one , and two refusing salvage surgery )  . 
the 5 - year local control rate , which was the same at 10 years , before and after salvage surgery amounted to 82% ( 95% ci , 7589 ) and 94% ( 95% ci , 9098 ) , respectively ( figure 3 )  . 
 number of 5 - year local control p - value local relapses ( % ) before salvage surgery according to the eortc / rtog late radiation morbidity scoring scheme [ 49 ] , there were six patients with grade 1 ( mild arytenoid edema ) , four with grade 2 ( moderate arytenoid edema ) , one with grade 3 ( severe edema ) , and three with grade 4 ( arytenoid necrosis ) laryngeal complications . 
the 5and 10 - year metachronous second cancer incidence was 11% ( 95% ci , 518 ) and 15% ( 95% ci , 721 ) , respectively . five patients developed non - small - cell lung cancer , four metachronous head and neck tumors including one patient with vocal cord sarcoma , two esophageal cancer , two prostate cancer , and one patient non - hodgkins lymphoma of the nasopharynx . 
 numerous reports regarding the treatment of early glottic cancer have evaluated a number of prognostic factors , i.e. , tumor volume and stage [ 20 , 28 , 37 ] , tumor kinetics including p53 status [ 3 , 13 , 48 ] , histological differentiation , intrinsic radiosensitivity [ 28 ] , smoking habits and hypoxia [ 9 ] , pretreatment hemoglobin level [ 14 , 59 , 69 ] , dose per fraction [ 70 ] , total dose [ 62 ] , overall treatment time [ 4 , 10 , 18 , 27 , 52 , 53 , 58 ] , field size [ 64 ] , beam energy [ 16 , 19 ] , radiation technique [ 61 ] , and anterior commissure involvement [ 41 , 51 ]  . 
 the majority of glottic cancers arises in the anterior part of the vocal cords , with relatively frequent involvement of the anterior commissure [ 44 ] ( table 6 )  . 
some investigators reported this to be associated with decreased local control following rt [ 29 , 60 , 71 ] , while others did not [ 5 , 16 , 42 ]  . 
in the present series , anterior commissure extension was found to be an independent prognostic factor in terms of local control , since we observed 16 relapses out of 61 patients with anterior months patients at risk according to salvage surgery after before 122 122 104 96 figure 3 . 
both rt and conservative surgery , i.e. , cordectomy , laser microsurgery or partial laryngectomy , seem to be equally effective modalities in terms of local control and survival [ 55 , 57 ] although not confirmed by any randomized comparison . 
 t - classification is a well - known prognostic factor in glottic cancer , and in all series , t1 tumors do better than t2 in terms of local control : at 5 years it ranges between 8095% for t1 , and 6080% for t2 [ 28 ]  . 
in order to ameliorate the local control in t2 tumors , either altered fractionation [ 22 , 26 , 31 ] or increased total dose [ 62 ] was proposed . 
 gender was reported by some to have an impact on local control , while others did not find it to be a significant factor [ 70 , 56 ] whether in glottic cancer or in other tumors of the head and neck region . 
 arytenoid protection is a potentially attractive technique to preserve the quality of the voice by decreasing the risk of laryngeal edema in the contralateral arytenoids , but only few data in the literature are concerning this particular point [ 1 , 6 , 15 , 40 ]  . 
 conclusion this study was a retrospective analysis performed in 122 consecutive patients with early glottic cancer treated with definitive rt , of which the major goal was to assess the importance of anterior commissure involvement as an independent prognostic factor . 
in case of anterior commissure extension , surgery , more aggressive irradiation including the use of altered fractionation , intensitymodulated rt , or innovative approaches such as concomitant radiochemotherapy should be explored . 
 material and methods : to form the actual vacuum mattress , the patient is pressed into the mattress with a vacuum foil which can also be used for daily repositioning and fixation . 
repositioning accuracy was determined by comparing daily , pretreatment , orthogonal portal images to the respective digitally reconstructed radiographs ( drrs ) in ten patients with abdominal and pelvic lesions receiving extracranial fractionated ( stereotactic ) radiotherapy . 
 key words : body fixation immobilization repositioning accuracy stereotactic radiotherapy strahlenther onkol 2004 ; 180 : 11722 doi 10.1007 / s00066 - 004 - 1146 - 0 reproduzierbarkeit der patientenpositionierung fr eine fraktionierte extrakranielle stereotaktische strahlentherapie unter verwendung einer doppelvakuumtechnik hintergrund und ziel : voraussetzung fr eine konformale fraktionierte strahlentherapie ist eine przise reproduzierbare positionierung des patienten und des zielvolumens . 
 ergebnisse : der mittelwert der fr alle patienten errechneten 3 - d - vektoren ( 187 fraktionen ) betrug 2 , 5 1 , 1 mder mit 10 mm grte 3 - d - vektor wurde bei einem in bauchlage bestrahlten patienten beobachtet . 
 schlsselwrter : krperfixation stereotaktische bestrahlung extrakranielle stereotaxie lagerungsgenauigkeit stereotaxie 1 department of radiotherapy - radiooncology , and 2 department of radiology 1 , stereotactic interventional planning laboratory , university hospital innsbruck , austria . 
double - vacuum fixation system in stereotactic radiotherapy introduction in extracranial stereotactic radiotherapy ( esrt ) , as in threedimensional ( 3 - d ) conformal radiotherapy , a precise method of repositioning and fixation is of paramount importance to ensure dose delivery and to keep the irradiated volume as small as possible . 
many positioning and fixation aids , mostly based on body masks [ 1 , 1114 ] and / or vacuum [ 6 , 10 , 21 , 22 ] or foam [ 5 , 16 , 18 , 19 ] mattresses are currently available and in use . 
 this study evaluates an extracranial stereotactic positioning system based on a double vacuum previously described , in principle , for angiography applications [ 3 , 4 ] and extracranial 3 - d navigated brachytherapy [ 20 ] in terms of its possible application for esrt . 
this vacuum can be adjusted between 40100 mbar . the fixation foil is inherently difficult to tear , so that , by pulling upward on this foil , the underlying vacuum mattress also gets pulled up and around the patient contours creating a deep and defined impression . 
at this point , the vacuum mattress can still be manually molded as desired , and special attention should be paid to heel and / or shoulder and head definition in the mattress as these are mainly responsible for craniocaudal positioning accuracy . 
 planning ct the mold can be created either directly preceding the planning ct or in a separate roothe planning ct protocol was 5 mm slice thickness acquired in spiral mode . 
the respective vacuum mattress ( available in various sizes and forms ) is reproducibly placed on this carbon table via the indexing syste then , the patient is positioned as desired and the vacuum conductor is placed over or beside the patient ( figure 2a )  . 
schematic representation of the double - vacuum technique ( 1 : vacuum mattress and its hose , connected to the vacuum pump ; 2 : the air between patient and fixation foil is evacuated , sandwiching the patient between the foil and mattress )  . 
schematische darstellung der doppelvakuumtechnik ( 1 : vakuummatratze und deren schlauch ; 2 : vakuumschlauch zur absaugung der luft zwischen patient und fixationsfolie , wodurch der patient fixiert und in seine matratze gepresst wird )  . 
x ( lateral ) and y ( anterior - posterior [ ap ] ) isocenter coordinates were calculated by measuring the distance from the beam axis to the centerrod of the stereotactic frame . 
then , the patient lies down in the mold . in this study , the fixation foil was used during the initial mold production process but not for the ensuing planning ct and daily fixation , but , depending , e.g. , on fractionation schedule and necessity of maximum fixation during treatment , the fixation foil could also be reused for repositioning of that specific patient ( for planning ct and treatments )  . 
in this case , after laying the patient down comfortably in the mold , the same vacuum conduction hose and foil are used to create the aforementioned sandwich , pressing the patient into the vacuum mattress with a pressure of up to 100 mb . 
 the stereotactic frame is ct / mri - compatible with arrowshaped hoses embedded in the anterior and lateral localizer plates ( figure 1 ) allowing the stereotactic isocenter coordinates to be calculated from the planning ct . 
prior to the initiation of radiotherapy , 10 ( cid : 1 ) 10 cm orthogonal digital portal images ( elekta iview - gt , amorphous silica detector ) were acquired on a daily basis and stored by the radiation therapists for retrospective evaluation . 
as with all patients , the orthogonal portals were viewed on a once - weekly basis by a physician . if corrections were made , only the original ( uncorrected ) images were included in this study . 
repositioning accuracy was retrospective - ly determined by comparing these with their respective drrs using the commercially available pipspro portal image processing system software package ( masthead imaging corporation , nanaimo , bc , canada ) which allows the user to compare two images by establishing the transformation necessary to orient them into perfect alignment . 
a chamfer transformation was calculated by determining variation of the anatomic structures relative to the field edge , whereby a set of orthogonal images provides the overall deviation of the patients setup in three axes . 
for these ten patients , the manufacturers claims regarding air tightness could be confirmed in that intermittent reevacuation under treatment was not necessary , even over an 8 - week treatment period . 
the additional time required compared to positioning by means of skin marks without positioning aid is so minimal that this system can also be used for conventionally fractionated therapy thus increasing confidence in patient setup and possibly allowing reduction of planning treatment volumes . 
for treatment volumes not fixated to bony structures and subject to organ movement , we recommend ct - based verification before initiating high - dose hypofractionated stereotactic treatment as do other groups using similar devices [ 22 ]  . all patients in this series , however , had appropriate ptv ( planning target volume ) margins to account for internal movement if required and received a conventionally fractionated treatment scheme , so orientation using bony landmarks as seen in the drrs was acceptable . 
 the learning curve became apparent by a clear decrease in sd with time ( table 1 ) , similar to a phenomenon observed by other groups analyzing extracranial positioning systems [ 5 , 12 ]  . 
 obviously , when treating volumes in motion , the repositioning accuracy values attained by such systems may well be smaller than the extent of expected organ movement under treatment [ 9 ]  . 
especially for tumors in the region of the liver and lower lung , it has been shown that organ motion can be significantly reduced by using an abdominal press [ 8 , 15 , 22 ]  . 
none of the patients in this series were candidates for an abdominal press but one was available for the body - fix ( figure 3 ) , and an evaluation is currently in progress at our institution . 
rigid fixation in the body region is especially important for transport between ct and treatment table , as transfer - induced changes of treatment position between ct and irradiation have been listed as a possibility of positioning errors in the craniocaudal ( z ) axis [ 21 ]  . also , rigid fixation is of utmost importance when performing stereotactic brachytherapy , not only in the head [ 2 ] , but also in the body regions [ 20 ]  . 
 when using the fixation foil only during the mold production process but not for daily treatments as in this study , we have found that repositioning times are comparable to those without positioning aid . 
it can be argued that this method is now comparable to nonstereotactic positioning aids such as foam mattresses [ 5 , 14 , 16 , 18 , 19 ] and thermoplastic mask materials [ 12 , 14 ]  . 
a similar study was performed by mitine et al . , except that a hemi - body foam mattress was used and the patients in the mask were in supine position . 
here , the mattress results were similar to those of the previous group , but the thermoplastic masks fared worse leading the authors to question the clinical feasibility of both systems [ 14 ]  . 
bauchpresse mittels eines individuell abgeformten vakuumkissens zur minimierung der zwerchfellbewegung . with regard to repositioning accuracy , our data as acquired for this study show that although repositioning results show a 95% ci of 4.7 mm , this is similar to other stereotactic body frames reported in literature . 
 the worst repositioning accuracy noted in the patient treated in prone position was possibly attributable to the patients slight obesity but also to the fact that the point of fixation / repositioning ( vacuum mattress ) was remote from the area to be treated ( paraspinal )  . 
this should be kept in mind for all treatments , since in times of multifield conformal therapy , skin dose and build - up effect are not as pronounced as when treating a supine patient through one dorsal field strahlenther onkol 2004 no . 
double - vacuum fixation system in stereotactic radiotherapy offered by the body - fix with its multitude of different - sized mattresses and the possibility of using it for both conventional 3 - d conformal as well as esrt indications . 
 conclusion the results of this study have shown that even when using the foil only for the vacuum mattress - forming process , daily setup time can be similar to using no positioning aid while offering very acceptable repositioning accuracy in most cases of fractionated conformal extracranial radiotherapy . 
with the increasing quality of modern portal imaging systems with integrated software for quick and on - line positioning assessment , we believe that once - weekly or even daily orthogonal verifications can be performed without significant time constraints . 
all patients with tumors in direct relation to bony structures undergoing hypofractionated irradiation at our institution , currently receive daily pretreatment orthogonal portal image verification , and corrections are applied on an individual basis depending on ptv margins . 
 acknowledgment the authors would like to express their sincere gratitude to the radiation therapists at the department of radiation oncology in innsbruck , for their patience , constructive criticism , and assistance in the clinical integration of this system . strahlentherapie und onkologie case study high - dose - rate interstitial brachytherapy for the treatment of penile carcinoma jir petera , karel odrzka , milan zouhar , jana bedrosov , martin dolezel1 background : interstitial low - dose - rate ( ldr ) brachytherapy allows conservative treatment of t1t2 penile carcinoma . 
highdose - rate ( hdr ) is often considered to be dangerous for interstitial implants because of a higher risk of complications , but numerous reports suggest that results may be comparable to ldr . 
 results : after 232 days from brachytherapy , the patient was without any evidence of the tumor , experienced no serious radiationinduced complications , and had a fully functional organ . 
 key words penile carcinoma interstitial high - dose brachytherapy strahlenther onkol 2004 ; 180 : 1235 doi 10.1007 / s00066 - 004 - 1124 - 6 interstitielle brachytherapie im high - dose - rate - ( hdr - ) verfahren zur behandlung des peniskarzinoms hintergrund : die interstitielle low - dose - rate - ( ldr - ) brachytherapie ermglicht eine konservative behandlung von peniskarzinomen im stadium t1t2 . 
die high - dose - rate - ( hdr - ) methode gilt in der praxis oft als gefhrlich fr die interstitielle brachytherapie , da ein hheres komplikationsrisiko befrchtet wird . 
zur interstitiellen hdr - brachytherapie des peniskarzinoms wurden bisher keine daten publiziert . fallbericht : berichtet wird ber einen 64 - jhrigen patienten mit einem plattenepithelkarzinom des penis t1 n0 m0 . 
die applizierte dosis betrug 18 ( cid : 1 ) 3 gy zweimal tglich . ergebnisse : der patient verblieb 232 tage nach der brachytherapie ohne tumor bei vllig funktionsfhigem organ , ohne dass schwere strahlenschden aufgetreten wren . 
consensus opinion from published reports on the management of localized carcinoma of the penis recommends that patients with small , distal , non - poorly differentiated lesions should be offered conserving treatment , while those with larger or more advanced lesions should be considered for amputation . 
all the published experience was based on the use of low - dose - rate ( ldr ) brachytherapy , and overall doses of 6070 gy were delivered in 67 days . 
 1 department of oncology and radiotherapy , charles university medical school and teaching hospital , hradec krlov , czech republic . received : november 22 , 2002 ; accepted : may 6 , 2003 strahlenther onkol 2004 no . 
interstitial hdr brachytherapy for penis carcinoma based largely on patient convenience , cost , machine availability and improved radiation safety , there is a strong move toward the use of high - dose - rate ( hdr ) afterloading devices for brachytherapy . 
due to the replacement of manual afterloading by the hdr device gammamed ( gammamed , mds nordion.gammamed , hahn , germany ) at our department , hdr interstitial brachytherapy had to be performed . 
 the dose distribution was calculated using the abacusgammamed planning syste step size of iridium source dwelling position was 5 mthe implanted volume covered by the 3 gy reference isodose was 9 cm3 . 
last follow - up on november 7 , 2002 ( 232 days from brachytherapy ) showed no evidence of the tumor and an inflammatory focus , 5 mm in diameter , close to the sulcus with bacterial infection ( both proven by cytologic examination )  . 
recently , several encouraging studies of hdr interstitial brachytherapy for head and neck tumors , prostate , breast cancer and even pancreatic carcinoma were published [ 2 , 3 , 5 , 7 , 9 , 10 ]  . 
in order to keep the overall treatment time comparable with the ldr course to prevent tumor repopulation , we used hyperfractionation , i.e. , two fractions per day at an interval of 6 h . 
according to the linear - quadratic model , 18 ( cid : 1 ) 3 gy in 14 days are equivalent to 66.77 gy to the tumor at a dose rate of 0.5 gy / h in 7 days , with a slightly higher effect on late tissues . 
interstitial hdr brachytherapy for penis carcinoma more experience and a longer follow - up are necessary to evaluate the role of hdr interstitial brachytherapy in the treatment of penile cancer . 
 strahlentherapie und onkologie original article extracapsular extension in positive axillary lymph nodes in female breast cancer patients patterns of failure and indications for postoperative locoregional irradiation heidi stranzl1 , ramona mayer1 , petra ofner2 , florentia peintinger3 , ulrike prettenhofer1 , arnulf hackl1 background and purpose : there has been little information regarding lymph node - positive breast cancer patients with extracapsular extension ( ece )  . 
the aim of this study was to evaluate the role of ece in predicting survival and relapse rates . patients and methods : from 19942002 , 1 , 078 lymph node - positive women with breast carcinoma were treated at our institution , whereas 301 patients ( 27.9% ) presented with ece . 
chemotherapy was administered to 69.8% , hormonal therapy to 53.2% , and combined systemic treatment to 26% of patients . results : the 1 - , 3 - , and 5 - year overall survival ( os ) was 98% , 84% , and 73% , the 1 - , 3 - , and 5 - year disease - free survival ( dfs ) 95% , 69% , and 58% , and the 1 - , 3 - , and 5 - year metastasis - free survival ( mfs ) 96% , 73% , and 60% . 
the relapse rates were 6.6% ( local ) , 0.3% ( supraclavicular ) , 0.7% ( isolated axillary ) , 1% ( local + axillary ) , and 0.7% ( local + supraclavicular ) , respectively . 81 patients ( 27% ) developed distant metastases . 
in december 2002 , 245 patients ( 81.4% ) were alive , 202 / 245 without progression , 32 / 245 with distant metastases , 5 / 245 with local / locoregional recurrence , and 6 / 245 patients with local and distant failure . 
 key words : breast cancer node - positive extracapsular extension relapse strahlenther onkol 2004 ; 180 : 317 doi 10.1007 / s00066 - 004 - 1170 - 0 positive axillre lymphknoten mit kapselperforation bei patientinnen mit mammakarzinorezidivmuster und indikation fr eine postoperative lokoregionre bestrahlung hintergrund und ziel : der stellenwert eines histologisch verifizierten lymphknoten - kapseldurchbruchs ( ece ) bei nodal positiven mammakarzinompatientinnen ist ungeklrt . 
 patienten und methodik : von 1994 bis 2002 wurden an unserer klinik 1 078 nodal positive patientinnen postoperativ bestrahlt . ein ece wurde bei 301 ( 27 , 9% ) patientinnen diagnostiziert . 
die anzahl der positiven axillren lymphknoten betrug ein bis drei ( 30 , 2% ) , vier bis sechs ( 27 , 9% ) , sieben bis neun ( 15 , 6% ) bzw . 
 ergebnisse : das 1 - , 3und 5 - jahres - gesamtberleben ( os ) lag bei 98% , 84% und 73% , das krankheitsfreie 1 - , 3und 5 - jahresberleben ( dfs ) bei 95% , 69% und 58% ( abbildung 1 ) und das metastasenfreie 1 - , 3und 5 - jahres - berleben ( mfs ) bei 96% , 73% und 60% ( tabelle 2 )  . 
folgende rezidivlokalisationen wurden beobachtet : lokal ( 6 , 6% ) , supraklavikulr ( 0 , 3% ) , isoliert axillr ( 0 , 7% ) , lokal + axillr ( 1% ) , lokal + supraklavikulr ( 0 , 7% ) ( tabelle 4 )  . 
im dezember 2002 lebten 245 patientinnen ( 81 , 4% ) , 202 / 245 ohne hinweis auf progression , 32 / 245 mit fernmetastasen , 5 / 245 mit einem lokalen bzw . 
 1 department of radiotherapy , university medical school , graz , austria , 2 department of medical informatics , statistics and documentation , university medical school , graz , austria . 3 division of gynecology , leoben , austria . received : march 10 , 2003 ; accepted : september 29 , 2003 strahlenther onkol 2004 no . 
randomized trials have demonstrated survival benefits for patients treated postoperatively with chemotherapy hormonal therapy followed by adjuvant radiotherapy compared with patients treated with adjuvant systemic therapy only [ 18 , 19 , 23 ]  . 
it has been extensively reviewed that there is no need for rni after adequate axillary dissection in the case of negative lymph nodes or with one to three pathologically involved nodes [ 9 , 11 , 2527 ]  . 
until recently , there has been little information [ 2 , 3 , 13 , 15 , 20 , 30 ] with regard to regional nodal failure ( rnf ) rates for lymph node - positive patients with extracapsular extension ( ece ) after adequate axillary surgery . 
the aim of our study was to evaluate the role of extranodal spread of tumor cells in predicting survival , local relapse and regional recurrence rates in lymph node - positive female breast cancer patients treated with irradiation with or without systemic therapy . patients and methods between july 1994 and december 2002 , 1 , 078 lymph nodepositive women with stage ii or iii breast carcinoma were treated at our single institution . 
 surgery all 301 patients underwent surgical treatment to the primary lesion , either modified radical mastectomy ( n = 141 ) or breastconserving therapy ( n = 160 )  . 
axillary lymph nodes were examined for the number of nodes removed , the number of nodes involved , and , regarding our special interest , for extracapsular extension ( table 1 )  . 
the remaining 210 patients ( 69.8% ) had four or more lymph nodes positive for metastases : 84 patients ( 27.9% ) had four to six involved nodes , 47 patients ( 15.6% ) seven to nine , and 79 patients ( 26.2% ) ten or more . 
regional nodal irradiation was considered if a minimum dose of 46 gy ( range : 4652 gy , median dose : 50 gy ) was given to the axillary apex and supraclavicular nodes to a depth of 35 cthe inferior border of this separate , third anterior field was matched with the upper border of the tangential fields and was half - beamblocked . 
no adjuvant systemic therapy was given to nine patients of the entire group . due to an estrogen receptor - negative tumor status in these patients , hormonal therapy was not considered appropriate . 
patients were routinely evaluated for tumor control in 3to 4 - month intervals in the first 3 years and in 6 - month intervals for the next 2 years . subsequently , these patients were observed on a yearly basis . procedures included a careful clinical examination , blood samples , routine chest radiographs , mammography / ultrasound , and abdominal ultrasound . 
statistical analysis of overall survival ( os ) , disease - specific survival ( dss ) , disease - free survival ( dfs ) , and metastasis - free survival ( mfs ) , as well as analysis of follow - up were performed using the kaplan - meier method . 
progressive disease ended in death in 36 cases ( 11.9% ) , 14 patients ( 4.7% ) expired of causes other than breast cancer , and six ( 2% ) died because of a second malignancy . 
the remaining 19 patients refused ( n = 10 ) rni , or rni was omitted ( n = 9 ) because of difficulties in patient arm positioning . these patients were treated with tangential irradiation alone . the rate of recurrence was as follows : local , 5.3% ( n = 16 ) ; supraclavicular fossa , 0.3% ( n = 1 ) ; local + supraclavicular fossa , 0.7% ( n = 2 ) ; local + axillary , 1% ( n = 3 ) ; isolated axillary , 0.7% ( n = 2 )  . 
the 5 - year dsf ( figure 1 ) was significantly reduced ( p = 0.04 ) in the subgroup with one to three positive nodes ( 69% ) versus the subgroup with four or more positive lymph nodes ( 54% )  . 
 treatment - related complications acute radiation treatment toxicity was generally minor , located in the skin and self - limiting ( maximum grade ii according to the eortc / rtog score )  . 
19 out of 23 patients ( 68% ) with lr and / or rnf subsequently developed distant metastases , 2 / 28 ( 7% ) developed a second malignancy in the contralateral breast and died , whereas only 7 / 28 patients ( 25% ) did not show any tumor progression with strahlenther onkol 2004 no . 
 second malignancy the rate of a second primary malignancy was 11.3% ( n = 34 )  . of the 34 patients , 22 ( 65% ) presented with contralateral breast carcinoma . 
in all named studies , the degree of nodal involvement ( one to three or four or more involved nodes ) varied substantially , reflecting a higher percentage of patients with four or more positive lymph nodes when ece was evident . 
we want to stress that there is a heterogeneity in therapy regimens as to whether patients were treated with surgical procedures as well as to the extent of postoperative irradiation , i.e. , local versus locoregional irradiation with three , four or five fields . 
recent data [ 15 , 20 , 30 ] have suggested that the presence of ece is not associated with an increased risk of axillary recurrence following adequate axillary dissection . 
 [ 7 ] proved ece to be an independent prognostic factor for both endpoints , with a 7% axillary recurrence rate for all patients as well as the ece - positive subgroup . 
 the median follow - up of our study population was restricted to 34 months , others [ 9 , 26 ] described the median time interval to isolated axillary failure to be < 23 months . 
the relation of ece and rate of axillary relapse after axillary surgery has been examined in some series [ 2 , 3 , 15 , 20 , 30 ]  . 
data have been published about the very low risk of isolated axillary recurrence in patients presenting with ece after complete dissection [ 3 , 13 , 17 , 20 , 30 ]  . 
currently , there are no sufficient data available to justify routine application of rni in patients ( one to three positive lymph nodes ) with an adequately dissected axilla , even in the presence of ece as shown by recent series [ 3 , 15 , 20 ] , which are similar to our observations . 
they have shown that the most important predictor of axillary relapse is the extent of axillary dissection and rni may solely have a role in case of axillary sampling . others [ 10 ] recommend rni for patients with ece and four strahlenther onkol 2004 no . 
our results ( n = 2 , 0.7% ) are consistent with prior studies [ 2 ] which have also demonstrated the low risk of developing an isolated axillary recurrence . 
for that reason , we suggest that axillary irradiation should not be given routinely to patients who underwent complete / full axillary dissection , even in the presence of ece . 
 optimal radiation treatment tangential postoperative radiation therapy to the breast / chest wall and lower axilla was typically used for treating patients who had one to three positive axillary nodes , as determined by axillary dissection , whereas a third radiation field ( supraclavicular ) was added for patients with four or more positive nodes . 
on the other hand , it could be argued that a substantial portion of the axillary region at risk for recurrence received a dose significantly below levels required for eradication of microscopic disease [ 8 ]  . previous studies [ 3 , 13 , 15 , 20 , 30 ] have reported on patients treated postoperatively with varying degrees of irradiation . the results of these studies and our data give reason to omit irradiation to an adequately dissected axilla for the sole indication of microscopic extracapsular tumor spread . 
in our study group , a significantly decreased 5 - year dfs was seen among patients with four or more positive lymph nodes and ece . although ece may adversely affect outcome , an increased axillary relapse rate is not mandatory if there is evidence of extranodal tumor spread [ 3 , 15 , 20 ]  . 
in our study , a third radiation field to the supraclavicular fossa was used in two out of three patients developing radiation pneumonitis . postoperative irradiation has the potential to cause late cardiac mortality in patients with left - sided cancers [ 5 ]  . 
that is why the amount of heart in the treatment field should be kept as low as possible , though relevant cardiovascular side effects are unlikely to occur [ 28 ]  . 
a recently published consensus statement advocates internal mammary node irradiation in carefully selected patients in the presence of defined tumor characteristics [ 27 ]  . careful chemotherapy treatment planning , particularly with doxorubicin - containing regimens , is useful in accomplishing this goal . 
 we would like to acknowledge the limitations of the study . since our report only addressed lymph node - positive patients with ece , we do not have data about a study group yet . therefore , it is difficult to base a recommendation for axillary treatment solely on the findings of this retrospective analysis , though the overall number of patients is substantial as compared to the literature . 
the benefit of irradiation must be based on the results of our study and other existing data , we conclude that isolated axillary nodal failure remains low in lymph node - positive patients with extranodal spread . 
therefore , we continue to recommend that an axillary radiation is not routinely indicated after complete axillary dissection . however , if there is concern about the completeness of strahlenther onkol 2004 no . 
additional studies on lymph node - positive breast cancer patients with a special focus on extranodal spread would be valuable to substantiate our conclusions and help to identify subgroups of patients who might benefit from axillary irradiation . 
 strahlentherapie und onkologie original article recurrent rectal cancer within the pelvis a multicenter analysis of 123 patients and recommendations for adjuvant radiotherapy stefan hcht1 , riad hammad1 , hans - joachim thiel2 , thomas wiegel1 , alessandra siegmann1 , jochen willner3 , peter wust4 , thomas herrmann5 , michael eble6 , michael flentje3 , detlef carstens7 , dirk bottke1 , patrick neumann8 , wolfgang hinkelbein1 background and purpose : recommendations for radiation ports in adjuvant radiation therapy for rectal cancer are mainly based on analysis of recurrence patterns . 
major inclusion criteria ( one sufficient ) for eligibility were : histological confirmation , clear bone destruction , and a positive pet scan , or at least three minor criteria : progressive soft tissue mass , invasion of adjacent organs on followup ct or mri , rising tumor markers , and typical appearance in cross - sectional imaging . 
when abdominoperineal resection was compared to low anterior resection as primary operation , there was a significant difference in extension of recurrent tumors in the inferior parts of the pelvis ( p < 0.025 in all statistical tests applied ) , whereas no significant difference was found in the superior parts of the pelvis . 
 conclusion : based on these results , a modest field size reduction in adjuvant radiotherapy for rectal cancer seems feasible , offering the perspective of a reduction in acute and late side effects . 
 key words : rectal cancer pelvic recurrence adjuvant therapy radiation ports strahlenther onkol 2004 ; 180 : 1520 doi 10.1007 / s00066 - 004 - 1130 - 8 pelvine rektumkarzinomrezidive . 
eine multicenteranalyse von 123 patienten und empfehlungen fr die feldwahl bei der adjuvanten bestrahlung hintergrund und ziel : die empfehlungen zur wahl der strahlenfelder bei der adjuvanten therapie des rektumkarzinoms basieren hauptschlich auf auswertungen der rezidivverteilungsmuster . 
georg , hamburg , germany , 8 institute for medical informatics , biometry , and epidemiology , university hospital benjamin franklin , free university of berlin , germany . received : december 2 , 2002 ; accepted : may 6 , 2003 strahlenther onkol 2004 no . 
beim vergleich von abdominoperinealer amputation mit tiefer anteriorer resektion zeigte sich ein signifikanter unterschied in der tumorausdehnung der rezidive nur in den kaudalen beckenanteilen ( p < 0 , 025 in allen angewendeten statistischen tests )  . schlussfolgerung : auf der basis der ergebnisse kann bei der adjuvanten radiotherapie eine moderate verringerung der feldgren empfohlen werden , die wahrscheinlich eine reduktion der rate an akuten und spten nebenwirkungen ermglichen wird . schlsselwrter : rektumkarzinom pelvines rezidiv adjuvante therapie strahlenfelder introduction the role of radiotherapy as adjuvant treatment after curative resection or given in a neoadjuvant setting prior to the operative procedure has a well - recognized role in reducing rates of locoregional tumor recurrence and , to some extent , thus contributes to improving rates of cancer - related mortality [ 4 , 5 ]  . based on the evidence of a clear survival benefit , postoperative radiochemotherapy in the early 1990s emerged as a standard of care in patients with stage ii and iii rectal cancer , since a positive impact on distant metastasis as well as local control could be demonstrated [ 7 , 17 , 25 , 26 ]  . 
at the time these studies were initiated , rates of local or regional tumor recurrence were fairly high and exceeding 20% in major surveys [ 15 ]  . therefore parallel to the evaluation of the benefit of adjuvant therapies , surgeons and pathologists sought for the anatomic and technical basis of tumor recurrence rates , and these investigations consecutively led to considerable improvements in operative maneuvers [ 10 , 11 , 19 , 28 ]  . 
 as these changes in operative therapy may not only influence rates of tumor recurrence in the pelvis but the pelvic pattern of recurrence itself , and recommendations for radiation ports in adjuvant therapy are largely based on rather outdated studies , a multicenter study was initiated to evaluate pelvic sites of recurrence on a large - scale multicenter basis of patients treated recently [ 9 , 27 ]  . 
 patients with clinical or serologic signs of inflammation or abscess formation were excluded , as it may be impossible to distinguish malignant from inflammatory soft tissue masses in these situations . 
 for graphic analysis of recurrence patterns and visualization of results , films were rendered out of the 3 - d database . extensive quality assurance tests were done while adjusting the bony pelvis model to the displayed recurrence patterns to achieve exact and anatomically correct representations of sites of recurrent tumors within the pelvis . 
synchrone metastasierung bei diagnose des tumorrezidivs . overall liver lungs lymph nodes paraaortic lymph nodes groin peritoneal cavity and abdominal wall bone brain uterus and vagina prostate and seminal vesicles bladder and urethra sacral and coccygeal bones sis of differences in recurrence patterns was facilitated by comparison on a sliceby - slice basis , thus reducing the amount of data to be handled . 
tests performed were pearson ( cid : 1 ) 2 - square test with continuity correction , likelihood ratio , fishers exact test , and linear - by - linear association . 
 results in 54% of the 123 patients lymph nodes were without metastatic deposits initially ( n0 ) , whereas n1 and n2 disease ( according to tnm - 5 ) was diagnosed in 23% each . 
initial surgical procedures were an abdominoperineal resection ( apr ) in 41% , low anterior resection ( lar ) in 36% , and others , namely variants of lar in 23% ( see table 1 for details )  . 
invasion in adjacent organs was a quite common event ( table 2 ) , and synchronous metastasis was diagnosed in 38% with the liver and lungs being the sites most often involved ( table 3 )  . 
adjuvant radiotherapy for rectal cancer the anatomic and technical basis of tumor recurrences within the pelvis has been extensively investigated over the past 2 decades by surgeons and pathologists and as a result of these attempts , major improvements in operative therapy have been implemented [ 10 , 11 , 19 , 28 ]  . 
in large multicenter randomized studies published within the last years , 5 - year locoregional recurrence rates decreased to a range of 618% with or without adjuvant or neoadjuvant radiotherapy [ 16 , 21 , 31 , 35 ]  . 
 although rates of pelvic recurrences in reality may be somewhat higher than estimated by these reports , as some studies report only first sites of failure and pelvic relapse in the later course of disease is not always assessed in patients under palliative chemotherapy for distant metastasis , there is no more clearcut evidence of a survival benefit attributable to the addition of radiotherapy to the treatment . 
given the fact that radiotherapy can cause severe and , in some instances , even fatal complications especially in elderly patients , there is an obvious need to redefine its role [ 5 , 8 , 14 , 29 ]  . 
 reducing side effects of radiotherapy therefore is one of the most important topics and modern 3 - d treatment planning systems and multiple - field techniques undoubtedly have enormous impact herein [ 20 ]  . 
many studies have demonstrated that the volume irradiated is a very critical factor influencing rates of acute as well as late complications , underlining the need to reduce the volume treated to an essential minimum [ 3 , 18 , 24 ]  . 
 modifications in operative therapy may not only influence rates but the pelvic pattern of recurrence itself ; therefore reevaluation of recommendations for radiation ports in adjuvant therapy should be based on recurrence patterns of patients treated recently . 
many of the studies reporting on pelvic recurrence patterns have some limitations ; they are either outdated or do not give exact anatomic information of the location of recurrent tumors within the pelvis or just simply cover a very large timespan within which changes in therapy very likely will have happened , thus compromising the ability to make their results a basis for recommendations in definition of planning target volumes in adjuvant radiotherapy [ 1 , 2 , 6 , 9 , 13 , 22 , 23 , 27 , 30 , 34 ]  . 
 graphic evaluation of the pelvic sites of recurrence in the 3 - d computer model at a first glance led to the conclusion that recurrent tumor may be situated anywhere within the pelvis . the volume involved shrunk considerably by excluding all sites involved just once . 
recurrence patterns were then analyzed in the subgroups of patients who had been previously treated by apr and lar . to limit differences mainly caused by chance , sites involved in < 10% were excluded for display purposes , as the subgroups were considerably smaller than the complete data set ( figures 2 and 3 )  . 
no difference in the three top ct slices of the pelvis was observed , whereas there was a statistically significant difference in the three lowest pelvic ct slices , with results of all of the aforementioned tests being p < 0.025 ( figure 4 )  . discussion pain and disabilities like fistula formation , severe neurologic deficits , compromised pelvic stability , bowel obstruction , etc . accompanied by tumor recurrences of rectal cancer within the pelvis have dramatic impacts on quality of life of afflicted patients . 
once the tumor has recurred , chances of cure are small even if extensive resections and multimodality treatment strategies are applied , and only patients with small tumors at the site of the anastomosis seem to fare somewhat better [ 30 , 32 , 33 , 36 ]  . 
adjuvant radiotherapy for rectal cancer the multicenter basis of data evaluated makes it unlikely that results are influenced by regional specialities or individual preferences of one surgeon or team of surgeons . 
still , there are some shortcomings in our study , as cts were mainly used for evaluation of disease extension in the pelvis ( ct in 94% and mri in 32% ) and hence tumor spread may be underestimated , as only a minority of patients ( 12% ) had laparotomy or laparoscopy for restaging and disease evaluation ( data not shown )  . 
in the majority of all reports on operative procedures ( 69% ) , no statement was found whether or not a total mesorectal excision ( tme ) had been performed , making it impossible to evaluate any potential impact in regard to tme procedures . only a minority of patients ( 17% ) had previously been treated with radiotherapy and of those , 81% recurred within the treated volume , making it very unlikely that our results are influenced by inclusion of these patients . 
as adjuvant radiotherapy will most often be used in risk conditions similar to those mandating the use of adjuvant chemotherapy , this should , in our opinion , not be a source of major concern . 
 be this as it may , we do not feel that our results are compromised in large scale as they do not stand in conflict with previous results of other studies . 
our recommendations for ports in adjuvant therapy ( figure 5 ) do fit well to current standards of therapy , and only minor modifications on anterior , superior and lateral borders with modest field size reductions result . 
as the amount of our data is limited for patients after apr , we would plea for more generous margins at the lower field borders , i.e. , inclusion of the perineal scar in this situation ; although this may affect acute skin toxicity , long - term side effects in the perineal region are not a major source of concern . 
the differences in metastatic involvement of liver and lungs of patients initially treated with apr and lar as detected in our data set probably simply reflect the different venous drainage of low and higher lying rectal tumors . 
 strahlentherapie und onkologie original article abrogation of radiation - inducible telomerase upregulation in hpv16 e6 transfectants of human lymphoblasts dirk neuhof1 , frdrique auberger1 , alexandra ruess1 , frederik wenz2 , klaus - josef weber1 background : telomerase activity in a human lymphoblastoid cell line with wild - type p53 status ( tk6 ) was previously shown to be rapidly induced by ionizing radiation doses as low as 10 cgy . 
since this low - dose response was absent in a closely related cell line overexpressing a mutant form of p53 ( wtk1 ) , the putative involvement of p53 was further investigated using stable human papillomavirus 16 ( hpv16 ) e6 transfectants of these cell lines . 
 material and methods : telomerase activity in hpv16 e6 transfectants of the human lymphoblastoid cell lines tk6 and wtk1 was measured by pcr / elisa and was quantified using internal standards ( titration by cell number ) run within each separate assay . 
radiation exposure ( up to 10 gy ) was unable to significantly further enhance telomerase activities , although the dynamic range of the assay would have allowed to record higher signals . 
present evidence from the literature , however , suggests that e6 mediates telomerase reverse transcriptase ( tert ) subunit transcriptional activation , whereas radiation signals to posttranscriptional / posttranslational control of telomerase activity . 
therefore , the present data enforce the previous hypothesis of a p53 dependence of telomerase upregulation by low doses of radiation and its abrogation , likely due to p53 degradation , in e6 - expressing cells . 
 key words telomerase radiation p53 hpv16 e6 lymphoblasts strahlenther onkol 2004 ; 180 : 526 doi 10.1007 / s00066 - 004 - 1129 - 1 verlust der strahleninduzierten telomeraseaktivierung in hpv16 - e6 - transfizierten humanen lymphoblasten hintergrund : eine vorhergehende studie an humanen lymphoblasten mit wildtyp - p53 - status ( tk6 ) zeigte eine rasche induktion der telomeraseaktivitt bereits durch kleine strahlendosen ( 10 cgy )  . 
da dieser effekt in einer eng verwandten zelllinie mit mutiertem p53 ( wtk1 ) nicht auftrat , sollte die vermutete rolle von p53 durch verwendung der mit hpv16 ( humanes papillomavirus 16 ) e6 stabil transfizierten zelllinien weiter untersucht werden . 
das e6 - produkt vermittelt die rasche degradation von p53 , ist aber auch als aktivator der telomerase bekannt . material und methodik : die telomeraseaktivitt in mit hpv16 e6 transfizierten zelllinien ( tk6e6 und wtk1e6 ) wurde mittels pcr / elisa gemessen und anhand interner standards in jedem separaten assay quantifiziert . 
zur bestimmung der mittleren telomerlngen diente die southern - hybridisierung terminaler restriktionsfragmente mit einer biotinylierten telomersonde . ergebnisse : die tk6e6und wtk1e6 - zellen zeigten eine gegenber den parentalen zellen deutlich erhhte telomeraseaktivitt und verlngerte telomere . 
bestrahlung ( bis 10 gy ) konnte diese telomeraseaktivitt nicht signifikant steigern , obwohl der dynamische bereich des verwendeten assays eine detektion hherer werte erlaubt htte . schlussfolgerung : die fehlende induktion der telomeraseaktivitt nach bestrahlung in e6 - transfizierten zellen knnte als ein sttigungsphnomen interpretiert werden , wenn ein gemeinsamer pfad der e6und der strahleninduzierten regulation der telomerase unterstellt wird . 
dies widerspricht aber aktuellen ergebnissen aus der literatur , wonach e6 transaktivierung der telomerase - reverse - transkriptase - ( tert - ) untereinheit vermittelt , whrend bestrahlung die telomeraseaktivitt offenbar ber posttranskriptionelle / posttranslationale mechanismen reguliert . 
die vorliegenden daten unterstreichen daher die frhere vermutung einer p53 - abhngigkeit der bei kleinen strahlendosen gemessenen telomeraseinduktion , die in e6 exprimierenden zellen , vermutlich durch die p53 - degradation , supprimiert ist . 
 schlsselwrter : telomerase bestrahlung p53 hpv16 e6 lymphoblasten 1 radiobiology research laboratory , department of clinical radiology , university of heidelberg , germany , 2 section for radiation oncology , university clinic mannheim , germany . received : december 2 , 2002 ; accepted : august 6 , 2003 strahlenther onkol 2004 no . 
with the exception of stem cell populations and primitive precursor cells , human somatic cells lack telomerase activity and telomeres shorten with each division until the cells reach replicative senescence [ 3 , 10 , 11 , 15 , 16 ]  . this growth arrest is mediated by the p53 dna damage response pathway [ 1 , 14 ] and is thought to prevent the deleterious effects arising when progressively shortened telomeres fail to prevent chromosomal fusions and rearrangements [ 32 , 50 ]  . by contrast , high levels of telomerase are expressed in the majority of human cancers [ 11 , 17 , 18 , 35 , 47 , 48 ]  . 
stabilization of telomere length by telomerase , or less frequently by an alternative recombinational ( alt ) pathway , appears to be a prerequisite for tumor cells to proliferate indefinitely [ 2 , 6 , 18 , 36 ]  . 
 in addition to telomere maintenance , telomerase can add telomeric sequences onto chromosome breaks at nontelomeric locations , a process termed chromosome healing , which requires only very short homologies to the telomere repeat [ 8 , 26 , 27 , 32 , 37 ]  . 
ionizing radiation - induced dna double - strand breaks provide a substrate for chromosome healing , but this appears to be a relatively rare event in mammalian cells [ 37 ] and its direct demonstration mimicked by i - scei restriction cutting involved highly selective experimental conditions [ 38 ]  . nevertheless , a role of telomerase in the cellular response to radiation damage is supported by the observations from several laboratories that telomerase activity represents a radiation - inducible function [ 7 , 13 , 22 , 28 , 29 , 42 ]  . 
this response is apparently absent in telomerase - negative cells , and distinct mechanisms for telomerase activation or reactivation during oncogenesis and positive modulation of that activity by radiation have been suggested [ 7 ]  . 
 oncogenic telomerase activation ( in telomerase - negative cells ) was first demonstrated for the human papillomavirus 16 ( hpv16 ) e6 gene product [ 21 ] , which is also known to promote the ubiquitination - dependent degradation of the p53 tumor suppressor protein [ 33 , 45 ]  . 
the telomerase activation by e6 may be mediated by an upregulation of the myc transcription factor which binds to specific sequences within the promotor of the telomerase reverse transcriptase ( tert ) subunit gene , thus directly activating tert expression [ 5 , 19 , 43 ]  . while these studies have not been proven universal , including diverse mechanisms of e6 / myc interaction [ 12 , 19 , 43 ] as well as other suggested pathways [ 30 , 39 , 41 ] , the prevailing view of telomerase activation by the e6 oncogene is that of tert transcriptional upregulation . 
the signaling pathway leading to radiation induction of telomerase activity is still unknown but appears to be distinct from tert transcriptional activation and rather regulates telomerase function on the posttranscriptional level [ 7 ]  . 
recent results from our laboratory with human lymphoblastoid cell lines have demonstrated some role for p53 in radiation - induced telomerase upregulation [ 28 ]  . while both the p53 wild - type ( tk6 ) and the closely related p53 mutant cells ( wtk1 ) induced telomerase activity to similar levels and with similar kinetics following irradiation with doses > 1 gy , a significant low - dose response ( down to 0.1 gy ) was only detectable in the p53 wild - type cells . 
 extending such previous work , telomerase activity was studied in the hpv16 e6 transfectant cell lines tk6e6 and wtk1e6 [ 49 ] , with the expectations of elevated telomerase activities in the e6 transfectants compared to the parental cell lines and of an abrogation of the response at low doses due to the wild - type p53 - negative status of the tk6e6 cells . 
 material and methods cell culture and irradiation the tk6e6 and the wtk1e6 cells are stable hpv16 e6 transfectants of the closely related human lymphoblastoid cell lines tk6 and wtk1 , respectively [ 49 ]  . 
the parental tk6 cells have wild - type p53 status , whereas wtk1 cells overexpress a mutated p53 with a single base pair substitution in codon 237 [ 23 ]  . 
the cells were grown at 37 c in suspension cultures in a humidified 6% co2 atmosphere in rpmi - 1640 medium supplemented with 10% heatinactivated horse serum ( gibco )  . 
cell number of the e6 transfectants per microplate well was reduced by a factor of 2 ( from 100 to 50 ) because of the higher baseline assay signal ( optical density ) with the transfectants ( see results )  . 
telomerase activity in hpv16 e6 transfectants of human lymphoblasts nal of the assay ( optical density ) after irradiation , telomerase activity of 501 , 000 unirradiated cells was measured in each experiment , and these data were used for an internal calibration curve . 
using the appropriate comparison of cell numbers ( included in the assay ) that led to identical densitometric readings [ 28 ] , relative increase of telomerase activity due to e6 transfection was about tenfold for the tk6 cells and about fivefold for the wtk1 cells , respectively . 
notably , the dynamic range of the calibration curves generated from the internal standards ( data not shown ) would have allowed to record an at least 20 - fold increase of enzyme activity ( cell number equivalent of 1 , 000 cells )  . 
the increase of mean trfl from wtk1e6 was slightly less pronounced than in the tk6e6 cells and exhibited a marked size heterogeneity smearing out between about 5 and 20 kbp , as far as detectable . 
while the previous data with the parental cell lines [ 28 ] exhibited a clear radiation induction of telomerase activity ( data included in figure 2 , for comparison ) , a respective dose response of the tk6e6 and wtk1e6 cells transfectant cells was not , or only marginally , expressed . 
this lack of a significant telomerase activation includes the low - dose range ( down to 0.1 gy ) where the tk6 cells , but not wtk1 cells , had been found to upregulate telomerase upon irradiation . 
although telomerase activation is not dependent on the e6 function to augment p53 degradation [ 4 , 20 , 25 , 31 , 46 ] , the higher telomerase baseline levels in the p53 - negative tk6e6 cells when compared with the mutant p53 - overexpressing wtk1e6 cells ( see results ) need to be addressed , briefly . 
the selective pressure , due to the presence of geneticin , for high levels of retroviral vector gene expression ( neo and e6 ) may be less stringent with the wtk1 cells , because the p53 mutants are much less apoptosis - susceptible than the tk6 cells and also the tk6e6 cells [ 40 , 44 , 49 ]  . 
a respective difference in e6 protein levels was not tested , but the more heterogeneous increase of telomere lengths ( trfl ) in the wtk1e6 cells ( not shown ) would be compatible with the idea that these cells are more tolerable to decreased or occasional losses of transgene expression . 
 in our previous study , telomerase activity of the parental tk6 and wtk1 cells was increased by ionizing radiation [ 28 ]  . telomerase is able to add telomeric sequences onto radiationinduced dna double - strand breaks . 
this process could be an important cofactor in the conversion of radiation - induced dna double - strand breaks into chromosome breaks , thus preventing double - strand break rejoining or , more importantly , misrejoining that could give rise to unstable chromosome aberrations . 
effect of different radiation doses on telomerase activity measured 1 h after exposure of tk6e6 cells ( circles ) and of wtk1e6 cells ( triangles ) , given as cell number equivalents relative to unirradiated controls . 
the tert subunit is limiting for telomerase function [ 24 , 34 ] , but no increased tert transcript levels were observed in irradiated telomerase - positive mouse cell lines , although telomerase activity was induced [ 7 ]  . 
taken together , these findings provide compelling evidence for a posttranscriptional mechanism of telomerase activation by radiation . considering that telomerase induction by e6 reflects tert promotor transactivation , one should expect that such increased baseline telomerase levels are still amenable to a positive functional modulation by radiation . 
either an elevated abundance of tert transcripts could by itself foster a negative regulation of the posttranscriptional / posttranslational activation mechanism , but no further evidence appears available to support this speculation . 
 rogation of the p53 - dependent low - dose response ( < 1 gy ) of tk6 by e6 transfection cells could be readily explained by the ability of e6 to trigger p53 degradation . 
but also for higher doses ( > 1 gy ) and for extended postirradiation incubations ( up to 24 h ) , a respective telomerase activation was lacking , or only marginally expressed , in both tk6e6 and wtk1e6 cells ( figures 2 and 3 )  . 
given the absence of further information , one may only speculate that the primary function of e6 to target various proteins for degradation [ 9 , 35 ] could also include some other radiation - inducible positive regulator ( s ) of telomerase activity . 
abrogation by e6 of the previously described response of p53 wild - type cells to low radiation doses enforces the existence of a p53 - dependent pathway of telomerase activation . 
but the general suppression of radiation - inducible telomerase activation , also at higher doses , suggests an additional mechanism through which e6 interferes with the upregulation of telomerase by ionizing radiation , and which was previously shown to be independent of p53 at such higher doses . 
 strahlentherapie und onkologie current discussion outcome of postoperative treatment for rectal cancer uicc stage ii and iii in day - to - day clinical practice results from a retrospective quality control analysis in six institutions in north bavaria ( germany ) jrn wulf1 , karin krmer1 , claas van aaken1 , franz dietzel2 , dietrich lucas3 , klaus pfndner4 , thomas schimpke3 , wolfgang schulze2 , hans - joachim thiel5 , klaus ziegler6 , michael flentje1 background and purpose : radiochemotherapy ( rcht ) as adjuvant treatment for rectal cancer uicc stage ii / iii has been recommended by the national cancer institute ( nci ) since 1991 and in germany since 1994 . 
the 5 - year actuarial rate was as follows : local control 75% ( 6384% ) , freedom from distant metastases 56% ( 4463% ) , disease - free survival ( dfs ) 53% ( 4259% ) , and overall survival ( os ) 53% ( 4564% )  . 
6% ( 211% ) of patients showed involved resection margins , in 33% of patients categorized pn0 less than the required twelve lymph nodes were examined , both leading to a significant decrease of local control . conclusion : while the quality of adjuvant treatment followed consensus guidelines , the number of referred patients which was lower as expected and the inferior treatment results as compared to randomized studies indicate that the consensus recommendations for adjuvant treatment have not been fully accepted . 
 key words : rectal cancer adjuvant treatment radiochemotherapy patterns of care strahlenther onkol 2004 ; 180 : 514 doi 10.1007 / s00066 - 004 - 1175 - 8 ergebnisse der postoperativen behandlung des rektumkarzinoms im uicc - stadium ii und iii in der tglichen klinischen praxis . 
resultate einer retrospektiven analyse zur qualittskontrolle in sechs frnkischen kliniken hintergrund und ziel : die adjuvante radiochemotherapie ( rcht ) des rektumkarzinoms im uicc - stadium ii / iii wird seit 1991 vom national cancer institute ( nci ) und in deutschland seit 1994 als standard empfohlen . 
die qualitt und ergebnisse der postoperativen therapie in der tglichen klinischen praxis wurden flchendeckend retrospektiv untersucht . patienten und methodik : insgesamt wurden 534 patienten aus sechs institutionen ausgewertet , die zwischen 1993 und 1998 behandelt wurden . 
nach 5 jahren betrugen die aktuarische lokale kontrolle 75% ( 6384% ) , die freiheit von fernmetastasen 56% ( 4463% ) , das krankheitsfreie berleben 53% ( 4259% ) und das gesamtberleben 53% ( 4564% )  . 
bei 6% ( 211% ) aller 1 department of radiotherapy , university of wrzburg , germany , 2 department of radiotherapy , bayreuth hospital , bayreuth , germany , 3 department of radiology , aschaffenburg hospital , aschaffenburg , germany , 4 department of radiotherapy , leopoldina hospital , schweinfurt , germany , 5 department of radiotherapy and radiooncology , bamberg hospital , bamberg , germany , 6 department of radiotherapy , ansbach hospital , ansbach , germany . received : march 19 , 2003 ; accepted : september 3 , 2003 strahlenther onkol 2004 no . 
outcome of adjuvant treatment for rectal cancer patienten war nicht in sano ( r1 / 2 ) reseziert worden ; bei 33% der pn0 kategorisierten tumoren wurden weniger als die geforderten zwlf lymphknoten untersucht ; beides fhrte zu einer signifikant reduzierten lokalen kontrolle . 
 schlussfolgerung : der niedrige anteil an der adjuvanten therapie zugewiesenen patienten sowie die im vergleich zu randomisierten studien ungnstigeren ergebnisse weisen auf die auswahl eines risikokollektivs hanstelle einer stadienbezogenen zuweisung scheint eine auswahl mit individueller risikoabschtzung durch den chirurgen bevorzugt zu werden . 
 schlsselwrter : rektumkarzinom adjuvante therapie radiochemotherapie qualittskontrolle introduction patients and methods combined radiochemotherapy ( rcht ) for rectal cancer uicc stage ii and iii was recommended in the usa by the national cancer institute ( nci ) in 1991 and in germany by a consensus meeting of the german cancer society in 1994 and 1998 [ 14 , 2325 ]  . 
while adjuvant chemotherapy ( cht ) or radiotherapy ( rt ) alone did not show a significant influence on local recurrence rates of 2125% after surgery , combined rcht decreased local recurrences to 714% after 5 years . 
these results were confirmed by a norwegian study which demonstrated a decrease of local failure rates from 30% to 12% and a statistically significant increase of the 5 - year survival rate from 50% to 65% ( p = 0.01 ) by adjuvant rcht [ 32 ]  . 
the beneficial effect of adjuvant treatment was only achieved by combined rcht with radiation doses > 4550 gy / reference point in daily fractions of 1.82.0 gy using a threeor four - field technique . 
studies applying lower doses or inadequate irradiation techniques ( ventrodorsal opposing fields only ) failed to improve local control and / or revealed major side effects [ 2 , 5 ]  . 
 the purpose of this multicentric retrospective analysis was to evaluate the quality and results of postoperative treatment in day - to - day practice not only in a single institution but in a complete region covered by six radiotherapeutic facilities . due to the lack of a cancer register in most parts of germany , this approach should reflect treatment results achieved after postoperative therapy in patients treated in daily routine . 
 six radiotherapeutic institutions in north bavaria , germany , participated in the evaluation , including a university hospital and five teaching hospitals ( the numbers characterizing clinics 16 are chosen randomly and are not related to the authors order of appearance )  . 
the six institutions provide radiotherapeutic care for about 2.3 million residents ( according to administrative data ) and completely covered the region of north bavaria ( whole upper and lower franconia , parts of middle franconia ) at the time of evaluation . 
 all patients registered at the radiotherapeutic departments in a 5 - year period from april 1 , 1993 to march 31 , 1998 with pathologically staged rectal cancer uicc stage ii ( n = 147 ; 28% ) and iii ( n = 367 ; 69% ) were evaluated . 
in single cases , patients stage i ( n = 9 ; 1% ) and iv ( n = 11 ; 2% ) were included if the treatment followed curative intention , e.g. , after resection of a synchronous liver metastasis . 
staging was performed according to the 1992 tnm classification ( including pn3 ) , which was the current version during the treatment period . during the evaluation period , a total of 534 patients received adjuvant treatment under curative intention . 
527 ( 99% ) were evaluable with complete charts and follow - up . median follow - up of patients was 47 months ( 1791 months )  . the retrospective evaluation was performed by analysis of the radiotherapeutic patient charts . 
data were completed by a questionnaire sent to general practitioners or institutions in charge of patient management to acquire data on cht , followup including local control , survival , and treatment - related toxicity . 
a description of evaluation , patient , tumor and treatment characteristics is given in tables 1 and 2 . patient evaluation was performed according to an intention - to - treat philosophy . 
local recurrence or distant metastases were diagnosed histologically or radiologically . rarely , clinical diagnosis alone was available based on typical symptoms such as pain , bleeding or progressive deterioration strahlenther onkol 2004 no . 
 for statistical analysis , the kaplan - meier method was used for actuarial analysis of local control , freedom from distant metastases , disease - free ( dfs ) and overall survival ( os )  . statistical significance was evaluated by the log - rank test . 
the mean values of independent variables or categories were compared by the t - test ( two variables / categories ) or by unifactorial variance analysis ( more than two variables / categories )  . 
multivariate analysis of factors having an influence on local control , distant metastases , dfs and os was performed by the cox regression with stepwise forward progression and exclusion of cases with missing values . 
 results surgery 51% ( 3864% ; p = 0.036 ) of patients were treated by low anterior resection ( lar ) , 43% ( 3356% ; n.s. ) by abdominoperineal resection ( apr ) , and 4% ( 18% ; n.s. ) underwent a hartmann procedure . 
zur statistischen auswertung der signifikanz der unterschiede zwischen den institutionen wurde der ( cid : 2 ) 2 - test oder der kruskal - wallis - h - test verwendet . 
age was no significant factor for the decision to administer cht : median and mean age of patients with rcht was 61 years ( 3483 years , sd 9 years ) compared to 65 / 64 years ( 4080 years , sd 9 years ) for patients with rt alone . 
in all institutions , rt consisted of two series : in a first series , a standard volume was irradiated including the tumor bed and pelvic lymphatic drainage ( cranial field border l4 / 5 or l5 / s1 , caudal field border middle third of obturator foramen after lar or including the perineum after apr )  . 
the median dose to this volume was 45 gy ( 252 gy , sd 5.1 gy ) , usually prescribed to the icru reference point , in one clinic to the 95% isodose . 
in five institutions , the first two cycles of cht were administered simultaneously with rt , in clinic 6 , the nci protocol with two cycles of cht prior to rt and a second and third cycle shortened to 3 days duration was used . 
in three clinics , 5 - fu was administered as bolus infusion ( 360500 mg / m2 ) , two institutions performed continuous infusion over 24 h ( 5001 , 500 mg / m2 ) , and in one clinic , a 5 - fu dose of 1 , 000 mg / m2 ( maximum 1 , 800 mg absolute ) was infused over 12 h . 
occasionally , levamisole , mitomycin c or a monoclonal antibody , 17 - 1a , were part of the cht . details of rt and cht are shown in table 2 . 
outcome of adjuvant treatment for rectal cancer local control freedom from distant metastases clinic 1 ( 77% ) clinic 2 ( 70% ) clinic 3 ( 80% ) clinic 4 ( 63% ) clinic 5 ( 73% ) clinic 6 ( 84% ) all ( 75% ) clinic 1 ( 56% ) clinic 2 ( 49% ) clinic 3 ( 58% ) clinic 4 ( 44% ) clinic 5 ( 63% ) clinic 6 ( 60% ) all ( 56% ) months figure 1 . 
single evaluation of local control rates from each institution revealed significantly superior results of clinic 6 compared to clinics 4 ( p = 0.01 ) and 5 ( p = 0.02 ) in log - rank test . 
whrend die lokalen kontrollraten sich insgesamt nicht signifikant unterschieden , zeigte sich im logrank - test im vergleich der einzelnen kliniken untereinander eine signifikant hhere lokale kontrollrate der klinik 6 gegenber den kliniken 4 ( p = 0 , 01 ) und 5 ( p = 0 , 02 )  . 
the local control rate of institution 6 was significantly superior to the result of clinics 4 ( p = 0.01 ) and 5 ( p = 0.02 ) in log - rank test ( figure 1 )  . 
88 of the 107 local recurrences ( 83% ) were associated with distant metastases , only 19 ( 17% ) occurred locally alone ( 3.8% of all patients )  . 
of the 107 patients with locally uncontrolled disease , 53% relapsed presacrally , 15% in the sacral bone , 22% at the anastomosis , and 30% at different pelvic locations ( the number exceeding 100% represents the rate of simultaneous recurrences at different locations )  . 
actuarial rate of freedom from distant metastases after 5 years was 56% in all patients , ranging from 44% to 63% between the six institutions with no significant difference in log - rank test ( figure 2 )  . 
overall survival was 53% after 5 years at kaplan - meier analysis for all patients , ranging from 45% to 64% between the six institutions without statistically significant differences in log - rank test ( figure 4 )  . 
 treatment - related acute toxicity of rt was low : acute intestinal side effects grade 1 were documented in 22% , grade 2 in 38% , and grade 3 in 10% of patients . 
outcome of adjuvant treatment for rectal cancer disease - free survival overall survival clinic 1 ( 52% ) clinic 2 ( 47% ) clinic 3 ( 55% ) clinic 4 ( 42% ) clinic 5 ( 58% ) clinic 6 ( 59% ) all ( 53% ) clinic 1 ( 60% ) clinic 2 ( 45% ) clinic 3 ( 64% ) clinic 4 ( 46% ) clinic 5 ( 54% ) clinic 6 ( 54% ) all ( 53% ) months months figure 3 . 
whrend sich das krankheitsfreie berleben insgesamt nicht signifikant unterschied , zeigte sich im log - rank - test im vergleich der einzelnen kliniken untereinander ein signifikant lngeres berleben bei klinik 6 gegenber klinik 4 ( p = 0 , 02 )  . patient selection for adjuvant treatment unfortunately , no cancer registry is available in bavaria . therefore , the proportion of patients referred to adjuvant therapy had to be estimated . 
according to cancer registers , the incidence of rectal cancer is 25 / 100 , 000 people [ 3 ] , 50% of these in uicc stages ii and iii . 
in conclusion , 132 patients with rectal cancer uicc stage ii and iii are expected every year , leading to a total of about 660 patients during the evaluation period of 5 years . 
in fact , only 245 patients were referred to adjuvant treatment from april 1 , 1993 to march 31 , 1998 , which is only about 37% of the expected number of patients . 
 the proportion of about 37% of referred patients and the only slowly increasing proportion of patients during the 5 years of evaluated treatment suggest that patients were not sent according to the consensus recommendations which are based on tumor stage alone , but according to individual risk factors figure 4 . 
another risk factor was pathologic lymph node status : surprisingly , 5 - year actuarial local control of pn0 was only 72% compared to 85% and 74% in patients categorized pn1 and pn2 , respectively . 
actuarial local control of correctly categorized pn0 was 74% compared to 83% in patients with an unknown number of nodes examined and 52% in pn0 categorized on the basis of less than twelve lymph nodes ( p < 0.001 , log - rank test )  . 
no significant accumulation of risk factors from multivariate analysis such as higher tumor grading , incomplete resection status or rt alone were seen in patients categorized pn0 compared to patients categorized pn +  . 
 cox regression proportional hazards from distant metastases 56% ( 4463% ) compared to local control rates ranging from 86% to 93% and freedom from metastases at rates of 6778% in randomized studies [ 4 , 6 , 7 , 16 , 32 ]  . 
according to our epidemiologic estimation , only about 37% of expected patients with rectal cancer uicc stage ii or iii have been referred to adjuvant treatment within the evaluation period . 
of course , the calculation of the proportion of admitted patients is only an estimation , because due to the lack of a cancer register precise data are not available and the administrative borders are not fully congruent with the area of patient recruitment for radiotherapeutic care . 
this conclusion has also been supported by an evaluation from the usa published by schroen et al . , who observed a rate of 40% for uicc stage ii and 60% for stage iii referred to adjuvant treatment [ 29 ]  . 
this is additionally supported by the only slight increase in the proportion of patients admitted in the year prior to the consensus recommendation ( 04 / 199303 / 1994 ) from 16.5% to 24% during the treatment period from 04 / 199703 / 1998 . 
even though the treatment results of patients not referred to adjuvant treatment might be much more favorable , it must , however , be admitted that the outcome of patients analyzed is not satisfactory . 
 discussion in the present evaluation , treatment results after adjuvant therapy are inferior to the results expected from randomized studies : 5 - year local control was 75% ( 6384% ) and freedom strahlenther onkol 2004 no . 
outcome of treatment in day - to - day clinical practice was influenced by several factors , which are different to the conditions in randomized studies : patient selection with only about 37% of all expected patients referred to postoperative treatment . 
58% of patients categorized pn0 did not fulfill criteria for pn0 : in 33% , less than twelve lymph nodes were assessed , in 25% the number of assessed lymph nodes was not reported . 
die behandlungsergebnisse im klinischen alltag wurden durch mehrere faktoren beeinflusst , die in groen randomisierten klinischen studien ausgeschlossen sind : es wurden nur etwa 37% der epidemiologisch erwarteten patienten einer postoperativen therapie zugewiesen ( mglicherweise auswahl eines risikokollektivs )  . 
58% der patienten mit pn0 ( n = 156 ) erfllten die pathologischen kriterien der pn0 - kategorie nicht : in 33% wurden weniger als zwlf lymphknoten untersucht , und in weiteren 25% wurde die anzahl der untersuchten lymphknoten nicht angegeben . limit in randomized studies ( 714% ) after adjuvant rcht , an estimated 200 local recurrences must occur among the total number of about 1 , 450 expected patients within a 5 - year period in the evaluated region . 
this observation is consistent with the results from randomized studies which showed an advantage from adjuvant treatment only for combined rcht , but not for rt alone [ 4 , 6 , 7 , 16 , 22 , 34 ]  . 
while the quality of adjuvant therapy was consistent with the consensus recommendations in terms of radiation dose , irradiation technique and cht protocols in all participating institutions , the proportion of combined rcht differed significantly ( 7199% ; p < 0.001 ) between the six clinics . 
in the present evaluation , the proportion of patients with macroscopic or microscopic residual disease was 6% ( 211% ) with local control rates of 43% and 72% , respectively ( compared to 76% after complete resection )  . 
the negative effect of infiltrated margins has been reported by other authors with local failure rates for close margins < 10 mm of 30% [ 9 , 22 ] and a significantly impaired 5 - year survival rate of only 311% after r1 / 2 resection [ 12 ]  . 
therefore , improvement of preoperative staging and consideration of neoadjuvant treatment for " down - staging of ct4 tumors might decrease the rate of incomplete resections associated with a high risk of local failure even after the adjuvant rcht . 
in the present study , node - negative patients had an inferior local control rate of 70% as compared to 87% for patients categorized pn1 , which indicates that in patients with uicc stage ii other or additional risk factors must have been present . 
relevant factors are described by willet et al . , who observed 10 - year local control rates of 95% in patients categorized pt3 pn0 with favorable pathologic findings ( well differentiated tumor , perirectal fat invasion < 2 mm , no venous or lymphatic vessel invasion ) , while only 71% of patients with unfavorable findings ( poorly differentiated tumor , moderate to deep perirectal fat invasion , venous or lymphatic vessel invasion ) were locally controlled after 10 years with surgery alone [ 33 ]  . 
pooled the data of three randomized studies and evaluated the influence of the tnm stage on the results of adjuvant treatment for rectal cancer : patients with only one risk factor such as nodal invasion had an improved outcome as compared to patients with two or more risk factors [ 8 ]  . 
 the hypothesis of accumulation of risk factors leading to an impaired local control rate in patients categorized pn0 is supported by the quality of pathologic lymph node assessment : only 42% ( n = 65 ) of pn0 patients ( n = 156 ) fulfilled the pathologic criterion of a minimum of twelve examined lymph nodes . in 33% , less than twelve lymph nodes were examined ( n = 52 ) , and in 25% , the number of nodes was not reported by the pathologist ( n = 39 )  . 
according to the data presented , pn0 patients with less than twelve lymph nodes had a 5 - year local control rate of 52% , which is even below that of pn3 patients ( 59% ) indicating that additional risk factors may have been missed on pathologic workup , e.g. , the resection status , which was not reported in 53 patients ( 10% )  . 
outcome of adjuvant treatment for rectal cancer correctly categorized pn0 has been stated by other authors , who found local recurrence rates ranging from 19% to 37% depending on the number of examined lymph nodes even after adjuvant rcht [ 31 ]  . 
while the rate of metastases only ( 22.8% ) corresponds well to the results of randomized studies , the proportion of combined failures is high and may be relevant for the inferior dfs . 
 conclusion we have tried to give a detailed analysis of quality and outcome of postoperative treatment in patients with rectal cancer uicc stages ii and iii in day - to - day clinical practice using a patterns - of - care approach in a defined region in north bavaria . 
to some extent , application of rt and cht varies between the six participating institutions , but is , in our opinion , well within a corridor of adequate treatment . 
treatment - related acute toxicity and especially late toxicity are low , as far as these data could be evaluated retrospectively with a median follow - up of 47 months . 
the main result is the considerable selection bias in referring patients to postoperative treatment with associated inferior treatment outcome if compared to the results from randomized studies . the impaired outcome of incompletely resected tumors , inaccurately categorized pn0 patients , the low rate of documented tme and the high rate of apr indicate obvious need for improvements in surgical and histopathologic assessment . 
as long as there are no central quality assurance and outcome programs such as , for instance , in the netherlands , retrospective analysis of treatment quality and results may be helpful to improve institutional outcome by achieving an interdisciplinary consensus on multimodal treatment in rectal cancer . 
this will be important even if preoperative approaches to achieve tumor cell devitalization or down - sizing and down - staging of tumors to increase the rate of sphincter preservation and to decrease the rate of incomplete resection will become the standard treatment in primary resectable tumors [ 17 , 18 , 26 , 28 ]  . 
 strahlentherapie und onkologie original article blood hemoglobin level and treatment outcome of early breast cancer michael henke1 , florian sindlinger1 , hans ikenberg2 , thomas gerds3 , martin schumacher3 background and purpose : to determine whether the blood hemoglobin concentration correlates with the prognosis of patients with early breast cancer and , if so , whether this is restricted to treatment modality . patients and methods : data were collected retrospectively from patients with early breast cancer ( t1 , 2 n02 m0 ) who underwent either breast - conserving surgery followed by adjuvant radiotherapy ( bcs - rt ; n = 96 ) or a modified radical mastectomy ( mrm ; n = 194 )  . 
 key words : anemia erythropoietin breast cancer radiotherapy strahlenther onkol 2004 ; 180 : 4551 doi 10.1007 / s00066 - 004 - 1123 - 7 bluthmoglobinspiegel und behandlungserfolg beim kleinen mammakarzinom hintergrund und ziel : es wird untersucht , ob eine beziehung zwischen dem hmoglobinspiegel des bluts und dem therapieerfolg bei patientinnen mit brustkrebs besteht und ob dies nur bei bestimmten behandlungsmodalitten zu beobachten ist . patienten und methodik : patientinnen mit kleinem mammakarzinom ( t1 , 2 n02 m0 ; tabelle 1 ) wurden retrospektiv erfasst . ihre therapie bestand entweder aus einer brusterhaltenden operation mit anschlieender bestrahlung ( bcs - rt ; n = 96 ) oder aus einer modifizierten radikalen mastektomie ( mrm ; n = 194 )  . 
die beziehung zwischen properativem hmoglobinwert , nodalstatus , histologischer differenzierung sowie hormonrezeptorstatus und krankheitsfreiem berleben wurde mit einem cox - regressionsmodell fr beide behandlungsmodalitten bestimmt und in kaplan - meier - graphiken dargestellt . 
 ergebnisse : bei patientinnen nach bcs - rt korrelierte die bluthmoglobinkonzentration signifikant mit dem krankheitsfreien berleben ( relatives risiko [ rr ] : 0 , 67 pro g / dl ; p = 0 , 007 ; tabellen 24 und abbildungen 1 und 2 ) , und zwar unabhngig von anderen bekannten prognosefaktoren des mammakarzinoms ( multivariat )  . 
 schlsselwrter : anmie erythropoetin mammakarzinom strahlentherapie 1 department of radiotherapy , radiological university clinic , 2 department of gynecology and obstretics , gynecological university clinic , and 3 institute for medical biometry and medical informatics , university freiburg , germany . 
hemoglobin level and breast cancer introduction anemia , a lack of hemoglobin - containing red blood cells sufficient to maintain adequate tissue oxygenation , is a common complication affecting > 50% of cancer patients [ 25 ]  . 
anemia was felt to represent a symptom of more advanced / aggressive disease . however , as data from intratumoral oxygen measurements suggest that low hemoglobin levels diminish tumor oxygenation [ 2 , 40 ] , impaired , hypoxia - mediated , radiation efficacy is also a possible explanation [ 13 , 30 ]  . 
clinical observations may support the latter : ( 1 ) a dose - response relationship exists between hemoglobin values and treatment outcome [ 3 , 16 ] ; ( 2 ) hemoglobin concentration and treatment outcome closely correlate , independent of known prognostic parameters such as histology , or stage of disease [ 10 , 35 ] ; and ( 3 ) hemoglobin levels are associated with radiation - induced side effects [ 15 , 21 ]  . 
we therefore intended to investigate the prognostic significance of blood hemoglobin concentration for patients with early breast cancer and , additionally , to find out whether an eventual hemoglobin effect will be restricted to radiotherapy . patients and methods patients patients with early breast cancer treated between january 1988 and december 1991 in the department of gynecology and obstetrics at the gynecologic university clinic , freiburg , germany , qualified for this analysis . 
at that time , treatment gradually changed from modified radical mastectomy without radiotherapy ( mrm ) to breast - conserving surgery followed by adjuvant radiotherapy ( bcs - rt )  . 
the decision which treatment modality should be used was at the surgeons discretion . to obtain comparable treatment groups , we restricted the analysis to patients with histologically proven and early ( t1 or t2 ) disease , a documented preoperative blood hemoglobin value , and at least one follow - up visit 3 months after treatment completion . 
patients with mastopathy , ductal carcinoma in situ , relapsing disease , t0 stage or metastases , inoperability , or radiotherapy at institutions other than ours were not included in this analysis . 
 treatment and clinical outcome bcs - rt patients received lumpectomy , segment resection , or quadrantectomy followed by axillary lymph node dissection . thereafter , they were treated by adjuvant radiotherapy . 
patients that completed therapy were followed up at 3 - month intervals within the first 2 years , at 6month intervals up to year 5 , and then on an annual basis . 
 data collection , primary variable , and statistical analyses patient details , hemoglobin level , tumor histology , classification , and receptor status were obtained from the hospital charts , as were details of surgical , radiotherapeutic or medical interventions . 
 the effect of the blood hemoglobin concentration on disease - free survival time following both , bcs - rt and mrm , was analyzed using a cox regression model [ 7 ]  . 
in order to account for the probable confounding factor of adjuvant treatment , the model was stratified for chemotherapy and adjusted up - front for risk factors of breast cancer such as nodal status ( n0 , n1 , n2 ) , tumor grade ( 1 , 2 , 3 ) [ 4 ] , progesterone and estrogen receptor status ( positive if > 20 fmol / mg cytosol protein ) , and age at diagnosis . 
 for demonstration purposes , patients were additionally grouped into low ( < 12 g / dl ) , normal ( 1214 g / dl ) and high ( 14 g / dl ) hemoglobin cohorts , and kaplan - meier graphs for these cohorts were constructed for both , bcs - rt and mrm [ 20 ]  . 
reasons for not including patients were : no surgical procedure performed ( n = 4 ) , irradiation following mastectomy ( n = 19 ) , lack of irradiation following breast - conserving surgery ( n = 24 ) , radiotherapy in clinics other than the study institution ( n = 9 ) , treatment and follow - up data unavailable ( n = 12 ) , and locally advanced breast cancer ( t3 or t4 ; n = 49 )  . 
 clinical outcome within the first 2 years following surgery , 20 ( 7% ) of all 290 patients had died , 21 suffered a local or systemic relapse , and ten and nine patients , respectively , were censored for these events . 
actuarial 5 - year survival , disease - free survival , and locoregional control probabilities were 85 4% , 70 5% , and 88 4% , respectively , for bcs - rt , and 74 3% , 70 3.4% , and 91 2% , for mrm . 
 blood hemoglobin levels blood hemoglobin levels before and after surgery were available for all and for 93% of patients , respectively , and for 29 patients immediately before starting radiotherapy . 
 disease - free survival and hemoglobin level according to treatment group a total of 29 events ( relapse or death ) were reported for patients treated with bcs - rt , twelve corresponding to local failures and 17 to either death or distant failures ( table 2 )  . 
 the distributions of tumor grade , nodal and hormone receptor status for both treatment groups , according to preoperative hemoglobin level , are displayed in table 3 . multivariate analysis demonstrated a relative risk ( rr ) of 0.67 ( 95% confidence interval [ ci ] : 0.500.89 ; p = 0.007 ) for table 1 . 
bcs - rt : breast - conserving surgery followed by adjuvant radiotherapy ; ci : confidence interval ; dfs : disease - free survival ; mrm : modified radical mastectomy ; n / a : not applicable ; nr : not reached . 
kaplan - meier graphs visualized this impaired disease - free survival for bcs - rt patients with low ( < 12 g / dl ) blood hemoglobin concentrations ( figure 1 )  . 
corresponding to the multivariate analysis , kaplan - meier plots did not demonstrate impaired disease - free survival for mrm patients with low blood hemoglobin values ( figure 2 )  . 
 we additionally analyzed the effect of preoperative hemoglobin in the whole study population by adding a treatment indicator and a treatment - hemoglobin interaction term to the multivariate cox regression model . 
 though retrospective studies , particularly on small samples , may be misleading , demographic data , treatment techniques and outcome of our bcs - rt and mrm patients compare well to literature data [ 9 , 17 , 28 , 29 , 31 , 39 , 41 ] and seem to exclude an eventual selection bias . 
further , by meticulously forming both patient cohorts preceding the statistical analyses we made sure to fulfill one of the major requirements for prognostic factor studies [ 34 ]  . 
the high incidence of axillary lymph node involvement 71% and 64% in bcs - rt and mrm , respectively in the low hemoglobin level groups ( < 12 g / dl ) may raise some suspicion of group imbalance . 
however , this incidence is comparable for both treatment modalities , and we further counteracted a possible bias by adjusting the cox model for nodal status and the major prognostic factors of breast cancer , like chemotherapy [ 32 ]  . 
treatment - covariate interactions are to be cautiously interpreted when p - values derive from different patient groups [ 34 ] , and preferably treatment - covariate interaction terms should be used in suitable regression models . 
the resulting interaction term , between preoperative hemoglobin and treatment regimen , again , was highly significant , supporting that the hemoglobin effect , indeed , may be restricted to bcs - rt . 
 though anemia is well known to be associated with prognosis in radiotherapy patients with overt cancer [ 8 , 12 , 27 ] , its significance for adjuvant irradiation following surgical resection has to our knowledge been described only once [ 10 ]  . 
this is suggested by the facts that ( 1 ) conservative surgery achieved comparable tumor control rates as did radical resection when assisted by adjuvant radiation , and ( 2 ) that initial tumor size ( t - stage ) did not predict relapse when the breast was irradiat > 14 g / dl 1214 g / dl < 12 g / dl months figure 1 . 
disease - free survival of early breast cancer patients receiving breast - conserving surgery followed by adjuvant radiotherapy ( bcsrt ; n = 96 ) according to preoperative blood hemoglobin level . 
correlation of risk factors in patients treated with breastconserving surgery followed by adjuvant radiotherapy ( bcs - rt )  . spearman rank correlation coefficients for hemoglobin level ( hb ) , nodal stage , tumor grade , age , adjuvant chemotherapy ( ctx ) , radiation dose ( rt dose ) , estrogen receptor ( er ) and progesterone receptor ( pr ) status . 
spearman - rank - korrelationskoeffizienten fr hmoglobinspiegel ( hb ) , nodalstatus , histologische differenzierung , alter , adjuvante chemotherapie ( ctx ) , bestrahlungsdosis ( rt dose ) , strogenrezeptor - ( er - ) und progesteronrezeptor - ( pr - ) status . 
spearman rank correlation coefficients for hemoglobin level ( hb ) , nodal stage , tumor grade , age , adjuvant chemotherapy ( ctx ) , estrogen receptor ( er ) and progesterone receptor ( pr ) status . 
spearman - rank - korrelationskoeffizienten fr hmoglobinspiegel ( hb ) , nodalstatus , histologische differenzierung , alter , adjuvante chemotherapie ( ctx ) , strogenrezeptor - ( er - ) und progesteronrezeptor - ( pr - ) status . 
the impact of hemoglobin level on the outcome of patients treated by bcs - rt may , thus , be interpreted as hemoglobinhypoxia - mediated changes of radiosensitivity [ 2 , 13 ]  . 
a prognostic significance of the hemoglobin concentration for patients undergoing chemotherapy , finally , is barely investigated [ 33 , 37 ] , albeit an oxygenenhanced activity of some cytostatic drugs is well documented [ 36 ]  . 
 although the mechanism of how blood hemoglobin relates to treatment efficacy is not clarified , a correlation between the two provided at least for radiotherapy patients a rationale for restoring depressed hemoglobin levels in order to improve therapy . 
 strahlentherapie und onkologie original article local recurrence rates in breast cancer patients treated with intraoperative electron - boost radiotherapy versus postoperative external - beam electron - boost irradiation a sequential intervention study roland reitsamer1 , florentia peintinger2 , michael kopp3 , christian menzel1 , h . 
dieter kogelnik3 , felix sedlmayer3 background and purpose : the purpose of this sequential intervention study was to determine the rate of local recurrences and the rate of distant metastases in patients with invasive breast cancer who had been treated with breast - conserving surgery and postoperative radiation therapy to the whole breast either with postoperative electron boost in group 1 or with intraoperative electron boost ( iort ) in group 2 . 
 conclusion : immediate iort boost yielded excellent local control figures in this prospective investigation and appears to be superior to conventional postoperative boost in a short - term follow - up . 
 key words : breast cancer intraoperative radiotherapy boost irradiaton breast - conserving surgery strahlenther onkol 2004 ; 180 : 3844 doi 10.1007 / s00066 - 004 - 1190 - 9 lokalrezidivrate bei brustkrebspatientinnen nach intraoperativer elektronenboostbestrahlung versus postoperativer konventioneller boostbestrahlung hintergrund und ziel : ziel dieser sequentiellen interventionsstudie war die bestimmung der lokalrezidivund fernmetastasenrate von patientinnen mit invasivem mammakarzinom , die mit brusterhaltender operation und anschlieender bestrahlung der gesamten brust , aber verschiedenen boostbestrahlungen therapiert worden waren . 
 1 department of senology , general hospital salzburg , austria , 2 department of gynecology and obstetrics , general hospital leoben , austria , 3 department of radiotherapy and radiooncology , general hospital salzburg , austria . 
die 4 - jahres - raten fr lokalrezidive betrugen 4 , 3% ( 95% - konfidenzintervall 1 , 88 , 2% ) und 0% ( 95%konfidenzintervall 01 , 9% ) und die 4 - jahres - raten fr fernmetastasen 7 , 9% ( 95% - konfidenzintervall 4.512 , 8% ) und 1 , 1% ( 95% - konfidenzintervall 0 , 13 , 8% )  . 
 schlussfolgerung : die intraoperative boostbestrahlung zeigt exzellente ergebnisse bezglich der lokalrezidivrate und scheint der postoperativen boostbestrahlung in der kurzzeitnachbeobachtung berlegen zu se schlsselwrter : mammakarzinom intraoperative radiotherapie boostbestrahlung brusterhaltende operation introduction breast conservation therapy with wide excision of the tumor and postoperative radiotherapy of 5055 gy to the whole breast is a standard of care for breast cancer patients . 
with this therapy , an excellent local tumor control can be achieved . the additional application of an external boost therapy of 1016 gy to the tumor bed can reduce the local failure rate by 40% . 
several methods are used to exactly localize the tumor bed : tumor bed clipping by the surgeon with titanium clips , perioperative brachytherapy , or intraoperative radiotherapy ( iort )  . 
this single high radiation dose is delivered to a surgically defined area , while uninvolved and dose - limiting tissues are displaced , with the goal of enhanced locoregional tumor control . 
current indications for iort are cancers of the stomach , liver , biliary tract , pancreas , colon and rectum , urinary bladder , prostate , and uterus , which are surrounded by normal tissues or organs with low dose tolerance . 
 according to our prospectively defined hypothesis , iort in boost modality for breast cancer patients would be able to reduce local recurrence rates , as this technique assures a boost to the target area with a higher precision as compared to conventional postoperative boost techniques . 
from january 1996 to october 1998 , 188 patients were treated with breast - conserving surgery and postoperative irradiation to the whole breast ; additionally , an external - beam electron boost was delivered to the tumor bed ( group 1 )  . 
the consecutive 190 patients from october 1998 to march 2001 were treated with breast - conserving surgery , intraoperative electron - boost technique and postoperative irradiation to the whole breast ( group 2 )  . 
in all patients wide excision of the tumor was performed with clear margins of minimally 35 maxillary dissection of levels i and ii was performed in all patients of group 1 . 
postoperative treatment consisted of external beam radiation therapy ( ebrt ) to the whole breast with 51 gy / 6 weeks ( 30 ( cid : 1 ) 1.7 gy equivalent to 52.254 gy icru ) for patients with invasive ductal carcinoma and 56 gy ( 33 ( cid : 1 ) 1.7 gy equivalent to 5758.8 gy icru ) for patients with invasive lobular carcinoma and subsequent external - beam electron - boost irradiation to the tumor bed with 12 gy in 2 - gy fractionation . 
after wound healing , ebrt to the whole breast with opposed tangential fields was performed with single fractional doses of 1.7 gy ( minimum target dose ) per day for 30 days , totaling 51 gy for patients with invasive ductal carcinoma , and with fractional doses of 1.7 gy per day for 33 days , totaling 56.1 gy for patients with invasive lobular carcinoma . 
included were patients with invasive breast tumors pt1 and pt2 , pn0 , pn1 , pn2 , m0 , who had breast - conserving surgery with histologically clear margins with a minimum of 35 m all patients had postoperative irradiation to the whole breast . patients in the study group ( group 2 ) received iort , patients in the control group ( group 1 ) received postoperative fractionated boost irradiation . 
iort boost versus postoperative boost in breast cancer patients complete censored intraop boost postop boost local recurrence rates and rates of distant metastases were projected by the kaplan - meier method , and the corresponding survival functions were compared with gehans wilcoxon test , cox - f - test , cox - mantel test , log - rank test and petos & petos wilcoxon test . 
patients were referred to as completed when the terminal event could be observed within the study period . however , by the end of the study period , most patients did not develop local recurrences or distant metastases , thus representing censored observations . 
in group 2 , mean and median times to the occurrence of distant metastases were 30.2 and 28 months ( 1153 months ) , respectively . seven patients died of disease , and eight patients are alive table 2 . 
awd : alive with disease ; dod : died of disease ; idc : invasive ductal carcinoma ; ilc : invasive lobular carcinoma ; ned : no evidence of disease . 
awd : lebend mit erkrankung ; dod : gestorben an der erkrankung ; idc : invasiv duktales karzinom ; ilc : invasiv lobulres karzinom ; ned : kein nachweis der erkrankung . 
 patient age ( years ) pausal status menohisto logical type grading tumor tumor number of size ( mm ) size ( pt ) positive axillary lymph nodes estrogen progesterone adjuvant time to receptor receptor therapy time to status distant local recurrence metastasis ( months ) ( months ) post post idc + ilc 2 pt1b pt1c pt1c pt1c pt1c 3 / 12 0 / 16 3 / 15 17 / 19 0 / 23 17 / 21 0 / 17 4 / 22 positive positive positive positive positive positive negative positive positive positive negative positive positive positive negative positive cmf + tam 40 strahlenther onkol 2004 no . 
iort boost versus postoperative boost in breast cancer patients complete censored intraop boost postop boost 0 6 12 18 24 30 36 42 48 54 60 66 72 78 84 90 time ( months ) figure 2 . 
even in patients with very small breast cancers ( < 1 cm ) , the local recurrence rate could be reduced from 6% in patients without irradiation to 0% in patients with postoperative radiotherapy [ 5 ]  . 
 menohisto logical type ( years ) pausal status grading tumor tumor number of size positive ( mm ) axillary lymph nodes estrogen receptor progesterone adjuvant receptor therapy status time to distant metastasis ( months ) strahlenther onkol 2004 no . 
this study as well as several others demonstrated a clear advantage in terms of local recurrences , but there was no significant advantage as regards overall survival [ 18 , 19 ]  . 
in a very recent study , the authors report the time to local recurrence to be an independent prognostic factor for breast cancer - specific survival [ 14 , 15 ]  . iort is an accepted method for the treatment of locally advanced abdominal tumors or difficult to treat brain tumors . the application of iort was restricted due to spatial distances between operating rooms and radiation facilities and due to complicated logistic problems to overcome . 
iort delivery requires either heavily shielded operating rooms , or the transport of the anesthetized patient to the radiation facility . the advent of dedicated units , which means the linear accelerator is installed in the operating room , and the availability of mobile self - shielded linear accelerators caused an increasing interest in iort and facilitated the wider use of iort . 
as a tumor bed boost , this technique has the potential to reduce local recurrence rates by avoiding topographic misses , which might be possible in conventional boost dose application . 
other factors such as tumor size , nodal status , histopathologic subtype , tumor grading , or surgical factors such as resection margins or adjuvant treatment factors have no statistically significant impact on local control . 
report that young age is an important risk factor for local recurrence and distant metastasis , while tumor size and axillary lymph node status are not related to local recurrence , but are important predictors of distant metastases [ 34 ]  . 
patients who do not live close to radiation facilities may choose mastectomy as a treatment option instead of lumpectomy if they cannot afford to travel long distances to the radiation facility [ 2225 ]  . 
we perform a dose escalation to the tumor bed of 9 gy ( 10 gy maximum target dose )  . according to the linear - quadratic model , the application of a single 9 - gy iort dose corresponds to the biological equivalent of 17 gy with respect to the acute reactions on the tumor and the normal tissue ( / ( cid : 2 ) = 10 ) , but to the biological equivalent of 26 gy with respect to the late reactions on the normal tissue ( / ( cid : 2 ) = 3 )  . 
that means that a single dose of 9 gy iort has a 1.7 - fold isoeffect on the tumor and the normal tissue according to the acute reactions and a 2.6 - fold isoeffect on the normal tissue according to the late reactions compared with fractionated radiation of 2 gy . 
our data indicate , that iort in boost modality combined with ebrt can achieve excellent local tumor control , which seems to be superior to postoperative fractionated external - beam boost irradiation . 
iort boost versus postoperative boost in breast cancer patients electrons has the advantages of high precision ( direct visualization of the tumor bed ) , good cosmesis , and high patient comfort ( reduction of the number of postoperative irradiation days )  . 
 strahlentherapie und onkologie originalarbeit nachkommen prkonzeptionell bestrahlter eltern abschlussbericht einer longitudinalstudie 19761994 und empfehlungen zur patientenberatung thomas herrmann1 , grit thiede1 , klaus - rdiger trott2 , lutz voigtmann1 ( ) hintergrund : die gute prognose einiger tumorerkrankungen im jungen erwachsenenalter fordert hufig die beratung der patienten mit kinderwunsch nach therapieende hinsichtlich der genetischen konsequenzen der strahlenbehandlung . patienten und methodik : es wird ber die ergebnisse der ber einen zeitraum von 20 jahren wiederholten untersuchungen von 61 kindern berichtet , von denen sich ein elternteil wegen einer tumorerkrankung einer alleinigen strahlentherapie ( nur in drei fllen mit zustzlicher chemotherapie ) unterziehen musste . 
die hufigsten tumorerkrankungen der 47 eltern waren lymphogranulomatose ( n = 25 ) , seminome ( n = 7 ) , schilddrsenkarzinome ( n = 3 ) und melanome ( n = 3 )  . ergebnisse : die untersuchten kinder zeigten eine neigung zur frhgeburtlichkeit ( 52 , 5% geburten vor dem errechneten geburtstermin ) bei regelrechtem geburtsgewicht und regelrechter geburtslnge . 
 schlussfolgerung : die problematik des fertilittserhalts sowie der durch die therapie ausgelsten erblich bedingten entwicklungsstrungen und erkrankungen der nachkommen sollte beim aufklrungsgesprch aktiv vom radioonkologen bei patienten entsprechenden lebensalters angesprochen werden , da wichtige entscheidungen wie kryokonservierung von sperma , ovaropexie und messung der gonadendosis whrend der bestrahlungsserie nur zu diesem zeitpunkt sinnvoll getroffen werden knnen . 
 schlsselwrter : kinder bestrahlter patienten karyotyp nach strahlentherapie tumorerkrankungen junger bestrahlungspatienten erbschden nach strahlentherapie strahlenther onkol 2004 ; 180 : 2130 doi 10.1007 / s00066 - 004 - 1223 - 4 offsprings of preconceptionally irradiated parents . 
final report of a longitudinal study 19761994 and recommendations for patients advisory background : many young adults with cancer of good prognosis seek advice from their doctors , because they are concerned about their ability to have children and about potential hereditary diseases in the children conceived or fathered after cancer therapy . patients and methods : results of repeated examinations of 61 children over a period of 20 years are reported . 
the most frequent indications for radiotherapy were hodgkins disease ( n = 25 ) , seminomas ( n = 7 ) , thyroid cancer ( n = 3 ) , and malignant melanomas ( n = 3 ) results : there was a trend to premature birth with 52.5% of the babies born before teryet , all had normal birth weight and delivery was unconspicuous . 
erbschden nach strahlentherapie conclusion : during the first consultation of young adult cancer patients , before the start of treatment , the problems of fertility and of therapy - induced mutations and hereditary diseases as well as developmental damage of the offspring need to be addressed directly by the radiation oncologist . 
the rate of radiation - induced hereditary diseases and developmental damage in the children conceived or fathered after curative radiotherapy of one parent is estimated to increase by < 0.1% ( after gonadal exposure of 1 gy )  . 
however , at present , heritable damage potentially induced by chemotherapy cannot be adequately quantified yet . key words : children of radiotherapy patients chromosome aberrations after radiotherapy tumors in young adult patients hereditary disease and developmental damage after radiotherapy einleitung durch die verbesserung der radioonkologischen heilungsergebnisse insbesondere auch bei jungen patienten sieht sich der radioonkologe im aufklrungsgesprch hufig mit der frage konfrontiert , ob und wann sich patienten nach ende einer strahlentherapie einen kinderwunsch erfllen knnen . aktuelle untersuchungen zur qualitt von aufklrungsgesprchen zeigen , dass insbesondere junge patienten hohe anforderungen an den informationsgehalt dieser gesprche stellen [ 35 , 36 ]  . 
diese arbeit soll zum einen den aktuellen kenntnisstand referieren und zum anderen ber eine longitudinalstudie berichten , in der kinder strahlenbehandelter patienten ber einen zeitraum von 20 jahren mehrfach nachuntersucht worden sind , um mgliche strahlenbedingte normabweichungen nicht nur in einer einmaligen beurteilung , sondern auch im entwicklungsverlauf erfassen zu knnen . 
whrend ber die ergebnisse der untersuchungen von 1986 in dieser zeitschrift bereits berichtet wurde [ 21 ] , sollen in der vorlie1976 1985 1993 / 94 untersuchungsjahr 1 untersuchung 2 untersuchungen 3 untersuchungen abbildung 1 . 
 genden arbeit besonders die ergebnisse der abschlieenden beurteilung der entwicklungswege von kindern prkonzeptionell bestrahlter eltern im jahr 1994 beschrieben werden . das untersuchungsspektrum , dem die kinder und eltern unterzogen wurden , ist in den vorhergegangenen berichten [ 20 , 21 ] bereits ausfhrlich dargestellt . 
es bestand neben einer grndlichen anamnese und klinischen untersuchung der kinder durch einen erfahrenen , insbesondere in der erkennung genetisch bedingter normabweichungen besonders geschulten pdiater in einem nach zustimmung der eltern durchgefhrten karporadiogramm und einem blutbild . 
deren eltern wegen zu groer anreisewege und fnf inzwischen erwachsene nachkommen prkonzeptionell bestrahlter , die in die voruntersuchungen noch einbezogen waren ( > 18 jahre ) , eine solche nachuntersuchung ab . 
in tabelle 1 und 2 werden auch die fr diese prkonzeptionell bestrahlten eltern abgeschtzten gonadendosen angegeben ( diese sind insbesondere bei den patienten , die vor 1976 bestrahlt wurden , mit einer durch die retrospektive dosisabschtzung bedingten fehlerbreite von 25% belastet [ 21 ] )  . 
 bei allen kindern bestrahlter vter wurde die paternitt mittels blutgruppengutachten ( untersuchungen 1976 und 1986 ) und dna - analyse ( 1994 ) berprin diese untersuchung wurden nur kinder aufgenommen , bei denen die vaterschaft zweifelsfrei festgestellt werden konnte . 
schwangerschaftswoche geboren ( vier eltern konnten keine angaben zur differenz zwischen errechnetem und definitivem geburtstermin machen )  . wie in den voruntersuchungen berwogen die mdchengeburten , allerdings angesichts der kleinheit der gesamtgruppe von 61 kindern mit 33 ( 54% ) weiblichen und 28 ( 46% ) mnnlichen geburten nur sehr gering . 
auch bei ermittlung von krpergewicht und krperlnge zu den drei untersuchungszeitpunkten zeigte sich , dass die kinder prkonzeptionell bestrahlter eltern nicht aus den standardabweichungswerten eines deutschen normalkollektivs ( eingetragen in die wachstumskurve der longitudinalen entwicklungsstudie bonn - dortmund nach reinken & van oost [ 32 ] ) herausfielen ( abbildungen 2 und 3 )  . 
dagegen zeigte das karporadiogramm dargestellt als differenz zwischen skelettalter und chronologischem alter ( tabelle 3 ) mit wenigen ausnahmen eine verzgerung des knochenwachstums , wobei allerdings die doppelte standardabweichung niemals unterschritten wurde . 
 diagnose anzahl alter zur therapiegonadendosis zeit ( jahre ) ( gy ) morbus hodgkin schilddrsenkarzinom 3 wilms - tumor melanom knochentumor tonsillenkarzinom nhl rechte leiste 1533 18 , 22 und 32 1 und 32 19 und 19 6 und 15 0 , 13 , 0 0 , 15 , 0 , 12 und 0 , 38 0 , 4 / 3 , 5 und 1 , 6 / 2 , 0 0 , 06 und 0 , 15 0 , 05 und 0 , 02 0 , 15 2 , 0 links , 8 , 0 rechts 133 0 , 022 , 0 a drei patientinnen erhielten zustzlich eine chemotherapie tabelle 2 . 
nhl : non - hodgkins lymphoma . diagnose anzahl alter zur therapiegonadendosis zeit ( jahre ) ( gy ) morbus hodgkin seminom melanom kleinhirntumor osteochondrosarkom 1 1732 2335 1035 0 , 010 , 3 0 , 21 , 4 0 , 05 0 , 05 0 , 011 , 4 doch , dass diese differenzen zu den unterschiedlichen untersuchungszeitpunkten sehr variierten . 
das durchschnittliche menarchealter bei 17 mdchen wich mit 13 , 3 1 , 2 jahren von dem von starke 1986 [ 41 ] fr ostdeutsche mdchen ermittelten wert von 13 , 1 jahren nicht wesentlich ab . 
dabei fallen neben einer schweren fehlbildung im handbereich eine angeborene taubheit , eine innenohrschwerhrigkeit sowie eine einseitige blindheit als besondere , die lebensqualitt einschrnkende normabweichung auf . ebenfalls auffllig ist die groe anzahl von hernien ( 16 hernien bei 13 kindern [ 21 , 3% ] ) bei den untersuchten kindern . 
erbschden nach strahlentherapie die 1994 erstmals durchgefhrten ultraschalluntersuchungen des retroperitonealraums zeigten bei allen 47 kindern keine angeborenen fehlbildungen . lediglich in einem fall wurde eine urethralklappe mit nachfolgender blasenwandhypertrophie entdeckt und einer operation zugefhrt . 
auer einer nabelhernie und einem wolff - parkinson - white - ( wpw - ) syndrom im ekg bei einem mdchen waren alle brigen befunde sowie der karyotyp dieser enkel prkonzeptionell bestrahlter eltern unauffllig . 
 der besondere fall eine patientin wurde wegen eines 1962 diagnostizierten non - hodgkin - lymphoms ( damals als morbus brill - symmers klassifiziert ) im alter von 17 jahren im bereich der rechten leiste unter rntgentiefentherapiebedingungen bestrahlt . 
bereits bei der ersten untersuchung 1976 wurde die besonderheit dieses falls deutlich , da zwei nicht lebensfhige frhgeborene ( trisomie e mit herzvitium und multiplen fehlbildungen , atemnotsyndrom bei frhgeburt ) die annahme einer radiogen induzierten genetischen schdigung bei hoher ovarialdosis nahe legten . 
krperhhe und - gewicht der mdchen im alter von 518 jahren zu allen drei untersuchungszeitpunkten , eingetragen in die wachstumskurve der longitudinalen entwicklungsstudie bonn - dortmund ( nach 32 ] )  . 
height and body weight of girls aged 518 years , measured during the three examinations in comparison with the growth curve of normal german girls determined in the longitudinal development study bonn - dortmund [ 32 ]  . 
 die beschriebene patientin hatte jedoch vor den schwer geschdigten , nicht lebensfhigen frhgeburten im jahre 1969 also 7 jahre nach der strahlentherapie bereits ein im phnotypus gesundes mdchen entbunden , das zu allen drei untersuchungszeitpunkten beurteilt wurde und eine krperlich und geistig vllig normale entwicklung zeigte . 
bei der 1994 erstmals durchgefhrten chromosomenanalyse dieser jungen frau in high - resolution banding - technik zeigten sich normabweichungen an den chromosomen 5 und 17 mit strahlenther onkol 2004 no . 
dabei fiel auf , dass die schwester des verstorbenen vaters der probandin ( tod an magenblutung bei dauermedikation mit antirheumatika wegen morbus bechterew ! ) ein kind mit katzenschreisyndrom geboren hatte , das nach 2 wochen verstarb . 
der karyotyp dieses kindes war am institut fr klinische genetik der universitt leipzig mit 46 , xx - 5 , + der ( 5 ) ( 17 q 23 ; 5p 13 - qter ) bestimmt worden . 
die sich darauf anschlieende zytogenetische untersuchung der mutter dieses kindes ( und schwester des vaters unserer probandin ) erbrachte 46 , xx , t ( 5 ; 17 ) ( p 13 ; q 23 )  . 
 die angegebenen bruchpunkte weichen nur minimal von denen ab , die bei unserer probandin bestimmt werden konnten , so dass das vorliegen einer vom grovater vterlicherseits vererbten familiren translokation 5 ; 17 angenommen werden muss . 
die meisten patienten , deren nachkommen untersucht werden konnten , waren an zwei neoplastischen erkrankungen mit typischer manifestation im frhen erwachsenenalter erkrankt : der lymphogranulomatose und dem semino diese beobachtung wird auch von vielen anderen autoren gemacht [ 1 , 4 , 40 ]  . alle brigen malignen erkrankungen des frhen erwachsenenalters sind entweder selten , oder ihre prognose ist sehr abbildung 3 . 
krperhhe und - gewicht der jungen im alter von 518 jahren zu allen drei untersuchungszeitpunkten , eingetragen in die wachstumskurve der longitudinalen entwicklungsstudie bonn - dortmund ( nach [ 32 ] )  . 
height and body weight of boys aged 518 years , measured during the three examinations in comparison with the growth curve of normal german boys determined in the longitudinal development study bonn - dortmund [ 32 ]  . 
 eltern , die als kinder an einem malignen tumor erkrankt waren , stellen angesichts der guten therapieergebnisse bei kindlichen neoplasien [ 24 , 25 , 43 ] eine in zukunft bedeutsame in der vorliegenden untersuchung nicht erfasste pastrahlenther onkol 2004 no . 
es empfiehlt sich deshalb bei der genannten patientengruppe , bei der im aufklrungsgesprch die frage des spteren kinderwunsches ventiliert wird , whrend der strahlentherapieserie dosimetrische kontrollmessungen durchzufhren , um aus radiotherapeutischer sicht ausreichend gesttzte aussagen zur fertilitt und zum genetischen risiko treffen zu knnen [ 19 ]  . 
2001 [ 37 ] zu der aussage , dass die beim hodentumor angewandte chemotherapie mit cisplatin , cyclophosphamid und procarbazin mit zunehmender kumulativer dosis auch die infertilittsrate ansteigen lsst und dass aus unkenntnis der fertilittssituation des mannes vor therapiebeginn vorausschauende aussagen schwierig sind . 
als prognostisch gnstige kriterien fr den erhalt der ovarialfunktion ergaben sich ein alter < 25 jahre zum therapiezeitpunkt , eine ovardosis < 5 gy und ein verzicht auf eine chemotherapie . 
 [ 10 ] haben 1991 ber hodgkin - patientinnen berichtet , bei denen laterale und mediale ovaropexien erfolgt waren . nur bei 8 / 13 patientinnen konnte eine erhaltene ovarialfunktion in endokrinologischen tests besttigt werden , und nur eine patientin wurde mutter eines gesunden kindes . 
zusammenfassend ist also die wahrscheinlichkeit des erhalts der ovarialfunktion bei an morbus hodgkin erkrankten patientinnen , die infradiafragmal bestrahlt werden , auch nach ovaropexie nicht sonderlich hoch insbesondere wenn eine zustzliche chemotherapie erfolgen muss . 
 anomalien anzahl der kinder trisomie der e - gruppea spalthnde , spaltfe , dysplastischer hoden , ohrmuscheldysplasie , gebissanomalie einseitige blindheit angeborene einseitige taubheit atemnotsyndrom ( bei frhgeburt ) a innenohrschwerhrigkeit fehlbildung des m . 
erbschden nach strahlentherapie generell ist die fertilitt von patienten mit durchgemachter tumorerkrankung um 15% verringert [ 30 ] , wobei mnner nur 76% der fertilitt einer unbehandelten vergleichspopulation erreichen , wohingegen frauen sich von einer gleich alten , nicht an krebs erkrankten gruppe nicht wesentlich unterscheiden . 
so sind beim mann bei kumulativen dosen > 1 , 5 gy und bei der frau allerdings sehr altersabhngig > 5 , 0 gy schwere einschrnkungen der fertilitt zu erwarten . 
bezieht man allerdings alle mindestens 10 tage vor dem errechneten geburtstermin geborenen kinder unserer untersuchung mit ein , ergibt sich mit 52 , 5% eine frhgeburtlichkeit , die jedoch offensichtlich ohne bleibende folgen fr die entwicklung der kinder ist . 
diese entwicklung , die in unserer untersuchung bei vielen probanden erstmals ber die gesamte kindheit verfolgt werden konnte , zeigte hinsichtlich krpergewicht und krperlnge sowohl bei mdchen als auch bei jungen keine abweichungen von normalkollektiven , deren eltern nicht bestrahlt worden waren . 
 [ 4 ] an 2 198 kindern bestrahlter eltern im vergleich zu 4 544 kindern nicht bestrahlter geschwister der krebspatienten lie sich keine eindeutige zuordnung des geschlechts der kinder zur abbildung 4 . 
angesichts der deutlich hheren gonadendosis bei unseren patienten im vergleich zu arbeitern in kernkraftwerken , wo ein solcher zusammenhang konstruiert wurde [ 9 ] , muss bei der gegenwrtigen datenlage eine verbindung zwischen prkonzeptioneller bestrahlung der eltern und neoplasierisiko der nachkommen bezweifelt werden [ 46 ]  . 
erbschden nach strahlentherapie gewandte verfahren der skelettalterbestimmung vergleich eines rntgenbildes der hand des probanden mit den bildern des atlasses von greulich & pyle [ 13 ] , die von amerikanischen kindern stammen kann per se bereits eine diskrete fehleinschtzung liefern , da bekannt ist , dass deutsche kinder durchschnittlich 6 monate gegenber ihren amerikanischen altersgenossen im skelettalter zurckbleiben [ 26 , 42 ]  . 
fr die annahme einer zuflligen abweichung in der longitudinalstudie spricht zudem , dass scheinbare knochenwachstumsdefizite bei abschluss der knochenreifung aufgehoben waren , die abweichung nach unten nie die grenzen ( 2s ) der deutschen longitudinalen entwicklungsstudie [ 32 ] verlie und individuell zu den verschiedenen untersuchungszeitpunkten erhebliche schwankungen bei gleichen individuen registriert werden konnten . 
im gegensatz dazu kommen die meisten neueren arbeiten zu dem schluss , dass es bisher keinen hinweis darauf gibt , dass eine prkonzeptionelle bestrahlung das risiko genetisch bedingter fehlbildungen bei den nachkommen erhht . 
 [ 1 ] besttigten diese aussage beim vergleich von kindern von hodgkin - patienten mit einer elternschaft vor ( 135 schwangerschaften ) oder nach der therapie ( 84 schwangerschaften ) sowie mit vergleichsdaten der allgemeinen bevlkerung . 
 [ 4 ] die ergebnisse der five center study des national cancer institute der usa , in der 2 198 nachkommen von tumorpatienten mit unterschiedlichen therapien ( einschlielich radiotherapie ) mit 4 544 kindern ihrer geschwister verglichen wurden . 
besonders aussagekrftig ist die eingebaute fallkontrollstudie ( nested case - control study ) ber 2 198 kinder von 1062 berlebenden krebspatienten , wobei 235 eltern eine als potentiell mutagen eingestufte strahlentherapie des abdomens und des beckens und / oder eine chemotherapie mit alkylierenden substanzen erhalten hatten . 
das risiko , an einer sporadischen , d.h. einer neuen , potentiell durch die therapie induzierten einzelgenerkrankung whrend der kindheit und der adoleszenz zu erkranken , war bei den kindern der mit mutagenen bzw . 
da die studie so angelegt war , dass sie eine verdoppelung der hufigkeit erblich bedingter erkrankungen mit 90%iger sicherheit signifikant htte nachweisen knnen , zogen die autoren den schluss , dass weder die krebserkrankungen der eltern als solche noch ihre erfolgreiche behandlung unter einschluss von strahlentherapie und / oder chemotherapie mit alkylierenden substanzen zu einer zur besorgnis anlass gebenden ( signifikanten ) erhhung der rate erblich bedingter fehlbildungen oder krankheiten fhrt . 
90 000 kanadischen kindern mit einer kongenitalen anomalie die hufigkeit des auftretens von krebserkrankungen und einer strahlentherapie des abdomens oder einer chemotherapie und verglichen diese zahlen mit denen von 90 000 eltern gesunder kanadischer kinder . 
in beiden gruppen waren krebserkrankung und therapie der eltern etwa gleich verteilt , so dass die autoren zu der schlussfolgerung kommen , dass das risiko einer kongenitalen anomalie unter den lebend geborenen nachkommen nicht von der krebserkrankung oder deren therapie abhngt . 
 im lichte dieser ergebnisse erscheinen die beschriebenen normabweichungen bei 35 der 61 kinder ( 57% ) unseres untersuchungsguts trotz unaufflligen karyotyps aller kinder ( mit ausnahme des besonderen falls ) ungewhnlich hoch , wobei die hernien mit 21 , 3% einen besonderen stellenwert einnehmen . 
allerdings handelt es sich dabei stets um untersuchungen zu einem stichtag und nicht , wie in unserer studie , um longitudinaluntersuchungen , in der die kinder teilweise zu drei untersuchungszeitpunkten naturgem auch eine hhere rate an normabweichungen erkennen lassen . 
betrachtet man nur die in tabelle 4 aufgefhrten kinder mit gravierenden angeborenen fehlbildungen ( unter auerachtlassung der nicht lebensfhigen frhgeburten ) , so sind 4 / 61 ( 6 , 5% ) zu konstatieren . 
 [ 4 ] ermittelten 3 , 4% . zusammenfassend bleibt festzustellen , dass in der beratung junger tumorpatienten mit kinderwunsch auf das sehr kleine , aber nach unserer einschtzung theoretisch vorhandene risiko einer leichten erhhung von erblich bedingten erkrankungen und fehlbildungen unter den nachkommen hinzuweisen ist . 
dabei muss auch bercksichtigt werden , dass die durch manche zytostatika induzierten mutationen hufig punktmutationen sind , die ein weitaus greres genetisches risiko bedingen als die ausgedehnten deletionen , die charakteristische folge einer bestrahlung sind und in der regel zum sehr frhen abort des conceptus fhren . 
 so anschaulich und fr viele rzte und patienten berzeugend die ergebnisse unserer wie auch der anderen hier zitierten studien sein mgen , eine wissenschaftlich fundierte beratung kommt nicht umhin , die ergebnisse der strahlengenetischen forschung und risikoberlegungen , wie sie vor allem von sankaranarayanan [ 34 ] und im bericht der vereinten nationen [ 44 ] verffentlicht worden sind , in das gesprch einzubeziehen . 
dabei wird von der hufigkeit ( inzidenz ) erblich ( mit ) bedingter erkrankungen in der bevlkerung ausgegangen , die durch mutationen im erbgut hervorgerufen werden . wenn multifaktoriell bedingte erkrankungen mit starker genetischer komponente , die sich erst im erwachsenenalter manifestieren , wie diabetes , bluthochdruck etc . 
unter den direkten nachkommen , kindern und enkeln , von eltern , die einem mutagen wie strahlung oder zytostatika ausgesetzt waren , ist jedoch nur mit einer erhhung der rate solcher durch ein einziges gen bedingter erkrankungen und fehlbildungen zu rechnen , die einem dominanten ( oder geschlechtsgebunden rezessiven ) erbgang folgen , denn die mutationskomponente ( mutation component [ mc ] nach sankaranarayanan [ 34 ] ) der anderen erblich bedingten erkrankungen liegt um grenordnungen niedriger . 
durch eine fraktioniert gegebene strahlendosis an den gonaden von 1 gy zu erwarten ist , sich die rate von erkrankungen mit dominantem erbgang nicht auf das doppelte erhht , sondern nur um 15% relativ bzw . 
whrend punktmutationen , wie sie fr manche zytostatika charakteristisch sind , praktisch zu 100% vererbbar sind ( ausgedrckt durch einen bewertungsfaktor , den potential recoverability correction factor [ prcf ] nach sankaranarayanan [ 34 ] , von 1 ) , liegt der prcf fr strahleninduzierte mutationen bei 0 , 3 . 
dieser wert ist so klein , dass bei den in der klinischen strahlentherapie vorkommenden gonadendosen der epidemiologische nachweis einer erhhten rate erblich bedingter entwicklungsstrungen und erkrankungen auch in sehr umfangreichen kohortenstudien und fallkontrollstudien nicht mglich ist , was mit den von uns und anderen autoren berichteten studien bereinstimmt . 
 zur beratung vor geplanter strahlentherapie im aufklrungsgesprch mit jungen krebspatienten sollten das thema des fertilittserhalts und die problematik von durch die therapie ausgelsten erblich bedingten entwicklungsstrungen und erkrankungen knftiger kinder aktiv vom radioonkologen angesprochen werden . 
dies ist weniger damit zu begrnden , dass es in dieser zeit zur teilweisen elimination von geschdigtem genmaterial kommen kann ( vor allem von dominanten letalmutationen , die fr die verminderte fertilitt in der ersten zeit nach therapie verantwortlich sind )  . 
nach diesem zeitraum von maximal 18 monaten sollte allerdings den patienten zur baldigen erfllung eines kinderwunsches geraten werden , da ansonsten die vernderungen des genetischen materials durch das zunehmende alter der eltern einen weitaus hheren stellenwert einnehmen knnten als durch prkonzeptionelle bestrahlung jemals denkbar . danksagung die autoren danken e . 
1 urban & vogel strahlentherapie und onkologie original article study on the tongue and groove effect of the elekta multileaf collimator using monte carlo simulation and film dosimetry freddy haryanto , matthias fippel , annemarie bakai , fridtjof nsslin1 background : nowadays , multileaf collimation of the treatment fields from medical linear accelerators is a common option . 
due to the design of the leaf sides , the tongue and groove effect occurs for certain multileaf collimator applications such as the abutment of fields where the beam edges are defined by the sides of the leaves . 
 material and methods : in this study , the tongue and groove effect was measured for two pairs of irregular multileaf collimator fields that were matched along leaf sides in two steps . 
measurements were made at 10 cm depth in a polystyrene phantom using kodak edr2 films for a photon beam energy of 6 mv on an elekta sli - plus accelerator . 
in the simulations , the design of the leaf sides was taken into account and one component module of beam code was modified to correctly simulate the elekta multileaf collimator . 
 key words : tongue and groove effect multileaf collimator monte carlo simulation strahlenther onkol 2004 ; 180 : 5761 doi 10.1007 / s00066 - 004 - 1135 - 3 untersuchung des nutund feder - effekts des elekta - lamellenkollimators mittels monte - carlo - simulation und filmdosimetrie hintergrund : heutzutage werden zunehmend lamellenkollimatoren fr die kollimierung von strahlenfeldern eingesetzt . 
dieser effekt ist besonders bedeutsam , wenn feldanschlsse zweier felder bei einer bestrahlung vorgesehen sind . material und methodik : zur untersuchung dieses effekts wurden zwei konfigurationen mit unregelmigen paarfeldern eingesetzt . 
die messungen erfolgten in einem polystyrol - phantom mit kodak - edr2 - filmen bei 6 - mv - photonenstrahlung an einem elekta - linearbeschleuniger ( sli - plus )  . 
 schlsselwrter : nut - und - feder - effekt lamellenkollimatoren monte - carlo - simulation introduction for several years , the computer - controlled multileaf collimator has replaced compensators for conformal radiation therapy . 
step - and - shoot and the dynamic multileaf collimator are two well - known techniques based on the multileaf collimator and are used to deliver intensity - modulated radiotherapy [ 3 , 12 ]  . 
at the tbingen university hospital , germany , the former of these techniques ( step - and - shoot ) is used with an elekta sli - plus linac equipped with the elekta multileaf collimator . 
many researchers have investigated the aspects of 1 department of medical physics , radiooncologic university clinic , tbingen , germany . received : december 12 , 2002 ; accepted : september 29 , 2003 strahlenther onkol 2004 no . 
in this convention , the coordinate system is based on the collimators coordinate syste in a first stage , the electron beam was modeled as a point source with 2 mm diameter at the surface of the target , and its energy has a spectrum with normal distribution . 
 the dosxyz [ 8 ] code was employed to simulate the measurements which were done in a polystyrene phantom . the second phase space file was used as input for this simuharyanto f , et al . 
one of these aspects , the tongue and groove effect , may become a significant issue when underdosage occurs in the region of overlap of two leaf pairs of a multileaf collimator [ 10 , 13 , 16 ]  . 
the results of several investigations show that synchronization of the leaves can avoid the tongue and groove effect [ 11 , 14 ] , but increases the total number of monitor units needed to deliver the required dose . 
the projection of the leaf pitch in the isocentric plane is 1.0 cm , but the projection of an individual leaf is 1.1 cthe elekta multileaf collimator is placed 29.8 cm below the target and has a thickness of 7.5 cmore detailed information of the elekta multileaf collimator can be found in the papers by jordan & williams [ 7 ] and sykes & williams [ 10 ]  . 
the parameters required to describe the leaf are : the width of leaves ( lw ) , the dimensions of the leaf gap ( lg ) , and the tongue and groove mechanism ( wg and wt ; figure 1 )  . 
 monte carlo simulation the 6 - mv photon beam of the elekta sli - plus was modeled using the beam prograa detailed model of this beam can be found in previous papers [ 4 , 5 ]  . 
design of the elekta multileaf collimator , described by the parameters : tongue width ( wt ) , groove width ( wg ) , leaf gap ( lg ) , and leaf width ( lw )  . 
the voxel size was 0.2 cm perpendicular to the leaf motion direction for overlap regions and 0.5 cm for other regions , 1 cm in direction of the leaf motions , and 1 cm high . the medium of voxels was set to the medium of polystyrene phanto measurement of the tongue and groove effect to reproduce the tongue and groove effect , two pairs of irregular fields were generated . 
the first irregular field of this pair is the half of a 20 ( cid : 1 ) 20 cm area that was blocked with the leaves of the left leaf bank , with the leaf ends at overtravel position of 10 cthe leaf ends of the leaves of the right leaf bank were set at 11 cm from the central axis . 
in the second field , only the leaf positions of the left leaf bank were changed . all leaves of the left leaf bank which were opened in the first field are closed in the second field and vice versa . 
in the first field , every alternate group of two leaves from the left bank was set to cross the central axis by 10 cm and the other leaves were set 11 cm from the central axis . 
the second field is the complement of the leaf configuration of the first field . using this pair of irregular fields , the tongue and groove effect was investigated for nine overlap regions between leaves 1213 , 1415 , 1617 , 1819 , 2021 , 2223 , 2425 , 2627 , and 2829 . 
 the tongue and groove effect was investigated by measurements with kodak edr2 films in a polystyrene phantom . measurements were performed at an elekta sli - plus with a 6mv photon beathe films were placed at a depth of 10 cm below the phantom surface with a source - to - phantom - surface distance of 90 call films were exposed to the same number of monitor units for each irregular subfield of the pair leaf configurations . 
the films were developed with a protec m45 film processor and scanned using the vidar vxr - 12 film digitizer with a pixel size of approximately 0.339 m results and discussion figure 4 shows a comparison of measured and simulated profiles for the first pair of irregular subfields . 
 there are no obvious differences in measurements and simulations of the peak deficit and its full - width at half - maximum at the same overlap region between the two pairs of the irregular fields . 
there will also be photon scattering and electron effects within the irradiated mediu conclusion in this study , the monte carlo simulation accurately reproduces the measured underdosage at overlap regions due to tongue and groove effect , if detailed information of the leaf side design is taken into account . 
this paper investigates whether exit dose measurements and evaluations of the optical density of portal films can be used to verify the energy of the electron beam in a clinically relevant setting . 
 material and methods : during irradiation of the head and neck region of an alderson - rando phantom with 6to 21 - mev electron beams , the exit dose rates behind the phantom and the dose rates at the position of a film cassette were measured . 
the optical density of films ( ec film / ec - l regular and ec - l fast cassettes , eastman kodak comp . , rochester , ny , usa ) exposed to beams of different energies was evaluated . 
due to its density behavior , the film with both types of cassettes failed to generate images for lower electron energies ( 6 and 9 mev ) but presented a strong ascent of the optical density until reaching the saturation with increasing electron energy . conclusion : measurements of the exit dose and evaluations of the optical density of portal films can be used to verify and document the energy of electron beams during radiotherapy . 
 key words : radiotherapy quality assurance electron beams energy verification photon contamination exit dose port film strahlenther onkol 2004 ; 180 : 625 doi 10.1007 / s00066 - 004 - 1172 - y in - vivo - verifikation der elektronenenergie mittels der austrittsdosis am patienten und der optischen dichte von filmen hintergrund und ziel : der tiefendosisverlauf von elektronenfeldern wird hauptschlich durch deren energie bestimmt . 
die vorliegende arbeit untersucht die eignung von messungen der austrittsdosis und der auswertung der optischen dichte von verifikationsfilmen zur energiekontrolle von elektronenfeldern in einem klinikrelevanten ansatz . material und methodik : bei der bestrahlung der halsregion eines alderson - rando - phantoms mit elektronen der energien von 6 bis 21 mev wurden die austrittsdosisleistung hinter dem phantom und die dosisleistung an der position einer filmkassette gemessen . 
die optische dichte von portfilmen ( ec - film / ec - l regular - und ec - l fast - kassetten , eastman kodak comp . , rochester , ny , usa ) , die mit den feldern der verschiedenen energien bestrahlt wurden , wurde ermittelt . 
wegen seiner belichtungscharakteristik ist der film mit beiden kassettentypen nicht zur bildgebung bei geringen elektronenenergien ( 6 und 9 mev ) geeignet , zeigt aber ansonsten einen starken anstieg der optischen dichte mit zunehmender elektronenenergie bis zum erreichen der sttigung . 
 schlsselwrter : strahlentherapie qualittssicherung elektronenfelder energieverifikation photonenkontamination austrittsdosis portfilm introduction the use of electron beams in radiotherapy offers the advantage of a steep decrease of dose beyond its maximum , thereby sparing organs at risk that are located deeper than the target volume [ 9 , 10 , 14 , 19 ]  . 
in principle , this verification is possible using 1 department of radiotherapy and radiooncology , university hospital carl gustav carus , technical university dresden , germany , 2 department of radiooncology and radiotherapy , clinical center darmstadt , germany . 
in vivo verification of electron energy the contaminant photons that are mainly generated as bremsstrahlung in the first scatter foil of the accelerator [ 6 , 18 , 21 , 23 ]  . 
as only the bremsstrahlung photons but not the electrons may transverse the patient , measurement of the exit dose behind the patient should be a measure of the electron energy of the beafurthermore , the photon contamination can be used to create images of the electron portals [ 3 , 5 , 7 , 12 , 13 ]  . 
therefore , evaluation of the optical density of the irradiated film , in theory , should reflect the electron energy of the bea the present study investigates whether exit dose measurements and measurements of the optical density of verification films can be used to verify and document the energy of electron beams in a clinically relevant setting . 
although in modern linear accelerators the electron energy is verified by computerized record - and - verify systems , there are two reasons for the use of the proposed measurements . 
first , the exit dose is , on a physical basis , directly related to the electron energy and to the scatter foils , whereas record - and - verify systems use electronic readings of accelerator parameters . 
 material and methods simulating a common clinical application , the head and neck region of an alderson - rando phantom was irradiated with electron beams of nominal energies of 6 , 9 , 12 , 15 , 18 , and 21 mev using a primus accelerator ( siemens medical solutions , erlangen , germany )  . 
the beam was shaped to a circle . for this , a 5 cm diameter aperture ( 1 cm mcp - 96 alloy ) was inserted into a customized ( 10 ( cid : 1 ) 10 cm2 ) electron tube . 
for comparison to other accelerators , rp values are given in table 1 . during irradiation the exit dose rate in the center of the beam was measured using an ionization chamber ( chamber type 31003 , sensitive volume 0.3 cm3 , unidos dosemeter , ptw freiburg , germany )  . 
the distance of the exit point to the focus was 117 cthe diameter of the phantom in the field was sufficient to prevent any contribution of the primary electrons to the exit dose even for the highest electron energy . 
the cassette was attached to the treatment table perpendicular to the beam direction with a distance between the cassette surface and the focus of 137.5 cfor the measurements of the dose in the film plane , the cassette was replaced by an rw - 3 plate with a thickness of 2 cm containing a drilling for the ionization chamber . 
the highly sensitive filmcassette combinations ( ec film / ec - l regular and ec - l fast cassette , eastman kodak corp . , rochester , usa ) [ 8 ] were exposed with 180 monitor units ( mu ) using electron beams of six different energies . 
the optical density of each image was measured in the center of the beam ( digital densitometer ii , typ 07 - 424 , cardinal health , cleveland , oh , usa )  . 
 for the monitor units applied , the dose of contaminant photons was not sufficient to generate images of the 6 - , 9 - , and 12 - mev electron beams for the ec - l regular cassette and of the 6and 9 - mev electron beams for the ec - l fast cassette ( table 1 )  . 
practical electron ranges rp ( source - surface distance 100 cm , beam size 25 ( cid : 1 ) 25 cm2 ) , measured exit and cassette dose rate values ( beam size 10 ( cid : 1 ) 10 cm2 , 5 cm diameter aperture ) , and optical densities ( including fog density of 0.19 ) in the center of the aperture of films exposed to 180 monitor units ( mu )  . 
different nominal electron energies enom were studied using a primus accelerator , the ec film , and two different types of cassettes ( ec - l regular and ec - l fast )  . 
praktische elektronenreichweite rp ( fokus - oberflchen - abstand 100 cm , feldgre 25 ( cid : 1 ) 25 cm2 ) , gemessene austrittsund kassettendosisleistung ( feldgre 10 ( cid : 1 ) 10 cm2 , apertur mit 5 cm durchmesser ) und optische dichte ( einschlielich der dichte 0 , 19 von schleier und unterlage ) im mittelpunkt der kreisapertur auf dem film bei belichtung mit 180 monitoreinheiten ( mu )  . 
verification films of a patient with a carcinoma of the submandibular gland treated with two lateral opposing 6 - mv photon beams sparing the spinal cord and dorsally abutted electron beams . 
the electron beams were applied with a source - skin distance of 115 cm using a ( 10 ( cid : 1 ) 10 cm2 ) electron tube with an mcp - 96 aperture . 
due to different diameters of the involved lymph nodes , a 9 - mev electron beam was applied from the left ( a ) and a 12 - mev electron beam from the right ( b ) side of the patient . 
die elektronenfelder wurden mit einem fokus - haut - abstand von 115 cm und einer apertur innerhalb des ( 10 ( cid : 1 ) 10 cm2 groen ) elektronentubus bestrahlt . 
wegen unterschiedlicher durchmesser der befallenen lymphknoten wurden von links ein 9 - mev - elektronenfeld ( a ) und von rechts ein 12 - mev - elektronenfeld ( b ) eingestrahlt . 
the further increase of the optical density led to an overexposure inside the aperture circle starting at 15 mev electron energy for the ec - l fast cassette and at 18 mev for the ec - l regular cassette . 
this is demonstrated in figure 1a and b showing port films of a patient with a carcinoma of the submandibular gland , who was treated with a 9 - mev electron beam from the left and a 12 - mev electron beam from the right side . 
 discussion in the present investigations , the measurements of the exit dose were sensitive enough to allow detection of radiation with an incorrect preset value of the electron energy or an incorrect combination of energy value and scatter foil . 
however , it should be noted that the specific values measured in this study apply only to the investigated accelerator with its specific combination of electron energies and scatter foil parameters . 
neglecting the minor amount of photons that are created by the electrons in the upper tissue layers [ 18 , 20 ] , the corrections for these parameters can be performed in the same manner as for primary photon beams based on the energy of the photon contamination [ 4 ]  . 
for example , for a 9 - mev electron beam a modification of 1 cm in the diameter of the patient leads to a change of the exit dose of about ( 5...8 ) % , if the diameters are in the range between 10 and 15 ca variation of the source - skin strahlenther onkol 2004 no . 
for some accelerators the difference in the photon contamination in electron beams of different energy may be lower or in the same order as the patient - related changes in the exit dose . 
 due to the high sensitivity of the ec film with the investigated types of cassettes , only a small dose interval exists for optimal exposure , i.e. , optical densities between 0.81.6 ( including the fog density )  . 
under the processing conditions applied here and in the case of 15 - mev electrons , this dose interval at the cassette entrance side was ( 11...15 ) mgy for the ec - l regular cassette and ( 8...12 ) mgy for the ec - l fast cassette [ 3 ]  . 
in the case of the 9and 12 - mev electrons , the use of the ec - l fast cassette instead of the ec - l regular cassette resulted in a higher optical density leading to evaluable images ( table 1 , figure 1 )  . 
starting with the 15 - mev electron beam in case of the ec - l fast and the 18 - mev electron beam for the ec - l regular cassette , the optical density of the film saturated . 
in this situation , exposure of the film has to be terminated after an adequate number of monitor units . film verification will fail , if the dose at the film plane is < 8 mgy . this is generally the case for 6 - mev electron beams . 
 under constant exposure and processing conditions , the optical density and , thereby , the quality of the image depend on the electron energy ( figure 1a and b )  . 
an advantage of the film verification compared with the exit dose measurements is that the distance between source and cassette is constant even when the diameter of the patient changes . 
 conclusion for the accelerator investigated , exit dose measurements and the evaluation of the optical density of verification films can be used to verify and document the energy of the electron beams . 
 strahlentherapie und onkologie original article primary radiotherapy of stage iia / biiib cervical carcinoma a comparison of continuous versus sequential regimens rpd mayer1 , csaba nemeskri1 , csaba petnehzi1 , gbor borgulya2 , szilvia varga1 , attila naszly1 background : comprehensive literature on cervical cancer demonstrates , even today , the need for optimization of the timing of external - beam radiotherapy ( ebrt ) and high - dose - rate brachytherapy ( hdr - bt ) in the treatment of stage iia / biiib cervical carcinoma . 
two regimens were compared : sequential radiation therapy ( srt ) with 4 ( cid : 1 ) 8 gy hdr - bt to point a followed by ebrt , and continuous radiation therapy ( crt ) in which 5 ( cid : 1 ) 6 gy hdr - bt to point a , one session per week , was integrated into the ebrt . 
nevertheless , this difference was not statistically significant ( p = 1.00 ) , and the same was found in a subgroup analysis of the different tumor stages , showing , however , an unequivocal trend . 
 conclusion : for the patients included in this study , no advantage has been found so far in using crt , i.e. , shortening the ott by weekly integration of hdr - bt into ebrt . 
to achieve a significant improvement in local control and disease - free survival ( dfs ) as well as overall survival ( os ) , the combination with modern chemotherapy regimens and regional deep hyperthermia may rather be the treatment option . 
 key words : cervical cancer high - dose - rate brachytherapy sequential regimen continuous regimen overall treatment time locoregional control late side effects strahlenther onkol 2004 ; 180 : 20915 doi 10.1007 / s00066 - 004 - 1122 - 8 primre strahlentherapie des zervixkarzinoms im stadium iia / biiib . 
zwei kombinierte strahlentherapieregime wurden verglichen : eine sequentielle therapie ( srt ) mit 4 ( cid : 1 ) 8 gy hdr - bt am punkt a , gefolgt von ebrt , und eine kontinuierliche therapie ( crt ) , bei der die wchentliche hdr - bt mit 5 ( cid : 1 ) 6 gy am punkt a in die ebrt integriert war . 
 1 center of oncoradiology , uzsoki hospital , budapest , hungary , 2 national pediatric cancer registry of the hungarian pediatric oncology working group , 2nd department of pediatrics , semmelweis university budapest , hungary . received : november 21 , 2002 ; accepted : january 22 , 2004 strahlenther onkol 2004 no . 
primary radiotherapy of cervical carcinoma ergebnisse : das progressionsfreie 5 - jahres - berleben ( dfs ) betrug in der crt - gruppe 71% und in der srt - gruppe 56% . 
die sptfolgen am rektum waren bei srt statistisch signifikant hufiger als bei crt ( 35 patienten bei srt und 18 patienten bei crt ; p = 0 , 037 )  . 
 schlussfolgerung : bisher ist in dem hier vorgestellten patientengut kein gnstiger effekt der crt mit wchentlich in die ebrt integrierter hdr - bt und verkrzter ott nachweisbar ; es besteht lediglich ein trend . 
 schlsselwrter : zervixkarzinom high - dose - rate - brachytherapie sequentielles regime kontinuierliches regime gesamtbehandlungszeit lokoregionre kontrolle sptfolgen introduction in the past , there was general agreement that radiotherapy alone should be used to treat advanced cervical cancer . 
exclusive radiotherapy mostly consists of combinations of external - beam irradiation ( ebrt ) to the pelvis followed by brachytherapy , but in some cases , the reverse sequence of therapeutic modalities is applied [ 10 ]  . 
 over the last decade , high - dose - rate brachytherapy ( hdr - bt ) has increasingly been used for the treatment of cervical cancer without consensus on fractionation guidelines [ 18 ]  . 
as an example , hdr - bt can be divided in four to eight fractions , given after or concurrently with the course of ebrt , in an attempt to reduce the tumor cell repopulation by shortening the overall treatment time ( ott ) [ 5 , 14 ]  . 
showed that prolongation of ott to > 55 days resulted in decreased survival and decreased pelvic control for all stages , but also stated that the optimal fractionation schedule for treating cervical cancer using hdr - bt is still unknown [ 19 , 20 ]  . 
found that the time intervals between external and intracavitary irradiation and the ott were the prognostic factors with the highest significance on multivariate analysis , besides the hemoglobin levels [ 3 ]  . 
 patients and methods between january 1991 and december 1996 , 95 ( 45% ) patients were treated with a continuous regimen ( crt ) of hdr - bt and ebrt and 115 ( 55% ) patients with a sequential regimen ( srt ) of hdr - bt followed by ebrt at the center of oncoradiology , budapest , hungary . 
all patients had a histologically proven squamous cell carcinoma of the uterine cervix stage iia / b or iiib according to the figo classification from 1987 . patients with stage iia were inoperable for general medical reasons . 
the hdr - bt dose was 6 gy to point a , while ebrt was delivered to a total dose of 6870 gy calculated to point a and 5254 gy calculated to point b . 
 the srt started with hdr - bt , 8 gy to point a once weekly , and was applied four times altogether , thereafter continued by ebrt up to 70 gy calculated to point a and 5254 gy calculated to point b . 
 ebrt was performed with a 1.25 - mv cobalt machine in 56 patients and with a 6to 18 - mv linear accelerator in 154 patients , respectively , using a box technique . 
 staging procedures included clinical examination ( bimanual pelvic and rectal examination ) , chest x - ray , abdominal and pelvic ultrasonography ( us ) or / and abdominal computed tomography ( ct ) , cystoscopy and rectoscopy . 
 we differentiated between stages ii and iiib of cervical cancer , in order to distinguish patients with a big tumor burden from those without : in 53 cases the tumor infiltrated one side of the parametria and in 141 cases both sides . 
 complications were assessed quantitatively and qualitatively using the ctc ( common toxicity criteria ) scale , and hospitalization due to complications was recorded ( ctc scale version 2 )  . 
cox regression analysis that takes substages and tumor extension to one or both sides of the parametria into account , revealed that srt was not significantly worse in terms of local progression than crt . 
among the seven patients with early bladder injury , just one showed late bladder injury , whereas 26 patients with late bladder injury did not show early bladder injury . around half of the 13 patients who had early rectal injury also sustained late rectal injury . 
the investigation of newer agents such as paclitaxel , gemcitabine , topotecan and vinorelbine in combination with irradiation is the subject of ongoing trials and the same holds true for the application of growth factor inhibitors , i.e. , epidermal growth factor and vascular endothelial growth factor . more details are given in roses overview [ 21 ]  . 
five sessions of locoregional hyperthermia in addition to standard pelvic radiotherapy of locally advanced cervical carcinoma lead to an improvement in both lc and os and therefore clearly result in a therapeutic gain [ 23 ]  . 
 to achieve a better response rate and local relapse - free survival rate , radiochemotherapy or thermoradiotherapy could be the treatment option for patients with figo stage iiib cervical carcinoma rather than the application of more aggressive solely radiotherapeutic regimens [ 4 , 5 ]  . 
 as far as exclusive radiotherapy is concerned , there is evidence that the total dose and ott have an influence on the results of primary radiotherapy in cervical canstrahlenther onkol 2004 no . 
 a number of patient , tumor , and treatment parameters have been reported to correlate with outcome after definitive radiotherapy of cervical carcinoma , but few studies have analyzed the interrelation between the timing or sequence of ebrt and hdr - bt regimens on outcome . 
 this study was performed to investigate the treatment endpoints ( lc , pfs ) and side effects in two patient groups equally balanced between two ebrt and hdr - bt treatment concepts over a period of 7 years . 
 the doses applied in ebrt and hdr - bt were comparable to those in other publications ; moreover , we did not differentiate between prescribed doses to point a depending on the figo stage . 
regarding pfs , the 5 - year cumulative rate amounted to 71% for the crt scheme and to 56% for the srt scheme , but the difference was not statistically significant , even if an analysis of substages was performed . 
from a radiobiological point of view , there are two major differences between the two regimens in our study : the ott is almost double compared to the crt schedule ; there is a higher dose per fraction applied in the bt component of the srt regimen , however , the total doses delivered by bt are the same . 
the impact of ott on survival was emphasized in several studies [ 3 , 13 , 17 , 18 ] , but no correlation was found between ott and outcome [ 7 ]  . 
this could be the reason for the low incidence of small bowel obstruction in our series , as the dose of external irradiation is supposed to play a major role in the development of small intestinal obstruction or perforation [ 9 , 12 ]  . 
 an analysis of the impact of the difference between the two regimens on the incidence of late side effects revealed that not the crt regimen with its dose density but the srt regimen with its relatively large hdr - bt fraction size was the most important factor for the development of late side effects . data from the literature show that hdr - bt fraction sizes > 7.5 gy lead to higher toxicities [ 9 , 11 , 13 ]  . 
primary radiotherapy of cervical carcinoma early bladder injury no pain no pain early rectal injury no pain no pain pain pain pain continuous therapy sequential therapy continuous therapy sequential therapy figure 5a abbildung 5a figure 5b abbildung 5b late bladder injury late rectal injury no pain no pain no pain no pain pain pain pain pain pain continuous therapy sequential therapy continuous therapy sequential therapy figure 5c abbildung 5c figure 5d abbildung 5d figures 5a to 5d . 
the impact of regimens on early bladder injury ( a ) , early rectal injury ( b ) , late bladder injury ( c ) , and late rectal injury ( d )  . 
einfluss des regimes auf die frhen nebenwirkungen der blase ( a ) und des rektums ( b ) sowie auf die spten nebenwirkungen der blase ( c ) und des rektums ( d )  . 
 to achieve a better treatment response rate and local relapse - free survival rate , radiochemotherapy or thermoradiotherapy should be the treatment option for patients with figo stage iiib cervical carcinoma rather than the application of more aggressive solely radiotherapeutic regimens [ 4 , 6 , 7 , 23 ]  . 
primary radiotherapy of cervical carcinoma strahlentherapie und onkologie original article 1 and nf - ( cid : 2 ) b parallels a biphasic the induction of tgf - ( cid : 1 ) time course of leukocyte / endothelial cell adhesion following low - dose x - irradiation franz rdel1 , ulrich schaller1 , stefan schultze - mosgau2 , horst - ulrich beuscher3 , ludwig keilholz1 , martin herrmann4 , reinhard voll4 , rolf sauer1 , guido hildebrandt5 1 expression , and nf - ( cid : 2 ) b activity following ld - rt has not been thoroughly investigated yet . background and purpose : low - dose radiotherapy ( ld - rt ) is known to exert an anti - inflammatory effect , but the knowledge of the underlying molecular mechanisms is still scarce . 
the authors have recently reported that transforming growth factor beta 1 ( tgf - ( cid : 1 ) 1 ) essentially contributes to a reduced endothelial adhesion of mononuclear cells ( pbmc ) following ld - rt . 
however , the time tgf - ( cid : 1 ) course of adhesion , tgf - ( cid : 1 ) material and methods : the human ea.hy.926 endothelial cell line ( ea.hy.926 ec ) was grown to 95% confluence . 
immediately after stimulation with the pro - inflammatory cytokine tumor necrosis factor alpha ( tnf - ( cid : 3 ) ) , ea.hy.926 ec were irradiated with single doses ranging from 0.3 up to 3 gy . 
neutralization of tgf - ( cid : 1 ) 1 activity restored adhesion at 4 and 24 h after ld - rt of ea.hy.926 ec , but it did not influence leukocyte adhesion 12 h after irradiation . 
 conclusion : ld - rt of stimulated human ea.hy.926 ec is followed by a biphasic time course of nf - ( cid : 2 ) b activity and an increased secretion of tgf - ( cid : 1 ) 1 . 
die autoren konnten krzlich zeigen , dass transforming growth factor beta 1 ( tgf - ( cid : 1 ) 1 ) zu einer verminderten adhsion von mononukleren zellen ( pbmc ) an endothelzellen nach ld - rt beitrgt . 
dabei war die tgf - ( cid : 1 ) 1 - sekretion mit der induktion des transkriptionsfaktors nuclear factor kap1 - sekretion und der nf - ( cid : 2 ) b - dna - bindungsaktivitt pa b ( nf - ( cid : 2 ) b ) assoziiert . 
sofort nach stimulierung mit dem proinflammatorischen zytokin tumor - nekrose - faktor alpha ( tnf - ( cid : 3 ) ) wurden die zellen mit einzeldosen zwischen 0 , 3 und 3 gy bestrahlt . 
nuklere extrakte und kulturberstnde wur1 department of radiooncology , university of erlangen - nuremberg , erlangen , germany , 2 department of oral and maxillofacial surgery , university of erlangen - nuremberg , erlangen , germany , 3 institute of microbiology and immunology , university of erlangen - nuremberg , erlangen , germany , 4 institute of clinical immunology and rheumatology , university of erlangen - nuremberg , erlangen , germany , 5 department of radiotherapy and radiooncology , university of leipzig , germany . 
 ergebnisse : 4 und 24 h nach bestrahlung aktivierter ea.hy.926 - endothelzellen war im dosisbereich von 0 , 3 bis 0 , 7 gy eine verminderte leukozytenadhsion im vergleich zu einer unbehandelten kontrolle zu beobachten . 
berraschenderweise zeigte sich 1 - sekretion und nf - ( cid : 2 ) b12 h nach bestrahlung ein relatives adhsionsmaximum ( anstieg um bis zu 30% ) bei 0 , 3 gy . 
die tgf - ( cid : 1 ) dna - bindungsaktivitt wiesen eine vergleichbare biphasische kinetik mit einem relativen minimum 12 h nach bestrahlung auf . eine neutralisation der tgf - ( cid : 1 ) 1 - aktivitt fhrte zur wiederherstellung der adhsion an ea.hy.926 - endothelzellen 4 und 24 h nach ld - rt , die gesteigerte adhsion 12 h nach bestrahlung wurde hingegen nicht beeinflusst . 
 schlussfolgerung : die ld - rt stimulierter humaner ea.hy.926 - endothelzellen fhrt zu einer biphasischen zeitabhngigkeit der nf - ( cid : 2 ) b - dna - bindungsaktivitt und tgf - ( cid : 1 ) 1 - sekretion . 
whereas xirradiation with higher doses exerts pro - inflammatory effects [ 8 , 9 ] , low - dose radiotherapy ( ld - rt ) has been described to display anti - inflammatory properties [ 24 , 31 , 32 ]  . 
ld - rt , therefore , has been in clinical use for the treatment of benign chronic inflammatory diseases and acute inflammatory disorders for decades [ 1 , 19 , 29 ]  . 
an improvement of the clinical symptoms is observed after fractionated irradiation with 0.51.0 gy , given three to five times weekly , not exceeding a cumulative dose of 6.0 gy [ 19 , 31 ]  . 
remarkably , the anti - inflammatory efficacy of ld - rt was clinically observed in various pathologic conditions , suggesting that it might target basic mechanisms of inflammation [ 31 , 32 ]  . 
indeed , there is growing experimental evidence that ld - rt modulates the function of a variety of cells , including endothelium , blood mononuclear cells ( pbmc ) , and macrophages [ 24 ]  . 
the effects comprise a reduced adhesion of pbmc to endothelial cells ( ec ) [ 6 , 11 , 25 ] , the induction of apoptosis , and the proteolytic shedding of l - selectin from lymphocytes [ 12 , 13 ]  . 
in stimulated macrophages , ld - rt caused a reduced activity of inducible nitric oxide synthase ( inos ) [ 5 , 7 ] and a lowered oxidative burst [ 27 ]  . 
tgf - ( cid : 1 ) 1 was found to play a key role for a decreased adhesion of pbmc to ec after ld - rt [ 25 ]  . expression of tgf - ( cid : 1 ) 1 parallels the induction of nuclear factor kappa b ( nf - ( cid : 2 ) b ) with a biphasic run of the curve of dnabinding and transcriptional activities showing relative maxima at 0.5 and 3 gy , respectively [ 23 ]  . 
 the results presented in this paper demonstrate that activation of nf - ( cid : 2 ) b and tgf - ( cid : 1 ) 1 after ld - rt display a biphasic time dependency . 
comparative studies demonstrated that adhesion properties were comparable between ea.hy.926 ec and primary huvec monolayers stimulated with the pro - inflammatory stimulus tumor necrosis factor alpha ( tnf ) [ 30 ]  . 
ea.hy.926 ec were grown in dulbeccos modified eagles medium ( dmem ) supplemented with 10% fetal calf serum ( fcs ) , 2% ascorbic acid , 1% sodium pyruvate and penicillin / streptomycin ( 100 u / 100 mg / ml ; all supplements from biochrom , berlin , germany ) in tissue culture flasks at 37 c in an atmosphere of 5% co2 . 
pbmc were isolated from heparinized blood of healthy donors , using density - gradient centrifugation ( biocoll separating solution , biochrom ) , as previously described [ 6 , 25 ]  . 
isolated pbmc ( 2 ( cid : 4 ) 106 / ml ) were washed twice and cultured in rpmi 1640 medium with 10% fcs / 1% penicillin / streptomycin ( all biochrom ) for at least 4 h at 37 c and 5% co2 prior to the adhesion assays . 
tnfstimulation was performed , since nonactivated ec do not display significant levels of activated nf - ( cid : 2 ) b and of cytokine expression and also adhesion of pbmc is low . 
as such we chose the cytokine tnf - , which plays a critical role in many inflammatory conditions in vivo and is a potent activator of the transcription factor nf - ( cid : 2 ) b . 
 adhesion assay 3 ( cid : 4 ) 105 ea.hy.926 ec cells / ml were seeded on fibronectincoated lab - tek slides ( nunc ) , grown to 95% confluency , stimulated and irradiated with doses ranging from 0.3 to 3 gy as described above . 
after blocking with bsa ( 1% in trisbuffered saline ) for 10 min , bound cells were visualized by incubation with streptavidin - cy3 ( 1 : 500 , dianova , hamburg , germany ) for 40 min at room temperature . 
after two final washes , adherent pbmc were counted in eight randomly selected microscope fields and documented using a fluorescence microscope ( ( cid : 4 ) 250 , axiophot , zeiss , jena , germany )  . 
image analysis was carried out after digitalizing with a ccd camera ( kappa , gleichen , germany ) connected to a personal computer ( optimas 6.2 , puchheim , germany )  . 
in one set of experiments , 5 g / ml neutralizing anti - tgf - ( cid : 1 ) 1 antibodies or 5 g / ml chicken control antibodies ( both r&d systems , wiesbaden , germany ) were added to ea.hy.926 ec immediately before stimulation and irradiation . 
 preparation of nuclear extracts and electrophoretic mobility shift assays ( emsa ) approximately 1 ( cid : 4 ) 107 ec were sedimented by low speed centrifugation ( 800 g ( cid : 4 ) 5 min ) and incubated in 200 l buffer a ( 20 nm hepes , ph 7.9 , 10 mm nacl , 1 mm edta , 1 mm dithiothreitol [ dtt ] containing the protease inhibitors pepstatin [ 0.7 g / ml ] , aprotinin [ 1.5 g / ml ] , leupeptin [ 1 g / ml ] , and phenyl - methyl - sulfonylfluoride [ 1 m ] , all sigma ) for 10 min on ice ; then 10 l of np - 40 solution ( 1% in h2o ) was added . 
the emsa were performed by incubating aliquots of nuclear extracts containing 10 g total protein with 32p - labeled ( amersham pharmacia , freiburg , germany ) double - stranded nf - ( cid : 2 ) b - specific oligonucleotide probes ( sense : 5 ( cid : 3 ) - agttgaggggactttcccagg - 3 ( cid : 3 ) ; eurogentec , searing , belgium ) as previously described [ 33 ]  . the reaction mixture contained 10 mm tris - hcl , ph 7.5 , 50 mm nacl , 1 mm etda , 1 mg / ml bsa , 2 mm didc , and 3 mm gtp . 
after electrophoresis , the gels were dried , and the dna - protein complexes were detected by autoradiography ( biomax film , kodak , rochester , ny , usa ) and , in addition , by phosphoimaging ( fuji fla 3000 , raytest , straubenstadt , germany )  . individual bands were quantified using the aida software package ( raytest )  . 
 quantification of tgf - ( cid : 1 ) immunosorbent assay ( elisa ) 1 secretion by enzyme - linked the tgf - ( cid : 1 ) 1 concentration in the culture supernatants was determined employing cytokine elisa kits ( opteia , pharmingen , heidelberg , germany )  . 
absorbance was measured at 450 nm using an elisa reader ( hts700 , perkin elmer , rodgaujgesheim , germany ) , and concentrations were calculated using a standard curve of recombinant tgf - ( cid : 1 ) 1 and the software package ht - soft ( perkin elmer )  . 
4 h after irradiation with 0.5 gy , pbmc adhesion was significantly ( p = 0.001 ) decreased to 50% of the control , whereas higher doses had only minor effects on cell adhesion ( figure 1a )  . 
by contrast , irradiation with 0.3 gy even showed an opposite effect as reflected by an increase of adherence by 1530% ( p = 0.02 ) at this time point ( figure 1b )  . 
adhsion von mononukleren zellen ( pbmc ) an stimulierte ( tnf - ( cid : 3 ) , 10 ng / ml ) ea.hy.926 - endothelzellen 4 ( a ) , 12 ( b ) und 24 h nach bestrahlung mit den angegebenen dosen . 
 correlation between leukocyte / ec adhesion and tgf - ( cid : 1 ) 1 secretion next we examined , whether tgf - ( cid : 1 ) 1 secretion of ea.hy.926 ec irradiated with ld - rt correlates with the biphasic time course of pbmc adhesion . 
 the functional relationship of tgf - ( cid : 1 ) 1 secretion and leukocyte / ec adhesion was analyzed by pretreatment of ea.hy.926 ec with saturating concentrations of anti - tgf - ( cid : 1 ) antibodies [ 25 ]  . 
neutralization of tgf - ( cid : 1 ) 1 increased adhesion of pbmc to ec at 4 and 24 h , thereby reaching 92 5% of the values of adhesion displayed by nonirradiated ec ( figure 3 )  . control antibodies or pbs did not influence the adhesion at any dose . 
the increase in pbmc adhesion 12 h after ld - rt , however , was not influenced by tgf - ( cid : 1 ) 1 antibody treatment . this indicates , that additional factors besides tgf - ( cid : 1 ) 1 may be responsible for the increase of adhesion at this time point . 
for quantitative considerations , phosphor imaging analyses were 0 gy 0.5 gy ( cid : 1 ) 0.3 gy 1 gy time after stimulation ( h ) figures 2a to 2d . 
adhsion von mononukleren zellen ( pbmc ) an aktivierte ea.hy.926 - endothelzellen in anwesenheit von anti - tgf - ( cid : 1 ) 1 - antikpern ( 5 g / ml ) bzw . 
bis zu 30 h nach stimulation und bestrahlung ( 0 , 5 gy ) wurden nuklere extrakte ( 10 g ) gewonnen und in einem emsa mit 32p - markierten nf - ( cid : 2 ) b - spezifischen oligonukleotiden inkubiert . 
these responses mainly act via activation of transcription factors like nf - ( cid : 2 ) b and activating protein - 1 ( ap - 1 ) [ 2 ] which are of crucial importance for the expression of several genes , coding for various effector molecules of the immune system like cytokines , adhesion molecules , and enzymes ( e.g. , inos ) [ 2 , 18 ]  . 
since there is substantial evidence for the involvement of cytokines and nf - ( cid : 2 ) b in the stress responses to irradiation as well as in the inflammatory response , these molecules may also represent a crucial link between ld - rt and its anti - inflammatory properties . 
 we have recently reported a significant reduction of leukocyte / ec adhesion after ld - rt with 0.3 gy and up to 1 gy [ 12 , 25 ]  . 
this reduction was inversely correlated to the ac1 and to the level of tgf - ( cid : 1 ) tivity of tgf - ( cid : 1 ) 1 mrna . 
the key role of tgf - ( cid : 1 ) 1 for the reduced adhesion was demonstrated by neutralization of the cytokine using specific antibodies consistent with published data on the anti - adhesive and anti - inflammatory properties of tgf - ( cid : 1 ) 1 on ec [ 16 ]  . 
interestingly , the kinetics of ec adhesion parallels the biphasic expression of the cytokine tgf - ( cid : 1 ) 1 12 h after irradiation with 0.3 gy , the minimum of tgf - ( cid : 1 ) 1 expression coincides with a maximum of adhesion . 
the studies with the neutralization of tgf - ( cid : 1 ) 1 and the inverse correlation between tgf - ( cid : 1 ) 1 expression and ec adhesion 4 and 24 h after ld - rt confirmed their direct functional interrelationship . however , the increased adhesion 12 h after ld - rt was not regulated by tgf - ( cid : 1 ) 1 , additional not yet identified molecules are supposed to be involved in this regulation . 
therefore , beside tgf - ( cid : 1 ) a biphasic characteristic of tgf - ( cid : 1 ) 1 induction has been reported for normal tissue and carcinoma cells of pig skin and mouse lung after exposure to ionizing radiation and uv - a , respectively [ 15 , 26 ]  . 
furthermore , several studies have shown that radiation - induced cellular responses often display discontinuous dose dependencies as shown for the activation of c - fos and c - myc , apoptosis , and the expression of the tumor suppressor p53 [ 4 , 11 , 21 ]  . 
notably , the induction of nf - ( cid : 2 ) b in human 244b lymphoblastoid and b16 melanoma cells by ld - rt also showed a biphasic kinetics [ 15 , 17 , 20 ]  . 
these results were in line with the data mentioned above , indicating a more general regulation of nf - ( cid : 2 ) b induction following ld - rt in ec and malignant cells . 
moreover , we recently demonstrated a correlation of tgf - ( cid : 1 ) 1 expression and nf - ( cid : 2 ) b activation [ 23 ]  . 
nf - ( cid : 2 ) b decoy oligonucleotides , that had been shown to specifically abrogate the transcriptional activity of nf - ( cid : 2 ) b - activated genes [ 14 ] , alleviated the irradiation - induced secretion of tgf - ( cid : 1 ) 1 by > 50% . 
furthermore , a central role of the nf - ( cid : 2 ) b subunit p65 / rela for the induction of tgf - ( cid : 1 ) 1 was recently described for monocytes of patients with myelofibrosis [ 22 ]  . 
 the underlying molecular mechanisms resulting in the biphasic induction of the nf - ( cid : 2 ) b and tgf - ( cid : 1 ) 1 activity after ldrt remain elusive . 
the biphasic time course is most likely the result of the overlay of more than one process triggered by the ld - rt and operating at different threshold doses and kinetics . 
our observations may also be linked to the phenomenon of low - dose hypersensitivity ( hrs ) and induced radioresistance ( irr ) , that have been reported for cellular survival at doses < 1.0 gy ( reviewed in [ 10 ] )  . 
although not proven to date , one can speculate that activation of nf - ( cid : 2 ) b and tgf - ( cid : 1 ) 1 expression may be part of this mechanis taken together , our results indicate a highly complex time - dependent regulation of leukocyte / ec adhesion following ld - rt . 
the discontinuous dose - response curve and biphasic kinetics most likely originate from the overlay of several individual processes that are initiated at different thresholds , displaydifferent time kinetics , and operate in a staggered manner . 
grtz2 , christoph glanzmann1 purpose : the incidence of osteonecrosis of the mandibula ( on ) after irradiation using modern three - dimensional planning as well as hyperfractionation or moderately accelerated irradiation has been evaluated and compared with the incidence of the preceding period . 
 patients and methods : the records of 268 head and neck cancer patients irradiated between january 1 , 1980 and december 31 , 1998 with a dose to the mandibula of at least 60 gy were retrospectively analyzed . 
 conclusion : comparison of the incidence of on during the period between 1980 and 1990 with the following period between 1990 and 1998 shows a decrease in risk to a value of approximately 5% using modern three - dimensional techniques as well as hyperfractionation or moderately accelerated fractionation . 
alle patienten erhielten eine ct - untersttzte computerisierte bestrahlungsplanung mit isodosenkarten auch in mehreren ebenen auerhalb des zentralstrahls und regelmigen feldkontrollaufnahmen . ergebnisse : die kumulative inzidenz einer mit mandibularesektion behandelten on nach bestrahlung betrug nach konventioneller fraktionierung ( abbildung 1a ) 6 , 2% ( 6066 , 6 gy ) bzw . 
20 , 1% ( > 66 , 672 gy ) , nach hyperfraktionierter bestrahlung ( abbildung 1c ) mit 7278 , 8 gy 6 , 6% ; nach akzelerierter bestrahlung ( abbildung 1b ) gem dem schema des mda - hospitals in houston , tx , usa , mit einer dosis von 63 , 970 , 5 gy wurde keine on beobachtet , whrend nach 6 ( cid : 1 ) 2 gy / woche bzw . 
 schlussfolgerung : ein vergleich der inzidenz von on der mandibula nach anwendung moderner dreidimensionaler bestrahlungsplanung und hyperfraktionierter oder mig akzelerierter bestrahlung mit gleichzeitigem boost nach dem schema des mda - hospitals zeigt gegenber der inzidenz in der vorausgegangenen periode zwischen 1980 und etwa 1987 einen rckgang auf werte von etwa 5% ( tabelle 2 )  . 
 schlsselwrter : komplikationen fraktionierung hyperfraktionierung akzelerierung osteoradionekrose mandibula bestrahlung 1 department of radiation oncology , and 2 department of cranio - maxillo - facial surgery , university hospital zurich , switzerland . 
a relationship between total dose using conventional fractionation and risk of on is known : after a dose < 60 gy using standard fractionation on is rare , the risk increases more steeply after 66 gy [ 16 ]  . 
several factors may influence the risk , but are less well established : tumor stage and site , dental extractions , compliance with dental / oral care , smoking , and alcohol abuse [ 16 ]  . 
 patients and methods patients since the early 1970s , all patients with cancer of the head and neck are examined in a joint clinic by the head and neck surgeon together with a radiotherapist , both before treatment and during regular follow - up after treatment . 
follow - up intervals are between 2 and 3 months in the 1st year after treatment , 3 months in the 2nd year , 6 months in the 3rd , 4th and 5th year , and annually thereafter . 
all our patients with bone exposure lasting > approximately 6 weeks or other signs of a bone problem are referred to the dental clinic of the department of oral and cranio - maxillo - facial surgery . 
for an analysis of the incidence rate of and different factors contributing to on , we checked the simulator and verification films as well as the irradiation details of patients with primary or postoperative irradiation for cancer of the head and neck between january 1 , 1980 and december 31 , 1998 . 
since no instances of on had been observed after a mandibular dose < 60 gy , the records of 268 patients with a mandibular dose of 60 gy or higher were further analyzed . 
patients with a bone problem associated with tumor recurrence and bone involvement were also excluded . one patient sustained a radiation - associated mandibular fracture in the region outside the surgical intervention performed for a tumor recurrence with bone involvement . 
diagnosis of on was confirmed by histological analysis in patients with bone resection ( all grade 3 and 4 on ) , by biopsy in two of the patients with grade 2 on , and by clinical and radiologic data during follow - up . 
 on grade 2 : bone exposure with necrosis of the exposed superficial cortical bone with or without minimal involvement of the underlying medullary bone , healing with conservative treatment and not requiring surgical treatment . 
 the retrospective analysis of our clinical records did not permit a detailed classification according to the lent / soma scale : according to the soma parameters , patients in our group on grade 2 are less than soma grade 3 in pain , mastication and denture use but can be in soma grade 3 in regard to management , because we use hyperbaric oxygenation ( hbo ) rather liberally in patients with bone exposure even without signs of necrosis [ 14 , 15 , 24 , 28 , 29 ]  . patients in our group on grade 3 had all a satisfactory result after a single mandibular resection ( soma scale grade 4 for management ) , whereas patients in our group on grade 4 had more than one surgical treatment without satisfactory result . 
 after the clinical diagnosis and radiographic examination of a bone necrosis , conservative treatment was applied initially : multiple daily saline irrigation , topical antiseptic treatment and systemic antibiotics during infectious episodes , gentle sequestrectomy and removal of visibly loosened bone elements as well as treatment with hbo . 
from 1988 until 1991 , routine fractionation was 1.8 gy mostly prescribed to the 95% isodose five , six , or seven times per week ( applying two fractions on 1 or 2 days / week with an interval of at least 6 h )  . hyperfractionation has been used since 1988 , applying two daily fractions of 1.20 gy on 5 days / week with an interfraction interval of at least 6 h . 
since 1991 , also moderately accelerated fractionation has been used : 1.8 gy seven times per week or 2.0 gy six times per week or the concomitant boost regime of the mda hospital in houston , tx , usa [ 1 ]  . 
 six patients in the group treated with 5 ( cid : 1 ) 2.0 gy / week had neoadjuvant chemotherapy before irradiation with a gap of > 4 weeks , 42 of the patients from the hyperfractionation group and five of the patients from the groups treated with accelerated fractionation had simultaneous chemotherapy including two cycles of cisplatinum 5 ( cid : 1 ) 20 mg / m2 / day for 5 days during weeks 1 and 5 . 
 75% of the patients with hyperfractionation had simultaneous therapy with cddp 5 ( cid : 1 ) 20 mg / m2 / day for 5 days during weeks 1 and 5 . 
 data analysis data analysis was performed using the statview program ( discontinued as of december 31 , 2002 by sas institute inc . , cary , nc , usa )  . 
the proportional hazards regression model ( cox model ) was used to estimate the relative risk of on with adjustment for confounding variables such as dental status , relation of tumor to bone , total dose , fractionation , and proportion of mandibula exposed to high doses . 
 results incidence of osteoradionecrosis table 1 shows a summary of the incidence of on in our patients included in different categories of irradiation regimes : the cumulative incidence at the end of follow - up of all grade 14 on was 12.5% and the incidence of grade 3 or 4 on 10.4% ; four patients with grade 4 on died due to complications associated with on . 
two of the four patients with fatal on died due to inanition and infectious complication without surgical intervention and the other two died of cardiorespiratory arrest after repeated surgery for on . 
when limiting the calculation to patients in whom at least a part of the horizontal branch had been included , the incidence of grade 3 or 4 on 10 years after irradiation was 13.5% , and when limiting the calculation to patients in whom the tumor abutted or invaded the bone , the cumulative incidence of grade 3 or 4 on was 14.6%. 
 25 patients were irradiated with 6 ( cid : 1 ) 2.0 gy or 7 ( cid : 1 ) 1.8 gy per week ( two fractions on 1 or 2 days between monday and friday ) : after a total dose of 6066.6 gy , no patient suffered from grade 3 or 4 on , whereas at higher doses , a grade 3 or grade 4 on was observed in two out of 15 patients . 
length of follow - up was significantly shorter in patients with accelerated fractionation using 7 ( cid : 1 ) 1.8 gy or 6 ( cid : 1 ) 2.0 gy per week compared to the other groups . 
 in a multivariate analysis of total dose , mandibular volume and universus bilateral irradiation using the cox model in patients after conventional fractionation , the only independent significant factor was total dose with p - values < 0.05. 
using the biological effective dose ( bed ) with an ( cid : 2 ) ( cid : 3 ) ( cid : 4 ) - ratio = 0.85 for bone , the maximal dose to the bone was a highly significant factor with a p - value < 0.001. 
 only in patients treated with conventional fractionation , univariate analysis showed a significant association between dental status and the incidence of on grade 3 or 4 : cumulative incidence was 28.8% in 32 patients with teeth in the target dose region compared to an incidence rate between 5% and 10.6% in groups without teeth in the irradiated part of the mandibula or in edentulous patients ( 8 / 189 patients )  . 
 in patients with teeth in the irradiated part of the mandibula and a dose between 66 and 72 gy using conventional fractionation , the cumulative incidence of on grade 3 or 4 was 51% ( 6 / 14 patients )  . 
however , a close correlation between teeth extraction after rt and the clinical beginning of on was observed in only one patient , yet the radiographs showed definitive evidence of on already before the extraction . 
 [ 25 ] from the mda hospital in patients with tonsillar region cancer , irradiated with a dose between 65 and 75 gy using conventional fractionation between 1968 and 1979 ( crude rate of on 12% , approximately 55% of these had surgical treatment )  . 
 [ 6 ] ( mount vernon hospital / middlesex ) randomized study ( total number [ oropharynx + oral cavity ] : 552 [ 220 ] chart / 366 [ 145 ] conventional ) chart , 54 gy in 36 fractions in 12 days conventional fractionation 66 gy 2 on ( 0 , 4% ) 6 on ( 1.4% ) strahlenther onkol 2004 no . 
osteoradionecrosis of the mandibula cols in our patients between 1980 and 1990 as well as 1990 and 2000 followed comparable lines including use of hbo before dental extractions after rt and also ct - based treatment has been used since 1979 , fractionation and dosimetric techniques changed in the period between 1988 and 1991 : increasing use of hyperfractionation and concomitant boost and better dose homogeneity with avoidance of higher dose in the mandibular region are probably important factors resulting in a lower risk of on . 
 in our own experience as well as according to some published reports , the incidence of on after hyperfractionated or moderately accelerated irradiation using the concomitant boost regime was lower compared to that after conventional irradiation and chart regime [ 1 , 6 , 9 , 13 , 18 , 19 , 22 ] ( table 2 )  . 
in using hyperfractionation , an interfraction interval > 4.5 h is important : an intermediate evaluation of the rtog 83 - 13 study [ 4 , 8 ] and the experience of niewald et al . [ 21 ] show an increase of the incidence of on after hyperfractionation with an interfraction interval of 4.5 h ( table 2 )  . 
 [ 21 ] , the incidence of on after hyperfractionation using two fractions of 1.2 gy per day on 5 days per week and a total dose of 82 gy , the incidence of on was 22.9% with an interval between the two fractions of 4 h in the majority of patients ( table 2 )  . 
 [ 19 , 22 ] and the randomized fractionation study rtog 90 - 03 [ 9 ] , the risk of on is < 5% after a total dose between 72 and 80 gy and an interfraction interval of 6 h . 
 after moderately accelerated irradiation using the concomitant boost regime of the mda hospital , houston , tx , usa ( 30 ( cid : 1 ) 1.8 gy plus 1012 ( cid : 1 ) 1.5 gy = 6972 gy primary irradiation ) in 6 weeks or 63.9 gy / 5 weeks postoperative irradiation , the incidence of on is very low ( tables 1 and 2 )  . 
 the influence of several cytotoxic agents applied during irradiation on the risk of on is often unknown [ 26 ] , but concomitant treatment with cisplatin does not seem to influence the risk of on significantly [ 16 ] , despite an increase in acute morbidity ( [ 2 ] and own results )  . 
 observations concerning the influence of the dental status on the risk of on differ : no clear correlation between preand postirradiation , tooth extraction and an increased incidence of on has been observed by toljanic et al . 
 [ 31 ] whereas according to morrish et al . , perier & moeller and thorn et al . [ 20 , 23 , 30 ] , the risk of on is increased by tooth extractions shortly before or after rt . 
the majority of these data are nevertheless compatible with an increased risk of on after dental extraction shortly before as well as after irradiation . besides careful surgical techniques including plastic methods for wound closure , accompanying supportive measures including antibiotic prophylaxis ( for detailed recommendations see [ 12 ] ) and probably also the use of hbo are important . 
also , in a former analysis of the results of rt in patients with cancer of the salivary glands , no instance of grade 3 or 4 on of the ramus ascendens has been observed after conventionally fractionated irradiation with doses between 60 and 70 gy ( included in glanzmann [ 10 ] )  . 
in a publication on the diagnostic aspects by chong et al . [ 3 ] , two patients with on of the ramus ascendens after a dose between 60 and 69 gy in 3039 fractions were included . 
 there was no clear correlation between the volume of the horizontal branch exposed to high doses and the risk of on , probably due to the low number of events . 
according to our own as well as published results , the cumulative incidence of serious on has decreased from approximately 15% after conventionally fractionated irradiation with a prescription dose to the target volume between 66 and 72 gy and techniques in use before about 1990 to a value of approximately 5% or less after hyperfractionated ( dose of 7280 gy ) or moderately accelerated fractionated irradiation ( 6472 gy , concomitant boost regime of mda hospital , houston , tx , usa ) using modern techniques of three - dimensional conformal irradiation and more homogeneous dose distribution . 
a further important decrease in the risk of on will be achieved using intensity - modulated radiotherapy ( imrt ) allowing a reduction of the radiation dose to the mandible as well as of the exposed mandibular volume in most situations . 
 strahlentherapie und onkologie aktuelles forum antitumorale wirkung von interferonen und interleukinen in kombination mit strahlentherapie teil i : immunologische grundlagen carsten herskind1 , 2 , katharina fleckenstein2 , jens lohr3 , chuan - yuan li4 , frederik wenz2 , frank lohr2 hintergrund : zytokine wie z.b. 
strahlensensibilisierenden wirkungen der interferone im vordergrund standen , kommt der funktion der interferone und interleukine ( il ) im rahmen der immunantwort gegenber tumorzellen eine zunehmend grere bedeutung fr die modulation der strahlentherapie zu . 
 ergebnisse : neue immunologische erkenntnisse haben gezeigt , dass lokale interaktionen zwischen antigenprsentierenden zellen ( apc ) und effektorzellen wie natrlichen killerzellen ( nk - zellen ) und t - lymphozyten wichtig fr eine effektive immunreaktion gegen tumoren sind . 
da die systemische gabe von interferonen relativ toxisch ist , wird die strategie verfolgt , ifn - ( cid : 1 ) gezielt in th1 - lymphozyten mittels il - 12 zu induzieren . 
 schlsselwrter : strahlentherapie biological response modifiers zytokine interferon interleukin immunreaktion tumorassoziierte antigene ( taa ) strahlenther onkol 2004 ; 180 : 18793 doi 10.1007 / s00066 - 004 - 9119 - x antitumoral action of interferons and interleukins in combination with radiotherapy . 
initially , the focus was on antiviral and radiosensitizing effects of interferons but increasingly , the function of interferons and interleukins ( il ) within the immune response to tumor cells is becoming important . method : the cellular immune response toward tumor cells is reviewed . 
 results : recent advances in immunology have demonstrated the importance of local interactions between antigen - presenting cells ( apc ) and effector cells such as natural killer ( nk ) cells and t - lymphocytes for an effective immune reaction against tumors . interferons stimulate such interactions , while il - 2 plays a central role in the activation of nk cells and t - lymphocytes . 
since systemic application of interferons is quite toxic , present strategies aim at local expression , e.g. , the induction of ifn - ( cid : 1 ) expression in th1 cells by il - 12 . 
 1 department of experimental clinical oncology , aarhus university hospital , aarhus , dnemark , 2 institut fr klinische radiologie , sektion strahlentherapie , mannheim , 3 department of pathology , university of california san francisco school of medicine , san francisco , california , usa , 4 department of radiation oncology , duke university medical center , durham , north carolina , usa . 
antitumorale wirkung von zytokinen und radiotherapie teil i conclusion : the improved understanding of immunologic mechanisms has emphasized the role of the cytokine network in the interaction between tumor cells and effector cells such as nk cells and t - lymphocytes . 
this opens new possibilities for the application of cytokines as biological response modifiers , which may eventually help widening the therapeutic window in radiotherapy . key words : radiotherapy biological response modifiers cytokines interferon interleukin immune response tumorassociated antigens ( taa ) einleitung5 interferone und interleukine wurden schon frh als biological response modifiers in der strahlentherapie eingesetzt , um eine biologische modulation der tumorantwort zu erzielen . grundlage des interesses an zytokinen wie interferon - ( ifn - ) , - ( cid : 2 ) , und interleukin - ( il - ) 2 war zunchst deren antivirale wirkung . 
mit der erkenntnis , dass sich auch auf tumorzellen zytokinrezeptoren befinden und zytokine die strahlenempfindlichkeit von tumorzellen modulieren knnen , wurden klinische und prklinische studien jedoch zunehmend auf strahlenbiologischer basis durchgefhrt . 
dieser wandel knnte auch als paradigmenwechsel angesehen werden und fordert eine multidisziplinre integration immunologischer , gentechnischer und strahlenbiologischer fachbereiche . die vernderung des rationals des klinischen einsatzes von interferonen und interleukinen in kombination mit strahlentherapie ist thema dieser bersicht , die aus zwei teilen besteht . 
die mglichkeiten einer gezielten immunologischen modulation werden am beispiel der induktion von ifndurch il - 12 erlutert . im zweiten teil der bersicht werden die bisherigen klinischen ergebnisse antitumoraler interaktionen der interferone mit der strahlentherapie zusammengefasst und neue immunologische strategien des einsatzes von interleukinen in kombination mit strahlentherapie in prklinischen testsystemen und klinischen studien dargestellt . 
 elemente der zellulren immunantwort zellulre effektoren das immunsystem bildet ein komplexes netzwerk , das vereinfachend in zwei ausfhrende arme geteilt ist , deren vernetzung untereinander jedoch in letzter zeit immer deutlicher wird : das sog . 
ein weiteres element des zellulren arms , die natrlichen killerzellen ( nk - zellen ) , nimmt eine zwischenstellung ein , indem es als element des innaten arms direkt antigentragende zellen eines bestimmten phnotyps lysieren kann , jedoch auch funktionen im rahmen von adaptiven reaktionen bernimmt . 
 typs zu einer funktionalen gruppe nicht eindeutig ist , so sind doch der berwiegende teil der t8 - lymphozyten den zytotoxischen t - zellen ( ctl ) und der grte teil der t4 - lymphozyten den immunregulativ wirksamen t - helfer - zellen zuzuordnen . 
regulatorischen t - zellen kompliziert worden , einer subgruppe der cd4 + - zellen , die auf unterschiedliche weise toleranz induzieren knnen [ 9 , 22 , 55 ]  . 
major - histocompatibility - complex - ( mhc - ) antigenen , dargeboten werden . dazu mssen die antigene von der prsentierenden zelle intrazellulr prozessiert und in peptidform an die mhcmolekle gebunden werden . 
whrend praktisch alle normalen zellen und auch ein teil der tumorzellen mhc - molekle der klasse i exprimieren ( mhc - i ) , finden sich mhc - molekle der klasse ii ( mhc - ii ) nur auf professionellen apc . 
 verschiedene andere oberflchenmolekle auf apc und effektoroder regulatorischen zellen sind an der antigenprsentation gegenber t - zellen beteiligt ( abbildung 1 ) : der t - zell - rezeptor ( tcr ) ist das molekl auf t - zellen , das primr mit einem auf mhc - moleklen prsentierten antigen reagiert . 
 zytokine knnen proinflammatorisch oder immunsuppressiv wirken , wobei die grenzen immer unschrfer werden und die wirkungsweise stark vom immunologischen kontext abzuhngen scheint und oft pleiotropisch ist [ 38 ]  . 
die sekretion ist meist kurz und selbstlimitierend und zieht gewhnlich die sekretion einer kaskade anderer zytokine nach sich [ 1 ]  . zytokine wirken normalerweise lokal autooder parakrin , knnen jedoch auch endokrin systemisch wirken . 
typ - i - interferone , die eine wichtige rolle in der immunantwort auf virale infektionen spielen . ifnwird berwiegend von phagozyten produziert , whrend ifn - ( cid : 2 ) auch von anderen zelltypen produziert werden kann . typ - i - interferone fhren zu erhhter expression von mhc - i und sind auch an der aktivierung von nk - zellen beteiligt [ 49 ]  . 
ifn ( typ - ii - interferon ) wird von th1 - lymphozyten exprimiert und charakterisiert zusammen mit il - 2 die typ - 1zytokinexpression ( abbildung 1a )  . 
hufig wird in tumorzellen die herunterregulierung von mhc - i - moleklen beobachtet , u.a. vermittelt durch ras - induzierte fehlregulierung des intrazellulren peptidtransports und der bausteine der proteasomkomplexe [ 51 ]  . 
auch die sekretion von transforming growth factor - ( cid : 2 ) ( tgf - ( cid : 2 ) ) , die in tumorzellen durch ras - mutation hochreguliert werden kann , unterdrckt die reaktion des immunsystems gegenber tumoren [ 58 ]  . 
antitumorale wirkung von zytokinen und radiotherapie teil i endothelial growth factor ( vegf ) , der von den meisten humanen tumoren sezerniert wird , zu einer beeintrchtigten dc - maturierung [ 40 ]  . 
 auswirkungen der bestrahlung auf das immunsystem ionisierende strahlung hat direkte und indirekte auswirkungen auf immunologische vorgnge , die vom bestrahlten volumen , von der dosis und der jeweils betrachteten zellpopulation abhngen . 
die antitumoralen effekte von niedrig dosierter ganzkrperbestrahlung ( total body irradiation [ tbi ] ) werden dabei hchstwahrscheinlich teilweise durch induktion von zytokinen wie il - 2 , ifn - ( cid : 2 ) und tumor - nekrosefaktor - ( tnf - ) mit konsekutiver nkund t - zell - aktivierung vermittelt [ 15 , 47 ]  . 
 die lokoregionre bestrahlung im kopf - halsoder abdominalbereich beeinflusst auch die systemische immunitt . whrend je nach zielvolumen der bestrahlung unterschiedliche effekte beobachtet werden , scheinen cd4 + - zellen empfindlicher als cd8 + - zellen und naive t - zellen empfindlicher als memory - t - zellen zu sein [ 4 , 42 , 56 ]  . 
 die fr die antigenprsentation mageblich verantwortlichen dc werden nach bestrahlung dezimiert ; allerdings werden dc auch schon kurz nach bestrahlung wieder in bestrahltes gewebe rekrutiert [ 8 , 20 ]  . 
auch in klinischen prparaten fanden sich nach lokaler bestrahlung t - zell - infiltrate , die berwiegend aus cd4 + - zellen bestanden , was auf eine potentiell erhhte immunogenitt des tumors hinweist [ 36 ]  . 
dem kmt - 17 - fibrosarkom unter wachstumsfrdernden bedingungen herunterreguliert ist , kann durch bestrahlung wieder normalisiert werden , was auch das metastatische potential dieses tumors senkt [ 52 ]  . 
auch eine reihe von zytokinen , die im rahmen der immunreaktion von bedeutung sind , wie z.b tnf - , wird durch bestrahlung induziert [ 16 , 46 ]  . 
zelladhsionsmolekle ( icam - 1 , integrin ) , mhc - i , b7.1 und gp96 , konnten durch bestrahlung induziert werden [ 14 , 26 , 28 , 48 ]  . 
whrend integrin bereits nach dosen von 5 gy induziert wurde [ 26 ] , waren allerdings in den meisten fllen hohe einzeldosen im bereich von > 25 gy fr eine signifikante induktion erforderlich . 
dagegen lie sich in vitro im b16 - melanom und im 4t1 - mammakarzinom eine radiogene induktion im dosisbereich bis zu 18 gy weder fr mhc - i noch fr b7.1 nachweisen [ 24 ]  . 
 strategie der ifn - ( cid : 1 ) - induktion durch il - 12 die rolle von il - 12 als stimulator der zellulren immunantwort durch induktion von ifnbildete die basis fr das interesse an il - 12 als antitumoral wirksamem immunmodulator , obwohl kein direkter antiproliferativer effekt in vitro beobachtet wurde [ 7 ]  . 
tgliche intraperitoneale injektionen von il - 12 bis zu 28 tage nach tumorinokulation hemmten effizient das wachstum von primrtumoren des b16 - melanoms und des renca - nierenzellkarzinoms , wenn auch keine heilungen beobachtet wurden [ 7 ]  . 
 eine hnliche antitumorale wirkung , teils sogar mit tumorheilung , wurde fr mc38 - adenokarzinome und mca205 - fibrosarkome nach lokaler injektion von fr il - 12 kodierenden adenoviralen vektoren in der ersten woche nach inokulation beschrieben [ 13 ]  . 
obwohl die wirkung von il - 12 in diesem fall mit einer ctl - reaktion verbunden war , scheint insgesamt die auslsung einer ctl - reaktion in tumortragenden tieren ein seltenes ereignis zu sein [ 11 ]  . 
in bereinstimmung damit wurde mehrfach von einer eingeschrnkten funktion der ctl - zellen in den ersten tagen nach il - 12 - injektion berichtet [ 21 , 24 ]  . 
 obwohl nk - zellen wichtig fr die frhe eliminierung von metastatischen manifestationen muriner tumoren zu sein scheinen , ist ihre bedeutung im rahmen der primrtumortherapie unklar und schwankt je nach tumormodell zwischen vernachlssigbarer [ 31 , 59 ] und miger relevanz [ 7 , 24 , 57 ]  . die wichtigkeit von cd8 + - lymphozyten gegenber nk - zellen bei der behandlung mit il - 12 ab tag 14 nach inokulation wurde fr verschiedene murine tumoren gezeigt [ 7 ]  . 
dies wurde durch eine starke tumorassoziierte wie auch periphere erhhung spezifischer cd8 + - zellen nach il - 12 - behandlung von murinen p815 - mastozytomen belegt , obwohl zytotoxische tests von splenozyten kaum zytolytische reaktionen verzeichneten [ 11 ]  . 
die wirkung von il - 12 lsst sich aber nicht ausschlielich ber die induktion von ifndurch il - 12 erklren , weil ifnals isolierter wirkstoff nur in geringem mae antitumorale wirkung ausbt [ 6 , 11 , 43 ] und cd4 + - zellen zudem fr die antitumorale wirkung von il - 12 nicht erforderlich waren [ 7 ]  . 
functional diversity of helper t lymphoeiner erfolgreichen induktion der immunantwort beteiligt . whrend t - zellen weitgehend mhc - gebunden reagieren , knnen nk - zellen mhc - i - negative zellen direkt lysieren und werden im gegenteil durch mhc - i in ihrer effektivitt gehemmt . 
induktion von mhc - i , mhc - ii und icam - 1 auf melanomzellen und apc wurde entweder direkt oder mittels stimulation der ifn - - produktion durch nkund t - zellen beobachtet [ 61 ]  . 
eine dauerhafte immunitt durch t - zellen erfordert die mhc - abhngige prsentation von taa , whrend nk - zellen antigene ber ig - hnliche rezeptoren ohne bindung an mhc erkennen knnen . 
besonderes interesse hat il - 12 als stimulator der zellulren immunantwort durch induktion von ifnerregt . il - 12 wird nur in apc exprimiert und induziert gezielt die expression von il - 2 und ifnin th1 - zellen , so dass die ifn - - expression auf den relevanten zelltyp begrenzt wird . eine wirkung von il - 12 konnte in murinen tumormodellen besttigt werden , allerdings scheint die wirkung vom tumormodell abzuhngen und konnte nicht vollstndig ber die induktion von ifnverstanden werden . 
die rolle der nkzellen gegenber cd8 + - lymphozyten ist noch unklar , obwohl nk - zellen die hauptschliche frhe komponente der immunreaktion darstellen , whrend t - lymphozyten fr eine dauerhafte immunitt wichtig sind . 
die interaktionen der biologischen wirkung ionisierender strahlung mit dem zytokinnetzwerk erffnen neue mglichkeiten fr zytokine als biological response modifiers in kombination mit strahlentherapie , die weiter in prklinischen studien verfolgt werden sollten . 
the interface between innate and acquired immunity : glycolipid antigen presentation by cd1d - expressing dendritic cells to nkt cells induces the differentiation of antigen - specific cytotoxic t lymphocytes . 
immunohistochemical study of cfos - positive lymphocytes infiltrated into human squamous cell carcinomas of the head and neck during radiation therapy and its clinical significance . clin cancer res 1997 ; 3 : 23017 . 
interleukin - 10 - treated human dendritic cells induce a melanoma - antigen - specific anergy in cd8 ( + ) t cells resulting in a failure to lyse tumor cells . 
combination immunotherapy of b16 melanoma using anti - cytotoxic t lymphocyte - associated antigen 4 ( ctla - 4 ) and granulocyte / macrophage colony - stimulating factor ( gm - csf ) - producing vaccines induces rejection of subcutaneous and metastatic tumors accompanied by autoimmune depigmentation . 
il - 12 directly up - regulates the expression of hla class i , hla class ii and icam - 1 on human melanoma cells : a mechanism for its antitumor activity ? eur j immunol 1999 ; 29 : 176273 . 
4 urban & vogel strahlentherapie und onkologie original article 3 - d conformal hdr brachytherapy as monotherapy for localized prostate cancer a pilot study thomas martin1 , dimos baltas1 , ralf kurek1 , sandra rddiger1 , marina kontova1 , georgios anagnostopoulos1 , thomas dannenberg2 , thomas buhleier2 , georgies skazikis1 , ulf tunn2 , nikolaos zamboglou1 purpose : pilot study to evaluate feasibility , acute toxicity and conformal quality of three - dimensional ( 3 - d ) conformal highdose - rate ( hdr ) brachytherapy as monotherapy for localized prostate cancer using intraoperative real - time planning . 
 patients and methods : between 05 / 2002 and 05 / 2003 , 52 patients with prostate cancer , prostate - specific antigen ( psa ) 10 ng / ml , gleason score 7 and clinical stage t2a were treated . 
dose - volume histograms ( dvhs ) were analyzed to evaluate the conformal quality of each implant using d90 , d10 urethra , and d10 rectuacute toxicity was evaluated using the ctc ( common toxicity criteria ) scales . results : median d90 was 106% of dref ( range : 93115% ) , median d10 urethra 159% of dref ( range : 127192% ) , and median d10 rectum 55% of dref ( range : 3568% )  . 
 conclusion : 3 - d conformal hdr brachytherapy as monotherapy using intraoperative real - time planning is a feasible and highly conformal treatment for localized prostate cancer associated with minimal acute toxicity . 
 key words : prostate cancer brachytherapy hdr monotherapy intraoperative real - time planning strahlenther onkol 2004 ; 180 : 22532 doi 10.1007 / s00066 - 004 - 1215 - 4 konformale 3 - d - hdr - brachytherapie als monotherapie beim lokal begrenzten prostatakarzinoeine pilotstudie ziel : pilotstudie zur evaluation der praktikabilitt , akuttoxizitt und konformalen qualitt der konformalen dreidimensionalen ( 3 - d ) high - dose - rate - ( hdr - ) brachytherapie als monotherapie beim lokal begrenzten prostatakarzinom unter einsatz intraoperativer real - time - planung . 
 patienten und methodik : zwischen 05 / 2002 und 05 / 2003 wurden 52 patienten mit einem prostatakarzinom , psa - wert ( prostataspezifisches antigen ) 10 ng / ml , gleason - score 7 und klinischem stadium t2a behandelt . 
alle patienten erhielten ein implantat fr vier fraktionen hdr - brachytherapie in 48 h mit einer referenzdosis ( dref ) von 9 , 5 gy bis zu einer gesamtdosis von 38 , 0 gy . 
 ergebnisse : die mediane d90 betrug 106% von dref ( range : 93115% ) , die mediane d10 urethra 159% von dref ( range : 127192% ) , die mediane d10 rektum 55% von dref ( range : 3568% )  . 
hdr monotherapy for prostate cancer schlussfolgerung : die konformale 3 - d - hdr - brachytherapie als monotherapie unter einsatz intraoperativer real - time - planung erweist sich als praktikable und hochkonformale behandlung mit minimalen akuten nebenwirkungen beim lokal begrenzten prostatakarzinoeine lngere nachbeobachtungszeit ist zur beurteilung von spttoxizitten und biochemischer kontrolle notwendig . schlsselwrter : prostatakarzinom brachytherapie hdr - monotherapie intraoperative real - time - planung introduction the incidence of prostate cancer is increasing rapidly and has reached 700 , 000 cases annually in europe and north america at the beginning of the 21th century [ 4 ]  . 
the widespread use of the prostatespecific antigen ( psa ) test and transrectal ultrasound ( trus ) , allowing earlier detection , has resulted in a significant stage downmigration with a majority of patients newly diagnosed with organ - confined disease [ 12 ]  . 
gleason score and pretreatment psa level have a major impact on the risk of extraprostatic disease , seminal vesicle infiltration and regional lymph node involvement and can be used as prognostic factors for the definition of risk categories in patients with clinically organ - confined stages [ 25 ]  . 
patients with pretreatment psa levels 10 ng / ml and gleason scores 26 are considered to belong to the low - risk group , patients with psa levels 10 ng / ml and gleason score 7 to the intermediate - risk group . 
however , although improvements have been made in implantation techniques and dose - planning procedures for permanent seed implantation , there are still a number of critical issues to discuss . 
first of all , there are still potential difficulties to deliver the prescription dose to the entire prostate because of an inherent lack of total control in depositing the seeds precisely to the preplanned position inside the gland [ 28 ]  . 
 high - dose - rate ( hdr ) brachytherapy using temporary 192ir implants as a boost in combination with external - beam irradiation was established in the 1990s as conformal treatment technique for prostate cancer [ 2 , 3 , 6 , 8 , 9 , 15 , 17 , 21 ]  . 
the ability to optimize dwell times and positions of the 192ir source along the implant needles allows optimal dose conformity to the prostate , unaffected by the limitations of permanent seed implantation . 
started a study to investigate conformal hdr brachytherapy as monotherapy for favorable - stage prostate cancer to overcome these limitations . the william beaumont group concluded , in their publication , that the hdr monotherapy protocol was feasible and very well tolerated with an excellent coverage of the prostate gland [ 22 ]  . 
based on our own experiences with hdr brachytherapy and on published feasibility reports [ 22 , 29 , 36 ] , we started a pilot study of 3 - d conformal hdr brachytherapy as monotherapy for localized prostate cancer in 2002 . 
we used the newly developed hdr planning system swift ( nucletron , veenendal , the netherlands ) for intraoperative real - time planning of hdr brachytherapy during the implantation procedure . 
in addition , we evaluated the benefits of the intraoperative real - time hdr planning system swift by analyzing the conformity and quality of all implants using a dosevolume histogram - ( dvh - ) based methodology . 
patients were eligible to participate in the pilot study if they fulfilled the following inclusion criteria : biopsy - proven adenocarcinoma of the prostate , clinical stage t2a , psa level 10 ng / ml , and gleason score 7 . all patients in our series gave their informed consent after detailed information about the aims , risks and technique of the pilot study . 
median volume of the prostate gland before brachytherapy was 35 ml ( range : 1778 ml ) the patients were clinically staged according to the tnm classification system strahlenther onkol 2004 no . 
in 36 / 52 patients neoadjuvant androgen deprivation ( naad ) using lhrh agonists was started by urologists before inclusion of the patients into our protocol . the median duration of naad was 3 months ( range : 24 months )  . 
in the next step , we defined the contours of prostate , urethra and anterior rectal wall , visualized on the monitor simultaneously in coronal , transverse and sagittal plane views ( figures 1a to 1c ) as well as a 3 - d reconstruction . 
the generated virtual needles , the active and inactive source dwell positions , and the resulting isodose distribution were visualized immediately in relation to the anatomy in all plane views ( figures 3a to 3c ) and as 3 - d reconstruction . 
 after finishing the intraoperative planning , we started with transperineal implantation of flexible plastic needles ( 20 cm in length and 1.9 mm in diameter ) with metal stylets into the prostate through the template under trus control . figure 1a abbildung 1a figure 1b abbildung 1b figure 1c abbildung 1c figures 1a to 1c . 
intraoperative real - time planning for hdr brachytherapy of prostate cancer : contouring of prostate , urethra and anterior rectal wall , visualized simultaneously in transverse ( a ) , sagittal ( b ) and coronal ( c ) ultrasound views . 
intraoperative real - time - planung fr die hdr - brachytherapie des prostatakarzinoms : konturierung von prostata , urethra und anteriorer rektumwand , simultan abgebildet in transversaler ( a ) , sagittaler ( b ) und koronaler ( c ) ultraschallansicht . 
die generierten virtuellen nadeln und die aktiven und inaktiven haltepositionen der quelle werden sofort in transversaler ( a ) , sagittaler ( b ) und koronaler ( c ) ultraschallansicht abgebildet . figure 3a abbildung 3a figure 3b abbildung 3b figure 3c abbildung 3c figures 3a to 3c . 
intraoperative real - time planning for hdr brachytherapy of prostate cancer : virtual needles , active and inactive source dwell positions and the resulting isodose distribution are visualized immediately after dose optimization in transverse ( a ) , sagittal ( b ) and coronal ( c ) ultrasound views . 
intraoperative real - time - planung fr die hdr - brachytherapie des prostatakarzinoms : virtuelle nadeln , aktive und inaktive haltepositionen der quelle und die resultierende isodosenverteilung werden sofort nach der dosisoptimierung in transversaler ( a ) , sagittaler ( b ) und koronaler ( c ) ultraschallansicht abgebildet . 
after placement of all plastic needles , we performed a final 3 - d ultrasound acquisition to document and verify the final in situ needle positions and to calculate the isodose distribution and dvhs . 
the ptv was defined as the entire prostate gland without margins . the circumference of the whole rectum and urethra was delineated from 10 mm above to 10 mm under the ptv . 
then , 3 - d dose optimization was performed to the ptv surface [ 14 , 37 ]  . to evaluate the conformal quality of the implants , we used dvh - based parameters for ptv , urethra , and rectu the strahlenther onkol 2004 no . 
4 urban & vogel ct - based dvh parameters were used for dosimetric analysis of all hdr implants to evaluate and document the quality of 3 - d conformal hdr brachytherapy . 
 discussion hdr brachytherapy as monotherapy for patients with localized prostate cancer is a new conformal treatment technique which aims to overcome the potential limitations of ldr brachytherapy using permanent implants of 125i or 103pd seeds . the well - known phenomenon of prostate edema after seed implantation can strongly affect the aim to deliver 100% of the dref to the entire gland [ 34 ]  . 
they found a significant increase of the prostate volume very shortly after needle implantation , but very little change of the volume during the subsequent 3236 h of hdr treatment delivery . 
hdr monotherapy for prostate cancer d10 urethra ( dose delivered to 10% of the urethra ) was limited to 175% and the d10 rectum ( dose delivered to 10% of the rectum ) to 75% of the reference dose ( dref )  . 
the first fraction of hdr brachytherapy was delivered on the day of implantation , second and third fraction on day 1 after implantation , with at least 6 h between the fractions , and the fourth fraction in the morning of day 2 after implantation . 
the mean duration for transperineal implantation using the real - time planning system swift was 60 mall patients tolerated the implantation procedure and subsequent delivery of four fractions of hdr brachytherapy very well with minimal discomfort . 
we noted no grade 45 acute genitourinary toxicity . 11 / 52 patients developed increased stool frequency as acute grade 1 gastrointestinal toxicity , no patient developed acute grade 25 gastrointestinal side effects . toxicity data are presented in table 2 . 
hdr monotherapy for prostate cancer for the hdr implants was based on trus images at the time of the first fraction with all needles in situ , these images incorporated the postimplant edema and , therefore , had no negative effects on the ability to deliver the full prescription dose to the entire prostate . 
to evaluate the quality of the implants , we used dvh parameters for prostate , urethra and rectum and documented the d10 of organs at risk and the d90 of the prostate . 
 it is strongly recommended to evaluate the d90 and the rectal and urethral doses after permanent seed implantation , because these data provide an evaluation of the overall quality of the implant [ 13 , 23 , 35 ]  . 
noted a biochemical control rate of 92% after permanent seed implants with a d90 > 140 gy , but a control rate of 68 % after implants with a d90 < 140 gy [ 31 ]  . 
these dosimetric data demonstrate that the approach of hdr brachytherapy as monotherapy using intraoperative real - time planning results in an excellent conformal 3 - d dose distribution and coverage of the prostate gland with better d90 values compared to most published results of ldr brachytherapy [ 16 , 24 , 30 ]  . 
analyzing 45 patients treated with 125i implants , they found that in patients who developed rtog grade 01 urinary toxicity an average of 10 mm of the urethra was irradiated to doses > 400 gy compared to 20 mm in patients who developed grade 23 urinary toxicity [ 32 ]  . 
limited the dose to any segment of the rectum to < 75% of the prescription dose of hdr brachytherapy , but reported no rectal d10 parameters [ 22 ]  . 
using swift , we had the advantage of visualizing the ultrasound images of prostate , urethra and rectum simultaneously in transverse , sagittal and coronal plane views and as 3 - d reconstruction in real time . 
ct - based 3 - d postplanning after implantation : evaluation of the isodose distribution in one representative ct slice within and surrounding the prostate and within the normal tissues ( green : 50% isodose ; red : 100% isodose ; yellow : 125% isodose ; light blue : 150% isodose ; dark blue : 200% isodose )  . 
ct - basiertes 3 - d - postplanning nach implantation : evaluation der isodosenverteilung in einem reprsentativen ct - schnitt innerhalb und auerhalb der prostata und innerhalb der normalgewebe ( grn : 50% - isodose ; rot : 100% - isodose ; gelb : 125% - isodose ; hellblau : 150% - isodose ; dunkelblau : 200% - isodose )  . 
 for an accurate treatment delivery of fractionated hdr brachytherapy using one implant and one single treatment plan , it is important to observe the degree of needle movement that may occur between the fractions . 
 after the short - term follow - up of median 8 months ( range : 315 months ) , acute genitourinary toxicity was mild or moderate with only two patients requiring suprapubic catheterization for 8 and 10 weeks , respectively , as grade 3 genitourinary toxicity . 
to minimize the risk of urinary retention , we currently include only patients with a prostate volume < 60 ml and an international prostate symptom score ( ipss ) < 10 into the protocol . 
 a potential advantage of hdr monotherapy compared to seed implantation might be the laboratory and clinical evidence that the ( cid : 1 ) ( cid : 2 ) ( cid : 3 ) - ratio for prostate cancer is significantly lower than for other tumors [ 5 ]  . 
interestingly , the median time to psa nadir was 24 months ( range : 657 months ) , which is significantly longer than for external - beam irradiation or permanent seed implantation . 
 conclusion 3 - d conformal hdr brachytherapy as monotherapy using the intraoperative real - time planning system swift for 52 patients with localized prostate cancer was a feasible and welltolerated treatment modality after the short - term follow - up of median 8 months . 
clinical and biochemical control rates and late toxicity will be reported as soon as longer follow - up time is available . further developments of our conformal hdr brachytherapy technique include the use of a newly developed template which is fixed to the perineum for the entire treatment and the use of the ultrasound - based real - time hdr treatment plan for delivering the first fraction hdr brachytherapy intraoperatively . 
 strahlentherapie und onkologie original article positional variability of a tandem applicator system in hdr brachytherapy for primary treatment of cervix cancer analysis of the anatomic pelvic position and comparison of the applicator positions during five insertions jrn wulf , karoline popp , ulrich oppitz , kurt baier , michael flentje1 purpose : evaluation of the interand intraindividual applicator variability of multiple high - dose - rate ( hdr ) brachytherapy applications for primary treatment of cancer of the uterine cervix . 
 material and methods : retrospective analysis of 460 pairs of orthogonal x - ray films for conventional treatment in 92 patients with five intrauterine applications using an hdr tandem applicator . 
evaluation of the differences of the applicator position in all 460 applications ( interindividual variability ) , of the five applications in a single patient ( intraindividual variability ) and of the intraindividual variability relative to the applicator position at the first application . 
 results : the position of the applicator origin in the pelvis ranged from 23 mm cranial and 55 mm caudal to the top of femoral heads , 23 mm right and 27 mm left to the pelvic midline , and 653 mm dorsal to the mid of the femoral heads . 
 key words : cervical cancer radiotherapy brachytherapy applicator variability midline shielding conformal radiotherapy dose matching strahlenther onkol 2004 ; 180 : 21624 doi 10.1007 / s00066 - 004 - 1192 - 7 lagevariabilitt des ring - stift - applikators bei der hdr - brachytherapie zur primrbestrahlung des zervixkarzinoms . analyse der anatomischen lage im becken sowie vergleich der applikatorlage im verlauf von fnf einlagen ziel : evaluation der interand intraindividuellen applikatorvariabilitt im verlauf von fnf hdr - ( high - dose - rate - ) brachytherapie - einlagen bei der primrbehandlung des zervixkarzinoms . 
vergleich der applikatorposition bei allen 460 applikationen ( interindividuelle variabilitt ) , der fnf applikatorpositionen bei jeder einzelnen patientin ( intraindividuelle variabilitt ) sowie der intraindividuellen lagevariabilitt relativ zur lage bei der ersten applikation . 
 ergebnisse : die anatomische lage des applikatorursprungs im becken variierte zwischen 23 mm kranial und 55 mm kaudal des femurkopfes , 23 mm rechts und 27 mm links der beckenmittellinie sowie 653 mm dorsal der hftkopfmitte . 
 schlsselwrter : zervixkarzinom strahlentherapie brachytherapie applikatorvariabilitt mittelblock konformale radiotherapie introduction primary radiotherapy for cancer of the uterine cervix under curative intention is always performed as a combination of teletherapy ( external - beam radiotherapy , ebrt ) and brachytherapy ( intracavitary radiotherapy , icrt )  . 
while midline shielding has to consider the summarized dose distribution of all brachytherapy fractions , it usually has to be performed prior to completion of brachytherapy . therefore , prediction of the expectable applicator positions during brachytherapy is important to achieve the most appropriate shield at the most effective position . 
additionally , more advanced treatment techniques using three - dimensional treatment planning for ebrt and brachytherapy will have to solve the problem of localizing the brachytherapy volume and icrt dose in the pelvis prior to its application , if dose matching of both modalities is intended [ 10 ]  . 
 to address these requirements , a systematic analysis of the applicator positions in the pelvis relative to bony landmarks and its variability during five fractions of intracavitary highdose - rate ( hdr ) brachytherapy was performed . 
to ease the transfer of the results into clinical practice , the evaluation was related to three clinical scenarios : decisions have to be made prior to brachytherapy ( scenario a ) , after the first brachytherapy application ( scenario b ) , or after completion of brachytherapy ( scenario c )  . 
to address the first case , the interindividual applicator variability measured by the comparison of all applicator positions independent of a certain patient , for the second case the intraindividual applicator variability relative to the first application , and for the third case the intraindividual applicator variability comparing the five individual applicator positions of the 92 patients were analyzed . 
4 urban & vogel material and methods patient and treatment characteristics 92 patients treated between 1985 and 1997 for cancer of the uterine cervix by combined teleand hdr brachytherapy were analyzed . 
they received exactly five brachytherapy applications with fraction doses of 8.5 gy to manchester point a [ 9 , 13 ] and a percutaneous dose of 50 gy ( 4852 gy ) in 2 - gy fractions 5 ( cid : 1 ) / week , normalized to the isocenter . 
 in wrzburg , brachytherapy was performed as definite treatment for the central part of the pelvis and not as boost following ebrt according to the treatment concept introduced by rotte [ 11 ]  . 
for that purpose , the frequency of use of an identical or different applicator system ( ring and tube ) for all five applications in an individual patient was evaluated . 
 to describe the applicator position in the pelvis anatomically , a three - dimensional reference system ( figures 1a and 1b ) was defined , which was related to bony structures clearly visible on the x - ray films : craniocaudal : a virtual line connecting the top of the femoral heads in longitudinal direction , lateral : the midline of the bony pelvis in lateral direction , ap : a virtual horizontal line crossing the center of the femoral heads ( if , in lateral films , the two centers of the two femoral heads were not identical , e.g. , in a slightly rotated patient , the mid between both centers was used as reference level )  . 
the position of the applicator origin was described in millimeters from the bony reference systeorigin positions cranial , right or anterior to the reference system were measwulf j , et al . 
in this strategy , the central pelvis was excluded from dose in ebrt by using an angulated , biaxial , bisegmental rotational technique [ 11 , 15 ] instead of midline shielding . 
icrt was always performed under general or spinal anesthesia , which was terminated after completion of tight packing of the vagina in order to increase the distance of the normal tissue from the applicator system as much as possible . after application , the patient moved into supine position and the legs were supported by a roll of a cotton sheet of standard size . 
the films were exposed from ap ( 0 ) and lateral , from the patients right side ( 270 ) by the use of an isocentric x - ray device . 
three different sizes of the ring applicator with diameters of 26 , 30 , and 34 mm and five different sizes of the intrauterine tube applicator with lengths of 20 , 30 , 40 , 50 , and 60 mm were available and could be combined individually . 
the individual applicator combination of ring and tandem was chosen according to the clinical and ultrasound assessment of the length of the uterus and the size of tumor at the cervix at the time of insertion . 
 to achieve comparable data for applicator variability independent of the chosen size of the tandem applicator , the origin of the applicator system was chosen for evaluation : the applicator origin was defined according to icru report 38 [ 9 ] as the intersection of the ring and tube axes , which is located in the center of the ring plane and anatomically correlates to the cervix level . 
the longitudinal position was measured craniocaudal to the femoral heads , the lateral position relative to the pelvic midline , and the anterior - posterior position relative to a horizontal line crossing the mid of the femoral heads . 
the angulation of the applicator system was measured relative to a vertical ( a ) and horizontal ( b ) line crossing the applicator origin ( dashed lines )  . 
das kncherne referenzsystem ( weie linien ) befindet sich in lngsrichtung auf hhe der oberen begrenzung der hftkpfe , mediolateral in beckenmitte und in anterior - posteriorer richtung in der mitte der hftkpfe . 
additionally , the angulation of the tandem position in the pelvis was measured by the angle of the applicator axis connecting the applicator tip and origin compared to the sagittal pelvic axis in the ap film and the horizontal axis through the center of the femoral heads in the lateral film , respectively ( figures 1a and 1b )  . 
 the clinical value of evaluation of interand intraindividual positional variability of the applicator consists of its transfer into margins , which predict the most probable applicator positions under the three defined clinical scenarios : prior to brachytherapy ( no information on individual applicator position available ; scenario a ) , after the first insertion ( scenario b ) , and after completion of brachytherapy ( scenario c )  . 
while in the first case all potential applicator positions have to be considered ( = interindividual variability ) , in the second case intraindividual applicator variability is measured relative to the first insertion , and in the third case intraindividual variability of all five insertions is calculated . 
 nevertheless , evaluation of interindividual variability is related to the anatomic pelvic reference system , while in scenarios b and c the individual applicator positions are compared to each other and , thus , do not relate to a defined anatomic position . 
therefore , achievement of comparable data requires that the mean of deviation is normalized to a theoretical zero - position , which differs in the three groups : for scenario a , it is the anatomic mean position of all applications ( 14 mm caudal to the top of the femoral heads , 1 mm left to the pelvic midline , and 26 mm dorsal to the mid of the femoral heads ) ; for analysis of scenario b , the applicator position of the first insertion has to be used as reference ; for evaluation of scenario c , the mean position of the five applicator positions represents the individual reference . 
because of the small number of cases in some stages , three classes of one sd ( < 5 mm , 510 mm , and > 10 mm ) of the origin variability ( coordinates in three dimensions relative to the bony reference system ) were related to figo stage . 
under the assumption of a 100% reproducibility , the dose to point a should be ideally 42.5 gy ( = 5 ( cid : 1 ) 8.5 gy ) and change with increasing applicator variability . 
for each of the three scenarios , the manchester point a was defined as 20 mm cranial and 20 mm lateral to the theoretical zero - position of the applicator origin as described above . 
starting from this point , the mean dose to the leftand right - handed point a was calculated from the three - dimensionally shifted applicator positions according to each particular group . 
 results anatomic position of the applicator in the pelvis the anatomic position of the applicator origin in the pelvis relative to the bony reference system ranged between 23 mm cranial and 55 mm caudal to the acetabulum of the hip joint , 23 mm and 27 mm lateral to the pelvic midline , and 6 mm and 53 mm posterior to the mid of the femoral heads . 
the applicator angle in lateral direction was measured between 27 to the right and 19 to the lein the ap direction , the angle ranged between 1 and 50 in anterior direction compared to the horizontal plane ( table 2 )  . 
the anatomic standard position of the applicator in the pelvis reflected by the mean is 14 mm caudal to the top of the femoral heads , 1 mm left to the pelvic midline , and 26 mm dorsal to the mid of the femoral heads . 
 origin position relative to the reference system ( mm ) longi tudinal lateral anteriorlateral posterior angle of the applicator axis ( ) anterior posterior variability cranial caudal right left anterior posterior median mean strahlenther onkol 2004 no . 
applicator variability in hdr brachytherapy for cervix cancer two components of the tandem applicator , the diameter of the ring was unchanged in 68% ; in 5% it differed in only one application by 4 mm ( one size ) and in 17% by 8 mm ( two sizes )  . in 4% the diameter of the ring differed in two applications and in 4% in more than two applications . 
 interand intraindividual variability of the applicator origin the evaluation revealed the largest variability in scenario a , while it was lowest in scenario c ; the variability in scenario b was in between : sd of interindividual applicator variability was 12.9 mm in longitudinal , 5.1 mm in lateral , and 7.6 mm in ap direction ; sd of intraindividual variability was 5.5 mm in longitudinal , 2.5 mm in lateral , and 4.2 mm in ap direction table 3 . 
comparison of the variability of the applicator origin ( not related to anatomic points ) in all applications independent of the patient ( interindividual variability , scenario a ) , in five applications in a single patient relative to the first application ( scenario b ) , and in five applications in a single patient ( intraindividual variability , scenario c )  . 
while the standard deviation ( sd ) of the intraindividual variability is almost half that of the interindividual variability , the intraindividual variability relative to the first application is in between . 
vergleich der lagevariabilitt des applikatorursprungs ( ohne bezug zum knchernen becken ) patientenunabhngig bei allen applikationen ( interindividuelle variabilitt , szenario a ) , den fnf individuellen applikationen einer patientin relativ zur ersten applikation ( szenario b ) sowie den fnf applikationen jeder einzelnen patientin ( intraindividuelle variabilitt , szenario c )  . 
 impact of applicator variability on dose to manchester point a according to the different applicator variability of the three scenarios , inter - , intraand intraindividual variability relative to the first insertion , the calculation of the cumulated dose to point a ( brachytherapy only ) showed corresponding results . 
in scenario a , the 95% ci is covered by a margin of 12.6 mm ( craniocaudal ) , 5 mm ( lateral ) , and 7.4 mm ( ap ) added to the anatomic mean position . 
in scenario b , the 95% ci is covered by a margin of 8.7 mm ( craniocaudal ) , 3.9 mm ( lateral ) , and 6.7 mm ( ap ) added to the position of the first application . 
due to the different positional variability interindividually ( a ) , intraindividually relative to the first application ( b ) , and intraindividually with all five applicator positions known ( c ) , the cumulated mean dose to point a differs considerably . 
aufgrund der unterschiedlichen lagevariabilitt unterscheidet sich die summendosis an punkt a interindividuell ( a ) , intraindividuell relativ zur ersten applikation ( b ) und intraindividuell ( alle fnf applikatorpositionen bekannt , c ) erheblich . 
comparison of variability of the applicator origin interindividually ( a ) , intraindividually relative to the first application ( b ) , and intraindividually ( all five applicator positions known , c ) in longitudinal ( a ) , lateral ( b ) , and anterior - posterior direction ( c )  . 
vergleich der variabilitt des applikatorursprungs interindividuell ( a ) , intraindividuell relativ zur ersten applikation ( b ) und intraindividuell ( smtliche fnf applikatorpositionen bekannt , c ) in longitudinaler ( a ) , lateraler ( b ) und anterior - posteriorer richtung ( c )  . 
the proportion of patients with an sd 5 mm did not increase with stage in longitudinal and lateral direction as it might be expected , if initial tumor fixation with subsequent increased mobility due to treatment were of importance for positional variation of the applicator position . 
only in ap direction , a tendency to increased applicator variability with advanced figo stage was observed : while in 95% of patients with stage i the sd of applicator variability was < 5 mm , this proportion decreased to 78% in stage ii and to only 63% in stage iii . 
the relevance of the small variability in stage iv could not be evaluated statistically because of the small number of patients in this group ( n = 5 )  . 
the description of the anatomic position of the applicator origin , which can be achieved relative to the chosen bony reference system , allows the clinical use for midline shielding or the transfer of table 4 . 
this strongly suggests the acquisition of an individual applicator position , if treatment - related procedures such as positioning of a midline shield or three - dimensional dose matching of teleand brachytherapy have to be performed . 
therefore , using the applicator position of the first insertion for orientation is a fair approach , even if the applicator variability is somewhat larger as compared to the situation after brachytherapy has been completed . 
the analysis of the impact of tumor stage or increased mobility of the uterus due to tumor shrinkage during the treatment course did not reveal significant influence on the applicator position in this study . 
the most important influence on the applicator position might result from the individual anatomic position of the uterus and from vaginal packing , which might change from application to application to an unpredictable extent . 
therefore , these individual characteristics might explain the difference between interand intraindividual variability of the applicator position and support the conclusion that information on individual applicator position should be achieved whenever possible . 
 while the presented evaluation is the first study , which analyzes applicator variability with respect to different clinical scenarios , some authors have previously focused on reproducibility of the applicator system [ 2 , 35 , 7 , 14 ]  . 
since multiple fractions are applied in hdr brachytherapy , changes of applicator position and geometric difference in flexible or individually composed applicator systems such as tandem - ovoid combinations will have an influence on dose prescription and reporting according to icru 38 [ 9 ]  . 
they found spatial pelvic variability of the applicator with an sd of 6.5 mm in longitudinal , 5.9 mm in lateral , and 7.7 mm in ap direction for all patients . 
this corresponds well to the results of our study regarding interindividual variability in lateral and ap direction , with sd being 5.1 mm in lateral and 7.6 mm in ap direction . 
 [ 5 ] described the impact of applicator variability on the icru prescription points a , b , p and the icru reference points for the rectum and bladder analyzing 40 consecutive patients with cervical cancer receiving ebrt and two intracavitary implants with a fletcher - suit tandem and ovoids . the difference of the applicator position was measured relative to a pelvic bony reference system , which was similar to the system used in our study . 
the authors found a displacement of the individual reference points by 06 mfor individual patients , the minimal shift of the reference points ranged between 0 and 26 mm , which corresponds well to the results of the intraindividual variability found in our study . 
according to the authors , these differences might result in changes of dose rates at points a , b , p and the rectum and bladder of 33% to + 35% , which emphasizes the importance of information on applicator variability . 
 [ 4 ] evaluated the impact of positional and geometric variability of hdr applicators consisting of a ring , tandem and ovoids on dose derived from 20 patients with four applications each . 
 [ 3 ] compared standard midline shielding ( smls ) to individualized midline shielding ( imls ) according to the uterine geometry with respect to dose homogeneity at point a in 20 patients . 
the dose profiles of imls were compared with the corresponding dose profile of a 5 cm smls and were found to be dependent on the positional variation of point a right ( ar ) and point a left ( al ) with respect to the midline . 
however , with smls , the ar and al doses would have ranged from 22% to 77% ( 35 16% ) for ar and from 21% to 96% ( 47 28.2% ) for al leading to considerable inhomogeneity , which stresses the advantage of imls based on information of individual applicator positions . 
the influence of lateral deviation of the applicator position and the applicator angulation relative to the pelvic midline and the type of midline shielding ( standard vs . customized ) was analyzed and discussed by wolfson et al . 
for the total of 32 patients , they found deviations to the right of the midline of 023 mm ( median 4 mm ) and to the left of 028 mm ( median 3 mm )  . 
this observation corresponds well to the results of our study with maximum deviations of 23 mm to the right and 27 mm to the left side if all applications are considered . 
the percentage of dose deviation at point a ranged from 523% ( median 15% ) in the eleven patients who had their tandem deviated to the right of the midline and from 629% ( median 12.5% ) in the twelve cases with the tandem angled to the lebased on these results and the experience that a potential median overdose to point a of > 10% is possible if a standard midline shield is used , the authors changed to customized shielding at their institution . 
 [ 1 ] propagated a wedge - shaped midline shield after they had observed an overdose at point a of up to 12 gy with a lateral shift of 10 mm from the midline if a standard rectangular shield was used . 
 conclusion summarizing these reports , it can be concluded that there is considerable variability of applicator positions of several centimeters , usually about 2030 mm , with a substantial impact on the prescribed and reported dose to manchester point a of 2035% . 
potentially , it is dependent on the number of applications , the length of the time period between beginning and completion of brachytherapy , and the timing of brachytherapy ( starting already at the beginning vs . after completion of teletherapy ) during the combined course of teleand brachytherapy . 
nevertheless , in our study with a large number of five fractions , the first fraction at the beginning of or occasionally even prior to teletherapy did not reveal a correlation between applicator variability and figo stage . 
only these individual factors can explain the difference between interand intraindividual variability found in the present study . the comparison of interand intraindividual applicator variability suggests that information on individual applicator position is essential for precise prescription and reporting of strahlenther onkol 2004 no . 
in patients with changing applicator sizes it is due to the individual clinical assessment and the treatment concept used , whether the midline can be derived from the 95% ci of the applicator position from the first insertion or whether data from following insertions can be taken into account . 
 nevertheless , the precise longitudinal positioning of the customized shield in the ap portals remains a difficult and partially unresolved problem , because the volume irradiated in brachytherapy will shift at least in caudal direction due to extraction of the applicator system and the vaginal packing . although the normal tissue and organs at risk potentially will not move to the same extent as the uterus itself after applicator extraction , in our practice ( four - field box technique was introduced in 1999 ) the midline shield ( which is performed according to the first application ) is shifted caudally to the position of the uterine cervix in the ct scan performed for threedimensional treatment planning of teletherapy . 
the amount of shifting is calculated from the anatomic difference of the position of the applicator origin ( which represents the cervix level ) derived from brachytherapy to the cervix seen on the ct scan for teletherapy treatment planning . 
no data on anatomic structures , the tumor and organs at risk such as the rectum , the urinary bladder or the small bowel are available . to achieve more accuracy and reliability concerning the dose to anatomic structures , further studies on volume shifts from brachyto teletherapy , potential compression and distortions of the target and organs at risk by vaginal packing are necessary . 
this individual anatomic information is not only important for calculation of the dose to the tumor but also of the dose to organs at risk [ 8 ] , especially if more effective treatment approaches such as combined radiochemotherapy are used [ 6 , 12 ]  . 
 strahlentherapie und onkologie original article the potential role of tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 protein expression in colorectal carcinomas correlation with classic histopathologic factors and patient survival athanassios c . 
tsamandas1 , dimitrios kardamakis2 , panagiota ravazoula1 , vassiliki zolota1 , stavroula salakou1 , konstantinos tepetes3 , cristina kalogeropoulou2 , irene tsota2 , theodore kourelis4 , thomas makatsoris4 , dionissios karavias3 , chrisoula d . 
kalofonos4 , theodore petsas2 purpose : this study investigates the expression of tumor growth factors tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 in tissue material from patients with colorectal carcinoma and evaluates their correlation with known prognostic markers and patient survival . 
according to the tnm classification of malignant tumors , 26 tumors were identified as being stage i , 30 stage ii , 48 stage iii , and 20 stage iv , whereas 106 tumors were low - grade and 18 high - grade malignancies . 
on paraffin sections , the streptavidin - biotin technique using antibodies against tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 was applied . 
 results : tgf ( cid : 1 ) 1 protein was expressed in 88 out of 124 ( 71% ) carcinomas , whereas tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 proteins were detected in all tumors examined . 
normal colonic mucosal epithelial cells expressed tgf ( cid : 1 ) 2 ( significantly less as compared to neoplastic cells ; p < 0.01 ) and tgf ( cid : 1 ) 3 ( p > 0.05 compared to neoplastic cells ) , but not tgf ( cid : 1 ) 1 . 
 conclusion : this study shows that in adenocarcinomas of the colon , there is a differential expression of tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 . tgf ( cid : 1 ) 1 may be implicated in the pathogenesis of these tumors , since it is expressed only in neoplastic but not in normal cells . tgf ( cid : 1 ) 1 is related with an increased disease - free and overall survival and constitutes an independent prognostic factor . 
 key words : colorectal carcinoma transforming growth factor beta prognostic factors strahlenther onkol 2004 ; 180 : 2018 doi 10.1007 / s00066 - 004 - 1149 - x potentieller stellenwert der tgf ( cid : 1 ) 1 - , tgf ( cid : 1 ) 2und tgf ( cid : 1 ) 3 - expression bei kolorektalkarzinomen . 
korrelation mit klassischen histopathologischen faktoren und berleben ziel : diese studie untersuchte die expression der tumorwachstumsfaktoren tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 in gewebeproben von patienten mit kolorektalen karzinomen und prfte ihre korrelation mit bekannten prognostischen markern und mit dem berleben der patienten . 
nach der tnm - klassifikation wurden 26 tumoren als stadium i , 30 als stadium ii , 48 als stadium iii und 20 als stadium iv eingeordnet , whrend 106 tumoren lowgradeund 18 high - grade - malignome waren . 
paraffinschnittprparate wurden nach der streptavidin - biotin - methode mit antikrpern gegen tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 und tgf ( cid : 1 ) 3 behandelt . 
 1 department of pathology , 2 department of radiology and radiotherapy , 3 department of surgery , and 4 department of medical oncology , university of patras school of medicine , patras , greece . 
normale epithelzellen der dickdarmschleimhaut exprimierten tgf ( cid : 1 ) 2 ( signifikant weniger verglichen mit neoplastischen zellen ; p < 0 , 01 ) und tgf ( cid : 1 ) 3 ( p > 0 , 05 verglichen mit neoplastischen zellen ) , aber kein tgf ( cid : 1 ) 1 . 
die statistische analyse ergab strkere tgf ( cid : 1 ) 1 - expression in low - grade - karzinomen ( p = 0 , 009 ) und eine verstrkte prsenz von tgf ( cid : 1 ) 2 in fortgeschrittenen tumoren ( p = 0 , 008 )  . 
 schlussfolgerung : diese studie zeigt fr adenokarzinome des kolons und rektums unterschiede in der expression von tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 und tgf ( cid : 1 ) 3 . 
tgf ( cid : 1 ) 1 knnte in der pathogenese dieser tumoren eine rolle spielen , da es nur in neoplastischen , nicht aber in normalen zellen exprimiert wird . 
 schlsselwrter : kolorektalkarzinom transforming growth factor beta prognostische faktoren introduction colorectal carcinoma is one of the most common cancers equally affecting men and women , and its prognosis is related to several clinical and pathologic parameters . 
in addition , other variables such as primary tumor size , tumor margins , degree of peritumoral lymphocytic infiltration , angioinvasive growth , number and location of lymph node metastases , dna ploidy , oncogene expression , and cell proliferation have also been used to pursue prognostic information [ 21 , 22 ]  . 
besides surgery , however , adjuvant treatment ( consisting of radioand chemotherapy ) is also instituted ; more specifically , in cases of rectal carcinoma adjuvant treatment may be given preor postoperatively [ 3 , 11 , 25 ]  . 
tumor - produced cytokines include transforming growth factor beta ( tgf ( cid : 1 ) )  . tgf ( cid : 1 ) is a member of a large family of related factors that affect several functions at the cellular level both in neonatal and adult organisms [ 5 , 15 ]  . 
in vitro , these factors induce cell cycle arrest in normal and some malignant epithelial cells by inducing inhibitors of cyclin - dependent kinases [ 5 , 9 , 10 , 20 , 23 , 32 ]  . 
in addition , it is important that malignant epithelial cells including those of gastrointestinal origin display acquired resistance to the growth - inhibitory effects of tgf ( cid : 1 ) [ 5 , 15 ]  . 
the latter is accomplished by either inactivating mutations or the downregulation of tgf ( cid : 1 ) receptors , or by deletion or mutation of elements of the tgf ( cid : 1 ) signal transduction pathways [ 1 , 2 , 5 , 12 , 1518 , 31 , 35 ]  . 
previously , we have shown that in cases of colorectal carcinoma , tgf ( cid : 1 ) 1 is produced actively and specifically by neoplastic cells , whereas normal colonic mucosal epithelial cells do not express tgf ( cid : 1 ) 1 protein or mrna [ 33 ]  . 
 this study investigates the immunohistochemical expression of tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 proteins in tissue specimens of colon adenocarcinomas and their possible relation with classic histopathologic factors and patient survival . 
 patients and methods in this study , 124 consecutive surgical specimens of primary colorectal carcinomas were included and examined , from an equal number of patients who underwent surgical excision at the university hospital of patras , greece , during the period between 19901998 . 
the slides and the pathology report for each patient were drawn out from the files of the pathology department and reviewed in order to confirm the pathologic grade and stage . 
according to a modification in the grading system proposed by the who [ 13 ] , 106 adenocarcinomas were low - grade ( well and moderately differentiated ) and strahlenther onkol 2004 no . 
 cases were regarded as positive if at least 5% of tumor cells displayed cytoplasmic staining for tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 . 
both the number of positive immunostained cells and the total number of cells ( at least 500 cells ) at selected areas were determined by visual inspection of five different fields per section . 
for each field , a percent value for tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 in neoplastic and nonneoplastic colonic tissue was obtained by dividing the positive cells by the total number of cells counted . 
tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 protein expression in relation to various pathologic parameters . 
tgf ( cid : 1 ) 1 - , tgf ( cid : 1 ) 2und tgf ( cid : 1 ) 3 - expression in relation zu verschiedenen pathologischen parametern . 
 all 51 patients with rectal carcinoma underwent postoperative radiotherapy using a 6 - mv linear accelerator and an isocentric threeor four - field technique , in prone position with the bladder distended . 
chemotherapy ( 5 - fluorouracil 450500 mg / m2 , leucovorin 200 mg / m2 ) was given postoperatively up to a total dose of 24 weekly fractions , unless the patient was voluntarily withdrawn or unacceptable toxicity occurred . 
additionally , 5 - fluorouracil ( 400 mg / m2 ) was administered as a single rapid infusion on the first 3 and the last 3 days of radiotherapy as a radiosensitizer . 
 condition detection of tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 protein expression relied on immunohistochemistry performed on 4 mm thick paraffin sections from one selected block per case ; this block contained neoplastic and nonneoplastic colonic tissue . 
in tumors stage iii and iv , stains were also performed in blocks from lymph nodes with metastatic disease in order to record any possible differences in the expression of all three forms of tgf ( cid : 1 ) in primary and metastatic foci . 
sections were dewaxed in xylene , hydrated through graded concentrated alcohol , and quenched with h2o2 ( 0.6% ) in 100% methanol for 20 min to inhibit endogenous peroxidase activity . 
subsequently , the sections were washed three times with phosphatebuffered saline ( pbs ) , saturated in 0.1% bovine serum albumin ( pbs / bsa ; sigma , dorset , uk ) for 30 min , and incubated for 30 min with the primary tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 antibodies ( all dilutions 1 : 100 , santa cruz biotechnology inc . , santa cruz , ca , usa )  . thereafter , sections were incubated with the biotinylated multilink anti - igg immunoglobulin ( diluted 1 : 80 , biogenex , san ramon , ca , usa ) and streptavidin - peroxidase complex ( diluted 1 : 80 , biogenex ) for 30 min each . 
 results immunohistochemical expression of tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 in primary tumors the results are shown in table 1 . 
tgf ( cid : 1 ) 2 protein was detected in the cytoplasm of neoplastic ( figures 1e and 1f ) and normal epithelial cells ( figure 1g )  . 
tgf ( cid : 1 ) 3 protein was detected in both normal mucosa ( figures 1i and 1j ) and neoplastic tissue ( figures 1i to 1k )  . 
immunohistochemical expression of tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 proteins was detected in metastatic foci of lymph nodes in all cases ( figures 1d , 1h , and 1l )  . 
no relation between the presence of tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 and tumor grade nor between tumor location and expression of all three factors was recorded . 
 correlation between tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 expression and clinical outcome in a follow - up period of 3148 months after the initial surgery , 75.8% of the patients ( 94 / 124 ) are alive . 
 statistical correlation between the immunohistochemical results for tgf ( cid : 1 ) 1 and survival showed that tgf ( cid : 1 ) 1 expression was related both with longer disease - free survival and overall survival ( figures 3a and 3b ; p < 0.05 in each case )  . 
to the contrary , tgf ( cid : 1 ) 2 expression was correlated with worse survival ( r = 0.189 ; p = 0.035 ; figure 4 )  . 
 cox analysis of the relationship between tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 values and the various clinicopathologic parameters with survival revealed that besides tumor stage and grade , of the three tgf ( cid : 1 ) isoforms only tgf ( cid : 1 ) 1 constituted an independent prognostic factor ( table 2 )  . 
 discussion this study demonstrates that in cases of colon adenocarcinoma , first , tgf ( cid : 1 ) 1 may be involved in tumor pathogenesis since it is expressed specifically within neoplastic cells , second , in advanced tumor stages tgf ( cid : 1 ) 2 seems to be implicated in tumor progression , and third , the expression of tgf ( cid : 1 ) 1 is correlated with better survival and prolonged disease - free survival . we have also found that tgf ( cid : 1 ) 1 constitutes an independent prognostic factor , both tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 proteins are expressed in neoplastic and normal colonic mucosal epithelial cells , and tgf ( cid : 1 ) 2 protein expression is related with poor prognosis . 
tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 , and tgf ( cid : 1 ) 3 expression in colorectal carcinoma figure 3a abbildung 3a figure 3b abbildung 3b figures 3a and 3b . 
kaplan - meier survival curves showing the relation of tgf ( cid : 1 ) 1 protein presence or absence with disease - free survival ( a ) and overall survival ( b ) ( p < 0.05 in each case )  . 
furthermore , tgf ( cid : 1 ) 1 levels have been reported to be elevated in colon carcinoma [ 5 , 27 , 30 , 33 ] and the presence of tgf ( cid : 1 ) 1 has been linked with the progress and the metastatic potential of the disease [ 8 , 34 ]  . 
 a previous study , based on an animal tumor model , showed a positive correlation between tumor size and tgf ( cid : 1 ) concentration in plasma [ 30 ]  . 
 the results of the current study are in agreement with our previous study and suggest that tgf ( cid : 1 ) 1 is involved in the pathogenesis of colon carcinoma , since it is produced actively and specifically by the neoplastic cells [ 33 ]  . 
however , these authors studied 39 patients with colorectal carcinoma and a maximum follow - up of 3 years , whereas in the current study , we included 124 patients with colorectal cancer and a maximum follow - up of 12.3 years ( 148 months )  . 
thus , one can speculate that the different results regarding tgf ( cid : 1 ) 1 expression and survival or tumor progression recorded in these two studies may be attributed to their different design . 
 on the other hand , the current study showed that tgf ( cid : 1 ) 2 protein was detected both in neoplastic and normal colonic mucosal epithelial cells , but its expression in tumor cells was statistically higher . 
this finding , combined with the loss of tgf ( cid : 1 ) 1 expression toward high - grade adenocarcinomas , implies that selective targeting of augmented tgf ( cid : 1 ) 1 in low - grade ( well and moderately differentiated ) colon adenocarcinomas may serve as a potentially effective adjunct treatment or chemoprevention strategy . 
these results are somehow in agreement with a previous study [ 5 ] and suggest that tgf ( cid : 1 ) 2 is involved in late stages of colon adenocarcinoma progression . the fact that the three tgf ( cid : 1 ) isoforms exhibit different and non - overlapping actions during embryonic development [ 24 ] , combined with the differences in tgf ( cid : 1 ) 1 and tgf ( cid : 1 ) 2 expression in normal and neoplastic colonic mucosa and their relation with prognosis , as recorded in the current study , allows us to speculate that these two growth factors ( members of the same family ) seem to be involved in different stages of colorectal carcinogenesis and tumor progress . 
previous studies in knockout mice have demonstrated that targeted disruption of the mouse tgf ( cid : 1 ) 1 gene results in multifocal inflammatory disease , indicating a prominent role of tgf ( cid : 1 ) 1 in suppressing excessive inflammation [ 5 , 28 ]  . 
on the other hand , tgf ( cid : 1 ) 3 / mice display a mild phenotype characterized by a localized defect in epithelial cell differentiation which manifests itself in failure of the palatal shelves to fuse leading to cleft palate [ 5 , 19 ]  . 
these findings suggest that the three factors ( tgf ( cid : 1 ) 1 , tgf ( cid : 1 ) 2 and tgf ( cid : 1 ) 3 ) play different and non - overlapping roles during normal development . 
this may explain the differences , first , in the presence of these three factors in neoplastic and normal colonic mucosal epithelial cells and , second , in the correlation of tgf ( cid : 1 ) 1 and tgf ( cid : 1 ) 2 with patient survival . 
thus , we are tempted to speculate that tgf ( cid : 1 ) 1 is involved in the pathogenesis of less aggressive tumors ( low - grade tumors ) , whereas tgf ( cid : 1 ) 2 seems to affect tumor progression in late stages . 
another significant finding is that tgf ( cid : 1 ) 1 expression constitutes conclusion this study shows that there is a differential expression in the three isoforms of tgf ( cid : 1 ) in colorectal carcinomas and this difference reflects on the malignant phenotype and , subsequently , on the survival of patients . 
 material and methods : the conventional procedure of extracranial radiosurgery is contained in the following steps : adaptation of the vacuum mattress , planning ct , three - dimensional ( 3 - d ) treatment planning , ct repositioning , and irradiation . 
in the new procedure of continuous extracranial radiosurgery , a short treatment planning is often used for simple target shapes ( spherical , rotation - symmetrical ) , and the irradiation follows directly after the planning procedure . 
the high quality of the digitally reconstructed radiographs ( drrs ) of each field enables a high precision in dose application by the comparison with the verification radiograph and the drr ( elekta iview , hamburg , germany )  . 
 key words : extracranial radiosurgery lung cancer strahlenther onkol 2004 ; 180 : 2414 doi 10.1007 / s00066 - 004 - 1169 - 6 methodik der kontinuierlichen extrakraniellen radiochirurgie bei lungenkarzinomen unter verwendung von exomio , einer software zur 3 - d - ct - simulation hintergrund : die radiochirurgie von hirntumoren ermglicht eine hohe przision , die dazu fhrte , dass diese methode auf die behandlung von lokalisierten lungentumoren und lungenmetastasen bertragen wurde . 
 material und methodik : bei der konventionellen methode wird die therapie in folgenden schritten durchgefhrt : anpassung der vakuummatratze , planungs - ct , dreidimensionale ( 3 - d ) bestrahlungsplanung , ct - repositionierung und bestrahlung . 
der vergleich der drrs mit den verifikationsaufnahmen ergab eine mittlere positionierungsgenauigkeit von 3 , 3 mm ( 2 , 94 , 7 mm )  . schlussfolgerung : die kontinuierliche extrakranielle radiochirurgie eignet sich besonders fr kleine periphere lungentumoren . sie stellt eine ablaufoptimierung der konventionellen methode dar und ist vor allem fr kliniken mit eingeschrnkter ct - kapazitt interessant . 
 schlsselwrter : extrakranielle radiochirurgie bronchialkarzinom 1 department of radiooncology , university of marburg , germany , 2 department of computer science , university of applied sciences , wiesbaden , germany . 
thoracic stereotactic radiotherapy is a new noninvasive approach for the treatment of inoperable small localized lung tumors and lung metastases [ 2 , 6 , 10 , 11 , 14 , 18 , 19 ]  . 
we incorporate the use of the exomio system for three - dimensional ( 3 - d ) ct simulation of lung cancer , which has not been reported so far . 
 material and methods conventionally , extracranial radiosurgery is time - consuming , because of the high precision in repositioning required for single dose fractions of up to 30 gy [ 5 ] , thus , the patient is first positioned in a vacuum mattress which forms part of the stereotactic frame . 
then , with a delay of at least 1 day , treatment commences , preceded by a further ct to take any patient movement within the frame into account . during this repositioning procedure , the patients position is compared with the position in the previous planning ct . 
 in our new procedure of continuous extracranial radiosurgery , the dose is administered directly after the exomio preplanning ct ( section thickness and distance = 3 mm ) followed by helax 3 - d dose documentation , and the patient does not have to move from within the stereotactic frame ( see figure 1 )  . 
advantages of the altered procedure include simplification of the method based on the avoidance of a repositioning ct , a one - step planning and , from the patients point of view , the performance of therapy in just one session . 
the high quality of the drr of each field enables an excellent comparison with the verification radiograph before dose application using the elekta iview verification system ( hamburg , germany )  . 
the positioning accuracy was calculated by the square root of the sum of the squares of the craniocaudal and the ventrodorsal accuracy measured by the comparison of the tumor shape in the drr and the verification film in correlation to bony structures . 
the target was segmented as clinical target volume ( ctv ) in the lung window including macroscopic tumor with a safety margin of approximately 3 m the method of continuous extracranial radiosurgery was performed from october 2001 to april 2003 on five patients with inoperable pulmonary cancer . 
the average ct planning time amounted to 20 min ( including planning ct , data transfer to exomio , target definition ) , and the average patient transport time to the linear accelerator was 12 m parallel to the transport , exomio preplanning , data transfer to the helax planning system and dose documentation were performed . 
the mean positioning accuracy of the patient in the vacuum bed ( total shift ) was 3.3 mm ( range : 2.94.7 mm ) measured by comparison of the field outlines , tumor contour , central axis , and bony structures of the drrs with the verification films ( elekta iview ; see figure 3 )  . 
time - sparing coplanar multileaf collimated field arrangement is often sufficient corresponding to dose - volume histograms and results in tailored spherical or rather cylindrical figure 3a abbildung 3a figure 3b abbildung 3b discussion using extracranial radiosurgery , excellent local control rates ranging between 67 and 100% during a median follow - up of 819 months were reported in patients with lung cancer or lung metastases [ 2 , 6 , 10 , 11 , 14 , 18 , 19 ]  . 
 avoiding the necessity of a repositioning ct is a significant advantage , because , if on the patients second visit to the clinic a repositioning ct is obtained in the course of the conventional procedure , it is absolutely possible that organ movements as well as gastric and intestinal contents differ from those of the first visit . 
 in case of continuous extracranial radiosurgery , the patient stays longer in the body frame during fast 3 - d treatment planning , which demands accurate verification before dose application . 
even if a reduction of the high - dose region , theoretically , reduces the risk of pneumonitis [ 17 ] , we believe a safety margin of at least 1 cm to be necessary , because a small tumor movement during irradiation can cause local failure which means an essentially higher risk for the patient . 
the most important requirement for a curative approach in radiosurgery for small peripheral lung tumors is the exclusion of mediastinal and distant metastases . most lymph node metastases were found at the level of the bifurcation and the aortic arch [ 13 ]  . 
 today , radiologists are currently investigating invasive techniques such as radiofrequency ablation ( rfa ) [ 12 , 20 ] and laser intraluminal thermotherapy ( litt ) for liver metastases [ 16 ] and different tumor sites [ 15 ]  . 
the main advantage of extracranial radiosurgery compared to litt and rfa , however , is that it is noninvasive , and the preliminary excellent results are underlining the approach to simplify the method . 
 conclusion continuous extracranial radiosurgery can be performed for small lung tumors or lung metastases with approximately spherical volumes whereas for complex target volumes , mediastinal targets and pulmonary targets with increased breathing , ct repositioning remains the standard . 
it can also be performed with all fast planning systems and may therefore prove useful for cancer sites other than the lung and , thus , for many radiation oncology departments . 
the hyperfractionated schedules that were used in these european protocols were 72 gy in 1 gy bid fractions or 66 to 68 gy in 1 , 1 gy bid fractions . 
by using these protocols no case of brain necrosis was observed , indicating that hyperfractionation without acceleration including limited volumes strahlenther onkol 2004 ; 180 : 245 doi 10.1007 / s00066 - 004 - 9141 - z for high dose areas is a safe method . 
 current discussion prostate cancer radiotherapy in austria overview on number of patients , intention to treat , and treatment techniques based on data from 2007 gregor goldner1 , samir sljivic1 , renee oismueller2 , johanna salinger3 , michael mittermller4 , tanja langsenlehner5 , walter harder6 , gerhard kametriser7 , helmut eiter8 , elisabeth nechvile9 purpose : aim of this analysis was to assess the current status of prostate cancer radiotherapy in austria and compare these numbers to patients treated with surgery . material and methods : a questionnaire was sent to all 14 austrian departments asking about numbers of prostate cancer patients treated and indication of treatment ( primary , postoperative ) , as well as the treatment technique used ( 3d - crt , imrt , brachytherapy ) , treatment volumes ( with / without pelvic irradiation ) , dose applied , and differences in treatment concepts . 
additional pelvic lymph node irradiation was based on signs of positive nodes in 4 departments and based on roach formula / partin table in 5 departments . conclusion : about 25% of prostate cancer patients receive primary radiotherapy . 
treatment technique and dose applied was in all centers investigated in accordance with the german s3 guidelines . key words : prostate cancer radiotherapy number of patients overview austria strahlenther onkol 2011 ; 187 : 27983 doi 10.1007 / s00066 - 011 - 2268 - 9 strahlentherapie des prostatakarzinoms in sterreich . 
patientenzahlen , therapieindikation und - technik basierend auf dem jahr 2007 ziel : erfassung des aktuellen status zur strahlentherapie des prostatakarzinoms in sterreich und vergleich mit den zahlen operierter patienten . material und methodik : alle 14 radioonkologischen zentren erhielten , basierend auf dem jahr 2007 , einen fragebogen zur anzahl der behandelten patienten , behandlungsintention ( primr / postoperativ ) , behandlungstechnik ( 3d - crt , imrt , brachytherapie ) , zu zielvolumina ( mit / ohne beckenbestrahlung ) , dosis und unterschiedliche therapiekonzepte . ergebnisse : 9 von 14 zentren ( 65% ) nahmen an der befragung teil abbildung 1 . 
 1department of radiotherapy , university of vienna medical school , vienna , austria , 2department of radiooncology , donauspital , vienna , austria , 3department of radiooncology and radiotherapy , landesklinikum , wiener neustadt , austria , 4department of radiotherapy and radiooncology , landesklinikum krems , austria , 5department of radiation oncology , medical university graz , graz , austria , 6department of radiotherapy , klinikum klagenfurt am wrthersee , klagenfurt , austria , 7department of radiotherapy and radiooncology , landeskrankenhaus salzburg , salzburg , austria , 8department of radiooncology , landeskrankenhaus feldkirch , austria , 9department of radiotherapy , city hospital , hietzing , vienna , austria . 
 schlsselwrter : prostatakarzinom strahlentherapie patientenzahlen berblick sterreich introduction prostate cancer is the most common malignancy in austrian men with about 5 , 000 diagnosed patients per year and about 60% of them showing local disease [ 12 ]  . 
in general , treatment options for local prostate cancer patients include radical prostatectomy , radiotherapy external beam radiotherapy and / or brachytherapy , hormonal therapy , and active surveillance . in austria , most the patients diagnosed with primary prostate cancer are referred to surgery or radiotherapy . 
both of these radical treatment options show , depending on risk parameters , a high potential of tumor control and are considered as equivalent [ 2 , 3 , 611 , 16 ]  . 
in addition , radiotherapy has been shown to be an effective and important treatment tool in patients presenting with biochemical and / or clinical recurrence after radical prostatectomy [ 1 , 13 , 15 ]  . the aim of this analysis was to assess the current status of prostate cancer radiotherapy in austria . 
furthermore , this analysis should allow an estimation of the potential for upcoming studies and was considered the basis for optimizing prostate cancer radiotherapy within all austrian radiation departments involved . material and methods in autumn 2008 , a questionnaire asking about primary and postoperative prostate cancer radiotherapy was sent out to all 14 austrian departments for radiooncology . 
the departments were asked to answer the questionnaire according to current status and to give if indicated the numbers of patients based on the year 2007 . for primary prostate cancer patients , a differentiation according to treatment technique 3d - crt ( three - dimensional conformal radiotherapy ) , imrt ( intensity - modulated radiation therapy ) , permanent interstitial brachytherapy ( seeds ) , teletherapy combined with hdr ( high dose rate ) brachytherapy , and hdr brachytherapy alone was assessed . 
regarding treatment volume , the centers were asked if only local radiation at the prostate / seminal vesicles region was performed or if the pelvic lymph nodes were included within the volume to treat and on which parameters this decision on different treatment volumes was based . 
finally , the questionnaire asked about regularity of follow - up visits and duration of follow - up within the departments for radiotherapy . results the questionnaire was answered by 9 ( 65% ) departments , while 5 departments decided not to participate ( figure 1 )  . 
a total of 1 , 191 prostate cancer patients were treated in the year 2007 in these 9 departments resulting in an average number of 132 prostate cancer patients / year and department . 
 primary radiotherapy the majority of primary prostate cancer patients , 764 patients ( 90% ) , were treated using the 3d - crt technique applying a total local dose of 7074gy . 
 the decision to include pelvic lymph nodes was based in 4 departments on the roach formula , in 1 department according to the partin table , and in 4 departments pelvic lymph nodes were included only in case of ct - positive nodes . 
the cranial border of the pelvic field was defined in 3 departments by the linea terminalis and in 6 departments by the bifurcation of the iliac communis . a differentiation regarding total dose applied according to risk groups ( low , intermediate , and high ) was performed in 5 centers . 
 postoperative radiotherapy ( adjuvant and salvage therapy ) three dimensional conformal radiotherapy was performed in all 344 postoperative prostate cancer patients , of whom 279 patients ( 81% ) received local treatment to the prostatic bed up to a dose of 6072gy and 42 patients ( 12% ) were treated with inclusion of the pelvic nodes up to a dose of 4550.4 gy followed by a boost to the prostatic bed of 1622 gy . 
 although , we were able to only present the data from 9 / 14 centers , we are confident that these data show a valid overview especially regarding the number of patients treated and indication of treatment . 
a total of 847 primary prostate cancer patients and 344 postoperative ( adjuvant and salvage ) patients were treated at these 9 participating centers , resulting in an estimate of 1 , 317 primary prostate cancer patients and 535 postoperative patients for all 14 austrian departments . one of the reasons to present the data based on the year 2007 was to be able to compare the numbers of radiotherapy patients to the data derived from the central austrian agency for statistics with regard to incidence rates and to compare the data to patients treated by surgery . 
a total of 5 , 107 patients were diagnosed with prostate cancer in austria in 2007 and 3 , 725 radical prostatectomies were performed in austria in 2007 [ 12 ]  . 
this reveals that a high percent of prostate cancer patients receive radical treatment ( surgery or radiotherapy ) , while hormonal therapy alone or active surveillance is less frequently performed . 
furthermore , surgery is selected about three times more often as the first treatment option compared to radiotherapy , although primary radiotherapy ( external beam or brachytherapy ) is regarded as an equivalent treatment option to surgery , showing comparable tumor control rates . 
prostate cancer is diagnosed after biopsy conducted by the urologist who might prefer surgery to radiotherapy as the treatment option and consequently patients are more often offered to surgery . in contrast to austria , the proportion between radiotherapy and surgery is about 2 to 1 in england in favor for radiotherapy , but most of the patients receive no radical treatment at all . 
 [ 4 ] reported on 21 , 334 primary prostate cancer patients treated in northern and yorkshire region in england during the period 20002006 using the data from northern and yorkshire cancer registry and information service . 
by analyzing the data of 3 , 486 patients , they were able to show that about 43% of patients received surgery ( radical prostatectomy or transurethral resection ) compared to 14% of patients receiving radiotherapy as the initial treatment . 
but there were huge differences between the participating countries , e.g. , in eindhoven , the netherlands patients are more often irradiated ( 36% ) than operated ( 31% ) , whereas in genoa , italy only 14% of patients were irradiated and 36% of patients received surgical treatment . in 2009 , the german s3 guidelines on prostate cancer therapy were published [ 3 ]  . 
dose has gradually been increased over the last decade to achieve better tumor control rates [ 2 , 7 , 10 , 11 ] and during the perior from 19982000 local dose in austria was also in the range of 6674gy [ 6 , 7 ]  . no consensus whether primary prostate cancer presenting with a certain risk profile should receive pelvic irradiation exists until now . 
in addition , in austrian radiotherapy departments , no consensus about additional lymph node irradiation exists 5 centers include the nodes depending on the partin table or roach formula and 4 centers include only if there is evidence of positive nodes . the analysis presented the data based on the year 2007 and only 1 center started with imrt prostate cancer treatment , whereas about 90% of patients received 3d - crt mainly using the four field box technique . 
many studies were able to demonstrate the benefits of imrt in terms of improved biochemical control by increasing dose without or only moderate increase of toxicity [ 8 , 9 ]  . 
the remaining 2 centers currently do not have the technical equipment for imrt . more than 800 primary prostate cancer patients treated in 9 departments per year in austria receive radiotherapy and about 350 patients were treated with salvage or adjuvant intention . 
dose applied ranges from 7078 gy for primary patients and from 6072 gy for postoperative patients , which is in accordance with the german guidelines . acknowledgment the authors would like to thank ptter , univ.doz. 
devries , and knocke - abulesz for their support . original article simple proposal for dosimetry with an elekta iviewgttm electronic portal imaging device ( epid ) using commercial software modules janett liebich , jrg licher , christian scherf , eugen kara , nadine koch , claus rdel , ulla ramm1 background : an electronic portal imaging device ( epid ) is used to control for patient setup and positioning during fractionated radiotherapy . 
the purpose of this study was to investigate a simple guidance for dosimetry with an elekta iviewgttm epid using commercial software modules . material and methods : epid measurements were performed using an elekta iviewgttm epid on a linear accelerator with 6mv x - ray beathe epid signal was studied for reproducibility , as well as characteristics as a function of dose , dose rate , and field size . 
fr alle felder stimmen die ergebnisse fr das kalibrierte epid im vergleich mit dem bestrahlungsplanungssystem mit abweichungen von maximal 23% innerhalb des feldes berein regionen mit hohen dosisgradienten ergaben sich grere abweichungen von bis zu 6% . 1klinik fr strahlentherapie und onkologie im zentrum der radiologie , klinikum der johann wolfgang goethe - universitt frankfurt / main , frankfurt am main , germany . received : may 17 , 2010 ; accepted : february 4 , 2011 published online : april 26 , 2011 strahlenther onkol 2011 no . 
an average of all frames acquired during radiation time , normalized to the maximum value of 65 , 535 ( 16 bit ) , is stored as a raw image ( praw )  . 
all images were processed to correct for individual pixel sensitivity and offset introduction the electronic portal imaging device ( epid ) is used to control for patient setup and positioning during fractionated radiotherapy . 
due to the rising complexity and conformity of irradiation techniques , the demand for an accurate verification of the dose delivered to the patient has also increased [ 9 , 20 , 22 ]  . 
the possibility of using the epid to acquire dosimetric information has been increasingly extended . applications of portal dosimetry have been reported for the type of epids based on a liquid - filled ionization chamber matrix [ 2 , 5 , 6 , 26 , 27 ] and the ccd camera - based epids [ 16 ]  . 
more recently , amorphous silicon ( a - si ) - based epids have been developed with excellent image quality [ 17 ] and requirements for dosimetric purposes [ 3 , 7 , 8 , 10 , 12 , 13 , 15 ]  . 
 so far only a few reports have addressed dosimetric applications for this type of detector from elekta [ 14 , 18 , 24 , 25 ]  . there are various possible approaches to portal dosimetry [ 21 ]  . 
the purpose of this study was to develop a calibration method to convert flat panel portal images to the equivalent water dose deposited in the detector plane at the depth of maximum dose in pmma ( polymethylmethacrylate , plexiglass , mass density = 1.18 g / cm3 ) and the comparison with the treatment planning system ( tps )  . 
to predict the portal dose image , an option that is not yet widely available in commercial treatment planning systems , we attempted to establish a preliminary work protocol . the most accurate way of modeling scattering processes is to utilize monte carlo computation [ 1 , 4 , 23 ]  . 
 material and methods experimental measurements were performed on a linear accelerator ( elekta ) with 6 mv x - ray beathe associated epid is an elekta iviewgttm a - si flat panel , mounted on the linac gantry . 
simple proposal for dosimetry with an electronic portal imaging device ( epid ) where ffij performs the correction for individual pixel sensitivity , by acquiring an image covering the whole sensitive detector area , ffij denotes the mean value of all individual pixel values of ffij , and dfij is a dark field image , acquired without irradiation , which serves as an offset correction . 
to obtain the real accumulated value , the indicated pixel value has to be divided by this factor . the basic data for the algorithms of the treatment planning system and the absolute dosimetry as quality assurance for our linacs were measured with an ionization chamber alternatively in a water tank or in a pmma phantofor experimental simplification , dose measurements were performed with an ionization chamber 0.3 cm3 , ptw freiburg , at the depth of maximum dose in a pmma phantom at 160 cm sdd . 
the pmma phantom has a thickness of 8 cm , the ionization chamber is placed at 1.5 cm depth from the phantom surface , i.e. , at the depth of maximum dose in pmma . for calibration purposes , the epid is irradiated with a field covering the whole detector area . 
figure 1 shows as an example the crossplane profile of a 6 mv field at depth of maximum dose and sdd of 160 cm , which shows the characteristic horns and dip . 
for individual pixel sensitivity correction a calibration matrix is defined that the pixel values of this profile were scaled as equal ( formula 1 , the red line in figure 1 )  . 
 consequently , the calibration pixel matrix has to be recalculated from the acquired image , i.e. , by convolving the epid image some groups use only a radial symmetwith the field profile . 
a more realistic way is to correct the whole area of figure2.ratio of the measured dose and the pixel value of the epid as a calibration factor that is dependent on the pixel value ( in 105 mgy ) for the epid to calculate the dose , fitted by an analytic funcx / t2 , whereby y is the calibration factor ( mgy ) and x is the pixel valtion y ue , with constant y0 = ( 42.640.08 ) * 105 mgy , a1 = ( 3.920.51 ) * 105 mgy , a2 = ( 1.30.11 ) * 105 mgy , t1 = ( 10 , 3321 , 853 ) und t2 = ( 223 , 46452 , 341 )  . y0 + a1 a2 x / t1 abbildung2.quotient aus der gemessenen dosis und dem pixelwert des epids als pixelwertabhngiger kalibrierfaktor ( in 105 mgy ) fr das epid zur umrechnung in dosis , gefittet mit einer anax / t2 , wobei y den kalibrierfaktor ( mgy ) und x den lytischen funktion y pixelwert bezeichnen , mit den konstanten y0 = ( 42 , 640 , 08 ) * 105 mgy , a1 = ( 3 , 920 , 51 ) * 105 mgy , a2 = ( 1 , 350 , 11 ) * 105 mgy , t1 = ( 10 3321 853 ) und t2 = ( 223 46452 341 )  . y0 + a1 a2 x / t1 the field , realized by measuring a dose correction map with , e.g. , a 2d array ( ptw ) at depth of maximum dose in pmma . as treatment planning system ( tps ) , we used oncentra masterplan ( nucletron )  . 
we cloned the pmma phantom , used for reference dose measurements , and set the layer according to the depth of 1.5 cm at the distance of 160 cm , distance of epid detector plane . 
simple proposal for dosimetry with an electronic portal imaging device ( epid ) where y is the calibration factor ( mgy ) and x is the pixel value ; y0 , a1 , a2 , t1 , and t2 are constants which were defined by the fit of the measurements to the function . dependencyondoserate to prove the epid response according to dose rate variations , the monitor units per minute of our linac were changed from 50 , 100 , 200 , and 400 mu / mthe doses were set at 10 , 20 , and 50 mu . 
as an example , the graph for 20 mu of the relative output factors of the epid compared to the measurements with the reference system is shown in figure 3 . 
this implies different scattering characteristics of the epid , which has to be adjusted with a correction factor for each pixel , e.g. , based on the beam - zone method [ 19 ] and the difference between the output factors of the epid and the reference system . epidcalibrationmodel summarizing the correction procedure explained above the epid calibration model is implemented . 
vergleich der relativen output - faktoren in abhngigkeit verschiedener feldgren des epids und den messungen in einer wasserquivalenten tiefe von 1 , 5 cm und einem sdd = 160 cm , normiert auf die referenzfeldgre von 10 10 cm2 . results epidsignalcharacteristics : reproducibility the long - term stability and reproducibility of the detector were observed by acquiring images every 12 weeks under fixed conditions . 
any change of various parameters of the linac or the epid , e.g. , during a servicing , resulted in a new calibration of the epid pixel value to dose . 
thus , the maximum oscillation was about 2% . dependencyondose to study the epid signal characteristics as a function of dose , we plotted the resulting pixel value by varying the number of monitor units from 1100 . 
the graph was fitted by an analytic function , which was chosen because of the progression the measured points show and the aim to fit the graph for satisfaction : strahlenther onkol 2011 no . 
a comparison of the results for a 10 10 cm2 field with 20 mu from the treatment planning system relative to the epid , the points that do not fulfill the - index ( 3% and 3mm ) are marked as failed points . 
b comparison of the results for a field of an imrt plan for head and neck irradiation from the treatment planning system relative to the epid , the points that do not fulfill the - index ( 3% and 3mm ) are marked as failed points . 
a vergleich der ergebnisse fr ein 10 10 cm2 mit 20 mu des bestrahlungsplanungssystems relativ zum epid ; als fehlpunkte sind diejenigen gekennzeichnet , die den - index ( 3% und 3mm ) nicht erfllen . 
b vergleich der ergebnisse fr das feld eines imrt - planes fr die kopfhals - bestrahlung vom bestrahlungsplanungssystem , relativ zum epid ; als fehlpunkte sind diejenigen gekennzeichnet , die den - index ( 3% und 3mm ) nicht erfllen . 
by comparing the two results , only a few inconsistencies in the region of field edge , illustrated in figure 4a , were observed . considering the necessary corrections for epid dosimetry pointed out by the investigation of the epid signal characteristics , we tested an imrt field . 
the evaluation with the - index ( 3% and 3mm ) indicates a very good agreement between the array and the epid as shown in figure 4c . discussion to study the practicability of the epid for dosimetric purposes , the physical and dosimetric properties as well as the response depending on various external parameters were investigated . 
because of spebecause of specific scattering properties , the epid shows a different behavior when varying the field size compared to the reference syste this difference only occurred from the different scattering in the epid versus the scattering in the pmma , because the conditions for the beam outcome from the head were the same . the gamma evaluation indicates very good correlation between the epid and 2d array measurement systems . 
the inconsistencies between the epid and tps may indicate the accuracy of the calculation of the tps compared to the dose distribution delivered by the linac for this imrt field . 
the specific scattering properties of the epid and the modeling of the field gradient of the tps depending on the resolution of the calculation matrix ( usually 3 mm ) and the right modeling of the interleaf leakage of the algorithm make it difficult to evaluate the field edge region precisely . 
no build - up layer was used for the epid dosimetry in order to maintain the possibility of using the epid at varying gantry angles ( not just zero degrees ) [ 24 ]  . 
this completely empirical calibration model is based on measurements and , therefore , does not require prior knowledge of the monte carlo simulation . the gamma evaluation indicates very good correlation between the acquired epid image and measured dose with a 2d array . 
simple proposal for dosimetry with an electronic portal imaging device ( epid ) this method maybe restricted to geometries without absorbers in the beathe presence of a patient can modify the epid response due to the additional scattered radiation . 
 in this study it could be shown that the epid , beyond the use for the control of the patient setup during radiotherapy , can also be used for dosimetric purposes . 
further refinement of the calibration model is needed to increase the accuracy of the procedure . original article feasibility and toxicity of concomitant radio / immunotherapy with mabthera ( rituximab ) for patients with non - hodkin 's lymphoma results of a prospective phase i / ii study alfred haidenberger1 * , sabine fromm - haidenberger2 * , alexander . 
de vries3 , bela - andre popper1 , michael steurer4 , ira skvortsova1 , johanna kantner4 , eberhard gunsilius4 , peter lukas1 purpose : non - hodgkin 's lymphomas ( nhl ) have a high radioand chemosensitivity . 
the purpose of this study was to evaluate the feasibility and toxicity of radiotherapy with concomitant application of rituximab in nhl patients . patients and methods : a total of 21 patients with b - cell lymphoma ( stage i : n = 11 ; ii : n = 5 ; iii : n = 1 ; iv : n = 4 ) were included in this study , treated with radiotherapy of 3040 gy and weekly application of rituximab ( 375mg / m2 )  . 
randomized trials are necessary to clarify the benefit of this treatment approach and its applicability . key words : rituximab radiotherapy non - hodgkin 's lymphoma radio / immunotherapy strahlenther onkol 2011 ; 187 : 3005 doi 10.1007 / s00066 - 011 - 2169 - y durchfhrbarkeit und toxizitt einer kombinierten radioimmuntherapie mit mabthera ( rituximab ) als neue behandlungsoption fr patienten mit non - hodkin - lymphomen ergebnisse einer prospektiven phase - i / ii - studie ziel : non - hodgkin - lymphome ( nhl ) haben eine hohe chemo - / radiosensitivitt und zeigen zunchst ein sehr gutes therapieansprechen . 
ziel dieser pilotstudie war die evaluierung von durchfhrbarkeit und toxizitt einer radiotherapie in kombination mit dem monoklonalen antikrper rituximab . patienten und methodik : 21 patienten ( pts ) mit nhl ( stadium i : 11 , ii : 5 , iii : 1 , iv : 4 ) wurden mit 3040 gy radiotherapie und 1x wchentlicher konkomittanter applikation von rituximab ( 375 mg / m2 ) behandelt . 
 * both authors contributed equally to this work . 1department of radiotherapy / radiooncology , medical university innsbruck , innsbruck , austria , 2institute of radiology , hospital gmunden , gmunden , austria 3department of radiotherapy / radiooncology , hospital feldkirch , feldkirch , austria , 4department of hematology , medical university innsbruck , innsbruck , austria . received : may 10 , 2010 ; accepted : february 4 , 2011 published online : april 26 , 2011 strahlenther onkol 2011 no . 
randomisierte studien sind notwendig , um nutzen und anwendbarkeit dieser kombinierten therapie beim nhl zu prfen . schlsselwrter : rituximab radiotherapie non - hodgkin - lymphom radioimmuntherapie were inclusion of the patient in another clinical study , known hypersensitivity for rituximab , second malignancy . 
in stage i and ii low - grade b - cell lymphoma with good prognostic factors , radiotherapy is the standard treatment , achieving local control rates of 95% and 50% of the patients are relapse free at 10 years [ 6 , 13 , 17 , 21 , 23 , 30 ]  . 
in patients with more aggressive histologies and / or advanced stages , the application of chop ( cyclophosphamide , doxorubicin , vincrstine , and prednisone ) chemotherapy with or without rt showed 5 - year survival rates of 6895% [ 14 , 19 , 27 ]  . 
although indolent and aggressive nhls are initially responsive to rt with or without chemotherapy , approximately 50% of patients relapse after 1015 years [ 6 , 30 ]  . rituximab , a mouse / human chimaeric igg ( 1 ) - kappa monoclonal antibody that targets the cd20 antigen found on the surface of malignant and normal b lymphocytes , is another therapeutic approach in the treatment of nhl . 
although the cytotoxic effect of rituximab on cd20 - positive malignant b - cells is not fully understood yet , it seems to involve complement - dependent cytotoxicity , antibody - dependent cellular cytotoxicity , and induction of apoptosis [ 1 , 9 ]  . 
 the use of combined therapy with rituximab and cytotoxic agents is supported by in vitro data indicating that rituximab sensitizes tumor cells to effects of conventional and newer chemotherapeutic agents [ 2 ]  . 
 [ 28 ] , proving that rituximab modulates radiation - triggered cell cycle distribution followed by apoptosis development ( figure 1 )  . considering the high radiosensitivity of b - cell lymphoma cells , the concept of a combined radio / immunotherapy seems very attractive , but no data for this treatment approach are available in literature yet . 
thus , based on the facts outlined above , this study was designed to evaluate toxicity and feasibility of radiotherapy and concomitant application of rituximab in nhl patients . patients and methods figure 1 . 
inhibition of c - myc , bcl - xl ( b - cell lymphoma - extra large ) , xiap ( x - linked inhibitor of apoptosis protein ) , survivin and hsp 70 ( heat shock protein 70 ) expression and up - regulation aif ( apoptosis - inducing factor ) lead to mitochondrial membrane potential dissipation , caspase activation , and radiation - induced apoptosis . 
mutant p53 is a nonobligatory component of this cascade ( [ 25 ] , urheberrechte : elsevier )  . between december 2005 and december 2006 , 21 patients with nhl were included in this study . 
inclusion criteria were histological proven nhl stage iiv , age between 18 and 80 years , good general status ( karnofsky index 80100% ) , written informed consent , and good patient compliance . 
in addition , a fluorodeoxyglucose positron emission tomography ( fdg - pet ) scan was performed because it is more sensitive than mri and ct and is playing an increasing role in the diagnostic and staging of lymphoma [ 16 ]  . 
 radiotherapy patients with indolent nhl received a total dose of 30 or 40 gy involved field ( ifrt ) , aggressive lymphomas were treated with a total dose of 40 gy extended field radiotherapy ( efrt ) , or ifrt of bulky disease , given in conventional fractionation ( 1.82 gy / day , 5 fraction / week ; table 1 )  . 
 for ifrt planning , clinical target volumes ( ctv ) consisted of nodal regions involved with nhl at the time of diagnosis ; the planning target volume ( ptv ) comprised the addition of a 5 mm margin to the ctv . 
initial infusion rate was 50mg / hour for the first 30 minutes , which was increased in 50 mg / hour increments every 30 minutes to a maximum dose of 375mg / m / week . 
three patients continued rituximab therapy after rt for 12 years . toxicity and follow - up toxicity was assessed according to the common terminology criteria adverse events ( ctc ) [ 3 ] and the who performance scale . 
completion of treatment was defined as irradiation with 3040 gy total dose and 34 cycles of concurrent rituximab infusions . all patients received a fdg - pet and ct scan 6 weeks after treatment to assess treatment response . 
radiation dose reduction and omission of rituximab in the third week of radio / immunotherapy was necessary in 1 patient due to radiation - induced mucositis grade 3 , strahlenther onkol 2011 no . 
complete remission rate 6 weeks after radio / immunotherapy detected by ct and fdg - pet was 100% . a total of 6 patients developed progression after radio / immunotherapy with a mean ttp of 27 month ( 1445 months ) : 1 patient ( cutaneous lymphoma , initially stage ia ) initially diagnosed in 1999 and initially treated with leuceran . 
 the fifth patient developed diffuse large cell b - cell lymphoma after the second kidney transplantation , initially located in the seminal vesicle ( ie ) and died due to systemic tumor progression 18 months after radio / immunotherapy . 
 discussion the therapeutic efficacy of rituximab in both indolent and aggressive b - cell nhl has been established in a large number of published clinical trials either as monotherapy or in combination with several chemotherapy regimens [ 4 , 11 , 18 , 25 ]  . 
 the rationale for using rituximab in combination with other agents , e.g. , fludarabine or chop chemotherapy , in patients with b - cell nhl is based on the clinical efficacy of both agents / regimen , no significant overlapping toxicities , and synergistic antitumor activity demonstrated in vitro [ 26 ]  . 
 [ 5 ] demonstrated the safety and efficacy of rituximab in combination with standard - dose systemic chemotherapy and showed an additive therapeutic benefit for the combination without significant toxicity . 
in vitro data with follicular lymphoma cell lines and cd - 20 positive burkitt ebv infected lymphoma cells showed strong synergism of rituximab and ionizing radiation to cause cell growth delay and apoptosis in both radiosensitive and radioresistant lymphoma cell lines . 
 based on these in vitro data , this study was designed to evaluate feasibility and toxicity of radiotherapy and concomitant application of rituximab in patients with nhl [ 12 ]  . 
 however , different cases of rituximab - associated adverse respiratory reactions , e.g. , interstitial pneumonitis , organizing pneumonia , and alveolar hemorrhage have been described [ 15 ]  . 
only in 1 patient with cervical irradiation was the rituximab application stopped after three cycles due to grade iii side effects of radiotherapy , i.e. , mucositis , dysphagia , and xerostomia . 
after a mean follow - up of 41.7 months no late toxicity was observed . six weeks after combined therapy , all patients ( 100% ) had a cr confirmed by fdg - pet scan and 71% are still without evidence of disease . 
of the 9 patients receiving no initial systemic treatment before radio / immunotherapy , 7 are still in complete remission without additional treatment . extended field radiotherapy or total nodal radiotherapy is considered as standard treatment in indolent nhl stage i , ii , and limited stage iii . 
optimal treatment volume of radiotherapy is still discussed controversy and there are only few studies comparing different radiation volumes in the literature [ 6 , 7 , 8 , 10 , 13 ]  . 
results show an improvement of pfs and os at 4 years of 88% and 92% , respectively , compared to 78% and 88% in the control group treated without rituximab ; however , there was still a pattern of continuous relapse that was explained by the authors as a result of different biological behavior compared to advanced stage lymphoma . beside data from the literature , many institutions generally tend to irradiate smaller volumes combined with systemic therapy . 
the authors determined that secondary tumors of the gastrointestinal tract were associated with a median radiation dose of 24 gy , a lower dose than used to treat nhl . also in this study , the majority of patients ( 90% ) were treated with ifrt . 
 one of these patients received radio ( ifrt ) / immunotherapy without initial systemic treatment to the left - sided cervical , supra - , and infraclavicular lymph nodes and recurrence was diagnosed in the left inguinal nodes . 
after 45 months , recurrent disease in the right inguinal nodes was diagnosed . one reason for concomitant application of rituximab to ifrt might be a reduction of out - of - field relapses , allowing the use of smaller irradiation fields and possibly improvement of pfs and os . another interesting aspect is rituximab maintenance after radio / immunotherapy . 
 [ 31 ] evaluated in a meta - analysis of 1 , 143 pts with follicular lymphoma a statistically significant better overall survival in patients treated with rituximab maintenance compared to observation or patients treated at relapse . 
 still , optimal duration of rituximab maintenance , its use after initial r - chop , and its benefit / efficacy compared to retreatment at progression remains unclear and has to be further investigated . conclusion radio / immunotherapy with rt and concomitant application of the immunomodulating monoclonal antibody rituximab is feasible and safe . 
 short communication iodine - 125 orbital brachytherapy with a prosthetic implant in situ clare stannard1 , gert maree2 , roger munro2 , karin lecuona3 , wolfgang sauerwein4 purpose : brachytherapy is one method of irradiating the orbit after enucleation of an eye with a malignant tumor that has a potential to recur . 
it consists of 6 trains of i - 125 seeds placed around the periphery of the orbit , a shorter central train , and a metal disc , loaded with seeds , placed beneath the eyelids . 
the presence of a prosthetic orbital implant requires omission of the central train and adjustment of the activity of the seeds in the anterior orbit around the prosthesis . patients and methods : this is a retrospective review of the technical modifications and outcome of 12 patients treated in this manner : 6 with retinoblastoma , 5 with malignant melanoma , and 1 with an intraocular rhabdomyosarcoma . 
there have been no orbital recurrences , no extrusion of the prosthesis , and cosmesis is good . conclusion : insertion of a prosthetic implant at the time of enucleation greatly enhances the subsequent cosmetic appearance . 
the patient is spared the expense and inconvenience of removing and replacing the prosthetic implant . key words : iodine - 125 orbital radiotherapy brachytherapy retinoblastoma uveal melanoma strahlenther onkol 2011 ; 187 : 3227 doi 10.1007 / s00066 - 011 - 2177 - y brachytherapie der orbita mit jod - 125 bei liegendem intraorbitalen implant nach enukleation hintergrund : bei hohem intraorbitalen rezidivrisiko nach enukleation eines tumortragenden auges kann die orbita mit einer 125i - brachytherapietechnik schonend bestrahlt werden . 
dabei werden 6 125i - seed - trains zirkulr in der orbita platziert , zusammen mit einem krzeren zentralen seed - train und einem mnzfrmigen applikator hinter den lidern , mit der strahlenden seite in richtung orbita . 
das kosmetische ergebnis war in allen fllen gut . schlussfolgerung : ein orbita - implant ergibt nach enukleation ein ausgezeichnetes kosmetisches resultat und sollte auer bei ausgedehntem tumorbefall anderen techniken vorgezogen werden . 
die hier neu vorgestellte technik erbringt auch ohne zentralen applikator eine hervorragende lokale kontrollrate und erspart dem patienten die aufwendige und nicht immer 1department of radiation oncology , groote schuur hospital and university of cape town , cape town , south africa , 2department of medical physics , groote schuur hospital and university of cape town , cape town , south africa , 3department of ophthalmology , groote schuur hospital and university of cape town , cape town , south africa , 4ncteam , strahlenklinik , universittsklinikum essen , essen , germany . received : may 10 , 2010 ; accepted : january 24 , 2011 published online : april 26 , 2011 strahlenther onkol 2011 no . 
 schlsselwrter : jod - 125 bestrahlung der orbita brachytherapie retinoblastom aderhautmelanom introduction the most common intraocular tumors are retinoblastoma in young children and malignant melanoma of the uveal tract in adults . 
ideally a prosthetic orbital implant should be inserted at the time for volume replacement and motility of the ocular prosthesis , thus , achieving the best cosmetic results [ 3 ]  . 
as the survival of children with retinoblastoma drops dramatically if the tumor has invaded the sclera or the resection line of the optic nerve [ 20 ] , these patients are managed with radiotherapy to the orbit and systemic chemotherapy . external beam radiotherapy , although excellent in preventing a recurrence , interferes with growth of the orbital bones in children with resulting poor cosmesis [ 9 , 10 ]  . 
in addition , the pituitary gland may receive some radiation which affects growth hormone production [ 13 ] , there may be future dental problems [ 8 ] , and in those with a germline mutation there is the added risk of second nonocular malignancies [ 1 ]  . to avoid these complications , a brachytherapy orbital implant was designed to irradiate the orbital contents , while shielding the bony orbit and eyelids [ 17 ]  . 
the implant consisted of 6 tubes , containing iodine - 125 seeds and partial shielding , implanted around the periphery of the orbit , a shorter central train of seeds , and a metal disc with i - 125 seeds on the posterior surface placed beneath the eyelids . in 2002 , we published our experience of treating retinoblastoma patients , who were at risk for developing an orbital recurrence after enucleation , with orbital brachytherapy . 
 we assumed initially that prosthetic orbital implants placed at the time of enucleation should be removed to allow insertion of the central line of sources required for the most homogeneous dose distribution . 
if orbital brachytherapy was anticipated after enucleation , the ophthalmologist delayed inserting the prosthetic implant until after the brachytherapy , accepting that the secondary orbital reconstruction was more difficult than when performed at the time of enucleation . in 2003 , a recommendation to remove the prosthetic implant of a 12 year old with an intraocular rhabdomyosarcoma that required orbital brachytherapy was refused . 
the brachytherapy implant was , therefore , planned without the central train of i - 125 seeds and the activity in the anterior part of the implant was increased accordingly . 
 patients and methods patients between january 2003 and august 2008 , 9 patients who had primary prosthetic orbital implants inserted at the time of enucleation were treated at the ocular oncology clinic at groote schuur hospital with orbital brachytherapy . 
tumor involved the resection margin of the optic nerve in 3 patients , was within 1 mm of it in 1 patient , was intrascleral in 3 patients , extrascleral in 4 patients , and was recurrent in the anteroinferior orbit in 1 patient ( figure 1 )  . the 6 retinoblastoma patients also received 46 cycles of chemotherapy : vincristine , etoposide and carboplatin or cyclophosphamide . 
the active length of each was determined from axial ct scans and was designed to extend from just below the skin of the eyelids to the apex of the orbit . 
this total activity was divided by the available seeds and a computer program used to distribute the seeds in the tubes and metal disc so as to give the most homogeneous dose distribution . 
as there was no central train of seeds , the activity of the anterior part of each peripheral train was increased . implant preparation the plastic tubes consisted of a heat shrinkable modified polyolefix material . 
a metal gutter , which consisted of half of a longitudinally sectioned 14 gauge angiocatheter intravenous placement needle , was also placed inside the tube for the chilstrahlenther onkol 2011 no . 
staging of rhabdomyosarcoma was based on the intergroup rhabdomyosarcoma study ( irs ) and staging of retinoblastoma was based on the proposed international retinoblastoma staging system ( irss ) [ 2 ] , while staging of malignant melanoma was based on the collaborative ocular melanoma study ( coms )  . 
die stadieneinteilung des rhabdomyosarkoms erfolgte nach der intergroup rhabdomyosarcoma study ( irs ) , die der retinoblastome nach dem vorgeschlagenen international retinoblastoma staging system ( irss ) [ 2 ]  . 
 it extended anteriorly beyond the most anterior seed by 11.5 c each gutter had a hole 1cm anterior to the most anterior seed for placement of a thin wire to secure the tube while the seed remained just below the surface of the ska 1 - cm filler was placed between the hole and the most anterior seed . 
the mean of the superior / inferior and medial / lateral diameters of the orbit were multiplied by to give the circumference , and divided by 6 to establish the spacing between each of the 6 peripheral tubes . 
an incision was made in the skin with a scalpel , through which a trochar and cannula were inserted and pushed through the tarsal plate towards the apex of the orbit . 
die applizierte dosis wurde auf die 0 , 5 - gy / std - isodose verordnet . tubes without gutters , used in the adults , were also sutured to the skin using a lead crimp , separated from the skin by a nylon button . implant calculation and dose distribution orthogonal x - rays of the orbit were taken . 
the theraplan plus computer program then generated isodose rate curves and these could be viewed in any plane so that the most representative could be selected ( figure 5 )  . 
the larger size of the adult orbit and the higher dose required for treating melanomas accounted for the higher activity and longer treatment time for these patients . the patient with the recurrent tumor in the anteroinferior orbit had an additional unshielded train of i - 125 seeds placed immediately inferior to the prosthetic implant , which increased the dose to this area . 
all patients were fitted with prosthetic eyes and cosmesis was good ( figure 6 )  . one patient experienced intermittent eyelid edema starting 10 months after the implant and clearing spontaneously . 
the dose was prescribed to the isodose rate line encompassing the orbital contents . the median dose to children with retinoblastoma was 35.5 gy over 73 hours ( range , 3440 gy over 54121 hours )  . 
the dose to the rhabdomyosarcoma was 46 gy over 94 hours and the median dose to the melanomas was 56 gy over 141 hours ( range , 5174 gy over 83169 hours )  . 
primary insertion of an orbital implant replaces the volume of the enucleated globe and improves the motility of the fitted ocular prosthesis , resulting in markedly improved cosmetic results following enucleation [ 3 ]  . 
the recurrence of orbital tumor is a distinct possibility in advanced disease , but it is not a contraindication to the insertion of an orbital implant because it can be detected both clinically and by regular mri scans [ 6 , 18 ]  . as we now know which tumors are likely to recur in the orbit on the basis of the histological assessment of the enucleated eye , those at risk can be treated with radiotherapy and / or chemotherapy adjunctively to minimize the risk [ 7 , 11 , 12 , 14 , 19 , 20 ]  . 
 [ 17 ] devised a means of irradiating an enucleated orbit with an i - 125 brachytherapy implant designed in such a way as to reduce the dose of irradiation to the eyelids and growing orbit in children . 
it was designed 25 years ago when prosthetic implants were not the norm and has yielded excellent results in terms of local control , cosmesis , and normal development of the bony orbit [ 21 ]  . the orbital brachytherapy implant has now been modified so that it can be used with a prosthetic implant in situ . 
there should be no future dental problems , late facial atrophy , reduced growth hormone production , or increased risk of second nonocular malignancies in those with retinoblastoma germline mutations . 
it is also suitable for treating adult orbits , without the shielding , as the short treatment time is an advantage over external beam irradiation . acknowledgments we thank kathrin sauerwein for drawing figures 2 and 3 . original article adjuvant low single dose cisplatin - based concurrent radiochemotherapy of oral cavity and oropharynx carcinoma impact of extracapsular nodal spread on distant metastases thomas kuhnt1 , ulf klockenbrink1 , stephan knipping2 , juergen lautermann3 , karen kriese4 , andreas wienke5 , guido hildebrandt1 , steffen hauptmann4 background : the aim of this study was to analyze the prognostic importance of extracapsular nodal spread ( ecs ) in patients with locally advanced squamous cell carcinoma ( scc ) of the oral cavity or oropharynx , and the impact of adjuvant low single dose cisplatin - based radiochemotherapy on distant metastases - free survival ( dmfs )  . patients and methods : the study population was selected from 195 patients with high - risk oral cavity or oropharyngeal cancer , who had either adjuvant radiotherapy ( rt ) or radiochemotherapy ( rct ) between january 1 , 1997 and december 31 , 2006 , at the university clinic of radiation oncology of the martin - luther - university hallewittenberg . 
the patients were matched ( one to one ) according to tumor site , sex , t stage , n stage , ecs , resection margin status , and karnofsky performance status . 
survival rates were calculated using the kaplanmeier method . results : there was a strong correlation between the degree of nodal involvement and ecs ( pn1 : 33% ; pn2b : 45% ; pn2c : 71% )  . 
adjuvant low single dose cisplatin - based concurrent chemotherapy seems to have no influence on occult microscopic systemic disease . key words : locally advanced scchn radiotherapy radiochemotherapy extracapsular nodal spread distant metastases outcome strahlenther onkol 2011 ; 187 : 2929 doi 10.1007 / s00066 - 011 - 2186 - x adjuvante , niedrig - einzeldosierte , cisplatin - haltige simultane radiochemotherapie von mundhhlenund oropharynxtumoren : der extrakapsulre lymphknotenbefall beeinflusst die fernmetastasierung hintergrund : ziel der untersuchung war die analyse der prognostischen bedeutung der extrakapsulren infiltration bei lymphknotenmetastasen ( extracapsular nodal spread ecs ) von patienten mit lokal fortgeschrittenen plattenepithelkarzinomen von mundhhle oder oropharynx und des einflusses der adjuvanten , niedrig - einzeldosierten cisplatin - haltigen radiochemotherapie auf das fernmetastasenfreie berleben ( dmfs )  . patienten und methodik : insgesamt wurden 195 patienten ausgewertet , die an der universittsklinik fr strahlentherapie der martin - luther - universitt halle - wittenberg zwischen dem 1 . 
dezember 2006 wegen eines hochrisiko - kopf - hals - karzinoms der mundhhle oder des oropharynx postoperativ eine alleinige radiotherapie ( rt ) oder eine simultane radiochemotherapie ( rct ) erhielten . 
fr die analyse wurden dann 42 aufeinander abgestimmte patienten1department of radiation oncology , university hospital of rostock , rostock , germany , department of otorhinolaryngology , head and neck surgery , stdtisches klinikum dessau , germany , 3department of otorhinolaryngology , head and neck surgery , hospital martha - maria , halle - doelau , germany , 4institute of pathology , martin - luther - university halle - wittenberg , halle ( saale ) , germany , 5institute of medical epidemiology , biostatistics and informatics , martin - luther - university halle - wittenberg , halle ( saale ) , germany . received : june 16 , 2010 ; accepted : february 4 , 2011 published online : april 26 , 2011 strahlenther onkol 2011 no . 
die patienten der beiden gruppen wurden eins zu eins gem primrlokalisation , geschlecht , t - stadium , n - stadium , ecs , resektionsrand und karnofsky - performance - status homogen verteilt . 
die berlebenskurven wurden mit der kaplan - meier - methode berechnet . ergebnisse : die hufigkeit der extrakapsulren weichgewebeinfiltration korrelierte mit dem ausma der lymphknotenmetastasierung ( pn1 : 33% ; pn2b : 45% ; pn2c : 71% )  . 
die adjuvante , niedrig dosierte cisplatinbasierte simultane chemotherapie hatte keinen einfluss auf die okkulte mikroskopische systemische metastasierung . schlsselwrter : lokal fortgeschrittene plattenepithelkarzinome kopf - hals - bereich radiotherapie radiochemotherapie extrakapsulrer lymphknotenbefall fernmetastasierung berleben introduction approximately 60% of patients with squamous cell carcinoma ( scc ) of the head and neck region ( h&n ) present with locally advanced disease ( uicc stage iii or iva , b ) [ 10 ]  . 
in a subgroup of these patients , the lymph node metastases are not confined to the lymph node parenchyma but invade the perinodal soft tissue , a behavior which is called extracapsular nodal spread ( ecs ) [ 7 ]  . 
 retrospective studies performed in the 1980s indicated that postoperative radiotherapy ( rt ) decreases the risk of locoregional recurrence in patients with multiple involved lymph nodes , ecs , and positive resection margins [ 15 , 18 ]  . 
during the last decade , many studies came to the conclusion that combined radiochemotherapy ( rct ) was more beneficial in these patients than rt alone [ 3 , 5 , 9 ]  . however , patients with two or more positive lymph nodes and with additional risk factors do not seem to benefit from rct regarding overall survival ( os ) , whereas patients with ecs do [ 2 ]  . 
therefore , ecs was suggested to be a surrogate marker for occult distant metastases ( dm ) and the key factor predicting worse overall survival . theoretically , with improved local disease control patients should survive longer but would be at higher risk to develop distant metastases . 
in fact , as a result of these studies , one could conclude that rct with cisplatin might have an impact on lc but no impact on distant metastases in patients with ecs . in this retrospective study , we analyzed whether ecs might be an independent factor for distant metastases - free survival ( dmfs ) and overall survival ( os ) in patients , who were treated with low single dose cisplatin - based radiochemotherapy . patients and methods patient population the study population was selected from 195 patients with high - risk oral cavity or oropharyngeal cancer , who had either adjuvant radiotherapy ( rt ) or radiochemotherapy ( rct ) between january 1 , 1997 and december 31 , 2006 , at the university clinic of radiation oncology of the martin - luther - university halle - wittenberg . 
ct or mri investigations were performed 6 weeks after the adjuvant treatment course , and then once a year over a time period of 5 years . radiotherapy all patients were immobilized in thermoplastic head , neck , and shoulder masks in order to conduct treatment - planning ct scans ( slice thickness 5 mm ) to define the target volumes and the organs at risk . 
a twodimensional ( 2d ) technique using two lateral opposing facial fields of 6 mv photons and 69 mv electron fields for the posterior cervical lymph nodes or a three - dimensional ( 3d ) conformal technique using a combination of 78 static coplanar fields and one dynamic arc portal were performed [ 17 ]  . 
three clinical target volumes ( ctv ) were defined : ctv 70 ( total dose 70 gy ) for high - risk regions ( i.e. , r1 without chemotherapy ) , ctv 64 ( total dose 64 gy ) for high - risk regions ( i.e. , r1 , ecs , or 2 involved nodes with concurrent chemotherapy ) , and ctv 50 ( total dose 50 gy ) for low - risk regions ( i.e. , pn0 or nodes down to the clavicles in both groups )  . 
planning target volume ( ptv ) was defined as the ctv plus a 5to 10 - mm margin to compensate variables of treatment setup and motion of internal organs ( icru report 50 )  . 
 chemotherapy chemotherapy consisted of 20 mg of cisplatin per square meter of body - surface area ( mg / m ) or 25 mg / m on days 15 and days 2933 as well as 5 - fluorouracil ( 5 - fu ) 600 mg / m on days 15 and days 2933 as a 120 - hour continuous infusion . 
since 2004 , treatment protocol was changed to monotherapy with cisplatin , as emerged from the eortc and rtog studies that cisplatin was the most important cytotoxic drug . statistical analysis the case - matching involved 84 patients with high - risk uicc stage iiiiva , b squamous cell carcinoma . 
the matching compared patients by primary tumor site , t - stage , n - stage , grading , and resection margin status on the basis of histopathological findings and surgical protocols . 
endpoints were locoregional control ( lc ) , diseasefree survival ( dfs ) , distant metastasis - free survival ( dmfs ) , and overall survival ( os ) analyzed by means of the kaplanmeier method [ 16 ]  . 
the median treatment time starting from surgery until the end of radiotherapy was 84 days ( sd : 13 days ) in the rt group , and 81 days ( sd : 13 days ) in the rct group . 
a combination of cisplatin + 5 - fu was applied in 23 / 42 patients ( 55% ) , whereas cisplatin alone was applied in 19 / 42 strahlenther onkol 2011 no . 
moreover , there was a significant correlation between ecs and the development of distant metastases ( p = 0.05 ; table 2 )  . overall survival , locoregional control , disease - free survival , and distant metastases - free survival overall survival ( os ) the 5 - year os rate of the entire patient cohort was 57% ( 48 / 84 patients )  . 
at the end of the evaluation period , 36 of 84 patients were still alive without signs of recurrence , metastases or second primary tumor , while 6 patients ( 6 / 84 ; 7% ) were alive with recurrence or metastases . 
locoregional recurrence or distant metastases was the cause of death in 30 / 36 ( 83% ) patients , 2 ( 6% ) patients died due to second primary malignancy , and 3 ( 8% ) patients died of other diseases . 
cisplatin which is given for that purpose is a potent radiosensitizer and the most commonly used drug for radiochemotherapy ( rct ) in the simultaneous setting in squamous cell carcinoma of the h&n , thus , even for local control [ 19 , 20 , 22 ]  . 
however , ens is a morphological prognosconcurrent cisplatin - based radiochemotherapy and locoregional control tumors with microscopically involved resection margins ( r1 ) , with the involvement of at least two regional lymph nodes , or with infiltration of the lymph node capsule are at a greater risk for locoregional recurrence [ 6 , 13 ]  . 
reported the first prospective trial in which patients were randomized to postoperative rt alone or combined rct with weekly higher doses of cisplatin ( 50mg / m ) [ 1 ]  . 
both the eortc and rtog trial demonstrated a significant benefit from higher single shot doses of cisplatin ( 100 mg / m2 / d on days 1 , 22 , and 43 ) on lc rates . 
 the rct reduced the risk of locoregional relapse by 45% in the eortc trial and 39% in the rtog trial [ 3 , 5 ]  . in our study population , no strong impact of ecs and lc was registered . 
more recently , the incidence of oropharyngeal cancer in younger populations has been increasing and this is associated with exposure to the human papilloma virus ( hpv ) [ 11 ]  . 
only in one of the three major randomized trials was the addition of concurrent chemotherapy associated with a significant improvement of os by 13% for the rct group [ 3 ]  . 
possibly , the lack of survival benefit in the rtog trial as compared to the eortc was a result of the higher nodal involvement rate in the rtog study population . 
comparative analysis of the nodal status distribution indicates a striking difference in n23 with 94% in the rtog trial as compared to only 57% in the eortc trial [ 2 ]  . in the present study , the lack of significant differences in os and dfs in patients with rct as compared to rt alone are very likely a result of the higher rate of distant metastases . 
 [ 21 ] have also shown that a gross tumor volume > 70ml in combination with locoregionally advanced stages ( t3 n13 ) are risk predictors for distant metastases ( dm ) in h&n cancer patients [ 18 ]  . 
there is no doubt that the risk of capsular rupture of neck nodes is related to the higher n2b , c / 3 categories of the tnm classification [ 7 ]  . 
kaplan - meier - schtzung des fernmetastasenfreien berlebens der radiotherapie ( rt ) oder radiochemotherapie - gruppe ( rct ) fr patienten mit ( a ) oder ohne ( b ) extrakapsulren lymphknotenbefall ( ecs )  . 
 risk of distant metastases ( dm ) in adjuvant treatment of scc h&n it has been concluded that patients with improved lc from rct regimes would survive longer and would , therefore , be strahlenther onkol 2011 no . 
however , between the cisplatin - based postoperative rct trials , the largest differences existed in single shot and not in the cumulative cisplatin doses [ 3 , 5 , 9 ]  . 
whereas the rtog and eortc trials applied high - single shot doses of cisplatin with 100mg / m2 on days 1 , 22 , and 43 , the german aro 963 study administered cisplatin in a fractionated manner with lower single doses ( 20mg / m2 ) applied over 10 days ( days 15 and 2933 )  . 
a part of the cohort of the present analysis was treated with cisplatin + 5 - fu according to the aro 96 - 3 study , reaching cumulative cisplatin doses of 360 mg . 
however , in the rtog and eortc studies , the dm rates in the rct group were 20% and 21% , whereas in the aro - 96 - 3 study the dm rate was 31% . 
 the retrospective nature of this analysis , the small differences in the matched criteria for the two groups ( i.e. , ecs ) allow us only to generate a hypothesis that an adjuvant low , single dose of cisplatin - based radiochemotherapy may not improve the distant control of scc of the h&n region . conclusion our data suggest that lower single shot doses of cisplatin - based chemotherapy concomitant to high - dose adjuvant rt have a positive impact on lc in patients without ecs . 
thus , patients with nodal stage ( p ) n2bc with ecs should either receive adjuvant higher single doses cisplatin or prior definitive therapy newer chemotherapy protocols in combination with taxanes with or without new biological agents . 
three - dimensional image - guided radiotherapy ( igrt ) with cone - beam computer tomography ( cbct ) , which results in more precise target localization , is quickly replacing two - dimensional ( 2d ) igrt . 
an overview on the clinical applications of kilovoltage gantry - mounted cbct systems with emphasis on the most frequently targeted body sites ( prostate , lung , head and neck ) is provided based on a review of the relevant literature . 
alternative imaging methods and their advantages / disadvantages are discussed . results : igrt with soft tissue detection improves set - up accuracy and is currently replacing 2d verification and frame - based stereotactic treatments ; safety margins are significantly reduced by this igrt technology . 
 conclusions : cbct allows for daily pretreatment position verification and online correction of set - up errors which improves the precision of patient repositioning with the possibility of shrinking safety margins , sparing organs at risk , and escalating radiation doses . 
head and neck strahlenther onkol 2011 ; 187 : 28491 doi 10.1007 / s00066 - 011 - 2236 - 4 kv - cone - beam - ct - basierte bildgefhrte strahlentherapie ein klinischer berblick hintergrund und methodik : die verwendung von eskalierten bestrahlungsdosen bei gleichzeitiger schonung der risikoorgane setzt multimodale bildgebung zur zielvolumendefinition , hochkonformale bestrahlungsplanung mittels intensittsmodulierter radiotherapie und enge sicherheitssume voraus . 
bildgefhrte strahlentherapie ( igrt ) dient der przisen lokalisation des zielvolumens , und konventionelle 2d techniken wie feldkontrollaufnahmen werden aktuell insbesondere durch dreidimensionale cone - beam - ( cbct - ) technik ersetzt . 
schwerpunkte sind die praktische anwendung und klinischen resultate bei prostatakarzinom , bronchialkarzinom und kopf - hals - tumoren . ergebnisse : igrt mittels cbct ist hocheffektiv zur verifikation der patientenpositionierung und insbesondere zur verifikation der tumorposition . 
mittels konformaler imrt - bestrahlungstechniken und prziser igrt konnten hypofraktionierte , eskalierte bestrahlungsdosen sicher appliziert werden , was in verbesserter lokaler tumorkontrolle ohne erhhte toxizitt resultierte . schlussfolgerungen : cbct ermglicht die verifikation der tumorposition zur online - korrektur von positionsfehlern vor der behandlung , was die anwendung von kleinen sicherheitssumen , normalgewebsschonung und dosiseskalation ermglicht . 
hno 1department of radiation oncology , university medical center mannheim , university of heidelberg , mannheim , germany , 2department of radiation oncology , university hospital wrzburg , wrzburg , germany . received : november 29 , 2010 ; accepted : february 21 , 2011 published online : april 26 , 2011 strahlenther onkol 2011 no . 
cbct - based igrt introduction radiotherapy has undergone rapid changes in the last decade including advanced image - based treatment planning and intensity - modulated delivery with modern dose calculation and verification methods . 
 soft tissue - based image - guided radiotherapy ( igrt ) is currently replacing two - dimensional ( 2d ) verification and frame - based intra [ 8 ] and extracranial stereotaxy [ 34 ]  . 
online position correction can be performed with ct - on - rails or conebeam ct ( cbct ) , ultrasound [ 26 ] or electromagnetic signals [ 46 ]  . 
cbcts acquire multiple projection radiographs ( for head and neck imaging ~350 , for thoracic / pelvic imaging up to 600 ) before a radiotherapy fraction within a 180360 gantry rotation ( acquisition time 40 s to 2 min )  . 
a volumetric image with high spatial resolution and sufficient soft tissue contrast is reconstructed and compared to the reference planning ct dataset for calculation of the target position relative to the planned reference position . 
more complex changes of the target and normal tissue ( weight loss , tumor regression ) are monitored allowing for plan adaptation . this review provides an overview about clinical applications of kv ( kilovoltage ) gantry - mounted cbct systems , with emphasis on the most frequently targeted tumor sites . 
alternative imaging methods and their advantages / disadvantages are discussed . image quality cbct image quality is inferior to diagnostic fan - beam cts due to increased scatter ( also contributing to streaking / cupping artifacts [ 63 ] ) and reduced contrast of large projection field sizes [ 29 ]  . 
bowtie filters , optimized image acquisition presets and reconstruction algorithms [ 5 ] , and appropriate quality assurance [ 3 ] ensure optimal image quality . extra dose due to imaging the cbct dose is 20 mgy / scan for pelvic and < 10 mgy / scan for head and neck imaging ( in vivo measurements [ 40 , 78 ] )  . 
 major clinical applications prostate cancer rationale for igrt in prostate cancer , decreased biochemical control rates were reported for patients with a distended rectum in the planning ct [ 16 ] , a situation not representative for the treatment course resulting in a systematic posterior displacement of the prostate . 
 without igrt , a decreased dose to the target was documented . randomized trials have confirmed increased biochemical control if doses were increased from 6470gy to 7479.2gy [ 2 , 18 , 44 , 84 ]  . 
consequences of large tvs and suboptimally conformal dose distributions were increased rates of especially late rectal toxicity [ 25 ]  . relevance of prostate position variability prostate motion is mainly caused by variable rectum and bladder filling , resulting in poor correlation between prostate position and bony anatomy . 
systematic errors are largest if the rectum is distended at treatment planning ; however , interfraction prostate position variability is still substantial with an initially empty rectum [ 45 ]  . 
translational prostate position variability is largest in anteriorposterior and superiorinferior directions and ap prostate motion is mainly explained by the rotation of the prostate around the lr axis at the apex [ 28 , 76 ]  . 
ctv - to - ptv safety margins of at least 10 mm are commonly accepted [ 17 , 19 ]  . practice of cbct - based igrt phantom studies have shown high accuracy of cbct with residual errors < 1mm [ 49 ] , but in clinical practice , this is more difficult . 
results of 2dand 3d - igrt are not different when implanted markers are used but volumetric igrt offers the advantage to also evaluate oar geometry ( e.g. , proper bladder filling ) [ 74 ]  . correction protocols once weekly imaging was shown to be of limited efficiency [ 75 ]  . 
im stadium i : fehlpositionierung der knchernen anatomie und des lungentumors nach rahmenbasierter stereotaktischer patientenpositionierung ( links ) ; bildregistrierung basierend auf der wirbelsule mit fehlpositionierung des lungentumors , verursacht durch einen base - line - shift ( mitte ) ; bildgefhrte strahlentherapie mit bildregistrierung basierend auf dem lungentumor mit fehlpositionierung der wirbelsule ( rechts )  . atic error by repeated imaging at the beginning of the treatment course and were shown to be effective in reducing safety margins [ 15 ] , while minimizing imaging frequency . 
the additional gain by daily imaging and online correction may be smaller compared to the step from no igrt to offline igrt [ 53 ]  . residual uncertainties in cbct - based igrt prostate rotation compensation adapting gantry / collimator angle or mlc configuration [ 21 ] has been suggested . 
robotic couches can perform rotational corrections , but the range of rotational motion is too small for prostate , where rotations up to 15 are observed , inducing substantial secondary patient displacements [ 33 ]  . 
investigational strategies of daily replanning were described [ 72 ]  . clinical results there is no high - evidence level data that igrt improves outcome for prostate cancer , but promising retrospective studies reported decreased toxicity when igrt was added to radiotherapy [ 9 , 14 ] and multiple studies reported low toxicity rates when igrt / imrt were practiced in dose escalation [ 35 ]  . 
the reason might be that standard margins were reduced by 50% , then probably being too small for compensation of extracapsular extension and intrafractional motion . lung cancer rationale for igrt although radiotherapy is accepted as the treatment of choice for medically inoperable early stage non - small cell lung cancer ( nsclc ) , rates of local control are disappointing with conventional techniques / fractionation ( local failure in 670% stage i / ii patients [ 62 ] which is substantially higher than with lobectomy [ 83 ] )  . 
dose escalation beyond 70gy has increased local control in both early and advanced stage nsclc [ 38 , 81 ]  . relevance of geometrical uncertainties geometrical uncertainties occur on different time scales . 
days : interfractional changes are larger compared to intrafractional errors ; analogously , it is distinguished between set - up error and baseline shifts of the tumor independently from the bony chest . 
changes of atelectasis and pleural effusion have been reported in almost 50% of patients [ 64 ] , altering shape and position of the tv . practice of cbct - based igrt image - guidance is especially challenging in lung cancer because all uncertainties need to be integrated into a consistent work flow . 
volume imaging is preferable to all 2d methods because it allows ( 1 ) separate analysis of tumor , nodal , and oar positions and ( 2 ) evaluation of shape / volume changes . 
breath - hold approaches in combination with fast - spiral planning ct [ 52 ] reduce the effect of breathing motion , making margin reduction and dose escalation possible due to less total irradiated lung tissue [ 57 ]  . 
cbct - based igrt this can be done by slow scanning [ 47 ] , respiration - correlated imaging [ 22 , 67 ] , or imaging in breath - hold technique . 
 correction protocols daily pretreatment image guidance with online correction of set - up errors and baseline shifts is required in sbrt to avoid target underdosage and has largely replaced frame - based setup [ 82 ]  . 
safety margins of 5 mm are required in a protocol with online igrt [ 66 ]  . residual uncertainties correction of large baseline tumor shifts bear the potential risk of increasing oar doses if the target moved closer to the oar [ 27 ]  . 
differential position changes of primary tumor and nodal disease cannot be corrected by a single couch shisuch nonrigid changes require replanning if certain thresholds are exceeded but no thresholds have been defined yet . 
 [ 51 ] reported decreased rates of severe pneumonitis and improved survival in patients treated with advanced technologies . intracranial and h&n targets rationale for igrt frame - based stereotactic set - up for treatment of intracranial lesions has been considered to be the most precise technique in radiotherapy and allowed establishing radiosurgery with its excellent clinical results in various intracranical tumors . 
noninvasive mask - / bite - block - based approaches allow fractionated treatment regimens but set - up accuracy is decreased compared to invasive fixation . relevance of geometrical uncertainties invasive frame - based stereotaxy is precise but a systematic difference between stereotactic set - up and igrt was observed in anteriorposterior direction , explained by a flex in the ring fixation system [ 48 ]  . 
good agreement between stereotactic set - up and igrt was reported but frame slippage of almost 5 mm was observed in 1 of 102 patients , which would have remained undetected without igrt [ 60 ]  . 
daily igrt is required and verification imaging after set - up correction is recommended especially in radiosurgery . in head and neck cancer , large set - up uncertainties were measured in anatomical subregions [ 50 , 58 , 77 ]  . 
intrafractional patient motion in mask or bite - block systems is larger compared to invasive radiosurgery , but still within acceptable limits of 12 mm [ 60 ]  . patient weight loss and shrinkage of head and neck tumors and salivary glands is frequently observed during radio ( chemo ) therapy [ 12 , 4 ]  . clinical results a 1 - year local control rate of 80% was reported after frameless image - guided radiosurgery of brain metastases , comparable to results using the frame - based approach [ 10 ]  . 
daily cbct for head and neck cancer enabled ctv - to - ptv margin reduction by ~50% [ 19 ] , which could facilitate future studies on dose escalation and / or toxicity reduction . 
in many clinical situations , matching of planning ct and cbct can be performed automatically based on bony anatomy , while manual matching by physicians / radiotherapists is still preferred for several situations , encouraging the assessment of both target position and oar geometry . 
it will likely be the basis for all precision radiotherapy such as imrt / vmat and ablative hypofractionated radiotherapy . acknowledgments parts of the authors original studies were supported by grants from elekta inc . 
 original article retrospective , monocentric analysis of late effects after total body irradiation ( tbi ) in adults tobias blling1 , 2 , david christoph kreuziger1 , iris ernst1 , hassan elsayed1 , normann willich1 purpose : total body irradiation ( tbi ) is a standard treatment modality within the multidisciplinary approach for allogeneous stem cell or bone marrow transplantation . 
this analysis aimed to retrospectively characterize late effects after tbi in adults treated in a single center . patients and methods : patients 18years treated with fractionated tbi ( 412gy ) between 1996 and 2008 were included in this study . 
analyses were performed by calculation of the cumulative incidences using the kaplanmeier method and the log rank test . results : a total of 308patients 18 years were treated including a tbi of whom 78patients were excluded from further analysis due to death within less than 1year after tbi . 
late toxicity follow - up was available in 120patients ( mean age 46.1years ; range , 1870years ) after a mean follow - up of 23months ( range , 1296months )  . 
the cumulative incidences ( ci ) at 3years were 28%for pulmonary event , 8%for pulmonary toxicity , 25%for kidney toxicity , 8%for cataract , 17%for bone toxicity , and 10%for secondary malignancy . 
regular follow - up examinations are advised for the early registration and treatment of adverse effects . key words : total body irradiation late effects adults bone marrow transplantation stem cell transplantation strahlenther onkol 2011 ; 187 : 3115 doi 10.1007 / s00066 - 011 - 2190 - 1 retrospektive , monozentrische analyse von sptfolgen nach ganzkrperbestrahlung ( tbi ) bei erwachsenen ziel : die ganzkrperbestrahlung ist eine standard - therapiemodalitt in dem multidisziplinren ansatz fr allogene stammzell oder knochenmarktransplantationen . 
 ziel dieser analyse war es , retrospektiv sptfolgen nach ganzkrperbestrahlung bei erwachsenen zu erheben . patienten und methode : patienten 18 jahre , die mittels fraktionierter tbi ( 412 gy ) zwischen 1996 und 2008 bestrahlt worden waren , wurden in diese studie eingeschlossen . 
eine sptfolgenerhebung war bei 120 patienten ( mittleres alter 46 , 1 jahre , 1870 jahre ) nach einer mittleren nachbeobachtung von 23 monaten ( 1296 monate ) mglich ( berleben : abbildung 1 )  . 
die kumulative inzidenz nach 3 jahren betrug 28% fr pulmonale ereignisse generell , 8% fr pulmonale toxizitt , 25% fr nierentoxizitt , 8% fr katarakte , 17% fr knochenschden und 10% fr sekundre malignome ( abbildung 2 )  . 
die kumulative inzidenz an knochenschden war bei weiblichen patienten signifikant hher als bei mnnlichen ( abbidlung 3 ; p = 0 , 019 )  . zusammenfassung : sptfolgen nach ganzkrperbestrahlung im kontext von allogener stammzelloder knochenmarktransplantationen treten regelmig auf . 
behandlung mglicher funktionsstrungen wird empfohlen . schlsselwrter : ganzkrperbestrahlung sptfolgen erwachsene knochenmarktransplantation stammzelltransplantation 1department of radiotherapy , university hospital of mnster , mnster , germany , 2department of radiotherapy , paracelsus clinic osnabrck , germany . received : june 25 , 2010 ; accepted : january 24 , 2011 published online : april 26 , 2011 strahlenther onkol 2011 no . 
the hazard ratio was calculated in case of significant differences in the log - rank test . results of 308adult patients treated with tbi , 78patients were known to have died within less than 1year after tbi and were , therefore , not considered for the analysis of late effects . 
regarding the remaining 230 patients , late effect follow - up information was obtained for 120 ( 68male , 52female ) patients after a mean follow - up time of 23 months ( range , 1296 months ) and a mean age of 46.1years ( range , 1870 years )  . 
stem cell transplantation was more frequent ( n = 98 ) than bone marrow transplantation ( n = 22 )  . figure 1 shows the overall survival curve of the complete patient group with late toxicity follow - up . 
analysis of late effects after tbi in adults introduction total body irradiation ( tbi ) is a standard treatment modality in the multidisciplinary framework of stem cell or bone marrow transplantation [ 6 , 14 ]  . 
beside its efficacy in the different treatment schedules , patients surviving tbi are known to be at risk to develop a broad variety of late side effects [ 1 , 3 , 5 , 10 , 12 , 14 ]  . 
 although patient survival is still the major concern in patients undergoing tbi [ 4 ] , the knowledge of late effects of this treatment approach is important for patient information and comparison of different treatment strategies . 
the aim of this analysis was to retrospectively characterize the pattern of late effects in patients surviving stem cell or bone marrow transplantation treated in a single center . patients and methods between june 1996 and july 2008 , 350 patients underwent treatment , which included tbi . 
tbi was performed with 2daily fractions of 2gy ( time interval at least 6hours ) on either 1 ( 4gy ) , 2 ( 8gy ) , 2.5 ( 10gy ) , or 3 ( 12gy ) consecutive days using a linear accelerator ( 6 or 15mv photons )  . 
in case of a tbi dose exceeding 8gy , shielding blocks in the lateral fields were placed at the side of the thorax to reduce the lung dose to 8gy . 
the shielded mediastinum , lateral ribs , and upper arms were concomitantly irradiated with an additional cumulative dose of 4 gy using an anterior / posteriorposterior / anterior field setting to obtain a cumulative dose of 12gy within these structures . 
therefore , chemotherapy regimens were categorized as fludarabin - based or cyclophosphamide - based in order to allow statistical analyses with sufficient patient numbers . patient characteristics including age , sex , diagnosis , prior treatments , and pre - existing functional deficits as well as treatment parameters , e.g. , tbi date , technique and dose , were collected retrospectively from patient charts . 
they were asked for status ( alive / dead ) , relapse , and toxicities regarding lungs , liver , kidneys , eyes ( cataract ) , bones , thyroid gland , other ( free text ) as well as secondary malignancies . 
the observed secondary malignancies were predominantly carcinomas ( n = 4 ; breast , colon , prostate , and bladder carcinoma ) as well as a multiple myeloma and a melanoma in 1patient each . to further characterize the influence of sex , age , tbi table 1 . 
anzahl der ereignisse , kumulative inzidenz nach 3 jahren und mittlere zeit zum ereignis fr die verschiedenen toxizitten bei patienten , die mittels ganzkrperbestrahlung behandelt wurden . toxicity number of events ( patients under evaluation ) 19 ( 93 ) pulmonary event 8 ( 93 ) pulmonary toxicity 12 ( 94 ) kidney toxicity 8 ( 93 ) cataract bone toxicity 15 ( 92 ) secondary malignancy 6 ( 104 ) cumulative incidence 3 years ( % ) mean time to event ( months ) dose , photon energy , and chemotherapy schedule , additional univariate analyses were performed . 
the comparison of the incidences of bone toxicity with regard to sex ( figure 3 ) showed significant differences ( p = 0.019 ) with higher rates of bone toxicity in female patients . 
 patients treated with 15 mv photons showed inferior survival ( p < 0.000 ) and higher rates of toxicity for the kidneys ( p < 0.000 ) , cataracts ( p = 0.002 ) , and bone toxicity ( p < 0.000 ) in univariate analyses . 
further univariate as well as multivariate analyses did not show any significant difference , possibly due to low patient numbers in the different subgroups . discussion recently , late effects after tumor therapy including radiotherapy , chemotherapy , and / or surgery have become a major focus of research due to increasing cure rates [ 3 , 17 ]  . 
this may be due to the limited number of patients in the different subgroups . cumulative incidences of pulmonary events ( defined as pulmonary toxicity and / or recurrent infection ) and pulmonary toxicity of 28% and 8% at 3years were observed in the present study . 
bone dysfunctions ( reported as bone necrosis , arthrosis , and a variety of further symptoms ) may be due to hormonal deficits following the conditioning therapy or prior treatments . 
whether these tumors really can be attributed to the tbi ( or conditioning therapy in all ) or whether they occurred independently of the first malignancy remains open . in summary , we have observed cumulative toxicity incidences after tbi that did not exceed 30% for any toxicity which is in concordance to published data . 
with respect to the known value of tbi [ 4 ] and the limited prognosis of this patient cohort in case of omission of stem cell / bone marrow transplantation , these rates seem to be acceptable in view of riskbenefit considerations . late effects after total body irradiation can frequently be observed . 
regular follow - up examinations are advised to register adverse effects at an early stage and allow early intervention . conclusion original article prognostic value of radiobiological hypoxia during fractionated irradiation for local tumor control daniel zips1 , simon bke1 , theresa kroeber1 , andreas meinzer1 , kerstin brchner1 , howard d . 
thames3 , michael baumann1 , 2 , ala yaromina1 background and purpose : previous experiments showed that the fraction of radiobiologically hypoxic tumor cells ( rhf ) in untreated tumors did not accurately predict local tumor control after fractionated irradiation . 
thus , the prognostic value of rhf determined during fractionated irradiation was investigated . materials and methods : six human squamous cell carcinoma lines were transplanted into nude mice and then irradiated with 15 fractions over 3 weeks . 
local tumor control rates were used to calculate the rhf and the tcd50 , i.e. , the radiation dose necessary to control 50% of the tumors , after single dose irradiation . 
single dose top - up tcd50 under ambient and clamp conditions after 15 fractions significantly correlated with tcd50 after 30 fractions in 6 weeks . conclusion : rhf after 15 fractions is not a prognostic parameter for the outcome after fractionated irradiation . 
in contrast , the radiobiological parameters number of tumor stem cells , intrinsic radiosensitivity , and number of radiobiologically hypoxic tumor cells appear promising to predict outcome after fractionated irradiation . keywords : human tumor xenograft head and neck cancer radiobiological hypoxia fractionated irradiation local tumor control strahlentheronkol2011 ; 187 : 30610 doi 10.1007 / s00066 - 011 - 2210 - 1 prognostischerwertderradiobiologischenhypoxiewhrendfraktionierterbestrahlungfrdielokale tumorkontrolle hintergrund und fragestellung : bisherige experimente haben gezeigt , dass die radiobiologische fraktion ( rhf ) in unbestrahlten tumoren die strahlenempfindlichkeit nach fraktionierter bestrahlung nicht exakt vorhersagt . 
hier wurde die rhf in fraktioniert bestrahlten tumoren bestimmt , um den prognostischen wert fr die fraktionierte bestrahlung zu ermitteln . material und methoden : sechs menschliche plattenepithelkarzinomlinien wurden in nacktmuse transplantiert und zunchst mit 15 fraktionen in 3 wochen bestrahlt . 
aus den tumorkontrolldaten wurden dietcd50 ( strahlendosis zur kontrolle von 50% der tumoren ) und die rhf berechnet und mit der tcd50 nach 30 fraktionen in 6 wochen verglichen . ergebnisse : die rhf nach 15 fraktionen variierte zwischen 28 und 100% ( tabelle 1 ) und korrelierte nicht mit der tcd50 nach 6 - wchiger fraktionierter bestrahlung ( abbildung 1 )  . 
dagegen korrelierten die tcd50 - werte nach einzeldosisbestrahlung signifikant mit der tcd50 nach 6 - wchiger bestrahlung . schlussfolgerung : die fraktion strahlenbiologisch hypoxischer tumorzellen nach 3 wochen fraktionierter bestrahlung scheint kein geeigneter prognostischer parameter zu sevielversprechend dagegen erscheinen die radiobiologischen parameter anzahl , intrinsische strahlenempfindlichkeit und anzahl radiobiologisch hypoxischer tumorstammzellen , um das ergebnis der fraktionierten bestrahlung vorherzusagen . schlsselwrter : tumorxenografts kopf - hals - tumoren strahlenbiologische hypoxie fraktionierte bestrahlung lokale tumorkontrolle 1department of radiation oncology and oncoray national center for radiation research in oncology , dresden , germany , 2experimental center , medical faculty and university hospital carl gustav carus , technische universitt , dresden , germany , 3division of quantitative sciences , university of texas , m.d. 
anderson cancer center , houston , tx , usa . received : february 7 , 2010 ; accepted : february 21 , 2011 published online : april 26 , 2011 strahlenther onkol 2011 no . 
radiobiological hypoxia and local tumor control after fractionated irradiation introduction solid tumors are characterized by specific pathophysiological features , e.g. , lactate accumulation , acidosis , abnormal perfusion , high interstitial fluid pressure , insufficient supply with nutrients and oxygen [ 14 , 15 ]  . 
during cancerogenesis malignant cells acquire the capability to survive under conditions of low oxygen which leads to the typical phenomenon of hypoxic and viable subvolumes within the tumor ( reviewed in [ 17 ] )  . 
in a panel of 10 different human head and neck squamous carcinomas ( hscc ) xenografted in nude mice , we used the clamped tumor control dose assay to determine rhf in untreated tumors , which ranged between 19% and 57% [ 20 ]  . 
however , rhf failed to accurately predict tcd50 after fractionated irradiation because five tumor models exhibited similar rhf values , but a large difference in tcd50 after fractionated irradiation by a factor of 2.5. 
this result may be explained by the fact that local tumor control after fractionated irradiation is determined not only by the initial extent of hypoxia but also by a number of other radiobiological factors , such as repopulation , reoxygenation , recovery from sublethal damage , redistribution , initial number and intrinsic radiosensitivity of tumor stem cells ( reviewed in [ 22 ] )  . 
as reoxygenation occurs during fractionated irradiation and the capacity to reoxygenate varies among different tumors [ 1 , 13 ] , we hypothesized that the prognostic value of rhf is higher when determined during fractionated irradiation than in untreated tumors . 
to test this hypothesis , rhf was determined after 3 weeks of fractionated irradiation in 6 tumor models from the previously studied panel . materials and methods animalsandtumorcelllines the animal facilities and the experiments were approved according to the institutional guidelines and the german animal welfare regulations . 
the experiments were performed using 7to 14 - week - old male and female nmri ( nu / nu ) mice obtained from the pathogen - free animal breeding facility ( experimental center , medical faculty , technische universitt dresden )  . 
to immunosuppress the nude mice further , they were total body irradiated 25 days before tumor transplantation with 4 gy ( 200 kv x - rays , 0.5 mm cu filter , ~1 gy / min )  . the experiments were performed using six established human squamous cell carcinomas ( hscc ) of head and neck : utscc - 15 , xf354 , ut - scc - 14 , fadu , sas , and ut - scc - 5 . 
it has been previously tested that none of the investigated tumor lines evoke significant residual immune response in nude mice [ 21 ]  . experimentaldesign to determine radiobiological hypoxic fraction ( rhf ) during fractionated irradiation , the animals were randomly allocated to one of two experimental arms : irradiation with 15 equal fractions over 19 days under normal blood flow conditions ( ambient ) followed by top - up single doses 24 hours after the last fraction either ( 1 ) under ambient conditions or ( 2 ) under homogeneously hypoxic ( clamp ) conditions . 
for correlation of rhf with outcome after fractionated irradiation , tcd50 values after 30 fractions over 6 weeks [ 19 ] determined in parallel were used for linear regression analysis . to achieve homogeneous hypoxia , a heavy clamp was placed over the proximal thigh of anesthetized mice 2 minutes before and during irradiation . 
for irradiation under ambient conditions , the nonanesthetized animals were immobilized using plastic tubes fixed on a lucite plate and the tumor - bearing leg was positioned in the irradiation field by a foot holder distal to the tumor . 
 the follow - up time after irradiation was at least 120 days , which is sufficient to detect 95% of local failures [ 18 ]  . a total of 896 tumors from the single dose experiments were included in the analysis . 
for each tumor cell line and for each experimental arm , the dose to cure 50% of tumors ( tcd50 ) was calculated as described previously [ 18 ]  . 
the radiobiological hypoxic fraction after irradiation with 15 fractions ( rhf15fx ) was calculated from the difference between the intercepts of the ambient and clamp single radiation doseresponse curves for local tumor control as described previously in detail [ 20 ]  . 
in contrast , top - up tcd50 values after single dose irradiation under ambient and clamp conditions of tumors previously irradiated with 15 fractions showed a strong association with radiation response after fractionated irradiation ( r2 = 0.97 , p = 0.0004 and r2 = 0.92 , p = 0.0024 , respectively ; figure 1 )  . discussion in the present study , the fraction of radiobiologically hypoxic tumor stem cells , i.e. , the radiobiological hypoxic fraction ( rhf ) , was determined after 3 weeks of fractionated irradiation in 6 human squamous cell carcinomas xenografted figure1 . 
tcd50 after fractionated irradiation ( tcd50 ( 30fx / 6w ) , [ 19 ] ) and radiobiological hypoxic fraction after 15 fractions ( rhf15fx ) , top - up tcd50 after irradiation with single doses under ambient ( top - up tcd50 ( sdambient ) ) and clamp ( top - up tcd50 ( sdclamp ) ) conditions of tumors previously irradiated with 15 fractions in 6 human squamous cell carcinoma lines in nude mice . 
tcd50 nach fraktionierter bestrahlung ( tcd50 ( 30fx / 6w ) , [ 19 ] ) und radiobiologisch hypoxische fraktion nach bestrahlung mit 15 fraktionen ( rhf15fx ) sowie top - up tcd50 nach einzeldosisbestrahlung unter ambienten ( top - up tcd50 ( sdambient ) ) und abgeklemmten ( top - up tcd50 ( sdclamp ) ) blutflussbedingungen nach bestrahlung mit 15 fraktionen in 6 human plattenepithelkarzinomlinien in nacktmusen . 
in a previous study , it was shown that the pretreatment rhf in the same 6 tumor models investigated here was found to be marginally significantly correlated with tcd50 after 30 fractions in 6 weeks ( r = 0.56 , p = 0.09 ; [ 20 ] )  . 
these findings do not support the hypothesis of the present study that rhf determined during fractionated irradiation has a higher prognostic value for outcome after fractionated irradiation than when determined in untreated tumors . 
thus , our experimental data suggest that potential surrogate markers of rhf , as rhf cannot be determined directly in patients , may provide prognostic information when assessed before start of treatment . 
in line with the results of the present study , in a previous investigation on fadu and another hscc model ( gl ) , the rhf determined after 2 and 4 weeks of fractionated irradiation was found to be different between the two tumor lines , whereas the tcd50 after 30 fractions over 6 weeks were not different [ 1 ]  . there are several limitations of the present study . 
first , the rhf and outcome of fractionated irradiation by nature of these assays could not be determined in the same individual tumor but parameters for a group of tumors were compared . 
the retrospective comparison of the prognostic value of rhf in the present study with data from previous experiments clearly represents a limitation of the present study . a possible explanation for the lack of correlation between rhf during treatment and outcome after fractionated irradiation is the fact that rhf represents a proportion , i.e. , a relative measure and not the total number of radiobiologically hypoxic tumor stem cells . 
obviously , it possible that a tumor with a small number of stem cells but a high rhf contains less radiobiologically hypoxic stem cells than a tumor with a higher number of stem cells and a lower rhf . 
the potential prognostic value of an absolute measure of radiobiologically hypoxic tumor stem cells is supported by the strong correlation of the single dose top - up tcd50 under ambient conditions after 15 fractions with the tcd50 after 30 fractions ( figure 1 )  . the tcd50 after single dose irradiation given under ambient conditions depends on the total number of surviving tumor stem cells , their intrinsic radiosensitivity , and the rhf [ 4 ]  . 
as the single dose tcd50 in the present study was determined after 3 weeks of fractionated irradiation , the total number of surviving stem cells is affected by a number of radiobiological mechanisms such as repopulation , reoxygenation , recovery of sublethal damage , and intrinsic radiosensitivity [ 22 ]  . 
interestingly , very similar to the observation reported here , our recent results using the hypoxia marker pimonidazole indicate that the total pimonidazole hypoxic tumor volume but not the fraction of pimonidazole hypoxic cells during treatment is prognostic for outcome after fractionated irradiation [ 19 ]  . 
the strong correlation of the single dose top - up tcd50 under clamp conditions after 15 fractions with the tcd50 after 30 fractions ( figure 1 ) suggests that the two parameters , number and intrinsic radiosensitivity of tumor stem cells , determine to a large extent the response to fractionated irradiation . taken together , our data obtained in a panel of hscc suggest that radiobiological parameters , such as the number of stem cells and their intrinsic radiosensitivity as well as the number of radiobiological hypoxic tumor stem cells determined during treatment , appear to be promising to predict local tumor control after fractionated radiotherapy . 
whether methods which can be applied in the clinic can predict outcome after radiotherapy in patients , e.g. , the gh2ax foci assay to estimate intrinsic radiosensitivity [ 7 , 10 ] , specific surface markers to assess the number of tumor stem cells [ 2 , 9 ] , and endogenous hypoxia markers [ 3 , 6 , 12 ] , requires further validation . acknowledgments the excellent technical assistance of k . 
the work was supported by the deutsche forschungsgemeinschaft ( dfg ba 1433 / 4 and ba 1433 / 5 ) , german federal ministry of education and research ( bmbf 03zik / oncoray ) and the schsische landesexzellenzinitiative . original article prospective study on the dose distribution to the acoustic structures during postoperative 3d conformal radiotherapy for parotid tumors dosimetric and audiometric aspects barbara a . 
jereczek - fossa1 , 5 , elena rondi2 , andrzej zarowski6 , alberto donofrio4 , daniela alterio1 , mario ciocca2 , livia corinna bianchi1 , marco krengli7 , luca calabrese3 , mohssen ansarin3 , gioacchino giugliano3 , roberto orecchia1 , 5 background and purpose : to analyze dose distribution in the hearing organ and to evaluate the dose effect on the hearing thresholds in patients treated with post - parotidectomy 3 - dimensional conformal radiotherapy ( 3d - crt )  . methods and materials : a total of 17 patients received post - parotidectomy 3d - crt ( median dose : 63 gy )  . 
longer followup and larger patient series are warranted to confirm these preliminary findings . key words : parotid tumors ear cochlea radiotherapy dosimetry dosevolume histograms strahlenther onkol 2011 ; 187 : 3506 doi 10.1007 / s00066 - 011 - 2170 - 5 prospektive studie zur dosisverteilung im hrorgan bei postoperativer 3d konformaler radiotherapie von parotistumoren . 
dosimetrische und audiometrische aspekte hintergrund und ziel : dosisverteilungsanalyse im hrorgan fr patienten mit 3 - dimensionaler konformaler radiotherapie ( 3d - crt ) nach parotidektomie . patienten und methoden : 17 patienten erhielten eine 3d - crt nach radikaler parotidektomie ( mittlere dosis : 63 gy )  . 
whrend des 2 - jhrigen follow - up zeigte keines der ohren perzeptive hrverluste bei sprachfrequenzen . 1division of radiotherapy , european institute of oncology , milan , italy , 2division of medical physics , european institute of oncology , milan , italy , 3division of head and neck surgery , european institute of oncology , milan , italy , 4department of experimental oncology , european institute of oncology , milan , italy , 5faculty of medicine of the university of milan , italy , 6university department of otolaryngology , head and neck surgery , st . 
augustinus hospital , antwerp , belgium , 7radiotherapy department , university of piemonte orientale , novara , italy . received : may 10 , 2010 ; accepted : february 22 , 2011 published online : may 16 , 2011 strahlenther onkol 2011 no . 
radiation dose to ear die mittleren dosen im ueren ipsilateralen gehrgang , in mastoidzellen , im trommelfell , in der eustachischen rhre , in bogengngen und cochlea waren 44 , 8 gy , 39 , 0 gy , 30 , 9 gy , 33 , 0 gy , 19 , 6 gy und 19 , 2 gy . 
die dosen im kontralateralen ohr waren vernachlssigbar , abgesehen von der eustachischen rhre ( bis zu 28 , 2 gy )  . schlussfolgerungen : 3d - crt nach parotidektomie ist mit relativ geringen dosen im hrorgan verbunden . 
lngere folgestudien und grere patientenserien sind gerechtfertigt , um diese vorlufigen ergebnisse zu besttigen . schlsselwrter : parotistumoren ohr cochlea radiotherapie dosimetrie dosis - volumen - histogramme introduction radiotherapy hearing impairment is a well - known complication of radiotherapy for head and neck cancer . 
in fact , up to 60% of the nasopharyngeal cancer patients treated with radiotherapy suffer from acute , transitory hearing deterioration during and within 3 months after irradiation [ 2 , 3 , 12 , 17 ]  . 
however , the dose to the auditory structures is only rarely assessed in standard radiotherapy for head and neck cancer and in clinical trials [ 1 , 11 , 24 , 26 , 29 , 30 , 32 ]  . 
relatively few dosimetric studies on the ear dose in radiotherapy planning for head and neck cancer have been published so far and the majority of them include nasopharynx , paranasal sinus , and nasal cavity tumors [ 2 , 3 ]  . 
the aim of our prospective study was to analyze the dose distribution in the ear structures in the patients treated with postoperative 3 - dimensional ( 3d ) conformal radiotherapy for parotid tumors . 
moreover , correlation with audiometric endpoints is analyzed . material and methods study design the inclusion criteria for this prospective study were as follows : radical surgery for parotid tumor ( no macroscopic residual disease was permitted ) , indication for postoperative radiotherapy with conventionally fractionated schedules ( minimum total dose 60 gy ) , no chemotherapy , no previous radiotherapy , availability for baseline audiometric evaluation and follow - up , and written conformed consent . 
patients with pre - existing hearing disorders or history of ear surgery were not included . patient population between september 2004 and january 2007 , 17 patients ( mean age , 56 years ) were treated at the european institute of oncology , milan , italy , with parotidectomy and postoperative 3dconformal radiotherapy for parotid tumors ( table 1 ) [ 28 ]  . 
median total radiotherapy dose prescribed to the international committee of radiation units and measurements ( icru ) reference point was 63 gy ( range , 6070 gy ) [ 15 ]  . elective lymph node irradiation was performed in 13 patients . 
the middle , lower cervical , and supraclavicular lymph nodes were treated with an anterior photon beam up to 50 gy prescribed at the depth of 3 cm . in all patients , a custom mask for head immobilization was used . 
correction for tissue inhomogeneity ( equivalent tissueair ratio correction ) was employed for all patients . dosimetric analysis using the original planning ct scans , the external , middle , and inner ear structures were delineated ( external auditory canal , mastoid cells , tympanic case , eustachian tube , semicircular canals , and cochlea )  . 
patienten - , tumorund therapie - bezogene eigenschaften . number of patients ( % ) characteristics gender male female age in years mean range tumor localization superficial deep superficial and deep unknown tumor stage ( tnm 2002 classification ) a metastatic parotid tumor recurrent parotid tumor tumor histotype adenoidcystic carcinoma metastasis salivary ducts carcinoma mucoepidermoid carcinoma squamous cell carcinoma myoepithelial carcinoma adenocarcinoma pleomorphic adenoma type of surgery superficial parotidectomy radical parotidectomy wide tumor excision neck surgery yes ( ipsilateral neck dissection ) dose to the tumor bed ( icru point ) b in gy mean range dose to the n - positive neck in gy mean range dose to the n - negative neck in gy mean range 9 ( 52.9% ) 8 ( 47% ) 3979 6 ( 35.2% ) 2 ( 11.7% ) 5 ( 29.4% ) 4 ( 23.5% ) 3 ( 17.6% ) 4 ( 23.5% ) 1 ( 5.8% ) 3 ( 17.6% ) 4 ( 23.5% ) 2 ( 11.7% ) 4 ( 23.5% ) 4 ( 23.5% ) 3 ( 17.6% ) 2 ( 11.7% ) 1 ( 5.8% ) 1 ( 5.8% ) 1 ( 5.8% ) 1 ( 5.8% ) 4 ( 23.5% ) 12 ( 70.5% ) 1 ( 5.8% ) 7 ( 41.1% ) 10 ( 58.8% ) 63 gy 6070 gy 63 gy 6066 gy 52 gy 5054 gy atnm tumor , node , metastasis classification [ 28 ] ; bicru international committee of radiation units and measurements [ 15 ]  . follow - up and audiometric evaluation the audiometric evaluation comprised pure tone audiometry performed in a soundproof chamber and tympanometry . 
four - tone ( 0 , 5 , 1 , 2 and 3khz ) average thresholds for air and bone conduction were used for data analysis [ 3 , 8 ]  . patients were longitudinally followed during a period of at least 2 years . 
audiometric evaluation was performed before irradiation and at 3 , 6 , and 24 months after completion of radiotherapy . statistical methods for the assessment of the significant long - term injury , the binomial test was used . 
minimum , maximum , mean , median , lower , and upper quartiles of the dvh curves were obtained by calculating the minimum , maximum , mean , median , and quartiles , respectively , of the percentages of the irradiated structure at each dose level . 
 results dosimetric analysis dosimetric analysis showed the highest doses in the ipsilateral external auditory canal ( up to 72.2 gy , mean dose 44.8 gy ; table 2 )  . 
the dvhs for the ipsilateral structures in all patients are shown in figures 16 . audiometric evaluation before radiotherapy , the median baseline audiometric thresholds were normal ( 20 dbhl and 18 dbhl for ipsiand contralateral ear , respectively )  . 
at 3 months after irradiation , 3 patients showed transient symptoms of middle ear underpressure and / or effusion that resolved completely by the following evaluations at 6 or 12 months . 
in particular , the mean dose to the ipsilateral cochlea was 19.2 gy and this value is below the reported value in the literature as a cochlea dose threshold [ 3 ]  . 
the maximum cochlear dose ( 52.2 gy ) observed in one patient in our series is near the threshold for late hearing loss . the threshold dose for the cochlea is not clear and ranges between 30 and 70 gy [ 14 , 17 , 25 , 27 ]  . 
 [ 2 ] observed in the retrospective analysis of 325 head and neck cancer patients that starting at 55 gy the incidence of sensodose ( gy ) dose ( gy ) figure 1 . 
the 5and 10 - year actuarial risk of clinically overt snhl increased to 37% above doses of 60.5 gy compared to 3% at doses below 60.5 gy [ 2 ]  . 
 [ 3 ] concluded that for conventionally fractionated radiotherapy , the mean dose to the cochlea should be limited to < 45 gy , which was the case in all patients in our series . contrarily to our findings ( no hearing loss at 2 years in the series of 17 parotid cancer patients ) , van der putten et al . 
to our knowledge , the majority of the reports on radiation - induced ototoxicity used conventional 2d - radiotherapy approach [ 17 ]  . our study has a number of limitations . 
the cumulative risk of a significant persistent snhl ( > 15 db ) seems to stabilize within 2 years [ 10 , 21 ] , whereas for severe snhl ( > 30 db ) the cumulative risk also continues to increase through the third and fourth year [ 10 ]  . 
in a series with long follow - up ( median of 13 years ) , stable rather than progressive character of snhl was observed [ 18 ]  . the limited number of patients included in our study does not allow for evaluation of the impact of various clinical and physical variables on the ear radiation - induced injury . 
several patient - , tumor - , and treatment - related factors have been reported to be associated with the risk of hearing impairment after irradiation including total radiotherapy dose [ 2 , 6 , 23 ] , fractionation [ 2 ] , site of the tumor ( nasopharyngeal and parotid tumors associated with the higher risk ) [ 22 ] , involvement of the upper cervical lymph nodes [ 9 ] , stereotactic radiotherapy in the patient affected by neurofibromatisis 2 [ 9 ] , age greater than 50 years [ 2 , 12 , 23 ] , hearing deficit present before radiotherapy [ 12 , 23 ] , and use of cisplatin - containing chemotherapy [ 2 , 13 ]  . 
lower ototoxicity in the parotid cancer patients when compared to the squamous cell head and neck cancer cases observed in some series may be explained by no use of chemotherapy in the postoperative approach in parotid tumors , lower mean patient age , lower radiotherapy dose ( due to adjuvant irradiation ) , unilateral radiotherapy , and particular ( superficial ) tumor location . the superficial position of the parotid bed after surgery and the use of unilateral irradiation is related to the higher dose to the superficial acoustic structures ( ipsilateral mastoid cells , external auditory canal , and middle ear ) when compared to the deep structures or contralateral acoustic organ ( apart from the contralateral eustachian tube dose of up to 28 gy )  . 
contrarily , the dysfunction of eustachian tube ( patulous tube ) was observed in about 50% of long - term survivors of nasopharyngeal carcinoma ; however , the correlation between radiation dose and risk of this late effect was not analyzed [ 7 ]  . new radiotherapy techniques and modalities can be associated with lower dose to the auditory structures . 
for example , use of conformal proton radiotherapy to the posterior fossa limited the dose to the inner and middle ear to an average mean of 25 + 4% , when compared to 75 + 6% administrated to these structures with 3d photon therapy [ 19 ]  . 
similarly , the use of intensity modulated radiotherapy ( imrt ) allows for a significant reduction in the cochlear dose when compared to the conventional radiation technique [ 20 ]  . conclusion postoperative modern 3d - conformal radiotherapy for parotid tumors is associated with relatively low doses to the auditory structures . 
this is due to the superficial position of the parotid bed , unilateral irradiation , use of conformal techniques , and postoperative approach requiring lower prescription doses than in the curative approach . 
in the future , these data will help to establish the reliable dose constraints for acoustic structures . original article adjuvant chemoradiation after laparoscopically assisted radical vaginal hysterectomy ( larvh ) in patients with cervical cancer oncologic outcome and morbidity arne gruen1 , thabea musik1 , christhardt khler2 , jrgen fller3 , thomas wendt3 , carmen stromberger1 , volker budach1 , achim schneider2 , simone marnitz1 purpose : compared to laparotomic surgery , laparoscopically assisted radical vaginal hysterectomy ( larvh ) offers decreased blood loss during surgery and faster convalescence of the patient postoperatively , while at the same time delivering similar oncologic results . 
 grade4 side effects were not observed . conclusion : with similar oncologic outcome data and mostly mild side effects , larvh followed by ( chemo ) radiation is a valid alternative in the treatment of cervical cancer patients . key words : cervical cancer laparoscopically assisted radical vaginal hysterectomy ( larvh ) ( chemo - ) radiotherapy toxicity strahlenther onkol 2011 ; 187 : 3449 doi 10.1007 / s00066 - 011 - 2197 - 7 adjuvante radiochemotherapie nach laproskopisch assistierter radikaler vaginaler hysterektomie ( larvh ) bei patientinnen mit zervixkarzinoonkologische ergebnisse und morbiditt ziel : die laparoskopisch assistierte radikale hysterektomie ( larvh ) bietet gegenber offenen verfahren bei patientinnen mit gynkologischen tumoren die vorteile eines geringeren blutverlusts und einer schnelleren rekonvaleszenz bei onkologisch gleichwertigen ergebnissen . 
bisher existieren keine daten zu onkologischen ergebnissen und toxizitt nach larvh und adjuvanter radio ( chemo ) therapie . patienten und methodik : 55 patientinnen ( 2878 jahre ) mit zervixkarzinomen ( figo ib1 bis iiia ) , ( tabellen 1 , 2 ) wurden ausgewertet . 
die patientinnen wurden nach larvh aufgrund von risikofaktoren einer postoperativen perkutanen strahlentherapie [ ebrt : n = 8 ( 14% ) , inklusive paraaortalfeld ( efrt ) : n = 4 ( 2 , 2% ) , einer ebrt und brachytherapie ( bt ) : n = 33 ( 60% ) , einer alleinigen bt : n = 14 ( 25 , 5% ) ] bzw . 
grad - 4 - nebenwirkungen wurden nicht beobachtet . schlussfolgerung : bei insgesamt sehr niedrigen raten gastrointestinaler ( gi ) und urogenitaler ( gu ) toxizitt stellt die larvh im kontext mit der adjuvanten radio ( chemo ) bzw . 
brachytherapie eine valide alternative zu offenen verfahren in der behandlung von patientinnen mit zervixkarzinomen dar . schlsselwrter : zervixkarzinom laparoskopisch assistierte radikale vaginale hysterktomie ( larvh ) radio ( chemo ) therapie toxizitt 1department of radiooncology , charit university medicine berlin , campus virchow - klinikum , berlin , germany , 2department of gynaecology , charit university medicine berlin , campus mitte und benjamin franklin , berlin , germany , 3department of radiooncology , university hospital , jena , germany . received : july 20 , 2010 ; accepted : january 24 , 2011 published online : may 16 , 2011 strahlenther onkol 2011 no . 
larvh in patients with cervical cancer introduction compared with open approaches , laparoscopically assisted radical vaginal hysterectomy ( larvh ) , total laparoscopic hysterectomy , and robot - assisted radical hysterectomy offer decreased blood loss during surgery , quicker recovery , and improved cosmetic results [ 26 , 48 ]  . 
the oncologic outcome of laparoscopically assisted techniques is considered equal to that of laparotomic hysterectomy [ 9 , 18 , 22 , 23 , 25 , 37 , 4043 ]  . with the presence of risk factors or their combinations ( pn + , r1 , g3 , l1 , v1 , iib ) , adjuvant chemoradiation is recommended to improve local control and disease - free and overall survival [ 14 , 16 , 28 , 34 , 38 , 44 , 45 ]  . 
extended field irradiation ( efrt ) is added when lymph node metastases are found [ 15 , 17 , 29 ]  . an increase in toxicity can be observed with the combination of radical surgery and radiation [ 24 ]  . 
the most pronounced incidence rates were seen in patients receiving radical hysterectomy followed by adjuvant radiotherapy [ 33 , 36 , 49 ] , whereas surgical interventions with less radicality followed by adjuvant radiotherapy were associated with a favorable spectrum of side effects [ 13 ] , corroborating the importance of atraumatic surgical interventions especially in patients necessitating postoperative adjuvant therapy . overall gastrointestinal ( gi ) and genitourinary ( gu ) late effects are observed in up to 17% of the patients [ 6 , 8 , 47 ] in the combined approach and 511% in radiation only regimens . 
the overall risk of developing lymphedema is increased in patients with cervical cancer receiving radiotherapy [ 1 , 4 , 12 ] , ranging from 2% after simple hysterectomy plus radiotherapy to 10% after radical hysterectomy plus radiotherapy . 
vaginal and uterine necroses are rare events necessitating surgery [ 27 , 32 ]  . it has not yet been systemically addressed whether larvh followed by adjuvant treatment is advantageous concerning either acute or late toxicity compared to patients receiving open surgery followed by adjuvant treatment [ 2 , 3 , 5 , 7 19 , 21 ]  . patients and methods from 19992004 , 204 women with histologically confirmed cervical cancer ( figo ib1iiia ) were subjected to larvh at the departments of gynecology , friedrich - schiller university jena and charit , berldue to risk factors , adjuvant ( chemo ) radiation was indicated in 94 patients . 
of these 94 patients , 27 received ( chemo ) radiation at other institutions and 12 were lost to follow - up ; therefore , 55 patients were analyzed . all patients were subjected to larvh beginning with systematic transperitoneal laparoscopic pelvic and paraaortic lymphadenectomy as described previously [ 22 ]  . the therapy decision was always based on the decision from a multidisciplinary tumor board . 
until 1996 , patients receiving bt alone received 40gy in 4 fractions ; after 1996 , patients received 28gy in 4 fractions standardized to 5 mm mucosal depth . chemotherapy of our patients ( n = 17 ) treated after 1999 presenting with 2 or more risk factors each , 12 received combined chemoradiotherapy . 
six patients received cisplatin monotherapy ( 4 patients received 20 mg / m body surface area ( bsa ) ; 2 patients received 40 mg / m bsa )  . 
figo - stadium und histologie . follow - up for follow - up , the patients were seen in the university outclinics in jena and berlin every 3 months during the first 2 years after treatment and every 6 months thereafter . 
each follow - up consisted of gynecological examinations and initiation of further diagnostics , if necessary . histology / figo stage adenocarcinoma sqamous cell carcinoma statistical analysis intraand postoperative data were collected retrospectively from the patients files and transferred to spss12.0 windows and window excel . 
grading showed 3 ( 5% ) well differentiated ( g1 ) , 22 ( 40% ) moderately differentiated ( g2 ) , and 30 ( 55% ) poorly differentiated tumors . 
lymphovascular space involvement ( lvsi ) was demonstrated in 11 of 17 ( 35% ) patients , while vascular space involvement ( vsi ) was observed in 15 of 29 ( 52% ) patients . 
lymph node statuses are shown in table 2 . surgery a total of 21 ( 38% ) patients underwent larvh type ii and 34 patients larvh type iii ( 62% ) according to piver et al . 
average metastasisand recurrence - free survival was 4.27years , corresponding to a 5 - year dfs of 81.8%. after 249 months , 10 ( 18.1% ) patients developed progressive disease . 
four patients showed pelvic wall recurrence , 1vaginal stump , and 1patient presented a schuchardts incision recurrence , which corresponds with a 5 - year local control rate of 89% . 
 during follow - up , 4 ( 7% ) patients developed distant metastases ( ovary , n = 1 ; peritoneum , n = 2 ; lung , n = 1 )  . all 10patients developing any kind of recurrence had been subjected to either ebrt or bt alone without chemotherapy . 
 after an average of 5.7months after diagnosis of progressive disease , 8patients had died . comparing the oncologic data with regard to risk factors ( r0 versus r1 ; pn1 versus pn0 ; g1 / 2 versus g3 ; v0 versus v1 ) , neither univariate analysis nor multivariate analysis ( cox regression analysis ) delivered significant results . 
the 5 - year dfs in 25patients ( 45.5% ) with good or moderate tumor differentiation ( g1 / g2 ) did not differ from patients with poorly differentiated tumors ( 84% versus 80% )  . 
specimen of only 17patients were analyzed for lvsi ; therefore , due dfs analysis was not performed for this subgroup . acute side effects were observed in 37patients ( 67% ) , mainly being gi and dermatologic symptoms . 
six patients with late complications had had an larvh typeiii , while 2patients had an larvh typeii . mild lymphedema make up the major share in late toxicities , although the affected patients had a similar mean number of lymph nodes excised compared to the remaining cohort ( 28ln versus 24ln )  . 
the fistula was treated by colpocleisis ; at the last follow - up , the patient was symptom free . discussion laparoscopically assisted radical vaginal hysterectomy ( larvh ) offers a valid alternative to laparotomic hysterectomy with apparent advantages , e.g. , decreased blood loss during surgery , shorter hospital stays , quicker convalescence , and improved cosmetic results , while at the same time delivering equal oncological outcome data [ 9 , 18 , 22 , 23 , 25 , 37 , 4043 ]  . 
 this led to the presumption that the toxicity profile of lavrh followed by adjuvant ( chemo ) radiation might also be favorable compared to that of laparotomic radical hysterectomy followed by ( chemo ) radiation . 
a further limitation of our study is the incomplete data concerning vascular ( vsi ) and lymphovascular space involvement ( lvsi ) in only 26of 55patients , thus , rendering comments on the prognostic values in this regard impossible . oncological outcome of the present study was comparable to the randomized trial by peters et al . 
though incomplete resections are an established negative predictor for outcome [ 11 ] , again , due to the small group size , local recurrencefree survival , disease - free survival , and overall survival ( 87% , 80% , and 5% , respectively ) did not differ significantly compared to the complete resection group ( 89% , 87% , 85% , respectively )  . there were no statistical differences in local recurrencefree survival , dfs , and os comparing g1 / 2 to g3tumors . 
although statistically not significant , our overall survival data for non - vsi ( 95% ) and vsi ( 80% ) patients exactly match those of the figo report . published data on lavrh mainly focuses on surgery - associated morbidity and outcome [ 2 , 5 , 7 ]  . 
the discussion and comparison of available data are hampered by a lack of documentation of radiogenic side effects [ 39 ] , intermingling of acute and late effects [ 20 ] , use of outdated scoring / documentation systems [ 11 ] , and use of outdated radiotherapy techniques leading to high numbers of bowel obstructions [ 20 ]  . there were 4grade3 acute toxicities in our group ( diarrhea , n = 1 ) , incontinence ( n = 1 , ebrt alone ) , vesicovaginal fistula ( n = 1 ) , and hematologic ( n = 1 )  . 
larvh in patients with cervical cancer incontinence rate is far more pronounced [ 30 , 31 , 46 ] with the rate of fistulas after surgery or radiotherapy being > 1% [ 10 ]  . 
in the subgroup of patients receiving ebrt and bt , some patients complained of pollacisuria and cystitis . grade 13 late effects were observed in 14.5% of the patients , 5 patients with lower extremity lymphedema . 
sophisticated radiotherapy techniques for external beam irradiation [ 30 , 31 , 46 ] and brachytherapy [ 10 ] provide the chance to further decrease therapy - related toxicity and should be widely used , even in patients with adjuvant radiation . conclusion our data demonstrates that larvh followed by adjuvant ( chemo ) radiation is feasible and safe . 
compared to the randomized controlled trials and retrospective data available , we were even able to decrease the incidence of severe side effects . original article treatment of acute radiodermatitis with an oil - in - water emulsion following radiation therapy for breast cancer a controlled , randomized trial jens - michael jensen1 , tanja gau1 , jrgen schultze2 , gunter lemmnitz3 , regina flster - holst1 , theodor may4 , christoph abels3 , ehrhardt proksch1 background : a side effect of radiotherapy for breast cancer is acute radiodermatitis . 
 patients and methods : we performed a randomized , controlled , open - label study with 66 patients ( itt population ) , treating the irradiated skin in one group ( n = 34 ) with an oil - in - water emulsion ( wo1932 ) , while leaving the other group untreated ( n = 32 )  . 
 clinical scoring ( ons radiation skin reaction scoring , pruritus ) and biophysical measurements ( stratum corneum hydration and transepidermal water loss ( tewl ) , as a marker of skin barrier function ) were determined at day1 ( directly after termination of the radiation therapy ) , day8 , and day47 ( 7 )  . results : irradiation increased the ons score and pruritus , whereas skin hydration and tewl were reduced . 
the primary hypothesis that the increase in skin hydration was significantly greater in the emulsion - treated compared to the untreated group as early as after 8 days of treatment could not be confirmed . 
at the end of the study ( day 47 7 ) , however , normalization of stratum corneum hydration was more advanced in the treatment group compared to the untreated group and nearly reached the values of the contralateral healthy breast skons score and pruritus also revealed an advantage for the emulsion - treated group . 
no adverse events were caused by the treatment regimens . conclusion : treatment of radiodermatitis with an oil - in - water emulsion was well tolerated , enhanced stratum corneum hydration , improved clinical indicators , and provided relief from itching . key words : radiodermatitis breast cancer stratum corneum hydration skin barrier function oil - in - water emulsion strahlenther onkol 2011 ; 187 : 37884 doi 10.1007 / s00066 - 011 - 2224 - 8 behandlung akuter radiodermatitis mit einer l - in - wasser - emulsion nach strahlentherapie bei brustkrebs . 
 patienten und methoden : in einer kontrollierten , randomisierten , unverblindeten studie behandelten wir 34 von 66 brustkrebspatientinnen ( itt - population ) mit einer l - in - wasser - emulsion ( wo1932 ) , 32 patienten blieben unbehandelt . 
 1department of dermatology , university hospitals of schleswig - holstein , university of kiel , germany , 2department of therapeutic radiology , university hospitals of schleswig - holstein , university of kiel , germany , 3august wolff gmbh & co . 
kg arzneimittel , bielefeld , germany , 4gesellschaft fr biometrie und psychometrie gbr , bielefeld , germany . received : september 27 , 2010 ; accepted : february 23 , 2011 published online : may 16 , 2011 strahlenther onkol 2011 no . 
die ergebnisse zeigen , dass wo1932 das klinische bild verbesserte , den wassergehalt des stratum corneum erhhte und den juckreiz reduzierte . schlsselwrter : radiodermatitis brustkrebs wassergehalt des stratum corneum hautbarriere l - in - wasser - emulsion introduction radiation therapy following surgery has been proven to be a very effective therapy for breast cancer [ 35 ] but commonly causes radiodermatitis . 
although radiation oncologists try to reduce irradiation treatment doses [ 13 , 17 , 22 ] , approximately 96% of all patients receiving radiation treatment experience skin reactions [ 8 , 16 , 19 , 20 , 37 ]  . 
reduced stratum corneum hydration , a disturbed skin barrier function when the skin is stressed , and itching are key signs of dry skin [ 5 ]  . patients often repeatedly request treatment for dry sk dermatologists suggest treating the dry skin with emollients . 
nevertheless , treatment after radiation therapy with emollients containing urea , dexpanthenol , hyaluronic acid , sulcrafate , aloe vera , triethanolamine , calendula , barrier films , or anti - inflammatory agents including corticosteroids has been studied [ reviewed by 15 and 3 , 12 , 21 , 25 , 29 , 33 ] , but there is still no widely accepted treatment regimen . 
for some of the agents , the potential development of contact sensitivity should not be underestimated ( in particular calendula and aloe vera )  . this study sought to prove the hypothesis that treatment with the oil - in - water emulsion wo1932 leads to a more rapid normalization of stratum corneum water content ( hydration ) , improves skin barrier function ( transepidermal water loss , tewl ) , ons score , and pruritus in the treatment group compared to the untreated control group . 
we asked whether the mean increase in relative skin hydration from baseline to visit 2 ( study day 8 ) was significantly greater in the treatment group compared to the untreated group . 
in addition , it was tested whether the increase in relative skin hydration from baseline to the end of study was greater in the treatment group compared to the control group . 
it was expected that the study preparation would lead to more rapid normalization of skin hydration on the irradiated breast . 1 material and methods patients and treatment regimens this single - center study was as a randomized , controlled and open label trial . 
a total of 68 adult females who had undergone radiotherapy for breast cancer following surgery and were experiencing radiodermatitis with an ons score of 03 were randomized to a treatment group ( n = 34 ) and to a control group ( n = 34 )  . 
 the intention - to - treat population ( itt ) comprised 66 patients ( treatment group : n = 34 , control group : n = 32 ) ; the per - protocol population ( pp ) comprised 64 patients ( treatment group : n = 34 , control group : n = 30 ) ; see statististical analyses for details . 
the oil - in - water emulsion contains unsaturated fatty acids among other excipients , in particular a mixture of 9 , 11and 9 , 12 - octadecadienoic acid ( linoleic acid )  . 
 biophysical measurements ( stratum corneum hydration and transepidermal water loss ( tewl ) ) and clinical assessments ( pruritus and ons scoring ) of both groups were performed at baseline ( visit 1 , day 1 ) , after 1week ( visit 2 , day 8 ) , and after 68 weeks of treatment ( visit 3 )  . 
pruritus was recorded by the patients in a pruritus diary , according to a visual analog scale from 110 ( 1 = no pruritus , 10 = severe , intolerable pruritus )  . 
cream treatment in radiodermatitis ( length in cm ) was transformed to a scale ranging from 0 ( no pruritus ) to 100 ( severe )  . biophysical measurements stratum corneum hydration and tewl were determined at each visit in both lesional and non - lesional skin using the corneometer and the tewameter tm210 ( both courage & khazaka , cologne , germany ) in accordance with the guidelines of the standardization group of the european contact dermatitis society [ 6 , 23 ]  . 
during the course of all measurements , relative environmental humidity was 45 2% and temperature was 22 1 c . the primary efficacy parameter of the study plan was the change in skin hydration as measured by the corneometer at visit 2 ( study day 8 ) compared to visit 1 ( baseline )  . 
in order to reduce environmental effects , skin hydration of the irradiated area was assessed in relation to the nonirradiated area and the differences between skin hydration of the irradiated field ( breast ) and skin hydration of the nonirradiated field ( contralateral breast ) were calculated before and after treatment . 
therefore , the treatment group comprised of 34 patients ( itt & pp ) , whereas the control group comprised of 32 patients ( itt ) and 30 patients ( pp ) , respectively . for the secondary efficacy parameters , the results for the pp population were reported only . 
the reason is that the pp population and itt population differ only in regard to 2 untreated patients that dropped out ( after visit 1 and before visit 2 )  . 
 a total of 66 patients were included ; however , 2 patients allocated to the control group dropped out before or at visit 1 ( violation of inclusion criteria and nonattendance ) and were excluded from the visit 1 , untreated o1932 visit 1 , w visit 2 , untreated o1932 visit 2 , w visit 3 , untreated o1932 visit 3 , w figure 1 . 
at study visit 1 before the initiation of treatment , the ons radiation skin scores were similarly distributed in both the treatment group and the control group ( figure 1 )  . 
pruritus decreased during the study , but was less pronounced in the treatment group compared to control group , especially at week 1 , 2 , 3 , and 5 ( p = 0.035 , p = 0.038 , p = 0.039 , p = 0.026 , respectively ; onesided , exact mannwhitney test ; figure 2 )  . stratum corneum hydration the primary hypothesis that the mean increase in relative skin hydration as measured by the corneometer from baseline was significantly greater in the treated group compared to the unpruritus = untreated , = wo1932 tolerability 1 3 5 7 9 11 13 15 17 19 21 23 25 27 29 31 33 35 37 39 41 43 figure 2 . 
time course of the severity of pruritus ( mean and standard error ) , which was assessed by the patients using a visual analogue scale ( 0 = no pruritus , 100 = severe pruritus ) , is shown . 
die abbildung zeigt den zeitverlauf des schweregrades des juckreizes ( mittelwert und standardfehler ) , der von den patienten auf einer visuellen analogskala ( 0 = kein juckreiz , 100 = schwerer juckreiz ) angegeben wurde . 
der juckreiz verringerte sich in beiden gruppen nach dem ende der bestrahlungstherapie allmhlich , wobei der juckreiz in der behandlungsgruppe im vergleich zur unbehandelten kontrollgruppe geringer ausgeprgt war . treated group was not yet confirmed at visit 2 ( study day 8 ; itt : p = 0.377 ; pp : p = 0.421 , one - sided t - test )  . 
corneometer values at visit 1 until visit 3 on the irradiated and nonirradiated side and after treatment with the wo1932 versus untreated controls are shown in table 1 and figure 3 . 
 transepidermal water loss transepidermal water loss ( tewl ) as a marker of skin barrier function in the irradiated fields was significantly lower compared to the unirradiated field throughout the study . 
however , the differences in tewl ( unirradiated irradiated skin ) were not significant between the treatment and control group at all visits ( figure 4 )  . wo1932 was well tolerated and no serious adverse events were reported . 
reported systemic adverse events , headache , and muscle pain in 2 patients ( out of 34 patients ) of the treatment group ( 5.9% ) were minor , classified as unrelated to the study drug , required no further action , and did not lead to discontinuation of the study . discussion acute radiodermatitis is probably the most disturbing side effect of radiation therapy for breast cancer . 
since damage of the skin above the cancer should be avoided , it is therefore widely accepted in radiation therapy and supported by older studies [ 14 , 18 , 38 , 39 ] to keep the irradiated area dry during and even after radiation therapy . 
powder increases the surface , leads to evaporation of the heat , and therefore reduces the erythema , but also reduces the water content of the stratum corneum [ 7 ] resulting in very dry skhowever , very dry skin leads to pruritus or burning sensations , which further impairs the patients quality of life [ 5 ]  . despite an inflammatory infiltrate in acute radiodermatitis , irradiated skin is primarily characterized as being dry sk therefore , we examined whether rehydration of the stratum corneum by an emulsion might reduce the clinical symptoms of radiodermatitis . 
it is known that an oil - in - water emulsion improves dry skin , leads to enhanced levels of stratum corneum hydration , and reduces clinical symptoms like redness , strahlenther onkol 2011 no . 
stratum corneum hydration ( corneometry ) at visit 1 ( day 1 , baseline ) , visit 2 ( day 8 ) , and at visit 3 ( day 47 7 ) in emulsion - treated and untreated patients are shown . 
at visit 3 , the differences between nonirradiated and irradiated fields in skin hydration were significantly lower in the treatment group compared to the control group ( p = 0.0096 ; one - sided t - test , itt population ) , but not at visit 1 or visit 2 . 
die tabelle zeigt die stratum - corneum - hydratation ( corneometrie ) bei allen drei visiten in emulsions - behandelter und unbehandelter haut im vergleich : die unterschiede zwischen bestrahlter und unbestrahlter haut waren erst bei der dritten visite in der behandlungsgruppe signifikant niedriger als in der kontrolle ( p = 0.0096 ; einseitiger t - test , itt - population )  . 
the key role of an emulsion is in the smoothing and rehydration of dry sk however , an emollient can also play an important role in terms of reduction of inflammation and pruritus and the restoration of normal epidermal differentiation , and this is of particular importance in radiodermatitis . during proper differentiation the water binding capacity normalizes because of enhanced production of physiological water binding compounds , e.g. , derived from filaggrin breakdown [ 28 ]  . 
the use of lipids helps to reduce tewl by providing provisional lipid layers as a substitute for the disturbed lipid layers in diseased skin conditions like severe dry skin and eczema [ 27 ]  . 
this is the first time that the positive effects of an emulsion on the dry skin condition in radiation dermatitis were shown by biophysical measurements of stratum corneum hydration . the increase in stratum corneum hydration in radiodermatitis is related to the composition of the oil - in - water emulsion since wo1932 is a medical device containing water , in particular among other excipients and a mixture of 9 , 11and 9 , 12 - octadecadienoic acid ( linoleic acids )  . 
this may be attributed to the unsaturated fatty acids in the formulation , in particular the mixture of linoleic acids , which influence skin physiology , skin barrier function , membrane fluidity , and eicosanoid production . 
in particular , linoleic acid is part of the phospholipids in cell membranes and also part of the ceramides in the intercellular lipids in skin barrier function [ 28 ]  . 
previous studies using urea , corticosteroids , or other ingredients could not prove significant further advantages of the components used in comparison to an oil - in - water emulsion [ reviewed by 15 and 3 , 12 , 21 , 25 , 29 , 33 ]  . stratum corneum hydration may correlate inversely proportionally to tewl as a marker of skin barrier function , as shown , for example , in atopic dermatitis [ 9 , 10 ]  . 
however , in the present study tewl was significantly reduced in irradiated skin compared to unirradiated skit is very likely that tewl is reduced in irradiated skin due to a hardening effect . 
stratum corneum hydration ( mean with standard error ) was significantly reduced in irradiated skin compared to unirradiated skin at visits 1 and 2 ( p < 0.01 , one - sided t - tests ) in the treatment group as well in the untreated control group ( n = 34 and 32 , respectively )  . 
at visit 3 ( day 47 7 ) , the difference ( unirradiated irradiated skin ) was no longer significant in the treatment group ( p = 0.11 , one - sided t - test ) , but was still significant in the control group ( p < 0.01 , one - sided t - test )  . 
die erniedrigte hydratation des stratum corneum in bestrahlter haut verbesserte sich schneller in der emulsions - behandelten gruppe und war bei der dritten visite ( tag 47 7 ) fast normal verglichen mit der haut der kontralateralen gesunden kontrollbrust ( p = 0 , 11 , einseitiger t - test ) , whrend sie in der kontrollgruppe noch signifikant niedriger war ( p < 0 , 01 ; t - test ) war . a hardening effect after repeated exposure to noxious stimuli is described for contact dermatitis ( e.g. , chromate allergy in masons ) [ reviewed in 36 ] , uv irradiation [ 1 , 2 ] , but also for xray irradiation [ 31 , 34 ]  . 
hardening occurs after chronic irritation of the skin because epidermal hyperproliferation leads in particular to thickening of the stratum corneua thickened stratum corneum may improve the barrier toward irritation from the outside and reduces tewl as a sign of the inside outside barrier . 
tewl ( mean with standard error ) was significantly reduced in irradiated skin compared to unirradiated skin at each visit ( p < 0.05 , one - sided t - tests ) in the treatment group as well in the untreated control group ( n = 34 and 30 , respectively )  . 
 es ergaben sich jedoch keine signifikanten unterschiede fr die tewl ( unbestrahlte / bestrahlte haut ) zwischen der behandlungsund der kontrollgruppe ( p > 0 , 05 ; einseitiger t - test fr jede visite )  . conclusion this randomized clinical trial indicate that treating skin directly after irradiation with an oil - in - water emulsion leads to beneficial effects , although the primary efficacy parameter , the assumption that the increase in skin hydration was significantly greater in the treatment group compared to the untreated group as early as after 8 days of treatment , did not reach significance at that time point . 
however , at visit 3 hydration was significantly more improved in the treatment group , and other secondary efficacy parameters , reduction in ons score and pruritus was in favor of the emulsion treatment . 
 original article incidence of dermatitis in head and neck cancer patients treated with primary radiotherapy and cetuximab edgar selzer1 , susanne liederer1 , christiane lemaire1 , gerhard kren2 , dejan radonjic1 , gabriela kornek3 , thomas knocke2 , richard ptter1 , barbara bachtiary1 purpose : to retrospectively assess the incidence of radiation dermatitis in patients with locally advanced squamous cell carcinoma of the head and neck ( scchn ) who received primary radiotherapy in combination with cetuximab in a curative intent . 
 patients and methods : a total of 112 consecutively treated patients who received cetuximab in combination with radiotherapy at the departments of radiotherapy at the medical university in vienna and the hospital hietzing ( vienna ) were analyzed . 
the incidence of dermatitis and mucositis within the radiation portals in 103 eligible patients was compared with a historical control group treated at the medical university of vienna as well as with published data . results : the incidence of grade 1 / 2 , 3 , and 4 dermatitis was 57% , 29% , and 1% in the radiotherapy plus cetuximab treated collective . 
only one case of grade 4 dermatitis was observed . conclusion : these results do not statistically differ significantly from the incidence reported in the bonner trial and indicate that cetuximab in combination with radiotherapy is well tolerated . 
 key words : head and neck cancer radiotherapy cetuximab dermatitis mucositis strahlenther onkol 2011 ; 187 : 3737 doi 10.1007 / s00066 - 011 - 2217 - 7 inzidenz von dermatitis bei patienten mit tumoren der kopf - hals - region unter einer primren strahlentherapie in kombination mit cetuximab ziel : retrospektive prfung der inzidenz der strahlendermatitis bei patienten mit lokal fortgeschrittenen nicht - resektablen tumoren der kopf - hals - region , die eine primre radiotherapie in kombination mit cetuximab in kurativer intention erhielten . 
 patienten und methodik : insgesamt wurden 112 konsekutiv behandelte patienten analysiert , die cetuximab in kombination mit radiotherapie an den abteilungen fr strahlentherapie der medizinischen universitt wien und des krankenhauses hietzing ( wien ) erhielten . 
die strahlentherapie bestand entweder aus einer konventionellen radiotherapie ( 70 gy in 7 wochen ) oder aus einem konkomitanten boost - protokoll ( 72 gy in 6 wochen )  . 
die inzidenz an dermatitis und mukositis innerhalb der bestrahlungsfelder wurde von 103 auswertbaren patienten ermittelt und mit einer historischen kontrollgruppe der medizinischen universitt wien wie auch mit publizierten daten verglichen . 
 ergebnisse : die inzidenz von grad - 1 / 2 - , - 3und - 4 - dermatitis betrug jeweils 57% , 29% und 1% in der radiotherapie - plus cetuximab - gruppe . 
 schlussfolgerung : die ergebnisse unterscheiden sich in statistischer weise nicht signifikant von der in der bonner - studie publizierten inzidenz und weisen darauf hin , dass cetuximab in kombination mit bestrahlung gut vertragen wird schlsselwrter : kopfund halstumoren radiotherapie cetuximab dermatitis mukositis 1department of radiotherapy , medical university of vienna , vienna , austria , 2department of radiotherapy , hospital hietzing , vienna , austria , 3department of internal medicine i , medical university of vienna , vienna , austria . received : august 26 , 2010 ; accepted : february 4 , 2011 published online : may 16 , 2011 strahlenther onkol 2011 urban & vogel selzer e , et al . 
incidence of dermatitis in h&n cancer patients receiving rt and cetuximab introduction the cornerstones of treatment for patients with locally advanced unresectable head and neck cancer are surgery and radiotherapy , which might be delivered alone or in various combinations with chemotherapy [ 1 , 6 , 12 , 16 , 20 , 22 , 24 , 26 ]  . 
with the recent introduction of cetuximab in the treatment of locally advanced non resectable head and neck cancer , an attractive novel therapeutic option has been provided to the head and neck oncologist , with potentially the same efficacy , but less side effects than observed during radiochemotherapy [ 4 , 9 , 10 ]  . 
the efficacy and tolerability of cetuximab has been demonstrated in several studies , one of the most widely cited being the landmark phase iii study reported by bonner et al . 
this study compared radiotherapy alone with radiotherapy plus cetuximab and showed excellent results regarding the median duration of locoregional control and the median duration of overall survival in the group of patients that received cetuximab . 
however , recently , several groups reported retrospective data and case studies suggesting that the combination of radiotherapy with cetuximab might lead to a potentially higher incidence of severe radiation dermatitis compared to the data published by bonner et al . 
for example , the results of one survey conducted in several eortc institutions [ 15 ] showed a strikingly high frequency of grade 3 / 4 radiation dermatitis in up to 49% of locally advanced squamous cell carcinoma of the head and neck ( scchn ) patients treated with cetuximab and concurrent radiotherapy , being significantly higher compared to the data presented in the previously mentioned bonner trial . 
in order to provide further data which might help to clarify this controversial issue , we retrospectively evaluated the incidence and grade of skin and other reactions , such as mucositis , for a collective of consecutively treated head and neck cancer patients who received primary radiotherapy in combination with cetuximab . 
 methods and materials patients a total of 112 patients with scchn were treated with cetuximab in combination with radiotherapy in a curative intent at the department of radiotherapy at the medical university of vienna and at the hospital hietzing in vienna between march 2006 and september 2009 . 
the concomitant boost protocol [ 14 ] in combination with cisplatin is regarded as the standard treatment for locally advanced stage iii / iv head and neck cancer at our institution . 
conventional radiotherapy is reserved as the primary treatment option for lower stage i / ii cancer , or for patients who are believed to be unfit to tolerate an intensified radiotherapy protocol . 
our historical control group consisted of 131 consecutively ( january 2001 to december 2004 ) treated patients ( concomitant boost radiotherapy ) with locally advanced inoperable head and neck cancer ( 5% stage iii and 93% stage iv )  . 
of the 131 patients from the historical control group , 72 received low dose cisplatin daily ( 6 mg / m2 ) during the first 20 treatment days plus mitoymcin c given as bolus injection ( 12 mg / m2 ) on day 21 of the treatment . radiotherapy a total of 112 patients were treated in a curative intent by conventional radiotherapy ( 35 fractions at 2.0 gy ) or the concomitant boost protocol ( 72 gy / 42 fractions ) plus concurrent cetuximab . 
reasons for receiving less than four cycles were systemic infusion reactions ( n = 6 ) , death due to sepsis ( 1 case ) , pneumonia ( 1 case ) , and lack of compliance ( 1 case )  . 
the total dose delivered was 70 gy / 72 gy to sites of gross disease and 50 gy / 54 gy to adjacent lymphatic drainage regions at risk for subclinical metastasis . 
 cetuximab the administration of intravenous cetuximab was initiated 1 week before start of radiotherapy at a loading dose of 400 mg / m2 of body surface area over a period of 120 minutes , followed by 60 minutes infusions of 250 mg / m2 for the duration of radiotherapy ( one infusion per week )  . 
dose modification options for grade 3 skin toxicity included a 1 - week delay , with dose reductions in increments of 50 mg / m2 ( minimum cetuximab dose 150 mg / m2 )  . 
 clinical evaluation and follow - up the entire group of patients receiving cetuximab and radiotherapy were monitored weekly regarding the following criteria : skin reactions in the radiation field and outside the radiation portals , allergic reaction , and mucositis . 
it should be mentioned in this context that the treatment of cetuximab - induced skin reactions has been continuously evolving over the past few years , especially with respect to the introduction of local as well as systemic antibiotics [ 7 ]  . number of patients patients medical university patients hospital hietzing age ( median [ range ] ) primary tumor site results ajcc stage from march 2006 until september 2009 , 112 patients were treated with a combination of radiotherapy and cetuximab at the departments of radiotherapy at the medical university of vienna and the hospital hietzing vienna . 
since the determination of the occurrence of dermatitis was the primary aim of this work , only patients who received at least four infusions of cetuximab were included in the final analysis . 
a comparison of the incidence of side effects of a historical control group of patients not receiving cetuximab treated at the medical university of vienna with the patients analyzed in the current study is shown in table 5 . 
these results were compared with a historical control group of patients treated at the department of radiotherapy at the medical university vienna , as well as with published reports from the literature . 
this percentage was higher compared to the incidence in both the historical control group without chemotherapy ( 44% ) as well as the radiotherapy plus cetuximab group ( 47% )  . 
inzidenz von mukositis ( grad 14 ) fr patienten die mit einem konkomitanten boost - protokoll ( n = 53 ; a ) oder mit konventioneller bestrahlung ( n = 50 , b ) behandelt wurden whrend der ersten 5 wochen der behandlung sowie fr die jeweils letzte woche der bestrahlung . end of therapy week total grade 1 grade 2 grade 3 grade 4 total grade 1 grade 2 grade 3 grade 4 48% 75% 27% 29% 17% 40% 4% 6% 0% 0% 34% 82% 18% 22% 12% 42% 4% 18% 0% 0% 91% 88% 89% 11% 6% 4% 55% 38% 29% 25% 44% 48% 0% 0% 8% 96% 88% 88% 24% 22% 14% 48% 32% 28% 24% 32% 46% 0% 2% 0% the incidence of grade 3 dermatitis in the historical treatment groups with or without chemotherapy was 31% and 20% , respectively , compared to 29% in the radiotherapy plus cetuximab group . 
inzidenz von dermatitis ( grad 14 ) fr patienten die mit einem konkomitanten boost - protokoll ( n = 53 ; a ) oder mit konventioneller bestrahlung ( n = 50 ; b ) behandelt wurden whrend der ersten 5 wochen der behandlung sowie fr die jeweils letzte woche der bestrahlung . end of therapy week total grade 1 grade 2 grade 3 grade 4 total grade 1 grade 2 grade 3 grade 4 2% 0% 0% 0% 0% 0% 50% 71% 38% 42% 10% 21% 2% 8% 0% 0% 0% 2% 0% 78% 86% 42% 34% 26% 32% 10% 16% 4% 0% 0% 2% table 4 . 
alle evaluierten unerwnschten ereignisse dargestellt nach schweregrad ( n = 103 ; ahk + hietzing )  . acne infusion reaction mucositis dermatitis nails grade 1 0% 9% 3% grade 2 5% 0% grade 3 9% 4% 0% grade 4 table 5 . 
historical control data were obtained by analysis of patients treated ( concomitant boost protocol ) at the department of radiotherapy at the medical university of vienna between 2001 and 2004 without cetuximab . 
die historischen kontrolldaten wurden durch auswertung von patienten ( konkomitanter boost ) erhalten , die an der abteilung fr strahlentherapie der medizinischen universitt wien zwischen 2001 und 2004 ohne cetuximab behandelt wurden . 
taken together , our data are in good agreement with the findings published in the bonner ( nct00004227 ) trial . however , and in obvious contrast to these data , several recently published reports relying on a rather heterogeneous collective of retrospectively analyzed patients suggested that there may be a significantly higher rate of radiation dermatitis if cetuximab was given concomitantly with radiotherapy . 
 [ 15 ] demonstrated the occurrence of up to 21% grade 3 dermatitis and a very high incidence of 28% grade 4 skin reactions in 125 head and neck cancer patients who were treated with a combination of radiotherapy and cetuximab . 
we assume that discrepancies in institutional experiences regarding the incidence of severe side effects may be explained , at least in part , by differences in skin care and the diversity of topical or systemic applications of protective medications . 
however , it should also be noted that cross - study comparisons should be interpreted with caution as the majority of the published data are retrospective in nature and different toxicity scales were used . 
in order to provide a definitive answer , prospective studies comparing the efficacy and toxicity of radiotherapy in combination with chemotherapy or cetuximab would be necessary . one major question is to what extent cetuximab might be able to serve as an alternative for the addition of cisplatin to radiation , a protocol which definitively increases the rate of mucositis . 
the survival benefit conferred either by a combination of radiotherapy with chemotherapy or with a cetuximab / radiotherapy regimen appears to be very similar for both compounds , lying between 8% and 10% [ 9 , 10 , 12 , 22 ]  . 
apart from differences in the pattern of local toxicity of combined radiochemoand radiotherapy plus cetuximab , cisplatin and cetuximab show also a different toxicity profile concerning systemic side effects which is an important fact to consider when treating head and neck cancer patients who often suffer from various comorbidities . 
preliminary results of a randomized phase ii ( tremplin ) study comparing tpf induction chemotherapy followed by radiotherapy plus cisplatin or cetuximab for locally advanced laryngeal or hypopharyngeal cancer indicate that cetuximab is less toxic than cisplatin when combined with radiotherapy [ 18 ]  . 
in addition , cetuximab also seems to be well tolerated in the re - irradiation setting [ 3 ]  . conclusion in conclusion , our data as well as publications representing the majority of analyzed patients in the literature indicate that cetuximab in combination with radiotherapy is well tolerated . 
most importantly , grade 4 skin reactions were very rare , thus , demonstrating that cetuximab containing protocols may be safely administered in combination with radiotherapy for the treatment of head and neck cancer patients . original article advantage of robotic needle placement on a prostate model in hdr brachytherapy gerd stramann1 , peter olbert3 , axel hegele3 , detlev richter2 , emmanouil fokas1 , nina timmesfeld4 , rainer hofmann3 , rita engenhart - cabillic1 purpose : to compare the accuracy of the robot - assisted needle positioning with that of the conventional template - guided method with the help of a prostate model in high dose rate ( hdr ) brachytherapy . material and methods : a prostate model of fresh porcine abdomen and special polyvinylchloride ( pvc ) sheets was developed . 
the robot - assisted needle positioning technique improves the degree of freedom by providing additional oblique insertion channels and could be potentially exploited not only for ldr but also for hdr brachytherapy . key words : robot - assisted brachytherapy hdr brachytherapy needle deviations accuracy needle insertion strahlenther onkol 2011 ; 187 : 36772 doi 10.1007 / s00066 - 011 - 2185 - y vorteil der robotergestzten nadelapplikation in der hdr - brachytherapie am prostatamodell fragestellung : ziel der arbeit ist der vergleich der genauigkeit der roboter - assistierten mit der template - gesttzten nadelpositionierung am prostatamodell . material und methode : fr die messung wurde ein prostatamodell aus frischem schweinebauch und speziellen pvc - folien entwickelt . 
zur verifikation des modells wurde die genauigkeit der interstitiellen template - gesttzten nadelpositionierung von 311 nadeln , die im rahmen einer hdr - brachytherapie positioniert wurden , anhand von ultraschallbildern ermittelt . 
danach erfolgte die messung der genauigkeit von jeweils 20 roboter - assistierten nadelpositionierung mit den geschwindigkeiten 2 , 7 / 5 , 4 / 9 , 8 mm / s und 20 template - gesttzten nadelpositionierung am prostatamodell . ergebnisse : die mittlere nadelpositionierungsgenauigkeit der manuellen template - gesttzten nadelapplikation am modell war mit der genauigkeit am realen patienten vergleichbar ( 3mm )  . 
die mittlere nadelpositionierungsgenauigkeit der robotergesttzten methode am prostatamodell war mit 1 , 80 , 6 mm ( geschwindigkeit 2 , 7mm / s ) signifikant besser als die templategesttzte manuelle applikation mit 2.70.7 mbei hheren geschwindigkeiten fr die roboter - gesttzte applikation konnte kein unterschied in der positionierungsgenauigkeit im vergleich zu der manuellen methode nachgewiesen werden . 
 schlufolgerungen : die von uns durchgefhrte studie zeigt erstmals einen signifikanten vorteil der roboter - gesttzten nadelapplikation bei einer geschwindigkeit von 2 , 7mm / s gegenber der konventionellen methode am prostatamodell . 
 schlsselwrter : roboter - assistierte brachytherapie hdr - brachytherapie nadelpositionierungsgenauigkeit 1university of marburg , department of radiotherapy and radiation oncology , marburg , germany , 2hochschule rheinmain , university of applied science , department of informatics , wiesbaden , germany , 3university of marburg , department of urology , marburg , germany , 4university of marburg , department of medical biometry and epidemiology , marburg , germany . received : june 21 , 2010 ; accepted : february 23 , 2011 published online : may 17 , 2011 strahlenther onkol 2011 no . 
robotic needle placement on a prostate model in hdr brachytherapy introduction the combination of external beam radiotherapy ( ebrt ) with high dose rate ( hdr ) brachytherapy boost has become a common treatment approach for prostate cancer patients in t13 , n0 , and m0 stages . 
brachytherapy allows for high - dose delivery within the prostate with sharp dose fall - off to the surrounding structures and sparing of the rectum and urinary bladder [ 9 ]  . 
 different fractionation regimens ( 24 fractions ) , target volumes ( tumor volume , prostate capsule , peripheral zone ) , and doses ( 315 gy per fraction ) have been previously described [ 3 , 11 , 14 , 15 ]  . 
 with an average trus positioning accuracy of 3 mm and a template grid resolution of 5 mm , an 8 - mm positioning gap can occur , theoretically , where no needle can be placed . 
 since the quality of the implant correlates directly with the precision of needle positioning and the accuracy of target volume definition , additional deviations in needle positioning occur leading to dose failures in areas of the target volume [ 8 , 10 , 21 ]  . 
 from a clinical point of view , patients with pubic arch interference can be treated with oblique needles and decrease toxicity by avoiding the critical structures near the penile bulb , while still fulfilling the radiotherapy oncology group ( rtog ) criteria [ 5 ]  . the described positioning gap and the impairment of correct needle placement induced by the pubic bone prompt the application of a robot - based solution which matches the needle geometry to the prostate volume and enables positioning of needles with all degrees of freedotherefore , we developed a prostate model to investigate the applicability of a robot - assisted system for hdr brachytherapy to potentially improve needle placement . 
the purpose of this study was to compare the accuracy of the robot - assisted needle positioning with that of the manual template - guided method based on the prostate model . 
 materials and methods to confirm the clinical relevance of our model and because of the limited information available regarding needle position accuracy in hdr brachytherapy , we initially investigated our patient data with respect to the needle positioning accuracies . 
 experiment 1 : accuracy of manual template - guided needle positioning the needle positioning accuracy for the manual templatebased and ultrasound - guided procedure for interstitial hdr brachytherapy implants of prostate cancer at our institution were investigated . 
for that purpose , the average spatial deviation in the xy plane of the needle tip from the center of the corresponding template hole was determined on the ultrasound image set acquired ; there were 11 implants ( 11 patients ) , based on a total of 322 needles . 
 especially important for the investigation were the following : utilization of fresh porcine abdomen for simulation of human skin resistance , subcutaneous tissue , muscle analogous to the figure 1 . 
the skin of the porcine abdomen corresponds to the thickness and the rigidity of human skin , while the fat and muscular layers lying underneath represent the subcutaneous adipose tissue and pelvic floor musculature , respectively . 
subsequently , the needle was inserted via robot - assistance without using a template , and the needle positioning deviation was measured in exactly the same manner as for the manual procedure . 
the experiments with the robot were performed using three different velocities ( velocity 1 = 2.7 mm / s ; velocity 2 = 5.4 mm / s ; velocity 3 = 9.8 mm / s )  . 
the construction of the model used to calculate the accuracy of positioning using the template - guided hand - free needle placement , as performed in interstitial brachytherapy of the prostate is shown ( left )  . 
therefore , oblique needle trajectories could follow the prostate contour from the apex to the reference scan to solve pubic bone limitations and to protect normal tissue , e.g. , neurovascular bundle ( figure 4 )  . second , the anterior rectal wall in the longitudinal ultrasound axis is mostly higher than the caudal portion of prostate . 
this method results in significantly higher displacement of the needles ( p = 0.043 ) when compared to the manual template - based method . discussion principally , hdr brachytherapy ( 192ir ) is performed using a template - guided parallel needle pattern with a uniform needle tip sharpened on three sides , while ldr brachytherapy with permanent implants ( 125i , 103pd ) is applied with a oblique needle tip sharpened only on one side for ultrasound - guided insertion of slightly curved trajectories to meet the pre - planned points between the template grid [ 4 , 17 , 23 , 27 ]  . 
although several robotic systems have been developed for automatic needle insertion in ldr brachytherapy [ 7 , 18 , 24 , 26 ] and preliminary clinical results are outstanding , no system has been developed for hdr brachytherapy . the first studies of robot - assisted puncture in brachytherapy were conducted by okamura et al . 
 finally , to the best of our knowledge , no study has been undertaken to demonstrate the benefit of the robot - assisted technique compared to the conventional method in hdr brachytherapy . 
first , hdr brachytherapy is used for the treatment of advanced localized prostate cancer , where the possibility of interference with the needle positioning , induced by the pubic bone , is from our own figure 5 . 
roboter - gesttzte positionierung mit unterschiedlichen geschwindigkeiten ( spalte 24 ) ; sd : standardabweichung . template - based ( conventional ) positioning the rectal wall to the anterior prostate region is necessary . 
 therefore , it is obvious that additional flexibility of needle positioning can be used to prevent dose inhomogenities , especially over dosage in the peripheral regions , if incorrect needle positions have to be compensated . a prerequisite of the robotic hdr brachytherapy system is that for the complete implant , usually 1020 needles has to be inserted before irradiation . 
in order to ensure the quality and validity of our model , we first tested this method by investigating the precision of needle positioning in our patients , in comparison to the model accuracy . 
the average needle positioning accuracy , as determined by our prostate model , closely resembled those of real patients ( approximately 3 mm ) and indicates that the designated model can successfully reproduce real patient conditions . 
finally , a muscular layer is located under this , which corresponds to the pelvic floor musculature ; a special pvc sheet represents the prostate capsule . we have demonstrated that the robot - assisted needle placement at a velocity of 2.7 mm / s is significantly more precise than the manual template - based method . 
 therefore , our data cannot be compared with those of fichtinger et al . , although both revealed high accuracy for the robotic syste because of the excellent accuracy described in this study , smaller needle diameters of 1.31.5 mm should also be used in robotic hdr brachytherapy . previous studies have shown that increasing needle inserbut in prac [ 2 , 13 ] but in praction velocity decreases the positioning error [ 2 , 13 ] but in pracstrahlenther onkol 2011 no . 
thus , the needle positioning forces at the distal end of the needle were measured and the highest lateral forces at the skin with increasing velocity ( unpublished data ) were registered . 
the latter prompts the application of higher force and , together with skin resistance , increase the risk of needle deflection from the preplanned trajectory . conclusion the robot - assisted needle positioning technique presented in this study is an efficient and feasible method to optimize hdr brachytherapy of the prostate . 
future in vivo studies should further exploit the beneficial role of robotic needle placement in hdr brachytherapy . original article interobserver variability of clinical target volume delineation in supra - diaphragmatic hodgkins disease a multi - institutional experience domenico genovesi1 , giampiero ausili cfaro1 , annamaria vinciguerra1 , antonietta augurio1 , monica di tommaso1 , rita marchese1 , umberto ricardi2 , andrea riccardo filippi2 , theodore girinsky3 , katiuscia di biagio4 , maurizio belfiglio4 , enza barbieri5 , vincenzo valentini6 background : to determine interobserver variability in clinical target volume ( ctv ) of supra - diaphragmatic hodgkins lymphoma . materials and methods : at the 2008 airo ( italian society of radiation oncology ) meeting , the radiation oncology department of chieti proposed a multi - institutional contouring dummy - run of two cases of early stage supra - diaphragmatic hodgkins lymphoma after chemotherapy . 
to quantify interobserver variability of ctv delineations , the total volume , craniocaudal , laterolateral , and anteroposterior diameters were calculated . results : a total of 18 institutions for case a and 15 institutions for case b submitted the targets . 
treffen der airo ( italienischen gesellschaft fr radioonkologie ) in mailand ( november 2008 ) schlug die abteilung fr strahlentherapie / radioonkologie von chieti eine multiinstitutionelle zielvolumen - konturierung ( dummyrun ) von zwei fllen supradiaphragmatischer hodgkin - lymphome im frhen stadium nach der chemotherapie vor . 
um die inter - beobachter - variabilitt bei der konturierung des klinischen zielvolumens zu quantifizieren , wurden das gesamtvolumen ( cc ) , die kraniokaudalen , laterolateralen und die anteroposterioren durchmesser ( cm ) berechnet . 1department of radiation oncology , g . 
annunziata hospital , chieti , italy , 2department of medical and surgical sciences , radiation oncology unit , university of turin , turin , italy , 3department of radiation oncology , institute gustave roussy , villejuif , france , 4department of clinical pharmacology and epidemiology , consorzio mario negri sud , s . 
gemelli , catholic university , rome , italy . received : september 14 , 2010 ; accepted : january 24 , 2011 published online : may 16 , 2011 strahlenther onkol 2011 no . 
diese variationen wurden bei der messung der kraniokaudalen ( durchschnittlich 16 , 25 cm ; range 6 , 522 , 5 cm ) ( abbildung 2 ) , anteroposterioren ( durchschnittlich 10 , 28 cm ; range 5 , 0414 , 82 cm ) ( abbildung 3 ) und laterolateralen durchmesser ( durchschnittlich 15 , 5 cm ; range 8 , 2322 , 88 cm ) ( abbildung 4 ) besttigt ( tabelle 1 )  . 
 der range der volumendefinition im fall b reichte von 341 , 8 bis zu 1662 cc ( abbildung 1 ) ; und diese variationen wurden bei der messung der kraniokaudalen ( durchschnittlich 23 cm ; range 8 , 028 , 5 cm ) ( abbildung 5 ) , anteroposterioren ( durchschnittlich 11 , 1 cm ; range 7 , 914 , 8 cm ) ( abbildung 6 ) und laterolateralen durchmesser ( durchschnittlich 18 , 8 cm ; range 12 , 924 , 0 cm ) ( abbildung 7 ) besttigt ( tabelle 2 )  . 
 schlussfolgerung : diese signifikante variabilitt besttigt die notwendigkeit der anwendung von spezifischen guidelines , um die uniformitt der konturierung bei hodgkin - lymphomen zu verbessern . schlsselwrter : hodgkin - lymphom konformale radiotherapie konturierung des klinischen zielvolumens inter - beobachter - variationen qualittssicherung introduction hodgkins lymphoma ( hl ) has an incidence of 23 / 100 , 000 per year in the us , europe , and italy [ 1 , 5 , 11 ]  . 
 radiation therapy has evolved from extended - field radiation therapy ( efrt ) to involved - field radiation therapy ( ifrt ) , reducing toxicity while maintaining high cure rates . standard of care for patients with early stage hodgkins lymphoma is currently represented by a combination of a brief chemotherapy ( 23 or 34 abvd or abvd - like cycles , respectively in favorable or unfavorable disease ) followed by 3036 gy ifrt [ 1113 , 2124 , 32 , 34 , 35 ]  . ongoing clinical research is currently evaluating a further reduction of radiation doses and volumes , towards the new concept of involved nodes radiation therapy ( inrt ) , adopted in eort - gela - iil h10 trial , which is still recruiting [ 2 , 6 , 8 , 10 , 18 , 19 , 30 , 36 , 43 ]  . when treating patients with standard ifrt , accurate identification of the involved lymphatic regions at diagnosis and post - chemotherapy is crucial for correct target volumes delineation . 
several studies have shown that radiologists differ in their interpretation of computed tomography ( ct ) images when determining mediastinal lymph node status in patients with lung cancer [ 4 , 7 , 20 ] ; in hl , a study designed to test the extent of variation among expert radiologists detection of cervicalthoracic disease by ct showed a variability that may affect patient care [ 16 ]  . yahalom and mauch [ 49 ] , reporting a survey performed among lymphoma radiotherapy experts for the fifth international symposium on hodgkins lymphoma in cologne , germany ( september 2001 ) and aiming to evaluate dose and fields prescribed by the experts in different clinical scenarios , demonstrated a wide heterogeneity in target volume delineation and dose prescription emphasizing the need for an international consensus . moreover , also well known as interobserver variability in the delineation of gross tumor volume ( gtv ) , clinical target volume ( ctv ) , and planning target volume ( ptv ) is a problem in modern radiotherapy treatment planning [ 29 , 31 , 37 , 39 , 40 , 42 , 4648 ]  . this study reports the results of a multi - institutional dummy - run study designed to estimate the consistency of interobserver variability in clinical target volume delineation in hodgkins disease . 
the planning ct scan was obtained with a standard acquisition protocol ( supine position ; free breathing ; slice thickness of 5 mm , and reconstruction interval of 5 mm )  . the purpose of this work was to quantify interobserver variability in routine clinical practice and participants were instructed to delineate target volumes employing their own segmenting tools without specific instructions about technical aspects such as image resolution or window / level setting . 
interobserver variability in hodgkins lymphoma radiotherapy minimum and maximum observation , mean value , standard deviation , median , 2575th percentiles and variations coefficient were calculated for each variable ( volume , craniocaudal , laterolateral , and anteroposterior diameters )  . 
however , because the volumes distribution is a nonnegative normal random variable and tends to be skewed to the right , the 95% twoclinical target volume moreover , we compared between each observer cranial limits of the ctvs delineated ( defined as the most cranial slice where the contour was inserted ) , caudal limits of the ctvs ( defined as the most caudal slice where the contour was inserted ) , maximum anteroposterior diameter ( extended from the extreme anterior point to the extreme posterior point of the ctvs delineated ) , and maximum laterolateral diameter ( extended from the extreme point on the right to the extreme point on the left of the ctvs delineated )  . 
the results were presented at the annual meeting meet the experts on tumors of hematopoietic and lymphoid tissues which was held in chieti on february 1920 , 2009 . clinical cases presentation case a was a 30 - year - old man with stage iia favorable right cervical , supraclavicular , and mediastinal classical hodgkins lymphoma ( nodular sclerosing subtype according to the updated who classification ) [ 41 ]  . 
the patient received two cycles of adriamycin , bleomycin , vinblastine , and dacarbazine ( abvd ) ; 18fdg pet - ct evaluation after chemotherapy was negative , with a reduction of 50% of the merged lymphadenopathy on the ct scan . 
the clinical target volume to be delineated was an involved field according yahalom and mauch [ 49 ] including mediastinal lymph nodes , right cervical , and supraclavicular lymph nodes . 
disease sites involved at diagnosis included the following : bilateral cervical and supraclavicular , paratracheal , parasternal , anterior mediastinal , and right paravertebral with a maximum diameter of 11 cm at ct . 
the clinical target volume to be delineated was an involved field according yahalom and mauch [ 49 ] including mediastinal lymph nodes , and bilateral cervical and supraclavicular lymph nodes . 
interobserver variability in hodgkins lymphoma radiotherapy sided confidence limit for an individual predicted volume and the coefficient of variation ( expressed as a percentage , cv% ) were based on the left - truncated normal distribution , where the fixed - point of truncation was zero [ 3 , 27 ]  . using noncentral - t distribution , the 95% two - sided confidence interval for cv% was then estimated [ 28 ]  . 
to compare relative variability across craniocaudal , laterolateral , and anteroposterior diameter distributions , for each case , the likelihood ratio test ( lrt ) for the equality of cv , against the alternative that there is at least one difference , was performed [ 17 ]  . results case a observers figure 2 . 
particularly , 9 of 18 centers contoured a ctv within a volume of 50% , 5 of 18 centers with volume 223.2 cc ( 25th percentile ) , and 4 / 18 centers with volume 637.9 cc ( 75th percentile )  . 
the estimated cv% and 95% confidence interval were 51% and 3687% , respectively . figures 2 , 3 , and 4 show , respectively , the variability of cranial and caucranial and caudal limits , of maximum anteroposterior diameter , and of maximum laterolateral diameter drawn by each observer on ct slices . 
variabilitt des laterolateralen maximaldurchmessers bei den von jedem beobachter definierten ctvs ( fall a )  . no significant departure from normality was found ( p value = 0.3410 ) and no outliers were detected . 
in this case , the result showed a significant disparity between centers : the 50% of measured volume of ctvs was between 464.5 and 1 , 264.7 cc with a median value of 886 cc . 
particularly , 7 of 15 centers contoured a ctv within a volume of 50% , 4 of 15 centers with volume 464.5 cc ( 25th percentile ) , and 4 of 15 centers with volume 1 , 264.7 cc ( 75th percentile )  . 
main variations in diameters were observed in the craniocaudal and laterolateral directions , while anteroposterior diameters were similar ( even if no statistically sigo statistically significant difference was found )  . 
a graphic representation of interobserver variation in delineation of case b is shown on a coronal plane in figure 9 . because the average size of ctvs in both cases were considerably different , their standard deviations cannot be compared to establish which distribution has greater dispersion . 
consequently , it was not possible to determine whether differences in the ctvs are greater in case a , where the pre - chemotherapy disease was more limited and there was a reduction of 50% after chemotherapy , or in case b , having more extensive disease in complete remission after chemotherapy . moreover , several variations were also observed for both cases in craniocaudal limits . 
another possible explanation is that the contouring variability could have been related to the different experience between participating centers in clinical practice of conformal radiotherapy for hl . the lack of uniformity could be determined by two factors : the variable identification of the lymph nodes gross tumor volume ( gtv / nodal ) and the variable delineation of lymph nodal areas surrounding bulky disease to generate the ctv . 
moreover , the complete response obtained in case b could make the delineation of gtv / nodal more difficult . interobserver variability in ctv delineation may reflect a diverging evaluation of exact localization of lymph node area . 
 several studies have shown that radiologists differ in their evaluation of ct images used to determine the mediastinal lymph node status of patients with lung cancer [ 4 , 7 , 20 ]  . 
interobserver variability in hodgkins lymphoma radiotherapy fletcher and coworkers [ 16 ] found that expert radiologists did not completely agree in their interpretation of cervicalthoracic ct images of hl and the authors list the potential disease sites at risk of misinterpretation . 
 yahalom and mauch [ 49 ] argued that the lack of uniformity could be due to the fact that involved field terminology is quite confusing and even the simple term of involved field has a variety of interpretations and non - uniform definitions . 
they report a survey conducted among lymphoma radiotherapy experts for the fifth international symposium on hodgkins lymphoma in cologne , germany ( september 2001 ) designed to examine dose and fields prescribed by the experts in different clinical scenarios . 
 the study demonstrated a wide heterogeneity in outlining the field borders and dose prescription emphasizing the need for an international consensus [ 49 ]  . results of reported experience seem to be confirmed by our study . 
variabilitt des laterolateralen maximaldurchmessers bei den von jedem beobachter definierten ctvs ( fall b )  . gested three steps in order to achieve a high degree of accuracy in identifying initially involved nodes : ( 1 ) fdg - pet scans should be carefully analyzed to detect involved lymph nodes that were overlooked on ct imaging ; ( 2 ) any morphological and / or functional asymmetry should be sought on ct and fdg - pet scans ; and ( 3 ) any decrease in size or the disappearance of lymph nodes that were initially visible should also be sought on the pre - chemotherapy ct scan compared to the post - chemotherapy ct scan . although these recommendations were developed in the context of a perspective clinical trial introducing the concept of inrt technique ( see h10 eortc - gela - iil trial ) , and not yet validated in clinical practice , they could be useful to achieve a better contouring uniformity in involved field radiotherapy technique ( ifrt )  . 
fall b : graphische darstellung der erfolgten inter - beobachter - variation von 15 untersuchungszentren im gleichen koronalschnitt . conclusion this experience highlights interobserver ctv variability in supra - diaphragmatic hl and the need to apply specific guidelines and educational training in order to improve contouring uniformity . 
moreover , with the aim of determining which sources of variability contributed the most to the overall observed variations and to obtain a correct determination of measurement accuracy , a repeatability analysis should be performed . acknowledgments we thank all the italian physicians of the ctvs delineation collaborative group mentioned hereafter for contributing to ctv delineation for this study : santa bambace , presidio ospedaliero r . 
dimiccoli , barletta ; salvina barra , istituto nazionale per la ricerca sul cancro , genova ; marco bertocchi , presidio unico ospedaliero , sanremo ; massimo cardinali , ospedali riuniti umberto i g.m. 
antonio e biagio , alessandria ; vincenzo fusco , centro di riferimento oncologico regionale , rionero in vulture ; gianstefano gardani , azienda ospedaliera san gerardo , monza ; mara griseri , ospedale ca foncello , treviso ; grazia lazzari , presidio ospedaliero s . 
maria , terni ; renzo mazzarotto , istituto oncologico veneto i.r.c.c.s. , padova ; maria alessandra mirri , ospedale san filippo neri , roma ; piera navarria , istituto clinico humanitas , rozzano ; marianna nuzzo , universit g . 
 current discussion effectiveness of postoperative radiotherapy in patients with small oral and oropharyngeal squamous cell carcinoma and concomitant ipsilateral singular cervical lymph node metastasis ( pn1 ) a meta - analysis maximilian moergel1 , philipp meurer1 , katharina ingel2 , thomas g . 
the present work investigated whether a meta - analysis of current data is able to evaluate the effectiveness of postoperative radiotherapy ( port ) in patients with small oscc ( pt1 , pt2 ) and a single ipsilateral lymph node metastasis ( pn1 )  . methods : the meta - analysis comprises randomized and non - randomized studies . 
high - risk tumors were excluded and defined by size pt3 / pt4 , lymph node involvement pn2 , or presence of additional histological risk factors , e.g. , involved positive resection margins , extra nodal spread of the disease , or lymphangiosis carcinomatosa . 
in contrast , a forest plot presentation of two of seven studies with and without events in the control and therapy arms presented an advantage for the irradiation group with the limitation of large heterogeneity and a lack of statistical significance . conclusion : present data are poor and exhibit limited internal and external validity ; thus , direct comparison was not possible with the eligible studies . 
therefore , a meta - analysis of present data may not serve as the basis for a general treatment recommendation but underlines the need of prospective , randomized , controlled clinical trials . key words : pn1 head and neck cancer radiation prognosis meta - analysis strahlenther onkol 2011 ; 187 : 33743 doi 10.1007 / s00066 - 011 - 2206 - x wirksamkeit der postoperativen strahlentherapie bei patienten mit kleinem oralen und oropharyngealen plattenepithelkarzinom und solitrer , ipsilateraler zervikaler lymphknotenmetastase ( pn1 )  . 
die vorliegende arbeit berprft , ob eine meta - analyse publizierter daten die wirksamkeit der postoperativen strahlentherapie auch bei patienten mit kleinem oralen oder oropharyngealen plattenepithelkarzinom ( pt1 , pt2 ) und gleichzeitiger solitrer lymphknotenmetastase ( pn1 ) bewerten kann . methoden : in die meta - analyse wurden randomisierte und nicht - randomisierte studien eingeschlossen . 
patienten mit hohem risikoprofil wurden primr von der studie ausgeschlossen und sind definiert durch tumorgre pt3 / pt4 , positivem lymphknotenbefall pn2 oder vorhandensein zustzlicher histologischer risikofaktoren , wie z.b. 
demgegenber erbrachte die forest - plot - darstellung von zwei studien , die ereignisse sowohl in kontrollund therapiearm besaen , einen begrenzten vorteil fr die bestrahlungsgruppe , jedoch mit der einschrnkung groer heterogenitt und einem mangel an statistischer signifikanz . 1department of oral and maxillofacial surgery , johannes gutenberg university , medical center , mainz , germany , 2institute of medical biostatistics , epidemiology and informatics ( imbei ) , johannes gutenberg university , medical center , mainz , germany , 3department of radiation oncology , university of jena , medical center , jena , germany . received : january 11 , 2011 ; accepted : march 16 , 2011 published online : may 16 , 2011 strahlenther onkol 2011 no.6 urban & vogel moergel m , et al . 
pn1 state and radiation effectiveness zusammenfassung : es gibt nur wenige publikationen zum thema mit geringer interner und externer validitt , so dass ein direkter vergleich nur eingeschrnkt mglich ist . 
die meta - analyse ist daher derzeit keine geeignete basis fr eine allgemeine behandlungsempfehlung und unterstreicht die notwendigkeit von prospektiv randomisierten klinischen studien . schlsselwrter : pn1 kopf und hals karzinom bestrahlung prognose meta - analyse introduction basic therapeutic strategies for oral and oropharyngeal squamous cell carcinomas ( oscc ) address the tumor and adjacent cervical lymphatic drainage areas . 
in advanced disease , radiotherapy along with surgery and often in combination with chemotherapy supports modern multimodality treatment [ 2 , 3 , 9 , 20 , 26 ]  . 
the decision for or against additional irradiation is predominantly guided by postoperative findings like the tnm / uicc stage , histological evaluation of the resection margins ( r1 / r2 ) , or presence of risk factors [ 16 , 27 ]  . 
interdisciplinary treatment guidelines by the deutsche krebsgesellschaft ( german cancer society ) listed the following tumor characteristics which necessitate postoperative radiotherapy : tumors larger than 4cm in diameter ( pt3 , pt4 ) , extended lymph node involvement ( pn2 ) , positive resection margins , if repetitive surgical intervention presence of extracapsular spread or lymphangiosis carcinois limited , matosa . there are precise irradiation recommendations for advanced stage , extended lymph node involvement , or in case additional histological risk factors exist , whereas irradiation of small tumors with involvement of only a singular lymph node is still optional today [ 13 ]  . taking tumor biology into account , a differentiate treatment of patients with small tumor and singular lymph node metastasis might be feasible . 
thus , the meta - analysis was conducted with the objective to fill an evident gap in present treatment guidelines by evaluation of previously published data . methods literature search articles of potential relevance published in english or german between january 1972 and december 2009 were identified by two independent physicians in medline . 
the complete computer - assisted research strategy and relevant hits are presented in table 1 . study selection and data extraction only randomized controlled trials ( rct ) , non - randomized studies with an interventional group , and retrospective observational studies were of interest . 
all eligible studies were assessed for quality of methodology and relevance to the objective of the review according to the suggestions of the grade working group [ 1 ]  . 
the principle measure of effect is presented as risk ratio . tumor diameter 4 centimeter ( pt1 , pt2 ) presence of ipsilateral lymph node metastasis ( pn1 ) patient underwent curative intended surgery with resection of the primary and neck dissection ( r0 resection status ) results exclusion criteria malignancy other than squamous cell carcinoma oscc > 4 cm or infiltration of surrounding tissue ( pt3 , pt4 ) secondary tumor presence of additional tumor lymph node metastasis > 3cm or contralateral lymph node involvement ( pt2 , pt3 ) identification of distant metastasis ( pm1 ) positive resection margins ( pr1 ) invasion of lymphatic vessel ( ilv ) perineural infiltration ( pni ) extracapsular spread ( ecs ) neoadjuvant chemotherapeutic / irradiation treatment in front of surgery the search strategy allowed 7 publications ( table 3 ) with potential information for the present meta - analysis to be identified . 
op : operation , rt : radiotherapie , loe : evidenz - level . author 1 chen background information year loe design anatomy retrospective tongue 2009 iii n ( total ) n ( survival ) n ( total ) n ( survival ) op + rt quality 2 sessions 2003 iii 3 sessions 2002 iii 4 sessions 2000 iii 5 szabo 1999 ib makkregar 1994 iii 7 kies 1984 iii retrospective base of tongue retrospective oral tongue 5 retrospective prospective retrospective retrospective floor of mouth lingual / sublingual oropharyngeal oral carcinoma total subgroup directly eligible for study no declaration of indication for irradiation in 13% , resection margin questionable tumor free no declaration of indication for irradiation in 10% , resection margin questionable tumor free no declaration of indication for irradiation 11.5% resection margins questionable tumor free no declaration of indication for irradiation no information of resection margins no declaration of indication for irradiation no information of resection margins no declaration of indication for irradiation no information of resection margins no information of additional risk factors strahlenther onkol 2011 no . 
pn1 state and radiation effectiveness studies excluded by abstract information ( n = 1 , 486 ) no breakdown of data by tnm grouping ( n = 115 ) hits ( n = 1 , 709 ) full text ( n = 223 ) potentially appropriate studies to be included in meta - analysis ( n = 108 ) studies withdrawn due to lack of outcome data ( n = 86 ) studies withdrawn by false postoperative intervention compared to operation alone ( o ) vs . 
operation an d postoperative radiation ( o + r ) ; ( n = 9 ) studies withdrawn by language ( n = 1 ) , publication was written in danish ( n = 1 ) studies withdrawn by publication ( n = 5 ) , pubmed listing was other than publication , e.g. , congress abstract ( n = 5 ) risk factors that usually require irradiation treatment , the 5 - year overall survival rate significantly rose to 92.3% for patients with port ( n = 20 ) vs . 
evaluated the treatment success of five different treatment modalities in patients with histological verified squamous cell derived tumors at the base of tongue in 2003 [ 23 ] , the oral tongue in 2002 [ 22 ] , and floor of the mouth in 2000 [ 21 ]  . 
the study population consisted of 262 patients with a primary tumor at the base of tongue and the observational period resulted in a 5 - year follow - up : 204 patients underwent surgery , 21 patients underwent tumor resection and concomitant neck dissection and of these 2 patients exhibited a pt1 / pt2 , pn1 stage . 
finally , 138 patients underwent postoperative irradiation ; 20 of these patients represented a pt1 / t2 , pn1 stage of which 11 patients survived [ 23 ]  . studies fulfilling inclusion criteria ( n = 7 ) figure 1 . 
a summary of the studies is presented in table 2 . meta - analysis of non - randomized observational studies a total of 6 retrospective studies with level of evidence iiib were found with relevant data for the present meta - analysis and summarized as follows [ 7 , 12 , 17 , 2123 ] : in 2009 , chen et al . 
 [ 7 ] retrospectively evaluated the effectiveness of postoperative irradiation treatment ( port ) in patients with small tongue carcinoma ( pt12 ) and singular lymph node metastasis ( pn1 ) and assessed patient records over 22 years ( 19802002 )  . 
 [ 7 ] performed a subgroup analysis with exclusion of patients with ecs , positive resection margins , lymphovascular infiltration ( lvi ) , or perineural infiltration ( pni )  . 
 [ 22 ] is of equal composition and evaluated tumors of the oral tongue compassing 332 patients : 268 patients received surgical therapy , 23 of them as combined tumor resection and neck dissection and 5 patients were diagnosed with pt1 / t2 and pn1 . 
nearly half of the patients ( n = 7 ) survived the observational period . the third study [ 21 ] reported patients with carcinomas localized at the floor of the mouth and included a total of 280 patients ; 235 of these underwent surgery . 
composite resection was performed in 24 patients with 4 patients in pt1 / t2 and pn1 stage , of whom all survived the observational period of 5 years , and 22 patients received postoperative irradiation , of whom 8 survived . a study performed by mak - kregar [ 17 ] investigated the survival rates of patients with carcinoma of the soft palate and the posterior pharyngeal wall treated between 1966 and 1986 . 
another patient with pt1 / t2 and pn1 had to be excluded from analysis , since he underwent definitive radiation therapy without prior operation . the last study published by kies et al . 
 [ 12 ] in 1984 reported the influence of preoperative administration of cisplatin , bleomycin , and methothrexate on the survival rate of patients with advanced head and neck cancer . 
both patients died during the observational period after 19 and 10 months , respectively . survival analysis taking all studies into account , the present analysis implies a slightly higher mortality when postoperative irradiation treatment ( port ) was applied ( 34 deaths ( 44% ) ) vs . 
thus , forest plot presentation and risk analysis were performed as a subgroup analysis of studies with and without events in both treatment arms for the studies by sessions et al . 
however , the test for homogeneity ( p = 0.04 ) and i2 ( 76% ) exhibit heterogeneity between the studies , and the test for overall effect ( p = 0.53 ) characterizes the risk ratio as statistically not significant ( figure 2 )  . 
 discussion despite the high prognostic relevance of lymph node involvement , few studies cover the topic of the pn1 neck in patients with small oscc ( pt1 / pt2 ) without further risk factors . 
a bias due to extrapolation of different outcome parameter , including inaccurate presentation of survival data in principle , is imminent and , therefore , once more limiting a general conclusion . 
unfortunately , most studies exhibit a significant lack of clinical data reporting and description of the operation procedure ( e.g. , handling of midline tumors , extension of neck dissection , or level of lymph node metastasis )  . 
additional clinical inferences between the studies may also contribute to missing data of the applied irradiation protocol , e.g. , radiation source , time delay to irradiation , mode of dose distribution calculation , total dosage , or fractionation scheme . in contrast to the shortcomings listed above , a recent publication focusing on the pn1 neck offered a precise description of relevant clinical data [ 10 ]  . 
another prospective multicenter study with focus on small oral carcinomas of stages pt1 / t2 and pn0 / n1 investigated a population of 93 patients and reported local tumor control in more than 90% of the patients by surgery alone , thus , sparing 77% of patients impairment by radiotherapy [ 29 ]  . 
concluded that surgery alone might be feasible for oscc at stages pt1 / pt2 and pn0 / n1 with employment of salvage surgery and additional radiotherapy in case of locoregional failure . 
altogether , data gathering and evaluation within the framework of the present analysis indicate that irradiation improves local control and survival when advanced tumor state ( pt3 / pt4 ) , nodal disease ( pn2 , pn3 ) , or additional risk factors are present . 
although involvement of the first lymph node is of high prognostic impact , only sparse and contradictory data are available for patients with smaller oscc ( pt1 / pt2 ) when additional risk factors are absent . 
finally , the authors conclude that the obvious limitations of model quality render the present meta - analysis not suitable for generation of a justifiable treatment recommendation and , thus , prospective clinical trials with focus on the topic are necessary . 
these clinical investigations should implement a reliable quality of life assessment along with analysis of survival and locoregional control [ 5 , 11 ]  . conclusion the published clinical data on oscc at stage pt1 / t2 and pn1 without risk factors is rare and of large heterogeneity . 
radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
effectiveness of adjuvant radiotherapy in patients with oropharyngeal and floor of mouth squamous cell carcinoma and concomitant histological verification of singular ipsilateral cervical lymph node metastasis ( pn1 - state ) a prospective multicenter randomized controlled clinical trial using a comprehensive cohort design . 
laryngoscope 2003 ; 113 : 125261 . original article reirradiation of spinal column metastases comparison of several treatment techniques and dosimetric validation for the use of vmat florian stieler , dirk wolff , linda bauer , hans - jrg wertz , frederik wenz , frank lohr1 background : for reirradiation of spinal column metastases , intensity - modulated radiation therapy ( imrt ) reduces the dose to the spinal cord , while allowing longer treatment times . 
we analyzed the potential of volumetric modulated arc therapy ( vmat ) to reduce treatment time and number of monitor units ( mu )  . patients and methods : in ct datasets of 9patients with spinal column metastases , the planned target volume ( ptv ) encompassed the macroscopic tumor including the spinal cord or medullary cone , respectively . 
we compared a posterior ( 3d - pa ) static field technique , a two - field wedge technique ( 3d - wedge ) and 5 - / 7 - beam imrt with vmat . 
conformity index ( ci ) , homogeneity index ( hi40 ) , dose volume histogram ( dvh ) parameters , treatments delivery time ( t ) , and mu were analyzed . 
dosimetry was validated with edr2film / ionization chambers . results : ptv coverage was insufficient for 3d - conformal radiotherapy ( 3d - crt ) when spinal cord tolerance was respected . 
vmat produced dose distributions similar to imrt with shorter treatment times ( vmat : mean 4 : 49min ; imrt : mean 6 : 50min ) and fewer mu ( vmat : 785 ; imrt : 860 )  . 
 - index analysis showed an agreement of 91.333.53% for the 5% / 5mm criteria . conclusion : for this paradigm , vmat produces high quality treatment plans with homogeneity / conformity similar to static imrt , shorter treatment times , and fewer mu . 
verification measurements showed good agreement between calculation and delivered dose , leading to clinical implementation . key words : volumetric intensity modulated arc therapy intensity - modulated radiation therapy 3d conformal radiation therapy spinal column metastases strahlenther onkol 2011 ; 187 : 40615 doi 10.1007 / s00066 - 011 - 2198 - 6 rebestrahlung von paraspinalen metastasen : vergleich verschiedener bestrahlungstechniken und dosimetrische validierung von vmat ziel : die intensittsmodulierte radiotherapie ( imrt ) ermglicht bei der rebestrahlung von wirbelsulenmetastasen eine reduktion der dosis im spinalkanal bei gleichzeitig lngerer bestrahlungszeit im vergleich zur konventionellen 3d - technik . 
wir analysierten das potential der volumetrisch modulierten rotationstherapie ( vmat ) , um die bestrahlungszeit und die anzahl der monitor - einheiten ( mu ) zu reduzieren . patienten und methoden : 9 ct - datenstze von patienten mit wirbelsulenmetastasen wurden untersucht , bei denen das zielvolumen ( zv ) den makroskopischen tumor inklusive spinalkanal umfasste . 
wir verglichen eine posteriore 3d - technik ( 3d - pa ) , eine 2 - feldertechnik mit keilen ( 3d - wedge ) und 5 / 7 - felder - imrt mit vmat . 
die dosimetrie wurde mit edr2 filmen und ionistationskammer berprft . ergebnisse : die zv - abdeckung fr die 3d - techniken war insuffizient , wenn die toleranzdosis des spinalmarks bercksichtigt wurde . 
mit vmat lieen sich hnliche dosisverteilungen wie mit imrt mit krzeren bestrahlungszeiten ( vmat mittel 4 : 49min . , imrt mittel 6 : 50min . ) und weniger mu ( vmat : 785 , imrt : 860 ) realisieren . 
die - analyse zeigte eine bereinstimmung von 91 , 333 , 53% fr 5% / 5mm . 1department of radiation oncology , university medical center mannheim , university heidelberg , germany . received : july 15 , 2010 ; accepted : january 24 , 2011 published online : june 27 , 2011 strahlenther onkol 2011 no . 
reirridiation of spinal metastates : comparison of treatment techniques schlussfolgerung : fr dieses paradigma erzeugt vmat qualitativ hochwertige bestrahlungsplne mit zu imrt vergleichbarer homogenitt / konformitt , krzeren bestrahlungszeiten und weniger mu . 
verifikationsmessungen zeigten gute bereinstimmungen zwischen errechneten und gemessenen dosen und erlaubten die klinische implementierung . schlsselwrter : volumetrisch intensittsmodulierte rotationstherapie intensittsmodulierte radiotherapie 3d konformale radiotherapie wirbelsulenmetastasen introduction spinal column metastases can cause morbidity , including pain and compression of the spinal cord with resulting neurologic deficits and fractures of the vertebral bones . 
 [ 15 ] reported a local control rate of 94.7% after a median followup of 12.3 months for the reirradiation of vertebral bone metastases with stereotactic conformal radiotherapy ( 414 beam directions ) or intensity - modulated radiotherapy ( imrt )  . 
using 3dconformal radiotherapy ( 3d - crt ) without any elements of fluence modulation for retreatment exceeds the radiation tolerance to the spinal cord when target doses of > 30gy are intended [ 18 ]  . 
we , therefore , explored the possibility of establishing volumetric modulated arc therapy ( vmat ) clinically to treat this target paradigseveral earlier studies have shown that vmat may reduce treatment time and primary monitor units ( mu ) for several target types with dose distributions similar to imrt [ 1 , 19 , 21 , 25 , 28 , 29 , 3233 ] , although the benefit is not easy to quantify theoretically , since only preliminary attempts at a comprehensive theory of vmat have been made [ 31 ]  . we report the analysis of different treatment techniques regarding plan quality , treatment efficiency , and dosimetric delivery accuracy of vmat for this target paradigm as evaluated prior to clinical implementation . materials and methods retreatments were planned based on ct datasets of 9patients with spinal column metastases who had previously been treated with 3d - crt to spinal cord tolerance . 
 we chose a prescription dose for the target of 40 gy with a fraction dose of 2 gy , planned for a 6mv synergy linear accelerator ( elekta , uk ) with a maximum dose rate of 600 mu per minute . 
 median dose to the sc was intended not to exceed 26 gy based on available data for retreatment tolerance [ 17 , 30 ]  . two different 3d - crt strategies were assessed in this study : a single posterior ( 3d - pa ) static field ( 180 ) and a two - field wedge technique ( 3d - wedge ) with two beams at angles of around 160 and 200 , respectively , depending on patient anatomy . 
as reference modulated treatment , we created an isotropically distributed 5 - beam imrt ( imrt - 5b ) and an isotropically distributed 7 - beam imrt ( imrt - 7b ) plan , respectively , using the tps hyperion ( university of tbingen , germany )  . 
vmat plans were generated with ergo + + 1.7.2 ( elekta - software , saint louis , mo , usa ) with two complete 360 rotations ( clockwise and counter clockwise ) to increase the modulation depth ( the first rotation focused on the whole ptv excluding the sc , the second focused on the part of the target immediately adjacent to the sc ) and were normalized as described for static imrt plans . for statistical analyses , exact wilcoxon signed - rank tests were used to assess any differences between the treatment paradigms . 
due to the fact that we prescribe dose to the median dose level in the ptv , we had to modify the ci as follows : stieler f , et al . 
reirridiation of spinal metastates : comparison of treatment techniques where vptv describes the target volume in cm and vd99% is the total volume in cm which receives the effective minimal target dose ( dose encompassing 99% of the ptv )  . 
the ci definition is characterized by the effective minimal dose applied to the ptv which follows the idea of the ci definition by the rtog . hi is defined as follows according to the rtog guidelines [ 24 ] : where dpresc is the prescription dose and dmax is the maximum dose in the treatment plan . 
 c95%pd describes the percentage coverage of the ptv by the isodose representing 95% of the prescription dose ( pd ) and scptv is the median dose to the spinal cord inside the ptv . 
for all approaches , ttt was measured on the unit with the same measuring device ( stopwatch ) and under the same circumstances ( first beam on to last beam off )  . to assess dosimetric accuracy , verification measurements were performed using radiographic films and ionization chambers in a homogenous rw3 phantom as described previously [ 7 ] , following the suggestions of rhein et al . 
the imrt approaches as shown in figure 1 show excellent ptv coverage with adequate sparing of the spinal cord , at the expense of a larger non - ptv volume exposed to primary beasimilar to imrt , the vmat approach in figure 1 shows a very good ptv coverage and oar sparing but exposes an even larger volume outside the ptv to primary beam . in table 1 the numeric comparison values of the different approaches are shown . 
 vmat plans ( 785 92 mu ) were delivered with fewer mu than imrt ( imrt - 5b : 843133 ; imrt - 7b : 878102 )  . looking at the treatment time as second efficiency aspect , 3d - pa ( 252 s ) and 3d - wedge ( 887 s ) are , of course , the fastest treatments . 
comparing the modulated techniques the vmat approach is with a mean treatment time of 289 69 s 20% faster than imrt - 5b ( 34872 s ) and 40% faster than imrt - 7b ( 47282 s )  . table 1 also reports the mean percentage coverage of the ptv with 95% of the pd ( c95%pd )  . 
for the 3d approaches , two c95%pd values are reported , one for the plan normalized to 26gy as the median sc dose and the other one normalized to 40gy as the median ptv dose . 
vmat has a slightly larger volume exposed to lower doses ( 525% of prescription dose ( pd ) ) as shown by the dvh for the volume encompassed by the external contour . 
exposure of oars such as lungs , complete sc and sc encompassed by the ptv were similar for the modulated techniques . figure 3 displays the mean dvhs of ptv and spinal cord inside the ptv ( sc ( ptv ) ) with a confidence interval ( cint ) of 95% . 
expectedly , the dvhs for the 3d approaches do not show a large interval range because of the simple beam geometry and the missing modulation which lead to similar results . 
 the cint range for vmat is wider than for the imrt techniques because the forward planning step in ergo + + leads to larger variations among the vmat plans . the differences between the introduced delivery techniques regarding the most relevant comparison parameters are reported with respective significance levels in table 2 . 
the small standard deviations lead to homogeneous results within the delivery techniques and to the majority of differences between techniques being statistically significant despite occasionally small absolute differences . validation of the new treatment paradigm started with assessing the accuracy of plan data transfer from the tps to the r&v syste we found slight variations regarding the strahlenther onkol 2011 no . 
for a - index based on a 5% dose criterion and a 5 mm dta acceptance criterion , 91.333.53% of points were within the acceptance criteria and ( 78.565.34% for 3% / 3mm )  . 
reirridiation of spinal metastates : comparison of treatment techniques discussion the potential benefits of modulated techniques for spinal column tumors were shown in earlier publications [ 5 , 11 , 15 , 22 , 35 ] when spinal cord tolerance was an issue [ 30 ]  . 
mean values standard deviations for homogeneity ( hi40 ) , conformity ( ci ) , number of monitor units ( mu ) , and treatment time ( time ) for the three different techniques . 
reirridiation of spinal metastates : comparison of treatment techniques 3000 2000 1000 3000 2000 1000 100 90 80 70 60 50 40 30 20 10 110 120 130 120 100 80 60 40 20 x - profile [ mm ] x - profile [ mm ] - index ( 3% / 3mm ) - index ( 5% / 5mm ) figure 4 . 
they reported rapid and long - term pain relief with low acute and late toxicity using imrt with a median of 7 incident beams ( range , 614 )  . 
 [ 5 ] examined the efficiency and the possible advantages of single fraction stereotactic radiosurgery ( srs ) using helical tomotherapy in the treatment of a patient with spinal column metastases in a case report . 
the ptv consisted only of the t6 vertebral bone and the treatment time was 13.6mthe long treatment time resulted from the high fraction dose ; thus , a lower fraction dose , e.g. , 2gy , would reduce treatment time accordingly . 
reirridiation of spinal metastates : comparison of treatment techniques for tomotherapy but it is of negligible clinical relevance in the retreatment of spinal lesions that will normally be restricted to lesions < 40cm in length . a first report by wu et al . 
treatment plans were generated with the tps eclipse ( varian medical systems , usa ) in conjunction with a novalis tx linear accelerator with a maximal dose rate of 1000mu / min and a single fraction dose of 16gy . 
similar to our results they found a reduction of mu ( 24% ) and also of treatment time ( 52% ) , interestingly with the two - arc treatment being delivered faster than the one - arc treatment and with fewer mu . 
dosimetric data of their approach , however , are missing because their technique had not been implemented clinically at the time of publication [ 35 ]  . we performed dosimetry with edr2 films and ionization chambers because this method is stable and has been extensively validated . 
early reports indicate their reliability and validity [ 2 , 14 , 27 ] and this approach is currently validated for vmat at our department [ 3 ]  . an important issue for dosimetric accuracy is the distance of the control points ( cp ) during the setup of our vmat plans . 
consequently the dose calculation is performed in a discrete way but the delivery is dynamic , which leads to disagreements in measurements against calculation especially in the low dose region outside the ptv at the border of the phantowe chose a distance between the cp of 5 which is sufficient to create plans of excellent plan quality but led to a lower number of pixels passing the - test with the criteria 3% / 3mm ( 78.565.34% ) than usually expected . 
since figure 3 clearly indicates that this disagreement was only in the low dose region with percentage differences translating into only small absolute differences , this trade - off was accepted to keep treatment times low while still obtaining excellent target coverage and organ at risk sparing . 
continuous monte carlo dose calculation instead of a static approximation would solve this issue . as a positive collateral result , a constant reduction in treatment time and mu while maintaining plan quality of modulated treatments as indicated in this manuscript and by others reduces the concern that secondary tumors might be caused by a high number of mu with modulated techniques [ 12 ]  . 
similarly , potentially detrimental effects of treatment protraction [ 4 , 9 , 16 ] are less likely with these fast modern techniques . conclusion with plan quality being similar to static imrt , vmat is an efficient treatment technique for target volumes with a central avoidance structure . 
the increased treatment efficiency reduces the treatment time without imaging for the patient down to less than 5mthis efficient treatment approach is dosimetrically sound and has successfully been implemented clinically . acknowledgment we gratefully acknowledge the help of markus alber with the implementation of hyperion . 
we are also indebted to roberto pellegrini and manuela duglio of 3d - line / elekta and kevin brown of elekta for the close collaboration during the implementation and initial evaluation of ergo + + and vmat . 
 financial support this work was supported within the framework of a research cooperation agreement between the department of radiation oncology , mannheim university medical center and elekta . original article randomized clinical trial of postoperative strontium - 90 radiation therapy for pterygia treatment using 30 gy / 3 fractions vs . 
40 gy / 4 fractions kiyoshi nakamatsu , yasumasa nishimura , shuichi kanamori , ryuta koike , izumi tachibana , tatsuyuki nishikawa , toru shibata1 background and purpose : postoperative adjuvant treatment with strontium - 90 radiation therapy ( rt ) is a proven technique for reducing the recurrence of pterygiuthis randomized trial was conducted to evaluate whether a total dose of 40 gy provides a better local control rate than a total dose of 30 gy for surgically resected pterygia . patients and methods : a single institutional randomized trial was conducted . 
between 1999 and 2003 , 74 pterygia in 71 patients were randomly allocated to 30 gy / 3 fractions / 15 days ( arm a ) or to 40 gy / 4 fractions / 22 days ( arm b )  . 
postoperative rt was given by a strontium - 90 eye applicator , and a dose of 10 gy per fraction was delivered in weekly fractions ( day 1 , 8 , 15 , 22 )  . results : of the 74 pterygia treated , 73 in 70 patients were analyzed . 
no serious acute and late complications were noted in either arm . conclusion : our new standard fractionation for postoperative rt for pterygia is 30 gy / 3 fractions . key words : postoperative radiation therapy randomized clinical study pterygium strontium - 90 strahlenther onkol 2011 ; 187 : 4015 doi 10.1007 / s00066 - 011 - 2212 - z eine randomisierte klinische studie zur postoperativen strontium - 90 - strahlentherapie fr pterygien : 30 gy / 3 fraktionen versus 40 gy / 4 fraktionen ziel : die postoperative adjuvante behandlung mit strontium - 90 - strahlentherapie ist eine anerkannte methode , um das wiederauftreten von pterygien zu vermeiden . 
anhand der vorliegenden randomisierten studie sollte untersucht werden , ob bei operativ entferntem ptergium eine dosis von 40 gy eine bessere kontrollrate als eine dosis von 30 gy bietet . patienten und methodik : eine einzelinstitutionelle , randomisierte untersuchung wurde durchgefhrt . 
zwischen 1999 und 2003 wurden 74 pterygien bei 71 patienten stichprobenartig entweder mit 30 gy / 3 fraktionen / 15 tage ( gruppe a ) oder 40 gy / 4 fraktionen / 22 tage ( gruppe b ) behandelt . 
die postoperative rt wurde mit einem strontium - 90augenapplikator durchgefhrt , und zwar in dosen von 10 gy pro wchentlicher teilbehandlung ( tag 1 , 8 , 15 , 22 )  . ergebnisse : von den 74 behandelten pterygien wurden 73 von 70 patienten analysiert . 
bei keiner der beiden gruppen wurden ernsthafte akute oder sptere komplikationen festgestellt . schlussfolgerung : unsere neue standardfraktionierung fr postoperative strahlentherapien betrgt 30 gy / 3 fraktionen . schlsselwrter : postoperative strahlentherapie randomisierten klinischen studie pterygium strontium - 90 1department of radiation oncology , kinki university faculty of medicine , osaka , japan . received : august 23 , 2010 ; accepted : march 16 , 2011 published online : june 27 , 2011 strahlenther onkol 2011 no . 
sr - 90 rt for pterygia introduction radiotherapy is a well - established option for the treatment of some benign diseases [ 7 , 8 , 14 ] , pterygium is a benign , slowly progressive fibrovascular tissue that originates from the bulbar conjunctiva and grows towards the cornea . 
 treatment choice for symptomatic cases is usually surgical excision , although some investigators reported that irradiation with strontium - 90 ( sr - 90 ) for early and moderately advanced pterygium without resection was very effective [ 16 , 22 ]  . 
it is common to perform some type of adjuvant treatment after resection because high recurrence rates of 3967% have been reported after surgery alone [ 5 , 10 ]  . 
it was reported that irradiation with sr - 90 after surgical resection was more effective than mitomycin - c in patients with primary and recurrent pterygium in terms of recurrence rates , and safer in terms of complications [ 20 ]  . 
 [ 10 ] reported that a single fraction rt of 25 gy after surgery achieved a highly significant control rate as compared to surgery and sham treatment in a prospective randomized trial , and no major complications were observed in the sr - 90 rt ar thus , postoperative sr - 90 rt is a proven technique for reducing the recurrence of pterygium . various dose fractionation schedules , including a total dose of 2030 gy in a single fraction or 2460 gy in 36 fractions , have been reported for postoperative sr - 90 rt ( table 1 ) [ 1 , 3 , 6 , 912 , 15 , 18 , 19 , 21 , 23 ]  . 
in our previous retrospective analysis of sr90 rt for 490 pterygia , a 5 - year local control rate of 88% was obtained by fractionated rt of 3142 gy in 45 fractions / 2229 days without serious complications [ 15 ]  . 
the time interval between surgery and the start of rt was an important prognostic factor , and the local control rate was poor for pterygium with an interval of more than 3 days [ 15 ]  . 
the local control rate was also poor for pterygia with a low rt dose ( 729 gy ) compared with those with high rt doses ( 3150 gy ) , although not significant [ 15 ]  . 
since the results suggested that 729 gy in 13 fractions is insufficient , we determined that at least 30 gy should be given in fractionated rt for pterygia [ 15 ]  . 
based on these findings , we planned a randomized study comparing 30 gy / 3 fractions with 40 gy / 4 fractions to clarify the optimal dose fractionation for pterygia . patients and methods inclusion criteria for this study were patients with primary pterygia , those for whom irradiation could be started within 3 days of surgical resection , and those who were not given anticancer drugs such as mitomycin - c at the time of surgery . 
patients were randomly allocated to receive 30 gy / 3 fractions within15 days ( arm a ) or 40 gy / 4 fractions within 22 days ( arm b )  . 
for all patients , the first rt was given within 3 days of surgery , and a dose of 10 gy per fraction was delivered in weekly fractions ( day 1 , 8 , 15 , 22 )  . 
zusammenfassung der klinischen ergebnisse der postoperativen strahlentherapie von pterygien . author , year [ ref . ] aswad , 1983 [ 1 ] beyer , 1991 [ 3 ] mackenzi , 1991 [ 11 ] jrgenliemk - schulz , 2004 [ 10 ] wilder , 1992 [ 23 ] lesions dose ( gy ) 54 135 764 44 338 fractions ott a recurrence rate ( % ) complications fukushima , 1999 [ 6 ] 393 1253 490 52 64 825 80 3035 3142 2936 12 isohashi , 2006 [ 9 ] nishimura , 2000 [ 15 ] smith , 2001 [ 21 ] schultze , 1996 [ 19 ] paryani , 1993 [ 18 ] monteiro - grillo , 2000 [ 12 ] a overall treatment time b not mentioned scar formation ( 9% ) scleromalacia ( 13% ) scleral necrosis ( 4.5% ) granuloma ( 5% ) irritation ( 5% ) , visual disturbance ( 3% ) , granuloma ( 0.9% ) , atrophy ( 0.6% ) visual disturbance ( 5.3% ) , pain ( 3.3% ) , congestion ( 2.5% ) no severe late complications scleromalacia ( 1.8% ) no severe late complications no severe late complications no severe late complications no severe late complications strahlenther onkol 2011 no . 
patienteneigenschaften. rt dose patients pterygia site side otta intervalb treatment for pterygia arm a ( 30gy / 3fr ) arm b ( 40gy / 4fr ) median ( range ) male female 60 years ( 3876 ) 62 years ( 4684 ) nasal temporal left right 15 days ; 40 22 days ; 1 1 day ; 30 2 days ; 7 3 days ; 4 22 days ; 26 29 days ; 6 1 day ; 17 2 days ; 11 3 days ; 4 aoverall treatment time , binterval between surgery and the first rt day . nakamatsu n , et al . 
for most patients , surgery was performed using the bare screra technique , which is characterized by leaving a large portion of the sclera bare after removing the pterygium and underlying conjunctiva . the first follow - up after treatment was scheduled 1 month after the last treatment , and follow - up was performed every 6 months for more than 2 years . 
early and late toxicities were scored according to nci - ctc version 3.0. for all patients , postoperative rt was performed at kinki university faculty of medicine with a sr - 90 eye applicator . 
because of the irradiation procedure , it was difficult to estimate the minimum dose at the surgical bed . the duration of local control was calculated from the date of surgery . 
a p - value < 0.05 was regarded as significant . results between july 1999 and july 2003 , 71 patients with 74 previously untreated pterygia were enrolled in this study . 
lokale kontrollrate fr arm a ( durchgezogene linie ) und arm b ( gestrichelte linie )  . one patient with a pterygium ( arm a ) was excluded from the analysis , because he refused to return to our hospital after one fraction ( 10 gy ) of rt . 
bilateral pterygia surgery was not done on the same day , and the randomization was performed for each pterygiuof the 73 pterygia , 41 pterygia in 39 patients were placed in arm a , and the remaining 32 in 31 patients in arm b . 
there were no statistical differences in sex , age , the interval time between surgery and rt , and the percentage extension of the rt period between arm a and arm b ( table 2 )  . 
sr - 90 rt for pterygia seventy - one pterygia were located on the nasal side , while the remaining two pterygia were located on the temporal side . all 73 pterygia were treated with a planned dose of rt and were followed for at least 24 months . 
in the present study , the overall recurrence rate by postoperative 90 - sr rt for pterygia was 21% ( 15 / 73 ) , and the 2 - year recurrence rate was 19% ( 14 / 73 )  . 
in terms of late toxicities , three cases of dry eye ( grade 1 ) were noted in arm a . discussion there are very few randomized studies comparing the dose fractionation for postoperative rt . 
in the present randomized study , a total rt dose of 30 gy / 3 fractions ( arm a ) and 40 gy / 4 fractions ( arm b ) were compared for surgically resected pterygia . 
table 1 shows a summary of clinical results for postoperative 90 - sr rt in other studies , and the recurrence rates ranged from 224% using prescription doses of 2060 gy in 16 fractions [ 1 , 3 , 6 , 912 , 15 , 18 , 19 , 21 , 23 ]  . the 2 - year recurrence rate for arm b ( 40 gy / 4 fractions / 22 days ) was 25% . 
this short interval between surgery and rt may be linked to the good local control rate [ 15 ]  . several authors reported that scleromalacia , scar formation , and scleral necrosis occurred as late complications , especially in case of long - term follow - up [ 11 , 13 , 15 ]  . 
thus , it seems safe to use a fractionated schedule rather than a single rt fraction . in the present study , only one case ( arm a ) recurred 42 months after treatment and the other cases recurred within 2 years ( a median of 6 months ) after treatment . 
ophoriginal article whole - brain radiotherapy combined with surgery or stereotactic radiotherapy in patients with brain oligometastases long - term analysis giuseppe roberto d ' agostino1 , rosa autorino1 , angelo pompucci2 , maria carmen de santis1 , stefania manfrida1 , giuseppe di lella3 , giovanna mantini1 , vincenzo frascino1 , silvia chiesa1 , alessio albanese2 , nicola dinapoli1 , luigi azario4 , alba fiorentino1 , vincenzo valentini1 , carmelo anile2 , mario balducci1 objective : to verify whether the treatment of brain oligometastases with whole - brain radiotherapy ( wbrt ) plus stereotactic radiotherapy ( srt ) or surgical resection results in different outcomes . methods : files of patients affected by brain metastases submitted to surgical resection followed by wbrt ( group a ) or wbrt + srt ( group b ) were retrospectively selected for this study . 
the two treatment groups were matched for the following potential prognostic factors : wbrt schedule , age , gender , performance status , tumor type , number of brain metastases , extracerebral metastases , and recursive partitioning analysis class ( rpa )  . 
the outcomes of patients in both groups were evaluated in terms of toxicity , local control , and overall survival . results : total of 97patients were selected ( 56male ; 42female ) who were respectively submitted to surgical resection followed by wbrt ( group a , n = 50 patients ) or wbrt + srt ( group b , n = 47 patients )  . 
die lokale tumorkontrolle nach 1 jahr betrug 46 , 0% ( gruppe a ) und 69 , 0% ( gruppe b ) , ohne dass dieser unterschied statistisch signifikant wre ( p = 0 , 10 )  . 
of physics , catholic university of the sacred heart , rome , italy . received : october 4 , 2010 ; accepted : march 18 , 2011 published online : june 28 , 2011 strahlenther onkol 2011 no . 
unsere daten sprechen fr eine behandlung mit wbrt plus srt bei vorliegen von ein oder zwei hirnmetastasen , die kleiner als 3 cm sind . schlsselwrter : hirnmetastasen oligometastasen stereotaktische radiotherapie operation ganzhirnbestrahlung introduction metastatic brain tumors are the most common intracranial neoplasm in adults , and although the exact incidence is unknown , it has been estimated to be as high as 200 , 000 cases per year [ 9 ]  . 
population - based data suggest that 810% of adult cancer patients develop brain metastases during their lives [ 4 , 11 , 27 ] , even if the absolute frequency of metastatic carcinoma to the brain is thought to be increasing as cancer patients live longer because of earlier diagnosis and more effective treatments regimens [ 21 ]  . the prognosis for most patients with brain metastases is poor and their life expectancy is measured in months [ 24 , 29 , 32 ]  . 
therefore , a more aggressive approach to these cases appears to be justified such as surgical resection of metastases or stereotactic radiosurgery with or without additional wbrt [ 3 , 5 , 8 , 9 , 13 , 14 , 16 , 20 , 25 , 28 ]  . however , no randomized studies have yet compared stereotactic radiotherapy ( srt ) to surgical resection and no definitive conclusions were reached regarding which of these treatments offers the best results in terms of patient safety and outcome . at our institution , patients with extracranial controlled disease and < 3 metastases are usually referred to a surgeon if they present neurological symptoms or lesions with diameter > 3 cm , while , in the case of any contraindication to surgery or asymptomatic disease and lesion diameter < 3 cm , patients are treated with wbrt followed by a stereotactic boost to the residual tumor . 
in this analysis , we aimed to verify in a series of cases with the above mentioned disease presentation and treated in the last decade whether treatment of brain oligometastases with wbrt plus srt would offer different outcome when compared with surgical resection plus wbrt . methods patients affected by brain metastases of any primary tumor , and treated at our institution with either resection of metastases plus wbrt ( group a ) or wbrt plus sbrt ( group b ) , were retrospectively analyzed . 
further inclusion criteria were the following : no prior radiotherapy or surgery to the brain , less than 3 brain metastases , diameter 3 cm for group b , confirmed by magnetic resonance imaging ( mri ) , controlled primary tumor , absent or controlled extracranial metastases , and rpa [ 10 ] class 12 . patient immobilization was obtained using a thermoplastic mask during wbrt , while a noninvasive stereotactic relocatable immobilization system ( 3d - line srl ) was used during the stereotactic phase . 
the dose was prescribed to the isocenter with the 95% isodose encompassing the whole brain and 80% isodose encompassing the entire gtv for sbrt . a 6mv photon beam delivered by a linac was used in both phases . 
in patients of groupa , the median total dose was 3 , 000 cgy ( range , 3 , 0004 , 000 cgy ) , while in patients of group , wbrt was administered with a median total dose of 3 , 750cgy ( range , 3 , 0004 , 000 cgy ) with a median daily dose of 250 cgy ( range , 200300 cgy )  . 
data regarding baseline characteristics and follow - up were obtained from patient files . the following potential prognostic factors were evaluated : age , sex , primary tumor type ( lung cancer , breast cancer , rectal cancer , other tumors ) , number and size of lesions , and rpa class . 
only recursive partitioning analysis ( rpa ) class1 and2 patients were included in the present study because patients with poor performance status ( rpa class3 ) are usually not offered sbrt or surgery . after treatment , patients were evaluated 1 month after treatment by mri and then quarterly . 
the cox proportional hazards regression model was used to analyze the effect of covariates on survival . results we retrospectively evaluated 651 files relative to patients submitted to wbrt for brain metastases from january , 1997 to march , 2010 , at our institution . 
among them , 97 cases were selected ( 56 males ; 42 females ) who were respectively submitted to surgical resection before wbrt ( groupa , n = 50patients ) or srt after wbrt ( groupb , n = 47 patients )  . patient characteristics of the entire cohort are summarized in tables 1 and 2 . 
srt : stereotaktische strahlentherapie , fsrt : fraktionierte stereotaktische strahlentherapie . total group a group b characteristics patients , n age , years rpa class fractionation fsrt total group a group b table 2 . 
tumorcharakteristika. characteristics primary tumor lung cancer breast cancer rectal cancer others no brain metastases 1 : 83 2 : 14 1 : 46 2 : 4 1 : 37 2 : 10 ( range , 3781 years )  . 
among the patients submitted to srt ( groupb ) , 17cases , selected on the basis of the site of their single metastasis with respect to brain critical structures , received radiosurgery ( srs , median dose 15 gy ; range , 1520gy )  . toxicity grade 3 acute toxicities , such as headache , hearing problems , nausea , and vomiting did not occur in treated patients . 
only 1patient with local relapse presented a neurocognitive deficit ( memory loss ) 7years after treatment . survival median follow - up was 95months ( range , 8171months ) in all patients . 
no statistically significant difference was found among patients treated by wbrt + sbrt ( 18months ) with respect to those treated by surgery + wbrt ( 11months ; p = 0.10 ; figure 1 )  . 
lokale tumorkontrolle in gruppe a ( rote linie ) verglichen mit der lokalen tumorkontrolle der patienten in gruppe b ( blaue linie ) im zeitlichen verlauf ( monate )  . 
recent studies [ 3 , 28 ] have demonstrated that life expectancy of these patients is influenced not only by the number of brain lesions , but also by several factors , such as the number of extracranial metastases , the patients age , karnofsky performance scale ( kps ) , and the status of primary disease . 
in fact , these therapeutic approaches represent , together with wbrt , the standard treatment of 13 brain metastases [ 18 ]  . a meta - analysis of randomized trials on adult cancer patients with single or multiple brain metastases from cancer of any histology was published in 2005 to investigate the role of radiotherapy in the management of brain metastases [ 30 ]  . 
a prospective trial including patients who underwent gross resection of a single brain metastasis indicated that there was an improvement in local control for patients who received postoperative wbrt without any significant difference in overall survival [ 22 ]  . 
these studies suggested that better brain control was achieved with the combined approach than with wbrt alone , although no significant difference was observed in terms of median overall survival . the meta - analysis by tsao et al . 
 [ 20 ] reported no significant difference ( p = 0.15 ) in overall survival between 74 patients treated by neurosurgery and 23 patients treated with srs and none of the srs group had local recurrence compared to 19patients of the neurosurgical group . unlike the majority of published studies , our data compare patients undergone surgery plus wbrt to patients submitted to wbrt followed by srt always performed by linear accelerators : this technology does not need a dedicated tool such as the gamma - knife nor does it require the positioning of a fixed stereotactic frame . 
the toxicity rates were , in fact , relatively low in both groups , which is in agreement with the evidence from the literature [ 7 ]  . in particular , we reported only 1 case of neurocognitive deficit after 7years , but it must be taken into account that control of the brain tumor remains the most important factor for stabilizing neurocognitive function [ 2 ] ; therefore , wbrt is still part of standard treatment for brain metastases . our study , with the limits of any retrospective analysis , proves that after a considerable follow - up the efficacy of srt is favorable comparable to surgery in producing adequate local control with the same overall survival . 
our survival analysis also failed to find any statistically significant association with the traditional prognostic factors ( e.g. , rpa class , primary tumor , number of brain lesions ) : this finding can be explained by selection bias , the small sample size , the effectiveness of brain metastases treatment , but also obviously by the impact of all treatments offered to patients during their clinical history . 
the continuity of care even after brain progression and the confidence that the mere presence of brain metastases does not preclude an aggressive approach to patient care may explain the long survival and the lack of differences in the various subgroups analyzed . in conclusion , our data suggest that wbrt + srt may be an effective , noninvasive approach which can be offered to patients affected by small brain metastases ( < 3 cm ) , especially when their extracranial disease is controlled and for personal or clinical reasons they are not candidates for metastasectomy ; surgery still remains the preferable treatment in symptomatic patients . original article ct - myelography for high - dose irradiation of spinal and paraspinal tumors with helical tomotherapy revival of an old tool matthias uhl , florian sterzing , gregor habl , kai schubert , gabriele sroka - perez , jrgen debus , klaus herfarth1 background and purpose : high - dose irradiation or reirradiation of spinal and paraspinal tumors is a challenge particularly in the presence of metal artifacts after surgery . 
precise delineation of the spinal cord is necessary treating paraand intraspinal tumors with a sufficient dose . patients and methods : the use of myelo - ct was evaluated in 23 patients with spinal and paraspinal tumors . 
treatment was performed by using a tomotherapy treatment unit . results : contouring of the myelon in all slices of the myelo - ct was possible in 20 of 23 patients . 
no separation between tumor and myelon could be observed in 3 patients . conclusion : myelo - ct offers a distinct delineation of the myelon and the paraspinal tumor in case of artifacts due to metal implants after surgery . 
using this tool in combination with advanced image guidance and imrt techniques , patients with relatively radioresistent paraspinal tumors might have the chance of improved local control using higher target doses . key words : myelo - ct paraspinal tumor helical tomotherapy strahlenther onkol 2011 ; 187 : 41620 doi 10.1007 / s00066 - 011 - 2219 - 5 wiederentdeckung eines alten werkzeugs : ct - myelographie fr die hochdosisbestrahlung von spinalen und paraspinalen tumoren mit der helikalen tomotherapie hintergrund : hochdosisbestrahlung oder rebestrahlung von spinalen und paraspinalen tumoren ist eine herausforderung , besonders in gegenwart von metallartefakten nach operation . 
daher ist eine genaue abgrenzung des rckenmarks notwendig , um die behandlung paraund intraspinaler tumoren mit einer ausreichenden dosis durchfhren zu knnen . patienten und methoden : die verwendung eines myelo - ct wurde bei 23 patienten mit spinalen und paraspinalen tumoren untersucht . 
eine abgrenzung des myelon vom tumorgewebe war bei 3 patienten nicht mglich . schlussfolgerung : das myelo - ct fhrt zu einer deutlichen abgrenzbarkeit des myelons von paraspinalen und spinalen tumoren bei metallartefakten nach operation . 
mit diesem werkzeug in kombination mit modernen imrt - techniken , knnte eine verbesserung der lokalrezidivrate bei patienten mit relativ radioresistenten paraspinalen tumoren erreicht werden . schlsselwrter : myelo - ct paraspinaler tumor helikale tomotherapie 1department of radiation oncology , university of heidelberg , heidelberg , germany . received : september 10 , 2010 ; accepted : january 24 , 2011 published online : june 27 , 2011 strahlenther onkol 2010 no . 
ct - myelography for high - dose irradiation of spinal and paraspinal tumors with ht introduction the management of paraspinal tumors with low radiosensitivity is a challenge [ 20 ] and there is still no consensus for treatment . 
the spinal cord dose limits in the literature are between 45 and 50gy given to the full cross section of the cord [ 4 , 10 , 14 ]  . 
the treatment of spinal and paraspinal tumors with new techniques like imrt , in combination with image guidance , deliver a highly conformal radiation in a safe manner , allowing increase dose to the tumor , while sparing normal tissue [ 6 , 7 , 11 , 16 , 17 , 23 ]  . 
new mri sequences seem to be more accurate for delineation of the myelon and the tumor ; however , in the case of metal artifacts after surgery , segmentation of normal tissue might be difficult with mri and ct ( figure 1 ) [ 1 , 13 , 22 ]  . patients and methods the use of myelo - ct for treatment planning was evaluated in 23 patients with spinal or paraspinal tumors between 2007 and 2009 . 
 all had had surgery previously , with either incomplete ( n = 18 ) resection or marginal ( n = 5 ) resection of the tumor , most of them with partial or total vertebrectomy and consecutive substitution of it . 
while 13 patients had never been irradiated previously , 2 patients with a sarcoma in the vertebral bodies of the thorax were treated about 20 years ago due to hodgkins disease . 
d kv - ct nach der myelographie . treatment planning was performed by using nonenhanced ct and enhanced myelo - ct in the same position and immobilization ( figure 1 )  . 
the dose to the spinal cord was limited to the tolerance dose using an alpha / beta of 2gy for the myelon in order to take lower fraction doses into account . of the 11 patients with cordoma , 10 were treated with an average dose of 68.7 gy , while 1patient , who was pretreated with 44 gy in another department without sparing the spinal cord , received a boost with 24 gy on average while sparing the myelon . 
applikation von kontrastmittel in den subarachnoidalraum bei einem patienten mit metallimplantaten nach erfolgter operation . elon and the paraspinal tumor in case of metal artifact , due to metal implants after surgery . 
 [ 22 ] also showed an advantage in planning of cyber knife stereotactic radiosurgery of spinal tumors in patients with postoperative metal material , a previous irradiation or intramedullary tumors by using myelo - ct instead of 3d - fiesta mri . myelo - ct will be an important tool for treatment planning of paraspinal tumous and metal artifacts until there is a new mri sequence which offers equal delineation . 
for the planning and for the daily image guidance the nonenhanced ct , which was fused with the enhanced myelo - ct before , was used , because of the better contrast between the vertebral body and the cerebrospinal fluid in the nonenhanced one ( figure 2 )  . 
in 3 patients , it was not possible to delineate the myelon from the tumor because there was no more flow of the cerebrospinal fluid between tumor and spinal cord . 
in such cases , a myeloct is not helpful . helical tomotherapy delivers a highly conformal dose distribution while sparing the normal tissue [ 9 , 12 , 18 , 19 , 25 ]  . 
dosisverteilung und dosis - volumen histogramm eines patienten mit chordomyelon , myelon + 3 , und myleon + 10 sind jeweils schnittmengen mit dem ptv . gins of 3mm around the spinal cord and a daily image guidance with the integrated mv - ct . 
ct - myelography for high - dose irradiation of spinal and paraspinal tumors with ht of 50gy was not exceeded [ 4 , 10 , 14 , 24 ] , while treating the tumor with a sufficient dose ( figure 3 )  . 
by using the myeloct in combination with advanced image guidance and imrt techniques , patients with relatively radioresistent paraspinal tumors might have the chance of improved local control using higher target doses . 
further follow - up for the local control rate is warranted . myelo - ct is a valuable tool for the radiation treatment of patients with relatively radioresistent spinal and paraspinal tumors in the presence of metal implants around the target . conclusion original article respiratory - induced prostate motion characterization and quantification in dynamic mri julien dinkel1 , christian thieke2 , 3 , christian plathow1 , 4 , patrick zamecnik1 , hermann prm5 , peter e huber2 , hans - ulrich kauczor1 , 6 , heinz - peter schlemmer1 , christian m . 
zechmann1 , 7 background and purpose : to investigate prostate movement during deep breathing and contraction of abdominal musculature by means of dynamic mri and analyze implications for image - guided radiotherapy of prostate cancer . patients and methods : a total of 43 patients and 8 healthy volunteers were examined with mri . 
images during deep respiration and during contraction of abdominal musculature ( via a coughing maneuver ) were obtained with dynamic twodimensional ( 2d ) balanced ssfp ; 3 frames / s were obtained over an acquisition time of 15 s . 
further investigations regarding possible applications in image - guided radiotherapy , e.g. , for individualized planning and in integrated linac / mri systems , are warranted . key words : dynamic mri organ motion prostate strahlenther onkol 2011 ; 187 : 42632 doi 10.1007 / s00066 - 011 - 2201 - 2 ateminduzierte bewegung der prostata : charakterisierung und quantifizierung mittels dynamischer mrt zielsetzung : ziel dieser studie war die nicht - invasive analyse der ateminduzierten prostatabewegung mittels dynamischer mrt - bildgebung im hinblick auf die auswirkungen fr die bildgesttzte radiotherapie beim prostatakarzinom . methoden : 43 patienten und 8 probanden wurden mittels mrt untersucht . 
die kraniokaudale atembedingte prostatabewegung betrug 2 , 7 1 , 9 ( sd ) mm ( range 0 , 510 , 6 mm ) , whrend die anteroposteriore bewegung bei 1 , 8 1 ( sd ) mm ( range 0 , 310 mm ) lag . 
die ap - bewegung betrug 8 , 3 7 , 7 ( sd ) mm ( range 0 , 726 mm )  . schlussfolgerung : die dynamische mrt ermglicht die nichtinvasive analyse der prostatabewegung . 
zur individuellen planung und integration in mrt - / linac - systeme , sind erforderlich . schlsselwrter : dynamische mrt organbewegung prostata 1department of radiology , german cancer research center , heidelberg , germany , 2clinical cooperation unit radiation oncology , german cancer research center , heidelberg , germany , 3department of radiation oncology , university clinic heidelberg , heidelberg , germany , 4radiology baden - baden , baden - baden , germany , 5software development for integrated diagnostics and therapy group , german cancer research center , heidelberg , germany , 6department of radiology , university clinic heidelberg , heidelberg , germany , 7department of nuclear medicine , university clinic heidelberg , heidelberg , germany . received : july 5 , 2010 ; accepted : february 4 , 2011 published online : june 27 , 2011 strahlenther onkol 2010 no . 
respiratory prostate motion in dynamic mri introduction the biochemical control rate ( psa recurrence free survival ) of prostate cancer after definitive radiotherapy could be significantly improved by escalating the total dose above 72 gy [ 5 , 11 , 15 , 22 , 24 , 29 ] , especially in patients with intermediate ( stage t2b , gleason score 7 , or psa level 10.120 ng / ml ) and high ( stage t2c , gleason score 810 , or psa level > 20 ng / ml ) [ 3 ] risk disease . 
however , the treatment toxicity can be increased with the use of higher radiation doses , particularly regarding the rectum and bladder , unless high precision radiotherapy techniques are used to limit exposure of normal tissues [ 8 , 9 , 13 , 30 ]  . 
first , a conformal dose distribution that restricts the high dose area to the prostate should be generated , e.g. , by three - dimensional conformal radiotherapy ( 3d - crt ) , intensity - modulated radiotherapy ( imrt ) , or particle therapy with protons or heavier ions . second , the movements of the prostate both between fractions ( interfractional ) and during treatment ( intrafractional ) should be taken into account by individualized margins or by compensation and correction techniques during delivery . 
in this context , daily online imaging and correction of prostate position , e.g. , by cone - beam ct , can be employed to minimize the effects of systematic and random interfractional prostate motion and setup variation . 
it is known that the anatomical position of the prostate gland and seminal vesicles is influenced by the physiological movements of respiration and of the surrounding pelvic organs [ 1 , 20 , 21 ]  . 
this has direct implications for radiotherapy planning and delivery , especially in conformal radiotherapy where the treatment planning margins can be much more closely tailored to the prostate . recent studies have evaluated the anatomical variability of the position of the prostate gland within the pelvis during a 67 week course of radical irradiation for prostate cancer [ 16 , 19 ]  . 
several methods have been proposed to evaluate prostate motion , including fluoroscopy , sonography , magnetic resonance imaging ( mri ) , and recently the implantation of magnetic intraprostatic fiducials [ 17 ]  . 
mri techniques have been recently successfully introduced for the evaluation of thoracic tumor motion [ 6 , 25 ]  . the objective of the presented study was to investigate the feasibility of cine mri imaging for quantitative evaluating prostate movements in real time and to analyze possible implications for image - guided radiotherapy . patients and methods subjects ' characteristics a total of 8 healthy volunteers with a median age of 30.2 years ( range , 24.232.7 ) were enrolled in this study . 
patients were excluded if they had any prior radiation therapy or surgery within the pelvis . after the nature of the procedure had been fully explained , informed consent was provided by all participants under an institutionally approved subject research protocol . mri examination all examinations were performed in supine position using a clinical 1.5 - t whole - body scanner ( magnetom symphony , siemens medical solutions , erlangen , germany ) equipped with eight receiver channels , a 6 - channel coil , endorectal coils , and a high performance gradient system ( 30 mt / m ; slew rate 120 mt / m / s )  . 
the following standard mr sequences for pelvic imaging were initially performed : axial turbo spin - echo ( tse ) t1and t2 - weighted , sagittal and coronal t2 - weighted turbo spin - echo imaging . 
during the examinations , 3 frames / s were acquired within an acquisition time of 15 s , which was sufficient to record 37 breathing cycles . all subjects were instructed to breathe deeply during the first mr - cine acquisition ( figure 1 )  . 
in a second step , the examination was repeated while the subjects contracted their abdominal musculature similarly to coughing ( figure 2 )  . data processing the cine movement studies were transferred to a workstation for further evaluation ( leonardo , siemens medical solutions , erlangen , germany )  . 
 only the movement of the base of the prostate ( upward near the inferior surface of the bladder ) was analyzed ; we assumed that there was negligible motion for the apex , as was found in previous studies [ 20 ] ( figures 3 and 4 )  . 
respiratory prostate motion in dynamic mri with standard software ( excel 97 , microsoft , redmond , wa , usa ; bias for windows , version 8.207 / 2006 , epsilon , frankfurt , germany )  . results all examinations were eligible for further evaluation . 
the results of prostate motion in each condition are summarized in tables 13 . respiratory - induced prostate motion synchronous the acquisition of 3 images / s allowed for continuous recording during 37 breathing cycles ( figure 5 )  . 
a computer - based semiautomatic volumetry of the bladder and prostate was performed using the free breathing standard t2 - weighted tse images of the pelvis and dedicated software ( syngo oncology , siemens , germany ) patched to enable mri data compatibility . statistical analyses pearson regression modeling was used to study the relationship between bladder or prostate volume with prostate motion . 
die unterschiede waren statistisch signifikant mit einem p - wert von 0 , 007 fr die kraniokaudale und 0 , 04 fr die anteroposteriore verschiebung ( gepaarter t - test )  . 
craniocaudal ( cc ) and anteroposterior ( ap ) prostate motion during free breathing ( resp ) and during contraction of the abdominal musculature ( m contraction ) in patients and volunteers . 
the small magnitudes of respiratory - induced prostate motion measured in our subjects and in the aforementioned literature foster the notion that normal shallow breathing in the supine position contributes negligibly to relevant intrafraction prostate motion . 
however , we could identify a subgroup of patients ( 31% of all subjects ) with relevant unusual prostate mobility ( > 3 mm respiratory - related prostate motion )  . nificant ( p = 0.007 for craniocaudal displacement and 0.04 for anteroposterior displacement )  . 
this might be due to the fact that the t1ct2c tumors do not grow beyond the prostate capsule and are , therefore , not fixated to the surrounding tissue . dynamic mri has been used in sagittal and sometimes combined with axial acquisitions to address intrafractional prostate motion [ 10 , 14 , 23 ]  . 
the sampling time was , therefore , very low ( 620s ) and the time window was longer than in our study in order to identify and characterize rectal peristaltism - related prostate motion . 
patients who most likely will not benefit from such a procedure could be spared , thus , making the therapy more adequate and more cost effective . particularly promising appears the use of dynamic mri in upcoming integrated , hybrid linac / mri systems [ 7 , 18 ]  . 
die box reprsentiert die standardabweichung und die mittellinie die durchschnittliche prostatabewegung . a limitation of our study is the relatively short examination time which prevented analysis of rectal activity and its influence on prostate movement . 
the prostate gland is known to move independent of the bony pelvis and its relative anatomical position can be affected by the activity of neighboring structures , e.g. , the rectum and bladder [ 17 , 27 ]  . 
this type of motion is usually evaluated using other methods like ultrasound devices and ct / cone - beam ct imaging on the treatment machine before treatment delivery [ 2 , 12 , 26 ]  . one possible application of dynamic mri for prostate motion in radiotherapy would be to select patients prior to the start of therapy who may potentially profit from sophisticated motion - adapted radiotherapy techniques like electromagnetic transponder implantation . 
 original article whole - brain radiotherapy combined with surgery or stereotactic radiotherapy in patients with brain oligometastases long - term analysis giuseppe roberto d ' agostino1 , rosa autorino1 , angelo pompucci2 , maria carmen de santis1 , stefania manfrida1 , giuseppe di lella3 , giovanna mantini1 , vincenzo frascino1 , silvia chiesa1 , alessio albanese2 , nicola dinapoli1 , luigi azario4 , alba fiorentino1 , vincenzo valentini1 , carmelo anile2 , mario balducci1 objective : to verify whether the treatment of brain oligometastases with whole - brain radiotherapy ( wbrt ) plus stereotactic radiotherapy ( srt ) or surgical resection results in different outcomes . methods : files of patients affected by brain metastases submitted to surgical resection followed by wbrt ( group a ) or wbrt + srt ( group b ) were retrospectively selected for this study . 
the two treatment groups were matched for the following potential prognostic factors : wbrt schedule , age , gender , performance status , tumor type , number of brain metastases , extracerebral metastases , and recursive partitioning analysis class ( rpa )  . 
the outcomes of patients in both groups were evaluated in terms of toxicity , local control , and overall survival . results : total of 97patients were selected ( 56male ; 42female ) who were respectively submitted to surgical resection followed by wbrt ( group a , n = 50 patients ) or wbrt + srt ( group b , n = 47 patients )  . 
die lokale tumorkontrolle nach 1 jahr betrug 46 , 0% ( gruppe a ) und 69 , 0% ( gruppe b ) , ohne dass dieser unterschied statistisch signifikant wre ( p = 0 , 10 )  . 
of physics , catholic university of the sacred heart , rome , italy . received : october 4 , 2010 ; accepted : march 18 , 2011 published online : june 28 , 2011 strahlenther onkol 2011 no . 
unsere daten sprechen fr eine behandlung mit wbrt plus srt bei vorliegen von ein oder zwei hirnmetastasen , die kleiner als 3 cm sind . schlsselwrter : hirnmetastasen oligometastasen stereotaktische radiotherapie operation ganzhirnbestrahlung introduction metastatic brain tumors are the most common intracranial neoplasm in adults , and although the exact incidence is unknown , it has been estimated to be as high as 200 , 000 cases per year [ 9 ]  . 
population - based data suggest that 810% of adult cancer patients develop brain metastases during their lives [ 4 , 11 , 27 ] , even if the absolute frequency of metastatic carcinoma to the brain is thought to be increasing as cancer patients live longer because of earlier diagnosis and more effective treatments regimens [ 21 ]  . the prognosis for most patients with brain metastases is poor and their life expectancy is measured in months [ 24 , 29 , 32 ]  . 
therefore , a more aggressive approach to these cases appears to be justified such as surgical resection of metastases or stereotactic radiosurgery with or without additional wbrt [ 3 , 5 , 8 , 9 , 13 , 14 , 16 , 20 , 25 , 28 ]  . however , no randomized studies have yet compared stereotactic radiotherapy ( srt ) to surgical resection and no definitive conclusions were reached regarding which of these treatments offers the best results in terms of patient safety and outcome . at our institution , patients with extracranial controlled disease and < 3 metastases are usually referred to a surgeon if they present neurological symptoms or lesions with diameter > 3 cm , while , in the case of any contraindication to surgery or asymptomatic disease and lesion diameter < 3 cm , patients are treated with wbrt followed by a stereotactic boost to the residual tumor . 
in this analysis , we aimed to verify in a series of cases with the above mentioned disease presentation and treated in the last decade whether treatment of brain oligometastases with wbrt plus srt would offer different outcome when compared with surgical resection plus wbrt . methods patients affected by brain metastases of any primary tumor , and treated at our institution with either resection of metastases plus wbrt ( group a ) or wbrt plus sbrt ( group b ) , were retrospectively analyzed . 
further inclusion criteria were the following : no prior radiotherapy or surgery to the brain , less than 3 brain metastases , diameter 3 cm for group b , confirmed by magnetic resonance imaging ( mri ) , controlled primary tumor , absent or controlled extracranial metastases , and rpa [ 10 ] class 12 . patient immobilization was obtained using a thermoplastic mask during wbrt , while a noninvasive stereotactic relocatable immobilization system ( 3d - line srl ) was used during the stereotactic phase . 
the dose was prescribed to the isocenter with the 95% isodose encompassing the whole brain and 80% isodose encompassing the entire gtv for sbrt . a 6mv photon beam delivered by a linac was used in both phases . 
in patients of groupa , the median total dose was 3 , 000 cgy ( range , 3 , 0004 , 000 cgy ) , while in patients of group , wbrt was administered with a median total dose of 3 , 750cgy ( range , 3 , 0004 , 000 cgy ) with a median daily dose of 250 cgy ( range , 200300 cgy )  . 
data regarding baseline characteristics and follow - up were obtained from patient files . the following potential prognostic factors were evaluated : age , sex , primary tumor type ( lung cancer , breast cancer , rectal cancer , other tumors ) , number and size of lesions , and rpa class . 
only recursive partitioning analysis ( rpa ) class1 and2 patients were included in the present study because patients with poor performance status ( rpa class3 ) are usually not offered sbrt or surgery . after treatment , patients were evaluated 1 month after treatment by mri and then quarterly . 
the cox proportional hazards regression model was used to analyze the effect of covariates on survival . results we retrospectively evaluated 651 files relative to patients submitted to wbrt for brain metastases from january , 1997 to march , 2010 , at our institution . 
among them , 97 cases were selected ( 56 males ; 42 females ) who were respectively submitted to surgical resection before wbrt ( groupa , n = 50patients ) or srt after wbrt ( groupb , n = 47 patients )  . patient characteristics of the entire cohort are summarized in tables 1 and 2 . 
srt : stereotaktische strahlentherapie , fsrt : fraktionierte stereotaktische strahlentherapie . total group a group b characteristics patients , n age , years rpa class fractionation fsrt total group a group b table 2 . 
tumorcharakteristika. characteristics primary tumor lung cancer breast cancer rectal cancer others no brain metastases 1 : 83 2 : 14 1 : 46 2 : 4 1 : 37 2 : 10 ( range , 3781 years )  . 
among the patients submitted to srt ( groupb ) , 17cases , selected on the basis of the site of their single metastasis with respect to brain critical structures , received radiosurgery ( srs , median dose 15 gy ; range , 1520gy )  . toxicity grade 3 acute toxicities , such as headache , hearing problems , nausea , and vomiting did not occur in treated patients . 
only 1patient with local relapse presented a neurocognitive deficit ( memory loss ) 7years after treatment . survival median follow - up was 95months ( range , 8171months ) in all patients . 
no statistically significant difference was found among patients treated by wbrt + sbrt ( 18months ) with respect to those treated by surgery + wbrt ( 11months ; p = 0.10 ; figure 1 )  . 
lokale tumorkontrolle in gruppe a ( rote linie ) verglichen mit der lokalen tumorkontrolle der patienten in gruppe b ( blaue linie ) im zeitlichen verlauf ( monate )  . 
recent studies [ 3 , 28 ] have demonstrated that life expectancy of these patients is influenced not only by the number of brain lesions , but also by several factors , such as the number of extracranial metastases , the patients age , karnofsky performance scale ( kps ) , and the status of primary disease . 
in fact , these therapeutic approaches represent , together with wbrt , the standard treatment of 13 brain metastases [ 18 ]  . a meta - analysis of randomized trials on adult cancer patients with single or multiple brain metastases from cancer of any histology was published in 2005 to investigate the role of radiotherapy in the management of brain metastases [ 30 ]  . 
a prospective trial including patients who underwent gross resection of a single brain metastasis indicated that there was an improvement in local control for patients who received postoperative wbrt without any significant difference in overall survival [ 22 ]  . 
these studies suggested that better brain control was achieved with the combined approach than with wbrt alone , although no significant difference was observed in terms of median overall survival . the meta - analysis by tsao et al . 
 [ 20 ] reported no significant difference ( p = 0.15 ) in overall survival between 74 patients treated by neurosurgery and 23 patients treated with srs and none of the srs group had local recurrence compared to 19patients of the neurosurgical group . unlike the majority of published studies , our data compare patients undergone surgery plus wbrt to patients submitted to wbrt followed by srt always performed by linear accelerators : this technology does not need a dedicated tool such as the gamma - knife nor does it require the positioning of a fixed stereotactic frame . 
the toxicity rates were , in fact , relatively low in both groups , which is in agreement with the evidence from the literature [ 7 ]  . in particular , we reported only 1 case of neurocognitive deficit after 7years , but it must be taken into account that control of the brain tumor remains the most important factor for stabilizing neurocognitive function [ 2 ] ; therefore , wbrt is still part of standard treatment for brain metastases . our study , with the limits of any retrospective analysis , proves that after a considerable follow - up the efficacy of srt is favorable comparable to surgery in producing adequate local control with the same overall survival . 
our survival analysis also failed to find any statistically significant association with the traditional prognostic factors ( e.g. , rpa class , primary tumor , number of brain lesions ) : this finding can be explained by selection bias , the small sample size , the effectiveness of brain metastases treatment , but also obviously by the impact of all treatments offered to patients during their clinical history . 
the continuity of care even after brain progression and the confidence that the mere presence of brain metastases does not preclude an aggressive approach to patient care may explain the long survival and the lack of differences in the various subgroups analyzed . in conclusion , our data suggest that wbrt + srt may be an effective , noninvasive approach which can be offered to patients affected by small brain metastases ( < 3 cm ) , especially when their extracranial disease is controlled and for personal or clinical reasons they are not candidates for metastasectomy ; surgery still remains the preferable treatment in symptomatic patients . original article reirradiation of spinal column metastases comparison of several treatment techniques and dosimetric validation for the use of vmat florian stieler , dirk wolff , linda bauer , hans - jrg wertz , frederik wenz , frank lohr1 background : for reirradiation of spinal column metastases , intensity - modulated radiation therapy ( imrt ) reduces the dose to the spinal cord , while allowing longer treatment times . 
we analyzed the potential of volumetric modulated arc therapy ( vmat ) to reduce treatment time and number of monitor units ( mu )  . patients and methods : in ct datasets of 9patients with spinal column metastases , the planned target volume ( ptv ) encompassed the macroscopic tumor including the spinal cord or medullary cone , respectively . 
we compared a posterior ( 3d - pa ) static field technique , a two - field wedge technique ( 3d - wedge ) and 5 - / 7 - beam imrt with vmat . 
conformity index ( ci ) , homogeneity index ( hi40 ) , dose volume histogram ( dvh ) parameters , treatments delivery time ( t ) , and mu were analyzed . 
dosimetry was validated with edr2film / ionization chambers . results : ptv coverage was insufficient for 3d - conformal radiotherapy ( 3d - crt ) when spinal cord tolerance was respected . 
vmat produced dose distributions similar to imrt with shorter treatment times ( vmat : mean 4 : 49min ; imrt : mean 6 : 50min ) and fewer mu ( vmat : 785 ; imrt : 860 )  . 
 - index analysis showed an agreement of 91.333.53% for the 5% / 5mm criteria . conclusion : for this paradigm , vmat produces high quality treatment plans with homogeneity / conformity similar to static imrt , shorter treatment times , and fewer mu . 
verification measurements showed good agreement between calculation and delivered dose , leading to clinical implementation . key words : volumetric intensity modulated arc therapy intensity - modulated radiation therapy 3d conformal radiation therapy spinal column metastases strahlenther onkol 2011 ; 187 : 40615 doi 10.1007 / s00066 - 011 - 2198 - 6 rebestrahlung von paraspinalen metastasen : vergleich verschiedener bestrahlungstechniken und dosimetrische validierung von vmat ziel : die intensittsmodulierte radiotherapie ( imrt ) ermglicht bei der rebestrahlung von wirbelsulenmetastasen eine reduktion der dosis im spinalkanal bei gleichzeitig lngerer bestrahlungszeit im vergleich zur konventionellen 3d - technik . 
wir analysierten das potential der volumetrisch modulierten rotationstherapie ( vmat ) , um die bestrahlungszeit und die anzahl der monitor - einheiten ( mu ) zu reduzieren . patienten und methoden : 9 ct - datenstze von patienten mit wirbelsulenmetastasen wurden untersucht , bei denen das zielvolumen ( zv ) den makroskopischen tumor inklusive spinalkanal umfasste . 
wir verglichen eine posteriore 3d - technik ( 3d - pa ) , eine 2 - feldertechnik mit keilen ( 3d - wedge ) und 5 / 7 - felder - imrt mit vmat . 
die dosimetrie wurde mit edr2 filmen und ionistationskammer berprft . ergebnisse : die zv - abdeckung fr die 3d - techniken war insuffizient , wenn die toleranzdosis des spinalmarks bercksichtigt wurde . 
mit vmat lieen sich hnliche dosisverteilungen wie mit imrt mit krzeren bestrahlungszeiten ( vmat mittel 4 : 49min . , imrt mittel 6 : 50min . ) und weniger mu ( vmat : 785 , imrt : 860 ) realisieren . 
die - analyse zeigte eine bereinstimmung von 91 , 333 , 53% fr 5% / 5mm . 1department of radiation oncology , university medical center mannheim , university heidelberg , germany . received : july 15 , 2010 ; accepted : january 24 , 2011 published online : june 27 , 2011 strahlenther onkol 2011 no . 
reirridiation of spinal metastates : comparison of treatment techniques schlussfolgerung : fr dieses paradigma erzeugt vmat qualitativ hochwertige bestrahlungsplne mit zu imrt vergleichbarer homogenitt / konformitt , krzeren bestrahlungszeiten und weniger mu . 
verifikationsmessungen zeigten gute bereinstimmungen zwischen errechneten und gemessenen dosen und erlaubten die klinische implementierung . schlsselwrter : volumetrisch intensittsmodulierte rotationstherapie intensittsmodulierte radiotherapie 3d konformale radiotherapie wirbelsulenmetastasen introduction spinal column metastases can cause morbidity , including pain and compression of the spinal cord with resulting neurologic deficits and fractures of the vertebral bones . 
 [ 15 ] reported a local control rate of 94.7% after a median followup of 12.3 months for the reirradiation of vertebral bone metastases with stereotactic conformal radiotherapy ( 414 beam directions ) or intensity - modulated radiotherapy ( imrt )  . 
using 3dconformal radiotherapy ( 3d - crt ) without any elements of fluence modulation for retreatment exceeds the radiation tolerance to the spinal cord when target doses of > 30gy are intended [ 18 ]  . 
we , therefore , explored the possibility of establishing volumetric modulated arc therapy ( vmat ) clinically to treat this target paradigseveral earlier studies have shown that vmat may reduce treatment time and primary monitor units ( mu ) for several target types with dose distributions similar to imrt [ 1 , 19 , 21 , 25 , 28 , 29 , 3233 ] , although the benefit is not easy to quantify theoretically , since only preliminary attempts at a comprehensive theory of vmat have been made [ 31 ]  . we report the analysis of different treatment techniques regarding plan quality , treatment efficiency , and dosimetric delivery accuracy of vmat for this target paradigm as evaluated prior to clinical implementation . materials and methods retreatments were planned based on ct datasets of 9patients with spinal column metastases who had previously been treated with 3d - crt to spinal cord tolerance . 
 we chose a prescription dose for the target of 40 gy with a fraction dose of 2 gy , planned for a 6mv synergy linear accelerator ( elekta , uk ) with a maximum dose rate of 600 mu per minute . 
 median dose to the sc was intended not to exceed 26 gy based on available data for retreatment tolerance [ 17 , 30 ]  . two different 3d - crt strategies were assessed in this study : a single posterior ( 3d - pa ) static field ( 180 ) and a two - field wedge technique ( 3d - wedge ) with two beams at angles of around 160 and 200 , respectively , depending on patient anatomy . 
as reference modulated treatment , we created an isotropically distributed 5 - beam imrt ( imrt - 5b ) and an isotropically distributed 7 - beam imrt ( imrt - 7b ) plan , respectively , using the tps hyperion ( university of tbingen , germany )  . 
vmat plans were generated with ergo + + 1.7.2 ( elekta - software , saint louis , mo , usa ) with two complete 360 rotations ( clockwise and counter clockwise ) to increase the modulation depth ( the first rotation focused on the whole ptv excluding the sc , the second focused on the part of the target immediately adjacent to the sc ) and were normalized as described for static imrt plans . for statistical analyses , exact wilcoxon signed - rank tests were used to assess any differences between the treatment paradigms . 
due to the fact that we prescribe dose to the median dose level in the ptv , we had to modify the ci as follows : stieler f , et al . 
reirridiation of spinal metastates : comparison of treatment techniques where vptv describes the target volume in cm and vd99% is the total volume in cm which receives the effective minimal target dose ( dose encompassing 99% of the ptv )  . 
the ci definition is characterized by the effective minimal dose applied to the ptv which follows the idea of the ci definition by the rtog . hi is defined as follows according to the rtog guidelines [ 24 ] : where dpresc is the prescription dose and dmax is the maximum dose in the treatment plan . 
 c95%pd describes the percentage coverage of the ptv by the isodose representing 95% of the prescription dose ( pd ) and scptv is the median dose to the spinal cord inside the ptv . 
for all approaches , ttt was measured on the unit with the same measuring device ( stopwatch ) and under the same circumstances ( first beam on to last beam off )  . to assess dosimetric accuracy , verification measurements were performed using radiographic films and ionization chambers in a homogenous rw3 phantom as described previously [ 7 ] , following the suggestions of rhein et al . 
the imrt approaches as shown in figure 1 show excellent ptv coverage with adequate sparing of the spinal cord , at the expense of a larger non - ptv volume exposed to primary beasimilar to imrt , the vmat approach in figure 1 shows a very good ptv coverage and oar sparing but exposes an even larger volume outside the ptv to primary beam . in table 1 the numeric comparison values of the different approaches are shown . 
 vmat plans ( 785 92 mu ) were delivered with fewer mu than imrt ( imrt - 5b : 843133 ; imrt - 7b : 878102 )  . looking at the treatment time as second efficiency aspect , 3d - pa ( 252 s ) and 3d - wedge ( 887 s ) are , of course , the fastest treatments . 
comparing the modulated techniques the vmat approach is with a mean treatment time of 289 69 s 20% faster than imrt - 5b ( 34872 s ) and 40% faster than imrt - 7b ( 47282 s )  . table 1 also reports the mean percentage coverage of the ptv with 95% of the pd ( c95%pd )  . 
for the 3d approaches , two c95%pd values are reported , one for the plan normalized to 26gy as the median sc dose and the other one normalized to 40gy as the median ptv dose . 
vmat has a slightly larger volume exposed to lower doses ( 525% of prescription dose ( pd ) ) as shown by the dvh for the volume encompassed by the external contour . 
exposure of oars such as lungs , complete sc and sc encompassed by the ptv were similar for the modulated techniques . figure 3 displays the mean dvhs of ptv and spinal cord inside the ptv ( sc ( ptv ) ) with a confidence interval ( cint ) of 95% . 
expectedly , the dvhs for the 3d approaches do not show a large interval range because of the simple beam geometry and the missing modulation which lead to similar results . 
 the cint range for vmat is wider than for the imrt techniques because the forward planning step in ergo + + leads to larger variations among the vmat plans . the differences between the introduced delivery techniques regarding the most relevant comparison parameters are reported with respective significance levels in table 2 . 
the small standard deviations lead to homogeneous results within the delivery techniques and to the majority of differences between techniques being statistically significant despite occasionally small absolute differences . validation of the new treatment paradigm started with assessing the accuracy of plan data transfer from the tps to the r&v syste we found slight variations regarding the strahlenther onkol 2011 no . 
for a - index based on a 5% dose criterion and a 5 mm dta acceptance criterion , 91.333.53% of points were within the acceptance criteria and ( 78.565.34% for 3% / 3mm )  . 
reirridiation of spinal metastates : comparison of treatment techniques discussion the potential benefits of modulated techniques for spinal column tumors were shown in earlier publications [ 5 , 11 , 15 , 22 , 35 ] when spinal cord tolerance was an issue [ 30 ]  . 
mean values standard deviations for homogeneity ( hi40 ) , conformity ( ci ) , number of monitor units ( mu ) , and treatment time ( time ) for the three different techniques . 
reirridiation of spinal metastates : comparison of treatment techniques 3000 2000 1000 3000 2000 1000 100 90 80 70 60 50 40 30 20 10 110 120 130 120 100 80 60 40 20 x - profile [ mm ] x - profile [ mm ] - index ( 3% / 3mm ) - index ( 5% / 5mm ) figure 4 . 
they reported rapid and long - term pain relief with low acute and late toxicity using imrt with a median of 7 incident beams ( range , 614 )  . 
 [ 5 ] examined the efficiency and the possible advantages of single fraction stereotactic radiosurgery ( srs ) using helical tomotherapy in the treatment of a patient with spinal column metastases in a case report . 
the ptv consisted only of the t6 vertebral bone and the treatment time was 13.6mthe long treatment time resulted from the high fraction dose ; thus , a lower fraction dose , e.g. , 2gy , would reduce treatment time accordingly . 
reirridiation of spinal metastates : comparison of treatment techniques for tomotherapy but it is of negligible clinical relevance in the retreatment of spinal lesions that will normally be restricted to lesions < 40cm in length . a first report by wu et al . 
treatment plans were generated with the tps eclipse ( varian medical systems , usa ) in conjunction with a novalis tx linear accelerator with a maximal dose rate of 1000mu / min and a single fraction dose of 16gy . 
similar to our results they found a reduction of mu ( 24% ) and also of treatment time ( 52% ) , interestingly with the two - arc treatment being delivered faster than the one - arc treatment and with fewer mu . 
dosimetric data of their approach , however , are missing because their technique had not been implemented clinically at the time of publication [ 35 ]  . we performed dosimetry with edr2 films and ionization chambers because this method is stable and has been extensively validated . 
early reports indicate their reliability and validity [ 2 , 14 , 27 ] and this approach is currently validated for vmat at our department [ 3 ]  . an important issue for dosimetric accuracy is the distance of the control points ( cp ) during the setup of our vmat plans . 
consequently the dose calculation is performed in a discrete way but the delivery is dynamic , which leads to disagreements in measurements against calculation especially in the low dose region outside the ptv at the border of the phantowe chose a distance between the cp of 5 which is sufficient to create plans of excellent plan quality but led to a lower number of pixels passing the - test with the criteria 3% / 3mm ( 78.565.34% ) than usually expected . 
since figure 3 clearly indicates that this disagreement was only in the low dose region with percentage differences translating into only small absolute differences , this trade - off was accepted to keep treatment times low while still obtaining excellent target coverage and organ at risk sparing . 
continuous monte carlo dose calculation instead of a static approximation would solve this issue . as a positive collateral result , a constant reduction in treatment time and mu while maintaining plan quality of modulated treatments as indicated in this manuscript and by others reduces the concern that secondary tumors might be caused by a high number of mu with modulated techniques [ 12 ]  . 
similarly , potentially detrimental effects of treatment protraction [ 4 , 9 , 16 ] are less likely with these fast modern techniques . conclusion with plan quality being similar to static imrt , vmat is an efficient treatment technique for target volumes with a central avoidance structure . 
the increased treatment efficiency reduces the treatment time without imaging for the patient down to less than 5mthis efficient treatment approach is dosimetrically sound and has successfully been implemented clinically . acknowledgment we gratefully acknowledge the help of markus alber with the implementation of hyperion . 
we are also indebted to roberto pellegrini and manuela duglio of 3d - line / elekta and kevin brown of elekta for the close collaboration during the implementation and initial evaluation of ergo + + and vmat . 
 financial support this work was supported within the framework of a research cooperation agreement between the department of radiation oncology , mannheim university medical center and elekta . original article prolonged survival when temozolomide is added to accelerated radiotherapy for glioblastoma multiforme matthias guckenberger1 , mario mayer1 , mathias buttmann2 , giles h . 
sweeney1 , michael flentje1 background : the goal of this study was to evaluate accelerated radiotherapy with and without temozolomide ( tmz ) for glioblastoma multiforme ( gbm )  . methods : this retrospective analysis evaluated 86patients with histologically proven gbm who were treated with accelerated radiotherapy of 1.8gy twice daily to a total dose of 54gy within 3weeks . 
a total of 41patients received radiotherapy only from 20022005 and 45patients were treated with tmz concomitantly and after radiotherapy from 20052007 . results : median overall survival ( os ) was 12.5months and 2 - year os was 15.4%. 
patient characteristics were well balanced between the two groups except for better performance status ( p = 0.05 ) and higher frequency of retreatment for the first recurrence ( p = 0.02 ) in the tmz group . 
hematological toxicity grade > ii was observed in 2 / 45 patients and 5 / 37 patients during simultaneous radiochemotherapy and adjuvant tmz . conclusion : tmz added to accelerated radiotherapy for gbm resulted in prolonged overall survival with low rates of severe hematological toxicity . key words : glioblastoma multiforme accelerated radiotherapy temozolomide strahlenther onkol 2011 ; 187 : 54854 doi 10.1007 / s00066 - 011 - 2242 - 6 bei akzelerierter bestrahlung des glioblastoma multiforme verlngert temozolomid das gesamtberleben hintergrund : untersucht wurde die behandlung des glioblastoma multiforme ( gbm ) mittels akzelerierter radiotherapie mit und ohne temozolomid - ( tmz - ) chemotherapie . methodik : in dieser retrospektiven auswertung wurden 86 patienten mit histologisch gesichertem gbm erfasst , die mittels akzelerierter strahlentherapie ( zweimal tglich 1 , 8gy bis zu einer gesamtdosis von 54gy in drei wochen ) behandelt wurden . 
im zeitraum 20022005 wurden 41 patienten mit alleiniger strahlentherapie behandelt ; im zeitraum 20052007 erfolgte bei 45 patienten zustzlich zur radiotherapie die simultane und adjuvante gabe von tmz . ergebnisse : das mediane berleben in der gesamtkohorte betrug 12 , 5 monate und das zweijahresberleben 15 , 4% . 
die patientenund behandlungscharakteristika waren zwischen den beiden gruppen ausgeglichen bis auf einen besseren allgemeinzustand ( p = 0 , 05 ) und eine hhere rate an rebehandlung beim ersten rezidiv ( p = 0 , 02 ) in der tmz - gruppe . 
whrend adjuvanter tmz - therapie beobachtet . schlussfolgerungen : tmz verbesserte im kontext der akzelerierten strahlentherapie das gesamtberleben bei gleichzeitig gnstigem toxizittsprofil . schlsselwrter : glioblastoma multiforme akzelerierte radiotherapie temozolomid 1department of radiation oncology , university hospital wrzburg , wrzburg , germany , 2department of neurology , university hospital wrzburg , wrzburg , germany , 3department of neurosurgery , university hospital wrzburg , wrzburg , germany . received : november 24 , 2010 ; accepted : march 18 , 2011 published online : august 18 , 2011 strahlenther onkol 2011 no . 
glioblastoma multiforme ( gbm , grade iv glioma ) accounts for about 1520% of all primary brain tumors and is associated with a devastating prognosis : median survival ranges between 1014 months despite modern multimodality treatment , and long - term survival is rare [ 7 , 12 ]  . postoperative radiotherapy has been the standard of care for many decades with conventionally fractionated irradiation doses of 60gy [ 1 , 15 , 30 ] especially for patients younger than 60 years [ 20 , 22 ]  . 
recently , the addition of systemic chemotherapy with the oral alkylating agent temozolomide ( tmz ) concomitantly and after conventionally fractionated radiotherapy improved overall survival to 27% at 2years and about 10% of the patients experienced long - term survival of more than 5years [ 27 ]  . 
based on this eortc - ncic trial , postoperative radiochemotherapy is the current standard of care , especially for patients with a methylated mgmt promoter [ 11 ]  . a large number of trials evaluated altered fractionation in radiotherapy for gbm , mostly acceleration via twice daily irradiation with or without hyperfractionation . 
however , two prospective randomized phaseiii trials [ 21 , 26 ] and a literature review based on 1 , 414 patients from 21 studies [ 18 ] showed no significant survival improvement by altered fractionation in comparison to conventionally fractionated radiotherapy . accelerated radiotherapy remains a reasonable treatment option for a patient collective with highly limited life expectancy . 
however , the authors did state an uneven distribution of major prognostic factors such as tumor histology and tmz in the analyzed studies . at our institution , accelerated radiotherapy with twice daily fractions of 1.8gy to a total dose of 54gy within 3weeks has been standard care since 2002 . 
it was the aim of this retrospective single - institution study to analyze the effect of tmz added to accelerated radiotherapy . methods between 2002 and 2007 , 86 patients were treated with accelerated radiotherapy for gbm at our institution . 
in contrast to the conventionally fractionated radiotherapy in the eortc - ncic protocol , accelerated radiotherapy resulted in lower overall tmz exposure in our patients . treatment protocol patient and treatment characteristics are summarized in table 1 . 
histological confirmation of gbm was performed in all patients , either by biopsy only ( n = 10 ) or after neurosurgical resection ( n = 76 ) ; complete intraoperative tumor resection was achieved in 28 patients . accelerated radiotherapy was performed in all patients with twice daily single fraction doses of 1.8gy to a total dose of 54gy within 3weeks . 
temozolomide plus accelerated rt for glioblastoma multiforme age <= 60 : n = 37 age > 60 : n = 49 follow - up ( months ) follow - up ( months ) figure 1 . 
gesamtberleben ( os ) und progressionsfreies berleben ( pfs ) fr das gesamtkollektiv . imaging : the resection cavity and residual macroscopic tumor visible on contrast - enhanced ct and mri with a safety margin of 23 cm was defined as the clinical target volume ( ctv ) ; this ctv always included the preoperative t2 - hyperintense region . 
a fractionated boost to the macroscopic tumor was given in 6 patients with a median of 3 fractions and a median total boost dose of 10gy . since 2005 , concomitant chemotherapy with tmz was prescribed in 45 patients at 75 mg / m2 7 days per week during the radiotherapy course . 
nausea and vomiting , which are common adverse effects of tmz , were managed with prophylactic antiemetic medication and prophylactic medication against pneumocystis pneumonia ( trimethoprim 160 mg and sulfamethoxazol 800mg twice weekly )  . adjuvant tmz was given in 37 / 45 patients between 2005 and 2007 . 
adjuvant acnu was prescribed in 8 patients between 2002 and 2005 . after primary treatment was finished , patients were seen at 3 - month intervals and mri imaging was performed at each visit . 
for patients who were unable or unwilling to attend follow - up at our center , the general practitioner and the referring neurologist were contacted for follow - up . statistical analysis patient and treatment characteristics were calculated and compared between the two groups using fishers exact test . 
of the 45 patients in the tmz group , 37 received adjuvant chemotherapy : the median number of adjuvant tmz cycles was 6 ( range , 112 ) and 73% of these patients received 4 cycles . 
at first tumor progression , neurosurgical resection was performed in 14 patients , a second course of rt , performed as fractionated stereotactic rt , was conducted in 6 patients , and chemotherapy was prescribed in 31 patients . 
patient age 60 years at the time of gbm diagnosis , karnofsky performance status better than 80 , and treatment with tmz were associated with significantly improved os in univariate analysis . 
for an interval of < 21 days and 21 days between surgery and start of radiotherapy , the 1 - year pfs rates were 19% and 8% ( figure 5 ) , respectively . 
the influence of tmz treatment on pfs was of borderline significance with 1 - year pfs rates of 21% and 9% for radiotherapy with and without tmz ( figure 6 )  . 
 discussion the median os after accelerated radiotherapy with twice daily fractions of 1.8gy to a total dose of 54gy without temozolomide was 11.3 months and 2 - year os was 5% . 
 [ 19 ] reported 92 patients treated with 60gy delivered in twice daily fractions of 1.5gy ; the median patient age was 59 years but median karnofsky performance status was only 70 . 
accelerated radiotherapy resulted in a median survival and a 2 - year os of 10 months and 5% , respectively . patient characteristics were similar between patients treated with and without tmz in our study except higher rates of re - treatment for the first recurrence and trends towards better performance status and more frequent complete tumor resection in the tmz group . 
einfluss der behandlung mit temozolomid auf das progressionsfreie berleben . therapy in 8 patients from the group not receiving tmz might have masked part of the therapeutic tmz effect . tmz given concomitantly and after accelerated radiotherapy resulted in a median os of 16 months with 2 - year os of 26% . 
it consequently seems that tmz results in a similar improvement of os when added to accelerated radiotherapy compared to conventionally fractionated radiotherapy . the absolute tmz dose given concomitantly to radiotherapy was only half of the dose compared to the eortcncic trial because acceleration of radiotherapy reduced the total irradiation time from 6 weeks to 3 weeks . 
in our study , only 2 / 45 patients developed hematological toxicity grade > ii supporting the hypothesis that dose reduction of tmz concomitant to radiotherapy has the potential to decrease toxicity without compromising oncological outcome . 
however , minimization of toxicity during radiotherapy should nevertheless be of high priority to prevent any interruption of treatment . local treatment of the first gbm recurrence with re - irradiation and / or neurosurgery was of borderline significance to improve os . 
re - irradiation was performed with a total dose of 30 gy in six fractions , and we previously reported overall survival of 7.9 months after re - irradiation with this fractionation schedule [ 28 ]  . 
more recent studies reported the integration of modern targeted chemotherapy into stereotactic re - irradiation and preliminary results are encouraging [ 10 , 17 , 25 ]  . although tmz improved os in our analysis , the influence of tmz on pfs did not reach statistical significance : 1 - year pfs rates were 21% and 9% for radiotherapy with and without tmz , respectively . 
this conflicting result is most likely explained by the difficulty to distinguish between local recurrence / progression and pseudoprogression , which is known to occur in up to 50% of patients [ 23 , 24 ]  . 
the retrospective nature of our analysis and follow - up outside our hospital in some patients may have contributed to this difficult differentiation between true progression and pseudoprogression . besides patient age , the interval between primary surgery and the start of radiotherapy was significantly associated with pfs but not with os . 
this missing influence of the interval between surgery and radiotherapy on os is in agreement with data in the literature for both younger [ 2 , 9 , 16 ] and older patient populations [ 14 ]  . 
however , conflicting data have been reported by other groups [ 6 , 13 ] , suggesting that the waiting time for radiotherapy should be kept short in clinical practice . assuming there are only small or no relevant differences in outcome between conventionally fractionated and accelerated radiotherapy , the patients individual preference for one or the other fractionation schedule becomes more relevant . 
consequently , the patients individual quality - of - live should be considered in the decisionmaking process for the fractionation schedule . conclusions concomitant and adjuvant temozolomide added to accelerated radiotherapy for glioblastoma multiforme resulted in prolonged overall survival with low rates of severe hematological toxicity . 
the improvement of overall survival by adding temozolomide appears to be similar to conventionally fractionated radiotherapy . original article radiosensitization of head and neck cancer cells by the phytochemical agent sulforaphane ulana kotowski1 , gregor heiduschka1 , markus brunner1 , cornelia czembirek2 , christina eder - czembirek2 , rainer schmidt3 , tammer fahim1 , dietmar thurnher1 background and purpose : sulforaphane is a naturally occurring compound found in broccoli and other cruciferous vegetables . 
the aim of this study was to investigate whether sulforaphane could act as a radiosensitizer in head and neck squamous cell carcinoma cell lines . material and methods : four head and neck squamous cell carcinoma cell lines ( i.e. , ( hnscc ) scc9 , scc25 , cal27 , and fadu ) were treated with sulforaphane and subsequently irradiated . 
possible regulation of akt and mcl - 1 was investigated by western blotting . results : sulforaphane and radiation in combination leads to stronger inhibition of cell proliferation and of clonogenic survival than each treatment method alone . 
western blot analysis of akt and mcl - 1 showed no changed expression . conclusion : sulforaphane is a promising agent in the treatment of head and neck cancer due to its antiproliferative and radiosensitizing properties . 
apoptosis is not regulated through akt or the mcl - 1 protein . key words : sulforaphane radiation radiosensitizer head and neck cancer strahlenther onkol 2011 ; 187 : 57580 doi 10.1007 / s00066 - 011 - 2218 - 6 strahlensensibilisierung von kopfund halstumorzellen durch den phytochemischen wirkstoff sulforaphan hintergrund und ziel : sulforaphan ist ein natrlicher , in brokkoli und anderen kreuzbltlern vorkommender wirkstoff . 
eine mgliche regulation von akt und mcl - 1 wurde mittels western blotting untersucht . ergebnisse : sulforaphan und bestrahlung in kombination fhrten zu einer strker inhibierten proliferation und koloniebildung als die einzelnen behandlungsmethoden alledie western - blot - analyse zeigte keine vernderte expression von akt und mcl - 1 . schlussfolgerung : sulforaphan ist aufgrund seiner antiproliferativen und strahlensensibiliserenden eigenschaften ein vielversprechender wirkstoff fr die behandlung von kopfund halstumoren . 
die apoptose wird weder durch akt noch durch mcl - 1 reguliert . schlsselwrter : sulforaphan bestrahlung radiosensitizer kopfund halstumoren introduction cancer is still one of the most frequent causes of death worldwide . 
among the different cancer entities , head and neck squamous cell carcinoma is the sixth most common cancer in the world with more than 600 , 000 deaths every year [ 17 ]  . 
in an on - going process , therapy 1department of otorhinolaryngology , head and neck surgery , medical university of vienna , austria , 2department of cranio - , maxillofacial and oral surgery , medical university of vienna , austria , 3department of radiotherapy and - biology , medical university of vienna , austria . received : september 1 , 2010 : accepted : february 4 , 2011 published online : august 16 , 2011 strahlenther onkol 2011 urban & vogel kotowski u , et al . 
the aim is , therefore , to find new strategies with fewer side effects for the treatment of malignant tumors . the naturally occurring compound sulforaphane ( sfn ) is an isothiocyanate isolated from broccoli and other cruciferous vegetables such as cabbage , cauliflower , and brussels sprouts . 
it inhibits cell growth via induction of cell cycle arrest and apoptosis in several human cancer cell lines , e.g. , breast , colon and prostate cancer [ 10 , 13 , 16 ]  . 
in vitro studies have shown that sulforaphane inhibits phase i biotransformation enzymes which are involved in the activation of carcinogenesis and induces phase ii detoxification enzymes including udpglucuronosyl transferase , gluthatione stransferase , and quinine reductase [ 1 , 4 , 14 ]  . 
recently , a placebo - controlled study showed that oral intake of sfn increases phase ii antioxidant enzymes in the nasal mucosa [ 19 ]  . in view of these findings and in search for new options to treat cancer , this study was performed . 
the aim of this study was to examine the effect of sulforaphane in the four head and neck cell carcinoma cell lines ( hnscc ) scc9 , scc25 , cal27 , and fadu and to investigate whether this agent has a radiosensitizing effect in vitro . 
experiments were carried out at least three independent times and were performed in triplicates . irradiation cells were treated with sulforaphane and subsequently irradiated with a single boost of 2 , 4 , or 8 gy using a conventional radiation source with 250 - kv x - rays . analysis of combination effects to determine the concentrations of the drug to be investigated in the combination study , doseresponse curves were generated with the graphpad 4.0 software from prism ( graphpad software inc . , san diego , ca , usa )  . 
interactions with radiation were calculated with the calcusyn software ( version 2.0 , biosoft , gb ) based on the chou - talalay equation [ 7 ]  . colony - forming assays aliquots of 5 105 cells were seeded in 10 cm culture dishes and incubated for 24 hours . 
then cells were treated with 2.5 m , 5 m , and 10 m sulforaphane and / or irradiated scc9 scc25 fraction aected , fa fraction aected , fa cal27 fadu fraction aected , fa fraction aected , fa figure 3 . 
thereafter , 4 102 of the analyzed , surviving cells were plated in 6 - well plates in drug - free mediu after 2 weeks of incubation , cells were washed three times with pbs , strahlenther onkol 2011 no . 
after 0 , 12 , and 24 hours , cell monolayers were washed twice with cold pbs , frozen with liquid nitrogen , and lysed with lysis buffer as described previously [ 11 ]  . 
bound antigen was visualized with the immun - star western c kit ( bio - rad laboratories , ca , usa ) and detected by chemidoc - it imaging system ( uvp , ca , usa )  . statistical analysis statistical analysis was performed using graph pad 4.0 software by prism ( graphpad software inc . , san diego , ca , usa )  . 
all experiments were repeated at least three times . results effect of sulforaphane and radiation on cell proliferation first , the growth inhibitory effects of sulforaphane and radiation in the hnscc cell lines scc9 , scc25 , cal27 , and fadu were examined . 
 a synergism could be demonstrated in all cell lines ( figure 3 )  . effect of combined treatment on clonogenic survival to determine the long - term effect of treatment on cells , clonogenic assays were performed . 
apoptose wurde nach 48 stunden unter anwendung des annexin - v apoptosis detection kit mittels durchflusszytometrie gemessen . treatment resulted in a synergistic inhibition of colony formation . has been published about the combined application of sulforaphane and radiation therapy . sulforaphane and irradiation induces apoptosis in hnscc because treatment with sulforaphane and radiation led to reduced proliferation of cancer cells , flow cytometry was performed to evaluate the induction of apoptosis . 
in addition , there was no significant difference of apoptosis rates between treatment with the single substance and treatment in combination with radiation . regulation of akt and mcl - 1 regulation of the anti - apoptotic proteins akt and mcl - 1 was analyzed before and after 12 and 24 hours of treatment with 10m sulforaphane and / or 4 gy . 
in all tested cell lines , no altered expression of the two enzymes could be demonstrated ( data not shown )  . discussion in this study , we demonstrated the radiosensitizing effect of the phytochemical agent sulforaphane in head and neck cancer cells . 
our experiments showed that treatment with sulforaphane in combination with radiation leads to a stronger inhibited proliferation than with sulforaphane or radiation alone as demonstrated with proliferation and clonogenic assays . 
this effect has been proven in many tumor entities [ 9 ] ; however , little sulforaphane as a single agent showed a dose dependent inhibition of cell proliferation with an ic50 from 5.037.36 m after 72 hours in our four tested cell lines . 
coincided insofar as that after treatment with sulforaphane apoptosis rates increased up to fourfold . to our knowledge , there is only one publication that investigated the combined treatment of sulforaphane and radiation so far . 
to examine whether there is a regulation of apoptosis on the molecular biological level , we analyzed the expression of the anti - apoptotic proteins mcl - 1 and akt . 
after treatment with sulforaphane , bcl - 2 was downregulated in many cancer cell lines , e.g. , breast cancer cells [ 18 ] , hepatoma cells [ 27 ] , leukemia cells [ 6 ] , prostate cancer cells [ 20 ] , and oral squamous carcinoma cells [ 5 ]  . 
we did , however , not detect an altered expression of mcl - 1 in our head and neck cancer cell lines or a regulation of akt , which is in accordance with the work by yao et al . 
 moreover it is not expensive and easily available . original article extrapulmonary small cell carcinoma : an indication for prophylactic cranial irradiation ? a single center experience martin frh1 , bela kacsir2 , silvia ess3 , thomas cerny1 , regulo rodriguez4 , ludwig plasswilm2 background : information about extrapulmonary small cell carcinoma ( epscc ) is limited and the role of prophylactic cranial irradiation ( pci ) is unknown . patients and methods : disease presentation and outcome of all epscc at our hospital between 1990 and 2009 were retrospectively analyzed . results : of 30 epscc , the male : female ratio was 58% : 42% ; 83% had a performance status of 02 . 
the location of the primary tumor was gastrointestinal ( n = 8 ) , unknown ( 6 ) , gynecological ( 6 ) , urogenital ( 5 ) , and ear nose throat ( 5 )  . 
median survival was 16 months ( 1107 months ) , 18 months ( 1107 months ) , and 9 months ( 0.425 months ) for ls + es , ls , and es , respectively . 
 prognosis was poor in patients with es . key words : extrapulmonary small cell carcinoma prophylactic cranial irradiation strahlenther onkol 2011 ; 187 : 5617 doi 10.1007 / s00066 - 011 - 2222 - x extrapulmonales kleinzelliges karzinom : eine indikation fr eine prophylaktische ganzhirnbestrahlung ? analyse aus einem kompetenzzentrum onkologie hintergrund : unser wissen ber das extrapulmonale kleinzellige karzinom ( ekk ) ist beschrnkt , und der stellenwert der prophylaktischen ganzhirnbestrahlung ist unklar . patienten und methoden : alle an unserem krankenhaus zwischen 1990 und 2009 behandelten patienten mit ekk wurden bezglich krankheitsprsentation und verlauf retrospektiv analysiert . resultate : bei den insgesamt 30 ekk war das mann / frau verhltnis 58% / 42% . 
lokalisation des primrtumors : gastrointestinal ( 8 ) , unbekannt ( 6 ) , gynkologisch ( 6 ) , urogenital ( 5 ) und hals - nasen - ohren - region ( 5 )  . 
das mediane berleben betrug 16 monate ( 1107 monate ) fr alle patienten , 18 monate ( 1107 monate ) fr patienten mit ls und 9 monate ( 0 , 425 monate ) fr patienten mit ms . 
gewichtsverlust von 5% und performance - status von 3 oder 4 waren mit schlechterem gesamtberleben assoziiert ( p < 0 , 001 und p < 0 , 01 )  . schlussfolgerung : die inzidenz von hirnmetastasen war relativ niedrig ( 13% )  . 
diagnosis is made by morphology ( uniform round to spindled - shaped small cells , sparse cytoplasm , high mitotic index , necrotic areas ) and immunohistochemistry ( cd56 ( ncam = neural cell adhesion molecule ) , synaptophysin , chromogranin a , mib - 1 )  . 
extrapulmonary small cell carcinoma ( epscc ) occurs in a variety of sites including the head and neck area , esophagus , stomach , pancreas , gallbladder , uterine cervix , vulva , kidney , urinary bladder , prostate , breast , thyroid , and even in the pleura and central nervous system [ 7 , 6 , 10 , 20 , 25 , 30 , 32 , 33 ]  . 
furthermore , the primary site may remain undetected in as many as 831% of the cases [ 10 , 14 , 13 ]  . whereas sclc has been extensively studied with regard to its natural history and optimal therapy , little is known about epscc . 
a number of studies have indicated that epscc has many features in common with sclc , such as early distant metastases , aggressive behavior , and frequent , but short - lasting response to chemotherapy [ 21 , 31 , 47 ]  . 
for instance , small cell carcinomas or the head and neck or gynecological area appear to have a more favorable prognosis than tumors arising from the gastrointestinal tract [ 7 , 20 , 47 ]  . no randomized trials involving patients with epscc have been performed to date . 
thus , treatment algorithms have historically been extrapolated from trials performed in patients with sclc , and patients with limited - stage ( ls ) epscc are typically treated with chemotherapy plus radiotherapy or even surgery , whereas patients with extensive stage ( es ) are offered palliative chemotherapy only . the use of prophylactic cranial irradiation ( pci ) has been shown to improve survival in patients with ls - sclc if complete or good partial remission to initial chemotherapy and radiotherapy had been achieved [ 2 ]  . 
more recently , a randomized phase iii trial demonstrated a significant reduction of symptomatic brain metastases as well as an absolute survival benefit of 13.8% at 1 year with the use of pci in patients with es - sclc responding to chemotherapy [ 39 ]  . 
 whether pci should also be offered to patients with epscc is unknown . thus , a retrospective analysis of the clinical presentation , therapy , and outcome of patients with epscc at the cantonal hospital of st . 
the secondary objective was to explore overall survival . materials and methods data collection and statistical analysis we retrospectively retrieved all clinical records from 30 patients with epscc who were included in the regional cantonal cancer registry of st . 
study eligibility required pathologically proven epscc with no evidence of pulmonary disease in chest imaging and / or negative bronchoscopy ( except for clinically obvious pulmonary metastases according to the treating physician in 3 patients )  . 
merkel cell tumors were excluded . age , gender , ecog performance status , primary tumor site , stage of the tumor , histologic component , sites of metastases , treatment modalities , and survival data were collected from patient records . 
 clinical responsecomplete response ( cr ) , partial response ( pr ) , stable disease ( sd ) , progressive disease ( pd ) was classified according to world health organization criteria [ 22 ] or response criteria in solid tumors criteria [ 42 ]  . 
patient demographics are summarized in table 1 : 24 patients ( 80% ) had pure high grade small cell carcinoma , 17 patients ( 57% ) had ls , and 13 ( 43% ) es . 
% n = 17 n = 13 male female smoking history never or ex smokersa < 30 packyears > 30 packyears performance statusb 0 2 > 2 weight loss < 5% 5% histology pure small cell carcinoma combined small cell carcinoma metastases at diagnosis brain lung liver adrenal gland lymph nodes peritoneum bone primary tumor site gastrointestinal tract stomach pancreas gall bladder colon rectum anal canal genitourinary bladder prostate head and neck paranasal sinus hypopharynx larynx gynecological site endometrium cervix vagina breast unknown primary 22 1 7 4 5 24 6 0 3 8 2 8 3 2 8 1 1 1 1 3 1 5 3 2 5 3 1 1 6 3 1 1 1 6 7 1 4 9 6 1 1 2 14 3 3 0 0 0 0 2 1 4 3 1 5 3 1 1 5 2 1 1 1 0 aex smokers = stopped > 10 years ago bperformance status according to ecog or who 8 5 0 3 2 4 4 5 8 10 3 0 3 8 2 8 3 2 5 1 1 1 1 1 0 1 0 1 0 0 0 0 1 1 0 0 0 6 location of progression all stages brain lung liver bone adrenal glands 2 lymph nodes limited stage disease extensive stage disease table 3 . 
patients with primary tumors in the stomach , gall bladder , pancreas , colon , and anal canal all presented as es , whereas out of the 3 patients with rectal cancers 2 were ls . 
primary sites predominantly presenting as ls included bladder ( 3 patients ) , head and neck ( 5 patients ) , and gynecological cancers ( 5 patients )  . brain metastases and patterns of relapse none of the patients had clinical evidence of brain metastases at the time of diagnosis . 
one patient with a pancreatic primary tumor had a negative initial brain imaging and relapsed in the adrenal gland and in the brain 22 months and 25 months after first line chemotherapy . 
of the 2 ls patients ( 12% ) who developed brain metastases during follow - up , 1 had a primary tumor in the cervix and relapsed 12 months after combined chemoradiotherapy with a solitary brain metastasis followed by a locoregional relapse in the cervix after 17 months . 
six patients ( 35% ) with ls and primary tumors in the breast , bladder , anal canal , rectum , and in the ear nose throat area underwent primary resection as the single treatment modality . 
gesamtberleben in bezug auf den allgemeinzustand ( who , ecog )  . treatment and survival outcomes whole population median survival for all patients was 16 months ( range , 1107 )  . 
a significant association between survival according to tumor stage ( p < 0.001 ) , weight loss ( p < 0.01 ) , and ecog performance status ( p < 0.01 ) was observed ( figures 13 )  . discussion epscc accounts for less than 0.4% of all cancers [ 9 , 30 , 31 , 36 ]  . 
we examined disease presentation , treatment , and outcomes with a particular focus on the incidence of brain metastasis in order to explore the potential role of pci . pci has recently been adopted as standard clinical practice in patients with lsand es - sclc , based on improved survival strahlenther onkol 2011 no . 
whereas the incidence of brain metastases in lsand es - sclc ranges from 2480% [ 1 , 16 , 26 ] , uncertainty exists about the incidence of brain metastases and , thus , the potential benefit of pci in epscc . 
 most of the series addressing the question of pci in epscc were small and often included less than 20 patients [ 4 , 5 , 24 , 35 , 40 , 46 ]  . 
two recent studies suggested that there may be a subset of patients , e.g. , patients with primary tumors in the head and neck region and patients with urothelial small cell cancer , who potentially benefit from pci [ 37 , 48 ]  . 
however , most studies have reported brain metastases to occur less frequently than in sclc , therefore , questioning the role of pci in epscc [ 4 , 5 , 24 , 35 , 40 , 46 ]  . 
furthermore , we confirm the infrequency of brain involvement at the time of diagnosis in epscc described in previous studies [ 28 ] : none of our patients presented with brain metastases , compared to sclc , where the incidence is estimated to be around 20% . 
one cannot exclude , however , that less frequent initial brain imaging in patients with epscc may potentially overestimate the observed difference in the incidence of brain metastases between sclc and epscc . 
interestingly , median overall survival rates of patients in our study ( i.e. , 16 months in ls and 9 months in es ) were strikingly similar to those reported in patients with sclc [ 12 , 29 , 38 , 47 ] ; and also comparable to other series including patients with epscc [ 27 , 35 ]  . 
patients with gynecologic small cell cancers were reported to have a more favorable prognosis [ 7 , 13 , 17 , 19 ] , whereas patients with small cell cancers of unknown primary site usually have a short survival of only 2.5 months [ 13 ]  . 
 [ 13 ] , we identified stage and performance status as being significantly correlated with survival . as previously described , we observed the best overall survival rates in patients treated with chemotherapy and radiation as part of multimodality treatment [ 10 , 11 , 13 , 27 , 35 , 47 ]  . 
our results confirm previous findings showing high response rates to chemotherapy in patients with es - epssc ( 91% ) [ 5 , 10 , 13 , 17 , 21 , 30 , 35 , 45 ]  . 
however , rapid recurrence determines the poor prognosis of patients with es and novel treatment approaches are desperately needed . radiation doses and schedules have not been prospectively studied in epscc . 
whereas higher radiation doses and hypofractionation have recently shown promising results in patients with non - small cell lung cancer [ 23 , 49 ] , such studies are lacking in epssc . 
furthermore , the role of pet - ct for radiation planning ( and staging ) , which is currently becoming increasingly important in sclc [ 18 ] , has yet to be defined in epscc and should be explored in future studies . we acknowledge that due to the retrospective nature of our analysis , no definitive answers with regard to the treatment , particularly the use of pci , can be given . 
extrapulmonary small cell carcinoma and prophylactic cranial irradiation ? conclusion brain metastases in patients with epscc appear to be less frequent than in sclc and further research needs to be performed to identify a group at risk who potentially benefit from pci . 
this work was supported by the ostschweizerische stiftung fr klinische krebsforschung ( oskk )  . strahlenther onkol 2011 ; 187 : 591603 doi 10.1007 / s00066 - 011 - 1003 - x abstracts 4th langendorff - symposium pros and cons on imaging in radiotherapy september 910 , 2011 freiburg i . 
however , interpretation can be ambiguous , and provide an arbitrary distinction as to the presence of disease that may result from different observers having different thresholds for calling an image positive ( brealey , brjrad 2007 )  . 
beyond interpretation , scan results need to be translated into clinically useful language and this is not trivial either : the words count ( bruzzi , nejm 2006 )  . 
with pet ( - ct ) observer variation of various aspects of scan interpretation has not been well addressed by the imaging community ( wahl , jnm 2009 )  . 
desouza cancer research uk / epsrc cancer imaging centre , institute of cancer research and royal marsden nhs foundation trust , london ( gb ) functional imaging methodologies offer opportunities to characterize tumours by their vascularity , cell density , hypoxic status , metabolism and stiffness . 
 in radiation therapy functional imaging is useful for treatment planning , especially if intensity modulated methods are used for dose painting , in order to deliver the highest doses to the functioning tumour bed . 
the combined effects of chemoradiation , particularly in an era of novel targeted agents where there is a growing demand for proof of mechanism of drug action , may also be monitored using these methods . 
shepherd turku university hospital , turku pet centre and department of oncology and radiotherapy , turku ( fi ) the routine use of pet / ct in treatment planning , emergence of new oncological pet tracers and precision of new radiation therapy devices all call for improvements in the definition of target volumes in 3d pet images . 
limitations arise from the low resolution of pet images , heterogeneity of pathological tissues and the failure of the standardised uptake value ( suv ) to provide an absolute quantity with a universal iso - contour at the surface of any gross tumour volume . 
after reviewing the key approaches taken by contemporary contouring software and emerging research tools , this talk reports on a multi - centre , double - blind experiment comparing the performance of different contouring methods on common data sets . 
methods involved in these experiments represent the state - of - the art , including adaptive thresholding , region growing and watershed algorithms , and the use of higher - level information such as image gradient and mutual information in hybrid images . 
meijer catharina hospital , department of radiotherapy , eindhoven ( nl ) dose escalation of the entire ptv for advanced tumours is regularly greatly hampered by the consequential high dose levels to surrounding organs at risk and local control is often unsatisfactory . 
a sensible boost level the non - uniform dose component can be based on discrete dose levels ( dose painting by contours ) or a continuing varying dose at the voxel level ( dose painting by numbers )  . 
dose painting by contours ( dpbc ) generally uses a threshold to distinguish high - risk subvolumes from low - risk subvolumes and has some pros and cons with respect to the dose painting by numbers ( dpbn ) approach . 
kneschaurek klinikum rechts der isar , klinik und poliklinik fr strahlentherapie und radiologische onkologie , mnchen ( de ) aim : most new linacs have the possibility to perform ct scans in the treatment roo several requirements for image - quality should be fulfilled in order to do adaptive replanning ( art ) on such a ct scan . 
this study compares five different systems of our clinic . methods : we tested : the planning ct scanner somatom emotion 16 ( siemens ) , the on - board imaging ( obi ) of clinac trilogy and clinac dhx ( varian ) , the megavoltage ct ( mvct ) of tomotherapy and the conebeam - ct of oncentra simulix evolution ( nucletron )  . 
in addition we measured the delivered dose in an octavius phantom ( ptw , freiburg )  . results : the resolution of the images depends very much on the imaging system and the chosen modus . 
4 mgy to more than 30 mgy per scan , depending on the system and the chosen quality . conclusions : there are large differences in image quality between the different systems and depending on the chosen modality . 
a constancy check of the different hu - tables is necessary for art on the on - board ct . innovative molecular imaging approaches for radiation oncology : new pet biomarkers and radiomics p . 
combs university hospital of heidelberg , department of radiation oncology , heidelberg ( de ) besides neurosurgery , radiotherapy is the single most active agent for the treatment of primary and secondary tumors of the central nervous system ( cns )  . 
different fractionation schemes , dose levels , combination treatments with chemotherapy and other agents , as well as novel radiation qualities have been evaluated , or are currently under investigation . a main breakthrough was the increase in overall survival ( os ) for primary glioblastomas with the addition of temozolomide . 
novel , molecular - based treatment approaches or concepts stratifiying patients on the basis of molecular markers such as mgmt or idh - 1 , have been reported as promising alternatives , however , prospective studies confirming these benefits still remain to be conducted . modern radiation techniques including stereotactic treatments as fractionated regimens , or as radiosurgery , or intensity - modulated radiotherapy ( imrt ) offer new and effective methods for various clinical situations . 
with the advent of these techniques also second courses of radiotherapy became available , and , for example , re - irradiation of recurrent gliomas could be established as a treatment standard . different beam qualities , such protons , or high - let particle beams , such as carbon ions , are currently under investigation for the treatment of brain tumors . 
therefore , several clinical study protocols focussing on glioblastomas ( cleopatra - trial ) , recurrent gliomas ( cinderella - trial ) or high - risk meningiomas ( marcie - trial ) are currently recruiting patients . 
tsien university of michigan medical center , department of radiation oncology , michigan ( us ) advances in physiologic mr and pet imaging can provide important tools to assess and predict an individual patients response to treatment in glioblastoma ( gb )  . 
schober2 1european institute for molecular imaging ( eimi ) , mnster ( de ) ; 2westfalian - wilhelms - university ( wwu ) , department of nuclear medicine , mnster ( de ) gliomas are the most common primary brain tumors . 
imaging based on magnetic resonance imaging ( mri ) and positron emission tomography ( pet ) plays an important role for primary diagnosis , planning of surgery and irradiation , and in the determination of treatment response and progression free survival ( pfs )  . 
besides l - [ s - methyl - 11c ] - methionine ( met ) and 3 - deoxy - 3 [ 18f ] fluoro - l - thymidine ( flt ) which monitor angiogenesis and proliferation and which are used already in the daily routine , new radiotracers have been developed to target the activated cleavage sites of matrix - metalloproteinases ( mmp ; 18f - br351 )  . 
moreover , to specifically study therapy - induced alterations of transcriptional regulation in gliomas , experimental cell lines have been constructed to enable the assessment of altered p53 and e2f1 expression in experimental glioma models . 
 the overview lecture will cover three aspects of imaging in experimental and clinical gliomas : assessment of response to anti - angiogenic treatment strategies ( met - / fltpet , mri ) first applications of the new mmp - targeted radiotracer 18f - br351 in patients with high - grade gliomas imaging transcriptional regulation of p53 and e2f - 1 by optical imaging techniques 18f - fluoroethyltyrosine - pet imaging in glioblastoma patients for radiotherapy planning and response analysis clinical and experimental evaluation m . 
eble1 , 4 1 department of radiation oncology , rwth aachen university hospital , aachen ( de ) ; 2institute of neuroscience and medicine , forschungszentrum jlich , jlich ( de ) ; 3department of nuclear medicine , rwth aachen university hospital , aachen ( de ) ; 4jlich - aachen research alliance ( jara ) section jara - brain , forschungszentrum jlich , jlich ( de ) purpose : fet - pet - based dose escalation in glioblastoma patients seems promising , but needs a clinical and experimental evaluation , aimed to improve survival , specificity of target volume definition ( tvd ) , and response prediction . methods and materials : in a clinical phase i / ii trial 22 patients had an integrated imrt boost to a dose of 72 gy within the auto - contoured post - surgical fet area , using a tumor brain ratio ( tbr ) of > 1.6. 
relapse pattern considered geographic changes of the tumor bed in fused chronological pet and mri . in an animal study ( tiere , tumorzellinie ) sensitivity and specificity of fetuptake in reactive changes of neuroglia was analyzed histologically / autoradiographically in control and irradiated ( 50 - 150 gy gamma - knife ) rat gliomas . 
welzel university medical center mannheim , university of heidelberg , department of radiation oncology , mannheim ( de ) cognitive dysfunction is a dose - limiting factor of cranial radiotherapy in both children and adults . 
cognitive dysfunction depends on the amount of damage caused to surrounding healthy tissue , the underlying disease ( tumor located in the central nervous system ) , associated pathologic processes ( shunt , hormone deficiency , epilepsy ) , other therapies ( surgery , chemotherapy , corticosteroid therapy , antiepileptic drugs ) , and age . 
 an assessment of neurocognitive dysfunction must involve standardized tests and questionnaires that are sensitive and specific , and take into account that tumors in different locations cause different patterns of cognitive impairment . 
this symposium will discuss the key researches on cognitive functioning after radiotherapy of the brain , and illustrate neurocognitive tests for primary assessment and ongoing evaluation of cognitive side effects after radiotherapy of the brain . a combination of external beam radiotherapy with peptide receptor radionuclide therapy ( prrt ) in irresectable meningeoma m . 
sweeney2 1university hospital wuerzburg , nuclear medicine , wuerzburg ( de ) ; 2university hospital wuerzburg , radiation oncology , wuerzburg ( de ) aim : irresectable or recurring meningeomas are usually treated by external beam radiotherapy ( ebrt )  . 
as it is expected that dose escalation would induce disproportionate high therapeutic efficacy , we combined both treatment modalities to improve the response rate and to reduce the doses delivered to surrounding organs at risk ( oar )  . methods : 10 patients with irresectable meningeoma ( 6 grade i , 3 grade ii , 1 grade iii ) have been treated with a combination of prrt ( lu - 177 - dotatoc or - tate ) and ebrt . 
in all other patients , a stabilization or improvement of tumor - associated symptoms was noted after a median follow - up of 6 months , on imaging no tumor progression were observed . conclusions : these preliminary data suggest that prrt can safely be added to ebrt to increase radiation dose or for a better preservation of oar . 
grosu1 1university hospital freiburg , radiotherapy , freiburg ( de ) ; 2university hospital freiburg , freiburg ( de ) ; 3university hospital freiburg , psychiatry , freiburg ( de ) ; 4university hospital freiburg , neuroradiologie , freiburg ( de ) ; 5university hospital freiburg , nuclear medicine , freiburg ( de ) ; 6university hospital freiburg , neurologie , freiburg ( de ) aim : several studies suggest that hippocampal - sparing whole - brain radiotherapy could reduce radiation - induced neurocognitive decline . 
this study is to evaluate changes in mr imaging with patients treated with or without hippocampal - sparing whole - brain radiotherapy methods : in a prospective randomized trail we will include patients with multiple brain metastases of solid tumors with indication to a whole - brain radiotherapy . 
one group will be treated with a standard whole - brain radiotherapy and boost to the metastases , the other group will receive this therapy in a hippocampal - sparing imrt or rapid arc technique . patients will be examined with mr imaging of the brain before and in a follow - up six weeks , three , nine and eighteen months after radiotherapy . 
 furthermore we will perform some neurocognitive tests at that times results : first results will be presented conclusions : sparing the hippocampus and the perihippocampal region could reduce neurocognitive decline . 
hence , the normal zonal anatomy of the prostate and its relation to adjacent structures can be optimally depicted , and most tumors can be recognized as low signal intensity areas within high signal intensity ( peripheral zone ) prostatic tissue , with a diagnostic accuracy up to 70% . 
it detects about 65% of all prostate cancers , but the sensitivity and negative predictive value increase to over 90% if only clinically significant high grade cancers ( gleason 4 + 3 or higher ) are considered . 
krause university medical centre rostock , department for nuclear medicine , rostock ( de ) pet and pet / ct with radioactively labelled choline derivatives are increasingly used for imaging prostate cancer . 
primary prostate cancer can be detected with only moderate sensitivity using pet and pet / ct using [ 11c ] and [ 18f ] - labeled choline derivates for mainly two reasons : first , the differentiation between benign prostatic hyperplasia , prostatitis , or high - grade intraepithelial neoplasia ( hgpin ) is not always possible . 
as a consequence pet and pet / ct using [ 11c ] and [ 18f ] - labeled choline derivates seem not be useful for the definition of the gross tumour volume in primary prostate cancer . 
at the present time , [ 11c ] - choline pet / ct is not recommended in the primary setting but may be utilized in clinically suspected prostate cancer with repeatedly negative prostate biopsies , in preparation of a focused re - biopsy . 
picchio scientific san raffaele institute , department of nuclear medicine , milan ( it ) in prostate cancer patients , the principal indication of choline pet / ct is represented by the restaging of the disease in case of biochemical relapse . 
 literature suggests that , in these patients , pet may accurately detect the presence of recurrences in lymph nodes , in skeleton , and , although with less accuracy , in prostate bed . 
choline pet / ct is complementary to conventional imaging modalities , but with the advantage of restaging the disease in a single step . it has been demonstrated that choline pet / ct positive detection rate improves with increasing psa values . 
however , in addition to psa levels , psa kinetics and other clinical and pathologic features , such as locally advanced tumour , lymph node involvement at initial staging and age , are independent predictive factors of positive choline pet / ct findings . 
lohr university medical center mannheim , department of radiation oncology , mannheim ( de ) dose escalation , particularly as hypofractionated precision therapy for small tumor volumes or performed with imrt for larger tumors , is improving outcome in several tumor entities . 
soft - tissue based position correction can be performed based on x - rays ( ct - on - rails , cone - beam - ct ( cbct ) ) , ultrasound or electromagnetic signals . 
an overview about online imaging strategies for precision radiotherapy is given , focussing on current use and future potential of cbct ( acceleration of acquisition ) and ultrasound ( tracking )  . advantages and disadvantages of various strategies are discussed . mri patterns of post - prostatectomy recurrence and of its response to salvage radiotherapy using dynamic contrast enhanced ( dce ) mri h . 
grosu1 1universittsklinikum freiburg , klinik fr strahlenheilkunde , freiburg ( de ) ; 2universittsklinikum freiburg , klinik fr urologie , freiburg ( de ) aim : to assess the value of dynamic contrast enhanced magnetic resonance imaging ( dce - mri ) without endorectal coil in detecting local relapse after radical prostatectomy for prostate cancer . methods : 33 patients undergoing dce - mri without endorectal coil before salvage radiotherapy ( rt ) without evidence for metastases were selected retrospectively and evaluated using information of post treatment dce - mri and remission of prostate - specific antigen ( psa ) after rt . 
11 / 33 patients had normal post - prostatectomy mri findings at median psa of 0.22 ng / ml ( mean 0.24 ng / ml ) without changes after salvage rt . 
 thus dce - mri without endorectal coil , which can simultaneously be used for rt planning , seems to be sensitive at low psa - levels and highly specific and may be used for dose escalation on macroscopic sites of local recurrence . original article combined - modality treatment in advanced oral squamous cell carcinoma primary surgery followed by adjuvant concomitant radiochemotherapy matthias kreppel1 , 4 , uta drebber2 , 4 , hans - theodor eich3 , 4 , timo dreiseidler1 , 4 , joachim e . 
zller1 , 4 , rolf - peter mller3 , 4 , martin scheer1 , 4 background : the efficacy of adjuvant radiochemotherapy ( rct ) in patients with advanced stage head and neck carcinoma has been proven in prospective randomized trials . 
we evaluated our experiences with adjuvant concomitant rct in advanced oscc to compare the results with other treatment schemes using adjuvant rct . patients and methods : a total of 183 patients with oscc of uicc stages iiivb were reviewed retrospectively . 
prognostic factors were identified through univariate and multivariate analysis . results : univariate analysis showed a significant impact of t , n , and uicc stage , histopathologic grading , surgical margins , extracaspular spread ( ecs ) , and lymphangiosis carcinomatosa on overall survival ( table 3 )  . 
the differences were significant in multivariate analysis ( p = 0.033 ) ( table 4 )  . conclusion : adjuvant concomitant rct is an effective treatment in patients with advanced stage oscc . 
prospective randomized trials are needed to confirm which patients should be treated with adjuvant rct . key words : oral cancer adjuvant radiochemotherapy prognosis carboplatin strahlenther onkol 2011 ; 187 : 55560 doi 10.1007 / s00066 - 010 - 2245 - 8 multimodale therapie bei fortgeschrittenen plattenepithelkarzinomen der mundhhle mit primrer operation , gefolgt von adjuvanter radiochemotherapie hintergrund : die wirksamkeit der adjuvanten radiochemotherapie bei fortgeschrittenen kopf - hals - karzinomen wurde in prospektiven randomisierten studien nachgewiesen . 
wir haben unsere erfahrungen mit adjuvanter radiochemotherapie bei oralen plattenepithelkarzinomen ausgewertet und mit anderen behandlungsprotokollen mit adjuvanter radiochemotherapie verglichen . methoden : 183 patienten mit oralen plattenepithelkarzinomen der stadien iiivb wurden retrospektiv ausgewertet . 
prognostische faktoren wurden univariat und multivariat analysiert . ergebnisse : univariat zeigte sich ein signifikanter einfluss von t - , nund uicc - klassifikation , von histopathologischen gradings , resektionsrndern , von extrakapsulrem wachstum und lymphangiosis carcinomatosa auf das gesamtberleben ( tabelle 3 )  . 
patienten im stadium iva hatten eine hhere 5 - jahres - berlebensrate ( 42 , 8% ) als patienten im stadium ivb ( 25 , 0% ) ( abbildung 1 )  . 
 die unterschiede waren multivariat signifikant ( p = 0 , 003 ) ( tabelle 4 )  . schlussfolgerung : adjuvante radiochemotherapie ist eine effektive behandlungsmethode bei fortgeschrittenen oralen platten epithelkarzinomen . 
fr 1department for oral and cranio - maxillo and facial plastic surgery , university of cologne , cologne , germany , 2department of pathology , university of cologne , cologne , germany , 3department of radiation oncology , university of cologne , cologne , germany , 4center of integrated oncology ( cio ) colognebonn , cologne and bonn , germany . received : november 25 , 2010 ; accepted : december 1 , 2010 published online : march 14 , 2011 strahlenther onkol 2011 no . 
prospektive randomisierte studien werden bentigt , um zu identifizieren , welche patienten mit einer adjuvanten radiochemotherapie behandelt werden sollen . schlsselwrter : mundhhlenkarzinom adjuvante radiochemotherapie prognose carboplatin introduction approximately 8090% of patients with stage i oral squamous cell carcinoma ( oscc ) are cured with surgery or radiotherapy ( rt ) alone , outcome for patients with advanced stage tumors , however , remains poor , yielding 5 - year survival rates from 4553% [ 15 , 22 , 42 ]  . 
locoregional recurrences and distant metastases are frequent after surgical resection of advanced stage oscc [ 7 ]  . for patients with resectable tumors , the preferred therapy is surgery followed by rt [ 13 ]  . 
although studies have shown that a combination of surgery and adjuvant rt increases overall survival ( os ) and locoregional control [ 17 , 29 , 37 ] , the improvements are modest [ 17 , 29 , 37 , 41 ]  . 
several studies have demonstrated that addition of chemotherapy ( ct ) to adjuvant rt may be beneficial for patients with advanced oscc [ 1 , 2 , 14 , 47 , 49 ]  . 
the rationale to incorporate ct into multimodal treatment schemes are the synergistic effects with rt to improve the tumor cell kill by inhibiting the dna repair in tumor cells , the decrease in tumor mass , the subsequent reoxygenation radiosentizing hypoxic tumor cells , selective toxicity depending on the cell cycle phase and induction of apoptosis [ 5 , 6 , 21 , 46 ]  . in 2004 , two independent prospective randomized trials conducted by the eortc and the rtog tested the use of concurrent radiochemotherapy ( rct ) for advanced head and neck cancer in a postoperative setting , producing level i evidence that postoperative irradiation and high dose cisplatin administered concomitantly resulted in a better disease - free survival and a higher locoregional control after 5 years than postoperative rt alone [ 8 , 15 ]  . 
concomitant application seems to be more successful than a sequential treatment strategy [ 4 , 12 ]  . however , all these prospective trials evaluated tumors from different sites of the head and neck region including oral cavity , larynx , and hypopharynx . 
to the best of our knowledge , there is only one study that compared the results of adjuvant rt and rct in advanced tongue carcinoma but no study that focuses on the effects adjuvant rct in patients with squamous cell carcinoma from all sites of the oral cavity excluding tumors from other sites of the head and neck region [ 24 ]  . the aim of this study was to retrospectively evaluate outcome in advanced oscc with adjuvant concomitant rct using a set of 183 of patients and to compare the results with other treatment schemes using adjuvant rct . patients and methods patients the retrospective study included 183 treatment - naive patients with biopsy proven oscc of advanced stages iiivb , who were treated with curative intent at the department of craniomaxillo - facial surgery at the university of cologne between 2002 and 2006 . 
as this is a retrospective study , an interdisciplinary team of surgeons and radiation oncologists determined the indications for concurrent postoperative rct individually so that some patients with stage ii disease without the risk factors of positive or close margins , lymphangiosis carcinomatosa , extracapsular spread , and poor histopathologic differentiation also received postoperative rct [ 6 , 24 , 50 ]  . treatment all patients were treated with radical surgery including neck dissection and adjuvant concomitant rct , starting 24 weeks after surgery . 
during weeks 1 and 5 of rt , carboplatin was given as a short - term infusion 1 hour before radiation at a dose of 70 mg / m2 / day . statistical analysis the kaplanmeier survival analysis method was used to estimate the events of interest for overall survival ( os , time interval from beginning of primary therapy until death ; patients who were alive at the last date of follow - up were classified as censored observations ) [ 30 ]  . 
kriterien fr die wahl einer adjuvanten radiochemotherapie . all patients with stage iii and iv disease positive resection margins or margins smaller than 5 mm lymphangiosis carcinomatosa extracapsular spread ( ecs ) poor histopathologic differentiation ( g3 ) prognostic impact of patientand tumor - related factors on survival , which were significant in univariate analysis [ 16 ]  . results patient and tumor characteristics table 1 shows patient and tumor characteristics . 
surgery plus radiochemotherapy in advanced oral squamous cell carcinoma ent model , where uicc stage was substituted by t stage and n stage , only t stage ( p = 0.011 ) and n stage ( p = 0.044 ) had a significant impact on os . 
several reports on the effects of neoadjuvant rct on oscc have been published [ 29 , 32 , 38 ] but only one report focuses on primary surgery followed by adjuvant rct in patients with oscc [ 24 ]  . 
 [ 24 ] reported a 3 - year os rate of 59.3% for patients with stage iii and 41.9% for patients with stage iv , which was not split into stages iva and ivb . 
a prospective randomized trial did not show advantages for cisplatin in terms of survival ; however the nephrotoxic and ototoxic side effects were more pronounced than for carboplatin [ 25 ]  . 
univariate analysis revealed that t stage , n stage and uicc stage groping of the 6th edition of the uicc are feasible predictors for os ( p < 0.001 ; table 3 )  . 
a prospective randomized controlled trial concluded that cetuximab in combination with radiotherapy leads to a significantly prolonged progression - free survival in patients with advanced head and neck carcinoma [ 911 ]  . 
the radiation - related toxicity was not substantially increased ; however , the efficacy in comparison to rct has not been tested in a clinical trial [ 3 ]  . we were able to demonstrate that the 6th edition of the uicc stage grouping had a significant impact on os in univariate analysis ( figure 1 ) and multivariate analysis . 
in fact , there are no reliable data so far that show differences in the treatment outcomes between the two nonmetastatic groups stage iva and ivb as quite often patients with stage ivb are not treated with curative intent and , therefore , are excluded from prospective studies [ 35 ]  . 
during the last 10 years , a few studies evaluating the effect of neoadjuvant rct in oscc have been published but none has addressed the issue of possible differences between patients of the uicc stages iva and ivb [ 18 , 22 , 26 , 28 , 32 , 33 ]  . patients in the eortc study who received concurrent adjuvant rct showed a 5 - year os rate of 53% ; patients in the rtog study group reached a 5 - year os of 64% [ 8 , 15 ]  . 
in fact , a recent study demonstrated that there are significant differences in survival and in the prevalence of cervical lymph node metastases among carcinoma from different subsites of the head and neck region and that the risk factors , which justify the use of adjuvant rct instead of rt also may vary [ 27 , 37 ]  . 
finally , oscc are treated quite differently compared to tumors of the larynx and hypopharynx in modern treatment protocols so that aggregate data may not be helpful [ 45 ]  . extracapsular spread and lymphangiosis carcinomatosa were both associated with a significantly decreased 5 - year os in univariate analysis in our study . 
although ecs failed to be a significant prognostic parameter in multivariate analysis , the differences in os were dramatic : patients with ecs had a 5 - year survival rate of 30% compared to 63% for patients without ecs ( p = 0.001 , log rank test )  . 
 [ 50 ] , who described ecs as one of the strongest prognosticators in metastatic oscc . adjuvant chemoradiation in advanced stage squamous cell carcinoma of the oral cavity is a well - established treatment option . 
the poor 5 - year os rate of 25% raises the question whether these patients should be treated in a neaodjuvant setting rather than with primary surgery and adjuvant rct . 
 in addition to clinicopathologic features , reliable biomarkers are needed to determine more precisely , which patient should be treated and with which agent . in the last few years , several molecular and histopathologic biomarkers influencing the prognosis in patients with oscc have been discovered [ 44 ]  . 
one of the most promising biomarkers for survival and lymphatic spread seems to be podoplan podoplanin is expressed frequently in oscc and correlates with cervical lymph node metastases and clinical outcome [ 36 , 51 ]  . 
 exploring the function of biomarkers like podoplanin offers the opportunity to move from a tumor model of temporal determinism to one of biological determinism , as carcinogenesis is not just defined by what stage the patient is in at detection but rather by molecular characteristics of the tumor and the host . original article comparison of radiochemotherapy alone to surgery plus radio ( chemo ) therapy for non - metastatic stage iii / iv squamous cell carcinoma of the head and neck a matched - pair analysis dirk rades1 , thekla meyners1 , nadja kazic2 , amira bajrovic3 , volker rudat4 , steven e . 
this study compared the outcomes of radiochemotherapy alone to surgery followed by radio ( chemo ) therapy ( radiotherapy plus / minus concurrent chemotherapy )  . patients and methods : data from 148 patients treated with radiochemotherapy alone were matched to 148 patients treated with surgery plus radio ( chemo ) therapy . 
on multivariate analyses , tcategory ( p < 0.001 ) , ncategory ( p = 0.004 ) , and hemoglobin level prior to radiotherapy ( p < 0.001 ) were associated with locoregional control . 
histologic grade ( p = 0.045 ) , tcategory ( p < 0.001 ) , ncategory ( p = 0.003 ) , and hemoglobin level prior to radiotherapy ( p < 0.001 ) were associated with metastases - free survival . 
histologic grade ( p = 0.030 ) , ecog performance status ( p = 0.033 ) , tcategory ( p = 0.007 ) , ncategory ( p = 0.024 ) and hemoglobin level before radiotherapy ( p < 0.001 ) were associated with overall survival . conclusion : outcomes of radiochemotherapy alone appeared similar to those of surgery plus radio ( chemo ) therapy . 
randomized trials comparing both treatments for different tumor sites are warranted . key words : head - and - neck cancer surgery radiochemotherapy strahlenther onkol 2011 ; 187 : 5417 doi 10.1007 / s00066 - 011 - 2262 - 2 vergleich von definitiver radiochemotherapie und operation plus radio ( chemo ) therapie beim nicht metastasierten plattenepithelkarzinom der kopf - hals - region im stadium iii / iv eine matched - pair - analyse hintergrund : die standardtherapie von nicht metastasierten plattenepithelkarzinomen der kopf - hals - region im stadium iii / iv variiert weltweit . 
diese studie verglich die behandlungsergebnisse der definitiven radiochemotherapie mit den ergebnissen der operation plus radiotherapie / radiochemotherapie . patienten und methoden : daten von 148 patienten , die eine definitive radiochemotherapie erhielten , wurden mit daten von 148 patienten , die eine operation plus radiotherapie / radiochemotherapie erhielten , in form einer matched - pair - analyse verglichen . 
es mussten die folgenden neun potentiellen prognosefaktoren ( 1 : 1 ) bereinstimmen : alter , geschlecht , allgemeinzustand , tumorlokalisation , grading , t - kategorie , n - kategorie , ajcc - stadium und hmoglobinwert vor strahlentherapie . 
die gruppen wurden hinsichtlich lokoregionaler kontrolle , metastasenfreien berlebens und gesamtberlebens verglichen . 1department of radiation oncology , university of lubeck , germany , 2department of radiation oncology , university of sarajevo , bosnia - herzegovina , 3department of radiation oncology , university of hamburg , germany , 4department of radiation oncology , saad specialist hospital al khobar , saudi arabia , 5department of radiation oncology , mayo clinic , scottsdale , az , usa . received : january 21 , 2011 ; accepted : may 23 , 2011 published online : august 16 , 2011 strahlenther onkol 2011 no . 
surgery plus radio ( chemo ) therapy vs radiochemotherapy alone for scchn ergebnisse : die raten fr die lokoregionale kontrolle nach 1 , 2 und 3 jahren betrugen 81% , 73% und 67% nach operation plus radio ( chemo ) therapie sowie 81% , 74% und 65% nach definitiver radiochemotherapie ( p = 0 , 89 )  . 
die raten fr das metastasenfreie berleben betrugen 86% , 80% und 75% nach operation plus radio ( chemo ) therapie sowie 87% , 80% und 72% nach definitiver radiochemotherapie ( p = 0 , 57 )  . 
die raten fr das gesamtberleben waren 80% , 64% und 63% nach operation plus radio ( chemo ) therapie sowie 83% , 68% und 60% nach definitiver radiochemotherapie ( p = 0 , 96 )  . 
in den multivarianzanalysen waren t - kategorie ( p < 0 , 001 ) , n - kategorie ( p = 0 , 004 ) und hmoglobin vor strahlentherapie ( p < 0 , 001 ) mit der lokoregionalen kontrolle assoziiert , grading ( p = 0 , 045 ) , t - kategorie ( p < 0 , 001 ) , n - kategorie ( p = 0 , 003 ) und hmoglobin vor strahlentherapie ( p < 0 , 001 ) mit dem metastasenfreien berleben sowie grading ( p = 0 , 030 ) , allgemeinzustand ( p = 0 , 033 ) , t - kategorie ( p = 0 , 007 ) , n - kategorie ( p = 0 , 024 ) und hmoglobin vor strahlentherapie ( p < 0 , 001 ) mit dem gesamtberleben . schlussfolgerung : die behandlungsergebnisse nach definitiver radiochemotherapie waren denen nach operation plus radio ( chemo ) therapie vergleichbar . 
die ergebnisse mssen in randomisierten studien fr die unterschiedlichen tumorlokalisationen berprft werden . schlsselwrter : kopf - hals - tumoren operation radiochemotherapie introduction the most appropriate treatment for advanced non - metastatic head and neck cancer is still controversial [ 12 , 16 , 17 , 19 , 20 ]  . 
many centers worldwide favor surgery followed by radio ( chemo ) therapy ( radiotherapy plus / minus concurrent chemotherapy ) , while others recommend radiochemotherapy ( radiotherapy plus concurrent chemotherapy ) alone . 
currently , there is little good quality evidence with respect to comparing surgery plus radio ( chemo ) therapy to radiochemotherapy alone for non - metastatic stage iii / iv squamous cell carcinoma of the head and neck ( scchn )  . the only published randomized trial that has compared surgery plus radiotherapy to concurrent radiochemotherapy failed to demonstrate a significant difference for the effect of treatment [ 15 ]  . 
because national standards ( and physician bias ) favor surgery plus radio ( chemo ) therapy or radiochemotherapy alone , a new randomized trial is difficult to perfor this study was performed as a matched - pair analysis following strict matching criteria . 
patients were matched for nine factors : age ( 56 versus > 56 years ) , gender , eastern cooperative oncology group ( ecog ) performance score ( 01 versus 2 ) , tumor site ( oropharynx versus oral cavity versus hypopharynx versus larynx ) , histologic grade ( g12 versus g3 ) , tcategory ( t12 versus t3 versus t4 ) , ncategory ( n01 versus n2ab versus n2c3 ) , american joint committee of cancer ( ajcc ) stage ( iii versus iv ) , and hemoglobin level before radiotherapy ( 11 versus > 11g / dl )  . 
patient characteristics are given in table 1 . treatment surgery plus radio ( chemo ) therapy surgery was performed as resection of the primary tumor plus bilateral modified radical neck dissection , while microscopically complete resection ( r0 resection ) was achieved in 109 of the 148 patients ( 74% ) , a microscopically residual tumor ( r1 resection ) was found in 39 patients ( 26% )  . 
the total dose delivered to the primary tumor and to the involved lymph nodes was 6070 gy ( median dose : 60 gy ) , depending on the extent of resection . 
the total dose administered to the clinically uninvolved cervical and supraclavicular lymph nodes was 5060 gy . in the surgery group , 69 of 148 patients ( 47% ) received postoperative radiotherapy alone , and 79 patients ( 53% ) with risk factors such as positive surgical margins , extracapsular spread of lymph node metastasis , and lymphovascular or perineural invasion received concurrent radiochemotherapy . 
concurrent chemotherapy consisted of 100 mg / m2 of cisplatin on radiotherapy days 1 , 22 , and 43 ( 19 of 79 patients ) , of 20 mg / m2 of cisplatin on radiotherapy days 15 and 2933 ( 13 patients ) , strahlenther onkol 2011 no . 
the total dose delivered to the primary tumor and to the involved lymph nodes was 6472 gy ( median dose : 70 gy ) , depending on the extent of resection . 
the concurrent chemotherapy consisted of 100 mg / m2 of cisplatin on radiotherapy days 1 , 22 , and 43 ( 38 of 148 patients , 26% ) , of 20 mg / m2 of cisplatin on radiotherapy days 15 and 2933 ( 39 patients , 26% ) , or of 20 mg / m2 of cisplatin plus 600 or 1000 mg / m2 of 5 - fluorouracil on radiotherapy days 15 and 2933 ( 71 patients , 48% )  . 
acute toxicity was evaluated according to common toxicity criteria 2.0 , late toxicity according to rtog criteria [ 2 ]  . statistical considerations locoregional control , metastases - free survival , and overall survival rates were calculated with the kaplanmeier method [ 9 ]  . 
to account for the matched - pair design , a stratified model ( cox regression model with backward stepwise selection of variables using the likelihood ratio test ) was used . 
in a prior study , locoregional after surgery plus radio ( chemo ) therapy was 88% at 1 year , the minimum follow - up time in the present study . 
a total of 296 patients allowed detection of a loss of clinical efficacy of 12.0% with a statistical power of 80% ( level of significance = 5% )  . results on univariate analysis of locoregional control , t category ( p = 0.002 ) , n category ( p < 0.001 ) , and hemoglobin before radiotherapy ( p < 0.001 ) were associated with locoregional control . 
the performance status ( rr 1.02 ; 95% ci 0.611.72 ; p = 0.94 ) was not significant . on univariate analysis of overall survival , performance status ( p = 0.015 ) , histologic grade ( p = 0.013 ) , t category strahlenther onkol 2011 no . 
unvariate analyse fr die lokoregionale kontrolle . at 1 year at 2 years at 3 years surgery + radio ( chemo ) therapy treatment surgery plus radio ( chemo ) therapy radiochemotherapy alone loco - regional control time to recurrence ( months ) surgery + radio ( chemo ) therapy p = 0.57 radiochemotherapy alone metastases - free survival time to metastases ( months ) surgery + radio ( chemo ) therapy p = 0.96 radiochemotherapy alone overall survival time to death ( months ) figure 1 . 
because of investigator biases in terms of therapy , a new randomized trial currently will be difficult to perforinstead of a randomized trial , we performed a matched - pair analysis in a larger series of patients . 
 however , hidden selection biases cannot be excluded because it was retrospective . according to the results of the present study , both treatment regimens resulted in similar locoregional control , metastases - free survival , and overall survival . 
if the 79 patients of the surgery plus radio ( chemo ) therapy group who received both radiotherapy and chemotherapy were compared to the radiochemotherapy alone group , acute toxicity rates were similar . 
in the present study , the actuarial laryngectomyfree survival rate at 3 years was 57% , which is well in the range of 32% to 73% in other studies that included both larynx and hypopharynx cancer patients not receiving surgery [ 4 , 13 ]  . 
in the subgroup analysis of patients with locally advanced larynx or hypopharynx cancer included the tax 324 study , the patients received induction chemotherapy with three courses of either pf ( 100 mg / m2 of cisplatin on day 1 plus 1000 mg / m2 of 5 - fluorouracil on days 15 ) or tpf ( 75 mg / m2 of docetaxel on day 1 plus 100 mg / m2 of cisplatin on day 1 plus 1000 mg / m2 of 5 - fluorouracil on days 15 ) [ 13 ]  . 
in the french gortec 200001 trial , the patients also received induction chemotherapy with three courses of either pf ( 100 mg / m2 of cisplatin on day 1 plus 1000 mg / m2 of 5 - fluorouracil on days 15 ) or tpf ( 75 mg / m2 of docetaxel on day 1 plus 75 mg / m2 of cisplatin on day 1 plus 750 mg / m2 of 5 - fluorouracil on days 15 ) [ 4 ]  . 
in responders , the 3 - year actuarial larynx preservation rates were 73% with tpf and 63% with pf . in our study , locoregional control was significantly associated with tcategory , ncategory , and hemoglobin before radiotherapy . 
metastases - free survival was significantly associated with histologic grade , tcategory , ncategory , and hemoglobin before radiotherapy , and overall survival was significantly associated with histologic grade , performance status , tcategory , ncategory , and hemoglobin level before radiotherapy . 
more recently , a significant impact of the performance status on overall survival ( p < 0.001 ) has been reported in re - analyses of two randomized trials including a total of 289 patients with locally advanced scchn [ 7 ]  . conclusion the results of radiochemotherapy alone appeared similar to those of surgery plus radio ( chemo ) therapy for patients with non - metastatic stage iii / iv scchn . 
however , subgroup analyses with respect to tumor site in a larger cohort of patients and randomized trials comparing both treatment options are warranted . original article feasibility of tomotherapy for graves ' ophthalmopathy dosimetry comparison with conventional radiotherapy nam p . 
krafft1 , paul vos2 , vincent vinh - hung3 , misty ceizyk1 , siyoung jang1 , anand desai1 , dave abraham1 , lars ewell1 , christopher watchman1 , russ hamilton1 , beng - hoey jo1 , ulf karlsson4 , lexie smith - raymond1 purpose : to compare the dosimetry of tomotherapy and the conventional half - beam technique ( hbt ) or non - split beam technique ( nsbt ) for target coverage and radiation dose to the lacrimal glands and lens . patients and methods : a retrospective review of 7 patients with graves ' ophthalmopathy who had radiotherapy because of disease progression on high steroid dose is reported : 3patients were treated with tomotherapy and 4patients with hbt . results : compared to hbt , tomotherapy may provide better target coverage and significant reduction of radiation dose to the lacrimal glands and a higher dose to the lens . 
the nsbt improved target coverage but resulted in significantly higher doses to the lens and lacrimal glands . conclusion : tomotherapy may provide better coverage of the target volume and may be more effective in reducing severe exophthalmos compared to the conventional radiotherapy technique . key words : graves exophthalmos tomotherapy target coverage strahlenther onkol 2011 ; 187 : 56874 doi 10.1007 / s00066 - 011 - 2220 - z wirksamkeit der tomotherapie von ophthalmopathie bei morbus basedow ziel : vergleich zwischen dosimetrie der tomotherapie und der konventionellen half - beam - technik ( hbt ) oder non - split - beamtechnik ( nsbt ) fr die erfassung des zielvolumens und der strahlendosis an trnendrsen und linse . patienten und methoden : eine retrospektive analyse von 7 patienten mit graves ' ophthalmopathie , die wegen progression der erkrankung zur notwendigkeit hochdosierter steroidgabe eine strahlentherapie erhielten . 
3 patienten wurden mit tomotherapie und 4 patienten mit hbt behandelt . ergebnisse : im vergleich zu hbt konnte die tomotherapie bessere erfassung des zielvolumens und signifikante reduktion der strahlendosis an den tranendrsen sowie eine hhere strahlendosis an der linse erreichen . 
nsbt verbesserte die erfassung des zielvolumens , resultierte aber in signifikant hherer strahlendosis an linse und trnendrsen . schlussfolgerung : tomotherapie kann verglichen mit konventioneller strahlentherapietechnik zu besserer erfassung des zielvolumens und wirksamerer verminderung des schweren exophthalmus fhren . schlsselwrter : exophthalmus bei morbus basedow tomotherapie zielvolumen 1department of radiation oncology , university of arizona , tucson , az , usa , 2department of biostatistics , east carolina university , greenville , nc , usa , 3department of radiation oncology , university hospitals of geneva , geneva , switzerland , 4department of radiation oncology , marshfield clinic , marshfield , wi , usa . received : september 22 , 2010 ; accepted : march 18 , 2011 published online : june 28 , 2011 strahlenther onkol 2011 n o . 
feasibility of tomotherapy for graves ' ophthalmopathy introduction materials and methods graves ophthalmopathy is a chronic autoimmune disease that targets the orbital tissues characterized by swelling of the rectus muscles , expansion of the fatty connective tissue in the posterior orbit resulting in proptosis , extraocular muscle dysfunction , and in severe cases compressive optic neuropathy [ 2 , 28 ]  . 
surgical decompression through removal of orbital fat and bone is usually indicated for severe proptosis resulting in exposure keratopathy or visual loss from optic nerve compression [ 7 , 22 ]  . even though the pathophysiology of graves ophthalmopathy is not fully elucidated , current evidence indicates involvement of both t and b lymphocytes in producing the retro - orbital inflammation as rituximab has been demonstrated to reduce significantly proptosis severity [ 31 , 32 ]  . 
thus , a high dose of steroid alone or in combination with radiotherapy has been employed successfully to reduce orbital inflammation and the severity of the ophthalmopathy [ 15 , 18 ]  . 
low dose radiotherapy has been demonstrated to be effective in reducing the severity of graves ophthalmopathy with lasting results and minimal morbidity [ 10 , 15 , 20 , 27 , 33 ]  . 
the effectiveness of radiotherapy may be limited in severe proptosis with a higher percentage of patients developing disease progression or no improvement following radiotherapy [ 10 , 26 ]  . the conventional radiotherapy technique involves two lateral fields with the anterior border of the lateral fields placed at the lateral bony canthus . 
the beam is usually split in half at the center of the beam ( half - beam technique ) to avoid beam divergence to the lens inducing severe cataracts [ 10 , 15 , 20 , 26 , 27 , 33 ]  . 
when the patient has severe proptosis , the half - beam technique ( hbt ) will underdose the soft tissue and extraocular muscles anterior to the radiation fields which may explain the high failure rates following conventional radiotherapy [ 20 ]  . an alternative technique is to cover the target at risk with two lateral fields without the half - beam block ( non - split beam technique )  . 
 thus , a radiotherapy technique that allows irradiation of the orbital soft tissue and muscles without excessive radiation to the organs at risk for radiation damage may improve treatment outcome , while preserving patient quality of life . tomotherapy is a new radiation technology combining intensity - modulated radiotherapy ( imrt ) with daily target imaging that provides effective target coverage , while minimizing the amount of normal tissue irradiated . 
the effectiveness of tomotherapy has been demonstrated in cancers of various anatomic sites with tumor location close to radiosensitive structures [ 11 , 14 , 19 , 24 ]  . 
however , tomotherapy has not been investigated in the treatment graves ophthalmopathy and prompted us to conduct this retrospective study . the medical records of 7 patients undergoing radiotherapy for graves ophthalmopathy at the university of arizona radiation oncology department were retrospectively reviewed following institutional review board ( irb ) approval . 
patients were selected if they had graves ophthalmopathy unresponsive to high steroid dose ( prednisone 30 mg by mouth every day ) and had severe exophthalmos and / or extraocular muscles paralysis resulting in blurring of the vision and / or diplopia . 
four patients were treated with hbt on the elekta sli linear accelerator ( 6 mv photons ) with two lateral radiation beams from february2005 to december2008 and served as historical controls . 
the anterior borders of the fields were set at the lateral bony canthus and the posterior borders were determined by the peripheral target volume ( ptv ) which included the retro - orbital soft tissues and extraocular muscles to avoid marginal miss . 
a total dose of 2 , 000 cgy in 200 cgy / fraction was delivered to the ptv . after 2008 , when the new helical tomotherapy unit ( 6mv photons ) was installed , we treated 3 patients with the intensity - modulated radiotherapy technique . 
the first patient was selected because of severe exophthalmos which would require radiotherapy to both ocular globes in order to include the enlarged extraocular muscles potentially leading to severe keratitis as the patient already had dry eyes prior to radiotherapy . 
following successful treatment completion of the first patient , the imrt technique was selected for the next 2patients . for direct treatment comparison with the conventional radiotherapy technique , the ptv of these last 3 patients was planned retrospectively as if they were to be treated with hbt or nsb to determine the target coverage and radiation dose to the lens and lacrimal glands . we also reviewed target coverage and dose to the lens and lacrimal glands of the first 4patients treated with hbt as historic controls . 
 because of the small number of patients , statistical analysis was not deemed helpful for dose comparison between the three radiotherapy techniques . results we identified 7female patients with graves ophthalmopathy treated at the university of arizona radiation oncology destrahlenther onkol 2011 no . 
table 1 summarizes patient eye disease before treatment , while the target coverage , max lens dose , and mean lacrimal dose between tomotherapy , hbt , and nsb technique are summarized in table 2 . 
igrt : bildgefhrte radiotherapie ; hbt : half - beam - technik . patient treatment diplopia cushingoid symptoms exophthalmos gaze tomotherapy bilateral tomotherapy bilateral tomotherapy bilateral bilateral bilateral dry paresis paresis paralysis paresis paresis paresis affected features duration 24 months 4 weeks 6 weeks 4 weeks 5 months 3 months 8 weeks table 2 . 
 all 3patients treated with tomotherapy had improvement of their exophthalmos after treatment . discussion to our knowledge , this is the first study examining the difference in radiation dose to the target coverage and the tissues at risk of complications between the conventional radiotherapy technique ( hbt and nsb ) and imrt technique based on helical tomotherapy for patients with graves ophthalmopathy . 
 our study highlights the fundamental difference between conventional radiotherapy , which is often based on bone structures in order to set up the treatment fields , and imrt which is based on the delineation of the soft tissues . compared to hbt which is the most common technique for graves ophthalmopathy , tomotherapy provided improved coverage to the target volume and sparing of lacrimal glands from excessive radiation . 
however , maximum lens dose was higher with tomotherapy possibly leading to increased risk of cataract as the threshold for cataract has been estimated at 500 cgy for fractionated radiotherapy [ 1 ]  . 
in addition , because of the precise setup based on ct imaging prior to treatment , radiation dose to the lacrimal gland was significantly less compared to the conventional imrt technique . 
klinische ergebnisse nach strahlentherapie der ophthalmopathie bei morbus basedow . patient treatment exophthalmos gaze diplopia follow - up ( months ) tomotherapy resolved tomotherapy resolved tomotherapy resolved no improvement requiring surgery improved paresis improved paresis resolved paralysis resolved paresis improved paresis improved paresis improved affected intermittent intermittent intermittent intermittent intermittent there is currently no consensus for the treatment of graves ophthalmopathy across different countries . 
however , grade 3 hypolacrimation and cataract formation also increased with radiotherapy dose ( more than 36gy ) suggesting that dose range in the 1520gy may be effective for graves orbital disease without excessive complications provided that target coverage is adequate with parotid gland dose by 3% with the conventional imrt technique for head and neck cancer [ 9 ]  . one can argue that because of the low radiation dose to the orbits ( 20gy ) , damage to the lacrimal glands is unlikely to occur . 
however , in a recent study of 16patients with an orbital pseudotumor treated to a mean orbital dose of 20gy , long - term hypolacrimation was observed in 3patients ( 18.7% ) [ 21 ]  . 
if we take into consideration that patients with graves disease had dry eyes at diagnosis and the additional risk of excessive lacrimal tear evaporation if they had severe proptosis , a major effort should be made to prevent iatrogenic damage to the lacrimal gland in the presence of bilateral exophthalmos . 
for example , patient1 ( figure 1 ) would have had excessive dry eyes and possible exposure keratitis with the conventional radiotherapy if the ptv were to be covered with two non - spitting lateral fields . 
 placing the anterior border of the radiation fields at the lateral bony canthus to spare the lens would have under - dosed the anterior portion of the extraocular muscles potentially resulting in treatment failure . 
in a study of 25 patients with graves ophthalmopathy , the anterior parts of the external eye muscles were not covered in 7patients ( 28% ) treated with the conventional radiotherapy technique . in another study , the lack of radiation coverage of the anterior orbits by the 20gy isodose line was also reported , resulting in the improvement of the proptosis of only 70% , while other parameters such as soft tissue swelling and extraocular muscle dysfunction were 89% and 85% , respectively [ 20 ]  . 
because of the sharp dose fall off associated with tomotherapy , the lacrimal glands may be spared from excessive radiation even though this structure is very close to the target volume . 
the patients exophthalmos improved and resolved following radiotherapy allowing discontinuation of steroid medication . new radiotherapy techniques such as tomotherapy [ 4 ]  . the difference in dose distribution between hbt and tomotherapy may explain why patients with severe exophthalmos at presentation did not respond well to radiotherapy and may explain why radiotherapy may not be effective in randomized trials if a significant portion of these patients were included in the trials [ 6 ]  . 
 [ 23 ] reported 16patients with moderate to severe graves ophthalmopathy ( nospecs scoring system class 3 , 4 , 6 ) who were treated with steroid alone or combined with radiotherapy . 
diplopia and eye motility increased significantly in the irradiated group but there was no improvement in the severity of the proptosis , suggesting that eye motility is independent of the degree of proptosis . 
for example , the european group on graves orbitopathy ( eugogo ) stated that the effective dose range for orbital radiotherapy ranged from 1020gy which differed significantly from the radiotherapy practice of german institutions on the same continent [ 3 ]  . 
 [ 26 ] reported that radiotherapy was effective to reduce soft tissue swelling ( 80% ) and significantly reduced the need for steroids ( 76% ) in 311patients with graves ophthalmopathy following treatment . 
thus , we raised the question why radiotherapy was less effective in reducing proptosis , while improving other parameters ( i.e. , retro - orbital soft tissue and muscles ) following treatment . 
in theory , radiotherapy should be very effective in the treatment of graves eye disease because of the induction of lymphocytes apoptosis even with low radiation dose [ 5 ]  . the radiotherapy fields should cover most of the target volume in order to be effective . 
when we analyze radiation dose distribution with hbt for graves ophthalmopathy reported in the literature , the posterior orbit was well covered with the 2 , 000cgy isodose line but the anterior soft tissue was underdosed [ 10 ]  . 
as the severity of the proptosis increased , a significant portion of the ptv will not receive any radiation , thus , limiting its efficacy to treat the disease with the conventional technique . 
by respecting these strict quality assurance measures , we limited setup errors to less than 1 m the dose to the lacrimal gland would have been significantly higher without image guidance . tomotherapy provides excellent image - guided radiotherapy treatment in addition to imrt dose delivery . 
 our preliminary results suggest that if the ptv coverage to the retro - orbital tissues at risk for inflammation is adequate , low orbital dose ( 20gy ) should be effective to control severe proptosis . 
we emphasize that our hypothesis needs be tested with prospective studies using imrt for graves orbital disease . if we take into account that tomotherapy may decrease radiation dose to the lacrimal glands compared to the conventional radiotherapy technique , this new technique may prevent severe keratitis as proptosis accelerated tear film evaporation , which then leads to ocular surface damage [ 13 ]  . 
tear film hyperosmolarity secondary to evaporation may stimulate several inflammatory cytokines production such as il - 1 and tnf - , which induce ocular surface inflammation [ 17 ]  . 
we argue that tomotherapy should be considered in the treatment of graves ophthalmopathy in case of severe exophthalmos as these patients are at risk for severe keratitis and suboptimal radiotherapy treatment . 
our preliminary results suggest that prospective studies with a large number of patients ( 100 or above ) should be performed with this new imrt technique to assess its efficacy for disease remission , side - effects , late complications , and patient quality of life in graves ophthalmopathy . conclusion intensity - modulated radiotherapy based on helical tomotherapy may provide significant improvement of graves ophthalmopathy because of increased coverage of the tissues at risk compared to the conventional half beam radiotherapy technique . 
this innovative technique should be investigated to assess if it can improve patient quality of life following orbital radiotherapy for graves disease and to possibly , reduce treatment cost associated with decompressive surgery . strahlentherapie und onkologie original article quality of life outcomes in patients with anal cancer after combined radiochemotherapy grit welzel , verena hgele , frederik wenz , sabine kathrin mai1 purpose : to assess self - reported quality of life ( qol ) experienced by anal cancer patients after radiochemotherapy , and to identify patientand disease - related factors associated with qol . patients and methods : a total of 88 patients treated for anal cancer at our institution between 1990 and 2006 were identified from our database . 
 the median follow - up was 36 months ( range , 5137 months )  . results : as for cancer - specific qol , global health qol score ( mean 60.4 ) was similar to the general german population , whereas most of the function and symptom scale scores were considerably lower / higher in anal cancer patients . 
as for site - specific qol , the mean function scale scores ranged from 22.1 ( sexual function ) to 63.2 ( body image ) , and the mean symptom scale scores from 14.7 ( weight loss ) to 69.0 ( stoma - related problems , 4 patients ) and 67.9 ( male sexual dysfunction ) , respectively . 
das mediane follow - up lag bei 36 monaten ( range 5137 ; siehe tabelle 1 )  . ergebnisse : tumorspezifische lq : die globale , gesundheitsbezogene lq ( mittelwert : 60 , 4 ) war vergleichbar mit der der deutschen normalbevlkerung , allerdings waren die meisten funktionsund symptomwerte der analkarzinompatienten im mittel deutlich niedriger / hher . 
die hchsten belastungen wurden in den bereichen rollenfunktion ( 21 , 8 punkte ) , emotionale funktion ( 20 , 7 punkte ) , soziale funktion ( 28 , 9 punkte ) , diarrhoe ( + 34 , 6 punkte ) , und finanzielle belastungen ( + 26 , 9 punkte ; p < 0 , 001 ) gefunden ( siehe abbildung 1 )  . 
organspezifische lq : die mittleren funktionswerte lagen zwischen 22 , 1 ( sexuelle funktion ) und 63 , 2 ( krperbild ) und die mittleren symptomwerte zwischen 14 , 7 ( gewichtsverlust ) und 69 , 0 ( probleme mit dem stoma , 4 patienten ) sowie 67 , 9 ( sexuelle dysfunktion , mnner ; siehe tabelle 2 )  . 
fatigue ( + 18 , 2 punkte ) hatte den strksten einfluss auf die lq . schlussfolgerung : die globale , gesundheitsbezogene lq von analkarzinompatienten entspricht nach kombinierter rcht der der deutschen allgemeinbevlkerung , allerdings gibt es spezifische beeintrchtigungen wie sexuelle dysfunktion , urologische / gastrointestinale beschwerden , finanzielle belastungen , fatigue und negative effekte auf die emotionale und soziale funktionsfhigkeit . schlsselwrter : analkarzinom radiochemotherapie lebensqualitt prdiktoren 1department of radiation oncology , university medical center mannheim , university of heidelberg , mannheim , germany . received : may 3 , 2010 ; accepted : december 1 , 2010 published online : february 21 , 2011 strahlenther onkol 2011 no . 
recent epidemiological data suggest an increase for both sexes , with males having a higher rate of increase , although the etiology is not well understood [ 25 ]  . 
the 5 - year overall survival and local control rates are 7080% , the colostomy - free survival rate is 6570% , and the complete pathologic response rate is about 90% [ 4 , 9 , 16 , 22 , 28 , 29 , 31 , 33 , 42 ]  . 
the treatment is associated with a high rate of acute toxicity and late toxicity including gastrointestinal symptoms and sphincter insufficiency [ 15 , 24 , 28 , 30 ]  . 
little is known , however , about patients self - reported long - term quality of life ( qol ) and the effects of specific disease - related symptoms on qol [ 1 , 11 , 45 ]  . 
the aim of this study was to assess self - reported long - term qol experienced by anal cancer patients after radiochemotherapy and to identify patientand disease - related factors associated with qol . patients and methods a total of 88 patients were treated for anal cancer at our institution between november 1990 and may 2006 . 
it consists of five scales of function ( physical , role , emotional , cognitive , and social ) ; three scales of symptoms ( fatigue , nausea or vomiting , and pain ) ; six single - item scales ( dyspnea , insomnia , appetite loss , constipation , diarrhea , and financial difficulties ) ; and a global health - status scale . 
it consists of four multi - item / single - function scales ( body image , sexual functioning , sexual enjoyment , and future perspective ) , seven multi - item symptom scales ( micturition problems , gastrointestinal tract symptoms , chemotherapy side effects , defecation problems , stoma - related problems , and sexual dysfunction in men or woman ) , and one single symptom item ( weight loss )  . 
clinical late toxicity was scored according to the lent / soma scale [ 39 ]  . of the 69 eligible anal cancer patients , 16 declined to participate because they expected the study to be too stressful , and 1 patient was excluded because the follow - up was too short ( < 5 months )  . 
using the international union against cancer ( uicc ) tnm classification system [ 40 ] , 40 patients had t1 or t2 lesions ; 38 patients presented with n0 ( no regional lymph node metastasis ) disease . 
the reliability ( internal consistency ) was assessed for all scales consisting of two or more items by calculating cronbachs coefficients . to evaluate the differences cancer - specific qol between healthy people and anal cancer patients , previously published reference values on the eortc - c30 questionnaire of the general german population [ 38 ] were compared with the qol data of anal cancer patients included in our study . 
based on work by osoba et al . , the minimum clinically meaningful difference in a qol variable was classified as a difference of > 10 points on the scale [ 32 ]  . 
the investigated patient - related factors comprised the patients age at time of qol assessment ( < 62 years versus > 62 years ) , gender ( male versus female ) , marital status ( married / partner versus single ) , employment status ( employed versus unemployed / retired ) , current tobacco consumption ( yes versus no ) , physical activity ( yes versus no ) , and medical comorbidities ( no comorbidities versus > 1 comorbidities )  . 
due to the small number of unemployed patients ( n = 3 ) , unemployed and retired patients were grouped together for the statistical analyses . all statistical analyses were performed using the statistical package for social sciences software , version 16.0.2 ( spss , chicago , il )  . 
for function scales , higher scores indicate a better level of functioning / quality of life , whereas high scores in the symptom scales represent more problems and mean a reduced quality of life . 
ql : globale lebensqualitt ; pf : krperliche funktion ; rf : rollenfunktion ; ef : emotionale funktion ; cf : kognitive funktion ; sf : soziale funktion ; fa : fatigue ; nv : nausea / emesis ; pa : schmerz ; dy : dyspnoe ; is : insomnie ; ap : inappetenz ; co : obstipation ; di : diarrhoe ; fi : finanzielle belastungen . previously reported [ 2729 ]  . 
since 2004 , 4 patients with positive lymph nodes received two additional cycles of chemotherapy consisting of 1 , 000 mg 5 - fluorouracil / m2 continuous infusion for 96 hours . 
while 45 patients completed therapy exactly according to protocol , 1 patient stopped therapy after the first cycle of chemotherapy at a dose of 43 gy because of toxicity , 1 patient with systemic lupus erythematodes had a treatment interruption of 12 weeks to palliate grade 4 skin toxicity , and 5 patients had modifications in chemotherapy because of hematological side effects . 
all scores of the qlq - c30 and qlq - cr38 were linearly transformed to a 0100 scale , and a high score represented a high level of functioning or high level of symptoms . 
quality of life outcomes after rct for anal cancer variables was assessed by students t test , mannwhitney u test , anova , and kruskalwallis test according to the nature of the variables . 
a two - sided p value of < 0.05 was considered statistically significant . the study was approved by the institutional review board of the medical faculty mannheim , heidelberg university , in accordance with the declaration of helsinki . results compared to previously published reference data of the general german population [ 38 ] , anal cancer patients had a clinically and statistically significant impaired cancer - specific qol on all functioning scales ( p < 0.01 ) with the exception of the global health subscale ( p > 0.05 ) , as shown in figure 1 . 
the functional scale scores ranged from 22.1 points ( sexual functioning ) to 63.2 points ( body image ) and the symptom scale scores from 14.7 points ( weight loss ) to 67.9 points ( male sexual dysfunction ) , and 69.0 points ( stoma - related problems , 4 patients ) , respectively . 
stoma - related problems ( 4 out of 4 patients ) , male sexual dysfunction , and female sexual dysfunction were the most frequently reported symptoms . late toxicity data were available for 46 patients ( table 3 )  . 
the following parameters were independent risk factors for poor qol : t3 / t4 tumor stage , tumor localization at the anal margin or anal canal + anal margin + rectum , radiotherapy dose > 50.4 gy , time since radiotherapy > 36 months , surgical treatment , male gender , being physically inactive , lent / soma gastrointestinal toxicity and lent / soma sphincter insufficiency . 
we assessed the impact of toxicity , patient and disease - related factors on qol , and the importance of disease - related qol symptoms on global qol and its specific dimensions . 
at least 5 months after combined radiochemotherapy when acute treatment effects are expected to have declined , global qol scores in patients with anal cancer were comparable to that of age - adjusted controls . 
many of our patients reported problems in work performance , hobbies or other daily activities , social life , and mood , as well as a negative perspective of the future . 
all three studies had a longer follow - up time than our study , the treatment schedule was different , and in two studies the patients were somewhat older [ 1 , 23 ]  . 
it is well known that younger cancer patients report more psychosocial deficits and suffer from more specific symptoms including body image dissatisfaction and financial problems [ 2 , 19 , 26 , 44 , 46 , 47 ]  . 
chronic fatigue and insomnia are two of the most prevalent problems in cancer patients generally , even years after therapy has been completed [ 5 , 8 , 10 , 17 , 20 , 23 , 36 , 37 ]  . 
nausea / vomiting , appetite loss , constipation , financial difficulties , body image , sexual function , micturition problems , chemotherapy side effects , male sexual dysfunction , and weight loss were not affected by late toxicity , and patientor disease - related factors . patients reporting high symptom scores tended to report lower function scores ( data not shown )  . 
financial burden was the strongest predictor of impaired body image ( r = 0.51 , p < 0.001 ) and sexual function ( r = 0.37 , p < 0.01 ) , and chemotherapyrelated side effects were the strongest predictor of worse sexstrahlenther onkol 2011 no . 
whether these associations are causal is uncertain , but they can not be explained by medical comorbidity . in summary , global qol of anal cancer patients is comparable with that of the general population , but there are specific limitations . 
similar to colorectal cancer patients , anal cancer patients suffer from fatigue , dyspnea , insomnia , constipation , diarrhea , financial difficulties , sexual dysfunction , and a reduction in emotional and social well - being [ 2 ]  . 
since the sample size was small , no bonferroni correction was made as part of the statistical analyses in order to prevent missing a possible correlation ( type 2 error ) , i.e. , p values refer to individual tests rather than to a global test for differences . 
the presented recommendations for various follow - up scenarios for early stage seminoma strongly promote the restrictive use of imaging procedures that utilize ionizing radiation ( especially ct ) , due to its potential to induce secondary malignancies . key words : testicular cancer seminoma follow - up recommendations radiotherapy strahlenther onkol 2011 ; 187 : 15866 doi 10.1007 / s00066 - 010 - 2227 - x interdisziplinre evidenzbasierte empfehlungen fr die nachbeobachtung von patienten mit testikulrem seminom im frhstadium ziel : empfehlungen fr die nachbeobachtung nach primrtherapie von patienten mit testikulrem seminom der klinischen stadien ( cs ) i und iia / b auf basis aktueller publizierter evidenz und ergnzender expertenmeinung . material und methodik : eine interdisziplinre multinationale arbeitsgruppe von urologen , internistischen onkologen und strahlentherapeuten analysierte die publizierten empfehlungen zur nachsorge von patienten mit testikulren keimzellmalignomen unterschiedlicher stadien . 
dabei wurden ausma , frequenz und zeitrume bildgebender verlaufskontrollen bezglich rckfallmuster , risikofaktoren und art der rckfalldetektion untersucht . ergebnisse : aktive surveillance , adjuvante carboplatinoder radiotherapie gelten als gleichwertige optionen beim seminom stadium i mit jeweils unterschiedlichen rckfallraten und - mustern . 
die allermeisten rckflle erfolgen in den ersten 2 ( 6 ) 1department of radiation oncology , university hospital , tbingen , germany , 2department of urology , university hospital , hamburg , germany , 3department of urology , krankenhaus maria - hilf gmbh , krefeld , germany , 4department of oncology , university hospital , marburg , germany , 5department of oncology , university hospital , tbingen , germany , 6department of oncology , kfj - spital , acr - itr vienna / ceaddp and lbi - acr vienna - cto , vienna , austria , 7department of medical oncology , kantonsspital st . 
gallen , switzerland , 8department of hemato - oncology , vivantes klinikum am urban , berlin , germany , 9medical oncology , kantonsspital graubnden , chur , switzerland . received : october 6 , 2010 ; accepted : december 3 , 2010 published online : february 21 , 2011 strahlenther onkol 2011 no . 
damit sollen strahlenexpositionen im rahmen der nachbeobachtung reduziert werden , da diese zur entwicklung von sekundrmalignomen beitragen knnen . schlsselwrter : hodenkrebs seminome nachsorge empfehlungen radiotherapie introduction over recent years , treatment recommendations for patients with testicular cancer have been published by several organizations / societies [ 1 , 24 , 2931 , 34 , 35 , 43 ]  . 
even in advanced stages and / or recurrent disease , relapse rates and mortality have been reduced significantly within the last 15 years due to the stringent application of the standard chemotherapy followed by resection of residual disease [ 6 ]  . furthermore , as a result of the high cure rates , data regarding treatment - associated late sequelae are available . 
thus , international follow - up guidance is unclear and differs widely , mainly regarding frequency , extent , and modality of the imaging procedures . at least , one recent publication documented that evidence - based follow - up could be achieved based on the knowledge of different risk factors and patterns of recurrence grouping patients into risk categories [ 38 ]  . 
an ideal follow - up schedule identifies a recurrence early without causing harm by unnecessary radiation exposure in these long - term survivors who are mainly young of age at the time of initial treatment . the excessive risk of the radiation exposure due to repeated computed tomography ( ct ) has been calculated [ 4 , 5 ]  . 
calculations have been published showing that a single ct of the abdomen performed in a 20 - year - old male leads to a radiation induced cancer in 1 of 660 cases . 
although these calculations are discussed controversially , it is of crucial importance that every effort should be made to minimize the radiation burden . apart from tumor relapse , and at least equally important , follow - up schedules should reveal long - term side effects of radiotherapy as well as chemotherapy [ 10 , 18 , 42 ]  . the following recommendations should help to coordinate the follow - up procedures and decisions in daily clinical practice . 
the grading of the recommendations according to the guidelines defined by the american society of clinical oncology is given in the text in parentheses , written in italics [ 2 ]  . classification of follow - up groups follow - up schedules are determined by the stage of disease and the choice of primary management . 
this is most obvious in the case of stage i disease where the risk of recurrence differs substantially between patients who have received adjuvant treatment and those who have decided for an active surveillance strategy . 
serum tumor markers hcg ( human chorionic gonadotropin ) and ldh ( lactate dehydrogenase ) might be controlled at every visit ; afp ( - fetoprotein ) once after orchidectomy . 
if possible , the tumor markers should always be checked in the same qualified laboratory . choice of imaging modality evidence ct scans of the trunk have to be performed for staging purposes at the time of diagnosis of a testicular cancer and best before orchidectomy to rule out reactive retroperitoneal lymph node enlargements due to surgery . there are only few publications focusing on the modalities of imaging in the follow - up of testicular cancers [ 9 , 11 , 15 , 21 , 41 ]  . 
it is , therefore , generally recommended only to scan the pelvis if the above mentioned risk factors are present . whether a ct of the thorax is always necessary or can be sufficiently replaced by chest x - rays for follow - up purposes in patients with stage i testicular cancer has been questioned recently [ 9 , 11 , 21 ]  . 
in retrospective analyses , tumor recurrence was diagnosed by elevated tumor markers , abdominal disease , or metastases visible in conventional imaging in all cases ( level iii , b ) [ 9 , 21 ]  . 
therefore we recommend chest x - ray instead of chest ct for routine follow - up of these patients . whether ultrasound could replace a ct scan of the abdomen for the evaluation of the retroperitoneum is under intensive debate . 
ultrasound appears to have similar sensitivity and specificity for detection of retroperitoneal metastases in patients with testicular cancer as ct of the abdomen ( level iii , b ) [ 13 , 27 ]  . 
whenever the main aim is to examine the presence of a larger retroperitoneal mass ( e.g. , growing teratoma ) , we recommend an ultrasound of the abdomen , mainly for the purpose of eliminating additional risk of radiation exposure . 
 if either the physician is not skilled enough or the patient is not suitable for ultrasound , a ct scan of the abdomen is the better choice . another issue for follow - up addresses the clinically appropriate imaging procedure , in particular , whether magnetic resonance imaging ( mri ) should replace ct in order to reduce radiation exposure [ 15 ]  . 
trials evaluating the use of mri are ongoing . 18fluorodeoxy - d - glucose positron emission tomography ( fdg - pet ) and fdg - pet - ct , respectively , play only limited roles in the follow - up of seminoma patients . 
finally , all patients should be instructed and encouraged to perform regular self - examination of the remaining testis . follow - up for long - term toxicity patients who have been cured with radiotherapy or chemotherapy are at risk for late toxicity [ 18 , 22 , 28 , 36 , 39 ]  . 
regular check - up of blood pressure , weight , body mass index ( bmi ) as well as blood lipids and fasting blood sugar levels are recommended at baseline and annually . 
in case of signs or symptoms of testosterone deficiency , substitution has to be discussed . it is very important that patients are advised to adapt their lifestyle to control additional risk factors ( e.g. , non - smoking , weight control , regular physical exercise )  . 
 [ 26 ] observed that recurrence in 2 , 466 patients after adjuvant treatment for stage i seminoma very rarely occurred later than 3 years ( 0.2% of the patients )  . 
moreover , they found that 7 of 11 recurrences were detected by scheduled abdominal cts ( at 12 and 24 months , respectively ) after adjuvant carboplat of note , ct of the chest and pelvis can safely be omitted in this patient group as they did not contribute to the detection of recurrences ( level iii , b ; table 1 ) [ 26 ]  . 
therefore , in these patients long - term sequelae from each of the specific therapeutic modalities have to be considered . whereas in patients undergoing radiotherapy , acute radiotoxicities are low due to reductions of irradiated target volumes and total doses , long - term effects such as the induction of secondary malignancies have to be considered . 
in patients receiving adjuvant or salvage chemotherapy , acute toxicities ( e.g. , acute organ toxicities , nausea , vomiting , and fatigue ) are usually manageable , but can be severe or even life - threatening and occur at a substantially higher rate compared to radiotherapy . 
patients undergoing active surveillance lack acute and late organ toxicities , but psychological distress might have a substantial impact on quality of life and has to be monitored as a higher proportion of patients on active surveillance may need professional support [ 22 , 28 , 36 , 38 , 39 ]  . cumulative radiation doses from follow - up ct scans are significant with every treatment modality and have to be kept in check , but are highest in patients under surveillance who need the closest monitoring . the current recommendations were developed by an interdisciplinary working group over the course of 2 years and finally consented [ 6 ]  . 
european consensus conference on diagnosis and treatment of germ cell cancer : a report of the second meeting of the european germ cell cancer consensus group ( egcccg )  . 
evidence - based guidelines for strahlentherapie und onkologie original article healing of late endoscopic changes in the rectum between 12 and 65 months after external beam radiotherapy gregor goldner1 , richard ptter1 , alexander kranz1 , alexandra bluhm1 , wolfgang drr1 , 2 purpose : to evaluate the time course of late rectal mucosal changes after prostate cancer radiotherapy ( rt )  . patients and materials : a rectosigmoidoscopy was performed at 12 , 24 , and 65 months after rt in 20 patients . 
rectal mucosal changes ( telangiectasia , congested mucosa , ulceration , stricture , and necrosis ) were scored and documented according to the vienna rectoscopy score ( vrs , score 03 )  . results : vrs of 0 and 3 , were found in 20% of patients ( n = 4 ) and 5% of patients ( n = 1 ) , respectively at all time points . 
a shift of the vrs from 2 to 1 was found with incidence rates of 60% at 12 months and 20% at 65 months , which is equivalent to an improvement rate of 67% . 
hence , the usual reports of complication rates overestimate the proportion of patients presenting with side effects of certain grades . key words : prostate cancer radiotherapy rectum endoscopy telangiectasia strahlenther onkol 2011 ; 187 : 2025 doi 10.1007 / s00066 - 010 - 2211 - 5 heilung von schleimhautvernderungen im rektum zwischen 12 und 65 monaten nach externer strahlentherapie hintergrund : wie entwickeln sich schleimhautvernderungen am rektum nach radiotherapie des prostatakarzinoms im zeitlichen verlauf ? patienten und material : bei 20 patienten wurde 12 , 24 und 65 monate nach rt eine rektosigmoidoskopie durchgefhrt . 
rektale schleimhautvernderungen wurden bewertet und entsprechend dem wiener rektoskopie - score ( vrs , score 03 ) graduiert . ergebnisse : ein vrs - score 0 und - score 3 wurde bei 20% ( 4 patienten ) und bei 5% ( 1 patient ) zu jedem zeitpunkt nach rt erhoben . 
eine verlagerung von vrs - score 2 zu - score 1 mit einer inzidenzrate von 60% nach 12 monaten und 20% nach 65 monaten wurde nachgewiesen , entsprechend einer verbesserung bei 67% der patienten ( tabelle 2 )  . 
durch diese art der prsentation wird der anteil an patienten mit einem bestimmten schweregrad von nebenwirkungen oftmals berschtzt . schlsselwrter : prostatakarzinom radiotherapie rektum endoskopie teleangiektasien 1department of radiotherapy and radiobiology , vienna general hospital , university of vienna medical school , vienna , austria , 2department of radiotherapy and radiation oncology , medical faculty carl gustav carus , university of technology dresden , germany . received : september 24 , 2010 ; accepted : october 6 , 2010 published online : february 24 , 2011 strahlenther onkol 2011 no . 
late endoscopic changes in the rectum after external beam rt introduction chronic radiation - induced proctitis occurs in 520% [ 27 , 911 , 16 , 17 ] of patients treated with three - dimensional ( 3d ) conformal radiotherapy ( 3dcrt ) of the pelvis ; the incidence depends on reporting by the patients and diagnostic procedures . 
 other mucosal lesions , such as congested mucosa , ulcerations , strictures , or necrosis and their precise localization are not considered . finally , little data about the development of mucosal changes over time after rt are available . 
for patients who were treated with a total dose of 74 gy , the dorsal safety margin was reduced to 5 mm for the application of the first 8 gy . 
intermediateand high - risk group patients also received androgen deprivation . to enable the evaluation of rectal mucosal changes caused by radiotherapy , a voluntary rectosigmoidoscopy was arranged before radiotherapy as well as 12 , 24 , and 60 months after the conclusion of therapy . 
internal medicine specialists for gastroenterology performed all rectosigmoidoscopies . to reduce the interobserver variability and to locate endoscopic findings , the examination and graduation of macroscopic mucosal changes was performed as published by our group in 2001 [ 17 ]  . 
in brief , the rectum was divided into 12 parts : an anorectal ( 04 cm ) , a distal ( 48 cm ) , a medium ( 812 cm ) , and a proximal ( > 12 cm ) area each with an anterior , lateral , and posterior section . 
 telangiectasia : grade 0 : none ; grade 1 : single telangiectasia ; grade 2 : multiple nonconfluent telangiectasia ; grade 3 : multiple confluent telangiectasia congested mucosa : grade 0 : none ; grade 1 : focal reddening of the mucosa combined with edematous mucosa ; grade 2 : diffuse nonconfluent reddening of the mucosa combined with edematous mucosa ; grade 3 : diffuse confluent reddening of the mucosa combined with edematous mucosa ulceration : grade 0 : none ; grade 1 : microulceration with or without superficial < 1 cm2 ; grade 2 : superficial > 1 cm2 ; grade 3 : deep ulceration ; grade 4 : fistula , perforation stricture : grade 0 : none ; grade 1 : more than two - thirds of the regular diameter ; grade 2 : one - third to two - third of the regular diameter ; grade 3 : less than one - third of the regular diameter ; grade 4 : complete obstruction necrosis : grade 0 : none ; grade 1 : necrosis types of mucosal reactions were then subsumed according to the vienna rectoscopy score ( score 05 ; table 1 )  . 
a total dose of 70 gy was applied in 6 low - risk patients and in 6 intermediate - risk patients , while 8 high - risk patients received a total dose of 74 gy . 
additional hormonal therapy was given for a median period of 6 months for the intermediateand high - risk group patients . prior to radiotherapy , 1 patient presented with single telangiectasia at the lateral wall corresponding to a vrs of 1 , while the remaining 19 patients ( 95% ) showed no signs of macroscopic rectal mucosal changes , corresponding to a vrs of 0 . 
 endoscopy after a median time of 12 ( range , 916 ) months after rt showed mucosal alterations of vrs 0 , 1 , 2 , and 3 in 20% , 15% , 60% , and 5% of the patients , respectively . 
 : verbesserung des vrs 65 monate nach rt ; : keine vernderung des vrs 65 monate nach rt . patient prior to rt 12 months 24 months 65 months 12 / 24 months to 65 months ectasias were found in 75% of the patients with a peak in the distal area at the anterior rectal wall section , corresponding to the high - dose region . 
after a median time of 24 ( range , 1736 ) months after radiotherapy , 20% , 40% , 35% , and 5% of the patients were classified as having a vrs of 0 , 1 , 2 , and 3 , respectively . 
 endoscopic examination after a median time of 65 ( range , 5779 ) months after rt showed mucosal changes corresponding to vrs grades 0 , 1 , 2 , and 3 in 20% , 55% , 20% , and 5% of the patients , respectively . 
 comparisons between 12 or 24 months and 65 months after radiotherapy showed a significant improvement ( wilcoxon signed - rank test , p < 0.001 ) in 66% of patients according to the vrs ( table 2 )  . radiation - induced chronic proctopathy is still a common late side - effect of radiotherapy of the pelvis . 
 [ 12 ] performed a median of four ( range , 26 ) sigmoidoscopies within a median of 27 months ( range , 1540 ) in 20 patients treated for prostate cancer up to a total dose of 65 gy . 
single telangiectasia was found in 3 patients ( 15% ) , multiple nonconfluent telangiectasias were detected in 12 patients ( 60% ) , and only 1 patient ( 5% ) was found to have multiple confluent telangiectasias . 
we were able to demonstrate that percentages of patients with high vrs ( vrs > 1 ) decrease after radiotherapy from 65% ( 12 months after rt ) to 40% ( 24 months after rt ) and finally to 25% ( 65 months after rt )  . 
the kaplanmeier estimate will be an overestimate of the actual proportion of these side effects , based on improvement of the telangiectasias and consequent rectal bleeding with time after radiotherapy . 
late endoscopic changes in the rectum after external beam rt strahlentherapie und onkologie editorial new electronic manuscript submission and tracking system strahlentherapie und onkologie is pleased to announce the launch of its new electronic manuscript submission and tracking systethe system will begin 1 march 2011 . 
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limitations of creatinine as marker for the glomerular filtration rate ( gfr ) led to the proposal of cystatin c as a more accurate biomarker especially in mild renal insufficiency or in patients with low muscle mass . 
intraclass correlation coefficients were calculated between the reference method ( 51 ) cr - edta clearance and estimated gfr by creatinine clearance and equations based on creatinine ( cockroft - gault , modification of diet in renal disease ( mdrd ) , wright ) or cystatin c ( larsson , dade - behring , hoek )  . 
in addition , sensitivity and specificity to discriminate gfr > 60 ml / min / 1.73 m2 were evaluated by receiver operating characteristic curve ( roc )  . results : the highest correlation coefficients were found for the cystatin c - based estimates in comparison with creatinine - based estimates or creatinine clearance , even though bland - altman plots revealed gfr overestimation for all equations tested . 
roc analyses revealed the highest auc to predict a gfr > 60 ml / min / 1.73 m2 for the creatininebased wright formula , closely followed by the mdrd formula and cystatin c - based equations of larsson , dade - behring , and hoek . conclusion : cystatin c - based gfr estimates showed the overall strongest correlation to the reference method . 
thus , we recommend cystatin c for gfr estimation in hnc patients as an alternative method to the estimated creatinine clearance in clinical practice . key words : glomerular filtration rate cystatin c estimated creatinine clearance strahlenther onkol 2011 ; 187 : 191201 doi 10.1007 / s00066 - 010 - 2203 - 5 cystatin c ein schneller und zuverlssiger marker zur bestimmung der glomerulren filtrationsrate vor einer cisplatinhaltigen chemotherapie bei patienten mit kopf - hals - tumoren zielsetzung : bei tumorpatienten ist die exakte bestimmung der nierenfunktion eine wichtige voraussetzung fr die individuelle therapieplanung . 
die aussagefhigkeit des serumkreatinins als marker der glomerulren filtrationsrate ( gfr ) ist jedoch limitiert aufgrund seiner abhngigkeit von der muskelmasse sowie fehlendem anstieg der serumkonzentration bei einer gfr > 60 ml / aauthors contributed equally to this work . 1department of radiation therapy and radiation oncology , university of dsseldorf , dsseldorf , germany , 2department of nephrology , university of dsseldorf , dsseldorf , germany , 3department of clinical chemistry , university of ulm , ulm , germany , 4department of surgery , university of dsseldorf , dsseldorf , germany ( current affiliation : department of general , visceral and trauma surgery , essen - sd hospital , essen ) 5maastro clinic , radiation oncology , maastricht , the netherlands , 6department of nuclear medicine , university of dsseldorf , dsseldorf , germany , 7department of clinical chemistry and laboratory diagnostics , university of dsseldorf , dsseldorf , germany , 8department of otorhinolaryngology , head and neck surgery , university of essen , essen , germany , 9department of anesthesiology , state university of new york at buffalo , buffalo , ny , usa . received : july 9 , 2010 ; accepted : november 15 , 2010 published online : february 24 , 2011 strahlenther onkol 2011 no . 
in der vorliegenden studie wurde die przision von cystatin - c - basierten sowie kreatininbasierten formeln zur berechung der gfr in kopf - hals - tumorpatienten verglichen . patienten und methodik : die studienkohorte bestand aus 52 kopf - hals - tumorpatienten ( gfr 37105 ml / min / 1 , 73 m2 ) sowie 17 patienten mit bekannter niereninsuffizienz stadium 35 ( gfr 1060 ml / min / 1 , 73 m2 )  . 
es wurde der intra - class - correlation factor berechnet zwischen der referenzmethode ( 51 ) cr - edta - clearance und der kreatinin - clearance , den kreatinin - basierten formeln ( cockroft - gault , modified diet in renal disease , wright ) und den cystatin - c - basierten formeln ( larsson , dade - behring , hoek ) zur gfr - berechnung . 
zustzlich ermittelten wir sensitivitt und spezifitt der verschiedenen clearance - bestimmungen zur erkennung einer gfr > 60 ml / min / 1 , 73 m2 mittels receiver operating characteristic curve ( roc )  . ergebnisse : die beste korrelation zur referenzmethode wurde fr die cystatin - c - basierten formeln zur gfr - bestimmung im vergleich zu kreatinin - basierten formeln oder der kreatinin - clearance ermittelt . 
da eine gfr < 60 ml / min / 1 , 73 m2 hufig als grenze angesehen wird zur durchfhrung einer chemotherapie , ermittelten wir die przision , mit der die verschiedenen gfrbestimmungen dies fr den einzelnen voraussagen konnten . 
bei der roc - analyse zeigte die kreatinin - basierte formel nach wright die hchste area under the curve , dicht gefolgt von der modified - diet - in - renal - disease - formel und den cystatin - c - basierten formeln nach larsson , dade - behring und hoek . schlssfolgerung : die cystatin - c - basierten formeln zur gfr - berechnung zeigten insgesamt die beste przision und korrelation zur referenzmethode in kopf - hals - tumorpatienten . 
daher empfehlen wir cystatin - c - basierte formeln zur gfr - berechnung im klinischen alltag bei diesen patienten . schlsselwrter : glomerulre filtrationsrate cystatin c cystatin - c - basierte formeln introduction recently , two randomized trials from the radiation therapy oncology group and the european organization for research and therapy of cancer for head and neck cancer patients ( hnc ) revealed an improved disease - free survival in patients receiving a platinum - based chemotherapy [ 5 ]  . 
the nephrotoxicity of cisplatin is dose - related , cumulative , and depends on the extent of diuresis and the preexisting renal dysfunction [ 10 , 21 , 2326 , 33 ]  . 
 therefore , an accurate estimation of renal function is needed for safe and effective use of this chemotherapeutic agent to prohibit toxic side effects [ 2 , 33 ]  . the glomerular filtration rate ( gfr ) is essential for the clinical assessment of renal function . 
an optimal gfr biomarker should be constantly produced at the same level , independent of age , body or muscle mass , and exclusively eliminated by glomerular filtration without tubular secretion or reabsorption . 
however , because of costs and inconvenience , plasma creatinine , creatinine clearance ( ecc ) , and creatinine - based estimation formulas are most commonly used to measure renal function [ 7 , 8 , 13 , 14 , 30 , 31 ]  . creatinine is of limited value in early renal insufficiency since plasma levels only rise if the gfr decreases below 60 ml / min / 1.73 as it is generated by muscle metabolism , plasma levels are dependent on muscle mass , age , and gender . 
the measurement of ecc is a more accurate assessment of glomerular function , but is hampered by its requirement of a timed and definitive urine collection and determination of its exact volume [ 8 , 13 , 31 ]  . 
the modification of diet in renal disease ( mdrd ) formula was generated from a study with 1 , 628 nondiabetic patients with chronic renal disease with reference to the renal clearance of iothalamate and showed a more accurate measurement when compared to the cockroft - gault formula . 
its prediction of gfr appears accurate in the range 2060 ml / min / 1.73 m , but is less precise in mild renal insufficiency and is limited to patients older than 18 years who suffer from chronic renal insufficiency [ 20 ]  . 
 [ 34 ] published four formulas in 2001 to predict gfr in cancer patients , which produced estimates less biased than the formulas from cockcroft - gault and jelliffe . cystatin c , an endogenous 13 kda protein of the cystatin superfamily of cysteine proteinase inhibitors , is expressed at a constant rate in all nucleated cells . 
a recent study showed measurement of cystatin c to be superior to creatinine for the detection of renal function deterioration in cancer patients treated with cisplatin - based regiments [ 1 , 28 ]  . 
cystatin c : a biomarker in nasopharyngeal cancer accurate in the elderly , diabetics , and young children , cystatin c - based gfr equations overestimate renal function in transplant patients . 
furthermore , the bias of cystatin c - based gfr estimation varied among patients with native kidney disease , transplant patients with an immunosuppressive therapy , and potential kidney donors , suggesting factors other than gfr to influence cystatin c levels . 
most recently , stevens reported cystatin c levels to be affected by inflammation , high leukocyte counts , increased c - reactive protein , lower serum albumin , age , body mass index , overweight , and proteinuria [ 29 ]  . 
this could be of crucial relevance in hnc patients , which often present with cachexia . thus , the aim of the present study was to determine the best method for gfr estimation in hnc patients in order to discriminate for the cut - off of 60 ml / min / 1.73 therefore , we measured plasma concentrations of creatinine and cystatin c as well as ecc in hnc patients with and without metastases , before and during combined chemoradiation with cisplatdifferent gfr equations being either based on creatinine ( mdrd , cockroft - gault , wright ) or cystatine c ( hoek , larrson , dade - behring ) were compared with gfr measured by the gold standard ( 51 ) cr - edta clearance . patients and methods study population we included 52 consecutive patients ( 22 men , 30 women ; mean age 58 years ; range , 3976 years ) with hnc presenting for combined radiochemotherapy . 
hnc tumor patients exhibited a gfr range from 37105 ml / min / 1.73 m2 with only 7 patients with a gfr below 60 ml / min / 1.73 m2 as measured by ( 51 ) cr - edta clearance . 
the coefficient of variation typically observed for the gfr measurement by plasma clearance of ( 51 ) cr - edta was as low as 4% for patients with gfr over 30 ml / min / 1.73 m and 11% for those with a gfr below 30 ml / min / 1.73 all measurements were performed in a fasting state between 8 : 00 a.and 12 : 00 noon by the same experienced nurse . 
creatinine measurements were performed in the same laboratory on a modular p analyzer using the creatinine plus enzymatic assay which is standardized against id - ms ( roche diagnostics , mannheim , germany )  . 
patients individual glomerular filtration rates as determined by ( 51 ) cr - edta plasma clearance or calculated by creatinine - based equations ( formulas of cockroft - gault , mdrd ( modification of diet in renal disease ) , and wright ) or cystatin c - based equations ( formulas according to hoek , larsson , or dade - behring )  . 
individuelle glomerulre filtrationsrate jedes einzelnen patienten , berechnet mittels ( 51 ) cr - edta - plasma - clearance oder rechnerisch geschtzt mittels kreatinin - basierter formeln ( cockroft - gault , mdrd [ modification of diet in renal disease ] , wright ) bzw . 
the bland - altman limits of agreement procedure uses data scale assessment to analyze both the accuracy ( bias ) and the precision between any two measured values when the range of data is sufficiently limited . 
in addition , the intraclass correlation coefficient ( icc ) for every pair of alternative measure and the reference standard was calculated , as it distinguishes the between patients variance from the between methods variance and , therefore , yields a more appropriate measure of agreement than an ordinary correlation coefficient . as cisplatin therapy is only administered to patients with a gfr > 60 ml / min , the predictive value of the alternative gfr measures was analyzed with respect to this cut - off . 
according to their ( 51 ) cr - edta clearance , patients were divided into two groups with either gfr > 60 ml / min or gfr < 60 ml / m receiver operating characteristics ( roc ) curves were calculated and area under the curve ( auc ) was calculated . 
statistical evaluation of the alternative gfr estimates in comparison to the gold standard ( 51 ) cr - edta including mean difference , standard deviation , 95% confidence interval , limits of agreement as well as intraclass correlation coefficient . 
statistische auswertung der alternativen gfr - berechnungen im vergleich zum goldstandard ( 51 ) cr - edta - clearance inklusive mittlere abweichung , standardabweichung , 95% - konfidenz - intervall , grenzen der bereinstimmung sowie intraklassen - korrelationskoeffizient . 
egfr : errechnete glomerulre filtrationsrate ; acc : nach ; ecc : kreatinin - clearance ; ci : konfidenzintervall ; icc : intraklassen korrelationskoeffizient . minimum maximum mean 95% ci lower limit 95% ci upper limit std . 
gfr was estimated by various formula using either creatinine or cystatin c ( table 1 ) and compared with plasma clearance of ( 51 ) cr - edta as gold standard . 
individual gfr estimates are summarized in table 1 . the mean differences to the plasma clearance of ( 51 ) credta with standard deviation and 95% confidence interval of the mean were calculated for all measurements ( table 2 )  . 
in comparison to our reference standard , all the different methods applied for estimation of gfr show a positive value for the mean difference , indicating an overestimation of renal function . 
according to the mean difference , the cystatin c - based estimation of hoek ( mean difference , 7.62 ml / min / 1.73 m2 ) and dade - behring ( mean difference , 8.35 ml / min / 1.73 m2 ) appear to be the most accurate calculations of gfr tested , while the ecc ( mean difference , 29.88 ml / min / 1.73 m2 ) and gfr estimation using the wright formula ( mean difference , 27.75 ml / min / 1.73 m2 ) showed the highest deviation from the reference method . 
all other methods showed a wide range between lower and upper limit of agreement , suggesting poorer precision in gfr estimation . to distinguish the between patients variance from the between methods variance , the intraclass correlation coeftable 3 . 
ecc as well as the wright and cockroft - gault estimates showed a moderate agreement with the gold standard , the mdrd formula a strong agreement with the gold standard , while the icc calculated for the dadestrahlenther onkol 2011 no . 
as judged by the icc , the hoek formula again appears to be the most precise estimation of gfr in comparison to the other alternative methods used . as the icc for all alternative methods showed at least a fair agreement , a bland - altman plot was performed on all seven ( figure 1a )  . 
overall , hoek and dade - behring estimates appeared to be the most accurate and precise alternative methods . cisplatin treatment on hnc patients is only applied with a gfr > 60 ml / min our collection of 69 patients 36.2% ( n = 25 ) exhibited a gfr reduction below this cut - off point and would have been excluded from cisplatin treatment . 
 thus , our patients were divided into two groups according to the degree of renal insufficiency ( renal insufficiency > stage 35 with gfr < 60 ml / min and renal insufficiency < 3 with gfr > 60 ml / min ) as measured by the gold standard . 
the latter exhibited the criterion with the highest sensitivity and specificity at an estimated gfr of 60.7 ml / min / 1.73 m2 and was , therefore , the alternative method with the highest accuracy to classify the individual patient to the respective gfr group . discussion a reliable method for estimation of renal function is of cardinal importance in oncological practice as cancer patients are often treated with nephrotoxic drugs . 
furthermore , early renal insufficiency influences the dosage of chemotherapeutics with renal elimination , while severe renal insufficiency might prohibit its administration to avoid life - threatening side effects . besides surgical measures and radiotherapy , patients suffering from hnc are frequently treated with cisplatin - based chemotherapy . 
notably , investigations have shown that about 20% of acute renal failure cases among hospitalized patients are due to platinum - based chemotherapy [ 4 , 19 , 22 , 27 ]  . 
thus , a precise measurement of gfr is needed for the decision making on type and dosage of chemotherapy as well as to monitor renal function after chemotherapeutical intervention in these patients . creatinine - based methods for gfr estimation are widely used as an index of renal function in clinical practice . 
although extensive data support the idea that inulin or ( 51 ) cr - edta clearances are the gold standard for gfr measurement , its use in clinical practice is very restricted since it requires an intravenous infusion and a complicated chemical assay for inulin and time - consuming protocols for ( 51 ) cr - edta measurement . in the past , the cockcroft - gault formula was the first to be recommended for estimation of renal function based on creatinine [ 9 ]  . 
the major disadvantage of a creatinine - based formula to estimate gfr is the fact that an increase in creatinine is only detected when renal function has already deteriorated below 60 ml / min / 1.73 m2 a gfr which normally already excludes cisplatin therapy . 
 furthermore , tubular secretion of creatinine was shown to be increased in gfr ranges between 40 and 60 ml / min / 1.73 m2 , leading to overestimation of renal function in exactly that gfr range that is crucial for therapeutic decision [ 7 , 8 , 13 ]  . 
moreover , not all investigations included a gold standard such as inulin or ( 51 ) cr - edta clearance . in contrast to published investigations , the strength of the data presented here is not only the comparison of cystatin c - based formula to predict gfr with creatinine based formula and the gold standard ( 51 ) cr - edta clearance , but also a comparison between different published cystatin c - based formula in a defined patient population . 
in fact , it has been postulated that increased cystatin c may inhibit the proteolytic activity of extracellular cysteine proteases , a feature often associated with malignant cell phenotype [ 7 , 8 ]  . 
in addition , some reports indicate that cystatin c serum levels may be increased in oncological patients , leading to biased results in gfr estimation , while others reported that there is no increase in cystatin c levels in malignancy [ 28 , 34 ]  . 
while one report showed increased levels of serum cystatin c in hnc patients when compared to healthy controls [ 35 ] , suggesting a pathological role of cystatin c in hnc , another investigation demonstrated that high levels of cystatin c strahlenther onkol 2011 no . 
 ( continued ) a bland - altman plot , showing a comparison between the gold standard ( 51 ) cr - edta clearance and gfr estimates by the cystatin c - based equations according to dade - behring , larsson , and hoek or creatinine - based equations according to the wright , mdrd , and cockroft gault formulas . 
 ( fortsetzung ) a bland - altman plots zum vergleich der mittels goldstandard ( 51 ) cr - edta - clearance ermittelten gfr und den cystatin c basierten gfr berechnungen nach dade - behring , larsson oder hoek bzw . 
 b receiver - operating - characteristic - curve - ( roc - ) analyse der cystatin - c - basierten bfr - berechnungen nach dade - behring , larsson oder hoek bzw . 
der kreatinin - basierten gfr - berechnungen nach wright , mdrd oder cockroft - gault , eine chronische niereninsuffizienz stadium 3 oder hher zu erkennen . in tumor tissue had a protective effect , being associated with prolonged survival [ 32 ]  . 
similar results were published for breast [ 15 , 16 ] and lung cancer [ 11 ]  . in the present investigation , all gfr estimates based on serum cystatin c showed a higher accuracy and precision in determination of gfr than estimates based on creatinine or 24 - hour urine collection . 
notably , an improvement of precision might be achieved by a 24 - hour catheter urine collection , but would implement invasive catheterization in a patient group with an already increased susceptibility for infections . 
among the creatinine - based estimates , the mdrd formula appeared to be the most accurate , but could not reach the performance of the cystatin c - based formula of hoek , dade - behring , or larsson . 
sensitivity and specificity of creatinine - based and cystatin c - based gfr estimates to discriminate gfr < 60 ml / min / 1.73 m2 as measured by the reference method ( 51 ) cr - edta plasma clearance were evaluated by receiver operating characteristic curve ( roc )  . 
especially the accuracy of the mdrd formula is highest at a range between 20 and 60 ml / min / 1.73 m2as it might have been expected , since it was initially designed for a patient group with chronic renal insufficiency stage 35 . 
notably and in line with our data , previous investigations have already suggested that cystatin c measurement can detect chemotherapy - induced renal toxicity earlier than creatinine [ 8 ]  . 
overall the cystatin c based formula of hoek appears to be the most precise and accurate . despite a less accurate overall estimation of gfr in comparison to the cystatin c - based formula of hoek , dadebehring , or larsson , the wright and the mdrd formulas exhibited the highest sensitivity and specificity in classifying a patient to either a potential cisplatin treatment group with a gfr above 60 ml / min / 1.73 m2 or with a gfr below 60 ml / min / 1.73 m2 , thereby , prohibiting a cisplatin - based chemotherapy . 
nevertheless , the cystatin c - based formula of larsson ( criterion 62.7 ) , dade - behring ( criterion < 60 ) , and hoek ( criterion < 63 ) also exhibited high accuracy with both sensitivity and specificity lying above 92% . 
as monitoring of renal function after chemotherapy is equally important , our overall data favors the cystatin c - based formula hoek , dadebehring , or larsson in hnc patients . conclusion the cystatin c - based formula of hoek , larsson , and dadebehring applied in this study promotes the use of cystatin c as a good estimate of the gfr , which is more accurate and precise than the mdrd or the cockcroft - gault formulas , especially in populations that do not match the group for which the mdrd2 formula was validated . 
thus , we propose cystatin c as the preferred endogenous parameter for gfr estimation in hnc patients . strahlentherapie und onkologie original article definition of the ctv prostate in ct and mri by using ctmri image fusion in imrt planning for prostate cancer bettina hentschel1 , wolfgang oehler1 , dirk strau1 , andreas ulrich2 , ansgar malich2 , bettina hentschel3 purpose : to determine the prostate volumes defined by using mri and ct scans , as well as the difference between prostate delineation in mri and ct in three dimensions ( 3d )  . 
a further goal was to use mri to identify subgroups of patients in whom seminal vesicle irradiation can be avoided . methods and materials : a total of 294 patients with biopsy - proven prostate cancer ( mri stages : t1 , 16 [ 5% ] ; t2 , 84 [ 29% ] ; t3 , 191 [ 65% ] ; t4 , 3 [ 1% ] ) underwent pelvic ct and mri scans before intensity - modulated radiation therapy ( imrt ) planning . 
the low - risk patients ( 59% , n = 171 of 290 ) calculated by applying the roach and diaz formula had a svi rate of 57% ( n = 97 of 171 ) , the high - risk patients ( 41% , n = 119 of 290 ) of 71% ( n = 85 of 119 )  . conclusions : compared with mri , ct scans overestimate prostate volume by 35% . 
das svi - risiko betrug 57 % ( 97 / 171 ) fr die entsprechend der roach - diaz - formel ermittelte niedrigrisikogruppe ( 59 % [ 171 / 290 ] ) und 71 % ( 85 / 119 ) fr die hochrisikopatienten ( 41 % [ 119 / 290 ] )  . schlussfolgerung : unsere ergebnisse zeigen , dass durch die mrt - integration in die imrt - bestrahlungsplanung die definition des ctv prostata przisiert werden kann und dass eine mr - basierte bestrahlungsplanung eine genaue definition des tumorstadiums ermglicht , da sie die exakte beurteilung einer tumorinfiltration der vesiculae seminales erlaubt . schlsselwrter : prostatakarzinom mrt definition ctv prostata imrt 1department of radiation oncology and radiotherapy , sdharz - krankenhaus , nordhausen , germany , 2department of radiology , sdharz - krankenhaus nordhausen , germany , 3institute for medical informatics , statistics and epidemiology , medical faculty , university of leipzig , germany . received : may 26 , 2010 ; accepted : september 27 , 2010 published online : february 24 , 2011 strahlenther onkol 2011 no . 
ctmri image fusion in imrt planning for prostate cancer introduction several studies have shown the importance of dose escalation in the radiotherapeutic management for various prognostic groups of prostate cancer [ 2 , 7 , 8 , 11 , 33 ]  . 
intensity - modulated radiation therapy ( imrt ) allows the delivery of the necessary high tumor total doses without increasing the dose to the organs at risk [ 13 ]  . 
the success of dose escalation depends on correct staging and target volume identification . current efforts are directed at different methods , such as magnetic resonance imaging ( mri ) and magnetic resonance spectroscopic imaging ( mrsi )  . 
results published in the literature suggest that mri , especially with high resolution 3.0 tesla t2weighted scans , dynamic contrast enhancement , and an endorectal surface coil , allows accurate staging in up to 94% of cases of seminal vesicle invasion ( svi ) [ 1 , 5 , 12 , 23 , 25 , 28 , 30 ]  . in the past , mri has not been routinely used for imrt treatment planning of prostate cancer . 
usually physicians rely upon clinical and biological features and an empirically derived equation by roach and diaz [ 6 , 26 ] to predict the risk of seminal vesicle involvement of prostate cancer [ 14 ]  . 
furthermore , the incidence of svi in prostate cancer patients defined by mri was compared with the results obtained with the equation described by roach and diaz . methods and materials patient data pelvic ct and mri scans were obtained for 294 consecutive patients with biopsy - proven prostate cancer . 
patientenmerkmale. number of patients nodal disease distant metastasis androgen deprivation gleason score t3b 182 13b 60c 2b 810 0b 9c < 10 1020 > 20 a mr - based t category b / cunknown in 4 cases ( bunknown in 1 case , cunknown in 3 cases ) an gleason score was 6 . 
selection of patients and decisions on radiation treatment protocols were based on the mri stages , histological grades , and psa levels ( table 1 )  . treatment typically , patients received a 7or 8 - field imrt sliding window technique . 
in 77 patients with more than 15% lymph node involvement , the pelvic node region was treated to incorporate the nodes at risk . treatment planning ct scans of the pelvis were obtained in 5 mm slice thicknesses at 5 mm intervals . 
patients were instructed to have an empty bladder before the initial ct and mri scans as well as for each treatment fraction . the pelvic mri was performed with a 1.5 tesla scanner ( philips intera system ) , using a circularly polarized pelvic phased array coil . 
criteria for svi were a focal , low signal intensity mass or diffuse enlargement with low signal intensity and loss of the perceptible vesicle wall on both t1and t2 - weighted sequences ( figure 1 ) [ 25 , 32 ]  . image fusion the axial mr image was superimposed on the ct image using the eclipse automatic registration algorithm of the strahlenther onkol 2011 no . 
contours of the prostate ( prostate ctvs ) were drawn on superimposed ct and axial mri slices of each scan by using the blend verification view , which displays both 3d images simultaneously with selectable opacity . the study aimed to evaluate the accuracy of mri in defining prostate ctv compared with the accuracy of ct . 
 [ 16 ] , who analyzed five areas with a distance of 9 mm between each level . in patients with seminal vesicle ( sv ) invasion identified by mri , the length of the sv as well as the tumor extension within the seminal vesicles were measured on axial and sagittal mri images in centimeters . 
we compared the results with the data obtained by the equation described by roach and diaz to predict the risk of sv involvement : svi = psa value + ( gleason score 6 ) 10 the formula calculates the incidence of sv involvement , with a cutoff of 13% used to classify patients into lowand high - risk groups . 
the differences between the mriand ct - based prostate volumes were statistically significant with p < 0.001 ( paired t test , correlation coefficient = 0.95 , figure 3 )  . the linear regression line ( figure 4 ) shows small differences for small prostate volumes , whereas a noticeable difference was registered for larger volumes . 
only in 12 cases did the ct - derived contour partially coincide with the contour on the mri in more than one slice . regions of largest discrepancies of prostate ctv defined by ct and mri were registered at the base of the prostate immediately adjacent to the seminal vesicles and at the apical portion of the prostate . 
beziehung zwischen ct - mri - definiertem prostatavolumen ( cm3 )  . results in all cases ( n = 294 ) of the current study , the prostate volume defined by ct was larger than the volume defined by mri . 
of the positive svs , 71% had svi beyond 2.0 cm from the prostatesv junction , 22% had svi beyond 3.0 cm , and 5% had involvement beyond 4.0 cm ( figure 5 )  . 
 [ 29 ] found in similar studies ( 18 , 22 , and 8 patients , respectively ) a mean increase of prostate volume of 27% , 43% , and 34.3% , respectively , in ct compared with mri . 
 similar to these previous findings , which are based on a relatively small number of patients , the results of our studies carried out on 294 patients showed a mean overestimation of the prostate volume by 35% in ct compared with mri . when discussing these results , one has to address potential limitations of our and the previous studies . 
ctmri image fusion in imrt planning for prostate cancer erature [ 3 , 10 ] , a ctmr image fusion and delineation procedure has been validated and found to be accurate and reproducible . 
no statistical difference was found between ctand mri - based ctvs although acquired with different slice thicknesses ( see appendix )  . another important aspect is that significant discrepancies of prostate volume could be probably caused by mri - produced distortions because of chemical shift artifacts and field inhomogeneities and that the organ volume defined by mri does not correlate with the real anatomical organ volume [ 9 , 20 ]  . 
 [ 15 ] reported a significant correlation between the prostate volume measured by using mri and the actual prostate volume measured after radical prostatectomy . the mri - delineated volume is smaller because the visibility of the prostate apex is better and the base of the prostate can be differentiated more precisely from the seminal vesicles . 
 the prostatic apex as well as the most superior portion of the prostate are grey areas on ct , because it is difficult to distinguish between the prostate , venous plexus , neurovascular bundles , and pelvic floor muscles , while mri yields more contrast resolution when differentiating the prostate gland from the periprostatic soft tissues . according to our findings , the areas defined by ct at each of the six levels were larger than the areas on mri with the largest differences appearing at the most superior and inferior portions of the prostate . 
what are the implications of these results for prostate imrt planning ? due to the fact that the volume of a mri - delineated prostate is smaller than that of a ct - delineated prostate , it could be expected that a treatment plan based on mri reduces the dose delivered to the surrounding normal tissue which leads to a reduced complication probability . 
the result of our study that the smallest discrepancies of prostate ctv between ct and mri were 5.0 cm2 at the central part of the prostate leads to the conclusion that the drawn ctv in the planning ct scans already covers an average margin of 0.36 cm surrounding the real anatomic contour of prostate defined by mri . designing optimal margins for the ctv must account for organ motion , setup errors and other treatment uncertainties , as well as the volume of normal tissues within high - dose regions . 
based on our analysis , the margin between ctv and ptv which is required to adequately cover setup error and organ motion could be reduced by the difference between the prostate volumes defined by mri and ct . 
therefore , we recommend the combined use of axial mri for delineation and the ct scan for imrt planning of the prostate . excluding the seminal vesicle from the ctv can significantly reduce the irradiated rectal volumes [ 17 ]  . 
based on our analysis , approximately 37% of patients could have been treated excluding their seminal vesicles . several studies have analyzed the probability of svi in relation to both prognostic factors psa level and gleason score [ 21 , 22 ]  . 
similar to our data , 58% of the patients with all three high - risk risk factors demonstrated sv involvement . overall the results of our study are unexpected because the incidence of sv invasion identified by mri was noticeably higher than calculated by the roachdiaz formula for the lowrisk group and , in contrast , a relatively low incidence of svi for high - risk patients was identified by mri . 
a possible explanation for this discrepancy between the calculated incidence of sv invasion and the risk of sv involvement identified by mri could be the small number of our patients in each ( the highand low - risk ) subgroup , which is not fully representative for both risk groups . it is obvious that mri fusion - based treatment planning can predict more accurately the correct staging . 
 [ 4 ] series , one might question the validity of our mri findings . a further aspect which possibly affects the svi staging accuracy is that mri examinations were performed with a pelvic phased array coil instead of the endorectal coil to improve the precision of ctmr image fusion . 
 although the mris of our study were interpreted by highly experienced mri radiologists , our results should be validated by further studies in other institute settings and with larger numbers of patients . 
it consisted of an empty lucite cylinder with an object figuring a solid organ with a spherical shape and a smooth surface : a 56.3 cm3 ( finite difference method ) heart of a turkey fixed in the middle of the container . 
for ct scan and mri , the container was filled with water . ct and axial t2 - weighted mr scan acquisition were obtained in 5 mm and 3 mm slice thickness , respectively . 
no difference in accuracy was observed between the various imaging modalities . to test the accuracy of prostate volume outlined on superimposed mrict scans , one of the prostate cancer patients underwent pelvic ct and mri scans acquired in 5 mm and 3 mm slice thickness , respectively , before imrt planning . 
the effect of changes in the health care policy in japan on radiotherapy structure was also examined . material and methods : the japanese society of therapeutic radiology and oncology surveyed the national structure of radiation oncology in 2007 . 
geographically , the number of designated cancer care hospitals was associated with population size . conclusions : the structure of radiation oncology in japan in terms of equipment , especially for designated cancer care hospitals , was as mature as that in european countries and the united states , even though the medical costs in relation to gdp in japan are lower . 
the survey data proved to be important to fully understand the radiation oncology medical care system in japan . key words : structure survey radiotherapy facility radiotherapy personnel radiotherapy equipment caseload medical care system strahlenther onkol 2011 ; 187 : 16774 doi 10.1007 / s00066 - 010 - 2205 - 3 japanische strukturerhebung zur radioonkologie im jahr 2007 unter besonderer bercksichtigung von auf krebsbehandlung spezialisierten krankenhusern hintergrund und ziel : es wurde die struktur der radioonkologie in auf krebsbehandlung spezialisierten krankenhusern in japan untersucht , und zwar im hinblick auf ausrstung , personal , patientenaufkommen und geografische verteilung . 
ebenso 1department of medical physics and engineering , osaka university graduate school of medicine , suita , osaka , japan , 2department of radiology , tokyo medical and dental university , tokyo , japan , 3department of radiology , national hospital organization hokkaido cancer center , sapporo , hokkaido , japan , 4department of radiology , sakai municipal hospital , sakai , osaka , japan , 5department of radiation oncology , st . 
lukes international hospital , tokyo , japan , 6department of radiology , hyogo college of medicine , nishinomiya , hyogo , japan , 7oncology center , osaka university hospital , suita , osaka , japan , 8department of radiology , toho university omori medical center , tokyo , japan , 9department of medical informatics , heavy ion medical center , national institute of radiological sciences , chiba , japan , 10department of radiation oncology , saitama medical university international medical center , saitama , japan , 11department of radiology , university of tokyo hospital , tokyo , japan , 12department of radiology , kyushu university hospital at beppu , oita , japan , 13department of radiation oncology and image - applied therapy , graduate school of medicine kyoto university , kyoto , japan , 14division of radiation oncology , shizuoka cancer center , shizuoka , japan , 15department of radiology , sapporo medical university , hokkaido , japan . received : august 13 , 2010 ; accepted : october 7 , 2010 published online : february 21 , 2011 strahlenther onkol 2011 no . 
structure survey of radiation oncology in japan wurden die auswirkungen von vernderungen in der japanischen gesundheitsfrsorge - politik auf die strahlungstherapie - struktur untersucht . material und methodik : die japanische gesellschaft fr radiologische therapie und onkologie hat eine erhebung zur nationalen struktur der strahlungsonkologie im jahr 2007 durchgefhrt . 
dabei wurden die strukturen von 349 auf krebsbehandlung spezialisierten krankenhusern und 372 anderen strahlentherapie - einrichtungen verglichen . ergebnisse : die jeweiligen ergebnisse in bezug auf die ausrstung und das personal in den auf krebsbehandlung spezialisierten krankenhusern und anderen einrichtungen waren : linearbeschleuniger pro einrichtung : 1 , 3 bzw . 
in geografischer hinsicht stand die anzahl der auf krebsbehandlung spezialisierten krankenhuser in relation zur bevlkerungszahl . schlussfolgerung : die struktur der radioonkologie in japan war , was die ausrstung und insbesondere die auf krebsbehandlung spezialisierten krankenhuser betrifft , ebenso ausgereift wie oder ausgereifter als in europischen lndern und in den vereinigten staaten , obwohl die medizinischen kosten im verhltnis zum bip in japan geringer sind . 
die erhebungsdaten haben sich als bedeutsam fr ein umfassendes verstndnis des radioonkologiekrankenpflegesystems in japan erwiesen . schlsselwrter : strukturerhebung strahlentherapie - einrichtung strahlentherapie - personal strahlentherapie - ausrstung patientenaufkommen medizinisches versorgungssystem introduction in developed countries in europe , such as france , germany , italy , and the uk , as well as in the united states , the rates of radiotherapy use for cancer treatment are as high as 50% or more because there are sufficient radiotherapy facilities and personnel , such as radiation oncologists ( ros ) , medical physicists ( mps ) , and radiotherapy technologists ( rtts ) [ 1 , 2 , 5 , 11 ]  . 
at the same time , the ministry of health , labor , and welfare began the accreditation of designated cancer care hospitals ( dcchs ) with the aim of correcting regional differences in the quality of cancer care and strengthening cooperation between regional cancer care hospitals [ 3 , 9 , 13 ]  . 
the japanese society of therapeutic radiology and oncology ( jastro ) has conducted national structure surveys of radiotherapy facilities in japan every 2 years since 1990 [ 18 , 19 ]  . 
 in this study , the recent structure of radiation oncology in japan was analyzed with special reference to dcchs in terms of equipment , personnel , patient load , and geographic distribution . 
furthermore , the medical care situation in japan was compared with european countries and the united states . materials and methods jastro carried out a national structure survey of radiation oncology in 2007 by administering a questionnaire in 2008 [ 19 ]  . 
the questionnaire consisted of items related to the number of treatment machines and modality by type , the number of personnel by job category , the number of patients by type , and the site . 
in this survey , full - time equivalent ( fte ) ( 40 hours / week only for radiation oncology service ) data were surveyed depending on clinical working hours for radiotherapy of each staff . 
the statistical significance was tested by means of the 2 test , students t test , or analysis of variance ( anova )  . the japanese blue book guidelines ( jbbg ) [ 6 , 7 ] were used for comparison with the results of this study . 
the numbers of new patients and total patients in all radiotherapy facilities in japan were estimated at approximately 181 , 000 ( 170 , 229 765 / 721 ) and 218 , 000 ( 205 , 087 765 / 721 ) , respectively . 
for dcchs , the corresponding numbers were approximately 117 , 000 ( 112 , 101 364 / 349 ) and 141 , 000 ( 135 , 383 364 / 349 )  . 
the number of patients in dcchs , thus , accounted for approximately 65% of the number of patients , both new and total ( 117 , 000 / 181 , 000 and 141 , 000 / 218 , 000 ) , in all radiotherapy facilities . 
the average numbers of new patients / facility were 321.2 for dcchs and 156.3 for the other radiotherapy facilities , and for the average numbers of total strahlenther onkol 2011 no . 
anzahl neuer patienten und aller patienten ( neu plus wiedereingeliefert ) , die der strahlentherapie bedrfen , in auf krebsbehandlung spezialisierten krankenhusern und anderen strahlentherapieeinrichtungen . designated cancer care hospitals facilities 349 112 , 101a new patients average no . 
 bpercentage calculated from the number of systems using this function and the total number of linac systems . ccomparison with the data of 2005 , calculated with the formula : data of 2007 ( % ) data of 2005 ( % ) dpercentage calculated from the number of patients and the number of linac units . 
 bei einrichtungen mit vollzeitquivalent < 1 wurde die anzahl der vollzeitquivalent - radioonkologen mit vollzeitquivalent = 1 berechnet , um eine berschtzung des patientenaufkommens pro vollzeitquivalent - radioonkologe zu vermeiden . 
bei einrichtungen mit vollzeitquivalent < 1 wurde die anzahl der vollzeitquivalentstrahlentherapie - mtas mit vollzeitquivalent = 1 berechnet , um eine berschtzung des patientenaufkommens pro vollzeitquivalentstrahlentherapie - mta zu vermeiden . 
rt : radiotherapy ; ro : radiation oncologist ; fte : full - time equivalent ( 40 hours / week only for rt practice ) ; jastro : japanese society of therapeutic radiology and oncology . designated cancer care hospitals ( n = 349 ) 171 facilities with rt bed average no . 
more than 200 patients / rtt ( jbbg warning level ) were treated in 18% of dcchs and in 8% of the other radiotherapy facilities , while figure 2b shows the percentage of distribution of facilities by patient load / fte rtt . 
in european countries and the united states , on the other hand , most facilities have a full - time ro . on a regional basis , the results of this study proved that dcchs were in appropriate locations . 
in the 2005 survey [ 9 ] , there were not enough dcchs in some regions with a large population because many university facilities were not strahlenther onkol 2011 no . 
bei einrichtungen mit vollzeitquivalent < 1 wurde die anzahl der vollzeitquivalent - radioonkologen mit vollzeitquivalent = 1 berechnet , um eine berschtzung des patientenaufkommens pro vollzeitquivalent - radioonkologe zu vermeiden . 
bei einrichtungen mit vollzeitquivalent < 1 wurde die anzahl der vollzeitquivalent - strahlentherapie - mtas mit vollzeitquivalent = 1 berechnet , um eine berschtzung des patientenaufkommens pro vollzeitquivalent - strahlentherapie - mta zu vermeiden . certified as dcchs by the ministry of health , labor , and welfare . 
current radiotherapy potential in radiotherapy facilities other than dcchs in japan is underutilized because of personnel shortages . in japan , a new educational system is being developed to train specialists for cancer care , including ros , mps , medical oncologists , oncology nurses , and palliative care doctors . 
 in japan , many radiotherapy hospitals do not even have their own department of radiotherapy , while we are of the opinion that all radiotherapy hospitals , whether designated or not , need to have figure 3 . 
the dotted line shows the average number of facilities of the prefectures per quarter for all radiotherapy hospitals and the dashed line shows the average number for designated cancer care hospitals . 
die gepunktete linie zeigt die durchschnittliche anzahl der einrichtungen der prfekturen pro viertel fr alle strahlentherapie - krankenhuser , und die gestrichelte line zeigt die durchschnittliche anzahl fr auf krebsbehandlung spezialisierte krankenhuser . 
structural features and personnel related to radiation oncology in developed countries and cost adapted from the directory of radiotherapy centers of the international atomic energy agency [ 4 ]  . 
at present , there is no national license for mps in japan , but those with a masters degree in radiation technology or science and engineering can take the accreditation test for mps administered by the japanese board of medical physics ( jbmp )  . 
further accreditation of dcchs by the ministry of health , labor , and welfare would be a move in the right direction for the geographical consolidation of radiotherapy facilities in japan . 
even though the medical costs in relation to gdp [ 10 ] in japan are the lowest among the aforementioned five countries , the outcome of cancer treatment in japan is the same or better than in the other developed countries . to evaluate medical care systems for cancer at regular intervals , it is very important to collect detailed information for all cancer care facilities . 
in japan , jastro regularly surveys the structural information for all radiotherapy facilities and pcs has been conducted every 4 years to investigate the processes and outcomes of cancer care using radiotherapy . 
we have recently established a japanese national cancer database based on the radiotherapy data , and we are preparing to collect cancer care data with this system . conclusion the structure of radiation oncology in dcchs in japan showed more maturity than that of other facilities in terms of equipment , functions , and staff . 
structure survey of radiation oncology in japan strahlentherapie und onkologie short communication ferumoxtran - 10 mr lymphography for target definition and follow - up in a patient undergoing image - guided , dose - escalated radiotherapy of lymph nodes upon psa relapse anja m . 
we present our initial experience with ferumoxtran - 10 mr lymphography as the basis for image - guided , doseescalated lymph node radiotherapy and for early follow - up after radiotherapy . patients and methods : a patient with suspicion for lymph node metastasis after radical prostatectomy was examined with mr lymphography with the lymph node - specific contrast media ferumoxtran - 10 . 
radiotherapy was performed as intensity - modulated radiotherapy with a total dose of 44 gy to the whole lymphatic drainage , 60 gy to the area of affected lymph nodes , 71 gy to the prostate bed , and 75 gy to the anastomosis region . 
8 weeks after completion of radiotherapy , a follow - up mr lymphography with ferumoxtran - 10 was performed . results : in the first mri with ferumoxtran - 10 , 5 metastatic lymph nodes were found in the iliac region . 
psa ( prostate - specific antigen ) decreased from 2.06 ng / ml pretherapeutically to 0.02 ng / ml at 2 weeks after treatment and was no longer detectable at 8 months after treatment . conclusions : lymph node staging with ferumoxtran - 10 and subsequent dose escalation with intensity - modulated radiotherapy led to the elimination of positive lymph nodes and a decrease in the psa value . key words : prostate cancer metastatic lymph nodes ferumoxtran - 10 radiotherapy intensity - modulated radiotherapy strahlenther onkol 2011 ; 187 : 20612 doi 10.1007 / s00066 - 010 - 2195 - 1 ferumoxtran - 10 - mr - lymphographie zur zieldefinition und therapiekontrolle bei einem patienten mit bildgefhrter dosiseskalierter strahlentherapie der lymphknoten bei psa - rezidiv ziel : die evaluation des lymphknotenstatus bei patienten mit prostatakarzinom ist fr eine erfolgreiche strahlentherapie notwendig . 
wir stellen erste erfahrungen mit ferumoxtran - 10 als grundlage fr eine bildgefhrte strahlentherapie der lymphabflusswege vor . patienten und methoden : ein patient mit verdacht auf lymphknotenmetastasen nach radikaler prostatektomie wurde mittels magnetresonanztomographie der lymphknoten mit dem lymphknotenspezifischen kontrastmittel ferumoxtran - 10 untersucht ( tabelle 1 )  . 
eine intensitts - modulierte strahlentherapie wurde mit folgender gesamtdosis durchgefhrt : 44 gy gesamte lymphabflusswege , 60 gy metastatische lymphknoten , 71 gy prostataloge und 75 gy anastomosenregion ( abbildung 2 )  . 
8 wochen nach beendigung der strahlentherapie wurde eine erneute magnetresonanztomographie der lymphknoten zur kontrolle durchgefhrt . electronic supplementary material / supplementals : the online version of this article ( doi : 10.1007 / s00066 - 010 - 2195 - 1 ) contains supplementary material , which is available to authorized users . 
 1department of clinical radiology and nuclear medicine , university medical center mannheim , germany , 2department of radiation oncology , university medical center nijmegen , the netherlands , 3department of radiation oncology , university medical center mannheim , germany , 4department of radiology , university medical center nijmegen , the netherlands . received : july 28 , 2010 ; accepted : august 11 , 2010 published online : february 21 , 2011 strahlenther onkol 2011 no . 
ferumoxtran - 10 mr lymphography in a patient undergoing image - guided , dose - escalated radiotherapy ergebnisse : in der ersten magnetresonanztomographie der lymphkntoten zeigten sich 5 metastatische lymphknoten iliakal ( abbildung 1a und 1b )  . 
der psa - wert ( prostataspezifisches antigen ) sank von 2 , 06 ng / ml vor therapie auf 0 , 02 ng / ml 2 wochen nach therapie und war 8 monate nach therapie nicht mehr messbar . schlussfolgerung : die intensittsmodulierte strahlentherapie mit gesteigerter dosis auf grundlage des lymphknotenstaging mittels ferumoxtran - 10 fhrte zu einer eliminierung metastatischer lymphknoten und einem absinken des psa - wertes . schlsselwrter : prostatakarzinom lymphknotenmetastasen ferumoxtran - 10 strahlentherapie intensittsmodulierte strahlentherapie introduction accurate evaluation of a patients lymph node situation is essential for defining clinical radiotherapy target volumes when treating prostate cancer [ 29 ]  . 
an optimal imaging procedure would ideally provide highly accurate pretherapeutic information on metastatic lymph node invasion on a node - by - node basis and could also be used for treatment follow - up . the gold standard for lymph node staging in prostate cancer is currently considered to be extended pelvic lymphadenectomy , but the procedure carries a significant morbidity risk with a complication rate of 550% [ 14 , 16 ] and is , therefore , not extensively used . 
while sentinel node dissection has been evaluated and initial reports suggest good accuracy with a detection rate of 98% , a false negative result of 6% is still reported [ 8 , 15 ]  . 
 the same limitations apply to sentinel node - guided radiotherapy which offers the possibility to increase radiotherapy dose to lymph nodes at elevated risk of invasion but does not enable dose escalation to actually affected lymph nodes [ 8 ]  . as a consequence of the shortcomings of established methods for lymph node staging , the decision to treat the draining lymph nodes in prostate cancer is usually based on calculated invasion risk , the basis of which is increasingly the subject of discussion [ 18 ]  . magnet resonance imaging ( mri ) of the lymph nodes with lymph node - specific contrast media ( ferumoxtran - 10 ) is a possibility to improve lymph node staging and therapy follow - up . 
 ferumoxtran - 10 , consisting of ultrasmall superparamagnetic iron oxide particles , is a biodegradable mr contrast agent with a long residence time in the intravascular compartment that is eventually incorporated into elements of the reticuloendothelial system , including lymph nodes . 
benign and reactive nodes share the presence of phagocytic or mononuclear cells , in contrast to massively involved metastatic nodes which are no longer accessible for those cells and , therefore , fail to show decreased signal intensity after ferumoxtran - 10 injection . 
ferumoxtran - 10 , thus , behaves as a negative contrast agent [ 3 ]  . we present an initial experience with ferumoxtran - 10 mr lymphography as the basis for image - guided , dose - escalated lymph node radiotherapy and for early follow - up after radiotherapy . material and methods patient a 58 - year - old patient with biopsy - proven bilateral prostate cancer ( stage pt3b n1 , gleason score 4 + 3 and a pretherapeutic psa value of 50 ng / ml ) had previously undergone radical prostatectomy including lymph node dissection . 
in a positron emission tomography / computer tomography 5 months after prostatectomy , one external iliac lymph node was suspicious for metastasis , but in a second lymph node dissection 4 months later no metastatic lymph node was found . 
to further investigate the rise in psa , a mr lymphography with ferumoxtran - 10 was performed . this mr lymphography was then the basis for imageguided , dose - escalated , intensity - modulated radiotherapy of the lymph nodes . 
finally , 8 weeks after completion of radiotherapy as described below , a follow - up mr lymphography with ferumoxtran - 10 was performed . administration of ferumoxtran - 10 permission for the diagnostic use of ferumoxtran - 10 by irb was obtained . 
the weight - adjusted dose of 2.6 mg ferumoxtran - 10 ( sinerem , guerbet , paris ) / kg body weight was given intravenously with a slow drip infusion 24 hours before mri examination . mri protocols all mr sequences were obtained with a 3 tesla scanner ( tim trio , siemens medical solutions , erlangen , germany ) together with a pelvic phased array coil ( medrad inc . , pittsburgh , pa , usa )  . 
the obtained sequences are described in table 1 . post - processing and reading the mri datasets were imported to the lymph node taskcard software ( siemens , erlangen , germany )  . 
the identified lymph nodes were delineated with a taskcard tool by manually setting a landmark within the center of the node and then applying an automatic contourdefining algoriththese delineations could be seen in every loaded mri sequence obtained in the same mri session . 
in the t2 * sequences , the delineated lymph nodes were assessed with levels of suspicion ( los ) 15 ( 1 : definitely no metastasis , 2 : probably no metastasis , 3 : equivocal , 4 : probably metastasis , 5 : definitely metastasis )  . 
different colors for the surroundings depending on the level of suspicion were given ( los 1 green , los 23 yellow , los 45 red ) ( figure 1a and 1b , esm / supplementals : movie 1 )  . 
evaluation of mri was performed by two readers ( 10 and 1.5 years of experience ) in consensus with full knowledge of the clinical results . radiotherapy planning treatment planning ct datasets were acquired at a brilliance big bore scanner , ( philips healthcare , eindhoven , the netherlands )  . 
a total dose of 44 gy in daily single doses of 2 gy was applied to the whole lymphatic drainage including elective lymph nodes and the prostate bed in the first part of the treatment sequence . 
finally , the prostate bed was irradiated to a final dose of 71 gy and the anastomosis region to 75 gy in a total of five fractions , thus , applying a single dose of 3 gy to the anastomosis region for this part of the treatment . 
the patient did not receive antihormonal treatment at any time before , during , or after radiotherapy . results in the first pretherapeutic mri with ferumoxtran - 10 , 5 metastatic lymph nodes ( level of suspicion 45 ) were found in the iliac region ( left internal iliac , right internal iliac , right external iliac , common iliac on both sides ) and 3 lymph nodes were classified as level of suspicion 3 ( table 2 , figure 1a and 1b , esm / supplementals : movie 1 )  . 
 green lymph nodes are judged to be benign , yellow lymph nodes have a level of suspicion of 3 and red lymph nodes have a level of suspicion of 45 ( metastatic )  . 
links der metastatische lymphknoten in der axialen t1 - gewichteten vibesequenz , rechts der wei erscheinende lymphknoten ohne ferumoxtran - 10 - aufnahme in der axialen t2 * - gewichteten aufnahme . radiation therapy was performed as intended in the sequence described above . 
image - guided radiotherapy treatment plan for the second target volume covering prostate bed , anastomosis region , and ferumoxtran - 10 positive lymph nodes with a maximum dose of 60 gy after treating prostate bed and total area of lymphatic drainage up to a dose of 44 gy . 
bestrahlungsplanung zur bildgefhrten strahlentherapie der prostataloge , der anastomosenregion und ferumoxtran - 10 positiver lymphknoten mit einer hchstdosis von 60 gy , nachdem prostataloge und die gesamten lymphabflusswege mit einer dosis von 44 gy bestrahlt wurden . 
anschlieend wurde die bestrahlung der prostataloge und der anastomose bis zu einer gesamtdosis von 71 / 75 gy fortgesetzt . apeutic mr lymphography is displayed as a 3d rendering in figure 2 . 
radiotherapy was tolerated well with no acute side effects other than a small epitheliolysis and two small intradermal bullae in the region of the rima ani . the scan 8 weeks postradiotherapy no longer showed lymph nodes suspicious for metastases based on the ferumoxtran - 10 enhanced images ( table 2 , figure 3a and 3b , esm / supplementals : movie 2 )  . this was paralleled by a decline of psa from 2.06 ng / ml pretherapeutically to 0.17 ng / ml at the end of the treatment , strahlenther onkol 2011 no . 
inv : ausma des befalls ; p : teilweise ; t : komplett ; los : verdachtsgrad ; mrl : magnetresonanzlymphographie . node location inv first los first smallest diameter ( mm ) first second left external iliac right common iliac left common iliac left common iliac right external iliac right obturator perirectal perirectal left internal iliac not definable not definable not definable 0.02 ng / ml at 2 weeks after treatment , and to a no longer detectable level at 8 months after treatment . discussion currently , a formula devised by roach et al . 
a value greater than 15% and advanced t stages ( t34 ) are defined as high risk and , therefore , taken as the cutoff upon which elective nodal irradiation is advised [ 20 , 29 ]  . 
patients at low risk for having lymph node metastases who are not candidates for surgical sampling can benefit from the potentially increased accuracy of this method with regard to detecting lymph node positivity with a minimally invasive method , while some patients with an a priori high risk for metastasis may prove negative and be spared further therapy . 
all patients with manifest lymph node metastases may then benefit from the improved detection of affected lymph nodes on a node - to - node basis with regard to targeted local therapy when mr imaging with ferumoxtran - 10 is performed . despite considerable toxicity , series comprised of lymph node - positive patients treated with an intensive apfigure 3a and 3b . 
a the 3 - d illustration of the pelvic vessels and the delineated non - metastatic lymph nodes in the second mri with ferumoxtran - 10 8 weeks after radiotherapy . 
 ( esm / supplementals : movie 2 ) b second mri with ferumoxtran - 10 eight weeks after radiotherapy without metastatic lymph nodes , same area as in figure 1b is shown . 
 ( zusatzmaterial online / supplementals : film 2 ) b zweite mrt mit ferumoxtran - 10 8 wochen nach strahlentherapie ohne nachweis metastatischer lymphknoten entsprechend der region in abbildung 1b . 
axiale t1 - gewichtete vibesequenz links , axiale t2 * - gewichtete sequenz rechts . proach combining surgery and radiotherapy with or without antihormonal therapy have proven in principle that intensive local therapy may cure ~50% of patients with lymph node - positive prostate cancer [ 4 , 24 ]  . 
this can be deduced from the disappointing results with those treatment paradigms in elective lymph node radiotherapy based on calculated risk and from series with radiotherapy alone in patients with manistrahlenther onkol 2011 no . 
unfortunately in the most recent evaluation , this difference could no longer be detected ; a benefit was only seen in a subgroup that was , however , evidently counterbalanced by detrimental results in another subgroup [ 17 , 20 ]  . in a similar effort , the french genito - urinary group studied this question ( getug - 01 ) and also recently published negative results [ 19 ]  . 
while whole pelvic radiotherapy with conventional techniques and doses < 55 gy does not lead to an increased survival rate in patients with high or intermediate risk of lymph node metastasis in prostate cancer [ 6 , 19 ] , it definitely leads to increased toxicity [ 1 ]  . conventional dose radiotherapy of manifest metastatic lymph nodes results in a maximum of only 1030% biochemical relapse - free survival after 10 years [ 11 , 12 , 23 ]  . 
while the combination of radiotherapy and antihormonal therapy seems to improve results , biochemical relapse - free survival still falls short of 50% at 10 years [ 11 ]  . 
such escalated doses might also obviate concomitant hormonal therapy [ 911 , 26 , 27 ]  . intensity - modulated radiotherapy of the pelvis , which has become standard practice in many radiotherapy centers , improves nodal coverage and allows application of a reduced dose to radiosensitive organs , such as bowel and bladder , followed by a decreased rate of posttherapeutic morbidity [ 2 , 7 , 25 , 2830 ]  . 
 [ 21 ] reported encouraging results using ferumoxtran - 10 detecting metastatic lymph nodes before salvage radiotherapy . accurate lymph node staging and subsequent dose escalation in our patient led to an elimination of ferumoxtran - 10 positive lymph nodes and a decrease of psa value close to being undetectable after a very short time . 
this suggests that the treatment paradigm seems to be highly effective and , as a consequence of the limited volume treated to high doses , seems to confer tolerable toxicity . the second important consequence from this observation is that ferumoxtran - 10 mr lymphography is apparently well suited to be used in follow - up and may , beyond just following lymph node size , provide new insight into the kinetics of the response to lymph node treatments . technical note procedure for creating a three - dimensional ( 3d ) model for superficial hyperthermia treatment planning marianne linthorst , tomas drizdal , hans joosten , gerard c . 
van rhoon , jacoba van der zee1 purpose : to make a patientand treatment - specific computed tomography ( ct ) scan and to create a three - dimensional ( 3d ) patient model for superficial hyperthermia treatment planning ( shtp )  . patients , materials , and methods : patients with recurrent breast adenocarcinoma in previously irradiated areas referred for radiotherapy ( rt ) and hyperthermia ( ht ) treatment and giving informed consent were included . 
after insertion of the thermometry catheters in the treatment area , a ct scan in the treatment position was made . results : a total of 26 patients have been , thus far , included in the study . 
during the study period , five types of adjustments were made to the procedure : ( 1 ) marking the rt field with radioopaque markers , ( 2 ) making the ct scan after the first ht treatment instead of before , ( 3 ) using an airand foam - filled ( dummy ) water bolus , ( 4 ) a change to radiolucent catheters for which radioopaque markers were needed , and ( 5 ) marking the visible / palpable extent of the tumor with radioopaque markers , if necessary . 
im verlauf der studiendauer wurden fnf arten von anpassungen im verfahren vorgenommen : ( 1 ) markierung des bestrahlungsfeldes mit rntgendichten markern ; ( 2 ) das ct wurde nach der ersten ht behandlung gemacht statt voher ; ( 3 ) dabei wurde ein mit luft und schaum gefllter wasserbolus ( dummy ) verwendet ; ( 4 ) ein wechsel zu strahlendurchlssigen kathetern , fr die rntgendichte marker bentigt wurden ; ( 5 ) markierung des sichtbaren und tastbaren tumors mit rntgendichten markern , wenn ntig . 
jeder ct - schnitt wurde automatisch segmentiert in muskel , fett , knochen und ludas strahlenfeld , der thermometrie - katheter , applikator und tumor wurden , wenn angegeben , manuell mit dem segmentierungsprogramm iseg segmentiert . 
creating a 3d model for superficial hyperthermia treatment planning introduction at least 19 randomized studies have shown that adding hyperthermia ( ht ) to radiotherapy ( rt ) and / or chemotherapy leads to improved survival and tumor control in oncological patients without a significant increase in observed side effects [ 40 ]  . 
 [ 20 ] , the addition of ht to rt improved the complete response ( cr ) from 35% to 62% , and 2 - year local control ( lc ) from 28% to 46% . 
the tripling of the cr rate in various superficial tumors for reirradiation and high - dose ht vs rt and low - dose ht as demonstrated in a randomized study by jones et al . 
 [ 13 ] resulted in the inclusion of radiation plus ht in the 2007 breast cancer guidelines for recurrent breast cancer and other localized cancer recurrences by the national comprehensive cancer network ( nccn )  . 
in several clinical trials , a correlation between treatment outcome and thermal dose parameters was demonstrated [ 3 , 9 , 26 , 31 , 39 , 43 ]  . 
 simple approaches to describe a clinically delivered thermal dose include the use of maximum , average , or minimum temperature for the duration of the treatment or the use of measurements for temperature distribution , such as t10 or t90 ( the temperature level above which 10% or 90% , respectively , of the measurements was )  . 
the temperature distribution during clinical treatment is spatially inhomogeneous due to variable tissue properties and blood flow , and changes over time due to changes in blood flow [ 7 ]  . 
a disadvantage of thermal dose parameters is that these have been shown to depend on the number of measurement sites and on tumor characteristics such as blood flow and tumor size [ 4 ]  . major limitations for further improvement of treatment quality lay in the difficulty to improve dosimetry and in the inability to prescribe a specified thermal dose [ 6 ]  . 
furthermore , noninvasive thermometry ( nit ) by magnetic resonance imaging is not realistic for superficial hyperthermia treatment ( sht ) , and nit by microwave radiometry or ultrasound has not been shown to provide the required spatial resolution and temperature sensitivity . clinical data support that the specific absorption rate ( sar ) distribution is a valuable parameter to predict the cr [ 40 ]  . 
in patients with recurrent breast cancer , they observed a much higher lc rate after the introduction of a better heating technique , especially in the patients with larger tumors . in a follow - up to these findings , we started a clinical study to investigate whether the predicted three - dimensional ( 3d ) sar distribution from sht modeling is prognostic for treatment outcome in patients with breast cancer recurrences in a previously irradiated area [ 23 , 24 , 25 ]  . 
the study of the relationship between the calculated 3d sar distribution and the clinical outcome is still ongoing and will be reported later . we believe that this paper contains important information for other researchers with an interest in similar studies or designing procedures for implementation of htp as a routine . methods patients and treatment patients with recurrent breast adenocarcinoma referred for reirradiation ( 84gy , twice weekly ) and ht ( four times , once weekly , 60min , after rt ) , and with the possibility to place interstitial thermometry catheters in the treatment area were eligible for the study on predicted sar distribution as a prognostic parameter for temperature distribution and clinical outcome . 
ht was induced with 433 mhz , utilizing up to six lucite cone applicators ( lca ) , with a perfused water bolus between the skin and applicators [ 33 , 36 , 37 , 41 ]  . 
multipoint fiber - optic thermometry probes ( ftp - 5 medical array sensor , takaoka electric mfg , tokyo , japan ) are placed in the catheters and on the skin . specification of a ct scan the ct scans were performed with a siemens somatom sensation open with a large bore of 85 cthe resolution of the ct scans was 512 512 pixels , 3.0 mm slice thickness , a slice distance of 2.5 mm , and together this corresponds to a 115 mm3 voxel cube . 
between 120 and 140 slices with margins of 5 cm superiorly ( including the supraclavicular region ) and margins of 5 cm inferiorly ( including the thoracic diaphragm ) of the treatment volume were required . 
ma : makroskopisch , mi : mikroskopisch , rt : radiotherapie , ht : hyperthermie , chemo : chemotherpie , horm : hormonell therapie , b / a : vor / nach die erste hyperthermie behandlung . catheters rt field ct scan patient ma / mi target depth ( mm ) ma + marker 30 tumor size ( mm ) 20 18 120 111 114 40 51 67 150 90 150 114 75 130 39 36 150 145 70 55 135 45 70 70 46 23 32 28 24 15 no . 
 this appeared insufficient to create a patientand treatment - specific model for shtp : information about the margins of the rt field , the ht treatment position of the patient , the distance of the applicators from the skin , and the location of the tumor was lacking . 
a axial ct image of breast tissue demonstrating a marked rt field ( green ) , fat ( orange ) , muscle ( brown ) , bone ( yellow ) , air ( blue ) and moulds ( pink )  . 
 b vergrertes bild mit strahlenfeld - marker ( grn )  . marking the rt field in combination with reirradiation , the whole rt volume is the target for ht treatment [ 35 ]  . 
the ht applicators are placed such that the rt field is widely covered ; the rt target volume can , therefore , not be deduced from the position of the ht applicators . 
applikatoren bestehend aus lca - abdrcken ( nicht segmentiert ) und umgekehrten halterungen auf einem dummy - wasserbolus ( nicht sichtbar im ct - bild )  . ct scan timing and patient positioning water bolus in the first 8patients , the ct scan was made after the catheters were inserted , prior to the first ht treatment . 
in the next 18 patients , the ct scan was planned after the first treatment , or the treatment position was simulated before the ct scan was made . the position of the lcas had been marked on the skmoulds representing the lca footprints were used to show the position of the lca on the thoracic wall . 
at first ( in 7 patients ) , the moulds were placed 2 cm from the skin by stubs , simulating the thickness of the water bolus ( figures 2 and 3 )  . 
dieses axiale ct - bild zeigt einen tumor , markiert mit einem rntgendichten marker und einen dummy - wasserbolus ( nicht sichtbar im ct )  . bolus appeared inaccurate because there were no applicators to maintain its correct position ( figure 4 )  . 
relative permittivitt ( r ) , wrmeleitfhigkeit ( ) und massendichte ( ) der verschiedenen gewebe ( f = 433 mhz )  . ( s m1 ) ( kg m3 ) radiolucent catheters during the course of the study , a change was made from radioopaque to radiolucent catheters , because the radioopaque catheters were not available anymore . 
therefore , from patient 8 , the radiolucent catheters were made visible with radioopaque markers ( figure 6 )  . marking the visible and palpable tumor it is not possible to predict whether a tumor will be visible on the ct scan . 
therefore , the clinically apparent tumors were marked with a metal thread on the skthis is not always possible , e.g. , when there are many lesions or when the tumor is subclinical . 
 figure 7 shows the markers around the tumor , which by itself can be discriminated from the surrounding fat tissue . segmentation of ct images the process was started by displaying a ct image in the workstation screen . 
with an obtained dose difference ( dd ) < 2% and distance to agreement ( dta ) < 2 mm , these results are comparable to that achieved in radiotherapy treatment planning ( rtp )  . the ht physician first defined the anatomical structures in the ct images . 
the dielectric properties assigned to the tissues are described in table 2 [ 10 ]  . even though they may consist of significantly different tissues concerning dielectric and thermoregulatory properties ( e.g. , previous surgery and / or rt ) [ 2 ] , the tissue of any structure was considered to be homogeneous . 
the tumor was segmented to evaluate the position of a hot spot during treatment , to predict the total absorbed energy in the tumor , and to compare this with the measured temperatures . 
without segmentation of the tumor , the manual segmentation took 2 h ; with segmentation of the tumor , it could take up to 3 h . discussion in this article , we present the procedure of making a ct scan and segmenting the ct images to create a patientand treatment - specific model for shtp that represents the real patient treatment set - up . 
since the irradiated volume is the target for ht and the area covered by the applicators is larger than the rt field , markers were introduced for the rt field margins . 
the dummy water bolus was introduced to make the distance from the applicator to the skin more realistic than with the stubs on the corners of the dummies placed on the ska change from radioopaque to radiolucent catheters made it necessary to place markers in the catheters . tumors were not always visible on the ct scan . 
therefore , it was necessary to introduce marking of the visible / palpable tumor . in order to have the same patient positioning during the actual treatments as on the ct , the same ht physician and technicians should prepare all treatments , and photographs should be taken of the patient during treatment . 
 in the study of kumaradas and sherar [ 15 ] , the ct imaging was performed before the ht treatment to determine the position of the catheters , to predict the temperature profile , and to identify possible hot spots , but they do not provide details about the procedure they used to place the patient in the ct scanner . 
 [ 21 ] , the patient model with a head and neck tumor , treated with the hypercollar , was segmented from a ct scan that was made for rtp . a much mentioned drawback of the segmentation of the ct images is the time - consuming and subjective process , especially of the manual segmentation . 
the time for manual segmentation can be reduced by further improvements to the program , e.g. , by importing information on rt field margins from the rtp , like was done for head and neck patients [ 22 ]  . we are convinced that htp will be an important tool for quality assessment and believe that the sar distribution has the potential to be a ht dose parameter . 
we expect that the use of shtp will translate into better ht treatment control . acknowledgment this work is financially supported by a grant of the koningin wilhelmina fund ( dutch cancer society ) project emcr 20073837 . original article effect of photon - beam energy on vmat and imrt treatment plan quality and dosimetric accuracy for advanced prostate cancer marlies pasler1 , dietmar georg2 , holger wirtz1 , johannes lutterbach1 purpose : the goal of the research was to evaluate treatment plan quality and dosimetric accuracy of volumetric modulated arc therapy ( vmat ) and intensity - modulated radiotherapy ( imrt ) plans using 6 , 10 , and 15 mv photon beams for prostate cancer including lymph nodes . methods : in this retrospective study , vmat and imrt plans were generated with the pinnacle treatment planning system ( tps ) ( v9.0 ) for 10 prostate cancer cases . 
dosimetric plan verification was performed with a 2d ionization chamber array placed in a full scatter phanto results : no differences were found for target and oar parameters in low and high energy photon beam plans for both vmat and imrt . 
in vmat , > 96% of detector points passed the 3% / 3 mm criterion ; marginally better accuracy was found in imrt ( > 97% )  . conclusion : for static and rotational imrt , 15 mv photons did not show advantages over 6 and 10 mv high energy photon beams in large volume pelvic plans . 
die planverifikation wurde mit einer 2d ionisationskammer - matrix in einem festkrperphantom durchgefhrt . ergebnisse : es wurden keine unterschiede zwischen niedrigen und hohen energien fr zielvolumenund risikoorganparametern in vmatund imrt - plnen gefunden ( tabellen 2 und 3 , abbildung 2 )  . 
in 6 - mv - vmat - plnen wurde ein geringfgig hheres niedrigdosisvolumen ( normalgewebe : dmean = 16 , 47 gy ) als in 10und 15 - mv - plnen ( je dmean = 15 , 90 gy und 15 , 74 gy ) gefunden ; hnliche ergebnisse wurden fr imrt - plne ermittelt . 
vmat - plne erreichten einen gamma - index < 1 ( 3 mm abstand und 3% dosis ) fr > 96% der detektorpunkte ; imrt - plne erreichten > 97% der detektorpunkte ( abbildung 3 )  . 1lake constance radiation oncology center singenfriedrichshafen , singen , germany , 2department of radiotherapy , medical university vienna , vienna , austria . received : june 29 , 2011 ; accepted : september 13 , 2011 published online : november 29 , 2011 strahlenther onkol 2011 no . 
effect of photon energy on vmat and imrt plans schlussfolgerung : unsere studie zeigt fr groe beckenvolumina bei 15 - mv - vmatund - imrt - plnen keinen vorteil gegenber plnen mit 6 und 10 mv . 
this treatment technique enables treatment plans of similar or better quality to be achieved compared to step - and - shoot imrt [ 2 , 5 , 7 , 8 ] , while reducing monitor units ( mu ) and delivery time . 
for deep - seated targets treated with static imrt , the use of low photon beam energy in combination with a low number of fields results in islands of higher dose ( greater than 50% of prescribed dose ) distant from the target [ 22 ]  . 
 for imrt , there is generally a greater volume irradiated with low doses , which should be carefully considered since there is concern about secondary malignancies [ 1 , 11 ]  . 
high energy photon beams have the advantage of lower attenuation with depth and , therefore , result in a smaller low - dose irradiated volume , but they can also lead to an increased risk of secondary malignancies due to neutrons generated in the accelerator head at photon energies > 8 mv [ 14 , 24 ]  . 
vmat with 6 and 18 mv for primary prostate radiotherapy with a simultaneous integrated boost and showed that there was no advantage of high energy photons over low energy photons . 
we , therefore , designed a study with 6 , 10 , and 15 mv photon beams for 5 - field imrt and vmat plans for prostate cancer involving pelvic lymph nodes . 
the aims of the present study were to evaluate the impact of three different photon energies on target volumes , organs at risk and normal tissue , compare dosimetric parameters derived from step - andshoot imrt technique vs . 
vmat , and examine dosimetric accuracy for both techniques . methods and materials target volume and organ at risk delineation this study involved 10 high - risk prostate cancer patients after an incomplete resection . 
the primary planning target volume ( ptvpc + ln ) was defined to include a 7 mm margin around the pelvic lymph nodes in all directions and a 10 mm margin around the prostate bed in all directions except the posterior direction , where a 6 mm margin was added . 
the boost ptv ( ptvb ) was defined to include a 7 mm margin around the prostate bed in all directions except the posterior direction , where a 6 mm margin was added . 
rectum , bladder , small bowel , and femoral heads were contoured as organs at risk ( oar )  . treatment planning for dose calculation , the pinnacle ( v9.0 , philips radiation oncology systems , fitchburg , wi , usa ) collapsed cone algorithm was used . 
 imrt plans were routinely generated using five coplanar , equidistant fields , where an average of 60 and 20 segments were optimized for ptvpc + ln and ptvb , respectively . 
for each patient , three imrt plans were created using 6 , 10 , and 15 mv photon beams . vmat plans were generated using the smartarc algorithm , which has been described in detail by bzdusek et al . 
for each patient , three vmat plans were created using 6 , 10 , and 15 mv photon beams . planning objectives a primary plan for the ptvpc + ln and a separate plan for the ptvb were generated for each patient . 
dose constraints for target volumes and oar are listed in table 1 . to ensure a fair comparison , all plans for both vmat and imrt were generated using the same tps and planning parameters , i.e. , isocenter , dose grid ( 4 4 4 mm ) , prescription , and optimization objectives . 
dosisvorgaben fr zielvolumina , hilfsstrukturen und risikoorgane . structure ptvpc + ln ptvboost r80% r90% composite plan constraints rectum bladder small bowel femoral heads vring dose constraint dmean = 100% dmin 95% dmax 107% dmean = 100% dmax 107% dmax 80% dmax 90% d60% < 40 gy d40% < 50 gy dmax < 76 gy dmean < 55 gy dmax < 78 gy dmean < 28 gy dmax < 52 gy dmean < 15 gy dmax < 55 gy dmean < 18 gy dmax < 50 gy evaluation of treatment plans dosevolume histograms ( dvh ) were analyzed with respect to d98% , d50% , and d2% , representing doses to 98% ( nearminimum dose ) , 50% , and 2% ( near - maximum dose ) of both target volumes , respectively . 
the conformity index was calculated as cipaddick = tvpi / ( pi * tv ) , where tvpi is the target volume , tv , within the prescribed isodose volume pi [ 21 ]  . to quantify the dose to normal tissue , the volume vring was introduced ( figure 1 ) , which was defined as the volume inside the body contour excluding the ptvpc + ln plus a margin of 0.7 cm ( r90% ) in all directions . 
the relative volumes of the 10% , 30% , and 50% isodoses ( vx% / vbody = vtissuex% ) were determined as a surrogate for low dose volumes . the total treatment delivery time ( tt ) , defined as the time between the start of the first beam and the end of the last beam , was measured for all plans . 
the number of monitor units ( mu ) was assessed for each target volume per fraction . dose measurements dosimetric verification was performed using a 2d ionization chamber array ( seven29 , ptw - freiburg , freiburg , germany )  . 
illustration der hilfsstrukturen vring ( blau ) , r90% ( grn ) so wie des zielvolumens ptvpc + ln ( rot )  . octagonal solid water phantom ( octavius , ptw - freiburg )  . 
the percentage of detectors with a index < 1 and mean were evaluated [ 17 ] using two different criteria ( dose difference / distance to agreement ) : 3% / 3 mm and 2% / 2 mm . the parameters described above were recorded as continuous variables ; mean and standard deviations were also calculated . 
due to the small sample size , we considered superiority of one photon beam energy , if results were improved in at least 8 of 10 patients . results treatment plan evaluation most target and oar dose parameters in vmat and imrt plans showed no differences between high and low energy photon beams ( see tables 2 and 3 for details )  . 
 in vmat ptvboost , however , 15 mv plans generated a higher hi ( up to 20% ) and required on average 30 mu more per fraction than the 6 and 10 mv plans . 
better ( + ) or worse ( ) results are indicated for improvement or worsening of a parameter in at least 8 / 10 treatment plans ; no difference between different energies or techniques is shown with ( 0 )  . 
better ( + ) or worse ( ) results are indicated for improvement or worsening of a parameter in at least 8 / 10 treatment plans ; no difference between different energies or techniques is shown with ( 0 )  . 
however , energy dependency was not found in the vicinity of the target or in associated oar , but near the surface resulting in islands of higher dose [ 15 , 22 ]  . 
we found more low - dose - irradiated volume in normal tissue surrounding the target when using 6 mv photons compared to 10 and 15 mv photons for ptvpc + ln . 
hence , the clinical significance of low dose volumes for high - risk prostate cancer patients remains to be determined . concerning neutron generation for photon energies > 8 mv , wiezorek et al . 
 furthermore , when comparing imrt and vmat , significant improvements in target coverage , homogeneity , and oar sparing , similar to the findings of others [ 7 , 8 , 28 ] , were observed . 
this reduction in delivery time and mus in vmat compared to imrt is clearly an advantage in light of the risk of secondary malignancy [ 11 , 12 ] since the scattered radiation outside the treated volume is , being first - order , directly proportional to the mus applied . 
besides experimental verification of imrt for patient - specific quality assurance , independent monitor unit verification is an attractive tool for clinical routine and large scale implementation [ 9 , 10 ]  . 
 for vmat , existing independent dose calculation tools need to be further developed . in the present study , the effect of photon beam energy on large pelvic vmat and imrt plans was investigated for the first time . 
die grafik stellt die obere und untere quantile ( box ) , median ( balken ) , maximum und minimum ( whisker ) dar . imrt and vmat plans were verified with an ionization chamber array , since it allows an accurate , stable , and fast manner of dosimetry [ 30 ]  . 
the reported evaluations are in the range of what we measured for a criterion of 3% / 3 mm ( > 95% of film / 2d array passing the test )  . 
for vmat plans , the deviation between measurement and calculation is slightly higher than for imrt , which may originate from the fact that pinnacle uses a continuous , variable dose rate in the optimization process , whereas the linac is bound to binned dose rates . 
another possible reason for higher inaccuracy in vmat plans may be the 4 gantry spacing of the pinnacle smartarc algorithm : leaf positions are interpolated between two consecutive control points . 
however , gantry spacing is a user - defined parameter , conclusion for static and rotational imrt , 15 mv photons did not have advantages over 6 and 10 mv high energy photon beams in large volume pelvic plans . 
for the investigated tps and linac combination , 10 mv photon beams can be used as the general purpose energy for intensity modulation , which also minimizes the neutron issue with respect to peripheral doses . 
 original article prognostic impact of hemoglobin level and other factors in patients with high - grade gliomas treated with postoperative radiochemotherapy and sequential chemotherapy based on temozolomide a 10 - year experience at a single institution giampiero ausili cfaro1 , domenico genovesi1 , annamaria vinciguerra1 , marianna trignani1 , maria taraborrelli1 , antonietta augurio1 , roberto buonaguidi2 , renato j . 
galzio3 , marta di nicola4 background and purpose : to evaluate the influence of serum hemoglobin level prior to radiotherapy and other prognostic factors on survival in patients with high - grade gliomas . material and methods : from 20012010 , we retrospectively evaluated a total of 48 patients with malignant glioma treated with surgery and postoperative radiochemotherapy with temozolomide . 
the kaplanmeier method was applied to estimate the overall survival , while the log - rank test was applied to evaluate the differences on survival probability between prognostic subgroups . results : results were assessed in 43 patients . 
the prognostic factors analyzed were gender , age , extent of surgery , performance status before and after radiotherapy , sequential chemotherapy , hemoglobin level , and methylation of the o - 6 - methylguanine - dna methyltransferase gene ( mgmt )  . 
the median overall survival in patients with a hemoglobin level 12 g / dl was 12 months and 23 months in patients with a hemoglobin level > 12 g / dl . 
in this research , it was found that a low hemoglobin level before radiotherapy can adversely influence the prognosis of patients with malignant gliomas . key words : glioblastoma radiotherapy hemoglobin prognosis strahlenther onkol 2011 ; 187 : 77883 doi 10.1007 / s00066 - 011 - 1129 - x prognostische bedeutung des hmoglobinspiegels und anderer allgemeiner prognosefaktoren bei patienten mit high - grade - gliomen , die mit postoperativer radiotherapie und temozolomid - basierter sequentieller radiotherapie behandelt wurden . 
den einfluss des hmoglobinspiegels vor beginne der radiotherapie und anderer prognosefaktoren auf das berleben von patienten mit high - grade - gliomen abzuschtzen . patienten und methoden : von 2001 bis 2010 haben wir 48 patienten mit bsartigen gliom retrospektiv beobachtet , die mit chirurgie und temozolomid - basierter postoperativer chemotherapie behandelt wurden . 
die kaplan meier - methode wurde angewendet , um die globale berlebensrate abzuschtzen ; der log - rank - test wurde angewendet , um die unterschiede der berlebenswahrscheinlichkeit bei unterschiedlichen prognose - untergruppen abzuschtzen . 1 department of radiation oncology , g . 
dannunzio university , spirito santo hospital , pescara , italy , 3department of operative unit of neurosurgery and health sciences , university of laquila , san salvatore hospital , laquila , italy , 4 laboratory of biostatistics , department of biomedical science , g . 
dannunzio university , chieti , italy . received : may 19 , 2011 ; accepted : september 15 , 2011 published online : november 25 , 2011 strahlenther onkol 2011 no . 
die durchschnittliche gesamt - berlebenszeit betrug 18 monate ( 95%ci 1240 monate ) , die 1und 2 - jahres - berlebensraten lagen bei 62 , 2% und 36 , 3% ( abbildung 1 )  . 
die analysierten prognosefaktoren waren : geschlecht , alter , umfang des chirurgischen eingriffs , performancezustand vor und nach der radiotherapie , sequentielle radiotherapie , hmoglobinspiegel und methylierung des o - 6 - methylguanin - dna - methyltransferase - gen ( mgmt )  . 
bei univariater analyse zeigte sich eine signifikante korrelation des berleben mit den variablen performance , zustand ( vor und nach der chemotherapie ) , sequentielle chemotherapie und hmoglobin ( tabelle 2 , tabelle 3 )  . 
die durchschnittliche gesamt - berlebenszeit bei patienten mit 12 g / dl hmoglobin betrug 12 monate und 23 monate bei patienten mit > 12 g / dl hmoglobin ( abbildung 2 )  . 
die 1und 2 - jahres - berlebensraten betrugen 46 , 7% und 20 , 0% bei patienten mit 12 mg / dl und 69 , 6% und 45 , 7% bei patienten mit > 12 g / dl hmoglobin . schlussfolgerung : unsere ergebnisse besttigen den einfluss bewhrter prognosefaktoren auf die berlebensraten . 
wie unsere studie ermittelte , kann ein niederer hmoglobinspiegel vor beginn der radiotherapie die prognose von patienten mit bsartigen gliomen negativ beeinflussen . schlsselwrter : glioblastom radiotherapie hmoglobinspiegel prognose background and purpose primary tumors of the central nervous system ( cns ) are rare entities , totaling 12% of all solid tumors . 
among these , the most frequent are high - grade gliomas , which account for 45 50% of all gliomas [ 29 ] , with glioblastoma ( gbm ) being the most common and aggressive cns tumor [ 11 , 24 ]  . 
however , although important , the benefit of the multidisciplinary treatment is still small and the median survival is less than 1 year for gbm patients [ 13 , 14 , 31 , 33 ]  . 
 new adjuvant strategies have been developed in order to prolong survival ( high - dose rt , new chemotherapy agents , etc . ) , but it is also important to understand factors influencing prognosis and how they can guide the therapeutic approach and improve survival of these patients . 
many researchers have analyzed the impact of clinical features on prognosis , and several variables have been described [ 4 , 910 , 16 , 17 , 34 ] ; among the variables examined , some studies have considered the prognostic value of hemogloba low hemoglobin ( hb ) level is an unfavorable prognostic factor in various solid tumors , but this correlation is uncertain for high - grade gliomas . 
 [ 19 ] in a multivariate analysis of prognostic factors established that anemia may negatively influence outcome in patients with malignant gliomas . therefore , the purposes of this study were to evaluate overall survival of patients with high - grade gliomas and to determine the influence on survival of pretreatment hemoglobin level in the context of other common prognostic factors . patients and methods patients characteristics between 2001 and 2010 , 48 patients with high - grade glioma were treated in our department . 
there were 8 ( 18.6% ) anaplastic astrocitoma ( grade 3 who ) and 35 ( 81.4% ) gbm ( grade 4 who ) , including 22 ( 48.8% ) men and 21 ( 51.2% ) women ( 20 patients ( 46.5% ) were aged < 55years , while 23 patients ( 53.5% ) were aged 55years )  . 
there were 15 patients ( 34.9% ) with a hemoglobin level 12 g / dl and 28 patients ( 65.1% ) with a hemoglobin level > 12 g / dl . 
all patients received the prescribed radiotherapy dose of 60 gy over 6 weeks in daily fractions of 2 gy with a 6 mv linear accelerator with a three - dimensional treatment planning syste eleven patients ( 67% ) received whole brain irradiation ( 40 gy ) with an additional boost to the tumor area ( 20 gy ) ; the remaining patients ( 33% ) received partial brain irradiation . 
the prescribed dose was specified to the icru point ( isocenter ) and normalized to 100% . statistical analysis the variables evaluated were analyzed as follows : all qualitative factors were summarized as frequency and percentage and all quantitative factors as mean and standard deviation or median and range , when appropriate . 
 follow - up was defined as the time interval between surgery for primary cancer and the last follow - up visit ( last controls were performed in 2010 ) or the date of death . 
in the univariate analysis of survival time , the log - rank test was applied to compare the different categories of patients with respect to age , gender , extent of surgery , performance status ( ps ) before and follow - up ( months ) figure 1 . 
calculating the exponential of the regression coefficients from the cox model provided an estimate of the hazard ratio ( hr ) and the 95% confidence interval ( 95% ci ) , while the corresponding p value was based on the wald test . 
all statistical analyses were performed using spss software 11.0 ( spss inc , chicago , il , usa )  . results survival the median overall survival time of all patients was 18 months ( 95%ci 1240 months )  . 
the median overall survival time of patients was 12 months for patients with a hemoglobin level 12 g / dl and 23 months for patients with a hemoglobin level > 12 g / dl ( figure 2 )  . 
die durchgezogene linie bezieht sich auf patienten mit hb 12 , die gepunktete auf patienten mit hb > 12 ( log - rank test p = 0 , 038 )  . prognostic factors specific clinical and tumor features affecting survival were considered . 
 among variables evaluated in the univariate analysis , age , ps before and after radiotherapy , hemoglobin level , and mgmt status were included in the multivariate model ( table 3 )  . 
 there have been many advances in the treatment of patients with malignant gliomas ; however , despite neurosurgery , radiation therapy , and chemotherapy advances , survival of strahlenther onkol 2010 no . 
it is necessary to focus on clinical , tumor , and molecular features to understand the differences in survival and to determine the factors that have an impact on survival in order to increase survival . 
nevertheless , several trials provide evidence of a correlation between low a hemoglobin level and local failure or survival rates in patients treated with radiotherapy . the association between low hemoglobin level , hypoxia , and local radiotherapy failure for head and neck [ 1 , 2 , 6 , 23 , 28 , 30 ] and other solid tumors has also been established [ 12 , 2527 ]  . 
unfortunately , to date the impact of hypoxia and low hemoglobin level has not been extensively studied in malignant gliomas as in the other solid tumors ; thus , only limited data are available on the influence of this factor on clinical outcome of gliomas . 
 they observed a median survival of 12.1 months for patients with a hemoglobin level > 12 g / dl , compared to 7.9 months for patients with a hemoglobin level 12 g / dl . 
in our study , we reaffirmed the prognostic impact of ps before radiotherapy , but in contrast to other series we were not able to demonstrate any correlation between age and survival . 
pcr and immunohistochemistry ( ihc ) techniques are employed to define a threshold for detecting methylation levels and this permits a high degree of standardization . in our study , assessment of mgmt status was performed on a subgroup of patients ( 28 / 43 ) submitted to surgery more recently and a low expression of mgmt was not a significant factor for prognosis . 
a separate study about prognostic factors in who grade iii glioma is necessary because of the difference observed in the outcome for grade iv glioblastoma using the same treatment protocols [ 15 , 34 ]  . our experience also suggests that a low hemoglobin level is correlated with shorter overall survival . 
intensity modulated radiotherapy ( imrt ) marlies pasler1 , holger wirtz1 , johannes lutterbach1 background and purpose : to compare plan quality criteria and dosimetric accuracy of step - and - shoot intensity - modulated radiotherapy ( ss - imrt ) and volumetric modulated arc radiotherapy ( vmat ) using two different gantry rotation times . patients and methods : this retrospective planning study based on 20 patients was comprised of 10 prostate cancer ( pc ) and 10 head and neck ( hn ) cancer cases . 
for each patient , one ss - imrt plan and two vmat plans at 90 s ( vmat90 ) and 120 s ( vmat120 ) per arc were generated with the pinnacle planning systetwo arcs were provided for the ptv plans and a single arc for boost volumes . 
dosimetric verification of the plans was performed using a 2d ionization chamber array placed in a full scatter phanto results : vmat reduced delivery time and monitor units for both treatment sites compared to imrt . 
in the vmat plan verification , an average of 97.1% of the detector points passed the 3 mm , 3% criterion , while in imrt verification it was 98.8%. conclusion : vmat90 , vmat120 , and imrt achieved comparable treatment plans . 
intensittsmodulierte strahlentherapie ( imrt ) ziel : vergleich von planqualitt und dosimetrischer genauigkeit von step - and - shoot intensittsmodulierter strahlentherapie ( ss - imrt ) und volumetrisch modulierter rotationstherapie ( vmat ) bei zwei unterschiedlichen gantry - rotationszeiten . patienten und methoden : diese retrospektive planungsstudie basierte auf 20 patienten : 10 mit prostatatumor ( pc ) und 10 mit kopf - hals - tumor ( hn )  . 
fr die dosimetrische verifikation der bestrahlungsplne wurden eine 2d ionisationskammer - matrix und ein oktagonales festkrperphantom verwendet . ergebnisse : im vergleich zur imrt wurden durch vmat - plne die bestrahlungszeit und die anzahl der monitoreinheiten fr beide behandlungslokalisationen reduziert ( tabellen 2 und 3 )  . 
fr hn - patienten konnte mit vmat120 eine vergleichbare risikoorganschonung sowie eine bessere zielvolumenabdeckung als mit vmat90 erzielt werden ( siehe tabellen 1 und 3 , sowie abbildung 2b )  . 
vmat - plne erreichten einen gamma - index < 1 ( 3 mm abstand und 3% dosis ) fr 97 , 1% der detektorpunkte , imrt - plne erreichten 98 , 8% der detektorpunkte . schlussfolgerung : vmat90 , vmat120 und imrt erzielten vergleichbare bestrahlungsplne . 
varying gantry rotation time in vmat introduction the development of the intensity - modulated radiotherapy ( imrt ) technique has enabled the delivery of highly conformal dose distribution to complex shaped targets , while limiting radiation damage to critical organs [ 12 ]  . 
this might result in larger uncertainties of treatment due to potential intrafraction patient motion and patient discomfort [ 13 ]  . volumetric modulated arc therapy ( vmat ) is a novel extension of imrt using superimposing arcs [ 29 ] and provides flexibility in the delivery by varying angular dose rate and gantry speed during dynamic movements of jaws and multileaf collimators ( mlc ) [ 2 , 18 ]  . 
 with the recent availability of several commercial products such as varians rapidarctm and elektas vmattm , intensity - modulated arc therapy techniques have gained interest in clinical practice [ 1 , 4 , 6 , 7 , 9 , 17 , 20 , 24 , 25 , 28 ]  . 
advantages of vmat over imrt are the reduction in monitor units ( mu ) and delivery time , hence , better delivery efficiency . both gantry speed and mlc speed are limited ; thus , better vmat plans might be generated when allowing more time per gantry rotation . 
in vmat , slower gantry movement would allow some leaves to travel to their correct positions from one control point to the next and to impart sufficient variations in dose rate between control points . 
the effect of increasing the rotation time in favor of improved dosimetric plan quality has not been investigated yet [ 3 ]  . this comparative study aims to evaluate vmat plans for complex shaped target volumes with special focus on the effect of gantry rotation time on plan quality . 
for the parotid glands , dmean < 26 gy was intended if they were located outside the high dose target volume . to ensure a fair comparison , the plans for all three techniques were generated using the same planning system and plan ning parameters such as isocenter , dose grid ( 4 4 4 mm ) , prescription , and optimization objectives . 
the only varying parameter was the weighting factor for the objectives . imrt plans for the dose calculation , the pinnacle collapsed cone algorithm ( v9.0 , philips radiation oncology systems , fitchburg , wi , usa ) was used . 
 imrt plans for pc were routinely generated using five coplanar , equidistant fields of 15 mv , where an average of 40 and 20 segments were optimized for ptv and boost , respectively . 
boost plans were generated using 47 beams and 4060 segments . patients and methods vmat plans two clinically relevant planning situations were investigated : prostate cancer ( pc ) and head and neck cancer ( hn )  . 
head and neck cancer patients were included if they had an advanced oropharyngeal tumor and required radiotherapy due to incomplete resection or pathologically proven lymph node metastases [ 8 ]  . 
r80% covered the area from 0.7 cm to 2 cm around the target volume , with a maximum dose in the pinnacle system v9.0 , vmat plans are optimized by the utilization of the smartarc algorithm , which was described in detail by bzdusek et al . 
vmat90 refers to a maximum delivery time of 90 s per arc ( allowing a total of 180 s for the double arc plan for ptvs ) , and vmat120 refers to 120 s per arc , overall 240 s for double arc plans . 
for hn plans , the start and stop gantry angles varied due to the shape of the target volume from a partial arc ( starting at 140 , stopping at 220 ) to a full 360 arc . 
the final gantry spacing was chosen at 4 for all plans . evaluation of treatment plans dosevolume histograms ( dvh ) were analyzed with respect to ptv coverage v95% ( relative volume of the target volume receiving at least 95% of the prescription dose )  . 
for evaluation , the 2d index was calculated using verisothe percentage of detectors with index < 1 at the 3% dose difference , 3 mm distance - to - agreement criterion and the mean were used as a measure of dosimetric accuracy [ 15 ]  . 
qualitatively , vmat plans are more conformal with fewer high dose areas in the surrounding normal tissue ( table 1 )  . the required mus for ptv were reduced by up to 88% in some cases in vmat90 compared to imrt ; the maximum mu reduction in vmat120 was 67% compared to imrt . head and neck cancer vmat plans for hn cases resulted in relatively high hi compared to imrt plans ( table 3 ) , similar to pc cases . 
the best ci and v95% were found in vmat120 plans . in table 1 , it is shown that the spinal cord received up to 30% higher maximum dose in vmat compared to imrt ( clinically unacceptable ) , which is due to objective limitations in smartarc planning , i.e. , it is not allowed to set constraints in terms of boundary values of top priority on objectives in vmat plans , whereas constraints are allowed in imrt plans . 
illustration der struktur vring ( blau ) , r90% ( grn ) und ptv ( rot )  . index ( hi ) was defined as hi = ( d5%d95% ) / dmean , where dn% is the minimal dose delivered to the percentage of the target volume . 
the reported values for targets were chosen to ease comparison with other studies [ 1 , 9 , 19 , 25 , 30 ]  . for all oars , dmax and dmean were assessed from the composite plan , which is the combination of ptv and boost plan . the total treatment delivery time ( tt ) , defined as the time between the start of the first beam and the end of the last beam , was measured for all plans . 
 the number of monitor units ( mu ) was assessed for each target volume per fraction . dose measurements dosimetric verification was performed using the 2d ionization chamber array ( seven29 , ptw - freiburg , freiburg , germany )  . 
abbreviations : see table 1 ; v95% : relative volume of ptv / boost volume receiving 95% of the prescription dose , hi : homogeneity index , ci : conformity index , dmax% : percentage maximum dose , tt : treatment time , ett : estimated treatment time . 
ptv ( rot ) : primres planungszielvolumen ; imrt : intensittsmodulierte strahlentherapie ; v90 ( v120 ) : volumetrisch modulierte rotationsbestrahlung mit einer maximalen bestrahlungszeit von 90 ( 120 ) sekunden pro rotation . 
the only varying parameter was the weighting factor for the objectives . the aim of this study was to evaluate the influence of gantry speed on plan quality and to compare both vmat90 and vmat120 with imrt . 
the linac used binned dose rates ; consequently , if the dose rate has to be slightly decreased due to limitations in the velocity of mlcs , jaws , and gantry motion , dose rate is reduced by 50% . 
 the maximum delivery time constraint in the pinnacle planning system is a soft constraint for the optimizer and affects the optimizer efficiency : we observed elongated , small segments in vmat120 plans ; in vmat90 plans the corresponding segment areas appear larger . 
the efficiency of the optimizer is , therefore , reduced in vmat120 plans for pc cases . comparing vmat and imrt , vmat plans resulted in better conformity but poorer homogeneity compared to imrt plans in our study . 
 [ 4 ] ; however , other investigations found both homogeneity and conformity improved by rapidarc compared to imrt [ 6 , 7 ] , similar homogeneity and conformity index [ 23 ] , or inferior conformity for vmat [ 27 ]  . 
 the reduction in delivery time and mus in vmat90 and vmat120 compared to imrt addresses the hypothesized increased risk of secondary malignancy , which is a major concern with imrt [ 10 , 11 ] , since the scattered radiation impinging on the patients body outside the treated volume is , at first - order , directly proportional to the mus applied . 
a further benefit of the time savings is the potential to reduce the effects of intrafractional motion and to allow increasing image guidance , e.g. , pretreatment cone - beam ct . 
dvh analysis for vmat plans indicated fewer high dose areas in normal tissue but at the same time there is more low - dose - irradiated volume , which should be carefully considered since the incidence for second malignancies increases with larger volumes to lower doses [ 10 ]  . quality assurance remains a challenge because vmat is a complex technique . 
for both vmat90 and vmat120 plans , the deviation between measured and calculated values is slightly higher than for imrt which shows that further improvement of the optimization and dose calculation process is necessary to improve the planning process . 
 original article radiotherapy for prevention and therapy of gynecomastia due to antiandrogen treatment in prostate cancer patients a patterns - of - care study burkhard neu1 , verena sautter1 , felix momm2 , ute melcher1 , heinrich seegenschmiedt3 , oliver micke4 , marie - luise sautter - bihl1 background : gynecomastia is a frequent side effect of antiandrogen therapy for prostate cancer and may compromise quality of life . 
although it has been successfully treated with radiotherapy ( rt ) for decades , the priority of rt as a preferred treatment option has recently been disputed as tamoxifen was also demonstrated to be effective . 
moreover , the participants were asked whether they were interested in participating in a prospective study . results : from a total of 294 institutions , 146 replies were received , of which 141 offered rt for gynecomastia . 
 the clinical results indicate that rt is a highly effective and well - tolerated treatment . key words : gynecomastia prostate cancer radiotherapy tamoxifen antiandrogen therapy strahlentheronkol 2011 ; 187 : 7717 doi 10.1007 / s00066 - 011 - 2283 - x strahlentherapie der brustdrse zur prophylaxe und therapie der androgeninduzierten gynkomastie bei prostatakarzinom hintergrund : die gynkomastie ist eine hufige nebenwirkung der antiandrogenbehandlung beim prostatakarzinom und kann die lebensqualitt beeintrchtigen . 
obwohl sich die strahlentherapie in der prophylaxe und therapie der gynkomastie seit jahrzehnten bewhrt hat , wird ihr stellenwert als primre behandlungsoption neuerdings in frage gestellt , da auch tamoxifen als effektiv beschrieben wurde . 
die gesamtdosis betrug bis zu 20 gy bei der prophylaktischen und 1 klinik fr radioonkologie und strahlentherapie , klinikum karlsruhe , karlsruhe , germany , 2 klinik fr strahlenheilkunde , universittsklinikum freiburg , freiburg i.br. , germany , 3 strahlenzentrum hamburg , hamburg , germany , 4 klinik fr strahlentherapie und radioonkologie , franziskus - hospital , bielefeld , germany . received : june 2 , 2011 ; accepted : june 16 , 2011 published online : november 29 , 2011 strahlenther onkol 2011 no . 
 schlussfolgerung : die prophylaktische und symptomatische strahlentherapie wird im deutschsprachigen raum flchendeckend angewandt , die patientenzahlen sind jedoch kledie klinischen resultate weisen darauf hin , dass die strahlentherapie eine hoch effektive und problemlos tolerierte behandlung darstellt . schlsselwrter : gynkomastie prostatakarzinom strahlentherapie tamoxifen antiandrogentherapie introduction author antiandrogen therapy ( at ) has substantially improved outcome of prostate cancer treatment ; however , a negative side effect is that gynecomastia develops in 6070% of patients [ 24 ]  . 
this issue is of increasing clinical relevance as at plays a growing role in adjuvant , curative , and palliative therapy of localized , locally advanced , and metastasized prostate cancer and is often recommended for several years [ 28 ]  . 
even though for decades numerous studies had shown that breast radiotherapy ( rt ) was effective both in the prophylactic ( table 1 ) [ 7 , 15 , 22 , 26 , 29 , 30 ] and the therapeutic [ 1 , 3 , 21 ] setting ( table2 ) , urologists no longer seem to consider rt routinely [ 18 ] or , even more , actually doubt its value [ 17 ] , since tamoxifen had been demonstrated as an effective systemic treatment alternative in a small randomized trial [ 19 ]  . 
in order to gain quantitative information whether breast irradiation is a vanishing tool in the management of at - induced gynecomastia , the present paper aims to provide a survey of indications , frequency , dose schedules , and techniques of rt in the daily practice of rt institutions in germany , austria , and switzerland . 
 di lorenzo 2005 widmark metzger tyrrell rupp ozen 1974 2010 2004 1980 2003 1986 year fass 53 72 50 50 51 52 54 79 87 40 referred to patient numbers , indications , rt technique , dose and if available results of treatment in terms of effectiveness to prevent gynecomastia and to alleviate symptoms if breast enlargement was already manifest . 
 information was obtained from 29 university departments , 65 hospital facilities , 43 private practices , and 19 so - called medical care centers ( 10 cases with double functions , e.g. , private practice associated with a hospital ) responded . breast irradiation for gynecomastia is offered by 97% radiation oncologists , whereas only five ( 3% ) departments do not treat these patients at all . 
 prophylactic and symptomatic radiotherapy a total of 136 institutions ( 96% ) irradiate patients before initiation of at and 77 departments ( 55% ) treat more patients in the prophylactic than in the symptomatic setting ( figure 2 )  . 
of the 129 departments treating patients for manifest gynecomastia , 39 ( 30% ) employed rt even after long - standing symptoms , whereas in 87 institutions ( 67% ) no indication was seen in this situation . 
 treatment technique in the majority ( 68% ) of the departments ( n = 95 ) , rt was performed without simulation using visually designed fields for clinical alignment , the remaining institutions used 3d planning ( n = 31 ) with or without simulation ( figure 3 )  . 
 field sizes varied considerably : the smallest specified field was an electron tube of 3cm diameter and the largest was 1015 cmost frequently the field size was 1010cm ( 42 institutions , 30% ; figure 4 )  . 
the 3 institutions with the highest rate of side effects used electron beams and observed erythema in 66% ( 53 gy ) , 91% ( 44 gy ) , and 100% ( 54 gy )  . 
one institution reported hyperpigmentation as a late result in 9.4% of the patients after single fraction rt with 12 gy electrons . 12x12 10x10 individually 8x10 field size [ cmxcm ] figure 4 . 
 dose and fractionation the total dose for prophylactic breast irradiation varied between 9 and 24 gy ; for symptomatic rt , total doses between 9 and 40 gy were applied . 
consecutively , erd was between 15.6 discussion the present patterns - of - care study shows that prophylactic and symptomatic rt for gynecomastia is used in the majority of rt institutions . 
relating to the growing number of prostate cancer patients who receive antiandrogen treatment , this indicates that rt is not comprehensively used as a routine tool to prevent or treat gynecomastia . 
 in accordance with the literature ( tables 1 and 2 ) , our survey confirms the effectiveness of rt by trend : gynecomastia was successfully prevented in 60100% of patients ( table 3 ) , whereas regression of an already manifest breast enlargement was only achieved in a minority of cases ( table 4 )  . 
prevention and therapy of gynecomastia due to antiandrogen treatment in pc patients 94 88 60 51 36 33 88 36 33 11 6 - 12 6 - 15 8 - 12 9 - 12 electron energy [ mev ] figure 5 . 
 in the literature , there is a large variety of treatment schedules and in the absence of evidence indicating the optimal regimen , guidelines or standard schedules have not been developed . 
 10 - 12 individually most institutions who answered our questionnaire reported using direct anterior electron fields with energies according to clinical estimation of tissue thickness or the peri - mamillary region ( 618 mev ) , 36 reported a defined standard energy for all patients ( 6 , 8 or 9 mev ) ( figure 5 )  . 
published studies show variations between one and four fractions with single doses of 312 gy and total doses up to 40 gy in the symptomatic setting ( tables 1 and 2 ) .in order to validate the effectiveness of different fractionation schedules , it appears reasonable to compare the biologically effective dose in terms of erd = n d ( 1 + d / ) [ 8 ] , assuming an ratio of 10 . 
of prophylactically treated patients total dose ( gy ) single dose ( gy ) prevention of gynecomastia 22 60 19 27 83 10 20 36 12 22 53 60 68 83 66 88 92 table 4 . 
 either alone ( n = 51 ) or in combination with 10mg tamoxifen daily for 24 weeks ( n = 50 ) or with single dose irradiation ( 12 gy electrons ; n = 50 )  . 
evidently , the patient number ( 50 per arm ) of this multicenter trial was small and the technique ( single dose rt without individual treatment planning , standard size of 5 cm around the nipple , and an energy of 612 mev ) may be of suboptimal effectiveness . another aspect is the durability of the treatment effect , which is limited to the time of intake : in a randomized doseescalation study using 120 mg tamoxifen in addition to bicalutamide for 12 months , a dose - dependent effect on prevention of gynecomastia was observed during medication . 
 as antiandrogen medication is often applied over years [ 4 , 25 , 28 ] , patients who receive comedication with tamoxifen over a prolonged period may be at risk of systemic side effects , like cardiovascular complications and thromboembolism , which might add to those already produced by bicalutamide [ 14 ]  . 
 recently , the value of radiotherapy as a preferential treatment option was questioned [ 13 , 17 , 18 ] as tamoxifen had been propagated as an effective drug to prevent gynecomastia [ 2 , 9 , 23 ]  . 
tamoxifen , 150mg bicalutamide was administered in contrast , rt has virtually no side effects [ 5 , 7 ] ; in our survey , skin reactions were only seen with single dose treatment and frequently after orthovolt x - ray use . 
on the other hand , gynecomastia is not a negligible or merely cosmetic side effect , as it may lead a substantial number of patients ( 16% ) to withdraw from their hormonal treatment [ 26 ] at the expense of oncological safety . 
the psychological impact of gynecomastia on the physical appearance should , therefore , not be underestimated [ 27 ] especially as increasing attention has recently been turned on quality of life aspects in the treatment of prostate cancer [ 10 , 20 ]  . as increasing effort is made to refine the technique of radiotherapy of the prostate [ 11 , 12 , 28 ] , it is plausible to strahlenther onkol 2011 no . 
such a study may provide insights about the optimal treatment schedule and a definite answer to the question which treatment modality is superior and provide a basis to elaborate guidelines for prevention of this frequent and bothersome side effect . 
 original article hematogenous metastases in patients with stage i or ii endometrial carcinoma pawe blecharz1 , krzysztof urbaski1 , anna mucha - maecka2 , krzysztof maecki2 , marian reinfuss2 , jerzy jakubowicz1 , piotr skotnicki2 aims : the aim of this study was to present the characteristics , methods of treatment , and the survival of patients with hematogenous metastases from endometrial carcinoma , free from local and other distant recurrences . 
 patients and methods : in 1 , 610 endometrial carcinoma patients managed with surgery and postoperative radiotherapy , we defined hematogenous metastases as a tumor spread to the lung or other sites via hematogenous routes . results : a total of 110 patients with stage i and ii endometrial carcinoma , presenting with 134 metastases sites ( 69 in the lungs , 32 in the liver , 23 in the bones , and 10 in the brain ) , were observed . 
primary treatment consisted of surgery in patients with solitary metastases to the lung ( 30 patients ) , liver ( 2 patients ) , and brain ( 2 patients )  . 
 presenting with a 36 - month survival rate were 11.6% ( 8 / 69 ) of patients with metastases to the lungs , 6.3% ( 2 / 32 ) of patients with metastases to the liver , 8.7% ( 2 / 23 ) of patients with metastases to the bones , and 20.0% ( 2 / 10 ) of patients with metastases to the bra conclusions : hormonal therapy and chemotherapy play a major role in the palliative management of patients with hematogenous metastases from endometrial carcinoma to the liver , lungs , and bones . 
radical treatment in patients with metastases to the lung or liver consists of resection of the metastasis combined with chemoand / or hormonotherapy for metastases to the bones treatment consists of radiotherapy + chemotherapy , for metastasis to the brain treatment consists of resection combined with radiotherapy . key words : endometrial carcinoma hematogenous metastases treatment results strahlenther onkol 2011 ; 187 : 80611 doi 10.1007 / s00066 - 011 - 2250 - 6 hmatogene metastasierung bei patientinnen mit endometriumkarzinom im stadium i und ii ziel : darstellung von charakteristika , behandlungsmethoden und berleben von patientinnen mit hmatogenen metastasen des endometriumkarzinoms ohne lokalen und fernrezidive . 
 patienten und methoden : bei 1610 patientinnen mit endometriumkarzinom , die mit operation und postoperativer strahlentherapie behandelt worden waren , definierten wir hmatogene metastasen als ausbreitung bsartiger tumoren in die lungen oder andere regionen ber die blutbahn . 
 ergebnisse : wir beobachteten 110 endometriumkarzinom - patientinnen , stadien i und ii , bei denen 134 metastasenlokalisatione festgestellt wurden : 69 in den lungen , 32 in der leber , 23 in den knochen und 10 im gehirn . 
nach 36 monaten betrug die berlebensrate 11 , 6% ( 8 / 69 ) der patientinnen mit lungenmetastasen , 6 , 3% ( 2 / 32 ) der patientinnen mit lebermetastasen , 8 , 7% ( 2 / 23 ) der patientinnen mit knochenmetastasen und 20 , 0% ( 2 / 10 ) der patientinnen mit gehirnmetastasen . 
die radikale behandlung bei lungenoder lebermetastasen umfasst chirurgische metastasenresektion und adjuvante chemound / oder hormontherapie , bei knochenmetastasen strahlenplus chemotherapie und bei gehirnmetastasen chirurgische metastasenresektion und adjuvante strahlentherapie . schlsselwrter : endometriumkarzinom hmatogene metastasierung behandlung ergebnisse 1department of gynecologic oncology , center of oncology maria skodowska - curie , memorial institute , krakw , poland , 2department of radiation oncology , center of oncology maria sklodowska - curie memorial institute , krakw , poland . received : december 12 , 2010 ; accepted : june 16 , 2011 published online : november 17 , 2011 strahlenther onkol 2011 no . 
hematogenous metastases in stage i or ii endometrial carcinoma introduction endometrial carcinoma ( ec ) is the most common invasive malignancy of the female reproductive tract [ 12 , 17 , 19 , 27 , 28 , 34 , 35 , 40 , 47 ]  . 
while the majority of patients will be found to have early stage disease , thereby maintaining a reasonable prognosis , local and / or distant recurrences occur in all stages of initial disease and are uniformly associated with poor survival [ 7 , 10 , 16 , 17 , 19 , 21 , 24 , 27 , 37 , 39 , 40 , 44 , 47 , 50 , 53 , 54 ]  . 
pelvic lymphadenectomy was performed in 11 ( 10% ) patients considered by the surgeon to be suspicious for lymph nodes metastases ; all these patients were pathologically negative for lymph node spread . by the year 2000 , surgery alone was applied only to endometrial cancer patients with figo ia stage and g1 histology . 
 all patients from the studied group underwent postoperative radiotherapy . a total of 22 women ( figo stage ia , ib g2 , g3 ) were treated with external irradiation alone ( 20% ) ; 88 patients ( 80% ) also received a brachytherapy vaginal cuff boost . 
external irradiation was delivered using the four - field box technique , vaginal boost with either low ( ldr ) ( 79 patients ) or high ( hdr ) ( 9 patients ) dose rate technology . 
the external beam dose was 50gy ( 5 fractions per week , 2gy per fraction ) ; the median brachytherapy dose was 30gy ( range , 2540gy ) for ldr applications and 12 gy ( range , 816 gy ) for hdr applications . the median relapse - free interval between the primary diagnosis and the first evidence of hm in patients with hm was as follows : lungs , 29 months ( range , 2546 months ) ; liver , 32 months ( range , 664 months ) ; bones , 26 months ( range , 536 months ) ; and brain , 28 months ( range , 1753 months )  . 
 in the group of 110 patients presented , 134 metastases sites were observed ( table 1 ) : 69 patients had hm to the lung ( 45 solitary , 10 multiple , and 14 multiple + others , i.e. , liver , bones , or brain ) , 32 patients had hm to the liver ( 14 solitary , 18 multiple + others , i.e. , lung , bones , or brain ) , 23 patients had hm to the bones ( 6 solitary , 4 multiple , and 13 multiple + others , i.e. , lung or liver ) , and 10 patients had hm to the brain ( 6 solitary , 1 multiple , and 3 multiple + others , i.e. , lung or liver )  . primary treatment of hm consisted of surgery in patients with solitary metastases to the lung ( 30 patients ) , liver ( 2 patients ) , and brain ( 2 patients )  . 
six patients with metastases to the brain and 19 patients with metastases to the bones were treated with short - term , split - course radiotherapy , composed of 2 series of 20 gy in 5 fractions each , 4 weeks apart . 
three patients with multiple metastases to the bones received lower half - body irradiation with single dose of 7 gy . progestins and combination chemotherapy were the most commonly used therapies for our patients . 
mostly progestins ( mpa , ma ) or doxorubicin alone were given during the period from 19851995 ; thereafter combination chemotherapy ( adr + cddp , adr + cbdca , adr + cddp + paclitaxel , cbdca + paclitaxel ) , or combination chemotherapy and endocrine therapy were used . 
 of the remaining 24 patients , chemotherapy was interrupted before completion for progression of disease ( 12 patients ) , worsening of ps ( 4 patients ) , patients refusal ( 2 patients ) , and unacceptable toxicity ( 6 patients ; all grade 34 hematological toxicity )  . 
mpa : medroxyprogesteronacetat , ma : megestrolacetat , adr : doxorubicin , cddp : cisplatin , cbdca : carboplatin , bmpr : palliative knochenmetastasenbestrahlung ( 20 gy / 5 fraktionen / 5 tage ) , wbpr : palliative ganzhirnbestrahlung ( 20 gy / 5 fraktionen / 5 tage ) , hbi : halbkrperbestrahlung , wbrt : ganzhirnbestrahlung ( 50 gy / 25 fraktionen / 5 wochen )  . site / number of hm methods of treatment no . 
mpa : medroxyprogesteronacetat , ma : megestrolacetat , adr : doxorubicin , cddp : cisplatin , cbdca : carboplatin , bmpr : palliative knochenmetastasenbestrahlung ( 20 gy / 5 fraktionen / 5 tage ) , wbrt : ganzhirnbestrahlung . site of lung number of patients methods of treatment liver bones 2 brain resection of metastasis + progestins ( mpa 6 patients , ma 1 patient , anastrozole 1 patient ) resection of metastasis + chemotherapy ( adr + cbdca ) bmpr + chemotherapy ( adr + cddp ) resection of metastasis + wbrt ( 2 / 15 ) rr and a pft of 3 months , chemotherapy alone or with mpa / bmpr resulted in a 20.0% ( 3 / 15 ) rr and a pft of 4 months . in the group of 23 patients with hm to the bones , 12 - , 36 - , and 60 - month survival rates were 21.7% ( 5 / 23 ) , 8.7% ( 2 / 23 ) , and 8.7% ( 2 / 23 ) , respectively . 
endocrine therapy with bmpr / hbi offered a 20.0% ( 2 / 10 ) rr and a pft of 3 months ; chemotherapy alone or with bmpr resulted in a 46.2% ( 6 / 13 ) rr and a pft of 11 months . in the group of 10 patients with hm to the brain , the 12 - , 36 - , and 60 - month survival rate was 20.0% ( 2 / 10 ) and the median survival was 4 months . 
two patients treated with stereotactic radiosurgery + wbrt survived 10 and 11 months , respectively , and died with distant recurrences ( peritoneal carcinosis and paraaortic nodes ) , but without recurrences in the bra the characteristic methods of treatment of 14 patients of the present group surviving more than 60 months are shown in table 2 . 
the authors emphasize a higher risk of distant metastases in nonendometrioid subtypes of ec [ 16 , 19 , 31 , 32 ]  . as reported in the literature , pulmonary metastases are the most common site of hm from ec appearing in 2.38.3% of cases [ 68 , 20 , 21 , 23 , 25 , 34 , 35 , 40 , 42 ] : 4.3% ( 69 / 1 , 610 ) was diagnosed in the present group of patients free from local or other distant recurrences . 
in the series reported in the literature , the incidence of brain metastases ranges from 0.30.9% [ 11 , 14 , 15 , 22 , 23 , 50 ] , which is in accordance with the value of 0.6% ( 10 / 1610 ) in our group of patients . in the present group of patients , 75.5% of hm appeared within the first 3 years , which is comparable with that reported in the literature [ 7 , 19 , 21 , 30 , 35 , 54 ]  . 
in the literature , the survival rate for these patients is generally poor , with 1 - year survival rates of 2030% and 5 - year survival rates of less than 10% [ 6 , 8 , 9 , 20 , 23 , 42 , 50 ]  . 
data from the literature and our own observations indicate that resection of pulmonary metastases combined with chemoand / or hormonotherapy is a cornerstone treatment for patients with hm to the lung from ec , especially those with solitary hm [ 4 , 8 , 23 , 41 ]  . 
 [ 23 ] successfully treated patients with bilateral multiple pulmonary metastases with surgery followed by chemotherapy consisting of paclitaxel and carboplatin . in our group of patients , single chemotherapy ( adr ) alone or with mpa offered a 22.2% ( 2 / 9 ) response rate ( rr ) and progression - free time ( pft ) of 5 months , combination chemotherapy alone resulted in a rr of 43.8% ( 7 / 16 ) and a pft of 9 months , while endocrine therapy resulted in a 25% rr . 
 the data from the literature has shown that in patients with advanced or recurrent ec , adr + cddp , cbdca + paclitaxel , and adr + cddp + paclitaxel are the most frequently used chemotherapy protocols worldwide [ 3 , 4 , 23 , 27 , 40 , 44 , 51 ]  . 
 hm to the liver in the present group of 32 patients with hm to the liver , 2 patients treated with resection of solitary metastasis , followed by chemotherapy ( adr + cbdca ) , survived 60 months . 
according to tangjitgamol et al . , only two case reports of hepatic resection of hm from ec have been published [ 13 , 50 ] ; the hepatic lesions were 9cm and 7cm and in both cases the patients underwent trisegmentectomy followed by systemic chemotherapy . 
hematogenous metastases in stage i or ii endometrial carcinoma endocrine therapy alone or with bmpr / wbpr offered a 13% rr and chemotherapy alone or with mpa / bmpr offered a 20% rr in our group of patients . 
the data from the literature shows that patient survival after the diagnosis of hm to the brain is poor , with a median survival time of usually less than 2 months ( range , 0.283 months ) [ 2 , 14 , 15 , 22 , 33 , 45 ]  . 
long - term survival is rare but has been documented in some patients with solitary brain lesions who underwent surgical resection and wbrt [ 15 , 32 , 43 , 45 , 50 ]  . 
 data from the literature and our own observations indicate that conventional surgery or stereotactic radiotherapy followed by wbrt is a cornerstone treatment for patients with hm to the brain from ec , especially in patients with solitary lesions , wellcontrolled extracranial disease , and good performance status [ 14 , 50 ]  . 
 [ 48 ] suggested that the stereotactic radiotherapy produces similar local control rates as does conventional surgery and the use of this method could allow wbrt to be omitted without compromising survival duration . 
 the radical treatment of patients with hm from ec according to location of metastasis is as follows : hm to the lung or liver : resection of metastasis combined with chemoand / or hormonotherapy , hm to the bones : bone metastases radiotherapy and chemohm to the brain : resection of metastasis or stereotactic radiosurgery , combined with wbrt . therapy , original article physical and clinical implications of radiotherapy treatment of prostate cancer using a full bladder protocol raffaella cambria1 , barbara a . 
jereczek - fossa2 , 3 , dario zerini2 , federica cattani1 , flavia serafini4 , rosa luraschi1 , guido pedroli1 , roberto orecchia2 , 3 purpose : to assess the dosimetric and clinical implication when applying the full bladder protocol for the treatment of the localized prostate cancer ( pca )  . patients and methods : a total of 26 consecutive patients were selected for the present study . 
the potential advantage for gu toxicity in applying the fb treatment protocol was measured : the ratio between full and empty bladder dosevolume points ( selected from our protocol ) is below 0.61 , excluding the higher dose region where dvhs converge . conclusion : having a fb during radiotherapy does not affect treatment effectiveness , on the contrary it helps achieve a more favorable dvh and lower gu toxicities . key words : prostate cancer bladder radiotherapy gu toxicity organ motion strahlenther onkol 2011 ; 187 : 799805 doi 10.1007 / s00066 - 011 - 2259 - x physikalische und klinische implikationen der behandlung bei gefllter blase in der strahlentherapie des prostatakarzinoms ziel : evaluierung der dosimetrischen und klinischen implikationen bei anwendung des gefllte - blase - ( fb - ) protokolls fr die behandlung des lokalisierten prostatakarzinoms ( pca )  . patienten und methoden : 26 patienten wurden fr die vorliegende studie ausgewhlt . 
die behandlungsplne wurden hinsichtlich dosis und dvh verglichen . ergebnisse : die ctv - verschiebungen waren vernachlssigbar in laterolateraler und superior - inferiorer richtung ( maximale verschiebung : 1 , 85 mm )  . 
der potentielle vorteil hinsichtlich der gu - toxizitt bei anwendung des fb - behandlungsprotokolls war messbar : das verhltnis der dosis - volumen - punkte ( aus unserem protokoll ) bei gefllter bzw . 
leerer blase lag unter 0 , 61 , mit ausnahme der hheren dosisbereiche , wo die dvhs konvergieren . schlussfolgerung : fb whrend der strahlentherapie hat keinen einfluss auf die wirksamkeit der behandlung , bewirkt jedoch gnstigere dvhs und niedrigere gu - toxizitt . schlsselwrter : prostatakarzinom blase strahlentherapie gu - toxizitt organbewegung 1department of medical physics of the istituto europeo di oncologia , milan , italy , 2department of radiation oncology of the istituto europeo di oncologia , milan , italy , 3universit degli studi di milano , milan , italy , 4 unit operativa di radioterapia , azienda ospedaliera santanna , como , italy . received : january 10 , 2011 ; accepted : june 16 , 2011 published online : november 25 , 2011 strahlenther onkol 2011 urban & vogel cambria r , et al . 
with regard to the urinary bladder filling state , it is , in general , suggested to maintain a constant bladder volume [ 4 ] , i.e. , either empty or filled . 
 [ 21 ] reported that patients informed to drink the same amount of liquid before every treatment are more able to maintain a constant bladder volume , although nakamura et al . 
another reason to treat with full bladder is to displace the organs at risk ( oars ) like the sigmoid colon and the small bowel from the target volume [ 21 ]  . 
in order to study the influence of bladder volume modifications on treatment , a study on the ctv - shift triggered by volumetric variations of the urinary bladder was performed . 
the analysis of the impact of bladder filling on the treatment planning was performed on the simulation computer tomography ( ct ) scan and on the ct scan after 40 gy . patients and methods patient selection and preparation a total of 26consecutive patients scheduled for radical radiotherapy for the organ - confined prostate carcinoma were selected for the present study . 
patients clinical data are summarized herein : mean age , 71 years ( range , 4583 years ) ; number of low - risk patients , 5 ; number of intermediate - risk patients , 12 ; number of high - risk patients 8 ; mean gleason score 7 ( 3 8 ) ; initial psa 11 ng / ml ( range , 0.540 ng / ml )  . 
all patients underwent two series of ct scans ( figure 1 ) : the first one was performed the day of the simulation , while the second one after 40 gy . 
each series consisted of two consecutive ct scans : the first acquired with full bladder ( ct1 - fb ) and the second one after emptying it ( ct2 - empty bladder , ct2 - eb )  . 
according to our treatment protocol , to achieve useful bladder filling , patients were asked to empty the bladder 2 h before the ct scans and , strahlenther onkol 2011 no . 
ctvs and oars , contoured on the second ct - eb scan of each series , were imported into the first one . treatment technique and planning the details of the treatment technique were already described previously [ 5 , 13 , 14 ]  . 
dose of 7680 gy in 2 gy per fraction is prescribed to the international commission of radiation units ( icru ) point ( isocenter ) ( icru62 ) [ 11 ]  . bladder volume variability and rectal movements first , bladder and the rectum variability in the ct series was studied . 
to minimize the influence of the rectal changes , the ct - fb and the ct - eb scans were performed consecutively and the two ct series data were analyzed in parallel . 
applying this procedure , in fact , we were sure that the rectal structure did not touch our ctv and that it did not induce shifts on it . ctv shift and dosimetric implications ctv displacements were evaluated by measuring the center of mass ( cm ) shifts ; it was assumed that ctv deformation could be neglected . 
the extent of the dose shift was evaluated by comparing the dose coverage in terms of minimum dose received by the ctv . bladder dosevolume histogram constraints to quantify the advantage of the full bladder treatment , the dosevolume histograms ( dvh ) , resulting from planning on the ct - fb to the one planned on the ct - eb , were compared . 
the dvh points , corresponding to the constraints proposed in the study of radiation therapy oncology group ( rtog ) 0126 [ 27 ] , were also evaluated : d15% < 80gy ; d25% < 75gy ; d35% < 70gy ; d50% < 65gy . 
the dvh comparison between a fb and an eb plan are reported as the ratio between the dose received by a selected percentage of the volume of the fb and the corresponding dose received by the same volume of the eb . statistical analysis the statistical analysis was performed by the medcalc ( b ) software . 
radiotherapy for pca treatment with a full bladder results clinical target and organ at risk volumes the clinical target ( p + sv , p , and sv ) , the urinary bladder , and the rectal volumes of all the 26 patients are shown in table 1 . 
concerning the urinary bladder , table 1 also reports the ratio between the volumes contoured in ct - eb and those contoured in ct - fb : veb / fb = vct - eb / vct - fb . 
figure 3 compares the rectal volume within the same ct series , while figure 4 shows the comparison between the rectal volumes before and after 40 gy : ( a ) the two rectal volumes contoured in the two full bladder ct scans and ( b ) those two contoured in the empty bladder ct scans , respectively . 
of the 26 patients , 18 patients were included in the ctv shift study as they had the prequisite rectal and bladder characteristics . ct1 - fb ct3 - fb ct2 - eb ct4 - eb figures 2a and 2b . 
bladder volume comparison : the graphs show the comparison between : ( a ) full bladder ( fb ) volumes and ( b ) empty bladder ( eb ) volumes before therapy and after 40 gy . 
blasenvolumenvergleich : die grafiken zeigen den vergleich zwischen ( a ) dem gefllte - blase - ( fb - ) volumen und ( b ) dem leerblase - ( eb - ) volumen vor der therapie und nach 40 gy bestrahlung . 
der punkte - plot gibt alle daten wieder und die verbindungslinien zwischen den beiden mittelwerten ; der fehlerbalken zeigt 1 sd ( standardabweichung ) n . ct1 - fb ct2 - eb ct3 - fb ct4 - eb figures 3a and 3b . 
rectal volume comparison : the graphs show the comparison between the contoured rectal volumes within the ct series , ( a ) ct1 - fb ( full bladder ) , ct2 - eb ( empty bladder ) and ( b ) ct3 - fb ( full bladder ) and ct4 - eb ( empty bladder )  . 
rektalvolumenvergleich : die grafiken zeigen den vergleich der konturierten rektalvolumen innerhalb der ct - serie ; ( a ) ct1fb ( gefllte blase ) , ct2 - eb ( leere blase ) und ( b ) ct3 - fb ( gefllte blase ) und ct4 - eb ( leere blase )  . 
rectal volumes comparison : the graphs show the comparison between rectal volumes ( a ) before therapy , ct1 - fb ( full bladder ) and ct3 - fb ( full bladder ) and ( b ) after 40 gy , ct2 - eb ( empty bladder ) and ct4 - eb ( empty bladder )  . 
rektalvolumenvergleich : die grafiken zeigen den vergleich der rektale volumen ( a ) vor der therapie , ct1 - fb ( gefllte blase ) und ct3 - fb ( gefllte blase ) und ( b ) nach 40 gy bestrahlung , ct2 - eb ( leere blase ) und ct4 - eb ( leere blase )  . 
blase : dvh - vergleich des fb - ( gefllte - ) blaseund des eb - ( leer - ) blase - bestrahlungsplans ( median ; 95% - ci )  . 
12 ctv shift and dosimetric implications the displacement of the center of mass of the ctvs in the laterolateral , anteriorposterior , and superiorinferior directions are shown in table 2 . 
the dosimetric evaluation based on the comparison between the minimum dose received by the planned ctv in the ct - fb , and that received by the ctv contoured in the ct - eb ( and imported into the ct - fb ) are reported in table 3 . bladder dosevolume histogram constraints the dvh comparison between the fb and the eb plan is reported in table 4 . discussion the aim of the present analysis was to study both the impact of bladder filling on ctv displacement and consequently on the dose coverage , and the possibility of reducing bladder toxicity in radiotherapy for pca . the first part of the work focused on the volume study . 
 [ 8 ] reported similar results : they observed a slight decrease in the p + sv volume but with no statistical meaning ; the same observation was reported by pinkawa et al . 
a volume reduction after 40 gy ( figure4 ) is also observed for the rectum ; the volume loss could also be explained by treatment tolerance in this case . the second part of this work focused on ctv displacement induced by the extreme bladder volume variability . 
to study the ctv shift , we had to assume that the clinical volumes ( p + sv , p , sv ) were not deformable , which we based on work from deurloo et al . 
returning to organ motion , many papers reported studies about this subject [ 28 , 31 , 38 ] , but only a few of them [ 19 , 24 , 25 ] , however , showed a ctv shift due sole to bladder volume variability . 
we measured the maximum shift of the cm of the ctv ( p + sv ) and ctv ( p ) in the anteriorposterior direction : 2.2mm ( 95% ci ) ( table2 )  . 
 [ 24 ] who demonstrated that the displacements of the prostate and seminal vesicles were not meaningful . the final task of the study was to verify the improvement in dvh , and as a consequence bladder toxicity , risk due to the full bladder treatment protocol ; it was shown that the ratio d50% ( fb ) / d50% ( eb ) is always well below 0.5% ( median ) meaning a lower risk of toxicity . 
comparing the rtog dosevolume limits [ 27 ] , it was noticed that the mean dose objectives ( d35% , d50% ) are better achieved by a full bladder plan , while the volumes exposed to higher doses ( d15% , d25% ) are comparable . 
 this last observation is quite obvious because part of the bladder volume is inside or near the ptv and this is the same for both cases . conclusion this study showed that ctv ( p + sv ) and ctv ( p ) shift due to the extreme bladder volume variability ( from full to empty ) has a low impact on the pca treatment , however , treating with a full bladder protocol could reduce probable bladder toxicity . 
on the other hand , if the variability of the center of mass of the ctv remains well below the limit of the margins employed to generate the ptv , then the minimum dose to the ctv is still above the icru requirements . 
thus , in our experience , it seems safer treating patients with a full bladder even if the filling bladder volume is variable . acknowledgments we would like to thank l . 
santoro for his scientific suggestions . original article impact of vegf gene polymorphisms and haplotypes on radiation - induced late toxicity in prostate cancer patients tanja langsenlehner1 , wilfried renner2 , armin gerger3 , gnter hofmann3 , eva - maria thurner1 , karin s . 
kapp1 , uwe langsenlehner4 background and purpose : vascular endothelial growth factor ( vegf ) is an important determinant of microvascular permeability and angiogenesis and has been shown to be up - regulated during the late phase of radiation injury . 
the present prospective study was performed to evaluate the role of vegf gene polymorphisms and haplotypes in the development of radiation - induced late side effects in prostate cancer patients . 
 patients and methods : the association of vegf gene polymorphisms and haplotypes with high - grade late rectal or urinary toxicity ( defined as late toxicity eortc / rtog 2 ) was analyzed using 493 prostate cancer patients from the austrian procagene study treated with definitive radiotherapy . 
 results : within a median follow - up time of 48 months , 42 patients ( 8.6% ) developed high - grade late rectal and 47 patients ( 9.6% ) urinary toxicity , respectively . 
 conclusion : we conclude that genetic variants in the vegf gene may influence the risk of high - grade late rectal toxicity after definitive radiotherapy for prostate cancer . key words : radiotherapy late toxicity predictive factors vegf polymorphisms haplotypes strahlenther onkol 2011 ; 187 : 78491 doi 10.1007 / s00066 - 011 - 1106 - 4 die bedeutung von vegf - genpolymorphismen und - haplotypen fr die entwicklung von radiogenen sptfolgen bei prostatakarzinompatienten hintergrund : vascular endothelial growth factor ( vegf ) ist ein wichtiger regulator der gefpermeabilitt und angiogenese , und in der chronischen strahlenreaktionsphase wurde die hochregulation von vegf gezeigt . 
 patienten und methoden : der zusammenhang zwischen vegf - genpolymorphismen und - haplotypen und hhergradigen rektalen und urogenitalen sptfolgen ( definiert als spttoxizitt eortc / rtog 2 ) wurde bei 493 prostatakarzinompatienten der procagene - studie , die einer definitiven strahlentherapie unterzogen wurden , untersucht . 
in der kaplan - meier - analyse zeigten trger des vegf - 7c > t - polymorphismus ein erhhtes risiko fr hhergradige rektale sptfolgen ( p = 0 , 003 ; abbildung 2 ) und in der multivariaten analyse , in welche klinische und dosimetrische faktoren eingeschlossen wurden , blieb der vegf - 7c > t - polymorphismus ein signifikanter prediktor ( hr = 28 ; 95% - ci 1 , 3495 , 813 ; p = 0 , 006 , tabelle 4 )  . 
zustzlich zeigte sich fr den attgt - haplotyp , bestehend aus 5 1 department of therapeutic radiology and oncology , medical university of graz , austria , 2 clinical institute of medical and chemical laboratory diagnostics , medical university of graz , austria , 3 division of oncology , department of internal medicine , medical university of graz , austria , 4 division of internal medicine , gkk outpatient department , graz , austria . received : march 12 , 2011 ; accepted : june 28 , 2011 published online : november 17 , 2011 strahlenther onkol 2011 no . 
vegf polymorphisms and radiation - induced late toxicity vor der kodierenden sequenz liegenden polymorphismen , eine signifikante assoziation mit hhergradiger rektaler spttoxizitt ( p = 0 , 001 ; abbildung 3 )  . 
keine signifikanten assoziationen wurden fr die brigen untersuchten polymorphismen und haplotypen gefunden ( tabellen 3 und 4 )  . schlussfolgerung : die vorliegenden daten zeigen , dass varianten im vegf - gen mglicherweise das auftreten von hhergradigen rektalen sptfolgen nach definitiver radiotherapie des prostatakarzinoms beeinflussen . 
 schlsselwrter : radiotherapie spttoxizitt prdiktoren vegf - polymorphismen haplotypen introduction radiotherapy is an effective treatment option for localized or locally advanced prostate cancer and treatment techniques have emerged rapidly during recent years [ 22 , 25 , 48 ]  . 
as a result , patients may experience symptoms associated with damage to normal tissue during the course of therapy for a few weeks after therapy or months or years later [ 21 ]  . the interindividual variability in normal tissue reactions exhibited after radiotherapy is still not fully understood . 
besides radiation dose , age , and comorbidities , a variety of cellular , molecular , and genetic factors have been shown to influence the heterogeneity in normal tissue reactions [ 40 ]  . 
in addition , several observations support the hypothesis that single nucleotide polymorphisms ( snps ) in genes related to the biological response to ionizing radiation may affect clinical radiosensitivity [ 5 , 10 , 11 , 15 , 20 , 47 ]  . 
in prostate cancer patients , single nucleotide polymorphisms ( snps ) in candidate genes involved in dna repair , steroid metabolism , and fibrotic tissue remodeling have been associated with the development of late toxicity after radiation therapy [ 9 , 10 , 14 , 37 ]  . vascular endothelial growth factor ( vegf ) is a pleiotropic growth factor that exerts several effects on the vascular endotheliuvegf is major player in angiogenesis and one of the most potent inducers of vascular permeability [ 17 , 23 ]  . 
in humans , vegf is expressed by different cell types , and in several tissues , vegf up - regulation has been shown during the late phase of radiation injury [ 33 , 36 , 45 , 46 ]  . hypoxia is a major inducer of vegf gene transcription [ 18 ]  . 
transforming growth factor beta ( tgf - ) , a key cytokine in the fibrotic process has been shown to stimulate vegf expression through mothers against decapentaplegic homolog 3 ( smad3 ) signalling [ 28 ]  . 
because vegf induces vegf receptors in fibroblasts and myofibroblasts [ 12 , 50 ] , tgf - - mediated vegf production may trigger an autocrine stimulus and influence the fibrotic response to radiation [ 7 ]  . tgfpolymorphisms have previously been associated with the risk of radiation - induced late toxicity [ 2 , 37 , 38 , 51 ]  . 
 the present prospective study was performed to investigate the association of vegf genotypes and haplotypes with high - grade late rectal or urinary side effects in prostate cancer patients treated with definitive radiotherapy . 
 follow - up follow - up examinations were performed at regular intervals and included psa measurements , digital rectal examinations ( dre ) , completion of a questionnaire on comorbidities , nutritional status , and medication as well as toxicity evaluations . 
 urinary and rectal toxicity was graded according to standard rtog / eortc criteria in all patients by the same senior staff radiation oncologist without knowledge of polymorphism status so as not to bias the evaluation [ 13 ]  . 
 selection of dna polymorphisms , dna isolation , and genotyping assay polymorphisms with a minor allele frequency of at least 0.10 and location in the promoter region , coding region , or untranslated region of the vegf gene were selected . 
using this approach , seven candidate polymorphisms were chosen for further analysis : - 2578c > a ( rs699947 ) , - 2489c > t ( rs1005230 ) , - 1498c > t ( rs833061 ) , - 634g > c ( rs2010963 ) , - 7c > t ( rs25648 ) , 936c > t ( rs3025039 ) , and 1612g > a ( rs10434 )  . upon study entry , each procagene participant had donated a tube of edta - blood , which was stored at 20c . 
general taqman reaction conditions were as described previously [ 30 ]  . construction of haplotypes and statistical analysis haplotypes and linkage disequilibrium were determined using the haploview program ( version 3.32 , edu / personal / jcbarret / haploview / )  . 
cox proportional hazards analysis was performed to calculate the hazard ratio ( hr ) and 95% confidence interval ( ci ) to evaluate the influence of genotypes on the risk of high - grade late side effects ; in addition , multivariate cox regression analysis was performed to adjust for other covariates . 
in a multivariate cox regression model including age at initiation of radiotherapy , oral anticoagulation , hormonal therapy , diabetes mellitus , smoking status , and dosimetric parameters as potential confounders , the vegf - 7c > t polymorphism and the remained significant factors prevegf attgt haplotype remained significant factors predicting for lower risk of high - grade late toxicity ( hr = 2.800 , 95% ci 1.3495.813 ; p = 0.006 and hr = 3.157 , 95% ci 1.4956.666 ; p = 0.003 , table 4 )  . 
in addition , a marginally significant association between the vegf - 2489c > t polymorphism and late rectal toxicity grade 2 was observed in multivariate analysis ( hr = 2.061 , 95% ci 1.0124.197 ; p = 0.046 ) , whereas the remaining vegf polymorphisms and haplotypes were not significantly associated with the development of late toxicity grade 2 ( tables 3 and 4 )  . 
from the initial group of 493 patients eligible for the present study , 3 ( 0.6% ) had a follow - up time < 4 months and were excluded from analysis . 
during follow - up , late rectal and bladder toxicity grade 2 according to the rtog criteria was detected in 42 ( 8.6% ) and 47 ( 9.6% ) patients , respectively . 
 genotypes did not deviate from hardyweinberg equilibriu in kaplanmeier analysis evaluated by logrank test , carriers of the vegf - 7c > t polymorphism were at increased risk of late rectal side effects grade 2 ( p = 0.003 ; figure 2 )  . 
furthermore , the attgt haplotype formed by five polymorphisms upstream the coding region , including the - 7c > t variant was significantly associated with discussion in this study , we investigated whether common snps in the vegf gene were associated with the occurrence of high - grade late rectal or urinary side effects in prostate cancer patients after definitive radiotherapy . 
furthermore , a significant association of the attgt haplotype formed by polymorphisms in the promoter and 5 utr region , including the - 7c > t variant with risk of late rectal toxicity was observed . 
vegf polymorphisms and radiation - induced late toxicity 2 copies 1 copy 0 copies 108 120 follow - up ( months ) 96 108 120 follow - up ( months ) figure 2 . 
 during the late phase of radiationinjury , vegf up - regulation has been detected in the rectum and several other tissues , and with the formation of fibrosis , a further increase in vegf expression has been found [ 32 , 33 ]  . 
 up - regulation of vegf during the late phase of injury produces a further increase in vascular permeability and has been associated with interstitial hypertension and poor blood flow [ 36 ]  . 
applying statistical corrections for multiple testing ( e.g. , bonferroni correction ) can be used to reduce this type 1 error risk , but at the same time increases type 2 error risk ( false negative )  . 
 the major strength of our investigation is the relatively large number of patients that have been enrolled ; furthermore , patients were from an ethnic homogenous population , and both patient recruitment and clinical outcome data collection were carried out independently without knowledge of polymorphism status . 
very recently , genome - wide association studies have been used to identify candidate genes and chromosomal sites linked to erectile dysfunction after radiotherapy for prostate cancer [ 27 ]  . 
using this approach , it is likely that substantial genetic determinants of high - grade radiation - induced toxicities might also be found in other genes , such as those for vegf receptor 1 , vegf receptor 2 , or hypoxia inducible factor . 
the increasing knowledge about genetic factors influencing individual radiosensitivity will help to establish tailored radiotherapy , allowing treatment modification in radiosensitive individuals in order to minimize severe side effects and increase quality of life . 
 acknowledgments this study was supported by the anniversary fund of the sterreichische nationalbank ; grant number : 11686 . nonhealing tissue response causing a secondary cycle of damage [ 4 , 36 ]  . 
recently , bevacizumab , an anti - vegf antibody was found to be effective in treatment of radiation - induced cerebral necrosis leading to radiographic response and to an improvement of cerebral edema with reduction of steroid medication . 
in experimental models , blockage of the vegf - related pathway was also shown to reduce radiation - induced fibrosis in rectal tissues [ 31 , 33 , 34 , 44 ]  . the hypothesis that polymorphisms of the vegf gene might modulate the risk of radiation - induced late toxicity has been built upon the notion that vegf gene polymorphisms influence vegf gene expression . 
the - 7c > t polymorphism lies within the 5 utr and has been found to associate with increased vegf mrna levels in colorectal adenocarcinoma tissues [ 49 ]  . 
the attgt haplotype is formed by the - 7c > t and additional polymorphisms in the promoter and 5 utr that contain key regulatory elements that are sensitive to hypoxia , and contribute to the high variability in vegf production among tissues [ 35 , 42 ]  . 
vegf polymorphisms and radiation - induced late toxicity case study simultaneous chemoradiation with cisplatin in a patient with recurrent cervical cancer undergoing hemodialysis analysis of cisplatin concentrations in serum and dialysate and therapy - related acute toxicity simone marnitz1 , ralph kettritz4 , andreas kahl4 , silvia lehenbauer - dehm3 , leonie frster1 , volker budach1 , christhardt khler2 purpose : to prove the feasibility and toxicity of platinum - based chemoradiation in a patient with recurrent cervical cancer undergoing concomitant hemodialysis . patient and methods : we report a patient with a renal transplant because of chronic renal failure who then underwent radical hysterectomy and lymphadenectomy due to cervical cancer figo stage ib1 . 
one year after primary therapy , a 53 54 68mm vaginal stump recurrence was treated by total translevatoric exenteration with lymphadenectomy , explantation of the transplant , and the right residual kidney . 
within 30 min after cisplatin application , the cisplatin serum concentration reached the highest level with 1 , 179.6g / l and showed nearly stable concentrations over 120 mthere was an accumulation of cisplatin from week1 ( 100% ) to week5 of application ( 219% )  . 
 conclusion : cisplatin application with a modified dose ( 20mg / m2 ) is feasible and safe in a patient with cervical carcinoma undergoing chemoradiation and hemodialysis . key words : cisplatin hemodialysis chemoradiation cervical cancer strahlenther onkol 2011 ; 187 : 8314 doi 10.1007 / s00066 - 011 - 2281 - z simultane radiochemotherapie mit cisplatin unter hmodialyse bei einer patientin mit rezidiviertem zervixkarzinoanalyse der cisplatin - konzentrationen aus serum und dialysat und der akuttoxizitt der behandlung zielsetzung : berprfung der durchfhrbarkeit und toxizitt einer cisplatinhaltigen kombinierten radiochemotherapie bei einer patientin mit rezidiviertem zervixkarzinom unter hmodialyse . patient und methoden : wir berichten ber eine nierentransplantierte patientin , die ein jahr zuvor wegen eines figo - ib1zervixkarzinoms mittels radikaler hysterektomie und lymphadenektomie behandelt worden war . 
sie prsentierte sich mit einem 53 54 68 mm groen vaginalstumpfrezidiv , welches mittels translevatorischer exenteration mit pelviner lymphadenektomie sowie explantation der transplantatniere und der funktionslosen rechten niere therapiert wurde . 
berlin , germany , 3 department of hematologyoncology , charit university medicine , berlin , germany , 4 department of nephrology , charit university medicine , berlin , germany . received : march 3 , 2011 ; accepted : september 14 , 2011 published online : november 25 , 2011 strahlenther onkol 2011 no . 
cisplatin concentrations and acute toxicity during simultaneous chemoradiation and cisplatin ergebnisse : die patientin erhielt eine radiochemotherapie mit einer reduzierten cisplatindosis von 20 mg / m2 einmal pro woche , ohne dass eine hhergradige toxizitt beobachtet wurde . 
 schlsselwrter : cisplatin hmodialyse radiochemotherapie zervixkarzinom introduction cisplatin - based chemoradiation is the standard of care in the treatment of locally advanced primary and recurrent cervical cancer [ 2 , 7 , 11 , 13 , 14 , 18 , 21 ]  . 
there is little data available with regard to platinbased chemotherapy in oncologic patients undergoing hemodialysis [ 4 , 6 , 15 , 16 , 19 ] and having renal failure . 
in 2009 , she underwent a laparoscopically assisted radical vaginal hysterectomy with para - aortic and right - sided pelvic lymphadenectomy ( because of the leftsided transplant ) as described previously [ 10 ] , because of a poorly differentiated squamous cell carcinoma of the cervix uteri ( 35mm )  . 
due to the high - risk parameters ( tumor size , grading , lvsi , and unknown status of the left - sided pelvic lymph nodes ) , the interdisciplinary tumor board recommended adjuvant chemoradiation . 
one year later , a central recurrence ( 53 54 68mm ) was diagnosed with infiltration of the bladder , vagina , and the rectuthere was no chance for local treatment without impairing residual transplant function . 
titanium clips were placed in the high - risk region . chemoradiation radiation treatment consisted of five weekly fractions at 1.8gy for a total dose of 50.4 gy ( a total of 28 fractions ) were given to the pelvic lymph nodes and former tumor region with a 7 - field imrt plan generated in order to decrease the dose to the small bowel [ 5 ]  . 
a boost was given to the clipmarked region + 3 mm margins with five weekly fractions of 1.8gy to a total of 16.2gy with a stereotactic technique [ 21 ]  . 
 discussion most of the available publications regarding cisplatin - based chemotherapy during hemodialysis were case reports [ 4 , 6 , 8 , 9 , 16 , 17 , 19 , 24 ] on patients with ovarian cancer [ 20 , 23 ] , testicular cancer [ 16 ] , extragonadal seminoma [ 4 ] , ureteral carcinoma [ 12 , 19 ] , medulloblastoma [ 6 ] , uterine cancer [ 8 , 24 ] , and other tumors [ 17 , 22 ]  . 
the present report on a patient with a kidney transplant is the first report on repeated measurements of cisplatin concentration in serum and dialysate in a patient with cervical cancer undergoing chemoradiation and hemodialysis . 
in the literature , there is data supporting dose reduction [ 17 , 20 , 24 ] , maintaining the normal doses [ 12 , 23 ] , and dose escalation [ 4 , 16 , 22 ]  . 
 [ 19 ] showed that the free cisplatin levels rebounded remarkably after dialysis , which might be underlined by our findings of higher cisplatin serum concentrations before starting a new application compared with the last cisplatin level after hemodialysis . 
this raises the question of the optimal timing between chemotherapy , radiotherapy , and hemodialysis , on the one hand , and a possible redistribution from the tissue , on the other [ 8 ]  . 
 the majority of authors did not evaluate acute toxicity [ 4 , 6 , 19 ] , while others estimated toxicity as manageable and tolerable [ 16 ] , acceptable [ 23 ] , or even minimal [ 9 ]  . 
dialysatkonzentration ( g / l ) von platin und cisplatin vor ( 0 min ) , 30 , 60 , 120 minuten nach der ersten cisplatingabe . week 1 week 2 week 3 week 4 week 5 figure 2 . 
akkumulation von cisplatin ( 120 min nach gabe ) im serum der patientin von woche 1 ( 100% ) bis woche 5 ( 219% )  . doubling of the measured cisplatin serum concentration comparing the first and the last week of application as described by other authors [ 6 , 17 ]  . 
cisplatin concentrations and acute toxicity during simultaneous chemoradiation and cisplatin original article vmat and step - and - shoot imrt in head and neck cancer a comparative plan analysis rolf wiehle1 , stefan knippen1 , anca - ligia grosu1 , gregor bruggmoser1 , norbert hodapp1 purpose : rotational imrt is a new technique , whose value still has to be assessed . 
we evaluated its adequacy for the treatment of head and neck ( h&n ) cancer compared to the well - established step - and - shoot imrt . materials and methods : a total of 15 patients , who were treated with either imrt ( 13 patients ) or vmat ( 2 patients ) in the h&n region , were chosen . 
a conformity function ( cf ) was defined to estimate normal tissue sparing . results : the qi for vmat amounts to 36.3 , whereas for imrt the mean value is 66.5 , indicating better ptv coverage as well as less overdosage for the rotational technique . 
while the sparing of organs at risk ( oar ) was similar for both techniques , the cf shows a significantly better sparing of healthy tissue for all doses with vmat treatment . conclusions : vmat results in dose distributions for h&n patients that are at least comparable with treatments performed with step - and - shoot imrt . 
wir untersuchten deren eignung fr die behandlung von kopf - hals - ( h&n - ) tumoren im vergleich zu etablierter step&shoot - imrt . material und methoden : es wurden 15 patienten ausgewhlt , die mit imrt ( 13 patienten ) oder vmat ( 2 patienten ) in der h&nregion behandelt wurden . 
eine konformittsfunktion ( cf ) wurde definiert , um die nomalgewebeschonung abzuschtzen . ergebnisse : der qi fr vmat betrgt 36 , 3 , whrend sich der mittelwert fr imrt auf 66 , 5 beluft , was eine bessere dosisabdeckung und - homogenitt bei der rotationsbestrahlung anzeigt . 
vmat vs ssimrt in h&n cancer introduction for radiotherapy treatment planning of carcinoma in the head and neck ( h&n ) region , several organs at risk ( oar ) , e.g. , the spinal cord and the parotid glands , have to be considered . 
by limiting the mean dose to the salivary glands to around 2530gy , it is possible to preserve much of their functionality [ 6 , 14 , 21 , 29 ] ; small displacements , however , may degrade this beneficial effect [ 5 , 9 , 10 ]  . 
 yu proposed a new approach of imrt called intensity ( or volumetric ) modulated arc therapy ( imat , vmat ) : rather than using a discrete number of beam directions , the gantry rotates around the patient , while the multileaf collimator ( mlc ) is continuously adjusted [ 31 , 32 ]  . 
since step - and - shoot imrt treatments in the h&n region take about 10min , this means that imat may reduce the treatment time by a factor of three [ 3 ]  . 
the usefulness of rotational imrt techniques in the treatment of multiple cerebral metastases [ 4 , 11 , 30 ] and h&n cancers [ 2 , 12 , 27 , 28 ] has been shown recently by various groups . 
comparison with imrt showed imat to yield better results in terms of sparing of oar and ptv coverage , if two arcs were used [ 27 , 28 ] , while bertelson et al . 
although the improvement in terms of dose distribution is reported to be small , the advantage of faster treatment and smaller number of monitor units ( mu ) , on the other hand , is generally considered important . the evaluation of dose distribution is an important , but difficult issue . 
because the very large amount of information they contain is hard to assess , the dose distribution is generally condensed into dvhs or even single number objects , e.g. , a conformity or homogeneity index . 
some of these parameters are easy to calculate and interpret , but lack significance under certain circumstances [ 15 , 20 , 22 ] , while others are of general usefulness , but difficult to access [ 16 , 18 , 19 ]  . 
obviously none of these parameters can replace the analysis of the 3d dose distribution by a skilled radiotherapist . we present a dosimetric comparison of two treatment techniques , calculated using two different treatment planning systems ( tps ) for two different linacs : step - and - shoot imrt with oncentra masterplan for an elekta synergy linac versus vmat planned with varian eclipse for a varian clinac2100 . 
 two new parameters , the quality index ( qi ) and the conformity function ( cf ) , are introduced and used to compare the resulting dose distributions . patients and methods patients a total of 15 patients with carcinoma of the h&n were selected for this study . 
both final dose calculation and optimization were performed using the pencil beam dose calculation algorithm [ 1 , 13 ]  . vmat planning the vmat treatments were planned with varian eclipse ( v8.6.15 ) for a varian clinac2100 linac with 6mv photons , using two arcs of 358.8. 
the aims were the same as for the imrt , but to achieve them the dvos as well as their relative weights had to be set to different values compared to imrt planning . 
if the situation occurred that the dvh was much better for one structure , but much worse for another , it was attempted to minimize one of the differences by adjusting the dvos . 
the dose calculation was performed using the analytical anisotropic algorithm ( aaa ) [ 17 , 2326 ]  . quality index ( qi ) assessing the quality of a dose distribution has not been made easier with the introduction of imrt into clinical practice . 
a dose distribution with a minimum dose of at least 95% and a maximum dose of at the most 107% for the ptv , yields an qi of zero . conformity function ( cf ) [ % ] vol ptv the conformity of dose distributions is sometimes measured in terms of a conformity index ( ci ) , which is defined as volume of the 95% isodose over volume of the ptv : ci = ci =  . 
a natural extension of this concept is to use the volume outside the ptv , which receives at least 95% of the prescribed dose and normalize it to the ptv volume : ci = %ci =  . 
because one is also interested in how well the normal tissue is spared from receiving lower doses , we further extended the idea and made the dose a variable , thereby introducing the cf : vol ptv outside ptv [ % ] relative dose ( % ) figure 1 . 
because calculating dvhs from a dose distribution and a structure set , both of which are discrete objects , is not unambiguous , we decided to have all dvhs calculated by the same tps . 
treatment plan and dose matrix were exported by masterplan und imported into eclipse in the dicom format ( ct and structure set had been imported already for treatment planning )  . 
to quantify the sparing of the spinal cord , the dose that is exceeded in 2% of its volume ( d2% ) was chosen , in order to suppress the influence of tiny hot spots . 
deciding which technique is better in terms of ptv coverage can be assisted by consulting the qi , whose mean value is 36.3 for imat and 66.5 for imrt ( see table 2 )  . 
d2% for all patients is shown in figure 3 ; for vmat the mean value amounts to d2% = 36.7 gy compared to d2% = 37.4gy for imrt ( see table 2 )  . 
the mean dose to the salivary glands as well as the v20gy for all patients are shown in figures 4 and 5 ; average patient data are given in table 2 . 
vmat vs ssimrt in h&n cancer imrt : external spinal cord parotid_1 parotid_r vmat : external spinal cord parotid_1 parotid_r discussion the use of rotational imrt allowed us to produce dose distributions whose qi was on average 45% lower than with conventional static imrt . 
to judge the meaning of its absolute value an example has to be considered : a qi of 50 would be calculated , if 10% of the ptv receives a dose of 90% , while the remaining 90% of the ptv is covered with doses between 95% and 107% . 
 in addition , one should bear in mind that , since the qi is calculated from the dvh , it cannot give any information about the position of hot and cold areas . 
 considering this , we believe the qi to be a very sensitive tool that was much more helpful in deciding which treatment yielded better results in terms of target coverage than the use of dvhs only . 
except for d2% [ spinal cord ] , all quantities are lower with statistical significance for vmat ( see table 2 )  . sparing of the spinal cord was of paramount importance and , therefore , had the highest weight of all dvos during optimization . 
the functionality of the salivary glands should largely be preserved for the patients considered here , according to the results presented in [ 6 , 14 , 29 ] , even though a boost of another 1020gy was added , which is not part of this analysis . 
while for small doses the irradiated normal tissue is between 10% and 50% larger for static treatments , the difference increases to between 100% and 230% in the dose range of 80100% . 
that rotational therapy is capable of reducing the volume of normal tissue subjected to high dose was plausible , but we were surprised to find that at low doses the sparing was also better . 
but since vmat allowed a reduction of the 95% isodose volume by about 13% , the integral dose which had to be applied in order to cover the ptv , was significantly reduced , which in turn also allowed a reduction of the volume subjected to low doses . conclusion we were able to show that vmat allows h&n patients to be treated at least equally well as with imrt in terms of ptv coverage and oar sparing and that the normal tissue receives much lower doses . 
the qi proved to be very sensitive in identifying the better plan in terms of ptv coverage , and cf allows normal tissue sparing to be brought into the focus of the therapist . fallstudie komplette remission multifokaler zerebraler metastasen bei chemotherapierefraktrem nsclc durch monotherapie mit gefitinib frauke mller1 , hendrik riesenberg1 , peter hirnle2 , hans - bjrn gehl3 , paul dwel4 , martin grner1 hintergrund : die wirksamkeit einer erstlinientherapie mit tyrosinkinaseinhibitoren auf den primrtumor bei patienten mit nicht kleinzelligem bronchialkarzinom im stadium iv und nachweis einer egf - rezeptor - mutation ist belegt . 
demgegenber existieren nur wenige daten zur wirksamkeit bei zerebraler metastasierung . fallbericht und ergebnisse : bei einer 43 - jhrigen patientin war die diagnose eines hepatisch und zerebral metastasierten nichtkleinzelligen bronchialkarzinoms gestellt worden . 
nach initialer notfallbestrahlung aufgrund einer oberen einflussstauung und einmaliger gabe von carboplatin erhielt die patientin bei positivem nachweis des mutierten egf - rezeptorgens parallel zur bestrahlung des primrtumors und der zervikalen lymphknotenmetastasen gefitinib in einer dosierung von 250 mg / tag . 
darber hinaus knnen unter alleiniger therapie mit dem tyrosinkinaseinhibitor vollremissionen zerebraler metastasen erreicht werden . schlsselwrter : nichtkleinzelliges bronchialkarzinom tyrosinkinaseinhibitoren zerebrale metastasen strahlenther onkol 2011 ; 187 : 82630 doi 10.1007 / s00066 - 011 - 2260 - 4 complete remission of multiple brain metastases of non - small cell lung cancer induced by gefitinib monotherapy background : while the activity of tyrosine kinase inhibitors as the first line treatment for primary tumors in patients with stageiv non - small cell lung cancer and a positive egf receptor mutation is well known , little data on the efficacy in controlling cerebral metastases are available . case report and results : a 43 - year - old woman was diagnosed with non - small cell lung cancer with cerebral and hepatic metastases . 
however , after she failed to respond to this therapy and in light of a positive egf receptor mutation , gefitinib was added at a dose of 250 mg / day while continuing radiation to the primary lesion and cervical lymph nodes . 
furthermore , complete remission of cerebral metastases can be achieved with tyrosine kinase inhibitor monotherapy . key words : non - small cell lung cancer tyrosine kinase inhibitors brain metastases 1klinik fr hmatologie , onkologie & palliativmedizin am klinikum bielefeld 2klinik fr strahlentherapie am klinikum bielefeld 3klinik fr radiologie am klinikum bielefeld 4onkologische schwerpunktpraxis bielefeld eingegangen : 24 . 
neben anzahl und lokalisation der zerebralen metastasen sind vor allem der allgemeinzustand des patienten sowie der remissionsstatus des primrtumors prognosebestimmend und fr das weitere therapeutische vorgehen entscheidend [ 14 , 16 , 19 , 26 ]  . 
sie fhrt bei 5070% der patienten zu einem objektivierbaren ansprechen und kann die mediane berlebenszeit von patienten mit symptomatischen zerebralen metastasen von 12 monaten im vergleich zur alleinigen steroidtherapie auf 46 monate verlngern [ 1 , 25 ]  . 
insbesondere bei palliativer ganzhirnbestrahlung ist eine verschlechterung der neurokognitiven fhigkeiten eher auf eine tumorprogression als auf eine folge der strahlentherapie zurckzufhren [ 11 , 24 ]  . ein wesentlicher nachteil der alleinigen ganzhirnbestrahlung besteht jedoch in der fehlenden wirkung auf extrakranielle tumormanifestationen , die aber fr ca . 
50% der patienten mit zerebralen metastasen die gesamtprognose bestimmt [ 10 ]  . whrend die datenlage zur liquorgngigkeit der herkmmlichen systemischen chemotherapie kontrovers beurteilt wird , haben prklinische untersuchungen fr den krzlich fr die therapie bestimmter nichtkleinzelliger bronchialkarzinome zugelassenen tyrosinkinaseinhibitor gefitinib eine sehr gute liquorgngigkeit ergeben [ 6 , 13 ]  . 
auch fr andere zielgerichtete therapeutika , beispielsweise cetuximab , gibt es studien hinsichtlich der berwindung der bluthirnschranke [ 20 ]  . whrend es in der literatur einige hinweise auf die invivo - wirksamkeit von gefitinib bei zerebraler metastasierung in simultaner oder sequentieller kombination mit ganzhirnbestrahlung gibt , beschreiben wir hier erstmals einen fall einer lang anhaltenden kompletten remission zerebraler metastasen bei einer patientin durch eine monotherapie mit gefitinib . in den letzten 4 wochen vor der stationren aufnahme starker nachtschwei . 
vor 10 jahren hatte die patientin ihren nikotinkonsum beendet . bei der aufnahme war der allgemeinzustand der normgewichtigen ( gre 172 cm , gewicht 68 kg ) patientin reduziert ( karnofsky - index 80% )  . 
multiple lebermetastasen mit einem maximalen durchmesser von 1 , 8 cm im segment v . szintigraphisch fand sich kein hinweis auf ossre metastasen . in der magnetresonanztomographie ( mrt ) des gehirns ( abbildung 1 ) stellten sich multiple disseminierte hirnfiliae bis zu 7 mm gro dar , die grte hiervon links hochparietal mit einem geringen perifokalen dem . histologie durch lymphknotenbiopsie rechts zervikal schlecht differenziertes adenokarzinom mit solidem wachstumsmuster ( g3 ) ; ttf1 - expression , ck 5 / 6 negativ , ck 7 durchgngig krftig positiv ; mutation des egf - rezeptorgens ( exon 19 , deletion e746t751 )  . diagnose zerebral und hepatisch metastasiertes adenokarzinom der lunge mit oberer einflussstauung bei einer jungen frau , die seit vielen jahren nichtraucherin ist . therapie / verlauf fallbeschreibung eine 43 - jhrige deutsche , dauerhaft auf barbados lebende patientin wurde mit einer seit 1 woche rasch zunehmenden rechtszervikalen schwellung und progredienten dyspnoe aufgenommen . 
 aufgrund des klinischen bildes einer oberen einflussstauung mit schwerer ateminsuffizienz wurde unmittelbar nach der gewebeentnahme eine notfallbestrahlung der zervikalen lymphknoten , des berganges zur rechten supraklavikularregion , des tumors im rechten oberlappen und des mediastinums bis 8 gy je 4 gy an zwei aufeinanderfolgenden ta gen , begleitet von einer symptomorientierten hoch dosierten steroidtherapie , eingeleitet , anschlieend fortsetzung der bestrahlenther onkol 2011 no . 
auf eine bestrahlung der hirnfiliae wurde aufgrund der fehlenden neurologischen symptomatik zu diesem zeitpunkt verzichtet . nach nachweis der spezifischen mutation im egf - rezeptorgen beginn einer therapie mit gefitinib ( 250 mg / tag ) parallel zur bestrahlung ab dem 13 . 
hierunter rasche , zunchst kontinuierliche klinische besserung ; laborchemisch rcklufige , zuletzt normalisierte ldh und in der computertomographie des thorax teilremission mit regress der tumormassen um > 25% 7 tage nach aufnahme der simultanen therapie . 
unter antikoagulatorischer und antibiotischer therapie setzte sich die rasche besserung der symptomatik weiter fort . zur planung der zerebralen bestrahlung und kontrolle des primrtumors nach abschluss der strahlentherapie fhrten wir am ende der stationren behandlung eine computertomographie von hals - / thorax - / oberbauch sowie eine mrt des schdels durch . 
in der zerebralen bildgebung war die vorbeschriebene disseminierte metastasierung bildgebend nicht mehr darstellbar , so dass auf die geplante zerebrale bestrahlung bei fortgesetzter gefitinib - therapie verzichtet wurde ( abbildung 2 )  . 
 bei weiteren kontrollen nach 10 und 20 wochen bestand weiterhin kein hinweis auf ein rezidiv der zerebralen metastasierung , allerdings zeigte die ct - untersuchung von thorax und abdomen einen progress des primrtumors und der lebermetastasen . 
lediglich bei der einleitung der therapie beschrieb die patientin leichtgradige abdominelle schmerzen , die nach wenigen tagen spontan abklangen . diskussion die wirksamkeit einer spezifischen therapie mit gefitinib bei patienten mit nichtkleinzelligem bronchialkarzinom im stadium iv und nachgewiesener aktivierender mutation des egfrezeptors ist durch randomisierte phase - iii - studien belegt [ 15 , 21 ]  . 
im vergleich zu einer chemotherapie mit carboplatin auc6 und paclitaxel 200 mg / m tag 1 alle 3 wochen erreicht diese population unter einer gefitinib - monotherapie eine hhere remissionsrate ( 71% versus 47% ) und eine verlngerung des progressionsfreien berlebens ( 9 monate versus 6 monate )  . 
dies vor allem dann , wenn eine erhhte durchlssigkeit der bluthirnschranke zu erwarten ist , beispielsweise bei bereits bestehender hirnmetastasierung oder nach erfolgter therapeutischer radiatio [ 6 , 13 ]  . 
 von den 17 patienten ( 81% ) , die auf die kombination ansprachen , zeigten 62% ( 13 patienten ) eine partielle remission und bei 19% der flle konnte sogar eine komplette remission wie bei der von uns beschriebenen patientin erreicht werden [ 12 ]  . 
 einschrnkend muss aber erwhnt werden , dass bei asiaten aufgrund der erhhten prvalenz aktivierender mutationen im egf - rezeptorgen eine erhhte suszeptibilitt gegenber bestimmten tyrosinkinaseinhibitoren besteht und die in der regel guten klinischen daten deshalb nicht ohne weiteres auf andere populationen bertragen werden knnen [ 2 ]  . die bisher grte prospektive europische studie mit gefitinib umfasst 41 patienten mit zerebral metastasiertem nichtkleinzelligem bronchialkarzinom , wobei 18% dieser patienten zuvor bereits eine ganzhirnbestrahlung erhalten hatten [ 4 ]  . 
 hier wurden partielle remissionen bei 10% und eine krankheitsstabilisierung bei weiteren 17% dokumentiert , wobei komplette remissionen nicht gesehen wurden . im gegensatz hierzu wurde bei der von uns beschriebenen patientin eine mehrere monate anhaltende remission einer multifokalen zerebralen metastasierung durch eine gefitinib - monotherapie ohne parallele oder sequentielle bestrahlung erreicht . 
die remission hielt auch an , als ein progress der extrakraniellen tumormanifestationen zu beobachten war . zum einen htte die gefitinib - therapie im fall eines zerebralen rezidivs eine erneute behandlungsoption durch eine ganzhirnbestrahlung erffnet , und zum anderen konnte durch dieses vorgehen die potentielle toxizitt einer ganzhirnbestrahlung fr die patientin zumindest zunchst vermieden werden . 
 insbesondere zeigte sich auch keine verstrkte lungen - , haut und knochenmarktoxizitt der thorakalen bestrahlung durch die simultane gabe von gefitinib . die vorliegenden daten lassen noch keinen schluss ber die sinnvollste behandlungssequenz zu : monotherapie oder simultane bzw . 
brain tumors in mice are susceptible to blockade of epidermal growth factor receptor ( egfr ) with the oral , specific egfr - tyrosine kinase inhibitor zd 1839 ( iressa )  . 
there was no significant survival difference between the different radiotherapy protocols . conclusion : concomitant carboplatin and paclitaxel is feasible and effective in advanced carcinomas of the head and neck . key words : head and neck cancer radiotherapy chemotherapy taxanes strahlenther onkol 2011 ; 187 : 64550 doi 10.1007 / s00066 - 011 - 1111 - 7 definitive radiochemotherapie fortgeschrittener kopf - hals - tumoren mit carboplatin und paclitaxel ziel der arbeit war die untersuchung der effektivitt und toxizitt einer simultanen radiochemotherapie mit carboplatin und paclitaxel bei fortgeschrittenen inoperablen oropharynxund hypopharynxkarzinomen . 
 patienten und methoden : fortgeschrittene und inoperable karzinome von oropharynx und hypopharynx wurden entweder mit einer simultanen hyperfraktioniert - akzelerierten ( 50 , 0gy / 2 , 0 mit concomitant boost bis 69 , 2gy / 1 , 6 ) oder einer konventionell fraktionierten radiochemotherapie ( 70 , 272gy / 1 , 8 ) zusammen mit paclitaxel ( 40mg / m2 ) und carboplatin ( auc1 ) fr insgesamt 6wochen behandelt . 
eine akute mukositis grad 3 oder hher trat bei 51 , 2% der patienten auf ; die rate an grad - 3 - leukopenien und - thrombopenien lag bei 6% . 
 schlussfolgerung : die kombinierte radiochemotherapie mit carboplatin und paclitaxel bei fortgeschrittenen kopf - hals - tumoren ist sicher durchfhrbar und effektiv . schlsselwrter : kopf - hals - tumoren strahlentherapie chemotherapie taxane 1department of radiation oncology , university of cologne , cologne , germany , 2department of otorhinolaryngology , head and neck surgery , university of cologne , cologne , germany , 3department of otorhinolaryngology and head and neck surgery , university of giessen , giessen , germany , 4department of otorhinolaryngology and head and neck surgery , friedrich - schiller university of jena , jena , germany . received : march 21 , 2011 : accepted : july 11 , 2011 published online : september 23 , 2011 strahlenther onkol 2011 no . 
definitive rt of advanced h&n cancer with carboplatin and paclitaxel introduction radiotherapy concurrent radiochemotherapy is the standard treatment for advanced inoperable squamous cell carcinomas of the head and neck ( scchn )  . 
the important role of platinum has been confirmed in a large meta - analysis of > 17 , 000 patients ( mach - nc ) , where platinum - based concomitant therapy showed the most potent benefit on survival compared to other single - agent protocols ( hr 0.74 , p = 0.006 ) [ 17 ]  . 
poly - agent radiochemotherapy protocols often include 5 - fluorouracil ( 5 - fu ) and platinum [ 10 ] ; however , the efficacy of additional 5 - fu is questionable and especially mucosa toxicity remains substantial [ 26 ]  . 
the number of larger phase iii trials using a new generation chemotherapy agent , such as paclitaxel , for concurrent radiotherapy in scchn is limited , and currently the focus is on combinations of targeted drugs and radiotherapy [ 3 , 29 ]  . paclitaxel representative of the second generation chemotherapy has been used in scchn single - agent [ 7 , 14 ] or platinum - based radiochemotherapy protocols [ 2 , 6 , 8 , 15 , 22 , 25 ]  . 
experience with concurrent paclitaxel and hyperfractionated - accelerated radiotherapy is limited , and the aim of this study was to demonstrate the efficacy and toxicity of concomitant radiochemotherapy with ccb , carboplatin , and paclitaxel in advanced scchn . 
 concurrent radiochemotherapy was used : the therapy of all newly diagnosed tumor patients presenting with advanced histologically proven carcinomas of the head and neck were discussed by an interdisciplinary tumor board , consisting of experienced head and neck surgeons and radiation oncologists . 
staging investigastaging investigations included mri or ct scan of the neck , thoracic ct scan , full blood cell count , serum chemistry profile , ecg , complete history and physical examination and assessment of karnofsky performance status . 
in addition , macroscopically involved primary tumor and lymph nodes ( ptv1 ) were treated with a second daily fraction of 1.6gy ( ccb ) from days 1325 to a total dose of 19.2gy. for conventional fractionation ( cf ) , ptv2 received 1.8gy once daily to a total dose of 50.4gy. 
 ptv2 additionally included potentially microscopically involved lymph node areas depending on primary tumor location [ 12 ]  . three - dimensional conformal radiotherapy was used ; a typical plan for ptv2 included 69 fields and 36 fields for ptv1 . 
radiotherapy was given within 1h after chemotherapy . chemotherapy concurrent chemotherapy was administered once weekly during radiotherapy with antiemetic coverage and consisted of carboplatin auc1 and paclitaxel 40 mg / m2 . 
additional antiemetics ( 5ht3 antagonists , corticosteroids , and metoclopramide ) were used on patients request . toxicity assessment and follow - up acute treatment toxicity was evaluated daily during chemotherapy , weekly during radiotherapy , and documented using who criteria . 
progression - free survival ( pfs ) was calculated from day1 of treatment to either death or diagnosis of recurrent disease ( local or distant metastases ) or last follow - up alive . 
 results patient characteristics a total of 84patients ( 69 men ( 82.1% ) and 15 women ( 17.9% ) ) treated in the protocol between 2000 and 2008 were included in this analysis . 
the median follow - up time of all patients alive was 36months ( range : 484months )  . treatment compliance and safety radiotherapy was completed to 69.2gy ( ccb ) or 70.2gy ( cf ) in 76patients ( 90.6% ) , 8patients received less than 70.2gy but more than 65gy , while the treatment of 1patient was stopped at 39.6gy and was not included in the survival analysis . 
 long - term toxicity was documented completely in 64patients ( 78.6% ) : osteoradionecrosis of the jaw was observed in 5patients ( 6.0% ) , permanent loss of taste occurred in 39patients ( 46.4% ) , 49 patients suffered from chronic dysphagia ( 58.3% ) , chronic mucositis occurred in 31 patients ( 36.9% ; 5with gradeiii / iv ) , chronic dermatitis in 20patients ( 23.8% ) ; 38patients ( 45.2% ) suffered from chronic pain ; in 14patients ( 16.7% ) laryngeal edema was documented . 
none of the patients suffered from chronic myelopathy in the follow - up period . survival and local control of 83 patients analyzed , 46 patients had died by end of the study . 
 patients treated with ccb had a 2 - year os probability of 47.6% ( 95% ci : 41.254.9 ) compared to 38.7% ( 95% ci : 25.252.2 ) for cf patients ( p = 0.73 , see figure 2 )  . 
 type of recurrence a total of 75 patients ( 89.3% ) were evaluable for recurrence analysis : 12 patients ( 16% ) developed distant metastases , 18patients ( 24% ) had a recurrent primary tumor , and 16patients ( 16.3% ) developed nodal recurrence . 
a second primary tumor was diagnosed in 5patients ( 6.7% ) , 7patients with recurrent primary tumor had simultaneous nodal recurrence , and 3patients with primary recurrence also developed distant metastases . discussion radiochemotherapy of advanced head and neck cancer remains a challenge for even experienced radiation oncologists to balance antitumor efficacy and treatment - related toxicity . 
 paclitaxel as " second generation " chemotherapy agent has shown antitumor efficacy when used in phase i and ii concomitant radiochemotherapy protocols with acceptable toxicity [ 7 , 11 , 16 , 24 ]  . 
 [ 6 ] , the recommended weekly paclitaxel dose was adjusted from the initial 60mg / m2 to 40mg / m2 together with carboplatin weekly auc1 and conventionally fractionated radiotherapy . 
 [ 1 ] reported on a phaseii trial including mostly operable patients treated with hyperfractionated radiotherapy , 3 times 5 - fu ( 750mg / m2 ) , cisplatin ( 50mg / m2 ) , and paclitaxel ( 70mg / m2 ) , and described manageable toxicity and good os and pfs rates . 
according to our data , the time of patients depending on feeding tubes is long or even life - long , although dysphagia may not only be treatment related but also an effect of the tumor itself . 
 despite pretreatment dental extraction being performed if necessary , the rate of osteoradionecrosis in this study was high but comparable to other intensive radiochemotherapy protocols [ 4 , 21 ] , including imrt [ 9 ]  . 
therefore , carboplatin is much better tolerated in multimorbid patients , especially those with increased cardiac risk . unacceptable hematological toxicity of taxane - containing induction chemotherapy protocols is currently debated . 
definitive rt of advanced h&n cancer with carboplatin and paclitaxel that of concurrent radiochemotherapy , the rate of severe hematological complications is quite low in our concurrent protocol . the combination of radiotherapy with targeted drugs , such as egfr - receptor inhibitors or tyrosine kinase inhibitors , has enhanced the treatment options in head and neck cancer . 
the relative low toxicity apart from skin toxicity makes this method attractive for patients otherwise not fit for concomitant radiochemotherapy [ 20 ]  . the percentage of patients with known hpv association was not determined in this study . 
as a much better outcome is observed in patients with hpv - associated tumors , the prognostic influence in this subgroup of patients with very advanced tumors is awaited . originalarbeit hmangiosarkom nach brusterhaltender therapie beim mammakarzinom : vier fallbeispiele mit molekulargenetischer diagnostik und literaturbersicht carolin nestle - krmling1 , 8 , edwin blke2 , wilfried budach2 , matthias peiper3 , 9 , dieter niederacher1 , wolfgang janni1 , claus ferdinand eisenberger3 , wolfram trudo knoefel3 , axel scherer4 , stephan ernst baldus5 , guido lammering2 , 6 , peter arne gerber7 , christiane matuschek2 hintergrund : die seltenen hmangiosarkome der mamma werden zunehmend hufiger beobachtet . 
ursache sind die heutzutage etablierten brusterhaltenden therapiekonzepte , bei denen die radiotherapie der restbrust eine feste therapieoption ist . patienten und methode : in dieser arbeit werden vier eigene flle mit molekulargetischer diagnostik und die aktuelle literaturbersicht beschrieben . 
eine genetische prdisposition wird angenommen , lie sich aber anhand der eigenen untersuchungen der tumorsuppressorgene brca1 , brca2 sowie p53 bei unseren patienten nicht nachweisen . schlussfolgerung : aufgrund der unsicheren datenlage umfasst die therapieempfehlung beim hmangiosarkom neben der radikalen tumorresektion im gesunden uneinheitliche systemische chemooder immuntherapieregime , die sich zumeist an der therapie anderer seltener hautsarkome wie dem kaposisarkom orientieren . 
eine systematische , registerbasierte erfassung aller flle wird in deutschland angestrebt . schlsselwrter : hmangiosarkom mammakarzinom sekundre neoplasie brusterhaltende therapie radiotherapie tram - flap strahlenther onkol 2011 ; 187 : 65664 doi 10.1007 / s00066 - 011 - 2251 - 5 hemangiosarcoma after breast - conserving therapy of breast cancer : report of four cases with molecular genetic diagnosis and literature review background : hemangiosarcomas of the breast represent a rare disease of the breast mainly occurring as secondary neoplasias with a latency of 510 years after primary treatment of breast cancer and are associated with an unfavourable prognosis . 
radiation therapy , which is integrated within the concept of breast conserving therapy ranks as the main risk factor . patients and methods : in this report we describe the clinical course of 4 patients including their molecular genetic pattern and give a summary of the actual literature . 
a genetic predisposition is assumed , but we could not find a significant role of tumor suppressor genes brca1 , brca2 or p53 in our patients . conclusion : due to limited data available for these tumors , recommendations for therapy include radical tumor resection achieving wide free margins and inconsistent regimens of chemoand / or immunetherapy modalities . 
efforts should be taken for a nationwide systematic registration of all cases of post - irradiation hemangiosarcomas . key words : hemangiosarcoma breast cancer secondary neoplasia breast conserving therapy radiation therapy tram flap 1frauenklinik , universittsklinikum dsseldorf , 2klinik und poliklinik fr strahlentherapie und radiologische onkologie , universittsklinikum dsseldorf , 3klinik fr allgemein - , viszeral und kinderchirurgie , universittsklinikum dsseldorf , 4institut fr radiologie , universittsklinikum dsseldorf , 5institut fr pathologie , universittsklinikum dsseldorf , 6radioonkologie ( maastro clinic ) , maastricht , the netherlands , 7hautklinik , universittsklinikum dsseldorf , 8aktuelle adresse : klinik fr senologie , sana - krankenhaus , dsseldorf - gerresheim , 9aktuelle adresse : klinik fr allgemein - , viszeralund unfallchirurgie , kliniken essen - sd , essen . 
mit der zunahme brusterhaltender therapiekonzepte ( heutzutage bis zu 70% aller therapierten mammakarzinome ) ist innerhalb einer mittleren latenzzeit von 5 , 5 jahren ( 110 jahre ) mit einer zunehmenden inzidenz an hmangiosarkomen zu rechnen . 
problematisch ist die hohe lokalrezidivrate von bis zu 90% ( im mittel bereits nach 7 , 5 monaten ) sowie jede pulmonale und hepatische metastasierung [ 6 , 15 , 32 , 39 , 43 ]  . wir berichten hier ber vier patientinnen , die sich mit einem teilweise bereits mehrfach rezidivierten hmangiosarkom im thoraxbereich vorstellten . 
zur abklrung einer eventuell bestehenden , genetisch prdisponierenden strahlensensibilitt [ 3 ] wurde bei drei patientinnen auerdem ein stammbaum erstellt und eine komplette molekulargenetische diagnostik der tumorsuppressorgene brca1 und 2 ( brustkrebsgen 1 und 2 ) sowie p53 durchgefhrt . 
in russland war 5 jahre zuvor ( 1995 ) ein primres mammakarzinom ( stadium pt1b pn0pm0 cm0 , gx , er positiv , pr negativ ) brusterhaltend operiert , nachbestrahlt sowie eine adjuvante endokrine therapie mit tamoxifen 20 mg tglich durchgefhrt worden . 
im april 1999 wurde bei einer neu aufgetretenen hyperpigmentierung , deformierung sowie starkem dem der linken brust unter dem verdacht auf ein hmangiosarkom ( dd : malignes melanom ) die ablatio der linken brust durchgefhrt und histologisch ein hmangiosarkom gesichert . 
es erfolgte daraufhin eine adjuvante chemotherapie mit vier zyklen vincristin ( 1 , 5 mg / m2 ) / doxorubicin ( 50 mg / m2 ) / cyclophosphamid ( 500 mg / m2 )  . 
unter dieser therapie kam es 6 monate spter ( oktober 1999 ) zu einem hmangiosarkomrezidiv im narbenbereich der thoraxwand , welches exzidiert und mit einem abdominalen advancement - lappen gedeckt worden war ( keine angaben ber tumorfreiheit der resektionsrnder )  . 
anschlieend erfolgte eine systemische therapie mit interferon a zweimal wchentlich sowie erneuter tamoxifengabe ( 20 mg ) bis juli 2000 . es wurde bei einem erneuten rezidiv eine chemotherapie mit sechs gaben von docetaxel ( 35 mg / m2 kof ) wchentlich sowie eine begleitende erneute restdosis - oberflchenbestrahlung der thoraxwand durchgefhrt ( 8 / 2000 )  . 
3 monate nach der letzten chemotherapie stellte sich die patientin im dezember 2000 erneut mit schmerzen der linken thoraxwand und lokaler klinischer progredienz einer akut 20 10 cm messenden infiltration vor ( abbildung 1 )  . 
das operationsprparat zeigte ausgedehnte anteile des bekannten hmangiosarkoms innerhalb des stratum papillare des koriums sowie im tiefer gelegenen subkutanen fettgewebe , welches kleinherdig bis in den lateralen und dorsalen resektionsrand hineinreichte . 
die familienanamnese war mit ausnahme eines kolonkarzinoms einer cousine unauffllig . wegen einer tief blau - roten verfrbung mit peaudorange - bildung im bereich der linken brust wurde im februar 2000 auswrts ber eine hautbiopsie die histologische distrahlenther onkol 2011 no . 
patient 2 : second tumor recurrence after resection of the tumor close to the sternum and surgery with a transposition flap . agnose einer fibrose und benignen angioproliferation gestellt , die auf die strahlentherapie zurckgefhrt wurde . 
nachdem es im verlauf zu einer progredienz des befundes kam , ergaben erneute biopsien die diagnose eines hmangiosarkoms , welches im juni 2000 auswrts mittels mastektomie und deckung durch ein abdominales advancement therapiert wurde ( r - status unbekannt )  . 
5 monate spter ( 11 / 2000 ) trat ein zweites rezidiv im bereich der linken thoraxwand auf , so dass sich die patientin in der universitts - frauenklinik vorstellte ( abbildung 2 )  . auch in diesem fall erfolgte nach seriellen hautbiopsien zur beurteilung der befundausdehnung eine ausgedehnte thoraxwand - weichteilresektion des hmangiosarkom - rezidivs mit defektdeckung durch einen doppelt gestielten tram - lappen . 
4 jahre ( 4 / 2000 ) zuvor war auswrts ein auf der rechten seite hormonrezeptorpositives mammakarzinom ( stadium pt1c pn0 cm0 , g2 ) brusterhaltend operiert und nachbestrahlt worden . 
bei der vorstellung im hiesigen brustzentrum zeigten sich die bereits histologisch gesicherten multizentrischen rundlich - knotigen und typisch lividen rezidivherde des hmangiosarkoms im bereich der rechten bestrahlten thoraxwand und axilla . 
die staging - untersuchungen ergaben keine hinweise auf weitere tumorabsiedelungen , so dass nach seriellen punchbiopsien der haut eine radikale tumorresektion mit beidseitiger extensiver resektion der thoraxwand - weichteile inklusive der linken restmamma erfolgte . 
die histologische aufarbeitung ergab ausgedehnte sarkominfiltrate beider thoraxwandseiten und wurde bis auf ein dorsales , prpektorales areal mit heranreichen eines tumorherdes an den absetzungsrand im gesunden reseziert ( abbildung 4 )  . 
patient after 4 years with no signs of recurrence ( c )  . der weitere verlauf war ber insgesamt 4 , 5 jahre unauffllig ohne einen anhalt fr ein lokoregionres rezidiv oder eine metastasierung . 
die von uns veranlasste bestimmung der vegf - rezeptoren ergab fr vegf - 1 einen positiven befund , so dass im falle eines erneuten rezidivs als ultima ratio eine individuelle therapieempfehlung mit bevacizumab ( anti - vegf ) erwogen wurde . 
nach abschluss der radio und chemotherapie wurde eine antihormonelle therapie mit einem aromatasehemmer eingeleitet . im ct - thorax - abdomen wurde der verdacht auf ossre metastasen rechtsseitig im wirbelkrperbogen und processus costalis des lendenwirbelkrpers ( lwk ) 4 sowie linksseitig in der massa lateralis des os sacrum geuert . 
aufgrund der ausgeprgten schmerzsymptomatik im bereich der mamma sowie des thoraxwandtumors rechts erfolgte eine subscapulre tumorresektion inklusive rippen - teilresektion mit defektdeckung mittels vicryl - netz und latissimus - muskellappen sowie eine mastektomie beidseits . 
die early breast cancer trialists cooperative group zeigte auf dem jahreskongress der european society for therapeutic radiology and oncology ( estro ) in leipzig 2006 , dass die strahlentherapie das risiko fr ein sarkom um den faktor 2 , 34 erhht , wobei die meisten sarkome angiosarkome waren ( unpublizierte daten )  . 
da sich allerdings bei unseren patienten keinerlei anzeichen fr das vorliegen einer ataxia teleangiectatica zeigten , wurde auf die entsprechende molekularbiologische diagnostik verzichtet . es ist allerdings bekannt , dass patientinnen mit mammakarzinom ein erhhtes risiko fr das auftreten von malignen zweittumoren aufweisen . 
als hauptrisikofaktor fr die entstehung von weichteilsarkomen gilt dabei eine vorausgegangene bestrahlung der entsprechenden weichteilregion mit prdisposition des thoraxwandund schulterbereichs [ 10 ]  . die retrospektive analyse einer franzsischen arbeitsgruppe zeigt einen zusammenhang zwischen brusterhaltender therapie mit strahlentherapie und dem auftreten eines angiosarkoms . 
dieses phnomen knnte auf die hher applizierte strahlendosis der zumeist durchgefhrten zustzlichen boostbestrahlung bei brusterhaltung zurckzufhren sedie zunahme der brusterhaltungsrate mit der bis auf wenige ausnahmen obligaten bestrahlung der restbrust , aber auch die zunahme der indikation zur bestrahlung nach mastektomie [ 40 , 41 ] lassen einen absoluten anstieg der sarkom - zweitneoplasien erwarten . 
andere untersucher konnten den zusammenhang von weichteilsarkomen und einem chronischen lymphdem des armes oder auch der brust ( stewarttrewes - syndrom ) nach mastektomie und strahlentherapie darstellen [ 26 , 29 ]  . 
hierbei kann auch das dem allein , selbst ohne vorausgegangene strahlentherapie , zu einem angiosarkom fhren . verschiedene berichte legen darber hinaus einen zusammenhang zwischen verschiedenen , genetischen vernderungen im bcra1und bcra2 - gen ( brustkrebsgen 1 und 2 ) , p53 - gen sowie ataxia - teleangiectatica - gen nahe [ 19 ]  . 
des weiteren knnen womglich andere nichtspezifische vernderungen von dna - reparatur - mechanismen eine erhhte strahlensensibilitt induzieren [ 31 ]  . hinsichtlich pathomorphologischer differenzierungsmerkmale zur diagnostik von angiosarkomen wird die immunhistochemie herangezogen . 
als endothel - zellmarker erfolgt eine faktor - viii - antigen - frbung ( von - willebrandfaktor ) sowie die positive reaktion auf cd31 und cd34 [ 29 ]  . 
hmangiosarkom nach brusterhaltender therapie exprimieren knnen , sind sie zumeist strogen - , progesteron sowie androgenrezeptornegativ [ 49 ]  . auch unter einer kombinierten radiochemotherapie mit 5 - fluorouracil ein ansprechen erreicht werden [ 57 ]  . das tumorgrading gilt als wichtigster histopathologischer prognosefaktor , welches mit dem differenzierungsgrad in negativer weise korreliert [ 5 , 9 ]  . therapeutisch steht die radikale chirurgische entfernung des tumors im sinne einer r0 - resektion weit im gesunden im vordergrund . 
auch wenn in einem retrospektiven vergleich publizierter flle kein unterschied hinsichtlich der ergebnisse nach einer weiten exzision oder mastektomie gefunden wurden [ 20 , 32 , 37 ] , so unterscheidet sich doch die lokale rezidivfreiheit mit 80% nach 5 jahren signifikant bei in sano resektion vs . 
in der regel entspricht dieses dem operativen vorgehen bei der mastektomie . theoretisch muss auch von einer tumor - prdiposition im gesamten bestrahlungsareal ausgegangen werden , welches fr die problematik der hufigen lokalrezidive trotz in - sanoresektion verantwortlich sein knnte . 
bei diesen drei kasuistiken erscheint jedoch die ausgeprgte strahlenempfindlichkeit der haut auffllig , welche bei einer patientin sogar zum abbruch der strahlentherapie gefhrt hatte . die effektivitt einer adjuvanten chemotherapie bei angiosarkomen ist derzeit nicht belegt . 
fr paclitaxel als monosubstanz konnte bei neun patienten mit einem gesichts - angiosarkom ber eine ansprechrate von 89% berichtet werden [ 16 ]  . in unserer ersten kasuistik wurde nach vorausgegangenen standard - chemotherapieschemata eine passagere remission nach nur sechsmaliger wchentlicher gabe von docetaxel erzielt . 
thalidomid ist derzeit fr die behandlung der erythema nodosum leprosum zugelassen und wird bei aids - patienten mit einem kaposi - sarkom sowie bei graft - versus - host - reaktion klinisch erprobt . 
 in abhngigkeit von entsprechenden tumorzelloberflchenantigenen , wie in unserem dritten fall , knnte die gabe eines vegf - antikrpers wie bevacizumab experimentell zum einsatz kommen . aufgrund der unsicheren datenlage wurde der aufbau eines nationalen registers zur erfassung der postradiogenen angiosarkomflle nach mammakarzinomtherapie im deutschsprachigen raum initiiert . ferner bestehen unklarheiten bezglich genetischer dispositionen . 
 schlussfolgerung die zunahme brusterhaltender operationen mit adjuvanter bestrahlung der restbrust sowie die steigende anzahl publizierter sekundrer hmangiosarkome in dieser gruppe legt einen direkten oder indirekten zusammenhang zwischen grunderkrankung und therapie nahe . 
10 original article regional hyperthermia combined with chemoradiotherapy in primary or recurrent locally advanced pancreatic cancer an open - label comparative cohort trial sergio maluta1 , moshe schaffer2 , fabio pioli1 , stefano dalloglio1 , stefano pasetto1 , pamela m . 
schaffer3 , bernard weber3 , maria grazia giri4 purpose : to evaluate the therapeutic effect of delivering regional hyperthermia ( ht ) plus chemoradiotherapy ( crt ) in patients suffering from locally advanced unresectable pancreatic cancer ( lapc )  . methods : between january 2000 and december 2008 , 68 patients affected by primary ( 56 / 68 ) or recurrent ( 12 / 68 ) lapc were treated either with crt alone or crt plus ht . 
ht did not increase crt toxicity . conclusion : ht can be added safely to crt in lapc , thus , resulting in slightly prolonged survival in certain cases . key words : pancreatic cancer hyperthermia chemoradiotherapy strahlenther onkol 2011 ; 187 : 61925 doi 10.1007 / s00066 - 011 - 2226 - 6 regionale hyperthermie kombiniert mit chemoradiotherapie bei erstdiagnose oder rezidiv eines primren oder rezidivierten lokal fortgeschrittenen pankreaskarzinoms : eine offene kohortenvergleichsstudie ziel : die evaluierung des therapeutischen effekts der regionalen hyperthermie ( ht ) , kombiniert mit chemoradiotherapie ( crt ) bei patienten mit einem lokal fortgeschrittenen , nicht resektablen pankreaskarzinom ( lapc )  . methoden : zwischen januar 2000 und dezember 2008 wurden 68 patienten mit erstdiagnose ( 56 / 68 ) oder rezidiv ( 12 / 68 ) eines lapc mit crt alleine oder mit crt in kombination mit ht behandelt . 
das mediane berleben ( os ) war 15 monate in der hat - gruppe versus 11 monate in der kontrollgruppe ( logrank - test : p = 0 , 025 )  . 
der zusatz einer ht fhrt zu keiner erhhung der nebenwirkungen der crt . schlussfolgerung : die ht kann ohne bedenken einer crt bei lapc hinzugefgt werden und ermglicht in bestimmten fllen das os zu verlngern . 
 schlsselwrter : pankreaskarzinom hyperthermie chemoradiotherapie 1department of radiotherapy , university hospital , verona , italy , 2department of oncology , ziv medical center and school of medicine , zefat , israel , 3bad trissl oncology hospital , oberaudorf , germany , 4department of health physics , university hospital , verona , italy . received : october 4 , 2010 ; accepted : june 30 , 2011 published online : september 19 , 2011 strahlenther onkol 2011 no . 
hyperthermia in pancreatic cancer introduction pancreatic cancer is the fourth frequent cause of cancer death in men and women in the united states with more than 37 , 000new cases per year and more than 33 , 000deaths from the disease . 
locally advanced pancreatic cancer ( lapc ) is defined as a surgically unresectable tumor because of the involvement of the celiac axis or the superior mesenteric artery , without evidence of distant metastases . 
according to the surveillance , epidemiology , and end results ( seer ; seer.cancer.gov ) database , about 26% of patients affected by pancreatic cancer are considered lapc and have a 5 - year overall survival ( os ) rate of 8.7%. 
 many studies investigated 5 - fluorouracil ( 5fu ) combined with rt ; treatment with 5fu plus rt increased os and quality of life in patients with lapc , as supported by the trials from the gastrointestinal tumor study group ( gitsg ) [ 25 ] and the eastern cooperative oncology group ( ecog 8282 ) [ 3 ]  . over the last 10years , gemcitabine ( gem ) has become the standard ct regimen in lapc , especially in combination with rt , as gem is also an active radiosensitizer . 
 in an australian multicenter trial , patients affected by lapc were treated with chemoradiotherapy ( crt ) [ 9 ] : gem was first administered in an induction phase together with 5fu and oxaliplatin , then concurrently with rt and then in the consolidation phase . 
it should be noted that less than one third of the patients enrolled in the study completed more than 80% of the planned treatment due to progressive disease or toxicity . considering these results , even a small benefit in terms of os is of importance and new therapies need to be continuously tested in order to improve the treatment of lapc without a concomitant increase of toxicity . 
cell cycle analysis with flow cytometry demonstrates that the effect may be due to an accumulation of cells in the s phase , which are known to be particularly sensitive to heat cytotoxicity [ 16 , 22 ]  . 
the effects of ht at various temperatures on intracellular uptake of 5fu and its conversion to active metabolites were also examined [ 23 ] ; it was found that temperatures ranging from 3942c are effective in increasing the rate of intracellular uptake of 5fu . 
 in a recent manuscript , raji human lymphoma cells were incubated with carboplatin , cisplatin , oxaliplatin , carmustine , gemcitabine ( gem ) , and etoposide at 37c or 42c and evaluated for cell culture growth [ 15 ]  . 
 there was a synergism of cytostatic effects of platinum drugs ( carboplatin , cisplatin , and oxaliplatin ) with cytostatic effect of heating to 42c and the summation of the cytostatic effect of carmustine or etoposide with the action of hyperthermia . 
 patients and methods patients between january 2000 and december 2008 , 68patients affected by primary or recurrent pancreatic carcinoma were enrolled in a prospective open - label comparative cohort trial . 
all patients were affected by primary pancreatic cancer , except for 5 patients in the ht group and 7 patients in the control group , who had a recurrent pancreatic carcinoma after pancreatic resection . 
 in spite of the lack of randomization , the two groups were well balanced in terms of age , gender , stage , lymph node status , distant metastases , and tumor localization ( table 1 )  . 
 m1 patients were eligible to be included in the study if the only organ involved was the liver and their life expectancy was judged to be more than 6months , according to the physicians discretion . 
we , therefore , enrolled 8metastatic patients , of whom 6patients were treated with crt plus ht and 2with crt alone . treatment an overview over the percentage of patients receiving the respective schemes of ct , rt , and / or ht is provided in table 3 . rt was delivered to the pancreas and the regional lymph nodes with a linear accelerator of energy > 6mv , using a 3d conformal technique . 
treatment volumes included the primary tumor , as defined on ct or pet - ct scans , and the areas of potential nodal involvement with at least a 3 cm margin in all directions covering the pancreaticoduodenal , portal hepatic , and celiac axis lymph nodes . 
der behandlungszyklus wurde alle 15 tage wiederholt . day 1 gemcitabine 1 , 000 mg / m2 day 2 day 3 day 4 hyperthermia start of rt course hyperthermia programs were used routinely . 
to counteract or avoid nephrotoxicity and hematological complications , the radiation field was required to spare the left kidney and half of the right kidney , while the spinal cord dose was limited to 45gy . in the ht group ( n = 40 patients ) , 66 gy / 33 fractions were delivered to 8patients , 60gy / 30fractions to 3patients , 42gy / 14fractions to 10patients , 30gy / 10fractions to 17patients ; 2 patients underwent stereotactic irradiation with 40gy in 4fractions of 10gy . 
in the control group ( n = 28patients ) , 66 gy / 33 fractions were administered to 2 patients , 60gy / 30fraction to 3patients , 42gy / 14fractions to 5patients , 30gy / 10fractions to 15patients , while 3patients received stereotactic irradiation with 40gy in 4fractions of 4gy . chemotherapy was scheduled as follows : in the ht cohort , gem was administered alone in 29 / 40 patients ; each cycle consisted of gem 1 , 000mg / mq day1 , ht day2 , initiation of rt plus ht on day4 ( table 4 ) ; the treatment cycle was repeated on day15 . 
gem and cisplatin were delivered in 7 / 40patients ; each cycle consisted of gem 1 , 000 mg / mq day 1 , ht day 2 , starting of rt plus ht day4 , cisplatin 30mg / mq day8 , cisplatin 30mg / mq day21 ; subsequently , the cycle was repeated . gem plus 5fu was delivered in 3 / 40patients ; each cycle consisted of gem 1 , 000mg / mq day1 , ht day2 , starting of rt plus ht day4 , 5fu 350mg / mq day8 . 
gem and oxaliplatin were delivered in 1patient ; at each cycle , gem was delivered at 1 , 000mg / mq day1 , ht at day2 , starting of rt plus ht at day4 , oxaliplatin 45mg / mq at day8 ; each cycle consisted of 21days . in the control cohort ( n = 28 ) , gem was administered alone in 19 patients , with cisplatin in 5 patients , 5fu in 3pastrahlenther onkol 2011 no . 
the doses of ct agents were the same as in the ht cohort ; the scheduling of ct and rt was also the same , with the exception of the absence of ht . 
 in all patients of both cohorts , ct was protracted until the end of rt ; the number of post - rt cycles of ct varied among patients according to the physicians discretion . prior to each ct administration , the following criteria had to be met : absolute neutrophil count 1 , 000 / l , platelets 100 , 000 / l , and absence of grade 2 nonhematologic toxicity . 
if any of these criteria were not met , treatment was postponed by 1 week and eventually stopped if minimum treatment conditions were still not met after 2 consecutive delays . 
the total dose of gem administered did not differ between the two groups . sufficient hydration to ensure a urinary output of at least 100ml / h before and 4h after the infusion of ct was required . 
 the tumor region was heated with circular arranged phase steered antennas in the radio wave range ( 80120mhz ) , using a bsd 2000 sigma eye applicator to achieve better control of the power density distribution . 
although invasive thermometry is recognized as the best way of measuring the temperature during the treatment , we decided to perform noninvasive endocavitary thermometry with a thermometer in the rectal lumen . 
for each treatment session , we determined the index temperatures , tmax , t90 , and tmt90 is the temperature reached or exceeded by 90% of the measurement points ; tmax and tmin are the maximal and minimal temperatures achieved at each ht session , respectively . 
 data analysis the primary endpoint of our study was os ; it was defined as the interval between the date of treatment choice and the date of death ( or date of last follow - up for surviving patients )  . 
the most common hematological toxicity was grade2 anemia ( 3patients in the ht group , 2patients in the control group ) , followed by grade2 neutropenia ( 2patients in each group ) , and elevate ast and / or alt ( 2patients in each group )  . 
these data show a homogeneous distribution of registered temperatures among ht sessions . efficacy after a 12 - month follow - up , 22 / 34patients ( 64.7% ) in the ht group and 16 / 26patients ( 61.5% ) in the control group were still alive . 
median os was 15months ( range : 620months ) in the ht group versus 11months ( range : 513months ) in the control group ( log - rank test : p = 0.025 ; figure 2 )  . 
although the difference in median os is statistically significant , the lack of randomization in this study compels us to be very careful in interpreting whether this difference is due to ht . cumulative proportion surviving ( kaplan - meier ) complete censored group 0 group 1 time ( months ) figure 2 . 
although the trial is not randomized , the characteristics of patients in the two cohorts were well balanced ( table 1 )  . the concomitant application of gem and ht has been previously tested on pancreatic cancer cell lines [ 1 ]  . 
this japanese study confirmed the hypothesis that the gem - mediated activation of nf - b ( a transcription factor implicated in gem resistance ) in pancreatic cell lines might be inhibited by heat , with subsequent enhancement of geminduced cytotoxicity . in addition , an interval of 20 or 24h between exposure to gem and ht led to enhanced cell lethality in cultured human lung cancer cell lines [ 11 ]  . 
one important series is the ecog study , a phase iii randomized trial with rt plus 5fu and mitomycin c ( 55patients ) versus rt alone ( 49patients ) [ 5 ]  . 
in the gercor trial [ 12 ] , the authors tested a particular treatment option , using ct first followed by crt in patients with controlled tumors ( i.e. , stable disease or with an objective response )  . 
these results are in accordance with systematic reviews or meta - analyses of crt in the treatment of lapc [ 27 , 28 , 35 ]  . ht plus ct was tested in studies performed by the munich [ 31 ] and the kyoto [ 14 ] groups . 
only two studies ( one from austria [ 18 ] and the gercor trial [ 12 ] ) achieved outcomes similar to ours in terms of median os and 1 - year os . 
furthermore , in the gercor trial , a rt dose of 65gy instead of a standard dose of 5455gy was delivered and patients in progression after initial ct ( about 30% ) were excluded from the study . 
for these reasons , our survival rates are not comparable with the subgroup of long - term survivors of the gercor trial . on the other hand , addition of hyperthermia sensitizes to radiation [ 6 ] , gaining a therapeutic effect at subtherapeutic doses of radiation without adding additional toxicity , as hyperthermia - related reactions are only acute and do not lead to late toxicity per se . 
the efficacy of triple modality therapy was also demonstrated in other tumor entities , e.g. , recurrence of rectal cancer [ 24 ]  . a quite homogeneous distribution of time - averaged temperatures was registered during ht at paratumoral endoluminal sites ( rectum , stoma , or vagina ) , which are known to be sufficient to estimate feasibility and effectiveness of a hyperthermia treatment . 
however , our trial was not randomized and was designed to investigate the noninferiority of crt plus ht versus crt alone . finally , there is evidence that ht plus crt is superior to crt alone , when using the regimens employed in this study . 
the efficacy data seem promising suggesting a slight but significant increase in survival in patients who suffer from a disease with very poor prognosis . strahlenther onkol 2011 ; 187 : 675704 doi 10.1007 / s00066 - 011 - 1004 - 9 abstracts ict 2011 international conference on tomotherapy heidelberg , germany september 1617 , 2011 organizers : faculty : jrgen debus , klaus herfarth , gabriele sroka - perez j . 
wong verlag urban & vogel , mnchen strahlentherapie und onkologie contents 677 prostate ( fc - 1 fc - 4 ) 678 sarcoma and hypofractionation ( fc - 5 fc - 10 ) 681 physics ( fc - 11 fc - 16 ) 683 miscellaneous ( fc - 17 fc - 23 ) 685 head - and - neck ( fc - 24 fc - 28 ) 688 breast , gynecology ( fc - 29 fc - 33 ) 690 new developments ( fc - 34 fc - 37 ) 692 poster presentations ( p1 p23 , p26 p32 ) 703 author index strahlenther onkol 2011 no . 
10 urban & vogel addendum : tomotherapy 2011 oral presentations prostate fc - 1 strahlenther onkol 2011 ; 187 : 677 hypofractionated tomotherapy treatment ( htt ) in prostate cancer lymph nodal relapse detectedby 11c - choline pet / ct g . 
di muzio1 1san raffaele hospital , radiotherapy , milano ; 2san raffaele hospital , physics dpt , milano ; 3san raffaele hospital , urology , milano , italy purpose : the aim isto update the hypofractionated tomotherapy treatment ( htt ) feasibility - study , by evaluation of acute / late toxicity and clinical outcome , in lymph nodalrelapse of patients ( pts ) already treated for prostate cancer and the role of11c - choline pet / ct as a guide of tomotherapy treatment . 
 material : from january 2005 to december 2010 , 40 prostate cancer pts with biochemical recurrenceafter prostatectomy ( psa0 > 0.2 ng / ml ) and with evidence of lymphnodal relapse at re - staging 11c - choline pet / ct ( pet / ct0 ) , were treatedwith high dose moderate hypofractionated tomotherapy treatment , guided by11c - choline pet / ct0 images . 
to evaluate treatment efficacy , psaserum measurement ( psa1 ) ( all pts ) and 11c - choline pet / ct ( pet / ct1 ) ( n = 19 ) were performed after treatment and compared to basal evaluations . 
in 36 / 40pts pet / ct0 suggested the presence of para - aortic and / or pelvic lymphnodal metastases ( lnms ) and mediastinal lymph nodes in the remaining 4 pts.pet / ct0 positive lymph nodes were treated with high dose radiotherapyusing a simultaneous integrated boost , as allowed by tomotherapy . 
after htt 37 / 40 pts documented significant reductionof psa value , 20 / 40 showed a psa valueless than 0 , 2 ng with a median duration of the response of 14 , 48 months ; 15 / 40 maintainedthis psa value for 25 months . 
among the 21 pts with follow - upgreater than 12 months , only 5 had g1 late toxicity ( 1 ge and 4gu ) ; none showedg2 - g3 late toxicity . conclusion : these preliminary data show that htt - 11c - cholinepet / ctguided is safe and effective in lymph nodal relapse of previouslytreated prostate cancer patients and could be a valid alternative to chemotherapy.although further evaluations are necessary , the good rate of local controlsuggests that htt treatment guided by 11c - choline pet / ct images may bereasonably proposed in these patients . fc - 2 strahlenther onkol 2011 ; 187 : 677 comparison of supine and prone treatment position for prostate cancer patients irradiated with tomotherapy t . 
kazmierska1 1greater poland cancer centre , ii radiotherapy department , poznan ; 2greater poland cancer centre , department of medical physics , poznan , poland backgrund : in the literature there are various papers exploring differences in dose distribution for prostate cancer patients relative to a treatment position supine or prone . 
techniques currently used , such as tomotherapy are much more conformal , thus the planning dose distribution between both positions can be more significant . purpose : to compare two different immobilization techniques prone and supine for patients with prostate cancer treated withebrt using helical tomotherapy . material and methods : the study included 47 patients with prostate cancer , radically irradiated with tomotherapy unit . 
gabriele1 1institute for research and treatment of cancer ( ircc ) candiolo , radiotherapy department , turin ; 2institute for research and treatment of cancer ( ircc ) candiolo , medical physic , turin ; 3institute for research and treatment of cancer ( ircc ) candiolo , turin , italy introduction / background / aim : the goal of this study was to assess the feasibility of image guided radiotherapy ( igrt ) by helical tomotherapy ( ht ) in patients affected by high risk ( hr ) or very high risk ( vhr ) prostate cancer ( pc ) , or affected by nodal recurrences , with / without local relapse , after radical treatment . 
ht allows a high conformation and dose escalation on tumor volumes with considerable spare of organs at risk ( oar ) , by daily megavoltage image . materials and methods : between october 2010 and april 2011 we treated 19 patients , in particular : 8 patients with nodal relapse after radical treatment ( in 1 cases recurrence at level of a single lymph node , in 7 cases recurrence in more than one lymph node ) and 12 patients with hr / vhr pc . 
 gastro - intestinal acute toxicity was evaluated in all patients and was the following : g1 in 10 patients ( 5 with nausea and 5 with moderate diarrhoea not requiring drugs ) ; g2 in 1 patient with extensive irradiation volume ( diarrhea requiring drugs ) ; no g3 - g4 toxicity was observed . 
genitourinary acute toxicity was g1 in 4 patients and g4 in one patient , with acute urinary obstruction requiring catheter , but this occurrence appeared after only three sessions ( at dose of 7.05 gy ) , and it resolved quickly with antibiotics , steroids and alpha 1 blockers . 
psa level was evaluated and it was decreased in all patients . discussion and conclusion : our initial experience shows that ht allows a good daily check of internal anatomy to ensure proper set - up patients . 
 our results are absolutely preliminary and further follow up is necessary to evaluate outcome and late toxicity . fc - 4 strahlenther onkol 2011 ; 187 : 678 tomotherapy for patients with prostate cancer at the medical center hamburg - eppendorf since 2006 r . 
tomotherapy for primary treatment of prostate cancer preliminary toxicity and remission data purpose : tomotherapy offers the possibility for intensity modulated and image guided radiotherapy in patients with prostate cancers . 
dose escalation is possible by boost integration for dose escalation in the prostate . material and methods : over the period of december 2006 to december 2008 82 patients with biopsy proven prostate cancer were treated primarily with helical tomotherapy . 
twenty - one patients were treated for a lowrisk prostate cancer , 24 patients for an intermediate - risk carcinoma , and 37 patients for a high - risk carcinoma . 
late complications and remission are analyzed . results : small target volumes ( prostate + / seminal vesicles ) were treated in 66 cases , additionally large volumes ( pelvic lymph nodes ) were irradiated in 16 cases . 
results of tomotherapy in patients with prostate cancer and hip endoprotheses purpose : endoprotheses of the hip bring some limitations for dose - escalated radiotherapy in the pelvis concerning the quality of the kv - planning - ct and dose distributions . 
tomotherapy treatment planning , daily image guidance by mv - ct and treatment results in patients with prostate cancer and hip endoprotheses are analyzed . material and methods : 19 patients with hip endoprotheses were irradiated with tomotherapy for prostate cancer . 
acute and late side effects are tolerable . sarcoma and hypofractionation fc - 5 strahlenther onkol 2011 ; 187 : 678 multitarget radiotherapy of primary disseminated multifocal ewings sarcoma with helical tomotherapy s . 
sterzing1 1university hospital heidelberg , radiation oncology , heidelberg ; 2department of radiation oncology , university hospital heidelberg , heidelberg , germany introduction : recent studies have proven the impact of local treatment of the primary tumor and all metastatic sites on the prognosis of patients with primary disseminated multifocal ewings sarcoma ( pdmes )  . 
helical tomotherapy is able to treat multiple tumor sites at a maximum length of 160 cm in one run and can therefore substantially accelerate dose delivery . patients and methods : four consecutive patients with pdmes were treated in our department with helical tomotherapy after chemotherapy . 
in the case of pulmonary metastases ( one patient with right - sided , one patient with bilateral lesions ) , the whole lung was irradiated with a total dose of 18 gy in 12 strahlenther onkol 2011 no . 
 conclusion : in a potentially curative setting , multitarget radiotherapy of patients with metastasized ewings sarcoma can be carried out with helical tomotherapy with good target coverage and excellent sparing of organs at risk . 
novel delivery techniques , namely dynamic jaw / dynamic couch technique , may further accelerate treatments due to fast couch travel between targets . fc - 6 strahlenther onkol 2011 ; 187 : 679 helical tomotherapy for radiotherapy of sarcomas where , when , why ? m . 
rper1 1tu mnchen , klinikum rechts der isar , department of radiation oncology , mnchen ; 2tu mnchen , klinikum rechts der isar , klinik fr orthopdie und sportorthopdie , mnchen , germany purpose : sarcomas are rare and should best be managed in specialized centres . 
this evaluation focuses on the role of helical tomotherapy ( ht )  . patients and methods : all sarcoma patients presenting between april 2007 ( installation of the tomotherapy hi - art system at our department ) and march 2011 were considered . 98 patients were identified : 17 lipo - , 13 sarcomas nos , 12 ewing - , 10 mfh , 9 myxofibro - , 7 chordomas , 6 rhabdomyo - , 6 angio - , 4 fibro - , 4 leiomyo - , 3 synovial , 3 osteo - , 2 chondrosarcomas , 1 clear - celland 1 dermatofibrosarcoma . 
we assessed the radiation source , technique , dose concepts , planning target volumes ( ptv ) in cm and length of ptv . results : median age of 98 patients ( 54 male ) was 59 years ( 6 - 84 years )  . 
pt site was a limb in 50 patients , trunk in 20 , spine / base of skull in 16 , abdominal in 7 and head and neck in 5 patients . 
 33 patients got ebrt at a linac ( 32 3d - crt , 1 imrt ) and 5 patients got stereotactic radiotherapy with a dedicated system , either as sfrt ( 4 ) or radiosurgery ( rs , 1 )  . 
 the other 54 patients ( 55 % ) underwent ht ( 21 patients with simultaneous integrated boost ) , 46 ht alone and 8 in combination with another radiotherapy ( rt ) technique : 3x interstitial hdr - brachytherapy , 2x stereotactic fractionated radiotherapy ( sfrt ) , 1x 3d - conformal ( 3d - crt ) externalbeam rt ( ebrt ) with a linac , 1x neutrons , 1x protons ( externally )  . 
linac target volumes were smaller with a median ptv of 852cm ( 86 - 5625cm ) and a restriction of ptv - length , median 18cm ( 7 - 37cm )  . 
stereotactic techniques were reserved to small volumes with a median ptv of 55cm ( 15 - 93cm ) and a ptv - length of 4cm ( 3 - 6cm )  . conclusion : ht was the preferred option in the treatment of large tumor volumes and of multiples rt sites . 
therefore , tomotherapy has become the method of choice in the treatment of sarcomas in our institution . supported by wilhelm sander - stiftung , germany ( wilhelm sander - therapieeinheit fr knochenund weichteilsarkome am klinikum rechts der isar , mnchen ) fc - 7 strahlenther onkol 2011 ; 187 : 679 hypofractionated radiotherapy using helical tomotherapy in the treatment of inoperable pleural mesothelioma e . 
polico1 1irst , radiotherapy , meldola ; 2irst , medical physics , meldola , italy aim : to evaluate the feasibility of total pleural radiotherapy with palliative aim in medically non - operable mesothelioma using an accelerated hypofractionated schedule and helical tomotherapy . 
 patients and methods : between january 2008 and december 2010 , 15 patients diagnosed with medically inoperable malignant pleural mesothelioma ( t2 / 4n0 / 3 ) , were treated by helical tomotherapy . 
three different volumes of interest ( voi ) were contoured in each case : roi 1 contains all the pleura ( involved and not - involved pleura plus diagnostic fistula ) , roi 2 ( total homolateral lung ) , and roi 3 ( roi 1 applied to the primary 1 cm isotropic reduction )  . 
the dose prescription was 25 gy / 5 daily fractions at the reference isodose ( 60% - 70% isodose ) with an increasing dose inhomogeneity up to 37.5 - 40 gy inside the reference isodose , corresponding mainly to the mesothelioma masses . 
the dose constraint used in the opposite lung was v5 / 5gy and the volume of the contralateral lung receiving 5 gy or more was observed to be less than 4% , and the average dose in the lung was lower than 4 gy . 
10 addendum : tomotherapy 2011 oral presentations fc - 8 strahlenther onkol 2011 ; 187 : 680 accelerated hypofractionated radiotherapy in inoperable locally advanced lung cancer using tomotherapy : our experience e . 
the dose prescription for gtv has always been 30 gy / 5 daily fractions at the reference isodose ( 60 - 70% ) with an increasing dose inhomogeneity inside the tumor , up to 40 gy . 
the dose prescription for the lymph node volume has always been 25 gy / 5 daily fractions at the reference isodose , with an increasing dose inhomogeneity up to 37.5 gy in the clinically involved lymph - nodes . 
this patient was surgically treated 70 days after completion of radiochemotherapy treatment . conclusions : preliminary data demonstrate the feasibility of a week - long treatment of the tumour by accelerated hypofractionated radiotherapy , while maintaining a dose similar to the oar or lower than conventional treatments , following 2 chemotherapy courses and 2 other chemotherapy cycles . 
this ongoing study underlines the possibility to administer hypofractionation not only for limited , small , pheripheral lesions but also for central primary tumor volumes ( t3 , t4 ) and for mediastinal lymph node stations . fc - 9 strahlenther onkol 2011 ; 187 : 680 feasibility and acute toxicity of single fraction half - body and wide pelvic irradiation with helical tomotherapy p . 
de la torre toms2 1hospital universitario puerta de hierro majadahonda , medical physics , majadahonda ; 2hospital universitario puerta de hierro majadahonda , radiation oncology , majadahonda , spain introduction : single fraction half - body irradiation has became an old fashioned pallitive treatment for wide spread bone metastatic patients mainly due to gi toxicity . 
nowadays , helical tomotherapy offers the possibility to delivery homogeneously high dose to the target volume while optimally sparing the organs at risk , specially the bowels . this work evaluates the feasibility of helical tomotherapy treatment by analyzing dose distributions , delivery quality assurances , precision of set up and the acute toxicity . material and methods : nine patients , 3 males and 6 females ( mean age 62 yo ) , previously diagnosed of wide bone metastatic disease , were treated using the accelerator tomotherapy hi - art ii . 
the dose prescription was 8 gray ( gy ) in a single fraction , except in three patients where the dose was 6.5 gy because the pelvic region had been previously treated . 
 the mean positioning corrections were 0.10 mm ( sd : 2.45 mm ) for lateral direction , - 1.38 mm ( sd : 5.49 mm ) for longitudinal direction , and 5.34 mm ( sd : 5.95 mm ) , for vertical direction . 
sanchez rubio1 1hospital universitario puerta de hierro majadahonda , medical physics , madrid , spain pulmonary irradiations involve location and dosimetric inaccuracies due to respiratory motion and inhomogeneity tissue , even more for high dose fractionations in case of small lung lesions where the reduction of normal tissue volume included in the ptv becomes essential . 
also a slow ct images set was obtained during free breathing in each case to use it for planning as an approach to the actual treatment situation ( an averaged density )  . 
the recommendations of rtog - 0236 - 0618 protocols for margins expansion ( 0.5cm in axial plane and 1.0cm in longitudinal direction ) were followed , slightly modified to avoid nearby oars such bronchial tree or ribs . 
doses prescriptions were also based in these protocols ( 60 or 54 gy in 3 weekly fractions ) a reduction of 2cc in gtvs volumes ( 13% - 20% for small lesions ) was obtained applying diaphragmatic compression . 
random errors for lateral and vertical axis are lower ( 2mm ) than longitudinal direction ( 3mm )  . pulmonary sbrt treatments are feasible in tomotherapy even without respiratory control : gtv shifts can be taken account , dose distributions satisfy rtog protocols and are truthful , treatment times are reasonable and igrt is suitable . 
jkel1 1heidelberger ionenstrahl - therapiezentrum ( hit ) , medizinphysik , heidelberg ; 2university hospital heidelberg , radiation oncology , heidelberg , germany for the treatment planning at the heidelberg ion - beam therapy center , water equivalent path length ( wepl ) is calculated based on kilovoltage ct ( kvct ) images . 
the aim of this study is to introduce dose calculation for carbon ions based on mvct and evaluate clinical feasibility . for a tomotherapy hi - art unit , a relation between wepl and hu was derived using a gammex phantom [ 2 ]  . 
to compare the results for both cases a 3d gamma analysis was performed . for the clinical case as well as for the recalculation in the head phantom gamma analysis shows acceptable results using 3mm distance to agreement ( dta ) and 7% dose difference . 
all these points are located at the distal edge , pointing out for remaining deficits in range calculation . for carbon ion beams dose calculation on tomotherapy mvct images were performed showing acceptable agreement in the first step . 
more detailed investigations on ct stability and resolution are ongoing . [ 1 ] wayne d newhauser , annelise giebeler , katja m langen , dragan mirkovic and radhe mohan can megavoltage computed tomography reduce proton range uncertainties in treatment plans for patients with large metal implants ? phys . 
50 ( 2005 ) 42594276 fc - 12 strahlenther onkol 2011 ; 187 : 681 image value to density calibration for kvct and mvct and possible effects on dose calculation s . 
dose distributions for a standard beam ( 2.5x10 cm ; 15s gantry period ) were calculated for three different water - equivalent phantoms ( one homogeneous , one with a lung - equivalent insert and one with a bone - equivalent insert ) , using for each phantom its corresponding ct scan and all three ivdts . 
for kvct , different helical treatment plans for two phantom cases ( homogeneous and with bony insert ) and three patient cases ( prostate , head & neck , chordoma ) were recalculated using ivdts for 80 kv , 120 kv , 140 kv and for 120 kv without a value for air . 
for different kv settings , maximum dose differences for the inhomogeneous phantom amounted also up to 6 % , while almost no differences were seen for the homogeneous phanto maximum dose differences for the patient cases were about 3 % , but varying for each treatment location . 
if no individual ivdts are used for different kv settings or if no correct value for air is included into an ivdt , the calculation errors are small , but nevertheless systematic and should be addressed wherever possible . 
however , since absolute dose calibration of tomotherapy machines is linked to the planning system , the usage of this air value is only advisable if it already has been used during atp of the machine . 
this might not be the case for machines with low serial numbers . fc - 13 strahlenther onkol 2011 ; 187 : 681 the influence of different configurations of leaves on accuracy of leaf opening times s . 
klter1 1university hospital heidelberg , department of radiation oncology , heidelberg , germany purpose : helical tomotherapy is a high precise radiation technique , which scans a target volume with a multiple of beamlets from 360 degrees . 
the accuracy of the mlc for different configurations of leaves was investigated . materials and methods : a calibration procedure with a field width of 2.5cm and a static gantry was generated on the operator station . 
a dynamic sinogram was used to create different constellations of open and closed leaves , which test the impact of friction between neighboured leaves and air pressure used for leaf movement . 
these differences in various configurations of leaves could have an impact on projection times in the range of 20ms , which is the same range as the leaf opening times . 
sanchez rubio1 1hospital universitario puerta de hierro majadahonda , medical physics , madrid , spain helical tomotherapy imrt dose verifications usually involve few absorbed dose measurement points ( as many as available ion chamber ) and a laborious timeconsuming film dosimetry for relative dose distribution comparison . 
the results were evaluated by the absolute and relative dose as gamma function and also compared to routinely measurements with a1sl exradin ion chamber and radiochromic ebt2 fil the dose distributions measured by arccheck array were in good agreements with plans calculated by tomotherapy planning systeusing a 3% 3mm gamma criteria with a 10% value of threshold , the passing rates of diode was > 92% and > 97% for absolute and relative dose distribution respectively . 
sampled doses for representative points from arccheck measured dose distribution were 2% greater than standard ionization measurements ; since there is a good agreement between ion chamber measurement with treatment planning system for homogeneous dose distributions but a systematic discrepancy of - 1.5% for real treatments , it can be considered that the higher spatial resolution of the diodes provides more accurate absorbed dose at a measurement point . 
aim of the study was firstly to evaluate the dose reproducibility for different plans with an increasing level of complexity , secondly to investigate its correlation with the patient anatomy modifications that can occur during fractionated treatments . 
 method : five ht plans , with increased level of complexity , ranked using an extension of the webbs modulation index ( mi ) [ webb s , pmb 2003 ] were initially analyzed . 
these plans were delivered several times and acquired , simultaneously , with the ptw 2d array ( 2d - octavius system ) and the integrated ht mega voltage computed tomography ( mvct ) detectors . 
as second step , four h&n plans , acquired by mvct detectors during clinical treatments delivery , were studied and correlated with patient anatomic variations evaluated by daily mvct imaging . all data sets were analysed with an in - house matlab tool based on the m.s. 
two indices were introduced : the riphan was used to evaluate data acquired with the 2d - octavius system set on the couch and the ritreat for h&n clinical data . 
debus1 1university hospital heidelberg , department of radiation oncology , heidelberg , germany purpose / objective : at the end of 2010 the second tomohd treatment unit worldwide was installed at the university hospital heidelberg . 
before the machine could be used in clinical routine a commissioning of the complete system was performed . besides the classical helical treatment modality the new tomodirect technique is available on all tomohd systems . 
this measuring equipment has proven reliability and accuracy for more than four years on a conventional tomotherapy hiart ii system . for the initial testing of the tomodirect feature simple target volume cofigurations in the cheese phantom were used . 
the treatment plans were then recalculated as dqa plans with different setups of the cheese phantom to test for different aspects of dose calculation like divergency of the beam , depth dose behavoire , missing tissue , influence of the couch or dose summation . additionally , measurements to analyse beam angle accuracy were performed using edr2 films and mvct detector data . 
the relative accuracy of the beam angles was determined using a conventional star shot technique on a transversally orientated filthe absolute orientation of the zero degree beam angle was measured with the detector array , using the tqa step wedge and a variation of beam angles . finally , multiple dqa plans were generated for the first patients and measured with ionization chambers and films in coronal and sagittal orientation . results : the dose measurements with the ionization chambers showed good agreement with the calculated dose . 
only when placing the ion chamber in regions with high dose gradients to measure dose in small organs at risk , deviation larger than 3% were found . conclusion : the modifications on the tomohd system required to deliver and calculate dose with a static beam did not reduce the accuracy of dose delivery . 
10 addendum : tomotherapy 2011 oral presentations miscellaneous fc - 17 strahlenther onkol 2011 ; 187 : 683 the impact of mvct imaging frequency reduction and manual registration suppression on ptv margins : a retrospective analysis on 259 patients treated on helical tomotherapy m . 
georges1 1centre paul strauss , radiotherapy , strasbourg , france purpose / objective ( s ) : it is standard practice that patients treated on helical tomotherapy ( ht ) have daily mvct imaging performed before each treatment fraction . 
these mvct images are compared to the kvct planning images , the registration procedure being automatically performed by software ( automatic deviations ) , then manually corrected by the radiation therapists ( total deviations )  . 
we measured transversal angular ( roll ) , lateral , cranial - caudal and anteroposterior set - up errors of patients treated for different tumor sites to investigate the necessity of the manual registration and the potential reduction of imaging frequency . materials / methods : about 6500 shifts of 259 patients treated with ht were recorded and analyzed : 87 patients treated for head - and - neck tumors with 9 - point fixation thermoplastic masks ( tm ) , 42 and 38 patients treated for abdominal - pelvic tumors respectively with or without vacuum cushions , 23 patients treated for hodgkins disease with 9 - point tm , 13 and 16 patients treated for pulmonary located tumors respectively with 9 - point tm or arm support , and 40 patients treated for brain tumors with 5 - point tm . systematic and random shifts were calculated for the automatic and total deviations on a patient and a population basis . 
furthermore , residual deviations and additional ptv margin were calculated if manual corrections were not applied . five imaging protocols were investigated : every other day , one day out of 3 , the first 3 days followed by once per week , the first five fractions and on an alternate week basis . 
residual deviations obtained by comparing these protocols with daily imaging and the resulting additional ptv margin were then calculated . results : statistically significant differences between automatic and manual deviations are shown for 50 to 80 % of the patients , depending on the tumor site . 
the additional margin that should be applied to ptv if manual corrections were not applied range from 2.5 mm for the brain tumors to 8 mm for pulmonary tumors treated with an arm support . 
the every other day and one day out of 3 give similar results and are the most accurate imaging protocols , involving additional margins to the ptv of 3 mm for head and neck and brain tumors , 5 mm for the pulmonary tumors treated with a 9 - point tm and 8 mm for all the other tumor sites . conclusions : applying no manual corrections after automatic registration or no mvct daily imaging implies a significant increase in the ptv margins . 
the magnitude of this increase depends on the contentions used and treated tumor site . fc - 18 strahlenther onkol 2011 ; 187 : 683 adaptive image - guided tomotherapy concomitant to chemotherapy in rectal cancer : early clinical experience n . 
di muzio1 1san raffaelescientific institute , radiotherapy , milan ; 2san raffaelescientific institute , medical physics , milan ; 3san raffaelescientific institute , radiology , milan , italy purpose : to test the clinical feasibility of adaptive rt concomitant to oxaliplatin ( oxa ) and 5fu c.i. 
concerning the second half of the treatment , more of the 90% ( range : 82.4% - 100% ) of the union was yet contained within a margin of 0.5 cm , while at least 1 cm margin is necessary to obtain the same coverage in the first part of the treatment . 
pathological stage was pcr , pt3n0 , pt4bn0 , pt3n0 , pt2n0 respectively . conclusion : the estimation of rectal volume variations gives the possibility to better guide the irradiation for preoperative treatment . 
in particular the tumour volume reduction and the possibility to decrease the ptv margin in the second half of the treatment could allow an escalation of tumour dose using sib adaptive strategies with reduced margins for the t component of the boost . 
the reduced motion of cranial rectum in the second half suggests also the possibility of adaptive concomitant boost during the last 6 fractions to the whole ptv1 with avoidance of the rectum outside ptv2 and overlap between ptv1 and bowel / bladder . fc - 19 strahlenther onkol 2011 ; 187 : 683 helical tomotherapy in the treatment of anal canal cancer : 3 - year clinical experience h . 
ozsahin1 1department of radiation oncology , centre hospitalieruniversitairevaudois ( chuv ) , lausanne , switzerland objective : to report a single - center experience treating patients with squamous - cell carcinoma of the anal canal using helical tomotherapy ( ht ) and concurrent chemotherapy ( ct )  . materials / methods : from october 2007 to february 2011 , 55 patients were treated with ht and concurrent ct ( 5 - fluorouracil / capecitabin and mitomycin ) for anal squamous - cell carcinoma . 
dose - volume histograms of several organs at risk ( oar ; bladder , small intestine , rectum , femoral heads , penile bulb , external genitalia ) were assessed in terms of conformal avoidance . 
for dosimetric comparisons , 3d rt and / or imrt plans were also computed for some of the patients using the cms planning system , for treatment with 6 - 18 mv photons and / or electrons with suitable energies from a siemens primus linear accelerator equipped with a multileaf collimator.locoregional control and survival curves were compared with the log - rank test , and multivariate analysis by the cox model . 
 results : with 360 - degree - of - freedom beam projection , ht has an advantage over other rt techniques ( 3d or 5 - field step - and - shot imrt )  . 
there is significant improvement over 3d or 5 - field imrt plans in terms of dose conformity around the ptv , and dose gradients are steeper outside the target volume , resulting in reduced doses to oars . 
using ht , acute toxicity was acceptable , and seemed to be better than historical standards . conclusions : our results suggest that ht combined with concurrent ct for anal cancer is effective and tolerable . 
the v15 of the small bowel was 145 , 90cc ( sd75 , 94cc ) and 112 , 71cc ( sd73 , 43cc ) , for hybridarc and tomotherapy , respectively . 
furthermore , hybridarc , using one single enhanced dynamic conformal arc and 6 discrete imrt beams , can achieve equivalent treatment plans ( ptv coverage and organ at risk sparing ) than the tomotherapy . fc - 22 strahlenther onkol 2011 ; 187 : 684 feasibilty of image - guided total marrow irradiation using helical tomotherapy t . 
de ridder1 1uz brussel , radiotherapy , brussel , belgium background and purpose : investigation of the technical feasibility and dosimetry of image - guided total marrow irradiation using helical tomotherapy in the treatment of relapsed multiple myeloma patients . 
dose in the junction region between upper and lower body plans was verified with edr2 film for both techniques . results : it is possible to create clinically acceptable plans for the upper body with tomotherapy . 
geinitz1 1klinikum rechts der isar tum , mnchen , klinik und poliklinik fr strahlentherapie und radiologische onkologie , mnchen , germany purpose : due to better overall survivor of the patients who are treated with csi in acurative intention the late toxicity issues tend to gain further importance . 
we therefore compared the doses at several risk organs ( oars ) in craniospinal irradiation using conventional radiation therapy and tomotherapy . patients and methods : nine patients who have undergone craniospinal irradiation ( csi ) with tomotheraphy at our institution in recent years due to various diseases were evaluated . 
additional oars were contured : inner ear , lenses , oral cavity , thyroid gland , pharynx , larynx , esophaghus , bowel , heart , lungs , kidneys , liver as well as autochtonous back musculature and male and female reproductive organs . 
we compared the v5 , v20 , v30 , v40 , v50 ( volumes of oar that received = 5 , 20 , 30 , 40 and 50 gy , respectively ) as well as the mean , median , maximum and minimum dose . 
for the evaluation of ptv homogenity ( hi ) as well as conformity ( ci ) indeces were calculated . results : as expected a larger body volume ( v5 ) was irradiated using tomotherapy . 
tomotherapy plans had better hi and ci and a better 95% - isodose ptv - coverage . conclusion : our study showed that tomotherapyresulted in better ptv - coverage and better sparing of the lenses , liver , bowel , parotis glands , lungs , heart and dorsal musculature . 
clinical studies on csi survivors should be undertaken to evaluate long term organ toxicity and the risk of second malignancies . fc - 21 strahlenther onkol 2011 ; 187 : 684 feasibility study of using the hybridarc treatment technique for preoperative irradiation of rectal cancer : comparison of dose patterns in lesion and organ at risk with the tomotherapy t . 
de ridder1 1uz brussel , radiotherapy , brussel , belgium purpose : hybridarc is a novel treatment technique blending aperture - enhanced dynamic conformal arcs with discrete imrt beams , allowing selection of dynamic arcs with a set of static imrt beams at specified intervals along each arc . 
 the aim was to evaluate the new technique with regard to achievable plan quality and treatment efficiency and to compare hybridarc against the well establish imrt treatment technique , tomotherapy , for the preoperative treatment of rectal cancer . material and methods : twelve patients treated with tomotherapy were considered and simulated with hybridarc . 
 planning objectives were to give at least 95% of the prescribed dose to 95% of the ptvs while keeping irradiated volumes of the organs at risk ( small bowel and bladder ) as low as possible . 
10 addendum : tomotherapy 2011 oral presentations fc - 23 strahlenther onkol 2011 ; 187 : 685 radiotherapy for women with stage ii supradiaphragmatic hodgkins disease : a dosimetric comparison of imrt by helical tomotherapy and a 3d - conformal radiotherapy ( 3d - crt ) d . 
noel1 1centre de lutte contre le cancer paul strauss , radiotherapy , strasbourg ; 2hpital de hautepierre , hematology , strasbourg ; 3centre de lutte contre le cancer paul strauss , nuclear medicine , strasbourg , france purpose long - term survival rate has reached more than 80% for patients with hodgkins disease . 
the adjuvant radiation treatment delivered a dose of 30gy in sites initially invaded with a complement of 6gy on those suspect of not sterilization observed on ct - scan simulation . 
the delineation of target volumes has been achieved on a simulation ct - scan made after chemotherapy using images fusion with a first simulation ct - scan and 18fdgpet performed in treatment position at the diagnosis . 
as expected , the volumes receiving the highest dose were lower with imrt , we observed a crossing of mean dvh at 19 , 13 and 16gy , respectively for right , left breast and breasts . 
ozsahin1 1department of radiation oncology , centre hospitalieruniversitairevaudois ( chuv ) , , lausanne , switzerland implement a carotid sparing protocol using helical objective : to tomotherapy ( ht ) in t1n0 squamous - cell laryngeal carcinoma . materials / methods : between july and august 2010 , 7 men with stage t1n0 laryngeal carcinoma were included in this study . 
a simple treatment planning algorithm for carotidsparing was used : maximum point dose to the carotids 35 gy , to the spinal cord 30 gy , and 100% ptv volume to becovered with 95% of the prescribed dose . 
carotid volume of interest extended to 1 cm above and below of the ptv.doses to the carotid arteries , critical organs , and planned target volume ( ptv ) with our standard laryngealirradiation protocol was compared . 
when necessary , theplanned adaptive software ( tomotherapy inc . , madison , wi ) was used to evaluate the need for a re - planning , which has never been indicated . 
early local control rate is 100% considering a 4 - 5months post treatment follow - up . conclusions : ht allows a clinically significant decrease of carotid irradiation dose compared tostandard irradiation protocols with an acceptable spinal cord dose tradeoff . 
further investigations and follow - up are underway to better evaluatethe late clinical outcomes especially the local control rate , late laryngeal and vascular toxicity , and expected potentialimpact on cerebrovascular events . fc - 25 strahlenther onkol 2011 ; 187 : 685 localization and quantification of delivered dose to the spinal cord during daily igrt h . 
duma1 1tu mnchen , klinikum rechts der isar , department of radiation oncology , mnchen ; 2klinikum rechts der isar der tu mnchen , klinik und poliklinik fr strahlentherapie und radiologische onkologie , mnchen ; 3tu mnchen , klinikum rechts der isar , institute of medical statistics and epidemiology , mnchen , germany purpose : in the presence of inhomogeneous dose distributions the spinal cord tolerance of relatively small volumes is strongly affected by low - dose irradiation of adjacent tissue . 
 the pct - dmax was localized for this patient on the slices 19 and 20 , right - sided ( grey underlined in the table )  . available about the localization of actual delivered doses to the spinal cord in humans . 
which quadrants ( anterior right , anterior left , posterior right , posterior left ) of the spinal cord received a higher dose than the pct - dmax ; 3 . 
for all patients the increase involved mainly the two anterior quadrants : anterior right and anterior lethe quadrants which received a higher dose than the expected pct - dmax did not overlap with the quadrants where the pct - dmax was located . 
thus , in radiotherapy plans that go as high as the known tolerance doses of the spinal cord a recalculation of dose on the mvct can be useful in order to predict the localization and magnitude of the changes in dmax . 
vermorken5 1university radiotherapy department antwerp , radiotherapy , duffel , belgium ; 2nki - avl , radiotherapy , amsterdam , netherland ; 3leuvens kankerinstituut , radiotherapy , leuven , belgium ; 4university radiotherapy department antwerp , radiotherapy , antwerp , belgium ; 5antwerp university hospital , oncology , edegem , belgium purpose : this study aims to compare standard step and shoot ( ss ) imrt , sliding window ( sw ) imrt , rapidarc ( ra ) volumetric modulated arc therapy ( vmat ) , smartarc ( sa ) vmat and helical tomotherapy ( ht ) for oropharyngeal cancer . 
it is not clear which imrt technique is superior in the treatment of head and neck cancer ( hnc ) patients in terms of coverage of the ptv , sparing the organs at risk ( oars ) , dose to the normal tissue , number of monitor units and delivery time . material and methods : target volumes and oars of five patients with oropharyngeal cancer were fully delineated on ct , after which an individual treatment plan was made on five different planning systems : a ss and a sa plan on pinnacle ; a sw and a ra plan on eclipse ; and a ht plan on tomohdtm . 
with a simultaneous integrated boost technique , a dose of 69.12 gy ( 2 , 16 gy / fraction ) in 32 fractions has been planned to the ptv of the gtv + 1cm and a dose of 56 gy ( 1.75 gy / fraction ) to the ptv of the remaining primary tumour region and the bilateral elective lymph node regions . 
for the ptvs we analyzed the homogeneity index ( hi ) the conformity index ( ci ) , the mean dose , the dnear - max ( d2 ) and the dnear - min ( d98 )  . 
mean dose to the remaining volume at risk is not higher with the rotational techniques , nor is the mean dose to the body ptv ! an extensive list of mean doses and organ specific critical doses and volumes is given . 
however , this sparing seems to require extra beam - on time and its clinical relevance remains to be proven . fc - 28 strahlenther onkol 2011 ; 187 : 687 tomotherapy in head and neck cancer : mind each gland fc - 27 strahlenther onkol 2011 ; 187 : 687 simultaneous integrated boost ( sib ) and simultaneous modulated accelerated radiation therapy ( smart ) for head & neck cancer patients using helical tomotherapy : experience of centre oscar lambret l . 
lartigau1 1centre oscar lambret , university department of radiotherapy , lille , france background : our aim was to evaluate the feasibility and efficacy of intensitymodulated radiation therapy ( imrt ) with simultaneous integrated boost ( sib ) or simultaneous modulated accelerated radiation therapy techniques for head & neck cancer patients treated with helical tomotherapy ( ht - imrt )  . methods and materials : between january 2009 and december 2010 , 145 patients underwent ht - imrt for head and neck tumours at the university department of radiotherapy , centre oscar lambret , lille ( france )  . 
there were 37 females and 114 males , with a mean age of 58 ( range 22 - 85 )  . the disease was stage ii in 5% of patients , stage iii in 20% , and stage iva in 75% . 
after this time of follow - up , 90% of patients were alive , and the disease - free survival rate between these advanced stage head & neck cancer patients was 68 , 25% . 
helical tomotherapy plans were homogeneous , with a median homogeneity index of 1.05 ( range , 0 , 8 1.2 ) for the high dose volume . conclusion : ht - imrt with sib and smart techniques for locoregionally advanced head & neck carcinomas was feasible and effective regarding early locoregional control and development of xerostomia . 
tribius1 1university medical center hamburgeppendorf , department of radiation oncology , hamburg ; 2university medical center hamburgeppendorf , martini - clinic prostate cancer center , hamburg ; 3university medical center hamburgeppendorf , department of medical physics , hamburg ; 4university medical center hamburgeppendorf , department of otolaryngology and head and neck surgery , hamburg , germany background radiation ( rt ) - induced xerostomia can have immediate and late functional and psychological impact on patients . 
helical tomotherapy ( ht ) is a ct - directed platform for delivering imrt that aims to deliver the lowest doses to the parotids and other organs at risk ( oar ) and achieve the shortest treatment time . 
 study aim : to assess the rate and severity of xerostomia resulting from rt low dose to the left and right ( l + r ) , low dose to the l or r , or high dose to the l + r parotid . methods : patients with locally advanced hnc treated with curative intent were eligible . 
oar were defined during treatment planning and prioritized in the planning algorithrt dose to the parotids was evaluated without compromising homogeneous coverage of the planning tumor volume 1 ( tumor site , primary neck nodes , supraclavicular region )  . 
anova test was performed for comparison of numerical variables . results : to date , the analysis set consists of 95 patients who had ht with information regarding xerostomia , 58 in group a , 29 in group b and 7 in group c . 
the currently small number of patients in group c ( n = 7 ) may be a confounding factor . conclusions : these data using tomotherapy show that the rate and severity of xerostomia is substantially reduced in patients who receive an rt dose < 26 gy to both the l + r parotids . 
10 addendum : tomotherapy 2011 oral presentations breast , gynecology fc - 29 strahlenther onkol 2011 ; 187 : 688 the potential role of preoperative helical tomotherapy in locally advanced breast tumors c . 
fourquet1 1institut curie , department of radiation oncology , paris ; 2institut curie , department of medical physics , paris , france purpose / objective ( s ) : locally advanced breast cancer ( bc ) not eligible for upfront radical surgery remains a challenging situation for oncologists and surgeons , both in a non - metastatic as well as in some metastatic settings ( responsive or stable systemic disease )  . 
this is a small series of patients ( pts ) treated with preoperative helical tomotherapy ( ht ) followed by radical surgery . materials / methods : five pts with locally advanced not operable bc received neoadjuvant chemotherapy ( nct ) followed by preoperative helical tomotherapy . 
irradiated volumes included : whole breast ( wb ) in all pts , axillary lymph nodes ( aln ) in 2 pts , internal mammary lymph nodes ( imln ) in 2 pts , supraclavicular ( scv ) and infraclavicular fossa ( icv ) in 3 pts . 
for the latter , the whole breast and gtv were prescribed 50gy in 25fx ( 2gy / fx ) and 55 gy in 25 fx ( 2.2gy / fx ) , respectively . 
pathological response is summarized in the table . conclusions : ht offers several advantages in locally advanced bc : a homogenous irradiation throughout all target volumes , lung and heart sparing and the possibility of a simultaneous integrated boost to gtv disease . 
these results need confirmation in the setting of a clinical trial . fc - 30 strahlenther onkol 2011 ; 187 : 688 tomotherapy versus topotherapy in breast cancer patients : experience of grupo imo ( madrid , spain ) g . 
marsiglia1 1instituto madrileo de oncologa ( imo ) , radiotherapy , madrid , spain introduction : radiation therapy in the context of breast conserving therapy , for early breast cancer is since 2005 one of the most validated procedures in oncology . 
the ebctcg showed that rt after breast conserving surgery in n ( - ) was associated with a ten year rate of local recurrence absolute reduction of 17 , 9% and a 3 , 6% in the 15 year rate of breast cancer mortality . 
radiotherapy has been associated with late cardiac mortality , lung toxicity and skin morbidity ( due to the volume of these organs that receive a high radiation dose with conventional treatments )  . 
28 were treated with tomotherapy and 21 with tomodirect , with different fractionations schedules ( 29 patients with fractions of 200 cgy and integrated boost , nine with standard whole breast irradiation without boost , 10 were treated with whole breast hypofractionation and one with accelerated partial breast irradiation [ apbi ] )  . 
 results : ptv average homogeneity index was similar with tomodirect and tomotherapy ( 1 , 08 for standard treatment , 1 , 09 for hypofractionation and 1 , 06 for apbi )  . 
results will be update at september / 2011 . conclusion : tomodirect is a technique capable of delivering a high homogeneity index and well tolerated treatment in early breast cancer patients . 
tomotherapy is , in our experience , an optimal treatment in patients candidates to whole breast hypofractionation and apbi , as it minimizes the median heart , lung , and contralateral breast dose . 
although further studies are required to evaluate local control , survival and late toxicity . fc - 31 strahlenther onkol 2011 ; 187 : 688 tomo vs vmat vs tangential fields to reduce cardiovascular complications in breast cancer therapy a . 
polico1 1irst , medical physics , meldola ; 2irst , radiotherapy , meldola , italy background : despite the current perception that breast cancer is the main reason for mortality in women affected by this disease , there is evidence to suggest that cardiovascular disease is the main cause of death of left breast cancer carriers . 
 coverage of the left breast and the dose volume histogram ( dvh ) of the myocardium , the left anterior descending coronary artery , the diagonal arteries , the right breast , and the left lung are considered . materials and methods : a patient , suffering from infiltrating ductal carcinoma and cardiopathy underwent conservative surgery and adjuvant chemotherapy , and was sent to our department for adjuvant radiotherapy . 
this is because it adequately covers the target , and at the same time allows an optimal myocardium , coronary artery and right breast sparing . fc - 32 strahlenther onkol 2011 ; 187 : 689 helical tomotherapy and breast cancer : skin toxicity of the first 85 breast cancer patients treated with tomotherapy m . 
herfarth1 1university hospital heidelberg , radiation oncology , heidelberg , germany purpose : in breast cancer treatment the target volume extends up to the air - toskin transition and is moved by breathing motion . 
the purpose of this study is to evaluate if the skin toxicity is accordant to this data . methods and materials : from july 2006 to february 2011 a total of 85 patients with indication for adjuvant irradiation of the whole breast or chest wall ( + / lymph nodes ) after surgery were treated using helical tomotherapy . 
the skin toxicity was evaluated utilizing the grading developed by the radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc )  . 
these results led to a further confirmation of our published data with homogenous and reproducible surface doses in patients with breast cancer who were treated with ht . fc - 33 strahlenther onkol 2011 ; 187 : 689 a planning study to compare tomodirect and helical tomotherapy for delivering simultaneous integrated boosts to the breast within the import - high radiotherapy trial s . 
manktelow1 1addenbrookes hospital cambridge , radiotherapy physics , cambridge , united kingdom purpose : to compare two different tomotherapy techniques for delivering simultaneous integrated boost radiotherapy to the breast , considering target dose coverage , organ at risk doses and planning and treatment times . method : nine computed tomography data sets for patients undergoing breast conservation surgery wereavailable froma mulitcentre planning study for the uk intensity modulated and partial organ ( import ) high trial.the tumour bed , partial breast andwhole breast ptvs had been outlined to allow delivery ofa three level radiation dose distribution to the breast in accordance with test arm 2 of the import high trial ; 53gy / 15# to the tumour bed ptv , 40gy / 15# to the partial breast ptvand 36gy / 15# to the whole breast ptv . 
 an alternative planning solution using tomodirect on version 4 of the planning software is currentlybeing investigatedusing the same nine datasets for comparison . results : helical tomotherapy technique : plans for each of thenine patient data sets were completed for the helical delivery technique.all ptv dose - volume constraintsand organ at risk dose constraints weresatisfied in all nine cases . 
average dose - volume statistics for all nine patientsare summarised in tables 3 and 4 for the ptv and organs at risk volumesrespectively . table 1 : ptv dose - volume constraints forimport high trial test arm 2 . ( wb = whole breast , pb = partial breast , tb = tumour bed )  . table 2 : organ at risk dose constraints strahlenther onkol 2011 no . 
10 addendum : tomotherapy 2011 oral presentations table 3 : ptv dose - volume statisticsusing ahelical delivery technique table 4 : organ at risk doses using a helical delivery technique tomodirect technique : atomodirect planning solution is currently being investigated.multiple solutionsusing two or more fixed gantry anglesare beingcompared and applied to the nine datasetsto identifyan optimum beam arrangement , balancing both targetcoverage and planning anddelivery times.we hypothesise that trial constraints will still be met for the target volumes , although potentially with a reduction in conformality . 
we hypothesise also that organ at risk doses , particularly for both lungs , will bereduced compared tothe helical technique , with the added advantage of shorter planning and delivery times . conclusions : helical tomotherapy provides a satisfactory solution for simultaneous integrated boost radiotherapy to the breast , although planning and delivery times are long . 
tomodirect may provide a faster solutionwith a possible reduction in treatment timeandlung dose . new developments fc - 34 strahlenther onkol 2011 ; 187 : 690 evaluation of a dose delivery verification system for in - vivo dosimetry in helical tomotherapy c . 
mazal1 1institut curie , medical physics , paris ; 2institut curie , medical physics , saint - cloud france in - vivo dosimetry checks the absorbed dose distribution delivered to the patient as a part of the quality assurance of the treatment . 
 tests of increasing complexity were created in order to evaluate its accuracy and sensitivity to detect both patient positioning or machine parameters variation that can occur during a fraction of a treatment . materials and method : tomotherapy has developed a dose verification system which allows in - vivo daily dosimetry quality control in several points of the patient volume . this system first determines each mlc leaf open time and then computes the delivered dose , using different data : the pulse by pulse signal collected by the onboard mvct exit detector , the machine output collected by the monitor chamber and attenuation data stored as a function of the beam radiological pathlength . the first part of our study consists of an evaluation of the dose reconstruction calculation accuracy . 
three test levels of increasing complexity were created , from the irradiation of a homogeneous cylindrical phantom to a head - and - neck rando phantom planned using the head - and - neck clinical protocol implemented in our institute . 
for level 3 , dose distributions using kodak edr2 films were compared to calculations . the second part verifies the ability of the system to detect errors that can occur during a treatment . 
thus , on one hand , using a deformed phantom and applying misalignment on a rigid phantom , variations correlated to patient were simulated and compared to ionization chamber measurements . 
 results / conclusion : accuracy of the dose reconstruction calculation was found to be within 6 % and 4mm in areas of low and high dose gradient respectively , for the three test levels . 
 the dose reconstruction system shows good sensitivity to the different tests of misalignment , deformation or machine parameters variations . patient exit detector data is being currently collected during selected treatments to fully validate the system before clinical implementation . fc - 35 strahlenther onkol 2011 ; 187 : 690 from hiart to hdtm , is it worth the effort ? d . 
de ost1 1university radiotherapy department antwerp , radiotherapy - tomotherapy , antwerp , belgium objective : to compare the planning process and the patient throughput between tomohdtm and tomotherapy hiart . materials and methods : in december 2010 , a tomohd machine with new software ( version hd1.0 ) on a 14 - blade computing server have been installed at our department . 
a comparative end - to - end test between tomohd and the parallel hiart system has been run on a phantotherefore , a helical hiart , a helical hd and a direct hd plan were made with the same constraints . 
the performance of the hd1.0 software is higher and the hd machine allows a fluent and faster treatment . fc - 36 strahlenther onkol 2011 ; 187 : 690 the next generation of tomotherapy : dynamic jaws and dynamic couch f . 
debus2 1university of heidelberg , radiation oncology , heidelberg ; 2university hospital heidelberg , radiation oncology , heidelberg , germany purpose : current helical tomotherapy has a couple of moving components , but field width and couch motion are constant during treatment . 
this report presents a series of planning studies to investigate plan quality and application speed of this new technique . methods and materials : a planning comparison was conducted for 10 patients with arteriovenous malformations for radiosurgery , 10 patients with sbrt , 15 patients with large volume irradiation ( tmi , hemithoracic and whole abdominal ) , 3 patients with multitarget treatments and 10 patients with nasopharyngeal cancer . 
treatment time , target coverage , dose to organs at risk and integral dose was evaluated . results : application time for the new technique could be reduced by 48 - 72% to regular delivery . 
axial mode with static couch offered the fastest treatments but produced severe underdosage at upper and lower target edge and yielded inferior conformity due to a restriction to cylindrical shape . conclusions : the new technology with dynamic jaw and couch movements improves the plan quality by reducing the dose penumbra and thereby reducing the integral dose . 
there are considerable limitations for small volume irradiations in tomotherapy in the current and future version . fc - 37 strahlenther onkol 2011 ; 187 : 691 on the dosimetric challenges of dynamic jaws tomotherapy : a monte carlo study e . 
vynckier4 1universit catholique de louvain , molecular imaging , radiotherapy and oncology , brussels , belgium ; 2tomotherapy , madison , usa ; 3university of wisconsin , medical physics , madison , usa ; 4universit catholique de louvain , brussels , belgium purpose : in its present configuration , tomotherapy uses three fixed different field widths ( 5 , 2.5 and 1 cm ) , limiting the control of the longitudinal modulation . 
the model was first used to compute dose / fw in a water phantom for a 10 cm x fw beam scanned to deliver a 10 x 10 cm2 field , normalized to the dose / 5 cm obtained for a same field but with a 10x5 cm beam ( fw is the light - projected beam width )  . 
a quality assurance check of the convolution / superposition ( c / s ) calculation was previously performed in the assymetric mode with an edr - 2 film according to manufacturer recommendations . 
this would allow using conservatively c / s as the reference in this simple case to validate tomopen in a first approach . results : for the source centred , the loss of output for small fws is due to source occlusion by the jaws . 
the further drop for 0.3 and 1 mm offaxis sources , more than 30% for the latter and the smallest field ( 0.2 cm ) , demonstrate the importance of quality assurance . 
0.3 mm is the tolerance allowed by tomotherapy.in the dynamic jaws mode , tomopen simulations were compared to c / s with an excellent agreement within 2% / 2mm , as illustrated in the figure embedded in this abstract ( asymmetric case only )  . conclusions : the new version of tomopen showed its ability to compute dynamic jaws - couch tomotherapy treatments . 
10 addendum : tomotherapy 2011 poster presentations poster presentations strahlenther onkol 2011 ; 187 : 692 igrt - ct equals igrt - ct ? a subjective and objective comparison of helical mvct to kvcbct m . 
geinitz1 1tu mnchen , klinikum rechts der isar , department of radiation oncology , mnchen , germany purpose : to assess objective and subjective differences between two different computer tomographies ( cts ) employed for igrt ( igrt - ct )  . 
the two cts that were compared were the helical mega - voltage ct ( mvct ) of tomotherapy and the kilo - voltage cone beam ct ( kvcbct ) of varian trilogy . methods and materials : patients with prostate ( pr ) or with head and neck ( h&n ) cancers were evaluated . 
for h&n a 1 cm square region in the centre of the 3rd cervical vertebral body and a 1 cm square region in the dorsal neck - muscles were evaluated . the questionnaires evaluated the handling of the igrt - ct , the performing of the registration of the igrt - ct to the planning - ct ( p - ct ) , the presence of artifacts , the identifiability of regions of interest [ roi ] ( i.e bladder , rectum and prostate ; parotid glands , spinal cord and ptv )  . the staff - member , who performed the online fusion of the igrt - ct to the p - ct , was asked to evaluate the process on a scale from 1 to 6 . 
german school notes were assigned ( from 1 - very good to 6 - bad )  . results : very large differences were observed from one kvcbct to another for the same tissue ( bones : range - 369hu to 1159hu ; muscles : - 74hu to 276 hu )  . 
1 depicts the measured values of the average hu for both igrt - cts and the pc - t for each patient individually . conclusion : the mvct is more stable with regard to the measured hus . 
bak4 1department of electroradiology , university of medical sciences and department of medical physics , greater poland cancer centre , poznan ; 2department of electroradiology , university of medical sciences and 2nd radiotherapy department , greater poland cancer centre , poznan ; 3department of medical physics , greater poland cancer centre , poznan ; 42nd radiotherapy department , greater poland cancer centre , poznan , poland aim : one of the technical challenges of head and neck ( han ) radiotherapy is to accurately determine the geometrical uncertainties since these have a significant impact on target coverage and organs at risk ( oars ) sparing . 
 additionally , the impact of geometrical uncertainties of the sc on the doses received in it was analysed . material and methods : data from 25 patients treated for han cancers were used . 
625 sets of the mvct scans were used in analysis . displacements were analysed in a sc region from c1 to th2 and in a sub - regions divided to three parts : c1 - c3 , c4 - c6 and c7 - th2 . 
generally , the highest increasing of the displacement were observed during first and third week of the treatment and it was depended , respectively , from stabilization of the patient position and weight lost effect . 
for first week the highest increasing effect , in second decreasing effect and in a next three weeks slow but long - term increasing effect were detected . analysis of the fraction dose showed small increase of the d ( v1 ) ( mean dose received in 1% of the sc )  . 
the strongest influence on the differences of the planned and delivered doses was detected for a displacement vector , and then for a region of a sc and finally for a weight loss effect . 
however the highest impact on the differences between planned and delivered fraction doses was detected during third week of irradiation for a c4 - c6 region and displacements from 1.5 mm to 2 mdifferences between planned and fig1 . : the median differences between the pct and the kvcbct were for bones 300130 hu and for muscles 2560 hu . 
 for all igrt - cts altogether the handling of the igrt - ct ( in 97% of the analyzed fractions ) , the performing of the registration of the igrt - ct to the p - ct ( in 88% of the analyzed fractions ) , the presence of artifacts ( in 85% of the analyzed fractions ) were graded with very good or good . 
the head and neck mvcts were graded for all rois ( parotid glands : 3 ; spinal cord : 2 and ptv : 2 ) one grade worse than the kvcbct . 
fraction dose summation based on changes of the anathomy provide more accurate results than simple rigid summation . strahlenther onkol 2011 ; 187 : 693 helical tomotherapy for soft tissue sarcoma of the thigh : preliminary results c . 
helfre1 1institut curie , radiotherapie , paris , france purpose : to report feasibility and preliminary clinical results of helical tomotherapy ( ht ) for adjuvant treatment in primary soft tissue sarcoma of the thigh . methods and materials : ten consecutive patients between january 2007 and july 2010 were treated in our institution for primary soft tissue sarcoma of the thigh with ht . 
no patient developed bone fracture . conclusion : helical tomotherapy provides excellent ptv coverage for large soft tissue sarcoma of the thigh and minimizes the dose to femur , skin and muscular tissue . 
long term follow - up is needed to confirm these preliminary results . tomotherapy , soft tissue sarcoma of thigh , treatment planning , toxicity . strahlenther onkol 2011 ; 187 : 693 the effect of tumor motion on dose distributions of pulmonary stereotactic body radiotherapy treatments performed with tomotherapy t . 
koch1 1sozialstiftung bamberg mvz am bruderwald , praxis fr strahlentherapie und radioonkologie , bamberg , germany purpose : to investigate the effect of tumor motion due to breathing on the dose distribution in pulmonary stereotactic body radiotherapy ( sbrt )  . methods and materials : for our measurements we used an inhomogeneous cirs - thorax - phantom with some self - made modifications . 
to simulate the tumor we used a cylinder - shaped rod ( 2.5cm diameter and 3cm long ) with water density which was placed inside one lobe of the phantom lung . 
for the sine - like motion , the most probable tumor position is the middle position and for cosine6 - like motion we detected a shift from the middle position . 
as a further result we have seen , that the blurring of the dose distribution with tomotherapy is less pronounced as compared to the dose distribution seen with the linac treatment . 
for larger motion amplitudes ( > 1.5cm or greater than one half of the tumor diameter in motion direction ) the blurring effect is too high , even for tomotherapy . 
in these cases gating , tracking or immobilization of the tumor is necessary . strahlenther onkol 2011 ; 187 : 693 peripheral doses in prostate treatment with tomotherapy : measurements versus monte carlo modelling e . 
sterpin3 1belgian nuclear research center , radioprotection dosimetry and calibration , mol ; 2university hospital uzbrussel , radiotherapy , brussel ; 3saint luc hospital , radiotherapy , brussels , belgium introduction : some of the patients cured with radiotherapy , could later develop a treatment induced secondary malignancy in organs located at a distance from the original tumor . 
it is therefore relevant to establish the doses that are absorbed in those distant organs , or peripheral doses [ 1 , 2 ]  . materials and methods : in this study we compared peripheral doses during aprostate treatment , delivered with a tomotherapy unit , versus monte carlo ( mc ) calculated doses . 
this study investigated potential prognostic factors , including hpv status , for locoregional control ( lrc ) , metastases - free survival ( mfs ) , and survival ( os )  . 
prert hemoglobin 12 g / dl ( rr1.98 ; p = 0.040 ) and t category t1t2 ( rr 3.33 ; p < 0.001 ) were significantly associated with improved mfs . 
positive hpv status ( rr 2.19 ; p = 0.019 ) , pre - rt hemoglobin 12g / dl ( rr2.15 ; p = 0.002 ) , t category t1t2 ( rr2.31 ; p = 0.002 ) , and ajcc stageiii ( rr1.91 ; p = 0.034 ) were significantly associated with improved os . conclusion : improved treatment outcomes were significantly associated with positive hpv status , better performance status , lower tumor stage , and pretreatment hemoglobin levels 12g / dl . 
these factors should be considered in future trials . key words : head and neck cancer radiotherapy prognostic factors hpv status treatment outcome strahlenther onkol 2011 ; 187 : 62632 doi 10.1007 / s00066 - 011 - 1139 - 8 prognosefaktoren ( inklusive hpv - status ) bei der bestrahlung lokal fortgeschrittener plattenepithelkarzinome im kopf - hals - bereich ( scchn ) hintergrund : die prognose von patienten mit lokal fortgeschrittenem plattenepithelkarzinom im kopf - hals - bereich ( scchn ) ist hufig schlecht . 
 diese studie untersuchte mgliche prognosefaktoren inklusive hpv - status fr die lokoregionale kontrolle ( lrc ) , das metastasenfreie berleben ( mfs ) und das gesamtberleben ( os )  . material und methode : zwlf mgliche prognosefaktoren wurden in einer serie von 170 patienten , die aufgrund eines scchn im stadium iii oder iv eine strahlentherapie erhielten , untersucht . 
diese faktoren waren alter ( 60 vs > 60jahre ) , geschlecht , allgemeinzustand ( ecog 01 vs 2 ) , hmoglobinwert vor strahlentherapie ( < 12 vs 12g / dl ) , tumorlokalisation ( oropharynx , mundhhle , hypopharynx , larynx ) , grading ( g12 vs g3 ) , t - kategorie ( t1t2 vs t3t4 ) , n - kategorie ( n0n1 vs n2n3 ) , ajccstadium ( iii vs iv ) , operation ( nein vs ja ) und chemotherapie ( nein vs ja )  . ergebnisse : in der multivariaten analyse waren ein positiver hpv - status ( rr 2 , 34 ; p = 0 , 014 ) , ein besserer allgemeinzustand ( rr 1 , 94 ; p = 0 , 017 ) , hmoglobinwerte 12g / dl ( rr 1 , 88 ; p = 0 , 018 ) , eine niedrigere t - kategorie ( rr 2 , 72 ; p < 0 , 001 ) und eine operation ( rr 2 , 29 ; p = 0 , 007 ) signifikant mit einer besseren lrc assoziiert . 
hmoglobinwerte 12g / dl ( rr 1 , 98 ; p = 0 , 040 ) und eine niedrigere t - kategorie ( rr 3 , 33 ; p < 0 , 001 ) waren signifikant mit einem besseren mfs assoziiert . 
ein positiver hpv - status ( rr 2 , 19 ; p = 0 , 019 ) , hmoglobinwerte 12g / dl ( rr 2 , 15 ; p = 0 , 002 ) , eine niedrigere t - kategorie ( rr 2 , 31 ; p = 0 , 002 ) und ajcc - stadiumiii ( rr 1 , 91 ; p = 0 , 034 ) waren signifikant mit einem besseren os assoziiert . 1department of radiation oncology , university of lubeck , lubeck , germany , 2institute of pathology , university of lubeck , lubeck , germany , 3department of radiation oncology , mayo clinic scottsdale , scottsdale , az , usa . received : june 7 , 2011 ; accepted : june 14 , 2011 published online : september 19 , 2011 strahlenther onkol 2011 no . 
prognostic factors for locally advanced scchn schlussfolgerungen : eine verbesserung der behandlungsergebnisse war signifikant mit positivem hpv - status , besserem allgemeinzustand , niedrigerem tumorstadium und hmoglobinwerten 12 g / dl vor therapie assoziiert . 
patientencharakteristika. entire cohort ( n = 170 ) n patients ( % ) hpv - positive ( n = 40 ) n patients ( % ) hpv - negative ( n = 130 ) n patients ( % ) p value introduction treatment options for locally advanced scchn have improved during recent decades , in particular with the introduction of high - precision radiotherapy techniques , new systemic agents , and less invasive surgical approaches [ 4 , 6 , 8 , 11 , 13 , 21 , 24 , 27 , 29 ]  . 
these results suggest an increased radiation sensitivity of hpv - positive tumors , although this concept is still controversial [ 9 ]  . age 60 years > 60 years gender female male ecog performance score 01 2 hemoglobin level pre - rt < 12 g / dl 12 g / dl tumor site oropharynx oral cavity hypopharynx larynx histologic grade g12 g3 most studies that investigated the potential role of the hpv status only included patients with oropharynx cancer [ 7 , 10 , 1820 , 23 , 28 ]  . 
the current study investigated 12 potential prognostic factors , including the hpv status for locoregional control ( lrc ) , metastases - free survival ( mfs ) , and overall survival ( os ) , in patients irradiated for locally advanced scchn . 
microscopically residual tumor ( r1 resection ) was present in 24 of 135 ( 18% ) patients including 7 of 32 ( 22% ) patients with hpv - positive tumors and 17 of 103 ( 17% ) patients with hpv - negative tumors . conventionally fractionated radiotherapy with doses per fraction of 2.0gy was administered with a linear accelerator and 46mv photons . 
the dose administered to uninvolved cervical and supraclavicular lymph nodes was 5060gy . a total of 93patients received concurrent chemotherapy that consisted either of 20mg / m2 of cisplatin on days 15 and 2933 ( 44patients ) , or 20mg / m2 of cisplatin plus 600 mg / m2 of 5 - fluorouracil on days 15 and 2933 ( 49patients )  . 
the distribution of the chemotherapy regimen was almost identical ( p = 0.99 ) in patients with hpv - positive tumors ( 48% cisplatin alone , 52% cisplatin / 5 - fluorouracil ) and those with hpv - negative tumors ( 47% cisplatin alone , 53% cisplatin / 5 - fluorouracil )  . 
in nondysplastic epithelium and dysplasia , large amounts of replicated virus episomes are found in the nucleus and easily recognized by using chromogene in situ hybridization ( cish )  . 
therefore , we adapted the morphologic criteria of positive hybridization - signals to the well - known morphology of cish for other genes [ 28 ]  . in addition , p16 immunoreactivity was qualitatively analyzed in accordance with morphologic criteria for p16 as a surstrahlenther onkol 2011 no . 
a tumor was defined as hpv positive , if it showed a specific hybridization result in at least 10% of tumor cells and a specific pattern of immunhistochemical p16 expression . the positive control was a squamos - type carcinoma in situ of the cervix uteri of a patient with known hpv subtype ( hpv - chip type 3.5c , chipron gmbh , berlin , germany )  . 
prognostic factors found significant or of borderline significance ( p < 0.06 ) in the univariate analysis were included in a multivariate analysis , performed with the cox proportional hazards model . results the 5 - year lrc rates were 80% in patients with a hpvpositive tumor and 54% in patients with a hpv - negative tumor ( p = 0.025 , figure 1 )  . 
according to the results , improved lrc was significantly associated with positive hpv status , better performance status , prert hemoglobin level 12 g / dl , and lower t category . 
these findings are consistent with data from the literature . the prognostic value of the performance status and the tumor stage have already been described [ 2 , 3 , 1517 , 25 ]  . 
tumor oxygenation can be affected by the oxygen - carrying capacity of the blood represented by the hemoglobin level [ 1 ]  . one major finding of the present study was the favorable impact of a positive hpv status on treatment outcome . 
 [ 30 ] described in a study of 66patients with oropharynx cancer that the hpv titer was significantly associated with the response to both induction chemotherapy ( one course of either cisplatin plus fluorouracil or carboplatin plus fluorouracil ) and subsequent radiochemotherapy ( 70 gy plus three courses of cisplatin )  . 
 [ 5 ] presented a series of 96patients with stage iii or iv oropharynx cancer who received induction chemotherapy with two courses of paclitaxel and carboplatin followed by radiotherapy plus concurrent weekly paclitaxel . 
 [ 10 ] reported on 198patients with stageiii or iv oropharynx cancer who received either with surgery alone ( n = 14 ) , surgery plus adjuvant radiotherapy ( n = 110 ) or definitive radio ( chemo ) therapy ( n = 71 )  . 
lrc and os were better in patients with a hpv - positive tumor in the surgery plus adjuvant radiotherapy group and the definitive radio ( chemo ) therapy group but not in the surgery alone group . it has been recognized that hpv - positive tumors are sensitive to radiation [ 5 , 9 ]  . 
the question arose whether hpv - positive tumors were associated with an increased radiosensitivity compared to hpv - negative tumors ? an in vitro study compared two naturally infected hpv 16 cell lines ( upci - scc90 and umscc47 ) and hpv - negative scchn cells ( sq20b ) with respect to radiosensitivity . 
it has been suggested that the oncoproteins e6 and e7 , in particular e6 * i , play a role in the enhanced radiosensitivity of hpv - positive oropharynx cancers associated with p53 - independent radiation - induced cell death [ 20 , 26 ]  . conclusion improved treatment outcomes in patients with locally advanced head and neck cancers were significantly associated with positive hpv status , better performance status , lower tumor stage , and pretreatment hemoglobin levels 12 g / dl . 
these factors need to be considered in future trials . original article practically acquired and modified cone - beam computed tomography images for accurate dose calculation in head and neck cancer chih - chung hu1 , 2 , wen - tao huang2 , chiao - ling tsai1 , jian - kuen wu1 , 3 , hsiao - ling chao1 , guo - ming huang1 , chun - wei wang1 , chien - jang wu3 , jason chia - hsien cheng1 , 4 , 5 , 6 background : on - line cone - beam computed tomography ( cbct ) may be used to reconstruct the dose for geometric changes of patients and tumors during radiotherapy course . 
 results : with 360 acquisition of cbct and high - resolution reconstruction , the uniformity of ct number distribution was improved and the otherwise large variations for background and high - density materials were reduced significantly . 
most dosimetric differences were from the setup errors related to the interval changes in body shape and tumor response . conclusion : the specific cbct acquisition , reconstruction , and ct number modification can generate accurate dose calculation for the potential use in adaptive radiotherapy . key words : cone - beam computed tomography linear accelerator dose calculation radiotherapy head and neck cancer strahlenther onkol 2011 ; 187 : 63344 doi 10.1007 / s00066 - 011 - 2247 - 1 routinemig akquirierte und modifizierte cone - beam - ct - bilder zur exakten , adaptiven dosis - berechnung bei kopfund hals - tumoren ziel : die on - line - cone - beam - computertomographie ( cbct ) kann zur anpassung der dosis bei geometrischen nderungen der patientenlagerung und des tumorvolumens whrend der strahlentherapie verwendet werden . 
 ergebnisse : mit der 360 - erfassung des cbct und einer hochaufgelsten rekonstruktion wurden sowohl die bereinstimmung der ct - dichtewerte verbessert als auch die sonst groen abweichungen des hintergrundes und bei dichteren materialien 1division of radiation oncology , department of oncology , national taiwan university hospital and college of medicine , no . 
7 chung - shan south road , taipei 100 , taiwan , 2department of radiological technology , yuanpei university , hsinchu , taiwan , 3institute of electro - optical science and technology , national taiwan normal university , taipei , taiwan , 4graduate institute of oncology , national taiwan university , taipei , taiwan , 5graduate institute of clinical medicine , national taiwan university , taipei , taiwan , 6graduate institute of biomedical electronics and bioinformatics , national taiwan university , taipei , taiwan . received : december 2 , 2010 ; accepted : may 19 , 2011 published online : september 23 , 2011 strahlenther onkol 2011 no . 
the goal of the system was to correct the positioning error . efforts have been made with repeated fan - beam ct ( fbct ) acquisition and re - planning procedures to account for the time - dependent variations during fractionated rt [ 16 , 27 , 28 ]  . 
the smaller pixel size suggests the potential use of cbct for re - planning purposes , including target contouring and dose calculation [ 10 , 11 , 22 ]  . cbct has greater scattering artifacts due to its larger beam - view size than fbct . 
despite the < 1% dose difference between fbct and varians cbct acquired for an inhomogeneous phantom , it becomes unacceptably large when the bowtie filter is not used for acquiring the cbct [ 30 ]  . 
however , the elektas x - ray volume imaging system , as compared to varians system , does not provide a tool for ct number calibration . site - specific dose calibration of cbct has been proposed with different modification requirements [ 6 , 20 ]  . 
the studies have shown the interval changes from weight loss and treatment response in the head and neck region by acquiring fbct or cbct and re - calculating the dose distribution [ 7 , 13 , 15 , 25 ]  . 
to apply elektas cbct images for improved resolution and accurate dose calculation of the head and neck region during the fractionated rt course , we designed an imaging acquiring and processing method to modify the ct numbers of cbct images for various phantoms and two nasopharyngeal cancer patients . 
we verified the agreement of dose distributions between planning fbct and modified cbct with no bowtie filter needed , as well as demonstrated the dose distributions on cbct with the interval changes of treatment responses and body shape from weight loss . patients and methods imaging devices the imaging devices included a siemens somatom emotion system ( siemens , concord , ca , usa ) for fbct and an elekta synergytm x - ray volume imaging system ( elekta oncology system ltd . , crawley , west sussex , uk ) for cbct . 
for different treatment regions , imaging settings of the small - collimator mode ( s mode ) and medium - collimator mode ( m mode ) were used to obtain different fields of view ( fovs )  . 
a specific mode for quality assurance ( qa mode ) was established by the manufacturer with the small collimator and full - rotation scanning settings using higher exposure factors to obtain premium quality images through a high - resolution reconstructive process . 
catphan - 503 consists of several types of sub - phantoms , with three of them ( ctp - 486 , ctp - 528 , and ctp - 401 ) used in this study . 
eight kinds of materials of different densities ( 0.1951.609 g / ml ) were imbedded into cirs - 062 . a shaped tumor in the head and neck region of a rando phantom was created and treated with an artificial intensitymodulated rt ( imrt ) plan . 
finally , the cbct images acquired in weeks 1 and 6 of imrt of a second nasopharyngeal cancer patient were also tested . imaging processing and analysis the profiles along the x - axis and y - axis of the ctp - 486 phantom for the uniformity test on fbct showed variations of ct numbers around 10 . 
the ct numbers ( mean standard deviation ) for fbct , s mode cbct , and m mode cbct were 1029 10 , 1140 20 , and 760 40 , respectively ( figure 1 )  . examining the central slice images of the ctp - 528 phantom acquired on fbct and the three scanning modes of cbct demonstrated that the spatial resolution of fbct was similar to that obtained when using the specific qa mode ( with small collimator and full - rotation scanning settings using higher exposure factors to obtain the premium quality images through a high - resolution reconstructive process ) to acquire cbct . 
 therefore , we chose not to use the bowtie filter but designed the high - resolution preset using the qa mode with a small col1400 1200 1000 limator , 32 ma , 10 ms , and 360 rotational cbct acquisition in the subsequent experiments . mathematical analyses were performed to obtain material density ( ) and the corresponding ct number ( hounsfield unit , hu )  . 
the hucurves showed two lincurves showed two lincurves showed two linear segments of different slopes ( with the corresponding slope coefficient ( a ) and the intercept ( b ) ) in two different density zones , air - to - water and water - to - teflon , with water as the intersection . 
a graphs of ct number ( hu ) versus material density ( ) defined for the radiation treatment planning system ( rtps ) and obtained on fan - beam computed tomography ( fbct ) for the cirs - 062 phantom with outer ( o ) and inner ( i ) pelvis as well as head regions . 
a graphische darstellung der ct - werte ( hu ) versus materialdichte ( ) , definiert fr das radiotherapie - planungssystems ( rtps ) und ermittelt durch eine fbct bei einem cirs - 062 - dummy mit ueren ( o ) und inneren ( i ) beckenund kopfregionen . 
such modified cbct images were imported to the planning system and defined as the modified cbct ( mcbct )  . dose planning on mcbct image sets an isocentric plan with two orthogonal beams was created in the center of the phantom for fbct and mcbct image sets . 
one nasopharyngeal cancer patient treated with imrt was selected with his cbct image acquired after the registration of the first cbct image set to obtain the positioning errors , the correction of the positioning errors , and the re - acquisition of the second cbct image set . 
 comparisons between fbct and the two mcbct , acquired in weeks 1 and 6 of the radiotherapy course , were performed for the second nasopharyngeal cancer patient . results imaging uniformity by optimal cbct acquisition using the high - resolution preset of cbct , the corresponding profiles on the x - axis and y - axis ( figure 3 ) showed the largest ct number variations of less than 50 . 
the results indicate acceptable imaging uniformity of 15 cm along the z - axis . ct number analysis and conversion for cbct based on the relationship between fbct and cbct shown on the graph of ct number ( hu ) versus material density ( ) , the ct number of water on cbct ( 1219.3 ) was first normalized to be the same as the ct number of water on fbct ( 1029.1 ) , with the difference of 190.2. 
two linear regression models ( densities from air - to - water and from water - to - teflon ) were then generated to convert the ct numbers of cbct to those of fbct . the following equations were obtained : figures 6a to 6d . 
dose distribution comparisons between ( a ) fan - beam computed tomography ( fbct ) ( thin dose lines ) , ( b ) unmodified cone - beam computed tomography ( cbct ) ( thick dose lines ) using soft - tissue window , and ( c ) bone - window settings , and ( d ) modified cbct ( thick dose lines ) using soft - tissue window setting on central slice of the ctp - 401 phantom planned with two orthogonal 6 - mv photon beams . 
vergleich der dosierungsverteilung zwischen ( a ) einer fbct ( dnne dosislinien ) , ( b ) einer unvernderten cbct ( dicke dosislinien ) unter anwendung eines weichgewebefensters , ( c ) knochenfenster - einstellungen und ( d ) einer vernderten cbct ( dicke dosislinien ) unter anwendung einer weichgewebefenster - einstellung am zentralschnitt des ctp - 401 - dummy und geplant mit zwei orthogonalen 6 - mv - photonenstrahlen . 
die 5 cm tiefen punkte sind in blau fr anterior - posterior und in pink fr links - rechts markiert . these ct numbers shown on the modified cbct , defined as mcbct , were close to the corresponding ct numbers on fbct ( figure 4 )  . 
the ct number differences between the maximum and minimum scanning values were around 150 by fbct as compared to around 250 by mcbct ( figure 5 )  . dose comparison for the ctp - 401 phantom the isodose curves were similar between fbct and mcbct with the separation of the corresponding isodose curves less strahlenther onkol 2011 no . 
cbct for dosimetry in head and neck cancer left parotid ( fbct ) left parotid ( cbct ) left parotid ( mcbct ) target ( fbct ) target ( cbct ) target ( mcbct ) right parotid ( fbct ) right parotid ( cbct ) right parotid ( mfbct ) brain stem ( fbct ) brain stem ( cbct ) brain stem ( mcbct ) spinal cord ( fbct ) spinal cord ( cbct ) spinal cord ( mcbct ) 1000 2000 3000 4000 5000 6000 7000 8000 dose ( cgy ) figures 7a to 7f . 
cbct for dosimetry in head and neck cancer left parotid ( fbct ) left parotid ( cbct ) left parotid ( mcbct ) target ( fbct ) target ( cbct ) target ( mcbct ) right parotid ( fbct ) right parotid ( cbct ) right parotid ( mfbct ) brain stem ( fbct ) brain stem ( cbct ) brain stem ( mcbct ) spinal cord ( fbct ) spinal cord ( cbct ) spinal cord ( mcbct ) 1000 2000 3000 4000 5000 6000 7000 8000 dose ( cgy ) figures 8a to 8f . 
the overlap of volumetric reconstructions from the week 1 and 6 ( a ) fan - beam computed tomography ( fbct ) and ( b ) modified cbct ( mcbct ) were shown with the color scale ( in cm ) indicating the setup errors . 
c , d , e the two transverse slices and one sagittal slice overlapped from the week1 ( gray ) and week6 ( orange ) cbct showed the setup errors mainly from the weight loss and regression of cervical lymph nodes . 
die aufgezeigte berlagerung volumetrischer rekonstruktionen der ersten und sechsten woche ( a ) fbct und ( b ) vernderter cbct ( mcbct ) , wobei die farbskala ( in cm ) setup - fehler anzeigt . 
c , d , e die beiden querlaufenden schnitte und ein sagittaler schnitt berlagernd von der ersten ( grau ) und sechsten woche ( orange ) cbct zeigen die setup - fehler , welche hauptschlich durch den gewichtsverlust und rckgang der halslymphknoten entstanden . 
cbct for dosimetry in head and neck cancer left parotid ( fbct ) left parotid ( cbct ) left parotid ( mcbct ) target ( fbct ) target ( cbct ) target ( mcbct ) right parotid ( fbct ) right parotid ( cbct ) right parotid ( mfbct ) brain stem ( fbct ) brain stem ( cbct ) brain stem ( mcbct ) 1000 2000 3000 4000 5000 6000 7000 8000 dose ( cgy ) figures 10a to 10f . 
the dosevolume histograms were similar between fbct and mcbct but not unmodified cbct ( figure 7 )  . dose comparison for the nasopharyngeal cancer patient plans the dose differences of target and structures were < 3% ( data not shown )  . 
the dose distributions were compared , and the dosevolume histograms were similar between fbct and mcbct but not unmodified cbct ( figure 8 )  . the dosimetric differences of a second nasopharyngeal cancer patient were shown between the first week and sixth week image sets mainly due to the setup errors from weight loss and the regression of cervical lymph nodes ( figure 9 )  . 
the dose distributions were similar between fbct and mcbct but not unmodified cbct ( figure 10 )  . discussion since the elektas cbct system does not provide a tool for ct number calibration , an acquired ct set must be converted to ct numbers using a proper calibration method . 
this study investigated a practical setting of elektas cbct acquisition to achieve good image quality and developed a method to modify the ct numbers of cbct for accurate dose calculation . 
our method represented one of the practical settings to generate acceptable spatial resolution and uniformity . several studies investigated the use of cbct for adaptive rt [ 2 , 24 , 26 , 29 , 30 ]  . 
we were able to simulate most dose errors of < 2% , with the cbct image modification and no filter was needed . although some planning systems may allow different electron density tables for calculating the doses on the unmodified cbct images [ 8 , 19 ] , it is essential to modify and obtain the high - resolution images for re - contouring tumor / structures in the adaptive rt process . 
the head and neck region is the site with smaller setup errors , and the total dose deviation from both the positioning error and the imaging difference may meet the clinical level of acceptance in using cbct for re - planning purposes . this study was limited in that we did the modification only for cbct images acquired by the small collimator . 
the cbct for thorax , abdomen , or pelvis needs a larger collimator , which further compromises imaging quality and demands another specific protocol to modify the cbct . by repeated fbct , the underdose problem of ptv and overdoses to the brain stem and parotids were observed when re - calculating the dose coverage with the initial imrt plan on patients during their fractionated rt courses [ 7 ]  . 
similarly by repeated cbct in head and neck cancer patients undergoing rt , dosimetric changes were caused by a combination of setup inaccuracy , organ deformation , tumor shrinkage , or weight loss [ 1 , 13 , 15 , 17 , 23 , 25 ]  . 
given the fact that body shape or tumor size may change during fractionated rt , especially in head and neck cancer patients , it may be helpful to develop the imaging modification method using the on - line cbct images for recontouring and re - calculating strategies . acknowledgments this work was supported by national science council , execute yuan , taiwan , roc ( nsc 96 - 2628 - b - 002 - 105 - my3 and 99 - 2314 - b - 002 - 111 ) , and national taiwan university hospital grants ntuh 98s1128 , 98n1235 , and 99s1361 . original article accelerated radiotherapy with concomitant boost technique ( 69.5 gy / 5 weeks ) an alternative in the treatment of locally advanced head and neck cancer jiri kubes1 , jakub cvek2 , vladimir vondracek1 , miloslav pala1 , david feltl2 background and purpose : to present the feasibility and results of accelerated radiotherapy with concomitant boost technique ( 69.5 gy / 5 weeks ) in the treatment of locally advanced head and neck cancer . patients and methods : a total of 65patients were treated between june2006 and august2009 . 
die spttoxizitten betrafen haut ( grad 3 : 9 , 5% ) und speicheldrsen ( grad 3 : 3 , 7% )  . schlussfolgerung : die akzelerierte strahlentherapie mit der concomitant - boost - technik ist bei patienten mit kopfund halstumoren durchfhrbar . 
diese technik hat ein akzeptables toxizittsprofil und gute heilungsergebnisse . schlsselwrter : akzelerierte strahlentherapie kopfund halstumoren concomitant - boost - technik introduction the role of the time factor in the radiotherapy of spinal cell head and neck cancer is well known . 
the prolongation of overall treatment time worsens treatment results and dimin ishes the effective dose of normofractionated radiotherapy approximately with 0.60.8yday with prolongation of over yday with prolongation of over yday with prolongation of over all time beyond 21days [ 14 , 18 ]  . 
the optimal overall treatment time should be approximately equal to the time of the 1institute of radiation oncology , faculty hospital na bulovce and 1st faculty of medicine charles university , prague , the czech republic , 2department of oncology , faculty hospital ostrava , the czech republic . received : december 1 , 2010 ; accepted : april 8 , 2011 published online : september 23 , 2011 strahlenther onkol 2011 no . 
accelerated rt in locally advanced head and neck cancer commencement of accelerated repopulation ; the prolongation of overall time may diminish the biological dose due to tumor stem cell repopulation , while shortening of the radiotherapy course can prevent the full effects of reoxygenation and redis tribution of tumor cells . 
moreover , hyperfractionation can be more significant in the second part of the radiotherapy course due to the short ening of the effective doubling time of tumor cells [ 3 ]  . there are various types of concomitant boost techniques described in literature . 
a similar accelerated schedule with high dose and short treatment time ( 69.5 y5 weeks ) in the treatment of head and neck cancer was applied by terhaard et al . 
 material and methods between january 2006 and june 2009 , we used this schedule for the treatment of 65patients with head and neck cancer ( 55men and 10 women ; 85% of them with locally advanced tumors , mainly oropharyngeal and laryngeal tumors )  . 
patientencharakteristika. gender age anatomic sites ajcc stage t stage n stage histology histological grade male female mean range oropharynx larynx hypopharynx oral cavity nasopharynx other not defined epidermoid value ( % ) 55 ( 85% ) 10 ( 15% ) 58.6 years 3878 years 27 ( 41.5% ) 21 ( 32.3% ) 5 ( 7.7% ) 7 ( 10.8% ) 1 ( 1.5% ) 4 ( 6.15% ) 7 ( 10.7% ) 15 ( 23% ) 40 ( 61.5% ) 3 ( 4.6% ) 0 13 ( 20% ) 21 ( 32.3% ) 29 ( 44.5% ) 2 ( 3.1% ) 25 ( 38.7% ) 9 ( 13.8% ) 8 ( 12.3% ) 9 ( 13.8% ) 9 ( 13.8% ) 3 ( 4.6% ) 2 ( 3.1% ) 65 ( 100% ) 9 ( 13.8% ) 19 ( 29.2% ) 31 ( 47.7% ) 5 ( 7.7% ) 1 ( 1.5% ) radiotherapy technique the treatment was performed on linear accelerators with a nominal photon beam energy of 6mev . 
clinical target volume for the initial phase of treatment included the primary tumor and involved lymph nodes ( tv ) with a 10 mm margin for subclinical spreading and neck lymphatic regions according to the institutional protocol for various primary sites ( in the ma jority of cases the ibv bilateral and retropharyngeal regions )  . 
the ma jority of patients had percutaneous en doscopic gastrostomy ( pe ) introduced during the first 2weeks of treatment . evaluation of treatment effects acute and late toxicities were evaluated according to the rto scale . 
the tu mor response was assessed by clinical examination at 3month intervals and with ct or mri imaging 3month after radiotherapy and , thereafter , once a year . statistics overall survival ( os ) and disease free survival ( dfs ) were calculated using the kaplanmeier method . 
the acute toxicity grade 3 or 4 was observed in the pharynx and esophagus ( 42% ) , skin ( 10% ) , mucous membranes ( 43% ) , and larynx ( 4% )  . 
late toxicity grade 3 was observed in skin ( 6% ) parotid glands ( 4% ) , but not in the spinal cord or subcutaneous tissue . a total of 48patients were alive and 17patients died ( 2of them without tumor ) at the time of evaluation in march2010 . 
kaplan meier survival curves for overall and disease free survival are shown in figure 1 . the influence of t stage , n stage , clinical stage , tumor grade , the site of primary tumor , the overall treatment time ( with a cutoff of 37days ) , and imrt technique to the overall survival and the diseasefree survival were evaluated . 
only n stage n0 was significantly better in dfs ( p = 0.014 ) and clini cal stageiv was significantly worse in os ( p = 0.028 ) and dfs ( p = 0.027 ) , which was expected . 
accelerated rt in locally advanced head and neck cancer ter results in shorter overall treatment time and imrt tech nique ; however , it was not statistically significant . discussion local control is still the main problem of the treatment of lo cally advanced head and neck cancer [ 6 ] , which can be solved by two different methods : ( 1 ) using a standard radiation dose ( about 70y of normofractionated radiotherapy ) in combina tion with concomitant chemotherapy or biological treatment or ( 2 ) using a more effective radiotherapy schedule . 
moreover , the higher dose of concomitant chemo therapy may yield poorer results [ 20 ] and the combination of chemotherapeutic agents has higher toxicity regardless of the treatment results [ 22 ]  . 
concomitant application of biological treatment is also effective and possibly less toxic [ 1 ] , but higher than primarily published toxicity of concomitant biological treatment was also described [ 12 ]  . radiotherapy alone can be intensified in two ways . 
concomitant boost technique combines the advantages of hyperfractionated and accelerated schedules , i.e. , sparing of healthy tissues and preventing the accelerated repopulation of tumor cells . the prolongation of treatment course duration over 4weeks may lead to the loss of the applied dose ( about 0.60.8 yday ) [ 14 , 18 ]  . 
in contrast , shortening treatment time to less than 3 or 4weeks increases the toxicity without effecting local control , as was described in the chart trial [ 4 ]  . 
optimal radiotherapy treatment time for head and neck cancer is most likely the same as the kickoff time of accelerated repopulation , which is about 28days after treatment start [ 7 ]  . the risk of alternative fractionated schedules is increased toxicity , both acute and late . 
table 2 shows that the concomitant boost regi men has the best ratio of bed for tumor , late tissues , and acute tissues as compared to most widely used regimens . concomitant boost schedules in the treatment of head and neck cancer are described in literature and their effectiveness and safety were verified in randomized trials . 
our work shows that this regimen can be safely used for the treatment of locally advanced head and neck cancer in localizations other than the larynx , with large boost volumes . overall survival and diseasefree survival are better than the results in the majority of published series . 
accelerated rt in locally advanced head and neck cancer significant number of patients were treated with accelerated radiotherapy due to contraindication for chemotherapy , so it can be inferred that they had substantial comorbidities . 
the percentage of mucositis and der matitis grade3 is slightly higher than during chemoradiothera py ( 70y35fractions7weeks with weekly cisplatinum 40mg m2 ; data not published ) at our institution , but the time of severe mucositis is shorter . 
the late toxicity is acceptable and is not different from chemoradiotherapy . a remarkable fact is that the number of distant metastatic recurrences is very low , which may be a result of a small num ber of patients with high grade ( grade 3 or 4 ) tumors that have higher metastatic potential . 
epidermoid tumors with good or intermediate differentia tion have higher dependency on overall treatment time [ 5 ]  . conclusion concomitant radiotherapy with accelerated boost ( 69.5y5weeks ) is a safe and highly effective technique for patients with locally advanced head and neck cancer . 
it can be recom mended as an alternative in the case of a contraindication to concomitant chemoradiotherapy and possible as a first choice treatment for grade1 or 2 epidermoid tumors , where the effect of the acceleration will be most prominent . 
alt2 , michael eichbaum1 , christof sohn1 , hans - ulrich kauczor2 , peter hallscheidt2 aim : the goal of this article is to provide an overview of diagnostic standard operating procedures for both clinical and imaging assessment of cervical and endometrial carcinoma , sarcoma of the uterus , and primary pelvic non - hodgkins lymphoma . methods : the literature was reviewed for methods used to diagnose malignancies in the female pelvis with a special focus on the role of mri as the imaging method of choice . 
 conclusion : whereas ultrasound still remains the imaging modality of choice in clinical practice for the early diagnosis of female pelvic malignancies , mri is more frequently recognized as a diagnostic tool for its accuracy in tumor identification . 
 schlussfolgerung : im klinischen alltag ist der ultraschall fr die primrdiagnostik weiblicher beckentumoren bildgebendes verfahren der wahl , wobei die mrt durch den hohen weichteilkontrast einen zunehmenden stellenwert als bildgebendes verfahren zur tumordetektion besitzt . 
cross - sectional imaging modalities , including ultrasound ( us ) , computed tomography ( ct ) , and magnetic resonance imaging ( mri ) have increasingly been used for optimal treatment planning in gynecologic malignancies . 
their staging criteria are based on the well - established international federation of gynecologists and obstetricians ( figo ) staging system and the tnm classification system [ 38 , 47 ]  . 
positron emission tomography ( pet ) , especially if combined with ct ( pet / ct ) , might have a benefit in staging and restaging gyne1department of obstetrics and gynecology , medical school , university of heidelberg , heidelberg , germany , 2department of diagnostic and interventional radiology , medical school , university of heidelberg , heidelberg , germany . received : march 24 , 2011 ; accepted : june 23 , 2011 published online : september 23 , 2011 strahlenther onkol 2011 no . 
imaging of female pelvic malignancies with mri , ct , and pet / ct ( part 1 ) cological malignancies , especially regarding lymph node metastases or recurrent tumor due to the simultaneous availability of functional and anatomical information [ 9 , 14 , 29 , 32 , 35 , 42 ]  . 
 this paper emphasizes the role of cross - sectional imaging modalities in pretreatment staging and restaging of gynecological pelvic malignancies . radiological diagnostics ct is widely used , being the gold standard in oncology for initial staging and re - evaluation after treatment . 
because differentiation of recurrent tumor and radiation fibrosis is also challenging on ct , mri has become the most valuable imaging tool for diagnosing pelvic tumors in women [ 31 ]  . 
due to a wide variety of possible imaging sequences , high spatial resolution , and superior soft tissue contrast , nonenhanced mri can often provide sufficient information without the need of contrast agent application . 
imaging evaluation may be improved by preparing the patient with a moderately filled bladder with urine , the application of an intravenous antiperistaltic agent ( i.e. , butylscopolamine ) and by distending the vagina with sterile ultrasound contact gel [ 3 , 4 , 11 , 53 ]  . t1 - weighted sequences easily depict pelvic structures from fat tissue , whereas t2 - weighted sequences allow for the distinction of pelvic organs as well as differentiation of their internal composition and homogeneity . 
however , for distinguishing tumor recurrence from scar tissue , the application of an intravenous contrast agent is crucial . an additional diagnostic imaging tool in mri is an endorectal coil , which is custom designed for mri of uterine and cervical structures . 
due to its positioning inside the rectum in direct contact with the cervix , the endorectal cervix coil provides more reliable tissue differentiation due to the high spatial resolution in a smaller field of view ( fov ) at 1.5t [ 20 , 34 , 40 , 44 ]  . 
whereas the ct presents precise and clear 3d information regarding a patients geometrical data and electron density distribution , the mri has , due to its good soft tissue differentiation , advantages in defining the tissue volume needing radiation ( gross tumor volume ( gtv ) , clinical target volume ( ctv ) , and planning target volume ( ptv ) ) [ 45 ]  . around the gtv , which is defined by three planes in the mri , a safety margin is added to define the clinical target volume . 
brachytherapy is used in patients with cervical cancer , but is seldom used in patients with primary endometrial cancer . becoming increasingly more interesting is positron emission tomography ( pet ) , a molecular imaging technique that can be used to visualize metabolic differences between tissues and , therefore , might depict suspicious lesions . 
unfortunately , it has its limitation in the difficulty of depicting tumor lesions precisely due to accumulation , also in normal tissues or inflammatory lesions [ 42 ]  . operating procedures and mri findings are described in detail in the following , while complementary information about ct and pet / ct findings are also mentioned . cervical cancer general information the incidence of cervical cancer varies between 3.645 / 100 , 000 women each year . 
according to the robert - kochinstitut , about 6 , 500 women in germany were diagnosed with an invasive cervical cancer in the year 2002 and more than 1 , 700 women died , leading to a mortality of 30% . 
the mean age was 52.2years with a peak between 3554 years and a second peak at 65years of age [ 2 ]  . diagnostic standard operating procedure clinical vaginal and colposcopical examinations of the cervix , including the bimanual palpation of the parametrial area in addition to cytological smears and biopsies are state of the art in diagnosing cervical cancer . 
awmf and dggg guidelines recommend the use of mri in staging a cervical tumor at a clinical figo stage ib2 or higher for the assessment of local tumor spread and infiltration of surrounding tissue ( table 1 ) [ 2 ]  . 
 radiological findings in diagnosing cervical cancer , the recommended standard protocol in mri includes t2 - weighted turbo spin echo ( tse ) sequences with high spatial resolution ( matrix 512 ) in the sagittal and transversal oblique ( short cervical axis ) planes in addition to a t1 - weighted tse sequence in the transversal plane . 
in order to correctly identify an interruption of the hypointense cervical stroma and diagnose parametrial infiltration , the transversal slices should be parallel to the short axis of the cervix [ 30 , 53 ]  . 
in the t1 - weighted contrast - enhanced fat - saturated sequence ( t1 - weighted fs km ) , the tumor presents as a hyperintense lesion , which is of great value for diagnosing small tumors . 
in the transversal plane of the t2 - weighted sequence , the hypointense ring of the cervix stroma is intact on the left side , but disrupted on the right side ( white arrow )  . 
in germany , about 11 , 300women are diagnosed with endometrial cancer annually [ 1 ]  . diagnostic standard operating procedure a transvaginal ultrasound is recommended to obtain an impression of the endometrial layer or suspicious lesions in the female pelvis , for example , in case of vaginal bleeding . 
further imaging modalities , e.g. , ct , pet , or mri , are not recommended by recent guidelines for staging endometrial cancer , since they have not been proven to be beneficial , although the extent of myomentrial infiltration can be estimated with mri ( table 3 ) [ 1 ]  . radiological findings again , mri is a superior imaging modality compared to ct in staging endometrial cancer . 
t2 - weighted turbo spin echo ( tse ) sequences with high spatial resolution ( matrix 512 ) in the sagittal , transversal oblique ( short uterine axis ) and coronal oblique ( long uterine axis ) planes are recommended for the staging of endometrial cancer . 
in order to correctly identify myometrial infiltration depth of more than 50% and consequently correctly distinguish between a local tumor stage t1a and t1b , the transversal slices should be parallel to the short axis of the uterus ( figures 4 and 5 ) [ 23 , 43 ]  . 
the assessment of myometrial invasion is difficult [ 31 ]  . in addition , recent studies have shown that in case of restaging for recurrence of endometrial carcinoma , pet / ct might be beneficial [ 8 , 24 ]  . 
 histologisch gesichertes zervixkarzinom im stadium t2b . in case of brachytherapy procedure planning , mri is more reliable and more appropriately assesses , compared to ct or clinical examination , size , configuration , and topography of the tumor , which leads to accurate delineation of the gtv and can facilitate dose optimization [ 7 , 10 , 16 , 39 , 51 ]  . endometrial cancer general information the incidence of endometrial cancer is about 142 , 000cases per year worldwide , yet it shows regional variations and rises with strahlenther onkol 2011 no . 
malignant sarcoma of the stroma , mixed cell tumors , e.g. , osteochondrorhabdomyosarcoma or mesodermal tumors , e.g. , muellerian adenocarcinoma , derive from endometrial tissue , whereas leiomyosarcomas often derive from the myometrium [ 46 ]  . diagnostic standard operating procedure the malignant endometrial sarcoma is often a coincidental diagnosis in women with simple hysterectomies , since most patients are asymptomatic . 
symptomatic patients present with uncharacteristic spotting or postmenopausal vaginal bleeding and pelvic pa hysteroscopy and curettage are generally recommended , whereas in case of tumor mass extruding the cervix , a biopsy leads to diagnosis ( tables 4 and 5 )  . 
cervical mass with parametrial infiltration and obstruction of the left ureter ( white arrow ) in a t2 - weighted sequence with high spatial resolution in the transversal and coronal planes . 
for pretreatment planning , ct and mri give 3d information about tumor size , configuration , and topography and can , therefore , influence dose adaption [ 11 , 52 ]  . 
 smooth muscle cell tumors with fuzzy margins , more than 50% of hyperintense signal volume in a tumor on t2 - weighted images or any small hyperintense signal volume on t1 - weighted images are findings which might suggest leiomyosarcoma . 
however , mri can only differentiate sarcoma of the uterus from endometrial cancer with combined findings of irregular tumor margins and marginal nodular lesions which might not be possible in all cases [ 25 ]  . 
 contrast - enhanced ct can provide an overview of infiltrated surrounding structures , distant metastases , ascites , renal obstruction or peritoneal spread , while a local tumor is uncharacteristic despite of its rapid growth [ 26 , 31 ]  . 
kurzer schwarzer pfeil : intramurales myom , erc : endorektalspule . may be significantly important for grading , staging , and followup in sarcomas [ 5 ]  . primary pelvic non - hodgkins lymphoma general information malignant lymphoma of the uterus or cervix is a very rare entity ( incidence > 1% )  . 
in the clinical examination , patients may either show no symptoms at all or present with pelvic pain , vaginal bleeding , or tumor mass discharge [ 37 ]  . diagnostic standard operating procedure for diagnosing lymphomas of the female genital tract , no gynecological guidelines have been published recently . 
however , contrast - enhanced , whole - body ct may be performed for therapy planning and follow - up after treatment every 3 or 6months [ 48 ]  . 
they often appear as homogeneously hyperintense masses without a clear margin to the surrounding healthy tissue , which is why their differentiation from degenerative benign leiomyomas , endometrial cancer , or a large cervical cancer is difficult [ 22 ]  . 
in the t1 - weighted sequence , vaginal lymphoma appears as a homogeneously hypointense lesion , which is moderately hyperintense in a t2 - weighted sequence and presents with high signal intensity post contrast . 
 whereas pet is the indicated modality in identifying and localizing lymphatic lesions with non - hodgkin lymphoma showing high fdg accumulation [ 29 , 42 ] , even for small lesions , the spatial resolution of pet / ct is still not sufficient [ 48 ]  . conclusions for visualizing female pelvic tumors , mri has become appreciated as the cross - sectional imaging modality of choice , whereas ultrasound still remains the gold standard in early diagnosis due to its widespread availability and cost effectiveness . 
advantages of mri are better tumor delineation in the entire pelvis , superior tissue contrast , and additional information concerning accompanying pathologies which can be helpful for further therapy planning . 
 although , ct has poor soft tissue contrast , which is a major drawback in the pelvis , it provides important information about peritoneal implants , lymph nodes , ascites , and distant metastases ( e.g. , of the lung and the liver )  . 
 according to the literature , pet / ct is beneficial in visualizing involved abdominal lymphatic pathways and might be helpful for restaging of a recurrent tumor or distant metastases , especially in lymphoma and cervical cancer . 
unfortunately , however , local tumor depiction might be challenging because of its low spatial resolution and bowel or urinary artifacts due to excretion of the radiotracer . brachytherapy can be the treatment of choice in patients with locally progressed cervical cancer and in occasional cases of endometrial cancer . 
for optimal pretreatment radiation planning , mri allows precise identification of the gtv and ctv in three planes . current discussion quality assurance for clinical studies in regional deep hyperthermia gregor bruggmoser1 * , stefan bauchowitz2 * , richard canters9 * , hans crezee3 * , michael ehmann4 * , johanna gellermann5 * , ulf lamprecht6 * , nicoletta lomax9 * , marc benjamin messmer1 , oliver ott2 * , sultan abdel - rahman7 * , rolf sauer2 , manfred schmidt2 * , andreas thomsen1 , rdiger wessalowski8 , gerard van rhoon10 * background : a guideline is provided for the implementation of regional deep hyperthermia treatments under strict rules of quality assurance . 
according to this guideline , hyperthermia treatment is always applied in combination with chemotherapy and / or radiotherapy . methods : the guideline is based on practical experience from several hyperthermia centers . 
 results : the guideline contains recommendations for hyperthermia treatments , including indication , preparation , treatment , and standardized analysis . key words : hyperthermia responsibilities thermometry radiation chemotherapy hyperthermia side effects strahlenther onkol 2011 ; 187 : 60510 doi 10.1007 / s00066 - 011 - 1145 - x qualittssicherung in der regionalen tiefenhyperthermie hintergrund : zur durchfhrung von qualittsgesicherten tiefenhyperthermiebehandlungen wurde eine leitlinie erstellt . 
dieses vorgehens erlaubt abgestimmte standards in der anwendung und der qualittskontrolle in der hyperthermie fr studien . ergebnisse : diese leitlinie enthlt empfehlungen fr hyperthermiebehandlungen mit indikationsstellung , vorbereitung , durchfhrung und standardisierter auswertung . 
 schlsselwrter : hyperthermie verantwortlichkeiten thermometrie bestrahlung chemotherapie hyperthermienebenwirkungen * the authors of this document are also members of the esho technical committee . 1 department of radiation oncology , university hospital of freiburg , germany , 2 clinic for radiotherapy , university hospital erlangen , germany , 3 department of radiation oncology , academic medical center ( amc ) , amsterdam , the netherlands , 4 department of radiation oncology , university medical center mannheim , germany , 5 formerly radiotherapy charit university clinic , germany , 6 hospital for radiation oncology , university hospital of tbingen , germany , 7 medical clinic iii , university clinic munich , munich , germany , 8 clinic of pediatric hematology , oncology and clinical immunology , university hospital of dsseldorf , germany , 9 clinic for radiation oncology , cantonal hospital aarau , switzerland , 10 department of radiation oncology , erasmus mc daniel den hoed cancer center , rotterdam , the netherlands . received : june 17 , 2011 ; accepted : july 4 , 2011 published online : september 19 , 2011 strahlenther onkol 2011 no . 
qa in regional deep hyperthermia background and purpose members of the esho technical committee in the interdisciplinary working group hyperthermia ( iah ) in the german cancer society defined an extensive guideline for regional hyperthermia as part of an overall quality assurance ( qa ) program in hyperthermia , which is essential for physicians , physicists , and technical personnel performing and supervising hyperthermia treatments [ 19 ]  . 
 the premise of this qa guideline program is that the effectiveness of hyperthermia as proven in several clinical studies relies exclusively on its thermal effect on tumors , [ 15 , 16 , 17 , 28 , 30 , 31 ]  . 
for this reason , it is mandatory that hyperthermia treatments are performed by devices that are technically capable of delivering selective and controlled heating to a predefined target volume , while causing minimal heating of normal tissue at the same time . 
 in addition , recording the temperature in the target volume directly or in the surrounding , tumor indicative , tissue is essential for an adequate evaluation of the treatment quality . 
in terms of this guideline , any other devices which technically do not fulfill the requirements for hyperthermia systems , e.g. , temperatures in the target volume between 40 and 43c for at least 60 min or not capable of measuring the temperatures at the described locations , should not be used for hyperthermia treatment . the current publication provides a short version of the quality assurance guideline for the clinical application of regional deep hyperthermia ( rht ) and mr - controlled partial body hyperthermia ( pbh ) in adult patients in a combined treatment using chemoand / or radiation therapy [ 6 , 22 , 23 , 24 , 25 , 27 ]  . 
it also provides a partial update of the esho quality assurance guidelines for regional hyperthermia of 1998 [ 19 ]  . responsibilities for the indication , planning , treatment , and documentation the physician is responsible for the indication for hyperthermia treatment , taking into account inclusion and exclusion criteria , based on medical history and patient information . 
it involves various professional groups , radiooncologists , medical oncologists , medical physicists , engineers , as well as technical staff , nurses , and personnel required for special applications . 
to preserve healthy tissue and possible risk organs , other probes are placed appropriately , including a record of the systemic temperature [ 2 , 4 , 8 ]  . relevant parameters for determining the quality of the hyperthermia are td43 ( t90 ) or cem43 [ t90 ] in min , td43 ( t50 ) or cem43 [ t50 ] in min , and tmean , tmin , tmax , t90 , t50 , t20 , t10 in c . the parameter relevant for sparing healthy tissue is tmax in normal tissue in c . 
for the western patient , who has gained weight at the abdominal wall , hips , or buttocks exceeding 2 cm thickness , these above mentioned requirements are technically best achieved when spatial power control is used , guided by active thermometry in the target volume . 
a procedure must be specified by the physician how to handle the situation in case of complaints , e.g. , if hot spots occur during therapy . three - dimensional ( 3d ) images ( mri , ct , us ) or orthogonal x - rays must be taken to prepare for treatment . 
 experience exists that in specific cases when the metal implant is small ( < 1 cm ) hyperthermia can be applied but with special attention to avoid preferential heating around the metal implant and under the supervision of the physician . 
alternatively , one may apply hyperthermia treatment planning ( htp ) to investigate whether excessive heating is caused by the metal implant . mr compatibility of the metal implants must be clarified for treatment in a hybrid system ( hyperthermia system combined with mri )  . preparation for treatment similar to planning in radiation therapy , 3d images in the supine position are used to define the hyperthermia target point in the middle of the treatment volume . 
for details regarding treatment planning , see the full qa document . hyperthermia treatment before therapy , the physician must be assured that the patient is able to tolerate hyperthermia treatment . 
the patient should preferably be positioned identically from treatment to treatment , with the hyperthermia target point within the active area of the applicator [ 3 , 9 ]  . for treatments , the dorsoventral diameter of the patient should fit into the applicator . 
 cooling of the surface for instance to 25 c ( a range of 2128 c is common ) must be guaranteed for adequate removal of the heat load from the patient . 
when the target volume includes the body surface , care should be taken to keep the whole tumor at therapeutic temperature , i.e. , local cooling may not be necessary . 
the thermometry system must be calibrated against a traceable national standard . usually , measurements are taken at various specific predefined positions applying a mapping method , or multiple sensors are applied . 
 thermal mapping : temperature measurement using thermal mapping , i.e. , moving the temperature probe within the thermometry catheter through the treatment volume , must be performed under specified conditions . 
to minimize the influence of moving organs , suitable triggering is used , for example , during a breath - hold cycle , or the temperature measurement is reduced to a smaller volume area . 
 e - field probes e - field probes may also be used for treatment control , but it is necessary to be particularly precise when positioning both the patient and the probes . 
for all applicators , it is important to align the e - field probes with the longitudinal axis of the applicator . temperature objectives during treatment temperature limitations for hyperthermia are for normal tissue the maximum temperature and for the hyperthermia target volume the minimum temperature and the duration of the treatment . to prevent acute toxicity , the general objective is to avoid that the temperature exceeds 43c in normal tissue . 
a detailed specification of the maximum and minimum temperatures for individual areas and organs is defined in the study protocol . treatment time the treatment time consists of the heating - up time : max . 
30min or when the target temperature as prescribed in the study protocol is reached , and therapy time : 60 min . amplitude and phase control ( sar steering ) with specific settings for frequency , phase , and amplitude , focusing of the electromagnetic fields in the treatment volume is achieved and will result in selective heating without overheating the surrounding normal tissue [ 4 , 5 , 29 ]  . hyperthermia treatment planning ( htp ) can be carried out to find the primary settings for power , phase , and amplitude . 
without htp , the applicator settings for a sar focus at the center of the applicator is used ( i.e. , offset settings to move the sar to the center of the applicator )  . 
a further possibility is the setting guided by using e - field probes . procedure to increase the target temperature the goal for an effective hyperthermia treatment is to apply the highest therapeutic temperature which is tolerable for the patient [ 9 , 29 ]  . 
to achieve this aim , the following is recommended : 1st treatment : start with about 1 / 3 to 2 / 3 of the expected power needed to adequately heat a tumor at the specific localization and applied applicator position . 2nd treatment onward , adapt the parameters from the experience of the prior treatments . power should be increased in case of a temperature increase of less than 0.6c in 5ma temperature increase of 1c in 5min is optimal ; increases of more than 2c in 5 min should be avoided . instructions for complaints during treatment in case of complaints , the power must be shut off immediately to determine whether the pain is caused by the applied rf power . 
if an improvement is realized within 30 s , one can assume that the complaint is power related and the control parameters ( focus , amplitude , power ) should be adapted to reduce energy deposition at the complaint area . 
if the pain is not reduced 3060 s after rf power is turned off , it can be assumed that the pain is caused by the tumor or the positioning of the patient in the applicator and , therefore , pain medication may be given . 
alternatively , the patient could be repositioned and water bags may be applied for complaints that affect surface regions [ 29 ]  . documentation and analysis accurate and reliable documentation is critical for the evaluation and analyses of any clinical hyperthermia study . 
this requires that all the parameters that characterize the quality of the hyperthermia treatment are recorded and stored according to the instructions mentioned in the main quality assurance guideline and in the study protocol . 
for tumor response and toxicity follow - up , the evaluation procedure as defined in the study should be followed with regard to the following points : radiological response ( recist ) , complete tumor response ( cr ) local tumor progression ( lp ) , time to progression ( ttp ) , overall survival ( os ) , and acute or late toxicity . physicaltechnical documentation all treatment - relevant control parameters of the system ( e.g. , power and phase ) and all temperature measurement values must be documented in a manner that they can be related to the measurement location or catheter . 
qa in regional deep hyperthermia clinical documentation acknowledgments in particular , the clinical documentation describes medication , given cytostatics , clinical parameters of the patient , and side effects caused by the therapy . 
side effects of the combined treatment correspond primarily to the spectrum of side effects of the chemotherapy or radiation therapy in the sense that the side effects of the primary therapy can be intensified by the tissue heating during hyperthermia . 
possible skin changes should be documented , if possible during or at the latest after terminating treatment . classifying the degree of severity should follow the internationally established scores : ctcae v4.03 for chemotherapy - associated side effects , and rtog v2.0 for radiation - specific side effects . hyperthermia - specific side effects side effects that are specifically caused by the hyperthermia treatment should be recorded . 
unwanted higher temperature in the skin or healthy tissue is the main risk , which is significantly increased in patients with disturbed temperature sensitivity , for example , in polyneuropathy . 
the temperature threshold for such irreversible damage is 4446 c depending on tissue type [ 13 , 33 ]  . standardized analysis of treatment data in order to create comparable analyses for all study participants , the relevant data are extracted from the stored values and analyzed using standard software , e.g. , rhythm ( rotterdam hyperthermia thermal modulator ) [ 7 ]  . 
the program calculates and documents all necessary thermal dose parameters ( e.g. , tmax , tmean , t20 / 50 / 90 , cem43t90 ) , the applicator control parameter , and the therapy period . 
the whole procedure is described , starting with the indication , preparation , treatment , and documentation , including standardized analysis of the results . the authors thank the members of the atzelsberg clinical circle of the iah for their constructive comments and their continuous stimulation to prepare the quality assurance document for regional deep hyperthermia . 
the opinion of the authors is solely based upon the available scientific knowledge and their personal experience in the clinical application of hyperthermia . original article topical use of a silymarin - based preparation to prevent radiodermatitis results of a prospective study in breast cancer patients martina becker - schiebe1 , ulrich mengs2 , margitta schaefer2 , michael bulitta3 , wolfgang hoffmann1 purpose : more than 80% of patients with breast cancer undergoing postsurgical radiotherapy ( rt ) will develop radiodermatitis and approximately 10% of these patients show grade3 lesions . 
in this study , a silymarin - based cream ( leviaderm ) was tested in comparison to our standard of care ( soc ) at the involved site . methods : a total of 101 patients were evaluated after breast - conserving surgery followed by rt with 50.4 gy plus boost 916 gy . 
of these , 51 patients were treated with the silymarin - based creain addition , 50patients were documented receiving a panthenol - containing cream interventionally , if local skin lesions occurred . 
2% with soc , while grade3 toxicity occurred only in 2% in the silymarin - based arm compared to 28% ( soc )  . conclusions : silymarin - based cream leviaderm may be a promising and effective treatment for the prevention of acute skin lesions caused by rt of breast cancer patients . 
to confirm the results of this nonrandomized , observational trial , this component should be tested in larger multicenter studies in this setting . key words : breast cancer radiodermatitis silymarin leviaderm panthenol strahlenther onkol 2011 ; 187 : 48591 doi 10.1007 / s00066 - 011 - 2204 - z prophylaxe und therapie der radiodermatitis mit einer silymarinhaltigen cremeformulierung : ergebnisse einer prospektiven untersuchung von mammakarzinom - patientinnen hintergrund : im rahmen einer strahlentherapie ( rt ) nach brusterhaltender operation von mammakarzinom - patientinnen stehen die hautreaktionen im vordergrund der akuten nebenwirkungen . 
in dieser untersuchung sollte daher geprft werden , inwieweit eine prophylaktische an wendung mit einer silymarinhaltigen cremeformulierung ( leviaderm ) , hautreaktionen im vergleich zur standardpflege reduzieren kann . material und methode : ausgewertet wurden insgesamt 101 mammakarzinom - patientinnen , die nach einer brusterhaltenden op mit einer zvd von 50 , 4 gy + boost 916 gy bestrahlt wurden . 
23 , 5% der patientinnen , die prophylaktisch eine silymarinhaltige pflege anwendeten , zeigten bei rt - ende keine hautreaktionen gegenber 2% im standardarm ; g3 - toxizitten kamen im verlauf nur in 2% der flle unter silymarinhaltiger lokal - pflege vor ( vs 28% im kontrollarm )  . 1klinik fr radioonkologie und strahlentherapie , klinikum braunschweig , braunschweig , germany , 2research & development , rottapharm / madaus , cologne , germany , 3crm biometrics gmbh , rheinbach , germany . received : august 18 , 2010 ; accepted : january 21 , 2011 published online : july 22 , 2011 strahlenther onkol 2011 no . 
silymarin - based cream in the treatment of radiodermatitis schlussfolgerung : unsere daten dieser prospektiven , nicht - randomisierten untersuchung zeigen , dass die prophylaktische anwendung einer antioxidativen silymarinhaltigen cremeformulierung wie leviaderm signifikant schweregrad und hufigkeit einer radiodermatitis bei mammakarzinom - patientinnen reduzieren kann . 
it is estimated that 8090% of patients with breast cancer develop radiodermatitis and approximately 10% of these patients show a grade3 skin lesion before the scheduled end of rt [ 19 , 27 ]  . 
this can further be a limiting factor for the radiotherapist to follow and complete treatment protocols and may influence the curative efficacy . up to now , there has been a substantial lack of evidencebased skin treatment recommendations . 
because there are no generally accepted preventive treatments to control the onset and progression of radiodermatitis , new therapies are warranted . leviaderm , a silymarin - based cream , represents a new concept by combining prevention and therapy of radiodermatitis . 
silymarin - based cream may induce antioxidative actions when the skin is exposed to external noxae such as pollution , chemical agents , or irradiation [ 2 , 8 , 31 ]  . 
the pathophysiology of radiation - induced skin morbidities is understood as a secondary inflammatory reaction , possibly from the release of free radicals producing doubleand single - strand dna breaks [ 9 ]  . 
initial results of two observational reports [ 1 , 2 ] described preventive effects of silymarin - based preparations . therefore , this study was designed to assess whether supportive care using a silymarin - based cream is effective in preventing and reducing acute radiation dermatitis in comparison to standard skin care using panthenol - containing creams . material and methods patients with histologically documented diagnosis of breast cancer after breast - conserving surgery were eligible for this study . 
the occurrence of side effects and adverse drug reactions were recorded unblinded by the medical staff of the department during the weekly clinical examinations . patients with known hypersensitivity against any of the ingredients of leviaderm ( a class ii medical device from rottapharm / madaus ) or dexpanthenol - containing cream and with prior rt were excluded from this study . 
in this evaluation , 51patients were treated with silymarin - based creaa total of 50patients received local standard of care ( soc ) treatment consisting out of 5% dexpanthenol - containing cream , which was applied as an interventional treatment to the affected breast skin after occurrence of the first signs of skin alterations ( e.g. , erythema ) every day during rt and , thereafter , until skin recovered to normal . 
 silymarin - based cream was applied to the skin three times a day , 2weeks before beginning rt , during rt , and 2weeks afterwards ( table 1 )  . 
adelmidrol , or n , nbis - ( hydroxyethyl ) - nonandiamide , here used in a subclinical concentration of 0.5% , belongs to a family of lipidic molecules collectively defined as aliamides , which in preclinical and clinical testing using therapeutical concentrations of at least 2% have been reported to restore skin reactivity by downregulating mast cell hyperactivity [ 17 , 28 ]  . 
 rt : radiotherapie , soc : standardpflege . end of 1st week rt end of 2nd week rt end of 3rd week rt end of 4th week rt end of 5th week rt end of rt treatment 2 weeks after end of rt 4 weeks after end of rt continue treatment continue treatment ( treatment stop 2 weeks after end of no treatment continue treatment if necessary no treatment start and continue treatment after onset and continuation of skin lesions rtog toxicity score during treatment period t0 t8 visit schedule rt week enrollment / 2 weeks before rt immediately before first rt session treatment with leviaderm start treatment treatment with soc bidity scoring criteria ) [ 7 , 19 , 24 ]  . 
furthermore , the subjective toxicity was assessed using the visual analogue scales ( vas ) for itch , pain , and burning with a score of 0 defined as no symptoms and a score of 10 defined as the worst severity ever experienced [ 37 ]  . 
due to the lack of randomization and the different therapy schemes , the given p values can only be interpreted in a descriptive manner ( fishers exact test , t - test )  . 
 t02 soc t4 soc t6 l t6 soc t8 l t8 soc grade 0 grade 1 grade 2 grade 3 figure 1 : rtog acute radiation morbidity scoring criteria for skin during treatment period ( t0t8 ) : differences were significant for visits t3 - t6 ( p < 0.02 , fishers exact test ) in favour of silymarin - based treatment ( l : leviaderm ; soc : standard of care )  . abbildung 1 : rtog - hauttoxizitts - score whrend der gesamten behandlungsperiode ( t0t8 ) : unter silymarinbasierter prophylaxe kam es signifikant seltener zu akuten hautreaktionen in den behandlungswochen t3 - t6 ( p < 0 , 02 , fishers exact test ) , ( l : leviaderm ; soc : standard of care )  . results a total of 101patients enrolled in this prospective trial were evaluable . 
 however , from visit t3 to visit t6 , the proportion of patients assessed as normal was markedly higher with leviaderm compared to soc ( figures 1 and 2 )  . 
the findings showed also significant benefit for leviaderm over soc during rt and follow - up ( t3t7 ; p < 0.004 ; table 2 and figure 3 )  . 
silymarin - based cream in the treatment of radiodermatitis leviaderm previous studies [ 21 ] have tried to identify factors associated with an increased risk of acute radiation - induced toxicity . 
es ergab sich ein signifikanter vorteil ( t3t7 , p < 0 , 004 , t - test ) fr die silymarinbasierte hautpflege gegenber der standardpflege ( soc )  . no side effects were documented during treatment with either leviaderm or soc . 
despite this demonstration of clinically significant activity of leviaderm , the results may be related to several factors , such as the different regimen of supportive treatment and the unblinded , nonrandomized study design . discussion the reaction of the skin to ionizing radiation is highly complex and depends on numerous radiation - related , treatment - related , and patient - related factors . 
 nevertheless , during postoperative radiotherapy 8090% of patients develop some degree of inflammation symptoms , such as erythema , dry or wet desquamation , skin folds , pitting , or edema . 
in severe cases , painful ulceration or necrosis may occur . modern radiation techniques , especially photon beams of higher energy , decreased skin dose , and improved dose - homogeneity , provide better normal tissue protection [ 5 , 11 , 16 ]  . 
 clinically the emphasis has been made on developing fractionation schedules , immobilization procedures [ 21 ] , and radiation techniques [ 14 , 25 ] , e.g. , 3d conformal therapy and intensitymodulated radiation therapy ( imrt ) , allowing the avoidance of hotspots [ 5 , 12 , 23 , 39 ]  . 
despite these technical innovations , acute radiodermatitis still represents an important skin toxicity factor , as it may cause important loss of life quality and patient compliance [ 36 ] with a potential negative impact on rt treatment efficacy [ 6 ]  . up to now guidelines [ 32 ] do not recommend any prophylactic agents to prevent radiodermatitis . 
therefore , in our department local standard of care ( soc ) treatment consists of interventional recommendations . all further recommendations are discussed controversially in the literature [ 3 ]  . 
data from comparative studies did not demonstrate any preventive effect using hydrophilic emulsions with or without any additional topicals like trolamine , sucralfate , theta crme , or aloe vera [ 9 , 13 , 22 , 29 , 32 ]  . 
therefore , we conducted our study in a prospective schedule , comparing effects of local skin care weekly before , during , and 4weeks after irradiation ( table 1 )  . there is evidence that antioxidative and anti - inflammatory topicals like calendula and corticosteroids may have preventive effects in skin care [ 15 ]  . 
in this randomized trial , 30% of patients found calendula difficult to apply due to its more solid consistence and was not recommended at the end [ 26 ]  . 
silymarin - based cream in the treatment of radiodermatitis two smaller observational reports demonstrated [ 1 , 2 ] initial promising results using silymarin - based cream in breast cancer patients compared to historical toxicity data . 
studies demonstrated that silymarin induces the stimulation of the synthetic rate of ribosomal rna ( rrna ) species by stimulation of polymerasei and rrna transcription , protecting the cell membrane from radical - induced damage and blockage of the uptake of toxins such as alpha - amanitthese mechanisms lead to an increase of superoxide dismutase ( sod ) activity of lymphocytes and erythrocytes , as well as to the expression of sod in lymphocytes . 
silymarin has also been shown to increase patient serum levels of glutathione and glutathione peroxidase and consecutively reduce inflammation processes [ 8 , 20 , 31 , 34 , 35 ]  . our observational results confirmed the beneficial effects of silymarin - based cream in reducing the rate of objective and subjective skin toxicity . 
these results , reaching statistical significance , were congruent to the subjective toxicity assessment of patients using the vas score and supported the high radioprotective effect of silymarin - based cream . in addition , the therapeutical effect of silymarin - based cream was superior compared to soc . 
it can be further stated that the silymarin - based cream was well tolerated and can , thus , be used over several weeks . conclusion prophylactic use of silymarin - based cream was associated with both a significant decrease in the duration of grade 2 / 3 dermatitis and in the maximum severity of dermatitis compared with standard of care treatment . 
despite the fact that the prophylactic treatment of silymarin - based cream is different from the recommended practice to use soc topically for supportive treatment after first signs of skin inflammation , the results of this trial show silymarin - based cream to be a promising candidate for a safe prophylactic treatment option of radiodermatitis . 
 in our study , over 100patients were prospectively and continuously monitored , which support the significance of our results ; however , we are aware that data from nonrandomized studies have to be proven in further randomized trials . 
this component is highly qualified to be tested in larger multicenter studies in this setting . acknowledgment the study was supported by the company rottapharm / madaus with regard to study documentation . case study erlotinib - induced rash spares previously irradiated skin irene m . 
vonk1 background : erlotinib is an epidermal growth factor receptor inhibitor prescribed to patients with locally advanced or metastasized non - small cell lung carcinoma after failure of at least one earlier chemotherapy treatment . 
 key words : erlotinib non - small cell lung cancer radiotherapy skin rash strahlenther onkol 2011 ; 187 : 499501 doi 10.1007 / s00066 - 011 - 2232 - 8 bei zuvor bestrahlter haut bleibt der erlotinib - hautausschlag aus hintergrund : erlotinib ist ein epidermaler wachstumsfaktorrezeptor - inhibitor , der bei patienten mit lokal fortgeschrittenem oder metastasiertem nicht - kleinzelligen bronchialkarzinom und progress nach mindestens einer chemotherapeutischen behandlung eingesetzt wird . 
etwa 75% der mit erlotinib behandelten patienten entwickeln akneiforme hautvernderungen . fallbericht : wir beschreiben einen patienten mit nicht - kleinzelligem bronchialkarzinom , der drei monate nach abschluss einer simultanen radiochemotherapie mit erlotinib behandelt wurde . 
diese interaktion sollte jedoch weiter erforscht werden , da die anzahl der patienten , die mit einer kombination beider therapiemethoden behandelt werden , stetig zunehmen wird und der therapeutische effekt von erlotinib im bereich vorbestrahlter lsionen prtherapeutisch besser abgeschtzt werden knnte . schlsselwrter : erlotinib nicht - kleinzelliges bronchialkarzinom strahlentherapie hautausschlag 1 department of radiation oncology , radiotherapeutisch instituut stedendriehoek en omstreken ( riso ) , deventer , the netherlands , 2 department of lung diseases , deventer hospital , deventer , the netherlands , 3 department of dermatology , deventer hospital , deventer , the netherlands . received : october 19 , 2010 ; accepted : april 18 , 2011 published online : july 25 , 2011 strahlenther onkol 2011 no . 
erlotinib - induced rash spared previously irradiated skin introduction erlotinib is an epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitor prescribed to patients with locally advanced or metastasized non - small cell lung carcinoma ( after failure of at least one earlier chemotherapy treatment ) or with pancreatic cancer . 
the exact etiology of the rash is unknown ; however , it is suggested that the inhibition of the egfr in basal epidermal keratinocytes and the outer root sheath of the hair follicle leads to growth arrest and subsequent inflammation . 
 areas with a high density of these cells ( pilosebaceous units in the head and upper body ) are frequently affected , whereas locations devoid of such appendages ( palms and soles ) are uniformly spared [ 6 ]  . case report a 46 - year old male , ex - smoker presented with complaints of cough and fatigue that did not respond to an initial course of antibiotics . 
computed tomography ( ct ) imaging revealed a 7 - cm mass in the right upper lobe that invaded the mediastinum and caused severe compression of the superior vena cava ( figure 2a )  . 
whole body positron emission tomography - ct showed abnormal metabolic activity in the primary mass , but no evidence of regional lymph node or distant metastasis ( figure 2b )  . 
computertomogramm des thorax ( a ) und positronen - emissions - computertomogramm ( b ) zeigen eine 7 cm groe masse mit pathologischer metabolischer aktivitt im rechten lungenoberlappen , die in das mediastinum eindringt und eine schwere kompression der vena cava superior verursacht . cava superior syndrome , this patient with a clinically stage iiib ( ct4n0m0 ) was treated with concurrent chemotherapy and radiotherapy with a dose of 63 gray ( gy ) in 35 fractions ( figure 3 ) and weekly carboplatin and paclitaxel . 
 treatment with erlotinib ( tarceva ; roche the netherlands ) was started , and after approximately 2 weeks he developed a typical acneiform rash on the face , trunk , and upper extremities . 
 discussion some other cases have been reported of patients with sparing of rash in previous irradiated skin [ 8 ] and several explanations for the rash - sparing mechanism have been proposed . 
the epidermal sensitivity to egfr inhibitors might be modified in irradiated areas due to egfr hyperexpression and the abnormality of transforming growth factor 1 associated with late radiotherapy changes [ 1 ]  . 
irradiation of the skin causes a lack of hair follicles and sebaceous glands in the radiation field [ 2 ] , and these changes might explain the absence of rash in previously irradiated areas . 
 another explanation could be a transient immunosuppression due to loss of langerhans and other immunocompetent cells might be causing the absence of lesions in previously radiated skin [ 5 ]  . conclusion the exact mechanism of erlotinibinduced rash sparing in previously irradiated skin seems to be unclear . 
the underlying mechanism of this phenomenon needs to be explored further because the numbers of patients treated with combinations of both therapeutic modalities is increasing [ 3 , 4 , 7 ] and the efficacy of erlotinib against lesion irradiated before the administration of erlotinib needs to be assessed . 
 original article dose escalation for patients with decreasing psa during radiotherapy for elevated psa after radical prostatectomy improves biochemical progression - free survival results of a retrospective study alessandra siegmann1a , dirk bottke2a , julia faehndrich1 , gunnar lohm1 , kurt miller3 , detlef bartkowiak2 , thomas wiegel2 , wolfgang hinkelbein1 purpose : the optimal dose for salvage radiotherapy ( srt ) after radical prostatectomy ( rp ) is still not defined . 
in a multivariate analysis , the total dose ( p = 0.017 ) , the re - achievement of an undetectable psa after srt ( p = 0.005 ) , and the infiltration of the seminal vesicles ( p = 0.049 ) were independent parameters of bned . conclusion : our analysis suggests that patient selection during srt for a dose escalation to 70.2 gy can improve the freedom from biochemical progression in patients with srt after rp . key words : prostate cancer radical prostatectomy salvage radiotherapy dose escalation strahlenther onkol 2011 ; 187 : 46772 doi 10.1007 / s00066 - 011 - 2229 - 3 eine dosiseskalation bei patienten mit psa - abfall unter einer salvage - strahlentherapie nach radikaler prostatektomie verbessert das biochemisch progressionsfreie berleben ergebnisse einer retrospektiven untersuchung ziel : die optimale dosis der salvage - strahlentherapie ( srt ) nach radikaler prostatektomie ( rp ) ist derzeit nicht definiert . 
in der vorliegenden arbeit wird die bedeutung des psa - abfalls unter laufender srt als selektionskriterium fr eine dosiserhhung auf 70 , 2 gy untersucht . patienten und methode : zwischen 1997 und 2007 wurden 301 patienten mit prostatakarzinom nach radikaler prostatektomie an der charit universittsmedizin , campus benjamin franklin , berlin , einer srt unterzogen . 
der einfluss dieser selektion mit der erhhten gesamtdosis auf die biochemische progressionsfreiheit ( bned ) nach srt wird analysiert . ergebnisse : die mediane nachbeobachtungszeit fr die gesamtgruppe war 30 monate , der mediane pr - srt - psa war 0 , 28 ng / ml . 
die berechnete bned nach 2 jahren war 74% fr die aboth authors contributed equally to the manuscript 1department of radiation oncology , charit universittsmedizin , campus benjamin - franklin , berlin , germany , 2department of radiation oncology , university hospital , ulm , germany , 3department of urology , charit universittsmedizin , campus benjamin - franklin , berlin , germany . received : october 11 , 2010 ; accepted : april 8 , 2011 published online : july 22 , 2011 strahlenther onkol 2011 no . 
charakteristika der 301 studienpatienten ( prozentstze bezogen auf die behandlungsgruppen )  . introduction radical prostatectomy ( rp ) is a first - line therapeutic option for patients with prostate cancer . 
for pt3tumors , it occurs in up to 50% of patients without and 70% of patients with positive surgical margins [ 8 , 18 , 20 , 27 ]  . 
specifically for r1 - resected cases , adjuvant rt has been discussed [ 4 , 5 , 21 , 28 , 31 ]  . uncertainty remains whether a psa increase after rp indicates isolated local disease , distant metastatic progression , or both [ 23 ]  . 
it is , thus , of major importance to distinguish local recurrence from distant metastasis in these patients to select the optimal therapy [ 17 , 19 , 25 , 26 , 29 ]  . assuming a local disease , srt of the prostate bed has widely been used in the absence of biopsy - proven local recurrence . 
 conformal radiotherapy of the prostatic fossa with about 66 gy aims at the presumed local recurrence , reducing the risk of a 2nd wave of metastasis and clinical progression of disease [ 9 ]  . 
ct , mri , and bone scan were carried out in individual cases , but not systematically . one patient had an undetectable psa before salvage radiotherapy and was not excluded from the analysis . 
in pt2 - tumors , the planning target volume included the prostate bed , the bladder neck , and periprostatic clips with a security margin of 1 cin pt3a - tumors , the basis of the former seminal vesicles was included and in pt3b - tumors the bed of seminal vesicles was also included . 
side effects were scored using the radiation therapy oncology group ( rtog ) and the european organisation for research and treatment of cancer ( eortc ) late effect toxicity criteria . 
complete biochemical response was defined as a psa below the detection limits of the respective laboratory ( range , 0.030.1 ng / ml ; 0.05 ng / ml in > 90% of the analyses ) , biochemical failure was psa of 0.2 ng / ml above the post - rt nadir plus further rise . 
the time until psa failure was the time from the start of srt to the midpoint between the first two psa increases during or after srt . the probability of psa failure was demonstrated by kaplanmeier curves [ 13 ] with log rank test for statistical comparison . 
the cox proportional hazards regression model was used for multivariate analysis to determine and analyze factors that may influence biochemical progression - free survival [ 10 ]  . using all available psa values , we calculated psa doubling times by linear regression analyses of the log ( psa ) for each patient . 
after completion of srt , 154 of 301 patients ( 51.2% ) achieved a psa nadir in the undetectable range versus 147 ( 48.8% ) with a detectable psa nadir or a continuously rising psa from the start of srt . 
the calculated 2 - year bned for the group of patients with an undetectable psa post - srt nadir was 90% and for the group with persistent detectable psa 41% ( p < 0.0005 ; figure 2 )  . univariate analysis of factors influencing bned after srt for all patients showed that seven out of eleven preradiotherapy factors were statistically significant predictors of outcome . 
bei 154 patienten war der psa - wert unter der nachweisgrenze , bei 147 blieb er im messbaren bereich . ( figure 2 ) and depending on the resection status ( figure 3 ) illustrate these findings . concerning acute and late side effects , no significant differences were observed between dose levels . 
no acute side effects of grade 3 or 4 were recorded ; however , 12patients ( 4% ) had rt - induced chronic complications grade 2 , 6patients ( 2% ) had complications associated with rectal symptoms ( grade 2 bleeding , tenesmus ) , 2patients had grade 2 ( transient ) cystitis , 4patients ( 1.3% ) had grade - 3 late cystitis , and 6patients ( 2% ) developed urethral stricture . discussion numerous retrospective studies describe the outcome of patients treated with salvage rt for either persistent or increasing psa following rp [ 1517 , 25 , 32 ]  . 
in the second investigation ( n = 364 patients ) [ 2 ] , three doses levels ( < 64 gy , 6466 gy , and 70.2 gy ) were investigated retrospectively . 
in our investigation , the patients were additionally selected with respect to a decreasing psa during rt , thus , giving the chance of avoidance of an overtreatment . differences in the definition for progression after srt [ 1 , 7 , 25 , 26 ] hamper direct comparisons between studies . 
here , we refer to a psa value of 0.2 ng / ml as recommended after a multi - institutional analysis based on over 1 , 500 patients [ 25 ]  . srt is generally associated with a low rate of severe acute and late side effects . 
urinary incontinence in 05% of the cases , moderate proctitis in 010% , and mild to moderate cystitis in up to 10% may result from this procedure [ 15 , 25 , 32 ]  . 
8 progression after rt ( logistic regression ) achieving undetectable psa post - rt ( logistic regression ) progression - free survival ( cox regression ) n.s. siegmann a , et al . 
vergleich von studien ber die gesamtdosis bei der srt . number of patients median follow - up ( months ) definition of biochemical relapse anscher 2000 [ 1 ] macdonald king 2008 [ 14 ] pisansky 2000 [ 19 ] 0.3 ng / ml 10% gain be2003 [ 15 ] 0.3 ng / ml > 60 > 0.1 ng / ml tween 2 consecutive measurements 50% after 4 years rate of biochemical relapse probability for freedom from biochemical failure median psa before rp median psa before rt resection status r1 median rt dose pt3b dose response relationship 46% after 5 years 17 ng / ml 0.9 ng / ml 64 gy > 64 gy 18 ng / ml 1.4 ng / ml 66 gy > 65 gy 45% after 5 years 25% ( 60 gy ) vs . 
 ( 3 ) in a large number of patients ( including r1 cases ) irradiation commenced when the psa level was < 0.2 ng / ml , thus , indicating a potential overtreatment in some patients with possibly benign nature of low level , gradual psa recurrences . 
therefore , the decision to offer radiation therapy should be balanced against its potential side effects . in conclusion , we could establish the new information that patients with decreasing psa during srt after rp should have a better outcome after receiving 70.2 instead of the standard 66.6 gy and should have a chance of a long - term durable response with no further treatment required . 
no such study has been published , so far . strahlenther onkol 2011 ; 187 : 513540 doi 10.1007 / s00066 - 011 - 1002 - y 15th annual meeting of the scientific association of swiss radiation oncology ( sasro ) abstracts from the march 31 april 2 , 2011 geneva , switzerland congress president : r . 
randomization was between control arm ( ca ) 25x2 gy / 5 weeks by tangential fields on breast / chest wall , plus supraclavicular - axillary field if node - positive , and sequential boost 8x2 gy weeks if bcs ( cumulative dose 66 gy / 7 weeks ) , versus experimental tt arm of 15x2.8 gy / 3 weeks , including nodal areas if n + , and sib of 0.6 gy if bcs ( cumulative dose 51 gy / 3 weeks )  . results : by february 2010 , 70 patients had a minimum follow - up of 3 months , 32 in ca ( 20 bcs , 12 ma ) , 38 in tt arm ( 23 bcs , 15 ma )  . 
treatments were evaluated in terms of safety and comfort for the patient , therapy effectiveness and efficiency and simplicity for the operators . results : the target coverage of all accepted plans was passing the criteria v99% > 95% of the prescribed dose . 
all treatments were successfully completed in 15 minutes ( from patient entrance to exit the bunker ) including all the igrt phases ( positioning , mvct scan , registration , position correction in the 3 dimensions + roll ) without extra actions from mtras , compared to helical irradiations ( th )  . 
some patients received the therapy with both the td and th techniques ( re - irradiation or boost ) and they have not noticed differences perceived in terms of delivery , positioning , comfort . conclusion : td is a useful option that combines non rotational imrt with the full integrated igrt tools of the hiartii system . caparrotti f , laouiti m , tudisco - pillet p , weber dc radiation oncology , geneva university hospitals ( hug ) objective : to assess qol after treatment of patients presenting brain metastases with wbrt ( 30 gy ) + sib ( 40 gy )  . materials and methods : between march and december 2010 , 30 patients with 1 to 4 brain metastases , were treated with wbrt + sib using volumetric modulated arc therapy ( ra ) in a prospective study . 
however , we noticed a significant improvement of gs , fu , md , cd , fa and gh scores in 4 ( 44% ) patients with a 7 months follow - up . 
endpoints were lung v20 , spinal cord maximal dose and mean heart dose . results : in 1 / 14 patients ( 7% ) , no difference between respiratory phases were found suggesting an absence of benefit of gating . 
aim of the study was to investigate the influence of different air filling in lungs on the acuros xb algorithm . materials and methods : ct datasets from 10 breast patients acquired in both free breathing ( fb ) and deep inspiration breath hold ( dibh ) conditions were selected . 
an analysis was performed in terms of dvhs and of 3d index evaluation , in particular within the low density mediuas a further comparison , anisotropic analytical algorithm ( aaa ) was used for dose distribution calculations . 
plans were created for 6mv beams from a clinac 2100ix equipped with mlc - 120 millenniuthree modalities were analysed : 3d - crt : 4 - 5 fields , no - one entering from contralateral lung . 
 imrt : 6 fields , no - one entering from contralateral lung . rapidarc : 2 partial arcs , no - one entering from contralateral lung . to distinguish between differences coming from the different management in heterogeneity , to those from the algorithm per se , all the plans have been recalculated assigning to the patient outline the water material with hu = 0 . 
ptv dose difference was differentiated between the target in soft tissue , where the mean dose was found lower of about 2% for acuros xb , and the target in lung tissue , where the mean dose was higher of about 1% . 
dvh parameters such as v ( dref ) , v ( 1.5xdref ) , d ( ptv , 50% ) , and d ( skin , 0.5ccm ) as well as quality indices ( dnr , dhi , ci ) of the plans generated with tg43 and mc have been determined and compared . results : dose calculations based on tg43 overestimate v ( dref ) and d ( ptv , 50% ) as compared to the mc calculations by up to 2% and 3% , respectively . 
by taking into account the lack of scattering volume at the skin surface in the mc dose calculations up to 6% lower maximal skin doses d ( skin , 0.5ccm ) are observed compared with tg43 based dose calculations . conclusion : the mc - based brachytherapy dose calculations within the smcp highlight limitations in dose prediction of todays treatment planning systems , based on the tg43 formalism , for hdr brachytherapy of partial breast irradiation . 
verification plans were compared with measurements carried out with the delta4 phantothis comparison was performed in terms of a gamma evaluation using 3% / 3 mm criteria . results : dvhs for the patients showed good agreement between smcp and acurosxb calculations regarding median , mean and standard deviations for all outlined structures . 
for verification plans on average 94% and 99% of the points fullfil the gamma criteria for the dose calculted using acurosxb and smcp , respectively . conclusion : acurosxb showed good agreement with smcp regarding the dose distributions for vmat h&n plans . 
 results : level i , ii , iii evidence has been published for the benefit of combined ht and radiotherapy ( rt ) + / chemotherapy ( ct ) in patients with cervical , vaginal and bladder cancer . 
in two other studies , adding ht to rt improved cr rate from 57% to 83% in one study , and 3 - yrs os from 67% to 94% in another . 
we present a detailed evaluation of ed over 3 years f / u in a total of 331 pts treated at our institution . materials and methods : patients were evaluated by a swiss multi - institutional f / u protocol prior to and at 6 weeks , 6 , 12 , 24 and 36 mths after seed implantation . 
 materials and methods : treatment planning was performed for 7 patients using 4 photon beams of truebeam linear accelerator ( varian medical systems ) : 6 and 10 mv beams with ( x6 and x10 ) and without ( x6fff and x10fff ) flattening filter . 
either one or two 360 arcs with maximum dose rate of 600 mu / min for flattened beams , and 1200 mu / min for fff beams were used , respectively . results : no difference was detected between the 4 beams with respect to ptv coverage , conformity and homogeneity . 
for plans using a single arc , treatment time was reduced by 35% ( 2sd = 10% ) , when using fff beams . conclusion : fff beams resulted in dose distributions similar to flattened beams . 
gallen , ch objective : interruptions during the course of radiotherapy are a relevant probleoften the number of days left , including the weekends , does not allow for an equivalent compensation . 
we developed an android based tool for the calculation of the compensatory daily dose based on existing guidelines . materials and methods : the developed java tool runs on mobile devices running the google android operating systethe tool is based on the classic model - controller - view model . 
the formulas recommended by the royal college of radiologists ( rcr ) were used as a basis for the calculations . results : the android based tool could be developed within several days and provided the option of entering the already applied treatment , the original prescribed treatment and the days left for compensation . 
additionally the tool calculated the expected influence on late effects of normal tissues in percent based on a comparison of bed3 values for the new proposed treatment and the originally planned treatment . conclusion : the feasibility of development of a custom java based android compatible tool was proven . 
 materials and methods : seven cases for four groups of tumors were evaluated prostate tumors ( planned with ra ) , vestibular schwannoma tumors ( ra and imrt ) , small intra - cranial tumors ( target volume < 5cm3 , ra and imrt ) , head and neck tumors ( imrt )  . 
treatment plan comparison were carried out using monitor units ( mu ) , dose - volume histogram parameters , homogeneity index ( hi ) and conformity / gradient index ( cgi , cgic and cgig ) [ wagner et al , ijrobp 2003 ]  . results : for the prostate plans as well as the vestibular schwannoma plans , no significant difference was observed between the 2 mlcs for all parameters used for the evaluation . 
using gafchromic films at three planes through the phantom , 4 co - planar field impt and distal edge tracking ( det ) plans have been delivered to a volume simulating a skull base chordoma . 
for range error treatments , measured distributions ( for + 3% and - 3% ) were subtracted and compared to a model for predicting potential delivery errors in the treatment planning systeagreement between films and the model was excellent , being the det plans somewhat more sensitive to range errors than the impt plans . 
 conclusion : using this new phantom , impt plans resulted to be more precisely delivered than det plans , and the effect of range errors have been measured for the first time . 
dose recalculation of the nominal plans has been performed on these modified ct data sets , and the resultant dose distributions compared to the nominal plans . results : although reduced filling leads to local dose overshoots , and increased filling to under - shoot , the changes in the dvhs for ctv and oars were not found to be significant ( < 5% )  . 
however cold and hot spots ( up to 50% when the two extreme scenarios are compared ) were observed , particularly behind the cavities , these were generally located in non - critical normal tissues . conclusion : this study implies that even major changes in the nasal cavity filling may not affect proton plan quality as much as may be expected . 
an end to end test including mri , ct , fusion of ct and mri , contouring , planning , setup with kv image pairs and treatment delivery was performed on a dedicated phantom to determine overall accuracy of the complete treatment cha to investigate intra - fractional motion in the mask system , 13 fractionated stereotactic patients received preand post - treatment cbct for a total of 65 fractions . 
 results : isocenter sphere radii were measured : 0.28 mm ( + / - 0.18 mm ) for couch rotation , 0.31 mm ( + / 0.08 mm ) for collimator , 0.42 mm ( + / 0.21 mm ) for gantry and 0.25 mm ( + / 0.15 mm ) for kv imager rotation . 
shifts during treatment in longitudinal and lateral direction were nonsystematic ; however we observed a systematic shift of - 0.5 mm ( + / 0.4 mm ) in vertical direction . 
 results : fourteen of the 22 patients received the prescribed dose of 45 gy in 15 fractions of 3 gy , two patients received a total dose of 60 and 45 gy with a combination of two different beams ( photons and neutrons ) , in 5 cases the daily fraction was modified to 2 gy because of bad tolerance and one patient died due to serious intracranial hypertension after 2 fractions of 3 gy and one of 2 gy . 
in contrast to the linear quadratic ( lq ) model , only one alphavalue is used to describe both , apoptotic and non - apoptotic cell death . results : the proposed ldhsmodel is fitting the data from harrigan et al . 
the model shows a dose rate dependency comparable to more advanced lqbased models using dose protraction factors or the lplmodel of curtis , but with different low and high dose rate limit for the survival curve . conclusion : a broad spectrum of observed radiobiological phenomena can be modelled by one unique approach . 
clonocgenic assays were performed to determine the effects of different dose rates on the cellular survival and immunoblots were used to validate and quantify the differential activation of signaling pathways . 
furthermore , we show that independent of the dose rate , fff beams are more efficient in reducing clonogenic cell survival than the more commonly used standard flattened bea conclusion : this study provides promising results as to how dose rates impact on tumour cell survival . 
 materials and methods : du145 ( p53mut / mut ) and lncap ( p53wt / wt ) cells were irradiated with either photons or 138 mev protons at the middle of spread - out - bragg peak ( sobp ) or in the plateau region . 
 conclusion : the increased rbe of protons in du145 cells compared to the rbe values determined in lncap cells indicates that the genetic cellular background possibly affects the overall rbe . 
rbe values < 1 in lncap cells in the plateau region indicates a more efficient repair of sublethal dna damage and possibly suggests that protons in the plateau region induce a different form of dna damage compared to the sobp . 
western blot data show reduction in y1003 phosporylation and co - immunoprecipiations suggest decreases in met binding to c - cbl and as well as met ubiquitination . conclusion : met inhibition by small molecules in cells with deregulated met strongly interferes with met downregulation most probably by less ccbl mediated ubiquitination of met and leads to accumulation of met in the cell . 
radiation oncology , university hospital zurich , switzerland objective : the combined treatment modality of ionizing radiation ( ir ) with microtubule stabilizing agents ( msa ) results in supra - additive tumor growth inhibition . 
here we investigated deregulation of matrix metalloproteinase ( mmp ) activity , as an important component of the tumor microenvironment , by the combined treatment modality of ir with the clinically relevant msa patupilone materials and methods : experiments were performed with human fibrosarcoma and glioblastoma tumor cells . 
the cell invasive capacity of the ht1080 and u251 cells was increased after irradiation with 2 gy by 30% and 50% , respectively and patupilone treatment completely abrogated ir - induced cell invasion . 
 furthermore , sirna depletion of timp - 1 or timp - 2 prevented ir - mediated induction of mmp activity and cell invasion to the same extent as pretreatment with patupilone . conclusion : these results indicate that patupilone counteracts an ir - induced mmp activation process by the reduction of secreted timp - 1 and timp - 2 proteins , required for activation of mmps . 
films were then scanned 18 hours after irradiation , and calibration curves between grey levels ( gl ) and dose were obtained for the different sobp extent and positions along the proton curve . results : within each stack , calibration curves well overlap for all the analyzed depths ; superimpositions were within the experimental error ( 1.5% in dose and 1% in lg )  . 
similar agreements were obtained comparing curves coming from stacks irradiated with different sobp extent ; in this case differences in lg are about 2% . conclusion : our investigations show that a calibration curve is independent from the position of the film within the sobp curve and from sobp extent . 
in this study , a planning strategy to overcome these limitations is proposed and evaluated . materials and methods : rapidarc ( ra ) plans for 6 breast cancer patients , were optimised on the original ct ( o ) and on an expanded one ( e ) , where body in the breast region and ptv were extended in air ( tissue hu assigned )  . 
from dose distributions and dvhs , it is evident that eo approach allows to irradiate the expanded target region as usually achieved in the past with skin flashing of treatment fields ; this would account also for intrafraction movements . 
gallen , switzerland1 objective : permanent in - vivo verification during imrt - irradiation is the purpose of the david - systeintroducing such a system into the daily routine requires the knowledge of its limits which are studied in this work . materials and methods : the david system , a multiwire ionization chamber , consists of 40 detection wires positioned exactly in the projection line of a leaf pair producing a signal proportional to the ionization density along this wire . 
the david system has been used on more than 50 patient fields with step - and - shoot imrttechnique of different clinical targets . results : regular imrt - segments are applied with leaf pair openings between 0.5 cm and 10 cm and 1 to 12 mus . 
of radiation - oncology ( maastro ) , grow ( school for oncology & developmental biology ) , maastricht university medical centre ( mumc ) , maastricht , the netherlands ; 2clinic and policlinic of radiationoncology , university hospital zurich ( uhz ) , switzerland ; 3dept . 
of neurosurgery , maastricht university medical centre ( mumc ) , maastricht , the netherlands purpose : to analyze the long - term results in terms of efficacy of patients with a meningioma treated with fractionated stereotactic radiotherapy ( scrt )  . patients and methods : seventy - two patients treated with fractionated stereotactic radiotherapy between 1996 and 2008 at maastro clinic ( n = 45 ) and in zurich ( uhz ) ( n = 27 ) were included . 
patients received scrt either as primary treatment ( n = 46 ) , as an adjuvant therapy following a subtotal resection ( n = 19 ) or for recurrent tumours after a complete primary resection ( n = 7 )  . 
progression - free survival for benign ( grade i ) meningiomas was 95% at 3 years and 95% at 5 years , and 40% for atypical meningiomas at 3 years . 
significant growth ( = smallest detectable difference outside measurement error ( sdd ) ) was defined as a volume change of 19.7% or more , as calculated in a previous study ( 1 )  . results : the 4 - year clinical control probability was 96 , 4% ( 0 , 03 ) , the 4 - year radiological control probability was 85 , 4% ( 0 , 1 ) ( median follow - up 40 months )  . 
no prognostic factors were found regarding vs swelling or growth . conclusion : using volume based assessment , good radiological and clinical control rates were observed but a lower rate of radiological control attributed to the more sensitive and more accurate volume measurements . 
we aimed to identify an appropriate method for matching planning ct - images with cbct images for prostate irradiation . materials and methods : cbct images of 86 patients were assessed . 
translational position errors calculated after cbct images acquired on the first treatment day with a routinely applied clip box ( rcb ) were re - assessed and matched for gray ( gv ) as well as for bone ( bv ) values . 
the clip boxes measured 7x6x8 cm , 9x8x8 cm and 13x22x8cm for rcb , mcb and lcb respectively . results : the calculated translational positioning error was under 0.3 cm in 52% up to 97% of patients , depending clip box definition , matching method and axis . 
between may 1988 and may 2007 , 110 patients , median age 3.6 years ( range , 1 months - 15.3 years ) , with brain tumors were treated with surgical intervention and conventional chemotherapy . 
on multivariate analysis , the presence of mri - abnormalities was an independent prognostic factor for overall survival . conclusion : mri - detectable brain abnormalities are common early findings in children treated with high - dose busulfan - thiotepa followed by radiation therapy , and may mimic early tumor recurrence . 
 material and methods : all patients treated between jan 2003 and july 2009 with radiosurgery ( single - fraction ( srs ) or hypofractionated radiosurgery ( srt ) ) for bm at maastro clinic were selected . 
patients with a short survival ( < 3 months ) were more likely to have heterogeneous - enhancing bm and were less likely to have rim - enhancing bm ( p = 0.03 ) , suggesting worse prognosis for heterogeneous bm . 
 conclusions : based on 3d - volume assessment on continuous imaging , increasing volume of metastatic disease and the pattern of contrast enhancement were found to be worse prognostic factors for survival . 
 materials and methods : it will be shown , in which way shift parameters and patient - specific characteristics , which are daily recorded influence the image - frequency and the entire treatment series . 
based on the two examples ( breastcancer and prostatecancer ) we show how igrt is daily practiced , documented and discussed in the plenu results : clinical experience shows that in the case of breast treatment matching to the sternum is to be preferred to match to the spine . 
after applying the couch shift , an additional mv image is taken , the visual markings on the test object are compared to the room lasers , and the absolute couch positions are evaluated . 
this method can be considered as an end - to - end test of the systems involved in patient positioning ( lasers , kv source and imager , matching , couch shift ) , and a check of the kv and mv isocenter . 
we measured the distances between contour of the breast and the medial border of treatment field at 3 levels : dbmax , at maximal convexity of the breast ; dbsup , at the superior quarter of the field ; dbinf , at the inferior quarter of the field . 
 materials and methods : since september 2010 based on clinical examination taking into account the breast volume and mobility of the patient , double simulation is performed in our department in prone and supine position for radiotherapy planning for breast conserving treatment . 
we used a 4 - itemed questionaire for pain , nervousness , anxiety , and discomfort , scored from 0 for no symptoms , 1 mild , 2 moderate , to 3 severe symptoms . 
before simulation , 1 patient had no symptoms , 11 had at least 1 symptom : pain was present by 5 patients , nervousness by 8 , anxiety by 5 , and discomfort by 6 . 
setup portal images , including open and compensation fields , were retrieved using the varian offline review systecentral lung distance ( cld ) were measured on intern and extern fields . results : a total of 796 portals were retrieved in this first review round . 
our aim was to identify the benefits and challenges of this new streamlined practice . materials and methods : patients received a single radiation therapy appointment in which both simulation and treatment was performed . 
the radcalc program was used to calculate daily monitor units for all treatment fields and remaining data was entered into a record & verification system including setup notes , daily fractionation doses and imaging protocols . 
on average , we required 45 minutes to perform the entire set - up , simulation , calculation and treatment . conclusions : our initial clinical experience demonstrates that online simulation and treatment is a feasible and proficient solution , replacing our conventional simulation process . 
respiratory tracking was utilized for all mediastinal volumes . results : on average 8.0min ( 1sd = 2.9min ) were required for patient setup in the roo for kv paired images we needed 3.8min ( 1sd = 1.8min ) for both acquisition and match procedures . 
during the last 10 years this knowledge has been transferred to the extracranial stereotactic radiation delivery , better known as stereotactic body radiation therapy ( sbrt ) ; this newer treatment option has emerged as a highly accurate and effective dose delivery for vertebral metastases , futhermore for intradural tumors and metastases or paraspinosous tumors . 
sbrt may be composed of imrt fields and dynamic arcs . materials and methods : 38 patients with 40 isocenters for sbrt are evaluated using iplan ( brainlab ) for treatment planning and novalis tx ( varian ) for treatment delivery . 
all patients have been immobilized with the aid of different utilities : bodyfix vacuum cushion with and without coversheet ( medical intelligence medizintechnik ) vacfix vacuum cushions ( par scenitific ) and ct - step ( sinmed )  . results : the application flow for the therapy as well as the advantages and disadvantages of each positioning device be presented with special regard to the stability and reproducibility of the repositioning as well as the comfort for the patients . conclusion : our experiences suggest that there is no one size fits all solution . 
we therefore performed time and accuracy studies to evaluate potential advantages of the truebeam . materials and methods : all patients were immobilized using a brainlab mask systepatients were treated either using a vmat or an imrt technique . 
for each fraction the time needed for preparation , imaging and treatment was collected using a matlab progra results : intrafractional motion was found to be below 1.1mm for all patients for all treatments . 
shifts during treatment in longitudinal and lateral direction were non - systematic , however we observed a systematic shift of - 0.5mm ( 2sd = 0.4mm ) in vertical direction , which is likely related to the sagging of the patient in the mask . 
with the leksell gamma knife perfexion ( elekta ab , sweden )  . the multidisciplinary gk team involves neurosurgeons , radio - oncologists , physicists , neuroradiologists , nurses and technologists , aiming at a full integration for optimal patient management . 
all the steps in the treatment process ( leksell coordinate frame fixation , imaging , planning , treatment ) are supervised by the members of the multidisciplinary teain our experience , radiotherapy technologist ( rtt ) have acquired an important role in the multidisciplinary team communication and integration . 
specifically , the rtt are responsible of : supervision of the image acquisition , performing the gamma knife unit control tests , patient setup , and patient surveillance during treatment . 
 with the help of a robotic chair and an led ( to determine the gazing angle ) , the eye is positioned vis - - vis the central axis of the collimated p + - beam according to the treatment plan . 
the protons are accelerated in a dedicated cyclotron and are guided in a beam line to the treatment facility . results : positioning software calculates an appropriate position of the robotic chair and the led based on the clip positions indentified on the images . 
this cas results in 10 ects ( european credit transfer system ) of 30 hours each , meaning 300 hours ( 100 lessons hours + 200 of practicing ) , divided in 2 units of 5 ects each . results : development of specific proficiencies to an expert valuation level in radio oncological dosimetry field . conclusion : aim of this conference is to provide an information about one of the solutions for improving the post diploma training available for the radiation technologists . 
 materials and methods : we shall use as a starting point a short film created by the hug communications department ( pulsation ) following a patient through the stages of a bone marrow transplant , including tbi . 
our power point presentation will then discribe the indications and treatment procedures of tbi as well as the risks and potential side effects . results : the film and presentation will be projected in order to share our long experience with this often unfamiliar and poorly known radiation therapy technique . conclusion : tbi is a treatment modality with potentially severe side effects and must be performed according to strict procedural guidelines . 
the aim of this prospective study is to prevent and reduce side effects of adt and improve the quality of life ( qol ) in frail patients ( pts ) treated with rt and adt for localized pc . 
 materials and methods : inclusion criteria are : age > 75 years , cardiovascular and pulmonary comorbidities , mini mental state examination ( mmse ) < 25 , vulnerable elder survey ( ves - 13 ) 3 and / or unipodal position < 5 seconds . 
all pts completed at baseline and at regular follow - up charleston comorbidity index , european organization for research and treatment of cancer quality of life questionnaire ( eortc ) qlq - c30 , mmse and ves - 13 questionnaires . 
 conclusion : preliminary results obtained with first pts are encouraging and open the way to a new multidisciplinary approach in the management of frail pts treated with combined adt and rt . 
regarding acute toxicity ( at ) 10 patients presented a ctc 3 grade 1 skin toxicity at the end of treatment and 3 patients grade conclusion : for our experience in this new clinical application of advanced imrt technics in breast cancer treatment we found a good ptv coverage and a very good sparing of the organ at risk and normal tissue . 
gallen objective : we describe the diagnostic procedure performed during the workup of a patient with psa failure after r1 prostatectomy focusing on the prostate bed , pelvic lymph node and a suspicious bone lesion . materials and methods : a patient with prostate cancer ( pt3b pn1 ( 4 / 11 ) m0 g3 ) prostatectomy r1 . 
for the clarification of these lesion we performed a cholin - pet , a pelvic mri and a mdp - spect - ct . results : the pelvic mri revealed a local recurrence in the prostate bed , the other imaging modalities were false negative in this region on first diagnosing . 
due to its small size the osteolytic bone lesion could not be properly assessed with a state - of - the - art spect or cholin - pet - ct , with the mri this lesion could be reasonably judged as negative . conclusion : for complete staging in the postoperative setting for prostate cancer the combination of several modalities may be necessary to correctly stage the prostate bed , lymph node status and bone status . 
our aim was to review our own practice in the last 3 years . materials and methods : all patients who received a bone scintigraphy between 2007 and 2010 as part of their workup before postoperative radiotherapy were analysed . 
we retrospectively analysed the time since operation , the psa value at referral , the psa dynamic from the last measurement and the concurrent mri scan for local or lymph node abnormalities . results : various reasons lead to bone scintigraphies even though this typical criterion was not met in 13 patients . 
the reasons included : high initial psa , androgen suppression therapy , suspect lymph nodes on mri , large local recurrence , positive lymph nodes during operation , quick psa rise , over 5 years from last staging , high postoperative nadir and high postoperative psa . 
gallen , 9007 sankt gallen objective : safety and activity in the combination of radiotherapy with bevacizumab in recurrent malignant gliomas . materials and methods : patients in case of recurrence from malignant gliomas who failed to standard treatment received bevacizumab ( 10 mg / kg i.v. ) every two weeks until tumorprogression and a hypofractionate or normal fractionated radiotherapy . 
critical structures like the optic chiasm were excluded and the dose to the re - irradiated target volume was restricted to a cumulative dose of 110 gy of the first and second radiation course . 
this study presents a training tool for prostate delineation , based on ct and mri images , and a mathematical formalism developed for this purpose . materials and methods : at the beginning of this study , delineation rules have been compiled and discussed with the involved physicians as well as an mri specialist . 
but , since the investigated cases diverged in stage and image quality , a clear numerically proven progress is difficult to assess on the basis of only ten patients , however a positive trend could be observed . conclusion : numerically based training tools are suitable to measure the contouring progress in an objective manner . 
the dose to the foetus was calculated with the peridose program ( van giessen , 2001 ) and measured in an alderson phantom with tld - 100 discs ( thermo luminescence dosimeters )  . 
the patient case gave rise to develop a three component model ( 3cm ) to calculate the scattered dose for our elekta linac : the internal scatter is assumed to be proportional to the body integral of the dose , the external scatter with and without wedges are assumed to be proportional to the monitor units . 
since it presents a further dose to the patient and requires additional time , we examined if it is possible to reduce the number of acquisitions from a daily to weekly cycle in patients with small displacements in the first therapy week defined as displacement of 4mm and a st.dev. 
of 2mm in x - , y - , and z - axis . materials and methods : for 34 consecutive head and neck patients , fixed with a thermoplastic mask pretreatment cone beam ct have been acquired at a elekta synergy accelerator . 
the patient displacements have been recorded for at minimum five weeks in x - , yand z - axis ; the mean deviation in the first week after therapy start were compared to later deviations . 
in 18 out of 34 patients the mean deviations in the first treatment week gave no reliable information about displacements in the following weeks , so a patient specific positioning reproducibility was not given . 
one of these 6 pts received concomitant chemotherapy with weekly cisplatall the pts underwent a planning pet scan in the treatment position , using a lung board as immobilization device . 
all pts were checked with cone beam ct ( cbct ) at least once a week and kv set up controls ( orthogonal fields ) twice a week before rt sessions . 
no grade 2 - 4 acute , subacute and late toxicities were registered . conclusion : curative 4d igrt - hypofractionated schedule is feasible and well tolerated even in our experience . 
walking without crutches was possible aga a steady pain decrease was reported from 7 / 10 on the painscale before treatment , to 5 / 10 after treatment completion to 2 / 10 after 2 months and at 6 month - follow - up . 
medication with nsar was still needed because of backpain , only half of the dose was needed compared prior to the therapy . conclusion : surprisingly also in this patient with a long history of clinical symptoms and a local trauma a sustained pain control was achieved with these very low rt - doses . 
the patient was referred to our department and then percutaneously irradiated with 2 gy single dose 5 fractions per week up to a total dose of 28 gy in a three field technique using mixed photons ( 6x and 18x )  . 
we review the literature to evaluate the risk of skr after surgery . materials and methods : medline was searched for case series of invasive breast carcinoma with mention of skr published in 2000 - 2010 . 
data abstracted were : period , tumor stage , type of surgery ( breast conserving [ bcs ] , skin and / or nipple sparing mastectomy [ ssm ] , other mastectomy [ mast ] ) , follow - up , counts of skr and local recurrences ( lr , defined as breast or chest wall recurrence with or without skr ) , and risk factors associated with skr . results : 27 articles were retrieved for a total of 10722 patients . 
of radiation oncology and nuclear medicine , inselspital , university of berne , switzerland objective : there is an increasing evidence in the literature to omit elective nodal irradiation ( eni ) not only in patients with non - small cell lung cancer ( nsclc ) but also in patients with limited disease of small cell lung cancer ( ld - sclc )  . 
range of metabolic tumor volume 19 309 ccmajor increase of the ptv ( up to 32% ) in 4 / 31 ( 13% ) patients due to pet positive lymph nodes being inconspicuous in ct ( skip metastases )  . 
all patients had a base pain score of more than 2 with 0 being no pain and 10 being the worst pain possible with no or not little response to pain medication . 
follow - up forms to assess toxicity and pain reduction were completed by the patient at day 7 and day 14 after the first fraction and thereafter monthly for a 12 month period . 
four patients who were irradiated in the spine ( 1 ) and extremities ( 3 ) reported pain relief of at least 50% following re - irradiation already at day 7 or at the latest one month after without any severe acute toxicities . 
 conclusion : analysis of follow up visits and completed pain questionnaires show that reirradiation of painful bone metastases is not only possible but safe for symptomatic relief without any severe toxicity complications . 
this can easily be performed using simultaneous integrated boost ( sib ) applied in rapidarc technique . materials and methods : in our department we started to treat patients with a limited number of brain metastases giving hypofractionated rapidarc technique with simultaneous integrated boost with locally curative intention according to stereotactic radiosurgery . 
visible metastases ( ptv1 ) are treated with 15 times 4 gy ( 5 f / week ) , whereas whole brain ( ptv2 ) is irradiated with 15 times 1.8 gy according to prophylactic cranial irradiation ( pci )  . 
in a next step we try to avoid the hippocampus to reduce neurocognitive dysfunction . zilli t , peguret n1 , vees h1 , rouzaud m1 , dipasquale g1 , nouet p1 , buchegger f2 , khan hg3 , miralbell r1 departments of radiation oncology1 and nuclear medecine2 , geneva university hospital , and institute of radiology jean violette3 , geneva , switzerland objective : to report the clinical outcome in patients ( pts ) treated with salvage radiotherapy ( srt ) for biochemical relapse after radical prostatectomy ( rp ) according to a dose - escalated , target - guided approach . 
 materials and methods : data of 98 pts with biochemical failure after rp undergoing endorectal magnetic resonance imaging ( mri ) ( n = 95 ) , pet ( n = 3 ) or both ( n = 37 ) before srt were analyzed . 
univariate and multivariate analyses were performed for clinical - , pathological - , and treatment - related factors predicting for biochemical relapse - free survival ( brfs )  . results : 28 of 98 pts recurred after srt . 
 conclusion : our experience in this advanced imrt technique and image guided application for bone metastases showed a safe and feasible treatment with an optimal ptv coverage and a reduced toxicity , spearing the neighbouring organs at risk . 
walking without crutches was possible aga a steady pain decrease was reported from 7 / 10 on the painscale before treatment , to 5 / 10 after treatment completion to 2 / 10 after 2 months and at 6 month - follow - up . 
medication with nsar was still needed because of backpain , only half of the dose was needed compared prior to the therapy . conclusion : surprisingly also in this patient with a long history of clinical symptoms and a local trauma a sustained pain control was achieved with these very low rt - doses . 
the 3 yr duration hasnt changed , but the amount of theoretical background has increased : now consisting of 50% practical training by institutions of radiology , nuclear medicine & ro and 50% of theoretical education at the hf bzg . 
aim : to assess how well graduates are now trained to begin work in a ro department especially with enriched theoretical & diagnostic background of rapidly developing new technologies in ro and interdisciplinarity within the whole field of radiation based medicine . 
graduates interest in ro shall be assessed and how to possibly encourage more students to choose a career in this field . materials and methods : the concept of education of ro at bzg will be presented . 
 materials and methods : from septembre 2010 we simulated selected patients in the two positions according to volume of breast , mobility of patient and tolerance of the patient in pp . 
sp achieved a better coverage of the ptv at the expense of increased dose near skpp was considered optimal in 8 of 9 right breasts and in 6 of 11 left breasts . 
courses were integrated into the k - med ( knowledge - based multimedia medical education ) platform , and online - exams were using k - med , as well . 
user - acceptance , duration of use and results of the exams were measured by surveys , collecting of user - tracking data and results of the exams , respectively . 
 the implementation of the e - learning courses in the existing curriculum led to a significant improvement of the examination outcomes ( p = 0.01 , rank sum test ) in comparison with former exams without e - learning courses . conclusion : our experience shows that e - learning can be successfully introduced into a curriculum if certain points are drawn into consideration . 
 patient and method : a 88 year old male with a spinocellular carcinoma of the left occipital scalp not treatable with electrons or orthovoltage because of the size and convexity of the volume was treated by hdr - brachytherapy ( 192ir - source ) using the freiburg - flab applicator set . 
this study correlated target coverage with small bowel dose - volume histograms and clinical tolerance in paraspinal and retroperitoneal tumors after high - dose proton radiotherapy ( pt )  . materials and methods : between 1997 and 2008 , 31 pts . 
 conclusion : proton irradiation , especially for large paraspinal and pelvic tumors is an excellent tool when the gtv requires high doses > 70 gy ( rbe ) , due to an almost complete absence of small bowel toxicity . 
five radiopaque clips ( 1 in the center of the surgical cavity and the others at 4 cardinal points ) were placed immediately after surgery to correcly delineate the surgical bed and were used as reference markers for igrt , either 2d or 3d modality . 
the surgical clips matching was performed with the planning ct ones . results : we registered the isocenter shifts along the longitudinal , vertical and lateral axes before each rt session . 
patients were eligible if they had 1 to 5 intracranial lesions with a maximum diameter of 3cm and were assigned to focal - only irradiation or wbi / sib according to the rtog recursive partitioning analysis prognostic classes ( rpa ) and number of bm . 
the level of treatment accuracy was acceptable and with 4 patients surviving more than 10 months we feel further exploration of the protocol may be worthwhile . objective : stereotactic radiotherapy ( srt ) and radiosurgery ( srs ) of brain tumors are safe and accurate techniques offering durable local control in selected patients . 
we present our first experiences especially concerning acute and subacute toxicity . materials and methods : since implementation of srt and srs ( linear accelerator - based techniques ) in feb . 
three patients reported initial pain relief , which was excellent in one patient with itn ( from grade iv to grade i ) and moderate in the two patients with ms ( from grade iv to grade iii )  . 
no complications were encountered other than transient dizziness in one patient 3 months after treatment . conclusion : these preliminary results suggest that novalis tx rs for tn with the following treatment parameters ( median maximal dose of 79 gy and mean dose to the trigeminal nerve of 30 gy ) is safe as far as short term follow up is concerned . objective : to assess toxicity and disease control in a cohort of patients treated with imrt for anal canal cancer at the hug . materials and methods : we retrospectively reviewed charts from 37 patients receiving chemoradiation ( n = 34 ) or rt alone ( n = 3 ) using imrt for ajcc stage i - iiib carcinoma of the anal canal or margin , between march 2006 and december 2010 . 
3 pts had induction intra - arterial chemotherapy . results : acute toxicity was acceptable , with maximal g3 skin toxicity in 10 pts ( 27% ) including all 3 hiv + pts , maximal g2 diarrhea in 8 pts , and maximal g2 urinary toxicity in 2 pts . 
follow - up : mean 11 months , range 2 41 months . results : complete remission ( cr ) after induction chemotherapy was observed in 6 / 36 ( 17% ) , partial remission ( pr ) in 24 / 36 ( 66% ) , no change / progressive disease ( nc , pd ) in 6 / 36 ( 17% ) patients , 3 patients with metabolic cr showed only a pr in their mri or ct studies . 
all patients with nc or pd ( n = 6 ) after induction chemotherapy survived less than 34 months ; all patients with a complete metabolic remission had no recurrence during follow - up ( range 3 months 17 months )  . conclusion : induction chemotherapy with tpf or tp followed by crt seems to be an effective treatment in patients with unresectable advanced head and neck cancer with a considerable toxicity that needs special expertise which is best assured in a multidisciplinary setting . 
follow - up : up to 21 months . results : the itv derived by 4d - ct was identical or smaller than the itv derived by non - gated pet in 20 / 22 lesions , in 2 / 22 lesions bigger due to spiculae as seen in the diagnostic lung window . 
one out - field recurrence in hilar and mediastinal lymph nodes 12 months after sbrt , one bone metastasis 18 months after sbrt , both patients were treated with 5 x 7 gy ( bed < 100 gy )  . 
verwey j1 , heufelder j2 , van goethem m - j3 , tourovsky a1 , grossmann m1 , jermann m1 , goitein g1 , lomax t1 , zografos l4 , hug e1 1center for proton therapy , paul scherrer institut , villigen , switzerland ; 2charit universittsmedizin berlin , berlin , germany ; 3kvi , groningen , the netherlands ; 4hpital ophtalmique jules gonin , lausanne , switzerland objective : in 2010 optis2 the new proton therapy facility for ocular tumours started with patient treatments 26 years after the beginning of the optis program at psi in 1984 . 
one aspect of proscan is the multi - room operation of gantry1 , gantry2 ( in development ) , and optis2 , all connected to one 250 mev compact proton cyclotron . materials and methods : a double - scattering system had to be developed de novo for optis2 to deliver a proton beam suitable for treatment with at least similar or preferably improved beam characteristics than optis . 
in view of the technical constraints and operational demands of proscan the software and the hardware of the control system of the treatment facilities was completely redesigned and implemented anew . results : in 2010 47 patients were treated with optis2 , and in the upcoming years it will provide ocular proton therapy for approximately 250 patients per year . 
 magnetic resonance spectroscopy used a clinical mr scanner ( philips , short echo single - voxel sv press , 3 - t ) to provide biochemical in addition to conventional morphological mr information . 
the treatment planning ct ( oncentra masterplan ) was matched with the preoperative ct and the target volume was defined to encompass the region of spectroscopic abnormality . results : mri examinations prior to radiotherapy showed an increased hyperintensitiy in diffusionweighted images ( dwi ) , a contrast enhancement and an increased choline and decreased n - acetyl - aspartate around the resection cavity corresponding to remaining tumor or tumor recurrence . mri examinations in the follow - up showed normalization of the initial pathologic spectra . conclusion : our first experience indicates that the definition of rt target volume according to the combined morphologic and metabolic abnormality may be an interesting information to confirm the correct application of the boost volume . 
three pts received induction platin - based chemotherapy . results : with a median follow - up of 22 months ( range 4 - 42 ) , the median duration of local control was 22 months . 
failure was from progressive disease in 1 pt , local relapse in 2 pts at 8 and 13 mos , lung primary in 1 pt , and death from unrelated causes in 4 pts . 
van der zee j2 kantonsspital aarau ag / kantonsspital olten , switzerland1 , erasmus medical center , rotterdam , the netherlands2 objective : standard therapy for muscle invasive bladder cancer is radical cystectomy . 
in a pilot protocol started 09 - 2010 we will treat up to 10 patients using platin - based single agent ct combined with fractionated rt and ht . materials and methods : muscle invasive bladder cancer stage t2 t4 / mx / m0 : patients were excluded from radical cystectomy due to co - morbidity . 
ct consists of weekly cisplatin or carboplatrepeated f / u includes cystoscopy / urine cytology / bladder function tests by the referring urologist . results : so far 2 patients have completed trimodality therapy . 
dose constraints were the following : maximum point dose to the carotids < 35 gy , to the spinal cord < 30 gy , and ptv was covered at > 95% of the prescribed dose ( 70 gy in 2 gy per fraction )  . 
in highintermediate and high - risk patients the recommended adjuvant treatment implies external beam pelvic radiotherapy ( pebrt ) with taking into consideration the toxicity of the organs at risk . 
we present our experience with adjuvant imrt in endometrial cancer with regard to toxicity and outcome . materials and methods : between 20062009 55 pts with median age of 67 underwent adjuvant pebrt and vaginal cuff bt for high intermediate and high risk stage . 
all acute and late toxicities ( rtog ) were scored . results : within a median follow up of 31 ( 15 - 45 ) months , 2% of the pts had died . 
however , in 17% of pts lymph edema of the lower extremities was observed . conclusion : imrt technique in adjuvant endometrial cancer for high - intermediate and high - risk patients provides a high probability of locoregional control with acceptable toxicity . 
 * equally contribution author purpose : pelvic radiation therapy ( rt ) represents a therapeutic option in the treatment of node - positive prostate cancer but it remains controversial , because of its high rate toxicities . 
in this study , we aimed to assess the rate of toxicities according to ctc - nci.v3 in such patients treated with either 3dcrt or imrt ( tomotherapy )  . methods and materials : from january 2008 to december 2010 , data were analyzed from 30 consecutive patients including 29 node - positive prostate cancer undergoing definitive or adjuvant rt ( imrt and / or 3dcrt ) after radical prostatectomy and lymphadenectomy combined to hormonal theramedian age was 66 years ( range : 52 - 83 )  . 
we therefore focused on primary and permanent teeth as oar , investigating the ability to identify the developing tooth bud in children and infants and to obtain individual tooth dose distributions . materials and methods : between 2003 and 2009 , 14 pediatric pts . 
individual teeth were contoured on transverse image slices from the original planning ct scan , and dvh data were retrospectively obtained from the total delivered treatment , calculated using in - house treatment planning software . results : all primary teeth and permanent incisors , canines , and first molars were individually contoured without difficulty in all patients . 
however , ctbased identification of the two permanent premolars and second molars correlated roughly with expected time of initial tooth calcification , with all teeth being readily identifiable by 4 years of age . 
cure without long - term sequelae of treatment is the goal and the strategy used should minimize the effect of radiation exposure to avoid the risk of second nontesticular cancers . 
 aim : to measure the radiation doses of organs at risk ( oar ) from ct scans during follow - up of patients under surveillance strategy and to compare this with the radiation doses and volumes of organs at risk ( oars ) of patients treated with adjuvant rt focused on mathematical models aiming at associated lifetime cancer risks . materials and methods : organ doses will be measured on 15 ct scans of one patient assigned to active surveillance strategy and compared to those of one patient treated with 20gy in 2gy / fraction adjuvant radiation using tomotherapy . 
cancer risks , in the form of lifetime attributable risk ( lar ) of cancer incidence , will be estimated by linear extrapolation using the organ radiation doses and the lar data . 
in this study , the disease profile , outcome , and prognostic factors were assessed in patients with stage i and ii pbl . patients and methods : thirteen rare cancer network ( rcn ) institutions enrolled 116 consecutive patients with pbl treated between 1987 and 2008 in this study . 
inclusion criteria were age > 16 years , stage i and ii , minimum 6 months follow - up and a biopsy - proven confirmation of non - hodgkins lymphoma ( nhl )  . 
eighty - seven patients underwent chemoradiotherapy ( cxrt ) , 15 radiotherapy ( rt ) without ( 13 ) or with ( 2 ) surgery , 14 chemotherapy ( cxt ) without ( 9 ) or with ( 5 ) surgery . 
median follow - up was 41 months ( range : 6 - 242 )  . results : the overall response rate at the end of treatment was 91% ( cr 74% , pr 17% )  . 
the 5 - yr overall survival ( os ) , lymphoma - specific survival ( lss ) , and local control ( lc ) were 76% , 78% and 92% , respectively . 
six patients developed grade 3 or more toxicities , according to common terminology criteria for adverse events ( ctcae ) v3.0. conclusion : this large multicenter study confirms the relatively good prognosis of early stage pbl treated with combined cxrt . 
comparative planning for intensity modulated radiotherapy ( imrt ) volumetric intensity modulated arc therapy ( rapid arc , ra ) was performed . materials and methods : eight patients treated with imrt after extrapleural pleuropneumonectomy ( epp ) were replanned for ra . 
treatment plan comparisons were carried out using monitor units ( mu ) and dose - volume histogram parameters . results : both imrt and ra , achieved acceptable ptv coverage and organ sparing . 
we calculated systematic and random setup errors in lateral ( x ) , superior - inferior ( y ) and anterior - posterior ( z ) directions , and the rotational correction around the superior - inferior axis ( roll )  . 
interplay effects of tumor motion phase and imrt segments is suppressed by using a low number ( < 10 ) of large segments with a high minimum number of mu ( > 20 mu at 200mu / min )  . 
tumor size , shape and midline position comparability has been verified for drr to epid and 4dct to cbct in a phantom study . results : major problems could be identified , separated and addressed independently based on several publications . 
to avoid air gaps an ultrasound gel was used between wax and filthe films were irradiated with the clinical conditions on ortovoltage unit and linac for each energy quality separately . 
an epson scanner and filmqa software ( isp ) together with the ksa procedure for film dosimetry were applied for the scanning and evaluation process . results : the measured dose distribution showed good coverage of the ptv and good nail sparing . 
a save , fast and homogeneous irradiation technique is presented . materials and methods : resected bone is packed fourfold to prevent infection with each sheath being evacuated to avoid air cavities . 
position of the package inside the water column is guaranteed by a plastic foil attached to the ground of the basirradiation is done with a preconfigured water phantom plan by laterally opposed beams with 10 mv photons . 
cone beam cts before and after irradiation were used to verify bone position and to calculate 3 - ddose distribution , respectively . results : up to now 7 patients had been treated with eci . 
setup of the water phantom on the linac and fixation of the sample takes 15 min , irradiation including cone beam cts additional 25 mindependent of its previously unknown shape , the bone can be placed well inside the homogeneous part of the irradiated volume . 
the purpose of this study was to evaluate the advantage of each of these technique for vestibular schwannoma ( vs ) and for the treatment of small metastasis ( target volume < 5 cm3 )  . materials and methods : stereotactic treatment plans were made for 7 patients . 
for all patients we made an imrt ( 6 non - coplanar fields ) and a ra ( 1 - 2 arcs ) plan which were created in eclipse ( v8.9 , varian medical system )  . 
 treatment plan comparison were carried out using monitor units ( mu ) , doses in critical structures , homogeneity index ( hi ) and conformity / gradient index ( cgi , cgic and cgig ) [ wagner et al , ijrobp 2003 ]  . results : in the overall comparison of imrt and rapidarc , we found acceptable organ sparing and ptv coverage . 
is the time and effort spent on the daily morning checks justified ? during introduction of an additional igrt test we evaluated the total time needed and how to increase efficiency . 
all measurements allow an immediate visual inspection and a later detailed analysis . results : patient workflow oriented qa procedures relate more closely to the treatment as a whole and is time - efficient . 
 no cirs report related to missing or insufficient daily qa checks was recorded . conclusion : it is impossible to check all parameters of todays complex treatments individually in an efficient manner . 
8 original article prostate image - guided radiotherapy by megavolt cone - beam ct sergio zucca , barbara carau , ignazio solla , elisabetta garibaldi , paolo farace , giancarlo lay , gianfranco meleddu , pietro gabriele1 purpose : to test megavolt cone - beam ct ( mv - cbct ) in order to evaluate setup errors in prostate radiotherapy . patients and methods : the setup of 9patients was verified weekly by electronic portal imaging ( epi ) and mv - cbct , both performed in the same treatment session . 
mv - cbcts were matched to simulation cts by manual registration based on bone markers ( bmr ) , by manual registration based on soft tissues ( str ) rectum , bladder , and seminal vesicles and by automatic registration ( ar ) performed by a mutual information algorith shifts were evaluated along the three main axes : anteroposterior ( ap ) , craniocaudal ( cc ) , and laterolateral ( ll )  . 
finally , in 4 additional patients showing intraprostatic calcifications , the calcification mismatch error was used to evaluate the three mv - cbct matching methods . results : a total of 50pairs of orthogonal epis and 50mv - cbcts were analyzed . 
mv - cbcts wurden mit simulations - cts abgeglichen , und zwar durch eine manuelle erfassung der knochenmarker ( bmr : bone marker ) , durch eine manuelle erfassung der weichgewebewerte ( str : soft tissues ) rektum , blase und samenblschen und durch eine automatische erfassung ( ar ) aufgrund eines informationsalgorithmus . 
darber hinaus wurden bei 4 zustzlichen patienten , die an prostataverkalkung litten , die diskrepanzwerte der verkalkung fr die analyse der drei mv - cbct - ausgleichsverfahren genutzt . ergebnisse : insgesamt wurden 50 orthogonale epis - paare und 50 mv - cbcts analysiert . 
was das verkalkungs - datenset ( 22 messungen ) angeht , war die abweichung der verkalkungswerte der ap - achse viel niedriger ( p < 0 , 05 ) bezogen auf str als bezogen auf bmr bzw . 
technological advances in dose delivery have increased the dose conformation to the target , allowing the risk of rectal toxicity to be reduced [ 1 , 3 , 8 , 26 , 32 , 34 ]  . 
image guidance is an effective strategy to improve patient positioning [ 33 ] , allowing tumor control to be increased by potential dose escalation [ 12 , 14 ]  . the electronic portal imaging ( epi ) device is the most used system to verify patient setup . 
by providing only twodimensional ( 2d ) imaging , it is unable to clearly identify soft tissue , and bone markers have to be used as a surrogate of the target position . 
it is well known that the interfraction reproducibility of prostate position is significantly affected by changes of rectum filling [ 29 ] and may be influenced , to a less extent [ 30 ] , by the filling of the bladder [ 21 ]  . 
 ultrasound - based imaging has been recently introduced , but it may overestimate the daily prostate motion , particularly in the ap direction , negatively impacting prostate dose coverage and rectal sparing [ 22 ]  . online three - dimensional ( 3d ) ct approaches capable of soft tissue imaging are under continuous investigation to assess patient setup immediately prior to treatment . 
on rail kilovolt ct and kilovolt cone - beam ct ( kv - cbct ) [ 24 ] , while promising , require a dedicated ct in the treatment room , or a dedicated kilovolt system mounted orthogonally to the treatment gantry . 
alternatively , megavolt cone - beam ct ( mv - cbct ) , which tomographically reconstructs the 2d images from epi , is capable of 3d imaging and is available in many centers [ 2 , 9 , 22 ]  . 
the additional dose from daily mv - cbcts of prostate patients is small compared to the treatment dose ( < 4% ) and can be compensated during the planning procedure [ 19 ]  . 
the poor image quality , due to the use of megavolt radiation and detectors as well as to the effect of cone - beam scattering , may hinder the clear identification of soft tissue structures in the pelvic area . 
despite these limitations , not only mv - ct [ 16 ] , but also mv - cbct , has been recently proposed as a practical direct method of daily prostate localization [ 2 ]  . in the present study , we investigate the potential of mvcbct for the assessment of systematic preparation and / or interfraction setup errors in prostate radiotherapy . 
for this purpose , soft tissue alignment was compared with bone alignment and the available manual / automated methods for performing image registration were analyzed . materials and methods subjects and study design between july 2009 and february 2010 , 13patients ( 4 with intraprostatic calcifications ) affected by prostate cancer were randomly enrolled in the study . 
in order to obtain a reproducible filling of bladder and rectum ( bladder full and rectum empty ) , a specific protocol was applied in all patients prior to the planning ct and every treatment fraction . 
all patients were positioned supine and immobilized by a knee - lock systeaxial ct slices at 3 - mm intervals were acquired ; isocenter was positioned in the center of mass of the prostate and mobile room lasers were used to a mark reference tattoo on the patient skin the treatment room , patient positioning was performed using room lasers and these skin markers . 
in each patient , the treatment setup verification was performed by a standard no action level ( nal ) protocol [ 6 ] based on the epis acquired in the first three treatment sessions . 
mv - cbcts were registered to the planning cts by three different methods : ( 1 ) manual matching based on bone markers ( bmr ) , ( 2 ) manual matching based on soft tissues ( str ) , and ( 3 ) automated registration ( ar )  . 
the calcification mismatch error was calculated with the three different methods for the registration of mv - cbcts to planning ct . epi and mv - cbct acquisitions all measurements were performed on oncor impressionplus ( siemens ag healthcare ) systems . 
the epi device ( optivue 1000 st ) includes a flat panel ( ag9 , perkinelmer , optoelectronics ) of a - si detectors ( 1024 1024 pixels ; 40 40 cm2 ) , coupled with a scintillator lanex ( kodak lanex fast gd2o2s : tb ) plate . 
mv - cbct was performed by means of a mvision 2.0 package , covering an arch of 200 ( from 90 to 110 ) by a 6 mev beam , at a dose rate of 50mu / mall scans were acquired using 9 mu . 
 images were reconstructed by filtered back - projection , with a matrix size of 256 256 , covering a maximum field view of 2727 cm2 . both in 2d and 3d modalities , the positioning of the epi device was characterized by an accuracy of 2.0 mm , as reported by other groups [ 10 ]  . epi analysis orthogonal epis were compared to the drrs images reconstructed by the treatment planning system from the planning ct . 
in the anteroposterior projections , the registration was performed focusing on the pubic symphysis and iliac bone , and in the lateral projections focusing primarily on the pubic symphysis and secondarily on the sacrum . the mean shifts along the three main axes anteroposterior ( ap ) , craniocaudal ( cc ) , and laterolateral ( ll ) were calculated . 
mv - cbcts were also automatically registered ( ar ) to planning cts using a mutual information algorithm available on a siemens therapist workspace platforthe time required for mv - cbct acquisition and automated registration was approximately 2 minutes , comparable to the time required for the epi acquisition and their manual registration . both in the manual and automatic registrations , rotations were not allowed since their correction can not be applied to the treatment couch . 
the shifts obtained after the three different mv - cbct registration methods were calculated and statistically compared . finally , in the four additional patients showing intraprostatic calcification , points of interest were defined in the center of the calcification and 3d coordinates were calculated both in the cts and mv - cbcts . 
for each mv - cbct registration procedure , the distances between the two points of interest ( calcification mismatch ) were calculated along the three main axes . statistical analysis to compare the measurements obtained by different techniques ( epi vs mv - cbct ) , the one - tail paired student t - test was applied with a tolerance value : the null hypothesis was that the differences of the mean shifts or distances were less than 2.0 m since the epi device was repositioned between the epi and the mv - cbct scans , such tolerance level was used for their comparison . to test the epi - based nal protocol , the one - tail student t - test was applied on the epi data set with the same tolerance value . 
patients shifts ( a ) and calcification displacements ( b ) along the ap axis , calculated by electronic portal imaging ( epi ) , and mv - cbct after automated ( ar ) , soft tissue ( str ) and bone markers ( bmr ) registration . 
abweichung des patienten ( a ) und kalzifizierungsbedingte abweichung ( b ) entlang der ap - achse ; berechnung mittels epi ( elektronisches portal - imaging ) und mv - cbct nach automatischer erfassung ( ar ) bzw . 
in the no - calcification data set , the shifts calculated along the ap axis applying bmr were significantly different ( p < 0.001 ) than applying ar and str ( figure 1a )  . in order to evaluate the different methods for the correction of patient position by mv - cbct , the calcification data set was analyzed using the intraprostatic calcifications as an internal fiducial marker ( figure 2 )  . 
along the ap direction , the calcification mismatch was significantly smaller ( p < 0.05 ) after str registration than after bmr , whereas ar produced a significantly higher calcification mismatch ( p < 0.01 ) with respect to str ( figure 2b )  . the time required for manual registration of mv - cbct and preparation ct based on str or bmr was about 2 min in both cases , whereas the ar procedure takes about 10 s . discussion to verify and correct patient position in prostate radiotherapy , epi aligned on bone anatomy are routinely used . 
however , the prostate position can vary with respect to bone structures due to movements and physiological changes of internal organs [ 21 ] and / or of the target [ 27 ]  . 
our study focuses on the role of mvcbct for soft tissue localization in prostate radiotherapy and on the influence of limited image definition , which was recently shown not to hinder prostate positioning . 
our results support these recent findings : despite poor image quality , 3d soft tissue imaging performed by mv - cbct ( and a corresponding registration with planning ct based on soft tissue ) showed a significant difference with respect to the epi setup , assuming a tolerance level of 2.0 mm , which is considered the current tracking limit [ 31 ]  . in our sample , the greatest difference between str and bmr occurred in the ap direction . 
accordingly , prostate shift with respect to bone structures occurred particularly in the ap direction and , to a less extent , in the cc direction [ 18 ]  . 
the cc interfraction movements we measured can be underestimated due to the poor imaging quality of mv - cbct , which fails to clearly visualize the prostate - bladder interface [ 2 ]  . the manual registration of mv - cbct with the preparation ct was executed by a single experienced radiation oncologist ; therefore , our results were not affected by interobserver variability . 
prostate mv - cbct in mv - cbct prostate localization , performed by an experienced radiation oncologist , was reported to be less than 2 mm [ 2 ] , which was the tolerance level we assumed . to verify the reliability of soft tissue registration on mv - cbct , we quantitatively measured the mismatch in 4 additional patients showing intraprostatic calcifications , as recently suggested [ 17 ] to assess kv - cbct based accuracy . 
despite such encouraging results , the main difficulties of using mv - cbct for soft tissue registration remain the low signal / noise and the low soft - tissue contrast . 
new approaches to generate soft - tissue improved mv - cbct using low z target are currently proposed and will likely reduce the gap with respect to kv - cbct [ 7 , 25 ]  . 
contrast noise ratio may be increased by a factor of 4 or greater and improvement of the spatial resolution is also apparent . the differences we observed between str and bmr registration demonstrated that methods involving softtissue imaging can have a clinical impact . 
for example , the application of mv - cbct in off - line protocols [ 5 ] could reduce the systematic error which affects the preparation positioning , as the patient setup imaged during planning ct does not usually represent the mean position during therapy . 
when distension of the rectum prevented a satisfactory match of the prostate with the planning target , the patient can be sent to the restroom and the treatment fraction can be restarted after re - positioning and a new verification of the setup [ 16 ]  . in addition , the potential of automated registration on mv - cbct to develop faster and operator independent setup protocols , as proposed on kv - cbct [ 28 ] was investigated  . 
the contours of bone , prostate , and rectum were delineated on planning ct ( a ) and overlaid on the mv - cbct after registration by manual soft tissue ( b ) , manual bone landmark ( c ) , and automated registration ( d )  . 
the distance between the cross - line and the calcification visible on mv - cbct is clearly lower in ( b ) than in ( c ) , particularly along ap direction . 
die konturen von knochen , prostata und rektum wurde auf planungscts bertragen ( a ) und nach manueller erfassung der weichgewebewerte ( b ) und der knochenmarker ( c ) bzw . 
die auf mv - cbcts sichtbare distanz zwischen dieser transversale und der verkalkung ist deutlich niedriger in ( b ) als in ( c ) , insbesondere entlang der ap - achse . 
the main limitation of our study was that the applied algorithm , available in our commercial package , was not optimized to perform registration of the prostate , since the whole field of view was considered during the registration procedure . 
focusing on a submask covering only the prostate might improve the performance of automatic registration , also limiting the effects of physiological changes ( bladder and / or rectum filling , gas pockets )  . conclusion our findings support the assessment of soft tissue position by mv - cbcts , instead of the application of epi procedures , to verify and correct patient setup immediately prior to treatment . 
prostate mv - cbct original article combination of dose escalation with technological advances ( intensity - modulated and image - guided radiotherapy ) is not associated with increased morbidity for patients with prostate cancer michael pinkawa , marc d . 
eble1 purpose : the aim was to evaluate treatment - related morbidity after intensity - modulated ( imrt ) and image - guided ( igrt ) radiotherapy with a total dose of 76gy in comparison to conventional conformal radiotherapy ( 3dcrt ) up to 70.272gy for patients with prostate cancer . 
 patients and methods : all patients were prospectively surveyed prior to , on the last day , as well as after a median time of 2 and 16months after rt using a validated questionnaire ( expanded prostate cancer index composite )  . 
3dcrt were patient age , use of antiandrogens , treatment volume ( whole pelvis ) , prognostic risk group , and urinary / bowel / sexual quality of life ( qol ) before treatment . 
3dcrt waren das patientenalter , der einsatz eines antiandrogens , zielvolumen ( becken ) , prognostische risikogruppe und lebensqualitt ( lq ) beim wasserlassen / stuhlgang / sexualitt vor der behandlung . 
dose escalation for prostate cancer schlussfolgerung : die verknpfung einer dosiseskalation mit technologischen fortschritten ( imrt und igrt ) ist bei patienten mit einem prostatakarzinom nicht mit erhhter morbiditt assoziiert . schlsselwrter : prostatakarzinom intensittsmoduliert radiotherapie bildgefhrte radiotherapie konformale radiotherapie lebensqualitt introduction external beam radiotherapy ( ebrt ) is a well - established curative treatment for prostate cancer [ 810 , 12 , 19 , 22 ]  . 
these trials were started more than 10years ago , so that conventional conformal radiotherapy ( 3dcrt ) was applied . major technical advances that are increasingly adopted for ebrt for localized prostate cancer are intensity - modulated radiotherapy ( imrt ) [ 8 , 12 ] and image - guided radiotherapy ( igrt ) [ 22 ]  . 
the volume of organs at risk can be especially reduced within the high dose region . the application of igrt before each fraction for prostate localization is the crucial prerequisite for the reduction of safety margins to account for prostate motion . 
as reported in a recent publication , 1.5cm posterior margins are needed without igrt , whereas 0.4cm are sufficient with daily igrt [ 22 ]  . the aim of this study is the comparison of health - related quality of life ( qol ) changes after 3dcrt with total doses of 70.272 gy versus dose - escalated imrt up to 76gy . 
matched pairs were selected to ensure two well comparable patient groups . patients and methods this prospective study was based on consecutive patients who were treated due to localized t1 - 3n0m0 prostatic carcinoma with 3dcrt in the years 20032007 and imrt in the years 20062008 . 
the treatment was based on a computed tomography ( ct ) scan in the supine position with a slice thickness of 5mpatients were asked to have a full bladder for the planning ct scan and each radiotherapy fraction . for 3dcrt , treatment plans were calculated using a fourfield box technique with 15mev photons and a multileaf collimator . 
the ptv was required to be enclosed by the 90% isodose relative to the international commission on radiation units and measurements ( icru ) reference point [ 13 ] with a margin of 1.5cm in the anterior / lateral and 1cm in the craniocaudal and dorsal directions to the clinical target volume ( ctv = prostate seminal vesicles )  . 
treatment of the whole pelvis was performed in case of an estimated risk of lymph node involvement above 15% ( according to partin tables [ 17 ] ) up to a total dose of 4546gy at 1.82.0gy daily fractions using the 3dcrt technique for all patients . for imrt , 8mm lateral / anterior , 5mm superior / inferior , and 4mm posterior margins were added to the ctv [ 22 ]  . 
the direct machine parameter optimization algorithm was applied for inverse planning with a 2cm2 minimum segment area , 5 minimum segment monitor units , and a maximum number of 70 segments . 
the general relationship between icru reference and ptv mean doses in imrt has been found to be similar to that in three - dimensional dose distributions [ 29 ]  . 
treatment planning objectives included a maximum dose of 50gy / 70gy to 50% / 20% of the rectum volume , a maximum dose of 55gy / 70gy to 50% / 30% of the bladder volume and a dose homogeneity of 5% within the ptv . 
dose escalation for prostate cancer igrt was applied using the bat sxi system ( b - mode acquisition and targeting ) [ 22 ] after setup to external skin marks immediately before imrt treatment . 
when the images are aligned on the monitor , the computer reveals the couch shifts in three dimensions to bring the prostate into alignment with the original planning ct position . patients were surveyed prospectively before ( time a ) , on the last day ( b ) , and a median time of 2 months ( range , 6 weeks6 months ) after ( c ) , and 16 months ( range , 1220 months ) after ( d ) radiotherapy using a validated questionnaire ( same median intervals and ranges after 3dcrt and imrt ) , the expanded prostate cancer index composite ( epic ) [ 26 , 28 ]  . 
 the multi - item scale scores were transformed lineary to a 0100 scale , with higher scores representing better qol . only patients with questionnaire results from both time a and time d were included in the analysis , resulting in an initial group of 362 patients after 3dcrt ( whole pelvic treatment in 61 cases ) [ 20 , 21 ] and 78 patients after imrt ( whole pelvic treatment with imrt as a boost in 16 cases , imrt as a boost following 3dcrt up to a dose of 60gy in 44 cases , imrt for the complete treatment in 18 cases )  . 
 for each patient in the imrt subgroup , a 3dcrt patient was matched according to the following criteria : age5years , use of antiandrogens , treatment volume ( whole pelvis ) , prognostic risk group , and urinary / bowel / sexual qol ( function score preferably 10 points ) before treatment . 
finally , 78 patients after 3dcrt and 78 patients after imrt resulted for the evaluation including 78 / 78 ( time a ) , 60 / 45 ( time b ) , 78 / 69 ( time c ) , and 78 / 78 ( time d ) questionnaires after 3dcrt / imrt . the questionnaire was given to the patients personally by one of the physicians at time a , b , and c . 
imrt ( links , verschreibungsdosis von 76gy ) versus 3dcrt ( rechts , verschreibungsdosis von 70 , 2gy ) bestrahlungsplne mit isodosen in einer axialen ct - schicht und den dosis - volumen - histogrammen fr prostata , rektum und blase . statistical analysis was performed using the spss 17.0 ( spss , chicago , il ) , software . 
the wilcoxons matched - pairs test was applied to determine differences between the treatment groups and longitudinal changes in specific subgroups of patients , including a prostate - specific antigen ( psa ) evaluation within 12 month after ebrt ( biochemical recurrence = rise by 2 ng / ml above the nadir psa )  . 
3dcrt and imrt treatment plans are shown in figure 1 ( example for same patient ) to demonstrate the crucial differences : ( 1 ) larger ptv in the 3dcrt plan ; ( 2 ) larger rectal and bladder volumes in the strahlenther onkol 2011 no . 
ausgewhlte symptome ( * signifikanter unterschied zwischen den untergruppen )  . time a ( % ) time b ( % ) time c ( % ) time d ( % ) pain on urination once a day occasional urinary dribbling rectal urgency once a day bloody stools rarely painful bowel movements once a day uncontrolled leakage of stool > rarely no ability to have erections erections not firm enough for sexual intercourse lack of energyonce a day 3dcrt 4 imrt 3dcrt 36 imrt 3dcrt 13 imrt 3dcrt 3 imrt 3dcrt 1 imrt 3dcrt 4 imrt 3dcrt 28 imrt 3dcrt 59 imrt 3dcrt 10 imrt 1 * ence was found for the sexual function score changes at time d . 
however , a bowel function score decrease of 7 points and a sexual function score decrease of 19 points resulted for 25% of patients in both subgroups at time d , respectively . percentages of selected symptoms are shown in table 3 . 
rectal toxicity is associated with both the rectal volume within a particular dose level and the dose to a particular rectal volume [ 14 , 7 , 11 , 16 ]  . 
by increasing the total dose to the prostate and decreasing safety margins around the prostate , we have changed two parameters , hoping to improve the tumor control without increasing rectal toxicity . 
 with the possibility to considerably reduce the ptv , igrt is probably of greater value in comparison to imrt . it is too early to assess tumor control for the patients in this study , but qol changes appear to be well comparable . 
patients after imrt reported painful bowel movements less frequently 2months after treatment in comparison to patients after 3dcrt , suggesting a faster relief of pain due to smaller rectum volumes within the high dose levels . 
rectal bleeding was reported more frequently after imrt ( not reaching the level of statistical significance ) , suggesting the predominant effect of the total dose to even smaller rectal volumes on the development of rectal bleeding . 
nevertheless , it has to be considered that imrt has only been used as a boost after an initial dose of 60gy with the 3dcrt technique for the majority of patients in this study . 
in contrast to rectal bleeding , the cumulative incidence of stool incontinence has been shown to increase even after more than 5years [ 2 ] , so that further differences might be found after longer follow - up intervals . 
specifically concerning incontinence , significantly higher percentages reporting uncontrolled leakage of stool in comparison to baseline were only found after 3dcrt , so that stool incontinence will unlikely occur more frequently in the imrt group several years after ebrt . 
the reduction of treated volume , thus , also an improved protection of the anal sphincter , appears to be the crucial factor [ 27 ]  . a comparable analysis , using qol information from the patients perspective , has not been published in the literature yet . 
 [ 30 ] report acute symptoms to be important precursors of late toxicities . the only domain with statistically significant differences concerning the actual scores was the sexual domain , with a significantly higher percentage of patients with erections firm enough for sexual intercourse more than 1year after treatment . 
it is not clear if differences existed for these patients concerning the ability for sexual intercourse or if a smaller ptv is responsible for the difference that was found in the present study . 
nevertheless , taking into account the limited number of patients with erections firm enough for sexual intercourse before ebrt , further studies with larger patient numbers should be performed to verify these data . conclusion the application of technological advances ( imrt and igrt ) for dose escalation is not associated with increased morbidity for patients with prostate cancer . 
advantages found in this study were a faster relief of pain during bowel movements , not significantly increased stool incontinence relative to baseline levels , and better long - term erectile function . 
 original article monte carlo simulations applied to conjunctival lymphoma radiotherapy treatment lorenzo brualla1 , ricardo palanco - zamora2 , klaus - peter steuhl3 , norbert bornfeld4 , wolfgang sauerwein1 introduction : small radiation fields are increasingly applied in clinical routine . 
 in this article , a code for automatic monte carlo simulation of linacs and an application in the treatment of conjunctival lymphoma are presented . methods : simulations of clinical linear accelerators were performed with the general - purpose radiation transport monte carlo code penelope . 
accelerator geometry files , in electron mode , were generated with the program autolinac . results : the monte carlo simulation of an annular electron 6mev field used for the treatment of the conjunctival lymphoma yielded absorbed dose results statistically compatible with experimental measurements . 
in this simulation , 2% standard statistical uncertainty was reached in the same time employed by a hybrid monte carlo commercial code ( emc ) ; however , emc showed discrepancies of up to 7% on the absorbed dose with respect to experimental data . 
results obtained with the analytic algorithm pencil beam convolution differed from experimental data by 10% for this case . conclusion : owing to the systematic application of variance - reduction techniques , it is possible to accurately estimate the absorbed dose in patient images , using monte carlo methods , in times within clinical routine requirements . 
the program autolinac allows systematic use of these variance - reduction techniques within the code penelope . key words : radiotherapy monte carlo variance - reduction linac small fields strahlenther onkol 2011 ; 187 : 4928 doi 10.1007 / s00066 - 011 - 2237 - 3 monte - carlo - simulation der strahlentherapie von konjunktivalen lymphomen einleitung : kleine bestrahlungsfelder werden in der klinischen routine immer hufiger eingesetzt . 
in diesem artikel wird ein computerprogramm fr die automatische monte - carlo - simulation von linacs und eine anwendung auf die behandlung von konjunktivalen lymphomen dargestellt ( abbildung 8 )  . methoden : klinische linearbeschleuniger - simulationen wurden mit dem allzweck - strahlungstransport - monte - carloprogramm penelope durchgefhrt . 
beschleuniger - geometrie - dateien fr den elektronenmodus wurden mit dem programm autolinac generiert ( abbildung 2 )  . ergebnisse : die monte - carlo - simulation eines ringfrmigen 6 - mev - elektronenfeldes , welches fr die behandlung eines konjunktivalen lymphoms benutzt wird ( abbildung 1 ) , zeigt dosisergebnisse , die statistisch mit experimentellen messungen vergleichbar sind ( abbildung 5 )  . 
in dieser simulation wird eine 2% - standardunsicherheit in der gleichen zeit wie bei einem kommerziellen hybrid - monte - carlo - programm ( emc ) erreicht , jedoch zeigt emc bei der absorbierten dosis bis zu 7% abweichung von den experimentellen daten . 
ergebnisse , die mit dem analytischen algorithmus pencil beam convolution erreicht wurden , weichen in diesem fall um 10% von den experimentellen daten ab ( abbildung 6 )  . 1ncteam , strahlenklinik , universittsklinikum essen , essen , germany , 2karolinska university hospital , stockholm , sweden , 3klinik fr erkrankungen des vorderen augenabschnittes , universittsklinikum essen , essen , germany , 4klinik fr erkrankungen des hinteren augenabschnittes , universittsklinikum essen , essen , germany . received : november 3 , 2010 ; accepted : april 8 , 2011 published online : july 25 , 2011 strahlenther onkol 2011 no . 
monte carlo simulations applied to conjunctival lymphoma schlussfolgerungen : durch die systematische anwendung von varianzreduktionstechniken ist es mglich , die absorbierte dosis in patientenbildern mit monte - carlo - methoden in den fr die klinische routine zur verfgung stehenden zeitrumen akkurat zu bestimmen . 
das programm autolinac erlaubt die systematische anwendung dieser varianzreduktionstechniken im programm penelope . schlsselwrter : strahlentherapie monte carlo varianzreduktion linac kleine felder introduction small and highly conformed radiation fields are increasingly employed in clinical routine . 
with the advent of image - guided radiotherapy ( igrt ) and the larger availability of multileaf collimators , small radiation fields find application in stereotactic radiotherapy and intensity - modulated radiotherapy ( imrt )  . 
 moreover , small radiation fields are essential for the treatment of tumors located in small anatomical structures surrounded by organs at risk , as is the case with eye tumors [ 15 , 20 , 21 ]  . however , small radiation fields entail experimental difficulties that do not arise in the dosimetry of the well - known reference fields [ 8 , 14 ]  . 
lack of lateral electronic equilibrium , the larger dependence of experimental measurements on the kind of chosen detector , finite volume effects , or the uncertainties associated with patient positioning are some of the challenges that arise in the dosimetry of small radiation fields [ 12 , 22 , 25 ]  . 
for this reason , the international atomic energy agency ( iaea ) has created a workgroup to develop a code of practice [ 1 ]  . in general , accurate treatment planning of small radiation fields with analytic algorithms is not possible [ 24 ]  . 
these algorithms yield only qualitative results for small fields , even when some sort of monte carlo source model or kernel is used ( see , for example , [ 26 ] and [ 17 ] )  . 
the low accuracy of analytical algorithms in these types of fields arises from the fact that these algorithms are tuned using free parameters experimentally obtained from measurements on reference , and hence much larger , fields . in view of these facts , it is not surprising that treatment planning of conjunctival lymphoma patients is based on heuristic criteria . 
researchers , thus , optimize their conjunctival lymphoma treatments based on recovery rates of patients [ 2 , 10 ]  . pure monte carlo simulations are able to cope with the problems related to small fields and to yield accurate results with the associated statistical uncertainties . 
in this article , we present an application of the recently published code autolinac [ 4 , 5 ] to the optimization and treatment planning of the irradiation technique used for the treatment of the conjunctival lymphoma [ 7 ]  . 
autolinac is a code that automatically generates the input files required for the monte carlo simulation of a clinical linear accelerator ( linac ) with the code penelope [ 19 ]  . 
therefore , autolinac produces files that yield reasonably fast monte carlo simulations and at the same time frees the end user from the programming effort required for simulating a linac with penelope . 
irradiation of the conjunctiva is extremely difficult owing to its complex geometry , the proximity of several organs at risk , such as the eye and the lacrimal gland , and the fact that the conjunctiva itself is an organ at risk [ 20 , 21 ]  . 
the block is placed on the downstream scraper of an electron applicator mounted on a varian clinac 2100 c / d in such a way that the center of the hole coincides with the beam central axis . 
figure 1 shows a drawing of the described collimating device . to obtain a homogeneous dose distribution , the eye of the patient is flooded in a water pool acting as a bolus . 
geometrie des linearbeschleunigers varian clinac 2100 c / d im elektronenmodus bei 6 mev mit 15 - cm - - 15 - cm - applikator , erzeugt mit dem programm autolinac . the monte carlo code penelope has been used to simulate the varian clinac 2100 c / d operating in electron mode at 6mev nominal energy with the described collimator and the 1515cm2 electron applicator . 
relative absorbed dose to water lateral profiles across the centered y - axis in a 15 cm 15cm open field irradiated with an electron beam ( 6 mev nominal energy )  . 
 zur bessern bersicht wurden statistische abweichungen nur an einzelnen stellen beispielhaft abgebildet . it is only necessary to introduce the information relative to the configuration of the linac , e.g. , model , operating mode , energy , field size . 
figure 2 shows a 3d image of the simulated linac in electron mode . the monte carlo simulation of the linac starts from the primary electron source and particles are transported downstreathe validity of the modeled geometry of the linac and the accuracy of the simulation itself have been assessed by comparison of simulated and experimental absorbed doses in water using a 1515cm2 open field with an electron beam of 6 mev nominal energy ( figures 3 and 4 )  . 
statistical uncertainties of all emc results are not shown because the algorithm does not provide thethe right hand side vertical axis corresponds to the difference plots in which computed results are compared to the experimental dataset . 
the compared algorithms are shown with thin lines : penelope ( black ) , emc ( blue ) , emc with gaussian smoothing ( red ) , pbc ( green )  . 
lateralprofile der relativdosis in einem wasserphantom in 1 , 5 cm tiefe mit komplettem kollimator einschlielich eines kurzen ( 1 , 8 cm ) woodmetall - stabs in der zentralachse . 
monte carlo simulations applied to conjunctival lymphoma 10 10 10 11 1012 1013 10 10 10 11 10 12 10 13 10 10 10 11 10 12 10 13 10 10 10 11 10 12 10 13 in general , conventional treatment planning systems are not capable of calculating with the desired accuracy the absorbed dose in a water phantom in the presence of the described collimator . 
in order to test eclipse for this particular problem , the collimator was modified since eclipse does not allow the simulation of collimators whose downstream surface protrudes beyond the lowermost surface of the third scraper . 
therefore , the length of the cylindrical rod ( lr ) was shortened to 1.8calso , eclipse only allows for cerrobend as a collimator material , so the rod was made of it . 
this approach not only limits the accuracy of the code , but also eliminates the possibility of controlling the statistical uncertainty . figure 6 shows dose lateral profiles obtained with the collimator adapted to the requirements of eclipse . 
energy spectra obtained with two pure monte carlo simulations ( penelope ) for a 6mev electron beam using , on the one hand , the full collimator with long pmma rod and , on the other hand , the cerrobend block only . 
the spectra were tallied at a depth of 1.5 cm in a water phanto the mean radius of each concentric detector appears on the upper right corner of each plot and is given in centimeters . 
each subplot shows for each collimator : the total energy spectrum , the electron component of the spectrum , and the photon component ( contamination ) of the spectru results using only the cerrobend holed collimator are plotted in blue for photons , red for electrons , and grey for the total energy spectra . 
ergebnisse fr den kompletten kollimator ( mit zentralem pmma - stab ) , sind in hellblau fr photonen , orange fr elektronen und schwarz fr die gesamtenergiespektren dargestellt . emc and gaussian - smoothed emc results differ by 7% in the penumbra tails compared to the experiment values . 
eclipse results were obtained with the maximum allowed number of histories and the finest available grid size . valuable information about the beam quality can be obtained through pure monte carlo simulations . 
in order to evaluate photon contamination produced by the cerrobend block and the pmma rod , two independent simulations of the linac and a water phantom were run with penelope . 
the goal was to characterize the quality of the beam at a depth of 1.5cm in the water phantothus , 20 concentric annular detectors were defined perpendicular to the beam path at this depth in the water strahlenther onkol 2011 no . 
monte carlo simulations applied to conjunctival lymphoma seen that , roughly , for every ten 6mev electrons that arrive at the 1.5cm depth , one photon of the same energy reaches the same depth . it can be derived from the previous study that analytical algorithms and , to some extent , hybrid monte carlo algorithms are not capable of coping with the accuracy requirements for treatment planning and treatment setup optimization in the presence of such small and highly conformed fields . 
to surmount these problems , pure monte carlo algorithms are required . monte carlo simulation of the absorbed dose in a conjunctival lymphoma patient to study the effect of the water bolus in front of the eye , two simulations were run . 
one simulation included the water bolus , while the other did not . simulation time using this high - resolution computerized tomography image was 160 minutes to obtain a standard statistical uncertainty of 2% of the absolute dose . 
if 1mm3 voxels would have been used , a more common size for computerized tomography voxels , the simulation would have taken 48minutes under the same conditions . figure 8 shows relative isodose lines displayed over the isocenter axial slice of the computerized tomography image . 
the absence of smoothing algorithms is noticed in the wiggling path of the lines when they encounter air material . conclusion the calculation of dose distributions in patients who have to undergo irradiation with small and highly conformed fields , in general , and of conjunctival lymphoma patients , in particular , are cases that are difficult to accurately deal with using the currently available commercial codes in radiotherapy . 
in these cases , uncontrolled statistical uncertainties , present both in the algorithms and experimental devices , hinder the possibility of ascertaining the absorbed dose at each anatomical structure of the patient . 
the width of each annulus was set to 2mthe first simulation used a collimator consisting only of the cerrobend block with the cylindrical hole , while the second simulation used the full collimator , i.e. , block , rod , and slab . figure 7 shows the energy spectra at 1.5 cm depth depending on the perpendicular distance to the beam central axis for both considered collimators . 
each subplot shows the following for each collimator : the total energy spectrum , the electron component of the spectrum , and the photon component of the spectru it can be seen that photon energy spectra are nearly independent of the radial distance to the beam central axis for both collimators . 
since the accelerator is operating in electron mode , photon presence arises from contamination , which is nearly isotropic in the direction of the beathe shielding effect produced by the pmma rod is observed with electron energy spectra being nearly one order of magnitude smaller for radii smaller than 2cm compared to results obtained at the same locations using only the cerrobend block as the collimating device . 
for radii larger than 2cm , the full collimator yields electron energy spectra up to one order of magnitude larger compared to the naked collimating block at the same radial distances . 
these caveats have hindered the routine application of monte carlo codes to the clinical environment . the presented application of the codes autolinac and penelope shows that it is possible to perform pure monte carlo simulations of small and highly conformed fields in times compatible with clinical routine requirements . 
the absorbed dose can be obtained in a high resolution computerized tomography image in 160minutes , reaching a 2% standard statistical uncertainty , while the same uncertainty is reached in 48minutes if a normal resolution computerized tomography image were used . 
systematic and efficient simulation of the linac and the computerized tomography image can be performed thanks to a code like autolinac , which frees the user from the demanding and error - prone tasks of geometry coding and variance - reduction techniques programming . acknowledgments the authors are grateful to g . 
hentschel for proofreading the article . original article patterns of care and course of symptoms in palliative radiotherapy a multicenter pilot study analysis birgitt van oorschot1 , michael schuler2 , anke simon3 , ursula schleicher4 , hans geinitz5 background and purpose : to evaluate patterns of care as well as effectiveness and side effects of palliative treatment in four german radiation oncology departments . patients and methods : all referrals in four german radiation oncology departments ( two university hospitals , one academic hospital , one private practice ) were prospective documented for 1month in 2008 ( 2months at one of the university hospitals )  . 
 in addition , symptoms and side effects were analyzed with standardized questionnaires before and at the end of radiotherapy . results : during the observation period , 603 patients underwent radiation therapy in the four centers and 153 ( 24% , study population ) were treated with palliative intent . 
62 patients reported severe or very severe pain , 12 patients reported severe or very severe dyspnea , 27 patients reported neurological deficits or signs of cranial pressure , and 43 patients reported a poor or very poor sense of well - being . 
radiation therapy led to a significant improvement of well - being ( 35% of patients ) and reduction of symptoms , especially with regard to pain ( 66% ) , dyspnea ( 61% ) , and neurological deficits ( 60% )  . 
unscheduled termination was observed in 19 patients ( 12% )  . conclusions : palliative radiation therapy is effective in reducing symptoms , increases subjective well - being , and has minimal side effects . 
more studies are necessary for subgroup analyses and for clarifying the different goals in palliative radiotherapy . key words : palliative radiotherapy pattern - of - care indications side effects symptom relief strahlenther onkol 2011 ; 187 : 4616 doi 10.1007 / s00066 - 011 - 2231 - 9 alltagspraxis und symptomverlauf bei palliativer strahlentherapie ergebnisse der pilotphase einer multicenterstudie ziel : evaluation der alltagspraxis , des symptomverlaufs und akuter nebenwirkungen bei palliativer strahlentherapie in vier strahlentherapeutischen einrichtungen . patienten und methode : alle erstvorstellungen in den vier einrichtungen ( zwei universittskliniken , ein lehrkrankenhaus und eine private praxis ) wurden einen monat lang im jahr 2008 prospektiv dokumentiert und ausgewertet ( ber 2 monate in einer der universittskliniken )  . 
66 patienten berichteten ber mittlere oder starke schmerzen zu beginn , 12 patienten berichteten ber mittlere oder starke dyspnoe , 27 patienten ber mittlere oder 1department of radiation oncology , university of wrzburg , wrzburg , germany , 2institute of psychotherapy and medical psychology , university of wrzburg , wrzburg , germany , 3department of radiation oncology , helios klinikum erfurt , erfurt , germany , 4center for radiotherapy , dren , germany , 5department of radiotherapy and radiooncology , technische universitt mnchen , munich , germany . received : october 22 , 2010 ; accepted : march 16 , 2011 published online : july 22 , 2011 strahlenther onkol 2011 no . 
 73% der patienten wurden mig hypofraktioniert bestrahlt ( einzeldosen > 2 , 0gy bis 3 , 0gy ) , und 12% der strahlentherapien wurden mit einzeldosen > 3 , 0gy8 , 0gy durchgefhrt . 
fr subgruppenanalysen und zur abgrenzung der verschiedenen endpunkte palliativer strahlentherapie sind weitere untersuchungen mit greren fallzahlen erforderlich . schlsselwrter : palliative strahlentherapie zielsetzung indikation nebenwirkungen symptomlinderung introduction radiotherapy ( rt ) is an established treatment method to relieve symptoms and to secure and improve patients quality of life in a palliative setting . 
evaluated concepts and practical guidelines are available for specific conditions in metastatic diseases such as brain metastases , bone metastases , spinal cord compression , lung cancer , head and neck cancer , esophageal and skin cancer , and pelvic disease [ 12 , 16 , 18 , 31 ]  . 
moreover , radiotherapy is effective in the management of symptoms which are caused by local tumor interference with normal tissue structures through either pressure or infiltration [ 13 , 32 ]  . 
in the present pattern - of - care study , our goal was to determine more about the treatment aims and day - to - day practice of palliative radiotherapy in selected german centers . 
while clinical studies examine a clearly defined problem relating to a limited subgroup , health services research describes patient care and its framework conditions and evaluates them under everyday conditions ( pattern - of - care studies , [ 20 ] )  . 
in dren , erfurt , and munich documentation was carried out in july 2008 , while in wrzburg additional documentation continued for two months ( july and august 2008 )  . 
the center in dren is a radiotherapy practice , the radiotherapy centers in munich and wrzburg are university institutes , and the clinic for radiotherapy in erfurt is an academic teaching hospital . 
patients with palliative radiochemotherapy were excluded . the german version of the edmonton symptom assessment scale ( esas , [ 4 ] ) was applied for symptom assessment at the start of and at the end of radiotherapy ( midos , [ 26 ] )  . 
 it rates pain , fatigue , constipation , dyspnea , weakness , anxiety , and sense of well - being with four - level likert scales from 0 ( = no symptoms ) to 3 ( = very severe symptoms )  . 
symptom relief was combined with other aims in 88% of cases : prevention ( 32% ) , restoration ( 18% ) , life prolongation ( 9% ) , or local control ( 5% )  . treatment planning and fractionation in 93 patients ( 61% ) a ct - planned , 3d conformal radiotherapy technique was used . 
 a total of 17 patients received hypofractionated rt with higher doses than 3 gy ( 12% ) : 7 patients with bone metastases , 2 patients with brain metastases , and 4 patients with metastases in miscellaneous other regions . 
of the 18 patients with bone metastases who were treated with the sole aim of pain relief , 2 received single - fraction radiation therapy with 18 gy ( 11% )  . unscheduled termination in 19 patients ( 12% ) , radiotherapy had to be terminated prematurely for the following reasons : deterioration of general health ( n = 10 ) and death of the patient ( n = 2 ) , inefficiency of therapy or systemic progress ( n = 5 ) or surgical intervention ( n = 1 )  . symptoms and side effects symptoms before and at the end of radiotherapy are shown in figure 1 and include the following : 62 patients reported severe or very severe pain , 12 patients reported severe or very severe dyspnea , 27 patients reported neurological deficits or signs of cranial pressure , and 43 patients reported a poor or very poor sense of well - being . 
self - rated general condition improved significantly in the course of radiotherapy : at the start , 65% rated their sense of well - being as less good or poor , at the end only 23% did ( p < 0.001 , cohens d 0.49 , figure 1 )  . 
in 7 patients ( 4.6% ) , acute toxicity grade iii was recorded : dysphagia grade iii in 3 patients , diarrhea grade iii in 2 patients , dry cough in 1 patient , and 1 local infection . 
patterns of care and course of symptoms in palliative rt pain ( n = 112 ) neurological deficits ( n = 102 ) dyspnea ( n = 97 ) fatigue ( n = 102 ) loss of appetite ( n = 97 ) symptoms of intracranial pressure ( n = 95 ) nausea / vomiting ( n = 95 ) subjective well - being ( n = 67 ) therapy for painful bone metastases without naming reasons [ 9 ]  . start symptom prevalence and symptom relief as far as symptom prevalence before the start of palliative rt is concerned , comparable data are available from the rapid response radiotherapy program of the sunnybrook regional cancer center , university of toronto ( 1 , 296 patients , [ 2 , 11 ] )  . 
in the study of janda and colleagues [ 17 ] , the mean global pain score of patients with advanced cancer commencing radiotherapy was 44.9 ( 10 - point likert scale )  . 
intensity of symptoms at the start of and at the end of rt ; scale values between 0 ( no symptoms ) and 3 ( severe symptoms ) , general condition 0 ( very good ) and 3 ( poor )  . 
signifikante unterschiede im symptomverlauf bei schmerzen , luftnot , neurologischen ausfllen und im befinden ( p < 0 , 01 ; mittelwertvergleich , t - test fr abhngige stichproben )  . tion of underutilization as documented in other studies [ 1 , 21 , 23 , 30 ]  . 
like hospice patients in the usa , only 3% of all 1 , 428 patients received radiotherapy during a stay in a german palliative ward [ 21 , 25 ]  . 
factors influencing radiotherapy referral are waiting times for radiotherapy consultation and treatment , uncertainty about the benefits of radiotherapy , travel distance , and perceived patient inconvenience [ 30 ]  . 
in our study sample , palliative radiotherapy improved sense of well - being , was effective in relieving symptoms , and was associated with a minimal rate of acute side effects . overall , compared with the concepts recommended in literature on radiotherapy for symptom control , more normofractionated or slightly hypofractionated concepts were applied and higher total doses were administered [ 22 ]  . 
this might be explained by skepticism toward hypofractionated concepts because of possible long - term side effects . with regard to pain relief in patients with bone metastases , 10123.0 gy was most often chosen , although a meta - analysis demonstrated that a dose of 8 gy in one fraction is sufficient to achieve this goal [ 7 , 12 ]  . 
in addition , fairchild and colleagues documented an international withholding in using evidence - based hypofractionated palliative radiodata on symptom control after radiotherapy is rare except for bone metastases or spinal cord compression . 
dyspnea improved in 61% of patients , more patients than in a prospective study of sundstrom and colleagues ( 40% , [ 34 ] ) and more patients than in the analysis of 1 , 250 patients with non - small cell lung cancer presented from reinfuss and colleagues ( 38% , [ 29 ] )  . 
patterns of care and course of symptoms in palliative rt sistent : two prospective studies employing 103 gy or 202.5 gy to the neurocranium showed a significant reduction of pain , fatigue , nausea , depression , sense of well - being , and shortness of breath during the 34 month follow - up after therapy [ 6 , 32 ]  . 
 an improvement of neurologic function after irradiation for spinal cord compression in the range of 2540% has been reported in several studies ( [ 39 ] , reviewed in [ 27 ] )  . sense of well - being and unscheduled termination the data on sense of well - being from toronto yields fewer good results than the present study ( 64% improvement of sense of well - being ) : 40% of patients with improved or stable well - being , most commonly due to the already explained selection of patients . 
the rate of prematurely termination ( 12% ) is higher than presented by reinfuss and collegues ( 8% , 1 , 250 palliative radiated patients with non - small lung cancer [ 29 ] )  . 
 well - established and simple prognostic scores , e.g. , for brain metastases or metastatic spinal cord compression [ 5 , 14 , 28 , 33 ] , should be used to minimize premature termination . 
the course of symptoms and the rate of prematurely discontinued therapies differ significantly from the retrospective subgroup analysis by gripp and colleagues ( 58% , [ 15 ] )  . 
whether this is due to a lack of follow - up or an indication for a better tailored palliative radiotherapy is to be clarified in further studies with larger patient numbers . limitations this survey in four radiation oncology departments is not representative in view of the fact that there are over 300 radiotherapy centers in germany . 
for this reason , no statements could be made concerning delayed toxicity , prolongation of life , or prevention of symptoms . conclusion palliative radiation therapy as assessed in this study reduces cancer - related symptoms , increases sense of well - being , and is associated with minimal side effects . 
evaluation of day - to - day practice in palliative radiotherapy can be carried out in a pattern - of - care study . original article evaluation of time , attendance of medical staff , and resources during radiotherapy for head and neck cancer patients the degro - quiro trial wilfried budach1 , edwin blke1 , rainer fietkau2 , andre buchali3 , thomas g . 
wendt4 , wolfgang popp5 , christiane matuschek1 , horst sack6 introduction : a number of national and international societies have published recommendations regarding the required equipment and manpower that is assumed to be necessary to treat a specific number of patients with radiotherapy . 
the german society of radiation oncology ( degro ) was interested in substantiating their recommendations by prospective evaluations of all important core procedures of radiotherapy in the most frequent cancer treated by radiotherapy . 
the results of the examinations of radiotherapy in head and neck cancer ( hnc ) patients are presented in this manuscript . patients and methods : four radiation therapy centers ( university of jena , university of erlangen , university of dsseldorf and the community hospital of neuruppin ) participated in this prospective study . 
working time of the different occupational groups and room occupancies for the core procedures of radiotherapy in hnc were prospectively documented during a 4 - month period and subsequently statistically analyzed . results : the time needed per patient varied considerably between individual patients and between centers for all evaluated procedures . 
room occupancy , presence of technicians , and overall medical staff times were 21 min , 26 min , and 42 min , respectively , for planning ct with i.v. 
contrast medium ( n = 79 ) , and 23 min , 44 min , and 51 min respectively , for planning ct without contrast medium ( n = 45 )  . 
medical physicists spent a mean time of 3h 8 min on physical treatment planning ( n = 97 ) and 1h 8 min on authorization of the treatment plan ( n = 71 )  . 
treatment simulations ( n = 185 ) required an average room occupancy of 23 min , and a mean technicians presence of 47 mthe mean room occupancy ( n = 84 ) was 24 min for the first radiotherapy including portal imaging associated with a mean presence of the technicians of 53 mfor routine radiotherapy sessions ( n = 2 , 012 ) and routine radiotherapy sessions including portal imaging ( n = 407 ) , mean room occupancies were 13 min and 16 min , respectively . 
imrt including portal imaging ( n = 213 ) required an average room occupancy of 24 min and a mean technician time of 48 min . conclusion : the data presented here allow an estimate of the required machine time and manpower needed for the core procedures of radiotherapy in an average head and neck cancer patient treated with a specific number of fractions . 
however , one has to be aware that a number of necessary and time consuming activities were not evaluated in the present study . key words : radiotherapy medical staff head and neck cancer resources time requirement strahlenther onkol 2011 ; 187 : 44960 doi 10.1007 / s00066 - 011 - 2273 - z 1department of radiation oncology , university of dsseldorf , dsseldorf , germany , 2department of radiation oncology , university of erlangen , erlangen , germany , 3department of radiation oncology , hospital neuruppin , neuruppin , germany , 4department of radiation oncology , university of jena , jena , germany , 5prime networks ag , basel , switzerland , 6department of radiation oncology , university of essen , essen , germany . received : february 18 , 2011 ; accepted : may 16 , 2011 published online : july 22 , 2011 strahlenther onkol 2011 no . 
evaluation of time , attendance of staff , and resources during rt for hnc patients evaluation der raumbelegungssowie der arbeitszeit fr das medizinische personal whrend der strahlentherapie von patienten mit kopf - hals - tumoren ( degro - quiro - trial ) fragestellung : internationale gesellschaften haben empfehlungen fr die erforderliche technische ausrstung und fr die anzahl von mitarbeitern zur behandlung von tumorpatienten in der strahlentherapie verffentlicht . 
ziel dieser untersuchung war es , die erforderlichen ressourcen bei der strahlentherapeutischen behandlung von kopfund halstumoren zu evaluieren . methodik : vier strahlentherapie - zentren ( universitt jena , universitt erlangen , universitt dsseldorf und das stdtische krankenhaus neuruppin ) nahmen an dieser prospektiven studie teil . 
die arbeitszeit der verschiedenen berufsgruppen sowie die raumbelegung bei der planung und durchfhrung der strahlentherapie wurde prospektiv whrend eines zeitraumes von 4 monaten dokumentiert und statistisch ausgewertet . ergebnis : die zeit fr die einzelne abschnitte der behandlung variierte erheblich zwischen den einzelnen patienten und den behandlungszentren . 
die definition des zielvolumens ( n = 91 ) war das zeitaufwendigste verfahren fr das rztliche personal und dauerte 1 h 45 mdie medizinphysiker brauchten 3 h 8 min fr die physikalische bestrahlungsplanung ( n = 97 )  . 
die verifikation der plne durch die rzte ( n = 71 ) betrug 1h 8 mdie simulationen von kopf - hals - tumorpatienten ( n = 185 ) erforderten eine durchschnittliche raumbelegungszeit von 23 min , und der zeitaufwand fr die mta betrug 47 mdie mittlere raumbelegung ( n = 84 ) betrug 24 min fr die ersten strahlentherapie einschlielich der verifikationsaufnahme . 
der zeitliche aufwand betrug fr eine mta 53 mfr die routinemige bestrahlung von kopf - hals - tumoren ohne verifikationsaufnahme ( n = 2012 ) waren 13 minuten erforderlich , mit verifikationsaufnahmen ( n = 407 ) 16 mdie anwesenheit von mehreren mtas korrelierte signifikant mit einer krzeren raumbelegungszeit ( p < 0 , 05 )  . 
die intensittsmodulierte radiotherapie mit verifikation ( n = 213 ) erforderte eine durchschnittliche raumbelegungszeit von 24 min mit der anwesenheit einer mta von 48 min . schlussfolgerung : die untersuchung ermglicht die abschtzung des durchschnittlichen personalund ressourcenbedarf fr die kernprozeduren einer strahlentherapie bei patienten mit kopf - hals - tumoren , die mit einer bestimmten anzahl von fraktionen behandelt werden . 
dabei ist zu beachten , dass eine reihe von erforderlichen und zeitaufwendigen ttigkeiten in der studie nicht evaluiert wurden . schlsselwrter : strahlentherapie medizinisches personal kopf - hals - tumoren ressourcen zeitbedarf introduction today , cancer as well as heart and vessel diseases are the leading causes of death in people living in western europe . 
extrapolating the present demographic trends , which show a dramatic increase in percentage of elderly people , cancer will become the most frequent potentially lethal disease in the near future . 
in addition , cancer treatment and care will draw heavily on the healthcare system and available resources . together with surgery and chemotherapy , radiotherapy has long been established as an important treatment modality . 
modern radiotherapy techniques allows for improved dose distributions and more precise delivery of the treatment resulting in less acute and late toxicity and improved survival , although the latter has not formally been shown so far [ 2 , 5 , 11 , 16 , 23 ]  . 
in addition to adequate equipment , sufficient and well - trained staff are required to achieve these benefits for the patients . although recommendations have been proposed about the required equipment and manpower that is assumed to be necessary to treat a specific number of patients with radiotherapy , none of these recommendations were based on actual measurements [ 3 , 6 , 7 , 9 , 12 , 14 , 15 , 17 , 18 , 21 ]  . 
evaluation of time , attendance of staff , and resources during rt for hnc patients patients and methods authorization of treatment planning this study was conducted at the departments of radiation oncology in three academic hospitals and one community hospital in germany ( university hospital of jena , university hospital of erlangen , university hospital of dsseldorf , and the community hospital of neuruppin ) between july 2009 and october 2009 . 
working times of technicians , medical physicists , and physicians required for important core procedures were prospectively documented in all hnc patients undergoing at least one of the following procedures during the time of evaluation . planning ct scan and contrast - enhanced planning ct scan besides the ct scan with / without i.v. 
contrast medium , this procedure included the individual modulation of the immobilization masks in centers 1 , 3 , and 4 , whereas in center 2 masks were already fitted in some of the patients before the planning ct scan in a separate procedure . 
durations for the latter action were not documented . definition of target volumes and organs at risk definition of target volumes and organs at risk typically included the contouring of the gross tumor volume ( gtv ) , the contouring of 23 clinical target volumes ( ctvs ) , and critical normal tissues like spinal cord , parotid glands and others ( if applicable / necessary )  . 
furthermore , the time used for generating any planning target volumes ( ptvs ) and , if necessary , planning risk volumes ( prvs ) as well as time needed for image fusion of the planning ct scan with previous imaging modalities ( ct , mri , pet ) was allocated to this module . 
it is noteworthy that the contouring of normal tissues and the generation of ptvs from ctvs as well as image fusion were performed by different occupational groups in the participating institutions . 
in general , the gtv and the ctvs were outlined by physicians in all institutions . physical treatment planning physical treatment planning included preparation of planning ct scans for treatment , planning , and performing all procedures necessary to generate the 3d conformal treatment plan , including necessary modifications after discussion and the final approval of the plan by the responsible physician . 
 it was also initially intended to evaluate intensity - modulated radiation therapy ( imrt ) treatment planning , but too few data sets were documented to make reliable estimates of the required times . in accordance to the german medical system and liability laws , all treatment plans have to be authorized by the responsible radiation therapist in charge . 
therefore , all resource consumption regarding this procedure , consisting of the complete documentation of the treatment plan , the transfer of the plan to the linear accelerator , including verification of all parameters , and all quality control measures , were evaluated . simulation at a treatment simulator centers 2 , 3 , and 4 used the treatment simulator to transfer the isocenter from treatment planning to the patient and to document the radiation portals by x - rays . 
center 1 used virtual simulation and no treatment simulator . initial irradiation including portal imaging all centers used portal imaging for initial irradiation . routine radiotherapy routine radiotherapy sessions without portal imaging were termed routine radiotherapy . routine radiotherapy ( 3d ) with portal imaging radiotherapy sessions with portal imaging other than the initial session were termed routine radiotherapy with portal imaging . routine radiotherapy ( imrt ) with portal imaging imrt was used in centers 1 and 2 only . 
since daily portal imaging was used in both centers for imrt cases , no data are available for the module routine radiotherapy ( imrt ) without portal imaging . at the linear accelerator , treatment simulator and planning ct scanner two independent examiners ( who had no other duties ) documented the room occupation time as well as the exact times of presence of the technicians , medical physicist , and physicians in an electronic database . 
the presence of residents , students , and other personnel in training were not systematically documented in all institutions and was not the subject of this study . the working times for all occupational groups regarding treatment planning procedures were documented using a case report by the employees themselves and transferred into the database by independent examiners on the next working day . 
 in cases of inconsistencies , direct consultations with the respective person were used to clarify these issues . the total working time of all involved specialists of a specific occupational group regarding each module was added to form one total time . 
for example , if 2 technicians were present during a 15 min procedure and a third technician and 2 physicians were present for only 5 min , then the resulting total working time for technicians was 35 min and for physicians 10 min . the average times for all modules and all occupational groups were calculated separately , including the 5% and 95% percentiles by using standard software ( exceltm )  . 
evaluation of time , attendance of staff , and resources during rt for hnc patients room occupancythe time which represents the duration of each modulehuman resources were measured by recording the actual time of presence for each occupational group and person . 
the nonparametric mannwhitney u test module of standard statistics software ( spss inc . ) was used to test differences between the centers for statistical significance ( p < 0.05 ) results the results are summarized in table 1 and displayed by center , procedure , and occupational group in figures 110 . 
evaluation of time , attendance of staff , and resources during rt for hnc patients centers 1 and 4 preferred planning ct scans without contrast enhancement , whereas centers 2 and 3 favored planning ct scans with contrast enhancement ( figures 1 and 2 )  . 
 on average , room occupancy was a little shorter for contrast enhanced ct scans ( 21 min ) compared to ct scans without contrast media ( 23 min )  . 
however , this can at least partly be explained by the fact that center 1 , which preferred noncontrast - enhanced ct scans , used of a single - detector spiral ct , whereas the remaining centers used multidetector spiral ct . 
 although center 2 prepared immobilization masks already in an upfront procedure that was not documented in this evaluation , this did not reduce the room occupancy or the human resource time needed . 
 mittelwerte und der gesamtmittelwert mit 5%und 95% percentilen sind dargestellt . h : min h : mm physician physicist technician 00 : 00 01 : 00 02 : 00 03 : 00 04 : 00 05 : 00 of a physician increased from 6 min in case of a ct scans without contrast enhancement to 15 min with contrast enhancement . the definition of target volumes and organs of risk ( figure 3 ) were the most time - consuming procedures for the physicians in all institutions ( 105 min ) , regardless of whether some of the contouring of the organs at risk was carried out by physicists or technicians as done in centers 3 and 4 . 
since neither the number of contoured volumes per patient was documented nor an independent quality control implemented in the study , the cause of this difference is unknown . the physical treatment planning ( figure 4 ) was the longest procedure with an average time of 198 min for the medical physicists . 
the extreme variations in centers 1 , 2 , and 3 were a consequence of the necessity multiple modifications of the treatment plan before final approval together with the physicians . the mean time required for authorization of the treatment plan ( figure 5 ) was 68 min physicists . 
this did not change the overall time compared to centers 1 and 2 . the room occupancy for treatment simulation took a mean time of 23 min ( figure 6 )  . 
center 1 used virtual simulation only ( no data )  . for the first radiotherapy including portal imaging , the mean occupancy of the linear accelerator room was 24 min ( figure 7 )  . 
evaluation of time , attendance of staff , and resources during rt for hnc patients treatment simulator , the marks for the isocenter were aligned during this procedure in all patients . 
the average time for the attendance of a physician was 7 mphysicists were present in only a few cases . routine radiotherapy sessions without portal imaging were the most frequently evaluated procedure ( n = 2 , 010 ) in all centers . 
the mean room occupancy time was 13 min and the mean working time of the technicians 24 min , indicating that on average approximately 2 technicians are present ( figure 8 )  . 
the room occupancy was 16 min on average ( figure 9 ) , which is 3 min longer than for routine radiotherapy without portal imaging ( figure 8 )  . 
the measured workload for the physician was on average 1 h 6 mhowever , one has to keep in mind that the assessed portal images were performed on a routine basis and evaluated by the physician in most cases after the radiotherapy session . 
the linac room was occupied for this procedure for 24 min on average ( figure 10 ) , which is 1.5 - times longer than for the same procedure without imrt . 
 discussion a number of national and international societies and working groups have published guidelines of needed megavolts units for a specific population and number of cancer patients , including some recommendations on the required human resources and costs of radiotherapy [ 1 , 6 , 8 , 14 , 17 , 18 , 21 ]  . 
these recommendations were based on some epidemiological considerations and surveys examining the number of actually available megavolt machines and human resources per cancer patient in a number of active radiotherapy institutes in different countries . 
 the estro project radiation therapy for cancer : quantifiphysician physicist technician 00 : 00 01 : 00 room occupancy medical staff center 2 n = 131 center 3 n = 44 center 4 n = 10 all centers n = 185 center 2 n = 131 center 3 n = 44 center 4 n = 10 all centers n = 185 figure 6 . 
mittelwerte und der gesamtmittelwert mit 5%und 95% - percentilen sind dargestellt . h : mm 02 : 00 h : mm 02 : 00 00 : 00 01 : 00 strahlenther onkol 2011 no . 
evaluation of time , attendance of staff , and resources during rt for hnc patients cation of radiation therapy infrastructure and staffing needs ( quarts ) is probably the most comprehensive project of this kind that has been published [ 1 , 17 ]  . 
in brief , quarts indicated that one linear accelerator can serve 400450 patients / year , one radiation oncologist is needed for 200250 patients / year , and one physicist is required for 450500 patients per year . 
according to quarts , in 9 out of 13 explored european countries , including large countries like germany , italy , and england , the capacity of available radiotherapy units were more than 20% below the requirements . 
the results demonstrate that the most time - consuming procedure for the physicians is the definition of target volumes ( 1h 45 min ) and for the physicists the treatment planning ( 3h 8 min ) and the authorization of the treatment plan ( 1h 8 min )  . 
the large width between the 5% and 95% percentiles for all procedures ( figures 35 ) most likely indicate in the first instance large differences in the complexity of individual cases but may also be a consequence of differences in the individual experience and diligence of physicians and physicist . 
it seems that physicians in centers 2 and 4 were able to contour the target volumes and organs at risk in approximately half of the time needed in centers 1 and 3 . 
the reasons for these discrepancies were not investigated ; however , if one adds the times of all medical staff involved into the procedures definition of target volumes , treatment planning , and authorization of the treatment plan , total times of 6h 26 min , 7h 1 min , 8h 25 min , and 2h 35 min , respectively , were observed in center 1 , center 2 , center 3 , and center 4 . 
the consistency between centers 13 in total medical staff time points out those statistical differences for the single procedures and occupational groups between these centers are mainly caused by organizational differences . 
 since the quality of the contouring and treatment planning was not independently evaluated , one cannot exclude that a part of the observed differences is associated to differences in quality . 
mittelwerte und der gesamtmittelwert mit 5%und 95% - percentilen sind dargestellt . physician physicist technician 00 : 00 01 : 00 room occupancy medical staff 00 : 00 01 : 00 02 : 00 strahlenther onkol 2011 no . 
mittelwerte und der gesamtmittelwert mit 5%und 95% - percentilen sind dargestellt . physician physicist technician room occupancy medical staff h : mm 02 : 00 h : mm 02 : 00 center 3 00 : 00 01 : 00 routine irradiation ( n = 2 , 012 ) routine irradiation with portal imaging ( n = 406 ) center 3 center 2 center 2 center 4 center 1 r = 0.80 center 1 r = 0.97 mean number of technicians present during the procedure figure 11 . 
evaluation of time , attendance of staff , and resources during rt for hnc patients however , the participating centers are convinced that the results in general are representative . at the planning ct , treatment simulator and linear accelerators , the room occupancy was measured in addition to the working time of the medical staff ( figures 1 , 2 , and 710 )  . 
although the differences between institutes appear quite substantial ( figures 1 and 2 ) , one has to take into account that a relevant number of cases were evaluated only in center 1 ( without contrast media ) and center 2 ( with contrast medium )  . 
this large discrepancy in the presence of physicians taken together with the fact that center 1 of did not use a treatment simulator is a consequence of different strategies : how the intention of this procedure can be implemented in a radiotherapy institute . room occupancy for the first radiotherapy fraction including portal imaging ( figure 7 ) showed relatively little variation between centers ( 2029 min )  . 
the engagement of only 1.2 technicians for this procedure , as in center 3 , results in a shorter time for overall medical staff , but also leads to longer room occupancy ( 29 min )  . 
again , a significant inverse correlation ( figure 11b ) was found between the number of available technicians and room occupancy , if one excludes the single and probably not representative case evaluated in center 4 . 
according to these observations , the presence of an adequate number of technicians seems to have the potential to cut down the necessary room occupancy at the linear accelerators for routine radiotherapy fractions with or without portal imaging by almost one half . 
 since in none of the centers more than 2.3 technicians were on average present , it is not known whether even shorter room occupancy can be achieved with more technicians and at which number of technicians a saturation of this effect will be observed . 
however , most of these linear accelerators are equipped with a cone beam , and the additional time needed for treatment verification by cone beam ct was not investigated in this study . 
 [ 22 ] investigated room occupancy at the linear accelerators for the first radiotherapy fractions and routine fractions for 3d and imrt cases with or without portal imaging in a mixed collective of head and neck and prostate cancer patients in a single center . 
on average , the times necessary for the different procedures in leuven were 7% ( routine radiotherapy with portal imaging ) to 33% ( routine radiotherapy ) shorter than in the evaluated german centers . 
 the data presented here allow an estimate about the required machine time and manpower needed for the core procedures of radiotherapy in an average hnc patient treated with a specific number of fractions . 
the actually required manpower will be underestimated for all occupational groups , but most pronounced for the physicians and to some extent for the physicists , because a number of necessary and time - consuming activities were not evaluated . 
evaluation of time , attendance of staff , and resources during rt for hnc patients ity assurance and mutual information , e.g. , morning rounds and periodical meetings of a number of different task forces including a part or sometimes all medical staff . 
 the presented data are a part of a larger project of the degro , in which the same evaluations were performed in other frequent cancers like breast , prostate , and rectal cancer . 
in addition , degro has started investigating the most relevant of the previously mentioned , but not yet evaluated procedures in a nondisease - specific manner to create a comprehensive database . original article dose escalation of radiotherapy for metastatic spinal cord compression ( mscc ) in patients with relatively favorable survival prognosis dirk rades1 , 3 , annika panzner1 , volker rudat2 , 3 , johann h . 
this study investigated whether patients with favorable survival prognoses benefit from a dose escalation beyond 30 gy . patients and methods : data from 191 patients treated with 30 gy / 10 fractions were matched to 191 patients ( 1 : 1 ) receiving higher doses ( 37.5 gy / 15 fractions or 40 gy / 20 fractions )  . 
all patients had favorable survival prognoses based on a validated scoring system and were matched for age , gender , tumor type , performance status , number of involved vertebrae , visceral or other bone metastases , interval from tumor diagnosis to radiotherapy , ambulatory status , and time developing motor deficits . 
diese studie untersuchte , ob patienten mit vergleichsweise guter berlebensprognose von einer dosiseskalation ber 30 gy hinaus profitieren . patienten und methoden : 191 patienten , die 30 gy / 10 fraktionen erhielten , wurden mit 191 patienten , die hhere dosen ( 37 , 5 gy / 15 fraktionen oder 40 gy / 20 fraktionen ) erhielten , verglichen ( matched - pair - analyse )  . 
die paarbildung erfolgte unter bercksichtigung folgender faktoren : alter , geschlecht , art des primrtumors , allgemeinzustand , anzahl betroffener wirbelkrper , viszerale metastasen , weitere knochenmetastasen , intervall von der erstdiagnose der tumorerkrankung bis zur bestrahlung , gehfhigkeit , entwicklungszeit motorischer defizite . 
beide grupen wurden hinsichtlich lokaler kontrolle , progressionsfreiem berleben , gesamtberleben und motorischer funktion verglichen . ergebnisse : die raten fr die lokale kontrolle nach 2 jahren betrugen 71 % nach 30 gy und 92 % nach hheren dosen ( p = 0 , 012 )  . 
die ergebnisse blieben in den multivarianzanalysen ( cox proportional hazards model ; stratified model ) signifikant 1department of radiation oncology , university of lubeck , lubeck , germany , 2department of radiation oncology , saad specialist hospital , al - khobar , saudi arabia , 3department of radiation oncology , university of hamburg , hamburg , germany , 4department of radiation oncology , medical school hannover , hannover , germany , 5department of radiation oncology , mayo clinic , scottsdale , az , usa . received : february 2 , 2011 ; accepted : june 16 , 2011 published online : october 28 , 2011 strahlenther onkol 2011 no . 
thus , this study investigated an escalation of the biologically effective radiation dose by 2023 % . introduction metastatic spinal cord compression ( mscc ) occurs in 514 % of all cancer patients during the course of their disease [ 9 , 10 ]  . 
a retrospective study suggested that a shorter course of radiotherapy such as 20 gy in 5fractions resulted in similar posttreatment motor function as longer - course radiotherapy such as 30 gy in 10 fractions or 40 gy in 20 fractions [ 15 ]  . 
however , longer - course radiotherapy resulted in better local control of mscc than shorter - course radiotherapy [ 14 , 15 ]  . in a large retrospective study , the three longer - course programs did not result in different local control rates [ 15 ]  . 
therefore , it appeared reasonable to investigate whether patients with more favorable prognoses benefit from an escalation of radiation dose beyond the standard 30 gy in 10 fractions . the survival prognoses of mscc patients can be predicted with a scoring system , which included the prognostic factors tumor type , interval between tumor diagnosis and mscc , other bone metastases , visceral metastases , ambulatory status before radiotherapy , and time developing motor deficits before radiotherapy [ 11 ]  . 
the patients were divided into five groups based on this score , a : 2025 points , b : 2630 points , c : 3135 points , d : 3640 points , and e : 4145 points . 
univariate analyse fr die lokale kontrolle . at 6 months ( % ) at 12 months ( % ) at 18 months ( % ) at 24 months ( % ) the goal of this study was to perform a matched - pair analysis and evaluate whether favorable mscc patients benefit from higher dose therapy . 
from 2 , 296 mscc patients treated with radiotherapy alone , 191 patients treated with 30 gy in 10 fractions were matched to 191 patients treated with higher doses ( 37.5 gy in 15 fractions or 40 gy in 20 fractions )  . 
the patients were matched for ten potential prognostic factors : age ( 63 versus > 63 years ) , gender , eastern cooperative oncology group ( ecog ) performance score ( 12 versus 34 ) , tumor type ( breast cancer versus prostate cancer versus myeloma / lymphoma versus lung cancer versus other tumors ) , number of involved vertebrae ( 12 versus 3 ) , other bone metastases ( no versus yes ) , visceral metastases ( no versus yes ) , interval from tumor diagnosis to mscc ( < 15 versus 15 months ) , ambulatory status before radiotherapy ( not ambulatory versus ambulatory ) , and time developing motor deficits before radiotherapy ( 17 versus > 7 days )  . 
further criteria for inclusion were mscc of the thoracic or lumbar spine , no prior surgery or radiotherapy to the involved sites , confirmation of mscc by mri , and administration of dexamethasone ( 1232 mg / day ) during radiotherapy . 
the latter was defined either as local recurrence of motor deficits , if radiotherapy led to an improvement in motor function , or as progression of motor deficits , if radiotherapy resulted in no change of motor deficits . 
motor function was evaluated before and after radiotherapy with a 5 - point scale : grade 0 : normal strength ; grade 1 : ambulatory without aid , grade 2 : ambulatory with aid , grade 3 : not ambulatory , grade 4 : paraplegia . 
1 local control , p = 0.012 time to local recurrence ( mos ) higher doses 30 gy in 10 fractions progression - free survival , p = 0.013 time to progression ( mos ) higher doses 30 gy in 10 fractions overall survival , p = 0.032 time to death ( mos ) figure 1 . 
comparison of 30 gy in 10 fractions to higher doses with respect to local control of mscc ( top ) , progression - free survival ( middle ) , and overall survival ( bottom )  . 
regarding functional outcome , univariate and multivariate analyses were performed with the ordered logit model , as the data for functional outcome are ordinal ( 1 = deterioration , 0 = no change , 1 = improvement )  . 
a total of 356 patients allowed detection of an improvement in clinical efficacy of 10 % with a statistical power of 82.5 % ( level of significance = 5 % )  . 
 the statistical power was 85 % to detect a difference of 10 % ( level of significance = 5 % ) for progression - free survival and overall survival which were evaluated for the entire cohort of 382 patients . 
on multivariate analysis , local control remained significantly associated with the radiation schedule ( relative risk [ rr ] : 2.42 ; 95 % confidence interval [ ci ] : 1.235.05 ; p = 0.011 ) , whereas visceral metastases ( rr : 2.74 ; 95 %ci : 0.936.57 ; p = 0.07 ) were not significant . 
it has been reported that longer - course radiotherapy with higher total doses resulted in better local control of mscc than shorter radiotherapy programs with lower total doses [ 14 , 15 ]  . 
because the risk of developing a local recurrence of mscc increases with life expectancy , the proportion of events was expected to be higher in the present study than in the preceding retrospective study . 
dose escalation for metastatic spinal cord compression the present matched - pair study , 9.7 % ( 37 / 382 ) of patients experienced a local recurrence of mscc , whereas in the preceding retrospective studies 4.4 % ( 34 / 764 ) of patients and 4.2 % ( 39 / 922 ) of patients treated with longer - course radiotherapy developed a local recurrence [ 13 , 15 ]  . 
patients with a short life expectancy may confound the results of a study comparing 30 gy to higher doses by masking the potential local control benefit from escalation of the radiation dose . the present study demonstrated a significant improvement in local control with doses greater than 30 gy . 
however , because this matchedpair study is based on retrospective data , a hidden selection bias cannot be completely excluded . local control and progression - free survival were only significantly associated with the radiation schedule . 
 this factor has already been demonstrated to be the strongest predictor for posttreatment motor function [ 11 , 14 , 15 ]  . in patients with a favorable survival prognosis , more intensive treatment modalities such as decompressive surgery and high - precision radiotherapy ( radiosurgery , fractionated stereotactic body radiotherapy , intensity modulated radiotherapy ) may be considered to further improve the results . 
furthermore , a recent matched - pair analysis did not reveal a significant benefit for decompressive surgery preceding radiotherapy when compared to radiotherapy alone with respect to local control , overall survival , and functional outcome [ 12 ]  . 
if high - precision radiotherapy is not available , administration of doses greater than 30 gy appears reasonable in favorable patients . conclusion in mscc patients with favorable survival prognoses , escalation of the radiation dose beyond 30 gy in 10 fractions resulted in significantly better local control , progression - free survival , and overall survival rates . 
this matched - pair study is a prerequisite for a randomized trial . original article comparison of different adjuvant radiotherapy approaches in childhood bladder / prostate rhabdomyosarcoma treated with conservative surgery frank heinzelmann1 , daniela thorwarth2 , ulf lamprecht2 , theodor w . 
kaulich2 , jrg fuchs3 , guido seitz3 , martin ebinger4 , rupert handgretinger4 , michael bamberg1 , martin weinmann1 background and purpose : multimodality treatment approaches provide high local control and satisfying overall survival ( os ) for children with localized bladder and / or prostate rhabdomyosarcoma ( bp - rms )  . 
therefore , a planning study combining organ preserving surgery with three different innovative adjuvant radiotherapy approaches was performed . patient and methods : a case of a 21 - month - old boy with bp - rms treated with polychemotherapy according to the cws 2002 - p protocol , prostatectomy , partial cystectomy , and adjuvant high dose rate brachytherapy ( hdr - bt ) was used to perform a planning study comparing hdr - bt with intensity - modulated radiotherapy ( imrt ) and intensity - modulated proton therapy ( impt ) planning . results : all modalities provide good coverage of the target volume and spare critical normal tissues . 
bt is equivalent to impt in adequately selected tumors . key words : bladder / prostate rhabdomyosarcoma childhood intensity - modulated radiotherapy brachytherapy intensity - modulated proton therapy strahlenther onkol 2011 ; 187 : 71521 doi 10.1007 / s00066 - 011 - 2261 - 3 ein vergleich dreier techniken zur adjuvanten strahlentherapie bei kindern mit rhabdomyosarkomen von blase / prostata nach blasenerhaltender , konservativer chirurgie hintergrund und ziel : die multimodale therapie von rhabdomyosarkomen von blase und prostata ( bp - rms ) in frhstadien bei kindern fhrt zu hohen lokalen kontrollraten . 
daher wurde nach organerhaltendem chirurgischem vorgehen eine planungsstudie mit drei innovativen adjuvanten strahlentherapie - strategien durchgefhrt . patient und methoden : anhand des realen falles eines 21 monate alten jungen mit bp - rms , der mit einer polychemotherapie nach cws - 2002 - p - protokoll , partieller zystektomie , prostatektomie und brachytherapie ( bt ) behandelt worden war , fhrte man eine planungsstudie durch , um die bt mit einer optimierten intensittsmodulierten radiotherapie ( imrt ) und einer protonenbestrahlung ( impt ) zu vergleichen . ergebnisse : alle drei radiotherapie - modalitten ermglichten eine gute zielvolumenerfassung und normalgewebsschonung . 
die bt ist der impt bei adquat ausgewhlten tumoren ebenbrtig . schlsselwrter : rhabdomyosarkome von blase / prostata kinder intensittsmodulierte radiotherapie brachytherapie intensittsmodulierte protonentherapie 1 department of radiation oncology , university of tuebingen , tuebingen , germany , 2 department of radiation oncology / medical physics , university of tuebingen , tuebingen , germany , 3 department of pediatric surgery , university of tuebingen , tuebingen , germany , 4 department of pediatric oncology , university of tuebingen , tuebingen , germany . received : january 21 , 2011 ; accepted : june 30 , 2011 published online : october 29 , 2011 strahlenther onkol 2011 no . 
childhood bladder / prostate rhabdomyosarcoma introduction the genitourinary tract is the second most common site for rhabdomyosarcoma ( rms ) in children [ 17 , 24 , 25 , 41 ]  . 
 although rms represents almost twothirds of all childhood sarcoma [ 27 ] , the absolute number of cases is low [ 1 ]  . the local treatment of bladder and / or prostate ( bp ) - rms is challenging . 
therefore , the vast majority of bp - rms is attributed to standard or high - risk groups , although the majority ( ~8090% ) are of embryonal histopathological subtype [ 1 , 12 , 24 , 25 , 28 ]  . 
total prostatectomy provides a good chance for local control , but is associated with a high risk of incontinence , while partial prostatectomy provides better continence rates but is associated with high rates of local relapse . to achieve organ preservation and good local control , a combination of conventional percutaneous radiotherapy and surgery is applied in many cases . 
in the largest published series yet , only 69% of all patients without cystectomy were continent , 40% had decreased renal function , and 25% had chronic hematuria [ 34 ]  . moreover , there is concern about integration of radiotherapy in very young children , which is of special relevance in children with bp - rms , since the mean age at diagnosis ranges from 2045 months [ 1 ]  . 
therefore , the introduction of novel radiotherapy techniques which provide smaller low - dose volumes compared to standard intensity - modulated radiotherapy ( imrt ) to reduce long - term adverse effects is mandatory . 
kernspintomographische tumorausdehnung eines rhabdomyosarkoms von prostata / blasenboden eines 21 monate alten jungen vor und nach abschluss von 3 zyklen chemotherapie mit i2va ( ifosfamid , dactinomycin , vincristin )  . intensity - modulated proton therapy ( impt ) and high - dose rate ( hdr ) brachytherapy ( bt )  . patient and methods case a 21 - month - old boy initially presented with urinary retention . 
 diagnostic workup with whole body gadolinium - enhanced magnetic resonance imaging ( mri ) revealed a 29 mm mass located in the prostate and the trigone of the bladder without lymph node or distant metastases ( tumor stage : ct1 cn0 m0 ; figure 1 )  . 
a biopsy was taken and confirmed the diagnosis of a rhabdomyosarcoma of the embryonal subtype . induction chemotherapy chemotherapy was started 14 days after biopsy according to the cws - 2002p protocol . 
response was evaluated after 3 cycles of i2va ( ifosfamide , vincristine , dactinomycine ) at week 8 and revealed only a poor response to chemotherapy ( mri : 24mm )  . surgery at week 9 , a total prostatectomy with partial bladder - sparing cystectomy ( complete resection without microscopic residuals ) in order to retain bladder function accompanied by reimplantation of the ureters and creation of a mitrofanoff stoma for continent intermittent catherization was performed . 
since preoperative surgical estimation indicated that partial cystectomy may lead to only small safety margins four catheters for interstitial hdr - bt were inserted during surgery ( figure 2 )  . 
bladder , rectum , testes , penis , femoral heads , and the growth plates of the pelvis and femur were defined as organs at risk . eight days after surgery hdr - bt with iridium192 was started with 3 gy per fraction prescribed to the ctv . 
implantation und rntgenkontrolle von vier kathetern fr die hdr - brachytherapie nach prostatektomie und partieller zystektomie eines blasen - / prostata - rhabdomyosarkoms . adjuvant chemotherapy twelve days after local treatment , systemic chemotherapy was continued and completed from week 13 to week 29 with 6 cycles of i2va according to the cws 2002 - p protocol . imrt and impt planning the dicom data sets and the delineated structures were transferred to the hyperion planning systeadditional margins of 15mm were added to the ctv to create a ptv for teletherapy . 
 dosevolume histograms ( dvh ) were generated for comparison of bt , imrt , and impt treatment plans . follow - up / evaluation of genitourinary late effects videourodynamic measurements , scintigraphy of the kidneys , bladder and kidney ultrasound and cystoscopy were performed during follow - up . 
 immediately after the last treatment , the catheters were removed . late effects of local therapy and evaluation or locoregional relapse the mitrofanoff stoma provided urine continence by intermittent clean catheterization 58 times per day . 
finally , 10months after completion of therapy , no fecal incontinence was reported and mri revealed no evidence of local relapse . dose distribution to organs at risk the dose distributions achieved by bt , imrt , and impt planning were compared ( figure 4 )  . 
 the pelvic and femoral growth plates and the femoral heads could be completely spared ( table 1 )  . since bt is able to generate steep dose gradients in tissue , a very satisfying sparing of the pelvic skeletal structures could also be achieved . 
the symphysis was irradiated with a mean dose of 3.1 gy ( left ) and 2.8 gy ( right ) but in all other skeletal pelvic structures mean doses below 1.3 gy could be achieved . 
 the doses in the imrt plan were three to fourfold higher ( table 1 )  . the genital organs at risk were divided into testes , penile bulb , and penile root . 
with imrt and impt planning , the penile root was contaminated with 25% of the overall dose prescribed to the reference point , while bt treatment irradiated this region with one - third of the prescribed dose . 
impt could spare testes completely , while imrt planning revealed a mean dose of 0.4 gy , whereas bt exposed them to 1 gy ( left testis : 2.78% of pdrp ) and 1.2 gy ( right testis : 3.33% of the pdrp )  . 
for the penile bulb , the results of impt were also slightly better than for imrt and bt ( table 1 )  . both bt and impt provide a significant reduction of the v2 and v5 volfigure 4 . 
imrt : intensittsmodulierte radiotherapie , impt : intensittsmodulierte protonenbestrahlung . organs at risk ( rectum , bladder , symphysis , pelvic growth plates , femoral growth plates , femoral heads , testes , penile bulb , penile root )  . 
for this purpose , mean and maximum doses as well as mean doses relative to the prescribed overall dose at the reference point ( pdrp ) were compared . the dose distribution of the bladder showed no significant differences between bt , imrt , and impt . 
this phenomenon was also verified in other organs close to the catheters ( rectum , penile root ) ( table 1 )  . with regard to rectum sparing , bt and impt were superior to imrt . 
therefore , we compared not only the absolute mean and maximum doses of each modality but also the dose relative to the prescribed overall dose . with regard to bladder sparing , all these modalities achieved comparable results . 
overall mean ( max / min ) doses on ptv and normal tissues with regard to the prescribed dose at reference point ( pdrp ) for imrt ( 44 gy ) , impt ( 44 gy ) , and brachytherapy ( 36 gy , 12 fractions )  . 
ptv und normalgewebe hinsichtlich verschriebener dosis im referenzpunkt ( pdrp ) fr imrt ( 44 gy ) , impt ( 44 gy ) und brachytherapie ( 36 gy , 12 fraktionen an 6d )  . 
a dose of 1 gy to the growth plates will not likely induce any relevant long - term effects on the skeletal structures [ 10 , 13 , 22 , 37 , 38 ]  . 
a steep dose - effect relation has been observed in a range between 15 and 30 gy [ 10 ]  . for the genital organs , bt was slightly inferior to impt and even imrt . 
however , all modalities generate doses to the testes which provide hardly any risk for inducing long - term adverse effect on endocrine function of the testes [ 37 ]  . 
normally , endocrine function is retained below doses of 12 gy [ 4 , 39 ]  . in contrast , even very low doses of radiation ( 0.1 gy ) may cause morphological and quantitative changes to spermatogonia [ 6 , 21 , 35 , 44 ]  . 
however , this concern is not supported by the limited data about late effects of bt in children [ 14 , 26 , 43 ]  . normally very high peak doses in small volumes do not translate into severe long - term adverse effects , if critical sequential organs like nerves , vessels , or urethra are spared . 
up to now , our patient has showed no relevant genitourinary or gastrointestinal late effects . although impt is able to provide favorable dose distributions [ 23 , 30 , 31 , 46 ] , the clinical data for impt in children with sarcoma are very limited [ 29 ]  . 
however , they did not observe an advantage of impt in terms of rectum sparing [ 7 ]  . a major limitation in impt is the extremely high sensitivity of the dose calculation regarding organ movements and day - to - day variations in patient positioning , which may lead to significant variations in the resulting dose distributions [ 40 ]  . 
when photon beam teletherapy is chosen , the optimization of dose distribution with imrt is also able to spare pelvic organs at risk . conclusion all three modalities provide good sparing of normal tissues . 
a main challenge for the future will be the integration of individually tailored radiotherapy strategies into the current multicenter protocols for treatment of children with rms . acknowledgments we thank markus alber for providing us with a research version of the planning system hyperion . original article erfassung mglicher verbesserungen im ablauf der strahlentherapie eine patientenbefragung felix momm1 , david joo1 , carola j . 
xander2 , sonja adebahr1 , viola duncker - rohr1 , felix heinemann1 , simon kirste1 , marc - benjamin memer1 , anca - ligia grosu1 , gerhild becker2 einleitung und hintergrund : im rahmen der qualittssicherung werden an den ablauf einer strahlentherapie zunehmend grere anforderungen gestellt . 
durch eine gezielte befragung der patienten sollten verbesserungsmglichkeiten des behandlungsablaufs aus deren perspektive identifiziert werden . patienten und methoden : mittels eines neu entwickelten fragebogens wurden in einem definierten erhebungszeitraum von 1 monat insgesamt 624 strahlentherapiepatienten ( rcklauf : n = 600 , 96 , 2% ) ber verschiedene aspekte des therapieablaufs befragt . 
weiterhin wurden bei der befragten stichprobe ausknfte ber ihre spezifischen bedrfnisse sowie vorschlge zu konkreten verbesserungsmglichkeiten im kontext einer strahlentherapeutischen behandlung erhoben . ergebnisse : insgesamt waren die patienten mit den therapieablufen zufrieden . 
zu der aussage mein erster kontakt zur klinik fr strahlenheilkunde verlief so , dass mir sowohl mit freundlichkeit als auch mit kompetenz das gefhl gegeben wurde : hier werde ich gut betreut ber 90% zustimmung . 
kostengnstigere verbesserungen wie musik im bestrahlungsraum sahen die patienten insgesamt als genauso wichtig an wie teure bauliche manahmen , beispielsweise tageslicht im bestrahlungsraupositiv hervorgehoben wurde die freundliche betreuung der patienten durch das personal . schlussfolgerungen : die situation der strahlentherapiepatienten war insgesamt zufriedenstellend . 
die strahlentherapie mit ihren komplexen ablufen kann hier als vorbild fr andere bereiche genutzt werden . schlsselwrter : strahlentherapie therapieablauf organisation patientenbetreuung lebensqualitt strahlentheronkol2011 ; 187 : 7506 doi 10.1007 / s00066 - 011 - 2264 - 0 surveyofpotentialimprovementsduringthecourseoftheradiotherapytreatmentapatientquestionnaire introduction and background : in the context of quality assurance , increasing demands are placed on the whole radiotherapy treatment process . 
it was the aim of this study to systematically ask patients about potential improvements during the course of radiotherapy treatment from their own perspective . patients and methods : in the defined time span ( 1 month ) , 624 radiotherapy patients ( 600 questionnaires were returned , 96.2% ) were interviewed using a questionnaire newly developed to inquire about several aspects of their treatment . 
furthermore , they were asked for their specific needs and suggestions for improvements that could be made during the course of radiotherapy treatment . results : overall , the patients were satisfied with the course of their radiotherapy treatment and with patient care . 
as an example , about 90% agreed with the statement : my first contact with the radiation oncology unit proceeded with kindness and competence so that i was given the impression that i will be well cared for in this clinic . 
in matters of organization radiation oncology with its complex procedures can be used as a model for other clinical departments . keywords : radiation oncology patient care organization therapy course quality of life einleitung seit mehr als 10 jahren wird in allen bereichen der medizin immer mehr wert auf die qualittssicherung gelegt . 
ber die direkten bedrfnisse des patienten , die unmittelbare auswirkungen auf den erfolg der strahlentherapie und auf seine lebensqualitt haben , gibt es verhltnismig wenige informationen [ 7 , 16 , 29 ]  . 
 vor diesem hintergrund entschlossen wir uns , alle patienten , die innerhalb eines monats in der freiburger klinik fr strahlenheilkunde behandelt wurden , ber ihre bedrfnisse zu befragen und ihnen explizit die mglichkeit zu geben , kritik zu uern oder verbesserungsvorschlge anzubringen [ 31 ]  . 
 patienten , material und methoden in einem definierten zeitraum von 4 wochen wurden alle patienten , die in die freiburger strahlentherapie kamen , mittels eines neu entwickelten fragebogens ber mgliche verbesserungen im ablauf der strahlentherapie befragt . 
die wartezeitimwartebereichbesonderserleichtern wrde meiner meinung nach 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert 6 - punkt - likert freitext 6 - punkt - likert 6 - punkt - likert freitext freitext freitext 6 - punkt - likert freitext strahlenther onkol 2011 no . 
die daten sind jedoch reprsentativ fr die in einem definierten zeitraum in der klinik tatschlich auftretenden patienten . ergebnisse demographischedaten ( tabelle2 ) die erkrankungsdaten sind nicht reprsentativ fr das gesamte in der klinik behandelte patientenkollektiv , weil sich in der nachsorbetreuungundaufklrung ( abbildung1 ) etwa 90% der patienten fhlten sich in der klinik gut betreut . 
eine groe mehrheit der patienten ( knapp 80% ) wnschte sich den kompletten zugang zu ihrer eigenen krankenakte . sehr wichtig war fr die patienten auch eine klare organisation des bestrahlungsablaufes : etwa 80% der patienten stimmten dem wunsch nach einem festgelegten bestrahlungstermin zu . 
eine wohnliche einrichtung des wartebereichs mit pflanzen oder einem aquarium sowie aktuelle zeitschriften im wartebereich wnschten sich jeweils etwa zwei drittel der patienten . stimmungderpatientenundgesamtbeurteilung ( abbildung3 ) die gesamtbeurteilung der strahlentherapie erfolgte ber die zustimmung zu der aussage : einem guten freund wrde ich eine strahlentherapie auf jeden fall empfehlen . 
mehr als 20% der patienten beantworteten diese frage nicht : whrend der studie ergab sich aus mndlichen aussagen vieler patienten , dass sie diese frage pauschal nicht beantworten knnten oder wollten und die indikation zur strahlentherapie mit einbezogen werden msse . 
etwa 70% aller patienten und mehr als 85% der patienten , die die frage beantworteten , wrde die strahlentherapie einem freund empfehlen . die antwort auf diese frage ist abhngig von der stimmung des patienten . 
15% der patienten aus dieser untergruppe verglichen mit weniger als 5% der nicht traurigen / niedergestimmten patienten wrden die strahlentherapie einem guten freund nicht empfehlen ( p < 0 , 0001 , chi - quadrat - test )  . 
158 patienten uerten sich zu punkten , die sie am meisten gestrt hatten , 237 uerten sich zu besonders positiven erlebnissen . als verbesserungsmglichkeit im bestrahlungsraum wurde hufig eine insgesamt freundlichere einrichtung genannt . 
verbesserungen im ablauf der strahlentherapie meine stimmung zur zeit ist traurig und niedergedrckt . diskussion einem guten freund wrde ich eine strahlentherapie auf jeden fall empfehlen . alle patienten traurige / niedergestimmte patienten patienten nicht traurige / niedergestimmte patienten 100% frage nicht beantwortet stimmt eher nicht stimmt nicht stimmt berhaupt nicht stimmt genau stimmt stimmt grtenteils * p < 0 , 0001 abbildung3 : allgemeine zufriedenheit in abhngigkeit von der stimmung der patienten ( n = 600 )  . figure3 : general satisfaction in relation to patients mood ( n = 600 )  . zelne patienten kritisierten die niedere raumtemperatur . 
 die weitaus meisten patienten berichteten von der persnlichen betreuung durch die mtras und rzte als positivstes erlebnis whrend ihrer therapie : in etwa 200 / 237 freitext - antworten wurden als besonders positiv die freundlichkeit und zuwendung des personals genannt . 
die exzellente rcklaufquote von mehr als 96% kam durch das studiendesign mit direkter betreuung durch einen doktoranden und mithilfe aller kollegen der abteilung zustande . ein erheblicher teil ( 38 , 8% ) der befragten patienten rekrutierte sich aus der spten nachsorge , d.h. 
auf diese weise kann die patientengruppe in die richtung von patienten mit besserer prognose und in besserem allgemeinzustand selektiert worden sein . zufriedenheitderpatientenmitderkommunikation insgesamt fhlten sich die patienten in der klinik gut betreut . 
wenn man das aufklrungsgesprch in die drei hauptteile ablauf der therapie , erkrankung und prognose sowie nebenwirkungen einteilt , waren die patienten mit der aufklrung ber die nebenwirkungen im vergleich am wenigsten zufrieden . 
der grund hierfr kann sein , dass die nebenwirkungen komplex zu erklren sind und dass im gesprch sehr hufig auch auf seltene , aber erhebliche nebenwirkungen eingegangen werden muss , die spter gar nicht auftreten [ 20 , 2223 , 25 ]  . wichtige grundlage fr die kommunikation zwischen arzt und patient ist die zeit , die der arzt fr den patienten aufwenden kann , und die erreichbarkeit des arztes . 
die erfahrung zeigt , dass die zeit fr das patientengesprch in jedem fall sehr gut investiert ist : ein gut aufgeklrter patient ist sicherer , muss weniger rckfragen stellen und toleriert z.b. 
explizit angekndigte nebenwirkungen sehr viel leichter [ 9 ]  . die patienten wurden auerdem gefragt , ob ihre angehrigen gengend in den beratungsprozess integriert wurden [ 6 , 13 , 14 , 26 ]  . 
verbesserungen im ablauf der strahlentherapie strahlentherapiepatienten wurde bereits in einer anderen studie ausfhrlich behandelt [ 17 ]  . wnschederpatientenbezglichderorganisation fr die oft mehr als 30 termine einer bestrahlungsbehandlung ist eine gute organisation unabdingbar . 
gerade in der strahlentherapie sind deshalb edv - technische betriebsablaufsysteme auch zur entlastung des personals von hohem nutzen [ 12 , 24 , 27 ]  . der hohe technische aufwand fr eine strahlentherapie bedingt die bildung groer zentren und damit hufig weite anfahrtswege zur therapie . 
eine mglichkeit , auch diese 20% der patienten zufrieden zu stellen , erscheint die bildung von filialen groer strahlentherapieeinrichtungen zu sein der filiale kann dezentral , ohne greren reiseaufwand , eine basis - strahlentherapie angeboten werden , die gleichzeitig vom zentrum bezglich der qualitt berprft und mit einem ausfallkonzept abgedeckt wird . die frage , ob sie die bestrahlungsrumlichkeiten in der nachsorge nicht mehr betreten wollten , wurde von den patienten sehr uneinheitlich beantwortet . 
eine mehrheit empfindet es aber als nicht strend , zur nachsorge nochmals an den ort der therapie zurckzukehren . ganz anders stellt sich die situation bei der frage nach dem zugang zur eigenen krankenakte dar . 
dies sollte bei verhandlungen mit den gerteherstellern ber wartungsvertrge und wartezeiten auf die techniker bercksichtigt werden . keine anderen fragen wurden von den patienten uneinheitlicher beantwortet als die nach verbesserungen durch musik oder tageslicht im bestrahlungsraujeweils etwa die hlfte der patienten sprach sich fr oder gegen die jeweilige manahme aus . 
im falle der musik knnte man dem patienten ein individuelles angebot machen , obwohl in vielen fllen die eigentliche therapiezeit so kurz ist , dass man kein komplettes musikstck hren kann . 
zustzliche vorschlge wie trinkwasserspender oder ein kaffeeautomat wurden in der eigenen klinik trotz anfnglicher bedenken wegen entsprechender hygienevorschriften bereits umgesetzt . gesamtbeurteilungundstimmungderpatienten die gesamtbeurteilung der strahlentherapie wurde nicht durch eine direkte benotung , sondern durch die indirekte frage nach der empfehlung fr einen guten freund abgefragt . 
 dieses sehr gute ergebnis wurde jedoch vermutlich durch das problem beeinflusst , dass eine nicht - empfehlung aus der sicht des patienten das eingestehen einer eigenen fehlentscheidung ( nmlich fr die strahlentherapie ) bedeutet htte . 
dass knapp ein drittel aller patienten , die sich in einer radioonkologischen klinik aufhalten ber traurigkeit und niedergestimmtheit berichten , zeigt erneut die absolute notwendigkeit des angebotes einer psychoonkologischen beratung in einer solchen einrichtung [ 2 ]  . 
am einfachsten kann dieser forderung im rahmen eines tumorzentrums oder eines onkologischen schwerpunktes entsprochen werden . schlussfolgerungen insgesamt waren die patienten mit den im fragebogen angesprochenen aspekten der versorgung und organisation zufrieden . 
arnegger2 , hans - ulrich kauczor1 , peter hallscheidt1 purpose : to compose diagnostic standard operating procedures for both clinical and imaging assessment for vulvar and vaginal cancer , for vaginal sarcoma , and for ovarian cancer . methods : the literature was reviewed for diagnosing the above mentioned malignancies in the female pelvis . 
imaging of female pelvic malignancies with mri , ct , and pet / ct ( part 2 ) introduction the prognosis in women with gynecologic malignancies like vulvar and vaginal cancer or ovarian cancer not only depends on local tumor spread but also on a wide range of additional findings , such as positive lymph nodes , ascites , or distant metastases . 
cross - sectional imaging modalities , including ultrasound ( us ) , computed tomography ( ct ) , and magnetic resonance imaging ( mri ) have increasingly been used for optimal treatment planning in gynecologic malignancies . 
their staging criteria are based on the well - established international federation of gynecologists and obstetricians ( figo ) staging system and the tnm classification system [ 33 , 42 ]  . 
positron emission tomography ( pet ) , especially if combined with ct ( pet / ct ) might have a benefit in staging and restaging gynecological malignancies , especially regarding lymph node metastases or recurrent tumor due to the simultaneous availability of functional and anatomical information [ 10 , 27 , 30 , 37 ]  . 
in addition , because the differentiation of recurrent tumor and radiation fibrosis is challenging on ct , mri has become the most valuable imaging tool for diagnosing pelvic tumors in women [ 26 ]  . 
due to a wide variety of possible imaging sequences , high spatial resolution , and superior soft tissue contrast , nonenhanced mri can often already provide sufficient information without the need of contrast agent application . 
due to its positioning inside the rectum , the endorectal coil provides more reliable tissue differentiation of all pelvic organs due to the high spatial resolution in a smaller field of view ( fov ) at 1.5 t [ 22 , 29 , 35 , 38 ]  . 
whereas the ct presents precise and clear 3d information regarding a patients geometrical data and electron density distribution , mri has , due to its good soft tissue differentiation , advantages in defining the tissue volume needing figure 1 . 
mri with high spatial resolution in the transversal plane : hyperintense mass of the left labia in the t2 - weighted sequence , longest diameter less than 2 cm ( white arrow )  . 
imaging of female pelvic malignancies with mri , ct , and pet / ct ( part 2 ) radiation ( gross tumor volume ( gtv ) , clinical target volume ( ctv ) , and planning target volume ( ptv ) ) [ 39 ]  . 
 for the aforementioned female pelvic malignancies , operating procedures and mri findings are described in detail in the following , while complementary information about ct and pet / ct findings is mentioned . 
however , imaging modalities play an essential role in assessing the infiltration depth into surrounding tissues , positive lymph nodes , ascites , and distant metastases [ 19 ]  . 
whereas ct is mainly employed for the assessment of lymph nodes , distant metastases , and peritoneal carcinomatosis , mri appears to be superior for imaging the local situation in cases where other diagnostic options such as cysto or rectoscopy are impracticable due to tumor size . 
t2 - weighted turbo spin echo ( tse ) sequences with high spatial resolution in the sagittal and transversal oblique ( short urethral axis for vulvar cancer and short vaginal axis for vaginal cancer ) planes are essential ; additionally , t1 - weighted tse images in sagittal and transversal plane with and without contrast enhancement are recommended ( table 2 )  . 
the degree of infiltration of the urethra is relevant for the tumor staging and can be ideally evaluated in t2 - weigted sequences with high spatial resolution in sagittal and transversal oblique ( short axis of the urethra ) plane . 
because of the hypointense presentation of the fat layer around the urethra , fat saturation at t1 - weighted sequence is not helpful ( figures 1 and 2 ) [ 46 ]  . 
according to the international federation of gynecology and obstetrics , a squamous cell carcinoma occurring within 5 years of treatment for a vulvar or cervical cancer is considered a recurrence of the vulvar or cervical tumor rather than a new primary focus [ 44 ]  . 
primary cancer of the vagina , i.e. , squamous cell carcinomas , has a low incidence ( 0.7 / 100 , 000 women ; < 2% of all female malignant genital tract cancers ) and is diagnosed in 15% of malignant vaginal tumors . 
 diagnostic standard operating procedure besides the standard procedures such as gynecological and colposcopic examinations and cytological biopsy , further imaging , e.g. , mri or ct , requires individual discussion and is not explicitly recommended by recent guidelines ( table 3 ) [ 1 ]  . 
figo : international federation of gynecology and obstetrics , tnm : tumor , node , metastasis . vaginal cancer vaginal wall paravaginal tissue pelvic bone mucosa of bladder and / or rectum , beyond pelvis regional lymph node metastases distant metastases figo strahlenther onkol 2011 no . 
imaging of female pelvic malignancies with mri , ct , and pet / ct ( part 2 ) radiological findings since the vaginal cavity normally appears collapsed , instillation of sterile ultrasound gel is recommended before starting the mr examination . 
in the mri , the vagina presents in its typical three layer formation : mucosa ( t1 - weighted hypointense , t2weighted hyperintense ) ; submucosa and muscularis layer ( t1 - weighted and t2 - weighted hypointense ) , and adventitia ( t1 - weighted and t2 - weighted hyperintense ) [ 11 ]  . 
in a t2 - weighted image , the cancer appears highly hyperintense , in which case a t2 - weighted transversal oblique and sagittal sequence should be performed to verify the tumor size and any infiltration into surrounding structures ( table 2 ) [ 17 ]  . 
a large multicystic intraabdominal mass with solid parts and papillary growth ( top to bottom ) in a t2 - weighted haste sequence ( single shot technique ) in the transversal plane , in the t1weighted fl2d sequence ( gradient spoiled ) in the transversal plane , and in the t1 - weighted fl3d sequence ( gradient spoiled ) fat saturated in the transversal plane after gd i.v. , and in the t2 - weighted tirm ( turbo inversion recovery magnitude ) sequence in the coronal plane . 
groe multizystische raumforderung des ovars mit soliden anteilen und papillrem wachstum in der t2w haste transversal , in der t1w fl2d transversal , in der t1w fl3d fs transversal nach kontrastmittelgabe und in der t2 tirm koronal . 
t2 - weighted sequence in the sagittal plane with high spatial resolution , non - enhanced t1 - weighted sequence in the transversal plane , and t1 - weighted fl2d ( gradient spoiled ) fat saturated post gd i.v. 
 radiological findings due to tumor necrosis and hemorrhage , rhabdomyosarcoma presents as an inhomogeneous structure in the mri hypointense signal prevails in t1 - weighted sequences and hyperintense signal in t2 - weighted sequences . 
regarding leiomyosarcoma of the vagina , which is often already palpable due to fast tumor growth and large size , mr images may reveal an extensive tumor mass in the pelvis . 
vaginal leiomyosarcoma presents as a cystic tumor with solid parts , characteristically showing an irregular and infiltrative growth pattern with moderate hypointensity in t1 - weighted sequences and increased hyperintensity in t2 - weighted sequence as well as after contrast [ 45 ]  . 
 primarily cystic primarily solid mucinous cystadenoma ( benign ) serous cystadenoma ( benign ) adenocarcinoma ( malignant ) fibroma ( benign ) brenner tumor ( usually benign ) granulosa cell tumor ( malignant , produces estrogen ) thecoma ( benign , produces estrogen , occasionally androgens ) sertoli - leydig cell tumors ( generally benign , may produce androgens and / or estrogen ) dysgerminoma ( malignant ) mixed type dermoid ( teratoma , usually benign , may produce thyroid hormone ) clear cell carcinoma ( usually malignant ) adenocarcinoma ( malignant ) endometrioid carcinoma ( malignant ) table 5 . 
the capsule , or outer wall of the tumor , is intact , there is no tumor on the ovarian surface , and there are no cancer cells in ascites or peritoneal washings tumor is limited to both ovaries . 
the capsule is intact , there is no tumor on the ovarian surface , and there are no cancer cells in ascites or peritoneal washings tumor is limited to one or both ovaries with any of the following : ruptured capsule , tumor on ovarian surface , or cancer cells in the ascites or peritoneal lavage . tumor involves one or both ovaries with pelvic extension extension and / or implants on uterus and / or tube ( s ) ; no malignant cells in ascites or peritoneal washings extension to other pelvic tissues ; no malignant cells in ascites or peritoneal washings pelvic extension ( 2a or 2b ) with malignant cells in ascites or peritoneal washings tumor involves one or both ovaries with microscopically confirmed peritoneal metastases outside the pelvis and / or regional lymph node metastases microscopic peritoneal metastasis beyond pelvis macroscopic peritoneal metastasis beyond pelvis , 2cm or less in greatest dimension peritoneal metastases , more than 2 cm in greatest dimension and / or regional lymph node metastases distant metastases ( excludes peritoneal metastases ) iiia iiib iiic contrast - enhanced ct can only give an overview about infiltrated structures and may detect distant metastases , ascites , or suspicious lymph nodes , but primary tumor will only present as an inhomogeneous mass without characteristic morphologic criteria [ 26 ]  . pet / ct may be significantly important for grading , staging , and followup in sarcomas [ 5 ]  . ovarian cancer general information the category of ovarian tumors consists of diverse entities with a wide morphological spectrum of ovarian and testicular stroma - type cells . 
there is a high growth - related tendency of rotation and , thus , constriction of the vascular stalk , leading as a consequence to ovarian necrosis ( table 4 )  . 
mri with t2 - weighted tirm ( turbo inversion recovery ) in the coronal plane , t2 - weighed in the transversal plane with high spatial resolution and t1 - weighted sequence fl2d ( gradient spoiled ) non - enhanced , in the transversal plane and with fat saturation after gd i.v. 
zystische raumforderung des linken ovars mit soliden anteilen , im mrt dargestellt in der t2w tirm koronal , in der t2w tse transversal , in der nativen t1w transversal und in der kontrastmittelgesttzten t1w fl2d ( fs ) koronal . 
between the ages of 4044 , the incidence of ovarian cancer ranges around 15 / 100 , 000 women , whereas it is about 57 / 100 , 000 in women aged 7074 [ 34 ]  . 
t2w : t2gewichtet , t1w : t1 - gewichtet , tra : transversal , sag : sagittal , cor : koronal , fs : fettgesttigt , tr : repetitionszeit , te : echozeit , fov : field of view , gd : gadolinium.. sequence plane fs tr ( ms ) te turbo spin echo turbo spin echo turbo spin echo short t1 inversion recovery incoherent gradient echo ( gradient spoiled ) 3d native , gd i.v. 
imaging of female pelvic malignancies with mri , ct , and pet / ct ( part 2 ) ovarian cancer correlates directly with the overall tumor stage [ 13 , 32 ]  . diagnostic standard operating procedure according to recent german guidelines , transvaginal ultrasound is the option of choice for diagnosing ovarian malignancies , and surgery appears to still be the most reliable staging modality for ovarian cancer and cannot , at least not now , be replaced by any imaging modality ( table 5 ) [ 2 ]  . 
 nevertheless , according to international guidelines , ultrasound plays a role in visualizing and characterizing ovarian tumors , whereas ct is the imaging modality of choice for preoperative evaluation of ovarian cancer and mri , with its excellent tissue contrast , for defining the tumor entity [ 21 ]  . 
in higher tumor stages ( t3 , t4 ) , however , studies found no statistical differences between ct and mri in defining disease extent [ 21 , 26 ]  . 
 radiological findings transvaginal ultrasound is the basic imaging tool used for diagnosing ovarian cancer , but multidetector ct is essential for the staging of ovarian cancer correctly , especially regarding metastases of lung , bones , and lymph nodes . 
 high resolution mri offers additional information for soft tissue differentiation , especially in t2 - weighted sequences , and is superior to ct for pelvic imaging ( table 6 )  . 
in mri , cancer of the ovary can be evaluated in t2 - weigted tse sequences in the transversal plane with high spatial resolution and t1 - weighted images in the transversal plane in three sequences ( nonenhanced , fat suppressed , and contrast enhanced ) to identify the different components of the tumor ( table 7 ) [ 14 ]  . 
after application of gd i.v. , mri allows for better differentiation between benign and malignant tumors by revealing necrotic areas , septa and cysts , papillary growth , peritoneal , omental , or lymph node metastases [ 14 , 26 ]  . 
in addition with ct , malignancy may be reasonably suspected in any cystic ovarian mass with solid components , tumor diameter greater than 4 cm , thickness of a cyst wall greater than 3 mm , or nodular structure ( figures 37 ) [ 7 , 26 ]  . 
 conclusion female pelvic malignancies are more frequently visualized with cross - sectional imaging modalities like mri and ct for further treatment planning , whereas ultrasound still remains the gold standard in diagnosis . 
imaging of female pelvic malignancies with mri , ct , and pet / ct ( part 2 ) menting basic gynecological diagnostics such as inspection , palpation , and ultrasound . ct provides important information about accompanying peritoneal implants , affected lymph nodes , ascites , or distant metastases ( e.g. , of the lung and the liver ) and is widely used for abdominal staging and restaging of ovarian cancer , although it has a poor soft tissue contrast in the entire pelvis . 
 according to the literature , pet / ct is beneficial in visualizing involved abdominal lymphatic pathways and might be helpful for restaging of recurrent tumor or distant metastases , especially in ovarian cancer or sarcomas . 
t2 - weighted and t1 - weighted sequences with high spatial resolution in the transversal plane and contrast - enhanced t1 - weighted sequence in the transversal and sagittal planes . 
 appearance cystic and solid , often papillary growth multilocular cystic with papillary growth in the cysts ovarian tumor signal t2 malignant epithelial tumor higher serous cystadenocarcinoma mucinous cystadenocarcinoma multilocular cystic with solid parts and nodular areas in the cyst lumen higher pseudomyxoma peritonei endometrioid carcinoma clear cell carcinoma multicystic mass with mucinous fluid large , cystic mass with few solid parts , often bilateral mostly unilocular , large cyst with enlarged cyst wall and multiple nodular changes or multilocular cystic mass high high high signal t1 high intermediate to low intermediate to low low to very high immature teratoma dysgerminoma granulosa cell tumor sertoli - leydig cell tumor solid tumor mass with necrosis and hemorrhage , diffuse calcifications , fat areas multilobular , solid lesion with prominent fibrovascular septical structures , central necrosis and hemorrhage in large tumors diffuse calcifications multilocular cystic to solid heterogeneous appearance , no papillary growth hemorrhage in the tumor , infarction , fibrous degeneration solid mass , lobular , cystic lymphoma secondary tumor ( metastasis ) solid , homogeneous mass , mostly bilateral , no ascites krukenberg tumor : oval to kidneylike shape , solid , central necrosis or cystic , contains mucinous mass , bilateral high high ( fat ) intermediate to low ( septum ) high ( necrosis ) high higher ( cysts ) intermediate to high ( solid parts ) intermediate to low intermediate intermediate heterogeneously , low to intermediate strahlenther onkol 2011 no . 
imaging of female pelvic malignancies with mri , ct , and pet / ct ( part 2 ) original article dysphagia impact on quality of life after radio ( chemo ) therapy of head and neck cancer julia maurer1 , matthias hipp1 , christof schfer2 , oliver klbl1 background : in the past , xerostomia was considered one of the most important determining factors of quality of life ( qol ) after radiotherapy ( rt ) of the head and neck region . 
 patients and methods : between september 2005 and august 2007 , 35 patients with locally advanced squamous cell carcinoma of the head and neck region were included in the prospective study . 
this means in particular to not only spare the parotids while planning the irradiation , but also to take into consideration the important structures for deglutition , like the retropharyngeal muscles . key words : carcinoma of the head and neck radiotherapy dysphagia quality of life strahlenther onkol 2011 ; 187 : 7449 doi 10.1007 / s00066 - 011 - 2275 - x dysphagie einfluss auf die lebensqualitt nach radio ( chemo ) therapie bei kopf - hals - tumoren hintergrund : die xerostomie galt in der vergangenheit als einer der wichtigsten determinierenden faktoren der lebensqualitt ( lq ) nach bestrahlung der kopf - hals - region . 
 patienten und methoden : 35 patienten mit lokal fortgeschrittenen plattenepithelkarzinomen der kopf - hals - region wurden zwischen 09 / 05 und 08 / 07 in die prospektive studie eingeschlossen . 
insbesondere der globale gesundheitszustand und die globale lq wurden sowohl nach abschluss der behandlung ( p = 0 , 033 ) als auch im weiteren verlauf ( p = 0 , 050 ) negativ beeinflusst . schlussfolgerung : die ergebnisse dieser arbeit sollten anlass sein , zuknftig einer strukturierten diagnostik , therapie und rehabilitation von schluckstrungen mehr bedeutung zukommen zu lassen und insbesondere bei der bestrahlungsplanung nicht nur wert auf die schonung der parotiden , sondern auch auf die der am schluckakt beteiligten strukturen , wie z.b. 
der retropharyngealen muskulatur , zu legen . schlsselwrter : kopf - hals - tumoren strahlentherapie dysphagie lebensqualitt 1department of radiotherapy , regensburg university medical center , regensburg , germany , 2department of radiotherapy , hospital st . 
elisabeth straubing , straubing , germany received : february 21 , 2011 ; accepted : july 21 , 2011 published online : october 28 , 2011 strahlenther onkol 2010 no . 
dysphagia and qol after radio ( chemo ) therapy of h&n cancer introduction scoring in previous assessments of the shortand long - term adverse reactions caused by radiotherapy of the head and neck region , xerostomia was viewed as the most important determining factor of quality of life . 
the main focus of the present paper was to elaborate on the influence of dysphagia on the quality of life [ 6 , 29 , 30 , 32 ]  . 
 patients and methods patients a total of 35 patients with squamous cell carcinoma of the head and neck , who were irradiated between september 2005 and august 2007 , were considered in the present study . 
at the beginning of the therapy , data of 35 patients were evaluated , at the end of therapy data of 34 patients , after 6 months data of 24 patients , and after 12 months of followup data of 21 patients . 
discomfort caused by dysphagia already increased in week 1 of treatment ( median i , p < 0.01 ) and reached its maximum at the end of week4 ( median ii )  . 
at the end of therapy , the majority ( 80% ) of the patients needed a feeding tube for additional alimentation ; 30% were wholly dependent on a feeding tube . 
these values did not change at the 12 - month follow - up . regarding dysphagia , there was no significant difference between adjuvant versus the primary treated patients . patients who had received simultaneous chemotherapy differed significantly from those who had not . 
what is more , an impact on appetite could be shown after 12 months due to the dysphagia ( p = 0.041 , r = 0.440 ) , but there were no additional significant impacts of single items in the questionnaire . 
dysphagia and qol after radio ( chemo ) therapy of h&n cancer acute dysphagia ; 76% of their patients suffered from acute dysphagia after radiotherapy or radiochemotherapy ( 35% moderately to severe )  . 
however , only 70% of the patients in this study were simultaneously treated with chemotherapy . in the literature , various factors ( e.g. , concomitant chemotherapy ) exert considerable influence on dysphagia and quality of life [ 20 ]  . 
 [ 18 ] presented results similar to this survey in a retrospective study about the treatment of larynx and hypopharynx carcinoma with concomitant platinum - based chemotherapy and imrt with 31 patients , measuring the acute and late side effects by means of ctc criteria . 
therefore , the control of dysphagia is of great importance . in the past , xerostomia was viewed as the most important factor of the quality of life after radiotherapy of the head and neck region [ 8 , 11 , 31 ]  . 
since the implementation of imrt has led to a decrease of ray - induced xerostomia , dysphagia has become one of the most important clinical side effects of radiotherapy in the head and neck region [ 15 ]  . 
more than a third of the patients use feeding tubes before , during , and also after the treatment [ 23 ]  . because of these well - known problems , the installation of a feeding tube was in many cases already recommended before starting therapy . 
in general the number of cases reporting dysphagia in the current literature is mostly slightly higher than in this survey showing dysphagia in about 50% of the cases after 6 and 12 months ( 15% moderate to severe ) [ 23 , 25 , 28 ]  . 
 [ 17 ] showed the following results : the quality of life according to the reports given by the patients was mostly influenced by xerostomia and the difficulty in swallowing . 
with 116 head and neck patients , the correlation between xerostomia and the items of qlq - c30 eortc after radiotherapy was not as distinctive as between the other toxicities as dysphagia and hoarseness . 
 [ 14 ] showed in a small prospective study that significant correlations exist between the objective and subjective difficulties in swallowing function and the dosevolume histogram parameters of the anatomical structures . 
a suggestion for further research includes the question of how to achieve the sparing of the structures which appear to have a positive impact on deglutition . original article pet - guided dose escalation tomotherapy in malignant pleural mesothelioma andrei fodor , claudio fiorino , italo delloca , sara broggi , marcella pasetti , giovanni mauro cattaneo , luigi gianolli , riccardo calandrino , nadia gisella di muzio purpose : to test the feasibility of salvage radiotherapy using pet - guided helical tomotherapy in patients with progressive malignant pleural mesothelioma ( mpm )  . patients and methods : a group of 12 consecutive mpm patients was treated with 56 gy / 25 fractions to the planning target volume ( ptv ) ; fdg - pet / ct simulation was always performed to include all positive lymph nodes and mpm infiltrations . 
subsequently , a second group of 12 consecutive patients was treated with the same dose to the whole pleura adding a simultaneous integrated boost of 62.5 gy to the fdg - pet / ct positive areas ( btv )  . 
no grade 3 ( rtog / eortc ) acute or late toxicities were reported in the first group , while 3cases of grade 3 late pneumonitis were registered in the second group : the duration of symptoms was 210 weeks . 
danach wurde eine zweite gruppe von 12 aufeinanderfolgenden patienten mit der gleichen dosis auf der gesamten pleura behandelt mit gleichzeitigemintegriertem boost von 62 , 5 gy auf die fdgpet / ct - positiven bereiche ( btv )  . 
in der ersten gruppe wurde keine akute oder spte grad - 3 - toxizitt ( rtog / eortc ) berichtet , whrend drei flle von spter grad - 3 - pneumonitis in der zweiten gruppe auftraten . 
es wurde signifikanter einfluss der strahlentherapie auf lokalrezidive beobachtet ( mediane zeit bis zum lokalrezidiv : 8 vs 17 monate ; rate 1 - jhriger lokalrezidivfreiheit : 16% vs 81% , p = 0 , 003 )  . 
helical tomotherapy in malignant pleural mesothelioma introduction there is no clear consensus on the optimal treatment of malignant pleural mesothelioma ( mpm ) , a multifocal or extensive disease on the pleural surface at the time of detection . 
despite the lack of controlled / randomized trials using combined treatments , the so - called trimodality therapy ( extrapleural pneumonectomy + adjuvant chemotherapy + radiotherapy ) has been adopted as the standard of care , based on a number of institutional experiences claiming improved outcome compared to the surgery alone approach [ 18 , 30 , 32 , 36 ]  . 
however , due to advanced disease at the time of diagnosis , most patients are considered to be unresectable [ 29 , 36 , 39 ] and are generally candidates for chemotherapy or palliative treatment . 
 the role of radiotherapy has not yet been clearly assessed but its impact has been claimed for the trimodality therapy [ 8 , 25 , 27 , 28 , 38 ] , suggesting that more aggressive local treatment with high radiation doses could provide some benefit . 
recent developments in the field of intensitymodulated and image - guided radiotherapy have led radiation oncologists to reconsider the role of radiotherapy , also for unresectable patients [ 1 ] , thanks to the greatly improved possibility of closely tailoring the dose distribution around the target [ 26 , 34 , 35 ]  . 
 based on these considerations , a feasibility study using high - dose image - guided tomotherapy was conducted at our institute in unresectable patients . materials and methods study design a two - step nonrandomized , dose escalation pilot study was performed with the aim of achieving good palliation in progressive disease ( pd ) patients . 
the patients included were not previously irradiated on the ipsilateral pleura / lung and showed ct / pet progression / relapse after the previous treatments ( surgery and / or chemotherapy )  . 
the optimal total dose , dose per fraction , and timing have not yet been defined for mpm patients , although there is some hope of improving local control by treatment acceleration . 
for this reason , and in order to reduce the hospitalization time , a moderately hypofractionated regimen was chosen ; the median prescribed dose to the planning target volume ( ptv ) was 56 gy in 25 fractions ( 2.24 gy / fraction ) [ 13 ] , approximately equivalent to a 2gy equivalent dose ( eqd2 ) around 60 gy , which is generally considered appropriate in many institutions . 
the dose prescription was 56 gy in 25 fractions to the ptv , while concomitantly delivering 62.5 gy to the pet - positive subvolumes ( named biological target volume , btv )  . 
thus , the btv could receive an eqd2 up to approximately 70 gy . patients characteristics the main patients characteristics are shown in table 1 ; the two groups ( no - sib and sib ) were quite homogeneous . 
the following surgeries were performed : 1 extrapleural pneumonectomy , 4pleurectomy / decortications , and 7biopsy / talc pleurodesis in the no - sib group , and 7pleurectomy / decortication and 5 biopsy / talc pleurodesis in the sib group . 
in the no - sib group , 10 patients received permetrexed - based chemotherapy , 1 patient received gemcitabinecisplatin , and 1patient with a previous gastrointestinal stromal tumor ( gist ) , in treatment for table 1 . 
two of the patients of the sib group , 1patient with talc pleurodesis and the other with biopsy only , did not receive chemotherapy , one of them due to renal failure . 
all patients were in progressive disease without other therapeutic options . imaging , contouring , and planning procedures the role of fdg - pet / ct in the definition of the target volume in the radiotherapy of mpm is not mentioned even in the most recent papers [ 22 ] , although some publications have shown that pet could play an important role in mpm diagnosis [ 4 , 16 ] and its prognostic value has been demonstrated [ 5 , 33 ]  . 
recent studies have shown that fdg - pet allows the stratification of the patients for surgical treatment [ 14 , 37 ] and permits the early prediction of chemotherapy response and survival [ 15 ]  . it was upon this evidence that we based the delineation of the clinical target volume ( ctv ) on fdg - pet / ct images taken for planning purposes with the patient in the same treatment position . 
patients were treated in the supine position , with their arms up on a wing - board and were asked to breathe normally during ct / pet acquisition and treatment . 
an isotropic margin of 10 mm in all directions was added to ctv to create the ptv . in the sib group , the ctv to ptv margin was reduced to 0.5 cm in all directions except the craniocaudal , where 0.8 cm was added , due to the improved confidence in applying daily set - up correction with megavoltage ct ( mvct ) image guidance , performed for every patient . 
ptv - oar overlaps for esophagus , heart , or spinal cord were used to limit the dose to 56 gy , 56 gy , and 50 gy , respectively . 
 normal tissue constraints from published intensity - modulated radiotherapy ( imrt ) studies [ 1 , 2 , 21 ] were adopted ; in addition , planning optimization was always stressed to obtain the lowest dose possible for every oar without compromising target coverage , an approach that we usually follow during tomotherapy optimization [ 7 , 11 , 12 ]  . 
a followup schedule with pet / ct at 4months after radiotherapy was planned in order to limit the influence of inflammatory phenomena ; then , contrast - enhanced thoracic ct ( ct ) and pet / ct were alternated every 4months . 
toxicities were defined according to radiation therapy oncology group ( rtog ) and european organization for research and treatment of cancer ( eortc ) criteria [ 9 ] ; the students t test and x test were used for comparing the characteristics of the two groups and the rates of different toxicities . 
 overall , cancer - specific and relapse - free survival curves were calculated from the first day of radiotherapy until either the date of death / relapse or the date of last follow - up with the kaplan meyer method . 
the impact of a number of variables , including dose ( no - sib group vs sib group ) , gender , location ( leftright ) , stage ( iii vs iiiiv ) , chemotherapy , type of surgery ( radical vs nonradical ) , age , and treatment duration , was assessed using logrank tests . 
median time between diagnosis and radiotherapy was 11months ( range , 620months ) for the no - sib group and 14 months ( range , 243 months ) for the sib group . 
apart from follow - up duration , no other characteristics of the two subgroups reported in table 1 significantly differ . planning data a summary of the relevant dosimetric data is reported in table 2 . 
the sparing of the main organs at risk was excellent in both groups ; in particular , the mean contralateral lung dose was very low ( < 8 gy )  . 
the long surviving patients ( > 12months ) of the sib group presented hemithoracic fibrosis at ct ; 3of these patients also presented a deviation from the axis in the direction of the disease . 
 when comparing the two groups , acute grade 2 dermatitis and late grade 3 pneumonitis were increased in the sib group ( p = 0.07 ) : considering all pulmonary symptoms , 6 of 12 experienced late grade 23 toxicity . 
this result is probably due to the fact that patients with smaller tumor volumes show some functioning of the lung , while the lung of the patients with a large btv had already been compromised . control and survival analysis in the no - sib group , the response was assessed with pet / ct in 7 patients and with contrast enhanced ct in 2 patients ( 3 died prior to the first follow - up )  . 
 athe radiation pneumonitis symptoms began 26 weeks after the end of radiotherapy than that of the no - sib group ( p = 0.01 ) , which could explain the increase in lung toxicity . the largest btv at fdg - pet / ct was registered in the second group ; it was 900 ml in a patient with a 43 - month inin the sib group , all patients underwent pet / ct evaluation . 
spte pulmonale toxizitten entsprechend pet - positiven volumen ( btv ) in der untergruppe mit dosiserhhung auf btv ( n = 12 ) : niedrigere volumen gehen mit einem erhhten toxizittsrisiko einher . 
relapse - free survival curves ( including both local and distant ) : the two groups with ( dotted line ) and without ( continuous line ) dose escalation on pet - positive volumes are compared ( boost vs no boost )  . 
rezidivfreies berleben ( einschlielich lokaler wie auch fernmetastasen ) in den gruppen mit ( gestrichelte linie ) und ohne ( durchgezogene linie ) dosiseskalation auf pet - positive volumen ( boost vs kein boost )  . 
overall survival curves : the two groups with ( dotted line ) and without ( continuous line ) dose escalation on pet - positive volumes are compared ( boost vs no boost )  . 
four patients were in pd at the first evaluation : 1 was in local pr with pd in the contralateral lung , 2 were in sd and abdominal pd , and 1 was in local and distant progression . 
 when comparing the two groups , the largely improved overall survival was not statistically significant ( 1 - year survival : 41% vs 59% , log - rank p = 0.19 , figure 2 )  . 
local relapse - free survival curves : the two groups with ( dotted line ) and without ( continuous line ) dose escalation on pet - positive volumes are compared ( boost vs no boost )  . 
cancer - specific survival curves : the two groups with ( dotted line ) and without ( continuous line ) dose escalation on pet - positive volumes are compared ( boost vs no boost )  . 
krankheitsspezifisches berleben in den gruppen mit ( gestrichelte linie ) und ohne ( durchgezogene linie ) dosiseskalation auf pet - positive volumen ( boost vs kein boost )  . heart fodor a , et al . 
the median time to local relapse for no - sib and sib groups was 8 and 17 months , respectively ; of note , the 1 - year local relapse - free rate was 16% vs 81% for the two groups ( log - rank p = 0.003 , figure 4 )  . 
a slightly larger difference , compared to overall survival , was found when considering cancerspecific survival ( 1 - year survival : 46% vs 71% , p = 0.12 , figure 5 )  . 
 no other variables were found to be correlated with overall and / or relapse - free survival . discussion several works failed to find an impact of radiotherapy on survival of unresectable mpm patients compared to best supportive care [ 17 , 24 ]  . 
a potential role of radiotherapy in mpm emerged from a number of studies in an adjuvant to surgery context [ 8 , 25 , 27 , 28 , 38 ] , while the feasibility of dose escalation with imrt for unresectable , recurrent mpm has only recently been suggested [ 26 ] ; on the other hand , several experiences have shown the role of the low dose received by the contralateral lung on fatal pneumonitis [ 2 , 25 , 31 , 40 ] , quite consistent with reported rates of fatal pneumonitis during whole lung irradiation in tbi [ 10 ]  . 
when lung doses are low , for pleural localization of disease or in tbi , the toxicity is acceptable [ 20 , 23 ]  . in our tomotherapy experience , we have been able to reduce the dose to the contralateral lung to safe levels , with average values of mld below 8 gy in both groups of patients ; as a result , no fatal radiotherapy - induced pneumonitis have been found to date . because of the presence of the ipsilateral lung , one could expect a higher rate of actinic pneumonitis compared to the most studied epp series . 
however , as in other published series , the toxicity was acceptable [ 18 , 25 ] , although increased in the sib group where 3patients experienced grade 3 pneumonitis . 
a memorial sloan kettering cancer center ( mskcc ) study has already shown that external beam radiotherapy doses 40 gy were associated with an improvement in survival with 1 - year local control of 42% [ 18 ]  . after epp the results demonstrated that a dose of 54 gy is necessary for microscopic and residual disease . 
in a mskcc phaseii trial , the investigators delivered 54 gy in 30 fractions to the ipsilateral hemithorax postoperatively and contralateral kidney contralateral lung ipsilateral kidney ipsilateral lung figure 6 . 
the improved overall survival with dose escalation could not be demonstrated , probably due to the limited number of patients . conclusion despite the study limitations , a statistically significant improvement in local control was obtained in consecutive , nonselected patients , when the dose was escalated on the pet - positive volumes in a sib approach with tomotherapy . 
 [ 3 ] demonstrated the influence of radiotherapy technique and dose in limiting in - field local failures , which makes distant relapse the most significant challenge ; this is , after decades of struggle , a remarkable result . 
 with our scheme using helical tomotherapy , in a consecutive , nonselected series of pd patients , one cr and several pr were obtained in the no - sib group ; all subsequently experienced pd , but the cr patient lived for 50.5months after the radiotherapy , with grade 1 dyspnea until bilateral progression . 
 similarly , in the dose - escalated sib group , only one cr was obtained in a non - operated , chemonaive patient , but more pr acknowledgment we thank deli aniko maria for her support in the revision and translation into german . original article radiochemotherapy with temozolomide for patients with glioblastoma prognostic factors and long - term outcome of unselected patients from a single institution johanna gerstein1 , kea franz2 , joachim p . 
steinbach3 , volkert seifert2 , claus rdel1 , christian weiss1 background : the objective of this retrospective analysis was to assess long - term outcome and prognostic factors of unselected patients treated for glioblastoma ( gb ) at a single center with surgery , standard radiotherapy ( rt ) , and concomitant temozolomide ( tmz )  . 
 patients and methods : between april 1999 and september 2009 , 181 patients with gb were treated with rt ( 60 gy in 30 fractions ) and concomitant tmz ( 75 mg / m / day throughout rt )  . 
in multivariate cox proportional hazards regression models , extent of resection ( p < 0.0001 ) , karnofskys performance score ( p < 0.0001 ) and adjuvant tmz ( p = 0.001 ) were significant independent prognostic factors for os . 
 key words : glioblastoma multiforme radiochemotherapy temozolomide strahlenther onkol 2011 ; 187 : 7228 doi 10.1007 / s00066 - 011 - 2230 - x radiochemotherapie mit temozolomid bei unselektionierten patienten mit glioblastom : prognostische faktoren und berleben im rahmen einer monoinstitutionellen serie hintergrund : ziel dieser retrospektiven analyse einer monoinstitutionellen serie war es , langzeitergebnisse sowie prognosefaktoren nach operation und simultaner radiochemotherapie ( rct ) mit temozolomid ( tmz ) zu untersuchen . 
 patienten und methoden : von 04 / 1999 bis 9 / 2009 , wurden 181 gb - patienten mit einer kombinierten rct ( 60 gy in 30 fraktionen ) mit tmz 75 mg / m / tag whrend der rt behandelt . 
 ergebnisse : das mediane gesamtberleben ( g ) und das progressionsfreie berleben ( pf ) lag bei 15 , 0 ( 95 % - ci : 13 , 116 , 8 monate ) bzw . 
in der multivariaten analyse waren resektionsstatus ( p < 0 , 0001 ) , karnofsky - index ( p < 0 , 0001 ) und adjuvante tmz - therapie ( p = 0 , 001 ) unabhngige prognostische faktoren . 
bei weiteren 35 patienten wurde die konkomitante chemotherapie unterbrochen . 1department of radiotherapy and oncology , johann wolfgang goethe university , frankfurt / main , germany , 2department of neurosurgery , johann wolfgang goethe university , frankfurt / main , germany , 3senckenberg institute of neurooncology , johann wolfgang goethe university , frankfurt / main , germany . 
 schlsselwrter : glioblastoma multiforme radiochemotherapie temozolomid introduction despite recent advances in the treatment of glioblastoma ( gb ) , median survival time is generally only 912months , with less than 15% of patients alive 2years post - diagnosis [ 12 , 20 ]  . 
until 2005 , standard therapy consisted of surgical resection and postoperative radiotherapy ( rt ) [ 23 ] , whereas the addition of various chemotherapeutics only resulted in marginal benefits [ 4 , 15 , 17 ]  . 
this changed with the publication of the randomized eortc 26981 / 22981 - ncicce3 trial in 2005 , demonstrating that the addition of temozolomide ( tmz ) to standard rt and further six cycles of adjuvant tmz significantly and clinically meaningful improved median and 2 - year survival when compared to postoperative rt alone [ 19 ]  . 
it remains uncertain , however , whether concomitant temozolomide , adjuvant temozolomide , or both are important for this improvement . and oncology of frankfurt university and were now analyzed , retrospectively . 
biopsy only had been performed in 53 patients ( 29.3% ) , 77 patients ( 42.5% ) had undergone partial / subtotal resection , and 51 patients ( 28.2% ) macroscopically complete resection , as determined from the surgical report and postoperative mri . 
 as the outcomes of randomized controlled trials need to be confirmed in routine clinical practice , taking into account differences in treatment and tumor characteristics between the trial population and unselected patients , the objective of this present retrospective analysis was to assess compliance , toxicity , and longterm outcome of 181patients treated for gb at a high - volume single center with surgery , standard rt , and concomitant tmz . 
furthermore , we analyzed in uniand multivariate analysis whether after introduction of tmz radiochemotherapy ( rct ) the well - established prognostic factors , such as age , extent of resection , karnofsky performance score , and the rpa ( recursive partitioning analysis ) score , retained their prognostic value in this large single center population . 
until the publication of the eortc - ncic trial in 2005 , adjuvant chemotherapy was not routinely applied after completion of rct in favor of salvage treatment ( surgery if feasible , chemotherapy or re - rt ) in patients with evidence of recurrent or progressive disease . 
from 2005 onwards , routine adjuvant tmz in addition to concomitant tmz was administered according to the published study protocol 4weeks after completion of rct for up to 6cycles ( 150200mg / m day15 , every 28days )  . 
prophylactic antibiotics against pneumocystis carinii were not routinely applied . posttherapeutic clinical , laboratory , and slice imaging ( ct / mri ) monitoring was started 34 weeks after end of rct , and at 3 - month intervals thereafter , or earlier if indicated . 
overall and progression - free survival curves were estimated actuarially using the kaplanmeier method ; differences in relation of subgroups were evaluated by the log - rank test for statistical significance . 
multivariate analyse prognostischer faktoren in bezug auf das gesamtberleben ( os ) und progressionsfreie berleben ( pfs ) bei patienten nach kombinierter radiochemotherapie mit temozolomid . death risk ratio ( 95% ci ) p - value progression risk ratio ( 95% ci ) p - value gerstein j , et al . 
in multivariate cox proportional hazards regression model , extent of resection ( p < 0.0001 ) , karnofskys performance score ( p < 0.0001 ) , and adjuvant tmz ( p = 0.001 ) were significant independent prognostic factors for os . 
at log - rank test evaluation , no significant correlation was found between pfs and age ( p = 0.22 ) , gender ( p = 0.81 ) , and kps ( p = 0.55 ) , whereas extent of resection ( p < 0.0001 ) , rpa score ( p = 0.001 ) , and adjuvant tmz ( p = 0.025 ) were statistically significant prognostic factors ( table 2 )  . 
at multivariate analysis , only extent of resection ( p < 0.0001 ) and adjuvant tmz ( p = 0.032 ) retained significance ( table 3 )  . treatment compliance and toxicity rt with concomitant tmz was well tolerated in the majority of patients and could be completed as scheduled in 146 patients ( 80.7% ) ( table 4 )  . 
another 35 patients ( 19.3% ) transiently interrupted concomitant chemotherapy . discussion the current standard of care for gb is surgical resection followed by rct with concomitant and adjuvant tmz according to the randomized eortc - ncic trial published in2005 [ 19 ]  . 
 it is well established that outcome results after treatment of gb are strongly dependent upon factors such as age , performance status , and extent of surgical resection [ 1 , 3 , 57 , 11 , 12 , 21 ]  . 
 our analysis of prognostic subgroups confirmed that extent of resection , kps , and adjuvant tmz were associated with a significant overall survival benefit , both in the uniand multivariate analysis . 
although some studies have failed to demonstrate a survival benefit with more extensive surgical resection versus biopsy alone [ 9 ] , most recent reports from single centers or randomized trials support that more extensive resection does significantly lengthen os [ 2 , 6 , 10 , 16 ]  . 
given that only 67 of 181patients in our series ( 37% ) had received standard adjuvant chemotherapy with tmz , a policy that was only introduced after the publication of the eortc / ncic trial in 2005 [ 19 ] , any statistical analysis with respect to the value of adjuvant tmz after concomitant rct needs to be interpreted with caution , as noncontrolled confounding factors may heavily influence results . 
however , the fact that adjuvant tmz chemotherapy was associated with improved overall and progression - free survival both in uniand multivariate analyses may suggest that administrating tmz after rct is superior to our former policy of vigilant follow - up and salvage treatment in case of tumor progression . 
at least for anaplastic gliomas , the ongoing catnon study with its 2 2 design comparing rt with or without concomitant tmz each with no or 12cycles adjuvant tmz will clarify the contribution of the concomitant versus the adjuvant part of tmz chemotherapy . the current study has several limitations , including the limitations of any retrospective data collection and the heterogeneous policy with respect to adjuvant tmz . 
nonetheless , it is the conclusion from our large single center experience and results from other mono - institutional series [ 6 , 8 , 22 , 24 ] ( table 5 ) that a combination of maximum surgery , concomitant rct with tmz , and adjuvant tmz for gb patients is associated with moderate toxicity and minimal hospitalization and yields survival results in daily clinical practice against which newer strategies , such as the integration of antiangiogenic drugs , kinase inhibitors , immunotherapies , or integrin antagonists , should be compared . acknowledgment the senckenberg institute of neurooncology is supported by the senckenberg foundation and the hertie foundation . 
js is a hertie professor for neurooncology . case study curative treatment for central nervous system medulloepithelioma despite residual disease after resection report of two cases treated according to the gpho protocol hit 2000 and review of the literature klaus mller1 , isabella zwiener9 , helmut welker2 , eberhard maa3 , rudolf bongartz4 , frank berthold5 , torsten pietsch7 , monika warmuth - metz8 , andr von bueren6 , stefan rutkowski6 medulloepithelioma of the central nervous system ( cns ) is an uncommon primitive neuroectodermal tumor ( pnet ) usually occurring in early childhood . 
 in this article , the authors report on 2cases of cns medulloepithelioma in which long - term survival ( more than 6years ) could be achieved despite evidence of , or suspected postoperative residual disease with an otherwise dismal prognosis . the patients were treated according to different strata of the protocol for primitive neuroectodermal tumors ( pnet ) of the germanaustrian multicenter trial of the german society for pediatric oncology and hematology ( gpoh ) for childhood brain tumors ( hit 2000 )  . 
treatment included postoperative hyperfractionated radiotherapy of the craniospinal axis followed by a boost to the tumor site in combination with chemotherapy . a review of the 2reported and 37 previously published cases confirmed gtr and older age as positive prognostic factors . 
 key words : medulloepithelioma long - term survival hyperfractionated radiotherapy residual disease hit 2000 chemotherapy strahlenther onkol 2011 ; 187 : 75762 doi 10.1007 / s00066 - 011 - 2256 - 0 kurative behandlung von inkomplett resezierten medulloepitheliomen des zns . 
bericht ber zwei flle , die nach dem gpho - protokoll hit 2000 behandelt wurden , und literaturdurchsicht das medulloepitheliom des zentralen nervensystems ist ein seltener , primitiver , neuroektodermaler tumor , der gewhnlich in der frhen kindheit auftritt . 
 dennoch ging man bisher davon aus , dass eine totalresektion fr einen kurativen therapieansatz unabdingbar sei . wir berichten nun ber zwei flle von zns - medulloepitheliomen , bei denen ein langzeitberleben ( lnger als 6 jahre ) erreicht werden konnte , obwohl mit sicherheit beziehungsweise hchstwahrscheinlich postoperativ resttumorgewebe in situ verblieben war . 
 die patienten wurden entsprechend verschiedenen zweigen des protokolls fr primitive , neuroektodermale tumore einer deutsch - sterreichischen , multizentrischen studie fr kindliche hirntumore ( hit 2000 ) der deutschen gesellschaft fr 1university of leipzig , department of radiotherapy and radiooncologyleipzig , germany 2katharinenhospital , department of radiotherapy and radiooncology , stuttgart , germany , 3klinikum stuttgart olgahospital , pediatrics 5 ( oncology , hematology , immunology ) , stuttgart , germany , 4university of cologne , department of radiotherapy and radiooncology , cologne , germany , 5university of cologne , department of pediatric oncology , cologne , germany , 6university medical center hamburg - eppendorf , department of pediatric hematology and oncology , hamburg , germany , 7university of bonn medical center , department of neuropathology , bonn , germany , 8university of wuerzburg , department of neuroradiology , wuerzburg , germany , 9university medical center of the johannes gutenberg university mainz , institute for medical biostatistics , epidemiology and informatics , mainz , germany . received : january 7 , 2011 ; accepted : july 21 , 2011 published online : october 28 , 2011 strahlenther onkol 2011 no . 
 eine auswertung der beiden vorgestellten und 37 weiterer , bereits publizierter flle besttigte eine totalresektion ( figure 5 ) und ein hheres alter ( figure 3 ) als positive prognosefaktoren . 
 schlsselwrter : medulloepitheliom langzeitberleben hyperfraktionierte bestrahlung inkomplette resektion hit 2000 chemotherapie introduction medulloepithelioma is a rare primitive neuroectodermal tumor of the central nervous system characterized by a highly malignant behavior [ 17 ]  . 
further histopathologic characteristics are ( 1 ) papillary , tubular , or trabecular arrangements of the cells with an external and internal limiting membrane that mimics the structure of the primitive neural tube and ( 2 ) have a tendency to display multiple lines of differentiation , including neuronal , glial , and mesenchymal elements [ 1 , 4 , 7 , 10 , 12 , 14 , 29 ]  . medulloepithelioma is extremely rare and usually presents in childhood or adolescence . 
 in contrast to the benign clinical course of intraorbital medulloepithelioma that is often cured by simple enucleation [ 11 ] , medulloepithelioma of the central nervous system ( cns ) is known for its poor prognosis , especially when incompletely resected . 
 here , we report on 2 cases of cns medulloepithelioma with long - term survival although residual disease after primary resection was evident in 1patient and highly suspected in the other patient . medulloblastoma as both tumors were located in the posterior fossa and biological behavior was presumed to be similar to medulloblastoma . 
both patients had neurological examinations and contrast - enhanced magnetic resonance imaging ( mri ) before and after treatment to assess extent of disease and response to therapy , respectively , and to exclude recurrent disease . 
both clinical cases were documented at the hit 2000 study center in wuerzburg , and the reference center for radiooncology in tbingen who gave a detailed treatment recommendation before starting therapy . 
according to the local radiologist , postoperative contrast - enhanced treatment concepts both patients were treated according to the guidelines of the gpho multicenter trial hit 2000 for children and adolescents with medulloblastoma , supratentorial pnet , or ependymoma who grade ii and iii . 
the aim of the hit 2000 study , which started to accrue patients in 2001 , was to improve survival by stratification of treatment based on histology , age , and clinical staging ( nonmetastatic / metastatic disease ; and absence or presence of residual tumor ) ( figure 1 ) [ 15 ]  . 
for patients , who did not meet the eligibility criteria , as the 2 cases of infratentorial medulloepithelioma reported here , the study protocol was used as a treatment guideline . 
three weeks following resection , the patient received hyperfractionated irradiation of the craniospinal axis with 1 gy twice a day to a total dose of 36 gy followed by a boost to the posterior fossa to 60 gy total dose . 
seven weeks after completion of radiotherapy , adjuvant maintenance chemotherapy was administered and consisted of 8 cycles containing cisplatin ( 70 mg / m2 ) , lomustine ( 75 mg / m2 ) , and vincristine ( 1.5 mg / m2 )  . 
 case 2 an 8 - year - old girl presented with a 10 - day history of increased intracranial pressure ( headache , nausea , vomiting ) , cerebellar ataxia , and right abducens paresis . 
at restaging after the first cycle , progressive disease was detected on mri with a nodular leptomeningeal disease within the posterior fossa and an extensive local relapse extending from the base of the fourth ventricle to the foramen magnum and to the right cerebellar peduncle . 
chemotherapy was , therefore , discontinued and hyperfractionated irradiation of the craniospinal axis was started with 1 gy twice a day to a total dose of 40 gy , followed by a boost to the posterior fossa to 60 gy total dose . 
 subsequently , the patient obtained four cycles of maintenance chemotherapy , including cisplatin ( 70 mg / m2 ) , lomustine ( 75 mg / m2 ) , and vincristine ( 1.5 mg / m2 )  . 
the girl was reported to be well and attended secondary school . literature search and statistical analysis of published cases in addition to the 2cases reported here , we aimed to evaluate prognostic factors of past series and the previous doctrine on the dismal prognosis of cns medulloepithelioma . 
the published data on 37 cases [ 1 , 2 , 46 , 8 , 10 , 12 , 14 , 16 , 1822 , 2830 , 32 , 3436 ] were reviewed by using univariable analysis with respect to age ( n = 37 ) , tumor location ( supra - / infratentorial ) ( n = 35 ) as well as extent and time of resection ( n = 27 ) using the kaplanmeier method and log - rank test . 
patients with supratentorial tumor location had a 5 - year os of 30 10% , as compared with patients showing an infratentorial tumor location ( 5 - year os of 23 12% ) ( p = 0.418 ) ( figure 4 )  . 
gesamtberleben von 39 zns - medulloepitheliom - patienten ( 37 wurden zwischen 1957 und 2010 in der literatur und 2 hier beschrieben ) ( 3und 5 - jahres - gesamtberleben : 30% 7% )  . 
treatments of both patients were stratified according to the risk profiles of the hit 2000 protocol and included radiotherapy of the craniospinal axis with a more intensive approach by using hyperfractionation , including a local dose escalation to improve local tumor control in both cases . 
adjuvant maintenance chemotherapy was applied in the child with localized disease and neoadjuvant , more intensive chemotherapy was used in the child with the inconclusive csf analysis followed by radiotherapy and maintenance chemotherapy . 
in our case , intensive radiotherapy using a hyperfractionated schedule with dose escalation used for metastatic medulloblastoma in the hit 2000 study was highly efficient , even after failure of chemotherapy . 
patients with supratentorial tumor site had a 5 - year os of 30 10% , whereas patients with infratentorial tumor location had a 5 - year os of 23 12% ( p = 0.418 , figure 4 )  . however , age at diagnosis might influence prognosis of cns medulloepithelioma . 
the use of postoperative craniospinal irradiation with a more intensive schedule combined with maintenance chemotherapy may offer a curative approach for medulloepithelioma even in case of subtotal resection or positive csf with an otherwise dismal prognosis . 
the remaining patients ( n = 234 ) consisted of patients with either stable or increasing psa during srt ( as treated from 2002 onwards ) , or probably with unknown psa status during srt ( as treated before 2002 )  . 
 patients with decreasing psa during srt have most likely a higher chance of improved psa outcome ( e.g. , undetectable psa after srt , long - term psa control ) as opposed to patients with unknown , stable , or even increasing psa values during srt due to several reasons , including decreased risk of disease outside the prostate bed and higher radiation responsiveness . 
therefore , this selection bias favors the 70.2 gy group at least in part irrespective of the applied total dose . we recommend to include the information psa decrease during srt yes vs . 
they point out correctly that in our retrospective analysis , the psa response during srt was unknown for " early " patients and state that the selection favored the high - dose cohort . 
 a preliminary analysis of a larger cohort with psa monitored during srt ( but still a short follow - up ) confirmed the positive effect for the high - dose group . 
 strahlentherapie und onkologie original article impact of radiotherapy on pain relief and recalcification in plasma cell neoplasms long - term experience mario balducci1 , silvia chiesa1 , stefania manfrida1 , elena rossi2 , tommaso za2 , vincenzo frascino1 , berardino de bari3 , stefan hohaus2 , francesco cellini4 , giovanna mantini1 , giuseppe roberto dagostino1 , maria antonietta gambacorta1 , antonello leone5 , vincenzo valentini1 , valerio de stefano2 purpose : to evaluate the impact of radiotherapy on pain relief and on recalcification in patients with osteolytic lesions due to plasma cell neoplasm . patients and methods : pain relief was evaluated according to a 010 verbal numerical rating scale ( nrs ) and recalcification was measured using radiological imaging . results : from 19962007 , 52 patients were treated ( table 1 )  . 
pain relief was achieved in 41 of 45 patients ( 91% ) : complete relief was obtained in 21 ( 51.2% ) and partial relief in 20 patients ( 48.8% ) ; patients with severe pain experienced resolution and none presented an increase of padrugs reduction / suspension was achieved in 7 of the 21 patients with complete response . 
of 42 patients evaluable for recalcification ( table 3 ) , 21 ( 50% ) presented a radiological response , which was identified as complete in 16 ( 38% )  . conclusion : our data confirm the effectiveness of radiotherapy for pain relief , including a reduction in drug intake , and on recalcification , thus , supporting its use in a multidisciplinary approach . key words : plasma cell neoplasm radiotherapy pain relief recalcification strahlenther onkol 2011 ; 187 : 1149 doi 10.1007 / s00066 - 010 - 2155 - 9 wirkung der strahlentherapie auf schmerzlinderung und rekalzifizierung beim multiplen myelom und plasmozytom : langzeit - erfahrung ziel : beurteilung der wirkung der strahlentherapie auf schmerzlinderung und rekalzifizierung bei patienten mit osteolysen auf grund von malignen plasmazellerkrankungen . patienten und methodik : die schmerzlinderung wurde anhand einer 010 numerischen verbalskala ( nvs ) beurteilt , whrend die rekalzifizierungsrate mittels radiologischer bildgebender verfahren gemessen wurde . ergebnisse : von 1996 bis 2007 wurden 52 patienten behandelt ( tabelle 1 )  . 
eine schmerzlinderung wurde bei 41 der 45 ( 91% ) patienten erreicht : eine vollstndige schmerzkontrolle bei 21 ( 51 , 2% ) und eine teilweise linderung bei 20 patienten ( 48 , 8% ) ; alle patienten mit ausgeprgter schmerzsymptomatik erfuhren eine reduktion der schmerzen , und bei keinem patienten nahmen die schmerzen zu . 
eine rekalzifizierung wurde bei 42 patienten radiologisch beurteilt ( tabelle 3 ) : 21 ( 50% ) zeigten eine verbesserung , eine komplette rekalzifizierung wurde bei 16 ( 38% ) patienten beobachtet . 1radiotherapy department , university hospital gemelli , rome , italy , 2hematology department , university hospital gemelli , rome , italy , 3radiotherapy oncology department , university hospital lyon sud , pierre benite , france , 4radiotherapy department , university hospital campus biomedico , rome , italy , 5radiology department , university hospital gemelli , rome , italy . received : april 9 , 2010 ; accepted : september 16 , 2010 published online : january 24 , 2011 strahlenther onkol 2011 no . 
pain relief and recalcification by rt in plasma cell neoplasms schlussfolgerung : unsere daten besttigen die wirksamkeit der strahlentherapie , die in einer multidisziplinren strategie bei malignen plasmazellerkrankungen eingesetzt werden kann , um eine schmerzlinderung mit reduzierung der schmerzmittelmedikation und eine rekalzifizierung zu erreichen . schlsselwrter : multiples myelom , plasmozytom strahlentherapie scherzlinderung rekalzifizierung introduction plasma cell neoplasms are rare tumors and include multiple myeloma and solitary plasmacytoma . 
multiple myeloma is 16 times more frequent than solitary plasmacytoma [ 13 ] , while less than 10% of all plasma cell neoplasms are reported to be solitary plasmacytoma [ 16 ]  . although these are rare tumors , they are the major causes of bone involvement [ 32 ]  . 
osteolysis is related to increased osteoclast activity with loss of bone structure ; it also leads to an increased risk of pathologic fractures and severe bone pain with a negative impact on quality of life [ 2 , 24 ]  . 
 radiotherapy is the treatment of choice in solitary plasmacytoma , and it plays an important role in the multidisciplinary approach of multiple myeloma to reduce pain and improve recalcification [ 31 , 32 ]  . 
our retrospective study analyzed the role of radiotherapy in the treatment of plasma cell neoplasms to define the impact of radiation on pain relief , recalcification , and local control . patients and methods from november 1996 to december 2007 , 52 patients with osteolytic lesions and diagnosis of plasma cell neoplasms were observed . 
out of 52 patients , 10 ( 19% ) were diagnosed with solitary plasmacytoma , and 42 ( 81% ) patients were diagnosed with symptomatic multiple myeloma , according to the international myeloma working groups criteria [ 12 ]  . histological data and laboratory tests , including electrophoreses of serum and urine , as well as immunofixation , and immunoglobulin serum levels , were obtained for all patients . 
clinical target volume ( ctv ) generally included the osteolytic lesion with extension to the adjacent soft tissues , if present , plus a 23 cm margin spinal lesions , the ctv was represented by involved vertebra plus the upper and lower vertebrae . 
the median total dose was 38 gy ( range , 1650 gy ) delivered in a median daily fraction of 2 gy ( range , 24 gy / day ) , tailored to performance status , degree of pain , site of bone lesion , and palliation guidelines [ 19 ]  . 
 in all treatment plans , 95% of the prescribed dose covered at least 95% of the ptv [ 17 , 18 ]  . bisphosphonates ( zoledronic acid fl i.v. , 4 mg ) were administered monthly for a median duration of 4 months . 
in addition , orthopanoramic radiographs were obtained before , during , and after radiotherapy [ 34 ]  . response criteria and statistical analysis pain was assessed according to a verbal numerical rating pain scale ( nrs ) [ 9 ]  . 
 ( % ) characteristics gender female male age at the diagnosis mean ( yrs ) range ( yrs ) staging at diagnosis solitary plasmacytoma multiple myeloma treatment timing radiotherapy ( rt ) exclusive radiotherapy rt prior to chemotherapy rt after chemotherapy surgery no yes irradiated sites spinal cord pelvic bone extremites skull ribs 19 ( 37 ) 33 ( 63 ) 2271 10 ( 19 ) 42 ( 81 ) 8 ( 15 ) 13 ( 25 ) 31 ( 60 ) 29 ( 56 ) 23 ( 44 ) 35 ( 68 ) 6 ( 12 ) 5 ( 9 ) 4 ( 7 ) 2 ( 4 ) strahlenther onkol 2011 no . 
pain relief and recalcification by rt in plasma cell neoplasms the response rate was defined according to the international consensus on palliative radiotherapy criteria [ 8 ] : complete response was defined as a pain score of zero at the treated site without any concomitant increase in analgesic intake ( stable or reducing analgesics ) ; partial response was defined as : ( i ) pain reduction of 2 or more at the treated site on the 010 scale without analgesic increase or ( ii ) analgesic reduction of 25% or more from baseline without an increase in pain ; pain progression was defined as an increase in the pain score of 2 or more points above baseline at the treated site with stable analgesic use or an increase of 25% or more compared with baseline with the pain score stable or 1 point above baseline . osteolytic lesions were evaluated by x - ray imaging and ct scan in 42 patients and by x - ray or ct in 10 patients . 
 recalcification was evaluated by x - ray imaging and ct scan according to the following criteria : ( 1 ) complete response : complete recalcification / reossification of primary osteolysis ; ( 2 ) partial response : evidence of marginal sclerosis around the lesion without complete reossification ; ( 3 ) stable disease : no change of radiological signs was observed ; ( 4 ) progressive disease : increase in lesion size . the median follow - up was 57 months ( range , 21210 months )  . 
grade 12 toxicity was observed in 23 patients ( 44% ) : hematological toxicity in 11 ( 48% ) , gastroenteric toxicity in 6 ( 26% ) , pharyngeal toxicity in 2 ( 9% ) , and cutaneous toxicity in 4 ( 17% ) patients . pain relief before radiotherapy , 45 patients ( 86.5% ) reported painful bone lesions ( 9 solitary plasmacytoma ) and were evaluable ( table 2 ) ; pain was mild in 13 patients ( 29% ) , moderate in 27 ( 60% ) , and severe in 5 patients ( 11% )  . two months after radiotherapy , no patient reported an increase of pa pain relief ( complete and partial ) was obtained in 41 / 45 patients ( 91% ) , including all patients with severe pain at baseline . 
the mean and median time to achieve recalcification was 5.9 and 6 months , respectively ( range , 314 )  . objective radiological response ( complete + partial ) was observed in 21 of the 42 ( 50% ) patients ( table 3 )  . 
in solitary plasmacytoma , a complete response was obtained in 6 patients ( 60% ) and stable disease in 4 ; progressive disease ( 7.1% ) was observed only in multiple myeloma and was always related to uncontrolled systemic disease . twelve of the 42 ( 28.5% ) patients received biphosphonates . 
related to grade of response they were : 4 of 16 patients with complete response , 4 of 5 with partial response , 3 of 18 of stable disease , and 1 of 3 with disease progression . 
schmerzlinderung. factor pain intensity at baseline mild moderate severe pain relief after radiotherapy complete mild baseline pain moderate baseline pain severe baseline pain partial mild baseline pain moderate baseline pain severe baseline pain no change mild baseline pain moderate baseline pain table 3 . 
disease progression was observed in 6 patients : 1 with skull , 4 with spine , and 1 with pelvic bone lesions ; time to progression was 7 , 18 , 21 , 2 , 46 , and 16 months , respectively . median time to local relapse had not been achieved yet . 
 with a median follow - up of 61 months ( range , 21210 months ) , the 5 - year local control was 81% in all patients ( figure 1 ) , being 90% and 76% , respectively ( p = 0.57 ) , in solitary plasmacytoma and multiple myeloma ( figure 2 ) figure 1 . 
lokale kontrolle bei 52 patienten . plasma cell neoplasms are often causes of bone involvement [ 10 , 32 ] and are represented by solitary plasmacytoma and multiple myeloma , symptomatic at diagnosis in 70% of cases [ 4 ]  . 
pain is a frequent presenting symptom in myeloma patients caused by bone localization and radiological lesions are often present [ 27 ]  . the pathophysiology of bone involvement remains complex and is represented by production of enzymes that stimulate osteoclasts to destroy the bone [ 28 ]  . 
in fact , initially radiotherapy induces the death of radiosensitive inflammatory cells , largely present in the bone metastases microenvironment , and inhibits the release of chemical pain mediators , interrupting the inflammatory cytokine cascade [ 32 ] ; later it leads apoptotic death of the tumor cells with tumor shrinkage and decreasing pressure in bone marrow . 
 thus , an analgesic effect is obtained during or immediately after radiotherapy , while recalcification is achieved after a few months ; external beam irradiation produces partial pain relief in 8090% of patients , complete pain relief in 50% , and reconstruction of the normal bone structure in 6585% of cases [ 28 ]  . data from the treatment of solid tumor bone metastases compared different schedules on pain relief and remineralization [ 3 , 7 , 15 , 19 ]  . 
no particular radiotherapy schedule was found to be superior to others with respect to pain relief . a reanalysis of dutch bone metastasis study calculated responses to initial treatment and retreatment , scoring pain relief using a numerical scale and taking into account changes in the administration of opioids . 
generally radiotherapy pain relief was obtained by radiotherapy in 75100% of cases [ 1 , 23 , 26 , 31 ]  . a retrospective review , published in 1980 by mill et al . 
 [ 23 ] , reported good pain relief in 116 patients treated with a radiation dose of 1520 gy ; however , the authors did not analyze the impact of response pain rate on drugs reduction or suspension . 
 [ 25 ] observed 42 patients with multiple myeloma and report the effect of radiotherapy on relief of pain ( measuring patient perception and the use of analgesic drugs ) , and recalcification ( comparing of radiographs before and after radiation )  . 
a retrospective multicenter study [ 1 ] reported the results of a large cohort of patients with plasma cell myeloma from 19 european and north american centers and analyzed only radiation doseresponse effects and prognostic factors for survival , progression to myeloma , and patterns of local failure without pain relief and remineralization analysis . few data are available for solitary plasmacytoma because it is rare . 
a short - term schedule was suggested for patients with a poor prognosis and total dose of 4050 gy in patients with a life expectancy > 1 year in order to achieve the best pain relief and recalcification . our data confirm the efficacy of irradiation : in fact , pain relief , estimated by the verbal numerical rating pain scale ( nrs ) [ 9 ] , was observed in 91% of cases and when the response with drugs was analyzed , a reduction or suspension of analgesic drugs in 33% of patients with complete response was observed . 
the remaining patients , who had reported moderate and severe pain score level at baseline , presented a pain score of zero after radiotherapy , but still needed analgesics . recalcification was observed in 50% of patients and in no case was surgery performed after radiotherapy . 
 there were 3 cases of local relapse ( 3 / 42 patients , 7.1% ) , which were concomitant with systemic relapse of the disease . unfortunately in our analysis , only 10 of 52 patients were affected by sp . 
nevertheless , even in this small subgroup , we observed an important reduction of pain score in all evaluable patients , with complete response in 66% of cases and reduction of analgesics in 5 patients . 
these data confirm the evidence reported in the literature concerning the role of radiotherapy in improving the outcomes of this disease . conclusion radiotherapy in plasma cell neoplasms can result in pain relief with the possibility of reducing analgesic drugs . 
these data support the early use of radiotherapy as part of a multidisciplinary approach to treat plasma cell neoplasm . strahlentherapie und onkologie original article preoperative oxaliplatin , capecitabine , and external beam radiotherapy in patients with newly diagnosed , primary operable , ct3nxm0 , low rectal cancer a phase ii study * dietmar fner1 , 2 , alexander f . 
this phase ii study investigated the efficacy and safety of preoperative capecitabine and oxaliplatin in combination with radiotherapy . patients and methods : patients with larc of the mid and lower rectum , t3nxm0 staged by mri received radiotherapy ( total dose 45 gy ) in combination with oral capecitabine ( 825 mg / m2 twice a day on radiotherapy days ; weeks 14 ) and oxaliplatin 50 mg / m2 intravenously ( days 1 , 8 , 15 , and 22 )  . 
efficacy was evaluated as rate of tumor down - categorization at the t level . results : a total of 59 patients were enrolled ( 19 women , 40 men ; median age of 61 years ) and all were evaluable for efficacy and toxicity . 
veit / glan , austria , 8department of therapeutic radiotherapy and oncology , medical university of graz , austria , 9department of radiotherapy , private medical paracelsus university salzburg , salzburg , austria , 10department of hematology and oncology , leoben - eisenerz hospital , leoben , austria , 11department of internal medicine i , innsbruck medical university , innsbruck , austria , 12department of radiotherapy , innsbruck medical university , innsbruck , austria , 13department of pathology , feldkirch hospital , feldkirch , austria , 14department of surgery , medical university of vienna , vienna , austria , 15department of internal medicine iv , wels - grieskirchen hospital , wels , austria . received : june 7 , 2010 ; accepted : november 11 , 2010 published online : january 21 , 2011 strahlenther onkol 2011 no . 
capox and external beam radiation in larc properative kombinierte radiochemotherapie mit oxaliplatin und capecitabin beim lokal fortgeschrittenen , primr operablen , ct3nxm0 , tiefen rektumkarzinom eine phase - ii - studie ziel : eine properative radiochemotherapie verbessert bei patienten mit einem tief sitzenden rektumkarzinom ( larc ) die lokale tumorkontrolle und ein so genanntes down - staging dient als berlebenssurrogatparameter . 
diese multizentrische phase - ii - studie soll die wirksamkeit und toxizitt einer neoadjuvanten durch capecitabin und oxaliplatin intensivierten radiochemotherapie prfen . patienten und methodik : patienten mit einem larc , das mittels mri als ct3nxm0 klassifizierten wurde , erhielten eine radiotherapie ( 45 gy in konventioneller fraktionierung ) mit konkomitanter gabe von capecitabin ( oral 2 x tglich 825 mg an den bestrahlungstagen , woche 14 ) und oxaliplatin intravens 50mg / m2 ( an den tagen 1 , 8 , 15 und 22 )  . 
die rate an tumor - downcategorization dient als parameter der wirksamkeit . ergebnisse : 59 patienten ( davon 68% mnnlich , mittleres alter 61 jahre ) wurden in die studie eingeschlossen . 
akute nebenwirkungen ctc - grad 3 ( common toxicity criteria ) wurden in 15 patienten ( 25% ) registriert , wobei mit 12% eine diarrhoe am hufigsten vorkam . schlussfolgerungen : eine properative radiochemotherapie mit capecitabin und oxaliplatin ist bei patienten mit mittels mri diagnostiziertem ct3 larc gut durchfhrbar . 
allerdings bertrifft die wirksamkeit nicht wesentlich die bisherigen erkenntnisse von studien mit kontinuierlicher 5 - fluorouraciloder alleiniger capecitabingabe . schlsselwrter : rektumkarzinom kombinierte radiochemotherapie capecitabin oxaliplatin introduction despite recent progress in the treatment of locally advanced rectal cancer ( larc ) , which is mainly as a result of improvements in surgical procedures [ 19 , 22 ] , better staging methods [ 2 , 35 ] , and regular use of chemoradiation , patients remain at risk of both local recurrence and distant metastasis . 
however , it has been repeatedly shown that patients with histopathologically confirmed down - staging or regression of the tumor have a better prognosis than patients without down - staging or regression [ 5 , 29 , 33 , 4042 ]  . 
since 5 - fluorouracil ( 5 - fu ) is a regimen in concomitant chemoradiation [ 3 , 10 , 37 , 40 ] with down - staging rates of about 50% , the rationale of the present study was , on the one hand , to exchange infusional 5 - fu with capecitabine and , on the other hand , to add oxaliplatin to intensify systemic therapy in order to improve the proportion of down - staging . 
capecitabine delivers 5 - fu to tumor cells via a three - step in vivo enzymatic conversion , the final step being mediated by thymidine phosphorylase , which is significantly upregulated in tumor tissue compared with healthy tissue [ 28 ] and by radiotherapy [ 38 ]  . 
 this may further increase the preferential delivery of 5 - fu to the tumor following capecitabine administration . in addition to using capecitabine combined with radiotherapy as an option for preoperative therapy in patients with rectal cancer , combining the drug with different chemotherapy agents , such as oxaliplatin or irinotecan , has a clear rationale based on a plethora of data in the metastatic colorectal setting . 
 capecitabine has been tested in combination with oxaliplatin and radiotherapy in several different regimens ( for a review see [ 13 ] ) : continuous capecitabine ( 7 days / week ) with oxaliplatin on days 1 and 29 [ 14 ] ; continuous capecitabine ( 5 days / week ) with weekly oxaliplatin on days 1 , 8 , 22 , and 29 [ 26 , 36 ] ; and discontinuous capecitabine ( days 114 and 2235 ) with oxaliplatin on days 1 , 8 , 22 , and 29 [ 32 , 34 ]  . 
 in contrary to almost all studies published so far in which staging was based either merely on clinical digital examination [ 4 , 8 , 15 , 21 ] or endorectal ultrasonography [ 10 , 15 , 26 , 34 , 42 ] and which consecutively led to a variety of t categories ( from ct2ct4 ) and n categories enrolled , all patients in this study were staged regarding the local extent of the tumor using mri and only ct3 cases regardless of their n status which cannot be accurately determined due to inappropriate sensitivity and specificity of imaging were included . 
the aim of this phase ii multicenter trial was to evaluate the efficacy expressed by down - staging at the t level and safety demonstrated by adverse events of preoperative daily capecitabine ( 5 days / week ) plus weekly oxaliplatin in combination with radiotherapy in the treatment of larc . patients and methods patients male and female patients 1880 years of age with histologically confirmed rectal adenocarcinoma up to a maximum of 14 cm strahlenther onkol 2011 no . 
the study protocol was approved by a local independent ethics committee and conducted in accordance with the declaration of helsinki . pretreatment evaluation before study entry , all patients underwent a medical history , physical examination , biopsy , ecg , and staging studies ( chest and abdominalpelvis computed tomography scan , colonoscopy and endorectal ultrasound )  . 
pelvic mri was mandatory for all patients using a pelvic phased array 1.5 - t six channel surface coil mr imaging machine employing sagittal t2weighted turbo spin - echo ( tse ) 5 , 480 / 100 with a field of view ( fov ) of 250 mm , 3 mm section thickness with gap 30% , and a base resolution of 448 sequences . 
optionally , a further sagittal t1 - weighted tse ( repetition time [ tr ] / echo time [ te ] 557 / 10 ) was used with axial tse t2 - weighted sequences ( tr / te 3 , 510 , fov 250 mm , base resolution 512 ) and selected use of an axial tse t2 - weighted sequence with fat saturation ( tr / te 3 , 800 / 115 )  . 
complete laboratory tests included a full blood count , electrolytes , creatinine , liver transaminases , alkaline phosphatase , total bilirubin , and carcinoembryonic antigen ( cea ) measurement . preoperative chemoradiation radiotherapy was delivered through three to four high - energy photon beams ( 8 mv ) via a 3 - dimensional conformation technique . 
all patients received a total dose of 45 gy , delivered in 25 fractions with a daily fraction of 1.8 gy given 5 days per week for 5 consecutive weeks . 
the permitted cranial limit of the fields was the l5s1 interval , and the caudal limit was at least 5 cm from the lower extension of the tumor ; dorsally , the whole sacral bony structure was encompassed . 
 capecitabine was administered at a dose of 825 mg / m2 twice daily ( b.i.d. ) on radiotherapy days during weeks 14 ( i.e. , the first 20 radiotherapy days )  . 
the first capecitabine dose was taken approximately 2 hours prior to radiotherapy and before oxaliplat if radiotherapy was interrupted for a nonsafety reason ( e.g. , device failure or public holiday ) , capecitabine was continued . 
then , 24 weeks after completion of chemoradiation , low anterior ( lar ) , intersphincteric resection , or abdominoperineal excision ( ape ) , all accompanied with total mesorectal excision ( tme ) , was performed as the preferred type of radical resection according to standardized technique [ 18 ]  . 
administration of adjuvant chemotherapy was left to the treating oncologists discretion . evaluation of efficacy and safety the primary efficacy variable was the rate of tumor down - categorization at the t level . 
the extent of residual tumor in the resected specimen was classified according to the tnm staging system of the american joint committee on cancer / international union against cancer ( ajcc / uicc )  . 
in case of a complete pathological response ( pcr ; i.e. , ypt0ypn0m0 ) , an independent pathologist re - evaluated the tumor tissue . safety was assessed throughout the study by documentation of adverse events and by performing clinical laboratory tests at screening , during treatment , and surgery . 
adverse events were graded using nci - ctc version 3.0. statistical analysis the intent - to - treat population ( itt ) consisted of all patients who received at least one dose of study medication . 
 patients not undergoing surgery or who were not evaluable for response were considered nonresponders . the primary efficacy endpoint was down - categorization ( defined as a decrease of 1 point ( s ) at the t level )  . 
capox and external beam radiation in larc results patient characteristics a total of 59 patients ( 19 women , 40 men ) were enrolled between december 2004 and december 2005 . 
a dose reduction with oxaliplatin therapy was required in 6 patients ( 10.1% ) , while 13 patients ( 22.0% ) had a reduction in capecitabine therapy and 5 ( 8.5% ) a reduction in radiotherapy . 
the median total radiotherapy dose was 45 gy and total doses received was 97% of planned doses . efficacy and surgical parameters out of the 59 patients enrolled , surgery was performed in all patients . 
a total of 41 ( 69.5% ) tumors ( all adenocarcinomas ) were well differentiated ( g12 ) , 9 ( 15.3% ) were classified g3 and the remaining 9 ( 15.3% ) cases were unclassified . 
patientenund tumorcharakteristika ( n = 59 )  . characteristic male / female , n median age , years ( range ) who performance status , 0 / 1 value 40 / 19 61 ( 3476 ) 54 / 5 distance from the dentate line , median cm ( range ) 5.42 ( 013 ) tumor stage ( by mri ) , ct3 , n tumor differentiation , g1 - 2 / g3 / not classified , n 41 / 9 / 9 histologic type , adenocarcinoma / mucinous / others , n 50 / 5 / 4 type of surgery , lar / ir / ape / not available , n lymph nodes removed , median ( range ) 45 / 2 / 11 / 1 15 ( 568 ) table 2 . 
postoperatives , pathologisches staging nach kombinierter radiochemotherapie mit capecitabin und oxaliplatin aller patienten ( n = 59 ) mit mri - klassiziertem ct3 - rektumkarzinodown - categorization : ypt0 - 2 ; n = 31 ; 52 , 5% . category level ypt , n ( % ) 6 ( 10 ) 2 ( 3 ) 23 ( 39 ) 26 ( 44 ) 2 ( 3 ) ypn , n ( % ) 43 ( 73 ) 10 ( 17 ) 6 ( 10 ) m , n ( % ) 59 ( 100 ) r , n ( % ) 52 ( 88 ) 7 ( 12 ) a aall at the circumferential resection margin related with the study treatment in 6 out of these 8 patients . 
 cause of withdrawl from treatment ( severe diarrhea , n = 4 , grade 3 hepatotoxicity , n = 1 ; grade 2 leucopenia , n = 1 ) was the results of the present phase ii study demonstrate that preoperative capecitabine and oxaliplatin in combination with radiotherapy is feasible in patients with larc . 
the goal of the present study was to intensify the systemic part of the combined chemoradiation regimen by adding oxaliplatin in order to maximize the rate of down - staging . 
it has been consistently reported that down - staging of the rectal tumor was associated with enhanced local control and increased disease - free survival [ 9 , 20 , 33 , 42 ]  . 
only patients with mri - proven ct3 category were included in the present study and , therefore , it is attempted to use the rate of down - categorization at the strahlenther onkol 2011 no . 
however , 2 patients were at least categorized ypt4 due to serosa involvement . dosages of capecitabine ( 825 mg / m2 bid ) and oxaliplatin ( 50 mg / m2 ) used in this study were based on previous studies and were also proven in this study to be tolerated well . 
as expected , the only clinically relevant toxicity was diarrhea , 6 patients with grade 3 and one patient with grade 4 , respectively , which was seen in 12% and which is exactly the same rate observed in the trial of rdel et al . 
it seems that a capecitabine abandoned week of radiotherapy decreases grade 3 / 4 diarrhea when compared with previous findings in which capecitabine was given on each day of radiation [ 11 , 26 , 36 ]  . 
furthermore , similar gastrointestinal adverse events were reported in studies that used 5 - fu either as a bolus injection or continuous infusion regimen [ 3 , 10 , 37 ]  . 
over all , grade 3 / 4 toxicities occurred in 13 ( 22.0% ) patients and 6 ( 10.1% ) out of these patients were withdrawn from preoperative treatment , depicting the known increased but acceptable rate of side effects accompanied with intensified chemoradiation [ 27 ]  . tumor down - categorization with respect to the t category was the primary end point of the present study and parameter of efficacy . 
notwithstanding the limitations of a nonrandomized comparison , here too our data on pcr and down - categorization rate at the t level are in line with findings obtained by fluorouracil - based chemoradiation regimens [ 1 , 4 , 10 , 17 , 37 , 40 ]  . 
in these studies and in trials using capecitabine concomitantly with radiation therapy [ 7 , 2325 , 30 , 39 ] , proportions of pcr and down - categorization at the t level clustered near 1015% and 5060% , respectively ( see table 4 )  . 
in contrast , protocols with intensified systemic chemoradiation using capecitabine and oxaliplatin [ 26 , 34 , 36 ] showed only slightly increased efficacy regarding pcr ( 1316% ) and down - categorization at the t level ( 5367% )  . 
results of the recently published accord 12 / 0405 prodige - 2 study [ 12 ] , which is a phase iii study , demonstrated the feasibility of an optimized regimen with concurrent radiation of 50 gy plus capecitabine ( 800 mg / m2 / bid / 5 / 7days ) and oxaliplatin ( 50 mg / m2 / week ) showing compatibility with surgery in 98% with no increase in postoperative complications and merely a trend in favor of a higher rate of r0 resections . 
nevertheless , grade 3 / 4 toxicities increased significantly from 11% to 25% and the benefit of an intensified chemotherapy by adding oxaliplatin could not be demonstrated . in addition , 43 ( 72.9% ) patients represented with negative lymph nodes , which fits in the observation of the present study that intensified chemotherapy does not enhance efficacy as expected . 
at this point , it is important to stress that we did not assess the clinical nodal status in this study , owing to the wellknown insufficiency of imaging [ 16 ] to reliably detect lymph node metastases preoperatively . 
 although most studies indicate down - staging at the nodal status , there is only one study from which valid data can be assumed : from a german trial [ 37 ] , it is known that preoperative chemoradiation in larc decreases lymph node involvement from 40% to 25% . 
regarding a nearly equal amount of lymph node positive cases ( 27.1% ) in the present study , it is justified to assume that down - categorization at the t level was accompanied by a down - staging at the nodal status . 
 cap cap cap cap cap cap cap capox capox capox capox capox 5 - fu / ox capox 45% 39% 37% 61% 55% 53% 72% 67% 52% 16% 8% 11% 11% 16% 12% 24% 18% 23% 14% 28% 13% 16% 15% 10% 25% 25% 33% 41% 30% 27% 22% 28% 17% 26% 27% 14% 12% 13% 23% 8% 11% 10% 30% 11% 16% 12% 16% 24% 12% conclusion preoperative oxaliplatin and capecitabine in combination with radiotherapy is feasible in patients with larc but efficacy was not as pronounced as expected . 
furthermore , summarizing all studies published so far , it is attempted to conclude that with regard to the surrogate parameters pcr , downcategorization at the t level and percentage of lymph node involvement , the addition of oxaliplatin to capecitabine was of no further benefit , but was consistently associated with an obvious increase in toxicities . 
hoffmann3 , matthias peiper4 , klaus orth4 , peter arne gerber5 , ethelyn rusnak6 , guido lammering1 , 7 * , wilfried budach1 * radiation necrosis of normal cns tissue represents one of the main risk factors of brain irradiation , occurring more frequently and earlier at higher total doses and higher doses per fraction . 
consequently , blocking the vascular endothelial growth factor ( vegf ) at an early stage could be an option to reduce the development of radiation necrosis by decreasing the vascular permeability . 
a patient with radiationinduced necrosis was treated with an anti - vegf antibody ( bevacizumab ) , in whom neurologic signs and symptoms improved in accordance with a decrease in t1 - weighted fluid - attenuated inversion recovery signals . 
our case report together with the current literature suggests bevacizumab as a treatment option for patients with symptoms and radiological signs of cerebral necrosis induced by radiotherapy . key words : cerebral radiation necrosis stereotactic neurosurgery radiation therapy bevacizumab hypoxia strahlenther onkol 2011 ; 187 : 1359 doi 10.1007 / s00066 - 010 - 2184 - 4 bevacizumab als behandlungsmglichkeit bei strahleninduzierter radionekrose die strahleninduzierte radionekrose des gehirns stellt eine schwerwiegende komplikation der strahlentherapie dar und tritt bei hohen gesamtdosen oder hohen fraktionierten einzeldosen hufiger und frher auf . 
wir prsentieren hier einen fall einer strahleninduzierten nekrose , bei dem sich unter therapie mit einem anti - vegf antikrper ( bevacizumab ) eine besserung der neurologischen zeichen und symptome in analogie zu einer mr - morphologischen abnahme des t2 - signals zeigte . 
 eine zusammenschau dieses falles und der aktuellen verfgbaren literatur lsst den schluss zu , dass bevacizumab eine behandlungsoption fr patienten mit symptomen und radiologischen zeichen einer strahleninduzierten zerebralen nekrose sein kann . schlsselwrter : zerebrale radionekrose stereotaktische neurochirurgie strahlentherapie bevacizumab hypoxie * authors contributed equally to this work . 1department of radiation oncology , university hospital dsseldorf , dsseldorf , germany , 2department of radiology , university hospital dsseldorf , dsseldorf , germany , 3department of otorhinolaryngology , university of duisburg - essen , essen , germany , 4department of surgery , department of surgery , hospital essen - sd , essen , germany , 5department of dermatology , university hospital dsseldorf , dsseldorf , germany , 6deparment of anesthesiology , state university of new york at buffalo , buffalo , ny , usa , 7radiation oncology ( maastro clinic ) , maastricht , the netherlands . received : june 14 , 2010 ; accepted : november 11 , 2010 published online : january 24 , 2011 strahlenther onkol 2011 no . 
bevacizumab as a treatment option for radiation - induced cerebral necrosis introduction cerebral radiation necrosis represents one of the most dreaded toxicities of radiation therapy to the brain [ 1 , 3 , 4 , 9 , 14 , 16 ]  . 
however , recently a growing number of groups have published their experience with bevacizumab ( avastin , genentech , san francisco , ca , usa ) as a treatment strategy for cerebral necrosis [ 13 , 21 , 22 , 25 ]  . 
in addition , a review of the current literature is given . case report a 19 - year - old caucasian man with a 2 - year history of an astrocytoma grade iii ( side ventricle basal ganglion ) was admitted with a recurrent relapse in august 2009 . 
he had received adjuvant radiotherapy of the brain with 59.4 gy ( 33 fractions over 6.5 weeks ) from may to july 2008 after partial tumor resection with concomitant daily temozolamide 75 mg / m2 , followed by maintenance temozolamide ( 150 mg / m2 once a day for 5 consecutive days every 28 days )  . 
on admission , magnetic resonance imaging ( mri ) of the brain showed a slowly progressing mass medial to the lateral ventricle at the former tumor bed without signs of contrast enhancement on mri . 
the patient underwent [ 18f ] fluoroethyltyrosine ( fet ) positron emission tomography ( pet ) , revealing no uptake of radionuclide in the corresponding region of the progressive mass . 
on the contrary the symptoms increased . these findings suggested a radiation - associated necrosis of the brain parenchyma , which prompted us to initiate a treatment attempt with bevacizumab ( 10 mg / kg every 2 weeks for 3 months )  . 
representative t1 - weighted neurocranial mri images after application of gadolinium with fat suppression of the patient 2 and 5 months after stereotactic radiosurgery , and 2 months after initiation of bevacizumab therapy . 
further 5 months later a new lesion developed at the dorsal border of the necrosis that was histologically proven to be glioblastoma . discussion cerebral radiation necrosis is a potential complication for patients undergoing radiation therapy of the central nervous system [ 4 , 8 , 10 , 14 ]  . 
seit 2007 publizierte berichte zur bevacizumab - behandlung bei radionekrose des zentralen nervensystems . treatment schedule cases biopsy proven necrosis neurocognitive improvements not reported dexamethasone requirements average reduction 8.6 mg toxicity not reported 8 weeks fu time ( mean ) study gonzalez et al . , 2007 [ 6 ] wong et al . , 2008 [ 25 ] liu et al . , 2009 [ 13 ] torcuator et al . , 2009 [ 21 ] levin et al . , 2010 [ 12 ] radiographic response ( mri ) 48% t1 60% flair 100% 3 / 4 without quantification 79% t1 49% flair 63% t1 59% flair 100% . 
2weeks 4 mini - mental status from 2630 ( total 30 ) not reported not reported 6 months not reported not reported not reported 5 months 3 / 6 improved 3 / 6 stable all improved all tapered off 1 / 6 fatigue 5.9 months all dose reduction 6 / 11 10 months initially 38 mg , dose reduction 75% to 32 mg not clearly related : pneumonia , wound - healing disorder , seizure case presented partially improved 8 weeks covery , t2 signals in the irradiated fields , and hemorrhagic transformation to necrotic cysts , causing a mass effect . 
the development of cerebral radiation necrosis after radiotherapy largely depends on the applied total dose and the dose per fraction , accounting for a risk of 219% [ 14 , 16 , 19 ]  . 
the latency period between irradiation and first symptoms varies from a few months to up to 3 years with a mean of 11.6 months [ 4 , 14 ]  . 
pathophysiological mechanisms underlying this toxicity are thought to mainly consist of endothelial abnormality with elevated cytokines , e.g. , vegf , resulting in increased vascular permeability , a cascade of inflammatory events , extracellular edema , loss of neuron covering with myelin , and finally hypoxia and necrosis [ 4 , 15 , 25 ]  . in experimental settings , brains of rabbits developed microhemorrhages when they were treated with proton stereotaxic radiosurgery . 
likewise , in the gastrointestinal tract of mice treated with 15 gy of whole - body irradiation , radiationinduced endothelial cell apoptosis was the key mechanism leading to stem cell dysfunction , crypts damage , and death [ 2 , 17 ]  . 
even though the kinetics of this damage are unidentified in experimental animals , patients who received radiation doses of 62.5 gy or more are faced with a more than 25% chance of radiation necrosis within 5 years . 
our patient received a dose of up to 18 gy to the brain ( the preexisiting applied dose in the irradiated area was 59.4 gy ) in a single fraction . the standard treatment in patients with radionecrosis consists of corticosteroids to reduce the amount of cerebral edema and , if required , cyst drainage . 
thus , we decided to treat our patient with bevacizumab , a humanized monoclonal antibody directed against the vegf , which has been recently promoted as a promising treatment option for cerebral necrosis due to the rationale that preventing vegf from reaching its endothelial targets might reverse the development of radiation necrosis . 
however , one drawback of using such an antiangiogenic drug is related to the fact that it complicates the interpretation of the treatment efficiency by mri due to profound effects on the vascular biology of these tumors ( pseudoregression ) [ 20 ]  . 
in these initial experience reports , neurocognitive defects , cerebral edema , and enhancement on mri were reversed and steroid requirements were reduced in most patients , while a few patients were clinically stable under bevacizumab treatment . 
in all patients , bevacizumab was well tolerated . an overview of all reported patients treated with bevacizumab , including the very recently published first randomized double - blind placebo - controlled clinical trial of bevacizumab therapy for radiation necrosis with 11 patients included in the bevacizumab treatment arm , is provided in table 1 . 
all patients in this trial treated with bevacizumab responded with decreases in t2 - weighted fluid - attenuated inversion recovery and t1weighted gadolinum - enhanced volumes and a decreased endothelial transfer constant ; all patients showed an improvement in neurological signs and symptoms . 
thus , it might be appropriate to also treat patients with low - dose anticoagulation while on bevacizumab treatment [ 18 ]  . conclusion to date , a total of 30 patients with bevacizumab treatment for cerebral radiation necrosis have been reported in the literature , most of whom responded with symptomatic relief , improvement in radiological signs of necrosis with limited toxicity except for thrombosis . 
thus , it can be concluded that bevacizumab at a dose of at least 7.5 mg / kg every 3 weeks for 12 weeks may stop further progression of radiation necrosis and relieve symptoms . 
2 strahlentherapie und onkologie current discussion optimizing the quality of breast cancer care at certified german breast centers a benchmarking analysis for 20032009 with a particular focus on the interdisciplinary specialty of radiation oncology sara y . 
beckmann5 , michael bamberg6 , diethelm wallwiener1 , * * , rainer souchon6 , * * purpose : a voluntary , external , science - based benchmarking program was established in germany in 2003 to analyze and improve the quality of breast cancer ( bc ) care . 
based on recent data from 2009 , we aim to show that such analyses can also be performed for individual interdisciplinary specialties , such as radiation oncology ( ro )  . methods : breast centers were invited to participate in the benchmarking progranine guideline - based quality indicators ( qis ) were initially defined , reviewed annually , and modified , expanded , or abandoned accordingly . 
qi changes over time were analyzed descriptively , with particular emphasis on relevance to radiation oncology . results : during the 20032009 study period , there were marked increases in breast center participation and postoperatively confirmed primary bcs . 
 during 20032009 , 2 / 7 ro - relevant qis ( radiotherapy after breast - conserving surgery or after mastectomy ) showed considerable increases ( from 20 to 85% and 8 to 70% , respectively )  . 
another three , initially high qis practically reached the required levels . conclusion : the current data confirm proof - of - concept for the established benchmarking program , which allows participating institutions to be compared and changes in quality of bc care to be tracked over time . 
 key words : breast cancer benchmarking quality of care quality assurance radiotherapy strahlenther onkol 2011 ; 187 : 8999 doi 10.1007 / s00066 - 010 - 2202 - 6 onkologische qualittsoptimierung in der mammakarzinomversorgung an zertifizierten deutschen brustzentren : eine benchmarkinganalyse fr 20032009 unter besonderer bercksichtigung eines querschnittsfaches , der radioonkologie ziel : in deutschland wurde 2003 ein flchendeckendes , freiwilliges , externes wissenschaftliches benchmarkingsystem zur analyse und verbesserung der versorgungsqualitt beim mammakarzinom etabliert . 
die zeitlichen vernderungen insbesondere der radioonkologisch relevanten qis wurden deskriptiv ausgewertet . * joint first authors and equal contributors . * * joint last authors and equal contributors . 1department of obstetrics and gynecology , university of tbingen , tbingen , germany , 2department of obstetrics and gynecology , university of heidelberg , heidelberg , germany , 3department of obstetrics and gynecology , university of ulm , ulm , germany , 4department of obstetrics and gynecology , university of kiel , kiel , germany , 5department of obstetrics and gynecology , university of erlangen , erlangen , germany , 6department of radiation oncology , university of tbingen , tbingen , germany . 
drei weitere , bereits initial hohe qi erreichten praktisch die vorgabewerte . schlussfolgerung : mit den aktuellen daten besttigt sich der proof - of - concept fr das etablierte benchmarkingsystem , welches den vergleich teilnehmender einrichtungen sowie die beobachtung zeitlicher vernderungen in der brustkrebsversorgungsqualitt des gesamten netzwerks erlaubt . 
anhand von teilspektren relevanter qi lassen sich zudem fortschritte , aber auch der weitere verbesserungsbedarf fr einzelne querschnittsfcher nachweisen . schlsselwrter : mammakarzinom benchmarking versorgungsqualitt qualittssicherung radiotherapie introduction over the past decade , specialist breast centers have been created in germany to improve the care provided to breast cancer patients . 
the main objective in establishing such multidisciplinary centers was to ensure that care was based on clinical guidelines and continual quality assurance ( qa ) measures , and that quality management ( qm ) systems were introduced . 
 in addition , it has become a legal requirement in germany in recent years that all healthcare service providers introduce qa programs and maintain a qm system [ 4 , 5 , 8 , 21 ]  . since 2003 , a qm system and continual qa with comprehensive documentation of all treatments and external analysis of the qa data have also been prerequisites for certification to the requirements of breast centers ( fachliche anforderungen fr brustzentren ; fab ) in germany [ 4 , 5 , 8 , 10 ]  . 
the fab were jointly developed by the german cancer society ( deutsche krebsgesellschaft ; dkg ) and the german society of senology ( deutsche gesellschaft fr senologie ; dgs ) largely on the basis of two evidence - based multidisciplinary level - 3 guidelines [ 1 , 16 , 17 , 22 ] and the eusoma ( european society of breast cancer specialists ) requirements for accreditation of breast units [ 2 ]  . 
 based on specific data items from the 173 , later 185 , individual fab items , the dgs , dkg , german society of obstetrics and gynecology ( dggg ) , and the west german breast center / german oncology center ( westdeutsches brust - centrum / deutsches onkologie centrum ; wbc / doc ) jointly developed a set of uniformly calculated structural and process quality indicators ( qis ) of breast cancer care as surrogates for long - term outcome qis . 
proof of concept for the program was demonstrated by analyzing the data from the first 4 - year and 5 - year periods [ 6 , 7 , 27 ]  . 
 the analysis of the 7 - year qi data reported here focuses particularly on the qis relevant to radiation oncology as an important interdisciplinary field in cancer therapy and aims to show that the 20032009 data confirm the previously reported 4and 5 - year results . methods study design and objectives the present study is the continuation of a previously reported prospective , interventional , multicenter proof - of - concept study which showed that the quality of bc care in germany could be measured scientifically , and improved by implementing a nationwide benchmarking program based on qis . 
these were derived from clinically relevant parameters which reflected key criteria of the two level - 3 guidelines developed by the relevant scientific medical societies [ 1 , 16 , 17 , 22 ]  . 
details of the study design and methodology have been reported previously [ 6 , 7 ]  . the objective of the present analysis was to demonstrate that it is also possible to consider the specific qis individually and to analyze them by medical specialty , i.e. , the interdisciplinary field of radiation oncology in the present case , and that nationwide collaborative benchmarking was associated with improvements in the guideline - concordant and appropriate radiation treatment of bc during 20032009 . participating centers , data collection , and data analysis specialist breast centers were invited to participate voluntarily in an external , independent , scientific benchmarking program developed by the dkg and the dgs and operated by the west german breast center / german oncology center ( wbc / doc ) , dsseldorf , germany . 
 data collection began individually for each breast center after its voluntary registration with the benchmarking prografor each patient , 173185 parameters from the dkg / dgs requirements of breast centers ( fachliche anforderungen an brustzentren ; fab [ 10 ] ) were collected by staff members of the participating centers from 1 january , 2003 to 31 december , 2009 . 
anonymized , encrypted datasets were submitted to the wbc / doc on cd - rom twice a year for independent external overall and center - specific analyses [ 7 ]  . 
standard software was used ( access , excel , and word from microsoft office 2002 / 2003 and microsoft sql server 2005 ( microsoft corporation , redmond , wa , usa ) )  . 
the query logic was written in sql and , hence , compatible with other software . quality indicators based on selected clinically relevant fab data items , qis were calculated according to uniform algorithms and were designed to determine the degree to which predefined quality targets were met . 
changes in qis during the 20032009 period were analyzed using descriptive methods ( tables and histograms ) and reported annually [ 7 , 28 , 29 ]  . plausibility checks and monitoring data plausibility was ensured by twice yearly wbc / doc monitoring visits and data reviews at the annual participants meetings . 
the monitoring visits were conducted primarily to ensure the correctness and completeness of the electronic documentation of patients medical records and also provided opportunities for advice on the documentation process [ 7 , 28 , 29 ]  . 
this was also accompanied by a steady increase in postoperatively confirmed primary bc patients per participating institution from 101.59 in 2003 to 165.5 in 2009 , reflecting an overall increase above the dkg / dgs requirement that breast centers should annually treat a minimum of 150 primary breast cancers . 
the overall number of primary bcs ( as confirmed by postoperative histology ) also increased 6.30 - fold during the 7 - year study period , as shown in figure 2 . 
for completeness , table 1 also lists 9 qis and sub - qis ( in italics ) that were discontinued at the end of 2006 and 2007 , thus , illustrating the discontinuation of qis that lacked discriminatory power . 
 table 2 shows the addition , modification , or discontinuation of qis , in particular the addition of new qis during 20052009 ( the latest addition being qi 7.2 ) , the replacement of nos . 
figure 3 shows the relative performance of qis as a percentage of the third - year dkg / dgs requirement , where applicable , illustrating how these qis developed during from 20032009 . 
9a ( radiotherapy after bcs ) and 10 ( radiotherapy after mastectomy ) increased from very low levels ( 21% and 10% ) to high ( 89% and 88% ) levels relative to the respective dkg / dgs requirements . 
from 2008 to 2009 , the percentage of patients given radiation therapy for dcis rose from 65% to 75% , thus , showing an increase in performance from 130% to 150% relative to the figure 2 . 
patients with primary breast cancer according to the dkg / dgs definition ( preor postoperatively histologically confirmed ; including dcis but excluding lcis alone ) and patients with postoperatively , histologically confirmed primary breast cancer as reported by the participating institutions during 20032009 . 
anzahl patientinnen mit primrem mammakarzinom gem dkg / dgs - definition ( proder postoperativ histologisch gesichert ; einschlielich dcis , aber ohne alleiniges lcis ) sowie anzahl patientinnen mit postoperativ gesichertem primrem mammakarzinom , wie seitens der teilnehmenden einrichtungen im zeitraum 20032009 gemeldet . 
3 and 4 ( both introduced in 2007 ) increased from 91% to 98% and from 83% to 92% , respectively , during 20032009 . discussion in line with european policies [ 12 , 13 ] , health policies in germany have in recent years emphasized the increasing importance attributed to breast cancer . 
efforts have been directed towards developing and implementing structured , multidisciplinary quality management programs designed to optimize breast cancer care and reduce both inappropriate care and the overand underprovision of care . 
n.d. : no details , dcis : ductal carcinoma in situ , dkg : deutsche krebsgesellschaft ( german cancer society ) , dgs : deutsche gesellschaft fr senologie ( german society of senology ) , l3 - gl / ed - bc ( 2003 ) : level - 3 guidelines for the early detection of breast cancer in germany ( 2003 ) [ 22 ] , l3 - gl / dt - bc ( 2004 ) : interdisciplinary s3 guidelines for the diagnosis and treatment of breast cancer in women ( 2004 ) [ 16 ] , l3 - gl / dt - bc ( 2008 ) : interdisciplinary s3 guidelines for the diagnosis and treatment of breast cancer . 
b square brackets and italics indicate qis which were discontinued at the end of 2006 or 2007 . study was initiated in 2003 , the necessary infrastructure for a benchmarking program with uniform data collection , external data analysis , and specific collaboration agreements did not exist in germany or elsewhere [ 7 ]  . 
 moreover , literature searches up to 2009 yielded no evidence that other countries had mandatory or voluntary supraregional interinstitutional benchmarking programs for assessing the quality of care provided to bc or other cancer patients . 
 this shows the novelty of the approach that has been pursued in germany since 2003 to create a nationwide benchmarking network of breast centers . guidelines of high methodological quality which are consistent with the principles of evidence - based medicine ( ebm ) aim to ensure and improve the quality of care for all patients , and cancer patients in particular . 
although the necessity of guideline - concordant treatment had long since been recognized , the implementation and acceptance of guideline - concordant procedures along the entire process chain of breast strahlenther onkol 2011 no . 
csquare brackets and italics indicate qis which were discontinued at the end of 2006 or 2007 . cancer care from diagnosis and treatment to follow - up was not studied on a large scale in germany until 2003 [ 6 , 7 ]  . 
 the creation of site - specific and comprehensive cancer centers , the implementation of a structured , intersectoral quality management ( qm ) system for the standardization and optimization of all procedures , and the comprehensive documentation of treatment procedures are considered key elements of quality assurance and high - quality care [ 4 , 8 ]  . 
performance of quality indicators ( qis ) during the 20032009 period as a percentage of the respective third - year dkg / dgs requirements of breast centers ( fab )  . 
1 ( preoperative histological confirmation of diagnosis ) was compared against the stricter dkg / dgs requirement of 90% ( for palpable tumors as opposed to 70% for nonpalpable tumors ) as the benchmark . 
qis labeled ex - 3 ( complete tumor staging data ) and ex - 4 ( her 2 / neu assessment ) were discontinued at the end of 2006 and replaced by qis 3 ( data on safety distance between tumor and resection margin ) and 4 ( specimen imaging ) in 2007 . 
1 : preoperative histological confirmation of diagnosis , 2a : appropriate axillary dissection , 2b : patients with slnb , ex - 3 : complete tumor staging data , 3 : data on safety distance between tumor and resection margin , ex - 4 : her - 2 / neu assessment , 4 : specimen imaging , 5 : hormone receptor assessment , 6 : guideline - concordant endocrine therapy in hormone receptor - positive patients , ex - 7.1a : guideline - concordant adjuvant and neoadjuvant chemotherapy during the previous analysis period ( age 70 years ) , 7.1a : guideline - concordant adjuvant and neoadjuvant chemotherapy during the current analysis period ( age 70 years ) , 7.2 : adjuvant combination chemotherapy with anthracyclines and / or taxanes , 8 : percentage of patients in clinical trials , 9a : radiotherapy after breast - conserving surgery , 9b : radiotherapy after breast - conserving surgery for dcis , 10 : radiotherapy after mastectomy , 11b : indication for breast - conserving therapy at t1 . 
relativer erfllungsgrad der qualittsindikatoren ( qis ) im zeitraum 20032009 als prozentsatz der jeweiligen vorgabe fr das dritte jahr der zertifizierung gem den fachlichen anforderungen an brustzentren ( fab )  . 
ex - 3 ( daten zum vollstndigen tumor staging ) und ex - 4 ( her 2 / neu - erfassung ) wurden ende 2006 aufgegeben und 2007 durch qis 3n ( angaben zum sicherheitsabstand zwischen tumor und resektionsrand ) und 4 ersetzt ( specimen imaging )  . 
1 : properative histologische diagnosesicherung ; 2a : ausreichende axillary dissection ; 2b : patienten mit wchterlymphknoten - biopsie ; ex - 3 : vollstndiges tumor - staging ; 3 : sicherheitsabstand zwischen tumor und resektionsrand ; ex - 4 : her - 2 / neu - status ; 4 : specimen imaging ; 5 : hormonrezeptor - status , 6 : leitliniengerechte endokrinologische therapie hormonrezeptor - positiver patientinnen ; ex - 7.1a : leitliniengerechte adjuvante und neoadjuvante chemotherapie im vorherigen untersuchungszeitraum ( alter 70 jahre ) ; 7.1a : leitliniengerechte adjuvante und neoadjuvante chemotherapie im aktuellen untersuchungszeitraum ( alter 70 jahre ) ; 7.2 : adjuvante kombinationschemotherapie mit anthrazyklinen und / oder taxanen ; 8 : prozentsatz von patientinnen in klinischen studien , 9a : strahlentherapie nach brusterhaltender op ; 9b : strahlentherapie nach brusterhaltender op eines dcis ; 10 : strahlentherapie nach mastektomie ; 11b : indikation zur brusterhaltenden therapie bei t1 . when the present nationwide , voluntary benchmarking program was implemented in germany in 2003 as the first of its kind , it was unclear whether it would be possible to objectify quality of care and outcome quality . 
in the absence of long - term indicators of outcome quality in breast cancer care , e.g. , morbidity and mortality rates , which require data covering at least 510 years , it was first necessary to define quality targets and use clinical measures based on the relevant level - 3 guidelines [ 16 , 17 ] to derive process qis as surrogates for outcome quality . 
the performance of these process qis over time has enabled us within a few years to objectify the extent of adherence to the process quality generally recognized as necessary for high - quality care . the 7 - year data reported here support the hypothesis that improvements in the quality of cancer care can be achieved and objectified by benchmarking and measuring the perforstrahlenther onkol 2011 no . 
quality indicator ( qi ) tracked 2003 2004 2005 2006 2007 2008 2009 3rd - year dkg / [ ex - 3 ] a complete tumor staging data 20032006 89% 101% 103% 100% data on safety distance between tumor and resection margin specimen radiography ( 2007 : preoperative in patients with microcalcifications ; 2008 : intraoperative ) percentage of patients in clinical trials 20072009 20072009 radiotherapy after breast - conserving surgery 20032009 21% 48% 63% 74% 83% 84% 89% > 95% radiotherapy after breast - conserving surgery for dcis 20082009 130% 150% > 50% radiotherapy after mastectomy 20032009 10% 33% 44% 59% 81% 81% 88% > 80% 20052009 40% 35% 35% 40% 60% 20% asquare brackets and italics indicate qis which were discontinued at the end of 2006 or 2007 . 
during 20032009 , radiotherapy after breast - conserving surgery ( qi 9a ) increased from 20% to 85% , and radiotherapy after mastectomy ( qi 10 ) increased from 8% to 70% . 
these improvements are likely due , on the one hand , to better documentation but may , on the other hand , also reflect a later increase in more guideline - concordant decision - making about adjuvant therapy . 
moreover , it must be borne in mind that the program initially covered only the very limited number of 6 , 000 patients from as few as 59 breast centers , and this raises some doubt as to whether the early data actually provide a representative picture of the situation in radiation oncology care in germany at that time . 
in fact it appears likely that initially patients receiving treatment were lost to documentation due to inadequacies in the documentation procedures , resulting in underestimation of treatment and , hence , overestimation of subsequent increases in the quality of radiation oncology care . 
nonetheless , the qi increases observed later in the study can be assumed to reflect actual improvements in quality of care , not least because regular monitoring visits contributed substantially to eliminating the initial deficits in treatment documentation . 
the increase observed for qi 9b , on the other hand , appears far more credible than the dramatic increases in qis 9a and 10 because qi 9b was introduced only recently , at a time when data collection and data administration were fully established . 
furthermore , evidence - based guidelines were not available initially , and the indications for adjuvant radiotherapy , though they had been clearly formulated , were not yet widely known [ 24 ]  . 
this situation changed when the dkg and dggg published evidence - based guidelines for the diagnosis , treatment , and follow - up care of breast cancer in 2004 [ 16 ] , updating them in 2008 [ 17 ]  . 
more recently , the german society of radiation oncology ( degro ) added supporting practical guidelines on breast - conserving therapy [ 19 ] , postmastectomy radiotherapy , irradiation of regional lymphatics and treatment of locally advanced disease [ 20 ] , and palliative radiotherapy of breast cancer - related brain metastases and leptomeningeal carcinomatosis [ 14 ] as well as bone metastases and metastatic spinal cord compression [ 23 ]  . by 2009 , the performance levels of qis 9a and 10 had practically reached the respective dkg / dgs requirements . 
9b , which was newly introduced in 2008 , the first and second - year performance levels of 65% and 75% already exceeded the dkg / dgs requirement of 50% introduced in 2009 . 
this likely reflects the increasing implementation of the degro guidelines . a meta - analysis published in 2005 investigating the effects of radiotherapy and of differences in the extent of surgery for early breast cancer on local recurrence and 15 - year survival is also likely to have prepared the ground for the still growing acceptance of adjuvant radiotherapy in breast cancer [ 11 ]  . 
it conveyed , also to the nonradiation oncologist , the evidence supporting the multiple benefits of radiation treatment in terms of both local and locoregional tumor control and patient survival if radiotherapy is systematically included as an integral part of a multimodal treatment plan . 
several recent studies have also found radiotherapy to have beneficial effects on the survival of breast cancer patients [ 15 , 25 , 26 ]  . as regards the qis nos . 
optimizing the quality of breast cancer care overall , the present 7 - year data confirm the trends seen in the 4and 5 - year results previously reported and discussed in detail by brucker et al . 
the success of the german voluntary benchmarking program for quality in breast cancer care is evidenced by the 3.86 - fold increase in participating centers from 59 to 228 and the 6.30 - fold increase from 5 , 994 to 37 , 740 in patients with primary breast cancer ( as confirmed by postoperative histology ) from 2003 to 2009 and the remarkable cumulative number of more than 167 , 000 datasets collected by the end of 2009 . the numerous challenges encountered when designing , setting up , and funding such programs , even at the institutional and regional levels , have recently been reported e.g. , for the united states , where the american society of clinical oncology ( asco ) and the national comprehensive cancer network ( nccn ) have collaborated to identify quality - of - care measures for breast cancer and other malignancies with the ultimate aim of implementing performance metrics at the national level [ 3 , 9 , 18 ]  . 
 conclusion the high incidence of breast cancer and the necessity for structured multidisciplinary care makes this cancer an ideal candidate to investigate whether a national scientific benchmarking program based on voluntary documentation of all treatment procedures and collection , centralized compilation , and external analysis of the data can be used to measure and evaluate of the quality of cancer care . 
the acceptance of the benchmarking concept and its postulates is evidenced by the increasing numbers of breast cancer patients treated at the participating breast centers in germany most of them now dkg / dgs certified from 15% in 2003 to about 70% in 2009 . 
 thus , the voluntary benchmarking program reported here has enabled the first direct , objective , and valid assessment of the reality of breast cancer care at specialist breast centers in germany . 
finally , in the age of the creation and certification of specialist breast centers , improvements in the primary treatment of breast cancer have been achieved by rapid increases in indication - appropriate radiotherapy and other cancer treatments between 2003 and 2009 . abbreviations bc : breast cancer ; bcs : breast - conserving surgery ; bct : breast - conserving therapy ; dggg : deutsche gesellschaft fr gynkologie und geburtshilfe ( german society of obstetrics and gynecology ) ; dgs : deutsche gesellschaft fr senologie ( german society of senology ) ; dcis : ductal carcinoma in situ ; degro : deutsche gesellschaft fr radioonkologie ( german society of radiation oncology ) ; dkg : deutsche krebsgesellschaft ( german cancer society ) ; doc : deutsches onkologie centrum holding gmbh ( german oncology centre ltd . ) ; eusoma : european society of breast cancer specialists ( formerly : of mastology ) ; fab : fachliche anforderungen an brustzentren ( requirements of breast centers ) ; her - 2 / neu : human epidermal growth factor receptor 2 ; pqi : process quality indicator ; qa : quality assurance ; qi : quality indicator ; qm : quality management ; slnb : sentinel lymph node biopsy ; sql : structured query language ; wbc : westdeutsches brust - centrum ( west german breast center ) ; xml : extensible markup language . 
mahyar badiian ( doc , dsseldorf , germany ) , johannes bruns ( dkg , berlin , germany ) , and hubertus fries ( wbc , dsseldorf , germany ) as well as andreas kmmerle ( onkozert gmbh , ulm , germany ) for fruitful discussions and support with data collection . strahlentherapie und onkologie original article omega - 3 fatty acid supplementation in cancer therapy does eicosapentanoic acid influence the radiosensitivity of tumor cells ? katrin manda1 , stephan kriesen1 , guido hildebrandt1 , rainer fietkau2 , gunther klautke2 purpose : the aim of this study was to evaluate whether the omega - 3 polyunsaturated fatty acid cis - 5 , 8 , 11 , 14 , 17 - eicosapentanoic acid ( epa ) can enhance the radiosensitivity of different human tumor cell lines . 
cell growth was observed during administration with different concentrations of epa , using it as the free fatty acid dissolved in ethanol or bound to bovine serum albumto investigate the influence of epa ( free and bound ) on radiosensitivity , tumor cells were pretreated 30 minutes or 24 hours prior to irradiation with the fatty acid . 
 results : when combined with irradiation , incubation with epa was found to result in enhanced radiosensitivity with substantial variation : while there was strong radiosensitization for ht - 29 and u251 cells , almost no effect for t98g cells was observed . 
 conclusion : the observations suggest that epa is not only a nutritional adjuvant but also may be a potential candidate to enhance the efficacy of irradiation on human cancer cells . key words : n - 3 pufa eicosapentanoic acid epa membrane lipid peroxidation strahlenther onkol 2011 ; 187 : 12734 doi 10.1007 / s00066 - 010 - 2166 - 6 omega - 3 - fettsuren in der krebstherapie : beeinflusst eicosapentaensure die strahlensensibilitt humaner tumorzellen ? ziel : in der vorliegenden arbeit wurde geprft , ob die polyungesttigte omega - 3 - fettsure cis - 5 , 8 , 11 , 14 , 17 - eicosapentaensure ( epa ) die strahlensensibilitt verschiedener humaner tumorzelllinien erhhen kann . methodik : zellen eines kolorektalen adenokarzinoms ( ht - 29 ) sowie zweier glioblastome ( t98g und u251 ) wurden unter standardbedingungen kultiviert . 
dabei erfolgte die zugabe von epa entweder als freie fettsure ( gelst in ethanol ) oder gebunden an albumzur untersuchung der wirkung von epa ( frei und gebunden ) auf die strahlensensibilitt der tumorzellen wurden die zellen 30 min bzw . 
24 h vor der bestrahlung mit der fettsure behandelt und das zellberleben anhand von koloniebildungstests ermittelt . ergebnisse : die zustzliche behandlung der zellen mit epa vor der bestrahlung resultierte in einer unterschiedlich stark ausgeprgten erhhung der radiosensitivitt der tumorzellen : whrend fr die ht - 29and u251 - zellen eine deutliche strahlensensibilisierung nachweisbar war , konnte bei den t98g - zellen kein effekt verzeichnet werden . 
 zusammenfassung : die erhaltenen ergebnisse zeigen , dass die omega - 3 - fettsure epa in der tumortherapie nicht nur als nahrungsergnzungsmittel von bedeutung ist , sondern mglicherweise auch zur wirkungssteigerung der bestrahlung auf tumorzellen beitragen kann . 
 schlsselwrter : n - 3 pufa eicosapentaensure epa membran lipidperoxidation 1department of radiotherapy , university of rostock , rostock , germany , 2department of radiation oncology , university hospital erlangen , erlangen , germany . received : april 26 , 2010 ; accepted : november 15 , 2010 published online : january 18 , 2011 strahlenther onkol 2011 no . 
eicosapentanoic acid in radiotherapy introduction knowledge about the importance of omega - 3 polyunsaturated fatty acids ( n - 3 pufas ) in human health and diseases has been increasing constantly during recent years . 
many studies showed a positive role of n - 3 pufas , including cardiovascular diseases [ 36 , 52 ] , various mental illnesses [ 44 ] , and cancer [ 1 , 15 ]  . 
 many experimental studies in different cell cultures and animal models determined the antitumor effect of n - 3 pufas in vitro [ 7 , 22 , 25 , 29 ] and in vivo [ 3 , 8 , 50 ]  . 
the central effect seems to be their influence on cell membranes , because they are the main starting substances for lipid peroxidation ( lipo ) [ 25 , 32 , 33 ]  . 
these products are basically responsible for significant consequences of cell function , such as alteration of membrane fluidity plus permeability , inhibition of nucleic acid and protein synthesis up to apoptosis [ 16 , 24 , 38 ] and possibly has effects on membraneassociated proteins , e.g. , egfr ( epidermal grow factor receptor ) [ 23 ] , or transmembrane proteins , e.g. , caveolin - 1 [ 4 ]  . 
eicosapentanoic acid in radiotherapy tomycthe u251 cells were incubated additionally with 2% hepes [ 4 - ( 2 - hydroxyethyl ) - 1 - piperazineethanesulfonic acid ] as well as nea ( nonessential amino acids ) and sodium pyruvate , each 1% . 
under a n2 atmosphere , 50 mg of the fatty acid was entirely dissolved in 100 l ethanol , diluted with 1553 l phosphate - buffered saline ( pbs ) , and then sterile filtered . 
for the final experiments the necessary amount of epaalbumin stock solution ( 1 mm ) was diluted with serum - free medium and sterile filtered prior to being added to cultures . experiments with epa only for cytotoxicity tests , cells were seeded in 24 - well test plates at a density of 2x103 cells / ml per dish and allowed to grow for 24 hours to achieve exponential growth before epa was added . 
for all three cell lines , experiments with solvent ethanol in appropriate amounts ( less than 0.3% vol / vol ) showed no differences to controls with ethanol - free attempts . 
 for the epaalbumin treatment , the medium was completely removed , cells were washed with pbs , replaced by the new serum - free medium containing the final drug concentration of epaalbumin , and incubated for 96 hours . 
the images were visualized with an eclipse te300 inverted microscope ( nikon , tokyo , japan )  . experiments with epa and irradiation appropriate numbers of cells were plated in 25 cm2 culture flasks , incubated overnight with standard medium , treated with epaethanol or epaalbumin , respectively , and exposed to various single doses of radiation using a linear accelerator ( md2 siemens , germany ) at 2 gy / min ( energy 6 mev )  . 
 results effect of epa only to investigate the influence on the growth of human tumor cells , epa was used in two different treatment methods , as free fatty acid dissolved in ethanol or bound to bsa . epaethanol increasing concentrations of epaethanol reduced the growth of cells of all three human tumor cell lines ( figure 1 )  . 
phase contrast microscopy allowed observation of lipid droplets in cells that were incubated for 24 hours with epa ( figure 2 ) , but no lipid droplets were observed in cells examined after a 30 - minute epa treatment . 
 epaalbumin even in the control experiments where cells were seeded in serum - free medium containing only bsa , cell counts for all three tumor cell lines were extremely decreased . 
therefore , the experimental setup was changed and cells were allowed to grow for 24 hours in standard mediu after that time , the medium was replaced by serum - free bsa - supplemented medium with or without epa . 
treatment of cells with 30 m epaalbumin instead of albumin showed inhibition of cell growth compared to controls , but these were not significant ( data not shown )  . 
eicosapentanoic acid in radiotherapy radiation doses ( 48 gy ) the radiosensitivity of u251 was more pronounced . for subsequent experiments with epaalbumin , it was necessary to evaluate the general influence of the lack of serum on the survival of the cells . 
 epaethanol the application of 30 m epaethanol 30 minutes prior to irradiation resulted in an enhancement of radiation toxicity in the ht - 29 and u251 cells ( figure 4a ) , whereas a 24 hour epa incubation prior to irradiation resulted in almost no radiosensitization of the two cell lines ( figure 4b )  . 
for the drug application only 30 minutes prior to radiation , there was an obvious reduction in cell survival fraction for ht - 29 cells , which showed a pronounced radiosensitization . 
effect of epaethanol and radiation on the surviving fraction of different cell lines ht - 29 , t98g , and u251 , when treated 30 minutes ( a ) or 24 hours ( b ) prior to irradiation . 
wirkung von epaethanol und bestrahlung auf die berlebensfraktion unterschiedlicher zelllinien ht - 29 , t98g und u251 , bei zugabe von epa ( a ) 30 min oder ( b ) 24 h vor der bestrahlung . 
500 zellen / 25 cm2 kulturflasche ( * p < 0 , 05 ; * * p < 0 , 003 )  . with ionizing radiation of 2 gy , the plating efficiency of u251 cells was greater than that of ht - 29 cells , but during higher epaalbumin when combined with irradiation , 30 - minute incubation with epaalbumin was found to result in enhanced radiosensitivity with substantial variation ( figure 5a )  . 
no radiosensitization was found in any of the cell lines if epaalbumin was administered 24 hours before irradiation ( fiure 5b )  . discussion the aim of this study was to investigate whether supplementation of the omega - 3 polyunsaturated fatty acid epa during radiotherapy can influence the radiosensitivity of human tumor cells . 
several studies have demonstrated that supplementation with epa results in growth inhibition of various human tumor cells , including cervical cancer [ 32 ] , pancreatic cancer [ 25 , 45 ] , and breast cancer [ 46 ]  . 
lipo is assumed to be the initial step for cell death after n - 3 pufa treatment , but the exact mechanism for the subsequently observed cytotoxic effect is not fully established yet . 
 for reduction of the growth rate of ht - 29 cells in the presence of epa , an increased detachment of adherent cells has been discussed [ 18 ]  . 
the reason for the cells different epa sensitivities could be explained by the existence of a cell type - specific apoptosis - inducing property of epa [ 17 ]  . 
as in many cancer cells , the tumor suppressor protein p53 is deleted in ht - 29 and t98g cells , which were shown to be clearly more sensitive to epa in our study than p53 - wt u251 cells . 
another possible reason for different cell responses to epa may be differences in antioxidant systems , which are known , for example , for the high cell sensitivity caused by low selenium - glutathione peroxidase levels [ 48 ]  . 
 due to the loss or diminished activity of 6and 5 - desaturases , tumor cell membranes have decreased pufa content [ 22 ] , the main points of attack for lipo [ 9 , 27 ]  . 
effect of epaalbumin and radiation on the surviving fraction of different cell lines ht - 29 , t98g , and u251 , when treated 30 minutes ( a ) or 24 hours ( b ) prior to irradiation . 
cells were seeded in standard medium 48 hours before irradiation ; 30 minutes ( a ) or 24 hours ( b ) before irradiation the medium was changed and cells were incubated in serum - free medium , without epa and bsa - supplemented ( ) or with epa , complexed to bsa ( )  . 
wirkung von epaalbumin und bestrahlung auf die berlebensfraktion unterschiedlicher zelllinien ht - 29 , t98g und u251 , bei zugabe von epa ( a ) 30 min oder ( b ) 24 h vor der bestrahlung . 
einsaat der zellen in standardmedium 48 h vor der bestrahlung ; 30 min ( a ) oder 24 h ( b ) vor der bestrahlung erfolgte ein mediumwechsel mit serumfreien medium ohne epa und bsa - zusatz ( ) bzw . 
such enrichment of pufas and shifting of fatty acid composition toward a higher degree of unsaturation enhances the membranes susceptibility to lipo [ 25 , 30 , 32 ]  . 
recent studies described a marked rise in the level of lipid peroxides generated by cells supplemented with increasing concentrations of epa , associated with a significant inhibition in cell growth and loss of cell viability [ 25 , 47 ]  . 
during epa treatment 24 hours prior to irradiation instead of 30 minutes prior to irradiation , the cells have time to store the excess of potentially damaging nonesterified fatty acids in a safer neutral lipid form , such as triacylglycerol , in lipid droplets [ 20 ]  . 
however , the exact cause for the different sensitivity of the cells is still unknown . in radiobiology the predominant view is that dna is the main target in irradiated cells . 
however , several studies have postulated that membranes are also critical targets for the action of ionizing radiation on cells [ 31 , 34 , 53 ] and that radiation - induced programmed cell death starts at the membrane level [ 28 , 43 ]  . 
primary intermediates of lipo , such as 9 - hydroxystearic acid , induce significant cell cycle arrest and apoptosis [ 1012 ] ; malondialdehyde ( mda ) is known to be genotoxic by reaction with nucleic acid bases , resulting in mdadna adducts [ 39 ] ; and isoprostanes readily form michael adducts with proteins and alter protein structures and functions [ 14 , 41 ]  . 
therefore , lipo caused by irradiation has extensive consequences for cells with changes in the structural order , fluidity , and permeability of membranes , for inhibition of mitochondrial respiration , and for the activity of enzymes associated with membranes , as well as for inhibition of synthesis of nucleic acids and proteins up to apoptosis . conclusion the results of this study demonstrate that the enrichment of pufas in cell membranes through epa supplementation can increase the extent of the lipo caused by radiation and consequently can elevate the radiosensitivity of different tumor cells . 
it is hypothesized that the uptake of an anti - cea antibody is directly related to the number of viable tumor cells and may be quantified by immuno - positron emission tomography ( immuno - pet )  . 
therefore , we evaluated a novel pretargeting system using tf2 , a humanized bispecific trivalent monoclonal antibody ( mab ) , directed against cea and the imp - 288 - peptide , a hapten for binding radiometals for imaging . 
the colorectal cancer cell lines ht29 , sw480 , and t84 with known varying cea expression were incubated ( 72 hours ) with 131i - tf2 or the tf2 - 111in - imp - 288 pretargeting systeparallel cultures were irradiated with 210 gy high - energy photons . 
 conclusions : this novel pretargeting system allows the quantitative analysis of cea - expressing colorectal cancer cells and represents a promising tool for evaluation of tumor cell viability after irradiation . 
 key words : bispecific antibody colorectal cancer carcinoembryonic antigen irradiation pretargeting strahlenther onkol 2011 ; 187 : 1206 doi 10.1007 / s00066 - 010 - 2191 - 5 neues carcinoembryonales - antigen - ( cea - ) spezifisches pretargeting - system zur bestimmung der tumorzellviabilitt nach bestrahlung kolorektaler karzinomzellen hintergrund : derzeit gibt es beim cea - exprimierenden rektumkarzinom ( der uicc - stadien ii und iii ) keine valide diagnostik zur frhzeitigen response - beurteilung auf eine neoadjuvante radiochemotherapie . 
allerdings wird vermutet , da mit einer immuno - positronen - emissions - tomographie ( immuno - pet ) und einem anti - cea - antikrper die anzahl viabler tumorzellen nach erfolgter radiatio quantifizierbar ist . 
dieses pretargeting - system besteht aus dem humanisierten bispezifischen trivalenten monoklonalen antikrper ( tf2 ) , der an cea sowie an das radioaktiv markierte hapten - peptid imp - 288 bindet . 
wir untersuchten in vitro die bindung und kinetik dieses pretargeting - systems vor und nach radiatio . 1department of nuclear medicine , university medical center , georg - august - university gttingen , gttingen germany , 2department of radiotherapy and radiation oncology , university medical center , georg - august - university gttingen , gttingen germany , 3department of radiology and nuclear medicine , university of lbeck , lbeck , germany , 4department of clinical pharmacology , university medical center , georg - august - university gttingen , gttingen , germany , 5department of nuclear medicine , martin - luther - university halle , halle , germany , 6department of radiotherapy , university of lbeck , lbeck , germany , 7department of general surgery , university medical center , georg - august - university gttingen , gttingen , germany . received : june 28 , 2010 ; accepted : november 11 , 2010 published online : january 24 , 2011 strahlenther onkol 2011 no . 
die inkubation ( 72 h ) der kolorektalen tumorzelllinien ht29 , sw480 und t84 mit unterschiedlicher cea - expression erfolgte mit 131i - tf2 und dem tf2 - 111in - imp - 288 - pretargeting - syste parallelkulturen wurden mit 210 gy hochenergetischer photonen bestrahlt . 
 ergebnisse : der tracer - uptake korrelierte sowohl mit der cea - expression als auch der zellzahl der jeweiligen zelllinie ( uptake / 106 zellen : 0 , 3% in ht29 , 1 , 5% in sw480 und 14% in t84 ; p < 0 , 001 )  . 
die radiatio erhhte dosisabhngig die spezifische aufnahme des pretargeting - systems ( 4fach in ht29 und t84 nach 10 gy ( 72 h ) , p < 0 , 001 )  . 
 schlussfolgerungen : das neue pretargeting - system erlaubt eine quantitative analyse der cea - expression kolorektaler tumorzellen und ist eine vielversprechende methode zur evaluation der tumorzellviabilitt nach radiatio . schlsselwrter : bispezifischer antikrper kolorektale karzinome carcinoembryonales antigen radiatio pretargeting introduction based on several trials of the german rectal cancer study group , preoperative 5 - fluorouracil ( 5 - fu ) - based radiochemotherapy ( rct ) is recommended for treatment of uicc stage ii and iii rectal cancer in germany [ 3234 , 38 , 42 , 43 ]  . 
from the clinical point of view , early detection of individual tumor response is mandatory for risk - adapted multimodal treatment in future trials [ 22 ]  . usually response to neoadjuvant rct is evaluated by contrast - enhanced computed tomography ( ct ) , magnetic resonance imaging ( mri ) , and endorectal ultrasound [ 4 , 11 , 16 , 18 , 23 , 36 ]  . 
other imaging methods like 18fdg ( [ 18f ] fluoro - 2 - deoxy - d - glucose ) positron emission tomography ( fdg - pet / ct ) seem to be useful in management of colorectal cancer [ 3 , 28 , 29 ]  . 
but in neoadjuvantly treated rectal cancer patients , the nonspecific glucose uptake caused by the tumor microenvironment itself or by rctinduced tumor cell damage followed by inflammatory processes are serious limitations for the use of fdg - pet / ct in response prediction [ 10 , 14 ]  . 
in this dilemma , immuno - pet offers an innovative imaging approach using direct targeting of biomarkers ( e.g. , carcinoembryonic antigen [ cea ] ; ceacam5 as surrogate markers for tumor cell viability ) before , during , and after multimodal treatment [ 9 , 17 , 19 , 20 , 27 , 41 , 45 ]  . cea is expressed on the tumor cell surface of more than 90% of colorectal cancers and has been a useful marker for cancer detection in molecular imaging for nearly 35 years [ 13 ]  . 
 the tumor - to - background ratio ( t / bg - r ) of directly radiolabeled anti - cea monoclonal antibodies ( mab ) is poor and most crucial for scintigraphic detection of cancer . 
in order to improve the t / bg - r , several cea - directed pretargeting systems using bispecific mab and a radiolabeled hapten - peptide have been described [ 8 . 
the isotope is attached to a small compound with rapid renal clearance from blood and tissues . tf2 , a novel humanized , recombinant bs - mab , assembles two fab fragments from a humanized anti - ceacam5 mab ( hmn - 14 , labetuzumab ) and a fab fragment of an anti - hsg ( histaminesuccinylglycine ) antibody into a unique tri - fab structure [ 37 ]  . 
this bs - mab has been paired with the haptenpeptide imp - 288 that contains two copies of the hapten histaminesuccinylglycine ( hsg ) to enhance local retention [ 24 ]  . 
in preclinical models t / bg - r of more than 40 - fold compared to directly labeled igg molecules have been described [ 15 , 37 ]  . within the interdisciplinary research unit kfo179 ( subject : biological basis of individual tumor response in patients with rectal cancer ) , sponsored by the german research foundation , we are preparing to use a tf2 pretargeting system with 68ga - labeled imp - 288 for immuno - pet / ct imaging in patients with uicc stage ii / iii rectal cancer before , during , and after preoperative rct . 
thus , in vitro studies using the colorectal cancer cell lines ht29 , sw480 , and t84 with known varying cea expression were performed to assess the following : what are the kinetics of tf2 and imp - 288 binding to colorectal cancer cell lines ? is the uptake of the bs - mab and imp - 288 related to cea expression ? does irradiation influence bs - mab uptake ? are changes in uptake associated with apoptosis or with changes in cea - rna expression ? materials and methods radiolabeling of tf2 and imp - 288 radiolabeling of 0.5 mg tf2 ( 10 mg / ml pbs , ibc pharmaceuticals , inc . , morris plains , nj , usa ) with 50 mbq sodium strahlenther onkol 2011 no . 
residual 111incl3 was removed by a c18 cartridge ( c18 sep - pak light waters , ireland )  . cell cultures all human cell lines used were obtained from the american type culture collection ( atcc ; manassas , va , usa ) and subcultured in 25 cm culture flasks and 7 ml cell culture medium according to their recommendations . 
the luminescence referenced against untreated cells was determined at 30 minutes , 2 hours , 4 hours , and 24 hours after assay start ( n = 6 )  . 
mittlerer uptake / 106 zellen von 131i - tf2 ( tf2 ) und des 111in - imp - 288 - tf2 - pretargeting - systems ( tf2 - imp288 )  . 
nach 4 h und nach 72 h war die aufnahme tf2 - 111in - imp - 288 - pretargeting - systems signifikant hher als die des direkt markierten antikrpers 131i - tf2 ( * * p < 0 , 05 )  . 
 reverse transcription to complementary dna was effected for 1 hour with 1 g total rna using superscript ii reverse transcriptase ( invitrogen , carlsbad , ca , usa ) and 20 units per sample recombinant rnase inhibitor ( usb , cleveland , oh , usa )  . 
primer sequences are given in table 1 . statistical analysis statistical analyses ( statistical analysis software : spss 15.0 for windows ) were performed using nonparametric tests ( wilcoxon , mannwhitney )  . 
 figures display the means and standard deviations as well as the statistical results of particular experiments . specific tracer uptake and influence on proliferation cell cultures received either 1 g / ml 131i - tf2 ( 100 kbq / ml ) or 1 g / ml 131i - tf2 and 50 g / ml cold antibody . 
 to determine the influence of 131i - tf2 and tf2 on proliferation , control cultures were supplemented either with 200 l phosphate buffered saline ( pbs ) or with excess ( 50 g / ml ) cold antibody . cell cultures received 20 ng / ml 111in - imp - 288 ( 70 kbq / ml ) or 20 ng / ml figure 2 . 
parallel cultures were preincubated for 24 hours with 1 g / ml cold tf2 prior to 111in - imp - 288 application ( n = 9 each interval )  . 
to determine the influence of imp - 288 on proliferation , the medium of control cultures was supplemented with 200 l pbs or with 20 ng / ml cold imp - 288 . 
 die werte der cea - expression wurden zustzlich auf die expression der housekeeping - gene ( gapdh , hprt1 , ubc ) bezogen . 2 gy 4 gy 10 gy 24 hours 48 hours 75 72 hours 96 131i - tf2 and 111in - imp - 288 uptake at each time , the uptake of 131i - tf2 was specific and significant ( p < 0.01 ) in t84 and ht29 cells . 
incubation with 10 - fold excess of cold imp - 288 had no influence on the binding of 111in - imp - 288 . the kinetics of the 131i - tf2 and tf2 - 111in - imp - 288 , respectively , pretargeting systems are shown in figure 1 . 
uptake of the pretargeted 111in - imp - 288 measured at 4 hours remained relatively fixed over 72 hours in the sw480 and ht29 cells , while it increased in the t84 cells at 24 hours , but thereafter , uptake of the 131itf2 and tf2 - 111in - imp - 288 remained at a more elevated level ( 14% )  . 
cell proliferation and viability was not affected by unlabeled or radiolabeled tf2 or imp - 288 . irradiation compared to sham - irradiated cells the specific uptake of tf2 - 111in - imp - 288 in sw480 cells increased slightly after irradiation . 
eine signifikante zunahme der apoptose wurde bei sw480 - zellen 48 h nach bestrahlung mit 4 gy nachgewiesen ( n = 6 , * p < 0 , 05 )  . 
in t84 cells , there were slightly elevated cea expression levels detectable after irradiation with 10 gy ( table 2 )  . apoptosis only sw480 cells showed a significant increase in apoptosis ( p < 0.05 ) occurring 48 hours after irradiation with 4 gy ( figure 3 )  . 
compared to sham - irradiated cancer cells , there was no elevated apoptosis in ht29 and t84 cells after irradiation . discussion in this study , we demonstrated a novel 131i - tf2 - 111in - imp - 288 pretargeting system for semiquantitative evaluation of tumor cell viability after irradiation . 
in this simple and one - dimensional 131i - tf2111in - imp - 288 pretargeting system model , therapy - induced changes of cea expression or binding affinity may not be considered . irradiation increased the specific uptake of the pretargeting system compared to shame - irradiated cells within the first few days in a dose dependent manner , up to 4 - fold after a single dose of 10 gy and 72 hours . 
our findings are consistent with data describing an enhanced uptake of different radiopharmaceuticals induced by irradiation of different solid tumors [ 7 , 12 , 26 , 44 ]  . patients in our planned clinical trial will be treated according to the cao / aio / aro - 04 protocol [ 21 , 39 ]  . 
immuno - pet / ct will be performed pretherapeutically ( pet / ct1 ) within the third week of rct ( pet / ct2 ) and immediately prior to resection of the rectal specimen ( pet / ct3 )  . 
however , we suggest that cea - mediated uptake on pet / ct within the third week of therapy should not be dominated by an early increase of the uptake of the pretargeting systecea is a glycoprotein made by the cell and expressed on the cell surface . 
in addition metabolic downsizing of the primary tumor and metastatic spread should be quantitatively recorded within this approach . conclusions our in vitro testing showed that the novel 131i - tf2 - 111inimp - 288 pretargeting system specifically binds to cea - expressing colorectal cancer cells without cytotoxic side effects . 
 the uptake of the radioimmunoconjugate can be used for semiquantitative evaluation of tumor cell viability , especially after neoadjuvant radiochemotherapy . acknowledgments this work was supported by the german research foundation ( dfg ) as a part of the clinical research group 179 ( kfo179 : biological basis of individual tumor response in patients with rectal cancer )  . 
goldenberg , chien - hsing chang , william mcbride , and edmund a rossi ( immunomedics , inc . , and ibc pharmaceuticals , inc . , usa ) for providing the antibody and peptide . 
 strahlentherapie und onkologie original article new approach for treatment of vertebral metastases using intensity - modulated radiotherapy * toshihiko inoue , ryoong - jin oh , hiroya shiomi1 purpose : to perform aggressive radiotherapy for vertebral metastases . 
using very steep dose gradients from intensity - modulated radiotherapy ( imrt ) , a protocol based on the concept of partial volume dose to the spinal cord was evaluated . patients and methods : 50 patients with vertebral metastases were treated using imrt . 
in previously unirradiated cases , where a prescribed dose of 80 gy ( bed10 ) was delivered , the constraint to the spinal cord should be less than 100 gy ( bed2 )  . 
for previously irradiated cases , on the other hand , the dose is the same as in the previously unirradiated case ; however , constraints for the spinal cord are a cumulative bed2 of less than 150 gy , bed2 of less than 100 gy in each instance , and a treatment gap of more than 6 months . 
they all received higher bed2 , ranging from 51157 gy of d1cc . results : among the 24 patients who survived longer than 1 year , there was 1 case of transient radiation myelitis . 
there were no other cases of spinal cord sequelae . conclusions : based on the present results , we recommend a bed2 of 100 gy or less at d1cc as a constraint for the spinal cord in previously unirradiated cases , and a cumulative bed2 of 150 gy or less at d1cc in previously irradiated cases , when the interval was not shorter than 6 months and the bed2 for each session was 100 gy or less . 
the prescribed bed10 of 80 gy could be safely delivered to the vertebral lesions . key words : radiotherapy intensity - modulated radiotherapy partial volume dose of spinal cord vertebral metastasis strahlenther onkol 2011 ; 187 : 10813 doi 10.1007 / s00066 - 010 - 2187 - 1 neue methode fr die behandlung von vertebralen metastasen mit intensittsmodulierter strahlentherapie hintergrund und ziel : aggressive strahlentherapie bei vertebralen metastasen . 
unter einsatz sehr steiler dosisgradienten intensittsmodulierter strahlentherapie ( imrt ) evaluierung eines therapieprotokolls basierend auf dem konzept der partiellen volumendosierung am rckenmark . patienten und methodik : wir behandelten mit imrt 50 patienten mit wirbelsulenmetastasen . 
in fllen mit vorheriger strahlentherapie wurde die gleiche dosis appliziert , wobei allerdings die belastung des rckenmarks kumulativ unter 150 gy bed2 und in der einzelapplikation bei weniger als 100 gy bed2 lag , auerdem die behandlungspause mehr als 6 monate betrug . 
 alle erhielten die hhere bed2 von mehr als 51 gy bis zu 157 gy d1cc . ergebnisse : unter 24 patienten , die lnger als ein jahr berlebten , gab es einen fall vorbergehender strahlenmyelitis . 
es wurden keine weiteren flle von bestrahlungsfolgen am rckenmark beobachtet . schlussfolgerung : auf basis der vorliegenden ergebnissen wrden wir eine bed2 von 100 gy oder weniger bei d1cc am rckenmark in fllen ohne vorangegangene strahlentherapie empfehlen und in fllen mit vorheriger strahlentherapie eine kumulative bed2 von 150 gy oder weniger bei d1cc , wenn das behandlungsintervall nicht krzer als 6 monate war und die dosis der einzelapplikation bei einer bed2 von 100 gy oder weniger lag . 
die verordnete dosis einer bed10 von 80 gy bei wirbelsulenlsionen lie sich sicher applizieren . schlsselwrter : strahlentherapie intensittsmodulierte strahlentherapie partielle volumendosierung am rckenmark vertebrale metastase * this paper was presented at the 15th workshop of germanjapanese radiological affiliation in tokyo , japan , on 23 may 2010 . 1 miyakojima igrt clinic , osaka , japan . received : june 18 , 2010 ; accepted : november 11 , 2010 published online : january 21 , 2011 strahlenther onkol 2011 no . 
according to the japanese structure survey of radiation oncology in 2007 , out of 205 , 087 cancer patients ( new + repeat ) treated with radiation in 721 japanese institutes , 27 , 970 ( 13.6% ) patients underwent radiotherapy for bone metastases [ 6 ]  . during the past 3 decades , results obtained from the clinical trials of the radiation therapy oncology group ( rtog ) have been a golden standard of radiotherapy for painful osseous metastases [ 20 ]  . 
is it possible to retreat previously irradiated lesions ? is it possible to use more aggressive treatment ? nowadays , there are more innovative treatment methods and fine diagnostic tools for osseous metastases [ 7 , 10 ]  . 
in this paper , we verify a new treatment protocol of aggressive intensity - modulated radiotherapy ( imrt ) for vertebral metastases with special reference of partial volume doses of the spinal cord . patients and methods between april 2007 and december 2009 , 50 patients with vertebral metastases were treated using imrt or intensitymodulated radiosurgery ( imrs )  . 
of the 78 lesions , 40 ( 51% ) were located in tissues adjacent to that which had been previously irradiated , and 20 of these 40 lesions were true in - field recurrences . 
twenty of 38 lesions developed as initial vertebral metastases , while the remaining 23 lesions developed as second or third vertebral metastases , but were located separately from the previously irradiated vertebral column . 
movement minimization was achieved using vac - lok cushions and hipfix thermoplastics ( civco , usa ) ; in addition , the exactrac x - ray positioning system and 6 - axis robotic couch for fine localization ( brainlab ag , germany ) were used . the median prescribed dose was 40 gy ( range , 1667.5 gy ) , the median fraction dose was 6 gy ( range , 2.820 gy ) , and the median fraction number was 5 ( range , 120 )  . the following imrt protocol for vertebral metastases was used . 
in previously unirradiated cases , when a prescribed dose of 80 gy of the biologically effective dose of / = 10 ( bed10 ) was delivered , the constraint for the spinal cord should be less than 100 gy of the biologically effective dose of / = 2 ( bed2 )  . 
in previously irradiated cases , the prescribed dose is the same as in previously unirradiated cases ; however , the constraints for the spinal cord are a cumulative bed2 of less than 150 gy , bed2 of less than 100 gy in each session , and a treatment gap of more than 6 months . the radiotherapy treatment planning for all the patients in the present study was performed on the basis of ct and mri results . 
the fusion of mri and ct images was achieved by means of iplan rt image 4.1.1 ( iplan rt dose 4.1.2 , since august 2010 ) and treatment planning was made using brainscan 5.31 ( brainlab ag germany )  . in this series , 24 of 50 patients were followed for more than 1 year . 
bei applikation einer bed10 von 80 gy ( eqd2 = 67 gy ) an der wirbelsule ( a ) , kann bei einsatz der imrt - technik wegen des steilen dosisabfalls von 95% auf 65% innerhalb von 2 mm eine bed2 von 100 gy ( eqd2 = 50 gy ) am rckenmark angewendet werden ( b )  . when a curative bed10 of 80 gy , or biologically equivalent dose in 2 gy fractions ( eqd2 ) of 67 gy , was delivered to the spinal column with imrt using the novalis unit , the spinal cord is protected due to a rapid dose fall - off from the 95% to the 65% level within only 2 maccordingly , the dose to the spinal cord was restricted to a bed2 of 100 gy ( eqd2 of 50 gy ) ( figure 1 )  . 
sites of relapse received the dose of 32.4 gy / 12 fractions , 40 gy / 5 fractions , 25 gy / 5 fractions , and 30 gy / 3 fractions with imrt , respectively . an osteolytic vertebral lesion was successfully treated with locally curative imrt as in the following . 
tumor regression was observed 4 months later , while recalcification of the right transverse process and right 7th rib were recognized 8 months and 14 months later , respectively ( figure 2 )  . 
he is still doing well at the 22 - month follow - up . partial volume dose of the spinal cord indicated that all of these patients received very high doses ( table 2 )  . 
patient 5 had had a history of radiotherapy of 40 gy / 20 fractions / 28 days 31 months before ; he underwent a second treatment for a recurrent 2nd cervical vertebral lesion with a locally curative dose of 45 gy / 10 fractions / 16 days . 
a bed10 of 88 gy ( eqd2 of 72 gy ) was delivered to the 7th cervical vertebra , but the d1cc of the spinal cord was only 51 gy ( bed2 ) due to the rapid dose fall - off using imrt ( figure 3 )  . 
she has not developed any side effects of the spinal cord during the 15 - month follow - up . patient 6 received imrt at the 7th cervical vertebra and developed transient radiation myelitis 16 months later . 
she developed hypesthesia in both arms 16 months later ; she also reported weakness of the left 5th finger , and abnormal heat sensation in the right half of her body 19 months later . 
 however , symptoms improved after 23 months without any treatment , and no particular side effects were detected in the spinal cord after 26 months ( figure 4 )  . 
nearly 70% use a standard dose fractionation to palliate localized painful metastasis by radiotherapy , independent of the site of involvement or tumor type [ 3 ]  . a single dose or fractionated half - body irradiation has been applied for widespread metastatic bone lesions [ 17 , 19 , 21 ]  . 
89strontium is also applicable for pain relief for widespread metastatic bone lesions [ 12 , 14 ]  . when more intensive treatment ( surgery , high - precision radiotherapy ) were not available , dose escalation beyond 30 gy in 10 fractions did not improve motor function , local control , or survival in metastatic spinal cord compression patients with oloigometastatic disease ( no visceral or other bone metastases , involvement of only 13 vertebrae ) from relatively radioresistant tumors ( e.g. , renal cell carcinoma , colorectal cancer , malignant melanoma ) [ 5 ]  . 
concerning metastatic spinal cord compression ( mscc ) in colorectal cancer patients , no significant difference was observed between short - course and long - course radiotherapy with respect to functional outcome . 
according to degro ( german society of radiation oncology ) practice guidelines , different therapeutic goals ( e.g. , pain relief , local tumor control , prevention of motor deficits , and stabilization of the spine or other bones ) require complex approaches considering individual factors ( i.e. , life expectancy and tumor progression at other sites )  . 
as far as oligometastases , the treatment goal of the vertebral column is not only pain relief but also stability of the metastatic vertebral lesion . the spinal cord is the oar in curative radiotherapy for the vertebral column . 
 [ 15 ] stated the tolerance dose of the spinal cord to be 50 gy / 25 fractions / 5 weeks for minimal injurious dose ( td5 / 5 ) and less than 60 gy / 30 fractions / 6 weeks for maximal injurious dose ( td50 / 5 ) using 16 mev supervoltage therapy . 
they concluded that the risk of radiation myelopathy appeared small after cumulated bed2 of 135.5 gy , when the interval was not shorter than 6 months and the dose of each course was bed2 of 98 gy or less . 
patient 6 received imrt ( bed10 = 72 gy ; eqd2 = 60 gy ) at the 7th cervical vertebra and developed transient radiation myelitis 16 months later ( c )  . 
nach 26 monaten hatten sich die symptome gebessert , und das rckenmark blieb frei von nebenwirkungen ( e )  . in this study , the median prescribed dose was 40 gy ( range , 1667.5 gy ) , the median fraction dose was 6 gy ( range , 2.820 gy ) , and the median fraction number was 5 ( range , 120 )  . 
the following dose schedules of 30 gy / 3 fractions , 40 gy / 4 fractions , 45 gy / 5 fractions , 50 gy / 10 fractions , and 60 gy / 10 fractions were applied for 4 cases , respectively . during the past 10 years , diagnostic tools , such as petct and diffusion mri , have also progressed rapidly . 
 [ 8 ] reported in 2010 that there is a lack of data for advanced precision radiotherapy of imrt for the vertebral column ; therefore , up - to - date information is necessary to establish the new tolerance dose level for the spinal cord . 
the relatively small number of vertebral metastases in this report treated with imrt is , thus , an important contribution of the new technology for aggressive treatment in the future . imrt can deliver a near - uniform dose to the target volume . 
the spinal cord is protected due to a rapid dose fall - off from 95% to 65% within only 2 maccordingly , we can restrict the dose to the spinal cord to a bed2 of 100 gy ( eqd2 of 50 gy )  . 
nowadays , we are faced with the new situation of late damage to the spinal cord . imrt is also challenging with respect to treatment planning for advanced vertebral lesions or local recurrences after previous moderate - dose palliative treatment . 
we also indicated the successful dose fall - off from 95% to 65% within only 2 mm using the novalis imrt hollow - out technique . based on our present data , it is likely that the partial volume dose of case 6 is estimated as an upper limit of spinal tolerance . 
in previously irradiated cases , we propose a cumulative bed2 of 150 gy or less at d1cc when the interval was not shorter than 6 months and the dose of each session was a bed2 of 100 gy or less . 
in this situation , we can also deliver the prescribed curative dose of 80 gy ( bed10 ) to the vertebral lesion . conclusion the spinal cord is a typical oar . 
in spite of the relatively small number of patients and nonuniform dose schedules , the present conclusion drawn from aggressive treatment for vertebral metastases is reasonable using the analysis of partial dose volume to the spinal cord . 
in this study , only 24 patients were followed for 12 months or longer ; however , the present data do not lose their importance in establishing the tolerance dose level to the spinal cord when using modern imrt technology . based on the present results , a bed2 of 100 gy or less at d1cc is proposed as a constraint for the spinal cord in previously unirradiated cases , and a cumulative bed2 of 150 gy or less at d1cc in previously irradiated cases , when the interval was not shorter than 6 months and the dose of each session was 100 gy or less ( bed2 )  . 
results of a randomized phase - iii trial to evaluate the efficacy of strontium - 89 adjuvant to local field external beam irradiation in the management of endocrine resistant metastatic prostate cancer . 
 2003 ; 95 : 2229 . strahlentherapie und onkologie case study gorhamstout syndrome of the pelvic girdle treated by radiation therapy a case report reinhard heyd1 , daniela rabeneck1 , 2 , oliver drnenburg3 , nikolaos tselis1 , nikolaos zamboglou1 background : the gorhamstout syndrome ( gss ) is a rare , benign idiopathic and progressive disorder causing massive osteolysis due to a vascular hyperproliferation replacing the bony structure . 
imaging studies revealed no progression of the osteolysis but only minimal signs of remineralization . conclusions : combined treatment with rt and bisphosphonate administration can prevent the progression of osteolysis in gss . 
 total doses of 4045 gy are recommended . key words : radiation therapy gorhamstout syndrome bone tumors benign disease strahlenther onkol 2011 ; 187 : 1403 doi 10.1007 / s00066 - 010 - 2174 - 6 strahlenbehandlung des gorham - stout - syndroms des beckengrtels : ein einzelfallbericht hintergrund : das gorham - stout - syndrom ( gss ) ist eine seltene , idiopathische und progressive erkrankung , bei der durch eine vaskulre hyperproliferation massive osteolysen entstehen . 
die erfahrungswerte ber die effektivitt der strahlentherapie beschrnken sich auf etwa 50 von weltweit 200 publizierten fllen . einzelfallbericht : eine 24 - jhrige bettlgerige patientin mit histologisch gesichertem gss , das zu einer massiven zerstrung des vorderen beckengrtels gefhrt hatte , erhielt eine strahlentherapie mit einer gesamtdosis von 45 , 0 gy , appliziert in fnf wchentlichen fraktionen von 1 , 8 gy . 
 bildgebende untersuchungen zeigten keine progression der osteolysen , jedoch nur minimale zeichen einer remineralisierung . schlussfolgerungen : die kombination von externer strahlentherapie und intravenser bisphosphonatgabe erwies sich als effektiv zur prvention einer progression der osteolysen beim gss . 
gesamtdosen von 40 bis 45 gy werden empfohlen . schlsselwrter strahlentherapie gorham - stout - syndrom knochentumoren gutartige erkrankungen 1strahlenklinik , klinikum offenbach , offenbach am main , germany , 2klinik fr strahlentherapie und onkologie , klinikum der j.w. 
goethe universitt frankfurt am main , frankfurt am main , germany , 3institut fr diagnostische und interventionelle radiologie , klinikum offenbach , offenbach am main , germany . received : may 3 , 2010 ; accepted : september 16 , 2010 published online : january 18 , 2011 strahlenther onkol 2011 no . 
we present a case successfully treated by the combination of rt and intravenously administered zoledronic acid . case report a 24 - year - old woman presented with severe pain of the anterior pelvis which radiated to both femurs . 
prior multiple ct - guided biopsies had been performed , and only the last biopsy produced histological evidence of gss . on clinical examination , a slight swelling of both femurs and painful limitation in the range of motion of the hips were noted . 
plain radiographs , ct scans , and mri of the pelvis demonstrated extensive destruction of the anterior pelvic girdle ( figure 1 )  . after ct - based treatment planning , a total dose of 45.0 gy given in 5 weekly fractions of 1.8 gy was applied using isocentric parallel opposing treatment portals . 
in addition to rt , intravenous administration of 4 mg zoledronic acid was applied and continued in 4 - week intervals and continued to the present . heyd r , et al . 
rt for gorhamstout syndrome introduction the gorhamstout syndrome ( gss ) ( synonyms include massive osteolysis , vanishing bone , disappearing bone , or phantom bone ) was first presented in 1838 by john barnard swett jackson [ 20 ]  . 
in 1955 , gorham and stout summarized the histological characteristics of the disease in 24 cases that were known at the time and re - examined the pathologic specimens of 8 cases , thus , becoming eponymous for the disease [ 11 ]  . today , nearly 200 cases of gss have been reported ; however no reliable epidemiological data are available [ 2 , 5 , 22 , 27 ]  . 
in advanced stages , the disease may spread within a few months to contiguous bones and may extend to adjacent soft tissue in more than 70% of cases [ 5 , 8 , 22 ]  . 
most affected sites are the skull ( particularly the mandible ) the shoulder , and the pelvic girdle [ 2 , 5 , 7 , 22 , 26 , 27 ]  . 
pelvic bones and proximal femurs are involved in approximately 12.9% of cases [ 22 ]  . gss is mostly apparent in children , adolescents , and young adults , while symptom onset is commonly observed in the second or third decade of life [ 2 , 5 , 15 , 26 , 27 ]  . 
there is no racial or gender predilection [ 2 , 14 , 15 , 27 ] , but some investigators reported an increased incidence in males [ 8 ]  . 
the prognosis is usually favorable , and the overall mortality is estimated to be 13% , increasing to over 30% in central lesions affecting the axial skeleton and involving visceral organs [ 5 , 8 , 26 ]  . histological findings demonstrate an increase of abnormal proliferation of thin - walled , endothelial - lined vessels of vascular or lymphatic origin which can simulate the appearance of hemangioendotheliomas , lymphangiomas , or hemangiomas [ 3 , 11 , 21 , 26 , 27 ]  . the leading clinical symptoms are weakness , pain , and instability or even fracture of the involved bones resulting in functional deficits [ 8 , 14 , 15 , 27 ]  . 
in up to 17% of the cases , the occlusion of the thoracic duct may cause a chylothorax or thoracic deformity resulting in a life - threatening respiratory condition [ 21 , 27 ]  . clinical observations suggest that a spontaneous arrest of the pathologic findings and also radiological disappearance is possible ; thus , conservative treatment is only indicated in rapidly progressive cases [ 6 , 14 , 27 ]  . 
numerous therapeutic approaches have been proposed , including surgical procedures , radiation therapy , embolization , bone graft , and several medications ( e.g. , bisphosphonates , - interferon - 2b , androgens , calcium , corticosteroids , calcitonin , vitamin d , and cytotoxic drugs ) , but so far a general treatment strategy has not been defined [ 2 , 8 , 10 , 21 , 22 , 27 , 29 ]  . recently , numerous reports on the efficacy of radiation therapy ( rt ) in gss each including a small number of pafigure 1 . 
basic research revealed an elevation of the serum levels of humeral factors , such as interleukin 1 and 6 ( il - 1 , il - 6 ) , and tumor necrosis factor alpha ( tnf - ) , which play a key role in stimulation of osteoclast precursor sensitivity and osteoclast activity [ 7 ]  . 
therefore , it is suggested that vascular hyperproliferation is rather a result than the cause of the disease . the diagnosis of gss is often delayed and usually made by excluding other disorders in combination with clinical data , radiological signs , and histological findings [ 5 ]  . 
ct scans are essential to plan the surgical procedures , and they provide precise information concerning the extent of the bony destruction and soft tissue involvement , but do not estimate the vascularity of the lesions . 
the t1 - weighted sequences typically show low signal intensity , increasing after gadolinium contrast application due to an inflammatory reaction and the increased capillary permeability of the vascular channels . 
 the t2 - weighted sequences often demonstrate mixed signal intensity with partial signal elevation due to hypervascularity [ 5 , 8 , 27 ]  . the differential diagnosis of gss includes other osteolystic disorders , such as hereditary osteolysis , acroosteolysis , and progressive osteolysis in progeria . 
in the early stages of the disease , when only isolated osteolyses are apparent , it must be distinguished from aneurysmatic bone cysts , other benign or malignant bone tumors , vascular malformations , or even soft tissue tumors causing bone arrosions [ 14 , 27 ]  . treatment of gss is only required in progressive cases when clinically relevant deformity , functional deficits , or other complication arise . 
however , the functional benefit of surgical procedures remains uncertabone graft has not been proven effective because the implanted bone material is absorbed within a few weeks [ 10 , 27 ]  . 
options for management of chylothorax include interferon , thoracic duct ligation , pleurectomy , pleurodesis with bleomycin , and rt [ 21 , 26 ]  . rt is known to be effective in a large variety of degenerative and hyperproliferative benign conditions affecting the skeletal system [ 1 , 4 , 9 , 1618 ] , but knowledge of the value of rt in gss is limited to several case reports and studies including a small number of patients . 
total doses in the range of 4045 gy are recommended as having the potency to arrest the progression of the bony lesions [ 8 , 24 ] , whereas lower doses of figure 2 . 
konventionelles bersichtsbild des beckens ein jahr nach abschluss der rt , das keine krankheitsprogression und diskrete zeichen einer remineralisierung zeigt . at the end of rt , the patient responded with marked pain relief , and after supportive remedial physical therapy for 5 weeks the patient was able to sit on the edge of the bed without any support . 
the kps was improved to 50% , and the ecog score was 2 . at the 3 - month follow - up , the patient had almost complete relief of pain and was able to walk short distances with the aid of crutches . 
plain radiographs and ct scans demonstrated stable disease without any progression of the osteolysis , while the mri revealed a slight increase of contrast enhancement . complete pain relief was noted 1 year after completion of rt , and the patient was able to walk short distances without the use of crutches ( kps = 90% , ecog score = 0 )  . 
the intravenous administration of zoledronic acid and also the remedial physical therapy will be continued to achieve further clinical improvement . discussion gss is a rare proliferative disorder with unknown etiology and pathophysiology . 
it is characterized by spontaneous , idiopathic , and progressive bone resorption not accompanied by new bone production [ 5 , 7 , 22 , 26 , 27 ]  . 
based on our observations , we can confirm other data that significant remineralization is unusual [ 8 ] , with signs being detected by imaging studies as late as 89 months [ 3 , 8 ]  . 
 [ 22 ] observed moderate disease progression over a period of 17 years in a patient treated with a combination of rt and long - term administration of altering bisphosphonates . 
however , the precise impact in the treatment of gss combined with rt or as sole treatment option remains unknown . ct - based three - dimensional rt planning is recommended for a precise target volume definition , as all affected bones and adjacent soft tissues have to be treated [ 3 , 8 ]  . 
handl - zeller and hohenberg [ 13 ] recommend early rt initiation in order to prevent the spreading of the disease and to reduce the extent of the target volume . 
so far , radiogenic induction of neoplasms has not been reported in the literature . conclusions gss is a rare musculoskeletal disorder of unknown origin and unpredictable prognosis , and no accepted treatment standard . 
total doses of 4045 gy are recommended , but remineralization is rarely detectable . strahlentherapie und onkologie original article outcome after re - irradiation of head and neck cancer patients nele platteaux , piet dirix , bianca vanstraelen , sandra nuyts1 purpose : to retrospectively report the outcome of head and neck cancer patients following re - irradiation . patients and methods : a total of 51 patients with recurrent or second primary head and neck cancer received re - irradiation at leuven university hospital . 
re - irradiation of head and neck cancer introduction despite improved tumor control and survival following radiation treatment for head and neck cancer ( hnc ) , through the use of intensified fractionation schedules and the addition of concomitant chemotherapy , locoregional recurrences remain frequent [ 3 , 33 , 35 , 36 , 39 , 47 ]  . 
moreover , chronic exposure of the upper aerodigestive tract to alcohol and tobacco , the most common risk factors of hnc , is thought to produce field cancerization , a process in which patients are at risk for developing cancer at different mucosal sites . 
 as most recurrences occur in the first 2 years after primary treatment and 80% arise in previously high - dose irradiated volumes , it is obvious that the management of these recurrences is a challenging clinical problem [ 4 , 6 ]  . 
the preference in operable patients is salvage surgery with 5 - year survival rates ranging from 1636% [ 2 , 9 , 20 , 34 , 40 , 49 ]  . 
moreover , only 20% of patients will be able to undergo salvage surgery because of the extent of the disease , medical contraindications , or patient refusal [ 20 , 22 , 49 ]  . 
obviously , the risk of morbidity is also higher as a result of radiation - induced tissue changes which complicate healing . in previously irradiated patients with unresectable recurrent hnc , the standard of care used to be palliative chemotherapy , associated with median survival of 59 months and with response rates of between 10 and 40% [ 11 , 12 , 20 , 54 ]  . 
re - irradiation can be delivered using brachytherapy , stereotactic radiosurgery , or external beam radiotherapy with or without chemotherapy and with or without debulking surgery upfront [ 19 ]  . 
it is to be expected that the use of more conformal techniques , such as intensity modulated ration therapy ( imrt ) , will improve outcome and decrease toxicity of reirradiation in the head and neck region . therefore , we report the outcome of high - dose re - irradiation in hnc patients with the majority of patients treated with three - dimensional ( 3d ) conformal planning techniques or imrt . materials and methods patient characteristics from 20002009 , 51 patients with recurrent ( n = 37 ) or second primary ( n = 14 ) hnc received re - irradiation at the university hospitals leuven . 
a total of 46 patients ( 90.2% ) were re - irradiated with curative intent , while 5 patients ( 9.8% ) were treated with palliative intent due to low performance status which made them unfit to undergo a radiation treatment ( rt ) of several weeks . 
the patient characteristics are shown in table 1 . from the completion of their initial rt , the mean time to retreatment was 60.5 months ( range , 3324 months )  . 
a complete history , clinical examination , and computer tomography ( ct ) scan of the head and neck region were completed in all patients at the time of re - irradiation . 
pretreatment workup generally included screening for distant metastases with a chest x - ray , ultrasound of the abdomen , complete blood chemistry , and further imaging , if indicated . treatment radiation the majority of the patients ( n = 48 , 94.1% ) were re - irradiated using 3d conformal techniques , including 10 patients with imrt . 
while 3 patients ( 5.9% ) were re - irradiated using conventional 2d radiation techniques , 1 patient was re - irradiated using external beam rt combined with brachytherapy and another was re - irradiated using rt combined with radiosurgery . 
 patients were immobilized with a thermoplastic 5 - point head and neck mask . gross tumor volumes ( gtv ) were outlined and expanded manually by 1.5 cm ( range , 0.52 ) to form planning target volumes . 
the median volumes of clinical ( ctv ) and planning ( ptv ) target volumes of recurrence were 63.3 ( range , 1.85230.8 ) cm and 127.2 ( range , 25429.1 ) cm , respectively . 
beam arrangements and field shapes were designed using 3d beams eye view ( bev ) display targets and normal structures , to avoid re - irradiation of critical normal structures such as the spinal cord and brainstem , while adequately treating the head - and - neck ptv within the 95% isodose . 
due to disease progression and patient refusal ( after 44 and 68 gy , respectively ) , 2 patients ( 3.9% ) did not complete their prescribed re - irradiation course . 
the majority of patients were treated with a 2 - gy fraction ( n = 32 ) , 11 with 1.8 gy per fraction , 1 with combined 2 and 1.8 gy per fraction , strahlenther onkol 2011 no . 
chemotherapy regimens at the time of re - irradiation contained either cisplatin ( n = 11 ) , cisplatin5 - fluoro - uracil ( n = 2 ) , carboplatin5 - fluorouracil ( n = 1 ) , carboplatin ( n = 1 ) or docetaxelcisplatin - 5 - fluorouracil ( n = 1 )  . 
eleven of these 14 patients had microscopic ( n = 8 ) or macroscopic ( n = 3 ) residual disease following surgery , whereas 3 patients had negative surgical margins . surgery toxicity acute radiation - related toxicities were classified according to the common toxicity criteria ( ctc ) system version 3.0. 
late radiation - related toxicities were classified according to the radiation therapy oncology group ( rtog ) / eortc morbidity scoring systelate toxicity was assessed every 3 months starting 6 months after end of retreatment during the first 2 years [ 56 ]  . 
 statistical analysis follow - up was measured from the last day of re - irradiation to the day of death or to the last clinic visit before this analysis ( july 2009 )  . 
the overall ( os ) , disease - free ( dfs ) , diseasespecific survival ( dss ) , distant control ( dc ) , and locoregional control ( lrc ) were estimated according to the kaplanmeier method . 
evaluating failure after re - irradiation , locoregional failure occurred in 13 ( 39.4% ) , local failure in 8 ( 24.2% ) , locoregional and distant metastasis in 9 ( 27.3% ) , local and distant metastasis in 2 ( 6.0% ) , and isolated distant failure in 1 ( 3.0% ) patients , respectively . 
distant metastasis are reported in the lungs in 5 , the bones in 2 , the skin in 5 , mediastinal ( 1 ) and axillary ( 2 ) lymph nodes in 3 , soft tissues , the liver , and the spleen in 1 patient each . survival the actuarial estimate of overall survival ( os ) was 30% at 2 years ( figure 2 )  . 
gesamtberleben , krankheitsfreies und krankheitsspezifisches berleben fr alle patienten . a total of 34 patients ( 66.7% ) died during follow - up after a median of 7.6 months ( range , 0.972.2 months ) : 31 patients ( 93.9% ) died due to disease and 3 patients ( 8.8% ) died of another cause . 
the actuarial diseasefree survival ( dfs ) rate was 27.5% at 2 years ( figure 2 )  . toxicity acute and late toxicity was assessed retrospectively by documenting all symptoms recorded during and following re - irradiation ( table 2 )  . 
surgery before re - irradiation was also significantly associated with improved dfs ( figure 3 ) and showed a trend for improved lrc and dss ( table 3 )  . 
re - irradiation of head and neck cancer and rt technique were not predictive for lrc , os , dfs , or dss . discussion the results of this study demonstrate that re - irradiation is a feasible option in previously irradiated hnc patients . 
it should be noted that 5 - year survival rates range from as low as 13% in unselected patients to as high as 93% in selected patients [ 20 ]  . 
long - term survival after re - irradiation ranged between 13 and 20% , while local or regional control ranged from 1333% [ 10 , 14 , 37 , 46 ]  . 
 our results are similar to previous studies showing overall survival rates of 50% , 30% , and 22.5% at 1 , 2 , and 5 years , respectively ( table 4 )  . 
our results show , however , no better results in dfs and lrc in re - irradiation of recurrent laryngeal and nasopharyngeal cancer than other tumor sites [ 7 , 27 , 51 , 52 ]  . 
 this is in contrast with the literature where the majority of patients re - irradiated at the larynx were treated with surgery first or had early stage laryngeal recurrences [ 7 , 51 ]  . 
furthermore , in cases where intracerebral pathology following previous irradiation needed to be classified either as tumor relapse or radiation - induced tissue changes . introduction with increasing incidence , brain metastases represent the most common intracranial tumors and are associated with very poor prognosis in most cases . 
however , this aspect might be important in cases with newly diagnosed , histologically unclassified cerebral lesion ( s ) lacking information about the primary tumor , and also with local tumor recurrences after previous irradiation of the neurocranium , where it can be important to differentiate between tumor relapse and radiationinduced necrosis . furthermore , one major limitation of srs is tumor size . 
 treatment of metastases exceeding a diameter of 3 cm or a volume of 14 cm3 increases the radiation burden to the surrounding tissue and may increase the risk of edema and / or radiation - induced tissue necrosis [ 12 , 24 , 25 , 31 ]  . for these selected cases , stereotactic ( interstitial ) brachytherapy ( sbt ) using 125iodine seeds has been reported to represent a feasible and minimally invasive treatment option initially described in 1989 [ 21 ]  . 
as salvage treatment , these authors implanted high activity 125iodine seeds for 46 days in 14 patients with progressive brain metastases following standard therapy and reported survival times of 20 months . 
in 1995 , the value of this treatment strategy was confirmed for singular cerebral metastases , with fair overall survival of up to 17 months and low procedural risk of 2% transient morbidity [ 17 ]  . 
these authors also emphasized the possibility of performing a stereotactic biopsy and sbt ( then called interstitial radiosurgery ) within the same operation . with the present retrospective single - center study , our results on sbt using 125iodine seeds to treat singular cerebral metastases are reported , and for the first time these are compared with an equivalent patient population treated with linac - based srs . patients and methods patient selection our institutions apply both treatment modalities linacbased srs and sbt by stereotactic implantation of 125iodine seeds . 
therefore , over time we developed the following selection criteria for sbt ( figure 1 ) : unclassified histology : need for stereotactic biopsy in cases of first diagnosis of an intracerebral lesion together with figure 1 . 
stereotactic brachytherapy for cerebral metastases tumor size : metastasis exceeding a diameter of > 3 cm or volume of > 14 cm3 , wbrt treatment , in cases of local recurrence after previous srs and / or the patient is not a candidate for microsurgical tumor removal due to eloquent and / or deep - seated location of the metastasis with only moderate mass effect , or patient refusal to undergo surgery . for the present evaluation , all patients with de novo , untreated singular cerebral metastases receiving sbt after 125iodine seed implantation were selected and were compared with our follow - up data of 142 patients with the same diagnosis who underwent linac - based srs . 
 patients with a karnofsky performance status ( kps ) [ 7 ] < 60 and / or poor estimated survival ( < 3 months ) due to uncontrollable systemic disease ( progression ) were excluded from this treatment protocol . the patients medical history , histology of the original tumor , neurological symptoms , complications , and need for steroid medication were evaluated . 
acute toxicities were identified as events arising within 90 days of starting sbt / srs and late toxicities as events that occurred thereafter . assessment of local tumor response on magnetic resonance imaging ( mri ) scans used the macdonald criteria [ 11 ]  . 
 the definition of complete remission , however , had to be modified for patients receiving sbt due to the frequently observed residual traces of contrast enhancement surrounding the implanted seeds resulting from treatment - induced local bloodbrain barrier disruption . local relapse was defined as a new enhancing lesion appearing in exactly the same site as the treated metastasis after complete response , or through histological confirmation by stereotactic biopsy after ( re ) growth of a previous partial response , or stable disease . the mri treatment response was documented along with clinical data in 3 - month intervals until the patients death or last contact . 
patients with stable extracerebral disease and progressive neurological dysfunction ; severe neurological disability dying from intercurrent illness ; and progressive systemic and neurological disease were considered as neurological deaths ; otherwise systemic death was assumed . treatment planning , irradiation , and surgical procedures sbt was mainly performed under general anesthesia , whereas srs patients received local anesthesia for head fixation using a modified riechertmundinger stereotactic frame . 
for both procedures , an intraoperative ct scan was fused with preoperative axial t1and t2 - weighted mri images and the target volume was outlined using specialized software ( stp3 ; until 2 / 1996 with stp2 , leibinger gmbh , freiburg , germany )  . for sbt , 125iodine seeds were implanted . 
the prescribed cumulative dose ( referring to the surface of the target ) was 50 gy with an irradiation time of 42 days , resulting in an initial dose rate of 0.1 cgy / mdetails of the stereotactic procedure for implantation were recently published [ 3 , 8 , 10 ]  . for srs , a linear accelerator ( sl25 , elekta , 6 mev photon beams ) equipped with tertiary changeable collimators with 330 mm diameter openings and a non - coplanar rotational scheme ( 610 arcs ranging from 20160 to 200340 ) was used [ 9 , 13 , 29 , 31 ]  . 
the prescribed surface doses ranged from 1822 gy ; the corresponding isodose levels from 5080% . for both groups , wbrt was only applied in case of recurrent cerebral disease . statistical analysis and outcome measures the end of the observation period was march 2009 . 
endpoints of the analysis were patient death irrespective of the cause , date of last patient contact , and date of occurrence of local or distant tumor relapse on mri . 
epidemiological and disease related features of both groups were equal , with the exception of lower kps and larger tumor volume in the sbt group ( table 1 )  . in 58 of 77 cases ( 75.3% ) , the necessity for a stereotactic biopsy was the criteria for offering sbt . 
kaplan - meier - berlebenskurven der patienten , die mittels stereotaktischer jod - 125 - brachytherapie ( sbt ) im vergleich zu srs ( linac ) an singulren hirnmetastasen behandelt wurden . 
46.4% ( figures 3a and 3b ; table 2 )  . mri examinations of 101 patients ( 71.1% ) in the srs group and 65 ( 72.2% ) in the sbt group were available for the interim evaluation of the radiographic treatment response at the first follow - up 3 months after srs and 4.5 months after initiation of sbt ( 42 days treatment time + 3 months ) ( table 2 )  . type and frequency of salvage therapies for local or distant recurrences did not differ significantly between the srs and sbt treated patients ( table 2 )  . 
 overall , no patient of either treatment group needed steroid medication for more than 3 weeks , and no patient required microsurgical intervention for radiation - induced space occupying changes . 
 [ 17 ] this positive outcome also applies for 17 patients with large metastases , which due to their tumor size ( diameters > 34 cm ) were not eligible for srs according to our treatment standards . 
the higher tolerability of sbt compared to srs might be attributed to the following radiobiological differences : ( 1 ) sbt ionizing radiation is distributed from the center of the tumor to its periphery . 
in contrast , srs is performed with much higher dose rates ( 1501000 cgy / minute ) as a single treatment often within less than 1 hour . our evaluated sbt population represents a typical population of patients with singular cerebral metastases regarding age , gender , distribution of histology , and rtog classes . 
the sbt treatment plan ( b ) shows two seed catheters ( red and green trajectory ) as well as the outlined tumor surface ( blue dotted line ) , and the 50 gy and 200 gy isodose lines ( yellow and red )  . 
die stereotaktisch gefhrte biopsie zeigte eine karzinommetastase , so dass in gleicher operation die sbt durchgefhrt wurde ( 50 gy kumulative oberflchendosis appliziert fr 42 tage , verwendung von jod - 125 - seeds )  . 
der sbtbestrahlungsplan ( b ) zeigt zwei seed - katheter ( rote und grne trajektorie ) , die eingezeichnete tumoroberflche ( blaue , gestrichelte linie ) sowie die 50 - gybzw . 
mri ( t1and t2 - weighted ) of a 61 - year - old man performed for staging of tumor status after being newly diagnosed with nsclc ( a ) revealed a singular cerebral metastasis . 
die mrt - sequenzen ( t1und t2 - gewichtet ) eines 61 jahre alten mannes , die im rahmen einer statuserhebung bei neu diagnostiziertem nsclc ( a ) durchgefhrt wurden , zeigen eine singulre metastase . 
 the distant and local cerebral disease control rates 1 year after srs treatment were reported to be 6482% and 7397% , respectively , [ 2 , 1416 , 20 , 22 , 30 ] , which also concur with our sbt results . 
this also supports our opinion about the efficacy of sbt for the treatment of singular cerebral metastases in selected cases . conclusion sbt using 125iodine seeds represents a minimally invasive , safe , and feasible method for local treatment of de novo , untreated singular cerebral metastases , allowing histological diagnosis with high accuracy , and treatment within one stereotactic procedure . 
 compared with microsurgical treatment , sbt has fewer restrictions regarding tumor localization ( eloquent / deep - seated brain structures ) and spares the patient additional wbrt by better local disease control . 
stereotactic brachytherapy for cerebral metastases strahlentherapie und onkologie original article celecoxib enhances radiation response of secondary bone tumors of a human non - small cell lung cancer via antiangiogenesis in vivo frank michael klenke1 , amir abdollahi2 , 3 , marc bischof2 , martha - maria gebhard4 , volker ewerbeck5 , peter e . 
somit reprsentiert die kombination von strahlentherapiemiteinercox - 2 - inhibitoneinenvielversprechendenansatz , umdietherapeutischeeffektivittderbestrahlungvon knochenmetastasenzuverbessern . schlsselwrter : angiogenese knochentumor cyclooxygenase intravitalmikroskopie strahlentherapie introduction radiotherapy is the standard treatment to achieve local control of bone metastases . 
as the response rate of tumors to radiation seems to be dependent on the delivered dose , strategies increasing the effective dose of radiation may be crucial to ameliorate the therapeutic efficacy of radiotherapy [ 16 , 22 , 25 , 27 , 45 , 50 ]  . 
recent strategies to optimize the efficacy of radiation are focused on molecular targets enhancing the radiation sensitivity of malignant tumors [ 1 , 2 , 4 , 11 , 13 , 15 , 28 , 31 , 36 , 37 , 40 , 53 ]  . 
in this respect , the prostaglandin signaling pathway seems to be of particular importance as it has been shown that the modulation of prostaglandin synthesis can ameliorate the response of tumors to radiation [ 30 , 35 , 37 , 40 ]  . cyclooxygenase ( cox ) with its two isoforms cox - 1 and cox - 2 is the rate limiting enzyme for the synthesis of prostaglandins from free arachidonic acids . 
elevated levels of cox - 2 in tumor cells are associated with resistance to apoptosis [ 23 , 48 ] , tumor angiogenesis [ 51 ] , and tumor cell invasiveness [ 8 , 9 , 49 ]  . 
it has been shown that the inhibition of cox - 2 mediates antitumor activities in various human malignant tissues including prostate , colorectal , breast , and non - small cell lung cancer [ 3 , 14 , 24 , 34 , 41 , 42 , 44 ]  . 
in a previous study , it was shown that the selective cox - 2 inhibitor celecoxib significantly reduced growth of secondary bone tumors of a non - small cell lung carcinoma . 
the antitumor effect was mediated by antiangiogenic and proapoptotic mechanisms in bone metastases [ 20 ]  . although cox - 2 inhibitors were shown to inhibit tumor growth if administered as monotherapeutic agents , several authors provided evidence that the drugs are considerably more effective if combined with a second treatment regimen . 
in this regard , selective cox - 2 inhibitors were recently reported to enhance the response of primary tumors to radiation in vitro and in vivo [ 30 , 32 , 33 , 35 , 37 , 40 , 52 ]  . 
the effects of the combined application of celecoxib and radiation were investigated by applying an animal model of bone metastases and intravital microscopy to continuously monitor angiogenesis , vascularization , and growth of secondary bone tumors . material and methods animal model and cell lines experiments were performed on 24 adult male severe combined immunodeficient mice ( scid , c.b - 17 / icrcrl - scid - br , charles river laboratories inc . , sulzfeld , germany , 78 weeks old , 2025 g body weight ) , following institutional guidelines approved by the local animal review board . 
all surgical procedures were performed in strictly aseptic conditions within a laminar flow unit ( merck eurolab , bruchsal , germany ) under deep anesthesia by an intraperitoneal injection of a mixture of ketamine ( ketanest , 65 mg / kg body weight , pfizer , karlsruhe , germany ) , xylazine ( rompun , 13 mg / kg body weight , bayer , leverkusen , germany ) , and acepromazine ( sedastress , 2 mg / kg body weight , medistar , holzwickede , germany )  . the human lung carcinoma cell line a 549 was obtained from the german cancer research institute ( heidelberg , germany )  . 
injection of 30 mg / kg body weight celecoxib ( celecoxib , n = 6 ) or the equivalent amount of the ( cmc ) - based vehicle alone ( control , n = 6 )  . 
animals that received radiation on day 15 were either treated with the vehicle ( radiation , n = 6 ) or with celecoxib ( celecoxib + radiation , n = 6 ) under the conditions described above . 
treatments started on day 8 after tumor implantation and were continued until termination of experiments on day 28 after tumor implantation . intravital microscopy within the first week after tumor implantation , mice were observed daily under epi - illumination with a stereotactic microscope ( leica mz75 , leica , germany ) employing a 5to 40 - fold magnification . 
 intravital fluorescence videomicroscopy was performed using an epi - illumination fluorescence microscope unit ( leica , germany ) equipped with a 4 ( ef 4 / 0.12 , leitz , wetzlar , germany ) and 40x ( zeiss achroplan 40 / 0.75 w , carl zeiss , germany ) objective on days 7 , 14 , 21 , and 28 after tumor implantation . 
fvd was quantified using a computer - based image analysis program ( capimage , engineering office zeintl , heidelberg , germany )  . histopathologic assessment all mice were sacrificed on day 28 after tumor implantation and the tumors were immediately excised along with the surrounding tissue of the calvaria and the brain for further histopathologic investigation . 
however , the 2d tumor size significantly increased until day 28 after tumor implantation as compared to day 7 ( prior to initiation of celecoxib / vehicle treatment ) figure 1 . 
the graph depicts the two - dimensional tumor surface ( mm2 ) of the tumors with different treatments on days 7 , 14 , 21 , and 28 after tumor implantation . 
furthermore , the combination of celecoxib and radiation induced a growth arrest of the tumors after the delivery of irradiation . angiogenesis and tumor vascularization first , newly formed vessels were observed within 6 days after tumor implantation in all tumors followed by a rapid onset of perfusion in these vessels within another 24 hours . 
intravital microscopy showed that the angiogenic sprouting originated from vessels located within the surrounding bone . as shown in figure 2 , functional vessel density significantly increased between days 7 and 14 in all treatment groups . 
 ( a ) the graph depicts the functional vessel densities ( fvd ) of the tumors with different treatments on days 7 , 14 , 21 , and 28 after tumor implantation . 
 ( a ) die grafik zeigt die funktionelle gefdichte ( fvd in mm / mm2 ) der tumoren whrend unterschiedlicher behandlungen an den tagen 7 , 14 , 21 und 28 nach tumorimplantation . 
direct comparison of celecoxib + radiation with the monotherapy regimes showed that the combination of radiation with celecoxib was superior to both monotherapies in terms of the ability to reduce the final functional vessel density on day 28 after tumor implantation . 
die tumoren , die entweder mit celecoxib ( b ) oder der bestrahlung ( c ) behandelt wurden , waren in ihrer gre hnlich , aber insgesamt deutlich kleiner als die unbehandelten tumoren . 
die tumoren , die sowohl mit der bestrahlung als auch mit celecoxib behandelt wurden ( d ) , waren am tag 28 nach tumorimplantation insgesamt betrachtet die kleinsten . histology discussion representative h&e stained tissue sections of the control group and the experimental groups are shown in figure 3 . 
 in accordance with in vivo findings , the volume of untreated secondary lung carcinomas increased significantly compared to the small pieces ( volume 0.51.0 mm ) that were initially implanted ( figure 3a )  . 
consistent with the in vivo findings , the combination of celecoxib and radiation showed markedly smaller tumor volumes as compared to the monotherapies with celecoxib or radiation alone . consistent with previous findings , radiation as well as celecoxib showed distinct antivascular properties in the present study [ 3 , 7 , 14 , 17 , 24 , 26 , 34 , 38 , 39 , 41 , 42 , 47 , 49 , 55 ]  . 
the decrease in functional vessel density and the inhibition of tumor growth proceeded simultaneously indicating that the antitumor effects of radiotherapy and celecoxib treatment can be attributed at least in part to antiangiogenic mechanisms . 
enhanced radiation response by celecoxib in secondary bone tumors implantation , which may explain why radiotherapy alone did not effectively stop tumor growth . based on findings that the modulation of prostaglandin synthesis can ameliorate the response of malignant primary tumors to radiation [ 30 , 35 , 37 , 40 ] , we hypothesized that combining radiation with cox - 2 inhibition may increase the radioresponse of secondary bone tumors . 
previous studies showed that the continuous administration of different cox2 inhibitors prior to single beam radiation of human tumor xenografts demonstrated to potentate the tumor response to radiation in vivo , while the normal tissue was not sensitized to radiation [ 18 , 30 , 33 ]  . 
the radioprotective capacity of cox - 2 has been further supported by the finding that radiation dose - dependently induced the expression of cox - 2 in pc - 3 tumor cells in vitro [ 43 ]  . the present study demonstrated that , in contrast to the monotherapies with either radiation or celecoxib , the combination of both regimes was capable to halt tumor progression effectively within the observation time period . 
 in comparison to the reduction of tumor size and functional vessel density achieved with radiotherapy only , treatment with radiation and celecoxib reduced tumor vascularization and tumor size by another 57% and 51% , respectively . 
these results are consistent with the enhanced inhibition of capillary sprouting from rat aortic rings by combined administration of radiation and the cox - 2 inhibitor rofecoxib [ 7 ]  . 
the inhibition of these survival factors with celecoxib enhanced the vascular damage induced by radiation in vivo as demonstrated by increased microvessel permeability of the vasculature of col26 murine colon cancer . 
 together the data add to the growing rationale of combining radiotherapy of tumors with specific signaling inhibitors including pdgf and vegf [ 29 , 46 ]  . although more experiments with additional tumor cell lines and different modalities of treatment , such as fractionated doses of radiation , should be performed to confirm the present data in a wider field , it is concluded that the simultaneous administration of celecoxib and radiation seems to be a rationale to enhance the therapeutic potential of local radiotherapy of bone metastases . 
due to the intrinsic antitumor properties of celecoxib , this regime offers the advantage to ameliorate the radioresponse of bone metastases locally and accomplish a systemic tumor therapy in nonirradiated regions concomitantly . acknowledgments this study was supported by a research grant ( f.02.0015 ) of the mwfk ba - wue ( ministry for science , research , and art of the state of badenwuerttemberg , germany ) to as . 
side effects were correlated with patient - , tumor - , and treatment - related parameters . results : overall , at least one episode of acute nausea occurred in 48% of the patients and at least one episode of vomiting occurred in 25% of patients . 
die nebenwirkungen wurden mit patienten - , tumorund therapiebezogenen parametern korreliert . ergebnisse : mindestens eine episode von belkeit trat bei 48% der patienten auf ; 25% hatten mindestens einmaliges erbrechen . 
die bestrahlungsregion , namentlich thorax ( p = 0 , 0110 ) und kopf / hals ( p = 0 , 0415 ) , konnte auch als risikofaktor besttigt werden . 
patientenbezogene parameter wie weibliches geschlecht ( p = 0 , 0003 ) und jngeres alter ( < 40 jahre ) ( p = 0 , 0029 ) sowie gewichtsabnahme von mehr als 5% ( p = 0 , 0004 ) und das vorliegen einer peg - sonde ( p = 0 , 0071 ) waren mit verstrkter belkeit und erbrechen verbunden , whrend alkoholabusus einen protektiven effekt zeigte ( p = 0 , 0553 )  . 
bei hoch emetogenen chemotherapie - protokollen war die prophylaxe mit der kombination aus 5 - ht3 - antagonist plus dexamethason einem 5 - ht3 - antagonisten allein berlegen ( p = 0 , 0383 )  . schlussfolgerung : knftige studien sollten effektivere prophylaxe - protokolle bei simultaner radiochemotherapie untersuchen , um die hohen raten an belkeit und erbrechen zu reduzieren . schlsselwrter : belkeit erbrechen radiochemotherapie nebenwirkungen antiemetika 1department of radiation oncology , j.w. 
goethe university , frankfurt / main , germany . received : july 22 , 2010 ; accepted : august 2 , 2010 published online : december 22 , 2010 strahlenther onkol 2011 no . 
nausea and emesis during chemoradiotherapy introduction nausea and emesis are major side effects of oncologic treatment , which weaken the physical condition , impair quality of life , and cause treatment modification or interruption , which occasionally has a negative impact on treatment outcome [ 3 , 23 ]  . 
for radiotherapy , where these acute reactions are considered to be less frequent and severe , the problem tends to be underestimated : according to a recent survey , one - third of patients with radiotherapy - induced nausea considered their antiemetic treatment insufficient [ 5 ]  . sex male female many studies have evaluated the incidence and severity as well as the prophylaxis and treatment of nausea and emesis caused by chemotherapy and although having received less attention by radiotherapy [ 8 , 9 , 12 ]  . 
for radiotherapy , the emetogenic risk is , apart from fractionation schedule and the irradiated volume ( e.g. , total body irradiation ) , mostly defined by the anatomic site of irradiation . 
treatment and patient - related risk profiles were elaborated and guidelines for prophylaxis and treatment could be established separately for both modalities [ 6 , 7 , 9 , 14 , 15 , 22 ]  . 
 ( for combined regimen , emesis prevention according to the chemotherapy - related risk level ( based on the drug with the highest emetic risk as well as patient specific risk factors ) is recommended [ 20 ] )  . 
 in this study , the prevalence of nausea and emesis and the impact of patientand treatment - related factors during crt with or without 5 - ht3 antagonist - based antiemetic prophylaxis were retrospectively evaluated . weight during crt no change ( 5% ) weight loss > 5% weight gain > 5% alcohol anamnesis 40 years 4160 years > 60 years peg patients and methods patient and tumor characteristics a total of 335 adult patients treated with standard crt protocols , in whom tumor stage ( n = 314 ) performance status ( who ) intravenous chemotherapy was administered in the inpatient setting and for whom acute side effects were sufficiently documented , were included in this retrospective study . 
the most frequent diagnoses were head and neck cancer ( 47% ) and rectal cancer ( 17% ) , followed by esophageal cancer ( 15% ) , cervical cancer ( 12% ) , anal cancer ( 7% ) , or other tumors ( 2% )  . 
most patients suffered from advanced tumor disease ( uicc stage iii or iv in 70% of cases )  . concurrent chemoradiotherapy three - dimensional ( 3d ) conformal rt was performed using either a 6 or 25 mv photon beam accelerator with individual field arrangement . 
the patients were treated with a median total dose of 52.4 gy ( range , 19.870.6 gy ) with daily fractions of 1.9 gy ( range , 1.82 gy ) ( icru report 50 )  . time ( n = 295 ) first chemotherapy cycle last chemotherapy cycle irradiation site pelvis thorax head and neck abdomen we evaluated 821 cycles of chemotherapy in 335 patients which were administered by intravenous infusion concomitantly to radiotherapy . 
as oral intake , which is a main parameter for the scoring of nausea , is often reduced in head and neck cancer patients by tumor and / or mucositis , the need of antiemetic drugs was also considered for scoring in these patients . 
 [ 10 ] , had a significant influence on nausea and emesis which was most pronounced between the highest and lowest level ( p < 0.001 ; table 2 )  . 
the emetogenic risk of radiotherapy , as established according to the site of irradiation , also showed an influence during crt : irradiation of the thorax was associated with the highest rates of grade 2 / 3 nausea emesis , which was also significant when compared with irradiation of the pelvis . 
antiemetic prophylaxis patients with high ( level iv / v ) emetogenic chemotherapy suffered significantly less from acute nausea when they received a combination of 5 - ht3 antagonist and dexamethasone for prophylaxis compared with 5 - ht3 antagonist alone . 
 discussion during crt almost half of the patients ( 48% ) had at least one episode of nausea and one - fourth ( 25% ) suffered from emesis , despite most patients having received an antiemetic prophylaxis based on the guideline recommendations at that time . 
in a study on head and neck cancer patients treated with intensity modulated radiation therapy , 65% of the 23 patients with concurrent chemotherapy suffered from nausea ( grade 1 : 35% ; grade 2 : 30% ) compared with 50% ( grade 1 ) of the 20 patients with radiotherapy alone [ 17 ]  . 
 [ 10 ] , which considers each agent in combined regimens , results in a more accurate gradation than considering only the most - emetic chemotherapy agent which is actually recommended [ 20 ]  . female gender and young age known as important patient - related risk factors for developing nausea and emesis during chemotherapy and during radiotherapy as well as the protective effect of alcohol abuse have also proven to be relevant factors for crt [ 12 , 19 ]  . 
abdomen as the site of irradiation , which is the most evaluated parameter for nausea and emesis in radiotherapy , was not confirmed , probably because this site was underrepresented ( 4% ) in our study . 
in the italian trial , the irradiated site , i.e. , upper abdomen and a field size > 400 cm2 , were the only radiotherapy - related risk factors for nausea and emesis [ 16 ]  . 
instead , irradiation of the thorax and head and neck , i.e. , in patients with esophagus or head and neck cancer , was associated with significant nausea and emesis . 
in the head and neck imrt trial already mentioned ( with nausea in 50% of the patients even during radiotherapy alone ) , the dose to the dorsal vagal complex of the mid - medulla and the use of a low neck field ( besides younger age ) were identified as significant factors for nausea [ 17 ]  . 
in our study , weight loss , as a potential consequence of these side effects , and the presence of a peg , which is used to prevent weight loss , was significantly associated with nausea and emesis during crt . 
it could be shown in former studies that weight loss during chemotherapy correlates with impaired tumor response , disease - free survival , and overall survival [ 25 ]  . 
thus , the importance of effective antiemetic prophylaxis in crt is evident , especially in predisposing conditions , such as cisplatin - based crt in younger women ( cervix cancer ) , in head and neck cancer patients , and in crt of the upper abdomen / lower thorax . all patients with high emetogenic chemotherapy had an antiemetic prophylaxis , more or less in line with the guidelines at that time [ 7 , 15 ]  . 
in this group , we could confirm the superiority of the combination of a 5 - ht3 antagonist with dexamethasone against a 5 - ht3 antagonist alone which is also the basis for more recent clinical recommendations [ 19 ]  . 
there were no differences between the efficacy of the 5 - ht3 antagonists used , namely ondansetron and granisetron , which are thought to have an equivalent effect at prescribed doses [ 15 ]  . 
in the italian trial , an antiemetic drug was given to a minority ( prophylactic in 12.4% , symptomatic in 4.6% ) , thus , confirming the radiation strahlenther onkol 2011 no . 
novel substances , such as the neurokinin - 1 receptor antagonist aprepitant , have been established as potent prophylactic antiemetics in chemotherapy [ 2 , 11 , 27 , 29 , ] but have not been evaluated in crt . 
only a few studies have focused on the prevention of nausea and emesis in crt : based on promising data in hyperthermo - chemo - radiotherapy for esophageal cancer [ 18 ] , the 5ht3 antagonist ramosetron was evaluated in crt for pancreaticobiliary cancer . 
in 10 patients who were refractory to prophylactic metoclopramide and rescue ondansetron , prophylactic ramosetron could reduce the symptoms in 60% ( 5 - fu 500 mg / m2 day 13 ; 40 gy ; split of 2 weeks ) [ 13 ]  . 
in a feasibility study , the prophylactic use of aprepitant ( plus 5ht3 plus dexamethasone ) resulted in a reduction of nausea and emesis when compared to historical controls ( 19 patients with pancreatic cancer , gemcitabine plus 5 - fu / capecitabine - based crt with 50.4 gy : grade 3 nausea and grade 4 vomiting in one patient ) [ 1 ]  . our study has several limitations , including those associated with collection of any retrospective data , especially when assessing subjective symptoms such as nausea and emesis . 
however , to the best of our knowledge , this is the only study investigating acute nausea and emesis with the use of different standard protocols of crt in clinical practice . 
 conclusion we conclude that , despite the use of 5 - ht3 antagonist plus dexamethasone - based prophylaxis in the majority of patients , acute nausea and emesis are still major adverse effects of crt affecting half of the patients . 
potent novel antiemetics which are already established as prevention of chemotherapy - induced nausea and emesis should also be evaluated for crt protocols . strahlentherapie und onkologie original article a randomized prospective study of rehabilitation therapy in the treatment of radiation - induced dysphagia and trismus y . 
peng1 purpose : to evaluate the therapeutic effect of rehabilitation therapy on radiation - induced dysphagia and trismus in nasopharyngeal carcinoma ( npc ) patients after radiotherapy . patients and methods : 43 npc patients after radiotherapy were included . 
the severity of dysphagia was assessed using the water swallow test , while trismus was evaluated with the lent / soma score and the interincisor distance ( iid )  . 
the water swallow test , the lent / soma score , as well as iid for both groups before and after treatment were analyzed and compared . results : after treatment , the rehabilitation group displayed a significant improvement in swallowing function , while the control group did not . 
der schweregrad der dysphagie wurde mit hilfe des wasserschlucktests bewertet , whrend der trismus durch den lent - soma score und den abstand der schneidezhne ( iid ) evaluiert wurde . 
der wasserschlucktest und der lent - soma score sowie der iid bei beiden gruppen wurde vor und nach behandlung analysiert und verglichen . ergebnisse : nach behandlung wies die rehabilitationsgruppe eine deutliche verbesserung der schluckfunktion im vergleich zur kontrollgruppe auf . 
rehabilitation of dysphagia and trismus fazit : rehabilitationstraining kann die schluckfunktion verbessern und verlangsamt die entwicklung des trismus von npcpatienten nach strahlentherapie . schlsselwrter : nasopharynxkarzinom strahlentherapie dysphagie trismus rehabilitationstraining introduction there is a high prevalence of nasopharyngeal carcinoma ( npc ) in south china , especially in guangdong province . 
radiotherapy has been proved to be effective for this disease ; however , there are many complications associated with radiotherapy [ 20 , 25 ] , including injury to cranial nerves or the brain stem [ 3 , 7 , 24 ]  . 
dysphagia may result in severe complications , such as aspiration pneumonia [ 16 , 19 ] , and permanent or long - term feeding tube dependence which significantly decrease patients quality of life [ 10 , 11 ]  . 
although rehabilitation exercises are generally believed to be effective , there are few prospective randomized studies concerning this issue , and arguments may be made that patients could recover their swallowing and mastication function over time without rehabilitation . 
the aim of this study is to determine if rehabilitation therapy provides effective therapeutic effect and quality of life advantages over standard care for dysphagia and trismus in npc patients after radiotherapy . patients and methods patient population and clinical data this project was approved by an authorized human research review board at our institute . 
patients included in this trial were inpatients and outpatients of sun yat - sen memorial hospital of sun yat - sen university and the cancer center of sun yat - sen university from november 2006 to november 2007 . 
patients with cancer relapse , metastases , other malignances , neurovascular disease , demyelinating disease , infection of the nervous system , or any oral and temporomandibular joint diseases were excluded from the study . 
the rehabilitation group received rehabilitation training guided by therapists during hospitalization and continued the rehabilitation exercises after being discharged from the hospital , while the control group did not perform any rehabilitation exercises . 
 no significant difference in age , gender , radiation dosage , or the status of dysphagia or trismus was present before treatment between the two groups . rehabilitation training maneuvers and regimen exercises for dysphagia tongue exercises range of motion exercises included ( 1 ) passive movement exercises , where the therapist or assistant holds a patients tongue with gauze and pulled it gently in different directions for exercises , and ( 2 ) active movement exercises , where the patient protrudes and then retracts the tongue , licks both sides of cheeks , licks lips , and rolls the tongue up to the soft palate . 
 resistance exercises required that a patient uses a scoop or spatula to give resistance to the tongue . pharynx and larynx exercises therapeutic postures and exercises consisted of a patient changing body position to maximize the swallow function and minimize aspiration under the guidance of a therapist . 
sensory procedures utilizing pharyngeal cold stimulation were performed by therapists or assistants , who gently stimulated a patients soft palate , tongue base , and pharyngeal wall with a swab dipped in ice water followed by asking the patient to swallow . exercise for trismus range of motion exercises for the temporomandibular jaw active jaw movement exercises included ( 1 ) patients opening and closing mouth repeatedly , ( 2 ) patients opening the mouth slightly , and then slowly moving the lower mandible to the left and later to the right , ( 3 ) the patient stretched his / her chin downward and forward then back to the original position like a moving bail . 
rehabilitation of dysphagia and trismus the mouth by hand ( i.e. , the maxillary and mandibular jaws were separated by a patients own hands wrapped with gauze ) and ( 2 ) using therabite to assist jaw motion , ( i.e. , an appropriately sized therabite was placed into the mouth to help open the mouth and move the jaw )  . rehabilitation exercise regimen in the rehabilitation group , the rehabilitation training exercises were performed 3 times per day . 
 ( 1 ) a guideline booklet describing the exact exercise regimen , number of cycles , and daily schedule in detail was distributed to each patient to make sure that patients and their family clearly understood the rehabilitation exercises . 
if a patient missed more than 15% of all days , the patient was excluded . functional assessment of dysphagia and trismus the swallow function was evaluated before and after treatment for both groups . 
the water swallow test was used to assess each patients swallow function and effect of rehabilitation [ 17 ] as follows : patients were asked to drink 30 ml tepid water . 
a score of 2 was given to patients who could finish drinking at one time , but required more than 5 seconds ; the patient needed to drink twice , but without coughing or a pause . 
the effect of treatment was interpreted as being deteriorated ( negative ) , ineffective , effective , and excellent when n was < 0 , 0 , 1 and > 1 , respectively . 
the efficacy rate was the percentage of patients with excellent and effective effects . low dry food , with an iid of 1.12.0 cm ; grade 3 , difficulty to swallow a soft diet , with an iid of 0.51.0 cm ; grade 4 , iid less than 0.5 cm and being dependent on a feeding tube . 
compared with the pretreatment iid , if the posttreatment iid increased , remained at the pretreatment value , narrowed but was more than 50% of pretreatment iid , or narrowed and was less than 50% of pretreatment iid , the therapeutic effect was interpreted to be excellent , effective , ineffective , and deteriorated , respectively . 
the efficacy rate was the percentage of patients with excellent and effective effect . out patients follow - up all patients received follow - up after they were discharged from the hospital as outpatients . 
 the iid was classified as one of four levels according to the lent / soma score [ 5 ] : grade 1 , trismus with an iid of 2.13.0 cm ; grade 2 , difficulty to swaltable 1 . 
wirksamkeit der trainingsmanahmen auf die dysphagie . rehabilitation group control group n0n1 > 1 excellent n0n1 = 1 effective n0n1 = 0 ineffective n0n1 < 0 deteriorated total 0.02 strahlenther onkol 2011 no . 
 pretreatment posttreatment discussion patients with head and neck cancer often develop dysphagia after chemoradiation and postoperative radiation due to injury to the brain stem or the lower cranial nerves [ 2 , 13 , 20 ]  . 
although investigators have reported that normal - tissue radioprotection could be achieved by gene therapy [ 22 ] , only a few therapeutic strategies have proved to be effective for these sequelae . 
the exercises and management of dysphagia include pharyngeal or cervical esophageal dilation , dietary modifications , postural strategies , swallowing maneuvers , such as the super - supraglottic swallow and the mendelsohn maneuver , and therapeutic exercises that target strength and range of motion for lips , tongue , and larynx [ 8 , 9 , 21 ]  . 
nguyen and colleagues [ 15 ] displayed that swallowing therapy is effective in improving dysphagia severity and reduces the need for tube feedings in cancer - free patients who developed aspiration following chemoradiation and postoperative radiation for headand - neck cancer . 
so far , no prospective controlled studies have documented the efficacy of rehabilitation therapy on swallowing disorders and trismus in patients undergoing treatment for head - and - neck cancer . 
rehabilitation of dysphagia and trismus of rehabilitation therapy on dysphagia and trismus in patients with npc follo wing radiotherapy . the results showed that patients who received rehabilitation therapy had improved on swallow function . 
there are a number of instrumental methods for assessing swallow function , including modified barium swallow ( mbs ) fluoroscopic exam , flexible endoscopic evaluation of swallowing safety ( fees ) and the 30 ml water swallow test . 
in this study , we used the 30 ml water swallow test to assess the severity of dysphagia because it is more feasible to perform , especially when swallow function needs to be evaluated once every month for each patient during follow - up . 
as previously described in the literature , the severity of trismus varies based on the site of the tumor to be radiated ( e.g. , tumors such as nasopharyngeal , base of tongue , salivary gland , and cancers of the maxilla or mandible ) , the dose of radiation received ( dosage > 60 gy ) , and the patients radiosensitivity . 
the range of motion exercises for the jaw and tongue and the resistance exercises could strengthen musculature , increase mobility , and improve the flexibility and elasticity of the temporomandibular joint . 
the rehabilitation exercises adopted in this study are comprehensive and are relatively easy to perfor patients and family members could be trained in the hospital and continue to practice at home . to start rehabilitation exercises at an early stage is critical to prevent the progress of dysphagia and trismus . 
for patients suffering from severe dysphagia and with delayed swallow , thickening liquids is helpful since it may slow the rate of bolus flow through the pharynx , while for trismus patients , a pureed diet is favorable . 
huber1 , 2 , jrgen debus1 purpose : in this retrospective investigation , the outcome and toxicity after reirradiation with concurrent cetuximab immunotherapy of recurrent head and neck cancer ( hnc ) in patients who had contraindications to platinum - based chemotherapy were analyzed . material and methods : ten patients with locally advanced recurrent hnc were retrospectively evaluated . 
cetuximab was applied as loading dose ( 400 mg / m2 ) 1 week prior to reirradiation and then weekly concurrently with radiotherapy ( 250 mg / m2 )  . results : the median overall survival time after initiation of reirradiation was 7 months ; the 1 - year overall survival ( os ) rate was 40% . 
severe late toxicities were noted in 2 patients : fibrosis of the temporomandibular joint in 1 patient and stenosis of the cervical esophagus in another . conclusions : imrt reirradiation with concurrent cetuximab immunotherapy in recurrent hnc is feasible with acceptable acute toxicity . 
further investigations are necessary to determine the clinical role of this therapy concept . key words : recurrent head and neck cancer reirradiation cetuximab imrt toxicity strahlenther onkol 2011 ; 187 : 328 doi 10.1007 / s00066 - 010 - 2149 - 7 imrt - re - bestrahlung mit simultaner cetuximab - immuntherapie bei rezidivierten kopf - hals - tumoren ziel : in dieser untersuchung analysierten wir behandlungsergebnis und toxizitt nach kombinierter re - bestrahlung mit simultaner cetuximab - immuntherapie von rezidivierten hno - tumoren bei patienten mit kontraindikation gegen platinhaltige chemotherapie . patientengut und methode : 10 patienten mit lokal fortgeschrittenen rezidivierten hno - tumoren wurden retrospektiv ausgewertet . 
cetuximab wurde als loading dose ( 400 mg / m2 ) eine woche vor re - bestrahlung und danach wchentlich simultan zur bestrahlung ( 250 mg / m2 ) verabreicht . ergebnisse : das mediane gesamtberleben nach re - bestrahlung war 7 monate ; das 1 - jahres - gesamtberleben betrug 40% . 
es sind weitere untersuchungen ntig , um den stellenwert dieser therapieform zu berprfen . schlsselwrter : rezidivierte hno - tumoren re - bestrahlung cetuximab imrt toxizitt 1department of radiation oncology , university of heidelberg , heidelberg , germany , 2division of radiation oncology , dkfz , heidelberg , germany . received : march 25 , 2010 ; accepted : october 7 , 2010 published online : december 23 , 2010 strahlenther onkol 2011 no . 
imrt reirradiation with cetuximab in recurrent head and neck cancer introduction in advanced head and neck cancer ( hnc ) , the local failure rate after primary treatment with operation and adjuvant irradiation or definitive chemoradiotherapy is 3050% [ 1 , 10 , 20 , 28 , 31 , 34 ]  . 
in the situation of recurrent disease , salvage treatment is difficult because of advanced tumor stage and altered normal tissue structure due to previous multimodal treatment by surgery , radiotherapy , or chemoradiotherapy . 
however , often the recurrent tumor is not resectable due to poor performance status or tumor infiltration of critical structures , e.g. , skull base , arterial vessels , or the jaw . although monochemotherapy is another possibility , in general , it cannot achieve long - term local control as in most cases of solid tumors . 
the most effective systemic treatment for recurrent and / or metastatic head and neck cancer is cisplatin - based chemotherapy in combination with cetuximab leading to a median survival of 10 months [ 33 ]  . another option is reirradiation alone or with concurrent chemotherapy , which can archive long - time survival in up to 25% of patients [ 23 ]  . 
however , there are often contraindications for platinumbased concurrent chemotherapy because of reduced performance status , age , renal dysfunction , or cisplatinum resistance . another possibility is offered by new targeted drugs : bonner et al . 
in view of these results , it could be expected that concurrent cetuximab immunotherapy would also improve the outcome of reirradiation of recurrent hnc in patients with reduced performance status , if the use of any conventional chemotherapy is not possible . we report here our initial experience of recurrent hnc patients treated by imrt reirradiation with concurrent cetuximab immunotherapy . 
in particular , local control , overall survival , distant metastasis - free survival , and acute and late toxicity were investigated . methods and materials patients between 2004 and 2008 , reirradiation in 10 patients with histologically proven locally recurrent hnc , who had been previously treated with external beam radiotherapy , was performed . 
usually restaging consisted of ct and / or mri of the head and neck area , x - ray or ct of the chest , and ultrasound of the abdomen . 
reirradiation was defined as volumetric overlap of over 70% between the retreatment and initial target volumes . in all cases , the initial radiation treatment was documented adequately either by simulation films with corresponding treatment data in case of conventional techniques or threedimensional ( 3d ) - isodose arrangements and dosevolume histogram information in case of conventional 3d or imrt techniques . 
imrt reirradiation with cetuximab in recurrent head and neck cancer total of 5 patients received chemotherapy prior reirradiation including cisplatin , 5 - fluorouracil ( 5 - fu ) , or docetaxel . treatment patients were fixed in the supine position by individual scotchcast masks and whole - body vacuum pillows . 
the clinical target volume ( ctv ) included the gross tumor volume with a safety margin of 0.51 cno elective irradiation of uninvolved nodal regions was performed , except for 1 patient . 
the absolute median ptv was 182.5 cm3 ( range , 481320 cm3 )  . inverse treatment planning was performed using the konrad software developed at the german cancer research center ( dkfz ) , which is connected to the 3d planning program virtuos to calculate and visualize the 3d dose distribution ( see figure 1 )  . 
the imrt treatment planning process has been described in detail previously [ 18 , 24 ]  . the ptv coverage complied with the recommendations of the international commission for radiation units [ 13 ]  . 
however , if adequate target coverage could not be achieved without exceeding those limits , a violation was accepted in small areas at the surface , if the limits could be maintained assuming a 50% dose tolerance recovery from the initial treatment course . a stereotactic setup was used in all cases . 
imrt was carried out using a step - and - shoot technique ( 6 mv photons ) with a linear accelerator ( siemens , concord , ca , usa )  . 
a cetuximab loading dose ( 400 mg / m2 body surface area ) was administered 1 week before starting reirradiation , followed by weekly doses of 250 mg / m2 concurrent to radiotherapy up to 57 times . patients were followed up clinically in combination with ct or mri every 3 months . 
 the endpoints of this retrospective analysis were local control ( lc ) , locoregional control ( lrc ) , distant metastasis - free survival ( dmfs ) , and overall survival ( os )  . 
statistical analysis was performed with statistica ( version.6 , stat - soft , tulsa , ok , usa ) and sigmaplot ( version.10 , systat software )  . acute and late toxicity was graded according to rtog criteria [ 8 ]  . 
late toxicity without total loss of function but with severe impact on the patients quality of life , such as severe limitation of oral intake caused by fibrosis , strictures , or stiffness of the temporomandibular joint , was also considered as severe radiation - induced late toxicity . 
in order to describe the cetuximab - related acneiform rash , the following clinical grading system ( nci - ctc ) was used : no ( grade 0 ) , strahlenther onkol 2011 no . 
imrt reirradiation with cetuximab in recurrent head and neck cancer light ( grade 1 ) , moderate ( grade 2 ) and severe ( grade 3 ) acnelike skin reaction [ 4 , 25 ]  . distant metastases were found in 2 patients ( 20% ) and occurred primary in the lung and axilla . 
the 1 - year dmfs was , thus , 75% ( figures 25 )  . results six weeks after reirradiation , 4 patients show a tumor regression and 5 patients had no change of tumor size in mri . 
a flap necrosis ( grade 4 ) developed during the reirradiation course in 1 patient ; however , surgical revision could be postponed and radiation treatment was completed without a break . 
acute hematological toxicity was not seen in the group . late toxicity after the first radiation course , 2 patients suffered from xerostomia , while another experienced trismus with a mouth open width of 2.5 cafter the second radiation course , 50% of the patients suffered from xerostomia in general and 4 patients ( 40% ) showed enhanced xerostomia after reirradiation ( table 3 )  . 
another patient developed stenosis of the cervical esophagus with dysphagia . bleeding events one patient died of acute arterial bleeding 0.5 months after the end of reirradiation , which was considered an acute toxicity event . 
another patient suffered from tumor - related infield erosion bleeding 6 months after the end of reirradiation , which was controlled by compression therapy . discussion treatment of locally recurrent head and neck cancer after previous radiotherapy is challenging . 
complete surgical removal is an attractive option but is often limited due to tumor infiltration into vital structures , including the major vessels , nerves , or skull base [ 12 ]  . 
rtog / ctc - kriterien wurden angewandt . grade 1 grade 2 grade 3 grade 4 grade 5 acute toxicity mucositis erythema hematotox acneiform rash taste smell late toxicity hearing defect : right left xerostomia : before reirradiation after reirradiation trismus dysphagia improve progression - free survival [ 14 ]  . 
in this situation , the most effective systemic treatment is cisplatin - based chemotherapy in combination with cetuximab leading to a median survival of 10 months [ 33 ]  . by definition , these patients suffer from a localized recurrence of their disease , the preferable treatment should include an effective local treatment component . 
since radiotherapy is used as the major local treatment in primary hnc not amenable to surgery , there is increasing interest in reirradiation for nonresectable local recurrence in hnc patients . 
imrt reirradiation with cetuximab in recurrent head and neck cancer two phase ii trials using conventional 2d or 3d conformal radiation techniques were conducted by the rtog in order to investigate the value of reirradiation with concurrent chemotherapy in this setting [ 16 , 26 , 27 ]  . 
with these approaches , the investigators reported 2 - year os rates of 17% and 26% , respectively , and emphasized the importance of adding a local treatment modality . often patients with recurrent hnc show reduced performance status , which eliminates the possibility to apply any conventional chemotherapy . 
 [ 5 ] showed that concurrent cetuximab immunotherapy significantly increases local control rates and os in primary radiotherapy of advanced hnc compared with radiation alone . in our group of patients treated by imrt reirradiation with a median dose of 50 gy and concurrent cetuximab immunotherapy , the os was 7 months . 
all patients in our group were treated with the imrt technique , which has been demonstrated to have superior target coverage and improved sparing of organs at risk in many sites of the body , especially in the head and neck region [ 35 ]  . reports in the published literature on reirradiation using imrt are rare [ 3 , 6 , 21 ]  . 
 [ 30 ] reported 54 patients with definitive imrt reirradiation ( median dose , 66 gy ) and concurrent platinum - based chemotherapy resulting in a median os of 25 months and a 2 - year lcr of 64% . 
moreover , patients were not selected , and many advanced tumors ( rt3 / 4 = 80% ) were included in our analysis leading to a larger median ptv of 183 cm3 . earlier reports of reirradiation with a mean dose of 5068 gy showed a 2 - year survival rate of up to 40% , but also late toxicity rates of up to 30% [ 9 , 17 , 23 ]  . 
 [ 30 ] , grade 4 acute toxicity occurred in approximately 30% of cases and severe late toxicity in 20% ( including 3 cases of osteoradionecrosis and 1 case of temporal lobe necrosis ) , in our treatment group grade 4 acute toxicity was observed in 2 patients ( 20% ) , i.e. , 1 flap necrosis and 1 acute arterial bleeding . 
two patients showed late toxicity : trismus and nonbacterial salivary gland inflammation with severe pain requiring opioid medication . increasing rates of late toxicity have been reported when cumulative lifetime doses over 100 gy were applied [ 22 ]  . 
 [ 18 ] reported that acneiform rash grade 15 occurred in 42% and grade 35 in 8% of cetuximab - treated patients ; 7% of the patients suffered an infusion reaction . 
 similar results were observed in our group : 4 patients had no rash , 2 patients had grade 1 , 2 patients grade 2 , and 2 patients grade 3 . 
it appears that reirradiation does not increase cetuximab - related toxicity , such as acneiform rash or allergic reaction , compared with primary radiotherapy . one patient died of acute arterial bleeding 0.5 months after the end of reirradiation , which was considered an acute toxicity event ; his cumulative lifetime dose was 121 gy . 
it has been reported that epidermal growth factor receptors , which are blocked by cetuximab , are also present on endothelial cells of arterial vessels [ 32 ]  . conclusion imrt reirradiation with concurrent cetuximab immunotherapy in recurrent hnc is feasible with acceptable toxicity in strahlenther onkol 2011 no . 
further investigations are necessary to determine the role of concurrent cetuximab immunotherapy in reirradiation of recurrent hnc . strahlentherapie und onkologie original article feasibility , toxicity , and efficacy of short induction chemotherapy of docetaxel plus cisplatin or carbo platin ( tp ) followed by concurrent chemoradio therapy for organ preservation in advanced cancer of the hypopharynx , larynx , and base of tongue early results sabine semrau1 , frank waldfahrer2 , michael lell3 , rainer linke4 , gunther klautke1 , torsten kuwert4 , michael uder3 , heinrich iro2 , rainer fietkau1 purpose : concurrent chemoradiotherapy ( crt ) is standard treatment for advanced head and neck cancer . 
the present study aimed to assess the feasibility , toxicity , and efficacy of induction with docetaxel and platinum salt ( tp ) and subsequent crt . patients and methods : a total of 25 patients with functionally inoperable cancer of the base of the tongue , hypopharynx , or larynx received 1 cycle of docetaxel ( 75 mg / m , day 1 ) combined with either cisplatin ( 30 mg / m , days 13 ; n = 23 ) or carboplatin ( auc 1.5 days 13 ; n = 2 )  . 
responders ( n = 22 , > 30% tumor reduction , graded by endoscopy ) and 1 non - responder received crt ( target dose : 6972 gy ) with cisplatin / paclitaxel , carboplatin / paclitaxel , or cisplatin / docetaxel . results : all patients completed ict with acceptable toxicity ( leukocytopenia grade 4 : 8% )  . 
the acute toxicity of crt was moderate , no grade 4 toxicities occurred , while grade 3 toxicities included the following : infection ( 39% ) , dermatitis ( 13% ) , leukocytopenia ( 30% ) , and thrombocytopenia ( 4% )  . 
 organ preservation was possible in 22 / 23 ( 95% ) cases . conclusion : short induction with a tp regimen and subsequent crt with a taxan is feasible and associated with an encouraging local control rate . key words : laryngeal cancer hypopharyngeal cancer induction chemotherapy chemoradiation strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2178 - 2 durchfhrbarkeit , toxizitt und effektivitt der kurzinduktionschemotherapie mit docetaxel und cisplatin oder carboplatin ( tp ) vor radiochemotherapie ( rct ) zum organerhalt bei patienten mit hypopharynx - , larynx und zungengrundkarzinomen erste ergebnisse ziel : die simultane radiochemotherapie ( crt ) ist standard bei fortgeschrittenen kopf - hals - tumoren . 
in der studie werden durchfhrbarkeit , toxizitt und effektivitt einer induktionschemotherapie mit docetaxel und einem platinsalz einschlielich der folgenden rct berichtet . 1klinik fr strahlentherapie der universitt erlangen - nrnberg , erlangen , germany , 2hals - nasen - ohrenklinik , kopfund halschirurgie der universitt erlangen - nrnberg , erlangen , germany , 3radiologisches institut der universitt erlangen - nrnberg , erlangen , germany , 4nuklearmedizinische klinik der universitt erlangen - nrnberg , erlangen , germany . received : may 18 , 2010 ; accepted : september 29 , 2010 published online : december 22 , 2010 strahlenther onkol 2010 urban & vogel semrau s , et al . 
induction chemotherapy and chemoradiation in h&n cancer for organ preservation patienten und methode : 25 patienten mit einem nicht funktionserhaltend operablen zungengrund - , hypopharynxund larynxkarzinom erhielten einen zyklus docetaxel ( 75 mg / m2 , d1 ) und cisplatin ( 30 mg / m2 d - 13 ) ( n = 23 ) oder carboplatin ( auc 1 , 5 d1 - 3 ) ( n = 2 )  . 
responder ( n = 22 , mehr als 30% rckbildung endoskopisch ) und ein non - responder erhielten nachfolgend eine rct ( zieldosis : 6972 gy ) mit cisplatin / paclitaxel rsp . 
die akuttoxizitt der rct war moderat , keine grad - 4 - toxizitt ; grad - 3 - toxizitten : infektion ( 39% ) , dermatitis ( 13% ) , leukozytopenie ( 30% ) , thrombozytopenie ( 4% )  . 
die organerhaltquote lag bei 95% ( 22 / 23 )  . schlussfolgerung : die kurzinduktion mit tp und die nachfolgende crt mit einem taxan sind durchfhrbar und fhrten zu einer ermutigenden tumorkontrolle . schlsselwrter : larynxkarzinom hypopharynxkarzinom induktionschemotherapie radiochemotherapie introduction concurrent chemoradiotherapy ( crt ) is the standard treatment for laryngeal and hypopharyngeal cancer , the surgical resection of which would endanger preservation of the patients ability to swallow or speak . 
compared to primary surgery , the use of crt for organ preservation does not result in a survival disadvantage [ 6 , 7 , 12 , 13 , 21 ]  . however , there are some arguments against primary crt . 
in essence , if complete remission is not achieved , surgical salvage treatment could be difficult and the functional outcome of crt may be uncertasignificant room for improvement , therefore , lies in the enhancement of the efficacy of both radiotherapy and chemotherapy and the identification of patients who will not respond to crt . induction regimens focus on the areas of patient selection and treatment escalation , whereby decisions regarding the combination partner , the number of treatment cycles , and the later selection criteria are based on historical evidence . 
integrating taxanes into the induction and crt without impairing the feasibility of crt is in one area of interest and the determination of early markers of prediction of the later response is crucial . based on this rationale , we developed a protocol using taxotere in combination with a platinum derivative for single cycle induction chemotherapy ( ict ) prior to a taxanecontaining crt . 
the results of the feasibility and toxicity assessments and early data on the efficacy with a focus on the proportion of prevented surgical procedures are presented here . informing them of the nature and scope of the procedure and the possible treatment alternatives . diagnostics for assessment of the extent of spread , whole - body pet / ct , ultrasound of the neck , and contrast - enhanced computed tomography ( ct ) were routinely performed prior to the start of treatment . 
the response to treatment was evaluated by panendoscopy , ct and pet / ct 3 weeks after ict and 6 weeks after crt . the chief criteria for recommendation of crt following ict were significant reduction of dimension ( > 30% ) of the primary tumor as determined by endoscopy , significant reduction of glucose uptake ( 20% ) in the primary tumor as determined by pet / ct , and the absence of tumor progression as determined by ct . 
crt was scheduled to begin 4 weeks to no more than 5 weeks after induction . patients and methods inclusion criteria chemoradiotherapy from march 2008 to september 2009 , 25 patients with squamous cell carcinomas of the larynx , pharynx , or base of the tongue expected to result in functional impairment if treated surgically were recruited . 
further eligibility requirements were ecog 02 , a maximum age of 78 years , and written informed consent after individual counseling crt was performed using a combination of cisplatin / paclitaxel ( n = 16 ) , carboplatin / paclitaxel ( n = 5 ) , or cisplatin / docetaxel ( n = 2 )  . 
chemotherapy was not performed in patients with leukocytopenia ( < 3 gpt / l ) , thrombocytopenia ( < 100 gpt / l ) , or dermatitis ( grade 3 or higher )  . 
for target volume definition , the pretreatment ct and pet / ct were used . criteria of analysis the acute adverse events occurring induction phase until from the 6 - week follow - up after crt were classified according to the common terminology criteria of adverse events ( version 3 )  . 
the response of lymph node metastases to the ict and crt was disregarded because of the possibility of subsequent neck dissection . statistical analysis the primary efficacy variable was a complete remission rate of more than 85% ( primary tumor ) 6 weeks after crt , as confirmed by panendoscopy . 
therapieprotokoll der induktionschemotherapie mit docetaxel und einem platinderivat vor einer taxanhaltigen rct . or carboplatin could be postponed for no more than 1 week in the second cycle or cancelled if there was insufficient restoration of myelopoesis . radiotherapy was administered using a 6 mv linear accelerator according to three - dimensional ( 3d ) planning . 
lymph nodes with a high risk of locoregional recurrence received a dose of 58.0 results patients the large majority of patients in the study population had stage iii or iva ( 88% ) cancer of the hypopharynx ( 40% ) or larynx ( 40% )  . 
crt was initiated 45 weeks after induction in 23 / 25 patients , and 67 weeks in 2 patients due to organizational reasons . chemoradiotherapy after ict , 23 patients received crt and 2 underwent surgery ( resection of base of tongue or larynx )  . 
the estimated biologically effective dose was greater than 69 gy . crt was performed using paclitaxel plus cisplatin in 16 cases , paclitaxel plus carboplatin in 5 cases , and cisplatin plus docetaxel in 2 cases . 
the latter treatment regimen was abandoned due to severe skin toxicity at docetaxel dose level 1 ( 10 mg / m / week )  . in the end , 56% of the patients received at least 80% of the planned dose , i.e. , a minimum of either cisplatin ( 140 mg / m2 ) or carboplatin ( auc 7 ) was combined with paclitaxel ( 140 mg / m2 )  . 
the 2 patients treated with docetaxel received 30 mg / m2 and 40 mg / m2 together with cisplatin 140 mg / m2 and 100 mg / m2 . toxicity no serious adverse events occurred during ict . 
notable events were grade 4 leukocytopenia ( 8% ) , which proceeded without complications but prevented further dose escalation , and reduced renal clearance ( grade 1 in 4 cases and grade 2 in 1 case )  . increased susceptibility to infection was a frequent side effect of crt . 
relevant toxicities are listed in table 2 . response to ict and treatment decisionmaking in 7 / 25 ( 28% ) patients , a single induction cycle induced clinically complete tumor regression evaluated by endoscopy , which was histologically confirmed in 5 cases ( 20% )  . 
patientencharakteristik. number of patients ( n = 25 ) percentage ( % ) male female primary site mesopharynx hypopharynx larynx t stage n stage uicc stage ( 7th edition ) strahlenther onkol 2010 semrau s , et al . 
akuttoxizitt der induktionstherapie und der radiochemotherapie . toxicity grade 2 ( absolute ) grade 2 ( relative ) grade 3 ( absolute ) grade 3 ( relative ) grade 4 ( absolute ) grade 4 ( relative ) induction chemotherapy ( n = 25 ) hematologic adverse events anemia transfusion leukocytopenia febrile neutropenia g0csf use thrombocytopenia nonhematologic adverse events infection elevated creatinine bleeding chemoradiotherapy ( n = 23 ) hematologic adverse events anemia transfusions leukocytopenia febrile neutropenia thrombocytopenia nonhematologic adverse events infection elevated creatinine bleeding dermatitis oral mucositis 8% 4% 4% 9% 9% ( 2 x crt with docetaxel ) 4% 4% 4% 1 ( required tracheotomy ) 4% response to crt after completion of crt , 21 of the 23 nonsurgically treated patients had an endoluminal diagnosis of complete tumor regression , which was confirmed by biopsy in 18 cases . 
with a questionable resection status after laryngectomy , he underwent brachytherapy and is free of tumor up to date . the complete remission rate for the primary tumor assessed by endoscopy was 22 / 23 patients ( 95% ) for all receiving crt and 88% in all 25 patients . 
the percentage of patients with surgery after icr or crt with curative intent was 12% ( 3 / 25 )  . at baseline , 19 of 25 patients had lymph node involvement . 
complete remission following crt was achieved in 17 ( 89% ) of the 19 patients with initial lymph node involvement . disease control and survival the median follow - up duration was 11 months ( range , 624 months )  . 
kosmesis und toxizitt nach einer nachbeobachtungszeit von mehr als 6 wochen nach dem therapieende . cases percentage ( % ) functional and cosmetic outcomes ( n = 21 ) ecog tracheostomy after treatment before treatment ( tumor - related ) during treatment ( bleeding ) after treatment ( toxicity - related ) after treatment ( recurrence - related ) voice change ( not related to tracheostomy ) none mild to moderate intermittent hoarseness nutrition complete return to oral nutrition feeding tube used for substitution , patient able to swallow liquids completely tube - dependent pain none mild pain with no functional impairment mucositis none erythema ulceration ( patchy ) ulceration ( confluent ) salivary gland changes none slight enlargement of the salivary glands saliva thick , viscous and sticky ; noticeable taste alteration severe secretory symptoms affecting daily activities lymphedema none localized without functional impairment localized with functional impairment generalized head and neck edema hyperpigmentation none mild and local severe telangiectasia none few fibrosis none sponginess of grip stiffness and tension vision no change symptomatic / no impairment hearing no change hearing loss ( no hearing aid required ) 1 1 ( oral ) 1 8 4 1 1 1 1 8 9 8 2 2 3 7 1 8 9 2 2 5 1 2 6 5 1 5 5 5 5 8 8 5 5 functional outcomes data from 21 of the 23 patients who received ict plus crt were available . 
the rehabilitation outcomes for swallowing function were not as good : 11 patients ( 52% ) were completely feeding tubefree and resumed a normal diet with no weight loss , while 8 were partially and 2 were completely tube - dependent . discussion this study demonstrates that ict and crt with a taxane and a platinum derivative are feasible and well tolerated . 
ict and crt induced complete remission in more than 80% of the patients with a low rate of secondary resections so far . the actual proposed crt was designed to enable the integration of taxanes , which have proved to be very effective in combination with cisplatin with or without 5 - fluorouracil and with radiotherapy [ 1 , 3 , 10 ]  . 
 [ 11 ] proposed a concurrent chemoradiation in which cisplatin ( 20 mg / m / day ) was administered on days 15 and 2933 and paclitaxel ( 25 mg / m / day ) was administered twice weekly for 12 cycles . 
however , this did not apply to the group given parallel doses of docetaxel , who developed grade 3 skin toxicities after 34 doses of 10 mg / m docetaxel strahlenther onkol 2010 semrau s , et al . 
thus , organ preserving surgical procedures without crt also result in significant swallowing problems [ 15 ]  . in the end , the question of whether one cycle of induction chemotherapy will suffice to achieve a predictable response to subsequent chemoradiotherapy remains to be clarified . 
this assumption is supported by the findings of a study performed at the university of michigan [ 23 ] , which investigated the prognostic relevance of one induction cycle for early tumor response . 
the induction regimen made it possible to keep the rate of secondary laryngectomy below 10% . although the number of patients in our population is too small and the follow - up period too short to draw reliable conclusions , the fact that only 2 patients had persistent local tumor and local recurrence after chemoradiotherapy is very promising . strahlentherapie und onkologie original article comparison of the micronucleus and chromosome aberration techniques for the documentation of cytogenetic damage in radiochemotherapy - treated patients with rectal cancer hendrik andreas wolff * 1 , steffen hennies * 1 , markus karl alfred herrmann1 , margret rave - frnk1 , david eickelmann1 , patricia virsik2 , klaus jung3 , markus schirmer4 , michael ghadimi5 , clemens friedrich hess1 , robert michael hermann1 , 6 , hans christiansen1 purpose : the goal of the interdisciplinary clinical research unit kfo179 ( biological basis of individual tumor response in patients with rectal cancer ) is to develop an individual response and toxicity score for patients with locally advanced rectal cancer treated with neoadjuvant radiochemotherapy . 
the aim of the present study was to find a reliable and sensitive method with easy scoring criteria and high numbers of cell counts in a short period of time in order to analyze dna damage in peripheral blood lymphocytes . 
thus , the cytokinesis - block micronucleus ( cbmn ) assay and the chromosome aberration technique ( cat ) were tested . materials and methods : peripheral blood lymphocytes obtained from 22 patients with rectal cancer before ( 0 gy ) , during ( 21.6 gy ) , and after ( 50.4 gy ) radiochemotherapy were stimulated in vitro by phytohemagglutinin ( pha ) ; the cultures were then processed for the cbmn assay and the cat to compare the two methods . results : a significant increase of chromosomal damage was observed in the course of radiochemotherapy parallel to increasing radiation doses , but independent of the chemotherapy applied . 
for further investigations , we prefer the cbmn assay , because it is simpler through easy scoring criteria , allows high numbers of cell counts in less time , is reliable , sensitive , and has higher statistical power . 
in the future , we plan to integrate cytogenetic damage during radiochemotherapy into the planned response and toxicity score within our interdisciplinary clinical research unit . key words : rectal cancer neoadjuvant radiochemotherapy micronuclei chromosome aberration technique lymphocytes strahlenther onkol 2011 ; 187 : 528 doi 10.1007 / s00066 - 010 - 2163 - 9 vergleich von mikronukleusund chromosomenaberrationstechnik fr die dokumentation zytogenetischer schden bei neoadjuvant radiochemotherapierten patienten mit rektumkarzinom ziel : ziel der interdisziplinren klinischen forschergruppe kfo179 ( biological basis of individual tumor response in patients with rectal cancer ) ist es , einen individuellen response - / toxizittsscore fr patienten zu entwickeln , die bei diagnostiziertem lokal fortgeschrittenem rektumkarzinom mit neoadjuvanter radiochemotherapie behandelt werden . 
ziel der vorliegenden arbeit war , eine einfache und zuverlssige methode zur detektion des individuellen zytogenetischen schadens durch die radiochemotherapie herauszuarbeiten , die im weiteren verlauf der arbeit der forschergruppe anwendung finden soll . 
hennies contributed equally to this work received : april 19 , 2010 ; accepted : september 16 , 2010 published online : december 23 , 2010 strahlenther onkol 2011 no . 
radiation - induced cytogenetic damage in rectal cancer patients patienten und methodik : periphere blutlymphozyten von 22 patienten wurden vor ( 0 gy ) , whrend ( 21 , 6 gy ) und nach ( 50 , 4 gy ) radiochemotherapie untersucht . 
der zytogenetische schaden wurde mittels mn und caa analysiert und die quivalenz beider methoden geprft . ergebnisse : eine signifikante zunahme chromosomaler schdigungen durch die bestrahlung in abhngigkeit von der applizierten dosis konnte bei beiden techniken , unabhngig von der applizierten chemotherapie , beobachtet werden . 
die gleichwertigkeit beider methoden konnte durch den quivalenztest nach westlake gezeigt werden . schlussfolgerung : es zeigte sich eine quivalenz der angewandten methoden , was uns nun die mglichkeit bietet , den mn gleichwertig gegenber der caa anzuwenden und fr die geplanten analysen bezglich des individuellen response - / toxizittsscores zu verwenden . 
die mikronukleustechnik ermglicht durch leichtere zhlkriterien in krzerer zeit eine grere anzahl von zellen zu zhlen , was zu einem valideren statistischen endergebnis fhrt . schlsselworte : rektumkarzinom neoadjuvante radiochemotherapie mikronuklei chromosomaberrationstechnik lymphozyten introduction neoadjuvant radiochemotherapy followed by surgery is the standard approach for treatment of locally advanced rectal cancer [ 21 , 24 , 30 , 40 , 43 ]  . 
the interdisciplinary clinical research unit kfo 179 ( biological basis of individual tumor response in patients with rectal cancer ) of the dfg ( german research foundation ) aims to enhance the understanding of the biological basis of tumor response and to establish predictors of response and of treatment toxicity . 
the ultimate goal is to develop an individual response and toxicity score . to document treatment response and toxicity , biological and molecular parameters were collected in addition to clinical data . 
radio ( rtx ) and chemotherapy ( ctx ) cause dna damage , which can be detected in whole blood lymphocytes using the chromosome aberration ( ca ) technique ( cat ) and by the cytokinesis - block micronucleus ( cbmn ) assay . concerning the cat , a dose - dependent increase in the yield of ca frequency has been shown in rtx of patients at different sites [ 2 , 8 , 26 , 27 ]  . 
it has been shown that the cbmn assay is simple , reliable , and sensitive , resulting from the statistical power afforded by a high scoring rate achievable in less time [ 9 , 1214 ]  . 
the aim of the present study was to compare the results of the cat and the cbmn assay in human lymphocytes of rectal cancer patients treated within the randomized clinical trial cao / aro / aio - 04 ( chirurgische arbeitsgemeinschaft fr onkologie ( cao ) / arbeitsgemeinschaft radiologischer onkologie ( aro ) / arbeitsgemeinschaft internistische onkologie ( aio ) - 04 ) of the german rectal cancer study group . 
in that study , patients with locally advanced rectal cancer ( uicc stage ii / iii ) were treated in a neoadjuvant setting with radiotherapy ( 50.4 gy ) either with standard chemotherapy with 5 - fluorouracil ( arm a ) or with an experimental chemotherapy regimen using 5 - fu and oxaliplatin ( arm b )  . 
a summary of patient characteristics are shown in table 1 . methods cell cultures to display cytogenetic damage , heparinized peripheral blood samples were obtained from untreated patients before therapy ( 0 gy ) and during therapy after 21.6 gy ( 12 fractions ) and 50.4 gy ( 28 fractions ) , respectively . chromosome aberrations whole blood lymphocytes ( 6 ml per culture ) were cultured in 54 ml roswell park memorial institute medium ( rpmi ; ph 7.2 ) containing 10% fetal calf serum , 100 l / ml pha , and antibiotics ( 104 iu / ml penicillin and 10 mg / ml streptomycin ( gibco , auckland , new zealand ) ) in 5% co2 atmosphere at 37 c . 
metaphase cells were prepared according to the standard method ( hypotonic 0.56 m kcl ; merck , darmstadt , germany ) treatment followed by fixation in methanol ( merck , darmstadt , germany ) plus glacial acetic acid ( 3 : 1 ; merck , darmstadt , germany ) and stored at 4 c . 
the optimal culture time for cell preparations containing not more than 6% of cells in their second postirradiation mitosi , was chosen according to the results of foregoing evaluation based upon fluorochrome - photolysis - giemsa ( fpg ) staining . 
patients ( % ) characteristic gender male female therapy arm a ( 5 - fu mono ) b ( 5 - fu and oxaliplatin ) pretherapeutic t stage pretherapeutic n stage pretherapeutic uicc stage 15 ( 68% ) 7 ( 32% ) 13 ( 59% ) 9 ( 41% ) 1 ( 5% ) 21 ( 95% ) 8 ( 36% ) 14 ( 64% ) 8 ( 36% ) 14 ( 64% ) allowed for differentiating between first and second postirradiation metaphases . scoring of chromosome aberrations was performed with a 1000x magnification light microscope . 
quantity and completeness of mitosis as well as condensation and identifiability were checked before starting to count structural chromosometype aberrations ( acentric fragments , dicentric chromosomes , centric rings ) in up to 200 metaphases for each patient at every dose point . 
this was not possible for every dose point because of the loss of lymphocytes during therapy . micronucleus test blood samples were diluted 1 : 2 with 0.9% nacl ( merck , darmstadt , germany ) before isolating the lymphocytes by using density gradient centrifugation . 
rpmi medium was added to a total volume of 50 ml and 500 l pha was supplemented prior to cultivation ( 37 c , 5% co2 ) for 44 hours . 
cytochalasin b ( cyt - b ) ( sigma , steinheim , germany ) was added at a concentration of 4.5 g / ml and after another 28 hours of cultivation , cells were cytospun on glass microscope slides . 
 after fixing with methanol and staining with fpg staining ( diff - quik , medion diagnostics gmbh , ddingen , switzerland ) , 1000 binucleated cells ( bn ) / dose point of every patient with well - preserved cytoplasm were analyzed and micronuclei ( mn ) as well as nucleoplasma bridges ( npb ) were counted . 
the results were denoted as mn per binucleated cell . in vitro experiments heparinized peripheral blood samples of 4 healthy donors ( 2 male , 2 female ; aged 2957 years ) were prepared as described above in the micronucleus test section . 
parallel to the addition of phytohemagglutinin ( pha ; biochrom , karlsruhe , germany ) , the following chemotherapeutic agents were added : 0.15 g / ml 5 - fu ( 1 hour and 24 hours incubation time ) and 2.5 m oxaliplatin ( 2 hours and 25 hours incubation time ) separately to each donors sample to display the cytogenetic damage caused by ctx . 
subsequent , pair - wise comparisons between methods and dose levels , respectively , were performed by wilcoxons matched pairs test due to the non - normality of the data . 
as a nonrejection of a null hypothesis , no difference between methods does not imply the equivalence of the methods ; thus , pair - wise equivalence tests were also performed [ 41 ] to compare yields of ca and mn . 
pair - wise comparisons , subsequent to a nonsignificant global result from analysis of variance , were performed at a bonferroni - adjusted significance level of * = 5% / 3 = 1.67%. 
analysis of variance was carried out with sas ( version 9.1 , sas institute )  . the cytogenetic damage of patients receiving 5 - fu , or 5 - fu and oxaliplatin was compared at a dose level of 50.4 gy by mannwhitney u - test . 
the spontaneous rate of mn comparing women and men was also evaluated with the mann whitney u - test . for the in vitro experiment to examine the influence of 5 - fu and of oxaliplatin separately on peripheral blood lymphocytes ( pbl ) of healthy donors , the wilcoxons matched pairs test was again performed . 
radiation - induced cytogenetic damage in rectal cancer patients difference between ca and mn for dicentric chromosomes ( dc ) at both dose points , the equivalence of both methods was shown by westlakes equivalence test ( table 4 , figures 2 and 3 )  . 
single comparisons between dose levels revealed a significant increase of ca or mn between each pair of dose level ( table 2 )  . arm a and arm b treatment comparing arm a with arm b patients , arm b patients showed less cytogenetic damage ( table 5 ) , but no significant differences were observed between arms . in vitro study since all patients received combined radiochemotherapy , we also performed a separate in vitro assay to examine the influence of 5 - fu and of oxaliplatin separately on pbl of healthy donors ( n = 4 ) with different doses and with different time of exposure ( table 6 )  . 
 cytogenetic techniques , including the widely used analysis of chromosome aberrations [ 2 , 8 , 15 , 26 , 27 , 31 , 34 , 37 , 46 ] and the nowadays frequently used micronucleus test [ 3 , 7 , 9 , 16 , 23 , 25 , 28 , 31 , 3436 , 39 , 42 ] , are not only reliable indicators of damage to the cell genome in vivo and in vitro , but are also applicable for different and combined radiation qualities [ 45 ]  . 
taking either ca or mn as an endpoint , we found that the neoadjuvant radiochemotherapy causes cytogenetic damage to the dna molecular structures of the patients lymphocytes , which increased significantly during the course of therapy in both techniques . 
an extensive induction of interphase death or apoptosis during radiochemotherapy could have caused a loss of cells with severe genomic damage , resulting in a false lowering of genomic damage . the use of the cat allows the discrimination between different types of cas , e.g. , dicentric chromosomes ( dc ) and acentric fragments ( af )  . 
kormos & kteles [ 22 ] compared the dose effect relationships of formations of dc and af with that of mn in cultured human lymphocytes after induction of ionizing radiations . 
 [ 18 ] , in vitro irradiated human lymphocytes of healthy donors with no recent diagnostic or occupational exposure to ionizing or non - ionizing radiation were exposed to radiation at different doses and different duration of exposure . 
a positive correlation between mn and specific chromosomal aberrations ( af , dc ) was shown [ 18 ]  . oxaliplatin as well as 5 - fu induce cytogenetic damage , which has been shown by several authors [ 1 , 20 , 29 , 44 ]  . 
the effect of ctx and rtx , either alone or in combination , showed no significance of the ctx on mutation so that it was wholly accounted for by the effect of rtx . 
contrary results concerning the relationship of cytogenetic damage caused by rtx and ctx as mentioned above are not described in the literature . in summary , both techniques detected therapy - induced dna damage in patients lymphocytes ; mn and dc were statistically equivalent . 
because of its simplicity through easy scoring criteria , high number of cell counts in less time , reliability , sensitivity , the possibility of using automated systems , and overall statistical power , we favor integrating the cbmn assay into the planned response and toxicity score . acknowledgment this work was supported by the german research society ( dfg , kfo 179 )  . 
 strahlentherapie und onkologie original article neoadjuvant radiochemotherapy and surgery for advanced rectal cancer prognostic significance of tumor regression * hans theodor eich1 , anna stepien1 , christian zimmermann1 , martin hellmich3 , ralf metzger2 , arnulf hlscher2 , rolf - peter mller1 purpose : preoperative radiochemotherapy is widely used in the treatment of locally advanced rectal cancer . 
the predictive value of response to neoadjuvant treatment remains uncertawe retrospectively evaluated the impact of downstaging and tumor regression as prognostic factors and its influence on the ability to perform sphincter - sparing surgery . 
all patients were treated with preoperative 5 - fluorouracil - based chemotherapy and pelvic radiation with a total dose of 50.4 gy followed by surgery 6 weeks later . results : a sphincter - preserving procedure could be performed on 42 patients , and in all 72 patients complete resection ( r0 ) was achieved . 
the impact of tumor regression grading needs to be further validated in prospective clinical trials . key words : radiotherapy rectal carcinoma neoadjuvant radiochemotherapy prognostic factors strahlenther onkol 2011 ; 187 : 22530 doi 10.1007 / s00066 - 011 - 2113 - 1 neoadjuvante radiochemotherapie und operation fortgeschrittener rektumkarzinome : tumorregression stellt prognostischen faktor dar hintergrund : die properative radiochemotherapie ( rcht ) gefolgt von einer operation stellt heute die standardbehandlung fr patienten mit lokal fortgeschrittenem rektumkarzinom dar . 
die behandlung bestand aus einer perkutanen radiotherapie mit 50 , 4 gy und einer simultanen 24 - h - dauerinfusion von 5 - fluorouracil ( woche 1 und 5 ) gefolgt von einer radikalen tumorresektion . 
neben dem ansprechen des tumors im sinne eines downstagings wurden mgliche prognostische faktoren analysiert . ergebnisse : nach einer medianen nachbeobachtungszeit von 28 monaten kam es bei keinem patienten zu einem lokalrezidiv und bei allen 72 patienten gelang eine komplette resektion ( r0 )  . 
 1department of radiation oncology , university of cologne , germany , 2department of general , visceral and cancer surgery , university of cologne , germany , 3institute of medical statistics , informatics , and epidemiology , university of cologne , germany . received : december 7 , 2009 ; accepted : april 15 , 2010 published online : march 7 , 2011 strahlenther onkol 2011 n0 . 
neoadjuvant radiochemotherapy for rectal cancer zeigten patienten unter 65 jahre ein signifikant besseres ansprechen auf die properative rcht im sinne eines downstagings als patienten ber 65 jahre ( p = 0 , 036 )  . 
 inwieweit die tumorregression als valider prognoseparameter angesehen werden kann , muss in prospektiven klinischen studien berprft werden . schlsselwrter : radiotherapie rektumkarzinom neoadjuvante radiochemotherapie prognostische faktoren introduction locally advanced rectal cancer is one of the most frequent tumors . 
most of the patients are male and the mean age is between 6065 years . prospective trials that have investigated the potential advantage of preoperative radiochemotherapy with 5 - fluorouracil ( 5 - fu ) over radiotherapy ( rt ) alone have shown that the addition of chemotherapy to preoperative rt results in downsizing and pathological downstaging and improves local control but has no significant effect on survival of patients . 
based on these clinical data , preoperative radiochemotherapy followed by surgery is the standard treatment for locally advanced rectal cancer [ 1 , 2 , 4 , 9 , 15 , 16 , 23 , 26 , 28 ]  . the purpose of this analysis was to evaluate the cologne experience of patients who received neoadjuvant radiochemotherapy for locally advanced rectal cancer . 
 surgery was performed in 46 patients at the department of general , visceral , and cancer surgery , university of cologne , germany , and in 26 patients at nonacademic referral hospitals ( n = 10 )  . the regime was used for locally advanced rectal cancer stage iiiii according to the uicc classification which were resectable and had no distant metastases . 
postoperative chemotherapy of patients with preand postoperative n + status was scheduled depending on the patients condition 46 weeks after surgery and was delivered in four courses ( 5 - fu 500 mg / m2 every 4 weeks )  . preoperative clinical staging all patients underwent a complete history , physical examination , digital rectal examination , transrectal rectoscopy with biopsy , full colonoscopy when possible , computed tomographic ( ct ) scan of the chest , abdomen and pelvis , and endosonography . 
every visible lymph node in the transrectal ultrasound and / or in the ct was classified as positive [ 25 ]  . histopathologic staging and assessment of tumor regression histopathologic staging was performed according to the ptnm classification of the uicc [ 31 ]  . 
the amount of fibrosis , ranging from no evidence of any treatment effect to a complete response with no viable tumor identified , as described by mller and junker [ 14 ]  . 
tumor downstaging was defined by a comparison in the pretreatment tn stage ( determined by clinical , radiographic , and ultrasound staging ) to the pathologic stage [ 30 ]  . follow - up follow - up examinations were recommended at 3 - month intervals for 2 years , then at 6 - month intervals for 3 years . 
recto and colonoscopy , abdominal ultrasound , ct of the abdomen , and chest radiograph were applied according to the guidelines of the german cancer society [ 13 , 27 ]  . 
alternate acceptable criteria included sequential enlargement of a mass in radiologic studies . statistical analysis the 2 trend test for ordered categories was used for ordered prognostic factors with more than two categories . 
the surgical procedures included abdominoperineal resection in 20 patients ( 28% ) , low anterior resection in 40 patients ( 56% ) , anterior resection in 5 patients ( 7% ) , intersphincter resection in 1 patient ( 1% )  . 
two of these patients , each with two liver metastases , were treated with radiofrequency ablation , 1 patient with three metastatic lesions with hemihepatectomy , and another patient with five metastases was treated with atypical liver segmentectomy . survival at a median follow - up of 28 months , 90% of the patients were alive . 
the 2 - year dfs for patients with intermediate ( less than 10% residual tumor cells ) or complete tumor regression ( ypt0 , ypn0 ) was 100% compared with 82% 9.4% for patients with 10% residual tumor cells and 76% 14.8% for patients with poor response ( > 10% residual tumor cells )  . 
a complete remission ( ypt0 , ypno ) was achieved in 8 patients ( 11% ) : 1 of these patients had an initial uicc stage of i , 2 patients stage ii , and 5 patients stage iii . 
neoadjuvant radiochemotherapy for rectal cancer ported some form of fecal incontinence , 6 patients complained about perianal pain , 1 patient about erectile dysfunction , and 3 patients had chronic diarrhea [ 5 , 7 , 8 ]  . 
 discussion this retrospective study presents the outcome of 72 consecutive patients , who received neoadjuvant radiochemotherapy for locally advanced rectal cancer comparable to the regimen of the german rectal cancer group [ 26 ]  . 
the following results emerge from this study : preoperative radiochemotherapy induces a significant downstaging with 8 patients ( 11% ) achieving a pathological complete response ( pcr ) of the tumor ( ypt0ypn0 )  . tumor regression revealed by the histopathological examination serves as a good prognostic index for disease - free survival . sphincter sparing was achieved in 59% of all patients . 
 [ 12 ] presented the results of preoperative radiochemotherapy in 117 patients with locally advanced rectal cancer : 45 gy in 25 fractions over 5 weeks with continuous infusion of 5 - fu ( 300 mg / m2 / day )  . 
the long - term outcome of patients exhibiting pcr is favorable ( local relapse rate 1.6% , 5 - year cancer - specific survival 94% ) [ 3 ]  . 
two - drug regimens were shown to be associated with higher pcr rates in an analysis of several trials including a total 3 , 157 patients [ 10 ]  . 
furthermore , molecular targeted agents such as cetuximab , an antibody targeting the epidermal growth factor receptor ( egfr ) , seems to be attractive in neoadjuvant regimens and are currently pursued . 
however , in the german margit phase ii trial , which enrolled 50 patients , the addition of cetuximab in combination with capecitabine , irinotecan , and radiotherapy failed to increase the pcr rate ( 8% ) as well as the downstaging rate ( 45% ) [ 11 ]  . 
however , a correlation between sp and t stage ( p = 0.027 ) could be defined ( table 5 )  . correlation between age and tumor staging interestingly , a relationship between downstaging and the patients age was observed . 
neoadjuvant radiochemotherapy for rectal cancer was 86% for patients when no viable tumor cells were detected , 75% for patients with intermediate pathologic response , and 63% for patients with a morphologically unaltered tumor mass ( p = 0.006 ) [ 24 ]  . 
 [ 32 ] reported on a statistically significant correlation between high - grade acute organ toxicity during preoperative radiochemotherapy and complete tumor regression after total mesorectal excision in multimodal treatment of locally advanced rectal cancer . 
however , in the cao / aro / aio - 94 study [ 26 ] , the abdominoperineal resection rate was only 26% in the preoperative radiochemotherapy arthe lower rate of sp in our retrospective analysis could be influenced by a number of variables , including the specific criteria used for sp by the referring surgeon and referral bias . 
this is possibly also caused by the large variety of referring surgeons in this limited number of patients with different experience in the surgical management of rectal carcinoma [ 19 ]  . 
 [ 12 ] clearly demonstrated that preoperative radiochemotherapy allowed sphincter sparing surgery in over 40% of patients whose tumors were located < 6 cm from the anal verge who otherwise would have required colostomy . conclusion neoadjuvant radiochemotherapy with 5 - fu and 50 gy pelvic irradiation represents the standard treatment for patients with locally advanced rectal cancer . 
operation mit oder ohne sphinktererhalt in bezug auf die prtherapeutische tumorlokalisation . < 6 - cm from anus 612 cm from anus > 12 cm from anus without sphincter preservation 11 ( 15% ) 14 ( 20% ) 4 ( 5% ) 29 ( 40% ) with sphincter preservation 9 ( 13% ) 23 ( 32% ) 11 ( 15% ) 43 ( 60% ) 20 ( 28% ) 37 ( 52% ) 15 ( 20% ) table 5 . 
the impact of trg needs to be further validated in prospective clinical trials . original article stereotactic body radiation therapy ( sbrt ) for treatment of adrenal gland metastases from non - small cell lung cancer richard holy , marc piroth , michael pinkawa , michael j . 
we present our initial institutional experiences with sbrt for adrenal gland metastases . patient and methods : between july 2002 and september 2009 , 18patients with a non - small cell lung cancer and adrenal metastasis received sbrt . 
an isolated adrenal metastasis was diagnosed in 13 patients , while 5 patients with multiple metastatic lesions had sbrt due to back padepending on treatment intent and target size , the dose / fraction concept varied from 5 x 4 gy to 5 x 8 gy . 
dose was given with an isotropic convergent beam technique to a median maximum dose of 132% to the targets central part . results : the mean clinical ( ctv ) and planning target volume ( ptv ) was 89 cm ( 5260 cm ) and 176 cm ( 20422 cm )  . 
a median progression - free survival time ( pfs ) of 4.2 months was obtained for the entire patient group , with a markedly increased pfs of 12 months in 13 patients suffering from an isolated metastasis of the adrenal gland . 
in these patients , median overall survival ( os ) was 23 months . conclusion : sbrt is a feasible and safe technique for lung cancer patients with adrenal gland metastasis . 
 acute side effects were mild . key words : stereotactic body radiation therapy adrenal metastases strahlenther onkol 2011 ; 187 : 24551 doi 10.1007 / s00066 - 011 - 2192 - z behandlung von nebennierenmetastasen nichtkleinzelliger bronchialkarzinome mit extrakranieller stereotaktischer strahlentherapie ( esrt ) hintergrund : nebennierenmetastasen nichtkleinzelliger bronchialkarzinome sind hufig , und die systemische therapie ist die meistgenutzte behandlungsoption . 
wir prsentieren unsere institutionellen erfahrungen mit der esrt von nebennierenmetastasen . patienten und methodik : zwischen juli 2002 und september 2009 wurden 18 patienten mit nebennierenmetastasen bei nichtkleinzelligen bronchialkarzinomen mit esrt behandelt ( tabelle 1 )  . 
die dosis wurde appliziert ber eine isozentrische conformale mehrfeldertechnik mit einem medianen dosismaximum von 132% im tumorzentrum . ergebnisse : das mittlere klinischen zielvolumen ( ctv ) und das mittlere planungszielvolumen ( ptv ) lag bei 89 cm ( 5260 cm ) bzw . 
das mediane berleben von 23 monaten der patienten mit isolierter nebennierenmetastase ist exzellent und vergleichbar mit chirurgischen daten , dabei mit dem vorteil der nicht invasiven behandlungsmethode und geringer nebenwirkungsrate . schlsselwrter : extrakranielle stereotaktische radiotherapie nebennierenmetastase background new irradiation techniques like stereotactic body radiation therapy ( sbrt ) or intensity - modulated radiotherapy ( imrt ) enables highly focused dose escalation in radiosensitive body regions [ 18 , 2729 ]  . the occurrence of metastatic disease in the adrenal gland is a common problem in patients suffering from lung cancer . 
open and laparoscopic adrenalectomy [ 57 , 11 , 1417 , 20 ] and radiofrequency ablation [ 30 ] were used for local palliative treatment of these adrenal gland metastases . 
the development of sbrt led to a highly conformal dose delivery to tumors located in the body and , thereby , offers the chance to achieve high local control rates [ 2 , 3 , 9 , 32 , 34 ]  . 
in the present analysis , we retrospectively evaluated our first experience with sbrt in patients with a nonsmall cell lung cancer suffering from adrenal gland metastases . patients and methods a total of 18patients with non - small cell lung cancer and metastases to the adrenal gland ( 9 on the right , 9 on the left side ) had sbrt between july 2002 and october 2009 ( table 1 )  . 
all patients suffered from a histological proven and advanced non - small cell lung cancer ( stage iibiv , uicc 6th edition , 2002 ) [ 23 ]  . in this retrospective analysis , sbrt was considered in patients with either a controlled primary tumor and an isolated metastasis of the adrenal gland with ( n = 3 ) or without back pain ( n = 10 ) or in multiple metastasized patients with localized back pain related to an adrenal gland metastasis ( n = 5 )  . 
 out of 13 patients treated with curative intent , 8 patients revealed a complete remission of the primary disease after combined chemoand radiotherapy at time of sbrt and 5 patients showed no evidence of locoregional failure after pneumonectomy and adjuvant radiotherapy . 
in all patients , staging or restaging included a computed tomography ( ct ) of the chest and abdomen , a bone scan , and a computed tomography of the brain . sbrt technique the stereotactic methodology using the stereotactic body frame ( elekta oncology systems ) had been described in detail elsewhere [ 2 , 13 , 32 ]  . 
prior to the first treatment , a second ct examination was performed in all patients in order to study the reproducibility of positioning the target in the stereotactic system . the clinical target volume ( ctv ) was defined to include the gross tumor volume ( gtv ) with a surrounding safety margin of 2 mm to include microscopic tumor extension . 
around the ctv a margin of 5 mm was added in the transverse and 510 mm in the craniocaudal direction to obtain the planning target volume ( ptv )  . 
the reproducibility of patient positioning was calculated by orthogonal portal imaging films prior to each fraction . treatment technique and dose prescription the radiation treatment was a conformal technique using a minimum of 5 coplanar or non - coplanar static beams of 1015 mv . 
klinische charakteristika der 18 aufgrund einer nebennierenmetastase eines nichtkleinzelligen bronchialkarzinoms behandelten patienten . patient female male age median histology adenocarcinoma squamous cell carcinoma non - small cellular adenosquamous unclear physical sign no physical sign singular metastasis of the adrenal gland number 61.5 strahlenther onkol 2011 n0 . 
patients with isolated metastasis ( n = 13 ) to the adrenal gland had a median followup of 21 months , while all multiple metastasized patients died within 6 months after end of sbrt . the ctv and ptv definition yielded a mean target volume of 89 cm ( range , 5260 cm ) and 176 cm ( range , 20422 cm ) , with a reduced ctv and ptv in patients with an isolated adrenal metastasis of 46 cm ( range , 599 cm ) and 111 cm ( range , 44190.5 cm ) , respectively ( table 2 )  . local and systemic control ten out of 13 patients ( 77% ) with localized disease in the adrenal gland prior to sbrt achieved local control . 
one patient had a localized failure at the sbrt treatment site 15 months after treatment and 1patient had a localized disease progression at the treatment site 4 months after treatment . 
the median pfs for those 13 patients suffering from a solitary metastasis of the adrenal gland at time of sbrt was 12 ( range , 242 ) months ( figure 2 )  . 
the recommendation for dosevolume load to the ptv was to cover at least 90% with an escalated dose of 125% , which resulted in a median maximum dose of 132% to the targets central part . 
two 3d plans did not achieve these objectives with a maximum dose of 115% and 120% . eight patients received a total dose of 40 gy with a single dose of 8 gy per fraction . 
the corresponding biological equivalent dose ( bed ) was 72 gy , calculated according to the formula bed ( gy ) = dose / fraction fraction number ( 1 + fraction dose / / ) and an / ratio of 10 gy for tumor tissue . 
sbrt and adrenal gland metastasis symptom relief eight patients suffered from back pain , requiring analgesics in 5 of the these 5 patients had a systemic tumor progression and sbrt of the adrenal gland was highly palliative . 
in 1 patient the irradiation was finished at midtreatment due to a worsened performance status from rapid tumor progression . complete pain relief during the follow - up period could be achieved in all but 2 patients . 
 one patient complained of unchanged back pa in subsequent magnetic resonance imaging of the vertebral column , osseous metastases at the thoracic and lumbar region were diagnosed . treatment - related toxicity the most common acute side effect was minimal to moderate nausea ( rtog grade 1 , n = 6 ) during the course of sbrt . 
the mean value dose volume histogram of the kidney at the irradiation site from all patients is shown in figure 4 . two and 4 weeks after sbrt , gastroscopy revealed multiple gastric ulcers in 1 patient and both a gastric ulcer and a duodenal ulcer in another patient . 
this corresponded to a maximum dose of 19.7 gy ( bed = 35.5 gy ) ( figure 5 )  . discussion the management of patients with a metastasis of the adrenal gland from a non - small cell lung cancer is unclear . 
in symptomatic patients , suffering from back pain , palliative irradiation may be a treatment option , but published clinical data are rare [ 22 , 24 , 33 ]  . 
sarela [ 21 ] updated these results and demonstrated a median pfs of 11 months and an actuarial pfs and os of 21% and 24% after 5 years , respectively . 
 nevertheless , they observed a 19% complication rate , which were severe in 12% of patients . a total of 43 lung cancer patients with a surgically removed isolated adrenal gland metastasis , treated between 1987 and 1998 , were included in a retrospective analysis from 8 centers [ 19 ]  . 
we used mostly a margin of 1cm in the craniocaudal direction refer to the ctv , which seemed to be sufficient . at the university of rochester , 30 patients , who had undergone sbrt for adrenal metastases from various primary sites , were retrospectively reviewed [ 4 ]  . 
in both studies no rtog grade 2 or greater toxicity was shown . of the patients in our study , 13 had sbrt for an isolated adrenal gland metastasis , resulting in a 77% local control rate . 
kaplan - meier - kurve des gesamtberlebens , solitre metastase und nicht solitre metastase ( i zensiert )  . up to 45 gy for palliation of symptomatic adrenal gland metastasis between 1972 and 1988 . 
dosis - volumen - histogramm des magens , zwei patienten mit ulkus des magens / duodenums nach stereotaktischer strahlentherapie der nebenniere . advanced tumor stage in these patients , the median overall survival time of 23 months was excellent . 
as a consequence , the irradiation should be applied with an empty stomach to achieve reproducible conditions . in the future , image - guided radiotherapy ( igrt ) will offer improved reproducibility of the target volume position and should be able to detect marked normal tissue movement . 
in contrast to the use of an upper abdominal pressure to fix diaphragmatic motion , this technique could prevent the pressing of the upper abdominal organs into the target area and reduce the risk of an increased retroperitoneal target movement . conclusion sbrt is a feasible and safe technique for lung cancer patients with adrenal gland metastasis . 
 original article quantitative assessment of hypoxia subtypes in microcirculatory supply units of malignant tumors using ( immuno - ) fluorescence techniques * constantin - alin maftei , christine bayer , kuangyu shi , sabrina t . 
this approach enables assessment and recognition of different hypoxia subtypes including hypoxemic hypoxia and may facilitate methods to ( clinically ) identify and eliminate hypoxia . key words : tumor hypoxia acute hypoxia chronic hypoxia hypoxia subtypes perfusion - limited hypoxia diffusion - limited hypoxia microcirculatory supply unit strahlenther onkol 2011 ; 187 : 2606 doi 10.1007 / s00066 - 010 - 2216 - 0 quantitative erfassung verschiedener hypoxieformen in mikrozirkulatorischen versorgungseinheiten maligner tumoren mit hilfe von ( immun - ) fluoreszenztechniken hintergrund und ziel : hypoxie ist ein charakteristikum solider tumoren , fhrt zur tumorprogression und therapieresistenz . 
deshalb werden hypoxiesubtypen in mikrozirkulatorischen versorgungseinheiten ( mcsus ) mit hilfe von ( immun - ) fluoreszenztechniken identifiziert . material und methoden : gefrierschnitte von xenotransplantierten menschlichen plattenepithelkarzinomen ( sas , fadu , utscc - 5 , ut - scc - 14 , ut - scc - 15 ) werden nach pimonidazol - frbung zur hypoxiemarkierung , hoechst - 33342 - fluoreszenz zum perfusionsnachweis und cd31 - gefdarstellung untersucht . 
folgende muster knnen in vitalem gewebe nachgewiesen werden : ( 1 ) normoxie : hoechst - 33342 - fluoreszenz um gefe , keine pimonidazol - anfrbung ; ( 2 ) chronische hypoxie : hoechst - 33342fluoreszenz in direkter gefnhe , pimonidazol in einer gewissen distanz zu den gefen ; ( 3 ) akute hypoxie : hoechst - 33342 - fluoreszenz fehlt , pimonidazol in unmittelbarer gefnachbarschaft und ( 4 ) hypoxmische hypoxie : hoechst - 33342 - fluoreszenz und pimonidazol in direkter gefnachbarschaft . * presented in part at the 16th jahreskongress der deutschen gesellschaft fr radioonkologie ( degro ) , magdeburg , germany , 2010 . 1department of radiotherapy and radiation oncology , klinikum rechts der isar , technical university of munich , munich , germany . received : august 26 , 2010 ; accepted : october 13 , 2010 published online : march 24 , 2011 strahlenther onkol 2011 n0 . 
quantitative assessment of hypoxia subtypes in tumors ergebnisse : die verteilungsmuster von hoechst , pimonidazol und cd31 in den mcsus weisen darauf hin , dass in 4 der 5 tumorlinien normoxische areale berwiegen ( 50 , 172 , 8% )  . 
 schlsselwrter : tumorhypoxie akute hypoxie chronische hypoxie hypoxieformen diffusionslimitierte hypoxie perfusionslimitierte hypoxie mikrozirkulatorische versorgungseinheit introduction hypoxia is a characteristic feature of malignant solid tumors and is known to increase aggressiveness and acquired treatment resistance under certain pathophysiological conditions [ 25 , 26 , 29 , 31 ]  . 
considering treatment resistance , oxygen concentrations below 12% can lead to substantial limitations in the efficacy of oxygen - dependent treatment modalities , such as standard radiotherapy , some chemotherapy ( and combinations thereof ) , photodynamic therapy , and immunotherapy [ 28 ]  . according to the traditional classification used in experimental and clinical oncology , a distinction is made between two types of hypoxia : chronic and acute . 
in the case of a central microvessel , the supplied tumor volume resembles a truncated cone with continuously decreasing diffusion distances from the arterial to the venous end [ 12 ]  . 
in addition to this type of hypoxia , brown [ 6 ] has initiated awareness of the existence and possible importance of acute hypoxia for tumor biology and cancer therapy . 
according to these reports , acute hypoxia is mainly caused by temporary , local disturbances in perfusion or strong variations in red blood cell fluxes and , thus , in fluctuations of the microvascular oxygen supply ( perfusion - limited hypoxia )  . 
 in general , chronic hypoxia ( i.e. , hypoxia lasting longer than 2 hours ) leads to anti - proliferative effects , induces g1 arrest in the cell cycle and , in the additional absence of key nutrients , leads to death of normal and most tumor cells . 
 these opposing hypoxia - related responses and biological pathways are called the janus face of tumor hypoxia [ 26 , 27 , 30 ]  . upon acute hypoxia , a small fraction of tumor cells can escape hypoxia - induced cell damage by triggering ( transient ) changes in transcription , gene and protein expression favoring tumor progression ( via hypoxia - responsive processes at oxygen concentrations below 1% )  . 
at oxygen concentrations below 0.1% , malignant cells can undergo ( permanent ) genomic and epigenomic modifications for development of survival strategies of aggressive phenotypes [ 10 , 14 ]  . the pathophysiology and consequences of chronic and acute hypoxia and their various subtypes have been discussed in detail recently [ 2 , 3 ]  . 
in a series of experimental tumors , acute hypoxia has been described as the dominating type of oxygen depletion [ 13 , 20 , 22 ] , whereas in others , only low levels of acute hypoxia were detected [ 4 , 8 , 9 , 15 , 24 ]  . 
the evaluation of different hypoxia subtypes is based on the categorization of the oxygenation and perfusion status of individual microcirculatory supply units ( mcsus ) in vital tissue of xenografted human squamous cell carcinomas ( hscc ) of the head and neck region . 
 material and methods tumor lines in this study , we have examined five xenografted human squamous cell carcinoma ( hscc ) lines of varying radiation resistance as assessed by tcd50 ( radiation dose in gy necessary to locally control 50% of tumors )  . 
information concerning the cell lines used ( ut - scc - 15 , ut - scc - 14 , fadu , sas , and utscc - 5 ) , the mouse tumor model , local tumor control assays , and pimonidazole and hoechst 33342 injection has been described in detail previously [ 18 , 32 , 34 , 35 ]  . 
at 100 mg / kg body weight in a volume of 0.1 ml saline 1 hour before tumor excision , and the perfusion marker hoechst 33342 ( sigma , deisenhofen , germany ) was given i.v. 
 pimonidazole was stained with the mab fitc - labeled anti - pimonidazole antibody ( hypoxyprobe , burlington , ma , usa ) diluted 1 : 50 in primary antibody diluent ( pad , serotec , oxford , u.k. ) by incubating for 1 hour at 37c in the dark [ 1 , 17 ]  . 
anti - cd31 was detected using the secondary antibody , alexafluor 594 ( invitrogen , eugene , or , usa ) diluted 1 : 200 in pbs for 1 hour at 37 c in the dark . 
 necrotic areas were detected by staining serial slices with hematoxylin and eosin and excluded from subsequent analyses . microcirculatory supply units for quantification of ( immuno - ) fluorescence staining , we counted the total number of microcirculatory supply units ( mcsus ) in individual whole tumor cross - sections . 
the pictures obtained were visually evaluated by two independent researchers ( cb , cm ) by categorizing mcsus according to their perfusion and oxygenation status ( see figure 1 )  . 
 on average , 207 mcsus were analyzed per whole tumor cross - section for ut - scc - 15 tumors , 404 for ut - scc - 14 tumors , 529 for fadu tumors , 300 for sas tumors , and 411 for ut - scc - 5 tumors . 
 analysis of whole tumor cryosections revealed the following four immanent mcsu patterns : ( 1 ) tumor normoxia : hoechst 33342 fluorescence around a microvessel and no pimonidazole staining ( figure 1a ) ; ( 2 ) diffusion - limited hypoxia : hoechst 33342 fluorescence around a microvessel , pimonidazole staining in areas distant from a microvessel ( 100 m ; figure 1b ) ; ( 3 ) acute perfusion stop : no hoechst 33342 fluorescence around a microvessel and pimonidazole staining in immediate vicinity of a microvessel ( figure 1c ) , and ( 4 ) acute / chronic hypoxemic hypoxia : hoechst 33342 fluorescence and pimonidazole staining directly surrounding a microvessel ( figure 1d )  . statistical analyses statistical analyses were performed using the statistical package for social sciences ( spss , chicago , il )  . 
sketches representing the four microcirculatory supply units ( mcsus ) : tumor normoxia ( a ) ; ( chronic ) diffusion - limited hypoxia ( b ) ; ( acute ) perfusion - limited hypoxia ( c ) ; ( acute / chronic ) hypoxemic hypoxia ( d )  . 
schematische darstellung der 4 mikrozirkulatorischen versorgungseinheiten ( mcsus ) : tumor - normoxie ( a ) : chronische , diffusionslimitierte hypoxie ( b ) ; akute , perfusionslimitierte hypoxie ( c ) ; ( akute / chronische ) hypoxmische hypoxie ( d )  . 
representative tissue sections showing examples of the four mcsus as suggested in figure 1 : tumor normoxia ( a ) ; ( chronic ) diffusion - limited hypoxia ( b ) ; ( acute ) perfusion - limited hypoxia ( c ) ; ( acute / chronic ) hypoxemic hypoxia ( d )  . 
pfmcsu : anteil perfundierter gefe in mikrozirkulatorischen versorgungseinheiten ( diese studie ) ; pf : errechneter anteil perfundierter gefe auf der grundlage von quantitativen digitalen analysen [ 33 ] ; phf : ermittelter hypoxieanteil anhand von pimonidazol - frbungen [ 33 ] ; tcd50 : strahlendosis in gy , die bentigt wird , um 50% aller tumoren lokal zu kontrollieren [ 33 ]  . tcd50 ( gy ) 37.7 ( 14 ; 49 ) 44.2 ( 35 ; 49 ) 61.5 ( 30 ; 53 ) 99.1 ( 91 ; 108 ) 101.8 ( 88 ; 117 ) by these authors [ 33 ]  . 
in addition , there was a positive correlation between the fraction of acute hypoxia assessed in our experiments and phf data ( p = 0.035 ) and a trend for a correlation between the fraction of chronic hypoxia in our study and phf values . 
considering the fact that pimonidazole detects chronic hypoxia more efficiently than acute hyp oxia , it is surprising that acute hypoxia contributes most to the correlation between total hypoxia and phf . 
one reason for this may be that our determination of chronic hypoxia is based on the indirect quantification of microvessels in the vicinity of pimonidazole stained regions , whereas acutely hypoxic microvessels are directly surrounded by pimonidazole staining . 
therefore , the mcsu approach is a valuable tool to estimate not only the total hypoxic fraction , but also allows the identification of hypoxia subtypes . comparison of our data ( fraction of normoxia , total hypoxia , subtypes of hypoxia , and pf ) with tcd50 data published by yaromina et al . 
surprisingly , in our experiments , the tumor line with the lowest tcd50 value ( ut - scc - 15 ) is the most hypoxic and the tumor line with the highest tcd50 value ( ut - scc - 5 ) is only moderately hypoxic ( total hypoxia )  . of all the hypoxic subtypes , only chronic hypoxia showed a weak correlation with tcd50 . 
 [ 34 ] investigated the same tumor lines using hoechst 33342 fluorescence , pimonidazole , and cd31 staining , and quantitative digital analysis to calculate the fraction of perfused vessels ( pf ) and pimonidazole hypoxic fraction ( phf )  . 
in addition , only a twodimensional aspect of a small tissue volume at a certain point in time is evaluated , despite the fact that pronounced spatial and temporal heterogeneity of the parameters assessed is a characteristic feature of malignant tumors , both on a microscopic and macroscopic scale . 
 analysis of microcirculatory supply units ( mcsus ) enables the assessment of hypoxemic hypoxia , may assist in recognition of different hypoxia subtypes and may facilitate the application of methods to ( clinically ) identify and eliminate hypoxia . 
furthermore , quantification of hypoxia subtypes in mcsus could be a useful addition to other technologies , which are only valid for the detection of total hypoxia [ e.g. , 5 , 16 ] and when oxygen measurements in necrotic tissue areas need to be excluded . acknowledgments this study has been supported in part by grants of the deutsche forschungsgemeinschaft ( dfg : ba 3514 / 1 - 1 ) , the bundesministerium fr bildung und forschung ( bmbf : 01ez0826 ) , and the deutsche krebshilfe ( 106758 )  . 
baumann for providing tumor cryosections . original article small interfering rna targeting hif - 1 reduces hypoxia - dependent transcription and radiosensitizes hypoxic ht 1080 human fibrosarcoma cells in vitro adrian staab1 , 5 , markus fleischer1 , 2 , juergen loeffler2 , harun m . 
said1 , astrid katzer1 , christian plathow3 , herrmann einsele2 , michael flentje1 , dirk vordermark1 , 4 background : hypoxia inducible factor - 1 has been identified as a potential target to overcome hypoxia - induced radioresistance the aim of the present study was to investigate whether selective hif - 1 inhibition via small interfering rna ( sirna ) targeting hypoxia - inducible factor 1 ( hif - 1 ) affects hypoxia - induced radioresistance in ht 1080 human fibrosarcoma cells . material and methods : hif - 1 expression in ht 1080 human fibrosarcoma cells in vitro was silenced using hif - 1 sirna sequence primers . 
cells were assayed for clonogenic survival after irradiation with 2 , 5 , or 10 gy , under normoxic or hypoxic conditions in the presence of hif - 1 - targeted or control sirna sequences . 
oer was obtained at cell survival levels of 50% , 37% , and 10% . results : hif - 1 - targeted sirna enhanced radiation treatment efficacy under severely hypoxic conditions compared to tumor cells treated with scrambled control sirna . 
oer was reduced on all survival levels after treatment with hif - 1 - targeted sirna , suggesting that inhibition of hif - 1 activation by using hif - 1 - targeted sirna increases radiosensitivity of hypoxic tumor cells in vitro . conclusion : inhibition of hif - 1 activation by using hif - 1 - targeted sirna clearly acts synergistically with radiotherapy and increase radiosensitivity of hypoxic cells in vitro . key words : hypoxia inducible factor - 1 small interfering rna hypoxia radiation oxygen strahlenther onkol 2011 ; 187 : 2529 doi 10.1007 / s00066 - 011 - 2167 - 0 hypoxia - inducible - factor - 1 - small - interfering - rna inhibiert die hypoxische akkumulation von hif - 1 und erhht die strahlensensitivitt von ht - 1080 - fibrosarkomzellen in vitro hintergrund und ziel : hypoxia - inducible factor - 1 ( hif - 1 ) wurde als potentielles therapeutisches target identifiziert . 
ziel der arbeit war es , zu untersuchen , ob die selektive hif - 1 - inhibition mittels small interfering rna ( sirna ) gegen hif - 1 die strahlensensibilitt von hypoxischen ht - 1080 - zellen beeinflussen kann . material und methodik : die hif - 1 - expression in humanen ht - 1080 - fibrosarkomzellen wurde mittels rna - interferenz nach transfektion der zellen mit sirna unter hypoxischen bedingungen ( 0 , 1% o2 , 12 h ) , bzw . 
das klonogene berleben wurde nach bestrahlung unter hypoxie und normoxie bestimmt und daraus eine oxygen enhancement ratio ( oer ) bei den berlebensniveaus 50% , 37% and 10% berechnet . resultate : hif - 1 - sirna erhht die strahlensensibilitt unter hypoxischen bedingen , verglichen mit ht - 1080 - zellen , die mit kontroll - sirna behandelt wurden . 
die oer` war bei allen berlebensniveaus reduziert . schlussfolgerung : eine selektive inhibition der hif - 1 - aktivierung durch hif - 1 - sirna wirkt synergistisch mit einer bestrahlung und erhht die strahlensensitivitt hypoxischer tumorzellen in vitro . schlsselwrter : hypoxia - inducible factor - 1 small interfering rna hypoxie bestrahlung sauerstoff 1department of radiation oncology , university of wrzburg , germany , 2medical clinic ii , university of wrzburg , germany , 3department of nuclear medicine , university of freiburg , germany , 4department of radiation oncology , martin luther university halle - wittenberg , germany , 5paul scherrer institute , villigen , switzerland . received : april 26 , 2010 ; accepted : january 24 , 2011 published online : march 25 , 2011 strahlenther onkol 2011 n0 . 
hypoxic radiosensitization by hif - 1 - targeted sirna background hypoxia is a common feature of solid tumors that profoundly affects the biological behavior , response to therapy , and prognosis of human cancers [ 10 , 31 ]  . 
despite of improvements in chemoand radiotherapy , long - term prognosis is still poor for many patients with newly diagnosed or recurrent cancer diseases [ 3 , 28 , 36 , 38 ]  . several reports have demonstrated an increased chemoresistance [ 4 , 5 ] and radioresistance [ 21 ] in hypoxic tumor cells resulting from activation of the hypoxia - inducible factor - 1 ( hif - 1 ) pathway . 
the hif - 1 system is a key regulator of a broad range of cellular and systemic responses to hypoxia and acts in all mammalian cells . the transcription factor hif - 1 is a heterodimer formed by the association of an oxygen - regulated hif - 1 subunit with a constitutively expressed hif - 1 subunit [ 22 , 34 ]  . 
 under hypoxic conditions , the rates of hydroxylation and ubiquitination decline , resulting in an accumulation of hif - 1 [ 7 ]  . associations between high levels of protein expression of hif - 1 in tumor tissues [ 30 ] and poor prognosis have been shown in patients with breast cancer [ 29 ] , head and neck cancer [ 1 , 14 ] cervical cancer [ 6 ] , esophagus [ 20 ] , stomach [ 9 ] , and non - small cell lung cancer [ 17 ]  . 
however , this approach was impaired by relevant cytotoxicity of the agent and a rather unspecific action of the compound inhibiting the interaction of hif - 1 and the transcriptional coactivator p300 [ 25 ]  . 
the aim of the present study was to investigate if selective hif - 1 inhibition by using small interfering rna ( sirna ) targeting hif - 1a affects hypoxiainduced radioresistance in human tumor cells . material and methods cell culture early - passage ht 1080 human fibrosarcoma cells from the american type culture collection ( atcc , rockville , md ) were maintained under standard conditions as previously described [ 32 ]  . 
on the following day , when the cells were still in the exponential growth phase , they were transferred without further medium change to a ruskinn ( cincinnati , oh , usa ) invivo2 hypoxic workstation for hypoxia treatment . 
the oxygen concentration of 0.1% was achieved inside the workstation before transferring the cells by calibrating the oxygen probe against air according to the manufacturers instructions ; adjusting the instrument settings to the desired o2 concentration , 5% co2 and 37c ; and subsequent flooding of the chamber with an appropriate gas mixture of pressurized air , n2 , and co2 through an automated gas mixing module . 
the design of the constructs and their application as a reporter system of tumor hypoxia has been previously reported [ 23 ]  . cells were exposed to experimental conditions as for pcr experiments in glass petri dishes . 
due to the known requirement of sufficient reoxygenation for the development of hypoxia - dependent , hre - mediated egfp fluorescence , all samples were returned to aerobic conditions in the incubator for 4hours before facs analysis as previously described [ 32 ]  . 
genotyping was performed by melting curve analysis : 50 c for 15 s , followed by a temperature increase from 50 c to 95 c ( 0.2 c / s ) with continuous fluorescence recording on channel f1 . 
amplification was carried out by using the faststart master hybridization probes kit ( roche diagnostics ) with the following parameters : 95 c for 9 s , 55 c for 15 s , 72 c for 20 s . 
cells under hypoxia , stimulated with hif - 1targeted or control sirna , were compared with the control sample . small interfering rna ( sirna ) treatment and transfection approximately 1.0 106 ht - 1080 carcinoma cells were gently resuspended in 100 l mem at room temperature . 
a protein expression analysis , gene expression analysis , facs analysis and in vitro clonogenic assay were all performed 16 hours after sirna transfection . hif - 1 expression was silenced using designed hif - 1 sirna sequence primers ( qiagen , hilden , germany ) that were transfected into ht 1080 cells according to the manufacturers instructions . 
cells were irradiated with a dose of 2 , 5 , or 10 gy ( dose rate 2.5gy / min , 6 mv photons , room temperature , adequate perspex bolus )  . 
the survival data were fitted with the linear - quadratic model : s ( d ) = exp [ ( d + d2 ) ] by optimizing variable parameters and [ 10 ]  . 
a modified oxygen enhancement ratio ( oer ' ) was calculated as the ratio of the doses to achieve the same survival at 0.1% o2 as at ambient oxygen tensions : oer = dhypoxia / dnormoxia . 
oer was obtained at cell survival levels of 50% , 37% , and 10% . western blot analysis at the end of the 16 - hour in vitro treatment under different conditions , petri dishes were immediately placed on ice . 
for quantification of hif - 1 protein content , the ratio of hif - 1 and - tubulin band densities of a control sample transfected with scrambled control sirna under hypoxic conditions ( 0.1% o2 , 12 hours ) ht 1080 cells , aliquots of which were run with each blot , were defined as 100% and used as a reference for quantification . 
means standard deviations ( sd ) were calculated for each condition . statistical analysis expression levels of mrna and clonogenic survival were compared between treatment groups by mann - whitney u test using statistica vs . 
expression of hif - 1a mrna was measured 16 hours after transfection of ht 1080 tumor cells with hif - 1a - targeted sirna ( sirna3 and sirna4 ) or scrambled control sirna ( nsrna )  . 
die hif - 1a - mrnaexpression wurde bestimmmt 16 stunden nach transfektion der ht1080 - tumorzellen mit hif - 1a - targeted sirna ( sirna3 and sirna4 ) oder kontrol sirna ( nsrna )  . 
ht 1080 human fibrosarcoma cells were pre - treated with 133 nm small interfering rna for 4 hours and transferred for 12 hours to hypoxic ( 0.1% o2 ) or maintained in aerobic ( 20% o2 ) conditions.transfection ht 1080 cells with hif - 1a - targeted sirna ( sirna3 and sirna4 ) inhibits the hypoxic activation of hre - mediated egfp fluorescence in stably transfected ht 1080 human fibrosarcoma cells . 
humane hat - 1080 - fibrosarkom - zellen wurden 4 stunden lang mit 133 nm small interfering rna vorbehandelt und anschlieend 12 stunden lang unter hypoxischen ( 0 , 1% o2 ) bzw . 
 transfektion der hat - 1080 - zellen mit hif - 1a - targeted sirna ( sirna3 and sirna4 ) inhibiert die hypoxische aktivierung des hif - 1 - regulierten promotors und green fluorescent protein ( gfp ) als marker ( 5hre - gfp ) in stabil transfizierten humanen ht - 1080 - fibrosarkomzellen . 
control cells or cells transfected with either scrambled control sirna ( nsrna ) or hif - 1targeted sirna ( sirna3 and sirna4 ) showed only basal egfp fluorescence below 15% under aerobic conditions compared to the hypoxic control ( 100% )  . down - regulation of hif - 1 protein in ht 1080 cells by small interfering rna under normoxic conditions , low basal expression of hif - 1 protein was measured . 
effects of treatment with in vitro hypoxia ( 0.1% o2 ) and / or hif - 1a - targeted sirna ( sirna3 and sirna4 ) or scrambled control sirna ( nsrna ) on the survival fraction ( sf ) of ht 1080 human fibrosarcoma cells . 
der einfluss von hypoxie in vitro ( 01% o2 ) und / oder hif - 1a - targeted sirna ( sirna3 und sirna4 ) oder kontroll - sirna ( nsrna ) auf die survival fraction ( sf ) von humanen hat - 1080 - fibrosarkomzellen . 
hif - 1 - targeted sirna ( sirna3 and sirna4 ) enhanced significantly radiation treatment efficacy under severely hypoxic conditions compared to tumor cells treated with scrambled control sirna ( ns sirna ) ( figure 6 , table 1 )  . oer was calculated at 50% , 37% , and 10% survival levels obtained from calculated and values . 
the reduction of oer values was significant on all survival levels after treatment with hif - 1 - targeted sirna ( sirna3 and sirna4 ) , except for the survival level 10% after incubation with sirna4 ( table 2 )  . discussion hif - 1 inhibition has been shown to slow tumor growth in in vitro and in vivo tumor models [ 16 , 39 ] and to act synergistically with other treatment modalities such as radiotherapy [ 25 ]  . 
ht 1080 human fibrosarcoma cells were pre - treated with 133 nm small interfering rna for 4 hours and transferred for 12 hours to hypoxic ( 0.1% o2 ) or maintained in aerobic ( 20% o2 ) conditions . 
humane hat - 1080 - fibrosarkom - zellen wurden 4 stunden lang mit 133 nm small interfering rna vorbehandelt und anschlieend 12 stunden lang unter hypoxischen ( 0 , 1% o2 ) bzw . 
mit kontroll - sirna transfizierte hypoxische hat - 1080 - zellen , wurden als 100% definiert und als referenz zur quantifikation verwendet ( a mittelwert se , n = 5 , * signifikanter unterschied p < 0 , 05 )  . 
clonogenic survival of ht 1080 human fibrosarcoma cells after radiation treatment in air ( 20% o2 ) : ht 1080 cells were transfected with scrambled control sirna ( nsrna ) 16 hours prior radiation treatment ( n = 3 , mean sem )  . 
klonogene berleben in humanen hat - 1080 - fibrosarkomzellen nach behandlung der zellen mit / ohne kontroll - sirna ( nsrna ) unter normoxischen bedingungen ( 20% o2 )  . 
we could demonstrate that knockdown of hypoxia - induced expression of hif - 1 with rna interference increased radiosensitivity of hypoxic cells and strongly suppressed hif - 1 m - rna expression compared to untreated human fibrosarcoma cells or ht 1080 cells treated with scrambled control sirna . the calculated modified oxygen enhancement ratio ( oer ) values were reduced after incubation with chetomin figure 6a and 6b . 
clonogenic survival after treatment with hif - 1atargeted sirna under normoxic and hypoxic conditions in ht 1080 huht 1080 huunder normoxic and hypoxic conditions in ht 1080 human fibrosarcoma cells . 
clonogenic survival of ht 1080 human fibrosarcoma cells after radiation treatment in air ( 20% o2 ) or hypoxia ( 0.1% o2 ) : ht108 cells were transfected with hif - 1a - targeted sirna ( a sirna3 , b sirna4 ) or scrambled control sirna ( nsrna ) 4 hours prior to hypoxia ( n = 3 , mean sem )  . 
ht 1080 cells were cultured for 12 hours under hypoxia / normoxia and in the presence of 133 nm hif - 1a - targeted sirna ( sirna3 and sirna4 ) or scrambled control sirna ( nsrna )  . 
hat - 1080 - zellen wurden 4 stunden lang mit hif - 1atargeted sirna ( a sirna3 , b sirna4 ) und kontroll - sirna ( nsrna ) vorbehandelt und anschlieend 12 stunden lang unter hypoxischen ( 0 , 1% o2 ) bzw . 
survival fraction ( sf ) after irradiation at oxygen concentrations of 20% ( air ) or 0.1% ( hypoxia = hyp ) following treatment with hif - 1atargeted sirna ( sirna3 and sirna4 ) or scrambled control sirna ( nsrna )  . 
survival fraction ( sf ) nach bestrahlung mit verschieden sauerstoffkonzentrationen ( 20% [ air ] oder 0.1% [ hypoxia = hyp ] ) und transfektion mit hif - 1a - targeted sirna ( sirna3 und sirna4 )  . 
modified oxygen enhancement ratio ( oer ) derived from clonogenic survival curves after irradiation at oxygen concentrations of 20% ( air ) or 0.1% ( hypoxia = hyp ) following treatment with hif - 1a - targeted sirna ( sirna3 and sirna4 ) where indicated . 
eine modifizierte oxygen enhancement ratio ( oer ) wurde abgeleitet aus den berlebenskurven nach bestrahlung mit verschieden sauerstoffkonzentrationen ( 20% [ air ] oder 0.1% [ hypoxia = hyp ] ) und transfektion mit hif - 1a - targeted sirna ( sirna3 und sirna4 )  . 
taken together , hif - 1 - targeted sirna and chetomin effectively radiosensitize hypoxic ht 1080 cells , whereas the radiosensitivity of normoxic cells remains unaffected [ 25 ]  . 
further experiments are necessary to understand completely the molecular aspects of hypoxia - induced radioresistance and the role of the hif - 1 pathway . nevertheless , these results indicate that selective inhibiton of the hypoxic hif - 1 pathway by downregulation of hif1protein via hif - 1 - targeted sirna treatment is as effective as treatment with chetomin as a small molecule blocking the hif pathway . 
in contrast hif - 1 - targeted sirna had no cytotoxic effect in aerobic or hypoxic ht 1080 cells in the clonogenic assay compared with untreated ht 1080 cells or cells transfected with scrambled control sirna . one explanation for the apparently more specific action of the sirna approach is the chetomin - induced disruption of the interaction of hif - 1 with the transcriptional coactivator p300 as a mechanism of action . 
 [ 39 ] could demonstrate that suppression of hif - 1 by using small interfering rna ( sirna ) results in a decrease of cell proliferation and increase of chemosensitivity of pancreatic cancer cells in vitro and in vivo . 
rna interference ( rnai ) of hif - 1 is an effective strategy for inhibiting tumor cell growth , and both tumor and normal cells can be the target for rnai - based anticancer treatment [ 27 ]  . 
furthermore hif - 1 is an important component of the apoptotic signaling machinery and selective ablation of hif - 1 protein expression by rna interference led to a reduction of caspase - 3 activity and reduction in the number of apoptotic cells after hypoxia [ 19 ]  . the success of hif - 1 inhibition in vivo depends on other factors of the tumor microenvironment such as glucose metabolism and ph [ 24 , 26 ] and potentially on the ability of a strategy to eliminate virtually all hif - 1 function as cell mixing experiments described by williams et al . 
hypoxic radiosensitization by hif - 1 - targeted sirna conclusion our results indicate that the selective inhibition of hif - 1 activation by using hif - 1 - targeted sirna treatment reduces hypoxic radioresistance in vitro as effectively as a pharmacologic approach with chetomin as a small molecule blocking the hif pathway . 
pharmacological therapeutics targeting pathognomonic changes in cancer cells are potential canidatates for clinical use in cancer therapy and using sirna to reduce hif - 1 levels in tumors may be of interest as a clinical treatment option in selected tumor entities . acknowledgment this work was supported in part by a grant from the deutsche forschungsgemeinschaft ( vo 871 / 23 ) to dv . 
 original article stereotactic body radiation therapy ( sbrt ) for adrenal metastases a feasibility study of advanced techniques with modulated photons and protons marta scorsetti1 , pietro mancosu1 , piera navarria1 , angelo tozzi1 , simona castiglioni1 , elena clerici1 , giacomo reggiori1 , francesca lobefalo1 , antonella fogliata2 , luca cozzi2 purpose : to compare advanced treatment techniques with photons and protons as a stereotactic body radiation therapy ( sbrt ) for adrenal glands metastases . materials and methods : planning computer tomographic ( ct ) scans of 10patients were selected . 
the main planning objective for the clinical target volume ( ctv ) was to cover 100% of the volume with 95% ( v95% = 100% ) and to keep the maximum dose below 107% of the prescribed dose ( v107% = 0% )  . 
for kidneys , the general planning objective was v15gy < 35% and for liver v15gy < ( liver volume700cm3 )  . results : all techniques achieved the minimum and maximum dose objective for ctv and ptv , d595% ranged from 1gy ( protons ) to 1.6gy ( conformal static fields ) on ctv . 
rapidarc presented the second lowest dose bath ( v10gy and integral dose ) after protons and the best conformality together with imrt . conclusions : stereotactic body radiation therapy ( sbrt ) to adrenal glands metastases is achievable with several advanced techniques with either photons or protons . 
die planungsvorgaben fr das ctv war die 100%ige abdeckung des volumens mit 95% der verschreibungsdosis ( v95% = 100% ) und die einhaltung einer maximalen dosis unterhalb von 107% der verschreibungsdosis ( v107% = 0% )  . 
 die planungsvorgabe fr das ptv war v95% > 80% . , fr die nieren v15gy < 35% und fr die leber v15gy < ( lebervolumen700cm3 )  . ergebnisse : alle bestrahlungstechniken erfllten die minimalen und maximalen dosisvorgaben fr das ctv und das ptv . 
die rapidarc - technik zeigte das zweitniedrigste dosisbad ( v10gy und integrale dosis ) nach den protonen und die beste konformitt zusammen mit der imrt - technik schlussfolgerung : die stereotaktische krperbestrahlungstherapie von metastasen in nebennieren ist mit mehreren fortgeschrittenen bestrahlungstechniken mit photonen oder protonen durchfhrbar . 
die intensittsmodulierten methoden , entweder 1department of radiation oncology , istituto clinico humanitas , rozzano - milan , italy , 2medical physics unit , oncology institute of southern switzerland , bellinzona , switzerland . received : august 5 , 2010 ; accepted : january 17 , 2011 published online : march 25 , 2011 strahlenther onkol 2011 n0 . 
dank ihrer einfachheit sollte die imrtoder die rapidarc - technik als erste option bei der bestrahlung von patienten , welche fr eine protonenbehandlung nicht in frage kommen , bercksichtigt werden . 
 the ctvptv ( clinical target volumeplanning target volume ) margin was 6mm in the cranialcaudal axis and 3mm in the anteriorposterior and lateral axes , allowing for residual intrafraction organ motion and for inaccuracies in image interpretation . 
 the main planning objective for ctv was to cover 100% of the volume with 95% of the prescribed dose ( v95% = 100% ) and to keep the maximum dose below 107% of the prescribed dose ( v107% = 0% )  . 
when detected , radiation therapy is generally adopted in case of palliative treatments aiming to pain control [ 15 , 16 , 20 , 23 , 24 , 31 , 33 ]  . 
advanced technology with improved immobilization and imaging modalities has enabled effective radiation treatment of thoracic , liver , pancreatic , renal tumors , and abdominal metastases [ 4 , 69 , 12 , 18 , 19 , 21 , 25 , 26 ] concerning the treatment of adrenal glands , chawla et al . 
volumetric modulated arc therapy [ 22 ] was also investigated and it has showed great potential in terms of increased delivery efficiency and further reduction of healthy tissue involvement [ 1 , 9 , 10 , 13 , 2830 , 32 ]  . at the istituto clinico humanitas ( ich ) , patients with solitary or oligometastases have been treated with sbrt techniques , using either static conformal fields or dynamic conformal arcs . 
in general , rapidarc allowed us to fulfill this prescription , while with previously adopted techniques , total dose was frequently downscaled about 1020% to meet the dose limits to organs at risk [ 2 ]  . 
 the present study aimed to assess the potential role of a variety of approaches : conformal static fields ( 3dc ) , dynamic conformal arcs ( dca ) , fixed gantry imrt ( imrt ) , rapidarc ( ra ) with photons , and intensity modulated protons with spot scanning ( impt )  . the objective of the study was to assess for each modality : ( 1 ) target coverfigure 1 . 
mittlere dosis - volumen - histogramme fr ctv , ptv , risikoorgane und gesundes gewebe . the general planning objectives were to minimize contralateral organ involvement for the ipsilateral kidney v15gy < 35% and for ipsilateral liver v15gy < ( liver volume700cm3 )  . 
plans were normalized to mean ptv dose . planning techniques for each patient , all photon plans were designed and optimized for a varian clinac 2100cd equipped with a millennium mlc ( 120leaves and a spatial resolution of 5mm at the isocenter in the target region )  . 
proton plans were optimized on for a generic machine with spot scanning using the same calculation grid as for photons . 3d conformal static fields ( 3dc ) in accordance with ichs clinical protocols , 3d conformal plans were designed using fivefixed gantry beams with or without wedges . 
for all fields , a margin of 5mm was applied from ptv to mlc leaves in the x - direction ( in - plane ) and of 8mm in the y - direction ( cross - plane )  . dynamic conformal arcs ( dca ) plans were designed with fiveconformal arcs , each of 30 . 
for all arcs , the same margins for the mlc leaves with respect to the ptv were applied as for the 3dc plans . intensity - modulated fixed gantry fields ( imrt ) plans were designed according to the dynamic sliding window method with fixed gantry beams . 
five beams with fixed jaws settings were applied ; gantry angles were optimized with the automatic beam geometry optimizer implemented in the eclipse planning systea minimum gantry separation angle of 30 was imposed . 
to minimize the number of mu , a high smoothing factor ~300 ( x - smooth and y - smooth parameters ) of the same order of magnitude of the priorities used for dosevolume objectives was applied . rapidarc ( ra ) plans were optimized using the proii algorithm for two partial arcs with a single isocenter . 
details on rapidarc optimization process have been published elsewhere by our group [ 1 , 5 , 10 , 22 , 29 ]  . proton fields ( impt ) for intensity modulated proton plans , the process consisted of the simultaneous optimization of the weight of each spot inside a point cloud describing oar and targets [ 17 , 27 ]  . 
optimization of the weight values for the spots was performed starting from a dose deposition coefficient matrix which was calculated as the dose that would be deposited in each of the cloud points when irradiating each single spot of the initial list with a unit intensity . 
 spot spacing was set to 3 mm , circular lateral target margins were set to 5mm , the proximal margin to 5mm , and the distal margin to 2mln all cases , a two - beam arrangement was adopted ; both beams had an incidence almost normal to the skin surface and were separated by about 100 . tools for analysis quantitative evaluation was performed by means of standard dosevolume histograms ( dvhs )  . 
for ptv and ctv , the values of d99% and d1% ( dose received by the 99% and 1% of the volume , respectively ) were defined and reported as an estimation of the minimum and the maximum dose , respectively . 
the conformality of the plans was measured using the conformity index ( ci95% ) defined as the ratio between the patient volume receiving at least 95% of the prescribed dose and the volume of the ptv . 
 the highest dose homogeneity in ptv , d595% , was observed for the impt plans . conformality , due to the small absolute volumes involved , is relatively poor with all techniques showing a ci95% > 2 . 
 rapidarc plan results were slightly better than other photon - based techniques . ipsilateral organs were irradiated similarly by rapidarc and imrt plans , at a level intermediate between the best ( impt ) and the worst ( 3dc and dca )  . 
 data confirmed that conformal approaches are intrinsically less efficient in achieving concomitant high target coverage and oar sparing . the average cumulative dvh for ptv , oar , and healthy tissue were constructed from the individual dvhs with a dose binning of 0.02gy. 
mu were reported for a calibration of 1gy for 100mu for a 1010cm2 field at 10cm depth and ssd = 90cthe wilcoxon matchedpaired signed - rank test was used to compare the results . 
in the tables , the statistical difference between pairs of techniques are indicated . results dose distributions for an example patient are shown in figure1 for axial , coronal , and sagittal views . 
mu / gy for ra was ~25% lower than the corresponding value for imrt and about 22% higher than the corresponding average of the unmodulated techniques . discussion the present planning study was performed to investigate the role of vmat , imrt with fixed gantry fields , and impt in comparison with conventional conformal techniques in patients affected by adrenal gland metastases . 
 cone beam ct ( cbct ) image guidance proved effective in monitoring the correct positioning and appraising daily shifts from the baseline , reducing the risk of missing the target . 
 on the other hand , for photons , the small size of the targets and the relatively limited modulation of the fields or arcs , suggested a potentially limited impact . 
 rapidarc might be a candidate for minimal impact since , rotating of the gantry around the body , the weight of the uncertainty is averaged over each control point . concerning the primary objectives of the study , all photon - based techniques ( 1 ) proved capable of respecting planning objectives on ctv and ptv , ( 2 ) largely respected dose constraints to the organs at risk , ( 3 ) maintained dose bath to healthy tissue at comparable levels . 
in addition , impt plans reduced the involvement of contralateral organs to virtually zero as well as reduced not only the integral dose by a factor of 2 to 3 but also the mean dose to healthy tissue . the low involvement of organs at risk , compared to dose volume constraints , might also suggest the possibility of exploring dose escalation protocols over the 45gy . 
in addition , when considering the proven [ 3 ] tendency of these patients to develop new metastases shortly after treatment and to locally progress with their diseases , sbrt might be considered . 
total treatment efficiency , in terms of time , was completely dominated here by the number of fields ( 5 for 3dc , dca , and imrt vs 2 for ra ) which leads to a time gain of a factor ~3 for ra ( including the dead time needed to reset the beam between one field and the next and neglecting the positioning and igrt time )  . 
rapidarc and imrt produced high level target coverage comparable to protons and , in terms of conformal avoidance , improved quality of treatment compared to the other techniques based on conformal fields with photons . 
hypofractionated sbrt of metastases of adrenal gland is , therefore , promising and intensity modulation might be preferable to other conventional techniques . original article adenocarcinoma of the esophagogastric junction : neoadjuvant radiochemotherapy and radical surgery early results and toxicity bernhard j . 
grabenbauer2 , 4 purpose : to retrospectively evaluate treatment results and toxicity following a combined approach consisting of neoadjuvant radiochemotherapy and radical surgery in advanced adenocarcinoma of the esophagus and gastroesophageal junction . patients and methods : between 2005 and 2009 , a total of 41 consecutive patients with newly diagnosed nonmetastatic adenocarcinoma of the esophagus and the esophagogastric junction were evaluated , of whom 23 received neoadjuvant radiochemotherapy ( rct )  . 
reasons for no surgery included advanced age of 79 , 82 , and 86 years ( n = 3 ) , severe comorbidity ( n = 1 ) , and progression during radiochemotherapy ( n = 1 )  . 
out of a total of 18 patients , regression grading revealed < 10% viable cells in 8 ( 44% ) including 3 cases ( 17% ) with complete regression , 1050% viable cells in 9 ( 50% ) and > 50% viable cells in 1 patient . 
 v10 > 20% ( p = 0.019 ) , v15 > 13% ( p = 0.008 ) , and v20 > 10% ( p = 0.008 ) were associated with a significant increase in the rate of pulmonary toxic effects . conclusion : neoadjuvant radiochemotherapy in patients with advanced adenocarcinoma of the esophagogastric junction followed by thoracoabdominal surgery is a feasible concept . 
however , to avoid toxic pulmonary effects constraints for low - dose radiation volume parameters need specific attention . key words : adenocarcinoma esophagus gastroesophageal junction radiochemotherapy strahlenther onkol 2011 ; 187 : 2317 doi 10.1007 / s00066 - 011 - 2171 - 4 adenokarzinome des gastrosophagealen bergangs : neoadjuvante radiochemotherapie und resektion . 
 patienten und methode : von 2005 bis 2009 wurden insgesamt 41 patienten mit einem neu diagnostizierten , nicht metastasierten adenokarzinom des sophagus und des sophagogastralen bergangs diagnostiziert , von denen 23 eine neoadjuvante radiochemotherapie ( rct ) erhielten . 
es wurde eine gesamtdosis von 50 , 4 gy mit 2 zyklen einer simultanen cisplatin / fuor t axol / 1department of surgery , klinikum coburg , coburg , germany , 2department of radiation oncology , diacura coburg , coburg , germany , 3department of pathology , klinikum coburg , coburg , germany , 4coburg cancer center , coburg , germany . received : may 12 , 2010 ; accepted : december 13 , 2010 published online : march 24 , 2011 strahlenther onkol 2011 n0 . 
dosis - volumen - parameter der radiotherapie , wie die v10 , v15 und v20 , wurden mit der pulmonalen toxizitt korreliert . ergebnisse : die gesamtberlebensrate nach 3 jahren betrug 61% . 
die ursachen fr inoperabilitt waren : fortgeschrittenes alter von 79 , 82 and 86 jahren ( n = 3 ) , schwere komorbiditt ( n = 1 ) und progression whrend der radiochemotherapie ( n = 1 )  . 
das regressions - grading zeigte < 10% vitale zellen bei 8 / 18 ( 44% ) inklusive 3 patienten mit kompletter regression , 1050% vitale zellen bei 9 / 18 ( 50% ) und > 50% vitale zellen bei 1 / 18 patienten . 
werte von v10 > 20% ( p = 0 , 019 ) , v15 > 13% ( p = 0 , 008 ) and v20 > 10% ( p = 0 , 008 ) waren signifikante prdiktoren fr diese pulmonale toxizitt . schlussfolgerungen : die neoadjuvante radiochemotherapie beim adenokarzinom des sophagus und gastrosophagealen bergangs , gefolgt von einem thorakoabdominellen eingriff , ist ein durchfhrbares gesamtkonzept . 
a total of 23 patients were scheduled for aggressive radiochemotherapy , of whom another 3 had to be excluded from further treatment due to progression , severe comorbidity , and advanced age , respectively . 
patient selection is displayed in figure 1 leaving a total of 20 patients to form the study group ( table 1 )  . radiochemotherapy ( rct ) treatment planning was performed on the basis of spiral - ct data ( somatom 64 , siemens , forchheim , germany ) using 3 mm slice reconstruction . 
planning target volume ( ptv ) was defined as all gross tumor volume plus a 1.5 cm circumferential margin as well as a 3 cm and 5 cm longitudinal margin for the proximal and distal expansion , respectively . 
obesity , gastroesophageal reflux , and barretts metaplasia may be responsible for a rapid increase in the rate ratio of adenocarcinoma of this region over other cancers [ 9 , 11 ]  . 
the 5 - year survival rates for these cancers have remained less than 30% over decades [ 3 , 19 ] , probably because of ineffective therapies , such as incomplete surgery , with limited rates of r0 resection despite curative intention to treat [ 3 ]  . 
this low rate may be due to inadequate staging , the advanced stage at which this cancer is often diagnosed [ 2 , 4 , 25 ] , or the limited experience of the hospital or operating surgeon . 
however , treating patients who have stage ii or iii cancer with radiochemotherapy to achieve a clinically significant downstaging before surgeryand , thus , to create a greater likelihood of r0 resectionmay be possible . 
 preoperative radiochemotherapy has not been frequently used although several meta - analyses demonstrated a benefit for patients who received preoperative radiochemotherapy compared with patients who did not [ 6 , 17 , 29 ]  . 
the purpose of this paper is to give our initial experience with neoadjuvant radiochemotherapy followed by radical surgery in an unselected group of patients with adenocarcinoma of the esophagogastric junction . patients and methods between 2005 and 2009 , a total of 41 consecutive patients with newly diagnosed nonmetastatic adenocarcinoma of the esophagus and the esophagogastric junction were referred for figure 1 . 
patientencharakteristika. total patient number gender male female 4460 years 6170 7180 8186 t category t3 t4 n category n0 n + grading g1 / 2 g3 typing adenocarcinoma tumor site ( according to siewert ) type i type ii type iii 85 15 35 35 15 15 85 15 30 70 40 60 80 20 prescription was applied according to the icru 50 guidelines with single fractions of 1.8 gy and a total dose of 50.4 gy ( pinnacle , philips medical systems , eindhoven , the netherlands )  . 
 dose constraints for organs at risk included a v20gy ( i.e. , the percentage of lung volume receiving 20 gy ) of less than 20% for both lungs , and v25gy < 10% for the whole heart . 
 simultaneous chemotherapy was given according to standard procedures using bolus cisplatin ( 20 mg / m2 / day ) and infusional fluorouracil ( fu , 800 mg / m2 / day ) on days 15 and 2933 during radiotherapy . 
only in cases of inadequate renal function parameters ( creatinine clearance < 60 ml / minute ) or cardiac dysfunctions ( ejection fraction < 45% , coronary artery disease ) , simultaneous chemotherapy was performed according to the protocol given by ajani et al . 
the choice of the regimen was at the discretion of the attending physician . surgery all patients underwent laparoscopy for exclusion of possible peritoneal deposits and implantation of a central venous access device ( port - a - cath ) and a percutaneous , laparoscopically guided jejunostomy ( plj ) prior to initiation of rct . 
this was combined with a two - field lymphadenectomy of mediastinal and abdominal lymph nodes , including the nodes of the celiac trunk and along the upper border of the pancreas ( ivorlewis procedure )  . 
the anastomosis between the esophageal stump and gastric pull - up was performed by a running submucosal suture at the gastric wall and a running complete transmural suture ( 4 / 0 ) at the esophageal wall . 
in 17 of 20 cases ( in 1 patient only transhiatal approach with palliative intention due to local peritoneal spread ) , an en bloc esophagectomy with two field lymph node dissection was performed . 
two elderly patients ( 82 and 86 years old ) were regarded as inoperable due to congestive heart disease ( nyha 23 ) and a history of prior upper lobe resection ( lung cancer ) , respectively . 
standard histopathological evaluation included the application of regression grading according to werner and hfler [ 30 ] as well as meticulous sections of all resection margins and dissected lymph nodes . 
 follow - up and statistical analysis all patients were followed - up every 3 months during the first year ( later every 6 months ) for clinical examination and ct scans of the lungs , upper abdomen , and pelvis . 
data from individual dosevolume histograms of all 23 patients were used to explore a possible impact of v10 , v15 , and v20 on pulmonary toxicity including pneumonia / pneumonitis ( grade 35 , ctc )  . 
eight of 23 patients died during follow - up , 5 patients died secondary to tumor progression with pulmonary , bone , and peritoneal metastases at 3 , 9 , 10 , 12 , and 13 months after initial diagnosis . 
 another patient died of septicemia , while on postoperative chemotherapy and a third patient died of fungal pneumonia 7 months after initial diagnosis . local progression was noted in 1 patient in whom postoperative surgical margins were positive and , therefore , only a palliative resection could be performed due to peritoneal carcinomatosis . 
a total of 8 patients experienced distant metastases , 3 patient are currently alive , 1 with no evidence of disease after successful treatment of a single brain and cervical nodal metastases . 
 surgery and downstaging of the 23 patients , 18 underwent radical surgery after a median time interval of 50 days ( range , 3874 days ) following radiochemotherapy ( table 2 )  . 
a total of 11 surgical complications occurred in 9 patients , including superficial wound healing disorders ( n = 2 ) and anastomotic leakage , which was treated by stenting ( n = 2 )  . 
resurgery was necessary in 3 cases ( 18% ) : 1 patient had relaparotomy due to small bowel obstruction , and 2 patients had rethoracotomy for repair of a lymphatic fistula and for drainage of mediastinal abscess , respectively . 
in the same case , successful surgery of a single metastatic disease was performed and the patient is alive after 65 months ( figure 2 )  . pathologic examination of the resected specimen in a total of 18 patients revealed no residual tumor at the resection margin in 17 patients ( 94% ) and positive margins in 1 patient . 
as for the t category , 12 of 18 ( 67% ) patients initially diagnosed with t3 tumors and 3 of 3 patients with t4 tumors experienced downstaging ( table 4 )  . 
regression grading in a total of 18 patients revealed very good regression ( < 10% viable cells ) in 8 ( 44% ) patients , including 3 cases of complete regression , medium regression ( 1050% viable cells ) in 9 ( 50% ) patients , and minimal regression ( > 50% viable cells ) in 1 patient . nine of 13 patients ( 69% ) with clinical n + disease were found to have ypn0 status . 
table 5 gives the regression of nodal disease . total dose of radiotherapy ( icru 50 ) 4550 gy 5155 gy type of chemotherapy taxol / fu platin / fu acute toxicity ( grade 2 + 3 ) hematologic gastrointestinal type of surgery thoracoabdominal ( ivorlewis procedure ) thoracoabdominal with pulmonary resection thoracoabdominal with reconstruction of bronchus transhiatal resection vo surgery regression grading ( werner / hfler , 2000 ) - grade 1a / b ( < 10% viable cells ) - grade 2 ( 1050% viable cells ) - grade 3 ( > 50% viable cells ) table 3 . 
chirurgische komplikationen bei 18 patien ten nach radikaler chirurgie ( mehrfachnennungen mglich )  . type of surgical complication hiatal hernia ( bowel obstruction ) cardiac dysrhythmia lymphatic leakage recurrent nerve palsy anastomotic leakage with consecutive stenting wound healing disorder resurgery thoracic drainage mortality acute toxicity of radiochemotherapy rates of maximum hematologic toxicity for ctc grade 1 , 2 , and 3 were 48% , 38% , and 5% , respectively . 
dose and volume parameters for patients with ( n = 8 ) and without pulmonary toxicity ( n = 15 ) following full dose radiochemotherapy ( absolute values are gives as median )  . 
dosisund volumenparameter von patienten mit pulmonaler toxizitt ( n = 8 ) und ohne pulmonale toxizitt ( n = 15 ) nach volldosierter radiochemotherapie ( absolutwerte als median )  . 
v10 , v15 , v20 : bilate rale lungenvolumina , die 10 gy , 15 gy , and 20 gy erhielten ; pts : patienten . patients with pulmonary toxicity ( n = 8 ) patients without pulmonary toxicity ( n = 15 ) v10 ( absolute ) 1442 ml 20 % > 20% 1 / 8 pts 7 / 8 pts v15 ( absolute ) 874 ml 13 % > 13% 4 / 8 pts 7 / 8 pts v20 ( absolute ) 541 ml 10 % > 10% 4 / 8 pts 7 / 8 pts p = 0.019 ( fishers test ) 611 ml 10 / 15 pts 5 / 10 pts 351 ml 11 / 15 pts 1 / 15 pts 223 ml 11 / 15 pts 1 / 15 pts p = 0.008 ( fishers test ) p = 0.008 ( fishers test ) toxic effects following surgery and adjuvant chemotherapy during the postoperative course or thereafter , 8 of 23 ( 35% ) patients experienced pulmonary complications including pneumonia and / or pneumonitis . 
na : nicht verfgbar ( 2 patienten waren aus internistischen grnden nicht operabel )  . ypn category ypn0 ypn1 discussion n category total following surgery alone , the prognosis of patients with advanced adenocarcinoma of the esophagus and gastroesophageal junction has been very poor . 
in our series , the rate of resection with clear margins ( r0 ) was 94% and the ypn0 rate was 67% , which both correspond nicely to the data provided by the literature [ 1 , 27 ]  . 
indeed , as a result of several meta - analyses , neoadjuvant rct is considered the standard approach in patients with carcinoma of the esophagus and gastroesophageal junction [ 6 , 8 , 10 ]  . 
a recent phase iii trial that compared preoperative chemotherapy with rct in patients with locally advanced adenocarcinoma of the esophagogastric junction was able to demonstrate an improvement in the 3 - year survival rate from 27% ( preoperative chemotherapy ) to 47% following rct . 
patients receiving rct had a higher probability of having pathologic complete response ( 16% vs 2% ) and negative lymph nodes ( 64% vs 38% ) at resection [ 27 ]  . 
 however , in contrast to patients with squamous cell carcinoma , neoadjuvant rct of adenocarcinoma of the esophagus results in a limited pcr rate [ 4 , 13 ]  . 
thus , complete surgery is currently indispensable in the treatment of this disease . it has been the ongoing and continuing hypothesis that neoadjuvant rct followed by surgery may cause significantly higher postoperative morbidity and mortality rates as compared to surgery with or without neoadjuvant chemotherapy [ 2023 ]  . 
from our series , it would even appear to suggest unexpectedly tight low - dose constraints with a v10 20 ( 30 ) % , v15 13% , and v20 10% ! a recent analysis [ 7 ] from the m.d. 
the authors identified an age > 60 years ( rr : 11.3 ) and a body mass index of 26 kg / m2 ( rr : 4 ) as significant risk factors for overall complications [ 7 ]  . 
 another factor that might contribute to an increased pulmonary toxicity is the application of taxan - containing chemotherapy either as combined approach together with radiation or alone as induction chemotherapy prior to surgery . 
mccurdy and coworkers [ 18 ] demonstrated among a group of 139 patients that increasing doses of taxanes correlated significantly with the development of pneumonitis symptoms as well as with the fdgpet - based pulmonary metabolic radiation response . 
die obere kurve reprsentiert 12 patienten mit v10 > 20% , die untere kurve 11 patienten mit einer v10 20% . survival rates of only about 20% may be encountered as reported from the control arms of randomized , phase iii trials [ 5 , 29 ]  . 
 meta - analyses comparing neoadjuvant , adjuvant , and perioperative chemotherapy to surgery alone in patients with esophageal cancer , including those with adenocarcinoma , failed to demonstrate a benefit of additional chemotherapy on survival [ 17 , 29 ]  . 
briefly , a total of 503 patients ( 74% gastric cancer , 14% esophageal cancer , 11% cancer of the gastroesophageal junction ) were randomly assigned to perioperative chemotherapy with three preand postoperative cycles of epirubicin , cisplatin , and fluorouracil or surgery alone . 
however , due to the inability of this regimen to increase r0 resection rates , physicians are very reluctant to regard this regimen as the first choice for the treatment of esophageal and esophagogastic cancer . 
this demonstrates that a complex therapeutic procedure such as neoadjuvant rct followed by radical surgery of esophageal adenocarcinoma may successfully performed by an experienced multidisciplinary team [ 15 ] , even at cancer centers not having a very high case load but having specific expertise . 
however , to avoid toxic pulmonary effects tight constraints for low - dose radiation volume parameters need specific attention . strahlentherapie und onkologie current discussion radiotherapy of splenomegaly a palliative treatment option for a benign phenomenon in malignant diseases * jan kriz1 , oliver micke2 , frank bruns3 , uwe haverkamp4 , ralph mcke5 , ulrich schfer5 , heinrich seegenschmiedt6 , rolf - peter mller1 , hans theodor eich1 purpose : since the 20th century , radiotherapy ( rt ) has been used for treatment of symptomatic splenomegaly ( sm )  . 
the purpose of this analysis was to determine the indication , treatment concepts , and efficiency of rt . material and methods : clinical features , treatment concepts , and outcome data during the past 20 years were analyzed . 
endpoints were pain relief , symptomatic and hematological response , and treatment - related side effects . results : from 19892009 , a total of 122 patients received 246 rt courses because of symptomatic sm . 
overall 31 patients had chronic myelogenous leukemia ( cml ) , 37 had chronic lymphocytic leukemia ( cll ) , 23 had osteomyelofibrosis ( omf ) , 17 had polycythemia vera ( pv ) , 5 had acute myelogenous leukemia , 4 had idiopathic thrombocytopenic purpura ( itp ) , 3 had non - hodgkin lymphoma ( nhl ) , and 2 had multiple myeloma ( mm )  . 
in addition , rt as a palliative treatment option for symptomatic sm should not be forgotten . key words : splenomegaly palliative radiotherapy abdominal pain benign disorders strahlenther onkol 2011 ; 187 : 2214 doi 10.1007 / s00066 - 011 - 2252 - 4 radiotherapie der splenomegalie . 
die vorliegende analyse untersucht indikation , rt - konzepte und die effektivitt der rt . material und methode : patientendaten der letzten 20 jahre wurden hinsichtlich klinischer angaben , rt - konzepte und ergebnisse evaluiert . 
endpunkte waren schmerzfreiheit , hmatologisches ansprechen nach rt sowie therapieassoziierte nebenwirkungen . ergebnisse : zwischen 1989 und 2009 wurden 122 patienten ( 79 mnner und 43 frauen ) mit insgesamt 246 rt - serien behandelt . 
 folgende grunderkrankungen waren ursache fr die splenomegalie : cml ( 31 ) , cll ( 37 ) , osteomyelofibrose , ( 23 ) , polycyt haemia vera ( 17 ) , aml ( 5 ) , idiopathische thrombozytopenie ( 4 ) , non - hodgkin - lymphom ( 3 ) und plasmozytom ( 2 ) ( tabelle1 )  . 
es wurden einzelreferenzdosen zwischen 0 , 12 gy und gesamtreferenzdosen zwischen 316 gy appliziert ( tabelle 2 )  . * presented at the 16th annual meeting of the german society for therapeutic radiology and oncology ( degro ) , magdeburg , germany , june 36 , 2010 . 1department of radiation oncology , university of cologne , germany , 2department of radiation oncology , st . 
franziskus hospital bielefeld , germany , 3department of radiation oncology , medical school hannover , germany , 4department of radiology and radiation oncology , clemens hospital mnster , germany , 5department of radiation oncology , hospital lippe , germany , 6center of radiotherapy , hamburg , germany . received : december 21 , 2010 ; accepted : january 24 , 2011 published online : march 7 , 2011 strahlenther onkol 2011 n0 . 
radiotherapy of splenomegaly bei 74 , 8% der rt - serien ( 74 , 8% ) , die aufgrund einer schmerzhaften splenomegalie durchgefhrt wurden , konnte eine schmerzlinderung erzielt werden . 
36 patienten verstarben weniger als 2 monaten nach abschluss der rt im rahmen der infausten prognose ihrer grunderkrankung . bei 73 , 6% der rt - serien kam es zu einer verbesserung hinsichtlich thrombozytopenien und die transfusionsfrequenz nahm ab ( tabelle 3 )  . 
es wurden lediglich hmatologische toxizitten < ii ( eortc / rtog ) beobachtet . schlussfolgerung : die vorliegende analyse belegt die hohe effektivitt der rt bei geringem nebenwirkungsspektrudie rt der symptomatischen splenomegalie sollte als wirksame palliative option nicht in vergessenheit geraten . schlsselwrter : splenomegalie palliative radiotherapie abdominelle schmerzen gutartige erkrankungen introduction results since the beginning of the 20th century , splenic irradiation ( si ) has been used as a palliative treatment for patients with various chronic lymphoid and myeloid malignancies [ 19 ]  . 
for years , it was the only effective treatment ; however , since antineoplastic drugs became available , si is reduced to cases with symptomatic splenomegaly ( sm ) in palliative intentions . 
patients with sm often suffer from hard abdominal pain , challenged breathing and ingestion , anemia , thrombopenia , and cytopenia due to massive sm . the major goal for patients with terminal diseases is to palliate symptoms without causing unpleasant side effects . 
the purpose of this analysis was to determine the indication , treatment concepts , and effectiveness of rt . patients and methods seven german departments of radiation oncology collected clinical features , treatment concepts , and outcome data of their patients treated with si during the past 20 years . 
overall 31 patients suffered from chronic myelogenous leukemia ( cml ) , 37 from chronic lymphocytic leukemia ( cll ) , 23 from osteomyelofibrosis ( omf ) , 17 from polycythemia vera ( pv ) , 5 from acute myelogenous leukemia ( aml ) , 4 from idiopathic thrombocytopenic purpura ( itp ) , 3 from nonhodgkins lymphoma ( nhl ) , and 2 from multiple myeloma ( mm ) ( table 1 )  . all patients were afflicted with terminal disease and symptomatic sm with either severe abdominal pain or cytopenia . 
all of them received systemic antineoplastic drugs before rt , but most of them were resistant to systemic therapy , so si was the only treatment option for sm . between 1989 and 2009 , a total of 122 patients received 246 rt courses because of symptomatic sm . 
field sizes ranged from 14 24 cm to 33 x 42 cthe decrease of splenic size was monitored with ultrasound and ct scans , and the field sizes were adapted ( shrinking field )  . 
 blood counts were carefully monitored before each fraction to minimize the risk of hematological toxicity . significant pain relief was achieved in 143 of 191 rt courses ( 74.8% ) given for splenic pa at least 50% regression was attained in 184 of 238 rt courses ( 77% ) given for splenomegaly ( figure 1 )  . 
patientencharakteristik. characteristic gender female male 50 > 50 diseases chronic myelogenous leukemia chronic lymphocytic leukemia osteomyelofibrosis polycythemia vera acute myelogenous leukemia non - hodgkins lymphoma multiple myeloma patients n ( % ) 43 ( 35% ) 79 ( 65% ) 12 ( 10% ) 110 ( 90% ) 31 ( 26% ) 37 ( 31% ) 23 ( 20% ) 17 ( 14% ) 5 ( 4% ) 3 ( 3% ) 2 ( 2% ) strahlenther onkol 2011 n0 . 
the following results emerge from this study : si is an effective palliative treatment option for patients with symptomatic sm that reduces pain due to significant reduction of splenic size and improves hematological parameters . side effects are mild and retreatment is possible . although there are only few retrospective studies with low numbers of treated patients for si available [ 18 , 20 ] , we compared our findings with results reported in the literature . 
considering that hematologic disorders , such as cll , cml , and aml , are accompanied by sm and due to the fact that sm is often resistant to chemotherapy , si is used as a palliative treatment option . 
of 19 courses ( 74% ) given for massive abdominal pain , 14 resulted in significant pain relief , while 15 of 24 ( 63% ) courses given for sm resulted in a reduction of splenic size of at least 50% . 
this occurs in more than a third of patients and is thought to be due to extramedullary hematopoesis [ 1 , 2 , 5 , 10 , 13 , 17 , 18 , 20 , 21 ]  . allogenic bone marrow transplantation is the only curative treatment option , whereas all other therapies are palliative [ 23 ]  . 
 four additional reported series of patients with omf showed a decrease of abdominal pain in 63100% [ 3 , 5 , 8 , 15 , 17 , 22 , 23 ]  . 
the treatment courses consisted of two fractions of 50 cgy in the first week , two fractions of 75 cgy in the second week , and two fractions of 100 cgy in the third week . 
of the 32 ( 61% ) courses given for symptomatic sm , 19 showed an improvement in decrease of splenic size and hematological parameters ; 8 of 10 ( 80% ) courses achieved a reduction of pain [ 9 ]  . 
77% of treatment courses attained at least 50% regression of splenic size and 75% resulted in pain relief . conclusion the present evaluation comprises the largest database of reported cases of rt given for sm so far and underlines the efficiency of rt as a palliative treatment . 
strahlenther onkol 2010 ; 186 : 56571 ( doi 10.1007 / s00066 - 010 - 2159 - 5 ) the authors would like to make the following correction in the above publication , i.e. , the overall survival ( os ) times reported were concerning mean instead of median survival times . 
 thus , the results paragraph of the article 's abstract must read as follows ( with the corrected term emphasized in bold italics ) : results : mean os and icc for the entire cohort were 9 and 7 months . 
the results of the subgroup rpa class analyses were similar to the entire cohort . strahlenther onkol 2011 ; 187 : 267 doi 10.1007 / s00066 - 011 - 7159 - 6 published online : march 25 , 2011 strahlenther onkol 2011 n0 . 
4 urban & vogel strahlentherapie und onkologie original article remission rates in breast cancer treated with preoperative chemotherapy and radiotherapy brbel gerlach1 , 4 , werner audretsch2 , frank gogolin3 , theodor knigshausen3 , ralf rohn1 , gerd schmitt1 , peter dimmerling1 , stephan gripp1 , karl axel hartmann1 purpose : evaluation of remission rates after neoadjuvant chemotherapy alone or followed by preoperative radiotherapy . 
the whole breast was homogeneously irradiated using 2 - gy fractions up to a total dose of 50 gy , followed by a boost of 611 gy to the tumor . results : a histologically proven complete remission ( pcr ) was achieved in 3% ( 2 / 64 ) in the ct and in 42% ( 56 / 134 ) in the ctrt group . 
the logistic regression analysis , including clinical tumor category ( ct ) , lymph node ( cn ) and metastasis status ( cm ) , grading ( g ) , hormone receptor status ( hrs ) , number of preoperative chemotherapy cycles , preoperative tumor volume , and preoperative radiotherapy , revealed that hrs ( p = 0.0232 ) and radiotherapy ( p < 0.0001 ) were significant factors for achieving pcr . 
 key words : breast cancer neoadjuvant therapy radiotherapy breast reconstruction strahlenther onkol 2003 ; 179 : 30611 doi 10.1007 / s00066 - 003 - 1019 - y remissionsraten nach properativer chemound strahlentherapie bei mammakarzinomen zielsetzung : bestimmung der remissionsraten von mammatumoren nach alleiniger neoadjuvanter chemotherapie oder properativer chemound strahlentherapie . 
 ergebnisse : eine histologisch gesicherte komplette remission ( pcr ) wurde bei 3% der patientinnen ( 2 / 64 ) in der ctund bei 42% ( 56 / 134 ) in der ct - rt - gruppe erreicht . 
die logistische regressionsanalyse , die klinisches tumorstadium ( ct ) , lymphknoten ( cn ) und metastasierungsstatus ( cm ) , grading ( g ) , hormonrezeptorstatus ( hrs ) , anzahl der properativen chemotherapiezyklen , properatives tumorvolumen und properative radiotherapie beinhaltete , zeigte , dass hrs ( p = 0 , 0232 ) und radiotherapie ( p < 0 , 0001 ) signifikante faktoren fr das erreichen einer pcr waren . 
 key words : mammatumoren neoadjuvante therapie radiotherapie brustrekonstruktion 1 department of radiation oncology , university clinic dsseldorf , germany , 2 department of senology , and 3 department of medicine , academic hospital dsseldorf gerresheim , germany , 4 department of radiation oncology , vu medical center amsterdam , the netherlands . 
remission rates in breast cancer after preoperative chemo - / radiotherapy introduction the large overview by the early breast cancer trialists collaborative group including 20 , 000 patients showed a twothird reduction in local recurrence and a moderate gain in overall survival for patients treated with radiotherapy [ 1 ]  . 
based on several randomized clinical trials with follow - up times > 10 years , breast - preserving surgery and subsequent radiotheraphy are regarded as a safe treatment option for stage i and ii tumors with respect to local recurrence - free survival and overall survival [ 2 , 4 , 13 , 19 , 26 , 27 , 34 , 35 ]  . 
here , the question arises how to sequence chemotherapy and irradiation in a comprehensive oncologic concept . some investigators have administered induction ( neoadjuvant ) chemotherapy to avoid mutilating surgery [ 6 , 18 , 28 , 36 ]  . 
however , long - term results of this approach are pending , and the volume of resection following induction chemotherapy is still a matter of debate [ 21 ]  . 
in a small series , we have achieved a histopathologically complete response in 24 out of 56 tumors , which was significantly more than after induction chemotherapy alone [ 2 ]  . 
since response rates after induction chemotherapy are well known [ 25 , 32 , 33 ] , our data will help to assess the additional benefit of moderate radiation doses for the local control of breast cancer . 
 patients and methods in this protocol , 194 patients with 198 biopsy - proven invasive breast tumors treated at the department of radiation oncology , university of dsseldorf , germany , during 1992 and 1999 were evaluated . 
patient characteristics are outlined in table 1 . other inclusion criteria were : nonmetastatic tumors ( except postsurgically defined supraclavicular or subscapular lymph node metastasis ) , < 77 years of age , tumor diameter > 3 cm or < 3 cm in case of an unfavorable ratio of tumor / breast volume or anatomic difficulties so that an initial breast - preserving approach was impossible . 
all patients underwent physical examination , chest x - ray , blood chemistry , bone scan , and liver sonography in order to rule out overt metastatic disease . myocutaneous flaps were indicated in patients with large tumors and / or an unfavorable tumor - breast relation . 
generally , patients with smaller tumors and a planned procedure without flaps like tumorectomy or modified radical mastectomy ( mrm ) underwent surgery immediately after chemotherapy . preoperative radiotherapy was administered in patients with larger tumors where further shrinkage was desired to facilitate surgery . 
this is reflected by the different initial tumor diameters of 3.3 and 5 cm in the chemotherapy and chemo - / radiotherapy group , respectively , measured by means of either ultrasound , mammography or mri mammography , or a combination of these ( table 1 )  . 
 systemic treatment breast cancer patients who are candidates for flap - supported surgery or have locally advanced tumors are subjected depending on performance status , comorbidity , age , and tumor factors such as c - erbb2 , different neoadjuvant chemostrahlenther onkol 2003 no . 
in both treatment groups , four cycles of epirubicin / cyclophosphamide ( ec 90 mg / m2 / 600 mg / m2 ) were administered in 3 - week intervals , followed by three cycles of cyclophosphamide / methotrexate / 5 - fu ( cmf 600 mg / m2 / 40 mg / m2 / 600 mg / m2 ) in patients with large tumors . 
the median time intervall between the end of chemoand beginning of radiotherapy was 4 weeks ranging from 0 to 20 weeks in the chemo - / radiotherapy group . two patients in this group received preoperative chemoand radiotherapy simultaneously . 
even in case of macroscopic tumor infiltration , the axillary lymphatic drainage was not irradiated , since most enlarged axillary lymph nodes responded to chemotherapy and all patients received a level iii axillary dissection after neoadjuvant treatment . 
 surgery the time interval between the end of neoadjuvant treatment and surgery ranged from 4 to 24 weeks ( median , 8 weeks ) and from 3 to 38 weeks ( median , 16 weeks ) for the chemotherapy and chemo - / radiotherapy group , respectively . 
full recovery from acute radiation side effects before surgery was allowed in the chemo - / radiotherapy group , which is the reason for the extended time interval between neoadjuvant treatment and surgery . 
there are no substantial data in the literature on the optimal interval between preoperative radiotherapy and surgery , and in our own experience wound complication rates are not increased if acute radiation side effects have subsided at the time of surgical intervention . 
in two patients of the chemotherapy group , radiotherapy was carried out after flap - supported surgery . this was due to a change of the surgical strategy caused by a minor response to neoadjuvant chemotherapy . 
2 / 64 cases ( 3% ) of the chemotherapy group achieved a complete ( pcr ) and 40 / 64 cases ( 63% ) a partial histopathologic response ( ppr )  . 
remission rates in breast cancer after preoperative chemo - / radiotherapy ( cn ) and metastasis status ( cm ) , grading ( g ) , hormone receptor status ( hrs ) , number of preoperative chemotherapy cycles , preoperative tumor volume , and preoperative radiotherapy , revealed that hrs ( p = 0.0232 ) and radiotherapy ( p < 0.0001 ) were significant factors for achieving pcr . 
cmf : cyclophosphamide / methotrexate / fluorouracil ; ct : chemotherapy ; ctrt : chemo - / radiotherapy ; ec : epirubicine / cyclophosphamide ; lat flap : latissimus dorsi myocutaneous flap ; mrm : modified radical mastectomy ; tram flap : trans - rectus abdominis myocutaneous flap . 
55% ( 74 / 134 ) in the chemo - / radiotherapy group ( 14 cases : tumorectomy ; 60 cases : tumorectomy + lat flap ) and 41% ( 26 / 64 ) in the chemotherapy group ( 25 cases : tumorectomy ; one case : tumorectomy + lat flap ) underwent breastpreserving surgery . 
in 74 / 198 cases ( 37% ) , modified radical mastectomy ( mrm ) without reconstruction was required . three patients ( 5% ; two cases : mrm + tram flap , one case : tumorectomy + lat flap ) in the chemotherapy group and 82 patients ( 61% ; 22 cases : mrm + tram flap ; 60 cases : tumorectomy + lat flap ) in the chemo - / radiotherapy group underwent flap - supported surgery . 
 the overall survival time was median 13 months ( range , 260 months ) in the chemotherapy and 19 months ( range , 264 months ) in the chemo - / radiotherapy group . 
in one patient in the chemotherapy and 13 patients in the chemo - / radiotherapy group , no information about follow - up were available . the tumor - free survival ranged from 1 to 18 months ( median , 10 months ) and from 6 to 36 months ( median , 25 months ) in the chemotherapy and chemo - / radiotherapy group , respectively . 
 discussion the results of this nonrandomized treatment schedule indicate that the rate of histopathologically complete response is significantly higher when cytotoxic drugs are combined with radiotherapy in a preoperative setting . 
the logistic regression analysis , including clinical tumor category ( ct ) , lymph node ( cn ) and metastasis status ( cm ) , grading ( g ) , hormone receptor status ( hrs ) , number of preoperative chemotherapy cycles , preoperative tumor volume , and preoperative radiotherapy , revealed that hrs ( p = 0.0232 ) and radiotherapy ( p < 0.0001 ) were significant factors for achieving pcr . 
remission rates in breast cancer after preoperative chemo - / radiotherapy followed by irradiation of the breast with 50 gy and a boost of 10 gy to the tumor site . 
in a protocol introduced by rilke et al [ 24 ] , 42 patients received neoadjuvant chemotherapy and preoperative irradiation with 15 gy . here , the rate of histopathologically complete response was < 10% . 
in our series with preoperative irradiation with 50 gy to the whole breast and a boost of 610 gy to the tumor site , a histopathologically complete response was achieved in 56 out of 134 cases ( 42% ) which is comparable with the data of serin et al [ 30 ]  . 
although our treatment policy and the study of colleoni et al [ 9 ] are similar with respect to initial tumor size , chemotherapy regimens and irradiation schedule , the reason for the divergence in complete response rates is not yet clear . 
79 of 134 cases ( 59% ) in the chemo - / radiotherapy and 29 / 64 cases ( 45% ) in the chemotherapy group received preoperative endocrine treatment which implies that the difference in complete remission rates in both groups cannot be attributed to the additional endocrine therapy . 
although the tumor diameters in both studies were comparable with those in our limited series , the difference in complete remission rates might be explained by the use of different chemotherapeutic agents . 
in larger tumors , however , conservative procedures are less often possible [ 7 , 29 ]  . the policy of resecting the tumor according to its pretreatment margins and the relatively large tumor diameters ( median , 3 cm [ chemotherapy group ] and 5.5 cm [ chemo - / radiotherapy group ] ) may be the reason for the relatively low breastpreserving rate of 50% in our protocol . 
in this context it has to be taken into consideration that in the past this policy resulted in a low rate of isolated locoregional recurrence [ 16 , 17 ]  . 
 these results indicate that preoperative radiation therapy , as used in this protocol , increases the rate of histopathologically complete response and breast preservation in the neoadjuvant treatment of breast cancer . 
 strahlentherapie und onkologie original article usefulness of tumor volumetry as a prognostic factor of survival in head and neck cancer ralf kurek1 , anna kalogera - fountzila2 , klaus muskalla3 , urania dafni4 , thomas schnabel5 , bernhard kober6 , sandra rddiger1 , thomas martin1 , george fountzilas2 , nikolaos zamboglou1 background : the tnm classification system of tumor stage does not always reflect the actual tumor mass present at diagnosis . this study aimed at evaluating the prognostic value of volumetric data regarding survival in head and neck cancer patients being treated with either cisplatin or carboplatin administered concomitantly with radiotherapy . 
 patients and methods : we retrospectively analyzed 107 patients suffering from squamous cell carcinoma of the head and neck in a greek - german cooperational study ( see table 1 )  . 
65 patients received chemotherapy with carboplatin and 42 with cisplatmore than 6 , 200 ct scans were analyzed by digitalization of contours which subsequently led to the computation of the tumor volume ( primary and macroscopic lymph node metastases )  . 
median initial tumor volume was 32.5 ml ( range 2.1220.1 ml ) in the carboplatin and 44.4 ml ( range 3.2202.5 ml ) in the cisplatin group ( see figure 1 )  . 
after treatment , tumor volumes did not differ significantly ( median of 3.1 ml [ range 0.0167.1 ml ] and 3.5 ml [ range 0.0166.0 ml ] , respectively )  . 
 key words : tumor volume head and neck cancer volumetry strahlenther onkol 2003 ; 179 : 2927 doi 10.1007 / s00066 - 003 - 1017 - 0 bedeutung der tumorvolumetrie zur berlebensprognose bei kopf - hals - tumoren hintergrund : das tnm - tumorklassifikationssystem reprsentiert nicht immer die tatschliche tumormasse bei diagnose . 
diese studie hatte die berprfung der prognostischen wertigkeit volumetrischer analysen bezglich des berlebens bei patienten mit kopf - hals - tumoren , die radiotherapeutisch und mit begleitender chemotherapie ( cisplatin oder carboplatin ) behandelt wurden , zur zielsetzung . 
 schlsselwrter : tumorvolumen kopf - hals - tumoren volumetrie 1 department of radiotherapy , klinikum offenbach , germany , 2 ahepa hospital , aristotle university of thessaloniki , school of medicine , thessaloniki , macedonia , greece , 3 department of radiotherapy , heinrich heine university dsseldorf , germany , 4 department of public health , school of nursing , university of athens , greece , 5 department of radiotherapy , clinic for radiooncology and nuclear medicine , ludwigshafen , germany , 6 department of radiotherapy , klinikum darmstadt , germany . 
 thereby , one does not take into account that large - volume tumors might shrink enormously in absolute terms but still fail to reach the 50% cutoff point ( e.g. , 64 cm3 reduced by as much as 31 cm3 ) , while other tumors ( e.g. , 8 cm3 reduced by as little as 4 cm3 ) are assigned as having partially responded . 
 other staging systems have been developed , e.g. , the classification of the international federation of gynecology and obstetrics ( figo ) for cervical cancer , aiming at a refinement of staging precisely tailored to a specific tumor entity , but the remaining problem with all staging systems is that they generalize and summarize different tumors with different volumes into the same stage . nowadays , with a significant progress in the area of imaging , it is easy to obtain a precise measure of the actual tumor volume . 
however , physicians are still relying just on the mass size and not on the tumor volume to stage patients and evaluate response , and only a few studies were undertaken so far to evaluate the clinical usefulness of tumor volumetry . 
 burghardt et al [ 3 ] associated the outcome of surgical treatment of 1 , 028 cervical cancers to tumor volumetry data . the results of this study indicated that volumetry of the tumor permitted a more accurate assessment of therapeutic results in those patients than did the figo classification . 
another interesting study , performed by kikuchi et al [ 15 ] found that the logarithmic tumor volume was the most important variable correlated with lymph node metastasis in early gastric cancer . mayr et al [ 17 ] investigated the usefulness of tumor volumetry by magnetic resonance imaging for quantitative assessment of tumor volume as well as tumor regression before , during and after radiation therapy . 
tumor volumetry turned out to be a sensitive measure of the responsiveness of cervical cancer to irradiation , and treatment response could be assessed as early as during the course of radiation therapy . 
volumetry could therefore not only help to improve the prediction of outcome but also the outcome itself by identifying patients at high risk of treatment failure and , thus , seek alternative treatment for these patients . 
 only limited data on volumetry regarding head and neck cancers has been published [ 4 , 7 , 19 ] , which itself would make it worthwhile to investigate volumetry in this patient cohort . the aim of this study was to evaluate the prognostic value of volumetric data regarding survival in head and neck cancer patients being treated with either cisplatin or carboplatin given concomitantly with radiotherapy which has not yet been performed in a sufficient manner . 
all patients were participants in two different phase ii studies conducted by the hellenic cooperative oncology group ( hecog ) in greece and by the department of radiotherapy , klinikum darmstadt , germany . 
the digitalized contours were extrapolated with a parabolic function to the contours of the next picture taking into account the distance between thethus , knowing the surface of the tumor , the volume could be estimated . 
 after treatment , tumor volumes did not differ significantly ( median of 3.1 ml [ range 0167.1 ml ] in the carboplatin group vs median of 3.5 ml [ range 0166.0 ml ] in the cisplatin group )  . 
 prognostic factors of survival chemotherapy treatment ( p = 0.017 ) along with pretherapeutic tumor volume ( p = 0.014 ) were the only factors significantly associated with survival among all initial patients characteristics assessed for prognostic value . 
cox regression was used to evaluate the significance of treatment ( cisplatin vs carboplatin ) , the tumor volume before treatment , the logarithm of the tumor volume before treatment , the absolute decrease in tumor volume , the percentage decrease of tumor volume , t - stage ( t1 / 2 vs t3 vs t4 ) , n - stage ( n0 vs n1 / 2 vs n3 ) , and age . 
the spss 10 software ( spss inc . , chicago , il , usa , 1999 ) was used for statistical analysis . patient treatment all patients received radiotherapy in shrinking - field technique up to a tumor volume dose of 7074 gy with a fractionation of 2 gy per day . 
carboplatin was administered at a dose of 400 mg / m2 on days 2 , 22 , and 42 of treatment , while cisplatin was administered at a dose of 100 mg / m2 on days 2 , 22 , and 42 . 
 examining other tumor characteristics such as absolute change in tumor volume , percent change , and after - treatment tumor volume showed that percent change was an independent prognostic factor of survival ( p = 0.02 ; table 3 )  . 
thus , percent decrease ( used in defining partial or complete response ) is a strong predictor of survival , but initial tumor volume is an independent significant predictor as well . 
 discussion for the vast majority of malignant diseases tumor size is known to be an important prognostic factor of patients survival [ 1 , 8 , 11 , 14 , 2022 ]  . 
tumor volume significantly influences radiotherapy outcome , and in many sites it is likely to be a superior prognostic indicator as compared to tumor stage , which reflects tumor size only partially and is mainly correlated to operability [ 5 ]  . 
it is astonishing that these findings have not yet widely changed the perception of tumor volume as a most important additional factor to be further examined in a broad range of malignant diseases . 
rudat et al [ 19 ] examined , in a very well elaborated study , prognostic clinical and treatment - related factors of local control , distant metastasisfree survival , and survival by means of a multivariate analysis in patients with advanced squamous cell carcinoma of the head and neck after concomitant boost radiochemotherapy . after evaluating the 68 patients included in this study , the authors found that total tumor volume and survival were significantly associated . 
in another study , dietz et al [ 4 ] related the degree of vascularity , which had been determined using color doppler imaging , to total tumor volume calculated from ct sections . 
tumor volumetry in head and neck cancer we evaluated the prognostic significance of treatment ( cisplatin vs carboplatin ) , the initial tumor volume before treatment , the logarithm of the tumor volume before treatment , the absolute decrease in tumor volume , the percentage decrease in tumor volume , the t - stage ( t1 / 2 vs t3 vs t4 ) , the n - stage ( n0 vs n1 / 2 vs n3 ) , presence or absence of distant metastasis , and age . 
only chemotherapy and initial tumor volume ( p = 0.014 ) remained prognostic in terms of survival when applying a cox model with backward selection procedure . even tand n - stage were eliminated . 
this demonstrates that in our patient group tumor volumetry was more important than the tnm classification systewe examined other tumor characteristics in a second cox model , further elucidating the possible effects of absolute decrease in tumor volume , percentage decrease in tumor volume , and after - treatment tumor volume on survival . 
we found that the percentage decrease in tumor volume after concurrent radiochemotherapy was an independent prognostic factor of survival along with treatment , but most importantly the initial tumor volume remained a significant independent predictor . 
they lack information captured by with the initial tumor volume . however , the fact that the cox regression model treatment showed also a significant effect on survival , means , that tumor volume characteristics alone cannot be used as surrogate markers of survival . 
 these data result from a retrospective analysis study , based on nonrandomized treatments , and should be interpreted cautiously , but the advantage of a retrospective analysis from ct films done years before enable us to correlate volumetric data with long - term survival . 
another point of criticism could be an inhomogeneous distribution of advanced tumors or tumors of adverse localization in the two chemotherapy treatment groups ( e.g. , 63% t4 - tumors and 34% tumors of the hypopharynx in the carboplatin group vs 43% t4 - tumors and 19% tumors of the hypopharynx in the cisplatin group )  . 
 in order to validate these data , we are currently performing a volumetric analysis of patients with locally advanced head and neck cancer in a prospective randomized study with three arms where patients were treated with either cisplatin or carboplatin and concomitant radiotherapy or with radiotherapy alone . 
tumor volumetry seems to be the most objective and reproducible basis for assessing the initial tumor load as well as the results of other treatment modalities such as radiotherapy , chemotherapy , or surgery . 
an additional promising feature of tumor volume as opposed to other prognostic factors such as lymph node or vascular involvement is that it can be determined accurately before treatment [ 3 ] , which stresses another disadvantage of the commonly applied tnm staging system , reflected in the discrepancies between clinical and pathologically confirmed tor n - stage . 
 strahlentherapie und onkologie originalarbeit primre radiochemotherapie inoperabler fortgeschrittener sophaguskarzinome ergebnisse einer phase - ii - studie und literaturbersicht peter fritz1 , 2 , peter stoll3 , michael wannenmacher1 , dietmar zierhut1 hintergrund : weder die chirurgischen noch die strahlentherapeutischen fortschritte konnten die mortalitt des sophaguskarzinoms signifikant senken . 
metaanalysen randomisierter studien auf der basis der evidence - based medicine knnen fr die simultane radiochemotherapie allenfalls eine verbesserung des 2 - jahres - berlebens bei ebenfalls hoher toxizitt darstellen . 
 schlsselwrter : sophaguskarzinom strahlentherapie simultane radiochemotherapie strahlenther onkol 2003 ; 179 : 32836 doi 10.1007 / s00066 - 003 - 1038 - 8 concurrent chemotherapy and radiation therapy for unresectable locally advanced carcinoma of the esophagus . 
 phase ii study and clinical review on literature background : neither surgical advances nor those in therapeutic radiology have been able to significantly reduce the mortality related to esophageal carcinomas . 
 patients and methods : for 50 patients with unresectable locally advanced esophageal carcinomas , a palliative concurrent chemotherapy and radiation therapy was carried out according to the intent to treat principle . 
the following factors exhibited a significant correlation to survival : the intensity of the chemotherapy , the karnofsky index , the age of the patients , and the improvement of oral food intake . 1 abteilung klinische radiologie ( schwerpunkt strahlentherapie und poliklinik ) der universitt heidelberg , 2 klinik fr radioonkologie , st . - marien - krankenhaus , siegen , 3 institut fr diagnostische und interventionelle radiologie , krankenhaus mnchen - schwabing , mnchen . 
at best , meta - analyses of randomized studies along the lines of evidence - based medicine demonstrate for concurrent chemotherapy and radiation therapy an improvement of 2 - year survival rates , but with these also involving a high level of toxicity . 
due to the heterogeneous data available , the value of the primary , sequential treatment combining chemotherapy and radiation therapy is uncerta key words : esophageal carcinoma radiotherapy concurrent radiochemotherapy einleitung die bsartigen neubildungen der speiserhre gehren mit einem anteil von ca . 
der von earlam & cunhamelo [ 12 ] 1980 verffentlichten sammelstatistik zur alleinigen strahlentherapie des sophaguskarzinoms , welche 49 verffentlichungen aus dem zeitraum 19541978 umfasst , ist auch im jahr 2003 nichts hinzuzufgen . 
so werden zahllose kombinationen von chirurgie , strahlentherapie , chemotherapie sowie endoskopischen und interventionell radiologischen verfahren eingesetzt , wobei das therapiekonzept oft mehr von fachspezifischen berzeugungen als von der datenlage bestimmt wird . 
 patienten und methodik behandlungsprotokoll an der universitt heidelberg wurde 19891996 bei 50 patienten mit inoperablen lokal fortgeschrittenen sophaguskarzinomen eine palliative simultane radiochemotherapie nach dem intent to treat - prinzip durchgefhrt . 
ernsthaft behinderte oder gar bettlgerige patienten , die auch unter stationren bedingungen nicht selbststndig das bestrahlungsgert aufsuchen konnten ( karnofsky - index 30% ) , wurden von der radiochemotherapie ausgeschlossen . 
zur klassifikation wurde die prtherapeutische , klinische tnm - klassifikation der union internationale contre le cancer ( uicc ) von 1978 angewendet , die sich auch mit der klassifikation der american joint committee on cancer ( ajcc ) von 1983 deckt ( tabelle 1 )  . der rckgriff auf diese historischen klassifikationen geschah aus zwei grnden . 
fr inoperable patienten ist deshalb eine treffsichere stadieneinteilung nur schwer mglich , sodass viele strahlentherapiestudien die alten klassifikationen auch heute noch zugrunde legen ( tabellen 2 und 3 )  . 
 zervikaler und intrathorakaler sophagus t1 : tumor 5 cm , keine obstruktion , kein befall der gesamten zirkumferenz , keine extrasophageale ausbreitung t2 : tumor > 5 cm , obstruktion und / oder befall der gesamten zirkumferenz , keine extrasophageale ausbreitung t3 : tumor mit extrasophagealer ausbreitung zervikaler sophagus n0 : kein befall der regionren lymphknoten n1 : bewegliche , unilaterale lymphome n2 : bewegliche , bilaterale lymphome n3 : fixierte regionre lymphknoten intrathorakaler sophagus n0 : kein befall der regionren lymphknoten n1 : befall bei chirurgischer exploration oder mediastinoskopie stadiengruppierung stadium i der uicc ( zervikal und intrathorakal ) : t1 , n0 , m0 stadium i des ajcc : t1 , n0 , m0 stadium ii der uicc ( zervikal ) : t1 , n12 , m0 ; ( intrathorakal ) : t2 , n0 , m0 stadium ii des ajcc : t1 , n12 , m0 oder t2 , n02 , m0 stadium iii der uicc ( zervikal ) : t3 , n03 , m0 ; ( intrathorakal ) : t13 , n1 , m0 stadium iii des ajcc : t3 , n03 , m0 oder t13 , n3 , m0 stadium iv der uicc ( zervikal und intrathorakal ) : t13 , n03 , m1 stadium iv der ajcc : t13 , n03 , m1 erste arbeiten zur endosonographie des sophaguskarzinoms erschienen erst ab 1986 [ 46 ]  . 
79% der flle vorhersagbar , sofern der tumor mit dem endoskop passierbar ist [ 7 , 32 ]  . dies ist je nach patientengut in 3874% der flle mglich [ 32 , 47 ]  . 
nach strahlenbehandlung und / oder chemotherapie sind die echostrukturen infolge von fibrosen , demen und anderen therapieassoziierten gewebsreaktionen schwer differenzierbar , sodass die methode fr die beurteilung des therapieerfolgs eine nur ungengende treffsicherheit aufweist und kaum fr eine operationsentscheidung z.b. 
die beibehaltung der klassifikation von 1978 , die wenigstens bezglich des t - stadiums durch bildgebende und endoskopische verfahren leicht zu verifizieren ist , war deshalb sinnvoll und ermglicht auch einen vergleich mit den ergebnissen der relevanten literatur . 
cddp : cisplatin , 5fu : 5 - fluorouracil , bleo : bleomycin , mmc : mitomycin - c , / / : simultan , ~ dauerinfusion , erhaltungschemotherapie , pec : plattenepithelkarzinome , adc : adenokarzinome , langzeitergebnisse der studie von herskovic et al . 
cddp : cisplatin , 5fu : 5 - fluorouracil , bleo : bleomycin , adm : adriamycin , mtx : methotrexat , / / : simultan , ~ : dauerinfusion , : hochdosis - cisplatin ( 100 mg / m2 ) , tod whrend der therapie , pec : plattenepithelkarzinome , adc : adenokarzinome , * plus 5 adjuvante chemotherapien nach bestrahfutraful mindestens ber 30 tage nach radiatio / die ( mediane behandlungsdauer 21 , 9 wochen ) , mediane lung bei roussel et al . 
 der mittelwert der maximalen axialen tumordurchmesser lag bei 4 , 0 c14% der tumoren hatten einen durchmesser bis 2 , 9 c74% der tumoren hatten einen durchmesser von 35 , 9 cbei 12% der tumoren lag der durchmesser bei 6 cm oder mehr . 
der mittelwert der tumorlnge betrug 8 , 7 cbei vier patienten ( 8% ) war die tumorlnge 5 cm ; bei 32 patienten ( 64% ) 510 cm ; bei 14 patienten ( 28% ) > 10 cm . das lumen des sophagus wurde an der stelle der maximalen stenosierung gemessen . 
der mittlere stenosedurchmesser lag bei 6 , 2 mm . die verteilung der t - stadien war t1 : sieben patienten ( 14% ) , t2 : 16 ( 32% ) , t3 : 27 ( 54% )  . 
10090% : sieben patienten ( 14% ) , 8070% : 15 patienten ( 30% ) , 6050% : neun patienten ( 18% ) , 40% : 19 patienten ( 38% )  . 
kaplan - meier overall survival time of entire group ( n = 50 )  . zum prognostischen einfluss des lebensalters bei therapiebeginn wurden mittels des log - rank - tests der einfluss der variablen 55 jahre vs . 
 > 55 jahre auf den verlauf der life - table - kurven geprdie mediane berlebenszeit der patienten < 55 jahre war 12 monate , die mediane berlebenszeit der lteren patienten betrug 7 , 8 monate . 
 die berlebenszeit der 25 patienten , welche ausschlielich regionale lymphknotenmetastasen aufwiesen , wurde gegen diejenige der 16 patienten mit fernmetastasen geprft . die mediane berlebenszeit der gruppe mit lymphknotenmetastasen betrug 13 , 3 monate , die der gruppe mit fernmetastasen betrug 7 , 4 monate . 
 die berlebenszeit war bei patienten mit karnofsky - indizes [ 27 ] von 50100% ( gruppen i , ii , iii ) hoch signifikant lnger ( p = 0 , 0005 ) als bei patienten mit einem karnofsky - index von 40% ( gruppe iv )  . 
survival according to swallowing score ( normal = eats solids , passiert / flssig = eats pureed food or drinks liquids only , keine passage = no swallowing at all ; log - rank test : p = 0.0003 , df = 2 )  . 
 therapie - boost 6 wochen nach der letzten brachytherapiefraktion berpr nc : 14 patienten ( 28% ; inkludiert sind die whrend der therapie verstorbenen ) , pr : 32 patienten ( 64% ; hierunter zhlen auch die partiellen remissionen nach brachytherapie - boost ) , cr : vier patienten ( 8% )  . 
der zusammenhang zwischen oraler ernhrungsmglichkeit und berlebenszeit war hoch signifikant ( mediane berlebenszeit : fast normale passage 13 , 7 monate ; nur passierte / flssige kost 8 , 5 monate ; keine passage 3 , 3 monate ; abbildung 2 )  . 
 der lokale therapieerfolg wurde definitiv 6 wochen nach ende der perkutanen strahlenbehandlung oder bei brachyein endokavitrer boost nach beendigung der perkutanen strahlentherapie wurde bei 17 patienten ( 34% ) durchgefhrt , die endoluminale afterloading - brachytherapie strahlenther onkol 2003 no . 
einmal pro woche wurden mit einem 192 - ir - hdrafterloadinggert 5 gy spezifiziert auf 10 mm distanz von der oberflche eines 8 mm durchmessenden applikatorschlauches appliziert [ 15 ]  . 
patienten , die nach durchschreiten des nadirs zum vorgesehenen zeitpunkt des nchsten chemotherapiezyklus keine leukozytenwerte 3000 / l und thrombozytenwerte 80000 / l erreicht hatten , wurden ebenfalls von der weiterfhrung der chemotherapie ausgeschlossen . 
ursachen fr den abbruch der chemotherapie nach dem ersten zyklus war die verschlechterung des allgemeinzustandes ( sieben patienten ) , tod whrend der therapie ( sechs patienten ) , ablehnung ( drei patienten ) , leukopenie ( zwei patienten , who grad 3 ) , fistel ( zwei patienten ) , verschlechterung der leberfunktion ( ein patient , who grad 3 )  . 
die remissionsraten im ersten follow - up 6 wochen nach radiochemotherapie beziehen sich auf 41 patienten mit mindestens einem chemotherapiezyklus und einer referenzdosis 40 gy : nc / minor response ( 17 / 41 ) 41 , 5% , pr ( 16 / 41 ) 39% , cr ( 8 / 41 ) 19 , 5% . zustzliche adjuvante zyklen erhielten weitere zwlf patienten , die mindestens eine partielle remission erreicht hatten . drei patienten erhielten einen , drei patienten zwei , vier patienten drei und zwei patienten noch vier zyklen . 
ursachen fr die stufenweise beendigung der erhaltungschemotherapie waren hmatologische toxizitt ( 3 / 12 ) 20% , no change nach zwei zyklen ( 3 / 12 ) 20% , belkeit / mukositis ( 4 / 12 ) 30% . todesflle traten whrend der erhaltungstherapie nicht auf . die intensitt der chemotherapie korrelierte signifikant mit der berlebenszeit der patienten ( abbildung 3 )  . 
mit einer sequenziellen oder simultanen 5fuund / oder cisplatinhaltigen radiopolychemotherapie knnen bei lokal und / oder systemisch fortgeschrittenen sophaguskarzinomen mediane berlebenszeiten von 620 monaten ( durchschnitt : 11 , 9 ) und ansprechraten des primrtumors zwischen 25 und 97% ( durchschnitt : 63% ) erreicht werden . fnf studien [ 20 , 34 , 38 , 44 , 47 ] berichten ber > 10% who grad - 3 / 4 - toxizitten und drei [ 34 , 38 , 49 ] ber therapiebedingte todesflle . 
dies zeigt ein berblick ber elf studien von 1990 bis 2000 mit kollektiven zwischen 22 und 65 patienten , die mindestens 75% fortgeschrittene sophaguskarzinome enthalten hatten [ 5 , 9 , 20 , 25 , 34 , 38 , 43 , 45 , 48 , 49 , 53 ]  . unsere eigenen ergebnisse knnen hier zwanglos eingeordnet werden . 
 es wurden randomisierte studien zur simultanen radiochemotherapie durchgefhrt ( tabelle 2 ) , wobei nur die radiation therapy oncology group - ( rtog - ) 85 - 01 - studie von herscovic et al . 
diese studie , deren aussage in followup - auswertungen [ 1 , 10 ] mit 5 - jahres - ergebnissen besttigt wurde , kann jedoch nicht zur allgemeinen empfehlung einer primren radiochemotherapie bei lokoregional fortgeschrittenen sophaguskarzinomen herangezogen werden , da die rtog hier ein fr die strahlentherapie vllig untypisches patientenkollektiv randomisiert hat . 
es ist weiterhin unklar , ob der signifikante vorteil der radiochemotherapie auch bei lokoregional fortgeschrittenen tumorstadien realisiert werden kann , zumal die radiochemotherapie der rtog - studie zu 44% schweren und 20% lebensbedrohlichen komplikationen gefhrt hatte , worunter ein patient verstarb , whrend im reinen strahlentherapie - arm kaum lebensbedrohliche komplikationen aufgetreten waren . 
 [ 44 ] , die ausschlielich t3 , n01 , m0 - tumoren ebenfalls klassifiziert nach der klinischen stadieneinteilung des ajcc von 1983 einschloss , hatte verglichen mit einer alleinigen palliativen strahlenbehandlung mit einem nahezu identischen radiochemotherapieschema auer einer verstrkten grad - iii - toxizitt keinen vorteil erbracht ( tabelle 2 )  . 
 eine aktuelle metaanalyse randomisierter studien zur primren radiochemotherapie des sophaguskarzinoms , die einen qualitativen mindeststandard nach den regeln der evidence - based medicine erfllten , wurde von einer cochrane - arbeitsgruppe vorgelegt [ 52 ]  . 
 die autoren kommen zu dem ergebniss , dass wegen den heterogenen und meist zu kurzen nachbeobachtungszeiten der studien allenfalls 1und 2 - jahres - ergebnisse einigermaen verlsslich mitgeteilt werden knnen . 
in sechs randomisierten studien ( tabelle 3 ) zur primren sequenziellen radiochemotherapie wurde nur in einer chinesischen arbeit von lu et al . [ 33 ] ein signifikanter vorteil bezglich des 1 - jahres - berlebens berichtet . 
bezglich der sequenziellen radiochemotherapie teilen die autoren mit : there was no evidence of clinical benefit with the sequential approach , either in terms of mortality , local control , dysphagia benefit and there were significant toxicities [ 52 ]  . 
 in allen radiochemotherapiestudien dominiert der anteil der plattenepithelkarzinome entsprechend der natrlichen biologischen verteilung der histologien bei weitem ( tabellen 2 und 3 ) , sodass histologiebezogene auswertungen mit vernftiger statistischer power nicht mglich sind . 
 das fazit ist , dass bei inoperablen lokoregional fortgeschrittenen sophaguskarzinomen durch eine primre radiochemotherapie das kurzzeitberleben innerhalb der ersten 2 jahre mglicherweise verbessert werden kann , sofern therapeut und patient bereit sind , therapiebedingte who grad - iii / iv - komplikationen und auch einzelne todesflle in kauf zu nehmen . 
die bisherigen radiochemotherapien sind unter palliativer zielsetzung somit kaum als standard zu empfehlen und unterliegen der einzelfallentscheidung , zumal gute lokale palliative effekte bei fortgeschrittenen sophaguskarzinomen auch mittels alleiniger bestrahlung erzielt werden knnen [ 8 , 40 , 50 , 51 ]  . 
nur die rtog - studie 85 - 01 [ 1 , 10 , 21 ] an berwiegend lokal begrenzten tumoren zeigte eine signifikante reduktion metachroner fernmetastasen im radiochemotherapiearzu diesem effekt existieren fr lokal fortgeschrittene sophaguskarzinome allerdings keine daten . 
primre radiochemotherapie fortgeschrittener sophaguskarzinome stand unter dem einfluss der gnstigen daten der rtog - studie zur simultanen radiochemotherapie und sollte in hnlicher weise in der hoffnung auf eine verbesserung der behandlungsergebnisse bei fortgeschrittenen sophguskarzinomen geprft werden . 
die dosierung der simultanen chemotherapie ( 5 - fu : 8001000 mg / m2 / d 15 als dauerinfusion und cisplatin : 20 mg / m2 / d 15 ) war damals nicht unblich und erschien der tumorlast unseres patientengutes angepasst und vertretbar , zumal die chemotherapie zur vermeidung kumulativer toxizitt bei den genannten kriterien sofort und definitiv beendet werden sollte [ 11 , 26 , 35 , 53 ]  . 
 [ 44 ] , dass bei einem patientengut mit berwiegenden t3 , n + - stadien und reduziertem allgemeinzustand eine simultane cisplatinhaltige chemotherapie in kurativer dosierung kaum durchfhrbar ist , da bei 42% ( 21 / 50 ) unserer patienten die simultane chemotherapie schon nach einem zyklus abgebrochen werden musste und sich die ergebnisse der strahlentherapie lokoregional fortgeschrittener sophaguskarzinome wohl kaum verbessert htten . 
ob die korrelation der berlebenszeit mit der anzahl der chemotherapiezyklen ( abbildung 3 ) nur eine selektion der fittesten darstellt oder tatschlich ausdruck eines therapieeffektes ist , lsst sich anhand unserer studie nicht entscheiden . 
die radiochemotherapie konnte die progression der fernmetastasierung nicht verhindern . urschlich war mglicherweise die a priori vorhandene groe tumorlast mit berwiegend langstreckigen tumoren und lokoregionaler metastasierung und die geringe systemische intensitt der chemotherapie , die bei den meisten patienten vorzeitig abgebrochen werden musste . 
 schlussfolgerungen als fazit kann aus heutiger sicht konstatiert werden , dass der benefit der primren simultanen radiochemotherapie mit 5 - fu / cisplatin bei lokoregional oder systemisch fortgeschrittenen sophaguskarzinomen allenfalls marginal ist . 
insbesondere patienten in hherem alter , mit fortgeschrittener tumorlast ( langstreckige tumoren > 5 cm , metastasen ) oder schlechtem allgemeinzustand profitieren hinsichtlich der restlebenszeit kaum noch von einer strahlenbehandlung , wie schon ltere verffentlichungen [ 18 , 31 ] gezeigt haben , zumal die ernhrung durch moderne endoskopische verfahren ( laserung , peg ) schneller und effektiver wiederhergestellt werden kann . 
al - sarraf m , martz k , herskovic a , leichman l , brindle js , vaitkevicius vk , cooper j , byhardt r , davis l , emami b . 
cooper js , guo md , herskovic a , macdonald js , martenson ja , al - sarraf m , byhardt r , russell ah , beitler jj , spencer s , asbell so , graham mv , leichman ll . 
hatlevoll r , hagen s , hansen hs , hultvorn r , jakobsen a , mntyl m , modig h , munck - wikland e , nygaard k , rosengren b , tausjf j , elgen k . bleomycin / cisplatin as neoadjuvant chermotherapy before radical radiotherapy in localized , inoperable carcinoma of the esophagus . 
hishikawa y , miura t , oshitani t , yoshimura h , ono k , takahashi m , nakajima t , murakami m , ikeda h , imanaka k , chatani m , inoue t . 
isenberg g , chak a , canto mi , levitan n , clayman j , pollack bj , sivak v jr . endoscopic ultrasoung in restaging of esophageal cancer after neoadjuvant chemoradiation . 
5 urban & vogel strahlentherapie und onkologie aktuelles forum wo stehen wir bei der behandlung des nasopharynxkarzinoms ? gabriele beckmann , michael flentje1 ziel : bersicht ber die entwicklung kombinierter behandlungsstrategien beim nasopharynxkarzino ergebnisse : die strahlentherapie ist akzeptierte standardtherapie bei der behandlung des nasopharynxkarzinoms . 
 schlussfolgerungen : um die bedeutung der beiden komponenten strahlentherapie und chemotherapie in der behandlung der nasopharynxkarzinome zu klren , mssen patienten mit unterschiedlichen histologischen subtypen nach einheitlichen schemata behandelt werden . 
nur so wird es mglich sein , stadiengerechte behandlungskonzepte , die zudem die tumorbiologie bercksichtigen , festzulegen . schlsselwrter : nasopharynxkarzinom prognosefaktoren alleinige bestrahlung kombinierte radiochemotherapie strahlenther onkol 2003 ; 179 : 28391 doi 10.1007 / s00066 - 003 - 1086 - 0 present status of treatment in nasopharyngeal carcinoma ? aim : review of the evolution of combined treatment strategies in nasopharyngeal carcinoma . 
it is hardly possible to compare the results of recent and historical trials because of different staging systems and because nasopharyngeal cancer occurring in the oceano - asian region are biologically different to those in western countries . 
aufgrund der lage des primrtumors in schdelbasisnhe , die bei fortgeschrittenen lokalbefunden hufig infiltriert ist , und der ausdehnung in den parapharyngealraum sind die mglichkeiten einer chirurgischen intervention limitiert , eine resektion in sano ist nur selten zu erreichen . 
darunter sind hervorzuheben die klassifikation der union international contre cancer ( uicc ) von 1992 , die der vorangehenden ajcc - version von 1988 fast entspricht , die berarbeitete fnfte version des american joint committee on cancer ( ajcc ) von 1997 , die im asiatischen raum gebruchliche klassifikation nach ho . 
im durchschnitt befinden sich 510% der patienten bereits bei diagnosestellung in einem metastasierten stadiubis zu 30% der patienten entwickeln auch bei anhaltender lokaler kontrolle im weiteren krankheitsverlauf fernmetastasen , wobei eine abhngigkeit vom ausma der zervikalen lymphknotenmetastasierung und vom t - stadium bei primrdiagnose besteht [ 5 , 38 , 40 , 44 ]  . 
 wegen der tendenz zur fernmetastasierung und der vergleichsweise hohen chemosensibilitt sind viele anstze unternommen worden , eine zytostatische systemtherapie in das primre behandlungskonzept zu integrieren und so die gesamtberlebensrate zu verbessern . 
die weiterentwicklungen auf den gebieten diagnostik , bestrahlungsplanung und gertetechnik haben zur verbesserung der strahlentherapieergebnisse im verlauf der letzten jahrzehnte infolge einer exakteren definition und erfassung des zielvolumens gefhrt [ 4 , 5 , 22 , 29 , 34 , 40 , 48 ]  . darber hinaus wurden analog zu anderen hno - tumoren intensivierte fraktionierungsschemata geprdarunter traten hohe remissionsraten , aber auch erhhte akutund spttoxizitten , v.a. 
 eine verbesserung des progressionsfeien berlebens bei akzeptabler spttoxizitt wurde nach akzelerierter bestrahlung mit sechs fraktionen pro woche gegenber der fnfmal wchentlichen fraktionierung , jeweils bis zur gesamtdosis von 66 gy , gesehen [ 30 ]  . 
 eine studie [ 47 ] aus hongkong musste dagegen nach randomisation von 159 der 400 geplanten patienten abgebrochen werden , weil sich in drei fllen nach der hyperfraktioniert - akzelerierten bestrahlung eine enzephalopathie des temporallappens entwickelte . 
hinzu kam die zunahme auch anderer neurologischer sptkomplikationen ( hirnnervenlhmung , myelopathie , schdigung von nervus opticus und chiasma ) im vergleich zur normfraktionierten standardtherapie . die behandlungsergebnisse unterschieden sich nicht , wobei die aussagekraft diesbezglich durch den vorzeitigen abbruch eingeschrnkt ist . 
 wegen der beschriebenen zns - nebenwirkungen und des mangelnden nachweises , dass intensivierte fraktionierungsschemata einen vorteil hinsichtlich lokaler kontrolle und berleben ergeben , muss zum gegenwrtigen zeitpunkt die konventionelle fraktionierung mit einzeldosen von 1 , 82 , 0 gy einmal tglich als standard gelten . 
 nach abschluss einer phase - ii - studie zur neoadjuvanten chemotherapie mit cisplatin und epirubicin begann die asian - oceanian clinical oncology association eine prospektiv randomisierte multizentrische phase - iii - studie [ 14 ]  . 
339 patienten mit who - iioder who - iii - histologie im stadium t3 / 4 oder n2c / 3 , m0 wurden in den arm alleinige radiotherapie ( 70 gy am primrtumor , 65 gy an lymphknotenmetastasen ) oder in den arm neoadjuvante chemotherapie vor bestrahlung eingebracht . 
das restaging 3 monate nach abschluss der gesamten therapie ergab im kombinationsarm zwar signifikant mehr komplette remissionen als im radiotherapiearm ( 55% gegenber lediglich 34% ) , insgesamt sind die ergebnisse jedoch im vergleich zu anderen studien schlecht . 
progressionsrate mit 55 / 171 im kombinationsarm und 92 / 168 im radiotherapieares traten weniger lokoregionre rezidive und weniger fernmetastasen auf . trotzdem war das gesamtberleben zum zeitpunkt der zwischenauswertung nicht signifikant unterschiedlich . 
 adjuvante chemotherapie die adjuvante chemotherapie nach strahlentherapie wird in erster linie mit dem ziel durchgefhrt , mikrometastasen zu vernichten . in einer randomisierten , von mailand ausgehenden multicenterstudie [ 42 ] wurden zwischen dezember 1979 und dezember 1983 von insgesamt 352 registrierten patienten ( stadien iiv ) nur diejenigen 229 patienten randomisiert , die nach einer radiatio mit einer gesamtdosis von 6070 gy eine komplette oder partielle remission erreicht hatten . 
bei der wahl des chemotherapieregimes , fr das erfahrungen in der palliativtherapie bei metastasierten nasopharynxkarzinomen bestand , wurde auf die gabe von cisplatin als einem der wirksamsten medikamente verzichtet , die gewhlten zytostatika waren niedrig dosiert , die resorptionsverhltnisse von cyclophosphamid nach peroraler gabe unklar . 
 auch die kombination aus neoadjuvanter chemotherapie , radiatio und adjuvanter chemotherapie wurde in einer kleineren prospektiv randomisierten studie [ 8 ] bei 82 patienten mit who - iii - tumoren gepr im ersten arm wurden zwei neoadjuvante zyklen cisplatin und 5 - fu , gefolgt von einer normfraktionierten radiatio mit mindestens 66 gy ( ggf . endokavitrer brachytherapieboost bei parapharyngealem befall ) , und vier zyklen adjuvanter chemotherapie gegeben und im zweiten arm mit der entsprechenden alleinigen radiatio verglichen . 
die chemotherapie hatte auch hier auf das krankheitsfreie berleben ( arm 1 : 68% , arm 2 : 72% ) , das gesamtberleben ( arm 1 : 80% , arm 2 : 80 , 5% ) nach 2 jahren und auf das rezidivmuster keinen einfluss . 
 die vorgestellten studienkonzepte zur neoadjuvanten und adjuvanten chemotherapie sind zwar heterogen , einheitlich zeigt sich jedoch , dass eine neoadjuvante chemotherapie in groen randomisierten studien trotz initial hoher ansprechraten keinen therapeutischen nutzen gebracht hat eine signifikante verbesserung der gesamtberlebensrate war nicht nachweisbar , whrend das krankheitsfreie berleben zumindest tendenziell verbessert wurde . 
die chemotherapie selbst hat zum teil gravierende substanzspezifische nebenwirkungen ( belkeit , erbrechen , niereninsuffizienz , pulmonale toxizitt , hmatotoxizitt mit septischen komplikationen ) , das ausma der akuttoxizitt der nachfolgenden strahlentherapie , insbesondere mukositis , wird jedoch nicht erhht . 
rfs / dfs = rezidivfreies / krankheitsfreies berleben , os = gesamtberleben , fdm = kein auftreten von fernmetastasen , = erste rezidivmanifestation als fernmetastase bei % der patienten , ^ = anzahl der patienten mit fernmetastasen , ec = epirubicin , cisplatin , bec = bleomycin , epirubicin , cisplatin , bc / 5 - fu = bleomycin , cisplatin , 5 - fu , p / 5 - fu / lv = cisplatin / 5 - fu / leukovorin , vca = vincristin , cyclophosphamid , adriamycin , cddp = cisplatin , n.s. 
diese substanz besitzt beim nasopharynxkarzinom sowohl in der neoadjuvanten als auch in der palliativen therapie ( responseraten bei kombinationschemotherapie 5091% , auch komplette remissionen ) eine nachgewiesene wirkung [ 7 ]  . 
 die rtog - 8117 - studie hatte die durchfhrbarkeit einer simultanen radiochemotherapie mit cisplatin 100 mg / m2 alle 3 wochen geprdie auswertung der 27 patienten mit nasopharynxkarzinom ergab im vergleich zu einem historischen kontrollkollektiv mit alleiniger radiotherapie ein besseres krankheitsfreies und gesamtberleben sowie eine geringere inzidenz von fernmetastasen [ 3 ]  . 
die toxizittsanalyse ergab vermehrt schleimhauttoxizitten und gradiii / iv - hmatotoxizitten unter der radiochemotherapie , sodass bei 13 von 78 patienten die therapie abgebrochen wurde . im radiotherapiearm waren keine abbrche ntig . 
 auf dem asco 2001 wurde eine aktualisierte auswertung prsentiert , die die ergebnisse der interimsanalyse mit einem 5 - jahres - gesamtberleben von 37% im standardarm und 67% im experimentalarm besttigte [ 1 ]  . 
 zum einen wurden im vergleich zu anderen studien im radiotherapiearm deutlich schlechtere ergebnisse erzielt . trotzdem ist eine 5 - jahres - berlebensrate von 67% deutlich hher , als aufgrund historischer daten erwartet wurde . 
der hhere anteil an weniger strahlensensiblen tumoren mit who - i - histologie in der intergroup - studie [ 1 , 2 ] ( 28% der patienten im radiochemotherapiearm und 22% im radiotherapiearm ) als im asiatischen raum knnte die diskrepanz der ergebnisse erklren . 
dem ist entgegenzuhalten , dass nicht zuletzt aufgrund von complianceproblemen nur die hlfte der patienten die adjuvante chemotherapie protokollgerecht erhielt und es keine daten gibt , die den stellenwert einer alleinigen adjuvanten chemotherapie belegen . 
blickt man auf die resultate der metaanalysen zur radiochemotherapie bei anderen tumoren im hno - bereich , dann zeigen auch diese weder fr neoadjuvante noch fr adjuvante chemotherapie , sondern nur fr die simultane radiochemotherapie eine verbesserung des gesamtberlebens [ 18 , 39 ]  . 
 die these , dass die verschiedenen histologischen subtypen unterschiedliches biologisches verhalten zeigen , wurde zwar in keiner randomisierten studie verifiziert , aber durch die beobachtung unterschiedlicher ansprechraten und rezidivraten gesttzt . 
da auch ethnische unterschiede im ansprechen auf chemotherapie diskutiert werden , stellt sich die frage , ob sich aus den ergebnissen der intergroup - studie [ 1 , 2 ] konsequenzen fr die therapie von nasopharynxkarzinomen im asiatischen raum ableiten lassen . 
 der ansatz der simultanen radiochemotherapie wurde in einer weiteren randomisierten phase - iii - studie [ 9 ] in hongkong gepr350 patienten mit fortgeschrittener lymphknotenmetastasierung wurden aufgenommen , 94% mit whoiii - histologie . 
von den geplanten acht zytostatikaapplikationen konnten bei 78% der patienten mindestens vier gegeben werden . bei hnlicher lokaler toxizitt war das progressionsfreie berleben nach 2 jahren nicht signifikant unterschiedlich ( kombinationsarm 76% , radiotherapiearm 62% )  . 
 auch andere untersucher griffen das konzept der simultanen radiochemotherapie mit modifiziertem chemotherapieschemata auf [ 20 ] und zeigten die durchfhrbarkeit und effizienz in kombination mit einer neoadjuvanten chemotherapie [ 41 ] und adjuvanten chemotherapie [ 10 , 12 , 45 ]  . 
bei kleinen patientenzahlen in den genannten , nicht randomisierten studien wurde im vergleich zur alleinigen radiotherapie in frhen stadien i / ii kein signifikanter vorteil der radiochemotherapie auf lokale kontrolle und gesamtberleben gesehen [ 10 ]  . 
 mit dieser intention haben die hongkong nasopharyngeal cancer study group und das canadian cancer center eine prospektiv randomisierte multizenterstudie ( npc 99 - 01 ) aufgelegt , in die patienten mit nicht verhornenden plattenepitheloder undifferenzierten karzinomen ( nicht who - ioder adenokarzinome ) der stadien t14 n23 nach uicc 1997 aufgenommen werden . 
in arm b wird cisplatin in einer dosierung von 100 mg / m2 alle 3 wochen simultan zur radiatio gegeben , gefolgt von drei zyklen adjuvanter chemotherapie mit cisplatin 80 mg / m2 , d 1 und 5 - fu 1000 mg / m2 , d 14 . arm c wurde im august 2000 aktiviert und prft neoadjuvant 3 ( cid : 1 ) cddp 100 mg / m2 , d 1 mit 5 - fu 1000 mg / m2 , d 15 alle 3 wochen mit anschlieender radiatio wie in arm a . 
 schlussfolgerungen zum jetzigen zeitpunkt gilt die kombination aus konventionell fraktionierter und 3 - d - geplanter konformaler bestrahlung mit einer chemotherapie als standard zumindest beim fortgeschrittenen nasopharynxkarzino die bislang publizierten studien unterscheiden sich bezglich der radiotherapiegesamtdosis und - fraktionierung sowie in der wahl der zytostatikakombinationen . 
 um die bedeutung der chemotherapie in den verschiedenen tund n - stadien , insbesondere auch bei t1 / t2 - tumoren , zu klren und dabei die verschiedenen histologischen entitten und ethnischen gruppen zu bercksichtigen , sind weitere randomisierte , am besten multinationale studien erforderlich , die entsprechende subgruppenanalysen zulassen . 
al - sarraf m , pajak tf , cooper js , mohiuddin m , herskovic a , ager pj . chemo - radiotherapy in patients with locally advanced nasopharyngeal carcinoma : a radiation therapy oncology group study . 
preliminary report of the asian - oceanian clinical oncology association randomized trial comparing cisplatin and epirubicin followed by radiotherapy versus radiotherapy alone in the treatment of patients with locoregionally advanced nasopharyngeal carcinoma . 
hong s , wu hg , chie ek , bang yj , heo ds , kim kh , sung mw , park ci . neoadjuvant chemotherapy and radiation therapy compared with radiation therapy alone in advanced nasopharyngeal carcinoma . 
retrospective analysis on treating nasopharyngeal carcinoma with accelerated fractionation ( 6 fractions per week ) in comparison with conventional fractionation ( 5 fractions per week ) : report on 3 - year tumor control and normal tissue toxicity . 
munter mw , debus j , hof h , nill s , haring p , bortfeld t , wannenmacher m . inverse treatment planning and stereotactic intensity - modulated radiation therapy ( imrt ) of the tumor and lymph node levels for nasopharyngeal carcinomas . 
sanguineti g , geara fb , garden as , tucker sl , ang kk , morrison wh , peters lj . carcinoma of the nasopharynx treated by radiotherapy alone : determinants of local and regional control . 
5 urban & vogel strahlentherapie und onkologie original article acute side effects during 3 - d - planned conformal radiotherapy of prostate cancer differences between patients self - reported questionnaire and the corresponding doctors report gregor goldner , natascha wachter - gerstner , stefan wachter , karin dieckmann , monika janda , richard ptter1 background : radiotherapy - induced side effects are often scored retrospectively according to the eortc / rtog scores for organs at risk by reviewing the medical records . 
 patients and methods : 47 patients with prostate cancer were questioned about their side effects by a radiotherapist and asked to fill in a questionnaire at the start , in the middle and at the end of radiotherapy . 
the data of this questionnaire and the doctors report were scored according to the german version of the eortc / rtog scores for gastrointestinal ( gi ) and genitourinary ( gu ) side effects and subsequently compared . 
we distinguished between moderate disagreement ( better / worse by one grade , assessed by the doctor ) and pronounced disagreement ( better / worse by two grades , assessed by the doctor )  . 
comparing doctors reports with patients questionnaires , for gi side effects an agreement was found in 22 / 47 patients , moderately better scores by the doctors report were found in 13 / 47 patients , and moderately worse scores in 9 / 47 patients on average . 
for gu side effects an agreement was seen in 22 / 47 patients , moderately better scores in 17 / 47 patients and moderately worse scores in 3 / 47 patients . 
if the eortc / rtog score is used in its original english version , a difference is found , particularly in the assessment of gu side effects , resulting in an higher amount of agreement concerning gu side effects and a minor amount of pronounced disagreement . 
 conclusion : in order to evaluate radiation - induced side effects , a patients self - reported questionnaire should be included in the analysis of morbidity , above all for grade 0 , 1 , and 2 side effects . 
the validity of data seems to be questionable , particularly in the assessment of grade 0 , 1 and 2 side effects , if only data from the doctors reports are taken into account . 
the german version of the eortc / rtog score not including the pretreatment status leads to different results , particularly in the assessment of grade 0 , 1 , and 2 urinary side effects , which asks for a revision . 
 key words : radiotherapy prostate cancer acute side effects eortc / rtog score german version patient questionnaire doctors report strahlenther onkol 2003 ; 179 : 3207 doi 10.1007 / s00066 - 003 - 1029 - 9 akute nebenwirkungen der strahlentherapie bei 3 - d - geplanter konformaler bestrahlung des prostatakarzinoms . 
einige studien konnten ein beroder unterschtzen von nebenwirkungen durch den arzt nachweisen . ziel dieser studie war es , prospektiv die unterschiede zwischen der erhebung von nebenwirkungen durch den arzt und den patienten festzustellen . 
 patienten und methodik : 47 patienten mit prostatakarzinom wurden von einem strahlentherapeuten zu ihren nebenwirkungen befragt und gebeten , einen fragebogen bezglich der nebenwirkungen zu beginn , in der mitte und am ende der radiotherapie auszufllen . 
die daten aus fragebogen und arztbericht wurden von zwei strahlentherapeuten anhand der deutschsprachigen version der eortc / rtog - scores fr gastrointestinale ( gi ) und urogenitale ( ug ) nebenwirkungen graduiert und verglichen . 
bei diffe1 department of radiotherapy and radiobiology , general hospital of vienna , medical school , university of vienna , austria . received : march 25 , 2002 ; accepted : january 17 , 2003 strahlenther onkol 2003 no . 
acute side effects of radiotherapy for prostate cancer renzen wurde zwischen moderaten abweichungen ( vom arzt um einen grad besser / schlechter bewertet ) und deutlichen abweichungen ( vom arzt um zwei grade besser / schlechter bewertet ) unterschieden . 
 ergebnisse : die giund ug - nebenwirkungen nahmen whrend der strahlenbehandlung im arztgesprch und im patientenfragebogen zu ( tabellen 1 und 2 ) die gi - nebenwirkungen zeigten im vergleich zwischen arzteinschtzung und patientenfragebogen eine bereinstimmung im durchschnitt von 22 / 47 patienten , moderat bessere bewertungen durch den arzt bei 13 / 47 und moderat schlechtere bei 9 / 47 patienten . 
bei den ug - nebenwirkungen konnten im durschnitt eine bereinstimmung bei 22 / 47 patienten , moderat bessere bewertungen durch den arzt bei 17 / 47 und moderat schlechtere bei 3 / 47 patienten nachgewiesen werden . 
bei beurteilung der nebenwirkungen anhand des englischen eortc / rtog - scores zeigt sich ein anderes bild , vor allem die urogenitalen nebenwirkungen betreffend ( grnde fr deutliche ber - / unterschtzung : tabelle 5 )  . 
die deutsche version des eortc / rtogscores fhrt , ohne bercksichtigung des nullzeitpunkts , zu anderen ergebnissen , vor allem bei der beurteilung von ug - nebenwirkungen grad 0 , 1 und 2 , sodass eine revision notwendig erscheint . 
 schlsselwrter : strahlentherapie prostatakarzinom akute nebenwirkungen eortc / rtog - score deutsche version patientenfragebogen arztbericht introduction curative treatment of prostate cancer aims at achieving a high rate of local tumor control with a low rate of side effects . 
3 - dplanned conformal radiotherapy allows small - volume radiation therapy of the prostate and therefore spares the organs at risk the urinary bladder and the rectum [ 7 , 8 , 19 , 23 , 24 , 26 , 30 ]  . the evaluation of radiation - induced acute side effects in the treatment of prostate cancer is of great importance when comparing radiotherapy with other treatment options . 
side effects are mostly evaluated retrospectively and scored according to the eortc / rtog criteria [ 13 , 9 , 10 , 13 , 14 , 16 , 20 , 21 , 27 , 32 ]  . 
 however , several studies have already shown a discrepancy between patients self - reported questionnaires and assessment of side effects by doctors or nursing stuff regarding side effects or quality of life [ 5 , 6 , 12 , 17 , 18 , 25 , 29 , 31 ]  . watkins - bruner et al [ 29 ] showed an agreement of grade 0 side effects for diarrhea in 56% and for dysuria in 75% between the doctors report and the patients self - reported questionnaire assessment . 
 youngblood et al [ 31 ] compared the patients self - reports on the number of symptoms ( identified with the oncology treatment toxicity assessment tool ) to the number of symptoms documented in the medical records ( by either the nurses or the physician ) and found a significant underestimation by the medical professionals . 
 the assessment of side effects in general either by the doctor or the patient remains clearly related to a subjective point of view besides all the objective parameters established in the different scoring systems . 
a total dose of 66 gy at the icru point was prescribed with single doses of 2 gy , five times a week , using a four - field box technique [ 26 ]  . 
 all 47 patients were asked to fill in an in - house developed questionnaire on side effects ( see appendix 1 ) at the start ( week 2 ) , in the middle ( week 4 ) , and at the end ( week 7 ) of radiotherapy . 
patients were asked to answer no , a little , yes and very much to the questions on general well - being , and the questions regarding pain , urge to have stool , mucus or blood in stool or urine , and uncontrolled loss of stool or urine ( four scales )  . 
frequency of stool and urine had to be filled in with the corresponding numbers by the patients . five questions regarding the management of side effects had to be answered with yes / no . 
 the patients answers and the medical reports were evaluated retrospectively by two experienced radiooncologists according to the german version of the eortc / rtog acute radiation morbidity scoring criteria [ 22 ] ( see appendix 2 ) for acute gi and gu side effects at the start , during , and at the end of radiotherapy . 
distribution of acute gastrointestinal side effects at the start ( week 2 ) , in the middle ( week 4 ) , and at the end ( week 7 ) of radiotherapy ( rt )  . 
verteilung der akuten gastrointestinalen nebenwirkungen zu beginn ( woche 2 ) , in der mitte ( woche 4 ) und am ende ( woche 7 ) der strahlentherapie ( rt )  . 
 eortc / rtog start of rt start of rt middle of rt middle of rt end of rt end of rt ( week 7 ) ( week 4 ) german patient doctor version ( week 4 ) patient ( week 2 ) patient ( week 2 ) doctor ( week 7 ) doctor grade 0 grade 1 grade 2 missing total grade 0 grade 1 grade 2 missing total table 2 . 
distribution of acute genitourinary side effects at the start ( week 2 ) , in the middle ( week 4 ) , and at the end ( week 7 ) of radiotherapy ( rt )  . 
verteilung der akuten urogenitalen nebenwirkungen zu beginn ( woche 2 ) , in der mitte ( woche 4 ) und am ende ( woche 7 ) der strahlentherapie ( rt )  . 
 eortc / rtog start of rt start of rt middle of rt middle of rt end of rt ( week 7 ) german doctor version ( week 4 ) patient ( week 4 ) doctor ( week 2 ) doctor ( week 2 ) patient end of rt ( week 7 ) patient results the patients median age at the time of radiation therapy was 70.6 years ( 5585 years )  . 
concerning the patients compliance which was very good regarding filling in the questionnaire only eight scores could not be evaluated due to missing questionnaires ( at the start of radiotherapy : one patient ; at the end : three patients )  . 
 gi and gu side effects are shown in detail in tables 1 and 2 at three time points during radiotherapy for the patients questionnaires and doctors reports for the different scores ( 02 )  . 
 the differences between the of the eortc / rtog score ( german version ) obtained from the doctors reports and the score obtained from the patients questionnaires are shown in detail in tables 3 and 4 and in figure 1 . 
we distinguished between full agreement , moderate disagreement ( assessed by the doctor by one grade better or worse ) , and pronounced disagreement ( assessed by the doctor by two grades better or worse )  . 
 discussion in the present study , discrepancies between side effects scored on the basis of patients questionnaires and medical professionals reports were found comparable to other studies [ 5 , 6 , 12 , 17 , 25 , 27 , 29 , 31 ]  . 
distribution of differences of gastrointestinal ( gi ) and genitourinary ( gu ) side effects according to the german version of eortc / rtog [ 22 ] criteria between doctors and patients records . 
verteilung der abweichungen der akuten gastrointestinalen ( gi ) und urogenitalen ( ug ) nebenwirkungen nach der deutschen version der eortc / rtog - kriterien [ 22 ] zwischen arztgesprch und patientenfragebogen . 
bereinstimmung : keine differenz zwischen arztgesprch und patientenfragebogen ; moderater unterschied : differenz zwischen arztgesprch und patientenfragebogen um einen grad ; starker unterschied : differenz zwischen arztgesprch und patientenfragebogen um zwei grade . 
distribution of moderate and pronounced disagreement regarding acute gastrointestinal ( gi ) and genitourinary ( gu ) side effects according to the german version of eortc / rtog criteria [ 22 ] between doctors and patients records . 
 + 1 / + 2 : doctor judges condition of patient about one / two scores better ; 1 / 2 : doctor judges condition of patient about one / two scores worse . 
verteilung der moderaten und deutlichen abweichungen , unterteilt in berund unterschtzung der akuten gastrointestinalen ( gi ) und urogenitalen ( gu ) nebenwirkungen nach der deutschen version der eortc / rtog - kriterien [ 22 ] zwischen arztgesprch und patientenfragebogen . 
fossa et al [ 6 ] showed that doctors underestimated the disturbance of sexual life in patients who had undergone androgen deprivation therapy , but overestimated the impairment of quality of life and psychologic distress experienced by these patients . 
vogelzang et al [ 25 ] designed a survey to characterize the epidemiology of cancer - related fatigue and pain from the of the patients , primary caregivers , and oncologists perspectives . 
although oncologists believed that pain adversely affected their patients to a greater degree than fatigue ( 61% vs 37% ) , patients felt that fatigue adversely affected their daily lives more than pain ( 61% vs 19% )  . moderate disagreement ( + 1 ) moderate disagreement ( 1 ) pronounced disagreement ( + 2 ) pronounced disagreement ( 2 ) watkins - bruner et al [ 29 ] found moderate disagreement on dysuria in 13% and on diarrhea in 31% . 
pronounced disagreement was reported both for dysuria and diarrhea in 13% . compared to our study , the amount of agreement in the study of watkins - bruner was similar for diarrhea with 56% and more frequent for dysurie with 75% . 
reasons for less agreement as found out in the present study are difficult to state clearly , but might be the following : three different time periods for evaluation with differences in agreement / disagreement ( figure 1 ) ; use of the german version of the eortc / rtog score [ 22 ] that implies a quantitative documentation of the absolute urination frequency and an attribution of daily urination frequency of more than six to grade 2 the question as to the causes of such discrepancies remained unanswered in the study of watkins - bruner et al [ 29 ] our study showed a large amount of moderate disagreement . 
this was most often observed in the attribution to grade 0 and grade 1 side effects ( 60% for gi and 73% for gu side effects ) and less often in the attribution to grade 1 and 2 side effects ( 40% for gi and 27% for gu side effects )  . 
with regard to the outcome of studies dealing with morbidity in general , grade 0 , 1 , and 2 acute and late side effects are most often reported when following the eortc / rtog score . 
grade 3 side effects are only rarely described [ 1 , 4 , 8 , 10 , 11 , 1316 , 21 , 23 , 27 , 28 , 32 ]  . grade 1 side effects during or after radiotherapy for prostate cancer seem to be more or less acceptable , as they represent only minor changes in the performance of daily life . 
grade 2 side effects , however , seem to represent some more pronounced change in daily life with some discomfort and can thus be regarded as the most important side effects during or after radiotherapy for prostate cancer , if the rate of grade 3 side effects ( or more ) approaches 0 . 
acute side effects of radiotherapy for prostate cancer start of rt week 2 middle of rt week 4 end of rt week 7 start of rt week 2 middle of rt week 4 end of rt week 7 moderate disagreement pronounced disagreement moderate disagreement pronounced disagreement figure 1a abbildung 1a figure 1b abbildung 1b figures 1a and 1b . 
acute gastrointestinal ( gi ; a ) and genitourinary ( gu ; b ) side effects : distribution of differences between doctors and patients records according to the german version of eortc / rtog score [ 22 ]  . 
moderate disagreement : difference about one score ( dark grey ) ; pronounced disagreement : difference about two scores ( light grey ) ; positive values : overestimation by the doctor ; negative values : underestimation by the doctor . 
akute gastrointestinale ( gi ; a ) und urogenitale ( gu ; b ) nebenwirkungen : verteilung der abweichungen zwischen arztgesprch und patientenfragebogen nach der deutschen version des eortc / rtog - scores [ 22 ]  . 
moderater unterschied : differenz um einen grad ( dunkelgrau ) ; starker unterschied : differenz um zwei grade ( hellgrau ) ; positive werte : arzt bewertet besser ; negative werte : arzt bewertet schlechter . 
there was only information with regard to a qualitative comparison : little higher frequency . this would be scored as 1 after the eortc / rtog score . however , in the questionnaire eleven patients recorded a frequency more than six times per day ( up to a maximum 15 times ) and per night resulting in a grade 2 side effect . 
 the german version [ 22 ] of the eortc / rtog score [ 2 ] includes a cutoff level for the frequency of urination six times per day discriminating between grade 1 and grade 2 acute ug side effects . 
in the original english version [ 2 ] this cutoff level is not given , and side effects related to urination are assessed by comparison with the pretreatment situation . grade 1 acute side effect are defined as a frequency of urination twice the pretreatment habit . 
the german way of scoring was the most frequent reason for disagreement in our study , as the physicians did a qualitative comparison ( little higher frequency ) , whereas the patients were asked to report the absolute numbers , which resulted in grade 0 or 1 for the doctors report and grade 1 or 2 for the patients report . 
 a patient with a daily urination frequency of four times before treatment and seven times during radiotherapy and no other symptoms is scored 0 in the original english version of eortc / rtog and 2 in the german version . 
during the regular clinical checkup during a fractionated course of radiotherapy , the doctor and the patient himself tend to compare the frequency of urination with the situation before the start of irradation . 
 underestimation genitourinary side effects gastrointestinal underestimation side effects overestimation 11 ( cid : 1 ) frequency of urination 1 ( cid : 1 ) drugs against dysuria 2 ( cid : 1 ) mucus in stool 1 ( cid : 1 ) medication against diarrhea 3 ( cid : 1 ) medication against pain strahlenther onkol 2003 no . 
acute side effects of radiotherapy for prostate cancer a patient with a daily urination frequency of five times before radiotherapy and seven times during irradiation would , in general , rate this change as small and of minor relevance , if at all . 
in any case such side effects have to be related to the pretreatment status and should then be graded in a reasonable way , reflecting the severity of the side effect itself and , if possible , also the subjective component of the side effect , which is , finally , the impairment of quality of life . 
it seems to be worthwhile to suggest a revision of the german version of the eortc / rtog score for the attribution of the frequency of urinary side effects to grade 1 and grade 2 . based on our experience , we would recommend to go back to the original english version and include the pretreatment status , in order to avoid an overestimation of this type of side effects on the one hand and a misunderstanding when reporting these side effects on an international level on the other hand . 
an agreement was found in a total of 26 / 47 ( vs 22 / 47 german version ) , a moderate disagreement in 17 / 47 ( vs 19 / 47 ) , and pronounced disagreement in 2 / 47 ( vs 4 / 47 ) with two patients missing in each comparison . 
 a questionnaire filled in by the patient ( in addition to a doctors report ) is essential to arrive at a comprehensive , valid and reliable evaluation of radiotherapy - induced side effects , in particular for the assessment of the true incidence of grade 0 , 1 , and 2 side effects . 
 strahlentherapie und onkologie original article dosimetric assessment of the field abutment region in head and neck treatments using a multileaf collimator khaled abdel - hakim1 , tetsuo nishimura1 , michikatsu takaih2 , shuji suzuki2 , harumi sakahara1 background and purpose : the use of conventional asymmetric collimators for junctioning of abutted fields can lead to significant dose inhomogeneity , due to jaw misalignment . 
 material and methods : to define either the anterior or the lateral fields , the mlc was used with either the longitudinal ( 0 angle ) or the transverse ( 90 angle ) settings . 
for 0 setting , each leaf moves in a direction perpendicular to the gantry rotation axis , hence the tongue and groove ( t&g ) design can effect matching - area dose at the side of the leaf ( figure 1a )  . 
four combinations of abutted anterior field and abutted lateral field defined by mlc , i.e. , abutted using mlc side - by - side , side - by - end , end - by - side and end - by - end , were compared ( table 1 )  . 
abutted fields using mlc sideby - end produced > 10% overdose that could be improved to 1% for 0.5 mm overlap of the leaf end from the lateral portals ( figure 4 )  . 
end - by - end showed an overdose of > 20% ( figure 3b )  . this overdose could be smoothed out by overlaps of both leaf ends by 0.8 mm from both lateral and anterior portals ( figure 6 )  . the ideal jaw position was found to be at 1 mm away from the beam central axis in any combination ( table 2 )  . 
 conclusion : the use of mlcs for photon field junction matching is appropriate and represents an alternative approach to the problem of field matching using the asymmetric jaws in head and neck treatments . 
 key words : multileaf collimators field matching dosimetry strahlenther onkol 2003 ; 179 : 3129 doi 10.1007 / s00066 - 003 - 1024 - 1 dosimetrische bewertung der feldanpassungsregion bei behandlungen im hals - nasen - ohren - bereich mit multileafkollimatoren hintergrund und ziel : die verwendung konventioneller asymmetrischer kollimatoren knnte durch geringfgiges versagen der kollimatorgeometrie zu einer signifikanten dosisinhomogenitt an der anpassungsregion benachbarter strahlenfelder ( matchline ) fhren . 
in dieser studie wurde die dosisinhomogenitt an der durch die multileafkollimatoren erzeugten feldanpassungsregion bei der strahlentherapie des hno - bereichs unter der bedingung einer drei - felder - bestrahlung mit einem isozentrum bewertet . 
 material und methodik : zur feldaufstellung wurden multileafkollimatoren verwendet , fr das anteriore feld die longitudinale ( 0 ) und fr das laterale feld die transversale kollimatoraufstellung ( 90 )  . 
bei 0 - aufstellung bewegt sich jeder multileafkollimator senkrecht zur gantry - rotationsache , und die tongue and groove - konfiguration erzeugt die dosis an der feldanpassungsregion der kollimatorseite ( abbildung 1a )  . 
 1 department of radiology , and 2 department of informatics , hamamatsu university school of medicine , hamamatsu , japan . received : march 19 , 2002 ; accepted : october 10 , 2002 strahlenther onkol 2003 no . 
matching using multileaf collimators ergebnisse : bei seit - zu - seit - aufstellung der multileaf - kollimatoren verursachten benachbarte felder eine unterdosierung von etwa 15% ( abbildung 3a )  . 
die seit - zu - end - aufstellung erzeugte eine berdosierung von > 10% , die aber durch eine berlappung der kollimatorenden der lateralen felder von 0 , 5 mm auf bis zu 1% reduziert werden konnte ( abbildung 4 )  . 
 schlsselwrter : multileaf - kollimator feldanpassung dosimetrie introduction in the treatment of head and neck primary cancers and their regions of nodal spread , field matching remains a dosimetric challenge [ 3 , 7 , 9 , 15 , 17 , 28 , 29 ]  . 
bilateral parallel - opposed fields are matched to the anterior lower neck ( aln ) field using a single isocenter . asymmetric collimators [ 20 , 25 ] provide half beams that make geometrically perfect match - planes possible . 
 the work of sohn et al [ 28 ] discussed the issue of dose uniformity across the junction of the three - field technique using asymmetric collimators and a single isocenter . 
they concluded that the dose variation is within 5% of the prescribed dose for a digital display tolerance of 1 mrecently , however , many investigators have studied the matching - area dose by creating gaps and overlaps within the specified tolerance . they concluded that collimator misalignment could produce inhomogeneities up to 40% [ 26 , 27 ] or 60% [ 11 ] above or below the prescribed dose for a 4 - mm overor underlap ( 1 mm for each collimator )  . 
maximum dose uniformity within the field - matching area of the treatment volume is important to accomplish for at least two reasons : to avoid reduced tumor control due to underdosage , and to avoid irreversible myelopathy due to radiation - induced damage of the spinal cord . 
several authors reported the acceptability of using mlcs as opposed to conventional blocks with regard to the dosimetry of the buildup and penumbra regions [ 2 , 5 , 6 , 12 , 13 , 16 , 18 , 23 , 24 ]  . 
 the objectives of this paper are : first , to present dosimetric characteristics of the matching area in a monoisocentric three - field irradiation of the head and neck using mlc for defining the junction , and second , to investigate the optimal setting and reproducibility of mlc leaves in order to reduce the magnitude of the introduced inhomogeneities . 
 material and methods multileaf collimator two varian 2100c linear accelerators ( varian associates , palo alto , ca , usa ) equipped with multileaf collimation were employed , using 4 - mv photons exclusively . 
these leaves project to 10.0 cm in length at isocenter , and the leaf span range ( maximum / minimum positions possible on the same carriage ) is limited to 14.5 cthe maximum available field size is 40 ( cid : 1 ) 40 cthe radial leaf direction is always parallel to the direction of motion of the lower x - jaw pair , i.e. , the mlc rotates with the main collimators . 
when the aperture of all mlc pairs was closed at the same stop position , the exposed film exhibited a straight line due to leakage through the rounded ends of the mlc . 
the check was performed following the procedures used by the american association of physicists in medicine ( aapm ) task group 40 [ 22 ] , that is light / radiation - field coincidence , gantry and collimator indicator , cross - hair centering , gantry and collimator rotation isocenter , coincidence of collimator and gantry axis with isocenter , and coincidence of radiation and mechanical isocenter . 
 mlc conformation mlc fields were designed for the two cardinal orientations of the collimators , since these are the only ones to be used in matching head and neck fields . 
in other cases , a better match to the blocked field can be only achieved at mlc 90 such that the shielding is well aligned with leaf movement ( figure 1b )  . 
accordingly , abutting half - beam blocked fields are described as : side - by - side , sideby - end , end - by - side , or end - by - end abutment ( table 1 )  . 
a ready - packed therapy verification film ( kodak xv2 , eastman kodak co . , rochester , ny , usa ) was inserted between two 30 ( cid : 1 ) 30 ( cid : 1 ) 5 cm solid water slabs . 
also , the top side of the film package was bent and taped at the surface to minimize the edge effect as the photon beam entered the phantowe chose field sizes that are most frequently used in clinical settings ; these were asymmetric 20 ( cid : 1 ) 10 cm and 12 ( cid : 1 ) 10 cm for anterior and lateral fields , respectively . 
in endby - end abutment ( figure 3b ) , a hot region > 20% was observed when the fields abut at the beam central axis . in side - by - end abutment ( figure 4 ) , film dosimetry showed a hot region between the two abutted fields with an overdose > 10% . 
in end - by - side abutment ( figure 5 ) , an area of overdose > 10% was observed . this could improve to uniform dose when the mlc leaves were moved by 0.8 mm across the beam central axis . 
on the other hand , jaw setting at 2 mm or more away from the beam central axis would definitely lead to pronounced round - ended effect of the leaf end or increased transmission of radiation to the patient . 
to test the reproducibility of mlc alignment and optimal overlap , we repeated the measurement a total of four times over a 1 - year period . optical density profiles were measured using a film scanner ( microdensitometer 2405 , abe sekkei co . , tokyo , japan ) with an aperture size of 0.1 ( cid : 1 ) 1.0 mm and a scanning pitch of 0.1 mfilms were scanned at 5 cm depth in the superior - inferior direction . 
schematic illustration of field arrangement and film positioning with respect to a solid water phantom . the multileaf collimator was tested and found to be within the manufacturers [ 30 ] and task group 40s [ 22 ] specifications of abbildung 2 . 
 the full width at half maximum ( fwhm ) , which is the width of the distribution halfway between the peak dose and a relative dose of 100% , ranged from 4.5 mm to 8 mm for any combination of field abutment . 
however , because of inherent mechanical and electronic tolerances , it is unavoidable that a junction will not be perfectly abutted . many authors have reported unacceptable overor underdose figure 3a abbildung 3a figure 3b abbildung 3b figures 3a and 3b . 
although we have not seen severe complications in the match - plane when using the monoisocentric technique , there is always some doubt about the accuracy and uniformity of the dose at the junction of the lateral and the anterior portals . 
using asymmetric collimators , 60% or 40% above or below the prescribed dose should concern the oncologist about the complications or the ability to effectively irradiate all sites of disease . 
however , the use of a penumbra generator has some disadvantages , such as the increase in the volume receiving an inhomogeneity , labor - intensive fabrication and mounting , the need to reenter the treatment room during treatment , figure 6 . 
die profile angepasster felder ( end - zu - end - aufstellung ) ergeben in der grenzzone > 20% berdosierung ohne berlappen aufgrund gewlbter enden ( film 6 )  . 
 jaw setting matching - area dose 0 mma 1 mmb 8 mma 1 mmb 28% 15% + 33% + 24% amanufacturers recommended jaw position ; bproposed jaw position the lifting of tray - mounted blocks , and inaccuracy in the tray position . 
in order to minimize any change in penumbra width , the ends of the leaves are rounded to keep divergent rays tangent to the front face as the leaves move . 
the experiment to localize the sides of the leaves showed a cold region at the interface between the two fields ; this was due to the t&g effect . however , their study and other similar dosimetric studies that have been made to localize mlc sides and ends , used a double - exposure technique , i.e. 
second , in the three - field technique , the two parallel opposing fields broaden the penumbra such that it may or may not resemble the dose gradient of the perpendicular anterior field depending on the distance between the lateral and the anterior fields as reported in our previous work [ 1 ]  . 
the 50% decrement line for the tongue side of a leaf is positioned approximately 1 mm inside the 50% decrement line for the groove side of its neighbor . this problem can only be minimized by abutting the sides by the ends of mlc leaves . 
matching using multileaf collimators therefore , according to the shape of the target in the lateral field , side - by - end or end - by - side abutment can be achieved . 
in cases of field abutment using mlc , consideration should be given to the current technology for mlcs design ( rounded ends and stepped sides ) and their consequent effect on the dose at the beam edge [ 14 ]  . our film dosimetry studies using this method demonstrated more desirable and reproducible homogeneous dose distribution at the junction . 
 it is important to point out that beveling at the front face of the leaves leads to the diamond - shaped pattern with the ends abutted at the field midline . 
to prevent secondary effects on the radiation field , a linear accelerator manufacturer currently recommends the following jaw setting : 8 mm at the isocenter for x - jaw margin , back from the front edge of the most retracted mlc leaf . 
additionally , a closed leaf pair should be shielded by a 0 - mm yjaw margin to prevent transmission of radiation to the patient . although this criterion appears to be acceptable for symmetric mlc fields , it may still be deficient for asymmetric fields . when the leaf end is used to define the match - line , an 8 - mm x - jaw backup margin leads to a more pronounced round - ended effect . 
when the leaf side constitutes the match - line , a 0mm y - jaw backup margin can increase or decrease the matchline dose due to the associated jaw tolerance as mentioned previously . 
in this study , we found that the best physical dose distribution at the matching area was obtained when the xor y - jaw was set at 1 mm away from the beam central axis . 
although the isocentric technique using mlc may not reduce the simulation - to - treatment variation , it does eliminate field - to - field junction variation , thus reducing the treatment - to - treatment variation which is considered a prerequisite in clinical practice . conclusion assessment of dose homogeneity in the abutting region of the three - field head and neck treatment using mlc has been demonstrated . 
the use of computer - controlled multileaf collimators to define the match - line is accurate , reproducible , and viable and represents an alternative approach to the problem of field matching using asymmetic jaws . 
 strahlentherapie und onkologie original article reirradiation of locally recurrent nasopharyngeal carcinoma erzsbet lengyel1 , kroly baricza1 , andres somogyi1 , judit olajos2 , zsuzsanna ppai3 , mria godny4 , gyorgy nmeth1 , 5 , olga sik1 , 5 purpose : to study the efficacy of reirradiation as salvage treatment in patients with locally recurrent nasopharyngeal carcinoma . patients and methods : between 1993 and 2000 , 20 consecutive patients ( twelve males and eight females ) with nasopharyngeal cancer , previously irradiated in different hungarian institutions , were reirradiated for biopsy - proven locally recurrent tumor . 
stages iiv ( ajcc 1997 staging system ) were assigned to five ( 25% ) , seven ( 35% ) , five ( 25% ) , and three ( 15% ) patients , respectively ; none of them had distant metastases , and only eight ( 40% ) displayed regional dissemination . 
the median time period between termination of primary treatment and local recurrence was 30 ( range , 10204 ) months . brachytherapy was the method most frequently used : in ten cases alone ( especially for rt1 tumors ) , and in eight cases in combination with external beam therapy . 
the median dose in the event of brachytherapy alone was 20 gy ( 4 ( cid : 1 ) 5 gy or 5 ( cid : 1 ) 4 gy , range , 1636 gy ) , and the dose range for exclusive external irradiation was 3040 gy . 
radiotherapy was supplemented by neck dissection ( six patients ) , nasopharyngectomy ( one patient ) , or chemotherapy ( eleven patients )  . results : 16 patients were reirradiated once , three twice , and one patient three times , with a median equivalent dose for tumor effect of 36 gy ( mean , 44 gy ; range , 19117 gy ; the estimated ( cid : 2 ) / ( cid : 3 ) - ratio was 10 gy )  . 
the median equivalent dose of reirradiation for late effect on normal tissue ( with an estimated 70% delivery of the tumor dose ) amounted to 30 gy ( mean , 37 gy ; range , 13101 gy , estimated ( cid : 2 ) / ( cid : 3 ) - ratio 3 gy )  . 
following reirradiation , a severe ( grade 3 or higher ) late toxicity ( ctc criteria , version 2 ) has been observed in two tumor - free patients ( 10% ) so far ( necrosis of soft palate and paresis of glossopharyngeal nerve )  . conclusion : retreatment of nasopharyngeal carcinoma with radiotherapy ( preferably a combined modality ) , can result in longterm local control and survival in a substantial proportion of patients , at the price of an acceptable morbidity . key words : nasopharyngeal carcinoma recurrent disease reirradiation strahlenther onkol 2003 ; 179 : 298305 doi 10.1007 / s00066 - 003 - 1048 - 6 wiederbestrahlung bei lokal rezidivierendem nasopharyngealem karzinom ziel : untersuchung der effektivitt einer wiederbestrahlung als palliativbehandlung bei patienten mit lokal rezidivierendem nasopharyngealem karzinom . patienten und methodik : im zeitraum von 1999 bis 2000 wurden 20 konsekutive patienten ( zwlf mnner und acht frauen ) mit nasopharyngealem karzinom , die sich bereits frher in verschiedenen ungarischen instituten einer strahlentherapie unterzogen hatten , wegen eines bioptisch nachgewiesenen rezidivtumors erneut bestrahlt . 
die mediane zeitspanne zwischen abschluss der primren therapie und auftreten des lokalrezidivs betrug 30 ( 10204 ) monate . 1 department of radiotherapy , national institute of oncology , budapest , hungary , 2 department of oncoradiology , josa andras hospital , nyiregyhaza , hungary , 3 department of medical oncology , national institute of oncology , budapest , hungary , 4 department of radiology , national institute of oncology , budapest , hungary , 5 department of oncotherapy , semmelweis university , budapest , hungary . received : may 22 , 2002 ; accepted : november 14 , 2002 strahlenther onkol 2003 no . 
reirradiation of locally recurrent nasopharyngeal carcinoma die brachytherapie wurde am hufigsten eingesetzt : in zehn fllen allein ( speziell fr rt1 - tumoren ) und in acht fallen kombiniert mit einer externen strahlentherapie . 
bei kombinierter bestrahlung war eine mediane brachytherapeutische dosis von 20 gy ( bereich 1640 gy ) mit einer externen bestrahlungsdosis von 3040 gy verbunden . die strahlentherapie wurde durch eine neck - dissection ( sechs patienten ) , nasopharyngektomie ( ein patient ) oder chemotherapie ( elf patienten ) ergnzt . ergebnisse : 16 patienten wurden einmal , drei zweimal und einer dreimal mit einer medianen tumorwirksamen quivalentdosis von 36 gy ( im mittel 44 gy , bereich 19117 gy ; geschtztes ( cid : 2 ) / ( cid : 3 ) - verhltnis 10 gy ) wiederbestrahlt . 
die mediane quivalentdosis der wiederbestrahlung fr den spteffekt auf normales gewebe ( mit einer geschtzten aufnahmerate von 70% der tumordosis ) lag bei 30 gy ( im mittel 37 gy , bereich 13101 gy , geschtztes ( cid : 2 ) / ( cid : 3 ) - verhltnis 3 gy )  . 
nach wiederbestrahlung wurde bei zwei tumorfreien patienten ( 10% ) eine schwere ( grad 3 oder hher ) spttoxizitt ( ctc - kriterien , version 2 ) beobachtet ( nekrose des weichen gaumens und parese des nervus glossopharyngeus )  . schlussfolgerung : die wiederholte behandlung des nasopharyngealen karzinoms mittels strahlentherapie ( vorzugsweise als kombinierte modalitt ) kann bei einem betrchtlichen patientenanteil in einer langfristigen lokalen kontrolle und berlebenszeit bei akzeptabler morbiditt resultieren . schlsselwrter : nasopharyngeales karzinom rezidivierende erkrankung wiederbestrahlung introduction reirradiation of a previously irradiated area must be considered a current problem , and it is necessary to define its indications , its dose and the technique required to obtain the best possible oncologic results at the price of an acceptable rate of side effects . 
patients survival is influenced by the correctly preformed treatment , while their quality of life is affected ( besides the consequences of the tumorous process ) by treatment - related complications . the most frequently reirradiated head and neck tumors are local recurrences of relatively radiosensitive nasopharyngeal cancers . 
in clinical practice , reirradiation of these cases is hampered by previous radiogenic damage to the adjacent normal tissues and their potential radiation - induced sequelae , the organs most threatened being the temporal lobes , nerves , spinal cord , temporomandibular joint , mucosa , bone , and eyes [ 9 , 11 , 12 , 21 , 24 , 31 , 33 , 35 , 37 ]  . according to the national cancer registry ( founded in 2000 ) , nasopharyngeal cancer has been a rare disease in hungary so far . 
115 and 101 new cases were identified in 2000 and 2001 , respectively [ 20 ] ; hence , retreatment of locally recurrent disease is a relatively infrequent indication . this article reports oncologic results of reirradiation in 20 patients with locally recurrent nasopharyngeal cancer , together with the radiation - induced side effects . patients and methods between 1993 and 2000 , 20 consecutive patients ( twelve males and eight females ) with locally recurrent nasopharyngeal cancer were reirradiated . 
all patients had histologically proven squamous cell carcinoma , namely who type i ( keratinizing squamous cell carcinoma ) in two ( 10% ) , type ii ( nonkeratinizing carcinoma ) in one ( 5% ) , and type iii ( differentiated carcinoma ) in 17 patients ( 85% )  . initial radiation treatment was performed using different total doses and techniques in various hungarian institutions . the nasopharynx and the regional cervical lymphatic regions were irradiated by external beam radiotherapy alone in 19 cases , with a median dose of 61 gy ( range , 46.570 gy ) , conventional fractionation ( 2 gy / day ) being applied in all but one case ( 2.5 gy / day )  . 
one patient underwent bilateral cervical lymph node dissection before radiotherapy , while four patients received combined ( cisplatin - based ) chemotherapy with neoadjuvant ( one subject ) or adjuvant ( three subjects ) intention . active follow - up facilitated the early detection of recurrent tumors ( figures 1a and 1b )  . 
in six cases , whole body [ 18f ] fluorodeoxyglucose positron emission tomographic ( pet ) examinations were performed to determine the exact tumor extension and to exclude distant metastases . 
the irradiated skin and soft tissues did not exhibit any marked sign of individual radiosensitivity or severe ( grade 3 or more ) late radiation sequelae according to the common toxicity criteria [ 5 ]  . 
16 subjects were reirradiated once , three twice , and one three times ( in this last case , the most recent radiotherapy was supplemented by nasopharyngectomy , and the patient is now tumor - free )  . 
the eight patients with simultaneous regional lymph node failure were managed by cervical dissection ( six patients ) or received cisplatin - based combined chemotherapy only ( two patients ) because of the very advanced stage of the disease . 
 the median dose of brachytherapy alone was 20 gy ( 4 ( cid : 1 ) 5 gy or 5 ( cid : 1 ) 4 gy ; range , 1636 gy ) , and the dose range for exclusive external irradiation was 3040 gy . 
in cases involving combined irradiation , a median of 20 gy ( range , 1640 gy ) brachytherapy was associated with 3040 gy external radiotherapy . for exact determination of the radiation doses of brachytherapy and external irradiation , the equivalent and cumulative equivalent doses were calculated for the entire treatment courses according to nag & gupta , with an estimated / ( cid : 2 ) of 10 gy for the tumor effect and of 3 gy for the late effect on normal tissues [ 26 ]  . radiation - induced side effects were graded on the basis of the common toxicity criteria [ 5 ]  . results the equivalent and cumulative equivalent doses for the entire treatment courses are given in table 2 . 
 with an estimated 70% delivery of the tumor dose to the normal tissue , the median equivalent dose for the late effect during reirradiation was 30 gy ( mean , 37 gy , range , 13101 gy )  . 
the median cumulative equivalent dose for the late effect on the normal tissue ( including previous irradiation ) was 98 gy ( mean , 98 gy ; range , 76148 gy )  . 
 in seven of the eight deceased patients , death was caused by the locally and regionally progressive tumor , and only one of them had distant ( bony ) metastases . 
1548% of the patients have locally persistent , recurrent or new primary tumors in the previously irradiated volume or its vicinity [ 6 , 7 , 13 , 23 , 33 , 35 ] ; retreatment of these cancers poses a great challenge to radiotherapists . possible treatment modalities include surgery , chemotherapy , radiotherapy , and their combinations [ 12 , 24 , 27 , 35 ]  . surgery ( transpalatal , transmaxillary or transcervical nasopharyngectomy ) can be used only for selected tumors ( rt12 or rarely rt3 )  . 
alone or combined with postoperative radiotherapy , it results in a somewhat more favorable survival rate in patients with early stage tumors than does reirradiation alone [ 13 , 18 , 24 ]  . 
quivalentdosen bei wiederbestrahlung und kumulative quivalentdosen der strahlentherapiezyklen fr ( anti - ) tumoreffekte ( ( cid : 2 ) ( cid : 4 ) ( cid : 3 ) = 10 gy ) und fr sptwirkungen auf normalgewebe ( ( cid : 2 ) ( cid : 4 ) ( cid : 3 ) = 3 gy )  . im fall von brachytherapie wurden fr sptwirkungen 70% der tumordosis angesetzt . 
the rate of response to monochemotherapy ( methotrexate , cisplatin , carboplatin , 5 - fluorouracil , bleomycin , vincristine , or doxorubicin ) or polychemotherapy can reach 1030% and 4050% , respectively , but survival is prolonged by merely 56 months [ 11 ]  . 
concurrent radiochemotherapy ( with external irradiation ) seems to be a promising tool which can improve local tumor control and survival , as it prolongs the duration of the response . 
positions of the two catheters ( green and light blue ) , critical organs ( eyes [ brownish pink ] and optic nerve [ cyclamen ] ) and 3 - d dose distribution ( target [ red ] ; blue points are reference points , and the blue cloud represents the isodose surface )  . 
positionen der zwei katheter ( grn und hellblau ) , gefhrdeter organe ( augen [ brunlich rosa ] und sehnerv [ violett ] ) und der 3 - d dosisverteilungen ( zielvolumen [ rot ] ; die blauen punkte geben referenzpunkte , die blaue wolke die isodosen - oberflche wieder )  . 
hsu et al [ 18 ] reported on 60 patients with recurrent ( rt14 ) nasopharyngeal carcinoma treated with nasopharyngectomy or postoperative radiotherapy ( 60 gy ) supplemented by concurrent chemotherapy in cases with positive or narrow ( < 2 mm ) surgical margins . 
marked fibrosis , edema , telangiectasia , or atrophy in the previously treated volume may be signs of increased individual radiosensitivity ( or unintentional , erroneous high - dose delivery ) , generally precluding a new course of radiotherapy . our patients revealed no clinical sign of diminished tissue tolerance , and , thus , we were able to initiate reirradiation . recurrences during early stages ( rt12 ) give a better therapeutic response ( about 50% local control ) as compared to advanced cases . 
stereotactic irradiation can be administered as a single high dose ( 735 gy , median 20 gy ) or a fractionated low - dose schedule ( 2.5 gy / fraction up to a total dose of 4550 gy )  . 
orecchia et al [ 28 ] performed irradiation in two to four fractions with a total dose of 24 gy , and achieved 1and 3 - year overall survival rates of 54 and 31% , respectively , with no severe early or late complications . 
nonetheless , the role of stereotactic techniques in the treatment of nasopharyngeal carcinoma has not been exactly determined yet , as the clinical observations published relate only to small patient groups with a relatively short follow - up . 
the outcome is modest : 5 - year local control and overall survival rates amount to 1540% and 837% , respectively [ 9 , 19 , 21 , 24 , 35 , 37 ]  . 
a majority of recent studies on reirradiation of locally recurrent nasophayngeal cancer cases relate to combined radiotherapy . these suggests that the combined treatment mode ( brachytherapy and external beam radiotherapy ) is the most successful method in terms of local control and can decrease the severe side effects on normal tissues most effectively [ 12 , 19 , 21 , 24 , 31 , 33 , 35 ]  . 
our results refer to a median follow - up of only 3 years , but their extrapolation suggests that they will remain within the given range up to 5 years , without reaching the best oncologic local control and survival results . 
with respect to radiation - induced late effects , the interval between the two radiation treatments should be at least 1 year , but both clinical observations and experimental data suggest that about 3 years are necessary for regeneration of the cns [ 2 , 34 ]  . 
severe late cns ( e.g. , temporal lobe necrosis or cranial neuropathy ) and other complications ( e.g. , trismus [ 1630% ] , soft tissue and bone necrosis [ 20% ] ) have to be expected in 434% and 1263% , respectively , of the patients after reirradiation with a high total dose ( table 3 )  . the side effects appear mainly after external beam therapy [ 810 , 12 , 16 , 21 , 3133 ] , their incidence correlating with the cumulative dose : 4% at < 100 gy and 39% > 100 gy , respectively [ 29 ]  . 
 conclusion reirradiation of locally recurrent nasopharyngeal cancer is an efficient treatment modality , which can be reasonably performed as an appropriate combination of external radiotherapy and brachytherapy with a cumulative equivalent dose of 5060 gy . 
 strahlentherapie und onkologie original article cell adhesion - mediated radioresistance ( cam - rr ) extracellular matrix - dependent improvement of cell survival in human tumor and normal cells in vitro nils cordes , viktor meineke1 background : cell - extracellular matrix ( ecm ) contact is thought to have great impact on cellular mechanisms resulting in increased cell survival upon exposure to ionizing radiation . 
several human tumor cell lines and normal human fibroblastic cell strains of different origin , all of them expressing the wide - spread and important integrin subunit ( cid : 1 ) 1 , were irradiated , and clonogenic cell survival , ( cid : 1 ) 1 - integrin cell surface expression , and adhesive functionality were investigated . 
 material and methods : human tumor cell lines a172 ( glioblastoma ) , patu8902 ( pancreas carcinoma ) , skmes1 ( lung carcinoma ) , a549 ( lung carcinoma ) , and ipc298 ( melanoma ) as well as normal human skin ( hsf1 ) and lung fibroblasts ( ccd32 ) and human keratinocytes ( hacat ) were irradiated with 08 gy . 
irradiated cells exhibited a significant , dose - dependent increase in ( cid : 1 ) 1 - integrin cell surface expression following irradiation . as a parameter of the adhesive functionality of the ( cid : 1 ) 1 - integrin , a radiation - dependent elevation of cell adhesion to fibronectin in comparison with adhesion to plastic was demonstrated . 
these findings might also be important for the understanding of malignant transformation , anchorage - independent cell growth , optimization of radiotherapeutic regimes and the prevention of normal tissue side effects on the basis of experimental radiobiological data . 
 key words : radioresistance ( cid : 1 ) 1 - integrin extracellular matrix tumor cells ionizing radiation strahlenther onkol 2003 ; 179 : 33744 doi 10.1007 / s00066 - 003 - 1074 - 4 zelladhsionsbedingte radioresistenz ( cam - rr )  . 
verbesserung des zellberlebens von tumorund normalzellen in abhngigkeit von der extrazellulren matrix in vitro hintergrund : es wird angenommen , dass zellkontakt zu einer extrazellulren matrix zellulre mechanismen stark beeinflusst , die u.a. 
humane tumorzelllinien und fibroblastenzellstmme , von denen alle die weit verbreitete und wichtige integrin - untereinheit ( cid : 1 ) 1 exprimieren , wurden bestrahlt und das klonogene berleben , die ( cid : 1 ) 1 - integrin - oberflchenexpression und die adhsive funktion des rezeptors untersucht . material und methodik : die humanen tumorzelllinien a172 ( glioblastom ) , patu8902 ( pankreaskarzinom ) , skmes1 ( bronchialkarzinom ) , a549 ( bronchialkarzinom ) und ipc298 ( melanom ) sowie die normalen haut ( hsf1 ) und lungenfibroblasten ( ccd32 ) sowie humane keratinozyten ( hacat ) wurden mit 08 gy bestrahlt . 
neben koloniebildungsassays wurden die ( cid : 1 ) 1 - integrin - oberflchenexpression mittels flusszytometrie und die rezeptorfunktionalitt in adhsionsassays analysiert . ergebnisse : fibronektin fhrte im vergleich zu plastik in allen getesteten zellen zu einem gesteigerten berleben nach bestrahlung . 
im adhsionstest zeigte sich parallel dazu eine bestrahlungsbedingte zunahme der zelladhsion an fibronektin . schlussfolgerung : die zellulre radiosensibilitt in vitro wird stark durch fibronektin im sinne einer zelladhsionsbedingten radioresistenz beeinflusst . 
die hier gewonnenen erkenntnisse knnten darber hinaus fr das verstndnis der malignen transformation , des adhsionsunabhngigen zellwachstums , der optimierung radiotherapeutischer konzepte und der prvention von normalgewebsreaktionen auf der basis experimenteller radiobiologischer daten von interesse sein . key words : strahlenresistenz ( cid : 1 ) 1 - integrin extrazellulre matrix tumorzellen ionisierende strahlung 1 institute of radiobiology , medical academy of the german armed forces , munich , germany . received : july 17 , 2002 ; accepted : october 25 , 2002 strahlenther onkol 2003 no . 
ecm - mediated radioresistance introduction it is thought that the presence of an extracellular matrix ( ecm ) confers an improved cellular status of resistance to cell - damaging agents such as ionizing radiation or drugs in vitro [ 9 , 21 , 41 ]  . 
 cell adhesion to the ecm or isolated matrix components , e.g. , fibronectin ( fn ) , is mediated particularly , among other cellular adhesion molecules such as intercellular adhesion molecules , vascular adhesion molecule - 1 [ 6 ] or proteins of the cd44 family [ 5 ] , by the integrin receptor family [ 24 ]  . 
integrin clustering initiated subsequent to cell attachment to the ecm activates cytoplasmic effectors that are capable of regulating survival , proliferation , migration , adhesion , and differentiation , and many more [ 1 , 8 , 19 , 23 , 24 , 33 , 34 ]  . 
the integrin subunit ( cid : 1 ) 1 is upregulated by irradiation on the cell surface providing an improved adhesion of cells to ecm proteins such as fn or laminthe downstream located protein kinases integrin - linked kinase [ 20 ] , protein kinase b / akt [ 15 ] and glycogen synthase kinase - 3 ( cid : 1 ) [ 43 ] are stimulated by irradiation in a figure 1 . 
doses 4 gy for a172 , skmes1 and a549 cells , 6 gy for patu8902 and ipc298 cells , and 2 gy for normal fibroblasts and keratinocytes grown on fn resulted in a p < 0.05 compared to cells grown on plastic . 
ein p < 0 , 05 wurde fr dosen 4 gy bei a172 , skmes1 und a549 tumorzellen , 6 gy fr patu8902 und ipc298 tumorzellen und 2 gy fr fibroblasten und keratinozyten , die fn - kontakt hatten , im vergleich zu plastik errechnet . 
 in this study , we provide molecular data of six human tumor cell lines and five normal human fibroblastic cell strains with a focus on ecm - dependent cell survival , ( cid : 1 ) 1 - integrin cell surface presentation , and the cellular adhesion of theses cells to the ecm protein fn as a function of radiation exposure . 
these data strongly support the important role of the integrin subunit ( cid : 1 ) 1 for radiation - modulated cell adhesion via a functional receptor and for ecm - dependent changes in cellular radiosensitivity . 
dulbeccos modified eagles medium ( paa , linz , austria ) or rpmi - 1040 medium ( sigma - aldrich gmbh , taufkirchen germany ; for ipc298 cells ) , supplemented with 10% fetal bovine serum ( paa ) and 1% nonessential amino acids ( gibco , karlsruhe , germany ) , was applied to cultivate the cells . 
 radiation exposure irradiation was delivered at room temperature using single doses of 240 - kv x - rays ( isovolt 320 / 10 ; seifert , ahrensburg , germany ) filtered with 3 mm be . 
calculation of the clonogenic inactivation ratio ( cir ) , mean inactivation dose ( mid ) , and sensitizer enhancement ratio ( ser ) of presented dose - effect curves ( see figure 1 )  . 
jeder datenpunkt zeigt den mittelwert standardabweichung von drei unabhngigen experimenten ( n = 18 )  . colony formation assay the colony formation assay was applied for measurement of clonogenic cell survival . 
exponentially growing cells were plated onto noncoated or fn - precoated ( 1 g / cm2 ; becton dickinson , heidelberg , germany ) six - well dishes ( becton dickinson ) 24 h prior to irradiation . 
 flow cytometric analysis of ( cid : 1 ) 1 - integrin expression analysis of b1 - integrin cell surface expression was performed as described previously [ 9 ]  . 
staining with fluorescein isothiocyanate - ( fitc - ) conjugated anti - ( cid : 1 ) 1 - integrin igg antibodies ( dako , hamburg , germany ) was performed for 1 h at room temperature . 
finally , prepared cells were resuspended in facsflow ( becton dickinson ) and measured using a fluorescence - activated cell sorter ( facscan , becton dickinson ) , equipped with a cellquest software . 
 adhesion assay determination of the adhesive functionality of the ( cid : 1 ) 1 - integrin was employed according to a previously described method [ 9 ]  . shortly , 96 - well plates ( nunc , wiesbaden , germany ) were coated with 10 g / ml fn in serum - free medium for 1 h at room temperature . 
subsequently , blocking of plates for 30 min at room temperature using 1 mg / ml bsa in pbs was performed . 48 h after radiation exposure , 5 ( cid : 2 ) 104 nonirradiated or irradiated cells were washed with serum - free medium and plated onto prepared wells in the absence or presence of functionblocking ( cid : 1 ) 1 - integrin antibodies ( mab 13 , 100 g / ml , pharmingen , heidelberg , germany )  . 
after washing , 100 l of 0.1 m hcl solution were added to each well , followed by measurement of absorbance of the resulting solution at 630 nm by means of a microplate spectrophotometer ( spectra max 190 , molecular devices , krefeld , germany )  . 
 data analysis means standard deviations ( sd ) of surviving fractions , clonogenic inactivation ratios , mean inactivation doses , sensitizer enhancement ratios , flow cytometric analysis of ( cid : 1 ) 1 - integrin cell surface expression , and cell adhesion to substrates were calculated with reference to untreated controls defined as 1.0 or in a percentage scale . 
clonogenic inactivation ratios ( cir ) were calculated according to the equation sf ( 2 ) plastic / sf ( 2 ) fn , mean inactivation doses ( mid , at 50% cell survival ) according to the equation midplastic / midfn , and sensitizer enhancement ratios ( ser ) by dividing the survival fraction of cells grown on plastic by the survival fraction of cells grown on fn at 10% cell survival . 
the fit of the dose - effect curves was calculated by means of the linear - quadratic model ( log s = d ( cid : 1 ) d2 ) indicating , additionally , means standard errors ( se ) for and ( cid : 1 ) - values . 
there was a significantly higher clonogenic cell survival at doses 4 gy for a172 , skmes1 and a549 cells , at 6 gy for patu8902 and ipc298 cells , and at 2 gy for the normal fibroblasts and keratinocytes adhered to fn ( figure 1 )  . 
as delineated in figure 2 , calculations of the clonogenic inactivation ratio , mean inactivation dose , and sensitizer enhancement ratio indicated a reduced radiosensitivity in all cell lines grown on fn except ipc298 cells compared to cells grown on plastic . 
fn as compared to plastic does not necessarily lead to an increase in the ratio , although , the dose - effect curves of all tumor and normal cells tested demonstrated a reduced radiosensitivity when the cells were attached to fn . flow cytometric analysis of ( cid : 1 ) 1 - integrin expression within a 48 - h time interval after irradiation ( 2 , 2.5 , 5 , 6 gy ) , a pronounced , significant dose - dependent rise of ( cid : 1 ) 1 - integrin table 1 . 
analysis of the ( cid : 3 ) and ( cid : 1 ) - values se was performed by means of the linear - quadratic model describing the dose dependence of cell inactivation according to the formula log sf = ( cid : 3 ) d ( cid : 1 ) d2 . 
die analyse der ( cid : 3 ) und ( cid : 1 ) - werte se erfolgte mit hilfe des linear - quadratischen modells , welches die dosisabhngigkeit der zellinaktivierung beschreibt , entsprechend der formel ln sf = ( cid : 3 ) d ( cid : 1 ) d2 . die ( cid : 3 ) und ( cid : 1 ) - werte sowie die ( cid : 3 ) ( cid : 4 ) ( cid : 1 ) - ratios sind fr alle getesteten zellen entsprechend des substrats ( plastik , fn ) , an das sie zum zeitpunkt der bestrahlung adhriert waren , aufgelistet . 
cells grown on plastic were irradiated with 2 gy ( ipc298 , hacat ) , or 6 gy ( ; a172 , patu8902 , skmes1 , a549 , hsf1 , ccd32 )  . 
subsequently , a 48 - h time interval was measured using flow cytometry to detect radiation - dependent changes of ( cid : 1 ) 1 - integrin cell surface expression . 
each data point shown represents the mean sd of three independent experiments of the ( cid : 1 ) 1 - integrin cell surface expression of irradiated cells in relation to untreated control cells ( = 100% ) at the same time point . 
auf plastik wachsende zellen wurden mit 2 gy ( ipc298 , hacat ) oder 6 gy ( ; a172 , patu8902 , skmes1 , a549 , hsf1 , ccd32 ) bestrahlt . 
jeder datenpunkt zeigt den mittelwert standardabweichung der oberflchenexpression des ( cid : 1 ) 1 - integrins bestrahlter zellen in beziehung zur unbehandelten kontrolle ( = 100% ) von drei unabhngigen experimenten . 
after delivery of 2 or 2.5 gy , the amount of ( cid : 1 ) 1 - integrin was raised in a range from 110 to 200% at 48 h compared to untreated controls . 
after delivery of 5 or 6 gy , the amount of ( cid : 1 ) 1 - integrin was raised in a range from 115 to 270% at 48 h compared to untreated controls which resulted both in p < 0.05 cell line - dependently . 
by contrast , patu8902 , ipc and hacat cells demonstrated a faster upregulation of the ( cid : 1 ) 1 - integrin presentation within 1224 h after irradiation . adhesion assay attachment of cells to fn was found to be fiveto tenfold higher compared to attachment to uncoated plastic or bsablocked culture plastic throughout the experiments ( figure 4 )  . this radiation - dependent improvement of cell attachment to fn was indicative of being dose - dependent for normal skin ( hsf1 ) and lung ( ccd32 ) fibroblasts . 
incubation of nonirradiated and irradiated cells using the ( cid : 1 ) 1 - integrin function - blocking antibody mab 13 inhibited adhesion to fn effectively and significantly ( figure 4 )  . 
in this study , we present molecular data of several human tumor cells and normal human fibroblasts and keratinocytes of different origin giving strong evidence of the involvement of the ( cid : 1 ) 1 - integrin cell surface expression and functionality of this receptor in radioresistance - mediating mechanisms in vitro . 
a second result is a dose - dependent radiation - induced upregulation of the integrin subunit ( cid : 1 ) 1 in all cells tested within a time interval of 48 h . 
the functionality of the ( cid : 1 ) 1 - integrin subunit was tested by plating nonirradiated and irradiated ( 2 or 6 gy ) skmes1 , a549 , hsf1 and ccd32 cells onto plastic , fn , or bsa for 45 mspecific inhibition of adhesion through the ( cid : 1 ) 1 - integrin was provided by incubation of nonirradiated controls or irradiated cells using function - blocking mab 13 antibodies ( 100 g / ml )  . 
die adhsionsfhigkeit unbestrahlter und bestrahlter skmes1 - , a549 - , hsf1und ccd32 - zellen via ( cid : 1 ) 1 - integrin an plastik , fn oder bsa wurde 48 h nach bestrahlung ( 2 oder 6 gy ) berprzur blockierung der ecm - bindungsstelle des ( cid : 1 ) 1 - integrins wurden unbestrahlte und bestrahlte zellen mit 100 g / ml eines spezifischen antikrpers ( mab 13 ) inkubiert . 
 * p < 0 , 05 . determination of clonogenic survival is a common method of assessing the cytotoxic potential of a specific agent such as ionizing radiation or drugs [ 4 , 1012 , 17 , 27 , 28 , 35 ]  . 
to date , only a few groups have tested the modulating impact of the ecm or isolated components on clonogenic survival [ 9 , 13 , 18 , 37 , 41 ]  . 
in this study , we strongly support these findings with data generated in several human malignant and nonmalignant cell lines of different orig presence of fn clearly showed that the reduced cellular radiotoxic effects are independent of the cells origin , differentiation status or genotype . the phenomenon of cell adhesion - mediated radioresistance ( cam - rr ) is defined here as reduction of cellular sensitivity toward ionizing radiation which is due to a modulation of specific critical cellular functions as a result of cell adhesion to either single ecm proteins or a physiologic composition of an ecm . 
attachment of cells via integrins , especially ( cid : 1 ) 1 - integrins , serves as survival factor [ 32 ] controlling apoptotic pathway events via pkb phosphorylation of , e.g. , bad or caspase - 9 [ 14 , 26 ] as well as regulating the cell cycle by cyclin d1 proteolysis inhibition [ 16 ] and retinoblastoma protein hyperphosphorylation [ 21 ]  . 
additionally , differentiation , motility - related cellular events , i.e. , adhesion or migration [ 40 ] , immunologic [ 2 , 29 , 36 ] and ecm - remodeling events [ 42 ] are being controlled . recent findings , furthermore , indicated the participation of ( cid : 1 ) 1 - integrin signaling upon exposure of cells to dna - damaging agents in dna repair mechanisms [ 25 ] , prevention of double - strand break occurrence [ 22 ] , and upregulation of the pglycoprotein responsible for a multidrug resistance phenotype strahlenther onkol 2003 no . 
by describing the multiple regulatory functions of ( cid : 1 ) 1 - integrin pathway signaling , the radiation - dependent alterations of integrin cell surface patterns can be interpreted more deeply . 
an increased cell membrane density of ( cid : 1 ) 1 - integrin is likely to positively influence cellular resistance to cytotoxic agents ( such as ionizing radiation ) due to a recruitment of an increasing number of ( cid : 1 ) 1 - integrin downstream mediators and / or a stimulation of specific ( cid : 1 ) 1 - integrin signaling protein kinases leading to an optimized , cell death - reducing cell physiology . 
the significant elevation in adhesion of cells to fn in a dose - dependent manner via an upregulation and / or switching - on of a functional integrin receptor is likely to result in an enhanced anchorage of cells in their corresponding microenvironment . in case of tumor cells , migration and metastatic spread could possibly be disturbed or even prevented this way . 
by specifically blocking the adhesive capability of ( cid : 1 ) 1 - integrins using specific monoclonal antibodies , we could support that this receptor plays a highly substantial role in the adhesion processes of the tested nonirradiated and irradiated cells . 
furthermore , by correlating the induction of functional ( cid : 1 ) 1 - integrin receptors on the cell surface to elevated cell adhesion to fn , irradiation demonstrated its possible impact on the impairment of cell motility and , thereby , participation in the inhibition of the first step of metastasis formation . 
these findings provide further insights into the cellular regulating processes concerning in vitro radiosensitivity and might also lead to a better molecular understanding of tumorigenesis , normal tissue side effects as well as possible molecular determinants for the failure of radiotherapeutic regimens . 
ukrain , an alkaloid thiophosphoric acid derivative of chelidonium majus l . , protects human fibroblasts but not human tumour cells in vitro against ionising radiation . int j radiat biol 2002 ; 78 : 1727 . 
 strahlentherapie und onkologie short comminucation optimization of radiation therapy for locally advanced adenoid cystic carcinomas with infiltration of the skull base using photon intensity - modulated radiation therapy ( imrt ) and a carbon ion boost daniela schulz - ertner1 , bernd didinger2 , anna nikoghosyan2 , oliver jkel3 , ivan zuna2 , michael wannenmacher1 , jrgen debus1 , 2 background : tumor doses > 70 gy are needed for local control in adenoid cystic carcinomas . 
furthermore , the mean doses to the oar can be reduced by 8.3% ( median % reduction of mean doses to oar ; p = 0.00001 ) using carbon ions . 
 conclusions : the combination of photon imrt with carbon ions improves the target coverage for the boost volume and offers better sparing of oar close to the ptv2 ( gross tumor volume ) in comparison with photon imrt alone . 
 key words : adenoid cystic carcinoma carbon ion therapy intensity - modulated radiation therapy strahlenther onkol 2003 ; 179 : 34551 doi 10.1007 / s00066 - 003 - 1071 - 7 therapieoptimierung bei lokal fortgeschrittenen adenoidzystischen karzinomen mit infiltration der schdelbasis durch verwendung intensittsmodulierter radiotherapie ( imrt ) mit kohlenstoffionenboost hintergrund : fr die lokale kontrolle adenoidzystischer karzinome werden tumordosen von > 70 gy bentigt . 
 1 department of radiation oncology , university of heidelberg , germany , 2 division of radiation oncology , german cancer research center ( dkfz ) heidelberg , germany , 3 division of medical physics , german cancer research center ( dkfz ) heidelberg , germany . 
optimization of rt for adenoid cystic carcinoma schlussfolgerungen : die verwendung von kohlenstoffionen in kombination mit photonen - imrt ermglicht im vergleich zur alleinigen imrt eine bessere erfassung des boostvolumens sowie eine bessere schonung von dem ptv2 benachbarten risikoorganen . 
inwiefern diese potentiellen vorteile zu einem klinischen nutzen fhren , wird derzeit im rahmen einer klinischen studie berpr schlsselwrter : adenoidzystisches karzinom kohlenstoffionentherapie intensittsmodulierte radiotherapie introduction adenoid cystic carcinomas are relatively rare tumors that account for approximately 510% of all salivary gland tumors [ 29 ]  . 
a selective management strategy with photon imrt for the clinical target volume covering the potential microscopic spread and a high - let radiation therapy boost with carbon ions to the macroscopic tumor residual is likely to reduce toxicity compared to fast neutron radiation therapy . 
 patients and methods patient characteristics for plan intercomparison , we selected nine patients with advanced adenoid cystic carcinoma infiltrating the skull base , originally treated with photon imrt and a carbon ion boost to the macroscopic tumor within a clinical phase i / ii study . 
during carbon ion radiation therapy , daily orthogonal x - rays were additionally performed prior to beam application to verify treatment position in order to exclude patient misalignment > 1 mas positioning errors > 1 mm were excluded , a safety margin of 1 mm was assumed to be adequate for the definition of the boost volume ( planning target volume 2 [ ptv2 ] )  . 
 imaging for treatment planning treatment planning data consisted of a three - dimensional ( 3d ) ct data cube generated from continuous 3 - mm ct slices obtained within a stereotactic localization systeadditionally , a planning mri scan was performed under stereotactic guidance containing contrast enhanced t1w and t2w mri sequences . 
optimization of rt for adenoid cystic carcinoma target volume definition the planning target volume 1 ( ptv1 ) was defined as primary tumor site including the typical tumor spread along the involved cranial nerves and the corresponding parts of the skull base plus a generous margin based upon clinical risk estimations . 
the target volumes were particularly complex - shaped in all cases , and thus conventional 3 - d radiation therapy was not likely to achieve complete target coverage while respecting the tolerance doses to the outlined oar . 
the brain stem was constrained to 54 gy , while very small volumes of < 1 cm3 at the surface were allowed to receive maximum doses up to 60 gy . 
dependent on the tumor site , further oar such as the contralateral parotid , the inner ears , and the lacrimal glands were contoured and additionally spared during the treatment planning process using the td 5 / 5 values introduced by emami et al [ 7 ]  . 
therefore , the treatment plans were considered to be realistic , although the use of smaller spot sizes of carbon ion beams or the use of a greater number of intensity levels for imrt might have further increased plan quality . 
beams were assumed to be delivered with a motorized multileaf collimator ( leaf width of 10 mm at the isocenter ) using the step - and - shoot technique with the beam turned off between the subfields [ 22 , 26 ]  . 
 combined photon imrt and carbon ion boost the photon imrt plan for ptv1 and the carbon ion boost plan for ptv2 were planned independently using the planning system konrad for the imrt plan and the treatment planning program trip for the carbon ion plan [ 17 ]  . 
ptv1 and ptv2 were treated in a sequential manner , but for plan evaluation , the photon imrt plan and the carbon ion boost plan were added in a ratio of 54 : 18 using a simple add - up program . as the photon imrt plans were normalized to the median dose of the ptv and the carbon ion plans to the maximum dose , the resulting sum plans and the photon imrt plans ( integrated boost ) were compared on the basis of absolute dose values , only . 
 the carbon ion boost plans typically consisted of two to three isocentric beam portals using 50400 mev per nucleon carbon ions and the intensity - controlled raster - scanning technique with energy variation for beam delivery . 
 physical metrics for plan intercomparison for the imrt plan ( integrated boost concept ) and the sum plan ( sequential boost technique using photon imrt for ptv1 and carbon ion radiation therapy for ptv2 ) , plan quality was evaluated by determination of several dose - volume histogram - ( dvh - ) derived physical metrics as maximum dose to ptv2 ( dmax / ptv2 ) and ptv1 ( dmax / ptv1 ) , minimum dose to ptv1 ( dmin / ptv1 ) and ptv2 ( dmin / ptv2 ) , mean dose to ptv1 ( dmean / ptv1 ) and ptv2 ( dmean / ptv2 ) , and the mean doses to several oar . 
therefore , the calculation of dmax and dmin for the ptvs did not take into account the 1 ml of the volume that received the highest and the lowest dose , respectively . further metrics determined were the target coverage ( cov95% = target volume that receives at least 95% of the prescribed dose ) , d95% ( dose received by at least 95% of the target volume ) , target heterogeneity , target conformality , and the integral dose to the non - target tissue . 
the definition of target heterogeneity used by the radiation therapy oncology group ( rtog ) [ 28 ] was modified for this investigation using the maximum dose after subtracting the 1 ml of the target volume that received the highest dose which was assumed to be a better parameter for assessing plan quality in inhomogeneous treatment plans for complexshaped targets . 
the aim of treatment planning was to optimize target coverage and homogeneity as well as to limit the dose to non - target tissue after the tolerance doses to specific neighboring oar had been fully utilized . 
as a result , maximum allowed doses to oar were reached but not exceeded in all treatment plans in order to achieve comparability of the plans . an example for comparative treatment planning for a patient with adenoid cystic carcinoma is given in figures 1a and 1b . 
 biological parameters have not been taken into consideration although experimental as well as clinical data suggest a biological advantage of high - let radiation therapy for adenoid cystic carcinomas [ 21 ]  . 
on the other hand , the integrated boost concept ( photon imrt alone ) includes an increased fraction dose within the boost volume which also might affect tumor control probability . 
physikalische parameter fr die planevaluation . physical metric definition maximum dose ( gy ) to the target volume minimum dose ( gy ) to the target volume mean dose ( gy ) to the target volume target coverage ( cov95 ) target volume ( % ) that receives at least 95% of the prescribed dose dose ( gy ) received by at least 95% of the target volume non - target tissue volume ( cm3 ) that receives at least 30 gy non - target tissue volume ( cm3 ) that receives at least 50.4 gy target heterogeneity maximum dose ( gy ) to ptv2 / desired dose ( gy ) target conformality total volume ( cm3 ) that receives at least 90% of ( tc90 ) the desired dose / target volume ( cm3 ) that receives at least 90% of the desired dose total volume ( cm3 ) of non - target tissue ( cid : 1 ) mean dose ( gy ) / 1 , 000 integral dose results with both techniques , highly conformal dose distributions can be generated that enable the prescription of the desired tumor doses of 54 gy to ptv1 and 72 gy to ptv2 . figure 1a abbildung 1a figure 1b abbildung 1b figures 1a and 1b . 
 mean oar doses and dose to nontarget tissue mean dose values to 60 oar in nine patients were determined from the dvhs . to assess the difference for both techniques , dose values for each oar were compared and the median percentage of dose reduction was calculated . 
using carbon ions , mean doses to dmin , dmax , and dmean the determined values for dmin , dmax , and dmean for the imrt alone versus imrt + carbon ion boost are summarized in table 3 . 
optimization of rt for adenoid cystic carcinoma the dose within the bragg peak at the end of the particle track . using the intensity - controlled raster - scan technique with active energy variation , carbon ion beams can be delivered precisely and safely to any irregularly shaped target . 
 on the other hand , one might argue that novel photon radiation therapy techniques like inversely planned photon imrt enable dose escalation and thus improve local control rates as well . 
the presented study compares photon imrt alone to photon imrt plus a carbon ion boost on a physical basis , only . the planning intercomparison is based on the concept that prescribed doses are adapted to the estimated risk for recurrence . 
as a consequence , 72 gy was prescribed to the gross tumor volume ( ptv2 ) , and 54 gy is thought to be sufficient to effectively treat the clinical target volume ( ptv1 )  . our data demonstrates that irradiation with carbon ions represents not only an interesting therapeutic approach in the treatment of locally advanced adenoid cystic carcinomas because of their potential biological advantages , but also because of their favorable physical properties . 
target coverage for ptv2 might be increased at the cost of target conformality for ptv2 , which might not be clinically relevant , as at the same time mean doses to neighboring oar can be significantly reduced . 
evaluating plan intercomparisons , one has to keep in mind that plan quality is also a function of the treatment planners experience and the time which is invested in the generation of a plan and in treatment delivery itself . 
in the individual case , the decision about which technique is to be preferred should at least be based upon clinical judgment . biological factors such as rbe values and biological effects of a modified fractionation using carbon ions as well as photon imrt with an integrated boost influence toxicity as well and have to be considered in the evaluation of toxicity . 
to assess the biological advantage of carbon ion radiation therapy in adenoid cystic carcinomas by means of local control probability and reduction of toxicity , a clinical phase i / ii study has been initiated . 
zielvolumenheterogenitt ( th ) sowie zielvolumenkonformitt fr ptv2 ( tc90 / boost ) und fr ptv1 ( tc90 / ptv1 )  . oar can be reduced by median 8.3% which was statistically significant at p = 0.00001. 
for patients presenting with inoperable tumors or macroscopic tumor residuals , local control rates after low - let radiation therapy ( photons , electrons ) remain poor ranging from 4% to 36% [ 8 , 24 , 31 ]  . skull base involvement and inoperability were found to be adverse prognostic factors by douglas et al [ 6 ]  . 
in lung metastasis of adenoid cystic carcinomas revealed rbe ( relative biological effectiveness ) values as high as 8 after irradiation with fast neutrons [ 1 ] , several prospective clinical trials have been carried out investigating fast neutron radiotherapy in adenoid cystic carcinomas [ 2 , 12 , 20 , 21 , 25 ]  . 
as late effects mainly occurred outside the target volume , more conformal radiation therapy is likely to reduce late toxicity to non - target tissue [ 4 , 30 ]  . carbon ion beams are high - let beams that offer similarly to neutrons an elevated rbe . 
optimization of rt for adenoid cystic carcinoma acknowledgment this study was supported by a grant of the tumor center heidelbergmannhei strahlentherapie und onkologie original article randomized phase iii trial of postoperative radiochemotherapy amifostine in head and neck cancer is there evidence for radioprotection ? peter vacha1 , fabian fehlauer1 , birgit mahlmann1 , meinolf marx1 , axel hinke2 , konrad sommer3 , eckart richter1 , thomas feyerabend4 purpose : experimental and clincial data suggest a reduction of radiation - induced acute toxicity by amifostine ( a )  . 
we investigated this issue in a randomized trial comparing radiochemotherapy ( rt + ct ) versus radiochemotherapy plus amifostine ( rc + ct + a ) in patients with head and neck cancer . 
 patients and methods : 56 patients with oro - / hypopharynx or larynx cancer ( t12 n12 g3 , t34 n02 g13 ) were randomized to receive rc + ct alone or rc + ct + a . 
patients were irradiated up to 60 gy ( r0 ) or 70 gy ( r1 / 2 ) and received chemotherapy ( 70 mg / m2 carboplatin , day 15 in week 1 and 5 of radiotherapy )  . 
 conclusions : according to our results , there is a radioprotective effect on salivary glands and a potential effect on oral mucosa by amifostine in postoperative radiotherapy combined with carboplatto improve the radioand chemoprotective effects of amifostine in clinical practice , the application of a higher dose ( > 250 mg ) seems to be necessary . 
 key words : amifostine head and neck cancer postoperative radiochemotherapy acute toxicity strahlenther onkol 2003 ; 179 : 3859 doi 10.1007 / s00066 - 003 - 1016 - 1 randomisierte phase - iii - studie zur postoperativen radiochemotherapie amifostin bei hno - tumoren . 
wir untersuchten diese frage in einer randomisierten studie mit dem vergleich von radiochemotherapie ( rc + ct ) versus radiochemotherapie + amifostin ( rc + ct + a ) bei hno - tumorpatienten . 
sie wurden mit 60 gy ( r0 ) oder 70 gy ( r1 / 2 ) bestrahlt und erhielten zytostatika ( 70 mg / m2 carboplatin , tag 15 in woche 1 und 5 der radiatio )  . 
 1 department of radiation oncology and nuclear medicine , university of lbeck , germany , 2 wisp research institute , langenfeld , germany , 3 department of head and neck surgery , university of lbeck , germany , 4 practice for radiation therapy bonn - rhein - sieg , bonn , germany . 
amifostine and radiochemotherapy in head and neck cancer schlussfolgerungen : wir sahen einen radioprotektiven effekt von amifostin auf die speicheldrsen und einen mglichen effekt auf die mundhhlenschleimhaut bei einer postoperativen radiochemotherapie mit carboplatum die radiound chemoprotektive wirkung von amifostin klinisch zu verbessern , mssen vermutlich hhere dosen als 250 mg verwendet werden . 
 schlsselwrter : amifostin hno - tumoren postoperative radiochemotherapie akute nebenwirkungen aintroduction in patients with advanced head and neck cancer , postoperative radiotherapy ( rt ) combined with chemotherapy ( ct ) is an integral part of the therapeutic concept . 
on the basis of former experimental and clinical experiences [ 10 , 23 ] , we designed an explorative prospective randomized trial in head and neck cancer patients who were intended to receive postoperative radiochemotherapy . 
patients suffered from advanced tumors of the larynx , oroor hypopharynx ( t34 n02 g13 ) or tumors at these sites with an unfavorable grading ( t12 n12 g3 )  . 
all patients received surgery ( r02 , i.e. , complete resection [ r0 ] , microscopically [ r1 ] or macroscopically non in sano [ r2 ] ) and were randomized to receive rt + ct or rt + ct + a . 
adequate bone marrow , liver and renal function ( leukocytes > 4 ( cid : 1 ) 103 / mm3 , thrombocytes > 100 ( cid : 1 ) 103 / mm3 , serum creatinine < 1.5 mg / 100 ml , creatinine clearance > 60 ml / min , serum bilirubin < 2 mg / dl ) , and informed consent of the patient were prerequisites . 
we used ct - based 3 - d treatment planning resulting in a conformal multiple - field technique with the use of individual blocks , multileaf collimator , asymmetric fields , and static or dynamic wedges . 
with conventionally fractionated rt ( 5 ( cid : 1 ) 2 gy / week ) and dose prescription according to the icru 50 report , the total dose was 60 gy for completely resected tumors ( r0 ) and 70 gy in patients with incomplete resection ( r12 )  . 
in the latter case , after 60 gy an individually planned boost of 5 ( cid : 1 ) 2 gy was delivered to the former tumor region . due to the individualized ct treatment planning , the doses to the salivary glands , at least for the parotid and the submandibular gland , were lower than the prescribed dose . 
 skin reactions , alopecia , body weight , performance status , oral mucositis , and salivary gland function were assessed weekly by two experienced radiooncologists independent from each other and without mutual knowledge of the assessment results . 
it has to be kept in mind that the parameters alopecia , body weight , and performance status are somewhat more objective judgments than the grading of mucositis and salivary gland function . 
according to the explorative character of the study , no adjustment for multiplicity was undertaken , and all p - values are presented without reference to any nominal significance level . 
six patients had to be excluded for reason of allergic skin reactions after the fifth application of amifostine ( one patient ) , patient refusal to the planned treatment ( three patients ) , diagnosis of a second malignancy ( one patient ) , or severe surgical complications ( one patient )  . 
 both groups were well balanced concerning age and sex ( table 2 ) and performance status ( mean 80% in both groups )  . in the control group , squamous cell cancer was diagnosed in 24 patients , one patient suffered from lymphoepithelial cancer . 
most tumors ( n = 14 ) were located in the oropharynx ( hypopharynx : four patients , larynx : five patients , multiple sites : one patient )  . 
 in the other group , squamous cell cancer and adenocarcinoma were found in 24 patients and one patient , respectively . the most frequent tumor site ( n = 14 ) was the oropharynx ( larynx : four patients , hypopharynx : eight patients )  . 
the level i resection rate was almost equal in both groups , whereas ipsilateral level i resection was performed more frequently in the amifostine group ( table 2 )  . side effects like nausea , vomiting , and clinically relevant hypotension due to amifostine were not observed . 
characteristics of 50 patients ( both treatment groups ) including age , sex , tumor stage , type of neck dissection surgery ( nd ) , and level i resection status , i.e. , resection of the submandibular gland . 
charakteristika von 50 patienten ( beide therapiegruppen ) inklusive alter , geschlecht , tumorstadium , art der neck - dissektion ( nd ) und des level - i - resektionsstatus , d.h. 
amifostine and radiochemotherapy in head and neck cancer mucosa salivary glands amifostine control amifostine control week 1 week 2 week 3 week 4 week 5 week 6 week 1 week 2 week 3 week 4 week 5 week 6 mean patient maxi per patient mean patient maxi per patient figure 1 . 
 acute xerostomia was evaluated in both groups except for patients with larynx cancer , as the parotid glands were partially or completely excluded from the treatment volume resulting in an evaluable group of 41 patients ( rt + ct : 22 ; rt + ct + a : 19 )  . 
in the further course of treatment , salivary gland toxicity increased even in the group treated with amifostine but was significantly lower compared to the control group ( for all treatment weeks : p = 0.024 ; figure 2 )  . 
 discussion the results of our prospective randomized trial clearly show the potential of amifostine to significantly decrease salivary gland toxicity , although the dose of amifostine was below that used by other investigators [ 7 , 17 ]  . 
in addition , a bias due to the nonblinded investigators cannot be excluded . in the literature , there are few studies with valid data on the application of amifostine in the context of radiotherapy of patients with head and neck cancer . 
schultze & kimmig [ 16 ] reported on nine patients with curative rt + ct who experienced less xerostomia by amifostine given at a dose of 500 mg twice weekly . 
 [ 11 ] , 28 patients were randomized to receive rt plus carboplatin with or without amifostine given over 10 days ( 500 mg ; day 15 , day 2933 )  . 
published a randomized study of 26 patients treated with accelerated radiotherapy ( 2 ( cid : 1 ) 2 gy / day ) with or without amifostine ( 150 mg / m2 )  . 
amifostine and radiochemotherapy in head and neck cancer in our study , grade 3 mucositis was observed in two patients each ( 8% ) of the group with amifostine and the control group , respectively . 
this comparatively lower incidence of severe mucositis of grade 3 and 4 may be attributed to the reduced radiation exposure of normal tissue by the use of conformal irradiation techniques . 
 [ 6 ] could demonstrate a significant reduction of xerostomia by amifostine ( 200 mg / m2 ) given daily 30 min before irradiation ( 6070 gy , conventional fractionation )  . 
 despite this clear result , sufficient clinical data on the possible radioprotective effect of amifostine are still missing , as most published trials are not reliable due to inconsistent treatment regimens , nonrandomization or inadequate patient numbers . 
in addition , these trials did not report in detail on the kind of neck dissection and the removal of the submandibular glands which has an impact on the grade of xerostomia independent of the radiotherapeutic effect . 
other aspects have been widely neglected in these studies : the quality of life [ 9 ] and the dose at the salivary glands which depends on the radiotherapeutic technique . 
heinrich seegenschmiedt2 , gerd stramann3 , oliver micke4 , hans - bruno makoski5 , nikolaos zamboglou1 , and the german cooperative group on radiotherapy for benign diseases ( gcg - bd ) background : graves orbitopathy ( go ) is a widely accepted indication for radiation therapy ( rt )  . 
in conjunction with the german cooperative group on radiotherapy for benign diseases ( gcg - bd ) , a national survey was conducted in order to assess whether or not there is a consensus on the indication for rt and various treatment factors which were studied . 
 material and methods : a questionnaire was circulated to 190 rt institutions to obtain relevant data concerning the patients workload , stage - dependent indication , and diagnostic procedures , which were considered to be necessary . 
 key words : graves orbitopathy radiation therapy benign disease quality assurance strahlenther onkol 2003 ; 179 : 3726 doi 10.1007 / s00066 - 003 - 0911 - 9 strahlentherapie bei der endokrinen orbitopathie : ergebnisse einer nationalen umfrage hintergrund : die endokrine orbitopathie stellt eine weithin akzeptierte indikation fr die radiotherapie ( rt ) dar . 
daten ber die jhrlichen fallzahlen , die stadienabhngige indikation und notwendigkeit diagnostischer manahmen , die bestrahlungstechnik und dosierung , kombination mit kortikoiden und eine salvage - bestrahlung nach vorangegangenem therapieversagen wurden erhoben . 
 schlsselwrter : endokrine orbitopathie strahlentherapie gutartige erkrankungen qualittssicherung 1 radiation clinic , offenbach hospital , offenbach , germany , 2 department of radio - oncology , radiotherapy and nuclear medicine , alfried krupp hospital , essen - rttenscheid , germany , 3 department of radiotherapy , medical center of radiology , philipps university marburg , germany , 4 clinic and polyclinic for radiotherapy / radioonkology , westphalian wilhelms university , mnster , germany , 5 radiation clinic , municipal hospitals duisburg , germany . 
radiotherapy for graves orbitopathy results of a national survey introduction graves disease is an organ - specific autoimmune disorder , which is often characterized by the triad , hyperthyroidism , orbitopathy and pretibial myxedema [ 24 ]  . 
in most instances , the orbital and periorbital findings , which include exophthalmos , muscle dysfunction , periorbital and eye lid edema , conjunctival chemosis and injection , eye lid retraction , and lagophthalmic keratitis , are localized symmetrically [ 6 , 24 ]  . 
the pathophysiologic origin of tao is suggested to be caused by circulating antibodies , which are directed against antigen structures on the surface of thyrocytes and which recognize these antigen structures on the surface of orbital fibroblasts . 
with activation of the cytokine cascade , they induce the biosynthesis of mucopolysaccharides ; the hygroscopic effect of glycosaminoglycans ( gag ) is responsible for the induction and maintenance of symptoms [ 6 , 15 , 23 , 24 ]  . 
while mild forms are treated locally , different treatment modalities have been proven to be effective for advanced forms of tao , including administration of systemic steroids or cyclosporine a [ 19 , 20 ] or radiotherapy ( rt ) [ 3 , 4 , 7 , 1214 , 16 , 17 , 20 , 23 ]  . 
this paper summarizes the results of a national survey , which was conducted in conjunction with the german cooperative group on radiotherapy for benign diseases ( gcg - bd ) of the german society of radiation oncology ( degro )  . 
from the analysis of the mailed questionnaires , it assessed whether or not there is any consensus on the various treatment factors studied . the final goal is standardization of patient and treatment setup , quality assurance of treatment performance , and improvement of treatment outcome . 
 parameter total number of cases university hospitals community hospitals western germany eastern germany mean cases / center university hospitals community hospitals western germany eastern germany range of cases / center university hospitals community hospitals western germany eastern germany material and methods a structured questionnaire was mailed to 190 german rt institutions to obtain relevant data and information on the annual frequency of tao cases presented and treated , the rt indication process according to the ata ( american thyroid association ) staging system [ 1 ] , and the diagnostic procedures which were considered to be necessary for appropriate indication of rt in tao . 
it was also asked whether rt was routinely combined with steroids , and which indication and dose - fractionation schedules were used for salvage rt after treatment failure following rt . 
between february and october 1999 , we received evaluable responses from 152 ( 80% ) of the 190 institutions , 134 ( 88% ) from western germany and 18 ( 12% ) from the former eastern germany . 
some of the institutions referred patients to larger institutions for rt ; others had inappropriate technical equipment for application of adequate rt technique , e.g. , telecobalt or orthovoltage units . 
thus , collective data about the case workload were available from 138144 rt institutions during the period of 19951998 , for a total 5 , 409 treated cases . of those , 1 , 913 ( 35% ) cases were treated in university and 3 , 496 ( 65% ) in community hospitals . 
from the cases studied in our analysis , 4 , 770 ( 88% ) underwent rt in the former western part of germany and 639 ( 12% ) in the former eastern part of germany ( see table 1 )  . 
in all replies , ata stages iiv were considered a typical indication for rt , but 25 ( 19% ) of 134 would also treat ata stage i , and 37 ( 28% ) ata stage table 1 . 
in 36 ( 27% ) , rt was only given after previous administration of steroids , and 97 ( 72% ) delivered rt without previous steroid medication ( 19 were not evaluable )  . 
of 152 institutions , 64 ( 42% ) regarded euthyroid status as a requirement for rt indication , while 67 ( 44% ) prescribed rt without awaiting normalization of thyroid dysfunction ( 21 provided no evaluative responses ) ; in 96 ( 63% ) institutions , the patients age did not influence rt indication , whereas in 35 ( 23% ) , an age limit was considered necessary ( 21 provided no data )  . 
of those , seven would have required patients to be older than 18 years , eleven older than 20 years , four older than 25 years , seven older than 30 years , one older than 35 years , four older than 40 years , and one institution older than 45 years . 
examination of eye motility was routinely performed in 91 ( 69% ) and assessment of the width of the palpebral fissure in 83 ( 63% ) of institutions . evaluation on the use of additional diagnostic procedures is summarized in table 2 . 
in 108 ( 82% ) , various combinations of different tests were suggested as essential for rt indication , i.e. , thyroid - stimulating hormone ( tsh ) in 106 ( 80% ) of 132 , t3 / t4 in 99 ( 75% ) , receptor antibodies in 60 ( 45% ) , and tpo antibodies in 21 table 2 . 
in 24 ( 18% ) institutions , laboratory tests were a major requirement before initiation of rt , and in 17 ( 13% ) , all these laboratory tests were performed routinely . 
 radiotherapy technique 135 ( 89% ) of 152 institutions provided data on rt technique . in 111 ( 82% ) of 135 institutions , a face mask immobilization system was used , 23 ( 17% ) used a simple head support , and only one ( 1% ) institution positioned patients without immobilization device . 
90 ( 67% ) used ct treatment planning , 36 ( 27% ) simulator - based portal positioning , and nine ( 7% ) applied no pretreatment planning to determine optimal treatment portals . 
81 ( 60% ) applied an angle rotation of 15 toward the posterior of the linear accelerator gantry in order to protect the lens from irradiation , and 81 ( 60% ) used asymmetric ventral borders of the portals or half - beam - block techniques for lens protection . 
67 ( 52% ) of 130 institutions would prescribe a second rt course as a salvage therapy following a previous treatment failure after rt alone or in combination with other treatment methods . 
based on the case workload , an estimated annual number of 1 , 600 cases have been treated in german rt institutions during the years 19951998 , which results in an incidence of 2 / 100 , 000 inhabitants per year . 
hufigkeiten der fraktionierungsregime , gesamtund einzeldosen . fractionation number of schedule institutions total doses ( gy ) number of institutionsb single doses number of institutions ( gy ) levels are also of interest in the diagnosis of tao , but they do not play a role as prognostic factors or good parameters for assessment of treatment outcome . 
 as ct or mri clearly demonstrates the extent of muscle involvement [ 24 ] and possible optic nerve compression , which may require immediate surgical decompression , careful imaging is a mandatory component of diagnostic work - up in tao prior to rt initiation . 
ultrasound permits evaluation of ventral and midparts of the orbit , while use of ct or mri is more sensitive for detection of different causes of exophthalmos . t1 - / t2 imaging and assessment of proton density give mri an advantage over ct to reveal more information about the disease activity [ 18 ]  . 
 pretreatment laboratory work - up is necessary before initiation of rt , as it permits assessment of the thyroid dysfunction , which is an important prognostic factor for the success of rt . 
tpo and receptor antibody serum with regard to rt techniques , 82% of the institutions applied a face mask immobilization system , and in 67% , ctbased treatment planning was used . both of these components should be improved in our future national practice , as both procedures permit a safe rt technique and precise calculation of brain and lens doses . 
these techniques may be helpful to achieve a safer rt technique , but to date , the experimental data are not substantiated by clinical evidence for an increase of malignant tumors of the brain or paranasal sinuses . 
ct - based virtual simulation has been reported to be a helpful tool for retrobulbar irradiation , which will permit a more sufficient inclusion of the eye muscle insertion at the globe [ 8 ]  . 
 lacking an adequate experimental in vitro or in vivo model , dose - finding studies are not available [ 27 ] ; optimization of dose - fractionation schemes remains subject to clinical trials . 
by contrast , for other entities of benign diseases , such as degenerative disorders or heterotopic ossification , adequate experimental models have been developed , which permit a definition of radiotherapeutic targets and an experimental optimization of the dose - fractionation schedules [ 10 , 21 ]  . 76% of the institutions applied total doses in the range of 1520 gy ; three institutions used higher ( > 20 gy ) and five lower ( < 10 gy ) total doses . 
conventionally fractionated schedules ( 5 ( cid : 1 ) 2.0 or 5 ( cid : 1 ) 1.8 gy per week ) were preferred by 57% of the institutions ; 35 institutions used the standard schedule of 10 ( cid : 1 ) 2.0 gy , mostly applied in the anglo - american literature . 
 moreover , it is not clear whether the combination of rt and simultaneous steroids provides a therapeutic advantage . our survey revealed that only 14% of the institutions routinely used this combined treatment . 
so far , two prospective trials have demonstrated an improvement in the outcome of patients which were treated with a combination of rt and corticoids [ 3 , 12 ]  . 
the risk of developing radiation - induced retinopathy , which usually occurs within 436 months after rt , increases significantly after administration of total rt doses of 3040 gy [ 4 ]  . 
 conclusions we strongly recommend a review of the national patterns of care for treatment of benign and malignant diseases on a regular basis and implementation of a quality assurance program both on a national as well as on an international level . prospective technical and clinical trials have to be performed to improve the applied rt technique and the long - term outcome in tao patients , who have been treated with ionizing radiation . 
 strahlentherapie und onkologie original article sensitivity of human tumor cells to retinoids or combined treatment with retinoids and ionizing radiation is not dependent on rar - ( cid : 1 ) 2 induction marcel a . 
peter rodemann1 purpose : the nuclear retinoic acid receptor beta 2 ( rar - ( cid : 1 ) 2 ) is supposed to be a prognostic marker of retinoid sensitivity in patients after retinoid treatment . 
therefore , we investigated the role of rar - ( cid : 1 ) 2 induction with respect to clonogenic survival of different human tumor cells under retinoid treatment alone or in combination with irradiation . material and methods : the retinoid responsiveness of seven human tumor cell lines ( htb35 , htb43 , scc4 , scc9 , mda - mb231 , hct116 , and caski ) as well as one normal human skin fibroblast ( hsf6 ) as control cells was analyzed by colony formation assay under retinoid and retinoid / radiation treatment . 
basic mrna levels of all retinoic acid receptors as well as the treatment - dependent modulation of mrna and protein levels of rar - ( cid : 1 ) were analyzed by rt - pcr and western blot analysis under the different treatment conditions . results : it could be shown that the clonogenic inactivation of tumor cells under retinoid treatment alone or in combination with irradiation was not correlated with the induction of rar - ( cid : 1 ) on mrna and protein level , respectively . 
the control cells ( hsf6 ) , however , demonstrated an induction . conclusion : the responsiveness of human tumor cells to retinoid treatment alone and particularly to combined treatment with irradiation is not necessarily associated with an induction of rar - ( cid : 1 ) 2 as it has been postulated so far . 
 schlussfolgerung : das ansprechen von humanen tumorzellen auf eine alleinige retinoidbehandlung und vor allem auf die kombinierte behandlung mit bestrahlung ist nicht , wie bislang angenommen , notwendigerweise mit einer induktion von rar - ( cid : 1 ) 2 verbunden . 
deshalb scheint der verlust einer rar - ( cid : 1 ) - induktion in tumoren kein geeigneter prognostischer faktor fr eine erfolgreiche retinoid - / bestrahlungstherapie zu sein , da rar - ( cid : 1 ) - defiziente tumoren auch eine starke retinoidantwort zeigen knnen . 
rar - ( cid : 1 ) and inhibition of proliferation introduction retinoids affect cell proliferation , differentiation , apoptosis , and radiation sensitivity in human squamous cell carcinoma cells both in vitro and in vivo [ 6 , 19 , 27 , 28 , 31 , 34 , 42 , 50 , 54 ]  . preclinical data indicate that treatment with retinoids , and especially the combination with interferons or other chemotherapeutic agents such as cisplatin , exerts significant antitumor activity due to the modulation of malignant cell growth and the induction of differentiation and / or programmed cell death in different tumor entities [ 15 , 5052 ]  . 
each of these receptors can be subdivided into several isotypes ( e.g. , ( cid : 2 ) 12 , ( cid : 1 ) 14 , and ( cid : 3 ) 12 ) which differ in their amino - terminal region and are formed by differential promoter usage or alternative splicing [ 8 ]  . 
 previous studies have shown that the loss of rar - ( cid : 1 ) is a critical early step in tumorigenesis of many different entities [ 23 , 41 , 69 ] , and it is postulated that rar - ( cid : 1 ) mediates anticancer effects of retinoids [ 23 , 32 ]  . 
 [ 43 ] and others , restoration of rar - ( cid : 1 ) expression in originally rar - ( cid : 1 ) - negative cells led to retinoid sensitivity of these cells . 
based on these results , it is generally assumed that the retinoid sensititivity of tumor cells is directly correlated to the induction of rar - ( cid : 1 )  . 
however , since it is unclear at present to what extent the expression profile of rar - ( cid : 1 ) 2 in human tumor cells determines their sensitivity to retinoids alone or combined retinoid / radiation therapy , we addressed this question by analyzing a variety of human tumor cell lines in vitro . 
 material and methods cell culture seven human carcinoma cell lines , i.e. , three squamous cell carcinoma cell lines of head and neck htb43 ( fadu ) , scc4 ( crl - 1624 ) , scc9 ( crl - 1629 ) , two cervical cancer cell lines htb35 ( siha ) and caski , one breast cancer cell line mdamb231 , and one colon carcinoma cell line hct116 obtained from the american type culture collection ( rockville , md , usa ) as well as one normal human skin fibroblast hsf6 as control were used in this study . 
the tumor cells were cultured in minimal essential medium ( mem , gibco ; grand island , ny , usa ) with the exception of caski which were cultured in rpmi - 1640 and fibroblasts were cultured in dulbeccos modified eagle medium ( dmem , gibco ; grand island , ny , usa )  . 
htb35 , htb43 , caski , hct116 and mda - mb231 cells were routinely subcultured twice a week , scc4 , scc9 and hsf6 once per week using 0.25% tryps at each passage , cells were seeded at a constant density of 1 ( cid : 4 ) 104 / cm2 . 
 drug treatment all - trans - retinoic acid and 13 - cis - retinoic acid ( atra , 13cra , hoffmann - la roche , basel , switzerland ) were prepared as 10 mm stock solution ( stored at 84 c ) in dmso . the working solution of 10 m was obtained by dilution of stock aliquots with culture mediu atra or 13cra were added to the culture medium of subconfluent , log phase , and confluent stationary cultures 24 h before seeding into colony formation assays , radiation exposure , total rna or protein isolation , respectively . 
 irradiation drug - treated or untreated cells were irradiated at room temperature with photons generated by a linear accelerator ( siemens mevatron , 4 mv , dose rate 2 gy / min ) at a single dose of 2 gy of ionizing radiation as described previously [ 6 , 27 ]  . 
the number of colonies > 50 cells were counted and depending upon the treatment condition the percentage of cell survival was calculated . rt - pcr technique total cellular rna from 15 ( cid : 4 ) 106 cells was isolated with the rneasy - mini kit as described in the manufacturers protocol ( qiagen , chatsworth , ca , usa )  . 
first - strand cdna synthesis was performed by oligo ( dt ) - priming from 1 g rna in a final volume of 20 l with the first - strand cdna synthesis kit for rt - pcr ( roche diagnostics , germany ) according to the manufacturers instructions . 
 for semiquantitative determination of mrna expression levels of rars , rxrs and ef1a , pcr was carried out using a gene amp pcr system 2400 ( perkin elmer , norwall , ct , usa ) with cdna derived from 25 ng of total rna in a standard pcr reaction buffer containing mgcl2 ( roche diagnostics , germany )  . 
the pcr reaction cycles comprised 45 - s denaturing at 95 c , 45 - s annealing at 59 c , and 45 - s extension at 72 c repeated for 35 cycles , with a subsequent 7 - min extension period at 72 c . 
the relative expression level of rar - ( cid : 1 ) mrna was calculated on the basis of the ratio of receptor product to ef1 ( cid : 2 )  . 
 western blot analysis the protein levels of rar - ( cid : 1 ) was analyzed by western blot analyses using a specific antibody against rar - ( cid : 1 )  . 
therefore , whole cell extracts were prepared from 1 ( cid : 4 ) 106 tumor and fibroblast cells in 50 l ripa buffer with protease inhibitors and were separated by sds - page on 9% resolving gels under denaturing conditions . 
blots were incubated for 30 min at 37 c with blocking buffer ( 5% non - fat dry milk powder in pbs ph 7.4 ) and for 24 h at 4 c with a polyclonal ( rabbit ) anti - retinoic acid ( cid : 1 ) ( rar - ( cid : 1 ) ) antibody ( biomol research laboratories inc . , plymouth meeting , pa , usa ) diluted 1 : 750 in pbs ( ph 7.4 ) or 1 h at room temperature with a polyclonal ( rabbit ) anti - ( cid : 1 ) - actin antibody ( sigma - aldrich , germany ) diluted 1 : 5 , 000 in pbs , respectively . after exten - sive washing in tbs containing 0.1% tween - 20 , blots were incubated for 30 min at room temperature with an anti - rabbit igg secondary antibody conjugated to horseradish peroxidase ( amersham , pharmacia biotech , uk limited , buckinghamshire , england )  . 
following washing at room temperature in tbs plus 0.1% tween - 20 , bands of rar - b protein were visualized by enhanced chemiluminescence detection systems ( ecl , amersham ) , according to the manufacturers protocol . 
to control equal loading of the gels ( within the same cells under different treatment ) , the expression of ( cid : 1 ) - actin was checked , and to compare the rar - ( cid : 1 ) expression levels under different treatment , the ratio of rar - ( cid : 1 ) to ( cid : 1 ) - actin was calculated . 
 statistical analysis the data obtained for plating efficiencies and surviving fractions from three to six independent experiments were compared for statistical significant differences using the analysis of variance ( anova )  . 
 results clonogenic cell survival on the basis of clonogenic cell survival after retinoid treatment , the human squamous cell carcinoma cell lines and the normal fibroblast cell strain used were classified into highly retinoid - sensitive ( surviving fraction < 0.5 ) and low retinoidsensitive ( surviving fraction > 0.5 ; figure 1 )  . 
in contrast to the other cell lines used , the breast cancer line mda - mb231 showed a significantly enhanced clonogenic activity as compared to the untreated control and was thus classified as retinoid - resistant . 
except cell lines hct116 and scc4 , all other cell lines tested as well as the normal human skin fibroblast cell strain ( hsf6 , proliferative state ) presented a cell line - specific significant enhancement of radiation toxicity in the range of 1059% . 
 mrna expression levels of nuclear retinoic acid receptors in order to elucidate whether the observed retinoid sensitivity status of the tumor cell lines tested was correlated to the expression profile of nuclear retinoic acid receptors , rt - pcr analyses of the basal and treatment / irradiation - dependent mrna expression were performed . 
in addition , no significant changes in the mrna expression of rar - ( cid : 2 ) , rar - ( cid : 3 ) , rxr - ( cid : 2 ) , and rxr - ( cid : 1 ) were apparent after retinoic acid treatment , radiation exposure or combined retinoic acid treatment ( data not shown )  . 
the mrna expression of rar - ( cid : 1 ) was modulated in the various tumor cell lines differentially as a function of the specific treatment procedure ( figure 3 )  . 
independent of the individual retinoid sensitivity , retinoid treatment , irradiation or combined retinoid / radiation exposure led to a variable decrease in rar - ( cid : 1 ) mrna levels in the cell lines htb43 , scc4 , und scc9 . 
no pronounced changes of rar - ( cid : 1 ) mrna levels were observed for the cell lines htb35 and hct116 , whereas the cell lines mda - mb231 and caski presented a strong induction of rar - ( cid : 1 ) mrna expression upon all treatment procedures ( figure 3 )  . 
surviving fraction of seven tumor cell lines ( mda - mb231 , htb43 , scc4 , hct116 , caski , scc9 , and htb35 ) and one proliferating normal human fibroblasts ( hsf6p ) as a function of retinoid treatment ( atra 10 m ; black bars ) or combined treatment ( atra 10 m plus 2 gy irradiation ; white bars )  . 
berlebensrate von sieben tumorzelllinien ( mda - mb231 , htb43 , scc4 , hct116 , caski , scc9 and htb35 ) und einem proliferierenden normalen humanen hautfibroblastenstamm ( hsf6p ) als eine funktion der retinoidbehandlung ( atra 10 m ; schwarze balken ) oder der kombinierten behandlung ( atra 10 m plus 2 gy bestrahlung ; weie balken )  . 
sf2 values of seven tumor cell lines ( mda - mb231 , htb43 , scc4 , hct116 , caski , scc9 , and htb35 ) and one proliferating normal human skin fibroblast ( hsf6p ) which were irradiated with 2 gy or pretreated with retinoid . numbers shown represent the means standard deviations of the corrected surviving fractions at 2 gy ( sf2 ) of three to six individual experiments with each individual cell line . drug treatment was performed for 24 h prior to the irradiation of plateau phase cell cultures . 
sf2 - werte von sieben tumorzelllinien ( mda - mb231 , htb43 , scc4 , hct116 , caski , scc9 and htb35 ) und einem proliferierenden normalen humanen hautfibroblastenstamm ( hsf6p ) , welche mit 2 gy bestrahlt oder mit retinoid vorbehandelt wurden . 
numbers shown represent the means standard deviations of the relative expression levels , determined by rt - pcr and pcr - elisa on the basis of the internal control gene ef1 ( cid : 2 )  . 
basaler mrna - expressionsgehalt der kernstndigen retinsurerezeptoren ( rars und rxrs ) von sieben tumorzelllinien und einem proliferierenden normalen humanen hautfibroblastenstamm . relative basale mrns - expression der kernstndigen retinsurerezeptoren rar - ( cid : 2 ) , - ( cid : 1 ) , - ( cid : 3 ) und rxr - ( cid : 2 ) , - ( cid : 1 ) der tumorzelllinien ( mda - mb231 , hct116 , caski , htb43 , scc4 , scc9 und htb 35 ) sowie eines proliferierenden normalen humanen hautfibroblastenstammes ( hsf6p )  . 
 discussion the data presented demonstrate that responsiveness of human tumor cell carcinoma cells to retinoid treatment with and without subsequent irradiation is not correlated to the basal expression level nor the induction of rar - ( cid : 1 ) 2 . 
this conclusion is based on results obtained by colony formation assays , rt - pcr , and western blot analyses using seven different tumor cell lines of different retinoid - responsiveness and one human skin fibroblast cell strain as control for normal rar - ( cid : 1 ) induction or responsiveness , respectively . 
the results presented are in contrast to the current opinion which postulates , that rar - ( cid : 1 ) 2 induction is essential for responsiveness to retinoid therapy and , thus , serves as a prognostic marker for therapy planning [ 4 , 26 , 37 , 43 , 66 , 71 ]  . retinoids have long been applied as anticancer agents with specific efficacy in therapy of acute promyelocytic leukemia and squamous cell carcinomas [ 10 , 28 , 36 , 42 , 45 , 52 ]  . they have also been described to reduce secondary recurrence of squamous cell carcinomas of head and neck and to cause regression of premalignant lesions [ 29 ]  . 
cell biological studies indicated that the ability of retinoids to modulate gene expression enables them to redirect aberrant differentiation , reregulate uncontrolled proliferation , and suppress the transformed phenotype [ 9 , 21 , 58 ]  . 
furthermore , retinoids in combination with ionizing irradiation also displayed tumor - specific radiosensitizing effect which is not apparent in normal cells [ 6 , 19 , 27 ]  . 
over the recent years , many preclinical and clinical studies investigated the efficacy of combined radiochemotherapy with respect to local tumor control , normal tissue side effects , and recurrence rate [ 3 , 5 , 7 , 14 , 1618 , 20 , 22 , 24 , 25 , 30 , 3840 , 44 , 46 , 48 , 49 , 55 , 56 , 60 , 62 ]  . 
thus , although for different tumor entities standard protocols exist applying radiation therapy together with conventional chemotherapeutics , e.g. , cisplatin [ 47 , 57 ] , combined retinoid / radiation therapy may offer a treatment alternative for patients at risk to develop normal tissue complications . 
various studies tried to identify the specific role of different receptors in normal and malignant cells with specific emphasis to their importance in treatment and prevention of cancer [ 8 , 13 , 69 , 70 ]  . 
treatment - dependent modulation of relative mrna expression levels of rar - ( cid : 1 ) in the cell lines mda - mb231 , hct116 , caski , htb43 , scc4 , scc9 , and htb35 as well as one proliferating normal human skin fibroblast ( hsf6p ) , determined by rt - pcr and pcr - elisa on the basis of internal control gene ef1 ( cid : 2 )  . 
cells were treated and / or irradiated as described in material and methods . relative rar - ( cid : 1 ) mrna expression of the untreated / unirradiated controls was set as 100% ( basal level )  . 
black bars : control ; white bars : irradiated with 2 gy ; diagonally striped bars : retinoid treatment alone ; cross - striped bars : combined treatment retinoid plus irradiation . 
die behandlungsund / oder bestrahlungsabhngige vernderung der relativen rar - ( cid : 1 ) - expression ist auf der grundlage der unbehandelten / unbestrahlten kontrollen dargestellt . schwarze balken : kontrollen ; weie balken : bestrahlt mit 2 gy ; diagonal gestreifte balken : alleinige retinoidbehandlung ; karierte balken : kombinierte behandlung retinoid plus bestrahlung . 
the basal protein levels as well as the treatment - dependent ( 2 gy irradiation , 13cra 10 m , 13cra 10 m plus 2 gy ) levels of rar - ( cid : 1 ) 2 were analyzed in seven tumor cell lines ( caski , mdamb231 , hct116 , scc4 , scc9 , htb43 , and htb35 ) and one proliferating normal human skin fibroblasts ( hsf6p ) using a polyclonal antibody directed against rar - ( cid : 1 ) protein ( as described in material and methods )  . 
der basale proteingehalt sowie der behandlungsabhngige gehalt ( bestrahlung 2 gy , 13cra 10 m , 13cra 10 m plus 2 gy ) an rar - ( cid : 1 ) 2 wurden mit hilfe eines polyklonalen rar - ( cid : 1 ) - antikrpers ( wie in material und methodik beschrieben ) in sieben tumorzelllinen ( caski , mda - mb231 , hct116 , scc4 , scc9 , htb43 und htb35 ) und einem proliferierenden normalen humanen hautfibroblastenstamm ( hsf6p ) analysiert . 
protein expression of nuclear rar - ( cid : 1 ) 2 , a 52 - kd protein , under single treatment with 13cra ( 10 m ) , irradiation ( ir ) with 2 gy or combined treatment ( 13cra + ir ) of seven tumor cell lines ( caski , mda - mb231 , hct116 , scc4 , scc9 , htb43 , and htb35 ) as well as one proliferating normal human skin fibroblast ( hsf6p )  . 
numbers shown represent the means standard deviations of the relative expression levels , determined by sds - gel electrophoresis and western blot on the basis of the internal control protein act tabelle 2 . 
proteinexpression des kernstndigen rar - ( cid : 1 ) 2 , einem 52 - kd - protein , unter einzelbehandlung mit 13cra ( 10 m ) , bestrahlung ( ir ) mit 2 gy bzw . kombinationsbehandlung ( 13cra + ir ) von sieben tumor - zelllinien ( caski , mda - mb231 , hct116 , scc4 , scc9 , htb43 and htb35 ) sowie einem proliferierenden normalen humanen hautfibroblastenstamm ( hsf6p )  . 
furthermore , it has been observed that the retinoiddependent induction of the rar - ( cid : 1 ) 2 isoform seems to be a requirement for retinoid responsiveness in a variety of human tumor cell lines in vivo and in vitro [ 2 , 4 , 9 , 37 , 53 , 59 , 6769 ]  . this assumption was based on in vitro experiments using retinoid - insensitive , rar - ( cid : 1 ) 2 - deficient human tumor cell lines which were transfected with rar - ( cid : 1 ) 2 gene to obtain rar - ( cid : 1 ) 2 overexpression restoring cellular retinoid responsiveness [ 33 , 35 ]  . 
clinical studies on patients with premalignant oral lesions [ 37 ] and renal cell carcinoma [ 4 ] could also correlate a positive clinical response to retinoids with a potential upregulation with rar - ( cid : 1 ) 2 upon retinoid treatment [ 2 , 37 , 67 ]  . 
 in contrast to these observations , however , a number of in vitro studies demonstrated that retinoid resistance and retinoid - dependent induction of rar - ( cid : 1 ) 2 occurred at the same time in a variety of human tumor cell lines [ 1 ]  . 
thus , conflicting data exist which make the interpretation of the role of rar - ( cid : 1 ) 2 for retinoid responsiveness of human tumor cells difficult [ 59 ]  . 
to elucidate the role of rar - ( cid : 1 ) 2 for retinoid sensitivity of human tumor cells which , based on described parameters , can clearly be separated in retinoid - insensitive and retinoid - sensitive cell lines , we analyzed the expression profile of rar - ( cid : 1 ) 2 in correlation to the cellular response profile . 
all cell lines tested showed low basal levels of rar - ( cid : 1 ) and a cell line - specific pattern of rar - ( cid : 1 ) upregulation upon treatment with 13 - cisretinoic acid which , however , could not be correlated to retinoid sensitivity or insensitivity . 
a similar pattern of rar - ( cid : 1 ) expression as shown for retinoid treatment alone could also be observed in the same tumor cell lines exposed to combined treatment with 13 - cis - retinoic acid and single - dose irradiation . 
consequently , our data are in favor of reports presented by different authors [ 4 , 61 ] concluding that there is no link between retinoid responsiveness of tumor cells and treatment - dependent upregulation of rar - ( cid : 1 ) 2 . since rar - ( cid : 1 ) 2 does not play the critical role as a mediator of retinoid responsiveness of human tumor cells , other components of retinoid signaling seem at least to be as important in this regulation . 
consequently , with emphasis on radiation oncology and the potential prognostic aspect of basal and inducible rar - ( cid : 1 ) expression , no specific answers can be expected by analyzing rar - ( cid : 1 ) profiles of different tumor entities . as potential candidates , cofactors of the transcriptional machinery complex consisting of retinoic acid receptor heterodimers and other regulating proteins such as pcaf ( p300 / cbp - associated factor ) , src - 1 ( steroid receptor coactivator 1 ) and hdac - 1 ( histone deacetylase 1 ) , which all can activate the retinoid - dependent gene transcription by deacetylation of histone proteins ( h14 ) , can be discussed [ 8 , 64 , 65 ]  . 
rar - ( cid : 1 ) and inhibition of proliferation the underlying mechanism of sensitivity in response to retinoid treatment as well as combined retinoid / radiation therapy is addressed in ongoing studies . 
herfarth1 , 2 , oxana izwekowa3 , christoph thilmann1 , andrea pirzkall1 , 2 , stefan delorme4 , udo hofmann5 , dirk schadendorf5 , dietmar zierhut2 , michael wannenmacher3 , jrgen debus1 purpose : stereotactic radiosurgery is an alternative option to neurosurgical excision in the management of patients with brain metastases . 
 key words : radiation brain metastases survival prognostic factors radiotherapy strahlenther onkol 2003 ; 179 : 36671 doi 10.1007 / s00066 - 003 - 1050 - z stereotaktische einzeitbestrahlung zerebraler melanommetastasen ziel : die stereotaktische radiochirurgie hat sich als alternative zur neurochirurgischen exzision bei der behandlung zerebraler metastasen erwiesen . 
die mediane dosis , die auf die tumorumschlieende 80% - isodose appliziert wurde , betrug 20 gy ( spannweite 1522 gy )  . ergebnisse : die neurologischen symptome besserten sich bei fnf der zwlf symptomatischen patienten . 
 1 division of radiation oncology , german cancer research center , heidelberg , germany , 2 deptartment of radiation oncology , university of heidelberg , germany , 3 kursk regional oncological hospital , kursk medical university , kursk , russia , 4 division of radiologic diagnostics and therapy , german cancer research center , heidelberg , germany , 5 skin cancer unit , german cancer research center , heidelberg , germany . 
 schlsselwrter : malignes melanom hirnmetastasen berleben prognostische faktoren radiotherapie strahlentherapie introduction malignant melanoma is the third most common tumor that metastasizes to the brain after breast and lung cancer [ 2 ]  . 
based on retrospective studies , the presence of extracerebral tumor is one of the most important prognostic factors for patients with cerebral melanoma metastases [ 6 , 12 , 19 ] as it is for cerebral metastases in general [ 16 ]  . 
 patients and methods patient characteristics between 1986 and may 2000 , 122 cerebral melanoma metastases in 64 patients ( 39 male , 25 female ) were treated with single high - dose stereotactic radiation therapy ( radiosurgery ) using a linear accelerator . 
the karnofsky performance index ( kpi ) was < 80 in eight patients ( 13% ) , leaving 87% of patients with an overall good performance scale of 80100 at the time of treatment . 
target definition and dose calculations were performed using various versions of stp treatment planning software ( stryker - leibinger , freiburg , germany ) or virtuos software ( dkfz , heidelberg , germany )  . 
for irregularly shaped targets , a manually driven micro - multileaf collimator ( leaf with 1.5 mm at isocenter ) was available and used since 1993 ( 16 metastases )  . 
however , the received information was noninstructive in many cases . on the other hand , the treated cerebral metastases were found to be stable at the last follow - up examination in most of the patients . 
 [ 17 ] reported an increased risk of cerebral recurrence if stereotactic radiosurgery was performed without wbrt , especially if metastatic disease was confined to the brahowever , nieder et al . 
 [ 14 ] analyzed adjuvant wbrt in patients with surgically excised solitary brain metastases and found a high recurrence rate especially in melanoma patients ( four of seven patients ) suggesting that the total dose with wbrt alone was not sufficient to control the disease . wronski & arbit [ 20 ] , on the other hand , found a comparable incidence of brain tumor recurrences with or without wbrt after surgical excision of cerebral melanoma metastases . 
a median survival of approximately 5 months [ 6 , 19 ] has been reported after wbrt . applying a more focused local therapy , retrospective studies report on 78 months survival after stereotactic radiosurgery [ 10 , 12 , 18 , 22 ] or neurosurgical resection [ 20 ]  . 
radiosurgery of cerebral melanoma metastases ity of staging examination ( e.g. , screening with less sensitive methods such as x - ray instead of ct scan of the lung , no pet scan , or less sensitive ultrasound ) , patients might have been falsely classified as being free from extracranial tumor progression . 
yet , clinical follow - up data showed strong evidence confirming the progress in most other patients : five patients deceased due to tumor progression before a second mri examination could take place ; neurosurgical excision of the treated lesion confirmed the diagnosis of local recurrence in another five patients . 
this figure is low compared to other studies . however , the true rate of symptomatic patients might be higher since minor or nonspecific neurologic symptoms ( e.g. , headache ) might not always have been attributed to the disease . 
only 8% of our patients developed new neurologic symptoms that might be therapy - related . three patients showed evidence of bleeding into the treated metastasis after radiation therapy ( data not shown ) , but only one patient became neurologically symptomatic . 
 strahlentherapie und onkologie fallbericht extranodales marginalzonen - b - zell - lymphom ( malt - lymphom ) der konjunktiven und des larynx kasuistik und literaturbersicht thomas kuhnt1 , bettina wollschlger2 , marc bloching3 , ulf krause4 , jrgen dunst1 hintergrund : extranodale non - hodgkin - lymphome ( nhl ) treten berwiegend im gastrointestinaltrakt auf . 
 patientin und methode : es wird ber eine 56 - jhrige frau berichtet , die sich im august 1990 erstmals wegen eines histologisch gesicherten low - grade - b - zell - nhl der konjunktiva des linken oberlides zur behandlung vorstellte . 
die histologische und immunhistochemische analyse ergab fr das larynxrezidiv und retrospektiv auch fr die vorherigen befunde ein marginalzonen - b - zell - nhl vom malt - typ niedriger malignitt . 
 schlussfolgerungen : unsere kasuistik steht hinsichtlich des krankheitsverlaufs und des remissionsverhaltens im einklang mit der literatur und zeigt , dass ein low - grade - b - zell - nhl vom malt - typ lange zeit mit einer radiotherapie lokal kontrolliert werden kann . 
 patient and method : a 56 - year old woman was first treated in august 1990 for a low - grade b - cell lymphoma in the conjunctiva of the left eyelid . 
42 months later an extranodal b - cell lymphoma , located in the conjunctiva of the right eyelid , was found . after a father period of 48 months a malt - type lymphoma arose in the supraglottic larynx . 
the final diagnosis was low - grade b - cell lymphoma of the malt - type , limited to the conjunctival eyelids and supraglottic larynx , with the clinical staging of ie a . 
the radiotherapy has been reported to achieve a long time of relapse - free intervall . the present case demonstrates , that even the recurrence of an extranodal , primary low - grade b - cell malt - type lymphoma responds well to local radiotherapy and can also have a long period of no evidence of disease . 
extranodales malt - lymphom der konjunktiven und des larynx einleitung beim primren , extranodalen low - grade - b - zell - nhl handelt es sich in der regel um lymphome vom mucosa - associated lymphoid tissue - ( malt - ) typ [ 44 ]  . 
erstmalig wurde 1983 von isaacson & wright [ 22 ] ein lymphom des malt der magenschleimhaut beschrieben , wo bisher auch die meisten flle ( 90% ) nachgewiesen wurden [ 39 ]  . 
3 ( cid : 1 ) 3 ( cid : 1 ) 4 cm3 grer , linksseitiger , submukser , nicht ulzerierter tumor des supraglottischen larynx diagnostiziert und laserchirurgisch reseziert ( abbildung 2 )  . 
eine extended - field - bestrahlung ( waldeyer - feld und modifiziertes mantelfeld mit aussparung der axillren lymphknoten ) wurde gewhlt , da in einem vorausgegangenen thorakalen computertomogramm eine unspezifische lymphknotenvergrerung beschrieben worden war . 
ein lymphknotenbefall , hochmaligne anteile , erhhte ldh , erhhtes ( cid : 1 ) 2 - mikroglobulin , schlechter allgemeinzustand ebenso wie t - zellige infiltrate werden mit einer schlechteren prognose verbunden [ 11 , 31 , 32 , 45 ]  . 
in ergnzung dazu publizierten andere autoren ber malt - lymphome im tracheobronchialtrakt , in den speicheldrsen , in der schilddrse , in der orbita bzw . ihren adnexstrukturen , auf der haut sowie seltener auch in der zervix , in der gallenblase , in der prostata und im larynx [ 1 , 3 , 5 , 30 , 34 , 45 , 46 ]  . 
bakterielle infektionen schtzen soll [ 39 , 40 , 45 ]  . ausgangspunkt der malignen transformation des malt sind klonogene marginalzonenzellen in den keimzentren des lymphatischen gewebes ( cd20 + , cd21 + , cd35 + , igm + , igd - , cd5und cd10 - ) [ 5 , 24 ]  . 
krzlich wurden bei 60% aller malt - lymphome genetische translokationen t 11 , 18 ( q21 , q21 ) , t 1 , 14 mit trisomie 3 , c - myc - ( 8q24 ) und p53 - ( 17p13 ) - mutationen beobachtet [ 39 , 41 ]  . 
seit der erstbeschreibung liegen bisher nur wenige fallberichte eines primren malt - lymphoms des larynx vor [ 8 , 9 , 17 , 19 , 20 , 23 ]  . 
ber niedrigmaligne b - zell malt - lymphome der orbita und der augenanhangsgebilde finden sich in den letzten 20 jahren verffentlichungen als einzelfallberichte und kleinerer serien aus nordamerika , japan , frankreich und italien mit circa 150 patienten [ 2 , 4 , 6 , 10 , 13 , 14 , 16 , 25 , 2629 , 31 , 3538 , 43 , 44 ]  . 
die lokale 10 - jahreskontrollrate lag nach radiotherapie , operation und chemotherapie bei 100% , 0% und 42% ( p < 0 , 01 ) und das gesamtberleben nach 20 jahren betrug 100% , 67% und 0% ( p = 0 , 08 ) , wobei rezidive in der operationsund chemotherapiegruppe jeweils nach - bestrahlt wurden . 
die autoren sahen vor allem in der sehr guten vertrglichkeit einen vorteil gegenber einer radiotherapie , bei bisher 100% lokaler kontrollrate ber einen nicht nher angegebenen zeitraum . weitere phase - ii / iii - studien , bisher nur unter einschluss niedrigmaligner b - zell - lymphome der stadien iiiv und vorbehandelte rezidive , laufen mit der gabe des anti - cd20antikrpers rituximab sowie mit radioaktiven anti - cd20antikrpern [ 7 , 15 ]  . 
extranodales malt - lymphom der konjunktiven und des larynx gen in first - line - therapien bei ungefhr 40% sowie bei circa 30% nochmalig in der second - line - therapie . 
eingesetzt wurden elektronen ( spanne 920 mev + bolus ) , photonen in orthovolttechnik , cobalt - 60 sowie der einsatz von linearbeschleunigern mit 46 mv bei einzeldosen zwischen 1 , 5 und 2 , 0 gy . 
patienten , die mit gesamtdosen zwischen 20 bis 30 gy bestrahlt wurden , wiesen die gleichen exzellenten lokalen kontrollraten auf wie patienten , die ber 30 gy therapiert wurden [ 2 , 4 , 38 ]  . 
 nebenwirkungen im wesentlichen werden bei einer radiotherapie im orbitabereich milde akutnebenwirkungen einer konjunktivitis , leichte periorbitale erytheme und deme beschrieben , die durch lokale , symptomatische therapien gut beherrschbar waren [ 2 , 4 , 38 ]  . 
nachweislich nahm jedoch der anteil an chronischen nebenwirkungen , wie das , , trockene auge , korneale ulzera , retinopathien , neuropathien oder glaukome im ctc - grad 3 und 4 bei gesamtdosen ber 35 gy deutlich zu [ 2 , 4 , 38 ]  . 
unser fall zeigt , in bereinstimmung mit den daten der literatur , dass bei adquater therapie auch das multifokale befallsmuster eine gute prognose aufweist . ob therapieoptionen wie die lokale applikation von interferonen oder die gabe des anti - cd20 - antikrpers mit und ohne radioaktivitt isoeffektiv sind , mssen zuknftige untersuchungen zeigen . 
involved - field irradiation in combination with total - body irradiation ( tbi ) not increase short - term toxicity compared to tbi alone in patients with advanced - stage low - grade non - hodgkin lymphoma . 
6 urban & vogel strahlentherapie und onkologie short communication early morbidity after radiotherapy with or without chemotherapy in advanced head and neck cancer experience from four nonrandomized studies sabine bieri1 , soeren m . 
allal4 , luca cozzi5 , christine landmann6 , may monney7 , jacques bernier5 background : data on early treatment - related morbidity after radiotherapy alone ( rt ; 217 patients ) or combined with chemotherapy ( rt + ct ; 182 patients ) of head and neck squamous cell carcinoma are analyzed . 
 patients and methods : the patients were treated between november 1985 and november 1996 in four swiss centers that independently introduced combined - modality therapy in selected cases of head and neck cancer . 
 results : although considerable variation was noted among the treatment schedules / centers , the main findings are as follows : ( 1 ) early morbidity was significantly enhanced after all five rt + ct schedules compared with rt alone ; ( 2 ) typically , a third of the patients lost > 10% of their body weight during concurrent rt + ct as compared with 10% of the patients receiving rt alone ; ( 3 ) at 12 weeks , the prevalence of grade 2 morbidity was 2560% after rt + ct as compared with 420% after rt alone . 
 key words : head and neck cancer chemotherapy radiotherapy adverse effects strahlenther onkol 2003 ; 179 : 3905 doi 10.1007 / s00066 - 003 - 1077 - 1 akute morbiditt nach strahlentherapie mit oder ohne chemotherapie in 399 fortgeschrittenen hals - nasen - ohrenkarzinomen . 
ergebnisse von vier nicht randomisierten studien hintergrund : vorstellung der akuten nebenwirkungen nach alleiniger radiotherapie ( rt ; 217 patienten ) oder kombinierter radiochemotherapie ( rt + ct ; 182 patienten ) bei patienten mit hals - nasen - ohren - tumoren . patienten und methodik : die patienten wurden zwischen november 1985 und november 1996 in vier schweizerischen spitlern behandelt . 
 schlsselwrter : hals - nasen - ohren - karzinome radiotherapie chemotherapie nebenwirkungen 1 department of radiation oncology , regional hospital of sion , switzerland , 2 gray laboratory cancer research trust , mount vernon hospital , northwood , united kingdom , 3 department of radiation oncology , university hospital of zurich , switzerland , 4 department of radiation oncology , university hospital of geneva , switzerland , 5 department of radiation oncology , institute of oncology of southern switzerland , bellinzona , 6 department of radiation oncology , university hospital of basel , switzerland , 7 department of radiation oncology , university hospital of lausanne , switzerland . 
early morbidity after radioand chemotherapy of head and neck cancer introduction combined chemotherapy ( ct ) and radiotherapy ( rt ) has been introduced in the treatment of advanced head and neck cancer in many departments over the last 2 decades [ 4 , 19 ]  . 
the advantage of ct added to locoregional therapy ( rt and / or surgery ) was statistically significant ( p < 0.0001 ) , but the absolute survival benefit was just 4% at 5 years [ 18 ]  . 
this benefit was shown to depend on the scheduling of rt and ct , and induction ct was not associated with a statistically significant therapeutic ganevertheless , a mailed questionnaire among 300 community cancer specialists in the usa showed that rt with induction ct was the most common treatment approach in locally advanced head and neck cancer [ 12 ]  . 
the situation in many european centers seems to be similar , and this state of affairs is reflected in the literature where quite a few papers are being published reporting combined - modality experience from nonrandomized series . 
 in the meta - analysis from paris [ 18 ] , concurrent rt and ct , so - called chemoradiotherapy , showed a relatively larger gain , the absolute benefit in 2 - year and 5 - year survival being 7% and 8% , respectively . 
 no toxicity data were available from the meta - analysis , and it is remarkable that , with a few notable exceptions , many of the individual studies have contained rather scarce data on early morbidity [ 20 ]  . 
 the conclusions regarding the therapeutic potential of rt + ct in four swiss centers were very cautiously formulated allowing for the nonrandomized nature of the studies [ 1 , 2 , 11 , 13 ]  . 
due to the absence of randomized controls and the differences in patient selection for rt + ct among the swiss centers , it was decided to focus on early morbidity . 
 patients and methods from november 1985 to november 1996 , 399 patients with histologically verified squamous cell carcinoma of the head and neck were treated with rt with or without ct in four swiss radiation oncology centers : basel , zurich , geneva , and vaud . 
in the three other centers , patients were considered for ct according to individual characteristics , like performance status , the extent of the disease , and the patients consent to receive chemotherapy . 
 radiotherapy ( rt ) the estimated benefit from chemoradiation is in line with the data from some recent phase iii studies showing quite subthe radiation dose - fractionation schedules are summarized in table 1 . 
 schedule radiotherapy chemotherapy ge - concomitant ge - neoadjuvant concomitant continuous infusion of cddp 20 mg / m2 on day 14 and 18 gy in 10 fractions ( 1 fraction per day ) + 28.8 gy in 24 fractions , 2 fractions dailya surgery ( gap of 12 days ) 2225 . 
field size reduced after 49.6 gy concomitant continuous infusion of cddp 20 mg / m2 on day 15 and 2025 concomitant ( day 14 and 2225 ) bolus injection of cddp 100 mg / m2 alone or combined with 5 - fu 1 , 000 mg / m2 in continuous infusion induction bolus injection of cddp 100 mg / m2 alone or combined with 5 - fu 1 , 000 mg / m2 in continuous infusion induction of bolus injection of cddp 100 mg / m2 alone or combined with 5 - fu 1 , 000 mg / m2 in continuous infusion awith a minimum interval of 6 h strahlenther onkol 2003 no . 
 all centers used a cone - down technique with all anatomic regions of possible microscopic spread included in the large volume and a boost volume covering the initial sites of macroscopic tumor involvement including the primary lesion and palpable lymph nodes . 
 there was no strong correlation between weight loss after rt + ct and patient - related factors or toxicity scores on the eortc / rtog scale if the analysis was restricted to oropharyngeal carcinoma ( the most frequent subsite within the head and neck in this material , n = 104 )  . 
 delayed healing of early morbidity a 12 - week follow - up was available in 49 of 217 patients ( 23% ) in the rt group and 31 of 182 patients ( 17% ) in the rt + ct group . 
 in order to test whether patients with a 12 - week follow - up were representative for the whole population , we compared the disease status and the maximum grade and the score at week 5 of early toxicity in patients who were ( 80 patients ) or table 4 . 
early morbidity after radioand chemotherapy of head and neck cancer were not ( 311 patients ) seen at week 12 . not surprisingly , patients seen at week 12 tended to have less advanced disease than those who were not . 
in terms of early toxicity , there was no general trend ; patients seen at week 12 had early reactions at week 5 that were comparable to the reactions seen at that time in patients who did not have a follow - up at week 12 . 
one patient died of malnutrition , refusing supportive care ; one malnourished died from candida septicemia ; one patient died from pneumonia as a consequence of a severe laryngeal edema ; one patient died from a massive oropharyngeal hemorrage in a setting of post - chemotherapy thrombopenia . 
 discussion depending of the dose of ct and radiation schedules , the early toxicity of rt + ct is often severe [ 1 , 2 , 8 , 10 , 14 , 21 ]  . however , as pointed out by trotti [ 20 ] , early toxicity is poorly documented in many studies . 
this is true both in the case of morphologic endpoints like the pattern of mucositis , as well as functional endpoints like dysphagia , weight loss and the need to hospitalize the patient for supportive care . 
 a particular concern is the observation that 29% of the patients had grade 2 mucosal reactions at week 12 after rt + ct as compared with just 4% after rt alone . 
 it was not the aim of this study to compare the relative merits of the different treatment schedules analyzed here . such a comparison would have required a more standardized scoring of morbidity between the centers . 
however , there is strong clinical evidence that protracting rt leads to a loss of locoregional control , and experimental studies seem to indicate that the same is the case after cytotoxic drug therapy [ 9 ]  . 
studies of treatment - related morbidity have largely been nonrandomized [ 6 ] , and one may argue that estimates of the prevalence of morbidity are less prone to the selection bias that affects most comparisons of efficacy of various treatments . 
the patients are often followed in a standard schedule during therapy and adverse events are scored using an established scoring syste also late treatment - related morbidity can be subject to nonrandomized studies [ 1214 ]  . 
in the present database , the quality of late morbidity data was too poor to allow any meaningful analysis to be carried out . only one of the studies analyzed here , namely basel , followed strahlenther onkol 2003 no . 
obviously , the experience from the introduction of new or modified treatments would be much more valuable if a formal prospective protocol were followed . conclusion the incidence of multiple early morbidity signs and symptoms was significantly higher after combined rt + ct than after rt alone . 
 strahlentherapie und onkologie original article californium - 252 ( 252cf ) versus conventional gamma radiation in the brachytherapy of advanced cervical carcinoma long - term treatment results of a randomized study taco tacev1 , blanka ptckov1 , vratislav strnad2 background : when photon radiotherapy is applied to cervical carcinoma , it has been observed that , despite important progress in radiotherapy technique and quality assurance , no significant increase in curative rates has resulted . 
treatment with californium - 252 ( 252cf ) , as a source of gamma / neutron radiation in brachytherapy , provides properties and new treatment modalities that help to overcome this factor . 
 patients and methods : from january 1985 to june 1993 , 227 women with stage iib and iiib cervical carcinoma were treated in a randomized brachytherapy study as follows : ( 1 ) 117 patients ( 55 with stage iib , 62 with stage iiib ) were treated with 252cf during the 1st week of therapy by 6 gy ( 40 gy - eq ) of the neutron component in point a . 
 key words : carcinoma of the cervix uteri ( cervical carcinoma ) brachytherapy californium - 252 ( 252cf ) treatment results strahlenther onkol 2003 ; 179 : 37784 doi 10.1007 / s00066 - 003 - 1005 - 4 californium - 252 ( 252cf ) versus konventionelle gamma - strahlentherapie in der brachytherapie von fortgeschrittenem zervixkarzinolangzeitergebnisse einer randomisierten studie hintergrund : trotz wichtiger fortschritte in den strahlentherapeutischen techniken und der qualittssicherung lieen sich durch die konventionelle photonentherapie beim zervixkarzinom keine signifikanten verbesserungen der heilungsraten erzielen . 
die neutronenbrachytherapie mit californium - 252 ( 252cf ) stellt eine neue therapiemodalitt dar , die dem therapeuten helfen kann , diese strahlenresistenz zu berwinden . patienten und methodik : zwischen januar 1985 bis juni 1993 wurden 227 patientinnen mit zervixkarzinom im stadium iib und iiib im rahmen einer randomisierten brachytherapiestudie wie folgt behandelt : 1 . 
die ergebnisse der behandlung zwischen beiden gruppen wurden verglichen . 1 masaryk memorial cancer institute , brno , czech republic , 2 department of radiation oncology , university of erlangen - nrnberg , erlangen , germany . 
 schlsselwrter : zervixkarzinom brachytherapie californium - 252 therapieergebnisse introduction despite important progress in radiotherapy technique and quality assurance , it has been observed that there is no significant increase in curative rates when photon radiotherapy only is applied to cervical carcinoma . 
we believe one of the factors responsible for the lack of effective advance in this area is that information relating to the biology of the tumor , itself , has not been sufficiently incorporated into radiation treatment . briefly , the eradication of cervical carcinoma in photon therapy is caused by specific interactions of photons with tumor cells , in which the biological effect leading to tumor cell death is determined by numerous factors and phenomena . 
most important here are the state of oxygenation of the tumor population , cell kinetic factors , including the cells ability to repair radiation damage , and other inherent factors , resulting in differences in the radiosensitivity of distinct tumor populations during irradiation [ 19 ]  . 
 tumor resistance to gamma radiation can be overcome by the application of radiotherapy with high linear energy transfer ( let ) or by tumor sensitization to the gamma radiation accomplished by systemic chemotherapy [ 10 , 20 ]  . 
 the discovery of 244cf in 1950 [ 28 ] , followed , in 1956 , by its radionuclide 252cf as a neutron / gamma radiation source with a neutron emission of 2.3 ( cid : 1 ) 1012 s1g [ 5 ] , opened up the possibility of high - let brachytherapy in tumor treatment [ 17 ]  . however , the results of the first tumor therapy trials using the 252cf nuclide were unconvincing [ 2 , 3 , 18 , 30 , 34 ]  . 
even in these early studies it was shown that inclusion of 252cf usage in tumor brachytherapy often produced better results , depending on the method of administration of 252cf , than conventional brachytherapy , thereby creating prospects for improved therapy outcomes [ 12 , 13 , 15 , 33 ]  . 
 our research program , started in 1985 , also used 252cf neutron brachytherapy , with gamma radiation , for treatment of cervical carcinoma , in a study pursuing two objectives . 
in addition to a clinical - experimental study aimed at the improvement of treatment procedure by determining optimum levels of the neutron component [ 22 , 25 , 27 ] , our program also consisted of a randomized clinical study comparing the curative effects of 252cf intracavitary therapy ( with added gamma radiation to ensure the application of the same gy - equivalent doses ) and gamma radiation - only intracavitary therapy . 
 the subject of the paper presented is to compare the treatment results of the actual 5 - year survival in patients with cervical carcinoma treated with brachytherapy by 252cf plus gamma radiation vs . 
 patients and methods following construction of a specialized therapy room for intracavitary 252cf therapy [ 21 ] , a randomized study of 227 patients with cervical carcinoma was conducted during the period of january 1985 to june 1993 . 
117 patients ( 55 with stage iib , 62 with stage iiib ) were treated with neutron brachytherapy by 252cf ( with supplementary gamma radiation ) , while 110 patients ( 50 stage iib , 60 stage iiib ) were treated solely by gamma brachytherapy . 
the stage of disease was determined according to the figo classification on the basis of the following examinations : inspection , palpation , biopsy , cystoscopy , intravenous pyelography ( ivp ) , renography , bone scintigraphy , liver sonography , chest x - ray , and hematologic / biochemical examination of the blood . 
the patients age , stage of disease , and tumor grade served as criteria for stratified randomization . these criteria were considered during distribution of patients into separate groups , so that there was no significant differentiation of any parameter in any of the groups to be compared . the distribution of patients into the particular groups was realized on the random selection principle . 
stratifikation der patientinnen mit zervixkarzinom im stadium iib und iiib nach alter . tients in the two groups are listed in table 1 , the staging and grading in table 2 . 
 as stated previously , one of our objectives was to test 252cf neutron brachytherapy versus gamma brachytherapy . for this purpose , we needed to equalize the irradiation in terms of gy - equivalent doses that both groups would receive . the conversion of 252cf doses to gy - equivalents ( gy - eq ) was made using the following formula : ( gy - eq ) = ( dn ( cid : 1 ) rben ) + ( dg ( cid : 1 ) rbe ) = 252cf neutron component dose , = 252cf gamma component dose , where : rben = relative biological effectiveness of neutrons , rbe = relative biological effectiveness of gamma radiation . the rbe of the 252cf neutron component had the value brachytherapy in both 252cf and gamma radiation - only groups for both the 252cf group and the gamma radiation - only group , low dose rate sources were used for intracavitary therapy . 
the dose at point a ( 56 gy ) of patients treated intracavitarily with gamma radiation only was split into two parts , applied in the 3rd and 5th week of therapy , respectively . 
 external radiation in both 252cf and gamma radiationonly groups ( all 227 patients ) for both groups , the external radiation was given by standard x - ray 20 - mev beams of a linear accelerator . 
the applied dose of 40 gy ( 2 gy / day ) was administered with two opposite fields as divided doses of 20 gy in full and split fields to the small pelvis . 
the width of the central shield of the split field was 4 cm and , consequently , the dose at point a of the split field was approximately 15 gy . the total dose applied to patients of all groups was 85 gyeq at point a and 59 gy - eq at point b . 
 after completion of treatment , patients in both groups received long - term follow - up monitoring according to the following scheme : once per month during the first 6 months following treatment ; once per 3 months for the period of 7 months following treatment to the end of the 3rd year ; and once per 6 months from the end of the 3rd year on . 
 a statistical comparison of the treatment results of the procedures was performed according to the log - rank test and kaplan - meier method for survival rates and according to the mann - whitney nonparametric test ( spss version 10.0.5 for windows ) for side effects rates . 
ergebnisse der behandlung mit 252cf und gamma - strahlentherapie und der alleinigen gamma - strahlentherapie bei patientinnen mit zervixkarzinom stadium iiib . gamma only ( 110 pts . ) 252cf + gamma ( 117 pts . ) time ( years ) figure 2 . 
 the distribution of deaths over time caused by a recurrence of primary disease ( small pelvis ) has been compared for the patients of both groups ( 252cf and gamma therapy only ) as shown in figure 5 . 
in patients treated with neutron brachytherapy , the appearance of early and late side effects was lower compared to the same reactions in patients treated by gamma radiation only , without being significant . 
 for an understanding of the differences between the therapy effects of radiation with different let quantities , it is necessary to compare certain biological activities on the cellular and tissue levels , which are induced during treatment as a result of specific interactions with the tumor cells by the gamma photons ( low let ; low kev per micron ) and neutrons ( high let ; high kev per micron )  . 
 during tumor brachytherapy , the biological effects of 252cf radiation are caused mainly by neutrons , even though the neutron component is 60% of the source spectruthis is due to the increase in the rbe value of the neutron as a consequence of the very rapidly diminishing dose input over a gamma only ( 110 pts . ) 252cf + gamma ( 117 pts . ) years discussion the above results show that application of 252cf neutron radiation , with gamma radiation , in uterovaginal intracavitary therapy creates promising prospects for improvement in the curative rates of cervical carcinoma as a consequence of eradication of that part of the tumor cell population resistant to conventional photon radiation . 
comparison of distribution of deaths over time due to recurrent primary disease ( in small pelvis ) of stage iib and iiib patients by treatment ( 252cf and gamma irradiation only )  . 
 gastrointestinal stage iii stage i acute proctitis 45.5% ( 50 ) 8.2% ( 9 ) 5.5% ( 6 ) stage ii chronic rectal proctitis ulcer rectovaginal fistula 4.5% ( 5 ) 16.2% ( 19 ) 1.8% ( 2 ) 0.8% ( 1 ) 0.8% ( 1 ) urologic stage i acute cystitis 8.2% ( 9 ) stage iii stage ii chronic urocystic cystitis 6.4% ( 7 ) 3.6% ( 4 ) ulcer 5.1% ( 6 ) 11.1% ( 13 ) gamma irradiation only ( n = 110 ) irradiation with 252cf ( n = 117 ) gamma irradiation only ( n = 110 ) irradiation with 252cf ( n = 117 ) very short distance ( a few centimeters )  . 
 further biological effects of high - let radiation include lower oxygen enhancement rate ( oer ) [ 30 , 33 ] , inhibition of sublethal and potentially lethal cell damage repair [ 11 , 28 , 31 ] and minimal dependency of radiation sensitivity on cell cycle [ 29 ]  . 
 the biological effect of a neutron component is generally expressed as the rbe ; the value for 252cf neutron radiation is in the range of 38 [ 1 , 6 , 8 , 9 , 13 ]  . 
with the use of 252cf for intracavitary therapy , this combined process is influenced by the qualitatively different natures and effects of these two radiation types : high let ( intracavitary 252cf radiation ) and low let ( gamma radiation , both external and brachytherapy )  . 
in patients irradiated with 252cf in the final phase ( after external radiation ) , the results were equivalent when compared to treatment by intracavitary gamma radiation only . in his interpretation of the reasons for this difference , maruyama hypothesized that reoxygenation of the surviving tumorous tissue after 252cf radiation in the initial phase of therapy has the potential effect of making the tumor more sensitive . 
he based this on the fact that , as a consequence of the neutron - cell interactions occurring in the 1st week of therapy , a great number of tumorous cells are destroyed , including hypoxic ones . 
this leads to a release of pressure on the vascular network inside and supplying the tumor , a resultant restoration or increase of blood flow , and , thus , an increase of po2 in the tumorous tissue . 
we learned that during the gamma radiation - only therapy there are no significant changes in the po2 of the tumor tissue , while these changes are significant during 252cf treatment applied in the initial phase of therapy with either 2 , 6 , or 9 gy of the neutron component . 
in our study , the reoxygenation ability was highest in tumors irradiated with low and medium neutron doses ( 2 and 6 gy , respectively ) , while after the full neutron dose ( 9 gy ) , the reoxygenation ability of the tumorous tissue was significantly reduced . 
 during monitoring of the changes in the regression dynamics of the tumorous tissue in the course of therapy , we discovered that by irradiation with the same gy - equivalent dose , strahlenther onkol 2003 no . 
252cf brachytherapy of cervical carcinoma even a 2 - gy portion of the 252cf neutron component in the dose significantly decreased the time needed for the tumor to regress to 50% of its initial size , compared to gamma irradiation only . 
it should be noted that the above changes in the dynamics of reoxygenation and tumor regression after neutron irradiation during the 1st week of therapy can be influenced not only by the neutron dose , but also by the initial state and subsequent radiation damage during treatment of the stromal elements of the tumor , mainly of the capillary network . 
 the correlation of the aforementioned phenomena , as a reflection of changes in the tumor tissue following interactions with different doses of the 252cf neutron component , and the therapy results was reported in 1997 [ 24 ]  . 
 there is evidence that in addition to the zonal heterogeneity produced by microenvironmental factors such as hypoxia , intrinsic genetic heterogeneity in the tumor stem cell population could play a role in determining a tumors response to treatment [ 36 ]  . 
 [ 37 ] endeavored to hypothetically explain , by means of a mathematical model , the reasons for the phenomenon of early and late application of 252cf in relation to external gamma irradiation during the therapeutic procedure . 
the authors based their work on the assumption that there are two types of cells : predominantly radiosensitive cells and a small amount of doubly resistant cells , which are mutations of normally radiosensitive ( i.e. , normally radioresistant ) cells . 
these doubly resistant cells are highly radioresistant to gamma radiation because they possess the ability to repair sublethal and potentially lethal dna damage and are characterized by their shorter cell cycle . 
 the results of our clinical research of 252cf usage in tumor brachytherapy show that this qualitatively new , highly effective method of treatment is able to eliminate tumor cells resistant to conventional gamma radiation . 
it should be noted that , compared to external fast neutron therapy , 252cf brachytherapy allows direct interaction of the neutrons with cells of the tumor population , thus minimizing the postradiation damage to healthy tissues . 
 the present state of research on the clinical use of 252cf in tumor brachytherapy has been assembled and summarized at the californium - 252 isotope for 21st century radiotherapy workshop , in detroit , usa , in 1996 [ 35 ]  . 
it was stated that the physics , dosimetry and clinical prerequisites for the introduction of 252cf sources into clinical practice have been achieved . however , the commercial manufacture of afterloading systems for mediumand high - activity 252cf sources was left unsolved . 
die autoren konnten bei 89 anmischen patienten ( hb < 12 g / dl ) gegenber 229 patienten mit normalen prtherapeutischen hmoglobinwerten ein signifikant schlechteres berleben ( p = 0 , 004 ; relatives todesrisiko der anmie = 1 , 47 ) in der univariaten analyse nachweisen . 
 frhere eigene untersuchungen bei operierten und nachbestrahlten hirntumoren zum prognoseeinfluss des hmoglobinwertes zeigten bei allerdings kleineren patientenzahlen ( n = 110 ) analoge ergebnisse nur bei den astrozytomen ( berwiegend grad iii ) , jedoch nicht bei den glioblastomen [ 1 , 2 ]  . 
so konnte bei den astrozytomen ( n = 37 ) ein mittleres berleben von 45 monaten bei einem prtherapeutischen hmoglobin > 8 mmol / l ( 12 , 8 g / dl ) gegenber 26 monaten bei hb < 8 mmol / l beobachtet werden . 
im gegensatz dazu betrug das mittlere berleben bei den glioblastomen ( n = 73 ) lediglich 6 monate bei einem hb > 8 mmol / l , aber 13 monate bei einem anmischen hb - wert < 8 mmol / l . 
infolge weitgehend identischer verteilung der prognoserelevanten parameter alter und karnofsky - index ist die vergleichbarkeit der anmischen mit der nicht anmischen gruppe sowohl beim astrozytom als auch beim glioblastom gegeben . 
schlechteren berlebensraten der eigenen untersuchungen bei der glioblastomgruppe mit normalen hmoglobinwerten beruhen damit offensichtlich selektionsbedingt auf einem hheren anteil zentral sitzender tumoren ( nicht untersucht ) , wobei auch die problematik der operativen radikalitt mit bedacht werden sollte . 
6 urban & vogel strahlentherapie und onkologie original article in vivo tgf - ( cid : 1 ) 3 expression during wound healing in irradiated tissue an experimental study stefan schultze - mosgau1 , falk wehrhan1 , kerstin amann2 , martin radespiel - trger3 , franz rdel4 , gerhard g . 
grabenbauer4 1 and tgf - ( cid : 1 ) background : wound - healing disorders frequently present a clinical problem in patients with squamous epithelial carcinomas of the head and neck region after surgical interventions such as grafts of free flaps in preirradiated graft bed tissues . 
while it was possible to experimentally show a fibro2 , a fibrosis - reducing and radioprotective effect has been described for tgf - ( cid : 1 ) sis - inducing activity for tgf - ( cid : 1 ) 3 on epithelial cells and fibroblasts . 
the influence of irradiation and tissue grafting on the tgf - ( cid : 1 ) 3 expression , however , remains uncertathe objective of the in vivo study was therefore to analyze the expression profile of tgf - ( cid : 1 ) 3 in the graft bed and in the transition area between the graft and the graft bed after irradiation and / or after surgery . 
a free myocutaneous gracilis flap was transplanted in 30 rats : group 1 ( n = 18 rats ) no transplantation , only irradiation ( 3 ( cid : 2 ) 10 gy ) ; group 2 ( n = 14 rats ) transplantation without preoperative irradiation ; group 3 ( n = 16 rats ) transplantation following preoperative irradiation ( 3 ( cid : 2 ) 10 gy )  . the interval between radiotherapy and grafting was 4 weeks . 
tissue samples were taken perioperatively and postoperatively after 3 , 4 , 7 , 11 , 14 , 28 , and 30 days from the transition area between the graft and the graft bed and from the graft bed itself . 
the rats that were irradiated but not operated on showed significantly ( p = 0.04 ) reduced tgf - ( cid : 1 ) 3 expression in the graft bed immediately after the end of the irradiation . 
the exogenous 3 could therefore present a new therapeutic approach for improving wound healing through radioprotection key words : free soft tissue grafts irradiated graft bed wound healing tgf - ( cid : 1 ) 3 immunohistology animal model strahlenther onkol 2003 ; 179 : 4106 doi 10.1007 / s00066 - 003 - 1049 - 5 in - vivo - tgf - ( cid : 1 ) 3 - expression bei der wundheilung in bestrahlten geweben . 
eine zentrale rolle nehmen dabei die isoformen des transforming growth factor ( cid : 1 ) ( tgf - ( cid : 1 ) 13 ) ewhrend fr 2 experimentell eine fibroseinduzierende aktivitt gezeigt werden konnte , sind fr tgf - ( cid : 1 ) tgf - ( cid : 1 ) 3 eine fibrosereduzierende wirkung und ein radioprotektiver effekt auf epithelzellen und fibroblasten beschrieben . 
ziel der in - vivo - untersuchung war deshalb die analyse 1 und tgf - ( cid : 1 ) 1 department of oral and maxillofacial surgery , 2 institute of pathology , 3 institute of medical informatics , biometry and epidemiology , and 4 department of radiation oncology , university of erlangen - nrnberg , erlangen , germany . 
tgf - ( cid : 1 ) 3 expression during wound healing in preirradiated tissues 3 im bergangsbereich zwischen transplantat und transplantatlager sowie im transplantatlager des expressionsprofils von tgf - ( cid : 1 ) nach alleiniger bestrahlung und / oder operation . 
bei 30 tieren erfolgte die verpflanzung eines freien myokutanen grazilislappens : gruppe 1 ( n = 18 tiere ) keine transplantation , nur radiotherapie ( 3 ( cid : 2 ) 10 gy ) ; gruppe 2 ( n = 14 tiere ) transplantation ohne properative radiotherapie ; gruppe 3 ( n = 16 tiere ) transplantation nach properativer radiotherapie ( 3 ( cid : 2 ) 10 gy )  . 
perioperativ sowie 3 , 4 , 7 , 11 , 14 , 28 und 30 tage postoperativ wurden gewebeproben aus dem bergangsbereich zwischen transplantat und lager sowie aus dem transplantatlager entnommen , die tgf - ( cid : 1 ) 3 - expression immunhistochemisch qualitativ und quantitativ ( labeling - index ) untersucht und auf statistische unterschiede berprft ( p < 0 , 05 )  . 
whrend eine alleinige transplantation ohne vorbestrahlung im postoperativen verlauf zu geringen unterschieden der tgf - ( cid : 1 ) 3 - expression im transplantatlager und im bergangsbereich transplantat / transplantatlager fhrte , zeigte sich in der bestrahlten und operierten gruppe eine signifikant reduzierte expression im lager ( p = 0 , 018 )  . 
die exogene applikation von tgf - ( cid : 1 ) 3 knnte einen neuen therapeutischen ansatz zur verbesserung der wundheilung durch radioprotektion nicht transformierter epithelzellen und fibroblasten nach properativer radiotherapie und chirurgie darstellen . 
 schlsselwrter : freie weichgewebetransplantate bestrahltes transplantatlager wundheilung tgf - ( cid : 1 ) logie tiermodell 3 immunhistointroduction wound - healing disorders occur in varying degrees within the framework of reconstructive surgery after preoperative radiotherapy of patients with head and neck tumors , particularly with the healing of free grafts in preirradiated tissue [ 8 , 14 , 15 , 17 , 26 , 29 , 35 ]  . 
here , the risk of losing a graft is increased compared with the use of free grafts in a nonirradiated bed [ 2 ]  . possible causes include delayed granulation tissue formation and delayed reepithelialization in the proliferation and remodeling phases of the wound - healing process , reduced vascularization , and increased fibrosis in the transition area between the graft and the preirradiated graft bed [ 31 , 34 ]  . 
 1 , tgf - ( cid : 1 ) 2 and tgf - ( cid : 1 ) the influence of radiotherapy can be seen particularly in the complex cytokine network which regulates the woundhealing process [ 16 , 20 ]  . 
experimentally , it was possible to show that both absence and overproduction of tgf - ( cid : 1 ) lead to wound - healing disorders [ 7 , 10 ]  . 
moreover , tgf - ( cid : 1 ) is an essential profibrotic factor that was found in high concentrations in the fibrotic tissue of various organs and in keloids [ 9 ]  . 
the fibrosis - promoting properties of tgf - ( cid : 1 ) include collagen deposition , stimulation of the synthesis of matrix components in fibroblasts , inhibition of collagenase and plasminogen activators , and chemotaxis for fibroblasts , monocytes and macrophages [ 1 , 24 ]  . 
 in vivo studies showed an increased expression of tgf - ( cid : 1 ) and tgf - ( cid : 1 ) 2 , as well as a consecutively increased synthesis of extracellular matrix components ( ecm ) and wound - healing disorders in the healing area between the grafted tissues and the preirradiated graft bed tissues [ 30 , 32 ]  . 
 1 , exogenous application of tgf - ( cid : 1 ) a radioprotective effect on nontransformed epithelial cells and fibroblasts is described for tgf - ( cid : 1 ) 3 , in addition to radiosensitization of the transformed cells [ 27 ]  . 
 knowledge of the course of tgf - ( cid : 1 ) 3 expression over time after exclusive irradiation and after transplantation of a graft in a preirradiated graft bed is , however , a prerequisite for the application of tgf - ( cid : 1 ) 3 after preoperative radiotherapy . 
the rats were kept in pairs in polycarbonate cages in accordance with the requirements of the german animal welfare act ( animal experiment permit 621 - 2531.31 - 13 / 96 ) at a temperature of 22 0.5 c , at 55% humidity in 12 - h light / dark cycles . 
 in the case of 30 rats , a free myocutaneous gracilis flap was taken from the right groin and grafted to the right neck region where it was microsurgically reanastomosed . 
tgf - ( cid : 1 ) 3 expression during wound healing in preirradiated tissues ing groups of animals were formed to determine the influence of preoperative irradiation on the expression of tgf - ( cid : 1 ) 3 during the healing of the graft : group 1 ( n = 18 rats ) no transplantation , radiotherapy only ( 3 ( cid : 2 ) 10 gy ) ; group 2 ( n = 14 rats ) transplantation without preoperative radiotherapy ; group 3 ( n = 16 rats ) transplantation after preoperative radiotherapy ( 3 ( cid : 2 ) 10 gy )  . 
 preoperative irradiation and transplantation of the free myocutaneous gracilis flap were carried out under inhalation anesthesia with isoflurane ( forene , abott , wiesbaden , germany ) following modification of the circulation system of the anesthesia unit ( tiberius 19 , draeger , bremen , germany )  . immediately before the operation , the rats were given antibiosis consisting of 10 , 000 iu of a broad - spectrum penicillin intraperitoneally ( tardomyocel , bayer , leverkusen , germany ) und and a volume substitution of 1520 ml full electrolyte solution intraperitoneally ( tuto - op , pharmacia - upjohn , erlangen , germany )  . 
 preoperative radiotherapy in the neck region the irradiation was carried out with a linear accelerator having 6 mev photons and a focus of 1 cm2 ( siemens mevatron 67 , siemens , erlangen , germany )  . 
in group 1 , one biopsy was taken per rat ( n = 18 ) from the irradiated neck region and from the skin of the nonirradiated right groin region as an intraindividual check immediately after the last fraction of irradiation , and on days 4 , 7 , 11 , 14 , and 28 after the irradiation had been completed . 
 transplantation of a free myocutaneous gracilis flap in the preirradiated neck region a free myocutaneous gracilis flap measuring 2.5 ( cid : 2 ) 2.5 cm was taken from the right groin and used as the flap model . 
macroscopically , it was possible to clearly identify the transition area by the sutures used for the gra immunohistochemical analysis the preparation of the formalin - fixed samples and immunohistochemical assay with the aid of the avidin - biotin - peroxidase complex was carried out by the method already described [ 32 ]  . 
 tgf - ( cid : 1 ) the samples were prepared in the transition area vertically to the suture at a depth , so that the epidermis , the dermis , and the subcutaneous layers could be seen . 
based on information provided by the manufacturer , it was possible to exclude cross - reactivity of the spe3 antibody with other subspecies ( isoforms tgf - ( cid : 1 ) cific tgf - ( cid : 1 ) and tgf - ( cid : 1 ) 2 )  . 
after incubation ( 30 min , rt ) with a biotinylated antibody ( swine - anti - rabbit , dako , glostrup , denmark , 1 : 200 ) and avidin - biotin / horseraddish - peroxidase complex ( abc / hrp complex , dako ; 30 min , rt ) , the chromogenic assay was carried out with aec ( 0.02% 3 - amino - 9 - ethylcarbazole in 50 mm acetate buffer ph 5 ; 5.5% dimethylformanide , dako )  . 
from each tissue sample , three sections were obtained consecutively and processed on microscopic slides , with one serving as a negative control in each case ( replacement of the primary antibody through incubation with bsa )  . 
 qualitative and quantitative analysis the localization and distribution of the cytoplasmatic tgf - ( cid : 1 ) expression in the fibroblasts in the graft and in the transition area between the graft and the graft bed were evaluated under a bright - field microscope ( axioskop , zeiss , oberkochen , germany ) at a magnification of 50400 ( cid : 2 )  . 
to quantify the expression , the labeling index was determined as a ratio of positively expressing cells and the total number of cells per visual field based on the method of randomized systematic subsampling [ 36 ]  . 
three visual fields per tissue section , sample localization , rat , day , and group were digitized at a magnification of 400 ( cid : 2 ) using a ccd camera ( kappa , gleichen , germany )  . 
300 50 cells in the median were evaluated per visual field , so that the overall number of evaluated cells with three visual fields per section was 900 150 cells . 
 statistical analysis in order to analyze the quantitative extent of tgf - ( cid : 1 ) 3 expression over time , the labeling index was determined per visual field , sample , rat , and day separately for the transition area strahlenther onkol 2003 no . 
tgf - ( cid : 1 ) 3 expression during wound healing in preirradiated tissues between the graft and the graft bed , for the irradiated neck region in groups 2 and 3 ( unconnected samples ) , and for the irradiated neck region and the nonirradiated right groin region in group 1 ( connected samples )  . 
quantitative comparisons without a normal data distribution were carried out with the mann - whitney - u - test for unconnected samples and with the wilcoxon test for connected samples . 
the p - values were adjusted according to bonferroni - holall calculations were made using the program spss v.10 for windows ( spss inc . , chicago , usa )  . 
 results macroscopic results in the group that had not been preirradiated ( group 2 ) , twelve out of 14 grafted tissue flaps healed macroscopically without any complications ( success rate : 86% )  . 
no complications were found with the rats that were exclusively irradiated . erythema or dermal desquamation in the irradiated neck region was not found in any rat at any point of time following irradiation . 
 qualitative analysis of tgf - ( cid : 1 ) 3 expression qualitatively , a reduced tgf - ( cid : 1 ) 3 expression was seen in the preirradiated graft bed and in the transition area between the grafted tissue and the irradiated bed compared with the transition area of the nonirradiated bed ( figures 1 and 2 )  . 
in group 2 , where grafting had taken place without preirradiation , the transition area showed a clear cytoplasmatic tgf - ( cid : 1 ) 3 expression in the fibroblasts ( figure 1 )  . 
perivascularly , an increased expression was found compared with the surrounding tissue . the transition area of the preirradiated and grafted group 3 , however , showed a decreased cytoplasmatic tgf - ( cid : 1 ) 3 expression compared with group 2 , where grafting was carried out without preirradiation ( figure 2 )  . labeling indices of tgf - ( cid : 1 ) 3 expression the quantitative expression of tgf - ( cid : 1 ) 3 after exclusive radiotherapy is shown in figure 3 . 
differences in the tgf - ( cid : 1 ) 3 expression were found in the irradiated and in the nonirradiated tissue on days 0 , 4 , 7 , and 11 after the end of the irradiation series ( figure 3 )  . 
here , the median labeling index for tgf - ( cid : 1 ) in the nonirradiated tissue was 47% ( 4350% ) directly after the end of irradiation and 31% ( 2437% ) on the 28th day after irradiation . 
tgf - ( cid : 1 ) istry ; 7th postoperative day in nonirradiated group ( tgf - ( cid : 1 ) sented by red - marked fibroblasts ; 200 ( cid : 2 ) magnification )  . 
tgf - ( cid : 1 ) 3 expression in the transition area by immunohistochemistry ; 7th postoperative day in the group irradiated with 30 gy ( tgf - ( cid : 1 ) 3 is represented by red - marked fibroblasts ; 200 ( cid : 2 ) magnification )  . 
tgf - ( cid : 1 ) 3 expression during wound healing in preirradiated tissues the 3rd postoperative day , of 21% ( 1723% ) on the 7th postoperative day , and of 29% ( 25.532% ) on the 28th postoperative day . 
 figure 5 shows the expression profile for tgf - ( cid : 1 ) 3 in the transition area of the grafted tissue and the nonirradiated ( group 2 ) and irradiated bed ( group 3 )  . 
the expression of tgf - ( cid : 1 ) 3 in the transition area of the nonirradiated group 2 showed a constant median labeling index over the entire study period . 
the tgf - ( cid : 1 ) 3 expression in the transition area of the preoperatively irradiated group 3 showed a median labeling index of 26% ( 2138% ) on the 3rd postoperative day , of 45% ( 4448% ) on the 14th postoperative day , and of 32% ( 2735% ) on the 28th postoperative day . 
the biphasic expression 3 could be the cause for the reduced tgf - ( cid : 1 ) pattern of tgf - ( cid : 1 ) expression on the 7th postoperative day in the irradiated and nonirradiated graft beds . 
it was also possible to show that no significant ( p = 0.73 ) differences in tgf - ( cid : 1 ) 3 expression existed in the preirradiated tissue in the transition area of the grafted and preirradiated or nonirradiated bed tissue in contrast to the case of cytokine expression . 
while several studies can be found on the influence of ionizing radiation on the expression of tgf - ( cid : 1 ) and tgf - ( cid : 1 ) 2 and the induction of fibrosis , there are few refer3 expression in irradiated and nonirradiated sk discussion figure 3 . 
it slightly increased over time to 31% ( 1840% ) on the 28th day after irradiation . 3 expression profiles over time in the nonirradiated graft bed ( group 2 ) and in the preoperatively irradiated graft bed ( group 3 ) are shown in figure 4 . 
the transition area between the grafted tissue and the nonirradiated graft bed showed expression profiles of 45% ( 3752% ) on the 3rd postoperative day , of 29% ( 28.532% ) on the 7th postoperative day , and of 38% ( 3549% ) on the 28th postoperative day . 
by comparison , the transition area of the irradiated graft bed tissue showed a lower tgf - ( cid : 1 ) 3 expression of 34% ( 2246% ) on 3 expression in preoperatively irradiated and nonirrafigure 4 . 
a fibrosis - protective effect was shown for tgf - ( cid : 1 ) 3 , and after the exogenous application of tgf - ( cid : 1 ) 3 to skin wounds , accelerated wound healing was found with an improvement of the architecture of the neodermis [ 33 ]  . 
under the aspect of fibrosis , it is thus possible to discuss antagonizing effects for tgf - ( cid : 1 ) 1 and tgf - ( cid : 1 ) 2 . 
in addition to the basic fibroblast growth factor ( fgf2 ) and the platelet - derived growth factor ( pdgf ) , the isoforms tgf - ( cid : 1 ) 3 influence fibroblast proliferation and collagen synthesis within the framework of wound healing . 
while a stimulation of type i collagen synthesis is described for tgf - ( cid : 1 ) 1 through an increase in the number of collagen - producing fibroblasts , the effect of tgf - ( cid : 1 ) appears to lie in the influence of the pro 2 ( i ) collagen promoter region [ 18 ]  . 
the cause for a fibrosis - protective effect is seen , on the one hand , in an increased proliferation rate of fibro - blasts after the application of tgf - ( cid : 1 ) 3 and , on the other hand , in an activation of the pro 2 ( i ) collagen promoter region [ 18 ]  . 
the effect of a pro 2 ( i ) collagen promoter activation is clearer with tgf - ( cid : 1 ) 3 than with fgf2 or pdgf [ 18 ]  . in addition to other cytokines , such as vegf , an induction of neovascularization was described for tgf - ( cid : 1 ) 3 in vivo [ 1 , 18 , 21 ]  . 
 the radiation - induced reduction of capillary vascularization and the increased ecm synthesis in the irradiated tissue is thought to be caused by the proliferative effect of tgf - ( cid : 1 ) [ 21 , 28 ]  . 
however , in nonirradiated tissue it was possible to show that tgf - ( cid : 1 ) 1 , depending on the concentration , produces either angiogenic effects on the endothelial cells or stimulating effects on the proliferation of fibroblasts and the synthesis of ecm components [ 11 , 19 ]  . 
at the same time , tgf - ( cid : 1 ) 1 inhibits ecm reduction and modulates the interaction of cells with the ecm via integrin receptors [ 13 ]  . 
thus , a link was observed between arteriosclerotic vascular changes and a reduction of the cd105 / tgf - ( cid : 1 ) 3 complex [ 22 ]  . 
 [ 21 ] studied the expression level of the tgf - ( cid : 1 ) isoforms in keloids and found an increased expression level for tgf - ( cid : 1 ) 3 in a normal skin architecture . in patients suffering from scleroderma , querfeld et al . 
 [ 28 ] compared the mrna content of tgf - ( cid : 1 ) 1 , 2 , 3 in inflammatory and fibrotically changed skin with that of healthy skhere , an increased level of mrna was found for tgf - ( cid : 1 ) 1 in fibrotic skin compared with that of healthy skin with no increased tgf - ( cid : 1 ) 3 rna . 
in our own in vivo studies , fibrosis and overexpression of tgf - ( cid : 1 ) 1 , 2 were found postoperatively in the irradiated bed , both clinically and histologically [ 31 ]  . 
other studies have shown that tgf - ( cid : 1 ) modulates the apoptosis rate of intestinal mucosa cells via the apoptosis - associated proteins bcl - xl and bcl - 2 [ 12 ]  . 
 an experimental and clinical approach for reducing fibrosis during wound healing in preirradiated tissue could be found in the application of recombinant tgf - ( cid : 1 ) 3 at the time of irradiation , in order to compensate the reduced expression rate of fibrosis - protective tgf - ( cid : 1 ) 3 and in order to increase the radioresistance of nontransformed cells . 
this appears to be expedient , since in cell culture experiments it was also possible to show an increased radioresistance of the stem cells of the mucosa of the small intestine after the application of tgf - ( cid : 1 ) during irradiation [ 27 ]  . 
thus , control of the profibrotic or wound - healing effects through exogenous modulation of cytoplasmatic signal proteins for tgf ( cid : 1 ) also appears to be possible in the signal chain of the cytokine effect via the smad proteins [ 6 ]  . 
 strahlentherapie und onkologie original article inverse automated treatment planning with and without individual optimization in interstitial permanent prostate brachytherapy with highand low - activity 125i michael pinkawa1 , uwe maurer1 , andrew mulhern1 , bernd gagel1 , thomas block2 , holger borchers3 , johannes grieger4 , thomas henkel5 , michael eble1 purpose : to determine whether dose distribution achieved with treatment plans using highand low - activity 125i implants differs . 
 patients and methods : based on intraoperative transrectal ultrasound scans of 71 patients , inverse automated treatment plans ( iatp ) were performed with 15.5 - kbq ( 0.42 - mci ) and 25.2 - kbq ( 0.68 - mci ) 125i implants using a commercial 3 - d planning system ( variseed )  . 
a prescription dose of 145 gy in 98% of the prostate volume ( v100 ) , a maximum dose to the urethra of 250 gy ( d1 ) , and a maximum dose to 10% of the anterior rectal wall of 145 gy ( d10 ) were required . 
after manual optimization , the differences were only marginal with a prostate v100 of 99% for both activities , a urethra d1 of 247 gy and 239 gy , and a rectum d10 of 135 gy and 124 gy for highand low - activity seeds . 
low - activity seeds required more sources ( 66 vs 47 ) and needles ( 24 vs 17 ; all numbers are median values )  . conclusions : concerning the prostate dose coverage , high - activity seeds are superior in the iatp . 
 key words : prostate cancer brachytherapy 125i permanent implants treatment planning strahlenther onkol 2003 ; 179 : 41722 doi 10.1007 / s00066 - 003 - 1042 - z inverse automatische bestrahlungsplanung mit und ohne individuelle optimierung bei der interstitiellen permanenten brachytherapie des prostatakarzinoms mit 125j hoher und niedriger aktivitt fragestellung : erzielt die bestrahlungsplanung sowohl mit hochals auch mit niedrigaktiven 125j - seeds eine optimale dosisverteilung ? patienten und methodik : basierend auf intraoperativen transrektalen ultraschallbildern von 71 patienten erfolgte eine inverse automatische bestrahlungsplanung ( iatp ) unter verwendung von 15 , 5 - kbq - ( 0 , 42 - mci - ) und 25 , 2 - kbq - ( 0 , 68 - mci - ) - 125j - seeds mit einem kommerziellen 3 - d - planungssystem ( variseed )  . 
eine verschreibungsdosis von 145 gy in 98% des prostatavolumens ( v100 ) , eine maximale dosis im bereich der urethra von 250 gy ( d1 ) und maximal 10% der rektumvorderwand im bereich der 145 - gy - isodose ( d10 ) wurden gefordert . 
nach manueller optimierung waren die unterschiede nur marginal ( prostata v100 von 99% fr beide aktivitten , urethra d1 von 247 gy und 239 gy und rektum d10 von 135 gy und 124 gy fr hohe und niedrige aktivitten )  . 
 1 department of radiotherapy , university hospital , rwth aachen , germany , 2 urologic practice , vaterstetten , germany , 3 department of urology , university hospital , rwth aachen , germany , 4 institute for clinical radiology , radiation clinic , university hospital , mannheim , germany , 5 outpatient surgical center ( ambulantes operationszentrum im ullsteinhaus gmbh ) , berlin - tempelhof , germany . 
bercksichtigt man die anzunehmende geringere toxizitt und krzere implantationsdauer fr eine kleinere anzahl von seeds , so sind hochaktive seeds fr erfahrene teams zu empfehlen . schlsselwrter : prostatakarzinom brachytherapie 125j permanentimplantate bestrahlungsplanung introduction prostate cancer is the most frequent malignant tumor of elderly men . 
by treating locally confined prostate cancer ( predicted by psa 10 ng / ml and gleason score 6 [ 3 ] ) with interstitial permanent brachytherapy using 125i seeds , it is possible to achieve similar biochemical relapse - free survival rates as after radical prostatectomy and conformal radiotherapy with doses between 70 and 75 gy [ 9 , 20 ]  . 
the problem of prostate movement inside the pelvis does not exist , because the radioactive sources are implanted inside the prostate [ 14 ]  . different activities of 125i seeds can be used . 
after definition of the required dose values for the prostate and the maximum values for the organs at risk ( urethra and anterior rectal wall ) , the planning software calculates the best possible loading plan . 
 patients and methods between january 2000 and april 2001 , a total of 71 patients with locally confined prostate cancer ( t12 , gleason score 6 , psa 10 ng / ml ) were treated with 125i seeds . 
a maximum number of 110 125i seeds ( rapid strands ) and 35 needles , a maximum distance of 5 mm to the organs at risk ( urethra , anterior rectal wall ) and 2 mm outside the prostate capsule were allowed . 
a minimum dose of 120 gy ( d100 the dose that covers 100% of the prostate volume ) to the prostate and a prescribed dose of 145 gy to 98% ( v100 the percentage of the prostate volume receiving the prescribed dose ) of the prostate volume were required . 
an importance factor of 10 ( highest factor ) for the prostate values and 1 ( lowest factor ) for the maximum values at the organs at risk was defined . 
the dose values covering 100% ( d100 ) and 90% ( d90 ) of the prostate volume as well as the volumes reached by the prescribed dose ( v100 ) and the maximum doses at the organs at risk were compared . 
with respect to the individual prostate volume , a significantly higher number of seeds and implant needles were required for both iatp and iatpopt using low - activity seeds ( table 1 )  . 
the limit dose of 250 gy was exceeded in 3% ( iatp ) / 6% ( iatpopt ) with low - activity and 28% ( iatp ) / 9% ( iatpopt ) with high - activity sources . 
 the maximum dose was mostly reached in only a small volume area , as shown in an example of a typical dose - volume histogram of the urethra ( figure 5 )  . 
 100% 200% rectum 150% seed the median maximum dose at 10% of the anterior rectal wall ( d10 ) was 88 ( 36138 ) and 123 ( 57183 ) gy according to the iatp for lowand high - activity seeds ( figure 6 ) , 123 ( 80152 ) and 135 ( 19152 ) gy after optimization . 
the set limit dose was exceeded in 0% ( iatp ) / 14% ( iatpopt ) and 6% ( iatp ) / 17% ( iatpopt ) with the application of low and high activities . 
the maximum number of 110 125i seeds and 35 needles defined for the iatp was exceeded in only one case after manual correction . as shown in table 2 , the dose values d100 and d90 and the volume percentage value v100 met the requirements clearly better after iatp with high - activity seeds than with low - activity seeds ( 92% compared to 52% of patients with a d90 of 130 gy , figure 2 )  . 
 urethra the maximum dose at the urethra ( d1 ) reached a median of 181 ( 94320 ) and 239 ( 152362 ) gy for lowand high - activity table 1 . 
the dose - volume histograms of 71 patients with treatment plans using both lowand high - activity seeds demonstrate a superiority of high - activity seeds considering the prostate dose values in the iatp with a commercially available 3 - d planning software ( variseed )  . 
while with iatp using high - activity seeds this dose recommendation could be achieved in nearly all patients , nearly 50% of patients were below this therapeutic dose level when low - activity seeds were used . 
taking into account that due to different reasons , including the users experience , the implant positions cannot be reached ideally [ 8 ] , even more patients would have an ineffective dose - volume prescription . 
after individual dose - volume optimization , the lowest d90 value was 164 gy in all of the 142 plans , and the prostate dose coverage was adequate for lowand high - activity seeds . 
based on these results , the american brachytherapy society recommended to use the modified peripheral loading technique and to minimize the length of the urethra which will be irradiated with > 200% of the prescribed dose [ 13 ]  . 
the necessity of transurethral resection of the prostate was reported for only 1.2% of patients with an average maximum urethral dose of 133% of the prescribed dose [ 12 ]  . 
with a significantly lower number of sources and implant needles for the treatment with high - activity seeds , a shorter implantation time and a lower urinary toxicity [ 5 ] can be expected . 
 strahlentherapie und onkologie original article palliative interstitial hdr brachytherapy for recurrent rectal cancer implantation techniques and results christos kolotas1 , 3 , sandra rddiger1 , gerd strassmann2 , thomas martin1 , nikolaos tselis1 , daniel m . 
aebersold3 , dimos baltas1 , nikolaos zamboglou1 purpose : to report the methods and clinical results of ct - based interstitial high - dose - rate ( hdr ) brachytherapy procedures for the palliative treatment of recurrent rectal cancer . 
patients implanted with metallic needles were given a single fraction of 1015 gy using hdr 192ir , and those who received transperineal implants of plastic catheters were given fractionated brachytherapy , 5 gy twice daily to a total dose of 3040 gy . 
 key words : rectal cancer recurrence hdr brachytherapy palliation strahlenther onkol 2003 ; 179 : 45863 doi 10.1007 / s00066 - 003 - 0921 - 7 palliative interstitielle hdr - brachytherapie bei rektumkarzinomrezidiven . 
zwei ct - gesteuerte techniken wurden angewandt : von 40 applikationen wurden 20 als metallnadeln ber das sakrum ( transsakrale technik ) und 20 als kunststoffkatheter transperineal in die prsakrale region eingefhrt ( transperineale technik )  . 
patienten mit metallnadelimplantaten wurde eine einzeldosis von 1015 gy im highdose - rate - ( hdr - ) verfahren ( 192ir ) appliziert , whrend jene mit transperinealen kunststoffimplantaten eine fraktionierte brachytherapie erhielten ( zweimal tglich 5 gy bis zu einer gesamtdosis von 3040 gy )  . 
das mediane tumorvolumen betrug 225 cm3 ( 412103 cm3 )  . ergebnisse : nach einer medianen nachbeobachtungszeit von 23 , 4 monaten waren 13 von 38 patienten noch am leben . 
6 / 38 1 department of radiation oncology , offenbach hospital , offenbach , germany , 2 department of radiotherapy , university hospital , philipps university , marburg , germany , 3 department of radio - oncology , university of bern , inselspital , bern , switzerland . 
 schlsselwrter : rektumkarzinomrezidiv hdr - brachytherapie palliative behandlung introduction local recurrence after curative surgery for rectal cancer occurs in 530% depending on the surgical technique , dukes histopathologic classification , and adjuvant treatment [ 1 , 2 , 5 , 15 , 17 ]  . 
radiotherapy is considered a standard palliative procedure for recurrent rectal cancer [ 3 , 12 , 20 , 22 ] , but reirradiation of this area in pretreated patients proves difficult as the tolerance of the surrounding tissue is limited . 
5 - fluorouracil ( 5 - fu ) is regarded as an active agent in the treatment of rectal cancer , but systemic chemotherapy with 5 - fu , either as a single agent or combined with other drugs , is often not beneficial in local recurrences after surgery and adjuvant radiochemotherapy . 
only in very few selected cases , such as anastomotic limited recurrences or after early detection of locally recurrent tumors involving the anterior pelvic structures , ( prostate , base of bladder , vagina , uterus ) , a curative resection using pelvic exenteration may be possible . 
 this paper describes a study of 38 patients treated with palliative intent between 19941998 at the department of radiation oncology offenbach , germany , by interstitial highdose - rate ( hdr ) brachytherapy alone for recurrent rectal cancer . 
at the time of brachytherapy , all patients had a presacral tumor mass , 28 / 38 patients also showed infiltration of the sacral bone , and 20 were presenting with distant metastases at the time of brachytherapy . 
in four patients , the placement of the catheters was performed intraoperatively and in 34 patients , 40 implants were done under ct guidance ( see table 1 )  . 
however , with four patients tumor resection was found to be impossible after the abdomen had been opened , and the only procedure possible was the implantation of plastic catheters . 
ct - guided insertion of interstitial radiotherapy catheters was performed in the ct suite using interactive ct scanning under local anesthesia ( 3050 ml lidocaine 0.5% ) and sedation ( pethidin 30100 mg , midazolam 25 mg )  . 
 brachytherapy planning at the end of the implantation , a sequence of ct slices is made with a slice thickness of 0.20.4 cm and table movements of 0.20.5 cm which are required for ct - based brachytherapy treatment planning [ 10 ]  . 
 we use the anatomic information available on the ct scans to optimize the three - dimensional ( 3 - d ) dose distribution in order to achieve a uniform dose value on the surface of the ptv . 
 there was no mortality associated with the treatment , and morbidity was limited : one patient previously treated by a hartmann procedure developed a fistula , and one patient with ulceration of the perineal area due to tumor prior to brachytherapy later developed an abscess . 
 symptomatic relief of pain was observed in 34 / 38 patients ( 89.5% ) , with 8 / 38 experiencing complete pain relief . reduction of analgesics required for control of pain was achieved in 25 / 38 . 
 implantation number of technique implantations volume ( cm3 ) mean tumor dose ( gy ) mean number ptv coverage of catheters intraoperative transsacral transperineal 352 ( 282632 ) 309 ( 951 , 029 ) 336 ( 412 , 103 ) 15.8 ( 1020 ) 10.4 ( 1015 ) 33.3 ( 1540 ) 7.7 ( 415 ) 12.4 ( 334 ) 7.7 ( 323 ) 82 ( 7886 ) 87.8 ( 8491 ) 88.5 ( 8493 ) strahlenther onkol 2003 no . 
brachytherapy for recurrent rectal cancer discussion the management of patients with pelvic recurrence of rectal cancer remains a major oncologic probleit depends on several factors such as the location and extent of the tumor , the primary surgical technique , and whether adjuvant or preoperative irradiation [ 15 ] was previously given . 
 in cases of an isolated local recurrence without any detectable distant metastasis , radiotherapy and / or surgery have a value in terms of improved overall and symptom - free survival . 
 [ 21 ] reported long - term survival rate of 33% in 47 patients who underwent abdominal sacral resections , but this is still a substantial operation with a mortality of approximately 8% and with major postoperative morbidity in most of the patients . 
despite the fact that 53% of our patients had distant metastases at the time of brachytherapy , they could not benefit from such radical surgery as described by wanebo et al . , because only one had received an anterior resection and 28 showed sacral infiltration . intraoperative radiotherapy ( iort ) in combination with surgery for treatment of a recurrence is a therapeutic option and shows encouraging results in patients with negative resection margins [ 4 , 7 , 18 ]  . 
 the therapeutic options for preirradiated patients with unresectable recurrent tumors of the sacral area are limited . there are few reports concerning the reirradiation of the pelvis for recurrent rectal cancer [ 11 , 16 ]  . 
they treated 30 patients with temporary or permanent implants of 192ir or 125i seeds in association with radical or debulking surgical resection and achieved local control rates of 66% for microscopic residual disease and 37.5% for gross residual disease . 
although interstitial brachytherapy is used in many institutes for different tumor sites , ct - guided implantation of catheters in the pelvis for the treatment of recurrent rectal cancer has not been previously reported in the literature . 
differences in results ( pain relief , tumor response ) were not found between our two methods where patients were treated with a single fraction of 1015 gy or with 3040 gy of fractionated brachytherapy ( 5 gy twice daily )  . 
the major symptom of patients with transsacral implants was pain due to osteolysis of the sacral bone , and it is well known with external radiotherapy that a single dose of 8 gy is effective for the palliation of a bone metastasis . 
the catheters used for the transperineal implantation should not be implanted in a parallel way , because such a configuration may injure critical structures including the bladder and small intestine . 
brachytherapy for recurrent rectal cancer strahlentherapie und onkologie originalarbeit frhe und spte effekte lokaler hochdosisstrahlentherapie des gehirns auf gedchtnis und aufmerksamkeitsfunktionen * susanne duchstein1 , gnther gademann1 , brigitte peters2 hintergrund : die stereotaktische strahlentherapie benigner tumoren der schdelbasis zeigt exzellente tumorkontrollraten und lange berlebenszeiten . 
 patienten und methoden : 21 patienten ( alter 42 11 jahre ) mit tumoren an der schdelbasis ( meningeome , hypophysenadenome ) wurden mit einer fraktionierten stereotaktischen strahlentherapie ( mittelwert 56 , 6 / 1 , 8 gy ) behandelt . 
 schlussfolgerung : die bestrahlung mit hohen lokalen dosen der zielvolumina in unmittelbarer nhe zu sensiblen hirnstrukturen wie den temporallappen fhrt bei patienten mit tumoren der hirnanhanggewebe zu keiner signifikanten verschlechterung der kognitiven funktionen . 
 schlsselwrter : hochdosisstrahlentherapie gutartige hirntumoren neuropsychologie strahlenther onkol 2003 ; 179 : 44151 doi 10.1007 / s00066 - 003 - 1034 - z early and late effects of local high dose radiotherapy of the brain on memory and attention * background : stereotactic radiotherapy of benign tumors of the base of skull shows excellent tumor control and long survival . aim is to study the impact of high dose radiation therapy on functions of memory and attention over time . 
 patients and methods : 21 patients ( age 42 11 years ) with tumors of the base of skull ( meningiomas , pituitary gland adenomas ) were treated by fractionated stereotactic radiotherapy ( mean total dose 56 , 6 gy / 1 , 8 gy )  . 
 results : in pretreatment tests there were significantly worse test results in comparison to the control group in ten of 32 tests . in postradiation tests only few changes were found in the early - delayed period and not much difference was seen in comparison to the baseline tests . 
in einer vielzahl von studien wurde ber neuropsychologische spteffekte berichtet , die mit der zns - prophylaxe bei kindern , die an akuter lymphoblastischer leukmie ( all ) erkrankt sind , aber auch mit der bestrahlung von hirntumoren in verbindung stehen . 
die dosis - wirkungs - beziehung fhrte zu einer nicht linearen verschlechterung fr alle altersgruppen mit strkerer schdigung bei hheren dosen . teilhirnbestrahlungen waren bei gleichen dosen weniger schdigend als ganzhirnbestrahlung . 
in einer sptuntersuchung [ 39 ] bezglich der therapie mit und ohne kranielle bestrahlung erreichten langzeitberlebende von all in einem medianen follow - up von 10 jahren signifikant schlechtere resultate in untertests des wechsler - intelligenztests . 
das zeitverzgerte auftreten kognitiver defizite nach kranieller bestrahlung legt nahe , dass wahrscheinlich eine interaktion zwischen dieser und entwicklungsprozessen im arbeitsgedchtnis und der verarbeitungsgeschwindigkeit des kindlichen gehirns fr das auftreten der defizite verantwortlich ist [ 33 ]  . 
 [ 9 ] kritisierten , dass sensitive neuropsychologische messinstrumente in den meisten untersuchungen zu den auswirkungen von hirnbestrahlungen nicht angewendet wurden . die alleinige erhebung des iq im erwachsenenalter ist unzureichend , da hier eher geringe vernderungen zu erwarten sind . 
in einzelnen bereichen fand man auch eine verbesserung der hirnfunktionen bei patienten mit kognitiven strungen nach bestrahlung durch hyperbare oxygenierung [ 18 ]  . die neurokognitiven auswirkungen kranieller bestrahlungen niedriggradiger primrer hirntumoren wurden von armstrong et al . 
die patienten hatten vor der bestrahlung ein normales verbales gedchtnis . es kam dann aber zu einer verschlechterung , die von einer phase der erholung im verbalen erinnern abgelst wurde . das visuelle gedchtnis war durch ein defizit zum zeitpunkt der baseline - untersuchung und eine erholung bis zu 1 jahr nach bestrahlung charakterisiert . 
 in einer prospektiven studie bei 17 jungen erwachsenen mit bestrahlung supratentorialer gliome fand sich eine vorbergehende verschlechterung in den reaktionszeiten nach 6 monaten , die nach 12 monaten auf das niveau der basisuntersuchung zurckging . 
gedchtnis und kognitive funktionen blieben bis 5 jahre nach der behandlung auch bei denjenigen patienten stabil , die bestrahlungsdosen bis 66 gy durch gesundes hirngewebe ( temporallappen ) erhielten . eine leichte verschlechterung der psychomotorischen geschwindigkeit wurde in etwa der hlfte der patienten gefunstrahlenther onkol 2003 no . 
 alter [ jahre ] geschlecht hndigkeit tumorart die bisherigen ergebnisse sprechen also fr mgliche , wenn auch geringe kognitive beeintrchtigungen nach teilhirnbestrahlungen im erwachsenenalter , die eine relativ hohe toleranzschwelle kortikaler hirnstrukturen erwarten lassen . 
fr patienten mit tumoren in und an der hirnregion ist es fr ihre zuknftige lebensqualitt uerst bedeutungsvoll zu wissen , welche kognitiven auswirkungen die strahlentherapie sowohlin der unmittelbaren phase als auch in der sptphase nach der therapie habenkann . 
 zielvolumen [ cm3 ] dosis [ gy ] * variationsbreite patienten und methoden an dieser prospektiven studie nahmen patienten mit histologisch nachgewiesenen tumoren der hirnanhanggewebe mit sitz an der schdelbasis und im sellabereich teil . 
diese tumoren sind besonders geeignet , schdigungen durch die bestrahlung zu evaluieren , da sie verdrngend wachsen , lngere rezidivfreie intervalle als andere aggressive hirntumoren haben und eine hochdosisstrahlentherapie im zielvolumen zur lokalen tumorkontrolle erhalten knnen . 
die bestrahlung kann in der 3 - d - planung so optimiert werden , dass durch die konzentrierte dosisverteilung auf das zielvolumen das gesunde hirngewebe maximal geschont wird [ 15 ]  . 
patients and controls : demographics , tumor characteristics and therapy . patienten kontrollgruppe signifikanz 42 11 2059 * 17 w / 4 m 96% rechtshnder 100 % rechtshnder 39 11 2061 * 12 w / 2 m f ( 1 , 33 ) = 0 , 823 , p = 0 , 371 n.s. meningeom rechts / links parasellr meningeom temperookzipital hypophysenadenom chordom esthesioneuroblastom glomustumor links kraniopharyngeom 38 , 96 ( 12133 ) * 56 , 56 ( 50 , 468 , 4 ) * darauf geachtet , dass bei nicht mittiger lage des tumors die gegenseite des gehirns nicht von der dosisverteilung erfasst wurde . 
die einzeldosen von 1 , 82 , 0 gy wurden fnfmal wchentlich verabreicht , sodass die strahlentherapie einen zeitraum von 67 wochen in anspruch nahtumorart und - lokalisation als einschlusskriterien fr diese untersuchung erlaubten nur ein eingeschrnktes patientenkollektiv . 
tumorbiopsie oder resektion wurden zwischen 2 und 48 monate vor behandlungsbeginn durchgefhrt . kontrollgruppe die personen in der kontrollgruppe unterzogen sich der neuropsychologischen untersuchung zum zeitpunkt der basisuntersuchung , um initiale defizite der patienten zu erheben . 
die daten der ersten nachuntersuchung wurden bei den patienten 3 monate und die daten fr die zweite nachuntersuchung 9 monate nach der beendigung der strahlentherapie zur erfassung mglicher frher effekte erhoben . 
 im kontrollierten wort - assoziationstest zur wortflssigkeit werden exekutive funktionen geprin drei durchgngen sollen so viele worte wie mglich in einer zeiteinheit von 1 minute mit unterschiedlichen anfangsbuchstaben benannt werden . 
 beim finger tapping test werden innerhalb von 10 sekunden so viele anschlge wie mglich auf eine taste mit dem zeigefinger jeder hand gemacht , um die psychomotorische geschwindigkeit zu prfen [ 21 ]  . die zahlenspanne ist der wechsler memory scale - revised ( wms - r ) entnommen und dient der erfassung des sprachlichen kurzzeitgedchtnisses [ 40 ]  . 
in beiden testformen werden der unmittelbare abruf und der verzgerte abruf geprft . mithilfe ausgewhlter verfahren der testbatterie zur aufmerksamkeitsprfung von zimmermann & fimm [ 3 , 43 ] sollen mgliche vernderungen in verschieden aspekten der aufmerksamkeit geprft werden . 
 allen tests geht eine kurze bungsphase voran , um das aufgabenverstndnis und die praxis der patienten zu prfen . der untertest alertness prft die phasische alertness , also die fhigkeit , in erwartung eines reizes hoher prioritt ( aufleuchten eines kreuzes auf dem bildschirm mit und ohne warnton ) das niveau der aufmerksamkeit zu steigern und aufrechtzuerhalten . 
 im untertest geteilte aufmerksamkeit wird mithilfe einer dual - task - aufgabe , in der gleichzeitig ein visueller und ein akustischer reiz beachtet werden sollen , die fhigkeit geprft , die aufmerksamkeit gleichzeitig auf mehrere reize zu richten . 
 der untertest inkompatibilitt soll die interferenzneigung durch eine reiz - reaktions - inkompatibilitt prfen . hierbei soll auf die richtung einer pfeilspitze reagiert werden , unabhngig von ihrem reprsentationsort links oder rechts von einem fixationspunkt . 
effekte lokaler hochdosisstrahlentherapie des gehirns die daten liegen als rohwerte aus der zahl der erreichten werte bis zu einem abbruchkriterium , als absolute anzahl der fehler oder auslassungen und in der gemessenen zeit in ms bei den aufmerksamkeitsprfungen vor . 
 das beck depressions inventar ( bdi ) [ 17 ] unterscheidet zwischen depressiven und nichtdepressiven und bestimmt die subjektive schwere einer depression , wobei zu 21 gruppen von aussagen jeweils die zutreffende angekreuzt werden soll . 
 in der symptomcheckliste scl 90 - r hatten die patienten in der globalen skala pst ( positive symptom total ) signifikant mehr symptome als belastend beurteilt ( f [ 1 , 33 ] = 5 , 19 , p = 0 , 029 ) sowie in der skala psychotizismus ( f [ 1 , 33 ] = 7 , 50 , p = 0 , 010 )  . 
in der ewl beschrieben sich die patienten signifikant weniger aktiviert ( skala aktiviertheit f [ 1 , 28 ] = 4 , 24 , p = 0 , 049 ) und selbstsicher ( skala selbstsicherheit f [ 1 , 28 ] = 8 , 37 , p = 0 , 007 )  . 
 mittels scorebildung wurden patientenund kontrollgruppe gegeneinander multivariat geprft , um eine gesamtaussage bezglich eines gruppenunterschiedes in den neuropsychologischen und den psychopathologischen variablen zu erhalten . die patienten unterschieden sich als gruppe vor der bestrahlung von den kontrollen ( f [ 1 , 23 ] = 4 , 24 , p = 0 , 051 )  . 
 nachsorgeuntersuchungen alle bisher in der nachsorge befindlichen patienten bis zum zeitpunkt 21 monate nach der hochdosisstrahlentherapie sind nach der mrt , die jeweils zu den entsprechenden terminen durchgefhrt wurde , frei von tumorprogressen oder sichtbaren strahlentherapeutisch induzierten vernderungen wie atrophien oder vernderungen der subkortikalen weien hirnmasse im gesunden gewebe . 
effekte lokaler hochdosisstrahlentherapie des gehirns frhe vernderungen nach 3 und 9 monaten die tabellen 3 und 4 geben eine bersicht ber die mittelwerte und standardabweichungen der punktwerte in den neuropsychologischen verfahren aller teilnehmenden patienten . 
hier erwiesen sich im mittelwertsvergleich nur wenige der variablen als signifikant verndert : in der berprfung der gedchtnisfunktionen nach 3 monaten verschlechterten sich die patienten nicht signifikant ( ausnahme : test zur zahlenspanne rckwrts ) , obwohl schwankungen in einzelnen verfahren zu beobachten waren . 
in den untertests der testbatterie zur aufmerksamkeitsprfung wurden in der frhen phase nach strahlentherapie nur sehr wenige signifikante vernderungen in der analyse des zeitlichen verlaufs innerhalb der gleichen patientengruppe festgestellt ( tabelle 4 )  . 
nach 3 und 9 monaten war die reaktionszeit fr quadrate im untertest geteilte aufmerksamkeit verlngert ( f [ 1 , 13 ] = 8 , 718 , p = 0 , 011 ) bzw . 
nur im untertest reaktionswechsel war nach 9 monaten eine tendenz zur verbesserung in den im vergleich zum reaktionszeiten zeitpunkt der basisuntersuchung vorhanden ( f [ 1 , 11 ] = 3 , 721 , p = 0 , 080 )  . 
 in der erfassung belastender symptome mit der symptomcheckliste scl 90 - r zeigte lediglich die skala ngstlichkeit eine signifikante abnahme der belastung nach 9 monaten ( f [ 1 , 15 ] = 5 , 070 , p = 0 , 040 )  . 
mittelwerte der reaktionszeiten fr die untertests alertness ohne warnton , go / nogo und reaktionswechsel in der kontrollgruppe ( basisuntersuchung ) und den patienten ( basisuntersuchung , 3 und 21 monate nach strahlentherapie )  . 
means of reaction times in alertness without warning tone , go / nogo , and reaction change in the control group ( at baseline ) and in the patients ( at baseline , 3 and 21 months follow - up )  . 
im bdi senkte sich das niveau der erlebten subjektiven schwere depressiver symptome erst nach 9 monaten ( f [ 1 , 15 ] = 6 , 902 , p = 0 , 019 ) signifikant . 
in der spten phase nach strahlentherapie wurden nur diejenigen patienten in die statistische analyse der vernderung bezglich der basisuntersuchung einbezogen , die auch zu den anderen untersuchungszeitpunkten in die statistische auswertung des verlaufs einbezogen waren . 
 in der wortflssigkeit erreichten die patienten im graphematischen kriterium eine signifikant grere menge an produzierten wrtern als in der basisuntersuchung ( f [ 1 , 14 ] = 10 , 280 , p = 0 , 006 ) ( abbildung 2 )  . 
 im recurring figures test war nach 21 monaten eine signifikante verbesserung ( f [ 1 , 14 ] = 4 , 614 , p = 0 , 500 ) in den rohwerten zu verzeichnen . im paarassoziationslernen waren nur visuell weniger lerndurchgnge ( f [ 1 , 12 ] = 37 , 463 , p = 0 , 0001 ) gegenber der ausgangsuntersuchung notwendig . 
 die mittleren reaktionszeiten , fehler und / oder auslassungen in den durchgefhrten untertests der testbatterie zur aufmerksamkeitsprfung waren im vergleich zu den ausgangswerten nur sehr gering verndert ( abbildung 1 ) , sodass keine signifikanzen fr die erreichten werte der untersuchten patientengruppe vorhanden waren ( tabelle 4 )  . 
im bdi senkte sich das niveau der subjektiv erlebten depressiven symptome ( f [ 1 , 15 ] = 4 , 342 , p = 0 , 055 ) im vergleich zum prtherapeutischen erleben . 
21 monate nach therapie nannten die patienten signifikant mehr worte ( f [ 1 , 14 ] = 11 , 267 , p = 0 , 006 ) und verbesserten damit ihre leistung . 
patients named statistically significant more words on 21 - months postradiation test ( f [ 1 , 14 ] = 11 , 267 , p = 0.006 ) and improved their test performance . 
die groe zahl an einzelvariablen ber die testzeitpunkte hinweg wurde multivariat mittels scorebildung geprft , indem diese zu gruppen zusammengefasst wurden , die jeweils ein gedchtnismerkmal reprsentieren [ 18 ]  . 
die datenlage [ 1 , 9 , 13 , 37 ] zeigt , dass eine schdigung gesunden hirngewebes im bereich der temporalund frontallappen fr die zuknftige lebensqualitt dieser patienten von bedeutung ist . 
bei diesen tumoren im bereich des sinus cavernosus , die schwer zu operieren sind oder nur eine subtotale resektion erlauben , bietet die fraktionierte strahlentherapie lange rezidivfreie intervalle und nur minimale therapiebezogene nebenwirkungen an [ 23 ]  . 
die externe lokale strahlentherapie bei meningeomen und hypophysenadenomen wird gut toleriert und gilt als effektive behandlungsmethode [ 2 , 4 , 10 , 24 , 25 , 31 ]  . 
 es gibt nur wenige prospektive untersuchungen meist aber an patienten mit malignen hirntumoren , die aufmerksamkeitsprozesse bercksichtigen und die messung von reaktionszeiten einbeziehen [ 5 , 22 , 38 ]  . 
deshalb wurde auf die gleichheit der gruppe in der analyse des zeitverlaufs starker wert gelegt . die patienten dienten als ihre eigene kontrollgruppe [ 13 ]  . somit kann auch ausgeschlossen werden , dass eine positive selektion der patienten die ergebnisse beeinflusst . 
 das angewandte verfahren der repeated - measurementanalyse erlaubt keinen rckschluss auf einzelne variablen , die hinter den faktoren stehen , gibt aber die mglichkeit , die richtung der vernderung in einer groen variablenmenge , gemessen an einer kleinen stichprobe , zu verdeutlichen . 
in der vorliegenden patientengruppe vernderten sich die gemessenen psychologischen parameter zu aufmerksamkeitsund gedchtnisfunktionen im zeitverlauf nicht wesentlich , sodass nach stereotaktischer strahlentherapie keine weiteren beeintrchtigungen in den kognitiven leistungen auftraten . die steigerung der leistung in einigen tests knnte ein lerneffekt semglich ist auch die verringerung des stressors erkrankung als eine einflussgre , die mit abnehmender schwere subjektiven belastungserlebens einhergeht . 
effekte lokaler hochdosisstrahlentherapie des gehirns rapie im arbeitsleben standen , konnten neun in den arbeitsprozess zurckkehren , drei wurden eu - rentner ( mit einer lngeren krankheitsgeschichte vor der bestrahlung ) , von denen zwei einer kleinen teilzeitbeschftigung nachgehen ( 21 monate nach bestrahlung )  . 
 dosen auf ein kleines volumen im zns , aber auch die applikation von strahlen in der radiochirurgischen behandlung arteriovenser malformationen keine akuten oder chronischen vernderungen der neuropsychologischen funktionen verursachen [ 41 , 42 ]  . 
hinzu kommt ein krankheitsverarbeitungsund anpassungsprozess der patienten , der individuell einer sehr groen variationsbreite unterliegt ( abbildung 3 )  . schlussfolgerungen die ergebnisse dieser studie zeigen , dass mit der stereotaktischen bestrahlung von tumoren der hirnanhanggewebe bei patienten im alter von 2060 jahren eine von negativen auswirkungen auf aufmerksamkeitsund gedchtnisprozesse weitgehend freie behandlungsmethode vorliegt , die gleichzeitig sehr gute klinische ergebnisse aufweist [ 10 ]  . 
alle kognitiven gefhrdungen , die in frheren untersuchungen ber teilhirnbestrahlungen beschrieben worden sind [ 9 , 14 , 37 ] , treffen fr die fraktionierte stereotaktische konformationsstrahlentherapie innerhalb des bisher untersuchten zeitraumes fr unser patientenkollektiv nicht zu . 
susanne duchstein universittsklinik fr strahlentherapie leipziger strae 44 39120 magdeburg deutschland telefon ( + 49 / 391 ) 67 - 132 76 , fax - 153 24 strahlenther onkol 2003 no . 
7 urban & vogel strahlentherapie und onkologie original article high - dose - rate intraoperative brachytherapy ( iohdr ) using flab technique in the treatment of soft tissue sarcomas franz rachbauer1 , arpad sztankay2 , alfons kreczy3 , tarek sununu1 , christian bach1 , michael nogler1 , martin krismer1 , paul eichberger2 , bernhard schiestl2 , peter lukas2 background : adjuvant radiotherapy has been shown to improve local control in patients with soft tissue sarcoma . 
high - dose - rate intraoperative brachytherapy ( iohdr ) as a boost therapy should therefore be able to further diminish the rate of local recurrence even when performing marginal resection . 
there are sparse data on iohdr using flab applicators as adjuvant boost to ebrt in combination with marginal resection of soft tissue sarcomas . patients and methods : within a period of 8 years , we prospectively studied 39 adult patients treated by marginal resection , iohdr using the flab technique and ebrt for soft tissue sarcomas . 
there were 32 high - grade and seven low - grade tumors , 35 were > 5 cmean follow - up was 26 months ( range 359 months )  . results : we could not detect any local recurrences . 
the 2 - year actuarial disease - free survival was 84% . conclusions : iohdr using the flab technique in combination with ebrt and marginal resection is an efficient treatment technique leading to optimal local control rates and limited functional impairment . key words : soft tissue sarcoma intraoperative high - dose - rate brachytherapy limb salvage surgery radiotherapy local recurrence strahlenther onkol 2003 ; 179 : 4805 doi 10.1007 / s00066 - 003 - 1063 - 7 intraoperative hochdosisbrachytherapie ( iohdr ) mittels flab - technik in der behandlung von weichteilsarkomen hintergrund : die adjuvante perkutane strahlentherapie hat unter beweis gestellt , dass sie die lokale kontrolle von weichteilsarkomen verbessern kann . 
die intraoperative hochdosisbrachytherapie ( iohdr ) als boost - therapie sollte daher in der lage sein , die lokalrezidivrate weiter zu senken , selbst wenn der tumor nur marginal reseziert wird . 
bis jetzt gibt es nur sehr wenige daten ber die iohdr unter verwendung von flabapplikatoren und marginaler resektion von weichteilsarkomen . patienten und methodik : innerhalb einer zeitspanne von 8 jahren haben wir prospektiv den verlauf von 39 erwachsenen patienten verfolgt , die wegen eines weichteilsarkoms mit marginaler tumorresektion , iohdr unter verwendung von flab - applikatoren und perkutaner strahlentherapie behandelt wurden . 
es traten keine nervenoder gefkomplikationen auf , bei allen patienten konnten funktionstchtige extremitten erhalten werden , was sich in einem mittleren musculoskeletal - tumor - society - ( msts - ) funktionswert von 88 , 5 ( 70100 ) zeigte . wundheilungsstrungen stellten sich bei elf patienten ein , die aber nur in acht fllen chirurgisch versorgt werden mussten . 
 1 department of orthopedics , 2 department of radiotherapy - radiooncology , and 3 institute of pathologic anatomy , university of innsbruck , austria . received : june 17 , 2002 ; accepted : january 17 , 2003 strahlenther onkol 2003 no . 
intraoperative brachytherapy for soft tissue sarcoma schlussfolgerungen : die iohdr in verbindung mit perkutaner strahlentherapie und marginaler tumorresektion stellt eine effektive behandlungstechnik dar , die den tumor lokal optimal kontrolliert und die extremittenfunktion nur geringfgig einschrnkt . schlsselwrter : weichteilsarkome intraoperative hochdosisbrachytherapie extremittenerhaltende chirurgie strahlentherapie lokalrezidiv introduction one of the major clinical problems in the treatment of soft tissue sarcomas is the propensity of the primary tumor to recur locally [ 7 ]  . 
 surgical excision has been the mainstay of treatment [ 23 ] , and radical procedures such as amputation came to be accepted as standard surgical therapy [ 7 ]  . 
adjuvant external beam irradiation ( ebrt ) has been shown to improve local control in patients with soft tissue sarcoma [ 3 ] allowing limb - sparing approaches to extremity sarcomas [ 33 ]  . 
 brachytherapy options include low dose - rate techniques , fractionated high - dose rate - brachytherapy , or intraoperative high - dose - rate therapy ( iohdr ) [ 21 ]  . 
 we hypothesized that the combination of iohdr , in special using the flab technique , ebrt and limb - sparing surgery by marginal resection , should lead to a low risk of local recurrence and morbidity . 
 three patients who underwent ablative surgery , two patients with intralesional resection and gross tumor remnants as well as five patients with superficial low - grade sarcomas were excluded from study . 
 29 tumors arose in the lower extremity , six in the upper extremity , two tumors were located retroperitoneally , one in the trunk , and one in the neck . 
 preoperative staging studies consisted in local magnetic resonance tomography , computed tomography of the whole trunk ( thorax , abdomen , and pelvis ) , complete blood count , and serum chemistry analysis . 
the staging systems of the musculoskeletal tumor society ( msts ) and the american joint committee on cancer ( ajcc ) were applied and compared to tnm staging system of the international union against cancer ( uicc ) ( tables 2 and 3 )  . the sequence of treatment was surgery and iohdr followed by ebrt . 
histologische klassifikation nach der herkunft der entarteten bindegewebszelle . cellular classification n = 39 liposarcoma malignant fibrous histiocytoma leiomyosarcoma malignant peripheral nerve sheath tumor rhabdomyosarcoma synovial sarcoma extraskeletal chondrosarcoma malignant schwannoma strahlenther onkol 2003 no . 
staging and grading ( tngm ) according to the american joint committee on cancer ( ajcc ) [ 11 ] with reference to tnm staging system [ 31 ]  . 
then , the applicator was secured with gauze packing or by temporary closure of the wound through large stitches in order to avoid displacement and to ensure a continuous contact between surface of the applicator and tumor bed . 
the dose of the intraoperative brachytherapy generally was 15 gy prescribed to the surface of the applicator flabs which corresponds to a dose of 10 gy prescribed at 0.5 cm depth within tissue . 
when the applicator was close to a major neurovascular bundle , the dose in the overlying hollow catheters was selectively reduced to a surface dose of 12 gy [ 1618 ]  . 
radiation therapy was delivered with megavolt beams using linear accelerators ( elekta sli , elekta precise , elekta oncology systems ltd . , crawley , west sussex , uk )  . external beam radiation was delivered to a total dose of 50 gy ( given as 2 gy per fraction ) in 5 weeks encompassing the surgical bed with a margin of 57 cneither entire muscle compartments nor the entire circumference of the extremities were generally irradiated , the joints were spared when possible . 
intraoperative brachytherapy for soft tissue sarcoma examination , ct scan of the body trunk ( chest and bowel ) , and magnet resonance imaging of the part of the body , which had undergone surgery . 
none of the patients was lost to follow - up . the patients status at most recent follow - up was assessed ; in the case of death , the local status of the last followup was used . 
 metastatic disease ( lung , liver , brain , muscles , subcutaneous fat ) developed in seven out of 38 patients ( 17.9% ) arising in each case in multiple foci . 
all seven patients had had primary lesions > 5 cgrading at initial diagnosis had been high - grade in six out of the doxorubicin - based adjuvant chemotherapy had been given to six out of these cases . 
 31 of 39 patients were alive , six patients had died of metastatic disease , and one patient had died of a cardiovascular incident with no evidence of disease at the time of death . the 2 - year actuarial disease - free survival was 84% ( figure 3 ) ; the overall survival was 81.9%. 
when tumor location was in the extremities ( n = 34 patients ) , the mean functional score as rated by the clinician on the msts was 88.5 ( range 70100 )  . 
there was no functional impairment when the tumor was located at the neck and at the trunk ( n = 2 patients )  . the two patients with retroperitoneal tumors had a diminished strength of bending the hip when compared to the other side due to resection of psoas muscle . 
 in two patients , inadvertent opening of the capsule and potential tumor spillage occurred during surgery , which had no impact whether on overall survival nor on local recurrence . there was neither treatment - related loss of limb or life , nor were neurologic or vascular complications . 
 when comparing radical amputation to wide local excision plus postoperative radiation , the merit of limb - sparing approaches to extremity sarcomas has been proven [ 7 , 25 , 29 , 34 ]  . 
 marginal excision plus radiotherapy and wide local excision have shown to have almost the same cumulative local control rate , whereas marginal excision alone led to a significantly lower local control rate [ 4 ]  . 
a combined therapy using brachytherapy , conservative resection , and ebrt showed no increased local morbidity and led to enhanced local tumor control in comparison to either external radiation or brachytherapy alone as an adjuvant to conservative resection [ 26 ]  . 
there are sparse data on the use of iohdr for soft tissue sarcomas [ 21 ]  . this led us to prospectively assess the effect of a combined treatment with brachytherapy using the flab technique as a local boost , marginal resection , and ebrt . 
we wanted to know whether this special application mode of brachytherapy is able to prevent local recurrence , whether there is substantial treatment - associated morbidity , and whether limb sparing can be achieved resulting in a functioning extremity . 
 [ 26 ] , the expected advantages of intraoperative irradiation are enhanced radiobiological effectiveness due to high single dose , high cumulative radiation dose in the immediate tumor bed , relative sparing of overlying skin and surrounding normal tissues , and direct visualization of tumor bed being able to localize the highest dose of radiation to the region at greatest risk of microscopic disease . whether there is an impact of timing of radiotherapy on local recurrence remains to be elucidated [ 27 ]  . 
 the munich flab is an intraoperative high - dose - rate applicator like the harrison - mick and the freiburg flab that are mainly used in the treatment of colorectal cancer [ 14 ]  . 
nevertheless , care has to be taken to have continuous contact between the applicator flab and the tumor bed through meticulously packing of the wound with sterile gauze . the chosen radiation source with its relatively sharp dose decline allows a boost radiation to the area immediately surrounding the tumor . 
tumors of the retroperitoneum , if they cannot be resected without leaving tumor behind , should undergo intraoperative radiation therapy by electron beams [ 16 ]  . we had no local recurrence , which is better than reported in literature . 
the majority of all lesions that are destined to recur locally will do so within 2 years following surgery [ 6 , 30 ]  . when excluding patients with a follow - up of < 24 months , there are 24 patients le treatment - related morbidity was mainly due to remaining dead space occurring following extensive resection , which led us to deliberately fill the gaps using local transposition flaps as well as free flaps if necessary . 
with the exception of two tumors that arose in the nerve sheath , we could preserve the major nerves even in close proximity to the tumor . the major nerves and vessels had to be shelled out in some cases and received a surface dose of 12 gy in the first cases and than later on 15 gy . 
as we had no such complications as well as considering experiences by others , we have switched to generally 15 gy surface doses . nevertheless , a final conclusion on late morbidity cannot be drawn due to the intermediate - term follow - up [ 28 ]  . 
 all patients with tumors of the lower extremity can walk without crutches ; there were no limitations of hand function . substantial postradiation edema and fibrosis limiting motion occurred mainly in big tumors and large fields of ebrt . 
 our observations are in accordance with the literature . the treatment with doxorubicin did not influence the risk of local recurrence , and survival rate did not differ significantly in the groups , which included as well compartmental or wide amputation and compartmental local excision . 
primary hostand tumor - related prognostic factors alone may determine the risk of metastases in high - grade soft tissue sarcomas ; local recurrence per se may not influence the prognosis in these cases [ 24 ]  . 
the majority of these studies accrued small numbers of patients and did not demonstrate a metastasis - free or an overall survival benefit for adjuvant chemotherapy [ 22 ]  . 
 iohdr using the flab technique in combination with ebrt is a favorable means of safely providing adjuvant local treatment after marginal resection for soft tissue sarcomas . brachytherapy allows delivery of a boost dose in a reduced volume of tissue , precisely mapped by the intraoperative procedure . 
 strahlentherapie und onkologie review article ethical aspects of patient information in radiation oncology an introduction and a review of the literature christof schfer , manfred herbst1 background : while legal aspects of patient information in radiotherapy are often discussed in clinical literature , ethical aspects are mainly a topic of debate only in bioethical literature . 
 methods : the basis of this project was a medline search ( 19902002 ) using the key words radiotherapy and patient information for the first part , and radiotherapy and ethics for the second part . 
under ethical aspects ( n = 26 papers ) , palliative radiotherapy confronts the physician with many unsolved problems concerning telling the truth and the patients misunderstandings which are often observed . 
for each of these , a definition is provided , as well as a detailed discussion of various typical situations in radiation oncology such as adjuvant therapy or palliative treatment . 
 conclusion : considerations regarding the ethical aspects of patient information can provide an impulse to clinical improvement . therefore , research in this field should be intensified in the future , especially in the area of palliative radiotherapy . 
 key words : patient information radiotherapy truth autonomy ( informed ) consent hope palliative radiotherapy research medical ethics bioethics disease death doctor - patient relationship strahlenther onkol 2003 ; 179 : 43140 doi 10.1007 / s00066 - 003 - 1054 - 8 ethische aspekte der aufklrung in der radioonkologie . 
eine einfhrung und literaturbersicht hintergrund : whrend juristische aspekte der patientenaufklrung in der radioonkologie oft in der klinischen literatur diskutiert werden , werden entsprechende ethische aspekte hauptschlich in der bioethischen literatur errtert . 
 methodik : grundlage dieser arbeit war eine medline - recherche ( 19902002 ) unter den stichwrtern strahlentherapie und aufklrung fr den ersten teil des beitrags sowie ethik und strahlentherapie fr den zweiten teil . 
unter ethischen aspekten ( n = 26 arbeiten ) konfrontiert die palliative radiotherapie die rzte mit vielen ungelsten problemen hinsichtlich der wahrheit am krankenbett und der oft beobachteten missverstndnisse der patienten . 
 schlsselwrter : aufklrung strahlentherapie wahrheit autonomie ( informierte ) einwilligung hoffnung palliative strahlentherapie forschung ( medizinische ) ethik bioethik krankheit tod arzt - patienten - verhltnis 1 clinic and policlinic for radiotherapy , university of regensburg , germany . 
in the past , the doctor had a more paternalistic relationship with the patient who followed medical instructions as would a child , and trusted in the doctor without asking questions . 
in germany , providing information to radiotherapy patients has recently become a topic of public interest since the events in the department of radiotherapy at the university hospital in hamburg [ 7 ]  . 
society views the medical profession as providing a service , and the present doctorpatient relationship has become more like a business affair . health is seen as a commodity which society must provide for its citizens . 
therefore , patient information has to be open , complete , truthful , and the ethical aspects must be considered as well as the legal aspects . in this context , providing patient information today is a very demanding topic [ 83 , 106 ]  . 
in addition , ethical aspects and principles are examined , and , finally , advice is given on how to best provide patient information as well as how to evaluate these issues in a scientific context . 
 the practice of patient information in radiation oncology analysis of the current literature to gain insight into the day - to - day practice of providing patient information , we performed an analysis of the current clinical literature . 
 the most commonly used method was the interview ( n = 45 ) ; in one paper a symptom checklist and in one a scoring system was used , in two an informed - consent questionnaire was judged , in three audiotapes and another videotapes were analyzed , and in two computer - based systems were examined . 
all together , the informed - consent questionnaire was rated positively by the patients [ 32 ] , as well as information booklets , where even possible improvements could be made [ 4 , 48 ]  . 
for special situations , aids were developed , e.g. , for patients with breast cancer ( decision board ) [ 105 ] or for patients with locally advanced non - small - cell lung cancer [ 14 ]  . 
other aids with a positive rating were telephone - based consultations by nurses [ 1 ] , audiotapes [ 39 ] and computer - based information [ 56 ]  . 
 the topic rated second in importance ( n = 16 ) was the patient - information consultation and the information behavior . all studies showed a high need for information [ 13 , 42 , 44 , 82 ]  . this was also true for other cultures such as south africa [ 65 ]  . the patients perspective and providing continuous information seemed to be important . 
ethical aspects of patient information in radiooncology ing them was the most important source of information [ 28 ]  . normally , patients get their information from inside the health system [ 17 ]  . 
another study disclosed problems in cooperation between nurse and physician , where the nurses were not clear about their own role in the distribution of information [ 93 ]  . 
in another recent german study , only 52% of the patients who received palliative radiotherapy rated the noncurative intent of treatment correctly , whereas 86% of the patient who received curative radiotherapy made a correct statement [ 84 ]  . 
cooperation between all participating disciplines is mandatory [ 16 ]  . often , the truth is withheld from the patient [ 68 ] and , as an article from the netherlands showed , most patients did not participate in the process of decision - making [ 100 ]  . 
misconceptions regarding their illness and unrealistic expectations of palliative therapy were often noticed by a canadian group [ 19 ]  . the remaining studies ( n = 16 ) dealt with various aspects of patient information . 
therefore , documentation of potential side effects during radiotherapy e.g. , 40% of patients with cervical and corpus cancer experience side effects and the recording of physical symptoms are important and should be done according to the patients perspective [ 20 , 59 ]  . 
if computer - based information with a touch - screen system is used , more efforts should be made to provide affordable information in suitable locations for older , generally less literate and technologically less proficient groups [ 72 ]  . 
in a european study concerning patient information in clinical research , faulty behavior of doctors was often found . 12% of the patients were not informed about study participation , 38% were not informed about randomization , and one third had no written informed consent [ 107 ]  . 
 a major problem of patient information in radiation oncology is the poor knowledge of the patients about rays , radiotherapy and prejudices which are propagated by the mass media [ 40 ]  . 
the availability of material and its influence on therapeutic decision ( allocation ) is a new problepatient information about this is difficult for a doctor without special knowledge in this field and is seen negatively by social science [ 60 ]  . 
 ethical basics of patient information in providing patient information , the doctors goal is to inform the patient about his overall state of health , the character of the underlying disease , necessary diagnostic and therapeutic procedures , and the probable course of the disease . 
in the following discussion , autonomy is often a topic of ethical debate , e.g. , when the limits of autonomy are discussed in cases of restricted resources , euthanasia , or medical futility [ 45 ]  . 
at a minimum , the patient should receive information regarding ( 1 ) nature of the procedure , including whether it is diagnostic or therapeutic ; ( 2 ) risks , especially those that are severe and likely to occur ; ( 3 ) benefits of the procedure ; and ( 4 ) alternatives to the procedure , along with their risks and benefits [ 12 ]  . 
as a result , providing patient information is very challenging , and the doctor not only needs medical expertise , but also empathy . how to best provide patient information in the clinical practice of radiation oncology providing patient information is very demanding for the doctor and has to fulfill medical , legal , psychological , socioeconomic and ethical aspects . 
 patients perspective physicians perspective the patient not only needs logical , but also psychological and emotional support , as two recent publications have shown [ 10 , 49 ]  . 
the pledge of secrecy and , if the patient wishes , the right not to know must also be respected . patient information is not a single act , but rather a process taking place over a long period of time . 
most radiotherapy patients suffer from cancer , addiction aesthetics alcoholism anxiety autonomy death decision disease donation of blood dying emancipation ethics committees freedom guilt happiness helsinki declaration hope human dignity identity informed consent life lowering of suffering mind - body relationship morals norm pain participation patient patients will person privacy of personal data prolongation of life quality of life rehabilitation religion resuscitation sorrow stress suffering suicide truth welfare acting and refraining compulsory treatment conscience consequences of no treatment death benefit double - blind test disease documentation genetics guidelines health human dignity liability medical law palliative therapy person pledge of secrecy precautions predictive medicine progress quality management religion research respect for nature and life responsibility reverence for life treatment mistake treatment stop treat or not treat truth compliance confidence consensus health education cost - benefit analysis data security decision - making guiding concepts progress resources quality management withholding of treatment doctor - patient relationship socioeconomic allocation aspects strahlenther onkol 2003 no . 
some philosophers interpret guidelines as a hidden paternalism in a double sense : patients are not only denied the exercise of their autonomy , they are also denied access to the knowledge that they have lost this autonomy [ 45 ]  . 
in addition , the possibility of participating in a clinical study has to be clarified very early . based on this information , the patient can autonomously decide for or against therapy . 
all side effects , both acute and chronic , must be described in detail , e.g. , pelvic insufficiency fracture after radiotherapy of gynecologic tumors [ 50 ] , veno - occlusive liver disease [ 9 ] , obstruction of the esophagus [ 109 ] , or many others [ 71 ]  . 
how to achieve this in an optimal manner is not clear - cut , but should be adapted to the wishes of the individual patient , as an australian study showed [ 63 ]  . 
 palliative radiotherapy in contrast to adjuvant therapy as a special case of curative radiation oncology , palliative treatment cannot cure the patient . the primary aim of palliative radiotherapy is to improve the patients quality of life . 
different questionnaires may be useful in clinical practice of radiooncology to measure quality of life to give patients the possibility to express subjective changes in wellbeing , e.g. , in head and neck cancer patients [ 54 ]  . 
since greater patient participation in the decision - making process was found to be associated with increased anxiety levels which persisted over a 2 - week time span , the extent of patient information about palliative radiotherapy is still an unsolved problem [ 31 ]  . 
in clinical practice , if the patient is very ill , autonomy can overstrain hion the other hand , the decisions should not be made by the doctor alone [ 61 , 80 ]  . 
thus , providing adequate patient information is a difficult task , and the individual habits and information needs of each individual must be considered , as a study with 89 patients showed [ 24 , 46 ]  . 
special decision aids like structured description and trade - off exercises can help in decision - making , as shown for patients with locally advanced lung cancer , if radiotherapy alone or combined modality treatment is in discussion [ 14 ]  . 
for the individual patient , an emergency is often a stressful situation ; some patients are even unconscious . the life - threatening nature and the limited decision time cause a restriction in the patients autonomy . 
this restriction is much more pronounced if the patient is unconscious or a child . in this case , the supposed will of the patient must be determined or a decision in the best interest of the patient must be done . 
many oncology and radiotherapy patients are treated based on specific study protocols . in the past , clinical research has resulted in major progress , but in many respects , further improvements are still needed , e.g. , the lowering of chronic side effects or improving survival time [ 102 ]  . 
first , the science should primarily be about improving the welfare of the patient , but other interests on the part of the doctors and the economy can often play a leading role in clinical practice . 
for example , an actual meta - analysis has shown that studies which were sponsored by industry seldom reported about serious side effects in contrast to nonsponsored ones [ 27 ]  . 
good studies have to fulfill certain criteria such as equality of each treatment arm or criteria to finish the study earlier than planned , as a new paper has shown [ 25 , 81 ]  . 
chronic consequences of the disease and therapy are even more important for thein children , radiotherapy is often combined with chemotherapy and surgery , and > 70% are treated according to study protocols . 
this patient information is demanding and is often done in specialized centers . the importance of this is demonstrated in a recent publication which discovered deficits among adult survivors of childhood cancer regarding basic aspects of their diagnosis and treatment ; thus , only 70% recalled the site of the former radiotherapy correctly [ 58 ]  . 
nowadays , there is still a great need for information about ethics in ( radiation ) oncology , a point which was previously mentioned in a paper from 1987 [ 98 ]  . 
providing adequate patient information about radiotherapy is a subject which more radiotherapists need to deal with [ 78 ] , e.g. , developing tools for testing the comprehension of the patient information . 
 what consequences can be drawn for clinical practice ? the consultation between the patient and the physician and taking into account the individual situation of the patient are always the most important points which must be considered strahlenther onkol 2003 no . 
the radiation oncologist and his colleagues must take part in continuous medical education , which should include more than just radiation oncology alone , but should also specially train communication skills . 
more education in bioethics should be offered and more chairs for ethics at medical universities should be funded ; the ethics commission should be consulted more often , and a work group for ethics should be built into the german society of radiation oncology ( degro ) [ 23 , 79 ]  . 
first of all , the current practice of patient information should be defined . once problems are identified , such as truthfulness or palliative medicine , they should be examined by multidisciplinary teams . 
 strahlentherapie und onkologie original article an intra - patient dose - escalation study of disodium pamidronate plus radiotherapy versus radiotherapy alone for the treatment of osteolytic metastases monitoring of recalcification using image - processing techniques e . 
lambros vlahos1 objective : to evalutate the clinical benefit and mainly to monitor quantitatively the recalcification of osteolytic lesions after radiotherapy with or without intravenous infusion of disodium pamidronate ( dp ) in different doses . 
primary endpoints were the mean value and energy of gray - level histogram in plain radiographs ( mvglh and eglh ) and relative electron density ( red ) of ct scans in bone lesions . 
in eleven patients ( group a ) the dp dose was increased stepwise from 90 up to 180 mg ( flat dose ) , while in other 15 patients ( group b ) a flat dose of 180 mg was administered intravenously in 2 h . 
improvement was significantly higher in patients of group b versus a , while the results of pamidronate groups ( a and b ) were superior to group c , concerning the above indices ( p < 0.05 , mannwhitney test )  . 
 conclusion : the 2 - h infusional flat dose of 180 mg every 4 weeks seems to be tolerable and superior to 90 mg regarding palliation and mainly recalcification of osteolytic lesions . 
last but not least , the findings of mvglh , eglh and red indicate an important increase in bone mass and bone formation , which was difficult to be identified visually by the experts . 
 key words : osteolytic metastases disodium pamidronate radiotherapy palliation image processing dose escalation strahlenther onkol 2003 ; 179 : 4719 doi 10.1007 / s00066 - 003 - 0978 - 3 intra - patienten - dosiseskalationsstudie zu pamidronat plus strahlentherapie gegenber alleiniger strahlentherapie bei der behandlung osteolytischer metastasen . 
berwachung der rekalzifizierung mit bildverarbeitungsverfahren ziel : quantitative evaluation klinischer vorteile und der rekalzifizierung osteolytischer lsionen nach strahlentherapie allein oder in kombination mit einer intravensen infusion von pamidronat in unterschiedlicher dosierung . 
primre endpunkte waren der mittelwert und die energie der graustufenhistogramme in den normalen rntgenbildern ( mvglh und eglh ) und die relative elektrondichte ( red ) von ct - aufnahmen im bereich der knchernen lsionen . 
bei elf patienten ( gruppe a ) wurde die pamidronat - dosis stufenweise von 90 auf 180 mg erhht , whrend bei 15 weiteren patienten ( gruppe b ) eine dosis von 180 mg intravens in 2 h verabreicht wurde . 
die verbesserung war bei patienten der gruppe b erheblich hher 1 department of radiology , aretaieion university hospital , athens , greece , 2 department of electrical and computer engineering , institute of communication and computer systems , national technical university of athens , greece . received : december 10 , 2001 ; accepted : march 24 , 2003 strahlenther onkol 2003 no . 
radiotherapy and dose escalation of disodium pamidronate for bone metastases als bei patienten der gruppe a , whrend die ergebnisse der pamidronat - gruppen ( a und b ) deutlich besser als die der gruppe c waren . 
zustzlich hatten die pamidronat - gruppen eine erheblich niedrigere morbiditt bezglich des skelettsystems als gruppe c . schlussfolgerung : eine 2 - stndige infusion von 180 mg pamidronat alle 4 wochen scheint hinsichtlich der palliation und der rekalzifizierung osteolytischer lsionen besser zu sein als die 90 - mg - dosierung . 
the exceptional role of local radiotherapy in the treatment of lytic bone metastases is certain [ 1 , 14 , 24 , 32 ]  . beyond this , bisphosphonates are potent inhibitors of normal and pathologic bone resorption [ 9 , 20 ]  . 
to measure the bone loss and the bone structure , many researchers are using image - processing techniques for densitometry based on gray - level histogram of a simple plain radiography [ 5 , 10 ]  . 
intravenous infusion of pamidronate , a second - generation bisphosphonate , reduces bone pain in breast cancer patients and produces radiographic changes consistent with healing of bone lesions [ 35 ]  . according to the american society of clinical oncology ( asco ) guidelines for clinical use of bisphosphonates , the recommended dose of intravenous disodium pamidronate ( dp ) is up to 90 mg every 34 weeks [ 11 ]  . 
in order to evaluate the tolerability and , mainly , the efficacy of an intravenous flat - dose infusion of 180 mg dp concurrently with radiotherapy administration , we conducted an open - label phase i / ii study using as primary endpoints the first - order statistics of gray - level histogram in plain radiographs and measurements of bone relative electron density [ 21 , 38 ]  . 
 patient and methods subjects and study design from october 1998 until january 2000 , 42 patients with osteolytic metastases were presented at the radiotherapy department of aretaieion university hospital , athens , greece , for palliative irradiation . 
the inclusion criteria for pamidronate treatment were as follows : osteolytic metastatic lesion at least 1 cm in diameter in weight - bearing bone ; stable state after chemotherapy , hormonal therapy and corticosteroid ; no previous infusion of bisphosphonates or calcitonin ; no previous radiotherapy in the region of metastasis ; absence of hypercalcemia , pathologic fracture or epidural spinal cord compression ; serum creatinine level 2.0 mg / dl ; leukocyte count 3 , 500 / mm3 ; hemoglobin > 11 g / dl ; platelets > 100 , 000 / mm3 ; total bilirubin < 2.5 mg / dl ; absence of ascites ; and no clinically significant electrocardiographic changes . 
 the first eleven patients who were eligible for entering pamidronate treatment received intravenous infusion with an escalated flat dose of 90 up to 180 mg dp ( aredia , novartis inc )  . 
the initial aredia dose level was 90 mg and was increased stepwise up to 180 mg in increments of 30 mg ( first infusion : 90 mg , second infusion : 120 mg , third infusion : 150 mg , and forth infusion : 180 mg )  . 
according to the protocol , the first session of aredia was administered concurrently with external beam local radiotherapy ( 6 - mev linear accelerator , 30 gy total dose , given in ten fractions )  . 
after documentation of the absence of any adverse events related to the administration of dp , the remaining 15 patients received a 180 - mg flat dose of aredia for all six sessions . 
by this way , the patients who received pamidronate were organized in two groups according to the dp dose : patients with dose escalation ( group a ) and patients without ( group b )  . 
16 patients did not meet the criteria for pamidronate treatment : five due to electrocardiographic abnormalities and eleven due to low blood profile ( hemoglobin 11 g / dl or number of leukocytes < 3 , 500 / mm3 )  . 
ais : analgesic intake score ; bps : bone pain score ; eglh : energy of gray - level histogram ; mvglh : mean value of gray - level histogram ; red : relative electron density by ct scan ; uhpc : urinary hydroxyprolinecreatinine ratio ( mmol / mmol )  . 
ais : score fr die einnahme von schmerzmitteln ; bps : knochenschmerzscore ; eglh : energie des graustufenhistogramms ; mvglh : mittelwert des graustufenhistogramms ; red : relative elektronendichte gem ct ; uhpc : urinhydroxyprolin - kreatinin - verhltnis . 
although some patients of group c had a low hemoglobin level or low number of leukocytes , there was no significant difference between group a versus b and group b versus c , in terms of the latter mentioned parameters . 
the bone pain scores ( bps ) were calculated by multiplying the pain severity ( 03 ) by the pain frequency ( 03 ) , as described in previous studies [ 11 , 12 ]  . 
the improvement on palliative effect was also assessed using the analgesic intake scale ( ais ) according to who ( 0 = no analgesics ; 1 = nsaids ; 2 = weak opioids ; 3 = morphine )  . 
 image processing analysis : first - order statistics of gray - level histogram x - ray of the region of interest ( roi ) for all patients was obtained at the baseline of the study . 
for this reason , a registration of all regions in all six sessions for each individual patient was done manually by overlapping the images retaining the same segmentation of anatomic morpholostrahlenther onkol 2003 no . 
the quantitative assessment of bone loss was obtained using mean value and energy in terms of the first - order statistics [ 23 , 33 , 38 ] , as defined below . 
 if n ( i ) is the number of pixels whose intensity is i and n is the total number of pixels in the roi , then the occurrence probability of intensity i is : p ( i ) = n ( i )  . with eight - bit gray - level quantization , the resulting distribution takes the form of a first - order histogram with 256 bins , where each bin is one of the integer sample values i = 0 , , 255 . 
 in our study , two variables of gray - level histogram in terms of first - order statistics were assessed using the following measures [ 23 , 33 ] : mean value of gray - level histogram ( mvglh ) = ( cid : 1 ) ip ( i ) , i = 0 estimating the value around which central clustering occurs ; energy of gray - level histogram ( eglh ) energy = ( cid : 1 ) p ( i ) 2 . i = 0 when each gray - level in the roi is equally probable , the resulting histogram is uniforas mineral is lost from the lytic metastasis , the distribution of pixel intensities is shifted and becomes more concentrated in the lower gray levels . 
consequently , the mean value decreases and the energy increases [ 15 , 33 ]  . by this way , the expected total experimental test set consisted of 376 radiographs ( 26 patients cross twelve treatment sessions , 16 patients as controls cross four measurements )  . 
sophisticated software was developed for the image - to - matrix transformation , for the segmentation , and for the assessment of the aforementioned values mvglh and eglh in every roi . 
in order to further confirm the validity of this technique , parallel with the assessments of gray - level histogram , we measured the bone mineral concentration obtained by quantitative computed tomography in terms of bone electron density values [ 21 ]  . our quantitative assessments were based on the corrections of bone relative electron density ( cid : 2 ) e reported by thomas [ 36 ] , as it appears in the following formula : ( cid : 2 ) e = + 1.0 , 1 , 950 where hu stands for hounsfield units . 
 the measurements of red values were performed at baseline and 6 months later ( after the sixth session of pamidronate )  . endpoints the primary endpoints were the image - processing indices ( mvglh , eglh ) and the red values for bone lesions . 
monitoring of image - processing indices for group a and b was performed every month during routine pamidronate treatment , while for group c the monitoring of the later indices was performed every 3 months . 
the evaluation of bps and ecog status was performed in every session with bisphosphonate ( monthly ) for groups a and b , while for group c these evaluations took place every 3 months together with the assessment of image - processing indices . 
whole - body bone scintiscans and relevant conventional radiographs were performed bimonthly for tracking any new skeletal metastases , while the examination was hastening in case of suspicious persistent skeletal pain . statistical analysis the evaluation of statistical difference between means of two groups of patients was evaluated using the mann - whitney utest , while the difference between means of the three groups was assessed using the kruskal - wallis test [ 31 ]  . 
the intragroup comparisons between means of different time points were assessed using the wilcoxon signed test or the freidman two - way anova for two or more than two related samples , respectively [ 31 ]  . 
kaplan - meier estimates of the time from baseline to the first occurrence of any new skeletal complication for the adjuvant pamidronate treatment ( group a + b ) versus radiotherapy alone ( group c ) were calculated ; the log - rank test was used for between - treatment comparisons [ 19 ]  . 
two patients in group a ( 18.2% ) and five patients in group b ( 33.3% ) developed flu - like fever up to 38 c after 26 h from the infusion , which lasted for nearly 24 h and was well managed with acetaminophen . 
four patients in group a ( 36.4% ) and six patients in group b ( 40% ) complained of myalgias / arthralgias after the infusion had lasted nearly 24 h . one patient in group a ( 9% ) and one patient in group b ( 6.7% ) reported tachycardia and / or tensive sense of precardiac heartbeat 15 min to 1 h after the infusion which had lasted a maximum of 25 mthese patients underwent electrostrahlenther onkol 2003 no . 
 side effects infusional doses of aredia i.v. escalated ( 90180 mg ) ( n = 11 , group a ) 180 mg ( n = 15 , group b ) treatment session 1st 2nd 3rd 4th 5th 6th 7th 8th 9th12th 1st 2nd 3rd 4th 5th 6th 7th12th nausea flu - like syndrome myalgias / arthralgias tachycardia tensive sense of precardiac heartbeat cardiography , which was normal , and continued their next treatment sessions . 
the appearance of the above adverse events in group a was correlated with the higher doses of aredia , as shown in table 2 ( fourth to sixth session )  . 
from baseline until the endpoint of treatment for each patient , there were no significant changes in the laboratory values of serum calcium , serum phosphate , and urine calcium in any case . 
 response concerning the patients characteristics , no significant difference between the three groups was noted , as shown in table 1 ( p > 0.05 , kruskal - wallis test )  . 
an roi regarding a 50 - year - old female patient ( group b ) with a lytic area at the femur with assessments of gray - level histogram is shown in figure 1 . 
the measurements were showing significant differences from baseline ( p < 0.05 , wilcoxon test ) for all of the aforementioned variables regarding all groups . moreover , there was a significantly higher improvement in group b concerning the latter variables , while both group a and b showed significant superiority to group c ( p < 0.05 , mann - whitney test )  . 
absolute values of changes in bps , ecog status , ais , imageprocessing indices ( mvglh and eglh ) , red values from ct scan , and levels of uhpc 6 months post baseline : measurements by treatment group . 
absolutwerte der vernderungen von bps , ecog - status , ais , bildverarbeitungsindizes ( mvglh und eglh ) , red - werten nach ctaufnahmen und hhe des uhpc 6 monate nach erhebung der ausgangswerte : messung gem den behandlungsgruppen . 
radiotherapy and dose escalation of disodium pamidronate for bone metastases up , indicating a significantly higher incidence of new skeletal complication for patients who did not receive pamidronate treatment ( p = 0.23 , fishers exact test )  . 
the kaplan - meier distribution for new skeletal complication - free survival ( nscfs ) stratified per group c versus both group a and b is shown in figure 3 . 
assessments of gray - level histogram in terms of mean value and energy ( mvglh , eglh ) at baseline and 6 months after initiation of multimodality treatment , are shown on the right side . 
 the changes of mvglh were highly correlated with changes of eglh ( spearman ( cid : 2 ) = 0.99 , p < 0.001 ) , which means that every change in the one index is followed by changes in the other . 
thus , for practical reasons the following step was to present the time changes of mvglh ( without eglh ) and red values during 1 year of follow - up stratified per group ( a , b , and c )  . 
these mean changes are shown in figure 2 indicating the superiority of pamidronate treatment as an adjuvant therapeutic modality to radiotherapy : both mvglh and red values were higher for group a and b in comparison with group c . 
after 8 months from the baseline , the means of mvglh and red for group a and b are converging to each other , while for all groups these variables remained stable for the roi . 
after this time point , the imageprocessing indices remained stable ( p > 0.05 , freidman twoway anova test )  . in all groups , 6 months post - baseline and thereafter the bps and the ecog status remained stable ( p > 0.05 , freidman two - way anova nonparametric test ) as long as no new bone metastases were observed . 
during a period range of 12 months after the initiation of the combined treatment , the remaining 25 patients of group a and b ( % ) showed no evidence of local relapse or new secondary lesions ( skeletal or elsewhere )  . 
as a comment , for quantitative measurements of bone mass in osteolytic lesions located in the thoracic or abdominal skeleton , the assessments of bone red values by using ct scans should then be the method of choice . bisphosphonates ( pamidronate ) , in the treatment of osteolytic metastases , reduce the incidence of nonvertebral pathologic fractures , hypercalcemia and bone pain and improve patients quality of life [ 6 , 11 , 12 , 35 , 37 ]  . 
 [ 39 ] concerning 79 patients with severe pagets disease given multiple intravenous pamidronate courses over a mean period of 45 months with pamidronate dose per course up to 180 mg , usually administered over 3 days . 
in our study , as shown in table 3 , the combined treatment of high doses of pamidronate up to 180 mg in conjunction with radiotherapy is superior to radiation alone ( group a and b ) , in terms of all measured variables 6 months post - baseline . 
the same conclusion is also coming from figure 2 , regarding the time course of image - processing indices . however , measurements of mvglh and red > 6 months post - baseline seem to be equalized , since the curves are converging to each other . 
the possible explanation for this might be the equal infusional dose of 180 mg of pamidronate for both group a and b , given after the fourth session of intravenous treatment . 
in all cases of drug - related toxicity , the onset of an adverse event was reported within 16 h after the infusion , probably related to the renal clearance of pamidronate [ 8 ]  . 
the two patients who complained of tachycardia and / or tensive sense of precardiac heartbeat had also neuropsychologic disorders , and these adverse events may be related with their psychologic profile , since neither electrocardiographic abnormalities nor clinical signs of hypoor hypercalcemia were diagnosed . 
 as for the uhpc values 6 months post - baseline , there was a 46.7% decrease in group a versus 53.1% in group b ( p < 0.05 , mann - whitney test ) and 30.1% in group c that was significantly inferior to both pamidronate groups ( p < 0.05 , mann - whitney test )  . 
 [ 26 ] measured the loss of bone mass observed in metastatic prostate cancer using dual - energy x - ray absorptiometry . more relevant to the current study , rizzoli et al . 
 [ 27 ] , in a randomized trial with or without administration of oral bisphosphonates in patients with skeletal metastases from mammary carcinoma , objectively measured the bone mineral density and reported a significant recalcification in the pamidronate group . 
by our method , using parallel measurements of the optical density of the x - ray film , the decalcification can be detected earlier as has been well documented previously [ 15 , 16 ]  . 
in this study , the validity of image - processing technique was further confirmed regarding the significant correlation of changes between image - processing indices and bone red values [ 36 ]  . the major disadvantage of the method is the failure of detecting assured bone - mass differences in case of bones superimposed by moving tissues ( e.g. , thorax , abdomen , etc . ) that produce random errors in the procedure of image analysis [ 2 , 33 ]  . consequently , the method of first - order statistics is limited in bone - density assessments of certain anatomic areas of weightbearing bones such as the axial bones of the extremities . 
radiotherapy and dose escalation of disodium pamidronate for bone metastases ( absolute value = 0.0125 ) is obviously related to the higher doses of pamidronate , while the lower changes in group c are apparently related to the absence of pamidronate treatment . since , the uhpc values are correlated with bone resorption procedure [ 29 ] , we may conclude that higher nonescalated dos - es of pamidronate up to 180 mg ( group b ) may enhance recalcification better than the escalated intravenous doses ( group a ) , while the absence of pamidronate treatment deprives the remineralization process of the molecules binding to bone hydroxyapatite [ 9 , 35 ]  . 
besides , this argument is in accordance with the results reported here , regarding the significant differences in the image - processing indices between adjuvant pamidronate treatment and radiotherapy alone . 
 in terms of prevention of new skeletal complications , the pamidronate groups were significantly superior not only in the incidence of new bone lesions but also in the delay of presentation of new metastases ( p = 0.011 , log - rank test )  . 
furthermore , the fact should not be underestimated that after response to treatment , the clinical status and the image - processing indices remained stable with reference to the initial osteolytic lesion . 
the results of this study indicate that the intravenous use of 180 mg dp ( aredia ) , in conjunction with radiotherapy , successfully relieves pain , minimizes the need for analgesic intake and mainly leads to recalcification of lytic metastases , which was difficult to be recognized visually by radiology experts . 
generally , bisphosphonates and radiotherapy are not a priori precluded in clinical trials or routine medical practice , and the idea of combining the two modalities has also been noted [ 11 , 17 ]  . 
the radiotherapy schedule ( 30 gy in ten fractions ) used in this study is in accordance with the american college of radiology recommendations regarding palliative irradiation in secondary bone lesions [ 28 ]  . 
additionally , koswig & budach [ 13 ] , in a prospective randomized trial , examined quantitatively , by the use of computerized tomography , the recalcification following radiotherapy for bone metastases ( 1 ( cid : 3 ) 8 gy vs . 10 ( cid : 3 ) 3 gy ) and reported a higher level of remineralization in the fractionated group than in the single - dose group . 
 [ 14 ] , in a retrospective analysis of 176 patients , concluded that the fractionation scheme of 10 ( cid : 3 ) 3 gy for 2 weeks offers high response rates and is recommended . 
although the hemoglobin in some patients of group c was < 11 g / dl as they were precluded from bisphosphonate treatment , overall , the mean values of hemoglobin were around 12 g / dl ( table 1 )  . 
even though our population was small and beyond the nonrandomized design of the study , the main aspect of this trial and the message that would be important for future trials is summarized to this : intravenous administration of 180 mg pamidronate in conjunction with local radiotherapy seems safe and effective as well ; lytic bone metastases may need higher dose of pamidronate than the recommended one ( 90 mg flat infusional dose )  . 
image - processing techniques in plain radiography are a simple and reliable tool for monitoring substantial changes in bone mass that is beyond the visual threshold of recognition by experts in radiology . 
the agreement between measurements for bone red and first - order statistics of gray - level histogram further ensures the validity of image - processing indices of mvglh and eglh . 
the high correlation in terms of spearman ( cid : 2 ) - test among measurements of mvglh and eglh was more or less expected , since they are both related to each other as they both represent first - order variables of statistics of texture analysis . 
beyond the strong indication of the efficacy and the tolerability of 180 mg pamidronate , the results presented here should also serve as stimulus to and foundation of continued study of multimodality therapy in the palliative treatment of osteolytic metastases . 
 strahlentherapie und onkologie original article sucralfate versus mesalazine versus hydrocortisone in the prevention of acute radiation proctitis during conformal radiotherapy for prostate carcinoma a randomized study * giuseppe sanguineti1 , paola franzone1 , michela marcenaro1 , franca foppiano2 , vito vitale1 purpose : to assess whether the topical use of steroids or 5 - aminosalicylic acid ( 5 - asa ) is superior to sucralfate in preventing acute rectal toxicity during three - dimensional conformal radiotherapy ( 3dcrt ) to 76 gy . 
 patients and methods : patients undergoing 3dcrt for prostate carcinoma at our institution were offered to be randomized to sucralfate 3 g in 15 ml suspension enema ( antepsin ) , mesalazine 4 g gel enema ( enterasyn ) , or hydrocortisone 100 mg foam enema ( colifoam )  . 
 results : the trial was opened in august 1999 , and after the first 24 patients had been treated , arm 2 was discontinued because of eight patients receiving mesalazine , seven actually developed acute rectal toxicity ( five patients grade 3 and two patients grade 2 )  . 
 key words : acute rectal toxicity radiotherapy prophylaxis strahlenther onkol 2003 ; 179 : 46470 doi 10.1007 / s00066 - 003 - 1082 - 4 sucralfat versus mesalazin versus hydrocortison zur prvention der akuten strahlenproktitis unter konformaler radiotherapie des prostatakarzinoms : eine randomisierte studie fragestellung : randomisierter vergleich der lokalen anwendung von steroiden oder 5 - asa oder sucralfat zur prvention einer akuten strahlenproktitis unter 3 - d - konformaler radiotherapie ( 3dcrt ) bis 76 gy . 
nachdem die ersten 24 patienten aufgenommen worden waren , wurde arm 2 abgebrochen , da sieben patienten unter mesalazin eine akute strahlenproktitis ( grad 3 bei fnf patienten und grad 2 bei zwei patienten ) entwickelten . 
prevention of proctitis during 3dcrt bis zum mai 2001 wurden 134 patienten der lokalen anwendung von sucralfat ( 63 patienten ) , mesalazin ( acht patienten ) oder hydrocortison ( 63 patienten ) zugefhrt . 
 schlsselwrter : akute strahlenproktitis radiotherapie prophylaxe introduction acute rectal toxicity is a frequent side effect of radiotherapy for prostate cancer , although reported percentages are often very different among institutions and data from controlled studies and modern techniques are scarce . 
as stated by four recent prospective studies , the incidence of grade 2 + gastrointestinal acute toxicity according to rtog scale ( table 1 ) [ 3 ] ranges between 19% and 71% [ 22 , 27 , 30 , 37 ]  . 
such variability is mainly due to differences in interpretation of rtog scoring criteria among observers , in the amount of rectum within the irradiated volume ( depending on several factors such as treated volumes , use of shields , margins around target volume , fields arrangement ) and in total dose / fractionation schedules . 
 acute rectal toxicity causes patient discomfort and reduces both patient compliance to treatment and quality of life [ 13 , 30 , 40 ]  . in addition , we and others have also reported a correlation between acute and late rectal toxicity [ 33 , 36 ]  . 
although this not an unequivocal finding and a causative relationship between the two is only suggested , acute toxicity prophylaxis may possibly translate in a lower rate of late reactions as well . this is particularly attractive since late rectal toxicity actually represents a major limiting factor of dose escalation even with modern techniques . in 1998 , zimmerman & feldmann [ 41 ] reviewed prophylactic treatments for radiation proctitis and failed to establish that any current regimen was effective . 
in particular , sucralfate , despite two early positive studies [ 14 , 39 ] , was not found to be beneficial in preventing both small bowel and rectal toxicity during radiotherapy [ 6 , 20 , 23 ] even was delivered topically as an enema [ 30 ]  . 
data on 5 - aminosalicylic acid ( 5 - asa ) and its precursors are controversial , with some studies showing a reduction of toxicity [ 17 , 18 , 25 , 31 ] , but with others showing no effect or possibly worsening of symptoms [ 1 , 9 , 24 , 32 ]  . 
corticosteroids have been successfully used in the treatment of acute and late radiation - induced proctitis although never tested within a randomized study [ 4 , 12 , 21 ]  . 
recently , it has been shown that topical hydrocortisone foam is well tolerated and has neither systemic effects on cortisol physiology nor late effects on rectal mucosa [ 38 ]  . the purpose of the present trial was to assess whether 5asa and hydrocortisone have any role in preventing acute proctitis due to radiotherapy . 
 patients and methods participation in the trial was offered to all patients with localized prostate carcinoma ( t14 n0x m0 ) who were to receive three - dimensional conformal radiotherapy ( 3dcrt ) to 76 gy . 
planning ct was obtained with 5 - mm slices throughout the whole treated field . after clinical target volume ( ctv ) contouring on each slice as appropriate , the planning target volume ( ptv ) was obtained by adding 1.3 cm to ctv except at the prostate - rectum interface where a 0.8 - cm margin was used . 
since we did not have the possibility to run a composite plan including both the prostate plus seminal vesicles and the prostate - only phases when appropriate , rectal dose - volume histograms were obtained for the initial 60 gy only . 
 grade no change increased frequency or change in quality of bowel habits not requiring medication ; rectal discomfort rectal or abdominal pain not requiring analgesics requiring analgesics diarrhea requiring parasympathodiarrhea requiring parenteral lytic drugs / mucus discharge not necessitating sanitary pads ; acute or subacute obstruction , fistula support ; severe mucus or blood or perforation ; gi bleeding requiring discharge necessitating sanitary pads ; abdominal distension transfusion ; abdominal pain or tenesmus requiring tube decompression or bowel diversion after enrollment , patients were randomized to sucralfate 3 g in 15 ml suspension enema ( antepsin , arm 1 ) , mesalazine 4 g gel enema ( enterasyn , arm 2 ) or hydrocortisone 100 mg foam enema ( colifoam , arm 3 )  . 
 patients were given a closed envelope with drug prescription and directions for intake on a self - administration basis . topical treatment had to be performed once daily , starting on day 1 of 3dcrt , preferably before going to sleep in order to retain enema for as long as possible . 
the two other drugs had already been manufactured with special devices to allow the proper dose and administration in the lower rectu additional information was available by research nurses . randomization was blind to the treating physician . 
 regarding treatment - related factors , we included in the analysis also the dose amount released per week ( weekly dose , wd ) which is a strong determinant of acute toxicity especially when using a time - dependent endpoint [ 34 ]  . 
however , because of concerns about worsening effects of radiation - induced toxicity by 5 - asa , an interim analysis was planned after the first 24 patients had been completed . 
 results the trial was opened in august 1999 , and after the first 24 patients had been treated , arm 2 was discontinued because of eight patients receiving mesalazine , seven actually developed acute rectal toxicity ( five patients grade 3 and two patients grade 2 )  . 
 until may 2001 , 110 additional patients were randomized . therefore , 134 consecutive patients were randomly assigned to sucralfate ( 63 patients ) , mesalazine ( eight patients ) or hydrocortisone ( 63 patients )  . 
one patient died during treatment at 14 gy due to acute myocardial infarction , one refused further 3dcrt at 44 gy , and one never started 3dcrt because he opted for surgery after randomization . 
most delaying patients were also treated six ( on saturdays as well ) instead of five times per week during 1 or more weeks in order to compensate for missed treatments . 
patients receiving mesalazine did show an increased risk of acute rectal toxicity compared to those who received sucralfate , but , again , no statistical difference was seen between the hydrocortisone and sucralfate arms ( table 3 )  . no other covariate showed predictive value , including those correlated with the amount of rectal volume receiving 20 or 50 of the initial 60 gy . 
most of the patients with wd < 28 gy / 3 weeks were still treated at wd 24 gy / 3 weeks ( figure 4 )  . the results were confirmed when the three patients who did figure 3 . 
ad : androgen deprivation ; ci : confidence interval ; d : total dose of radiotherapy ; hr : hazard ratio ; v20 / 50 : percentage of rectal volume receiving at least 20 / 50 gy ; wd123 : weekly dose during the first 3 weeks of radiotherapy . 
hr : hazard ratio ; wd : wchentliche strahlendosis in den ersten 3 wochen der radiotherapie ; d : gesamte strahlendosis ; v20 / 50 : prozentualer anteil des rektumvolumens unter mindestens 20 / 50 gy ; ad : androgenblockade . 
at a microscopic level , there is evidence of cell depletion of the mucosal layer associated with an inflammatory infiltrate and slight mucosa edema [ 29 ]  . sucralfate ( aluminum sucrose octasulphate ) has been extensively investigated as protective agent [ 6 , 14 , 20 , 23 , 30 , 39 ]  . despite two positive studies , demonstrating a reduction of stools or diarrheal stools per day [ 14 , 39 ] , four other studies did not show any benefit on either small bowel [ 6 , 23 ] or colorectum [ 20 , 23 ]  . 
86 patients from four different institutions who were to receive radiotherapy to the prostate using a four - field technique were randomized to either 3 g of sucralfate given in 15 ml suspension or 15 ml placebo suspension . peak incidences of rtog proctitis were similar in both arms : figure 4 . 
 due to the lack of both financial support and drug company interest , we did not have the possibility to provide patients with a placebo product manufactured in the same way as the experimental drugs . 
in order to minimize the bias due to the lack of treatment in one arm , we decided to give a treatment to each arbased on the above findings [ 30 ] , we considered the sucralfate arm to be the control group . 
in general , double - blind studies yield significantly smaller treatment results than trials that are not double - blinded [ 16 ] especially for softer outcomes [ 10 ]  . 
prevention of proctitis during 3dcrt lack of masking to patient may have kept control of bias related to physician preference but not of that related to patient preference , even if , again , every patient did receive a treatment . 
however , since unmasking bias usually leads to differences between treatments [ 16 ] , it is unlikely that the design had an impact at least on our negative findings , i.e. , the comparison of the steroid and the sucralfate arms . 
 to our knowledge , this is the first study to enroll a homogeneous group of patients who were consistently planned to be treated with the same conformal technique to the same total dose . 
the rationale is that both drugs , that have been successfully employed in the treatment of inflammatory bowel disease [ 19 ] , interfere with the metabolism of eicosanoids whose production increases during the acute phase of toxicity [ 2 ]  . 
prior to the present study , results with 5asa and its precursors have been controversial [ 1 , 9 , 17 , 18 , 24 , 25 , 31 , 32 ]  . sulfasalazine 500 mg tablets t.i.d. 
other endpoints ( such as the higher maximum change from baseline in the severity of diarrhea and the number of days of diarrhea per week ) were significantly different in favor of the control / placebo arm [ 1 ]  . 
 [ 24 ] reported an increased incidence and severity in patients randomized to olsalazine , a precursor of 5 - asa . regarding topical treatment , the only available report is from freund et al . 
the study was prematurely closed after 16 patients had been entered because 75% of the 5 - asa arm patients developed severe rectal toxicity compared to just one patient in the placebo group [ 9 ]  . 
our experience is similar in that we prematurely closed the arm after a significantly higher ( 62.5% ) incidence of severe reactions had been found in the 5 - asa arm . we conclude that topical 5 - asa is contraindicated during radiotherapy although the exact mechanisms remain obscure [ 26 ]  . 
secondly , it has been shown that hydrocortisone foam treatment does not modify the daily cortisol profile and is not associated with late changes of treated mucosa [ 38 ]  . 
finally , topical steroids are commonly used to treat acute and late proctitis [ 4 , 12 , 21 ]  . however , to our knowledge , no study has tested the role of topical hydrocortisone in preventing acute proctitis so far . our study failed to find a benefit for hydrocortisone compared to sucralfate . as a whole , our study questions the exact role of eicosanoids in the pathogenesis of rectal toxicity and confirms the scarce knowledge of the pathophysiology of acute rectal symptoms [ 11 , 15 , 35 ]  . 
therefore , our data , in a provocative way , suggest that a wd < 26 gy during the first 3 weeks reduces the risk of grade 2 + toxicity by 50% . since , due to the limited amount of prostate cancer cell repopulation during treatment , overall treatment time is usually not considered a critical factor in prostate cancer [ 8 ] , this strategy seems free of significant side effects . 
 strahlentherapie und onkologie original article analysis of competing risk parameters in irradiated prostate cancer patients ramona mayer1 , karl pummer2 , franz quehenberger3 , 4 , elisabeth mayer1 , guenther feigl5 , uwe langsenlehner1 , arnulf hackl1 purpose : retrospective competing risk analysis of prognostic factors in definitive - irradiated prostate cancer patients . 
 patients and methods : data of 652 patients were analyzed according to three age subgroups ( < 65 , 65 75 , > 75 years ; table 1 )  . 
adjuvant hormone therapy ( n = 261 ) consisted either of orchiectomy ( n = 151 ) or lhrh agonist with / without antiandrogen therapy or , in the early years , diethystilbestrol . neoadjuvant hormone therapy ( n = 31 ) using lhrh agonists was given 6 months before and during radiotherapy . 
higher age ( > 75 years ) decreased the relative risk of lf , dm , and pcd significantly . key words : prostate cancer external radiotherapy competing risk analysis biochemical failure clinical failure survival prognostic factors strahlenther onkol 2003 ; 179 : 4526 doi 10.1007 / s00066 - 003 - 1058 - 4 analyse konkurrierender risikoparameter nach bestrahlung des prostatakarzinoms ziel : retrospektive analyse prognostischer faktoren bei patienten mit primr bestrahltem prostatakarzinom unter beachtung konkurrierender risiken . patienten und methodik : die daten von 652 patienten wurden in drei altersgruppen geteilt ( < 65 , 65 75 , > 75 jahre ) und analysiert ( tabelle 1 )  . 
als adjuvante hormontherapie ( n = 261 ) wurde entweder eine orchiektomie ( n = 151 ) oder eine therapie mit lhrh - agonisten mit / ohne antiandrogene oder in frhen jahren dithylstilbstrol durchgefhrt . 
 ergebnisse : bei 69 / 340 patienten wurde in der nachsorgezeit ein psa - anstieg ( biochemisches versagen ) beobachtet ; 5 jahre nach dem biochemischen versagen zeigten 64 , 9% dieser patienten auch ein klinisches versagen . 
in der multivariaten analyse ( tabellen 2 und 3 ) waren tumorstadium ( relatives risiko [ rr ] 4 , 54 ) , prtherapeutischer psa - wert ( rr 2 , 79 ) und tumordifferenzierung ( rr 2 , 96 ) signifikante prognosefaktoren fr das biochemischen versagen ( tabelle 2 )  . 
die hormontherapie erniedrigte deutlich , jedoch nicht signifikant , das risiko von biochemischen versagen ( rr 0 , 67 ) , fernmetastasen ( rr 0 , 59 ) und tumorassoziiertem tod ( rr 0 , 60 )  . 
die mediane nachsorgezeit betrug 7 , 6 jahre . schlussfolgerung : das risiko des biochemischen versagens wurde durch das prtherapeutische psa , das tumorstadium und die tumordifferenzierung signifikant vorhergesagt ; 5 jahre nach biochemischem versagen betrug die kumulative inzidenz eines in1 department of radiotherapy , 2 department of urology , and 3 department of informatics , statistics and documentation , university medical school of graz , austria , 4 department of medical statistics , university of leiden , the netherlands , 5 international neuroscience institute , hannover , germany . received : june 5 , 2002 ; accepted : february 21 , 2003 strahlenther onkol 2003 no . 
 schlsselwrter : prostatakarzinom externe strahlentherapie analyse konkurrierender risiken biochemisches versagen klinisches versagen berleben prognostische faktoren introduction localized adenocarcinoma of the prostate can be treated by means of established techniques like external photon radiotherapy , brachytherapy ( or combination of both ) or special centers - adapted therapies such as proton therapy [ 4 , 9 , 25 , 30 , 34 , 36 ]  . 
by using conformal radiotherapy as well as different technical aids , sufficient irradiation doses can be delivered with a reduced risk of radiation - induced side effects [ 5 , 7 , 13 , 15 , 24 , 35 , 40 , 41 , 45 ]  . 
 the introduction of serum psa level evaluation as part of routine examination of prostate cancer patients had a tremendous impact on the definition of study endpoints used in surgical as well as radiation studies . 
even though the precise definition of biochemical control , particularly following radiation treatment , is still somewhat controversial [ 19 , 39 ] , it is undeniable that the biochemical control as a defined endpoint of clinical studies enabled the scientific community to analyze their studies in a much more accurate manner than before [ 27 , 28 , 32 , 42 , 43 ]  . 
clinical failure as an endpoint is due to its mode of determination of a less precise finding than biochemical failure but very important to the patient , because it causes morbidity and ultimately results in death . 
 in this analysis , we tried to identify prognostic indicators for biochemical failure as well as clinical failure and prostate cancer death in definitive - irradiated prostate cancer patients . progression of disease is slow after initial treatment , and death from other causes should be accounted for by the competing risk analysis [ 1 , 2 , 8 , 10 , 18 ]  . 
this method adjusts for patients who die of intercurrent diseases prior to reaching the event of interest and omits overestimation of the probability of failure in the presence of competing risks . 
36 patients who were diagnosed to have lymph node and / or distant metastases at the time of radiotherapy were excluded ; the remaining 652 patients formed the study cohort . 
mean age at the time of radiotherapy was 70.2 years ( median 70.3 years , range 46.985.6 years ) ; the distributions of tumor and treatment characteristics according to the three age groups ( < 65 , 65 75 , > 75 years ) are listed in table 1 . 
 prior to radiotherapy , all patients were staged with digital rectal examination , chest x - ray , bone x - ray or bone scan . computed tomography ( ct ) or magnetic resonance imaging ( mri ) of the pelvis were available in 95% of the patients . 
 external radiotherapy radiotherapy consisted of high energy photon beams ( median 70 gy , mean 68.8 gy , range , 5072 gy ) and was delivered to the prostate and / or seminal vesicles in a three - field technique with two lateral and one anterior field ; in all patients , the definition of the target volume was based on ct scans . 
irradiated prostate cancer : analysis of competing risk parameters target volume ( prostate gland seminal vesicles ) plus a 1 - cm marg since 1998 , three - dimensional treatment planning was available , and the dose was described in the central part of the ptv on or near the central axis of the beam intersections as recommended by the international commission on radiation units and measurements ( icru )  . 
 hormone therapy neoadjuvant hormone therapy was given to 31 men using luteinizing hormone - releasing hormone ( lhrh ) agonists and started 6 months before radiotherapy and stopped at the end of radiotherapy . 
261 patients received adjuvant hormone therapy using either orchiectomy ( n = 151 ) or lhrh agonists with / without antiandrogen therapy or , in the early years , diethystilbestrol . 
 follow - up data were acquired by analyzing both the medical records obtained during regular follow - up examinations at the department of radiotherapy and the reports of the treating urologists . 
the proportional hazards model for subdistributions of a competing risk [ 11 , 16 ] was used to analyze the effects of pre - rt variables ( preirradiation psa , tumor stage , tumor grade , age ) and treatment variables ( androgen deprivation ) and to adjust for potential confounding variables ( univariate and multivariate analysis )  . 
follow - up was defined according to the reverse kaplanmeier method , which means that the kaplan - meier survival curve is constructed reversing censor and failure and the median follow - up is the 50% point of that curve [ 3 , 38 ]  . 
in contrast to that , predictors of a lower relative risk of prostate cancer death were old age ( > 75 years ; rr 0.09 ; 95% ci 0.010.62 ; p = 0.01 ) and age as a continuous variable ( rr 0.92 , 95% ci 0.890.96 ; p < 0.0001 ) , which means that with each year of age the hazard of prostate cancer death decreases by 8% . 
in comparison to that , higher age ( > 75 years ) decreased the relative risk of local failure as well as the risk of distant failure and prostate cancer death significantly . 
 discussion prostate cancer is a disease that occurs mostly in elderly patients who , due to their higher age , have an increased incidence of comorbidities and , by that , a higher risk of intercurrent death [ 10 , 17 , 26 ]  . 
 [ 18 ] demonstrated that in patients < 65 years of age , there was no statistically significant difference in the biochemical control rate regardless of which of the two statistical methods kaplan - meier or competing risk analysis was used . 
in patients > 65 years of age , however , the kaplan - meier method estimated the biochemical control rate clearly too low , because the competing risks were not taken into consideration . 
this particular problem must especially be taken into account when comparing control rates of the generally several years younger surgically treated patients with the control rates of the generally older radiotherapeutically treated patients . in our study , we retrospectively analyzed the data of a group of patients with localized prostate cancer who underwent definitive radiotherapy treatment . 
in our experience , the ct examination , in spite of its limitations , is not only important for the detection of enlarged lymph nodes or metastases but also for the detection of unrelated secondary malignant diseases . 
these results , however , were not included in the evaluation of the results of our retrospective analysis . for the staging process of our patients , we used only the results of the clinical evaluation ( including ct scans )  . 
in recent years , the ptv included the prostate gland and / or seminal vesicles with an adequate safety margin to further reduce the risk of acute and late radiation side effects . 
the definition of young age and old age varies throughout the literature and makes a direct comparison of results rather difficult [ 2 , 17 , 2123 , 31 ]  . an interesting analysis was done by huguenin et al . 
the authors estimated the rates of distant failure as a first failure by using the cumulative incidence method and found that patients in their old age group ( > 65 years ) had a significantly higher incidence of distant failure . 
in our analysis , we went one step further and subdivided the old age group ( > 65 years ) into two subgroups ( 65 75 , > 75 )  . 
although the relative risk of dying from prostate cancer was low in our patients > 75 years , this must be interpreted with caution , since these patients actually underwent definitive treatment , and one can only speculate how these patients would have done without therapy . 
the authors found out , that patients with untreated poorly differentiated prostate cancer face a high risk of death from this tumor even if prostate cancer was diagnosed as late as age 74 years . 
 a further issue analyzed in our study was to find out whether the predictive value of the biochemical control rate is also valid and true for clinical events such as local failure , distant failure , and prostate cancer death . 
increasingly more studies started to use the psa value as the only measure of therapeutic success . the precise definition of biochemical failure following radiation treatment , however , is still discussed controversially [ 19 , 39 ]  . 
 [ 39 ] compared the fccc and the astro definition and found out , that the fccc definition had a slightly decreased specificity compared to the astro definition , but a substantially increased sensitivity . 
an important but sometimes underrated issue that not so many studies have tried to shed a light on so far is whether the psa value can also serve as a powerful indicator for clinical endpoints such as local failure , distant failure , and prostate cancer death . 
in contrast to that , the relative risk of distant metastasis was predicted by tumor stage and gleason score ; for cause - specific survival , only the tumor stage turned out to be an independent predictor . 
 in addition to the other prediction factors , we also looked at the independent influence of additional hormonal therapy . the multivariate analysis showed that hormonal therapy decreased the relative risk of biochemical failure , distant failure , and survival without reaching statistical significance . 
irradiated prostate cancer : analysis of competing risk parameters strahlentherapie und onkologie case report lung cancer and rosai - dorfmans disease a clinicopathological study johannes lutterbach1 , karl henne1 , axel pagenstecher2 , joachim bhm3 case report : a 60 - year - old female patient underwent craniotomy for a cerebral lesion in the frontoparietal lobe . 
the patient died more than 7 years after the diagnosis of a metastasizing lung cancer due to pneumonia . conclusion : in a patient with a pulmonary neoplasm and suspected supraclavicular lymph node spread , rosai - dorfmans syndrome should be considered as a rare differential diagnosis . key words : brain metastasis long - term survival lung cancer radiation therapy rosai - dorfmans disease sinus histiocytosis strahlenther onkol 2003 ; 179 : 48692 doi 10.1007 / s00066 - 003 - 1032 - 1 bronchialkarzinom und rosai - dorfman - syndrom : eine klinisch - pathologische studie fallbericht : eine 60 - jhrige patientin wurde aufgrund einer frontoparietal lokalisierten zerebralen raumforderung operiert . 
 schlsselwrter : gehirnmetastasen langzeitberleben lungenkarzinom strahlentherapie rosai - dorfman - syndrom sinushistiozytose introduction despite remarkable therapeutic advances , lung cancer still carries a poor prognosis as indicated by a 2 - year survival of about 10% [ 13 , 24 ]  . 
in patients with early - stage primary tumors and a single brain metastasis , aggressive treatment yielded a 5 - year survival of more than 20% [ 12 ]  . 
 1 department of radiation therapy , 2 department of neuropathology , and 3 department of pathology , university hospital , freiburg , germany . received : april 4 , 2002 ; accepted : june 19 , 2002 strahlenther onkol 2003 no . 
lung cancer and rosai - dorfmans disease in 1969 , rosai & dorfman [ 21 ] first described a rare syndrome characterized by bilateral lymph node enlargement in the neck due to massive histiocytosis in dilated subcapsular and medullary lymph sinuses . 
 case report in march 1992 , a 60 - year old female patient was admitted to freiburg university hospital , department of neurosurgery . she complained about weakness in her right arthe symptoms had increased gradually over 6 weeks . 
 a computed tomography of the brain showed a cystic lesion in the left hemisphere of 9 cm in maximum diameter , with perifocal edema and midline - shiafter drainage of the cyst ( figure 1a ) the symptoms improved markedly . 
in daily fractions of 2 gy , whole brain radiation therapy was given to a dose of 40 gy , followed by a 10 - gy boost to the tumor bed . the treatment was administered via lateral opposed fields with 6 mv photons of a linear accelerator . 
 as prior medical history was empty and the patient never used to smoke , a complete tumor staging was performed . an x - ray examination and a computed tomography of the chest revealed a suspicious lesion close to the hilus of the left lung with a diameter of 2.8 cm ( figures 2a and 2b )  . 
further diagnostic procedures , including computed tomography of the abdomen , gastroscopy , colonoscopy , gynecological examination , mammography , ultrasound and fine - needle biopsy of the thyroid gland revealed no abnormalities . 
given the poor prognosis of patients with non - small cell lung cancer metastatic to the brain in general and considering the fact that the patient was asymptomatic with regard to the bronchial neoplasm she remained without further treatment . 
repeated computed tomography scans of the brain showed no tumor recurrence in the left frontoparietal region or any new cerebral lesions ( see figure 1b )  . on x - ray examinations of the chest , a slow but continuous growth of the primary tumor was seen . 
 in june 1996 , the patient was readmitted to our hospital . she complained about a painless cervical and submandibular swelling that had developed within 6 weeks , loss of appetite and decrease in performance status . 
laboratory data were : hemoglobin 11.5 g / dl , white blood cells 15 , 400 / mm3 with 87% segmented neutrophils , 6% lymphocytes , 6% monocytes , < 1% eosinophils , and < 1% basophils , thrombocytes 330 , 000 / mm3 , erythrocyte sedimentation rate 50 / 80 mm , c - reactive protein 32 mg / dl , total serum protein 7.2 g / dl with hypergammaglobulinemia of 33% . 
besides serologic evidence of a latent infection with epstein - barr virus , cytomegalovirus , and toxoplasma , no antibodies against human immunodeficiency virus , treponema pallidum , salstrahlenther onkol 2003 no . 
in september 1998 , a total atelectasis of the left lung due to complete obstruction of the main bronchus by exophytic tumor masses was found by bronchoscopy ( see figures 2g and 2h )  . 
similar cases , some of them with survival times of 10 years or more , have occasionally been reported in the literature [ 1 , 3 , 15 ]  . 
in these histologic types of lung carcinomas , the overall proliferation index and the apoptotic index of the tumor cells showed a median value of 21% and 1% , respectively . 
however , doubling time in adenocarcinomas varied from 2.8 months to 10 months . retrospectively , the decision not to treat the primary tumor turned out to be wrong in our case . 
given the fact that the patient had no cerebral recurrence and did not develop extracerebral metastases in the further course of the disease , radical surgery of the bronchial neoplasm might have resulted in cure . 
 although similarities to malignant lymphoma have been noted [ 2 ] , only five of more than 400 cases which were studied in a registry for shml had associated hematological neoplasms [ 5 ]  . 
another confounding aspect was that the laboratory findings were suggestive of an acute infection , but the patient was completely asymptomatic with regard to her lung tumor and no other inflammatory focus could be detected . 
lung cancer and rosai - dorfmans disease lymph node enlargement , histological examination excluded a tumor metastasis and revealed the typical features of shml characterized by massive sinus histiocytosis with immunohistological expression of s100 - protein ( figure 4d )  . 
in less problematic situations , various treatment concepts were adopted , including the administration of radiation therapy [ 17 ] , chemotherapy [ 6 ] , antiobiotics [ 22 ] , tuberculostatics [ 22 ] , steroids [ 19 ] , and interferon [ 11 ]  . 
the optimal management of this rare histiocytic disorder is still unknown . in this case , resection of a solitary brain metastasis followed by whole brain radiation therapy yielded durable cerebral control . 
 material and methods : peripheral lymphocytes of twelve rectal cancer patients who had undergone postoperative radiochemotherapy 23 years ago were investigated for residual chromosomal damage using 24 - color fluorescence in situ hybridization ( 24color fish )  . 
all twelve patients had received a total dose of 55.8 gy in conventional fractionation of 1.8 gy and a 120 - h continuous infusion of 5 - fluorouracil ( 5 - fu ) chemotherapy ( 1 , 000 mg / m2 per day ) in the 1st and 5th week of irradiation . 
the aberration types , occurring as simple translocations , reciprocal translocations , breaks , dicentrics , inversions , rings and complex chromosomal rearrangements , did not show any specific accumulation in one or the other group either . 
 conclusion : while there was a significant amifostine - mediated clinical amelioration of normal tissue toxicity , the comparison of residual chromosomal damage 23 years after completion of radiochemotherapy was characterized by a high interindividual variation , and no equivalent difference could be detected between the two groups . 
 key words : radiation - induced chromosomal aberrations residual chromosomal damage 24 - color fish amifostine strahlenther onkol 2003 ; 179 : 4938 doi 10.1007 / s00066 - 003 - 1095 - z chromosomale residualschden nach radiochemotherapie mit und ohne amifostin , nachgewiesen durch 24 - farben - fish hintergrund : amifostin ist eine radioprotektiv wirkende substanz , die zur verringerung der akuten nebenwirkungen bei konventionell fraktionierter radiotherapie angewandt wird . 
 material und methodik : lymphozyten von zwlf patienten , die wegen eines rektumkarzinoms vor 23 jahren eine radiochemotherapie erhalten hatten , wurden mittels 24 - farben - fluoreszenz - in - situ - hybridisierungstechnik ( 24 - farben - fish ) auf chromosomale residualschden untersucht . 
alle patienten hatten eine gesamtdosis von 55 , 8 gy in einzeldosen von 1 , 8 gy sowie eine chemotherapie mit 5 - fluorouracil ( 5 - fu ) als 120 - h - dauerinfusion ( 1 , 000 mg / m2 pro tag ) in der 1 . 
sieben 1 department of radiation oncology , friedrich schiller university , jena , germany , 2 institute of human genetics and anthropology , friedrich schiller university , jena , germany , 3 department of radiation oncology , martin luther university , halle , germany . 
 ergebnisse : die auswertung der durchschnittlichen anzahl von brchen pro mitose ( b / m ) zeigte einen erhhten anteil chromosomaler residualschden sowohl in der mit amifostin ( 0 , 65 b / m [ 0 , 320 , 97 ] ) als auch in der ohne amifostin behandelten patientengruppe ( 0 , 76 b / m [ 0 , 311 , 25 ] )  . 
auerdem zeigten die aufgetretenen aberrationstypen ( einfache translokationen , reziproke translokationen , brche , dizentrische , inversionen , ringchromosomen und komplexe chromosomale rearrangements ) keine spezifische hufung in einer der beiden gruppen . 
 schlussfolgerung : whrend eine signifikante klinisch feststellbare abschwchung der normalgewebstoxizitt in der patientengruppe mit amifostin zu beobachten war , zeigte der vergleich hinsichtlich der chromosomalen residualschden 23 jahre nach abschluss der radiochemotherapie eine hohe interindividuelle variabilitt ohne einen unterschied zwischen beiden gruppen . 
 schlsselwrter : strahleninduzierte chromosomenaberrationen chromosomale residualschden 24 - farben - fish amifostin introduction material and methods amifostine , an organic thiol derivative , is a drug which protects normal tissue against radiation and some cytotoxic agents [ 26 ]  . 
moreover , it is a well - known fact that previous exposure to ionizing radiation ( radiotherapy or accidental exposure ) leads to residual chromosomal damage that can be detected in peripheral blood lymphocytes [ 24 , 10 , 12 , 13 , 28 ]  . 
 [ 9 ] , milder side effects in the acute clinical reaction to radiochemotherapy were observed in the patients with additional amifostine compared to the nonrandomized control group without amifostine . 
now , it was the aim to determine whether amifostine has an influence not only on the clinical reaction but also on the amount of residual chromosomal damage , as the latter is an expression of intrinsic radiosensitivity [ 8 , 18 ]  . 
for this purpose , 24 - color fluorescence in situ hybridization ( 24 - color fish ) was applied , using a probe mix of the 24 different human whole chromosome painting ( wcp ) probes . 
thus , nearly all possible chromosomal aberrations , such as reciprocal and nonreciprocal translocations , complex rearrangements , ring chromosomes , acentric fragments , dicentric fragments or insertions , could be detected and characterized in more detail . 
15 of them had received additional amifostine , and 15 had been treated without amifostine ; the administration of amifostine was not randomized and based on the patients preference [ 9 ]  . 
all patients had received the same radiochemotherapy regimen : a total radiation dose of 55.8 gy in conventional fractionation of 1.8 gy and a 120 - h continuous infusion of 5 - fluorouracil ( 5 - fu ) chemotherapy ( 1 , 000 mg / m2 per day ) in the 1st and 5th week of irradiation . 
seven out of twelve patients ( p1 , p2 , p4 , p5 , p7 , p8 , p11 ) had been given additional amifostine on chemotherapy days in a total dose of 500 mg ( corresponding to about 300 mg / m2 ) as short infusion immediately prior to the daily radiation fraction . 
patients of both groups ( with and without amifostine ) belonged approximately to the same age group ( mean age of the group with amifostine : 63.8 years , range 5671 years ; without amifostine : 56.6 years , range 5163 years )  . 
radiation - induced chromosomal aberrations detected by 24 - color fish was added to 9 ml rpmi 1640 medium ( including 12% fetal calf serum , 1% phytohemagglutinine , and 1% penicillin - streptomycin ) and cultured for 72 h ( 37 c )  . 
 [ 14 ] : after 72 - h incubation ( 37 c ) with the probe mix , posthybridization washes and detection , metaphase images were captured on a fluorescence microscope ( zeiss axioplan ) with suitable filter combinations ( fitc / texasred / spectrumorange / cyanine 5 / cyanine 5.5 / dapi ) using isis - software ( metasystems , altlussheim , germany )  . 
aberration types and involved chromosomes were characterized in detail and classified , as described earlier [ 14 ] , into breaks / acentric fragments , reciprocal translocations , nonreciprocal translocations , complex chromosomal rearrangements ( ccr ) , ring chromosomes , dicentrics , inversions , and insertions . 
simple translocations were defined as containing material from two chromosomes combined with one break in each chromosome ; complex rearrangements consist of at least two chromosomes with , together , three or more breaks [ 20 , 21 ]  . 
the total number of break events in each patient was summed up and divided by the number of metaphases analyzed to get the average rate of breaks per mitosis ( b / m )  . 
 the average rate of b / m , the portion of cells containing chromosomal aberrations as well as the frequency distribution of different aberration types in the group of patients treated with amifostine was compared to those treated without amifostine . 
total number of breaks observed in 100 analyzed metaphases per patient ( b / 100 mp ; light gray ) and total number of cells containing aberrations ( dark gray ) observed in each individual patient ( p1p12 ; 24 - color fish analysis )  . 
the black bar a indicates those patients treated with additional amifostine ( p1 , p5 , p2 , p7 , p4 , p8 , p11 )  . taking the average number of breaks per mitosis ( b / m ) in each of the two groups , there was no significant difference detectable in residual chromosomal damage mainly due to the high interindividual variation ( with amifostine 0.65 b / m compared to 0.76 b / m in those treated without amifostine )  . 
gesamtanzahl der in 100 metaphasen pro patient gefundenen bruchereignisse ( b / 100 mp ; hellgrau ) und gesamtanzahl der aberrationen enthaltenden zellen pro patient ( dunkelgrau ) ( p1p12 ; 24 - farben - fish - analyse )  . 
der schwarze balken a markiert die patienten , die zustzlich mit amifostin behandelt worden waren ( p1 , p5 , p2 , p7 , p4 , p8 , p11 )  . 
 containing chromosomal damage in every individual patient . in the group treated with amifostine , the average number of aberrant metaphases per 100 analyzed cells was 22.1 ( range 1332 ) versus 24.4 ( range 1335 ) in those treated without amifostine . 
if only those cells affected by aberrations were considered , each aberrant cell contained , on average , 2.9 breaks ( with amifostine ) and 3.0 breaks ( without amifostine ) , respectively . 
radiation - induced chromosomal aberrations detected by 24 - color fish vealed no specific accumulation pattern for either of the two groups ( as illustrated in figure 2 )  . 
while there was a significant difference in clinical reaction ( patients with additional amifostine had less acute skin and bowel toxicity ; for details see [ 9 ] ) , no equivalent effect could be assessed concerning residual chromosomal damage between the two groups 23 years after completion of radiochemotherapy . 
several clinical studies have demonstrated that this substance protects normal tissue and thus reduces side effects of radiation and antineoplastic chemotherapy [ 6 , 24 , 27 , 30 ]  . 
previous studies on the ability of amifostine to protect the bone marrow were mainly focussed on this clinical endpoint . chromosomal aberrations as an expression of dna damage were previously investigated in vivo only in the bone marrow of mice [ 7 ] or in human bone marrow under in vitro conditions [ 16 ]  . 
to the best of our knowledge , there is no data reported on the effect of amifostine concerning the extent of chromosomal aberrations in human blood cells under in vivo conditions . 
patients treated with additional amifostine ( p1 , p5 , p2 , p7 , p4 , p8 , p11 ) are displayed on the left side and marked with a black bar a . 
no significant differences in residual chromosomal damage could be detected between the two groups ( with / without amifostine ) with regard to a distinct accumulation of the different specified aberration types ( b : double strand breaks ; tr : reciprocal translocations ; t : translocations ; inv / r : inversions and ring chromosomes ; dic : dicentric chromosomes ; ccr : complex chromosomal rearrangements )  . 
berblick ber die unterschiedlichen aberrationstypen und absoluten - hufigkeiten , die bei den zwlf untersuchten patienten beobachtet wurden ( 100 analysierte zellen pro patient , 24 - farben - fish - analyse )  . 
die patienten , die zustzlich amifostin erhalten hatten ( p1 , p5 , p2 , p7 , p4 , p8 , p11 ) , sind auf der linken seite des diagramms dargestellt und mit einem schwarzen balken a markiert . 
hinsichtlich der chromosomalen residualschden in den beiden gruppen ( mit / ohne amifostin ) konnten keine unterschiede bezglich einer deutlichen hufung einzelner spezifischer aberrationstypen ( b : doppelstrangbrche ; tr : reziproke translokationen ; t : translokationen ; inv / r : inversionen und ringchromosomen ; dic : dizentrische ; ccr : komplexe chromosomale rearrangements ) festgestellt werden . 
radiation - induced chromosomal aberrations detected by 24 - color fish clinical difference was spotted : patients with amifostine had less acute skin and bowel toxicity than those treated without amifostine . 
 [ 9 ] that even the application of a relatively small dosage administered only over a short period of time ( twice , for 1 week each , simultaneously with the 5 - fu chemotherapy ) is sufficient to cause milder clinical side effect . 
 now , looking for a suggested chromosome - protective effect of this substance 23 years after therapy , an increased amount of residual chromosomal damage was found by 24color fish in all twelve out of 30 patients . 
the two groups with and without amifostine showed , on average , 0.65 b / m and 0.76 b / m , respectively , which is both significantly enhanced compared to a basic value of 0.000.05 b / m in nonirradiated controls observed in a previous study [ 14 ]  . 
although the main conditions except the use of amifostine were very similar in all patients ( same diagnosis and treatment scheme , age group , time interval after therapy ) , the data showed a high interindividual variation within the two groups ( figure 1 )  . 
this interindividual variation in the analysis of residual chromosomal aberrations is a well - known fact already observed by others especially in in vivo studies on tumor patients [ 12 ]  . 
as our study also comprised a relatively small number of patients ( n = 12 ) , this typical interindividual variability has quite an impact and could have masked a possible protective or modulating effect of amifostine . 
as the present study was focused on the residual chromosomal damage after partial body irradiation with maximal bone marrow protection , both studies have two different conditions and endpoints and are not directly comparable . 
at the time of our analysis 23 years after completion of radiochemotherapy , both groups had about the same average portion of aberrant cells ( 22.1% with amifostine , 24.4% without ) with a similar degree of damage and a similar distribution of stable and unstable aberrations . 
as the lymphocytes were cultured for 72 h , it has to be taken into consideration that a certain amount of analyzed cells have already performed their second mitotic division . 
this is mainly the case for so - called unstable aberrations like dicentrics , breaks , and acentric fragments . nevertheless , these kinds of aberrations have also been detected in the present study ( figure 2 )  . 
the aberration frequency of this specific translocation type alone showed a similar value and variation in both groups , as it was true for all other parameters like the b / m rate . 
moreover , stable aberrations are of clinical relevance to patients as they are assumed to be causally related to the development of a secondary neoplasia / radiation - induced leukemogenesis [ 11 , 13 ]  . 
 although the exact mechanism of action of amifostine has not fully been solved yet , several studies showed its properties to modulate the apoptotic cell death induced by chemotherapy [ 19 ] or by radiochemotherapy [ 5 ]  . 
thus , it could be speculated , that the amount of residual chromosomal damage in the amifostine - treated group is accumulated , because it prevented cells from apoptosis that would normally not have survived . 
this would lead to cells not capable of entering mitosis agahowever , studies focusing on such questions could only be performed in interphase cells e.g. , with techniques like those proposed by lemke et al . 
 regarding long - persisting residual chromosomal damage , the bystander effect has to be taken into account [ 17 ]  . this leads to indirect and delayed effects of damage , caused by radiation - induced clastogenic factors circulating in the peripheral blood . 
 an itemized analysis ( figure 2 ) of different aberration types was performed , because it is described in the literature that a specific increase ( for instance in ccr ) can indicate hypersensitivity to ionizing radiation [ 18 ]  . 
radiation - induced chromosomal aberrations detected by 24 - color fish conclusion although application of amifostine led to a reduction of clinical side effects of radiochemotherapy , no equivalent influence could be detected on the amount of residual chromosomal damage . 
 strahlentherapie und onkologie original article prognostic impact of hemoglobin level prior to radiotherapy on survival in patients with glioblastoma karel odrazka1 , jiri petera1 , tereza kohlova1 , martin dolezel1 , miloslava vaculikova1 , milan zouhar1 , vaclav malek2 , vladimir hobza2 , ivan latr2 , stanislav nemecek2 , miroslav sercl3 , pavel ryska3 , milan blaha4 , eva cermakova5 purpose : to evaluate prognostic factors in patients with glioblastoma treated with postoperative or primary radiotherapy . 
univariate analysis revealed age 55 years ( p < 0.001 ) , pre - radiotherapy hemoglobin ( hb ) level > 12 g / dl ( p = 0.009 ) , and pre - radiotherapy dose of dexamethasone 2 mg / day ( p = 0.005 ) to be associated with prolonged survival . 
at multivariate analysis , younger age ( p < 0.001 ) , higher hb level ( p = 0.002 ) , lower dose of dexamethasone ( p = 0.026 ) , and a hemispheric tumor location ( p = 0.019 ) were identified as independent prognostic factors for longer survival . 
 key words : glioblastoma radiotherapy hemoglobin strahlenther onkol 2003 ; 179 : 6159 doi 10.1007 / s00066 - 003 - 1097 - x die prognostische bedeutung der hmoglobinkonzentration vor der strahlentherapie fr die berlebenszeit von patienten mit glioblastom ziel : evaluation prognostischer faktoren bei patienten mit glioblastom , die mit postoperativer oder primrer strahlentherapie behandelt wurden . 
mittels der univariaten analyse stellten sich folgende faktoren dar , die mit einer lngeren berlebenszeit verbunden sind : ein alter 55 jahre ( p < 0 , 001 ) , eine hmoglobin - ( hb - ) konzentration zu beginn der strahlentherapie > 12 g / dl ( p = 0 , 009 ) und eine prtherapeutische dexamethasondosis 2 mg / tag ( p = 0 , 005 )  . 
die multivariate analyse ermittelte ein jngeres alter ( p < 0 , 001 ) , eine hhere hb - konzentration ( p = 0 , 002 ) , eine niedrigere dexamethasondosis ( p = 0 , 026 ) und eine hemisphrische tumorlokalisation ( p = 0.019 ) als unabhngige prognostische faktoren fr eine lngere berlebenszeit . 
die mittlere berlebenszeit bei patienten mit einer hb - konzentration > 12 g / dl betrug 12 , 1 monate , bei patienten mit einem niedrigeren blut - hb - wert da1 department of oncology and radiotherapy , 2 department of neurosurgery , 3 department of radiology , and 4 2nd department of internal medicine , charles university hospital , hradec kralove , czech republic , 5 department of medical biophysics , charles university medical school , hradec kralove , czech republic . 
however , the efficacy of irradiation is limited by the inherent radioresistance of glioma cells and the radiosensitivity of the surrounding brain tissue . focal dose escalation beyond 60 gy is feasible using advanced technologies , but the predominant failure pattern remains local [ 1 , 5 , 26 ]  . 
several other variables that determine survival were described , including presence of fits , steroid dependency , tumor location , midline shift , and extent of surgery [ 1012 , 20 , 27 ]  . 
numerous studies have consistently shown that low hemoglobin ( hb ) level is an adverse prognostic factor for the outcome of patients with various tumor types , including cervical cancer , head and neck cancer , or non - small cell lung cancer [ 17 , 18 , 32 ]  . 
unfortunately , studies on malignant gliomas rarely included serum hb level in the analysis of prognostic factors . therefore , the aim of this study was to evaluate the influence of hb level prior to radiotherapy on the survival of patients with glioblastoma in the context of other common prognostic factors . 
85 patients completed the full course of radiotherapy and only these were included in the analysis ( table 1 )  . there were 43 male ( 51% ) and 42 ( 49% ) female patients . 
the greatest tumor diameter ranged from 1 to 8 cm , with a median diameter of 5 cthe tumor originated from the right side of the brain in 44 patients ( 52% ) , while 41 patients ( 48% ) had their tumors on the left . hemispheric tumor location was identified in 67 patients ( 79% )  . 
gross total resection was performed in 15 patients ( 18% ) , 58 patients ( 68% ) had a subtotal surgical resection , and biopsy only was taken in twelve patients ( 14% )  . 
eight of these twelve patients presented with tumors not amenable to surgery , three patients were medically inoperable , and one patient refused the operation . statistics ( ( cid : 1 ) 2 - test ) was utilized to examine possible differences between specific subgroups in the distribution of other prognostic factors . 
 radiation therapy prognostic factors 73 patients ( 86% ) were given postoperative external - beam irradiation , while twelve patients ( 14% ) were primarily treated with radiotherapy after biopsy . 
the 57 patients ( 67% ) , treated between 1989 and 1997 , received whole brain irradiation ( 40 gy ) with an additional boost to the tumor area ( 20 gy )  . 
another margin of 10 mm was left between the ptv and the leaves of the multileaf collimator accounting for beam penumbra . the prescribed dose was specified to the icru point ( isocenter ) and normalized to 100% . 
younger age ( p < 0.001 ) , lower dose of dexamethasone ( p = 0.005 ) , and a higher level of serum hb ( p = 0.009 ) were associated with prolonged survival . 
intratumoral measurements of the oxygen tension have confirmed that hypoxia was associated with poor local control and survival in patients treated with irradiation for cervical and head and neck cancer [ 4 , 16 , 25 ]  . 
in an overview performed by overgaard & horsman , modification of tumor hypoxia was shown to improve the locoregional control , especially in head and neck carcinoma [ 23 ]  . 
nevertheless , a large number of trials provided evidence of an association between low serum hb levels and higher failure rate / lower survival rate in patients treated with curative radiotherapy [ 14 , 17 , 18 , 29 ]  . 
similarly , positron emission tomography with 18f - fluoromisonidazole proved to be a useful tool for assessing hypoxia in human gliomas [ 28 ]  . to overcome the presupposed hypoxia of glioma cells , studies have been performed using radiotherapy in combination with hypoxic cell modifiers . 
this is perhaps due to the exclusion of patients that did not complete the full course of radiotherapy from the analysis . conclusion we suggest that low hb level may further increase the existing intratumoral hypoxia , thus making glioblastoma even more resistant to irradiation . 
 strahlentherapie und onkologie original article carbon ion radiotherapy for chordomas and low - grade chondrosarcomas of the skull base results in 67 patients daniela schulz - ertner1 , anna nikoghosyan2 , christoph thilmann2 , thomas haberer3 , oliver jkel2 , christian karger2 , michael scholz3 , gerhard kraft3 , michael wannenmacher1 , jrgen debus1 , 2 purpose : to prospectively evaluate outcome and toxicity after carbon ion radiotherapy ( rt ) in chordomas and low - grade chondrosarcomas . 
 patients and methods : between september 1998 and december 2001 , 74 patients were treated for chordomas and chondrosarcomas with carbon ion rt at the gesellschaft fr schwerionenforschung ( gsi )  . 
seven patients reirradiated with reduced carbon ion doses after conventional rt were excluded from the analysis , leaving 67 evaluable patients ( 44 chordomas and 23 chondrosarcomas ) who received a full course of carbon ion therapy . 
the observation of tumor regressions at a dose level of 60 gye may indicate that the biological effectiveness of carbon ions in chordomas and chondrosarcomas is higher than initially estimated . 
 key words : carbon ion radiotherapy chordomas chondrosarcomas strahlenther onkol 2003 ; 179 : 598605 doi 10.1007 / s00066 - 003 - 1120 - 2 kohlenstoffionentherapie von chordomen und niedriggradigen chondrosarkomen der schdelbasis . 
 1 department of clinical radiology , university of heidelberg , germany , 2 german cancer research center ( dkfz ) , heidelberg , germany , 3 department of biophysics , german ion research center ( gsi ) , darmstadt , germany . 
carbon ion rt for chordomas and chondrosarcomas schlussfolgerungen : die daten belegen die klinische effektivitt und sicherheit der kohlenstoffionentherapie mit einem gescannten kohlenstoffionenstrahl bei patienten mit chordomen und chondrosarkomen der schdelbasis . 
die beobachtung von tumorregressionen bei einer dosis von 60 gye weist darauf hin , dass die biologische wirksamkeit der kohlenstoffionen bei chordomen und chondrosarkomen hher sein knnte als ursprnglich angenommen . 
complete resection is exceptional , and recurrence rates after surgery alone are high [ 12 ]  . therefore , high - dose radiotherapy ( rt ) is generally recommended after incomplete resection [ 5 , 26 ]  . 
there is a clear dose - response relationship with improved local control rates after tumor doses > 65 gy first described by pearlman & fried - man [ 32 ]  . 
conformal rt with photons utilizing stereotactic target localization techniques allows moderate dose escalation in some of the patients , but dose prescription is still limited to 6065 gy in most patients due to limited capabilities of photons regarding dose conformation . 
in the treatment of chordomas , doses up to 80 gy might be applied with proton rt at acceptable toxicity rates . while modern photon rt techniques like fractionated stereotactic rt yield local control rates of up to 50% at 5 years in chordomas of the skull base [ 8 ] , proton rt yields local control rates in the range of 65% at 5 years [ 27 ]  . 
 initial results of this trial after treatment of 37 patients already indicated that carbon ion therapy yields results at least comparable to proton rt [ 6 , 39 ]  . 
 patients and methods between august 1998 and december 2001 , 74 patients with skull base chordomas and low - grade chondrosarcomas were treated with carbon ions at gsi within a prospective clinical phase i / ii trial . 
seven patients who received a reduced carbon ion dose after previous irradiation with photons or protons were excluded from this analysis , leaving 67 evaluable patients who received a full course of carbon ion rt with curative intent . 
mean tumor volumes determined from the maximum diameters on treatment planning mri scans were 49 ml ( range 0.6594 ml ) in chordomas and 23 ml ( range 1.6125 ml ) in low - grade chondrosarcomas . 
carbon ion rt for chordomas and chondrosarcomas ceived three - dimensional treatment planning based on ct and mri scans with a slice thickness of 3 mthe stereotactic coordinates of the target point were obtained using a stereotactic localization system [ 36 ]  . 
the gross tumor volume ( gtv ) was defined as hyperintensity lesion on t2w mri plus a safety margin of 1 mm , the clinical target volume ( ctv ) included the gtv and suspected subclinical disease based on clinical risk estimation plus a safety margin of 12 mm for possible patient misalignment and uncertainties in the geometric precision of the dose distribution . 
treatment planning was performed using the in - house developed treatment planning programs voxelplan [ 11 , 36 ] and trip [ 23 , 24 ] and included biological plan optimization taking into account the rbe which varies across the irradiated volume [ 22 ]  . 
 details of the planning procedure as well as the quality assurance program have been previously described and will be outlined only briefly [ 16 , 18 , 23 , 24 , 37 ]  . 
in a second step , the distribution of the absorbed dose is optimized to yield a homogeneous biologically effective dose distribution in the target volume taking into account the rbe of the carbon ions . 
the rbe was calculated for each voxel using the local effect model ( lem ) developed by scholz & kraft [ 38 ]  . currently , the calculation of the rbe is based on the biological endpoint induction of late effects in normal brain tissue . the rbe calculation results in a mean rbe of about 3 within the target volume . 
 follow - up and statistical analysis all patients had follow - up examinations performed 6 weeks after rt , in 3to 6 - month intervals during the first 2 years , and annually thereafter . 
 radiation - induced reactions occurring during rt or within the first 6 months after rt were scored as acute reactions . local control was defined as absence of clinical or radiographic signs of tumor enlargement . 
the center of the brain stem received < 50 gye , however , very small volumes of < 1 cm3 at the surface were allowed to receive up to 60 gye . 
thick red line : target volume ; thick green line : brain stem ; thick blue line : optic chiasm ; red area : at least 90% of the prescribed dose ; yellow area : 6090% of the prescibed dose ; green area : 5060% of the prescribed dose ; blue area : 1050% of the prescibed dose . 
six patients showed improvement of their abducent nerve paresis , visual acuity improved in two patients , pareses of the cranial nerves vii and xii improved in two patients , respectively . 
 vage rt with another full course of carbon ion rt was delivered in this patient after subtotal resection of the recurrence , since almost no dose had been applied in this region during the first course of carbon ion rt . 
actuarial local control in 44 patients with chordomas and 23 patients with chondrosarcomas treated with carbon ions by histology ; chordomas : dotted line , chondrosarcomas : solid line ( kaplanmeier curve )  . 
aktuarische lokale kontrollwahrscheinlichkeit in abhngigkeit von der histologie bei 44 patienten mit chordomen und 23 patienten mit chondrosarkomen ; chordome : gestrichelte linie , chondrosarkome : durchgezogene linie ( kaplan - meier - kurve )  . 
 toxicity acute toxicity was mild and included minor skin reactions ctci in six patients , one patient developed a skin reaction ctcii , 60 patients did not show any skin erythema . 
three patients showed contrast - enhancing lesions within the temporal lobes on t1w mri scans at 10 , 12 , and 14 months after rt with target doses of 60 , 70 , and 60 gye , respectively . 
another patient with impingement of the optic tract by tumor developed homonymous hemianopsia caused by a contrast - enhancing lesion in the region of the optic tract ( ctciii )  . 
the third patient showed neurosensory hearing impairment after treatment of a chondrosarcoma of the petrous bone , but useful hearing was preserved without the need for a hearing aid ( ctcii )  . 
 discussion our data indicate that carbon ion rt is highly effective in the treatment of chordomas and low - grade chondrosarcomas . using carbon ion rt , high cure rates can be obtained , while severe radiation - induced side effects are minimized . 
reported a 5 - year progressionfree survival rate of 23% in 48 patients treated with conventional photon rt with doses ranging from 20 to 62 gy [ 4 ]  . 
treated 15 patients with chordomas and chondrosarcomas with gamma - knife radiosurgery using maximum single tumor doses between 24 and 40 gy ( mean 36 gy )  . they selected only patients with small tumors ( average tumor diameter < 30 mm )  . 
the temporal lobe damage rate was determined for a subgroup of 96 chordoma and chondrosarcoma patients treated at the mgh between 1984 and 1993 within a prospective dose - finding study . in this study , the patients were randomized to receive 66.6 or 72 gye of proton and photon irradiation with conventional fractionation ( 1.8 cge / day , five fractions per week )  . 
treated 58 patients with chordomas and chondrosarcomas of the skull base with proton rt at the loma linda university medical center ( usa ) between march 1992 and january 1998 . 
reported the outcome in 18 children with base of skull or cervical spine chordomas treated with mixed photon and 160 - mev proton beams at the mgh in boston ( usa ) between 1981 and 1990 . 
cervical spine tumors had a worse overall and disease - free survival compared to skull base tumors . late side effects included brain necrosis in one , impairment of hearing in three , and pituitary insufficiency in two out of 18 patients [ 1 ]  . 
reported the results of combined photon and proton rt at the centre de protonthrapie dorsay in 45 patients with chordomas and chondrosarcomas of the skull base treated between december 1995 and december 1998 . 
 although treatment results after combined photon and proton rt have never been compared to proton rt alone in a randomized manner , the use of protons alone appears to be favorable from the theoretical point of view , as higher tumor doses might be delivered at the same toxicity level . 
the physical selectivity of proton rt might be compensated in part by new developments in the field of photon rt which enable inverse treatment planning and intensity - modulated photon rt . using these modern photon techniques , dose distributions might be achieved that are almost comparable to proton rt . on the other hand , inverse treatment planning and intensity modulation for protons will be implemented at some centers in the near future as well . 
reported on 45 patients with chordomas and chondrosarcomas treated between 1977 and 1986 with a median tumor dose of 65 gye helium ions at the lawrence berkeley laboratory ( lbl ) in berkeley , usa . 
for patients with residual tumors measuring < 20 ml and for tumors with > 20 ml , 5 - year actuarial local control rates were 80% and 33% , respectively [ 2 ]  . 
 our data suggest similar effectiveness of carbon ion rt when comparing the results obtained in our trial with the results after proton rt , however , at another target dose level . assuming isoeffectiveness of 60 gye of carbon ions compared to 7080 gye of protons , the rbe for these tumors might be estimated to be > 3 using carbon ions . 
in fact , toxicity can be reduced not only because of the radiobiological advantage of carbon ions but is further decreased due to the use of the raster scan technique that represents an intensity - modulated beam delivery systeclinically observed toxicity is very mild and in accordance with the expectations based on our radiobiological model that provides the basis for biological plan optimization . the effectiveness of carbon ion rt for chordomas and lowgrade chondrosarcomas is underlined by the high rate of partial remissions of 31% for chordomas and 17% for chondrosarcomas . 
patients with spinal chordomas and lowgrade chondrosarcomas might be good candidates for carbon ion rt as well , although metal implants after surgery might prevent accurate target definition [ 33 ] and cause artifacts on the planning ct that influence carbon ion treatment planning . conclusions high local control rates can be achieved with low toxicity by the application of carbon ion rt using the intensity - controlled raster scan technique . 
carbon ion rt for chordomas and chondrosarcomas strahlentherapie und onkologie original article oxygenation status of cervical carcinomas before and during spinal anesthesia for application of brachytherapy hajo dirk weitmann1 , burkhard gustorff2 , peter vaupel3 , tomas hendrik knocke1 , richard ptter1 background and purpose : to date , no information is available concerning the impact of spinal anesthesia on the oxygenation status of carcinomas of the uterine cervix . 
 patients and methods : in ten patients with cervical carcinoma who received spinal anesthesia for a first application of brachytherapy , intratumoral po2 measurements ( po2 histography system , eppendorf - netheler - hinz , hamburg , germany ) were performed . 
patients breathed room air spontaneously . for further evaluation , all intratumoral po2 values were pooled , and overall median po2 values and fractions of hypoxic po2 values 5 mmhg were calculated . 
 results : there were no significant changes of systemic parameters , median subcutaneous po2 values , median intratumoral po2 values , and the fractions of hypoxic po2values 5 mmhg in the tumor upon administration of spinal anesthesia . 
the variability of measured po2 values increased during spinal anesthesia , although substantial changes in the oxygenation status were only seen in individual cases ( n = 2 )  . 
 conclusion : this study shows for the first time that the oxygenation status of cervical carcinomas , in general , is not influenced by spinal anesthesia prior to application of brachytherapy . 
at the same time , since no substantial changes in tumor oxygenation were observed , spinal anesthesia should not affect the o2 - related efficacy of high - dose - rate brachytherapy . 
 key words : tumor oxygenation cervical carcinoma spinal anesthesia po2 histography strahlenther onkol 2003 ; 179 : 63340 doi 10.1007 / s00066 - 003 - 1060 - x oxygenierung von zervixkarzinomen vor und unter spinalansthesie fr die brachytherapie fragestellung und ziel : diese studie untersucht erstmals den einfluss einer spinalansthesie auf den oygenierungsstatus von zervixkarzinomen . 
 patienten und methodik : bei zehn patientinnen mit zervixkarzinom , die eine spinalansthesie fr die erste brachytherapieapplikation erhielten , wurden intratumorale po2 - messungen mit dem po2 - histographie - system ( eppendorf - netheler - hinz , hamburg ) durchgefhrt . 
die patientinnen atmeten spontan raumluzur weiteren auswertung wurden alle intratumoralen po2 - werte gepoolt und mediane po2 - werte sowie die hypoxische fraktion der intratumoralen po2 - werte 5 mmhg bestimmt . 
ebenso wurden mediane po2 - werte fr die subkutis berechnet . ergebnisse : signifikante nderungen der gemessenen vitalparameter , medianen po2 - werte in der subkutis und im tumor sowie der hypoxischen fraktion 5 mmhg in den zervixkarzinomen wurden nicht festgestellt . 
 schlsselwrter : tumoroxygenierung zervixkarzinom spinalansthesie po2 - histographie 1 department of radiotherapy and radiobiology , university of vienna , general hospital of vienna , austria , 2 department of anesthesia and general intensive care b , university of vienna , general hospital of vienna , austria , 3 institute of physiology and pathophysiology , university of mainz , germany . 
oxygenation status of cercical carcinomas before and during spinal anesthesia introduction in vivo measurement of tumor oxygenation in the clinical setting can be performed by means of polarographic needle po2 histography . 
in comparison with the oxygen distributions found in normal tissues , in solid tumors a left shift of the distribution curve of measured po2 values ( po2 histogram ) and hypoxic regions was noticed . 
 there is good evidence that the oxygenation status of certain types of human tumors plays an important role in determining the therapeutic response of these tumors [ 14 , 15 , 29 , 30 ]  . 
in the treatment of carcinoma of the uterine cervix by both irradiation and surgery , tumors with a poorer oxygenation or a larger hypoxic fraction have a worse treatment outcome , and both the local control and rate of distant metastases are influenced by the oxygenation status [ 12 , 14 , 15 , 21 , 23 , 43 ]  . tissue hypoxia , which results from an inadequate oxygen supply , compromises biological functions [ 19 , 20 ]  . 
another effect of hypoxia in cervical cancers is the expression of hypoxia - inducible factor ( hif - ) 1 which induces angiogenesis via overexpression of vascular endothelial growth factor ( vegf ) [ 2 , 35 ]  . 
the extent of neoangiogenesis , as assessed by determination of microvessel density , is influenced by vegf expression and is considered to support progression of cervical cancer [ 7 , 32 ]  . 
 [ 19 ] found that hypoxic cervical cancers with low apoptotic index have a high probability of lymphatic spread and of recurrence despite adjuvant treatment with radioor chemotherapy in addition to radical surgery . 
in patients undergoing general anesthesia using inhalational anesthetics , consideration should also be given to the fact that these agents can falsify the po2 readings of the o2 - sensitive cathode of the probe [ 41 ]  . 
however , po2 values measured in cervical carcinomas were found to be lower during propofol anesthesia with oxygen - enriched ( 40% o2 ) respiratory support [ 18 , 42 ]  . an alternative to general anesthesia is spinal anesthesia , which provides both analgesia , motor block and sympathetic block of the lower extremities . 
 patients and methods between december 1998 and august 2000 , po2 measurements ( po2 histography system , eppendorf - netheler - hinz , hamburg , germany ) were performed in ten patients with cervical carcinoma who received spinal anesthesia for a first application of brachytherapy . 
inclusion criteria were : tumor stage ib or ii , no vaginal bleeding , karnofsky performance status of 90100% , minimum tumor diameter of 2 cm , maximum tumor diameter of 5 cm , intracervical brachytherapy as first part of radiation treatment , no contraindications to spinal anesthesia , american society of anesthesiologists status 13 . 
the patients received high - dose - rate ( hdr ) brachytherapy with weekly applications of 7 gy per fraction in point a [ 23 , 33 , 39 ]  . 
 spinal anesthesia and po2 measurements prior to po2 measurements , a spinal catheter ( g 28 , portex , uk ) was inserted in the third lumbar interspace using 2 ml mepivacaine 1% for local anesthesia of the sk 500 ml ringers lactate was infused intravenously . 
in case of substantial decreases in mean arterial blood pressure ( > 20% from baseline ) or arterial hbo2 saturation ( < 90% ) , patients were excluded from the study and treated appropriately . 
ac : adenokarzinom ; asc : adenosquamses karzinom ; chb : hmoglobinkonzentration ; n : anzahl der durchgefhrten po2 - messungen ; scc : plattenepithelkarzino patient age ( years ) stage tumor tumor histology grade tumor ( figo ) ( g / dl ) n before spinal anesthesia anesthesia n during spinal clinical tumor diameter ( cm ) and the vaginal temperature measured . after introduction of specula into the vagina , the tumor was inspected and the cervical os localized . 
to provide a guiding structure for the electrode tracks , two thin catheters were introduced into the macroscopically visible tumor in the cervix ( 6 - oclock and 12 - oclock position )  . 
the vaginal temperature was measured , and 30 min after the last application of bupivacaine a second series of intratumoral po2 measurements was performed in the same way as the first series using tracks directly adjacent to the initial ones . 
 evaluation and statistics for further evaluation , all intratumoral po2 values were pooled , and overall median po2 values and fractions of hypoxic po2 values 5 mm hg were calculated . 
according to the figo classification , the tumors of five patients were classified as stage iib , three as stage iia , and two as stage ib ( table 1 )  . eight patients had squamous cell carcinoma of the uterine cervix , one adenocarcinoma , and one adenosquamous carcinoma . 
heart rate ranged from 55 to 80 beats per minute ( mean : 70 bpm ; median : 72 bpm ) before spinal anesthesia , and from 55 to 75 bpm ( mean : 66 bpm ; median : 68 bpm ) during spinal anesthesia ( figure 1a )  . 
mean arterial blood pressure varied between 78 and 118 mm hg ( mean : 102 mm hg ; median : 104 mm hg ) before spinal anesthesia , and between 78 and 113 mm hg ( mean : 98 mm hg ; median : 102 mm hg ) during spinal anesthesia ( figure 1b )  . 
arterial hbo2 saturation ranged from 96 to 100% ( mean : 97% ; median : 97% ) before spinal anesthesia , and from 95 to 100% ( mean : 98% ; median : 98% ) during spinal anesthesia ( figure 1c )  . 
 po2 measurements in the subcutis there were no significant changes of median po2 values in the subcutis upon administration of spinal anesthesia ( figure 3 )  . before spinal anesthesia , median po2 values ranged from 33 to 85 mmhg ( mean : 63 mmhg ; median : 66 mmhg )  . 
 mittelwert ( ( cid : 1 ) ) , die whisker reichen von minimum bis maximum , die box gibt 25% - perzentile , median und 75% - perzentile an . 
oxygenation status of cercical carcinomas before and during spinal anesthesia median po2 values decreased in four patients and increased in three , and in two patients there was no change during spinal anesthesia compared to baseline values . 
the differences between median po2 values before and during spinal anesthesia ranged from 29 mm hg in patient #4 to + 9 mm hg in patient #8 ( mean : 4 mm hg ; median : 1 mm hg )  . 
 intratumoral po2 measurements on comparison of measurements before and during spinal anesthesia , there were no significant changes in median po2values ( figure 4a ) and the fractions of hypoxic po2 values 5 mm hg in the tumor ( figure 4b )  . 
the differences between median po2 values before and during spinal anesthesia ranged from 10 mm hg in patient #9 to + 17 mm hg in patient #2 ( mean : + 2 mm hg ; median : + 2 mm hg )  . 
 the fractions of hypoxic po2 values 5 mm hg in the tumor ( hf5 ) ranged from 0 to 61% ( mean : 15% ; median : 1% ) before spinal anesthesia , and from 0 to 100% ( mean : 19% ; median : 0% ) during spinal anesthesia ( figure 4b )  . 
the differences ranged from 28% in patient #7 to + 39% in patient #3 ( mean : + 4% ; median : 0% )  . here again , the variability of the po2 values increased during spinal anesthesia . 
 tumor oxygenation in the absence of anesthesia in comparison with the data of patients at our department showing even higher tumor stages , trends to a higher mean and median of the median intratumoral po2 values and to lowfigures 4a and 4b . 
 authors and year number patients tumor stages ( figo ) patients ( years ) anesthesia and o2 supplementation range of mean / median medians ( mmhg ) medians ( mmhg ) range of hf2.5 mean / median of hf2.5 range of hf5 mean / median of hf5 hckel et al . 
1999 [ 5 ] 2877 iibiva 2194 50 / 54 2395 60 / 60 shot spinal anesthesia may lead to a substantial decrease in mean arterial blood pressure due to sympathetic block . 
however , a particular advantage of the spinal catheter anesthesia technique used in this study is that changes in mean arterial blood pressure can be avoided by means of an incremental titration of the anesthetic . 
general anesthesia is performed with o2 - enriched respiratory support . in this study , regional anesthesia did not impact respiration , since the upper anesthetic level did not exceed t8 in any of the patients . 
 impact of general anesthesia on the oxygenation status of cervical carcinomas only few data are available concerning po2 histography in cervical carcinomas during general anesthesia ( table 2 )  . 
some groups have reported incomplete data about their method of general anesthesia or inspiratory o2 supply , and sometimes comparable information about raw data is lacking [ 13 , 26 , 40 ]  . 
during general anesthesia with propofol and n2o and 40% oxygen supply , the measured mean and median hypoxic fractions ( < 2.5 or < 5 mm hg ) are higher whereas the ranges of hypoxic fractions ( < 2.5 or < 5 mm hg ) are stable ( table 2 )  . 
however , the use of anesthesia during po2 measurements was generally discouraged , because modified tumor oxygenation owing to cardiovascular effects of anesthesia had been demonstrated in animal experiments [ 22 , 37 ]  . 
patients usually breathe room air during po2 measurements , because it has been shown that increased inspiratory o2 concentrations may increase the mean tumor po2 , although at the same time there appears to be a lesser effect on the fraction of po2 measurements that are profoundly hypoxic [ 8 ]  . 
despite the use of general anesthesia during the studies , the distribution of hypoxic versus oxygenated tumors ( defined either by the median po2 or the hypoxic fraction ) is very similar to that measured by others in conscious patients breathing room air [ 12 ]  . 
an earlier study comparing intratumoral po2 measurements taken before and during propofol anesthesia found no difference in hypoxic fractions , although lower median po2 values were noticed [ 40 ]  . 
the heterogeneity in individual oxygen tension measurements within a tumor does not preclude the use of electrode measurements as a prognostic tool provided a sufficient number of tracks and measurements are taken so that the variation within tumors is minimized compared to the heterogeneity between tumors [ 10 , 12 , 17 , 45 ]  . 
haslinger , technician at the division of radiobiology , department of radiotherapy and radiobiology ( university of vienna , austria ) , for her practical assistance in the po2 measurements and d . 
during general anesthesia , only small and negligible changes of the rectal and intratumoral temperatures have been reported , and the temperature measured in the tumor periphery and tumor center did not differ from the rectal temperature [ 40 ]  . 
 patients clinical data tumor stages and clinical tumor diameter reported here are substantially different to our patient group investigated earlier [ 33 ] because the comparison of po2 values was only performed in patients starting their treatment course with intracervical brachytherapy . 
the histopathologic grading of the tumors in this series with only one patient having a grade 3 tumor is lower than in the patients undergoing po2 histography at our department with 21 out of 51 patients having a grade 3 tumor [ 23 ]  . 
however , the influence of spinal anesthesia on the intratumoral oxygenation status will not be compromised by the differences between the patients in this series and in the preceding study [ 23 ] , since tumor oxygenation is independent of clinical tumor size , stage , histology and histopathologic grade [ 17 , 18 , 44 ]  . 
age distribution , hemoglobin concentrations , and histopathologic tumor types of the patients in this series are similar to those found in the group of patients treated at our department for cervical cancer [ 33 ]  . 
the variability of measured po2 values increased during spinal anesthesia , although substantial changes in the oxygenation status were only seen in individual cases ( n = 2 )  . 
 strahlentherapie und onkologie review article current and future strategies in radiotherapy of childhood low - grade glioma of the brain part ii : treatment - related late toxicity rolf - dieter kortmann1 , beate timmermann1 , roger e . 
gnekow4 , karin dieckmann5 , sylvia kay1 , michael bamberg1 background : for more than 60 years , radiation therapy has been an integral part in the management of childhood low - grade glioma . 
 material and methods : studies on the use of radiation therapy in children with low - grade glioma were systematically reviewed for data on radiotherapy - induced side effects on brain parenchyma , endocrine dysfunction , growth retardation , neurocognitive dysfunction , vasculopathy , and secondary neoplasms . 
past reports included only retrospective series from the 1930s to present days , a time during which treatment policies and radiation techniques widely varied and considerably changed in recent years . 
in spite of these shortcomings and often conflicting observations , it appears that especially younger children and children with neurofibromatosis ( nf ) are at risk of endocrinopathies in terms of growth retardation and developmental abnormalities , as well as neurocognitive dysfunction expressed as problems in the psychosocial environment such as in education and occupation . 
young children with nf appear to have an increased risk of vasculopathies . 33 cases of moyamoya disease were found ( preferably in the very young ) , 18 of whom were nf - positive . 
other cerebrovascular accidents ( 24 cases , of whom 14 were nf - positive ) and secondary neoplasms ( 15 cases , of whom only five occurred in field four were high - grade astrocytomas ) are a rare condition . 
 conclusions : more studies and clear definitions of clinical endpoints such as neurocognitive and endocrinological outcome are needed in order to clarify the impact of radiation therapy on the risk of late sequelae . 
these information and the contribution of tumor , surgery and chemotherapy will help to define the role of radiation therapy in the future management of childhood low - grade glioma and whether the use of highly sophisticated and expensive treatment techniques is justifiable . 
the recently initiated prospective study of the apro ( pediatric radiooncology working party ) on documentation of dose prescription to organs at risk and the network of the gpoh to explore late effects as well as the forthcoming prospective siop / gpoh ( international society of pediatric oncology / german society of pediatric oncology and hematology ) lgg 2003 trial are addressing these issues . 
 key words : children toxicity late effects radiation therapy low - grade glioma strahlenther onkol 2003 ; 179 : 58597 doi 10.1007 / s00066 - 003 - 8104 - 0 aktuelle und zuknftige strategien bei der bestrahlung von niedrigmalignen gliomen des gehirns im kindesalter . 
 1 department of radiooncology , university of tbingen , germany , 2 radiotherapy department , cookridge hospital , leeds , united kingdom , 3 department of radiotherapy , padua general hospital , italy , 4 childrens hospital augsburg , germany , 5 department of radiooncology , general hospital vienna , austria . received : october 16 , 2002 ; accepted : may 6 , 2003 strahlenther onkol 2003 no . 
radiotherapy of childhood low - grade glioma part ii material und methodik : studien ber die anwendung von radiotherapie bei niedrigmalignen gliomen im kindesalter wurden systematisch analysiert im hinblick auf daten bezglich strahlentherapieinduzierter sptfolgen im hirnparenchym , endokriner funktion , wachstum und entwicklung , neurokognitiver funktion , gefvernderungen und zweittumoren . 
zurckliegende berichte schlossen nur retrospektive serien der 30er jahre bis heute ein , also eine zeit , in der sich behandlungsrichtlinien und strahlentherapietechniken erheblich unterschieden und sich in jngster zeit deutlich nderten . 
trotz dieser einschrnkungen und hufig widersprchlicher beobachtungen scheint es , als wiesen insbesondere jngere kinder und kinder mit neurofibromatose ( nf ) ein besonderes risiko fr endokrinologische strungen in form von wachstumsverzgerung und entwicklungsstrungen ebenso wie fr neurokognitive dysfunktionen , ausgedrckt als probleme in der psychosozialen umgebung wie erziehung , ausbildung und beruf , auf . 
andere zerebrovaskulre ereignisse ( 24 flle , davon 14 nf - positiv ) und zweittumoren ( 15 flle , von denen fnf innerhalb der bestrahlungsfelder auftraten vier waren hochmaligne astrozytome ) sind selten . 
 schlussfolgerungen : weitere prospektive studien und eine klare definition klinischer endpunkte wie neurokognitives und endokrinologisches behandlungsergebnis sind notwendig , um den einfluss der strahlentherapie auf das risiko fr therapiefolgen abzuklren . 
diese informationen und der beitrag von tumor , operation und chemotherapie werden dazu dienen , die rolle der strahlentherapie in zuknftigen behandlungsstrategien zu definieren , und klren helfen , ob die anwendung hochprziser und aufwendiger bestrahlungstechniken gerechtfertigt ist . 
die krzlich initiierte prospektive studie der apro ( arbeitsgemeinschaft pdiatrische radioonkologie ) zur dokumentation von dosisverschreibungen innerhalb von risikoorganen und das kompetenznetzwerk pdiatrische onkologie der gpoh zur untersuchung von sptfolgen befassen sich ebenso wie die in vorbereitung befindliche siop / gpoh ( international society of pediatric oncology / gesellschaft fr pdiatrische onkologie und hmatologie - ) lgg - 2003 - studie mit diesen themen . 
 schlsselwrter : kinder nebenwirkungen sptfolgen strahlentherapie niedrigmaligne gliome introduction children harboring a low - grade glioma of the supratentorial midline , at hemispheric and cerebellar sites show an excellent prognosis with 10and 20 - year overall survival rates often in excess of 80% . 
resection is the treatment of choice , if location and extent of disease permit aggressive surgery , followed by surveillance , radiotherapy or , recently , chemotherapy [ 24 , 36 , 67 ]  . 
however , data on late effects in the literature are difficult to interpret , and the impact on the selection of treatment modality with respect to age , prognostic factors and risk factors to develop late effects is largely unknown [ 39 , 59 , 70 ]  . 
 the recognition and importance of radiation - induced sequelae have stimulated investigation of alternative treatment approaches , especially the introduction of modern treatment techniques which have the potential to limit the high - dose regions to the tumor itself , thereby reducing the dose to surrounding normal tissue . 
today , low - grade glioma are therefore a challenging issue for the radiooncologist , because the use of modern technologies would ideally lead to a decrease in long - term toxicity while maintaining or even improving the overall outcome . 
the literature was reviewed with respect to changes in brain parenchyma , endocrine dysfunction , growth retardation , neurocognitive dysfunction , vascular changes , and radiation - induced secondary neoplasms . 
 effects on brain parenchyma postradiation changes include a wide spectrum of abnormalities from subclinical changes detectable only by mri to focal neurologic deficits and intellectual impairment due to brain necrosis or diffuse white matter injury , respectively . 
it appears , that all changes are likely to result from complex alterations within several functional compartments with at least four contributing factors : damage to vessel structures , deletion of oligodendrocyte progenitor cells and mature oligodendrostrahlenther onkol 2003 no . 
radiotherapy of childhood low - grade glioma part ii cytes , deletion of neural stem cell population in the hippocampus , cerebellum and cortex , and , finally , generalized alterations of cytokine expression [ 7 ]  . 
 necrosis of brain parenchyma radiation necrosis is a function of total dose and fraction size with threshold doses of approximately 45 gy in ten fractions , 60 gy in 35 fractions , and 70 gy in 60 fractions , respectively [ 14 , 62 ]  . 
with conventional fractionation schedules of 1.82.0 gy / day , total doses up to 54 gy , usually applied in lowgrade glioma , are well tolerated without the risk of necrosis . 
at approximately 6 months , the morbidity was 16% , and neurologic symptoms occurred in children with tumors involving the brain stewhile only one child had a persisting neurologic deficit , marginal restriction of upward gaze , without functional significance , three children had imaging evidence of peritumoral edema causing the morbidity . 
all but one patient had normal or stable neurologic examination . it can be concluded that these asymptomatic mri changes are common in children with low - grade astrocytomas undergoing conventional fractionated radiation therapy . 
due to the high local dose , a circumscribed area of radionecrosis is a constant feature which spreads from the center of the implant to the periphery within weeks [ 41 ]  . 
 diffuse changes of white matter on imaging ( leukoencephalopathy ) diffuse white matter changes on imaging often labeled as leukoencephalopathy is a well - known phenomenon after whole brain irradiation for childhood leukemia . 
although some authors reported conflicting results , it is assumed that the clinical counterpart of diffuse white matter changes is a decline in neurocognitive function , which essentially depends on age at treatment and concomitant application of methotrexate and dose prescription as low as 1824 gy [ 44 , 46 , 47 , 59 ]  . changes on imaging , however , do not appear to correlate with neurocognitive dysfunction [ 61 ]  . 
diffuse changes of brain parenchyma as detected by imaging in low - grade glioma are a difficult issue and reports are scarce , although large treatment portals encompassing a large volume of normal brain tissue , even whole brain irradiation , with markedly higher doses have been used in past series . 
 neurocognitive dysfunction / behavioral changes the risk of neurocognitive dysfunction and changes in behavior is an important issue in the management of low - grade glioma , as quality of life may be severely compromised [ 10 , 17 , 72 ]  . 
they observed obvious difficulties in 15 children that necessitated removal from regular classes and / or placement in a special education program and , automatically , led to an inability to work outside a sheltered environment . 
 [ 13 ] noted in a series of 65 patients , 54 being treated with radiotherapy , that 18 were severely intellectually disabled , most of whom underwent radiotherapy at a median age of 4 years . 
 [ 67 ] retrospectively reviewed 33 patients who were conservatively treated with surgery and subsequently received radiotherapy , if 5 years , or chemotherapy , if < 5 years of age . 
at a mean follow - up of 10.9 years from diagnosis , 16 of 28 children ( 57% ) were in school or had completed schooling with regular academic achievements . 
 [ 34 ] reported that no patient in their series , treated with protons , had a drop of > 10% in quality of life assessment on lansky performance scale . 
in four cases of supratentorial lesions , epilepsy was present , in posterior fossa tumors three cases with ataxia , two with paresis of the facial nerve , one of whom also had hypacusis and anstrahlenther onkol 2003 no . 
 [ 71 ] noted , in their series of 21 patients , one child with seizures and one with neurologic deficits at last follow - up , horwich & bloom [ 33 ] one case with epilepsy and one case with hemiparesis . 
 endocrine dysfunction endocrine dysfunction may arise as a consequence of tumor or surgical and / or radiotherapeutic approach , particularly in glioma of the supratentorial midline ( table 1 )  . 
 in many series , endocrinological disorders were noted at time of presentation in tumors of the supratentorial midline indicating that tumor growth and infiltration of functionally important areas are a causative factor . 
five patients had precocious puberty before radiotherapy , and no additional case was observed during follow - up , although large treatment portals , even craniospinal irradiation , had been performed in some cases . 
 [ 5 ] including children and young adults with optic glioma , 21 of 57 patients ( 37% ) had endocrinological disorders at last follow - up , however , in 14 cases deficits were present at time of diagnosis . 
 [ 29 ] performed a detailed endocrinological workup during follow - up investigations and noted only four of 25 cases prior to surgery and radiotherapy . the variation of different endocrinopathies was high , with a preponderance of growth hormone deficiency in ten patients . other authors could confirm the high incidence of disorders following treatment [ 11 , 23 , 69 ] ( table 1 )  . 
the results of this analysis showed that endocrinopathies , including growth hormone deficiency , diabetes insipidus , precocious puberty , and testosterone deficiency , may be the effect of tumor , surgery and chemotherapy and cannot be attributed solely to the effects of radiation , even at the age < 5 years . 
 in an identical setting in which chemotherapy was applied as first - line treatment in younger and radiotherapy in older children ( working group of philadelphia [ 50 ] ) , similar observations were made [ 67 ]  . 
however , the specific cause of endocrinopathy could not be determined from the series , and it is remarkable that two of the four patients who did not receive radiation treatment did require endocrine replacement indicating that tumor , radical surgery , and possibly chemotherapy are important contributing factors . 
initial endocrinological status was not assessed . deficiencies were observed after all treatment modalities in a similar manner suggesting that tumor , surgery , radiotherapy , and chemotherapy possess an impact on the risk of developing endocrinological disorders in an comparable way ( table 1 )  . 
 [ 18 ] used conformal radiotherapy in glioma of the visual pathway in ten patients . four of them had disorders at diagnosis , and no new case was strahlenther onkol 2003 no . 
 [ 1 ] investigated growth hormone deficiency caused by cranial irradiation during childhood in cohorts of 18 , 24 , 3040 , and 4560 gy ( optic glioma )  . 
peak growth hormone levels were modeled as a function of time after radiotherapy and volume of the hypothalamus receiving a dose within the specified intervals of 020 gy , 2040 gy , and 4060 gy . 
the effects appeared to depend on hypothalamic dose - volume relationship and may be predicted on the basis of a linear model that sums the effects of the entire distribution of dose . 
 growth retardation , however , without influence of irradiation , can be enhanced by chemotherapy as observed in an analysis of long - term survivors of childhood cancer [ 68 ]  . 
the addition of vincristine , an agent frequently used in low - grade glioma , was a significant factor affecting growth in 51 children . ogilvy - stuart & shalet [ 48 ] noted , in their analysis , that the replacement therapy with growth hormone inadequately prevents radiation - induced growth retardation and that the addition of chemotherapy to cranial irradiation is an important contributing factor for loss in expected stature as compared to radiotherapy alone . 
radiation - induced alterations of vasculature are complex and suspected to consist in an initial progressive loss of endothelia with subsequent formation of thrombi , which is followed by an abnormal endothelial proliferation with concomitant thickening of basement membranes . 
the time interval between treatment and onset of symptoms or diagnosis of changes , respectively , varies widely and is reported to range between a few months and > 10 years ( table 1 )  . 
in total , 32 cases of moyamoya syndrome were found in the literature , 18 with and eleven without nf association , in three cases no information was given ( table 1 )  . 
there was only one case of a ruptured aneurysm observed in conjunction with moyamoya in a child with repeat irradiation to a cumulative dose of 110 gy [ 43 ]  . 
although comparisons between adults and children and low - grade glioma and pituitary adenoma , respectively , might be misleading , it is well known that irradiation of parts of the visual pathway in pituitary adenoma at dose prescriptions and fractionation schemes , which are similar to those used in childhood low - grade glioma , does not carry a significant risk of late radiation injury . 
in a total of 1 , 202 patients undergoing surgery followed by radiotherapy or radiotherapy alone , only 20 cases ( 1.6% ) of radiation - induced late effects were observed ( table 2 ) [ 6 ]  . 
fractionated doses in excess of 2.0 gy , however , are associated with an increased risk of late complications [ 2 , 3 , 31 ] ( table 2 )  . 
 atheromatous disease affecting cerebral blood vessels was infrequently observed in the literature and , if occurring , often seen in conjunction with nf [ 5 , 26 , 51 , 58 ] ( table 1 )  . 
the contribution of patients with nf was eleven out of 37 patients ( 30% ) as compared to two of 32 ( 6% ) in patients without the presence of nf . 
however , it should be considered that the cases were not specifically investigated with respect to other vascular accidents which could be explained also by involvement of the renal artery or by an eventual pheochromocytoma , which is frequently observed in nf patients . 
 other authors have also seen this complication in their series in patients with nf [ 5 , 9 , 32 , 37 , 40 , 53 ] , only rarely in patients without nf [ 25 ] ( table 1 )  . 
according to the findings of kestle et al . , particularly children with nf appear to have an increased risk of developing moyamoya after radiotherapy [ 37 ]  . this phenomenon did not occur in any of the 19 children not receiving radiation therapy , while among the 28 children irradiated , five developed moyamoya disease . 
radiotherapy of childhood low - grade glioma part ii development of secondary tumors in adults undergoing radiotherapy for pituitary adenoma in similar dose prescriptions , treatment fields and regions exposed to irradiation , the risk of secondary neoplasms is low ( 0.7% ) [ 6 ] ( table 3 )  . 
radiotherapy of childhood low - grade glioma part ii [ 69 ] noted one case of secondary tumor ( medullary astrocytoma ) outside the treatment portals in a patient with nf , without giving further details . 
 the combination of chemotherapy and radiotherapy in primary brain tumors appears to carry an increased risk of secondary tumors according to a recent analysis performed by the pediatric oncology group in 198 children < 3 years of age with malignant brain tumors who were treated with prolonged postoperative chemotherapy in an effort to delay irradiation and reduce long - term neurotoxicity [ 21 ]  . 
conversely , in adults a potentially increased risk of developing acute myeloid leukemia was discussed after chemotherapy for high - grade glioma , whereas radiation therapy appeared not to confer additional risk [ 52 ]  . 
as all presently applied treatments carry a risk of late sequelae and the tumor itself often causes severe deficits , the interrelationship between these factors is far from being clear . 
a major objection when interpreting these findings is the lack of sufficient pretreatment assessment of deficits , the heterogeneity of treatment techniques , and the fact that in many of these analyses the treatment - related parameters including doses to organs at risk were not documented . 
additionally , the series of patients who have been investigated spanned decades ranging from the 1930s to the 1990s , from orthovoltage treatment units to highly specialized megavoltage linear accelerators with varying treatment volumes comprising whole brain and partial brain irradiation and varying fractionation schemes . 
 in fractionated external radiation therapy , the risk of necrosis of brain parenchyma is low and plays only a role in stereotactic radiosurgery and brachytherapy [ 27 , 28 , 41 , 66 ]  . the lesions , however , are often small and circumscribed and are usually sufficiently treated conservatively without a risk of long - term morbidity . 
newer techniques in mri are able to precisely identify changes with respect to spatial distribution and corresponding integral dose distribution , but their role remain to be clarified [ 53 , 61 , 64 , 65 , 69 ]  . 
however , the potential relationship should be judged with caution , as younger children often present with nf and harbor large tumors frequently extending over the entire supratentorial midline and requiring large treatment portals . despite these shortcomings , the data reported support the present strategy to postpone radiotherapy in younger children in order to reduce the risk of severe disorders . 
radiotherapy of childhood low - grade glioma part ii true risk of radiation - induced vascular accidents , however , remains unknown , because children with nf have a genuine high risk of vasculopathies . 
it is therefore necessary to specifically address the question of radiation - induced changes with respect to nf and accompanying vascular changes , dose to normal brain tissue , and treatment techniques . 
although this observation clearly emphasizes the need for prolonged follow - up of long - term survivors , the decision for radiation therapy should not be based on the risk of radiation - induced secondary malignancies . 
 adequate pre - radiotherapy investigation must take into consideration all factors that may eventually adversely influence the treatment outcome , while radiation therapy must enable the highest tumor control with as low toxicity as possible . identification of possible pretreatment and treatment - related factors that may contribute to the occurrence of toxicity and comprehensive and close follow - up over prolonged periods of time must be considered as an imperative of current state of the art of radiation therapy in this disease . 
with the use of sophisticated treatment planning and delivery such as threedimensional treatment planning and intensity - modulated radiotherapy ( imrt ) , it is expected that more limited amount of normal brain tissue is exposed to radiation , enabling , thus , increase in the dose to the target while limiting toxicity . 
new technologies in imaging and the possibility to record the integral dose distribution within the planning target volume and organs at risk open up new approaches in assessing late effects ( i.e. , endocrinological disorders and changes in brain parenchyma ) with respect to dose prescription [ 45 , 64 ]  . 
 although the experiences are scarce mainly due to small patient numbers and short follow - ups , the addition of chemotherapy might enhance the risk of late effects , such as endocrinological disorders , growth retardation , and neurocognitive dysfunction . 
 the recently initiated prospective study of the apro ( pediatric radiooncology working party ) on recording of doses to organs at risk and the forthcoming siop / gpoh ( international society of pediatric oncology / greman society of pediatric oncology and hematology ) lgg 2003 study in cooperation with the gpoh network in pediatric oncology is addressing issues like preand posttherapeutic assessment of all relevant clinical and psychosocial parameters , treatment according to risk and age groups , the preferable use of modern radiotherapy techniques in conjunction with recording of integral dose to organs at risk ( dose - volume histograms )  . 
 strahlentherapie und onkologie original article long - term survival following radiotherapy and cytarabine chemotherapy for sporadic primary central nervous system lymphoma christoph pttgen1 , martin stuschke1 , georg stben1 , armin schmitz1 , karl schwechheimer2 , hans - heinrich wacker3 , friedhelm rauhut4 , susanne kleuker5 , hans wilhelm6 , sara grehl1 , thorsten fehlings7 purpose : to analyze the long - term results following whole brain radiotherapy ( wbrt ) with sequential intrathecal ( i.th. ) cytosine arabinoside ( ara - c ) intravenous ( i.v. ) ara - c in patients with primary central nervous system lymphoma ( pcnsl )  . 
all had sporadic pcnsl with proven histology of high - grade cns lymphoma ( twelve diffuse large - cell b - lymphomas , one lymphoblastic lymphoma , one large t - cell lymphoma )  . 
patients were treated with two to four cycles of induction chemotherapy ( 40 mg / m2 ara - c i.th. ) , four patients received additional ara - c i.v. 
alle patienten hatten ein histologisch gesichertes hochgradig malignes zns - lymphom ( zwlf diffuse grozellige b - zell - lymphome , ein lymphoblastisches lymphom , ein anaplastisches ki1 - lymphom )  . 
sechs von 14 patienten erhielten 50 , 4 gy als wbrt , vier patienten erhielten 1 department of radiotherapy , university hospital essen , germany , 2 department of neuropathology , university hospital essen , germany , 3 lymph - node registry of the german society of pathology , institute of hematopathology , university of kiel , germany , 4 department of neurosurgery , university hospital essen , germany , 5 department of pediatrics , university hospital essen , germany , 6 department of neurology , university hospital essen , germany , 7 department of diagnostic radiology , university hospital essen , germany . 
 schlsselwrter : primres zns - lymphom ganzhirnbestrahlung cytosinarabinosid introduction patients and methods primary sporadic central nervous system lymphoma ( pcnsl ) is a rare neoplasm , but the incidence has increased significantly within the past 2 decades [ 14 ]  . 
brain lymphomas are , according to their clinical behavior , aggressive and morphologically in the vast majority diffuse polymorphous large - cell lymphomas , though other b - cell subtypes and rare lymphomas such as ki1 lymphomas of t - cell origin have been described [ 10 , 24 , 29 ]  . 
in the rtog 8315 study , local cerebral relapses were observed in 61% of patients with pcnsl and negative cerebrospinal fluid ( csf ) cytology within a limited follow - up time . 
patients received 40 gy wbrt followed by 20 gy boost to the contrast - enhancing lesions plus a 2 - cm margin given with 1.8 gy per fraction , five fractions per week [ 35 , 36 ]  . 
 [ 34 ] found 21 survivors out of 693 pcnsl patients with a follow - up > 5 years , mainly treated with radiotherapy alone in the period between 1964 and 1984 . 
in a more recent review , survival at 5 years was estimated to be 17% after wbrt with total doses > 40 gy [ 41 ]  . leptomeningeal involvement was found in considerable percentages between 1042% of patients with primary cerebral lymphomas at the time of diagnosis in several large series [ 2 , 8 , 34 , 41 ]  . 
 [ 2 ] with a high proportion of csf examinations at the start of therapy as well as at the time of recurrence showed that leptomeningeal relapse , with 41% , was quite common and that meningeal recurrence was reduced in patients who received treatment that included the leptomeninges . 
 we report the long - term results of thoroughly staged pcnsl patients receiving intrathecal ( i.th. ) cytosine arabinoside ( ara - c ) as prophylactic treatment for leptomeningeal lymphoma spread before and after high - dose wbrt with or without intravenous ( i.v. ) systemic ara - c administration prior to radiotherapy . 
 all patients were recruited between july 1987 and august 1995 at the department of radiotherapy , university clinic essen , germany , according to protocol guidelines initially planned for a randomized multicenter study . 
 staging procedures all patients had contrast - enhanced ct scans of the brain . original histology after resection ( n = 5 ) or stereotactic biopsy ( n = 9 ) was reexamined in 1996 . 
 further investigations included cytospin evaluation of csf , ophthalmologic examination ( split lamp ) , ct of thoracic and abdominal organs , complete blood cell counts , lactate dehydrogenase ( ldh ) , immunoelectrophoresis and protein electrophoresis , and bone marrow biopsy . 
the clinical target volume ( ctv ) comprised the whole neurocranium extended to the inferior border of the second cervical vertebra . the posterior half of the orbit was included in the ctv . 
thereafter , irradiation of the tumor region was continued with shrinking portals ( boost ) , which enclosed the macroscopic tumor region plus a safety margin of 2 c nevertheless , a total dose of 50.4 gy for the boost volume was planned . 
perceptual discrimination and information - processing abilities were tested with a divided attention test [ 4 ]  . these tests were completed with an adapted version of a thurstone cognitive ability test [ 28 , 30 ]  . 
 results those patients , who were randomized to systemic i.v. ara - c , were planned to additionally receive four cycles of ara - c ( 150 mg / m2 i.v. , d14 , q3wk ) before the start of wbrt on day 56 . 
 follow - up after treatment completion , a routine follow - up including physical examination and contrast ct or mri , respectively , between july 1987 and august 1995 , 14 patients were treated according to protocol guidelines . 
they received 50 gy wbrt ( two patients ) , 40 gy wbrt plus a 10 - gy boost ( two patients ) , and 56 gy ( wbrt , one patient ) , respectively . 
cr : complete remission ; f : female ; kps : karnofsky performance scale ; m : male ; na : not available ; ned : no evidence of disease ; pd loc : progressive disease locally ; pd sys : systemic progressive disease ; pr : partial remission . 
ten patients received the planned total tumor dose of 50.4 gy , six patients had wbrt up to 50.4 gy , four patients had wbrt up to 39.6 gy and received a boost of 10.8 gy in the macroscopic tumor region . 
chemotherapy alone , median survival amounted to 39 months ( 95% ci : 365 months ) with survival rates at 2 and 3 years of 51% ( 95% ci : 3369% ) and 38% ( 95% ci : 2155% )  . 
 causes of death progressive disease leading to death was observed in three cases during or early after completion of therapy , one of these patients had generalized disease manifestations at autopsy . 
 discussion studies on induction chemotherapy containing blood - brain barrier - crossing drugs , i.e. , high - dose methotrexate ( mtx ) , followed by wbrt with or without post - radiotherapy i.v. ara - c repeatedly achieved long - term survival rates of > 40% at 3 years and > 25% at 5 years [ 1 , 5 , 7 , 9 , 20 , 46 ]  . 
established patient - dependent prognostic factors like age and perfomance status [ 8 , 13 , 23 , 31 , 36 , 41 , 42 , 45 ] can profoundly influence the treatment results and may even dominate differences in efficacy between alternative treatment options . 
ara - c , however , seems to be worse than those observed with modern highdose mtx - based regimens [ 11 , 12 , 18 , 37 , 42 ]  . 
one of the longterm survivors in our series had a pcnsl of t - cell origin , which due to its rarity is much less well defined than b - cell lymphomas . 
in patients who were treated with chod / bvam followed by wbrt , dementia occurred in five ( 62% ) of eight patients being 60 years [ 5 ]  . 
the experiences from the present study agree with the aforementioned reports , that long - term survivors from pcnsl > 60 years have a considerable risk of late neurologic toxicity after regimens with wbrt to doses 40 gy . 
the risk of developing bilateral blindness , as observed in one patient , is rather low after irradiation alone up to 50.4 gy with conventional fractionation [ 22 , 36 , 40 , 44 ] , and therefore an additional toxicity of ara - c has to be suspected . 
the latency times to expression of neurologic side effects are in the range of 2430 months for older patients and may take > 5 years in patients < 60 years [ 1 , 8 , 48 ]  . 
the rates of complete remissions , observed in several studies with highdose mtx - containing regimens alone are in the range of 6090% with a rather low risk of late neurotoxicity after chemotherapy alone , especially in older patients [ 11 , 12 , 18 , 37 , 42 ]  . 
in order to clarify the role of wbrt in pcnsl , the neuro - oncologic working party of the german cancer society has set up a phase iii study on high - dose mtx with or without wbrt after complete remission . 
as , especially in younger patients , toxicity of radiotherapy is mild , moderate doses of radiotherapy might optimize the therapeutic benefit in pcnsl patients with complete response to chemotherapy , as it has been recently demonstrated in extracerebral lymphomas [ 17 , 21 , 33 , 39 ]  . 
this is in part due to the increased risk of severe neurotoxicity , especially when combined with wbrt , and the lack of a prospective assessment of its survival effect . 
the proven efficacy and moderate toxicity of radiotherapy in younger patients should guarantee radiotherapy a firm place in modern multimodal treatment protocols for pcnsl . strahlentherapie und onkologie original article impact of anemia prevention by recombinant human erythropoietin on the sensitivity of xenografted glioblastomas to fractionated irradiation georg stben1 , oliver thews2 , christoph pttgen1 , kai knhmann1 , horst sack1 , martin stuschke1 , peter vaupel2 background : pronounced oxygen deficiency in tumors which might be caused by a diminished oxygen transport capacity of the blood ( e.g. , in anemia ) reduces the efficacy of ionizing radiation . 
 material and methods : anemia was induced by total body irradiation ( tbi , 2 ( cid : 1 ) 4 gy ) of mice prior to tumor implantation into the subcutis of the hind leg . 
in one experimental group , the development of anemia was prevented by rhuepo ( 750 u / kg s.c. ) given three times weekly starting 10 days prior to tbi . 
the prevention of anemia by rhuepo treatment ( chb = 13.3 g / dl ) resulted in a significantly prolonged growth delay ( 61 5 days ) compared to the anemia group , even though the growth inhibition found in control animals was not completely achieved . 
 material und methodik : in musen wurde eine anmie durch ganzkrperbestrahlung ( tbi , 2 ( cid : 1 ) 4 gy ) unmittelbar vor tumorimplantation in die subkutis des hinterlaufs erzeugt . 
die anmieprvention mit rhuepo ( chb = 13 , 3 g / dl ) fhrte wieder zu einer signifikanten zunahme der wachstumsverzgerung ( 61 5 tage ) im vergleich zur anmiegruppe , wobei jedoch die wachstumshemmung bei den kontrolltieren nicht vollstndig erreicht wurde . 
 schlsselwrter : strahlensensibilitt anmie hypoxie erythropoietin fraktionierte bestrahlung 1 west german tumor center , department of radiotherapy , university hospital essen , germany , 2 institute of physiology and pathophysiology , university of mainz , germany . 
animal studies have clearly demonstrated that while anemia worsens already existing hypoxia , anemia correction either by erythrocyte transfusion or stimulation of erythropoiesis upon erythropoietin treatment leads to an improvement of the o2 - status in experimental tumors [ 21 , 22 ]  . the impact of hemoglobin level on tumor oxygenation has also been demonstrated in human tumors [ 33 , 34 , 36 ] , even though in some cases a worsening of the o2 - status was found only with pronounced anemia [ 2 , 8 ]  . 
 anemia is a common phenomenon in clinical oncology which can be caused by the neoplastic disorder itself ( due to e.g. , deficiency of erythropoietic factors , bone marrow inhibition by inflammatory cytokines , hemolysis , bone marrow infiltration , or paraneoplastic syndromes ) , by myelosuppressive therapy modalities , by cisplatin - induced nephrotoxicity leading to a reduced erythropoietin production , or by acute or chronic tumor bleeding [ 19 , 24 ]  . 
many clinical studies have demonstrated a significant impact of the hemoglobin level on the radiotherapy outcome with anemic patients showing a poor longterm prognosis following irradiation ( for a review see [ 11 ] )  . 
these studies clearly demonstrated that anemia reduces the antitumoral effect of radiotherapy , whereas restoring the hemoglobin concentration ( chb ) to normal levels renders the radiotherapy more effective [ 27 , 31 ]  . 
however , these studies were performed only with a single irradiation dose ( 10 or 12 gy ) and therefore the question remains as to whether these results were transferable to the clinical setting , where the total dose is applied in multiple fractions . 
for this reason , the aim of the present study was to analyze whether anemia plays a role for radiosensitivity in a fractionated irradiation schedule and whether anemia correction or prevention by rhuepo prior to irradiation can restore the efficacy of fractionated irradiation . 
animals were housed in laminar air flow units at the department of radiation oncology and had unlimited access to water ( supplemented with chlortetracycline [ 10 g / l ] and k + - sorbate [ 1.35 g / l ] acidified to a ph = 3.0 ) and a high - calorie laboratory diet . 
tumors were repeatedly characterized by means of dna content , volume - doubling time , and isoenzyme pattern of lactate dehydrogenase ( ldh ) and glucose - 6phosphate dehydrogenase ( gpd ) [ 3 ]  . 
 tumor growth tumor size was measured using two perpendicular diameters twice to three times a week , and tumor volume was calculated by v = a ( cid : 1 ) b2 / 2 ( where a and b are the long and short axes , respectively )  . 
a decrease in body temperature during anesthesia was avoided by surrounding the animal gently with a perspex tube . in addition , two thermostatically controlled fan heaters were positioned at a distance of 40 cm to the experimental setting during irradiation . 
 induction of anemia animals received total body irradiation ( tbi ) at a dose of 2 ( cid : 1 ) 4 gy ( 5 - mev photons generated by a linear accelerator at a dose rate of 2.5 gy / min ) , 6 and 30 h prior to tumor implantation . 
 tumor irradiation the tumor - bearing mouse legs were irradiated with 5 - mev photons generated by a linear accelerator at a dose rate of 2.5 gy / mthe focus - isocenter distance was 100 cm with field sizes of 3 ( cid : 1 ) 2 cm at the isocenter . 
 based on previous experiments which showed the nadir of the hemoglobin content 1214 days after tbi , the fractionated irradiation of the tumor was applied 14 days after first tbi . 
hemoglobin concentrations ( chb ) , hematocrit values , and tumor volumes on the day of the first fraction of tumor irradiation in animals not receiving total body irradiation ( tbi ; control ) , animals treated with tbi alone ( anemic ) , and mice receiving tbi and recombinant human erythropoietin ( epo - treated )  . 
hmoglobinkonzentrationen ( chb ) , hmatokritwerte und tumorvolumina am tag der ersten tumorbestrahlung in unbehandelten kontrolltieren ( control ) , in tieren , die nur ganzkrperbestrahlung ( tbi ) erhielten ( anemic ) , und musen , die sowohl mit tbi als auch mit rekombinantem humanem erythropoietin behandelt wurden ( epotreated )  . 
hemoglobin concentration ( chb ) as a function of time in animals treated only with total body irradiation ( tbi , 2 ( cid : 1 ) 4 gy on days 0 and 1 ) for anemia induction ( dots ) and animals additionally treated with recombinant human erythropoietin ( rhuepo , from day 10 until day + 17 , three times a week ; triangles )  . 
arrow heads indicate the times of rhuepo treatment , arrows mark tbi , tumor implantation and tumor irradiation ( 4 ( cid : 1 ) 7 gy given daily , starting 14 days after first tbi )  . 
verlauf der hmoglobinkonzentration ( chb ) in tieren , die zur anmieinduktion nur ganzkrperbestrahlung ( tbi , 2 ( cid : 1 ) 4 gy an den tagen 0 und 1 ) erhielten ( punkte ) , und in musen , die zustzlich mit rekombinantem humanem erythropoietin ( rhuepo , von tag 10 bis tag + 17 , dreimal wchentlich ) behandelt wurden ( dreiecke )  . 
die pfeilspitzen bezeichnen die zeitpunkte der rhuepo - gabe , pfeile markieren die tbi , tumorimplantation und tumorbestrahlung ( 4 ( cid : 1 ) 7 gy tglich , beginnend 14 tage nach der ersten tbi )  . 
angegeben sind jeweils mittelwert sem von mindestens 20 tieren ; * * p < 0 , 001 . results are expressed as means standard error of the mean ( sem )  . 
thus , rhuepo therapy for 10 days prior to tbi resulted in prevention ( or reversal ) of the radiation - induced anemia by the time of the fractionated tumor irradiation ( 13 days after tumor implantation )  . 
 the fractionated irradiation of tumors with a dose of 4 ( cid : 1 ) 7 gy resulted in a significant tumor growth delay with a subsequent regrowth of the tumors in all experimental groups . 
in nonanemic control animals ( without rhuepo treatment ) , the time period needed to reach four times the initial tumor volume was 79 4 days ( figure 2 )  . 
the prevention of anemia by rhuepo treatment resulted in a significantly slower regrowth ( 61 5 days to reach four times the initial volume ; figure 2 ) compared to the anemic animals . 
relative tumor volume ( normalized to the mean volume on the 1st day of tumor irradiation ) as a function of time in control animals ( without tbi ) , animals treated with tbi alone ( anemic ) and mice receiving tbi and rhuepo ( epo - treated )  . 
 since previous studies clearly showed that neither tbi nor rhuepo treatment affect tumor growth per se [ 27 ] , the differences in growth delay have to be attributed to differences in radiosensitivity upon fractionated irradiation . 
 discussion tbi of mice at a dose of 2 ( cid : 1 ) 4 gy induces a long - lasting reduction in the hemoglobin level of approximately 30% with a nadir chb being reached 14 days after tbi . 
in comparison to previous studies where anemia was induced by a single dose of 5 gy during tbi [ 27 ] , the schedule using 2 ( cid : 1 ) 4 gy resulted in a slightly longer duration of the reduction in chb necessary for the fractionated tumor irradiation scheme . 
the chb on the day of the first fraction of tumor irradiation was 9.9 g / dl which corresponds to a clinically relevant moderate anemia ( nci scale )  . 
for this reason , the model of radiation - induced anemia used in the present study seems to be comparable to the clinical situation found in large - field irradiation . 
previous data with the same tumor and animal model and almost the same procedure for anemia induction clearly showed that neither tbi applied immediately prior to tumor implantation nor the application of rhuepo over 4 weeks ( in the same schedule as used in the present study ) had a marked impact on tumor growth per se [ 27 ]  . 
as has been demonstrated in another tumor system [ 30 , 31 ] , erythropoietin had no promoting impact on tumor growth since neither a direct stimulation of cell proliferation by the pleiotropic growth factor epo [ 37 ] nor by an improvement in tumor oxygenation [ 21 ] which might induce a faster cell division [ 29 ] was seen . 
 irradiation of the htz11 glioblastoma tumors in a fractionated schedule of 4 ( cid : 1 ) 7 gy induced a pronounced growth inhibition of approximately 60 days followed by an exponential regrowth ( figure 2 )  . 
as might have been expected , the growth delay induced by this fractionated scheme was found to be significantly longer compared to single irradiation dose of 12 gy [ 27 ]  . 
however , it was unclear what impact anemia might have during such a fractionated irradiation schedule . several experimental studies have clearly shown that tumor oxygenation is slightly worsened during fractionated irradiation only if the total dose exceeds 45 gy [ 40 ]  . 
the intensified tumor hypoxia in this case is most probably the result of vascular destruction [ 38 , 39 ] followed by a deterioration of nutrient supply [ 32 ]  . 
these data may indicate that during fractionated irradiation , the impact of moderate anemia on the oxygenation status of the tumor and , by this , on the radiosensitivity plays only a minor role due to the overwhelming destruction of tumor vasculature . 
anemia prevention , however , improved the efficacy of radiation as indicated by a significantly longer growth retardation of approximately 12 days compared to anemic mice . at present , it is unclear whether the oxygenation status is indeed significantly improved by rhuepo during fractionated irradiation in anemic subjects . 
a pronounced worsening of the o2 - status has been described in fractionated schedules only at high total doses ( > 45 gy ) applied over > 3 weeks [ 40 ]  . 
in a previous study , it has been shown that after fractionated irradiation using six fractions of 6 gy applied within 11 days , the oxygenation status changed only slightly over 4 weeks [ 28 ]  . 
since the regrowth rate of the tumors after the growth delay was comparable in all three groups , it is unclear whether differences in tumor composition ( e.g. , fraction of apoptotic or necrotic cells ) after irradiation play a role in strahlenther onkol 2003 no . 
 since the irradiation schedule used in the present study is only loosely based on that used in clinical radiotherapy , the results obtained in the present study can only be transferred to the clinical setting with some reservation . 
further studies need to elucidate whether the hemoglobin level also plays a role at the end of a regular irradiation schedule ( e.g. , after several weeks ) when the tumor vasculature is severely injured resulting in a pronounced deterioration of the o2 - status . 
animal experiments in a well - defined tumor model showed that anemia reduced the oxygen supply to the tumor and , by this , worsened the o2 - status [ 21 ] which may induce tumor neovascularization by increased vascular endothelial growth factor ( vegf ) production [ 7 ]  . 
in turn , anemia correction or prevention led to a reduction in hypoxia , even though the values seen in control animals were not restored [ 20 , 21 ]  . in some human tumors , it has also been shown that anemia with a chb < 11 g / dl reduced tumor oxygenation [ 33 , 34 , 36 ] , whereas in others with only mild anemia , no substantial changes in the o2 - status were seen [ 2 ]  . 
obviously , compared to the well - defined tumor models in animal experiments , solid tumors in the clinical setting show a more pronounced heterogeneity of the o2 - status , which could mask the impact of chb [ 2 , 8 ]  . 
the anemia - induced increase in tumor hypoxia ( which , in turn , is known to reduce radiosensitivity ) has been discussed as a prominent mechanism by which a lower chb may influence the outcome of radiotherapy in the clinical setting [ 46 , 10 , 13 , 15 , 17 , 35 ]  . 
however , clinical studies concerning the impact of anemia correction ( e.g. , by rhuepo application ) on the efficacy of radiotherapy are rare [ 9 , 13 , 23 ]  . 
in a preliminary study on head and neck cancers undergoing preoperative chemoradiotherapy , it has been shown that patients with a reduced chb had a worse locoregional control and a shorter overall survival [ 9 ]  . 
however , since this is the only finalized clinical study and the results are only preliminary , presently ongoing clinical studies [ 14 , 16 ] have to show whether anemia correction by rhuepo can indeed improve radiosensitivity and the long - term prognosis of patients upon fractionated irradiation in the clinical setting . 
 conclusions the present study demonstrated , in a well - defined tumor model , that clinically relevant anemia ( chb = 9.9 g / dl ) limits the efficacy of radiotherapy in a fractionated schedule . 
the results , however , clearly show that at least during the early period of fractionation , anemia worsens radiosensitivity and anemia prevention by rhuepo partially restores the efficacy of fractionated irradiation . 
go3 purpose : analysis of the results of radiotherapy in a large group of cerebral gliomas with identification of prognostic factors and the outcome with respect to different decades of treatment . 
 patients and methods : two decades ( 19791999 ) of radiotherapy in supratentorial astrocytic and oligodendroglial tumors ( n = 821 ) at the university hospital groningen were retrospectively evaluated . 
 results : glioblastoma multiforme , including gliosarcoma , was the most frequent supratentorial glioma ( n = 442 ) with a poor survival , i.e. , median survival time ( mst ) 7 months , especially in patients > 50 years of age and with poor performance . 
over time , a decrease in radiation dose ( from 60 to 45 gy ) and from whole brain irradiation to local - field treatment was observed , following the literature . 
the inherent biology of the glioma is reflected by the study of recurrent tumors with progression to higher grades of malignancy in 3240% and by the histology of recurrent oligodendroglial tumors . 
however , reduction in long - term side effects was not evaluated , especially in low - grade gliomas which were treated in the second decade of the study with local fields only and a reduced radiotherapy dose using computerized three - dimensional ( 3 - d ) planning . 
 ergebnisse : das glioblastoma multiforme war das am hufigsten vorkommende supratentorielle gliom ( n = 422 ) und wies eine kurze berlebensdauer auf ( medianes berleben [ mst ] 7 monate ) , insbesondere bei patienten > 50 jahre und in schlechtem zustand . 
 schlsselwrter : radiotherapie gliome berleben introduction after the introduction of radiotherapy , this modality has been applied in a wide variety of malignant conditions as well as in patients with supratentorial brain gliomas . 
the evidence of the effect of radiotherapy in malignant brain gliomas came from four prospective randomized trials published at the end of the 1970s and in the beginning of the 1980s showing a doubling of median survival time ( mst ) with radiotherapy compared to surgery alone [ 1 , 25 , 45 , 46 ]  . 
however , for low - grade gliomas , as yet no randomized studies are available and preliminary results of one randomized trial show no survival improvement with radiotherapy [ 21 ]  . 
 in this study , the groningen experience spanning over two decades with this modern form of radiotherapy of supratentorial gliomas and including more than 800 patients is reported and the results are discussed in the light of the present knowledge on radiotherapy of these tumors . 
 patients and methods we retrieved the records of all patients who had surgery for a supratentorial glioma at the university hospital groningen or at the martini hospital groningen between 1979 and 1991 . concomitantly , all records of patients who had radiotherapy for a supratentorial glioma at the university hospital groningen or at the institute of radiotherapy friesland were retrieved and matched with the records of the operated patients . patients who had surgery only and those who had surgery and radiotherapy were identified . 
included were low - grade astrocytoma ( a ) , including gemistocytic astrocytoma ( ga ) , anaplastic astrocytoma ( aa ) , glioblastoma multiforme ( gbm ) and gliosarcoma ( gs ) , oligodendroglioma ( o ) , oligoastrocytoma ( oa ) , anaplastic oligodendroglioma ( ao ) , and anaplastic oligoastrocytoma ( aoa )  . 
 the patient performance was scored after surgery using the neurologic status ( ns ; 0 = neurologic findings absent ; 1 = minor neurologic findings , able to work ; 2 = able to be at home although nursing care may be required ; 3 = major neurologic findings , requires wheelchair , hospitalization , and medical care ; 4 = serious physical or neurologic state , requires hospitalization )  . 
additional treatments such as second or third operations or a second course of radiotherapy or brachytherapy were also evaluated . adjuvant chemotherapy was given to 39 patients with aa and gbm . 
no patient was lost to follow - up except for one patient who left the netherlands 6 years after surgery and radiotherapy for an aa , but was included in the analysis . 
in each histopathologic category of glioma , prognostic factors for survival , histopathology of recurrent tumor and survival of patients treated in the first decade compared to those treated in the second decade were studied . 
histology , median age at diagnosis , median duration of preoperative symptoms , median survival time ( mst ) , 2 - year , 5 - year , and 10 - year survival rate ( sr ) of 821 glioma patients . 
a : astrocytoma ; aa : anaplastic astrocytoma ; ao : anaplastic oligodendroglioma ; aoa : anaplastic oligoastrocytoma ; ga : gemistocytic astrocytoma ; gbm : glioblastoma multiforme ; gs : gliosarcoma ; o : oligodendroglioma ; oa : oligoastrocytoma . 
a : astrozytom ; aa : anaplastisches astrozytom ; ao : anaplastisches oligodendrogliom ; aoa : anaplastisches oligoastrozytom ; ga : gemischtzelliges astrozytom ; gbm : glioblastoma multiforme ; gs : gliosarkom ; o : oligodendrogliom ; oa : oligoastrozyto age ( years ) duration of symptoms mst ( months ) ( months ) 2 - year sr ( % ) ( % ) 5 - year sr ( % ) ( % ) 10 - year sr ( % ) 103 0 of 49 months ( table 1 and figure 1 )  . 
favorable prognostic factors for survival were young age , good performance , long duration of preoperative symptoms , absence of a gemistocytic component , and the treatment variables of macroscopic excision and the application of radiotherapy . 
radiotherapy was omitted in 22 patients in the 19791991 cohort for reasons of low performance in seven patients , patient refusal in three , wait - and - see policy in four , and unknown in eight . 
in high - grade gliomas , the planning target volume ( ptv ) of the tumor area was defined as the ct contrast - enhancing area with a margin of 23 cin low - grade gliomas , the ptv was defined as the ct low - attenuation zone plus a margin of 2 c from 1988 on , t2 - weighted spin - echo mri was used in helping define the ptv for non - contrast - enhancing low - grade gliomas [ 18 ]  . from 1994 on , a 3 - d planning system was used with conformal beams avoiding as much normal brain tissue as possible , especially in low - grade gliomas . 
 statistical methods survival analysis was performed by uniand multivariate analysis using the kaplan - meier method for univariate variable testing with log - rank statistics and cox proportional hazards modeling for multivariate testing . 
 astrocytoma and gemistocytic astrocytoma ( who grade ii ) these low - grade tumors occurred preferentially in younger patients and had a relatively favorable prognosis with an mst 120 180 240 300 survival ( months ) figure 1 . 
the prognosis for aa with an mst of 10 months was definitely poorer than for a , but slightly better than for gbm ( table 1 and figure 1 )  . 
both on uniand multivariate analysis , age , performance , duration of preoperative symptoms , radiotherapy , and extent of surgery were of independent prognostic significance ( table 4 )  . 
 a second operation was performed in 21 patients ( 16% )  . the aa remained aa in ten patients , progressed to gbm in six , regressed to a in four , and changed into aoa in one patient . 
 glioblastoma multiforme ( who grade iv ) the most frequent primary brain glioma was the gbm preferentially occurring > 50 years of age and having an mst of 7 months as wells as a short duration of preoperative symptoms ( table 1 )  . 
on uniand multivariate analysis , independent prognostic factors for longer survival were age < 50 years , good performance , duration of symptoms > 3 months , macroscopic excision , and radiotherapy ( table 5 )  . 
in the 19791991 cohort , the reasons for omitting radiotherapy were low performance in 77 patients ( 59% ) , patient refusal in four ( 3% ) , deterioration between the first visit to the radiotherapy department and the first treatment in three ( 2% ) , unknown in 36 ( 28% ) , or the opinion of the neurosurgeon that , in general , radiotherapy was useless for gbm in ten patients ( 8% )  . 
the histology of these recurrent tumors was as follows : o in nine patients , ao in five , oa in two , a in two , and malignant oa in one patient ( figure 2 )  . 
one patient was treated with 0.5 mci 32p in a cystic recurrence after 56 gy and lived for 36 months , and one patient was treated with brachytherapy on recurrence after 59.4 gy external radiotherapy and lived for 47 months . 
 oligodendroglioma and oligoastrocytoma ( who grade ii ) these gliomas are relatively infrequent , occurring at a median age < 50 years and carrying a favorable prognosis with an mst of 103 months ( table 1 )  . 
on multivariate anaplastic oligodendroglioma and anaplastic oligoastrocytoma ( who grade iii ) the median age of these patients was > 50 years , and these tumors were the least frequent of the whole series . 
the other patients received a variable total dose in the range of 658 gy ( median 45 gy )  . in the second decade , this policy was gradually changed and radiotherapy was directed to the tumor area with local fields only . 
simultaneously , in lowgrade gliomas the total dose was decreased ( median 54 gy ) , and for gbm a short scheme of 15 ( cid : 1 ) 3 gy was introduced for patients with poor prognostic factors . 
radiotherapy in supratentorial gliomas comparing all patients treated with radiotherapy in the first decade ( 19791989 ) to those treated in the second decade ( 19891999 ) , no differences were observed regarding survival except for the gbm patients who showed a superior survival in the first decade . 
another well - known feature is the association between increasing age of the patient and increasing grade of malignancy which was also found in this study [ 5 ]  . 
in older patients , high - grade gliomas prevail which may evolve after a period of a low - grade tumor or arise de novo [ 7 , 27 ]  . 
the histology of the recurrent tumor after a primary a , i.e. , progression to aa or gbm in 14 of 35 cases ( 40% ) , may reflect the former phenomenon . 
in o , the relation between tumor grade and age was also found with higher prevalence of low - grade o in young patients [ 12 , 33 ]  . 
other reports show somewhat better 5 - year survival figures , although they may include pleomorphic xanthastrocytoma and / or , more importantly , pilocytic a [ 15 , 35 ] or they may be restricted to patients with radiotherapy only , thereby excluding some poor - performance patients [ 24 , 31 , 41 ]  . 
clearly , these data do not support the notion that ga should be considered aa [ 26 ] , as the 5 - year survival of aa in our series was only 12% . 
the effect of radiotherapy on survival of low - grade gliomas is still debated in the literature based on retrospective studies [ 15 , 28 , 30 , 31 , 41 ]  . 
the only prospective randomized trial to answer this issue showed no benefit of radiotherapy on survival at interim analysis , only an improvement in progression - free survival [ 21 ]  . 
radiotherapy in supratentorial gliomas radiotherapy and anaplastic astrocytoma a major problem in evaluating the role of radiotherapy in aa is that there are no separate trials on radiotherapy for aa . the aa is often included with gbm in studies on malignant astrocytomas , which conclude that radiotherapy prolongs survival . 
 the aa holds an intermediate position in the continuous spectrum of astrocytic tumors , between a and gbm [ 9 , 11 ] , which implies the risk of both underand overdiagnosis . 
four randomized trials were performed at the end of the 1970s and in the beginning of the 1980s , all reporting a doubling of the mst from 45 months without to 810 months with postoperative irradiation [ 1 , 25 , 45 , 46 ]  . 
survival rate depends on prognostic factors such as age , performance , duration of symptoms , partial or no resectability of the tumor , and the patients inability to undergo a series of radiotherapy sessions . 
in patients > 50 years , with low performance , short symptom time and irresectability of the tumor , the prognosis is poor and will clinically not be significantly modified by radiotherapy [ 10 , 20 , 38 ]  . 
in the first place , classification and grading problems still persist although a two - graded system identifying a lowgrade and an anaplastic or high - grade o is mostly accepted [ 14 ]  . 
in our series as in those of others [ 9 , 13 , 47 ] , o has superior survival compared with a and ao has a superior survival compared with aa . 
according to the who classification , an oa contains at least 25% of o ; recently , however , a smaller fraction of o in a was found to possibly have prognostic and clinical relevance [ 14 ]  . 
furthermore , the identification of an oligodendroglial component in an astrocytic tumor leads to improved survival which is intermediate between o and a in this series and in the literature [ 14 ]  . 
radiotherapy in supratentorial gliomas droglial tumors as long - term survivors are at risk of radiationinduced white - matter damage and also because chemotherapy has recently been introduced as primary modality therapy after surgery [ 14 ]  . 
interestingly , in nearly all recurrent tumors histology again showed an oligodendroglial tumor or at least a mixed tumor which is in keeping with the concept that these tumors are genetically different from astrocytic tumors [ 37 ]  . 
 radiotherapy in 19791989 and in 19901999 in the first period of the study , the low - grade gliomas were irradiated using the same approach as for the high - grade gliomas with a dose of 59.460 gy and whole brain radiotherapy as the first part of treatment . 
the results of an eortc dose - response trial with identical survival after 45 gy compared to 59.4 gy [ 22 ] and the results of the study of pu et al . [ 36 ] , demonstrating that the low - grade glioma progresses from the original tumor site , have changed the policy of radiation treatment from whole brain radiotherapy with boost dosis up to 60 gy to 45 gy of local - field irradiation only . 
despite recent advances in radiotherapy , hardware development , e.g. , 3 - d computer planning systems and the use of mri in defining target areas , no difference in survival was found comparing patients treated in the first decade to those treated in the second decade of the study . 
however , the cognitive status of the low - grade glioma patients was not measured , and this may have improved due to reduction of dose to large areas of uninvolved white matter with conformal radiotherapy techniques [ 17 , 42 , 44 ]  . 
for gbm , a short scheme of 45 gy in 15 fractions in patients > 50 years and / or performance > nsr 1 was introduced in the second period of the study explaining the fact that less patients were treated up to 60 gy . 
for patients with more favorable prognostic factors , the standard scheme remains 60 gy in 6 weeks , because an mrc randomized trial proved a gain in mst of 3 months with 60 gy over 45 gy [ 4 ]  . 
regarding the radiotherapy treatment field design of high - grade gliomas , a change of strategy with time is observed in this patient series . in the beginning , whole brain irradiation as part of the treatment was applied , based on autopsy studies showing that brain isotope scanning , arteriography and surgical reports underestimated the wide infiltration of the gbm [ 23 , 39 ]  . 
later , the prospective study of hochberg & pruitt showed that in 90% of cases after radiotherapy , gbm progressed from within its original site of contrast enhancement plus a margin of 2 cm [ 19 ]  . 
moreover , survival data for patients treated with partial brain irradiation are essentially equivalent to those observed with whole brain irradiation in combination with a boost dose to the tumor [ 16 , 40 ]  . since then , local - field irradiation only became the standard approach as was the case in our institute . 
 strahlentherapie und onkologie short communication preliminary results on the influence of chemoradiation on apparent diffusion coefficients of primary rectal carcinoma measured by magnetic resonance imaging christian kremser1 , werner judmaier1 , patrick hein2 , jrgen griebel3 , peter lukas2 , alexander de vries2 purpose : to study changes of the apparent diffusion coefficient ( adc ) measured by magnetic resonance imaging ( mri ) in patients with primary rectal carcinoma during a course of combined chemoradiation . 
 patients and methods : diffusion - weighted echo - planar imaging at 1.5 t was performed in patients ( n = 8 ) with primary rectal carcinoma ( ct3 ) undergoing preoperative chemoradiation . 
separating the patients into two groups , a significant increase in adc value during week 1 of therapy , followed by a steady decrease , was found for the therapy - responder group . 
 conclusion : with these preliminary results it could be shown that mr diffusion imaging is able to detect individual changes of tumor adc values during the course of combined chemoradiation reflecting biological changes within the tumor tissue . 
 key words : magnetic resonance imaging apparent diffusion coefficient rectum neoplasms chemoradiation strahlenther onkol 2003 ; 179 : 6419 doi 10.1007 / s00066 - 003 - 1045 - 9 erste ergebnisse zum einfluss kombinierter radiochemotherapie auf die mittels magnetresonanztomographie gemessenen diffusionskoeffizienten in primren rektumkarzinomen ziel : untersuchung von nderungen des mittels diffusionsgewichteter magnetresonanztomographie ( dmrt ) gemessenen diffusionskoeffizienten ( adc ) in primren rektumkarzinomen whrend kombinierter radiochemotherapie . 
 patienten und methodik : diffusionsgewichtete echoplanare bildgebung wurde an einem 1 , 5 - t - mr - gert bei patienten ( n = 8 ) mit primren rektumkarzinomen ( ct3 ) whrend kombinierter radiochemotherapie durchgefhrt . 
 schlussfolgerung : diese vorlufigen ergebnisse zeigen , dass die dmrt in der lage ist , individuelle nderungen der adc - werte , die biologische vernderungen im tumorgewebe widerspiegeln , whrend kombinierter radiochemotherapie zu detektieren . 
 schlsselwrter : magnetresonanztomographie diffusionskoeffizient rektum neoplasmen kombinierte radiochemotherapie 1 department of radiology , and 2 department of radiation therapy , university of innsbruck , austria , 3 department of medical radiation hygiene , bfs federal office for radiation detection , neuherberg , germany . 
adc changes in rectal carcinoma during chemoradiation introduction magnetic resonance imaging ( mri ) is widely used for the detection and diagnosis of tumors , whereby mainly morphometric macroscopic tissue information is usually obtained . 
the mobility of water molecules within a given voxel is determined by the microscopic cellular structure , i.e. , the presence of barriers , such as cell membranes and macromolecules . 
due to the restricted motion of water molecules , the diffusion coefficients obtained by quantitative dwi differ from the free diffusion values and are called apparent diffusion coefficients ( adc ) [ 24 ]  . 
 to date , the most important clinical application of dwi has been the detection and characterization of cerebral ischemia [ 17 ] , where a reduction of adc up to 50% was observed to occur immediately after induction of ischemia . 
so far , the use of dwi for the diagnosis of tumors did not find widespread applications although there have been reports about the possible usefulness of dwi in discriminating between brain abscess and necrotic or cystic tumors [ 8 ] , the evaluation of medulloblastomas and metastatic disease [ 10 ] , and the characterization of hepatic lesions [ 27 ]  . 
during this process , the cell structure changes are leading to changes of the microscopic water environment which should be observable by dwi . several studies have shown changes in tumor adc [ 3 , 4 , 28 ] after treatment . however , most of these studies were performed on experimental tumor models and , to our knowledge , so far only one applied radiation therapy [ 4 ]  . 
 patient group 1 group 2 it was the purpose of this study to apply dwi in patients with primary rectal carcinoma and to investigate changes of adc during a course of preoperative combined chemoradiation . 
 patients and methods the study was performed on eight patients ( mean age , 54.1 years ) with rectal carcinoma ( ct3 ) , whereby only patients with primary histologically proven adenocarcinoma g2 of the rectum without metastatic spread who were scheduled for preoperative chemoradiation were included . 
during clinical staging , each tumor , assessed by intrarectal ultrasound examination , showed an infiltration into the perirectal fat and confirmed the diagnosis of a ct3 tumor [ 15 ]  . 
excluded from the study were patients with tumor invasion of the sphincter , previous surgery or radiation in the area of the abdomen , previous chemotherapy , patients with acute or previous second malignancies , contraindications for the mr examination , or premature discontinuation of therapy including delayed or cancelled operation . 
a therapy response was defined if the pathologic observation revealed no invasion ( ypt02 ) , no therapy response if the observation yielded invasion into the perirectal fat ( ypt3 )  . 
 treatment technique each patient received preoperative combined chemoradiation [ 25 ] and a total irradiation dose between 38.3 and 44 gy , at a single dose of 1.1 gy administered twice daily . 
parallel to this , 350 mg / m2 5 - fluorouracil ( 5 - fluorouracil ebewe ; ebewe limited company , austria ) was administered continuously through an implanted central venous catheter ( port - a - cath deltec cadd - 1 system ; sims deltec , inc . , usa ) on each treatment day . 
written informed consent was obtained from all patients , after the nature of the procedure had been fully explained to the magnetic resonance imaging mri was performed on a 1.5 - t whole body imager ( magnetom vision plus ; siemens , erlangen , germany ) equipped with an echo - planar capable gradient system ( rise time 300 s , 23 mt ) and a phased - array body coil . 
 before dwi , t1 - weighted images in sagittal and transverse orientation were obtained in all patients using a standard turbo spin - echo ( tse ) sequence ( tr = 800 ms , te = 12 ms , turbo factor : 3 , acquisition matrix : 256 , fov : 300350 mm , slice thickness : 5 mm , slice gap : 1.5 mm , number of slices : 15 )  . the transverse t1 - weighted images were used to obtain an estimate of the respective tumor volume . 
an estimate of the tumor volume was then calculated by summing up the product of slice distance ( = slice thickness + slice gap ) and the crosssectional area of the tumor at each slice location . 
however , the accuracy of this volumetric method , which follows the cavalieri method , was sufficient to detect overall changes of tumor volume related to therapy [ 18 ]  . 
sequential sampling of kspace was used with an effective echo time of 123 ms , a bandwidth of 1 250 hz / pixel , and an acquisition matrix of 128 ( cid : 1 ) 128 , which was interpolated to 256 ( cid : 1 ) 256 during image calculation . 
a total of 20 consecutive slices were acquired in order to cover the whole tumor with an fov of 300 mm , a slice thickness of 5 mm , and a slice gap of 1 m from the obtained differently diffusion - weighted images , adc maps were calculated using a linear regression model based on the logarithm of signal intensities following s ( b ) = s ( 0 ) ( cid : 1 ) exp ( b ( cid : 1 ) adc ) , eq . 
1 where s ( b ) is the signal intensity with diffusion gradient , s ( 0 ) is the signal intensity without diffusion gradient , and b is the gradient factor ( in seconds per square millimeter ) of the used pulse sequence , being a measure of the strength of the diffusion gradient . 
for detailed statistical analysis , all individual pixel adc values of each evaluated roi for all patients were pooled and taken into account , giving rise to a large number of data samples . 
the differences of the adc values between tumors without downstaging and tumors with downstaging were tested using the nonparametric mann - whitney test , whereby all individual pixel adc values included within every evaluated roi were used as data samples . 
in two patients ( #2 , #4 ) , a statistically significant ( wilcoxon test ; p < 0.05 ) increase of the mean adc value was found within the 1st week after beginning of therapy , followed by a decrease between 1st and 3rd week and a slight reincrease during the 4th week ( figures 3a and 3b )  . 
it has to be noted that these two patients also showed an increase in tumor volume during the 1st week of therapy which was not found for the other patients ( table 2 )  . 
 week 4 taking all individual roi pixel adc values for all patients within both groups ( therapy responder and nonresponder ) into account , adc histograms were obtained as shown in figures 4a to 4e . 
while there was no obvious difference in adc pixel value distributions between responder and nonresponder group found before the start of therapy , the adc distribution for the therapy - responder group showed a clear shift to higher adc values after the 1st week of therapy . 
 to test if a correlation between tumor volume and corresponding adc values exists , a spearman test was used . no correlation ( r = 0.002 ) between the time course of adc values and the time course of tumor volume during therapy was found for patients without tumor downstaging , whereas a weak correlation ( r = 0.498 ; two - tailed significance level : 0.05 ) was found for patients with tumor t - downstaging . 
the total mean values for the downstaging ( d ) and non - downstaging ( nd ) group were obtained by taking all individual roi ( region of interest ) pixel adc values into account . 
a twotailed mann - whitney test showed that the difference of adc values between patients with tumor t - downstaging and patients without tumor downstaging was highly significant ( p < 0.02 for all data ) during the whole course of therapy . 
changes of adc values during repeated measurements within an individ ( cid : 1 ) mean ( cid : 1 ) mean week week figure 3a abbildung 3a figure 3b abbildung 3b figures 3a and 3b . 
the solid line and error bars correspond to the mean adc value obtained from the individual pixel values of all evaluated rois ( regions of interest ) of one group of patients . 
die durchgezogene linie und die fehlerbalken beziehen sich auf den mittleren adc - wert , der fr die jeweilige tumorgruppe durch einbeziehung aller individuellen pixel aus allen ausgewerteten rois berechnet wurde . 
adc changes in rectal carcinoma during chemoradiation nonresponder responder week 0 nonresponder responder week 1 adc ( ( cid : 1 ) 103 mm2 / s ) adc ( ( cid : 1 ) 103 mm2 / s ) figure 4a abbildung 4a figure 4b abbildung 4b nonresponder responder week 2 nonresponder responder week 3 adc ( ( cid : 1 ) 103 mm2 / s ) adc ( ( cid : 1 ) 103 mm2 / s ) figure 4c abbildung 4c figure 4d abbildung 4d nonresponder responder week 4 adc ( ( cid : 1 ) 103 mm2 / s ) figure 4e abbildung 4e figures 4a to 4e . 
adc changes in rectal carcinoma during chemoradiation ual patient group were tested using a paired wilcoxon test , which revealed that for patients without tumor downstaging no significant ( p = 0.25 ) change of tumor adc values occurred during the 1st week of therapy , whereas for patients with tumor t - downstaging a highly significant ( p < 0.01 ) increase of adc was obtained . 
it was our hypothesis that changes of the cellular structure within tumor tissue , due to its interaction with ionizing radiation , should be manifested as changes of the corresponding adc coefficient , i.e. , as changes of the molecular water mobility . 
 it was shown that the spatial resolution and sensitivity of the used dwi method were sufficient to quantitatively analyze areas of differing adc values within a tumor by means of adc histograms and to detect changes of these histograms during therapy . 
 within the 1st week of therapy , a significant increase in mean adc , averaged over the group of therapy responders , was observed , whereas within the 1st week no significant change of adc was observed in the group of nonresponders . after the 1st week of therapy , adc values were found to be significantly lower for nonresponding tumors as compared to responding tumors . 
 since the diffusion process within the intracellular volume ( icv ) is slower than for the extracellular volume ( ecv ) , a change of adc values may be explained as a change of the icv / ecv ratio [ 1 ]  . 
adc changes during the course of radiation therapy should follow the well - known stages of therapy effects . ( 1 ) at the beginning of radiation therapy , ionizing radiation leads to a change of vessel permeability for water [ 26 ] resulting in an increase of the ecv , i.e. , to an interstitial edema , which would be observed as increased adc compared to the pre - therapy value . 
with failure of the na - k atpase pump , a cytotoxic edema will form due to a shift of water from the ecv to the icv [ 10 ] which is supposed to be accompanied by an overall decrease in the observed adc values . 
 ( 3 ) later , as a consequence of the cytotoxic edema , cell death will occur , which will lead to an increase of the interstitial space due to cell loss . these effects are expected to increase the mobility of water molecules within the damaged tissue [ 14 ] , which should lead to another increase in adc values . 
 in accordance with these arguments , a shift of the adc value distribution to higher adc values was observed for patients of the therapy - responder group during the 1st week of therapy . 
it has to be noted that only in two patients of the responder group , an increase of the mean adc was seen , whereby this , as expected , was accompanied by a noticeable increase in tumor volume . 
since the increase of adc was statistically significant for the therapy - responder group and was not detectable for the nonresponder group , this behavior might be a predictor of therapy outcome . 
it might be speculated that high single irradiation levels more likely trigger apoptic cell death [ 29 ] , whereas interphase cell death [ 20 ] , which is sometimes accompanied with an initial increase of cellular volume , dominates for low irradiation levels . 
we found a possible explanation in the histologic findings of the resected tumor remnants : a marked fibrotic response was present in all specimens as a response to tumor necrosis . 
adc changes in rectal carcinoma during chemoradiation to detect relevant biological changes during chemoradiation . to our knowledge , however , this study is the first to monitor tumor adc values during a course of low - dose hyperfractionated chemoradiation in patients . 
in in vivo tissues , the reported adcs have often shown higher values than expected [ 13 ] , which has been attributed to the influence of perfusion on signal attenuation in dwi [ 27 ]  . 
as part of this tumor monitoring project , perfusion imaging was also performed , whereby details of the measurement protocol and results have been published elsewhere [ 57 ]  . 
thereby , for example , in all patients an increase of perfusion during the course of therapy was found , whereas only in two patients an increase in adc values was observed . 
it will be part of an ongoing study to correlate diffusion and perfusion effects during the course of combined chemoradiation in more detail , which should lead to a better understanding of the mechanisms underlying tumor tissue response to radiation therapy . 
 conclusion in this preliminary study , it could be shown that mr diffusion imaging is able to detect individual changes of tumor adc values during the course of combined chemoradiation corresponding to biological changes within the tumor tissue . 
this would permit therapy modifications based on individual tumor characteristics . our initial data encourage further studies to prove the possible value of totally noninvasive and rapid dwi imaging on predicting and controlling therapy outcome . 
 strahlentherapie und onkologie original article amifostine as radioprotective agent for the rectal mucosa during irradiation of pelvic tumors a phase ii randomized study using various toxicity scales and rectosigmoidoscopy john kouvaris1 , vassilis kouloulias1 , 2 , elias malas3 , christos antypas1 , john kokakis1 , spyros michopoulos4 , george matsopoulos2 , lambros vlahos1 aim : to evaluate the cytoprotective effect of amifostine against radiation - induced acute toxicity to the rectal mucosa . patients and methods : 36 patients irradiated for prostate or gynecologic cancer were randomized to receive amifostine ( n = 18 , group a ) or not ( n = 18 , group b )  . 
the radiation - induced acute rectal toxicity was evaluated by using three different toxicity scales : who scale , eortc / rtog toxicity criteria , and a modified toxicity scale based on the lent - soma grading scale and the endoscopic terminology of the world organization for digestive endoscopy . 
the area under the curve ( auc ) for dose - volume histograms ( dvhs ) of the rectum was also assessed during a 3 - d treatment planning schedule , and no significant differences were assessed between the two groups , indicating a homogeneous dose - volume effect . results : amifostine was well tolerated . 
die strahlungsinduzierte akute toxizitt auf die rektumschleimhaut wurde mit hilfe von drei verschiedenen toxizittsskalen ausgewertet : der who - skala , den toxizittskriterien der eortc / rtog und einer modifizierten toxizittsskala , die sowohl auf der lentsoma - skala als auch auf der endoskopischen terminologie der weltorganisation fr intestinale endoskopie beruht . 
whrend des 3 - d - therapieplans wurde auch die flche unter der kurve ( auc ) fr die auswertung in rektalen dosis - volumen - histogrammen ( dvh ) bestimmt . 
 1 radiology - radiotherapy department , and 2 department of electrical and computer engineering , institute of communication and computer systems , national technical university of athens , greece , 3 endoscopy - gastroenterology unit , department of surgical oncology , aretaieion university hospital , athens , greece , 4 department of gastroenterology , alexandra general hospital of athens , greece . 
 schlsselwrter : amifostin strahlentherapie rektale mukosa rektosigmoidoskopie toxizittsgrad randomisierte studie introduction rectal toxicity is often dose - limiting during pelvic radiation therapy [ 2 , 9 , 19 ]  . 
since conformal radiotherapy of pelvic tumors aims at reducing irradiation of organs at risk such as the rectum [ 14 , 15 ] , it is important to evaluate the side effects as comprehensively as possible . 
endoscopy is considered to give the best estimation of moderate rectal mucosal damage , which does not inevitably lead to clinically evident mucositis [ 12 ]  . furthermore , proven effective prophylactic local or systemic therapies for radiation - induced anorectal mucositis do not exist up to now [ 33 ]  . amifostine ( ethyol ; schering - plough pharmaceuticals ) , an organic thiophosphate , was the first cytoprotective drug to enter clinical trials [ 23 , 28 ]  . 
it has recently been approved for use as a radioprotector in the usa and the european union , after the encouraging results of an important multicenter randomized study in head and neck cancer patients [ 3 ]  . 
as a broad - spectrum cytoprotective agent for normal tissues against irradiation , it has already been entered in clinical practice , and certain guidelines have been reported for its use [ 11 ]  . the cytoprotective efficacy of amifostine on the rectal mucosa against radiation - induced proctitis has not yet been analytically studied in terms of endoscopic objective findings . 
 the aim of this study was to investigate , in a prospective randomized way , the radioprotective effect of amifostine on the rectal mucosa , using subjective as well as objective analytic endpoints , by performing rectosigmoidoscopy . 
patients were randomly assigned to undergo radiotherapy ( control arm , group b ) or radiotherapy supported by intravenous administration of amifos - tine ( amifostine arm , group a ) , according to a table of random numbers ( 0 vs 1 )  . 
 recruitment and eligibility criteria patients recruited into the study had a who performance status 1 and were referred for radical radiotherapy ( prostate and cervical carcinoma ) or postoperative radiotherapy ( endometrial carcinoma )  . 
during radiation treatment , two patients of group b and one patient of group a were not found eligible for the study due to reduction of hemoglobulin level < 11 g / dl or wbc counts < 2 , 500 / l . 
finally , eleven patients with cervical carcinoma , nine with endometrial carcinoma , and 16 with prostate carcinoma were eligible for the trial , a total of 18 patients in each ar pretreatment and treatment evaluation baseline studies included physical examinations , blood counts with differential and platelet counts , complete biochemical profiles , chest x - rays , and ecgs . 
the second investigator evaluated rectal toxicity according to eortc / rtog toxicity criteria . the third investigator assessed acute rectal radiation morbidity using a modified toxicity scale based on the lentsoma grading scale , as shown in table 2 . 
this modification took into account the initial lent - soma scale [ 16 ] , focused on endpoints for acute rectal mucositis , together with the scoring system based on the endoscopic terminology of the world organization for digestive endoscopy , as published by the esge ( european society of gastrointestinal endoscopy ) [ 6 ]  . 
the onset and duration of > grade 1 who intestinal toxicity ( in days ) along with the delays ( if any ) in radiotherapy schedule ( in days ) were also recorded . 
toxicity grade for rectumodification to subjective objective management analytic ( soma ) scale to fit the radiation - induced acute toxicity to the rectufive subjective and three objective items have been used for the evaluation of radiation - induced acute rectal mucositis . the second and third item of the objective scale were based on findings from flexible rectosigmoidoscopy and were in accordance with the endoscopic terminology of the world organization for digestive endoscopy . 
 grade 1 grade 2 grade 3 grade 4 subjective tenesmus mucosal loss sphincter control stool frequency pain objective bleeding mucosa surface ulceration occasional urgency occasional occasional 24 per day occasional and minimal intermittent urgency intermittent intermittent 48 per day intermittent and tolerable persistent urgency persistent persistent > 8 per day persistent and intense refractory refractory refractory uncontrolled diarrhea refractory and excruciating occult localized - spotted congested mucosa superficial 1 cm2 occasionally > 2 / week punctate congested mucosa persistent / daily diffused congested mucosa gross hemorrhage bleeding mucosa superficial > 1 cm2 deep ulcer surgical intervention strahlenther onkol 2003 no . 
radiotherapy treatment planning was based on recent ct scans . a standard fractionation schedule was used in all cases ( 2 gy / fraction , five fractions / week )  . 
anterior - posterior diamond - shaped fields extending from the upper edge of the fifth lumbar vertebra down to the lower edge of the pubic bones and laterally to the midline of the femoral head were employed for external beam irradiation , to a total dose of 50 gy , using a midline block at 44 gy . 1 week after completion of teletherapy , one to two sessions of low / medium - dose - rate brachytherapy were performed ( dose range 1636 gy , depending on the primary disease )  . 
in all patients , a 3 - d treatment planning was performed in conjunction with dose - volume histogram ( dvh ) for the target and the rectum ( organ at risk ) as well . 
automatic registration and segmentation regarding the outline of auc - dvh as well as measurements of the auc - dvh ( in cm2 ) were performed using a sophisticated software in the national technical university of athens , greece [ 22 ]  . 
the appropriate scaling factor was adjusted ( 10 cm = 100% of prescribed dose at x - axis and 10 cm = 100% of delineated rectum volume at y - axis ) to ensure reproducibility and comparability between different plots . 
 immediately following documentation of mucositis grade 3 ( incontinence and cramping ) or in case of no symptom relief , radiotherapy was interrupted until the grade of mucositis regressed to 1 . 
amifostine ( 500 - mg flat dose ) was diluted in 50 ml of normal saline and injected intravenously over 6 mthe injection was repeated daily , 2030 min before each radiotherapy fraction . 
 ( cid : 1 ) 2 - test and fishers exact test for 2 ( cid : 1 ) 2 tables were used to test relationships between categorical tumor variables [ 29 ]  . 
this side effect was considered to be an allergiclike reaction to amifostine , and after 4 days of interruption , cytoprotection was reinstituted in this patient in conjunction with corticosteroid treatment ( 250 mg / 2 ml hydrocortisone diluted in normal saline ) without any further sign of such a reaction . 
 efficacy of amifostine concerning the auc - dvh , no significant differences were assessed between amifostine and control group for each patient subgroup as well as overall ( table 1 )  . 
according to table 3 , the incidence of who and eortc / rtog toxicity was significantly lower in the amifostine ar no grade 2 or higher who and eortc / rtog acute toxicity was noted in the amifostine group , while acute rectal toxicity was observed in 16 / 18 of control versus 2 / 18 of amifostine group ( p < 0.001 , fishers test )  . 
concerning the who and rtog scale , patients with prostate cancer had significantly lower toxicity when amifostine was administered , with a p - value < 0.008 ( bonferroni correction )  . 
however , a trend toward lower toxicity but not a statistical significance was noted in the radiation - induced toxicity scores of cytoprotected patients with gynecologic tumors for all toxicity scales . 
nevertheless , when stratified for either patients with prostate or gynecologic cancer , there was only a trend toward lower toxicity scores related to cytoprotection according to the modified lent - soma scale . 
grade 2 urinary toxicity ( frequency of urination , dysuria , urgency ) was noted in 8 / 18 patients ( 44.4% ) of the control versus 2 / 18 ( 11.1% ) in the amifostine group ( p = 0.06 , fishers exact test )  . 
in patients treated for prostate cancer , psa levels had dropped to < 1.5 ng / ml 1 year posttreatment in 17 / 18 patients ( 94% ) of both groups . 
 discussion the mechanism by which amifostine exerts its selective cytoprotective effect on normal tissues is based on its active uptake of free thiol ( wr - 1065 ) in higher concentrations in normal organs than in cancerous tissues . 
the differential uptake of free thiol is due to differences in the microenvironment at the tissue level , resulting in slow entry of the free thiol into tumoral tissues [ 4 , 27 ]  . 
the combined hypovascularity , low alkaline phosphatase concentration , and low ph of cancerous tissues result in low rates of pro - drug ( wr - 2721 ) activation into its active metabolite ( wr - 1065 )  . 
selective protection is afforded to normal tissues by reduced metabolism of amifostine to the active metabolite wr - 1065 and low tumor uptake of wr - 1065 [ 32 ]  . 
once the free thiol has entered a normal cell , it is available to bind directly to and , thus , detoxify the reactive species of alkylating agent - generated carbonium or immonium ions , aquatic platinum species , or ions produced by radiation . 
 concerning preclinical studies , ben - josef et al [ 1 ] , studying the local application of amifostine in the rectum of male copenhagen rats , reported significantly high concentrations preferentially in the rectal wall . 
liu et al [ 17 ] reported the results of a randomized clinical study conducted in china that evaluated the use of amifostine and radiotherapy in 100 patients with locally advanced rectal cancer . 
dunst et al [ 8 ] , in a nonrandomized trial of amifostine versus control , reported a significantly lower bowel toxicity in patients with rectal cancer who underwent postoperative pelvic irradiation with 50.4 gy combined with amifostine , even when the drug was administered intermittently . 
in an interim analysis of another study , kligerman et al [ 13 ] also reported that no moderate or severe late radiationrelated gastrointestinal toxicities were observed in the amifostine group . 
all of the three independent investigators noted significantly lower toxicity in the amifostine arnot only the mean toxicity score but also the severity of anorectal mucositis was significantly reduced for all cytoprotected patients ( prostate and gynecologic cancer ) , as shown in tables 3 and 4 . nevertheless , when stratified by either prostate or gynecologic cancer , the statistical significance of lower toxicity scores related to cytoprotection was changed to only a trend toward reduced radiation - induced morbidity . 
the reduction in radiationinduced rectal toxicity also restricted the delays of radiotherapy related to lower intestinal morbidity , although only a trend toward decrease of radiotherapy interruptions was measured . beyond the fact that the modern techniques for prostate canstrahlenther onkol 2003 no . 
cytoprotective efficacy of amifostine against acute rectal toxicity cer using high doses of 3 - d conformal radiotherapy and / or brachytherapy show a low risk of acute rectal effects [ 2 , 15 , 21 ] , we have noticed some symptomatic intestinal side effects ( rectal or abdominal pain requiring analgesics ) , even though no pure opposite fields were used for pelvic irradiation . 
at the completion of radiotherapy , several patients in the control arm presented focal or diffuse reddening of the rectal mucosa combined with an edematous halo and superficial ulceration > 1 cm2 . 
in fact , hovdenak et al [ 12 ] , by examining the sequential development and associations of clinical , endoscopic , and histopathologic signs of rectal toxicity , have concluded that in contrast to clinical symptoms , endoscopic changes stabilize and histologic changes start to regress from the 2nd to the 6th week of treatment . 
this tremendously interesting observation may explain the apparent lower sensitivity of rectosigmoidoscopy , since the second endoscopic evaluation was performed at the end of treatment , when the findings of rectal mucositis have regressed . 
in terms of rectal dvhs , geinitz et al [ 10 ] reported that the irradiated volume fractions of rectum for patients with bleedings after prostate irradiation were significantly higher than for nonbleeding patient , no matter how the rectum borders were defined . 
according to our study , no significant differences between amifostine and control arm were monitored in the auc - dvh concerning the rectum as organ at risk , a fact which indicates that the impact of dosevolume effect on normal tissue complication probability was homogeneous between the treatment arms [ 19 ]  . 
however , significant differences were noted for the auc - dvh between patients irradiated either for prostate or gynecologic cancer . this was more or less expected , since the radiotherapy schedule was different for these two anatomic sites . 
the latter report probably explains the fact that no grade 4 toxicity ( rectal bleeding ) was tracked in our patients during the radiotherapy schedule , since due to conformal treatment planning , the above limitations were not reached . 
sauer et al [ 26 ] reported > 10% of grade 3 or higher ( 1% grade 4 ) acute rectal toxicity in patients undergoing chemotherapy and pelvic irradiation with 50 gy . 
 we may also comment on the fact that in our study , the cumulative dvhs were computed for the whole rectum , including the rectal cavity , whereas the rectal wall was not analyzed . first , uncertainties related to difficulties in distinguishing the rectal wall from the content will result in less reproducible data [ 7 , 18 ]  . 
second , regarding the 4 - field technique , contouring of the rectal wall leads to similar dvhs compared to the delineation of the outer rectal contour when expressed in percentage [ 7 ]  . 
one precondition for the evaluation of relative rectal volume was that the rectum should be contoured in the same way for all patients within the radiation field [ 10 ]  . 
 the use of a specific analytic scale for the objective measurements of acute radiation - induced rectal mucositis by means of endoscopy offers a possibility to have accurate endpoints for the evaluation of tissue damage , but the criteria of rectosigmoidoscopy findings are still not conclusively defined in the literature . 
mean values of who score , eortc / rtog scale , modified soma score , onset and duration of > grade 1 who intestinal toxicity and delays in radiotherapy ( in days ) stratified by group . 
cytoprotective efficacy of amifostine against acute rectal toxicity patients presenting complaints such as rectal bleeding , pain , increased stool frequency , urgency and incontinence , but systematic endoscopic evaluation including symptomatic as well as asymptomatic patients is rarely available [ 30 ]  . 
in order to document and compare data collected from endoscopy after radiotherapy , we have introduced a graduation system based mainly on the lent - soma criteria focused on acute effects , but also on the standardization of the terminology published by the esge . 
our experience on 36 patients has shown that the use of this terminology is practicable and provides a definition of terms usable for both , the radiation oncologists and the endoscopists . 
in a previous work , wachter et al [ 30 ] proposed a detailed grading system based on a standardization of the endoscopic terminology . however , beyond the scientific merit of such a toxicity scale , the grading system had not much in common with toxicity scales already used during routine clinical practice in radiotherapy departments [ 5 , 16 , 31 ]  . 
certainly , a grading system serving as a common language , thus facilitating the communication between endoscopists and radiation oncologists , would easily become the golden standard , and consequently , future investigations should be focused on a simple and compact way of expressing objectively the radiation - induced rectal toxicity in a standard common grading scale . 
despite the small number of patients , this prospective randomized study has demonstrated that the administration of amifostine before every session of radiation therapy can significantly reduce the incidence and severity of acute anorectal mucositis during pelvic irradiation . 
 strahlentherapie und onkologie original article physical and technical quality assurance in the chartwel - bronchus trial dietmar lehmann1 , hans - karl leetz2 , norbert hodapp3 , lutz voigtmann ( ) 1 , thomas herrmann1 , * , michael baumann1 , * background : on - site physical quality assurance ( qa ) was performed in the participating centers of the chartwel - bronchus trial to ensure that physical and technical treatment parameters correspond with the requirements of this trial . 
in addition , two phantoms with drillings for an ionization chamber were shipped with detailed instructions for ct - based treatment planning of a fixed field ( rw3 phantom ) and a standardized isocentric 3 - field technique ( rando humanoid phantom )  . using their routine treatment planning system , the participating centers performed point dose calculations for the isocenters in both phantoms and for defined points in the lungs and the spinal cord of the rando phantoduring the on - site visit , the doses in these points and the deviation of the actual monitor calibration from the internal reference value of the department were determined . 
 conclusion : the chartwel - bronchus physical qa program revealed a high conformity of geometric and dosimetric parameters and valid dose calculations by the ct - based treatment planning systems in all audited departments . 
 key words : radiation therapy chartwel - bronchus trial randomized clinical trial physical quality assurance external audits strahlenther onkol 2003 ; 179 : 1527 doi 10.1007 / s00066 - 003 - 1008 - 1 physikalisch - technische qualittssicherung in der chartwel - bronchus - studie hintergrund : in den an der chartwel - bronchus - studie beteiligten einrichtungen wurde eine physikalische qualittskontrolle durchgefhrt ( tabelle 1 ) , um zu gewhrleisten , dass die anforderungen des studienprotokolls bezglich der physikalisch - technischen parameter eingehalten werden . 
 material und methodik : den kliniken wurden fragebgen zur gertetechnischen ausrstung und zu hausinternen qualittskontrollen , ein rw3 - plattenphantom mit einer messbohrung und ein rando - humanoid - phantom mit messbohrungen im isozentrum , in den beiden lungen und am rckenmark zugestellt . 
die aufgabenstellung umfasste ct - gesttzte planungen eines stehfeldes ( rw3 - phantom ) und einer isozentrischen 3 - felder - technik ( rando - phantom ) mit jeweils 2 , 0 gy im referenzpunkt und berechnung der dosen am ort der messbohrungen ( abbildung 1 )  . 
die maximale prozentuale abweichung im isozentrum lag dann bei 3 , 0% ( abbildung 4 ) , die grte abweichung wurde im messpunkt in der linken lunge mit 7% gefunden 1 clinic of radiotherapy and radiation oncology , medical faculty carl gustav carus , university of dresden , germany , 2 homburg , germany , 3 department of radiotherapy , university of freiburg , germany . 
die abweichungen der geometrischen parameter von den sollwerten waren in allen kliniken vernachlssigbar klein ( tabelle 2 )  . schlussfolgerung : die ergebnisse der physikalischen qualittskontrolle im rahmen der chartwel - bronchus - studie zeigen ein hohes ma an bereinstimmung geometrischer und dosimetrischer parameter und eine valide dosisberechnung mit hilfe der ctbasierten behandlungsplanungssysteme in allen berprften zentren . schlsselwrter : strahlentherapie chartwel - bronchus - studie randomisierte studie physikalische qualittssicherung externe berprfungen introduction a randomized trial sponsored by the medical research council ( mrc , united kingdom ) showed a significant improvement in survival of 9% compared to conventional fractionation to 60 gy when patients with inoperable non - small - cell lung cancer were treated with chart ( continuous hyperfractionated accelerated radiation therapy , i.e. , three daily fractions of 1.5 gy with a minimum interfraction time interval of 6 h in 12 consecutive days ) to 54 gy [ 5 , 911 ]  . 
radiation dose escalation using chart or the more practical and cost - effective chartwel regimen ( chart weekend less , i.e. , three daily fractions of 1.5 gy from monday to friday ) is a promising option to further improve these results [ 24 , 12 ]  . 
after phase i / ii trials have shown that dose escalation using chartwel to 60 gy in 2.5 weeks is feasible [ 3 , 12 ] , a randomized multicenter phase iii trial was initiated by the arbeitsgemeinschaft radioonkologie der deutschen krebsgesellschaft ( trial aro 97 - 1 )  . 
as several studies indicate the importance of conformal techniques for intensifying radiotherapy in lung cancer [ 2 , 7 , 8 , 13 , 14 ] , 3 - d conformal radiotherapy is strongly recommended in the chartwel - bronchus trial to safely achieve the increase in total dose of 10% compared to the mrc trial . to guarantee high - quality treatment , the chartwelbronchus trial is accompanied not only by a medical quality assurance ( qa ) program but , for the first time in a multicenter aro trial , also by an audit of physical and technical treatment parameters [ 15 ]  . 
due to the large number of parameters which influence the conformity between calculated and delivered dose , a complete evaluation would be beyond the human and financial resources of such a progratherefore , a suitable number of checks was selected which cover the specific requirements of the trial . 
the present paper reports the results of the on - site visits of the physical qa team for those eleven centers in germany , poland , and the czech republic that had entered at least five patients into the chartwel trial until june 1 , 2002 . 
 material and methods during the on - site visit , geometric and dosimetric parameters as well as the validity of the ct - based treatment planning system for dose calculations were examined . 
in preparation for the on - site visit , questionnaires and phantoms with appropriate instructions for treatment planning of a fixed field and a standardized isocentric 3 - field technique were sent to the participating departments ( table 1 )  . 
 questionnaire questionnaires were used to obtain information on the equipment , in - house qa policies , recent results of the regular checks of dosimetric and geometric parameters , and on intervention levels . 
 radiotherapy department radiotherapist / physicist / director date of qa visit universitt wrzburg , klinik fr strahlentherapie vordermark / sauer / flentje allgemeines krankenhaus hagen , strahlentherapie souchon / cwiekala / souchon lungenklinik hemer , radiologie wahlers / drge / wahlers universittsklinikum charit , klinik fr strahlen therapie , berlin hinkelbein / jahn / budach universittsklinikum carl gustav carus , klinik und poliklinik fr strahlentherapie und radio onkologie , dresden baumann / lehmann / herrmann martin - luther - universitt halle , medizinische fakultt , klinik fr strahlentherapie dunst / gerlach / dunst stdtisches klinikum grlitz gmbh , radio logische klinik marschke / grnberg / philips universitt rostock , klinik fr strahlentherapie kchenmeister / ernst / fietkau klinika onkologii i radioterapii , gdansk , poland dziadziusko / szewczyk / jassem klinika radioterapie a onkologie , praha , czech republic kulhavy / stankus / doc . 
mudr kovalcik centrum onkologii , warszawa , poland kepka / bulski / fijuth june 24 , 1998 august 11 , 1998 august 12 , 1998 august 26 , 1998 october 16 , 1998 january 16 , 1999 july 7 , 1999 september 15 , 1999 april 19 , 2001 june 26 , 2001 june 14 , 2002 strahlenther onkol 2003 no . 
physical qa in the chartwel trial inspection of geometric parameters the geometric and technical parameters of the treatment facilities audited during the on - site visits are listed in table 2 . 
 audit of dosimetric parameters systematic deviations of the dose to monitor unit calibration of the accelerator were checked using a simple phantom made of sheets of rw3 ( ptw freiburg , germany ) at a field size of 10 ( cid : 1 ) 10 cm2 and at a measuring depth of 10 cfor departments ae the focus to surface distance was 100 cm , for the other departments the distance between focus and detector was 100 c the monitor units corresponding to a dose of 2.0 gy at the normalization point at the center of the drilling for the ionization chamber were determined using the treatment planning system and , additionally , with hand calculations . 
in parallel , a medical physicist of the audited department determined the actual monitor deviation of the linear accelerator compared to the in - house reference value . measurements in a humanoid phantom dosimetric evaluations of ct - based treatment planning and dose application were performed using a rando humanoid phantom of the thorax ( the phantom laboratory , salem , ny , usa )  . 
treatment planning was performed by the medical physicists of the participating centers using their departmental therapy planning system before the on - site visit . for this , ct scans of the phantom were acquired and the dose distribution of the standardized isocentric 3 - field technique was calculated . 
most deviations were < 1 mthe largest deviations were observed for the diameters of the isocenter sphere , for the distance indicator , and for the difference between the rotation axis of the collimator and the central ray of the light field . 
laser indication ; deviation ( mm ) radius of isocenter , perpendicular on gantry axis ( mm ) radius of isocenter , along gantry rotation axis ( mm ) light field size deviation at 90 / 270 gantry angle ( mm ) gantry angle vs . 
the measuring point at the isocenter receives dose contributions from three , the measuring point at the spinal cord from two , and the measuring points in the lungs from one field . 
 dosimetric parameters figure 2 shows the deviations of the dose measured in the rw3 phantom from the reference value of 2.0 gy without and with correction for the actual calibration state of the linacs refigure 3 . 
to separate the influence of the treatment planning system on this deviation from other sources , the measurements obtained in the humanoid phantom were corrected for the deviations determined in the rw3 phantom ( figure 2 )  . 
percental deviation of the absorbed dose measured in the rw3 phantom from the prescribed value of 2.0 gy without and with correction for the actual monitor calibration of the linac related to the internal reference value . 
prozentuale abweichung der im rw3 - phantom gemessenen dosis vom vorgegebenen wert von 2 , 0 gy ohne und nach korrektur mit der gefundenen abweichung der aktuellen monitorkalibrierung des beschleunigers vom klinikinternen referenzwert . 
percental deviation of the absorbed dose measured at the isocenter for the given isocentric 3 - field technique from the prescribed value of 2.0 gy after correction according to the corrected results shown in figure 2 . 
prozentuale abweichung der im isozentrum der 3 - felder - technik gemessenen dosis vom vorgegebenen wert von 2 , 0 gy nach korrektur mit den in abbildung 2 dargestellten korrigierten ergebnissen . 
the remaining part of the deviations measured in the rw3 phantom , i.e. , those deviations of up to 2.1% observed after correction for the actual calibration state of the linacs seem to be systematic and are in the same order of deviations found during the estro - equal measurements [ 6 ]  . 
these deviations may be caused by the calibration of the individual dosimeter used for in - house basic dosimetry , inadequate use of dosimetric correction factors or insufficient adaptation of the actual linac status to the basic data of the planning syste the deviations of the dose measurements in the isocenter of the rando phantom measurements for the ct - planned 3 - field technique never exceeded 4.0% compared with the prescribed dose ( figure 3 )  . 
to separate the influence of the treatment planning system on this deviation from other sources , all measurements obtained using the humanoid phantom were corrected for the deviations determined in the rw3 phantom ( figure 2 )  . 
the values determined in the isocenter of the humanoid phantom in the present study are in close correspondence with the results reported by aird et al [ 1 ] for the chart trial of the mrc . 
these fluctuations seem to be caused mainly by an incorrect consideration of scattering and inhomogeneities for photon energies 10 mv in one type of therapy planning system that is used by several of the participating centers . 
 conclusion the results of the chartwel - bronchus physical audit program show a very high conformity of geometric and dosimetric parameters and valid dose calculations by the ct - based treatment planning systems in all audited departments . 
nevertheless , the good results do not suggest abstention from further audits , because only results from clinical trials with proven quality standards in all important aspects are acceptable as a basis for new medical evidence , and this includes physical treatment parameters for radiotherapy trials . 
percental deviation of the dose at the three measuring points left lung , right lung , and spinal cord from the values calculated with the treatment planning syste the same correction as in figure 4 was applied . 
 discussion the aim of the present study was to evaluate the conformity of geometric and dosimetric treatment parameters , as well as the validity of ct - based treatment planning for dose calculation in the setting of the multicenter chartwel - bronchus trial . special consideration was given to the intrathoracic location of the target volume and the organs at risk and to the precision requirements of the trial . 
in this context , the variability of physical densities and the dose contribution resulting from scattered radiation are important variables for the physical model of the planning system and the quality of treatment delivery . 
the measured spatial deviations of < 2 mm and the angle deviations of < 1 are not relevant to the overall dose uncertainty in the target volumes defined in the chartwel - bronchus trial , even if these are located in close proximity to critical structures such as the spinal cord . 
to obtain an estimate of these limits , a comparative measurement with ferrous sulfate dosimeters ( fricke dosimeters ) was carried out simultaneously with the start of the on - site visits ( june 17 , 1998 at ptb braunschweig , germany )  . 
overall , the deviation of the dose measured in the rw3 phantom from the prescribed dose was small in all participating centers ( figure 2 )  . the deviations resulted mostly from differences between the actual monitor calibration and the internal reference and lie strahlenther onkol 2003 no . 
 strahlentherapie und onkologie case report irradiation for conjunctival granulocytic sarcoma katharina fleckenstein1 , hans geinitz1 , anca grosu1 , katharina goetze2 , martin werner3 , michael molls1 case history and findings : a 73 - year - old woman with a history of myeloproliferative syndrome ( mps ) presented with bilateral chemosis , redness and burning of the eyes . 
 conclusion : detection of orbital granulocytic sarcoma , even in the absence of typical leukemic symptoms is of practical importance , because treatment with irradiation can lead to stabilization or improvement in the patients vision . 
 key words : granulocytic sarcoma radiotherapy conjunctiva strahlenther onkol 2003 ; 179 : 18790 doi 10.1007 / s00066 - 003 - 1002 - 7 telestrahlentherapie zur behandlung eines konjunktivalen granulozytren myelosarkoms : fallbericht und literaturbersicht vorgeschichte und befunde : wir berichten ber eine patientin mit bekanntem myeloproliferativen syndrom , die ber eine schwellung und rtung der konjunktiven sowie ber brennen der augen klagte . 
 schlsselwrter : myelosarkom strahlentherapie konjunktiva introduction whereas diffuse leukemic infiltrates in the eye are common in fatal cases of leukemia , orbital tumor formation , known as chloroma , or granulocytic sarcoma , is a rather uncommon manifestation of acute non - lymphocytic leukemia [ 14 , 15 , 19 , 32 ]  . it is more common in the pediatric population but can occasionally be seen in elderly patients . 
occasionally , it may precede the clinical onset of acute myelogenous leukemia ( aml ) , presenting a diagnostic challenge [ 2 , 6 , 8 , 22 , 29 ]  . 
we describe the case of an elderly patient who presented with gross 1 department of radiation oncology , 2 department of hematology and oncology , and 3 department of pathology , technical university of munich , germany . 
 case report a 73 - year - old female patient was referred to the department of ophthalmology with a few weeks history of bilateral chemosis , redness and burning sensation of the eyes . 
 in view of the patients age and performance status a palliative low - dose chemotherapy with ara - c was initiated as peripheral blast counts increased concurrently with radiation therapy . 
 discussion ocular leukemic involvement is well described in the literature , but symptomatic ocular lesions , especially as an initial symptom are rather rare [ 11 , 14 , 20 ]  . 
according to the french - american - british cooperative group ( fab ) classification acute myeloblastic leukemia ( m2 ) and acute myelomonocytic leukemia ( m4 ) involve the ocular tissue more figure 1 . 
granulocytic sarcoma is usually diagnosed in children with a history of acute non - lymphocytic leukemia and most often indicates advanced disease [ 1 , 4 , 19 , 24 , 28 , 32 ]  . 
reports from turkey , uganda and egypt suggest that chloroma of the orbit is more frequent in these countries compared to other countries [ 3 , 15 , 17 , 27 , 32 ]  . 
several studies suggest that there is an association between 8 ; 21 translocation in acute myelogenous leukemia and granulocytic sarcoma in children [ 7 , 23 , 25 , 26 ]  . 
furthermore , our patient developed extramedullary leukemic tumor formation in the conjunctiva as a rare site of manifestation within the orbita . different postmortem analyses of autopsy eyes for ocular involvement in leukemia showed the choroid being the most frequently involved ocular site whereas leukemic infiltrates of the conjunctiva were seen in only 24% of eyes involved by leukemia [ 11 , 14 ]  . reviewing the literature , granulocytic sarcoma in the pediatric population has mainly been treated with chemotherapy . 
in pediatric patients good response to chemotherapy has been reported [ 7 , 13 , 16 , 26 ] even though in an older study by cavdar et al [ 3 ] who described 20 pediatric patients with ocular granulocytic sarcoma and complete remission after chemotherapy , relapse of leukemia was usually accompanied by the recurrence of ocular lesions . our case highlights the role of external beam radiotherapy as a very effective local treatment . 
several analyses of autopsy eyes in patients with leukemia showed that leukemic infiltrations are usually found in more than one ocular tissue [ 11 , 14 , 20 ]  . 
another alternative treatment of more superficial focal tumor manifestations could be the use of soft x - ray irradiation units as shown by willner et al [ 31 ] for the treatment of recurrent pterygia . with a total dose of 30 gy complete resolution of infiltration of the conjunctiva could be achieved . 
only few cases of ocular granulocytic sarcoma treated with local irradiation have been described , but all of them reported good results [ 18 , 29 , 30 ]  . 
watkins et al [ 30 ] and van veen et al [ 29 ] each described a case of complete remission of a large solid extraconal orbital granulocytic sarcoma in adult patients after local irradiation with 36 and 40 gy , respectively , together with chemotherapy . 
murray et al [ 18 ] reported a case of an elderly patient with diffuse scleral monocytic sarcoma who was treated successfully with a total dose of 20 gy in nine fractions without concurrent chemotherapy . two other case reports regarding local irradiation of lymphoblastic sarcoma of the iris and conjunctiva , respectively , described excellent results with a total dose of 20 gy [ 5 , 21 ]  . 
in conclusion a total dose of 20 gy might be sufficient for the treatment of diffuse tumor infiltration , while higher doses of 3040 gy might be preferable for initially larger tumor volumes as described by watkins et al [ 30 ] and van veen et al [ 29 ]  . 
nevertheless , detection of orbital granulocytic sarcoma , even in the absence of typical leukemic symptoms is of practical importance , because treatment with irradiation can lead to stabilization or improvement in the patients vision and hence make the affected individuals final period of life more comfortable . 
 strahlentherapie und onkologie aktuelles forum zelltodliganden in kombination mit ionisierender strahlung : rationale und kenntnisstand claus belka , angelika betsch , patrizia marini , verena jendrossek , michael bamberg , wilfried budach1 hintergrund : zuknftige forschungsstrategien in der strahlentherapie werden neben der weiteren verbesserung der bestrahlungstechnologie wege zur biologischen optimierung umfassen . 
hier knnen mehrere bereiche abgegrenzt werden : prdiktion , entwicklung neuer zytotoxischer wirkprinzipien , erhhung der normalgewebstoleranz und optimierung der radiochemotherapie . essenziell fr die wissenschaftliche bearbeitung der genannten anstze ist die aufklrung der grundlegenden mechanismen des strahleninduzierten zelltods . 
trail ( tnf - related apoptosis inducing ligand ) , ein mitglied der tnf - todesligandfamilie , induziert apoptose in tumorzelllinien , ohne nach heutigem kenntnisstand in normalgeweben toxisch zu seaufgrund der getrennten signalkaskaden ist eine kombination von trail mit ionisierender strahlung sinnvoll . 
anhand der vorgestellten kombination von trail mit bestrahlung wird deutlich , dass es mglich ist , auf basis molekularoder zellbiologischer untersuchungen vllig neue strategien zur optimierung der strahlenwirkung zu entwickeln . 
 schlsselwrter : apoptose trail bestrahlung klonogenitt kombinationstherapie strahlenther onkol 2003 ; 179 : 14151 doi 10.1007 / s00066 - 003 - 1047 - 7 death inducing ligands in combination with ionizing radiation : objective and current knowledge background : apart from optimization of the radiation technology , future new strategies in radiation oncology will focus on the biological optimisation leading to improved adaptation of the tumor therapy on each tumor entity . 
in this regard , different areas of biological research may be distinguished : prediction , development of new cytotoxic agents , improvement of the tolerance of normal tissue and the optimisation of radiochemotherapy . 
trail ( tnf - related apoptosis inducing ligand ) is a type - ii membrane protein belonging to the tnf family , which preferentially induces apoptotic cell death in a wide variety of tumor cells but not in normal cells . 
our study presents the rationale , own data , data of other groups as well as the current status of the latest findings regarding the function and physiological role of the trail death ligand . 
die kombination ionisierender strahlung mit interferon , retinoiden und quabain oder die blockade der cyclooxygenase - 2 eine spezifische modulation der intrinsischen radiosensitivitt maligner zellen bewirken [ 11 , 54 , 69 ]  . neben diesen strategien zur beeinflussung der wirkung der strahlentherapie auf den tumor wird von anderen arbeitsgruppen die entwicklung und anwendung weitgehend normalgewebsspezifischer radioprotektoren wie amifostin oder bbi verfolgt [ 13 , 23 , 24 , 30 ]  . 
hier ist das ziel , das therapeutische fenster zwischen normalgewebsschdigung und tumorwirkung zu vergrern . neue biologische forschungsstrategien zielen zunehmend auf die molekulare analyse von zelltodvorgngen und sich daraus entwickelnden neuen optionen zu spezifischen wirkprinzipien und kombinationen . 
die bezeichnung caspase leitet sich von der tatsache ab , dass diese enzyme cysteinproteasen sind , die ihr substrat spezifisch nach einem aspartatrest im zusammenhang mit einer vier aminosuren umfassenden erkennungssequenz schneiden . 
obwohl in einzelfllen die expression von apoptoseresistenzproteinen wie z.b. survivin mit dem ansprechen oder der prognose korreliert , lassen sich heutzutage keine globalen rckschlsse von der expression einzelner proteine auf das ansprechen auf eine strahlentherapie ziehen [ 58 ]  . 
wesentliche ursachen sind ebenso in dem komplexen regulativen zusammenspiel der zelltodrelevanten proteine zu suchen wie in der tatsache , dass apoptose nur eine spielart des programmierten zelltods darstellt und die rolle anderer formen des programmierten zelltods in der strahlenbiologie so gut wie nicht definiert ist . 
darber hinaus konnte fr verschiedene gewebe wie zentrales nervensystem ( zns ) oder darm gezeigt werden , dass apoptoseprozesse von pathogenetischer relevanz fr die ausbildung akuter oder spter schden nach strahlentherapie sind [ 5 , 53 , 56 ]  . 
so wurde an der zelloberflche von t - lymphozyten der so genannte cd95 - rezeptor erkannt , der durch den dazugehrigen cd95 - / fas - / apo - 1 - liganden ( cd95 - l ) aktiviert werden kann . 
dementsprechend spricht man bei dieser form des zelltods von rezeptorvermittelter apoptose und nannte diese art der rezeptoren zelltodrezeptoren ( death - receptors ) und die dazugehrigen liganden zelltodliganden ( death - ligands )  . 
sowohl muse , die einen inaktiven cd95 - l bilden , als auch muse , deren cd95 - rezeptor das signal nicht mehr korrekt nach intrazellulr weitergeben kann , entwickeln ein lymphoproliferatives syndrom , da aktivierte t - lymphozyten nicht mehr durch autound parakrine stimulation des cd95 - rezeptors abgettet werden [ 22 , 73 ]  . 
 da auch ionisierende strahlung zur induktion von apoptose fhrt , war zielsetzung der eigenen wissenschaftlichen arbeit zunchst , die ablufe von apoptoseprozessen nach bestrahlung von zellen auf molekularer ebene aufzuklren , um in einem zweiten schritt die mechanismen gestrter apoptose zu analysieren und strategien zur modulation von apoptoseresistenzen zu entwickeln . 
bekannt war jedoch , dass sich die caspasen aufgrund ihrer moleklgre in zwei verschiedene gruppen einteilen lassen : caspasen im grenbereich von 5060 kda sowie caspasen im molekulargewichtsbereich von 30 kda . 
die analyse zeigt , dass nur die caspasen im hheren gewichtsbereich ( caspase - 2 , - 8 , - 9 , - 10 ) neben dem eigentlichen enzymbereich eine zustzliche proteinstruktur ( lange prodomne ) aufweisen . 
caspasen mit langer prodomne wurden daher als aktivator - caspasen bezeichnet , da sie die initialen apoptosesignale durch interaktion der prodomne mit anderen moleklen in die aktivierung der nachgeschalteten caspasen - endstrecke bertragen . 
im unterschied dazu wurden caspasen ohne prodomne als effektor - caspasen bezeichnet , da ihre aufgabe nur in der koordinierten proteolytischen degradation der zellen besteht [ 1 , 62 ]  . 
 am beispiel der caspase - 8 ( flice ) konnte gezeigt werden , dass diese prodomne notwendig ist , um die verbindung mit dem cd95 - zelltodrezeptor ber das fadd - ( fas associated death domain - ) adaptermolekl herzustellen und so die verbindung von cd95 - rezeptorstimulation und apoptoseinduktion zu vermitteln [ 17 , 41 , 46 ] ( abbildungen 1 und 2 )  . 
wie erwhnt , dient caspase - 8 als aktivator - caspase nach stimulation von zelltodrezeptoren wie tumor - nekrose - faktor ( tnf - ) , cd95 - l oder tnf - related apoptosis inducing ligand ( trail oder apo - 2 - l ) [ 6 , 7 ]  . die initiale interpretation war daher , dass ionisierende strahlen apoptose ber eine aktivierung des cd95 - signalwegs auslsen knnten , da neben der aktivierung von caspase - 8 eine hochregulierung des cd95 - rezeptors und - liganden beobachtet werden konnte [ 7 ]  . 
cd95 - zelltodrezeptor - vermittelte apoptose und aktivierungsinduzierter zelltod : unstimulierte t - lymphozyten exprimieren neben dem t - zell - rezeptor ( tcr ) auch den cd95 - rezeptor ( 1 )  . 
after stimulation with a specific antigen ( ag ) in the context of an mhc molecule , cd95 - ligand expression is triggered ( 2 )  . after downregulation of inhibitory molecules ( c - flip ) apoptosis is triggered via interaction with the cd95 receptor ( 3 )  . 
hierzu wurden unterschiedliche , molekular charakterisierte zellsysteme verwendet : jurkat - t - lymphoblasten mit berexpression von bcl - 2 ( b - cell lymphoma 2 ) , jurkatt - lymphoblasten ohne expression von caspase - 8 , jurkat - tlymphoblasten mit berexpression einer dominant negativen caspase - 8 ( funktionelle blockade von caspase - 8 ) , jurkat - tstrahlenther onkol 2003 no . 
fr die apoptoseregulation durch p53 konnte gezeigt werden , dass in der regel seine funktion als transkriptionsfaktor , nicht aber sein einfluss auf die zellzyklusregulation relevant ist [ 3 , 20 ]  . 
wesentliche zielproteine fr die p53 - vermittelte transkription sind bax ( bcl2 associated x protein ) , noxa ( abgeleitet von lateinisch noxe ) und puma ( p53 upregulated modulator of apoptosis )  . alle drei gehren zu den proapoptotischen mitgliedern der bcl - 2 - familie [ 44 , 49 , 51 ]  . 
 obwohl die mechanismen der cytochrom - c - freisetzung im detail noch nicht verstanden sind , stellen sie doch einen schlsselschritt fr die aktivierung der nachgeschalteten caspase - netzwerke dar . 
caspase - 9 kann effektor - caspasen wie zum beispiel caspase - 3 aktivieren und initiiert so die finale apoptose . somit fhrt p53 zur apoptoseinduktion via caspase - 9 [ 65 ]  . dieser prozess wird durch die antiapoptotischen molekle der bcl - 2 - gruppe antagonisiert [ 35 ]  . 
 whrend der mitochondriale schaden nur einen verstrkungsmechanismus bei der cd95 - vermittelten apoptose darstellt , sind mitochondriale vernderungen fr die strahleninduzierte apoptose essenziell , da sie durch bcl - 2 vollstndig gehemmt werden [ 9 , 60 , 61 ]  . insgesamt konnte somit unzweifelhaft gezeigt werden , dass distinkte signalwege zur apoptoseinduktion nach bestrahlung oder stimulation von zelltodrezeptoren fhren , obwohl berlappende moleklgruppen aktiviert werden ( abbildung 3 )  . 
 lymphoblasten mit einer inaktivierenden punktmutation des cd95 - rezeptors und bjab - lymphoblasten mit berexpression einer dominant negativen fadd - mutante ( funktionelle blockade des fadd - adaptermolekls )  . 
es zeigte sich , dass die cd95 - vermittelte apoptose in zellsystemen mit fehlender oder blockierter caspase - 8 , blockiertem fadd oder einer inaktivierenden punktmutation des cd95 - rezeptors weitgehend gestrt ist . 
der einsatz von tnfwurde in einzelnen klinischen studien getestet . aufgrund der hohen toxizitt , die zu einem groen teil durch die pleiotrophe wirkung von tnfund fehlende wirkspiegel bei tolerablen dosen verursacht wird , ist ein klinischer einsatz in der tumortherapie nicht mglich [ 32 , 43 ]  . 
 im unterschied zur situation bei tnfund cd95 - l wurde nachgewiesen , dass trail in vielen tumorzelllinien apoptose induziert , jedoch zu keinerlei toxizitt in normalgewebe fhrt [ 2 , 72 , 75 ]  . 
als besonders trail - sensitive zelllinien haben sich dabei verschiedene darm - , lungen - , mamma - , nieren - , znsund haut - tumorzelllinien erwiesen [ 2 , 18 , 55 ] ( tabelle 1 )  . 
50% aller tumorzelllinien eine trail - sensitivitt auf . aufgrund dieser beobachtungen wurde trail schnell als magic bullet fr die tumortherapie eingestuft ( zur bersicht [ 28 , 47 , 71 ] )  . 
 trail : molekl und rezeptoren innerhalb der tnf - familie spielen insbesondere tnf - , cd95 - / fas - ligand und trail eine wichtige rolle in der vermittlung von apoptose in vitro . 
a selection of trail - sensitive tumor cells . kolonkarzinom bronchialkarzinom nci - h460 , hop - 92 , hop - 62 , nci - h226 , colo 205 , hct 15 , hcc - 2998 a549 mda - mb - 231 , mca - n , sum149 , sum229 , mcf10a , sum102 sf - 539 , sf - 295 , u251 , glial u251 malme - 3m , m14 mammakarzinom melanom nierenzellkarzinom rxf - 393 , achn , tk - 10 lymphomzellen zervixkarzinom jurkat , 9d , raji hela , me180 [ 2 , 55 ] [ 2 , 18 ] [ 2 , 18 ] [ 55 ] [ 55 ] abbildung 3 . 
parallel dazu kommt es durch die proteolytische spaltung von bid zur freisetzung von cytochromc aus dem mitochondriudas freigesetzte cytochrom - c aktiviert zusammen mit apaf - 1 und datp caspase - 9 . 
da die direkte aktivierung von caspase - 8 und caspase - 3 nicht durch bcl - 2 hemmbar ist , wird die cd95 - vermittelte apoptose durch bcl - 2 nur verzgert , jedoch nicht blockiert . 
comparison of cd95 and radiation induced apoptosis pathways : the activation of the cd95 cell death receptor directly activates caspase - 8 followed by the caspase - 8 dependent activation of caspase - 3 . 
zelltodliganden in kombination mit ionisierender strahlung dna - datenbankanalysen wurde ein neuer apoptoseinduzierender ligand identifiziert und als apo - 2 - l oder tnf - related apoptosis - inducing ligand ( trail ) bezeichnet [ 55 ]  . 
die signaltransduktion von trail erfolgt analog der signaltransduktion des cd95 - rezeptors ( abbildung 4 )  . die alleinige rolle von caspase - 8 als schlsselcaspase fr die trail - signaltransduktion ist durch eine neue beobachtung eingeschrnkt worden : die eng mit caspase - 8 verwandte caspase - 10 kann die rolle von caspase - 8 in einzelnen zellsystemen bernehmen [ 34 ]  . 
 trail : physiologische wirkung und wirkung auf tumoren von hoher bedeutung fr einen einsatz als tumortherapeutikum ist die tatsache , dass der trail - / apo2 - ligand , im unterschied zum cd95 - ligand , zumindest in den bisher getesteten modellen keinerlei toxizitt in normalgeweben aufweist . selbst hohe dosen fhrten bei musen oder cynomolgusaffen nicht zu organschden . 
 in untersuchungen an isolierten humanen leberzellen zeigte sich allerdings , dass einzelne biochemische prparationen von trail zur induktion von apoptose fhren [ 33 ]  . diese beobachtung dmpfte die euphorie hinsichtlich eines klinischen einsatzes von trail erheblich [ 48 ]  . 
in nachfolgenden studien konnte dann jedoch eindeutig gezeigt werden , dass diese beobachtungen auf die verwendung eines trail - proteins mit einem so genannten his - tag , das zur aufreinigung genutzt wird , beruht . 
in diesem zusammenhang konnte gezeigt werden , dass die alleinige stimulierung von dr5 nicht ausreicht , um apoptose in leberzellen zu induzieren , hingegen effektiv bei dr5 exprimierenden tumoren wirkt . 
nach bindung an trail - r1 ( dr4 ) und trail - r2 ( dr5 ) , zwei so genannte death - inducing receptors mit einer kompletten zytoplasmatischen domne , folgt die rekrutierung von caspasen und die induktion der caspasen - kaskade ber die das apoptotische signal bermittelt wird . 
zwei weitere rezeptoren , trail - r3 ( dcr1 ) und trail - r4 ( dcr2 ) , fungieren als so genannte decoy - rezeptoren und inhibieren die induktion von apoptose durch kompetition mit dr4 und dr5 um die trail - bindung . 
in contrast , neither trail - r3 ( dcr1 ) which is a gpi linked protein nor trail - r4 ( dcr2 ) which is a type i transmembrane protein containing a truncated cytoplasmatic death domain are capable of inducing apoptosis . 
weiterfhrende experimente zeigten , dass die abttung von tumorzellen durch trail ber natrliche killerzellen vermittelt wird und unabhngig vom perforin / granzymsystem wirkt [ 64 , 66 , 67 ]  . 
 die fehlende toxizitt in normalgeweben wird zumindest teilweise damit erklrt , dass viele humane normalgewebe trail - / apo - 2 - l - rezeptoren und decoy - rezeptoren gleichzeitig exprimieren . 
einfluss von trail auf die eradikation klonogener solider tumorzellen : die kombination von trail mit bestrahlung bei scc4plattenepithelkarzinomen ( koloniebildungstest nach delayed plating , behandlung mit 100 ng / ml trail , trail - behandlung zeitgleich mit der bestrahlung mit 2 , 4 oder 6 gy ) fhrt zu einer zustzlichen abttung klonogener tumorzellen erkennbar an der parallelverschiebung der kurve . 
effects of trail in combination with radiation : combined treatment of scc4 squamous cell carcinomas ( colony formation after delayed plating , 100 ng / ml trail , trail treatment concomitant with radiation with 2 , 4 or 6 gy ) leads to an additional kill of clonogenic tumor cells indicated by a parallel shift of the survival curve . 
einfluss von trail auf die eradikation klonogener lymphoider tumorzellen : der einfluss von trail auf die eradikation klonogener tumorzellen durch bestrahlung wurde in einem zweiten langzeitassay ( 14 tage ) geprft ( 100 ng / ml trail )  . 
effects of trail in combination with radiation on jurkat tcell lymphoma cells : the influence of trail on the eradication of clonogenic tumor cells was determined by a long - term assay . 
 da eine verbesserte apoptoseinduktion nicht zwangslufig mit einer optimierten eradikation klonogener tumorzellen assoziiert ist , wurde in weiterfhrenden experimenten die auswirkung einer kombinationsbehandlung auf das klonogene berleben gepr in den abbildungen 5 und 6 sind zwei charakteristische ergebnisse dargestellt : nach zeitgleicher behandlung einer plattenepithelkarzinomlinie ( scc4 ) mit trail und bestrahlung kann man deutlich erkennen , dass die krmmung der kurve nicht verndert wird . 
zelltodliganden in kombination mit ionisierender strahlung nicht als adhrente kolonien wachsen , ist die bestimmung des klonogenen berlebens nur indirekt ber die verwendung des so genannten well controll assays mglich [ 14 , 59 ]  . 
darber hinaus wurde eine erhebliche wachstumsverzgerung eines mcf - 7 - xenografts bei kombinierter behandlung mit trail und bestrahlung festgestellt . in einer weiteren studie wurde gezeigt , dass bestrahlung zu einer erheblichen sensibilisierung gegenber trail - induzierter apoptose bei erythroblastr differenzierten leukmien fhrt . 
 zusammengefasst legen die daten nahe , dass die kombination von trail mit bestrahlung nicht nur in vitro , sondern auch in ersten anstzen in vivo zu viel versprechenden ergebnissen gefhrt hat . trail und chemotherapie auch die effektivitt der chemotherapie ist hufig limitiert durch das auftreten von intrinsischen und erworbenen resistenzen der tumorzelllinie gegenber dem chemotherapeutikueine groe vielzahl von mechanismen kann eine medikamentenresistenz induzieren . 
 untersuchungen an chemotherapieresistenten tumorzelllinien ( ovarialkarzinom - , mesotheliom - , multiple - myelom - , nierenzellkarzinomzellen ) zeigten , dass trail alleine keinen oder nur einen geringen effekt auf die zellen ausbte . die kombination aus chemotherapie und trail konnte jedoch die resistenz der zelllinien durchbrechen und fhrte zu einer signifikanten apoptoseinduktion . 
die wirkungsverstrkung von trail in kombination mit chemotherapie wird wie bei ionisierender strahlung durch eine hochregulation der expression des trail - rezeptors dr5 erklrt [ 2 , 19 , 40 , 42 , 45 , 70 , 72 ]  . 
die mglicherweise fehlende toxizitt gegenber normalgewebe wird einerseits durch die kompetition der so genannten decoy - rezeptoren mit rezeptoren mit intakter zytoplasmatischer domne um den trail - liganden erklrt , andererseits wurde eine expression von caspase - 8 - inhibitoren wie c - flip in normalgewebe nachgewiesen [ 39 ]  . 
 weitere untersuchungen sind demnach notwendig , um die genauen molekularbiologischen ablufe von trail zu verstehen , um so eine sichere und tumorspezifische therapie auch in kombination mit chemotherapie oder bestrahlung zu ermglichen . 
da gezeigt wurde , dass die bestrahlung zu einer wirkungsverstrkung von trail fhrt , sind die untersuchungen auf diesem gebiet insbesondere auch an normalgewebszellen wichtig , da die fehlende toxizitt bei kombiniert fraktionierter behandlung belegt werden sollte , bevor ein klinischer einsatz erfolgen kann . 
 bei der forschung mit neuen substanzen ist zu bemerken , dass es bei der sich abzeichnenden groen zahl potentieller neuartiger substanzen schwierig sein wird , systematisierte vorgehensweisen zur festlegung der prioritt zu entwickeln . auch sind bislang keinerlei kriterien definiert worden , welche prklinischen grundvoraussetzungen erfllt sein mssen , bevor neue substanzen in studien mit bestrahlung geprft werden . 
in diesem zusammenhang ist zu hoffen , dass foren wie die eortc radiotherapy group mit der neuen translational research group werkzeuge generieren , die bei der bearbeitung der oben genannten problemstellung hilfreich sind . 
ashkenazi a , pai rc , fong s , leung s , lawrence da , marsters sa , blackie c , chang l , mcmurtrey ae , hebert a , deforge l , koumenis il , lewis d , harris l , bussiere j , koeppen h , shahrokh z , schwall rh . 
belka c , rudner j , wesselborg s , stepczynska a , marini p , lepple - wienhues a , faltin h , bamberg m , budach w , schulze - osthoff k . 
engels ih , stepczynska a , stroh c , lauber k , berg c , schwenzer r , wajant h , janicke ru , porter ag , belka c , gregor m , schulze - osthoff k , wesselborg s . 
flice , a novel fadd - homologous ice / ced - 3 - like protease , is recruited to the cd95 ( fas / apo - 1 ) death inducing signaling complex . 
paris f , fuks z , kang a , capodieci p , juan g , ehleiter d , haimovitz - friedman a , cordon - cardo c , kolesnick r . 
activation of caspase - 8 in drug - induced apoptosis of b - lymphoid cells is independent of cd95 / fas receptor - ligand interaction and occurs downstream of caspase - 3 . 
3 urban & vogel strahlentherapie und onkologie originalarbeit strahlentherapie benigner erkrankungen : morbus peyronie viktor meineke1 , christian uebler2 , frank - michael khn2 , heidelore hofmann2 , nils cordes1 , johannes ring2 , hermann - josef vogt2 hintergrund : die induratio penis plastica ( ipp ) oder der so genannte morbus peyronie ist eine fr den patienten sehr belastende erkrankung , die durch die leitsymptome induration , deviation und schmerz gekennzeichnet ist . 
 patienten und methoden : die dargestellten untersuchungsergebnisse beziehen sich auf die daten einer univarianten , retrospektiven untersuchung von 67 patienten , die in der dermatologischen klinik und poliklinik der technischen universitt mnchen im zeitraum von 1990 bis 1995 wegen einer ipp mit rntgenweichstrahlen behandelt worden sind . 
 ergebnisse : bei 58 von 67 der untersuchten patienten ( 86 , 6% ) konnte ein fortschreiten der erkrankung gestoppt werden , 25 von 67 patienten ( 37 , 3% ) klagten vor der therapie ber schmerzen , zumeist bei der erektion . 
es konnte gezeigt werden , dass der therapieerfolg signifikant mit krzerer anamnesedauer ( p < 0 , 05 ) , geringer plaquegre ( p < 0 , 025 ) und tendenziell niedrigerem alter des patienten korreliert . 
 schlsselwrter : induratio penis plastica morbus peyronie radiotherapie strahlenther onkol 2003 ; 179 : 1816 doii 10.1007 / s00066 - 003 - 0984 - 5 radiotherapy in benign diseases : morbus peyronie purpose : the induratio penis plastica ( ipp ) or the so - called morbus peyronie is a burdening disease for patients with three main symptoms , induration , deviation and pathe etiology of this fibrosing and plaque forming disease is largely unknown up to now . patients and methods : the presented data refer to a retrospective univariant examination of 67 patients , which have been treated for ipp with soft x - rays in the dermatological clinic of the technical university of munich between 1990 and 1995 . 
the aim of the study was to examine , how far a progression of the disease can be stopped with soft x - rays and how the pain symptomatic is reduced . 
it could be shown that therapeutic outcome significantly correlates to a shorter duration of anamnesis ( p < 0.05 ) , smaller plaque size ( p < 0.025 ) and a tendency to lower age of the patients . 
strahlentherapie bei induratio penis plastica einleitung mehr als 250 jahre nach der beschreibung durch ihren namensgeber franois de la peyronie ist die pathogenese der induratio penis plastica ( ipp ) oder peyronies disease noch immer umstritten [ 8 ]  . 
um den spontanen und therapeutisch beeinflussten krankheitsverlauf zu beschreiben und zu unterscheiden , ist es sinnvoll , diese kardinalsymptome standardisiert zu dokumentieren und zu beschreiben [ 2 , 3 , 12 ]  . 
abhngig von der strke oder dauer der entzndungsvorgnge erfolgt eine aktivierung der fibroblasten , wobei das normale produktionsverhltnis kollagen typ i / typ iii gestrt ist und exzessive mengen typ iii gebildet werden [ 25 ]  . bereits relativ frh treten kalkdepots auf , im weiteren verlauf kann es zur bildung von knorpelund knochenartigem gewebe als folge einer osteoblastischen metaplasie der gefendothelzellen in reaktion mit den kalzifizierten plaques kommen . 
verbessert und zu einer etablierten und bewhrten therapieform weiterentwickelt wurde diese bestrahlungsform durch die so genannte moulagentechnik , bei der radiumtrger oder iridium in wachsplatten eingebracht werden , die den penis umhllen [ 13 ]  . 
 in dieser arbeit sollen die ergebnisse des seit vielen jahrzehnten in unserer klinik auf der von holthusen und molineus 1951 [ 28 ] beschriebenen methode basierenden therapieverfahrens , der behandlung der ipp mit rntgenweichstrahlen , retrospektiv auf ihre wirksamkeit berprft werden [ 23 ]  . 
 patienten und methoden die folgende retrospektive untersuchung bezieht sich auf die daten von 67 patienten ( tabelle 1 ) , die in der dermatologischen klinik und poliklinik der technischen universitt mnchen im zeitraum von 19901995 wegen einer ipp mit rntgenweichstrahlen in behandlung waren . 
 anzahl der patienten alter bis 29 jahre alter bis 39 jahre alter bis 49 jahre alter bis 59 jahre alter bis 69 jahre alter bis 79 jahre morbus dupuytren knuckle pads morbus ledderhose diabetes mellitus schmerzen bei erektion schmerzen bei geschlechtsverkehr schmerzen bei druck / berhrung in ruhe erschwerte immissio mangelnde gliedsteife libidoverlust strahlenther onkol 2003 no . 
total number and size of indurations . indurationen solitr zwei drei vier gre 1 ( cid : 1 ) 1 cm gre bis 2 ( cid : 1 ) 2 cm gre bis 2 ( cid : 1 ) 4 cm gre 2 ( cid : 1 ) 4 cm keine angabe nach schwellkrperinjektionsstestung ( skit )  . 
den patienten wurde hierzu erklrt , dass ein rckgang der symptomatik um etwa 80% einem starken rckgang , ein rckgang um 50% einem mittleren rckgang und ein rckgang um lediglich 25% einem geringen symptomrckgang entspricht . 
die stadieneinteilungen beziehen sich nur zum teil auf andere in der literatur beschriebene klassifikationen [ 2 , 12 ]  . diese form der rntgenweichstrahlentherapie der ipp an unserer klinik wurde seit 1970 an bisher mehr als 700 patienten durchgefhrt . 
 die abhngigkeit des therapieerfolgs von beschwerdedauer , plaquegre und alter der patienten wurde mit dem ( cid : 1 ) 2 - test analysiert . radiotherapie / bestrahlungstechnik alle patienten wurden mit dem dermopan ii ( siemens , mnchen , deutschland ) bestrahlt . 
zustzlich erfolgt durch die druckanmie mit der cellonplatte eine strkere schonung des gewebes ( gerteeinstellungen : 50 kv , 1 , 0 mm aluminiumfilter , fokushautabstand 15 cm )  . 
nach jeweils einer 8 - wchigen pause wurde diese bestrahlung von 2 ( cid : 1 ) 4 gy bis zu einer gesamtdosis von blicherweise bis 32 gy wiederholt , im individualfall auch weniger . 
bei erneuter bestrahlung wegen neu aufgetretener plaques im alten strahlenfeld bei zwei patienten wurde die penishaut so verschoben , dass eine erneute strahlenbelastung der haut ber dem bereits bestrahlten erstherd vermieden wurde . 
 bei 58 patienten ( 86 , 6% ) konnte ein fortschreiten der erkrankung gestoppt werden , bei fnf patienten ( 7 , 5% ) kam der prozess auch durch die therapie zu keinem stillstand . 
bei 21 ( 84% ) dieser patienten fand sich ein meist vollstndiger rckgang , ausprgung der deviation anzahl der patienten richtung der deviation anzahl der patienten ergebnisse strahlenther onkol 2003 no . 
 von allen 60 patienten , die vor therapie eine penisdeviation aufwiesen , konnte bei 23 ( 38 , 3% ) eine besserung bzw . vollstndige rckbildung beobachtet werden ( tabelle 5 )  . 
 bei einem patienten stellte sich eine geringgradige besserung bereits kurz vor bestrahlungsbeginn eda dieser effekt nicht auf die therapie zurckzufhren ist , wurde der fall zustzlich unter keine angabe eingereiht . 
 ein vergleich der besserung von schmerz , induration und deviation bezglich ihres zeitlichen auftretens lsst erkennen , dass ein rckgang der schmerzen oft schon nach einem oder mehreren bestrahlungsdurchgngen zu verzeichnen war . 
influence of therapy on progression of ipp and pain . therapieeinfluss auf progression patienten fortschreiten konnte gestoppt werden fortschreiten konnte nicht gestoppt werden bereits vor therapie nicht mehr progredient gesamt therapieeinfluss auf schmerzsymptomatik vollstndige rckbildung gebessert stark mittel / wenig gleich strker gesamt tabelle 5 . 
palpatory findings of indurations and deviation after therapy . tastbefund indurationen befund deviation ( cid : 1 ) stark mittel wenig vollstndige rckbildung gebessert gleich schlechter stark mittel wenig ( cid : 1 ) 8 16 gesamt keine angaben vollstndig zurckgebildet regression weicher gleich grer gesamt keine angaben tabelle 6 . 
 eintreten der besserung schmerz induration deviation nach erster bestrahlung nach mehreren bestrahlungen gegen therapieende 3 monate nach therapieende > 3 monate nach therapieende gesamt keine angaben mehrere monate nach der letzten radiatio feststellbar ( tabelle 6 )  . 
 um zu berprfen , ob ein zusammenhang zwischen dem andauern der symptomatik und dem therapieerfolg besteht , erfolgte eine einteilung der patienten in eine gruppe mit beschwerdedauer bis einschlielich 6 monate und eine gruppe mit lngerer anamnese . 
 in der gruppe mit krzerer anamnesedauer lag die erfolgsquote signifikant hher ( p < 0 , 05 ) , whrend die anzahl der therapieversager unter anlegung strengster mastbe ( stationrer befund mit eingerechnet , was isoliert betrachtet gleichfalls als therapieteilerfolg zu betrachten wre ) dennoch weniger als ein viertel betrug . 
bei lngerer krankheitsdauer hingegen waren beide kategorien annhernd gleich stark vertreten . es zeigte sich ebenfalls , dass kleine indurationen ( als grenze wurde 1 cm2 festgelegt ) deutlich besser auf die therapie mit rntgenweichstrahlen ansprachen als grere ( p < 0 , 025 )  . 
 eine heilung im sinne einer reduktion aller symptome auf null lie sich sogar bei sieben patienten ( 10 , 4% ) erreichen . hufig war es die deviation , die trotz therapieerfolgen noch bestehen blieb . 
bei 29 patienten ( 43 , 3% ) konnte eine deutliche besserung ( starke bis vollstndige rckbildung mindestens eines leitsymptoms ) verzeichnet werden , bei zehn patienten ( 14 , 9% ) wurde ein mittel bis gering ausgeprgter rckgang der symptomatik erreicht . 
bei 16 patienten ( 23 , 9% ) war der befund stationr und bei fnf patienten ( 7 , 5% ) kam es zu einer verschlechterung . trotz abfilterung der strahlung durch die cellonschicht lsst sich dennoch eine restliche belastung der haut nicht vollstndig vermeiden . 
strahlentherapie bei induratio penis plastica scher nachkontrolle bei insgesamt sechs patienten , hiervon ein patient mit einem zweiten bestrahlungszyklus , einzelne diskrete teleangiektasien und minimale hyperpigmentierungen im bestrahlungsfeld festgestellt werden , die jedoch fr die patienten weder ein gesundheitliches noch ein kosmetisches problem darstellten . 
hiervon befand sich ein patient gleichfalls im zweiten bestrahlungszyklus und zeigte einen beginnenden lichen sclerosus et atrophicus mit sekundrer passagerer vorhautblutung , die nicht im zusammenhang mit der bestrahlungstherapie stand . 
 in dieser studie waren die bewertungskriterien fr einen erfolg der rntgenweichstrahlentherapie ein fortschreiten der erkrankung zu verhindern und die schmerzsymptomatik abzubauen sowie nach mglichkeit eine regression der plaques und die rckbildung der deviation zu erreichen . 
von den drei kardinalsymptomen der ipp induration , deviation und schmerz war der schmerz bei der erektion das am schnellsten und ausgeprgtesten reagierende sympto dies ist in bereinstimmung mit der literatur , in der eine besserung zwischen 80% [ 18 ] und 83% [ 10 ] angegeben wird . 
in der literatur werden 20%69 % [ 31 ] , im durchschnitt 57% [ 18 ] angegeben . es konnte gezeigt werden , dass der therapieerfolg von kurzer beschwerdedauer , geringer plaquegre und eher niedrigem alter des patienten jeweils positiv beeinflusst wird . auch in einigen frheren studien [ 18 ] konnte ein besseres ansprechen auf die bestrahlung beobachtet werden , wenn die anamnesedauer weniger als 6 monate betrug . 
 niedrigeres lebensalter korreliert auch in der literatur [ 5 ] mit besseren therapieerfolgen bei der ipp nach radiatio . andererseits wird gerade bei dieser altersgruppe ein akuterer und progressiverer verlauf der erkrankung beschrieben [ 27 ] , was besonders fr diese gruppe ein schnelles therapieren erforderlich macht . 
 die an sich sehr seltenen nebenwirkungen der rntgenweichstrahlentherapie ( rtung , hyperpigmentierung , teleangiektasiebildung ) traten selten und in der regel nur dann auf , wenn wegen einer neuerkrankung eine weitere radiatio erforderlich wurde und sich eine berschneidung der therapiefelder nicht vermeiden lie . 
naturgem knnen durch die radiotherapie nur ipp - bedingte sexualstrungen beseitigt werden , nicht jedoch andere ursachen , wie sie in der bevorzugten altersklasse der ipp in gleicher weise vorkommen wie in vergleichskollektiven [ 28 , 30 ]  . 
 eine radiatio einer ipp , sei es mit rntgenweichstrahlen oder der niedrigdosisstrahlentherapie mit der moulagentechnik , ist eine ausgesprochen nebenwirkungsarme , schmerzlose und einfach zu handhabende methode ohne systemische belastung . 
insofern stellt der langfristig bewiesene erfolg des verfahrens bei der ipp vergleichbaren erkrankungen wie dem morbus dupuytren ein zustzliches argument fr die radiotherapie als eine primre therapie der ipp dar [ 1 , 24 , 29 ]  . aus strahlenbiologischer sicht besteht besonderes interesse , die wirkung einer rntgenweichstrahlentherapie im gewebe zu erklren . 
zu klren ist , inwieweit hnliche oder gleiche mechanismen , die bei hohen strahlendosen zu einer fibrose fhren knnen bei niedriger strahlendosis antiinflammatorisch und damit antifibrotisch wirken knnen [ 11 ]  . 
 vorstellbar ist neben der beeinflussung der fibrose auch eine direkte oder indirekte wirkung auf entzndungszellen . so ist bei florider ipp stets eine derb - elastische plaque als zeichen einer entzndlichen reaktion um die eigentliche induration zu tasten . 
denkbare pathomechanismen einer strahlentherapie bei ipp wren daher auch ein direkter antientzndlicher effekt im sinne einer direkten beeinflussung des entzndlichen infiltrats durch proliferationshemmung oder aber indirekt ber eine makrophagenaktivierung durch bestrahlung und konsekutive abrumung des infiltrats bei niedriger strahlendosis [ 16 ]  . 
3 urban & vogel strahlentherapie und onkologie original article psychosocial stress in cancer patients during and after radiotherapy susanne sehlen1 , helmuth hollenhorst1 , beatrice schymura1 , peter herschbach2 , uelker aydemir3 , martina firsching1 , eckhart dhmke1 background and purpose : the aim of this study was to investigate stress in tumor patients by means of a cancer - specific questionnaire in the course of radiotherapy . 
 material and methods : disease - specific aspects of psychosocial stress ( herschbachs questionnaire on stress in cancer patients , qsc ) were self - assessed by patients with different tumor types before radiotherapy ( ti1 ) , after radiotherapy ( ti2 ) , and 6 weeks after the end of radiotherapy ( ti3 )  . 
we investigated 265 of 446 patients ( 157 male , 108 female ; median age 58.6 years ) with complete data of ti1ti3 . results : in the course of investigation , the most prominent stress scale of the patients proved to be physical efficiency , without significant changes during treatment and after therapy . 
 conclusion : patients who experienced stress at the beginning of radiotherapy also had the same or increased levels of stress during and shortly after treatment and needed permanent psychosocial support to improve quality of life . 
 key words : psychosocial stress radiotherapy psychooncology prediction of stress quality of life strahlenther onkol 2003 ; 179 : 17580 doi 10.1007 / s00066 - 003 - 1018 - z psychosoziale belastung von tumorpatienten whrend und nach einer strahlentherapie hintergrund und fragestellung : ziel dieser studie war es , die psychosoziale belastung von tumorpatienten mit hilfe eines krebsspezifischen fragebogens zu untersuchen und die vernderungen im verlauf festzuhalten . material und methodik : krankheitsspezifische aspekte psychosozialer belastung ( herschbachs fragebogen zur belastung von krebskranken patienten , fbk ) wurden zu beginn ( ti1 ) , nach abschluss der strahlentherapie ( ti2 ) und 6 wochen spter ( ti3 ) von patienten mit unterschiedlichen tumorerkrankungen selbst eingeschtzt . 
von 446 patienten , die die einschlusskriterien erfllten , untersuchten wir 265 ( 157 mnner , 108 frauen ; medianes alter 58 , 6 jahre ) mit kompletten daten von ti1 bis ti3 . ergebnisse : im verlauf gleich bleibend am hchsten war die belastung durch einschrnkung der physischen leistungsfhigkeit . es wurden signifikante anstiege von angst , schmerzen und informationsdefiziten zwischen ti1 und ti3 beobachtet ( p < 0 , 001 , p = 0 , 001 , p = 0 , 035 )  . 
 schlussfolgerung : eine lang anhaltende psychosoziale untersttzung erscheint durch gleich bleibend hohe oder ansteigende belastungswerte whrend und nach einer radioonkologischen behandlung dringend erforderlich , um die lebensqualitt zu erhhen . dabei kann eine frhzeitige identifizierung von belasteten patienten hilfreich se schlsselwrter : psychosoziale belastung strahlentherapie psychoonkologie vorhersagbarkeit einer belastung lebensqualitt 1 department and polyclinic of radiotherapy , klinikum grohadern , ludwig maximilians university , munich , germany , 2 institute and polyclinic of psychosomatic medicine , psychotherapy and medical psychology , technical university , munich , germany , 3 institute of biometrics and epidemiology , klinikum grohadern , ludwig maximilians university , munich , germany . 
empiric studies on the extent of psychosocial stress among cancer patients have produced inconsistent results [ 3 , 5 , 13 , 22 , 26 ]  . only a few of these studies are representative of a radiotherapy treatment schedule . 
patients entering radiotherapy have been found to show significantly elevated levels of psychopathologic symptomatology [ 7 ] and continue thinking about their illness and treatment modalities over a long period [ 18 ]  . 
this is because they suffer from specific stresses such as the fear of the first radiotherapy session , the size of radiotherapeutic devices , the fear of side effects and of meeting other tumor patients . 
these observations of disease - specific stress and ways of coping with it ( coping and defense mechanisms ) are important factors that can affect the quality of life ( qol ) of tumor patients during radiotherapy [ 22 ]  . 
for prophylactic psychosocial intervention at the beginning of radiotherapy , the early identification of patients with increasing stress levels is of decisive importance [ 12 , 19 ]  . the aim of this prospective study therefore was to assess the changes in specific stresses in tumor patients during and after radiotherapy and the influence of medical and sociodemographic variables on stress . 
 material and methods at the beginning of radiotherapy ( ti1 ) , at the end of radiotherapy ( ti2 ) , and 6 weeks after the end of radiotherapy ( ti3 ) , the participating patients filled in the psychometrically tested instrument questionnaire on stress in cancer patients ( qsc ) [ 9 ]  . 
reliability analysis on a sample of cancer patients ( n = 1 , 645 ) with various diagnoses resulted in the following homogeneity values ( cronbachs alpha ) for the six scales of the qsc : scale 1 : pain , four items , alpha 0.73 ; scale 2 : anxiety / psychologic distress , ten items , alpha 0.89 ; scale 3 : information , five items , alpha 0.77 ; scale 4 : physical efficiency , five items , alpha 0.86 ; scale 5 : social behavior ; scale 6 : partnership / family , nine items : alpha 0.79. 
an indication of the validity can be gathered from pearsons product - moment correlation of the qsc total score , with the following psychometric values ( level of significance p < 0.001 ) : sf36 physical component summary : r = 0.53 ; sf36 mental component summary : r = 0.64 ; scl - 90 - r global severity index : r = 0.77 ( n = 171 breast cancer patients of a rehabilitation hospital )  . 
 between november 1997 and may 1999 , 732 patients at the department of radiotherapy , klinikum grohadern , ludwig maximilians university , munich , germany , were screened for the study . 
6 weeks after the end of radiotherapy , another 3.8% of the participants were excluded from the study : 1.5% had died , 1.8% could not continue because of decreased kps , and 0.5% were excluded for organizational reasons . 
to ensure that our analysis was not influenced by selection bias , the distribution of patients into participants and nonparticipants was assessed by means of the ( cid : 1 ) 2 - test . 
on evaluating the individual items during the course of treatment , it was noticeable that at ti2 fear of disease progress ( p = 0.001 ) , not being able to care for the family in future ( p = 0.002 ) , fear of becoming helpless ( p = 0.001 ) , fear of pain ( ti1 : 1.71 , ti2 : 1.52 , ti3 : 1.81 ; p = 0.003 ) , and fear of death ( ti1 : 1.40 , ti2 : 1.21 , ti3 : 1.43 ; p = 0.005 ) were lower than they were at ti1 and ti3 . 
by contrast , the stress level for feeling flabby and weak ( ti1 : 1.85 , ti2 : 2.18 , ti3 : 2.21 ; p = 0.001 ) and relationship to doctors ( ti1 : 0.37 , ti2 : 0.60 , ti3 : 0.62 ; p = 0.005 ) steadily increased throughout the study . 
 correlation with medical and sociodemographic variables we investigated the factors sex , age , tnm category , and tumor groups with regard to changes of stress levels in the course of radiotherapy . 
the other diagnosis groups remained constant throughout the observation period ( figure 2 )  . age , tumor stages , and lymph node metastases played no essential role in the stress measurements during the follow - up qsc total score investigations . 
patients with an addiction to alcohol or nicotine had a 7.7 - fold higher risk compared to patients without such addictions ; patients at an advanced tumor stage had a 4.8 - fold higher risk compared with patients at early stages ; patients with a metabolic disorder and patients > 60 years had a 2.8 - fold and 2.3 - fold higher risk and married patients a 0.3 - fold lower risk of increasing stress factors . 
the probability of correctly predicting increase in stress ( sensitivity ) 6 weeks after the start of radiotherapy was 78% and the probability of correctly predicting decrease in stress ( specificity ) was 67% with the variables tumor stage , marital status , addiction to alcohol or nicotine , metabolic disorder , and age . 
the herschbach questionnaire ( qsc ) [ 9 ] was specifically developed for studying cancer patients and is therefore an especially suitable instrument for assessing psychosocial stress in patients during radiotherapy . 
the few data from recent studies have demonstrated that stress in tumor patients is high at the beginning of radiotherapy [ 25 ] and decreases in the course of treatment [ 15 , 19 , 20 , 21 ]  . 
we saw an increase in stress factors on the scales for pain , anxiety , and information and a constant high level of stress due to restriction of physical efficiency from ti1 to ti3 . after the acute phase of treatment , when the close relationship to health professionals was over , the fear of not being able to control the disease , the accompanying loss of physical fitness , and the resulting restrictions in the social environment increased . 
according to andersen [ 1 ] , anxiety remains the same even after several treatment cycles and is reactivated after an interval by each new confrontation with the aftercare setting . 
we observed a significant increase in the qsc total score from ti1 to ti3 in women and men , whereas irwin et al [ 14 ] saw a reduction in stress symptomatology from the onset of radiotherapy until the end of treatment . 
the influence of these medical criteria on stress levels has also been observed by other authors [ 10 ]  . patients with breast cancer had the highest stress levels for all factors assessed . 
at the beginning of radiotherapy , patients with head and neck cancer showed low levels of stress , but 6 weeks after the end of radiation , they demonstrated high stress levels . 
it is reasonable to assume that those who refused to participate were no less psychologically reactive than other patients and that our patient sample was representative of a university radiotherapy department . 
it will hasten recovery and rehabilitation as shown in head and neck cancer patients [ 4 ] and can alert physicians to those patients at risk of high levels of stress and poor posttreatment adaptation . 
in contrast to timeconsuming and costly psychologic evaluation we found that by using only five pretreatment variables , increase in stress could be predicted in patients 6 weeks after the start of radiotherapy : patients with advanced tumor stages , patients with addiction to alcohol or nicotine , patients who had a metabolic disorder , elderly patients , and patients who were single , divorced or widowed were at risk of increased stress after radiotherapy and needed additional attention and support to prevent further psychologic morbidity . 
although there are more precise methods of predicting stress in patients without taking into consideration the total number of patients , we decided on this model because the variables were confirmed by our clinical experience . 
 to our knowledge , this study is the first prospective trial to report stress symptomatology associated with radiotherapy before onset and 6 weeks after treatment in a large number of patients using all relevant medical and sociodemographic data and a cancer - specific questionnaire . 
 strahlentherapie und onkologie original article inhibition of the inos pathway in inflammatory macrophages by low - dose x - irradiation in vitro is there a time dependence ? guido hildebrandt1 , gabriela loppnow1 , jutta jahns1 , marion hindemith1 , ulf anderegg2 , anja saalbach2 , friedrich kamprad1 background : low radiation doses ( 1.25 gy ) , if applied 6 h before or after stimulation , are known to inhibit the inducible nitric oxide synthase ( inos ) pathway in inflammatory macrophages in vitro . 
we therefore investigated the time dependence and the underlying molecular mechanism of this effect , since it may be involved in the clinically observed anti - inflammatory and analgesic efficacy of low - dose radiotherapy . 
 material and methods : metabolic activity , nitric oxide ( no ) production , inosand hemoxygenase 1 - ( ho - 1 - ) protein and - mrna expression by macrophages in vitro after stimulation with lps / ifn - ( cid : 1 ) ( 0.1 g ml1 / 100 u ml1 ) were investigated . 
a dose - dependent modulation of the cumulative no production was observed with significant inhibition by low radiation doses ( 1.25 gy ) and return to control level and even higher concentrations by higher doses ( 5 gy )  . 
 conclusion : the inhibitory interference of low radiation doses with the inos pathway in inflammatory macrophages appears to be based on radiation effects on the translational and posttranslational control mechanisms of inos activity . 
however , contrary to our working hypothesis this is not related to radiation - induced induction of ho - 1 expression and thereby increased degradation of heme which is essential for inos activity . 
 key words : inflammation low - dose radiotherapy macrophages inducible nitric oxide synthase ( inos ) hemoxygenase - 1 ( ho - 1 ) proteasome strahlenther onkol 2003 ; 179 : 15866 doi 10.1007 / s00066 - 003 - 1044 - x inhibition der inos - aktivitt inflammatorischer makrophagen durch niedrig dosierte bestrahlung in vitro . 
gibt es eine zeitabhngigkeit ? hintergrund : niedrige strahlendosen ( 1 , 25 gy ) , wenn 6 h vor oder nach zellstimulation appliziert , knnen die aktivitt der induzierbaren stickoxidsynthase ( inos ) inflammatorischer makrophagen in vitro inhibieren . 
 material und methodik : metabolische aktivitt , kumulative stickoxid - ( no - ) produktion , inosund hmoxygenase - 1 - ( ho - 1 - ) proteinund - mrna - expression durch makrophagen wurden nach stimulation mit lps / ifn - ( cid : 1 ) ( 0 , 1 g ml1 / 100 u ml1 ) in vitro untersucht . 
es wurde eine dosisabhngige , diskontinuierliche modulation der kumulativen no - produktion mit signifikanter inhibition durch niedrige strahlendosen ( 1 , 25 gy ) und rckkehr zu kontrollwerten oder hheren konzentrationen nach dosen 5 gy beobachtet . 
das ausma 1 department of radiotherapy and radiooncology , and 2 department of experimental dermatology , university of leipzig , germany . received : may 8 , 2002 ; accepted : october 25 , 2002 strahlenther onkol 2003 no . 
die inosmrna - expression blieb 318 h nach stimulation und unmittelbar anschlieender bestrahlung mit dosen 1 , 25 gy unbeeinflusst . die inos - protein - expression war 624 h nach stimulation und unmittelbar anschlieender bestrahlung mit dosen 1 , 25 gy vermindert . 
im gegensatz zu unserer arbeitshypothese ist dies nicht durch eine induktion des stressproteins ho - 1 durch niedrige dosen und die dadurch bedingte gesteigerte degradation von hm als essentiellem oxidativem kofaktor der inos - aktivitt zu erklren . 
andere posttranslationelle modifikationen wie der proteasom - degradations - pathway knnten involviert se schlsselwrter : entzndung niedrig dosierte strahlentherapie makrophagen induzierbare stickoxidsynthase ( inos ) hmoxygenase - 1 ( ho - 1 ) proteasom introduction in many european countries , radiation therapy of a variety of painful joint diseases with total doses between 1.5 and 6 gy is still practiced on a large scale as the most effective and least toxic treatment , for example in insertion tendinitis , periarthritis humeroscapularis and osteoarthritis [ 13 , 18 , 28 , 29 ]  . 
by contrast , little is known about possible mechanisms underlying these clinical observations [ 25 , 32 , 33 ] , and experimental investigations are rare . recently , we investigated in vitro low - dose radiation effects on resting and activated macrophages with special emphasis on the inducible nitric oxide synthase ( inos ) pathway , a key enzyme in the inflammatory response [ 16 ]  . 
in addition , we demonstrated , using the air pouch model in mice in vivo , that low radiation doses interfere with the inos and the hemoxygenase 1 ( ho - 1 ) pathway [ 17 ]  . 
 the aim of this study was to explore , whether this inhibitory efficacy is dependent on the time of irradiation in relation to the time of activation and , moreover , whether there are also detectable changes on the transcriptional level . 
to distinguish between preand posttranscriptional / - translational effects , irradiation of macrophages was performed either 6 , 4 , or 2 h before stimulation , immediately after stimulation ( 0 h ) , or 2 , 4 , and 6 h after stimulation . 
 materials and methods cell culture raw 264.7 macrophages were obtained from the european collection of cell cultures ( salisbury , uk ) and maintained in dulbeccos modified eagles medium ( dmem ) , supplemented with 10% fetal calf serum ( fcs , heat - inactivated ) , 2% ascorbic acid and penicillin / streptomycin ( 100 u / 100 g ml1 ) at 37 c . when 90% confluent , cells were removed and adjusted to a concentration of 3 ( cid : 2 ) 105 cells / ml and either seeded into 96 - well plates ( 200 l / well ; griess assay , mtt assay ) or t75 ( western blot analysis ) or t25 - culture flasks ( northern blot analysis )  . 
dosimetry was carried out in air using a 0.1 cm3 sealed ionization chamber ( model 2332 ) connected to the integrating dosimeter ptw dl4 / di4 ( ptw pychlau , freiburg , germany ) , calibrated against a secondary standard . 
the results were expressed as mean absorbance550 nm690 nm of sample / mean absorbance550 nm690 nm of control sem ( cid : 2 ) 100% ( n = 6 )  . 
an equal volume of laemmli gel loading buffer [ 4% sodium dodecyl sulphate ( sds , biorad laboratories ltd . , hercules , ca , usa ) , 20% glycerol , 10% 2 - mercaptoethanol , 2 mm edta , 1 mg ml1 of coomassie brilliant blue in 0.125 m tris / hcl ] was added , thus diluting samples to 1 mg ml1 of protein before the samples were eventually boiled for 5 m samples ( 10 l protein / lane ) were loaded on 7.5% or 15% gels for sds - page . 
the membranes were incubated in polyclonal rabbit anti - mouse inos ( 1 : 5 , 000 dilution , santa cruz , ca , usa ) , and polyclonal rabbit anti - rat ho - 1 ( 1 : 2 , 000 dilution , stress gen biotechnologies , victoria , bc , canada )  . 
a horseradish peroxidase - ( hrp - ) conjugated secondary antibody ( goat anti - rabbit igg - hrp , 1 : 20 , 000 dilution ) was used from the ecl system ( santa cruz , ca , usa )  . 
 northern blot analysis 3 , 6 , and 18 h following irradiation and stimulation of flasks ( group e ) , rna for northern blot analysis was prepared with the perfect rna mini kit ( eppendorf , hamburg , germany ) according to the original protocol . 
the time of lps / ifn - ( cid : 1 ) stimulation is marked as time 0 ( open triangle ) , the different times of irradiation are marked by arrows ( groups ah ) , the time points of sampling for analysis ( griess assay , mtt assay , western blot , northern blot ) by closed circles . 
der zeitpunkt der lps / ifn - ( cid : 1 ) - stimulation entspricht 0 h ( offenes dreieck ) , die verschiedenen bestrahlungszeitpunkte sind mit pfeilen ( gruppen ah ) , die zeitpunkte der probenentnahmen ( griess - assay , mtt - assay , westernblot , northernblot ) mit geschlossenen kreisen gekennzeichnet . 
 the assay of cumulative no production using the griess reaction all experiments for cumulative nitrite measurements were performed as time courses over 30 h with 3 - h sampling intervals . 
this was assessed spectrophotometrically after addition of 100 l griess reagent [ 1% sulfanilamide and 0.1% n - ( 1 - naphthyl ) ethylenediamine in 5% o - phosphoric acid ] to an equal volume of sample medium in 96 - well plates . 
optical densities were measured by dual wavelength analysis ( 550 nm 690 nm ) in a plate reader ( spectra - classic , tecan , crailsheim , germany ) , medium containing a range of known sodium nitrite concentrations was used to calibrate the experimental data and to calculate absolute nitrite concentrations by linear regression . 
 metabolic activity assay metabolic activity was assessed in parallel with the griess assay by the 3 - [ 4 , 5 - dimethylthiazol - 2 - yl ] - 2 , 5 - diphenyl - tetrazolium bromide ( mtt ) dehydrogenation assay . 
in each well the medium was replaced by 100 l mtt solution ( 0.5 mg ml1 ) for 15 min , followed by complete removal of the mtt solution and two washes with dpbs - a . 
as recently reported [ 16 ] , radiaitself with doses between 0 and 10 gy tion effects on no2 could be entirely excluded . cumulative no2 production of raw 264.7 macophages irradiated 6 , 4 , or 2 h before stimulation ( groups bd )  . 
after drying , the membrane was uv - crosslinked for 2 m northern blots were hybridized with digoxigenin - labeled in vitro transcription products from cdna clones for inos or ho - 1 . 
the following primer pairs were used : 5 ( cid : 3 ) ccatggaacatcccaaatac 3 ( cid : 3 ) ; sense primer : antisense primer : 5 ( cid : 3 ) tctgcatgtacttcatgaagg 3 ( cid : 3 )  . the cdna clone for ho - 1 had been generated by cloning of rt - pcr product ( bases 586932 ) into a pbluescript vector . the following primer pairs were used : 5 ( cid : 3 ) aggccatggccttgcccagc 3 ( cid : 3 ) ; sense primer : antisense primer : 5 ( cid : 3 ) gagcggtgtctgggatgagc 3 ( cid : 3 )  . ethidium - bromide - stained 18s rna , 28s rna and a gap - dh probe were used as internal standards for normalization of loaded rna . 
the detection of hybridization bands was performed by incubation of the membranes with antidig - fab fragments , conjugated to alkaline phosphatase ( boehringer , mannheim , germany )  . 
 results radiation effects on viability of raw 264.7 macrophages in resting cells ( group a ) , radiation doses 0.6 gy resulted in a significant dose - dependent decrease in mtt dehydrogenation within the first 6 h after irradiation , followed by a steep increase between 6 and 12 h for all doses . 
however , in line with previous experiments [ 16 ] , metabolic activity of activated raw 264.7 macrophages ( groups bh ) was not affected by radiation doses 10 gy ( data not shown )  . 
 radiation effects on the cumulative no release of raw 264.7 macrophages production of raw 264.7 macrophages ircumulative no2 radiated 6 h after complete medium change ( group a )  . 
dose - dependent cumulative nitrite production by raw 264.7 macrophages irradiated 6 , 4 , 2 , or 0 h before lps / ifn - ( cid : 1 ) stimulation ( 0.1 g ml1 / 100 u ml1 ; groups be )  . 
dose - dependent cumulative nitrite production by raw 264.7 macrophages irradiated either 6 , 4 , 2 h before or 0 , 2 , 4 , 6 h after lps / ifn - ( cid : 1 ) stimulation ( 0.1 g ml1 / 100 u ml1 ) at 30 h after cell activation . 
dosisabhngige kumulative no2 raw - 264.7 - makrophagen , die entweder 6 , 4 , 2 h vor oder 0 , 2 , 4 , 6 h nach lps / ifn - ( cid : 1 ) - stimulation ( 0 , 1 g ml1 / 100 u ml1 ) bestrahlt wurden , zum zeitpunkt 30 h nach zellaktivierung . 
dose - dependent cumulative nitrite production by raw 264.7 macrophages irradiated 0 , 2 , 4 , or 6 h after lps / ifn - ( cid : 1 ) stimulation ( 0.1 g ml1 / 100 u ml1 ; group eh )  . 
again , radiaconcentrations tion doses of 510 gy resulted in higher no2 compared with the unirradiated control , and the degree of release inhibition did not depend on the time point of irradiation after cell activation within the chosen time window of 6 h . 
this suppression was found regardless whether radiation was applied before or after stimulation , but the shorter the interval between radiation and stimulation , the more pronounced was the suppressive effect ( figure 4 )  . 
we could recently demonstrate that in activated raw 264.7 macrophages irradiated 6 h after stimulation , the detected inos - protein level 18 h after stimulation was decreased by low radiation doses , yet there was no change after higher doses [ 16 ]  . 
 to determine the kinetics of inos - protein expression , western blot analysis was performed 624 h after stimulation and subsequent irradiation ( group e ) with doses of 010 gy . irradiation of lps / ifn - - activated macrophages with doses of 0.61.25 gy reduced inos - protein expression at all times after stimulation , yet the maximum inhibitory effect was observed 12 h after cell activation and irradiation . 
densitometric results are relative mean sem of twelve samples from three independent experiments ( n = 4 / experiment ) as compared to the shamirradiated stimulated control ( 0 gy )  . 
die densitometrischen angaben entsprechen den relativen mittelwerten se von zwlf proben aus drei unabhngigen experimenten ( n = 4 / experiment ) im vergleich zur scheinbestrahlten stimulierten kontrolle ( 0 gy )  . 
modulation of inos activity by low - dose x - irradiation inos - mrna expression of activated raw 264.7 macrophages ( group e ) to determine the kinetics of inos - mrna expression , northern blot analysis was performed 318 h following stimulation and subsequent irradiation with doses of 010 gy ( group e )  . the northern blot analysis demonstrates , that irradiation in the dose range of 010 gy immediately after lps / ifnstimulation of raw 264.7 macrophages does not affect the inosmrna expression pattern 318 h after activation in any way which could be related to protein expression ( figure 5 )  . ho - 1 - protein expression of activated raw 264.7 macrophages ( group e ) in contrast to our working hypothesis , ho - 1 - protein levels in activated and subsequently irradiated raw 264.7 macrophages were not increased after low radiation doses . 
they showed a similar time and dose dependence as inos - protein expression within the investigated dose range of 010 gy with the exception of the 18 - h time point , where a small increase in the ho1 - protein level was observed after 0.6 gy ( data not shown )  . ho - 1 - mrna expression of activated raw 264.7 macrophages ( group e ) as for ho - 1 - protein levels in activated and irradiated raw 264.7 macrophages , there was no detectable induction of ho1 - mrna expression with low doses , but a more or less comparable timeand dose - dependent kinetics as for ho - 1 - protein expression within the investigated dose range of 010 gy ( data not shown )  . 
 discussion previously published experimental work of our group demonstrated that low radiation doses ( 0.61.25 gy ) suppress the inos system of activated macrophages , a key enzyme in the inflammatory response [ 16 ]  . 
furthermore , the anti - inflammatory efficacy of low - dose x - irradiation could be clinically and histologically confirmed in experimental models of osteoarthritis [ 12 ] and rheumatoid arthritis [ 14 ]  . 
recently , schaue et al [ 27 ] investigated the effects of low radiation doses on oxidative burst activity of murine raw 264.7 macrophages after pma ( phorbol myristate acetate , 106 m ) or zymosan ( 0.5 mg ml1 ) stimulation [ 27 ]  . 
one of the functions of inflammatory macrophages is the expression of inos which , through synthesis of no , is involved in numerous physiologic and pathologic processes , plays an important role in macrophage - mediated cytotoxicity , and fulfills mediator functions during the inflammatory response [ 1 ]  . 
sustained no overproduction contributes to persistent inflammation and tissue destruction [ 19 ]  . several investigators have already demonstrated that no is locally increased in arthritic joints of patients with rheumatoid arthritis and osteoarthritis [ 3 , 30 ] , and that no plays a pathophysiologic role for both arthritic diseases [ 4 , 11 ]  . 
 in macrophage - driven experimental arthritis models , pharmacologic inhibition of no production clinically and histologically attenuates rheumatoid arthritis and osteoarthritis [ 37 ] and , furthermore , considerably reduces important catabolic factors such as collagenase 1 ( mmp - 1 ) , stromelysin 1 ( mmp - 3 ) , il - 1 ( cid : 2 ) , peroxynitrite as well as cyclooxgenase 2 ( cox - 2 ) expression [ 5 , 23 ]  . 
 based on our experimental data obtained , we hypothesized that the inhibitory effect of low radiation doses on the no pathway might be one radiobiological mechanism underlying the clinically observed efficacy of anti - inflammatory radiotherapy and might result in the reduction of swelling as well as relief of pain [ 16 ]  . 
to get further insight and to test this hypothetical mechanism , we investigated in vitro whether this inhibitory efficacy depends on the time of irradiation in relation to the time of activation . 
furthermore , based on the in vivo observation that the decreased inos - protein expression is accompanied by an increased ho - 1 - protein expression [ 17 ] , we analyzed in parallel radiation effects on inosand ho - 1mrna and - protein expression in stimulated raw 264.7 macrophages , to prove this experimental observation in vitro . following low - dose irradiation ( 0.31.25 gy ) , there was no obvious effect on tnf - - synthesis of lps / ifn - - activated macrophages [ 16 ] , and the dose - dependent depression of no release occurred whether macrophages were irradiated 6 h prior to activation or 6 h afterwards . 
therefore , it seems to be unlikely that inos suppression occurred at the transcriptional level since , within 24 h after lps and / or ifnstimulation , a substantial increase in inos activity is induced [ 9 ]  . 
 the northern and western blot analyses demonstrated that inos - mrna , ho - 1 - mrna , and ho - 1 - protein expression following doses 1.25 gy remained unchanged 324 h after cell activation and subsequent irradiation , but inos - protein expression after low dose irradiation ( 0.31.25 gy ) was significantly reduced . 
modulation of inos activity by low - dose x - irradiation all isoforms of nitric oxide synthase have a bidomain structure : an oxygenase domain within the amino - terminal half which contains thiolate - bound heme and a reductase domain within the carboxy - terminal half , with a 3040% homology to cytochrome p450 reductase [ 20 ]  . 
each subunit is thought to attach at least five other molecules besides the three cosubstrates ( l - arginine , nadph , o2 ) and the partner monomer , namely heme , tetrahydrobiopterin , calmodulin , and the flavins fmn and fad [ 20 ]  . 
thus , at least 17 binding reactions are required to assemble a 300 - kd homodimer ( 300 - kd enzyme ) to generate a 30 - d product [ 19 ]  . 
heme depletion may also account for the loss of inos enzyme activity in macrophages that contained normal amounts of inos protein after prolonged culture following a single application of ifnand lps [ 35 ]  . 
 several stimuli transcriptionally induce ho - 1 expression [ 10 ] , which catalyzes the catabolism of heme to equimolar quantities of carbon monoxide , iron and bilirubin and therefore may reduce the availability of the essential oxidative cofactor heme . 
 therefore , we investigated in vitro , whether radiation - induced expression of the stress protein ho - 1 could explain the observed modulation of inos activity after low - dose irradiation of activated macrophages . 
the increased ho - 1 expression and decreased inos expression after low - dose irradiation of chronic granulomatous tissue [ 17 ] and arthritic joints [ 15 ] in vivo would confirm this hypothesis . contrary to the in vivo results , in vitro neither ho - 1 - protein nor ho - 1 - mrna expression was increased after lowdose irradiation ( 0.31.25 gy ) of activated macrophages . thus , the observed modulation of inos activity at least in murine raw264.7 macrophages in vitro cannot be explained through radiation - induced expression of the stress protein ho - 1 and thereby reduced availability of the essential oxidative cofactor heme . 
cytokines like tnfand ifnas well as lps and other bacterial cell wall products transcriptionally stimulate inos - gene expression in macrophages [ 19 ] , although there may be an additional effect on mrna stability . the mouse inos promoter consists of two clusters of regulatory elements . 
a proximal region functions as the basal promoter containing an octamer element and an nf ( cid : 4 ) b - binding site , which mediates responsiveness to lps . 
the distal region functions as an enhancer element and responds to lps and ifnthrough nf ( cid : 4 ) b , interferon regulatory factor - 1 , interferon - stimulated response element , and ifn - - activation site binding sites . 
 one of the most important transcription factors for gene expression of cytokines , adhesion molecules , chemokines , growth factors , and inducible enzymes is nf ( cid : 4 ) b [ 31 ]  . 
degradation of i ( cid : 4 ) b frees nf ( cid : 4 ) b for translocation to the nucleus and activation of the transcription of nf ( cid : 4 ) b - dependent target genes such as inos [ 31 ]  . 
 pajonk & mcbride [ 22 ] have recently shown cell type - independent , direct radiation effects on the proteolytic activity of the 26s proteasome , and thus could identify the 26s proteasome as a possible direct target structure of irradiation . 
they found that low radiation doses ( 2.0 gy ) reduce the proteolytic activity of the 26s proteasome in constitutively nf ( cid : 4 ) bexpressing ecv cells and that doses < 0.5 gy cause an increase in the i ( cid : 4 ) b - protein concentrations [ 22 ]  . 
moreover , musial & eissa [ 21 ] have demonstrated that the proteasome pathway is the primary degradation pathway for human and murine inos and that the 26s proteasome can regulate inos activity either on the transcriptional and / or the posttranslational level . 
since the 26s proteasome is responsible for selective atpand ubiquitin - dependent degradation of all short - lived and 7090% of all long - lived cellular proteins [ 7 ] , including key molecules of signal transduction , cell cycle control and immune response , this observation is an important focus for further experimental investigations . 
in vitro studies with primary murine macrophages demonstrated that the anti - inflammatory cytokine tgf - ( cid : 2 ) 1 destabilized inos mrna , retarded the synthesis of inos protein and accelerated its degradation [ 34 ]  . 
whether low - dose irradiation also transcriptionally induces a relative maximum in tgf - ( cid : 2 ) 1 - production in stimulated macrophages as already demonstrated in activated miend1 - endothelial cells [ 26 ] , and if such an effect might by responsible for the observed suppression of inos protein and no production is currently investigated . 
 conclusion in comparison to higher radiation doses , low - dose x - irradiation ( 0.61.25 gy ) has contrary effects on the functional abilities of activated macrophages and suppresses inos - protein expression and cumulative no production without affecting inos - gene expression . 
further investigations are currently performed , to clarify the role of the stress protein ho - 1 [ 10 ] , the anti - inflammatory cytokine tgf - ( cid : 2 ) 1 [ 34 ] , and the protestrahlenther onkol 2003 no . 
in vivo measurement of the rectal dose was performed with thermoluminescent dosimeter ( tld ) during hdr icr . the median follow - up period was 26 months ( range 660 months )  . results : a total of 16 patients ( 12% ) experienced rectal bleeding , which occurred 433 months ( median 11 months ) after the completion of rt . 
 key words : cervix cancer high - dose - rate brachytherapy in vivo dosimetry rectal complications strahlenther onkol 2003 ; 179 : 1916 doi 10.1007 / s00066 - 003 - 1015 - 2 vergleich zwischen in - vivo - dosimetrie und bariumkontrasttechnik zur voraussage rektaler komplikationen bei intrakavitrer und externer radiotherapie von patientinnen mit zervixkarzinom ziel : untersuchung der korrelation zwischen sptnebenwirkungen am rektum und der rektalen dosis bei patientinnen mit zervixkarzinom , die mit intrakavitrer brachytherapie ( hdr - icr ) behandelt wurden , sowie analyse der faktoren , die rektale komplikationen reduzieren . patienten und methodik : es wurde eine retrospektive analyse von insgesamt 136 patientinnen mit zervixkarzinom durchgefhrt , die im zeitraum von 1995 bis 1999 mit perkutaner strahlentherapie ( ebrt ) and hdr - icr behandelt wurden . 
die berechnete rektale dosis unterschied sich nicht zwischen patientinnen mit und oh1 department of radiation oncology , samsung medical center , sungkyunkwan university school of medicine , seoul , korea . 
 this work was presented at the annual meeting of the american society of therapeutic radiology and oncology in san francisco , ca , usa , in november 2001 . received : february 27 , 2002 ; accepted : october 25 , 2002 strahlenther onkol 2003 no . 
bei einer gemessenen bed > 110 gy3 bestand eine hohe wahrscheinlichkeit fr spte rektale nebenwirkungen . schlussfolgerung : die in - vivo - dosimetrie mit tld hat sich als guter prdiktor von sptnebenwirkungen am rektum erwiesen . falls in - vivo - dosimetriewerte ein risiko spterer proktitis anzeigen , sollte die rektumdosis reduziert werden . 
 schlsselwrter : zervixkarzinom hdr - brachytherapie in - vivo - dosimetrie rektale nebenwirkungen introduction intracavitary radiotherapy ( icr ) is an essential component of curative radiotherapy ( rt ) for uterine cervix cancer . 
 since 1995 , we have prospectively calculated the rectal point dose with the method of barium contrast criteria and have concomitantly measured the rectal dose with thermoluminescent dosimeters ( tld ) during the first fraction of highdose - rate ( hdr ) icr . 
point a was defined as a point 2 cm lateral to the intrauterine tube and 2 cm cranial to the cervical bone according to the manchester system [ 27 ]  . 
we tried to place the tld chips at the nearest site of the rectal reference point using fluoroscopy , and the higher tld dose was defined as the measured rectal dose ( figure 2 )  . 
according to this glossary , the grading system is as follows : grade 1 , mild or occasional bleeding which developed 3 months after the initiation of rt and subsided spontaneously without medical management ; grade 2 , rectal bleeding requiring blood transfusion and / or hospitalization ; grade 3 , rectal bleeding requiring surgery . 
in order to find the factors which affect rectal complications , the authors categorized the data into a binary form arranged in 2 ( cid : 1 ) 2 contingency tables with a reasonable basis . fishers exact test was done with less expected frequencies because the number of patients with rectal complications was small . 
when the measured icr total rectal dose exceeded 16 gy , the ratio of the measured rectal dose to a point dose was > 70% ; when the measured rectal bed exceeded 110 gy3 , a high possibility of late rectal complications could be found . 
however , since there is a wide variation in terms of treatment technique , complication grading system , and patient characteristics , it is difficult to compare our results of a 12% rate of rectal complications with those of others . 
 for definition of the rectal reference point , some authors [ 5 , 7 , 9 , 19 , 21 , 30 ] used the icru report 38 criteria , while others [ 8 , 16 , 25 ] applied the barium contrast criteria . 
in the group that defined the rectal reference point according to the icru report 38 [ 12 ] , the results of the correlation between the rectal dose and the rectal complications were controversial . 
according to clark et al [ 5 ] , patients with a rectal reference point greater than the prescribed point a dose had a significantly higher probability of developing a figures 3a to 3c . 
the measured mean rectal doses and the bed , however , were higher in the group with complications , showing a significant difference between the two groups . fishers exact two - tailed test revealed the presence of a significant increase in the probability of developing rectal table 2 . 
yet , van lancker & storme [ 30 ] insisted that neither the single rectal reference point nor combinations of multiple rectal reference points were good predictors of complications , and suggested that volume calculation was a highly reliable predictor . 
in addition , because there were other rectal points besides the icru reference point which were receiving a dose close to the maximum , deshpande et al [ 9 ] proposed that doses to multiple rectal reference points with icru - defined rectal reference point should be recorded . 
 unlike the controversial results obtained by the groups that used the rectal reference point according to the icru report 38 , most studies [ 8 , 16 , 28 ] applying the barium contrast criteria showed a significant correlation between rectal dose and rectal complications . 
this negative result came from the discrepancy between the planned calculated rectal dose and in vivo measured rectal dose , and the cause of this discrepancy was mainly due to different instrumentation devices between icr simulation and treatment . 
according to senkus - konefka et al [ 23 ] , a significant correlation was found between the size of applicators and doses to bladder and rectu to predict late rectal complications , in vivo measurements of the rectal dose have been performed during icr [ 4 , 5 , 8 , 14 , 18 , 22 , 26 , 29 ]  . 
although clark et al [ 5 ] who used diode detectors , or cunningham et al [ 8 ] who employed tld , described the uncertainty of in vivo dosimetry and little value on routine basis , many institutes [ 4 , 18 , 24 , 26 , 29 ] used in vivo dosimetry and reported a good correlation between the measured rectal doses and complications . 
in our study , the measured rectal doses of the patients with rectal complications were higher than those of the patients without complication , and the difference was statistically significant . 
however , there is a possibility of tld localization errors and difficulty of absolute dose measurement in the rectuas cunningham et al [ 8 ] have pointed out , dosimetry with tld bears problems of uncertainty in the localization of tld and difficulty in reproducibility . 
therefore , the authors have attempted to reduce the localization error by confirming the same position of the applicators in every treatment fluoroscopically , but the possibility of localization error still exists . 
however , since the icru report 38 has been widely used although not to perfection in the treatment of cervical cancer , reporting the dose received by the rectal mucosa is mandatory for intercomparison between treatment methods according to icru 38 . 
our study does not have these data , and for a more serious intercomparison , a comparison between the icru 38 rectal reference point dose versus the institutional measurement is needed . 
in our study , measured rectal bed was higher in patients with rectal complications and the difference was statistically significant ; a value > 110 gy3 indicated a high possibility of rectal complications . 
however , since the calculated rectal dose at the rectal reference point did not correlate with late rectal complications , more precise point determination or other methods , e.g. , multiple reference points or dvh calculation , should be considered . 
if the measured icr rectal dose exceeds this recommended dose , the duration and loading of radioactive isotope in intracavitary applicators should be modified to reduce the possibility of late rectal complications . 
also , rectal dose limitation could be achieved by transvaginal packing , the use of an applicator with proper shielding and by reducing icr fraction size with increasing icr fraction numbers . 
 strahlentherapie und onkologie short communication locoregional failure 15 years after mastectomy in women with one to three positive axillary nodes with or without irradiation the significance of tumor size jnos fodor , csaba polgr , tibor major , gyrgy nmeth1 background : there is insufficient evidence to suggest the routine use of postmastectomy radiotherapy ( pmrt ) in patients with one to three positive axillary nodes and t1 / 2 tumors . 
we have assessed the risk of locoregional recurrence ( lrr ) with or without rt in this group of patients , and focused on the results in subgroups defined by tumor size . 
 key words : postmastectomy radiotherapy one to three positive nodes tumor size strahlenther onkol 2003 ; 179 : 197202 doi 10.1007 / s00066 - 003 - 1010 - 7 lokoregionre rezidive 15 jahre nach mastektomie bei patientinnen mit ein bis drei axillren lymphknotenmetastasen mit oder ohne strahlentherapie . 
der einfluss der tumorgre hintergrund : es gibt nicht gengend hinweise darauf , ob eine adjuvante strahlentherapie nach mastektomie bei patientinnen mit kleinen tumoren ( t1 / 2 ) und ein bis drei positiven axillren lymphknoten indiziert ist . 
wir haben das risiko , lokoregionre rezidive ( lrr ) zu entwickeln , bei dieser gruppe mit oder ohne radiotherapie ( rt ) untersucht und insbesondere die untergruppen analysiert , die aus der gre des primrtumors gebildet wurden . 
 patienten und methodik : von 1983 bis 1987 fhrten wir bei 249 patientinnen mit t1 / 2 - karzinomen der brust und ein bis drei positiven axillren lymphknoten eine mastektomie und dissektion der axilla durch . 
folgende rezidivlokalisationen 1 department of radiotherapy , national institute of oncology , budapest , hungary . received : february 21 , 2002 ; accepted : august 2 , 2002 strahlenther onkol 2003 no . 
locoregional failure after mastectomy wurden beobachtet : brustwand 17 ( 65% ) , achselhhle fnf ( 19% ) , supraklavikulargrube drei ( 12% ) und parasternale lymphknoten eine ( 4% )  . 
41% ohne strahlenbehandlung ( p = 0 , 2 )  . in der subgruppe der pt1 - tumoren lag die rate an isolierten lrr bei 9% ( 3 / 36 ) ohne rt vs . 
patientinnen mit t2 - tumoren und ein bis drei axillren lymphknotenmetastasen haben dagegen ein hohes risiko fr die entwicklung eines lrr mit oder ohne adjuvante strahlenbehandlung , jedoch signifikant niedriger in der gruppe mit rt . 
 schlsselwrter : strahlentherapie nach mastektomie ein bis drei positive lymphknoten tumorgre introduction reasons for the use of postmastectomy radiotherapy ( pmrt ) in women with node - positive breast cancer include a reduction of the risks for local - regional recurrence ( lrr ) and distant relapse [ 4 , 14 , 26 , 28 ]  . 
there is consensus on the routine use of pmrt in patients with t1 / 2 tumors and four or more positive axillary lymph nodes , but whether or not to use it in patients with one to three involved nodes is still being debated [ 7 , 11 , 12 , 23 , 26 , 28 ] , as well as investigated in clinical trials [ 11 , 23 ]  . 
the lrr rates in patients with one to three involved nodes in the danish [ 21 , 22 ] and british columbia [ 25 ] trials were much higher than in other series [ 1 , 8 , 10 , 18 , 27 , 30 ]  . 
only a few studies have examined the risk of lrr in patients with one to three positive nodes focusing on tumor size [ 2 , 17 , 24 , 27 , 31 , 32 ]  . 
the median dose of pmrt was 50 gy ( range , 4252 gy ) given over 5 weeks to the chest wall and to the regional lymph nodes including the ipsilateral axilla , internal mammary region , and supraclavicular fossa . 
the number of women treated with rt alone , cmf alone , tamoxifen alone , cmf and rt , or tamoxifen and rt were 125 , 36 , 25 , five , and 46 , respectively . 
the following endpoints were studied : the occurrence of isolated lrr ( coming before distant relapse ) for isolated lrr - free survival ; locoregional or distant relapse ( whichever came first ) for diseasefree survival ; and death from breast cancer , other malignancy , or death without cancer for overall survival . survival and recurrence rates were estimated by the kaplan - meier method and compared by the log rank test [ 16 ]  . regression analyses were done according to the methods of cox [ 3 ]  . 
 results all patients by the date of analysis , in december 2001 , with a median follow - up of 189 months ( range , 167227 months ) , 120 ( 48% ) out of the 249 patients had disease recurrence . 
the anatomic sites of isolated lrr were as follows : chest wall , 17 ( 65% ) ; axilla , five ( 19% ) ; supraclavicular fossa , three ( 12% ) ; and internal mammary nodes , one ( 4% )  . 
the median time to development of an isolated lrr was 26 months ( range , 6153 months ) , and in nonirradiated patients 92% and in irradiated patients 50% occurred within 5 years . 
the number of total lrr ( recurrence with or without distant failure ) amounted to 38 , and their anatomic sites were as follows : chest wall , 23 ( 61% ) ; axilla , six ( 16% ) ; supraclavicular fossa , seven ( 18% ) ; internal mammary nodes one ( 3% ) ; and chest wall plus axilla , one ( 3% )  . 
 lrr rate in relation to systemic treatment the rate of isolated lrr for patients treated with cmf alone , cmf and rt , tamoxifen alone , or tamoxifen and rt amounted to 25% ( 9 / 36 ) , 20% ( 1 / 5 ) , 12% ( 3 / 25 ) , and 8.7% ( 4 / 46 ) , respectively . 
the crude rate of isolated lrr for nonirradiated patients with t2 tumor ( n = 38 ) by anatomic sites was as follows : chest wall , 13% ; supraclavicular fossa , 5% ; axilla , 3% ; and parasternal nodes , 3% . 
isolated locoregional recurrence - free survival without ( n = 38 , lower curve ) or with ( n = 76 , upper curve ) radiotherapy in patients with one to three involved nodes and t2 tumor . 
isoliertes lokoregionres rezidivfreies berleben ohne ( n = 38 , untere kurve ) oder mit bestrahlung ( n = 76 , obere kurve ) bei patientinnen mit t2 - karzinomen und ein bis drei axillren lymphknotenmetastasen . only a few studies have examined the risk of lrr in postmastectomy patients with one to three positive axillary nodes and t1 / 2 tumors focusing on tumor size [ 2 , 17 , 24 , 27 , 31 , 32 ]  . in the current study , we assessed the risk of lrr without or with rt in this group of patients , focused on the results in subgroups defined by tumor size . 
 our results indicate that the incidence of isolated lrr either with or without rt is low ( crude rate 8% and 8% , respectively , at a median follow - up of 189 months ) in patients with one to three involved nodes and t1 tumor . 
our findings , as demonstrated in table 3 , were consistent with those noted in most of the other studies [ 2 , 17 , 27 , 31 , 32 ]  . 
in the aforementioned five studies ( table 3 ) , lrr rates without rt in patients with t2 tumor ranged from 7% to 22% , and in five out of six studies this rate was > 10% . 
in two other studies , the lrr rates were also relatively high , 18% and 15% at a median follow - up time of 112 and 62 months , respectively [ 24 , 32 ] , and in one study the 4 - year lrr rate amounted to 22% [ 2 ]  . 
this finding is supported by the analysis of dunst et al [ 4 ]  . there is insufficient evidence to suggest how age and eni should be employed to modify decisions on the use or nonuse of pmrt in patients with one to three positive nodes and t1 / 2 tumors [ 26 ]  . 
eni is believed to correlate with the number of involved axillary lymph nodes and does not appear to be an independent predictor of lrr [ 13 , 23 ]  . 
the impact of patient age on the risk of lrr after mastectomy is uncertasome series have reported an increased risk of lrr in young women [ 2 , 9 ] , but others have not [ 24 , 32 ]  . 
thus , patient age ( 45 vs > 45 years ) may help to identify those patients with t2 tumors who are at high risk of lrr . in our study , the isolated lrr rate was 25% in patients who were treated with cmf alone , and 0% in patients receiving no adjuvant treatment . 
 author patients ( n ) method of evaluation lrr ( % ) without rt with rt pisansky et al [ 24 ] 8 - year cumulative recht et al [ 27 ] 10 - year cumulative taghian et al [ 31 ] crude ; median fu , 9 years cheng et al [ 2 ] katz et al [ 17 ] zellar et al [ 32 ] present study 190 214 4 - year actuarial 10 - year actuarial 5 - year crude 15 - year crude specific sites of failures , internal mammary node recurrence was not reported [ 17 , 27 ]  . 
however , there is insufficient evidence on how to select different treatment volumes for pmrt , and this decision is left to the discretion of the treating radiation oncologist [ 23 , 26 ]  . in the current investigation , overall survival was not improved significantly by rt . 
a risk of 20% of lrr is considered by most radiation oncologists a substantial argument to justify radiation , even in the absence of a statistically significant survival benefit [ 7 , 11 ]  . 
 likelihood of poor - risk patients being given chemotherapy ( greater preponderance of eni and young age in this group ) and the very small number of patients in the second group . 
in agreement with the findings of other reports [ 1 , 5 , 8 , 17 , 27 ] , the results of the current investigation demonstrate that the chest wall is the site at greatest risk of recurrence in patients undergoing mastectomy . therefore , when pmrt is given , treatment of the chest wall is mandatory . 
after axillary dissection ( minimum level i / ii ) , rt of this site is not suggested to be given routinely [ 6 , 23 , 26 , 28 ]  . the crude rate of supraclavicular recurrence at 15 years in our nonirradiated patients with t2 tumor and one to three positive nodes was 5% . 
the risk of supraclavicular failure in patients with one to three positive nodes is low , and there is insufficient evidence to justify the routine use of an elective supraclavicular field [ 6 , 26 ]  . 
in our patients one recurrence occurred , and in the other two series , examining conclusion at present , there is insufficient evidence to suggest the routine use of pmrt in patients with one to three involved nodes and t1 / 2 tumors , and this special issue is being investigated in clinical trials . 
 strahlentherapie und onkologie original article concurrent radiochemotherapy with vinorelbine plus cisplatin or carboplatin in patients with locally advanced non - small - cell lung cancer ( nsclc ) and an increased risk of treatment complications preliminary results sabine semrau1 , anette bier2 , ulrike thierbach3 , christian virchow2 , peter ketterer3 , rainer fietkau1 background : in elderly patients , patients with multiple morbidities , and patients with a reduced general condition , the standard treatment of inoperable non - small - cell lung cancer ( nsclc ) consists of either chemotherapy or radiation therapy alone and is associated with an extremely poor prognosis . 
 patients and methods : a total of 33 patients ( six women , 27 men , median age 65 years ) with locally advanced , functionally inoperable pulmonary carcinomas , recurrent lung cancer or postoperative macroscopic residual tumors ( r2 ) with an increased risk of treatment complications ( who performance status 2 / 3 ; cardiac , renal or pulmonary failure ; marked pretherapeutic weight loss ; age between 7175 years ) received 12.5 mg of vinorelbine per m2 body surface area ( bsa ) on days 1 , 8 , 15 , 29 , 36 and 43 plus either cisplatin 20 mg / m2 bsa ( ten patients ) or carboplatin 70 mg / m2 bsa ( 23 patients ) on days 15 and 2933 together with conventionally fractionated radiotherapy . 
 results : briefly , 31 of 33 patients successfully completed radiation therapy and 26 received four cycles of vinorelbine plus at least two cycles of cisplatin or carboplathematotoxic side effects included grade iii leukocytopenia ( n = 8 ) , grade iii thrombocytopenia ( n = 5 ) , and grade iv thrombocytopenia ( n = 2 )  . 
the survival rates plus standard deviations were as follows : 1 - year survival : 60 8% , 2 - year survival : 36 9% , 3 - year survival : 24 9% , median survival time : 17 months ( 5 ; 29 months ; 95% confidence interval [ ci ] ) , median progression - free survival : 11 months ( 9 ; 13 months ; 95% ci )  . 
 key words : non - small - cell lung cancer concurrent radiochemotherapy cisplatin carboplatin vinorelbine strahlenther onkol 2003 ; 179 : 82331 doi 10.1007 / s00066 - 003 - 1127 - 8 simultane radiochemotherapie mit vinorelbin und cisplatin / carboplatin bei patienten mit lokal fortgeschrittenem nsclc und erhhtem behandlungsrisiko . 
 ergebnisse : die bestrahlung wurde bei 31 von 33 patienten in voller dosierung und die chemotherapie bei 26 patienten mit mindestens zwei kursen cisplatin oder carboplatin und vier kursen vinorelbin durchgefhrt . 
hmatotoxische nebenwirkungen schlossen leukozytopenien grad iii ( n = 8 ) , grad - iii - thrombozytopenien ( n = 5 ) und grad - iv - thrombozytopenien ( n = 2 ) esonstige nebenwirkungen : periphere neuropathie grad iii ( n = 1 ) und sophagitis grad iv ( n = 1 )  . 
die berlebensraten einschlielich standardabweichungen betrugen : 1 - jahres - berlebensrate : 60 8% , 2 - jahres - berlebensrate : 36 9% , 3 - jahresberlebensrate : 24 9% , mediane berlebenszeit : 17 monate ( 5 ; 29 monate ; 95% - konfidenzintervall [ ki ] ) , medianes progressionsfreies berleben : 11 monate ( 9 ; 13 monate ; 95% - ki )  . 
 schlsselwrter : nichtkleinzelliges bronchialkarzinom simultane radiochemotherapie cisplatin carboplatin vinorelbin introduction compared to sequential radiotherapy - chemotherapy [ 3 , 69 ] or radiation therapy alone [ 10 , 29 ] , concurrent radiochemotherapy was found in most studies to significantly improve the survival of patients with small - cell lung cancer or with functionally or locally inoperable non - small - cell lung cancer ( nsclc )  . 
there is no differentiated data available on concurrent radiochemotherapy in patients with unfavorable starting conditions , such as extensive weight loss , concomitant cardiac , renal or pulmonary diseases , or old age . 
 patients and methods patient population and characteristics between june 30 , 1997 and january 31 , 2002 , 33 patients ( six women , 27 men ) with a functionally inoperable nsclc , a relapse of the same , or postoperative residual nsclc ( r2 ) without distant metastases underwent concurrent radiochemotherapy ( vinorelbine plus cisplatin or carboplatin ) at the department of radiotherapy , rostock university hospital , germany . 
 inoperable patients with better starting conditions were irradiated in the same manner , but their concurrent chemotherapy was carried out using cpt11 and cisplatthese results were published in a separate article . 
in order to exclude possible distant metastases , all abdominal studies were performed by ultrasound or ct . most patients had stage iiia ( n = 4 ) or stage iiib disease ( n = 19 ) , seven had stage i or ii disease , two presented with a relapse , and one had macroscopic tumor residue after tumor resection . 
the target volume included the region of the primary tumor plus a 1to 2 - cm safety margin as well as the ipsilateral hilar lymph nodes and bilateral mediastinal lymph node sites . 
thus , the entire macroscopic tumor volume received a dose of 63 gy ( 90% isodose ; approximately 66 gy according to icru 50 ) ; the total dose to the prophylactically irradiated volume was 4550.4 gy ( 90% isodose ; approximately 4753 gy according to icru 50 )  . 
if peripheral cytopenia occurred ( leukocytes < 3 , 000 / ml or thrombocytes < 100 , 000 / ml ) , the scheduled dose fraction of vinorelbine was postponed for 1 day , or for 1 week in the case of cisplatin and carboplatcarboplatin was administered as the platinum salt in cases where cardiac comstrahlenther onkol 2003 no . 
 pensation limited fluid infusion to < 2 l / day as well as in patients with renal insufficiency ( renal clearance < 60 ml / min , > 30 ml / min ) or who performance status grade 3 . 
the tumor response was documented by comparing x - ray films taken at two different levels before and 6 weeks after completion of radio - chemotherapy ( or right at the end of treatment in seven cases ) and 3 months after completion of therapy . 
the outcome was rated as a complete response ( cr ) , partial response ( pr ) , stable disease ( sd ) , or progressive disease ( pd ) according to the who definitions . 
 results remission of the 33 patients studied , 21 ( 63% ) exhibited a complete ( n = 7 ) or partial response ( n = 14 ) to radiochemotherapy . 
the survival figures for the total population , with standard deviations , were as follows : median survival : 17 months ( 5 ; 29 months , 95% confidence interval [ ci ] ) , 1 - year survival : 60 8% , 2 - year survival : 36 9% , and 3 - year survival : 24 9% ( figure 2 )  . 
however , the median survival time with carboplatin / vinorelbine was 21 months ( 7 ; 35 months , 95% ci ) compared to only 17 months ( 2 ; 35 months , 95% ci ) with cisplatin / vinorelbine . 
 furthermore , we found that patients with three or more classic risk factors ( see patients and methods and table 1 ) tended to have shorter survival times than patients with only one or two risk factors . 
the latter group survived a median 22 months ( 0 ; 24 months , 95% ci ) , whereas those with three risk factors survived a median 17 months ( 3 ; 31 , 95% ci )  . 
concurrent radiochemotherapy with vinorelbine plus cisplatin or carboplatin in inoperable nsclc 8 months in those with progressive disease ( 2 ; 14 months , 95% ci ; figure 5 )  . analysis of relapse disease progression occurred after a median 11 months ( 9 ; 13 months , 95% ci )  . 
the median hb concentration was 8.1 mmol / l ( 5.710.3 mmol / l ) at baseline and 7.1 mmol / l ( 5.08.8 mmol / l ) at the nadir after the first treatment cycle . 
one patient developed grade iv esophagitis . six patients received antibiotics for pneumonia during the study ; however , each of them had received prior treatment for the same condition before the start of radiochemotherapy . 
patients with a complete response survived a median 38 months ( 18 ; 58 months , 95% ci ) and those with a partial response a median 23 months ( 20 ; 26 months , 95% ci )  . by comparison , the median survival was only 7 months ( 4 ; 10 months , 95% ci ) in patients with stable disease and survival ( months ) survival ( months ) figure 4 . 
concurrent radiochemotherapy with vinorelbine plus cisplatin or carboplatin in inoperable nsclc feasibility of radiochemotherapy as a whole , 31 of 33 patients ( 94% ) completed radiotherapy according to the protocol . 
likewise , most cycles of chemotherapy were administered on schedule , i.e. , 43 of 46 ( 91% ) cycles of carboplatin , 20 of 20 ( 100% ) cycles of cisplatin , and 148 of 198 ( 75% ) cycles of vinorelbine . 
 discussion a number of randomized trials have shown that patients with inoperable nsclc treated with sequential irradiation and chemotherapy and especially with concurrent radiochemotherapy have a significantly better prognosis than those treated with radiation therapy alone [ 4 , 5 , 6 , 8 , 13 , 18 , 19 , 25 , 27 , 29 ]  . the intensity - modulated radiotherapy offers an opportunity of dose escalation and may provide another tool for improving local control and survival [ 20 ]  . 
 it is generally assumed that increasing the treatment intensity by administering chemotherapy in addition to radiation therapy does not have a beneficial effect on patients > 70 years of age or patients in a reduced general condition due to concomitant diseases . 
laus team found that conventionally fractionated radiation therapy with up to 61 gy in combination with two cycles of etoposide and carboplatin led to response rates of 87% , a median survival time of 12 months , and an overall 2 - year survival rate of 40% . 
however , these findings have to be viewed critically for the following reasons : the statistical analysis of these authors was based on subgroup data from merely two studies [ 15 , 26 ]  . 
as far as we can tell , the number of patients barely exceeded 20 . both protocols investigated [ 15 , 26 ] consisted of lengthy induction chemotherapy with cisplatin plus vinblastine or etoposide followed by concurrent radiochemotherapy using cisplatin . cumulatively , the overall doses of cytostatics were significantly higher than those used in our study . 
 however , daily clinical practice has shown that at least one quarter of all patients with nsclc also suffer from chronic obstructive pulmonary disease ( copd ) , 20 of 100 patients have coronary heart disease ( chd ) requiring treatment , 22% hypertension , and 13% arteriosclerosis [ 23 ]  . 
due to the numerical significance of this patient population and in light of the poor results achieved by irradiation or chemotherapy alone , it is necessary to develop intensified treatment protocols which are tolerated by and improve the survival of these risk patients . 
 induction chemotherapy might lead to higher local toxicity during concurrent radiochemotherapy , as has been described after accelerated hyperfractionated [ 24 , 35 ] or hypofractionated radiotherapy [ 32 ]  . 
authors performing concurrent radiochemotherapy using newer substances ( gemcitabine , paclitaxel , docetaxel , irinotecan , vinorelbine ) alone or in combination with a platinum salt have observed significantly varying rates of local side effects . 
the incidence of pneumonitis reportedly ranges between 75% ( gemcitabine 1 , 000 mg / m2 ) [ 28 ] and < 5% for paclitaxel / carboplatin [ 1 ]  . 
vinorelbine / platinum salt combinations have a rather favorable spectrum of side effects , as was shown in a phase iii study of cisplatin / paclitaxel versus cisplatin / gemcitabine and cisplatin / vinorelbine [ 31 ]  . 
if there was no response to antibiotics in the six cases where pneumonia occurred , cytostatic treatment was interrupted until abatement of the pneumonia in order to avoid cytopenic complications . 
 because of the low probability of side effects , especially pneumonitis [ 33 ] , and the expected enhancement of local control , we proposed this chemoradiation schedule to patients formerly classified as ineligible for surgery due to impaired lung function in spite of the lack of published results on concurrent radiochemotherapy in inoperable stage i and ii nsclc . 
cisplatin was initially the first choice in patients with sufficient renal and cardiac function . we did not detect any considerable differences in the frequency of toxicity and intensity of side effects between the two groups . 
morbidity was higher in the carboplatin / vinorelbine group , since these patients had three risk factors on average , which were mostly related to renal and cardiac compensation problems . 
considering the fact that carboplatin has a generally low rate of renal toxicity and that both schedules produced relatively good results in all of these patients , we have exclusively used carboplatin / vinorelbine since 2002 . 
the survival time and the local rate of tumor control of nearly 50% support the results of a wide range of the phase ii and iii studies on concurrent radiochemotherapy [ 2 , 3 , 8 , 11 ]  . 
we think it unlikely that sequential radiotherapy - chemotherapy might achieve better results , especially since the duration of concurrent radiochemotherapy is 68 weeks compared to at least 14 weeks for the sequential schedule . 
 strahlentherapie und onkologie original article low - dose irradiation and short - exposure suboptimaldose paclitaxel adversely modulate metastatic potential of squamous carcinoma cells jzsef lvey1 , kroly fazekas2 , andrea ladnyi2 , gyrgy nmeth1 , jzsef tmr2 background and purpose : low - dose irradiation and suboptimal drug concentrations may induce unexpected biological responses . 
 material and methods : 2 gy irradiation , 7 and 100 nm ptx treatment , and their combinations were tested on squamous and transitional cell carcinoma lines a431 , kb and ecv304 . 
cytoskeleton of interphase cells was investigated with immunocytochemistry and confocal laser scanning microscopy ; viability and clonogenicity were assessed with mtt test and standard clonogenic assay . effects on tumor growth and metastatic potential of a431 cells were tested in vivo using a liver metastasis model in scid mice . results : exposure of human tumor cells to irradiation induced bundling of microtubules , similar to ptx . 
single or combination treatments with low - dose ptx did affect cell proliferation to no relevant extent in vitro or in vivo ( primary tumor xenografts of a431 cells )  . 
 key words : low - dose irradiation paclitaxel proliferation metastasis strahlenther onkol 2003 ; 179 : 8128 doi 10.1007 / s00066 - 003 - 1051 - y ungnstiger einfluss niedrig dosierter bestrahlung und kurzzeitiger suboptimal dosierter paclitaxel - exposition auf das metastatische potential von plattenepithelkarzinomzellen hintergrund und ziel : niedrig dosierte bestrahlung kann in kombination mit suboptimal konzentrierten medikamenten unerwartete biologische reaktionen hervorrufen . 
das primre tumorwachstum in vivo und die metastasierungsfhigkeit in die leber wurden an scidmusen berpr ergebnisse : niedrig dosierte bestrahlung fhrte bei a431 - zellen zu hnlichen aggregationen der mikrotubuli wie bei einer behandlung mit ptx . 
 schlussfolgerung : die kurzzeitige behandlung mit ptx und die bestrahlung knnen ihre wirkungen gegenseitig modifizieren , ohne die proliferation oder die tumorigenitt signifikant zu ndern , obwohl ptx und bestrahlung das metastasierungspotential der tumorzellen signifikant modifizieren knnen . 
doses which are used as conventional fraction dose in clinical radiotherapy cause cytoplasmic rearrangements , changes in the cytoskeleton , and the expression of several molecular factors related to apoptosis , proliferation and cell adhesion [ 4 , 10 , 15 , 18 ]  . 
the systemic cytostatic drug treatment is based upon the presumption that the administered drug reaches the tumor cells via the blood vessels and the tumor cells are exposed to the pharmacologic concentration . 
poor vascularization , bad functionality of the vessels and slow diffusion through the extracellular matrix may all decrease the concentration of the drug in the proximity of the tumor cells [ 9 , 17 ]  . 
when a drug is administered , tumor cells at various distances from the vessels are exposed to various concentrations . the effects of cytostatic drugs are mostly dose - dependent , and many drugs have different mechanisms of action at different doses , some of which may have undesirable consequences . one of the recently introduced anticancer drugs is taxol ( paclitaxel , ptx )  . 
although the g2 / m - phase of the cell cycle is considered the primary target , ptx effect is universal throughout the cell cycle ( interphase ) [ 23 ] resulting in disturbances of cell functions other than mitosis , such as cell movement or angiogenesis [ 1 , 2 , 31 ]  . 
ptx is also considered to be a radiation sensitizer even at low doses ; however , in the light of the controversial experimental data , the existence and extent of this effect are a subject of intensive debate [ 3 , 6 , 8 , 12 , 16 , 30 ]  . 
in this study , we have tested the biological effect of low - dose or suboptimal ptx treatment and irradiation on human squamous cell carcinoma cell lines a431 , kb and transitional carcinoma cell line ecv304 in vitro and in vivo . 
 treatments irradiation was carried out with a therapeutic x - ray source ( thx 250 , medicor , budapest , hungary ) at 200 kv , 15 ma , using 0.5 - mm cu filter with a dose rate of 1.85 gy / mprior to irradiation , cells were plated in 6 - , 24or 96 - well plastic tissue culture plates or t25 and t75 tissue culture flasks . 
ptx treatment was performed using the same tissue culture plates with 6 , 24 or 96 wells , or plastic tubes as during irradiation , and was diluted in culture mediucells were exposed to 7 nm and 100 nm ptx and further incubated at 37 c for 10 min ; then , cell cultures were carefully washed three times with serum - free mediu the treatment schedule contained eight groups : medium control , 7 nm ptx , 100 nm ptx , 2 gy irradiation , 7 nm ptx before 2 gy irradiation , 2 gy irradiation before 7 nm ptx , 100 nm ptx before 2 gy irradiation , and 2 gy irradiation followed by 100 nm ptx . 
the time interval between the double treatments was 30 m cell viability cell viability was assessed by mtt test 48 h after treatment . cells were cultured in a 96 - well plate and exposed to 5 mg / ml mtt ( sigma ) solution for 3 h . 
formazan deposits were dissolved in dmso ( reanal , budapest , hungary ) , and optical densities were measured at 540 nm wavelength using a biorad laboratories plate reader and microplate manager software ( biorad , munich , germany )  . 
 clonogenic survival for clonogenic survival assay , cells were placed in six - well culture plates and allowed to attach for 24 h in the presence of seruthe number of cells per well was set to produce around 100200 surviving colonies after the treatment . 
 immunocytochemistry of tubulin and intermediate filaments for fluorescence analysis of ( cid : 1 ) - tubulin and intermediate filaments , cells were plated on glass plates , placed in 24 - well plastic plates . 
cells were allowed to attach for 24 h in the presence of serum , then treated according to the mentioned schedules . 4 h after treatment , cells were permeabilized with 0.1% triton - x for 2 min , then fixed in methanol at 20 c . 
it was followed by 1 - h incubation with primary monoclonal anti - tubulin ( cid : 1 ) ( sigma ; 1 : 500 ) and anti - cytokeratin 19 ( dako , glostrup , denmark ; 1 : 50 ) antibodies . 
after exposure to biotinylated anti - mouse igg secondary antibodies ( amersham , uk ; 1 : 100 ) for 1 h , samples were stained with streptavidin fitc ( amersham ; 1 : 100 ) and propidium iodide ( 1 : 200 )  . 
balken : 5 washed three times between each step with phosphatebuffered saline ( pbs , icn , aurora , oh , usa ) containing calcium and magnesiu glass plates were then placed on microscopic slides and covered by vectashield ( vector , burlingame , ca , usa )  . 
short exposure of a431 cells to 2 gy irradiation also induced severe bundling of microtubules ( figure 2b ) comparable to the effect of 100 nm ptx ( figure 1b )  . 
7 nm ptx also produced significant aggregation of the microtubules ( figures 3a and 3b ) and was also capable of suspending the effect of irradiation ( figure 3c )  . 
 cytokeratin intermediate filaments of a431 cells ( figure 1c ) responded to high - dose ptx by granular aggregation in the cytoplasm at the peripheral membranes and cell adhesions ( figure 1d ) , and this effect was also suspended by the combination with irradiation ( data not shown )  . 
 effects of ptx and irradiation on cell proliferation , clonogenicity , and tumorigenicity in vitro and in vivo none of the single in vitro treatments of irradiation or various doses of ptx produced biologically significant effect on cell strahlenther onkol 2003 no . 
the maximal effect could be seen when 100 nm ptx and irradiation were combined with each other in any order ; however , even these treatments failed to induce > 30% inhibition ( figure 4 )  . 
2 gy irradiation , 7 nm ptx , and combinations with 7 nm ptx did not affect the clonogenic survival of a431 cells either ( figure 5 ) suggeststrahlenther onkol 2003 no . 
 testing further the biological consequences of the various suboptimal in vitro treatments on tumorigenicity , pretreated a431 cells were injected into the spleen of scid mice , and the growth of the primary tumor was evaluated . 
 effect of low - dose in vitro ptx and irradiation exposure on the metastatic potential evaluation of the effects of various suboptimal in vitro pretreatments on the metastatic potential of a431 cells gave unexpected results . 
on the other hand , 100 nm ptx exposure significantly stimulated the liver - metastatic capacity which was also eliminated by the combination with low - dose irradiation ( figure 7 )  . 
cells were placed in six - well culture plates and allowed to attach for 24 h in the presence of serufollowing treatment with ptx and irradiation , plates were incubated for 14 days ; then , cells were stained with giemsa . 
statistisch signifikante ergebnisse ( student - t - test ) sind mit einem stern markiert . tumorigenicity can significantly modulate the metastatic potential of a431 cells , depending on the order of the two treatment forms , ptx and irradiation . 
 discussion results of our experiments support the initial idea that suboptimal treatment schedules consisting of irradiation and chemotherapy may have very important and unexpected effects on the behavior of tumor cells even without affecting their proliferation . 
the decrease of antimetastastic potential by low - dose irradiation in our experiment is different from what has previously been published for melanoma cells [ 15 , 18 ]  . 
the possible explanation is that the lipoxygenase metabolism and its sensitivity to radiation reported before are different in various cell types , since melanoma cells are poor while a431 cells are high and constitutive 12 - lipoxygenase ( 12 - lox ) expressors and the expression of 12 - lox correlates with the metastatic potential [ 5 , 28 ]  . 
modulation of certain inflammatory pathways or alteration of membrane lipid levels may also play a role in the antimetastatic effect of low - dose irradiation [ 21 , 26 ]  . 
tumor cells were pretreated in vitro with irradiation and paclitaxel ( ptx ) and their combinations as indicated and injected into the spleen of the anesthetized animals ( 2 ( cid : 1 ) 105 / animal )  . 
tumor cells were pretreated in vitro and injected into the spleen of scid mice as described in figure 6 . animals were sacrificed upon the death of the first control animal . livers were dissected and the number of liver metastases counted under stereomicroscope . 
primary cytostatic effect of ptx through the stabilization of the microtubules is well described depending on concentration and exposure time [ 24 ] ; however , such short exposure we used was not investigated in detail . 
ptx has other effects such as the modulation of apoptotic pathways [ 27 ]  . furthermore , ptx was also used in experiments as a migration and angiogenesis inhibitor [ 1 , 2 , 31 ]  . 
there are a wide variety of ptx - containing chemoradiation schedules from the high - dose 2 - week cycles through the weekly , three times weekly to continuous regimens [ 7 , 22 , 29 ]  . 
 our data indicated that in specific circumstances when low - dose irradiation or short - exposure suboptimal doses of ptx were administered , differences in the primary effect on the microtubules and cytokeratin could be seen in a doseand combination - dependent manner . 
low - dose irradiation and short - exposure paclitaxel treatment proved that the two modalities can suspend each others effect in any order in case of the modulation on cytoskeleton architecture and metastatic potential without significant modulation of the proliferative and tumorigenic capacity . 
 whatever the underlying mechanism is , our data draw the attention to the fact that despite detailed preclinical and clinical investigations , irradiation with a dose comparable to a fraction used in clinical settings and a widely used and investigated drug can behave in a manner we do not expect , when the circumstances are suboptimal . 
these results highlight the importance of taking into consideration the biology of the tumor and the possible unexpected effects of a drug , when a new clinical investigation is designed . 
 acknowledgment this work was supported by the ministry of education of hungary ( nkfp 1 / 48 / 2001 , jt )  . strahlentherapie und onkologie originalarbeit strahlentherapie beim morbus ledderhose indikation und klinische ergebnisse michael heinrich seegenschmiedt , mared attassi1 hintergrund : der morbus ledderhose ( ml ) ist eine hyperproliferative erkrankung der plantaraponeurose , die dem morbus dupuytren ( md ) sehr hnlich ist . 
 patienten und methoden : von juni 1996 bis dezember 2002 wurden zwlf frauen und 13 mnner im alter von 976 ( median 56 ) jahren mit symptomatischem ml bestrahlt und mindestens 1 jahr kontrolliert . 
zustzlich bestanden 14 - mal ( 56% ) starke fuschmerzen , achtmal ( 32% ) probleme beim laufen , zwlfmal ( 48% ) andere symptome ( druck , schwellung , spannung )  . 
bei 11 von 36 ( 44% ) fen nahm die zahl ( minus 16 ) oder die gre der knoten und bei 7 von 13 ( 54% ) fen die zahl ( 9 ) oder die lnge der strnge ab ; normale gehfunktion erreichten sechs von zwlf ( 50% ) fen ; die schmerzen verschwanden ganz oder teilweise bei 9 von 15 ( 60% ) fen , die brigen symptome verschwanden bei 8 von 18 ( 44% ) fen . 
die nebenwirkungen waren insgesamt gering : whrend und bis zu 3 monaten nach der rt hatten fnf ( 14% ) fe eine leichte hautrtung ( ctc 1 ) im rt - feld ; bei drei ( 8% ) fen blieb die haut langfristig ( > 12 monate ) trocken . 
 schlsselwrter : morbus ledderhose plantarfibromatose fibromatosis plantaris morbus dupuytren weichteiltumor nicht maligne erkrankung radiotherapie klinische studie strahlenther onkol 2003 ; 179 : 84753 doi 10.1007 / s00066 - 003 - 0994 - 3 radiation therapy for morbus ledderhose indication and clinical results background : morbus ledderhose ( ml ) is a rare hyperproliferative disorder of the plantar aponeurosis which is similar in its clinical course to morbus dupuytren ( md )  . 
 patients and methods : from june 1996 to december 2001 , 25 patients ( 12 female / 13 male ) aged 976 ( median : 56 ) years had radiotherapy ( rt ) for symptomatic ml . 
21 ( 84% ) patients had one or more signs : 14 ( 56% ) severe local pain , eight ( 32% ) walking difficulties , twelve ( 48% ) other symptoms , pressure or tension sensation . 
the rt field involved all nodules and cords plus safety margtwo rt - series were applied ( each 5 ( cid : 1 ) 3 gy in 1 week ) separated by 812 weeks up to a total dose of 30 gy . 
radiotherapie bei morbus ledderhose gait was improved in six of twelve ( 50% ) feet ; pain was reduced or had completely disappeared in 9 of 15 ( 60% ) feet , and other symptoms disappeared in 8 of 18 ( 44% ) symptomatic feet . 
 treatment side effects were minimal : during and within 3 months of the rt course only a slight erythema ( ctc 1 ) was seen in five treated lesions , while dry skin changes within the rt portal were observed in three cases ( 11% ) in long term fu ( > 12 months )  . conclusions : radiotherapy is effective in treating ml and may prevent otherwise necessary surgical interventions . 
 key words : morbus ledderhose plantar fibromatosis fibromatosis plantaris morbus dupuytren soft tissue tumor  . non - malignant disease radiotherapy clinical study einleitung morbus ledderhose ( ml ) oder fibromatosis plantaris ist eine seltene erkrankung der plantaraponeurose [ 6 ] , die 1897 erstmals beschrieben wurde [ 24 ]  . 
der ml ist klinisch und ( patho - ) histologisch dem morbus dupuytren ( md ) sehr hnlich , was die bezeichnung dupuytrensche erkrankung der plantarfaszie unterstreicht [ 9 ]  . 
die hhere inzidenz in der kaukasischen rasse und hereditre disposition , ein zeitgleich oder spter auftretender md , morbus peyronie ( mp ) oder knchelpolster an fingern ( knuckle pads ) weisen auf hnliche pathomechanismen fr diese hyperproliferative bindegewebserkrankung hin [ 8 , 10 , 14 , 38 , 45 ]  . 
neben der genetischen disposition werden traumatische , neuropathische , metabolische , endokrine , infektise und autoimmune ursachen und arthropathien diskutiert [ 10 , 14 , 20 ]  . der ml tritt bei mnnern hufiger auf als bei frauen . 
erste symptome treten ab der vierten dekade auf ; der hufigkeitsgipfel liegt in der fnften und sechsten dekade ; kinder und jugendliche sind selten betroffen [ 17 , 31 ]  . 
 klinisch erscheinen die knoten und strnge an der ganzen fusohle , bevorzugt medial , im bereich der nicht gewichtstragenden fusohle ( erster bis dritter zehenstrang ) ( abbildung 1 )  . 
orthesen und kortikoidinjektionen [ 29 ] , bis hin zu chirurgischen manahmen , doch deren langzeitresultate sind durch hohe komplikationsund rezidivraten gekennzeichnet [ 2 , 4 , 6 , 13 , 18 , 25 , 30 , 44 ]  . 
 patienten und methoden patienten / fe von juni 1996 bis dezember 2002 wurden 32 patienten mit ml in unserer klinik vorgestellt ; davon wurden zwlf frauen und 13 mnner im alter von 9 bis 76 jahren ( median 56 jahre ) wegen symptomen und subjektiver beeintrchtigung bestrahlt und fr mindestens ein jahr nachbeobachtet . 
typisches rtfeld im medialen anteil des rechten hohlfues mit groem sicherheitsabstand nach proximal / distal ( 2 cm ) sowie medial / lateral ( 1 cm ) ; zustzlich besteht eine fuwarze im bereich des linken fuballens d3 / 4 . 
typical rt - portal at the medial concavity of the right foot with large safety margin in proximal / distal ( 2 cm ) and medial / lateral ( 1 cm ) direction ; additionally plantar wart is recognized in the left d3 / 4 ball of foot . 
radiotherapie bei morbus ledderhose zwlf patienten hatten neben dem ml noch einen md , zwei typische knchelpolster ( knuckle pads ) und einer eine induratio penis plastica ( mp )  . 
den beginn und die dauer vor beginn der radiotherapie konnten viele patienten nur grob abschtzen ; die symptomarme spanne reichte von 0 , 56 jahre ( median 2 jahre )  . 
weitere symptome bestanden bei 15 ( 60% ) patienten mit schmerzen an der fusohle ( 20 fe ; 56% ) , acht ( 32% ) hatten gehstrungen ( 12 fe ; 33% ) , zwlf ( 48% ) andere symptome , z.b. 
das rt - konzept umfasste analog zur therapie des md insgesamt 2 rtserien zu je fnf fraktionen mit 3 gy einzeldosis ( 15 gy pro woche ) im abstand von 812 wochen ( gesamtdosis : 30 gy )  . 
 als vollstndige besserung wurde das vllige verschwinden der klinisch dokumentierten knoten , strnge bzw . subjektiven symptome und die wiedererlangung der vollen funktion des fues gewertet ; als wesentlich gebessert wurde der rckgang der knoten , strnge bzw . 
die verschlechterung der gehfunktion und / oder jede durchgefhrte operative manahme wurden als therapieversagen eingestu statistik relevante patientenund krankheitsparameter wurden mit median , mittelwert , standardabweichung und spanne fr stetigen parameter beschrieben ; absolutund prozentwerte wurden fr alle kategorialen variablen verwendet . 
8 von 36 ( 22% ) fen einen stabilen befund ; 20 ( 80% ) patienten bzw . 28 ( 78% ) fe waren in einem oder mehreren befunden oder symptomen rcklufig im vergleich zur ausgangssituation . tabelle 1 fasst die resultate fr alle patienten und fe zum zeitpunkt der letzten nachsorgeuntersuchung zusammen . 
ohne prognostische bedeutung waren alter , geschlecht , der vorlauf bis zur strahlentherapie oder andere patienten - , krankheitsoder therapiebezogene faktoren ; lediglich der beidseitige befall fiel fr einige endpunkte ungnstiger aus ( nicht signifikant )  . 
fnf ( 11% ) fen eine leichte hautrtung ( ctc 1 ) im bestrahlten feld auf ; zum aktuellen zeitpunkt wurde nur bei drei ( 8% ) fen im langzeitverlauf eine etwas trockenere haut im bestrahlten areal beobachtet im vergleich zu nicht bestrahlten arealen der haut an der fusohle . 
aktivierte monozyten und makrophagen , die die myofibroblastenproliferation auslsen , gelten auch als radiosensitives target , ebenso zytokine und wachstumsfaktoren , die die zellproliferation kontrollieren [ 3 , 32 , 34 , 40 , 41 ]  . 
radiotherapie bei morbus ledderhose wachstum , starke schmerzen oder gangstrungen bestehen . bei der resektion von knoten und strngen sind jedoch hohe rezidivund komplikationsraten bekannt [ 1 , 2 , 4 , 13 , 18 , 25 , 30 , 44 ]  . 
neben der lokalen exzision ( lex ) einzelner knoten und strnge kommem die weite subtotale exzision ( wex ) oder die komplette plantare fasziektomie ( pfe ) infrage , die oft gekoppelt mit freien haut ( total skin graft ) und fettgewebstransplantationen ( dermal fat graft ) erfolgt . 
rezidive mssen ausgedehnter operiert werden ( wex , pfe ) als zum zeitpunkt der primrmanifestation , und die prognose des rezidivs ist schlechter als die der primrlsion [ 22 ]  . 
 [ 13 ] operierten 13 fe bei elf patienten : siebenmal mit lex , neunmal mit wex und achtmal mit pfe . nur vier ( 36% ) patienten blieben langfristig ohne rezidiv , ein ( 14% ) patient nach lex , zwei ( 22% ) nach wex und drei ( 38% ) nach pfe . 
 [ 4 ] bei 33 patienten mit 2 jahren nachbeobachtung : 7 von 17 ( 41% ) patienten mit primrlsion , davon vier ( 40% ) nach lex , einer ( 33% ) nach wex und zwei ( 50% ) nach wex mit pfe oder hauttransplantation . 
fr rezidive wird heute die erweiterte operation ( wex / pfe ) mit freier hauttransplantation empfohlen [ 13 ]  . neu ist das verfahren mit freier hautund subkutaner fetttransplantation aus der bauchhaut , die als weniger komplikationstrchtig gilt [ 23 ]  . 
 wegen der wirksamkeit bei niedrig - malignen weichteiltumoren und desmoiden [ 28 ] wurde die radiatio als adjuvante manahme beim rezidiv des ml von fuchirurgen / orthopden ins spiel gebracht [ 13 ]  . 
unsere studie betritt daher klinisch neuland , da zur primren bestrahlung beim ml bislang keine klinischen studien vorliegen , die eine abschtzung von effektivitt und toxizitt der bestrahlung im frhen , progredienten stadium erlauben wrden . 
unsere untersuchung besttigt das gute ansprechen beim ml : in vielen fllen waren klinische manifestationen rcklufig , ein kleinerer teil blieb stabil , eine progression trat in keinem fall auf . 
von groer bedeutung fr die richtige bewertung knftiger klinischer studienergebnisse ist es , die indikationsstellung nur auf progrediente und symptomatische flle zu begrenzen und mit nachbeobachtung ber 510 jahre zu kontrollieren . 
martin brown2 background : eppendorf electrode measurements of tumor oxygenation have defined an adverse effect of tumor hypoxia on prognosis after radiotherapy and other treatment modalities , in particular in head and neck and cervix carcinomas as well as soft tissue sarcomas . 
recently , the immunohistochemical detection of proteins involved in the hypoxic response of tumor cells has been discussed as a method to estimate hypoxia in clinical tumor specimens . material and methods : this review focuses on clinical and experimental data , regarding prognostic impact and comparability with other methods of hypoxia detection , for three proteins suggested as endogenous markers of tumor hypoxia : hypoxia - inducible factor - 1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) ) , carbonic anhydrase 9 ( ca 9 ) , and glucose transporter 1 ( glut1 )  . results : none of the three potential hypoxia markers is exclusively hypoxia - specific , and in each case protein can be detected under normoxic conditions in vitro . 
in nine of 13 reports , among them all three that refer to curative radiotherapy for head and neck cancer , hif - 1 ( cid : 1 ) overexpression was associated with poor outcome . 
clinical trials assessing a markers ability to predict a benefit from specific hypoxia - directed treatment ( e.g. , tirapazamine , arcon concept ) are necessary to define the potential of individual markers . 
 key words : tumor hypoxia hypoxia markers radiotherapy radiation resistance strahlenther onkol 2003 ; 179 : 80111 doi 10.1007 / s00066 - 003 - 1150 - 9 endogene tumorhypoxiemarker : indikatoren klinischer strahlenresistenz ? hintergrund : eppendorf - elektroden - messungen der tumoroxygenierung haben den ungnstigen effekt der tumorhypoxie auf die prognose nach strahlenbehandlung und anderen therapieformen gesichert , insbesondere bei hnound zervixkarzinomen sowie weichteilsarkomen . 
 material und methodik : diese bersicht umfasst klinische und experimentelle daten zum prognostischen wert und zur vergleichbarkeit mit anderen methoden der hypoxiemessung fr drei potentielle endogene hypoxiemarker , und zwar hypoxia - inducible factor - 1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) ) , carboanhydrase 9 ( ca 9 ) und glucose - transporter 1 ( glut1 )  . 
hif - 1 ( cid : 1 ) reagiert schnell auf hypoxie , aber auch auf reoxygenierung , so dass die stabilitt dieses markers im rahmen einer routinemigen probengewinnung problematisch ist . 
in neun von 13 arbeiten , darunter alle drei zur primren radiotherapie von hno - tumoren , war die hif - 1 ( cid : 1 ) - berexpression mit einer ungnstigen prognose assoziiert ( tabelle 2 )  . 
ca 9 war ein negativer prognosefaktor fr zervixkarzinome , hno - tumoren und bronchialkarzinome , in zwei weiteren hno - serien aber nicht mit der prognose korreliert ( tabelle 3 )  . 
 1 department of radiation oncology , university of wrzburg , germany , 2 department of radiation oncology , division of radiation and cancer biology , stanford university school of medicine , stanford , ca , usa . received : january 13 , 2003 ; accepted : september 8 , 2003 strahlenther onkol 2003 no . 
 schlsselwrter : tumorhypoxie hypoxiemarker strahlentherapie strahlenresistenz introduction the presence of hypoxic regions within tumors has been shown to adversely affect the outcome of radiotherapy and other treatment modalities in several tumor entities , including carcinomas of the head and neck and uterine cervix as well as soft tissue sarcomas [ 12 , 21 , 29 , 40 , 50 , 52 , 59 ]  . 
different approaches are pursued to overcome or exploit the low - oxygen conditions of these tumors , among them an escalation of radiation dose to hypoxic tumor regions [ 56 ] , inhalation of modified gas mixtures during the radiotherapy session with or without vasoactive substances [ 6 , 35 ] , use of hypoxia - specific cytotoxins such as tirapazamine ( review in [ 13 ] ) , correction of anemia [ 19 , 68 ] , use of hypoxia - mediated gene therapy [ 18 , 54 , 63 ] , and administration of genetically altered anaerobic bacteria [ 47 ]  . 
although the association of tumor hypoxia and poor prognosis has mainly been established on the basis of eppendorf oxygen electrode measurements , this invasive method cannot easily be applied to intraabdominal or intracranial tumor sites , and alternative ways of determining tumor hypoxia are desirable . 
other methods to estimate tumor hypoxia , including the immunohistochemical detection of injectable 2 - nitroimidazole hypoxia markers , such as pimonidazole and ef5 , are currently being tested in clinical trials [ 37 , 51 ] , and nuclear medicine and magnetic resonance imaging techniques [ 14 , 28 ] have been suggested . 
these proteins , among them hypoxia - inducible factor - 1 ( hif - 1 ) , carbonic anhydrase 9 ( ca 9 ) and the glucose transporter 1 ( glut1 ) , can be detected immunohistochemically in archival pathologic material allowing retrospective analysis of tumor oxygenation and treatment outcome . 
this review will summarize clinical studies on the prognostic impact of the expression of such markers in various tumor entities , experimental data on the biological role of these proteins as well as studies on the comparison of such markers with other methods of hypoxia detection . 
 in 51 cervix carcinoma patients treated with radiotherapy for mainly advanced tumors , the 3 - year disease - free survival was 36% for patients with hypoxic tumors and 66% for patients with better - oxygenated tumors , using the median hp5 value of 22% as a cutoff point [ 40 ]  . 
most recently , in a thorough statistical analysis of a large cohort of 106 cervix cancer patients treated with radiotherapy at princess margret hospital , 3 - year progression - free survival was also decreased with 37% in patients with hypoxic tumors ( > 50% hp5 ) versus 67% in the better oxygenated , the prognostic impact of hypoxia being significant on multivariate analysis only in node - negative patients [ 21 ]  . 
 the hypoxic response of tumor cells the adverse effect of tumor hypoxia on prognosis is a result of several mechanisms including ( 1 ) direct treatment resistance of hypoxic tumor cells due to lack of oxygen in fixation of dna damage caused by radiation or drugs , ( 2 ) resistance of hypoxic cells to chemotherapy because they are furthest from blood vessels and often nonproliferating , and ( 3 ) hypoxiamediated selection of tumor cells with a more aggressive and metastatic phenotype ( review in [ 13 ] )  . 
a major common mechanism of regulation of hypoxia - inducible genes is through the transcription factor hypoxia - inducible factor - 1 ( hif - 1 ) , a dimer consisting of the subunits hif - 1 , the expression of which is induced by hypoxia , and hif - 1 ( cid : 2 ) which is constitutively expressed independently of hypoxia ( review in [ 62 ] )  . hif - 1 is rapidly degraded via the ubiquitin pathway under normoxic conditions but accumulates under hypoxia ( figure 1 )  . 
the functional von - hippel - lindau ( vhl ) protein is essential for hif - 1a ubiquitination , explaining the constitutive overexpression of hif - 1 in clinical tumors with vhl mutations ( see below )  . 
the hypoxia - dependent mechanism allowing stabilization of hif - 1 is its modification under aerobic conditions by a prolyl hydroxylase which allows hif - 1 to interact with the vhl complex to produce polyubiquitination that targets the protein for proteasome - dependent degradastrahlenther onkol 2003 no . 
under normoxic conditions , hif - 1 ( cid : 1 ) , after oxygen - dependent modification by a prolyl hydroxylase , binds to the von - hippel - lindau ( vhl ) protein and is degraded via the ubiquitin pathway . 
in hypoxia , hif - 1 ( cid : 1 ) is stabilized , translocates to the nucleus , forms the dimer hif - 1 with its partner hif - 1 ( cid : 2 ) and binds to hypoxia - responsive elements ( hres ) of hypoxia - regulated genes . 
schematische darstellung der funktion des hypoxia - inducible factor - 1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) )  . unter normoxischen bedingungen bindet hif - 1a nach o2 - abhngiger modifikation durch eine prolylhydroxylase an das von - hippel - lindau - ( vhl - ) protein und wird ber den ubiquitin - weg abgebaut . 
unter hypoxie wird hif - 1 ( cid : 1 ) stabilisiert und transloziert in den nukleus , wo es mit hif - 1 ( cid : 2 ) das dimer hif - 1 bildet und an sog . 
under hypoxia , hif - 1 translocates to the nucleus , forms a dimer with hif - 1 ( cid : 2 ) and binds to hypoxia - responsive elements ( hres ) of hypoxia - regulated genes . 
over 30 hif - 1regulated genes have been described , among them vascular endothelial growth factor ( vegf ) , glucose transporter 1 ( glut1 ) , lactate dehydrogenase a ( ldh - a ) and nitric oxide synthase ( nos ; review in [ 61 ] )  . 
each of the hif - 1 - regulated proteins , as well as the transcription factor subunit itself , can be regarded as a potential surrogate marker of tumor hypoxia . 
most clinical and experimental investigations of such markers have focused on hif - 1 , glut1 and ca 9 , which have been reported to be the most consistently upregulated by hypoxia in expression - profiling studies [ 44 ]  . 
despite some interest in the use of vegf as an endogenous hypoxia marker [ 7 , 20 ] , immunohistochemical studies of this marker have revealed no association with hypoxia as measured by pimonidazole binding or eppendorf electrode [ 57 , 75 ]  . 
 experimental data on endogenous hypoxia markers the oxygen - concentration dependence and time course of marker accumulation under in vitro hypoxia as well as the inducibility by nonhypoxic stimuli are critical characteristics of potential hypoxia markers . 
a critical level is about 0.5% o2 , representing the half - maximal oxygen effect on radiosensitivity [ 26 ]  . with regard to time , it is of interest to differentiate between indicators of chronic ( diffusion - limited ) hypoxia and of acute ( intermittent , perfusion - limited ) hypoxia . 
for comparison , the binding of injectable 2 - nitroimidazole - derivative hypoxia markers such as pimonidazole has been shown to increase dramatically below an o2 concentration of about 1.3% ( 10 mmhg ) and is considered to indicate chronic hypoxia [ 24 , 58 ]  . 
 hif - 1 a landmark study on the expression of hif - 1 protein in hela cells during chronic hypoxia ( 4 h ) reported detectable protein at 20% o2 , a modest increase between 20% and 6% , a dramatic rise below 6% with a maximum at 0.5% , and a drop at 0% , attributed to an effect of anoxia on overall transcription and translation [ 34 ]  . 
similar observations were made in ht 1080 human fibrosarcoma cells when hif - 1 gene transactivation was measured by means of green fluorescent protein driven by a promoter containing hres to which the hif - 1 complex binds [ 72 , 73 ]  . 
demonstrated that 13 of 17 cell lines investigated , among them breast carcinoma , sarcoma and lymphoma lines , constitutively expressed hif - 1 at normoxia [ 82 ]  . 
upon reoxygenation , hif - 1 levels decreased by 8 min and became undetectable after 32 mthese data suggest that proper sample collection is crucial in the interpretation of hif - 1 labeling in tumor tissue , as ex vivo changes in oxygenation of a tissue block may rapidly affect strahlenther onkol 2003 no . 
hypoxia - dependent accumulation of hypoxia - inducible factor - 1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) ) protein in nuclear extracts of u87 mg human glioblastoma cells in vitro . 
hypoxieabhngige akkumulation des hypoxia - induciblefactor - 1 ( cid : 1 ) - ( hif - 1 ( cid : 1 ) - ) proteins in kernextrakten von u87 mg humanen glioblastomzellen in vitro . 
however , based on the in vitro data , marker positivity would be expected at higher o2 concentrations than , e.g. , for pimonidazole , and some staining would even be expected in normoxic regions . 
these include nitric oxide ( no ) , interleukin - 1 ( cid : 2 ) ( il - 1 ( cid : 2 ) ) , tumor necrosis factor ( tnf - ) , trophic stimuli including serum , insulin and insulinlike growth factors ( igf - 1 , igf - 2 ) as well as genetic alterations such as v - src oncogene overexpression or p53 , pvhl or pten inactivation ( review in [ 66 ] )  . 
 the colocalization of hif - 1 and the injectable hypoxia marker ef5 , a 2 - nitroimidazole derivative such as pimonidazole , was investigated in cervical carcinoma xenografts [ 74 ]  . 
however , the percentages of ef5 - positive pixels staining for hif - 1 and of hif - 1 - positive pixels staining for ef5 ranged between 10% and 20% , indicating considerable discordance between these two markers . 
 a flow - cytometric study of hif - 1 and pimonidazole staining in u87 human glioma xenograft tumors from mice breathing modified o2 concentrations indicated a correlation of the percentages of positive cells for the two markers and a response of both markers to 10% o2 and carbogen ( 95% o2 / 5% co2 ) breathing [ 71 ]  . 
since there is a second oxygen - dependent step that inhibits hif - 1 transactivation of target genes [ 45 ] , it would be anticipated that ca 9 protein levels , like other target genes , would show a better correlation with low oxygen levels than would hif - 1 itself . for ca 9 , wykoff et al . 
have demonstrated in several cell lines , including hela and a549 , that the hypoxic induction of mrna is hif - 1 - mediated and that vhl dysfunction in renal cell carcinoma cell lines causes hypoxia - independent ca 9 upregulation . 
hypoxic overexpression of ca 9 protein was also observed in three head and neck carcinoma cell lines , two of them showing weak bands in normoxic conditions [ 5 ]  . 
in a549 cells , a progressive increase in ca 9 protein levels was observed for cells exposed for 16 h over a range from 5% to 0.1% o2 [ 77 ]  . 
an investigation of the expression time course in d247 - mg glioblastoma cells showed much higher ca 9 expression , both at mrna and protein levels , after 24 h at 1.5% o2 than after 10 h , indicating an association with chronic hypoxia [ 44 ]  . recent results from kaluz et al . 
suggest that in hela cells , cell density - induced ca 9 expression is caused by mild hypoxia due to cell - to - cell contact and regulated by an hif - 1independent pathway involving phosphatidylinositol - 3 - kinase ( pi3k ) [ 38 ]  . 
such distinct mechanisms at different oxygen concentration ranges could explain strong ca 9 labeling in regions consistent with severe chronic hypoxia ( e.g. , as identifiable by pimonidazole adduct formation ) and weaker labeling closer to blood vessels , as observed in some histopathologic studies [ 37 , 53 ]  . 
in a flow - cytometric analysis , increased ca 9 positivity of cells from cervical carcinoma xenografts was found to be associated with worse perfusion ( as indicated by hoechst 33342 label ) and more intense pimonidazole label [ 53 ]  . 
by sorting of live cells according to ca 9 status and subsequent plating for clonogenic survival assay , the authors of this study convincingly demonstrated that cells with strong ca 9 signal were more radioresistant than those with weak or no signal . 
however , glut1 protein was detectable under normoxic conditions , and induction of glut1 mrna was also observed in cultured cells after transformation with the ras oncogene [ 15 ]  . 
 distribution of endogenous hypoxia markers in human histopathologic material hif - 1 the presence of hif - 1 in normal tissue and human tumor material has been investigated in two large immunohistochemical series [ 67 , 81 ]  . 
cells in normal tissues identified as being , at least in some cases , hif - 1 - positive included adrenal cortical cells , distal tubular epithelial cells of the kidney , acinar cells of the pancreas , and seminiferous tubules of the testis [ 81 ]  . 
however , localized positive areas or more diffuse staining patterns were also observed , suggesting that these may be a result of genetic alterations or microenvironmental factors other than chronic hypoxia . 
percentage of human tumors containing tumor cells positive for hypoxia - inducible factor - 1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) ) or for carbonic anhydrase 9 ( ca 9 ) , as detected by immunohistochemistry in three large histopathologic series . 
prozentualer anteil humaner tumoren mit immunohistochemisch fr hypoxia - inducible factor - 1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) ) oder carboanhydrase 9 ( ca 9 ) positiven tumorzellen in der bersicht dreier histopathologischer serien . 
die prozentangaben sind der anteil an tumoren mit spezifischer anfrbung und weisen nicht auf die prozentzahl positiver zellen in diesen tumoren h tumor entity hif - 1 - positive tumors zhong et al . 
 [ 31 ] ca 9 - positive tumors 100% prostate adenocarcinoma colon adenocarcinoma breast adenocarcinoma breast ( metastatic lymph nodes ) breast fibroadenoma high - grade glioma low - grade glioma cervix carcinoma head and neck carcinoma 100% 100% hypoxia ( considering the rapid hif - 1 accumulation under hypoxic conditions ) , and a third pattern of staining unrelated to the distance from the nearest blood vessel [ 27 ]  . 
demonstrated that in 75% of clear cell renal carcinomas , nuclear hif - 1 staining was present in virtually all cells , while focal expression was observed in non - clear cell renal carcinomas [ 76 ]  . 
considering the role of the vhl protein in hif - 1 degradation under normoxic conditions ( figure 1 ) , clear cell renal carcinoma is considered a classic example of hif - 1 overexpression resulting from genetic alteration rather than microenvironmental stimuli . 
similarly , immunohistologic studies in brain tumors found a predominantly perinecrotic hif - 1 staining pattern in glioblastoma multiforme [ 65 , 80 ] , but a similarly strong but diffuse staining in hemangioblastomas and oligodendrogliomas [ 9 , 80 ] , which both are well vascularized and do not usually contain areas of necrosis . it was suggested that in hemangioblastomas and oligodendrogliomas oncogenic stimuli and not hypoxia cause hif - 1 stabilization . in oropharyngeal carcinoma , focal hif - 1 expression distal from the closest blood vessel was observed in 65% of positive tumors ( figure 3 ) and diffuse staining in the remainder [ 1 ]  . 
identified three distinct patterns of hif - 1 localization : one with positive cells within a typical oxygen diffusion distance ( 50200 mm ) , reflecting chronic hypoxia , one with staining adjacent to blood vessels interpreted as acute or intermittent figure 3 . 
immunohistochemical staining for hypoxia - inducible factor1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) ) in a tissue section of squamous cell carcinoma of the oropharynx . 
positive staining is observed at a distance from blood vessels ( arrowheads ) , a pattern compatible with chronic hypoxia , similar to staining patterns typical of the injectable tumor hypoxia marker pimonidazole . 
immunhistochemische frbung zum nachweis von hypoxia - inducible factor - 1 ( cid : 1 ) ( hif - 1 ( cid : 1 ) ) an einem schnitt eines plattenepithelkarzinoms des oropharynx . 
endogenous hypoxia markers ca 9 in a large screen of ca 9 expression in normal tissues and tumors , high levels of ca 9 were found in normal bile duct , gall bladder , gastric mucosa , intestinal crypt cells , and the choroid plexus , but not in normal kidney , breast , brain , or prostate [ 31 ]  . 
 a perinecrotic staining pattern , consistent with areas of chronic hypoxia , was also suggested by two studies of ca 9 expression in cervical carcinoma , three head and neck cancer series , and one report on non - small - cell lung cancer [ 5 , 23 , 37 , 41 , 48 , 53 ]  . 
in head and neck tumors , the mean distance of ca 9positive regions from blood vessels was 80 m , interpreted as representing oxygen concentrations around 1% [ 5 ]  . 
 glut1 in a comprehensive analysis of glut1 expression in tissue and tumor material , glut1 was largely undetectable in normal epithelial tissues and benign tumors , but expressed in a variety of human carcinomas [ 79 ]  . 
in colorectal carcinoma , glut1 staining was typically localized to the plasma membrane and expressed in 90% of cases , while normal colonic epithelium was always negative [ 25 ]  . 
a perinecrotic localization of glut1 in rectal cancer has recently been described [ 17 ]  . glut1 is also regularly expressed in head and neck carcinoma [ 49 ]  . 
in cervical carcinoma , glut1 was described as being consistently located at a distance from perfused blood vessels with heavy staining both in and around areas of necrosis [ 2 ]  . 
 prognostic value of marker expression in tumor patients the prognostic role of potential endogenous markers of tumor hypoxia has been investigated in several tumor entities : the clinical results for hif - 1 are summarized in table 2 . 
of 13 papers identified , nine describe an association of high hif1 expression and poor prognosis , either expressed as overall survival , disease - free / progression - free survival or initial response to treatment . 
in particular , such observations were made in all three papers reporting on curative radiotherapy ( with or without chemotherapy ) of head and neck tumors [ 2 , 30 , 42 ]  . 
in cervix cancer , an association of high hif - 1 expression and poor disease - free and overall survival has been described for mainly surgically treated patients [ 10 ]  . 
in more advanced stages treated with radiotherapy , a correlation of hif - 1 overexpression and low oxygenation as assessed by eppendorf electrode measurements , but no impact on disease - free survival was found [ 27 ]  . 
these data can be interpreted as supporting in principle the use of hif - 1 as an endogenous hypoxia marker , with the limitation that in cervical cancer the prognostic value even of eppendorf electrode measurements is somewhat less clear than in head and neck tumors [ 21 ]  . 
 of five clinical reports on ca 9 , three , including patient groups with head and neck cancer treated with chemoradiation and advanced cervix cancer treated with radiotherapy , found an association of high ca 9 expression and poor outcome ( table 3 )  . 
however , a cohort of nasopharyngeal carcinoma patients treated with radiotherapy ( with or without chemotherapy ) and a group of head and neck cancer patients treated with various modalities showed no association of ca 9 expression and prognosis [ 30 , 37 ]  . 
in contrast to the data for hif - 1 , for which an association with high microvessel density ( mvd ) and high vegf expression was frequently described across all tumor entitities ( table 2 ) , ca 9 expression appeared to be related to low mvd and not to vegf expression ( table 3 )  . 
in 112 patients treated surgically for colorectal carcinoma ( mainly stages dukes b1c1 ) , comparison of survival between patients with strong versus weak glut1 immunostaining revealed a significantly decreased survival rate on univariate analysis for patients with strong expression of the marker [ 25 ]  . 
an association of high glut1 expression with poor overall survival and metastasis - free survival , but not local control , was also observed in a preliminary report on rectal carcinoma patients [ 17 ]  . 
for the whole group , there was a significantly improved metastasis - free survival in patients with glut1 - negative versus glut1 - positive tumors , but no such effect on disease - free survival or overall survival . 
a combined analysis of glut1 and glut3 expression in resected stage i non - small - cell lung cancer revealed significantly improved overall survival in the absence of both markers as compared to positivity for one or both [ 78 ]  . 
 correlation of marker expression with other hypoxia detection methods in patients several investigators have reported on the association of the percentage of cells in a biopsy specimen that were positive for a specific marker with the percentage of eppendorf measurements below a certain oxygen pressure , e.g. , 5 mm hg ( hp5 )  . all these studies were performed in carcinoma of the cervix . 
endogenous hypoxia markers ( cid : 1 ) ( cid : 1 ) ( cid : 1 ) ( cid : 1 ) ( cid : 1 ) ( cid : 1 ) ( cid : 1 ) age were positively and significantly correlated , although hif - 1 in this study was not associated with prognosis [ 27 ]  . in a different group of 130 patients with mainly advanced cervical carcinoma , a semiquantitative score describing the proportion of ca 9 - positive cells was significantly correlated with hp10 , hp5 , hp2.5 , and with median po2 [ 48 ]  . 
finally , in a prospective study of glut1 expression in cervix cancer , the glut1 positivity score was significantly correlated with hp2.5 ( trend for hp5 and hp10 ; [ 2 ] )  . this patient group was different from the cohort analyzed retrospectively in the same report , showing a significant impact of glut1 status on metastasisfree survival only . 
by comparison , the semiquantitative labeling score for the injectable hypoxia marker pimonidazole , to which endogenous markers may be an alternative , was not correlated with eppendorf electrode measurements in a group of 28 patients with advanced cervix cancer [ 51 ]  . 
it should be kept in mind that electrode measurements and immunohistochemical marker detection usually describe different areas of a tumor , as in none of these studies biopsies were consistently taken from the electrode track . the colocalization of the injectable hypoxia marker pimonidazole and hif1 in surgical specimens from patients with scchn was recently described by janssen et al . 
while typical pimonidazole staining at a distance from blood vessels with peaks around 80 mm was observed , the hif - 1 staining pattern was more variable without clear peaks . 
whereas the staining pattern for pimonidazole and ca 9 was similar in these tumors , ca 9 positivity was observed already at shorter distances from the blood vessels than pimonidazole , suggesting upregulation of ca 9 at intermediate oxygen concentrations . in this group , pimonidazole but not ca 9 staining was associated with locoregional control . 
 future directions in the clinical implementation of endogenous hypoxia markers the experimental and clinical data summarized above suggest that endogenous markers of tumor hypoxia may have a role in the selection of patients for modified treatment in the future . hif - 1 and ca 9 have shown the potential to function as intrinsic hypoxia markers , but there is a long list of other candidate proteins that have not yet been investigated . 
the extensive data collected on hif - 1 expression in clinical tumor specimens supporting an effect on prognosis suggests a use of this marker , but the poor stability of this protein upon reoxygenation would call for prospective collection of tumor material under standardized conditions . 
 the ultimate test for each hypoxia marker , endogenous or injected , is its ability to predict a benefit from modified treatment aimed specifically at hypoxic tumor cells , including , e.g. , the arcon ( accelerated radiotherapy , carbogen and nicotinamide ) treatment or hypoxic cytotoxins such as tirapazamine . 
 similarly , it would be of great interest to investigate hypoxia marker expression in archival tumor material from trials in which the hypoxic cytotoxin tirapazamine was or is investigated and to determine the treatment response of subgroups . to address the question whether the impact of hif - 1 , ca 9 or glut1 overexpression on prognosis is a direct result of hypoxic radioresistance or of hypoxia - induced pro - metastatic events two effects which can hardly be separated even in the context of eppendorf electrode measurements , it appears useful to compare the association of marker expression and prognosis in subgroups treated with and without radiotherapy [ 70 ]  . 
published data on cervix carcinoma and oligodendroglioma have been reanalyzed in this respect : the impact of marker expression on prognosis was not stronger in irradiated patients , but the adjuvant nature of radiotherapy in these groups limits the interpretation of this result . 
although not exclusively hypoxia - specific , the association of marker expression with measurements of tumor hypoxia using the eppendorf electrode suggests that these proteins are potential surrogate markers of tumor hypoxia . 
with regard to marker distribution in tumor sections and colocalization with injectable markers , ca 9 appears to be more suitable for clinical use than hif - 1 . however , ca 9 has a relatively slow response to changes in tumor oxygenation and so probably does not reflect the dynamic nature of tumor hypoxia as well as do electrode measurements or measurements of injectable markers . 
ultimately , clinical trials evaluating the ability of a marker to predict a benefit from hypoxia - directed treatment are necessary to judge the value of any potential marker of tumor hypoxia . 
 strahlentherapie und onkologie originalarbeit behandlungsergebnisse beim follikulren keim zentrumslymphom stadium i und ii holger neumann1 , hilpert blanck2 , rainer koch3 , steffen fiedler2 , aquina lesche2 , thomas herrmann2 hintergrund : in den frhen stadien des follikulren keimzentrumslymphoms wird die strahlentherapie als kurative behandlungsmanahme eingesetzt . 
kombiniert radiotherapie / chemotherapie ( 13 patienten ) behandelt . strahlentherapie wurde als involved - field - ( ifi ) ( 104 patienten ) , extended - field - ( efi ) ( neun patienten ) und total - nodale bestrahlung ( tni ) ( drei patienten ) durchgefhrt . 
 schlsselwrter : follikulres keimzentrumslymphom zentrozytisch - zentroblastisches ( cc - cb - ) lymphom radiotherapie rezidivmuster strahlenther onkol 2003 ; 179 : 8406 doi 10.1007 / s00066 - 003 - 1025 - 0 follicle centre lymphoma : treatment results for stage i and ii purpose : radiotherapy is a curative treatment modality in the early stages of follicle centre lymphoma . 
radiotherapy was applied as involved - field - ( ifi ) ( 104 patients ) , extended - field ( nine patients ) or total - nodal ( three patients ) irradiation . 
patients received doses between 25 gy and 50 gy ( median 35 gy )  . results : the 5and 10 - year actuarial overall survival rates were 76% and 51% . 
 key words : follicle centre lymphoma cc - cb - lymphoma radiotherapy relapse pattern 1 praxis fr strahlentherapie , humaine - klinik dresden , 2 klinik fr strahlentherapie / radioonkologie der technischen universitt dresden , 3 institut fr biomedizin / medizinische statistik der technischen universitt dresden . 
behandlung des follikulren keimzentrumslymphoms einleitung die follikulren keimzentrumslymphome stellen nach den grozelligen b - zell - lymphomen die zweithufigste entitt nodaler lymphome dar und sind daher von hoher klinischer relevanz [ 36 ]  . 
in einer multizentrischen studie wird gegenwrtig geprft , ob durch eine intensivierung der primren strahlentherapie mit ausdehnung der bestrahlten regionen das rezidivrisiko gesenkt und eine verbesserung der gesamtprognose erzielt werden kann [ 30 ]  . 
die histologische diagnose zentrozytisch - zentroblastisches ( cc - cb ) lymphom basierte auf den einteilungskriterien der kiel - klassifikation und entspricht den follikulren keimzentrumslymphomen ( r.e.a.l. - klassifikation ) oder follikulren lymphomen ( who - klassifikation ) [ 14 , 36 , 37 ]  . 
 patienten und methoden im universittsklinikum dresden wurden im zeitraum 19701999 insgesamt 116 patienten mit follikulrem keimzentrumslymphom stadium i ( n = 71 / 61% ) und ii ( n = 45 / 39% ) behandelt . 
staginguntersuchungen waren bis zur einfhrung der computertomographie ( ct ) ( bei 52% der patienten ) die lymphographie ( 48% ) und der abdominale ultraschall sowie eine komplette labordiagnostik und histologische sicherung bei allen patienten . 
 therapie die strahlentherapie wurde berwiegend als involved - field ( ifi ) - bestrahlung ( 86% ) , bei neun patienten ( 8% ) als extended - field - ( efi ) - bestrahlung sowie bei drei patienten ( 3% ) als total - nodale bestrahlung ( tni ) durchgefhrt . 
infradiaphragmale efi erfolgte ber ein umgekehrtes y - feld zur erfassung der paraaortalen , iliakalen und inguinalen lymphknoten ber ventrodorsale gegenfelder oder eine gesamte abdominale oder pelvine bestrahlung in abhngigkeit von der lymphomlokalisation . 
drei patienten erhielten dosen von 25 gy , davon zwei therapieabbrecher . bei einem patienten wurde eine primr palliative behandlung ( 5 ( cid : 1 ) 5 gy ) aufgrund schlechten allgemeinzustands bei ausgetabelle 1 . 
 klinisches stadium ( nach ann - arbor - klassifikation ) alter < 50 jahre > 50 jahre stadium i stadium ii geschlecht mnnlich weiblich befallene lymphknotenregionen supradiaphragmal infradiaphragmal primrlokalisation nodal extranodal patienten strahlenther onkol 2003 no . 
die einzeldosen betrugen blicherweise 1 , 82 gy ( ein patient 5 gy ) und bei bestrahlung des abdomens ( magenoder mesenterialbefall ) 1 , 0 gy ( fnf patienten )  . 
 statistische analyse die berlebensdaten wurden berechnet vom zeitpunkt der diagnosestellung bis zum todesdatum oder zensiert bis zum letzten beobachtungstermrezidivfreies berleben wurde ermittelt vom therapieabschluss bis zum datum des rezidivnachweises nur bei patienten mit initial kompletter remission . 
 rezidive wurden in in - field , out - field / nodal , out - field / extranodal oder disseminiert ( > 2 rezidivlokalisationen oder knochenmarkbefall ) gruppiert ; des weiteren erfolgte eine unterteilung nach rezidivlokalisation auf der gleichen zwerchfellseite oder transdiaphragmal . 
des weiteren war ein hochsignifikanter , prognostisch gnstiger einfluss auf das gesamtberleben bei patienten nachweisbar , die sich beim primren staging einer lymphographie unterzogen hatten ( 48% ) ( p < 0 , 004 )  . 
 at risk nach 10 / 15 jahren : 15 / 5 patientem at risk nach 10 / 15 jahren : 14 / 5 patientem berlebensfunktion zensiert berlebensfunktion zensiert 25 30 berlebenszeit ( jahre ) 25 30 rezidivfreie berlebenszeit ( jahre ) abbildung 1 figure 1 abbildung 2 figure 2 abbildungen 1 und 2 . 
behandlung des follikulren keimzentrumslymphoms at risk nach 10 / 15 jahren : ab 51 jahre : 8 / 2 patienten bis 50 jahre : 9 / 3 patientn altersgruppe ab 51 ab 51 zensiert p < 0 , 01 bis 50 bis 50 zensiert at risk nach 10 / 15 jahren : stadium i : 10 / 3 patienten stadium ii : 5 / 2 patientn stadium stadium 2 stadium 2 zensiert p < 0 , 03 stadium 1 stadium 1 zensiert berlebenszeit ( jahre ) berlebenszeit ( jahre ) abbildung 3 figure 3 abbildung 4 figure 4 abbildungen 3 und 4 . 
fnf patienten hatten in der region des lymphknotenrezidivs eine bestrahlungsdosis von 35 gy erhalten , ein patient 25 gy ( 5 ( cid : 1 ) 5 gy )  . 
ein patient wurde initial mit palliativer zielstellung ( 5 ( cid : 1 ) 5 gy ) behandelt , da ein ausgedehnter bulky - tumor ( 8 ( cid : 1 ) 10 cm ) bestand und der patient sich in reduziertem allgemeinzustand befand . 
rezidivmuster nach radiotherapie in abhngigkeit vom bestrahlungsvolumen ( ifi = involved - field - bestrahlung ; efi = extendedfield - bestrahlung ; tni = total - nodale bestrahlung ; 3 rezidivlokalisationen oder knochenmarkbefall )  . 
 bestrahlungsvolumen tni total rezidivlokalisation total limitiert ( gleiche zwerchfellseite ) in - field nodal extranodal transdiaphragmal nodal extranodal disseminiert unbekannt 44 ( 100% ) 5 ( 11% ) 1 ( 2% ) 0 1 ( 2% ) 2 ( 4% ) 6 ( 14% ) 1 ( 2% ) 2 ( 4% ) 19 ( 43% ) 2 ( 4% ) 0 3 ( 7% ) 8 ( 18% ) 0 21 ( 48% ) 3 ( 7% ) 8 ( 18% ) strahlenther onkol 2003 no . 
behandlung des follikulren keimzentrumslymphoms diskussion die rezidivfreien berlebensraten sind mit den bisher publizierten daten vergleichbar [ 9 , 12 , 13 , 19 , 26 , 27 , 38 ]  . 
das mediane alter der patienten dieser serie betrgt 62 jahre , andere autoren [ 12 , 26 , 27 ] geben ein medianes patientenalter von 5256 jahren an . der entscheidende prognosefaktor in unserem krankengut wie auch in anderen literaturberichten [ 7 , 13 , 22 , 26 , 30 ] ist das alter der patienten . 
im gegensatz zu mitteilungen anderer autoren [ 19 ] ist jedoch die rezidivrate bei patienten lter als 60 jahre in unserer untersuchung nicht signifikant hher , eine hhere aggressivitt der erkrankung bei lteren patienten scheint somit nicht unmittelbare ursache zu se46% der verstorbenen patienten lter als 60 jahre sind interkurrent verstorben ; sie scheinen jede form intensiver behandlung schlechter zu tolerieren . 
der hochsignifikante einfluss der lymphographie ( p < 0 , 004 ) in der multivariaten und univariaten analyse in unserer untersuchung kann mglicherweise als beleg fr limitierungen beim lymphknotenstaging mittels ct zumindest in den anfangsjahren der schnittbilddiagnostik interpretiert werden [ 6 , 10 , 40 ]  . 
diese beobachtungen sttzen die hypothese , dass die krankheit vor ihrer ausbreitung ursprung in einer einzelnen anatomischen region hat , somit eine lokale therapie im frhen stadium kurativ wirksam sein kann . 
 die zahl der in - field - rezidive entspricht den berichten anderer autoren [ 9 , 18 , 19 , 26 , 27 , 34 , 35 ] mit vergleichbarem patientengut und vergleichbaren bestrahlungsdosen . 
 der relativ hohe anteil nodaler rezidive ( 50% ) vorwiegend transdiaphragmal ( 48% ) entspricht ebenfalls den erfahrungen anderer untersucher [ 19 , 26 , 27 ] und kann mglicherweise durch eine prophylaktisch grovolumige bestrahlung gesenkt werden [ 30 ]  . 
eine abschtzung des stellenwerts prophylaktischer strahlentherapie anhand der vorliegenden daten ist nicht mglich , da nur 3% der patienten eine total - nodale und nur wenige patienten ( 8% ) eine efi erhielten . 
dieses ergebnis ist konkordant mit der berwiegenden zahl klinischer untersuchungen [ 3 , 5 , 21 , 24 , 41 ] sowie ergebnissen aktueller mikrobiologischer untersuchungen , die eine fusion strahlenther onkol 2003 no . 
behandlung des follikulren keimzentrumslymphoms zwischen aberrierten chromosomen und genen ( bcl2 ) beim follikulren keimzentrumslymphom fr die gesteigerte resistenz gegenber zytostatischen substanzen verantwortlich machen [ 7 , 15 ]  . 
neue therapeutische strategien sind weiterhin der einsatz des anti - cd20 - antikrpers idec - c2b8 ( rituximab ) , dessen substanzielle antilymphomaktivitt allein oder in kombination mit zytostatischer chemotherapie zu remissionsraten von 4050% fhren kann [ 3 , 4 , 8 , 11 , 15 , 39 ]  . 
 schlussfolgerungen zusammenfassend kann festgestellt werden , dass aufgrund der vorliegenden daten in bereinstimmung mit den ergebnissen anderer retrospektiver studien [ 9 , 12 , 13 , 19 , 20 , 26 , 27 , 38 ] die radiotherapie eine effektive und gut vertrgliche behandlungsmethode beim follikulren keimzentrumslymphom in den frhen stadien ist . 
der stellenwert einer prophylaktischen bestrahlung smtlicher lymphknotenregionen ist nicht gesichert und wird gegenwrtig in einer multizentrischen prospektiven studie [ 30 ] gepr die bedeutung einer zustzlichen zytostatischen chemotherapie vor oder nach strahlentherapie wie auch neuer innovativer therapiekonzepte ( interferon - alpha , anti - cd20 - antikrper , antikrpergekoppelte radioisotope ) ist ebenfalls unklar und gegenstand aktueller untersuchungen [ 15 , 16 , 31 , 33 ]  . 
kamath ss , marcus rb , lynch jw ; et al : the impact of radiotherapy dose and other treatment - releated and clinical factors on in - field control in stage i and ii non - hodgkin 's lymphoma . 
adjuvant cyclophasphamide , doxorubicin , vincristine , and prednisone chemotherapy after radiation therapy in stage i low - grade and intermediate - grade non - hodgkins lymphoma . cancer 1993 ; 71 : 234250 . 
 korrespondenzanschrift holger neumann humaine - klinik dresden malerstrae 31 01326 dresden deutschland telefon ( + 49 / 351 ) 26 - 360 , fax - 83531 e - mail : neumann@humaine - dd.de strahlenther onkol 2003 no . 
12 urban & vogel strahlentherapie und onkologie original article acute toxicity of adjuvant radiotherapy in locally advanced differentiated thyroid carcinoma first results of the multicenter study differentiated thyroid carcinoma ( msds ) andreas schuck1 , martin biermann2 , michaela k . 
mller1 , achim heinecke3 , otmar schober2 , normann willich1 background and purpose : the indication for adjuvant postoperative radiotherapy in patients with differentiated thyroid carcinoma ( dtc ) extending beyond the thyroid capsule has been an issue of controversy during the past 2 decades . 
in the multicenter study differentiated thyroid carcinoma ( msds ) , a randomization has been performed concerning external - beam radiotherapy in patients with dtc extending beyond the thyroid capsule ( pt4 pn0 / 1 / ( cid : 1 ) cm0 , tnm classification , 5th edition , 1997 ) following surgery and radioiodine therapy . radiation - associated toxicity has been prospectively evaluated . patients and methods : radiotherapy was performed with 50.4 gy ( pn0 ) or 54.0 gy ( pn1 / x ) to the cervical , supraclavicular and upper mediastinal lymph nodes . 
acute toxicity is tolerable in these patients . key words : differentiated thyroid carcinoma radiotherapy toxicity strahlenther onkol 2003 ; 179 : 8329 doi 10.1007 / s00066 - 003 - 1158 - 1 akute nebenwirkungen der adjuvanten strahlentherapie beim lokal fortgeschrittenen differenzierten schilddrsenkarzinoerste ergebnisse der multizentrischen studie differenziertes schilddrsenkarzinom ( msds ) hintergrund und ziel : die indikation zur postoperativen radiotherapie bei patienten mit differenziertem schilddrsenkarzinom ( dtc ) mit organkapselberschreitendem wachstum wurde in den letzten 20 jahren kontrovers diskutiert . 
 patienten und methodik : die radiotherapie im bereich der zervikalen , supraklavikulren und oberen mediastinalen lymphabflussgebiete wurde mit 50 , 4 gy ( pn0 ) oder 54 , 0 gy ( pn1 / x ) durchgefhrt . 
22 dieser patienten wurden bislang bestrahlt und bezglich der akutnebenwirkungen prospektiv nach den rtog / eortc - kriterien evaluiert . ergebnisse : whrend der radiotherapie wurde bei vier patienten maximal eine nebenwirkung vom schweregrad i beobachtet , 16 patienten entwickelten maximale akute nebenwirkungen grad ii und zwei patienten grad iii ( 9.1% ; 95% - konfidenzinterval [ ki ] 1.129 , 2% ) als . 
grad - iii - nebenwirkungen wurden nicht mehr beobachtet . schlussfolgerung : die mehrzahl der patienten entwickelt unter der strahlenbehandlung geringe bis mittelgradige nebenwirkungen , die sich bei der ersten nachsorgeuntersuchung bereits weitgehend zurckgebildet haben . 
 schlsselwrter : differenziertes schilddrsenkarzinom radiotherapie toxizitt iodine - 131 ( 131i ) therapy for ablation of the thyroid remnant was conducted according to the guidelines of the deutsche krebsgesellschaft ( german cancer society ) [ 10 ]  . introduction differentiated thyroid carcinoma ( dtc ) is a rare tumor with an incidence of 3 / 100 , 000 inhabitants in germany [ 3 ]  . 
the standard treatment for locally advanced dtc is surgical resection , radioiodine therapy , and suppression of thyroid - stimulating hormone ( tsh ) [ 10 , 15 ]  . 
patients with localized dtc extending beyond the thyroid capsule with or without lymph node metastases ( pt4 tumors according to the uicc classification , 5th edition , 1997 ) were treated with surgery and radioiodine therapy . 
patients with stage pt4 pn0 / 1 / x m0 dtc ( according to the uicc classification , 5th edition , 1997 ) with completion of surgical therapy with r0 / r1 resection were enrolled at the time of initial radioiodine therapy for ablation of the thyroid remnant , 4 weeks after surgery . patients had to be 1869 years old and had to have a karnofsky index 70% at the time of surgery . 
this included determination of human thyroglobulin ( htg ) after endogenous tsh stimulation following 4 weeks withdrawal of l - thyroxine and the following imaging modalities : 131i whole body scan , ultrasound imaging of the neck and abdomen , chest x - ray in two planes , and one thoracic ct scan without contrast agents any time between the time of surgery and the restaging . 
 radiotherapy patients randomized or allocated to therapy arm a ( externalbeam radiotherapy ) received external - beam radiotherapy in addition to surgery , ablative radioiodine therapy , and tshsuppressive l - thyroxine therapy ( tsh < 0.1 u / ml )  . 
in accordance with the current guidelines of the german society of radiation oncology ( degro ) [ 24 ] , external - beam radiotherapy was initiated after completion of ablative radioiodine therapy with complete elimination of cervical 131i uptake . 
 second order : thyroid bed , cervical lymph node regions including the central cervical compartment , the parajugular and submandibular lymph nodes , infraand supraclavicular lymph nodes , and upper mediastinu field margins were the mandible and mastoid process ( cranial ) , tracheal bifurcation ( caudal ) , and posterior cervical lymph nodes ( posterior )  . 
three - dimensional ( 3 - d ) or quasi - 3 - d planning according to icru 50 ( international commission of radiation units and measurements ) was mandatory . 
 toxicity radiation - associated toxicity has been evaluated prospectively according to the rtog / eortc criteria [ 23 ] for bone marrow , skin , mucosa , salivary glands , pharynx and esophagus , larynx , lung , upper gastrointestinal tract , and spinal cord . these are shown in table 2 . 
the evaluation of toxicity is performed by the treating radiation oncologist at the end of external - beam radiotherapy and at the first follow - up visit of the patient which is scheduled 2 months after the end of radiotherapy . 
 toxicity data are collected from the participating centers on case report forms ( crf ) , which are held available as files in the portable document format ( pdf ) on the studys webserver . 
 based on a maximum rate of 5% serious acute and of 5% serious chronic toxicity and a 10% chance of type 1 and type 2 error , a step function was calculated in advance for the maximum number of serious adverse events ( sae ) at a given number of completed radiotherapies , and incorporated into the strahlenther onkol 2003 no . 
 skin no change mucous no change membrane follicular , faint or dull erythema ; tender or bright erythema ; epilation ; dry desquamation ; decreased sweating injection , may experience mild pain not requiring analgesic confluent , moist desquamation ulceration , hemorrhage , other than skin folds ; pitting edema confluent fibrous mucositis may include severe pain requiring narcotic ulceration , hemorrhage , or necrosis necrosis patchy moist desquamation ; moderate edema patchy mucositis which may produce an inflammatory serosanguinous discharge ; may experience moderate pain requiring analgesic moderate to complete dryness ; ( complete dryness ; no taste ) thick , sticky saliva ; markedly altered taste acute salivary gland necrosis pharynx no change mild dysphagia or odynophagia ; moderate dysphagia or odynosevere dysphagia or odynoand phagia with dehydration or esophagus complete obstruction , ulceration , perforation , fistula salivary no change mild mouth dryness ; slightly gland thickened saliva ; may have slightly altered taste such as metallic taste ; these changes are not reflected in base - line feeding behavior , such as increased use of liquids with meals may require topical anesthetic or nonnarcotic analgesics ; may require soft diet larynx no change mild or intermittent hoarseness ; cough not requiring antitussive ; erythema of mucosa lung no change mild symptoms or dry cough or dyspnea on exertion spinal cord bone marrow normal leucos ( n / l ) : < 4 , 0003 , 000 thrombos ( n / l ) : < 100 , 00075 , 000 hb ( g / dl ) : < 1110 phagia ; may require narcotic analgesics ; may require puree weight loss ( > 15% from pretreatment base line ) or liquid diet requiring ng tube , i.v. 
fluids , or hyperalimentation whispered speech , throat pain marked dyspnea , stridor or or referred ear pain requiring narcotic ; confluent fibrinous exudate ; marked arytenoid hemoptysis with tracheostomy or intubation necessary persistent hoarseness but able to vocalize ; referred ear pain , sore throat , patchy fibrinous exudate or mild arytenoid edema not requiring edema narcotic ; cough requiring antitussive persistent cough requiring narcotic , antitussive agents ; dyspnea with minimal effort but not at rest severe respiratory insufficiency ; continuous oxygen or assisted ventilation severe cough unresponsive to narcotic antitussive agents or dyspnea at rest ; clinical or radiologic evidence of acute pneumonitis ; intermittent oxygen or steroids may be required paresthesia , paresis < 3 , 0002 , 000 < 2 , 0001 , 000 < 75 , 00050 , 000 < 50 , 00025 , 000 < 108 < 86.5 < 1 , 000 < 25 , 000 < 6.5 no change mild lhermittes sign severe lhermittes sign mono - , para - , quadriplegia study protocol . 
in the remaining 22 patients , acute toxicity during radiotherapy was evaluated , and in 19 of these patients , at least one follow - up examination after the completion of radiotherapy was performed . 
 the second - order target volume was treated with 45 gy in one patient , 50 gy in twelve , 54 gy in six , and 60 gy in two patients . 
maximal acute toxicity for skin , mucosa , salivary glands , pharynx , and larynx during radiotherapy and toxicity at the first follow - up visit after radiotherapy within 100 days after completion of treatment are shown in figures 2a to 2e . 
 in the two patients who experienced grade iii toxicities , a follow - up evaluation within 100 days after radiotherapy was performed and , at the time of this examination , no or only grade i toxicities were evident . 
 the critical value of grade iii and iv acute and chronic side effects as defined in the trial was not observed in the radiation ar the median karnofsky index during radiotherapy was 90% ( range 50100% )  . 
in 2003 , a new classification was introduced by the uicc : tumors with minimal penetration in the surrounding soft tissues are now classified as pt3 , tumors which show an infiltration of adjacent organs or structures are classified as pt4 . 
for dtc extending beyond the thyroid capsule , a positive influence on local control and survival has been shown in several retrospective analyses [ 7 , 12 , 27 ]  . 
the degro recommends radiotherapy for patients who present with pt4 tumors according to the uicc classification ( 5th edition , 1997 ) and considers radiotherapy a treatment option in patients with pt3 tumors and extensive lymph node involvement . 
toxicity in radiotherapy of differentiated thyroid carcinoma skin mucosa figure 2a abbildung 2a figure 2b abbildung 2b salivary glands pharynx figure 2c abbildung 2c figure 2d abbildung 2d larynx figures 2a to 2e . 
nebenwirkungen an der haut ( a ) , der schleimhaut ( b ) , den speicheldrsen ( c ) , am pharynx ( d ) und am larynx ( e ) whrend und innerhalb von 100 tagen nach abschluss der radiotherapie ( rt )  . figure 2e abbildung 2e patients developed subcutaneous fibrosis , and one patient developed spinal cord necrosis after repeated irradiation to the spinal cord [ 27 ]  . 
at the time of the analysis , 43 of 289 patients were in the randomization arfurthermore , only a few patients were allocated to the radiotherapy ar36 patients have been randomized or allocated to arm a ( with external - beam radiotherapy )  . 
the rtog / eortc score was chosen because it evaluates radiation - associated acute and chronic side effects and is easier to handle in a multicenter study than the lent - soma score . 
so far , there is no sufficient follow - up data available to evaluate chronic radiation side effects . the salivary function also changed during the observed period of time : even though the number of patients with grade ii toxicity is reduced at the follow - up visit , > 50% of the patients experience some sort of salivary impairment . 
 in head and neck cancers , the acute and chronic toxicities of conventional radiotherapy have been defined in the past . using the rtog score , the rates of acute grade iii and iv toxicities have been generally < 25% in rtog studies . 
however , some groups have reported up to 50% acute grade iii toxicities using rtog or similar descriptive criteria [ 6 , 9 , 17 , 26 ]  . although radiation doses are similar , radiation fields differ considerably between patients with head and neck cancers and patients with dtc . 
 conclusion in summary , the main acute toxicity in the patients of this study who received postoperative radiotherapy for locally advanced dtc was pharyngitis , esophagitis , laryngitis , and skin reactions . 
 acknowledgment the study is supported by the deutsche krebshilfe grant t 14 / 97 / wi i . strahlentherapie und onkologie case study differentiation between recurrent tumor and radiation necrosis in a child with anaplastic ependymoma after chemotherapy and radiation therapy bettina beuthien - baumann1 , gabriele hahn2 , cornelia winkler3 , georg heubner4 background : in patients after treatment for malignant brain tumors , a clear distinction between tumor recurrence and radiation necrosis can be challenging . 
diagnostic workup included repeated mri scans , pet with an 18f - amino acid and 18f - fluorodeoxyglucose ( fdg ) , as well as a brain biopsy . results : amino acid pet , performed when the lesions were still small , showed multiple small areas of mild uptake in close correlation to the mri lesions . 
although not typical , this result was suspicious of tumor seeding , the more since the lesions appeared in gray matter areas outside the high - dose - rate irradiation field . 
in the following months , the clinical picture stabilized . conclusion : the final interpretation of the lesions was multiple focal radiation necrosis based on perfusion abnormalities after chemotherapy and conformal hyperfractionated radiotherapy , probably due to an individually enhanced vulnerability of the cerebral vessels . key words : anaplastic ependymoma magnetic resonance imaging positron emission tomography hyperfractionated radiotherapy radiation necrosis strahlenther onkol 2003 ; 179 : 81922 doi 10.1007 / s00066 - 003 - 1141 - x differenzierung zwischen tumorrezidiv und strahlennekrose bei einem kind mit anaplastischem ependymom nach chemotherapie und strahlentherapie hintergrund : die differenzierung zwischen tumorrezidiv und strahlennekrose bei patienten nach therapie von malignen hirntumoren kann eine diagnostische herausforderung darstellen . 
dieser fallbericht schildert den klinischen verlauf und das diagnostische vorgehen bei einer patientin mit anaplastischem ependymom und schwer zu interpretierenden magnetresonanz ( mrt ) und positronenemissionstomographischen ( pet ) befunden . fallbericht : 1 , 5 jahre nach resektion , hyperfraktionierter strahlentherapie ( abbildung 1 ) und chemotherapie eines anaplastischen ependymoms im parietalen kortex ergab das mrt eines 11 - jhrigen mdchens multiple kleine kontrastmittelanreicherungen im frontalen kortex ( abbildung 2a )  . 
wenngleich nicht typisch , erschien dieser befund als verdchtig fr eine tumoraussaat , da die lsionen in einer hirnregion auftraten , die auerhalb der hochdosisregion des bestrahlungsfeldes lag ( abbildung 1 )  . 
eine fdg - pet , durchgefhrt bei zunahme der gre und anzahl der lsionen im mrt ( abbildung 2b ) , zeigte keinen intensiven glucosestoff1 department of nuclear medicine and pet center rossendorf , 2 section children radiology , institute of radiology , 3 department of radiation therapy and radiooncology , and 4 department of pediatrics , university hospital carl gustav carus , dresden , germany . 
 schlussfolgerung : abschlieend wurden die befunde als multiple fokale strahlennekrosen auf der grundlage einer vaskulren strung nach chemotherapie und strahlentherapie , vermutlich einer individuell erhhten empfindlichkeit der zerebralen blutgefe , interpretiert . schlsselwrter : anaplastisches ependymom magnetresonanztomographie positronenemissionstomographie hyperfraktionierte strahlentherapie strahlennekrose introduction anaplastic ependymoma is a rare malignant brain tumor which constitutes 510% of primary brain tumors in the first 2 decades of life [ 9 ]  . 
after three - dimensional treatment planning , a conformal hyperfractionated radiotherapy with 2 ( cid : 1 ) 1.2 gy per day to the extended tumor region up to 66 gy and a boost of 6 gy to the immediate tumor region was applied with a linear accelerator ( figure 1 )  . 
radiotherapy was followed by eight courses of chemotherapy with ccnu , vincristine and cisplat the entire treatment regimen was performed according to the hit - med 99 study protocol [ 19 ]  . 
to differentiate tumor spread from radiation necrosis , a pet with the 18f - labeled amino acid 18f - 3 - omethy - fluoro - dopa ( 18f - 3 - omfd ) was performed in november 2000 . 
the pet scan showed mild patchy tracer uptake in the frontal cortex ; on the overlay of the pet data on the actual mri ( mpitool [ 15 ] ) , these mildly increased uptake sites were in close correlation to the mri lesions ( figure 2a )  . although the uptake of the amino acid was low , seeding seemed more likely than radiation necrosis , since most of the lesions occurred in an area outside the 40 - gy isodose of radiotherapy . 
on mri , the size and number of lesions increased , now showing an additional lesion of about 3 cm in diameter in the left parietal region involving white and gray matter structures . 
 the rationale for using radioactively labeled amino acids is the upregulation of amino acid transporters in brain tumors in contrast to normal brain tissue [ 10 , 14 , 21 , 22 ]  . 
although a radioactive amino acid tracer for single - photon emission computed tomography ( spect ) exists as well , pet was applied to benefit from the scanners high resolution of 45 mm in terms of the rather small lesions this patient showed at the time of investigation . 
furthermore , tumor seeding seemed more likely than radiation necrosis , since the lesions did not appear in the high - radiation field but in brain areas which received lower radiation doses which normally do not evoke radiation necrosis [ 1 , 17 ]  . 
in retrospect , the small areas with mild amino acid uptake most likely represented leakage of tracer from damaged vessels into brain tissue , a pathology occurring early in the development of necrosis , as described in the publication by castel & caill [ 3 ]  . 
high - grade tumors typically show a glucose uptake higher than normal gray matter , while in low - grade brain tumors the glucose mefigure 2a abbildung 2a figure 2b abbildung 2b figures 2a and 2b . 
radiation necrosis normally shows very low glucose metabolism [ 4 ]  . since an anaplastic ependymoma is a highly malignant tumor and the lesion was mostly located in white matter , a high glucose uptake and a high contrast to the surrounding white matter structures could be expected in the case of recurrence . 
 the final interpretation of the early and late brain lesions was focal perfusion abnormalities after chemotherapy and radiotherapy resulting in multiple areas of necrosis , most probably due to an individually enhanced vulnerability of the cerebral vessels . 
 strahlentherapie und onkologie original article effects of radiation treatment planning and patient fixation on the results of postoperative radiotherapy of childhood medulloblastoma bla kocsis1 , gbor szkely2 , lilla pap1 , gyrgy nmeth1 purpose : to assess the prognostic factors and the benefit of introducing head fixation and ct - assisted radiation treatment planning following postoperative radiotherapy in 83 children with medulloblastoma . 
the influence of various factors including age , sex , tumor location , extent , type of surgery , risk group , radiation dose to posterior fossa and spinal axis , and the effect of head fixation and ct - assisted radiation treatment planning on 5 - year relapse - free and 5 - year overall survival was investigated . 
univariate analysis identified metastatic disease ( p = 0.034 ) and the application of head fixation and individual radiation treatment planning ( p = 0.013 ) as significant prognostic factors for overall survival . 
 key words : childhood medulloblastoma radiotherapy radiation treatment planning head fixation survival strahlenther onkol 2003 ; 179 : 8549 doi 10.1007 / s00066 - 003 - 1102 - 4 auswirkungen der bestrahlungsplanung und der patientenfixation auf den therapieerfolg beim medulloblastom ziel : beurteilung der prognostischen faktoren und des nutzens der einfhrung von kopffixation und ct - assistierter bestrahlungsplanung fr die postoperative radiotherapie bei 83 kindern mit medulloblasto patienten und methodik : zwischen 1986 und 1994 wurden 24 kinder ohne kopffixation behandelt , und die boostbestrahlung wurde ohne individuelle bestrahlungsplanung durchgefhrt . 
untersucht wurde der einfluss verschiedener faktoren , wie alter , geschlecht , tumorlokalisation und - ausdehnung , die art des chirurgischen eingriffs , die risikogruppe , die auf die posteriore fossa und die wirbelsule applizierte strahlendosis sowie der effekt der kopffixation und der ct - assistierten bestrahlungsplanung , auf das rezidivfreie 5 - jahres - berleben und auf das 5 - jahres - gesamtberleben . 
in der univariaten analyse erwiesen sich metastasen ( p = 0 , 034 ) sowie die kopffixation und individuelle bestrahlungsplanung ( p = 0 , 013 ) als signifikante prognostische faktoren fr das gesamtberleben . 
auch auf das rezidivfreie berleben hatten metastasen ( p = 0 , 028 ) sowie die einfhrung der kopffixation und der individuellen bestrahlungsplanung ( p = 0 , 009 ) signifikanten einfluss . 
in der multivariaten analyse waren metastasen ( p = 0 , 04 ) sowie die kopffixation und individuelle bestrahlungsplanung ( p = 0 , 045 ) unabhngige prognosefaktoren fr das gesamtberleben und das rezidivfreie berleben ( p = 0 , 036 und p = 0 , 041 )  . 
fr die postoperative bestrahlung der posterioren fossa wird in jedem fall unbedingt die kopffixation und die individuelle , auf ct basierende bestrahlung empfohlen . schlsselwrter : kindheit medulloblastom strahlentherapie bestrahlungsplanung kopffixation berleben 1 department of radiotherapy , and 2 department of cytogenetics , national institute of oncology , budapest , hungary . received : september 18 , 2002 ; accepted : august 28 , 2003 strahlenther onkol 2003 no . 
survival data of childhood medulloblastoma introduction medulloblastoma is a highly malignant , infratentorial , neuroectodermal tumor accounting for 20% of all pediatric brain tumors [ 3 , 17 ]  . 
medulloblastoma is primarily a disease of the very young child , with a peak incidence between 5 and 10 years of age , but rare in adults [ 3 , 17 ]  . regarding certain characteristics , it differs well from other tumors of the central nervous system ; these include its high radiosensitivity [ 22 ] , metastasis formation via the liquor circulation , and its property to metastasize outside the central nervous system [ 1 , 12 , 13 ]  . 
 the prognostic factors in childhood medulloblastoma have been well studied but have varied during the past 30 years : age , sex , histologic subtype , tumor location , quality of resection , and cerebrospinal fluid involvement have been found to be significant and nonsignificant by various studies [ 13 , 7 , 8 , 13 , 16 , 17 , 21 ]  . 
 according to the current consensus , it seems that in patients < 2 years of age , metastatic disease , involvement of brain stem or fourth ventricular floor , and radiation dose to the posterior fossa < 50 gy are correlated with a worse outcome [ 3 , 17 ]  . 
conformal radiotherapy of the brain requires precise and reproducible patient setup [ 15 ]  . thermoplastic masks provide an accurate immobilization of patients with brain tumors [ 6 ]  . 
 it was the purpose of this study to assess the benefit of introducing ct - assisted radiation treatment planning and head fixation in the postoperative radiotherapy of children with medulloblastoma . 
 patients and methods between 1986 and 2000 , 83 children with medulloblastoma received postoperative radiotherapy at the department of radiotherapy of the national institute of oncology , budapest , hungary . 
all 83 patients underwent surgery ; in 42 patients ( 50.6% ) radical ( subtotal or total ) and in 41 patients ( 49.4% ) partial tumor extirpation was performed . 
 chemotherapy was initiated within 8 days after surgery . in hungary , chemotherapy of children with medulloblastoma contains the following drugs : cyclophosphamide , ifosfamide , vincristine , cisplatin , carboplatin , etoposide , methotrexate , bcnu , and procarbazine . 
 the patients were divided into two groups , depending on whether radiotherapy was performed with head fixation and ct - based individual radiation treatment planning or not . head fixation and treatment planning were not in routine use between january 1 , 1986 and december 31 , 1994 . 
 initially , for boost radiation treatment planning , we obtained an image of the head circumference and projected the anatomic scheme onto the resultant contour for determination of the target volume . 
 the influence of various factors including age , sex , tumor location , extent , type of surgery , risk group , radiation dose to posterior fossa and spinal axis , and the effect of head fixation and ct - assisted radiation treatment planning on 5 - year relapse - free survival and 5 - year overall survival was investigated . 
overall survival ( months from diagnosis to last follow - up or death ) and relapse - free survival ( without progression or recurrence ) were calculated according to kaplan & meier [ 14 ]  . the survival curves were compared by the log - rank test . 
 in univariate cox regression analysis , metastatic disease ( p = 0.034 ) and the application of head fixation and individual radiation treatment planning ( p = 0.013 ) were found to significantly influence overall survival . 
the final model during multivariate cox regression analysis revealed metastatic disease ( p = 0.04 ) and the use of head fixation and individual radiation treatment planning ( p = 0.045 ) as independent prognostic factors for overall survival as endpoint ( table 2 )  . 
 figure 1 gives the overall survival curves for 59 patients receiving radiotherapy with head fixation and ct - based in - dividual radiation treatment planning and 24 patients without head fixation and with conventional radiation treatment planning . 
 no significant impact on overall survival was noted for the other categories ( age , sex , location , type of surgery , risk group , radiation dose )  . 
prognostic factors with 5 - year overall survival as endpoint ( p * : log - rank test ; p * * : univariate cox model ; p * * * : multivariate cox model )  . 
prognosefaktoren fr das 5 - jahres - gesamtberleben ( p * : log - rank - test ; p * * : univariates cox - modell ; p * * * : multivariates coxmodell )  . 
kaplan - meier survival curves demonstrating the influence of orfit head fixation and individual radiation treatment planning ( since 1995 ) on the overall survival rate in the study population . 
die kaplan - meier - berlebenskurven zeigen den einfluss der kopffixation und der individuellen bestrahlungsplanung ( seit 1995 ) auf die gesamtberlebensrate in der untersuchten population . prognostic factors for relapse - free survival are outlined in table 3 and similar to those predicting overall survival . 
 univariate cox regression analysis identified metastatic disease ( p = 0.028 ) as well as head fixation and individual radiation treatment planning ( p = 0.009 ) as having an impact on relapse - free survival . 
the final model of multivariate cox regression analysis identified metastatic disease ( p = 0.036 ) and the application of head fixation and individual radiation treatment planning ( p = 0.041 ) as independent prognostic factors for relapse - free survival as endpoint ( table 3 )  . figure 2 gives the relapse - free survival curves for 59 patients receiving radiotherapy with head fixation and ct - based individual radiation treatment planning and 24 patients without head fixation and with conventional radiation treatment planning . 
therefore , the usefulness of chemotherapy remained unknown . patients who received radiation doses > 50 gy to the posterior fossa , had a lower 5 - year relapse - free and overall table 3 . 
prognostic factors with 5 - year relapse - free survival as endpoint ( p * : log - rank test ; p * * : univariate cox model ; p * * * : multivariate cox model )  . 
prognosefaktoren fr das rezidivfreie 5 - jahres - berleben ( p * : log - rank - test ; p * * : univariates cox - modell ; p * * * : multivariates cox - modell )  . 
other causes of death were seen in three cases ( pneumonia , acute lymphoid leukemia as second primary , and a graft - versus - host reaction following bone marrow transplantation )  . 
zns : zentralnervensyste site of recurring tumor number of patients posterior fossa cerebrum spine entire cns distant metastasis total discussion in this study , we evaluated overall survival , relapse - free survival and prognostic factors in a group of patients with medulloblastoma diagnosed between 1986 and 2000 who were treated by surgery , chemotherapy and radiotherapy . 
a recent paper revealed excellent tumor control in medulloblastoma with acceptable acute toxicity and long - term survival up to 96% [ 17 ]  . the rate and the pattern of recurrences were similar to those observed by others [ 2 , 3 , 17 ]  . 
 according to current knowledge , the therapeutic results in medulloblastomas were favorably affected by the complex management in which radiotherapy played a determinant role [ 7 , 8 , 18 , 20 , 25 ]  . 
in medulloblastoma and other tumors , stereotactic irradiation techniques reveal an acceptable toxicity and promising results in tumor control in recurrent disease or as primary treatment [ 11 ]  . 
all this can be attributed to the fact that with the introduction of head fixation and ctbased individual radiation treatment planning the 20 - gy boost irradiation to the posterior fossa was applied in both risk groups with greater precision and reproduction of daily adjustments . 
the radiation dose to the posterior fossa , which has been reported to be a prognostic factor , is not correlated with 5 - year relapse - free and overall survival [ 3 , 17 ]  . 
patients who received radiation dose > 50 gy to the posterior fossa , had a lower survival rate than those who received 50 gy . despite careful analysis , we could not find the exact reason for this . 
 strahlentherapie und onkologie originalarbeit beurteilung der lebensqualitt von patienten mit plattenepithelkarzinomen der mundhhle vergleich von zwei behandlungsstrategien in einer prospektiven studie erste ergebnisse jrg wiltfang1 , gerhard grabenbauer2 , alexandra bloch - birkholz1 , anna leher3 , friedrich wilhelm neukam1 , peter keler1 hintergrund : das plattenepithelkarzinom der mundhhle gehrt zu den zehn hufigsten malignen tumoren des krpers . 
zur beurteilung der lebensqualitt wurden der quality of life core questionnaire ( qlq - c30 ) und das so genannte kopf - hals - modul ( h&n 35 ) der european organisation for research and treatment of cancer ( eortc ) herangezogen . 
 schlussfolgerung : es stellt sich die frage , ob die einschrnkung der lebensqualitt durch aggressive therapieformen gerechtfertigt werden kann oder ob dem funktionserhalt durch weniger radikale therapieoptionen der vorzug zu geben ist . 
 schlsselwrter : lebensqualitt plattenepithelkarzinom tumortherapie strahlenther onkol 2003 ; 179 : 6829 doi 10.1007 / s00066 - 003 - 1143 - 8 evaluation of quality of life of patients with oral squamous cell carcinoma . 
when considering long - term survival , there is substantial evidence that evidenced modality treatment including neoadjuvant rct is superior to the primary surgical approach with postoperative radiation . patients and methods : this longitudinal study prospectively evaluates quality of life in two groups consisting of 53 neoadjuvant and primarily surgically treated patients with oral cancer , using the quality - of - life core questionnaire ( qlq - c30 ) and the head and neck cancer module ( h&n 35 ) of the european organization for research and treatment of cancer ( eortc )  . 
 conclusion : temporary limitations in quality of life can be expected after tumor treatment of oral cancer as presented here . neoadjuvant therapy concept is more aggressive and might result in a longer disease - free survival , but the restriction in quality of life is more severe . 
 key words : quality of life oral squamous cell carcinoma tumor therapy hintergrund patienten und methoden der fortschritt in der mikrovaskulr - rekonstruktiven chirurgie erlaubt bei der behandlung von plattenepithelkarzinomen der mundhhle die radikale tumorresektion mit sofortiger defektrekonstruktion in einer sitzung . 
von diesen technischchirurgischen entwicklungen konnten die patienten jedoch nur begrenzt profitieren , da sich die 5 - jahres - berlebenswahrscheinlichkeit trotz dieser neuerungen nur unwesentlich verbessern lie [ 15 ]  . die einfhrung multimodaler , interdisziplinrer kombinationsbehandlungen sollte ein lngeres tumorfreies berleben von patienten mit plattenepithelkarzinomen der mundhhle ermglichen . 
erstere gilt als aggressiver , nebenwirkungsreicher und belastender , bietet jedoch eine hhere berlebenswahrscheinlichkeit als das eher konventionelle vorgehen mit postoperativer bestrahlung [ 1 , 2 , 5 , 7 , 1115 , 2224 , 27 ]  . 
 aus diesem grund , aber auch unter dem aspekt der wahl einer individuell angepassten therapie sollte der therapiebedingten beeinflussung der lebensqualitt whrend der behandlung und nach deren abschluss ein hoher stellenwert eingerumt werden . 
aus sicht des patienten knnte die frage , ein langfristiges berleben unter massiven einschrnkungen der lebensqualitt in kauf zu nehmen , durchaus anders beantwortet werden als aus rztlicher sicht alle in den letzten jahren wurde eine ganze reihe von fragebgen zur beurteilung der lebensqualitt von patienten mit plattenepithelkarzinomen des oberen aerodigestivtrakts entwickelt [ 810 , 12 , 20 , 21 , 24 ]  . 
lebensqualitt bei der behandlung von plattenepithelkarzinomen der mundhhle therapiebeginn resektion und rekonstruktion postoperative radiotherapie 3 monate 12 monate 24 monate qlq - c30 h&n 35 kombinierte radiochemotherapie als vorbehandlung qlq - c30 h&n 35 qlq - c30 h&n 35 abbildung 1 . 
therapieschema bei neoadjuvanter therapie ( grau unterlegtes feld ) sowie primr chirurgischer therapie ( dunkelgrau unterlegtes feld ) und postoperativer radiotherapie . ermittlung der lebensqualitt zum zeitpunkt vor sowie 3 , 12 und 24 monate nach behandlungsabschluss ( rct - / chirurgie - gruppe )  . 
therapeutic concepts for oral squamous cell carcinomas : combined radiochemotherapy as neoadjuvant therapy ( grey field ) before resection of the tumor or postoperative radiotherapy in an adjuvant approach ( dark grey field )  . 
das chirurgische konzept wurde auch bei den patienten angewendet , bei denen die neoadjuvante rct zu einer klinischen vollremission im ursprnglichen tumorbereich gefhrt hatte , da dieses ergebnis nur nach pathohistologischer untersuchung des resektats besttigt werden konnte . 
 bestimmung der lebensqualitt die lebensqualitt wurde ber den erhebungsbogen qlqc30 ( quality - of - life core questionnaire ) der eortc ( european organization for research and treatment of cancer ) tabelle 3 . 
 tumorstadium vor therapienach therapieaufteilung abschluss beginn nicht beurteilbar total gem therapieschema chir / rt rung fand nicht statt , da sich nur kardial und renal belastbare patienten der kombinierten rct unterziehen knnen . 
 gem der uicc - kriterien litten sechs patienten an plattenepithelkarzinomen im stadium i , 13 im stadium ii , 20 im stadium iii und 14 im stadium iv ( tabelle 3 )  . 
bei dieser gelegenheit wurde das tumortragende areal in einem sicherheitsabstand von 15 bis 20 mm um den sichtoder tastbaren tumorrand hinaus ttowiert und , falls erforderlich , nochmals eine gewebeprobe gewonnen . 
criteria for inclusion / exclusion in the neoadjuvant erlangen tumor therapy concept . primres , unvorbehandeltes plattenepithelkarzinom der mundhhle / oropharynx keine fernmetastasierung ( m0 ) gesamtprotein > 6 g / dl kreatininwert < 1 , 5 mg / dl kreatininclearance > 100 ml / min thrombozytenkonzentration > 100 000 / l leukozytenkonzentration > 4000 / l got , gpt , bilirubin nicht hher als doppelter normwert plasmaelektrolyte im normbereich keine kardiale , renale oder psychiatrische grunderkrankung keine drogenabhngigkeit kein kinderwunsch bei weiblichen patienten schriftliche einverstndniserklrung ausreichende mitarbeit strahlenther onkol 2003 no . 
da dieser fragebogen eher allgemeine aspekte der lebensqualitt berhrt , wurde zur erfragung spezifischer probleme der kopf - hals - region das head and neck module ( h&n35 ) herangezogen . 
radiochemotherapie / chirurgie ( rct - / chirurgie - gruppe ) im vergleich mit chirurgie / radiotherapie ( chirurgie / rt - gruppe )  . prtherapeutische beurteilung der lebensqualitt gem den eortcqlq - c30 - / h&n - 35 - fragebgen . 
in den tabellen werden neben den p - werten fr unterschiede zwischen den gruppen ( signifikanzniveau = 0 , 05 ) auch die mittelwerte und standardabweichungen der qlq - c30 - / h&n35 - bewertungsskalen dargestellt ( tabellen 4 bis 6 )  . 
 ergebnisse die gesamtzahl von 53 patienten konnte bis zu 3 monaten nach abschluss der therapie nachbeobachtet und befragt werden , immerhin 32 patienten bis zu 1 jahr nach abschluss der behandlung . 
in der bewertungsskala sank der angegebene mittelwert von etwa 85 punkten auf werte zwischen 70 und 75 punkten und dokumentierte so eine deutlich empfundene einschrnkung des gesundheitsgefhls und damit auch der lebensqualitt . dabei fiel in der neoadjuvant vorbehandelten gruppe ein strkeres absinken der punktzahl auf ( 86 auf 72 ) als in der primr chirurgisch behandelten patientengruppe ( 85 auf 76 )  . 1 jahr nach therapieabschluss waren diese werte in beiden strahlenther onkol 2003 no . 
sowohl der rckgang nach 3 monaten ( p = 0 , 038 ) als auch der wiederanstieg der werte nach 1 jahr ( p = 0 , 038 ) ergab signifikante unterschiede . 
verdeutlicht wird diese gravierende einschrnkung der lebensqualitt durch die unfhigkeit vieler patienten , in gesellschaft adquat nahrung aufzunehmen . die entsprechenden werte ( trouble social eating ) sanken in beiden gruppen von knapp 100 properativ auf 59 bzw . 
hier kam es nur in der neoadjuvanten gruppe zu einer erwhnenswerten erholung nach 1 jahr ( 81 punkte ) , whrend in der anderen patientengruppe der wert mit 59 punkten 1 jahr nach therapieabschluss nahezu unverndert blieb . 
 die funktionseinschrnkung bei der nahrungsaufnahme wird auch durch die reduktion der mundffnung sowie die probleme , die mit der strahlenbedingten xerostomie ( trockener mund , zhflieender schleim ) verbunden sind , dokumentiert . 
die beurteilung durch die patienten zeigte einen dramatischen abfall von prtherapeutischen werten um 95 auf werte zwischen 50 und 60 , die sich auch 1 jahr postoperativ nicht wesentlich erholt hatten . 
signifikante unterschiede zwischen den therapiegruppen waren 1 jahr nach therapieabschluss in bezug auf die mundffnung feststellbar ( p = 0 , 003 ) , wobei die mundffnung in der primr operierten patientengruppe 1 jahr postoperativ deutlich besser bewertet wurde ( 91 zu 75 )  . 
 ein allgemeines krankheitsgefhl war wiederum in der chirurgie - / rt - behandlungsgruppe deutlicher aufgetreten ( 56 ) als in der neoadjuvanten gruppe ( 61 ) und hatte sich nach 1 jahr bei diesen patienten auch nur unwesentlich erholt ( von 56 auf 62 punkte )  . 
vor allem in den ersten monaten nach therapieabschluss war in der beurteilung der allgemeinen lebensqualitt gem der eortckriterien ein deutliches absinken feststellbar [ 4 , 6 , 810 , 18 , 20 , 21 ]  . 
vor allem funktionelle einschrnkungen bei der nahrungsaufnahme , in der kontaktaufnahme zum sozialen umfeld und beim sprechen sind durch die aufwendigen mikrovaskulren rekonstruktionstechniken im bereich der mundhhle bedingt , die nach 1 jahr nur in wenigen fllen schon zu einer vollstndigen wiederherstellung der essentiellen funktionen von kauen , sprechen und schlucken fhren knnen [ 810 , 20 , 21 ]  . 
die hier befragte patientengruppe war hinsichtlich der tumorqualitt , tumorlokalisation und der krankenvorgeschichte ( nikotinund alkoholabusus ) einheitlich strukturiert , sodass messbare oder auch subjektiv empfundene unterschiede nicht zu tage traten . 
 anhand der verwendeten fragebgen war es in wesentlichen bereichen der beurteilung funktioneller parameter mglich , einflsse der neoadjuvanten vorbehandlung von auswirkungen der postoperativen bestrahlung zu unterscheiden . im vergleich beider behandlungskonzepte waren in bezug auf die allgemeine lebensqualitt sowie vor allem die funktion des kau - , sprechund schluckorgans relevante unterschiede feststellbar . 
 in der subjektiven beurteilung von lebensqualitt und krankheitsspezifischen problemen durch patienten mit plattenepithelkarzinomen der mundhhle berichteten schliephake & jamil [ 20 , 21 ] ber hnliche erfahrungen wie in der hier vorgestellten studie . 
 in der hier vorgelegten untersuchung schienen die patienten , die neoadjuvant vorbehandelt wurden , 3 monate nach abschluss der therapie in geringerem mae unter den folgen der therapie zu leiden als die , die primr operiert wurden . 
besonders im emotionalen bereich , in der sozialen integrationsfhigkeit und in den kognitiven funktionen wurden von den patienten der neoadjuvant vorbehandelten gruppe hhere punktwerte angegeben als von den primr operierten . nach 1 jahr hatten sich diese unterschiede zwischen den beiden behandlungsgruppen nahezu nivelliert [ 8 ]  . 
vor allem die strahleninduzierte mukositis , verbunden mit der in dieser bestrahlungsregion fast unvermeidlichen xerostomie , fhren zu einer strkeren einschrnkung von kau - , schluckund sprachfunktion als in der primr strahlenther onkol 2003 no . 
lebensqualitt bei der behandlung von plattenepithelkarzinomen der mundhhle chirurgisch versorgten patientengruppe [ 3 , 16 , 17 , 19 , 23 , 26 ]  . wundheilungsstrungen sind in dieser patientengruppe durch einen protrahierten verlauf gekennzeichnet . 
diese studie wird ber einen insgesamt 2 - jhrigen zeitraum fortgefhrt , da eine vollstndige oropharyngeale rehabilitation mit wiederherstellung der kaufunktion nach der primren tumorresektion mindestens 1 jahr in anspruch nimmt . 
hammerlid e , bjordal k , ahlner - elmqvist m , boysen m , evensen jf , bjorklund a , jannert m , kaasa s , sulivan m , westin t . 
a prospective , multicentric , randomised dosak study of advanced squamous cell carcinoma of the oral cavity and the oropharynx ( a 3 - year follow - up )  . 
10 urban & vogel strahlentherapie und onkologie originalarbeit strahleninduzierte mukositis und neutrophile granulozyten in der mundschleimhaut heinz schmidberger , margret rave - frnk , solan kim , andrea hille , olivier pradier , clemens f . 
 patienten und methoden : bei zehn patienten mit tumoren der kopf - hals - region , die sich einer strahlentherapie unterzogen , wurde die anzahl enoraler neutrophiler granulozyten in der mundsplflssigkeit im verlauf einer radiotherapie oder einer radiochemotherapie ( 5 - fu , mitomycin ) untersucht . 
die patienten / probanden splten den rachenraum 30 s mit 15 ml steriler physiologischer nacl - lsung . das sputum wurde zentrifugiert , mit 2 g / ml akridin - orange in 1 ml rpmi resuspendiert und anschlieend 15 min bei 37 c inkubiert . 
 schlsselwrter : strahleninduzierte mukositis neutrophile granulozyten nebenwirkungen strahlenther onkol 2003 ; 179 : 66772 doi 10.1007 / s00066 - 003 - 1121 - 1 radiation - induced mucositis and neutrophil granulocytes in oral mucosa background : chemotherapy - induced mucositis can be related to a decrease in oral neutrophils . 
 die chemotherapieinduzierte mukositis kann neben einer abnahme der leukozytenanzahl im blut auch mit einer verarmung der mundschleimhaut an funktionsfhigen neutrophilen granulozyten vergesellschaftet sein und durch diese verarmung negativ beeinflusst werden [ 11 , 16 ]  . 
 die vorliegende arbeit sollte die hypothese prfen , ob es durch ionisierende strahlen zu einer abnahme der neutrophilen granulozyten in der mundschleimhaut kommt und ob dieses phnomen mit dem grad der radiogenen mukositis korreliert . 
ferner sollte untersucht werden , ob die zahl der neutrophilen granulozyten in der mundsplflssigkeit einen geeigneten parameter darstellt , um die graduierung der radiogenen mukositis zu verfeinern , oder ob dieser parameter als surrogat fr die quantifizierung einer mukositis in klinischen studien herangezogen werden knnte . 
 patienten und methoden insgesamt wurden 15 patienten , die wegen einer tumorerkrankung im kopfund halsbereich eine strahlentherapie ( sieben mnnlich , eine weiblich ) oder eine kombinierte strahlenund chemotherapie ( sieben mnnlich ) erhielten , in die studie einbezogen . 
patienten mit kombinierter radiochemotherapie erhielten 5 - fu ( 600 mg / m2 ) an den ersten 5 tagen und mitomycin ( 10 mg / m2 ) an den tagen 1 und 36 der strahlentherapie . 
jeweils zwei eckquadrate einer zhlkammer , entsprechend einem volumen von je 0 , 1 mm3 , wurden bei einem vergrerungsfaktor von 160 an einem zeiss - 14 - fluoreszenz - mikroskop ausgezhlt . 
angewendet wurden der t - test fr nicht verbundene daten mit ungleicher varianz und der u - test von mann - whitney , der fr nicht normalverteilte daten geeignet und gegen ausreier unempfindlich ist . 
 ergebnisse insgesamt wurden 15 patienten in die studie aufgenommen . zwei patienten mussten wegen mangelnder kooperation bei der regelmigen mundsplung aus der studie ausgeschlossen werden , zwei weitere patienten brachen die strahlentherapie auf eigenen wunsch ab und ein patient musste wegen einer interkurrenten erkrankung die therapie unterbrechen . letztlich waren zehn patienten mit ihren detaillierten daten auswertbar . 
alle patienten , die zumindest eine grad - ii - mukositis , und auch die patientin , die nur eine grad - i - mukositis entwickelte , zeigten dieses muster . 
 zuund abnahme der neutrophilen granulozyten im zeitlichen verlauf und bezogen auf den grad der klinisch klassifizierten mukositis fr die anzahl der neutrophilen granulozyten in der mundsplflssigkeit wurden zudem groe interindividuelle unterschiede festgestellt . 
 patient alter gechlecht primrtumor ( jahre ) ( w / m ) tnm klassifikation strahlenmukositis neutrophile chemo therapie dosis ( ja / nein ) [ gy ] granulozyten vor therapie / max . 
wert ( grad ) unterlippenkarzinom tonsillenkarzinom oropharynxkarzinom mundhhlenkarzinom larynxkarzinom oropharynxkarzinom hypopharynxkarzinom larynxkarzinom zungenrandund oropharynxkarzinom t4 n2b g2 ausgedehntes oropharynxkarzinom pt4 pn0 m0 g2 nein pt2 pn0 m0 g2 nein t2 n0 m0 g2 nein t0 pn2b m0 g2 nein nein t3 n0 m0 nein t4 n2c m1 g2 t4 n3 m0 g2 t4 n2c m0 g2 t4 n2 mx g2 100 400 5 133 3 067 104 133 87 800 4 117 4 408 82 688 108 000 1 539 563 110 067 17 825 182 083 522 025 893 200 2 270 833 28 942 5 662 833 7 512 941 strahlenther onkol 2003 no . 
strahleninduzierte mukositis und neutrophile 100 000 80 000 60 000 40 000 20 000 10 000 6 000 000 5 000 000 4 000 000 3 000 000 2 000 000 1 000 000 1000 dosis ( gy ) dosis ( gy ) abbildung 1a figure 1a abbildung 1b figure 1b abbildungen 1a und 1b . 
the right curve is representative for two patients with grade i mucositis ( b )  . aufgefhrt , die unterschiede sind tendenziell noch hher , liegen aber im gleichen grenordnungsbereich . 
bei alleiniger strahlentherapie wurde der maximale anstieg zu beginn der dritten therapiewoche ( nach zwlf fraktionen ) erreicht , danach fielen die werte wieder ab und erreichten zum therapieende den ausgangswert . 
 patienten rt + ct patienten nur rt gesunde spender diskussion validitt der eingesetzten methode neutrophile granulozyten bilden einen wichtigen bestandteil der schleimhautbarriere gegen mikrobielle infektionen . ein nachlassen der produktion oder des turnovers von neutrophilen granulozyten kann mit einem erhhten infektionsrisiko verbunden se in der vorliegenden arbeit wurde eine von wright et al . 
healthy volunteers show constant counts ( closed circles ) ; after radiotherapy maximal counts are found after twelve fractions ( open squares ) ; after chemoirradiation , maximal counts occur after 14 fractions ( closed triangles )  . 
trotz der groen variabilitt der messwerte deutet sich ein verlaufsmuster an , das durch eine jeweilige zunahme der anzahl der neutrophilen granulozyten bei beginnender oder zunehmender mukositis und eine ( leichte ) abnahme bei abheilender mukositis gekennzeichnet ist . 
tendenziell lie sich ein zusammenhang zwischen dem ausma der radiogenen mukositis und der anzahl der neutrophilen granulozyten in der mundsplflssigkeit dahingehend feststellen , dass mit zunehmender mukositis die anzahl der neutrophilen granulozyten zunah dieser anstieg ist jedoch durch unregelmige schwankungen und groe standardabweichungen gekennzeichnet . 
 die eingangs formulierte hypothese , dass eine verarmung der mundschleimhaut an neutrophilen granulozyten einer der mechanismen der radiogenen mukositis sein knnte , wird durch diese beobachtung dennoch widerlegt , da es im zuge der ausbildung einer radiogenen mukositis stets zu einer zunahme und nie zu einer abnahme der gezhlten neutrophilen granulozyten in der mundsplflssigkeit ka eine leukozyteninfiltration der mukosa und der submukosa zum ende der zweiten bestrahlungswoche , also beim bergang vom erythem zu einer fokalen mukositis , wurde auch von drr et al . 
rttinger1 , detlef bartkowiak1 , donald bunjes2 , roman wennauer3 , dagmar dohr1 purpose : total body irradiation ( tbi ) with and without additional radioimmunotherapy ( rit ) was examined for renal toxicity after stem cell transplantation . 
 patients and methods : serum creatinine levels of 35 patients ( 15 female , 20 male , median age 40.5 years , range 1760 years ) after tbi alone and of 23 patients ( eight female , 15 male , median age 47 , range 1658 years ) after tbi with additional rit were determined between 10 / 1997 and 11 / 1999 . 
tbi was performed by external - beam radiotherapy in six fractions over 3 days with renal doses of 12 gy in the tbi - alone group and 6 gy in the group with additional rit . 
in the absence of a positive dose - response relationship for the 188re - labeled antibody , the observation may be explained by an underestimation of the biologically effective dose and the inaccuracy of the dose determination at the glomerular level . key words : renal toxicity total body irradiation radioimmunotherapy strahlenther onkol 2003 ; 179 : 7027 doi 10.1007 / s00066 - 003 - 1090 - 4 erhhte nephrotoxizitt bei ganzkrperbestrahlung und zustzlicher radioimmuntherapie ziel : bestimmung der nephrotoxizitt bei ganzkrperbestrahlung ( gkb ) mit und ohne radioimmuntherapie ( rit )  . 
 patienten und methodik : zwischen 10 / 1997 und 11 / 1999 wurden die serumkreatininwerte von 35 patienten ( 15 weiblich , 20 mnnlich , alter 1760 jahre , median 40 , 5 jahre ) nach alleiniger gkb bzw . 
 ergebnisse : innerhalb von 12 monaten nach behandlung erhhten sich die kreatininwerte von 77 mmol / l ( sd 11 ) auf 89 mmol / l ( sd 20 ) bei alleiniger gkb und von 78 mmol / l ( sd 13 ) auf 144 mmol / l ( sd 52 ) bei kombinierter gkb / rit . 
10 gbq 188re - markierten monoklonalen cd66 - antikrpern mit einer kalkulierten nierendosis von 8 , 3 gy ( 2 , 311 , 6 gy ) eine erhhte nierentoxizitt , wie bereits frher beobachtet . 
bei fehlender dosis - wirkungs - beziehung zum 188re - markierten antikrper knnte die beobachtung mit einer unterschtzung der biologisch effektiven dosis und einer unzureichenden dosisermittlung an den glomeruli erklrt werden . 
renal toxicity of tbi with additional rit introduction total body irradiation ( tbi ) with its cytotoxic and immunosuppressive effect is well established for conditioning leukemia patients for bone marrow transplantation ( bmt ) [ 1 , 2 , 13 ]  . 
besides acute side effect [ 10 ] , severe consequences such as pulmonary dysfunction [ 15 ] and renal toxicity [ 4 , 7 , 10 ] have to be considered . 
 renal dysfunction has been observed to develop at a median of 9 months following tbi and is characterized by an increase of serum creatinine , caused by a glomerular filtration rate < 50% , proteinuria , anemia , and hypertension [ 5 , 16 ]  . 
 in an attempt to deliver radiation selectively to the bone marrow with radiolabeled antibodies [ 12 ] , patients with a high risk of relapse ( acute myelogenous leukemia [ aml ] beyond first complete remission [ cr ] , aml in first cr with high - risk cytogenetic features , poor response to primary induction chemotherapy , high - risk myelodysplastic syndrome [ mds ] , acute lymphoblastic leukemia [ all ; ph + ] in first cr , chronic myelocytic leukemia [ cml ] beyond first chronic phase ) received additional radioimmunotherapy ( rit ) with 188re - labeled anti - cd66 monoclonal antibody . 
previously , a 14% incidence of radiation nephropathy in rit patients with high - risk aml / mds has been observed [ 3 ]  . the present study is focused on the time course of renal toxicity developing in patients after tbi with and without prior rit . 
in 23 patients ( eight female , 15 male , median age 47 years [ 1658 years ] ) , an additional rit was performed ( table 1 )  . 
serum creatinine levels were determined before , 3 , 6 , 9 , and 12 months after transplantation . prior to therapy , all patients had normal serum creatinine values ( table 2 )  . 
188re - labeled anti - cd66 mouse monoclonal antibody in various fraction numbers and fraction sizes , depending on the output of the re generator ( table 4 )  . 
renal toxicity of tbi with additional rit nephrotoxic agents all patients had prophylactic antiviral drugs ( acyclovir 3 ( cid : 1 ) 5 mg / kg body weight daily day 1 until + 7 )  . 
the mean incorporated dose was 2 , 019 mg ( 2 , 140 ) for patients without rit and 1 , 648 mg ( 1 , 381 ) for patients with rit . 
increased serum creatinine levels occurred in three of 35 patients with tbi alone and in 16 of 23 patients with tbi / rit ( tables 2 and 4 )  . 
the elevated values within the observation period were 124 mmol / l , 140 mmol / l , and 148 mmol / l in three patients with tbi alone , and ranged between 119 mmol / l and 296 mmol / l ( median 154 mmol / l ) in 16 patients with tbi / rit . 
renal toxicity of tbi with additional rit the patients with radiation nephropathy syndrome progressed to end - stage renal disease within the minimal observation period of 2 years since rit [ 3 ]  . 
 discussion the combination of tbi and rit was designed to escalate bone marrow and spleen doses while limiting non - target organ toxicity [ 3 , 12 , 18 ]  . 
 antibodies in rit patients , renal failure occurred irrespective of the applied dose , which was estimated to average 7.25 gy ( range 2.311.6 gy ) in the 16 patients , who developed pathologic serum creatinine levels , and 9.4 gy ( range 5.210.0 gy ) in the seven patients with maintained normal values . 
patients who demonstrated unspecific antibody binding to non - target tissues such as liver , kidneys , heart or lungs , exceeding specific binding to the bone marrow , were excluded from the study . 
thus , cross - reactivity of the antibody is an unlikely reason for the observed renal toxicity . rhenium conjugate during the injection of 188re - labeled anti - cd66 , glomeruli are exposed to peak doses . 
there is an increased protein concentration in the vessels leaving the glomeruli , before most of the fluid filtered in the glomeruli is reabsorbed into the blood [ 17 ]  . 
thus , immediately after 188re application , when dose deposition in the kidney should be limited to the vascular bed and its immediate surrounding , a focal accumulation of dose within and around the glomeruli has to be expected . 
a further uneven dose distribution may result from the spherical glomerular architecture and the short range of ( cid : 1 ) - particles , such that intraand periglomerular doses may rise in a cubic manner . 
serumkreatininverlauf ( mit standardabweichung ) nach gkb ( 35 patienten ) und gkb / rit ( 23 patienten )  . was not taken into account by the dosimetric procedures in this study . 
deposition in the whole nephrons should occur with further degradation of the protein and liberation of the nuclide [ 20 ]  . this includes a 30% loss of activity from the bone marrow during the first 40 h , which is retrieved in the urine at a rate of 1% of the initial activity per hour [ 18 ]  . 
 dosimetry a potential underestimation of the dose contribution to the whole kidney by an unproportional low background in the bowel appears as an additional , although minor source of error due to the two - dimensional determination of the activity by a.p. 
 strahlentherapie und onkologie current discussion can the addition of regional radiotherapy counterbalance important risk factors in breast cancer patients with extracapsular invasion of axillary lymphnode metastases ? gnther gruber1 , gilles berclaz2 , hans - jrg altermatt3 , richard h . 
 patients and methods : from 08 / 1988 to 06 / 1998 , 81 patients with extranodal invasion were treated with adjuvant rt ( median total dose : 50.4 gy ) , 46 / 81 only locally , 35 / 81 locoregionally due to presumed adverse parameters . 
despite their overrepresentation in the locoregional rt group , no difference was found between both groups in regard to disease - free survival ( dfs ; p = 0.83 ) and overall survival ( os ; p = 0.56 ) , suggesting that regional rt was able to counterbalance the increased risk . 
there was even a trend toward a better 3 - year dfs , 61% in locoregional rt and 37% in local rt , in the subgroup of patients with four or more positive lymph nodes . 
 key words : treatment volume extranodal extracapsular pattern of failure strahlenther onkol 2003 ; 179 : 6616 doi 10.1007 / s00066 - 003 - 1084 - 2 kann die zustzliche regionre bestrahlung risikofaktoren bei nodal positiven mammakarzinompatientinnen mit extranodalem wachstum ausgleichen ? ziel : evaluation einer nderung des rckfallmusters durch eine lokoregionre bestrahlung ( rt ) im vergleich zur rein lokalen rt bei patientinnen mit extranodalem wachstu patienten und methodik : von 08 / 1988 bis 06 / 1998 wurden 81 nodal positive patientinnen mit extranodalem wachstum adjuvant bestrahlt ( mediane gesamtdosis : 50 , 4 gy ) , 46 nur lokal , 35 zustzlich regionr aufgrund von risikokriterien . 
trotz deren berreprsentation in der lokoregionren bestrahlungsgruppe konnte kein unterschied zu nur lokal behandelten patientinnen gefunden werden ( krankheitsfreies berleben [ dfs ] : p = 0 , 83 ; gesamtberleben [ os ] : p = 0 , 56 ; abbildungen 1 und 2 )  . 
in der untergruppe mit vier oder mehr positiven lymphknoten betrug das 3 - jahres - dfs sogar 61% in der lokoregionren gruppe versus 37% in der gruppe mit lokaler rt ( abbildung 3 )  . 
multivariat blieben t3 / t4 - tumoren , vier oder mehr positive lymphknoten und lvi signifikant , fr das dfs und fernmetastasenfreie berleben ( dmfs ) zustzlich fehlende strogenrezeptoren und die abwesenheit der regionren bestrahlung ( tabelle 4 )  . 1 department of radiation oncology and 2 department of gynecology , inselspital , university of bern , switzerland , 3 institute of pathology , bern , switzerland . 
locoregional rt in breast cancer patients with extracapsular invasion schlussfolgerung : im vergleich zur nur lokalen rt scheint eine zustzliche regionre rt bedeutende risikofaktoren bei patientinnen mit extranodalem wachstum auszugleichen . schlsselwrter : bestrahlungsvolumen extranodal extrakapsulr rckfallmuster introduction extracapsular invasion of lymph node metastases is well known as predictive and prognostic factor in many malignant solid tumors and demands additive irradiation . 
 in spite of overwhelming data concerning the status of axillary lymph nodes in breast cancer , there are only few publications with retrospective data which discuss the prognostic and therapeutic impact in case of extracapsular invasion of axillary lymph node metastases [ 5 , 7 , 1517 ]  . 
in retrospective analyses of randomized patients , extracapsular invasion has been presumed to be a key factor for the difference in overall survival ( os ) between irradiated and unirradiated patients [ 20 , 25 ]  . 
randomized trials have revived the opinion that better locoregional control may decrease the risk of secondary dissemination and improve os [ 2022 , 24 ] , provided that the primary metastasization rate is low [ 12 ]  . 
 patients and methods between 08 / 1988 and 06 / 1998 , 81 node - positive breast cancer patients with a median age of 57 years ( mean : 56 years , range : 2687 years ) were treated . 
the median number of resected lymph nodes was 15 ( mean : 17 , range : six to 37 ) , of which a median of five ( mean : seven , range : one to 27 ) were positive . 
 staging routinely included chest x - rays , blood tests , liver ultrasounds , bone scans , and , in several cases , computed tomographies ( ct ) of the thorax . 
the chemotherapeutic regimens used were ac ( a : adriamycin or epirubicin , c : cyclophosphamide ) in 13 , cmf ( m : methotrexate , f : 5 - fluorouracil [ 5 - fu ] ) in 18 , and ac / cmf in 31 cases . 
cmfvp ( v : vincristine , p : prednisone ) , ac / tc ( t : docetaxel or paclitaxel ) , and ta / cmf were given once each , fac in four patients . after definition of the clinical target volume ( ctv ) , treatment fields were planned three - dimensionally . 
locoregional rt in breast cancer patients with extracapsular invasion diotherapy ( rt ) also for the ipsilateral subclavian region , the infraclavicular chest wall , and level iii of the axilla . 
the method of kaplan - meier was used for the estimation of survival times , and the log - rank test for univariate analyses of various parameters as to disease - free survival ( dfs ) , distant metastasis - free survival ( dmfs ) , and os . 
 after 5 years , 65% ( 10% ) of the locoregional rt group versus 44% ( 13% ) of the group of patients with local rt were disease - free . 
 as to the number of four or more metastatic lymph nodes , the 3 - year dfs was 61% ( 10% ) in locoregionally treated patients versus 37% ( 12% ) in patients with local rt ( figure 3 )  . 
 for prognostic parameters , the log - rank test was used . despite the significant imbalance of the three most important factors , i.e. , number of positive nodes , t - stage and lvi ( tables 1 and 3 ) , locoregional rt counterbalanced these risk factors in terms of dfs and os . 
the dfs and dmfs rates were significantly influenced by the number of positive nodes , higher t - stage , lvi , and estrogen receptor negativity ( table 3 )  . 
 the frequency of isolated local or regional recurrences as well as the total number of locoregional recurrences with distant metastases were similar in the group of patients with more advanced tumors and additional regional therapy versus the group of patients with less advanced tumors but only local irradiation . 
 one isolated local failure occurred in the 35 patients with locoregional rt ( 2.9% ) and none in the local rt group . there was no isolated regional recurrence in the locoregional rt group . 
this may explain the large differences of extracapsular invasion rates in the literature . most series revealed extracapsular invasion rates in the range of 2450% [ 5 , 7 , 9 , 11 , 14 , 16 , 17 , 23 , 25 , 29 ]  . 
 [ 28 ] reported on 539 patients whose 3 , 259 metastatic axillary nodes were investigated prospectively and very carefully : 1 , 957 ( 60% ) showed an extracapsular invasion . 
95% ci : 95% confidence interval ; er : estrogen receptor ; lvi : lymphatic vessel invasion ; pr : progesteron receptor ; rr : relative risk ; rt : radiotherapy . 
 parameter dfs ( 95% ci ) dmfs ( 95% ci ) ( 95% ci ) first reports which found a correlation of extracapsular invasion with decreased survival were published in 1976 / 1977 [ 8 , 18 ]  . 
 [ 5 ] reported similar numbers , with extracapsular invasion in 77.5% of patients with four to seven positive lymph nodes , and 92% of patients with more than seven positive lymph nodes . 
in axillary lymph nodes with a diameter > 2 cm , the same authors found extracapsular invasion in 84.2%. it seems quite understandable that the frequency of extracapsular invasion goes parallel to the number of involved lymph nodes [ 11 , 29 ] : the higher their number the more extracapsular invasion may lose its presumed independent prognostic character toward the higher number of positive lymph nodes . 
if extracapsular invasion in a small number of positive lymph nodes becomes an independent prognostic factor , it is allowed to suggest that the number of involved nodes loses its independence at all against the parameter of the finding of extranodal invasion . 
 [ 14 ] have revealed extracapsular invasion ( hazard ratio : 1.93 ; p = 0.05 ) and pt - stage to be independent risk factors in 353 patients with involved nodes . 
few publications [ 5 , 9 , 11 , 17 , 23 , 29 ] mentioned patients with extracapsular invasion treated with local or locoregional rt , but only two retrospective studies [ 5 , 17 ] compared the results of irradiated against unirradiated patients with extranodal invasion of their involved axillary lymph nodes . 
the selection criteria for additional irradiation in both studies were not specified and , therefore , we presume the aggressiveness of the tumor as selection bias for the postoperative rt to be comparable to the treatment decisions in our study . 
a recent update of the danish trials showed a 14 - year os of 35% with rt versus 22% without rt in the case of lymph node capsule invasion ( p < 0.0001 ; relative gain 37% ) [ 20 ]  . 
the effect of rt on distant metastases and better os was reported by other authors even in very high - risk patients with ten or more positive nodes [ 14 , 13 ]  . 
chest wall and subclavian region are the most common sites of locoregional failure , whereas a relapse on level i / ii of the axilla is uncommon ( reviewed in [ 27 ] )  . 
locoregional rt in breast cancer patients with extracapsular invasion of unnecessarily big supraclavicular and lower neck volumes . in analogy to the nomenclature of other regional lymph nodes areas like axilla or mammaria interna , we omit the term supraclavicular in favor of the term subclavia . 
the main difference in comparison to a widely used supraclavicular field ( figure in [ 23 ] ) is the upper field border , which can be reduced to the upper part of the costovertebral joint of the first rib ( as bony landmark on the simulation film )  . 
 according to a consensus statement on postmastectomy rt [ 10 ] , the chest wall should be treated in all patients , and the inclusion of the axillary apex and subclavian area is appropriate for selected node - positive cases , particularly those with four or more positive nodes . 
 we see the finding of extranodal invasion in involved axillary nodes at least of similar importance as the finding of more than three involved nodes and recommend the same treatment volume for these patients , namely chest wall and subclavian area , as for patients with more than three lymph node metastases . 
grabenbauer1 background : to evaluate retrospectively long - term results and patterns of recurrence in patients with low - grade non - hodgkins lymphoma ( nhl ) ann arbor stage iii and limited stage iii . patients and methods : 58 patients , who had been treated between 1980 and 1996 , were analyzed . 
end points of the investigation were remission rate , overalland disease - free survival , and patterns of recurrence , as well as the prognostic impact of age , b - symptoms , chemotherapy , irradiation dose , treatment volume , and ann arbor stage . results : 6 weeks after treatment 91% of the patients had complete , 7% partial response . 
regarding overall survival , multivariate analysis identified age ( p = 0.001 ) as independent prognostic factor . in the subgroup of patients with follicular lymphoma 92% were found in complete , 6% in partial remission , one patient ( 2% ) with progressive disease . 
out - of - field recurrence rate for all 58 patients was 34% and the proportion of relapses at nodal or lymphatic sites outside the treated areas in relation to all registered recurrences was 77% . 
 key words : low - grade non - hodgkins lymphoma radiotherapy age strahlenther onkol 2003 ; 179 : 694701 doi 10.1007 / s00066 - 003 - 1062 - 8 strahlentherapie bei niedrigmalignen , nodalen non - hodgkin - lymphomen im stadium iiii hintergrund : retrospektive auswertung der langzeitergebnisse und rezidivmuster bei patienten mit niedrigmalignem nonhodgkin - lymphom ( nhl ) stadium iii und lokal begrenzt stadium iii . patienten und methode : 58 patienten , die zwischen 1980 und 1996 behandelt wurden , wurden ausgewertet . 
untersucht wurden remissionsverhalten , gesamtund krankheitsfreies berleben und rezidivmuster sowie der prognostische einfluss der faktoren alter , b - symptomatik , chemotherapie , strahlendosis am tumor , zielvolumen und stadium nach ann arbor . ergebnisse : 6 wochen nach der strahlentherapie zeigten 91% der patienten eine komplette , 7% eine partielle remission . 
 1 department of radiation oncology , 2 department of hematology and oncology , and 3 institute of pathology , university of erlangen , germany . received : june 17 , 2002 ; accepted august 15 , 2002 strahlenther onkol 2003 no . 
radiotherapy for nodal low - grade non - hodgkins lymphoma schlussfolgerungen : die ergebnisse dieser retrospektiven analyse besttigen die radiotherapie als kuratives konzept in der behandlung niedrigmaligner nhls im frhen stadium insbesondere bei jngeren patienten . 
die rezidivanalyse gibt hinweise , dass die total nodale bestrahlung fr diese patienten als therapiestandard sinnvoll wre . schlsselwrter : niedrigmalignes non - hodgkin - lymphom radiotherapie alter was usually given with two parallel opposed fields . 
total dose at the tumor site ranged between 26 gy and 50 gy ( median 40 gy )  . chemotherapy was additionally given to 13 patients ( 22% )  . 
six patients ( 46% ) of them presented in clinical stage iiia , three ( 23% ) in stage iib , two ( 15% ) in stage iia , and one patient ( 8% ) in stage ib and ia , respectively . 
although localized presentations are uncommon in nhls , the goal of treatment should be cure in those who are shown to have truly localized disease after undergoing appropriate staging procedures . 
open questions are : how extensive or how limited should irradiation be ? what is the exact dose of radiotherapy needed for control or for cure ? are there prognostic tumor or treatment factors that allow to predict the quality of remission , survival outcome or the risk for recurrence in different subgroups ? the purpose of this study was to analyze retrospectively results after radiotherapy for stage iiii low - grade lymphomas , to learn about the long - term effectiveness of radiotherapy in this setting and to elucidate ways to improve the therapeutic ratio . 
 patients and methods between 1980 and 1996 , a total of 58 patients with ann arbor [ 39 , 49 ] stage iiii low - grade nhls were treated at the university of erlangen , department of radiation oncology . 
27 patients ( 47% ) presented in clinical ann arbor stage i , 21 ( 36% ) and ten ( 17% ) in stage ii and limited iii , respectively . 48 patients ( 83% ) were histologically classified as follicular nhls ( who classification [ 25 , 35 ] )  . 
78% of the patients underwent radiotherapy alone ( n = 45 ) , 13 patients ( 22% ) received additional chemotherapy . patients age ranged from 23 to 78 years ( median age : 51 )  . 
involved - field irradiation , in which the radiotherapy fields were limited to the involved nodal region only , was administered to 14 ( 24% ) of the 58 patients . 
28 patients ( 48% ) received extended - field radiotherapy , 13 ( 22% ) and three ( 5% ) patients received total nodal irradiation ( tni ) or total lymphatic irradiation ( tli ) , respectively . 
radiotherapy characteristic all patients gender female male age ( median : 51 ) 2029 3039 4049 5059 6069 7079 b - symptoms who classification follicular ( stage iiii ) follicular ( only stage i - ii ) low gradea mantle cell lymphoplasmacytic ann arbor stage chemotherapy radiotherapy dose ( median : 40 gy ) median > median target volume involved - field irradiation extended - field irradiation total nodal irradiation total lymphatic irradiation anot otherwise classified patients n ( % ) 58 ( 100 ) 21 ( 36 ) 37 ( 64 ) 5 ( 9 ) 7 ( 12 ) 14 ( 24 ) 15 ( 26 ) 9 ( 16 ) 8 ( 14 ) 6 ( 10 ) 52 ( 90 ) 48 ( 80 ) 38 ( 63 ) 4 ( 7 ) 3 ( 5 ) 3 ( 5 ) 28 ( 48 ) 20 ( 34 ) 10 ( 17 ) 45 ( 78 ) 13 ( 22 ) 34 ( 59 ) 24 ( 41 ) 14 ( 24 ) 28 ( 48 ) 13 ( 22 ) 3 ( 5 ) strahlenther onkol 2003 no . 
radiotherapy for nodal low - grade non - hodgkins lymphoma ferent chemotherapy regimes ( abvd , ceop , chop , cop , copp , mopp , vipe ) were administered in two up to eight cycles ( median six cycles )  . 
partial remission was classified with tumor volume reduction more than 50% . kaplan - meier analysis [ 27 ] was performed to determine tumor control - , disease - free survival and overall survival rates . curves were compared using the log - rank test [ 32 ]  . 
age was the only factor that reached significance , while b - symptoms , use of chemotherapy , radiotherapy dose , target volume , and clinical ann arbor stage did not have any significant impact on lymphoma control . 
considering stage iii follicular lymphoma patients only , 35 out of 38 ( 92% ) showed a complete , three ( 8% ) a partial remission . survival overall survival for all patients with low - grade nhl was 86% and 69% at 5 and 10 years , respectively ( figure 1 )  . 
age ( p = 0.001 ) , total radiotherapy dose ( p = 0.01 ) and b - symptoms ( p = 0.01 ) also influenced disease - free survival , while other variables showed no significant impact . disease - free survival rates for the 38 patients with stage iii follicular nhl were 81% and 67% at 5 and 10 years , respectively . patterns of recurrence 53 of all enclosed patients with lowgrade nhl reached complete response 6 weeks after radiotherapy . 
radiotherapy for nodal low - grade non - hodgkins lymphoma seven patients who relapsed within the irradiation fields received a median total dose of 40 gy ( range : 3050 gy )  . 
in this retrospective analysis no correlation between dose at tumor site and recurrence rate ( p = n.s. ) could be shown ( table 4 )  . age , b - symptoms , target volume and ann arbor stage also showed no significant impact on recurrence rates . among the 44 patients with follicular lymphoma that reached complete remission 18 developed a relapse . 
rezidivmuster in abhngigkeit von bestrahlungsvolumen und - dosis . site of first relapse field in and out out of field of field n ( % ) 58 ( 100 ) 6 ( 10 ) 1 ( 2 ) total 3 ( 5 ) 14 ( 24 ) involved - field radiotherapy 1 ( 2 ) 28 ( 48 ) extended - field radiotherapy 2 ( 3 ) total nodal irradiation ( tni ) 13 ( 22 ) total lymphatic irradiation ( tli ) 3 ( 5 ) 40 gy 40 gy median rt - dose at tumor site 1 ( 2 ) 50 gy 16 ( 28 ) 2 ( 3 ) 11 ( 19 ) 1 ( 2 ) 2 ( 3 ) 40 gy analyzed prognostic variables showed an independent significant influence on recurrence rate or location of relapse . 
 discussion after a median follow - up period of 8.75 years overall survival rates for all 58 patients were 86% and 69% 5 and 10 years after radiotherapy , respectively . 
compared to that , our results are less favorable , but again it has to be remarked that the cited studies only included patients with clinical stage i or iii disease . among the analyzed prognostic factors only age ( p = 0.001 ) could demonstrate independent and significant predictive power . 
berlebensraten bei niedrigmalignem nhl in der literatur und eigene ergebnisse . study group patients ann arbor stage overall survival ( % ) at 10 years 5 years disease - free survival ( % ) at 5 years 10 years mclaughlin et al . 
radiotherapy for nodal low - grade non - hodgkins lymphoma this correlation is well known and has been described in literature before [ 5 , 15 , 16 , 21 , 26 , 31 , 37 , 40 , 43 , 45 , 47 , 48 , 51 ]  . 
during long - term followup they found three in - field recurrences ( 5% ) , which led them to recommend a total dose of 35 gy in 20 fractions over four weeks . 
based on our results with recurrences appearing mainly outside the extended field volume we would rather recommend total nodal irradiation ( tni ) as an appropriate approach for early - stage nonhodgkins lymphoma . 
on the basis of these results they recommended total radiotherapy doses of 2025 gy for small volume low - grade orbital lymphomas , 30 gy for the adjuvant situation and a minimal tumor dose of 40 gy for macroscopic or bulky disease . 
they found a dose - effect - relationship for local control with a relapse rate of 31% after 2634 gy and 4% after 36 gy ; no relapses occurred after a total dose of 40 gy or more . 
 in our study we identified seven patients with in - field relapses ( 12% ) with a median total radiotherapy dose of 40 gy . in comparison to the mentioned studies this seems to be relatively high , but this may partly result from differing patient selection criteria . 
 in summary , for smaller tumors ( < 3 cm ) a total dose of 2530 gy can lead to an adequate local control , especially for lymphomas located in the orbita [ 26 ]  . 
in the adjuvant situation a minimal dose of 30 gy is recommended , in case of macroscopic disease a minimum dose of 40 gy should lead to acceptable local control rates . 
among these patients ( n = 28 ) 43% developed recurrence outside the original radiotherapy field , whereas out - of - field recurrence rates after involved - field irradiation ( n = 14 ) and total nodal irradiation ( n = 13 ) were much lower with 21% and 8% , respectively . 
out - of - field recurrence rate for all 58 patients was 29% and the proportion of relapses at nodal or lymphatic sites outside the treated areas in relation to all registered recurrences was 74% . 
similar patterns of relapse were found in previous studies reporting on involved - field or extended - field radiotherapy , out - of - field recurrence rates between 55% and 80% have been described [ 5 , 11 , 14 , 29 , 39 , 43 , 46 , 48 ]  . 
some of them showed prolonged relapse - free survival after total lymphatic irradiation compared to extended - field / involved - field irradiation [ 31 , 39 ] , the extension of treatment portals , however , did not impact overall survival . 
in addition , other groups have reported that the use of more extensive radiotherapy fields did not improve overall survival [ 16 , 20 , 31 , 39 , 40 , 53 ] , but larger portals obviously induce more acute and late toxicity [ 53 ]  . 
in the absence of randomized data , the optimal treatment volume remains unclear . the role of additional chemotherapy in localized stage low - grade non - hodgkins lymphoma is not well defined . 
randomized trials comparing involved - field radiotherapy alone with combination of chemotherapy and involved - field irradiation for stage iii follicular lymphoma have failed to show a significant improvement in progression - free or overall survival in patients receiving chemotherapy [ 10 , 14 , 36 , 38 , 54 ]  . however , besa et al . 
 [ 5 ] observed 15 - year progression - free and overall survival rates of 60% and 63% , respectively , 84 patients receiving involved - field radiotherapy combined with chemotherapy consisting of cyclophosphamide , vinciristine , and prednisone . 
anderson cancer center [ 5 , 45 ] , a phase iii clinical trial is being conducted in which involved - field radiotherapy alone is compared with chemotherapy and involved - field irradiation in patients with stage iii follicular lymphoma . biologic approaches have enriched the modern armamentarium against non - hodgkins lymphoma [ 4 , 24 ]  . 
interferon alpha seems to have been established as a life - extending therapy for selected patients with follicular lymphoma [ 1 , 6 , 22 , 23 , 28 , 41 ]  . 
humanized anti - cd20 monoclonal antibody ( rituximab ) has a 50% response rate in patients with follicular lymphoma , is still active when given a second time , and has been demonstrating synergistic activity when combined with chemotherapy [ 6 , 9 , 12 , 17 , 18 , 42 , 44 ]  . 
these results induce hope for the treatment of patients with systemic disease , but , as shown before , in case of localized lymphoma , radiotherapy with or without accompanying systemic therapy generates superior results and should therefore remain treatment of choice . 
 conclusions nodal low - grade non - hodgkins lymphoma was shown to be a curable disease by radiotherapy alone , but the exact target volume and radiotherapy dose still remain unclear . 
on the basis of our results we assume that tni can lead to better tumor control rates than radiotherapy techniques with less extensive treatment portals . among the analyzed prognostic factors only age proved to be of predicting clinical relevance . 
 strahlentherapie und onkologie original article increased metabolic activity in the spinal cord of patients with long - standing lhermittes sign olga sik1 , 2 , tibor csere3 , klra stefanits3 , szabolcs szakll jr.4 , zsolt lengyel4 , gza sfrny5 , katalin vnczky6 , erzsbet lengyel2 , judit olajos7 , gbor bajzik8 , lajos trn4 , 9 purpose : to investigate the pathophysiology of the radiation - induced , chronic lhermittes sign ( ls ) on the basis of long - standing case histories with partial functional recovery . 
 patients and methods : as radiotherapy in two nasopharyngeal cancer patients , a biologically effective dose ( bed ) of 103.8 gy2 ( case 1 ) and 94.8 gy2 ( case 2 ) was delivered to the cervical spinal cord . 
 results : pet demonstrated increased [ 18f ] fluorodeoxyglucose ( fdg ) accumulation and [ 15o ] butanol perfusion , but negligible [ 11c ] methionine uptake in the irradiated spinal cord segments in both patients . 
 conclusions : these data suggests a close direct relationship between regional perfusion and metabolism of the spinal cord , similarly as in the brathe postirradiation recovery may be related to energy - demanding conduction , explaining the increased metabolism and perfusion . 
 key words : nasopharyngeal carcinoma radiation myelopathy functional recovery permanent lhermittes sign positron emission tomography [ 18f ] fluorodeoxyglucose [ 15o ] butanol [ 11c ] methionine radiosensitivity strahlenther onkol 2003 ; 179 : 6903 doi 10.1007 / s00066 - 003 - 1115 - z erhhte metabolische aktivitt im rckenmark von patienten mit anhaltendem lhermitte - zeichen ziel : untersuchung der pathophysiologie des strahleninduzierten chronischen lhermitte - zeichens auf der basis der langzeitbeobachtung von zwei patienten mit partieller funktioneller erholung . 
 patienten und methodik : bei zwei patienten mit nasopharynxkarzinom wurde die halswirbelsule mit einer biologisch effektiven dosis ( bed ) von 103 , 8 gy2 ( patient 1 ) bzw . 
 ergebnisse : im pet zeigten sich bei beiden patienten eine erhhte [ 18f - ] fluorodesoxyglucose - ( fdg - ) aufnahme und [ 15o - ] butanol - perfusion , jedoch eine vernachlssigbar geringe [ 11c - ] methionin - aufnahme in den bestrahlten segmenten . 
die erholung nach der strahlentherapie drfte mit energie verbrauchenden prozessen 1 department of oncotherapy , semmelweis university , budapest , hungary , 2 department of radiotherapy , national institute of oncology , budapest , hungary , 3 department of oncotherapy , university of pcs , hungary , 4 pet center , university of debrecen , hungary , 5 national research institute for radiobiology and radiation hygiene , budapest , hungary , 6 outpatient department of neurology , national institute of oncology , budapest , hungary , 7 department of oncoradiology , jsa andrs county hospital , nyregyhza , hungary , 8 department of diagnostic imaging , university of kaposvr , hungary , 9 pet study group of the hungarian academy of sciences , debrecen , hungary . 
 schlsselwrter : nasopharynxkarzinom strahleninduzierte myelopathie funktionelle erholung permanentes lhermitte - zeichen positronenemissionstomographie [ 18f - ] fluorodesoxyglucose [ 15o - ] butanol [ 11c - ] methionin strahlenempfindlichkeit introduction radiation myelopathy , a rare , but extremely serious side effect of radiotherapy , usually exhibits a chronic , progressive , irreversible clinical course . 
a 43 - year - old female diagnosed in 1995 with stage ia extranodal ( nasopharyngeal ) hodgkins disease ( revised pathology ) received telecobalt irradiation ( details in table 1 )  . following irradiation , she was symptom - free until 2000 , when she exhibited a pronounced ls ( grade 2 toxicity ) without other spinal cord - related sensory or motor disturbances , but with emg signs of a peripheral neurogenic lesion . 
a 41 - year - old man diagnosed with nasopharyngeal cancer ( t2 n2b m0 ) in 1976 , received telecobalt irradiation ( relevant doses in table 1 )  . 
sensory and motor impairments related to spinal cord levels c3t1 developed after 2 months : ls , mild sensory disturbances below c8 and mild , mainly distal paresis in both arms ( grade 3 toxicity according to common toxicity criteria [ ctc ] , version 2.0 [ 19 ] )  . electromyography ( emg ) revealed signs of a peripheral neurogenic lesion . 
 after 25 years , a moderate ls was still detectable , with very little sensory ( paresthesia in the hands and feet ) or motor ( diminished biceps and radial reflexes bilaterally ) impairment ( grade 2 toxicity )  . electroneurography ( eng ) revealed that the motor conduction velocity was slightly reduced in the right peroneal nerve ( 42 m / s ) , as was the sensory conduction velocity in the right ( 40.6 m / s ) and left ( 36.4 m / s ) ulnar nerves ( normal value 45 m / s ) , but all other investigated peripheral nerve conduction velocities proved normal . 
 mri ( magnetic resonance imaging ) investigations were performed on a 1.5 - t system ( magnetom vision plus , siemens , erlangen , germany ) , and pet ( positron emission tomography ) examinations with a ge 4096 plus scanner ( general electric , uppsala , sweden ) , using [ 18f ] fluorodeoxyglucose ( fdg ) , [ 11c ] methionine and [ 15o ] butanol as tracers . 
for numerical comparisons , standardized uptake values ( suvs ) were determined in the axial plane of the fdg and methionine pet images by placing a region of interest ( roi ) covering the cervical spinal cord between vertebral bodies c2 and c7 , and t1 and t3 to characterize the irradiated and nonirradiated segments , respectively . 
in case 1 , the fields were divided , when 40 gy was reached in the midline of the nasopharynx , and for the nasopharynx and the upper cervical region , a shrinkage - field technique was applied . 
the indicated technique and the different thicknesses of the head and neck regions explain the different radation doses to the cervical spinal cord , nasopharyngeal region , and upper cervical vertebral bodies bthe biologically effective dose ( bed = nd [ 1 + d / ( cid : 1 ) / ( cid : 2 ) ] , where n denotes the number of fractions , d the dose per fraction , and ( cid : 1 ) / ( cid : 2 ) = 2 gy is indicated , presuming white matter injury in the cervical spinal cord ) strahlenther onkol 2003 no . 
only the rare ls , manifested with a longer latency period , may forecast permanent spinal cord injury [ 1 , 2 , 13 ] , but this did not hold true in case 2 . 
in the few studies on large patient groups with ls , the rate of occurrence was 3.613% [ 2 , 7 , 13 , 27 , 35 ]  . only a single ls case with extraordinarily severe symptoms lasting for 1 year has been described in the english literature [ 29 ]  . according to the ctc version 2.0 [ 19 ] , our patients initially had grade 3 ( case 1 ) and grade 2 ( case 2 ) sequelae . 
the most noteworthy features included complete clinical recovery from the motor injuries ( case 1 ) , incomplete regeneration of the sensory symptoms ( case 1 ) , and permanency of the ls ( both cases )  . 
development of this symptom starts at around 30 gy [ 1 , 13 ] , the main risk factors for its manifestation [ 7 , 17 ] being a total dose of 50 gy and a daily dose of 2 gy ( equivalent to a calculated critical bed of 100 gy2 )  . 
the probability of occurrence of ls shows a shallow dose - effect curve [ 7 ] ; at a total dose of < 50 gy or 50 gy , this probability is 3.3% or 8% , respectively , and at a fraction dose of < 2 gy or 2 gy , it is 3.4% or 10% , respectively . 
 mri , sensitive in the detection of demyelination , failed to show pathologic signs in our patients ; thus , we applied pet , a very sensitive tool to revealing the functional status of different organs [ 15 , 16 , 21 , 22 , 31 ]  . 
few studies have been published on pet investigations of the spinal cord ; this may be due , in part , to the normally very low fdg uptake , because of the considerable mass of white matter with a low glucose consumption relative to the small bulk of gray matter [ 3 , 14 , 18 , 32 , 33 ]  . 
our data argued in favor of a close direct relationship between the regional spinal cord blood flow and the glucose metabolism , similarly as in the brain [ 23 ]  . 
this is to be expected : stabilization in the clinical state after improvement during many years would not be anticipated to be still accompanied by a restoration process involving intensive cell proliferation . 
pet investigations in chronic lhermittes sign tribute substantially , if at all , to a metabolic activity increase . the pathologic results [ 12 , 20 , 25 , 26 ] also argue against a substantial inflammatory reaction in radiation myelopathy . 
 we earlier hypothetized [ 6 ] that radiation - induced demyelination of the axon membrane induces a high compensatory expression of sodium channels to restore conduction , similarly as in multiple sclerosis [ 8 , 30 ]  . 
although this hypothesis was not proved by molecular biological studies , it is consistent with our findings , and we support this phenomenon as the underlying mechanis individual radiosensitivity can contribute to the development of radiation - induced toxic reactions . 
the fibroblast radiosensitivity in case 1 was higher than that in case 2 ; besides the higher bed , this may have contributed to the differences between the two cases ( more severe sequelae and longer history in case 1 )  . 
this seems probable , even if the fibroblasts radiosensitivity may be used only as an estimate of that of oligodendrocytes or endothelial cells , as targets of radiation damage to the cns . 
 acknowledgments the authors thank julianna pisch , md , department of radiation oncology , beth israel medical center , new york , usa , for her useful comments during the preparation of the manuscript . 
 strahlentherapie und onkologie original article aggressive simultaneous radiochemotherapy with cisplatin and paclitaxel in combination with accelerated hyperfractionated radiotherapy in locally advanced head and neck tumors results of a phase iii trial thomas kuhnt1 , axel becker1 , 2 , steffi pigorsch1 , tanja pelz1 , marc bloching3 , marcus passmann3 , erwin lotterer4 , gabriele hnsgen1 , jrgen dunst1 background : simultaneous radiochemotherapy ( srct ) is the treatment of first choice in locally advanced head and neck cancers . we have tested a very aggressive combination protocol with cisplatin and escalated paclitaxel in combination with accelerated hyperfractionated radiotherapy to assess the maximum tolerated dose ( mtd ) , dose - limiting toxicity ( dlt ) , overall toxicity , and response rate . 
irradiation was administered in daily doses of 2 gy up to 30 gy followed by 1.4 gy twice daily up to 70.6 gy to the primary tumor and involved nodes and 51 gy to the clinically negative regional nodes . 
the chemotherapy schedule included cisplatin in a fixed dose of 20 mg / m2 on days 15 and 2933 and paclitaxel at increasing dose levels of 20 , 25 , 30 mg / m2 twice weekly over the whole treatment time . 
we recruited mainly patients with large tumors for this protocol ; all patients were stage iv , and the mean tumor volume ( primary + metastases ) amounted to 72 61 cm3 . 
in summary , six patients died of local tumor progression ( n = 2 ) , distant metastases ( n = 2 ) , or therapy - related complications ( n = 2 ) during follow - up . 
 conclusions : this very aggressive srct protocol yielded excellent response and survival figures but was associated with a very high rate of acute toxicity ( 8% therapy - related deaths )  . 
 key words : head and neck cancer radiotherapy chemotherapy prognosis strahlenther onkol 2003 ; 179 : 67381 doi 10.1007 / s00066 - 003 - 1106 - 0 1 department of radiotherapy , martin luther university , halle , germany , 2 department of radiotherapy , municipial hospital , dessau , germany , 3 department of head and neck surgery , martin luther university , halle , germany , 4 department of internal medicine i , martin luther university , halle , germany . 
 patienten und methodik : zwischen 1998 und 2001 behandelten wir 23 patienten ( 20 mnner , drei frauen ) , die an einem primr inoperablen , therapienaiven plattenepithelkarzinom im hno - bereich litten , mit einer definitiven radiotherapie mit 2 gy bis 30 gy und anschlieend 2 ( cid : 1 ) 1 , 4 gy bis 70 , 6 gy plus simultaner gabe von cisplatin in gleich bleibender dosierung von 20 mg / m2 krperoberflche ( kof ) fnfmal wchentlich an tag 15 und 2933 plus paclitaxel zweimal wchentlich in den dosisstufen von 20 / 25 / 30 mg / m2 kof ber die gesamte bestrahlungszeit . 
die dlt wurde definiert als toxizitt grad 4 oder toxizitt grad 3 , die zu einer therapieunterbrechung oder einer ungeplanten hospitalisierung gefhrt hatte , oder jegliche grad - 3 - neurotoxizitt . 
die dlt bestand in feuchten desquamationen der haut ctc - grad 4 ( n = 2 ) und einer febrilen neutropenie ctc - grad 3 ( n = 1 )  . 
sechs patienten starben an einer lokalen tumorprogression ( n = 2 ) , an fernmetastasen ( n = 2 ) oder an den therapiefolgen ( n = 2 ) whrend der nachuntersuchungszeit . 
 schlussfolgerungen : die vorliegende studie zeigt , dass die kombination von zwei eigenstndig wirksamen zytostatika in hoher dosierung , ber den gesamten therapiezeitraum appliziert , mit einer intensivierten , zeitverkrzten radiotherapie auch im kopfhals - bereich mglich ist . 
 schlsselwrter : hno - tumoren radiotherapie chemotherapie prognose introduction accelerated hyperfractionated radiotherapy with shortening of the overall treatment time of radiotherapy has yielded improved disease - free survival and overall survival in locally advanced head and neck tumors as compared to conventionally fractionated irradiation [ 1 , 10 , 15 ]  . 
moreover , two recent german studies have confirmed that the addition of concurrent chemotherapy even to accelerated hyperfractionated radiotherapy may further improve local control and survival [ 6 , 30 ]  . 
many of these studies , however , have used single - agent regimens and did not include cisplatinum . recently published studies with srct have observed a survival benefit of up to 20% with platinum - based or combination regimens [ 4 , 7 , 35 ]  . 
 patients and methods treatment protocol the basis for the treatment schedule comes from a recently started randomized study of the german cancer society . the study uses a hyperfractionated accelerated fractionation regimen up to a total dose of 70 gy in combination with simultaneous 5 - fluorouracil / mitomycin c ( 5 - fu / mmc ) or cisplatin monotherapy in locally advanced head and neck tumors . 
paclitaxel was administered twice weekly on the basis of a dosefinding phase i / ii study which we had performed earlier in recurrent head and neck cancers [ 3 ]  . 
we used a fixed dose of cisplatin ( under the assumption that cisplatin is the most effective drug in combination with radiotherapy in head and neck cancers ) , and the dose of paclitaxel was escalated . 
 staging procedures prior to treatment all patients underwent clinical examination , contrast - enhanced ct scans ( additional mri in the majority of patients ) , thoracic ct ( to exclude lung metastases ) , abdominal liver ultrasound or ct ( to exclude liver metastases ) , and routine laboratory workup . 
 the total tumor volume and the necrotic tumor volume ( as named in ct scan the hypodense tumor area without accumulation of contrast material ) was calculated from pretreatment ct scans using the ellipsoid formula ( volume = 1 / 6 ( cid : 1 ) ( cid : 1 ) a ( cid : 1 ) b ( cid : 1 ) c , with a , b , and c being the largest diameter in three dimensions )  . 
 cisplatin 20 mg / m2 taxol 20 / 25 / 30 mg / m2 radiotherapy : 5 2 gy / week , 2 1.4 gy / d td 70.6 gy radiotherapy radiotherapy was administered with 6or 10 - mv photons and electrons . 
all patients had cast fixation with individual masks and underwent three - dimensional ( 3 - d ) treatment planning with a thickness of ct slices of 35 m3 - d conformal therapy was used in all patients . 
the clinical target volumes ( ctv ) received the following doses according to a previous study [ 6 ] : ctv 1 : primary tumor and all macroscopic nodes with a safety margin of about 23 cm ( smaller margins in areas with defined anatomic borders , e.g. , lymph nodes adjacent to the spine )  . 
 inclusion criteria exclusion criteria severe comorbidity ( especially impaired renal or cardiac function ) secondary cancers distant metastases at diagnosis pregnancy or breast - feeding inoperable , locally advanced squamous cell cancer of the head and neck region sites : oral cavity , oropharynx , hypopharynx age 1875 years karnofsky index 70% measurable tumor no severe comorbidity with contraindications to scheduled chemotherapy adequate compliance informed consent strahlenther onkol 2003 no . 
 all doses refer to a reference point in the middle of the grade 4 toxicity or grade 3 toxicity requiring treatment interruption or unplanned hospitalization or grade 3 neurologic toxicity . 
after reaching the dose level of the mtd , the study was planned to be continued as an early phase ii study with a paclitaxel dose which was one dose level below the level of the mtd . 
 chemotherapy patients received cisplatin in a fixed dose of 20 mg / m2 on days 15 and 2933 as short infusion ( infusion time about 30 min ) immediately prior to the daily radiation fraction . 
prophylactic feeding gastrostomy tubes were used in all patients . premedication prior to the infusion of paclitaxel ( 1 / 2 h before infusion ) consisted of dexamethasone 8 mg i.v. , ranitidine 50 mg i.v. , and diphenhydramine 2 mg i.v. 
immediately after the cisplatin infusion , an additonal infusion therapy with isotonic electrolytes 500 ml , glucose solution 500 ml , and mannitol 500 ml was administered over about 12 h . 
we used , however , a stringent supportive treatment in case of neutropenia ( leukocytes < 1 gpt / l ) or fever consisting of quinolone ( ciprobay i.v. ) , nitroimidazole ( clont i.v. ) , and fluconazole ( diflucan )  . 
moreover , we tried to keep the hemoglobin level in the normal range by administering blood transfusions if the hemoglobin level dropped below 6.8 mmol / l ( corresponding to 11 g / dl )  . 
an intensive rinsing of the oral cavity was done by iodine solution and dexpanthenol solutions with or without antifungal agents or sage tea and vitamin a oil ( vitadral l )  . 
to avoid skin reactions , we applied a dexamethasone / dexpanthenol salve and a bactericidal salve ( ratio 1 : 1 ) ( bepanthen salbe / fucidine salbe )  . 
 determination of dlt and mtd patients were recruited in cohorts of three to six , and the mtd was reached if two out of six patients in one cohort developed dlt . 
 determination of remission the tumor response was determined according to the who criteria ( cr : complete response , pr : partial response , nc : no change , pd : progressive disease ) 6 weeks after the end of therapy on the basis of a clinical examination and ct scans and / or mri . 
 results patient population from may 1998 through june 2001 , 24 patients were enrolled in the protocol in our department , 21 males and three females . one patient died on day 10 after start of radiotherapy due to an infection of the gastrostomy tube and was considered an early toxic death but excluded from further analysis leaving 23 patients who were evaluated for acute toxicity and response . 
primary tumor sites were the oral cavity in three patients , the oropharynx in ten , the oro - / hypopharynx in three , the hypopharynx in six , and the larynx in one . 
aggressive rct in head and neck cancer category , was t1 in one patient , t2 in none of the patients , t3 in two , and t4 in 20 patients . 
cisplatin was administered in the scheduled doses in all patients but one ; this patient received 5 ( cid : 1 ) 20 mg / m2 cisplatin in week 1 , but further cisplatin therapy was omitted due to subsequent impaired renal function with creatinine elevation . patients received a mean number of twelve paclitaxel infusions ( range nine to 13 )  . 
 mtd and dlt the mtd of paclitaxel in this combination protocol was reached in the third cohort at a dose level of 30 mg / m2 , when two severe skin erythemas grade 4 and one febrile neutropenia grade 3 occurred . 
in summary , three patients were treated in cohort 1 at a dose level of 20 mg / m2 paclitaxel twice weekly , 17 patients ( three patients in cohort 2 and 14 additional patients after having reached the mtd ) at a dose level of 25 mg / m2 twice weekly , and three patients ( cohort 3 where the mtd was reached ) at a dose level of 30 mg / m2 twice weekly . 
18 / 23 patients ( 78% ) required blood transfusions ( 13 units ) to keep the hemoglobin level > 6.8 mmol / l ( 11g / dl ) , and five patients received additional epoetin alfa . 
 toxicities ( ctc criteria ) ( n ) grade 0 grade 1 grade 2 grade 3 grade 4 side effects mucositis erythema hb levela leukocytes platelets liver function renal function infections cohort 1 paclitaxel 20 mg / m2 cohort 2 paclitaxel 25 mg / m2 cohort 3 paclitaxel 30 mg / m2 figure 2 . 
 in summary , six patients died of local tumor progression ( n = 2 ) , distant metastases with locoregionally controlled disease ( n = 2 ) , or therapy - related septic complications ( n = 2 )  . at the date of analysis , 18 patients ( 75% ) were alive with a median follow - up of 30 months . 
 discussion several recent meta - analyses have demonstrated a small ( about 5% absolute difference ) but significant benefit in overall survival for srct as compared to radiotherapy alone in patients with locally advanced head and neck cancer [ 26 ]  . 
therefore , the earlier studies which used conventional fractionation in the radiation - alone arms did not answer the question whether the benefit of chemotherapy would also be present if optimal radiotherapy with accelerated fractionation would be used . some very recent studies , however , support an advantage of rct even over optimal radiotherapy . 
budach [ 6 ] compared an accelerated hyperfractionated radiotherapy regimen with a total dose of 77 gy to the same fractionation regimen with a reduced dose ( 70 gy ) plus additional 5 - fu / mmc . 
the addition of chemotherapy increased locoregional control , distant metastases - free survival , and overall survival as compared to the accelerated hyperfractionated radiotherapy regimen , suggesting that rct is superior even to optimal radiotherapy . 
more recent studies using platinum - based chemotherapy regimens or combinations of 5 - fu / mmc have demonstrated a higher survival benefit than earlier studies suggesting that these regimens might be superior to other drugs [ 4 , 7 , 16 , 17 , 20 , 35 , 37 ]  . 
even in low concentrations , paclitaxel induces a specific arrest at the g2 - / m checkpoint of the cell cycle by fusion with tubulin , an important part of the cytoskeleton . 
the cells persist in a g2 arrest , a phase with high radiosensitivity . additionally , an improvement in reoxygenation and an activation of apoptosis have been observed [ 5 , 14 , 27 ]  . 
so far , nine phase i / ii trials with srct including paclitaxel in tumors of the head and neck have been published ( table 4 ) [ 5 , 8 , 19 , 23 , 28 , 3134 ]  . the treatment schedules were different , but all studies showed a nearly 100% response rate . 
dlt was either skin toxicity ( moist dermatitis grade 4 ) , oral cavity mucositis grade 3 , and febrile neutropenia grade 3 ( 8 / 9 studies mucositis , 4 / 9 studies neutropenia als dlt )  . 
achf : acceleration - hyperfractionation ; auc : area under the curve ; cbdca : carboplatinum ; cddp : cisplatin ; ci : continuous infusion ; d : dermatitis ; d : day ; dlt : dose - limiting toxicity ; 5 - fu : 5 - fluorouracil ; gi : gastrointestinal disorder ; h : hours ; hf : hyperfractionation ; hu : hydroxyurea ; lv : leucovorin ; mtd : maximum tolerated dose ; mu : mucositis ; nf : normfractionation ; np : neutropenia ; os : overall survival ; si : single infusion . 
we administered paclitaxel twice weekly in combination with cisplat the rationale results from experimental findings and was also chosen on the basis of a preceding study in recurrent head and neck tumors [ 2 , 36 ]  . our study supports the high efficacy of paclitaxel with regard to response . 
the fact that we recruited mainly patients with locally very advanced tumors for this phase i / ii protocol is underlined by a comparison of tumor volumes in patients in other protocols . 
for example , the median tumor volume of 133 patients with head and neck cancers who have recently been recruited for a study on tumor oxygenation in our department amounted to 49 cm3 . 
nevertheless , we assume that a subset of patients with very unfavorable tumors on the one hand and good performance status on the other might benefit from this approach , and the regimen should therefore be tested in a randomized study against standard rct regimens . 
 this study was supported by a research grant of bristol - myers squibb . acknowledgment strahlentherapie und onkologie short communication moist skin care can diminish acute radiation - induced skin toxicity felix momm , christian weienberger , susanne bartelt , michael henke1 background : radiation treatment may induce acute skin reactions . 
 patients and methods : 88 patients with carcinomas of the head and neck undergoing radiotherapy with curative intent ( mean total dose 60 gy , range : 5074 gy ) were evaluated weekly for acute skin reactions according to the rtog - ctc score . 
the incidence of grade i , ii , and iii reactions and the radiation dose at occurrence of a particular reaction were determined and statistically analyzed using the log - rank test . 
 key words : radiotherapy skin care urea lotion head and neck cancer strahlenther onkol 2003 ; 179 : 70812 doi 10.1007 / s00066 - 003 - 1142 - 9 feuchte hautpflege kann akute hautreaktionen bei einer strahlentherapie vermindern hintergrund : eine strahlentherapie kann akute hautreaktionen hervorrufen , die sich auf verschiedene weise behandeln lassen . die einzelnen behandlungsmethoden wurden bislang jedoch nur unzureichend ausgewertet . 
 patienten und methodik : bei 88 patienten mit plattenepithelkarzinomen im kopf - hals - bereich ( tabelle 1 ) , die mit kurativer intention bestrahlt wurden ( mittlere gesamtdosis 60 gy , 5074 gy ) , wurden wchentlich akute hautreaktionen nach dem rtog - ctcscore bestimmt . 
die inzidenz von grad - i - , - iiund - iii - reaktionen und die strahlendosis bei auftreten der entsprechenden reaktionen wurden bestimmt und mittels log - rank - test analysiert ( abbildung 2 )  . 
50% der patienten mit feuchter hautpflege zeigten bei einer dosis von 26 gy eine hautreaktion grad i , mit trockener hautpflege bei einer dosis von 22 gy ( p = 0 , 03 )  . 
22% der patienten mit feuchter hautpflege litten unter einer akuten hauttoxizitt grad iii , verglichen mit 56% der patienten in der kontrollgruppe ( p = 0 , 0007 ; abbildung 2 )  . 
 schlussfolgerung : feuchte hautpflege mit einer 3%igen urea - lotion verzgert das auftreten und verringert das ausma akuter hautreaktionen whrend einer strahlentherapie bei perkutan bestrahlten patienten mit tumoren im kopf - hals - bereich . 
in most cases , late skin toxicity is not difficult to handle , although it can lead to problems in reirradiations or interactions with cytotoxic drugs [ 6 , 16 , 17 ]  . 
thanks to welldocumented data describing skin toxicity in our patients with head and neck cancer , we were able to investigate retrospectively , whether a moist skin care with 3% urea lotion may reduce skin toxicity in patients undergoing radiotherapy . 
 patients and methods design and patients from january 1997 to january 1999 , data on acute skin reactions was collected for patients with head and neck cancer treated within two multicenter studies ( wr - 38 , mf - 4449 ) [ 1 , 8 ] ( table 1 )  . 
both studies were conducted according to good clinical practice ( gcp ) standards and audited independently . at that time , irradiated skin of inpatients was treated with 3% urea lotion ( eucerin 3% , beiersdorf , hamburg , germany )  . 
outpatients were treated with either urea lotion or powder , depending randomly on the date when they started therapy ( azulon , baxter oncology gmbh , formerly asta medica awd ; frankfurt / main , germany )  . 
the present study evaluates the effect of moist skin care of 43 hospitalized patients and 20 outpatients as compared to dry skin care of 25 outpatients ( controls )  . 
 radiotherapy irradiation was performed using a 6 - mev linear accelerator , and standard radiotherapy dose / fractionation protocols ( 5 ( cid : 1 ) 2 gy / week ) were followed . 
60 gy ( 4 gy ) were applied in case of complete tumor resection ( r0 , r1 ) , and 70 gy ( 4 gy ) for primary treatment or macroscopically incompletely resected tumors ( r2 )  . 
moist skin care in radiation therapy if skin lesions grade iii or iv occurred , treatment with lotion or powder was stopped and the patient received appropriate wound care programs ( povidone - iodine and zinc ointments )  . 
 being treated in clinical trials , all patients were seen at least three to five times per week by a physician , who took care for their compliance with the skin care progra clinical scoring all patients were monitored daily during the course of radiotherapy . 
in order to avoid interobserver variations , it was ensured that the weekly skin toxicity scoring ( rtog - ctc score ) was performed by one and the same physician [ 3 , 20 , 21 ]  . 
the patients of the wr - 38 trial were randomly allocated to receive amifostine ( open - label study ) and those of study mf - 4449 to receive either epoetin beta or placebo . 
a secondary variable was the necessity of hospitalization of outpatients during the radiotherapy course . statistical analyses to graphically demonstrate results , dose - incidence and time plots were performed ( figures 1 and 2 )  . 
there was a fairly even distribution between the moist skin care and the control group in terms of sex , tumor localization , stage , hemoglobin level , and treatment parameters . 
additionally , regression lines for all other dose - time observations ( n = 479 ) are constructed ( moist skin care patients : solid line ; controls : dotted line )  . 
zustzlich sind regressionsgeraden fr alle anderen dosis - zeit - aufzeichnungen ( n = 479 ) eingetragen ( patienten mit feuchter hautpflege : durchgezogene linie ; kontrollen : gepunktete linie )  . 
moist skin care in radiation therapy grade i p = 0.03 grade iii p = 0.0007 discussion grade ii p = 0.006 of controls causing 45 days of hospitalization ( 2.25 days / patient ) in the moist skin care and 150 days ( 6 days / patient ) in the control patients . 
reasons for hospitalization included acute skin and / or mucosa reactions due to radiotherapy : in some of our patients , moist skin care could prevent hospitalizations , which means saving of high treatment costs . 
 differences in dose densities between both groups were not found : dose - time plots at occurrence of a particular reaction were comparable for both groups ( figure 1 )  . 
 further , hemoglobin values of both skin care groups did not differ ( table 1 ) , ruling out a distinct , hemoglobin levelrelated reaction pattern [ 8 ]  . 
however , no imbalance of amifostine administration was seen between both groups ( table 1 ) , and amifostine is not reported to influence acute skin reactions [ 1 ]  . 
dexpanthenol cream or anti - inflammatory agents were used , but seem not to influence the skin reaction , though inducing considerable side effects [ 7 , 11 , 19 ]  . 
the median dose causing a grade i skin reaction was 26 gy in moist skin care patients and 22 gy in controls ( p = 0.03 , log - rank test ; figure 2 )  . 
 94% of the moist skin care patients and 96% of the controls suffered from skin toxicity grade ii , and the median dose for grade ii reactions to occur was 51 gy versus 34 gy ( p = 0.006 ; figure 2 )  . 
water - binding agents ( such as hyaluronic acid ) are regarded as the underlying cause [ 10 ]  . as we used a 3% urea lotion , characterized by its water - binding properties , our results are consistent with those from former studies . 
an exception might be the use of special growth factors ( e.g. , keratinocyte growth factor [ kgf ] ) [ 19 ] , which has to be examined for its effectiveness and safety in interaction with tumor therapy in future studies . 
modern irradiation techniques , such as high - energy linear accelerators or intensitymodulated radiotherapy , are intended to reduce side effects , but still , supportive measures like skin care are an essential issue . 
 an efficient control of side effects is even more important in palliative treatment to maintain the patients quality of life . thus , further studies on supportive measures for radiotherapy patients are warranted . 
the underlying mechanism is possibly related to its water - binding capacity and should be further studied . although most radiotherapy centers prefer dry skin care [ 23 ] and report good results with this treatment , it still seems possible to optimize skin care programs for radiotherapy patients . strahlentherapie und onkologie mitteilung der dgmp zur personalsituation der medizinischen strahlenphysik in der strahlentherapie in deutschland auswertung einer umfrage hans - karl leetz1 , hermann hans eipper2 , hans gfirtner3 , peter schneider4 , klaus welker5 zusammenfassung um einen berblick ber die aktuelle personalsituation in der medizinischen strahlenphysik zu gewinnen , wurde vom arbeitsausschuss personalbedarf der deutschen gesellschaft fr medizinische physik ( dgmp ) im jahr 1999 eine umfrage unter den auf diesem gebiet ttigen dgmp - mitgliedern durchgefhrt . 
unter bercksichtigung der altersverteilung der mitglieder der dgmp errechnet sich fr die bundesrepublik ein bedarf an ausbildungskapazitt von etwa 100 medizinphysikern im jahr ( davon 19 fr die strahlentherapie ) , wenn dieses defizit im verlauf von 10 jahren abgebaut werden soll . 
 schlsselwrter : personalbedarf ausbildungskapazitt medizinische strahlenphysik strahlenther onkol 2003 ; 179 : 7216 doi 10.1007 / s00066 - 003 - 1154 - 5 staffing levels in medical radiation physics in radiation therapy in germany . 
summary of a questionnaire abstract to get a general idea of the actual staffing level situation in medical radiation physics in 1999 a survey was carried out by the taskgroup personalbedarf of deutsche gesellschaft fr medizinische physik ( dgmp ) among all dgmp - members who are active in this field . 
from the answers regarding equipment and activities numbers for staff are calculated by the methods given in report 8 and 10 for this spot check target and compared with effective staffing levels . 
from the age distribution of dgmp - members and the calculated deficit resulted a training capacity of about 100 medical physicists at all per year ( 19 in radiation therapy ) if the deficit shall be cut back in 10 years . 
basis der umfrage waren die in den berichten 8 und 10 der deutschen gesellschaft fr medizinische physik ( dgmp ) zum personalbedarf in der medizinischen strahlenphysik definierten hauptkomponenten [ 1 , 2 ]  . 
ziele der aktion waren die ermittlung zuverlssiger ist - werte fr die personalsituation in der medizinischen strahlenphysik , die berechnung der soll - werte fr das in der umfrage erfasste kollektiv unter anwendung der formalismen aus den berichten zum personalbedarf , allen in kliniken und vergleichbaren institutionen ttigen medizinphysikern , die mitglied der dgmp sind , sowie einidie projektion der stichprobenresultate auf deutschland , die abschtzung des ausbildungsbedarfs . 
 1 universittskliniken , institut fr radiologische physik , homburg / saar , 2 stdtisches krankenhaus merheim , radiologische klinik , bereich medizinische physik , kln , 3 klinikum passau , medizinische physik , passau , 4 klinikum fulda , institut fr medizinische physik , fulda , 5 krankenhaus moabit , abteilung medizinische physik , berl eingang : 29 . 
personalsituation der medizinischen strahlenphysik material und methodik der fragebogen [ 12 ] sollte einerseits einen mglichst geringen aufwand zur beantwortung erfordern , andererseits aber auch eine zuverlssige basis fr die anwendung der in den dgmp - berichten 8 und 10 enthaltenen formalismen zur berechnung des personalbedarfs ergeben . 
 die aktuelle personalausstattung wurde horizontal in anzahl der mitarbeiter und anzahl der darin enthaltenen physiker unterteilt , vertikal in den gesamtbereich der medizinischen strahlenphysik und die betreuten teilbereiche strahlentherapie , nuklearmedizin , rntgendiagnostik , strahlenschutz und sonstiges . 
zur plausibilittskontrolle der beantworteten fragebgen wurden rechnerisch die gesamtpersonalzahl mit der summe der personalzahlen der teilbereiche verglichen und die brigen abschnitte der fragebgen auf offensichtliche widersprche in den antworten durchgesehen . 
 in den dgmp - berichten 8 und 10 ist angegeben , wie aus den zahlen der hauptkomponenten der personalbedarf fr eine solide qualitt der dienstleistungen in der medizinischen strahlenphysik berechnet werden kann . 
aus den daten der stichprobe wurden in gleicher weise die soll - werte fr das personal berechnet und zusammen mit den aus den fragebogendaten entnommenen ist - werten in tabelle 3 zusammengestellt . 
im sollwert fr die rntgendiagnostik sind die fr die edv - systeme pacs ( picture archiving and communication system ) und ris ( radiologie - informationssystem ) berechneten personalzahlen enthalten . 
 hochrechnung der stichprobe auf deutschland ist - werte die ist - werte - hochrechnung der stichprobe aus tabelle 3 wurde fr physiker und gesamtpersonal auf unterschiedlichen wegen vollzogen : die zahl der in deutschen kliniken auf dem gebiet der medizinischen strahlenphysik ttigen physiker wurde durch auszhlung des mitgliederverzeichnisses der dgmp ermittelt ( alle physiker mit einer adresse , welche auf eine ttigkeit in der medizinischen strahlenphysik hindeutet ) [ 3 ]  . 
mit diesen fr alte und neue bundeslnder unterschiedlichen nichtmitglieder - faktoren wurden die resultate der zweiten spalte von tabelle 4 korrigiert und die gesamtzahl der in bundesdeutschen kliniken auf dem fachgebiet der medizinischen strahlenphysik ttigen physiker zu 635 berechnet . 
in der stichprobe waren 475 , 8 physiker ermittelt worden ( tabelle 3 ) , d.h. , der faktor fr die hochrechnung der physikerzahlen von der stichprobe zu deutschland betrgt 1 , 34 . 
 unter der annahme , dass sich das in der stichprobe gefundene verhltnis von physikern zum gesamtpersonal bei der bertragung auf deutschland nicht ndert , wurde mit dem faktor 1 , 34 auch das gesamtpersonal von 1128 mitarbeitern insgesamt auf deutschland hochgerechnet . 
 ( die nachkommastellen bei den personalanzahlen ergeben sich aus teilzeitbeschftigung und anteiliger betreuung anderer bereiche . ) in der medizinischen strahlenphysik ttiges personal ( ist - anzahlen aus 173 ausgewerteten fragebgen ) gesamtgebiet gesamt physiker rntgendiagnostik gesamt physiker nuklearmedizin gesamt physiker strahlentherapie gesamt physiker strahlenschutz gesamt physiker andere bereiche gesamt physiker 845 , 2 475 , 8 531 , 9 319 , 9 107 , 5 68 , 1 122 , 1 51 , 5 51 , 1 26 , 4 32 , 7 9 , 9 strahlenther onkol 2003 no . 
aufteilung des in der medizinischen strahlenphysik ttigen personals auf die einzelnen arbeitsbereiche . arbeitsbereich gesamtpersonal physiker allein strahlentherapie nuklearmedizin rntgendiagnostik strahlenschutz sonstige bereiche lenphysik auf die einzelnen fachgebiete wurde gem den prozentwerten aus tabelle 2 der stichprobenauswertung durchgefhrt , das resultat ist in tabelle 5 wiedergegeben . 
 soll - werte zur hochrechnung der soll - werte aus der stichprobe ( tabelle 3 ) auf deutschland wurden die in dem fragebogen abgefragten gerte - , untersuchungsund behandlungszahlen sowie andere daten benutzt . 
 hochrechnung der soll - werte fr die strahlentherapie die aus der stichprobe ermittelten zahlen von gerten und bestrahlungsserien wurden mit den werten in dem von heilmann [ 4 ] im auftrag der deutschen gesellschaft fr radioonkologie ( degro ) herausgegebenen band abteilungen und praxen fr strahlentherapie in deutschland verglitabelle 3 . 
medizinische strahlenphysik in kliniken der bundesrepublik : aus fragebogendaten fr die stichprobe ermittelte ist - werte , nach dgmp - berichten 8 und 10 berechnete soll - werte , rechnerisches defizit und besetzungsanteil an gesamtpersonal und physikern . 
 arbeitsgebiet defizit % gesamtpersonal soll ist wert wert physiker ist wert 531 , 9 strahlentherapie 107 , 5 nuklearmedizin 122 , 1 rntgendiagnostik strahlenschutz , allgemein 51 , 1 strahlenschutzbevollmchtigte sonstige bereiche summe 845 , 2 956 , 9 197 , 8 230 , 2 86 , 3 425 , 0 90 , 3 108 , 1 35 , 2 55 , 6 54 , 3 53 , 0 59 , 2 319 , 9 68 , 1 51 , 5 26 , 4 nicht def . 
der mittelwert 1 , 5 wurde als faktor zur hochrechnung der soll - zahlen fr physiker und gesamtpersonal in der strahlentherapie aus der stichprobe ( tabelle 3 ) auf deutschland gewhlt . 
 gesamtresultat der hochrechnung die anwendung der beschriebenen hochrechnungsfaktoren auf die soll - werte der stichprobe aus tabelle 3 ergibt die sollwerte fr den deutschlandweiten personalbedarf in der medizinischen strahlenphysik fr den bereich strahlentherapie , die differenz zu tabelle 3 das rechnerische defizit in absoluten und relativen zahlen . 
 soll wert 394 , 4 99 , 1 67 , 7 34 , 1 diskussion der umfrageergebnisse fr die strahlentherapie aus den prozentualen defizitzahlen der tabelle 7 geht hervor , dass das rechnerische defizit beim gesamtpersonal ( physiker und andere berufsgruppen ) wesentlich hher ist als bei den physikern allein . hier spiegelt sich die tatsache wider , dass die medizinphysikalischen arbeitsgruppen in kliniken keine vernnftig abgestufte qualifikationsstruktur aufweisen und nur mangelhaft mit hilfspersonal ausgestattet sind . 
mangels hilfspersonal bernehmen medizinphysiker hufig aufgaben , die preiswerter und rationeller von anderen berufsgruppen ( medizinisch - technische assistenten , physikalisch - technische assistenten , bropersonal , zivildienstleistende ) erbracht werden knnen . 
 74 , 5 31 , 0 16 , 2 7 , 7 81 , 1 68 , 7 76 , 1 77 , 4 defizit % 154 , 6 75 , 5 fachgebietsbezogen ist das defizit an physikern in der strahlentherapie mit 28% am geringsten ; dennoch ist dieses defizit gravierend , da die anwesenheit von physikern in der strahlentherapie gesetzlich vorgeschrieben ist . 
deshalb knnen wegen des defizits von 166 physikern etwa 80 beschleuniger - installationen ( mit zwei physikern pro installation ) nicht in betrieb gehen , und die im fragebogen abgefragte solide qualitt der arbeitsleistung wird nur zu etwa 72% erreicht . 
 bezugsgre stichprobe heilmann zvei 1999 verhltnis physiker gesamtpersonal gesamtgebiet davon in strahlentherapie nuklearmedizin rntgendiagnostik strahlenschutz sonstiges 1128 390 beschleuniger 261 kobaltanlagen afterloadinggerte 122 kilovoltgerte bestrahlungsserien 150 422 320 physiker 305 163 329 mittelwert deutschland / stichprobe 1 , 49 2 , 11 1 , 30 1 , 58 1 , 10 1 , 46 f = 1 , 50 tabelle 7 . 
medizinische strahlenphysik in deutschen kliniken : ist - werte , soll - werte , rechnerisches defizit und besetzungsanteil an gesamtpersonal und physikern . gesamtpersonal ist werte werte solldefizit % physiker ist solldefizit % vorhanden werte werte vorhanden 1128 4041 2913 1500 865 gesamtgebiet davon in strahlentherapie nukleartherapie nukleardiagnostik rntgen , konventionell rntgen fd / sel rntgen rdv 1435 592 166 30 1393 18 379 1249 strahlenschutz 239 201 in der schweiz befragte eine arbeitsgruppe der schweizerischen gesellschaft fr strahlenbiologie und medizinische physik ( sgsmp ) [ 8 ] 13 kliniken nach deren personalbestand in der medizinischen physik und nach ihrem gerteund untersuchungsspektrum in rntgendiagnostik , nuklearmedizin , strahlentherapie und strahlenschutz ; die arbeitsgruppe ermittelte in allen vier gebieten , wie viel prozent des laut dgmp - bericht nr . 
 resultate hnlicher umfragen in sterreich und in der schweiz wenige monate nach erscheinen der deutschen anhaltszahlen zum personalbedarf [ 1 ] erschienen in sterreich [ 7 ] und in der schweiz [ 8 ] vergleichende darstellungen des ist - bestandes an mitarbeitern der medizinischen physik zum sollbedarf nach dgmp - bericht nr . 
schmidt [ 7 ] die damals elf sterreichischen kliniken mit standorten von linearbeschleunigern nach personalund gerteausstattung sowie den behandlungszahlen und ermittelte den personalbedarf fr die medizinische physik in der strahlentherapie . 
die umfrage ergab , dass fr die strahlentherapie - abteilungen in sterreich 74 , 5 physikmitarbeiter , davon 31 , 2 physiker , vorhanden sein sollten ; in wirklichkeit war mit 72 , 3 gesamtmitarbeitern 97% des bedarfs abgedeckt ; mit 27 , 9 physikern war das soll ebenfalls zu 90% erfllt . 
schmidt , dass die hohen deckungsgrade nur scheinbar ausreichend seien , da die dgmp - anhaltszahlen keine aussage zum bedarf an physikern fr die bereiche forschung , entwicklung und lehre machen , bereiche , die zumindest an den sterreichischen universitten natrlich auch vertreten sind . 
 deutschland deutschland kliniken schweiz % vorhanden stichprobe ( tabelle 3 ) % vorhanden % vorhanden kliniken hochrechnung ( tabelle 7 ) medizinphysiker strahlentherapie nuklearmedizin rntgendiagnostik 55 strahlenschutz mitarbeiter strahlentherapie nuklearmedizin rntgendiagnostik 17 strahlenschutz strahlenther onkol 2003 no . 
personalsituation der medizinischen strahlenphysik geburtsjahr 1916 1918 1920 1922 1924 1926 1928 1930 1932 1934 1936 1938 1940 1942 1944 1946 1948 1950 1952 1954 1956 1958 1960 1962 1964 1966 1968 1970 1972 1974 1976 0 0 0 0 2 2 2 abbildung 1 . 
fasst man als ziel ins auge , dass dieses defizit in 10 jahren abgebaut werden soll , resultiert daraus und aus der altersstruktur die forderung nach einer jhrlichen ausbildungskapazitt von 106 ( = 86 + 20 ) medizinphysikern in deutschland . 
 mittelfristige perspektiven seit dem erscheinen der dgmp - berichte 8 und 10 , die dieser umfrageanalyse zugrunde liegen , haben sich fr alle von der auerdem werden in der eu - directive 97 / 43 ( patientenrichtlinie ) [ 9 ] in verschiedenen artikeln ( optimierung , verfahren , ausbildung , ausrstung , qualittssicherung , qualittskontrolle , klinische kontrolle ) umfangreiche vorgaben gemacht , die zur anhebung der qualitt bei minimaler strahlenexposition des patienten fhren sollen und damit natrlich unmittelbar positive auswirkungen auf den strahlenschutz besitzen . 
 alle diese gesichtspunkte bedeuten mittelfristig eine weitere steigerung des bedarfs an personal in der medizinischen physik und die notwendigkeit zu einer anpassung der dgmp - berichte zum personalbedarf an diese situation . 
10 , empfehlungen zum personalbedarf in der medizinischen strahlenphysik , teil ii : ergnzungen fr spezialtechniken und spezialaufgaben , fulda 1998 , isbn 3 - 925218 - 64 - 5 . 
rat der europischen union : richtlinie 97 / 43 euratom des rates vom 30.6.1997 ber den strahlenschutz von personen gegen die gefahren ionisierender strahlung bei medizinischer exposition und aufhebung der richtlinie 84 / 466 eurato amtsblatt der europischen gemeinschaften l 180 / 26 vom 9.7.1997. 
10 urban & vogel strahlentherapie und onkologie original article stereotactic intensity - modulated radiation therapy ( imrt ) and inverse treatment planning for advanced pleural mesothelioma feasibility and initial results marc w . 
mnter1 , simeon nill2 , christoph thilmann1 , holger hof1 , angelika hss2 , peter hring3 , mike partridge2 , christian manegold4 , michael wannenmacher5 , jrgen debus1 background and purpose : complex - shaped malignant pleural mesotheliomas ( mpms ) with challenging volumes are extremely difficult to treat by conventional radiotherapy due to tolerance doses of the surrounding normal tissue . 
all patients were positioned using noninvasive patient fixation techniques which can be attached to the applied extracranial stereotactic systedue to craniocaudal extension of the tumor , it was necessary to develop a special software attached to the inverse planning program konrad , which can connect two inverse treatment plans and consider the applied dose of the first treatment plan in the area of the matchline of the second treatment plan . 
the presented possibilities of stereotactic imrt in the treatment of mpm will justify the evaluation of imrt in early - stage pleural mesothelioma combined with chemotherapy in a study protocol , in order to improve the outcome of these patients . 
 key words : imrt inverse treatment planning malignant pleural mesothelioma radiotherapy stereotactic strahlenther onkol 2003 ; 179 : 53541 doi 10.1007 / s00066 - 003 - 1055 - 7 stereotaktische intensittsmodulierte strahlentherapie ( imrt ) und inverse bestrahlungsplanung fr fortgeschrittene pleuramesotheliome . 
durchfhrbarkeit und erste ergebnisse hintergrund und ziel : komplex geformte bsartige pleuramesotheliome mit einem ausgedehnten volumen sind aufgrund der toleranzdosen des umgebenden normalgewebes nur sehr schwierig mit hilfe der konventionellen strahlentherapie zu behandeln . 
aufgrund der kraniokaudalen ausdehnung der tumoren war es notwendig , eine spezielle , mit dem inversen planungsprogramm konrad verbundene software zu entwickeln , die zwei unterschiedliche bestrahlungsplne 1 clinical cooperation unit radiation oncology , german cancer research center ( dkfz ) , heidelberg , germany , 2 department of medical physics , german cancer research center ( dkfz ) , heidelberg , germany , 3 department of central dosimetry , german cancer research center ( dkfz ) , heidelberg , germany , 4 department of medical oncology / internal medicine , thoraxklinik heidelberg ggmbh , heidelberg , germany , 5 department of clinical radiology , university of heidelberg , heidelberg , germany . 
des weiteren sollte durch die imrt eine dosiseskalation mglich sein . schlsselwrter : imrt inverse bestrahlungsplanung pleuramesotheliom stereotaktisch strahlentherapie introduction patients and methods diffuse malignant pleural mesothelioma ( mpm ) represents the most common tumor of the pleural cavity . 
pleural mesothelioma has been a rare neoplasm so far , but its incidence is increasing dramatically in most western countries and a peak will be expected around the year 2030 [ 24 ]  . 
 [ 5 ] reported on a study in which patients were divided into groups of treatment and palliative care , and no survival benefit was found in the treatment group . 
external - beam radiation therapy is mainly focused on palliative pain relief and the prevention of tumor seeding into the chest wall following invasive diagnostic procedures by prophylactic treatment of incision sites [ 4 ]  . 
one major problem in escalating the dose for radiation therapy is the large volume when treating the whole mesothelioma and the tolerance doses of the most critical normal structures in close relationship to the pleural cavity . 
 therefore , stereotactic inversely planned intensity - modulated radiation therapy ( imrt ) is used in this feasibility study to treat the complete macroscopic tumor of unresectable mpm in a palliative concept . 
treatment planning was performed by an inverse treatment planning syste patient immobilization and imaging studies the patients were immobilized by noninvasive patient immobilization systems , which can be used for highly conformal radiotherapy . 
either a custom - made body cast extending from the shoulders to the abdomen and a separate head mask both made from scotchcast [ 15 ] or an individual whole body vacuum pillow in combination with a scotchcast mask was used for treatment . 
this immobilization system was attached to the stereotactic head and neck localization systea spiral computed tomography ( ct ) scan of the whole thoracic region with a superior and inferior margin exceeding the macroscopstrahlenther onkol 2003 no . 
stereotactic inversely planned imrt for advanced malignant pleural mesothelioma ically visible tumor of at least 3 cm was performed under shallow breathing , and the slices were reconstructed with a slice thickness of 3 or 5 mboth immobilization setups can be attached to the extracranial stereotaxy systestereotactically guided imrt treatment was performed in all cases . 
 definition of target volumes the target volume and critical structures were defined slice by slice on the treatment planning ct in the three - dimensional ( 3 - d ) conformal radiotherapy planning system virtuos ( dkfz , heidelberg , germany )  . 
an additional margin of 5 mm was added to generate the planning target volume ( ptv )  . in addition , both lungs and further nearby critical structures ( e.g. , esophagus , heart , myelon , liver , stomach ) were also segmented . 
 inverse treatment planning and dose prescription for treatment planning , the konrad inverse planning system ( mrc - systems , heidelberg , germany ) , which is linked to the 3 - d planning program virtuos to calculate and visualize the 3 - d dose distribution , or the corvus ( nomos corp . , usa ) inverse planning system was used . 
 the crucial step in both inverse planning systems is that the physician defines the dose which is applied to the target volume and the dose which may be tolerated by the critical structures . 
in order to find the best balance between the different demands of the target volume and the critical structures , the physician has to perform a trial - and - error approach by changing the parameters of the inverse planning system . the konrad system uses a gradient optimization procedure , while corvus has implemented a simulated annealing procedure . 
besides the dose prescription , the user can select in both planning systems the couch , gantry and collimator angles as well as the number of intensity levels which represent the complexity of the beam modulation . 
a primus linear accelerator ( siemens ) with 6or 15 - mev photons and an integrated motorized multileaf collimator ( mlc ) is used to deliver imrt in a step - and - shoot technique . 
konrad is able to consider the already optimized dose distribution of previous treatment plans . therefore , underor overdosage of the target volume and overdosage of the critical structures can be avoided . 
the 3 - d dose distribution and the dose - volume histogram ( dvh ) of both inversely planned imrt plans can be visualized in one master plan for evaluation . 
the maximum dose to the cervical spinal cord was limited to 45 gy , the maximum dose to the liver to 50 gy , and the maximum dose to the esophagus and heart to 60 gy . 
stereotactic inversely planned imrt for advanced malignant pleural mesothelioma results due to the size of the mesothelioma , five patients were treated with two target points ( figure 1 ) and three patients with one target point . 
therefore , the pure treatment time ranged between 10 and 21 madditionally , approximately 5 min have to be calculated for gantry movement depending on the number of beams and approximately 58 min for patient positioning in the immobilization device and patient positioning to the iso - center . 
the outlined mean volume of the lung affected by the tumor amounted to 887 cm3 ( range : 01 , 251 cm3 ) and that of the healthy lung to 2 , 037 cm3 ( range : 1 , 5112 , 937 cm3 )  . 
the first three patients were treated with a median total dose of 40 gy . afterwards , total dose was escalated to a median total dose of 48 gy in one patient , followed by three patients with a median total dose of 50 gy . 
according to the authors , neither radical surgery nor radiotherapy were effective in respect to the median survival , and only patients who received chemotherapy showed a significantly better median survival as compared with no chemotherapy . 
it should be noted that more than half of the patients presented in the study by ruffie et al . [ 26 ] received no treatment , and the patient groups with combined treatment modalities were rather small . 
nevertheless , a trend was visible , especially in those patient groups receiving radiotherapy as part of the combined treatment approach in terms of a better median survival compared to the group with best supportive care and single - modality therapies . 
due to the fact that singlemodality therapies for mpm , be it radiation therapy , chemotherapy , or surgery , cannot prolong life by more than several months at best , different studies using bior trimodal treatment approaches were performed . 
 however , it should be mentioned that the role of radiotherapy in the treatment of mpm , except for palliative treatment , is , at present , not clearly defined . 
different studies demonstrated that radiation therapy can reduce symptoms like dyspnea , dysphagia , vena cava obstruction , and especially pain in up to two thirds of cases [ 3 , 9 , 10 ]  . 
 when considering definitive radical irradiation in the treatment of mpm , the results are difficult to assess due to the fact that most studies were uncontrolled , presented only small patient numbers and used different staging systems . 
in comparison with conventionally fractionated radiotherapy , the authors evaluated different treatment schedules such as the use of split - course therapy , hypofractionation , hyperfractionation , an additional boost to the major tumor area , or a combination of conventional fractionation and hypofractionation . the authors concluded that the results achieved by the altered fractionation regimes did not differ from those achieved with conventional fractionation , but the 2 - year survival rate was encouraging with 21% . 
the different fractionation schedules were applied to overcome the general problems of radiation therapy in the treatment of mpm , e.g. , the large volume required for treatment of advanced lesions and the total doses needed to control the disease exceeding the tolerance dose of the surrounding critical normal structure , like heart , spinal cord , lungs , liver , and esophagus . 
1 : rechte lunge ; 2 : linke lunge ; 3 : herz ; 4 : rckenmark ; 5 : kraniales ptv ; 6 : kaudales ptv ; 7 : leber . cluded subgroups with no mediastinal nodal involvement and epithelial histology . 
stereotactic inversely planned imrt for advanced malignant pleural mesothelioma treatment technique where the chest wall and parietal pleura were covered by several electron fields in addition to smaller photon fields . 
the authors of the study concluded that the whole pleura could not be treated by rotational electron - field techniques due to the anatomy , especially in the axillary areas and the shoulders . 
moreover , the tolerance doses of the surrounding critical normal structures could be respected , and especially the volume of the contralateral lung which received > 20 gy could be limited as presented . 
the noninvasive patient immobilization systems used allow a high repositioning accuracy as already described [ 15 , 25 , 33 ] and therefore guarantee , together with the stereotactic definition of the target point , a high quality of treatment . 
stereotactic inversely planned imrt could be interesting especially for patients with favorable prognostic factors such as imig stages i and ii , age < 50 years , female sex , and epithelial type [ 11 ]  . one possible study protocol might be an integrated imrt boost concept [ 32 ] with the treatment of the whole ipsilateral pleural space applying a higher daily dose to the grossly visible tumor in the same fraction . 
 strahlentherapie und onkologie original article tumor volume and tumor hypoxia in head and neck cancers the amount of the hypoxic volume is important jrgen dunst1 , peter stadler2 , axel becker1 , christine lautenschlger3 , tanja pelz1 , gabriele hnsgen1 , michael molls2 , thomas kuhnt1 background : the prognostic impact of tumor volume and hypoxia is well established . 
we have investigated a possible prognostic impact of the hypoxic tumor volume which can be calculated as the product of tumor volume and hypoxia . patients and methods : 125 patients with squamous cell cancer of the head and neck were investigated . 
the total tumor volume was calculated from pretreatment ct scans as the sum of all visible macroscopic tumor lesions ( e.g. , primary tumor plus neck nodes ) , and all patients underwent measurement of tumor oxygenation by po2 histography . the hypoxic tumor volume was calculated as the product of the total tumor volume and the relative frequency of po2 readings < 5 mmhg . 
the nonhypoxic volume was the difference between total tumor volume and hypoxic volume . results : the total tumor volume ranged from 2 to 283 cm3 ( mean 47 53 cm3 ) , the hypoxic volume from 0 to 199 cm3 ( mean 18 30 cm3 ) , and the nonhypoxic volume from 1 to 237 cm3 ( mean 29 34 cm3 ) , and there was a strong correlation between the three parameters . 
as a consequence , methods to measure and localize the hypoxic volume should be further developed . key words : head and neck cancer tumor volume hypoxia prognosis strahlenther onkol 2003 ; 179 : 5216 doi 10.1007 / s00066 - 003 - 1066 - 4 tumorvolumen und hypoxie in kopf - hals - tumoren . 
bei allen patienten wurden der oxygenierungsstatus des tumors durch po2 - histographie bestimmt und das absolute hypoxische volumen als produkt von tumorvolumen und relativem anteil von po2 - messungen < 5 mmhg berechnet . 
 ergebnisse : das gesamte tumorvolumen betrug 2283 cm3 ( im mittel 47 53 cm3 ) , das hypoxische volumen 0199 cm3 ( im mittel 18 30 cm3 ) und das nichthypoxische volumen 1237 cm3 ( im mittel 29 34 cm3 )  . 
84 patienten verstarben im nachbeobachtungszeitraum , und 41 berlebten ; die mediane berlebenszeit 1department of radiotherapy , martin luther university halle - wittenberg , germany , 2department of radiotherapy , technical university of munich , germany , 3department of medical biometry , martin luther university halle - wittenberg , germany . received : july 8 , 2002 ; accepted : may 6 , 2003 strahlenther onkol 2003 no . 
 schlsselwrter : kopf - hals - tumoren tumorvolumen hypoxie prognose introduction the prognostic impact of tumor volume in patients undergoing radiotherapy is well established [ 1 , 4 , 6 , 8 , 9 , 13 , 15 , 22 ]  . 
for example , a tumor with 109 clonogenic cells ( corresponding to about 25 cm diameter ) and a homogeneous radiosensitivity with an sf2 of 50% can be cured with nearly 100% chance using standard radiation doses in the range of 6070 gy . 
the hypoxic volume can be calculated from the total volume and the oxygenation status of a tumor . in this report , we want to demonstrate that the hypoxic volume is a stronger predictor of survival than the total tumor volume . 
 tumor oxygenation measurements tumor volumes the total tumor volume ranged from 2 to 283 cm3 , the hypoxic volume from 0 to 199 cm3 , and the nonhypoxic volume from 1 to 237 cm3 ( table 2 )  . 
 total tumor volume hypoxic tumor nonhypoxic tumor volume volume mean sd ( cm3 ) range ( cm3 ) median ( cm3 ) 47 53 2283 32.0 18 30 0199 29 34 1237 17.6 dunst j , et al . 
all macroscopically visible tumor sites including primary tumor and neck nodes were identified , and the volumes of all sites were calculated with the ellipsoid formula ( volume = 1 / 6 ( cid : 1 ) ( cid : 1 ) a ( cid : 1 ) b ( cid : 1 ) c , with a , b , and c being the largest diameters in three dimensions )  . 
 the hypoxic tumor volume was calculated as the product of the total tumor volume and the relative frequency of hypoxic readings ( < 5 mmhg ) in the po2 histography as described recently [ 17 ]  . 
 to further analyze the impact of the different types of tumor volume , the patients were divided into subgroups depending on whether or not their tumor volumes ( total tumor volume , hypoxic and nonhypoxic volume ) were below or table 4 . 
the low impact of the nonhypoxic volume was also demonstrated by the fact that patients with a larger nonhypoxic volume had a median survival slightly above the survival of patients with a small nonhypoxic volume . 
 in a multivariate cox regression model including total tumor tolume , hypoxic and nonhypoxic volume , the hypoxic volume was the strongest prognostic factor and more important than the total tumor volume ( table 5 )  . 
various clinical investigations have demonstrated that hypoxic cancers have a worse prognosis as compared to better oxygenated tumors [ 5 , 9 , 10 , 12 , 1416 ]  . 
this was also be expected from the data in the literature , because hypoxia is , besides tumor volume , a further independent prognostic factor , and hypoxia was found not to be size - dependent in all investigations [ 5 , 9 , 10 , 14 , 16 ]  . 
 a recent analysis in cervix cancer has suggested that tumor volume and hypoxia are independent prognostic factors and that the hypoxic volume adds few , if any , information as compared to the total tumor volume [ 9 ]  . 
according to our findings , this can be explained by the strong correlation between the total tumor volume and the hypoxic volume . we have distinguished the hypoxic volume from the nonhypoxic volume . 
according to these data , the preferential information should be obtained for the hypoxic volume , and the prognostic impact of the total tumor volume might be explained by the strong correlation with the hypoxic volume . 
first , we have measured the oxygenation only in one lesion in each patient ( mainly in neck nodes ) , but calculated the tumor volume from all lesions ( primary tumor plus nodes )  . 
however , these limitations cannot be completely ruled out for technical and ethical reasons , and we assume that they do not limit the basic hypothesis which we have generated from our data . 
tumors with a high percentage of poorly perfused areas on gd - enhanced t1 - weighted mr images had a significantly higher frequency of metastatic spread at diagnosis as compared to tumors with a small amount of poorly perfused areas [ 7 ]  . 
it seems useful not only to measure the tumor volume but to develop methods to measure the hypoxic volume . currently , various techniques to detect hypoxia are under clinical investigation . 
these include , besides po2 histography , pathohistologic methods with hypoxia - binding markers like pimonidazole or ef5 , spectroscopy , perfusion studies or positron emission tomography ( pet )  . 
according to our results , further efforts should be undertaken to develop methods that not only measure the relative distribution of hypoxia , but exactly quantify the amount of hypoxia . 
 strahlentherapie und onkologie original article optimization of dose distributions for adjuvant locoregional radiotherapy of gastric cancer by imrt frank lohr , barbara dobler , sabine mai , brigitte hermann , uta tiefenbacher , petra wieland , volker steil , frederik wenz1 background and purpose : locoregional relapse is a problem frequently encountered with advanced gastric cancer . 
the potential of intensity - modulated radiotherapy ( imrt ) to reduce toxicity by significantly reducing maximum and median doses to organs at risk while still applying sufficient dose to the target volume in the upper abdomen was studied . patient and methods : for a typical configuration of target volumes and organs , a step - and - shoot imrt plan ( eight beam orientations ) , developed as a class solution for treatment of tumors in the upper abdomen ( figures 1 to 3 ) , a conventional plan , a combination of the conventional plan with a kidney - sparing boost plan , and a conventional plan with noncoplanar ap and pa fields for improved kidney sparing were compared with respect to coverage of target volume and dose to organs at risk with a dose of 45 gy delivered as the median dose to the target volume . 
liver was spared better with imrt . dose to the lungs was not significantly different , and dose to the spinal cord was higher ( but well below tolerance ) with imrt . the dose distribution within the target volume was less homogeneous than for the conventional plans . 
 conclusion : imrt has the potential to deliver efficient doses to target volumes in the upper abdomen , while delivering dose to organs at risk in a more advantageous fashion than a conventional technique . 
 key words : gastric cancer adjuvant radiochemotherapy intensity - modulated radiotherapy imrt strahlenther onkol 2003 ; 179 : 55763 doi 10.1007 / s00066 - 003 - 1087 - z optimierung der dosisverteilung bei der adjuvanten bestrahlung des magenkarzinoms mit imrt hintergrund und ziel : die adjuvante therapie des fortgeschrittenen magenkarzinoms wird kontrovers diskutiert . 
es wurde daher versucht , durch einsatz der intensittsmodulierten strahlentherapie ( imrt ) bei einem typischen zielvolumen im oberbauch die mediane und maximale risikoorganbelastung bei vergleichbarer zielvolumenabdeckung zu reduzieren . patient und methodik : fr eine typische konfiguration von zielvolumen und risikoorganen wurden eine als class solution entwickelte acht - felder - imrt - technik ( abbildungen 1 bis 3 ) , ein konventioneller plan , eine kombination dieses konventionellen plans mit einem nierenschonenden boostplan und ein konventioneller plan mit nonkoplanarer ausrichtung von a.p. 
feld zur besseren nierenschonung hinsichtlich zielvolumeneinfassung und belastung der risikoorgane verglichen . ergebnisse : mit konventionellen techniken konnte zwar die rechte niere ausreichend geschont werden , die linke niere wurde jedoch je nach plan mit einer medianen dosis zwischen 14 , 8 und 26 , 9 gy belastet . 
die dosisverteilung im zielvolumen war bei imrt inhomogener , auch mittels imrt konnten zuverlssig > 90% der verschreibungsdosis auf > 90% des zielvolumens appliziert werden ( tabelle 1 )  . 
 1 department of radiation oncology , mannheim medical center , university of heidelberg , germany . received : august 22 , 2002 ; accepted : january 17 , 2003 strahlenther onkol 2003 no . 
imrt for gastric cancer schlussfolgerung : imrt moduliert die belastung der risikoorgane im oberbauch gegenber einer konventionell 3 - d - geplanten technik gnstiger , sodass ausschpfung und einhaltung der organtoleranzen erleichtert werden . 
bei der klinischen implementierung muss die besondere mobilitt der oberbauchorgane bei der planung und der patientenpositionierung bercksichtigt werden . die zahlreichen technischen und biologischen unwgbarkeiten der anwendung der imrt insbesondere in dieser region erfordern die vorsichtige implementierung , langfristige nachbeobachtung und weitere untersuchungen . 
with locoregional relapse amounting to 3050% in total numbers and to 1520% as the only manifestation of recurrent disease , the need for an efficient adjuvant strategy is undisputed [ 8 , 9 ]  . 
until recently , however , sound evidence was lacking that adjuvant therapy can indeed improve the dire prognosis of patients with advanced disease . neither perioperative chemotherapy nor radiotherapy alone were able to unequivocally improve results . 
 toxicity of this approach , however , is high [ 11 , 12 ] , since the extension of the target volume has to be large , as it is suggested by pattern of relapse analyses [ 8 , 9 ]  . 
usually , the complete stomach bed , the left diaphragm and the lymph nodes around the stomach , the splenic artery and the hepatic artery in the hepatoduodenal ligament as well as the paraaortal and paracaval lymph nodes are considered to be at risk of relapse [ 5 , 17 ]  . 
the resulting target volume is therefore large and multiconcave and can very often not be irradiated in its entity to what is considered a sufficient dose of approximately 45 gy ( though the dose at the isocenter may well be 45 gy ) because of the fear of potential kidney and occasionally also liver damage . 
 intensity - modulated radiotherapy ( imrt ) might be a way around these problems , although it is also fraught with a multitude of problems and caveats that have to be studied and solved . 
 patient and methods the patient treated as presented was a 40 - year - old woman who had undergone total gastrectomy for a t2 n1 gastric adenocarcinoma located at the gastric antrum with 6 / 16 positive nodes found at both curvatures . 
 [ 11 ] on an outpatient basis . target volume was defined in accordance with the requirements of intergroup 116 [ 11 ] , with all volumes being defined as planning target volumes ( ptvs )  . 
for logistic reasons , treatment of this particular patient was begun with a conventional three - dimensional ( 3 - d ) four - field box technique first and then continued with the presented imrt technique . 
for plan comparison , four plans or plan combinations were chosen , and evaluation was performed for a total dose of 45 gy delivered as the median dose to the target volume for each plan or plan combination . 
dose calculation for both planning systems is based on a pencil - beam algorith conventional treatment ( 23 mv ) and imrt ( 6 mv ) were planned for and performed with a siemens kd2 linac fitted with the siemens automatic multileaf collimator ( leaf width 1 cm at isocenter ) controlled by primeview software . 
dose distribution was intended to be homogeneous within the target volume . dose - volume constraints were chosen as depicted in figure 1 . basic beam geometry comprised eight fields , six of which where applied in a basically equispaced coplanar fashion with small alternating table angles to further dilute dose deposition outside the target . 
a satisfactory compromise between treatment time and target - dose homogeneity was achieved by delivering the intensity matrices for each beam angle discretized into three intensity steps strahlenther onkol 2003 no . 
once the class solution is created , actual treatment planning for any new patient takes only two or three planning runs to further adjust the parameters which amounts to a total hands on time of the planner of < 1 h , total time for planning very much depending on the optimization software . 
proper patient positioning was assured by frequent isocenter checks with port films as well as port films taken for one beam angle at a time during treatment that allows verification of the position of the intensity matrix with respect to anatomy . 
 for plan comparison , four plans were chosen , and evaluation was performed for a total dose of 45 gy delivered as median dose to the target volume for each plan or plan combination : first , the imrt plan as described above ; second , a conventional four - field box technique ; third , the conventional four - field box technique combined with a kidney - sparing boost technique ( opposing laterals at level of kidneys , four - field box elsewhere ) after reaching 16.2 gy ; fourth , a conventional four - field box technique with the ap and pa beams delivered at 90 table angle and 325 / 145 gantry angle to better spare the caudal part of the kidneys . 
for comparison reasons , dose was prescribed as the median dose to target volume , because this prescription modus conforms best with prescription philosophy of icru 50 and therefore facilitates comparison of homogeneous plans with inhomogeneous plans such as the ones created by imrt . median dose to target has been chosen for postulated correlation of median dose with tumor cure probability [ 19 ] the results of the study this claim is based on [ 10 ] are , however , probably artifactual , since organ motion was small in this study when compared to safety margmedian dose to the ptv in this study therefore rather resembled minimum dose to the actual tumor volume . 
 verification of the imrt plan was performed based on the recently published procedures as devised by the german cancer research center ( deutsches krebsforschungszentrum , dkfz ) , heidelberg [ 15 ]  . 
 results figures 3a and 3b show the dose distribution for the imrt ( figure 3a ) and the coplanar conventional 3 - d plan ( figure 3b ) in all three planes as well as the respective dose - volume histograms ( dvh )  . 
imrt for gastric cancer clinically relevant plan parameters ( median and partial volume doses to target , kidneys , liver , lungs , and spinal cord ) are reported in a comprehensive and detailed fashion in table 1 . 
doses are reported as if each plan ( or in one case the figure 3a abbildung 3a combination of two plans ) were irradiated up to a total dose of 45 gy as the median dose to the target volume . 
for the same reason , small bowel is not specified , since a relevant part of it is situated within the target volume and therefore target doses can be assumed to apply to a relevant fraction of small bowel as well . 
while the conventional techniques irradiate spinal cord only to doses of 2530 gy , imrt offers the possibility to apply higher doses ( nevertheless well below tolerance ) thereby reducing dose to the kidneys . 
with conventional techniques , the majority of the left kidney would have been functionally ablated with parts of the right kidney still reaching a dose of 15 gy , the upper limit of what can be considered safe . 
 the liver , which especially poses a problem when it is small in comparison to the target as in our case , was exposed to significantly lower doses with imrt than with any of the other techniques . 
 discussion if the initial treatment method for any given tumor system yields superb results or a moderate percentage of treatment failures can be salvaged , a major change in primary treatment is not indicated . such a situation does not exist for carcinoma of the stomach . 
clinically relevant plan parameters ( median and partial volume doses to target and organs at risk ) for each plan ( or in one case the combination of two plans ) delivered to a total dose of 45 gy as median dose to target volume . 
the gitsg radiochemotherapy series in patients with minimal residual disease [ 16 ] as well as the swog - initiated randomized trial 9008 / intergroup 116 [ 11 ] in the adjuvant situation provided a proof of principle of the beneficial effects of radiochemotherapy . 
 as impressively shown above , imrt can distribute the dose outside the target volume in a more advantageous fashion for a target that is presumed immobile , especially when as to some extent in the presented case the position of the kidneys interferes with adequate target volume coverage . 
this is possible not only with 23 mv but also with 6 mv when , as in our case , patient diameter is sufficiently small and enough beam angles are used [ 14 ]  . 
while with the conventional techniques one kidney is more or less sacrificed , with imrt the dose can be modulated in a fashion to stay within the tolerance confines for both kidneys . 
for other cases with a more problematic geometry this will get even clearer , when the target volume is defined without preemptively taking into account the limitations of conventional treatment planning , something that is often done in clinical practice . 
 as for most procedures with impressive upsides , several issues may represent significant downsides of the concept ( in addition to already widely discussed economical problems related to the implementation of a complex technique in times of scarce resources )  . 
it is the very nature of imrt as of any other technique with a high number of portals to increase the body volume that is exposed to low doses , but it is a specific feature of inverse treatment planning to increase the dose inhomogeneity within the target volume to improve a dose distribution that is highly conformal to the target . 
the significance of minute dose spikes like these in different normal tissues is not yet known ( certainly negligible in parallel organs like the liver , more relevant in predominantly serial organs like the spinal cord , simply unknown in the small bowel ) and , again , has to be the subject of further studies . 
are tolerance doses comparable if , say , only the papillae but all of them are irradiated to high doses ? or , on a different note : the spinal cord is certainly a serial organ when the whole axial plane is irradiated . 
how does it behave , if only parts of its axial plane are irradiated ? is only the function of , for example , the anterior tractus impaired ? are tolerance doses the same ? all this has to be answered , and one of the merits of precise patient positioning and highly conformal irradiation is the opportunity to gather data that finally answer these questions . 
 the other obvious problem is target and organ motion not only between fractions as , for example , in prostate cancer [ 1 ] ( the effects of which are no different from a conventionally created highly conformal 3 - d dose distribution ) but also during a single fraction . 
in reality , however , during a course of fractionated radiotherapy this kind of error only seems to result in reduced gradient steepness and in a reduction of magnitude of maxima of the intensity matrix for a given beam angle . 
 exact patient positioning by port films , electronic portal imaging , or better for soft tissue targets like the prostate or the upper abdominal area that may be represented by the celiac trunk ct as well as ultrasound on - table imaging is as crucial for imrt as for conventional 3 - d techniques . 
given the sometimes to some respect even potentially beneficial effects of minimal random patient movement ( as discussed above ) , more elaborate technical concepts for patient immobilization like breathing control or even target tracking may be of no greater importance for imrt than for a conventional 3 - d treatment . 
 there are , in addition , more general concerns inherent to imrt , that were recently summed up by goffman & glatstein [ 7 ] : as mentioned above , exposure of large body regions is higher with imrt than with conventional conformal radiotherapy . 
this is an issue certainly to be kept in mind when treating children or younger adults with a favorable perspective on cure , as it had to be learned from hodgkins disease . for patients suffering from advanced stomach cancer with overall relapse rates in excess of 40% , this problem runs a distant second to the problem of actually curing the disease in the first place . 
therefore , with further evolution of the planning systems optimization process and further automatization of treatment delivery ( e.g. , external steering of the table ) , treatment time will probably be reduced but will still exceed 15 min . this long treatment time has caused concern that by pulsing the actual dose delivery , as it is the principle of step - and - shoot imrt , the biological effectiveness toward the tumor might be reduced . 
while this can be modeled in vitro to a certain extent something that has to be and actually is currently done [ 18 ] , only time will finally tell if this is really of concern except for a subset of histologies such as melanoma . 
 conclusion for postoperative radiotherapy of advanced gastric cancer , imrt with eight beam orientations and three intensity steps has the potential to deliver efficient doses to target volumes while delivering dose to organs at risk in a more advantageous fashion when compared to a conventional technique . 
the method has to be carefully implemented , and the multitude of potential risks related to its application has to be the subject of thorough follow - up and further studies , although most of the currently discussed more general concerns may not be too relevant to patients with advanced gastric cancer . 
 strahlentherapie und onkologie review article current and future strategies in radiotherapy of childhood low - grade glioma of the brain part i : treatment modalities of radiation therapy rolf - dieter kortmann1 , beate timmermann1 , roger e . 
gnekow4 , karin dieckmann5 , sylvia kay1 , michael bamberg1 background : treatment of childhood low - grade gliomas is a challenging issue owing to their low incidence and the lack of consensus about optimal treatment approach . material and methods : reports in the literature spanning 60 years of radiation therapy , including orthovoltage , megavoltage and recently modern high - precision treatments , were reviewed with respect to visual function , survival , prognostic factors , dose prescriptions , target volumes , and treatment techniques . 
based on these experiences , future strategies in the management of childhood low - grade glioma are presented . results : evaluation of published reports is difficult because of inconsistencies in data presentation , relatively short follow - up in some series and failure to present findings and results in a comparable way . 
even with the shortcomings of the reports available in the literature , primarily concerning indications , age at treatment , dose response , timing and use of optimal treatment fields , radiation therapy continues to play an important role in the management of these tumors achieving long - term survival rates up to 80% or more . 
recent advances in treatment techniques , such as 3 - d treatment planning and various high - precision treatments achieved promising initial outcome , however with limited patient numbers and short follow - ups . 
 conclusions : radiation therapy is an effective treatment modality in children with low - grade glioma regarding tumor control and improvement and / or preservation of neurologic function or vision , respectively . 
more prospective studies are needed to address the impact of modern radiation therapy technologies ( including intensity - modulated radiotherapy ) on outcome especially in the very young and to define the role of radiation therapy as a part of a comprehensive treatment approach . 
 key words : low - grade glioma children radiation therapy surgery strahlenther onkol 2003 ; 179 : 50920 doi 10.1007 / s00066 - 003 - 9104 - 9 aktuelle und zuknftige strategien bei der bestrahlung von niedrigmalignen gliomen des gehirns im kindesalter . 
 teil i : strahlentherapeutische behandlungsmodalitten hintergrund : die behandlung maligner gliome im kindesalter ist wegen deren geringer hufigkeit und kontroversen ber optimale behandlungsstrategien eine herausforderung an den radioonkologen . material und methodik : es wurden berichte in der literatur , die 60 jahre strahlentherapie von orthovoltsowie megavolttechniken bis zu den heute modernen przisionstechniken umfassen , analysiert . 
basierend auf diesen erfahrungen werden zuknftige strategien bei der behandlung niedrigmaligner gliome im kindesalter vorgelegt . ergebnisse : die evaluierung publizierter berichte ist aufgrund heterogener aufarbeitung der daten , teilweise kurzer nachbeobachtungszeitrume und fehlender darstellung der ergebnisse in vergleichbarer form erschwert . 
trotz begrenzter aussagekraft der literaturangaben , die in erster linie die indikationen , das behandlungsalter , dosis - wirkungs - beziehungen , den zeitpunkt der bestrahlung und die anwendung optimaler bestrahlungsfelder betreffen , spielt die strahlentherapie unverndert eine wichtige rol1 department of radiooncology , university of tbingen , germany , 2 radiotherapy department , cookridge hospital , leeds , united kingdom , 3 department of radiotherapy , padua general hospital , italy , 4 childrens hospital , augsburg , germany , 5 department of radiooncology , general hospital vienna , austria . 
aktuelle fortschritte bei bestrahlungstechniken wie 3 - dbestrahlungplanung und unterschiedlichen hochprzisionstechniken erreichten viel versprechende klinische ergebnisse bei jedoch begrenzten patientenzahlen und kurzen nachbeobachtungszeitrumen . schlussfolgerungen : die strahlentherapie ist eine effektive behandlungsmodalitt bei kindern mit niedrigmalignen gliomen hinsichtlich tumorkontrolle und verbesserung oder erhalt neurologischer funktionen oder des sehvermgens . 
prospektive studien , die die bedeutung moderner bestrahlungstechniken ( unter einschluss intensittsmodulierter bestrahlung ) fr das klinische ergebnis , besonders bei kleinen kindern , beinhalten , sind notwendig , um den stellenwert der strahlentherapie innerhalb eines umfassenden behandlungskonzeptes zu untersuchen . 
their biological behavior varies greatly : even small chiasmatic tumors may display an aggressive , malignant growth pattern causing rapid visual deterioration , progressive neurologic deficits and diencephalic syndrome , whereas larger tumors may remain quiescent for years . 
 recent advances in neurosurgery , radiation techniques and the introduction of chemotherapy have opened up new possibilities but have also introduced controversies in the optimal management of childhood low - grade gliomas . 
numerous reports addressed these questions favoring one or another approach , identified possible prognostic factors and suggested optimal treatment approach based on these factors [ 3 , 5 , 8 , 1418 , 3133 , 35 , 36 , 40 , 5255 , 57 , 74 , 76 , 77 ]  . 
 this review is , therefore , undertaken to offer better insight in the radiotherapy treatment parameters and treatment outcome , while the second part of this review will focus on radiotherapy - related toxicity . 
 hemispheric gliomas low - grade gliomas of the cerebral hemispheres in children generally carry an excellent long - time prognosis , because disease progression is rarely observed after complete resection [ 16 , 18 , 55 , 68 ]  . 
 [ 55 ] observed no disease progression in 21 patients who underwent a complete tumor resection , compared to two of twelve ( 17% ) undergoing nearly complete resections and eleven of 37 ( 30% ) undergoing subtotal resections . 
in an analysis of 51 patients with supratentorial pilocytic astrocytoma , for 16 patients undergoing complete resection the 10 - year survival rate was 100% , while it was 74% for 35 patients who had subtotal removal or biopsy [ 18 ]  . 
complete surgical resection , as judged by postoperative neuroimaging and operative record , appears possible in 8490% of all patients [ 21 ]  . extended periods of stable disease , and sporadic cases of tumor regression , following partial resection are reported for small numbers of patients [ 10 , 27 , 61 ]  . 
however , for the majority of cases residual tumor tends to progress over long periods of time , mostly within 45 years after initial operation , and progression - free survival rates are between 2980% and 079% at 5 and 10 years [ 10 , 24 , 27 , 61 , 64 ]  . 
numerous reports over the years consistently support the high efficacy ( 90% ) of radiotherapy in stabilization and improvement of visual function [ 3 , 6 , 8 , 11 , 14 , 17 , 3133 , 37 , 52 , 54 , 57 , 69 , 70 , 76 , 77 ] ( table 1 )  . 
however , the comparisons are biased because a conservative approach without treatment can be assumed in the majority of patients with clinically stable tumors , whereas the proportion of patients with progressive tumors will probably be higher in the cohort undergoing radiotherapy . 
 author total dosea improved taveras et al . , 1956 [ 70 ] 815 gy montgomery et al . , 1977 [ 52 ] hoyt & baghdassarian , 1969 [ 33 ] 28 3565 gy ( allmost all 50 gy )  . 
radiotherapy of childhood low - grade glioma part i was 85% for 33 patients with tumors of the optic nerve , compared to 44% in 52 patients with tumors involving the optic chiasalmost all patients ( 93% ) with chiasmal tumors died of tumor progression . 
posttreatment progression over 15 years was not observed in patients with tumors confined to the optic nerve , but was noted in five patients ( 14% ) with chiasmal tumors , and in 14 patients ( 43% ) with chiasmal lesions with invasion of the adjacent midbrasurvival rates at 5 , 10 , and 15 years were 94% , 81% , and 74% , respectively , and corresponding progression - free survival rates were 85% , 75% , and 75% , respectively . 
the 5 - , 10 - , and 15 - year progression - free survival rates for the nf patients were 90% , 70% , and 70% , respectively , as compared to 76% for all time intervals for the nf - negative cohort without finding a statistical difference . 
 [ 36 ] compared 38 nf patients with 49 patients without nf and found a statistically significant difference in relapse - free survival rates in favor of nf patients ( 89% , 89% , and 84% at 5 , 10 , and 15 years , respectively ) as compared to nf - negative patients ( 56% , 50% , and 47% , respectively )  . 
 [ 3 ] , patients with neurologic signs at time of treatment achieved poorer survival rates : 57% versus 92% in the absence of neurologic signs at 5 and 10 years , respectively . 
for patients 10 years of age at the time of radiotherapy , a 10 - year progression - free survival of 51% was found as compared to 91% for patients > 10 years . 
other possible prognostic factors such as presence of hydrocephalus and extent of resection could not be confirmed in unior multivariate analysis in series of other authors [ 31 , 36 , 45 ]  . 
 timing of postoperative radiotherapy several retrospective studies have indicated an advantage for immediate postoperative radiotherapy regarding overall survival and progression - free survival in adults [ 23 , 62 , 63 ] , although there are opposite observations [ 30 ]  . 
48 patients received immediate postoperative irradiation after incomplete resection and twelve ( 25% ) relapsed , whereas the rate of tumor progression among 55 patients in whom radiotherapy was deferred was 42% . 
however , as noted in adults , the results were not translated into overall survival with rates at 5 and 10 years of 81% / 73% versus 87% / 83% for those patients not receiving immediate radiotherapy . 
107 out of 142 children with tumors of all sites were observed , while 31 patients received radiotherapy and four chemotherapy ( they were < 5 years of age ) , respectively , when showing progressive disease . 
the progression - free survival and overall survival rates of all patients were 70% and 90% , respectively , whereas the overall survival rate was only 65% at 4 years in children after treatment for progressive disease . 
 [ 69 ] , the policy to treat with radiation therapy as determined by clinical progression or increase in tumor size on imaging achieved a better result with a 15 - year progression - free survival rate of 82.1% and overall survival rate of 85.1%. 
preliminary data in 96 patients show that a 3 - year progression - free survival rate of 87.1% and an overall survival rate of 95.7% can be obtained by radiotherapy at a median follow - up of 90 months complete incomplete resection biopsy clinical diagnosis / imaging symptoms / progress nonsurgical treatment < 5 years 5 years progression figure 1 . 
 dose - response effects the optimum dose for radiation therapy in childhood lowgrade glioma has not been well established [ 1 , 17 , 25 , 31 , 36 , strahlenther onkol 2003 no . 
retrospective analyses are rare , comprising small patient numbers and very heterogeneous dose prescriptions . additionally , it can be assumed that the selection of dose prescriptions was strongly influenced by patient age , extent and site of tumor with a tendency to a lower dose in younger children with larger tumors ( larger treatment portals ) , and consequently , the reported results were conflicting . 
although it is difficult to define an adequate dose prescription , the recently recommended and generally accepted dose prescription ranges between 45 and 54 gy in 1.8 - gy fractions depending on age at treatment , extent of disease , and location of tumor . 
 tumor volume response to radiation author radiographically determined response of optic gliomas to radiotherapy has not been well documented , because it has been assumed that low - grade gliomas in children are indolent and unresponsive to radiotherapy . 
 [ 15 ] of 80 patients with a low - grade glioma , 19 patients with residual macroscopic lesions who received radiation therapy were selected for volumetric analysis of tumor response to treatment . 
it took a median time of 62 months until maximal response in terms of a partial remission ( in 24% of cases ) and a complete remission ( 16% ) , which was in sharp contrast to the rapid clinical response . 
 treatment fields in childhood low - grade gliomas , local failure is the predominant feature in progressive or recurrent disease , and leptomeningeal spread is a rare event ( < 5% ) [ 56 ]  . 
the clinical target volume ( ctv ) included the visible tumor in ct and mri plus 5 mm , the planning target volume ( ptv ) consisted of the ctv plus 2 mm safety margno treatment failure was observed suggesting that limiting the high - dose volume did not cause an increase in marginal or out - of - field failure rate . 
 new approaches in radiotherapy stereotactic radiotherapy stereotactic irradiation techniques in conjunction with rigid head fixation systems comprising single high - dose delivery ( radiosurgery ) , fractionated convergence therapy , and fractionated 3 - d conformal therapy are well established in adults , but data for childhood central nervous system malignancies , in particular low - grade glioma , are scarce . 
preliminary data reveal low acute toxicity and promising results in recurrent tumors as well as in primary treatment [ 2 , 4 , 9 , 12 , 19 , 22 , 29 , 34 , 47 , 65 , 66 ]  . 
since survival rates have correlated with the degree of resection suggesting the necessity for radical local treatment [ 18 , 55 ] , longterm outcome might be improved if radiosurgery can convert a subtotal excision to a complete excision . 
application may be restricted to selected hemispheric lesions < 5 cm in order to limit the risk for serious morbidity due to increasing dose inhomogeneity combined with an increased exposure of normal brain to high doses . 
 [ 29 ] investigated the role of radiosurgery in a series of 25 children , 13 of whom had pilocytic and low - grade astrocytomas ( table 3 )  . 
during a median follow - up of 21 months , eleven of the 13 children with benign glial neoplasms had tumor control , and all of them have remained alive . 
in one child a complete remission on imaging could be obtained , four showed a reduction in size , three were stable at a mean follow - up of 21 months . 
since patients treated in these series represent a very inhomogeneous cohort , due to often slow growth rates of low - grade glioma and possible late toxicity , it is necessary to evaluate a much longer follow - up , before a definite conclusion regarding the role of radiosurgery will be reached . 
clinical and radiologic improvement was achieved in all patients , as well as an almost complete remission in two patients at a follow - up between 5 and 47 months . 
 [ 60 ] treated 14 children and achieved a 3 - year local progression - free survival and overall survival rate of 87% and 100% , respectively , compared with 89% and 98% for a historic control treated with conventional radiotherapy . 
 proton therapy the major advantage of proton therapy over conventional radiation techniques is the high degree of dose conformity around the tumor that can be achieved , since protons have no exit dose beyond the target . 
by anatomic sites , these data translated into rates of local control and survival of 87% / 93% for midline tumors , 71% / 86% for hemispheric tumors , and 60% / 60% for brain stem tumors . 
the 5and 10year survival rates in 97 patients with pilocytic astrocytoma were 85% and 83% and in patients with who grade ii astrocytomas ( 250 patients ) 61% and 51% , respectively . 
there are very few cases in the literature in which reirradiation was performed , the major demand being a sparing of normal tissue thus requiring a precise and focused radiotherapy . 
 [ 29 ] treated one child using radiosurgery at a reduced dose of 12 gy to the tumor margdespite treatment , tumor progression continued and was evident on imaging 6 months after therapy . 
in the report of weiss et al . [ 76 ] , one patient was reirradiated 8 years after primary treatment because of recurrent disease at a dose prescription of 30 gy given in 3 weeks . 
 [ 51 ] reported the case of a 6 - year - old boy who underwent surgery followed by radiotherapy of the affected regions of the brain and spinal canal . 
the role of surgery in gliomas of the visual pathway has to be seen in the light of preservation of neurologic and visual function and is therefore limited to biopsy in the majority of cases to obtain histologic confirmation [ 26 , 48 , 68 ]  . 
 the timing of postoperative radiotherapy in childhood hemispheric and cerebellar low - grade glioma now appears clearer following a report from the eortc study in adults showing that an improvement in progression - free but not overall survival is obtained after immediate postoperative radiotherapy [ 39 ] , a fact which can also be seen in children [ 16 ]  . however , a reliable identification of prognostic factors supporting the use of immediate postoperative radiotherapy is still lacking for children [ 16 ]  . 
radiotherapy of childhood low - grade glioma part i presently , it is recommended to employ radiotherapy for patients with progressive disease only , regardless of tumor location [ 16 , 26 , 48 ]  . 
in some series , nf appears to be associated with a better survival and a better response rate to radiotherapy as compared to the absence of nf [ 6 , 31 , 35 , 36 , 45 ]  . although data for a clear dose - response relationship are lacking , there is consent today to apply total doses between 45 and 54 gy ( 1.8 gy fractionated dose ) depending on the location and extent of tumors as well as age at treatment [ 1 , 17 , 31 , 32 , 52 ]  . 
low - grade gliomas in children can demonstrate shrinkage on radiographic studies in response on radiotherapy , but such shrinkage is not directly related to tumor control or improvement of symptoms . 
it can be concluded that normal tissue sparing through the use of advanced radiation therapy treatment planning and delivery techniques should be beneficial to pediatric patients if the rate and patterns of failure are similar to conventional techniques at a longer follow - up . 
possibly , the recent advances in intensity - modulated radiotherapy will be able to achieve a similar dose conformity even in larger tumors . brachytherapy might be a useful alternative , but is applicable only in selected tumors [ 46 ]  . 
reirradiation might be feasible in selected cases by using modern treatment techniques [ 1 , 55 , 76 ]  . the role of radiation therapy in disseminated low - grade glioma is largely unknown and mandates further investigations [ 51 , 56 ]  . today , prospective trials in childhood brain tumors are indispensable to assess the role of radiotherapy both in terms of survival and late effects [ 43 , 59 , 72 ]  . 
 strahlentherapie und onkologie original article a little to a lot or a lot to a little ? an analysis of pneumonitis risk from dose - volume histogram parameters of the lung in patients with lung cancer treated with 3 - d conformal radiotherapy jochen willner , andre jost , kurt baier , michael flentje1 purpose : to determine whether a little dose to a large normal lung volume or a high dose to a small lung volume is more critical for induction of clinical pneumonitis . 
the second question is if dose - volume histogram ( dvh ) parameters are more reliable , if the lungs are analyzed as separate organs or as a whole organ . 
the majority of patients ( n = 48 ) received radiochemotherapy for non - small - cell lung cancer ( nsclc ) with a combination of paclitaxel and carboplatpatients were generally treated 5 fx / week , single dose 2 gy , using a two - series approach ( shrinking field ) up to a total dose of 6070 gy . 
for every individual patient , the overall dose distribution was recalculated in the helax - tms by means of adding dose plans according to the total dose applied in each series . 
low - dose volume ( 10 gy , vlow ) , moderate - dose volume ( > 1040 gy , vmod ) and high - dose volume ( > 40 gy , vhigh ) , as well as v10v40 and mean lung dose ( mld ) were defined from the cumulative dvh . 
from the logistic regression curves , a dvh template indicating critical borders of v10v40 was generated for the ipsilateral as well as for the total lung . conclusion : our data indicate that it is reasonable to disperse the dose outside the target volume over large areas in order to reduce the volumes of lung receiving > 40 gy . 
further validation of these constraints is necessary prior to general recommendation . key words : dose - volume relationship clinical pneumonitis 3 - d conformal radiotherapy ntcp dose - volume constraints strahlenther onkol 2003 ; 179 : 54856 doi 10.1007 / s00066 - 003 - 1078 - 0 dosis - volumen - histogramm - analyse zum pneumonitisrisiko bei 3 - d - konformaler strahlentherapie im bereich der lunge ziel : klrung der frage , ob es bei bestrahlung im lungenbereich gnstiger ist , ein groes lungenvolumen mit niedriger dosis zu belasten oder umgekehrt und welche dosis - volumen - histogramm - ( dvh - ) parameter am besten mit dem auftreten einer klinischen pneumonitis korrelieren . 
die zweite frage ist , ob die dvh - parameter verlsslicher sind , wenn beide lungenhlften als separate volumina oder als ein gemeinsames volumen definiert werden . patienten und methodik : wir analysierten die klinischen und dvh - daten von 49 patienten , die wegen eines bronchialkarzinoms eine thorakale bestrahlung erhielten . 
der grte teil ( n = 48 ) erhielt wegen eines nichtkleinzelligen bronchialkarzinoms eine radiochemotherapie mit paclitaxel und carboplatalle patienten wurden von beginn an nach 3 - d - konformaler bestrahlungsplanung ( helax - tms ) normfraktioniert mit gesamtdosen zwi1 department of radiotherapy , university of wrzburg , germany . received : july 23 , 2002 ; accepted : january 17 , 2003 strahlenther onkol 2003 no . 
am kumulativen dvh der gesamtverteilung wurden v10 , v20 , v30 , v40 , die mittlere lungendosis ( mld ) , das niedrigdosisvolumen ( 10 gy , vlow ) , mitteldosisvolumen ( > 1040 gy , vmod ) und das hochdosisvolumen ( > 40 gy , vhigh ) definiert . 
bei analyse der ipsilateralen lunge zeigte sich eine enge korrelation der pneumonitisrate zum vhigh mit einer zunahme von 13% auf bis zu 60% , wohingegen mit zunehmendem vlow die rate auf < 10% fiel . 
die mld zeigte eine enge korrelation zum ntcp - modell nach kutcher , jedoch berschtzte die ntcp - berechnung das pneumonitisrisiko fr die ipsilaterale lunge und unterschtzte das risiko fr die gesamtlunge . 
 schlussfolgerung : unsere daten legen nahe , dass eine verteilung der niedrigdosisareale auerhalb des zielvolumens ber ein mglichst groes lungenvolumen sinnvoll ist , wenn damit das volumen der lunge , das > 40 gy erhlt , reduziert werden kann . 
 schlsselwrter : dosis - volumen - beziehung pneumonitis 3 - d - konformale bestrahlung dosis - volumen - grenzwerte worse in terms of inducing clinical pneumonitis is still an unresolved problem [ 4 ]  . 
 figure 1 schematically demonstrates the problethe two typical cumulative dose - volume histogram ( dvh ) plots have a very similar mld but different highand low - dose regions . introduction three - dimensional ( 3 - d ) conformal treatment planning and delivery is increasingly becoming standard in primary radiotherapy or radiochemotherapy of lung cancer [ 10 ]  . 
we and others have demonstrated that local control of non - small - cell lung cancer ( nsclc ) is a function of tumor volume and total dose applied [ 17 , 19 , 27 ]  . 
however , the sensitivity of the normal lung to radiation damage ( pneumonitis and fibrosis ) is the major problem in thoracic radiotherapy , especially if dose escalation is intended [ 21 , 23 ]  . 
second , they generally consider the lung as a whole organ and do not distinguish between the dose to the involved and the contralateral lung [ 7 , 8 , 12 ]  . 
several authors have demonstrated that the pneumonitis rate increases with mean ( total ) lung dose ( mld ) > 20 gy or with v20 ( volume receiving > 20 gy ) > 30% or v30 > 20% of the total lung [ 1 , 7 , 8 ]  . 
dose - volume relationship for clinical pneumonitis when interpreting data from cumulative dvhs one should keep in mind , that the volume percentage given for a certain dose ( e.g. , 10 gy = v10 ) indicate the proportion of lung receiving at least this dose and more . 
the volume of lung receiving less than the given dose ( the low - dose volume as determined in this report ) is defined by 100% minus the v - value . 
a high volume percentage in the low - dose region of the dvh therefore does not indicate a large low - dose volume ; on the contrary , it indicates a small low - dose volume . 
 the purpose of this study is an analysis of the different dvh parameters and correlation with the observed pneumonitis rate in patients treated with 3 - d conformal radiotherapy for lung cancer at our institution . 
the second question is if dvh parameters are more reliable if ipsilateral and contralateral lung are defined and analyzed as separate organs at risk or if the lung should be defined as a whole organ ( ipsiand contralateral lung together )  . 
 patients and methods we analyzed the clinical and dvh data from 49 patients ( 47 males , two females , mean age 63.8 years , range 4574 years ) treated at the department of radiation oncology of the university of wrzburg , germany , for a thoracic malignancy . 
follow - up of all patients was by clinical examination and chest x - ray or ct scan up to a minimum of 3 months following termination of irradiation and , thus , was considered sufficient to determine if pneumonitis occurred . 
in this analysis , only grade ii and iii pneumonitis was scored as clinical pneumonitis , whereas grade i pneumonitis was regarded as subclinical disease and scored as no clinical pneumonitis . 
 the majority of patients ( n = 48 ) were treated in a radiochemotherapy trial for nsclc with a combination of paclitaxel and carboplatin , one patient received opposed - field irradiation with 3 gy single dose to a total dose of 39 gy for a small - cell carcinoma . 
the dose of this patient was normalized to a standard - fractionation - equivalent dose using the linearquadratic model with an / ( cid : 2 ) value of 3 gy . 
general policy was to spare the contralateral lung as much as possible and to optimize the weight of opposed versus oblique fields in a way that the overall maximum spinal cord dose was between 40 and 45 gy . 
in the following , the target volume was restricted to the primary tumor and involved lymph nodes , and irradiation proceeded witout interruption up to the total dose of 6066 gy . 
 for this analysis , the lung was defined both as separate organs ( ipsilateral and contralateral ) and as a single organ ( total lung ) resulting in three dvhs for each patient . 
care was taken to exclude the gross tumor volume from the lung volume . for detailed dvh analysis , we chose the unnormalized dvh mode resulting in absolute doses at the x - axis of the cumulative dvh . for calculation of normal tissue complication probabilities ( ntcps ) , we used the program diet [ 24 ] which was developed at our institution . 
the program uses the 3 - d dose matrix and normalized dvhs from the tms and calculates ntcp according to different models , among them lymans and kutchers model [ 11 , 14 ]  . 
 in order to demonstrate the variation and typical configuration of the dvh used in this analysis , a simplified mean dvh was calculated by averaging the relative volumes receiving a minimum dose of 10 gy , 20 gy , 30 gy , 40 gy , 50 gy , and 60 gy . 
 for analysis of the influence of highversus moderateversus low - dose volumes , we used a simplified differential dvh , which was reduced to three dose regions : a : low - dose volume ( vlow ) , i.e. , the volume of lung receiving 10 gy ; b : moderate - dose volume ( vmod ) , i.e. , the volume of lung receiving > 1040 gy ; and c : high - dose volume ( vhigh ) , i.e. , the volume of lung receiving > 40 gy up to 70 gy . 
 since the lung is considered a parallel organ , we used a poisson statistical model of cellular / functional subunit damage because of its simple mechanistic interpretation [ 9 , 22 ] for ntcp calculations . 
all cases developed within 3 months from termination of radiotherapy . incidence of pneumonitis according to total dose applied the overall clinical pneumonitis rate in this selected patient cohort was dependent on the total dose applied . 
for the group treated to total doses between 52 and 62 gy , the pneumonitis rate was 26% ( 7 / 27 ) , whereas for the group between 63 and 70 gy the rate increased up to 50% ( 11 / 22 )  . correlation of the mld to v10v60 , vlow , vmod , vhigh , and to pneumonitis rate the mld was significantly correlated to v10v60 , vlow , vmod and vhigh of the ipsilateral , contralateral and whole lung . 
the incidence of pneumonitis increased with increasing mld for the ipsilateral lung ( figure 3 ) with a d50 of 32 gy and a ( cid : 1 ) 50 of 0.98. 
 correlation between low - , moderateand high - dose volume and pneumonitis rate for the ipsilateral as well as the total lung , we observed a negative correlation between the lowand the moderate - dose volume , a weak negative correlation between the lowand the high - dose volume , and no correlation between the moderateand the high - dose volume ( table 1 )  . 
by contrast , with increasing vlow the pneumonitis rate dropped to < 10% , in cases within the 4th quartile ( 4055% of the lung receiving < 10 gy )  . 
quartile v 10 gy v > 40 724 2433 3340 4055% volume 2028 2832 3239 3952% volume v 10 gy v > 40 2736 3644 4449 4971% volume 1216 1618 1820 2029% volume figure 5 . 
from this analysis we conclude , that for the contralateral lung the values for v20 , v30 , v40 , and v50 should not fall below 12% , 11% , 8% , and 5% , respectively . 
 since there are complex correlations between the irradiated volumes within each patient within each lung and between the two lungs , the ratio of v10 ( representing the low - dose region of the dvh , inversely correlated to the amount of lung receiving low dose ) and v40 ( representing the high - dose region ) for the whole lung was calculated and related to the observed pneumonitis rate . 
pneumonitis rate for subgroups of patients with a v30 ( volume of lung receiving 30 gy ) above or below the value given at the x - axis : high rate of pneumonitis with low values of v30 ( with low dose in contralateral lung )  . 
pneumonitisrate fr die untergruppen mit v30 ( volumen , welches 30 gy erhlt ) ber oder unter dem auf der x - achse angegebenen wert : hohe pneumonitisrate bei niedrigen v30 - werten ( also bei maximaler entlastung der kontralateralen lunge )  . 
 logistic regression dvh template the logistic regression curve for v10v40 ( figure 8 ) showed an increasing steepness toward higher doses and the best correlation between volume dose and pneumonitis rate for v40 for the ipsilateral as well as for the total lung . 
the bars delineate the range between 50% and 10% pneumonitis risk taken from figure 8 . the values calculated for v20 and v30 as relevant volumes for estimation of risk for pneumonitis for the whole lung were 30% and 20% , respectively . 
 logistic regression v10v40 ipsilateral lung logistic regression v10v40 ( total lung ) 10 20 30 40 50 60 70 80 90 100 90 100 volume ( % ) volume ( % ) figure 8 . 
 [ 5 ] described a dose - volume relationship for radiation - induced lung damage ; these data , however , were based on literature reviews and data from the pre - ct era . 
dose - volume relationship for clinical pneumonitis dvh template ipsilateral dvh template total lung ntcp predictions 30% risk of pneumonitis ( range 1050% ) 30% risk of pneumonitis ( range 1050% ) 10 20 30 40 50 60 70 dose ( gy ) 10 20 30 40 50 60 70 dose ( gy ) figure 9 . 
 for ntcp calculation models , the complex information of dvhs has to be reduced to a simplified dvh presuming that the individual nonuniform dose distribution in the lung may be equivalent to a uniform irradiation of a certain volume ( veff ) and dose to the whole lung . 
with respect to the nonuniform effect of irradiated volumes in the highand low - dose regions as demonstrated in this study , it is not surprising that the calculated ntcp value does not provide more reliable prediction of the pneumonitis risk than the simple mld , which has been shown to correlate closely to the ntcp value . 
the dvh analysis presented in this report is based on 3 - d conformal treatment plans from the onset of treatment and is a result of the addition of the different dose plans of an individual patient according to the applied dose within a single ct study . 
for example , higher values for v10 mean increasing volume is irradiated with at least 10 gy and vice versa a smaller volume of lung is irradiated with a dose of < 10 gy . 
we found complex interrelationships between low - , moderate - , and high - dose volumes , making it difficult to discuss the effects of a single dose and volume without taking account of the volume of the remaining irradiated lung . 
however , the pneumonitis rate increased with increasing values of v10 , v20 , v30 , and v40 , with the latter providing the best correlation , and decreased with increasing volume of lung irradiated with low dose , indirectly meaning that a more dispersed dose distribution with large areas treated to doses < 10 gy and with reduction of the volume receiving > 40 gy may be favorable for reducing pneumonitis risk . 
the v10 / v40 ratio showed a minimum in pneumonitis rate at 33.5 , suggesting that both predominant highdose region as well as predominant low - dose region ( small volume of lung receiving low dose ) of the dvh are amenable of producing an elevated pneumonitis risk . 
since the steepness of the dose - response curve increases toward the higher doses , a 10% volume increase at v40 produced a 20% increase in pneumonitis rate , whereas the same volume increase in the low - dose region resulted in only 10% increase in pneumonitis rate . 
 in this analysis , kutchers ntcp model generally overestimated the risk of pneumonitis in the separate - organ analysis and underestimated the risk if both lungs were defined as a whole organ . 
this may be an effect of the treatment policy followed in this study , since the beam arrangement and dose were concentrated to the ipsilateral lung and the contralateral lung was spared as much as possible . 
for the total lung , we calculated a d50 of 26.9 gy , which is in the same range as the td50 of 28 gy estimated by martel et al . 
 [ 2 ] , the ( cid : 1 ) 50 of 0.98 calculated in this model can be translated into a value of 0.41 for m in the lyman model for ntcp , which fairly compares to the m = 0.43 and ntd50 of 31.8 gy calculated by kwa et al . 
again , we speculate that our policy of sparing the contralateral lung as much as possible produced this phenomenon , but a description of the irradiation techniques used in their analysis is missing . 
 however , the mld was significantly correlated to v10v60 , vlow , vmod and vhigh of the ipsilateral , contralateral and whole lung and is therefore less suitable for discriminating strahlenther onkol 2003 no . 
this means that mld is , like ntcp values , not a useful parameter to answer the question if the high - dose lung volume or the low - dose lung volume is more critical for the incidence of pneumonitis . 
therefore in our opinion , mld may be of some use in estimation of excessive pneumonitis risk , but it is not a suitable dose constraint for imrt planning . a recent and promising approach which warrants further investigations is the implementation of physical lung function parameters or biological predictors like transforming growth factor ( tgf - ) ( cid : 2 ) serum measurements into risk estimation [ 6 , 16 ]  . 
however , the measurement of tgf - ( cid : 2 ) may result in falsely high values , since tgf - ( cid : 2 ) is mainly stored in blood platelets and the method and time until preparation of the individual blood probe is a critical parameter . 
 dvh template the dvh template presented in this report is the first publication of dvh - based tolerance data from dose distributions calculated by a whole series 3 - d conformal treatment plan on the dose regions of the dvh taking into consideration doses > 30 gy and < 20 gy . 
the values calculated for v20 and v30 for the whole lung confirm the widely accepted 30% and 20% of lung as relevant volumes for estimation of risk for pneumonitis if total lung is considered [ 7 , 8 ]  . 
from the narrower range in the higher dose regions compared to the lower dose regions , reflecting the increase in steepness of the dose - effect curve , we found that volume reduction in the high - dose region ( > 40 gy ) is more effective in reducing pneumonitis rate than a similar reduction in the low - dose region of the dvh . 
two recommendations to reduce the pneumonitis risk for a specific patient can be deduced : the low dose ( 10 gy ) should be dispersed to as much normal lung as possible , and the high - dose region > 40 gy should be as small as possible . 
since the high - dose region is closely correlated to the size of the target volume , a central point in pneumonitis rate is the definition of the target volume and the conformality of the treatment plan [ 10 , 25 , 29 ]  . 
 whole - organ or separate - organ analysis most publications on dvh analysis of the lung are based on analysis of the whole lung as a paired organ and not on separate analysis of the ipsiand contralateral lung . 
classification of pneumonitis used in their study was mainly based on clinical symptoms . in contrast to our method , they also included patients with mild symptoms but without the need for steroids as having a pneumonitis . 
for the hodgkins disease patients with a low incidence of pneumonitis , they found a better correlation between the calculated ntcp and the observed pneumonitis rate , when the lungs were analyzed separately . 
for the lung cancer patients , however , they found a somewhat better correlation , if the lungs of a patient were looked at as a single organ . these apparently contradictory statements are not surprising in view of our results for the contralateral lung . 
we observed an increase in pneumonitis rate , in patients whose contralateral lung was extremely spared , which we interpret as an indirect result of an increased dose to the ipsilateral lung . 
the contralateral lung with a low dose and volume burden is correlated to a clinical - based pneumonitis scale and not to a scale considering exclusively local effects , a worsening of the correlation can be expected . 
 [ 20 ] , in a similar analysis , also found no agreement for the lung functioning as a paired organ and therefore favored a separate - organ analysis . the crude rate of clinical pneumonitis of 37% as presented in this analysis does not necessarily reflect the incidence of pneumonitis following 3 - d conformal radiotherapy for lung cancer . 
with respect to the widespread use of radiochemotherapy in nsclc involving platinum or paclitaxel , there are only few reports on an increased frequency of pulmonary toxicity caused by the combination of chemotherapy and radiotherapy [ 15 ] and especially of paclitaxel and radiotherapy [ 26 ]  . 
in the cohort of patients analyzed in this report , the majority ( 44 / 49 patients ) received concurrent low - dose paclitaxel during radiotherapy following induction chemotherapy with paclitaxel and carboplatthus , conclusions regarding the influence of paclitaxel on pneumonitis rate are not possible from our data . due to the retrospective nature of this modeling analysis , one has to keep in mind , that the parameters identified are primarily true for the patient group analyzed . 
finally , the ratio of patients with and without pneumonitis may have influenced the results . however , if a true relationship of dose , volume and pneumonitis exists , the patients selection should not influence the conclusions as presented . we recommend that these parameters have to be validated by prospective trials prior to a general recommendation for strahlenther onkol 2003 no . 
 conclusion our data showed that in 3 - d conformal treatment of patients with lung cancer , it is reasonable to disperse a low radiation dose ( 10 gy ) over a large lung volume if by this way the highdose volume ( > 40 gy ) can be reduced . 
a reduction in the high - dose region ( v40 ) of the dvh to a certain degree reduces the pneumonitis rate more than a corresponding reduction in the low - dose region ( v10 / v20 )  . 
from this we conclude , that a little dose to a large volume is good , but a lot to a little , i.e. , a reduction of the high - dose ( > 40 gy ) volume , is better in order to keep the pneumonitis rate as low as possible . for this purpose , a discussion on the reduction of the extension of the traditional target volumes is mandatory . 
landmarks for dvh optimization were defined in a dvh template for both the lung as a whole organ and for separate - organ analysis for the ipsilateral lung and may serve as a basis for dvh constraints in imrt planning . 
 strahlentherapie und onkologie original article the use of the multislice ct for the determination of respiratory lung tumor movement in stereotactic single - dose irradiation holger hof1 , 2 , klaus k . 
herfarth1 , 2 , marc mnter1 , 2 , marco essig1 , michael wannenmacher2 , jrgen debus1 , 2 background : in three - dimensional ( 3 - d ) precision high - dose radiation therapy of lung tumors , the exact definition of the planning target volume ( ptv ) is indispensable . 
therefore , the feasibility of a 3 - d determination of respiratory lung tumor movements by the use of a multislice ct scanner was investigated . patients and methods : the respiratory motion of 21 lung tumors in 20 consecutively treated patients was examined . 
the 3 - d differences of these coordinates between the sequentially obtained cycles were assessed ( figure 2 ) , and a correlation with the tumor localization was performed . results : in the craniocaudal ( z - ) direction the mean tumor movement was 5.1 mm ( standard deviation [ sd ] 2.4 mm , maximum 10 mm ) , in the ventrodorsal ( y - ) direction 3.1 mm ( sd 1.5 mm , maximum 6.7 mm ) , and in the lateral ( x - ) direction 2.6 mm ( sd 1.4 mm , maximum 5.8 mm ; figures 3 to 5 )  . 
 key words : multislice ct lung tumors stereotactic radiation therapy respiratory movement strahlenther onkol 2003 ; 179 : 5427 doi 10.1007 / s00066 - 003 - 1070 - 8 die verwendung der mehrzeilen - ct zur bestimmung von atembedingten lungentumorbewegungen bei der stereotaktischen einzeitbestrahlung hintergrund : die dreidimensionale hochdosisprzisionsbestrahlung von lungentumoren erfordert eine exakte definition des planungszielvolumens ( ptv )  . 
zwei unterschiedliche tumorregionen wurden jeweils wiederholt ohne tischvorschub in einer auflsung von vier simultan akquirierten schichten ber eine distanz von 1 cm gescannt ( sechs wiederholungen , scanzeit 0 , 75 s , abstand 3 s , schichtdicke 2 , 5 mm )  . 
 schlsselwrter : mehrzeilen - ct lungentumoren stereotaktische bestrahlung atembewegung 1 department of radiologic diagnostics and therapy , dkfz ( german cancer research center ) , heidelberg , germany , 2 department of clinical radiology , university of heidelberg , germany . 
multislice ct for determination of lung tumor movement introduction stereotactic single - dose irradiation of lung tumors is a sophisticated method for the treatment of selected primary lung tumors as well as of single pulmonary metastases . 
in analogy to mask systems for immobilization of the head [ 1 ] or pelvis [ 8 ] , using a stereotactic setup consisting of a vacuum pillow for patient fixation in a stereotactic frame , high accuracy in patient positioning and target - point setup can also be achieved in the thoracic region , resulting in a minimization of normal tissue being irradiated and in the possibility of dose escalation . 
when performing irradiation under spontaneous breathing , sufficient immobilization can be achieved using an abdominal pressure device [ 2 , 7 , 14 ] , reducing the movement of the diaphragm in the craniocaudal direction . 
nevertheless , the remaining extent of lung movement has to be determined for precise target volume definition in three - dimensional ( 3 - d ) radiotherapy planning . a standard technique for the measurement of maximum deviations of the tumor position is fluoroscopy [ 3 , 14 , 15 ]  . 
the detection of different tumor positions in different breathing phases can easily be performed during one single session , together with the acquisition of the planning ct data set required for radiotherapy planning . 
all patients received stereotactic single - dose treatment with doses at the isocenter ranging from 24 to 26 gy . the median gross tumor volume ( gtv ) was 17 cm3 ( range 387 cm3 ) , while the planning target volume ( ptv ) had a median size of 79 cm3 ( range 23226 cm3 )  . 
the size of the ptv was determined based on the gtv , adding a margin of 3 mm for patient repositioning errors as well as a margin according to the individually measured breathing mobility . 
the minimum margin in the horizontal direction was 6 mm and in the longitudinal direction 10 m the tumors were localized in the lower lobe in three , in the middle lobe in four , and in the upper lobe in 14 cases . 
an abdominal pressure device to reduce lung movements was used in 14 patients , leading to shallow breathing . the pressure device consisted of a plexiglas plate firmly attached to the stereotactic frame . 
 determination of breathing - induced tumor movement after acquisition of the planning ct data set , an additional examination for determination of the lung movement was performed in the same session without the patient being dislocated inside the positioning device . 
for the measurement of breathing - induced tumor movement , sequential multislice data acquisitions were performed over both regions where the upper and lower tumor edge , respectively , were supposed to be located in ( estimated from the planning series ) , i.e. , four simultaneously acquired slices of a certain body region were taken repeatedly with no table movement . the acquisition time was 0.75 s , the delay between acquisitions 3 s , and the slice thickness 2.5 mm , covering a volume of 10 mm in length . 
measurement of the tumor movement was performed by choosing a remarkable point inside the respective tumor region ( e.g. , spikes , vessel crossing the tumor , etc . ) , in the following related to as reference point , and determining its stereotactic coordinates by measuring the distance from the stereotactic center ( figure 1 )  . 
in mediolateral ( x - ) and ventrodorsal ( y - ) direction , movements were defined by calculating the widest distance between the repeatedly defined stereotactic coordinates of the reference point . finally , for each patient the maximum movement of two different reference points of the tumor during the 15 s of ct scanning could be described three - dimensionally . 
abdominal compression was used to keep the extent of tumor movements in the z - direction < 1 c before treatment , an additional spiral ct scan of the tumor region was performed for exact patient repositioning and in order to control the tumor position , which possibly could be different , e.g. , by different abdominal compression levels resulting from an altered abdominal filling status . 
definition of stereotactic coordinates for a chosen anatomic reference point ( arrow ) , by measurement of the distance from the stereotactic center ( cross hairs ) in xand y - direction . 
in the first sequence obtained , the tumor edge ( arrow ) is found in the last slice ( a ) , a later sequence shows the edge in the second slice ( b )  . 
in der ersten sequenz erscheint der tumorrand ( pfeil ) in der letzten ct - schicht ( a ) , eine sptere sequenz stellt den tumorrand in der zweiten ct - schicht dar ( b )  . 
remarkably , in 33% ( n = 7 ) of the measurements the deviation in xand y - direction , respectively , was higher than the movement in z - direction . 
more than in conventional radiotherapy , where relatively generous safety margins are used , the reduction of lung movements and the exact definition of the remains is essential in stereotactic radiotherapy in order to maximize the advantages this technique offers . even more important it becomes when high single doses are applied with an absolute need for normal tissue sparing from the high - dose region as far as possible . 
significant differences between the two measured points of up to 7.5 mm were identified in several patients , although in 57% of all measurements , identical results between the two points were seen . 
second , an exact definition of the tumor position may be hard , especially in small tumors or in central locations , when the tumor is disguised by overlying mediastinal structures [ 18 ]  . 
 when using a multislice ct scanner for the acquisition of the treatment planning scans , it is convenient to use the same device for the additional definition of tumor motion . 
although we also performed fluoroscopy in these first patients , in order to detect possible improvements on tumor motion by abdominal compression , this examination could be replaced in the future by two dynamic ct series , with and without the compression device . 
the difference to the study presented was the use of a single - slice ct scanner , which did not allow the exact definition of the amount of movement . the cause for this was the lack of 3 - d information on the tumor position , only 2 - d data on the tumor extent in a selected table position could be achieved . 
again , the tumor motion in between these sequential slices could only be measured indirectly by comparing the shape of the tumor in each slice to the treatment planning spiral scan . 
other techniques , like the incorporation of slow ct scans of the tumor region in the ptv definition , may lead to a better tumor coverage by an increased detection of extreme tumor positions , but they do not allow absolute quantification of the tumor motion [ 12 ]  . 
the multislice technique instead is not restricted to a narrow slice of the body but displays a real 3 - d volume at a certain time with good spatial resolution , offering the possibility of direct position measurements in all dimensions . 
concerning the resolution quality in the z - direction , the influence of the slice thickness chosen , which accounts for the maximum possible resolution because of the partial volume effect , becomes apparent . 
at the same time , slice thickness yet also determines the size of the region to be scanned simultaneously , which consists of four consecutive slices in current multislice ct scanners [ 9 ]  . 
in our situation , we chose a slice thickness of 2.5 mm , which resulted in a limitation of the region size in z - direction of 1 cthis was supposed to be a good compromise , as for stereotactic singledose therapy tumor movement should be reduced to < 1 cm with no need for the determination of further movement . 
taking into account the repositioning error of the patient , also present in the vacuum pillow used , of approximately 3 mm [ 6 ] , even resolution > 2.5 mm is not absolutely necessary . 
here , quite a short scan time of 0.75 s per scan was used for the exact definition of the points to be measured , avoiding blurredness of the images caused by breathing . 
 indeed , the measured breathing - induced tumor movements of the two regions show an inconsistency in some cases , which can , on one hand , result from a true difference in the motility of different parts of the tumor caused by tighter or weaker attachment to normal tissue structures like vessels or the bronchial systemore likely yet , the difference is related to the different breathing phases when data acquisition was performed . 
at the first look , it could seem that this inconsistency is less in axial ( z - ) direction compared to the in - plane ( xand y - ) directions , but this is only a result of the lower resolution in the z - direction allowing no further discrimination than the chosen slice thickness , in this case 2.5 mfor the definition of the ptv , the results of the region with the highest movement were taken into account . 
 [ 14 ] presented results regarding the fluoroscopic estimation of respiratory movement for patients treated in a similar setup as in the presented study , also using an abdominal pressure device for the stabilization of diaphragm motion . 
because most of the tumors ( n = 14 , 66% ) were located in the upper lobe and only four ( 19% ) and three ( 14% ) of the tumors were located in the middle and lower lobe , respectively , these two latter groups were accumulated to one group for serious statistic testing . 
unexpectedly , no significant correlation between tumor location and the amount of motion could be found , although the highest movement of 10 mm in z - direction was seen in tumors of the upper lung regions . 
multislice ct for determination of lung tumor movement est movement would be expected to take place in the lower lung regions [ 4 , 17 ] , which are closer related to the diaphragm , although stevens et al . 
 in this study , the cause for the insignificance of the differences could be seen in the abdominal compression used in 14 patients with tumors located in the lower and middle lobes , which inhibits the diaphragm from moving . 
the idea that an impaired pulmonary function in some patients could result in forced breathing under abdominal compression could not be verified , as no general lung function tests were performed . in the meantime , a new generation of multislice ct scanners with further increased slice numbers of up to 16 is available , which could be useful for even more precise measurements in the z - direction or to cover even large tumors . 
limited by resolution to tumor movements of up to 1 cm ( using a slice thickness of 2.5 mm ) , it is valuable for the exact definition of the remaining tumor motion in stereotactic high - dose radiotherapy when methods to induce shallow breathing , e.g. , an abdominal pressure device , are used . 
 strahlentherapie und onkologie original article hemoglobin as an independent prognostic factor in the radiotherapy of head and neck tumors ulrich schfer , oliver micke , stefan bodo mller , patrick schller , normann willich1 purpose : the purpose of this study was to analyze the prognostic value of baseline hemoglobin levels before radiotherapy in patients with head and neck tumors . 
 patients and methods : in a retrospective study with a median follow - up of 43 months , we analyzed the results of 214 patients irradiated for head and neck cancer between january 1 , 1990 and january 1 , 1998 ( 180 men and 34 women ; median age 58 years )  . the treatment concept consisted in adjuvant radiotherapy in 58 patients , 77 patients received definitive radiochemotherapy , 42 patients definitive radiotherapy , and 37 patients reirradiation for in - field recurrence . 
several known prognostic factors like sex , age , tumor stage , histologic grading , performance status , and treatment scheme were analyzed for their influence on overall and event - free survival and correlated with pretreatment hemoglobin values ( kaplan - meier method )  . 
 key words : head and neck tumor anemia irradiation strahlenther onkol 2003 ; 179 : 52734 doi 10.1007 / s00066 - 003 - 1117 - x hmoglobin als unabhngiger prognostischer faktor in der strahlentherapie bei kopf - hals - tumoren ziel : der prognostische wert des prtherapeutischen hmoglobinwerts vor strahlentherapie wurde retrospektiv bei patienten mit kopf - hals - malignomen untersucht . 
die behandlung war bei 58 patienten adjuvant , 77 patienten erhielten eine definitive radiochemotherapie , 42 patienten eine definitive radiotherapie und 37 patienten eine wiederholungsbestrahlung nach in - field - rezidiv . 
bezogen auf das gesamtund ereignisfreie berleben wurden bekannte prognostische parameter wie geschlecht , alter , tumorstadium , grading , allgemeinzustand und behandlungsschema untersucht und dem prtherapeutischen hmoglobinwert gegenbergestellt ( kaplan - meier - methode )  . 
in der univariaten analyse waren prognostische faktoren fr das gesamtberleben / ereignisfreie berleben das behandlungsschema ( p < 0 , 001 / p < 0 , 001 ) , das tumorstadium ( p < 0 , 001 / p < 0 , 001 ) , der allgemeinzustand ( p < 0 , 001 / p < 0 , 001 ) und der prtherapeutische hmoglobinwert ( p = 0 , 014 / p = 0 , 05 )  . 
hemoglobin as prognostic factor schlussfolgerung : in dieser retrospektiven analyse erwies sich der prtherapeutische hmoglobinwert als signifikant unabhngiger prognostischer parameter in der strahlentherapie von patienten mit kopf - hals - karzinomen . 
this is why baseline hemoglobin is being discussed as a potential prognostic factor for survival and tumor response [ 3 , 10 , 32 , 35 , 36 ]  . 
 the aim of this study was to examine the influence of baseline hemoglobin on survival and response within a wide spectrum of radiotherapy modalities of head and neck tumors . therefore , treatment results of patients treated with adjuvant or definitive radiotherapy as well as reirradiation were uniand multivariately analyzed , especially with regard to baseline hemoglobin values . patients and methods treatment results of 214 patients were considered who were presented at the department of radiotherapy from january 1 , 1990 to january 1 , 1998 and who received adjuvant or definitive radiotherapy or retreatment of a head and neck carcinoma . 
 treatment adjuvant radiotherapy ( adrt ) was carried out in accordance with the current recommendations : a total dose of 60 gy in 30 fractions / 1 fraction per day was administered to the tumor bed and involved lymph node regions and 50 gy to uninvolved regions . definitive treatment was carried out either as a simultaneous radiochemotherapy ( rct ) or as radiotherapy alone . rct took place as a hyperfractionated scheme ( twice daily 1.8 gy ) with simultaneous application of cisplatin ( 60 mg / m2 ) on day 2 and a 24 - h infusion of 5 - fluorouracil ( 350 mg / m2 ) during days 25 . 
each cycle lasted 2 weeks and was divided into 1 week of treatment ( daily radiotherapy with 2 gy with simultaneous application of 5 - fluorouracil and hydroxyurea ) followed by a 1 - week break . 
histologic grading was g1 ( well differentiated ) in 21 , g2 ( moderately differentiated ) in 126 , and g3g4 ( poorly differentiated or undifferentiated ) in 67 cases . 
all patients with complete response ( cr ; disappearance of all tumor lesions ) or partial response ( pr ; 50% decrease in tumor size ) were classified as remission , patients with no change ( nc ; < 50% decrease in tumor size ) , progressive disease ( pd ; appearance of one or more new lesions and / or progression of existing tumor ) or death were classified as no remission . 
 relative risks for the term response as dependent variable associated with other risk factors ( age , sex , performance status , treatment scheme , ajcc stage , and baseline hemoglobin ) as independent variables were estimated by logistic regression analyses . 
event - free survival was calculated from the start of therapy until the appearance of a local progression , distant metastases , secondary tumor , or death from every cause [ 15 ]  . patients without events were censored from the date of last information . 
after univariate analysis , all variables that showed a significant influence in the univariate analysis were then entered into a cox proportional hazards regression analysis with a backward stepwise procedure , eliminating the least significant variable at each step . 
adrt : adjuvant radiotherapy ; ajcc : american joint committee on cancer ; n.s. : not significant ; rct : definitive radiochemotherapy ; rert : reirradiation ; rt : definitive radiotherapy . 
adrt : adjuvante strahlentherapie ; ajcc : american joint committee on cancer ; n.s. : nicht signifikant ; rct : definitive radiochemotherapie ; rert : wiederholungsbestrahlung ; rt : definitive radiotherapie . baseline hemoglobin overall survival ( median ) ( g / dl ) ( median ) ( months ) event - free survival p ( median ) ( months ) schfer u , et al . 
in the subsequent multivariate analysis , the prognostic factors general condition , treatment , tumor stage and baseline hemoglobin value appeared independent of each other ( table 2 )  . 
die kurven sind aufgeteilt nach prtherapeutischen hmoglobinwerten oberoder unterhalb des medians ( ( cid : 1 ) : prtherapeutische hmoglobinwerte > median ; : prtherapeutische hmoglobinwerte < median )  . discussion the primary object of this review was to investigate the effect of baseline hemoglobin levels on local control and survival after radiation therapy in patients with head and neck cancer in different stages . 
 in collective statistics by grau & overgaard [ 14 ] with a total of 17 , 272 patients from 51 studies , an influence of baseline hemoglobin levels on survival or remission was found in strahlenther onkol 2003 no . 
risk factors with significant influence on tumor response ( multivariate logistic regression analysis ) inclusive of relative risk ( 95% confidence interval ) not to reach a remission . ajcc : american joint committee on cancer ; ecog : eastern cooperative oncology group . 
 [ 22 ] could show that in cases of baseline hemoglobin levels < 14.5 g / dl for men or < 13 g / dl for women , survival was reduced by about 40% and locoregional control by about 30% after definitive radiotherapy of locally advanced head and neck tumors . 
furthermore , hemoglobin was an independent and at least equally powerful predictor of outcome when compared to the known risk factors of site , treatment modality , resection status , t - , and n - stage . 
 [ 10 ] reported that actuarial 2year local control rates for patients who presented with a hemo - globin level < 13 g / dl were 66% , as compared to 95% for patients with a pretreatment level > 13 g / dl . 
 the presumed link between low hemoglobin levels and poor local control and overall survival of solid tumors is molecular oxygen , a well - known radiosensitizer [ 31 ]  . 
recent studies point out that anemia might possess an impact on the progression of angiogenesis in malignant diseases [ 7 , 8 ]  . studies have identified intratumoral hypoxia as an unfavorable factor for locoregional control and survival in patients receiving definitive radiotherapy for cervical or head and neck cancer [ 28 ]  . 
 [ 12 ] , the investigators showed an improved survival and locoregional control with the use of erythropoietin in patients with anemia at the beginning of chemoradiation for oral cavity and oropharyngeal cancer . 
in a pilot study , the feasibility of a therapy with erythropoietin for anemic patients with cancer of the head and neck and the pelvis was tested by henke et al . 
divided their patients in groups with baseline hemoglobin values < or baseline hemoglobin level is a strong prognostic indicator for the treatment success of radiotherapy in head and neck tustrahlenther onkol 2003 no . 
however , the usefulness of correction of anemia with transfusion of anemic patients or the use of recombinant human erythropoietin in curative settings prior to treatment with radiotherapy is unknown . 
 strahlentherapie und onkologie original article uv or x - irradiation increases the cytoplasmic accumulation of rhodamine 123 in various cancer cell lines ingrid elena dumitriu1 , franz roedel2 , thomas d . 
in the case of the tumor cell lines , even though the irradiation - induced inhibition of membrane transporters was accompanied by phosphatidylserine exposure , only a minority of cells had lost their mitochondrial membrane potential during the observation period . 
 key words : abc transporter uvb ionizing radiation apoptosis strahlenther onkol 2003 ; 179 : 56470 doi 10.1007 / s00066 - 003 - 1079 - z uvund rntgenbestrahlung erhhen die zytoplasmatische akkumulation von rhodamin 123 in tumorzelllinien hintergrund : in frheren studien konnte gezeigt werden , dass mitglieder der familie der abc - ( atp - binding cassette - ) membrantransporter gegen uv - induzierte apoptose schtzen knnen . 
 schlsselwrter : abc - transporter uvb ionisierende strahlung apoptose 1 institute for clinical immunology , department of medicine iii , friedrich alexander university of erlangen - nuremberg , erlangen , germany , 2 department of radiooncology , university of erlangen - nuremberg , erlangen , germany . 
rhodamine accumulation in various cancer cell lines introduction multidrug resistance ( mdr ) is the phenomenon of simultaneous cross - resistance of mammalian cells to a variety of anticancer drugs following exposure to one of such agents [ 10 , 33 ]  . one of the mechanisms involved in cellular drug resistance is the increased expression on the cell surface of mdr molecules like p - glycoprotein ( pgp ) , multidrug resistance - associated protein 1 ( mrp1 ) , major vault protein ( mvp ) / lung resistance - related protein ( lrp ) , and breast cancer resistance protein ( bcrp ) [ 8 , 11 , 21 ]  . 
the members of this family are highly conserved throughout evolution and use atp ( adenosine triphosphate ) hydrolysis as energy supply to export a wide range of substrates such as xenobiotics , ions , amino acids , sugars , peptides , and even proteins ( e.g. , interleukin - [ il - ] 1 ( cid : 1 ) ) [ 6 ]  . 
recently , it has been shown that pgp protects against apoptosis induced by various chemotherapeutic agents , fas or tumor necrosis factor - ( tnf - ) receptor ligation and uv irradiation [ 14 , 30 ]  . 
 considering the fact that tumor cell resistance to cytotoxic drugs is one of the major obstacles to successful chemotherapy , we investigated the effect of dna damage following irradiation with uvb and x - ray on the functional activity of membrane transporters . 
it is well established that rh123 is taken up passively and the final amount of labeling is dependent on the active export of the fluorochrome mediated by atp - dependent membrane transporters [ 8 , 23 , 34 ]  . 
in the case of pgp , this efflux has also been found to be inhibited by cyclosporine a and verapamil , which are established modulators of mdr [ 18 , 21 , 29 ]  . 
instead , pump substrates like rh123 have been shown to be exported by a variety of efflux pumps . therefore , an inhibition of rh123 export can be considered a more general inhibition of the net export performed by the concerted action of all the abc transporters , which are active in the cells under investigation . 
hence , determining cellular rh123 accumulation in the presence or absence of modulators of abc transporters gives valuable information on export activity and on the efficiency of its inhibitors [ 4 ]  . 
 material and methods reagents oligomycin , sulfinpyrazone , probenecid , rh123 hydrate , propidium iodide ( pi ) , and 3 , 3 ( cid : 1 ) - dihexyloxacarbocyanine iodide [ dioc6 ( 3 ) ] were purchased from sigma ( munich , germany )  . staurosporine and zvad - fmk ( z - val - ala - asp - fluoromethylketone ) were purchased from alexis biochemicals ( grnberg , germany ) ; cyclosporine a was from novartis ( nuremberg , germany ) ; verapamil was from knoll ( ludwigshafen , germany ) ; annexin v - fitc was from boehringer ( mannheim , germany )  . 
 cells and cell culture peripheral blood mononuclear cells ( pbmc ) were isolated from heparinized peripheral blood of normal healthy volunteers by standard density centrifugation ( lymphoprep , gibcobrl , eggenstein , germany )  . 
in some experiments , plastic - adherent cells were removed by resuspending 2 ( cid : 2 ) 106 ml1 pbmc in dmem ( dulbeccos modified eagles medium ) and allowing them to adhere to plastic at 37 c in a humidified atmosphere with 5% co2 for 60 mthe nonadherent cells ( pbl ) were washed and resuspended in rpmi1640 - based culture mediu the human malignant cell lines , u937 ( myelomonocytic cell line ) , jurkat ( t - cell leukemia ) , ramos ( burkitts lymphoma ) , raji ( burkitts lymphoma ) , ball - 1 ( acute b lymphoblastic leukemia ) , nalm - 6 ( pre - b acute lymphoblastic leukemia ) and arh77 ( multiple myeloma ) , were maintained in rpmi 1640 supplemented with 10% heat inactivated fetal calf serum ( fcs ) ( gibcobrl , eggenstein , germany ) , 1% glutamine , and 1% penicillin - streptomycthis medium is referred to as r10 . 
 rh123 accumulation assay the cells ( 12 ( cid : 2 ) 106 ml1 ) were cultured in 5 ml polystyrene tubes , in r10 containing 5 g ml1 rh123 [ 17 , 34 ] and 1 g ml1 pi . 
the final concentrations of these compounds were as follows : cyclosporine a 7.5 g ml1 , verapamil 30 m , sulfinpyrazone 2.25 mm , probenecid 1 mm , oligomycin 10 m , staurosporine 400 nm [ 13 ] , and zvad - fmk 100 m . 
in addition , cells plated at 1 ( cid : 2 ) 106 ml1 in flat - bottom 24 - well tissue culture plates were irradiated with 3 mj cm2 s of uvb ( 60960 mj cm2 ) or with x - ray ( 0.550 gy ) using orthovoltage irradiation ( stabilipan , siemens , germany ) at a dose rate of 1.15 gy / m the baseline dye uptake was estimated by an immediate measurement of an aliquot of cells . 
 flow cytofluorometry rh123 accumulation was measured using an epics - xl flow cytofluorometer ( coulter , hialeah , usa ) equipped with a 15 - mw argon laser , tuned to 488 nm and standard sets of filters for green ( fl - 1 for rh123 ) and red ( fl - 3 for pi ) fluorescence . 
in this assay , it is assumed that the fluorochrome is taken up passively and that the amount of labeling reflects active export [ 8 , 23 , 34 ]  . 
 hibitors of abc transporters cyclosporine a and verapamil , which are preferentially but not exclusively acting on pgp [ 21 , 29 ] , and sulfinpyrazone as well as probenecid , that were described to favorably inhibit the export mediated by mrp1 [ 23 ]  . 
addition of all inhibitors of abc transporters induced a higher accumulation of rh123 in all tested cell lines ( exemplified for ramos cells in figure 1 ) and in peripheral blood lymphocytes ( pbl ; not shown )  . 
the most powerful inhibitor was cyclosporine a and sulfinpyrazone for most of the cell lines and pbl , respectively . uvb irradiation increased rh123 accumulation in pbl then , we studied the effect of uvb irradiation on rh123 accumulation in pbl . 
most intriguingly , the effect of uvb on the accumulation of rh123 was more pronounced in uvb - irradiated cells , when compared to cells treated with the classic inhibitors of abc transporters ( figure 2b )  . 
rhodamine accumulation in various cancer cell lines 960 uvb 60 uvb 0 uvb time ( min ) 960 uvb 60 uvb sulfinpyrazone cyclosporine a 0 uvb 100 200 300 figures 2a and 2b . 
uvb - bestrahlung von lymphozyten fhrt zu einer zytoplasmatischen anreicherung von rhodamnach bestrahlung von blutlymphozyten konnte eine dosisund zeitabhngige zunahme des zytoplasmatischen fluorochroms beobachtet werden ( a )  . dabei war die inhibition der transportaktivitt nach uvb - bestrahlung ausgeprgter als die durch mdr - modulatoren ( b )  . 
 irradiation with uvb or x - ray increased rh123 accumulation in human malignant cell lines irradiation with uvb or x - ray of malignant cell lines induced a dose - dependent increase of fluorochrome accumulation in five out of seven cell lines within a 7 - h observation period ( four cell lines exemplarily shown in figure 3 )  . 
from the seven tested cell lines , only raji and nalm - 6 did not react to uvb irradiation within the 7 - h observation interval ( raji exemplarily shown in figure 3 )  . however , in the case of x - irradiation , nalm - 6 cells reacted to a dose of 30 gy ( not shown ) , while no influence on rh123 accumulation was to be observed for raji cells for up to 50 gy . since > 90% of both nalm - 6 and raji cells remained viable for > 24 h following irradiation with uvb , we were able to study rh123 accumulation at later time points . 
 radiation - induced rh123 accumulation is accompanied by an early apoptotic phenotype next , we checked for the relationship between apoptosis - related cellular changes and irradiation - induced increase in fluorochrome accumulation . 
in the case of pbl , the cells gated for analysis contained < 5% apoptotic ( annexin v - positive / pinegative ) and an even lower percentage of necrotic cells ( pipositive )  . 
however , for the highest irradiation doses up to 80% of the gated cells bound annexin v at the end of the observation period . nalm - 6 and raji cells represented exceptions since < 10% of these cells were positive for annexin v ( not shown )  . 
in all experiments , cells with shrunken cytoplasm or with granular morphology ( low fsc and / or high ssc ) , and those that were permeable for the cationic dye pi , were excluded from analysis . 
 less than 20% of the cells have lost their mitochondrial membrane potential at the end of the observation intervals , suggesting that the majority of the cells retained functional mitochondria ( not shown )  . 
 increased rh123 accumulation is not a general feature of cells executing apoptotic cell death to further analyze the role of apoptosis on irradiation - induced inhibition of membrane transporters , we tested the effect of the broad - spectrum caspase inhibitor , zvad - fmk [ 32 ]  . 
then , we checked if other forms of apoptosis could influence the activity of membrane transporters . we used an alternative inducer of apoptosis , staurosporine ( 400 nm ) [ 13 ]  . 
 discussion mdr mediated by members of the abc family of membrane transporters is one of the escape mechanisms used by tumor cells to circumvent chemotherapy - induced death [ 10 , 15 , 33 ]  . it is still not completely understood how tumor cells can acquire insensitivity to various structurally diverse toxic drugs with different intracellular targets . 
one of the most extensively studied reason of mdr is the increased expression of members of the superfamily of abc membrane transporters , e.g. , pgp [ 33 ]  . 
rhodamine accumulation in various cancer cell lines u937 ramos ball raji 0 uvb 120 uvb 240 uvb 480 uvb 0 gy 15 gy 30 gy 50 gy time ( min ) figure 3 . 
uvb or x - ray irradiation increased cytoplasmic rhodamine accumulation in various human malignant cell lines in short - term assays . during an observation interval of up to 7 h , a dose - dependent increase in the accumulation of rhodamine was observed for both uvbor x - ray - irradiated cells . 
 u937 0 uvb 480 uvb 480 uvb + zvad ramos 0 uvb 480 uvb 480 uvb + zvad 0 uvb staurosporine staurosporine + zvad 0 uvb staurosporine staurosporine + zvad time ( min ) figures 4a to 4d . 
increased rhodamine accumulation is a unique feature of irradiation and not a general hallmark of apoptotic cell death . treatment with the broad - spectrum caspase inhibitor zvad - fmk ( zvad ) increased rhodamine accumulation in uvb - irradiated u937 and ramos cells ( a , b )  . 
in addition , staurosporine - induced apoptosis had only a minor effect on rhodamine accumulation , which again was not influenced by zvad - fmk ( c , d )  . 
die behandlung mit dem breitspektrum - caspase - inhibitor zvad - fmk ( zvad ) fhrte zu einer erhhten rhodaminakkumulation in uvbbestrahlten u937and ramos - zellen ( a , b )  . 
zustzlich zeigte eine staurosporininduzierte apoptose nur einen geringen effekt auf die rhodaminanreicherung , die ebenfalls nicht durch zvad - fmk beeinflusst wurden konnte ( c , d ) intrazellulres rhodamin wurde durchflusszytometrisch bestimmt , die uvb - dosen sind in mj cm2 angegeben . 
rhodamine accumulation in various cancer cell lines in an energy - dependent efflux of chemotherapeutic agents from the cytoplasm , followed by a reduced drug accumulation and by resistance to the therapeutic intervention [ 15 , 33 ]  . 
recently , it has been shown that pgp protects against apoptosis induced by various chemotherapeutic agents , cross - linking of fas or tnf receptors , and uv irradiation [ 14 , 30 ]  . we investigated the effect of irradiation on the export function of membrane atp - dependent transporters . 
we used an rh123 accumulation assay , in which fluorochrome uptake is passive and the final accumulation is a function of active export [ 8 , 23 , 34 ]  . 
we were able to confirm that rh123 accumulation increased in samples treated with established inhibitors of abc transporters or with the atp - depleting agent oligomycwhen pbl were irradiated with uvb , we observed that rh123 accumulation increased in comparison with nonirradiated controls . 
this effect most likely reflected the irradiation - induced inhibition of the atp - dependent membrane transporters exporting rh123 . when we used various human malignant hematopoietic cell lines , cyclosporine a inhibited the export of rh123 better than verapamil , sulfinpyrazone , and probenecid for most cell lines tested . 
uvb or x - ray irradiation of malignant cell lines also induced a doseand time - dependent increase of rh123 accumulation in five of the seven tested cell lines , within a 7 - h observation interval . 
it is remarkable that nalm - 6 and raji displayed the lowest apoptosis rates compared to all other cell lines studied , with < 10% apoptotic cells 24 h after irradiation . 
surprisingly , raji did not respond to x - rays as high as 50 gy , whereas nalm - 6 showed an increased rh123 accumulation in response to 30 gy as soon as 3 h after irradiation . 
 due to the fact that uvb is a powerful inducer of apoptosis , we were interested in the relationship between the occurrence of the inhibition of the membrane transport and apoptosis . 
on the contrary , when we measured ps exposure on cell lines , for the highest irradiation dose up to 80% of the gated cells were positive at the end of the observation interval . 
these data suggest that the effect induced by irradiation on the export function of the abc transporters is a unique feature accompanying irradiation and not a general hallmark of apoptotic cell death . 
that might be interesting in as much , as there is growing evidence , that delivering combined radiochemotherapy revealed a higher clinical benefit [ 25 , 28 ] when compared to irradiation or chemotherapy alone as well as increasing side effects caused by interaction of the different treatment compounds [ 9 ]  . 
considering the fact that members of the abc transporters family are overexpressed by human tumors , the inhibition of the function of abc transporters by irradiation may offer new potential for reverting mdr of cancer cells . 
 acknowledgments this work was supported by grants of the wilhelm sander foundation and by the interdisciplinary center for clinical research 01 ks 9601 / 1 of the friedrich alexander university of erlangen - nuremberg . 
 strahlentherapie und onkologie technische note verbesserte lagerungsreproduzierbarkeit eines nichtinvasiven hochprzisionsmaskensystems in der stereotaktischen radiotherapie durch eine integrierte kieferfixierung eric lopatta1 , susie - maria liesenfeld1 , priska bank1 , reinhard wurm2 , robert gnther1 , tilo wiezorek1 , thomas g . 
die reproduzierbarkeit der lagerung wurde durch ausmessung von verschiebungen anatomischer strukturen auf filmebene in 0 und 90 bestimmt . vor den aufnahmen in gantryposition 0 und 90 erfolgte die feinjustierung des simulators ber ein optisches ringsysteinsgesamt wurden whrend der 2bis 7 - wchigen therapie 844 messungen an einem digitalen bildverarbeitungssystem erhoben . 
 ergebnisse : im vergleich der standardabweichungen der messergebnisse ergibt sich unter verwendung einer zustzlichen kieferfixierung eine signifikante verbesserung der lagerungsreproduzierbarkeit in den drei freiheitsgraden : lateralverschiebung 0 , 6 mm mit kieferfixierung vs . 
 schlsselwrter : nichtinvasive fixierungstechnik hirntumoren fraktionierte stereotaktische radiotherapie reproduzierbarkeit gesichtsmaske digitale bildverarbeitung strahlenther onkol 2003 ; 179 : 5715 doi 10.1007 / s00066 - 003 - 0941 - 3 improved patient repositioning accuracy by integrating an additional jaw fixation into a high precision face mask system in stereotactic radiotherapy of the head background : for high precision radiotherapy of the neurocranium a precise , reproducible positioning technique is the basic prerequisite . 
the aim of this study was to assess the influence of a modification of the commercially available stereotactical brainlab - head mask system on accuracy in patient positioning during fractionated radiotherapy . 
the positioning accuracy was assessed by measurements of the shifting of anatomical landmarks in relation to the rigid mask system on biplanar simulator films using a digital imaging systebefore each measurement a fine adjustment of the simulator to an optical ring system was performed . 
during a 27 weeks lasting course of radiotherapy displacement measurements in relation to the reference images for all three dimensions ( z , y and x ) were done once a week . 
 results : an additional jaw fixation improves the reproducibilty of patient positioning significantly in all three spatial dimensions . the standard deviation in lateral direction ( x ) was 0.6 mm with jaw fixation vs . 
 key words : noninvasive immobilization technique brain tumors fractionated stereotactic radiotherapy reproducibility head - mask system digital imaging einleitung fortschritte durch einsatz von computertomographie ( ct ) und magnetresonanztomographie ( mrt ) ermglichen bessere abgrenzbarkeit vom normalgewebe gegenber zu bestrahlendem tumorgewebe und tragen zu einer verringerung des klinischen zielvolumens ( clinical target volume , ctv ) bei . das planungszielvolumen ( ptv ) wird unter anderem durch die patientenbewegung whrend der einzelnen bestrahlung einerseits , aber insbesondere bei der bestrahlung von intrakraniellen tumoren auch durch variation der lage des zielvolumens ( isozentrums ) von tag zu tag beeinflusst . 
sie wurden aus rigiden , invasiven fixierungsmethoden , wie sie im rahmen der hochprzisionsbestrahlung der radiochirurgie zur anwendung kommen , entwickelt . technisch basieren diese systeme auf der kombination einer reversiblen patientenfixierung mit einem stereotaktischen koordinatensystem [ 2 , 3 , 9 , 13 ]  . 
diese fixierung erfolgt entweder durch ein plastisch formbares maskenmaterial [ 10 ] oder durch die fixierung eines festen anatomischen punktes ( oberkiefer , uerer gehrgang [ 4 , 13 , 15 ] ) am stereotaktischen rahmen . systematische untersuchungen ber die lagerungsgenauigkeit dieser systeme zeigen , dass die przision invasiver fixierungssysteme erreicht wird [ 3 , 6 , 1012 , 16 ] und lagerungsvariabilitten von weniger als 2 mm erzielt werden knnen . 
in der vorliegenden arbeit wird der einfluss einer modifikation des kommerziell erhltlichen stereotaktischen brainlabkopfmaskensystems [ 12 ] in form einer zustzlichen kieferfixierung auf die lagerungsgenauigkeit und - reproduzierbarkeit whrend einer fraktionierten strahlentherapie untersucht . 
mit dem originalen maskensystem wurden in der pilotphase der untersuchung elf patienten fixiert ( abbildung 1a )  . anschlieend wurden 18 der insgesamt 29 patienten mit einer zustzlichen kieferfixierung behandelt . 
bei der anfertigung der lokalisationsaufnahmen am simulator wird die speicherfolienkassette grundstzlich in einer kassettenhalterung am bildverstrker befestigt . mit hilfe dieser vorrichtung wird gewhrleistet , dass die ebene der speicherfolie senkrecht zum zentralstrahl steht . 
hochprzisionsmaskensystem vor dem planungs - ct und bei jeder kontrolle erfolgte die messung der verschiebungen anatomischer fixpunkte ( landmarks ) in bezug auf definierte punkte am stereotaktischen rahmensystehufig genutzte anatomische fixpunkte waren gut erkennbare kncherne strukturen wie die fossa orbitalis oder die fossa pterygoidea . 
bei benutzung des kalibrier - tools ergibt sich der bekannte abstand von 10 cm im isozentruohne benutzung des kalibrier - tools muss der abstandswert in cm 10 ( cid : 1 ) vergrerungsfaktor betragen . 
 die standardabweichungen der ermittelten verschiebungen in allen drei freiheitsgraden wurden mit microsoft excel 97 und spss 10 errechnet und auf signifikanz mit dem mann - whitney - u - test gepr zustzlich erfolgte die kalkulation der absoluten abweichungen whrend der wchentlichen kontrollen im vergleich zur ersten messung vor dem planungs - ct . 
die mediane longitudinale variabilitt , in den anteroposterioren aufnahmen gemessen , verringerte sich auf 0 , 5 mm nach fixierung deutlich gegenber 1 , 3 mm ohne fixierung ( p < 0 , 001 )  . die in den lateralen aufnahmen ermittelte longitudinalverschiebung besttigte diese ergebnisse ( 0 , 5 mm mit und 1 , 5 mm ohne zustzliches kieferfixierung ( p < 0 , 001 ) )  . 
die mediane vertikale verschieblichkeit , die ausschlielich in den lateralen aufnahmen bestimmt wurde , betrug 0 , 6 mm mit und 0 , 9 mm ohne zustzliche fixierung ( p < 0 , 001 ) ( abbildung 3 )  . 
das mittel der regressionskoeffizienten der verlufe aller patienten mit fixierung betrug 0 , 087 im vergleich zu 0 , 052 aller patienten ohne fixierung . ein eindeutiger trend einer systematischen verschiebung in eine richtung in abhngigkeit von der behandlungszeit konnte nicht bewiesen werden . 
dies belegen eine vielzahl von publikationen , die abweichungen von zwei millimeter oder auch weniger nachweisen konnten [ 1 , 3 , 5 , 1012 , 15 , 16 ]  . 
diese methode vermeidet zwar nicht die interindividuellen unterschiede bei der definition anatomischer fixpunkte , aber es werden fehlerquellen wie die ungenauigkeiten bei der verwendung eines stahlmaes und der filmausgabe mit verzeichungen durch die direkte digitale bildverarbeitung vermieden . in abhngigkeit von der gesamtbehandlungsdauer konnte kein eindeutiger trend einer zunahme der lagerungsvariabilitt ermittelt werden . 
8 urban & vogel strahlentherapie und onkologie original article fanconis anemia and clinical radiosensitivity report on two adult patients with locally advanced solid tumors treated by radiotherapy michael bremer1 , detlev schindler2 , michaela gro2 , thilo drk3 , susanne morlot4 , johann h . 
 case report and results : two 24and 32 - year - old male patients with fa were treated by definitive radiotherapy for locally advanced squamous cell head and neck cancers . 
in the first patient , long - term tumor control could be achieved after delivery of 67 gy with a in part hyperfractionated split - course treatment regimen and , concurrently , one course of carboplatin followed by salvage neck dissection . 
5 years later , additional radiotherapy was administered due to a second ( squamous cell carcinoma of the anus ) and third ( squamous cell carcinoma of the head and neck ) primary , which the patient succumbed to . 
while the diagnosis fa could be based on flow cytometric analysis of a lymphocyte culture in the second patient , the diagnosis in the first patient had to be confirmed by hypersensitivity to mitomycin of a fibroblast cell line due to complete somatic lymphohematopoietic mosaicisin this patient , phenotype complementation and molecular genetic analysis revealed a pathogenic mutation in the fanca gene . 
 key words : fanconis anemia clinical radiosensitivity cytogenetic analysis strahlenther onkol 2003 ; 179 : 74853 doi 10.1007 / s00066 - 003 - 1099 - 8 fanconi - anmie und klinische strahlensensibilitt . 
bericht ber die radiotherapie von zwei erwachsenen patienten mit lokal fortgeschrittenen soliden tumoren hintergrund : patienten mit fanconi - anmie ( fa ) weisen eine erhhte klinische strahlensensibilitt unterschiedlicher ausprgung auf . 
beim ersten patienten konnte nach einer teilweise hyperfraktionierten splitcourse - bestrahlung mit 67 gy simultan zu einem kurs carboplatin und einer salvage - neck - dissection eine langfristige tumorkontrolle erreicht werden . 
whrend die diagnose fa beim zweiten patienten durch eine durchflusszytometrische g2phasen - analyse einer stimulierten lymphozytenkultur gestellt werden konnte , gelang dies beim ersten patienten aufgrund einer vollstndigen somatischen mosaikbildung der hmatopoetischen zellen nur durch nachweis einer mitomycin - berempfindlichkeit einer fibroblastenkultur . 
 schlsselwrter : fanconi - anmie klinische strahlensensibilitt zytogenetische analyse 1 department of radiation oncology , hannover medical school , hannover , germany , 2 institute of human genetics , university of wrzburg , germany , 3 department of obstetrics and gynecology , hannover medical school , hannover , germany , 4 institute of human genetics , hannover medical school , hannover , germany . 
fanconis anemia and clinical radiosensitivity introduction fanconis anemia ( fa ) is a rare autosomal recessive disorder characterized by multiple congenital abnormalities , progressive bone marrow failure of variable degree and cancer susceptibility due to an underlying defect in dna damage response [ 5 ]  . 
 due to their increased chromosomal instability , fa patients tend to develop malignancies , most commonly leukemia , but solid tumors have been described as well appearing at a much younger age than in the general population [ 1 ]  . 
 case report and results patient 1 the 24 - year - old male patient presented in 1993 with a locally advanced and inoperable squamous cell carcinoma of the base of the tongue with bilateral cervical lymph node metastases ( tnm stage : ct4cn2g2m0 )  . 
definitive radiotherapy was delivered by telecobalt using a three - field junctional technique including the bilateral cervical and supraclavicular lymph nodes ( two opposing lateral fields in the upper portion , field sizes : 10 ( cid : 1 ) 13 cm ; one anterior field in the lower portion , field size : 20 ( cid : 1 ) 8 cm )  . 
 initially , a hyperfractionated accelerated split - course regimen ( 2 ( cid : 1 ) 1.6 gy daily ) was applied with concurrent administration of one course of carboplatinum ( 60 mg / m2 , day 15 )  . 
a second course of chemotherapy was omitted due to development of pancytopenia ( ctc grade 3 toxicity ) within 3 weeks after onset of the first course ( hemoglobin : 84 g / l ; white blood count : 1.7 ( cid : 1 ) 109 / l , recovery after 4 weeks , platelets : 88 ( cid : 1 ) 109 / l , recovery after 10 days )  . 
furthermore , confluent oral mucositis developed within the 2nd week of treatment ( after delivery of 27.2 gy ) requiring total parenteral feeding ( ctc grade 3 toxicity )  . 
due to the marked mucositis , radiotherapy was restarted 14 days later with conventional fractionation ( fraction size : 1.8 gy once daily , five fractions weekly ) to a total dose of 67 gy . 
while the primary showed complete regression , some cervical lymph nodes persisted in the right neck requiring salvage neck dissection 14 days after the end of radiotherapy revealing residues figure 1a abbildung 1a figure 1b abbildung 1b figures 1a and 1b . 
after spincter - preserving local excision , postoperative radiotherapy ( without chemotherapy ) was performed , which was delivered by 23 - mv linac photons using an isocentric four - field box technique to a total dose of 55.8 gy ( single dose 1.8 gy , five fractions weekly )  . 
treatment was well tolerated with only moderate local skin reactions ( ctc grade 2 ) confined to the perineuonly 4 months later , an inoperable squamous cell carcinoma of the floor of the mouth was diagnosed . 
local reirradiation with reduced treatment volume and total dose ( 25.2 gy , single dose 1.8 gy delivered once daily ) was performed with three concurrent applications of weekly gemcitabine ( 100 mg / m2 )  . 
moderate hematologic symptoms with thrombocytopenia ( nadir : 63 ( cid : 1 ) 109 / l ) and anemia ( nadir : 95 g / l ) recovered spontaneously at the end of treatment . 
 despite the presence of several clinical abnormalities suggestive of fa ( short stature with 160 cm of height and 42 kg of weight , loosely scattered caf - au - lait spots on the trunk , cryptorchidism of the right testis ) and skeletal malformations ( absent left thumb , bilateral clinodactyly of the fifth digit , navicular hypoplasia , brachymesophalangia ) , ( figures 1a and 1b ) , the diagnosis fa had not been considered until he appeared with his second tumor . 
due to a complete somatic mosaicism of the hemato - poietic cells ( see below ) , the cytogenetic confirmation of fa has not been established until the occurrence of the third primary . 
 patient 2 the 32 - year - old male patient presented in 2001 with a locally advanced squamous cell carcinoma of the lateral and posterior oropharyngeal wall reaching up to the base of skull superiorily ( tnm stage : ct4cn2g2m0 )  . 
prior to the beginning of radiotherapy , a ct scan of the neck revealed locally progressive disease with vast tumor masses reaching bilaterally from the base of skull to the lower neck . 
 in this patient , fa had been clinically diagnosed years ago on the basis of several abnormalities and morphologic malformations ( short stature with 152 cm of height and 38 kg of weight ; small facial size , bilaterally absent radii and thumbs , skin hyperpigmentation , hypothyroidism , hypogonadism , diabetes mellitus )  . 
pretreatment peripheral blood analysis revealed normocytic anemia ( hemoglobin 109 g / l ) and thrombocytopenia ( 93 ( cid : 1 ) 109 / l ) while the white blood count was within the normal range . 
 radiotherapy was delivered by 6 - mv linac photons using two opposing lateral fields ( field size : 16 ( cid : 1 ) 18 cm ) and a thermoplastic head mask for immobilization . 
to test for increased acute radiosensitivity , single dose was reduced to 1.0 gy for the first five fractions once daily and raised to 1.5 gy per fraction since no signs of increased early skin or mucosal toxicity were observed at that time . 
after delivery of a total dose of only 8.0 gy ( 7 treatment days ) , radiotherapy had to be discontinued due to the development of severe thrombocytopenia ( platelets : 5 ( cid : 1 ) 109 / l ) , which became fatal only few days afterwards despite intensive supportive care including platelets substitution ( ctc grade 5 toxicity )  . 
while cells of fa patient 2 displayed a high degree of spontaneous g2 accumulation that is characteristic of fa patients ( without exposure to mitomycin ) , the g2 - phase fraction in patient 1 was within the normal range ( figure 2 )  . 
however , the diagnosis fa in patient 1 could be confirmed in a fibroblast cell line established from a skin biopsy which showed extreme hypersensitivity to mitomycin by activating the accumulation of cells in the g2 phase ( figure 3a )  . 
after separate retroviral introduction of full - length cdnas encoding different fa genes and one control in different subcultures , the mitomycin - activated accumulation of cells in the g2 phase was selectively complemented by fanca cdna ( figure 3b )  . 
subsequent molecular genetic analysis revealed a pathogenic 4 - bp deletion ( 1111deltggt ) on one allele of exon 13 in the fanca gene , whereas the underlying pathogenic mutation on the other allele could not be identified after sequencing the fancacoding region . 
durchflusszytometrisch bestimmte spontane g2 - phasen - anteile ( g2 - phasen dividiert durch die wachstumsfraktion ) in pha - stimulierten 72 - h - lymphozytenkulturen ohne mitomycin - exposition ( cutoff - wert : 0 , 31 )  . 
die schwarzen rauten reprsentieren die ergebnisse von 201 fa - zellkulturen ( mittlerer quotient sd : 0 , 486 0 , 09 ) , die grauen punkte diejenigen von 219 normalen kontrollen ( mittlerer quotient sd : 0 , 207 0 , 041 )  . 
der g2 - phasen - anteil von fa - patient 1 ( ) fllt aufgrund einer somatischen mosaikbildung der hmato - poetischen zellen in den normalwertbereich , whrend bei fa - patient 2 ( ) der fr fa - patienten typische spontane g2 - block nachweisbar ist . 
reports of hyperpigmentation or desquamation of irradiated skin areas after 5 gy single fraction total body ( tbi ) or thoracoabdominal ( tai ) irradiation or even fatal regimen - related toxicity after 6 gy fractionated tbi [ 11 ] have lent support to the assumption of an increased clinical radiosensitivity . 
because of the extreme clinical variability of the disease , diagnosis must be based on cytogenetic tests that measure the hypersensitivity of cells to the chromosomal breaking effect of crosslinking agents such as mitomycin and deboxybutane ( deb ) , which provide a sensitive and specific diagnostic criterion for the disorder [ 13 ]  . 
 in contrast to the hypersensitivity to crosslinking agents , cultured cell lines of fa patients display variable levels of in vitro radiosensitivity , if at all , and are reported to be comparable with the moderate radiosensitivity of ataxia telangiectasia ( at ) heterozygotes or li - fraumeni syndrome fibroblasts [ 4 , 19 , 21 ]  . 
 [ 16 ] in a 32 - year - old fa patient with head and neck cancer , limits the possible value of predictive assays for guiding clinical decision - making in individual cases [ 3 ]  . 
in this context , the 24 - color fish ( fluorescence in situ hybridization ) method appears to be a promising cytogenetic approach to detect and quantify genetically determined intrinsic radiosensitivity [ 14 ]  . 
the molecular basis seems to be based on genetic reversion at the disease locus of a lymphohematopoietic stem cell causing a significant accumulation of corrected cells in the patients blood . 
however , it remains unclear , to which extent , if at all , somatic mosaicism may have contributed to the limited treatment - related hematotoxicity observed in this patient . 
there are some clinical data demonstrating a protective effect of amifostine from radiation hematotoxicity , particularly granulocytopoiesis in patients undergoing radiotherapy for squamous cell carcinoma of the head and neck [ 17 ]  . 
clinical evidence of the usefulness of these measures in fa patients are still missing but would be of significant importance for patients with dna repair disorders as well as for patients with elevated radiosensitivity in general . 
 although clinical radioresponsiveness is hardly predictable in fa patients and might turn out to be dramatic or even fatal , from our own clinical observations it does not seem appropriate to exclude fa patients from radiotherapy in general . 
long - term tumor control with acceptable toxicity seems to be achievable , even if the ultimate outcome remains obscure due to the possible occurrence of multiple new primaries during follow - up . 
if surgical interventions are inadequate due to the advanced tumor stage , definitive radiotherapy or even radiochemotherapy seems to be feasible on the basis of altered fractionation schedules and may yield longterm tumor control . 
 strahlentherapie und onkologie original article transperineal high - dose - rate interstitial radiation therapy in the management of gynecologic malignancies jun itami , ryusuke hara , takuyou kozuka , hideomi yamashita , kaori nakajima , kouji shibata , yoshihisa abe , masashi fuse , masashi ito1 background : high - dose - rate interstitial radiation therapy is a newly introduced modality , and its role in the management of gynecologic malignancies remains to be studied . 
 patients and methods : eight patients with primary and nine with recurrent gynecologic malignancies underwent high - dose - rate interstitial radiation therapy with / without external - beam irradiation . 
grade 2 and 4 late complications were seen in five patients , and the incidence was significantly higher in patients with a larger volume enclosed by the prescribed fractional dose of high - dose - rate interstitial radiation therapy . 
 conclusion : although high - dose - rate interstitial radiation therapy is a promising modality , it must be applied cautiously to patients with bulky tumors because of the high incidence of serious complications . key words : interstitial radiation therapy brachytherapy high dose rate gynecologic malignancy complication strahlenther onkol 2003 ; 179 : 73741 doi 10.1007 / s00066 - 003 - 1069 - 1 transperineale interstitielle high - dose - rate - brachytherapie bei gynkologischen malignomen hintergrund : die interstitielle high - dose - rate - ( hdr - ) bestrahlung ist eine neu eingefhrte modalitt , deren rolle bei der behandlung von gynkologischen malignomen noch zu klren ist . 
 patienten und methodik : acht patientinnen mit primren malignomen und neun patientinnen mit redizidiven im gynkologischen bereich unterzogen sich einer interstitiellen hdr - bestrahlung ( mit / ohne perkutane bestrahlung ) mit 46 gy bei einer gesamtdosis von 1554 gy . 
die interstitielle bestrahlung wurde zweimal tglich im abstand von > 6 h durchgefhrt . ergebnisse : die lokale 2 - jahres - kontrollrate betrug bei der primrtherapie 75% und bei der behandlung von rezidiven 47% ( p = 0 , 46 )  . 
bei 78% der patientinnen mit einem volumen > 100 cm3 fanden sich nach 18 monaten komplikationen grad 2 und 4 , dagegen bei 0% der patientinnen mit kleinerem volumen ( p < 0 , 04 )  . 
 schlussfolgerung : obwohl die interstitielle hdr - bestrahlung eine viel versprechende modalitt ist , muss sie bei patientinnen mit groen tumoren wegen der hohen inzidenz schwerer komplikationen vorsichtig angewandt werden . 
 schlsselwrter : interstitielle bestrahlung brachytherapie high - dose - rate gynkologisches malignom komplikationen 1 department of radiation therapy and oncology , international medical center of japan , tokyo , japan . received : july 8 , 2002 ; accepted : may 6 , 2003 strahlenther onkol 2003 no . 
high - dose - rate interstitial irradiation for gynecologic malignancies introduction high - dose - rate intracavitary irradiation is an established method in the management of gynecologic malignancies , especially in cervical cancer . 
while there have been many studies evaluating interstitial low - doserate radiation therapy , the number of studies on high - doserate interstitial irradiation is limited [ 3 , 4 , 10 , 21 ]  . 
high - dose - rate interstitial irradiation was applied as primary treatment in eight patients , and for the management of recurrent tumors in nine ( table 1 )  . 
maximum tumor size ranged from 2 to 8.4 cm with a mean of 5.2 c external - beam radiation therapy to the whole pelvis with a mean pelvic center dose of 35.4 gy was applied in 14 patients , of which three had been irradiated previously . 
in patients undergoing primary treatment , bilateral parametria including the cervix were implanted applicators in six patients with cervical cancer , while only the right parametrium was treated in one patient with cervical cancer after radical hysterectomy with a positive surgical margimplantation was performed to the posterior vaginal wall in a patient with vaginal cancer . 
in the nine patients with recurrences , implantation was done to the bilateral parametria with / without cervix in three , to the vaginal vault in four , and to the uretable 1 . 
a syed - neblett template ( alpha omega services ) was used in 15 patients , in six of whom tandem and obturator applicators were loaded simultaneously ( figure 1 )  . a rectal template ( alpha omega services ) was employed in one patient . 
thereafter , orthogonal x - rays were taken , which were used for digitization of the applicator positions in cadplan bt ( varian , palo alto , ca , usa )  . 
the volume encompassed by the fractional dose ( treatment dose ) of interstitial irradiation was defined as v ( td ) , and ranged between 16 and 246 cm3 with a mean of 106 cm3 . 
 for calculation of survival and late complication rates , the product - limit method by kaplan & meier [ 11 ] was used with differences evaluated by log - rank test . 
in patients with a maximum tumor size > 6 cm , local control rate was 25% at 8 months , while 69% of the patients with tumors 6 cm remained locally controlled at 2 years . 
grade 4 late complications were observed in four patients , of which three developed a rectovaginal fistula in the center of the uncontrolled tumor and subsequently died of their tumor . 
actuarial incidence of grade 2 and 4 late complications at 18 months was 78% and 0% in the patients with v ( td ) > 100 cm3 and with smaller v ( td ) , respectively ( p < 0.04 ; figure 2 )  . 
the patients treated by simultaneous loading of tandem and obturator flexiguides did not show a statistically significant difference in the incidence of rectovaginal fistulas in comparison to those treated without tande discussion in intracavitary irradiation , inadequate coverage of the target volume by the prescribed dose is due to suboptimal alignment of tandem and / or ovoids as well as bulky tumor extending outside the dose prescription points , such as manchester point a . transperineal low - dose - rate interstitial radiation therapy has proven to be effective in overcoming these shortcomings in intracavitary irradiation [ 1 , 5 , 7 , 17 ]  . 
by contrast , only a few clinical experiences have been reported regarding transperineal high - dose - rate interstitial irradiation [ 3 , 4 , 10 , 21 ]  . 
in our department , high - dose - rate intracavitary irradiation in four fractional doses of 6 gy at the manchester point a has been delivered for stage iiib cervical cancer subsequent to a central pelvic dose of 30 gy by external - beam irradiation [ 20 ]  . 
accordingly , high - dose - rate interstitial irradiation with 5 ( cid : 1 ) 5 gy was administered as a principle in the current study , because it has almost the same biologically effective dose [ 6 ] as high - dose - rate intracavitary irradiation , on the assumption that / ( cid : 2 ) = 10 gy . 
 our study showed that a 2 - year local control rate of 47% could be obtained even in patients with recurrent tumors , although the high incidence of grade 2 and 4 late complications of up to 71% poses a serious proble the maximum tumor size was shown to be the most influential prognostic factor in terms of local control . 
reported an excellent local control rate of 94% with a mean follow - up of 40 months , and a difference of local control by tumor size was not found [ 3 ]  . 
high - dose - rate interstitial irradiation for gynecologic malignancies pear to be related to local control , provided that v ( td ) was < 100 cm3 [ 10 ] , while the same group had described poorer local control in patients with larger tumors [ 21 ]  . 
it must be further studied whether such an intensification of high - dose - rate interstitial radiation therapy including new modalities improves the local control rate even in large tumors [ 8 , 16 ]  . 
the four patients with grade 4 late complication must be viewed with caution , because three of them had a rectovaginal fistula occurring in the uncontrolled tumor and fistula formation per se might be a sign of tumor progression and not treatment - related . 
 [ 17 ] , the simultaneous loading of tandem and obturator applicators is preferably to be avoided in lowdose - rate interstitial irradiation , because of the increased incidence of rectovaginal fistulas . 
it seems that not only the maximum dose to the rectal wall , but also the high - dose region have an influence on the incidence of rectal injury [ 15 ]  . 
large v ( td ) combined with long source movement apparently contributes to the widening of high - dose area of the anterior rectal wall . with respect to the incidence of rectal injury in high - dose - rate interstitial irradiation for gynecologic malignancies , the relationships between v ( td ) , maximum rectal dose , and highdose region must be further eludicated . 
 although high - dose - rate interstitial radiation therapy is a promising modality to attain local control in gynecologic malignancies , it must be delivered very cautiously to patients with bulky tumors , considering the high incidence of serious late complications in patients with v ( td ) > 100 cm3 . 
 strahlentherapie und onkologie original article preoperative irradiation for prevention of heterotopic ossification following prosthetic total hip replacement results of a prospective study in 462 hips oliver koelbl1 , julia seufert1 , fabian pohl1 , annette tauscher2 , harald lehmann3 , hans - werner springorum2 , michael flentje1 background : the effectiveness of preor postoperative radiotherapy for prevention of heterotopic ossification ( ho ) following total hip replacement ( thr ) has already been demonstrated in the past . 
the purpose of this prospective study was to analyze the effectiveness of preoperative irradiation on the evening before surgery and to identify risk factors for ho in a homogeneous collective of patients . 
 patients and methods : from july 1997 to july 2001 , 416 patients ( 462 hips ; 235 males , 227 females ) received preoperative radiotherapy of the hip on the evening before surgery with a 7 - gy single fraction . 
sex , body height , hypertrophic osteoarthritis of higher degree , size of the femoral component of the prosthesis , previous ipsior contralateral ho , and short course of nonsteroidal anti - inflammatory drug ( diclofenac ) therapy significantly influenced the ho rate in univariate analysis . 
the cumulative dose of diclofenac ( 300 mg or > 300 mg ) within the first 7 postoperative days and previous ipsior contralateral ho influenced the incidence of ho in multivariate analysis . 
 conclusion : preoperative radiotherapy on the evening before surgery is an effective treatment modality to reduce overall ( brooker 14 ) and clinically relevant , severe hos ( brooker 34 ) , and includes several advantages compared to postoperative irradiation . 
 key words : total hip arthroplasty heterotopic ossification preoperative radiotherapy nonsteroidal anti inflammatory drugs strahlenther onkol 2003 ; 179 : 76773 doi 10.1007 / s00066 - 003 - 1088 - y properative bestrahlung zur vermeidung heterotoper ossifikationen nach totalendoprothetischem hftgelenkersatz . ergebnisse einer prospektiven studie an 462 hften hintergrund : die wirksamkeit einer proder postoperativen radiatio zur vermeidung heterotoper ossifikationen ( ho ) nach totalendoprothetischem hftgelenkersatz ( tep ) wurde in der vergangenheit bereits gezeigt . 
 patienten und methodik : von 07 / 1997 bis 07 / 2001 wurde bei 416 patienten ( 462 hften ; 235 mnner , 227 frauen ) eine properative einzeitbestrahlung der hfte mit einer dosis von 7 gy durchgefhrt . 
 1 clinic and policlinic for radiotherapy , university of wrzburg , germany , 2 orthopedic clinic , caritas hospital , bad mergentheim , germany , 3 insitute of radiology , caritas hospital , bad mergentheim , germany . 
geschlecht , krpergre , ausma der osteoarthritis , gre des prothesenschafts , vorherige ipsioder kontralaterale ho und die zustzliche gabe von nichtsteroidalen antiphlogistika ( diclofenac ) hatten in der univariaten analyse signifikanten einfluss auf die ho - rate . 
 schlsselwrter : totalendoprothese des hftgelenks heterotope ossifikationen properative bestrahlung nichtsteroidale antiphlogistika introduction heterotopic ossification ( ho ) is a well - known complication after total hip replacement ( thr )  . 
endogenous factors associated with the development of ho after tha include previous ho [ 7 ] , sex and age [ 2 , 23 ] , idiopathic skeletal hyperostosis [ 4 ] , ankylosing spondylitis [ 47 ] , and hypertrophic osteoarthritis [ 1 ]  . 
in 1975 , dahl [ 6 ] showed the effectiveness of nonsteroidal anti - inflammatory drugs ( nsaids ) for prevention of ho and in 1981 , coventry & scanlon [ 5 ] demonstrated that the incidence of ho was reduced by postoperative irradiation . 
postoperative irradiation includes the disadvantage of necessary patient transport from the orthopedic clinic to the department of radiotherapy on the 1st or 2nd postoperative day , which means pain caused by the transport and risk of luxation of the prosthesis . 
the procedure of early ( < 4 h before surgery ) preoperative irradiation , however , can result in logistic problems , if there is a greater distance between the department of radiotherapy and the orthopedic clinic . 
there are several reasons for this : the great number of possible risk factors as described above , which were not included into analysis of most studies , an additional therapy with nsaids , which was often not well documented and therefore depreciated the evaluation of the effectiveness of radiotherapy , the small number of studied hips diminishing the statistical validity , and the different time of irradiation , i.e. , immediately before surgery or on the evening before the day of surgery . 
 the purpose of this study was , therefore , to analyze a large , homogeneous collective of 462 operated hips and to evaluate the effectiveness of preoperative radiotherapy for prevention of ectopic ossification , to evaluate the effect of an additional therapy with nsaids , and to define risk factors for the development of ho . 
 patients and methods from july 1997 to july 2001 , 416 patients ( 462 hips ) received preoperative radiotherapy of the hip on the evening before surgery with a 7 - gy single fraction . 
 the following information was obtained for each patient : preoperative factors : age and sex ; height and weight ( obesity ) ; diagnosis of diseased hip ; previous surgery on the ipsior contralateral side ; previous ho on the ipsiand contralateral side , time between radiotherapy and surgery ( table 1 ) ; operative factors : type and size of prosthesis , operative approach to the hip , fixation of prosthesis , blood loss , duration of surgery ( table 2 ) ; postoperative factors : development of ho , antibiotic therapy , nsaid therapy , other analgesic therapy , hematoma , swelling in the operative area ( table 3 )  . 
the indications for radiotherapy were hypertrophic osteoarthritis ( 383 hips , 82.9% ) , replacement of the prosthesis ( n = 51 , 11.0% ) , other previous strahlenther onkol 2003 no . 
 definite osteophytes beginning joint space narrowing presence of two of the following : joint space narrowing , osteophytosis , subchondral sclerosis , cyst formation presence of three of the following : joint space narrowing , osteophytosis , subchondral sclerosis , cyst formation contralateral side . 
a standardized intraoperative antibiotic therapy ( 1.5 g cefotaxime ) was used in 253 patients ( 54.8% ) , 156 patients ( 33.8% ) were administered other antibiotic drugs ( table 2 )  . 
76.4% ( 353 / 462 ) received nsaid ( diclofenac ) as postoperative analgesic , 23.6% ( 109 / 531 ) at least for 3 days within the 1st postoperative week . 
 no soft tissue ossification separate small foci of ossification about the hip ossification projecting from the proximal femur or pelvis with at least 1 cm between opposing bone surfaces ossification projecting from the proximal femur or pelvis with < 1 cm between opposing bone surfaces ossification completely bridging the proximal femur and pelvis in 50 - mg increments . 
 the ( cid : 1 ) 2 - test of independence ( significance level : p - value < 0.05 ) was used to evaluate dependency in categorical and grouped numerical data . 
a stepwise logistic regression was performed . preoperative factors of the preoperative parameters shown in table 1 , sex , body height , hypertrophic osteoarthritis of higher degree , and previous ipsior contralateral ho significantly influenced the ho rate ( table 6 )  . 
 postoperative swelling or hematoma , additional or exclusive analgesic with tramadole - hcl or metamizole - sodium , postoperative antibiotic therapy , or pain 3 months after surgery did not correlate with ho . 
in the stepwise multivariate analysis , only the size of prosthesis kept its statistically significant influence on ho ( p = 0.04 ; table 6 )  . in the multivariate analysis , previous ipsior contralateral ho and therapy with > 300 mg diclofenac within the 1st postoperative week were independent variables influencing the incidence of ho ( table 6 )  . 
 ment modalities were analyzed regarding their effectiveness to reduce ossification after hip surgery : the use of nsaids [ 11 , 18 , 26 , 34 ] and radiotherapy [ 12 , 15 , 22 , 26 , 27 , 41 , 43 , 45 ]  . the inhibition of ho development by nsaids is probably due to a nonspecific suppression of the inflammatory response by inhibiting the prostaglandin synthesis mechanism [ 22 ]  . 
showing a comparable effectiveness , preoperative radiotherapy offers discussion with > 100 , 000 operations per year , thr is the surgical hip intervention most frequently performed in germany [ 14 ]  . 
although the incidence of ho ranges between 8% and 90% depending on risk factors [ 29 , 39 ] , a minority of patients with ho ( 1030% ) develop functional impairment [ 32 , 40 , 46 ]  . 
the large number of hip operations , however , leads to a significant number of patients with clinically relevant symptoms [ 31 ]  . the etiology of ho is still unknown . it is presumed that a protein called bone morphogenetic protein released by a loinflammacal prostaglandin - inducing tion is responsible for the process [ 13 , 25 , 37 , 40 ]  . 
preoperative irradiation for prevention of heterotopic ossification after thr additional advantages : no postoperative pain caused by transport , no risk of luxation of hip prosthesis , and lower costs because patients are transported by taxi and not by ambulance . 
many factors suggested to be predisposing in the literature are based on an analysis of patients not receiving prophylactic treatment [ 9 , 36 ] , a systematic analysis of ho risk factors in patients treated prophylactically is missing so far . 
while some authors report a correlation between ho and operative approach or kind of fixation ( cemented or uncemented ) [ 14 , 35 ] , others describe the converse [ 8 ]  . 
because of the homogeneity of surgical procedure in our study with all patients receiving anterolateral approach and uncemented fixation , this was not a point at issue in our analysis . 
hypertrophic coxarthrosis [ 10 ] was found to increase the incidence of ho . in our study , only patients with coxarthrosis of higher degree ( kellgren 34 ) developed severe ho ( brooker grade 34 )  . 
there are studies without any nsaid therapy being performed , in some nsaid therapy is only rarely applied during the initial postoperative period , and in others no statements concerning nsaid therapy are made [ 20 , 2628 , 46 ]  . 
neither the overall ho rate nor the incidence of clinically relevant , severe ho were increased as compared to historical data reported by studies analyzing postoperative radiotherapy , and preoperative radiotherapy includes several advantages compared to postoperative irradiation . 
 strahlentherapie und onkologie aktuelles forum langzeitergebnisse der postoperativen strahlentherapie des endometriumkarzinoms im stadium i oliver micke , frank bruns , gabriele halek , ulrich schfer , andreas schuck , normann willich1 hintergrund : im stadium i des endometriumkarzinoms steht die operative behandlung eindeutig im vordergrund . 
aufgrund retrospektiver untersuchungen ist der wert einer lokalen vaginalbestrahlung zur vermeidung von scheidenrezidiven relativ abgesichert . der wert einer zustzlichen externen bestrahlung des kleinen beckens ist unter bercksichtigung verschiedener prognostischer kriterien noch unklar . 
in dieser zeit erhielten , abhngig von den in der literatur anerkannten prognosefaktoren , 68 patientinnen eine alleinige high - dose - rate - ( hdr - ) brachytherapie und 60 patientinnen eine kombination aus perkutaner teletherapie und hdr - brachytherapie . 
die toxizitt war vor allem durch grad - 1und grad - 2nebenwirkungen gekennzeichnet , wobei chronische grad - 3 - / 4 - nebenwirkungen an darm und rektum in weniger als 4% der flle bei der kombiniert behandelten gruppe auftraten . 
mit schwerwiegenden nebenwirkungen ist bei einer kombinationsbehandlung nur in wenigen fllen zu rechnen . schlsselwrter : endometriumkarzinom postoperative strahlentherapie brachytherapie teletherapie strahlenther onkol 2003 ; 179 : 72936 doi 10.1007 / s00066 - 003 - 1059 - 3 long - term results of postoperative radiotherapy for stage i endometrial carcinoma background : surgical resection is the primary treatment in stage i endometrial carcinoma . 
the statistical analysis was performed as a retrospective cohort study . results : depth of tumor invasion and grading could be identified as statistically significant prognostic factors for local recurrence - free and tumor - specific survival . 
it could be shown that an additional external beam irradiation is indicated with a tumor invasion of more than 50% of the myometriuin the majority of cases grade i and ii radiation - associated side effects were observed . 
die wahrscheinlichkeit , dass eine blutung in der postmenopause durch ein karzinom verursacht ist , betrgt etwa 10% und weist eine altersabhngigkeit auf [ 27 ]  . folgende faktoren gelten beim endometriumkarzinom als prognostisch bedeutsam : tumorgre ( volumen ) , histologischer typ , histologischer differenzierungsgrad ( grading ) , myometrane infiltrationstiefe , lymphknotenmetastasen ( pelvin und paraaortal ) , gefeinbruch , metastasen im adnexbereich , ploidiestatus , hormonrezeptorstatus , begleiterkrankungen , art des tumorwachstums ( exooder endophytisch ) , kurze symptomzeit bzw . 
 von den 128 patientinnen wiesen 14 ( 10 , 9% ) das stadium ia , 55 patientinnen ( 43 , 0% ) das stadium ib und 59 patientinnen ( 46 , 1% ) das stadium ic gem der federation of gynecology and obstretics - ( figo - ) klassifikation von 1988 auf . histologisch war das adenokarzinom mit 122 / 128 fllen ( 95 , 3% ) mit abstand der hufigste tumor , gefolgt von dem adenosquamsen karzinom in drei fllen ( 2 , 3% ) , dem papillren ( adeno - ) karzinom in zwei fllen sowie dem adenokankroid in einem fall . 
aufgegliedert nach dem histopathologischen malignittsgrad ( grading ) hatten 53 patientinnen ( 41 , 7% ) einen g1 - tumor , 67 patientinnen ( 52 , 8% ) einen g2tumor und sieben patientinnen ( 5 , 5% ) einen g3 - tumor . 
in 103 fllen ( 80 , 5% ) erfolgte eine hysterektomie unter mitnahme beider adnexe ( he + ae ) , die in elf fllen ( 8 , 6% ) durch eine pelvine lymphknotenentfernung ( he + ae + lne ) ergnzt wurde . 
im anschluss daran erhielten 68 patientinnen ( 53 , 1% ) eine alleinige brachytherapie und 60 patientinnen ( 46 , 9% ) eine kombinierte teleund brachytherapie . brachytherapie die brachytherapie erfolgte in hdr - afterloadingtechnik ( iridium - 192 ) mit einem handelsblichen zylinderapplikator , wobei die dosierung auf 5 mm gewebetiefe bzw . 
bei 118 / 128 patientinnen , darunter 59 / 60 kombiniert behandelten , wurde eine gesamtdosis von 20 gy in drei fraktionen zu 7 / 7 / 6 gy , eine fraktion pro woche , ber die gesamte vaginallnge appliziert . in der gruppe der kombiniert behandelten patientinnen erhielt nur eine patientin ( 86 jahre ) eine mit 1 ( cid : 1 ) 7 gy reduzierte dosis . 
in der gruppe der mit alleiniger brachytherapie behandelten patientinnen erhielten zwei eine mit 14 gy ( 2 ( cid : 1 ) 7 gy ) reduzierte , vier eine mit 21 gy ( 3 ( cid : 1 ) 7 gy ) vergleichbare und drei wegen residualtumors am vaginalstumpf eine mit 2842 gy ( 46 ( cid : 1 ) 7 gy ) erhhte gesamtdosis . 
das zielvolumen beinhaltete in allen fllen das kleine becken , 52 patientinnen erhielten darber hinaus eine bestrahlung der paraaortalregion . die perkutanbestrahlung erfolgte bis 1991 in der regel bei allen patientinnen mit einem figo - stadium ic sowie bei allen g3 - tumoren ( n = 7 )  . 
nach 1991 erfolgte mit ausnahme von g3 - tumoren nach radikaler ( abdominaler ) hysterektomie berwiegend eine alleinige brachytherapie , so dass in dem hier betrachteten patientenkollektiv lediglich 41 / 59 patientinnen mit figo - stadium ic eine kombinierte strahlentherapie erhielten . 
patientinnen mit figo - stadium ib / g2 erhielten in abhngigkeit von der durchfhrung einer pelvinen lymphknotenentfernung , aber auch in abhngigkeit vom behandlungsjahr ( > 1991 ) in insgesamt 22 / 39 fllen eine alleinige brachytherapie . 
 die nachsorgeuntersuchungen , die gem den nachsorgeempfehlungen zunchst vierteljhrlich erfolgten , fanden interdisziplinr in der klinikeigenen nachsorgeambulanz sowie bei den niedergelassenen frauenund allgemeinrzten statt . letztere wurden zur vervollstndigung der follow - up - daten angeschrieben . 
dabei ist bei einem stadium ia der tumor auf das endometrium beschrnkt , bei stadium ib liegt eine invasion bis zur myometriummitte vor und bei stadium ic ist die myometriummitte berschritten . 
im rahmen dieser untersuchung erfolgte fr alle patientinnen , die nach der alten klassifikation von 1971 gruppiert worden waren , anhand der vorliegenden pathologieberichte eine retrospektive angleichung des tumorstadiums an die figoklassifikation von 1988 . 
 die ausprgungen alter ( gruppiert in dekaden ) , histologie , operationsart und die applizierte dosis der brachytherapie waren in den beiden behandlungsgruppen , alleinige brachytherapie und kombinationstherapie aus brachyund teletherapie , im ( cid : 1 ) 2 - test gleich verteilt . 
11 urban & vogel ergebnisse von allen 128 patientinnen entwickelten sieben ( 5 , 5% ) ein lokalrezidiv , weitere drei fernmetastasen , deren lokalisationen in tabelle 1 wiedergegeben sind . 
 die analyse erfolgte mit den faktoren , bei denen ein einfluss auf die lokalrezidivwahrscheinlichkeit anzunehmen ist . da patientinnen mit einer tumorinvasionstiefe ber 50% des myometriums und einem hohen histopathologischen malignittsgrad , wie aus der literatur bekannt , hufiger rezidivieren und daher auch hufiger eine kombinierte tele - / brachytherapie erhalten , lag ein ungleichgewicht der behandlungsgruppen in bezug auf diese beiden parameter vor . 
 brachykombinierte gesamt therapie therapie anzahl der patientinnen anzahl der patientinnen mit rezidiv anzahl der patientinnen ohne rezidiv 64 anzahl der patientinnen mit lokal rezidiv anzahl der patientinnen mit fern metastasen lokalrezidiv - lokalisationen vaginalstumpf beckenlymphknoten rektum peritoneum vaginalstumpf und beckenlymphknoten 2 fernmetastasen - lokalisationen lunge knochen * 100% 5 , 9% 94 , 1% 5 , 9% 1 , 5% 1 , 5% 1 , 7% 2 , 9% 100% 10 , 0% 90 , 0% 5 , 0% 5 , 0% 1 , 7% 1 , 7% 3 , 3% 1 , 7% 100% 7 , 8% 92 , 2% 5 , 5% 2 , 3% 0 , 8% 1 , 6% 0 , 8% 0 , 8% 1 , 6% 1 , 6% 0 , 8% micke o , et al . 
strahlentherapie beim endometriumkarzinom in stadium i die operationstechnik wurde im rahmen dieser untersuchung nicht stratifiziert , da insbesondere die mutmalich prognostisch bedeutsame pelvine lymphknotenentfernung nur bei einer minderheit der patientinnen ( n = 22 ) durchgefhrt wurde . 
alle patientinnen mit stadium ib ( n = 13 ) erhielten aufgrund des operativ besttigten pn0 eine alleinige brachytherapie ; acht von neun patientinnen mit stadium ic erhielten dessen ungeachtet eine kombinierte strahlentherapie . 
 fr jede ausprgung eines faktors wurde der unterschied zwischen den verschiedenen kurven univariat mit dem log - rank - test auf signifikanz getestet . eine match - pair - analyse wurde nicht durchgefhrt . 
 die figo - stadien ia und ib wurden zusammengefasst , um ein greres patientenkollektiv zu erhalten , sodass in dieser analyse lediglich in tumoren unterschieden wurde , die bis zu 50% des myometriums infiltrierten , und tumoren , die > 50% des myometriums infiltrierten . 
bei patientinnen , die einen tiefen myometriumbefall > 50% aufwiesen ( n = 74 ) , konnte gezeigt werden , dass die zustzliche teletherapie einen signifikanten einfluss auf das lokalrezidivfreie berleben hat ( p = 0 , 0324 ) : die mit alleiniger brachytherapie behandelten patientinnen ( n = 18 ) zeigten eine lokalrezidivfreie 1 - jahres - berlebensrate von 93 , 8% , eine 2 - jahres - berlebensrate von 80 , 4% und eine 5 - jahres - berlebensrate von 73 , 1% . 
fr patientinnen mit einem histopathologischen malignittsgrad g2 / 3 ( n = 74 ) ergab sich folgendes bild : die lokalrezidivfreie 1 - jahres - berlebensrate bei den patientinnen , die mit afterloadingtechnik behandelt wurden ( n = 32 ) betrug 96 , 9% , die 2 - jahres - berlebensrate 90 , 4% und die 5jahres - berlebensrate 86 , 8% . 
unbercksichtigt bei dieser analyse blieb das auftreten eines nicht tumorbedingten todes einer patient alle sieben patientinnen mit lokalrezidiv sind nach einem median von 2 , 3 monaten und einem mittelwert von 9 , 7 monaten verstorben . 
fr das lokalrezidivfreie berleben waren das figo - stadium ( mit myometriuminvasion ) , das grading und die strahlentherapiemodalitt bei einer tumorinvasionstiefe > 50% des myometriums ( tabelle 2 ) signifikant . 
 in der multivariaten cox - regression erwies sich allein die tumorinvasionstiefe als signifikant unabhngiger prognostischer faktor sowohl fr das lokalrezidivfreie als auch fr das tumorspezifische berleben ( p < 0 , 05 )  . 
es zeigt sich erwartungsgem ein hoch signifikanter unterschied zwischen den beiden behandlungsgruppen ( pakut = 0 , 001 im ( cid : 1 ) 2 - test , pchronisch = 0 , 031 im ( cid : 1 ) 2 - test )  . 
strahlentherapie beim endometriumkarzinom in stadium i tinnen akute nebenwirkungen an darm und rektum , davon 9 / 59 ( 15 , 3% ) mig bis starke ( akute ) grad - 2 - / grad - 3 - nebenwirkungen ; demgegenber traten bei keiner patientin , die eine alleinige brachytherapie erhielten , grad - 2 - / grad - 3 - nebenwirkungen an darm und rektum und nur bei 2 / 66 patientinnen ( 3% ) eine leichte darmirritation grad 1 auf . 
die zustzlich geplante brachytherapie konnte aber bei drei dieser patientinnen regulr beendet werden , so dass im bereich der mittellinienstrukturen eine mindestdosis von 43 gy erreicht wurde diese drei patientinnen haben bis zum stichtag der untersuchung rezidivfrei berlebt . 
die vierte und mit 86 jahren lteste patientin brach die kombinierte behandlung nach 32 gy ( 25 gy teletherapie + 1 ( cid : 1 ) 7 gy brachytherapie ) ab , sie verstarb nicht tumorbedingt 6 , 5 jahre nach therapieende . 
schwerwiegende nebenwirkungen an darm und rektum ( grad 3 und 4 ) fanden sich nur bei 4 / 112 patientinnen , darunter eine einzige patientin , die eine alleinige brachytherapie mit 20 gy erhielt . 
bei dieser patientin konnte nicht eindeutig ermittelt werden , ob die komplikation auf die vorangegangene strahlenbehandlung zurckzufhren war , jedoch konnten auch keine anderen ursachen fr eine darmobstruktion mit darmnekrose ermittelt werden . 
vornehmlich von gynkologischer seite wird dabei hufig die meinung vertreten , dass eine adquate operationstechnik mit sorgfltiger lymphknotendissektion fr die versorgung des endometriumkarzinoms und die metastasenprophylaxe im beckenbereich ausreicht eine strategie , die jedoch mit einer deutlich erhhten morbiditt in diesem frhstadium einhergeht [ 16 , 22 , 25 , 29 ]  . 
in abhngigkeit von dem postulierten risiko wird dann insbesondere der umfang der adjuvanten bestrahlung festgelegt mit dem ziel , eine optimale tumorkontrolle bei mglichst hoher lebensqualitt und mglichst geringer morbiditt zu erreichen [ 17 , 19 , 26 , 30 ]  . in der literatur werden die myometriale tiefeninvasion und der histopathologische malignittsgrad als wichtigste prognostische faktoren beschrieben , was auch unsere untersuchung besttigt . 
jedoch differieren die angaben zu der myometralen invasionstiefe in der literatur je nach betrachtungsweise des untersuchenden pathologen bei der beschreibung des ausmaes der wandinfiltration und der gewhlten tnmklassifikation [ 11 , 12 ]  . 
demgegenber weisen g1 - tumoren im stadium ic eine inzidenz von 15% an pelvinen lymphknotenmetastasen auf , die mit steigendem grading bei g3 - tumoren lediglich auf 24% anwchst [ 5 ]  . 
 seit einigen jahren wird zur vereinfachung der risikoabschtzung von einigen autoren die bildung von so genannten risikoscores fr das operierte endometriumkarzinom propagiert , mit deren hilfe das erforderliche ausma der adjuvanten postoperativen strahlentherapie festgelegt werden soll , um eine berbzw . 
277 patientinnen erhielten darber hinaus keine weitere therapie ( kontrollgruppe ) ; 263 patientinnen erhielten zustzlich eine perkutane beckenbestrahlung mit 40 gy , wobei nach einer dosis von 20 gy ein mittelblock eingesetzt wurde . 
in einem zeitraum von 310 jahren fand sich in der gruppe , die zustzlich perkutan bestrahlt worden war , eine signifikante verbesserung der lokalen kontrolle mit einer lokalrezidivfreien 10 - jahres - berlebensrate von 98 , 1% gegenber 93 , 1% in der kontrollgruppe bei gleichverteilung der prognostischen faktoren in beiden therapiegruppen . 
das gesamtberleben wurde zwar durch diesen sachverhalt nicht verbessert , die subgruppenanalyse zeigte jedoch in der tendenz einen berlebensvorteil fr patientinnen mit g3 - tumoren und einer myometralen tiefeninvasion > 50% bei zustzlicher perkutanbestrahlung [ 1 ]  . 
 die krzlich publizierten ergebnisse der ebenfalls prospektiv randomisierten portec - ( post - operative radiation therapy in endometrial cancer - ) studie zeigen ebenfalls keine verbesserung des gesamtberlebens bei durchfhrung einer postoperativen beckenbestrahlung im figo - stadium ib / g23 und ic / g12 trotz verbesserter lokaler kontrolle . auch in dieser studie wurde auf ein chirurgisches lymphknotenstaging verzichtet . 
nach einbringung von 715 patientinnen und einer medianen nachbeobachtungszeit von 52 monaten fand sich eine lokalrezidivfreie 5 - jahres - berlebensrate von 96% gegenber 86% in der kontrollgruppe ; interessanterweise traten drei viertel der rezidive dabei in der scheide auf [ 2 , 6 ]  . 
patientinnen erhielten immer dann eine zustzliche perkutane ( kobalt - 60 - ) bestrahlung mit 56 gy , wenn eine tumorinvasion eines g2 - / g3 - tumors in das mittlere drittel des myometriums ( stadium ib ) vorlag oder wenn ungeachtet des gradings das uere drittel des myometriums erreicht war ( stadium ic )  . 
alle anderen patientinnen , die ungeachtet des gradings eine tumorinvasionstiefe bis zu ein drittel des myometriums ( stadium ia ) oder bei einem histopathologischen malignittsgrad g1 bis zu zwei drittel des myometriums ( stadium ib ) aufwiesen , erhielten eine intrakavitre hdr - brachytherapie mit einer dosis von 14 gy . 
diese ergebnisse mssen allerdings vor dem hintergrund , dass es sich um eine retrospektive analyse handelt und eine subgruppenanalyse hinsichtlich des operativen vorgehens ( insbesondere bezglich einer zustzlich durchgefhrten pelvinen lymphknotenentfernung ) aufgrund zu kleiner fallzahlen nicht sinnvoll war , zurckhaltend interpretiert werden . 
dennoch kann man festhalten , dass unsere ergebnisse im einklang mit den oben beschriebenen studien [ 1 , 6 , 13 , 20 ] stehen , die eine zustzliche perkutane strahlentherapie des beckens bei einer tumorinvasionstiefe von > 50% des myometriums empfehlen , auch wenn eine statistisch signifikante verbesserung des gesamtberlebens dadurch wahrscheinlich nicht erreicht werden kann . 
1983 ber systematische untersuchungen von creasman & delgado [ 18 ] , die eine ansteigende inzidenz von paraaortalen lymphknotenmetastasen beim endometriumkarzinom von 3 , 5% im stadium ia / g2 bis 46% ( ! ) im stadium ib / g3 beobachtet haben , und folgerten , dass eine adjuvante paraaortalbestrahlung bei hochrisikopatientinnen durchaus gerechtfertigt sei . 
 [ 31 ] relativierten daher die indikation zur adjuvanten paraaortalbestrahlung bei hochrisikopatientinnen mit endometriumkarzinom im stadium i zurecht insofern , als sie eine histologische abklrung von suspekten befunden aus der damals noch blichen lymphangiographie forderten und eine extended - field - bestrahlung nur bei histologischer besttigung empfahlen . 
trotz hufiger grad - 1und grad - 2 - nebenwirkungen insbesondere an darm und rektum traten nur vereinzelt schwerwiegende grad - 3 - / 4 - nebenwirkungen nach kombinierter strahlentherapie auf . 
unsere ergebnisse stehen somit im einklang mit den von anderen autoren [ 9 , 10 , 20 , 24 , 32 , 33 , 34 ] beschriebenen raten an schweren komplikationen nach postoperativer perkutanbestrahlung des beckens , wie z.b. 
dies deckt sich mit den angaben aus der lteren literatur , die bei hinzunahme der paraaortalregion in das zielvolumen der perkutanbestrahlung keine erhhung der komplikationsrate am dnndarm sah , wenn paraaortal eine gesamtdosis von 4550 gy nicht berschritten wurde [ 18 , 31 ]  . 
creutzberg cl , van putten wl , koper pc , et al . , for the portec study group . surgery and postoperative radiotherapy versus surgery alone for patients with stage i endometrial carcinoma : multicenter randomized trial . 
 korrespondenzanschrift oliver micke klinik und poliklinik fr strahlentherapie radioonkologie universittsklinikum mnster albert - schweitzer - strae 33 48129 mnster deutschland telefon ( + 49 251 ) 8347 - 839 , fax - 355 e - mail : omicke@uni - muenster.de strahlenther onkol 2003 no . 
11 urban & vogel strahlentherapie und onkologie original article qualittssicherung im stereotaktischen raum bestimmung der genauigkeit von ort und dosis bei ein - zeit - bestrahlungen andreas mack1 , gnther mack2 , dirk weltz3 , andreas hnes4 , anja jess5 , berndt wowra5 , heinz czempiel6 , bernd heck6 , hans - jrg kreiner6 , volker seifert7 , heinz bttcher8 hintergrund : ein - zeit - bestrahlungen in der stereotaxie erfordern methoden der qualittssicherung von hoher przision . 
 material und methoden : ein qualittssicherungspaket wurde entwickelt , das den anforderungen der e - din 6875 - 1 [ 38 ] gengt . es besteht aus einem vielseitig verwendbaren przisionsphantom , einem dosismesssystem fr den gewebequivalenten radiochrom - film gafchromic typ md 55 mit hochwertigem scanner und vielseitiger , nutzerfreundlicher software fr standardisierte testroutinen . 
die einfache handhabung erlaubt den einsatz fr die tgliche routine ( nach e - din 6875 - 1 [ 38 ] ) , aber auch fr die modellierung komplizierter dreidimsionaler streuverhltnisse , z.b. 
 schlsselwrter : qualittssicherung ( quasir ) radiochirurgie stereotaxie systemtest dosimetrie kleiner felder filmdosimetrie strahlenther onkol 2003 ; 179 : 7606 doi 10.1007 / s00066 - 003 - 1068 - 2 quality assurance in stereotactic space . 
the complete operational sequence of a treatment from imaging over irradiation planning up to the patient irradiation has to be controlled and verified in a phantom ( figure 2 )  . 
it consists of versatile usable precision phantom ( figure 1 ) , a dose measuring system for the tissue equivalent radiochromic film gafchromic type md 55 ii using a high - quality scanner , and a software for standardized test routines ( figures 2 to 4 )  . 
the simple handling permits the employment for the daily routine ( according to e - din 6875 - 1 [ 38 ] ) , in addition , for the modelling of complicated 3 - d of scattering conditions , e.g. 
um das behandlungsrisiko minimal zu halten , sind hohe genauigkeit und reproduzierbarkeitgefordert : die geometrischen positionen mssen przise bekannt sein und die gesamtabweichung der kette an unsicherheiten von der bildgebung bis zur bestrahlung bzw . 
qualittskontrolle muss unter 1 mm liegen [ 14 ] , denn ein - zeit - bestrahlungen sind nicht korrigierbar und die vervollstndigung unterbrochener behandlungen haben nachteilige auswirkungen auf den patienten [ 21 , 22 ]  . 
fr die tgliche anwendung sollten messungen einfach , schnell und mit hoher sicherheit und genauigkeit durchzufhren se da entsprechende komplette systeme kommerziell nicht erhltlich und auch in der literatur nicht beschrieben sind , wurde ein qualittssicherungspaket entwickelt [ 16 ]  . 
in dem vorliegenden beitrag werden komponenten sowie tests beschrieben und diskutiert , die sich an dem qualittsstandard nach e - din 6875 - 1 [ 38 ] fr perkutane stereotaktische bestrahlung orientieren . 
 material und methoden das qualittssicherungspaket , im folgenden quasir genannt ( quality assurance system in radiosurgery ) , basiert auf folgenden prozeduren : messungen von dosen und rumlichen dosisverteilungen erfolgen mit den gewebequivalenten und selbst entwickelnden gafchromic - filmen , die mit einem hochwertigen trommelscanner ausgewertet werden . 
 komponenten des systems detektor detektoren fr die radiochirurgie sollten geeignet sein fr gebiete mit hohen dosisgradienten und fr kleine feldgren [ 10 , 11 , 13 ] ( 0 , 52 cm und kleiner ) , in denen sich kein sekundr - elektronengleichgewicht aufbaut [ 19 ]  . 
weiterhin sollte der detektor integrierend messen , da die dosis unter umstnden in portionen appliziert wird ( fraktionierte bestrahlungen , bgen und mlc [ multileafkollimator ] fr den beschleuniger ) , und keine nennenswerte richtungsabhngigkeit [ 35 ] zeigen ( 201 einzelstrahlen beim gamma knife [ 34 ] ) , bei gleichzeitiger gewebequivalenz . 
probleme treten bei kleinen energien ( hohe filmempfindlichkeit ) , bei groen feldgren und bei greren tiefen auf , da sich dort die zusammensetzung des spektrums aufgrund von sekundr gestreuten photonen kleinerer energie verndert [ 13 , 17 , 20 , 30 , 31 ]  . 
verschiedene effekte [ 16 , 24 ] wurden untersucht und werden durch standardisierte messverfahren und spezielle algorithmen bercksichtigt : nichtlinearitt der einfrbung mit der bestrahlungsdosis , abhngigkeit der lichtabsorption von der temperatur , nachdunkelung der einfrbung mit der zeit sowie empfindlichkeit gegenber uv - licht . 
 scanner zur filmauswertung wurde der trommelscanner imacon flex tight precision ii ( auflsung bis zu 5760 dpi ) gewhlt , im roten farbkanal getestet und modifiziert [ 4 , 25 ]  . 
die des kopfes zu bercksichtigen , braucht man messanordnungen , mit denen solch komplizierte streuverhltnisse nachgebildet werden knnen . dazu dient ein kugelfrmiges kopfphantom mit 16 cm durchmesser , bestehend aus zwei halbkugeln und einer zentralen aussparung von 7 , 2 cm3 , die platten verschiedener materialien und dicken sowie einstze fr alle handelsblichen messkammern fr stereotaxie , fr tdls , alanindosimeter und vor allem fr filme und filmstapel aufnehmen kann ( abbildung 1 )  . 
das kopfphantom kann entweder mittels fiducialboxen in der computertomographie ( ct ) und magnetresonanztomographie ( mri ) zuerst sichtbar gemacht und dann positioniert werden oder im falle der verifikation eines vorab berechneten dosisplans direkt im stereotaktischen rahmen eingespannt und justiert werden . 
 standardisierte messverfahren global system test dieser test quantifiziert die gesamtgenauigkeit des systems ( bildgebung plus radiochirurgisches system ) mittels einer ein - zeit - bestrahlung im isozentru die berprfung geschieht mit einem radiochromen film ( gafchromic ) , der im zentrum mit einem aufgedruckten doppelkreuz ( cid : 1 ) markiert ist . 
er wird zwischen zwei platten ( plexiglas oder teflon ) positioniert , in welchen jeweils ein im mrund ct - bild 2 eingearbeisichtbares kapillares kreuz gefllt mit cuso4 tet ist ( abbildung 1 )  . 
weiterhin gehrt ein spezielles mr - phantom mit 145 quidistant angeordneten stben mit einer auswertesoftware zum quasir - paket , um abweichungen und inhomogenitten der gradientenfelder des mri abbildung 2 . 
systemtest fr die radiochirurgie kreuztest : ein mit einem doppelkreuz ( cid : 1 ) bedruckter gafchromic - film eingelegt zwischen den beiden kapillarkreuz - einstzen des kugelphantoms durchluft im kopfphantom alle schritte der radiochirurgischen behandlung . 
dieser teil wird gegenstand einer weiteren verffentlichung se l - test fr die wahl der geeignetsten stereotaktischen bestrahlungstechnik wird eine kleine , irregulr geformte , knstliche lsion mglichst exakt durch die rumliche dosisverteilung nachgebildet und verifiziert . 
l - test : das vorgegebene zielvolumen mit den dimensionen 12 mm ( cid : 1 ) 8 mm ( cid : 1 ) 4 mm ( a ) wurde im planungssystem berechnet ( b ) und experimentell verifiziert . 
the screenshot shows dose distributions and profiles on the basis of absolute dose measurements ( c ) and the representation as a 21 / 2 - d doseplot ( d )  . 
 empfindlichkeitsfunktion die farbdichte wchst im allgemeinen nicht linear als funktion der dosis , da das absorptionsspektrum mit der dosis variiert und bei hohen dosen sttigung eintritt [ 7 , 12 ]  . 
verifikation der dosisplanung anhand eines akustikusneurinoms ( an ) : die filme liegen in einem stapel zwischen den einstzen ( a ) und werden im phantom gem den daten im protokoll bestrahlt . 
das an wurde geplant ( b ) und die filme analysiert der bildschirmausdruck zeigt absolut gemessene dosisverteilungen in verschiedenen ebenen ( c ) sowie die 3 - d - darstellung der dazugehrigen dosisverteilung ( d )  . 
verification of a calculated dose plan for an acoustic neurinoma ( an ) : the films are embedded between the slabs and inserted into the phantom ( a ) which is adjusted according to the data in the protocol . 
 ortsauflsung da gafchromic - filme frei von limitierender korngre sind , ist die ortsauflsung in der filmebene nur durch die pixelgre und durch die przision der positionierung des films limitiert . 
dann kann er in das phantom eingesetzt werden , entweder zwischen den zwei kreuzeinstzen fr die berprfung der treffsicherheit , zwischen den l - einstzen fr messungen des dosisgradienten oder als filmstapel zur verifikation von dosisverteilungen . das phantom mit eingebetteten filmen , eingespannt im stereotaktischen rahmen , luft nun durch alle schritte : bildgebung , definition des targets , planung bis hin zur einstellung der koordinaten und der eigentlichen bestrahlung gem den planungsdaten im protokoll ( abbildungen 2 und 3a bis 3d )  . absolute dosismessungen ( doppelbelichtungsverfahren ) fr absolute dosismessungen wird pro filmpackung eine kalibrierung durchgefhrt . 
neben der berprfung einzelner geometrischer parameter , insbesondere der gesamtgenauigkeit des systems , ist es mittels eines filmstapels mglich , vorab berechnete dreidimensionale dosisverteilungen mit einer unsicherheit von 3% zu bestimmen . 
die verwendung des kopfphantoms fr die radiochirurgie ist vielseitig , da es mit unterschiedlichen einstzen ausgestattet werden kann , um knochenstrukturen , gewebe und luft in komplizierten lokalisationen zu simulieren . 
mit diesem systems knnen folgende genauigkeiten erreicht werden : positionierung < 0 , 05 mm in filmebene und unsicherheiten der dosismessung < 3% im dosisbereich von 1065 gy , fr kleine dosen ( 210 gy ) ~ = 5% . das system ist fr routinemessungen nach den qualittsforderungen der e - din 6875 - 1 [ 38 ] entwickelt und geeignet . 
 diskussion aufgrund unserer erfahrung und der von experten anderer zentren sollten durch qualittssicherungsmanahmen im wesentlichen drei kritische fragestellungen der radiochirurgie abgedeckt sein : zum einen messungen der geometrischen positionen und somit die qualitt bzw . 
das 8 - gyund das 10 - gy - volumen als ma fr eine toleranzdosis , wichtig . die quasir - ausrstung kann auch zu anderen zwecken verwendet werden , z.b. 
zur berprfung der genauigkeit der dosisberechnung fr extreme positionen wie im falle der augentumoren ( aderhautmelanome ) oder zum testen der auswirkungen von plugs oder sonstigen modifikatoren des strahlenfeldes ( keile , blcke , kompensatoren )  . 
das system quasir kann zur berprfung von dosisplanungen auch fr superponierte und fraktioniert gegebene felder hinsichtlich dosis und position sowie fr reproduzierbarkeit von lokalen dosen und anderen anwendungen fr quasir und forschung eingesetzt werden . 
use of a new type of radiochromic film , a new parallel - plate micro reccanello - chamber , mosfets , and tld 800 microcubes in the dosimetry of small beams . 
andreas mack gamma knife zentrum / gkf - gmbh schleusenweg 216 , nebengebude 95 60528 frankfurt deutschland telefon ( + 49 / 69 ) 677 359 14 , fax - 11 e - mail : a.mack@gkfrankfurt.de strahlenther onkol 2003 no . 
11 urban & vogel strahlentherapie und onkologie original article radiogene hodenbelastung durch streustrahlung bei adjuvanter 3 - d - beckenbestrahlung nach anteriorer resektion beim rektumkarzinom einfluss auf die fertilitt marc d . 
 ergebnisse : die mittlere gonadendosis aller 18 patienten pro bestrahlungsfraktion betrug 0 , 057 gy ( median 0 , 05 gy ) , wobei die mittelwerte der einzelnen patienten zwischen 0 , 035 und 0 , 114 gy lagen . 
nach 28 fraktionen , 50 , 4 gy entsprechend , errechnete sich kumulativ eine gesamtdosis am hoden von 1 , 60 gy ( 0 , 983 , 19 gy )  . 
 schlsselwrter : gonadenbelastung gonadendosis in - vivo - dosimetrie infertilitt strahlentherapie strahlenther onkol 2003 ; 179 : 7549 doi 10.1007 / s00066 - 003 - 1108 - y male gonadal dose in adjuvant 3 - d - pelvic irradiation after anterior resection of rectal cancer . 
 patients and method : we measured the scattered gonadal dose of 18 patients in vivo with thermoluminescence detectors , which were fixed on four defined points on the scrotum during radiation on three consecutive days . 
if gonadal total doses exceed 1.5 gy a substantial increase in irreversible azoospermia must be expected . with respect to the data reported in the literature our measured mean gonadal total dose of 1.60 gy will lead with high probability to an irreversible infertility . 
because of the small number of patients in our study , the data must be interpreted with caution , 1 abteilung fr klinische radiologie , radiologische klinik der universitt heidelberg . 
the possibility of sperm cryoconservation should be discussed with the patient . key words : gonadal dose in - vivo - dosimetry infertility radiotherapy einleitung das rektumkarzinom gehrt zu den hufigsten malignomen , wobei nicht selten jngere mnner erkranken . 
 patienten und methode wir fhrten bei 18 patienten , die zwischen november 2000 und august 2002 eine perkutane bestrahlung des beckens erhielten , mithilfe von thermolumineszenzdetektoren ( tld ) in - vivo - messungen zur bestimmung der streustrahlenbedingten gonadendosis durch . 
die untere feldgrenze wurde in projektion auf die sitzbeinunterkante gewhlt , wobei hier individuell patientenabhngig sowie tumorstadienund tumorsitzabhngig anpassungen von bis zu 1 cm in kraniale oder kaudale richtung vorgenommen wurden . 
die adjuvante postoperative bestrahlung des beckens erfolgte mit einer einzeldosis von 1 , 8 gy tglich , fnfmal wchentlich appliziert , bis zu einer gesamtdosis von 50 , 4 gy . 
 ergebnisse die mittlere gonadendosis aller 18 patienten pro bestrahlungsfraktion betrug 0 , 057 gy ( median 0 , 05 gy ) , wobei die mittelwerte der einzelnen patienten zwischen 0 , 035 und 0 , 114 gy lagen . 
bei einer angestrebten gesamtdosis von 50 , 4 gy errechnete sich kumulativ eine durchschnittliche gesamtdosis am hoden von 1 , 60 gy ( 0 , 983 , 19 gy )  . 
die patienten mssen tglich angewiesen werden , das genitale mglichst weit nach kaudal zu verlagern , um einen optimal weiten abstand des hodens vom kaudalen rand des bestrahlungsfeldes zu gewhrleisten . 
die perkutane bestrahlung des beckens gehrt im rahmen neoadjuvanter oder adjuvanter therapieregime zur behandlung von rektumkarzinomen im stadium ii und iii in kombination mit 5 - fu und folinsure zur standardtherapie [ 5 , 14 , 16 , 30 ]  . 
nach den daten des seer sind 17 , 9% der patienten bei diagnosestellung unter 55 jahre , 5 , 8% unter 45 jahre und 1 , 3% unter 35 jahre alt [ 27 ]  . 
es muss konstatiert werden , dass die anzahl der mnnlichen patienten , die in einem alter an einem rektumkarzinom erkranken , in dem der kinderwunsch respektive die fertilitt noch eine bedeutsame rolle spielt , nicht zu vernachlssigen ist . 
um das durch eine bestrahlung des beckens bedingte risiko einer infertilitt abschtzen zu knnen , was unter anderem fr das aufklrende gesprch mit dem patienten sehr wichtig ist , ist es notwendig , die streustrahlendosis an den gonaden zu kennen . 
das phnomen des negativen fraktionierungseffekts wurde von regaud & nogier [ 25 ] 1911 erstmals beschrieben . regaud & nogier [ 25 ] stellten fest , dass die fraktionierte bestrahlung auf das mnnliche keimepithel einen strkeren einfluss hat als die mit hherer gesamtdosis applizierte einmaldosis . 
nach einzeitdosen von 2 bis 3 gy erholt sich die spermatogenese nach clifton & brenner [ 4 ] erst nach 18 bis 30 monaten , oberhalb von 4 gy nach 5 jahren und lnger [ 24 ]  . 
auch nach applikation einer einzeitigen dosis von mehr als 6 gy ist nach initial sicherer azoospermie noch eine partielle erholung des keimepithels mglich [ 7 , 11 , 20 , 34 ]  . 
 [ 33 ] wiesen bei drei von sieben patienten , die eine hodenstreudosis von 0 , 2 < 0 , 3 gy fraktioniert erhielten , passagere fsh - erhhungen als zeichen einer verminderten spermatogenese nach . 
nach den ergebnissen von greiner ist nach gonadengesamtdosen von bis zu 1 gy bei tglichen einzeldosen von 0 , 030 , 05 gy eine komplette erholung der spermatogenese kaum gefhrdet [ 7 ]  . 
bei allen patienten mit testikulren gesamtdosen von 1 , 69 gy oder mehr und einzeldosen von ber 0 , 09 gy wurde von greiner [ 7 ] eine irreversible azoospermie gesehen . 
 der grenzwert , ab dem mit einem permanenten sistieren der spermienproduktion zu rechnen ist , wird in einer literaturzusammenstellung von gruber & schwegler [ 10 ] mit 1 , 2 bis 3 gy angegeben . 
von greiner [ 7 ] und anderen autoren [ 10 , 13 , 18 , 26 ] wird eine erholung der spermatogenese oberhalb von 1 , 5 gy als zunehmend unmglich angesehen . 
 [ 32 ] zeigten an fnf patienten , dass nach einer bestrahlung des hodens mit einer gesamtdosis von 13 gy bei einzeldosen von 1 , 3 gy nach 2 jahren eine normalisierung des luteinisierenden hormons und des testosterons bei allen patienten erreicht war . 
die bestrahlung erfolgte standardmig bis 50 , 4 gy ( 28 fraktionen )  . nach 45 gy ( 25 fraktionen ) wurde zur kompletten dnndarmschonung eine umstellung der bestrahlungstechnik ( s.o. ) auf seitlich opponierende und kranial verkrzte gegenfelder durchgefhrt . 
obwohl die ergebnisse aufgrund der kleinen patientenzahl zurckhaltend zu beurteilen sind , scheint der einfluss der streustrahlung auf die fertilitt bei einer standardmigen bestrahlung des beckens mit 50 , 4 gy eindeutig zu se in die betrachtung der sexuellen dysfunktion , hier fertilittsstrung als folge der adjuvanten strahlentherapie , mssen die mglichen postoperativ bedingten dysfunktionen mit einbezogen werden . 
die totale mesorektale exzision ( tme ) die erwiesenermaen zu einer senkung der lokalrezidivrate fhrt [ 19 ] , kann auch die rate an postoperativen sexuellen dysfunktionen senken [ 21 , 23 ]  . 
der patient muss zwingend chirurgischerseits , trotz einer verbesserung der situation durch tme , ber mgliche sexuelle dysfunktionen wie die impotentia coeundi oder ejakulationsstrungen und strahlentherapeutischerseits ber die hohe wahrscheinlichkeit der infertilitt aufgeklrt werden . 
wenngleich die chance der konzeption post radiotherapie sicher sehr klein ist , sollte der patient angehalten werden , fr mindestens 6 monate , besser 1 jahr , eine kontrazeption durchzufhren , um sicherzustellen , dass es wenn noch mglich sicher zu einer reifung von spermatozoen ohne therapiebedingte chromosomale lsionen kommt [ 1 , 17 ]  . 
die mglichkeit einer prtherapeutischen spermakryokonservierung sollte mit dem patienten besprochen werden . bei unseren messwerten gab es einige ausreier , die zeigen , dass im ungnstigen fall eine deutlich hhere strahlendosis am hoden mglich ist als die von uns errechnete kumulative dosis von 1 , 60 gy . 
es ist notwendig , die patienten regelmig anzuweisen , das genitale mglichst weit nach kaudal zu verlagern , um einen optimal weiten abstand des hodens vom kaudalen rand des bestrahlungsfeldes zu gewhrleisten . 
auch die hodenlagerung , die in unserer untersuchung , wie an einigen ausreierwerten erkennbar , wohl problematisch war , ist bei der bestrahlung in bauchlage im lochbrett schlechter reproduzierbar als z.b. 
 schlussfolgerungen die von uns ermittelte gonadendosis von 1 , 60 gy in einzelfraktionen von 0 , 057 gy durch eine adjuvante perkutane bestrahlung des beckens nach rektumkarzinomoperation fhrt nach den daten der literatur mit einer sehr hohen wahrscheinlichkeit zur infertilitt . 
11 urban & vogel strahlentherapie und onkologie original article therapeutic outcome and prognostic factors in the radiotherapy of recurrences of cervical carcinoma following surgery andrea hille , elisabeth weiss , clemens f . 
 key words : cervical carcinoma recurrences radiotherapy prognostic factors strahlenther onkol 2003 ; 179 : 7427 doi 10.1007 / s00066 - 003 - 1100 - 6 therapieergebnisse und prognosefaktoren bei der radiotherapie von zervixkarzinomrezidiven nach operation ziel : analyse der effektivitt einer radiotherapie bei rezidiven eines zervixkarzinoms nach primrer operation . 
in abhngigkeit von der tumormasse und der rezidivlokalisation ( tabelle 1 ) wurde eine perkutane bestrahlung oder eine kombination mit intrakavitrer brachytherapie bis zu einer gesamtdosis von 5065 gy appliziert . 
 ergebnisse : die 5 - jahres - berlebensrate lag bei allen patientinnen bei 28% , das ereignisfreie berleben bei 24% , die lokale kontrolle bei 48% ( abbildung 1 )  . 
im fall einer kompletten oder nur mikroskopisch inkompletten resektion lag die 5 - jahres - berlebensrate bei 67% , bei makroskopischem resttumor lebte nach 37 monaten keine patientin mehr ( p = 0 , 05 ; abbildung 2 )  . 
alle patientinnen , die mit kombinierter radiotherapie behandelt wurden , berlebten , whrend keine patientin mit alleiniger externer bestrahlung nach 32 monaten lebte ( p = 0 , 01 )  . 
 schlussfolgerung : die chance , zervixkarzinomrezidive zu kontrollieren , ist abhngig von der tumormasse , der mglichkeit einer vollstndigen operativen entfernung und / oder der mglichkeit , eine brachytherapie durchzufhren . 
 schlsselwrter zervixkarzinom rezidive radiotherapie prognosefaktoren 1 department of radiotherapy , university of gttingen , germany . received : september 18 , 2002 ; accepted : july 3 , 2003 strahlenther onkol 2003 no . 
outcome and prognosis in radiotherapy of recurrent cervical carcinoma introduction a recurrence rate of about 1025% has to be expected in early carcinoma of the cervix following primary surgery [ 25 , 35 , 37 , 38 ]  . 
the prognosis of patients with recurrences following radical surgery is poor [ 5 , 21 , 22 , 42 , 44 ] , reports with regard to prognostic factors are sparse . 
 patients and methods between 1989 and 1999 , 26 patients of the university hospital in gttingen , germany , underwent radiation therapy for recurrences of cervical carcinoma following primary surgery . 
 the primary stages according to the international federation of gynecology and obstetrics ( figo ) classification were stage ia / b 18 times , stage iia / b eight times . 
 the surgical procedures in the primary situation consisted of wertheim - meigs surgery ( corresponding to radical hysterectomy piver iii / iv ) in 21 patients and simple hysterectomy in five . 
two patients had undergone vaginal brachytherapy for close margins after wertheim - meigs surgery ( corresponding to radical hysterectomy piver iii / iv )  . 5 ( cid : 1 ) 8 gy had been given to a patient with stage iia , another patient with stage ib had undergone brachytherapy with 3 ( cid : 1 ) 6 and 1 ( cid : 1 ) 4 gy . 
17 patients had inoperable tumors or macroscopic residual tumor following surgery of the recurrence . three patients had a microscopically incomplete surgery and six a complete tumor resection . external - beam radiotherapy was given using 16 - mev and 20 - mev accelerators ( sl 75 / 20 , phillips , eindhoven , the netherlands , and 2300 c / d , varian , palo alto , usa )  . 
brachy therapy was performed using high - dose - rate ( hdr ) remote afterloading machines with an iridium - 192 ( 192ir ) source ( buchler mc , buchler , braunschweig , germany , and varisource , varian ) in a linear source arrangement . 
a boost of 9 gy ( single dose 1.8 gy ) was given in case of tumors at the pelvic wall , sometimes with midline blocking respecting the afterloading applicator , sometimes without midline blocking . 
patientinnen mit hochrisikofaktoren in der primrsituation und lokalisation des rezidivs . high risk factors in the primary situation ( n ) site and extent of recurrence ( n ) time to recurrence ( months ) 21 ( 251 ) lymph - / hemangiosis ( 3 ) positive pelvic lymph nodes ( 5 ) bulky disease ( > 3.5 cm ) ( 2 ) parametric involvement ( 6 ) central without infiltration of the pelvic wall ( 16 ) vagina paravaginal tissue only ( 7 ) with infiltration of the wall of rectum or bladder ( 4 ) with infiltration of the lymph nodes ( 5 ) iliac lymph nodes ( 1 ) iliac and inguinal lymph iliac and paraaortic lymph nodes ( 1 ) nodes ( 3 ) central with infiltration of the pelvic wall ( 10 ) without lymph nodes ( 9 ) with lymph nodes ( 1 ) strahlenther onkol 2003 no . 
 the dose specification for all three groups was to the 90% isodose until 12 / 1995 and from 01 / 1996 on until now according to icru 50 recommendations [ 17 ]  . 
 most of the patient information was available from the medical files , part of the information either from mail or phone call with the referring physician or through direct communication with patients or relatives . 
the estimated 5 - year pelvic control rate was 64% in case of surgery without residual tumor and in case of microscopic tumor and 30% in case of macroscopic tumor or inoperability . 
central recurrences had an estimated 42% 5 - year overall survival and a 48% pelvic control rate , whereas recurrences with pelvic wall results survival and recurrences of all patients , 14 ( 54% ) had a tumor relapse . 
the time to recurrence after primary therapy was 375 months ( 26 months ) and the time to relapse or progress after therapy of the recurrence was 237 months ( 11 months )  . the incidence of failure , time to relapse , and locations of failure following therapy of the recurrences are summarized in table 2 . 
one patient with relapse localized at the pelvic wall and radiotherapy of the pelvis with 39.6 gy and a boost to the pelvic wall suffered from paraaortic lymph node metastases after 22 months . despite irradiation of the paraaortic nodes with 50 gy , pulmonary metastases occurred after another 14 months . 
 the therapeutic outcome of the whole group was as follows ( table 3 and figure 1 ) : the estimated 5 - year overall survival , relapse - free survival , and pelvic control were 28% , 24% , and 48% , respectively . 
 number of 5 - year overall 5 - year relapse5 - year pelvic patients free survival survival control whole group resection without or with only microscopic residual tumor r0 or r1 no resection or r2 site and extent of recurrence central without infiltration of the pelvic wall vagina paravaginal tissue only all others central with infiltration of the pelvic wall strahlenther onkol 2003 no . 
outcome and prognosis in radiotherapy of recurrent cervical carcinoma o complete + censored pelvic control overall survival relapse - free survival complete surgery / surgery with microscopic tumor left o complete + censored p = 0.05 biopsy / surgery with macroscopic tumor left time in months from end of therapy time in months from end of therapy figure 1 . 
after 3 months , one patient who had undergone pelvic irradiation with 50 gy and a boost of 10 gy to the rectosigmoid suffered from a fistula between rectosigmoid and vagina which had to be removed by surgery . 
 the therapeutic outcome of the whole patient group with a recurrence following surgery in our study is comparable to the literature [ 5 , 14 , 22 , 42 ]  . 
nevertheless , the prognosis is poor and the tumor should be controlled in the primary situation . eleven of the 26 patients in our study had prognostic high risk factors in the primary situation but had not undergone postoperative pelvic irradiation for various reasons . 
adjuvant radiotherapy in case of risk factors has been the usual clinical practice for early cervical carcinoma in many departments [ 2 , 12 , 19 , 33 , 39 , 45 ]  . 
many authors emphasize the value and necessity of adjuvant treatment in patients with high risk factors [ 4 , 20 , 26 , 37 ] like positive pelvic lymph nodes , parametric involvement , positive margins , lymphor hemangiosis , bulky tumors , deep invasion of cervical stroma , or histology of adenocarcinoma , clear - cell or small - cell carcinoma [ 1 , 3 , 7 , 10 , 15 , 16 , 27 , 31 , 34 ]  . 
though no improvement in overall survival could be shown until now [ 13 , 23 , 30 , 33 , 35 , 37 , 38 ] , retrospective and prospective analyses found better local control rates with postoperative irradiation in case of high - risk carcinomas as compared to surgery alone [ 3 , 20 , 35 ]  . 
outcome and prognosis in radiotherapy of recurrent cervical carcinoma rences have to be expected despite optimal primary therapy , and in our study no difference in outcome following the recurrence therapy was found between patients with high risk factors in the primary situation but no adjuvant therapy and patients without high risk factors primarily . 
 we are aware , that the material we analyzed is far too small to allow extensive subgroup analyses , yet we found some interesting results . the time between primary surgery and recurrences in our study is short ( on average 26 months ) , as described by others . in several reports , recurrences were diagnosed within the first 24 months [ 21 , 26 , 41 ]  . 
though early recurrences occurring within the first 6 months have been reported to have a less favorable prognosis [ 21 ] , we like others [ 36 , 41 ] did not find a difference in outcome compared to recurrences occurring later . 
 the outcome of recurrent cancer of the cervix in our study and other reports [ 14 , 21 , 28 , 35 , 43 ] show that the best results are obtained in patients with central recurrence , especially in patients with tumors confined to the vagina or paravaginal tissue . 
as a reason for this , an earlier detection of recurrences of the central pelvis and , thus , a smaller tumor volume are discussed [ 18 , 21 , 43 ]  . 
 in our series , recurrences with complete surgery or only microscopic residual tumor , independent of the location , were found to have a better therapeutic outcome compared to inoperable recurrences or surgery with macroscopic residual tumor . 
however , concerning the lower oxygenation in the pelvis after surgery , the lower dose may often be insufficient for local control , especially in case of a high tumor burden , independent of the location , or pelvic wall infiltration with incomplete surgery . 
though we analyzed only 26 patients , the conclusion from our subgroup analysis should be that the prognosis mostly depends on a small tumor burden with the possibility of brachytherapy and / or a complete surgery or surgery with only microscopic residual tumor . 
the prognosis , especially for inoperable recurrences , recurrences with a high tumor burden or pelvic wall infiltration without the possibility of vaginal brachytherapy , is unfavorable , possibly due to a underdosage of large tumors and aggressive tumor biology . 
concerning the worse treatment results of recurrences with pelvic wall infiltration and / or incomplete surgery with external irradiation , further efforts have to be made to improve the therapeutic ratio of radiotherapy . 
more aggressive treatment modalities such as radiochemotherapy [ 8 , 9 , 11 , 28 , 32 , 40 , 44 ] and / or higher radiation doses [ 5 , 21 ] are needed . 
the probability of controlling the recurrence mostly depends on a small tumor burden with the possibility of brachytherapy and / or complete surgery or surgery with only microscopic residual tumor . 
 strahlentherapie und onkologie kurzmitteilung induratio penis plastica claudia pambor , gnther gademann1 hintergrund : bei patienten mit induratio penis plastica ( ipp ) wurde die wirkung einer strahlentherapie mit schnellen elektronen untersucht . 
 ergebnisse : whrend sich die induration ( 27 , 6% ) und deviation ( 24 , 1% ) des erigierten penis wenig verbesserten , konnte bei knapp zwei drittel der patienten ( 65% ) mit schmerzen eine deutliche linderung erzielt werden . 
 schlsselwrter : induratio penis plastica radiotherapie benigner erkrankungen andrologie penile induration strahlenther onkol 2003 ; 179 : 78790 doi 10.1007 / s00066 - 003 - 1022 - 3 induratio penis plastica background : to evaluate the benefit of radiotherapy with fast electrons in induratio penis plastica ( ipp )  . 
 results : induration ( 27.6% ) and deviation ( 24.1% ) of the erected penis are little improved , but in two - third of patients ( 65% ) with painful erection defined relief could be obtained . 
 key words : peyronies disease radiation therapy for benign disease andrology penile induration einleitung franois gigot de la peyronie ( 16781747 ) [ 13 ] , leibarzt louis xv . , beschrieb im jahr 1743 nodse vernderungen zwischen den corpora cavernosa des mnnlichen gliedes , die eine penile kurvatur und ein unbehagen bei der erektion verursachen . 
die einbeziehung entzndlicher prozesse in die entstehungsgeschichte der ipp konnte anfang der 1990er jahre histologisch besttigt werden [ 15 ]  . dennoch fehlen aufgrund der seltenheit der erkrankung gesicherte kenntnisse ber verlauf und therapie der ipp [ 5 ]  . 
die ersten feingeweblichen vernderungen zeigen sich an den gefen in form von entzndungen , in denen sich spter die fibrose entwickelt , die im weiteren verlauf durch knorpel - , knochenoder kalkbildung kompliziert sein kann [ 2 , 12 , 15 , 18 ]  . 
 bei der behandlung der ipp kommen verschiedenste therapieverfahren zur anwendung , wobei fr die radiotherapie bekannt ist , dass sie die besten ergebnisse in einem frhen krankheitsstadium zeigt [ 7 ]  . 
diese wurden von der modernen strahlentherapie mit einsatz schneller elektronen am linearbeschleuniger abgelst . im folgenden stellen wir unsere ergebnisse bei der strahlentherapeutischen behandlung der ipp vor und betrachten sie im vergleich mit anderen therapiemglichkeiten . 
 patienten und methoden im zeitraum von 7 jahren wurden an der klinik fr strahlentherapie der otto - von - guericke - universitt magdeburg 58 patienten mit einer klinisch manifesten ipp behandelt . 
die symptome wurden anhand eines fragebogens erfasst , der die erhebung der subjektiven beschwerden ( schmerzhafte erektion , deviation , kohabitationsund miktionsbeschwerden ) und des lokalbefundes in gre , ausdehnung und lokalisation beinhaltete . 
 ein gemeinsames auftreten mit der dupuytren - kontraktur in der literatur mit 760% beschrieben [ 5 , 11 , 12 , 20 , 21 ] sahen wir in unserem patientengut bei elf patienten ( 19% )  . 
in der vergangenheit hatten sich 15 patienten ( 26% ) einer konservativen medikamentsen therapie mit k - paraaminobenzoat ( potaba ) , vitamin e und / oder hyaluronidaseinjektionen unterzogen , ohne dass dabei eine besserung ihrer beschwerden erzielt werden konnte . 
erfolgt die bewertung der therapie nach den in tabelle 1 aufgefhrten kriterien , erfuhren sechs patienten ( 10 , 3% ) eine heilung einschlielich rckbildung des palpationsbefundes ( tabelle 2 )  . 
diese trat innerhalb von 6 wochen bis zu 2 jahren post radiationem e betrachtet man die dauer der erkrankung vor beginn der therapie , so zeigt sich , dass von 18 patienten , deren therapie innerhalb von 6 monaten nach krankheitsbeginn eingeleitet wurde , ein drittel eine besserung oder vollstndige rckbildung ihrer symptome aufwies , whrend in der patientengruppe mit lngerer anamnesedauer 75% der patienten nicht von der therapie profitierten . 
 heilung regression komplette rckbildung aller symptome 50% rckbildung der deviation und induration ; subjektiv deutliche abnahme der schmerzhaften erektion status idem keine befund - / symptomnderung progression zunahme der prtherapeutischen symptome tabelle 2 . 
 symptom patientenzahl ( % ) induration ( n = 58 ) deviation bei erektion ( n = 54 ) schmerz bei erektion ( n = 20 ) 16 ( 27 , 6 ) 13 ( 24 , 1 ) 13 ( 65 ) teleangiektasien , atrophien oder ulzera konnten bei den 58 patienten beobachtet werden . 
 bei den 15 patienten mit medikamentser vortherapie zeichnete sich kein einfluss dieser behandlung auf den therapieerfolg ab : vier patienten zeigten eine regredienz ihrer erkrankung , bei neun patienten konnte keine nderung der symptomatik beobachtet werden und zwei patienten erlebten einen progress ihrer erkrankung . 
 diskussion obwohl insgesamt gesehen von einer hohen akzeptanz der radiotherapie bei gutartigen erkrankungen in deutschland ausgegangen werden kann , beruhen die erhobenen daten ber strahlentherapeutische behandlungen der ipp jedoch fast ausschlielich auf retrospektiven auswertungen [ 16 ] , die aufgrund der seltenheit der erkrankung meist kleine patientengruppen beinhalten , die ber einen greren zeitraum zusammengestellt wurden und zudem oftmals verschiedenen behandlungsmethoden in folge oder auch kombiniert zugefhrt wurden . 
im allgemeinen wird angenommen , dass unabhngig von der therapieform bei etwa einem drittel der patienten beschwerdeund erscheinungsfreiheit erzielt werden , ein drittel eine deutliche besserung erfhrt und ein drittel unbeeinflusst bleibt [ 20 ]  . 
alle patienten , die seit 1985 mit schnellen elektronen therapiert wurden , zeigten wie auch in unserer studie keine nebenwirkungen [ 7 ]  . auch wird in der von kammerer [ 7 ] beschriebenen patientengruppe von rezidiven auerhalb des bestrahlungsfeldes berichtet , die den schluss aufkommen lieen , in das zielvolumen den gesamten penisschaft unter einschluss der peniswurzel und ausschluss der glans penis einzubeziehen . 
hascher - klnder [ 6 ] berichtet bei der behandlung mit k - paraaminobenzoat ( potaba ) ber eine meist erfolgreiche therapie , wenn es gelang , ohne hufige unterbrechung die medikation langzeitig durchzufhren . 
bei einer medikamentsen therapie muss auch immer in betracht gezogen werden , dass es sich um eine systemische anwendung handelt , die auch systemische nebenwirkungen ausbilden kann [ 3 ]  . 
whrend sich die indurationen und die damit verbundene deviation des gliedes im fortgeschrittenen stadium nur wenig bessern , konnte bei zwei dritteln der patienten mit schmerzen eine deutliche linderung erzielt werden . 
11 urban & vogel strahlentherapie und onkologie original article low - dose radiotherapy for painful heel spur retrospective study of 117 patients ralph mcke1 , klaus schnekaes2 , oliver micke3 , m . 
heinrich seegenschmiedt4 , dorothee berning3 , rainer heyder1 purpose : retrospective analysis of 117 patients treated between 1996 and 2000 with low - dose radiotherapy ( rt ) for painful heel spurs . patients and methods : 71 women and 46 men were irradiated on 136 painful heel spurs in one ( n = 104 ) or two radiation series ( n = 13 )  . 
by contrast , an interval of > 6 months until the initiation of rt resulted in only 73% of patients with clinical improvement . conclusion : low - dose rt reveals a benefit in > 80% of the patients . 
 key words : benign disorder painful heel spur low - dose radiotherapy 6 - mv photons strahlenther onkol 2003 ; 179 : 7748 doi 10.1007 / s00066 - 003 - 1126 - 9 strahlentherapie des schmerzhaften fersensporns . 
eine retrospektive analyse von 117 patienten ziel : analyse der analgetischen radiotherapie ( rt ) von 117 patienten mit schmerzhaftem fersensporn , die von 1996 bis 2000 behandelt wurden . patienten und methodik : 71 frauen und 46 mnner mit einem altersmedian von 58 jahren ( 3084 jahre ) und 136 fersenspornen ( links n = 43 , rechts n = 55 , beide n = 19 ) wurden in einer ( n = 104 ) oder zwei serien ( n = 13 ) bestrahlt . 
 die rt erfolgte zweimal pro woche mit einem 6 - mv - photonen - stehfeld mit 0 , 5 gy einzeldosis bis zu einer gesamtdosis von 5 , 0 gy . 
 ergebnisse : direkt nach rt waren 27 patienten schmerzfrei , 40 patienten gaben eine wesentliche besserung , 31 patienten eine leichte besserung sowie 19 patienten keine beeinflussung an ( tabelle 1 )  . 
mit einem medianen follow - up von 20 monaten ( 163 monate ) waren 03 / 2001 von 100 untersuchten patienten 75 schmerzfrei , zwlf gaben eine wesentliche besserung , drei eine besserung und zehn keine beeinflussung an ( tabelle 1 )  . 
bei einer medianen schmerzdauer vor rt von 6 monaten ( 160 monate ) fhrte der beginn der rt im intervall 6 monate ( n = 70 ) bei 94 , 2% zu einer schmerzkontrolle , im gegensatz dazu im intervall > 6 monate ( n = 30 ) bei 72 , 8% ( abbildung 1 )  . 
 schlsselwrter : schmerzhafter fersensporn strahlentherapie 6 - mv - photonen 1 department of radiotherapy , radiation oncology and nuclear medicine , weiden hospital , weiden , germany , 2 hensenstrae 144 , mnster , germany , 3 department of radiotherapy , university hospital mnster , germany , 4 department of radiation oncology , radiotherapy and nuclear medicine , alfried krupp hospital , essen , germany . received : november 27 , 2002 ; accepted : july 3 , 2003 strahlenther onkol 2003 no . 
radiotherapy for painful heel spurs introduction the term heel spur was first described by the german surgeon plettner in 1900 who used the anatomic term kalkaneussporn ( english : calcaneal spur )  . 
he described , in his radiomorphologic study , the exostotic plantar bone formation at the insertion of the plantar fascia and muscles of the calf ( cited in [ 42 ] ) which is termed nowadays plantar heel spur . 
 chronic damage or continuous microtrauma to the insertion of the plantar aponeurosis and the small foot muscles due to increased strain plays an important role in the pathogenesis . the increased strain may be a result of foot deformity , obesity , or extensive sports activities [ 36 , 49 ]  . 
 the treatment follows the principles of therapy for osteoarthritis : decreasing weight burden by means of orthopedic shoes or insoles , local infiltration with corticoid crystal suspensions , and local anesthesia . 
systemic nonsteroidal anti - inflammatory agents ( nsaids ) , iontophoresis , microwave and ultrasound applications are common treatment modalities [ 3 , 7 ]  . different surgical techniques are also in use [ 3 ]  . 
although radiotherapy ( rt ) is known for good results in heel spurs and other musculoskeletal degenerative and inflammatory entities [ 34 ] in the past , the decision for rt is still regarded as last resort approach to treat refractory cases . 
 the goal of this retrospective clinical study was to analyze the therapeutic effect of irradiation with 6 - mv photons immediately after completion of rt and during follow - up and to identify possible prognostic factors . 
 patients and methods at the department of radiotherapy , radiooncology and nuclear medicine , weiden hospital , germany , a total of 117 patients ( 71 female , 46 male ) with painful heel spurs were treated between january 1996 and december 2000 . 
at the end of rt , 27 patients ( 23% ) were free of pain , 40 patients ( 34% ) experienced marked improvement , 31 ( 27% ) some improvement , and 19 patients ( 16% ) felt no change . 
with regard to the number of rt series , 78 of 88 patients ( 86.6% ) who underwent a single rt series had pain control compared to nine of 13 patients ( 69.2% ) with two rt series . 
 result patients ( n = 117 ) at the end of radiotherapy patients ( n = 100 ) at the time of data analysis complete pain relief markedly improved slightly improved unchanged 27 ( 23.1% ) 40 ( 34.2% ) 31 ( 26.5% ) 19 ( 16.2% ) strahlenther onkol 2003 no . 
treatment onset within the first 6 months of symptoms ( n = 70 ) led to pain control in 94% of patients . rt given > 6 months after the beginning of clinical symptoms ( n = 30 ) resulted in pain control in 73% of cases ( p = 0.045 ; figure 1 )  . 
 discussion there is a long tradition for rt of benign degenerative or inflammatory lesions [ 1 , 24 , 26 , 27 , 34 , 35 , 39 , 45 ]  . 
rt of benign diseases accounts for 810% of all rt procedures in germany . as much as 70% of these indications represent painful disorders in the locomotor system [ 42 ]  . 
numerous studies have described the effectiveness of rt under orthovolt as well as megavolt conditions [ 2 , 9 , 14 , 23 , 29 , 3335 , 39 , 40 , 43 , 45 , 50 ] ( table 2 )  . 
 pain control ( pain - free , markedly improved , slightly , slightly improved ) p = 0.045 pain history before rt 6 months ( n = 70 ) pain history before rt > 6 months ( n = 30 ) 10 15 20 25 30 35 40 45 50 55 60 65 months figure 1 . 
univariate analysis ( log - rank ) for pain control ( 60 months ) depending on duration of pain history : upper curve : 6 months , lower curve : > 6 months . 
univariate analyse ( log - rank ) der schmerzkontrolle ( 60 monate ) in abhngigkeit von der schmerzdauer : obere kurve : 6 monate , untere kurve : > 6 monate . 
other studies describe an influence on the vascular endothelium with improved tissue perfusion ; destruction of inflammatory cells ( especially lymphocytes ) with release of cytokines and proteolytic enzymes ; modulation of the vegetative nervous system ; altering of the tissue ph ; increased membrane permeability [ 26 , 30 , 47 , 48 ]  . 
recent studies showed , that there are also effects of low - dose ionizing radiation on the molecular and cellular level involving adhesion molecules , cytokine expression , and inflammation cascade [ 1618 , 21 , 32 , 38 ]  . 
 radiation side effects did not occur in any of our patients . this corresponds to the reported absence of chronic or acute adverse effects in the literature ( table 2 )  . 
however , so far , no increased tumor rate has been reported in the literature for the chosen dose range [ 8 , 22 , 25 , 39 ]  . 
it seems useful to recall the epidemiologic evidence that the attributable carcinogenic lifetime risk is considerably smaller at older age than earlier in life [ 5 , 6 , 8 ] .the applied gonad dose during the treatment of heel spurs is in the range of diagnostic imaging [ 13 ]  . 
when standard radiation protection measures are taken ( minimal field size , gonad shields , etc . ) , the risk of rt in this subpopulation of mostly elder patients can almost be neglected . 
controlled prospective studies should assess the effect of rt by comparison with sham treatments to assess the possible role of placebo effects . strahlentherapie und onkologie original article apoptotic response of irradiated t - lymphocytes an epidemiologic study in canine radiotherapy patients * simona stankeov1 , nigel edward alfred crompton2 , hans blattmann2 , priska theiler2 , gillian carolyn emery2 , malgorzata roos3 , barbara kaser - hotz1 background : evaluation of radiation - induced apoptosis in t - lymphocytes was developed for human medicine in order to predict the sensitivity of individual patients to radiation therapy and has regular use in cases of suspected hypersensitivity . 
the sensitivity of a patients peripheral blood t - lymphocytes to radiation - induced apoptosis does not change as a result of the trauma of radiotherapy during the course of tumor treatment . 
 key words : radiation - induced apoptosis lymphocyte flow cytometry radiation therapy in dogs strahlenther onkol 2003 ; 179 : 77986 doi 10.1007 / s00066 - 003 - 1096 - y strahleninduzierte apoptosehufigkeit in t - lymphozyten . 
eine epidemiologische studie zur radiotherapie bei hunden hintergrund : die bestimmung der strahleninduzierten apoptose bei lymphozyten wurde fr die humanmedizin zur prognose der individuellen strahlenempfindlichkeit einzelner patienten entwickelt , wo der test regelmig bei verdacht auf hypersensibilitt eingesetzt wird . 
 ergebnisse : die apoptoserate der lymphozyten ist von der dosis ( abbildungen 1 und 4 ) , vom alter ( abbildungen 3 und 5 ) und vom gewicht ( abbildung 7 ) der patienten abhngig . 
 schlsselwrter strahleninduzierte apoptose lymphozyten flow - zytometer strahlentherapie bei hunden 1 section of diagnostic imaging and radio - oncology , faculty of veterinary medicine , university of zurich , switzerland , 2 division of radiation medicine , department of life sciences , paul scherrer institute , villigen , switzerland , 3 biostatistics , ispm , university of zurich , switzerland . 
in veterinary medicine , radiation oncology is also becoming increasingly important [ 19 , 20 ] as cancer is also a major cause of death in pet dogs [ 3 ]  . 
actual dose limits for external radiotherapy , however , are generally given by normal tissue complication probabilities ( ntcp ) because of the inevitable exposure of normal tissues during treatment [ 15 , 17 , 32 ]  . 
various approaches have been described in the literature using different biological tests , and normal as well as malignant cells [ 2 , 18 , 25 , 26 , 28 ]  . 
for normal and radioresistant patients dose to the tumor could be raised above the clinical standard , to yield a higher tcp , while for radiosensitive patients dose could be reduced slightly , thus avoiding increased ntcp [ 8 , 14 ]  . 
it has been proposed to use levels of apoptosis induced by exposure to radiation in normal blood cells , specifically cd4 and cd8 t - lymphocytes , as a measure of the bodys cells potential to respond to radiation damage . 
by analyzing two different cell types , cd4 and cd8 t - lymphocytes , and by reducing variation in radiation - induced apoptosis in leukocytes caused by its age dependence , higher precision was achieved . if successful , such an assay could lead to individualized treatment schemes , resulting in higher therapeutic gain factors . 
in an earlier veterinary study , a correlation was observed between radiation - induced apoptosis in cd4 and cd8 t - lymphocytes and age , indicating that such an assay should be evaluated for application in veterinary radiation therapy [ 31 ]  . 
 material and methods patient material blood for analysis of radiation - induced apoptosis was taken from two cohorts of dogs : a cohort of healthy dogs and a cohort of patients , who presented for radiotherapy with spontaneous tumors at the section of diagnostic imaging and radio - oncology , faculty of veterinary medicine , university of zurich ( tierspital zurich ) , switzerland . 
seven tumor - bearing dogs received 24 gy of palliative treatment with electrons ( three fractions , 8 gy / fraction on days 0 , 7 , and 21 )  . 
three of the tumor - bearing dogs treated with palliative radiation therapy received concomitant chemotherapy with carboplatin 250 mg / m2 ( paraplatin , bristol - myers squibb , baar , switzerland ) three times during the course of radiation therapy . 
 antibiotics ( synulox , amoxicillin , 12 mg / kg b.i.d. , pfizer ag , zurich , switzerland ) and corticosteroids ( prednisolon , prednisolon , 1 mg / kg s.i.d. , streuli ag , uznach , switzerland ) were given orally for 3 weeks to treat acute side effects and to prevent secondary infections of the skin , pruritus , and subsequent automutilation . 
when dogs were available for follow - up 3 months after therapy ( n = 10 ) , the rtog / eortc for late effects was used to score reactions . preparation of lymphocytes for flow cytometry 4 ml of fresh blood from each donor was harvested by venipuncture into heparin tubes and sent expeditiously , via express strahlenther onkol 2003 no . 
blood , which was processed after 48 h , showed signs of deterioration , detectable as blood clots during incubation and as a reduced apoptotic yield during analysis of the data . 
blood was diluted 1 : 10 in rpmi 1640 medium ( life technologies , basel , switzerland ) containing 20% fetal bovine seruthe diluted suspension was then distributed into 25 - cm2 cell culture flasks . 
the blood samples were irradiated at room temperature under aerobic conditions with 0 - , 2 - , and 4 - gy x - rays ( philips mcn 321 x - ray tube , hamburg , germany , 300 kvp , 10.65 ma , at a dose rate of 3.4 gy / min )  . 
dosimetry was performed using a farmer dosimeter 2570 ( nuclear enterprises , zurzach , switzerland )  . after irradiation in vitro , the samples were incubated for 48 h at 37 c and 5% co2 . 
after incubation , the blood suspension was transferred into a 5 - ml tube and centrifuged at 1 , 300 rpm for 5 min ( 300 g ) at room temperature . 
fitc - conjugated monoclonal antibodies ( connex gmbh , martinsried , germany ) were added to this cell suspension ( anti - caninecd4 fitc specific for cd4 t - lymphocytes and anti - caninecd8 fitc for cd8 t - lymphocytes ) at a dilution of 1 : 81 ( 5 l antibody into 400 l cell suspension )  . 
after 20 min incubation at room temperature , 4 ml of facs lysing solution ( bectondickinson , basel , switzerland ; diluted 1 : 10 in bi - distilled water ) were added to the cell suspension to induce lysis of erythrocytes . 
the supernatant was withdrawn , and the remaining cells were resuspended in 4 ml phosphate buffer solution ( pbs ; facs flow , becton dickinson ) , neutralizing the lysing solution . 
after a further centrifugation ( 300 g ) followed by withdrawal of the supernatant , the cells were resuspended in 200 l pbs to which 5 l of a propidium iodide ( pi ) stock solution ( 1 mg / ml in pbs ) were added in order to stain the dna . then , 50 l of 1 mg / ml rnase ( bovine pancreas rnase a , serva , heidelberg , germany ) were added to eliminate broadening of the cellular dna distribution due to intracellular rna . the cells were subsequently examined using a facscan flow cytometer ( becton dickinson , san jose , ca , usa )  . 
 flow cytometry to identify the cd4and cd8 - positive t - lymphocytes , a twodimensional ( 2 - d ) scatter - plot of antibody fluorescence ( fl1height ) versus cellular dna content ( fl2 - height ) was used . to determine the percent of apoptotic cells , a 2 - d scatter - plot of cellular dna content ( fl2 - height ) versus cell size ( fscheight ) was used . 
 statistics evaluation of the results was performed using statview version 4.0 statistical software using the following tests : mannwhitney u - test for comparison of means in two independent groups , t - test for paired data , pearsons correlation ( r ) , and t - test of the slope ( b - values ) , for linear regression lines . 
 results interdose comparisons of the percent apoptosis induced by 2and 4 - gy x - rays in the cd4 and cd8 t - lymphocytes were examined using linear regression analysis ( figure 1 )  . 
internal consistency of the test when predicting radiation - induced apoptosis by comparing cd4 and cd8 t - lymphocytes is displayed in figure 2 . data are presented with the background spontaneous apoptosis ( 0 gy ) levels subtracted . 
a strong correlation between radiation - induced apoptosis in the two cell lines was observed ( r = 0.80 , p < 0.0001 for 20 gy , and r = 0.77 , p < 0.0001 for 40 gy )  . 
interdose comparison of the percent apoptosis induced by 2gy and 4 - gy x - rays in cd4 ( ( cid : 1 ) ) and cd8 ( ( cid : 2 ) ____ ) t - lymphocytes from a cohort of 17 healthy dogs and 38 tumor - bearing dogs . 
interleukocyte comparison of the percent apoptosis induced by 2 - gy ( ( cid : 1 ) _____ ) and 4 - gy ( ( cid : 2 ) ) x - rays in cd4 and cd8 t - lymphocytes from a cohort of 17 healthy dogs and 38 tumor - bearing dogs . 
vergleich der strahleninduzierten apoptoserate fr cd4und cd8 - t - lymphozyten durch 2 - gy ( ( cid : 2 ) _____ ) und 4 - gy - rntgenstrahlen ( ( cid : 1 ) ) in einer gruppe von 17 gesunden und 38 an tumoren erkrankten hunden . 
box plots of radiationinduced apoptosis split by age into individuals < 2 years and 2 years demonstrate the significantly higher apoptosis rate of the young animals ( figure 3 )  . 
the difference in radiation - induced apoptosis in the cd4 t - cells at 4 gy for younger ( < 2 years ) and older ( 2 years ) dogs was highly significant ( p > 0.0001 , u - test )  . 
therefore , in the subsequent analyses we excluded young dogs ( < 2 years ) from the control group of healthy dogs in order to be able to obtain a more reliable comparison between the two groups . 
no differences between healthy dogs ( n = 17 ) and cancer patients ( n = 38 ) for any parameter , cell type or dose , were observed ( figure 4 )  . 
no significant dependence of spontaneous apoptosis on age in the cd4 and cd8 tlymphocytes before radiation therapy was seen ( p > 0.92 for cd4 t - lymphocytes , p > 0.6 for cd8 t - lymphocytes )  . investigations of potential changes in sensitivity to radiation - induced apoptosis during fractionated radiation therapy in tumor - bearing dogs were performed . 
percent apoptosis induced by 4 - gy x - rays in cd4 and cd8 t - lymphocytes as a function of age in 17 healthy dogs and 38 tumor - bearing dogs . 
percent apoptosis induced by 2 - gy x - rays in cd4 and cd8 t - lymphocytes for both times points ( ) ; percent apoptosis induced by 4 - gy x - rays in cd4 and cd8 t - lymphocytes for both time points ( )  . 
strahleninduzierte apoptosehufigkeit nach 2 - gy - rntgenstrahlen in cd4und in cd8 - t - lymphozyten fr beide zeitpunkte ( ) ; apoptosehufigkeit nach 4 - gy - rntgenstrahlen in cd4und cd8 - t - lymphozyten fr beide zeitpunkte ( )  . 
 tion and a second sample ( t1 ) at the end of radiation therapy . statistical analyses ( t - test ) of the paired t0 and t1 data were performed . 
no changes in sensitivity to radiation - induced apoptosis during fractionated radiation therapy were observed . a clear dependence of radiation - induced apoptosis in cd4 t - lymphocytes on weight in the cohort of 38 tumor - bearing dogs was observed ( figure 7 )  . 
no correlation between weight and spontaneous apoptosis for cd4 or cd8 t - lymphocytes was seen ( p > 0.23 for cd4 and p > 0.71 for cd8 t - lymphocytes )  . 
 four parameters were measured from each blood sample . in order to integrate this data into a single graph , the data were standardized using z - scores ( number of standard deviations from the mean ) and a mean value for the two doses was calculated for each cell type . 
first , the z - score was determined for the age - corrected 2 - 0 - gy values of radiation - induced apoptosis , then , the z - scores were determined for the age - corrected 4 - 0 - gy values . 
one dog amongst the untreated cohort ( 1 / 55 ) deviated by more than two standard deviations from the mean , otherwise , none of the dogs could be identified as hyperor hyposensitive . 
the assay would assist , together with other information , in avoiding massive normal tissue reactions in hypersensitive patients and potentially in optimizing treatment dose for individual patients . markedly reducedcapacity for radiation - induced apoptosis in cd4 and cd8 t - lymphocytes has been observed in humans in strahlenther onkol 2003 no . 
 the present study was designed to explore the feasibility and usefulness of applying the assay on canine patients , to investigate if levels of radiation - induced apoptosis in cancer patients differ from that in healthy individuals , and to evaluate to what extent sensitivity of t - lymphocytes to radiationinduced apoptosis is modified during radiation treatment . 
a good correlation was found between sensitivity to radiation - induced apoptosis at two radiation doses , as well as between levels of induced apoptosis in two t - lymphocyte cell types . 
in order to evaluate the significance of this trend , the slope of the curve ( b - value ) was compared to a theoretical b - value of 1 , which would indicate an equivalent apoptotic yield in both cell types , and a t - test was performed . 
 does the sensitivity of the t - lymphocytes to radiation - induced apoptosis change because of radiation therapy ? the leukocyte apoptosis assay revealed significantly decreased levels of induced apoptosis after exposure to radiation in rafigure 8 . 
the background ( 0 gy ) level of apoptosis and the expected contribution of age ( as determined from the regression formula derived from figure 6 ) were subtracted . the data are presented as pooled z - scores ( number of standard deviations from the mean ) , see text for further details . 
eine gruppe umfasst unbestrahlte tiere , 17 gesunde hunde und 38 tumorpatienten vor bestrahlung ( ( cid : 1 ) , ( cid : 2 ) ) , die andere gruppe umfasst 38 bestrahlte hunde mit tumoren ( ( cid : 3 ) )  . 
this explanation , however , was already refuted in the original publication of crompton et al . , where no consistent selection for radiation resistance with time following treatment was observed ( see table 1 in [ 4 ] )  . 
a third explanation assumes that patients exposed to radiation therapy will display a compromised radiation - induced apoptosis , in at least the t - lymphocytes , as a consequence of the treatment . 
apoptosis and radiation therapy in dogs each patient had a blood sample taken on two separate occasions , once before the first radiation treatment and once at the end of radiation therapy . 
observed a decreased cd4 / cd8 ratio after radiation therapy in breast cancer patients and patients with seminoma of the testis [ 12 ] ; this information is not available for our study as the number of cd4 and cd8 cells have not been determined . 
one results from the response of the whole organism to the radiation therapy , the other results from the response of specifically the t - lymphocytes to the direct effects of dose received during therapy . 
the whole organism response could be due to tissue damage either in the tumor or the surrounding healthy tissues , which would induce a defensive physiologic response , e.g. , a cytokine - induced inflammatory response . 
direct effects could result from a well - known response of cells to radiation where such cells carry within them evidence of the exposure , i.e. , radiation - induced heritable damage [ 10 ] , but also from direct exposure of the bone marrow [ 16 ]  . 
despite a difference of means , the t - test revealed no significant differences in the levels of radiation - induced apoptosis observed before and after the 3 weeks of radiation therapy . 
it was usually taken at the end of the treatment , when cells exposed early during the course of radiation therapy may have been replaced . sometimes , the second probe was taken after the first dose fraction , when it will have received a dose much smaller than this because any t - lymphocyte will , on average , have spent only a brief period within the irradiation volume as this was in most cases small compared to the total body volume . 
young dogs ( < 2 years ) displayed significantly higher levels of radiation - induced apoptosis than older dogs . the control group of healthy dogs consisted primarily of dogs < 2 years . 
large differences in mean age between the two dog populations led to the decision to omit dogs < 2 years from the study in order to obtain groups with comparable age distributions . 
similar inverse relationships have even been reported in humans [ 27 ]  . the biological basis for this inverse relationship between size and life span in the dog has not been adequately explained [ 24 ]  . 
the heavier dogs had a lower average age and displayed commensurately elevated levels of apoptosis , which certainly contributed to the correlation between apoptosis and weight . big differences in physiologic longevity were found between mixed breed dogs and pure breed dogs , with respect to weight . data reported by patronek et al . 
however , in this study this was not observed , most probably because the large number of breeds and the usually small number of individuals per breed precluded statistical significance . 
 tissue response and apoptosis in this study , different tumor locations were included and , as a consequence , different normal tissues or different areas of the dogs bodies were at risk of displaying radiation - induced injuries . 
these medications modified the susceptibility to radiation injuries and made the scoring of radiation injuries unreliable , despite the use of such established systems as the rtog / eortc grading system [ 29 ] for acute and late skin reactions . 
in order to evaluate the clinical relevance of the correlation between the apoptosis assay and normal tissue response , either alternative indicators of normal tissue response must be found , which are not affected by such medications , or unethical treatments in the absence of medications to reduce inflammation and infection would have to be performed . 
in treatment planning , however , the first priority is to limit dose to the sensitive normal tissues thus avoiding severe damage , especially late radiation damage [ 17 , 29 ]  . 
als ursachen fr die entstehung dieses verschleies werden strungen der sehnendurchblutung in der hypovaskularisierten zone etwa 1 cm vom ansatz der supraspinatussehne am tuberculum majus , biomechanische faktoren , bedingt durch besonderheiten in der morphologie am sehnen - knorpel - knochen - ansatz und mechanische irritationen zwischen humeruskopf und schulterdach bei abduktionsbewegungen angeschuldigt [ 6 ]  . die insertionstendinopathien der supraspinatussehne gehren zum , erstmalig von neer beschriebenen , impingement - syndro er verstand darunter ein anstoen der rotatorensehnen im bereich des vorderen akromions , des ligamentum coracoacromiale bzw . 
analog dazu bezeichnet das non - outlet - impingement eine funktionelle einengung der supraspinatussehne , beispielsweise durch eine tendinosis oder bursitis calcarea , eine instabilitt der rotatorenmanschette , ein prominentes tuberculum oder dislokationen des ac - gelenks . 
pathognomonisch ist ein umschriebener druckschmerzpunkt am tuberculum majus . bei den isometrischen tests spricht vor allem die schmerzhafte abduktion gegen widerstand fr eine beteiligung der strahlenther onkol 2003 ; 179 : 1312 doi 10.1007 / s00066 - 003 - 8905 - 1 supraspinatussehne . 
 neben der anamneseerhebung und einer ausfhrlichen klinischen untersuchung unter einschluss der oben beschriebenen tests erfolgten bei jedem patienten vor der randomisation auch eine rntgenuntersuchung der schulter in zwei ebenen sowie eine sonographie zum ausschluss einer rotatorenmanschettenruptur . 
 der grund zur untersuchung der insertionstendinopathien der schulter lag darin , dass dieses krankheitsbild bislang nur retrospektiv und ohne kontrollgruppe mit der eswt behandelt wurde trotz teilweise groer fallzahlen [ 1 , 3 ]  . 
der stichprobenumfang war mit insgesamt 30 patienten limitiert , und somit war die bildung von untergruppen zur differenzierung zwischen ursache des supraspinatussehnensyndroms und ansprechen auf die therapie , wie von adamietz angeregt , fr diese stichprobengre statistisch nicht sinnvoll . 
adamietz widerspricht sich insofern selbst , als er die strahlentherapie fr eine wenig erfolgversprechende indikation , das outlet - syndrom , prferiert . selbstverstndlich ist die niedrig dosierte strahlentherapie erfolgreich in der behandlung des non - outlet - syndroms und wird in unserer klinik auch durchgefhrt . 
so werden fr insertionstendinopathien in den von der degro herausgegebenen leitlinien zur radiotherapie gutartiger erkrankungen [ 5 ] einzeldosen zwischen 0 , 5 und 1 , 0 gy und gesamtdosen zwischen 3 , 0 und 12 , 0 gy angegeben . 
zur wahl der fraktionierung ist zu sagen , dass , wie auch im artikel dargelegt , aus organisatorischen grnden fnf fraktionen pro woche gegeben wurden . solche fraktionierungsschemata sind auch im angelschsischen sprachraum blich [ 10 ] und keinesfalls fragwrdig . 
in der routinebehandlung gutartiger erkrankungen geschieht dies seit lngerem ohneh ein cross - over - design mit wechsel der therapie nach einem ersten , erfolglosen behandlungszyklus ist gngiges vorgehen in vielen studien . 
2 urban & vogel strahlentherapie und onkologie original article significant increase in residual dna damage as a possible mechanism of radiosensitization by gemcitabine christian weiss1 , 2 , gerhard g . 
grabenbauer1 , rolf sauer1 , luitpold distel2 purpose : to investigate the effect of gemcitabine ( dfdc ) , a promising radiosensitizing nucleoside analog , on the induction and repair of dna double - strand breaks ( dsbs ) after ionizing radiation ( rt ) in a pancreatic tumor cell line . material and methods : bxpc3 pancreatic tumor cells were treated using different concentrations of gemcitabine with and without subsequent irradiation . 
dna dsbs were detected by constant - field gel electrophoresis under neutral conditions . results : with the addition of gemcitabine ( 0.51 , 000 mol / l for 2 h prior to rt ) to rt ( 075 gy ) , a considerable and dose - dependent increase of remaining dna damage after 24 h ( 5.4 - fold for 0.5 mol / l dfdc , 12.2 - fold for 1 , 000 mol / l dfdc at 25 gy ) was noted . 
enhancement factors were inversely correlated with increasing x - ray dose ( 7.8 - fold for 0.5 mol / l dfdc at 1 gy decreasing to 1.6 - fold at 75 gy )  . 
 key words : radiochemotherapy gemcitabine radiosensitization dna double - strand break pancreatic carcinoma strahlenther onkol 2003 ; 179 : 938 doi 10.1007 / s00066 - 003 - 1046 - 8 erhhter dna - restschaden als mglicher mechanismus der radiosensibilisierung durch gemcitabin ziel : untersuchung des effekts von gemcitabin , einem viel versprechenden nukleosidanalogon , auf die induktion und die reparatur von dna - doppelstrangbrchen ( dsbs ) nach ionisierender strahlung ( rt ) an einer pankreastumorzelllinie . 
die berechneten verstrkungsfaktoren zeigten eine inverse korrelation fr steigende bestrahlungsdosen ( 7 , 8fach fr 0 , 5 mol / l dfdc bei 1 gy abnehmend auf 1 , 6fach bei 75 gy )  . 
 schlussfolgerung : diese ergebnisse strken die hypothese der dna - reparaturhemmung als einen der hauptmechanismen der radiosensibilisierung durch gemcitab schlsselwrter : radiochemotherapie gemcitabin radiosensibilisierung dna - doppelstrangbruch pankreaskarzinom 1 department of radiation oncology , and 2 division of radiobiology , friedrich alexander university of erlangen - nrnberg , erlangen , germany . received : may 16 , 2002 ; accepted : september 9 , 2002 strahlenther onkol 2003 no . 
radiosensitization by gemcitabine introduction adenocarcinoma of the pancreas ranks third among malignancies of the gastrointestinal tract , its incidence is rising , and the patients prognosis remains poor [ 2 ]  . 
the widespread use of new techniques such as conformal , three - dimensional or intraoperative radiotherapy and combination of different modalities , including modern chemotherapeutic agents , inspired a great number of studies . 
 the nucleoside analog gemcitabine ( dfdc ) is a promising agent for palliative chemotherapy as well as concurrent rct , yet the exact mechanism of radiosensitization induced by dfdc remains to be elucidated . 
all three of these metabolites interfere with different steps in the processing of dna . dfdctp is incorporated into dna and known to impair dna replication and repair [ 26 ]  . 
furthermore , dfdcdp is an inhibitor of ribonucleotide reductase , and its action was shown to lead to depletion of the dna precursor pool , dntp [ 1 , 15 , 27 ]  . 
these functions of dfdc will result in a self - potentiating mechanism , because breakdown of dfdcmp is inhibited , whereas a reduction of dctp will reduce feedback inhibition of deoxycytidine kinase , and inhibition of ctp synthetase will also enhance incorporation of dfdc into rna . 
it has been hypothesized , that the incorporation of dfdc into the dna could lead to a repair inhibition of dna damage caused by ionizing radiation ( rt )  . therefore , constant - field gel electrophoresis ( cfge ) was used to measure the dna damages induced initially as well as those remaining after 24 h for combined and single treatment of pancreatic tumor cells with gemcitabine and irradiation . 
residual dna damage can be used as a measure of non - repaired dna , which is supposed to strongly correlate with the extent of cellular radiosensitivity [ 4 ]  . 
 material and methods cell culturebxpc3 human pancreatic cancer cells were obtained from the european collection of cell cultures and maintained in rpmi medium ( biochrom , berlin , germany ) containing 10% fetal bovine serum ( gibco , auckland , new zealand ) , 2 mmol / l glutamine ( gibco ) in an atmosphere of 95% air and 5% co2 at 37 c . 
 dna double - strand break induction and repair experiments cfge was used to determine the induction and the remaining amount of dna double - strand breaks ( dsbs ) in a pancreatic tumor cell line ( bxpc3 )  . 
the repair time of 24 h was chosen to detect the level of non - repaired dna damage in cells , whereas the amount of initial dna dsbs indicates the damage without repair . initial dna damage for dna dsb induction experiments , cells were incubated for 2 h with doses of 0.5 , 1 , 100 , and 1 , 000 mol / l gemcitabine in serum - free medium ( rpmi , biochrom )  . 
then , cells were washed twice in cold ( + 4 c ) pbs , trypsinized , counted , and embedded in melting 0.5% agarose ( biozym , oldendorf , germany ) to approximately 40 , 000 cells per plug . 
after irradiation , plugs were transferred to the lysis solution ( 1 mg / ml proteinase k , 1% sodium - n - laurylsarcosinate , lysis buffer : 100 mmol / l edta , 50 mmol / l nacl , ph 8.0 ) , kept 2 h at 4 c , for lysing cell membranes and for diffusion of proteinase k into the cell . 
the gels were stained with ethidium bromide , and images were acquired by a ccd camera ( kappa , gleichen , germany ) under illumination with 312 - nm uv light , using a band pass filter ( 605 / 25 nm )  . data analysis by an image analysis system ( biomas , erlangen , germany ) , the luminescence in the plug and in the gel was measured and the fraction released ( far ) was calculated by the dna migrated into the gel divided by the total amount of dna in one lane . 
2 urban & vogel where dsbs were expressed in gy equivalents at different doses of the combined treatment ( rad + gem ) and radiation treatment alone ( rad )  . 
remaining dna dsbs expressed in gy equivalents after 24 h for various combinations of gemcitabine ( triangles for 0.5 mol / l , stars for 1 mol / l , diamonds for 100 mol / l , and squares 1 , 000 mol / l ) and irradiation compared to irradiation alone ( filled circles ) in a pancreatic tumor cell line ( bxpc3 )  . 
dna - dsb - restschaden nach 24 h in gy - quivalenten fr verschiedene kombinationen von gemcitabin ( dreiecke fr 0 , 5 mol / l , sterne fr 1 mol / l , rauten fr 100 mol / l , quadrate fr 1 000 mol / l ) und bestrahlung im vergleich mit alleiniger bestrahlung ( gefllte kreise ) einer pankreastumorzelllinie ( bxpc3 )  . 
daten ergeben sich aus zumindest neun einzelwerten und drei unabhngigen versuchen . die fehlerbalken geben die standardabweichungen wieder . results combined treatment of bxpc3 pancreatic tumor cells with gemcitabine and subsequent irradiation produced an increased remaining dna damage , depending on the gemcitabine concentration used . 
conversely , the induction of initial dna dsbs for different gemcitabine concentrations was not affected as shown in figure 2 . the effect of irradiation alone compared with combined treatment demonstrated a significant increase in residual dna damage , which was summarized in enhancement ratios for different gemcitabine and radiation doses ( table 2 )  . 
the linear part of the curves , represented by the - values , indicates the effect at low irradiation doses with a gy equivalent of 2.94 102 gy1 ( table 1 )  . 
initial dna damage for various combinations of gemcitabine ( triangles for 0.5 mol / l , stars for 1 mol / l , diamonds for 100 mol / l , and squares 1 , 000 mol / l ) and irradiation compared to irradiation alone ( open circles ) in a pancreatic tumor cell line ( bxpc3 )  . 
initiale dna - dsbs in gy - quivalenten fr verschiedene kombinationen von gemcitabin ( dreiecke fr 0 , 5 mol / l , sterne fr 1 mol / l , rauten fr 100 mol / l , quadrate fr 1 000 mol / l ) und bestrahlung im vergleich mit alleiniger bestrahlung ( offene kreise ) einer pankreastumorzelllinie ( bxpc3 )  . 
 the induction of dna dsbs by irradiation alone was not influenced by simultaneous gemcitabine treatment , although gemcitabine alone led to a slight increase of initially induced dna dsbs and a modest elevation of residual dna damage . an increase in dna dsbs , produced by single - agent treatment with gemcitabine and measured by the fluorometric analysis of dna unwinding assay ( fadu ) , has already been described [ 22 ]  . 
for various nucleoside analogs , such as bromodeoxuridine ( brdurd ) or iododeoxyuridine ( idurd ) , radiosensitization by incorporation into dna and increased induction of dna damage , conferring to their unique biochemical properties to produce highly reactive free radicals , has been reported [ 13 ]  . 
even fluoropyrimidine analogs , such as fluorodeoxyuridine ( fdurd ) , which only differ from idurd or brurd by a fluorine atom , do not radiosensitize through increased initial dna damage , but mainly by inhibition of thymidylate synthetase [ 18 ]  . 
in this respect , it is reasonable to postulate that gemcitabine would not contribute to the induction of dna damage by producing highly reactive free radicals [ 6 ]  . furthermore , our study demonstrated a considerable increase in remaining dna damage for combined treatment with gemcitabine and subsequent irradiation in a pancreatic tumor cell line , dependent on the utilized gemcitabine concentration . 
sie zeigen den verbleibenden dna - schaden an und wurden nach folgender formel errechnet : dsb ( gy - quivalente ) = ( cid : 1 ) d + ( cid : 2 ) d2 . 
in the second column ( ( cid : 1 ) rad ) values represent the enhancement factors at the origin of the curves , in the next three columns ( dsb ( rad + gem ) / dsbrad ) the enhancement factors at 10 , 25 , and 75 gy are shown . 
on the other hand , the increasing amount of residual dna damage , for combined treatment , measured after 24 h , could strengthen the hypothesis of dna repair inhibition as a crucial mechanism of the well - recognized radiosensitization by gemcitabine , although several other studies failed to show neither effects on the induction nor on the repair of dna damage [ 6 , 15 ]  . 
this study could not demonstrate any effect on dna repair , not even when comparing ku80and dna - pk - proficient and - deficient cell lines [ 29 ]  . 
gemcitabine has been found to interfere with dna synthesis through several mechanisms , for example : ( a ) dfdc inhibits dna polymerase and ( cid : 2 ) [ 23 ] ; ( b ) dfdc causes masked dna - chain termination [ 11 ]  . 
the considerable effect on the amount of remaining dna dsbs demonstrated by our results , is in contrast to other investigations and may be due to the long time interval of 24 h for dna dsb repair experiments and the use of cfge instead of pfge ( pulsedfield gel electrophoresis )  . 
especially , the long time interval for repair experiments , allowing for the completion of fast and slow repair processes , could be responsible for our results . otherwise , with increasing intervals following rt , there is a risk of measuring beginning apoptosis , though other groups found no evidence for enhancementof radiosensitization by gemcitabine with increased programmed cell death [ 12 , 17 , 19 ]  . 
 moreover , a considerable effect of clinically relevant gemcitabine concentrations was demonstrated , as gemcitabine , 15 min after a 30 - min infusion , led to plasma concentrations between 10 to 40 mol / l [ 20 ]  . 
this was quite unexpected , as the key enzyme for the activation of gemcitabine , deoxycytidine kinase ( dcyd kinase ) , is described to be saturated by concentrations between 10 to 230 mol / l dfdc , in dependence on the cell lines used [ 5 , 28 ]  . 
furthermore , van haperen et al found no correlations between dcyd kinase and cell survival [ 28 ] , implicating that other pathways or mechanisms , like depletion of the nucleoside triphosphate pools [ 15 ] , inhibition of deoxycytidine monophosphate deaminase [ 9 ] , or effects on the cell cycle [ 14 , 16 , 24 ] , may have contributed to the dose - dependent effects of gemcitabine , especially at higher concentrations . this could be the reason for the only modest increase of residual dna damage between 100 and 1 , 000 mol / l , as demonstrated by our results and almost identical curves at lower dfdc concentrations . 
 furthermore , the calculated enhancement factors for combined gemcitabine and radiation treatment were significantly higher for low - dose compared to high - dose irradiation . this seems to be an important point for the clinical use of gemcitabine within simultaneous rct schemes . 
 strahlentherapie und onkologie originalarbeit radiochemotherapie mit gemcitabin und cisplatin bei pankreaskarzinom durchfhrbar und effektiv ralf wilkowski1 , martin thoma1 , volker heinemann2 , horst - gnter rau3 , andreas wagner4 , clemens stoffregen5 , eckhart dhmke1 hintergrund : die simultane radiochemotherapie unter verwendung von gemcitabin scheint bei der behandlung des pankreaskarzinoms ein hoffnungsvoller ansatz , da gemcitabin als monosubstanz oder in kombination mit anderen zytostatika eine verbesserte wirksamkeit beim ( metastasierten ) pankreaskarzinom im vergleich zu 5 - fu - haltigen therapieschemata zeigt und zudem strahlensensibilisierendes potential besitzt . 
 patienten und methode : 57 patienten ( w / m 23 / 34 ) mit pankreaskarzinom wurden insgesamt behandelt , davon 33 patienten mit inoperablem tumor , 19 patienten nach tumorresektion ( r1 - resektion und / oder pn + ) sowie fnf patienten mit lokalrezidiv . 
simultan zur bestrahlung wurden cisplatin 30 mg / m2 und gemcitabin 300 mg / m2 an den tagen 1 , 8 , 22 und 29 verabreicht . nach abschluss der simultanen radiochemotherapie wurden sequentiell zwei zyklen gemcitabin / cisplatin ( 1000 mg / m2 / 50 mg / m2 d 1 , 15 ) verabreicht . 
 ergebnisse : bei einer medianen nachbeobachtungszeit von 8 , 2 monaten betrgt die aktuelle mediane berlebenszeit 14 , 8 monate ( inoperable patienten 10 , 3 monate , postoperative patienten 15 , 1 monate )  . 
insgesamt konnten 14 patienten sekundr operiert werden . unter adquater antiemese mit ondansetron und dexamethason traten keine gastrointestinalen toxizitten who - iii oder - iv auf . die hmatotoxizitt war die gravierendste nebenwirkung ( leukopenie grad iii und iv bei 29 und fnf patienten , thrombopenie grad iii und iv bei 21 und acht patienten ) , jedoch nur mit geringer klinischer relevanz ( ein neutropenischer infekt , eine hbwirksame epistaxis )  . 
 schlsselwrter : pankreaskarzinom radiotherapie chemotherapie gemcitabin cisplatin strahlenther onkol 2003 ; 179 : 7886 doi 10.1007 / s00066 - 003 - 1036 - x radiochemotherapy with gemcitabine and cisplatin in pancreatic cancer feasible and effective background : concomittant radiotherapy and chemotherapy with gemcitabine appears to be a promising tool for the treatment of pancreatic cancer since gemcitabine applied as single or combination therapy proved to have better efficacy in pancreatic cancer than 5 - fu containing schemes and furthermore offers radiosensitizing potential . 
in the present paper our pilot data of concomittant and sequential chemoradiation with gemcitabine and cisplatin are presented . patients and methods : a total of 57 patients ( f / m 23 / 34 ) with pancreatic cancer was treated , of whom 33 patients had irresectable tumors , 19 patients following resection ( r1 and / or pn + ) and five patients with local recurrent disease . 
 1 klinik und poliklinik fr strahlentherapie , klinikum grohadern , ludwig - maximilians - universitt mnchen , 2 medizinische klinik iii , klinikum grohadern , ludwig - maximilians - universitt mnchen , 3 abteilung fr viszeralchirurgie , klinikum dachau , 4 medizinische klinik ii , klinikum grohadern , ludwig - maximilians - universitt mnchen , 5 lilly deutschland gmbh , bad homburg . 
in 14 patients a secondary resection was possible . using leveled antiemetics with ondansetron and dexamethasone no gastrointestinal toxicities grade iii or iv were observed . hematologic toxicities were the most grave side effects ( leukocytopenia iii / iv in 29 / five patients and thrombocytopenia iii / iv in 21 / eight patients ) , however with minor clinical relevancy ( one neutropenic infection , one thrombopenic epistaxis )  . conclusion : the presented treatment scheme using concomittant and sequential gemcitabine and cisplatin with radiation is feasible with justifiable side effects . 
to evaluate the promising remission and survival rates , randomized trials of neoadjuvant and primary chemoradiation are started . key words : pancreatic cancer radiotherapy chemotherapy gemcitabine cisplatin einleitung die behandlung des pankreaskarzinoms ist nach jahren der stagnation wieder zunehmend in das blickfeld des wissenschaftlichen interesses gerckt . 
in bezug auf die mortalitt steht das pankreaskarzinom allerdings an fnfter stelle , was die bisher unbefriedigende prognose widerspiegelt und den bedarf , neue therapiestrategien zu entwickeln [ 37 ]  . 
etwa 40% der tumoren werden in einem lokal fortgeschrittenen stadium entdeckt , und bei weiteren 40% der patienten liegen bei diagnosestellung bereits fernmetastasen vor . das pankreaskarzinom hat mit einer 5 - jahres - berlebensrate von 14% die schlechteste prognose unter den gastrointestinalen tumoren [ 3 ]  . 
 bei lokal fortgeschrittenen , inoperablen tumoren hat sich die kombinierte radiochemotherapie insbesondere durch die arbeiten der gastrointestinal tumor study group ( gitsg ) [ 12 , 14 ] als wirksamste therapiemanahme etabliert . 
 seitens der eingesetzten chemotherapeutika galt ber jahrzehnte 5 - fu als mittel der wahl und ist auch heute noch bei konkomittanter strahlentherapie als standard anzusehen . kombinationschemotherapien , wie fam ( 5 - fu , doxorubicin , mitomycin c ) , smf ( streptozotocin , mitomycin c , 5 - fu ) oder das mallinson - regime ( 5 - fu , cyclophosphamid , methotrexat und vincristin ) fhrten bei gesteigerter toxizitt zu keiner verbesserung der berlebenszeit [ 9 ]  . 
darberhinaus wurden fr gemcitabin strahlensensibilisierende effekte experimentell nachgewiesen [ 24 , 27 , 29 , 34 ] , die den einsatz dieser substanz simultan zur bestrahlung als hoffnungsvoll erscheinen lassen . 
 inzwischen liegen erste ermutigende ergebnisse fr die simultane radiochemotherapie beim pankreaskarzinom unter verwendung von gemcitabin als monosubstanz [ 2 , 10 , 16 , 23 , 26 , 28 , 32 , 39 ] oder in kombinationschemotherapien [ 4 , 22 ] vor . 
anzumerken ist jedoch , dass einige autoren [ 2 , 4 , 10 , 22 ] auf verstrkte insbesondere gastrointestinale oder hmatologische toxizitten aufmerksam machen , so dass die anwendung von gemcitabin simultan zur strahlentherapie nicht unumstritten ist , zumal eine ideale dosierung und applikationsform noch nicht definiert werden konnte [ 30 ]  . 
hierbei zeigte sich fr cisplatin ein synergistischer effekt , wobei gemcitabin dna - reparaturmechanismen nach cisplatin - induzierter schdigung hemmen kann und cisplatin den gemcitabin - katabolismus durch hemmung der ribonukleotidreduktase beinflusst . 
in anlehnung an die verbesserte effektivitt , die durch die kombination von gemcitabin und cisplatin bei alleiniger chemotherapie gezeigt werden konnte [ 15 ] , verwendeten wir diese beiden substanzen sequentiell und simultan zur bestrahlung . neben den remissionsund berlebensraten soll im folgenden ein besonderes augenmerk auf die beobachteten nebenwirkungen und toxizitten gelegt werden , um die durchfhrbarkeit dieses regimes zu beurteilen . 
radiochemotherapie bei pankreaskarzinom patienten und methode von februar 2000 bis september 2001 wurden insgesamt 57 patienten ( w / m = 23 / 34 ) mit histologisch nachgewiesenem pankreaskarzinom mit kombinierter radiochemotherapie behandelt . 
die feststellung der inoperabilitt erfolgte von erfahrenen pankreaschirurgen innerhalb unserer klinik anhand etablierter kriterien ( gefbeteiligung der peripankreatischen hauptgefe > 180 , regionre lymphknotenmetastasierung , ausgedehnte retroperitoneale infiltration )  . 
19 patienten ( gruppe 2 ) wurden postoperativ nach inkompletter ( r1 - ) resektion und / oder histologisch gesichertem lymphknotenbefall behandelt ( pn + bei 14 patienten )  . 
einschlusskriterien zur therapie waren alter ( < 75 jahre ) , allgemeinzustand ( karnofsky - index 70 ) , eine ausreichende nierenfunktion ( kreatinin - clearance > 80 ml / min ) sowie der ausschluss einer systemischen metastasierung ( mittels abdominellem und thorakalem ct )  . 
bei operierten patienten das tumorbett sowie die regionalen peripankreatischen lymphknoten mit einem sicherheitssaum von 23 cbei 50 patienten wurde dieses volumen bis zu einer gesamtdosis von 45 , 0 gy im icru - referenzpunkt in konventioneller fraktionierung mit 1 , 8 gy einzeldosis fnfmal wchentlich bestrahlt . 
nach abschluss der simultanen radiochemotherapie wurden sequentiell zwei zyklen nach dem g / c - schema bestehend aus gemcitabin 1000 mg / m2 und cisplatin 50 mg / m2 an den tagen 1 und 15 mit zykluswiederholung ab tag 29 verabreicht . 
clinical and treatment data of patients with irresectable ( group 1 ) , postoperative ( group 2 ) or locally recurrent ( group 3 ) pancreatic cancer . patientenzahl alter median ( bereich ) karnofsky - performance - index tumorbzw . 
radiochemotherapie bei pankreaskarzinom gewertet , als komplette remission ( cr ) das verschwinden jeglicher ct - morphologischer krankheitszeichen und als progress ( pd ) eine mindestens 25%ige zunahme der tumorgre oder das auftreten neuer herde . 
nachsorgeuntersuchungen mittels klinischer und laboruntersuchungen , ct von abdomen und thorax sowie bestimmung der tumormarker ca19 - 9 und cea bei abschluss der strahlentherapie , nach beendigung der sequentiellen chemotherapie sowie im anschluss in 812 - wchentlichen abstnden durchgefhrt . 
nach einer erholungsphase bedingt durch das chemotherapiefreie intervall in der dritten behandlungswoche nimmt bis zum ende der simultanen radiochemotherapie ( tag 36 ) der anteil der patienten mit thrombopenie insbesondere who - grad iii und iv kontinuierlich zu . 
seitens der leukozyten ist ein hnlicher verlauf zu sehen , wobei die erholungsphase nach der dritten behandlungswoche weniger ausgeprgt erscheint hier ist hauptschlich ein rckgang des teils der patienten mit gradiii - leukopenie zu verzeichnen . 
der makroskopische tumor ( 1 , innere umrandung , umschlossen von der 100% - isodose 3 ) sowie tumor und regionaler lymphabfluss ( 2 , uere umrandung , umschlossen von der 90% - isodose 4 ) wurden als zielvolumina markiert . 
gross tumor volume ( 1 , enclosed by the 100% - isodose 3 ) and tumor with locoregional lymph nodes ( 2 , enclosed by the 90% - isodose 4 ) were marked as treatment volumes . 
hierunter besserte sich die leberfunktion deutlich , allerdings trat im rahmen der steroid - induzierten immunsuppression eine atypische pneumonie auf , an der der patient verstarb ( 3 , 3 monate nach therapie )  . 
hierbei wurde in elf fllen eine whipple - operation ( acht r0und drei r1 - resektionen ) durchgefhrt , in zwei fllen eine pankreaslinksresektion ( eine r0und eine r1 - resektion )  . 
 berleben die mediane nachbeobachtungszeit nach abschluss der radiochemotherapie betrgt fr alle patienten zum zeitpunkt der datenerhebung im februar 2002 8 , 2 monate ( 0 , 420 , 7 monate )  . 
die aktuelle mediane berlebenszeit ab diagnose betrgt fr alle patienten 14 , 8 1 , 9 monate , wobei die postoperativ behandelten patienten mit einem medianen berleben von 15 , 1 monaten die gnstigste prognose haben . 
das mediane berleben ab diagnose betrgt fr die primr inoperablen patienten , bei denen eine sekundre tumorresektion durchgefhrt wurde ( n = 14 ) 11 , 7 3 , 4 monate , fr die nicht resezierten patienten 10 , 0 3 , 7 monate ( nicht signifikant )  . 
hier gleichen sich die medianen berlebenszeiten der inoperablen patienten mit 16 , 4 2 , 1 monaten und die der postoperativ behandelten patienten mit 15 , 1 monaten an , bei den patienten mit lokalrezidiv ist das mediane tumorabhngige berleben noch nicht zu berechnen . 
 das mediane progressionsfreie berleben nach abschluss der radiochemotherapie , berechnet nach der kaplanmeier - methode , betrgt fr alle patienten 11 , 1 1 , 0 monate . fr die inoperablen patienten betrgt das progressionsfreie berleben im median 10 , 8 3 , 7 monate , nach tumorresektion 10 , 7 1 , 1 monate , bei patienten mit lokalrezidiv kann noch kein me - dian berechnet werden , da drei der fnf patienten bisher progressionsfrei sind . 
die medianen berlebenszeiten fr inoperable patienten ( gruppe 1 ) betragen 10 , 3 2 , 2 monate , fr postoperativ behandelte patienten ( gruppe 2 ) 15 , 1 monate . 
 eine patientin mit vorbestehendem diabetes mellitus entwickelte eine periphere polyneuropathie ( 1 monat nach radiochemotherapie ) , deren ursache nicht eindeutig geklrt werden konnte , die aber letztlich das absetzen der sequentiellen cisplatin - applikationen erforderlich machte . 
in verschiedenen 5 - fu - basierten studien aufbauend auf den ergebnissen der gastrointestinal tumor study group ( gitsg ) [ 12 , 14 ] konnte eine verbesserung des ansprechens und auch des berlebens gezeigt werden im vergleich zu alleiniger bestrahlung oder chemotherapie . 
in den randomisierten gitsg - studien wurden mit kombinierter radiochemotherapie mediane berlebenszeiten von etwa 10 monaten erreicht . in weiteren nicht randomisierten studien [ 5 , 17 , 18 ] wurden berlebenszeiten zwischen 9 , 6 und 11 monaten sowie ansprechraten zwischen 10% und 37% angegeben . 
 resektables pankreaskarzinom fr die adjuvante behandlungssituation nach potentiell kurativer resektion eines pankreaskarzinoms gibt es bisher trotz der hohen lokalrezidivrate von bis zu 50% und der schlechten langzeitprognose keine etablierte therapiestrategie . 
zum einen konnte zwar in randomisierten studien von der gitsg [ 13 , 19 ] ein signifikanter berlebensvorteil zugunsten adjuvanter 5 - fu - basierter radiochemotherapie gezeigt werden , der auch von anderen studien besttigt wurde [ 11 , 36 , 41 ]  . zum anderen jedoch zeigten groe europische studien keine signifikanten vorteile fr die adjuvante radiochemotherapie [ 21 ] oder sogar eine verschlechterung der prognose im vergleich zu alleiniger chemotherapie [ 31 ]  . 
inzwischen hat jedoch bei alleiniger chemotherapie gemcitabin zunehmend an bedeutung gewonnen , da bei guter vertrglichkeit und gnstigem nebenwirkungsprofil eine verbesserte ansprechrate und symptompalliation im vergleich zu 5 - fu gezeigt werden konnte [ 6 , 33 ]  . 
die mehrzahl der studien verwendete gemcitabin als monosubstanz [ 2 , 10 , 16 , 23 , 26 , 28 , 32 , 39 ] , wobei die optimale dosis und applikationsart bisher nicht definiert werden konnten [ 30 ]  . 
hierzu liegen arbeiten zur kombination von gemcitabin mit mitomycin c [ 22 ] und cisplatin [ 4 ] vor sowie eigene pilotdaten zur kombination mit 5 - fu [ 38 ] , die zeigen , dass diese kombinationsbehandlung effektiv , aber auch toxisch ist . 
 die beobachteten hmatotoxizitten mit 50% gradiiiiv - thrombopenien und 60% grad - iiiiv - leukopenien sind im vergleich mit 5 - fu - basierten studien , bei denen lediglich in etwa 20% grad - iiiiv - toxizitten zu erwarten sind , hher . 
auerdem deutet die tatsache , dass bisher von den 57 behandelten patienten lediglich in vier fllen ein lokalrezidiv ( n = 2 ) oder eine erneute lokale tumorprogression ( n = 2 ) auftrat , darauf hin , dass die von uns durchgefhrte behandlung eine hohe lokale effektivitt besitzt . 
 unsere ergebnisse zeigen fr primr inoperable patienten bezglich des gesamtberlebens ( median 10 , 3 monate ) im vergleich mit den daten der literatur zur 5 - fu - basierten radiochemotherapie noch keinen vorteil bei z.t. 
 schlussfolgerung zusammenfassend sprechen die erzielten ergebnisse somit fr eine verbesserte lokale effizienz durch die strahlentherapie mit gemcitabin und cisplat einschrnkend muss natrlich darauf hingewiesen werden , dass es sich bei den hier vorgestellten daten nur um pilotdaten handelt , die nicht randomisiert erhoben wurden , was die vergleichbarkeit insbesondere bezglich der berlebenszeiten mit anderen arbeiten bzw . 
um seine wertigkeit insbesondere im vergleich zur bisher als standard angesehenen 5 - fu - basierten radiochemotherapie zu evaluie - ren , sind derzeit zwei randomisierte studien gestartet . fr operable patienten wird eine neoadjuvante radiochemotherapie mit anschlieender operation gegen alleinige operation verglichen ( studienzentrale erlangen , studienleiter hohenberger , strahlentherapie : grabenbauer )  . 
bei inoperablen patienten wird eine primre radiochemotherapie mit gemcitabin / cisplatin sequentieller chemotherapie mit gemcitabin / cisplatin verglichen mit primrer radiochemotherapie mit 5 - fu ( studienzentrale mnchengrohadern , studienleiter wilkowski )  . 
therapy of locally unresectable pancreatic carcinoma : a randomized comparison of high dose ( 6000 rads ) radiation alone , moderate dose radiation ( 4000 rads + 5 - fluorouracil ) and high dose radiation + 5 - fluorouracil . 
a phase i study of preoperative gemcitabine ( gem ) with radiation therapy ( rt ) followed by postoperative gem for patients with localized , resectable pancreatic adenocarcinoma ( pac )  . 
a phase i trial of radiation therapy ( rt ) plus concurrent fixed dose amifostine ( ami ) with escalating doses of twice - weekly gemcitabine in advanced pancreatic cancer . 
2 urban & vogel strahlentherapie und onkologie technical note remote afterloading for neutron brachytherapy using californium - 252 taco tacev1 , grigor grigorov2 , toms paprek2 , vladimr kolark2 background : despite a pronounced technical progress attained in radiotherapy of malignant neoplasms , no remarkable improvement in the treatment results has been achieved . 
the design of a remote afterloading device using 252cf sources remains an unsolved problem . material and methods : the afterloading device has been designed as a stationary radiator which is composed of three mutually interconnected units : the control and drive unit consisting of a control computer and a motor - driven bowden system carrying the 252cf source ; the source which is housed in a watertight concrete vessel - storage strong room , situated in the ground at a depth of 125 cm beneath the patients bed ; the afterloading application module installed in the irradiation room . results : remote afterloading allows simple , inexpensive and highly efficient radiation protection and work safety for the operating personnel . 
the sources may be moved arbitrarily during treatment with a position accuracy of 0.51.0 mm within a distance of 520 cm from the source storage position in the strong room to the application position . 
both afterloading systems unused indexer outputs are protected electronically and mechanically against any unintentional movement of the source outside the application tubes . conclusion : the technologic concept of the present automatic afterloading device for neutron brachytherapy represents a possible option from the range of conceivable design variants , which while minimizing technologic and economic requirements provides the operating personnel with optimum protection and work safety , thus extending the applicability of high let radiationbased treatment methods in clinical practice . key words : brachytherapy californium - 252 remote afterloading automatisches afterloading fr die neutronen - brachytherapie mit californium - 252 hintergrund : trotz eines erkennbaren technischen fortschritts in der strahlentherapie maligner neoplasmen ist keine nennenswerte verbesserung der behandlungsergebnisse erzielt worden . 
das design einer automatischen afterloading - einheit fr 252cf - neutronen - brachytherapie ist ein bislang noch offenes problem . material und methodik : die afterloading - einheit ist als eine im bestrahlungsraum fest eingebaute vorrichtung konstruiert , die sich aus drei miteinander verbundenen elementen zusammensetzt : die steuerund antriebseinheit besteht aus einem steuercomputer und aus einem motorantrieb mit stahlseil , welcher den 252cfstrahler trgt . der strahler wird in einem wasserdichten behlter in einem aufbewahrungstresor untergebracht , der im boden in einer tiefe von 125 cm unter dem bett des patienten platziert wird . das afterloading - applikationsmodul wird im bestrahlungsraum aufgestellt . ergebnisse : automatisches afterloading ermglicht einen preiswerten und hchst effizienten strahlenschutz mit gleichzeitiger arbeitssicherheit fr das bedienungspersonal . 
die quellen knnen whrend der behandlung mit einer positionsgenauigkeit von strahlenther onkol 2003 ; 179 : 1137 doi 10.1007 / s00066 - 003 - 1006 - 3 1 masaryk memorial cancer institute , brno , czech republic , 2 delong instruments , brno , czech republic . received : february 13 , 2002 ; accepted : august 15 , 2002 strahlenther onkol 2003 no . 
beide afterloading - systeme verwenden indexer - austritte , die elektronisch und mechanisch gegen etwaige unbeabsichtigte bewegung der quelle auerhalb der applikationsrhre geschtzt werden . schlussfolgerung : das technische konzept der prsentierten automatischen afterloading - einheit fr die neutronen - brachytherapie stellt eine der mglichen designvarianten dar , die bei minimierung der technischen und konomischen anforderungen dem personal einen optimalen strahlenschutz und arbeitssicherheit bietet . 
 schlsselwrter : brachytherapie californium - 252 automatisches afterloading introduction despite a pronounced technical progress attained in the radiotherapy of malignant neoplasms [ 1 , 3 , 6 ] , no remarkable improvement in the treatment results has been achieved . 
the reason for this stagnation is the interaction between tumor cell and photon radiation , where the required biological effect , implicating tumor cell killing , is being mediated in most cases and , therefore , conditioned by several factors and phenomena , which , in turn , result in a variety of radiosensitivity data for different tumor populations [ 7 ]  . 
although the physical and radiobiological background for using neutrons and other unconventional radiation sources has already been worked out , any clinical application of these sources for external tumor irradiation remains rather objectionable . 
 the discovery of californium - 252 ( 252cf ) nuclide [ 2 , 10 ] , a source of gamma neutron radiation , featuring a neutron emission of 2.3 ( cid : 1 ) 1012 s1g1 and a mean energy of 2.102.37 mev , established good conditions for using neutrons in tumor brachytherapy [ 5 ]  . 
in contrast to teletherapy , brachytherapy makes an immediate interaction of neutrons and tumors possible , and , moreover , the economic and technical requirements connected with its introduction into clinical practice do not exceed those of conventional photon brachytherapy . 
 since the mid - 70s , the physical , dosimetric , clinical and radiobiological background for using 252cf nuclide in tumor brachytherapy has been gradually established , being confirmed by clinical application results [ 5 ]  . 
the prospects of neutron brachytherapy were evaluated , on the basis of long - term results achieved in the treatment of tumors of the oral cavity and cervical carcinoma , during the californium - 252 isotope for 21st century radiotherapy workshop , held in detroit , usa , in 1996 [ 12 ]  . 
a problem that remains unsolved is the design of a remote afterloading device using 252cf sources . the key design problem connected with any automatically operating afterloading device for neutron brachytherapy consists in an appropriate technical approach to the safety at work and radiation protection of the operating personnel . whereas the shielding from photon radiation of afterloading devices employing nuclide - based gamma radiation sources may be achieved by using heavy elements , such as tungsten , an appropriate shielding from neutrons requires materials consisting of light elements , such as water , paraffin or plastics , in the molecules of which hydrogen atoms are prevailing . 
however , this circumstance makes the volume of the storage strong room increase considerably , particularly in cases where mediumand high - activity sources are used for treatment . this paper deals with our design of an automatic afterloading device intended for 252cf source - based neutron brachytherapy . 
 material and methods when dealing with the design concept of the 252cf sourcebased remote afterloading system , we made use of the experience gained by our experimental worksite , where the storage strong room had the form of a concrete block situated beneath the irradiation rooneutron source cartridges were placed at the bottom ends of 1 m long polyethylene rods , which used to be pushed into stainless - steel pipes situated in a concrete block [ 8 ]  . 
we have employed this simple and inexpensive method of neutron radiation shielding in the design of our neutron brachytherapy afterloading device . the afterloading device has been designed as a stationary radiator which is composed of three mutually interconnected units ( figure 1 ) : the control and drive unit , which is installed in the anteroom to the radiation room , consists of a control computer and a motor - driven bowden system which is carrying the 252cf source . 
during treatment , this unit slides the source into the application position , carries out program - controlled movements in the application system , and , finally , slides the source back into the storage strong roothe design of the control and drive system makes it possible to move the source , as needed , automatically from any application position into the storage strong room quickly and safely . 
 the control computer is coordinating the operation of the drive motors , the indexer and the electronic sensor system whose task is to secure accurate movements of the source in the bowden syste furthermore , it processes and checks the signals coming from the entire system control , informastrahlenther onkol 2003 no . 
these 18 sources are divided into six airtight stainless - steel cartridges of 17 mm length and 1.2 mm diameter each , to be inserted in the form of triplets . 
each of the thus created sources is moved via an independent drive unit and may be directed , by means of the indexer , to any of the three different positions during treatment , so that a total of 18 independent outputs for interstitial treatment are available . for intracavitary treatment , we have employed an hk252m41.58 - type source with an initial content activity of 6.0 ( cid : 1 ) 109 bq , whose effective length is 9.0 mm , while the cartridges total length and diameter amount to 15 mm and 3.0 + 0 , 12 mm , respectively . 
in view of very severe requirements concerning source transport and subsequent installation into the cartridge , we have employed a medium - activity source ( 200 g ) for the first stage of the neutron afterloading operation in the clinical environment . 
 the 252cf afterloading units are placed in the rooms formerly accommodated with radiocobalt irradiators ( now disposed of ) , whose walls and ceiling are made of barite concrete having a thickness of 60120 cto achieve the required neutron radiation protection , the walls and the ceiling of the irradiation room have been thickened by adding a 24 cm thick neutronstop brick wall . 
 results the tumor neutron brachytherapy afterloading system described above has been designed to conform to european standards for the development and production of such devices , taking the specific radiohygiene - related requirements concerning neutron radiation protection into account . 
its basic operating parameters bear comparison with those of similar nuclide source devices , however , with a certain distinctiveness : it allows simple , inexpensive and highly efficient radiation protection and work safety for the operating personnel which is handling neutron radiation sources , including highactivity ones . 
konstruktionsschema einer automatischen afterloading - anlage zur neutronenbrachytherapie mit 252cf . tion and safety elements , displaying these signals continuously on the computer monitor screen and on control panels situated in the operating personnel room and at the entrance to the irradiation room . the source is housed in a watertight concrete vessel - storage strong room , situated in the ground at a depth of 125 cm beneath the patients bed . 
to shield off the 252cf source gamma radiation , the stainless - steel tube is bridged with a 3 cm thick lead sheet extending over the whole length of the storage strong roothe remaining free space of the tank is filled with polyethylene bricks of neutronstop type , and the upper outside surface of the strong room is covered with a steel sheet coated with a floor - covering material . 
 while 192ir nuclide gamma source - based afterloading is capable , thanks to the high specific activity of this source , to minimize the volume of the radiation source so as to make it applicable in interstitial and intracavitary high - dose rate ( hdr ) brachytherapy , such an approach is impracticable for neutron afterloading , due to the relatively low specific activity of 252cf . 
 our selection of applicable medical 252cf sources has been based on the current market situation , where only the national scientific center of russia is offering neutron sources for medical purposes , namely , hk252m41 and hk252m3 types , featuring an activity range from 1.2 ( cid : 1 ) 1076.0 ( cid : 1 ) 1010 bq . 
leistung der raumdosisquivalente fr neutronen und photonen in applikationsrumen fr intrakavitre ( a ) und interstitielle ( b ) brachytherapie . standard application ( of 6 gy on the referential isodose ) at intracavitary afterloading we found , on the applicator surface , the value of the equivalent rate doses of photon radiation 10 sv / h , or 5.4 sv / h in 1 h . the sources may be moved arbitrarily during treatment with a position accuracy of 0.51 mm within a distance of 520 cm from the source parking position in the storage strong room to the application position . to reduce the time of the sources safe transfer from the storage strong room to the application position , the transfer speed features two set - point values : in the underground up to the indexer output 100 mm / s , in the application system 50 mm / s . 
 if the application systems patency is disturbed during treatment , both afterloading systems interrupt the treatment and return the sources into their parking positions in the storage strong room automatically . 
 both afterloading systems unused indexer outputs are protected electronically and mechanically against any unintentional movement of the source outside the application tubes . the connection of the indexers with the application tubes is being checked electronically and mechanically . 
in the intracavitary afterloading system , allowing therapeutic application of high - activity sources , the connection of the application tubes with the application system is also being checked electronically . 
 the treatment history information is printed in the form of a log , and , in addition , managed by the central computer ; it is saved in the central computer memory . 
 conclusion the results of neutron brachytherapy treatment of cervical cancer and tumors of the oral cavity , using 252cf nuclide , show the potential to reach 80% local control of advanced tumors [ 4 , 5 , 9 , 11 ] , as a consequence of breaking down the tumor resistance against conventional photon irradiation . 
 the technical concept of the presented automatic afterloading device for neutron brachytherapy represents one of the possible options from a range of conceivable design variants , which while minimizing the technical and economic requirements provides the operating personnel with optimum protection and work safety , thus extending the applicability of high let radiation - based treatment methods in clinical practice . 
 strahlentherapie und onkologie review article radiation - induced bystander effects mechanisms , biological implications , and current investigations at the leipzig lipsion facility jan sterreicher1 , 2 , kevin m . 
tanner4 background : the bystander effect is a relatively new area of radiobiological research , which is aimed at studying post - radiation changes in neighboring non - hit cells or tissues . 
the bystander effect of ionizing irradiation is important after low - dose irradiation in the range of up to 0.2 gy , where a higher incidence of stochastic damage was observed than was expected from a linearquadratic model . 
it is also important when the irradiation of a cell population is highly non - unifor objective : this review summarizes most of the important results and proposed bystander effect mechanisms as well as their impact on theory and clinical practice . 
several groups worldwide are working on understanding its different aspects and its impact on radiobiology and radiation protection . conclusion : the observation of a bystander effect has posed many questions , and answering them is a challenging topic for radiobiology in the future . 
 key words : radiobiology bystander effect radiation induction cell - cell communication strahlenther onkol 2003 ; 179 : 6977 doi 10.1007 / s00066 - 003 - 1000 - 9 strahleninduzierte bystander - effekte . 
der strahleninduzierte bystander - effekt spielt eine wichtige rolle vor allem im niedrigdosisbereich 0 , 2 gy , wo die inzidenz des stochastischen zellschadens in experimenten grer ist als die berechnung nach dem linearquadratischen modell . 
 ziel : dieser bersichtsartikel fasst die wichtigsten ergebnisse der bystander - effekt - forschung zusammen und gibt einen ausblick auf mgliche mechanismen sowie auf die bedeutung fr theorie und klinische praxis . 
 schlsselwrter : radiobiologie bystander - effekt strahleninduktion interzellulre kommunikation 1 department of nuclear solid state physics , faculty of physics and geosciences , university of leipzig , germany , 2 department of radiobiology and immunology , purkyne military medical academy , hradec krlov , czech republic , 3 gray cancer institute , mount vernon hospital , northwood , middlesex , united kingdom , 4 clinic and polyclinic of radiation oncology , martin luther university halle - wittenberg , germany . 
radiation - induced bystander effects introduction the expression bystander effect derives from an observation in cancer gene therapy , where tumor cells were transfected with herpes simplex virus thymidine kinase ( hsv - tk ) rendering them susceptible to the cytotoxicity of subsequent ganciclovir therapy . 
studies by various groups after the first description of a radiation - induced bystander effect can be divided into two main approaches . one is using - particle irradiation of fibroblasts with the endpoint of sister chromatid exchange ( sce ) , media transfer experiments with reactive oxygen species ( ros ) , and cell - to - cell communication by gap junctions ( gjic )  . 
it is a matter of discussion whether epithelial cells and fibroblasts both show the bystander effect , whether the various endpoints used can be compared , whether the mechanisms are more likely by ros or by cytokines ( like interleukins [ il ] , tumor necrosis factor alpha [ tnf - ] ) , and whether - particle irradiation and - exposure are equally effective . 
in the data of nagasawa & little [ 39 ] , comparable levels of bystander sces were seen with 0.3 mgy - particles and 2 gy of x - rays . 
 the theoretical role of a bystander effect of ionizing irradiation radiation - induced dna mutations and oncogenic transformation are classified as stochastic effects of ionizing irradiation [ 12 , 41 ]  . 
the probability of radiation - induced stochastic effects is still described by the useful linear - quadratic model [ 18 , 33 ] , from which a linear probability of dose - effect up to about 1 gy is followed by a quadratic dose - effect relationship for higher absorbed doses [ 18 ]  . 
 in terms of timescale , initial direct and indirect effects of ionizing radiation last up to 1 ( cid : 1 ) 106 s after irradiation [ 33 ]  . bystander effect mechanisms are generally slower , because they start after the release of compounds with clastogenic activity up to 1 h after irradiation and the endpoint can be seen days after irradiation . 
activation of these still poorly characterized signaling pathways can induce various endpoints such as dna damage , dna mutations , chromosomal imbalance and genomic instability , [ 24 , 57 , 59 ] , apoptosis [ 3 , 5 , 44 ] , micronucleus formation [ 6 , 43 ] , oncogenic transformation [ 10 , 50 ] , decline in cell survival and colony forming ability [ 27 , 38 ] , and premature differentiation of nondifferentiated subpopulations of epithelium [ 4 , 5 ]  . 
with the development of the microbeam single - ion irradiation technology , interest has turned to the post - irradiation behavior of surrounding nonirradiated cells and / or tissues . the microbeam facilities will specially be helpful in understanding the microdosimetry part of the effects of ionizing radiation directly at the single - cell level and the pathways of cell - to - cell communication . 
is the linear - quadratic model still valid in the range of very lowand low - dose irradiation ? results of the bystander effect research bystander effect - like phenomena have been reported since the early 1950s , when parsons et al [ 43 ] published reports on changes in sternal bone marrow following x - ray therapy of the spleen in chronic granulocytic leukemia . 
 further data about the interaction of cells hit and cells not hit by ionizing radiation came from hollowell & littlefield [ 20 ] in 1968 , who observed chromosome damage induced by plasma obtained from patients undergoing cancer radiotherapy . 
radiation - induced bystander effects clinical observations and experimental results concerning examples of abscopal effects have been reported by several authors , probably describing bystander effect - like phenomena , but possibly ( also ) inflammatory responses [ 22 , 35 ]  . the bystander effect using high let irradiation at very low doses was first described by nagasawa & little [ 39 ] in 1992 . 
the first one deals with ros and further free radical actions , their transport from irradiated to nonirradiated cells , the signaling pathways , and the role of cell - cell communication [ 25 ]  . 
 the pathways of the bystander effect for a better understanding of the bystander effect , it makes sense to divide this phenomenon into two functional parts : the part of action and the part of reaction . 
the irradiated cell is able to excrete molecules , and an unirradiated cell is able to react to these molecules , in a sense that together they are creating the bystander effect . 
the first function is the ability of irradiated cell ( s ) to release molecules inducing a bystander effect either into the extracellular space , to the medium ( in vitro model ) or to the extracellular matrix ( in vivo model ) , or to directly transport these molecules to the cytoplasm of neighboring cells via gap junctions [ 1 , 2 , 8 , 38 ]  . 
 the second function of bystander effect development now on the receiving side is the ability of neighboring , nonirradiated cells to react to the compounds ( with properties such as lipid peroxide and cytokines ) produced by irradiated cell ( s ) [ 38 ]  . 
with a fibroblast cell line in the same experimental setting , the bystander effect is not seen [ 36 ]  . some neighboring nonirradiated cells may also have a low frequency of response , so that a bystander effect might escape detection . 
it includes a decrease in cell survival , reduced proliferation rate , and dna damage with genomic instability , and higher apoptosis and micronucleus formation rates can be observed [ 36 , 10 , 27 , 38 , 44 , 57 , 59 ]  . 
this may be due to the relatively short time period of research in this area , starting around 1992 [ 39 ] , or due to low levels of molecules involved in this biological mechanisin recent years , p53 and p21 [ 31 ] as well as waf1 , p34 , cyclin b and rad 51 [ 1 ] were found to be overexpressed in bystander - responding cell lines . 
these molecules play an important role in apoptosis induction , cell cycle arrest , cell cycle delay , and signal transduction pathways [ 21 , 28 , 51 , 56 ]  . 
 gjic the next type of transport of radiation - induced molecules from hit to non - hit cells is often realized via gap junctions [ 1 , 8 ]  . 
this type of molecular transport from irradiated to nonirradiated cells is somehow limited by a decrease of the density of gap junctions in irradiated cells [ 24 , 52 ]  . 
in their experiment using a hamster - human hybrid cell line , the authors inhibited reactive oxygen radicals by dimethylsulfoxide ( dmso ) , a well - known scavenger of reactive oxygen radicals [ 19 , 26 , 55 , 57 ]  . 
their experiment had a human - hamster hybrid in the form of cho cells enriched with a single copy of human chromosome 11 containing cd59 gene locus as an indicator of mutagenicity . irradiation with eight - particles ( 90 kev / m let ) of the cystrahlenther onkol 2003 no . 
it is well known that thiols can bind reactive oxygen radicals and subsequently inhibit an indirect effect of irradiation [ 19 , 33 ]  . however , wu et al [ 57 ] found a threeto fourfold lower incidence of cd59 mutation when dmso was given , whereas bso treatment led up to sevenfold higher incidence of cd59 mutation after cytoplasmic irradiation . 
by contrast , dmso reacts mainly with oh with a short half - time , allowing a diffusion of up to 4 nm only [ 48 ] , not 8 m as used in this experimental setup . 
matsumoto et al [ 31 ] confirmed a radiation - induced generation of nitric oxide ( no ) , which , alone or via its metabolites , has a mutagenic effect [ 40 ]  . 
studies of malyshev et al [ 29 ] and forester et al [ 16 ] showed that no induces a heat - shock protein ( hsp ) production , particularly hsp 72 [ 32 ] , as well as a wild - type p53 protein , which plays a role in the adaptation of the organism to various stressors . 
komarova et al [ 23 ] proposed that tumor suppressor protein - ( tp 53 - ) dependent stress response induces secretion of growth inhibitors , which influence the bystander cells . 
it can be used on individual cells , even if confluent cell lines are left in situ . prise et al [ 44 ] have demonstrated the production of micronuclei , and , to a lesser degree , of apoptosis in a fibroblast population , when a small number of human fibroblasts were individually targeted by - particles . 
in a 3 - d model of urothelial cells , belyakov et al [ 5 ] measured a 10% higher premature differentiation of undifferentiated bystander cells than was found in the control group . 
an important study has been published by mothersill et al [ 38 ] describing the influence of oxidative stress and the energy balance for the ability of irradiated cells to produce and release clastogenic factors . 
however , if an irradiated cell line is protected against the consequences of oxidative stress , then a bystander effect via medium transfer to a nonirradiated cell culture is highly significant . 
the authors suggested that positive energy balance with adenosine triphosphate ( atp ) excess in irradiated cells is a supporting factor for the overproduction of factors inducing the bystander effect [ 38 ]  . 
 variation in quantification of the bystander effect in various in vitro or ex vivo experimental setups , several authors [ 57 , 36 , 38 , 39 , 44 , 50 , 59 ] measured an up to threeto fivefold higher presence of bystander effect in bystander nonirradiated populations in comparison with nonirradiated no - bystander control groups . 
this ratio is relatively high , for example in vitro , the frequency of cell alterations such as dna mutation and micronucleus formation in control ( noninfluenced ) groups is in the range of 104 [ 7 , 57 ]  . 
radiation - induced bystander effects theoretical impact of the radiation - induced bystander effects taking the above into account , there is a theoretical impact of the radiation - induced bystander effect . 
here , the frequency of the bystander effect significantly outnumbers the stochastic calculation . this means that the linear - quadratic model should be revised in this low - dose range . 
according to marples & joiner [ 30 ] , the revision of the linear - quadratic model will involve doses up to around 1 gy ( see limitation of the linear - quadratic model in the low - dose range )  . 
the knowledge of the effects on health from the hiroshima and nagasaki atomic bomb victims entered into these calculations as well as the information about pathogenetic mechanisms of damages in bronchial epithelium by radon - generated - particles . 
 abscopal effects in patients during radiotherapy understanding the development of the bystander effect may be a new impulse for the study of abscopal effects found in patients during or after radiotherapy . 
 in experiments with rats after irradiation of basal parts of the lung , a response in upper ( shielded ) parts of the lung was observed [ 22 , 34 , 44 ]  . 
 in targeted radiotherapy , as for example in boron neutron capture therapy ( bnct ) or in radioimmunotherapy , irradiation of the tumor may be highly heterogeneous in different tumor regions that would otherwise not be reached and survive . the anti - inflammatory effect of radiotherapy widely used in benign arthropathia is well known but not so well explained . in a model of adjuvant arthritis , the anti - inflammatory efficiency of low - dose radiotherapy has been confirmed by rdel et al [ 47 ] in vitro and in vivo . 
they had evidence for low - dose radiotherapy interfering with the combined effects of activated macrophages ( via cytotoxic and induced immunmodulatory no ) with endothelial cells ( via adhesion molecules like l - selectin and modulation of il - 10 and tnf - ) [ 47 ]  . 
more research on this topic is needed to clarify the controversies . limitation of the linear - quadratic model in the low - dose range dna damage results in proportion to dose applied in a model of linear relationship . 
so far , little is known regarding the mechanisms leading to radiation - induced genomic instability . bystander effects may influence the relationship between dose and damage in the low - dose region . 
 current biomedical research at lipsion microbeam facilities although clastogenic effects of irradiated blood plasma on nonirradiated tissue have been known since about 1954 [ 43 ] , and further abscopal effects have been described [ 13 , 34 , 37 ] , further research has not yielded a full explanation of the phenomenon . 
2 urban & vogel accelerator nanoprobe columbia university , usa [ 46 ] , the third is located at the department of nuclear engineering , texas a & m university , usa [ 9 ] , and the fourth belongs to the japanese atomic energy research institute in takasaki [ 49 ]  . further facilities are being developed at the institute of nuclear physics , krakov , poland , at the cenb , gradignan , france , and in germany at the gsi darmstadt , at the ptb braunschweig and , including our facility with a focused beam width of 40 nm , at leipzig university [ 11 ]  . 
a recent novel approach has also been developed at the gray laboratory which involves focused soft x - rays , giving submicron resolution [ 14 ]  . however , experimental work with microbeam facilities is still limited to in vitro or ex vivo experiments , where it is possible to follow the exact number , behavior , morphologic and functional status of each observed cell [ 15 , 46 ]  . 
 microbeam facility at leipzig university the biomedical research at lipsion concentrated on microscopy and tomography on chondrocytes in pig cartilages . it serves as a model of irradiation with the new facility of the microbeam to be able to hit a target in the submicrometer range . 
 an irradiation platform with an ion exit window ( the protons of the beam are produced in vacuum ) of si3n4 ( 100 nm thick ) and / or a mylar foil and a positioning system for the mini - petri dish ( 2 ( cid : 1 ) 2 mm active area ) is under construction . the prototype is currently undergoing testing and final adjustment . 
the mini - petri dish must contain fiducial markers outside the active area , which allow an accurate repositioning of the dish between the off - line cell observer and the irradiation stage . 
detektorbereich mit sekundrelektronen ( se ) , protoneninduzierter rntgenstrahlung ( pixe ) , ionentransmissionsmikroskopie ( stim ) und rutherford - rckstreuspektrometrie ( rbs )  . nical approach of the microbeam , individual cells and even targets within individual cells are within reach . 
 a typical microbeam facility is composed of ( figure 1 ) : an accelerator ( often a van de graaff model ) generating exact numbers of 3he2 + - particles or protons , equipped with a particle detector and a fast beam gate ; the nanoprobe : a collimating or focusing system creating a beam of 1 m diameter ; a microscope with an automatic positioning system for the specially designed cell culture ( petri ) dishes , a computerized image analysis system . so far , four charged - particle microbeam systems are in use worldwide for experimental radiation biology studies : the first started working at the gray laboratory in northwood , united kingdom [ 14 , 15 , 44 ] , the second is situated at the center for radiobiological research , figure 2 . 
 we have started experiments with cultures of human fibroblasts ( ag 01522 ) and human endothelial cells ( huvec )  . in a first series of experiments , the bystander effect of the cell lines is demonstrated by media transfer using as endpoints surviving fraction , apoptosis rates , and micronucleus formation . 
 outlook with further bystander effect research , and especially with the more precise single - cell research the use of microbeam offers , several dark spots in the picture of the bystander effects can be addressed . 
in radioimmunotherapy the understanding of a bystander effect in either enhancing tumor cell killing or damaging normal neighboring cells will be crucial . possible molecular biological mechanisms of bystander effects involving protein identification , cell signaling pathways , modulation of gene regulation , and role of ros will need to be studied . 
 the degree of radiation - induced bystander effect inhibition or enhancement will contribute to understanding the mechanism , but will probably also be an approach to treatment as is the case in the herpes simplex virus / thymidine kinase gene / ganciclovir model gene therapy . 
 the topic of low - dose irradiations including the levels of damage measurement of single cells and cell cultures irradiated by different energies and numbers of various types of ionizing radiation should be investigated . 
 in summary , the future of the bystander effect research is a panel of investigation , where many research groups with very different points of interest can find challenge to give more color and shadow to the picture . 
 strahlentherapie und onkologie original article logical checking function increases the accuracy of data entry in the patterns of care study katsuyuki kinoshita1 , teruki teshima1 , yuko ohno2 , toshihiko inoue3 , takashi yamashita4 , masahiro hiraoka5 , norio mitsuhashi6 , minako sumi7 , and japanese pcs working group background : for clinical studies , the use of a databases combined with a computer is becoming popular for data capturing . 
the study presented here quantitatively and prospectively evaluated the effectiveness for data management with this function using the database of patterns of care study ( pcs ) in japan . patients and methods : the first external audit was performed from september 1998 to march 1999 using the pcs database without the function , and the second from april to september 1999 with the function . 
this indicates the potential for increasing the accuracy of data capturing with the aid of a computer . key words : computer database data capturing logical checking patterns of care study ( pcs ) strahlenther onkol 2003 ; 179 : 10712 doi 10.1007 / s00066 - 003 - 1011 - 6 logische kontrollfunktionen erhhen die genauigkeit der datenerfassung in patterns - of - care - studien hintergrund : in klinischen studien verbreitet sich fr die datenerfassung zunehmend die verwendung von datenbanken zusammen mit computern . 
diese studie ermittelte quantitativ und prospektiv die effizienz dieser funktionen fr die datenverwaltung anhand der datenbank patterns of care study ( pcs ) in japan . patienten und methode : die erste externe erhebung wurde von september 1998 bis mrz 1999 durchgefhrt unter verwendung der pcs - datenbank ohne logische kontrollfunktionen und die zweite erhebung von april bis september 1999 mit diesen funktionen . 
 ergebnisse : in der datenbank ohne logische kontrollfunktionen betrug der anteil unkorrekter daten 2812 von 596186 ( 0 , 47% ) , whrend mit diesen funktionen die entsprechende zahl auf 161 von 533656 ( 0 , 03% ) signifikant vermindert wurde ( p < 0 , 0001 )  . 
 schlsselwrter : computer - datenbank datenerhebung logische kontrollfunktionen patterns - of - care - studie ( pcs ) 1 department of medical engineering , osaka university medical school , suita , japan , 2 department of care metrics , osaka university medical school , suita , japan , 3 division of multidisciplinary radiotherapy , osaka university graduate school of medicine , suita , japan , 4 department of radiotherapy , cancer institute , tokyo , japan , 5 department of therapeutic radiology and oncology , kyoto university graduate school of medicine , kyoto , japan , 6 department of radiology , tokyo womens medical college , tokyo , japan , 7 department of radiotherapy , national cancer institute , tokyo , japan . received : february 21 , 2002 ; accepted : october 25 , 2002 strahlenther onkol 2003 no . 
computer software increases the accuracy of data entry in the pcs introduction constant efforts are being made in the medical field to improve the quality of clinical data generation , data analysis , and data communication . 
in this study , the effectiveness of the logical checking function using the database of patterns of care study ( pcs ) in japan was quantitatively and prospectively evaluated . patients and methods in 1996 , we introduced pcs in order to establish clinical quality assurance of radiotherapy in japan , courtesy of the american college of radiology in the united states . 
as for lung cancer , an original database was developed according to the general rules for the clinical and pathologic recording of lung cancer established by the japan lung cancer society [ 11 ]  . 
ten young radiation oncologists participated in the audits after 1 - day training in the use of a computer for data entry and construction of an internet mailing list of all the members mailing addresses for the purpose of sharing any problems encountered on site during the pcs audit and real - time solutions . as a result of this training , accurate and uniform data entry was achieved . 
the data of 1 , 584 patients were accumulated in the pcs database from september 1998 to march 1999 . by using a computer , the number of erroneous data was dramatically reduced compared with that entered into the conventional case report form ( crf )  . 
the total numbers of patients checked for breast cancer , esophagus cancer , cervix cancer , and lung cancer during the two periods were 856 , 609 , 773 , and 774 , respectively . 
these include a variety of data such as eligibility criteria for pcs , demographics , symptoms , history , staging work - up , staging , pathology , treatment course , treatment information on external beam , brachytherapy , surgery and chemotherapy , outcome , relapse patterns , and complications . 
there are 316 items ( 57 for numerical items , 224 for text , and 35 for dates ) per patient for the breast cancer format , 329 ( 77 , 214 , and 38 , respectively ) for esophageal cancer , 463 ( 78 , 346 , and 39 , respectively ) for uterine cervix cancer , and 389 ( 86 , 264 , and 39 , respectively ) for lung cancer . 
beispiel von dokumentationskriterien in der japanischen pcs - datenbank fr lungenkrebs . main category in number the data format survey items in the category of survey items in each category type of items of surgery eligibility criteria demographics symptom history staging work - up staging pathology treatment course 33 external beam brachytherapy surgery chemotherapy outcome relapse pattern complication others text surgery performed date date of surgery text extent of surgery plastic surgery text combined resection , specify text residual tumor text surgical findings ( jlsg95a ) text extent of surgery with lymph text node dissection ( jlsg95a ) surgical t / n stage ( uicc97b ) text text stage pathologic findings text ( jlsg95a ) maximum diameter of tumor number pathologic t / n stage ( uicc97b ) site # of pathologic metastatic nodes ( jlsg95a ) pathologic stage curability text text text text ageneral rule for clinical and pathological record of lung cancer , 4th edn . 
computer software increases the accuracy of data entry in the pcs breast cancer , 282 for esophageal cancer , 340 for cervix cancer , and 394 for lung cancer ( total 1 , 428 )  . 
 since the total number of data for one disease site during both periods exceeded 100 , 000 , erroneous data were retrieved with an original retrieval system using the hypercard ( apple computer , inc . , cupertino , ca , usa )  . 
the function of this program was to import all the accumulated data into the system and to produce a frequency distribution of the data for each survey itethe erroneous data could thus be easily retrieved . 
the numbers of erroneous data were compared for these two periods captured with and without application of the logical checking function to the database . the statistical significance was determined by means of the ( cid : 1 ) 2 - test . 
 results number of accumulated data the total number of data ( total number of patients times data items ) without application of the logical checking function was 596 , 186 and that for application of the function 533 , 656 ( table 2 )  . 
in the database without application of the logical checking function , total numerical items numbered 116 , 941 , text items 419 , 572 , and dates 59 , 673 , and the corresponding numbers for application of the function were 105 , 602 , 374 , 292 , and 53 , 762 . 
the japan lung cancer study group , 1995 [ 11 ]  . define data type define range define data format selection number date text lower limit < _ < _ upper limit japanese yy / mm / dd western mm / dd / yy date item figure 2 . 
second , the format of the dates was changed from the japanese yy / mm / dd format to mm / dd / yy , as used in the western countries , in order to make future international comparisons of pcs between japan and the united states possible . table 2 shows the numbers of patients and total data accumulated in our pcs database for the four disease sites . 
the numbers of patients entered in the database without the logical checking function were 444 for breast cancer , 327 for esophageal cancer , 433 for cervix cancer , and 380 for lung cancer ( total 1 , 584 )  . 
the corresponding numbers of patients for the database with the logical checking function were 412 for table 3 shows the reduction in erroneous data by disease site for the two survey periods with and without application of the logical checking function to the japanese pcs database . 
the percentage of erroneous data was thus significantly reduced , compared to data captured with the conventional crf as a result of using a database with a computer and a logical checking function ( figure 3 )  . 
without the logical checking function , the number of erroneous data for numerical items was 1 , 563 out of 116 , 941 ( 1.34% ) , and strahlenther onkol 2003 no . 
 patterns of erroneous data in japanese pcs database table 4 shows the patterns of erroneous data for the two survey periods with and without application of the logical checking function for the japanese pcs database . 
also , incorrect data that had been inputted in text form such as facilities names instead of their id numbers was also reduced to 0 . as for dates , the generation of the specific date format in japan was reduced to 0 as a result of the logical checking function . 
the generation of erroneous data that were out of the range was also reduced to 0 as well as the numerical data . discussion the scientific accuracy of clinical research is an ethical obligation [ 2 ]  . 
the purpose of clinical studies is to improve the quality of treatment for the patient . currently , the data of prospective clinical studies are collected mostly by means of conventional crf . 
as far as we know , no prospective technical evaluation of the use of a computerized database with this logical checking function installed has been reported for actual clinical studies . the logical checking function uses three steps . 
third , data are selected from among the survey items according to category in order to eliminate potential errors in data entry in textual forfor numbers and dates , the number of erroneous data in the japanese pcs database number date type of data figure 4 . 
rckgang fehlerhafter daten in abhngigkeit vom datentyp fr zwei dokumentationsperioden mit und ohne anwendung von logischen kontrollfunktionen in der japanischen pcs - datenbank . was significantly reduced by use of the logical checking function . 
as for textual items , there were no errors , because all survey items were categorized from the beginning . our literature survey found no detailed analyses of patterns of errors in crf . 
die muster fehlerhafter daten in zwei dokumentationsperioden mit und ohne anwendung von logischen kontrollfunktionen in der japanischen pcs - datenbank . type of data type of wrong data periods september 1998 to april 1999 to march 1999 ( without logical checking function ) september 1999 ( with logical checking function ) numerical date including text out of range miss typing wrong format subtotal out of range wrong format miss typing subtotal total 1 , 109 1 , 563 1 , 174 1 , 249 2 , 812 strahlenther onkol 2003 no . 
computer software increases the accuracy of data entry in the pcs roneous data by using the logical checking function which sets number as a data type and thus eliminates errors in the analysis . 
in the case of data outside the range ( e.g. , by misclassifying a unit or simple typing mistakes such as gy for cgy ) , they can be analyzed without apparent errors shown by the computer so that the result is incorrect . 
 although the number of erroneous data could be significantly reduced by using the logical checking function for the pcs database , it may be difficult to reduce the incidence of errors to 0 . 
though it may be possible to reduce erroneous data by making the logical checking function more intense , it may also disturb the fair entry of extreme data that are beyond the normal range . for a future possibilities of the pcs database , new functions using the currently accumulated data need to be considered . 
this involves a new checking system of data entry with a range using mean values and their standard deviations of the survey items in the pcs data accumulated to date . 
the technical evaluation in this process will also be required . our study provides definite evidence that the logical checking function of computer software has significantly increased the accuracy of data entry of external audit results in the pcs in japan . 
the importance of these findings is that such technology will reduce the labor involved in data management and improve the accuracy not only of pcs but also of most prospective clinical studies that are currently being conducted . 
hanks , md , chairman and professor of department of radiation oncology , fox chase cancer center and principal investigator of patterns of care study in the united states , and jean b . 
owen , phd , director of patterns of care study , american college of radiology , philadelphia , pa , usa , for their great support and appropriate advice on performing audits for pcs in japan . strahlentherapie und onkologie original article effects of serum starvation on radiosensitivity , proliferation and apoptosis in four human tumor cell lines with different p53 status natsuo oya , friedo zlzer , frank werner , christian streffer1 purpose : the effects of serum starvation on radiation sensitivity , cell proliferation and apoptosis were investigated with particular consideration of the p53 status . 
 material and methods : four human tumor cell lines , be11 ( melanoma , p53 wild - type ) , mewo ( melanoma , p53 mutant ) , 4197 ( squamous cell carcinoma , p53 wild - type ) and 4451 ( squamous cell carcinoma , p53 mutant ) , were used . 
after the cells had been incubated in starvation medium ( 0.5% fcs ) for 16 days , changes in cell cycle distribution , induction of apoptosis and necrosis , and changes in radiation sensitivity were assessed by two - parameter flow cytometric measurements of dna content / brdu labeling , two - parameter flow cytometric measurements of dna - dye - exclusion / annexin v binding , and a conventional colony assay , respectively . 
 results : p53 wild - type cell lines showed a decrease in the brdu labeling index and an increase in the apoptotic cell frequency in starvation mediup53 mutant cell lines showed a decrease in the brdu labeling index but no evidence of apoptosis . 
the radiation sensitivity was increased in 4451 and slightly decreased in be11 and 4197 in starvation mediu conclusion : these data suggest a functional involvement of p53 in starvation - induced g1 - block and apoptosis in tumor cells . 
 key words : serum starvation cell cycle distribution radiosensitivity apoptosis annexin v assay p53 strahlenther onkol 2003 ; 179 : 99106 doi 10.1007 / s00066 - 003 - 0973 - 8 wirkung eines serummangelmediums auf die strahlenempfindlichkeit , proliferation und apoptose von vier menschlichen tumorzelllinien mit unterschiedlichem p53 - status ziel : die wirkungen eines serummangelmediums auf die zellulre strahlenempfindlichkeit , proliferation und apoptose wurden unter besonderer bercksichtigung des p53 - status untersucht . 
 material und methodik : vier menschliche tumorzelllinien , be11 ( melanom , p53 - wildtyp ) , mewo ( melanom , p53 - mutante ) , 4197 ( plattenepithelkarzinom , p53 - wildtyp ) und 4451 ( plattenepithelkarzinom , p53 - mutante ) , wurden verwendet . 
nach inkubation der zellen ( 16 tage ) in einem serummangelmedium ( 0 , 5% fks ) wurden vernderungen der proliferation , der apoptose und des auftretens von nekrosen bei den zellen sowie vernderungen der strahlenempfindlichkeit mit dem durchflusszytometer ( dnabrdu , dna - annexin v ) und dem koloniebildungstest untersucht . 
 schlsselwrter : serummangel zellproliferation strahlenempfindlichkeit apoptose annexin - v - assay p53 1 institute for medical radiation biology , university hospital essen , germany . recieved : december 3 , 2001 ; accepted : august 2 , 2002 strahlenther onkol 2003 no . 
recently , chronic hypoxia has gained particular attention , since its effects on tumor cell proliferation must be discussed separately from the classic effects of short - term hypoxia as a cause of radiation resistance [ 1 , 5 , 12 , 16 , 19 ]  . 
chronic starvation and acidosis also seem to be important factors , which may determine proliferation , metabolism , and the response of tumor cells to various treatments . the effects of serum starvation on cells have been discussed with respect to repair of radiation damage [ 8 ] , cell cycle arrest [ 7 , 26 , 28 , 32 ] , and apoptosis [ 2 , 3 , 6 , 9 , 13 ]  . 
in particular , apoptosis has been widely studied after serum starvation , suggesting that serum starvation is one of the major stimulants of apoptosis , and that certain molecular mechanisms , including expression of insulin - like growth factor binding protein ( igfbp ) , myc and p53 , might be involved in the modulation of starvation - induced apoptosis [ 2 , 4 , 6 , 9 , 13 ]  . many previous studies have suggested that p53 is involved in the cellular response to starvation . 
in the present study , using four human tumor cell lines , the effects of starvation on radiation sensitivity , cell proliferation and apoptosis were systematically investigated with particular consideration of the p53 status . 
 materials and methods cell lines , culture conditions , and irradiation all experiments were carried out with four human cell lines , be11 , mewo , 4197 , and 4451 . 
be11 and 4197 were classified as p53 wild - type , while a mutation in the p53 gene was found in exon 7 of mewo and 4451 [ 28 ]  . 
 two different media , normal medium and starvation medium , were used in the present study , both of which were modified from minimal essential medium without nahco3 ( mem , biochrom kg )  . 
3060 min after irradiation with 28 gy , the cells were trypsinized , counted , and plated into petri dishes with 5 ml of fresh normal mediucolonies were fixed 9 , 1314 , 89 , and 14 days after plating for be11 , mewo , 4197 and 4451 , respectively [ 31 ]  . 
 proliferation assay with brdu two - parameter measurements of dna content / brdu labeling using a facscan flow cytometer ( becton - dickinson ) were performed to assess the time course of cell proliferation in starvation medium without irradiation . 
the procedure of immunofluorescence staining consisted of isolation of nuclei by pepsin , partial dna denaturation by 2 n hcl , incubation with anti - brdu mouse igg ( becton - dickinson , 1 : 100 ) , incubation with fitc - conjugated goat anti - mouse igg ( sigma , 1 : 200 ) , and dna stain with propidium iodide ( pi )  . 
about 5 , 000 nuclei from each sample were measured and displayed in a green ( fitc ) versus red ( pi ) scattergram , on which the appropriate windows for g1 - , g2 - , brdu - labeled sand unlabeled s - phase cells were set to determine the percentage of each fraction . 
annexin v binds to phosphatidylserine ( ps ) , which locates only on the inner side of the cell membrane in normal vital cells , and will be exposed at the outer layer in the early stage of apoptosis [ 20 , 21 ]  . 
thus , apoptotic cells and necrotic cells were determined as annexin v - fitc ( + ) pi ( ) cells and annexin v - fitc ( + ) pi ( + ) cells , respectively . 
 the experiments with annexin v were carried out using annexin v - fitc apoptosis detection kit ( calbiochem ) according to the attached protocol of the providing company with slight modification . 
the cells were washed with pbs ( ) , trypsinized , centrifuged , and resuspended in binding buffer ( 10 mm hepes , 150 mm nacl , 2.5 mm cacl2 , 1 mm mgcl2 , 4% bsa )  . 
the cells were then incubated with fitc - labeled annexin v ( 0.5 g / ml , 15 min in the dark at room temperature ) and stained with pi . about 5 , 000 cells from each sample were measured and disstrahlenther onkol 2003 no . 
2 urban & vogel played in a red ( pi ) versus green ( fitc ) scattergram , on which the fractions of vital cells , apoptotic cells , and necrotic cells were determined [ 20 , 21 ]  . 
be11 and mewo cells on glass slides after 5 - day culture in starvation medium were also microscopically examined for apoptotic processes with annexin v - fitc / pi double staining , h - e staining , and dapi staining . approximately 500 cells per slide were scored under microscopy , and the frequency of the cells with nuclear condensation and / or nuclear fragmentation in h - e and dapi staining was compared with the annexin v - fitc ( + ) pi ( ) fraction determined in fcma . 
 statistics comparisons of means ( n = 34 for colony assay and n = 46 for proliferation assay and apoptosis assay ) were performed by using the students t - test with or without welchs correction depending on the variances of the data sets , using statview 5.0 , unless stated otherwise . 
after 3 - day culture in starvation medium , the radiation sensitivity was increased in 4451 cells , unchanged in mewo , and slightly but significantly decreased in be11 and 4197 cells . 
5 - day culture in starvation medium had similar effects . proliferation assay examples of the scattergram of flow cytometry with fitc - labeled brdu and pi are shown in figures 4a and 4b . 
 figures 5a and 5b illustrate the time course of the brdu labeling index and the percentage of quiescent s - phase cells . generally , the brdu labeling index ( percentage of brdu - positive cells ) decreased with time of culture in starvation mediuthe labeling index decreased quickly in 4197 ( p53 wildtype ) and slowly in the other cell lines , corresponding to the changes in the number of harvested cells . 
wachstumskurven fr be11 - , mewo - , 4197und 4451zellen in mangelmediu die balken entsprechen der standardabweichung aus mindesten vier unabhngigen experimenten . priming culture 3 - day starvation 5 - day starvation be11 mewo 4197 4451 figure 2 . 
koloniebildungsvermgen von be11 - , mewo - , 4197und 4451 - zellen nach 3und nach 5 - tgiger kultur in mangelmediudie angaben der standardabweichung basieren jeweils auf mindesten drei unabhngigen experimenten . 
proliferation and apoptosis after starvation be11 and mewo 4197 and 4451 be11 priming culture mewo priming culture be11 3 - day starvation mewo 3 - day starvation be11 5 - day starvation mewo 5 - day starvation 4197 priming culture 4451 priming culture 4197 3 - day starvation 4451 3 - day starvation 4197 5 - day starvation 4451 5 - day starvation and 4b . 
the control level of apoptosis was significantly lower in be11 and 4197 than in mewo and 4451 . when cultured in starvation medium , the apoptotic cell frequency in be11 increased dramatically from 5% on day 3 to 40% on day 4 , not being associated with an increase in the necrotic cell frequency . 
statistically significant differences ( p < 0.05 ) between the survival fractions after starvation and those of the respective priming cultures were observed in be11 , 4197 , and 4451 both after 3and 5 - day culture in starvation medium , at least at one dose level . 
statistisch signifikante unterschiede ( p < 0 , 05 ) zwischen den berlebensraten nach mangelkultur und den entsprechenden ausgangskulturen wurden bei be11 - , 4197und 4451 - zellen sowohl nach 3als auch nach 5 - tgiger kultur in mangelmedium unter mindestens einer strahlendosis beobachtet . 
die unterschiede zwischen den kurven wurden auch anhand der auc - werte der einzelnen experimenten analysiert ; es ergaben sich fr be11 - , 4197und 4451 - zellen nach 3und nach 5 - tgiger kultur in mangelmedium im vergleich zu den entsprechenden ausgangskulturen signifikant unterschiedliche berlebenskurven . 
 an increase in the number of brdu - unlabeled cells with an s - phase dna content ( quiescent s - phase cells [ 30 , 31 ] ) associated with a decrease in brdu labeling index was generally observed . 
however , a marked accumulation of quiescent sphase cells , as high as 20% , was observed only in 4197 on day 5 in starvation mediu apoptosis assay examples of the scattergram of flow cytometry in the fcma with fitc - labeled annexin v and pi are shown in figures 4a in order to confirm the data on the induction of apoptosis measured by flow cytometry , be11 and mewo cells were also studied for appearance of apoptotic cells under the microscope . 
 the be11 cells stained with h - e after 5 days of starvation showed cytoplasmic collapse to various degrees , while the nuclear condensation or fragmentation was seen only in severely collapsed cytoplasma ( figure 7b )  . 
however , the microscopic examination with annexin v demonstrated that even mildly collapsed cells were annexin v - positive ( figure 7c )  . thus , it is suggested that the changes at the cell membrane ( ps translocation ) precede the morphologic changes in the nuclestrahlenther onkol 2003 no . 
proliferation and apoptosis after starvation figure 4a abbildung 4a well accepted that p53 participates in the control of a cell cycle checkpoint before the cells enter s - phase [ 24 ]  . 
previous studies in our laboratory using the same cell lines as in the present study showed that entry into s - phase can be delayed only in the p53 wild - type cell lines , when the cells were irradiated in a quiescent state after 6 - day culture in starvation medium [ 28 ]  . 
another study demonstrated an increased fraction of quiescent s - phase cells in p53 mutant cell lines after irradiation and / or hyperthermia [ 29 , 30 ]  . the present data show that p53 also plays an important role in cell cycle progression during starvation , as well as for the modification of radiosensitivity . a more rapid decrease in the brdu labeling index ( a decrease in the number of active s - phase cells ) was observed in the p53 wild - type cell lines . 
examples of scattergram of flow cytometry with fitc - labeled brdu ( a ) and propidium iodide ( pi ) ( b ) for cell proliferation assay and with annexin v - fitc and pi for apoptosis assay , representing be11 after 4 - day culture in starvation mediu abbildungen 4a und 4b . 
 discussion since extreme physiologic conditions can persist for weeks or months in human tumors in vivo , it is essential to know not only the effects of the temporal ( acute ) physiologic conditions at the time of irradiation , but also the effects of the long - term ( chronic ) starvation , in order to draw necessary consequences for tumor therapy . 
it is although there is no obvious explanation for the mechanisms of the induction of quiescent s - phase cells , it is conceivable that they have entered s - phase , starting dna synthesis , and thereafter have lost the ability to continue dna synthesis . 
in the examined four cell lines , the decrease in brdu labeling index during starvation appeared to be associated with both the accumulation of quiescent s - phase cells and that of the g0 / g1phase cells . 
however , the ratio of the g0 / g1 - phase to quiescent s - phase was larger for the p53 wild - type cell lines ( 4.7 for be11 and 4.7 for 4197 ) than that for the p53 mutant cell lines ( 3.1 for mewo and 2.9 for 4451 ) on day 6 in starvation medium , suggesting that the starvation - induced g1 - block capacity may also depend on the p53 status . 
considering that simultaneous expression of myc and p53 often triggers apoptosis [ 22 , 25 , 27 ] , it is strongly suggested that starvation - induced apoptosis occurs in a p53 - dependent manner . 
however , the discrepancy in the extent of starvation - induced apoptosis observed between 4197 ( 10% on day 6 ) and be11 ( 40% on day 4 ) was large , although both cell lines had wild - type p53 . 
therefore , the possible involvement of p53 - independent phenomena must be considered . time after exchange of medium ( days ) time after exchange of medium ( days ) figure 5a abbildung 5a figure 5b abbildung 5b figures 5a and 5b . 
zeitlicher verlauf des brdu - markierungsindex ( a ) und des prozentualen anteils von s0 - zellen ( b ) in mangelmediudie balken entsprechen der standardabweichung aus mindestens vier unabhngigen experimenten . 
 * p < 0 , 05 , p < 0 , 01 verglichen mit den entsprechenden ausgangskulturen ( tag 0 )  . be11 mewo 4197 4451 be11 mewo 4197 4451 be11 mewo 4197 4451 be11 mewo 4197 4451 time after exchange of medium ( days ) time after exchange of medium ( days ) figure 6a abbildung 6a figure 6b abbildung 6b figures 6a and 6b . 
time course of the frequency of apoptotic cells in the annexin v - fitc ( + ) pi ( ) fraction ( a ) and the frequency of necrotic cells in the annexin v - fitc ( + ) pi ( + ) fraction ( b ) in starvation mediuerror bars represent s.e. 
zeitlicher verlauf der hufigkeit apoptotischer zellen in der annexin - v - fitc ( + ) - pi ( ) - fraktion ( a ) und der hufigkeit nekrotischer zellen in der annexin - v - fitc ( + ) - pi ( + ) - fraktion ( b ) in mangelmediudie balken entsprechen der standardabweichung aus mindestens vier unabhngigen experimenten . 
proliferation and apoptosis after starvation creased radiation sensitivity observed in be11 and 4197 after 3and 5 - day culture in starvation medium could be explained by the prolonged g1 - block , considering the evidence that be11 and 4197 cells irradiated in serum starvation - induced g1 - block showed a remarkable delay in progression into s - phase , when their growth was stimulated with fresh medium [ 28 ]  . 
further , it has been reported that chinese hamster v79 cells cultured in 40% growth medium are more radioresistant than in 100% growth medium without any changes in cell cycle distribution [ 17 ]  . 
under such conditions , the changed degree of spread in monolayer and the consequently changed chromatin conformation were found to affect the kinetics of the dna doublestrand break repair [ 10 ]  . 
this mechanism may also partly account for the increased radioresistance observed in our p53 wild - type cell lines in starvation mediu the increased radiation sensitivity observed in 4451 after 3and 5 - day culture in starvation medium could be explained neither by the accumulation of quiescent s - phase cells nor by apoptosis . one consideration might be that the capacity of the dna damage repair differs in starvation medium as compared to normal conditions . 
it is also possible that p53 mutant cells tend to bear less g1block in starvation medium , go quicker into s - phase , achieve faster redistribution in the cell cycle , and therefore show higher radiosensitivity than p53 wild - type cells . 
it has been widely accepted that the major role of wild - type p53 is the control of the cell cycle checkpoints and induction of apoptosis , and that its mutation results in the loss of these functions . 
the lack of apoptosis in these cells apparently enables them to exist longer under conditions of starvation . however , not all of the present data could be explained by the p53 status . 
recently , the compromised functions of wild - type p53 in tumor cells [ 14 ] and the variation of mutant p53 functioning like wild - type p53 in tumor cells [ 18 ] have been reported . 
long arrows , arrow heads , and short arrows represent the annexin v + / pi cells with mildly collapsed cytoplasma , annexin v + / pi cells with severely collapsed cytoplasma , and annexin v + / pi + cells with severely collapsed cytoplasma and with nuclear condensation / fragmentation , respectively . 
lange pfeile , pfeilspitzen und kurze pfeile weisen auf annexin - v ( + ) / pi ( ) - zellen mit geringfgig geschdigtem zytoplasma , auf annexin - v ( + ) / pi ( ) - zellen mit schwer geschdigtem zytoplasma und auf annexin - v ( + ) / pi ( + ) - zellen mit schwer geschdigtem zytoplasma und zellkernkondensation bzw . 
 comparison of the results in annexin v assay with those in brdu assay indicated that the extent of the decrease in the brdu labeling index was not correlated to that of apoptosis . only 10% of 4197 cells became apoptotic in spite of a drastic decrease in the brdu labeling index , while about 50% of be11 became apoptotic in spite of a moderate decrease in the brdu labeling index , suggesting that the two possible roles of p53 , to arrest cell cycle and to promote apoptosis , can be uncoupled by other factors [ 11 , 22 ]  . with respect to the effects of serum starvation on radiation sensitivity , it is unlikely that apoptosis plays a major role in the determination of radiation sensitivity , because the preceding starvation or acidosis had no significant influence on radiation - induced apoptosis ( data not shown )  . 
the apoptotic frequency as high as 50% observed in be11 after 5 - day culture in starvation medium was not reflected in the radiation sensitivity of the clonogenic cells , but in the reduced plating efficiency . 
proliferation and apoptosis after starvation tions of p53 function , as well as p53 - independent procedures , are involved in the response of the tumor cells to starvation . acknowledgment this study was supported by alexander von humboldt foundation ( scholarships to natsuo oya )  . 
als weitere potentielle prognostische faktoren wurden , neben der hmoglobinkonzentration ( hb ) , tumorlokalisation ( kopf / korpus ) , geschlecht ( weiblich / mnnlich ) , lymphknotenstatus ( cn0 / cn1 ) , dosierung der externen strahlentherapie ( 50 , 4 gy / 59 , 4 gy ) , ikterus bei diagnosestellung ( ja / nein ) , gewichtsverlust bei diagnosestellung ( 5 kg / < 5 kg ) , epigastrisch - lumbaler schmerz bei diagnosestellung ( ja / nein ) , maximaler tumordurchmesser ( < 40 mm / 40 mm ) gepr ergebnisse : die hmoglobinkonzentration vor therapiebeginn lag zwischen 9 , 6 and 15 , 0 g / dl . 
bei der multivariaten analyse erwies sich die hmoglobinkonzentration zum diagnosezeitpunkt als der einzige prognostische faktor , der mit dem metastasenfreien berleben ( p = 0 , 026 ) , dem krankheitsfreien berleben ( p = 0 , 032 ) und dem gesamtberleben ( p = 0 , 048 ) korrelierte . 
 schlussfolgerungen : in einer patientengruppe , die wegen lokal fortgeschrittener pankreaskarzinome radiochemotherapie erhielt , wurde eine signifikante korrelation zwischen dem hmoglobinspiegel vor therapiebeginn und metastasenfreiem berleben , krankheitsfreiem berleben und gesamtberleben beobachtet . 
in particular , hemoglobin ( hb ) concentration affects the outcome of patients with neoplasms of the uterine cervix , head and neck and bladder tumors [ 5 , 6 , 15 , 17 , 19 , 23 , 24 ]  . 
 in particular , a number of publications confirmed the impact of anemia on local disease control in patients undergoing radiation therapy [ 5 , 15 , 17 , 19 , 23 , 24 ]  . 
recently , koong et al have observed that pancreatic tumors show a high degree of hypoxia at intraoperative measurements of tumor oxygenation using the eppendorf polarographic electrode [ 8 ]  . 
therefore , it can be hypothesized that the dismal prognosis of patients with pancreatic carcinoma , and particularly the poor response rate after radiation or concomitant chemoradiation is , at least in part , due to tumor cell hypoxia . furthermore , considering the correlation between anemia and degree of tumor hypoxia [ 13 ] , it can be hypothesized that also in pancreatic tumors , anemia can worsen the degree of tumor hypoxia . 
 however , to the best of our knowledge , in the literature there are no analyses on the correlation between anemia and pattern of failures in patients with tumors of the exocrine pancreas treated with radiotherapy . 
 the aim of this study was to evaluate , in a population of patients with locally advanced pancreatic carcinoma undergoing concomitant chemoradiation , the impact of pretreatment hb concentration on prognosis . 
using as cut - off the median value observed in the study population , the differences in the following endpoints were evaluated : local control , metastasis - free survival , disease - free survival , and overall survival . 
 patients and methods patients were enrolled in the study in a period when the same protocol of concomitant chemotherapy was used , even if the radiation dose was progressively increased . 
 chemoradiation was used only in patients with unresectable ( ct4 ) disease , while patients with resectable ( ct13 ) carcinoma were treated with surgery plus intraand postoperative radiotherapy [ 14 ]  . 
criteria on which concomitant chemoradiation was based , were the following : patients with unresectable pancreatic carcinoma limited to the locoregional area with no evidence of liver or distant metastases ( ct4 n01 m0 ) , age < 75 years , eastern cooperative oncology group ( ecog ) performance score 02 , granulocyte count > 4 , 000 / mm3 , platelet count > 100 , 000 / mm3 , hb concentration > 9 g / dl . 
the patients histories were examined , and physical examination , ecg , complete blood count ( cbc ) , blood chemistry , tumor biopsy , chest x - ray , and abdominal ct were performed . 
pretreatment hb level was calculated from cbc evaluation performed 3 days before radiotherapy . external beam radiation was delivered with 9 mv photons using the three - field technique ( one anterior and two opposed lateral fields )  . 
the clinical target volume ( ctv ) was designed to adequately cover the tumor volume ( with at least a 2 - cm margin ) and primary lymphatic drainage ( hilar , hepatic artery , celiac , peripancreatic , superior mesenteric and paraaortic nodes at the level of d12l2 body )  . 
 in patients treated with higher doses ( 59.4 gy ) , 50.4 gy were delivered to the previously described ctv , and 9 gy to the macroscopic tumor ( plus 2 - cm margin ) only . 
 results in four patients ( 13.3% ) treatment was interrupted before delivery of the prescribed dose due to grade 3 hematologic toxicity ( one patient ) , grade 3 gastrointestinal toxicity ( one patient ) , and cholangitis ( two patients )  . 
patients with an hb or > the median value ( 11.5 g / dl ) were compared to detect differences in terms of potential prognostic factors ( table 2 )  . 
no significant differences in terms of sex , age , clinical n - stage , tumor site , symptoms at diagnosis , maximum tumor diameter , and radiation dose were observed . 
 p - value overall , 19 patients ( 63.3% ) had distant metastases ( 14 hepatic , two pulmonary , two hepatic and peritoneal , and one pulmonary and peritoneal )  . 
metastasis - free survival was 5.1 months in patients with an hb 11.5 g / dl and 10.7 months in those with an hb > 11.5 g / dl ( p = 0.010 ; figure 1 )  . 
einfluss des hmoglobin - ( hb - ) wertes auf das metastasenfreie berleben ( p = 0 , 010 ) : das metastasenfreie berleben zeigt die gestrichelte kurve fr patienten mit einem hb > 11 , 5 g / dl , die durchgezogene kurve fr patienten mit einem hb 11 , 5 g / dl . 
first , chemoradiation was based on a short - course concurrent chemotherapy ; to date , low - dose prolonged infusions are more frequently used due to lower associated toxicity . 
however , it should be noted that , as for the incidence of metastases , disease - free and overall survival , the small sample size did not hinder the significant impact of hb on these factors . 
it should be kept in mind that the inclusion criteria for patient treatment were based on an ecog score of 02 and an initial hb value of > 9 g / dl . 
consequently , the absence of an impact of performance status on the outcome might depend on the exclusion of patients with worse clinical conditions ( ecog 34 )  . as for the exclusion of patients with an hb 9 g / dl , this implies that the results of our study can only be extended to the population of nonanemic or moderately anemic patients . these limitations should be considered in relation to the biological significance of our study even if they are not clinically relevant since , usually , patients with severe anemia or in poor general condition , in common clinical practice , are excluded from combined chemoradiation treatments . in our study , there were no statistical differences in terms of response or actuarial local control . 
this is in contrast to results obtained in a number of studies conducted on patients with head and neck [ 5 , 19 , 24 ] , uterine cervix [ 6 , 15 , 23 ] and bladder tumors [ 17 ] where significant differences were observed in terms of response and local control . 
 the reasons for these differences could be found in the different histologic type analyzed in our experience ; in fact , in most studies patients were affected by squamous cell carcinoma [ 5 , 6 , 19 , 20 , 23 , 24 ] , with the single exception of bladder tumors [ 17 ] ; the small sample we analyzed where the number of patients with partial response ( 4 / 30 ) and local progression ( 2 / 30 ) was limited ; strahlenther onkol 2003 no . 
according to their conclusions these results suggest that the amount of hypoxia within a tumor represents the most important stimulus for upregulation of angiogenesis and that anemia acts as a cofactor via worsening of tumor tissue oxygenation [ 4 ]  . 
the correlation between tumor angiogenesis and metastasizing potential , particularly in pancreatic carcinoma , seems to be confirmed by a recent japanese study . seo et al [ 21 ] have evaluated the surgical specimens of 142 resected pancreatic carcinomas to analyze vegf expression and microvessel density ( mvd )  . 
 based on these observations , it is desirable that other analyses of this type are carried out to verify that our results are not anecdotal ; prospective assessments on vegf behavior in anemic patients , not affected by pancreatic carcinoma , with monitoring of the incidence of distant metastases are carried out . these studies should confirm the hypothesis that anemia is able to stimulate angiogenesis through a higher vegf concentration [ 3 ] and that angiogenesis is able to favor the development of metastases in these patients . 
 if the impact of anemia in patients with pancreatic carcinoma is confirmed by other studies , clinical trials to assess whether early correction of anemia would have an impact on outcome , would be justified . 
considering the extremely high rate of metastases in anemic patients ( 100% at 1 year ) , a therapeutic approach with anemic patients treated with a systemic ( chemotherapy ) rather than a locoregional therapy ( surgery plus radiotherapy ) could be evaluated . 
 finally , based on the proven efficacy of recombinant erythropoietin ( repo ) in the correction of anemia in neoplastic patients [ 9 , 22 ] , a strategy could be tested where , as first therapy , 23 cycles of chemotherapy combined with repo are administered to anemic patients with pancreatic carcinoma . 
 als supraspinatussehnensyndrom werden degenerative vernderungen am chondral - apophysren ansatz der supraspinatussehne ( ssp ) verstanden , die durch eine enge zwischen tuberculum majus humeri und ligamentum coracoacromiale verursacht werden ( abbildung 1 )  . 
das outlet - impingement wird durch anatomische strukturen , die den subakromialraum von kranial einengen , verursacht , wie formanomalien des akromions ( typ ii und iii nach bigliani & morrison ) , verdickung und tendopathie des ligamentum coracoacromiale und kaudale osteophyten am akromioklavikulargelenk ( ac - gelenksarthrosen )  . 
das non - outlet - impingement entsteht dagegen durch eine tendinosis calcarea , durch bursitiden , eine instabilitt der rotatorenmanschette , ein prominentens tuberculum oder eine ac - dislokation [ 5 ]  . 
dabei zeigte sich , dass die strahlentherapie beim outlet - impingement ( hypertrostrahlenther onkol 2003 ; 179 : 12930 doi 10.1007 / s00066 - 003 - 9905 - x phie des ac - gelenks ) , bei einer chronischen tendinitis der supraspinatussehne und bei einem gelenkerguss erfolglos blieb . 
bei einer kompletten ruptur der ssp - sehne , einer akuten tendinitis der ssp - sehne zeigte die bestrahlung hingegen gute ergebnisse ( non - outlet - impingement )  . 
in einer an unserem hause erst krzlich abgeschlossenen , unverffentlichten untersuchung an 84 bestrahlten schultergelenken konnten wir bei einer tendinosis calcarea der ssp - sehne , einer bursitis subdeltoidea und bei einer partiellen ruptur der sspsehne ein sehr gutes ansprechen der strahlentherapie verzeichnen : in 80% der flle konnte eine vllige schmerzfreiheit erzielt werden . 
doch gab schon von pannewitz [ 5 ] 1933 die empfehlung , bei degenerativen gelenkerkrankungen eine einzeldosis von 0 , 30 , 4 gy gelenkumschlieend zu applizieren und die fraktionierung an die schmerzanamnesedauer anzupassen . 
die autoren htten vielmehr darauf aufmerksam machen mssen , dass die strahlentherapie beim non - outlet - impingement sehr wohl erfolgreich sein kann ( schmerzfreiheit in 80% der flle ) und dem patienten nicht als letzte therapieoption nach durchprobieren aller mglichen behandlungsanstze vorenthalten werden darf . 
 wenn orthopden , chirurgen , radiologen und strahlentherapeuten in zukunft im rahmen von studien zusammenarbeiten wollen , muss eine eindeutige diagnose verlangt werden , um die untersuchte therapiemodalitt auch zielgerichtet einsetzen zu knnen . 
dabei wurde eine fraktionierung von 3 - mal 0 , 5 gy mit 3 ( cid : 1 ) 1 , 0 gy ( 2 - mal / woche , zwei serien mit einer behandlungspause von 6 wochen ) verglichen . 
2 urban & vogel strahlentherapie und onkologie technical note hyperfractionated 192ir brachytherapy for recurrent retroperitoneal sarcoma : a technique for delivery of local tumor boost dose johannes classen1 , thomas hehr1 , ulf lamprecht1 , andreas zumbrgel2 , michael bamberg1 , wilfried budach1 background : radical surgery is the treatment of first choice for retroperitoneal sarcoma . 
yet , there is evidence that adjuvant irradiation does improve local tumor control . material and methods : in order to deliver sufficiently high radiation doses to the retroperitoneum , different techniques for application of a local tumor boost dose in addition to external beam treatment have been proposed . 
 results : hfir of the tumor bed was easily accomplished facilitating delivery of high radiation doses to the retroperitoneuno major late effects of treatment have been observed with a follow - up of 15 and 28 months , respectively . 
thus , sufficiently high doses of radiation mandatory for long - lasting local tumor control can be delivered in the tumor bed of the retroperitoneum without exceeding normal tissue radiotolerance in this unfavorable disease . 
 key words : retroperitoneal sarcoma brachytherapy hyperfractionation radiotherapy strahlenther onkol 2003 ; 179 : 11822 doi 10.1007 / s00066 - 003 - 0998 - z hyperfraktionierte 192ir - brachytherapie bei rezidivierenden retroperitonealen sarkomen : eine technik fr die boost - bestrahlung hintergrund : die radikale resektion ist die therapie der wahl bei der behandlung retroperitonealer sarkome ( rps )  . 
bei zwei patientinnen mit rezidiven eines rps wurde nach ct - basierter bildgesttzter bestrahlungsplanung eine hyperfraktionierte 192ir - brachytherapie mit 2 ( cid : 1 ) 1 , 52 , 0 gy pro tag in 510 mm gewebetiefe bis zu einer gesamtdosis von 18 bzw . 
32 , 5 gy durchgefhrt . ergebnisse : die vorgestellte brachytherapietechnik erwies sich als einfach durchfhrbar und ermglichte die applikation hoher strahlendosen im retroperitoneuchronische nebenwirkungen traten bei einer nachbeobachtungszeit von 15 bzw . 
daten der literatur zur bestrahlung von rps werden diskutiert . schlussfolgerung : die hyperfraktionierte 192ir - brachytherapie des retroperitoneums ist eine problemlos durchfhrbare technik , mit deren hilfe eine dosisaufsttigung im tumorbett bei einem gnstigen nebenwirkungsspektrum erreicht werden kann . 
 schlsselwrter : retroperitoneale sarkome brachytherapie hyperfraktionierung strahlentherapie 1 department of radiation oncology , and 2 department of urology , tbingen , germany . received : january 30 , 2002 ; accepted : november 14 , 2002 strahlenther onkol 2003 no . 
retroperitoneal sarcoma introduction soft tissue sarcoma has a low incidence of 23 / 100 , 000 with primary retroperitoneal location accounting for only 1015% of all cases , thus representing approximately 240 new cases in germany every year . 
the prognosis of retroperitoneal sarcoma is dismal with a 5 - year survival rate of 2060% [ 1012 ]  . while distant metastasis is the main cause of tumor - related death in extremity sarcoma , local failure is the primary pattern of relapse in retroperitoneal sarcoma in up to 90% of relapsing patients [ 10 ] ultimately leading to death by local complications of uncontrolled tumor progression [ 12 , 15 ]  . 
 local resection is the primary treatment of retroperitoneal sarcoma , and complete surgical resection has been demonstrated to be an independent favorable prognostic factor for disease - specific and disease - free survival apart from tumor grading ( g1 / 2 ) [ 11 , 15 , 16 , 22 ] , tumor size ( < 10 cm ) , and histology ( liposarcoma ) [ 15 ]  . 
even though it is widely accepted that sarcomas are , in fact , radiosensitive , the role of radiotherapy in primary retroperitoneal sarcoma has , to date , only poorly been defined due to a lack of randomized clinical series . 
hence , percutaneous megavolt treatment is limited in the total radiation dose that can safely be delivered to the target volume without the risk of major acute or late complications . 
3 months prior to admission , a right - sided retroperitoneal liposarcoma had been resected with histology disclosing tumor - positive margins . therefore , on readmission recurrent sarcoma was suspected . following preoperative staging including detailed imaging studies ( figure 1 ) , the patient was relaparatomized and gross tumor resection was performed including right - sided nephrectomy once the diagnosis of recurrent liposarcoma had been confirmed on frozen section pathology . 
careful attention was paid to parallel positioning of the catheters in the tumor bed at a distance of approximately 10 mm avoiding sharp edging or bending of the catheters as well as close proximity to large vessels and nerves . 
the data set of the ct was then transferred to the brachytherapy planning system ( abacus 2.0 ) , the catheters were individually identified , and image - guided brachytherapy planning was performed . 
in order to compensate for this treatment interruption , brachytherapy was continued with an increased reference dose of 2.0 gy for eight fractions once symptoms had resolved under conservative treatment and antibiotics . 
 discussion retroperitoneal sarcoma has an unfavorable prognosis due to a high rate of local recurrences after primary resection ultimately leading to death by uncontrolled primary tumor growth in many patients . 
radical surgical resection is the mainstay of treatment , and patients with histologically complete tumor resection have a significantly improved prognosis over those with microscopically or macroscopically involved margins [ 11 , 15 , 22 ]  . 
the role of radiotherapy in retroperitoneal sarcoma , however , remains controversial . retrospective analysis of small patient series indicates that radiotherapy may , in fact , improve local tumor control . 
heslin et al [ 10 ] demonstrated an improved local tumor control of 38% vs 59% ( p = 0.02 ) in favor of adjuvant radiotherapy compared to surgery alone in a population of 48 patients . 
furthermore , a dose - response relationship for improved local tumor control rates with increasing radiation doses has been demonstrated in two small series : fein et al [ 5 ] observed a relapse rate of 38% for doses < 52.2 gy as compared to 25% for higher doses . 
 with total doses > 60 gy , however , optimal treatment planning is a challenge to the radiation oncologist due to doselimiting normal tissue tolerance of , e.g. , small bowel , liver , or kidneys . 
dosisverteilung der interstitiellen brachytherapie im retroperitoneuisodosen von auen nach innen : 1 , 0 / 1 , 5 / 2 , 0 gy . prescribed at 5 mm depth to the target volume which was determined from the ct scan , surgical clip marks , and intraoperatively specified regions of risk at relapse ( figure 3 )  . 
at day 12 following surgery allowing for initial wound healing , hyperfractionated 192ir brachytherapy was initiated inserting bronchial catheters ( 1.84 mm diameter , 1 , 300 mm length , onesided closed end , provided by former isotopentechnik dr . sauerwein , now varian medical systems haan gmbh ) into the guiding tubes and connecting the catheters to the multichannel brachytherapy machine ( gammamed 12i afterloader )  . 
a total dose of 18 gy was applied followed by 3 - d - planned treatment with 15 mv photons of 45 gy ( 5 ( cid : 1 ) 1.8 gy / week ) resulting in a cumulative dose of 63 gy to the tumor bed . 
this catheter was then removed early , and replanning with the remaining catheters was performed . treatment was well tolerated except for mild nausea grade 2 ( ctc ) and diarrhea grade 1 during the additional course of external beam radiotherapy ( ebrt )  . 
 case 2 in april 1999 , a 56 - year - old female patient was admitted to tbingen university hospital for a suspected recurrent rightsided retroperitoneal sarcoma 18 months after primary resection in a peripheral hospital . 
hyperfractionation will then deliver small single radiation doses of 1.5 gy twice daily , thus ensuring a sufficiently high dose in the tumor bed for potential improvement of tumor control at a low risk of late complications of radiotherapy . 
furthermore , overall treatment time of brachytherapy is shortened by hyperfractionation not only increasing the dose delivered per time but also reducing the risk of potential complications caused by interstitial catheter positioning . apreoperative radiotherapy bmedian dose in eight patients treated with additional ebrt cebrt in 13 patients debrt in 16 patients best - known strategy for local dose escalation is intraoperative electron beam radiotherapy ( iort ) with single doses in the range of 1020 gy followed by additional ebrt ( table 1 )  . reported tumor control rates of combined iort and ebrt compare favorably to patients treated exclusively with ebrt . the only randomized trial available for radiotherapy of retroperitoneal sarcoma comparing 5055 gy ebrt with 20 gy iort followed by 3540 gy ebrt showed a local failure rate of 40% versus 80% ( p < 0.05 ) in favor of iort while tumor - specific survival was unaffected [ 21 ]  . 
therefore , intraoperative high dose - rate brachytherapy has been proposed , and encouraging results with an acceptable profile of treatment - related toxicity have been reported [ 1 ]  . 
however , iort is limited in dose independent of the choice of beam quality by the inherent problem that irradiation has to be applied by one single - fraction high - dose treatment bearing the risk of increased late complications of radiotherapy if normal tissue tolerance is not adequately taken into account . 
this technique bears several potential advantages over single - dose iort : intraoperative positioning and fixation of the plastic catheters by sutures are easy and quick to accomplish , and no premanufactured templates need to be adapted for placement in the tumor bed . 
furthermore , wound healing is not impaired by brachytherapy since onset of irradiation can brachytherapy via intraoperatively implanted plastic tubes or 3 - d - planned brachytherapy techniques have been reported previously for a variety of tumor histologies and tumor locations [ 3 , 68 , 14 , 17 , 19 ]  . 
the number of patients treated for retroperitoneal sarcoma , however , was very small in any series , and techniques varied with respect to fractionation , type of implants , or the use of templates . 
displacement of intraoperatively placed catheters is an inherent problem in the technique proposed and should be avoidable by scrupulous intraoperative placement and fixation of the catheters as well as careful postoperative handling of catheter material and wound molding . 
 conclusion hyperfractionated brachytherapy facilitates the delivery of high radiation doses in patients with retroperitoneal sarcoma and may be used alone or for delivery of local tumor boost irradiation in these patients . 
 strahlentherapie und onkologie case report epidural metastasis in nasopharyngeal carcinoma athanasios bagatzounis1 , eleni erakleous2 , ioannis michaelides3 background : in nasopharyngeal carcinoma , both , a short metastasis - free interval after primary treatment and the occurrence of epidural metastasis have been associated with poor prognosis . 
we present the clinical course of a young patient with these two conditions and review the literature . patient : a 26 - year - old male with stage t2n3m0 non - keratinizing carcinoma ( who type 2 ) of the nasopharynx was treated with induction chemotherapy and radical radiotherapy . 
since no further metastatic lesions were detectable , the patient was treated with radiotherapy alone ( 3 960 cgy / 22 fractions )  . results : treatment resulted in complete resolution of neurological and radiological signs of the disease and the patient continues to be disease - free , 32 months after salvage treatment . 
 key words : epidural metastasis nasopharyngeal cancer radiotherapy mr imaging strahlenther onkol 2003 ; 179 : 1238 doi 10.1007 / s00066 - 003 - 0972 - 9 epidurale metastase beim nasopharynxkarzinoein fallbericht hintergrund : epidurale metastasen und kurzes metastasenfreies intervall nach primrtherapie von patienten mit nasopharynxkarzinom sind assoziiert mit einer schlechten prognose . 
wir prsentieren den klinischen verlauf bei einem patienten mit diesen zwei bedingungen und geben eine literaturbersicht zu dieser thematik . patient : ein 26 - jhriger patient mit einem nicht keratinisierenden ( who typ 2 ) t2n3m0 - nasopharynxkarzinom wurde mit neoadjuvanter chemotherapie und anschlieender definitiver radiotherapie behandelt . 
6 monate nach dokumentation einer kompletten klinischen remission entwickelte der patient eine vertebrale metastase in hhe c7th1 , die von einem epiduralen weichteiltumor begleitet wurde ( abbildungen 1a bis 1c )  . 
bei auftreten einer solitren epiduralen metastase nach kurzem metastasenfreien intervall nach primrtherapie eines nasopharynxkarzinoms kann ein langzeitberleben erreicht werden . schlsselwrter : epidurale metastasen nasopharynxkarzinom radiotherapie magnetresonanztomographie 1 clinic for radiation oncology , bank of cyprus oncology center , 2 medical diagnostic center ayios therissos , 3 institute for pathology , nicosia general hospital , nicosia , cyprus . 
epidural metastasis in nasopharyngeal carcinoma introduction nasopharyngeal carcinoma occurs commonly in southwest asia and the mediterranean basin [ 31 ] and is , as molecular studies suggest , a clonal expansion of ebv - infected cells [ 22 , 24 ]  . in mediterranean countries , patients under the age of 30 years comprise 1421% of the affected population [ 5 , 21 ] and nearly all of the tumors are from the non - keratinizing ( who type 2 ) or the undifferentiated histological subtype ( who type 3 ) [ 21 ]  . 
 nasopharyngeal carcinoma has been reported to have a higher incidence of distant metastases as compared to other head and neck cancers , with bone metastasis being the most common [ 1 , 11 , 27 ]  . 
 there are a few case reports in the literature dealing with epidural metastasis from nasopharyngeal carcinoma [ 9 , 16 ]  . this condition is usually associated with advanced disease , and patients experience poor outcomes . 
 we present the favorable clinical course of a patient with vertebral metastases and an epidural soft tissue mass diagnosed 6 months after the completion of the initial treatment and salvaged by radiation therapy . 
an excisional biopsy revealed a lymph node metastasis from a non - keratinizing carcinoma ( ck8 + , hmb45 - , lca - , ck20 - , ebv + , ck34b12 + , ck7 - , chromograninand nse - )  . 
 the patient underwent one course of induction chemotherapy , containing cisplatinum 50 mg / m2 iv on days 1 and 2 , folinic acid 350 mg iv over 2 hours , 5 - fluorouracil 400 mg / m2 iv bolus , followed by 5 - fluorouracil 400 mg / m2 iv over 22 hours . the large node mass responded dramatically fast to induction chemotherapy . 
the nasopharynx and the upper neck above the c4 / 5 interspace were treated by means of two individually shaped lateral portals with 6 mv photons and a total dose of 5 , 000 cgy within 5 weeks . 
after a dose of 4 , 000 cgy the fields were reduced to exclude the spinal cord . the primary tumor received a boost of 2 , 400 cgy by means of a three - field technique ( one anterior field and two lateral wedge fields ) over 2 / 2 weeks . 
the residual right jugulo - digastric nodal mass was boosted with a 4 ( cid : 1 ) 4 cm , 12 mev electron beam and a dose of 1 , 000 cgy in five fractions . 
the lower neck lymphatics received a total dose of 5 , 000 cgy over a period of 5 weeks through an anterior portal and protection of the midline structures with a lead block . 
 4 months after the end of therapy the patient complained of a pain in the lower neck - region , radiating to the left arm . this symptom was interpreted as a side effect from treatment and was no further investigated . 
the symptoms disappeared and repeated mri and bone scan examinations at 3 , 12 and 28 months post - treatment showed a complete tumor resolution ( figures 2a and 2b )  . 
newer , less examined predictive factors are tumor angiogenesis , c - erbb2 expression [ 26 ] , the presence of ebstein - barr virus dna in the peripheral blood cells [ 17 ] and chromosomal loss at 3p14p21 [ 7 ]  . 
 despite higher tumor burden at initial presentation , patients with non - keratinizing carcinomas ( who type 2 ) and undifferentiated carcinomas ( who type 3 ) experience better outcomes than patients with squamous cell carcinoma ( who type 1 ) [ 29 ]  . 
t1 - weighted sagittal plane shows bony lesions with low signal intensity involving the bodies of c7 and d1 ( large arrows ) without any evidence of collapse fracture , associated with an anterior epidural soft tissue mass at the level of d1 ( small arrow )  . 
the high signal intensity changes from c1 to c4 vertebrae represent fatty bone marrow replacement and are due to the previous irradiation of the primary tumor and its proximal lymphatics . 
die t1 - gewichtete sagittalaufnahme zeigt knochenlsionen niedriger signalintensitt in den wirbelkrpern c7 und th1 ( dicke pfeile ) , die mit einem ventralen epiduralen weichteiltumor in hhe th1 assoziiert sind ( dnner pfeil )  . 
die hyperintensen vernderungen , die in den wirbelkrpern c1c4 zu sehen sind , entsprechen fettiger degeneration des knochenmarks nach vorausgegangener bestrahlung des primrtumors und seines proximalen lymphabflusses . findings of arguello et al [ 3 ] , epidural metastatic disease arise from cancer cells located within the vertebral marrow which invade into the spinal canal through the foramina of the vertebral veins . 
they form a tumor mass at the same location from which the cells emerged from the vertebra , and compress the cord predominantly anteriorly . our patient developed pain in the lower neck radiating to his left arm 4 months after completion of the initial treatment . 
although we did not obtain a biopsy from these lesions , their appearance on mri and the short interval of their occurrence after the initial treatment of the nasopharyngeal carcinoma , make the association with this carcinoma very likely . the short metastasis - free interval after achievement of a clinical complete response with sequential chemoradiotherapy indicates that this lesion may have existed at the time of the primary diagnosis . 
the accuracy of bone scintigraphy in the diagnosis of bone metastases in asymptomatic patients with newly diagnosed carcinoma of the nasopharynx is very low , so that its routine use has been questioned [ 15 , 28 ]  . 
in our patient , bone scintigraphy was not performed at initial staging . kostakoglu et al [ 12 ] reported from a patient with undifferentiated stage iv ( t3n3m0 ) nasopharyngeal carcinoma ( who type iii ) who underwent pre and 1 month post therapy bone scintigraphy as part of an ongoing trial combining scintigraphic and radiographic modalities . 
t1 - weighted after iv gadolinium administration sagittal ( b ) and axial ( c ) planes at the level of d1 demonstrate diffuse enhancement of the dural lesion ( large arrow ) which appears to involve the anterior epidural spaces bilaterally ( arrows ) , extending laterally into the intervertebral foramina ( if ) of d1 to d2 , to the epidural veins ( batsons plexus ) ( e ) and to the area around the basivertebral vein ( b )  . 
die t1 - gewichteten aufnahmen nach gadoliniumgabe sagittal ( b ) und axial ( c ) in hhe von th1 zeigen ein diffuses enhancement der epiduralen lsion ( dicker pfeil ) , die in die beiden vorderen epiduralen rume ( pfeile ) einwchst , sich nach lateral in die intervertebralforamina ( if ) von th1 bis th2 ausdehnt , die epiduralen venen ( batsons plexus ) ( e ) und die region um die vena vertebrobasilaris infiltriert ( b )  . 
among these , seven had metastatic disease confined in the bones and received either radiation therapy alone ( three patients ) or consolidative radiation therapy after systemic chemotherapy ( four patients )  . 
their series provided the largest series of long - term survivors ( > 36 months ) from metastatic carcinoma of the nasopharynx and included 20 patients with a median age of 28 years . 
an additional case report on a patient with continuous disease - free survival 16 years after the initial treatment , 8 years after radiotherapy for locoregional recurrence and 20 months after removal of a solitary lung metastasis has been reported by nozaki et al [ 20 ]  . papavasiliou et al [ 21 ] reported on two patients who experienced long - term survival after treatment for metastatic disease to the mediastinu once there is evidence of metastatic disease to the vertebrae , it is important to assess its extent using mri scanning that has been proven to be more sensitive than bone scintigraphy [ 19 ]  . 
in some cases , as in our patient , soft tissue extensions in the epidural space can spread in longitudifigure 2a abbildung 2a figure 2b abbildung 2b figures 2a and 2b . 
 despite excellent response of the locoregional disease to a short induction chemotherapy and achievement of a longlasting locoregional control with the subsequent radiotherapy , our patient experienced an early distant metastasis . 
more intensive systemic therapy , as used by al - sarraf et al [ 2 ] , in the randomized intergroup study 0099 ( cisplatin 100 mg / m2 on days 1 , 22 and 43 during radiotherapy and three courses with cisplatin 80 mg / m2 on day 1 and fluorouracil 1000 mg / m2 / d on days 14 administered every 4 weeks ) , reduced the frequency of all relapses from 61% in the radiotherapy arm to 23% in the combined modality ar the reduction was more pronounced for bony metastases ( from 22% to 4% ) than for lung ( from 13% to 6% ) or liver metastases ( from 7% to 4% )  . 
the reason was the previous irradiation of the spinal cord above the level of c4 , as the fatty degeneration of the vertebral bodies on mr imaging suggests ( see figure 1a )  . 
 strahlentherapie und onkologie original article the impact of gross tumor volume ( gtv ) and clinical target volume ( ctv ) definition on the total accuracy in radiotherapy theoretical aspects and practical experiences elisabeth weiss , clemens f . 
hess1 aim : to evaluate the impact of interobserver variability in the contouring of gross tumor volumes ( gtvs ) and clinical target volumes ( ctvs ) on the global geometric accuracy in radiation therapy . 
causes are multifactorial and include imageand observer - related factors , such as the subjective interpretation of image information . conclusion : consequences to reduce interobserver variability are proposed , among others the selection of adequate imaging modalities , intensified radiologic training , and the use of telecommunication tools . 
 key words : interobserver variability setup error organ motion geometric precision radiotherapy strahlenther onkol 2003 ; 179 : 2130 doi 10.1007 / s00066 - 003 - 0976 - 5 die bedeutung der definition von tumorvolumen und klinischem zielvolumen auf die geometrische przision der strahlentherapie . 
theoretische aspekte und praktische erfahrungen ziel : analyse der bedeutung der untersucher - variabilitt bei der zielvolumendefinition fr die przision der strahlenbehandlung . material und methodik : anhand einer literaturbersicht wird die grenordnung der untersucher - variabilitt dargestellt , ursachen und konsequenzen werden diskutiert . 
die untersucher - variabilitt wird mit anderen ursachen geometrischer ungenauigkeiten verglichen , insbesondere der lagerungsungenauigkeit und der organbewegung . ergebnisse : die untersucher - variabilitt ist ein bedeutender , fr einige tumorlokalisationen vielleicht der grte faktor , der die geometrische przision beeinflusst . 
die auswahl geeigneter bildgebung , gezieltes radiologisches training und der einsatz moderner telekommunikationsmethoden . schlsselwrter : untersucher - variabilitt lagerungsungenauigkeit organbeweglichkeit geometrische przision strahlentherapie 1 department of radiation therapy , university of gttingen , germany . received : december 3 , 2001 ; accepted : august 2 , 2002 strahlenther onkol 2003 no . 
research in this field has concentrated on geometric misfits related to patient positioning [ 10 ] and organ motion , such as breathing or changing filling status of bladder and bowel [ 19 ]  . the knowledge of both types of uncertainties is required to define the safety margin of the planning target volume ( ptv ) according to the icru 50 and 62 recommendations [ 8 , 11 , 12 ]  . numerous studies addressing spatial accuracy have been performed . 
they are all based on the assumption that the fundamental step in treatment planning the definition of gross tumor volume ( gtv ) and clinical target volume ( ctv ) has been performed adequately . 
in particular , if based on a 3 - d slice - by - slice delineation , the definition of gtv or ctv has been assumed to be correct without question . 
only in the recent years , analyses of the variability of target volume definitions in the form of interobserver studies have been published . inadequate definition of the gtv or ctv leads to a systematic geometric miss of the tumor in the individual patient during the whole course of radiation therapy . 
the resulting underdosage of the same parts of the target volume during each fraction will significantly impair the probability of tumor control . the uncertainty of gtv and ctv definition caused by interobserver variability has had little impact on treatment planning until now . 
for some tumor locations , inconsistencies in target volume definition may dominate all other errors in radiation therapy planning and delivery . it is the aim of this article to review the literature on interobserver variabilities in the definition of gtvs and ctvs . causes for the observed uncertainties will be presented and discussed . 
finally , suggestions will be made , how to reduce the variability in target volume definition . methodological differences and a large diversity of approaches to the problem hamper a homogeneous analysis of studies on interobserver variability and allow comparisons with other errors only in a limited scope . 
the primary intention of this article is therefore to present a synopsis and to increase awareness of uncertainties caused by observer variability . material and methods definition of gtv and ctv in contrast to the ptv , which includes margins for geometric variations , in particular an internal and a setup margin , both gtv and ctv are purely oncologic volume concepts . 
the ctv includes regions of subclinical tumor spread adjacent to the gtv and other locations of suspected tumor manifestations , e.g. , lymph nodes [ 11 , 12 ]  . 
in general , all observers were provided with an identical set of instructions , clinical information on the patient including tumor stage , and relevant images of the tumor region . 
the latter eliminates the error of incorrect outline transmission from the ct hard copy to the treatment planning syste to guarantee independence of results , observers were not allowed to see the volumes delineated by other observers . 
ptv variability is , however , not under discussion in this review . there are a number of articles comparing interobserver variability in dependence on the used imaging technique ( ct and / or mri ) or the application of contrast mediuwhereas all cited studies analyzed variations between different observers , some also evaluated intraobserver differences . 
 first , a comparison of absolute distances between delineated contours and magnitudes of inserted volumes is performed , which is most frequently based on the calculation of means and the range of variations around the means , or by comparison of maximum and minimum volumes . 
interobserver variability in the gtv and ctv definition second , volumes are related to each other with the intention to calculate a common volume , i.e. , a volume on which all observers agree , and an encompassing volume , i.e. , the smallest volume that includes all observers volumes . 
further , by defining geometric or gravity centers of the respective volumes , 3 - d vectors have been calculated to represent differences in the position of the volumes relative to each other . 
in one study the intraclass coefficient ( icc ) was used as a measure of correlation between multiple observers with a value of 1.0 corresponding to absolute correlation and an icc > 0.7 defining excellent agreement [ 38 ]  . 
logue et al [ 21 ] calculated variations in isocenter positions as the distances between the respective isocenters from the gold standard isocenter , which was defined by the radiologists . 
some authors found a particularly high variation in the craniocaudal extension of the volumes [ 4 , 33 ]  . the variation of delineated prostate volumes in axial ct scans was highest at the top and bottom of the prostate [ 5 ]  . 
 in general , interindividual variations in the outlined volumes by an average factor of 1.32 have to be considered even for well - circumscribed carcinomas such as prostate carcinomas and cerebral tumors . 
 it should be added that similar to the definition of gtv and ctv , there has been a ct - based interobserver study on the delineation of critical organs in patients with prostate cancer . 
for some tumor locations it has been claimed that the degree of interobserver variability in volume definition is in the order of the magnitude of differences in volume definition seen between imaging modalities [ 37 ]  . 
in all analyses target volumes derived from cts were compared to mriderived volumes concerning both the size of volumes and other imaging - related changes in interobserver variability . mri has been claimed necessary for the target volume definition of many tumors in radiation therapy planning for its good strahlenther onkol 2003 no . 
 organ author patients observers ( n ) contoured volume radiologic basis results size of volumes relation of volumes prostate cazzaniga et al 3 dubois et al [ 4 ] 41 6 ros p + sv + margin ct , urethrogram 1 ro , 1 radiol . 
icc : intraclass coefficient ; ro : strahlentherapeut . factor magnitude quantitative volumect = 0.9 ( cid : 1 ) volumemri ( + ct ) ( brain , base of the skull ) , no improved consistency in volume definition with mri volumect ( + mri ) = 1.31.4 ( cid : 1 ) volumemri ( prostate , head and neck ) , probably improved consistency with mri ratio common / encompassing volume improved by approx . 
ct volumes differed largely from mri volumes at the apex , the base of the seminal vesicles , and the posterior prostate confinement [ 26 , 29 ]  . several reports have dealt with the correct identification of the prostatic apex in particular . 
in a study by milosevic et al [ 22 ] , two radiation oncologists and one diagnostic radiologist independently identified prostatic apices on ct , mri , and urethrogra interobserver agreement was significantly improved with mri compared to ct and urethrograthe localization of the apex was superior with mri relative to ct and urethrograsimilar results were found by debois et al [ 3 ]  . 
 although the final pathologic proof is missing , it appears that mri not only reduces interand intraobserver variability in the definition of the target volumes but also leads to a probably true identification of the real anatomic prostate volume due to improved visibility of the organs boundaries . 
similar to the prostate , for the head and neck region , rasch et al [ 28 ] found that mean ct - derived volumes were by a factor of 1.3 larger than mri - derived volumes . interobserver variability was smaller with mri than ct . 
the authors have concluded that ct and mri are complimentary methods : although soft tissue structures are generally better identified on mri , the recognition of the craniocaudal extension of the target volume was superior on ct scans . 
ten haken et al [ 37 ] found that tumor volumes defined on mri were larger than volumes derived from ct and had a greater share of composite volumes derived from ct and mri information together . 
the authors come to the same conclusions : it is unclear which imaging modality best describes tumor extensions in the braboth ct and mri input should be considered for treatment planning of brain tumors . 
there are seven publications where not only radiation oncologists outlined the target volumes , but other specialists with clinical and radiologic experience of the respective type of tumor [ 4 , 6 , 20 , 21 , 27 , 40 , 45 ]  . 
in both studies radiologists drew smaller volumes than radiation oncologists due to a precise , anatomic way of contouring with individualized management of lymph nodes and tumor [ 6 , 40 ]  . 
in summary , radiation oncologists tend to delineate larger volumes than physicians from other specialities maybe because of the unconscious integration of other geometric uncertainties relevant in radiotherapy , maybe because of the wish to really encompass the complete tumor with all uncertainties in the localization of microscopic disease , maybe because of limited radiologic knowledge . 
analyses revealed that individuals drew varying outlines at different points of time . fiorino et al [ 5 ] found an average 5% variation in the size of the contoured volumes when the same physician repeated contouring directly after the first drawing of the volume . 
in general , one would expect the contouring of visible , well - delineated tumors such as prostate and brain tumors to result in less variation than the definition of adjuvant regions and areas of microscopic disease . 
a comparison of all studies dealing with prostate carcinomas revealed that as far as it was mentioned in the articles all observers had the same task : to insert the prostate seminal vesicles [ 5 , 26 , 28 , 33 , 38 ]  . 
notably , improved protocols were found to reduce intraobserver variation in the ctv delineation of the breast [ 9 ]  . comparison of the variability in gtv and ctv definition with other uncertainties that influence geometric precision a direct comparison of uncertainties caused by positioning , organ motion and target volume delineation is not possible due to the different ways to analyze and present uncertainties . still , to get an idea of the magnitude of the principal factors contributing to the geometric uncertainty of target volume coverage , in the following the different uncertainties will be presented together for prostate and brain tumors . 
these two tumor entities differ with respect to the extent of organ motion ( small for brain ) , positioning accuracy ( high for brain ) and variabilities in target volume delineation ( in some studies good agreement particularly of volume size for prostate )  . 
 the depicted volumes have the following magnitudes : 479 cm3 gtv1 570 cm3 gtv2 gtv1 / gtv2 = ctv1 / ctv2 = 0.73 common / encompassing encompassing encompassing gtv = 0.62 concerning the size of volumes , with increasing 3 - d expansion of the original gtvs their relative difference is reduced . 
fr die ptvs wurde zu den ctvs ein 0.5 cm groer saum addiert . die abgebildeten volumina haben die folgenden gren : 82 cm3 gtv1 113 cm3 gtv2 gtv1 / gtv2 = 0 , 73 schnittmenge / vereinigungsschnittmenge / vereinigungsschnittmenge / vereinigungsmenge = 0 , 62 mit zunehmender expansion der ursprnglich eingezeichneten volumina relativiert sich ihr unterschied sowohl hinsichtlich der volumengre als auch hinsichtlich der relativen lage zueinander ( schnittmenge / vereinigungsmenge )  . 479 cm3 ctv1 570 cm3 ctv2 ctv1 / ctv2 = 0 , 84 657 cm3 ptv1 767 cm3 ptv2 ptv1 / ptv2 = 0 , 86 menge = 0 , 80 menge = 0 , 78 the errors from setup and organ motion were calculated according to stroom et al [ 35 ] based on the errors published by hurkmans et al [ 10 ] and langen & jones [ 19 ]  . 
since errors from positioning and organ movement are usually given in centimeters , for reasons of comparability the radii of the delineated target volumes are presented , although target volumes seldom resemble closely a spherical shape . 
this means that interobserver variations play an even more important role in tumors of the head and neck , lung , and esophagus . in general , for tumors with only small differences in the size of delineated volumes and good agreement on the location of gtvs and ctvs , e.g. , prostate tumors , it seems that the errors from patient positioning and organ movement are larger than errors from gtv definition [ 28 ]  . 
in patients with a high interobserver variability both in volume size and volume location , the uncertainty from contouring exceeds the errors caused by patient positioning and organ motion [ 45 ]  . discussion from the magnitude of recorded uncertainties it appears that for many tumor locations , variabilities in target volume delineation might have a greater impact on the accuracy of dose delivery than errors in treatment setup and organ motion [ 10 , 19 , 43 ]  . 
according to jones et al [ 13 ] , each target volume represents the clinicians individual approach and is therefore , by definition , error - free as long as patients are not enrolled in a clinical trial . 
 in our view , intraand interobserver variations add to the overall uncertainty in treatment planning and delivery and should therefore be considered among other factors such as positioning uncertainty and organ motion . 
from the observers view , there is both a systematic error , since it could be shown that single observers draw either always large or always small volumes , but also a random component represented particularly by intraobserver variations [ 24 ]  . 
 the addition of margins to the already existing safety margins for ptv delineation would result in an enlargement of target volumes , an increase in irradiated volumes , and a higher percentage of toxicities . 
after all , all dose - effect curves based on clinical studies include more or less unknowingly inconsistencies in target volume definition ! in our view , the primary aim should therefore be first , the systematic evaluation of causes responsible for uncertainties in the identification of target volumes and second , their maximum reduction . 
the reduction in the variability of target volume definition will finally have to result in a reevaluation of dose - effect curves with potentially lower doses necessary for the same clinical endpoint . we therefore make the following suggestions to reduce uncertainties in gtv and ctv definition in clinical practice : instructions . 
for a consistent contouring of gtvs and ctvs , among others the assessment of edema and contrast enhancement , and the specification of the size of lymph nodes that should be judged as pathologic have to be part of instructions for target volume delineation . 
selection of adequate imaging techniques , good quality of all images used for treatment planning , and exploitation of all available technical means for image registration and multimodality imaging [ 1 , 23 , 30 , 32 ] are vital for increased accuracy in target volume definition . 
in the times of conformal 3 - d treatment planning , training in diagnostic radiology and a close liaison with other specialists , particularly diagnostic radiologists and surgeons , are essential . 
 after evaluation and discussion of various parameters influencing target volume definition , it has to be noted that it remains still largely unclear what in fact defines the ideal gtv strahlenther onkol 2003 no . 
however , precise instructions , radiologic training and modern techniques of imaging and image processing are able to reduce differences in target volume definition whatever the true target volume looks like . 
 conclusion in summary , interobserver variability in the definition of gtv and ctv is a major for some tumor locations probably the largest factor contributing to the global uncertainty in radiation treatment planning . 
 strahlentherapie und onkologie original article multivariate analysis of prognostic factors in patients with glioblastoma johannes lutterbach1 , willi sauerbrei2 , roland guttenberger1 background : to identify prognostic factors for overall survival in patients with newly diagnosed glioblastoma undergoing radiation therapy . 
mean age of the 415 patients who were included in the study was 59 years ( 1981 years ) , karnofsky performance status ( kps ) was 70 in 280 patients . 
 key words : glioblastoma radiotherapy multivariate analysis prognosis hemoglobin ldh strahlenther onkol 2003 ; 179 : 815 doi 10.1007 / s00066 - 003 - 1004 - 5 multivariate analyse prognostischer faktoren bei patienten mit glioblastom hintergrund : die vorliegende studie untersucht prognosefaktoren fr das gesamtberleben bei patienten , die aufgrund eines neu diagnostizierten glioblastoms bestrahlt wurden . patienten und methodik : von januar 1980 bis juni 2000 wurden 432 glioblastompatienten an unserer klinik behandelt . 
prognostic factors in patients with glioblastoma introduction in prospective clinical trials , median survival times of around 9 months and 2 - year survival of < 10% were reported for patients with glioblastoma . 
 various models have been proposed to separate patients with high - grade gliomas into groups of varying prognosis . based on data derived from 1 , 578 patients who had been treated in studies of the radiation therapy oncology group ( rtog ) , curran et al [ 9 ] developed a set of classes from a recursive partitioning model . 
this study confirmed the importance of younger age , good performance status , history of seizures , and complete surgical resection of the tumor as all being independent favorable prognostic variables . 
 however , these models can be criticized for their inclusion of both anaplastic astrocytoma and glioblastoma resulting in a histologically heterogeneous population and , moreover , for taking into account not only pretreatment but also treatment - related factors such as extent of resection or total dose . 
for radiation oncologists , the latter aspect is especially problematic in clinical practice as the extent of resection is often difficult to determine and the total dose is , of course , not known prior to the beginning of radiation therapy . 
 patients and methods it was the consistent policy at our department to indicate radiation therapy in all patients with histologically confirmed glioblastoma except for those with a kps 40 or an organic cerebral psychosyndrome . 
17 patients who underwent radiation therapy were excluded from the analysis : two patients were < 18 years , ten had adjuvant chemotherapy , and five were treated with fractionation schemes other than those described below . this resulted in a nearly unselected population of 415 patients who underwent primary or postoperative radiation therapy between january 1980 and june 2000 . 
hemoglobin ( hb ) and serum lactate dehydrogenase ( ldh ) levels were determined on admission for neurosurgery ( normal range hb 13.018.0 g / dl in males ; 12.016.0 g / dl in females ; ldh 80240 u / l ) and known in 318 and 234 patients , respectively . 
tumor size , defined as the maximal diameter of the contrast - enhancing lesion in transverse ct / t1 - weighted mri sections , was 4.0 cm in 126 patients and > 4.0 cm in 111 patients , respectively . 
 the radiation schedule for patients who had a biopsy consisted of a daily dose of 2.0 gray ( gy ) given five times a week up to a planned total dose of 60 gy . 
besides modified fractionation schemes , postoperative patients were also offered standard treatment with 30 fractions of 2 gy ( n = 40 )  . 17 patients reached the planned total dose . 293 patients completed their treatment within the prescribed treatment time . 
therefore , the first fractions were given as whole brain radiotherapy resulting in a short interval between surgery and the beginning of radiation therapy ( median 14 days )  . 
at 20 gy ( conventional fractionation ) , 21 gy ( hypofractionation ) , or 31.5 gy ( accelerated hyperfractionation ) , the planning target volume was shrunk to the contrastenhancing lesion as shown on ct scans or mri with a 3 - cm margin [ 1 ]  . 
the variables from the resulting model ( table 3 ) were used as adjustment factors to investigate the prognostic value of three further variables in the corresponding subgroups with available data . 
because of the small sample size , patients with 0 and 1 point , respectively , and 3 and 4 points , respectively , were combined . results survival no patient was lost to follow - up . 
the strata were defined based on objectively assessable variables only . as has been shown previously , the neurosurgeons intraoperative impression and postoperative mri findings frequently differ with regard to the extent of resection [ 15 ]  . 
 in the patients in whom tumor diameter ( n = 237 ) , pretreatment hb level ( n = 318 ) or pretreatment ldh level ( n = 234 ) were known , the effects of these variables were investigated in models adjusting for the three significant characteristics age , kps , and central tumor location . 
 based on the results of the multivariate analysis , we developed a simple score by attaching points to the categories of the three significant variables resulting in score values from 0 to 4 ( table 3 )  . 
the underlying idea was to develop a prognostic model which might be helpful to optimize patient selection for different treatment approaches and to identify variables for risk - adapted treatment studies . 
randomized clinical trials have always more or less restrictive selection criteria and , in general , patients are entered from several centers . multivariate analysis of variables known in all patients identified older age , low performance status , and central tumor location as risk factors . 
due to missing values , the influence of hb , serum ldh levels , and tumor diameter was investigated in subgroups of 318 patients , 234 patients , and 237 patients , respectively . 
the report of the medical research council brain tumour working party divided patients into three age groups of < 45 years , 4559 years , and > 59 years [ 34 ]  . 
in the trial , the mrc prognostic index was derived from [ 34 ] ; patients with a who performance status of 01 had a median survival of 10 months compared with 5.5 months in patients with a who performance status of 34 . 
however , in a population - based survey including 1 , 417 patients with primary brain tumors the largest subgroup suffered from glioblastoma , liigant et al [ 19 ] found that median survival of patients with frontal , parietal , and temporal tumors was 18 months , 15 months , and 14 months , respectively , compared with only 7 months in patients in whom deep structures of the central nervous system were affected . 
 hemoglobin low hb levels have been shown to negatively influence local control and survival in a variety of neoplasms , e.g. , carcinomas of the uterine cervix [ 25 ] , bladder [ 26 ] , or head and neck [ 10 ]  . to our knowledge , the impact of anemia on prognosis has not yet been investigated in patients with glioblastomas . 
they found no survival difference in 72 children who were treated for medulloblastoma , irrespective of whether they had hb levels < or > 10 g / dl during radiotherapy . 
in our study , hb levels could be assessed in more than 300 patients , and anemia was defined according to generally accepted levels ( normal range hb 13.018.0 g / dl in males , 12.016.0 g / dl in females )  . 
prognostic factors in patients with glioblastoma ilar study on patients with laryngeal cancer , we could show that even patients with moderate anemia ( hb > 10 g / dl ) had a worse outcome than patients with normal hb values [ 20 ]  . 
in 80% of patients with glioblastomas who underwent oxygen measurements during surgery in the study of rampling et al [ 27 ] , more than 25% of the po2 readings were < 2.5 mm hg , far below the oxygen levels encountered in surrounding normal brain tissue . 
cerami et al [ 6 ] and brines et al [ 4 ] investigated the effects of erythropoietin on the central nervous system and demonstrated that erythropoietin is active in addition to its erythropoietic effect . peripherally injected erythropoietin crossed the blood - brain barrier and protected brain tissue from a variety of neuronal insults . 
 kleinberg et al [ 14 ] conducted a phase i study with rsr13 , a novel radioenhancing agent that noncovalently binds to hb , thereby reducing oxygen - binding affinity and increasing tissue oxygen release to hypoxic tissues . 
elevation of serum ldh levels was diagnosed in 38% of glioma patients enrolled in the study of buckell et al [ 5 ] , a finding that was later confirmed by smrcka et al [ 32 ]  . 
besides this , overall survival was influenced by other parameters like the length of history of fits , the extent of resection , and the total radiation dose . in both studies , median overall survival ranged from 4 months in the most unfavorable subgroup to 18 months in the best prognostic subgroup . 
it is interesting to note that in the rtog and mrc trials as well as in our nearly unselected patient population the median survival of poor - risk patients was similar . 
from our point of view , the inclusion of both anaplastic astrocytoma and glioblastoma and the consideration of treatment - related factors in both models are problematic . therefore we analyzed glioblastoma patients and pretreatment variables only . 
identification of new factors including molecular and genetic aspects [ 7 , 11 , 29 , 37 ] with a stronger prognostic effect is needed in order to define patient subgroups which can be useful for risk - adapted therapeutic strategies . 
 strahlentherapie und onkologie original article influence of fractionated irradiation on neutrophilic granulocyte function alfred haidenberger1 , paul hengster2 , marialuise kunc3 , oliver micke4 , thomas wolfgruber1 , thomas auer1 , peter lukas1 , alexander devries1 background : a recent study has demonstrated that radiation therapy with single doses of up to 32 gy has only a minor effect on neutrophilic granulocyte function . 
therefore , the aim of the current study was to verify the influence of fractionated radiation therapy on granulocyte function . material and methods : density gradient - purified granulocytes of voluntary healthy donors were used for all experiments . 
 conclusion : the study shows , that clinically used fractionated irradiation has an impact on granulocyte function , but contrary to common assumption , it is not the total dose itself but rather the fractionation which influences granulocyte function . 
 key words : chemiluminescence neutrophilic granulocytes fractionated irradiation function of granulocytes strahlenther onkol 2003 ; 179 : 459 doi 10.1007 / s00066 - 003 - 1041 - 0 einfluss fraktionierter bestrahlung auf die funktion neutrophiler granulozyten hintergrund : krzlich konnte gezeigt werden , dass eine bestrahlung mit einzeldosen bis zu 32 gy nur einen geringen einfluss auf die granulozytenfunktion hat . 
da die verwendeten dosierungsschemata nur selten anwendung in der klinischen routine finden , war es ziel der vorliegenden studie , daten ber den einfluss einer fraktionierten bestrahlung auf die granulozytenfunktion zu erheben . 
die annahme , dass nur die gesamtdosis fr eine funk1 department of radiotherapy , 2 department of transplant surgery , and 3 daniel swarovski research laboratory , leopold franzens university innsbruck , austria , 4 department of radiotherapy , university of mnster , germany . received : may 8 , 2002 ; accepted : october 21 , 2002 strahlenther onkol 2003 no . 
in addition to tumor modalities , therapeutic modalities such as steroids and chemotherapy clearly result in immunosuppression [ 24 ]  . also irradiation seems to have an impact on granulocytopoietic activity [ 26 ]  . neutrophilic granulocytes represent a major factor in cellular defense against bacteria and fungi [ 29 ]  . 
their main function consists in phagocytosis and killing of invading bacteria by releasing reactive oxygen species ( ros ) [ 4 ] , a process also known as oxidative burst [ 30 ] , which can be triggered by a number of chemical stimuli as well , e.g. , phorbol myristate acid ( pma ) , a complex lipid that induces the liberation of superoxide . 
therefore , the phagocytic function of granulocytes can be elegantly detected and quantified using chemiluminescence [ 1 ]  . recently , it was shown that radiation therapy with single doses of up to 32 gy did not significantly diminish ros release of granulocytes [ 9 ]  . 
therefore , the aim of the present study was to investigate the clinical influence of fractionated irradiation on the function of neutrophilic granulocytes . material and methods cells fresh blood from volunteer donors was used as leukocyte source after separating plasma and red blood cells . 
buffy coat ( 35 ml ) was layered on 15 ml lymphoprep ( nycomed pharma , oslo , norway ) in a conical 50 - ml tube ( falcon , becton dickinson labware , nj , usa ) and centrifuged at 1 , 000 g for 20 mthe band containing mononuclear cells was removed . the buffy coat was resuspended in 2% gelatin / phosphatebuffered saline . 
remaining erythrocytes were lysed by adding nh4cl 0.84% for 20 min at 37 c and then centrifuging aga after washing , cell count was adjusted to 1 ( cid : 1 ) 106 / ml in rpmi 1640 without fetal calf serum ( fcs )  . 
 chemiluminescence for the initial measurements , 50 l of luminol ( sigma , deisenhofen , germany ) , 1 : 1 , 000 dilution of 1.77 mg dissolved in 1 ml dimethylsulfoxide ( final concentration 44.5 m ) , were added and the initial value was assessed by chemiluminescence . chemiluminescence was performed in 96 - well microplates ( isoplate 1450 - 581 , wallac , turku , finland ) and evaluated at 24 c in the microplate luminometer lucy - 1 ( anthos , salzburg , austria )  . 
in order to investigate the relevant changes in ros release after pma stimulation and to minimize the influence of the absolute cell count and day - by - day variations , relative changes were calculated by setting the starting point before stimulation equal to 100% . differences between relative changes and irradiation were evaluated using the nonparametric mann - whitney u - test at a significance level of p < 0.05. 
the highest absolute ros release after stimulation was seen after radiation treatment with a single dose of 12 gy , whereas the lowest absolute ros release was observed after fractionated irradiation with a total dose of 18 gy . 
the main function of these cells is phagocytosis and killing of invading bacteria [ 3 ]  . besides the fact that the function of specific immune cells is reduced in cancer patients , little is known about the influence of irradiation on the function of neutrophilic granulocytes [ 19 ]  . 
recently , it was shown that irradiation with single doses of up to 32 gy had only a minor effect on the function of granulocytes , leaving functionally almost intact neutrophils table 1 . 
 it is well established that low - dose radiotherapy ( ld - rt ) together with total - body irradiation ( tbi ) enhances t - cell activation by facilitating signal transduction and modulating the expression of a number of genes involved in cytokine expression and cell survival in the immune organs [ 16 ]  . 
in contrast to tbi , irradiation as a localized treatment affects immune cells at the tumor site only but not cells circulating in the blood stream [ 10 ]  . 
therefore , the effect of tbi is qualitatively and quantitatively different from that of localized or regional irradiation [ 2 ]  . the present study shows that pma stimulation can increase ros independent of the radiotherapy schemes used . the finding that fractionated irradiation results in a marked decrease in ros release as compared to the same radiation dose given as a single dose may initially appear to be counterintuitive . 
counterintuitive , because normal cells have the capacity to repair sublethal damage caused by high single doses during the interval [ 23 ] , and therefore the effect of radiation on the function of cells should be higher following high single doses . 
similar results , however , were described in testes tissue where fractionated irradiation resulted in a more rapid decline in sperm number , longer recovery time , higher vulnerability , and a higher rate of irreversible azoospermia [ 7 , 11 , 18 ]  . 
liu et al [ 17 ] demonstrated different effects of low and high radiation doses on the immune syste low - dose radiation resulted in immune enhancement , and high - dose radiation in immunosuppression . 
limitations of these studies are the radiation treatment given as tbi , and the disregard of the release of stress hormones and the decrease in chemotactic , phagocytic and bactericidal activity of neutrophil granulocytes after anesthesia [ 8 ]  . pma stimulation causes an irreversible , complete release of ros . 
data involving doses > 18 gy were not tested in our study because of the limited life span of granulocytes . in this connection it must be discussed whether these doses could change the chemotactic behavior , which might result in a temporary , clinically effective immunodeficiency . conclusion our study shows that it is not the total dose itself but rather the fractionation which influences granulocyte function . 
in order to further characterize the mechanisms underlying these observations , cellular function ( protein expression , surface markers , oxygen consumption ) and structural parameters ( dna damage ) will be investigated . 
mueller2 , ulrike lambrecht1 , elisabeth pauli3 , oliver ganslandt4 , hermann stefan3 , rolf sauer1 ziel : diese prospektive studie untersuchte die effizienz einer fraktionierten stereotaktischen radiotherapie ( rt ) bei therapieresistenter temporallappenepilepsie . patienten und methoden : einschlusskriterien waren patienten im alter von 17 bis 65 jahren , die weder medikaments noch epilepsiechirurgisch anfallsfrei wurden und einen einseitigen fokus aufwiesen . 
zwei patientenkohorten zu je sechs patienten wurden zwischen 1997 und 1999 einer fraktionierten , stereotaktisch gefhrten radiotherapie mit 21 gy ( 7 ( cid : 1 ) 3 gy ) bzw . 
46% ( 2394% , entsprechend 0 , 223 anflle monatlich ) gemittelt ber den 18 - monatigen beobachtungszeitraueine verkrzung der anflle trat bei 46% ( fnf von elf ) der patienten edie anfallsintensitt verringerte sich gleichzeitig bei 64% ( sieben von elf ) , bei drei patienten ( 27% ) gab es keine besserung , eine person ( 9% ) klagte ber eine anfallsintensivierung . 
 schlsselwrter : fraktionierte stereotaktische radiotherapie pharmakoresistente temporallappenepilepsie strahlenther onkol 2003 ; 179 : 17 doi 10.1007 / s00066 - 003 - 1001 - 8 fractionated stereotactically guided radiotherapy for pharmacoresistant epilepsy aim : this prospective study evaluated the efficiency of fractionated stereotactically guided radiotherapy as a treatment of pharmacoresistant temporal lobe epilepsy . 
 patients and methods : inclusion criteria were patients aged between 17 and 65 years with one - sided temporally located focus , without sufficient epilepsy control by antiepileptic drugs or neurosurgery . 
 key words : fractionated stereotactic radiotherapy pharmacoresistant temporal lobe epilepsy 1 klinik und poliklinik fr strahlentherapie , 2 institut fr medizinische physik , 3 neurologische klinik , abteilung epileptologie , 4 neurochirurgische klinik , friedrich - alexander - universitt erlangen - nrnberg , erlangen . 
die patienten sind aufgrund ihrer krankheit nur selten zu einem selbststndigen leben oder zu einer geregelten arbeit fhig ; auch antiepileptika der neuesten generation vermgen die anflle nicht immer gnzlich zu unterdrcken . 
nach einschtzung der american epilepsy foundation werden trotz des einsatzes einer pharmakotherapie etwa 20% der patienten nicht anfallsfrei ( 3 , 2022 )  . bei einer altersspezifischen prvalenz zwischen 0 , 5 und 1% fr die epilepsie kann angenommen werden , dass in deutschland bis zu 160000 patienten mit pharmakoresistenten epilepsien leben . 
die rt bietet sich nicht nur als alternative an , sie verfgt auch ber eine vielzahl von therapeutischen vorteilen , wie die fehlende invasivitt , die abwesenheit von intraund post - operative risiken sowie die minimierung langfristiger therapiefolgen durch fraktionierung [ 1 , 9 , 24 ]  . 
gemeinsames kriterium aller patienten war die pharmakoresistente epilepsie bei vorliegen eines fokus im temporallappengebiet mit komplex - partiellen anfllen , meist kombiniert mit einfach - partiellen und sekundr generalisierten grand - mal - anfllen . 
ursprnglich handelte es sich um zwlf patienten , ein patient wurde von der weiteren evaluierung ( anfallsfreiheit , qualittsnderung etc . ) ausgeschlossen , da ein pilozytotisches astrozytom auslser der epilepsie war , nach dessen resektion die anflle sistierten . 
die nur patienten und methoden einschlusskriterien zielgruppe dieser studie waren patienten im alter von 17 bis 65 jahren mit einer manifesten , pharmakologisch resistenten epilepsie bei gesichertem , einseitigem fokus im temporallappen . weiterhin sollten alle epilepsiechirurgischen mglichkeiten ausgeschpft sein . als ausschlusskriterien waren ein fokus auerhalb des temporallappens , die fehlende geschftsfhigkeit und einsichtigkeit , ein immundefizienzsyndrom mit erhhter radiosensibilitt sowie schwangerschaft festgelegt . 
die studie wurde von der ethikkommission der medizinischen fakultt der friedrich - alexander - universitt erlangen - nrnberg positiv beurteilt , das schriftliche einverstndnis jedes patienten vor der behandlung eingeholt . identifikation des fokus das zielvolumen der rt war in der regel mit dem anzustrebenden ausma eines geplanten epilepsie - chirurgischen eingriffs identisch . 
die basisdiagnostik umfasste neben anamnese und neurologischer untersuchung das eeg ( siemens mingograf eeg21 ) mit oberflchenelektroden nach dem internationalen 10 / 20 - system , die bei den patienten auch stationr als epilepsiemonitoring durchgefhrt wurde . 
die sicherheitszone ber die pathologische signalgebung hinaus betrug 1 , 5 c neuropsychologische testung der berliner amnesie - test ( bat ) , frher der wechsler memory scale - revised ( wms - r ) und hamburg - wechsler - intelligenztest fr erwachsene ( hawie - r ) sowie der boston naming test , der token test und der rey - figure test wurden eingesetzt , um einbuen beim verbalgedchtnis , amnesiescore , bei aphasischen strungen etc . 
die anfallsfrequenzen vor und nach der rt sind in tabelle 2 zusammengefasst ; die monatlichen anfallszahlen wurden zu vierteljhrlichen durchschnittszahlen gemittelt , verteilt ber den 18 - monatigen minimalen beobachtungszeitrau die anfallsfrequenz nahm im durchschnitt des 18 - monatigen beobachtungsintervalls von monatlich 11 , 75 auf 7 , 45 ab . 
die 90bis 95% - isodose erfasste das epileptogene gebiet vollstndig ( siehe auch abbildung 1 )  . die dosisspezifikation erfolgte auf den referenzpunkt ( icru 50 ) , der in der regel dem isozentrum entsprach . 
nach einer zwischenauswertung ( sechs patienten ) zeigte sich eine gute anfallsreduktion , allerdings gab es auch hinweise auf neuropsychologische einbuen , weswegen die einzeldosis auf 2 gy bei erhhter gesamtdosis ( 30 gy ) gesenkt wurde ; die biologisch quivalente dosis ( bed ) blieb somit konstant . 
die folgenden zahlen beziehen sich auf die auswertbaren elf patienten : die anfallsdauer reduzierte sich bei fnf patienten ( 46% ) , keine nderung war bei den brigen patienten zu sehen . 
die intensitt wurde bei sieben patienten ( 64% ) gemildert , bei drei patienten ( 27% ) gab es keine besserung , in einem fall ( 9% ) eine verschlechterung . vier patienten ( 36% ) erfuhren durch die rt eine positive regelmigkeit ihrer anflle , die seitdem nur noch als anfallsserien auftreten . 
die reorientierungszeit wurde ( nach komplex - partiellen anfllen ) bei einem patienten verkrzt ( von 45 min auf 10 s ) , bei einem weiteren verlngert ( von 30 s auf 5 min ) , ebenso lie sich die reorientierungszeit bei zwei patienten nach generalisierten anfllen verkrzen . 
 radiotherapie wiederholen wrden , wenn sie damals schon gewusst htten , wie ihre befindenslage heute ist : sechs patienten ( 60% ) hielten die radiotherapie fr einen erfolg , fr eine patientin ist der erfolg fraglich , da sie keine wesentliche erleichterung bemerke , und drei patienten ( 30% ) wrden der rt nicht noch einmal zustimmen , da sie keinen erfolg bemerken wrden . 
als weiterer parameter der therapiekontrolle wurde nach 12 monaten eine kontroll - mrt durchgefhrt , die morphologische vernderungen darstellen sollte ; es spiegelten sich jedoch bei keinem der untersuchten neu aufgetretene lsionen im sinn einer sklerose wider . 
whrend des stationren aufenthalts erlitten zwei patienten je einen epileptischen anfall , eine weitere patientin litt im selben zeitraum unter drei fraglichen psychogenen anfllen , die bereits vor beginn der radiotherapie aufgetreten waren . 
drei patienten beklagten eine reversible strahleninduzierte alopecia areata , ebenfalls drei patienten klagten ber leichte befindlichkeitsstrungen wie unwohlsein , geringen neuropsychologische testergebnisse tabelle 4 gibt die ergebnisse der neuropsychologischen verlaufsuntersuchungen wieder . 
die gedchtnisleistung bei den vor und nach der rt untersuchten personen war bei drei patienten ( 33% ) unverndert und zeigte sich bei vier patienten ( 45% ) um bis zu 1 , 5 sd sowie bei strahlenther onkol 2003 no . 
die verbalen leistungen waren bei sechs von neun patienten nicht fassbar verndert , bei den brigen drei patienten um 12 sd schlechter . diskussion ziel dieses protokolls war es , die wirksamkeit ionisierender strahlung zur beeinflussung pharmakoresistenter epilepsien , die keiner epilepsiechirurgischen behandlung zugnglich waren , zu evaluieren . 
die vagusnervstimulation fhrte bei je einem drittel der behandelten patienten zu einer anfallsreduktion von ber 50% , von 2050% und bei einem drittel zu keiner verbesserung [ 5 , 20 ]  . eine positive vernderung der anfallsqualitt ( intensitt und dauer ) erlebten ber 50% [ 20 ]  . 
die so genannte gamma - knife - bestrahlung , bei der eine dosis von 1 ( cid : 1 ) 20 gy auf einen umschriebenen mesiobasalen fokus appliziert wird , kann allerdings nur nach strikter selektion des patientengutes angewendet werden . 
aufgrund von kontraindikationen knnen diese patienten weder operabel noch invasiv diagnostizierbar se hier wre ein neues , nicht invasives vorgehen hilfreich , das sich spezifisch auf die darstellung von nervenzellen richtet , die im sinne einer epilepsie geschdigt bzw . 
die hypothese , dass patienten mit temporallappenepilepsie durch den verlust von pyramidenzellen im gebiet der epileptogenen foci eine verminderte konzentration von n - acetylaspartat ( naa ) aufweisen , gilt gemeinhin als akzeptiert [ 4 , 10 , 16 ]  . 
die bildung eines quotienten aus naa und weiteren nervenzelltypischen substanzen ( cholin , kreatin ) , die bei epilepsiebedingter astrozytose ansteigen , wurde schon von verschiedenen autoren beschrieben , um einen fokus abzugrenzen [ 4 , 8 , 10 , 16 ]  . 
 es handelt sich bei den patienten der hier vorgelegten studie um schwerste , nicht therapierbare flle , deren neuropsychologische testergebnisse mit sehr hoher wahrscheinlichkeit auch ohne radiotherapie eine weitere verschlechterung erfahren htten . 
diese nicht invasive methode zeichnet sich bei der bisher nur geringen fallzahl durch hohes ansprechen bei geringen nebenwirkungen aus , wobei die indikationsstellung eine wesentliche rolle spielt . vergleichende untersuchungen an groen fallzahlen knnen diese methode weiter etablieren . 
eberhardt ke , stefan h , buchfelder m , pauli e , hopp p , huk w , tomandl bf : the significance of bilateral csi changes for the postoperative outcome in temporal lobe epilepsy . 
1 urban & vogel strahlentherapie und onkologie originalarbeit zeitfaktor und tumorrepopulierung whrend einer fraktionierten radiotherapie vergleich zweier xenotransplantierter plattenepithelkarzinome stefan hesselmann1 , katja lindel2 , kirsten horn1 , stefan knemann1 , andreas schuck1 , normann willich1 , christian rbe3 hintergrund : in der vorliegenden untersuchung wurde die effizienz einer akzeleriert fraktionierten bestrahlung im vergleich zu einer konventionell fraktionierten bestrahlung zur lokalen tumorkontrolle zweier humaner plattenepithelkarzinome am heterotransplantatmodell nu / nu - maus untersucht . 
andere ursachen , insbesondere eine zunahme der hypoxischen tumorzellfraktion , knnen jedoch nicht ausgeschlossen werden . schlsselwrter : fraktionierte strahlentherapie humane tumorxenografts tcd50 repopulierung strahlenther onkol 2003 ; 179 : 3844 doi 10.1007 / s00066 - 003 - 0954 - y time factor and repopulation during fractionated radiotherapy . 
comparison between two xenografted human squamous cell carcinoma background : a series of experiments were performed to determine the local tumour control of two human squamous cell carcinoma lines in nude mice . 
local irradiation was given without anaesthesia under ambient conditions to air breathing animals using 18 mev electrons of an linear accelerator ( mevatron 77 , siemens , munich )  . 
 1 klinik und poliklinik fr strahlentherapie radioonkologie , universittsklinikum mnster , 2 klinik fr radio - onkologie , universitt bern , schweiz , 3 abteilung fr strahlentherapie der radiologischen universittsklinik , universittskliniken des saarlandes , homburg / saar . 
als ursache dieses zeitfaktors wird eine beschleunigte repopulierung klonogener tumorzellen vermutet , die durch die behandlung selbst induziert wird und bei konventionell fraktionierter strahlentherapie ein hauptgrund fr die mangelnde lokale tumorkontrolle ist . 
der genaue mechanismus der repopulierung und ihr einfluss auf das verhalten eines tumors unter fraktionierter bestrahlung ist bis jetzt noch nicht eindeutig geklrt [ 15 , 27 , 29 ]  . 
es wurde untersucht , welchen einfluss mehrere strahlenapplikationen tglich bei verkrzter gesamtbehandlungszeit im vergleich zu einer strahlenapplikation am tag auf die kurabilitt von xenotransplantierten menschlichen plattenepithekarzinomen des kopf - hals - bereichs haben . weiter wurde der unterschied in der mittleren tumorkontrolldosis ( tumor control dose 50% ( tcd50 ) ) zwischen einer akzeleriert fraktionierten und einer konventionell fraktionierten strahlenbehandlung ermittelt . 
 als tumormodell wurden zwei auf die nacktmaus transplantierte menschliche plattenepithelkarzinomlinien verwendet . fr die experimente wurden 46 wochen alte weibliche und konstanzprfung um das heterotransplantatmodell sinnvoll in der experimentellen strahlentherapie einsetzen zu knnen , ist es erforderstrahlenther onkol 2003 no . 
so wurden von unserer arbeitsgruppe verschiedene konstanzprfungen ( histologische untersuchung des tumors in smtlichen passagen , bestimmung der volumenverdopplungszeit und durchflusszytometrische untersuchungen mittels brdurd - markierung ) bei der seriellen passagierung durchgefhrt , um die phnotypische stabilitt der tumoren zu besttigen . 
 absolutes tumorvolumen = ( lange achse ) ( cid : 1 ) ( kurze achse ) 2 ( cid : 1 ) 0 , 5 bestrahlungshalterung zur lagerung der tiere whrend der bestrahlung wurde eine spezielle halterungsvorrichtung entwickelt , die bei zuverlssiger fixierung eine optimale abschirmung des krpers und der pfote bei guter dosishomogenitt im tumortragenden bein ermglicht . 
weiter wurde ein 25 ( cid : 1 ) 25 cm groer tubus mit einer feldgre von 31 ( cid : 1 ) 31 cm gewhlt , sodass mit der speziellen halterung bis zu maximal zwlf muse in einem durchgang bestrahlt werden konnten . 
diese dosis ist ntig , um 50% der tumoren lokal zu kontrollieren . als lokal kontrolliert galten tumoren , die kontinuierlich bis zum ende des beobachtungszeitraumes geschrumpft oder makroskopisch verschwunden waren . 
 diskussion ziel dieser studie war die untersuchung des zeitfaktors und damit mglicherweise die repopulierungsleistung zweier humaner plattenepithelkarzinome unter ambientem blutfluss . mit zunehmender gesamtbehandlungszeit ist bei beiden tumoren ein abnehmender effekt der bestrahlung festzustellen bzw . 
die in unserem versuchsaufbau beobachtete zunahme der erforderlichen strahlendosis whrend einer fraktionierten strahlentherapie unter normalen blutflussbedingungen mit zunehmender gesamtbehandlungszeit wurde bereits bei anderen experimentaltumoren gefunden und kann mglicherweise auf eine beschleunigte repopulierung durch klonogene tumorzellen whrend einer fraktionierten strahlentherapie zurckgefhrt werden , obgleich die zugrunde liegenden mechanismen noch nicht vollstndig entschlsselt sind [ 1 , 4 , 5 , 8 , 15 , 21 , 22 , 27 , 29 ]  . 
 da die experimente unter nicht abgeklemmten blutflussbedingungen durchgefhrt wurden und hypoxische tumorzellen strahlenresistenter sind als gut oxygenierte tumorzellen kann eine zunahme der hypoxischen zellfraktion durch eine rarefizierung des gefnetzes den beobachteten zeitfaktor einer fraktionierten strahlentherapie ebenfalls erklren . 
diese beiden mechanismen schlieen sich zwar aufgrund der mglichkeit intratumoraler heterogenitt gegenseitig nicht vollkommen aus , es ist jedoch wahrscheinlich , dass mit zunehmender tumorhypoxie die proliferation von tumorzellen abnimmt [ 26 ]  . 
 [ 4 ] deuten darauf hin , dass fr die abnahme der lokalen tumorkontrolle mit zunehmender gesamtbehandlungszeit die repopulierung durch klonogene tumorzellen im vergleich zur zunahme der hypoxischen zellfraktion der magebendere faktor sein knnte . 
da die reparatur von subletalen strahlenschden innerhalb von 5 stunden abgeschlossen zu sein scheint und das zeitintervall zwischen zwei fraktionen in unseren experimenten mindestens 6 stunden betrug , erscheint dies eher unwahrscheinlich [ 18 ]  . 
bei der analyse von repopulierungsdaten muss jedoch unterschieden werden zwischen einer repopulierung whrend der fraktionierten strahlenbehandlung , whrend der bestrahlungspause und nach abschluss der strahlenbehandlung , da die repopulierungskinetik whrend einer behandlungspause nicht notwendigerweise der kinetik whrend einer kontinuierlichen fraktionierten strahlentherapie entsprechen muss [ 7 , 13 , 32 ]  . der in unseren experimenten festgestellte effekt knnte nun dementsprechend auf eine repopulierung whrend der fraktionierten bestrahlung im 24 - stunden - intervall , whrend der 72 - stndigen bestrahlungspause oder nach abschluss der bestrahlungsserie beruhen . 
zeitfaktor und tumorrepopulierung zustzlich konnte in einer aktuellen untersuchung an zwei xenotransplantierten plattenepithelkarzinomen gezeigt werden , dass kein unterschied in der hhe des zeitfakors zwischen einer kontinuierlich fraktionierten oder einer fraktionierten radiotherapie mit pausen besteht , sodass analysen zur repopulierungskinetik whrend einer kontinuierlich fraktionierten radiotherapie aus behandlungsprotokollen mit einer pause entwickelt werden knnen [ 6 ]  . 
schlussfolgerten aus ihren untersuchungen , dass die repopulierung mit einer zeitverzgerung von einigen wochen beginnt und dass der anstieg der tcd50 mit zunehmender gesamtbehandlungszeit anschlieend linear dargestellt werden kann ( dog - leg )  . 
diese initiale verzgerung des repopulierungsbeginns zwischen 1 und 3 wochen whrend einer fraktionierten strahlentherapie wurde ebenfalls bei untersuchungen unter abgeklemmtem blutfluss an verschiedenen experimentaltumoren beschrieben [ 20 , 23 , 27 , 29 ]  . 
diese vermutung , dass die zur lokalen tumorkontrolle notwendige strahlendosis aufgrund einer eventuellen , frhzeitig einsetzenden repopulierung linear und insgesamt ohne groe verzgerung direkt nach dem behandlungsbeginn ansteigt , konnte bei untersuchungen an verschiedenen experimentaltumoren beobachtet werden [ 1 , 4 , 5 , 9 , 10 ]  . 
diese uneinheitlichen ergebnisse bezglich des repopulierungsbeginns bei tumoren unterschiedlicher histologie , tumoren gleicher histologie und identischen tumorzelllinien in verschiedenen experimenten weisen auf eine ausgeprgte interund intratumorale heterogenitt der proliferationskinetik der bestrahlten tumoren whrend einer fraktionierten strahlentherapie hdie ursache hierfr ist unklar [ 5 ]  . 
plattenepithelkarzinome des kopf - hals - bereichs , die akzelerierte fraktionierung eine sinnvolle alternative sein knnte , da hierdurch der einfluss der repopulierung reduziert wird und eine erhhte lokale tumorkontrolle erreicht werden kann . 
diese experimentell gewonnenen ergebnisse werden durch klinische studien untersttzt , die im vergleich zu einer konventionellen bestrahlung durch eine akzelerierung der bestrahlung eine bessere lokale tumorkontrolle erreichten [ 3 , 11 , 17 , 24 ]  . 
andere denkbare methoden zur minimierung des zeitfaktors wie proliferationshemmung durch chemotherapeutika oder blockade proliferationsstimulierender signaltransduktionswege sind wissenschaftlich bislang nicht belegt und mssen zurzeit als spekulativ betrachtet werden [ 28 ]  . schlussfolgerung heutzutage gibt es keinen zweifel mehr daran , dass die repopulierung durch klonogene tumorzellen ein magebender faktor fr die lokale tumorkontrolle ist . 
a radiation therapy oncology group ( rtog ) phase iii randomized study to compare hyperfractionation and two variants of accelerated fractionation to standard fractionation radiotherapy for head and neck squamous cell carcinoma : first report of rtog 9003 . 
strahlenther onkol 1991 ; 167 : 2630 . korrespondenzanschrift stefan hesselmann klinik und poliklinik fr strahlentherapie radioonkologie universittsklinikum mnster albert - schweitzer - strae 33 , 48129 mnster deutschland telefon ( + 49 / 251 ) 8347 - 834 , fax : - 355 e - mail : hessels@uni - muenster.de strahlenther onkol 2003 no . 
1 urban & vogel strahlentherapie und onkologie originalarbeit retrospektive ergebnisse der perkutanen strahlen therapie der tuba eustachii bei chronischer otitis media jrgen schultze1 , constantin reinke1 , knut arvid frese2 , bernhard kimmig1 hintergrund : die behandlungsergebnisse der symptomatischen radiotherapie bei chronischer otitis media sollten retrospektiv evaluiert werden . patienten und methoden : zwischen 1980 und 1997 wurden 66 patienten vorgestellt . 
die beschwerden bestanden im median 4 , 7 jahre , die primr konservative ( adstringentien , antibiotika ) und operative therapie ( parazentese , paukenrhrchen , tympanoplastik ) hatte keine dauerhafte besserung erbracht . 
unter den ausschlussgrnden fr eine strahlentherapie waren ablehnung des patienten ( neunmal ) , radiogene vorbelastungen ( sechsmal ) und spontane besserung nach initialer vorstellung . die ergebnisevaluation erfolgte ber die subjektiven angaben der patienten und den hno - rztlichen untersuchungsbefund . 
in der gruppe der nicht bestrahlten 26 patienten , von denen 22 evaluiert werden konnten , gaben 16 ( 72% ) unverndert beschwerden und ein persistieren der otitis media an . 
in einer subgruppenanalyse hinsichtlich der beschwerdedauer zeigte sich die strahlentherapie bei den akuten und subakuten fllen als sehr effektiv , whrend die patienten in einem chronischen stadium , mehr als 5 jahre nach diagnosestellung , kaum noch auf die radiotherapie reagierten . schlussfolgerung : die radiotherapie ist eine geeignete methode zur symptomatischen besserung der therapierefraktren chronischen otitis media . 
die strahlentherapie sollte bereits nach versagen der initial erfolglosen konservativen und operativen therapie durchgefhrt werden . schlsselwrter : chronische otitis media strahlentherapie gutartige erkrankungen strahlenther onkol 2003 ; 179 : 317 doi 10.1007 / s00066 - 003 - 1026 - z retrospective results of radiation therapy of the eustachian tube in chronic otitis media background : the treatment results of symptomatic radiation therapy of the eustachian tube in chronic otitis media had to be evaluated retrospectively . patients and methods : between 1980 and 1997 , 66 patients were referred for therapy . 
the complaints lasted for 4.7 years in the median , primary conservative ( adstringentia , antibiotics ) and surgical treatment ( paracentesis , tympanic tubule , tympanoplastic ) did not lead to lasting cure . 
under the causes for exclusion of radiation therapy were non - acceptance of the patients ( nine ) , prior radiation therapies ( six ) or spontaneous improvement after initial presentation in our department . 
in the group of 26 nonirradiated patients , 22 could be interviewed indicating in 16 cases ( 72% ) that the complaints were unchanged and chronic otitis media was lasting . 
strahlentherapie der chronischen otitis media conclusions : radiation therapy is an effective tool for symptomatic improvement of the therapy - resistant chronic otitis media . a dose of 6 gy seems to be sufficient to achieve an antiinflammatory effect . 
 key words : chronic otitis media radiation therapy benign diseases einleitung die chronische otitis media auf dem boden einer chronischen tubenfunktionsstrung ist eine fr den patienten sehr belastende erkrankung und stellt den therapeuten vor erhebliche probleme . 
die zeitgleich beginnende steigerung der aktivitt des lokalen schleimhautimmunsystems hat dann zur folge , dass jeder bakterielle reiz einerseits die hyperplasie und metaplasie des oberflchenepithels anregt , andererseits die entstehung eines gewebedems mit relativer zellulrer infiltration auslst . 
es entwickelt sich ein unterdruck , dann ein adhsivprozess , und schlielich resultiert daraus eine chronische otitis media mesotympanica oder ein cholesteato grundstzlich kann man drei hauptformen der ventilationsund drainagestrungen voneinander differenzieren : zum einen die reine tubare insuffizienz , die tubenfunktionsstrung mit chronischem paukenerguss , als zweites die chronische otitis media mesotympanica und drittens das cholesteatodie tubenfunktionsstrung kann einen reversiblen verlauf haben , die chronische otitis media mesotympanica nimmt einen chronischen verlauf , ist zumindest nur partiell reversibel und bedarf einer chirurgischen sanierung . 
das cholesteatom bedarf immer einer chirurgischen sanierung . im chronischen erkrankungsstadium besteht funktionell eine deutliche schallleitungsschwerhrigkeit im bereich von 2040 db sowie ein schallleitungsblock bei unterbrechung der schallleitungskette von 6070 db sowie ein pathologisch verndertes tympanogramim rntgenbild nach schller kann eine verschleierung des mastoidzellsystems infolge der verminderung des luftgehaltes auftreten . 
 ziel dieser untersuchung war die retrospektive evaluation der effektivitt der perkutanen radiotherapie bei patienten mit einem chronischem paukenerguss , einer chronischen otitis media mesotympanica und einem cholesteatom auf dem boden einer tubenfunktionsstrung . 
da diese art der behandlung zuvor nur kasuistisch durchgefhrt wurde , galt es zustzlich zu klren , inwieweit die strahlentherapie tatschlich ein tragfhiges behandlungskonzept bieten und eine sinnvolle therapiealternative sein kann . 
 die dieser arbeit zugrunde liegenden und ber 17 jahre recherchierten 66 behandlungsflle sollen dazu beitragen , eine bewertung der effektivitt der radiotherapie zu erreichen und eine klare indikation fr den einsatz dieses verfahrens zu erarbeiten . 
 patienten und methoden in der radiologischen klinik / klinik fr strahlentherapie der universitt kiel wurden zwischen 1980 und 1997 insgesamt 66 patienten mit der diagnose eines chronischen paukenergusses , einer chronischen otitis media mesotympanica oder eines cholesteatoms vorgestellt . 
die hno - rztliche befundung ergab bei den patienten mit chronischem paukenerguss und chronischer otitis media mesotympanica in 28 fllen eine lokalisation der erkrankung rechts , in 24 fllen links . 
 die abschlieende otologische diagnose ergab bei 22 patienten eine tubenventilationsstrung , bei 34 patienten eine chronische otitis media mesotympanica , in zehn fllen ein cholesteato die bei allen patienten durchgefhrte audiometrie ergab berwiegend einseitige , teilweise auch beidseitige schallleitungsschwerhrigkeit . 
zustzlich erfolgte bei sechs patienten ein felsenbein - ct , in einem fall wurde auch eine magnetresonanztomographie durchgefhrt , um den verdacht auf ein akustikusneurinom auszuschlieen ( abbildung 1 )  . 
die grnde waren die ablehnung der behandlung durch den patienten ( neun flle ) , strahlentherapeutische vorbelastung aufgrund maligner erkrankungen ( sechs patienten ) oder das interkurrente auftreten anderer erkrankungen sowie spontanremissionen . 
als positives ergebnis wurden ein ausbleiben des ohrschmerzes , der otorrh oder des schwindels sowie eine verbesserung des hrvermgens gewertet . die stabilisierung eines symptoms alleine wurde nicht als eine verbesserung gewertet . 
die herddosis betrug 6 gy , fraktioniert dreimal wchentlich mit einzeldosen von 1 gy , die typische feldgre betrug 5 ( cid : 1 ) 5 cm , allen patienten wurde eine gesichtsmaske appliziert . 
improved ent - examination ( n = 38 )  . vor rt nach rt 3 monate nach rt > 1 jahr nach rt tympanometrie 0 otoskopie audiogramm fr 26 der 28 patienten in subjektiv beschwerdefreiem zustand sind die hno - rztlichen untersuchungen nach strahlentherapie lckenlos dokumentiert ( tabelle 2 )  . 
 zwlf patienten gaben an , durch die perkutane radiotherapie keine nderung ihrer situation festgestellt zu haben . druckund vllegefhl , hrmissempfindungen , ohrschmerz , otorrhen sowie schwindel seien unverndert , lediglich die hrminderung wurde von neun patienten nicht mehr als so strend empfunden . 
 einflussfaktor beschwerdedauer von 26 patienten mit einer symptomatischen besserung nach radiotherapie waren 15 in einem akuten , elf in einem subakuten krankheitsstadiu bei den therapierefraktren fllen war lediglich ein patient in einem akuten , vier patienten in einem subakuten und sieben patienten in einem chronischen erkrankungsstadiu diskussion die wirksamkeit der strahlentherapie auch bei gutartigen erkrankungen ist bekannt und im schrifttum der letzten jahre mehrfach belegt [ 11 , 21 , 22 , 24 ]  . fr die strahlentherapeutische behandlung der chronischen otitis media wurden verschiedene behandlungsanstze beschrieben [ 1214 ]  . 
thullen [ 27 ] fhrte eine endokavitre , intratubare bestrahlung des tubenostiums durch , wobei die dosis lokal durch eine strontiumeinlage appliziert wurde . diese erfolgte durch einen tubenkatheter , mit dem eine lokaldosis von 510 gy appliziert wurde . 
 zuvor behandelten aber auch crowe & burnam [ 6 ] durch eine kontaktbehandlung mit radiu das nuklid wurde in einer 15 mm langen kapsel mit 3 mm durchmesser , die aus einer messinghnlichen legierung bestand , untergebracht und auf einen dnnen metallstab aufgeschraubt . 
hnliche therapien wurden whrend des zweiten weltkriegs zur behandlung der aerootitis media herangezogen . fast alle groen ausbildungsorte der us - luftwaffe sowie die u - boot - sttzpunkte der us - navy wurden mit radiumtrgern in ortsfesten wie auch mobilen gerten zur behandlung einer aerootitis media ausgerstet . 
fr die behandlung solcher prozesse im mittelohrbereich finden sich erste literaturhinweise von szasz [ 25 ] aus dem jahr 1922 sowie ammersbach & wucherpfennig [ 1 ] , die mit einer rntgenbestrahlung bei einer chronischen mittelohrentzndung das so genannte schleimohr behandelten . 
wie bei thullen [ 26 ] befand sich in unserem kollektiv etwa die hlfte aller therapierefraktren patienten in einem chronischen krankheitsstadiu thullen [ 28 ] folgerte daraus , dass die tube durch das chronische entzndungsstadium stenotisch verndert wre . 
1 urban & vogel strahlentherapie und onkologie original article recursive partitioning analysis ( rpa ) class does not predict survival in patients with four or more brain metastases carsten nieder , nicolaus andratschke , anca l . 
grosu , michael molls1 background : we evaluated prognostic factors for survival in patients with four or more brain metastases in order to determine whether intense local treatment might be justified for some of theif up to three brain metastases are present , surgical resection or radiosurgery are currently being considered in case of favorable prognostic factors . 
recursive partitioning analysis ( rpa ) prognostic classes have been described by the radiation therapy oncology group ( rtog ) in 1997 ( class i : karnofsky performance status [ kps ] 70% , age 65 years , no extracranial metastases , controlled primary tumor ; class iii : kps < 70% ; class ii : others )  . 
criteria of rpa class i ( ii ) were met in 4% ( 41% ) , whereas 56% had kps < 70% and thus were grouped into class iii ( tables 1 and 2 )  . complete or partial remission of brain metastases was found in 46% of patients who underwent computed tomography . 
number of brain metastases , rpa class , and treatment - related factors such as total dose or remission of brain metastases had no appreciable influence on survival ( figure 1 )  . 
multivariate analysis failed to identify any significant prognostic factor . conclusions : patients with four or more brain metastases seem to represent a group with unfavorable prognosis where remission of brain metastases or administration of more than 30 gy were not associated with increased survival . 
 key words : brain metastases radiation therapy prognostic factors strahlenther onkol 2003 ; 179 : 1620 doi 10.1007 / s00066 - 003 - 1028 - x die rpa - klasse erlaubt keine vorhersage der berlebenszeit von patienten mit vier oder mehr hirnmetastasen hintergrund : die prognosefaktoren fr patienten mit vier oder mehr hirnmetastasen wurden ausgewertet , um festzulegen , ob einige dieser patienten eine intensivierte lokalbehandlung erhalten sollten . 
 patienten und methoden : retrospektive analyse ( intention - to - treat ) von 113 patienten , die an einer einzigen klinik mittels ganzhirnbestrahlung ohne resektion oder radiochirurgie behandelt wurden . 
die kriterien fr klasse i lauten : karnofsky - index ( kps ) 70% , alter 65 jahre , keine extrakraniellen metastasen , kontrollierter primrtumor ; klasse iii : kps < 70% ; klasse ii : andere . 
eine komplette oder partielle remission der hirnmetastasen wurde bei 46% der patienten , 1 department of radiotherapy and radiologic oncology , klinikum rechts der isar , technical university of munich , germany . received : march 25 , 2002 ; accepted : june 19 , 2002 strahlenther onkol 2003 no . 
 schlussfolgerung : patienten mit vier oder mehr hirnmetastasen scheinen eine subgruppe mit ungnstiger prognose zu reprsentieren , bei denen ein ansprechen der metastasen oder eine hher dosierte strahlentherapie das berleben nicht verbesserten . die zahl der patienten in rpa - klasse i war zu gering fr definitive schlussfolgerungen . 
for instance , two randomized trials excluding patients with multiple brain metastases have shown that surgical resection plus radiotherapy is significantly better than radiotherapy alone [ 20 , 26 ]  . 
stereotactic radiosurgery ( srs ) also achieves local control in 8092% , whereby survival is comparable to that reported from surgical series when a matching patient selection is provided [ 13 , 5 , 7 , 16 , 21 , 24 ]  . 
such patients also were included in the randomized study rtog 95 - 08 , a trial of whole - brain radiotherapy ( wbrt ) plus stereotactic radiosurgery [ 25 ]  . 
for example , in a randomized study by kondziolka et al [ 13 ] median survival of patients with four brain metastases treated with stereotactic radiosurgery plus whole - brain radiotherapy was 3 months only . 
the role of chemotherapy in primary as well as metastatic brain tumors is still not satisfactory defined and hence subject of numerous ongoing studies [ 6 , 10 , 11 ]  . 
in 1997 , gaspar et al [ 8 ] performed a recursive partitioning analysis ( rpa ) of three rtog studies , resulting in three different rpa classes with clearly distinct prognosis . 
class i includes patients 65 years of age , karnofsky performance status ( kps ) of 70% , with controlled primary tumor and no extracranial metastases . class iii includes patients with kps < 70% , class ii patients who do not qualify for class i or iii . 
in order to answer the question whether or not this scoring system might be applicable to the particular group of patients with four or more lesions , we performed an evaluation of our database . 
all patients had histologic confirmation of their primary malignancy or a stereotactic biopsy of the brain ( in case of an unknown primary tumor ) , chest radiograph and / or ct ( depending on primary tumor ) , abdominal ultrasound and / or ct ( depending on primary tumor ) , and radionuclide bone scan . 
 in all cases , whole - brain radiotherapy was administered 5 days / week by use of a 6 - mv photon beam from a linear acstrahlenther onkol 2003 no . 
1 urban & vogel tering continuous variables for age , kps , and number of brain metastases and categorized variables for primary tumor , extracranial metastases , and rpa class . 
number of brain metastases , rpa class ( figure 1 ) , and treatmentrelated factors such as total dose or remission of brain metastases had no appreciable influence on survival . 
 discussion this retrospective intention - to - treat analysis of 113 patients irradiated at a single institution essentially confirmed that patients with four or more brain metastases represent a group with unfavorable prognosis . 
wronski et al [ 27 ] examined 119 patients with renal carcinoma and found that median survival of 15 patients with four or more brain metastases treated with whole - brain radiotherapy was 2 months , significantly shorter than that of the remaining patients . 
survival curves for time to death from any cause were computed on the basis of intentionto - treat using the method of kaplan & meier , beginning on the first day of radiotherapy . 
despite a reasonable sample size , significant prognostic factors were difficult to determine . compared to previous reports [ 8 , 9 , 14 , 19 ] , our results suggest that the influence of established prognostic factors that could only be seen as trend in our patient population is less pronounced in an analysis of a well - defined rather than an unselected patient group . 
additionally , a generally accepted scoring system that can be applied in daily routine might facilitate both realistic estimation of a patients prognosis and creation of inclusion criteria for future therapeutic trials . 
these figures as well as the fact that remission of brain metastases or administration of more than 30 gy were not associated with increased survival lead us to conclude that a short or very short palliative treatment course might be appropriate for the majority of patients , particularly those in rpa class ii and iii . 
 strahlentherapie und onkologie kurzmitteilung kraniospinale bestrahlung patientenlagerung und verifikation lothar wisser1 , tan phu nguyen1 , peter barwig2 , anja stolz2 , markus niewald1 , heinrich schller2 hintergrund : die verbesserung der technik sowohl hinsichtlich der reproduzierbarkeit der patientenlagerung als auch der verifikation der feldanschlsse stellt einen entscheidenden schritt zur qualittssicherung bei der bestrahlung der kraniospinalen achse dar . 
 schlsselwrter : kraniospinale bestrahlung qualittssicherung verifikation feldanschluss patientenlagerung strahlenther onkol 2003 ; 179 : 503 doi 10.1007 / s00066 - 003 - 0989 - 0 craniospinal irradiation patient positioning and verification with portal films background : implementation of an important step for quality assurance in irradiation of the craniospinal axis was made through changes in the irradiation technique . 
crucial improvements in patient positioning and the possibility of taking portal films of the field junctions are described . material and methods : a box for the positioning of the head of the patient in has been developed . 
 furthermore , a method for taking portal films of the field junctions between the lateral cranial and the upper dorsal spinal field as well as between the two dorsal spinal fields is described . 
 key words : craniospinal irradiation quality assurance portal verification field junctions patient positioning einleitung einige tumoren des zentralnervensystems zeichnen sich durch die fhigkeit aus , sich innerhalb des liquorraums auszubreiten , sich an den meningen festzusetzen und dort zellkolonien auszubilden . 
weiter ist darauf zu achten , dass die relative lage von vakuumkissen zu kopfhalterung eindeutig definiert ist , um variabilitten der kopfrotation im atlantookzipitalgelenk durch differierende krperpositionen zu vermeiden [ 4 ]  . 
hierdurch konnte ein entscheidender beitrag zur qualittssicherung geleistet werden . die anfertigung der verifikationsaufnahmen mit den feldgrenzen der seitlichen zerebralfelder und der dorsoventralen wirbelsulenfelder ist mit einer speziellen technik unter verwendung des multileafkollimators ( mlc ) mglich . 
gleichzeitig ist es blich , die zerebralen liquorrume ber zwei seitlich opponierende felder zu bestrahlen , um kritische strukturen wie augen , gesichtsschdel und nasenrachen besser schonen zu knnen [ 2 , 3 , 6 , 9 , 11 ]  . 
der verstrkung der unerwnschten wirkungen . die verifikation des feldanschlusses zwischen schdelfeld und wirbelsulenfeld war bisher aufgrund der um 90 verschiedenen bestrahlungsrichtungen nicht mglich und die verifikation des feldanschlusses zwischen den beiden wirbelsulenfeldern war wegen der berschneidung ventral nicht aussagekrftig . 
die akzeptanz der hilfsmittel beim patienten sollte ebenfalls gesteigert werden . die bonner box , eine kopfbox aus plexiglas , wurde entworfen und eigens angefertigt , um die abformung eines individuellen gesichtsabdrucks bei bauchlage der patienten in einem eingesetzten stck thermoelastischem material zu ermglichen ( abbildung 1 )  . 
 ohne deren position zu verndern , wird nun bei der bestrahlung des wirbelsulenfelds durch eine im bereich des filmes auerhalb des patienten aufgefahrene lamelle des mlc der film erneut belichtet , diesmal orthogonal . 
bei korrekter einstellung aller bestrahlungsparameter ( tischund kollimatordrehung ) sollten sich beide feldgrenzen , die kaudale des seitlichen hirnschdelfeldes und die kraniale des wirbelsulenfeldes , aneinander angrenzend darstellen . eine simultane kontrolle von kollimatorbzw . 
tischdrehung und tischverschub ist somit ebenso mglich wie eine bildgebende dokumentation des feldanschlusses ( abbildungen 2a bis 2c )  . eine zweite mglichkeit , die diese technik bietet , ist das anbringen der kontrollfilme unter dem patienten auf der tischplatte . 
der vorteil dieser technik besteht darin , dass sogar beide opponierenden schdelfelder in ihrer kaudaisodosenplne , die unter verwendung des planungssystems pinnacle der adac - laboratories erstellt wurden , zeigen insbesondere im bereich der feldanschlsse nahezu optimale dosisverteilungen ohne nennenswerte hotoder cold - spots ( abbildung 3 )  . 
 diskussion die methode der kraniospinalen bestrahlung mit zwei lateral opponierenden gegenfeldern im kopfbereich und ein bis zwei dorsalen stehfeldern im wirbelsulenbereich ist in den standardwerken der strahlentherapie hinlnglich beschrieben [ 2 , 3 , 9 , 11 ]  . 
 die lagerung des kopfes stellte in der vergangenheit ebenfalls oft ein problem dar , da die reproduzierbarkeit der kopfhaltung in bauchlage unter zuhilfenahme der handelsblichen positionierungshilfen suboptimal oder nicht fr die bauchlage geeignet war [ 1 ]  . 
 die spezielle anordnung der bestrahlungsfelder zueinander und die vorgestellte verifikationstechnik ermglichen erstmals eine dokumentation der relation der feldgrenzen zueinander sowohl an der grenze zwischen zerebralund wirbelsulenfeld als auch an der grenze zwischen kranialem und kaudalem wirbelsulenfeld . 
 die bequemlichkeit fr den patienten wurde verbessert und somit auch die akzeptanz der verwendeten hilfsmittel . durch die mglichkeit der dokumentation der feldanschlsse wird ein entscheidender schritt zur qualittssicherung geleistet . danksagung der besondere dank gilt dem leiter der werkstatt in der radiologischen klinik der universitt bonn , herrn reinhard hiepko , der durch seine hervorragenden ideen und deren perfekte umsetzung die strahlentherapie nicht nur bei der entwicklung der bonner box in idealer zusammenarbeit untersttzt . 
 korrespondenzanschrift lothar wisser abteilung fr strahlentherapie gebude 49 radiologische klinik universitt des saarlandes 66421 homburg / saar telefon ( + 49 / 6841 ) 16 - 24873 fax - 24699 e - mail : rawisser@uniklinik - saarland.de strahlenther onkol 2003 no . 
1 urban & vogel strahlentherapie und onkologie kurzmitteilung strahlentherapie des keloids in deutschland patterns - of - care - studie ergebnisse einer umfrage joachim kutzner1 , lida schneider2 , michael heinrich seegenschmiedt3 hintergrund : keloide stellen eine gutartige gewebswucherung der haut dar . 
 patienten und methode : durch eine umfrage an 250 strahlentherapiekliniken / - praxen in deutschland 1997 / 2000 wurden daten zur keloidbehandlung bezglich der therapiedurchfhrung , ergebnisse und nebenwirkungen ermittelt . 
 ergebnisse : die strahlentherapie erfolgte berwiegend kurzfristig postoperativ mit konventioneller rntgenstrahlentherapie und beschleunigerelektronen von 412 mev energie bei einer fraktionierung von 3 bis 5 ( cid : 1 ) / woche bei einzeldosen von 23 gy und gesamtdosen von 1020 gy . 
die beobachteten nebenwirkungen waren gering , insbesondere wurde keine malignombildung festgestellt . schlussfolgerung : die postoperative strahlentherapie des keloids wird in deutschland berwiegend unter hnlichen bedingungen durchgefhrt und bietet bei guter vertrglichkeit und nur geringen nebenwirkungen eine wirksame rezidivprophylaxe . 
 patients and method : dates of investigations with questionnaire on mail of 250 radiotherapy institutions in germany in 1997 / 2000 were collected to know therapy modalities , results and side effects . 
 results : mostly radiotherapy was applicated soon postoperatively with kilovoltage radiotherapy or elektrons 412 mev fractionated 35 times a week and single doses of 23 gy up to total doses of 1020 gy . 
a follow - up for 2 years is necessary to see outcome and relapses of irradiation . key words : keloids radiotherapy of benign diseases radiation side effects 1 klinik und poliklinik fr radiologie der universittskliniken mainz , 2 strahlentherapie und onkologie der stdt . 
strahlentherapie des keloids in deutschland einleitung auch wenn das keloid eine gutartige erkrankung hnlich einer hypertrophen narbenbildung darstellt , werden die betroffenen patienten durch schmerzen , wachstum mit raumforderung , juckreiz und oberflchenempfindlichkeit erheblich belstigt . 
wegen der hohen rezidivquote nach alleiniger operation erscheint die operative entfernung gefolgt von einer sich kurzfristig anschlieenden bestrahlung die therapie der wahl zu se diese untersuchung als pattern of care study erfolgte zur ermittlung der in deutschland durchgefhrten strahlentherapie des keloids . 110 1150 51200 zur ermittlung der verschiedenen therapieformen bei der bestrahlung eines keloids in bezug auf dosierung , fraktionierung und strahlenqualitt erfolgte 1997 der versand eines fragebogens an alle deutschen strahlentherapeuten in einer praxis oder klinik . 
bei insgesamt 77 kliniken betrug der zeitraum zwischen 1 und 35 jahren , bei 29 kliniken 15 jahre , bei 23 kliniken 610 jahre , bei 22 kliniken 1120 jahre und bei drei kliniken ber 20 jahre . 
auf eine wertung wurde verzichtet , eine hochrechnung einer angenommenen mittleren patientenanzahl unter bercksichtigung von erfassungszeitraum und klinikanzahl erfolgte nicht ( tabelle 1 )  . eine eigene auswertung besttigten 20 kliniken , verneint wurde dies bei 62 rckmeldungen . 
different types of radiation for keloid therapy . konventionelle rntgenstrahlung elektronen ( beschleuniger ) ( 412 mev ) strontium - 90 - strahlenquelle ( dermaplatte ) caesium - 137 - strahlenquelle iridium - 192 - al - quelle photonen in einigen kliniken wurden mehrere strahlenqualitten eingesetzt tabelle 3 . 
als dermaplatte fr kleine keloidbestrahlungen geeignet , fand in acht kliniken anwendung , iridium - 192 , caesium - 137 und photonen des beschleunigers kamen selten zum einsatz ( tabelle 2 )  . 
used x - ray single doses . gesamt : 0 , 57 gy dosisvariationen innerhalb einer klinik : n = 46 kliniken ( n = 94 ) unter 2 gy ed 23 gy ed 25 gy ed ber 5 gy ed mehrfachzhlungen eingeschlossen die gesamtdosen schwankten zwischen 3 und 30 gy , die meisten kliniken ( n = 83 ) gaben 1020 gy ( tabelle 5 )  . die fraktionierung der bestrahlung reichte von 1 bis 7 ( cid : 1 ) / woche bezogen auf 88 kliniken , berwiegend wurde 5 ( cid : 1 ) / woche bestrahlt . 
einzeldosen , gesamtdosen und fraktionierung variierten auch innerhalb der einzelnen kliniken . in den meisten kliniken ( n = 92 ) erfolgte die bestrahlung nach operativer keloidentfernung als prophylaktische behandlung , in vier kliniken wurde vor der operation bestrahlt . der zeitpunkt der bestrahlung schwankte zwischen dem operationstag und 7 tage postoperativ , der hauptanteil des tabelle 5 . 
 in unterschiedlichen zeitabstnden zwischen 1 woche und 132 monaten wurden patienten einmalig in 45 kliniken und mehrfach in 13 kliniken untersucht , die anzahl der untersuchten patienten fehlte jedoch mehrfach in der rckmeldung . 
13 kliniken fhrten keine nachkontrollen durch . insgesamt wurden 101 ( 11 , 4% ) rezidive in 26 kliniken beobachtet , wobei einige patienten mehrere keloide aufwiesen , sodass die anzahl der keloide / bestrahlungsfelder nicht genau mit der der patientenanzahl bereinstimmt . 
in einer klinik wurde ein teil des patientenkollektivs mit einzeldosen von 0 , 5 gy und 1 gy bei gesamtdosen von 4 gy bei acht patienten und gesamtdosen von 67 gy bei 50 patienten bestrahlt . 
 diskussion von der degro und auch von anderen medizinischen fachgesellschaften werden zunehmend leitlinien fr behandlungen herausgegeben , deren juristisch zwar nicht bindender , jedoch richtungweisender charakter abweichungen bei entsprechender dokumentation zulsst . 
zur aufstellung von leitlinien ist jedoch der istzustand der gegenwrtigen therapiemanahme zu erfassen unter bercksichtigung eines ausreichend hohen rcklaufs bei befragungen zur ermittlung einer relevanten aussage ber durchfhrung , therapieergebnisse und nebenwirkungen . 
bei der anwendung der konventionellen rntgenstrahlung ist der teilweise lange erfassungszeitraum zu bercksichtigen , in den letzten jahren drfte berwiegend die elektronentherapie genutzt worden sebei einer fraktionierung von 3 bis 5 ( cid : 1 ) / woche wurden berwiegend gesamtdosen von 1020 gy gegeben , die bestrahlung erfolgte kurzfristig nach der operation berwiegend bis einschlielich dem der operation folgenden tag . auch wenn keine genaue aufschlsselung der rezidivquote bei sehr niedriger einzelund niedriger gesamtdosis erfolgte , erscheint der prventiveffekt der bestrahlung zweifelhaft [ 4 ]  . 
 bei der wertung der rezidive muss die kleine patientenzahl mancher klinik bedacht werden : bei patientenzahlen von 110 und einer rezidivbildung von 14 ergeben sich 40100% rezidivbeobachtungen in einer klinik . 
zur exakten beurteilung der rezidivhufigkeit ist eine klinische patientenkontrolle ber mindestens 24 monate erforderlich . einmalige , relativ kurzfristige patientennachuntersuchungen lassen eine sichere beurteilung des freien intervalls bis zum rezidiv nicht zu und erfassen sptere rezidive nicht . 
 bedingt durch die kleinen bestrahlungsfeldgren , die strahlenqualitt und die hautlokalisation bei hufigem auftreten im kopf - halssowie oberen thoraxbereich ist die gonadenbelastung gering [ 11 , 17 ]  . 
schittkowski m , schneider h , gruschow k , ziegler , pj , guthoff r , fietkau r . 3 jahre erfahrung mit der niedrig dosierten fraktionierten perkutanen teletherapie bei subfoveolren neovaskularisationen . 
1 urban & vogel strahlentherapie und onkologie original article radiation therapy for chordoma and chondrosarcoma of the skull base and the cervical spine prognostic factors and patterns of failure georges nol1 , jean - louis habrand2 , eric jauffret1 , renaud de crevoisier2 , sygon dederke3 , hamid mammar1 , christine haie - mder2 , dominique pontvert4 , dominique hasboun3 , rgis ferrand1 , gilbert boisserie3 , anne beaudr2 , genevive gaboriaud4 , ferran guedea5 , lourdes petriz5 , jean - jacques mazeron1 , 3 background : prospective analysis of local tumor control , survival and treatment complications in 67 consecutive patients treated with fractionated photon and proton radiation for chordoma or chondrosarcoma of the base of the skull and the cervical spine . patients and methods : between december 1995 and january 2000 , 67 patients with a median age of 52 years ( range : 1485 years ) , were treated at the centre de protonthrapie dorsay ( cpo ) , france , using the 201 - mev proton beam , 49 for chordoma and 18 for chondrosarcoma . 
 results : within a median follow - up of 29 months ( range : 471 months ) , the 3 - year local control rates were 71% and 85% for chordomas and chondrosarcomas , respectively , and the 3 - year overall survival rates 88% and 75% , respectively . 
in univariate analysis , age 52 years at the time of radiotherapy ( p = 0.002 ) , maximum diameter < 45 mm ( p = 0.02 ) , and gtv < 28 ml ( p = 0.02 ) impacted positively on local control . 
 key words : proton therapy chordoma chondrosarcoma base of the skull cervical spine relapse strahlenther onkol 2003 ; 179 : 2418 doi 10.1007 / s00066 - 003 - 1065 - 5 strahlentherapie von chordomen und chondrosarkomen der schdelbasis und im bereich der halswirbelsule . 
 prognoseund risikofaktoren hintergrund : prospektive analyse der lokalen tumorkontrolle , berlebenszeit und behandlungsfolgen bei 67 patienten mit einem chordom oder chondrosarkom der schdelbasis und im bereich der halswirbelsule , die mit einer fraktionierten strahlentherapie mit protonen und photonen behandelt wurden . 
 1 centre de protonthrapie dorsay , orsay , france , 2 institut gustave roussy , villejuif , france , 3 groupe piti salptrire , ap - hp , paris , france , 4 institut curie , paris , france , 5 catalan institute of oncology , barcelona , spa received : june 21 , 2002 ; accepted : november 14 , 2002 strahlenther onkol 2003 no . 
proton therapy in chordomas and chondrosarcomas and patterns of relapse ergebnisse : im medianen nachbeobachtungszeitraum von 29 monaten ( 471 monate ) betrugen die lokale kontrollrate nach 3 jahren 71% bzw . 
in der univariaten analyse zeigte sich ein positiver einfluss auf die lokale kontrollrate bei einem alter 52 jahre zu bestrahlungsbeginn ( p = 0 , 002 ) , einem maximalen tumordurchmesser < 45 mm ( p = 0 , 02 ) und einem gtv < 28 ml ( p = 0 , 02 )  . 
distant failures have been reported anecdotically only , so that local outcome represents the major concern and the unique endpoint for long - term evaluation of treatment efficacy [ 10 ]  . 
surgery - related complications are frequently observed as well , and figures up to 40% have been reported [ 17 , 25 ]  . conventional radiotherapy ( rt ) with high - energy photons up to a dose of 5055 gy does not provide a high local control rate [ 4 , 13 , 19 ]  . 
from the literature , these tumors are considered radioresistant and require doses in excess of 60 gy . however , these dose levels cannot be safely delivered since they exceed the tolerance of most neurologic structures , especially brain stem and optic pathway [ 21 , 26 , 39 , 45 ]  . proton beam is an elegant way to improve dose gradient between gross tumor volume ( gtv ) and surrounding structures due to the unique distribution in the matter of the bragg peak . 
it has been commonly acknowledged that its superiority lies mainly in the absence of exit dose : sharp lateral and distal fall - off of the dose , within a few millimeters . 
another advantage is that the beams intensity can be modulated all along its path with high precision , which further increases dose gradient [ 30 , 31 , 35 , 37 ]  . 
 from recent literature , surgery followed by irradiation with charged particles have been advocated to be the gold standard in the management of patients with chordomas and chondrosarcomas of the skull base and cervical spine [ 4 , 29 , 35 , 36 , 46 ]  . 
 however , local failure cannot be completely overcome , and is possibly related with pathologic histologies , quality of surgery , timing of radiation , total dose , relative proportion of photons and protons , etc . 
 in this paper , we will update our previously reported series of patients treated at the centre de protonthrapie dorsay ( cpo ) , france , with special emphasis on pattern of failure and influence of prognostic factors [ 36 ]  . 
 patients and methods from december 1995 through january 2000 , 67 patients underwent fractionated proton rt at cpo either for chondrosarcoma or chordoma of the skull base or the cervical spine . 
two patients with chordoma were excluded from the analysis for the following reasons : one had previously undergone radiosurgery , and the other declined the proton part of treatment at the time of its initiation ; the photon part only delivered 22 cge . 
consequently , the actual evaluation concerns 65 patients with histologically proven chondrosarcomas or chordomas in which comprehensive serial imaging ( i.e. , magnetic resonance [ mr ] and computed tomography [ ct ] ) , as well as clinical data have been made available at the time of analysis or death of the patient . 
 symptoms presenting depended on tumor sites : first cranial nerves ( especially vith , in 32% ; and iiird in 23% ) in upper clivus or petroclival fissure , with or without involvement of the ipsilateral cavernous sinus ; rest of cranial nerves ( 25% ) , hydrocephalus ( 21% ) , or sensorimotor deficits ( 15% ) in other situations . 
 in 28 cases the tumor developed in the clivus , in 20 cases in the cavernous sinus , in ten cases in the petrous apex , and in 4 cases in several of these . 
final surgical resection was deemed macroscopically complete in nine patients ( 14% ; but all treated at time of relapse ) , and grossly incomplete in 50 ( 77% )  . 
tumor volume , at initiation of rt , ranged from 1 to 125 ml ( mean : 28 ml , median : 21 ml ) , which corresponded to 15100 mm in diameter . 
then , a 3 - d virtual simulation based on 3 - mm slice contrast ct and 1.5 - mm slice contrast mri was performed with the patient in a supine position . 
 total chordoma chondrosarcoma characteristics range mean median number of patients follow - up ( months ) f / m ratio last surgery 471 29 / 36 complete incomplete biopsy 14 - 85 age ( years ) at time range mean of rt median for recurrence for primary tumor 42 range mean median range mean median tumor size at time of rt ( ml ) maximum tumor diameter at time of rt ( mm ) tumor site base of the skull clivus sphenoidoclival petroclival miscellaneous cervical 1125 15100 20 / 27 1485 2125 15100 1768 1124 1593 target volume was delineated along with critical normal structures ( mainly brain stem , upper spinal cord , optic nerves , optic chiasm , and cochlea ) , based on the high - definition contrast - enhanced t1 - weighted mri and ct scan . 
the clinical target volume ( ctv ) included a 5to 10 - mm safety margin around the gtv , with possible minor adaptations according to the anatomic situation and presence of natural barriers . 
special attention was paid to the three patients with a cervical site , to achieve strict spinal immobilization : an occipitocervical titanium plaque was implanted by the neurosurgeon prior to simulation . 
proton dose will be expressed below in cobalt gray equivalent ( cge ) , which is defined as the physical proton dose multiplied by the relative biological effectiveness ( relative to cobalt - 60 ) of 1.1. 
proton therapy in chordomas and chondrosarcomas and patterns of relapse doses of critical structures : 55 cge maximum dose to the optic nerves and optic chiasm ; 64 cge to the anterior surface of the brain stem , and 53 cge to its center . 
in order to assess dose uniformity within the target and its appropriate coverage , a conformity index was employed , i.e. , the percent gtv encompassed by the 95% isodose line . 
 statistical methods the follow - up period after completion of treatment ranged from 4 to 71 months ( mean : 32 months , median : 29 months , only two patients being followed for < 12 months )  . 
prognostic factors were analyzed with respect to age , sex , extent of surgery ( complete vs incomplete vs biopsy ) , pathology ( chordoma vs chondrosarcoma ) , and radiotherapy parameters . 
 results overall survival and prognostic factors eight patients died , seven from relapse of the chordoma or chondrosarcoma and one from pulmonary embolism , without evidence of disease at the last radiologic follow - up . 
sex , quality of last surgery , tumor volumes at the time of radiotherapy , total irradiation dose , duration of radiotherapy , and timing of radiotherapy ( in advance or at time of recurrence ) were not significant . 
sex , quality of last surgery , total dose , timing , and protraction of irradiation were not signififollow - up ( months ) patients at risk chordoma chondrosarcoma figure 2 . 
two patients presented with an oculomotor impairment ( grade 3 , rtog ) , one patient experienced severe hearing loss requiring hearing aid ( grade 3 , rtog ) , and one developed a rapid bilateral loss of vision down to light perception only 8 months following treatment ( grade 4 , rtog )  . 
in multivariate analysis , only age remained predictive of local control ( p = 0.03 ) , with a cutoff value of 52 years : 2and 3 - year local control rate were 100% and 80% ( 7.4% ) for patients aged 52 years versus 94 % ( 6.1% ) and 68% ( 8.8% ) above this age . 
nonetheless , among ten evaluable failures , four originated in the ctv , outside the gtv , and four in the gtv , close to a shielded area , as well as in optic nerve and brain stem in two cases each . 
during the course of radiotherapy and 46 weeks following it , all patients developed the expected side effects , which consisted in some degrees of partial alopecia , erythema , headaches , and moderate hearing loss associated with external or medial otitis . 
all of these patients needed hormone replacement ( grade 2 , rtog )  . mild hearing loss not requiring hearing aid was observed in twelve patients ( grade 2 , rtog ; 18% )  . 
proton therapy in chordomas and chondrosarcomas and patterns of relapse ure following high radiation doses is poorly understood [ 23 ]  . in the literature , factors such as pathologic subtypes , age , sex , treatment modality ( surgery , radiotherapy , or both ) , and quality of resection , have been suspected to influence outcome . 
attempts have been made by several authors to correlate the pathologic types , or subtypes , with prognosis : chondrosarcomas appear to fare better than chordomas in most publications [ 8 , 25 , 29 , 35 ] , as does the chondroid subtype of chordoma compared with the nonchondroid one , yet less convincingly [ 28 ]  . 
no pathologic criterion has turned out to be prognostic in our own series , but this could have been biased by the small number of patients diagnosed with these supposedly more favorable features . 
our series does not include children < 14 years of age , but we are suspecting , in our own age range , a relationship between age and prognosis : in patients > 52 years , local control and survival are deteriorating significantly . 
halperin [ 27 ] suspected that hormonal or genetic factors could have played a role , although they acknowledged that sometimes , significant differences could show up just by chance . 
not surprisingly , the greater the number of resections , the higher the failure rate [ 8 , 24 , 25 , 34 ]  . this could be explained by increasing difficulty to achieve full resection in fibrotic tissues , or by increasing tumor size from one resection to the subsequent one ( see below )  . 
following surgery and / or conventional radiotherapy , it boosted to 3.56.5 years , although late recurrences are likely to further deteriorate these figures [ 40 , 41 ]  . 
the most frequent riks are cranial nerve palsies , affecting mainly the iiird , vth , and viith ( 80% ) [ 17 ] , cerebrospinal fluid leakage ( 30% ) , and meningitis ( 10% ) [ 25 ]  . 
 from a therapeutic standpoint , small lesions can be treated much more conveniently than larger ones : a uniform dose distribution can be achieved more easily [ 48 ] , and the likelihood of tight connections with several critical structures ( such as brain stem and optic chiasm ) can be reduced [ 5 , 29 ]  . 
if a substantial reduction in size cannot be achieved , some authors recommend the use of natural spacers , like autologous fat grafting , to push away these structures by few millimeters [ 18 ]  . we also point out that , when high - dose irradiation is contemplated , much efforts should be paid to remove , whenever feasible , any tumor extension lying along critical structures ( mainly optic nerves , chiasm , and brain stem )  . 
although protons can achieve a steeper dose gradient than photons ( approximately 1015% dose decrease per millimeter , in the fall - off region ) , they cannot overcome such physical constraints . 
this has sustained strong feelings that these tumors were highly radioresistant , with possible exceptions [ 2 , 14 , 15 , 20 , 22 , 24 , 40 ]  . 
the role of escalated doses has become critical with the introduction of ballistic innovations in radiotherapy , such as stereotactic monoor multifractionated irradiation , conformal photon therapy , and heavy charged particles . 
the reasons can be two - fold : higher effectiveness on tumor clonogens , and improved dose gradient between tumor boundaries and adjacent critical structures ( that minimizes underdosed areas )  . 
nonetheless , the us series show that 70 cge could be a safer choice in terms of local control [ 3 ] , whereas 80 cge could be more appropriate for higher - risk patients ( e.g. , females with spinal chordomas )  . 
one controversial issue remains the necessity or not to give most of the dose using protons alone , a policy favored in the usa , or to mix photons and protons , like we do . 
this was initially designed for trivial economic reasons ( the cost of one proton session being ten - fold that of a photon one ) , and for beams line availability . 
for the cns , it corresponds to about 55 gy for the critical structures mentioned above , a dose constraint that is readily achievable when photons are stopped around 45 gy , and protons administered for the remaining 22 cge . 
on the other hand , we acknowledge that there are situations in which the proton part should be favored , in order to decrease the integral dose to surrounding tissues . 
this is mainly the case in pediatric tumors in which doses > 20 gy to the full brain have been associated with demyelination processes , and 30 gy with cognitive impairments . 
we will also mention the possible role of high - let charged particles , such as carbon ion , that could add some biological advantages , such as improved oxygen effect on the tumor hypoxic component [ 19 , 20 ]  . 
 strahlentherapie und onkologie review article radiochemotherapy of malignant glioma in adults clinical experiences rolf - dieter kortmann1 , branislav jeremic1 , michael weller2 , ludwig plasswilm1 , michael bamberg1 background : standard treatment in patients with malignant glioma consists of surgery and postoperative radiotherapy . 
a high early recurrence rate , particularly in glioblastoma , has led to the investigation of additional chemotherapy . material and methods : recent results of radiochemotherapy published in the literature were reviewed with respect to outcome in phase ii and iii trials . 
while early prospective studies established adjuvant nitrosoureas , particularly bcnu , as suitable adjuvant to surgery and postoperative radiotherapy , further studies largely concentrated on combined chemotherapeutic protocols , mostly procarbazine , ccnu and vincristine ( pcv ) , which was shown to prolong survival in anaplastic astrocytoma . 
different modes of application and sequencing of radiotherapy and chemotherapy are presently actively investigated , but failed to substantially improve outcome . conclusions : therefore , search for newer and more effective drugs continues , as well as for optimal administration and sequencing , especially from the standpoint of accompanying acute and late toxicity . 
finally , recent endeavors focused on basic research such as angiogenesis , migration and invasion , or induction of cell differentiation , but these strategies are still away from broader clinical investigation . key words : brain tumors malignant glioma chemotherapy radiotherapy radiochemotherapy adults strahlenther onkol 2003 ; 179 : 21932 doi 10.1007 / s00066 - 003 - 1027 - y radiochemotherapie maligner gliome im erwachsenenalter . 
klinische erfahrungen hintergrund : die standardtherapie bei patienten mit malignen gliomen besteht aus operation und postoperativer bestrahlung . hohe frhe rckfallraten , insbesondere beim glioblastom , fhrten zur untersuchung zustzlicher chemotherapien . material und methodik : in der literatur verffentlichte ergebnisse der radiochemotherapie wurden unter bercksichtigung des therapeutischen ergebnisses von phase - iiund - iii - studien analysiert . 
whrend frhere prospektive studien die adjuvante gabe von nitrosoharnstoffen , insbesondere bcnu , als geeignete adjuvante therapie zu operation und strahlentherapie etablierten , konzentrierten sich folgende studienprotokolle auf kombinierte behandlungen , insbesondere procarbazin , ccnu und vincristin ( pcv ) , die ein verlngertes berleben bei anaplastischen astrozytomen zeigten . 
die neuere studie des mrc erbrachte jedoch keinen effekt einer adjuvanten behandlung mit pcv , weder bei grad - iiinoch grad - iv - gliomen . lediglich bei hochmalignen gliomen mit oligodendroglialer komponente besitzen zustzliche chemotherapien mglicherweise einen entscheidenden therapeutischen vorteil . 
alternative applikationsweisen und die reihenfolge von bestrahlung und chemotherapie werden derzeit untersucht , konnten jedoch keine substantielle verbesserung des therapeutischen ergebnisses erreichen . schlussfolgerungen : die suche nach neueren und effektiveren substanzen wird fortgesetzt , ebenso wie nach der optimalen applikationsweise und reihenfolge , vor allem vor dem hintergrund der begleitenden akuten maximalen nebenwirkungen und therapiefolgen . 
 schlsselwrter : hirntumoren maligne gliome chemotherapie radiotherapie radiochemotherapie erwachsenenalter 1 department for radiation oncology , and 2 department of neurology , university of tbingen , germany . received : march 25 , 2002 ; accepted : november 14 , 2002 strahlenther onkol 2003 no . 
radiochemotherapy of malignant glioma in adults introduction approximately half of all malignant brain tumors are gliomas . their malignancy is divided into four grades according to the who classification : grades i and ii are defined as low - grade malignancy , while grades iii and iv are defined as high - grade malignancy [ 61 ]  . 
high - grade ( iii and iv ) gliomas comprise approximately 75% of all gliomas and are the most aggressive variants which , if untreated , lead to fatal outcome in only a few weeks time . 
besides surgery , which is an important initial therapeutic measure in malignant glioma , postoperative external - beam radiotherapy including modern treatment techniques is considered the standard of treatment in these cases [ 1 , 3 , 48 , 119 ]  . 
today , the data from walker et al [ 116 ] are still valid which showed doubling of the median survival time in glioblastoma from 45 months to 912 months with the addition of postoperative radiotherapy . 
therefore , recent therapeutic endeavors concentrated on phase i / ii studies including optimized combinations of these treatment modalities as well as on optimized sequencing of their application ( before , during , or after radiotherapy ) in order to identify new pathways for improvement of survival in this highly aggressive disease . 
 efficacy of chemotherapy current aspects and future perspectives in the use of chemotherapy must be considered from the standpoint of pathobiological effects on tumor cells , to understand the effects of cytotoxic drugs leading to possible innovative approaches . 
particularities in microenvironment , such as angiogenesis typical of glioblastoma , and different partial oxygen pressures and ph values in and around the tumor area , make the transfer of data from in vitro sensitivity tests to varying in vivo conditions more difficult . 
highgrade gliomas , which responded to acnu in 30% of cases , showed a low level of dna alkyltransferase , while progressive tumors typically display high enzyme activity [ 82 ]  . 
additionally , there are different molecular - genetic properties regarding tumor development [ 123 ] cell cycle the growth fraction of the tumor represent parts of the tumors where proliferation occurs and thereby indicates responsivity to cell cyclespecific , cytotoxic agents . 
labeling index ( a proportion of cells found in s - phase [ synthesis of dna ] ) is approximately 510% in glioblastoma and < 1% in astrocytoma [ 46 , 47 ]  . 
even with cell loss by necrosis occurring in up to 85% of cases , tumor volume doubling can still occur within 56 weeks [ 47 ] blood - brain barrier poorly liposoluble , high - molecular or protein - bound substances cross the blood - brain barrier ( bbb ) only poorly . 
brain tumors always show local changes in the bbb with gaps in vascular endothelium , so - called open tight junctions [ 76 ] , allowing penetration of chemotherapeutic substances into tumor cell regions . 
the immediate neighborhood of normal - appearing brain on imaging contains microscopic tumor infiltration . in this area around the visible tumor , the bbb is intact tumor vascularity neovascularization is a typical feature of glioblastomas . 
they are characterized by an inefficient blood circulation , accompanied by regions of thrombosis and , therefore , insufficient oxygen and nutrient supply extracellular matrix , nutrition , oxygenation , ph value extracellular matrix is often pathologically changed . 
through regional differences in oxygen and nutrient supply , heterogeneity of the tumor microenvironment can occur [ 88 ] besides chemosensitivity of various tumor entities , another important aspect of efficacy of drugs / substances is their ability to reach the tumor cells . 
based on this assumption , penetrability into cns tissue and cerebrospinal fluid ( csf ) including also the appropriate application mode , play an important role in the delivery and efficacy of chemotherapy in malignant glioma . 
radiochemotherapy of malignant glioma in adults according to a recent analysis of two large us studies , only small subsets of patients had a marginal benefit from additional bcnu treatment , namely patients < 44 years and those with a simultaneously high karnofsky index [ 22 ]  . while the 18 - month survival for patients treated with radiotherapy alone was 38.4% , the corresponding outcome for those treated with additional chemotherapy was 44.9%. 
 procarbazine with procarbazine as a single agent , a response rate of 52% with a median duration of > 6 months was observed in early studies [ 124 ]  . 
in conjunction with ccnu and vincristine , an effective multiagent protocol was established ( pcv ) [ 53 , 72 ] which is now one of the most widely used adjuvant chemtherapy protocol in the usa and some european countries . 
having lower nephroand ototoxicity than cisplatin , carboplatin was tested in primary treatment settings . it showed no survival advantage over bcnu with a median survival time of 11 months versus 10.5 months after bcnu alone ( + radiotherapy ) [ 77 ]  . 
in other studies , up to 35% of objective remission rates were achieved with carboplatin despite of low blood - brain barrier penetrability [ 118 , 127 ] , but a benefit in recurrent disease was seen only in patients with anaplastic astrocytoma and not with glioblastoma [ 52 ]  . 
 multiagent chemotherapy multiagent chemotherapy offers the advantage of combining the efficacy of different single agents which have differing targets within the cell cycle , thereby achieving an additive effect . however , reports on the efficacy are controversial and do not allow reliable conclusions regarding the advantages of past and contemporary combinations . 
by contrast , in another study in which ccnu and vm - 26 or ccnu , vm - 26 and 5 - fu were compared with ccnu alone , an advantage for the combined protocol was found . 
however , the triplet combination was accompanied by considerable toxicity [ 63 ]  . in a large , randomized study of the mrc ( medical research council ) , pcv achieved no advantage over postoperative radiotherapy alone [ 81 ]  . 
the median survival time with radiotherapy alone was 9.5 months as compared to 10 months in the adjuvant pcv arage , karnofsky index , resection status , and who tumor grade ( iii vs iv ) had no effect on survival times ( table 3 )  . 
treatment was tolerated well and yielded a median survival of 16 months which led to its testing in a phase iii trial ( eortc study 26981 / 22981 )  . 
 preliminary evaluation of the recently closed randomized noa - 1 study ( noa : german neurooncologic working group ) showed that the combination of ara - c / acnu or vm - 26 / acnu simultaneously with radiotherapy and followed by six additional courses in a favorable subset of patients ( karnofsky index > 70 ) yielded a median survival time of almost 18 months , with no difference between the two treatment arms ( noa , unpublished )  . 
the agents included temozolomide , paclitaxel , vp - 16 , tamoxifen , fotemustine , carboplatin , procarbazine , acnu , 5 - fu , irinotecan , the known combination with pcv and others with varying combinations and dose prescriptions . 
 the combination of carboplatin with rmp - 7 , a bradykinin analog , which selectively opens the blood - brain barrier in the tumor area in an experimental model , yielded promising results in a phase ii study with a partial response rate in 30% of cases and a stable disease in 49% of cases [ 38 ]  . 
however , it remains questionable whether rmp - 7 will selectively open blood - tumor barriers compared with the blood - brain barrier in human patients , raising some toxicity concerns . 
 the topoisomerase i inhibitor topotecan is currently investigated in phase i / ii studies owing to its preclinical radiosensitizing properties [ 31 , 37 , 39 , 60 , 68 ]  . 
 radiotherapy / chemotherapy timing of administration of chemotherapy ( before radiotherapy , simultaneously with or after irradiation ) , the selection and the combination of single agents , the dose and the application mode ( e.g. , continuous infusion ) are substantial criteria of combined application of radiotherapy and chemotherapy , as it has been shown in other cns malignancies [ 65 ]  . 
 neoadjuvant therapy neoadjuvant treatment approaches ( postoperative chemotherapy , before irradiation ) offer the possibility of increasing the efficacy of chemotherapy without increasing the dose . surgery disrupts the blood - brain barrier allowing chemotherapeutic agents to reach tumor - bearing areas in higher concentrations . 
although paclitaxel , bcnu , cisplatin / carboplatin , and vp - 16 have shown acceptable toxicity in numerous recent phase i und ii studies , convincing survival advantages have not been achieved [ 27 , 40 , 42 , 102 ] ( table 4 )  . 
jeremic et al [ 55 ] applied two cycles of carboplatin and etoposide given before a more aggressive radiotherapeutic approach ( accelerated hyperfractionated radiotherapy , 54 gy total dose ) in 35 patients with glioblastoma and in ten patients with anaplastic astrocytoma , but with limited success . 
kirby et al [ 59 ] treated patients with newly diagnosed malignant glioma , particularly anaplastic oligodendroglioma , with four cycles of pcv , commencing radiotherapy at the time of progression . 
in our own experience , pcv given in eleven patients with anaplastic oligoastrocytoma or oligodendroglioma before radiotherapy achieved a median progression - free survival of more than 14 months [ 111 ]  . 
 substances with intrinsic cytotoxic effect , such as mitomycin c , cisplatin , carboplatin , bcnu , hydroxyurea , and topotecan , were examined in the past and recently , but did not yield an unequivocally positive effect . 
in the large rtog study , bcnu concurrently with and after hyperfractionated radiotherapy in escalating or accelerating schedules showed no advantage with a best median overall survival of 12.8 months [ 20 , 83 ]  . 
 the administration of cisplatin did not show a survival advantage and was only associated with the typical toxicity [ 36 ]  . similarly , carboplatin as a safer and more tolerable substance , with or without vp - 16 , did not improve outcome [ 56 , 70 ]  . 
jeremic et al [ 56 ] reported on accelerated hyperfractionated radiotherapy and concurrent weekly carboplatin / etoposide in a large phase ii study of 79 patients with either glioblastoma ( n = 61 ) or anaplastic astrocytoma ( n = 18 )  . 
the corresponding 2and 4 - year survival was 33% and 11% for all patients , 13% and 1.6% for patients with glioblastoma , and 100% and 44% for patients with anaplastic astrocytomas . 
likewise , the use of hydroxyurea showed no difference in survival time in compartemozolomid ison with other studies [ 95 ] , and also no difference was observed when it was added to bcnu , both given weekly during accelerated hyperfractionated radiotherapy [ 50 ]  . 
mean performance status was not deteriorated indicating that the treatment was well tolerated and did not have a negative impact on quality of life . in other series , the median survival time was , however , in the range of 911 months [ 31 , 37 , 60 ]  . 
effectiveness of topotecan as a single treatment approach in recurrent disease is dismal . the response rate in a series of 31 patients was 3% ( complete remission ) and 68% ( stable disease ) [ 78 ]  . 
the eortc is currently conducting a prospective randomized study with temozolomide given postoperatively concurrent to radiotherapy and afterwards as compared to radiotherapy alone ( eortc study 26981 / 22981 )  . 
however , through the changes of blood vessels caused by radiotherapeutic effects at peripheral arteries , longer diffusion times to surviving tumor cells may occur with consecutive decrease in efficacy . 
nitrosoureas are the most - used substances within this treatment approach and were investigated in large , randomized studies but without achieving a substantial survival advantage [ 29 ]  . 
also , no major breakthrough was seen after numerous phase i and ii studies with multiagent or intraarterial chemotherapy , not even when high - dose radiotherstrahlenther onkol 2003 no . 
 anaplastic glioma ( who grade iii ) anaplastic astrocytoma ( who grade iii ) in the majority of studies published to date on radiotherapy in malignant glioma , anaplastic gliomas were not differentiated from glioblastoma . 
treatment results were frequently described in terms of malignant glioma , so that judgment of prognosis according to histology was obscured or impossible . reliable , however , were the results of the rtog study 8302 , in which central pathology review was used [ 122 ]  . 
 anaplastic oligodendroglioma / oligoastrocytoma ( who grade iii ) allelic losses of chromosomes in tumors of oligodendroglial origin may exhibit increased chemosensitivities and better survival suggesting that in future molecular genetic analysis should be incorporated into patient management and clinical trials of low - grade gliomas [ 16 , 103 ]  . 
an additional astrocytic component may have a negative impact on outcome [ 58 ] , however other studies could not confirm this assumption [ 8 , 67 , 111 ]  . 
in one series , median survival time in patients with mixed oligoastrocytoma who grade iii was below 49.8 months as compared to 76 months in patients with pure anaplastic oligodendroglioma [ 58 ]  . 
jeremic et al found a trend toward improved survival for pure anaplastic oligodendroglioma as compared to mixed anaplastic oligodendroglioma ( 5 - year survival : 56% vs 40% ) [ 54 ]  . 
only two patients ( 8.2% ) experienced progressive disease , and the median progression - free survival in those patients who achieved a complete remission was 25.2 months [ 13 ]  . 
budr : bromodeoxyuridine ; cht : chemotherapy ; iudr : deoxyuridine ; mst : median survival time ; pcv : procarbazine , ccnu , vincristine ; hu : hydroxyurea ; rt : radiotherapy ; 6tg : 6 - thioguanine . 
radiochemotherapy of malignant glioma in adults tigated in randomized studies ( rtog 9402 before radiotherapy ; noa - 4 before radiotherapy postponing irradiation ; eortc 26951 after radiotherapy )  . 
in the framework of small series , intraarterial chemotherapy in malignant gliomas was accompanied by substantial toxicity [ 45 , 49 ] and led to shorter survival time in one study [ 106 ] , although another study with a limited patient number showed promising results for intraarterial neoadjuvant cisplatin / etoposide followed by standard radiotherapy [ 79 ]  . 
this treatment approach is based on the observation that tumor cell spheroids in body liquids can execute only up to ten cell divisions , if no links to vascular systems exist . 
numerous experimental results indicate the importance of these signal pathways in clinical situations : ( 1 ) human glioblastoma cell lines in vitro and experimental rat glioma cell lines in vitro and in vivo [ 89 ] produce substantial amounts of vegf ; ( 2 ) a receptor was extracted from tumor endothelium , but not from surrounding normal endothelium [ 89 , 90 ] ; and ( 3 ) inhibition of vegf activity by an endogenously encoded soluble receptor can occur . 
the induction of cell differentiation opens up a possibility of transforming a high - grade tumor into a low - grade tumor or even starting a process of cellular age transformation with terminal differentiation and apoptosis of tumor cells [ 75 ]  . 
the specificity of this approach relies on the systemic administration of a nontoxic prodrug which will be selectively converted into a toxic agent in cells transduced with the enzyme - encoding viral vector . 
clinical studies have focused on the activation of ganciclovir by thymidine kinase . a phase iii clinical trial including 248 patients with newly diagnosed glioblastoma failed to reveal an advantage of standard radiotherapy plus thymidine kinase / ganciclovir compared with radiotherapy alone [ 100 ]  . 
radiochemotherapy of malignant glioma in adults acute and late toxicity after radio - / chemotherapy common side effects of chemotherapy include nausea and vomiting , hematologic toxicity ( nitrosoureas ) , nephrotoxicity , ototoxicity ( cisplatin ) , polyneuropathy ( vincristine ) , flu - like symptoms ( ifn ) , pulmonary fibrosis ( nitrosoureas ) , and an impairment in the quality of life . 
 besides known acute toxicity of chemotherapy , cns - specific toxicity has to be considered , in particular the issue of interaction with radiotherapy leading to an additive or subadditive effect during combined radio - / chemotherapy . 
all changes caused by irradiation are likely to result from complex alterations within several functional cns compartments such as damage to vessel structures , deletion of oligodendrocyte progenitors and mature oligodendrocytes , deletion of neural stem cells and generalized alterations of cytokine expression , most likely to be interlinked with chemotherapy - induced changes [ 6 ]  . 
in four of 26 patients who received six cycles of pcv in recurrent disease after radiotherapy , focal neurologic deficits , neurocognitive impairments , pathologic eeg changes , and definitive characteristics of atrophy in mri were seen [ 94 ] , indicating also the potential of chemotherapy to cause not only acute , but also late toxicity . 
 conclusions despite postoperative radiotherapy , almost all patients with glioblastoma die from their disease 2 years after diagnosis . 3 decades of intensive investigation on additional chemotherapy did not substantially improve outcome . 
a meta - analysis of 16 randomized studies , in which chemotherapy in addition to irradiation was compared with radiotherapy alone , revealed only a marginal benefit for additional chemotherapy . 
unlike in the previous analysis , there was no evidence that the effect of chemotherapy differed in any group of patients defined by age , sex , histology , performance status , or extent of resection . the author concluded that this small but clear improvement in survival from chemotherapy should encourage further study of drug treatment of these tumors [ 110 ]  . 
various multiagent protocols such as pcv ( procarbazine , ccnu und vincristine ) , or nitrosoureas combined with other drugs ( table 4 ) , did not achieve a convincing improvement in survival . 
the mrc concluded that additionally chemotherapy should not be routinely given outside controlled trials and that it is ethically justified to continue with randomized trials including postoperative radiotherapy alone as the standard ar different ways of application and sequences of radio / chemotherapy were investigated without obtaining a convincing advantage of a particular timing . 
the modulation of blood - brain barrier penetrability by ionizing radiation has recently been discussed for the efficacy of newest agents , and is currently investigated in numerous phase i und ii studies such as topotecan as well as for classic chemotherapeutic agents . the blood - brain barrier will be opened and therefore increase drug concentration in the tumor area , particularly in the infiltration zone of glioma cells . 
consequently , constant plasma concentrations during the entire course of radiotherapy should be more favorable than only one or two applications in higher doses , thereby achieving a continuous effect of chemotherapy and possibly enhancing a radiosensitising effect . 
experimental treatment approaches including inhibition of angiogenesis , migration and invasion , and induction of cell differentiation should be further investigated in future studies . the ability of ionizing radiation to induce molecular - genetic modulation is not yet investigated in glioma cells and may play a substantial role in simultaneous administration of radio - / chemotherapy . 
the first published phase iii trial by buckner et al considering toxicity of chemotherapy and the impact on quality of life showed a good feasibility of these assessments and underlined the necessity of an adequate evaluation [ 12 , 39 ]  . 
 strahlentherapie und onkologie originalarbeit psychometrische eigenschaften des stress index radioonkologie ( siro ) ein neuer fragebogen zur erfassung der lebensqualitt bei patienten unter strahlentherapie susanne sehlen1 , hermann fahmller1 , peter herschbach2 , uelker aydemir3 , marcus lenk1 , eckhart dhmke1 hintergrund : die strahlentherapeutische behandlung von tumorpatienten ist hufig mit starken psychosozialen belastungen verbunden , fr deren erfassung es bisher keinen spezifischen fragebogen gibt . 
mit dem stress index radioonkologie ( siro ) , der auf den analyseergebnissen umfangreicher voruntersuchungen beruht , soll erstmals ein screening - instrument zur verfgung gestellt werden , mit dem die psychosozialen belastungen von tumorpatienten , einschlielich der durch strahlentherapie induzierten , erfasst werden knnen . 
 schlussfolgerungen : die fragebogen - vorform hat sich als reliabel , valide und praktikabel erwiesen und kann unverndert als neuer selbstberichts - fragebogen ( siro ) zur erfassung der psychosozialen belastung radioonkologischer patienten bernommen werden . schlsselwrter : radiotherapie psychosozialer stress lebensqualitt fragebogen psychoonkologie strahlenther onkol 2003 ; 179 : 2619 doi 10.1007 / s00066 - 003 - 1057 - 5 psychometric properties of the stress index radiooncology ( siro ) a new questionnaire measuring quality of life of cancer patients during radiotherapy purpose : in the course of radiotherapy oncological patients often experience considerable psychosocial distress . 
the stress index radiooncology ( siro ) , which is based upon the results of extensive preliminary studies , will be made available as a screening - instrument to facilitate measurement of psychosocial distress of cancer patients , including radiotherapy - induced distress . 
the aim of this study is , to psychometrically evaluate the preliminary version of the questionnaire , to transfer it to the final version ( siro ) and to gain information about the psychosocial distress of radiooncological patients at the beginning of radiotherapy . 
 1 klinik und poliklinik fr strahlentherapie , ludwig - maximilians - universitt , klinikum grohadern , mnchen , 2 institut und poliklinik fr psychosomatische medizin , psychotherapie und medizinische psychologie , technische universitt , mnchen , 3 institut fr biometrie und epidemiologie , ludwig - maximilians - universitt , klinikum grohadern , mnchen . 
psychometrische eigenschaften des siro ein neuer fragebogen results : the requirements for reliability ( table 3 ) and validity ( table 4 ) of the siro have either been fulfilled or exceeded . 
the highest distress value has been found in the scale psycho - physical distress , followed by the scale partnership problems , radiotherapeutical distress , and information deficits ( figure 1 )  . 
 conclusions : the preliminary version of the new self - report questionnaire ( siro ) has proven to be valid , reliable and practicable , and can therefore be taken unchanged to measure the psychosocial distress of radiooncological patients . 
 key words : radiotherapy psychosocial distress quality of life questionnaire psychooncology einleitung die diagnose einer tumorerkrankung sowie deren behandlung und behandlungsbedingte nebenwirkungen sind hufig mit starken psychosozialen belastungen verbunden , die sich z.t. 
dazu gefhrt , dass lebensqualittsthemen bei der konzeptualisierung von krebsbehandlungsprogrammen ein hoher stellenwert beigemessen wird [ 7 , 16 ]  . durch eine mittlerweile umfangreiche literatur konnte belegt werden , dass viel dazu beigetragen werden kann , dem psychosozial belasteten tumorpatienten bei der bewltigung seiner probleme zu helfen [ 3 , 26 , 31 , 32 ]  . 
whrend unbestritten ist , dass zahlreiche onkologische patienten in dieser belastungssituation untersttzung brauchen [ 17 , 18 , 41 ] , besteht hufig unklarheit darber , nach welchen indikationskriterien die individuelle behandlungsbedrftigkeit von tumorpatienten festgestellt werden kann [ 12 , 35 , 42 ]  . 
einige studien untersuchten die belastung radioonkologischer patienten mit krebsspezifischen fragebgen , die jedoch entweder die spezifischen aspekte der strahlentherapeutischen behandlung nicht miteinbezogen [ 7 , 17 , 19 , 24 ] , ausschlielich strahlentherapeutische belastungsbereiche erfassten , ohne auf die gesamtsituation der patienten einzugehen [ 25 , 27 ] , strker physische als psychische belastungen reflektierten [ 6 ] oder sich auf bestimmte diagnosegruppen beschrnkten [ 20 , 21 , 28 ]  . 
deshalb besteht ein bedarf nach einem messinstrument , mit dessen hilfe die gesamte belastungssituation von tumorpatienten unterschiedlicher diagnosen , einschlielich der situationsspezifischen aspekte der strahlentherapie , mglichst rasch , einfach und zuverlssig erfasst werden kann . 
 diesem bedarf nach einem messinstrument , das die gesamte belastungssituation radioonkologischer patienten bercksichtigt , wurde durch die entwicklung des neuen fragebogens stress index radioonkologie ( siro ) entsprochen , der neben krebsspezifischen auch strahlentherapiespezifische items enthlt , die zu der neuen skala strahlentherapeutische belastungen zusammengefasst wurden . 
ziel der vorliegenden untersuchung war erstens , die vorform des neuen fragebogens mithilfe einer reprsentativen stichprobe durch eine itemanalyse , faktorenanalytische skalenbildung und statistische berprfung der gtekriterien ( reliabilitt , validitt ) in die endgltige fragebogenversion ( siro ) zu berfhren . zweitens sollten durch die analyse der patientendaten informationen ber das belastungsprofil stationrer bzw . 
 patienten und methoden zwischen september und dezember 2001 wurden 104 tumorpatienten mit unterschiedlichen diagnosen , die sich am beginn einer strahlentherapie befanden , in der klinik und poliklinik fr strahlentherapie des klinikums grohadern der ludwig - maximilians - universitt mnchen mit selbsteinschtzungsfragebgen untersucht . 
voraussetzung fr die teilnahme war ein mindestalter von 18 und ein hchstalter von 85 jahren , ein karnofsky - index von 50 sowie die sprachliche und kognitive fhigkeit des patienten , die fragebgen inhaltlich zu erfassen . 
von den verweigerern hatten fnf einen zu niedrigen karnofsky - index , drei verfgten ber unzureichende kenntnisse der deutschen sprache und einer lehnte ab , weil er sich mit der momentanen lebenssituation berfordert fhlte . 
die stichprobe setzte sich mehrheitlich aus patienten mit tumoren im kopf - hals - bereich ( 21 ) und gastrointestinaltrakt ( 21 ) zusammen , gefolgt von lymphomen ( 18 ) , strahlenther onkol 2003 no . 
30 - mintigen gesprchen wurde die belastung der patienten durch einschrnkungen in der leistungsfhigkeit , emotionale und strahlentherapeutische belastungen , die belastung infolge von partnerschaftlichen problemen sowie durch defizite in der information und psychosozialen untersttzung von einer strahlentherapeutin bzw . einem psychologen exploriert und zu einer einschtzung der gesamtbelastung zusammengefasst . 
 entwicklung des neuen fragebogens siro fr die fragebogen - vorform wurde eine maximale itemzahl von 24 festgelegt , die zusammen mit der bearbeitungsinstruktion auf einer din - a4 - seite platz finden konnten . 
die 24 items der fragebogen - vorform wurden aus zwei quellen gewonnen : 19 krankheitsspezifische items wurden primr aus der analyse empirischer daten abgeleitet , die mit dem fragebogen zur belastung von krebspatienten ( fbk [ 18 ] ) , der self - rating depression scale ( sds [ 44 ] ) , und der functional assessment of cancer treatment general ( fact - g [ 5 ] ) whrend einer lebensqualittsstudie mit 732 patienten erhoben wurden [ 33 , 35 ]  . 
 item item und skalen mittlere standardbelastung abweichung treffend % zu datenanalyse die statistische auswertung der patientendaten wurde mit dem programm spss 10 , 0 fr windows durchgefhrt . die psychometrische berprfung erfolgte durch eine faktorenanalyse ( hauptkomponentenanalyse , obliminrotation mit kaiser - normalisierung ) , reliabilittsanalysen ( cronbachs alpha ) , deskriptive statistiken , produktmoment - korrelationen , t - tests und anova . 
 ergebnisse skalenbildung die 24 items der fragebogen - vorform wurden von 30 , 8% bis 94 , 2% der patienten als fr sie zutreffend beantwortet ( tabelle 2 )  . 
aufgrund der zufrieden stellenden bis sehr guten relevanz der belastungsbeschreibungen , die im bereich vergleichbarer studien [ 17 , 39 ] liegen , musste keines der items aus dem fragebogen herausgenommen werden . 
zur bildung homogener subskalen wurde mit den 24 items eine faktorenanalyse ( hauptkomponentenanalyse mit schiefwinkliger faktorenrotation ) durchgefhrt , die eine struktur von vier faktoren untersttzte , die als folgende vier subskalen bezeichnet wurden : 1 . 
psychometrische eigenschaften des siro ein neuer fragebogen inhaltliche validitt aufgrund der theoretischen konzeption des zu messenden konstruktes ( psychosoziale belastung durch erkrankung und radiotherapie ) und der art und entwicklung der einzelitems kann der siro inhaltliche validitt fr sich in anspruch nehmen . 
 insgesamt werden diese befunde als indikatoren fr die die konvergente validitt der siro - vorform wurde zustzlich durch einen vergleich der selbsteinschtzung der patienten mit der fremdeinschtzung durch die interviewer in bezug auf die psychosoziale gesamtbelastung berprft [ 10 ]  . die produkt - moment - korrelation beider einschtzungen ist statistisch signifikant ( r = 0 , 53 , p = 0 , 009 )  . 
 diskriminante validitt zur abschtzung der diskriminanten validitt wurde die hypothese berprft , dass patienten mit einem fortgeschritteneren krankheitsstadium ( t3 - t4 , n2 - n3 , m1 ) hher belastet sind als solche mit einem niedrigeren krankheitsstadium ( t1t2 , n0n1 , m0 )  . 
im sinne hoher diskriminanter validitt ist der fragebogen in der lage , patienten mit unterschiedlichen krankheitsstadien hinsichtlich der belastung in den anzahl skalen items mittelwert cronbachs alpha ( sd ) konvergente validitt des siro gewertet . 
 skalen psychophysische belastungen ( p = 0 , 017 ) , strahlentherapeutische belastungen ( p = 0 , 029 ) , informationsdefizite ( p = 0 , 032 ) und der gesamtbelastungsskala ( p = 0 , 003 ) zu unterscheiden . 
zum ausfllen des fragebogens werden zwischen 5 und 10 minuten bentigt . die hohe praktikabilitt des fragebogens ist fr die indikationsstellung psychosozialer behandlungsbedrftigkeit im klinischen alltag wie auch in der klinischen forschung von vorteil . 
 belastungsprofil der untersuchten patienten auf einzelitemebene des siro waren die tumorpatienten zu beginn der strahlentherapie am strksten dadurch belastet , dass sie in haushalt / beruf weniger leistungsfhig / belastbar sind , hobbys weniger nachgehen knnen , bei ttigkeiten sich hufiger ausruhen mssen , gefolgt von der angst vor einer ausweitung / ausbreitung der erkrankung , vor nebenwirkungen der strahlentherapie und der angst , hilflos und abhngig zu se auf skalenebene waren die patienten am strksten durch psychophysische beeintrchtigungen belastet , gefolgt von partnerschaftlichen problemen und der strahlentherapeutischen behandlung . 
 innerhalb der verschiedenen diagnosegruppen wiesen patienten mit einem bronchialkarzinom ( m = 2 , 28 / sd = 0 , 74 ) die hchste , solche mit einem urogenitaltumor ( m = 0 , 64 / sd = 0 , 93 ) die niedrigste gesamtbelastung auf . 
auch auf skalenebene wider : in der skala partnerschaftliche probleme waren patienten mit einem bronchialkarzinom besonders stark belastet ( m = 3 , 75 / sd = 0 , 87 )  . 
in zahlreichen studien wurde auf die notwendigkeit hingewiesen , hoch belasteten patienten zu einem mglichst frhen zeitpunkt geeignete interventionen anzubieten , um sie in dieser schwierigen situation zur verbesserung ihrer lebensqualitt zu untersttzen [ 8 , 10 , 15 , 37 , 38 ]  . es besteht jedoch oft unklarheit darber , nach welchen indikationskriterien die individuelle behandlungsbedrftigkeit von tumorpatienten festgestellt werden soll . 
um die indikationsstellung zu erleichtern , wird die entwicklung von geeigneten screening - fragebgen fr notwendig erachtet , weil die durchfhrung psychiatrischer interviews zu zeitaufwendig und deshalb im klinischen alltag bei der hohen anzahl von patienten konomisch kaum durchfhrbar ist [ 33 , 35 ]  . 
unangemessen scheint darber hinaus , die belastung von tumorpatienten , die aufgrund ihrer lebenssituation hohen stressfaktoren ausgesetzt sind , vorwiegend aus dem blickwinkel psychopathologischen nomenklatur zu erfassen [ 23 ]  . 
deshalb war das vorrangige ziel dieser arbeit , ein messinstrument zu entwickeln , mit dem die belastungssituation von tumorpatienten unterschiedlicher diagnosen unter einbeziehung von spezifischen strahlentherapieinduzierten belastungen mglichst rasch , einfach , zuverlssig und valide erfasst werden kann . 
aufgrund der neuen skala strahlentherapeutische belastungen , die in der faktorenanalyse als eigenstndige skala ausgewiesen wurde , konnten zustzlich zu den krebsspezifischen belastungen informationen ber die strahlentherapierelevanten belastungen von tumorpatienten gewonnen werden . 
aufgrund seiner multidimensionalitt bietet der siro qualitative hinweise zur art der seelischen belastung , sodass sich auch fr die behandelnden rzte selbst wichtige orientierungshilfen fr den eigenen adquaten umgang mit diesen patienten ergeben . 
eine einschrnkung der reprsentativitt der ergebnisse kann dennoch nicht ausgeschlossen werden , weil die gruppe der verweigerer im bildungsund karnofsky - status im vergleich zu den teilnehmenden patienten einen signifikanten unterschied aufwies . 
unerwartet war , dass die leistungsminderungen und die daraus resultierenden einschrnkungen in den sozialen rollenfunktionen ( familie , beruf , freizeit ) von den patienten belastender erlebt wurden als z.b. 
in den skalen des neuen fragebogens spiegelt sich dieses ergebnis verstrkt wider , was darauf zurckzufhren ist , dass in den neuen fragebogen vor allem items aufgenommen wurden , die bereiche hoher psychosozialer belastung der patienten reprsentieren . 
 [ 34 ] zeigten , dass die lebensqualitt von tumorpatienten whrend der strahlentherapie und 6 wochen danach in allen subskalen signifikant abnahdieses ergebnis unterstreicht die notwendigkeit , hoch belastete patienten mglichst schon zu beginn einer strahlentherapie zu identifizieren , um ihnen eine geeignete psychosoziale untersttzung anbieten zu knnen . 
bei den halb standardisierten interviews , die mit 25 der patienten durchgefhrt wurden , zeigte sich , dass die ngste in bezug auf nebenwirkungen der strahlentherapie auch durch die aufklrungsgesprche ausgelst wurden , bei denen ein teil der patienten aufgrund von informationen ber den umfang mglicher nebenwirkungen verunsichert wurde . 
der bestrahlungssituation ausgelst wurden , am strksten bei den ersten bestrahlungen waren und sich danach reduzierten ngste , die durch entsprechendes anschauungsmaterial ( fotos , modell etc . ) leicht verringert werden knnen . 
die patientenzahlen innerhalb der diagnosegruppen sind fr eine sinnvolle interpretation der belastungsunterschiede jedoch zu kle schlussfolgerungen die psychometrische berprfung des neuen fragebogens zeigte , dass der siro eine hohe reliabilitt ( cronbachs alpha ) in den subskalen ( 0 , 780 , 87 ) und in der gesamtbelastungsskala ( 0 , 90 ) aufweist . 
die festlegung des schwellenwerts sollte nicht absolut oder theoretisch erfolgen , denn es bestnde dann die gefahr , dass bei einem zu geringen wert die zahl der bedrftigen patienten nicht betreut werden knnte . 
der schwellenwert wird somit immer wieder flexibel an die ressourcen der jeweiligen einrichtung anzupassen se in vorbereitung ist eine multizentrische studie an einem groen patientenkollektiv , in der die kritischen belastungsschwellenwerte des siro ermittelt werden . 
4 urban & vogel strahlentherapie und onkologie aktuelles forum die behandlung des zentralen neurozytoms : eine metaanalyse basierend auf den daten von 358 patienten dirk rades1 , fabian fehlauer1 , steven schild2 , karin lamszus3 , winfried alberti1 hintergrund : das zentrale neurozytom wird als seltene benigne lsion des zentralen nervensystems beschrieben . 
diese retrospektive analyse vergleicht vier therapien bezglich lokaler kontrolle und gesamtberleben : alleinige komplette resektion ( kr ) , komplette resektion plus strahlentherapie ( kr - rt ) , alleinige inkomplette resektion ( ir ) und inkomplette resektion plus strahlentherapie ( ir - rt )  . 
 material und methoden : die seit 1982 in der literatur verffentlichten flle wurden hinsichtlich folgender parameter untersucht : alter , geschlecht , ausma der resektion , vorliegen eines atypischen neurozytoms , lokale kontrolle und gesamtberleben ( follow - up mindestens 12 monate )  . 
die 5 - jahres - berlebensraten betrugen 99 , 2% und 86 , 1% . schlussfolgerungen : die komplette resektion ist bei der behandlung des zentralen neurozytoms deutlich effektiver als die inkomplette resektion . 
ob die patienten nach einer kompletten resektion von einer strahlentherapie profitieren , bleibt unklar . nach inkompletter resektion fhrt die strahlentherapie zu einer signifikanten verbesserung der lokalen kontrolle , nicht aber des gesamtberlebens . schlsselwrter : zentrales neurozytom behandlungsoptionen metaanalyse strahlenther onkol 2003 ; 179 : 2138 doi 10.1007 / s00066 - 003 - 1061 - 9 treatment for central neurocytoma : a meta - analysis based on the data of 358 patients background : central neurocytomas are described as uncommon benign cns lesions . 
this retrospective analysis compares four therapies for local control and overall survival : complete resection alone ( kr ) , complete resection plus radiotherapy ( kr - rt ) , incomplete resection alone ( ir ) , and incomplete resection plus radiotherapy ( itr - rt )  . 
 material and methods : the cases published in the literature since 1982 were reviewed for age , gender , extent of resection , atypical neurocytoma , radiotherapy , local control , and overall survival ( minimum follow - up 12 months )  . 
statistical analysis was performed with the kaplan - meier analysis and the log - rank test . results : complete data were obtained from 358 patients ( kr 118 , kr - rt 35 , ir 91 , ir - rt 114 )  . 
behandlung des zentralen neurozytoms eine metaanalyse conclusions : complete resection is much more effective for the treatment of central neurocytoma than incomplete resection . after complete resection the additional benefit of postoperative radiotherapy remains unclear . 
als ursache hierfr sind die metastatisch bedingte rckenmarkkompression , hirneigene tumoren , hirnmetastasen oder die meningeosis carcinomatosa zu nennen [ 3 , 10 , 12 , 13 , 16 , 20 , 23 , 34 ]  . 
extraventrikulre manifestationen , insbesondere spinale tumoren , sind selten [ 2 , 17 , 26 , 27 ]  . makroskopisch erscheint das zentrale neurozytom als graue , teilweise kalzifizierte masse . 
zentrale neurozytome weisen im allgemeinen eine geringe proliferative aktivitt mit einem ki67 - index < 5% und einem mib - 1 - index von 0 , 1%5% auf [ 2 , 9 , 18 , 19 , 24 , 29 , 31 , 32 ]  . 
in der magnetresonanztomographie zeigt sich im vergleich zum kortex eine gleiche oder gering erhhte signalintensitt in der t1und der t2 - wichtung . die gabe von gadolinium - dtpa fhrt zu einem geringen homogenen enhancement . 
die vorliegende retrospektive analyse vergleicht vier verschiedene therapieregimes im hinblick auf die lokale kontrolle und das gesamtberleben : alleinige komplette resektion ( kr ) , komplette resektion plus strahlentherapie ( kr - rt ) , alleinige inkomplette resektion ( ir ) und inkomplette resektion plus strahlentherapie ( ir - rt )  . 
 material und methoden die seit 1982 ber das zentrale neurozytom verffentlichten publikationen wurden im hinblick auf folgende parameter untersucht : alter , geschlecht , ausma der resektion ( komplett , inkomplett ) und deren besttigung , vorliegen eines atypischen neurozytoms , strahlentherapie , lokale kontrolle , gesamtberleben und follow - up . 
als atypisch wurden neurozytome bei einem mib - 1 - index > 5% , bei vorliegen histologischer kriterien eines anaplastischen tumors ( erhhte mitoserate , nekrosen ) oder bei einem klinisch malignen verlauf ( kraniospinale disseminierung ) definiert . 
 diskussion die vorliegende retrospektive analyse wurde durchgefhrt , um das optimale therapieregime bei der behandlung des zentralen neurozytoms zu definieren . die vier in der literatur am hufigsten beschriebenen therapien wurden im hinblick auf die lokale kontrolle und das gesamtberleben miteinander verglichen . 
 95% ( 108 / 114 ) die vorliegende analyse basiert auf heterogenen daten von patienten , die in zahlreichen lndern zu verschiedenen zeiten ( 19822001 ) mit unterschiedlichen techniken behandelt wurden [ 2 , 7 , 9 , 11 , 1719 , 24 , 26 , 27 , 29 , 3133 , 35 ]  . 
 die mediane zeit bis zum auftreten eines rezidivs betrug nach kr 36 monate ( bereich : 4128 monate ) , nach krrt 39 monate ( 2454 monate ) , nach ir 21 monate ( 1216 monate ) und nach ir - rt 32 monate ( 2276 monate )  . 
war die dosis pro fraktion ungleich 2 , 0 gy , wurde die eqd2 ( equivalent dose in 2 gy fractions ) mithilfe des linear - quadratischen modells ( / ( cid : 2 ) = 3 gy ) berechnet [ 4 , 14 , 28 ]  . 
p - werte fr den vergleich der vier untergruppen im hinblick auf die lokale kontrolle und das gesamtberleben mittels log - ranktest : alleinige komplette resektion ( kr ) , komplette resektion plus strahlentherapie ( kr - rt ) , alleinige inkomplette resektion ( ir ) , inkomplette resektion plus strahlentherapie ( ir - rt )  . 
p - values for the comparison of the four subgroups for local control and overall survival using the log - rank test : complete resection alone ( kr ) , complete resection plus radiotherapy ( kr - rt ) , incomplete resection alone ( ir ) , incomplete resection plus radiotherapy ( ir - rt )  . 
die gesamtrezidivrate betrug 59% ( 19 / 32 ) bei den patienten mit einem atypischen neurozytom versus 20% ( 65 / 326 ) bei den brigen patienten , die gesamtmortalitt 34% ( 11 / 32 ) versus 3% ( 11 / 326 )  . 
fr die vergleiche ir versus kr , ir versus kr - rt und ir versus ir - rt ergaben sich die p - werte 0 , 000 , 0 , 004 sowie 0 , 000 und waren somit den werten in tabelle 3 vergleichbar . bezglich der operationsbedingten toxizitt wurden keine unterschiede nach kompletter versus inkompletter resektion berichtet . 
dies kann durch die geringe anzahl von patienten in der gruppe kr - rt ( n = 35 ) bedingt sedie ergebnisse knnen auch dahingehend interpretiert werden , dass nach einer kompletten resektion durch eine strahlentherapie abbildung 2 . 
was die spttoxizitt der strahlentherapie anbelangt , so ist nach einer konventionell fraktionierten gesamtdosis von 60 gy ( appliziert auf ein drittel von grohirn oder hirnstamm ) innerhalb von 5 jahren bei 5% der patienten mit einer hirnnekrose zu rechnen ( toleranzdosis 5 / 5 ) [ 8 ]  . 
da es sich beim neurozytom um einen benignen tumor handelt , sollte die dosis so niedrig wie mglich se demzufolge empfehlen wir nach dem derzeitigen wissen eine gesamtdosis von 54 gy ( dosis pro fraktion 2 gy )  . 
 korrespondenzadresse dirk rades abteilung fr strahlentherapie und radioonkologie universittsklinikum hamburg - eppendorf martinistrae 52 20246 hamburg deutschland telefon : ( + + 49 / 40 ) 42803 - 6140 , fax - 2846 e - mail : rades.dirk@gmx.net strahlenther onkol 2003 no . 
bale2 , roy moncayo3 , karl seydl1 , thomas trieb2 , wilhelm eisner4 , johannes burtscher4 , eveline donnemiller3 , gnther stockhammer5 , peter lukas1 purpose : to present a simple and precise method of combining functional information of cranial spect and pet images with ct and mri , in any combination . 
this frame is reproducibly connected to the vbh vacuum mouthpiece , granting objectively identical repositioning of the frame with respect to the craniuusing these markers , the desired 3 - d imaging modalities can then be manually or automatically registered . 
this information can be used for diagnosis , treatment planning , and evaluation of follow - up , while the same vacuum mouthpiece allows precisely reproducible stereotactic head fixation during radiotherapy . 
 conclusion : this technique is a simple , objective and accurate registration tool to combine diagnosis , treatment planning , treatment , and follow - up , all via an individualized vacuum mouthpiece . 
 ergebnisse : 244 ctund mrt - datenstze von 49 patienten wurden mit einem durchschnittlichen root square mean error ( rsme ) von 0 , 9 mm berlagert , whrend an 18 patienten 64 ct - spect - fusionen zu einem rsme von 1 , 4 und 40 ct - pet - datenstze von acht patienten zu 1 , 3 mm fusioniert wurden . 
 * presented at : degro / gro / dgmp , munich , germany , october 2000 ( elekta poster award for functional imaging and treatment planning ) , astro 2001 , san francisco , ca , usa , and rsna 2001 , chicago , il , usa . received : april 8 , 2002 ; accepted : october 21 , 2002 strahlenther onkol 2003 no . 
multimodality cranial image fusion introduction it is now general practice to incorporate both ct and mri images into the treatment - planning process , since ct images , although to date largely inexpendable due to their role in dose planning and excellent spatial resolution , will often not provide adequate imaging of critical soft tissue structures such as the optic chiasm or tumors themselves . 
mr images on the other hand , although subject to distortion artifacts [ 8 ] , often provide the required resolution leading to improvements in target volume definition [ 23 ]  . 
the functional information offered by spect / pet images can also improve understanding of tumor size , location and activity , possibly also leading to changes of actual treatment volumes [ 911 ]  . 
 a general problem , however , when comparing any two sets of one patients images without prior fusion , is that these studies are generally not performed with rigorous attention paid to identical patient positioning or scanner protocols . thus , the slices are rarely in the same anatomic plane . 
in addition , differences in scanner characteristics and protocols ( slice thickness , spacing , pixel size , matrix size , etc . ) hardly allow correlation of features in separate scans with 3 - d accuracy < 5 mm [ 21 ]  . 
 we present the application of a noninvasive , simple and fast method of image registration allowing precise and objective assignment of functional information from spect and / or pet to ct / mri , based on external landmarks as reference points . 
their connection to the rigid upper palate via the same vacuum mouthpiece , used for noninvasive head fixation in ( stereotactic ) radiotherapy [ 25 ] , guarantees their identical relationship to the cranial anatomy . 
 material and methods the system , consisting of the sip - lab innsbruck frame , reproducibly connected to the vogele - bale - hohner ( vbh ) vacuum mouthpiece ( both medical intelligence gmbh , schwabmnchen , germany ) , and the methodology of image registration have been previously described [ 3 ]  . 
 in short , spherical external markers can be placed in precise relation to cranial anatomy and made visible in all imaging modalities via a hockey mask - like frame , in contact with the cranium only via a vacuum mouthpiece ( figure 1 )  . 
a vacuum pump ( not visible ) , connected via a vacuum hose ( 2 ) to this mouthpiece creates the required negative pressure which only builds if the mouthpiece is seated against the upper palate perfectly . 
thus , at least four ( up to twelve ) reference points ( 3 ) are in precise relation to cranial anatomy and , since they are visible in all modalities , can then be correlated to each other in the registration process . 
dieser befindet sich dank eines vakuumzahnabdrucks ( 1 ) , der ber einen schlauch ( 2 ) an eine vakuumpumpe angeschlossen ist ( nicht sichtbar ) , in exakter relation zum schdel . 
das vakuum baut sich nur bei absolut korrektem sitz des zahnabdrucks auf . zur bildregistrierung werden mindestens vier ( bis zu zwlf ) referenzmarker ( 3 ) jedes datensatzes miteinander korreliert . 
when manually registering two data sets , registration accuracy is calculated by the software as the root square mean error ( rsme ) which is the mean distance of the respective frame reference points in the two data sets . 
this assumption is , however , granted by the fact that the frame is reproducibly connected to the vacuum mouthpiece , which itself is in reliable relation to the cranium thanks to the negative pressure acting on the hard palate [ 18 ]  . 
 up to ten further previously registered studies , be it ct , mri or functional imaging studies ( spect / pet ) , can then be uploaded and compared to each other individually . 
the threshold levels of all image sets as well as the weighting of one modality over the other can be adjusted via mouse - controlled sliders , allowing quick visualization of any region in any magnification in three planes ( axial , coronal , sagittal )  . 
 results vacuum mouthpiece production , as a simple , one - time procedure , takes 1020 minside the scanner room , hose connection to the ( portable ) vacuum pump , vacuum mouthpiece insertion , and mounting of the sip frame adds an additional 12 min to image acquisition time . it must be emphasized that there is no need for either reproducible positioning of the head or head fixation in any scanner . 
using this method , correlation of functional with anatomic data is routinely performed at our hospital where to date , well over 100 patients have received radiation treatment of cranial tumors fixated via the vacuum mouthpiece . 
am rechten sehnerv ( seit jahren erblindet ) zeigt sich eine auffllige verdickung , der linke sehnerv , obwohl histologisch befallen und klinisch fast erblindet , ist unauffllig ( pfeil in der axialen ansicht )  . 
bildschirmansicht der prtherapeutischen ct - 99mtc - octreotid - spect - fusion ; intensive aktivitt nicht nur ber dem rechten , sondern auch ber dem linken auge . ebenfalls sichtbar sind zwei ctund spect - referenzmarker am rahmen . only in radiotherapy treatment planning and followup ( as required , i.e. , when unclear whether tumor growth or different slicing / active tumor vs necrosis ) but also , if available , in the preceding diagnostic procedures and neurosurgical interventions [ 1 ]  . 
if all follow - up studies are included , a total of 311 registrations were performed at our department with this method to date ( mean of 6.7 registrations per patient )  . 
 a 52 - year - old woman presented with a 2 - year history of complete blindness on the right and rapidly progressing loss of vision of the left eye . 
a right temporal surgical approach exposing both optic nerves to the chiasm showed an atrophic right optic nerve and an uninvolved chiasbiopsy of the visible tumor on the right and the arachnoid sheath of the left optic nerve revealed a bilateral psammomatous meningioma . 
the identical slice 4 weeks after radiotherapy ; no more abnormal activity over left optic nerve ( correlating with clinical response of regained [ 80% ] vision ) , while that over the right optic nerve ( outside the 50% isodose line ) remained unchanged . 
99mtc - tricinehynic - d - phe1 - tyr3 - octreotide spect ( 4 h post - injection ) [ 6 ] superposition then confirmed the diagnosis of bilateral meningioma , showing intense somatostatin receptor activity over the right and , to a slightly lesser degree , the left optic nerve ( figure 3a )  . 
the intraorbital aspect of the left optic nerve up to the optic chiasm was delineated as gross tumor volume ( gtv ) , with 5 mm added as planning treatment volume ( ptv ) as defined by the international commission on radiation units and measurements [ 15 ]  . 
while followup ct and mri ( again with vacuum mouthpiece and sip frame ) showed no discernible difference to the pretreatment status , 99mtc - octreotide spect showed an impressive response to treatment with no more abnormal activity in the left retrobulbar region ( gtv ) corresponding to the clinical improvement ( figure 3b )  . 
the right retrobulbar activity ( outside the ptv ) , on the other hand , remained virtually unchanged ( the activity seen in the pituitary and nasal cavity regions is physiological [ 20 ] )  . 
especially for some types of functional tracers ( i.e. , 201tl chloride ) where anatomic structures ( such as cranial contours ) are hardly discernible , assigning an anatomic correlate to focal uptake can be a guessing game . 
a reliable method of registration with ct or mri to accurately define localization would be of high diagnostic utility . while a detailed discussion of all fusion methods far exceeds the scope of this article , excellent review articles and books on medical image registration are available [ 12 , 17 ]  . 
table 3 gives a general overview of the different methods , usually based on either intrinsic ( anatomic ) features , extrinsic features or non - imagebased ( calibrated coordinate ) systems . 
 accuracy using contours for registration ( such as the head and hat [ 21 ] or the iterative closest point algorithm ) may yield gross misregistrations , although the contours align perfectly due to identical axes of symmetry . 
our own experience is in accordance with that of other groups [ 7 ] in that such anatomic landmarks can be coregistered to about 25 mm for ct and mri . 
this identical relationship can be granted by invasive frames , implanted bone markers , thermoplastic masks [ 14 ] , skin markers or , as in ours , via a noninvasive frame reproducibly attached to a vacuum mouthpiece . 
 when using skin markers , skin shift was the factor causing most inaccuracies ( errors in the direction perpendicular to the skin surface were generally much smaller than those in other directions ) [ 22 ]  . 
the accuracy of all mask - based systems is , however , limited by possible distortions of the underlying sk the patient would also need to be fixated for each imaging procedure . 
multimodality cranial image fusion tively in identical relationship to the cranium due to the vacuum of the mouthpiece , irrespective of patient compliance . identical positioning or fixation of the head with respect to the imaging plane is not necessary , as the markers define orientation in the 3 - d data set . 
this can be and has been performed in a variety of clinical situations at our institution with an individually formed vacuum mattress rigidly connected to the base plate of the head fixation system , in addition to the sip frame as described . the reason the sip frame curves around the head , thus spreading the markers as evenly as possible over a large surface with the most posterior markers located behind the ear ( figure 1 ) , is to minimize the distance from the marker centroid to a point of interest ( isocenter ) in the posterior ( occipital ) regions of the head . 
this is of relevance , because the localization error increases not only as a function of marker / fiducial localization error ( rsme ) but also as the distance from the marker centroid to the point of interest increases [ 19 , 26 ]  . the frame also fits into the head coil of mr scanners , thus decreasing effects of image distortions [ 8 ]  . 
 since the markers are larger than the dimensions of a single voxel , defining their center of mass in large magnification allows the rsme to be well under the voxel dimension of the respective imaging modality [ 16 ]  . 
it must be reminded , however , that the rsmes achieved in this study only represent the mean difference of the reference points ( frame ) to each other between the two fused data sets , not the anatomic accuracy of the registration . 
our experiences on anatomic correlation between data sets , however , confirmed the results of a phantom study conducted at this institution [ 4 ] , whereby fiducial ( frame ) and actual target registration error between ct / mr and ct / spect datasets correlated to < 1.5 mnonetheless , each registration should be thoroughly checked in three planes by a physician before incorporating it in the treatmentplanning process . 
 although the fused images of the patient described as case report , as well as the others involved to date , were used and considered for ctv volume delineation , incorporation of the automatic registration software in the actual treatment - planning software is currently in progress at our institution . 
in addition , the integration of software for ( semi ) automated marker detection has already been developed [ 5 ] and used ( tiani , medgraph , vienna , austria ) to expedite and simplify the registration process . 
 ideally , the vacuum mouthpiece ( its production takes about 10 min requiring very little training and costing about 40 . / patient ) is made at initial presentation of a patient with symptoms suspicious of a cranial tumor . 
the negative pressure of the vacuum mouthpiece allows the most direct , noninvasive connection to the cranium , granting not only precise repositioning for fractionated treatments but now also accurate and simple integration of multimodal cranial imaging into radiotherapy treatment planning and follow - up using an external reference frame . 
the reference points on this frame grant completely objective registration using relatively simple and ubiquitous software , independent of a users capability of defining anatomic landmarks or the varying limitations of more elaborate and costly algorithms . 
 acknowledgment the authors would like to express their sincere gratitude to the involved radiation technicians ( ct / mri / nuclear medicine ) , especially thomas lang and martin knoflach from the sip - lab . 
 strahlentherapie und onkologie short communication a small prospective study of chordomas treated with radiotherapy and razoxane walter rhomberg1 , franz - karl bhler1 , hansjrg novak2 , susanne dertinger3 , gerhard breitfellner3 purpose : to evaluate the local effect of conventional photon irradiation in chordomas if the radiosensitizing agent razoxane is added . 
 patients and methods : between 1988 and 1996 , five patients with histologically confirmed chordomas of the skull base or the spine ( three females , two males ) were irradiated with 6and 25 - mev photons under razoxane medication , one patient was treated with a telecobalt unit . 
 results : after a potential median follow - up time of 10 years , three of the five patients are alive and show neither symptoms nor signs of recurrence in ct or mr images . 
 key words : chordomas razoxane radiosensitizing agents radiation therapy combined - modality treatment strahlenther onkol 2003 ; 179 : 24953 doi 10.1007 / s00066 - 003 - 1052 - x prospektive studie zum einsatz von razoxan bei der bestrahlung von chordomen hintergrund : aufgrund der beschrnkten sensibilitt von chordomen gegenber einer photonenbestrahlung wurde eine prospektive studie unter zugabe von razoxan per os durchgefhrt . 
 patienten und methodik : zwischen 1988 und 1996 wurden fnf patienten mit histologisch gesicherten chordomen der schdelbasis und der wirbelsule ( drei frauen und zwei mnner ) mit hochenergetischen photonen am linearbeschleuniger bei gleichzeitiger medikation von razoxan bestrahlt . 
ein patient mit einem persistierenden sakralen chordom starb nach 8 jahren an herzinsuffizienz , ein anderer nach 6 , 5 jahren an einer postoperativen blutung nach rezidivoperation an der oberen brustwirbelsule . 
although the growth of these tumors is reported to be slow , the local control rates and the long - term prognosis of patients with chordomas remain limited even in the era of particle therapy [ 5 , 11 , 18 , 23 , 35 ]  . 
the reason to use radiotherapy together with razoxane for chordomas were favorable results seen earlier with this combination in chondroand soft tissue sarcomas [ 17 , 31 , 32 ]  . 
concomitantly , the radiosensitizer razoxane ( cambridge laboratory , uk ; commercially available at torrex - pharma , vienna , austria ) was given at a dose of 125 mg twice daily during the irradiation days until the end of radiotherapy . 
typical chordomas have inhomogeneous , predominantly low signal intensity on t1 - weighted mri scans and equal or exceeding csf signal intensity or pd / t2wi [ 27 ]  . this description was right as to the patients shown in figures 1 and 2 . 
the local control in the five patients is presently 60 , 68 + , 76 , 130 + , and 155 + months , respectively . three patients are alive and show neither symptoms nor signs of a recurrence in ct or mr images . 
klinik , therapie und ergebnisse bei fnf patienten mit chordomen , die unter zugabe von razoxan per os bestrahlt wurden . patient age ( years ) / sex location resection total razoxane dose ( g ) rtx dose ( gy ) / fractions / time ( weeks ) tumor response local control ( months ) survival ( months ) 44 / f 13 / f 70 / m 72 / f 76 / m base of skull base of skull os sacrum biopsy only biopsy , r2 resection after 36 gy biopsy biopsy r2 resection 11.5 67 / 35 / 11 63 / 34 / 12 63 / 35 / 7 59 / 28 / 7 54 / 23 / 10 complete complete no change partial not evaluable 155 + 130 + 155 + 130 + strahlenther onkol 2003 no . 
leukopenia who grade 3 developed in two of five patients due to razoxane , the leukocyte nadir being between day 10 and 14 . there were no serious long - term complications . 
razoxane in irradiation of chordomas discussion conclusions conventional high - dose photon irradiation with doses around 50 gy is associated with local control rates of 27% only [ 11 ]  . the median time to recurrence or new symptoms for those with overt disease is reported to be 3.5 years [ 8 , 11 , 25 ] , sometimes even less [ 6 , 13 , 38 ]  . 
freedom from symptoms after 10 years was observed in < 10% of the zurich cases [ 14 ] , and no 10 - year survivors were seen among four patients treated with radiotherapy alone in a series of 21 patients by keisch et al [ 20 ]  . 
several authors come to the conclusion that overt residual chordoma is rarely cured with conventional external - beam irradiation [ 6 , 8 , 14 , 29 ] , and radiation doses > 48 or 55 gy are advocated to achieve a worthwhile palliation [ 13 , 29 , 30 ]  . 
 apart from the introduction of new surgical techniques [ 4 ] , an extensive use of surgery [ 36 ] , or the application of a homogeneous dose distribution [ 1 , 37 ] , some progress in the treatment of chordomas was made by using high - let irradiation , e.g. , proton beams and heavy ions . 
the local control rates in patients with chordomas of the skull base ( chondrosarcomas excluded ) treated at the harvard cyclotron in boston using a 160 - mev proton beam were reported to have increased up to 60% at 5 years [ 23 , 35 ] ; similar outcomes were seen in other centers [ 5 , 18 ]  . 
however , the disadvantages of a restricted availability of high - let beams , high costs , and the risk for normal structures such as the optic nerve or the brain stem have to be kept in mind if this kind of treatment is considered . 
occasional but serious problems reported with the heavy - ion treatment were blindness , pituitary insufficiency with the need for hormonal substitution , and damage to the brain stem [ 5 , 11 , 18 , 19 ] , and the rate of objective partial tumor remissions may still be limited [ 9 ]  . 
 recently , also the introduction of radiosurgery and other modern 3 - d treatment techniques were claimed to provide superior results compared to conventional techniques [ 10 , 18 , 21 ]  . 
the addition of iort or gamma knife may not further improve the results [ 12 ] ; at the same time , the mean tumor volume has to be small [ 24 ]  . 
 thus , a local control over 5 years in all of the five cases described and the objective regression in three of four measurable lesions compare favorably with recent communications using high - let irradiation or stereotactic techniques . 
prognostic differences in favor of the chondroid versus the epithelial variant of the chordomas are probably existing [ 1 , 12 ] , although this prognostic criterion is not always confirmed [ 7 ]  . 
the trend of these results would be in line with the improved local control seen in other mesenchymal tumors when radiotherapy was combined with the sensitizer razoxane [ 28 ]  . 
 strahlentherapie und onkologie original article multimodality therapy including radiotherapy and chemotherapy improves event - free survival in stage c esthesioneuroblastoma hans theodor eich1 , barbara hero2 , susanne staar1 , oliver micke3 , heinrich seegenschmiedt4 , adrian mattke5 , frank berthold2 , rolf - peter mller1 background : to evaluate the efficacy of multimodality therapy in patients with esthesioneuroblastoma ( enb )  . 
 patients and methods : from 01 / 1979 through 08 / 2001 , 47 patients with enb ( 20 men , 27 women , age 581 years ) , were registered from 18 oncologic centers . 
initial treatment included surgery alone in seven patients , radiotherapy ( rt ) with or without chemotherapy ( ctx ) in twelve , surgery plus postoperative rt in 15 , and multimodality therapy ( surgery plus preor postoperative ctx plus postoperative rt ) in 13 . results : the 5 - year overall survival ( os ) for the whole group was 64 8% and the 5 - year event - free survival ( efs ) 50 8% . 
none of the patients with multimodality treatment had a metastatic relapse . conclusion : multimodality treatment ( surgery plus preor postoperative ctx plus postoperative rt ) appears to be highly efficient in preventing local and systemic relapse in patients with advanced enb . 
timing and optimal agents of ctx need to be further evaluated . key words : esthesioneuroblastoma neuroectodermal tumors olfactory neuroblastoma multimodality therapy surgery radiotherapy chemotherapy strahlenther onkol 2003 ; 179 : 23340 doi 10.1007 / s00066 - 003 - 1089 - x multimodale therapieanstze mit radiotherapie und chemotherapie verbessern das ereignisfreie berleben bei patienten mit sthesioneuroblastomen im stadium kadish c hintergrund : der stellenwert multimodaler therapieanstze in der behandlung von sthesioneuroblastomen ( enb ) soll untersucht werden . patienten und methodik : analysiert wurden 47 patienten ( 20 mnner , 27 frauen ; alter : 581 jahre ) , die im zeitraum 01 / 197908 / 2001 aufgrund eines enb in 18 onkologischen zentren behandelt worden waren ( tabelle 1 )  . 
im rahmen der primrtherapie wurden sieben patienten nur operiert , zwlf erhielten eine definitive radiotherapie ( rt ) chemotherapie ( ctx ) , 15 wurden operiert und postoperativ bestrahlt und 13 erhielten eine multimodale therapie ( operation plus pr - / postoperative ctx plus postoperative rt )  . ergebnisse : das 5 - jahres - gesamtberleben ( os ) aller patienten betrug 64 8% und das ereignisfreie 5 - jahres - berleben ( efs ) 50 8% ( abbildung 1 )  . 
patienten mit multimodaler therapie hatten ein signifikant verbessertes 5 - jahres - efs ( 74 13% ) im vergleich zu den anderen therapiegruppen ( 41 9% ; p = 0 , 05 ; abbildung 2 ) , allerdings zeigte sich kein signifikanter unterschied im 5 - jahres - os ( p = 0 , 39 )  . 
keiner der patienten mit multimodaler therapie entwickelte metastasen . 1 department of radiotherapy , university of cologne , germany , 2 department of pediatric oncology , childrens hospital , university of cologne , germany , 3 department of radiotherapy , university of mnster , germany , 4 department of radiotherapy , alfried krupp hospital essen , germany , 5 childrens hospital , olgaspital , stuttgart , germany . 
esthesioneuroblastoma schlussfolgerung : multimodale therapieanstze unter einschluss von operation plus pr - / postoperativer ctx plus postoperativer rt erscheinen hocheffektiv in der verhinderung eines lokalen und systemischen rezidivs bei patienten mit kadish - c - enb . 
der zeitpunkt und die optimale zusammensetzung einer polychemotherapie mssen weiter untersucht werden . schlsselwrter : sthesioneuroblastom neuroektodermale tumoren olfaktoriusneuroblastom multimodale therapie chirurgie radiotherapie chemotherapie introduction esthesioneuroblastoma ( enb ) is a rare neuroectodermal tumor originating from the olfactory epithelium , first described by berger & luc in 1924 [ 1 ]  . 
current therapeutic options include surgery alone , radiotherapy ( rt ) alone , a combination of both modalities with preand postoperative rt , chemotherapy ( ctx ) and high - dose ctx followed by autologous bone marrow transplantation [ 2 , 4 , 6 , 10 , 1315 , 20 , 24 , 27 , 29 , 34 , 35 , 37 , 38 , 41 ]  . 
a questionnaire including data of patients characteristics , initial symptoms , tumor extent , histologic margin status of final pathologic studies , primary therapy , tumor recurrence , and follow - up was sent to the treatment centers of radiotherapy and pediatric oncology in germany . 
patients were staged according the kadish system ( table 1 ) which is predominantly used in literature , although multiple modifications have been proposed [ 3 , 6 , 9 , 21 , 29 ]  . 
 statistical analysis treatment response was assessed by clinical examinations and computed tomography ( ct ) or magnetic resonance imaging ( mri ) and classified as complete response , partial response , stable disease , and progressive disease according to common use . 
overall survival ( os ) and event - free survival ( efs ) were calculated from diagnosis to the first event ( death from enb , local recurrence / lymph node , or distant metastases , respectively ) using the kaplan - meier life table method . 
ctx : chemotherapy ; dod : dead of local disease ; dom : dead of metastases ; ln : lymph node ; ned : no evidence of disease ; rec : recurrence ; rt : radiotherapy . 
ctx : chemotherapie ; dod : tod durch primrtumor ; dom : tod durch metastasen ; ln : lymphknoten ; ned : keine krankheitszeichen ; rec : rezidiv ; rt : radiotherapie . 
of metastases stage dose ( gy ) daily fractions overall survival ( months ) survival eventoutcome free ( months ) surgery rt + ctx surgery + rt brain ( 31 ) lung ( 31 ) liver ( 6 ) liver ( 0 ) ln ( 0 ) ln ( 0 ) bone ( 11 ) ln ( 37 ) ln ( 0 ) bone ( 6 ) ln ( 0 ) meningeal ( 70 ) meningeal ( 7 ) 8 ln ( 88 ) ln ( 5 ) brain ( 56 ) ln ( 0 ) dod / neda neda neda died , ned died , ned alive , rec dod / neda dod / neda dod / died , ned continued overleaf fortsetzung auf der nchsten seite patients were treated by a multimodality approach consisting of neoadjuvant ctx , surgery and postoperative rt in five or surgery , postoperative rt and ctx in eight ( table 1 )  . 
 in 35 / 47 patients , a surgical procedure was employed consisting of a nasal tumor resection in 12 / 35 patients , a craniotomy and lateral rhinotomy ( craniofacial resection ) in 17 / 35 patients and intracranial surgery plus lateral rhinotomy in 6 / 35 patients . 
for 22 patients with adjuvant rt , the median dose to the target volume was 50 gy ( range 3260 gy ) , median dose per fraction 2 gy ( range 1.83 gy ) , median number of fractions 25 ( range 1630 )  . 
12 / 40 patients received definitive rt with or without ctx and 6 / 40 patients rt after incomplete surgery . for the latter group , the median dose to the target volume was 60 gy ( range 4070 gy ) , median dose per fraction 2 gy ( range 1.83 gy ) with a median number of 29 fractions ( range 2036 )  . 
most of the patients with definitive rt were treated early in the series with palliative intent because of advanced , unresectable nature of the primary tumors and poor general condition . 
the planning target volume ( ptv ) encompassed the primary tumor site and varied upon the tumor extension including a safety margin of 12 cthe ptv was chosen to cover the 90% isodose . 
 treatment protocol for enb during this 21 - year time span , chemotherapeutic agents were used in various combinations , most based on trials for childhood neuroblastoma or soft tissue sarcoma . 
the 5 - year efs of the combined modality group was 64 13% , in the radiotherapy group with or without ctx 39 15% , and for surgery alone 0% ( p = 0.01 ; figure 2 )  . 
for kadish stage c patients , multimodality therapy ( n = 11 ) was associated with a significantly better 5 - year efs ( 72 14% vs 17 9% ; p = 0.01 ) and a trend for better 5 - year os ( 69 15% vs 47 12% ; p = 0.19 ) , compared to all other treatment modalities ( figure 3 )  . 
 lymph node and distant metastases after a median follow - up of 34 months ( range 588 months ) , 10 / 47 patients ( 21% ) developed nodal and / or distant metastases . 
 role of surgery surgery is the mainstay of treatment for enb , but local recurrence rates after surgery only are reported to be within the range of 4486% [ 6 , 9 , 21 ]  . 
salvage therapy for the four patients of the combined modality group consisted of local excision only ( n = 1 ) , surgery plus rt ( n = 2 ) , and ctx ( n = 1 )  . 
for the three patients of the multimodality group , salvage therapy consisted of rt plus ctx ( n = 2 ) , and ctx ( n = 1 )  . 
it was acceptable including hearing dysfunction ( n = 2 ) , amenorrhea ( n = 2 ) , slight facial asymmetry ( n = 2 ) , persistent peripheral neuropathy ( n = 1 ) , loss of sense of smell ( n = 1 ) , and cardiotoxicity who grade ii ( n = 1 )  . 
the wide variety of treatment approaches which is due to the multiinstitutional collection of enb patients is interesting and reflects the absence of by some authors , rt as well has been proposed as primary treatment in enb . 
an epidemiologic study at the mayo clinic conducted from 1951 to 1990 showed no significant difference in survival rates between patients who had only rt and those who had surgery only for the primary lesions [ 14 ]  . 
 moreover , a combined approach with postoperative rt is reported to result in better local control ( 040% ) [ 6 , 11 , 12 , 17 , 21 , 31 , 36 ]  . 
oconnor et al [ 31 ] observed recurrences after surgery , but not after a combined approach , and elkon et al [ 12 ] reported values of 44% for surgery alone and 29% for surgery plus rt . 
the authors recommend adjuvant rt particularly for high - grade tumors according to hyams system and high - stage tumors according to the kadish system [ 19 , 21 ]  . 
however , they were able to show improved local tumor control after preoperative rt [ 10 ]  . polin et al [ 32 ] reported on 34 patients with preoperative neoadjuvant rt with or without chemotherapy . 
two thirds of the patients showed a significant reduction in tumor burden leading to a greater chance of gross total tumor resection and long - term disease - free progression . 
 role of chemotherapy the histologic similarity of enb to other chemosensitive neoplasms such as neuroblastoma , small cell lung carcinoma , and primitive neuroectodermal tumors indicated a possible efficastrahlenther onkol 2003 no . 
various drugs have been used for ctx of enb , especially platinum - based regimens and combination therapy using cyclophosphamide , vincristine , and occasionally doxorubicin [ 34 ]  . 
some clinical responses have been reported to mechlorethamine , dacarbazine ( dtic ) , actinomycin , methotrexate , bcnu , procarbazine , and thiotepa [ 28 , 34 ]  . 
in a retrospective analysis of ten patients , mcelroy et al [ 27 ] have demonstrated that cisplatinum - based chemotherapy is active in advanced , and especially high - grade enb . 
eden et al reported results in 16 patients with stage a or b and 24 with stage c disease treated with rt ( median dose 50 gy ) and surgery for stage a and b disease , with addition of ctx ( cyclophosphamide and vincristin ) for stage c disease [ 10 ]  . 
although primary tumor response to ctx did not show significant survival advantage in patients treated with multimodality regimen , the disease - free intervall was significantly better than in those patients who did not receive ctx prior to surgery . 
five patients had neoadjuvant ctx plus surgery plus rt and eight patients surgery plus rt plus ctx . all five patients with neoadjuvant ctx had initially inoperable tumors , but in all of them complete tumor resection was possible . 
wether the use of new radiation treatment techniques with the option of local dose escalation and the use of imrt can lead to an improvement of local control remains to be seen [ 8 , 18 , 41 ]  . 
the additional use of ctx seems to have a strong impact on the reduction of metastatic spread in comparison with the combined modality group ( surgery plus rt ) which has been considered the best treatment so far [ 6 ]  . 
moreover , it has to be emphasized that 11 / 13 patients with multimodality therapy were < 20 years of age and , thus , more likely to tolerate an intensified approach considering their general condition and fewer comorbidities compared to older patients [ 25 ]  . 
in addition , the tumor has also been observed to behave differently and tends to be more aggressively in the younger population [ 5 , 21 , 26 ]  . 
if there was no ctx applied during initial therapy , ctx appears useful . for patients with large recurrent tumors unsuitable for further local therapy , high - dose ctx and bone marrow transplantation have been reported to be a promising approach [ 10 ]  . 
in the university of virginia series of five patients salvaged with high - dose ctx and bone marrow transplantation , three were alive with no evidence of disease , whereas only four of 17 patients ( 24% ) salvaged with surgery and ctx or rt were alive with no evidence of disease [ 10 ]  . 
 conclusion though the debate regarding the optimal therapy for enb has not yet been resolved , local control and minimization of risk of metastatic spread are essential to achieve improved survival rates . 
esthesioneuroblastoma strahlentherapie und onkologie urban & vogel 2000 originalarbeit dose measurements in the build - up region for the photon beams from clinac - 1800 dual energy medical linear accelerator manickam ravikumar , ramamoorthy ravichandran1 aim : since the skin dose becomes the limiting factor while deciding the tumorcidal dose , the detailed analysis of dose distribution in the build - up region is necessary for high - energy photon beams . 
 materials and methods : measurements were made with 6and 18 - mv photons using a ptw parallel - plate ionization chamber ( b 23344 - 036 ) and a rdm - 1f electrometer . 
build - up ionization measurements were made with the chamber fitted into a 25 ( cid : 2 ) 25 ( cid : 2 ) 25 cm polystyrene phantom with a fixed ssd of 100 cthe entrance and build - up dose measurements were made with a polycarbonate and a mesh type metallic shielding tray and a 45 wedge . 
exit dose measurements were carried out for the graphite patient supporting assembly table top , 1.0 cm thick piece of wood and the 1.0 cm thick patient supporting perspex base frame for head and neck treatments . 
at tray - surface distances above 60 cm the tpf almost remained close to unity for 6 - mv photons for all field sizes , whereas the continuous decrease in tpf could be noted for 18 - mv photon beams even after the tpf reached unity . conclusion : the increase in surface dose with field size for both photon energies is due to the electron scattering from the intervening materials . 
the increase in dose enhancement percentage with graphite compared to perspex supporting assembly indicates that the electron backscatter is proportional to the atomic number of the mediu key words : dose distribution build - up region relative surface dose dosismessung in der aufbauregion fr klinische photonenstrahlen des medizinischen linearbeschleunigers clinac 1800 mit zwei photonenenergien fragestellung : die applizierte dosis im tumorzielvolumen wird entscheidend von der hautdosis begrenzt . 
in dieser studie werden die parameter der klinischen photonenstrahlen , die die hautdosis und die aufbauregion bestimmen , fr photonenenergien von 6 mv und 18 mv vorgestellt und analysiert . material und methoden : die messungen wurden fr photonen der energie von 6 mv und 18 mv unter verwendung einer ionisationskammer der ptw ( typ b 23344 - 036 , flachkammer ) und eines elektrometers ( typ rdm - 1f ) durchgefhrt . 
fr die dosismessung in der aufbauregion wurde die ionisationskammer in ein polystyrenphantom mit einem definierten volumen von 25 ( cid : 2 ) 25 ( cid : 2 ) 25 cm und einem festen fokus - oberflchen - abstand von 100 cm eingepasst . 
dose measurements in the build - up region ergebnisse : der geometrische abstand dmax ( des maximums der tiefendosis ) verringerte sich leicht mit der feldgre , wie das auch bei anderen beschleunigern beobachtet wird . 
die analyse der daten zeigt , dass der trgerstreufaktor ( tray perturbation factor , tpf ) an der oberflche mit zunehmendem trger - oberflchen - abstand fr beide photonenenergien und alle benutzten feldgren kleiner wurde . 
im gegensatz dazu nahm der tpf bei 18 mv sogar bis unterhalb einem wert von 1 ab . schlussfolgerung : die zunahme der oberflchendosis mit zunehmender feldgre entsteht fr beide photonenenergien durch die ( compton - ) elektronenstreuung der im strahlengang liegenden materialien . 
die relative zunahme der dosisverstrkung bei der graphitunterlage gegenber der perspexunterlage deutet darauf hin , dass die rckstreuung der elektronen des jeweiligen mediums proportional zur ordnungszahl des mediums ist . schlsselwrter : dosisverteilung aufbauregion relative oberflchendosis t he skin sparing effect of megavoltage gamma and x - ray source made it possible to deliver high tumorcidal doses to deep seated tumors at the same time maintaining the dose to superficial layers of skin minimuhigh - dose delivery to deep tumors , however , requires careful consideration of dose distributions in the build - up regions to avoid lethal damage to the skin and the subcutaneous tissues . 
in many clinical situations the skin dose is the limiting factor to deliver the high dose to the tumor at depth . hence , careful analysis of dose distribution in the build - up region is necessary for high - energy photon beams . 
 previous studies [ 7 , 8 , 10 , 12 , 14 , 15 , 17 , 18 ] have shown that the dose distribution in the build - up region depends on several factors such as source to skin distance ( ssd ) , field size , presence of secondary blocking tray and the distance between the skin and the blocking tray . 
a number of studies [ 24 , 7 , 14 , 15 ] has been carried out by many authors for the early generation linear accelerators and different model cobalt - 60 machines . 
the entrance and exit dose regions are of current interest as our accelerator is equipped with a kapton thin window monitor chamber , which is reported to vary the entrance and exit doses significantly [ 11 ]  . 
this chamber has a sensitive volume of 0.2 cm3 ( diameter 16 mm ) with an electrode separation of 1.5 m the ion chamber polarizing voltage was 400 v and both positive and negative collecting potentials were used for measurements . 
build - up ionization measurements were made with the chamber fitted into a 25 ( cid : 2 ) 25 ( cid : 2 ) 25 cm polystyrene phantom at a fixed fsd of 100 c various thicknesses of polystyrene sheets were added on to the surface of the phantom to vary the depth of measurement . polystyrene phantom of 25 cm thickness was used for providing saturation backscattering medium for the entrance dose measurements . 
the entrance and build - up dose measurements were taken with a 0.6 cm polycarbonate and a mesh type metallic shielding tray positioned at 61.5 cm from the virtual source . 
the percentage depth dose ( pdd ) is quantified as the ratio of dose at the depth of measurement to that of a dose at the depth of maximu the tray perturbation factor ( tpf ) at surface is defined as the ratio of relative fractional dose at the phantom surface with and without tray . the relative surface dose factors were estimated with a 45 universal wedge in position for 5 ( cid : 2 ) 5 cm and 15 ( cid : 2 ) 15 cm field sizes . 
dose measurements in the build - up region ( 25 ( cid : 2 ) 25 cm ) and the 1.0 cm thick patient supporting perspex base frame for head and neck treatments were used for exit dose measurements . 
the validity of positioning the parallel plate chamber in the reverse geometry was confirmed by measuring the percent depth dose for a 10 ( cid : 2 ) 10 cm field with chambers positioned on both sides . 
 the validity of measurements for field size ( 25 ( cid : 2 ) 25 cm ) same to that of polystyrene phantom size ( 25 ( cid : 2 ) 25 cm ) was checked against the measurement adding an additional polystyrene block around the smaller phanto no significant difference was observed as a result of the added phantom material . 
the relative fractional surface dose compared to the dose at dmax for both energies for field sizes ranging from 5 ( cid : 2 ) 5 to 25 ( cid : 2 ) 25 cm with shielding tray in position and open portal is shown in figures 2a and 2b for 6and 18 - mv photons . 
 percentage dose build - up curves at 100 cm ssd with 0.6 cm polycarbonate blocking tray present are shown in figures 3a and 3b for 6and 18 - mv beams . 
 the influence of shielding trays for both energies is shown in terms of variation of tray perturbation factors ( tpf ) at surface with tray - surface distance in figures 5a and 5b for field sizes of 5 ( cid : 2 ) 5 , 15 ( cid : 2 ) 15 and 25 ( cid : 2 ) 25 cm at surface . 
at tray - surface distances above 60 cm the tpf almost remains close to unity for 6 - mv photons for all field sizes , whereas the continuous decrease in tpf can be noted for 18 - mv photon beams even after the tpf reaches unity . this could be due to the limited range of scattered electrons from the polycarbonate tray . 
the 45 wedge was kept at 49.2 cm from the source during measurement for both photon energies . the ionization readings for thin and thick side wedge orientations agreed within 0.5%. 
the data show that the relative surface dose is less for smaller field size ( 5 ( cid : 2 ) 5 cm ) compared to the larger field ( 15 ( cid : 2 ) 15 cm ) at all ssds for both energies . 
also it is noticed that rsf remains almost constant for a 5 ( cid : 2 ) 5 cm field at all ssds both at 6and 18 - mv photon beams . 
the decreases in exit dose for a 15 ( cid : 2 ) 15 cm field with no backscatter were 16% and 11% for the 6 - mv and 18 - mv photons beams , respectively . 
 table 1 indicates the percentage of surface dose enhancement for 5 ( cid : 2 ) 5 and 15 ( cid : 2 ) 15 cm fields for various clinical backscattering media in comparison with no backscattering mediuthe table shows that the enhancements in dose are more for a larger field size ( 15 ( cid : 2 ) 15 cm ) compared to smaller field size ( 5 ( cid : 2 ) 5 cm ) for all clinical backscattering mediums . 
prozentuale dosiserhhung bei unterschiedlichen rckstreumedien . discussion the increase in surface dose with field size for both photon energies is due to the electron scattering from flattening filter , monitor chambers , primary and secondary collimators and the air column between the distal collimator and the phantom surface . 
whereas for 18 - mv photon beams the decrease in tpf at extended distances proves that the polycarbonate tray absorbs more secondary electrons compared to that of the secondary electrons produced . these effects depend on the range of secondary electrons generated from the collimator and the blocking tray . 
the increase in dose enhancement percentage with graphite compared to the perspex supporting assembly indicates that the electron backscatter is proportional to the atomic number of the mediuwhen the depth dose tables are used to assess the dose at the exit surface , the dose due to loss of backscatter and the enhancement due to patient support devices should be considered . 
 strahlentherapie und onkologie urban & vogel 2000 originalarbeit bestrahlung von schdelbasistumoren mit kohlenstoffionen bei der gsi erste klinische ergebnisse und zuknftige perspektiven jrgen debus1 , thomas haberer2 , daniela schulz - ertner1 , oliver jkel3 , frederik wenz1 , wolfgang enghardt4 , wolfgang schlegel3 , gerhard kraft2 , michael wannenmacher1 hintergrund : strahlenbiologische und medizinphysikalische untersuchungen versprechen vorteile bei der patientenbestrahlung mit schweren ionen . 
die vorliegende arbeit berichtet ber die ersten klinischen ergebnisse bei 45 patienten mit schdelbasistumoren , die zwischen dezember 1997 und september 1999 am schwerionensynchrotron der gesellschaft fr schwerionenforschung ( gsi ) , darmstadt , mit kohlenstoffionen bestrahlt wurden . patienten und methode : die patienten ( 23 frauen , 22 mnner ) waren im mittel 48 ( 18 bis 80 ) jahre alt und litten an chordomen ( 17 ) , chondrosarkomen ( zehn ) und anderen tumoren der schdelbasis . 
bei den anderen tumorhistologien wurde nach fraktionierter stereotaktischer radiotherapie ein kohlenstoffionenboost von 15 bis 18 gye auf den makroskopischen tumor appliziert ( mediane gesamtdosis 63 gye )  . ergebnisse : der mittlere nachbeobachtungszeitraum betrug neun monate . 
als konsequente fortfhrung des projektes ist der bau eines ausschlielich klinisch genutzten teilchenbeschleunigers in heidelberg geplant . schlsselwrter : schdelbasis kohlenstoffionen schwerionentherapie strahlentherapie gsi fractionated carbon ion irradiation of skull base tumors at gsi . 
we report the results of 23 women and 22 men ( median age 48 years ) with skull base tumors irradiated with carbon ion beams at the gesellschaft fr schwerionenforschung ( gsi ) , darmstadt , from december 1997 until september 1999 . patients and methods : the study included patients with chordomas ( 17 ) , chondrosarcomas ( 10 ) and other skull base tumors ( table 1 )  . 
other histologies were treated with a carbon ion boost of 15 to 18 gye delivered to the macroscopic tumor after fractionated stereotactic radiotherapy ( median total dose 63 gye )  . 1radiologische universittsklinik , heidelberg , 2gesellschaft fr schwerionenforschung , darmstadt , 3deutsches krebsforschungszentrum , heidelberg , 4forschungszentrum rossendorf bei dresden . dem mentor dieses projektes , herrn hans - joachim specht , mit dank gewidmet . eingang des manuskripts : 22 . 
no severe toxicity and no local recurrence within the treated volume were observed . conclusion : clinical effectiveness and technical feasibility of this therapy modality could clearly be demonstrated in our study . 
aufgrund des geringen metastasierungspotentials [ 8 , 19 ] hngen die therapieerfolge bei diesen patienten entscheidend vom ausma der lokalen kontrolle ab . schwerionen sind den photonen in ihrer physikalischen selektivitt und biologischen wirksamkeit berlegen . 
durch den anschlieenden steilen dosisabfall wird hinter dem tumor liegendes normalgewebe geschont . nach strahlenbiologischen abschtzungen sollten diese dosisverteilungen erlauben , die dosis im tumor im vergleich zur photonenbestrahlung um 15 bis 35% zu erhhen [ 1 ]  . darber hinaus haben schwerionen im bereich des braggpeaks eine hhere biologische wirksamkeit als photonen ( hoch - let - effekt )  . 
aufgrund eines sauerstoffverstrkungsfaktors ( oer ) von nahe 1 im bragg - peak ist schwerionenstrahlung auch bei hypoxischen tumoren wirksa zellzyklusbedingte unterschiede in der radiosensitivitt von zellen sind gering , so dass sich unterschiede in der therapieantwort langsam und schnell proliferierender tumoren reduzieren sollten . 
es wurden zudem eine verzgerung der zellteilung nach hoch - let - bestrahlung sowie eine abnahme der schutzeffekte durch die benachbarten zellen beschrieben [ 2 , 17 ]  . positive trends im rahmen von phase - ii - studien zeigten sich nach schwerionenbestrahlungen in berkeley , kalifornien , wobei diese therapieanlage aus technischen grnden nur bis 1992 betrieben werden konnte [ 1 ]  . 
die vorliegende arbeit berichtet ber die ersten klinischen ergebnisse und zeigt die sich daraus ergebenden zukunftsperspektiven auf . patienten und methode patienten es wurden 45 patienten ( 23 frauen , 22 mnner ) mit tumoren der schdelbasis in unsere klinische studie aufgenommen . 
bestrahlung von schdelbasistumoren bei der gsi bestrahlungsplanung und patientenpositionierung von jedem patienten wurden in stereotaktischer lagerung aufnahmen mit dem computertomographen ( ct ) und dem magnetresonanztomographen ( mrt ) angefertigt , auf denen der tumor inklusive eines adquaten sicherheitsabstandes entlang der typischen anatomischen ausbreitung als zielvolumen markiert wurde . 
die am deutschen krebsforschungszentrum entwickelten techniken der stereotaktischen zielpunktlokalisation und patientenpositionierung , die die reproduzierbarkeit der patientenlagerung bei den aufeinanderfolgenden einzelbestrahlungen millimetergenau ermglichen , wurden an anderer stelle detailliert beschrieben [ 10 ] , ebenso die methode der dreidimensionalen strahlentherapieplanung und berechnung der dosisverteilung mittels des am deutschen krebsforschungszentrum entwickelten computerprogramms voxelplan [ 6 ]  . 
ein typischer behandlungsplan fr einen schdelbasistumor ist in abbildung 1 dargestellt . fr den fall , da die kohlenstoffbestrahlung aus technischen grnden fr 4 tage htte unterbrochen werden mssen , wurde fr alle patienten ein bestrahlungsplan fr eine fraktionierte stereotaktische radiotherapie ( fsrt ) erstellt . bestrahlung die indikation fr die strahlentherapie wurde bei inoperablen tumoren und mikroskopischen oder makroskopischen tumorresiduen gestellt . 
bei adenoidzystischen karzinomen , malignen meningeomen und malignen schwannomen wurde nach fraktionierter stereotaktischer radiotherapie ein kohlenstoffionenboost von 15 bis 18 gy in einzeldosen von 3 , 0 gye auf den makroskopischen tumor appliziert . 
erstmalig kamen das an der gsi entwickelte intensittsmodulierte rasterscan - verfahren [ 9 ] sowie die online - therapiekontrolle mittels positronenemissionstomographie am patienten zum einsatz [ 4 , 5 ]  . 
lokales therapieversagen wurde strenger definiert als in den whorichtlinien vorgegeben : als erneutes auftreten des tumors an gleicher stelle oder als erneutes tumorwachstum , erkennbar als eine auf zwei aufeinanderfolgenden mrtschichtaufnahmen klar beurteilbare zunahme der tumorflche . 
bestrahlung von schdelbasistumoren bei der gsi wurden nach dem kaplan - meier - verfahren berechnet . strahlenreaktionen wurden nach den bewertungskriterien der radiation therapy oncology group ( rtog ) , der european organization for research and treatment of cancer ( eortc ) bzw . 
bei 16 / 17 patienten mit chordomen und bei 7 / 8 patienten mit adenoidzystischen karzinomen konnte eine tumorkontrolle erreicht werden . eine partielle tumorremission wurde insgesamt bei sieben patienten beobachtet , darunter drei chordome , zwei adenoidzystische karzinome ( abbildung 2 ) , ein abrikossow - tumor und ein transitionalzellkarzino eine lokale kontrolle innerhalb des bestrahlungsvolumens konnte bei allen patienten erreicht werden . 
die kaplanmeier - berechnung ergibt nach einem jahr eine lokale kontrollrate von insgesamt 94% . berlebensraten nur ein patient ( 2 , 2% ) mit transitionalzellkarzinom ist innerhalb des nachbeobachtungszeitraums verstorben . 
die in der kurzen phase des laufenden projektes erzielten klinischen ergebnisse sind als positiv zu werten . dennoch sind die nachsorgezeiten noch zu kurz , um die langzeitkontrolle endgltig zu bewerten . 
in der literatur wird ausfhrlich diskutiert , dass dies mit grter wahrscheinlichkeit zu einer erhhung der heilungsraten , zu einer verlngerung der berlebenszeiten und zu einer verbesserung der lebensqualitt der patienten fhrt [ 3 , 18 ]  . 
zwei medizinphysikalische neuerungen konnten im rahmen dieser studie etabliert und ihre technische durchfhrbarkeit und effizienz bewiesen werden : das intensittsmodulierte rasterscanverfahren erlaubt eine dosiskonformation an das tumorvolumen in niemals zuvor erreichter rumlicher przision ; durch die online - therapiekontrolle mittels positronenemissionstomographie knnen erstmals lage und intensitt des strahls im krper des patienten whrend der bestrahlung berwacht werden [ 5 ]  . bei der gsi kommen kohlenstoffionen zum einsatz . 
unsere klinischen daten scheinen die strahlenbiologischen vorhersagen zu untersttzen . die kapazitt der gesellschaft fr schwerionenforschung als weltweit kooperierendes institut der physikalischen grundlagenforschung ist fr die strahlentherapie auf etwa 70 patientenbestrahlungen pro jahr begrenzt . 
erforderlich ist die durchfhrung klinischer studien mit ausreichend groen patientenzahlen , die statistisch belastbare ergebnisse liefern . prinzipiell sind all jene tumoren eine potentielle indikation fr die ionentherapie , bei denen mit der konventionellen strahlentherapie keine befriedigenden ergebnisse erzielt werden . 
hier wren die tumoren im kopf - hals - bereich , darunter nasenhauptund nasennebenhhlentumoren , speicheldrsenkarzinome und tumoren der nasen - rachenregion , bestimmte weichteilsarkome und prostataadenokarzinome , etwa 30% der hirnund rckenmarkstumoren sowie ausgewhlte bauchraumtumoren des kindesalters zu nennen [ 1 , 2 , 7 ]  . ein projektvorschlag fr den bau einer klinisch genutzten therapieanlage fr ionenstrahlung , die eng mit der radiologischen universittsklinik heidelberg kooperiert und in ihrer direkten nachbarschaft nahe dem deutschen krebsforschungszentrum gebaut werden soll , wurde ausgearbeitet . 
an ihr soll neben der bestrahlung mit kohlenstoffionen auch die therapie mit anderer teilchenstrahlung ( protonen , heliumionen ) mglich sein , um innerhalb der teilchentherapie vergleichende klinische studien durchzufhren . 
die kapazitt der anlage soll bei etwa 1 000 patienten pro jahr liegen . die investitionsund betriebskosten einer solchen anlage fhren zu behandlungskosten von etwa 40 000 dm pro patient und sind mit den kosten aufwendiger operativer und medikamentser therapieformen vergleichbar . 
im jahre 2004 knnte deutschland somit ber eine ionentherapieanlage verfgen , die eine medizinische versorgungslcke schlieen und international neue mastbe setzen wrde . die autoren mchten sich an dieser stelle bei allen bedanken , die mit groem engagement an der realisierung dieses projektes beteiligt waren . 
insbesondere den hier nicht genannten personen und arbeitsgruppen der gsi , darmstadt , des dkfz , heidelberg , des forschungszentrums rossendorf bei dresden und der universittsklinik heidelberg danken wir fr die hilfe und die gewhrte institutionelle frderung . 
ermglicht wurde das gesamtprojekt erst durch die frderung von einzelforschungsvorhaben durch das bundesministerium fr bildung und forschung , die deutsche krebshilfe und die dfg sowie durch die forschungsfrderung des universittsklinikums . 
 patienten und methodik : von juli 1998 bis dezember 1990 wur den flir die studie c - 04 ( 3 ) 2151 patienten mit dukes b ( uicc stadium ii ) und dukes c ( uicc - stadium iii ) rekrutiert . 
 ftir die behandlung wurden die patienten randomisiert inner halb einer stratifizierung , definiert durch geschlecht und tu morbefall von lymphknoten ( 0 , 1 - 4 , ~ 5 ) , urn entweder fu + fs , fu + lev oder fu + fs + lev zu erhalten . 
 ergebnisse : ein paarweiser vergleich zwischen patienten , die entweder fu + fs oder fu + lev erhiclten , zcigte eine ver langerung des dfs zugunsten der fu + fs - gruppe . 
18 pati cnten starbcn wahrend der adjuvanten therapie , davon vier in der fu + fs - , drei in der fu + levund clf in dcr fu + fs + lev - gruppe . 
 schlussfolgerung : bei patienten mit dukes - bund dukes - c karzinom des kolons scheint die adjuvantc behandlung mit fu + fs im vergleieh zu fu + lev cincn klcincn vorteil im dfs und eine grenzwertige verlangerung des os zu bewirken . 
zu alzlich mub man au h an die eben ilenen , aber ravi rend n neur logi h n zwar wirkungcn on lc ami 01 dcllken , dic hier niehl crwiihnl \ erden . 
leucovor nd i varni f the col n : result from na liems with ouk ii nal urgicaladju ant breast and bowel pr ~e t lin n col 1999 : 17 : 35539 . 
 plasmaund speichelpharmakokinetik von 5 - fluorouracil hintergrund : bei kranken , die eine chemotherapie mit 5 - fluo rouracil ( 5 - fu ) erhalten , besleht eine enge korrelation zwi schen der toxizitat und individuehen pharmakokinetischen parametern . 
der zweite therapiekurs wurde 14 tage spater mit einer dosiseskalation von s - fu um 25 , dann 50 und schlieblich 100% angesehlossen , individuell korri giert durch die auep - werte . 
die pharmakokinetik im speichel entsprach der im serum und zeigte ein biexponentielles muster : eine initiale schnelle phase mit einer halbwertszeit von durchschnittlich 8 min , die dann in eine durchschnittlich acht sttindige abklingquote tiberging . 
mit der auc im speichel kor relierte die wahrscheinlichkeit , eine mukositis zu entwickeln ( p < 0 , 001 ) , wobei diese komplikation , stomatitis und diarrho bei den 24% der patienten nachgewiesen wurden , die die hoch sten fu - speichelkonzentrationen aufwiesen . 
 i i fur d n kliniker n g , nz be onderem illlete c zu wis en , da unminclbar nach beginn d i ' infu ion bereil im peichel nachweisbar i lund 20 min piiler dart konzcnlrationen crreichl \ er den . 
dies entspricht einem anteil von 20% ( 95% - vertrauensbereich : 1328% ) , in dem die konfidenzintervalle korrekt eingesetzt wurden . schlussfolgerung : autoren , gutachter und herausgeber sollten zur hebung der qualitt der zeitschrift darauf achten , dass alle quantitativen ergebnisse mit konfidenzintervallen angegeben werden . schlsselwrter : konfidenzintervall qualittsmanagement qualittssicherung confidence intervals and their relevance for interpretation of results . 
audit of the journal strahlentherapie und onkologie background : the statistical quality of the contributions to strahlentherapie und onkologie is assessed , aiming for improvement of the journal and consequently its impact factor . material and methods : all 181 articles published during 1998 and 1999 in the categories review , original contribution , and short communication were analysed concerning the appropriate use of confidence intervals . result : forty - four publications were excluded from analysis , because they did not contain quantitative data or because the quotation of a confidence interval would not have been meaningful for other reasons . 
of the remaining 137 publications only 27 presented all relevant results with clearly defined and correctly interpreted confidence intervals . this corresponds to a fraction of 20% ( 95% ci : 1328% )  . conclusion : authors , peer reviewers , and editors could contribute to improve the quality of the journal by setting value on the documentation of confidence intervals . key words : confidence interval audit d ie vorliegende arbeit ist die erste in einer reihe von beitrgen , die dazu dienen sollen , die qualitt unserer zeitschrift zu verbessern . 
wichtige methodische grundlagen des wissenschaftlichen arbeitens werden dargestellt , gefolgt von einer diesbezglichen qualittsanalyse der letzten jahrgnge der zeitschrift strahlentherapie und onkologie . dadurch soll die qualitt der beitrge in der zeitschrift mittelfristig verbessert werden , damit sie im internationalen rahmen wieder eine wichtige rolle spielt und einen angemessenen impact factor erhlt . 
es ist geplant , diese bestandsaufnahme in etwa zwei jahren zu wiederholen , um qualitative vernderungen feststellen zu knnen . mittelwert , standardabweichung und standardfehler werden messungen wiederholt , dann erhlt man im allgemeinen nicht jedesmal exakt denselben wert , sondern die einzelnen messergebnisse schwanken um den tatschlichen 1institut fr biophysik und strahlenbiologie und 2abteilung fr radio - onkologie und strahlentherapie , universitt hamburg . eingang des manuskripts : 31 . 
der mittelwert ist der durchschnittswert aller messergebnisse : mittelwert = summe der einzelergebnisse anzahl der messungen im allgemeinen sind resultate mit messfehlern behaftet . unterschiedliche techniken knnen messfehler sehr unterschiedlichen ausmaes zur folge haben . 
durch eine grere anzahl von messungen kann die standardabweichung lediglich genauer ermittelt werden . in den meisten fllen ist von groem interesse , wie zuverlssig der mittelwert ist , der aus einzelmessungen berechnet wurde . 
man muss die standardabweichung lediglich durch die wurzel aus der anzahl der messungen dividieren : standardfehler = standardabweichung anzahl der messungen je hufiger gemessen wird , umso genauer wird der mittelwert bestimmt . 
die doppelte anzahl an messungen bedeutet nicht doppelte genauigkeit . die anzahl der messungen muss vervierfacht werden , wenn der standardfehler halbiert werden soll . die angabe des standardfehlers ( und auch der standardabweichung ) erbrigt sich , wenn alle einzelmessungen dokumentiert werden . 
dann kann sich der leser selbst ein bild von der genauigkeit der ergebnisse machen und konfidenzintervalle selber berechnen . folgen die messdaten einer ( gauschen ) normalverteilung , dann liegt der tatschliche mittelwert mit einer wahrscheinlichkeit von 68 , 27% innerhalb des durch den gemessenen mittelwert standardfehler definierten intervalls . 
das bedeutet berraschenderweise auch , dass in etwa einem drittel der flle der tatschliche mittelwert auerhalb dieses intervalls liegt , und zwar mit je einer wahrscheinlichkeit von etwa einem sechstel oberhalb und einem sechstel unterhalb des intervalls . 
fr normalverteilte daten gilt ferner , dass der wahre mittelwert mit 95% wahrscheinlichkeit in dem intervall gemessener mittelwert 1 , 96 ( cid : 2 ) standardfehler liegt ( und mit je 2 , 5% wahrscheinlichkeit darunter oder darber )  . das 95% - konfidenzintervall ist also etwa doppelt so gro wie der standardfehler . 
diese zusammenhnge knnen bei der interpretation graphischer darstellungen von ergebnissen sehr hilfreich sein . medianwert und 95% - vertrauensbereich die berechnung einer standardabweichung und eines standardfehlers ist nur dann sinnvoll , wenn die einzelergebnisse unimodal und zumindest annhernd normal verteilt sind . anderenfalls , und sicherheitshalber immer bei unbekannter verteilung , ist es sinnvoller , medianwerte und dazugehrige 95% - konfidenzintervalle zu berechnen . 
bei einer geraden anzahl messwerte ist der median der mittelwert aus den zwei zahlen , die in der mitte stehen . die ermittlung des 95% - vertrauensbereichs des medians ist ebenfalls sehr einfach . 
das 95% - konfidenzintervall ist jedoch am verbreitetsten , da man mit ihm erkennen kann , ob sich ein ergebnis statistisch signifikant ( auf 95% - signifikanzniveau , p 0 , 05 ) von einem anderen wert unterscheidet . qualittsanalyse der zeitschrift strahlentherapie und onkologie ( jahrgnge 1998 und 1999 ) alle arbeiten der rubriken aktuelles forum , originalarbeiten und kurzmitteilungen wurden von zwei beobachtern ausgewertet . 
konfidenzintervalle und die beurteilung von resultaten bei der darstellung von dosisprofilen , berechnungen und anderen problemen der bestrahlungsplanung [ 52 , 79 , 92 , 111 , 143 , 149 , 156 , 175 ]  . von den verbleibenden 137 publikationen zeigen lediglich 27 arbeiten alle resultate mit konfidenzintervall , wobei diese klar definiert und richtig interpretiert werden [ 68 , 11 , 21 , 28 , 44 , 55 , 69 , 80 , 82 , 84 , 94 , 97 , 98 , 100 , 102 , 110 , 119 , 120 , 124 , 142 , 148 , 152 , 153 , 166 , 182 ]  . 
reinbek : rowohlt , 1997 . ten war einer der autoren der vorliegenden arbeit beteiligt . in zwei arbeiten ( 1 , 5% ; 0 , 2%6% ) werden zum teil wenigstens spannweiten angegeben [ 18 , 25 ]  . 
in einer arbeit ist von einem multivariaten standardfehler die rede , den wir jedoch nicht verstanden haben [ 114 ]  . in zehn publikationen ( 7% ; 3%13% ) werden konfidenzintervalle falsch benutzt , beispielsweise bei der beschreibung der altersstruktur der patienten , etwa in der form : das durchschnittsalter der patienten betrug 64 11 jahre [ 17 , 43 , 67 , 74 , 86 , 93 , 101 , 104 , 140 , 163 ]  . 
bei sechs publikationen ( 4% ; 1%10% ) wird die standardabweichung angegeben , obwohl das 95% - konfidenzintervall oder wenigstens der standardfehler sinnvoller gewesen wren [ 24 , 38 , 54 , 78 , 135 , 154 ]  . manahmen zur qualittsverbesserung die autoren , gutachter und herausgeber der zeitschrift sollten darauf achten , dass in zukunft alle quantitativen ergebnisse mit konfidenzintervallen angegeben werden . 
hit 91 ( prospective , co - operative study for the treatment of malignant brain tumors in childhood ) : accuracy and acute toxicity of the irradiation of the craniospinal axis . 
 patienten und methode : 1m zeitraum juni 1998 bis juni 1999 wurden bei 48 hirntumorpatienten und elf patienten , die sich einer primliren prostataradiatio unterzogen , parallel ~lanungs - cr und - mrt durchgefiihrt , wobei die bildakquisi tion auch im mrt in bestrahlungsposition erfolgte . 
 ergebnisse : bei neun himtumorund bei zwei prostatakarzinompatienten fuhrte die zusatzliche obertragung der mrt - bild - information zu einer modifikation der aus der bestrahlungsplanung resultierenden feldkonformierung mit tels abschirmblticken bzw . 
 schlussfolgerung : das einfache verfahren der direktprojektion von auf mrt - aufnahmen markierten strukturen in si mulationsaufnahmen beliebiger einstrahlrichtung ermoglicht eine plausibilitatskontrolle der aus dem planungsprozess hervorgehenden feldanordnung und feldkonformierung und lasst im weiteren auch eine zielvolumenorientierte di rekteinzeichnung von ausblockungen in simulationsaufnahmen zu . 
 patients and methods : between june 1998 and june 1999 in 48 patients with brain tumors and 11 patients with carcinoma of the prostate cr treatment planning and mri were performed with identical patient positioning using the same devices as in the simulation . 
 results : for 9 patients with brain tumors and 2 patients with a carcinoma of the prostate the transposition of mri information on the simulation films showed the necessity of a modification of the shielding or the treatment portals . 
 conclusions : the simple method of direct transposition of mri structures into simulation films allows to accomplish a verification of the portals and conformation which result of the treatment planning process . 
 die hier vorgestellte moglichkeit der direkttibertragung von strukturen aus mrt - aufnahmen jeglicher schichtfiihrung in die entsprechenden simulationsaufnahmen kann in jede r einrichtung , die zugriff auf einen mrt hat . 
nach simulation der feldanordnung , die sich aus der ct - rechner - planung ergibt , erfolgt dann im ers te n schritt die obertragung des tumorvolumens von einer paramedianen auf die die medianschicht wiedergebende mrt - aufnahme . 
 in der taglichen praxis werden zwei bis drei paramediane mrt - aufnahmen benotigt , die jeweils am lichtkasten mit der medianschicht - mrt - aufnahme tiberlagert werden , urn so die maximale tumorausdehnung in diese aufnahme ein zuzeichnen . 
afterwards the sagittal mri with the transposed tumor volume is matched with the lateral simulation film ( c ) on the hr~ghtenmg screen with the help of the grid which is positioned in the plane of the central beam and of anatomical landmarks . 
hut the extension in the cranio - caudal direction can e : asily be transkrre : d by using the : grid he : e : a use : of the : ide : nticalmagnification factor . 
it is nec essary for the individualized shielding or ihe verifica tion of shielding which r . : sults of the treatment planning process 10 takl : notice of this point . 
 die aus der bestrahlungsplanung resultierende konformie rung mittels abschirmblocken wurde nach der beschriebe nen uberlagerung bei insgesamt neun hillen bei himradia tio im sinne einer volumeneinschrankung modifiziert , bei zwei patienten wnrde eine feldverbreiterung erforderlich . 
 die vorgestellte methode weist den v orzug auf , dass sie zur ubertragung auf keine weiteren elektrooptischen vorrich tungen [ 4 , 7 , 9 , 10 ] oder elektronischen bildverarbeitungs programme [ 11 ] , die das verzerrungsrisiko erhohen , zurtick greift , die differenzen , die sich aufgrund der verschiedenen aufnahmeprojektionen zwischen mrt ( parallelprojektion ) und simulation ( zentralstrahlprojektion ) bei exzentrisch ge legenen hirntumoren ergeben , liegen im bereich weniger millimeter und sind unseres erachtens filr die belange der strahlentherapie vernachlassigbar . 
we have investigated the possible role of such radiosensitivity as a marker of cancer predisposition and response to radiotherapy in the general population . results : we found that 42% ( 57 / 135 ) of breast cancer patients exhibit chromosomal radiosensitivity when lymphocytes are irradiated in the g2 phase of the cell cycle , compared with 6% ( 6 / 105 ) of healthy controls ( figure 1 )  . 
the pattern of inheritance is relatively simple and attributable to 1 or 2 genes segregating in each family ( figure 4 )  . in a prospective study of 123 breast cancer patients , 9 ( 7% ) had severe acute reactions to radiotherapy and their mean g2 sensitivity was significantly greater ( p = 0.001 ) than that of the remaining patients ( figure 5 )  . 
using another chromosomal assay ( micronucleus induction in g0 lymphocytes ) we found that the mean radiosensitivity of patients with severe late reactions was higher than that of normal reactors . 
however , the discriminatory power of these chromosomal assays is too low for them to be used alone in a clinical setting . conclusion : our results provide good evidence that genes other than atm , that confer chromosomal radiosensitivity , are involved in low penetrance predisposition to breast cancer in a high proportion of cases and contribute to adverse reactions after radiotherapy . 
 key words : chromosome aberrations radiosensitivity breast cancer cancer predisposition radiotherapy normal tissue damage chromosomale strahlenempfindlichkeit , krebsdisposition und reaktion auf strahlentherapie ziel : diese arbeit ist eine kurze zusammenfassung der untersuchungen , die whrend der vorangegangenen sechs jahre zu dem thema im department of cancer genetics , paterson institute for cancer research , manchester , england , gemacht worden sind . patienten und methode : patienten mit der rezessiv vererbten erkrankung ataxia telangiectasia , die eine erhhte krebsdisposition haben und starke reaktionen bei der strahlentherapie zeigen , haben zellen hoher strahlenempfindlichkeit , insbesondere wenn chromosomale schden als ma der strahlenempfindlichkeit verwendet werden . 
diese zahlen sind sehr viel hher als die geschtzten hufigkeiten fr trger des ataxia - telangiectasia - gens ( heterozygote ) unter brustkrebspatientinnen ( < 5% ) und bei kontrollen ( 0 , 5% )  . 
das muster der vererbbarkeit ist relativ einfach und kann einer segregation von ein oder zwei genen in jeder familie zugeordnet werden ( abbildung 4 )  . in einer prospektiven studie von 123 brustkrebspatientinnen hatten neun ( 7% ) schwere akute schden bei der strahlentherapie , und ihre mediane g2 - empfindlichkeit war signifikant hher ( p = 0 , 001 ) als die der brigen patientinnen ( abbildung 5 )  . 
bei verwendung eines anderen chromosomalen tests ( die induktion von mikronuklei in g0lymphozyten ) beobachteten wir , dass die mediane strahlenempfindlichkeit der patientinnen mit schweren sptschden hher war als diejenige bei patientinnen mit normalreaktionen . 
 schlussfolgerung : unsere ergebnisse geben gute hinweise dafr , dass andere gene als atm , die eine chromosomale strahlenempfindlichkeit bedingen , bei einer hohen zahl der flle mit niedriger penetranz der prdisposition fr brustkrebs involviert sind und zu den ungnstigen reaktionen bei der strahlentherapie beitragen . 
 schlsselwrter : chromosomenaberrationen strahlenempfindlichkeit brustkrebs prdisposition fr krebs strahlentherapie schden in normalen geweben t he content of this paper is based upon an invited lecture given at the meeting on trends of radiobiology and radiooncology 25 years radiobiology in essen , at the universittsklinikum , essen , from 15 to 17th july 1999 . 
the lecture was a review of studies in the department of cancer genetics at the paterson institute for cancer research in manchester , england , over the previous 6 years , on the relationships between cellular radiosensitivity ( measured as chromosome damage ) , predisposition to cancer and adverse reactions to radiotherapy [ 1 , 2 , 13 , 1618 ]  . 
 an association between elevated sensitivity to the chromosome - damaging effects of ionizing radiation , predisposition to cancer and enhanced susceptibility to normal tissue damage after radiotherapy was first observed in the rare , recessively inherited , multi - system disorder , ataxia - telangiectasia ( a - t ) [ 8 , 21 ]  . 
genomic instability , associated with atm mutations , is the likely cause of the high cancer susceptibility and of the defects in processing dna damage after exposure to radiation [ 9 ]  . 
these defects are manifested as an elevated cellular radiosensitivity ( chromosome aberrations and cell death ) and extreme clinical radiosensitivity after radiotherapy [ 20 ]  . cancer predisposition since the initial observation of chromosomal radiosensitivity of ataxia - telangiectasia cells , 20 other inherited cancer - prone conditions have been shown to exhibit some degree of enhanced sensitivity in such tests , although rarely to the extent seen in ataxia - telangiectasia ( references in [ 17 ] )  . 
the heterozygotes have none of the clinical symptoms of the homozygotes except for a moderately increased risk of cancer ; female carriers are reported to have an approximately 4 - fold relative risk of breast cancer [ 5 ]  . 
 [ 15 ] at the national cancer institute in the usa had earlier obtained almost complete discrimination between ataxia - telangiectasia heterozygotes and normal healthy donors using a chromosome breakage assay that involved x - irradiating cultured fibroblasts or lymphocytes in the g2 phase of the cell cycle . 
we obtained similar results using a g2 lymphocyte assay that we developed at the paterson institute [ 16 ]  . it has been estimated that approximately 5% of all breast cancer cases are ataxia - telangiectasia heterozygotes [ 5 ]  . 
this is in contrast to women who inherit mutations in the brca1 or brca2 genes ( less than 5% of breast cancer cases ) which are highly penetrant and , interestingly , appear to result in defects in the repair of radiation damage [ 24 ]  . 
unexpectedly , we found that 42% of 135 patients were g2 - sensitive [ 16 , 17 ]  . amongst 105 normal donors the frequency was 6% ( figure 1 )  . 
in view of the association between cancer predisposition and chromosomal radiosensitivity , noted above , we postulated the existence of other low penetrance genes , in addition to atm , that confer g2 sensitivity and a risk of breast cancer . 
it is conceivable that this increased sensitivity is somehow associated with the disease state of these patients , although we have seen no change in g2 sensitivity in patients tested before , and at 5 to 39 months after radiotherapy [ 13 ]  . 
chromosomal radiosensitivity and response to radiotherapy normals n = 105 cancer patients n = 135 breast cancer patients n = 135 index cases n = 16 relatives n = 37 aberrations per 100 cells figure 1 . 
chromosomale g2 - strahlenempfindlichkeit bei normalen personen ( oben ) und bei brustkrebspatientinnen ( unten )  . die gestrichelte vertikale linie gibt den schnittpunkt zwischen einer normalen und einer empfindlichen reaktion an . 
we therefore tested 69 blood relatives of 24 patients selected on the basis of their g2 scores [ 13 , 18 ]  . twenty - three of 37 ( 62% ) first degree relatives of 16 g2 - sensitive patients were also sensitive , whereas only 1 of 24 ( 4% ) first degree relatives of 8 normal - responding patients was sensitive ( figures 2 and 3 )  . 
 earlier studies of female - only blood relatives of breast cancer patients had shown that , on average , they were more g2sensitive than were normal controls , but these studies did not address the question of heritability by examining the segregation of sensitivity within families ( references in [ 13 ] )  . when we examined the distribution of g2 values among 78 family members we saw a significant trimodal distribution , suggesting the presence of a limited number of major genes determining the radiosensitivity . 
segregation analysis of family members showed clear evidence of heritability of radiosensitivity and a model with a single major gene with 2 alleles accounted for 82% of the variance between family members . 
on this model we discern 3 phenotypes : normal sensitivity ( homozygous normal ) , high sensitivity ( homozygous mutant ) and intermediate sensitivity ( heterozygous normal / mutant )  . 
the 2 alleles combine in an additive ( codominant ) manner , giving complete heterozygote expression ( families 1 and 2 in figure 4 )  . the single gene model did not adequately explain the patterns of segregation in 3 or 4 of the families . 
in these , the inclusion of a second bi - allelic gene with co - dominant expression and a similar effect on radiosensitivity to that of the first aberrations per 100 cells figure 2 . 
chromosomale g2 - strahlenempfindlichkeit von nicht ausgewhlten brustkrebspatientinnen ( oben ) , patientinnen mit empfindlichen reaktionen ( mitte ) und verwandten ersten grades der empfindlichen patientinnen ( unten ) ( nach [ 13 ] mit erlaubnis der american society of human genetics )  . gene , gave a significantly improved fit to the data . 
 at present the identity of the putative genes is not known . they appear to be involved in the processing of dna damage of the type induced by ionizing radiation , mutants ( or variants ) are relatively common in the normal population and at high frequency amongst breast cancer patients . 
the observed number of breast cancers in 18 first or second degree relatives of the sensitive index cases was 3 , the expected number being 1.35 , derived from regional cancer statistics . 
chromosomal radiosensitivity and response to radiotherapy breast cancer patients n = 135 index cases n = 8 relatives n = 24 ns , nn ( nn ) ( ns or ss ) ( nn ) ns , ns ns , ns nn , nn ns , ns aberrations per 100 cells figure 3 . 
chromosomale g2 - strahlenempfindlichkeit von nicht ausgewhlten brustkrebspatientinnen ( oben ) , patientinnen mit normalen reaktionen ( mitte ) und verwandten ersten grades der normal reagierenden personen ( unten ) ( nach [ 18 ] )  . nn , nn ns , nn ns , nn ns , nn the next step is to attempt to identify the underlying genes by genetic linkage studies or a candidate gene approach . the former method will be aided by the relatively large effect of the mutant genes on radiosensitivity , but the possible presence of multiple genes could be a complicating factor . 
if the genes can be identified this could lead to more effective targeting of medical resources , for example , for mammography and preventative chemotherapy , to women at greatest risk . 
this could potentially have a major impact on breast cancer incidence , bearing in mind that almost half of breast cancers arise in carriers of these mutant genes . response to radiotherapy the elevated chromosomal radiosensitivity of ataxia - telangiectasia cells is the likely reason for their enhanced susceptibility to radiation - induced cell death , which is manifested as extreme , life - threatening , normal tissue damage after radiotherapy [ 7 ]  . 
pedigrees of families 1 , 2 and 8 showing putative genotypes based on the single gene ( families 1 and 2 ) or 2 gene ( family 8 ) model . 
stammbume der familien 1 , 2 und 8 , die basiert auf dem ein - gen ( familien 1 und 2 ) oder zwei - gen - modell ( familie 8 ) putative genotypen zeigen . 
chromosomal radiosensitivity and response to radiotherapy normal acute reactions n = 114 normal fibrosis n = 39 severe acute reactions n = 9 severe fibrosis n = 8 aberrations per 100 cells figure 5 . 
die vertikalen linien geben mediane werte an ( modifiziert nach [ 2 ] )  . in a prospective study , we applied the g2 assay to 123 breast cancer cases prior to their radiotherapy [ 2 ]  . 
nine of the patients were judged to have severe reactions , manifested as very severe erythema , sufficient to warrant premature termination of the treatment schedule or to cause moist desquamation or severe edema . 
the g2 sensitivity of these highly radiosensitive ( hr ) patients was significantly greater ( p = 0.001 ) than that of the remaining patients , but there was complete overlap between the values of the 2 groups ( figure 5 )  . 
in this test , lymphocytes were irradiated in the g0 stage of the cell cycle and chromosome damage was assessed by quantifying micronuclei ( mn ) , which arise mainly from chromosome fragments , in cells that have undergone 1 mitotic division after irradiation [ 5 ]  . 
bildung von strahleninduzierten mikronuklei in g0lymphozyten von brustkrebspatientinnen , bei denen eine normale ( oben ) oder schwere ( unten ) fibrose nach strahlentherapie auftrat . die zellen wurden mit 3 , 5 gy gammastrahlen bei hoher dosisleistung bestrahlt . 
vertikale linien geben mediane werte an ( modifiziert nach [ 2 ] )  . reactions of 5% , the predictive value would be low ; only about 20% of patients with a positive test would be true severe reactors . there are 3 main conclusions from our studies . 
firstly , that since our family studies of chromosomal radiosensitivity have indicated that it is a heritable trait ( at least with the g2 assay ) , there would appear to be a genetic contribution to enhanced clinical radiosensitivity in breast cancer patients . secondly , that since our ability to discriminate between normal and hr reactors is rather poor , there must be factors other than cellular radiosensitivity ( measured as chromosome damage ) that contribute to adverse reactions . 
in our own studies we have identified patient age ( for acute reactions ) and variations in treatment volume and dose homogeneity ( for late reactions ) as significant confounding factors . 
it is nevertheless encouraging that predictive tests involving the use of peripheral blood lymphocytes , a readily available source of cells , are able to identify patients with hr reactions as effectively , if not more so , than tests involving the use of skin fibroblasts [ 14 ]  . 
because of the modest degree of enhanced radiosensitivity ( measured as clonogenic survival ) exhibited by fibroblasts and lymphocytes of ataxia - telangiectasia heterozygotes , it had been widely predicted that a high proportion of severely reacting breast cancer cases would be carriers of mutations in the atm gene [ 4 ]  . 
this prediction was also based on the close numerical relationship between the proportion of patients who typically exhibit adverse reactions and the estimated frequency of ataxia - telangiectasia heterozygotes among breast cancer cases ( about 5% in both cases )  . however , when we screened 16 patients who had shown severe acute reactions we found no atm mutations [ 1 ]  . 
later studies on patients with severe late reactions [ 19 ] confirmed our conclusion that the genetic contribution to hr reactions in breast cancer cases must come largely from mutations of genes other than those in atm . conclusions the observation of elevated chromosomal radiosensitivity in ataxia - telangiectasia patients led us to investigate the possibility of a wider role for such sensitivity in cancer predisposition and response to radiotherapy . 
our results provide good evidence that genes other than atm that confer chromosomal radiosensitivity , are involved in low penetrance predisposition to breast cancer in a high proportion of cases and contribute to adverse reactions after therapy . 
the challenge now is to identify these genes in order to predict cancer susceptibility and the risks associated with treatment . i would like to thank all my colleagues and collaborators , listed as authors in publications [ 1 , 2 , 13 , 1618 ] , cited below , for their valuable contributions to this work . 
funding for these studies has been provided by the cancer research campaign , the christie hospital endowment fund , the national radiological protection board and the uk coordinating committee on cancer research . strahlentherapie und onkologie urban & vogel 2000 originalarbeit erste erfahrungen mit einem nichtinvasiven patientenfixierungssystem fr die stereotaktische strahlentherapie der prostata klaus k . 
wir stellen ein neues fixierungssystem fr die stereotaktisch gefhrte , intensittsmodulierte strahlentherapie ( imrt ) im beckenbereich im hinblick auf die positionierungsgenauigkeit der prostata vor . material und methode : das neue fixierungssystem besteht aus einer umschlieenden krpermaske aus scotchcast , die vom abdomen bis zu den distalen abschnitten der oberschenkel reicht , sowie einer kopfmaske aus dem gleichen material . 
zur bestimmung der lagerungsprzision wurden bei zwei patienten insgesamt 16 ct - untersuchungen ( 25 schichten , 3 mm schichtdicke ) jeweils unmittelbar vor oder nach einer bestrahlung mit markierung des bestrahlten isozentrums durchgefhrt . die abweichungen von knchernen strukturen sowie von anatomischen strukturen innerhalb des zielvolumens wurden dann in allen drei dimensionen gemessen . ergebnisse : mittlere positionierungsfehler von 0 , 15 0 , 3 mm ( laterolateral ) , 0 , 9 1 mm ( anterior - posterior ) , 1 1 mm ( transversaler vektorieller fehler ) und < 3 mm schichtdicke ( kraniokaudal ) wurden unter bezug auf kncherne orientierungspunkte ermittelt ; whrend 0 , 9 0 , 9 mm ( laterolateral ) , 1 , 8 1 , 5 mm ( anterior - posterior ) , 2 , 2 1 , 5 mm ( transversaler vektorieller fehler ) und < 3 mm ( kraniokaudal ) fr die abweichungen von prostatabegrenzung oder in der prostata gelegenen orientierungspunkten festgestellt wurden . 
die hufig als mazahl fr den positionierungsfehler verwendete standardabweichung der absoluten patientenbewegung lag in der transversalebene zwischen 0 , 3 und 1 , 7 mdie transversale vektorielle maximalabweichung der prostata lag bei 4 , 4 mm . schlussfolgerung : das vorgestellte fixierungssystem ermglicht eine sehr genaue und zuverlssige patientenpositionierung fr die behandlung von extrakraniellen tumoren . 
da die relativpositionierungsgenauigkeit der zielstruktur gegenber dem knchernen skelett variabler ist als die positionierungsgenauigkeit des skeletts , ist durch reine externe immobilisierungsmanahmen keine weitere verbesserung mglich . schlsselwrter : nichtinvasive patientenfixierung positionierungsgenauigkeit extrakranielle stereotaxie intensittsmodulierte strahlentherapie imrt prostatakarzinom first experiences with a noninvasive patient set - up system for radiation therapy of the prostate purpose : highly conformal radiotherapy techniques require precise patient positioning . 
we report our first experience with a new cast system for fixation of the pelvis during stereotactically guided intensity modulated radiotherapy ( imrt ) of the prostate with respect to positioning accuracy of the prostate . material and methods : the immobilization device consists of a custom - made wrap - around body cast that extends from the abdomen to the thighs and a separate head mask , both made from scotchcast , and attaches to a frame for extracranial stereotaxy . 
sixteen ct - studies ( 25 slices , thickness : 3 mm ) of 2 patients who were immobilized for imrt of prostate tumors were evaluated with respect to set - up accuracy of bony structures and the prostate itself . 
the worst case transversal vectorial deviation for the prostate was 4.4 mfigure 4 summarizes the set - up accuracy of bony landmarks and the prostate . conclusion : the presented combination of a body cast and head mask system in a rigid stereotactic body frame ensures reliable noninvasive patient fixation for fractionated extracranial stereotactic radiotherapy . 
no further improvement of repositioning can be achieved with external immobilization devices since the positioning error of the target relative to the skeleton exceeds the accuracy of the positioning of the skeleton itself . key words : noninvasive patient immobilization set - up accuracy fractionated extracranial stereotactic radiotherapy imrt prostate tumors z ahlreiche fixierungssysteme mit unterschiedlicher przision stehen fr die patientenfixierung im rahmen der behandlung von kopf - hals - tumoren zur verfgung . 
systeme , die auf thermoplastischen kunststoffen basieren , gewhrleisten eine ausreichende przision fr die konventionelle behandlung von tumoren im hno - bereich [ 20 , 29 ]  . nur rigide maskensysteme erfllen die anforderungen , die neue przise bestrahlungsverfahren wie die teilchentherapie , die dreidimensional geplante konventionelle konformationsstrahlentherapie ( crt ) mit photonen oder die invers geplante intensittsmodulierte strahlentherapie ( imrt ) an die patientenlagerung stellen [ 6 , 14 , 27 , 28 ]  . 
neben dem verbreiteten alpha - cradle system , das jedoch nicht in einem stereotaxiesystem integriert ist , kommen vakuummatratzen - systeme in stereotaktischen basisgerten zum einsatz [ 5 , 13 , 18 ]  . 
problematisch ist jedoch die im vergleich zu den kopf - hals - systemen deutlich geringere przision , die nur durch aufwendige positionierungskontrollen und gegebenenfalls positionierungskorrekturen reduziert werden kann [ 13 ]  . 
wir haben krzlich ein neu entwickeltes nichtinvasives fixierungssystem fr die extrakranielle stereotaktisch gefhrte strahlentherapie beschrieben , mit dem sich affektionen im wirbelsulenbereich mit hoher przision behandeln lassen [ 19 ]  . 
krpermaske , kopfmaskensystem und basissystem fr die extrakranielle stereotaktisch gefhrte strahlentherapie das im rahmen dieser untersuchungen verwandte fixierungssystem wird mit einem am deutschen krebsforschungszentrum entwickelten lokalisationssystem ( kommerziell erhltlich durch leibinger , freiburg ) fr die extrakranielle stereotaktisch gefhrte strahlentherapie verbunden [ 5 ]  . 
ein stereotaktischer metallgrundring trgt wechselweise entweder v - frmige lokalisatoren , die whrend der bestrahlungsplanungsuntersuchung im ct ein stereotaktisches koordinatensystem aufspannen , oder ein schieblehrensystem , mit dem das errechnete isozentrum im bestrahlungsraum stereotaktisch eingestellt wird . 
die eigentliche patientenfixierung kann dann mit hilfe von vakuummatratzen [ 5 , 13 ] oder mit hilfe des neu entwickelten krpermaskensystems auf scotchcast - basis durchgefhrt werden [ 19 ]  . 
dabei wird der patient auf ein etwa 20 cm breites brett gelagert , das mehrere bohrungen fr schraubverbindungen besitzt . patient und brett werden dann mit maskenmaterial ( scotchcast ) umwickelt und zur aushrtung auf ein basisbrett gehoben , das mit dem schmalen brett ber schrauben verbunden wird und die kopplung an das stereotaxiesystem herstellt . 
die patienten wurden wchentlich in fixierung mit stereotaktischen lokalisatoren und metallmarkierung des bestrahlten isozentrums unmittelbar vor oder direkt nach der bestrahlung im ct untersucht ( abbildungen 2a bis 2d )  . 
patientenfixierung fr stereotaktische prostatabestrahlung dann die abweichung des bestrahlten vom geplanten isozentrums auf groen ct - folien ( mastab 1 : 1 , 4 ) in allen drei dimensionen bestimmt , wobei die abweichung in lngsrichtung aufgrund der schichtdicke nur mit > 3 mm oder < 3 mm angegeben werden konnte . 
daher wurden unterschiedliche orientierungspunkte fr die abweichung in xund y - richtung verwandt ( laterale abweichung : symphysenspalt ; anterior - posteriore abweichung : symphysenvorderkante ; jeweils im definierten abstand zum koordinatenursprung )  . 
zur bestimmung der abweichungen des bestrahlten vom geplanten isozentrum fr die prostata in der transversalebene wurden die mittleren abstnde von vorderund hinterrand der prostata ( fr die anterior - posteriore abweichung ) am jeweils grten durchmesser vom stereotaktischen nullpunkt whrend der therapieplanung mit den werten bei den kontrollen bzw . 
planungs - ct ( a ) mit markierung des geplanten isozentrums ( pfeil ) sowie drei reprsentativen ct - schichten mit metallmarkierung des bestrahlten isozentrums ( pfeile ) entsprechend der lasermarkierungen auf der krpermaske . 
bei beiden patienten wurde das prostatakarzinom mittels transrektaler biopsie gesichert . weiterfhrende staginguntersuchungen mit ct , mrt und sonographie statuierten je ein t3und t4 - tumorstadium ohne hinweis auf regionalen lymphknotenbefall oder fernmetastasen . 
beide patienten wurden aufgefordert , whrend der behandlung auf meteorismusfrdernde speisen zu verzichten und auf eine auf die behandlung abgestimmte blasenund mastdarmleerung zu achten . die bestrahlungsplanung erfolgte invers mit hilfe des im deutschen krebsforschungszentrum entwickelten bestrahlungsplanungsprogramms konrad [ 25 ]  . 
nach stereotaktischer einstellung des zielpunktes wurde die bestrahlung an einem primus - linearbeschleuniger ( siemens , concord , usa ) mit 15 - mev - photonen unter verwendung eines integrierten , motorgetriebenen multileafkollimators mit 10 mm leafbreite durchgefhrt . 
die zeit fr die tgliche lagerung inklusive zielpunkteinstellung betrgt etwa zehn minuten . ergebnisse die herstellungszeit fr eines der beschriebenen kopf - krper - maskensysteme betrgt etwa drei bis vier stunden . 
folgende mittelwerte standardabweichung des betrags der individuellen abweichungen des bestrahlten vom geplanten isozentrum wurden fr die knchernen beckenstrukturen als referenz ermittelt : 0 , 15 0 , 3 mm ( laterolateral ) , 0 , 9 1 mm ( anterior - posterior ) , 1 1 mm ( vektorieller fehler in der transversalebene )  . die kraniokaudale abweichung wurde mit lediglich einer ( 1 / 16 ) ausnahme ( 3 bis 6 mm ) als < 3 mm schichtdicke bestimmt . 
die abbildungen 2a bis 2d zeigen das bestrahlungsplanungs - ct mit markierung des geplanten isozentrums ( abbildung 2a ) und drei reprsentative , im verlauf der lagerungskontrollen aufgenommene ct - schichten mit markierung des jeweils bestrahlten isozentrums ( abbildungen 2b bis 2d )  . 
abbildung 4 stellt die individuellen abweichungen in der transversalebene graphisch dar . die samenblasen wurden als variabelste struktur mit einer mittleren vektoriellen abweichung in der transversalebene von 4 , 3 3 , 4 mm ermittelt . 
4 , 2 3 , 2 mm lag . diskussion zahlreiche publikationen weisen auf eine dosis - wirkungbeziehung bei der lokalen strahlenbehandlung des prostatakarzinoms hin [ 10 , 24 ]  . 
selbst bei berprfung mittels portfilmen und gegebenenfalls korrektur der positionierung vor jeder fraktion wurde eine standardabweichung von 2 , 2 bis 2 , 7 mm mit maximalabweichungen von bis zu 9 , 5 mm beobachtet [ 12 ]  . schalenartige systeme wie das alpha - cradle - system oder vakuummatratzen reduzieren die standardabweichung auf etwa 2 mm in der transversalebene , sind jedoch ebenfalls mit hohen maximalfehlern von 7 bis 10 mm vor allem in longitudinaler richtung sowie dreidimensionalen vektorfehlern von > 5 mm in einem drittel der untersuchten flle behaftet [ 3 , 7 , 16 ] , so dass interaktive korrekturen nach der jeweiligen lagerungskontrolle notwendig sind , um eine hohe lagerungsprzision zu gewhrleisten [ 13 ]  . 
um die tatschliche position der prostata zu detektieren , mussten diese kontrollen bisher aufwendig mittels ct durchgefhrt werden . ein neues , ultraschallbasiertes system kann die ct - kontrollen mglicherweise ersetzen [ 17 ]  . erste untersuchungen mit einem kathetersystem zur prostatapositionierung in der transversalebene verliefen vielversprechend [ 2 ]  . 
bisher ist jedoch die korrektur von fehlern in der longitudinalen ebene sowie von rotationsfehlern nicht mglich . wir stellten krzlich ein neu entwickeltes nichtinvasives fixierungssystem fr die extrakranielle stereotaxie auf basis von scotchcast - maskenmaterial vor [ 19 ] , ber dessen erste anwendung im beckenbereich wir hier berichten . 
wir entschlossen uns , die erreichbare przision zunchst bei zwei patienten , dafr jedoch mit regelmigen ct - lagerungskontrollen , durchzufhren , um im rahmen der imrt von prostatakarzinomen schnell zu einer abschtzung der mglichkeiten des systems zu gelangen . 
interaktive korrekturen der positionierung sind nicht notwendig , es bleibt lediglich der beschriebene minimale zufllige lagerungsfehler , der mit einer transversalen standardabweichung von 0 , 3 bis 1 , 7 mm fr die prostata im bereich der bisher therapierten , hauptschlich paraspinalen regionen ( standardabweichung von 1 , 4 bis 1 , 9 mm ) , und damit an der grenze der auflsung der bildgebenden verfahren liegt . 
insbesondere die kombination mit einer kopfmaske sowie die lagerung mit angewinkelten beinen gewhrleisten eine sichere lngsfixierung , welche bei den anderen systemen das hauptproblem darstellt . die lagerungsvariabilitt der knchernen strukturen war im vergleich zur bildauflsung uerst gering . 
eine die konventionelle konformationsbestrahlung ( crt ) mit verschiedenen imrt - techniken vergleichende planungsstudie konnte fr die bestrahlung komplex geformter tumoren , adhrent zu dosislimitierenden risikoorganen , eine gesteigerte tumorkonformitt und damit einhergehende mglichkeit der dosiseskalation bei gleicher respektierung der risikoorgane fr alle imrt - techniken nachweisen [ 22 ]  . 
die komplexen dosisverteilungen mit steilen dosisgradienten am bergang von tumor zu normalgewebe , die auf diese art erzeugt werden knnen , stellen jedoch erhhte anforderungen an die patientenpositionierung [ 23 ]  . verschiedene mazahlen werden in der beschreibung der lagerungsprzision verwandt . 
von bedeutung ist auch die jeweils beobachtete maximalabweichung . bei lagerung ohne zustzliche hilfsmittel wurden fr die prostata standardabweichungen von 3 , 6 bis 6 , 1 mm [ 26 ] bzw . ein mittelwert des dreidimensionalen fehlervektors von 8 , 66 4 , 95 mm [ 4 ] beobachtet . 
patientenfixierung fr stereotaktische prostatabestrahlung unter den gegebenen umstnden die gesamtbeweglichkeit der prostata so gering , dass bei rigider zirkumferentieller fixierung des beckens und relativ gleich bleibender rektumund blasenfllung eine zustzliche invasive fixierung der prostata wahrscheinlich unterbleiben kann . 
da die relativpositionierungsgenauigkeit des zielvolumens gegenber dem knchernen skelett grer ist als die positionierungsgenauigkeit des skeletts , ist durch reine externe immobilisierungsmanahmen keine weitere verbesserung mglich . die einstrahlrichtungen bei einer solchen stereotaktischen bestrahlung im krperstammbereich sind in hinblick auf den tisch und darauf liegenden patienten auf vor allem koplanare oder nur leicht angewinkelte nonkoplanare felder beschrnkt . 
int j radiat oncol biol phys 1998 ; 41 : 107986 . zusammenfassend ermglicht das vorgestellte system neben der przisen behandlung von wirbelsulentumoren auch die zuverlssige positionierung der prostata und damit die konformierende strahlentherapie von prostatatumoren ohne invasive fixierung . 
wenn sich die przision des systems im tglichen gebrauch an greren patientenzahlen besttigt , ist eine deutlich bessere schonung der risikoorgane im rahmen von dosiseskalationsstudien zur prostatabestrahlung mglich . wir bedanken uns herzlich bei a . 
this is an investigation of the image quality and time requirement of a new verification film system compared to a conventional portal film system . material and methods : for conventional verifications we used agfa curix ht 1000 films which were compared to the new kodak ec - l film syste344 agfa curix ht 1000 and 381 kodak ec - l portal films of different tumor sites ( prostate , rectum , head and neck ) were visually judged on a light box by 2 experienced physicians . 
subjective judgement of image quality , masking of films and time requirement were checked . results : in this investigation 68% of 175 kodak ec - l ap / pa - films were judged good , only 18% were classified moderate or poor 14% , but only 22% of 173 conventional ap / pa verification films ( agfa curix ht 1000 ) were judged to be good . conclusions : the image quality , detail perception and time required for film inspection of the new kodak ec - l film system was significantly improved when compared with standard portal films . 
they could be read more accurately and the detection of set - up deviation was facilitated . key words : portal film image quality verification in radiotherapy portal imaging ein neues film - folien - system fr verifikationsaufnahmen von bestrahlungsfeldern : kodak ec - l ziel : vergleich von bildqualitt , bildbetrachtungszeit und anzahl der kontrollaufnahmen bei verifikationsaufnahmen mit einem herkmmlichen ( agfa curix ht 1000 ) und einem neuen film - folien - system ( kodak ec - l )  . material und methode : bei den bestrahlungsserien von drei unterschiedlichen tumorlokalisationen ( prostata , rektum und kopf / hals ) wurden die verifikationskontrollen zweier film - folien - systeme verglichen . 
die bildqualitt beider film - folien - systeme wurde mit einem subjektiven fragebogen erfragt , einblendungsbedarf und die bildbetrachtungszeit wurden erfasst . ergebnisse : bei der auswertung der ap / pa angefertigten verifikationsaufnahmen wurden 68% der 175 aufnahmen der kodak - ec - l - filme , aber nur 22% der 173 herkmmlichen agfa - curix - ht - filme als gut klassifiziert . schlussfolgerung : die bildqualitt der neuen kodak - ec - l - filme war signifikant besser und erleichterte die auswertung der verifikationsaufnahmen . 
so wurden relevante abweichungen seit der umstellung auf das neue film - foliensystem besser erkannt . schlsselwrter : verifikationsaufnahmen film - folien - system bildqualitt portal imaging c onformal irradiation techniques reduce the treated volume and may allow dose escalation in the target volume without increasing side effects . 
portal film systems and portal imaging show the position of the radiation fields with regard to the anatomic structures and are established methods to detect set - up deviations [ 1 , 6 ]  . 
verification film system for quality control material and methods in our portal film evaluation we retrospectively compared the broadly used agfa curix ht 1000 a in cronex 2 mm cassette with the new kodak ec - l film system ( see figure 1 for the decrease of required dose with ec - l film )  . 
during treatment sessions we exposed the verification films to a specific number of monitor units applying specially developed exposure tables for the kodak ec - l [ 13 ]  . 
for both types of films we used the same development machine ( an agfa curix 242 u ) and , in order to compare the quality of the developed films a light box ( luminous density : 2000 cd / m2 ) with a mask option for focussing the light on a special part of the film . all verification films of a complete irradiation series of several patients with different tumor sites were included in the evaluation : 18 patients with prostate carcinomas ( 214 films ) , 24 with rectum carcinomas ( 237 films ) and 26 with head and neck carcinomas ( 274 films )  . 
sensitometric curves of the agfa ht 1000 a in standard cassette ( cronex , 2 mm lead , reflecting walls ) and kodak ec - l system ( ec - l film in ec - l cassette ) for 5 - mv photons . 
sensitometrische kurve von agfa ht 1000 a in einer standardkassette ( 2 mm blei , verspiegelte oberflchen ) und vom kodak - ec - l - film - folien - system ( ec - l - film in ec - l - kassette ) fr 5 - mv - photonen . 
only 22% of 173 conventional ap / pa verification films ( agfa curix ht 1000 ) were judged to be good , the rest was classified as moderate ( 34% ) or poor ( 44% )  . 
however , 68% of 175 kodak ec - l films were judged good and only 32% were classified moderate ( 18% ) or poor ( 14% )  . the relative enhancement of image quality with the new kodak ec - l was even more pronounced when the results of lateral verification films were evaluated . 
kodak - ec - l - verifikationsaufnahme : kopf - hals - region . films were judged poor ( 56% good and 27% moderate ) but 57% of the conventional verification films were judged poor ( 7% good and 36% moderate )  . 
 details details of our evaluation are shown in tables 1 and 2 . pictures of verification films from different body locations which were judged to be good are shown in figures 3 and 4 . discussion recognition time the number of ap / pa films with an image quality allowing a recognition of bony anatomical structures in less than 5 seconds increased from 29% for conventional films up to 66% for the new systefor this purpose we measured the time to recognize the bony anatomic markers . looking at the results on lateral verification films the percentage of quickly analyzable films increased 4 times when using the kodak ec - l . 
for smaller field sizes like prostate fields this effect is not so impressive because of the reduction of bony landmarks , but the percentage of quickly analyzable films was still increased more than a factor of 2 when using the kodak ec - l ( see table 2 )  . need for masking the need for masking decreased from 54 to 14% in ap / pa when using the new films instead of the conventional film syste for lateral verification films the use of the kodak ec - l reduces the need for masking to a quarter . number of simulations using the new kodak - ec - l film system for verification raised the number of resimulations during the irradiation series by a factor of 1.2 ( independently of the tumor site )  . although in this investigation the differences of image quality of both verification film systems were judged mostly by subjective criteria the new kodak ec - l verification films demonstrate substantially better contrast in the clinical routine ( see figures 1 and 2 and the literature [ 3 , 5 ] )  . they show remarkably more details of bony anatomic structures ( see figures 3 and 4 )  . 
even in smaller irradiation fields with only rare anatomic landmarks the better contrast of this film helps the observer to find set - up deviations more quickly ( see table 2 , lateral prostate verification films )  . 
instead of resimulation in the patients also a direct correction of the set - up deviation at the treatment unit is now better possible . the use of the specially developed exposure tables for the kodak ec - l system helps to avoid a misexposure [ 3 ] and the verification has only to be repeated in the few cases when films are judged poor . 
therefore , the kodak ec - l film screen system substantially helps to improve the systematic quality management in the daily radiation therapy which is a basic condition for future development of conformal irradiation techniques . of course we believe that electronic portal imaging systems will increasingly assert themselves , especially when they will be part of an integrated planning and therapy systebut special cases like adjoining or non - coplanar fields will continue to remain a domain of the portal film systems in the near future . strahlentherapie und onkologie urban & vogel 2000 originalarbeit supratentorial low - grade glioma : results and prognostic factors following postoperative radiotherapy gerhard g . 
huk4 , rolf sauer1 background and purpose : to assess treatment outcome and prognostic factors following postoperative external radiotherapy in 77 patients with low - grade glioma . patients and methods : between 1977 and 1996 , 45 patients with astrocytoma , 14 with oligodendroglioma and 18 with mixed glioma received postoperative radiotherapy with a median total dose of 52 gy ( range , 45 to 61 gy )  . 
the influence of various factors including histology , gender , age , seizures , duration of symptoms ( 6 weeks vs > 6 weeks ) , ct pattern ( enhancement vs no enhancement ) , type of surgery , total radiotherapy dose and timing of radiotherapy on relapse - free survival and overall survival was investigated . results : the median overall survival time was 81 months , the 5and 10 - year survival rates were 54% and 31% , respectively . 
univariate analyses identified the total radiotherapy dose ( p = 0.01 ) , duration of symptoms ( p = 0.05 ) , the presence of seizures ( p = 0.04 ) , and the ct pattern following intravenous contrast ( p = 0.005 ) as significant prognostic factors for overall survival . 
on multivariate analysis , only the ct pattern ( enhancement vs no enhancement ) remained as independent prognostic factors for both progression - free survival and overall survival . conclusion : a minimum total dose of 52 gy is recommended for the postoperative radiotherapy in low - grade glioma . tumors with ct enhancement seem to need further intensification of treatment . key words : low - grade glioma radiotherapy prognostic factors supratentorielle low - grade - gliome : ergebnisse und prognosefaktoren nach postoperativer radiotherapie hintergrund : es sollten ergebnisse und prognosefaktoren nach postoperativer radiotherapie bei 77 patienten mit low - grade - gliomen evaluiert werden . patienten und methoden : zwischen 1977 und 1996 wurden 45 patienten mit einem low - grade - astrozytom , 14 mit einem oligodendrogliom und 18 mit einem gemischten gliom postoperativ bis zu einer medianen gesamtdosis von 52 gy bestrahlt ( spanne zwischen 45 und 61 gy )  . 
in univariaten analysen wurden die gesamtdosis der radiotherapie ( p = 0 , 01 ) , die dauer der symptome ( p = 0 , 05 ) , das vorhandensein von anfllen ( p = 0 , 04 ) und die kontrastmittelaufnahme im prtherapeutischen ct ( p = 0 , 005 ) als signifikante prognosefaktoren fr das gesamtberleben identifiziert . 
die progressionsfreie berlebensrate wurde durch die gesamtdosis der radiotherapie ( p = 0 , 04 ) , die dauer der symptomatik ( p = 0 , 01 ) und die kontrastmittelaufnahme im ct ( p = 0 , 006 ) beeinflusst . 
supratentorial low - grade glioma s upratentorial low - grade gliomas comprise between 10 and 15% of all primary brain tumors and between 25 and 30% of gliomas in adults . 
following surgery and postoperative radiotherapy patients with supratentorial low - grade gliomas can expect 5 - , 10and 15 - year survival rates of 40 to 50% , 20 to 30% and 10 to 15% , respectively [ 1 , 4 , 10 , 1720 , 22 , 23 , 35 , 37 , 43 ]  . 
firstly , the optimal timing of postoperative radiotherapy is unclear . while several studies indicated improved outcome in terms of overall survival rates by immediate postoperative radiotherapy [ 17 , 18 ] others could not demonstrate such an effect [ 19 , 22 , 23 ]  . 
some retrospective data indicated an advantage for patients treated with a dose above 54 gy [ 33 , 43 ] , while in other series prognosis was not influenced by the applied total dose of radiotherapy [ 22 , 36 ]  . in an attempt to improve the overall survival rates it seems desirable to first identify patient groups being at higher risk for early progression than average group patients . 
experimental approaches such as hyperfractionated radiotherapy [ 9 ] , radiochemotherapy [ 3 , 15 ] and dose escalation studies by the use of stereotactic and 3d conformal techniques [ 6 , 25 , 26 , 39 ] could thereby specifically be targeted to those high - risk patients while excluding the subgroup of patients with good results after standard treatment . 
it was the purpose of this retrospective study to assess treatment outcome and possible prognostic factors in a group of patients with low - grade glioma being uniformly treated by surgery and postoperative radiotherapy . patients and methods patients with the following criteria were retrospectively identified in the database of the departments of radiation oncology , neurosurgery and the cancer registry of the university of erlangen - nrnberg : a histopathologic diagnosis of low - grade glioma ( who grade ii ) including astrocytoma , mixed glioma and oligodendroglioma [ 45 ] established by biopsy or resection , an age between 18 and 65 years , tumor location was required to be supratentorial , and radiation treatment had to be delivered by megavoltage techniques with a minimum total dose of 45 gy . 
forty - five patients ( 58% ) had low - grade astrocytoma , 14 ( 19% ) had oligodendroglioma and 18 ( 23% ) mixed glioma . there were 32 male ( 42% ) and 45 female ( 58% ) patients with a median age of 39 years ( range , 19 to 64 years )  . 
fifty ( 65% ) patients had a previous history of seizures , motor disorders were present in 25 patients ( 33% ) , headache in 15 ( 20% ) , speech disorders in 20 ( 26% ) , memory deficits in 15 ( 20% ) , a psychosyndrome in 19 ( 25% ) and objective signs of elevated intracranial pressure with papilledema in 17 ( 22% ) patients . median time between onset of the first symptom and diagnosis of low - grade glioma was 6 months ( range , 1 to 84 months )  . data on the functional category ( mrc scores [ 2 ] ) were available in all patients with 53 ( 69% ) having a normal activity , 10 ( 13% ) a partial incapacity and 14 ( 18% ) a total incapacity . patients characteristics are outlined in detail in table 1 . 
based on neurosurgical reports and / or postoperative ct / mri images the extent of surgery was defined as total / subtotal ( 50 to 90% tumor reduction ) or partial resection / biopsy ( < 50% tumor reduction )  . 
thirty - six ( 47% ) lesions were classified as contrast enhancing and 27 ( 53% ) remained isodense following intravenous contrast , a mass effect was diagnosed in 29 ( 38% ) of the patients . postoperative radiotherapy was administered using co - 60 in 18 ( 23% ) patients and 6to 10 - mv photons in 59 ( 73% ) patients . 
the clinical target volume encompassed the contrast total number of patients histology gender age at diagnosis tumor location mrc - score seizures duration of symptoms ct pattern type of surgery treatment era single fraction total dose astrocytoma oligodendroglioma mixed glioma male female 1930 years 3139 years 4049 years 5164 years frontal temporal parietal occipital basal ganglia normal activity partial incapacity 6 weeks > 6 weeks not available enhancement no enhancement not available biopsy , partial subtotal , total 19771985 19861996 170180 cgy 200 cgy 250 cgy 4550 gy 50.455 gy 5661 gy table 1 . 
supratentorial low - grade glioma enhanced area including edema ( whenever present ) and a 2 cm safety margin and for the non - enhancing tumors the hypodense area was covered with an identical margall patients were treated by an uninterrupted course of conventionally fractionated external radiotherapy with a median single fraction size of 180 cgy and a median total dose of 5 , 200 cgy . only multiple field techniques were applied with a minimum of 2 to 3 portals . 
survival and progression - free survival were calculated according to kaplan and meier [ 11 ] , differences between curves were evaluated by means of the log - rank test . 
median follow - up was 7.5 years with a range between 3 and 21 years . results overall survival and progression - free survival rates for all 77 patients were 54% and 45% at 5 years and 31% and 24% at 10 years , respectively . 
sixty - two ( 81% ) patients experienced a tumor progression or recurrence during follow - up and 56 ( 73% ) of the patients died as a result of tumor progression . 
the final model during the multivariate cox regression analysis revealed the pattern of ct enhancement ( p = 0.01 ) as the only independent prognostic factors for overall survival as endpoint ( table 2 )  . 
the influence of the patterns of ct enhancement and the applied total radiotherapy dose on overall survival are outlined in figures 3 and 4 . the following factors were of no significant impact on overall survival : histology , treatment era ( 1977 to 1985 vs 1986 to 1995 ) , the timing of radiation therapy ( immediately vs delayed radiotherapy ) , age at diagnosis , gender , tumor location and the functional category ( mrc )  . 
an overview on the factors investigated and their outcome on overall survival is outlined in table 2 . a progression or recurrence as determined by imaging criteria was noted in 62 of the 77 patients ( 81% ) after a time interval between 3 and 140 months ( median , 56 months ) after surgery . 
prognostic factors for relapse - free survival are outlined in table 3 and similiar to those predicting for overall survival . at risk 31 6 % no seizures 40 10 % at risk seizures p = 0.04 61 7 % years years 35 8 % 23 10 % 54 6 % years figure 1 . 
gesamtberleben fr 77 patienten mit low - gradegliom , die ein anfallsleiden ( ) oder keine anflle ( - ) vor diagnosestellung hatten ( p = 0 , 04 )  . 
 the final model of the multivariate cox regression analysis identified the ct - pattern ( p = 0.02 ) and the total dose ( p = 0.06 ) as independent factors with relapse - free survival as endpoint . 
no significant impact on relapse - free survival was noted for the functional categories ( mrc ) , age at diagnosis , histology and timing of radiotherapy . although this study was not designed to evaluate radiation toxicities , the following treatment - related side effects were recorded in the patient charts : transient increasing headache or seizures during radiation ( 4 patients ) , retinopathy with permanent vision impairment ( 1 patient ) , delayed hypopituitarism ( 3 patients ) ; and delayed cognitive impairment ( 3 patients )  . discussion we evaluated overall survival , progression - free survival and prognostic factors in a group of patients with supratentorial low - grade astrocytoma , oligodendroglioma and mixed glioma diagnosed since 1977 who were treated by surgery and either delayed or immediate external radiotherapy . 
prognosefaktoren fr das rezidivfreie berleben ( p * = log - rank - test ; p * * = univariate cox - analyse ; p * * * = multivariates finales cox - modell )  . gy and a history longer than 6 weeks were associated with a better progression - free survival . 
a non - enhancement following intravenous contrast media was able to predict for an excellent long - term prognosis with a 5 - year and 10 - year survival rate of 62% and 45% . 
 [ 20 ] reviewed 53 cases of adult fibrillary supratentorial astrocytoma and found that ct contrast enhancement of the original tumor was associated with a 6.8 - fold increase in risk for later recurrence . 
a combination of 4 variables including age , duration of symptoms , preoperative neurological status and ct contrast enhancement turned out to give the best fitting prognostic model for survival in a recent series given by schuurman et al . 
it appeared that these non - treatment variables had a profound effect on the duration of survival of patients with supratentorial low - grade glioma . in an attempt to further evaluate possible prognostic markers many authors have found a good correlation between the immunocytochemical expression of the proliferation associated antigen ki - 67 as detected by the monoclonal antibody mib1 [ 7 , 8 , 13 , 14 , 16 , 2931 , 41 ]  . 
this ratio was small for long - term survivors among patients with grade - iii tumors and tended to be greater for patients with grade - ii tumors who experienced an early progression [ 27 ]  . 
investigations of the mib1 / apoptosis ratio in a subgroup of the patients in this series resulted in very similiar findings and will be reported in detail elsewhere . several retrospective studies have concluded that survival and progression - free survival were enhanced by immediate postoperative radiotherapy [ 4 , 17 , 33 - 34 , 36 ] whereas other similiar analyses have been unable to demonstrate survival benefits attributable to early postoperative radiation treatment [ 1 , 23 , 24 , 37 ]  . 
in a recent paper [ 19 ] treatment delay until signs of progression were seen by imaging criteria was not associated with a worse prognosis among 87 patients with favorable prognostic factors compared to a group of patients with less favorable prognostic factors and immediate radiotherapy . 
 in our series , the 5and 10 - year survival rates were 52% and 29% for patients treated immediately after surgery and 69% and 46% for patients treated only in case of disease progression . 
 [ 19 ] we observed better survival rates and longer overall survival times for patients in the delayed radiotherapy group . it is obviously a widespread policy in many centers to submit patients with bulky residual or inoperable disease and other adverse prognostic factors to immediate radiotherapy , whereas younger patients with complete resections are more likely to have their treatment delayed . 
it may , however , be argued that immediate radiotherapy in this favorable patient group would be able to achieve a survival plateau with a considerable number of long - term survivors . 
 in 2 recent prospective studies using local radiation fields , external radiotherapy was shown to be no longer of adverse influence on the cognitive function as compared to non - irradiated groups of tumor patients [ 38 , 40 ]  . 
 [ 5 ] clear evidence of neuropsychiatric impairment was demonstrated for long - term survivors following whole brain irradiation and not for patients after local irradiation . the existence of a dose - response relationship in supratentorial low - grade glioma is another issue of ongoing debate . a number of investigators demonstrated some evidence that higher doses can contribute to a better survival rate [ 21 , 33 , 43 ]  . 
 [ 33 , 34 ] published results on 167 patients , 139 of whom received postoperative radiotherapy . the 5and 10 - year survival rates of 68% and 39% for the subgroup of patients treated with higher doses ( > 53 gy ) were higher as compared to the survival rates for patients treated with lower doses ( < 53 gy ) being 47% and 21% , respectively . 
very similar results were seen in this retrospective series with significantly better relapse - free survival rates of 60% and 32% at 5 and 10 years following doses above 52 gy . 
with a minimum follow - up of 4 years and 343 evaluable patients the rates for survival and progression - free survival at 5 years were 58% vs 59% and 47% vs 50% , respectively , for the different dose groups [ 12 ]  . the present analysis was intended to identify prognostic factors following postoperative radiotherapy in patients with supratentorial low - grade glioma . 
among these factors the nontreatment related variables like duration of symptoms , the presence of seizures and ct contrast pattern outweigh the treatment - related variables like total dose and extent of resection . 
on the basis of these findings we are in the position to define a high - risk group in the cohort of patients with lowgrade glioma characterized by a short duration of symptoms ( < 6 weeks ) , the absence of seizures and positive ct enhancement , who should be considered for intensification of treatment within prospective trials . strahlentherapie und onkologie urban & vogel 2000 aktuelles forum a review of current and future treatment strategies for malignant astrocytomas in adults carsten nieder1 , ursula nestle2 background : for more than 20 years , after establishing the role of postoperative radiotherapy for malignant astrocytomas , no definitive improvement in survival rates could be observed , despite advances in established treatment modalities such as radiotherapy and chemotherapy . 
this review discusses available laboratory and clinical data as well as recent advances in our knowledge about prognostic factors ( table 1 ) and their implications for the design of future clinical trials . results : elucidation of the biology of malignant astrocytomas allowed for development of rational new approaches , such as gene therapy and immunotherapy , which could interfere with established treatment regimens or being used independently . 
possible strategies include the restoration of defective cancer - inhibitory genes , cell transduction or transfection with antisense dna corresponding to genes coding for growth factors and their receptors , or with the so - called suicide genes . 
by p - glycoprotein antagonists or o6 - alkyl - guanine - dna - transferase inhibitors , inhibition of matrix metalloproteinases , inhibition of protein kinase c , and administration of agents such as phenylbutyrate or valproic acid that showed promising antiproliferative effects in vitro . 
 key words : malignant glioma glioblastoma multiforme anaplastic astrocytoma therapy prognostic factors eine bersicht ber gegenwrtige und knftige strategien zur behandlung maligner astrozytome bei erwachsenen hintergrund : trotz fortschritten auf dem gebiet etablierter behandlungsverfahren , wie der strahlenund chemotherapie , konnte in der behandlung maligner astrozytome in den letzten 20 jahren , nachdem die rolle einer postoperativen strahlentherapie gesichert worden war , keine definitive verbesserung der berlebensraten erzielt werden . 
in dieser arbeit werden sowohl die verfgbaren laborund klinischen daten als auch die aktuellen fortschritte auf dem gebiet prognostischer faktoren ( tabelle 1 ) und deren bedeutung fr das design knftiger klinischer studien diskutiert . ergebnisse : die aufklrung der biologie dieser tumoren ermglichte die entwicklung rationaler neuer strategien , zum beispiel basierend auf der genund immuntherapie , die entweder zusammen mit etablierten methoden oder allein anwendbar sind . 
mgliche strategien bestehen in der wiederherstellung defekter tumorsuppressorgene , der transduktion oder transfektion mit antisense - dna zu genen , die fr wachstumsfaktoren und deren rezeptoren kodieren , oder in der sogenannten suizidgentherapie . 
weitere therapiemglichkeiten bestehen im aufheben der chemotherapieresistenz , zum beispiel mit p - glykoprotein - antagonisten oder o6 - alkyl - guanin - dna - transferase - inhibitoren , der gabe von matrixmetalloproteinaseinhibitoren , proteinkinase - c - inhibitoren und anders wirksamen substanzen , die im labor antiproliferative effekte gezeigt haben , wie beispielsweise phenylbutyrat und valproat . schlussfolgerung : derzeit beginnen mehrere der neu entwickelten strategien ihre klinische erprobung ( tabelle 2 )  . 
treatment of malignant astrocytomas t reatment of high - grade ( or so - called malignant ) astrocytomas has been one of the most challenging fields in oncology for more than 20 years . 
despite considerable effort and notable advances in the surgical , radiotherapeutic , and chemotherapeutic field , the trend towards continuous improvement in outcome that could be observed for many other neoplasms seems to be almost completely absent . 
patients prognosis is mainly determined by several tumorand patient - related factors , whereas changes in treatment protocols so far have contributed little to avoid death from uncontrolled local disease , which still remains the leading cause of death after a median time of approximately 10 to 12 months for glioblastoma multiforme and up to 36 months for anaplastic astrocytoma [ 13 ]  . 
it will provide information about the development of new approaches , such as gene therapy and immunotherapy that could interfere with established treatment modalities or being used independently to target , e . 
articles listing one of the key words glioblastoma multiforme , anaplastic astrocytoma , malignant astrocytoma , or malignant glioma , which were published between 1989 and 1999 , were identified and reviewed according to their quality of evidence ( for clinical studies )  . 
 established prognostic factors for survival when summarizing published data , age , performance status and / or neurologic function status , and tumor grade have consistently been found to be the most important prognostic factors , followed by extent of surgical resection ( or residual tumor volume determined within 72 hours after surgery )  . 
less consistently reported factors include necessity for corticosteroids ( or dose ) , duration of symptoms , and presenting neurologic abnormalities or tumor side ( frontal more favorable ) [ 13 , 23 , 50 , 52 , 66 ]  . 
 [ 13 ] reanalyzed the survival of more than 1 , 500 patients with malignant astrocytomas in the radiation therapy oncology group ( rtog ) database and found that 5 variables ( duration of symptoms , mental status , age at diagnosis , tumor grade , and postoperative performance status ) defined 6 patient subgroups with distinct prognoses ( median survival from 5 to 59 months )  . 
although there is no generally accepted consensus about inclusion criteria for future phase - ii or - iii trials of investigative therapies , it seems reasonable to assume that patients with longer life expectancy are more likely to profit from such therapies . 
 [ 13 ] , the latter group includes all patients younger than 50 years ( except glioblastoma multiforme with poor performance status ) and selected patients older than 50 years ( 22% of all patients , table 1 )  . 
g. , by variants of the ki - 67 antibody such as mib - 1 or by bromodeoxyuridine labeling index was found to correlate to tumor grade , but not to survival when analyzed by appropriate methods , i . 
expression of p27kip1 , a cell cycle regulator , was recently suggested to be of independent prognostic value , however , the multivariate analysis did not include performance status [ 48 ]  . the prognostic importance of epidermal growth factor receptor ( egfr ) amplification in glioblastoma multiforme remains unclear , too . 
in a recent immunohistochemical analysis , high level of expression of the urokinase type of plasminogen activator was found to correlate to grade and to survival , however , multivariate analysis did not include performance status and extent of resection [ 31 ]  . 
 radiotherapy almost all studies discussed here included both anaplastic astrocytoma and glioblastoma multiforme histologies , a few were limited to glioblastoma multiforme alone , whereas none was restricted to anaplastic astrocytoma . 
 level - 1 evidence in 1978 , a phase - iii trial by the brain tumor study group ( btsg ) established the role of radiotherapy after maximal surgical resection [ 75 ]  . 
a combined evaluation of 3 btsg median survival patients characteristics >= 18 months all aa except age >= 50 years with symptom 11 months duration <= 3 months gbm age < 50 years with kps > 80% aa age >= 50 years with symptom duration <= 3 months gbm age < 50 years with kps <= 80% gbm age >= 50 years with both kps >= 70% and able to work neurologic function after surgical resection <= 9 months all other gbm table 1 . 
treatment of malignant astrocytomas studies as well as a randomized medical research council ( mrc ) trial suggested that a postoperative dose of 60 gy in conventional fractionation was more effective than lower doses [ 6 , 74 ]  . 
in part , the limited success of dose escalation with external beam radiotherapy was caused by increased normal tissue toxicity , which could be reduced by minimizing the amount of irradiated normal brain , e . 
 [ 21 ] , who developed a technique for fusion of f - 18 - fdg positron emission tomography and magnetic resonance imaging and applied this technique in the radiotherapy planning of malignant astrocytomas , the latter was observed in a few cases only . huncharek [ 32 ] performed a metaanalysis of 9 randomized trials involving over 1 , 700 patients who received radiotherapy with or without misonidazole . 
 [ 41 ] did not find a survival difference when administering 60 gy via a temporary stereotactic 125i implant after 50 gy external beam radiotherapy compared to the external beam treatment alone . 
further treatment intensification by combining hyperthermia and brachytherapy after surgery and external beam radiotherapy plus hydroxyurea for glioblastoma multiforme in a randomized phase - ii / iii trial significantly improved time to progression from 33 to 49 weeks and median survival from 76 to 85 weeks [ 67 ]  . 
a detailed prospective evaluation of quality of life ( qol ) in a comparable study would be helpful in order to decide whether or not the moderate survival benefit of hyperthermia represents a real therapeutic gain . level - 2 evidence studies of accelerated hyperfractionated radiotherapy did not demonstrate improved survival [ 8 , 52 , 64 , 79 ]  . 
several groups treated elderly patients and / or those with other unfavorable prognostic factors with more convenient hypofractionated schedules to , for example , 42 gy ( dose per fraction 3.5 gy ) [ 40 ] or 36 gy ( dose per fraction 3 gy ) [ 18 ]  . 
furthermore , no severe acute or late toxicity from hypofractionated partial brain irradiation has been observed in these studies . neither addition of radiosensitizers such as etanidazole , tirapazamine , bromodeoxyuridine , or hyperbaric oxygen nor use of neutron beams or proton beams have resulted in a significant gain [ 62 ]  . 
a recent update of their data ( long - term outcome ) essentially confirmed this figure , but also revealed that reoperation may be nearly inevitable in long - term survivors [ 65 ]  . 
experimental studies measuring the regrowth delay of in vitro or in vivo irradiated human malignant glioma cells suggest that continuous ultra - low dose - rate irradiation increases the effect of fractionated high - dose - rate treatment [ 80 ]  . 
its role as an important part of promising new combined - modality approaches such as suicide gene therapy will be discussed later . chemotherapy since the 1970s , many cytotoxic drugs , most often nitrosoureas , have been added to surgery and radiotherapy . 
by itself , none of the studies reported so far was convincing enough to make chemotherapy a generally accepted part of standard first - line treatment , especially for glioblastoma multiforme and / or unselected groups of patients with malignant astrocytomas . 
unfortunately , there is currently no level - 1 evidence for treatment of anaplastic astrocytoma , because all previous studies included both anaplastic astrocytoma and glioblastoma multiforme . level - 1 evidence a metaanalysis of 16 randomized clinical trials from a 17year period suggested a moderate increase of survival of 8.6% at 2 years by adding chemotherapy . 
a recently published randomized mrc trial , which did not confirm improved survival when comparing adjuvant radiotherapy plus procarbazine , ccnu , and vincristine ( pcv ) vs radiotherapy alone , challenges the results of the metaanalysis [ 9 ]  . 
those studies include a phase - iii trial comparing bcnu plus procarbazine or bcnu plus hydroxyurea , procarbazine , and teniposide to single agent bcnu [ 63 ] and a phase - iii trial comparing bcnu plus 6mercaptopurine to bcnu alone [ 27 ]  . 
with bcnu , was comprehensively evaluated but found to be more toxic rather than more effective than intravenous administration and , thus , did not offer a therapeutic gain [ 62 ]  . level - 2 evidence a recent phase - ii study of intensified chemotherapy , where bcnu was preceded by carboplatin and teniposide , administered during radiotherapy to 56 patients with glioblastoma multiforme , resulted in a median time to progression of 7.5 months and a median survival of 12.5 months [ 10 ]  . 
 level - 3 evidence the practice of routine use of adjuvant pcv chemotherapy for patients with anaplastic astrocytoma by some neurooncologists is based largely on a post hoc analysis of an otherwise negative trial [ 42 ]  . 
 [ 55 ] reviewed the rtog database and identified 257 patients with anaplastic astrocytoma treated with bcnu and 175 treated with pcv . this retrospective analysis did not suggest any survival benefit for pcv . 
the influence of selection factors on recent results of a retrospective study in 85 patients with anaplastic astrocytoma ( age < 55 years ) , which showed a favorable median survival of 80 months ( intra - arterial bcnu , procarbazine , vincristine ) vs 25 months ( no chemotherapy ) , is not entirely clear [ 24 ]  . 
so far , superiority of combination pcv or bcnu - pv has not been confirmed in a prospective study designed specifically to address this issue . however , increasing evidence suggests that patients with anaplastic astrocytoma are more likely to profit from chemotherapy . 
regarding high - dose chemotherapy regimens with autologous bone marrow or peripheral blood stem cell support , increased toxicity appears to be a major probleresults reported so far are less encouraging than anticipated [ 49 ]  . 
biodegradable polymers may be impregnated with cytotoxic chemotherapeutic drugs , such as bcnu or 5 - fu , and the polymer wafers placed into the tumor bed during surgery , possibly exposing tumor cells to higher drug concentration [ 47 ]  . 
it is also being studied whether new drugs including paclitaxel , topotecan , irinotecan , temozolomide , cladribine , and difluromethylornithine alone or in combination are more effective than nitrosoureas . 
temozolomide , which can be administered orally , showed some encouraging results in recurrent or progressive astrocytomas [ 7 ]  . resistance of tumor cells to cytotoxic chemotherapeutic drugs through several possible mechanisms of intrinsic drug resistance is a major problethese mechanisms include the existence of p - glycoprotein ( pgp ) , an energy - dependent drug efflux pump removing a wide range of lipophilic chemotherapeutic drugs [ 28 ]  . 
in tumors expressing pgp , chemoresistance could be overcome by adding pgp antagonists . another mechanism involved in chemoresistance is intracellular drug inactivation or transformation as a result of increased concentrations of detoxifying enzymes such as gluthatione s - transferases ( gst )  . 
gst immunoreactivity was found in tumor blood vessels as well as neoplastic cells , without evidence of a correlation between the frequency of reactive cells and grade of malignancy [ 73 ]  . 
metallothionein , a family of predominantly intracellular protein thiol compounds involved in cisplatin resistance , was recently identified by immunohistochemistry in 64% of anaplastic astrocytoma and 80% of glioblastoma multiforme [ 30 ]  . 
overall survival was not influenced by metallothionein expression [ 30 ]  . in conclusion , drug resistance in malignant astrocytomas can result from expression of pgp and other proteins in neoplastic cells as well as from the function of these proteins in endothelial cells of tumor blood vessels . 
 other pharmacologic approaches valproic acid , a drug employed in epilepsy treatment , significantly inhibited growth of 1 rat and 3 human glioma cell lines in vitro in a dose - dependent manner [ 39 ]  . 
however , the fact that this result was achieved at non - toxic , clinically achievable doses makes valproic acid an attractive agent for in - vivo studies . on the other hand , the use of anticonvulsant drugs during a course of chemotherapy might lead to more rapid metabolism of chemotherapeutic agents , as has been reported for paclitaxel and cytochrome p450 system stimulating anticonvulsant drugs [ 20 ]  . 
treatment of malignant astrocytomas more about interactions between chemotherapy on the one hand and anticonvulsant as well as other drugs on the other hand , because rational combinations of these standard components of treatment might contribute to improvement of the therapeutic index . 
 [ 15 ] studied 1 rat and 4 human glioma cell lines in vitro after exposure to clinically obtainable concentrations of phenylbutyrate , a novel differentiating and cytotoxic compound used , e . 
its metabolite phenylacetate , which has some pharmacokinetic disadvantages , showed little activity against recurrent malignant astrocytomas in a phaseii study ( median time to progression 2 months ) [ 12 ]  . 
recently , protamine was found to induce a dose - dependent significant decrease in volume , angiogenesis , mitotic index and viable tumor areas in rats with subcutaneous c6 gliomas [ 3 ]  . 
the growth inhibition produced by moderate doses of protamine was similar to that produced by toxic doses of suramthe combination of protamine and bcnu had a synergistic curtailing effect on tumor growth [ 3 ]  . 
these promising results might justify further evaluation of protamine in humans , where it is commonly used to antagonize heparin . accumulating evidence suggests an important role of platelet - derived growth factor ( pdgf ) and vascular endothelial growth factor ( vegf ) ligands and receptors in the vascularization of astrocytomas [ 49 ]  . 
this agent showed some activity ( objective tumor regression in 4 / 42 patients ) in recurrent gliomas [ 44 ] and is now under evaluation for patients with glioblastoma multiforme ( su - 101 plus bcnu )  . 
other inhibitory agents such as marimistat have been tested in several tumor types , including a randomized , placebo - controlled phase - iii trial for patients with newly diagnosed glioblastoma multiforme . 
results from this trial are expected soon . protein kinase c ( pkc ) represents a family of serine / threonine kinases , which transduce signaling events from tyrosine kinase membrane receptors and a variety of intracellular biochemical pathways . 
a detailed overview of currently available methods and their limitations can be found in references [ 2 , 70 ]  . suicide gene therapy includes transferring a prodrug activating gene into the malignant cell , converting an inactive agent into a cytotoxic one [ 2 , 70 ]  . 
when the prodrugs 5 - fluorocytosine and ganciclovir were combined with radiotherapy and double suicide gene therapy , more than 70% of the animals with so - called advanced tumors ( 14 days old ) were alive by day 120 ( maximum observation time )  . 
it has been demonstrated that the negative cell cycle regulator waf1 / cip1 , which is transcriptionally activated by p53 and inhibits cyclin - dependent kinases , is often overexpressed in astrocytomas , rendering cells resistant to cytotoxic chemotherapy [ 58 ]  . 
the tp53 gene encodes a protein which ultimately plays a role in cell cycle regulation ( arrest of dnadamaged cells at the g1 / s interface ) , response to dna damage , and apoptosis . 
 antibody therapy the identification of tumor - associated antigens , such as growth factor receptors that are present in tumor tissue but not normal cns tissue , the production of homogenous , high affinity monoclonal antibodies ( mab ) to such antigens along with the use of compartmental administration , e . 
increased uptake might be achieved by administration of antibody fragments or selective pharmacologic opening of the blood - tumor barrier using bradykinin or the bradykinin analogue rmp - 7 , which increases uptake of both cytotoxic chemotherapeutic agents and various - sized tracers ( up to 70 kd ) into brain tumors [ 45 ]  . 
 level - 2 evidence treatment of 59 patients with malignant astrocytomas after surgical resection and standard radiation therapy with intravenous 125i - labeled anti - egfr mab resulted in overall median survival of 13.5 months [ 68 ] , which is similar to many studies of surgery and standard radiotherapy alone [ 52 ]  . 
a median survival of 25 months in newly diagnosed glioblastoma multiforme with small residual lesions after surgery and external - beam radiotherapy [ 57 ]  . perspectives in malignant astrocytomas , expression of vegf is significantly upregulated , compared with normal brain [ 49 ]  . 
the density of vessels was decreased in antibody - treated tumors and the magnitude of response was greater in more rapidly proliferating , more angiogenesis - dependent tumors [ 38 ]  . 
gliomas often express fas ( cd 95 ) , a transmembrane glycoprotein belonging to the nerve growth factor / tnf receptor superfamily , whereas normal cells in cns do not [ 78 ]  . 
the same holds true for targeting cytotoxins to the interleukin - 13 receptor , which was recently identified in human glioblastoma multiforme specimens , but not in normal brain [ 14 ]  . 
 challenges in the design of future studies as more aggressive treatment is offered to select groups of patients , new challenges must be faced , especially with regard to design of future studies . 
it might even be advisable to study certain approaches in limited subsets of anaplastic astrocytoma or glioblastoma multiforme , defined by definite genetic abnormalities and / or by residual tumor mass after surgical resection . 
it is also mandatory to evaluate predictive factors for response more precisely than in the past . better measures of tumor response may need to be developed in addition to standard response criteria such as radiographic response and time to progression , which do not imply improved survival nor improved qol . 
the latter fact argues against the use of time to tumor progression as endpoint for trials evaluating intense , locally directed therapies such as srs , brachytherapy , or gene therapy . 
for a disease like astrocytoma that threatens intellect , locomotion , and other basic human functions , it could be argued that qol is a more important measure of successful treatment than survival . qol measurements can be performed using a brain tumorspecific questionnaire , designed as a supplement to the qlq - c30 qol instrument developed by the european organization for the research and treatment of cancer ( eortc ) [ 1 , 53 ] , or the functional assessment of cancer therapy ( fact ) brain subscale , a brain tumor - specific qol instrument that incorporates patient and caregiver input [ 77 ]  . 
these instruments generally should be preferred over simple , only moderately correlating , scales like the karnofsky performance status or the barthel activities of daily living index [ 53 ]  . 
 of course , it must be emphasized that the growth of a tumor results from numerous factors , such as multiple genetic events , neoangiogenesis and escape from immune control . the current experience in cancer treatment shows that several components in this complex process should be targeted to provide maximal chances of cure and that it is unlikely for a single therapeutic approach to be applicable to all patients . therefore , rational combinations between established treatments and newly developed approaches , aiming for example at inhibition of neoangiogenesis , induction of apoptosis , or restoration of cell cycle control , might offer the best opportunity to improve the prognosis of patients with malignant astrocytomas . 
treatment of malignant astrocytomas experimental and phase i phase ii / iii fas - mediated apoptosis suicide gene therapy + / radiotherapy modulation of drug resistance ( pgp , agat , waf1 / cip1 antisense ) new radiosensitizers , like gadolinium - texaphyrin , rsr13 , etc . 
in the delivery of both genetic vectors and mab and the immunresponse - related toxicity of some vectors , require further preclinical and phase - i studies of many promising therapies ( table 2 )  . 
however , meanwhile carefully designed phase - ii and - iii studies of simpler , but already feasible sound strategies in well - defined subgroups of patients are needed to improve the prognosis of patients with malignant astrocytomas . strahlentherapie und onkologie urban & vogel 2000 originalarbeit p53 : biology and role for cellular radiosensitivity jochen dahm - daphi1 purpose : p53 is the most commonly mutated gene in human tumors with large impact on cellular biology and response to radiation . 
a general proof is still lacking . conclusion : the emerging picture in the year 2000 shows p53 as a central protein in a multi - enzyme multi - function network which is far from being fully understood . 
 key words : apoptosis dsb exonuclease g1 - arrest irradiation p53 radiotherapy recombination tumor x - rays p53 : seine biologie und seine rolle fr die zellulre strahlenempfindlichkeit hintergrund : p53 ist das am hufigsten mutierte gen in menschlichen tumoren mit groem einfluss auf die zellulre biologie und strahlenantwort . 
ein allgemein gltiger beweis steht noch aus . schlussfolgerung : p53 zeigt sich im jahre 2000 als ein zentrales protein in einem multienzym - multifunktions - netzwerk , das bei weitem noch nicht vllig aufgeklrt ist . 
p53 and cellular radiosensitivity p 53 was first described in 1979 by lane and crawford as a target protein for the large t - antigen of the oncogenic simian virus 40 ( sv40 )  . 
beside knowledge about the proteins natural properties radiooncologists seek to identify the role of p53 alterations for cellular radiation response which will be the perspective of the current paper . structure and gene locus the human p53 gene is located on chromosome 17 p13.1. 
it is involved in organogenesis , tissue homeostasis , cell - cycle control , regulation of proliferation and dna - replication , maintenance of genetic stability and senescence . mutagenesis the mutation spectrum of the gene is dominated by point mutations resulting in an altered sequence of amino acids , protein structure and function ( missense mutations )  . 
most mutations are c / g to t / a transitions presumably arising from spontaneous desamination of methylated cytosines . the less frequent g to t transversions likely result from oxidative attack to guanines [ 35 ]  . 
the vast majority ( < 80% ) of mutations are located in the core domain affecting the principal function of p53 as a transcription factor . some codons within this central region are hot - spots of mutagenesis , namely at the positions 175 , 245 , 248 , 273 and 283 . these codons are found over - represented among all mutations for 3 reasons . 
although mutations are restricted to 1 allel , these cells may have widely lost wildtype function since mutant and wild - type proteins form a tetramer upon activation which is then entirely forced into mutant conformation ( transdominant negative effect of mutant p53 ) [ 102 ]  . regulation p53 protein content varies upon cell - cycle progression with a maximum in early s - phase [ 96 ]  . 
activity of wild - type p53 is regulated on several levels through up - stream stimuli , one of which is dna damage by ionizing radiation ( ir ) ( figure 1 )  . 
by far more important is the post - translational modification preventing p53 from binding to mdm2 , a reaction which usually initiates the ubiquitin - mediated protein degradation [ 29 ]  . 
after ionizing radiation , phosphorylation of the aminoacid serine at position 15 by the kinases atm or atr is considered the key - event ( for review see [ 33 , 56 ] )  . 
atm ( and atr = at related ) is the protein mutated in patients with the syndrome ataxia teleangiectasia . in those mutated at cells p53 is not phosphorylated and , thus , the response to ionizing radiation is attenuated [ 50 , 62 ]  . 
the second enzyme which phosphorylates serin - 15 in vitro , the dna - dependent protein kinase , dna - pk [ 119 ] appears not to be an essential enzyme for p53 activation in vivo [ 47 ]  . 
after a variety of stimuli , such as genotoxic stress by ionizing radiation , cells undergo p53 - dependent apoptosis . the central domain serves as transcription factor for the bax promoter [ 73 ]  . 
p53 also regulates other pathways into apoptosis through pigs ( p53 inducible genes ) , many of which interfere with metabolism of reactive oxygen species at the mitochondrial membrane [ 85 ]  . 
upper : several up - stream stimuli enhance p53 activity partly mediated by mdm2 protemiddle : the linearized p53 protein shows the major domains and binding proteins specifically regulating its activity . 
following dna damage activated p53 enhances the transcription and translation of p21waf1 / cip1 which is a universal inhibitor of cyclin - dependent kinases [ 25 , 55 ]  . 
at the g1 / s border , p21 inhibits the complex of cyclin e / cdk2 which usually initiates transition from g1 to s - phase by phosphorylation of the rb - protein and stabilization of the transcription factor e2f - 1 . 
p53 is , furthermore , involved in regulation of replication itself via gadd45 [ 50 ] , p21cip1 / waf1 - pcna [ 17 , 59 ] and by direct interaction with polymerase ( see below )  . 
wild - type p53 mediates a g2 - block after dna - damage [ 103 ] through induction of the cdk - inhibitor p14 - 3 - 3 and / or p21 [ 41 , 45 ] and suppression of cyclin b eventually in cooperation with gadd45 . 
however , these cells still perform a prominent g2 - block after irradiation [ 49 ] which might be controlled upon other mechanisms such as proteins of the mpm - 2 family . 
by physically binding to other repair proteins in a presumably larger repair complex ( such as rad51 , brca1 and 2 , rpa and others ) [ 14 , 23 , 67 , 105 , 108 , 124 ] or exerts its own dna - binding and repair functions . 
it catalyses single - strand dna transfer , strand invasion and renaturation upon recombination [ 4 ] , it has 3 - 5 - exonuclease activity in vitro which appears to inhibit erroneous replication and recombination through recognition and resolution of dnastretches harboring base mismatches [ 22 ]  . three different repair modes can be distinguished in which p53 is involved : 1 . 
cells having lost wild - type function showed a 3to 100 - fold higher rate of hr [ 22 , 70 , 113 , 116 ] which might contribute to the known phenomenon of genomic instability . 
the enhanced rates of non - homologous endjoining are also observed for p53mut but not for p53null cells [ 106 ]  . from these results the possibility arose , that either repair velocity , capacity or repair fidelity could be influenced by the cellular p53 status . 
one study suggested a proficiency for repair of double - strand breaks in cells with p53mut another study showed no differences between normal fibroblasts and those of li - fraumeni heterozygotes ( p53 wild - type / mut ) or between p53null and various mutants [ 12 , 21 , 72 ]  . 
our own results ( figure 2 ) show any significant differences in the repair capacity between p53 wildtype and p53mut tumor cells , far from reflecting 3to 100fold differences observed for recombination with the p53mut p53wt figure 2 . 
non - repaired double - strand breaks ( dsb ) were measured after 90 gy of x - irradiation followed by 24 hours of repair incubation using the constant - field gel electrophoresis . 
cell strains with a mutant p53 were du145 , rt112 , mcf - 7 variant bb , ssc4451 , and wild - type p53 strains were lncap , mcf7 , ssc4197 . 
 in conclusion , during the past 20 years our knowledge of p53 has been drastically extended from a simple growth and tumor suppressing protein to a major regulator in a network of interacting functions . 
beside the characterized defined pathways a considerable heterogeneity in p53 activity and its down - stream effects were observed among cell types and tissues [ 52 , 63 , 64 ]  . 
the picture is further complicated by the p53 homologues p73 and p51 / p61 which regulate identical targets similar or dissimilar to the parental protein [ 97 , 126 ]  . 
the gene loss , a dominant mutation or a p53 protein degradation by papilloma virus protein hpv e6 is regularly coupled with a lack of g1 - arrest , which allow the cells to proliferate and presumably to maintain clonogenic capability . 
in line with these results , fibroblasts of li - fraumeni heterozygotes [ 72 , 117 ] with a dominant - negative p53 germ - line mutation [ 102 ] are more radioresistant than normal human fibroblasts . however , the situation appears to be more complex with tumor cells . 
several reports fail to show any influence of p53 inactivation on tumor cell radiosensitivity [ 9 , 20 , 44 , 48 , 66 , 101 , 123 ]  . 
a few investigators even described wild - type cells as more resistant than those with an altered p53 [ 81 , 88 , 95 ]  . on the other hand , various studies found an increased radioresistance for cells with inactive p53 compared to those expressing wild - type function [ 5 , 9 , 32 , 58 , 65 , 69 , 76 , 92 , 94 , 98 , 122 ]  . 
the nci group who investigated the largest number of tumor cells found for p53 mutant strains after a variety of dna damaging agents a reduced g1 - block coupled to a ( short - term ) growth advantage . 
cell strains used were not isogenetic which means that different radiosensitivity is not necessarily determined by p53 status alone [ 19 , 48 , 66 , 69 , 88 , 98 , 101 , 123 ]  . 
the e6 protein inactivates wild - type p53 but a pure p53 - null phenotype is not necessarily achieved since hpv proteins might also exert its own effect on survival [ 121 ]  . 
a mutant or wild - type p53 gene was transformed into wild - type , mutant or null background , respectively [ 32 , 101 , 122 ] or an isogenetic pair with / without wtp53 was used [ 65 ]  . 
however , the studies using the most cell lines would argue for a resistant phenotype associated with a lack of p53 wild - type function [ 58 , 69 , 98 ]  . the lack of either of p53s main functions could in principle account for tumor cell radioresistance . 
the permanent arrest in tumor cells appears to be less pronounced compared to fibroblasts [ 58 , 60 ] but it is not sufficiently studied as yet due to a lack of appropriate methods . 
several genes inhibit cell growth and colony formation in co - operation with or as executor of p53 [ 3 , 64 ]  . loss of their activities results in enhanced colony formation and accelerated proliferation . 
biochemically , some properties have been described such as enhanced binding of p53mut to dna sequences attached to the nuclear matrix ( mar ) [ 115 ]  . p53mut shows enhanced constitutive binding to topoisomerase i [ 34 ] mediating a helicase activity and the transcription of bag - 1 , an anti - apoptotic protein is enhanced by mutant p53 . 
moreover , cell killing by etoposide is reduced in cells which overexpress certain mutant p53 proteins ( 175h , 179h , but not 273h ) compared to controls which have no p53 protein ( p53null ) [ 6 ]  . 
p53 and cellular radiosensitivity p53 and radiotherapy conclusion and perspective if p53 inactivation renders tumor cells more radioresistant it could be assumed that also tumors lacking wild - type p53 are more radioresistant and consequentially patients are more prone to relapse or cancer - related death . 
animal studies appear to confirm this notion [ 31 , 61 ] as do human tumors bearing a p53 mutation with a naturally more aggressive phenotype [ 27 , 42 , 100 , 109 ]  . 
nineteen out of 34 studies screened found that low p53 expression ( assumed to be wild - type ) was correlated with a favorable prognosis while 11 showed no influence and 4 studies described worse prognosis for a p53 wild - type expression pattern ( see [ 11 ] and references therein and favorable [ 2 , 36 , 38 , 39 , 43 , 51 , 54 , 84 , 86 , 87 , 89 , 99 , 118 , 120 ] vs no influence [ 24 , 26 , 75 , 78 , 79 , 91 , 100 , 114 ] vs worse [ 83 , 90 ] )  . 
however , careful metaanalysis can reveal at least for some entities , such as rectal cancer , a better rate of local control and survival for wild - type than for p53mut tumors [ 81 ]  . 
the clinical ambiguity of p53 status can largely be due to the technique of immunohistochemistry which has only 75% sensitivity and a 63% positive predictive value for p53 mutations [ 35 ]  . 
studies evaluating p53 alternatively by direct sequencing found gene p53 mutations are associated with a worse prognosis [ 37 , 42 , 43 , 51 , 71 , 109 ] while immunohistochemistry showed no correlation [ 37 , 71 , 109 ] which is though not an appropriate single method to compare with clinical endpoints . 
on the other hand , facing the complexity of genetic as well of epigenetic regulatory events it seems unlikely to extract p53 status alone as the single determinator for radiosensitivity . 
today , patients with this disease still have fatal prognosis necessitating efforts towards more effective treatment . material and methods : this report provides a review of adjuvant and neoadjuvant radiotherapy in pancreatic carcinoma without distant metastasis . 
radiotherapy in neoadjuvant intention is an approach for downstaging to achieve resectability in initially irresectable tumors . results : the widespread use of new techniques such as supervoltage irradiation , computer based 3 - d - planning , interventional therapy and combination of different therapeutic modalities induced a great number of studies . 
patients with irresectable tumors possibly can be downstaged and be brought to resection nevertheless . conclusions : simultaneous radiochemotherapy with 5 - fu and mitomycin c can be performed without elevated risk of acute side effects of higher degree . 
neoadjuvant simultaneous radiochemotherapy should only be performed as a part of a clinical trial . key words : ductal pancreatic carcinoma radiotherapy chemotherapy adjuvante und neoadjuvante radiochemotherapie des duktalen pankreaskarzinoms hintergrund : das duktale pankreaskarzinom ist die dritthufigste bsartige erkrankung des verdauungstrakts bei steigender inzidenz . 
bei inoperablen tumoren kann in neoadjuvanter intention ein downstaging angestrebt werden , um den tumor resektabel zu machen . ergebnisse : die verbreitung neuer radiotherapeutischer techniken , wie zum beispiel der hochvoltbestrahlung , der computergesttzten 3 - d - bestrahlungsplanung , der interventionellen therapie und der kombination verschiedener therapiemodalitten , hat zu einer vielzahl von studien gefhrt . 
inoperable tumoren knnen unter umstnden nach tumorverkleinerung dennoch resektabel werden . schlussfolgerungen : eine simultane radiochemotherapie mit den substanzen 5 - fu und mitomycin c ist ohne hhergradige akute nebenwirkungen durchfhrbar . 
traditionally , resection of the primary tumor in an early stage may offer the only chance for cure but it is only possible in about 10 to 30% of all patients [ 11 , 20 , 23 ]  . twenty - five years ago the answer to the question what can the radiotherapist do for the patient with cancer of the pancreas ? was : little or nothing [ 9 ]  . 
to date , the interdisciplinary guidelines of the german cancer society and the german surgical society recommend radiochemotherapy ( rct ) as the most effective therapeutic mean and as a standard for definitive treatment in locally advanced irresectable carcinoma [ 18 ]  . 
3 - d - conformal radiotherapy as a standard allows a more precise definition of the target volume and can effectively spare the dose - limiting organs ( liver , kidneys , small bowel and stomach )  . 
the patient should be supine during simulation and treatment . the clinical target volume ( ctv ) includes the tumor itself and the macroscopically involved lymph nodes ( 1.0 cm in ct scan ) , the extended clinical target volume includes furthermore regional nodal areas at risk . 
3 - d - conformal planning is performed using helical ct scan in supine treatment position without breathhold of the tumor region and the locoregional lymph nodes ( thoracic vertebra 10 through lumbar vertebra 5 , intravenous and oral contrast enhancement )  . 
adjuvant therapy since 5 - year overall survival rates after curative whipples procedure are below 10% [ 23 ] the question has been raised if adjuvant treatment could improve this unsatisfactory situation . 
 a prospective randomized trial of the gastrointestinal study group [ 12 , 19 ] compared 3 treatment arms : resection only ( arm 1 ) , resection followed by adjuvant radiochemotherapy up to a total dose of 40 gy with ( arm 2 ) or without ( arm 3 ) split - course . 
adjuvant treatment consisted in group ii ( 19 patients ) of radiation , in some patients supplemented by chemotherapy with 5 - fu ( 500 mg / m2 intravenous bolus ) on days 1 to 3 and 29 to 31 of irradiation . 
in group iii ( 20 patients ) chemotherapy was different : 1000 mg / m2 / d 5 - fu over 96 hours during the 1st and the 5th treatment week and a single dose of 10 mg / m2 of mitomycin c on day 1 . 
these patients neither had substantial acute toxicity ( who grade iii / iv ) nor late toxicity and median overall survival time as well as median disease - free survival times were 23 months and 12 months , respectively . 
 a retrospective study performed at the mayo clinic [ 10 ] , compared 89 patients with resection only with 29 patients who received adjuvant radiation therapy and in all but 2 cases simultaneous chemotherapy with 5 - fu . 
acute toxicity was only moderate . potentially therapy - related late toxicity was seen in 5 patients : compression fracture of a vertebra within the radiation therapy field , fibrosis of the pancreas , small bowel stenosis with the need of surgical treatment , renal failure 10 years author schedule number of patients median os 2 ( 3 ) - yearlocal failure ( months ) os ( % ) rate ( evaluable ) ( % ) gitsg 1987 , kalser et al . 
radiochemotherapy in ductal pancreatic carcinoma after diagnosis and fatal peritonitis after thrombosis of the superior mesenteric ve tic agents such as cisplatin , gemcitabine and doxorubicine could improve these results . 
 in another study performed at the johns hopkins university [ 8 ] a total dose of 50.4 gy was delivered to the tumor region and the regional lymphatics including 23.4 gy to the whole liver plus chemotherapy ( 5 - fu 200 mg / m2 / d ; d 138 ; 5 days per week and leucovorin 5 mg / m2 / d )  . 
the same number of patients had local relapse . acute toxicity ( who grade iii / iv ) was reported in only 3 / 14 patients , but therapy could be given as planned only in one half of the patients . 
even if local control is improved after adjuvant therapy , the frequent development of peritoneal and / or hepatic metastasis cannot be prevented . not even inclusion of the liver and the whole abdomen into the radiation treatment volume does show any advantage . 
as the patients with resection after neoadjuvant therapy had better overall survival in comparison to the patients without resection after chemoradiation , this kind of treatment was further evaluated during the 90s and meanwhile several studies of preoperative therapy have been published . 
chemotherapy consisted of 51 / 10 ( 10% ) locoreg . 4 / 39 ( 11% ) mhep : 20 mper : 4 adj : 21% neoadj : mper : 10% 0% res author number radiation of patients therapy ( gy ) chemotherapy ( mg / m2 ) median os 1 ( 2 , 4 , 5 ) year - os ( months ) local failure rate resectability r0rate resection yeung et al . 
 = not available ; iort = intraoperative radiation therapy ; ebrt = external beam radiotherapy ; 5 - fu = 5 - fluorouracil ; mmc = mitomycin c ; d = day ; w = week ; os = overall survival rate ; no res = patients without tumor resection ; res = patients with tumor resection ; pts = patients ; y = years ; locoreg . 
 = nicht angegeben ; iort = intraoperative strahlentherapie ; ebrt = externe beam - bestrahlung ; 5 - fu = 5 - fluorouracil ; mmc = mitomycin c ; d = tag ; w = woche ; os = gesamtberlebensrate ; no res = patienten ohne tumorresektion ; res = patienten mit tumorresektion ; pts = patienten ; y = jahre ; locoreg . 
patients in the 2 preoperative arms were irradiated with single fractions of 1.8 gy and a total dose of 50.4 gy , or an accelerated schedule using 3.0 gy single dose up to 30 gy . 
median overall survival of the patients in the 2 preoperative arms was again 19 months for the 52 / 91 resected patients ( 57% ) without a significant difference between conventional and accelerated fractionation . 
at restaging ( 4 weeks after radiochemotherapy ) 8 patients were not operable due to distant metastasis ( 5 patients ) or medical complications ( 3 patients ) not attributed to radiochemotherapy . 
recurrent disease was noted in the resected patients with distant metastases in 12 patients ( 60% ) and local - regional recurrence in 2 patients ( 10% )  . the fox chase cancer center ( fccc ) initiated 3 studies on preoperative chemoradiation in pancreatic carcinoma : yeung et al . 
 the second study of the fccc [ 15 ] included 30 patients whose tumors were found to be resectable and 4 patients with tumors classified to be irresectable into the study . 
eleven patients ( 44% ) were resectable after preoperative treatment . one of them died postoperatively with respiratory failure . the overall survival time of the remaining 10 resected patients was excellent with 45 months ( median ) and the 5 - year survival was 40% . 
the rate of resectability was similar to the single center study [ 13 ] with 45% ( 24 / 53 patients )  . but survival times were sobering : the resected patients had a median overall survival time of 15.7 months , a median disease - free survival time of 8.5 months and a 2 - year survival rate of 27% . 
though , one has to keep in mind that the assessment of resectability of a tumor based on ct and mri scans is very difficult and enormous interindividual variations among surgeons and radiologists have to be encountered . 
intraoperative therapy intraoperative radiation therapy offers the possibility of delivering a higher dose to the target volume without injuring the neighboring , dose - limiting organs small intestine , stomach , liver , kidneys and spinal cord . 
median survival ( 18 m vs 12 m ) as well as the frequency of local failure after one year ( 20% vs 100% ) were better in the group with intraoperative radiotherapy but the patient number with intraoperative radiotherapy was too small for a reasonable statistical analysis . 
 two trials from japan [ 1 , 27 ] with 3 treatment arms each compared adjuvant intraoperative radiotherapy only versus a combination of external beam radiation and intraoperative radiotherapy versus external beam radiation only . 
local failure rate was clearly diminished ( 27% vs 57% ) and tendency towards better overall survival ( 19 m vs 12 m ) was noted for the patients who received resection and intraoperative radiotherapy . however , in summary trials failed to establish any conclusive evidence that intraoperative radiotherapy significantly prolonged survival rates despite intraoperative radiotherapy showed significant improvement in local disease progression . patients receiving intraoperative radiotherapy did not experience a higher surgical complication rate than those not receiving intraoperative radiotherapy . 
the rtog provided data indicating that intraoperative radiotherapy rapidly and consistently palliated severe visceral padisregarded that intraoperative radiotherapy is very expensive and not standardized there could exist also a radiobiological disadvantage for intraoperative radiotherapy : 4 to 6 weeks of temporal separation between the external beam radiation dose and the intraoperative radiotherapy dose could devaluate its effect on tumor cells substantially because of accelerated repopulation [ 13 ]  . 
 study number of patients iort ( gy ) median os ( months ) 1 ( 2 , 5 ) - yearmedian dfs ( months ) local failure rate ( % ) sindelar et al . 
radiochemotherapy in ductal pancreatic carcinoma irresectable tumors external beam radiation therapy with and without chemotherapy in neoadjuvant intention since definitive chemoradiation in irresectable pancreatic carcinoma with high rates of local failure is not curative , the question was raised if neoadjuvant radiation with and without chemotherapy can convert irresectable to resectable tumors . the first group which reported on this kind of therapy [ 24 ] assessed the efficacy of radiotherapy without chemotherapy in a pilot study of 17 patients with irresectable or borderlineresectable tumors . 
 [ 17 ] treated 16 patients with irresectable tumors with a total dose of 45 gy and 225 mg / m2 / d 5 - fu ( civ , during the whole treatment time ) in neoadjuvant intention . these patients were compared to a group of 24 patients with tumors classified to be primarily resectable . 
neoadjuvant chemoradiation was well tolerated with only one patient suffering from grade - iv toxicity ( secondary gastric outlet stenosis after radiation - induced gastritis which could be treated without surgery ) and 3 patients with stomatitis and nausea of grade iii . 
median survival of the patients with neoadjuvant therapy was 9.6 months compared to 12.2 months in the group with tumors classified to be resectable at diagnosis where 15 / 24 patients were resected . 
 a recently published study from milan , italy [ 3 ] , included 32 patients with initially irresectable patients due to vascular invasion and / or massive regional nodal metastases . 
the high rate of local failure ( 53% ) is just the consequence of a great number of patients who were still irresectable after radiochemotherapy . it is not clear whether these relatively poor results can be attributed to the rather unhappy choice of a split - course protocol leading to tumor cell repopulation or to the new kind of chemotherapy or to a negative patient selection . 
radiochemotherapy in ductal pancreatic carcinoma radiotherapy 28 ( cid : 2 ) 1.8 gy + boost chemotherapy f - fu 1g / m2 / 24h mmc 10 mg / m2 d 15 d 2933 120 h pvi i.v. 
behandlungsschema ( d = tag ; 5 - fu = 5 - fluorouracil ; h = stunden ; mmc = mitomycin c ; pvi = kontinuierliche vense dauerinfusion )  . 
simultaneous chemotherapy consisted of 5 - fu ( 1000 mg / m2 / d ; 120 hours continuous infusion on days 1 to 5 and 29 to 33 ) and mitomycin c ( 10 mg / m2 ; intravenous bolus , on days 2 and 30 )  . 
toxicity was predominantly hematological ( grade 3 : 30% , grade 4 : 7% ) , furthermore nausea / vomiting ( grade 3 : 20% , grade 4 : 0% )  . 
the tumor - related overall survival rates were better for resected than for not resected patients ( 50% vs 6% 2 - year survival , p = 0.07 ) , median overall survival of the whole group was 11 months ( median follow - up 28 months )  . 
preliminary results of a phase - i study at erlangen on simultaneous neoadjuvant chemoradiation using gemcitabine and cddp in 13 patients with irresectable tumors indicate even higher resectability rates can be achieved : 8 / 13 patients were downstaged and resectable after radiochemotherapy . 
adjuvant radiochemotherapy : no results from randomized controlled trials are available to clearly prove the efficacy of adjuvant radiochemotherapy following r0 - resection of pancreatic adenocarcinoma with overall survival as primary endpoint . 
however , small series of patients treated by postoperative radiochemotherapy using 5 - fu with or without mitomycin indicate a possible survival benefit in the order of 2 - year survival rates up to 30 to 40% . 
as neoadjuvant radiochemotherapy is feasible without additional surgical complications , clinical trials may be able to address the following endpoints : facilitation of r0 - resection by effective downstaging , palliative effect if resection is not possible after radiochemotherapy . 
available studies reported on resection rates of 37 to 100% and 5 - year overall survival rates ranging from below 20% to 58% for patients with tumors found to be resectable at diagnosis . 
we recommend simultaneous chemotherapy with 5 - fu on days 1 to 5 and 29 to 33 as protracted venous infusion ( 650 to 1000 mg / m2 / 24 hours ) with or without an intravenous bolus of mitomycin c on days 1 and 29 ( 10 mg / m2 )  . 
radiochemotherapy in ductal pancreatic carcinoma strahlentherapie und onkologie urban & vogel 2000 originalarbeit chromosomal aberrations induced in mice bone marrow by treating with cisplatin and irradiation florian wrschmidt1 , mark j . 
bardenheuer2 , wolfgang - ullrich mller3 , michael molls1 background : the aim of this study was to quantify the combined effect of cisplatin and radiation on chromosomal damage with emphasis on the time interval between cisplatin and radiation . 
 methods and materials : bone marrow of female nmri - nu ( + ) mice was taken as a model system for a highly proliferative tissue irradiated with cobalt - 60 ( 1 to 4 gy )  . 
rather , cisplatin might act as an independent cytotoxic agent . key words : chromosomal aberrations cisplatin radiotherapy bone marrow experimental study chromosomale aberrationen nach cisplatin und bestrahlung im knochenmark von musen hintergrund : bestimmung des chromosomalen schadens nach kombinierter therapie mit cisplatin und bestrahlung unter besonderer bercksichtigung des zeitintervalls zwischen cisplatingabe und bestrahlung . material und methoden : knochenmark weiblicher nmri - nu ( + ) - muse wurde als modellsystem fr ein stark proliferierendes gewebe benutzt . 
cisplatin wurde zu verschiedenen zeiten vor und nach bestrahlung appliziert . knochenmark und metaphasen wurden nach standardprotokollen aufgearbeitet . ergebnisse : der anteil aberranter metaphasen nahm nach bestrahlung oder cisplatingabe dosisabhngig zu ( sigmoide dosis - wirkungs - beziehung )  . 
fr aberrante chromosomen hingegen wurden supraadditive werte nur nach cisplatinapplikation zwei und anderthalb stunden vor bestrahlung bestimmt . dies zeigt , dass supraadditivitt von dem gewhlten parameter abhngig ist . schlussfolgerung : es ist zweifelhaft , ob durch die kombinierte behandlung mit cisplatin und bestrahlung tatschlich supraadditive werte oder ein strahlensensibilisierender effekt durch cisplatin zum beispiel in der klinischen anwendung zu erwarten ist . 
in cervical cancer treated concurrently with a cisplatin - based chemotherapy and radiotherapy as was published very recently in 3 large prospective randomized trials [ 3 , 6 , 7 , 11 ]  . 
the radiosensitizing potential of cisplatin is unclear as results seem to depend on the model system and assay used ( clonogenic assay , growth delay , stem cell assay , crypt cell assay ) [ 1 ]  . 
 the aim of the current study was to evaluate the combined effect of cisplatin and radiation on chromosomal damage . the interval between cisplatin and radiation was of specific interest with regards to a potential supraadditive or radiosensitizing effect of cisplatbone marrow of mice was taken as a model system of a highly proliferative tissue . 
the field size was 22 ( cid : 2 ) 20 cm and the sourcesurface distance was 77.5 cthe center of the body of the animals was taken as the reference point . 
metaphases were counted under the microscope considering the total number of chromosomes and the number of chromosomes with aberrations . metaphases with 39 to 42 chromosomes were analyzed if all chromosomes were identifiable . 
metaphases with 41 and 42 chromosomes were analyzed as numerical aberrations ; in the rare situation of metaphases with 39 chromosomes , this was considered to be technically induced due to the loss of a chromosome . 
 according to phillips [ 8 ] , the cumulative probability of metaphase damage results from the multiplication of the probabilities of no damage to metaphases with the single agents ( cisplatin and radiation )  . in the combined cisplatin radiation experiments the significance of a higher than additive level was determined according to hogan et al . 
a sigmoidal dose - response was found indicated by the fitted curve ( goodness of fit , r2 = 0.989 ) showing a steep increase of the percentage of aberrant metaphases between 1 and 2 gy and plateauing at doses above 2 gy . 
the animals were kept according to international standards of animal care at a 12 hours lights - on 12 hours lights - off rhythm and received water ad libitu data analysis wrschmidt f , et al . 
a sigmoidal dose - response curve could be fitted to the data ( goodness of fit , r2 = 0.969 ) with an initial steep part for cisplatin doses of up to 20 mg / kg and a plateau for higher doses . 
a single dose of cisplatin ( 9 mg / kg ) was injected at figure 1a abbildung 1a figure 1b abbildung 1b dose ( gy ) dose ( gy ) figures 1a and 1b . 
der prozentsatz aberranter metaphasen ( a ) und aberranter chromosomen ( b ) als funktion des zeitintervalls in stunden zwischen cisplatininjektion ( 9 mg / kg intraperitoneal ) und bestrahlung ( einzeldosis von 1 , 5 gy )  . 
the additive value was calculated to be 3.48%. discussion to our knowledge , the data presented here quantify for the first time the combined effect of cisplatin and radiation on chromosomal damage . 
thus , any conclusions concerning the clinical situation should be drawn with extreme care keeping in mind the above mentioned limitations . for radiation alone , a sigmoidal dose - response relationship was observed . 
analyzing the distribution of the different types of aberrations , more metaphases carrying multiple damaged chromosomes were observed at doses of 1.5 gy or higher in comparison to lower radiation doses ( data not shown )  . 
the situation is less clear for the application of cisplat at a dose of 4.5 mg / kg or higher , the predominant types of damage were chromatid breaks and an increasing number of multiple damaged metaphases could be found ( data not shown )  . 
the analysis of the frequency of the types of aberrations ( data not shown ) did not show a time - dependent distribution of chromatid breaks , chromosomal breaks , numerical aberrations , or the number of aberrant chromosomes per metaphase . 
analyzing the percentage of aberrant chromosomes ( see figure 3b ) , however , reveals supraadditive values only if cisplatin was given 2 and 1.5 hours before irradiation but not at time intervals after irradiation . 
according to the results of the present experimental study performed in normal mice bone marrow as a model of a highly proliferative tissue , it is in our opinion doubtful to always achieve a true supraadditive or radiosensitizing effect of cisplatin combined with radiation . 
chromosomal aberrations after cisplatin and radiotherapy strahlentherapie und onkologie urban & vogel 2000 originalarbeit sentinel node concept in breast cancer ion - christian kiricuta1 background / purpose : it seems that there exists a specific lymph node center called sentinel node ( sn ) which appears to be the primary site of metastases . 
the sentinel node concept ( snc ) is fundamentally based on the orderly progression of tumor cells within the lymphatic systeit is the most important new concept in surgical and radiation oncology . 
 material and methods : lymphoscintigraphy and gamma probe biopsy is necessary to show predictable lymph flow to the regional sentinel node , to multiple sentinel nodes or unpredictable lymph flow to extra - regional sentinel nodes and for performing sentinel node procedure . 
the standard protocol for the evaluation of the sentinel node metastases consists of extensive histopathological investigation including step hematoxylin & eosin ( h&e ) stained sections and immunohistochemistry . results : a high rate of success of the identification of the sentinel node for breast cancer was reported . 
new target volumes are defined for adjuvant radiotherapy or lymphatic basins could be spared from unnecessary irradiation . conclusion : the sentinel node concept seems to revolutionize the treatment of early breast cancer . 
biopsy of the sentinel node is a highly accurate , minimally invasive method of staging patients and can substantially reduce the morbidity and costs of treatment by avoiding unnecessary complete axillary lymph node dissection . 
the identification of the individual lymphatic flow pattern would permit the irradiation of the individual locoregional lymphatic basin . key words : sentinel lymph node breast cancer staging adjuvant treatment minimally invasive treatment regional lymphatics das sentinel - lymphknoten - konzept beim mammakarzinom hintergrund / ziel : es scheint , als ob es einen bestimmten lymphknoten gibt , der als wchter - lymphknoten oder sentinel node ( sn ) bezeichnet werden kann und der als erster von tumorzellen befallen wird . 
 patienten und methode : die lymphszintigraphie und die von einer szintillationsmesssonde gesteuerte biopsie sind notwendig , um den eigentlichen lymphstrom zu dem vermuteten regionalen sentinel node oder zu unvorhersehbaren sentinel nodes , die extraregional lokalisiert sein knnten , zu dokumentieren . 
in das standardprotokoll des sentinelnode - konzepts ist die aufwndige histopathologische aufarbeitung des sentinel - lymphknotens mit hmatoxylineosin - ( h&e - ) frbungstechnik und immunhistochemie fest einbezogen . ergebnisse : eine hohe erfolgsrate ( um 100% ) wurde fr die identifizierung des sentinel node beim mammakarzinom berichtet . 
neue zielvolumenbestimmungen fr die adjuvante strahlentherapie beim mammakarzinom sind mit hilfe des sentinelnode - konzepts mglich . schlussfolgerungen : das sentinel - node - konzept wird die adjuvante behandlung des mammakarzinoms beeinflussen . die sentinel - node - biopsie ist ein sehr akkurates verfahren , minimalinvasiv und mit einer hohen erfolgsrate , die eine optimale stadienbestimmung ermglicht . 
die identifizierung der eigentlichen regionalen lymphabflusswege und eine individuelle zielvolumenbestimmung fr eine perkutane strahlentherapie werden so ermglicht . schlsselwrter : sentinel - lymphknoten tumorstaging adjuvante therapie minimalinvasive therapie regionale lymphknoten t he subject of selective lymph node dissection ( slnd ) has been one of the most important controversies in the management of patients with malignancy . 
the first involves the anatomical extent of surgical dissection against the orderly pattern of tumor spread . the second considers the blood and lymphatic system so unified , insofar as tumor spread is concerned , that there can be no orderly pattern of tumor cell dissemination based on mechanical considerations stressed thus the systemic nature of the cancer . 
in breast cancer these 2 opposite opinions are known as the halstedian [ 19 , 20 ] and fishers theory [ 12 ]  . in fishers theory the pattern of tumor spread is not solely dictated by anatomical considerations but is influenced by intrinsic factors in tumor cells and in the organs to which they gain access . 
the clinical routine shows that despite of nodal involvement long - time survivors with only local treatment exist and only the involvement of the axillary nodes could be considered as local disease , whereas the involvement of the supraclavicular nodes should be considered as systemic disease [ 24 , 25 ]  . 
the representation of the metastatic spread for a solid tumor on the example of breast cancer in the light of the halstedian orderly progression , the fishers random progression and as in the routine observed and described as the reality are shown in figure 1 . distinct differences what survival concerns exist between patients with uninvolved locoregional lymph nodes and involved axillary nodes . 
no difference between patients with involvement of the supraclavicular nodes at primary diagnosis to patients with distant disease ( m1 stage ) was noted as shown in table 1 . stage of disease involvement of the axillary nodes ( number of involved nodes ) 10 - year survival rates ( % ) 1 3 4 9 > 10 n + ( low ) n + ( high ) n + ( very high ) supraclavicular node involvement ( m1 ) 65 75 45 65 25 30 table 1 . 
zehn - jahres - berlebensraten der nodal negativen und nodal positiven patientinnen im vergleich mit patientinnen , bei denen die supraklavikulren lymphknoten bei primrdiagnose befallen waren , oder patientinnen mit einer fernmetastasierung bei primrdiagnose ( daten von [ 25 , 42 ] )  . a historical owerview of the most important hypothesis on the orderly pattern of spread or systemic nature of cancer and the evolution to the sentinel node concept and procedure and of clinical facts which sustain these hypothesis are summarized in table 2 . the sentinel node concept the sentinel node concept , originally described by cabanas in 1977 [ 4 ] is based on the orderly progression of tumor cells within the lymphatic syste metastasis to lymph nodes is not a random event and can be determined by identifying the lymph flow from the tumor site to the primary draining lymph node . 
 the factors which preclude nodal uptake determined by reduced functional capacity or lower detection rate are as follows : extensive tumor infiltration , lymph node hyperplasia , fatty degeneration and prior excision biopsies . point of view / author hypothesis clinical facts 1863 virchow [ 46 ] regional lymph nodes are effective barrier to tumor cell dissemination 19071935 halsted [ 19 , 20 ] surgical paradigm the cancer of the breast spread by direct extension along lymphatic pathways to distant premenopausal breast cancer patients succeeded to sites and preserved continuity with original growth clinical facts are expected . 
many cancer patients with lymph node involvement live for extended periods of time after effective locoregional treatment randomized dbcg study [ 38 ] on 1 , 708 high - risk demonstrate that postoperative rt improved distant disease - free survival , survival ( 9% ) and reduced the incidence of locoregional disease the randomized nsabp study failed to demonstrate that postoperative rt improved either distant disease - free survival or survival although it reduced the incidence of locoregional disease it offers an alternative to routine lymph node dissection . randomized trials were started to validate this procedure ( breast cancer , melanoma ) 1968 fisher [ 12 ] systemic disease 1977 cabanas [ 4 ] sn concept 1992 morton et al . 
das sentinel - lymphknoten - konzept [ 37 ]  . drainage patterns over the years almost every lymphatic basin and region has been demonstrated by lymphoscintigraphy employing a variety of injection techniques and tracers . 
in breast cancer patients ege [ 11 ] demonstrated by lymphoscintigraphy the lymphatic regions as shown in table 4 . the concordance between lymph node biopsy and lymphoscintigraphy ( surgery vs nuclear medicine ) the drainage of different sites of the breast was studied using node biopsy and nuclear medicine methods as lymphoscintigraphy . 
haagensen [ 18 ] in 1967 and handley [ 21 ] studied extensively the lymphatic drainage of each quadrant and the central area by performing systematic lymph node dissection of the mammaria interna lymph nodes on 1 001 respectively on 800 breast cancer patients . 
comparative to these data the patterns of lymphatic drainage from different tumor locations found in 122 examined breast cancer patients through lymphoscintigraphy ( parasternal foci ) and gamma probe procedure ( for axillary sentinel nodes ) are shown in figure 3b . 
the results of borgstein [ 2 , 3 ] are in agreement with the data from handley [ 21 ] and haagensen [ 19 ]  . the rate of success of the sentinel node procedure the rate of success of the sentinel node procedure for the breast cancer patients was reported as high as 100% [ 33 ]  . lymphoscintigraphy and pathological investigation in 1993 alex et al . 
the accurate localization of sentinel node was demonstrated using technetium - 99m - sulfur colloid , antimony trisulfide colloid or nanocolloidal albumin . the distribution of administered particles heavily depends on the particle size . 
molecules smaller than a few nanometers may leak into capillaries and may be dispersed into the vasculymph flow is orderly and predictable tumor cells disseminate sequentially the sn is the first node encountered by tumor cell sn status predicts distant basin status applicable to early stage of disease basin involvement is less frequent surgical procedure table 3 . 
die theoretischen grundlagen des sentinel - lymphknoten - konzepts [ 23 ]  . injection site lymph node groups mammary , peri - areolar chest wall subcutaneous , subperiosteal subcostal posterior rectus sheath peritumoral , intracutaneous axillary , supraclavicular , upper parasternal axillary , supraclavicular , upper parasternal diaphragmatic , parasternal , internal mammary mediastinal superficial lymphatics at risk table 4 . 
die lymphdrainage der einzelnen bereiche der brust und thoraxwand ( nach [ 11 ] )  . lar syste particles larger than 100 nm usually become trapped in interstitial space and never enter the lymphatic syste accurate localization of sentinel nodes was demonstrated using technetium - 99m - sulfur colloid , antimony trisulfide colloid or nanocolloidal albumin [ 47 ]  . 
 [ 37 ] reported 100% sensitivity with lymphoscintigraphy in 155 patients with microcolloidal albumearly and dynamic scans are necessary for identification of lymphatic channels . the task of the pathologist is to screen sentinel nodes for metastases . 
 [ 30 ] reported that in the 383 patients with single spots , 365 ( 95.3% ) were at level i , 13 ( 3.3% ) at level ii and none at level iii . 
a review of studies which reported the results of more than 100 sentinel node dissections shows a high rate of identification of the sentinel nodes in more than 90% of the patients and a low rate for false negative results about 5% ( table 6 )  . 
not seldom is this node localized in non - locoregional nodes or in 2 lymphatic basins or anatomically unpredictable lymph node basins as defined adenocarcinoma ( including breast ) intraoperative procedure postoperative procedure single h&e frozen - section analysis with imprint cytology h&e step sections ( 3 with 500 m interval or 5 with 250 m interval ) with cam5.2 ich squamous cell cancer melanoma intraoperative procedure postoperative procedure intraoperative procedure postoperative procedure single h&e frozen - section analysis with imprint cytology h&e step sections ( 3 with 500 m interval or 5 with 250 m interval ) with ae1 / 3 ich not recommended h&e step sections ( 3 with 500 m interval or 5 with 250 m interval ) with s100 and hmb45 ihc table 5 . 
thus , the sentinel node procedure is deciding which lymphatic basin is really the locoregional . the data reported on the sentinel node procedure what concerns the staging and properly indications for adjuvant local or systemic treatment were reconsidered in the tnm classification . 
recently the tnm committee has proposed for trial to use the following option [ 41 ] to record sentinel lymph node status : pnx ( sn ) : sentinel lymph node could not be assessed , pn0 ( sn ) : no sentinel lymph node metastasis , pn1 ( sn ) : sentinel lymph node metastasis . for that a standardization of the procedure would be indicatsentinel node procedure vs complete axillary dissection in breast cancer patients the high predictable power of the sentinel node procedure about the nodal status of the whole lymphatic basin was demonstrated in many studies [ 30 , 44 ]  . 
the sentinel node was positive in 22.7% of the patients , in 53.5% there was the only 1 node involved , in 12% it was false negative . recently , veronesi et al . 
die aussagekraft der sentinel - node - biopsie zum axillastatus im vergleich zur kompletten axilladissektion ( nach [ 3 ] )  . sentinel node axillary nodes number of patients 143 ( 69.4% ) 53 ( 25.7% ) 10 ( 4.8% ) total 206 sentinel lymph nodes and axillary lymph node status was 96.8% ( 359 of 371 ) , while the rate of false negatives among patients with at least 1 positive lymph node was 6.7% ( 12 of 180 )  . clinical consequences from sentinel node procedure in breast cancer patients the clinical consequences of the sentinel node procedure are as follows : 1 . 
it indicates the radiation oncologist how to choose adequate target volumes for properly irradiation . the residual tumor after an incomplete axillary dissection , extension of the axillary dissection the importance of the adequate number of axillary lymph nodes to be examined to describe a real pn0 axillary status was described by kiricuta et al . 
in pn0 patients if more than 9 nodes were examined a 10 - year survival around 90% was noted . later , a mathematical model based on 1 , 446 complete axillary dissections performed by veronesi et al . 
how many other nodes have to be examined in sentinel - node positive patients to be sure that all involved nodes are removed ? based on a mathematical model developed by us [ 27 ] using the data of 1 , 396 complete axillary dissections for t1 and t2 breast tumors performed by veronesi et al . 
bereinstimmung zwischen dem axillastatus anhand der sentinel - lymphknoten - biopsie und dem nach kompletter axilladissektion bei 206 patientinnen mit mammakarzinom ( nach [ 13 ] )  . an open problem is the case in which the sentinel node is minimally involved . 
in klammern sind die werte fr einen t2 - primrtumor angegeben [ 26 ]  . tochemical staining , an axillary node involvement in 7.7% compared to a 25% incidence when micrometastases were detected by h&e staining . 
of the 64 patients with metastases measuring more than 2 mm in maximum diameter , 38 ( 59% ) had additional metastatic axillary nodes , whereas of the 49 cases with micrometastases only in the sentinel node , 9 ( 18% ) harbored metastatic deposits in the non - sentinel node . 
 [ 45 ] showed that sentinel lymph nodes involved by microfoci of cancer cells are , however , associated with a considerable rate of metastastic involvement in the rest of the axillary lymph nodes of 53% ( 27 of 51 )  . 
they concluded that the presence of microfoci in the sentinel lymph node is an indication to perform a total axillary dissection . the parasternal lymph nodes in breast cancer the study of borgstein et al . 
 [ 2 , 3 ] with lymphoscintigraphy revealed the individual lymph flow to the mammaria interna lymph nodes for the different quadrants of the breast ( see figure 3b )  . 
the outer quadrants drain their lymph to the parasternal nodes in a lower probability ( 8 to 19% ) than the inner quadrants and central area ( 21 to 31% )  . 
 the role of adjuvant therapy in breast cancer patients axillary lymph node dissection at levels i , ii and iii when metastatic involvement is suspected , should provide an answer as to whether metastatic spread to the axilla has occurred . 
the dbcg study [ 38 ] demonstrated improvement in survival additionally to improved local control if adjuvant radiotherapy to high - risk patients ( > 3 nodes involved ) was administered . 
the today obtained improvement of survival by adjuvant treatment is summarized in table 10 . target volume definitions for adjuvant treatment based on the new data obtained by the sentinel lymph node concept new definitions for the clinical target volume for adjuvant radiotherapy are possible . 
for instance for a primary tumor in the breast independent of the location in one of the quadrants of the breast or centrally and independent of the status of the axillary lymph nodes if no drainage to the parasternal nodes is visible by gamma probe an avoidance of the irradiation of these region should be possible . 
if simultaneous drainage to the parasternal and axillary nodes is evident and no nodes are clinically palpable in the axilla or the parasternal nodes visible by an imaging method only adjuvant irradiation of these areas should be indicated . all these new definitions of clinical target volume definitions have to be investigated by clinical trials . conclusions the sentinel node concept seems to revolutionize the treatment of early cancers . 
biopsy of the sentinel node is a highly accurate , minimally invasive method of staging patients and can substantially reduce the morbidity and costs of treatment by avoiding unnecessary complete axillary lymph node dissection or adjuvant treatment . 
sentinel node concept in breast cancer strahlentherapie und onkologie urban & vogel 2000 aktuelles forum strahlentherapeutische strategien in der multimodalen therapie des resektablen und nicht resektablen pankreaskarzinoms thomas wiegel1 , norbert runkel2 , hermann frommhold3 , christian rbe4 , wolfgang hinkelbein1 hintergrund : die prognose der patienten mit pankreaskarzinom ist unverndert schlecht . 
auch die integration der intraoperativen strahlentherapie ( iort ) wird kontrovers diskutiert . material und methode : seit den ergebnissen der gitsg - studie gilt die postoperative adjuvante radiochemotherapie mit 5 - fu in den usa als standard . 
in einzelnen spezialisierten institutionen werden diese konzepte mit einer iort kombiniert . neuere chemotherapeutika wie gemcitabin und die taxane werden in phase - ii - studien als kombinierte radiochemotherapie bei primr inoperablem pankreaskarzinom getestet . ergebnisse : sowohl durch die postoperative adjuvante als auch durch die neoadjuvante radiochemotherapie mit anschlieender pankreatikoduodenektomie knnen mediane berlebensraten von 15 bis 25 monaten erreicht werden . durch die neoadjuvante radiochemotherapie bei primr resektablem pankreaskarzinom scheint die rate positiver postoperativer schnittrnder sowie die anzahl der patienten mit lymphknotenmetastasen reduziert zu werden . 
neuere substanzen wie gemcitabin und die taxane scheinen in vitro wirksame strahlensensitizer zu sein ersten ergebnissen in phase - iund phase - ii - studien wurde die mtd noch nicht gefunden . 
 schlussfolgerungen : vor dem hintergrund der unverndert schlechten prognose des pankreaskarzinoms werden zur zeit unterschiedliche konzepte der adjuvanten und neoadjuvanten kombinierten radiochemotherapie , teils auch mit neueren substanzen , geprdies betrifft sowohl resektable als auch nicht resektable pankreaskarzinome . 
multimodale therapie des pankreaskarzinoms chemotherapie bei lokoregionr begrenztem inoperablen pankreaskarzinom bei entsprechendem allgemeinzustand derzeit die therapie der wahl . schlsselwrter : pankreaskarzinom strahlentherapie radiochemotherapie radiotherapeutic strategies in the multimodality approach of resectable and non - resectable pancreatic carcinoma background : the prognosis of patients with adenocarcinoma of the pancreas remains poor . 
the value of combined radio - chemotherapy adjuvant or even palliative in case of unresectable tumors is controversial due to the short median survival times of all patients ranging from 8 to 15 months . 
 material and methods : since the publication of the results of the historic gitsg study , in the us postoperative adjuvant radio - chemotherapy with 5 - fu remains the treatment of choice . 
more modern chemotherapeutic agents like gemcitabine or the taxanes are under investigation , using combined radio - chemotherapy in phase - ii protocols in patients with unresectable tumors . results : in case of both , adjuvant or neoadjuvant radio - chemotherapy following or before pancreaticoduodenectomy , median survival times range from 15 to 25 months . 
for the moment , there is no proven survival advantage or increase of local control ( about 80% in both cases ) for patients treated with neoadjuvant radiochemotherapy compared with adjuvant radio - chemotherapy . 
 conclusions : due to the worse prognosis of patients with adenocarcinoma of the pancreas , new combined treatment modalities as adjuvant and neoadjuvant radio - chemotherapy , particularly with more modern chemotherapeutic agents , for patients with resectable and unresectable tumors are under investigation . 
in patients with unresectable tumors and good condition , combined radio - chemotherapy remains the treatment of choice . key words : pancreatic carcinoma radiotherapy radio - chemotherapy i n den letzten jahren hat die inzidenz des duktalen adenokarzinoms des pankreas weltweit zugenommen . 
ursache fr die schlechte prognose ist die oft bereits bei diagnosestellung vorhandene lebermetastasierung und / oder eine lokale inoperabilitt , weshalb nur 10 bis 20% der tumoren zu diesem zeitpunkt unter kurativer intention resektabel sind [ 1 ]  . hufig wird die diagnose wegen retroperitonealer schmerzen gestellt , die in der regel einem weit fortgeschrittenen tumorstadium entsprechen . 
nach kompletter tumorresektion ( r0 ) betragen die mediane berlebenszeit je nach tumorstadium , lymphknotenstatus und adjuvanten therapiemanahmen 13 bis 25 monate und die fnf - jahres - berlebensrate 5 bis 20% [ 1 , 11 , 32 , 33 ]  . 
die mediane berlebenszeit von patienten mit r1 / r2 - resektion des tumors entspricht der von patienten , die ohne operation eine palliative radiochemotherapie erhalten , und betrgt acht bis elf monate [ 32 , 38 ]  . 
dosisfindungsstudien sowohl fr 5 - fu als auch fr gemcitabine oder die taxane sind abgeschlossen oder werden durchgefhrt [ 2 , 5 , 19 , 27 , 37 ]  . 
die einfhrung der 3 - d - planung erlaubt die applikation hherer dosen als 40 gy , die lange als standard galten [ 16 , 32 ]  . ber die intraoperative boost - therapie liegt eine groe zahl allerdings ausschlielich retrospektiver untersuchungen vor [ 6 , 15 , 36 ]  . 
die wertigkeit dieser therapien im vergleich zur palliativen kombinierten radiochemotherapie wird untersucht , und die ersten ergebnisse von phase - i / iistudien der kombinierten radiochemotherapie bei inoperablem pankreaskarzinom mit neueren substanzen werden diskutiert . 
 adjuvante therapiekonzepte seit publikation der ergebnisse der randomisierten studie der gitsg im jahre 1987 wird in den vereinigten staaten , im gegensatz zum europischen raum , in vielen zentren eine adjuvante kombinierte radiochemotherapie nach einer pankreatikoduodenektomie durchgefhrt . 
die patienten erhielten eine split - course - therapie mit 40 gy ( nach zwei wochen radiotherapie zwei wochen pause ) , an jeweils drei tagen in der woche 1 und 5 wurden 500 mg / m2 5 - fu als bolus gegeben . 
wegen dieser kritikpunkte wurde das konzept , teilweise in geringen modifikationen , in randomisierten studien der eortc und der espac berprft [ 14 , 19 ]  . in der nachfolgeuntersuchung der gitsg - studie durch die eortc ( eortc - protokoll 40891 ) wurden bei gleicher gesamtdosis ( 40 gy ) mit zwei wochen pause nach 20 gy und bei gleicher chemotherapie ohne eine weiterbehandlung nach ende der radiochemotherapie im vergleich zu keiner therapie insgesamt 218 patienten randomisiert . 
die patienten wurden jedoch nicht nach resektionsstatus ( r0 oder r1 ) stratifiziert , und nur ein relativ geringer anteil hatte wirklich ein pankreaskarzinom , sodass die aussagekraft dieser studie neben weiteren kritik - punkten ( split - course - technik ) zu gering fr definitive schlussfolgerungen ist [ 25 ]  . zeitgleich zu der studie der eortc wurde eine vierarmige , prospektiv randomisierte studie der espac ( espac - 1 ) gestartet . 
der standardarm war die alleinige postoperative nachbeobachtung , im zweiten arm wurde eine alleinige radiotherapie bis 40 gy , im dritten arm eine kombinierte radiochemotherapie mit 5 - fu als bolusgabe und im vierten arm zustzlich eine sechs monate dauernde erhaltungstherapie mit 5 - fu eingesetzt . 
die patienten konnten nach der radikaloperation zwischen keiner therapie , einer standardtherapie ( radiochemotherapie hnlich der therapie der gitsg ) und einer intensivierten therapie ( hhere gesamtdosis und prophylaktische leberbestrahlung ) whlen . 
bei einer medianen nachbeobachtung von 14 monaten fr die lebenden patienten ergab sich ein signifikanter berlebensvorteil fr die patienten mit standardtherapie , jedoch kein weiterer vorteil fr die mit intensivierter therapie . 
in der multivariaten analyse zeigte sich ein signifikanter berlebensvorteil bei tumoren > 3 cm , bei einem intraoperativen blutverlust von weniger als 700 ml und marginal bei positivem schnittrand [ 38 ]  . die kritik an diesen ergebnissen bezog sich auf die freie auswahlmglichkeit der patienten . 
die morbiditt der adjuvanten therapie wird allgemein als relativ gering eingestu etwa 30% der patienten zeigen eine gastrointestinale toxizitt grad 1 / 2 , die rate schwerer sptnebenwirkungen liegt bei 3% [ 5 ]  . von der rtog wurde 1997 eine prospektiv randomisierte studie aktiviert , in der eine synthese der bisherigen kritikpunkte versucht wurde ( rtog 97 - 04 )  . 
es wird zwischen 5 - fudauerinfusion ( drei wochen 250 mg / m2 ) und einer gabe von gemcitabine ( drei wochen , 1 - mal 1000 mg / m2 / woche ) randomisiert . 
dann erfolgt die radiochemotherapie in beiden armen identisch mit einer dauerinfusion 5 - fu ( 250 mg / m2 tglich ) whrend der gesamten radiotherapie bis 50 , 4 gy . die therapie wird abgeschlossen durch zwei zyklen 5 - fu ( vier wochen dauerinfusion 250 mg / m2 und zwei wochen pause ) oder drei zyklen gemcitabine ( 1000 mg / m2 / woche mit jeweils einer woche pause ) [ 20 ]  . 
die dauerinfusion von 5 - fu richtet sich nach den ergebnissen der dosisfindungsstudie der eastern cooperative oncology group ( ecog ) , in der 250 mg / m2 als mtd bei einer bestrahlungsdosis von 59 , 4 gy definiert wurden [ 34 ]  . eine zustzliche prophylaktische leberbestrahlung ohne nachweis von lebermetastasen wurde am m . 
da zustzlich keine verbesserung der berlebenszeit , aber eine hohe toxizitt resultierte , ist eine prophylaktische leberbestrahlung nicht zu empfehlen [ 3 ]  . zusammenfassend lassen die retrospektiven resultate groer einzelinstitutionen sowie die bisherigen ergebnisse randomisierter studien zwar eine signifikante verlngerung der berlebenszeit erkennen . 
eine erhaltungstherapie , vorzugsweise mit 5 - fu , eventuell jedoch auch mit gemcitabine , sollte bis zum progress angeschlossen werden . neoadjuvante therapiekonzepte im gegensatz zu der postoperativen kombinierten radiochemotherapie , die mehr als 25% der patienten wegen der operativen morbiditt nicht erhalten knnen [ 16 , 21 , 31 , 38 ] , bietet die neoadjuvante kombinierte radiochemotherapie besonders bei primr operablem , mglicherweise auch beim inoperablen pankreaskarzinom theoretische vorteile . 
die mediane berlebenszeit von patienten mit r1 / r2 - resektion des tumors entspricht der von patienten , die ohne operation eine palliative radiochemotherapie erhalten , und betrgt acht bis elf monate [ 32 , 38 ]  . 
da sie nur eine lebenserwartung von etwa fnf bis acht monaten haben , knnen sie dann einer nebenwirkungsrmeren palliativen therapie zugefhrt werden [ 16 , 21 , 36 ]  . 
auch die zustzliche bestimmung des ca 19 - 9 kann bei der entscheidung zur operation helfen : steigt es unter der radiochemotherapie an , betrgt die wahrscheinlichkeit der inoperabilitt oder der fernmetastasierung ber 90% [ 35 ]  . 
besonders die niedrige , kaum mehr verbesserungsfhig erscheinende lokalrezidivrate unter 20% fhrte die autoren zu der schlussfolgerung , dass das primat zuknftiger therapiekonzepte in verbesserungen der systemischen komponente zu suchen sein sollte . aus der arbeitsgruppe um evans aus dem m . 
anderson cancer center wurden vergleichbare ergebnisse der radiochemotherapie mit 50 , 4 gy gesamtdosis berichtet . allerdings mussten etwa 30% der patienten wegen der akutreaktionen ( besonders belkeit , erbrechen und gewichtsverlust ) stationr behandelt werden [ 16 ]  . 
 [ 22 ] ber 35 patienten mit primr resektablem pankreaskarzinom , die mit einer akzelerierten strahlentherapie ( 10 - mal 3 gy ber zwei wochen ) und zustzlicher kontinuierlicher 5 - fugabe ( 300 mg / m2 ber fnf tage ) neoadjuvant ambulant behandelt wurden . 
55% der pankreaskarzinome zeigten eine geringe remission , 25% eine zerstrung von 10 bis 50% der tumorzellen , 20% eine zerstrung von 50 bis 90% der tumorzellen , ein tumor einen progress . 
die uerst geringe lokale rezidivrate von 10% zeigt nach ansicht der autoren , vergleichbar anderen , den dringenden bedarf einer weiterfhrenden chemotherapie nach abschluss der primren therapie , denn die meisten patienten verstarben an der fernmetastasierung [ 22 ]  . zwischen 1991 und 1993 wurde von der ecog eine multizentrische phase - ii - studie zur neoadjuvanten radiochemotherapie des primr resektablen pankreaskarzinoms initiiert [ 11 ]  . 
1000 mg / m2 5 - fu wurden als 96 - stunden - infusion in den wochen 1 und 5 zustzlich mit 10 mg / m2 mitomycin c an tag 2 gegeben . 
von den autoren wurde kritisch diskutiert , dass viele der patienten nach schrferen kriterien primr nicht resektabel gewesen wren und die relativ schlechten ergebnisse hierdurch erklrbar wren [ 11 ]  . bei primr als inoperabel eingestuftem pankreaskarzinom wurde durch die neoadjuvante radiochemotherapie in ca . 
10 bis 20% eine radikale resektion ( r0 ) mglich [ 12 , 13 , 29 ]  . bei den patienten mit weiterhin nicht resektablem pankreaskarzinom kann dann die palliative erhaltungschemotherapie eingesetzt werden . zusammenfassend erscheint aus theoretischer sicht die neoadjuvante radiochemotherapie besonders bei primr resektablem pankreaskarzinom sehr interessant , obwohl signifikante berlebensvorteile bei sehr hohen lokalen kontrollraten von ber 80% bisher nicht berichtet wurden . 
das ziel der operation muss der negative schnittrand , das heit die komplette tumorresektion , se besteht postoperativ ein positiver schnittrand , wird die berlebenszeit der patienten durch die radikale operation mit ihrer einschrnkung der lebensqualitt nicht verlngert . 
bei bis zu 25% der patienten , die vier wochen nach der neoadjuvanten therapie fernmetastasen entwickeln oder als inoperabel eingestuft werden , kann die nunmehr rein palliative therapie durch eine kontinuierlich weitergefhrte chemotherapie komplettiert werden . 
besonders wichtig ist , dass mehr als 25% der operierten patienten postoperativ eine radiochemotherapie aus unterschiedlichen grnden nicht erhalten knnen , ein punkt , dem von der mehrheit der autoren besondere bedeutung eingerumt wird . 
diese sind inzwischen aktiviert oder werden mit neueren substanzen geplant . therapiekonzepte bei lokoregionr begrenztem inoperablen pankreaskarzinom die lokalrezidivrate mit der alleinigen strahlentherapie , auch mit dosen ber 50 gy , betrgt bis zu 70% [ 4 , 26 ]  . 
nach dem ergebnis einer randomisierten studie der gitsg gilt die kombinierte radiochemotherapie mit 5 - fu als bolusinjektion an den ersten drei tagen der jeweils zweiwchigen bestrahlung ( jeweils 20 gy ) mit einer pause von zwei wochen als therapie der wahl . 
im rahmen dieser dreiarmigen studie konnte gezeigt werden , dass durch die zustzliche erhhung der gesamtdosis von 40 auf 60 gy nur eine marginale verlngerung der berlebenszeit erreicht wird [ 17 ]  . aus den bereits beschriebenen grnden wird heute jedoch keine split - course - therapie mehr eingesetzt , die typische fraktionierung betrgt 1 , 8 gy bis zu einer gesamtdosis von 45 bis 50 , 4 gy . fraktionierungsschemata , durch die die behandlungszeit bei geringer nebenwirkungsrate verkrzt werden kann , sind wegen der relativ langen behandlungszeit von besonderem interesse . 
diese daten sind vergleichbar den ergebnissen bei anderen kollektiven , die gesamtbehandlungszeit der patienten ist jedoch um zwei bis drei wochen krzer [ 17 , 24 , 26 ]  . 
 [ 13 ] berichten ber 35 patienten mit primr nicht resektablem pankreaskarzinom , die einer kombinierten radiochemotherapie von 54 gy in drei blcken mit je 18 gy ber zwei wochen unterzogen wurden . 
parallel zu jedem block wurden 1000 mg / m2 5 - fu ber 4 , 5 tage , 300 mg / m2 streptozocin an tag 1 bis 3 und cisplatin 100 mg / m2 an tag 3 appliziert . 
insbesondere die verwendete gesamtdosis von 40 gy und die split - coursetechnik werden jedoch inzwischen kritisch beurteilt [ 34 ]  . zusammenfassend belegen die daten die hohe effektivitt der kombinierten radiochemotherapie bei primr inoperablem pankreaskarzinosie sollte , ob akzeleriert oder nicht akzeleriert , die therapie der wahl se durch sie werden das berleben der patienten bei miger toxizitt verdoppelt und eine hervorragende palliation erzielt . 
nach ende der radiochemotherapie sollte eine erhaltungschemotherapie bis zum progress zum einsatz kommen . die iort im multimodalen therapiekonzept die intraoperative strahlentherapie ( iort ) mit schnellen elektronen ist seit mitte der 70er jahre in vielen zentren etabliert [ 37 ]  . 
diese liegen in einer hohen einzeitdosis bei einem gut zu definierenden zielvolumen ( pankreas bzw . pankreasbett mit angrenzenden lymphknoten ) , wobei die nebenwirkungsrate wegen des steilen dosisabfalls der schnellen elektronen bei einer dosis von 10 bis 20 gy gering ist [ 6 , 37 ]  . 
diese lokale kontrolle ist hher als bei alleiniger palliativer radiochemotherapie , die zwischen 30 und 50% liegt [ 24 , 28 ] , sie hat jedoch den nachteil einer erhhten morbiditt durch die zustzliche laparotomie . die besten daten der lokalen tumorkontrolle werden durch die kombination aller drei verfahren , der kurativen resektion in verbindung mit iort und der proder postoperativen radiochemotherapie , erzielt . 
an zentren mit groer erfahrung betrgt die lokale tumorkontrollrate dann zwischen 80 und 90% , wobei die zustzliche toxizitt der iort gering zu sein scheint [ 16 , 22 , 39 ]  . 
gerade fr diese multimodalen konzepte sind randomisierte studien dringend erforderlich . die iort des pankreaskarzinoms erfordert eine sorgfltige properative bestrahlungsplanung sowohl fr den einsatz eines optimalen tubusses als auch der elektronenenergie . 
 [ 6 ] anhand der planungsunterlagen , der ct , der operationsund histologieberichte retrospektiv zeigen , dass in 53% der flle das zielvolumen zu klein und in 60% der flle die elektronenenergie zu niedrig gewhlt worden war . 
die einzeitdosis sollte deshalb in kombination mit einer perkutanen radiotherapie 10 bis 15 gy nicht berschreiten [ 39 ]  . zusammenfassend deuten diese daten darauf hin , dass mit einem iort - boost von 10 bis 15 gy zustzlich zu einer neoadjuvanten kombinierten radiochemotherapie oder vor einer adjuvanten radiochemotherapie die lokale kontrollrate signifikant erhht werden kann . 
zur weiteren evaluierung ist jedoch die durchfhrung randomisierter prospektiver multicenterstudien notwendig , um die mglichen vorteile bei hherem aufwand und nebenwirkungspotential objektiv zu definieren . tersucht [ 2 , 26 , 29 ]  . 
derzeit sind nur daten aus phase - ioder phase - ii - studien publiziert , der einsatz auerhalb klinisch kontrollierter studien als kombinierte radiochemotherapie beim pankreaskarzinom ist deshalb nicht indiziert . erste ergebnisse bei patienten mit inoperablem pankreaskarzinom zeigen , dass bei einmaliger wchentlicher gabe von 200 bis 400 mg / m2 gemcitabine parallel zu einer einzeldosis von 1 , 8 gy bis zu einer gesamtdosis von 50 , 4 gy die mtd mit 400 mg / m2 noch nicht erreicht wurde . 
diese phase - i - studie wird derzeit mit 60 mg / m2 fortgesetzt [ 2 ]  . bei paralleler gabe zu 3 gy einzeldosis ( gesamtdosis 30 gy ) ist jedoch wegen der verstrkten akutreaktion vorsicht angebracht . 
 [ 38 ] an 16 patienten mit inoperablem pankreaskarzinom mit 400 mg / m2 gemcitabine ( insgesamt sieben wchentliche gaben ) trat die akuttoxizitt typischerweise erst nach ende der radiotherapie whrend der dritten und vierten woche auf . 
zwei monate nach therapie zeigten 4 / 16 patienten eine partielle remission und zehn eine stabile erkrankung [ 38 ]  . die ersten ergebnisse der kombinierten radiochemotherapie mit 30 bis 50 mg / m2 paclitaxel und 1 , 8 gy einzeldosis bis 50 , 4 gy sind ebenfalls ermutigend . 
bei 13 patienten wurden in der ct vier partielle remissionen ( 31% ) beobachtet [ 26 ]  . neuere chemotherapeutische substanzen aufgrund der schlechten prognose werden neue substanzen wie die taxane und gemcitabine intensiv auf ihre wirksamkeit auch beim nicht metastasierten pankreaskarzinom undie beschriebenen remissionsraten mit bis zu 30% bei beiden substanzen bei allerdings sehr kleinen fallzahlen mit akzeptabler toxizitt zeigen das mgliche potential dieser therapie . 
therapy for locally unresectable pancreatic carcinoma : a randomized comparison of high dose ( 6000 rads ) radiation alone , moderate dose radiatiobn ( 4000 rads and 5 - fluorouracil ) , and high dose radiation + 5 - fluorouracil . 
ein beispiel susanne richter1 , michael flentje2 , jrgen richter2 ziel : untersuchung einer fr anlagen mit asymmetrisch einstellbaren blenden vorteilhaften bestrahlungstechnik mit einer kombination von kraniokaudal aneinander grenzenden feldern und feldern ber die gesamte zielvolumenlnge hinsichtlich des feldanschlusses sowie der schonung von normalgewebe und risikoorganen . 
an example aim : a treatment technique favorable for linacs with asymmetric jaws , which combines cranio - caudal matching fields with fields enclosing the whole target volume , is investigated with respect to field matching and sparing of normal tissue and organs at risk . 
 results : in the region of the matching line the summation of the measured normalized curves resulted in relative dose maxima of 6.0% ( caudal ) and 4.5% ( cranial ) , respectively . 
for fields enclosing the whole target volume the dose maxima in the region of the matching line decreased to 2.0% ( caudal ) and 1.8% ( cranial ) , respectively . 
the 5 - field technique with adjoining fields results in a better sparing of the organs at risk compared to the other techniques , whereas the tumor control remains the same . 
 key words : three - dimensional treatment planning treatment techniques asymmetric jaws field matching dosevolume histogram complication probability 1klinik fr strahlentherapie , georg - august - universitt gttingen , 2klinik fr strahlentherapie , julius - maximilians - universitt wrzburg . eingang des manuskripts : 25 . 
es wurde eine fnf - felder - technik mit individuellen blcken sowie keilen geplant , wobei sich zwei felder ( gantry 0 bzw . 307 ) ber die gesamte zielvolumenlnge erstreckten . 
die felder ber die gesamte zielvolumenlnge lieferten je rund ein drittel der dosis zum referenzdosispunkt ( isozentrum ) , das gewicht der drei asymmetrisch ausgelenkten felder wurde jeweils individuell angepasst und manuell optimiert . 
fr die risikoorgane blase und darm ( ohne zielvolumen ) wurden die normalgewebekomplikationswahrscheinlichkeiten ( ntcp ) und fr das zielvolumen die tumorkontrollwahrscheinlichkeiten ( tcp ) fr die einzelnen techniken verglichen . 
in the middle the isocenter plane is presented , in the right a plane 4 cm cranial and in the left picture a plane 5 cm caudal to the isocenter plane are shown . ergebnisse feldanschlussproblematik zur untersuchung des feldanschlusses der gemessenen bzw . 
die dosisberhhung ( cid : 2 ) d im bereich des feldanschlusses wurde als abweichung des maximums dmax vom mittelwert der dosen dl ( links ) und dr ( rechts ) in jeweils 0.05 cm abstand von dmax definiert , das heit , ( cid : 2 ) d = dmax ( dl + dr ) 1 wie aus abbildung 3 ersichtlich ist , zeigt sich fr das im helax tms erstellte addierte dosisprofil keine merkliche dosisberhhung . 
4 , 5% ( kranial ) , in die auch die mechanische positionierungsungenauigkeit der blenden eingeht . zur weiteren untersuchung wurden die dosisprofile der kraniokaudal aneinander grenzenden felder mit den vom helax - tms - system berechneten dosisbeitrgen der einzelnen felder zum referenzdosispunkt ( im isozentrum ) multipliziert und anschlieend addiert . 
 die messung der dosisprofile erfolgte nur auf der achse durch das isozentrum , senkrecht zur isozentrumsebene . durch die variation des gantry - winkels und die divergenz der felder verndert sich der feldanschluss jedoch auerhalb dieser achse . 
auerdem liegen die positionierungsungenauigkeiten der blenden bei 1 mm und die lagerungsungenauigkeit des patienten sowie die organbewegungen im bereich von mindestens 2 mm und fhren damit zu einer reduktion der berbzw . 
 technikvergleich der vergleich der dosis - volumen - histogramme fr die organe blase und darm zeigt eine deutlich bessere schonung durch diesen individuellen plan im vergleich zur individuellen vier - felder - box bzw . 
describes the distribution of values in a patient group , n0 is the tumor cell density . der vergleich der normalgewebekomplikationswahrscheinlichkeiten des individuellen fnf - felder - plans mit der vier - felder - box bzw . 
 diskussion die hier vorgestellte technik bietet im vergleich zu konventionellen techniken ( vier - felder - box , gegenfelder ) eine organ modell 4 - felderntcp [ % ] gegenfelder 5 - felderplan darm ( ohne zv ) blase lyman kutcher lyman kutcher 5 , 38 6 , 47 27 , 92 30 , 28 0 , 05 0 , 02 2 , 95 3 , 67 tabelle 2 . 
trotz der signifikanten unterschiede in den dosis - volumen - histogrammen ergeben sich keine komplikationswahrscheinlichkeiten fr die blase , da die toleranzdosis mit 65 gy immer noch sehr hoch ist . 
although there are significant differences in the dose - volume histograms no complication probabilities occur for the bladder because the tolerance dose value of 65 gy is still very high . 
for the normal tissue ntcp values could not be calculated because of a lack of knowledge of parameter values . tcp [ % ] 4 - feldergegenfelder 5 - felderplan zielvolumen poisson 97 , 42 webb / nahum 74 , 53 96 , 88 73 , 47 97 , 89 75 , 81 tabelle 3 . 
im modell webb / nahum werden die von patient zu patient variierenden - werte durch den parameter bercksichtigt , die zu einer verbreiterung der dosis - wirkungs - beziehung und somit zu einer verringerung der tcp fhren . 
tumor control probabilities for the planning target volume . in the model webb / nahum the values varying from patient to patient are taken into consideration by resulting in a broadening of the dose effect curve and hence in a decrease of tcp . 
durch die aufteilung eines feldes in mehrere abschnitte hat man zustzliche freiheitsgrade zur optimierung der dosisverteilung zum beispiel knnen die felder zum ausgleich unterschiedlicher gewebetiefen oder streubeitrge unterschiedlich gewichtet werden , keile lassen sich nach bedarf variieren . 
je grer der abstand der anschlussebene zur isozentrumsebene , je breiter die felder und je grer der winkel zwischen den feldern , desto grer ist das gebiet , in dem dosisinhomogenitten auftreten knnen . 
in der routine wird eine feinjustierung der blenden vorgenommen , sodass diese eine berlappung von 1 mm aufweisen . mit phantommessungen und filmdosimetrischen methoden konnten die autoren keine wesentlichen beroder unterdosierungen im feldanschlussbereich feststellen . 
des weiteren weisen sie darauf hin , dass auch intensittsmodulierte techniken mit einer vielzahl von kleinen feldern in einer homogenen zielvolumenerfassung resultieren und dass die vorgestellte technik weitaus akkurater ist als die konventionelle art der feldanpassung mit verschiedenen isozentren . 
 abschlieend kann festgestellt werden , dass eine technik mit aneinander grenzenden individuell gewichteten feldern hinsichtlich besserer schonung des normalgewebes zu empfehlen ist , vor allem wenn zustzliche felder ber die gesamte zielvolumenlnge verwendung finden [ 11 ]  . 
the tumor is regarded as low - grade sarcoma by some authors ; its cause and pathogenesis are presently unknown . patient and method : this is a case report on a 27 - year - old man who underwent 4 surgical procedures of the left lower extremity because of a recurrent soft tissue neoplasm , initially ( august 1993 ) diagnosed as a myxolipoma . 
a palliative resection with macroscopic residuals left was performed in february 1998 , followed by a radiation therapy with 56 gy total dose and a concomitant administration of the radiosensitizer razoxane per os . the single radiation doses were 200 cgy 5 times a week . results : the small residuals of the tumor obviously regressed although an objective response could not be shown because the lesion was not clearly measurable . 
a follow - up 2 years after the radiation treatment revealed no recurrence . the time of the local control achieved as yet is already longer than any former time to regrowth between the surgical procedures . 
this is , to our knowlegde , the first description of a therapeutic irradiation of a recurrent aggressive angiomyxoma . conclusion : radiation therapy combined with the sensitizer razoxane is able to control a recurrent aam for an unknown time . 
it remains open whether a radiation treatment alone would have had a similar effect . key words : aggressive angiomyxoma radiotherapy razoxane combined modality therapy soft tissue neoplasm das aggressive angiomyxom : bestrahlung bei rezidiv hintergrund : das aggressive angiomyxom ( aam ) ist ein 1983 erstmals beschriebener weichteiltumor , der vorwiegend in der beckenund genitalregion auftritt und eine starke neigung zur lokalen rezidivierung hat . 
der tumor wird von einigen autoren als low - grade - sarkom eingestuft , seine entstehungsursache ist unbekannt . patient und methode : ein 27 - jhriger mann wurde unter der ursprnglichen diagnose eines myxolipoms viermal am linken unterschenkel radikal operiert . 
der r2 - resezierte rezidivtumor wurde mit einzeldosen von 200 cgy fnfmal pro woche bis zu einer gesamtdosis von 56 gy unter peroraler gabe von razoxan bestrahlt . ergebnis : die residuen des tumors gingen mutmalich zurck , eine objektivierung des rckgangs war jedoch wegen mangelnder messbarkeit des tumors nicht mglich . 
die dauer der bisher erreichten lokalen kontrolle ist lnger als die der intervalle , die zwischen den frheren operationen und den jeweils folgenden rezidiven lagen ( 18 , 19 , 17 monate )  . 
dies ist die erste beschreibung einer therapeutischen bestrahlung eines rezidivierten aggressiven angiomyxoms . schlussfolgerung : eine strahlenbehandlung mit peroraler gabe von razoxan scheint imstande zu sein , ein r2 - reseziertes rezidiv eines aam lokal auf unbestimmte zeit zu kontrollieren . 
aggressive angiomyxoma a ggressive angiomyxoma ( aam ) is a distinctive , locally aggressive , fibromyxoid tumor of the pelvic and genital soft tissues , first described by rosai et al . 
a loss of an x chromosome in 8 of 20 metaphase cells analyzed were described in another case [ 10 ]  . since aam lack metastatic potential [ 1 ] , adjunctive radiotherapy has obviously rarely been considered . 
we report on a male patient with extensive aggressive angiomyxoma of the left lower extremity who received a full course of radiation therapy because of repeated recurrences . case report history a 27 - year - old male patient underwent 3 seemingly radical excisions and an r - 2 resection of a presumable myxolipoma of the left lower leg in august 1993 , february 1995 , september 1996 and finally in february 1998 . 
the history was otherwise not remarkable . in view of the repeated recurrences , the histology was reevaluated in 1998 and the diagnosis changed to aam . pathology macroscopically , the lesions were found to be composed of yellowish - gray nodular tissue with a gelatinous consistence . microscopically , the he staining showed a gray myxoid matrix with few bland - looking scattered stellate cells and occasionally some fibroblast - like cells . 
in areas without a prominent vascular picture , myxolipoma might erroneously have been diagnosed most frequently ( figure 2 )  . clinical findings the patient was first seen at our department of plastic surgery in february 1995 with a firm subcutaneous tumor in the medial aspect of his left lower leg . 
the patient developed a third recurrence under the scar just proximal of the medial malleolus which grew so big that in february 1998 a further excision of the tumor together with a scar revision had to be performed . 
between march 17 and april 27 , 1998 , large parts of the left lower limb were irradiated with 6 - mev photons using single doses of 200 cgy 5 times a week . 
concomitantly to the radiotherapy , the radiosensitizer razoxane was administered in twice daily doses of 125 mg per mouth , starting 5 days before the first irradiation . a skin necrosis developed in the radiation field in september 1998 . 
in may 1999 , a mrt revealed an increased , sharply demarcated t1signalling in the subcutaneous tissue in a size of about 3 to 1 cthere was no palpable correlation to this finding ; its significance is unclear . 
the stromal cells of this tumor were found to stain consistently for vimentin but not for the s - 100 protevariable results were reported as to the staining for muscle - specific actin or desmin [ 3 , 4 , 19 ]  . 
in establishing the diagnosis , other myxoid tumors like myxoid neurofibroma , angio - myofibroma or liposarcoma have to be ruled out . the location of the reported tumor is rather unusual . 
because of the presumable sarcomatous nature of such a lesion , these authors from the mayo clinic were the first to use preoperative and intraoperative radiotherapy in one case to prevent local recurrence [ 14 ]  . 
despite the short follow - up , the time of tumor control is already longer than the previous intervals to the recurrences . mesenchymal tumors are more difficult to be determined as to their dignity , grading or infiltrating borders in comparison to carcinomas . 
in the present case , however , primarily the repeated consideration of clinical signs and the natural history of the disease led to a reevaluation and change of the former diagnosis of a recurrent lipomyxoma . 
immunohistochemical studies of aam have shown differing results in the razoxane was added to the radiation treatment for 3 reasons : the drug potentiates radiation effects in experimental tumors [ 6 ] , and it is able to normalize tumor blood vessels [ 11 ]  . 
further experiences with radiation therapy have to be awaited , before this question can be answered . strahlentherapie und onkologie urban & vogel 2000 originalarbeit variation in supraclavicular lymph node depth is partly determined by treatment position hartmut t . 
klages , frank szafinski , hans - bruno makoski1 background : the so - called supraclavicular region bears the confluence of deep jugular , upper mediastinal and axillary lymph node groups and therefore it is often part of the target volume in common malignancies like lung cancer , breast cancer and head and neck cancer . 
for treating this area , several authors recommend an anterior portal with the dose prescribed to a tissue depth of 3 cm , which does not fit our institutions experience . patients and methods : in 119 consecutive patients a computed tomography for planning purposes was performed . 
we used the subclavian blood vessels between clavicula and first rib as an estimate of the confluence of the mentioned lymph node regions and determined their tissue depth ( which does not describe the deepest part of the lymph vessels )  . results : mean and median of the tissue depth were 5 cm in a range from 2 to 9 conly in less than 20% of the measurements we found the vessels located 3 cm or less under the surface which would correspond to a depth of the lymph node target volume 4 to 5 c increasing body mass resulted in deeper location of the vessels . 
arms risen above the head resulted in 55% of the measurements in tissue depths of 6 cm or deeper compared to 6% in patients treated with arms beside the body . conclusion : standardized treatment prescriptions do not cope adequately with individual anatomy . 
patient immobilization is crucial for accuracy of treatment delivery . key words : radiotherapy planning supraclavicular lymph nodes breast cancer lung cancer head and neck cancer die tiefe der supraklavikulren lymphknoten wird zum teil durch die lagerung bei der behandlung bestimmt hintergrund : in der so genannten supraklavikularregion findet sich der zusammenfluss der tief zervikalen , oberen mediastinalen und zentral axillren lymphwege ; daher gehrt sie oft zum zielvolumen hufiger tumorerkrankungen wie bronchial - , mammaund kopf - hals - karzinomen . 
viele empfehlungen zur bestrahlung dieser region verschreiben ein anteriores stehfeld mit dosierung auf 3 cm gewebetiefe , was nicht den erfahrungen unserer institution entspricht . patienten und methoden : bei 119 konsekutiven patienten wurde eine computertomographie zur planung durchgefhrt . 
als schtzung des zusammenflusses der genannten lymphknotenregionen dienten uns die subklaviagefe zwischen klavikula und erster rippe , deren gewebetiefe bestimmt wurde ( die damit nicht den oberflchenfernsten teil des lymphgefareals beschreibt , abbildung 1 )  . ergebnisse : arithmetisches mittel und median der gewebetiefe betrugen 5 cm bei einem gemessenen wertebereich von 2 bis 9 cnur weniger als 20% aller messungen fanden eine geftiefe von 3 cm oder weniger , die zu einer zielvolumentiefe von 4 bis 5 cm fhren wrde . 
bei armhaltung ber dem kopf resultierten 55% aller messungen in einer gewebetiefe von 6 cm oder mehr , verglichen mit 6% bei armhaltung neben dem krper ( abbildung 2 )  . schlussfolgerung : pauschale empfehlungen zur dosierungstiefe der genannten lymphknoten werden der individuellen anatomie nicht gerecht . 
variation in supraclavicular lymph node depth r adiation therapy for the so - called supraclavicular region is commonly employed in patients with the most frequent malignancies in western societies : lung cancer , breast cancer and cancer of the head and neck . 
depending on the primary tumor , radiation therapy aims at different lymph node groups : in lung cancer at the upper mediastinal lymph nodes and the apex of the lung , in head and neck cancer at the lower jugular lymph nodes and in breast cancer at the central axillary or infraclavicular lymph nodes . 
even the guidelines for treating breast cancer , recently issued by the german society of radiooncology ( degro ) , describe this technique as appropriate although it is not primarily advised [ 18 ]  . 
these recommendations are not in accordance with the daily experience in our institution . the shortcomings of standardized field arrangements for treatment of lymphatic regions have previously been discussed in this journal , like for inguinal radiotherapy in vulvar carcinoma [ 1 ] , for paraaortal treatment in seminoma [ 20 ] , and for infradiaphragmatic irradiation in non hodgkin lymphoma [ 10 ]  . 
similarly , we wanted to record the average lymph node depth in the supraclavicular fossa . patients and methods we chose the subclavian vessels as an estimate of the confluence of central axillary , deep jugular and upper mediastinal lymph nodes . 
eighty - three of the patients had both arms above their heads , 34 patients had their arms beside the body , 1 patient different positions of her arms . seventy subjects were female , 49 male , which reflects the great portion of patients with female breast cancer . 
in 76 of the patients we recorded both height ( median 168 cm , range 153 to 189 cm ) and weight ( median 71 kg , range 44 to 104 kg ) and computed their body mass as the percentage of optimal body weight [ 13 ] ( median 109% , range 75 to 167% )  . results the median and mean depth of the subclavian vessels between clavicula and first rib was 5 cm with a range between 2 and 9 cm and a standard deviation of 1.6 conly in 40 of the 238 measurements ( 19.7% ) in 119 patients we found a tissue depth of the vessels of 3 cm or less ( figure 2 ) which would result in a target volume depth of 4 to 5 cwe recorded only minor differences between left and right side ( pearsons correlation coefficient was .92 [ 3 ] )  . two determinants of the tissue depth were identified . 
in the 76 subjects in which body height and weight had been recorded table 1 gives an impression of increasing tissue depth of the vessels with increasing body mass of the patients expressed in terms of optimal body weight . 
the pearsons correlation coefficient is .63 : the greater the body mass of the patient , the deeper the location of the subclavian vessels . the position of the patients arms is even more important . 
if the patients arms are moved above her or his head , more soft tissues like subcutaneous fat and thoracic muscles are located between the surface and the subclavian vessels . 
figure 3 demonstrates the different tissue depth distributions of the vessels for arms risen above the head ( 167 measurements ) or positioned near the body ( 71 measurements )  . figure 1a abbildung 1a figure 1b abbildung 1b figures 1a and 1b . 
hufigkeitsverteilung der beobachteten gewebetiefe der subclaviagefe . discussion the above quoted recommendations for conventional radiotherapy planning of the supraand infraclavicular fossa fail to cover the lymphatic vessels surrounding the subclavian artery and vein in the majority of patients . 
variation in supraclavicular lymph node depth therefore , an individual target volume delineation by computed tomography seems to be more adequate with regard to the supraclavicular nodes than a standardized portal prescription [ 2 , 6 , 1719 ]  . 
we cannot rely on a volume model and a computed isodose distribution if we cannot rely on the patients position . conclusion treatment position and patient immobilization , especially of the arms , influence the location of the supraclavicular lymph node region in treatment of the chest and the head and neck . 
 strahlentherapie und onkologie urban & vogel 2000 originalarbeit intermittent use of amifostine during postoperative radiochemotherapy and acute toxicity in rectal cancer patients jrgen dunst , susanne semlin , steffi pigorsch , arndt - christian mller , thomas reese1 purpose : amifostine has been shown to be able to reduce acute radiation toxicity if administered daily prior to radiation during a course of a conventionally fractionated radiotherapy . 
5 - fu chemotherapy was administered as 120 - hours continuous infusion in the first and fifth radiation week via a central venous catheter in a daily dosage of 1 000 mg / m2 . 
side effects of amifostine were mild and included hypotension ( 53% grade i , 7% grade ii ) and nausea ( 47% grade i , 13% grade ii )  . 
 conclusions : in this phase - ii study , amifostine significantly reduced acute skin and bowel toxicity of adjuvant chemoradiation in patients with rectal cancer even if the drug was administered only intermittently and not during the whole course of radiotherapy . 
 key words : rectal cancer radiotherapy amifostine radioprotection acute toxicity intermittierende gabe von amifostin bei postoperativer radiochemotherapie und akute toxizitt bei rektumkarzinompatienten hintergrund : amifostin ist in den letzten jahren in mehreren phase - ii / iii - studien als radioprotektor eingesetzt worden . 
amifostine postoperatively in rectal cancer folgte nach den empfehlungen der deutschen krebsgesellschaft ( 28 fraktionen grovolumig mit 1 , 8 gy in drei - feldertechnik , drei fraktionen boost auf sakrum und prsakralregion , zwei kurse 5 - fu mit 1000 mg / m2 pro tag als 120stunden - dauerinfusion in woche 1 und 5 )  . 
amifostin wurde nur an den chemotherapietagen ( tage 1 bis 5 und 29 bis 33 ) in einer dosis von jeweils 500 mg direkt vor der tglichen bestrahlungsfraktion intravens appliziert . 
whrend des studienzeitraums wurden weitere 15 patienten mit rektumkarzinom , die die einschlusskriterien erfllten , aber an der studie nicht teilnehmen wollten , mit einer identischen radiochemotherapie ohne amifostin behandelt ; diese dienten als nicht randomisierte kontrollgruppe . 
die toxizitt von amifostin war mild ( hypotension grad i in 53% und grad ii in 7% , nausea grad i in 47% und grad ii in 13% )  . 
 schlussfolgerungen : in dieser phase - ii - studie ergeben sich hinweise fr eine mgliche klinische effektivitt von amifostin auch bei intermittierender gabe whrend einer radiochemotherapie bei patienten mit rektumkarzino schlsselwrter : rektumkarzinom radiotherapie amifostin radioprotektion akute nebenwirkungen a mifostine is a thiol derivative and has been shown to have radioprotective properties in animal experiments ( for review see [ 5 , 15 , 16 ] )  . 
in a second randomized study , amifostine reduced the frequency and severity of esophagitis and pneumonitis in patients treated with definitive radiotherapy for non - small - cell lung cancer [ 2 ]  . 
amifostine may also be associated with mild to moderate side effects ( mild emesis , hypotension )  . these side effects , even if mild , result in discomfort for the patients especially if they occur regularly over a period of several weeks . 
another approach is to use amifostine only during a part of the radiation treatment where the risk of side effects is higher . in our investigation we have used amifostine only intermittently during 2 weeks of a 6 - week schedule of postoperative chemoradiation in rectal cancer patients . 
the mean age was 58 years ( range 41 to 72 years )  . all patients were offered to participate in an open phase - ii study using intermittent amifostine during 2 weeks of the 6week radiotherapy treatment and agreed to treatment according to the protocol . 
fifteen additional patients who were treated during the same period received the identical radiochemotherapy treatment but they had refused to participate and received no amifostine ; this group served as non - randomized control group . 
fifteen patients had no lymph node involvement ( pn0 ) , 11 were classified as pn1 and 4 as pn2 . the distribution of patients characteristics in both groups is given in table 1 . 
amifostine postoperatively in rectal cancer treatment protocol and amifostine administration the adjuvant treatment consisted of locoregional radiotherapy plus 6 courses of 5 - fu chemotherapy ( 1 week 5 - fu , 3 weeks breaks )  . 
ct planning was used in all cases . 5 - fu chemotherapy was administered as 120 - hours continuous infusion in the first and fifth radiation week ( days 1 to 5 and 29 to 33 ) via a central venous catheter in a daily dosage of 1000 mg / m2 . 
 amifostine ( ethyol , essex , germany ) was given on days with radiation and chemotherapy treatment ( days 1 to 5 and 29 to 33 ) immediately prior to the daily radiation fraction as short infusion over 5 to 10 minutes in a daily dose of 500 mg . this dose was chosen with regard to the results of a dosefinding study and a phase - iii study of amifostine combined with pelvic radiotherapy [ 6 , 7 ]  . 
toxicity scoring included radiation - induced bowel toxicity ( enteritis ) , skin toxicity ( erythema ) in the radiation fields , 5 - fu - associated oral mucositis , nausea and emesis , hematological toxicity and changes in blood pressure . 
acute toxicity was recorded once weekly according to the ctc criteria and the maximum toxicity during the preceding week of treatment was recorded . statistical methods for comparison of acute toxicity , the individual patients scores were used . 
this peak was not observed in patients with amifostine ( figure 2 )  . 5 - fu - related mucositis was more pronounced in patients without amifostine as compared to the amifostine group ( 3 / 15 vs 1 / 15 patients with grade - ii and 6 / 15 vs 3 / 15 patients with grade - i mucositis )  . 
nevertheless , the difference in the nausea scores in weeks 1 and 5 ( weeks with amifostine administration ) were significantly higher in patients with amifostine as compared to patients without amifostine . 
no late radiation - related complications have occurred until now . discussion the radioprotective properties of amifostine and its ability to reduce radiation - induced normal tissue reactions have been demonstrated in animal studies and also in some recent clinical phase - ii / iii studies [ 2 , 4 , 1013 ]  . 
bolus injections seem also feasible [ 14 ]  . the objective of our study was to evaluate whether or not amifostine may also be effective if the drug is administered only intermittently during a 6 - week course of radiochemotherapy and not during the entire radiation treatment . 
the overall toxicity of adjuvant radiochemotherapy is small . most of recent treatment series with routine ct - treatment planning , sparing of normal tissue by individual collimation and the use of a belly board have reported low rates of side effects in patients with adjuvant treatment of rectal cancer . the overall toxicity in our patients was , as expected , mild even without amifostine . 
nevertheless , our study , although not randomized , shows a lower frequency of radiation - related acute side effects in patients treated with additional amifostine and suggests that amifostine may be effective in this subgroup of patients even if used only during a part of the treatment course . 
it should be noted that the daily dose of amifostine in this investigation was higher than in other studies where the drug was administered daily over 5 to 7 weeks ( 500 mg which corresponds to about 300 mg / m2 in this study as compared to 200 mg / m2 in most other studies )  . 
moreover , the use of amifostine at the time of concurrent radiochemotherapy is theoretically reasonable because acute toxicity , especially bowel toxicity , is more pronounced during this treatment phase . 
an impact of amifostine on 5 - fu - related mucositis was also not demonstrated , although there was a trend towards reduced mucositis . the follow - up in this study is too short with regard to late radiation sequelae . 
however , 2 recent randomized studies which both have demonstrated a beneficial effect of amifostine on acute toxicity have shown identical locoregional failure rates after amifostine as compared to patients without amifostine so that a negative effect of amifostine on local tumor control is unlikely [ 2 , 10 ]  . the question whether amifostine is surely able to reduce acute mucositis and enteritis is controversially discussed in the literature . 
if one assumes that amifostine is comparable to a dose reduction of about 20% a beneficial effect can only be expected if the administered radiation dose lies about 10 to 20% above the tolerance dose of the organ . 
if , on the other hand , the administered radiation dose largely exceeds the tolerance level of an organ , a significant effect of amifostine is unlikely to be observed because the moderate dose - modifying effect of the drug is not sufficient for reducing the side effects below the threshold . 
we have chosen patients with rectal cancer for our investigation because the risk of side effects in this group of patients is low and acute radiation toxicity ( mainly bowel toxicity ) can often be managed by short treatment breaks or transient moderate dose reductions . 
the comparison of patients given additional amifostine with a non - randomized control group suggests a beneficial effect of amifostine on radiation - related skin and bowel toxicity even if the drug is administered only intermittently . 
seven of the 8 patients who suffered from hepatic failure had poor pretreatment liver functions . conclusion : radiotherapy with or without transarterial embolization and / or percutaneous ethanol injection appears effective in controlling hepatocellular carcinoma and prolonged survival . 
individualized treatment strategies are presented depending on the tumor presentation and the degree of liver function impairment . key words : hepatocellular carcinoma radiotherapy liver function bestrahlung hepatozellulrer karzinome hintergrund : retrospektive evaluierung der wirksamkeit einer bestrahlung mit oder ohne transarterielle embolisation oder perkutaner alkoholinjektion bei patienten mit inoperablem hepatozellulren karzinom . patienten und methodik : von oktober 1984 bis november 1997 wurden 62 patienten mit einer gesamtdosis von 50 bis 70 gy in 25 bis 35 fraktionen mit oder ohne transarterielle embolisation oder perkutane alkoholinjektion behandelt . der mediane follow - up betrug 8 , 6 monate ( 1 , 5 bis 92 monate )  . ergebnisse : das mediane gesamtberleben betrug 9 , 5 monate . 
sieben der acht patienten , die ein leberversagen erlitten , hatten eine schlechte prtherapeutische leberfunktion . schlussfolgerung : die bestrahlung mit oder ohne transarterielle embolisation und / oder perkutane alkoholinjektion scheint bei der behandlung des hepatozellulren karzinoms wirksam zu sein und verlngert das berleben . 
individualisierte behandlungsstrategien , abhngig von der tumorprsentation und dem ausma der leberfunktionseinschrnkung , werden vorgestellt . schlsselwrter : hepatozellulres karzinom bestrahlung leberfunktion h epatocellular carcinoma , the 3rd cause of cancer death for men and 6th for women in japan [ 7 ] , originates mainly in the cirrhotic liver generally found in patients with long - term b or c hepatitis [ 20 ]  . 
it is characterized by a high incidence of intrahepatic metastasis and / or multifocal carcinogenesis as imaging studies often fail to disclose tumor extension and / or lesions , only to be discovered during laparotomy . the best outcome has been achieved in patients whose tumors were surgically resected [ 9 ]  . 
two other modalities , transarterial embolization ( tae ) and percutaneous ethanol injection ( pei ) , are used for smaller tumors , but not effective in the presence of extracapsular extension or portal vein tumor thrombosis ( pvtt ) [ 8 , 19 ]  . 
the latter underwent transarterial embolization and / or percutaneous ethanol injection before and / or after radiotherapy to control tumors located outside the radiation fields , and 2 patients received percutaneous ethanol injection for tumors located inside the radiation fields . 
radiotherapy in combination with or without transarterial embolization was used for bulky tumors , and transarterial embolization and / or percutaneous ethanol injection alone were used for small metastases outside the radiation field . radiotherapy was carried out using either a 6to 20 - mv microtron or a 6 - mev linear accelerator . 
a few patients whose diaphragmatic movements exceeded 3 cm as measured by a simulator were treated with the linear accelerator equipped with a respiratory gating systethis system was designed to overcome the hepatic movement due to respiration by regulating the linear accelerator to release radiation only in expiratory phases . 
however , there was a substantial shift of the positioning marker on the abdomen by the belt itself , therefore , the majority of patients were treated with microtron without the respiratory gating system . the treatment volume included the tumor itself and / or the tumor thrombus with a 1or 2 - cm margin longitudinally and number of patients childs classification field size tumor numbers treatment strategy total 100 cm2 < 100 cm2 solitary 2 or more with tae with pei table 1 . 
relatively large tumors were treated through parallel opposing fields at various angles , whereas small tumors were treated either by parallel opposing portals or 2 rectangular portals , or in some cases , stereotactic or conformal radiotherapy with minimal doses to non - cancerous parts of the liver . stereotactic radiotherapy techniques for hepatocellular carcinoma previously described elsewhere [ 21 ] , was given to only 1 patient whose hepatic movement was reduced within 1 cm by lying in the ventral position . 
in patients with more pronounced respiratory tumor movements , conformal radiotherapy is preferred over stereotactic radiotherapy as the former allows the moving tumor volume in the longitudinal directions is irradiated without a geographical miss while minimizing involvement of normal tissue irradiation at any other directions . the patients received doses from 50 to 70 gy in 25 to 35 fractions in 5 to 7 weeks , however , in 4 patients who presented with massive tumors encompassing the entire right lobe in addition to having poor liver functions a total dose of 30 gy was given in 15 fractions over 3 weeks through parallel opposing fields . diagnosis of hepatocellular carcinoma for those who did not undergo surgery was made solely by imaging studies which have been reported to be very accurate [ 18 ]  . patients were retrospectively grouped according to the childs classification for pretreatment liver functions to evaluate the influence of pretreatment liver function on survival [ 6 ]  . 
for evaluation of the afp value it was considered elevated if it exceeded 100 ng / ml , reduced or markedly reduced if it declined to less than 50 or 10% of the original value , respectively . 
a multivariate analysis for prognostic factors included the pretreatment liver function , number of tumors , age , sex , pretreatment afp value , field size , and the presence of extrahepatic metastases and / or portal vein tumor thrombosis . results overall median survival rates of all 62 patients were 9.5 months ( figure 1 ) , and 12 patients survived more than 2 years from the beginning of radiotherapy . 
in 49 patients followed by ct or ultrasound studies , 6 - month , 1 - year and 2year actuarial local control rates in the irradiated regions were 67 , 54 and 36% , respectively . 
fr die 29 patienten im child - a - stadium zeigten sich signifikant lngere berlebensraten im vergleich zu den 33 patienten mit child - boder child - c - stadium . patients tolerated treatment well but most patients experienced transient general fatigue during radiotherapy which disappeared within 1 to 2 weeks after the completion of treatment . 
there were 6 out of 62 patients whose serum concentrations of liver enzymes ( got : glutamate oxaloacetate transaminase ; gpt : glutamate pyruvate transaminase ) doubled when compared to the values taken before radiotherapy . 
ct studies revealed regeneration of the unirradiated liver in all 4 patients ( figure 2 ) who were irradiated through a field size larger than 100 cm2 , and in only 1 out of 8 patients who were treated through a field size smaller than 100 cm2 . 
afp values , measured every 1 to 2 months following radiotherapy , were reduced in 18 out of 35 patients who had presented with initially elevated values , and 11 of those showed a marked reduction . 
the median survival for those 11 patients was 16.7 months , significantly longer than 6.3 months for the remaining 24 patients . figure 2a abbildung 2a figure 2b abbildung 2b figure 2 . 
ein 54 - jhriger mann mit einem groen und mehreren kleinen manifestationen eines hepatozellulren karzinoms wurde mittels transarterieller embolisation mit nachfolgender bestrahlung behandelt : auf die groe tumormanifestation wurden 50 gy in 25 fraktionen verabreicht . 
prognostische faktoren fr das gesamtberleben . significant prognostic factors associated with survival were childs pretreatment staging [ 4 ] , radiation field size and the existence of tumor thrombus ( table 2 )  . 
prognostic factors for patients with childs a stage were the existence of tumor thrombus , whereas those for patients with childs b and c stages were radiation field size and the number of tumors present , respectively . discussion considering uncertainties regarding radiotherapeutic response of sometimes bulky tumors , limited abilities of current imaging technologies to detect tumor extension , and postradiotherapy liver functions of the non - cancerous but often diseased liver , a question arises as if there has been any benefit in treating these patients with radiotherapy in the first place . 
thus , radiotherapy with or without transarterial embolization and / or percutaneous ethanol injection improved overall survival rates considerably when compared to those who received no treatment . in our series most patients had relatively large tumors associated with intrahepatic metastases , and bulky tumors were individually irradiated . 
whole liver irradiation was , however , not employed as it has been reported ineffective in controlling hepatocellular carcinoma because of its poor tolerance [ 16 ] , and in an attempt to prevent further functional exacerbation of the diseased liver . 
concerning the dose - response of bulky tumors , our results have shown that 1 - year local control rate was 67% for those who had received doses exceeding 50 gy , and that 36% of the tumors treated remained under local control over 2 years . 
thus , doses in the range of 50 to 70 gy were apparently effective in some patients , however , others have found in 7 autopsied cases that the doses in this range are not adequate to eradicate hepatocellular carcinoma [ 1 ]  . 
there has been a theory that the doses in this range are appropriate as radiotherapy inflicts not only direct cytocidal effect but also fibrotic vascular occlusion which may eliminate nourishment to the tumor , facilitating an improved tumor control [ 5 , 11 ]  . as high radiation doses are required for local control as our preliminary results indicate , high - dose localized radiotherapy such as stereotactic or conformal radiotherapy may offer a better chance for local control while sparing the non - cancerous liver from excess doses of radiation . 
in 17 hepatocellular carcinoma lesions in 14 patients , all lesions were under control for a median observation period of 11 months ( 2 to 25 months )  . only 1 patient with 3 lesions had experienced temporary gpt elevation , but other patients had no significant acute adverse effects [ 17 ]  . 
a better gating system to overcome respiratory hepatic movements is important as it will allow lower probabilities of geographical miss and lower doses to the non - cancerous liver . evaluation of pretherapy liver functions is essential in the management of patients with hepatocellular carcinoma . 
a 15 - minute icg ( indocyanine green ) dye retention rate level has been reported to have a predictive value for hepatic failure after hepatectomy [ 14 , 22 ]  . 
in 6 patients with childs b or c stage who suffered from radiation hepatitis in our series , 4 had radiation fields larger than 100 cm2 , and 1 patient underwent conformal radiotherapy . 
this process was detected by ct in all 4 patients who underwent radiotherapy through a field size larger than 100 cm2 , but only in 1 of the 8 patients who were irradiated through a field size smaller than 100 cm2 . 
the doses used for large - field radiotherapy in our series appeared to have damaged the liver to the extent that it promoted regeneration , suggesting that the doses used represent the maximal tolerance level for the diseased liver . our current policy in the management of surgically ineligible patients with hepatocellular carcinoma is based on childs classification on pretherapeutic liver function , the tumor size and numbers . 
because of a tendency to develop intrahepatic metastases or multifocal carcinogenesis during a course of these patients , repeated treatments are frequently required , and this must be taken into account when planning a treatment for the first time . 
smaller tumors outside the radiation field and / or residual tumors after radiotherapy may be treated by transarterial embolization and / or percutaneous ethanol injection which is effective for tumors smaller 3 cm in size [ 8 ] our present guide lines are as follows : 1 . 
wittekind * ( leipzig ) * kooperierende mitglieder 1 deutsche gesellschaft fr radioonkologie ( degro ) und arbeitsgemeinschaft radiologische onkologie ( aro ) , strahlenklinik akh hagen 2 deutsche gesellschaft fr urologie ( dgu ) und arbeitsgemeinschaft urologische onkologie ( auo ) , klinik fr urologie im universittsklinikum essen 3 arbeitsgemeinschaft internistische onkologie ( aio ) , zentrum fr innere medizin iv der martin - luther - universitt hallewittenberg 4 klinik fr urologie der rheinischen friedrich - wilhelmsuniversitt bonn 5 zentrum innere medizin des klinikums der philipps - universitt marburg 6 abteilung fr innere medizin ii der eberhard - karls - universitt tbingen 7 abteilung fr strahlentherapie der eberhard - karls - universitt tbingen 8 urologische abteilung , albertinen - krankenhaus hamburg 9 urologische abteilung des bundeswehrkrankenhauses hamburg 10 urologische klinik der philipps - universitt marburg 11 urologische klinik des kaiser - franz - josef - spitals wien 12 klinik fr urologie der westflischen wilhelms - universitt mnster 13 urologische klinik des klinikums der stadt mannheim 14 klinik fr urologie der medizinischen hochschule hannover 15 klinik fr strahlentherapie und radioonkologie der georgaugust - universitt gttingen 16 urologische abteilung des krankenhauses am urban berlin 17 urologische klinik des klinikums schwerin 18 institut fr pathologie der universitt leipzig 19 abteilung fr strahlentherapie der eberhard - karls - universitt tbingen eingang des manuskripts : 23 . 
interdisziplinrer konsensus zur diagnostik und therapie von hodentumoren hintergrund : 1996 war von der interdisziplinren arbeitsgruppe hodentumoren ( iah ) , in der vertreter aller an der diagnostik und therapie des germinalen hodentumors beteiligten disziplinen aus den jeweiligen fachgesellschaften und arbeitsgruppen der deutschen krebsgesellschaft zusammenarbeiten , ein interdisziplinrer konsensus zur diagnostik und therapie von hodentumoren erarbeitet worden ( strahlenther onkol 1997 ; 173 : 397406 )  . 
hierfr sind durch den 1998 erfolgten zusammenschluss der iah mit der organgruppe hodentumoren der arbeitsgemeinschaft urologische onkologie ( auo ) zur german testicular cancer study group ( gtcsg ) die wissenschaftliche basis erweitert und die qualitt der erarbeiteten diagnostischen und therapeutischen standards fr hodentumoren erhht worden mit der zielsetzung , eine breite umsetzung der interdisziplinr erstellten empfehlungen zu ermglichen . 
 methodik : in erweiterung der erarbeitung des konsensus von 1996 erfolgte die berarbeitung auf grundlage aktueller literaturdaten in anlehnung an die prinzipien der evidence - based medicine ( ebm )  . 
das methodische vorgehen entsprach dabei dem der cochrane collaboration , deren bewertungskriterien bernommen wurden . ergebnisse : der zu 21 themenkomplexen anhand wissenschaftlich begrndeter entscheidungskriterien erarbeitete interdisziplinre update - konsensus przisiert und definiert diagnostische und therapeutische standards entsprechend dem aktuellen wissensstand ber diese tumorentitt . 
 schlsselwrter : testikulre keimzelltumoren evidenzbasierte medizin ( ebm ) interdisziplinre diagnostikund therapieempfehlungen interdisciplinary consensus on diagnosis and treatment of testicular germ cell tumors : results of an update conference based on evidence - based medicine ( ebm ) background : an interdisciplinary consensus statement on the diagnosis and therapy of testicular tumors was prepared in 1996 by the interdisciplinary testicular tumor working group ( iah ) with input from representatives from diagnostic and therapeutic disciplines of various working groups of the german cancer society ( strahlenther onkol 1997 ; 173 : 397406 )  . 
in 1998 the iah met again together with the testicular tumor working party of the urooncology working group ( auo ) and formed the german testicular cancer study group ( gtcsg )  . 
 methods : according to the principles of evidence - based medicine ( ebm ) , the consensus from 1996 was modified , based on the current level of evidence from the published literature . 
the methodological process and evaluation criteria used were that of the cochrane collaboration . results : an interdisciplinary update consensus statement summarizes and defines the diagnostic and therapeutic standards according to the current scientific practices in testicular cancer . 
 this interdisciplinary update consensus was presented at the 24th national congress of the german cancer society on march 21st and subsequently evaluated and approved by the various german scientific medical societies . 
 key words : testicular germ cell tumors evidence - based medicine ( ebm ) interdisciplinary diagnostic and treatment strategies einleitung 1996 wurde von der interdisziplinren arbeitsgruppe hodentumoren ( iah ) , in der vertreter an der behandlung von hodentumoren beteiligter arbeitsgruppen der deutschen krebsgesellschaft ( aio , auo , aro ) zusammenarbeiten , ein interdisziplinrer konsensus zur diagnostik und therapie von hodentumoren erarbeitet und publiziert [ 1 , 2 ]  . 
die beteiligung aller wissenschaftlichen fachgesellschaften , die mit der klinik von hodentumoren befasst sind , sollte dabei die wissenschaftliche basis erweitern , die qualitt der von der gruppe erarbeiteten diagnostischen und therapeutischen standards fr hodentumoren erhhen und eine breite umsetzung der interdisziplinr erarbeiteten empfehlungen zur diagnostik und therapie ermglichen [ 3 , 4 ]  . aufgrund von in der zwischenzeit erarbeiteten nderungen der therapeutischen standards wurde es notwendig , den konsensus von 1996 zu aktualisieren . 
interdisziplinrer konsensus zur diagnostik und therapie von hodentumoren len literatur wissenschaftlich begrndete hilfestellungen fr rztliche entscheidungsprozesse zu formulieren , dadurch die versorgungsergebnisse zu verbessern , die behandlungsrisiken zu minimieren und somit eine qualitativ hoch stehende , auch im internationalen vergleich bestehende medizinische versorgung von patienten mit hodentumoren in deutschland zu gewhrleisten . unter beachtung gesundheitskonomischer forderungen der bundesrztekammer und der kassenrztlichen bundesvereinigung und in bereinstimmung mit den bemhungen der deutschen krebsgesellschaft um qualittssicherung in der onkologie wurde die berarbeitung des konsensus von 1996 in erweiterung des vorgehens bei der erarbeitung des ersten konsensus nach den prinzipien der evidenzbasierten medizin ( ebm ) in einem mehrstufigen prozess vorgenommen [ 37 ]  . 
die erarbeiteten ergebnisse wurden in anlehnung an die kriterien der evidence - based medicine ( ebm ) und somit nach der sicherheit ihrer aussagen bewertet . hierbei wurden gte und validitt der in den jeweiligen publikationen enthaltenen daten hierarchisch entsprechend ihren zugrunde liegenden evidenztypen unterschiedlichen evidenzstufen zugeordnet [ 6 ] ( tabelle 1 )  . 
deutschen krebskongress vorgestellt und nachfolgend von den daran beteiligten wissenschaftlichen fachgesellschaften ( arbeitskreis onkologie der deutschen gesellschaft fr urologie [ ako der dgu ] , der deutschen gesellschaft fr hmatologie und onkologie [ dgho ] und der deutschen gesellschaft fr radioonkologie [ degro ] ) geprft und gebilligt . 
hierarchy of scientific evidence ( declining from stage ia to iv ) according to cochrane collaboration [ 6 ]  . nem drittel der flle besteht gleichzeitig eine testikulre intraepitheliale neoplasie . 
bei unaufflligen tumormarkerwerten kann eine diagnosesicherung durch biopsie aus dem tumorprozess erfolgen oder unter der verdachtsdiagnose eines extragonadalen keimzelltumors das ansprechen auf die chemotherapie beobachtet und das weitere vorgehen festgelegt werden . 
fr die beurteilung der gewebeentnahmen ist es erforderlich , dass pro zentimeter tumor eine scheibe ( block ) , jedoch mindestens drei insgesamt , sowie blcke aus der unmittelbaren tumorumgebung und aus dem tumorfernen hodengewebe histologisch untersucht werden . 
weitere entnahmen mssen aus dem samenstrangabsetzungsrand und aus einem hodennahen ( 1 cm abstand ) querschnitt vom samenstrang erfolgen . die tumoren werden entsprechend der who - klassifikation [ 44 ] klassifiziert . bei den immunhistologischen untersuchungen sollten folgende antikrper verwendet werden : gegen zytokeratin ( erkennung von nicht seminomatsen strukturen ) , plap ( erkennung einer testikulren intraepithelialen neoplasie ) und cd31 / faktor viii ( darstellung von gefendothelien )  . das histopathologische gutachten , das nach den richtlinien der basisdokumentation fr tumorkranke [ 45 ] erstellt werden sollte , muss folgende angaben enthalten : tumorlokalisation [ 46 ] und - gre , seitenangabe , hodendystopie , tumorausbreitung ( rete testis , tunica albuginea , tunica vaginalis , nebenhoden , samenstrang , skrotum ) , blutund lymphgefinvasion , pt - kategorie ( uicc [ 47 ] ) , histologischer typ ( who - icd - 0 ) , intratubulre keimzellneoplasie ( tin )  . bei pluriform strukturierten tumoren sind fakultativ die nachgewiesenen strukturen und ihr geschtzter prozentualer anteil , bei seminomen der nachweis von synzytiotrophoblasten , bei spermatozytischen seminomen eine zustzliche sarkomkomponente anzugeben . 
 der morphologische nachweis einer testikulren intraepithelialen neoplasie erfolgt lichtmikroskopisch am he - prparat mit immunhistologischem nachweis der plap oder im semidnnschnitt ( bei entsprechender erfahrung )  . ausbreitungsdiagnostik die nachfolgenden angaben zur wertigkeit der jeweiligen bildgebenden diagnostikverfahren beruhen in der regel nicht auf prospektiven phase - iii - studien , sodass eine ebm - graduierung im einzelnen nicht vorgenommen werden kann ; allerdings ist die validitt der angaben dem ebm - grad iia ( analog der genauigkeit von phase - iii - studien ) gleichzusetzen , da das ergebnis der bildgebung in der regel mit der histopathologischen diagnose korreliert wird [ 48 , 49 ]  . 
unter einhaltung der richtlinien der bundesrztekammer zum gerteund untersuchungsstandard [ 5658 ] werden fr das spiral - ct des thorax und der leber die parameter 5 / 8 / 4 mm ( kollimation / tischvorschub / inkrement ) , fr die des brigen abdomens die parameter 8 / 10 / 8 mm empfohlen . fr die beurteilung der lunge und des mediastinums ist die computertomographie sensitiver im vergleich zur rntgenuntersuchung des thorax . 
es muss allerdings beachtet werden , dass pulmonale / pleurale knotige vernderungen < 1 cm zu falsch positiven bewertungen fhren knnen [ 52 , 54 , 55 , 59 , 60 ]  . auch mit einer computertomographie des abdomens / beckens ist die differenzierung der klinischen stadien i und iia nur begrenzt mglich aufgrund falsch positiver bzw . falsch negativer befunde von bis zu 30% wegen schwieriger differenzierung der lymphknotendignitt aufgrund morphologischer grenbestimmung [ 5153 , 6163 ]  . 
eine mrt des abdomens / beckens hingegen bringt keinen zustzlichen diagnostischen gewinn und ist daher nur bei kontraindikation gegen die intravense applikation von rntgenkontrastmitteln ( ct - untersuchung ) einzusetzen [ 6567 ]  . 
die pet - untersuchung fhrt zu falsch negativen befunden bei differenzierten teratomen , falsch positiven bei entzndlichen reaktionen und kann mikrometastasen nicht nachweisen ; sie ist daher auf studien beschrnkt [ 6876 ]  . 
patienten mit fortgeschrittener erkrankung sind darber hinaus den prognosegruppen nach den kriterien der igcccg zuzuordnen : gute , intermedire und schlechte prognose ( siehe tabelle 2 ) [ 77 , 81 ]  . 
da die tumorentwicklung aus der testikulren intraepithelialen neoplasie meist verzgert abluft , ist bei patienten mit kinderwunsch eine abwartende strategie gerechtfertigt , vorausgesetzt , es bestehen eine ( zur assistierten konzeption ausreichende ) restspermiogenese und die bereitschaft des patienten zu regelmigen kontrolluntersuchungen . die definitive therapie hngt von der gesamtsituation des patienten ab . 
liegt eine testikulre intraepitheliale neoplasie gute prognose nichtseminom testis / primrer retroperitonealer tumor und niedrige marker und keine nicht pulmonalen viszeralen metastasen seminom jede primrlokalisation , jede markerhhe und keine nicht pulmonalen viszeralen metastasen intermedire prognose nichtseminom testis / primrer retroperitonealer tumor und intermedire marker und keine nicht pulmonalen viszeralen metastasen seminom jede primrlokalisation , jede markerhhe und nicht pulmonale viszerale metastasen ( leber , zentralnervensystem , skelett , intestinum ) berlebensrate > 90% niedrige marker : afp < 1 000 ng / ml , ( cid : 2 ) - hcg < 1 000 ng / ml ( < 5 000 iu / l ) und ldh < 1 , 5 ( cid : 2 ) normalwert berlebensrate > 75% intermedire marker : afp 1 000 - 10 000 ng / ml oder ( cid : 2 ) - hcg 1 00010 000 ng / ml ( 5 00050 000 iu / l ) oder ldh 1 , 510 ( cid : 2 ) normalwert schlechte prognose nichtseminom primrer mediastinaler keimzelltumor oder hohe marker : afp > 10 000 ng / ml , berlebensrate < 50% testis / retroperitonealer tumor mit nicht pulmonalen viszeralen metastasen ( leber , ldh > 10 ( cid : 2 ) normalwert zentralnervensystem , skelett , instestinum ) oder hohem marker ( cid : 2 ) - hcg > 10 000 ng / ml ( 50 000 u / l ) oder tabelle 2 . 
eine ablatio testis ist sinnvoll , wenn ein gesunder kontralateraler hoden vorhanden ist und eine bestrahlungsbehandlung der testikulren intraepithelialen neoplasie den gesunden hoden gefhrdet ( streustrahlung ) oder eventuell auch bei prtherapeutisch bereits stark atrophischem hoden . 
sie sollte nur in individuellen fllen ( resektion sonstiger herde im krper mglich , teratomhaltige primrhistologie , zystische vernderung des hirntumors in der bildgebung und operationstechnisch gnstige lokalisation ) erfolgen . mit der intermediate - prognosis - gruppe in der igcccgklassifikation wurde eine gruppe von patienten definiert , die eine fnf - jahres - berlebensrate von etwa 80% erreicht . fr diese patienten gibt es keine abgeschlossenen prospektiven studien . 
unter prognostischen aspekten ist zwischen einer primren hirnmetastasierung mit einer langfristigen berlebenswahrscheinlichkeit von etwa 30 bis 40% ( kurative indikation ) und einer unter therapie oder im rezidiv auftretenden filialisierung mit einer fnf - jahres - berlebenswahrscheinlichkeit von etwa 2 bis 5% zu unterscheiden . 
aus diesem grund ist die behandlung dieser patienten an zentren und innerhalb von studien dringend erforderlich . nichtseminom die standardtherapie fr die salvagebehandlung besteht in der gabe von pei / vip bzw . 
die tumormarker mssen unter bercksichtigung der halbwertszeiten ( afp fnf bis sieben tage , ( cid : 2 ) - hcg 24 bis 36 stunden , ldh 24 stunden ) nach orchiektomie kontrolliert werden , wenn sie primr erhht waren . 
individuelle faktoren knnen ein von diesen empfehlungen abweichendes vorgehen notwendig machen , da nur der mindesterforderliche rahmen dargestellt werden kann . die nachsorge besteht aus standarduntersuchung , tumormarkerbestimmungen und bildgebender diagnostik . 
die intervalle sind einheitlich fr alle stadien , histologien und therapiemodalitten im ersten und zweiten jahr alle drei , im dritten jahr alle vier , im vierten und fnften jahr alle sechs monate , danach jhrlich durchzufhren ( tabelle 4 )  . 
die positronenemissionstomographie mit ( 18f ) - 2 - fluoro - 2 - deoxy - d - glukose ( 18fdg - pet ) bei der diagnostik retroperitonealer lymphknotenmetastasen von hodentumoren . 
importance of bleomycin in combination chemotherapy for good - prognosis testicular nonseminoma : a randomized study of the european organization for research and treatment of cancer genitourinary tract cancer cooperative group . 
randomized trial of bleomycin , etoposide , and cisplatin compared with bleomycin , etoposide , and carboplatin in good - prognosis metastatic nonseminomatous germ cell cancer : a multiinstitutional medical research council / european organization for research and treatment of cancer trial . 
european organization for research and treatment of cancer , genito - urinary group , and the medical research council testicular cancer working party , cambridge , united kingdo j clin oncol 1998 ; 16 : 71624 . 
four cycles of bep vs four cycles of vip in patients with intermediate - prognosis metastatic testicular nonseminoma : a randomized study of the eortc genitourinary tract cancer cooperative group . 
randomized comparison of cisplatin and etoposide and either bleomycin or ifosfamide in treatment of advanced disseminated germ cell tumors : an eastern cooperative oncology group , southwest oncology group , and cancer and leukemia group b study . 
does necrosis on frozen - section analysis of a mass after chemotherapy justify a limited retroperitoneal resection in patients with advanced testis cancer ? br j urol 1997 ; 80 : 6537 . 
intensive induction - sequential chemotherapy with bop / vip - b compared with treatment with bep / ep for poor prognosis metastatic germ cell tumor : a randomized medical research council / european organization for research and treatment of cancer study . 
the feasibility of daily ct - based 3d treatment planning is studied in a patient with localized prostate carcinoma using a new patient positioning syste methods : daily ct planning was applied during boost irradiation of a patient with prostate cancer : after patient immobilization the pelvis was scanned in 3 mm ct slices . 
the shift of the single markers from ct scan to ct scan was more extensive than those of the center of all 7 markers combined ( 47% of the deviations were smaller than 3 mm )  . 
the new patient positioning system exactrac is an interesting tool especially for daily ct planning since conventional simulation can be omitted . key words : daily ct 3d treatment planning patient positioning system radiation therapy tgliche ct - planung whrend der boostbestrahlung bei prostatakarzinodurchfhrbarkeit und zeitaufwand hintergrund : bei der bestrahlung der prostata kommt es aufgrund der organbewegung zu unsicherheiten bei der tglichen lokalisation des klinischen zielvolumens . 
mit hilfe der tglichen ct - planung kann die organbewegung zu einem gewissen grad kompensiert werden , sodass die sicherheitsabstnde verkleinert werden knnen und eine reduktion der normalgewebsbelastung erreicht wird . 
die durchfhrbarkeit der tglichen ct - gesttzten dreidimensionalen bestrahlungsplanung unter anwendung eines neuen positionierungssystems wird an einem patienten vorgestellt . methoden : die tgliche ct - planung wurde bei einem patienten mit prostatakarzinom whrend der boostbestrahlung angewandt . 
die prostata wurde in allen schichten konturiert , und die sicherheitsabstnde der micromultileafs wurden automatisch in den vom planenden arzt gewnschten abstand gesetzt ( 0 , 8 cm )  . 
das neue patientenpositionierungssystem exactrac ist eine interessante alternative zur konventionellen lagerung , insbesondere bei der tglichen ctplanung , da die konventionelle simulation entfllt . schlsselwrter : tgliche ct - planung dreidimensionale bestrahlungsplanung patientenpositionierungssystem strahlentherapie t he feasibility of daily ct - based 3d treatment planning was studied in a patient with localized prostate carcinoma . 
using this procedure uncertainties in the irradiation of the prostate due to internal organ shift mainly caused by filling variations of the bladder and the rectum [ 15 ] should be minimized . 
 patient and methods a 74 - year - old patient with localized prostate cancer was treated with conformal radiotherapy via a 4 - field box technique ( ap , pa , lat - lat ) to a dose of 50 gy in 2 - gy fractions ( prostate and seminal vesicles )  . 
the boost was applied via 4 non - coplanar fields ( gantry angles 70 , 100 , 260 , and 290 , table angles 350 , 0 , 0 , 10 ) using a brainlab m3 micromultileaf collimator with a leaf width of 0.3 cm in the isocenter . 
 planning and treatment procedures for boost irradiation were as follows : after the patient was immobilized in a vacuum bed on the ct couch 7 radioopaque body markers with an infrared reflectable surface coat were attached to the patients skin ventral to the pelvis . 
the clinical target volume ( prostate ) was contoured in each ct slice . the isocenter and the shape and size of the treatment portals were then defined using the brainscan planning system for stereotactic body irradiation . 
the safety margins of the leafs towards the clinical target volume were set automatically and the margin width was defined to be 0.8 cm ( this includes the safety margins from the clinical target volume to the planning target volume as well as the margins allowed to compensate for penumbra )  . 
the computer system calculates from the position of the markers the center of gravity of these markers ( marker isocenter ) and the position of the planned target point ( ptv target point ) relative to the marker center of gravity . the data were then transferred to computers that controlled the micromultileaf collimator and the patient positioning system exactrac . 
part of the positioning system are 2 wall mounted infrared stereo cameras in the treatment room which are capable to identify the body markers attached on the patients skthis setting enables the system to get information on the current patient position within the treatment room and since the body markers were scanned in the ct on the position of the ptv target point in relation to the body markers . 
the exactrac system is calibrated in the room coordinate syste that means that the position of each marker is determined in the room coordinate system . the calibration is performed by a special phantom which is placed in the isocenter of the treatment machine . 
after placing the patient in the vacuum bed on the treatment couch the deviation of the current patient position in relation to the linac isocenter is displayed in all 6 degrees of freedom ( craniocaudal , ventro - dorsal , lateral - lateral and rotation around the 3 axes )  . 
the treatment couch was then moved until the system indicated that the patient was in the right position with the ptv target point and the linac isocenter being at the same location . 
the patient position was corrected if the displacement in one direction was greater than 5 m the patient was then irradiated via the fields mentioned above and the leaf positions were documented by portal imaging . results after an initial learning period the overall time for planning and irradiation took about 1 hour 10 minutes . 
positioning accuracy was always better than 7 mm ( 3d shift ) as indicated by the verification images with 75% of the deviations not exceeding 3 mm in each direction . 
 the isocenter of this new configuration using the least square algorithsince 75% of the set - up deviations did not exceed 3 mm , this procedure seems to be reasonable . 
on the other hand the dislocation of a single marker is rather large with only 47% of the deviations being below 3 m since the more cranial located markers had a higher amplitude in movement due to breathing than those that were positioned further caudal we also observed a rotation of the patient around the coronal axis through the isocenter ( an axis that runs parallel to the treatment couch leading from left lateral to right lateral )  . 
 eral - lateral direction , 5 mm in the cranio - caudal direction and 0.75 mm in the ventro - dorsal direction ( the movement of the marker isocenter in the cranio - caudal direction is shown in figure 1 )  . 
this might have been caused by periodically occurring muscle spasms . to assess daily repositioning accuracy of a single marker image fusion of all ct scans was done on the basis of bony alignment ( pelvic ring ) using the brainscan image fusion software . 
with the aid of this software the ct data sets can be shifted and rotated in all directions until the deviation between the bony structures in the axial slices as well as in the reconstructed coronal and sagittal planes is minimal . 
after image fusion the deviations of the aligned bony structures were less than 2 m the position of all markers was outlined on the patients skin after their first placement . 
in each of the fused ct images the position of every single marker was recorded relative to a coordinate system which was attached to the rigid bony structures of the pelvis . 
the axes were adjusted to the skin surface : z - axis perpendicular to the skin surface , x - axis tangential to the skin surface leading from medial to lateral , y - axis extending in the sagittal plane from caudal to cranial . 
maximal marker movement ( expressed as the difference of the marker position of day 1 to 1 of the following days ) was 10 mm in one direction , 47% of the deviations did not exceed 3 mthe daily shift of one arbitrarily chosen marker is depicted in figure 2 . discussion the exactrac system proved to be easy to operate and patient positioning was done within a time frame that does not differ much from conventional patient positioning ( by means of skin marks and laser guidance )  . 
the disadvantages of the body - marker system are those of all skin - attached location systems : movement of the markers due to a shift of the skin and the underlying soft tissue as well as due to breathing and general muscle tension . 
to minimize the effect of a single marker movement 7 of the markers were attached to the patients skin ( instead of 3 that are theoretically sufficient to define a coordinate system on a rigid body )  . 
therefore very small deviations of the markers perpendicular to the treatment couch transform into calculated large deviations in the cranio - caudal direction of the patient . to minimize the displacement the markers should be attached as far caudal to the pelvis as possible . 
 another problem that might lead to deviations in patient positioning are uncertainties in data acquisition during the ct scans : due to breathing each ct slice represents a marker ( and organ - ) position in different states of inspiration or expiration . 
again the application of a higher number of markers should reduce these errors : the more markers are utilized the higher is the chance that the position of the single markers is recorded in different states of breathing thus minimizing the risk of a systematic marker shi one advantage of the exactrac positioning system is the fact that patient set - up is objectively monitored by the system and does not depend on the subjective estimation of the technician . 
in daily ct treatment planning the exactrac system has the advantage that after planning has been carried out no additional simulation is necessary to transpose the treatment portals and the isocenter on the patient skthus additional uncertainties are avoided and planning time is reduced . the advantage of daily ct planning with an imaging of the clinical target volume just before treatment may be a little reduced by the fact that organ shift might occur during the time between ct scan and irradiation . 
in 16% of 55 patients irradiated for prostate carcinoma they observed an ap prostate shift of more than 5 mm during an observation time of 7 minutes . the mean time of dislocation was 20 seconds . 
one means to reduce the ap prostate shift is the internal immobilization by a rectal balloon catheter [ 1 ]  . therefore , the combination of internal fixation by a rectal balloon catheter together with daily ct planning immediately prior to boost irradiation might allow careful dose escalation . 
a fast and easy to use patient positioning system which reduces planning time by sparing conventional simulation helps to implement daily ct planning in selected cases . strahlentherapie und onkologie urban & vogel 2000 originalarbeit effect of doxorubicin on cell survival and micronuclei formation in hela cells exposed to different doses of gamma - radiation ganesh chandra jagetia , vijayashree nayak1 purpose : the present study was undertaken to obtain an insight into the combined effects of doxorubicin with radiation on the cell survival and micronuclei induction in hela cells . material and methods : hela s3 cells were allowed to grow till they reached plateau phase , inoculated with 10 g / ml doxorubicin hydrochloride and then exposed to 0 , 0.5 , 1 , 2 and 3 gy - radiation . 
clonogenicity of cells was measured using the colony forming assay , micronuclei formation using the micronucleus assay . results : the treatment of hela cells with doxorubicin ( adriamycin ) for 2 hours before exposure to different doses of radiation resulted in a significant and dose - dependent decline in the cell survival and cell proliferation when compared to the pbs + irradiation group . 
the pretreatment of hela cells with doxorubicin before irradiation to various doses of - rays resulted in a significant elevation in the frequency of micronuclei when compared with the concurrent pbs + irradiation group . 
the correlation between cell survival and micronuclei induction was also determined for pbs or doxorubicin + irradiation group , where the clonogenicity of cells declined with the increase in micronuclei formation . 
the correlation between cell survival and micronuclei induction was linear quadratic for both pbs + irradiation and doxorubicin + irradiation groups . conclusion : from our study it can be concluded that combination treatment with doxorubicin and radiation increased the genotoxic effect of the either treatment given alone . key words : hela cells survival micronuclei doxorubicin cell proliferation radiation wirkung von doxorubicin auf das zellberleben und die mikronukleibildung in hela - zellen nach gamma - bestrahlung mit verschiedenen dosen hintergrund : der kombinierte effekt einer doxorubicingabe mit bestrahlung auf das zellberleben und die mikronukleiinduktion wurde an hela - zellen untersucht . material und methoden : hela - s3 - zellen in der plateauphase wurden mit 10 g / ml doxorubicinhydrochlorid inokuliert und dann einer - bestrahlung von 0 , 0 , 5 , 1 , 2 und 3 gy ausgesetzt . 
die klonogenitt der zellen wurde mit dem koloniebildungstest , die bildung von mikronuklei mit hilfe des mikronukleusassays untersucht . ergebnisse : die behandlung von hela - zellen mit doxorubicin fr zwei stunden vor einer - bestrahlung mit verschiedenen dosen resultierte in einer signifikanten und dosisabhngigen abnahme des zellberlebens und der zellproliferation im vergleich zu einer nur bestrahlten kontrollgruppe . 
die korrelation zwischen zellberleben und mikronukleusinduktion wurde ebenso fr die allein bestrahlte wie fr die mit doxorubicin und bestrahlung behandelte gruppe bestimmt ; die klonogenitt der zellen nahm dabei mit ansteigender mikronukleusformation ab . 
effect of doxorubicin in combination with radiation d oxorubicin ( adriamycin ) , an antibiotic having a wide spectrum of anti - neoplastic activity was isolated from the cultures of mutant fungus , streptomyces peucetius caesius . 
 in an attempt to increase the efficacy of single drug regimen , doxorubicin has also been used as an adjuvant to several other drugs in the treatment of breast cancer [ 17 ]  . 
 the use of cytotoxic chemotherapeutic drugs in conjunction with radiation for the treatment of difficult neoplasia no doubt has increased the survival of the patients receiving them , however , at the cost of development of second malignancies in the treated individuals [ 14 ]  . 
doxorubicin is a topoisomerase - ii inhibitor that exerts its cytotoxic effects by stabilizing the dna double strand breaks in the cellular genome [ 29 ] and combination of it with ionizing radiation may increase the mutagenesis and carcinogenesis more than either treatment given alone . 
 experimental design a fixed number ( 5 ( cid : 2 ) 105 ) of exponentially growing cells were inoculated into several individual culture flasks and were allowed to grow till they reached plateau phase . 
the plateau phase cell cultures were divided into 2 groups as follows : pbs + irradiation : the cells of this group were treated with 50 l of sterile phosphate buffered ( pbs ) saline before irradiation . 
 irradiation after 2 hours of pbs or drug treatment , the cells were exposed to 0 , 0.5 , 1 , 2 and 3 gy - radiation from a 60cobalt therapy source ( gammatron , siemens , germany ) at a dose rate of 1 gy / minute at a distance ( ssd ) of 54.5 c clonogenic assay clonogenicity of cells was measured using colony forming assay of puck et al . 
the cells from each group of flasks were dislodged by trypsin edta treatment . usually , 200 to 300 cells were plated on to culture dishes ( nunc , denmark ) containing 5 ml medium in triplicate for each radiation dose . 
the cells were allowed to grow for 11 days . the resultant colonies were stained with 1% crystal violet in methanol and clusters containing 50 or more cells were scored as a colony . 
the plating efficiency of cells was determined and the surviving fraction was fitted on to non - linear polynomial functions . micronucleus assay the cells remaining after the clonogenic assay were used for micronucleus assay , where 3 ( cid : 2 ) 106 cells were inoculated in triplicate for each dose of radiation for each group . 
the cells were left undisturbed and were allowed to grow for another 24 hours . thereafter , the medium containing cytochalasin - b was removed and cells were washed once with pbs . 
finally , cells were dislodged with trypsin edta treatment , centrifuged , subjected to mild hypotonic treatment ( 0.7% ammonium oxalate ) for 5 minutes at 37 c , centrifuged again and the resultant cell pellet was fixed in carnoys fixative ( 3 : 1 methanol , acetic acid )  . 
a minimum of 2 000 binucleate cells with well preserved cytoplasm were scored from each culture for the presence of micronuclei and a total of 6 000 cells per dose point were scored and the frequency of micronucleated binucleate cells ( mn ) was determined . 
the treatment of hela cells with 10 g / ml of doxorubicin before irradiation resulted in a significant decline in the cell survival and this decline was 1.4 - fold at all the exposure doses except 3 gy , where it was 1.3 - fold when compared with the concurrent pbs + irradiation group . 
the cell survival data of both the groups were fitted on various models , however , a best fit was obtained for the second order polynomial function ( figure 1 )  . although the pretreatment of hela cells with doxorubicin resulted in greater cell kill than the pbs + irradiation , the slope of the curve remained unchanged suggesting that the effect of drug treatment had an additive effect on the cell kill . micronuclei the frequency of mn increased in a dose - dependent manner in both pbs + irradiation and doxorubicin + irradiation groups ( figure 2 )  . 
however , the frequency of 4 mn was significantly higher in the doxorubicin + irradiation group after 0.5 to 3 gy except for 2 gy , where the increase was non - significant . the dose response relationship for both groups was linear for total mn and 1 mn , while it was linear quadratic for 2 , 3 , and 4 mn ( table 1 )  . proliferation index irradiation of hela cells caused a dose - dependent decline in the cell proliferation indices as evidenced by a steady decline in the frequency of binucleate cells followed by a simultaneous increase in the frequency of mononucleate cells in both pbs + irradiation and doxorubicin + irradiation groups . however , this decline was significantly higher in doxorubicin + irradiation group compared to pbs + irradiation group , except for 1 and 2 gy irradiation ( table 2 )  . the frequency of mononucleate cells was significantly higher in the doxorubicin + irradiation group compared to pbs + irradiation group except for 1 and 2 gy exposure . 
the frequency of trinucleate cells was significantly lower in doxorubicin + irradiation group in comparison with the pbs + irradiation group after exposure to 0 , 2 and 3 gy . 
 correlation between cell survival and micronuclei formation to ascertain the relationship between mn formation and cell survival , the surviving fraction was plotted on x - axis , while the mn were plotted on y - axis . 
obere kurve jeweils : doxorubicin + bestrahlung ; untere kurve : alleinige bestrahlung in pbs - puffer . exposure dose ( gy ) exposure dose ( gy ) exposure dose ( gy ) exposure dose ( gy ) jagetia gc , et al . 
effect of doxorubicin in combination with radiation exposure dose ( gy ) exposure dose ( gy ) exposure dose ( gy ) exposure dose ( gy ) exposure dose ( gy ) clined with the increase in mn induction in both pbs + irradiation and doxorubicin + irradiation groups ( figure 3 ) , indicating a close correlation between the clonogenicity of cells and mn formation . 
this decline was maximum for 0.5 gy ( 15% ) , while it was lesser ( 5% ) for the remaining doses when compared with the preceding dose of radiation . 
einfluss der doxorubicinbehandlung auf den proliferationsindex von hela - zellen nach - bestrahlung mit verschiedenen dosen . surviving fraction surviving fraction figure 3a abbildung 3a figure 3b abbildung 3b figures 3a to 3b . 
the survival curves of both groups were concave in nature and doxorubicin treatment did not change the slope of the curve , suggesting that the effect of doxorubicin treatment was additive . 
the cell killing effect of 3 gy irradiation in the irradiated control group was similar to the effect observed for doxorubicin + 0.5 gy irradiation , indicating that with doxorubicin treatment the radiation dose may be reduced to 1 / 6 to get the similar effect . 
recently , teniposide ( a topoisomerase - ii inhibitor ) and taxol ( an anti - cancer agent ) have been reported to enhance the cell killing effect of radiation in v79 cells [ 1 , 11 ]  . 
this decline in cell survival has been reflected in the cell proliferation indices , where the frequency of binucleate cells declined significantly in the doxorubicin + irradiation group compared to the pbs + irradiation group except 2 and 3 gy , where it was higher . 
this hypersensitivity at low doses may be due to changed expression of some genes only at low doses and not at high doses where some sort of radioresistance is developed [ 13 ]  . the increase in the mn frequency in doxorubicin + irradiation group was significantly higher compared to the pbs + irradiation group . 
this elevation in the radiation - induced mn formation by doxorubicin was dependent on the exposure dose and the lowest dose ( 0.5 gy ) gave the highest enhancement , where the mn frequency increased by a factor of 3.5. 
this may be due to an increase in the cell kill at higher doses in the doxorubicin + irradiation group when compared with the pbs + irradiation group . this is supported by the survival studies , where the surviving fraction of hela cells declined consistently with the increase in irradiation dose . 
teniposide , another topoisomerase - ii inhibitor has been reported to increase the frequency of radiation - induced mn in v79 cells [ 1 ] and mice [ 12 ]  . 
almost 31 and 39% cells contained 2 or more than 2 mn after 3 - gy exposure in pbs + irradiation and doxorubicin + irradiation groups and the surviving fractions were also the lowest , suggesting that there exists a quantitative relationship between micronuclei induction and cell survival . 
the pattern of micronuclei formation also indicates that doxorubicin pretreatment had an additive effect . with the increase in mn frequency , the cell survival declined , indicating an inverse relationship and the correlation between mn frequency and cell survival was linear quadratic . 
since the micronuclei formation represent loss of dna , as a consequence , the cells expressing more than 1 micronuclei may lose a sizeable amount of genetic material , resulting in the inhibition of cell proliferation and subsequent cell death . 
this contention is supported by the induction of a higher number of mn - bearing cells at higher exposure doses followed by a higher cell killing effect , indicating that there is a definite quantitative relation between mn formation and cell death . the hypersensitivity of low - dose exposure is also apparent for micronuclei formation , where 15 and 19% of the cells had 2 or more than 2 mn at 0.5 gy in the pbs + irradiation and doxorubicin + irradiation groups , respectively and it was higher than 1 gy exposure for both groups . doxorubicin is a topoisomerase - ii inhibitor and it intercalates with the cellular dna inducing single and double strand breaks of dna [ 29 ] , which may result in the enhancement of radiosensitivity of hela cells . 
the scission of dna is believed to be either by the inhibition of topoisomerase - ii [ 27 ] or by the generation of free radicals by doxorubicin [ 18 ] , which may be the reason for the increased cytotoxic effect after doxorubicin treatment . 
similarly , doxorubicin has also been reported to accumulate the cells in g2 + m phase of the cell cycle [ 25 ] , which may also increase the effect of radiation , as the cells that are in g2 + m phase of the cell cycle are most radiosensitive . 
further , doxorubicin has been reported to induce apoptosis in hela cells [ 25 ] that may also be responsible for the enhanced cell killing in doxorubicin + irradiation group . 
the changes in the fidelity of the genome of normal cells by combination treatment may lead to mutagenesis and clastogenesis , which may either be detrimental to the cell causing cell death or alternatively it may offer an advantage in the form of unrestricted proliferation resulting in the induction of neoplastic disorders . 
effect of doxorubicin in combination with radiation strahlentherapie und onkologie urban & vogel 2000 originalarbeit remission rates following preoperative chemotherapy and radiation therapy in patients with breast cancer brbel aryus1 , 4 , werner audretsch2 , frank gogolin3 , stefan gripp1 , theodor knigshausen3 , guido lammering1 , ralf rohn1 , karl axel hartmann1 purpose : to evaluate remission and breast - conservation rates after preoperative chemotherapy or chemo - radiotherapy ( ct - rt )  . patients and methods : seventy - three patients with 74 biopsy - proven invasive breast cancers prospectively entered the protocol . 
the median time interval between end of neoadjuvant therapy and surgery was 11 weeks ( range : 10 to 22 weeks ) and 27 weeks ( range : 11 to 41 weeks ) for the chemotherapyand chemo - radiotherapy group . 
the median time interval between end of chemotherapy and the beginning of irradiation ranged between 2 and 8 weeks ( median 4 weeks ) in the chemo - radiotherapy group . results : side - effects due to chemoor radiotherapy were moderate and reversible . 
in the chemotherapy group 17 / 18 patients ( 94% ) achieved a partial ( ppr ) and 1 / 18 patients ( 6% ) a complete histopathological response ( pcr )  . 
in 45 / 74 cases ( 61% ) the breast was preserved , immediate breast reconstructions with rectus myocutaneous flaps ( tram ) after mastectomy were performed in 8 / 74 cases ( 11% ) and modified radical mastectomies without reconstruction were required in 21 / 74 cases ( 28% )  . 
the breast conservation rates were similar in both treatment groups . conclusions : even though the small number of patients in the present protocol does not permit definite conclusions , the results of combined modality treatment seem promising with regard to tumor remission within the treated breast and as a tool for breast conservation in advanced stage disease . 
 key words : breast cancer neoadjuvant therapy radiotherapy breast reconstruction remissionsraten von mammakarzinomen nach neoadjuvanter chemound strahlentherapie fragestellung : es wurde untersucht , ob sich remissionsraten und die anzahl brusterhaltender therapien bei mammakarzinomen nach alleiniger neoadjuvanter chemotherapie oder kombinierter neoadjuvanter chemostrahlentherapie unterscheiden . patienten und methodik : 73 patientinnen mit 74 histologisch gesicherten invasiven mammakarzinomen wurden prospektiv in einem neoadjuvanten protokoll behandelt . 
eine antihormo1department of radiation oncology , university dsseldorf , germany , 2department of senology , and 3department of medicine , academic hospital dsseldorf gerresheim , germany , 4department of radiation oncology , academisch ziekenhuis vrije universiteit amsterdam , netherlands . 
das mediane zeitintervall zwischen abschluss der neoadjuvanten therapie und operation betrug elf wochen ( zehn bis 22 wochen ) bei der chemotherapieund 27 wochen ( elf bis 41 wochen ) bei der radiochemotherapiegruppe . 
das mediane zeitintervall zwischen beendigung der chemotherapie und beginn der strahlentherapie lag in der radiochemotherapiegruppe bei vier wochen ( zwei bis acht wochen )  . ergebnisse : nebenwirkungen im rahmen der chemooder strahlentherapie waren milde und reversibel . 
17 / 18 patientinnen ( 94% ) der chemotherapiegruppe wiesen eine partielle remission ( ppr ) und 1 / 18 patientinnen ( 6% ) eine komplette remission ( pcr ) auf . 
die rate an brusterhaltenden therapien ist in beiden behandlungsgruppen vergleichbar . schlussfolgerung : bei eingeschrnkter aussagekraft wegen der kleinen patientenzahl sind die ergebnisse des vorliegenden protokolls hinsichtlich der tumorremission nach kombinationsbehandlung vielversprechend . 
 schlsselwrter : mammakarzinom neoadjuvante therapie radiotherapie brustrekonstruktion s everal randomized clinical trials have shown that breast preserving surgery and subsequent radiotherapy is a safe treatment option for stage i and ii tumors with respect to local recurrence - free survival and overall survival [ 3 , 9 , 16 , 18 , 23 , 25 ]  . 
depending on the eligibility criteria for various induction chemotherapy protocols , breast preserving rates are higher than 80% in some series [ 4 , 15 , 20 , 24 ]  . 
 [ 22 ] demonstrated that induction chemotherapy followed by preoperative radiotherapy permits to select patients with locally advanced or stage ii breast cancer > 3 cm in diameter for conservative treatment . 
myocutaneous flaps can be used if the resulting defect after tumorectomy is considered too large for acceptable cosmesis [ 1 , 6 , 8 , 12 , 13 ]  . patients with planned flap - supported surgery are subjected to preoperative irradiation in order to avoid radiotherapy of the transplanted musculo - cutaneous tissue . 
our results of tumor remission and breast preservation rates after induction chemotherapy alone ( ct ) or followed by preoperative radiotherapy ( ct - rt ) are demonstrated in this report . 
other inclusion criteria were : non - metastatic tumors , < 75 years of age , largest tumor diameter > 3 cpatients with tumors < 3 cm were subjected to preoperative treatment when an initial breast - preserving approach was impossible due to e . 
overt metastatic disease was ruled out by physical examination , chest xray , blood chemistry , bone scan and liver sonography . myocutaneous flaps were indicated in patients with large tumors and / or unfavorable tumor - breast relation . 
this is reflected by the different initial tumor diameters of 3 and 7 cm for the chemotherapy and chemo - radiotherapy group , respectively ( table 1 )  . before treatment the original tumor site was marked by ink and documented by photographs . 
informed consent was obtained from all patients . systemic treatment different neoadjuvant chemotherapy regimens were used depending on performance status , co - morbidity , age and tumor factors such as c - erbb2 . 
cmf ( 600 mg / m2 cyclophosphamide , 40 mg / m2 methotrexate and 600 mg / m2 5 - fu ) and ec ( 90 mg / m2 epirubicin and 600 mg / m2 cyclophosphamide ) were administered in 3 - week intervals . preoperative radiotherapy for treatment planning a ct - simulator was used that allows patient positioning in the treatment set - up . 
the axillary lymphatic drainage was not irradiated even in case of macroscopic tumor infiltration , because most enlarged axillary lymph nodes responded to chemotherapy and all patients received a level i to ii axillary dissection after neoadjuvant treatment . surgery the median time interval between end of neoadjuvant therapy and surgery was 11 weeks ( range : 10 to 22 weeks ) and 27 weeks ( range : 11 to 41 weeks ) for the chemotherapyand chemo - radiotherapy group , respectively . 
in our experience wound complication preoperative antihormonal treatment ( % ) 5 ( 28 ) 33 ( 60 ) cmf ( n ) ec ( n ) other preoperative radiotherapy whole breast ( gy ) boost dose ( gy ) type of surgery tumorectomy ( n ) tumorectomy + lat ( n ) mrm ( n ) mrm - tram ( n ) tumor response 50 ( 4951 ) 10 ( 611 ) partial remission ( % ) complete remission ( % ) 17 ( 94 ) 1 ( 6 ) 32 ( 57 ) 24 ( 43 ) table 2 . 
therapieschemata und tumorresponseverhalten ( ct = chemotherapie ; ct - rt = radiochemotherapie )  . rates are not increased when acute radiation side - effects have subsided at the time of surgical intervention . 
patients with planned flap - supported surgery collected red blood cells for autotransfusion during the procedure . preoperative radiotherapy was chosen for most patients with planned flap - supported surgery to avoid irradiation of normal tissue ( table 2 )  . 
a minimum of 10 nodes was removed ( range 10 to 36 )  . results no toxic deaths were observed , and side - effects related to radiotherapy and chemotherapy were manageable , generally mild or moderate and reversible . 
of the 18 patients treated with chemotherapy alone 17 ( 94% ) had a partial ( ppr ) and 1 ( 6% ) had a complete histopathological response ( pcr )  . 
however , it has to be taken into consideration that the patient number is small and that there is an imbalance between the chemotherapyand chemo - radiotherapy groups with regard to sample size , tumor diameter and chemotherapy regimens . 
therefore , the present study does not allow definite conclusions but the combined modality treatment seems promising as a further tool for breast conservation in advanced stage disease . preoperative chemotherapy was introduced to make locally advanced tumors operable [ 14 ]  . 
studies comprising predominantly tumors < 5 cm report breast preservation rates exceeding 80% [ 2 , 4 , 25 ]  . in larger tumors , however , conservative procedures are less often possible [ 5 , 21 ]  . 
the relatively low breast preservation rate of 61% in our protocol can be attributed to the policy of resecting the tumor according to its pretreatment margins . as mentioned before , this policy resulted in a low rate of isolated locoregional recurrences [ 12 , 13 ]  . data on preoperative radiotherapy in combination with chemotherapy are scarce . 
 [ 7 ] applied a chemotherapy regimen of doxorubicin and cyclophosphamide followed by a homogeneous dose of 50 gy to the whole breast and a boost of 10 gy to the tumor . 
during this period , 33 patients with hormone - receptor positive tumors received antihormonal therapy and it can be hypothesized that the high proportion of complete responses is caused by this additional treatment . 
this difference is mainly caused by the additional radiation therapy , since tumors in the chemotherapy group were smaller and chemotherapy regimes were similar in both treatment groups . these results indicate that radiation therapy , as applied in this protocol , increases the proportion of complete histopathological responses in neoadjuvant breast cancer treatment . 
interestingly , only 1 of 11 patients with complete responses in a total of 434 patients treated in the nsabp - b - 18 trial relapsed within 5 years [ 10 ]  . 
 strahlentherapie und onkologie urban & vogel 2000 originalarbeit lebensalterspezifische ergebnisse der adjuvanten radiotherapie des mammakarzinoms jrgen schultze , egbert hft , bernhard kimmig1 fragestellung : es sollte untersucht werden , ob bliche qualittsstandards in der klinischen routinebehandlung auch bei lteren patienten konsequent eingehalten werden knnen und ob das alter die behandlungsergebnisse beeinflut . patienten und methodik : 218 mammakarzinompatientinnen wurden in den jahren 1990 und 1991 in unserer klinik bestrahlt . 
43 frauen waren jnger als 50 jahre ( gruppe i ) , 92 zwischen 50 und 64 jahren ( gruppe ii ) , 83 weitere lter als 64 jahre ( gruppe iii )  . 
44 patienten wurden zustzlich chemotherapiert . ergebnisse : die fnf - jahres - berlebensrate lag bei 79 , 8% ( n = 174 ) , tumorfrei berlebten 59 , 1% ( n = 129 )  . 
eine behandlung lterer menschen unterhalb des geltenden therapiestandards ist rztlich nicht zu vertreten . schlsselwrter : mammakarzinom strahlentherapie lebensalter age related results of adjuvant radiation therapy in breast cancer background : aim of our work was to evaluate the standards of treatment in elder women with breast cancer and their results of radiation therapy . patients and methods : in our hospital 218 breast cancer patients were treated in the years 1990 and 1991 . 
forty - three women were younger than 50 years of age ( group i ) , 92 between 50 and 64 years ( group ii ) , 83 elder than 64 years ( group iii )  . 
all of the patients were irradiated uniformly locoregionally with 50 gy co60 - photons , followed by a boost to the tumor bed with 10 gy with 6to 12 - mev electrons . 
forty - four patients had an additional chemotherapy . results : the 5 - year survival rate was 79.8% ( n = 174 ) , the disease free survival was 59.1% ( n = 129 ) ( table 6 )  . 
the mean rate of local recurrence was 3.6% ( n = 8 ) , 4% after mastectomy ( n = 6 ) and 3% ( n = 2 ) with breast conservation . age group specific 5 - year survival rates were 72% ( i ) , 85.6% ( ii ) and 77.1% ( iii ) , respectively , disease free survival rates were 48.8% ( i ) , 65.2% ( ii ) and 57.8% ( iii ) , respectively . 
schtzungsweise 46 000 neuerkrankungen treten jhrlich in deutschland auf [ 3 ]  . eine erhhte sensibilitt fr die erkrankungswahrscheinlichkeit sowie erheblich verbesserte diagnostische mittel haben dazu gefhrt , da das mammakarzinom frher diagnostiziert werden kann . 
in den tumorstadien t1 und t2 ermglicht die brusterhaltende therapie [ 9 ] in kombination mit der postoperativen radiotherapie gleich gute ergebnisse wie durch die mastektomie [ 28 ]  . 
grundstzlich findet die radiotherapie beim mammakarzinom anwendung als adjuvante radiotherapie nach brusterhaltender theraals adjuvante radiotherapie nach modifiziert radikaler zur definitiven behandlung des lokal fortgeschrittenen zur palliativbehandlung des metastasierten mammakarzipie , mastektomie , mammakarzinoms , noms . in abhngigkeit vom lebensalter wird die strahlenbehandlung dann gegebenenfalls kombiniert mit einer systemischen therapie , die entweder als polychemotherapie oder als hormontherapie erfolgt . ziel dieser untersuchung war die berprfung der behandlungsergebnisse bei patientinnen , die in den jahren 1990 bis 1991 in unserer klinik behandelt wurden . 
besonders interessierte dabei die frage , ob auch bei lteren patienten die blichen qualittsstandards eingehalten und ob bei adquater therapie gleich gute ergebnisse wie bei jngeren patientinnen erzielt werden knnen . 
zudem wollten wir untersuchen , welche der angewandten therapiearten die hchsten berlebensraten hatten und welche lokalrezidivraten auftraten . patienten und methode in den jahren 1990 und 1991 wurden 218 patientinnen wegen eines mammakarzinoms in unserer klinik radiotherapiert . es ergab sich die in den tabellen 1 und 2 dargestellte stadieneinteilung . chirurgische therapie eine mehrheit von 149 der 218 patientinnen war mastektomiert worden ( 68 , 3% )  . 
dieses heute mindestens umgekehrte verhltnis beruhte auf einer relativ spten einfhrung konsequent brusterhaltender operationstechniken durch die zuweisenden rzte in schleswig - holstein . eine axilladissektion erfolgte in 207 fllen ( 94 , 9% )  . 
lediglich bei sieben patientinnen wurde darauf verzichtet ( 3 , 2% )  . in vier fllen fand wegen primrer inoperabilitt in hherem tumorstadium keine operation statt . 14 patientinnen ( 6 , 4% ) entwickelten eine beidseitige tumorerkrankung . 
lediglich bei den patientinnen , die mit einer polychemotherapie behandelt wurden , wurde die radiotherapie erst drei bis vier monate postoperativ begonnen . die bestrahlungsplanung wurde am therapiesimulator ( sls 9 , firma philips ) unter zuhilfenahme eines therapieplanungscomputertomographen ( tomoscan cx , firma philips ) vorgenommen . 
 die brusterhaltend operierten patientinnen erhielten nach einem festen schema in der blichen fraktionierung von 1 , 8 bis 2 gy / tag innerhalb von sechs wochen eine gesamtdosis von 60 gy . 
weitere 10 gy wurden mit 6bis 12 - mev - elektronen als boost ber dem tumorbett appliziert . bei den mastektomierten patientinnen wurden damals die lokoregionren lymphabfluwege in axilla , supraklavikulargrube und parasternalregion smtlich mitbestrahlt . 
im bereich der narbenregion erfolgte eine zustzliche aufsttigung des tumorbettes mit weiteren 10 gy und 6bis 10 - mev - elektronen . die radiotherapie wurde ausschlielich mit kobalt - 60 - photonen durchgefhrt , da fr das kobaltgert ein speziell fr die mammatherapie konzipierter teilfeldblocker vorhanden war . 
lebensalterspezifische radiotherapie des mammakarzinoms die eine eigene tischkonstruktion mit lateraler armsttze am kobaltgert bereitstand . tumorstadium 13 patienten wurden lediglich bis 50 gy gesamtdosis bestrahlt ( 5 , 9% )  . adjuvante therapie eine polychemotherapie nach dem cmf - schema wurde bei 44 patientinnen durchgefhrt . 
fr 15 patientinnen lagen keine angaben ber die verordnung von tamoxifen vor . von den 115 patientinnen , die tamoxifen als adjuvans erhielten , hatten 77 positive und schwach positive strogenrezeptoren . 
bei 17 patientinnen lagen negative strogenrezeptoren vor , bei 21 patientinnen war eine rezeptorbestimmung nicht erfolgt . in den 85 fllen , bei denen kein tamoxifen eingesetzt wurde , fand sich jedoch bei 26 patientinnen ein positiver strogenrezeptor , bei sieben patientinnen ein schwach positiver und bei 30 patientinnen ein negativer rezeptor . 
in der jngeren gruppe waren 43 patientinnen , in der mittleren 92 und in der lteren 83 patientinnen . die gruppen wurden separat hinsichtlich der tumorstadien , der verabreichten therapie und des weiteren verlaufs untersucht . 
die nachbeobachtungszeit aller patienten betrug mindestens fnf jahre bis hchstens sieben jahre . altersverteilung bei erstdiagnose : die jngste patientin war 33 jahre alt , die lteste 87 jahre , der median lag bei 60 , 5 jahren . 
109 patientinnen waren lter als 60 jahre ( 50% ) , 83 patientinnen waren lter als 65 jahre ( 38 , 1% ) , 39 patientinnen waren lter als 70 jahre ( 17 , 9% ) , und 18 patientinnen waren lter als 75 jahre ( 8 , 3% )  . 
sechs patientinnen waren lter als 80 jahre ( 2 , 7% )  . die verteilung der tumorstadien in den altersgruppen , die durchgefhrte chirurgische primrtherapie , der nodalstatus sowie angaben zu systemischen therapien ergeben sich aus den tabellen 3 und 4 . ergebnisse gesamtberleben die fnf - jahres - berlebensrate betrug 79 , 8% ( n = 174 )  . 
verstorben waren insgesamt 44 patientinnen ( 20 , 2% ) , davon 32 an den folgen des tumorleidens und zwlf durch internistische grunderkrankungen oder andere ursachen . jngere gruppe ( n = 43 ) mittlere ltere gruppe gruppe ( n = 83 ) ( n = 92 ) gesamt ( n = 218 ) mastektomie brusterhaltung inoperabel systemisch : polychemotherapie ( n = 44 ) hormontherapie ( n = 115 ) tabelle 3 . 
age related tumor status and primary treatment . nodalstatus jngere mittlere ltere gruppe gruppe gruppe ( n = 83 ) ( n = 92 ) ( n = 43 ) gesamt ( n = 218 ) tabelle 4 . 
dieser beruht jedoch im wesentlichen auf dem gnstigeren primrstadium bei initialer therapie . von den 181 patientinnen mit t1und t2 - tumoren wurden 63 brusterhaltend operiert ( 34 , 8% ) , von den 34 patientinnen im stadium t3 und t4 wurde lediglich eine ( 2 , 9% ) brusterhaltend behandelt . 
in den stadien t1 und t2 berlebten 95 der ablativ operierten patientinnen ( 80 , 5% ) und 59 der 63 brusterhaltend operierten patientinnen ( 93 , 6% ) tumorfrei . von den 34 patientinnen in den stadien t3 und t4 berlebten nur 18 patientinnen fnf jahre ( 52 , 9% )  . 
tumorfrei waren lediglich zwlf von ihnen ( 29 , 4% )  . lokalrezidivrate von den 209 patientinnen , die postoperativ eine adjuvante radiotherapie erhielten , wurden 196 mit einer lokalen gesamtdosis von 60 gy , 13 patientinnen mit einer gesamtdosis von 50 gy behandelt . 
bei den 196 postoperativ mit bis zu 60 gy bestrahlten patientinnen erlitten sieben ein lokalrezidiv ( 3 , 5% ) , so da die kumulative lokalrezidivrate des gesamtkollektivs mit 3 , 6% ( acht von 209 patientinnen ) anzugeben ist . 
die kumulativen behandlungsergebnisse wurden jetzt fr die jeweilige vordefinierte altersgruppe ermittelt . vergleich der therapiemodalitten in den drei altersgruppen operation : nur ein knappes drittel der patientinnen wurde , unabhngig von der tumorgre , brusterhaltend operiert . am niedrigsten lag die rate in der gruppe der ltesten patientinnen mit 27 , 7% , signifikante unterschiede ergaben sich jedoch nicht ( tabelle 5 )  . polychemotherapie : der anteil der nodal positiven patientinnen , die mit polychemotherapie behandelt wurden , nahm mit dem alter ab . 
so erhielten 70% der lteren rezeptorpositiven patientinnen tamoxifen , whrend in der jngeren gruppe 85% und in der mittleren gruppe 94% mit tamoxifen behandelt wurden . behandlungsergebnisse in den altersgruppen gesamtberleben : 174 frauen , entsprechend 79 , 8% , berlebten fnf jahre . 
57 , 8% tumorfreien berlebens deutlich besser ab als die jngere gruppe mit lediglich 48 , 8% . lokalrezidive : von den acht lokalrezidiven traten vier bei patientinnen der jngeren altersgruppe auf . 
nur eine der vier frauen war initial nodal positiv , alle anderen drei nodal negativ gewesen . bei der mittleren altersgruppe erlitten drei patientinnen ein lokalrezidiv entsprechend einer rate von 3 , 2% . 
das entspricht einer rezidivrate von 1 , 2% . vertrglichkeit : eine auswertung der behandlungsunterlagen hinsichtlich radiogener nebenwirkungen ergab keine altersgruppenspezifischen unterschiede bei insgesamt geringer behandlungstoxizitt . diskussion fnf - jahres - berleben die gesamtberlebensrate der in der radiologischen universittsklinik behandelten patienten betrug nach fnf jahren 79 , 8% . 
 [ 30 ] ist bei nodal negativen tumoren nach operation und radiotherapie eine fnf - jahresberlebensrate von 69% zu erwarten , sauer [ 31 ] berichtete ber zehn - jahres - berlebensraten von 71% . die von uns festgestellte kumulative berlebensrate von 79 , 8% ist damit mit den angaben aus der literatur vergleichbar . t1und t2 - stadien : grere aussagekraft hat jedoch die darstellung in den jeweiligen tumorstadien . 
 [ 16 ] gaben 1993 eine berlebensrate fr t1n0 - tumoren von 87 bis 92% , fr nodal negative t2 - tumoren von 76 bis 81% an . die prognose nodal positiver tumoren ist dagegen deutlich schlechter . 
 [ 5 ] die berlebensrate bei t3und t4 - tumoren ohne fernmetastasen fr unter 50jhrige in diskrepanz zu unseren ergebnissen mit 80 , 8% , fr 60bis 69jhrige aber geringer mit 61 , 7% an . lokalrezidiv die lokalrezidivrate betrug insgesamt 3 , 6% : 3% in der gruppe der brusterhaltend therapierten , 4% bei den mastektomierten patientinnen . 
schon 1986 wurde von fisher et al . [ 11 ] eine lokalrezidivrate nach brusterhaltung unter 10% angegeben , wenn eine strahlentherapie durchgefhrt wurde . fnde diese nicht statt , stiege die lokalrezidivrate auf 30 bis 50% [ 10 ]  . 
levitt [ 24 ] gab eine lokalrezidivinzidenz von 28 , 8% ohne radiotherapie gegenber 6 , 2% mit bestrahlung auch westerhausen [ 35 ] beschrieb eine verminderung der lokalrezidivrate nach radiotherapie um mindestens 50% . die arbeitsgruppe um veronesi [ 34 ] fand 1993 eine lokalrezidivrate von 8 , 8% fr quadrantektomie und anschlieende adjuvante radiotherapie . 
die ergebnisse zeigen , da eine radiotherapie nach brusterhaltender operation obligat ist [ 33 ]  . daran , da eine strahlentherapie auch nach mastektomie sinnvoll sein kann , haben seegenschmiedt et al . 
auch wir ermittelten bei den jngeren patientinnen unter 50 jahren mit 9 , 3% die hchste lokalrezidivquote , whrend die quote bei den 50bis 65jhrigen auf 3 , 2% , bei den ber 65jhrigen sogar auf 1 , 2% sinkt . 
schon 1995 hatte sich diese rate auf 50% erhht [ 32 ]  . die von uns festgestellte fnf - jahres - berlebensrate nach brusterhaltung und radiotherapie lag bei 92% , vergleichbare zahlen gaben mansfield et al . 
nach einschtzung von dunst [ 10 ] ist mit einer rate von 5 bis 8% zu rechnen , diese liee sich aber durch eine lokale dosisaufsttigung wie in unserem kollektiv bis auf 1% senken . ablative therapie : 68 , 3% der patientinnen in unserem kollektiv wurden ablativ behandelt . 
 [ 19 ] hielten bei anwendung gleicher therapierichtlinien und dosierungen die durchfhrung einer radiotherapie bei lteren patienten fr problemlos und fanden keine entsprechend abweichenden toxizitten . primrtherapie : nach fleming et al . 
mit der vorstellung , da sich die tumorzellen bei lteren frauen langsamer teilen , empfahlen die autoren , ltere patientinnen nur bei genauerer indikationsstellung mit einer polychemotherapie zu behandeln . alle unsere patientinnen wurden , unabhngig vom alter , nach einem identischen schema behandelt . 
 [ 4 ] diese feststellung fr die niederlande nicht treffen : in einer untersuchung ber den einflu des alters auf die behandlungsstrategie kamen sie zu dem ergebnis , da ltere patientinnen seltener eine radiotherapie erhielten als jngere . 
 [ 12 ] erhalten in den usa ltere patientinnen grundstzlich eine weniger intensive therapie . einer der grnde drften die unterschiedlichen krankenversicherungssysteme in den vereinigten staaten und den niederlanden seso fand constanza [ 8 ] schon in der diagnostik eine weniger intensive und verzgerte durchfhrung bei lteren patientinnen . 
insofern mag der schlu erlaubt sein , da die menge der zur verfgung stehenden ressourcen und die kriterien , nach denen die behandlungen in deutschland indiziert werden , einen wesentlichen einflu auf die therapieergebnisse haben und dieser faktor in etlichen untersuchungen hinsichtlich der therapeutischen mglichkeiten zu wenig beachtung findet . altersspezifisches berleben : die jngste gruppe hatte ein gesamtberleben von 72% , die mittlere altersgruppe erreichte 85 , 6% und die lteste gruppe 77 , 1% . 
 [ 22 ] forderten , ltere patientinnen verstrkt in klinische studien aufzunehmen , damit fr sie dezidiertere therapieempfehlungen erarbeitet werden knnten . das lebensalter allein kann keineswegs als argument dafr dienen , diese patientinnen schlechter zu behandeln und ihnen etwa eine adjuvante radiotherapie vorzuenthalten . 
there were no statistically significant differences between patients treated with radiochemotherapy vs radiotherapy in terms of 5 - year survival ( 63% after radiochemotherapy vs 53% after radiotherapy , p = 0.16 ) , relapsefree survival ( 52% vs 50% ) and locoregional control ( 69% vs 67% )  . 
severe late toxicity was documented in 5% of treated patients . conclusions : prognosis of patients with uicc stage iii rectal cancer remains poor after standard surgery followed by postoperative adjuvant treatment ( pelvic radiotherapy and bolus intravenous injection of 5 - fu and leucovorin )  . 
more effective multimodality treatment strategies should be investigated in prospective randomized trials . key words : rectal cancer adjuvant treatment radiochemotherapy die postoperative adjuvante radiotherapie und radiochemotherapie der uicc - stadien ii und iii des rektumkarzinoms . 
44 patienten erhielten eine alleinige radiotherapie , bei 68 wurde zustzlich eine chemotherapie mit vier bis sechs fnftgigen zyklen 5 - fu ( 420 mg / m2 / tag ) und leucovorin ( 200 mg / m2 / tag ) durchgefhrt . 
 ergebnisse : das fnf - jahres - gesamtberleben war 84% fr das uicc - stadium ii und 45% fr das uicc - stadium iii ( p = 0 , 0045 )  . 
darber hinaus sollten effektivere multimodale therapiekonzepte im rahmen von prospektiven studien erforscht werden . schlsselwrter : rektumkarzinom adjuvante therapie radiochemotherapie s urgery is the main treatment option in rectal cancer . tnm - stage is the most important prognostic factor [ 22 ]  . once the tumor has penetrated the rectal wall ( stage dukes b2 or uicc stage ii ) or has spread to regional lymph nodes ( stage dukes c or uicc stage iii ) , there is a significant risk of developing a locoregional recurrence and / or distant metastasis that can rarely be cured . these high - risk tumors have been in the past the subject of randomized trials using preoperative or postoperative radiotherapy or radiochemotherapy [ 2 , 3 , 15 , 17 , 18 , 24 , 34 , 46 , 47 , 49 , 50 , 51 ]  . 
the randomized gastrointestinal tumor study group ( gitsg ) - trial first demonstrated a benefit in relapsefree survival after postoperative combined radiochemotherapy over surgery [ 17 ]  . since the consensus conference of the national health institute in 1990 , postoperative radiochemotherapy ( 50 gy + 5.4 gy to the pelvis and 6 weekly 5 - fluorouracil [ 5 - fu ] courses ) is recommended following curative surgery of rectal cancer uicc stage ii to iii [ 35 ]  . 
the consensus conference of the german cancer society has recently adopted these recommendations [ 42 ]  . quality of surgery is a well - known independent prognostic factor in rectal cancer , since it can substantially influence the development of a locoregional recurrence [ 22 ]  . 
figures of 4 to 10% [ 13 , 21 , 27 ] from single - institutional series contrast with figures of 24 to 34% from the randomized trials using standard surgery [ 18 , 24 , 46 , 47 ]  . the purpose of this study was to retrospectively evaluate the results of standard surgery followed by adjuvant radiotherapy or radiochemotherapy for uicc stage ii and iii rectal cancer . patients and methods one hundred and twelve patients ( 70 males , 42 females ) , referred from 12 surgical departments , were postoperatively treated after potentially curative ( r0 ) surgery for rectal cancer at the department of radiotherapy of the university of wrzburg between 1983 and 1994 . 
median age of patients was 60 years ( range : 30 to 83 )  . radiotherapy was given 3 to 17 weeks following surgery ( median 6 weeks ) and consisted of a 8 / 16 mv 4 - field isocentric box technique in 90 cases , a 3 - field isocentric technique in 15 cases and a co - 60 rotational technique in 7 cases . 
the tumor bed received a boost of 10 to 20 gy in 5 to 10 fractions . sixty - eight patients received additional chemotherapy with 4 to 6 courses of 5 - fu and leucovoreach course consisted of 5 daily bolus intravenous injections of 420 mg / m2 / d 5 - fu and 200 mg / m2 / d leucovor two of the chemotherapy courses were given during the first and last week of radiation treatment . 
endpoints studied included overall survival , relapse - free survival , freedom from locoregional recurrence , sites of relapse , acute and late toxicity . uicc stage ii ( n = 37 ) uicc stage iii ( n = 75 ) p = 0.0045 multivariate analysis was used to determine prognostic factors with significant impact on survival and relapse - free survival , including age , primary tumor stage , primary tumor location ( above vs below peritoneal reflection ) , presence of lymphatic vessel invasion , surgical method ( abdominoperineal excision vs anterior resection ) and radiation dose . 
for patients with stage iii disease survival differences between the 2 groups reached a statistically marginal significant value ( 55% vs 37% , p = 0.069 ) ( see figure 3 )  . 
multivariate analysis revealed that negative lymph node stage ( p = 0.015 ) , high tumor differentiation ( p = 0.0025 ) and chemotherapy ( p = 0.049 ) were associated with better overall survival rates and were independently statistically significant . 
five - year relapse - free survival was similar for patients treated with radiotherapy or combined modality ( 50% vs 52% ) ( figure 2 )  . for patients with uicc stage iii disease , a marginally significant difference in disease - free survival ( 32% after radiotherapy vs 42% after radiochemotherapy , p = 0.069 ) was observed ( figure 3 )  . 
all but 3 of the 18 classifiable pelvic recurrences occurred within the pelvis were in - field ( table 2 )  . the 5 - year rate of distant failure was 10% for n0 , 41% for n1 and 53% for n2 stage , respectively . 
adjuvant treatment for rectal cancer location of the recurrence absolute adjuvant patients in radiation number dose to the site of later recurrence complete remission after salvage operation anastomotic in - field presacral in - field perineal in - field out - field peritoneal out - field not classifiable 4660 gy 5262 gy 4660 gy 0 gy 0 gy unknown 0 / 11 table 2 . 
grade 3 and 4 leukopenia occurred in 25% of patients treated with radiochemotherapy and none in patients treated with radiation therapy alone . five patients experienced grade 4 late toxicity : i . 
 discussion this is a report of results of adjuvant therapy in 112 patients referred to our institution from 12 different surgical departments within a period of 10 years ( 1983 to 1994 )  . 
during this period , there was no consensus about the indications of adjuvant therapy for rectal cancer in our results , due to a negative patient selection , cannot be excluded . in germany and bias according to the surgical reports , all patients were treated with standard surgical techniques . 
the number of examined lymph nodes and circumferential tumor margins were not routinely reported by the histopathologist [ 1 , 7 , 19 , 38 , 39 ]  . with the exception that in the early years , higher radiation doses were used for high - risk tumors ( lymphatic invasion , r1 - resection ) , quality of treatment is comparable with that of recent published randomized trials using adjuvant radiotherapy [ 2 ] or radiochemotherapy [ 36 , 49 , 51 ]  . 
 the acute and late toxicity on our series correlates with the findings from other series using appropriate radiotherapy techniques [ 28 , 36 , 49 , 51 ]  . the significant differences in overall survival ( 84% vs 45% ) , relapse - free survival ( 80% vs 39% ) , local recurrence rates ( 16% vs 40% ) and distant metastasis rates ( 10% vs 53% ) between patients with uicc stage ii and iii disease show treatment radiation complications dose 1 . 
severe late complications after adjuvant therapy ( ar = anterior resection ; ae = abdominoperineal excision ; rt = radiation therapy ; rtch = radiochemotherapy )  . that among high - risk rectal cancer 2 groups with distinct prognosis exist . 
this has to be considered when comparing results from different series , since differences in the proportion of nodal positive to nodal negative cancers can substantially influence the results . the overall 5 - year survival ( 63% ) and disease - free survival ( 53% ) for the 68 patients treated with radiochemotherapy in our series are slightly lower than that reported from randomized trials recently [ 36 , 49 , 51 ]  . 
this study showed a significant improvement in overall survival ( 70% vs 60% ) and disease - free survival ( 63% vs 53% ) for patients treated with continuous infusion 5 - fu [ 36 ]  . 
in the intergroup 0114 trial , 4 different schemes of chemotherapy were used ( 5 - fu alone , 5 - fu with leucovorin , 5 - fu with levamisole and 5 - fu with leucovorin and levamisole )  . 
in the norwegian trial , the 5 - year recurrence - free and overall survival was 64% for the patients treated postoperatively with 46 gy and bolus 5 - fu 30 minutes before 6 of the radiotherapy fractions [ 51 ]  . 
 the 54% overall survival and 50% disease - free survival for the 44 patients treated with postoperative radiotherapy alone are slightly better than the corresponding rates in the eortc series using postoperative radiotherapy alone ( 47% and 40% ) [ 2 ]  . 
 the locoregional recurrence rate of 33% among the group treated with adjuvant radiotherapy is similar to that reported from the randomized eortc trial ( 35% ) [ 2 ]  . 
since the different chemotherapy schedules seem to play a minor role in locoregional control [ 36 ] , the main reason for these differences must be the negative patient selection in our series , as mentioned before . the estimated 5 - year probability of developing distant metastases in our series was 41% after radiotherapy and 32% after radiochemotherapy . 
 [ 36 ] reported a statistically significant decrease in distant metastasis rate after continuous infusion 5 - fu , as compared to bolus 5 - fu ( 31% vs 40% , p = 0 , 03 )  . currently , there are some controversies regarding the optimal management of high - risk rectal cancer , as defined uicc stages ii and iii [ 26 , 27 , 37 ]  . 
the inability of standard surgery with or without adjuvant treatment to achieve optimal locoregional control has been demonstrated in previous randomized series using a surgical control arm [ 3 , 15 , 17 , 29 , 49 , 51 ]  . 
applying the technique of tme ( total mesorectal excision ) , some surgeons have reported locoregional recurrence rates lower than that have ever been reported from series using adjuvant therapy after standard surgery [ 6 , 13 , 21 , 23 , 45 ]  . 
 quality of surgery is an independent prognostic factor for survival in rectal cancer since it can influence the incidence of a locoregional recurrence , but has no influence on the initial occurrence of distant metastasis [ 27 ]  . 
in a retrospective series of 1 , 285 patients with rectal cancer treated with surgery alone and were free of local recurrence on follow - up , kckerling et al . [ 27 ] found that metachronous distant metastases occurred in 40% of patients with stage iii disease , as compared to 16% in stage ii and 8% in stage i patients . 
this is higher than in the surgical series of kckerling and can be explained by the fact that most patients with distant metastases in our series ( 25 / 35 ) had local recurrences . 
as the gastrointestinal intergroup trial showed , continuous 5 - fu could reduce distant failures by nearly 9% ( from 40% to 31% ) , compared to bolus 5 - fu . this was statistically significant [ 36 ]  . 
after a median followup of 48 months , no reduction in distant failures could been observed after modulation of 5 - fu with leucovorin , levamisole or both , compared to 5 - fu alone , in the intergroup 0114 trial [ 49 ]  . 
additional studies will continue to be done to determine the optimal mode of administration as well as modulation of 5 - fu in order to decrease the incidence of metachronous distant metastasis in uicc stage iii rectal cancer . patients with uicc stage ii rectal cancer have a significant lower risk for developing distant metastasis than patients with uicc stage iii disease [ 27 ]  . 
a randomized comparison of tme alone vs standard adjuvant treatment could shown , whether optimized surgery alone is appropriate for this group of patients . radiotherapy is more effective when applied preoperatively , as a randomized swedish trial has shown [ 16 ]  . 
there seemed to be a trend towards tumor down - staging and sphincter preservation in the preoperative arm . the randomized swedish rectal cancer trial has recently shown that preoperative short - term radiotherapy with high single doses can improve survival , compared to standard surgery alone [ 47 ]  . 
yet , results of this trial indicate that this method can affect bowel function and there is a need for finding predictive factors for local recurrence to exclude patients with high probability of cure by surgery alone [ 12 ]  . further , this method cannot produce a significant downstaging and may not be appropriate for local advanced tumors or tumors located in the lower rectum , when sphincter preservation is attempted . a major challenge for the future is identifying those tumors that cannot be resected without leaving microscopic residual disease . 
thin - slice mri can provide excellent information about the local extension of rectal cancer and its relation to the mesorectal fascia [ 4 , 5 , 30 ] , but need further evaluation . since quality of life plays an increasingly important role for cancer patients , some centers have employed high - dose neoadjuvant radiotherapy and radiochemotherapy for resectable cancer of the lower third of the rectum in an attempt to preserve sphincter function [ 31 , 33 , 43 , 52 ]  . 
 conclusions prognosis of patients with uicc stage iii rectal cancer remains poor after standard surgery followed by postoperative adjuvant treatment ( pelvic radiotherapy and bolus intravenous injection of 5 - fu and leucovorin )  . 
adjuvant treatment for rectal cancer strahlentherapie und onkologie urban & vogel 2000 kurzmitteilung soft tissue sarcomas after radiation treatment for breast cancer three case studies and review of literature ulrich schulz1 , josef michael gokel2 , waldemar poleska3 aims : by means of 3 cases with infield soft tissue carcinomas after radiotherapy for breast cancer , symptoms and therapy are described . 
consequences for treatment planning and patients information before radiotherapy for breast cancer are discussed . patients : three of 1 , 025 patients with breast cancer irradiated from 1984 to 1997 suffered from infield secondary soft tissue sarcomas . 
two patients had been treated with breast - conserving therapy ( computerized planning , 50 gy to reference point , 5 times 2 gy / week , 5 - mv photons ) , 1 patient received a local boost dose of 15 gy ( 10 - mev electrons ) , patient 3 radiotherapy of the thoracic wall and regional lymph nodes after mastectomy using 12 - mev electrons ( thoracic wall ) and 5 - mv photons ( lymph node areas ) to 50 gy , 5 times 2 gy / week . no adjuvant chemotherapy was given . 
radiation dose could play a role , but there are very sparse data about this . conclusions : secondary soft tissue sarcomas are very rare , but familiar complications of radiotherapy . 
because of unclear correlations to the treatment parameters and rareness of this event , in our opinion no regular information to the patient receiving radiotherapy for breast cancer is mandatory . key words : breast neoplasms neoplasms , second / primary radiotherapy adverse side effects soft tissue sarcomas weichteilsarkome nach strahlentherapie wegen mammakarzinoms : drei fallstudien und literaturbersicht ziel : anhand von drei fllen von sekundren weichteilsarkomen innerhalb der bestrahlungsfelder werden symptomatik und therapie beschrieben und konsequenzen fr therapiekonzept und aufklrung bei der behandlung des mammakarzinoms diskutiert . patienten : drei von 1 025 wegen mammakarzinoms zwischen 1984 und 1997 bestrahlte patientinnen erlitten weichteilsarkome ( zwei angiosarkome , ein malignes fibrses histiozytom ) innerhalb der bestrahlungsfelder . 
zwei patientinnen waren brusterhaltend behandelt worden ( rechneroptimierte mammabestrahlung , 50 gy zvd , 5mal 2 gy / woche , 5 - mv - photonen ) , eine patientin erhielt zustzlich 15 gy mit 10mev - elektronen im tumorgebiet ( 4mal 2 , 5 gy / woche )  . 
bei der dritten patientin wurden nach mastektomie die brustwand ( 12 - mev - elektronen ) und der regionre lymphabflu ( 5 - mv - photonen ) mit 5mal 2 gy / woche bis 50 gy zvd bestrahlt . 
13 monaten , die dritte patientin an fernmetastasen und lokalrezidiv nach zwlf monaten . ergebnisse : die inzidenz spontan entstandener sarkome betrgt etwa 0 , 06% der malignen mammatumoren , die sekundr entstandener sarkome nach operation und bestrahlung von mammakarzinomen 0 , 09 bis 0 , 45% . 
eine aufklrungspflicht halten wir wegen der seltenheit von zweittumoren und angesichts sprlicher daten nicht fr gegeben . schlsselwrter : mammakarzinom strahleninduzierte tumoren brusterhaltende therapie weichteilsarkome t he induction of secondary tumors is a rare but wellknown long - term consequence of radiotherapy . 
 in our clinic for radiotherapy and radiation oncology and the clinic for gynecology and obstetrics of the klinikum krefeld 3 patients were observed between 1984 and 1997 who had soft tissue sarcoma in the radiation field following breast cancer , and these are discussed in the following report . 
a total of 1 , 025 patients underwent breast operations and subsequent radiotherapy in this period for breast carcinoma . case reports patient 1 patient 1 was born in 1922 , childless . 
 after clinical clarification lumpectomy in june 1992 as well as biopsy control of the margins of the right breast and contralateral biopsy in the upper outer area of the left breast were performed . 
the dissection of axillary lymph nodes was performed in a second operation due to heightened risk from anesthesia . pathological - histological diagnosis : invasive ductal , partly scirrhous breast carcinoma , tumor size 2 cm in diameter ; score of malignancy : 1 . 
 primary healing of the wound , slight lymph edema of the right forearpostoperative radiotherapy with 5 - mev photons , 5 times 2 gy per week up to a total of 50 gy on the complete remaining right breast ( inhomogeneity maximal + 10% ) .thereafter irradiation of the tumor region over a 6 6 cm area with 10 - mev electrons in fractions of 4 times 2.5 gy per week up to a total dose of 65 gy . 
on clinical examination edematous swelling of the right breast with extensive regressing moist epitheliolysis in the boost field was noticed . further consultation in june 1993 : lasting extreme tiredness , locally normal postoperative findings . 
thereafter continuation of follow - up with the local gynecologist . in july 1997 5 years after diagnosis of breast cancer a striking reddish discoloration of the middle section of the right breast occurred . 
from then on repeated local recurrences occurred , steady worsening of the general condition , increasingly frequent hemorrhage from the skin tumors leading to anemia , making blood transfusions necessary were noticed . the patient died of locally progressive tumor in november 1998 . patient 2 patient 2 was born in 1939 , childless , with no previous serious illness . 
in september 1993 , breast carcinoma on the left side at the edge of the outer quadrants was diagnosed . pathological - histological diagnosis : invasive ductal carcinoma , tumor size 1.2 cm , score of malignancy 2 . 
tumor staging : pt1 , pn1 , pm0 . computer - planned postoperative multifield irradiation of the left breast was performed with 50 gy tumor dose ( icru 50 ) , 5 times 2 gy per week , homogeneity + 8% / - 5% , using 5 - mev photons . 
thereafter boost in the region of the tumor with electrons , 12 mev , field size 6 6 cm , with 16 gy up to a total dose of 66 gy . 
no adjuvant chemotherapy was given . at the beginning of 1997 , about 3.5 years after diagnosis of breast cancer , the patient complained of increasing lymphedema of the left breast and left armammography and sonography identified an edema in july 1997 , however no signs of a new tumor could be detected . 
on clinical examination reddish discoloration and an unusually large number of newly formed teleangiectasiae of the breast skin as well as painful hardening and induration of the mammary gland itself were to be seen , therefore left mastectomy in july 1997 because of clinically suspected angiosarcoma , that being 46 months after the start of breast carcinoma treatment . 
pathological - histological diagnosis : poorly , in part moderately differentiated angiosarcoma ( tumor grading g 3 , in part g 2 ) of 26 5 cm . after local recurrence , a further resection with transposition flap had to be performed in august 1997 due to local recurrence of the angiosarcoma . 
now new skin changes could be seen in the previously healthy right breast , clinically resembling a hematoma , however , on histological examination turned out to be a moderately differentiated angiosarcoma as well . 
lymph node metastasis of the angiosarcoma in 1 of 13 axillary lymph nodes . systemic postoperative chemotherapy with epirubicine and ifosfamide ( 1 course ) and local chemotherapy with mitomycin c and mitoxantrone were applied . 
in addition , a large number of solid foci in the liver most probably representing metastases and polycyclic tumor formations of the pleura in the middle and lower left field as well as a 3 mm large spot in the upper right lung field were present . 
she had given birth to 10 children . right mastectomy in may 1993 with axillary and infraclavicular lymph node dissection due to an invasive ductal breast carcinoma in the lower inner quadrant ; tumor size 3.0 cm , score of malignancy g 2 . 
receptor status positive for estrogen and progesterone . due to the formation of seroma and to prolonged wound healing in the mastectomy area , the start of postoperative irradiation was delayed until 10 weeks after the operation . 
dose 5 times 2 gy per week up to a total dosage of 50 gy ( icru 50 ) within 5 weeks . overall satisfactory tolerance of the radiotherapy ; moist epitheliolysis in the axillary , supraand infraclavicular field at the end of the treatment . 
excision and histological examination led to the diagnosis of a malignant fibrous histiocytoma ( g 2 ) 6.5 cm in size ( figures 2a and 2b )  . the resection margins were free of tumor . 
gross recurrence occurred 4 months later , death from local tumor growth in may 1999 . discussion in these 3 patients , all histological examinations were performed by the same pathologist ( jmg )  . 
after occurrence of the sarcomas , all previous histologies were reviewed , and the diagnoses of a secondary sarcoma were confirmed . for all 3 patients the breast carcinoma was the first tumorous disease . 
all 3 patients showed deviations from the normal follow - up which retrospectively appear significant : in the case of patient 1 the accumulation of technetium - 99m in the right breast , which had been used for the bone scintigraphy 10 months after radiotherapy represented an unusual finding , which , however , was not further clarified . 
 in the case of patient 2 there was petechial bleeding on the edge of the boost field and a flat hematoma 4 weeks after radiotherapy was completed , the cause of which remains unclear . 
six months before the clinical manifestation of the angiosarcoma she complained of increasing lymphedema of the breast and arm , however no tumor could be detected by clinical or x - ray examination . in the case of patient 3 a revision of the axilla was undertaken 1 year after the primary operation due to suspected tumor recurrence , but only hematoma was found . 
incidentally this hematoma was not situated in the position of the subsequent malignant fibrous histiocytoma , which occurred in the upper arm muscles approximately 5 cm further away . in 1948 , in a classic publication on radiation - induced bone sarcoma following treatment of benign bone diseases , cahan et al . 
 these criteria , modified for the type of tissue affected , are currently used for radiation - induced secondary tumors [ 6 ]  . angiosarcomas can be highly differentiated and can be reminiscent of hemangiomas . 
primary angiosarcomas occur only in 1 in 1 , 700 to 1 in 2 , 000 cases of malignant tumors in the female breast and predominantly when the patient is in her 30s and 40s . about 1% of all sarcomas are angiosarcomas [ 1 ]  . 
not all 1 , 025 patients had a regular follow - up in our institutions , so that the true incidence of secondary tumors may be higher ( table 1 )  . 
 the period of latency from the end of radiotherapy following breast preserving treatment of breast cancer to the diagnosis of sarcoma amounts to 27 [ 4 ] or 29 to 72 months [ 2 , 15 ] , respectively , with 60 months as the mean figure . 
the latency periods in our patients were 61 , 46 and 59 months after primary treatment , respectively , this range being comparable to the literature referring to patients with primary breast cancer . 
the independent role of the radiotherapy treatment as a causal factor of the chronic lymphedema which often occurs in breast carcinoma treatment was long a source of controversial discussion , but today it is accepted as indisputable . 
on the other hand , chabner [ 7 ] described shorter periods of latency after chemotherapy plus radiotherapy . dunst [ 8 ] discusses for patients with ewings sarcoma cumulative risks of secondary sarcomas as 0% for doses below stewarttreves syndrome survival > 5 yrs pat . 
early mr - examination can considerably facilitate the diagnosis . therapy : mastectomy is the most effective treatment of an intramammary soft tissue sarcoma , although neoadjuvant strategies were reported recently in primary soft tissue sarcoma [ 13 ] possibly leading to a higher rate of r0 - resections . more radical intervention may also be required if necessary , e . 
chemotherapy can lead to temporary improvement , although the response is less good than in spontaneously occurring soft tissue sarcomas [ 12 ] ; this is explained by poorer local circulation of the blood . the prognosis for a post - irradiation soft tissue sarcoma is bad , as to be seen in our cases ; more than half of the patients die within 18 months . 
the most common reason for treatment failure is lung metastasis , although bone metastases and complications due to local progression may also lead to death , like in our patients . strahlentherapie und onkologie urban & vogel 2000 aktuelles forum influence of treatment technique on dose - volume histogram and normal tissue complication probability for small bowel and bladder a prospective study using a 3 - d planning system and a radiobiological model in patients receiving postoperative pelvic irradiation oliver klbl , susanne richter , michael flentje1 purpose : a prospective study was undertaken to evaluate the influence of pelvic irradiation techniques on the dose - volume histograms of organs at risk and to analyze its possible clinical relevance using radiobiological models . patients and methods : for 20 patients receiving postoperative pelvic irradiation because of rectal cancer a 3 - field technique ( 3 - ft ) , a 4 - field technique ( 4 - ft ) and an opposing field technique ( oft ) were designed by a 3 - d planning system ( helax , tms )  . 
 conclusion : using multiple field techniques both the dose to the organs of risk and the fractional part of risk organs within the high - dose region can be reduced significantly . 
using the biological model a small , but significant difference between a 3 - ft and a 4 - ft was demonstrated in favor to the 4 - ft . key words : pelvic radiotherapy treatment planning small bowel injury bladder injury der einflu der bestrahlungstechnik auf dosis - volumen - histogramm und nebenwirkungswahrscheinlichkeit von dnndarm und harnblase bei der postoperativen bestrahlung des rektumkarzinoms . 
eine prospektive studie unter verwendung eines 3d - bestrahlungsplanungssystems und strahlenbiologischer modelle hintergrund : in einer prospektiven analyse wurde der einflu unterschiedlicher pelviner bestrahlungstechniken auf die dosisund volumenbelastung der risikoorgane dnndarm und blase untersucht und dessen klinische relevanz mittels strahlenbiologischer modelle berprft . patienten und methode : bei 20 patienten , die einer adjuvanten bestrahlung des kleinen beckens nach operation eines rektumkarzinoms zugefhrt wurden , wurden eine drei - felder - technik ( 3 - ft ) , eine vier - felder - technik ( 4 - ft ) und eine gegenfeldtechnik ( gft ) unter verwendung eines 3d - bestrahlungsplanungssystems geplant . 
die zu erwartende komplikationsrate ( ntcp ) des dnndarms und der harnblase wurde errechnet nach dem model von lyman und kutcher unter verwendung der daten von emami . ergebnisse : die mediane dosis im bereich des ptv war fr alle untersuchten techniken gleich ( 3 - ft / 4 - ft / gft : 99 , 2% / 98 , 6% / 98 , 1% bezogen auf die dosis im normierungspunkt ; p > 0 , 05 )  . 
die gft zeigte im vergleich mit den mehrfeldertechniken eine signifikant hhere dosisund volumenbelastung der harnblase , was sich in einer signifikant hheren ntcp widerspiegelte ( 5 , 46% )  . 
zwischen 3 - ft und 4 - ft bestand lediglich ein sehr kleiner unterschied zugunsten der 4 - ft . schlsselwrter : pelvine bestrahlungstechnik bestrahlungsplanung dnndarmtoxizitt blasentoxizitt c arcinoma of the rectum is one of the most common cancer in the industrial nations [ 15 ]  . 
 the purpose of this study was to analyze the influence of different radiation techniques on the dose - volume histograms ( dvh ) of the small bowel and the urinary bladder by using a 3 - d planning systethe possible clinical relevance of these results was examined by radiobiological models . 
 patients and methods this study includes 20 consecutive patients ( 6 female , 14 male ) treated at the department of radiotherapy of the university of wrzburg between november 1996 and august 1997 . 
criteria for inclusion in this analysis were patients with a diagnosis of rectal cancer who underwent either anterior ( 17 patients ) or abdominoperineal ( 3 patients ) resection and received adjuvant postoperative external beam radiation therapy . 
the octagonal opening in the center of the belly board had a longitudinal and transverse diameter of 35 cdepending on size and weight of patients the opening was reduced by an insert on a diameter of 30 cm . volumes of interest the volumes of interest ( voi ) defined in each axial ct - slice are shown in figure 1 : a typical standard planning target volume ( ptv ) for postoperative adjuvant irradiation of rectal cancer , volume of small bowel ( vsb ) within the longitudinal extension of ptv , volume of bladder ( vb )  . position and extension of ptv were orientated by osseous ( l5 / s1 , linea terminalis , foramina obturatoria ) and soft tissue ( arteria iliaca interna , vena cava inferior , perineum ) structures . 
in the adjuvant situation normal tissues and organs may be part of the ptv both due to a risk of subclinical tumor involvement and requirements to compensate positioning uncertainties and movement . the dvh of the voi were analyzed relating to minimum , maximum , median and mean dose to small bowel and bladder . 
additionally the volume of small bowel and bladder within the 90% , 80% , 60% and 40% isodose was calculated . treatment planning treatment planning was done by a 3 - d planning system ( helax , tms )  . 
three different treatment techniques were designed using beams eye view for creating individual collimated blocks : 3 - field technique ( 3 - ft ) , 4 - field technique ( 4 - ft ) and opposing field technique ( oft )  . for the 3 - ft individual wedges were used to homogenize dose distribution within the ptv ( figure 2 )  . the dose was prescribed for the reference point according to icru 50 . 
all relative dose values are referring to the reference point ( icru 50 )  . the beam weights were specified relating the dose contribution to the reference point ( icru 50 ) ( figure 2 )  . 
treatment techniques for pelvic irradiation radiobiological model the dvh of small bowel and bladder were exported from tms into a special evaluation program ( diet = dose information evaluation for tms ) [ 21 ] using rtog data format offering the complete data being essential for the exact description of a treatment plan ( ct - information , voi , dose distribution , dvh )  . 
the ntcp values were determined by a dose reduction algorithm ( kutcher - burman model , [ 10 ] ) and a volume reduction algorithm ( lyman - wolbarst model , [ 14 ] )  . 
for each dose bin of a differential dvh a reference dose was calculated according to the linear - quadratic model . the parameter values necessary for evaluation ( td50 , slope , size factor , a / b ) were taken from emami et al . 
the calculation was done for a total dose of 50.4 gy ( single dose of 1.8 gy ) ( icru 50 )  . statistics for statistical analysis the 2 test and mann - whitney u - test were used . 
two - tailed p values were used and were considered statistically significant if < 0.05. results planning target volume median ptv was 1 , 345 cm3 ( range 1 , 042 to 1 , 693 cm3 )  . 
there was no significant difference between 3 - ft and 4 - ft relating the 90 / 80 / 60% isodose , but a trend vsb within the 90% isodose being smaller using the 4 - ft . 
blase : analyse des dosis - volumen - histogramms ( in prozent ) ( vb : volumen der harnblase ) ( statistisch signifikante unterschiede kursiv gedruckt )  . klbl o , et al . 
comparing 3 - ft and 4 - ft there was a small absolute , but a statistically significant difference in favor to the 4 - ft ( table 6 )  . discussion radiotherapy of the pelvis either as definitive or adjuvant treatment plays a significant role in the management of many gastrointestinal , gynecologic and genitourinary malignancies . 
these include hypertension [ 18 ] , diabetes mellitus [ 16 ] , pelvic inflammatory disease [ 30 ] , body habitus [ 19 ] , prior abdominal or pelvic surgery [ 13 ] , simultaneous chemotherapy [ 28 ]  . 
omental sling , retroversion of the uterus , permanent silastic prosthesis , placement of a removable pelvic spacer or an absorbable mesh sling have been used to move physically bowel from the pelvis [ 1 , 4 , 27 ]  . 
it is generally accepted that the total radiation dose [ 20 ] and the irradiated volume of the small bowel [ 6 ] are one of the major factors responsible for both acute and late side effects . 
 [ 5 ] irradiating in prone position without belly board , too , reported on an average small bowel volume within the high - dose region ( 95% isodose ) of 400 cm3 and a planning target volume of 900 cm3 . in our study using prone position in combination with a belly board the median volume of small bowel within the highdose region ( 90% isodose ) was 109.2 cm3 and the planning target volume 1 , 345 cm3 , although the definition of the planning target volume has been orientated on the same anatomical landmarks as done by the other investigators . 
the positive effect of a belly board on the reduction of small bowel volume within the high - dose region was confirmed by several studies [ 9 , 23 , 24 ]  . for irradiation of pelvis the most frequent used treatment techniques are 3 - ft , 4 - ft and ap / pa - field techniques . 
detailed data of the influence of these different treatment techniques on toxicity are rare in literature , respectively the knowledge of the influence of different treatment techniques on side effects is often based on individual clinical observation not on a systematic analysis . 
the methodology of most previous studies includes only an oral small bowel contrast and the production of orthogonal simulation films in prone position to define small bowel volume [ 8 ]  . 
another critical point of several studies was that either the part of small bowel within all treatment fields or the whole small bowel within the longitudinal field extension was measured . without the use of a planning system offering the possibility of dvh an analysis of irradiated dose to the whole small bowel was not possible . 
but it is well known , that prior pelvic surgery is often associated with an increased pelvic small bowel volume [ 6 ]  . at most a qualitative analysis was possible by this methodology but not a quantitative with regard to the exact irradiated volume of risk organs and the 3 - d dose distribution . in a retrospective study letschert et al . 
 [ 12 ] found a high incidence of severe small bowel complications ( 37% ) in patients treated with extended ap / pa - fields , whereas the complication rate was 6% for limited 3 - field pelvic treatment . 
in strahlentherapie und onkologie urban & vogel 2000 originalarbeit optimization of tumor radiotherapy part vi : modification of tumor glucose metabolism for increasing the bioavailability of 2 - deoxy - d - glucose ( 2 - dg ) in a murine tumor model rakesh kumar sharma1 , surender singh1 , mahavir degaonkar2 , partha raghunathan2 , amarnath maitra3 , viney jain4 aim : differential radiomodification induced by 2 - deoxy - d - glucose ( 2 - dg ) is proving to be a feasible modality for optimizing tumor radiotherapy . 
the finding may have interesting clinical implications in the form of increased manifestation of the radiation - induced damage in the case of use of these drugs as a potential adjuvant in radiotherapy of tumors . key words : mrs bioenergetics metabolic engineering 2 - deoxy - d - glucose hematoporphyrin derivative ehrlich ascites tumor radiotherapy optimization optimierung der tumorbestrahlung . 
teil vi : vernderung des glucosemetabolismus im tumor zur steigerung der bioverfgbarkeit von 2 - deoxy - d - glucose in einem murinen tumormodell hintergrund : die durch 2 - deoxy - d - glucose ( 2 - dg ) induzierte differentielle radiomodifikation kann zur optimierung der radiotherapie bei tumoren benutzt werden . 
unsere frheren arbeiten mit ehrlich - aszites - tumorzellen haben gezeigt , da die vorbehandlung mit hmatoporphyrinderivaten die aufnahme und phosphorylierung von 2 - dg erhht . die vernderungen des bioenergetischen profils waren auerdem ausgeprgter und lnger anhaltend . 
die vielversprechende kombination von hmatoporphyrinderivaten und 2 - dg wurde nun an ehrlich - aszites - tumor - tragenden musen weiter untersucht , um die auswirkungen auf das ansprechen nach radiotherapie zu bestimmen . material und methoden : solide tumoren ( mittleres volumen = 0 , 9 0 , 1 cm3 ) wurden auf swiss - albino - a - muse implantiert und mittels 60co fokal bestrahlt ( 10 gy )  . 
das bioenergetische profil im tumor wurde mittels 31p - mr - spektroskopie untersucht . ergebnisse : die aufnahme und phosphorylierung von 2 - dg konnte nach vorbehandlung mit hmatoporphyrinderivaten erhht werden . 
metabolic modulation of 2 - dg schlufolgerung : die vorgelegte studie zeigt , da eine vorbehandlung mit hmatoporphyrinderivaten die bioverfgbarkeit von 2 - dg in einem muse - ehrlich - aszites - tumor - modell erhhen kann . 
diese ergebnisse knnten interessante klinische konsequenzen haben , wenn man diese substanzen zusammen mit der bestrahlung von tumoren verwendet , da sich der bestrahlungsinduzierte schaden mglicherweise verstrkt manifestiert . schlsselwrter : mrs bioenergetik 2 - deoxy - d - glucose hmatoporphyrinderivate ehrlich - aszites - tumor radiotherapieoptimierung t he natural physiological and biochemical differences between normal and tumor cells may be utilized to design potent metabolic modulators of radiation response [ 10 , 11 ]  . 
 [ 13 ] suggested that by modulating energy supply using 2 - deoxy - d - glucose ( 2 - dg ) which blocks glucose utilization and glycolysis , the cellular repair processes could be selectively inhibited in the tumors [ 915 ]  . 
 the bioenergetic status of a tumor modulates some of the essential bioclinical parameters such as cell cycle , growth rate and resistance to therapy [ 1 , 18 , 19 , 21 , 35 , 38 ]  . 
the non - invasive follow - up of tumors plays a major role in therapy planning and monitoring of response to therapeutic regimes [ 20 ]  . energy - linked differential radiomodification of 2 - dg has proved to be a promising approach for improving radiotherapy of tumors [ 14 , 22 ]  . 
assessment of tumor bioenergetic status by 31p - mr spectroscopy has been suggested as a clinically applicable albeit indirect method to measure the effects induced by energy - linked radiomodifiers alone or in combination with other metabolic modulators in ehrlich ascites tumor cells [ 31 ]  . 
hematoporphyrin derivatives have been shown to affect the energy yielding pathways by inhibiting cytochrome - c oxidase , thereby reducing oxidative phosphorylation in tumor cells [ 4 ] , which in turn increases glucose utilization and glycolysis [ 16 ]  . 
 encouraging results of the combination of hematoporphyrin derivatives and 2 - dg in our studies on a perfused ehrlich ascites tumor cell system [ 31 ] followed by in - vitro validation [ 5 ] , prompted us to evaluate this promising combination in the murine tumor model for confirmation . 
preliminary results have already been reported [ 32 , 33 ]  . materials and methods tumor implantation and growth mrs experiments were carried out in 3 to 4 months old swiss - albino strain a male mice , weighing 25 2 g , given water and food ( hindustan lever , india ) ad libitum , with ehrlich ascites tumor grown in the thigh muscle to produce a solid tumor . 
 ehrlich ascites tumor cell line was regularly maintained by the serial weekly passage of tumor cell suspension in the ascites fluid of the mice by injecting 2.5 3 107 cells intraperitoneally . exponentially growing cells harvested on 7th day , were used as inoculuthe solid tumors were grown by injecting 1.5 3 107 cells in 0.2 ml volume subcutaneously in right hind leg of the mice . 
tumor volume ( v ) was calculated daily from day 4 after implantation by using the formula , v = p / 6 ( d1 3 d2 3 d3 ) , where the geometric assessment of the 3 orthogonal diameters d1 , d2 and d3 was carried out using calipers . 
the source - to - tumor surface distance was 80 cm . anesthesia and drug treatment tumor bearing mice were anesthetized by thiopentone sodium ( intraval , may & baker pharmaceuticals , uk ) injected intraperitoneally at a dose of 50 mg / kg body weight prior to mrs studies . 
a single turn 50 - mm triple band double tuned mini - surface rf coil switched to h - 1 / p - 31 mode was positioned over the region of interest ( tumor area ) for spectral accumulations . 
it covered a length of 5 cm and a depth of 2.5 cthe tumor bearing leg was raised with the help of a small pad ( h = ~1.5 cm ) so that the accumulation of signals from non - tumor areas are reduced . 
the homogeneity of the magnetic field was optimized for each experimental mice by shimming on the water proton resonance done with the help of a double tuned surface coil in the same coil geometry as for 31p measurement , taking symmetry of the peak as reference . 
a total of 2 , 048 transients were accumulated to ensure good signal - to - noise ratio , covering a spectral sweepwidth of 5 khz with an acquisition size of 8 k datapoints per free induction decay ( fid )  . 
since the peaks were broad and not very well resolved , height ratios were taken for comparison of the relative amount of metabolites of interest on the premise that signals originating from equivalent mass of tumor area were compared , and there was no change in line - width during dynamic measurements . 
major metabolites detected include 3 resonances from the a - , b - , and g - phosphates of ntp ( predominantly atp ) , inorganic phosphate ( pi ) , and phosphocreatine ( pcr )  . 
phospholipid metabolites observed include phosphomonoesters ( pme ) , primarily consisting of phosphocholine ( pc ) and phosphoethanolamine ( pe ) , and phosphodiesters ( pde ) , primarily consisting of glycerophosphocholine ( gpc ) and glycerophosphoethanolamine ( gpe )  . 
the g - ntp peaks overlap with b - phosphate of nucleoside diphosphate ( ndp )  . the a - ntp peak may contain contributions of a - phosphate of ndp together with other compounds such as oxidized and reduced nad / nadp . 
administered 2 - dg , none of the animals died but they displayed a series of observable behavioral responses over an approximately 4 - hour time period . ten minutes following 2 - dg administration mice became ataxic with limb splayed . 
31p - mr - spektren eines soliden ehrlich - aszites - tumors , die die effekte einer radiotherapie zeigen ( 60co fokales bestrahlungsfeld , gre 2 3 2 cm , 10 gy , dosisrate 0 , 4 gy / minute , hautabstand 80 cm )  . sharma rk , et al . 
nach abnahme des ersten spektrums wurden 2 - dg 2 g / kg krpergewicht intravens injiziert . 105 ' control chemical shift thesia was avoided after 2 - dg administration , as the animal was usually lethargic and motionless for about 4 hours . 
even 24 hours post treatment , the signal due to 2 - dg - 6 - p was clearly visible in the pme region of the spectra ( results not shown )  . 
after 2 to 3 hours of 2 - dg treatment , the b - atp / pi ratio decreased to about 55% and remained practically unchanged at this value even 10 hours post treatment . figure 3 shows the changes in the 31p spectrum of tumor after 2 - dg administration . 
maximum accumulation of 2 - dg - 6 - p was obpme ( 2 - dg - 6 - p ) b - atp / pi ratio effects of photosan - 3 ( ps - 3 ) and 2 - dg in unirradiated and irradiated tumors effects of 2 - dg on the radiation induced changes due to practical consideration ( distance of radiation source from nmr facility ) , the pretreatment control spectrum from the same mouse was not acquired and the results were compared with the average values of control studies under identical conditions . 
a comparison of the accumulation of pme and b - atp / pi ratio following treatment with 2 - dg with and without irradiation at 3 hours and 5 hours post treatment is shown in figure 6 . 
charakteristische 31pmr - spektren eines ehrlich - aszitestumors , die die effekte von 2 - dg ( 2 g / kg krpergewicht intravens ) zeigt , das zehn minuten vor bestrahlung ( 10 gy ) appliziert wurde . chemical shift the b - atp / pi , pcr / b - atp , gpc / b - atp ratios following combined treatment are displayed in figure 10 . 
by that time most of the fluctuations in phosphorylated metabolites appears to be over . discussion the size of rf coil used in the present investigation was larger than the tumor volume selected , hence the signals obtained do not essentially originate from tumor area only . 
the contaminated signal outside the region - of - interest arising from the high levels of skeletal muscle pcr , as shown in figure 1 , was not used for bioenergetic measurements . 
as we are primarily interested in monitoring the time course of the fate of drug and the induced effects , the posttreatment spectra were compared with pretreatment control , wherever possible . 
when treated effectively with radiation , tumors are reported to exhibit an anomalous reversal of the pattern of untreated growth , which does not simply reflect a decrease in tumor size [ 18 , 21 ]  . 
potential mechanisms to explain the observed spectral changes following tumor irradiation may include tissue effects ( such as perfusion , reoxygenation , recruitment of quiescent cells and immune responses ) , direct cellular effects ( such as biochemical or cytokinetic changes ) and repair of potentially lethal damage [ 17 , 18 , 21 , 27 , 37 , 38 ]  . effects of 2 - deoxy - d - glucose alone and in combination with photosan - 3 the time courses of the effects of photosan - 3 ( ps - 3 ) and 2 - deoxy - d - glucose ( 2 - dg ) alone and in sequential combination were studied in solid ehrlich ascites tumor in mice . 
the increased intensity in the signals in the pme region observed within ~ 35 minutes of injecting 2 - dg reflects phosphorylation of 2 - dg by hexokinase to 2 - dg - 6 - p similar to our earlier observation [ 31 ]  . 
this indicates that the rates of formation and intracellular levels of 2 - dg - 6 - p following the administration of 2 - dg may also be dependent on tumor viability and energetics . 
the build - up of the accumulated 2 - dg - 6 - p inhibits glycolysis by blocking hexosephosphate isomerase , thus inhibiting interconversion of hexose - 6 - phosphate and resulting in reduced atp levels . 
saturation in the levels of 2 - dg - 6 - p reflects that after attaining a particular level , the processes that lead to degradation of 2 - dg - 6 - p may be stimulated in addition to the reduced rate of 2 - dg phosphorylation due to reduced availability of energy ( atp ) [ 29 , 31 ]  . 
vernderungen in den 31p - mr - spektren , die durch ps - 3 und 2 - dg in kombination mit bestrahlung ausgelst wurden . 1200 1600 1200 1600 1200 1600 time ( min ) time ( min ) time ( min ) figure 10 . 
however , the bioenergetic status following ps - 3 and 2 - dg administration in the mouse tumor model of ehrlich ascites tumor cells was not observed to be decreased . these changes in energetic status following combined treatment may be related to tumor reoxygenation , i . 
the reacquisition of radiosensitivity of cells that were hypoxic before treatment , possibly due to an increase in tumor blood perfusion . the tissue concentrations of high energy phosphates depend on the rates of their synthesis and consumption . 
high energy phosphate synthesis may be reduced either by insufficient oxygen ( hypoxia ) or glucose ( hypoglycemia ) supply , or by insufficient blood perfusion ( ischemia )  . 
in the latter case , the tissue may suffer not only from lack of oxygen and glucose or other substrates of high energy phosphate synthesis , but also from the insufficient removal of waste products e . 
the finding that upon ps - 3 and 2 - dg combination the high - energy phosphate levels do not show much variation , suggests that they are well regulated : increased consumption is matched by corresponding increases in synthesis and vice versa . 
metabolic modulation of 2 - dg effects of 2 - dg on the radiation induced changes effects of combined 2 - dg treatment with gamma irradiation on sarcoma - 180 and normal mice showed differential responses [ 12 , 15 ]  . 
 effects of ps - 3 and 2 - dg on the radiotherapeutic responses a phenomenal increase in glycerophosphorylcholine ( gpc ) levels and corresponding decrease in pme was observed along with acid shift in ph [ 33 ]  . 
the decline in the bioenergetic status of the tumor is consistent with the tumor vasculature becoming incapable of providing a nutritive blood ( and hence oxygen ) supply to the rapidly proliferating tissue , leading to the onset and development of hypoxia [ 24 , 39 ]  . 
the observation of decreased pme content of tumors following treatment is in line with the in - vivo 31p - mrs studies on the response of radiotherapy on human breast tumor [ 34 ]  . 
we have previously hypothesized that elevation of gpc with constant decrease in pc upon irradiation may be due to increased breakdown and decrease in the biosynthesis of membrane phospholipids [ 30 ]  . 
this interpretation could also explain the present finding in the context of increased accumulation of 2 - dg - 6 - p following 2 - dg administration after ps - 3 pretreatment . 
are these related to a need to manufacture membranes for dividing cells , to changes in membrane composition related to invasion and metastasis , or to phospholipase activation during signal transduction involved in the control of cell proliferation ? the changes in tumor energetics observed following irradiation after administration of ps - 3 and 2 - dg treatment is consistent with reduced oxygen demand as a consequence of cessation of growth and improved blood supply as the tumor shrinks [ 35 ]  . a reduction in tumor cell density via cell death may lead to a reduction in interstitial tumor pressure with a consequent increase in tumor blood flow . 
it would also lead to a reduction in competition for available oxygen [ 23 ]  . this study demonstrated that tumor cells in vivo are more well - equipped to maintain the bioenergetic status during severe energy limiting conditions . 
therefore , approaches directed in increasing the bioavailability of 2 - dg are necessitated so as to optimize its use as adjuvant to radiotherapy . in conclusion , our results on a murine tumor model show that the mr spectroscopic studies in animal tumor models have great promise as a method for predicting and monitoring of response to therapy [ 3 , 7 , 8 , 20 , 28 ]  . 
the relationship between metabolic modulators and / or radiotherapy induced changes in tumor and energy metabolism seems to be complex and dependent on several factors , such as tumor size , vasculature ( vascular density , malformation of vessels , and vascular collapse ) , ph , oxygenation and nutritional conditions and all parameters should be taken into consideration while using the bioenergetic status as an indirect measure of tumor regression . 
improved methods of spatial localization and deeper insight into the biochemical and pharmacological significance of the observed spectral changes are required to forecast the exact implications of such studies in actual therapeutic practices . 
rd - p1 - 96 / inm - 280 . strahlentherapie und onkologie urban & vogel 2000 originalarbeit konventionelle und virtuelle simulation bei der retrobulbrbestrahlung stephan gripp , rolf doeker , michael glag , petra vogelsang , hildegard pape1 hintergrund : zur therapie der endokrinen orbitopathie wird die bestrahlung der retrobulbrrume eingesetzt . 
die konventionelle simulation mit lateralen 4 4 cm2 groen , ventral am lidwinkel ausgerichteten feldern wurde im observers eye view ( oev ) und mit digital rekonstruierten radiographien ( drr ) durchgefhrt . 
die zielvolumenerfassung und schonung der augenlinsen wurden in axialen schichten und multiplanaren rekonstruktionen ( mpr ) berprder abstand der orbitaspitze zu kornea , lidwinkel und kanthus sowie der kornea zur linsenrckflche wurde gemessen . ergebnisse : in allen 25 fllen wurden hypophyse und linse geschont . 
der vergleich mit normalwerten ergab eine deutliche abweichung des abstands kornea kanthus , whrend der abstand kornea linsenrckflche mit den normalwerten bereinstimmte . schlufolgerung : die konventionelle simulation der retrobulbrbestrahlung mit seitlichen , am lidwinkel ausgerichteten feldern gewhrleistet eine sichere schonung der augenlinsen und hypophyse . 
der lidwinkel oder die kornea sind als orientierungspunkte fr die ventrale feldgrenze besser geeignet als der laterale kanthus . schlsselwrter : ct - simulation virtuelle simulation endokrine orbitopathie morbus basedow retrobulbrbestrahlung conventional and ct simulation of radiotherapy in graves ophthalmopathy background : radiotherapy is commonly used in graves ophthalmopathy . 
the conventional simulation of 4 4 cm2 lateral portals confined anteriorly by the fleshy canthus was performed on a ct - simulator using the observers eye view ( oev ) and digitally reconstructed radiographs ( drr )  . 
the distances between the apex of the orbita and cornea , fleshy canthus , and bony canthus were measured as well as the distance between cornea and posterior face of the lens . results : the pituitary gland and the ocular lenses were spared in each case ( 25 / 25 )  . 
the distance between cornea and canthus differed significantly from normal eyes while the distance between cornea and posterior face of the lens was very similar to normal eyes . conclusions : conventional simulation of orbital irradiation with lateral fields confined anteriorly by the fleshy canthus ensures protection of the ocular lenses and the pituitary gland . 
the fleshy canthus and the cornea are more reliable landmarks as compared to the bony canthus . key words : ct simulation virtual simulation graves ophthalmopathy graves disease retrobulbar irradiation 1klinik fr strahlentherapie und radiologische onkologie , heinrich - heine - universitt dsseldorf . eingang des manuskripts : 9 . 
die position der lidwinkel wurde im observers eye view ( oev ) , einer oberflchenrekonstruktion , die durch unterschiedliche schattierung einen rumlichen eindruck vermittelt , definiert ( abbildung 1 )  . 
dreidimensionale ct - informationen ( schnittbilder ) standen fr diese planung nicht zur verfgung . anschlieend wurden in den axialen ct - schichten sowie anhand multiplanarer rekonstruktionen ( mpr ) die vollstndige erfassung der orbita und der augenmuskeln sowie die schonung der augenlinsen und der hypophyse kontrolliert . in den entsprechenden axialen schichten wurden die abstnde zwischen orbitaspitze und kornea , lidwinkel und lateralem kanthus sowie der abstand zwischen dem muskelansatz der extraokulren augenmuskeln zur kornea bestimmt ( abbildung 3 )  . 
die 95% - konfidenzintervalle wurden aus der probenstandardabweichung mit hilfe der t - verteilung berechnet [ 5 ]  . ergebnisse in allen fllen ( 25 / 25 ) befanden sich beide augenlinsen und die hypophyse auerhalb des zielvolumens . 
die genaue pathogenese ist unbekannt , jedoch deuten zahlreiche untersuchungen darauf hin , da stimulierte retrobulbre t - lymphozyten durch sekretion verschiedener zytokine parakrin orbitale fibroblasten aktivieren , die glykosaminoglykane synthetisieren [ 3 ]  . 
eine kausale therapie ist ebensowenig bekannt wie prventive manahmen . strahlentherapie und antiinflammatorische corticoidgaben gelten bei schweren verlufen als therapiestandard [ 19 ]  . bei therapieresistentem exophthalmus oder visusverlust wird die orbita operativ dekomprimiert [ 1 ]  . 
klinisch [ 18 ] sowie kernspintomographisch [ 14 ] sind 20 gy effektiver als 10 gy , andererseits verbessert eine dosiserhhung auf 30 gy die ergebnisse nicht [ 17 ]  . 
daher ist eine fraktionierte bestrahlung von 20 gy in einzeldosen von 2 gy vor allem im angloamerikanischen sprachraum blich geworden , whrend auch niedrigere dosen erfolgreich angewendet wurden [ 2 , 10 , 22 , 24 ]  . das zielvolumen wird von den charakteristischen morphologischen vernderungen der orbitalen gewebe bestimmt . insbesondere verdickungen der augenmuskeln , die sich in ct , mrt und ultraschall mit groer regelmigkeit nachweisen lassen , stellen einen typischen befund dar und knnen in bis zu 40% auch ohne klinischen befund nachgewiesen werden [ 7 ]  . 
die hypophyse , aufgrund irriger pathogenetischer vorstellungen frher in das zielvolumen eingeschlossen , wird geschont . die bestrahlung der retrobulbrrume erfolgt ber seitliche gegenfelder , deren ventrale feldgrenzen am therapiesimulator anhand des knchernen augenwinkels ( processus frontalis ossis zygomatici ) [ 6 ] oder mit bleikugelmarkierungen [ 8 ] festgelegt werden . 
im unterschied zur konventionellen simulation ermglicht die ct - gesttzte simulation [ 23 ] durch den hohen weichteilkontrast und die dreidimensionale auflsung eine exakte definition des zielvolumens ohne rckgriff auf kncherne leitstrukturen . 
an unserer institution erfolgte die planung der retrobulbrbestrahlung bei morbus basedow bis 1997 mit einem konventionellen therapiesimulator nach einer einheitlichen technik : die lidwinkel wurden mit bleikugeln markiert und laterale 4 4 cm2 groe gegenfelder mit einem divergenzausgleich von 2 dorsal an die lidwinkelmarken angesetzt . 
the lead ball indicates the fleshy canthus . ebenfalls in 96% in sagittaler ausdehnung vollstndig erfat . die augenmuskeln wurden bei verwendung der lidwinkel als ventrale feldgrenze in 28% ( 7 / 25 ) nicht vollstndig eingeschlossen . 
der abstand zwischen kornea und lidwinkel ergibt sich daraus mit 14 , 3 mm und stimmt mit den gemessenen abstnden zwischen kornea und ansatz der ueren augenmuskeln von 14 , 1 mm ( 13 , 6 bis 14 , 5 mm ) bere die ergebnisse der topographischen orbitamessungen ( mittelwerte , wertebereiche und 95% - konfidenzintervalle ) sind in tabelle 1 zusammengefat . mit einem divergenzausgleich von 5 ( sad = 100 cm ) empfohlen [ 6 , 16 ]  . 
bei allen von uns untersuchten patienten fhrte allerdings diese wahl der ventralen feldbegrenzung zu unvollstndiger erfassung der augenmuskeln . detaillierte topographische untersuchungen an 66 computertomographischen normalbefunden ergaben einen mittleren abstand von kornea zu lateralem kanthus von 16 mm [ 12 ]  . 
selbst bei normalbefunden unterliegt der diskussion mit zunehmender verbreitung von ct - simulatoren ( virtuelle simulation ) stehen geeignete werkzeuge zur verfgung , die vollstndige erfassung des zielvolumens durch die konventionelle simulation und die schonung kritischer organe detailliert zu berprfen . 
digital rekonstruierte radiographien ( drr ) und oberflchenrekonstruktionen im observers eye view ( oev ) gestatten eine realistische nachbildung des konventionellen simulationsprozesses , whrend sich am gesamten ct - datensatz das bestrahlte volumen in axialen ct - schichten und multiplanaren rekonstruktionen detailliert untersuchen lt . 
der direkte vergleich von konventioneller und ct - gesttzter simulation wird allerdings durch die geringere auflsung / bildqualitt der digital rekonstruierten radiographien ( 1 , 5 mm bei 3 - mm / 3 - mm - schichten ) gegenber rntgenaufnahmen ( 0 , 24 mm ) eingeschrnkt [ 9 ]  . bei der strahlentherapie der endokrinen orbitopathie umfat das zielvolumen den retrobulbrraum und insbesondere die extraokulren augenmuskeln . 
results of measurements on orbital cts and 95% confidence intervals . abstand kornea kanthus wesentlich strkeren schwankungen als der abstand zwischen augenlid und linsenrckflche [ 12 ]  . von einigen autoren wurde die kornea bzw . 
die empfohlenen abstnde zwischen korneascheitel und ventraler feldgrenze schwanken zwischen 12 und 20 m der abstand zwischen kornea und linsenrckflche von 7 , 5 mm bei einem normalkollektiv [ 12 ] stimmt im rahmen der bildauflsung von ca . 
ein abstand zwischen ventraler feldgrenze und augenlid von 12 bis 15 mm [ 4 , 21 ] trgt dem halbschatten an linearbeschleunigern rechnung . dieser wert entspricht gerade dem hier ermittelten abstand der kornea zum lidwinkel ( 14 , 3 mm ) und zu der insertionsstelle der augenmuskeln am bulbus ( 14 , 1 mm )  . 
die neuesten empfehlungen der stanford - gruppe [ 24 ] favorisieren ebenfalls lidwinkelmarken zur ventralen feldbegrenzung und entsprechen damit weitgehend unserer konventionellen simulationspraxis . schlufolgerung mit der ct - simulation ist eine quantitative bewertung konventioneller simulationstechniken mglich . 
die konventionelle simulation der retrobulbrbestrahlung mit lateralen feldern , die ventral durch die lidwinkel begrenzt sind , fhrt zu einer sicheren schonung von augenlinsen und hypophyse bei zuverlssiger erfassung der retrobulbrrume . 
the semi - 3 - d and 3 - d treatment plans were compared to hypothetical 2 - d plans using dose - volume histograms and dose non - uniformity ratios . 
the accuracy of tumor bed localization and the conformity of planning target volume and treated volume were also analyzed in each technique . results : with the help of conformal semi - 3 - d and 3 - d brachytherapy planning we could define reference dose points , active source positions and dwell times individually . 
we could achieve the best conformity between the planning target volume and the treated volume with the ct - image based 3 - d treatment planning , at the cost of worse dose homogeneity . 
the mean treated volume was reduced by 25.1% with semi - 3 - d planning , however , it was increased by 16.2% with 3 - d planning , compared to the 2 - d planning . 
 conclusion : the application of clips into the tumor bed and the conformal ( semi - 3 - d and 3 - d ) planning help to avoid geographical miss . 
die bedeutung der semi - 3dund 3d - behandlungsplanung ziel : zu vergleichen sind die konventionelle 2d - , die simulatorgesttzte semi - 3dund das heutzutage entwickelte ctgeplante 3d - brachytherapie - planungssystem bei der interstitiellen radiotherapie des mammakarzinoms . patienten und methode : bei 103 patientinnen mit mammakarzinom der stadien t12 , n01 wurde das tumorbett mit klips whrend der brusterhaltenden operation markiert . 
die genauigkeit der lokalisation des tumorbetts und die konformitt des planungszielvolumens und des bestrahlungsvolumen wurden bei allen techniken analysiert . ergebnisse : mit hilfe der konformellen semi - 3dund 3d - brachytherapie - planung konnten wir die referenzdosispunkte , die aktiven quellenpositionen und quellenstandzeiten definieren . 
mit der semi - 3d - planung reduzierte sich das durchschnittliche bestrahlungsvolumen um 25 , 1% , mit der 3d - planung wurde es , verglichen mit der 2d - planung , um 16 , 2% erhht . schlufolgerung : klipmarkierung des tumorbetts und die konformelle ( semi - 3dund 3d - ) planung helfen , den geographischen fehler zu verhindern . 
die konformelle 3d - brachytherapie braucht eine neue bestrahlungsplanungskonzeption , die die irregulre dreidimensionale form des zielvolumens bercksichtigt . die etablierung der ct - gesttzten 3d - brachytherapie in die klinische routine ist ein erstrebenswertes ziel . schlsselwrter : mammakarzinom brachytherapie 3d - ct - planung t hree - dimensional ( 3 - d ) treatment planning has made the most promising progress in the last decade of radiotherapy . 
currently , the conformal 3 - d teletherapy is already part of routine clinical work in the vast majority of the radiotherapy departments , however , the 3 - d brachytherapy treatment planning has just become the center of interest [ 1 , 3 , 4 , 6 , 8 , 15 ]  . 
recent experiences especially in interstitial 3 - d brachytherapy highlighted the necessity of reconsidering the traditional rules of dose and volume specification for prescribing and reporting interstitial therapy [ 1 , 46 , 12 , 13 ]  . the widely accepted paris - system [ 9 ] does not meet every requirement of conformal brachytherapy planning . 
the socalled conformal thinking in brachytherapy prefers prescriptions of dose to the 3 - d target volume and normal tissue volumes , rather than to fixed reference points . the aim of this study was to compare the conventional 2 - d , the simulator - guided semi - 3 - d and the recently developed ct - image based 3 - d brachytherapy treatment planning in the interstitial radiotherapy of breast cancer and to interpret the differences between traditional 2 - d and recent 3 - d treatment planning . 
all patients received postoperative brachytherapy to the tumor bed via flexible implant tubes as a boost after 46 to 50 gy teletherapy ( 52 patients ) or as a sole brachytherapy ( 51 patients )  . 
the mean follow - up time was 27 ( 7 to 44 ) months . implant technique all patients were treated with a nucletron - microselectron hdr remote afterloading equipment using an iridium - 192 isotope with initial activity of 370 gbq ( 10 ci )  . 
the rules of the parissystem were used for planning of the implant geometry [ 9 ]  . before implantation a simulation x - ray examination was done with template on the breast to define the entrance and exit points of the needles being guided by the clips of the tumor bed . 
after the pre - implant simulation , 3 to 11 ( median : 7 ) guide needles were inserted into the previously targeted area in a triangular setting with template guidance . 
the spacing between the needles was 15 mm , the adjacent planes were separated by 13 m single , double and triple plane implant was performed in 6 , 89 and 8 cases , respectively . 
our planning concepts are based on the 3 - d reconstruction of the catheters , tumor bed clips and skin points using 2 x - ray films with variable angle ( figure 1 )  . 
secondary reconstruction of the volume data was done in paraxial plane , perpendicular to the implanted catheters and the target volume was delineated in each slice ( figures 3 and 4 )  . 
with the help of bps software , dose points were placed on the surface of the reconstructed 3 - d target volume ( figures 5 and 6 ) and dose optimization on the surface of this target volume was performed ( figure 7 )  . hypothetical 2 - d planning on the hypothetical 2 - d plans the distances of reference dose points from the catheters were uniformly chosen at 5 mm , since this reference distance can guarantee similar dose homogeneity as the traditional paris - system at our implant geometry [ 9 ]  . 
the active lengths were defined as the whole in - breast sections of the catheters , except the most peripheral 10 mm sections at both ends under the sk figure 3 . 
dosispunkte ( blau ) auf der oberflche des 3d - zielvolumens ( rot )  . analysis of 2 - d , semi - 3 - d and 3 - d dose plans the conformal semi - 3 - d and 3 - d dose plans were compared to the hypothetical 2 - d plans for each implantation . the accuracy of tumor bed localization and the conformity of planning target volume and treated volume was analyzed in each technique . 
the evaluations involved the use of cumulative dose - volume histograms and dose non - uniformity ratios ( dnr ) , defined as the ratio of the 150% high - dose volume ( v 150% ) to the 100% reference - dose volume ( v 100% ) , as described by saw et al . 
the mean central dose ( mcd ) [ 9 ] , maximum basal dose ( mbd ) , total reference air kerma ( trak ) , minimum dose of surgical clips ( minimal clip dose ) and mean skin dose ( calculated as average dose values of skin points ) were compared . 
for the last 10 implantations where ct - image based 3 - d dose plans were also available the mean target doses ( mtd ) were also compared to each other . 
the mean target dose was defined as average dose values of all dose points on the surface of the three - dimensional target for 2 - d , semi - 3 - d and 3 - d treatment plans . 
anatomical based dose - volume histograms were not used , since our software version was not capable of calculating them . results comparison of 2 - d and semi - 3 - d plans the results of quantitative assessment of 2 - d and semi - 3 - d treatment plans are summarized in table 1 . 
die 100% - referenzisodosenflche : blau , zielvolumen : rot . pressing implant homogeneity ( dnr , mcd and mbd ) were significantly better with 2 - d planning ( table 1 )  . 
highdose volume and trak slightly decreased with semi - 3 - d planning ( table 1 )  . comparison of 2 - d , semi - 3 - d and 3 - d plans the results of quantitative assessment of 2 - d , semi - 3 - d and 3 - d treatment plans are summarized in table 2 . 
semi - 3 - d planning reduced the treated volume by 19% , but 3 - d planning increased it by 16.2% ( compared to 2 - d planning )  . 
the values of minimal clip dose , ratio of underdosaged clips and mean target dose were the best , however , values of dnr , mcd and mbd were the worst with 3 - d planning ( table 2 )  . 
ct - image based conformal brachytherapie of breast cancer discussion the traditional paris - system was described by pierquin et al . [ 9 ] in 1964 for interstitial , radioactive wires with uniform linear activity . 
the rules of other dosimetry systems for interstitial brachytherapy , such as manchester and quimby are also unique , but primarly they are also based on geometrical considerations [ 2 , 7 ]  . 
the traditional dosimetry systems take the 3 - d shape of the target volume into account only by the selection of implant geometry , however , postimplant modification of dose distribution is not possible . since the stepping source afterloading equipments and the modern brachytherapy planning softwares are nowadays routinely available , computerized dose optimization on individually defined dose points and geometry can be performed . in this way we can achieve conformal dose distribution , tailored to the 3 - d shape of the target volume . 
 recent developments in image based interstitial brachytherapy have fundamentally changed the philosophy of brachytherapy treatment planning and raised the question of how to report dose and volume specification in interstitial brachytherapy [ 1 , 46 , 8 , 14 ]  . 
the aim of the icru report 58 [ 4 ] was to develop a common language for reporting interstitial therapy , which was suitable for all brachytherapy systems . however , its elements are based on the traditional parissystem [ 9 ]  . 
currently , the guidelines of the icru report 58 are suitable to compare recent sophisticated 3 - d brachytherapy treatments to a well validated , but 35 - year - old brachytherapy syste saw et al . 
however , it is not to be expected that in different clinical situations target volume coverage and irradiation of critical structures have the same power on implant quality , as well as on clinical outcome . 
we were able to achieve the best conformity between the planning target volume and the treated volume with the ct - image based 3d treatment planning at the cost of worse dose homogeneity , expressed by the higher values of dnr , mcd and mbd compared to 2 - d treatment planning . 
the adequate homogeneity is also important , but it is relatively subsidiary . despite the worse dose homogeneity ( higher dnr , mcd and mbd ) of semi - 3 - d and 3 - d plans , high - dose volume slightly decreased with conformal planning , explained by the shorter active lengths with semi - 3 - d and 3 - d planning . the mean skin dose was markedly reducible with semi - 3 - d and 3 - d treatment planning . 
the treated volume ( v 100% ) and trak was also decreased significantly with semi - 3 - d planning , however , it was unexpectedly increased with 3 - d planning . 
the explanation for this result is , that at 3 - d treatment planning , the treated volume conforming to the clinical target volume as defined on multiple ct - slices ( 3 - d visualization ) , was significantly larger in all cases , than the treated volume at semi - 3 - d treatment planning , where the positions of surgical clips were taken into account . 
semi - 3 - d treatment planning based on the positions of surgical clips is a useful tool to avoid geographical miss , however , it underestimates the real extent of the target volume . 
the irregular 3 - d shape of the target volume and the normal tissue structures can only be localized correctly on the basis of visual information obtained from cross - sectional imaging . 
 [ 15 ] implemented 3 - d virtual brachytherapy of breast cancer to solve this problethe virtual implant procedure was performed by the help of radioopaque skin markers , virtual image of template , pre - implant and post - implant ct scans . 
they found , that 3 - d virtual brachytherapy showed excellent agreement in target volume coverage between the preplanned virtual implant and the actual position of the final afterloading needles . however , they noted that there were practical limitations to their technique , because the needle placement must occur with minimal displacement or compression of the breast . 
semi - 3 - d treatment planning based on the positions of surgical clips is a useful tool to avoid geographical miss , however , it underestimates the real extent of the target volume . 
the irregular 3 - d shape of the target volume and the normal tissue structures can only be localized correctly on the basis of visual information obtained from cross - sectional imaging . 
the best conformity between the planning target volume and the treated volume is accessible with the ct - image based 3 - d treatment planning , however , within the scope of our study , it yielded the worst dose homogeneity . 
larger treated volume in 3 - d planning might increase the incidence of fibrosis , but at a mean follow - up of 27 months serious side effects were not observed . currently , conformal 3 - d brachytherapy is still a promising subject of clinical research . 
the time effort of breast implantation with 3 - d treatment planning is about 3 to 4 hours , but it can be reduced to 2 to 3 hours under optimal technical conditions ( on - line connection between helical ct and treatment planning system ) , which would allow its routine use in clinical practice . 
however , until this forthcoming common language based on world - wide consent is lacking , one can report the results of interstitial brachytherapy following the guidelines of the icru report 58 [ 4 ]  . 
ct - image based conformal brachytherapie of breast cancer strahlentherapie und onkologie urban & vogel 2000 originalarbeit erste ergebnisse der neoadjuvanten simultanen radiochemotherapie bei fortgeschrittenen rektumkarzinomen ute kchenmeister1 , ralf kirchner2 , jochen mellert2 , gunther klautke1 , ralph mcke1 , ulrich - theodor hopt2 , rainer fietkau1 hintergrund : bei lokal weit fortgeschrittenen rektumkarzinomen ist das erreichen einer r0 - resektion schwierig . muss jedoch makroskopisch oder mikroskopisch tumorrest zurckgelassen werden , ist die prognose der patienten schlecht . 
in der ersten und fnften bestrahlungswoche erhielten die patienten an fnf aufeinander folgenden tagen eine dosis von tglich 1000 mg / m2 5 - fu als intravense dauerinfusion ber 24 stunden . 
 schlsselwrter : rektumkarzinom properative therapie radiochemotherapie first results of concurrent preoperative radiochemotherapy of locally advanced rectal cancer purpose : in locally advanced rectal cancer tumor - negative margins often cannot be obtained by surgery alone . 
due to the poor prognosis of patients with r1 / r2 resection the deutsche krebsgesellschaft recommends concurrent preoperative radiochemotherapy for patients with locally advanced rectal cancer . patients and methods : between may 1997 and november 1999 22 patients were treated with preoperative radiochemotherapy . 
on days 1 to 5 and 29 to 33 patients received concurrently 5 - fluorouracil ( 5 - fu ) as continuous infusion of 1 , 000 mg / m2 . 
if there was any sign of cardiac toxicity chemotherapy was changed to 5 - fu / folinic acid or ralitrexed . results : surgery following radiochemotherapy was performed in 19 / 22 patients . 
muss mikroskopisch oder makroskopisch tumor zurckgelassen werden , so sinkt die fnf - jahres - berlebensrate von 50 bis 75% in den uicc - stadien ii / iii auf 15 bis 20% [ 15 ]  . 
in klinisch lokal weit fortgeschrittenen stadien ( klinisches stadium mason iv ) ist eine kurative resektion nur in 40 bis 55% der flle mglich [ 21 , 23 , 24 ]  . 
die mediane nachbeobachtungszeit betrgt 16 monate ( sechs bis 35 monate )  . properativ wurde die t - kategorie mittels endosonographie oder , falls diese nicht mglich war , mittels ct - untersuchung evaluiert . 
acht patienten hatten properativ einen ct3 - tumor , 14 patienten einen ct4 - tumor , fnf patienten hatten endosonographisch keine lymphknotenmetastasen ( cn0 ) , bei 17 patienten ergab sich im ct oder in der sonographischen untersuchung der verdacht auf lymphknotenmetastasen , drei patienten wiesen zum zeitpunkt der diagnose fernmetastasen auf . 
die mehrzahl der tumoren ( 12 / 22 ) befand sich im distalen rektum ( 0 bis 5 cm ab ano ) , 7 / 22 im mittleren drittel ( 5 bis 10 cm ab ano ) sowie 3 / 22 im proximalen drittel ( > 10 cm ab ano )  . strahlentherapie die bestrahlung erfolgte am linearbeschleuniger mit 9bzw . 
 chemotherapie in der ersten und fnften bestrahlungswoche erhielten die patienten an fnf aufeinander folgenden tagen eine dosis von tglich 1 000 mg / m2 5 - fluorouracil ( 5 - fu ) ( maximaldosis 1 800 mg ) als intravense dauerinfusion ber 120 stunden . 
bei auftretender kardiotoxizitt wurde die chemotherapie auf 5 - fu - bolusinfusion oder auf ralitrexed ( 3 , 0 mg / m2 alle drei wochen ) umgestellt . statistische analyse die berlebensraten wurden analog kaplan - meier unter verwendung des pc - programm - pakets spss nach diagnosestellung berechnet . 
ein patient ( ohne fernmetastasen ) verweigerte die operation . bei 16 / 19 ( 84% ) operierten patienten konnte lokal eine r0resektion erreicht werden ; die bei einem patienten synchron aufgetretenen fernmetastasen wurden nicht reseziert . bei drei patienten wurde mikroskopischer residualtumor zurckgelassen . 
pathohistologisch fand sich bei einem patienten kein tumor nach abschluss der radiochemotherapie , ein downstaging um mindestens eine t - kategorie wurde bei 12 / 19 ( 63% ) patienten erzielt ( tabelle 2 )  . tumorhhe operationsart ( n = 22 ) 05 cm 510 cm > 10 cm keine operation : resektion : exstirpation : keine operation : resektion : exstirpation keine operation : resektion : exstirpation : tabelle 1 . 
downstaging of the t stage and the lymph node involvement . rezidivanalyse , berlebensdaten bei einer medianen nachbeobachtungszeit von 16 monaten ist bisher kein lokales rezidiv bei den operierten patienten aufgetreten , auch nicht bei den drei r1 - resezierten patienten . 
das progressionsfreie berleben der 19 operierten patienten betrgt nach 24 monaten 62 14% ( abbildung 1 ) , der r0 - resezierten patienten 61 14%  . die berlebensrate aller patienten war nach zwei jahren 76 10% ( abbildung 2a ) , der operierten patienten 89 8% ( abbildung 2b ) , der r0 - resezierten patienten 87 8% . toxizitt die akuttoxizitt der simultanen radiochemotherapie war vertretbar . 
auffllig war der hohe anteil an patienten mit kardiotoxizitt ; immerhin wurde der verdacht bei 4 / 22 ( 18% ) patienten geuert , sodass hier das chemotherapieschema umgestellt wurde . 
ned - survival of all surgically treated patients following neoadjuvant radiochemotherapy . die vorliegende untersuchung zeigt , dass nach einer properativen radiochemotherapie bei fortgeschrittenen tumoren zeit in monaten zeit in monaten abbildung 2a . 
entsprechend der hier vorliegenden untersuchung konnten bei fortgeschrittenen t3 - / t4 - tumoren in 5 bis 20% pathohistologisch komplette remissionen und r0 - resektionen bei 60 bis 90% der patienten erzielt werden . die unterschiede in den r0 - resektionsraten und in den remissionsraten drften sich im wesentlichen damit erklren lassen , dass von den operateuren die resektabilitt primr verschieden eingestuft wird und somit unterschiedlich fortgeschrittene tumoren in den verschiedenen zentren neoadjuvant behandelt werden . 
unsere ersten berlebensdaten nach zwei jahren ( 76% gesamtberlebensrate , 89% der operierten patienten ) weisen darauf hin , dass die prognose der kurativ operierten patienten nahezu derjenigen entspricht , deren tumoren primr bereits komplett reseziert werden konnten . 
mit 18% liegen wir in unserem krankengut im oberen drittel ; dies kann zum einen auf die kleine fallzahl , den reduzierten allgemeinzustand wie auch auf die tatsache , dass wir unsere patienten regelmig nach kardialen symptome fragten , zurckzufhren sebei vorliegen einer kardialen symptomatik wurde die chemotherapie bei den ersten patienten auf 5 - fu - bolusinfusion , spter auf ralitrexed umgestellt . 
daher verwenden wir ralitrexed jetzt als ersatz fr 5 - fu bei verdacht auf kardiale nebenwirkungen des 5 - fu . in der literatur lsst sich noch kein eindeutiger trend erkennen , ob sich durch eine properative radiochemotherapie die rate an funktionserhaltenden eingriffen erhhen lsst . 
sphincter preservation by the help of neoadjuvant radiochemotherapy . alle tumoren in den distalen 2 cm des rektums gelegen bei allen patienten klinisch abdominoperineale resektion erforderlich bei allen patienten klinisch abdominoperineale resektion erforderlich alle tumoren in den distalen 4 cm des rektums gelegen manchen autoren bis zu 86% betrgt , fanden hyams et al . [ 16 ] im rahmen der nsabp - studie , dass nur bei 27% der patienten die sphinkterfunktion erhalten werden konnte . dabei muss allerdings beachtet werden , dass in dieser analyse nur diejenigen patienten erfasst wurden , bei denen der operateur vor der randomisation zu der einschtzung kam , er msse diesen tumor bei einer primren operation exstirpieren . 
durch eine alleinige bestrahlung war die rate funktionserhaltender eingriffe mit 5 , 3% niedriger als bei einer simultanen radiochemotherapie mit 25% . eine kurzzeitvorbestrahlung ( zum beispiel mit 5 - mal 5 gy ) ist bei diesen fortgeschrittenen und zum teil sehr tief sitzenden tumoren nicht indiziert , denn eine ausreichende tumorrckbildung ( downstaging ) wird durch eine kurzzeitbestrahlung in der regel nicht erreicht . 
sowohl in der stockholm - ials auch in der stockholm - ii - studie war die rate der r0 - resektionen im properativ behandelten arm identisch mit derjenigen der allein operierten patienten [ 5 , 6 ]  . 
das tumoransprechen war bei lngerem intervall signifikant besser ( 71 , 17% nach sechs bis acht wochen versus 53 , 1% nach null bis zwei wochen , p = 0 , 007 )  . 
daher konnten auch wesentlich mehr patienten kontinenzerhaltend in der gruppe operiert werden , bei der das intervall zwischen sechs und acht wochen betrug ( 76% versus 68% , p = 0 , 27 )  . auch wenn die ersten ergebnisse der properativen simultanen radiochemotherapie erfreulich sind , denken wir , dass sowohl die rate an kontinenzerhaltenden eingriffen als auch die r0 - resektionsrate noch verbessert werden mssen . dabei darf nicht vergessen werden , dass wir hier im wesentlichen sehr weit fortgeschrittene tumoren mit entsprechend groen tumorvolumina behandelt haben . 
 [ 1 ] deuten auf eine dosis - effekt - beziehung hin : patienten mit prognostisch ungnstigen tumoren ( fixiert , tief ulzerierend , im distalen drittel des rektums liegend ) wurden mit 55 gy properativ bestrahlt ; ansonsten wurden 45 gy appliziert . 
trotz der niedrigeren tumorstadien traten in der mit 45 gy behandelten gruppe 20% ( 31 / 156 ) lokalrezidive im vergleich zu 6% ( 7 / 119 ) nach 55 gy auf . die von uns applizierte tumordosis gem icru betrug 53 , 5 gy , entspricht also in etwa der hheren dosis von ahmad et al . 
 da sich in der palliativen therapie des kolorektalen karzinoms neue substanzen ( irinotecan , oxaliplatin , ralitrexed , orale 5 - fu - derivate ) mit gutem erfolg etabliert haben , werden derzeit erste phase - ii - studien ( tabelle 5 ) mit diesen zytostatika durchgefhrt . 
die dabei erreichten pathohistologisch gesicherten kompletten remissionen sind zumindest erfolgversprechend . zusammenfassend besttigen die vorliegenden ergebnisse die empfehlungen der deutschen krebsgesellschaft , dass bei tumoren , die vom operateur primr als unsicher kurativ resezierbar angesehen werden , eine properative radiochemotherapie erfolgreich durchgefhrt werden kann . 
influence of the interval between preoperative radiation therapy and surgery on downstaging and on the rate of sphincter - sparing surgery for rectal - cancer : the lyon r 90 - 01 randomized trial . 
a clinical trial to evaluate the worth of preoperative multimodality therapy in patients with operable carcinoma of the rectum : a progress report of national surgical breast and bowel project protocol r - 03 . 
combined modality therapy of locally advanced or recurrent adenocarcinoma of the rectum : preliminary report of a phase i trial of chemotherapy ( ct ) with cpt - 11 , 5 - fu and concomitant irradiation ( rt )  . 
der zeitliche verlauf der anzahl der patienten im risiko wurde in etwa jeder zweiten arbeit mit aktuarischer auswertung ausreichend dokumentiert . schlussfolgerung : autoren , gutachter und herausgeber sollten zur hebung der qualitt der zeitschrift darauf achten , dass alle zeit - ereignis - daten aktuarisch ausgewertet werden . schlsselwrter : berlebensdaten zeit - ereignis - daten aktuarische auswertung qualittssicherung actuarial analysis of time - failure data and its relevance for interpretation of results . 
 audit of the journal strahlentherapie und onkologie background : the statistical quality of the contributions to strahlentherapie und onkologie is assessed , aiming for improvement of the journal and consequently its impact factor . material and methods : all 181 articles published during 1998 and 1999 in the categories review , original contribution , and short communication were analyzed concerning actuarial analysis of time - failure data . result : one hundred and twenty - three publications without time - failure data were excluded from analysis . 
the number of patients at risk during the course of follow - up was documented adequately in 22 of the 45 publications with actuarial analysis . conclusion : authors , peer reviewers , and editors could contribute to improve the quality of the journal by setting value on acturial analysis of time - failure data . key words : survival data time - failure data actuarial analysis audit 1 abteilung fr strahlentherapie und radio - onkologie , 2 institut fr biophysik und strahlenbiologie der universitt hamburg . 
zeit - ereignis - daten bei der beurteilung von resultaten b ei der auswertung klinischer forschungsergebnisse ist die anwendung adquater statistischer verfahren unabdingbare grundvoraussetzung fr eine korrekte interpretation der resultate . 
es ist geplant , diese bestandsaufnahme in etwa zwei jahren zu wiederholen , um qualitative vernderungen feststellen zu knnen . aktuarische auswertung von zeit - ereignis - daten fr aussagefhige klinische studien ist es oft notwendig , eine groe anzahl von patienten ber viele jahre hinweg nachzubeobachten . 
auch ohne diese hindernisse ist es praktisch unmglich , eine groe studie ohne informationslcken abzuschlieen . da die patienten nicht alle gleichzeitig in die studie eingebracht werden knnen , ist die nachbeobachtungszeit zwangslufig fr jeden patienten verschieden lang . 
diese probleme spielen gerade in der radioonkologie eine wichtige rolle , da die nachbeobachtungszeit im allgemeinen sehr lang ist und es sich berwiegend um ltere patienten handelt . wenn patienten , die aus der beobachtung fallen , bei der auswertung als geheilt oder komplikationsfrei gewertet werden , dann fllt das ergebnis besser aus , als es tatschlich ist , denn bei den nur kurzzeitig nachbeobachteten patienten ist die wahrscheinlichkeit fr die entwicklung von rezidiven oder sptnebenwirkungen gering . 
die nicht vollstndig nachbeobachteten patienten gar nicht mitzuzhlen ist aber auch nicht korrekt , denn je lnger ein patient rezidivoder komplikationsfrei bleibt , umso wahrscheinlicher wird es , dass er tatschlich erfolgreich behandelt wurde . die aktuarische analyse bietet einen ausweg aus diesem dilemma , da alle verfgbaren informationen bercksichtigt werden . die kaplan - meier - methode die kaplan - meier - methode [ 74 ] ( product limit method ) ist ein adquates verfahren , um die erwhnten probleme zu bercksichtigen . 
bei der aktuarischen auswertung der berlebensdauer wrden sie allerdings eine rolle spielen . bei der auswertung interessiert man sich nicht dafr , wann die behandlung stattgefunden hat , sondern wie lange nach beginn der behandlung ein ereignis eingetreten ist . 
die zahlen an der zeitachse wurden fr dieses beispiel willkrlich gewhlt , um eine auswertung nach kaplanmeier vornehmen zu knnen . aus den derart aufbereiteten daten kann tabelle 1 erstellt werden . 
mit den daten der tabelle 1 erfolgt dann die berechnung der aktuarischen komplikationsrate . bei der methode nach kaplan - meier wird die wahrscheinlichkeit , an einem bestimmten tag keine komplikation zu bekommen , folgendermaen aus den vorhandenen daten abgeschtzt : anzahl der an dem tag keine komplikationen zeigenden patienten anzahl der patienten in der beobachtung an dem tag wobei nur die an diesem tag noch unter beobachtung stehenden bzw . 
die berechnung muss nur fr die tage durchgefhrt werden , an denen ein ereignis eingetreten ist , denn an allen anderen tagen betrgt die wahrscheinlichkeit , den tag zu berleben , 100% . 
auf diese weise wird tabelle 2 erstellt . obwohl nur acht von elf patienten keine komplikationen aufwiesen , entsprechend einem anteil von 73% , betrgt nach aktuarischer auswertung der anteil der patienten ohne komplikationen lediglich 29% . 
durch die aktuarische analyse ergibt sich somit ein vllig anderes bild bei der beurteilung der behandlungsergebnisse . die ergebnisse der letzten spalte der tabelle 2 sind in abbildung 4 als treppenfunktion gegen die zeit aufgetragen . zeit nach behandlungsbeginn abbildung 3 . 
preparation of the data in figure 1 for actuarial analysis . jedem ereignis entspricht in dieser darstellung eine stufe . der vollstndigkeit halber sind fehlerbalken ( standardfehler ) eingezeichnet , auf deren berechnung hier nicht weiter eingegangen wird . am tag 44 nimmt mit dem ersten rezidiv die wahrscheinlichkeit fr komplikationsfreiheit um 1 / 8 = 12 , 5% auf 87 , 5% ab , weil zu diesem zeitpunkt acht patienten im risiko sind . die komplikation vom tag 84 reduziert die wahrscheinlichkeit erheblich strker , und zwar um 1 / 3 ( cid : 2 ) 87 , 5% = 29 , 2% auf 87 , 5% 29 , 2% = 58 , 3% , denn es sind nur noch drei patienten im risiko . 
ein einziger patient macht jetzt ein drittel des gesamten noch verbliebenen kollektivs aus . die kaplan - meier - methode bercksichtigt die informationen aller patienten genau so lange , wie sie jeweils beobachtet wurden . 
der spte teil der kaplan - meier - kurve sttzt sich auf eine immer kleiner werdende patientenanzahl und wird dadurch immer ungenauer . unterschiede zwischen kaplan - meier - kurven knnen mit verschiedenen statistischen verfahren verglichen werden . am verbreitetsten ist der log - rank - test . 
von der weiteren analyse wurden insgesamt 40 publikationen ausgeschlossen , davon 32 , bei denen keine quantitativen ergebnisse gezeigt werden , und acht , bei denen keine eigenen daten ausgewertet wurden [ 49 , 50 , 56 , 92 , 134 , 170 , 173 , 176 ]  . 
in ebenfalls elf arbeiten wurden die ergebnisse lediglich nicht aktuarisch ( crude ) ausgewertet [ 5 , 24 , 72 , 77 , 81 , 128 , 132 , 144 , 150 , 151 , 153 ]  . 
allerdings wurde in beiden fllen nicht eindeutig vermerkt , ob mit den zeitangaben die gesamte nachbeobachtungszeit oder die zeit bis zum auftreten des ereignisses gemeint ist . ber spte nebenwirkungen wird lediglich in 16 [ 16 , 22 , 30 , 31 , 38 , 40 , 63 , 6972 , 101 , 108 , 118 , 139 , 150 ] der 58 arbeiten quantitativ mit zeit - ereignis - daten berichtet ( 28% ; 95%konfidenzintervall : 16 bis 41% )  . 
nur drei [ 16 , 30 , 118 ] dieser 16 datenstze wurden aktuarisch ausgewertet , entsprechend einem anteil von 19% ( 95% - konfidenzintervall : 4 bis 46% )  . dieser anteil ist signifikant geringer als die oben ermittelten 78% ( p < 0 , 00001 )  . manahmen zur qualittsverbesserung es ist sehr erfreulich , dass zeit - ereignis - daten in der berwiegenden zahl der flle aktuarisch ausgewertet wurden . auffllig war jedoch die geringe anzahl an berichten ber spte nebenwirkungen , die dann auch noch alle , mit einer einzigen ausnahme , nicht aktuarisch ausgewertet wurden . 
a 2 - week pretreatment with 13 - cisretinoic acid + interferon - ( cid : 3 ) - 2a prior to definitive radiation improves tumor tissue oxygenation in cervical cancers . 
gadolinium - dtpa - konzentrations - zeit - kurven wurden vor , whrend und nach einem prolongierten bolus im arteriellen blut und im tumor erhoben und daraus der perfusionsindex ( pi ) berechnet . 
die anschlieende chirurgische resektion ermglichte eine pathologische klassifizierung und somit einen vergleich der perfusionsindexwerte mit dem therapieansprechen . ergebnisse : bei neun patienten konnte ein tumor - downstaging ( ypt02 ) ( gruppe 1 ) , bei fnf patienten kein tumordownstaging ( ypt3 ) ( gruppe 2 ) nachgewiesen werden . 
der bei therapieende erhobene mittlere perfusionsindexwert fr gruppe 1 ( n = 6 ) betrug 9 , 6 ml / min / 100 g ( 2 , 8 ) und fr gruppe 2 ( n = 4 ) 10 , 7 ml / min / 100 g ( 1 , 6 )  . hier konnte kein signifikanter unterschied nachgewiesen werden . schlussfolgerung : der perfusionsindexwert kombiniert zwei parameter : tumorperfusion und extraktionsfraktion . 
der berraschende negative einfluss hoher perfusionsindexwerte auf ein therapieansprechen kann somit mglicherweise durch einen hohen anteil an arealen hoher perfusion ( eventuell arteriovensen shunts ) mit niedriger extraktionsfraktion ( = minimaler stoffaustausch ) erklrt werden . 
da das tumorstadium einen signifikanten einfluss auf die tumorfreie berlebenszeit hat , knnte mglicherweise der perfusionsindexausgangswert als neuer prognosefaktor bei primren rektumkarzinomen ohne sphinkterinfiltration , die properativ mit einer kombinierten radiochemotherapie behandelt werden , zugezogen werden . 
zur berprfung dieser hypothese ist eine prospektive studie in vorbereitung . schlsselwrter : tumormikrozirkulation blutfluss dynamische mr - messungen rektumkarzinom properative strahlentherapie perfusionsindex prognosefaktor perfusions - index values evaluated by dynamic magnetic resonance imaging in advanced rectal carcinoma : a new predictor of response to preoperative chemoradiation ? purpose : the aim of our study was to evaluate in vivo the influence of tumor microcirculation data on therapy outcome . patients and methods : tumor perfusion data of primary rectal carcinoma ( n = 14 , ct3 ) who underwent preoperative chemoradiation have been analyzed ( table 1 )  . 
the perfusion data were acquired at the beginning and at the end of therapy by use of an ultrafast t1 - mapping sequence on a whole - body magnetic resonance imager . 
subsequent resection of the tumors allowed for a correlation of perfusion index values with the pathological classification . results : nine patients showed a t downstaging ( ypt02 , group 1 ) , 5 patients did not ( ypt3 , group 2 )  . 
the difference in perfusion index values after chemoradiation between group 1 and group 2 was not significant different ( table 2 )  . conclusion : our used perfusion index value combines 2 parameters : tumor perfusion and extraction fraction . 
to examine this hypotheses a prospective trial is in preparation . key words : tumor microcirculation blood flow dynamic mr imaging rectal carcinoma preoperative chemoradiation perfusion index prognostic factor d ie tumormikrozirkulation und ihr einfluss auf einen erhofften therapieerfolg stehen seit langem im zentrum des wissenschaftlichen interesses . 
so geht man davon aus , dass sie ein zentraler parameter fr die versorgung des tumors mit nhrund wirkstoffen ( zum beispiel sauerstoff , chemotherapeutika ) ist und damit direkt einen einfluss auf das ansprechen des tumors auf verschiedene therapieanstze hat [ 12 , 23 , 24 ]  . 
dass das therapieergebnis speziell bei der kombinierten radiochemotherapie abhngig vom sauerstoffgehalt und von der akkumulation des chemotherapeutikums ist , ist durch zahlreiche studien hinreichend belegt worden [ 6 , 16 , 21 ]  . bei der dynamischen magnetresonanz ( dmrt - ) und der dynamischen computertomographie ( dct ) wird zu verschiedenen zeitpunkten vor und nach kontrastmittelgabe in einem areal die kontrastmittelkonzentration gemessen . 
aus den erhaltenen daten lassen sich parameter berechnen , die aussagen ber die mikrozirkulation in diesem areal erlauben . bisher liegen nur wenige untersuchungen vor , die mittels dmrt oder dct erhobene mikrozirkulationsparameter mit einem therapieansprechen vergleichen . 
 [ 9 ] untersuchten bei hno - karzinom - patienten den primrtumor und / oder eine lymphknotenmetastase ; die tumoren befanden sich in unterschiedlichen t - stadien und wurden teilweise mit verschiedenen bestrahlungsgesamtdosen behandelt . gruppe von patienten mit einem primren rektumkarzinom im stadium ct3 an , die sich einer standardisierten properativen kombinierten radiochemotherapie unterzogen , und verglichen diese mit dem postoperativ gesicherten pathologischen ergebnis . patienten und methode zwischen oktober 1998 und februar 2000 wurden 14 patienten ( alter 38 bis 71 jahre , mittleres alter 54 , 1 jahre ) mit einem primren rektumkarzinom in diese untersuchung aufgenommen . 
von der untersuchung ausgeschlossen wurden patienten mit einem rektumkarzinom in den stadien ctx , t1 , t2 , t4 , malignittsgrad x , 1 , 3 oder 4 , metastatischer aussaat , infiltration des sphinkters , vorheriger operation und / oder strahlentherapie im abdominalbereich , vorheriger chemotherapie und patienten mit einem aktuellen oder frheren zweitmalignodas tumorstadium wurde mittels ultraschall erhoben . vor therapiebeginn zeigte jeder tumor eine infiltration in das perirektale fettgewebe und wurde laut uicc 1997 dem klinischen stadium t3 zugeordnet [ 11 ]  . 
der gruppe 2 , t - downstaging nein , wurden patienten , bei denen pathologisch weiterhin eine infiltration in das perirektale fettgewebe nachweisbar war , zugeteilt . therapieschema ziel der untersuchung um den einfluss von mikrozirkulationsdaten auf ein therapieansprechen zu untersuchen , wendeten wir eine krzlich publizierte dmrt - methode [ 3 , 4 ] bei einer homogenen jeder patient unterzog sich einer kombinierten hyperfraktionierten radiochemotherapie mit einer gesamtdosis zwischen 38 , 3 und 45 gy und einer einzeldosis von 1 , 1 gy zweimal pro tag . 
mr - perfusionsindexwerte beim rektumkarzinom patienten staging properativ ( gy ) staging postoperativ initiale pi - werte woche 4 pi - werte ( ml / min / 100 g ) ( ml / min / 100 g ) gruppe 1 gruppe 2 ct3n2m0 ct3n1m0 ct3n0m0 ct3n2m0 ct3n0m0 ct3n1m0 ct3n1m0 ct3n0m0 ct3n0m0 ct3n0m0 ct3n0m0 ct3n1m0 ct3n2m0 ct3n0m0 39 , 4 39 , 4 39 , 4 39 , 9 38 , 3 39 , 4 43 , 9 43 , 6 39 , 4 43 , 8 43 , 8 ypt2n1m0 ypt2n1m0 ypt2n2m0 ypt2n2m0 ypt0n0m0 ypt2n0m0 ypt2n0m0 ypt2n0m0 ypt2n0m0 ypt3n1m0 ypt3n0m0 ypt3n0m0 ypt3n1m0 ypt3n0m0 11 , 0 10 , 3 10 , 0 11 , 1 10 , 5 10 , 2 12 , 8 12 , 8 11 , 3 12 , 5 10 , 3 tabelle 1 . 
patients characteristics and evaluated pi - values ( before and at the end of treatment [ week 4 ] ; td = total dose )  . patient ber einen vorher implantierten zentralen katheter ( port - a - cath deltec cadd - 1 - system , pharmaciaupjohn ) 350 mg / m2 5 - fluorouracil kontinuierlich ber 24 stunden an jedem bestrahlungstag . 
alle patienten wurden innerhalb der dritten woche nach therapieende operiert . die rektumstudie wurde durch die rtliche ethikkommission genehmigt , alle patienten wurden ber die studie vollstndig aufgeklrt und erklrten freiwillig schriftlich ihr einverstndnis . methode zum erhalt der perfusionsparameter da die methode krzlich ausfhrlich vorgestellt wurde [ 3 , 4 ] , soll an dieser stelle nur kurz auf sie eingegangen werden . zum erhalt von reproduzierbaren konzentrations - zeitkurven wurde eine inversion - recovery - snapshot - flashsequenz an einem klinischen 1 , 5 - tesla - magnetresonanztomographen ( magnetom vision , siemens , germany ) installiert . 
 die transaxiale messschicht ( field of view [ fov ] : 30 cm , schichtdicke : 5 mm ) wurde so gewhlt , dass der tumor und die arteriellen gefe ( arteriae iliacae externae ) eindeutig auf den bildern identifiziert werden konnten . 
fr die dynamischen t1 - maps wurde eine kontrastmitteldosis von 0 , 05 mmol / kg gd - dtpa als prolongierter bolus mittels eines perfusors ber vier minuten ( flussrate : 90 bis 105 ml / stunde ) in die linke brachialvene injiziert . 
die gesamtuntersuchungszeit , inklusive lagerung und messschichtplanung , betrug ungefhr 15 minuten . anschlieend wurden messungen in den regions of interest ( roi ) im arteriellen blut und ber den gesamten tumor durchgefhrt und konzentrations - zeit - kurven berechnet . 
alle regionen wurden durch einen der autoren ( adv ) vor therapieende eingezeichnet . als erster schritt in richtung quantitativer auswertung wurde der perfusionsindex ( pi ) nach der formel pi = gk / ga [ 15 , 17 ] berechnet , wobei ga das maximum der arteriellen inputfunktion und gk die maximale steigung der organkurve ( tumorkurve ) sind . 
fr die berechnung von gk wurde an der stelle des steilsten anstiegs der organkurve eine lineare regressionsgerade durch mindestens neun datenpunkte ( vier punkte vor , vier punkte nach der stelle des steilsten anstiegs ) gelegt . die dmrt - untersuchung erfolgte vor therapiebeginn und in der letzten therapiewoche . 
bei fnf von 14 patienten konnte ein downstaging im tumorstadium nicht nachgewiesen werden ; diese wurden der t - downstaging - nein - gruppe ( gruppe 2 ) zugeordnet ( tabelle 1 )  . 
bei keinem patienten musste die therapie aufgrund von nebeneffekten > grad 2 nach rtog / eortc [ 13 ] abgebrochen werden . der mittlere perfusionsindexwert ( n = 14 ) bei therapiebeginn betrug 9 ml / min / 100 g ( 2 ) , fr gruppe 1 ( n = 9 ) 8 , 2 ml / min / 100 g und fr gruppe 2 ( n = 5 ) 10 , 4 ml / min / 100 g . 
weder die korrelationsanalyse noch der mann - whitney - test erbrachte signifikante werte ( tabelle 2 )  . diskussion im rahmen dieser untersuchung wurden perfusionsindexwerte vor beginn und am ende einer kombinierten hyperfraktionierten radiochemotherapie mittels dmrt erhoben . 
hnlich wie bei anderen stichprobenmethoden , wie zum beispiel der polarographischen sauerstoffmessung oder gewebebiopsien , ist dabei die zentrale frage , ob der umfang der stichprobe fr diesen schluss ausreichend ist . 
aus diesem grund sind auch verlaufsdaten eher mit vorsicht zu betrachten . in der diskussion der folgenden studien muss beachtet werden , dass hufig der begriff des kontrastmittel - uptakes gleichgesetzt wird mit perfusion , mikrozirkulation oder blutfluss . 
dabei wird auer acht gelassen , dass sich die kontrastmittelzunahme aus mindestens zwei parametern , der perfusion und der extravasation des kontrastmittels in das gewebe whrend der messung , zusammensetzt [ 2 , 7 ]  . 
sie konnten eine signifikante korrelation zwischen der lokalen tumorkontrolle und dem gemessenen grad der kontrastmittelzunahme ( rsi ) zu therapiebeginn ( p = 0 , 05 ) und nach ca . 
mr - perfusionsindexwerte beim rektumkarzinom tumorperfusion zu beginn und nach 20 gy ( rsi 2 , 8 ) eine bessere lokale tumorkontrolle als patientinnen mit einer niedrigeren tumorperfusion ( rsi < 2 , 8 )  . 
 [ 8 ] korrelierten ihre mittels dmrt - messungen erhobenen daten mit den berlebenszeiten von 37 patientinnen bei histologisch verifiziertem zervixkarzino bei 27 patientinnen bestand die chirurgische therapie in einer totalen hysterektomie , bei zehn patientinnen in einer evisceratio pelvis . 
die gruppe mit hohen si - u / s - werten hatte nach einer mittleren nachbeobachtungszeit von 24 monaten ( fnf bis 39 monate ) eine signifikant hhere berlebenswahrscheinlichkeit als die gruppe mit niedrigen si - u / s - werten . 
auch bei dieser publikation ist zu bedenken , dass es sich um eine heterogene gruppe bezglich stadien ( ib bis iva ) und therapie handelt . eine aufschlsselung der erhobenen werte nach figo - stadien wurde in beiden studien nicht vorgenommen . 
 [ 9 ] erhoben mittels dct bei 43 patienten mit hno - karzinomen unterschiedlicher entitten , stadien ( i bis iv ) und therapieschemata ( 55 gy oder 66 gy ) die perfusionsrate und korrelierten sie mit der lokalen tumorkontrolle . 
 [ 10 ] erhoben mittels dmrt bei 13 patienten mit einem oropharynxkarzinom ( t - stadien x , 3 und 4 ) , die entsprechend chart - protokoll therapiert wurden , die kontrastmittelzunahme ( e ) im tumor ( n = 5 ) oder in einem befallenen lymphknoten ( n = 7 )  . 
sie konnten einen signifikanten unterschied lokaler tumorkontrolle ( gruppe 1 ) versus keine lokale tumorkontrolle ( gruppe 2 ) der erhaltenen e - werte ( gruppe 1 0 , 67 0 , 04 versus gruppe 2 1 , 07 0 , 25 ) bei therapieende nachweisen ( p = 0 , 04 ) , der unterschied gruppe 1 ( e = 0 , 76 0 , 09 ) versus gruppe 2 ( e = 0 , 81 0 , 21 ) war bei therapiebeginn nicht signifikant . auch in diesen beiden publikationen erfolgte keine aufschlsselung der werte nach stadien , entitten oder verwendeten therapieschemata . 
 auf dem weg zwischen venser punktionsstelle und dem arteriellen zugang zum gewebe kommt es zu einer verzgerung und degradierung des injizierten kontrastmittelbolus . diese vernderungen sind im wesentlichen bedingt durch die passage durch das herz - lungen - system und hngen in ihrer ausprgung von der individuellen herz - kreislauf - situation des patienten ab . 
fr die verlssliche beurteilung der kontrastmittelkinetik im gewebe ist es deshalb mit von zentraler bedeutung , dass die konzentrations - zeit - kurve am arteriellen zugang zum gewebe , auch arterielle input - funktion genannt , bekannt ist . 
um diese mgliche fehlerquelle zu minimieren , wurde der perfusionsindex in unserer studie nach der formel pi = gk / ga [ 15 , 17 ] , somit unter mitbercksichtigung der arteriellen input - funktion ( ga = das maximum der arteriellen input - funktion ) berechnet . ein einfluss der blutzusammensetzung ( zum beispiel hmatokrit ) auf die perfusionsindexwerte konnte mittels der wchentlich durchgefhrten blutbildbestimmungen , die keine abweichungen von den normalwerten aufwiesen , ausgeschlossen werden . wir konnten aufzeigen , dass hohe perfusionsindexwerte bei therapiebeginn einen signifikanten negativen einfluss ( p = 0 , 012 ) , whrend niedrige perfusionsindexwerte einen signifikant positiven einfluss auf ein therapieansprechen haben . dagegen scheinen die perfusionsindexwerte bei therapieende keinen einfluss auf ein therapieansprechen zu haben . der perfusionsindexwert , unser verwendeter parameter , kombiniert zwei parameter zum erhalt der tumormikrozirkulation , die tumorperfusion und die extraktionsfraktion [ 2 , 7 ]  . 
so stellt sich die frage , ob sich der hohe perfusionsindexwert in der t - downstaging - nein - gruppe aus einem hohen anteil mit hoher perfusion und einem kleinen anteil mit extravasation zusammensetzt . 
dies wrde bedeuten , dass in dieser gruppe ein hoher anteil an arealen mit hoher perfusion vorhanden ist , was die vermutung zulsst , dass es sich hierbei um einen hohen anteil an arteriovensen shuntgefen handelt . 
dass in diesem fall nur ein minimaler austausch an stoffen in das umliegende gewebe stattfindet mit wahrscheinlich negativem einfluss auf das therapieergebnis , ist hinreichend bekannt [ 5 , 18 , 22 , 23 , 25 ]  . zur zeit ist uns keine methode bekannt , die es erlaubt , zwischen der reinen perfusion ( = blutfluss durch ein organ oder gewebe pro zeit und volumen ) und der extravasation des verwendeten kontrastmittels zu unterscheiden und somit die aufkommenden fragen zu beantworten . unseres erachtens deutet die literaturbersicht an , dass die tumormikrozirkulation und die neuen methoden zu ihrer in - vivo - erfassung mittels dynamischer mr einen wichtigen beitrag leisten knnen zur individualisierung der tumortherapie . 
die mediane nachbeobachtungszeit betrgt 189 tage ( streuung : 15 bis 548 tage )  . ergebnisse : akute nebenwirkungen waren : erhhte stuhlfrequenz ( 4 / 34 ) , abgespanntheit ( 2 / 34 ) , schmerzen in den leisten ( 1 / 34 ) , belkeit und perianales brennen ( 1 / 34 ) , schwindel ( 1 / 34 ) , leichter harnverhalt ( 1 / 34 )  . 
die klinischen tund n - kategorien ergaben 3 , 29 und 2 fr t4 , t3 und unbekannt und 20 , 11 und 3 fr n + , nund unbekannt . 
in einzelfllen wurde trotz des kurzen zeitintervalls bis zur operation ein downstaging erreicht . schlsselwrter : rektumkarzinom properative strahlentherapie nebenwirkungen short - term hypofractionated radiotherapy followed by total mesorectal excision purpose : is preoperative short - term radiotherapy of operable rectal carcinoma feasible with regard to early side effects and perioperative complications ? patients and methods : as of december 1996 to march 1999 , 34 patients with locally advanced rectal cancer have been irradiated preoperatively with 5 times 5 gy . 
the median follow - up period is 189 days ( range : 15 to 548 days )  . results : the following early side reactions were registered : increased bowel movements ( 4 / 34 ) , fatigue ( 2 / 34 ) , pain in the groins ( 1 / 34 ) , nausea and perianal smart ( 1 / 34 ) , vertigo ( 1 / 34 ) , temporary urinary obstruction ( 1 / 34 )  . 
preoperative t and n categories showed a distribution of 3 , 29 and 2 for t4 , t3 and unknown and 20 , 11 and 3 for n + , nand unknown ; postoperative t and n categories showed a distribution of 3 , 19 and 11 for t4 , t3 and t2 and 19 and 14 for n + and n -  . 
perioperative complications were : 2 cases of leaking anastomosis and postoperative bowel atonia , 1 case with bowel obstruction , delayed wound healing , wound dehiscence and temporary renal dysfunction . 
 conclusion : preoperative radiotherapy is feasible with moderate toxicity and is able to induce down staging despite the short time interval between radiotherapy and surgery . key words : rectal cancer preoperative radiotherapy side effects d ie radiochemotherapie des rektumkarzinoms gilt als behandlungsstandard und wird auerhalb von studien bei t4 - tumoren als properative manahme und bei tumoren der uicc - stadien ii und iii als postoperative adjuvansbehandlung empfohlen [ 15 ]  . 
da in der vergangenheit nach hypofraktionierung ber erhhte nebenwirkungsund operative komplikationsraten berichtet wurde [ 9 , 13 , 14 ] , erfolgte abweichend von der schwedischen studie die properative strahlentherapie ber kleine zielvolumina ohne komplette erfassung der iliakalen lymphabflusswege . ein weiterer unterschied besteht darin , dass bei der operation eine totale mesorektale exzision durchgefhrt wurde [ 6 ]  . 
dorsale felder der gre von 9 2 cm ( cid : 2 ) 11 , 5 2 , 4 cm sowie bilaterale opponierende felder einer mittleren gre von 9 1 , 5 cm ( cid : 2 ) 11 , 5 2 c die ct - untersuchung erfolgte in spiraltechnik mit 3mm - schichtdicke und einem 4 , 5 - mm - vorschub bei einem rekonstruktionsinkrement von 3 mm bei retrograder kontrastmittelfllung des rektums ( gastrografin )  . 
der sicherheitsabstand zwischen tumorrand und grenze des bestrahlungsfeldes betrug nach kranial und kaudal im mittel 2 cm und nach ventral ebenfalls 2 cder gesamte sakralkanal wurde dorsal in den seitlichen strahlengang einbezogen . 
die operation wurde im median 14 6 tage nach abschluss der bestrahlung durchgefhrt . parameter alter ( jahre ) geschlecht : weiblich ( n ) mnnlich ( n ) tumorlokalisation : unteres drittel mittleres drittel oberes drittel 66 ( 3387 ) maximaler initialer tumordurchmesser ( cm ) 5 ( 312 ) prtherapeutisches tumorstadium ( uicc ) : tabelle 1 . 
in 20 von 27 fllen ( 74% ) mit kontinenzerhaltender resektion entschloss man sich zur anlage eines protektiven anus praeter , welcher zwischenzeitlich bei 15 patienten nach drei bis sechs monaten zurckverlegt werden konnte . 
bei jedem zyklus wurden an fnf aufeinander folgenden tagen 500 mg / m2 krperoberflche 5 - fluorouracil im bolus appliziert . nebenwirkungen und nachsorge alle patienten wurden in dreimonatigen intervallen nachuntersucht . 
das intraoperative staging ergab in drei fllen eine viszerale metastasierung . komplikationen postoperative komplikationen sind in tabelle 4 aufgefhrt . schwerwiegende nebenwirkungen ( eortc - rtog - score > 3 ) an rektum , harnblase und haut wurden nicht gesehen . 
15 der 18 zytostatisch behandelten patienten tolerierten die chemotherapie problemlos . akuttoxizitt anzahl keine beschwerden stuhlfrequenz erhht mdigkeit , abgespanntheit ziehende schmerzen in beiden leisten belkeit und perianales brennen schwindel , kreislaufbeschwerden leichter harnverhalt myokardinfarkt mit letalem ausgang 21 tage post radiationem tabelle 2 . 
early side effects after preoperative radiotherapy of locally advanced rectal cancer until surgery ( n = 34 )  . klinische tumorausdehnung vor radiotherapie pathologische tumorausdehnung bei operation unbekannt ut3 nach pt2 ut4 nach pt3 ut3 nach pt4 ut gleich pt unbekannt unbekannt un + nach pn0 unnach pn + un gleich pn unbekannt tabelle 3 . 
tumor remission after preoperative radiotherapy of locally advanced rectal cancer ( n = 33 )  . anzahl keine komplikationen narbenhernie postoperative magen - / darmatonie anastomoseninsuffizienz konservativ beherrschbar relaparotomie hernierung der ersten jejunumschlinge in die bursa omentalis , tod nach relaparotomie im multiorganversagen postoperativ passagere niereninsuffizienz bei ureterstriktur wunddehiszenz ( klein ) wundheilungsstrung , operative revision 1 ( cid : 2 ) 1 ( cid : 2 ) tabelle 4 . 
kleinvolumige radiotherapie vor totaler mesorektaler exzision diskussion von spezialisierten zentren werden nach alleiniger totaler mesorektaler exzision bei hochrisikopatienten lokalrezidivraten von weniger als 10% berichtet [ 2 , 6 , 7 ]  . 
diese komplikation wird offensichtlich durch die kleinvolumige bestrahlung in einer dreioder vier - felder - technik vermieden . es traten bislang unter der kombinierten behandlung des rektumkarzinoms drei interkurrente todesflle auf ( myokardinfarkt , irinotecan - assoziierte kolitis mit sepsis , dnndarmhernierung in die bursa omentalis )  . 
in keinem fall ist ein zusammenhang mit der strahlentherapie zu erkennen . die dnndarmhernierung zeigte sich frh postoperativ als prolongierte und therapieresistente magenund darmatonie und fhrte nach relaparotomie zum tod im multiorganversagen . 
bei eingeschrnkter fallzahl unserer untersuchung ergibt sich durch die kleinvolumige properative radiotherapie keine zustzliche perioperative mortalitt . die reduktion des bestrahlungsvolumens im vergleich zum swedish rectal cancer trial ( 1997 ) ist dadurch begrndet , dass bei ungesichertem stellenwert adjuvanter verfahren bei totaler mesorektaler exzision akute lumbosakrale plexopathien vermieden werden mssen . 
die ergebnisse der randomisierten niederlndischen studie werden hierber aufschlsse geben . die kurzzeitvorbestrahlung in verbindung mit totaler mesorektaler exzision ist aufgrund der publizierten frhergebnisse der dutch colo rectal group [ 10 ] und unserer daten ein sicheres und gut vertrgliches verfahren . 
 neben den prund postoperativen laufenden studienprotokollen der eortc ( 22921 ) und der aro ( 95 - 1 ) sowie postoperativer radio - / chemotherapie gem cao / aio / aro - konsensus ( 1998 ) ist die kleinvolumige kurzzeitvorbestrahlung als weitere behandlungsoption vor totaler mesorektaler exzision mglich . 
four arm phase iii clinical trial for t3t4 resectable rectal cancer comparing pre - operative pelvic irradiation to pre - operative irradiation combined with fluoruracil and leucoverin with or without postoperative adjuvant chemotherapy . 
the purpose of this analysis was to assess current knowledge , with focus on correlation with radiation dose , irradiated volume and age . method : full scale iq ( fsiq ) data , representing 1 , 938 children , were derived from 36 publications and analyzed as to radiation dose , irradiated volume , and age . results : fsiq after whole brain irradiation showed a non - linear decline as dosage increased . 
fsiq test results below the normal level ( < 85 ) were found at doses higher than 24 and 36 gy in children under age 3 , and older than age 6 , respectively . 
mean fsiq test result after 18 gy was 100 , thus at the mean standard value ; a minor decline was detectable only when compared to test results of a control group . 
partial brain irradiation caused minor fsiq decline , with measurable effects at dose levels > 50 gy . conclusion : the collected data suggest that whole brain irradiation doses of 18 and 24 gy have no major impact on intellectual outcome in children older than age 6 , but may cause impairment in younger children . 
thus , further research is required to evaluate the effect of low - dose whole brain irradiation as well as partial brain irradiation on fsiq development . key words : children radiation therapy brain cognitive function full scale iq full - scale - iq - ( fsiq - ) vernderungen nach ganzund teilhirnbestrahlung des kindlichen gehirns . 
diese arbeit bestimmt den momentanen wissensstand und analysiert kausale zusammenhnge von bestrahlungsdosis , bestrahltem volumen und dem alter der kinder zur zeit der bestrahlung . methode : aus 36 englischsprachigen publikationen wurden full - scale - iq - ( fsiq - ) daten von 1 936 kindern gewonnen und bezglich bestrahlungsdosis , bestrahltem volumen und dem alter der kinder analysiert . ergebnisse : die fsiq - werte fielen nicht linear mit steigenden bestrahlungsdosen ab ( abbildungen 1 und 2 )  . 
bei kindern unter drei jahren lagen die testergebnisse nach 24 gy ganzhirnbestrahlung unterhalb des normalwertbereichs ( fsiq 90 bis 110 ) , wohingegen die werte bei kindern ber sechs jahren erst nach 36 gy im selben mae abfielen . 
der mittlere testwert nach 18 gy ganzhirnbestrahlung lag bei 100 ; das bedeutet , auf dem standardisierten mittelwert der fsiqtests war nur ein geringer abfall der testwerte im vergleich zur ebenfalls getesteten kontrollgruppe ( mittelwert 104 ) zu erheben ( tabelle 1 )  . 
kleine kinder wurden nach 18 gy ganzhirnbestrahlung im niedrig normalen bereich getestet . teilhirnbestrahlungen verursachten geringe abflle der fsiq - testwerte nach gesamtdosen > 50 gy . schlussfolgerung : die gesammelten daten zeigen , dass ganzhirndosen von 18 und 24 gy keinen oder nur einen geringen einfluss auf die intellektuelle entwicklung von kindern ber sechs jahren haben . 
full scale iq ( fsiq ) after cranial irradiation limitationen auf und weisen auf mgliche interpretationsfehler hweitere testungen und prospektive studien sind erforderlich , um den einfluss niedriger dosen in der ganzhirnbestrahlung sicherer bestimmen zu knnen . 
der erwartete normalgewebsschonende effekt zunehmend eingesetzter 3 - d - geplanter teilhirnbestrahlungen sollte bezglich der entwicklung der kognitiven leistungsfhigkeit dokumentiert werden . schlsselwrter : ganzhirnbestrahlung teilhirnbestrahlung kinder full - scale - iq kognitive funktionen gehirn a s modern therapy regimens improve long - term survival rates for childhood cancer , long - term sequelae relating to such treatment has become an important field of research in recent years . 
numerous investigations have resulted in controversial findings , ranging from direct attribution to radiation of severe detriment of neuropsychological functioning , to lack of causal relationship between radiation therapy and central nervous system complications [ 22 ]  . 
 in recent years 2 reviews have attempted to address this problems by integrating data from several studies so as to gain sufficient numbers of patients for multivariate analysis [ 6 , 31 ]  . 
a more recent review [ 38 ] suggested that whole brain irradiation doses of 18 to 24 gy result in mild intellectual deficit and that it may be more deleterious than local irradiation . 
accompanying factors such as sex , tumor type and location , combined treatment modalities , and psychosocial factors have been found to contribute to radiation induced sequelae [ 37 , 39 , 44 , 45 ]  . studies focusing on iq deficit following partial brain radiation are rare , but of high interest . 
modern radiation treatment concepts for localized brain tumors intend to spare healthy normal brain tissue by conforming radiation doses to the tumor outline and are expected to reduce the rate of treatment associated sequelae . 
 normal tissue complication probabilities correlate highly with dose distribution , and several mathematical models have been developed to calculate values that offer additional information for decision - making and treatment selection . empirical clinical data with well - accepted radiation dose to volume relationship are available for a variety of endpoints , such as functional loss and necrosis for many organs [ 1 , 10 ]  . however , the current lack of data in terms of intellectual functioning after radiation therapy to the childs brain , handicaps the physicians ability to estimate or calculate the probability of possible cognitive deficits . the influence of methotrexate ( mtx ) therapy with or without radiation therapy . 
in order to permit estimation of normal tissue complication probabilities we tried to establish a data - base that allows modeled calculation of fsiq change after whole brain irradiation and partial brain irradiation , dependent on dose and irradiated volume . methods we identified 36 publications written in english language providing information of fsiq in relation to radiation doses prescribed for whole brain and / or partial brain irradiation . these data constituted the basis of this analysis and included 1 , 938 children . 
a minimum follow - up of 3 years was reported by 30 publications ; 6 reports provided data based on an observation period of minimum 1 year and up to 3 years . we excluded reports that did not report one or both of the following : absolute , mean or median fsiq data , radiation dose prescribed in cgy or gy . 
studies with a follow - up shorter than 1 year were excluded from this analysis . data basis for fsiq development after whole brain irradiation of the 36 publications reviewed 33 [ 25 , 8 , 9 , 1117 , 19 , 20 , 23 , 2530 , 32 , 34 , 35 , 37 , 39 , 40 , 4345 ] specifically reported fsiq values ( absolute , mean , or median ) with respect to dose following whole brain irradiation . 
publications reporting changes of fsiq but without reproducible documentation of radiation dose delivered were excluded from this analysis . age - at - treatment was derived from 16 publications [ 8 , 9 , 13 , 1517 , 19 , 23 , 2729 , 35 , 37 , 39 ]  . 
although most publications reported on age - dependent treatment effects , not every study provided data reflecting the chosen age ranges in this study . data basis for fsiq after partial brain irradiation this study reviewed literature on intellectual functioning following whole brain and partial brain irradiation with regard to full scale iq ( fsiq ) in order to collect data and report the status of current knowledge . 
however , the clear attribution of the children to the prescribed doses , suggested this classification . the primary tumors in the cases studied were mostly astrocytoma or glioma ( n = 62 ) and pituitary or parasellar tumors ( n = 59 )  . 
using this statistical method , however , prohibited the calculation of standard error or standard deviation as usually not all base data for each child tested was provided in a report . 
the intend of this present review was a comprehensive yet basically simple display of dose effects on outcome in terms of fsiq test scores in children following cranial radiation therapy . data calculation of normal tissue complication probabilities assuming that fsiq drop after radiation therapy below a certain level may indicate a critical dose for the occurrence of late side effects , the td5 and td50 for children with fsiq < 90 and < 80 can be calculated . 
 [ 33 ] the complication probability can be calculated by fitting the slope parameter m and the volume parameter n . results control groups control groups and baseline values several groups of children who received no cranial radiation therapy were identified as controls . 
in addition , a third control group consisting of healthy children , such as siblings or normal population , was included for evaluation of non - radiation related fsiq changes . 
in table 1 each of these groups is classified as to number of children , baseline results , and tumor type or healthy . data management data sheets were coded for each study with the following parameters : number of children ; radiation dose and , if available , error of the dose and dose range ; absolute , mean or median fsiq with standard deviation and range ; fsiq drop ; percentage of children with fsiq < 90 and < 80 ; evaluation of other iq qualities ; specification for control groups ; age , error in age ; tumor specification and combined mtx therapy . 
the data were evaluated in 3 groups : children with malignant diseases of the central nervous system ( glioma ) , those with acute lymphoblastic leukemia , and those with extracranial malignant diseases ( non - central nervous system ) after appropriate treatment . 
fsiq : full scale iq , wbi : ganzhirnbestrahlung , pbi : teilhirnbestrahlung . 12 18 24 30 36 42 48 54 60 66 72 dose [ gy ] radiation doses after whole brain and partial brain irradiation are summarized in table 1 . 
 [ 20 ] are displayed separately , since they represent children treated 2 times with whole brain irradiation , first as prophylactic treatment ( 24 gy ) and again after diagnosis of recurrent disease ( 30 gy )  . 
 [ 41 ] , who developed a model of fsiq decline after doses of 18 gy , 24 gy , and 36 gy whole brain irradiation , according to age . 
the linear fsiq decline for age 2 , age 4 , age 6 , age 8 , and age 10 is plotted , as predicted by the model . however , data collected for the present review suggest a non - linear decline of fsiq after whole brain irradiation with more pronounced dose effects for the group of younger children ( < 3 years , and 3 to 6 years ) , but substantial decline at higher dose levels for older children ( > 6 years ) as well . whole group resulted in comparable fsiq decline dependent on whole brain irradiation dose as in the whole evaluated population . 
no report provided data for age analysis according to our requirement . percentage of children tested with fsiq < 90 , and < 80 a gauss bell - shaped plot of normal distribution of fsiq shows certain percentages of the normal population below the expected mean value of 100 . 
based on this slope and the baseline of 25% and 8.9% for healthy children with fsiq < 90 and < 80% , respectively , the dose causing 50% probability for fsiq below defined threshold value can be estimated . according to the evaluated data and the calculated slope we suggest a 50% probability at 30 gy whole brain irradiation for fsiq < 90 and at 38.5 gy whole brain irradiation for fsiq < 80 . 
the estimated error for the slope within the respective dose limits is assumed not to exceed 10% . estimation of 5% increase of percentage of fsiq < 90 and < 80 is far more uncertain since the data do not suggest a linear relationship between increase of whole brain irradiation dose and fsiq decline at these points . 
coarse approximation indicates a dose of about 22.5 gy whole brain irradiation to increase the percentage of children below fsiq 90 by 5% and 26 gy for fsiq < 80 . 
in addition discrete or mean percentages of children below age 3 are plotted which were tested with an fsiq < 90 ; the vast majority of these data points are distributed above the fsiq < 90 curve , thus indicating that this subgroup is at even higher susceptibility for radiation induced fsiq drop . 
further evaluation for age relationship to percentages below given threshold values was limited by lack of reported data . for comparison , the percentage of children below given fsiq values after partial brain irradiation was plotted in figure 3 indicating a minor fsiq decline at substantial higher doses when compared to whole brain irradiation . approximation of normal tissue complication probabilities derived from data contributing to figure 3 the 5% and 50% increase of percentage of children below defined fsiq values following whole brain irradiation can be approximated . 
for comparison , display of percentage of children < 3 years with fsiq < 90 after whole brain irradiation and percentage of children after partial brain irradiation with fsiq < 90 and < 80 . 
full scale iq ( fsiq ) after cranial irradiation influence of mtx administration with and without whole brain irradiation the influence of mtx effects in combination with radiation therapy could not be evaluated in this study , since at the 18 , 24 , and 36 gy dose level nearly all children received a combined therapy regimen , with only a limited number of children known to have undergone radiation therapy without combination with any form of mtx therapy . 
the majority of studies provides data concerning fsiq , some report other iq data , such as performance iq ( piq ) or verbal iq ( viq ) , as well . 
not all of these iq may be found similar impaired after radiation therapy . other functional qualities , such as memory and attention may well be deficient without significant expression in other test scores . 
thus , focus of this review on fsiq was given by the broad data basis and the fact that fsiq represents a general assessment of intellectual functioning with defined mean value and standard distribution of test values in the normal population . 
whereas these authors found a correlation between irradiated volume ( whole brain irradiation vs partial brain irradiation ) and decline in fsiq , no analysis in regard to radiation doses was provided . the present review analyzed fsiq development after whole brain and partial brain irradiation . 
analysis of 36 studies and more than 1 , 900 children showed a clear correlation between test results and radiation dose and volume . in the whole group of children , the mean fsiq after 18 and 24 gy whole brain irradiation was within the normal range . at doses higher than 24 gy a negative correlation with increasing doses was found . 
their model assumed a patient with an initial score of 100 and whole brain irradiation treatment with 18 , 24 , and 36 gy at ages from 2 to 10 and predicts a linear decrease with increasing dose . 
for the younger children ( less than age 6 ) the estimated value at 18 and 24 gy from the model and our compiled data almost overlap , but at higher doses the documented decline exceeds by far the prediction of the model . 
evaluation of the control groups in the present review found the whole group as well as all subgroups at fsiq levels of about 104 . no significant difference was found between healthy children and children with brain tumors or acute lymphoblastic leukemia , either before or after undergoing sufficient treatment but without radiation therapy . the definition of 100 as the baseline for calculation of fsiq drop and as the starting point of the curves may be controversial , but to ensure comparability of all collected data we decided to use the standardized mean value of all iq tests . however , this may have consequences if a drop is calculated in the collected data , with possible underestimation of detrimental effects , this with special respect to fsiq impairment following a whole brain irradiation dose of 18 gy . 
the wmfsiq in this review of 100.0 points was exactly as high as the expected mean value in a normal population , but 4.2 points lower than the mean score of all control groups . therefore , a minor effect of radiation therapy with 18 gy could not be excluded with certainty . the influence of the findings and interpretation of a single study on possible discrete drop in cognitive functioning following whole brain irradiation with 18 gy in this review may be documented . 
a recent longitudinal study [ 14 ] evaluated 129 children with acute lymphoblastic leukemia following 18 gy whole brain irradiation in combination with mtx containing chemotherapy in comparison to a second group of 74 children which were only treated with intravenous and intrathecal mtx . 
after a follow - up of more than 7 years , the irradiated children scored with a mean fsiq of 95 , compared to 104.5 in children treated with chemotherapy alone . 
as the mean follow - up of all children ranged between 6.4 years ( 18 gy ) and 5.8 years ( chemo ) only a subgroup of children can have contributed to this last test value . 
it would have been of great interest to compare the latest test results of the subgroup with longest follow - up with their own initial score . this documents a common dilemma ; test results at different times after therapy and from different subgroups may lead to significantly different conclusions . 
 [ 20 ] provide in their study data for intellectual outcome after 2 courses of whole brain irradiation with initial doses of 24 gy and additional doses of 30 gy at the time of recurrent disease . 
although the authors did not report the time gap between the 2 whole brain irradiation treatment courses this seems to demonstrate a splitcourse effect with considerable reduction of expected fsiq detriment . 
this may confirm the hypothesis that hyperfractionation can reduce functional detriment . tumor localization and histology can have a major impact on fsiq following partial brain irradiation with substantial impairment in children with hypothalamic tumor extension [ 18 ] and tumors of the parapituitary region [ 15 ]  . 
fsiq test results are undoubtedly associated with factors , such as hydrocephalus [ 15 , 18 ] , extend and number of surgeries [ 3 ] , and degree of neurological deficit and disability [ 18 , 28 ]  . 
overall , the paucity of current data on cognitive functioning following partial brain irradiation does not allow definitive conclusions regarding dose - effect relationship . phylaxis , yet can safely avoid normal tissue complications , precise knowledge of tumoricidal dose and tolerance doses of normal tissue is required . 
calculation of normal tissue complication probabilities ( ntcp ) offers an additional estimate of the increase of risk for the occurrence of deterministic and therefore doseand / or volume - dependent radiation induced sequelae . 
typically , an increase in risk of 5% and 50% for a follow - up time of 5 years is calculated . the data for td5 / td50 were approximated from curves derived from data of several publications . 
data contributing to this estimation are quite inhomogeneous ; children with whole brain irradiation doses up to 30 gy have mostly been treated for acute lymphoblastic leukemia , at higher doses the leading diagnosis was medulloblastoma . 
we could not account for the influence , and thus possible immanent errors , of primary tumor and cofactors such as surgery , combined toxicity of chemotherapy and effects caused by different daily fractionation regimens . 
we tried to account for the age at treatment as an important factor by excluding the children younger than age 3 for this approximation ; still the data reflect a wide age - range at the time of treatment . thus , an average effect of whole brain irradiation on rate of children with post - treatment fsiq < 90 and < 80 points has been estimated . 
approximation of this value risk had an even higher degree of uncertainty , with doses of 22.5 gy and 26 gy possibly causing a 5% increase of children with an fsiq < 90 , and < 80 , respectively . to our knowledge , miralbell et al . 
this would suggest a substantially minor steep dose - effect relationship than observed in the present evaluation where about 90% of reported children were tested below 90 points at this high dose level . 
full scale iq ( fsiq ) after cranial irradiation based on complication endpoints , such as necrosis which usually do not occur in a normal population there is no need for this discrimination . 
calculation for 50% new events would result in slightly higher dose levels . increase of percentage of children with test results < 90 and < 80 points was also documented after localized cranial irradiation . 
the only reliable conclusion based on current data is that there is an increase in the percentage of children with fsiq < 90 and < 80 following local cranial irradiation , whereas , although , far less pronounced as expected after comparable whole brain irradiation doses . 
the link of dose and its effects at conventionally fractionated doses higher than 54 gy remains yet unclear ; also if this function may be linear or non - linear . conclusion the intent of the present study was to improve knowledge of the causal correlation of cranial radiation therapy and intellectual development . 
the collected data suggest that whole brain irradiation doses of 18 to 24 gy cause no major impairment of intellectual development in children older than age 6 , but may be already correlated to an impairment in children younger than age 3 . 
several limitations , such as inhomogeneous primary tumors , influence of cofactors and treatment parameters as well as the criteria to collect and analyze the data might initiate critical discussion . thus , we support suggestions by others of a standardized test design with evaluation of various , comparable essential data , such as fsiq , piq , and viq . 
including them might have influenced our conclusions . in order to detect a possible effect following whole brain irradiation with 18 gy , further data collection is required . baseline testing in form of a prospective study design is required to clarify if the small fsiq decline compared to fsiq of the control group , as found in this review , represents a reproducible effect . 
whole brain irradiation with 18 gy is currently recommended as standard dose in the prophylactic treatment of children with high - risk acute lymphoblastic leukemia ( wbc count > 25 , 000 ) and the rationale to exclude cranial radiation therapy in the prophylaxis for acute lymphoblastic leukemia is based on the studies reporting intellectual detriment . 
reevaluation of the large group of children treated with whole brain irradiation doses > 36 gy in the past , and now with significant long - term follow - up , could provide essential , additional information , as inhomogeneous data situation at this dose level requires further research . acknowledgement : the authors wish to thank john o . 
a. , for his assistance in the preparation of the manuscript . strahlentherapie und onkologie urban & vogel 2000 originalarbeit full scale iq ( fsiq ) changes in children treated with whole brain and partial brain irradiation a review and analysis martin fuss1 , karin poljanc2 , eugen b . 
the purpose of this analysis was to assess current knowledge , with focus on correlation with radiation dose , irradiated volume and age . method : full scale iq ( fsiq ) data , representing 1 , 938 children , were derived from 36 publications and analyzed as to radiation dose , irradiated volume , and age . results : fsiq after whole brain irradiation showed a non - linear decline as dosage increased . 
fsiq test results below the normal level ( < 85 ) were found at doses higher than 24 and 36 gy in children under age 3 , and older than age 6 , respectively . 
mean fsiq test result after 18 gy was 100 , thus at the mean standard value ; a minor decline was detectable only when compared to test results of a control group . 
partial brain irradiation caused minor fsiq decline , with measurable effects at dose levels > 50 gy . conclusion : the collected data suggest that whole brain irradiation doses of 18 and 24 gy have no major impact on intellectual outcome in children older than age 6 , but may cause impairment in younger children . 
thus , further research is required to evaluate the effect of low - dose whole brain irradiation as well as partial brain irradiation on fsiq development . key words : children radiation therapy brain cognitive function full scale iq full - scale - iq - ( fsiq - ) vernderungen nach ganzund teilhirnbestrahlung des kindlichen gehirns . 
diese arbeit bestimmt den momentanen wissensstand und analysiert kausale zusammenhnge von bestrahlungsdosis , bestrahltem volumen und dem alter der kinder zur zeit der bestrahlung . methode : aus 36 englischsprachigen publikationen wurden full - scale - iq - ( fsiq - ) daten von 1 936 kindern gewonnen und bezglich bestrahlungsdosis , bestrahltem volumen und dem alter der kinder analysiert . ergebnisse : die fsiq - werte fielen nicht linear mit steigenden bestrahlungsdosen ab ( abbildungen 1 und 2 )  . 
bei kindern unter drei jahren lagen die testergebnisse nach 24 gy ganzhirnbestrahlung unterhalb des normalwertbereichs ( fsiq 90 bis 110 ) , wohingegen die werte bei kindern ber sechs jahren erst nach 36 gy im selben mae abfielen . 
der mittlere testwert nach 18 gy ganzhirnbestrahlung lag bei 100 ; das bedeutet , auf dem standardisierten mittelwert der fsiqtests war nur ein geringer abfall der testwerte im vergleich zur ebenfalls getesteten kontrollgruppe ( mittelwert 104 ) zu erheben ( tabelle 1 )  . 
kleine kinder wurden nach 18 gy ganzhirnbestrahlung im niedrig normalen bereich getestet . teilhirnbestrahlungen verursachten geringe abflle der fsiq - testwerte nach gesamtdosen > 50 gy . schlussfolgerung : die gesammelten daten zeigen , dass ganzhirndosen von 18 und 24 gy keinen oder nur einen geringen einfluss auf die intellektuelle entwicklung von kindern ber sechs jahren haben . 
full scale iq ( fsiq ) after cranial irradiation limitationen auf und weisen auf mgliche interpretationsfehler hweitere testungen und prospektive studien sind erforderlich , um den einfluss niedriger dosen in der ganzhirnbestrahlung sicherer bestimmen zu knnen . 
der erwartete normalgewebsschonende effekt zunehmend eingesetzter 3 - d - geplanter teilhirnbestrahlungen sollte bezglich der entwicklung der kognitiven leistungsfhigkeit dokumentiert werden . schlsselwrter : ganzhirnbestrahlung teilhirnbestrahlung kinder full - scale - iq kognitive funktionen gehirn a s modern therapy regimens improve long - term survival rates for childhood cancer , long - term sequelae relating to such treatment has become an important field of research in recent years . 
numerous investigations have resulted in controversial findings , ranging from direct attribution to radiation of severe detriment of neuropsychological functioning , to lack of causal relationship between radiation therapy and central nervous system complications [ 22 ]  . 
 in recent years 2 reviews have attempted to address this problems by integrating data from several studies so as to gain sufficient numbers of patients for multivariate analysis [ 6 , 31 ]  . 
a more recent review [ 38 ] suggested that whole brain irradiation doses of 18 to 24 gy result in mild intellectual deficit and that it may be more deleterious than local irradiation . 
accompanying factors such as sex , tumor type and location , combined treatment modalities , and psychosocial factors have been found to contribute to radiation induced sequelae [ 37 , 39 , 44 , 45 ]  . studies focusing on iq deficit following partial brain radiation are rare , but of high interest . 
modern radiation treatment concepts for localized brain tumors intend to spare healthy normal brain tissue by conforming radiation doses to the tumor outline and are expected to reduce the rate of treatment associated sequelae . 
 normal tissue complication probabilities correlate highly with dose distribution , and several mathematical models have been developed to calculate values that offer additional information for decision - making and treatment selection . empirical clinical data with well - accepted radiation dose to volume relationship are available for a variety of endpoints , such as functional loss and necrosis for many organs [ 1 , 10 ]  . however , the current lack of data in terms of intellectual functioning after radiation therapy to the childs brain , handicaps the physicians ability to estimate or calculate the probability of possible cognitive deficits . the influence of methotrexate ( mtx ) therapy with or without radiation therapy . 
in order to permit estimation of normal tissue complication probabilities we tried to establish a data - base that allows modeled calculation of fsiq change after whole brain irradiation and partial brain irradiation , dependent on dose and irradiated volume . methods we identified 36 publications written in english language providing information of fsiq in relation to radiation doses prescribed for whole brain and / or partial brain irradiation . these data constituted the basis of this analysis and included 1 , 938 children . 
a minimum follow - up of 3 years was reported by 30 publications ; 6 reports provided data based on an observation period of minimum 1 year and up to 3 years . we excluded reports that did not report one or both of the following : absolute , mean or median fsiq data , radiation dose prescribed in cgy or gy . 
studies with a follow - up shorter than 1 year were excluded from this analysis . data basis for fsiq development after whole brain irradiation of the 36 publications reviewed 33 [ 25 , 8 , 9 , 1117 , 19 , 20 , 23 , 2530 , 32 , 34 , 35 , 37 , 39 , 40 , 4345 ] specifically reported fsiq values ( absolute , mean , or median ) with respect to dose following whole brain irradiation . 
publications reporting changes of fsiq but without reproducible documentation of radiation dose delivered were excluded from this analysis . age - at - treatment was derived from 16 publications [ 8 , 9 , 13 , 1517 , 19 , 23 , 2729 , 35 , 37 , 39 ]  . 
although most publications reported on age - dependent treatment effects , not every study provided data reflecting the chosen age ranges in this study . data basis for fsiq after partial brain irradiation this study reviewed literature on intellectual functioning following whole brain and partial brain irradiation with regard to full scale iq ( fsiq ) in order to collect data and report the status of current knowledge . 
however , the clear attribution of the children to the prescribed doses , suggested this classification . the primary tumors in the cases studied were mostly astrocytoma or glioma ( n = 62 ) and pituitary or parasellar tumors ( n = 59 )  . 
using this statistical method , however , prohibited the calculation of standard error or standard deviation as usually not all base data for each child tested was provided in a report . 
the intend of this present review was a comprehensive yet basically simple display of dose effects on outcome in terms of fsiq test scores in children following cranial radiation therapy . data calculation of normal tissue complication probabilities assuming that fsiq drop after radiation therapy below a certain level may indicate a critical dose for the occurrence of late side effects , the td5 and td50 for children with fsiq < 90 and < 80 can be calculated . 
 [ 33 ] the complication probability can be calculated by fitting the slope parameter m and the volume parameter n . results control groups control groups and baseline values several groups of children who received no cranial radiation therapy were identified as controls . 
in addition , a third control group consisting of healthy children , such as siblings or normal population , was included for evaluation of non - radiation related fsiq changes . 
in table 1 each of these groups is classified as to number of children , baseline results , and tumor type or healthy . data management data sheets were coded for each study with the following parameters : number of children ; radiation dose and , if available , error of the dose and dose range ; absolute , mean or median fsiq with standard deviation and range ; fsiq drop ; percentage of children with fsiq < 90 and < 80 ; evaluation of other iq qualities ; specification for control groups ; age , error in age ; tumor specification and combined mtx therapy . 
the data were evaluated in 3 groups : children with malignant diseases of the central nervous system ( glioma ) , those with acute lymphoblastic leukemia , and those with extracranial malignant diseases ( non - central nervous system ) after appropriate treatment . 
fsiq : full scale iq , wbi : ganzhirnbestrahlung , pbi : teilhirnbestrahlung . 12 18 24 30 36 42 48 54 60 66 72 dose [ gy ] radiation doses after whole brain and partial brain irradiation are summarized in table 1 . 
 [ 20 ] are displayed separately , since they represent children treated 2 times with whole brain irradiation , first as prophylactic treatment ( 24 gy ) and again after diagnosis of recurrent disease ( 30 gy )  . 
 [ 41 ] , who developed a model of fsiq decline after doses of 18 gy , 24 gy , and 36 gy whole brain irradiation , according to age . 
the linear fsiq decline for age 2 , age 4 , age 6 , age 8 , and age 10 is plotted , as predicted by the model . however , data collected for the present review suggest a non - linear decline of fsiq after whole brain irradiation with more pronounced dose effects for the group of younger children ( < 3 years , and 3 to 6 years ) , but substantial decline at higher dose levels for older children ( > 6 years ) as well . whole group resulted in comparable fsiq decline dependent on whole brain irradiation dose as in the whole evaluated population . 
no report provided data for age analysis according to our requirement . percentage of children tested with fsiq < 90 , and < 80 a gauss bell - shaped plot of normal distribution of fsiq shows certain percentages of the normal population below the expected mean value of 100 . 
based on this slope and the baseline of 25% and 8.9% for healthy children with fsiq < 90 and < 80% , respectively , the dose causing 50% probability for fsiq below defined threshold value can be estimated . according to the evaluated data and the calculated slope we suggest a 50% probability at 30 gy whole brain irradiation for fsiq < 90 and at 38.5 gy whole brain irradiation for fsiq < 80 . 
the estimated error for the slope within the respective dose limits is assumed not to exceed 10% . estimation of 5% increase of percentage of fsiq < 90 and < 80 is far more uncertain since the data do not suggest a linear relationship between increase of whole brain irradiation dose and fsiq decline at these points . 
coarse approximation indicates a dose of about 22.5 gy whole brain irradiation to increase the percentage of children below fsiq 90 by 5% and 26 gy for fsiq < 80 . 
in addition discrete or mean percentages of children below age 3 are plotted which were tested with an fsiq < 90 ; the vast majority of these data points are distributed above the fsiq < 90 curve , thus indicating that this subgroup is at even higher susceptibility for radiation induced fsiq drop . 
further evaluation for age relationship to percentages below given threshold values was limited by lack of reported data . for comparison , the percentage of children below given fsiq values after partial brain irradiation was plotted in figure 3 indicating a minor fsiq decline at substantial higher doses when compared to whole brain irradiation . approximation of normal tissue complication probabilities derived from data contributing to figure 3 the 5% and 50% increase of percentage of children below defined fsiq values following whole brain irradiation can be approximated . 
for comparison , display of percentage of children < 3 years with fsiq < 90 after whole brain irradiation and percentage of children after partial brain irradiation with fsiq < 90 and < 80 . 
full scale iq ( fsiq ) after cranial irradiation influence of mtx administration with and without whole brain irradiation the influence of mtx effects in combination with radiation therapy could not be evaluated in this study , since at the 18 , 24 , and 36 gy dose level nearly all children received a combined therapy regimen , with only a limited number of children known to have undergone radiation therapy without combination with any form of mtx therapy . 
the majority of studies provides data concerning fsiq , some report other iq data , such as performance iq ( piq ) or verbal iq ( viq ) , as well . 
not all of these iq may be found similar impaired after radiation therapy . other functional qualities , such as memory and attention may well be deficient without significant expression in other test scores . 
thus , focus of this review on fsiq was given by the broad data basis and the fact that fsiq represents a general assessment of intellectual functioning with defined mean value and standard distribution of test values in the normal population . 
whereas these authors found a correlation between irradiated volume ( whole brain irradiation vs partial brain irradiation ) and decline in fsiq , no analysis in regard to radiation doses was provided . the present review analyzed fsiq development after whole brain and partial brain irradiation . 
analysis of 36 studies and more than 1 , 900 children showed a clear correlation between test results and radiation dose and volume . in the whole group of children , the mean fsiq after 18 and 24 gy whole brain irradiation was within the normal range . at doses higher than 24 gy a negative correlation with increasing doses was found . 
their model assumed a patient with an initial score of 100 and whole brain irradiation treatment with 18 , 24 , and 36 gy at ages from 2 to 10 and predicts a linear decrease with increasing dose . 
for the younger children ( less than age 6 ) the estimated value at 18 and 24 gy from the model and our compiled data almost overlap , but at higher doses the documented decline exceeds by far the prediction of the model . 
evaluation of the control groups in the present review found the whole group as well as all subgroups at fsiq levels of about 104 . no significant difference was found between healthy children and children with brain tumors or acute lymphoblastic leukemia , either before or after undergoing sufficient treatment but without radiation therapy . the definition of 100 as the baseline for calculation of fsiq drop and as the starting point of the curves may be controversial , but to ensure comparability of all collected data we decided to use the standardized mean value of all iq tests . however , this may have consequences if a drop is calculated in the collected data , with possible underestimation of detrimental effects , this with special respect to fsiq impairment following a whole brain irradiation dose of 18 gy . 
the wmfsiq in this review of 100.0 points was exactly as high as the expected mean value in a normal population , but 4.2 points lower than the mean score of all control groups . therefore , a minor effect of radiation therapy with 18 gy could not be excluded with certainty . the influence of the findings and interpretation of a single study on possible discrete drop in cognitive functioning following whole brain irradiation with 18 gy in this review may be documented . 
a recent longitudinal study [ 14 ] evaluated 129 children with acute lymphoblastic leukemia following 18 gy whole brain irradiation in combination with mtx containing chemotherapy in comparison to a second group of 74 children which were only treated with intravenous and intrathecal mtx . 
after a follow - up of more than 7 years , the irradiated children scored with a mean fsiq of 95 , compared to 104.5 in children treated with chemotherapy alone . 
as the mean follow - up of all children ranged between 6.4 years ( 18 gy ) and 5.8 years ( chemo ) only a subgroup of children can have contributed to this last test value . 
it would have been of great interest to compare the latest test results of the subgroup with longest follow - up with their own initial score . this documents a common dilemma ; test results at different times after therapy and from different subgroups may lead to significantly different conclusions . 
 [ 20 ] provide in their study data for intellectual outcome after 2 courses of whole brain irradiation with initial doses of 24 gy and additional doses of 30 gy at the time of recurrent disease . 
although the authors did not report the time gap between the 2 whole brain irradiation treatment courses this seems to demonstrate a splitcourse effect with considerable reduction of expected fsiq detriment . 
this may confirm the hypothesis that hyperfractionation can reduce functional detriment . tumor localization and histology can have a major impact on fsiq following partial brain irradiation with substantial impairment in children with hypothalamic tumor extension [ 18 ] and tumors of the parapituitary region [ 15 ]  . 
fsiq test results are undoubtedly associated with factors , such as hydrocephalus [ 15 , 18 ] , extend and number of surgeries [ 3 ] , and degree of neurological deficit and disability [ 18 , 28 ]  . 
overall , the paucity of current data on cognitive functioning following partial brain irradiation does not allow definitive conclusions regarding dose - effect relationship . phylaxis , yet can safely avoid normal tissue complications , precise knowledge of tumoricidal dose and tolerance doses of normal tissue is required . 
calculation of normal tissue complication probabilities ( ntcp ) offers an additional estimate of the increase of risk for the occurrence of deterministic and therefore doseand / or volume - dependent radiation induced sequelae . 
typically , an increase in risk of 5% and 50% for a follow - up time of 5 years is calculated . the data for td5 / td50 were approximated from curves derived from data of several publications . 
data contributing to this estimation are quite inhomogeneous ; children with whole brain irradiation doses up to 30 gy have mostly been treated for acute lymphoblastic leukemia , at higher doses the leading diagnosis was medulloblastoma . 
we could not account for the influence , and thus possible immanent errors , of primary tumor and cofactors such as surgery , combined toxicity of chemotherapy and effects caused by different daily fractionation regimens . 
we tried to account for the age at treatment as an important factor by excluding the children younger than age 3 for this approximation ; still the data reflect a wide age - range at the time of treatment . thus , an average effect of whole brain irradiation on rate of children with post - treatment fsiq < 90 and < 80 points has been estimated . 
approximation of this value risk had an even higher degree of uncertainty , with doses of 22.5 gy and 26 gy possibly causing a 5% increase of children with an fsiq < 90 , and < 80 , respectively . to our knowledge , miralbell et al . 
this would suggest a substantially minor steep dose - effect relationship than observed in the present evaluation where about 90% of reported children were tested below 90 points at this high dose level . 
full scale iq ( fsiq ) after cranial irradiation based on complication endpoints , such as necrosis which usually do not occur in a normal population there is no need for this discrimination . 
calculation for 50% new events would result in slightly higher dose levels . increase of percentage of children with test results < 90 and < 80 points was also documented after localized cranial irradiation . 
the only reliable conclusion based on current data is that there is an increase in the percentage of children with fsiq < 90 and < 80 following local cranial irradiation , whereas , although , far less pronounced as expected after comparable whole brain irradiation doses . 
the link of dose and its effects at conventionally fractionated doses higher than 54 gy remains yet unclear ; also if this function may be linear or non - linear . conclusion the intent of the present study was to improve knowledge of the causal correlation of cranial radiation therapy and intellectual development . 
the collected data suggest that whole brain irradiation doses of 18 to 24 gy cause no major impairment of intellectual development in children older than age 6 , but may be already correlated to an impairment in children younger than age 3 . 
several limitations , such as inhomogeneous primary tumors , influence of cofactors and treatment parameters as well as the criteria to collect and analyze the data might initiate critical discussion . thus , we support suggestions by others of a standardized test design with evaluation of various , comparable essential data , such as fsiq , piq , and viq . 
including them might have influenced our conclusions . in order to detect a possible effect following whole brain irradiation with 18 gy , further data collection is required . baseline testing in form of a prospective study design is required to clarify if the small fsiq decline compared to fsiq of the control group , as found in this review , represents a reproducible effect . 
whole brain irradiation with 18 gy is currently recommended as standard dose in the prophylactic treatment of children with high - risk acute lymphoblastic leukemia ( wbc count > 25 , 000 ) and the rationale to exclude cranial radiation therapy in the prophylaxis for acute lymphoblastic leukemia is based on the studies reporting intellectual detriment . 
reevaluation of the large group of children treated with whole brain irradiation doses > 36 gy in the past , and now with significant long - term follow - up , could provide essential , additional information , as inhomogeneous data situation at this dose level requires further research . acknowledgement : the authors wish to thank john o . 
a. , for his assistance in the preparation of the manuscript . strahlentherapie und onkologie urban & vogel 2000 originalarbeit erste ergebnisse der neoadjuvanten simultanen radiochemotherapie bei fortgeschrittenen rektumkarzinomen ute kchenmeister1 , ralf kirchner2 , jochen mellert2 , gunther klautke1 , ralph mcke1 , ulrich - theodor hopt2 , rainer fietkau1 hintergrund : bei lokal weit fortgeschrittenen rektumkarzinomen ist das erreichen einer r0 - resektion schwierig . muss jedoch makroskopisch oder mikroskopisch tumorrest zurckgelassen werden , ist die prognose der patienten schlecht . 
in der ersten und fnften bestrahlungswoche erhielten die patienten an fnf aufeinander folgenden tagen eine dosis von tglich 1000 mg / m2 5 - fu als intravense dauerinfusion ber 24 stunden . 
 schlsselwrter : rektumkarzinom properative therapie radiochemotherapie first results of concurrent preoperative radiochemotherapy of locally advanced rectal cancer purpose : in locally advanced rectal cancer tumor - negative margins often cannot be obtained by surgery alone . 
due to the poor prognosis of patients with r1 / r2 resection the deutsche krebsgesellschaft recommends concurrent preoperative radiochemotherapy for patients with locally advanced rectal cancer . patients and methods : between may 1997 and november 1999 22 patients were treated with preoperative radiochemotherapy . 
on days 1 to 5 and 29 to 33 patients received concurrently 5 - fluorouracil ( 5 - fu ) as continuous infusion of 1 , 000 mg / m2 . 
if there was any sign of cardiac toxicity chemotherapy was changed to 5 - fu / folinic acid or ralitrexed . results : surgery following radiochemotherapy was performed in 19 / 22 patients . 
muss mikroskopisch oder makroskopisch tumor zurckgelassen werden , so sinkt die fnf - jahres - berlebensrate von 50 bis 75% in den uicc - stadien ii / iii auf 15 bis 20% [ 15 ]  . 
in klinisch lokal weit fortgeschrittenen stadien ( klinisches stadium mason iv ) ist eine kurative resektion nur in 40 bis 55% der flle mglich [ 21 , 23 , 24 ]  . 
die mediane nachbeobachtungszeit betrgt 16 monate ( sechs bis 35 monate )  . properativ wurde die t - kategorie mittels endosonographie oder , falls diese nicht mglich war , mittels ct - untersuchung evaluiert . 
acht patienten hatten properativ einen ct3 - tumor , 14 patienten einen ct4 - tumor , fnf patienten hatten endosonographisch keine lymphknotenmetastasen ( cn0 ) , bei 17 patienten ergab sich im ct oder in der sonographischen untersuchung der verdacht auf lymphknotenmetastasen , drei patienten wiesen zum zeitpunkt der diagnose fernmetastasen auf . 
die mehrzahl der tumoren ( 12 / 22 ) befand sich im distalen rektum ( 0 bis 5 cm ab ano ) , 7 / 22 im mittleren drittel ( 5 bis 10 cm ab ano ) sowie 3 / 22 im proximalen drittel ( > 10 cm ab ano )  . strahlentherapie die bestrahlung erfolgte am linearbeschleuniger mit 9bzw . 
 chemotherapie in der ersten und fnften bestrahlungswoche erhielten die patienten an fnf aufeinander folgenden tagen eine dosis von tglich 1 000 mg / m2 5 - fluorouracil ( 5 - fu ) ( maximaldosis 1 800 mg ) als intravense dauerinfusion ber 120 stunden . 
bei auftretender kardiotoxizitt wurde die chemotherapie auf 5 - fu - bolusinfusion oder auf ralitrexed ( 3 , 0 mg / m2 alle drei wochen ) umgestellt . statistische analyse die berlebensraten wurden analog kaplan - meier unter verwendung des pc - programm - pakets spss nach diagnosestellung berechnet . 
ein patient ( ohne fernmetastasen ) verweigerte die operation . bei 16 / 19 ( 84% ) operierten patienten konnte lokal eine r0resektion erreicht werden ; die bei einem patienten synchron aufgetretenen fernmetastasen wurden nicht reseziert . bei drei patienten wurde mikroskopischer residualtumor zurckgelassen . 
pathohistologisch fand sich bei einem patienten kein tumor nach abschluss der radiochemotherapie , ein downstaging um mindestens eine t - kategorie wurde bei 12 / 19 ( 63% ) patienten erzielt ( tabelle 2 )  . tumorhhe operationsart ( n = 22 ) 05 cm 510 cm > 10 cm keine operation : resektion : exstirpation : keine operation : resektion : exstirpation keine operation : resektion : exstirpation : tabelle 1 . 
downstaging of the t stage and the lymph node involvement . rezidivanalyse , berlebensdaten bei einer medianen nachbeobachtungszeit von 16 monaten ist bisher kein lokales rezidiv bei den operierten patienten aufgetreten , auch nicht bei den drei r1 - resezierten patienten . 
das progressionsfreie berleben der 19 operierten patienten betrgt nach 24 monaten 62 14% ( abbildung 1 ) , der r0 - resezierten patienten 61 14%  . die berlebensrate aller patienten war nach zwei jahren 76 10% ( abbildung 2a ) , der operierten patienten 89 8% ( abbildung 2b ) , der r0 - resezierten patienten 87 8% . toxizitt die akuttoxizitt der simultanen radiochemotherapie war vertretbar . 
auffllig war der hohe anteil an patienten mit kardiotoxizitt ; immerhin wurde der verdacht bei 4 / 22 ( 18% ) patienten geuert , sodass hier das chemotherapieschema umgestellt wurde . 
ned - survival of all surgically treated patients following neoadjuvant radiochemotherapy . die vorliegende untersuchung zeigt , dass nach einer properativen radiochemotherapie bei fortgeschrittenen tumoren zeit in monaten zeit in monaten abbildung 2a . 
entsprechend der hier vorliegenden untersuchung konnten bei fortgeschrittenen t3 - / t4 - tumoren in 5 bis 20% pathohistologisch komplette remissionen und r0 - resektionen bei 60 bis 90% der patienten erzielt werden . die unterschiede in den r0 - resektionsraten und in den remissionsraten drften sich im wesentlichen damit erklren lassen , dass von den operateuren die resektabilitt primr verschieden eingestuft wird und somit unterschiedlich fortgeschrittene tumoren in den verschiedenen zentren neoadjuvant behandelt werden . 
unsere ersten berlebensdaten nach zwei jahren ( 76% gesamtberlebensrate , 89% der operierten patienten ) weisen darauf hin , dass die prognose der kurativ operierten patienten nahezu derjenigen entspricht , deren tumoren primr bereits komplett reseziert werden konnten . 
mit 18% liegen wir in unserem krankengut im oberen drittel ; dies kann zum einen auf die kleine fallzahl , den reduzierten allgemeinzustand wie auch auf die tatsache , dass wir unsere patienten regelmig nach kardialen symptome fragten , zurckzufhren sebei vorliegen einer kardialen symptomatik wurde die chemotherapie bei den ersten patienten auf 5 - fu - bolusinfusion , spter auf ralitrexed umgestellt . 
daher verwenden wir ralitrexed jetzt als ersatz fr 5 - fu bei verdacht auf kardiale nebenwirkungen des 5 - fu . in der literatur lsst sich noch kein eindeutiger trend erkennen , ob sich durch eine properative radiochemotherapie die rate an funktionserhaltenden eingriffen erhhen lsst . 
sphincter preservation by the help of neoadjuvant radiochemotherapy . alle tumoren in den distalen 2 cm des rektums gelegen bei allen patienten klinisch abdominoperineale resektion erforderlich bei allen patienten klinisch abdominoperineale resektion erforderlich alle tumoren in den distalen 4 cm des rektums gelegen manchen autoren bis zu 86% betrgt , fanden hyams et al . [ 16 ] im rahmen der nsabp - studie , dass nur bei 27% der patienten die sphinkterfunktion erhalten werden konnte . dabei muss allerdings beachtet werden , dass in dieser analyse nur diejenigen patienten erfasst wurden , bei denen der operateur vor der randomisation zu der einschtzung kam , er msse diesen tumor bei einer primren operation exstirpieren . 
durch eine alleinige bestrahlung war die rate funktionserhaltender eingriffe mit 5 , 3% niedriger als bei einer simultanen radiochemotherapie mit 25% . eine kurzzeitvorbestrahlung ( zum beispiel mit 5 - mal 5 gy ) ist bei diesen fortgeschrittenen und zum teil sehr tief sitzenden tumoren nicht indiziert , denn eine ausreichende tumorrckbildung ( downstaging ) wird durch eine kurzzeitbestrahlung in der regel nicht erreicht . 
sowohl in der stockholm - ials auch in der stockholm - ii - studie war die rate der r0 - resektionen im properativ behandelten arm identisch mit derjenigen der allein operierten patienten [ 5 , 6 ]  . 
das tumoransprechen war bei lngerem intervall signifikant besser ( 71 , 17% nach sechs bis acht wochen versus 53 , 1% nach null bis zwei wochen , p = 0 , 007 )  . 
daher konnten auch wesentlich mehr patienten kontinenzerhaltend in der gruppe operiert werden , bei der das intervall zwischen sechs und acht wochen betrug ( 76% versus 68% , p = 0 , 27 )  . auch wenn die ersten ergebnisse der properativen simultanen radiochemotherapie erfreulich sind , denken wir , dass sowohl die rate an kontinenzerhaltenden eingriffen als auch die r0 - resektionsrate noch verbessert werden mssen . dabei darf nicht vergessen werden , dass wir hier im wesentlichen sehr weit fortgeschrittene tumoren mit entsprechend groen tumorvolumina behandelt haben . 
 [ 1 ] deuten auf eine dosis - effekt - beziehung hin : patienten mit prognostisch ungnstigen tumoren ( fixiert , tief ulzerierend , im distalen drittel des rektums liegend ) wurden mit 55 gy properativ bestrahlt ; ansonsten wurden 45 gy appliziert . 
trotz der niedrigeren tumorstadien traten in der mit 45 gy behandelten gruppe 20% ( 31 / 156 ) lokalrezidive im vergleich zu 6% ( 7 / 119 ) nach 55 gy auf . die von uns applizierte tumordosis gem icru betrug 53 , 5 gy , entspricht also in etwa der hheren dosis von ahmad et al . 
 da sich in der palliativen therapie des kolorektalen karzinoms neue substanzen ( irinotecan , oxaliplatin , ralitrexed , orale 5 - fu - derivate ) mit gutem erfolg etabliert haben , werden derzeit erste phase - ii - studien ( tabelle 5 ) mit diesen zytostatika durchgefhrt . 
die dabei erreichten pathohistologisch gesicherten kompletten remissionen sind zumindest erfolgversprechend . zusammenfassend besttigen die vorliegenden ergebnisse die empfehlungen der deutschen krebsgesellschaft , dass bei tumoren , die vom operateur primr als unsicher kurativ resezierbar angesehen werden , eine properative radiochemotherapie erfolgreich durchgefhrt werden kann . 
influence of the interval between preoperative radiation therapy and surgery on downstaging and on the rate of sphincter - sparing surgery for rectal - cancer : the lyon r 90 - 01 randomized trial . 
a clinical trial to evaluate the worth of preoperative multimodality therapy in patients with operable carcinoma of the rectum : a progress report of national surgical breast and bowel project protocol r - 03 . 
combined modality therapy of locally advanced or recurrent adenocarcinoma of the rectum : preliminary report of a phase i trial of chemotherapy ( ct ) with cpt - 11 , 5 - fu and concomitant irradiation ( rt )  . 
bei tumoren in der kopf - hals - region findet sich ein einfluss des intervalls zwischen operation und bestrahlung auf die lokoregionre prognose nur , wenn ungnstige bedingungen vorliegen , wie z . 
zwar weisen einzelne daten darauf hin , dass sich dadurch die lokale kontrollrate verschlechtert , andererseits muss bei einer verzgerten oder dosisreduzierten chemotherapie unter umstnden mit einer erhhten fernmetastasierungsrate gerechnet werden . 
 schlsselwrter : zeitintervall operation bestrahlung chemotherapie mammakarzinom kopf - hals - karzinom bronchialkarzinom influence of the timing of surgery and postoperative radiotherapy on treatment results background : the timing of surgery and postoperative radiotherapy especially if combined with chemotherapy has been a subject of interest over the past years . methods : this analysis was based on a literature review of mostly retrospective publications . 
data concerning the interval between surgery and radiotherapy were correlated with the locoregional control , incidence of distant metastases and prognosis of breast cancer , lung carcinoma , and head and neck carcinomas . results and conclusions : the reviewed data did not show a clear relationship of the time interval between surgery and start of radiotherapy and locoregional control . 
however , evaluation of the data was difficult , because in most publications , retrospective analyses were performed and other prognostically more relevant parameters may influence locoregional control stronger than the time interval . 
although some data suggest that delaying the initiation of radiotherapy due to chemotherapy may increase the risk of local recurrences , there may , on the other hand , be an increased likelihood of systemic metastases , if radiotherapy is applied before chemotherapy . 
concerning lung cancer , only one retrospective analysis exists suggesting a better survival of patients with an interval of more than 36 days between surgery and radiotherapy as compared to patients with a shorter interval . key words : time interval surgery radiotherapy chemotherapy breast cancer head and neck cancer lung carcinoma 1 klinik und poliklinik fr strahlentherapie , universitt rostock . eingang des manuskripts : 28 . 
dabei wird im rahmen der multimodalen tumorbehandlung die adjuvante bestrahlung immer hufiger mit einer chemotherapie kombiniert . kommt es zu verzgerungen der adjuvanten strahlentherapie durch gerteengpsse , - ausfall , wundheilungsstrungen , kurbehandlungen oder interkurrente erkrankungen , wird an den therapeuten die frage herangetragen , welchen einfluss dies auf die behandlungsergebnisse hat . 
bei der kombination mit chemotherapie ergibt sich das zustzliche problem , welches behandlungsverfahren postoperativ zunchst eingesetzt wird : chemotherapie oder bestrahlung ? dabei schwingt die angst mit , dass durch eine verzgerung der bestrahlung die therapieergebnisse verschlechtert werden . im rahmen eines bersichtsartikels soll anhand von literaturergebnissen der einfluss des zeitintervalls zwischen operation und bestrahlung auf die lokale kontrolle untersucht werden , und zwar bei tumoren in der kopf - hals - region , mammakarzinom und bronchialkarzinom . tumoren in der kopf - hals - region ( tabelle 1 ) tumoren in der kopf - hals - region sind durch eine hohe lokale rezidivrate , weniger durch eine neigung zur fernmetastasierung gekennzeichnet . 
die strahlentherapie nimmt deshalb in der adjuvanten behandlung eine bedeutende rolle e1979 berichtete vikram [ 23 ] erstmals , dass vermehrt lokoregionre rezidive auftraten , wenn die postoperative behandlung mehr als sieben wochen hinausgezgert wird . 
allerdings bezogen sich diese ergebnisse nur auf sehr wenige patienten ( insgesamt 21 ) ; in der gruppe mit einem kurzen zeitintervall zwischen operation und radiotherapie waren berwiegend t1und t2 - tumoren vertreten , und es wurden nur 45 bis 54 gy appliziert . 
bei patienten , die r0 - reseziert waren , traten lokale rezidive bei vier von 25 patienten auf , die innerhalb sechs wochen postoperativ bestrahlt wurden , gegenber vier lokalrezidiven bei vier patienten , deren behandlung ber sechs wochen hinausgezgert wurde . 
sie stellten dabei fest , dass das intervall zwischen operation und bestrahlung nur dann einen einfluss auf die lokoregionre rezidivrate hat , wenn eine geringere bestrahlungsdosis als 60 gy appliziert wird . 
 [ 11 ] weist auf das problem verschiedener einflussfaktoren auf die therapieergebnisse der postoperativen bestrahlung hbei 63 patienten war die lokale kontrolle am besten , wenn innerhalb von sechs wochen nach der operation mit der bestrahlung begonnen wurde , und verschlechterte sich deutlich , wenn dieser zeitraum auf sechs bis acht wochen bzw . 
bei der weiteren analyse der daten stellten die autoren jedoch fest , dass die verlngerung des zeitintervalls mit anderen parametern verknpft war , die ebenfalls die prognose verschlechtern und nicht mittels tumorstadium oder differenzierungsgrad erfasst werden . 
wurden diese flle aus der analyse ausgeschlossen , so konnte der zeitzusammenhang nicht mehr besttigt werden . mammakarzinom ( tabellen 2 und 3 ) bei dieser tumorentitt kann durch die kombinierte operative und strahlentherapeutische behandlung die lokale rezidivrate unter 10% abgesenkt werden . 
1994 [ 21 ] < 1 monat 13 monate 36 monate > 6 monate < 7 wochen > 7 wochen < 4 wochen 58 wochen 912 wochen 08 wochen 812 wochen 1216 wochen > 16 wochen < 8 wochen 812 wochen < 25 tage 2550 tage 5075 tage > 75 tage 5 , 0% * 6 , 0% 0 , 0% 0 , 0% 8 , 4% 12 , 4% 2 , 0% 5 , 4% 6 , 3% kein einfluss n.s. * 5 jahre 85% * 91% n.s. 100% p = 0 , 34 kein unabhngiger prognostischer parameter crude rates nach 5 jahren ; kein unabhngiger prognostischer faktor kein unterschied p = 0 , 189 kein einfluss nicht kein unabhngiger prognostischer faktor angegeben im cox - proportionalhazard - modell n.s. p < 0 , 05 kein einfluss kein einfluss brusterhaltende therapie ; zeitintervall unabhngiger prognostischer parameter ; ct nach bestrahlung meek et al . 
 [ 21 ] fanden in einem cox - proportional - hazard - modell , dass das tumorstadium , der resektionsstatus und ein verlngertes zeitintervall zwischen operation und bestrahlung unabhngige prdiktive parameter fr ein lokales rezidiv waren . 
patienten mit einem intervall zwischen operation und bestrahlung ber 50 tage hatten 5 , 6% lokale rezidive gegenber 1 , 7% bei jenen patienten , deren intervall geringer als 50 tage war . 
daher ist die verzgerung des strahlentherapiebeginns nicht auf die applikation der chemotherapie zurckzufhren , sondern auf eine verzgerte zuweisung oder verzgerte wundheilung . operation strahlentherapie chemotherapie 1991 und 1993 berichteten recht et al . 
im strahlentherapie - polychemotherapie - arm betrug die lokalrezidivrate nur 5 , 5% verglichen mit 13% im polychemotherapie - strahlentherapie - arm ( p = 0 , 07 )  . ein divergentes ergebnis dazu mussten diese autoren jedoch bei der fernmetastasierung feststellen . 
 [ 28 ] untersttzt , die ebenfalls vermehrt fernmetastasen sahen , wenn weniger als sechs zyklen chemotherapie vor beginn der strahlentherapie appliziert wurden . bronchialkarzinom bronchialkarzinome sind sowohl durch eine hohe lokale rezidivrate als auch fernmetastasierungsrate gekennzeichnet . in einer retrospektiven untersuchung fanden wrschmidt et al . 
berraschenderweise hatten patienten mit einem lngeren zeitintervall ( 37 bis 84 tage ) eine bessere fnf - jahres - berlebensrate ( 26% ) als patienten mit einem kurzen zeitintervall ( 18 bis 36 tage 15% ; p = 0 , 13 )  . 
die autoren schlossen daraus , dass ein bestrahlungsbeginn postoperativ beim bronchialkarzinom innerhalb von sechs wochen nach der operation nicht notwendig ist , und fhren dies darauf zurck , dass nach so ausgedehnten operationen die patienten einen lngeren zeitraum bentigen , um sich zu erholen . 
da es sich hier um die einzige mir bekannte studie handelt , mssen die ergebnisse sicher noch mit vorsicht bewertet werden . kritische wrdigung die vorgestellten ergebnisse knnen keinen eindeutigen zusammenhang zwischen der lnge des intervalls operation bestrahlung und der lokalen rezidivrate aufzeigen . tierexperimentelle untersuchungen existieren meines wissens nicht . 
dieser widerspruch zwischen den theoretischen berlegungen und den tatschlich in studien gefundenen ergebnissen kann auf folgenden grnden beruhen : das intervall operation bestrahlung ist nur einer der parameter , die die lokale prognose beeinflussen . 
so muss vermutet werden , dass patienten , die in der wartezeit auf die bestrahlung ein lokoregionres rezidiv entwickelten , nicht erfasst wurden , da sie in den nachsorgedateien als rezidivpatienten abgespeichert wurden . 
patienten , bei denen man fernmetastasen im zeitintervall zwischen operation und radiotherapie diagnostizieren musste , wurden nicht in der strahlentherapie angemeldet , da das lokale problem sekundr wurde und die systemische behandlung im vordergrund stand . bei patientinnen mit mammakarzinom ist die situation noch wesentlich komplizierter , da neben dem lokalrezidiv die fernmetastasierung die prognose beeinflusst . 
 [ 18 ] zeigt , dass bei einer verzgerung der radiotherapie mit einer erhhten rate lokaler rezidive zu rechnen ist , und dies auch bei einer zustzlichen behandlung mittels chemotherapie . 
dies knnte sowohl ausdruck der verzgerten chemotherapie als auch der erniedrigten chemotherapiedosen im strahlentherapie - polychemotherapie - arm sekritisch muss allerdings angemerkt werden , dass die nachbeobachtungszeit nicht ausreicht , da erfahrungsgem bei mammakarzinomuntersuchungen erst die daten nach zehn jahren oder spter den einfluss der lokalen kontrolle auf das berleben zeigen [ 19 ]  . 
eine reevaluation der studie ist bislang noch nicht erfolgt . in unserer tglichen praxis sollten wir aufgrund der dargestellten daten und der theoretischen berlegungen weiter davon ausgehen , dass das intervall zwischen operation und bestrahlung ein parameter ist , der die lokale rezidivrate beeinflussen kann . 
vermutlich haben andere parameter einen wesentlich strkeren einfluss , aber im sinne einer therapieoptimierung sollte daher bei patienten mit kopf - hals - tumoren das postoperative intervall im rahmen der altbewhrten sechs wochen bleiben . 
patients with early stage invasive cancer with close or positive margins treated with conservative surgery and radiation have an increased risk of breast recurrence that is delayed by adjuvant systemic therapy . 
 schlsselwrter : zeitfaktor fraktionierte strahlentherapie onkologische therapie proliferation repopulierung hypoxie what do we know about the mechanisms of the time factor in oncological therapy ? background : experimental studies and prospective randomized clinical trials have demonstrated a detrimental effect of prolongation of overall treatment time on local tumor control . 
 key words : time factor fractionated irradiation oncological therapy proliferation repopulation hypoxia i n der radioonkologie ist ein zeitfaktor , das heit eine abnahme der tumorkontrollwahrscheinlichkeit mit zunehmender gesamtbehandlungszeit einer fraktionierten strahlentherapie , durch untersuchungen an experimentaltumoren [ 1 , 5 , 6 , 7 , 23 ] und durch randomisierte klinische studien an plattenepithelkarzinomen des kopf - hals - bereiches und nichtkleinzelligen bronchialkarzinomen belegt ( literaturzitate in : [ 4 , 26 ] )  . 
der schwerpunkt liegt dabei auf der strahlentherapie , die chirurgische therapie und systemische therapie werden in anderen beitrgen dieser ausgabe abgehandelt [ 16 , 30 ]  . 1 klinik und poliklinik fr strahlentherapie und radioonkologie , universittsklinikum carl gustav carus , technische universitt dresden . diese arbeit wurde in teilen durch die deutsche forschungsgemeinschaft ( ba 1433 ) untersttzt . eingang des manuskripts : 28 . 
mechanismen des zeitfaktors in der onkologischen therapie die wachstumsgeschwindigkeit unbehandelter tumoren reicht zur erklrung des zeitfaktors nicht aus die meisten tumoren , insbesondere solide tumoren des erwachsenen , haben eine relativ lange volumenverdopplungszeit ( tabelle 1 )  . 
fr plattenepithelkarzinome des kopf - hals - bereiches und fr nichtkleinzellige bronchialkarzinome liegt die durchschnittliche volumenverdopplungszeit im bereich von sechs wochen bis drei monaten . wrde die volumenverdopplungszeit unbehandelter tumoren die proliferationsgeschwindigkeit klonogener tumorzellen whrend der therapie widerspiegeln , so wre ber die zeitdauer einer kurativen strahlentherapie von sechs bis sieben wochen etwa eine zunahme der zahl klonogener tumorzellen um den faktor 2 , also z . 
ausnahmen sind seltene , ausgesprochen schnell proliferierende tumoren mit volumenverdopplungszeiten von wenigen tagen . natrlich kann das wachstum unbehandelter tumoren immer dann die ergebnisse einer onkologischen behandlung verschlechtern , wenn der beginn der therapie durch verschleppung der diagnose oder aufgrund von wartelisten ber lngere zeit verzgert wird . 
hier kann eine verdopplung des tumorvolumens den unterschied zwischen tumor histologie durchschnittl . vdt ( tage ) range lungenmetastasen kolon / rektum adenokarzinom adenokarzinom brustdrse adenokarzinom niere adenokarzinom schilddrse gebrmutter adenokarzinom fibrosarkom osteosarkom teratom lymphom plattenepithelkarzinom 57 primrtumoren lunge rektum brustdrse adenokarzinom plattenepithelkarzinom 85 undifferenziertes karzinom adenokarzinom adenokarzinom 84107 5698 3798 44103 55111 4375 4693 2438 2536 1939 121181 7595 6793 426938 68134 resektabilitt und einem nicht mehr resektablen tumor bedeuten . 
darber hinaus kann aufgrund einer grenzunahme der anteil strahlenresistenter hypoxischer tumorzellen zunehmen und die intratumorale verfgbarkeit der chemotherapie infolge verschlechterter durchblutungsbedingungen abnehmen . beschleunigte proliferation klonogener tumorzellen als eine wesentliche ursache des zeitfaktors die volumenverdopplungszeit eines tumors wird durch drei gren beeinflusst , nmlich die zellzykluszeit , die wachstumsfraktion und den zellverlust . 
zellverlust aus dem tumor kann dabei durch das abdrngen von zellen in nekrosen , durch abschilfern , resorption , apoptose und differenzierung bedingt sefalls whrend einer behandlung der zellverlust abnimmt , falls ruhende tumorzellen zu proliferieren beginnen oder falls die proliferationsgeschwindigkeit der stammzellen zunimmt , besteht die mglichkeit , dass sich die verdopplungszeit klonogener tumorzellen deutlich verkrzt [ 10 , 13 , 28 ]  . 
diese beschleunigte proliferation wird heute als wesentlicher mechanismus des zeitfaktors in der onkologischen therapie angesehen . untersuchungen an experimentaltumoren unter klinikhnlichen bedingungen zeigen , dass , bei erheblichen unterschieden im ausma dieses phnomens , die zur lokalen kontrolle notwendige strahlendosis mit zunehmender gesamtbehandlungszeit ansteigt [ 1 , 57 , 23 ]  . 
hierzu mssen alternative erklrungsmechanismen wie tumor ( tage ) tpot ( tage ) zellverlust kopf - hals - bereich ( plattenepithelkarzinome ) nichtkleinzellige bronchialkarzinome ( 4375 ) * ( 7595 ) ( 1 , 870 ) ( 1 , 4130 ) > 90 > 95 tabelle 1 . 
diese ergebnisse knnten darauf hinweisen , dass solche tumoren , die dem normalen plattenepithel in ihrem aufbau noch weitgehend hneln , durch eine kompensatorische umstellung ihrer proliferationsstruktur aktiv auf einen strahleninsult reagieren . 
derzeit knnen zu dieser interessanten frage aufgrund widersprchlicher experimenteller befunde jedoch noch keine schlussfolgerungen gezogen werden [ 6 ]  . zunehmende hypoxie als alternative erklrungsmglichkeit des zeitfaktors da hypoxische tumorzellen strahlenresistenter sind als gut oxygenierte tumorzellen , knnte auch ein wachsender anteil hypoxischer tumorzellen mit zunehmender gesamtbehandlungszeit den zeitfaktor der fraktionierten strahlentherapie erklren . 
von mehreren arbeitsgruppen wurden daher untersuchungen ber den einfluss der gesamtbehandlungszeit auf die lokale tumorkontrolle whrend fraktionierter bestrahlung unter abgeklemmtem blutfluss , das heit unter homogen anoxischen bedingungen , durchgefhrt [ 24 , 27 , 29 ]  . 
durch diese experimente konnte fr verschiedene tumormodelle ( zwei murine plattenepithelkarzinome , ein murines ovarialkarzinom , ein menschliches plattenepithelkarzinom auf nacktmusen ) ein zeitfaktor nachgewiesen werden , der auf einer zunahme der proliferationsgeschwindigkeit klonogener tumorzellen whrend der strahlentherapie beruht . 
durch zytokinkaskaden whrend der wundheilung , zu einer beschleunigten proliferation stimuliert werden knnen [ 2 ]  . als mgliche ursachen der beschleunigten repopulierung unterschiedlicher experimentaltumoren whrend strahlentherapie durch klonogene tumorzellen wurden eine kompensatorische verschiebung von asymmetrischen zu symmetrischen stammzellteilungen , eine verminderte apoptose und eine zunehmende proliferation infolge einer verbesserten versorgungssituation berlebender tumorzellen diskutiert [ 6 , 19 , 21 , 27 , 29 ]  . 
die breite der erklrungen zeigt , dass weitere untersuchungen zu den mechanismen der repopulierung und eventuellen unterschieden zwischen verschiedenen tumoren notwendig sind . in klinischen untersuchungen wurde versucht , durch prtherapeutische messungen von zellkinetischen parametern in tumorbiopsien voraussagen zum zeitfaktor individueller tumoren whrend einer strahlentherapie zu treffen . 
eine wesentliche ursache hierfr drfte die vernderung zellkinetischer parameter der klonogenen zellen whrend der therapie sewiederholte messungen im verlauf der therapie knnen dieses problem nicht lsen , da ein marker zur identifizierung der wenigen berlebenden klonogenen tumorzellen nicht zur verfgung steht . 
whrend fraktionierter strahlentherapie ergaben sich keine signifikanten vernderungen des markierungsindex fr brdu , einem marker der s - phase , und ki67 , einem marker fr alle zellen innerhalb des zellzyklus . 
mediane labelling - indices ( li ) fr die proliferationsparameter ki67 ( ( cid : 2 ) ) und brdu ( ( cid : 3 ) ) whrend fraktionierter strahlentherapie von fadu - tumoren in nacktmusen . 
median labeling indices ( li ) for the proliferation marker ki67 ( ( cid : 2 ) ) and brdu ( ( cid : 3 ) ) during fractionated radiotherapy of fadu tumors in nude mice . 
mechanismen des zeitfaktors in der onkologischen therapie umfangreichen untersuchungen an einem rattensarkom nachweisen , dass ab der dritten woche einer strahlentherapie mit 5 - mal 3 gy pro woche das gefnetz zunehmend rarefiziert wird und die interstitiell bestimmten po2 - werte abnehmen . 
experimentell ergibt sich hierfr jedoch kein anhalt . im gegenteil , in einer experimentellen untersuchung nahm die kapazitt von plattenepithelkarzinomen zur erholung von subletalen strahlenschden whrend fraktionierter bestrahlung ab [ 17 ]  . 
eine mgliche interpretation dieser befunde ist , dass eine gesteigerte proliferationsgeschwindigkeit von mukosastammzellen bzw . klonogenen tumorzellen mit einer verringerten erholungskapazitt von subletalen strahlenschden einhergeht . knnen lange gesamtbehandlungszeiten auch eine verbesserte tumorkontrolle bewirken ? mgliche mechanismen eines inversen zeitfaktors durch mehrere mechanismen knnte es theoretisch auch zu einer steigerung der empfindlichkeit eines tumors mit zunehmender gesamtbehandlungszeit der onkologischen therapie kommen ( inverser zeitfaktor )  . 
da messungen des interstitiellen po2s oder auch der immunhistochemische nachweis hypoxischer zellen nicht zwischen klonogenen und nichtklonogenen tumorzellen unterscheiden knnen , kann dieses phnomen derzeit nur in aufwendigen radiobiologischen experimenten auf stammzellebene weiter abgeklrt werden . ruhende tumorzellen in der g0 - phase sind relativ unempfindlich gegenber strahlung und vielen chemotherapeutika . 
immunhistochemische darstellung intratumoraler gefe in einem unbehandelten humanen plattenepithelkarzinom auf nacktmusen ( links ) sowie in der gleichen tumorlinie nach bestrahlung mit 20 fraktionen in vier wochen ( rechts )  . 
immunohistochemical image of the intratumoral vessels in an untreated human squamous cell carcinoma in nude mice ( left ) compared to the same tumor line after irradiation with 20 fractions in 4 weeks ( right )  . the staining was performed using the rat monoclonal anti - mouse - endothelium antibody 9f1 . 
 methodik : in der arbeit wird anhand einer literaturanalyse die rolle der gesamtbehandlungsdauer und der dosisintensitt bei der optimierung chemotherapeutischer protokolle am beispiel dreier wichtiger onkologischer erkrankungen untersucht . ergebnis und schlussfolgerung : sowohl tumormodelle und die daraus folgenden hypothesen als vor allem auch gut entworfene klinische studien knnen fortschritte in der chemotherapeutischen behandlung von tumorerkrankungen ermglichen . schlsselwrter : chemotherapie gesamtbehandlungszeit dosisintensitt remissionsrate the role of treatment duration in chemotherapy regimens for the treatment of malignant diseases background : the treatment of malignant tumors consists in the optimal combination of the 4 modalities surgery , radiotherapy , chemotherapy , and immunotherapy . 
 result and conclusion : tumor models with the resulting hypotheses and well - designed clinical trials will lead to progress in the treatment of malignant tumors . key words : chemotherapy treatment duration dose intensity remission rate sulen chirurgie , strahlentherapie , d ie behandlung bsartiger tumoren ruht auf den vier systemische chemotherapie und immuntherapie . 
die bestmgliche behandlung von bsartigen erkrankungen wird einerseits durch interdisziplinre konzepte , ohne die eine onkologische behandlung nicht denkbar ist , andererseits aber auch durch die kontinuierliche optimierung der einzelnen behandlungsmodalitten erreicht . 
hierbei spielen vernderungen der zeitlichen dauer und der abfolge bekannt wirksamer substanzen eine wichtige rolle . unter dem begriff chemotherapie verstehen wir eine tumortherapie durch verabreichung zytotoxischer substanzen , soge1 innere medizin i , universittskliniken des saarlandes , homburg / saar . eingang des manuskripts : 28 . 
der begriff chemotherapie geht auf paul ehrlich zurck , der aus der tatsache , dass chemische substanzen mikroorganismen differenziell anfrbten , schloss , dass dieser mechanismus zur gezielten behandlung von bakteriellen infektionen einsetzbar sein msse . 
die von ihm ertrumte wunderwaffe ( magic bullet ) ist mit der erfindung des penicillins fr die antimikrobielle chemotherapie wirklichkeit geworden , scheint fr die behandlung bsartiger tumoren aber noch in weiter ferne zu liegen . 
dies liegt einerseits daran , dass entartete zellen zwar genetisch verndert sind , sich von den gutartigen , differenzierten ursprungszellen hinsichtlich ihres stoffwechsels und damit auch der metabolisierung von zytostatika in der regel nur quantitativ unterscheiden . 
angriffspunkt zytostatischer verfahren ist das wissen darum , dass die tumorzellpopulation als ganze nicht nur entdifferenziert ist , sondern einen sehr viel hheren prozentsatz als das normalgewebe an zellen enthlt , die der wachstumsfraktion angehren . 
es scheint auf den ersten blick ohne weiteres hinterfragen einsichtig , dass der zeitfaktor , also der versuch , mglichst viel in mglichst kurzer zeit zu applizieren , hier von besonderer bedeutung ist . 
aufgabe dieser kurzen darstellung soll die beschreibung unterschiedlich lang dauernder chemotherapieprotokolle und ihrer klinischen und theoretischen grundlagen im hinblick auf die frage sein , welche rolle hier die gesamtbehandlungsdauer spielt . 
tumorspezifische parameter wie die klonale heterogenitt mit entwicklung resistenter zellen , der anteil der aktiv proliferierenden zellen in einem gewebe und pharmakokinetische parameter , zu denen die metabolisierung , tumorzirkulation ( tumordosis ) sowie die unterscheidung zwischen gesamtdosis und dosisintensitt ( dosis pro zeit ) zhlen , entscheiden ber den mglichen erfolg einer chemotherapie . 
dabei spielen neben tumorspezifischen auch individuelle , von patient zu patient verschieden faktoren , die hufig nicht oder schlecht definierbar sind , eine groe rolle . all dies soll die bedeutung von hypothesen und modellhaften therapieschemata aber nicht relativieren , sondern die wichtigkeit rational entworfener und konsequent durchgefhrter therapiestudien untermauern , da nur so aussagen zu erwarten sind , die interindividuelle unterschiede relativieren knnen . 
 grundlagen der internistischen tumortherapie modelle , hypothesen und kochrezepte ? der auf den ersten blick zufllig erscheinenden vielfalt internistisch - onkologischer behandlungskonzepte und ihrer fortentwicklung in den letzten jahrzehnten liegen neben empirischen , durch phase - iii - studien validierten und in die klinische praxis integrierten regimen , die zuweilen eher beliebig zusammengesetzt denn rational begrndet erscheinen ( daher pejorativ : kochrezepte ) , aber modelle und hypothesen zugrunde , die im labor und tierversuch sowie im mathematischen modellversuch entwickelt sind und einer rationalen klinischen berprfung bedrfen . 
der errterung dieser grundlagen seien einige ausgewhlte beispiele internistischonkologischer behandlungsverfahren vorangestellt , die die breite der biologischen varianz systemischer tumoren wie auch der angewendeten therapiekonzepte illustrieren sollen . insbesondere wird die frage , inwieweit fr unterschiedliche gesamtbehandlungszeiten klinisch validierte daten vorliegen , errtert . 
ausgegangen wird dabei von der situation einer kurativ intentionierten systemischen chemotherapie , da die bedingungen einer palliativen behandlung sowohl von der behandlungsindikation wie der durchfhrung der therapie her grundstzlich andere sind als die einer kurativen behandlung . 
hodentumoren , die durch systemische behandlungen in 90% der flle in komplette remissionen zu bringen sind und bei denen mehr als 75% der patienten nach fnf jahren noch krankheitsfrei leben . 
auf der anderen seite finden sich tumoren ( etwa 40% aller tumoren ) , die zwar chemotherapiesensibel sind , aber selten oder nie geheilt werden knnen und damit primr palliativ behandelt werden mit dem ziel , die tumorprogression zu verlangsamen und damit entweder eine subjektive beschwerdebesserung oder eine deutliche verlngerung der berlebenszeit zu erreichen . 
zu letzteren zhlen weichteiltumoren , lymphatische tumoren so genannter niedriger malignitt ( ! ) wie die chronische lymphatische leukmie oder das plasmozyto bei vielen tumoren , wie magenoder bronchialtumoren und plattenepithelkarzinomen , ist nur eine beschwerdelinderung mglich , und bei anderen ( etwa 20% aller erkrankungen ) ist auch dies nicht durch chemotherapie erreichbar , die damit selten oder nie indiziert ist . 
normalgewebe mit geringerer wachstumsfraktion knnen dann dadurch geschtzt werden , dass der citrovorum - faktor ( folinsure ) hoch dosiert appliziert wird und damit die nukleinsuresynthese im gesunden gewebe ermglicht . zytostatika werden unterschieden anhand ihrer molekularen wirkmechanismen auf den zellulren stoffwechsel und ihres angriffspunktes im zellzyklus . 
phasenspezifische medikamente setzen in einer bestimmten phase ( g1 , s , g2 , m ) des zyklus an , zyklusspezifische medikamente eliminieren alle proliferierenden beziehungsweise aktiv im zyklus befindlichen medikamente , whrend zyklusunabhngig aktive medikamente auch ruhende ( g0 - ) zellen zerstren knnen . die folgenden beispiele zeigen , wie chemotherapieprotokolle aus diesen verschiedenen medikamenten zusammengesetzt werden knnen . 
sind diese kombinationen zunchst empirisch entstanden , indem man versucht hat , die wirksamsten einzelsubstanzen so zu kombinieren , dass die wirkungen wenn mglich additiv , die nebenwirkungen nicht additiv waren , so ist in letzter zeit vermehrt versucht worden , dosisdichte und scheduling dieser substanzen auf rationaler basis zu optimieren . 
wichtig ist dabei , dass die dosierungen einzelner medikamente nicht durch kombinationen so weit kompromittiert werden , dass ihre wirksamkeit vermindert wird und dadurch eventuelle synergismen der kombinationsschemata aufgewogen werden . 
da die wichtigste nebenwirkung fast aller heute eingesetzten zytostatika die passagere unterdrckung der hmatopoese ist , wurde in die einfhrung von wachstumsfaktoren , die diese stimulieren , groe hoffnung gesetzt . 
chemotherapieprotokolle gliedern sich hufig in sogenannte induktionstherapien ( intensive anfangstherapie bis zur remission ) , konsolidierungskurse ( mildere therapie zur stabilisierung dieser remission ) und erhaltungstherapien ( milde therapien zur erhaltung der remission )  . 
akute myeloische leukmie akute myeloische leukmien entstehen aus der klonalen proliferation frher hmatopoetischer zellen , die zeichen einer myeloischen , monozytren oder selten auch erythrozytren und megaloblastren differenzierung zeigen knnen . 
diese proliferationen werden von frhen vorluferzellen , den so genannten aml - stammzellen , unterhalten , die nur einen geringen anteil des sichtbaren leukmieanteils ausmachen , aber die klonale proliferation unterhalten wie auch rezidive verursachen . 
unklar ist , ob diese kurze , hochdosierte oligosubstanztherapie ausreicht oder ob ihr eine erhaltungstherapie ( siehe oben ) , die teilweise ber monate oder jahre angeschlossen wird , folgen muss . 
dies gilt aber nur , solange die aml - klone chemotherapiesensitiv sind . bezglich der gesamtbehandlungsdauer folgt also fr die akute myeloische leukmie : mglichst kurze , intensive behandlung mit induktion und konsolidierung ( rasch , frh , kurz , hoch )  . 
kolorektale karzinome adjuvante therapie gnzlich anders ist die adjuvante situation bei kolorektalen karzinomen , da keine rasche induktion einer systemischen erkrankung vonnten ist , sondern die reduktion der rezidivrate , die vom tumorstadium und der dadurch verursachten minimalsystemischen erkrankung abhngig ist , mit dem ziel , das gesamtberleben zu verlngern . 
so konnten die impact - investigatoren [ 5 ] anhand der daten von 1493 patienten in den stadien dukes b und c aus drei studien zeigen , dass durch eine adjuvante behandlung mit 5 - fluorouracil und leukovorin im vergleich zu einem plazebo das ereignisfreie drei - jahres - berleben von 62% auf 71% erhht werden konnte . 
non - hodgkin - lymphome non - hodgkin - lymphome sind klonale proliferationen lymphatischer zellen , die auf verschiedenen stufen der physiologischen reifung entarten knnen und dadurch eine ausgeprgte heterogenitt besitzen , die sich an unterschiedlicher morphologie , klinik und therapieempfindlichkeit zeigt . dem entspricht inzwischen eine differenzierte , an der biologie orientierte behandlungsstrategie . 
so genannte niedrig maligne ( kiel - klassifikation ) oder indolente ( realbzw . who - klassifikation ) non - hodgkin - lymphome sind primr hufig disseminiert , haben aber eine langsame wachstumstendenz . 
dem entspricht eine primr spt einsetzende behandlung ( bei behandlungsbedrftigkeit ) mit wenigen medikamenten ber sechs bis acht monate ( cop - schema )  . damit lassen sich bei 86% der patienten remissionen ( nur 21% komplette remissionen ; n = 162 patienten ) erreichen . eine intensivierung mit verkrzung der cyclophosphamidapplikation und anwendung von anthrazyklinen in der induktionsbehandlung fhrt zu keiner verbesserung der ergebnisse ( 90% remissionen , 20% komplette remissionen ; n = 182 patienten ; hiddemann und unterhalt , deutsche studiengruppe niedrig maligne non - hodgkin - lymphome , pers . mitteilung , februar 2000 )  . aggressive oder hoch maligne lymphome hingegen zeichnen sich durch eine kurze tumorverdopplungszeit sowie eine hohe wachstumsfraktion aus . 
rasche , dosisintensivierte induktionstherapien wie das acvb - regime der gela [ 1 ] oder ein zeitverkrztes , intensiviertes chop [ 16 ] knnten hier therapieverbesserungen bei verkrzter gesamtbehandlungszeit bringen . 
so konnte in der nhl - b - 94 - studie der deutschen studiengruppe hoch maligne non - hodgkin - lymphome allein durch eine verkrzung der therapiedauer von 18 auf zwlf wochen bei gleicher gesamtdosis bei patienten zwischen 60 und 75 jahren aller klinischen risikogruppen die rate kompletter remissionen von 55 , 7% auf 70 , 6% erhht werden ( n = 365 ; zwischenauswertung 4 / 1999 , eigene daten )  . 
ob dies ein biologischer effekt der stammzelltransplantation ist ( unzureichendes in - vivo - purging der autogenen stammzellen ) oder darauf hindeutet , dass eine konsolidierung bei minimaler resterkrankung nach intensiver induktion auch bei aggressiven lymphomen wichtig ist , lsst sich heute noch nicht sagen . 
eine vernderung der gesamtbehandlungsdauer kann aber die therapieergebnisse beeinflussen , wie das ergebnis der verkrzten , aber dosisverdichteten behandlung bei den aggressiven non - hodgkin - lymphomen zeigt . zur beschreibung dieser effekte sind in den letzten jahrzehnten unterschiedliche modelle entwickelt worden , die versuchen , die biologie des tumorwachstums und die beziehung zwischen dosis und zeit der therapieapplikation so in eine beziehung zueinander zu setzen , dass optimierungen wirksamer therapie berechenbar beziehungsweise vorhersagbar erscheinen [ 11 , 12 , 15 ]  . 
diesen dosis - wirliegen folgende biologische kungs - beziehungsmodellen annahmen zugrunde : die wachstumskurve verndert sich in abhngigkeit vom volumen ( gompertzsches wachstum ) ; tumorzellen befinden sich zu einem gegebenen zeitpunkt in unterschiedlichen wachstumskompartimenten und sind somit gegenber einer chemotherapie unterschiedlich sensibel ; der anteil proliferierender ( empfindlicher ) zellen , temporr ruhender ( temporr nicht empfindlicher , aber rekrutierbarer ) zellen und differenzierter zellen sowie der primr oder sekundr resistenten zellen , die sich in denselben wachstumskompartimenten befinden knnen , charakterisiert einen individuellen tumor und seine chemosensibilitt . 
das skipper - schaber modell [ 13 ] , das so genannte log - kill - modell , geht von einer festen beziehung zwischen applizierter chemotherapiedosis und zelltod sowie einer festen killrate pro zyklus ( 1 log - order ) aus und postuliert somit , dass durch erhhung der applizierten dosis bei frhem beginn eine heilung bei jedem tumor mglich ist , sofern sich keine resistenz entwickelt hat . 
 [ 3 ] entwickelte mathematische modell versuchte erstmals , den fr die klinische behandlung wichtigen aspekt der sekundren resistenz zu erklren , indem zwischen der genetischen mutationsrate eines tumors und seiner ( erworbenen ) resistenz gegenber zytostatika eine direkte beziehung hergestellt wurde . 
neben der genetischen existiert nmlich auch eine kinetische resistenz von tumorzellen , was durch die klinische beobachtung , dass rezidivierte tumoren wieder auf die ursprnglich gegebenen zyostatika ansprechen knnten , untermauert wird . 
die hypothese ist grundlage vieler hochdosistherapieschemata , bei denen nach intensiver induktionschemotherapie und erreichen einer remission einer oder mehrere blcke einer nicht kreuzresistenten chemotherapie appliziert werden , um zuvor ruhende , aber prinzipiell sensitive tumorzellen zu eradizieren . 
dass eine direkte beziehung zwischen der applizierten dosis einer substanz und der wirkung auf den tumor besteht , ist aus in - vitro - versuchen , die zeigen , dass schon eine geringe dosisreduktion nicht unbedingt die rate kompletter remissionen , aber der heilungen reduzieren knnen , bekannt . 
 [ 8 ] das konzept der relativen dosisintensitt , das beschreibt , dass die gegebene menge von zytostatika pro zeiteinheit in direkter beziehung zum therapieerfolgt steht , unabhngig von der zeitlichen abfolge und der applikationsfor vor allem aufgrund der unzureichenden bercksichtigung der tatsache , dass in solchen modellen die quivalenzdosen verschiedener zytostatika nicht ausreichend berechnet wurden , haben sich die auf basis des modells der relativen dosisintensitt entwickelten schemata bis jetzt nicht als berlegen erwiesen . 
eine direkte beziehung zwischen der gegebenen dosis und der effizienz einer chemotherapiekombination wurde anhand von systematischen reviews publizierter studien fr hodgkinund non - hodgkin - lymphome erhoben und als risikoreduktion ( log hazard reduction ) fr die jeweilige kombination beschrieben . 
in die berechnung der effektiven dosis einer substanzkombination gehen die erhobenen quipotenzwerte der verwendeten substanzen fr die jeweilige erkrankung , die gesamtdosis und die gesamtbehandlungszeit sowie die tumorspezifische latenzzeit , die hufig jedoch nur geschtzt werden kann , eso lassen sich unter bercksichtigung der tatsache , dass in flexi - therapieregimes fr lymphome die effektivsten substanzen , das heit vor allem die anthrazykline , hufig unterdosiert wurden , whrend wenig oder kaum effektive substanzen unberprft einbezogen werden , die ergebnisse der intergroupstudie von fisher et al . 
 [ 2 ] ( siehe oben ) nachvollziehen . vorhergesagt wurde mit dem effective - dose - modell das ergebnis der beacopp - studie der deutschen hodgkinstudiengruppe [ 4 , 14 ] , an weiteren studien steht die rationale berprfung dieses theoretischen ansatzes aus . 
fr unsere fragestellung lsst sich jedoch heute schon folgern , dass unter bercksichtigung der oben genannten parameter der gesamtbehandlungszeit in der chemotherapie eine uerst wichtige bedeutung zukommt , da unabhngig von der gesamtdosis einer applizierten chemotherapie die kinetische resistenz von tumoren nur bei einer ausreilangen gesamtbehandlungsdauer durchbrochen chend werden kann . zusammenfassung und ausblick die oben angefhrten beispiele und modelle zeigen , dass die beschreibung eines optimalen therapiekonzeptes wesentlich von der biologie der tumorzellen , ihrer wachstumsrate , klonalen heterogenitt und resistenzlage , aber auch von dem zugrunde liegenden dosiskonzept abhngt . von besonderem interesse fr die optimierung chemotherapeutischer behandlungskonzepte war in den letzten jahren der stellenwert des zeitfaktors . 
von chronobiologischen fragestellungen abgesehen , die den rahmen diese kurzen darstellung sprengen wrden , gehen dabei sowohl die gesamtbehandlungsdauer eines therapieregimes wie auch der zeitliche ablauf und die dauer der applikation ( das sogenannte scheduling und die infusionsdauer ) und die dosisdichte ( dosis pro zeit ) in diese berlegungen e systematische untersuchungen zum stellenwert des scheduling fehlen hufig ; zur frage der rolle der dosisdichte wie der gesamtbehandlungsdauer werden in prospektiven studien , die auf rationalen , aus retrospektiven analysen und dosis - wirkungs - modellen fuenden grundlagen beruhen sollten , in den nchsten jahren ergebnisse zu erwarten seeine weiterentwicklung der chemotherapie ist ohne solche phase - iii - studien nicht denkbar , von der entwicklung gnzlich neuer substanzen natrlich abgesehen . 
moderate dose escalation for advanced stage hodgkins disease using the bleomycin , etoposide , adriamycin , cyclophosphamide , vincristine , procarbazine , and prednisone scheme and adjuvant radiotherapy : a study of the german hodgkins lymphoma study group . 
buschke [ 6 ] fasste 1963 auf der jahrestagung der american radium society den damaligen kenntnisstand wie folgt zusammen : ... , it becomes increasingly certain that such prolonged treatment [ of more than six weeks ] does not significantly alter the possibility of controlling the tumor , at least as far as epidermoid carcinoma is concerned . 
this , then , would mean that the prolongation of over - all treatment time is one of the most important factors for increasing the differential between effect on the tumor and effect on the vasculo - connective tissue ... 
. wenige jahre spter postulierte auch ellis [ 8 ] in seiner nsdformel , dass ein zeitfaktor im gegensatz zu normalgeweben , bei denen die klinische erfahrung die bedeutung der behandlungszeit zur vermeidung oder erholung von strahlennebenwirkungen erkennen lie , fr tumoren nicht vorhanden sei . 
applying doubtful assumptions to questionable data ... , dennoch blieb die einschtzung von buschke und ellis bis weit in die achtziger jahre hinein klinisch vorherrschend . im gegensatz zu diesen einschtzungen zeigten experimentelle untersuchungen , dass die fraktion berlebender klonogener tumorzellen [ 13 ] bzw . 
als konsequenz aus den laboruntersuchungen und den retrospektiven analysen klinischer daten zur tumorkontrolle wurden in gemeinsamer anstrengung von radioonkologen und strahlenbiologen akzelerierte ( also in ihrer gesamtbehandlungszeit verkrzte ) fraktionierungsschemata entwickelt , die zum ziel hatten , dem effekt der schnellen proliferation klonogener tumorzellen whrend der therapie entgegenzuwirken . 
mittlerweile liegen vier randomisierte studien fr kopf - hals - tumoren [ 7 , 11 , 14 , 16 ] , zwei fr nichtkleinzellige bronchialkarzinome [ 1 , 18 ] und eine fr kleinzellige bronchialkarzinome [ 24 ] vor . 
sechs dieser studien untersttzen , dass durch eine akzelerierte fraktionierung eine bessere lokale tumorkontrolle erreicht werden kann als durch konventionelle fraktionierung , die siebte studie hatte eine zu geringe statistische power [ 1 ] und widerlegt daher die brigen ergebnisse nicht [ 2 ]  . derzeit ist offen , ob die bislang getesteten akzelerierungsschemata eine weite klinische verbreitung finden werden , da in einigen der studien eine unerwartet hohe normalgewebstoxizitt beobachtet wurde [ 4 , 7 , 14 ] so dass kein oder ein nur geringer therapeutischer gewinn gegenber konventioneller fraktionierung erreicht werden konnte und andere schemata aus praktikabilittsgrnden derzeit in vielen zentren nicht angeboten werden knnen . 
heute wissen wir , dass die gesamtbehandlungszeit einer strahlenbehandlung bei plattenepithelkarzinomen des kopf - hals - bereiches , bei nichtkleinzelligen bronchialkarzinomen und bei kleinzelligen bronchialkarzinomen einen wichtigen einfluss auf die behandlungsergebnisse hat und dass dieser einfluss durch die wahl geeigneter behandlungsschemata minimiert werden kann . 
es ist zu erwarten , dass in den nchsten jahren weitere tumorentitten zu dieser liste hinzugefgt werden und dass akzelerierungsschemata fr einen breiten klinischen gebrauch optimiert werden knnen . bereits heute liegen klinische therapieleitlinien vor , die praktikable mglichkeiten aufzeigen , um verlngerungen der gesamtbehandlungszeit durch ungeplante therapieunterbrechungen zu vermeiden [ 3 , 5 ]  . ein gesichtspunkt , der in der wissenschaftlichen diskussion zum zeitfaktor der strahlentherapie bislang im hintergrund stand , ist , dass onkologische patienten meist nicht nur bestrahlt werden , sondern zustzlich eine operation und eine chemobzw . 
warum sollten whrend dieser zeit verbliebene tumorzellen im wundbett , in dem proliferationsstimulierende zytokine im berfluss vorhanden sind , nicht ausgezeichnet proliferieren knnen ? warum sollte eine neoadjuvante chemotherapie vor strahlentherapie nicht ebenfalls eine schnelle repopulierung von tumorzellen induzieren oder umgekehrt eine strahlentherapie vor chemotherapie nicht die proliferation systemischer mikrometastasen stimulieren ? wenn man die tumorbiologischen und klinischen erfahrungen der radioonkologie auf chirurgie und chemotherapie bertrgt , spricht vieles dafr , dass mit einem zeitfaktor , auch wenn dieser bislang ungengend untersucht ist , bei der multidisziplinren kombinationstherapie zu rechnen ist . um dieser frage nach einem erweiterten zeitfaktor in der onkologischen therapie nher zu treten , errterten chirurgen , internistische onkologen , radioonkologen und strahlenbiologen diese thematik gemeinsam whrend eines symposiums auf dem 5 . 
a randomised phase iii study of accelerated or standard fraction radiotherapy with or without concurrent carboplatin in inoperable non - small cell lung cancer : final report of an australian multi - centre trial . 
a radiation therapy oncology group ( rtog ) phase iii randomized study to compare hyperfractionation and two variants of accelerated fractionation to standard fractionation radiotherapy for head and neck squamous cell carcinomas : preliminary results of rtog 9003 . 
accelerated fractionation ( af ) compared to conventional fractionation ( cf ) improves loco - regional control in the radiotherapy of advanced head and neck cancers : results of the eortc 22851 randomized trial . 
der bogen wurde dabei von den mechanismen des zeitfaktors [ 17 ] ber die derzeitige evidenz fr einen zeitfaktor whrend strahlen [ 20 ] und chemotherapie [ 23 ] , therapiepausen [ 9 ] und wartezeiten [ 10 , 12 ] bis hin zur zeitlichen abfolge verschiedener therapiemodalitten [ 25 ] und zu den mglichkeiten der minimierung des einflusses der zeitfaktors auf ergebnisse der onkologischen therapie [ 22 ] gespannt . 
die beitrge des symposiums sind im vorliegenden heft als themenschwerpunkt zusammengefasst . referenten und zuhrer des symposiums stimmten darin berein , dass eine multidisziplinre betrachtung des zeitfaktors in der onkologie fr die weitere optimierung unserer behandlungsergebnisse berfllig war . 
es wurden nur studien aufgenommen , bei denen die strahlentherapie die definitive lokoregionale therapie war . ergebnisse und schlussfolgerung : sowohl bei den plattenepithelkarzinomen der kopf - hals - region als auch bei kleinzelligen und nichtkleinzelligen bronchialkarzinomen liegen studienergebnisse vor . 
bei gleicher effektivitt beider fraktionierungsschemata gegen den tumor kann die gesamtdosis bei akzelerierte fraktionierung reduziert werden . schlsselwrter : akzelerierung repopulierung randomisierte studien metaanalyse evidence for an influence of overall treatment time on radiotherapeutic outcome in different tumor entities background and method : the effect of overall treatment time on therapeutic outcome was analyzed comparing the randomized trials on accelerated fractionation for the different tumor entities . 
only studies using radiotherapy as the definitive locoregional treatment modality were included . results and conclusion : randomized studies were performed for squamous cell carcinomas of the head and neck region as well as for small - cell and non - small - cell carcinomas of the lung . 
these studies showed , that locoregional control can be improved by accelerated fractionation in comparison to conventional fractionation with the same total dose . with the same antitumor effectiveness of both fractionation schedules , total dose can be reduced using accelerated fractionation . key words : acceleration repopulation randomized trials meta - analysis d ie durchfhrung von randomisierten phase - iii - studien , in denen die gesamtdauer der strahlentherapie systematisch variiert wird , stellte einen schwerpunkt der klinischen forschung in der strahlentherapie in den letzten 15 jahren dar . 
die rationale fr die verwendung von akzelerierten fraktionierungsschemata , bei denen die gesamtbehandlungszeit im vergleich zur konventionellen fraktionierung ( 1 - mal 1 , 8 bis 2 , 0 gy pro tag an fnf tagen pro woche ) verkrzt wird , ist die minderung des resistenzfrdernden effektes der tumorzellrepopulierung whrend der therapie , fr welche in akzelerierten schemata weniger zeit bleibt . bei der reinen akzelerierten fraktionierung wird im vergleich zur konventionellen fraktionierung nur die gesamtbehandlungszeit unter beibehaltung der gesamtdosis und dosis pro fraktion gesenkt . 
bei akzeleriert hyperfraktionierten schemata wird zustzlich die dosis pro fraktion gesenkt . mittlerweile liegen mature ergebnisse von randomisierten studien zur akzelerierten fraktionierung oder akzelerierten hyperfraktionierung vor , die eine bewertung dieser schemata aus klinischer sicht mglich machen . 
gesamtbehandlungszeit und therapieergebnisse bei verschiedenen tumorentitten sicht wird entsprechend der eingangs gestellten fragestellung im wesentlichen auf die effektivitt der akzeleriert fraktionierten und akzeleriert hyperfraktionierten schemata gegen tumoren eingegangen , weniger jedoch auf normalgewebseffekte . ter hyperfraktionierung mit konstanter gesamtdosis im vergleich zur konventionellen fraktionierung zusammen , so belegen sie eindrucksvoll , dass bei einer verkrzung der gesamtbehandlungszeit um 1 woche die lokale tumorkontrolle verbessert wird . kopf - hals - tumoren in tabelle 1 sind die ergebnisse von randomisierten studien zur akzelerierten fraktionierung und akzelerierten hyperfraktionierung bei kopf - hals - tumoren wiedergegeben , in denen die strahlentherapie die definitive lokoregionale therapiemanahme war . 
zum teil handelt es sich um mature studienauswertungen [ 3 , 6 ] , zum teil jedoch um interimsanalysen in abstraktfordie ersten drei studien der tabelle 1 zeigen daten zur reinen akzelerierung . 
in den ersten beiden studien wurden im wesentlichen zeitintervalle von 24 stunden zwischen den fraktionen , in der studie aus vancouver ein zeitintervall von mindestens sechs stunden zwischen den zwei fraktionen pro tag eingehalten . 
in dem akzelerierten split - course - schema der eortc - 22851 - studie wurde die gesamtbehandlungszeit um zwei wochen , die gesamtdosis jedoch nicht wesentlich gegenber der konventionellen fraktionierung verndert [ 6 ]  . 
die dosisintensitt schwankte in dieser studie allerdings stark whrend der behandlungsdauer von 22 , 5 gy wochendosis in den wochen 1 und 5 bis auf 0 gy in der pause in woche 3 . 
die gesamtbehandlungsdauer wurde um mehr als vier wochen im vergleich zur konventionellen fraktionierung reduziert . die gesamtdosen wurden ebenfalls reduziert mit dem ziel , die sonst antizipierten erhhten akutund sptnebenwirkungen zu vermeiden . die effektivitt der intensivierten akzeleriert fraktionierten oder akzeleriert hyperfraktionierten schemata im vergleich zur konventionellen fraktionierung ist in erster linie an den lokoregionalen tumorkontrollraten zu erkennen . 
alle studien zeigten mindestens eine gleich gute und hufig eine verbesserte tumorkontrolle im experimentellen ar in vier von den fnf studien , bei denen die gesamtdosis nicht wesentlich gendert wurde , wurden signifikante verbesserungen der lokoregionalen tumorkontrolle in den akzeleriert fraktionierten oder akzeleriert hyperfraktionierten armen beobachtet . 
die negative studie aus vancouver wurde wegen erhhter grad - iv - akutnebenwirkungen abgebrochen und hat wegen der kleinen fallzahl nur eine geringe sensitivitt bei der detektion von unterschieden in den behandlungseffekten auf die tumoren [ 7 ]  . 
fasst man die ergebnisse der studien mit akzelerierter fraktionierung und akzelerierbei der chart - studie und der studie aus wien , bei denen die gesamtbehandlungszeit und die gesamtdosis im arm mit akzelerierter hyperfraktionierung gesenkt wurden , fanden sich zwischen den behandlungsarmen keine signifikanten unterschiede mehr in der tumorkontrolle [ 3 , 4 ]  . 
in einer simultanen gesamtanalyse aller sieben studien betrgt der k - wert , der die repopulierungsleistung am besten beschreibt , 0 , 54 0 , 06 gy / d . nimmt man eine steilere dosis - effekt - beziehung , charakterisiert durch 50 = 3 , an , dann sind die ergebnisse hnlich . 
alle studien zeigen positive k - werte von 0 , 15 bis 0 , 85 gy / d , die mit ausnahme der studie aus vancouver alle signifikant grer als 0 gy / d waren . 
aus diesen quantitativen analysen folgt , dass bei bercksichtigung aller nachfolgenden therapievariablen , gesamtdosis , gesamtbehandlungszeit und dosis pro fraktion , alle studien in tabelle 1 einen gleichgerichteten effekt der gesamtbehandlungszeit auf die tumorkontrolle zeigen . die klinische bewertung der oben genannten therapieschemata ist jedoch komplex . 
in the case of a differing number or size of the fractions per treatment day , the respective treatment days are given in brackets . with differing treatment days per week , the respective weeks are also given in brackets . 
the fractionation schedules are outlined as described in table 1 ; || = simultaneous chemotherapy ; cbdca = carboplatin ; e = etoposide ; p = cisplatin . bronchialkarzinome tabelle 2 zeigt die drei randomisierten studien zur akzelerierten fraktionierung oder akzelerierten hyperfraktionierung bei kleinzelligen und nichtkleinzelligen bronchialkarzinomen . zwei dieser studien zeigen eine signifikante verbesserung des langzeitberlebens durch eine vernderung des fraktionierungsschemas [ 1 , 9 , 12 ]  . 
sie wiesen nach , dass durch eine moderate steigerung der effektiven dosis bei sonst gleichen technischen parametern der strahlentherapie die prognose sowohl beim kleinzelligen bronchialkarzinom , limitierte erkrankung , als auch beim nichtoperablen , nichtkleinzelligen bronchialkarzinom in den stadien i bis iiib verbessert werden kann . 
mit den parametern / ( cid : 3 ) = 10 gy , 50 = 1 oder 3 und k = 0 , 5 gy / d lsst sich fr die chart - studie eine steigerung der effektiven dosis von 10% , fr die studie von turrisi von 23% berechnen . 
 [ 1 ] hatte bei der moderaten fallzahl nur eine geringe sensitivitt , tatschliche unterschiede zwischen den behandlungsarmen auch aufzudecken . sonstige tumorentitten bei den brigen tumorentitten liegen nach einer systematischen medline - recherche keinen greren phase - iii - studien zur akzelerierten fraktionierung oder akzelerierten hyperfraktionierung vor , die den einfluss der gesamtbehandlungszeit auf die tumorkontrolle zuverlssig abschtzen lieen . 
jedoch sollte als nullhypothese bei allen schneller wachsenden tumoren von einem deutlichen effekt der gesamtbehandlungszeit auf das therapieergebnis ausgegangen werden . schlussfolgerung sowohl bei den plattenepithelkarzinomen der kopf - halsregion als auch bei kleinzelligen und nichtkleinzelligen bronchialkarzinomen liegen studienergebnisse vor . 
a randomised phase iii study of accelerated or standard fraction radiotherapy with or without concurrent carboplatin in inoperable non - small cell lung cancer : final report of an australian multi - centre trial . 
a radiation therapy oncology group ( rtog ) phase iii randomized study to compare hyperfractionation and two variants of accelerated fractionation to standard fractionation radiotherapy for head and neck squamous cell carcinomas : preliminary results of rtog 9003 . 
feldmann1 hintergrund : eine reihe von experimentellen und klinischen studien zeigen , dass mit zunehmender gesamtbehandlungszeit die zur tumorkontrolle notwendige strahlendosis ansteigt . methodik : in einer literaturbersicht wurde der frage der verschlechterung der klinischen therapieergebnisse durch das einlegen einer bestrahlungspause nachgegangen . ergebnisse und schlussfolgerung : ein schlechteres berleben bzw . 
therapiepausen sollten daher bei patienten , die kurativ behandelt werden , unterbleiben . schlsselwrter : gesamtbehandlungszeit therapiepause repopulierung split - course radiotherapy or treatment interruptions clinical implications background : experimental and clinical studies have shown that a prolonged overall treatment time is associated with a decrease in local tumor control . methods : in a brief review , the clinical data of radiotherapy with split - course or treatment interruption were collected . results and conclusion : there was a detrimental effect of the treatment interruption on overall or disease - specific survival in patients with locally advanced head and neck cancer or non - small - cell lung cancer in particular in patients with good prognostic factors and well to moderate differentiated tumors . 
therefore , interruption of radiotherapy in patients with curative treatment should be avoided . key words : overall treatment time split - course repopulation d ie gesamtbehandlungszeit einer strahlenbehandlung umfasst den zeitraum von bestrahlungsbeginn bis strahlentherapieende unter einbeziehung aller pausen . 
bei therapiebedingten unterbrechungen und einer daraus resultierenden verlngerung der gesamtbehandlungszeit wurde retrospektiv in einer reihe von studien nachgegangen . klinische untersuchungen insgesamt wurden in den jahren 1994 bis 1998 acht grere retrospektive studien publiziert mit insgesamt 6926 patienten , in denen eine kontinuierliche strahlentherapie mit einer split - course - strahlentherapie verglichen wurde . 
in der dahanca - v - studie wurden patienten mit plattenepithelkarzinomen des larynx und pharynx in konventioneller fraktionierung ( 6 , 5 wochen ) bis zu einer gesamtdosis von 66 bis 68 gy bestrahlt . die lokoregionale tumorkontrolle ( fnf jahre ) war bei den kontinuierlich bestrahlten patienten mit 41% signifikant besser als in der split - course - gruppe ( 30% )  . 
 [ 11 ] untersuchten den einfluss einer bestrahlungspause bei 864 patienten mit larynxkarzinom . 352 patienten hatten eine systematische pause von zwei wochen nach 50 gy ( split - course - therapie )  . 
in einer univariaten analyse konnte gezeigt werden , dass patienten mit einer pause signifikant schlechtere lokale kontrollraten hatten ( unterschied von 7% fr t1 - tumoren und 11% fr t2 - tumoren )  . 
bei den fortgeschrittenen larynxkarzinomen ( t3 / t4 ) ergaben sich keine wesentlichen unterschiede in der lokoregionalen tumorkontrolle ( 32% mit kontinuierlicher bestrahlung und 30% mit split - course - strahlentherapie )  . in einer retrospektiven untersuchung von levendag et al . [ 6 ] konnte an 1493 patienten mit kopf - hals - tumoren ( mundhhle , oropharynx , hypopharynx , nasopharynx , larynx ) gezeigt werden , dass patienten mit einem splitcourse - regime niedrigere lokale kontrollraten hatten als patienten , bei denen die strahlentherapie kontinuierlich durchgefhrt wurde . 
diese betrugen 31% fr patienten , die kontinuierlich bestrahlt wurden , und 21 , 5% fr patienten mit split - course - strahlentherapie und einer dauer autor tumor behandlung zahl der patienten pause ergebnis hansen et al . 1997 [ 3 ] van den bogaert et al . 
1995 [ 11 ] lokal fortgeschrittene pharynxund larynxkarzinome larynxkarzinome ( t1t2 ) kopf - hals - tumoren ( oropharynx , hypopharynx , larynx , nasopharynx ) undifferenzierte nasopharynxkarzinome ( t1t4 ) 84% t3 / t4 nasopharynxkarzinome levendag et al . 1996 [ 6 ] luo et al . 1994 [ 7 ] kwong et al . 1997 [ 5 ] cox et al . 1993 [ 1 ] konventionell 310 ohne pause 191 mit pause geplante pause von 3 wochen 4072 gy ( durchschnitt 66 gy ) konventionell 5079 gy ( durchschnitt 64 gy ) 512 ohne pause 352 mit pause geplante pause von 2 wochen 1493 nicht geplante unterbrechung 6072 gy konventionell 1093 ohne pause 353 mit pause 1045 tage ( durchschnittlich 28 , 6 tage ) 3 ( cid : 2 ) 3 , 5 gy / wo 229 ohne pause bis 59 , 5 gy 567 mit pause unterbrechung > 7 tage inoperable nichtkleinzellige bronchialkarzinome ( rtog 8311 , 8321 , 8403 ) 1244 5560 gy konventionell 6079 , 2 gy hyperfraktioniert willers et al . 1998 [ 12 ] inoperables bronchialstadium iiii 70 gy konventionell 59 tage 1013 tage 14 tage 724 wochen kajanti et al . 1995 [ 4 ] sophaguskarzinom t12 5071 gy konventionell 138 mit pause 215 ohne pause 3 wochen tabelle 1 . 
split - course radiotherapy and treatment interruptions clinical investigations . lokoregionale kontrolle ( 5 jahre ) 30% mit pause , 41% ohne pause lokoregionale kontrolle ( 3 jahre ) um 7% schlechter bei t1 und 11% schlechter bei t2 fr patienten mit pause lokale kontrollraten fr patienten mit splitcourse - technik niedriger als fr patienten ohne pause stadium iii / iv 5 - jahres - berleben 31% ohne pause vs . 
18 , 8% ( pause 3145 tage ) niedrigere lokale kontrolle und berleben fr patienten mit pause 2und 5 - jahres - berleben signifikant besser bei hyperfraktionierter radiotherapie ohne pause 33% + 15% vs . 
ein ungnstiger einfluss der prolongierten pause konnte in der split - course - gruppe , bezogen auf die lokoregionale tumorkontrolle und das erkrankungsfreie berleben , im rahmen einer stadienadaptierten univariaten analyse gefunden werden . 
 [ 1 ] gingen der frage nach , inwieweit sich der negative effekt einer bestrahlungspause auch beim inoperablen nichtkleinzelligen bronchialkarzinom bemerkbar macht . die datenbasis bildeten patienten , die zwischen 1983 und 1989 in drei randomisierten studien ( rtog 8311 , 8321 , 8403 ) behandelt wurden . 
in den rtog - studien 8321 und 8403 handelte es sich um konventionell fraktionierte behandlungen mit einzeldosen von 1 , 8 gy und 2 gy bis zu gesamtdosen von 55 bis 60 gy . 
insgesamt wurden 229 patienten ausgewertet , die einer definitiven strahlentherapie in konventioneller fraktionierung bis zu einer gesamtdosis von 70 gy zugefhrt wurden . nach einem ersten behandlungskurs ( 40 bis 50 gy ) erfolgte ein restaging , bevor ein zweiter behandlungszyklus mit 20 bis 30 gy appliziert wurde . 
die ein - , zweiund fnf - jahres - berlebensraten waren in den stadien t1 und t2 tendenziell schlechter fr die patienten mit splitcourse - therapie , zeigten aber keine statistische signifikanz . diskussion und schlussfolgerung die klinische bedeutung einer bestrahlungspause im hinblick auf das berleben und die lokalrezidivrate wurde nur in retrospektiven studien bei einer reihe von tumorentitten untersucht [ 1 , 5 , 6 , 12 ]  . 
erkrankungsfreies berleben lie sich bei patienten mit lokal fortgeschrittenen kopf - hals - tumoren und bronchialkarzinomen fr die behandlungsgruppe mit bestrahlungspause nachweisen [ 1 , 6 , 7 ]  . 
dies spricht dafr , dass die akzelerierte repopulierung klinisch durchaus von bedeutung ist . bei der behandlung von kopf - hals - tumoren zeigt insbesondere eine studie , dass die behandlungsergebnisse vor allem bei gut bis mig differenzierten karzinomen signifikant besser sind , wenn die bestrahlung ohne pause erfolgt [ 3 ]  . diese beobachtung lie sich in der chartstudie ebenfalls nachvollziehen , bei der die gut differenzierten tumoren die beste lokoregionale tumorkontrolle erzielten . 
interruptions of high - dose radiation therapy decrease long - term survival of favorable patients with unresectable non - small cell carcinoma of the lung : analysis of 1244 cases from 3 radiation therapy oncology group ( rtog ) trials . 
int j radiat oncol biol phys 1994 ; 30 : 11079 . unter bercksichtigung dieser datenlage stellt sich die frage , in welcher grenordnung die verlorene dosis pro tag behandlungspause liegt . 
aufgrund einzelner daten bei kopf - halstumoren knnen dosen von 0 , 4 bis 0 , 8 gy pro tag als schtzbereich angenommen werden [ 9 , 13 ]  . 
115 patienten mit einem histologisch gesicherten primren rektumkarzinom ohne hinweis auf eine fernmetastasierung und einer endosonographisch ermittelten tiefeninfiltration von mindestens t3 wurden einer properativen radiochemotherapie im zeitraum 3 / 1993 bis 10 / 1999 unterzogen . 
bei 57 patienten ( 53% ) zeigte sich nach vortherapie keine vernderung des lymphknotenstatus , whrend bei elf patienten ( 10% ) , die primr als un0 eingeschtzt wurden , lymphknotenmetastasen nachweisbar waren . 
bercksichtigt man jedoch die problematik der genauigkeit prtherapeutischer stagingverfahren , so kann angenommen werden , dass therapiebedingte wartezeiten beim rektumkarzinom hchstens fr sehr wenige , einzelne patienten von prognostischem nachteil sind . schlsselwrter : rektumkarzinom properative radiochemotherapie lokaler tumorprogress fernmetastasierung the importance of delay in tumor patients exemplified by the pretreatment of locally advanced rectal cancer background : with the intention to achieve tumor reduction and thereby increase r0 - resection rate , preoperative radiochemotherapy is increasingly applied in locally advanced rectum cancer . 
along with the advantages of prior therapy , a delay of surgical treatment occurs which might despite continuing therapy give way to local tumor progression or metastatic disease . patients and methods : since 1993 we have treated locally advanced rectum carcinomas by preoperative radiotherapy according to a preoperative study protocol . 
hundred and fifteen patients with histologically proven primary rectum carcinoma without evidence of regional or distant metastases and endosonographically determined infiltration depth of stage t3 or more underwent preoperative radiochemotherapy between 3 / 1993 and 10 / 1999 . 
distant metastatic manifestations were excluded by radiography and ultrasound scanning . 1 charit , campus buch , humboldt - universitt zu berlin , robert - rssle - klinik , klinik fr chirurgie und chirurgische onkologie , 2 charit , campus virchow - klinikum , humboldt - universitt zu berlin , radiologie und strahlenklinik , 3 charit , campus virchow - klinikum , humboldt - universitt zu berlin , medizinische klinik und poliklinik . eingang des manuskripts : 28 . 
fifty - seven patients ( 53% ) showed no change in lymphonodal status after preoperative therapy , whereas lymphonode metastases were detected in 11 patients ( 10% ) who were judged un0 preoperatively . 
considering the lack of precision in pretherapeutic staging diagnostics , we conclude that delays due to therapeutic regimen are responsible for prognostic disadvantage in only a small number of patients . key words : rectum carcinoma preoperative radiochemotherapy local progress distant metastases d er r0 - resektion kommt fr den weiteren tumorfreien verlauf von patienten mit gastrointestinalen tumoren eine wesentliche bedeutung zu . 
verschiedene autoren konnten nachweisen , dass durch eine properative therapie nicht nur eine deutliche tumorverkleinerung erreicht werden konnte [ 12 ] , sondern auch initial als nicht resektabel eingeschtzte rektumkarzinome durch eine vortherapie resektabel wurden [ 2 ]  . 
darber hinaus wird dadurch eine hhere rate an sphinktererhaltenden eingriffen erwartet [ 8 , 10 , 17 ]  . den vorteilen der vorbehandlung steht eine wartezeit , die sich von der therapieentscheidung bis zur endgltigen tumorentfernung erstreckt , gegenber . 
ber die auswirkung einer bewusst in kauf genommenen verzgerung durch eine vorbehandlung des rektumkarzinoms findet man in den bisher publizierten studien wenig angaben [ 4 , 9 , 11 , 13 , 15 , 16 ]  . 
eine fernmetastasierung auftritt , sollte daher anhand des eigenen krankengutes analysiert werden . patienten und methode 115 patienten mit einem histologisch gesicherten primren rektumkarzinom ohne hinweis auf eine fernmetastasierung und einer endosonographisch ermittelten tiefeninfiltration von mindestens t3 wurden einer properativen radiochemotherapie im zeitraum 3 / 1993 bis 10 / 1999 unterzogen . 
davon wurden 108 patienten ( 88 patienten ut3 , 20 patienten ut4 ) operiert und konnten hinsichtlich des tumoransprechens auf die vortherapie untersucht werden . die systemische chemotherapie bestand aus zwei zyklen : der erste zyklus lief von tag 1 bis 5 , der zweite zyklus von tag 22 bis 28 . 
im ersten zyklus wurde 5fluorouracil mit 300 mg / m2 / d dosiert , diese dosis wurde bei gleichbleibender leukovorinmenge ( 50 mg ) im zweiten zyklus auf 350 mg / m2 / d erhht . 
direkt im anschluss hieran wurde ber drei stunden 5 - fluorouracil infundiert . die properative bestrahlung umfasste den primrtumor mit einer sicherheitszone von 2 cm ( zielvolumen erster ordnung ) sowie die regionalen lymphabflussgebiete ( zielvolumen zweiter ordnung )  . 
es wurde angestrebt , die tumorregion und die lokoregionalen lymphabflusswege in einer rechnergesttzten mehrfeldertechnik mit einer zielvolumendosis von 5 ( cid : 2 ) 1 , 8 gy bis zu 45 gy zu bestrahlen . die resektion des rektumkarzinoms erfolgte vier bis sechs wochen nach der fnfwchigen radiochemotherapie . vor und nach der properativen therapie erfolgte zur lokalen responsebeurteilung eine endorektale ultraschalluntersuchung und bei stenosierenden tumoren eine computertomographie bzw . 
bei 40 patienten ( 37% ) erfolgte zustzlich prtherapeutisch eine staginglaparoskopie inklusive laparoskopischem ultraschall . ergebnisse die durchschnittliche wartezeit vom zeitpunkt der entscheidung zur properativen therapie bis zur operation betrug 75 tage ( 10 , 7 wochen ) , wobei die mittlere wartezeit nach beendigung der radiochemotherapie 40 16 tage ( 5 , 7 wochen ) war . 
bei 22 patienten ( 20 , 4% ) lag die mittlere wartezeit nach radiochemotherapie bei ber 42 tagen . eine reduktion der tumorinfiltrationstiefe ( ypt < ut ) wurde insgesamt bei 55 von 108 patienten ( 51% ) festgestellt ( tabelle 1 )  . 
lediglich bei drei patienten ( 3% ) mit einem initialen ut3 - tumor wurde nach vortherapie eine progredienz der infiltrationstiefe des tumors histologisch ( ypt4 ) festgestellt . vernderungen bezglich des lymphknotenstatus vor und nach radiochemotherapie sind in tabelle 2 zusammengefasst . 
bei 57 patienten ( 53% ) zeigte sich nach vortherapie keine vernderung des lymphknotenstatus , whrend bei elf patienten ( 10% ) , die primr als un0 eingeschtzt wurden , lymphknotenmetastasen nachweisbar waren . insgesamt wurden bei acht patienten nach properativer radiochemotherapie fernmetastasen entdeckt . 
dieser patient verstarb nach zwlf monaten an progredientem lokalrezidiv . lymphknotenbefall un0 n = 40 unpos . n = 68 gesamt regression befundkonstanz progress 29 / 40 ( 73% ) 11 / 40 ( 27% ) 40 / 68 ( 59% ) 28 / 68 ( 41% ) 40 / 108 ( 37% ) 57 / 108 ( 53% ) 11 / 108 ( 10% ) tabelle 2 . 
welche gefahren hieraus tatschlich resultieren , ist bisher noch wenig untersucht worden [ 1 , 14 ]  . unsere ergebnisse hinsichtlich lokalem und systemischem progress unter vortherapie stimmen mit den daten von hyams [ 6 ] berein , obwohl unsere durchschnittliche wartezeit von elf wochen um 16 wochen geringer war . 
eine therapieverzgerung whrend der vortherapie , wie sie bei 6% unserer patienten auftrat , hat offensichtlich insgesamt keinen weiteren negativen einfluss . die grnde fr einen tumorprogress knnen vielfltig und ausdruck einer ungnstigen tumorbiologie sein , andererseits ist auch ein scheinbarer progress vorstellbar . 
dabei fllt nicht nur eine unterscheidung zwischen tumorsen und entzndlichen lymphknoten unmittelbar perirektal schwer , auch knnen die entfernteren lymphknoten entlang der arteria und vena rectalis superior mit dieser methode nicht beurteilt werden . ein systemischer progress von 6% erscheint auf den ersten blick hoch . 
dabei wird sowohl das computertomogramm als auch der ultraschall bei einer lebermetastasengre unter 5 mm ungenau . auch die problematik bei der diagnose einer wenig ausgeprgten peritonealkarzinose mittels bildgebender verfahren ist bekannt . 
zwei von drei patienten mit einer spter diagnostizierten peritonealkarzinose hatten keine laparoskopie und knnten damit ausdruck eines nur scheinbaren progresses se die laparoskopie kann in vielen , wenn auch nicht in allen fllen eine peritonealkarzinose diagnostizieren und so einer fehleinschtzung vorbeugen . ein tumorprogress whrend der vortherapie beim rektumkarzinom lsst sich sicher nicht vollstndig vermeiden . bercksichtigt man jedoch die problematik der genauigkeit prtherapeutischer stagingverfahren , so kann angenommen werden , dass therapiebedingte wartezeiten beim rektumkarzinom hchstens fr sehr wenige einzelne patienten von prognostischem nachteil sind . 
a clinical trial to evaluate the worth of preoperative multimodality therapy in patients with operable carcinoma of the rectua progress report of national surgical adjuvant breast and bowel protocol ( nsabp ) r - 03 . 
die wahrscheinlichste ursache dieses zeitfaktors ist die proliferation klonogener tumorzellen whrend der therapie . durch eine gezielte hemmung der proliferation klonogener zellen whrend einer strahlenbehandlung knnten daher mglicherweise wesentliche fortschritte in der radioonkologie erreicht werden . 
 methodik : in einer kurzen bersicht werden die mglichkeiten zur minimierung des zeitfaktors diskutiert . ergebnisse und schlussfolgerungen : eine hemmung der proliferation klonogener tumorzellen whrend der bestrahlung durch simultane chemotherapie , durch blockade proliferationsstimulierender signaltransduktionswege oder durch pharmakologische inhibition der tumorneoangiogenese ist wissenschaftlich interessant , jedoch in ihrer wirksamkeit zur minimierung des zeitfaktors auf die ergebnisse einer strahlentherapie bislang nicht belegt . 
important progress in radiation oncology might therefore be expected from inhibition of proliferation of clonogenic cells during radiation treatment . methods : possibilities to minimize the time factor are briefly discussed . results and conclusions : inhibition of proliferation of clonogenic tumor cells during irradiation by simultaneous chemotherapy , by inhibition of signal transduction pathways that stimulate proliferation , or by pharmacological inhibition of angiogenesis are scientifically interesting but currently not proven to be effective to counteract the loss of local tumor control with increasing overall treatment of fractionated irradiation . 
by accelerated fractionation and by prevention or compensation of unscheduled treatment gaps . key words : time factor of fractionated radiotherapy proliferation repopulation accelerated fractionation chemotherapy egf - receptor inhibition antiangiogenic therapy 1 st . 
nach 200 mg / kg cyclophosphamid nahm die zahl klonogener zellen pro tumor erheblich ab , blieb danach fr zwei wochen konstant und stieg dann mit der doppelten geschwindigkeit im vergleich zum unbehandelten tumor wieder an . 
dies zeigt , dass eine chemotherapie ebenso wie eine strahlentherapie zu einer akzelerierten repopulierung solider tumoren fhren kann . ob dieses phnomen fr alle oder nur fr bestimmte tumoren zutrifft , ob es bezglich dieses effektes unterschiede zwischen verschiedenen chemotherapeutika gibt , ob die verzgerung vor beginn der akzelerierten bestrahlung immer zwei wochen betrgt und ob die mechanismen der akzelerierten repopulierung nach chemotherapie dieselben sind wie nach bestrahlung , ist ungeklrt . 
es liegt nahe , die enttuschenden klinischen ergebnisse einer neoadjuvanten chemotherapie vor strahlentherapie von kopf - hals - tumoren [ 5 , 17 ] auf die induktion akzelerierter repopulierung durch das chemotherapeutikum zurckzufhren . 
durch analogieschlsse aus ergebnissen an normalgewebsexperimenten kann man vermuten , dass mit einer repopulierungshemmenden wirkung eher bei antibiotischen zytostatika gerechnet werden kann als bei alkylanzien oder platinderivaten . ausschaltung der proliferation durch blockade proliferationsstimulierender signaltransduktionswege der epidermal growth factor receptor ( egfr ) und seine liganden egf und tgf sind wichtige bestandteile proliferationsregulierender signaltransduktionswege . 
folgerichtig sollte durch die hemmung des egfr - systems der einfluss der gesamtbehandlungszeit auf die tumorkontrolle zu vermindern sedie wenigen bisher vorliegenden experimentellen befunde zeigen eine verlngerte wachstumsverzgerung von experimentaltumoren nach kombinierter egfr - blockade und bestrahlung [ 8 ] und eine reduktion des anteils von zellen in der s - phase des zellzyklus sowie eine herabgesetzte proliferationsrate von tumorzellen durch egfr - blockade in vitro [ 6 ]  . 
selbst wenn eine verminderung der proliferationsrate durch diesen mechanismus erreicht werden knnte , wre das noch keine evidenz fr eine verminderte repopulierungsrate klonogener tumorzellen , denn diese ist weitgehend unabhngig von der proliferationsrate der gesamtheit der tumorzellen [ 7 ]  . whrend einer fraktionierten bestrahlung sagt die gemessene proliferationsrate nichts ber die aktuelle repopulierungsrate aus [ 1 , 10 ]  . 
experimente , die gezielt den einfluss einer egfr - blockade auf die proliferation rezidivfhiger klonogener tumorzellen whrend onkologischer therapie untersuchen , sind daher unbedingt notwendig . ausschaltung der proliferation durch aushungern : hemmung der angiogenese das wachstum von tumoren ber ein sehr kleines volumen von etwa 1 mm3 hinaus hngt von der neubildung von gefen ab . 
neuere experimentelle untersuchungen weisen darauf hin , dass zwar die nekrotischen tumoranteile durch eine hemmung der angiogenese zunehmen , in den vitalen tumorarealen , in denen weiterhin gefe vorhanden sind , die proliferationsgeschwindigkeit der tumorzellen jedoch unverndert bleibt [ 11 ]  . 
da die therapeutisch relevante akzelerierung der repopulierung vermutlich erst gegen ende der strahlentherapie erfolgt , wenn die zahl rezidivfhiger klonogener tumorzellen auf wenige tausend gesunken ist und durch die bis dahin akkumulierte strahlendosis die proliferationsfhigkeit der endothelzellen und damit die fhigkeit zur neoangiogenese wesentlich eingeschrnkt ist , findet das maximum der repopulierung mglicherweise bei einem minimum an angiogenese statt . 
methoden zur minimierung des zeitfaktors der vorstellung einzusetzen , die repopulierung whrend einer strahlentherapie zu hemmen , einer experimentellen berprfung . schlussfolgerungen die einzige derzeit gesicherte methode zur minimierung des einflusses der proliferation klonogener tumorzellen auf die ergebnisse einer strahlenbzw . 
 ergebnisse : zwischen immunhistochemisch p53 - positiven ( 10% angefrbte zellen ) und p53 - negativen ( < 10% angefrbte zellen ) tumoren fand sich weder fr den po2 - median noch fr die relative anzahl von werten 5 mm hg ein statistisch signifikanter unterschied . 
zu experimentellen und klinischen ergebnissen , die bei anderen tumorentitten zeigen , dass hypoxie zu einer p53 - vermittelten steigerung der malignitt fhrt , ergibt sich trotzdem kein prinzipieller widerspruch . die in unserer studie adquate oxygenierung von p53 - positiven und p53 - negativen tumoren reflektiert sich in einer vergleichbaren klinischen tumoraggressivitt beider gruppen . 
 schlsselwrter : p53 - berexpression hypoxie kopf - hals - karzinome no association between p53 - overexpression and polarographically measured tumor oxygenation in patients with head and neck carcinomas purpose : clinical investigation of a potential relationship between the polarographically measured tumor oxygenation and the p53 status in patients with squamous cell carcinoma of the head and neck . patients and methods : in 99 patients with mostly advanced , histologically proven squamous cell carcinoma of the head and neck we estimated the classical tumor parameters ( tnm stage , histological grading ) the immunohistochemical p53overexpression ( do - 7 ) and the tumor oxygenation status ( eppendorf po2 histograph )  . 
the tumor volume and the hemoglobin concentration were evaluated simultaneously . results : no statistically significant difference could be detected between immunohistological p53 - positive ( p53 10% stained cells ) and p53 - negative tumors ( p53 < 10% stained cells ) regarding both the median po2 and the relative frequency of values 5 mm hg . 
moreover , no statistically relevant differences could be seen between both p53 - groups considering the hemoglobin concentration , the tnm stage , the histological grading and the tumor volume . conclusion : our data imply that there is no association between p53 - overexpression and tumor hypoxia in head and 1 klinik fr strahlentherapie und 2 pathologisches institut der martin - luther - universitt , halle - wittenberg , 3 klinik fr radioonkologie und 4 pathologisches institut der technischen universitt mnchen . die arbeit wurde zu teilen durch die deutsche krebshilfe und durch die dfg untersttzt . eingang des manuskripts : 2 . 
however , this is not necessarily in contradiction to experimental or clinical data that confirmed a relationship between hypoxia and p53 - mediated increased malignancy of tumor cells in other tumor entities . 
 key words : p53 hypoxia head and neck carcinomas m it hilfe polarographischer messmethoden war es bei plattenepithelkarzinomen der zervixund der kopfhals - region in den letzten jahren mglich zu zeigen , dass hypoxische tumoren auf eine primre radioonkologische therapie signifikant schlechter ansprechen als ihre besser oxygenierten pendants [ 16 , 20 , 26 ]  . 
 [ 11 ] belegt , dass sauerstoffmangel im tumor einen selektionsdruck hervorruft , der jenen zellen einen berlebensvorteil verschafft , die aufgrund von p53 - mutationen ihr apoptotisches potential verloren haben . 
 ziel der vorliegenden arbeit war es , bei patienten mit plattenepithelkarzinomen der kopf - hals - region zu prfen , ob sich auch klinisch eine beziehung zwischen tumoroxygenierung und p53 - status nachweisen lsst bzw . 
 schen universitt mnchen 99 patienten mit berwiegend fortgeschrittenen , histologisch gesicherten plattenepithelkarzinomen der kopf - hals - region vor therapiebeginn ( primre radioonkologische behandlung oder chirurgie adjuvante radioonkologische therapie ) in die studie einbezogen . 
jede einzelne tumorlokalisation ( primrtumor und alle metastasen ) wurden dreidimensional ausgemessen und mit hilfe der rotationsellipsoidformel das jeweilige volumen berechnet ( 1 / 6 ( cid : 2 ) a ( cid : 2 ) b ( cid : 2 ) c )  . 
nur im fall des unbekannten primrtumors basierte die bestimmung auf entsprechendem material aus einem betroffenen lymphknoten . alle untersuchungen erfolgten im pathologischen institut der martin - luther - universitt halle - wittenberg durch einen pathologen , der hinsichtlich der tumoroxygenierung bzw . 
 nach der auswahl reprsentativer proben des in 4%igem formalin fixierten materials wurden 3 bis 4 m starke gewebsschnitte auf mit poly - l - lysin beschichtete , kommerziell erhltliche objekttrger aufgezogen . 
der peroxidasenmarkierung mit einem biotinilierten sekundrantikrper mittels der avidin - biotin - komplexmethode ( vectastain - elite - abc - kit , vector laboratories , burlingame , usa ) folgten die sichtbarmachung der peroxidasereaktion am avidin - biotin - komplex mit 3 , 3 - diaminobenzidin ( dab ) als chromogen und anschlieende frbung der schnittprparate mit hmatoxyl die menge der p53 exprimierenden zellen wurde in den abschnitten mit der besten anfrbung durch die auszhlung von jeweils mindestens 300 zellen bestimmt und in prozent angegeben . 
in bereinstimmung mit der literatur wurden tumoren als p53positiv ( + p53 ) gewertet , wenn sie 10% p53 - angefrbte tumorzellen enthielten [ 9 , 15 , 18 , 23 , 25 , 32 ]  . 
in allen anderen fllen erfolgte eine zuordnung in die p53 - negative gruppe ( p53 )  . hmoglobinbestimmung da bei kopf - hals - karzinomen krzlich eine beziehung zwischen tumor - po2 und hmoglobinkonzentration im blut nachgewiesen werden konnte , wurde der hmoglobinwert als indirekte kontrollgre der tumoroxygenierung in die untersuchung einbezogen [ 5 ]  . 
aus diesem grund sind alle p - werte als deskriptiv zu werten [ 1 ]  . ergebnisse bei 71 patienten ( 71 , 7% ) erwiesen sich die untersuchten tumoren als immunhistochemisch p53 - positiv ( 10% angefrbte zellen )  . 
in 28 fllen ( 28 , 3% ) war ein nachweis von p53 entsprechend den gewhlten kriterien nicht mglich ( < 10% angefrbte zellen )  . der auf basis der jeweiligen po2 - median - werte aller tumoren bestimmte durchschnittliche po2 - median betrug 14 mm hg ( 95% - konfidenzintervall [ 95%ki ] : 11 bis 16 mm hg , spanne : 0 bis 59 mm hg )  . 
 die p53 - positiven tumoren hatten durchschnittlich einen po2 - median von 15 mm hg ( 95%ki : 12 bis 18 mm hg , spanne : 0 bis 59 mm hg ) und einen relativen anteil von werten 5 mm hg von 32% ( 95%ki : 25 bis 38% , spanne : 0 bis 92% )  . 
bei p53 - negativen tumoren wurde im mittel ein po2median von 12 mm hg gemessen ( 95%ki : 7 bis 16 mm hg , spanne : 0 bis 47 mm hg ) , und die relative anzahl von messwerten 5 mm hg lag im durchschnitt bei 36% ( 95%ki : 25 bis 47% , spanne : 0 bis 90% )  . 
der tendenziell bessere oxygenierungsstatus von p53 - positiven tumoren erreichte weder p53 - positive tumoren p53 - negative tumoren p53 - positive tumoren p53 - negative tumoren abbildung 1a figure 1a abbildung 1b figure 1b abbildungen 1a und 1b . 
p53 - berexpression und tumoroxygenierung fr den po2 - median noch fr die relative anzahl von werten 5 mm hg ein statistisch signifikantes niveau ( abbildung 1 )  . hinsichtlich der einzelnen kriterien der tnm - klassifikation , des histologischen gradings und des tumorvolumens fanden sich zwischen p53 - positiven und p53 - negativen tumoren keine statistisch relevanten unterschiede . 
patient characteristics and comparison of classical tumor parameters , of tumor volume as well as hemoglobin concentration regarding p53 - positive and p53 - negative tumors . se an der assoziation von p53 und hypoxie resultiert aus der biologischen funktion dieses tumorsuppressorgens . whrend es im normalen proliferationsgeschehen anscheinend eine eher untergeordnete rolle spielt , wird es in stresssituationen aktiviert . 
das spektrum der exogenen stimuli , die zur p53 - expression fhren , ist breit gefchert und umfasst wahrscheinlich alle potentiell die integritt des genoms gefhrdenden faktoren ( zum beispiel ionisierende strahlung , chemische mutagene , hyperthermie , virale onkoproteine , hypoxie )  . 
in normalen zellen liegt das p53 - protein in sehr geringen konzentrationen vor , und erst als adaptive intrazellulre antwort auf stressfaktoren steigt seine konzentration auf ein vielfaches an [ 22 ]  . 
funktionell ist p53 ein wichtiger sensor von dna - schdigungen und aktiviert prozesse , die entweder die reparatur des defekts ermglichen ( g1 - arretierung des zellzyklus ) oder zur eliminierung der betroffenen zelle fhren ( apoptose )  . 
kritisch wird die situation , wenn es zur inaktivierung von p53 durch mutationen kommt , einem vorgang , der in 40 bis 50% menschlicher tumorzellen durch analysen des genetischen status nachvollziehbar ist [ 14 ]  . 
man kann deshalb davon ausgehen , dass p53 - mutationen zwar nicht das initiale ereignis der kanzerogenese darstellen , aber kausal an der entwicklung und entdifferenzierung von tumoren beteiligt sind . 
 [ 11 ] in vitro zeigen , dass zellverbnde mit wildtyp - p53 auf hypoxie mit apoptose reagierten , whrend ihre p53 - mutierten korrelate im gleichen ansatz grtenteils berlebten . 
erste klinische hinweise auf einen p53 - bedingten selektionseffekt der tumorhypoxie wurden fr eine kleine gruppe von mammakarzinompatienten publiziert [ 13 ]  . bei der formulierung der basishypothese unserer studie sind wir davon ausgegangen , dass hnliche phnomene prinzipiell auch bei kopf - hals - karzinomen nachweisbar sein mssten . 
im falle einer assoziation von polarographisch gemessener hypoxie und p53 - status wre es mit hilfe der eppendorf - po2 - sonde potentiell mglich , nicht nur die strahlentherapeutisch relevante hypoxie der tumoren zu bestimmen , sondern indirekt auch hinweise auf die aggressivitt der malignome zu gewinnen . 
im widerspruch zu allen vorliegenden experimentellen und klinischen daten fand sich jedoch in unserem patientengut keine statistisch relevante beziehung von p53 - status und tumoroxygenierung . auch bezglich des kontrollparameters fr den oxygenierungsstatus , der hmoglobinkonzentration , konnten keine effekte nachgewiesen werden . 
p53 - berexpression und tumoroxygenierung obwohl die po2 - histographie mit der eppendorf - sonde gegenwrtig als goldstandard bei der klinischen bestimmung der tumoroxygenierung betrachtet wird , hat sie eine reihe nicht unwesentlicher nachteile . 
der selektive effekt der akuten hypoxie ist wahrscheinlich zu vernachlssigen . fr die validitt der messmethode sprechen hingegen die mit baugleichen po2 - histographen in der klinik gewonnenen daten , welche zeigen , dass hypoxie unabhngig von der therapie ( alleinige chirurgie , radioonkologische behandlung chirurgie ) mit einer gesteigerten tumoraggressivitt einhergeht ( krzeres berleben , verminderte lokale kontrolle , erhhte rate an fernmetastasen , ungnstigeres histologisches grading ) [ 7 , 13 , 16 , 20 , 26 ]  . 
der bei rektumkarzinomen besttigte gleichsinnige p53 - status in biopsien und in den spter analysierten operationsprparaten lsst jedoch eine gewisse homogenitt der p53 - expression im gesamten tumor vermuten [ 2 , 24 , 28 ]  . der von uns verwendete antikrper do - 7 ist p53 - panreaktiv , das heit , er markiert sowohl den wildtyp als auch die mutierte form des proteins . 
insbesondere zu beginn der klinischen p53 - analysen ist man davon ausgegangen , dass wildtyp - p53 aufgrund seiner kurzen halbwertszeit im gegensatz zu mutierten varianten immunhistochemisch nicht nachweisbar ist [ 6 , 22 ]  . 
eine reihe von autoren konnte zeigen , dass der nachweis einer p53 - berexpression nicht zwangslufig mit einer p53 - mutation assoziiert ist [ 2 , 32 , 33 ]  . 
wildtypp53 kann auer durch mutationen auch durch komplexbildung mit viralen proteinen ( zum beispiel e1b - , e6 - protein der hpv - 16 / 18 - viren ) sowie durch die bindung an zellulres mdm - 2 - protein stabilisiert und inaktiviert werden [ 6 , 22 ]  . 
betrachtet man die meisten zur relation p53 - berexpression und mutation publizierten literaturdaten , wird deutlich , dass eine berexpression ohne mutation nicht ungewhnlich ist [ 2 , 6 , 22 , 32 , 33 ]  . 
festigen sich diese daten in weiteren untersuchungen , knnte das heien , dass in frher publizierten arbeiten p53 - mutationen infolge einer selektiven sequenzierung bersehen worden sind und auch dort mglicherweise eine engere beziehung zwischen mutation und berexpression bestand , als zunchst angenommen . die kritische wertung der methoden zusammenfassend , sind wir der meinung , dass die in der studie erlangten ergebnisse nicht allein auf methodische unzulnglichkeiten zurckgefhrt werden knnen , sondern zu wesentlichen teilen ein reales biologisches phnomen widerspiegeln , das es zu interpretieren gilt . betrachtet man die vermeintlichen widersprche zu den experimentellen daten , muss auf einen wesentlichen punkt hingewiesen werden . 
hier ist interund intratumoral eher eine mischung verschiedener mutationen zu erwarten , aus der sich mehr chancen ergeben , einem hypoxievermittelten selektionsdruck auszuweichen . tumoren , die nicht mit p53 - mutationen einhergehen , sttzen dieses konzept . 
wenn man davon ausgeht , dass p53 im rahmen der apoptose erst relativ spt zum tragen kommt , besteht die mglichkeit , dass dieser prozess auch durch vorgeschaltete , bereits mutierte gene verhindert werden kann ( zum beispiel n - myc - onkogen beim neuroblastom )  . 
bei kopf - hals - karzinomen betrgt die prvalenz des hpv - virus je nach studie 0 bis 82% [ 27 ]  . in jngster zeit gibt es berdies vermehrt hinweise darauf , dass die bedeutung der apoptose bei plattenepithelkarzinomen berund die des p53 - unabhngigen mitosetods unterschtzt wird [ 8 ]  . 
dies entsprche auch dem prinzip der konvergenten evolution , das besagt , dass ein analoger selektionsdruck zu einem vergleichbaren phnotyp fhrt , aber nicht zwangsweise mit einem identischen genotyp einhergehen muss [ 12 ]  . 
klinisch findet dieser sachverhalt seine besttigung in den sehr differenten ergebnissen von studien , die sich mit der prognoserelevanz einer p53 - berexpression bei hno - tumoren befasst haben [ 15 , 18 , 21 , 23 , 25 , 29 , 32 ]  . 
p53 - berexpression und tumoroxygenierung zusammenfassend kann gesagt werden , dass die prsentierten ergebnisse gegen eine assoziation von p53 - berexpression und tumorhypoxie bei kopf - hals - karzinomen sprechen . 
prognostic significance of clinical parameters and biological markers in patients with squamous cell carcinoma of the head and neck treated with concurrent chemoradiotherapy . clin cancer res 1999 ; 5 : 8016 . 
 conclusions : the new 3d hdr brachytherapy technique , combined with 3d external irradiation and androgen deprivation , is a feasible , so far well tolerated and effective treatment in the short - time follow - up of median 18 months . key words : prostate cancer hdr brachytherapy 3d external beam radiotherapy androgen deprivation dosevolume histograms interstitielle 3d - hdr - brachytherapie kombiniert mit externer 3d - radiotherapie und androgendeprivation beim prostatakarzinom : erste ergebnisse hintergrund : auswertung der praktikabilitt , vertrglichkeit und effektivitt einer neuen interstitiellen 3d - hdrbrachytherapie - technik , kombiniert mit externer 3d - radiotherapie und androgendeprivation beim prostatakarzinom . patienten und methoden : von januar 1997 bis august 1998 behandelten wir 35 patienten mit prostatakarzinomen im stadium ct13 n0 m0 . 
 schlussfolgerung : die neue 3d - hdr - brachytherapie - technik , kombiniert mit externer 3d - radiotherapie und androgendeprivation , stellt eine praktikable , bisher gut vertrgliche und effektive therapiemodalitt nach kurzzeitnachbeobachtung von median 18 monaten dar . 
 schlsselwrter : prostatakarzinom hdr - brachytherapie externe 3d - radiotherapie androgendeprivation dosis - volumen - histogramme p rostate cancer is one of the major health problems in europe and the united states . 
however , the american prostate cancer guidelines panel has analyzed all available literature data on radiation and surgical treatment series and concluded that there was no clear - cut evidence for the superiority of any one treatment [ 18 ]  . 
with the introduction of the routinely use of posttreatment psa level and postradiation biopsies it has been shown that permanent eradication of prostate cancer after external beam radiation is not achieved as often as previously believed [ 22 , 24 ]  . 
dose escalation trials performing 3d conformal ebrt alone are currently underway to determine the optimal increase in radiation dose to the prostate without increasing late side effects . interstitial brachytherapy is the alternative conformal treatment modality with the possibility to deliver a high dose precisely to the prostate gland and to spare at the same time organs at risk because of the steep dose gradient . 
but ldr brachytherapy is indicated only in patients with organ confined disease , a low initial psa level and a low gleason score because of inherent technical and radiobiological problems . 
in the 1990s high - dose rate ( hdr ) brachytherapy using temporary ir - 192 implants has become a well established conformal treatment combined with 3d conformal ebrt [ 1 , 13 , 23 ]  . 
additionally we have integrated neoadjuvant and adjuvant androgen deprivation in our treatment concept with the aim to achieve a significant volume reduction of the prostate gland before brachytherapy and to increase the efficiency using the combined modality [ 6 , 26 ]  . in this publication we report the combined treatment modality , including our new prostate brachytherapy technique , and the preliminary results in 35 patients with localized adenocarcinoma of the prostate . patients and methods patients between january 1997 and august 1998 a total of 35 patients with localized prostate cancer , without distant and lymph node metastases , were treated in our department using the combination of 3d interstitial hdr brachytherapy , 3d external beam irradiation and androgen deprivation . 
the mean age of the patients was 69 years ( range 57 to 78 years )  . pretreatment investigations included digital rectal examination , transrectal ultrasound and serum psa level . 
follow - up examinations included digital rectal examination , trus and serum psa level on a 3 - monthly basis during the first posttreatment year and thereafter every 6 months . 
 methods in our department we routinely use computed tomography ( ct ) for hdr brachytherapy planning in order to image the target volume and also the adjacent critical structures [ 12 , androgen deprivation : all patients received different hormonal treatments for neoadjuvant androgen deprivation prior to interstitial brachytherapy . 
hormonal treatment continued in all patients for adjuvant androgen deprivation simultaneously to brachytherapy and external beam irradiation and was stopped 3 months after external beam radiotherapy . 3d interstitial hdr brachytherapy : all patients received 4 fractions of 3d interstitial hdr brachytherapy in 6 weeks . the time between each fraction was 14 days . 
for the transrectal implantation procedure the patient was placed in lithotomy position and received an antibiotic prophylaxis using 120 mg gentamyc 50 mg pethidin iv and 5 mg midazolam iv were given for a sedation analgesic premedication . the new transrectal implantation technique for hdr brachytherapy was performed in a similar way as the technique for transrectal prostate biopsy . 
the contours of the planning target volume ( ptv ) and the critical tissues ( urethra , rectum ) were defined on all ct slices . the ptv was defined as the whole prostate gland . 
using various options we could evaluate this 3d image in all sections , including rotation , zooming and changing the degree of transparency of the objects ( figure 2 )  . 
3d interstitial hdr brachytherapy for prostate cancer the median follow - up at the time of evaluation of posttreatment psa level and toxicity was 18 months ( range 12 to 28 months )  . analysis of dose - volume histograms in hdr brachytherapy toxicity the transrectal implantation procedure was very well tolerated by all patients under sedation analgesic premedication . we noted no serious bleeding or acute complications during any of the implantations . 
one of the 35 patients developed a periprostatic hematoma 2 days after implantation which required surgical intervention , but he could continue with brachytherapy 2 weeks later . acute side effects were evaluated according to the rtog / eortc toxicity criteria . 
we have analyzed all 140 dvhs in our series for the coverage of the ptv by the reference dose , for the maximum and mean doses to the rectum and the maximum and mean doses to the urethra . 
of patients acute gastrointestinal toxicity acute urinary grade 1 grade 2 grade 3 grade 1 grade 2 grade 3 late urinary grade 1 grade 2 grade 3 grade 1 grade 2 grade 3 late gastrointestinal figure 2 . 
 therapy dose was 26 to 28 gy or 45.0 gy , if brachytherapy dose was 20 to 24 gy . results biochemical control the posttreatment psa levels dropped to less than 1.5 ng / ml in 29 / 32 patients ( 91% )  . 
the distribution of the posttreatment psa levels is given in table 2 . according to the definition of biochemical failure after radiotherapy of the astro consensus panel [ 2 ] we noted 2 / 32 patients ( 6% ) with biochemical relapse in our series . 
mittelwerte fr die erfassung des planungszielvolumens durch die referenzdosis sowie fr die maximale und mittlere dosisbelastung von rektum und urethra . discussion the surgical treatment of localized prostate cancer using radical prostatectomy still remains one of the most effective therapies with 10 - year survival rates of 65 to 77% in stages t1 / t2 and 38% in stage t3 [ 19 , 29 ]  . 
 to improve local control and survival rates after definitive radiotherapy , an increasing of the total radiation dose can be considered , but an increased external beam dose will at the same time increase the toxicity rate . 
this seems to be a promising conformal approach , but long - term results of local control , survival and late side effects are not yet available . interstitial brachytherapy is another attractive conformal treatment modality which aims to improve the treatment outcome in localized prostate cancer . 
ldr brachytherapy using permanent implants of iodine - 125 or palladium - 103 seeds has been used in the last 30 years and became more and more popular in the united states with more than 10 , 000 treated patients in 1996 . 
 [ 5 ] reported a 5 - year biochemical control rate of 93% and a 5 - year disease - specific survival of 100% in 320 patients with stage t1 / t2 , gleason < 6 and median initial psa level of 7.9 ng / ml treated with iodine - 125 seeds . 
although improvements have been made in the implantation technique and dose planning of permanent seeds during the last decade by using the ultrasound guided transperineal approach , it is radiobiological less desirable and contraindicated in locally advanced tumors , high initial psa level and in patients with prior transurethral resections . 
 [ 14 ] reported in a large series of 171 patients an excellent local control rate of 89% for t1 / t2 and 85% for t3 stages using 2 hdr brachytherapy fractions of each 15 gy combined with 50 gy of ebrt . 
 we evaluated relatively high doses around the 4 needles and a non - homogeneous dose distribution within the prostate . but the mean value for the reference dose covering the ptv was 82% in our series and the high - dose regions of 200 or 300% of the reference dose were within the prostate , where the tumor cells are located . 
in our series the mean value for the maximum dose to the urethra was 15.3 gy per fraction , but this dose was delivered only to less than 0.5% of the volume of the whole urethra , which we could prove by using dose - volume histograms . 
the value for the mean dose to the whole urethra was 8.7 gy per fraction , which is below the assumed tolerance level of this organ ( see table 4 )  . 
 3d - dokumentation der 100% - isodose ( referenzdosis = 5 gy ) auf der oberflche des ptv in bezug zur rektumwand . it is not the aim of 3d conformal brachytherapy to achieve a high degree of dose homogeneity within the prostate , but to achieve precisely an effective dose to the tumor cells and to spare at the same time the critical tissues within and surrounding the prostate . 
based on a spiral ct scan we reconstructed the non - parallel needles , defined an individual planning target volume , optimized the 3d dose distribution and immediately evaluated the conformal quality of the hdr implant . 
the efficiency of our combined conformal treatment with an initial response of normalized posttreatment psa levels in 91% of the patients is promising . conclusions the new approach of transrectal implantation and ctbased 3d treatment planning for 3d interstitial hdr brachytherapy of localized prostate cancer , combined with 3d external beam irradiation and androgen deprivation , is a feasible and so far well tolerated modality in the short - time follow - up of median 18 months . 
of course , a longer followup time is needed for a definite evaluation of radiation induced long - term complications . it seems to be an effective conformal treatment based on the encouraging rate of normalization of psa levels . 
3d interstitial hdr brachytherapy for prostate cancer strahlentherapie und onkologie urban & vogel 2000 originalarbeit multimodale therapie des fortgeschrittenen inoperablen sophaguskarzinoms eine retrospektive analyse ralph mcke , peter - georg ziegler , torsten libera , gunther klautke , rainer fietkau1 hintergrund : in einer retrospektiven analyse von 161 patienten mit inoperablem sophaguskarzinom wurde der einfluss der radiochemotherapie und der brachytherapie auf das gesamtberleben berprft . patienten und methoden : von 1984 bis 1999 wurden 161 patienten mit fortgeschrittenem sophaguskarzinom der stadien ii bis iv mit einer alleinigen strahlentherapie ( 131 ) oder einer simultanen radiochemotherapie ( 30 ) behandelt . 
die mediane nachbeobachtungszeit lag bei acht monaten ( ein bis 64 monate ) , die mediane perkutan applizierte strahlendosis betrug 51 gy ( 18 bis 66 , 6 gy ) , die mediane gesamtdosis der brachytherapie 10 gy ( 4 bis 25 gy )  . 
in der univariaten analyse zeigten sich vorteile fr die radiochemotherapie mit einem medianen gesamtberleben von 13 monaten und einer vier - jahres - berlebenbsrate von 18% ( p = 0 , 0368 ) sowie fr die zustzliche brachytherapie mit einem medianen gesamtberleben von 14 monaten und einer vier - jahres - berlebensrate von 12 , 2% ( p = 0 , 0008 )  . 
der stellenwert einer brachytherapie im rahmen einer simultanen radiochemotherapie muss noch abgeklrt werden . schlsselwrter : sophaguskarzinom strahlentherapie simultane radiochemotherapie brachytherapie multimodality treatment of advanced esophageal cancer : a retrospective analysis background : the records of 161 patients with inoperable esophageal carcinoma were reviewed to determine the influence of concurrent radiochemotherapy and brachytherapy on overall survival . 
 patients and methods : from 1984 to 1999 161 patients suffering from advanced esophageal carcinoma stage ii to iv were treated with radiotherapy alone ( 131 ) or radiochemotherapy ( 30 )  . 
in 48 patients additional brachytherapy was given . median follow - up was 8 months ( 1 to 64 months ) , the median external beam dosis was 51 gy ( 18 to 66.6 gy ) and the median brachytherapy dose was 10 gy ( 4 to 25 gy )  . 
chemotherapy consisted of cisplatin and 5 - fluorouracil . results : median survival for all patients was 10 months , 3 - year survival rate 13% and the 5 - year survival 5.2%. 
combination of concurrent radiochemotherapy and brachytherapy was possible without significant increase of local toxicity . conclusions : our retrospective analysis demonstrates that concurrent radiochemotherapy and additional brachytherapy are effective treatment schedules without significant increase of toxicity and may improve overall survival of patients with inoperable carcinoma of the esophagus . 
multimodale therapie des inoperablen sophaguskarzinoms d as sophaguskarzinom gehrt weltweit zu den zehn hufigsten tumoren , die inzidenz liegt in westeuropa bei ungefhr 1 bis 2% aller neu diagnostizierten tumoren [ 27 , 28 ]  . 
trotz verbesserung der operativen techniken sowie der radiotherapeutischen mglichkeiten sind die bisher erzielten fnf - jahres - berlebensraten mit 40 bis 60% fr t1 / 2n0 - tumoren sowie 5 bis 10% fr t3 / 4 - tumoren bedingt durch lokalrezidive und systemischen progress weiterhin unbefriedigend [ 9 , 30 , 33 ]  . 
vorliegende resultate randomisierter und auch retrospektiver studien zeigen eindeutig verbesserte ergebnisse in hinsicht auf die lokale kontrolle sowie das gesamtberleben [ 1 , 5 , 8 , 1012 , 14 , 18 , 21 , 25 , 31 , 32 , 34 , 35 , 38 ]  . 
 ziel dieser arbeit war es , retrospektiv den effekt einer simultanen radiochemotherapie sowie der intraluminalen brachytherapie zu bewerten . patienten und methoden von 1984 bis 1999 wurden an der klinik und poliklinik fr strahlentherapie der universitt rostock 161 patienten mit fortgeschrittenem sophaguskarzinom der stadien ii ( n = 52 ) , iii ( n = 78 ) und iv ( n = 31 ) nach der uicc - klassifikation von 1987 radioonkologisch behandelt . 
die 34 frauen und 127 mnner waren im median 59 jahre alt ( 42 bis 82 jahre )  . bei allen patienten lag eine histologische sicherung des sophaguskarzinoms vor : 142 patienten hatten ein plattenepithelkarzinom ( 88 , 2% ) , elf patienten ein adenokarzinom ( 6 , 8% ) sowie acht patienten andere histologische subtypen ( 5 , 0% )  . 
 131 patienten ( 81 , 4% ) mit einem prtherapeutischen gewichtsverlust von 9 , 4 kg ( 0 bis 44 kg ) unterzogen sich einer alleinigen strahlentherapie , 37 von ihnen mit einem prtherapeutischen gewichtsverlust von 9 , 4 kg ( 0 bis 21 kg ) in kombination mit brachytherapie . 
30 patienten ( 18 , 6% ) mit einem prtherapeutischen gewichtsverlust von 10 , 0 kg ( 0 bis 44 kg ) erhielten eine simultane radiochemotherapie , in elf fllen davon wurde diese mit einer brachytherapie kombiniert . 
 die mediane brachytherapiedosis betrug 10 gy ( 4 bis 25 gy ) mit einer einzeldosis von 5 gy ( 2 , 5 bis 12 , 5 gy ) bezogen auf 5 mm gewebetiefe . 
 chemotherapie die an den tagen 1 bis 5 und 29 bis 33 hauptschlich verabreichten chemotherapeutika waren cisplatin mit 20 mg / m2 krperoberflche ( kof ) als kurzinfusion sowie 5 - fluorouracil mit 800 mg / m2 kof als 24 - stunden - dauerinfusion . 
bei kontraindikationen gegen cisplatin applizierten wir carboplatin in einer dosierung entsprechend auc 4 als kurzinfusion . statistik bei einer medianen nachbeobachtungszeit von acht monaten ( ein bis 64 monate ) erfolgte die berechnung von berlebensraten nach kaplan und meier . 
die multivariatanalyse mit einschluss von radiochemotherapie , brachytherapie , perkutaner gesamtstrahlendosis , tumorlnge , tumorlokalisation sowie initialem gewichtsverlust erfolgte mit dem cox - regressionsmodell . ergebnisse remissionen konnten in 57 , 3% der flle erreicht werden ( 92 patienten ) , davon in 9 , 3% komplette remissionen ( 15 patienten ) sowie in 48% partielle remissionen ( 77 patienten )  . die mit abstand hchste remissionsrate mit 73 , 3% ( 22 patienten ) konnte nach simultaner radiochemotherapie erzielt werden , davon in 26 , 6% komplette remissionen ( acht patienten ) und 46 , 7% partielle remissionen ( 14 patienten )  . 
die mediane gesamtberlebenszeit fr alle patienten betrug zehn monate , die berlebensraten lagen nach drei jahren bei 13% sowie nach fnf jahren bei 5 , 2% . simultane radiochemotherapie im univariaten vergleich zur alleinigen bestrahlung zeigte sich ein signifikanter vorteil fr patienten , die sich einer simultanen radiochemotherapie unterzogen hatten . 
die mediane gesamtberlebenszeit betrug hierbei 13 monate , die berlebensrate nach vier jahren 18% , nach alleiniger radiotherapie lagen die entsprechenden werte im median bei neun monaten sowie nach vier jahren bei 3 , 2% ( p = 0 , 0368 ) ( abbildung 1 )  . 
 intraluminale brachytherapie die perkutane strahlentherapie wurde mit 60co oder 9 - mvphotonen durchgefhrt , im median wurden 50 , 7 gy ( 18 bis 66 , 6 gy ) mit einer tagesdosis von 1 , 8 gy ( 1 , 0 bis 3 , 0 gy ) auf die 90%ige isodose ( maximum = 100% ) appliziert . 
die auf die stadien bezogenen resultate bezglich der brachytherapie sind in tabelle 2 dargestellt . simultane radiochemotherapie + brachytherapie alle elf patienten erreichten eine remission , sieben patienten komplett und vier patienten partiell . 
wegen der noch zu geringen patientenanzahl in beiden gruppen ( elf gegen 19 ) wird ein signifikanzniveau noch nicht erreicht ( p = 0 , 4238 )  . multivariatanalyse hinsichtlich des gesamtberlebens zeigten sich signifikante vorteile fr eine gesamtstrahlendosis ber 50 gy , fr die brachytherapie sowie fr die simultane radiochemotherapie ( tabelle 3 )  . therapietoxizitt die therapietoxizitt wurde nach den rtog - kriterien eingestu eine radiogene sophagitis grad 3 trat in 9 , 3% der flle ( zwlf patienten ) nach radiotherapie sowie in 10% ( drei patienten ) nach radiochemotherapie auf . 
 serten lokalen kontrolle durch nutzung der endoluminalen bestrahlung liegen , denn auch nach alleiniger radiochemotherapie sind lokalrezidivraten von 30 bis 40% bekannt [ 14 , 18 , 21 , 38 ]  . diskussion unsere remissionsraten besttigen schon vorliegende resultate randomisierter studien sowie retrospektiver analysen mit angaben zwischen 46 und 86% [ 8 , 14 , 25 , 32 , 35 ]  . die daten belegen die berlegenheit einer simultanen radiochemotherapie mit medianen berlebensraten von zwlf bis 18 monaten gegenber der alleinigen strahlentherapie mit medianen berlebenszeiten von sieben bis zehn monaten [ 8 , 10 , 11 , 14 , 21 , 25 , 30 , 32 , 35 , 38 ]  . 
die von uns gewhlte chemotherapiekombination aus 5 - fluorouracil und cisplatin erbrachte in studien die besten resultate in kombination mit einer bestrahlung [ 1 , 5 , 12 , 14 , 21 ]  . andere in der simultanen radiochemotherapie eingesetzte prparate wie bleomycin und etoposid fhrten nicht zu einer verbesserung der berlebensraten bei gesteigerter toxizitt [ 2 , 13 , 20 , 24 ]  . 
 [ 21 ] im radiochemotherapiearm gewhlte dosis von 50 gy erscheint uns zu gering , wobei allerdings in dieser studie berwiegend patienten im uicc - stadium iia ( t2n0m0 ) rekrutiert wurden . 
 der aus unseren daten hervorgehende vorteil fr den zustzlichen einsatz der brachytherapie ist ebenfalls vergleichbar mit ergebnissen anderer autoren mit medianen berlebensraten von 13 bis 15 monaten [ 6 , 7 , 14 , 17 , 22 , 23 , 26 , 29 , 37 ]  . 
dadurch kann hufiger die sondierbarkeit des sophagus mit applikatoren um 10 mm durchmesser erreicht werden [ 15 ] , die mit einer besseren dosisverteilung im vergleich zu dnneren applikatoren verknpft ist . 
anhand der untersuchung von operationsprparaten wissen wir , dass sich nach einer vorbestrahlung mit 40 gy kaum noch vitale tumorzellen in den ueren wandschichten befinden , jedoch im bereich der sophagusmukosa [ 3 ]  . die nach stadien stratifizierte auswertung sollte vorsichtig bewertet werden , da die zuordnung der flle , die in den 80er jahren behandelt wurden ( hier fehlen zum teil ctund endosonographiebefunde ) , schwierig war . 
multimodale therapie des inoperablen sophaguskarzinoms aktuelles therapieprotokoll fr diese patienten eine radiotherapie in einzeldosisschritten von 1 , 8 gy bis 63 gy , die simultane chemotherapie in woche 1 und 5 mit cisplatin und 5 - fluorouracil sowie eine anschlieende fraktionierte brachytherapie mit einer einzeldosis von 4 , 0 gy bis 12 , 0 gy ( abbildung 4 )  . 
in nur drei dieser 77 arbeiten wurde dies adquat bercksichtigt , entsprechend einem anteil von 4% ( 95% - vertrauensbereich : 0 , 8 bis 11% )  . schlussfolgerung : zur verbesserung der qualitt der zeitschrift ist es wnschenswert , den fehler erster art auf einem akzeptablen niveau zu halten und damit die anzahl zufllig signifikanter ergebnisse zu reduzieren . 
autoren , gutachter und herausgeber der zeitschrift sollten darauf achten , dass bei mehr als einem signifikanztest eine entsprechende korrektur des signifikanzniveaus durchgefhrt wird . schlsselwrter : fehler erster art multiples testen qualittssicherung multiple significance testing and its relevance for interpretation of results . 
audit of the journal strahlentherapie und onkologie background : the statistical quality of the contributions to strahlentherapie und onkologie is assessed , aiming for improvement of the journal and consequently its impact factor . material and methods : all 181 articles published during 1998 and 1999 in the categories review , original contribution , and short communication were analyzed concerning the appropriate use of multiple tests . result : one hundred and four publications were excluded from analysis , because they did not contain quantitative data or because no or only 1 statistical test was performed . 
dadurch soll die qualitt der beitrge in der zeitschrift mittelfristig verbessert werden , damit sie im internationalen rahmen wieder eine wichtige rolle spielt und einen angemessenen impact factor erhlt . es ist geplant , diese bestandsaufnahme in etwa zwei jahren zu wiederholen , um qualitative vernderungen feststellen zu knnen . 1institut fr biophysik und strahlenbiologie und 2abteilung fr radio - onkologie und strahlentherapie , universitt hamburg . 
multiple signifikanztests statistische signifikanz und der fehler erster art ein beobachteter unterschied gilt als statistisch signifikant , wenn die wahrscheinlichkeit weniger als 5% betrgt ( p < 0 , 05 ) , dass die erzielten oder extremere ergebnisse zufllig aufgetreten sind , wenn in wirklichkeit berhaupt gar kein unterschied vorhanden ist . 
werden n unabhngige statistische tests durchgefhrt , so steigt der fehler erster art gem der folgenden formel an : = 1 ( 10 , 05 ) n folglich steigt bei fnf tests auf 23% , bei zehn tests auf 40% und bei 20 tests auf 64% an . 
wenn man eine gengend groe anzahl irrelevanter parameter testet , so erhlt man praktisch immer ein signifikantes ergebnis . dieses problem lsst sich dadurch umgehen , dass man in jeder wissenschaftlichen untersuchung nur einen einzigen parameter untersucht . 
dieser wert ergibt sich aus der formel : i = 10.951 / n folglich msste i bei fnf tests auf 1% , bei zehn tests auf 0 , 51% und bei 20 tests auf 0 , 256% abgesenkt werden , um den gesamtfehler erster art konstant bei 5% zu halten . wem diese formel zu umstndlich ist , kann eine einfache nherungsformel benutzen , die so genannte bonferronikorrektur [ 136 ] : i = 0 , 05 die ergebnisse unterscheiden sich kaum von der exakten formel . 
weitere hinweise sind in referenz [ 14 ] zu finden . qualittsanalyse der zeitschrift strahlentherapie und onkologie ( jahrgnge 1998 und 1999 ) alle arbeiten der rubriken aktuelles forum , originalarbeiten und kurzmitteilungen wurden von zwei beobachtern ausgewertet . 
ferner wurde nicht berprft , ob es sich tatschlich um unabhngige tests handelt . dies ist sicherlich nicht immer der fall . bei einer arbeit [ 60 ] wurde zunchst ein primrer endpunkt festgelegt . 
die explorative analyse erfolgte dann aber trotzde in einer anderen publikation [ 166 ] wird ein p - wert mit 0 , 05 < p < 0 , 1 als statistisch signifikant bezeichnet . 
in zwei dieser arbeiten wurde der fehler erster art entsprechend adjustiert [ 6 , 178 ]  . von den 77 publikationen mit mehr als einem signifikanztest wurde in lediglich drei arbeiten eine korrektur fr multiples testen durchgefhrt [ 6 , 31 , 178 ]  . 
system description of reliability and accuracy martina schiebe , wolfgang hoffmann1 background : ct simulation systems provide integration of ct - based planning target volumes , which allows to operate without the conventional simulator . 
 results : among all patients the mean difference of isocenter position between conventional and virtual simulation was 3.5 mthe isocenter displacements ranged from 0 to 6 mthere was no significant difference in isocenter accuracy between the different treatment regions . conclusions : virtual simulation with advantagesim 4.1. 
mit der konventionellen rntgensimulation fr unterschiedliche bestrahlungsregionen . patientengut und methode : bei 27 prostatakarzinompatienten , 23 patienten mit kopf - hals - tumoren und 30 bronchialkarzinompatienten erfolgte eine virtuelle simulation mit advantagesim 4.1.. 
die genauigkeit der digital rekonstruierten beams eye views wurde im vergleich zu den konventionellen simulationsund verifikationsaufnahmen ermittelt . ergebnisse : die mittlere abweichung der virtuell am patienten ermittelten isozentrumsposition im vergleich zur konventionellen simulation war 3 , 5 mdie verschiebung der isozentrumsund lasermarkierungen betrug 0 bis 6 mm ohne signifikanten unterschied bezglich der verschiedenen bestrahlungsregionen . schlussfolgerung : das neue virtuelle simulationssystem advantagesim 4.1. 
physical simulation has been established as a standard tool in the planning of external beam radiotherapy to assure reliable delivery of radiation treatment [ 3 , 5 ]  . recently ct simulation systems provide integration of ctbased planning target volumes with a three - dimensional geometrical model , which allows to operate without the conventional x - ray simulator [ 1 ]  . 
the virtual simulation software allows to calculate the beam isocenter for ct treatment plans using the planning target volume outlined in each ct scan immediately after the time of ct data acquisition . 
the definitive isocenter is placed with a laser coordinate system to transfer the planning parameters to the patients skthe treatment plan is devised after the patient left the ct simulator and then digital radiographs are reconstructed as simulator radiographs for each field . 
the patients position on the ct couch was checked using the initial parameters of the ct starting point and then the definitive treatment isocenter position and the lines indicating the laser positions were marked on the patients sk after the completion of the ct examination , isocentric conformal techniques were planned for each patient . 
the beams eye views , axial and sagittal multiplanar reconstructions were generated , and the depth control of soft tissue and bones was used to reveal optimal 3d visualization of the planning target volume ( ptv ) and the organs at risk . 
these data were transferred to the planning system ( cadplan 6.0 , varian ) for physical 3d treatment planning . after virtual simulation , the isocenter position , the field and collimating settings were verified by physical simulation using a varian simulator . 
if necessary , adjustment of the isocenter was made to match with the ct plan isocenter . the digitally reconstructed beams eye views were compared with the conventional simulator images and the first treatment verification and the deviation in lateral ( x ) , longitudinal ( y ) and axial ( z ) direction was measured ( figure 1 )  . 
the accuracy of the conventional simulator was used as standard for the imaging information of the virtual beams eye views . the aim of our analysis was to validate the virtual simulation process and to determine the accuracy of the new virtual simulation with the recently released software of advantagesim version 4.1.8 ( general electric medical systems ) which is now commercially available . results patients and methods eighty patients were enrolled in this prospective clinical analysis . 
additionally the head and neck cancer patients were immobilized using an articast masc system . initially laser set - up points at the ct starting position were fixed on the patients skin using radioopaque markers . a spiral ct ( general electric medical systems ) was used to generate the scans with a slice thickness of 5 to 7 mafter the first series of ct scans patients remained in their position . the clinical target volume and the planning target volume were outlined in each ct scan using the advantagesim software . 
the coordinates of the beam isocenter were transferred to the lap analogic laser systethe isocenter position was defined in the longitudinal ( y ) and axial ( z ) direction by the position of the ct couch . 
 definition of the x - axis was towards the patients right and left , the y - axis was defined towards the patients anterior and posterior surface , z - axis was towards the patients head and feet . 
the isocenter displacements detected on conventional simulation films ranged from 0 to 6 m mean deviation in x - direction was 2.9 mm , in y - direction 1.4 mm and in z - direction 2.0 mthe mean values and standard deviations for the physical simulation and port filming following physical simulation are listed in table 1 . 
the evaluation of these ct simulation procedures required more efficient 3d planning tools [ 5 ]  . in the present analysis the accuracy of the isocenter and laser position of the new virtual simulation system advantagesim 4.1. 
for all patients the mean isocenter displacement was 3.5 mthe different treatment regions did not show any siginificant difference in the accuracy of the isocenter positioning . previous studies reported about isocenter displacements between 1 and 5 mm for treatment target volumes of the pelvis and lung [ 1 , 2 , 7 ]  . 
 the mean isocenter deviation between the first treatment check and simulation film was 4.5 mm ( 3d vector ) and similar to the accuracy of the 3d reconstructed beams eye views . 
this is comparable to previous published data , which revealed mean deviations of about 4 to 8 mm and less than 15 mm in 95% of patients with difficult positioning [ 4 ]  . it seems to be an advantage of this and comparable systems to give better information about soft tissue structures , compared to conventional simulation . 
the virtual simulation provides accurate volumetric information of the organs in the treatment fields and are essential in reducing side effects , such as pulmonary or cardiac complications in the irradiation of lung cancer [ 2 ]  . the matching of beams eye views and actual simulator radiographs allows the precise evaluation of the coverage of the ptv and the shielding of organs at risk , furthermore application of contrast medium could be reduced . 3d reconstructed beams eye views help to shape the beams and to easily define the treatment techniques also in noncoplanar complex situations [ 12 ]  . the new virtual simulation system advantagesim 4.1. 
int j radiat strahlentherapie und onkologie urban & vogel 2000 originalarbeit long - term results of pulsed irradiation of skin metastases from breast cancer effectiveness and sequelae peter fritz , frank w . 
effectiveness and sequelae of this new irradiation method were observed in patients with disseminated cutaneous metastases of breast cancer . patients and methods : a flexible , reusable skin mold ( weight 110 g ) was developed for use with a pulsed dose rate ( pdr ) afterloader . 
an array of 18 parallel catheters ( 2 mm diameter ) at equal distances of 10 or 12 mm was constructed by fixation of the catheters in a plastic wire mesh . 
the array is sewn between 2 foam rubber slabs of 5 mm thickness to provide a defined constant distance to the skirradiations are possible up to a maximum field size of 20 ( cid : 2 ) 23.5 cm using a nominal 37 gbq ir - 192 source . 
between april 1994 and december 1997 , 52 patients suffering from cutaneous metastases at the thoracic wall were treated with 54 fields and total doses of 38 to 50 gy ( median 42 gy ) applying 2 pdr courses with a pause of 4 to 5 weeks . 
in newly irradiated patients ( n = 14 ) no contractures or skin necrosis were observed . conclusions : pulsed brachytherapy is an effective and time - sparing method for the treatment of cutaneous metastases from breast cancer . 
two sessions of approximately 20 gy pdr were tolerated on preirradiated skin without severe sequelae . key words : pulsed brachytherapy molds chest wall recurrences breast cancer langzeitergebnisse der gepulsten bestrahlung von hautmetastasen des mammakarzinoms effektivitt und strahlenfolgen hintergrund : das konzept der von brenner und hall inaugurierten gepulsten brachytherapie basiert auf einem unblichen fraktionierungsschema . 
die effektivitt und die folgen dieser neuen bestrahlungsmethode wurden an patienten mit disseminierten hautmetastasen des mammakarzinoms nachbeobachtet . patienten und methode : es wurde eine flexible , wiederverwendbare hautmoulage ( gewicht 110 g ) fr ein pdr - afterloading - gert entwickelt . 
die pdr - bestrahlungen werden mit einer nominal 37 gbq ir - 192quelle mit pulsen von 1 gy und einer pulsperiode von 1 , 2 stunden durchgefhrt ( durchschnittliche dosisleistung : 0 , 8 gy / stunde )  . 
im nicht vorbelasteten kollektiv ( n = 14 ) wurden keinerlei kontrakturen oder hautnekrosen beobachtet . schlussfolgerungen : die gepulste brachytherapie ist eine zeitsparende und effektive methode zur behandlung von hautmetastasen bei narbenrezidiven des mammakarzinoms . 
 schlsselwrter : gepulste brachytherapie moulagen brustwandrezidive mammakarzinom a local recurrence after mastectomy is defined as the appearance of tumor in the skin , subcutaneous tissues or muscles of the chest wall . 
further sites of regional recurrences are the supraclavicular fossa with an incidence of 10 to 25% and the axillar and the internal mammary chain , each being equally involved with an incidence of only about 5 to 10% [ 4 ]  . 
even though the relative risk of a locoregional relapse after appropriate postoperative radiotherapy is small , the treatment of in - field recurrences remains a quantitatively large problem due to the high incidence of breast cancer . 
in case of reirradiation a method with maximum therapeutic ratio should be chosen . according to radiobiological considerations , continuous low dose rate ( cldr ) irradiation yields the greatest therapeutic ratio . 
cldr brachytherapy with molds is one of the oldest techniques in radiotherapy and is suitable for tumors limited to the cutis and subcutis [ 16 ]  . in 1991 , theoretical considerations of pulsed dose rate ( pdr ) brachytherapy published by brenner et al . 
 [ 6 ] suggested the replacement of cldr brachytherapy with line sources by an afterloading method with a stepping source . theoretically , the radiobiological effect of cldr irradiation can be achieved by superfractionation , giving a series of exposures of 10 to 60 minutes duration at medium dose rates of 1 to 3 gy / hour , with comparable or longer gaps in which repair of sublethal damage will occur [ 9 , 11 ]  . 
the fractionation scheme maintaining radiobiological equivalence to cldr is calculated on the basis of the linear quadratic ( lq ) model , using the term ( g ) to describe the repair of sublethal damage as introduced by lea et al . 
furthermore , with pulsed brachytherapy the overall dose rate ( total dose / overall treatment time ) of the implant can be kept constant because the decay of the ir192 source does not automatically lead to a prolongation of the treatment time . 
pdr brachytherapy thus potentially combines the radiobiological properties of cldr brachytherapy with the technical advantages of the stepping source . data concerning reirradiation of the thoracic wall are sparse [ 7 , 19 ]  . 
this work reports long - term results of pdr , this new brachytherapy method using large afterloading molds for contact irradiation of newly or preirradiated skin . methods and materials irradiation device the pdr remote afterloading system1 uses a nominal 37 gbq ir - 192 stepping source . 
the catheters are woven in parallel into a plastic wire mesh to maintain equal distances of 10 to 12 mthe array is placed between 2 layers of a very stable foam rubber2 , which is flexible enough to adjust to the shape of the chest wall . 
the foam rubber flaps are 5 mm thick and provide a spacing of the catheters at a defined constant distance from the skthis material is not tissue - equivalent but as shown by tld dosimetry on patients and on a chest wall phantom it does not significantly influence the dose distribution [ 12 ]  . 
with the curved mold the depth dose curve becomes a little bit flatter , the average curvature of the chest wall has a radius of 10 cat 5 mm depth there is virtually no difference between a curved and a plane mold , whereas at 10 mm the depth dose is 8.5% greater with the curved mold ( figure 3 )  . 
because no patient showed a radius of the curvature of the thoracic wall below 10 cm , a standard optimized treatment plan for a plane array was used for all patients . 
dose profiles of the mold at different distances from the catheter plane using film dosimetry and tld dosimetry have been shown in previous papers [ 12 , 15 ]  . relationship between pulse period and pulse pause the predicted cldr isoeffect with pulsed brachytherapy is achieved by superfractionation . 
in figure 4 it can be seen that 80% of the total dose to each dose point a , b and c is accumulated from 8 / 18 catheters closest to the respective dose point . 
the time of irradiation corresponding to the dwell times of these 8 / 18 catheters is termed the effective pulse time . in a stepping source applicator , the dose rate to an individual point varies strongly with the distance of the source to the respective point . 
a = uere schaumgummiplatte ; b = wiederverwendbare katheteranordnung im plastiknetz ; c = schaumgummiplatte mit 5 mm dicken plastikknpfen als abstandhalter zur haut . the field sizes that can be irradiated are limited by the number of channels and the available number of source positions . with the present microselectron - pdr system field sizes to a maximum of 23.5 ( cid : 2 ) 20 cm ( 12 mm equidistance ) , which is quite adequate for most situations encountered in clinical practice are possible . 
using all 18 channels with step lengths of 1 cm 18 ( cid : 2 ) 24 = 432 source positions are activated . dosimetry the reference dose is prescribed to the skin surface , this means at 0.5 cm from the plane of the catheters . 
the algorithms generally used by planning systems for the calculation of the ir - 192 dose [ 17 , 21 ] are based on measured data reaching only down to 1 cm distance from the source . 
however , recent monte carlo calculations [ 26 ] and measurements [ 23 ] have yielded good agreement of the algorithms and measured data for ir - 192 , lying within about 2 to 3% , for distances between 0.5 and 10 c thus , the dose calculated by the planning system seems to be reliable . 
optimierter bestrahlungsplan fr eine 17 ( cid : 2 ) 23 , 5 cm moulage ( berechnet mit dem nps - brachytherapie - planungssystem )  . als resultat der optimierung verluft die 90% - isodose auf der hautoberflche direkt unter den ueren quellenpositionen . gy / hour , except for few dwell positions in the adjacent catheters . 
 if we now irradiate at a pulse period consisting of the effective pulse time plus a 1 - hour pause , we assure that for each tissue element the irradiation of 80% of the dose is followed by a period of 1 hour in which the remaining 20% of the dose are irradiated at low dose rate ( within approximately 20 minutes ) , and which is otherwise radiation - free . this should cause only a moderate increase in unrepaired sublethal damage from each pulse , and thus only a small increase of relative effectiveness [ 15 ]  . 
using the effective pulse time to calculate the pulse period , we can shorten the time between the duty cycles of the pdr afterloader and thus shorten the overall treatment time , while still retaining a pulse time of 1 hour between 80% of the pulses for any skin point ( figure 5 )  . 
some more details about dosimetry and radiobiological considerations have been reported in previous papers [ 12 , 15 ]  . application the mold is attached to the irradiation field which includes a 5 - cm security margin on gross disease with a self - adhesive elasticated bandage . 
verification and documentation are performed with fluoroscopy and computed tomography as described in an earlier paper [ 12 ]  . because of missing clinical experience concerning pdr tolerance of the skin , a split course was chosen as a precaution to enable observation and limitation of unacceptable severe acute reactions in time . 
a skin dose of 40 to 50 gy was believed to be necessary , and was divided into 2 almost identical pdr applications with a pause interval of 4 to 5 weeks . severe acute reactions ( epitheliolysis ) after half the total dose ( 20 to 25 gy ) in our opinion would have indicated high toxicity of pdr brachytherapy contradicting the postulated equivalence of cldr and pdr . 
tiefendosiskurven fr eine pdr - moulage , fr orthovolttherapie und fr unterschiedliche elektronenenergien ( a = ebene moulage ; b = 100 - kev - rntgenstrahlen , 2 mm al ; c = 4 , 5mev - elektronen ; d = 7 , 5 - mev - elektronen )  . between april 1994 and december 1997 , 52 female patients suffering from chest wall recurrences of a breast carcinoma after mastectomy were irradiated in the area of the thoracic wall . 
dose contributions to 3 points ( a , b , and c ) at reference distance ( surface of the skin = 100% ) on the boarders ( a , c ) and under the middle of the mold ( b ) from each of the 18 catheters ( top diagrams )  . 
dosisbeitrge der 18 katheter in drei punkten ( a , b und c ) auf der referenzisodose ( hautoberflche = 100% ) am rande ( a und c ) und in der mitte der moulage ( b )  . 
to 14 out of 46 patients pdr irradiation was applied on previously unirradiated sk for these patients the interval from mastectomy to local recurrence was at a median of 27 months ( range 9 to 84 months )  . 
the extent of disease at the time of chest wall recurrence and during the follow - up period was established through full examination every 3 to 4 months in our outpatients department . 
all patients were observed in an oncological follow - up program with blood counts , liver sonography , x - ray of the chest and bone scans if the alkaline phosphatase showed pathological values . n1bi n1bii n1biii n1biv n2 table 1 . 
on 24 patients ( 46% ) more or less extended nodules and / or plaques or in 2 cases an inflammatory carcinoma ( type b , c , d recurrence ) were treated . 
bei 62% dieser patientinnen traten teleangiektasien innerhalb eines jahres nach der pdr - bestrahlung auf . 4 / 32 ( 12% ) 4 / 32 ( 12% ) patients follow - up minimal marked telangiectasia telangiectasia incidence ( months ) overall contracture of skin skin necrosis 24 < 36 12 < 24 6 < 12 8 / 11 3 / 11 100% 100% 0 / 3 ( 0% ) 0 / 11 ( 0% ) 0 / 0 ( 0% ) 0 / 3 ( 0% ) 0 / 11 ( 0% ) 0 / 0 ( 0% ) table 3 . 
 local control in patients with type b , c and d recurrences ( gross disease ) in 24 patients and 26 fields complete remissions were achieved in 25 out of 26 fields ( 96% ) ( figures 7a and 7b )  . the follow - up was between 7.2 and 38 months ( median 18 months )  . 
taking into respect that 2 patients with inflammatory carcinoma were treated with 2 abutted fields the local control rate was 21 out of 26 fields ( 81% ) or 21 out of 24 patients ( 87% )  . in patients with type a recurrences ( microscopic disease ) on 22 patients and 22 fields the local control rate was 20 / 22 fields ( 91% )  . 
 all in - field recurrences occurred within 1 year after pdr irradiation as a limited number ( 1 to 3 ) of regrowing skin metastases which could be partially removed through careful and limited excisions . 
this situation presented as disseminated rapidly spreading skin metastases around the irradiation field and was always combined with a lymphogenous spread to the pleura causing pleural effusions and distant metastases during the further course of the disease . 
an attempt with doxorubicine - containing chemotherapy was made on these patients . acute reactions moist desquamation which covered less than 50% of the mold field developed in 16 out of 48 fields ( 33% )  . 
concerning the grade and incidence of this acute reaction there was no significant difference between previously irradiated and unirradiated skat present we have no explanation for this observation . late effects late effects of pdr brachytherapy on human skin are shown in figure 8 . 
 [ 25 ] showed that about 50% of all patients with only local relapse live more than 5 years if the size of the nodes does not exceed 1 cm or if the relapse - free interval was more than 24 months . 
according to bedwinek et al . [ 3 ] the rates of local failure for radiotherapy studies were quite high , with a range of 25 to 76% and an average of about 51% . even after local excision of the recurrence before irradiation the rates of local recurrences remains high . 
in comparison , our results appear to be excellent yielding local failure in 9% ( 2 out of 22 patients ) after local excision and pdr radiotherapy , and in 13% ( 3 out of 24 patients ) after primary pdr irradiation of skin metastases without excision . 
pulsed irradiation of skin metastases from breast cancer ed to temporary erythemas and dry or moist desquamations . no information on late effects is provided . telangiectasia occurred in all patients independent of preirradiation within 2 years after pdr irradiation . 
since our work was not a comparative study our results allow no conclusion to the question whether pdr brachytherapy is equivalent or not to cldr brachytherapy or fractionated electron beam radiotherapy with respect to this late effect . 
during the 4 weeks break between the sessions and after the therapy patients are required to come in 2 to 4 times for evaluation of skin reactions and response to therapy . 
in this clinical situation the occurrence of telangiectasia should not be emphasized , and , until development of better means , it should be respected as a fair price for a very likely long - lasting local control . 
in addition to pdr brachytherapy for interstitial boost after breast - conserving surgery and external beam radiation therapy [ 13 ] the mold technique is a further field for pdr brachytherapy which yields beneficial results . 
this clinical study was supported by german cancer aid . strahlentherapie und onkologie urban & vogel 2000 originalarbeit radiotherapy as adjunct to surgery for malignant carotid body paragangliomas presenting with lymph node metastases ramona mayer1 , johannes fruhwirth2 , alfred beham3 , reinhard groell4 , johann poschauko1 , arnulf hackl1 purpose : three cases of malignant carotid body paragangliomas with nodal metastases are reported . patients and methods : between 1985 and 1994 , 3 female patients ( 51 to 65 years of age ) were referred for postoperative radiotherapy after complete ( 2 ) or incomplete ( 1 ) surgical excision of a malignant carotid paraganglioma ( shamblin iii )  . 
preoperative angiographic embolization of the tumor - supplying arteries was performed in all cases . in 2 patients resection of the internal carotid artery and reconstruction by saphenous vein graft was necessary . 
continuous course radiotherapy of the tumor bed ( 50 to 56 gy / 2 gy ) and regional lymph nodes ( 50 gy ) using photon beams was delivered in 2 patients . 
the third patient having had incomplete resection cancelled radiotherapy after 4 gy . results : within an observation time of 110 and 119 months no evidence of recurrence was obtained in both patients irradiated postoperatively . 
twelve months after the withdrawn irradiation she presented with a tumor progression into the brain and an ulcerated mass on the right side of the neck and was irradiated consecutively for palliation ( figures 1a to 1f )  . 
in none of the patients severe acute or late radiation - induced complications were observed . conclusion : in patients with malignant paraganglioma moderate dose postoperative radiotherapy of the tumor bed and regional lymph nodes is well tolerated . 
 key words : malignant paraganglioma carotid body tumor lymph node metastases surgery pathology external radiotherapy local control adjuvante strahlentherapie maligner paragangliome des glomus caroticum mit lymphknotenmetastasen hintergrund : bericht ber drei patienten mit einem malignen paraganglioma caroticum mit histologisch verifizierten regionren lymphknotenmetastasen . patienten und methode : zwischen 1985 und 1994 wurden drei patientinnen ( alter 51 bis 65 jahre ) nach kompletter ( zwei ) bzw . 
die dritte patientin verstarb am lokalen tumorprogress ; zwlf monate nach abbruch der bestrahlung war es zu einem ausgedehnten tumorwachstum mit infiltration bis in das hirn und zu exulzerierten lymphknotenmetastasen gekommen , sodass zu diesem zeitpunkt nur mehr eine bestrahlung in palliativer intention mglich war ( abbildungen 1a bis 1f )  . 
 schlsselwrter : maligne paragangliome glomus - caroticum - tumoren lymphknotenmetastasen chirurgie pathologie externe strahlentherapie lokale kontrolle c arotid body paragangliomas are uncommon neuroendocrine tumors of the head and neck area originating in the paraganglia of the chemoreceptor system ; located at the bifurcation of the common carotid arteries , they present clinically as a swelling in the anterolateral region of the neck [ 3 , 5 , 16 , 18 ]  . 
in advanced stages the tumor may extend to the angle of the mandible , to the base of the skull and / or the parapharyngeal space resulting in symptoms like pain , dysphagia and cranial nerve palsies [ 18 , 20 ]  . 
 most carotid paragangliomas are benign tumors with a slow growth rate ; the criterion of malignancy is not based on typical histologic features of malignant disease , such as nuclear pleomorphism , hyperchromasia , and mitotic activity . 
since necrosis and vascular invasion are also not unquestionable signs of malignancy , the diagnosis of a malignant carotid body paraganglioma has to be established on the basis of histologically proven metastases [ 13 ]  . 
 we present 3 patients with sporadic carotid body paraganglioma metastatic to regional lymph nodes . patients and methods between 1985 and 1994 , 3 female patients ( 51 to 65 years of age ) were referred for postoperative radiotherapy after complete ( 2 ) or incomplete ( 1 ) surgical excision of a malignant carotid paraganglioma . 
initial evaluation had included clinical history , physical examination , angiography of the aortic arch and supraaortic branches and computed tomography ( ct ) / magnetic resonance imaging ( mri )  . 
preoperative angiographic embolization of the tumorsupplying arteries by intravascular injection of gelfoam and implantation of microcoils was performed in all cases to enable safer surgical removal with less intraoperative bleeding . in 2 patients resection of the internal carotid artery and reconstruction by saphenous vein graft was necessary . 
 external radiotherapy continuous course radiotherapy of the tumor bed ( 50 to 56 gy / 2 gy ) and regional lymph nodes ( 50 gy ) was delivered by photon beams . 
the third patient had only incomplete surgery , but she cancelled radiotherapy after 4 gy ; 12 months later she presented with an extensive tumor progression and was irradiated consecutively for palliation ( 56 gy ) ( figures 1a to 1f )  . pathology the primary tumors were histologically composed of large , polygonal cells with centrally located nuclei of different size and chromatin content , so - called chief cells . 
these cells either showed a typical arrangement to nests or zellballen , which were surrounded by a distinct vasculature or , in the case of distinct cellular pleomorphism , to broad sheets without any organoid pattern . 
mitotic figures could be found frequently all over the tumors , whereas necrosis and vascular invasion were restricted to circumscribed areas . immunohistochemically , the large cells revealed reactivity for nse and , to a variable extent , for synaptophysin , neuropeptides and cytoskeletal proteins . 
by the application of antibodies to s - 100 protein and glial fibrillary acidic protein spindle shaped cells , located peripherally to the chief cells , could be demonstrated , which corresponded to sustentacular cells . ultrastructural investigations revealed the presence of neurosecretory granules within the cytoplasm of most chief cells [ 10 ]  . the lymph node metastases showed a morphological architecture and immunohistochemical profile identical to the primary tumors ( figure 2 )  . follow - up investigations included clinical investigation and ct / mri every 12 months ; angiography was not performed routinely . 
malignant carotid paraganglioma figure 1a abbildung 1a figure 1b abbildung 1b figure 1c abbildung 1c figure 1d abbildung 1d figure 1e abbildung 1e figure 1f abbildung 1f figures 1a to 1f . 
residuales lymphatisches gewebe ist mit einem pfeil gekennzeichnet ( gomori - frbung , ( cid : 2 ) 400 )  . tion of an advanced malignant carotid body paraganglioma . twelve months later she presented with a tumor progression into the brain and an ulcerated mass on the right side of the neck ( figures 1a to 1f ) and was irradiated consecutively for palliation . 
 in the other 2 patients with an malignant carotid paraganglioma and a follow - up of 110 and 119 months local control could be achieved ; 1 of them died due to intercurrent disease without evidence of clinical or radiologic recurrence . despite moderate skin reactions and / or inflammatory changes in the external auditory canal and temporary hair loss , no serious acute or late radiation induced complications were observed . 
nerve palsy obtained in 1 patient remained unchanged after treatment . discussion carotid body paragangliomas usually are slow growing tumors causing a long lasting clinical history in most cases [ 18 ]  . however , invading the brain or metastasizing to local or distant sites they can cause severe symptoms and can be lethal [ 3 , 15 , 16 ]  . 
in carotid paragangliomas the risk of metastatic disease seems to be higher compared with other paragangliomas of the head and neck region [ 6 , 20 ]  . malignant behavior is recognized in approximately 4 to 22% of cases [ 1820 ] and includes metastatic involvement of lymph nodes , bone , lung , liver , retroperitoneum and brain [ 1 - 3 , 7 , 8 , 12 , 1517 , 20 , 22 , 24 ]  . 
in patients with malignant carotid body tumors with spread to cervical lymph nodes adjuvant irradiation treatment of the tumor bed and regional lymph nodes seems to be beneficial [ 2 , 3 , 21 ]  . 
radiation dose used in our patients varied from 50 to 56 gy and was within the bounds of radiation dose used by others [ 3 , 16 , 20 ]  . 
therapeutic options of metastatic disease might include surgery , radiotherapy or chemotherapy . surgery might be an option in selected cases , if the patient is in good condition and the surgical approach is technically feasible . 
malignant carotid paraganglioma strahlentherapie und onkologie urban & vogel 2000 originalarbeit herpes zoster in breast cancer patients after radiotherapy jrgen dunst1 , bettina steil1 , steffi furch1 , annette fach1 , gisela bormann2 , wolfgang marsch2 purpose : we have studied the incidence of herpes zoster in patients with adjuvant radiotherapy for breast cancer with special emphasis on possible correlations with other prognostic factors or survival . 
in case of postmastectomy radiotherapy , the lateral chest wall and lymphatics ( axilla , parasternal and supraclavicular nodes ) were irradiated with an anterior photon field to 50 gy ( axilla 44 gy ) and most of the chest wall with an electron field to 44 gy in 2 - gy fractions . 
after breast - preservation , the breast was irradiated via tangential fields with 6to 8 - mv photons up to 50 gy plus 8 gy electron boost to the tumor bed . 
the frequency of zoster was determined retrospectively by reviewing the patients records . results : a zoster after radiotherapy occurred in 41 / 1 155 patients ( 3.7% ) , mostly within the first 2 years after completion of radiotherapy . 
type of treatment ( mastectomy vs breast - preservation ) had no impact on the frequency of herpes zoster ( 36 / 961 patients after mastectomy and 5 / 194 patients after breast - preservation )  . 
there was also no correlation with other prognostic factors such as age , menopausal status , stage of disease or the use of adjuvant chemotherapy , nor was the occurrence of zoster linked to the degree of acute skin reaction in the radiation field . 
moreover , patients with zoster had the same prognosis as compared to patients without zoster with regard to local control and survival . conclusions : the observed frequency of zoster ( about 4% of patients after postoperative radiotherapy ) in this retrospective study suggests that the risk of developing zoster in this patient group may be 3to 5 - fold higher as compared to the incidence in the general population . 
however , the occurrence of zoster was not linked to prognosis and treatment response . key words : breast cancer zoster radiotherapy prognosis herpes zoster bei brustkrebspatientinnen nach radiotherapie hintergrund : wir haben in einer retrospektiven analyse die hufigkeit eines herpes zoster bei patientinnen mit mammakarzinom und postoperativer radiotherapie untersucht . patientinnen und methode : von januar 1985 bis dezember 1993 erhielten 1 155 patientinnen an unserer klinik eine postoperative bestrahlung nach mastektomie ( n = 961 ) oder brusterhaltender operation ( n = 194 ) in kurativer intention . das alter betrug 34 bis 79 jahre . 
die nachbeobachtungszeit betrug drei monate bis 12 , 5 jahre ( median 3 , 1 jahre )  . ergebnisse : 41 / 1 155 patientinnen ( 3 , 7% ) entwickelten im nachbeobachtungszeitraum einen herpes zoster . 
zoster after postoperative radiotherapy schlussfolgerungen : die beobachtete hufigkeit von herpes zoster ( etwa 4% nach drei jahren follow - up ) lsst vermuten , dass ein herpes zoster im untersuchten kollektiv etwa dreibis fnffach hufiger auftritt als anhand der inzidenzen in der normalbevlkerung erwartet . 
the secondary infection is caused by the reactivation of the latent infection of the dorsal ganglion cells with the varicella - zoster virus and remains mostly localized to a dermatom [ 9 ]  . 
other risk factors for the development of zoster are an impaired immunity ( a decline in immune function ) , such as malignancies ( especially lymphomas ) , cytotoxic and immunosuppressive therapy , and infection with the human immunodeficiency virus [ 9 ]  . 
 patients with breast cancer are not considered a risk population for zoster although there are very few data available . radiation may also exert a transient immune depression , especially when large fields are applied . 
 patients and methods a total of 1 155 patients with breast cancer received postoperative irradiation either after mastectomy ( n = 961 ) or after breast preservation ( n = 194 ) in our department in the period from 1 / 1985 through 12 / 1993 . 
 radiotherapy in patients with postmastectomy radiotherapy , the lymphatics ( axilla , bilateral parasternal and ipsilateral supraclavicular nodes ) and part of the chest wall were irradiated with an anterior field with telecobalt or 9 - mv photons . 
 systemic therapy of these patients 746 received adjuvant systemic therapy , either chemotherapy alone ( n = 100 ) , mainly according to the cmf - regimen , or hormonal therapy with tamoxifen ( n = 428 ) or a combination of both ( n = 218 )  . 
a subset of the patients with postmastectomy irradiation received chemotherapy after the completion of radiotherapy . statistical evaluation the patients were followed routinely in our department for 3 to 5 years and thereafter in individual intervals . 
 results overall frequency of herpes zoster forty - one patients out of the total study population of 1 155 patients ( 3.7% ) developed a zoster after radiotherapy , mostly within the first 2 years after the completion of radiotherapy . 
 type of treatment ( mastectomy vs breast - preservation ) had no impact on the frequency of herpes zoster ( 36 / 961 patients after mastectomy and 5 / 194 patients after breast - preservation )  . 
zoster after postoperative radiotherapy parameter subgroups herpes zoster frequency of ( n / all patients ) herpes zoster total population menopausal status t - category n - category skin erythema pneumonitis esophagitis lymphedema 40 years 4150 years 5160 years 6170 years > 70 years premenopausal postmenopaual t12 t34 n13 chemotherapy tamoxifen both none mild / moderate severe none present none present none present 41 / 1155 3 / 137 16 / 377 15 / 334 5 / 252 2 / 55 16 / 443 25 / 712 29 / 887 11 / 245 20 / 494 21 / 640 17 / 409 4 / 100 12 / 428 8 / 218 8 / 357 20 / 403 13 / 395 32 / 975 9 / 180 35 / 1015 6 / 140 33 / 985 8 / 169 type of surgery mastectomy 36 / 961 breast preservation 5 / 194 systemic therapy none table 1 . 
patients with erythema in the radiation field had the same risk of zoster as patients without any skin toxicity ( 5% vs 2% , ns )  . herpes zoster and treatment outcome the occurrence of a zoster had no impact on local control ( figure 1 ) , distant - metastases - free survival and overall survival ( figure 2 )  . 
moreover , with regard to the underlying immunosuppressive disorders which favor the development of a zoster it is unclear whether the occurrence of zoster is associated with a more or less favorable prognosis . 
 high frequencies of zoster in the range of 30% or more have been described for several malignancies , especially for patients with hematological disorders [ 6 , 8 , 11 , 13 ]  . 
in a study on hodgkins disease , patients treated with chemotherapy and radiation had a 2to 3 - fold enhanced risk of zoster in comparison to patients receiving radiotherapy alone ( 27% vs 11.5% ) [ 6 ]  . 
bone marrow transplantations [ 13 ]  . age of 80 , about 8 to 15 patients in our population should have been expected to develop a zoster during the median follow - up time of 3 years . 
the observed frequency ( n = 41 ) suggests that the risk of zoster may be enhanced by a factor of about 3 to 5 ( or more ) in patients with breast cancer and adjuvant radiotherapy . 
thus , acute skin erythema in the radiation field did not seem to be a risk factor for the later development of a zoster . it is not clear in as much radiotherapy contributes to the risk of herpes zoster . 
there are also reports about zoster after 20 gy tbi for rheumatoid arthritis suggesting that immunosuppression after large field irradiation may be associated with an increased risk of zoster [ 14 ]  . 
the frequency of 3 to 4% in our series corresponds to the data in the literature . however , our analysis was retrospective and the occurrence of a zoster was not systematically reported and documented during follow - up so that the real incidence might have been underestimated in our study . 
this observation might be important for daily clinical practice with regard to the information of patients and other physicians involved in the care and follow - up of patients after curative radiotherapy . in summary , we observed a herpes zoster in 3.7% of breast cancer patients after postoperative radiotherapy during a median follow - up period of 3 years . 
this frequency is about 3 to 5 times higher than expected in the general population . however , the occurrence of a zoster was not associated with side effects or outcome . 
since all patients had received radiotherapy , the contribution of radiation to the occurrence of zoster could not be determined . strahlentherapie und onkologie urban & vogel 2000 originalarbeit vaskularisation von freien myokutanen grazilislappen im ersatzschwachen transplantatlager nach properativer radiotherapie eine experimentelle untersuchung stefan schultze - mosgau1 , franz rdel2 , ludwig keilholz2 , gerhard g . 
grabenbauer2 , jrg wiltfang1 , martin radespiel - trger3 , rolf sauer2 , friedrich wilhelm neukam1 hintergrund : nach properativer radiotherapie vor ablativer chirurgie von plattenepithelkarzinomen der kopfund halsregion werden schden am gefbindegewebe beobachtet , die zu einer verzgerung der einheilung freier lappen im vorbestrahlten transplantatlager fhren knnen . 
 material und methoden : wistar - ratten ( mnnlich , krpergewicht 300 bis 500 g ) wurden zur erzeugung eines vorbestrahlten transplantatlagers mit 3 - mal 10 gy ( 30 tiere ) und 5 - mal 10 gy ( 30 tiere ) im halsbereich bestrahlt ( kontrollgruppe : 42 nicht bestrahlte tiere )  . 
bei allen tieren erfolgte nach einem zeitintervall von vier wochen die transplantation eines freien myokutanen grazilislappens ( 2 , 5 ( cid : 2 ) 2 , 5 cm ) von der rechten leiste in den halsbereich mit anastomosierung an den halsgefen . 
nach heund immunhistochemischer frbung ( markierung der kapillarendothelien mit polyklonalem goat - f [ ab ] - 2 - anti - von - willebrand - faktor ) erfolgte die quantitative histomorphometrische ( nh - image ) erfassung der relation kapillarflche / gesamtflche und des kapillarlumens . 
quantitativ nahm die relation kapillarflche / gesamtflche im bergangsbereich zwischen transplantat und bestrahltem transplantatlager als hinweis auf eine abnehmende kapillarisierung im gegensatz zur kontrollgruppe vom dritten bis siebten tag nach bestrahlung signifikant ab ( p = 0 , 004 )  . 
tag wurde ein signifikanter unterschied zwischen der kontrollgruppe und den bestrahlten tieren festgestellt ( p = 0 , 005 )  . ebenfalls trat im zeitlichen verlauf eine signifikante abnahme des mittleren kapillarlumens im bergang zwischen transplantiertem und bestrahltem gewebe im vergleich zur kontrollgruppe auf ( p < 0 , 001 und p = 0 , 003 )  . 
eine optimierung des zeitintervalls zwischen radiotherapie und transplantation und der bestrahlungsdosis ist deshalb fr den einheilungserfolg freier transplantate bedeutungsvoll . schlsselwrter : freie weichgewebetransplantate bestrahltes transplantatlager wundheilung vaskularisation tiermodell vascularization of free gracilis flaps in irradiated neck region an experimental study background : following preoperative radiotherapy prior to ablative surgery of squamous epithelial carcinomas of the head and neck region , inflammatory changes to the connective tissue and vascular endothelium are observed . 
 material and methods : in wistar rats ( male , weight 300 to 500 g ) undergoing preoperative irradiation of the neck region with 3 times 10 gy ( 30 animals ) and 5 times 10 gy ( 30 animals ) and non - irradiated rats ( 42 animals ) , a free myocutaneous gracilis flap taken from the groin was transplanted to the irradiated region of the neck . 
on day 3 , 4 , 5 , 7 , 14 and 28 post operation , the capillary sprouting , structural changes and the distribution patterns were analyzed by h & e and immunohistochemical staining ( goatf [ ab ] - 2 - anti - von willebrand factor antibody )  . 
three histological sections ( 2 to 4 m ) per sample were investigated histomorphometrically , qualitatively and quantitatively ( ratio capillary area / total area , and capillary lumen ) by nhimage - digitized measurement . 
a statistical analysis was performed using the mann - whitney test . results : in contrast to non - irradiated rats , irradiated animals showed a qualitatively reduced and a more irregular capillary distribution with more marked pericapillary fibrosis in the irradiated transplant bed . 
further optimization of the time interval between radiotherapy and surgery and the total radiation dose are therefore needed . key words : free flaps irradiated transplant bed wound healing vascularization animal model p atienten mit plattenepithelkarzinomen im mund - , kieferund gesichtsbereich werden im rahmen einer multimodalen tumortherapie interdisziplinr chirurgisch , chemound strahlentherapeutisch behandelt . 
durch eine radiotherapie kann es dabei durch eine direkte schdigung der an der wundheilung beteiligten zellulren elemente ( verminderte leukozytenfunktion , verminderte phagozytoseaktivitt in der entzndungsphase , vermehrte kollagenexpression durch fibroblasten in der proliferationsphase , zerstrung der reproduktiven integritt von fibroblasten und endothelzellen ) zu akuten und chronischen wundheilungsstrungen und erhhten wundinfektionsraten kommen [ 26 , 28 ]  . 
ein problem der properativen radiotherapie besteht darin , dass nicht nur in unterschiedlichem ausma wundheilungsstrungen bei der nachfolgenden chirurgischen therapie auftreten knnen [ 2 ] , sondern insbesondere die einheilung von freien transplantaten , die zur funktionsorientierten und sthetischen rekonstruktion des hartund weichgewebes nach ablativer tumorchirurgie eingesetzt werden , verzgert bzw . 
klinische untersuchungen zur erfolgsbeurteilung freier vaskulrer transplantate im vorbestrahlten transplantatlager zeigen , dass strungen der mikrozirkulation infolge von thrombosierungen oder perfusionsstrungen die hufigste ursache fr einen misserfolg sind [ 2224 , 27 , 29 ]  . 
bisher fehlen jedoch weitgehend analysen der vaskularisation und der strahleninduzierten schdigung der gefe im bergangsbereich zwischen bestrahltem ortsstndigen transplantatlager und transplantat . die kenntnis der einheilvorgnge , insbesondere der vaskularisation , knnte eine aussage ber den zeitpunkt , ab dem ein freies transplantat ausreichend vom transplantatlager aus perfundiert ist , ermglichen . 
welche vernderungen des kapillarlumens treten nach properativer bestrahlung auf ? material und methode tierexperimenteller versuchsaufbau in einem tierexperimentellen ansatz wurden 102 mnnliche wistar - ratten ( krpergewicht 300 bis 500 g , charles river wiga , sulzfeld , deutschland ) eingesetzt . 
die haltung der tiere erfolgte entsprechend des tierschutzgesetzes ( tierversuchsantrag 621 - 2531.31 - 13 / 96 ) zu zweit in polycarbonat - kfigen bei 22 0 , 5 c , 55% luftfeuchte und zwlf stunden hell - dunkel - zyklus . 
die tiere erhielten eine standardernhrung mit konzentratfertigfutter ( no.1320 , altromin , lage , deutschland ) und wasser ad libitu bei allen 102 tieren wurde die verpflanzung eines freien mikrochirurgisch reanastomosierten myokutanen grazilislappens von der rechten leiste in den rechten halsbereich durchgefhrt . 
zur berprfung des einflusses einer properativen radiotherapie auf die vaskularisationsvorgnge bei der einheilung des freien weichgewebetransplantats wurden die tiere properativ bestrahlt , sodass folgende gruppeneinteilung resultierte : gruppe 1 ( 42 tiere ) = verpflanzung ohne properative radiotherapie , gruppe 2 ( 30 tiere ) = verpflanzung mit properativer radiotherapie von 30 gy und gruppe 3 ( 30 tiere ) = verpflanzung mit properativer radiotherapie von 50 gy . 
 properative bestrahlung im halsbereich zur bestrahlung wurde ein linearbeschleuniger mit 6 - mvphotonen und einem bolus von 1 cm ( siemens mevatron 67 , siemens , erlangen , deutschland ) verwendet . 
die bestrahlung erfolgte durch ein anteriores stehfeld ( 5 ( cid : 2 ) 5 cm )  . die kraniale grenze des ttowierten bestrahlungsfeldes war der unterkiefer , die kaudale grenze die klavikul . 
 verpflanzung eines freien myokutanen grazilislappens in den vorbestrahlten halsbereich die topographisch - anatomische beschreibung des lappenmodells erfolgt auf der grundlage der angaben von greens anatomy of the rat [ 7 ]  . 
als lappenmodell wurde ein freier myokutaner grazilislappen in einer gre von 2 , 5 ( cid : 2 ) 2 , 5 cm aus der leistenregion der rechten unteren extremitt verwendet ( abbildung 1 )  . 
als modifikation wurden der musculus semitendinosus in den muskulren lappenanteil und die saphenagefe als zustzliche gefversorgung neben der arteria und vena femoris profunda mit einbezogen . zur erzeugung eines tranplantatlagers , das eine klinisch vergleichbare situation mit funktioneller beanspruchung durch kopfbewegungen gewhrleistet , wurde im rechten hals im tiermodell ein 3 ( cid : 2 ) 3 cm groer resektionsdefekt geschaffen ( abbildung 1 ) , der bei den vorbestrahlten tieren innerhalb des ttowierten bestrahlungsfeldes lag . 
nach standzeiten von drei , vier , fnf , sieben , 14 und 28 tagen wurden pro tier je drei biopsien ( 1 ( cid : 2 ) 1 ( cid : 2 ) 0 , 5 cm ) aus dem transplantat , dem transplantatlager und dem bergangsbereich zwischen transplantiertem und ortsstndigem transplantatlager entnommen . die properative bestrahlung der tiere und die transplantation des myokutanen grazilislappens erfolgten in inhalationsnarkose mit isofluran ( forene , abbott , wiesbaden , deutschland ) [ 21 ] ber ein modifiziertes kreislaufsystem des narkoseapparats ( tiberius 19 , draeger , bremen , deutschland )  . als perioperative medikation erhielten die tiere eine antibiose mit 10 000 ie breitspektrumpenicillin intraperitoneal ( tardomyocel , bayer , leverkusen , deutschland ) und eine volumensubstitution mit 15 bis 20 ml infusionslsung intrapeabbildung 1 . 
vaskularisation von freien transplantaten im vorbestrahlten transplantatlager ritoneal ( tuto - op , pharmacia - upjohn , erlangen , deutschland ) sowie intraoperativ eine weitere volumenund elektrolytsubstitution ( 15 bis 20 ml intraperitoneal )  . 
die anfertigung von gewebeschnitten erfolgte in form von lngsschnitten ( 2 m schichtdicke , schlittenmikrotom jung hn 40 , leica , nussloch , deutschland ) senkrecht zum verlauf des bergangsbereichs zwischen transplantat und transplantatlager . 
nach hydrierung in tbs ( 0 , 05 m tris / hcl ; 0 , 15 m nacl ; ph 7 , 6 ) ( fnf minuten , rt ) wurde zur unterdrckung der endogenen peroxidaseaktivitt h2o2 ( 3% , 20 minuten , rt ) verwendet . 
 ( polyklonales fr die markierung der kapillarendothelien mit anti - vonwillebrand - faktor - ( vwf - ) antiserum ziege f [ ab ] - 2 , loxo / novocastra , dossenheim , deutschland ) wurde zur demaskierung des epitops mit citratpuffer ( 10 mm ; ph 6 , 0 ) und mikrowelle vorbehandelt , und unspezifische bindungsstellen wurden mit kaninchenserum ( dako diagnostika , glostrup , dnemark ) ( 20 minuten , rt ) und blockiermedium blotto ( tbs mit 5% magermilchpulver , 0 , 1% tween 20 ) ( 30 minuten , rt ) abgesttigt . 
die inkubation der prparate erfolgte in einer feuchten , dunklen kammer ( 4 c , zwlf stunden ) mit einer antikrperverdnnung von 1 : 100 ( tbs / 2 , 5% bsa )  . 
als sekundrantikrper wurde mit einem biotinylierten kaninchen - anti - ziege - antikrper ( dako , glostrup , dnemark ) in der gleichen verdnnung inkubiert ( 30 minuten , rt )  . 
die chromogene nachweisreaktion erfolgte mit aec ( 0 , 02% 3 - amino - 9 - ethylcarbazole in 50 mm acetatpuffer ph 5 ; 5 , 5% dimethylformamid ) ( dako ) und h2o2 ( endkonzentration 0 , 005% ) unter mikroskopischer sichtkontrolle . 
von jeder gewebeprobe wurden auf einem objekttrger drei konsekutive schnitte inkubiert und jeweils einer als negativkontrolle ( inkubation mit bsa ohne primrantikrper ) mitgefhrt . als positivkontrolle diente ein als positiv bekanntes prparat . 
 histomorphometrische analyse die prparate wurden qualitativ im hellfeldmikroskop ( axioskop , zeiss , oberkochen , deutschland ) bei zehnbis 40facher vergrerung auf vernderungen des epithelialen aufbaus , entzndungszeichen , fibrosierung im subkutangewebe und lumenvernderungen sowie gefwandverdickungen der kapillaren untersucht . 
von jeder probe pro tier / tag / untersuchungsgruppe wurden drei gesichtsfelder im hellfeldmikroskop ( aristoplan , leitz , wetzlar , deutschland ) ausgewhlt , bei zehnfacher vergrerung ber eine ccd - kamera ( hamamatsu c2400 , bridgewater , usa ) digitalisiert und pc - gesttzt mit einem image - programm ( scion image pc v1.61 , scion corporation , usa ) ausgewertet . nach kalibrierung des messsystems mit einem 2 - mm - eichmikrometer ergab sich bei zehnfacher vergrerung und bekannter messdistanz von 700 m eine messstrecke aus 424 pixeln . 
alle berechnungen wurden mit dem programm spss v9 fr windows ( spss inc . , chicago , usa ) durchgefhrt . ergebnisse ein erythem und eine trockene desquamation im halsbereich zwischen ende der radiotherapie und transplantation wurden nach bestrahlung mit 50 gy bei der hlfte der tiere gesehen . 
 der epithelaufbau und die ausprgung der bindegewebsstrukturen im transplantierten gewebe , im transplantatlagergewebe und im bergangsbereich bei nicht bestrahlten tieren ( gruppe 1 ) entsprach in heund vwf - frbungen den befunden an der entnahmestelle des transplantats . 
das subkutane bindegewebe zeigte einen deutlich hheren anteil an kollagenen faserstrukturen mit dichterer strukturierung bei gleichzeitigem verlust von zellulren elementen und eine geflumenverkleinerung mit gefwandverdickung im sinne einer fibrosierung ( abbildung 3 )  . 
increase of collagenous fibers ( 1 ) , thickening of capillary wall ( 2 ) ; he staining , magnification ( cid : 2 ) 40 . transplantat lager bergang transplantat / lager gruppe 1 keine bestrahlung gruppe 2 30 gy gruppe 3 50 gy gruppe 1 keine bestrahlung gruppe 2 30 gy gruppe 3 50 gy 3 . 
whrend bei den nicht bestrahlten tieren die mediane relation des transplantats der medianen relation im bergangsbereich zwischen transplantat und transplantatlager entsprach , fand sich bei den bestrahlten tieren eine deutlich geringere relation im bergangsbereich zwischen transplantat und vorbestrahltem transplantatlager als im transplantatgewebe ( p < 0 , 05 )  . im bergangsbereich fand sich im beobachtungszeitraum vom dritten bis siebten tag in der nicht bestrahlten gruppe als hinweis auf eine bessere kapillarisierung ein signifikant grerer medianwert als in gruppe 2 ( p = 0 , 004 ) und gruppe 3 ( p = 0 , 004 )  . 
 im transplantatlager zeigte sich im beobachtungszeitraum von dritten bis zum siebten postoperativen tag ein signifikanter unterschied des mittleren kapillarlumens der mit 30 gy bestrahlten tiere sowie der mit 50 gy bestrahlten tiere im vergleich zu den nicht bestrahlten tieren ( p = 0 , 008 )  . 
 diskussion ein klinisches problem der properativen radiotherapie von malignomen im mund - , kieferund gesichtsbereich besteht darin , dass aufgrund strahlenbedingter schdigung zellulrer elemente im bestrahlten transplantatlager ein ber den gefstiel gut vaskularisiertes transplantat verzgert oder gar nicht einheilt . 
in der vorliegenden tierexperimentellen untersuchung an der ratte konnte ein dosiseffekt fr die erfolgssicherheit freier vaskulrer grazilislappen im vorbestrahlten transplantatlager ( 30 gy und 50 gy ) nachgewiesen werden . als hinweis auf eine strahleninduzierte genese dieser einheilungsstrungen konnte im mit 50 gy vorbestrahlten transplantatlager eine aufhebung des regelrechten epithelaufbaus und das auftreten von atypischen morphologien der epithelzellen festgestellt werden . 
im vergleich zum nicht bestrahlten transplantatlagergewebe wurtransplantat lager bergang transplantat / lager gruppe 1 keine bestrahlung gruppe 2 30 gy gruppe 3 50 gy gruppe 1 keine bestrahlung gruppe 2 30 gy gruppe 3 50 gy 3 . 
diese vernderungen waren ebenfalls dosisabhngig und knnen als hinweise auf eine durch die bestrahlung induzierte frhe fibrosierung gewertet werden , da diese vernderungen weder im transplantat noch im unbestrahlten transplantatlager gesehen wurden . histomorphometrisch konnten im transplantatlager nach bestrahlung eine signifikante abnahme der vaskularisation ( p = 0 , 005 ) und eine signifikante reduktion des mittleren kapillarlumens ( p < 0 , 001 ) gegenber dem nicht vorbestrahlten transplantatlager nachgewiesen werden . 
eine einschrnkung des histomorphometrischen analyseverfahren liegt im fehlen des nachweises einer regelrechten kapillarperfusion . die ergebnisse zeigen zum einem , dass es im zeitlichen verlauf zu einer verschlechterung der vaskularisation und abnahme der kapillardurchmesser im mit 30 gy und 50 gy bestrahlten gewebe kommt , zum anderen , dass sich durch ein freies vaskulres weichgewebetransplantat keine verbesserung der vaskularisation im bergangsbereich zum vorbestrahlten gewebe erreichen lsst . 
 [ 19 ] , die eine vaskularisation im bergangsbereich zwischen transplantiertem gewebe und bestrahltem transplantatlager durch eine aussprossung von gefen aus dem transplantat in das transplantatlager diskutierten [ 12 , 19 , 31 ]  . 
vielmehr knnen als ursache fr die stetige abnahme der gefdichte pro gesamtflche eine zunehmende strahleninduzierte fibrosierung mit resultierendem gefverschluss und der zelluntergang von vaskulren endothelzellen durch apoptose angenommen werden [ 11 ]  . 
eine strahleninduzierte fibroseinduktion , die ber eine gesteigerte zytokinexpression , vor allem von transforming growth factor beta ( tgf ( cid : 2 ) ) , eine beschleunigte differenzierung von vorluferfibroblasten zu funktionellen fibrozyten und eine zunehmende produktion von komponenten der extrazellulren matrix ( kollagen ) reguliert wird , ist bereits fr lunge und haut beschrieben worden [ 17 ]  . 
 [ 5 ] zeigten bei patienten ( n = 6 ) bis zu einem jahr nach bestrahlung mit 50 gy noch eine gesteigerte tgf ( cid : 2 ) - expression bei gleichzeitiger fibrosierung des bestrahlten gewebes . zum experimentellen vergleich strahlenbiologischer einflsse auf das transplantatlager wurde neben einer nicht bestrahlten kontrollgruppe eine maximale gesamtreferenzdosis von 50 gy eingesetzt , um die biologische breite strahlungsbedingter vernderungen vollstndig experimentell zu erfassen . die gewhlten strahlendosen mit einer maximalen gesamtreferenzdosis von 50 gy sind bewusst hoch gewhlt , um die biologische breite strahlungsbedingter vernderungen vollstndig experimentell erfassen zu knnen . 
hierbei entsprachen eine bestrahlung mit 30 gy bei anwendung des lq - modells bei einem / ( cid : 2 ) - wert von 10 gy ( typischer frhschaden ) etwa 50 gy und einem / ( cid : 2 ) - wert von 3 gy ( typischer sptschaden ) 78 gy bei einer klinischen fraktionierung mit 2 gy . 
sowohl frhals auch sptschden knnen durch das gewhlte schema erhht sein , da neben der dosis pro fraktion auch die dosisintensitt pro woche , insbesondere die biologische dosisintensitt pro woche , hoch war . 
 da in der vorliegenden experimentellen analyse die vaskularisation im bergangsbereich zwischen transplantat und vorbestrahltem transplantatlager vergleichbar mit dem im vorbestrahlten transplantatlager war , scheinen der vaskularisationszustand des lagergewebes und weniger der vaskularisationszustand des transplantatgewebes limitierend fr die einheilung der transplantate zu sein [ 18 ]  . 
for this reason edp 20 scanditronix diodes , with 20 mm water - equivalent build - up cap , were irradiated by 2 varian linear accelerators ( clinac 1800 and clinac 2100 ) 18 mv photon beams with 3 different collimator settings . 
diodes were calibrated by comparison with a farmer 2571 ionization chamber at reference conditions ( 10 cm ( cid : 2 ) 10 cm open field , source - skin distance 100 cm , build - up depth 3.3 cm ) in order to convert the semiconductor signal into water absorbed dose . 
beam shaping blocks consist of low melting point alloy ( 8 cm height ) placed on a 6 - mm - thick plexiglas tray by a double side adhesive tape . 
the measured data will be interpreted with respect to the influences of the distance - square law and the secondary electron contamination of the photon beam . materials and methods entrance dose measurements were performed by means of p - type edp scanditronix diodes edp20 ( 1.5 mm detector diameter and 20 - mm water - equivalent build - up cap ) [ 6 , 8 ] which were irradiated by 18 - mv photon beams produced by a varian clinac 1800 and a varian clinac 2100 linear accelerators . 
 the upper line represents the source - skin distance correction factor for a standard 10 cm ( cid : 2 ) 10 cm open field and the lower ones are referred to the tray and the shaped field mean values . 
this is mainly due to the simple fact that the source distances of the diode and reference point in the phantom are different and the data in figure 2 correspond very well to the distance - square law . 
however , with shielding blocks and shielding block tray in place , the calibration correction factor is even more diminished , reflecting the entrance secondary electron contamination due to the presence of these materials . the data analysis shows that the block geometry only slightly influences the shaped beam correction factor vs sourceskin distance , whereas it is the tray which mainly affects the diode reading . 
the fact that the differences in shaping blocks ( both in form and in blocked surface ) and collimator settings have no influence on the correction factor corresponds to the observations of wiezorek et al . 
quelle - haut - abstand - ( ssd - ) korrekturfaktor fr offenes , mit eingeschobenem blocktrger versehenes und irregulres feld . due to the function of the shielding block tray as a source of secondary electrons , this effect increases with decreasing source - skin distance , i . 
focus - skin distance and shaping block tray also compton scattered photons produced by the photon beam across the tray and the transmission blocks could play a role , as described by other authors [ 2 , 3 ] , but in this case one would expect a more expressed effect of the block configuration . the good agreement between the experimental values and the linear fitting means that the interpolating line equation strahlentherapie und onkologie urban & vogel 2000 aktuelles forum der fehler zweiter art und seine bedeutung bei der beurteilung von resultaten qualittsanalyse der zeitschrift strahlentherapie und onkologie annette raabe1 , hans - hermann dubben1 , hans - peter beck - bornholdt2 hintergrund : das ziel der vorliegenden arbeit ist es , die wissenschaftliche qualitt der beitrge in strahlentherapie und onkologie zu verbessern und damit auch den impact factor anzuheben . material und methoden : in allen 181 arbeiten der rubriken aktuelles forum , originalarbeiten und kurzmitteilungen der jahrgnge 1998 und 1999 wurde der korrekte umgang mit dem fehler zweiter art berprft . ergebnis : 99 publikationen wurden aus unterschiedlichen und im einzelnen spezifizierten grnden von der bewertung ausgeschlossen . 
in keiner einzigen der verbleibenden 82 klinischen publikationen wurden berlegungen zum fehler zweiter art angestellt . schlussfolgerung : zur verbesserung der qualitt der zeitschrift ist es wnschenswert , den fehler zweiter art zumindest in klinischen arbeiten in zukunft zu bercksichtigen . 
autoren , gutachter und herausgeber der zeitschrift sollten darauf achten , dass entsprechende berechnungen durchgefhrt werden . schlsselwrter : fehler zweiter art power qualittssicherung type ii error and its relevance for interpretation of results . 
audit of the journal strahlentherapie und onkologie background : the statistical quality of the contributions to strahlentherapie und onkologie is assessed , aiming for improvement of the journal and consequently its impact factor . material and methods : all 181 articles published during 1998 and 1999 in the categories review , original contribution , and short communication were analyzed concerning the appropriate consideration of type ii error . result : ninety - nine publications were excluded from analysis for different specified reasons . 
in none of the remaining 82 clinical publications type ii error was considered . conclusion : authors , peer reviewers , and editors could contribute to improve the quality of the journal by setting value on adequate consideration of type ii error . key words : type ii error power audit b ei der auswertung klinischer forschungsergebnisse ist die anwendung adquater statistischer verfahren unabdingbare grundvoraussetzung fr eine korrekte interpretation der resultate . 
es ist geplant , diese bestandsaufnahme in etwa zwei jahren zu wiederholen , um qualitative vernderungen feststellen zu knnen . fehler zweiter art und statistische power die etwas abstrakt bezeichneten fehler erster art und fehler zweiter art sind keineswegs auf statistische probleme beschrnkt . 
mchte man hingegen vermeiden , dass auch nur ein einziger tatschlicher verbrecher irrtmlich freigesprochen wird , dann muss man die ansprche an die zeugen und indizien reduzieren . damit ist aber unweigerlich verbunden , dass auch einige unschuldige eingesperrt werden . 
dem irrtmlich freigesprochenen verbrecher entspricht das tatschlich vorhandene bedeutsame ergebnis , das in einer studie jedoch zufllig bersehen wird . betrachten wir ein beispiel : ein arzt hat in einer klinischen studie die wirksamkeit zweier therapien miteinander verglichen . 
eine analyse der daten ergibt einen p - wert von 0 , 6 , und der statistiker bezeichnet den unterschied zwischen den beiden therapien als nicht signifikant . dies bedeutet lediglich , dass es nicht gelungen ist , einen unterschied plausibel aufzuzeigen . 
man kann daraus jedoch nicht ableiten , dass die beiden therapien tatschlich gleichwertig sind , denn es besteht die mglichkeit , dass das problem einfach nur nicht genau genug untersucht wurde . 
man konnte lediglich die schuld des angeklagten nicht nachweisen . aus statistischer sicht ist es sogar grundstzlich unmglich zu beweisen , dass zwei therapien exakt gleiche wirksamkeit besitzen [ 136 ]  . 
so mag bei der wirksamkeit eines schmerzmittels ein unterschied von weniger als fnf prozentpunkten klinisch nicht mehr relevant sebei einer radiogenen myelitis hingegen wre ein unterschied von einem prozentpunkt bereits von hoher klinischer relevanz . bei der planung einer studie , aber auch beim studium einer publikation ist die kenntnis des klinisch relevanten unterschieds unerlsslich . 
dies wre dann der klinisch relevante unterschied . die power gibt an , mit welcher wahrscheinlichkeit wir den von uns als klinisch relevant erachteten unterschied mit statistischer signifikanz nachweisen knnen , falls er vorhanden ist . 
das beinhaltet natrlich ein risiko von 20% , mit der studie den klinisch relevanten unterschied zu bersehen , also einen fehler zweiter art zu begehen [ 14 ]  . im gegensatz zum signifikanzniveau , das international fast immer 5% betrgt ( p 0 , 05 ) , ist bei der power die konvention nicht ganz so starr . 
in den international fhrenden medizinischen fachzeitschriften ist eine power von 80% blich . der anteil der studien mit einer power von 90% nimmt in den letzten jahren jedoch zu . die power einer studie hngt nicht nur von dem als klinisch relevant erachteten unterschied ab , sondern auch von der anzahl der patienten , der hufigkeit der beobachteten ereignisse ( sterbefall , rezidiv , eintritt einer nebenwirkung ) und von dem gewhlten signifikanzniveau . 
die anzahl der patienten , die fr eine studie bentigt werden , kann berechnet werden . das ist jedoch relativ kompliziert und ergibt , selbst wenn man nur den hufigsten fragestellungen gerecht werden will , ein umfangreiches tabellenwerk . 
wir werden uns hier mit einer faustformel begngen , die recht gute abschtzungen erlaubt . auch unmittelbar einleuchtend ist , dass die hufigkeit der zu beobachtenden ereignisse einen einfluss auf die power hat . 
wenn man feststellen mchte , ob eine sehr seltene nebenwirkung bei den betrachteten behandlungen verschieden hufig auftritt , dann muss man viel mehr patienten untersuchen , als wenn das ereignis bei jedem zweiten patienten eintritt . dass die fehler erster und zweiter art voneinander abhngen , liegt nicht so unmittelbar auf der hand . 
aber das eingangs angefhrte rechtsprechungsdilemma hat uns bereits darauf eingestimmt , dass die beiden fehler nicht unabhngig voneinander sind . in tabelle 1 gibt die erste spalte an , welchen unterschied wir mit der gesamtzahl der patienten , die in der zweiten spalte angegeben ist , erkennen knnen . 
die formel gilt fr studien mit irrtumswahrscheinlichkeiten von 5% fr den fehler erster art . dies ist alles nicht neu , dennoch ist der fehlschluss wo kein signifikanter unterschied gefunden wird , da ist auch kein unterschied , in der medizinischen forschung weit verbreitet . qualittsanalyse der zeitschrift strahlentherapie und onkologie ( jahrgnge 1998 und 1999 ) alle arbeiten der rubriken aktuelles forum , originalarbeiten und kurzmitteilungen wurden von zwei beobachtern ausgewertet . 
tabelle 1 wurde berechnet fr eine fnfprozentige wahrscheinlichkeit des fehlers erster art ( 5% signifikanzniveau ) und eine 20 - prozentige wahrscheinlichkeit des fehlers zweiter art ( 80% power )  . 
aber wrden sie einen feuermelder kaufen , der eine fehlalarmquote von 5% hat und der bei 20% der brnde keinen alarm schlgt ? in tabelle 2 gibt die zweite spalte an , welche power fr einen realen unterschied in den heilungsraten von 20 prozentpunkten mit der gesamtzahl der patienten , die in der ersten spalte angegeben ist , erzielt werden kann . 
sind jedoch nur 60 patienten in der studie , so wird ein unterschied von 20 prozentpunkten nur in etwa einem drittel der flle erkannt . nachweisbarer unterschied * gesamtzahl der bentigten in prozentpunkten auswertbaren patienten tabelle 1 . 
assumptions : even distribution of patients between groups ; type i error of 5% ; type ii error of 20% . 2800 10% gesamtzahl der patienten power 1012% 1519% 1928% 2843% 1215% 4376% tabelle 2 . 
der fehler zweiter art und seine bedeutung bei der ergebnisbeurteilung schlossen , in denen entweder keine eigenen daten vorgestellt wurden [ 50 , 51 , 57 , 134 , 174 ] oder die keine quantitativen ergebnisse enthielten ; dies waren bersichtsartikel [ 1 , 2 , 34 , 36 , 63 , 74 , 75 , 105 , 117 , 144 , 165 , 171 , 177 , 180 ] , fallbeschreibungen [ 30 , 42 , 68 , 99 , 107 , 133 , 139 , 175 ] , kommentare [ 46 , 53 , 83 , 90 , 115 , 127 , 172 , 173 ] , ein tagungsbericht [ 137 ] sowie ein bericht ber die praxis der prophylaxe und therapie akuter nebenwirkungen [ 181 ]  . 
das entspricht einem prozentualen anteil von 0% ( einseitiges 95% - konfidenzintervall bis 3 , 6% )  . als anhaltspunkt fr den fehler zweiter art dient die anzahl der untersuchten patienten in den studien ( tabelle 1 , abbildung 1 )  . 
mit den 1 588 patienten dieser studie erzielt man eine power von 90% fr das entdecken von 8%unterschieden . manahmen zur qualittsverbesserung zur verbesserung der qualitt der zeitschrift ist es wnschenswert , dass der fehler zweiter art bei der planung und auswertung klinischer studien bercksichtigung findet . 
a 2 - week pretreatment with 13 - cisretinoic acid + interferon - ( cid : 3 ) - 2a prior to definitive radiation improves tumor tissue oxygenation in cervical cancers . 
the total dose of the external beam irradiation varied between 60 and 98 gy for external beam radiotherapy alone and 10 gy to 82 gy for combined external beam radiotherapy and iodine seeds . 
one to 4 iodine seeds with a median activity of 21.05 mbq were permanently implanted 3 days before the start of external radiotherapy or 6 and 7 iodine seeds alone were used . 
local tumor control rates were determined and tcd37% values were calculated applying the maximum likelihood method . results : with increasing number of implanted iodine seeds the tcd37% ( of external beam irradiation ) decreased . 
 conclusions : the combined treatment of tumors with implanted low - dose - rate iodine seeds and external beam irradiation can decrease the total dose of the external beam irradiation and , hence , offer the possibility of considerable dose sparing of normal tissues without compromising local tumor control rates . key words : interstitial brachytherapy iodine seeds fractionated external beam irradiation tcd37% local tumor control experimental tumor system kombinierte fraktionierte externe bestrahlung und low - dose - rate - jod - 125 - seeds in einem experimentellen tumorsystem hintergrund : prfung des effekts der kombination von permanent implantierten low - dose - rate - jod - 125 - seeds und fraktionierter externer bestrahlung auf die lokalen tumorkontrollraten in einem experimentellen tumorsystem . material und methoden : die experimente wurden am rhabdomyosarkom r1h der ratte durchgefhrt , welches subkutan auf den rcken von wag / raj - albinoratten transplantiert wurde . 
die gesamtdosen der externen bestrahlung variierten zwischen 60 und 98 gy fr alleinige externe bestrahlung und 10 und 82 gy fr die kombination aus externer bestrahlung und implantierten jod - seeds . 
ein bis vier jod - seeds mit einer medianen aktivitt von 21 , 05 mbq wurden drei tage vor beginn der externen bestrahlung permanent in die tumoren implantiert ; als kontrollen wurden tumoren mit sechs bis sieben jod - seeds permanent implantiert ohne zustzliche externe bestrahlung . 
nach alleiniger externer bestrahlung betrug die tcd37% 103 , 2 gy ( 95% - vertrauensbereich 101 , 3 bis 105 , 1 gy ) und nahm nach implantation eines jod - seeds auf 69 , 7 gy ( 63 , 7 bis 74 , 7 gy ) ab bzw . 
external beam irradiation and iodine - 125 seeds schlussfolgerung : die kombination von externer bestrahlung und implantation von jod - seeds in tumoren ermglicht eine erhebliche verringerung der extern applizierten dosis und damit auch eine verringerung der belastung von normalgeweben ohne gefahr niedriger tumorkontrollraten . schlsselwrter : interstitielle brachytherapie jod - seeds fraktionierte externe bestrahlung lokale tumorkontrolle tcd37% experimentelles tumorsystem i nsufficient local control of the primary tumor still is the main obstacle for a tumor cure in most solid tumors . 
several approaches may be used to avoid this dilemma by reducing the volume of normal tissue included in the treatment field ( stereotactic radiotherapy , conformal radiotherapy , 3 - d treatment planning )  . 
the application of implantable radioactive devices in combination with external beam therapy are attractive , as the dose delivered to the tumor might be increased without increasing the risk of unacceptable normal tissue toxicity . 
here we report on the results of combined fractionated external beam radiotherapy and implanted low - dose - rate iodine - 125 seeds in an experimental tumor syste materials and methods tumor - host system the experiments were done on the rhabdomyosarcoma r1h of the rat . 
the total doses applied varied between 60 and 98 gy in 6 to 10 weeks for external beam radiotherapy alone and 10 to 82 gy in 1 to 8 weeks for external beam radiotherapy combined with iodine - 125 seeds . 
though a regular spacing of iodine seeds was attempted if more than 1 seed was used , this was usually not feasible due to seed movements within hours to days after implantation . 
the number of animals per group varied between 3 and 7 ; accidentally , 1 animal received 7 iodine seeds . all experiments were approved by the local ethics committee on animal experiments . endpoints and data analysis local tumor control rates were used as the endpoint . 
the statistical analysis applied the maximum likelihood method assuming poisson statistics : p = exp ( - n ) where p denotes the probability of local tumor control and n the average number of clonogenic tumor cells after treatment . 
assuming isoeffectivity of the dose fractions n = n0 exp ( - d / d0 ) where n0 is the number of clonogenic tumor cells at the start of treatment , d the total dose , and d0 the radiosensitivity . 
n0 can be determined using the tumor volume v0 at the start of treatment and the numeric density of the clonogenic tumor cells : n0 = n0 v0 n0 amounts to 2.3 ( cid : 2 ) 108 cells per gram [ 6 ]  . 
the initial tumor volume was determined for each individual tumor measuring 2 perpendicular tumor diameters and assuming a rotational ellipsoid . the total dose d was composed of the dose delivered by external beam radiotherapy de and implanted iodineseeds : d = de + n an where n is the number of implanted iodine seeds and an the effective dose per seed of n iodine seeds . 
die durchgezogene linie zeigt die lineare regression mit 95%vertrauensbereich der regression ( r2 = 0 , 9473 , p = 0 , 0011 )  . for all treatments and a variable parameter an depending on the number of iodine seeds implanted . discussion results in figure 1 the local tumor control dose ( tcd37% ) for 1 - g tumors is shown . 
these tumor cells could be expected to proliferate at a lower rate than clonogenic cells in the periphery of the tumor with better nutritional support and oxygenation status . continuous irradiation with low - dose - rate iodine - 125 seeds can be advantageous under these circumstances as tumor cells may have a higher probability of being redistributed to radiosensitive phases of the cell cycle compared to acutely irradiated tumor cells . with increasing number of implanted iodine - 125 seeds the external dose can be decreased . 
experiments by doll [ 3 ] at the same tumor system with series of x - ray images taken at different times during seed implantation showed that the seeds moved within the tumors . 
however , tumor volume shrinkage can bring about a 30% increase in dose delivered to tumor or adjacent normal tissue which might shrink centripetally towards the implanted iodine seeds as was calculated by dale et al . 
 [ 2 ] based on clinical data of kreth et al . [ 8 ] in glioblastoma patients implanted with iodine - 125 seeds . problems with seed implantation geometry might be minimized with ctor ultrasound - based planning systems , which allow target volume directed planning of the brachytherapy procedure . 
different dose plans might be evaluated according to a specified index termed coin . in summary , implanted seeds offer the possibility of considerable dose sparing of normal tissues if used in combination with external beam irradiation . acknowledgements : the skillful technical assistance of maria omniczynski is gratefully acknowledged . 
 jung is highly appreciated for extensive discussions and suggestions he contributed to the work . strahlentherapie und onkologie urban & vogel 2000 originalarbeit endoskopische prtherapeutische clipmarkierung von tumoren im gastrointestinaltrakt eine methode zur exakteren definition von zielvolumina michaela riepl1 , alexander pietsch2 , gunther klautke1 , roman fehr1 , rainer fietkau1 hintergrund : bei tumoren im gastrointestinaltrakt gelingt es im computertomogramm ( ct ) fr die 3 - d - bestrahlungsplanung hufig nicht , die genaue ausdehnung des primrtumors zu verifizieren . 
dies erschwert bei der planung der perkutanen strahlentherapie die exakte bestimmung des makroskopischen tumorvolumens und somit die des zielvolumens erster ordnung ( zv 1 ) , in einigen fllen auch bereits die des zielvolumens zweiter ordnung ( zv 2 )  . patienten und methode : elf patienten mit makroskopischen tumoren ( rektumkarzinom : n = 5 , distales sophagus - / kardiakarzinom : n = 6 ) vor neoadjuvanter oder definitiver radiochemotherapie wurden in die analyse aufgenommen . unmittelbar vor der 3 - d - bestrahlungsplanung wurden endoskopisch der distale und proximale tumorrand mit metallclips versehen , anschlieend erfolgten das planungs - ct und die definition des zielvolumens zweiter ordnung . 
von zwei unabhngigen untersuchern wurde beurteilt , inwiefern die durch clips definierte primrtumorausdehnung einfluss auf die gewhlten planungszielvolumina hatte und ob die anzahl der clips zum zeitpunkt des zweiten planungs - ct noch ausreichend war , um das zielvolumen erster ordnung eindeutig festzulegen . ergebnisse : bei allen patienten gelang es komplikationslos , die tumorrnder durch clips zu markieren . 
bei ausgeprgter tumorrckbildung nach neoadjuvanter radiochemotherapie erleichterten die markierungen in drei fllen intraoperativ die genaue bestimmung der primrtumorregion . schlussfolgerung : bei patienten mit tumoren im gastrointestinaltrakt erleichtert die prtherapeutische clipmarkierung die definition der zielvolumima und erhht die przision der planung . 
die clips sind auf den rntgendokumentationsaufnahmen der bestrahlungsfelder in der regel gut nachzuvollziehen und tragen so zur qualittskontrolle bei . schlsselwrter : clipmarkierung gastrointestinale tumoren bestrahlungsplanung endoscopic clipping for gastrointestinal tumors . 
a method to define the target volume more precisely background : in many cases it is not possible to exactly define the extension of carcinoma of the gastrointestinal tract with the help of computertomography scans made for 3 - d - radiation treatment planning . 
consequently , the planning of external beam radiotherapy is made more difficult for the gross tumor volume as well as , in some cases , also for the clinical target volume . 
with the help of the clips it was possible to exactly define the position and the extension of the primary tumor . the clinical target volume was modified according to the position of the clips in 5 / 11 patients ; the gross tumor volume was modified in 7 / 11 patients . 
moreover , the clips helped the surgeon to define the primary tumor region following marked regression after neoadjuvant therapy in 3 patients . conclusions : endoscopic clipping of gastrointestinal tumors helps to define the tumor volumes more precisely in radiation therapy . 
das alter der patienten ( neun mnner , zwei frauen ) lag zwischen 41 und 69 jahren . prtherapeutische diagnostische untersuchungen bei den sechs patienten mit sophagus - / kardiakarzinom waren in allen fllen ein ct und eine gastroskopie verbunden mit einer endosonographie durchgefhrt worden , in jeweils einem fall ein sophagusbreischluck und eine kernspintomographie . 
ein patient mit kardiakarzinom klagte nach der clipmarkierung ber vorbergehende abdominelle schmerzen , die mit eib ei gastrointestinalen tumoren knnen der tumorsitz und die karzinomausdehnung sowohl im diagnostischen computertomogramm ( ct ) als auch im planungs - ct trotz sorgfltiger oraler , rektaler und intravenser kontrastmittelapplikation hufig nicht exakt bestimmt werden . 
diese methoden knnen zur bestrahlungsplanung jedoch nicht direkt eingesetzt werden . beispielsweise differieren beim rektumkarzinom die angaben zum abstand des tumors von der anokutangrenze und lngenausdehnung zwischen starrer rektoskopie und koloskopie . 
bei tumoren des sophagus oder des sophagogastralen bergangs gelingt es zwar meist , die angegebenen mae fr den proximalen tumorrand auf das ct zu bertragen , hufig in relation zur trachealbifurkation , wobei bereiche mit flchigem wachstum nicht identifiziert werden knnen . 
problematisch ist jedoch vielfach die genaue definition des tumorunterrandes , die in der endoskopie meist nur in beschreibungen wie : der tumor greift auf die kardia ber , zusammengefasst wird . 
 im rahmen der properativen radio - ( chemo - ) therapie muss das zielvolumen mglichst klein und individuell angepasst sein , um postoperative komplikationen zu reduzieren . vergleichbar gilt es bei der definitiven radiochemotherapie , bei der hhere dosen erforderlich sind , akutund spttoxizitt durch mglichst exakt konformierte felder zu minimieren . 
der bestrahlungsbeginn verzgerte sich durch diesen eingriff nicht . bei den patienten mit rektumkarzinom wurden durchschnittlich fnf clips gesetzt , zwei bis vier clips kranial , null bis vier clips kaudal . 
die sophagus - / kardiakarzinome wurden durchschnittlich mit sechs clips markiert , zwei bis drei clips hiervon kranial , drei bis vier kaudal ( tabellen 1 und 2 )  . auffallend war bei der zur clipmarkierung durchgefhrten endoskopie , dass in allen fllen die tumorstenose berwunden werden konnte , zum teil nach bougierung oder mit dnneren endoskopen . 
planning ct slice with clipping ; abanal ( a ) and anal ( b ) border of the tumor ; rectal cancer ; neoadjuvant therapy planned . abbildung 3a figure 3a abbildung 3b figure 3b abbildungen 3a und 3b . 
bei zehn der elf patienten war die clipmarkierung vorher erfolgt , achtmal hiervon am gleichen tag , jeweils einmal am vortag oder zwei tage vorher . nur beim ersten patienten war die clipmarkierung nach der primren ct - planung vorgenommen worden , da hierbei die tumorausdehnung nicht ausreichend bestimmbar gewesen war . 
planning target volume nach icru [ 9 ] beinhaltet neben den oben genannten regionen auch noch einen sicherheitssaum , der , wie gefordert [ 7 ] , bei unserer unten folgenden definition der zielvolumina eingeschlossen ist . 
da fr diese zielvolumina mit sicherheitssaum keine eigene benennung definiert ist ( zum beispiel planungszielvolumen 2 und 1 ) , werden die begriffe zielvolumen zweiter und erster ordnung beibehalten . bestrahlungsplanung zielvolumina und bestrahlungstechnik beim rektumkarzinom : das zielvolumen zweiter ordnung umfasste die primrtumorregion sowie die risikobezirke prsakral entlang der blasenhinterwand bzw . 
das zielvolumen zweiter ordnung ( zv 2 ) ist hier als makroskopischer tumor ( primrtumor und befallene lymphknoten ) und potenzielles tumorausbreitungsgebiet definiert , entsprechend das zielvolumen erster ordnung ( zv 1 ) als makroskopisch befallene regionen . 
laut icrurichtlinien [ 9 ] entsprche das zielvolumen zweiter ordnung dem ctv ( clinical target volume ) , das zielvolumen erster ordnung dem gtv ( gross tumor volume )  . zielvolumina und bestrahlungstechnik beim distalen sophagus - / kardiakarzinom : das zielvolumen zweiter ordnung umfasste nach kranial in allen fllen den sophagus beziehungsweise die parasophagealen lymphknoten bis in hhe des jugulums , wobei 5 cm abstand zum oberrand des makroskopischen tumorbefalls bestehen mussten . 
beim zielvolumen erster ordnung betrug der sicherheitsabstand zum makroskopischen tumorbefall in alle richtungen 2 cm . die bestrahlung erfolgte sowohl fr das zielvolumen zweiter ordnung als auch fr das zielvolumen erster ordnung ber drei bis vier felder in isozentrischer technik unter verwendung von individualkollimatoren , die je nach tumorlokalisation und - ausdehnung zur mglichst guten lungenschonung ausgewinkelt wurden ( gantry zum beispiel 0 , 180 , 255 , 105 )  . 
 [ 12 ] zum rektumkarzinom . ergebnisse abgrenzbarkeit des tumors durch die vordiagnostik bei den patienten mit rektumkarzinom handelte es sich in vier fllen um tumoren im unteren drittel , bei denen der tumorunterrand direkt durch den oberrand des analkanals definiert war . 
viermal war der oberrand darstellbar , der untere tumorrand aber nicht , zweimal der unterrand bei fehlenden angaben ber den oberrand . einfluss der clipmarkierung auf das zielvolumen zweiter ordnung die clips ermglichten in allen fllen eine genaue definition der lage und kraniokaudalen ausdehnung des primrtumors im ct . 
diese relativen grenvernderungen der zielvolumina wurden von zwei unabhngigen untersuchern beurteilt und eingestuin fnf fllen , einmal rektumkarzinom , viermal sophagus - / kardiakarzinom , war die clipmarkierung bereits fr die festlegung des zielvolumens zweiter ordnung entscheidend . 
 nderung des zielvolumens zweiter ordnung beim rektumkarzinom : bei einer patientin mit einem karzinom am rektosigmoidalen bergang war im ct die primrtumorregion nicht sicher zu identifizieren , suspekt wirkte eine darmschlinge , die lateral am vergrerten uterus fixiert zu sein schien . nach der clipmarkierung zeigte sich allerdings , dass der primrtumor weiter kranial und ventral lag , sodass er bei blicher konturierung nur knapp am feldrand gelegen htte . 
 nderung des zielvolumens zweiter ordnung beim sophagus - / kardiakarzinom : bei den patienten mit sophagus - / kardiakarzinom war in zwei fllen der tumorunterrand weiter kaudal gelegen als in den voruntersuchungen beschrieben . in einem fall zeigte sich hierbei ein vorher nicht entdeckter fundusbefall , der durch zirkulre clipmarkierung im planungs - ct gut erkennbar war . 
in zwei fllen konnte das zielvolumen kleiner gewhlt werden , da der markierte tumorunterrand weiter kranial lag als vorher diagnostiziert . einfluss der clipmarkierung auf das zielvolumen erster ordnung wie bei der festlegung des zielvolumens zweiter ordnung wurden die gewhlten zielvolumina mit denen verglichen , die sich aus der vorliegenden diagnostik ohne clips ergeben htten . 
das zielvolumen erster ordnung wurde insgesamt in sieben fllen durch die clipmarkierung verndert : nderung des zielvolumens erster ordnung beim rektumkarzinom : bei der patientin mit dem oben beschriebenen tumor am rektosigmoidalen bergang wre es unserer meinung nach ohne die markierungen nicht mglich gewesen , das boostvolumen korrekt zu whlen . 
in diesem und einem weiteren fall eines rektumkarzinoms whlten wir das zielvolumen erster ordnung auerdem grer als blich : da jeweils nach oraler applikation einer bariumlsung eine kontrastierte dnndarmschlinge in allen drei boostfeldern lag , htten wir uns in unkenntnis der exakten tumorlage fr eine individuelle ausblockung dieser darmschlingen in einem der felder ( gantry 180 , patient in rckenlage ) bzw . 
bei einer patientin konnte der boost kleiner gewhlt werden , da der tumoroberrand weiter kaudal lag als der vorbeschreibung nach angenommen . nderung des zielvolumens erster ordnung beim sophagus - / kardiakarzinom : bei den patienten mit sophagus - / kardiakarzinom war bei den zwei patienten , bei denen das zielvolumen zweiter ordnung durch die clips kleiner gewhlt werden konnte , auch das boostvolumen kleiner ; in den zwei fllen , in denen sich ein ausgedehnterer tumorbefall gezeigt hatte , war das zielvolumen erster ordnung grer . haltbarkeit der clips in sechs fllen , bei allen fnf patienten mit rektumkarzinom und bei einem patienten mit kardiakarzinom , war auch bei der verifikation der boostfelder noch eine ausreichende anzahl der markierungen vorhanden , um den tumoroberund - unterrand festzulegen . 
 erfolgte das ursprngliche planungs - ct nicht am tag der clipmarkierung , sondern wie bei zwei patienten einen oder zwei tage spter , fehlte in unserem kollektiv schon jeweils ein clip ( siehe tabellen 1 und 2 )  . 
in drei fllen ein patient mit sophaguskarzinom , zwei patienten mit rektumkarzinom fhrte die neoadjuvante therapie zu einer so guten makroskopischen rckbildung des tumors , dass die clips fr die chirurgen eine wichtige hilfe zur exakten definition der primrtumorregion waren . 
 diskussion bei der beurteilung des sitzes und der ausdehnung von sophagusund rektumkarzinomen dominieren fr die festlegung der tumorausdehnung kraniokaudal die endoskopie , fr die beurteilung der wandberschreitung und peritumoraler lymphknoten die endosonographie . 
das nmr liefert gegenber dem ct keine zustzlichen informationen , was die primrtumorausdehnung betrifbei einem unserer sophaguskarzinompatienten wurde im kernspintomogramm ein ausgedehnter fundusbefall diagnostiziert , der sich bei der clipmarkierung nicht besttigte . 
unzureichend ist sowohl im ct als auch im nmr und dies ist vor allem fr die festlegung strahlentherapeutischer zielvolumina entscheidend auch die mglichkeit ein flchenhaftes , aber wenig infiltrierendes wachstum zu erkennen . 
die radioonkologische empfehlung , aus diesem grund vor allem bei sophaguskazinomen den sicherheitssaum kraniokaudal grozgig zu whlen ( zielvolumen zweiter ordnung : 3 bis 5 cm [ 14 ] ) , kann ber diesen mangel an information nicht hinwegtuschen . fr die boostplanung von mammakarzinomen ist das intraoperative clippen des tumorbettes eine etablierte methode , um postoperativ unter durchleuchtung oder im planungsct den ursprnglichen tumorsitz zu identifizieren . 
fr das properative clippen von gastrointestinalen tumoren fehlen klinische daten bisher , lediglich eine verffentlichung schildert einen einzelfall , in dem die prtherapeutische clipmarkierung eines sophaguskarzinoms die planung der radiotherapie erleichterte [ 15 ]  . bei mittels 3 - d - planung immer exakter geplanten und individuell kollimierten zielvolumina wachsen ebenfalls die anforderungen an die qualittskontrolle und - sicherung der medizinischen festlegung der tumorausdehnung . 
mit der clipmarkierung ist die bertragbarkeit der computerplanung auf den patienten besser kontrollierbar , da bei der dokumentation der bestrahlungsfeldpforten ( ersteinstellung ) oder bei einer weiteren rntgenkontrolle ( nicht verifikationsfilme ) im laufe der bestrahlungen die lage der clips auf dem film nachvollziehbar ist . 
damit das verfahren erfolgreich eingesetzt werden kann , ist eine exakte zeitliche planung notwendig : endoskopie , clippung , definition des isozentrums unter rntgensimulation und planungs - ct mssen an einem tag erfolgen . 
die dazu notwendige interdisziplinre zusammenarbeit war bei uns problemlos . ein zustzlicher vorteil der clipmarkierung kann bei der definitiven operativen sanierung entstehen : nach sehr guter makroskopischer rckbildung oder sogar einer vollremission geben verbliebene clips dem chirurgen hinweise zur ursprnglichen ausdehnung des tumors . 
clipmarkierung von gastrointestinalen tumoren entzndliche vernderungen von tumorinfiltrationen nach neoadjuvanter therapie hufig nicht zu unterscheiden [ 1 , 10 ]  . kardiakarzinome ; hier ging es vor allem um die festlegung des tumorunterrandes . 
 schlussfolgerung bei patienten mit tumoren im sophagus und rektum , bei denen im ct die ausdehnung des primrtumors nicht klar erkennbar ist , erleichtert die prtherapeutische clippung der tumorregion die definition der zielvolumina in allen fllen . 
in unserem kollektiv traf dies besonders auf rektumkarzinome im mittleren oder oberen drittel zu sowie auf distale sophagus - / die clips sind in den meisten fllen auf den ersteinstellungsaufnahmen der endgltigen bestrahlungsfelder zu erkennen , verbessern so die verifikation und tragen zur qualittskontrolle bei . 
die radiotherapie nimmt im rahmen der schmerztherapie , der behandlung von ( drohenden ) frakturen und von myelonkompressionen eine wichtige rolle im palliativen konzept eziel der vorliegenden retrospektiven arbeit ist es , anhand dieser indikationen den effekt der strahlentherapie auf analgesie , rekalzifizierung und neurologische symptomatik am eigenen patientenkollektiv aufzuzeigen und mgliche einflussfaktoren auf den therapieeffekt zu evaluieren . patienten und methoden : vom 1 . 
1998 wurden 42 patienten ( 19 frauen , 23 mnner ) im alter von 46 bis 85 jahren ( median : 64 , 9 jahre ) in 71 zielvolumina aufgrund einer bestehenden symptomatik ( 67 / 71 : ossre schmerzen , 45 / 71 : fraktur / - gefahr , 13 / 71 : rckenmarkkompression ) radiotherapiert ( median 36 gy , 2 bis 3 gy 5 - mal / woche )  . die zeit zwischen diagnose und erster bestrahlung betrug im median 11 , 9 monate ( 0 , 3 bis 90 monate )  . 
zum zeitpunkt der ersten radiotherapie befanden sich fnf patienten im stadium ii , 37 im stadium iii nach salmon / durie ; der karnofsky - index lag im median bei 70% ( 40 bis 90% )  . 
das mediane berleben aller patienten nach erstdiagnosestellung betrug 34 , 9 monate ( 7 , 5 bis 119 , 3 monate ) , nach erster radiotherapie 13 , 1 monate ( 0 , 2 bis 105 , 3 monate )  . schlussfolgerung : die radiotherapie ist bei adquater indikationsstellung unabhngig vom zeitpunkt ihres einsatzes eine effektive palliative manahme . 
das berleben bleibt durch die bestrahlung unberhrt . schlsselwrter : multiples myelom radiotherapie palliation role of radiotherapy in the treatment of multiple myeloma background : chemotherapy is the treatment of choice in multiple myeloma ; but there are no curative options . 
in our retrospective study we report the effect of radiotherapy on reduction of pain , recalcification and the reduction of neurological symptoms and evaluate factors which have an impact on therapeutic outcome . 
dec 1998 , 42 patients ( 19 women , 23 men ; range of ages 46 to 85 years , median age 64.9 years ) with 71 target volumes were irradiated ( median dose 36 gy , 2 to 3 gy 5 times / week ) because of symp - tomatic disease ( 67 / 71 : osseous pain , 45 / 71 : fractures / impending fractures , 13 / 71 : spinal cord compression ) ( tables 1 and 2 )  . 
 results : during follow - up ( at least 6 months ) in 85% of target volumes complete and partial pain relief ( measured by patients perception and the use of analgetic medication ) was achieved ; recurrences were seen in 8.8%. 
aufgrund der palliativen situation besteht bei erstdiagnosestellung daher nicht zwingend sofortiger handlungsbedarf ; der erkrankungsbeginn ist hufig symptomarm und uncharakteristisch . schmerzhafte knochendestruktionen , knochenmarkdepressionen mit anmie , episoden von niereninsuffizienzen , hyperkalzmien , rezidivierende bakterielle infekte und neurologische symptome prgen den weiteren verlauf [ 2 , 5 , 17 , 18 ]  . 
hierbei ist aufgrund der infiltration des knochenmarks mit malignen plasmazellen und der gesteigerten osteoklastenttigkeit mit einer inzidenz von 55 bis 90% der ossre schmerz das fhrende symptom [ 17 , 18 , 23 ]  . 
 die radiotherapie nimmt dabei als lokales verfahren im palliativen konzept zum zweck der schmerzlinderung , der ossren stabilisierung sowie der reduktion neurologischer symptome einen wichtigen stellenwert ein [ 9 ]  . 
ziel der vorliegenden retrospektiven arbeit ist es daher , anhand der bestehenden indikationen den effekt der strahlentherapie auf analgesie , rekalzifizierung und neurologische symptomatik am eigenen patientengut aufzuzeigen und mgliche einflussfaktoren auf den therapieverlauf zu evaluieren . 
der ausschluss aus unserer analyse erfolgte bei vorliegen einer aktuell behandlungsbedrftigen malignen zweiterkrankung ( n = 7 ) , bei unzureichender datenlage ( n = 3 ) , bei nicht durchgefhrter behandlung ( n = 3 ) sowie bei abbruch der radiotherapie vor erreichen der geplanten gesamtdosis ( n = 7 ) aufgrund einer operationswrdigen pathologischen fraktur ( 2 / 7 ) , der foudroyanten verschlechterung des allgemeinzustands ( 2 / 7 ) , einer anhaltenden thrombopenie , eines myelominduzierten todesfalles sowie aufgrund des wunsches eines patienten ( je 1 / 7 )  . 
dritten zeitpunkt radiotherapiert ( tabelle 1 )  . knochenschmerzen ( n = 26 ) , auffllige laborwerte bei symptomlosigkeit ( n = 7 ) und pathologische frakturen ( n = 4 ) hatten zur erstdiagnose gefhrt ; bei fnf patienten bestand initial die diagnose einer monoklonalen gammopathie unbekannter signifikanz ( n = 5 )  . 
whrend die mehrheit der patienten zum zeitpunkt der erstdiagnose im stadium i und ii ( salmon / durie ) war , befanden sich die meisten zum zeitpunkt der ersten radiotherapie im stadium iii . 
whrend der bestrahlung von 34 zielvolumina ( 47 , 8% ) kamen bisphosphonate zum einsatz . die zeitspanne zwischen erstdiagnose und erster bestrahlung betrug 0 , 3 bis 90 monate ( median 11 , 9 monate )  . 
22 patienten ( 52 , 3% ) wurden innerhalb des ersten jahres nach diagnosestellung erstmalig radiotherapiert , die anderen 20 gesamtzahl der pro patient bestrahlten zielvolumina ( zv ) anzahl der verteilung der zv patienten auf die bestrahlungs - ( rt - ) behandlungen 1 . 
patients and tumor characteristics in 42 patients with multiple myeloma ( * age at the time of diagnosis ; * * karnofsky performance index at the time of the different courses of radiotherapy ; n = 59 , because 17 patients were irradiated twice and 3 times at different times , respectively )  . zwlf bis 90 monate spter . 
zustzlich war die indikation gegeben bei drohenden frakturen ( 18 zielvolumina ) , bei frakturkonsolidierungen ohne operative stabilisierung ( 17 zielvolumina , berwiegend im bereich der wirbelsule ) , bei postoperativer stabilisierung ( zehn zielvolumina ) sowie bei neurologischer symptomatik bei myelonkompression ( 13 zielvolumina )  . 
um den vergleich mit literaturdaten zu ermglichen , haben wir die daten bezglich der schmerzen sowie der rekalzifizierung zielvolumenund nicht patientenbezogen ausgewertet . ergebnisse analgetischer effekt im gesamten verlauf der mindestens sechsmonatigen nachbeobachtungszeit zeigte sich eine analgesie in 85% der zielvolumina ( 57 / 67 ) ( komplett 34 , 3% , partiell 50 , 7% )  . 
eine simultan zur radiotherapie durchgefhrte chemotherapie erwies sich dagegen als signifikanter einflussfaktor fr das erreichen des analgetischen effekts , der in 26 / 27 zielvolumina ( 96 , 3% ) dokumentiert wurde , verglichen mit 77 , 5% ( 31 / 40 zielvolumina ) in nur strahlentherapierten regionen ( p < 0 , 05 )  . 
dagegen kam es bei patienten mit einem karnofsky - index 70 bis 90 zu einer signifikant besseren remineralisation ( 50 , 0 bis 68 , 4% ) als bei einem karnofsky - index 40 bis 60 ( 0 bis 18 , 2% ) ( p < 0 , 005 )  . 
auffllig war jedoch , dass die rekalzifizierung in den auswertungszeitpunkt whrend bei rtende nach 6 wo nach 3 mo nach 6 mo auswertbare zv schmerzfreiheit schmerzlinderung ansprechrate ( % ) progress rezidiv fehlerrate ( % ) 33 ( 49 , 3 ) 34 ( 50 , 7 ) 53 ( 79 , 1 ) 14 ( 20 , 9 ) 52 ( 85 , 2 ) 9 ( 14 , 7 ) nicht auswertbare zv 0 44 ( 80 , 0 ) 11 ( 20 , 0 ) 39 ( 88 , 6 ) 5 ( 11 , 4 ) nach initialem therapieerfolg nc rezidiv progress tabelle 4 . 
ebenfalls von relevanz war die simultane chemotherapie : 18 / 24 zielvolumina ( 75 , 0% ) rekalzifizierten im vergleich zu 8 / 32 regionen nach alleiniger radiotherapie ( 25 , 0% ) ( p < 0 , 0005 )  . 
die rekalzifizierung war bei frakturgefhrdeten lsionen deutlicher ( 9 / 18 zielvolumina ) als bei bereits frakturierten knochen ( 5 / 17 zielvolumina ) , bei denen nur in kombination mit einer operation eine vergleichbare rekalzifizierung induziert werden konnte ( 4 / 8 zielvolumina )  . 
 effekt auf die myelonkompression bei 7 / 13 patienten ( 53 , 8% ) mit einer neurologischen symptomatik aufgrund einer myelonkompression kam es zu einer remission der beschwerden ( n = 2 mit kompletter , n = 5 mit partieller remission )  . 
nur bei 4% der therapien wurden grad - iii - toxizitten festgestellt ( mukositis , blutbildvernderung , kreatininanstieg )  . eine wesentliche erhhung der nebenwirkungen unter simultaner chemotherapie wurde nicht registriert . daten zur nachbeobachtung 17 patienten verstarben innerhalb der sechsmonatigen postradiotherapeutischen nachbeobachtungszeit . 
 diskussion natrlich beeinflusst die retrospektivitt dieser arbeit ihre aussagekraft , noch dazu wenn die patientenrekrutierung bei einer seltenen erkrankung 1% aller malignen , 10% aller hmatologischen neoplasien [ 2 ] einen zeitraum von zehn jahren erfasst . 
auch ist es retrospektiv schwierig , den analgetischen effekt korrekt zu quantifizieren und die rekalzifizierung mittels konventioneller rntgenbilder , wie sie in der klinischen routine blicherweise innerhalb der ersten drei bis sechs monate nach beendigung der radiotherapie ossrer lsionen aufgenommen werden , zu beurteilen . 
andererseits liegen von radiotherapeutischer seite wenige aktuelle arbeiten vor , die sich gezielt mit den fragen der radiogen induzierten analgesie ( tabelle 5 ) , der rekalzifizierung und der reduktion neurologischer defizite bei patienten mit einem multiplen myelom beschftigen . 
unser patientenkollektiv , das hinsichtlich der patientenund tumorcharakteristika und der lokalisation der zielvolumina im wesentlichen den angaben in den bisherigen verffentlichungen [ 1 , 7 , 13 , 16 , 1921 , 24 , 30 ] entspricht , ermglichte uns trotz der genannten methodischen probleme eine diesbezgliche untersuchung . 
 analgetischer effekt die alleinige chemotherapie ist insbesondere auch im rahmen einer rezidivtherapie nur unzureichend in der lage , eine ossre schmerzsymptomatik zu lindern [ 7 , 16 , 19 ]  . 
dieser kann nach literaturangaben bereits nach einer dosis von 10 bis 20 gy erreicht werden [ 16 ] ; vergleichbar ist aus der radiotherapeutischen behandlung ossrer metastasen bei soliden tumoren bekannt , dass hypofraktionierte , niedrig dosierte schemata ( zum beispiel 1 - mal 8 gy , 4 - mal 4 gy , 4 - mal 5 gy ) zu einer adquaten schmerzlinderung fhren [ 8 , 12 , 14 , 15 ]  . 
nach durchsicht der literatur ist uns jedoch auch keine publikation bekannt geworden , die untersucht , ob eine kombinierte bisphosphonat - radiotherapie erwartungsgem zu einer verbesserung des lokalen bestrahlungseffektes fhrt . 
 rekalzifizierung zur rekalzifizierung bei multiplem myelom wurde gem unserer literaturdurchsicht nur eine arbeit publiziert , in der eine zu unseren daten vergleichbare ansprechrate von 51% angegeben wurde [ 22 ]  . 
die rekalzifizierungsrate bei ossren metastasen solider tumoren liegt zwischen 11 und 77% [ 25 , 29 ] ; dieser effekt ist , wie die prospektive arbeit von koswig et al . 
 abweichend von literaturdaten [ 25 ] zeigte sich bei uns ein schlechtes ansprechen in der wirbelsule ; dies kann mglicherweise durch den recht hohen anteil ( 41% ) an frakturierten wirbelkrpern und somit durch eine negativselektion bei einer kleinen patientenzahl erklrt werden . 
im falle der postoperativen situation ist zur stabilisierung des befundes die bestrahlung ebenfalls angezeigt [ 27 ]  . effekt auf die myelonkompression die inzidenz von 31% ( 13 / 42 patienten ) mit einer myelonkompression ist im vergleich zu literaturdaten mit ca . 
bereinstimmung zeigt sich jedoch hinsichtlich des zusammenhangs zwischen reduktion des neurologischen defizits und der berlebensrate [ 28 ]  . nachbeobachtung die in unserem patientengut beschriebene mediane berlebenszeit von 34 , 9 monaten entspricht den in der literatur verfgbaren angaben unter standardchemotherapie ( 27 bis 35 monate )  . 
neben den bekannten prognosekriterien ( ausma der knochenmarksinfiltration , anmie , m - gradient ) knnen inzwischen weitere tumorspezifische parameter ( ( cid : 2 ) 2 - mikroglobulin , plasmazell - labeling - index ) als etabliert angesehen werden [ 18 ]  . 
unzweifelhaft ist allerdings , dass das ansprechen auf die chemotherapie einen erheblichen einfluss auf das berleben nimmt , whrend ein verzgerter chemotherapiebeginn das behandlungsresultat nicht negativ beeintrchtigt [ 10 , 17 , 18 ]  . 
the present study examines the use of various media and , in particular , the application of the internet , in a mixed cohort of radiotherapy patients . patients and methods : all patients undergoing radiotherapy at the university of wrzburg were analyzed simultaneously in may of 2000 using a newly developed 9 - item questionnaire . 
the rates of internet use were substantially higher in subgroups with younger age , higher education and palliative treatment . conclusion : the importance of the medium internet for the information of tumor patients is currently still low but likely to increase based on demographic factors . 
 key words : internet radiotherapy patient education media das internet als quelle medizinischer informationen : untersuchung an einem gemischten kollektiv von strahlentherapiepatienten hintergrund : die verbreitung des internets hat die informationsmuster fr tumorpatienten verndert . 
die vorliegende studie untersucht die nutzung verschiedener medien und insbesondere die anwendung des internets an einem gemischten kollektiv von strahlentherapiepatienten . patienten und methoden : alle patienten , die sich im mai 2000 an der wrzburger strahlentherapieklinik in behandlung befanden , wurden um die beantwortung eines neun - punkte - fragebogens gebeten . 
die fragen bezogen sich auf die bewertung verschiedener medien zur informationsgewinnung ber die jeweilige tumorerkrankung ( von 0 = unwichtig bis 2 = sehr wichtig ) und die bisherige internetnutzung . ergebnisse : fr 95% der patienten ( n = 139 ) waren fragebgen auswertbar . 
unter acht medien wurden fernsehen ( mittelwert 0 , 94 ) , patientenbroschre ( 0 , 83 ) und tageszeitung als fr medizinische informationen am wichtigsten genannt , whrend das internet ( 0 , 24 ) an letzter stelle lag . 
61 , 2% kannten das internet als medizinische informationsquelle , aber nur 11 , 5% hatten selbst im internet nach medizinischen informationen gesucht , und 15 , 1% hatten solche informationen ber bekannte oder verwandte erhalten . 
internet use by radiotherapy patients t he widespread application of the internet in recent years has had a tremendous effect not only on the commercial but also on the medical sector . 
current papers investigate the credibility of patient information available in the internet [ 1 , 7 , 11 ] or cover the structure of internet patient support groups [ 5 , 6 ]  . 
a single report on patients internet use at the pediatric department of harvard medical school in boston ( usa ) in 1999 found a total internet access of 73% and a significant correlation with family income [ 9 ]  . 
the number of internet users in germany is not comparable to american data and only average even on a european scale : in 1999 10% of the population were reported to have internet access as compared to 32 to 41% in denmark , finland and sweden [ 4 ]  . 
 data on the actual use of the internet by tumor patients may be of interest for 2 reasons : while such information may help to evaluate the acceptance of established patient information services , it is also useful for the individual physician to know patterns of information acquisition applied by his patients . 
in the present study , a mixed cohort of tumor patients was therefore investigated concerning the importance of various media as sources of medical information and , in particular , the current use of the internet for that purpose . patients and methods on a single day in may of 2000 , all patients currently undergoing treatment at the department of radiation oncology of the university of wrzburg were asked to complete a newly developed questionnaire ( see table 2 )  . 
in 9 questions data was collected on the use of the internet as a source of medical information , the main points of interest , the importance of various media and the patients education . 
demographic and clinical data on the subgroup of patients who have received medical information from the internet by searching the internet themselves or with the help of family or friends ( question 4 : yes or question 5 : yes ) is given in table 1 . in a further analysis subgroups of patients were analyzed . the grading of different sources of medical information varied depending on formal school education . 
while patients with basic education ( hauptschulabschluss ) rated television ( mean score 0.96 ) , patient brochures ( 0.84 ) and daily newspaper ( 0.8 ) as most important in this order , patients with higher education assigned television ( 0.91 ) and medical books ( 0.84 ) the greatest importance . 
anteile von patienten , die ber das internet ( durch eigene suche oder ber verwandte / bekannte ) informationen zu ihrer tumorerkrankung erhalten haben . discussion in the age of informed consent a clear and honest patient information on the perspective and side effects of a tumor treatment is a duty of every physician . 
the often life - threatening situation of the tumor patient and the severity of treatment consequences ( resection of organs , permanent impairment of organ function after chemoor radiotherapy ) justifies the patients desire for additional information . 
previous studies in radiotherapy patients have documented both a need for more contact with fellow patients [ 8 ] and efforts to obtain further information about the treatment [ 10 ]  . 
apart from the abundance of information of varying credibility in the conventional media ( television , newspaper , magazines ) , the internet represents an additional source of international information for tumor patients . 
 in the present study , the importance of the medium internet as a patient information source and the structure of patients internet use has been documented for the first time , based on questionnaires handed out to patients of a university radiation oncology department . 
whereas only 1 out of 9 patients has searched the internet for medical information on his own and about 20% have received such data directly or indirectly , the proportion of internet users was markedly higher in subgroups . 
young age and higher education in particular were associated with higher rates of internet application . interestingly , internet use was also high in patients treated with palliative intent a finding also reflected by the high rate in the diagnosis group bone metastasis . 
the low rate of internet use among patients with ent tumors is likely to be associated with the known risk factors for these diseases ( alcohol , smoking ) and low socioeconomic status . 
internet use by radiotherapy patients demographic data available from the internet on the use of the medium in germany has documented a majority of users with higher education but an increasing percentage of users with basic education [ 3 ]  . 
there appears to be little strahlentherapie und onkologie urban & vogel 2000 originalarbeit prognostic value of hemoglobin concentrations in patients with advanced head and neck cancer treated with combined radio - chemotherapy and surgery wolfgang wagner1 , robert hermann1 , joachim hartlapp2 , elmar esser3 , bernhard christoph5 , michael karl mller6 , rainer krech4 , olaf koch1 purpose : hemoglobin levels are currently the focus of interest as prognostic factors in patients with head and neck cancer . 
the therapy comprised 2 courses of induction chemotherapy with ifosfamide ( 1 , 500 mg / m2 , day 1 to 5 ) and cisplatin ( 60 mg / m2 , day 5 ) followed by hyperfractionated accelerated radiotherapy with a total dose of only 30 gy . surgery involved tumor resection and neck dissection . results : the 1 - year overall survival rate and the 2 - year survival rate were 79% and 56% , respectively . 
relapsing disease could be treated with 1 additional course of radiotherapy which is supposed to be well tolerated . key words : locally advanced head and neck cancer neoadjuvant combined radio - chemotherapy prognostic factors hemoglobin concentrations hmoglobinkonzentrationen als prognosefaktor bei patienten mit fortgeschrittenen kopf - hals - tumoren , die kombiniert radiochemotherapiert und anschlieend operiert wurden hintergrund : hmoglobinkonzentrationen sind in der letzten zeit , insbesondere bei patienten mit kopf - hals - tumoren , als prognosefaktor in den mittelpunkt des interesses gerckt . 
in unserer studie haben wir den einflu des hmoglobins in einem multimodalen regime getestet . patienten und methoden : 43 patienten mit fortgeschrittenen kopf - hals - tumoren wurden mit kombinierter radiochemotherapie behandelt . 
die therapie bestand aus zwei induktionskursen mit ifosfamid ( 1 500 mg / m2 , tag 1 bis 5 ) und cisplatin ( 60 mg / m2 , tag 5 ) , gefolgt von einer hyperfraktioniert akzelerierten radiatio mit einer gesamtherddosis von nur 30 gy . 
hemoglobin levels in head and neck cancer patients schlufolgerung : in unserer studie besa hmoglobin einen signifikanten prognostischen einflu auf das berleben bei patienten mit kopf - hals - tumoren , die einer kombinierten radiochemotherapie unterzogen wurden ( univariate analyse )  . 
im falle eines rezidivs knnte dem patienten noch ein voller kurs reiner strahlentherapie zugemutet werden . schlsselwrter : fortgeschrittene kopf - hals - tumoren kombinierte neoadjuvante radiochemotherapie prognosefaktoren hmoglobinkonzentration l ocally advanced carcinomas of the head and neck had been treated in the past by radical extirpation followed by adjuvant radiotherapy with total doses of about 60 gy . 
 recently , combined radio - chemotherapy or neoadjuvant combined radio - chemotherapy followed by surgery had been able to improve overall survival and locoregional disease control [ 1 , 2 , 11 , 24 , 31 , 37 ]  . 
hemoglobin levels are currently the focus of interest as a prognostic factor in patients with head and neck cancer [ 4 , 5 , 8 , 12 , 15 , 34 ]  . there is no doubt that hypoxic tumor areas are clinically relevant obstacles to a successful therapeutic outcome in radiosensitive malignancies [ 17 , 19 , 29 , 32 ]  . 
in addition to this , a loss of p53 and overexpression of the apoptosis inhibiting bcl2 were both detected in hypoxic cells and are believed to contribute indirectly to therapeutic resistance [ 17 ]  . the question whether or not hypoxia is influenced significantly by peripheral hemoglobin levels is not answered definitely yet . 
several investigators , however , found an improved therapeutic outcome in different epithelial cancers in patients with sufficiently high hemoglobin ( hb ) levels compared to those with anemia ; the normal reference values for anemia are defined as approximately 12 g / dl [ 6 ]  . 
statisticallly , hemoglobin levels showed to be an independent prognostic factor . a promising approach would be to start investigations on the issue of treating anemia before radiation or correcting it during therapy and by that improving tumor oxygenation and sensitivity to radiation . 
 rhuepo has been shown to elevate hemoglobin levels in tumor patients [ 9 , 10 , 35 ]  . in the present study we investigated whether different hemoglobin concentrations have a significant influence on local tumor control and survival in radio - chemotherapy of locally advanced head and neck cancer . 
the regimen comprised radiation ( total dose 30 gy ) in combination with chemotherapeutic treatment with ifosfamide and cisplatin . good experiences had been made using the substances cisplatin and 5 - fu . 
although up to now the best chemotherapeutic agents and combinations and the optimal rate to integrate chemotherapy with irradiation are still not defined [ 1 ]  . ifosfamid has a well known influence on remission rate in patients with head and neck cancer and there are some informations that the impact on survival is not minor than in comparison to 5 - fu [ 20 , 24 , 36 ]  . patients , materials and methods between 1 jan 1995 and 9 aug 1996 we included 43 patients with biopsy - proven advanced head and neck cancers to receive a neoadjuvant radio - chemotherapy with ifosfamide and cisplatthe inclusion criteria were defined as follows : < 75 years of age , karnofsky performance status > 60% , tumor stage iv as defined by the american joint committee ( t24 ; n03 ; m0 ) and tumor localization : hypopharynx , pharynx , or oral cavity . after obtaining a biopsy specimen the borders of the tumor area were marked with ink . the chemotherapy schedule consisted of : 2 cycles of ifosfamide ( 1 , 500 mg / m2 , day 1 to 5 and day 22 to mesna ( 300 mg / m2 , day 1 to 5 and day 22 to 26 ) , 2 cycles of cisplatin ( 60 mg / m2 , day 5 and 26 ) followed by hyperfractioned accelerated radiotherapy . chemotherapy 26 ) , radiotherapy the total dosage of 30 gy was given over 2 weeks . 
treatment fields were adapted to the maximum extension of the primary tumor and cervical node extension , as assessed during the initial clinical , endoscopic and radiological ( sonography , computed tomography and magnetic resonance imaging ) evaluation , including a safety distance . 
in most cases the maximum tumor size was represented by tumor extension before the first chemotherapeutic cycle , in the case of progression during therapy it was represented by postchemotherapeutic tumor extension . 
after surgery in the case of a non - r0 resection the irradiation dose was boosted up to a total dose of 60 gy in conventional fractionation ( with single doses of 1 , 8 gy )  . diagnosis surgery tumor surgery was carried out at day 52 in median ( range 43 to 64 ) either by radical resection of the primary tumor and conventional neck dissection of the nodes , as was the case in 30 patients , or by simple laser resection and conventional neck dissection of the nodes . 
radical resection was defined as resection in sano with a safety distance of 1 c safety distance was reduced for the mandibula . surgery of the oral cavity and the oropharynx was performed as en bloc resection involving the neighboring lymph node drainage area . 
tumors with median location or involving midline structures were resected bilaterally . hemoglobin levels hemoglobin concentrations were determined before therapy , on days 10 to 14 , after 2nd chemotherapeutic cycle and before surgery . 
the normal reference values for hemoglobin in our hospital are 14 to 18 g / dl for males and 12 to 16 g / dl for females . disease - free and overall survival were estimated on the basis of the product limit method of kaplan - meier . 
the logrank test was used to compare survival curves between subgroups . p - values are given explicitly without adjustment of type i error and without reference to any specific level of significance . prognostic factors were tested during univariate analysis and within subgroups . results demographic data a total of 43 patients with locally advanced head and neck cancer underwent therapy . 
data of all patients were documented and evaluated . forty - one patients ( 95% ) were male , 2 were female ( 5% )  . the median age was 55 years ( range 41 to 69 years )  . 
the median follow - up time is 756 days . almost all patients suffered from advanced t3 or t4 head and neck carcinomas ( n = 42 , 98% ) , respectively with extensive involvement of the lymph nodes ( n2b or n2c ) ( n = 37 , 86% )  . 
in accordance with the definition of the american joint committee all patients were allocated to stage iv ( table 1 )  . the majority of patients suffered from advanced oropharyngeal and hypopharyngeal carcinomas . 
half of the tumors were located unilaterally ( n = 21 , 49% ) , 19 ( 44% ) extended beyond the midline and 3 ( 7% ) had a median location . 
below our normal laboratory reference values for males . response criteria response was assessed from macroscopic and microscopic criteria : complete remission ( cr ) : no residual tumor mass detectable by diagnostic imaging procedures ; partial remission ( pr ) : measurable tumor mass reduced by no change ( nc ) : measurable tumor mass reduced by less more than 50% ; than 50% ; table 1 . 
we found the diagnosis of relapsing tumor by imaging procedures in an area pretreated by radiation and surgery to be not reliable . oral cavity nasopharynx oropharynx hypopharynx 15 ( 35% ) 1 ( 2% ) 23 ( 53% ) 30 ( 70% ) table 2 . 
two patients suffered from fever of unknown origin . anemia was recorded in 25 patients and was mild to moderate in 19 patients ( 76% ) ( 7 patients grade i , 12 patients grade ii )  . 
in 3 cases the postoperative irradiation dose of the neck had to be increased because tumor involvement was found in resected lymph nodes . after chemotherapy half of all patients were in partial remission ( based on ct - imaging findings )  . the tumor response to the combined radio - chemotherapy was examined by means of ct and sonographic imaging ( n = 31 ) and by histological examination of the resected material ( n = 42 )  . three patients achieved complete remission without retraceable tumors on ct - imaging , partial remission was seen in 18 patients ( table 5 )  . 
in 26 patients we achieved a so - called r0 resection , in 10 patients we documented an r1 situation and in 6 patients macroscopic residual tumor had been documented postoperatively ( r2 resection )  . 
histological examination showed complete remission in 16 patients ( 38% ) and partial remission in 8 patients ( 19% )  . following tumor resection we found complete tumor necrosis at the primary site in 48% and necrosis of the nodes in 50% ( n = 42 ) ( table 6 )  . overall survival and recurrence - free survival the 1 - year survival rate ( beginning with the time of diagnosis ) was 79% , the 2 - year survival rate 56% . 
thus far , we have not seen any severe late sequelae such as xerostomia , fibrosis of the tissue , lymph edema or osteoradionecrosis as frequently observed after high - dose 60 to 70 gy irradiation . the median observation period ( from diagnosis to last consultation or to death ) was 756 days ranging between 91 ( died ) to 1 , 238 days . prognostic factors side effects non - hematologic toxicity : nausea and emesis were mild to moderate : more than 50% ( 23 ) showed no gastrointestinal symptoms ( 6 patients with grade iii , none with grade iv , according to who classification )  . 
table 7 summarizes the patients and tumor criteria in correlation to the low vs high hemoglobin group . table 8 documents the result of therapy in correlation to the low vs high hemoglobin group . in our patients we found a significant influence of posttherapeutic hemoglobin levels on recurrence - free survival after combined radio - chemotherapy . 
patients with posttherapeutic hemoglobin levels of less than 11.5 g / dl ( n = 20 ) had a significantly poorer outcome than patients with hemoglobin concentrations of more than 11.5 g / dl ( n = 22 , p = 0.0084 ) ( figure 2 )  . 
posttherapeutic hemoglobin levels had been measured at day 8 ( median ) after surgery ( range day 3 to day 14 )  . subgroup analysis showed that patients with t3 tumor and hemoglobin levels of more than 11.5 g / dl ( n = 12 ) in particular will benefit with respect to the outcome of therapy ( figure 3 )  . 
the decrease of the hemoglobin concentration during therapy ( < 2 , 5 g / dl vs > 2 , 5 g / dl ) had not influenced survival significantly ( figure 4 )  . criterion response tumor ( n = 31 ) ( clinical ) response nodes ( n = 41 ) ( clinical ) response tumor ( n = 41 ) ( pathological ) response nodes ( n = 41 ) ( pathological ) recurrence - free survival * after 1 year after 2 years overall survival * after 1 year after 2 years hb postth . 
therapieergebnisse in relation zum posttherapeutischen hmoglobinwert . in our evaluation we have not found any significance in outcome between overall survival / recurrence - free survival and decrease of hemoglobin concentration during therapy . besides we have not documented any significance in outcome between overall survival / recurrence - free survival and decrease of hemoglobin levels in correlation to the nadir . comparison of preand posttherapeutic hemoglobin concentrations ( figure 5 ) showed an average decrease of 2.75 g / dl with a standard deviation of 1.4 and a median of 2.55. 
ausgangskriterien in relation zum posttherapeutischen hmoglobinwert . criterion age ( n = 42 ) average median range criterion category sex ( n = 42 ) male female oral cavity site of the primary tumor nasopharynx oropharynx ( n = 42 ) hypopharynx no exceeding exceeding median localization middle line t - stage ( n = 42 ) n - stage ( n = 42 ) grading ( n = 41 ) t3 / 11.5 g / dl ( n = 12 ) t3 / < 11.5 g / dl ( n = 6 ) < 11.5 g / dl ( n = 20 ) logrank test : p = 0.0084 t4 / < 11.5 g / dl ( n = 14 ) logrank test ( strat . ) : p = 0.18 1000 1200 1000 1200 time [ days ] time [ days ] figure 2 . 
however , a tendency to improved local control can be seen for those patients , who can be transferred to an operable tumor stage ( reviewed in [ 30 ] )  . 
in our regimen even manifested relapses could be successfully treated with another 60 or 70 gy after low - dose radiotherapy and will allow a second chance of a definitive cure . similar results were reported by mohr et al . 
hemoglobin levels in head and neck cancer patients hb - levels decrease 2.5 g / dl ( n = 21 ) decrease > 2.5 g / dl ( n = 21 ) logrank test : p = 0.12 1000 1200 time [ days ] figure 4 . 
beziehung zwischen unterschiedlichen verminderungen des hmoglobinwertes und dem rezidivfreien berleben . thus far , the influence of prognostic factors on local control and survival including tumor stage , tumor differentiation , patients gender and age , tobacco pack - years , hemoglobin levels , treatment duration , total dose and fractionation , has in part not been adequately defined . in our report , stage was of prognostic value , too , whereas tumor localization did not appear to influence the outcome . recently , tumor oxygenation status , hypoxia ( and hence hemoglobin rates ) in patients with epithelial , radiosensitive carcinomas has been the focus of interest with respect to outcome of therapy and rate of local failures . 
the existence of hypoxic tumor areas , with respect to the fraction of po2 values less than 2.5 mm hg , was associated with a poorer local control probability . the correlation between hemoglobin level and local tumor control during irradiation therapy in 25 published clinical trials was reviewed by dische [ 7 ]  . 
the hemoglobin level was a significant predictor of local tumor control in 23 studies involving patients with cancers of the uterine cervix , head and neck , lung or bladder . 
 [ 18 ] reported that the majority of 51 trials showed a correlation between hemoglobin concentration and treatment outcome in patients with several epithelial malignancies . in a number of studies multivariate analysis was used to separate the effect of hemoglobin level from other patient , tumor or treatment - related factors that might have influenced tumor control . 
consistent with previous investigations ( reviewed in [ 23 ] ) , we found posttherapeutic hemoglobin concentrations to be of prognostic value . it is , however , still necessary to confirm our results by evaluating the data obtained in a larger number of patients by means of multivariate analysis . hence , we felt , that when multivariate analysis is not possible , the best way to improve a univariate analysis is to practice a further subgroup analysis . 
in this subgroup analysis we have found that higher hemoglobin concentrations are of benefit to patients with t3 tumor in particular , and we believe that our data furnish evidence that the hemoglobin level is an independent prognostic factor . the strong apparent correlation between hemoglobin level , local control and survival for a variety of tumors support consideration of correcting anemia respective preventing of anemia before initiation of radiation therapy . 
this may prove more important as clinical trials increasingly use intensive induction chemotherapy in the treatment of head and neck carcinomas and other malignancies possibly inducing severe anemia . in the past some investigators have therefore suggested to improve hemoglobin concentration by blood transfusions before and during radiotherapy . 
in recent reports it could be shown that correction of anemia by erythropoietin in patients with carcinomas of the head and neck reduced the need for blood transfusions [ 10 ] and increased the efficacy of a neoadjuvant radio - chemotherapy significantly [ 16 ]  . in combined radio - chemotherapy , neoadjuvant chemotherapy may cause myelosuppression and hence anemia , which in thus far , a lot of clinical trials have confirmed hemoglobin level to be of significant influence in patients with head and neck cancer who underwent radiotherapy . 
in our study we were able to show for the first time that hemoglobin possesses a significant influence in head and neck cancer patients who underwent combined treatment modality ( preoperative chemotherapy plus irradiation ) , too . 
results must be confirmed in an ongoing placebo - controlled phaseiii study . strahlentherapie und onkologie urban & vogel 2000 originalarbeit effect and toxicity of endoluminal high - dose - rate ( hdr ) brachytherapy in centrally located tumors of the upper respiratory tract wolfgang harms1 , peter schraube2 , heinrich becker3 , detlev latz4 , felix herth3 , peter fritz5 , michael wannenmacher1 aim : to assess effect and toxicity of high - dose - rate afterloading ( hdr ) alone or in combination with external beam radiotherapy ( ebrt ) in centrally located tumors of the upper respiratory tract . patients and methods : from 1987 to 1996 , 55 patients were treated . 
twenty - one patients ( group a1 : 17 non - small - cell lung cancer [ nsclc ] , a2 : 4 metastases from other malignancies ) were treated using hdr alone due to a relapse after external beam irradiation . 
in 34 previously untreated and inoperable patients ( group b1 : 27 nsclc , b2 : 7 metastases from other malignancies ) hdr was given as a boost after ebrt ( 30 to 60 gy , median 50 )  . 
the brachytherapy dose ( group a : 5 to 27 gy , median 20 ; b : 10 to 20 gy , median 15 ) was prescribed to 1 cm distance from the source axis . 
a distanciable applicator was used in 39 / 55 patients . results : in group a1 , a response rate ( cr , pr ) of 53% ( group b1 : 77% ) was reached . 
prognostic favorable factors in group b1 were a tumor diameter < 20 mm , the lack of radiological mediastinal involvement , a complete remission , and a karnofsky performance status > 70 . 
complications caused by persistent or progressive local disease occurred in 3 patients in group a ( fatal hemorrhage , tracheomediastinal fistula , hemoptysis ) and in 2 patients in group b ( fatal hemorrhage , hemoptysis )  . conclusions : hdr brachytherapy is an effective treatment with moderate side effects . 
in combination with external beam irradiation long - term remissions can be reached in one third of the patients . key words : hdr brachytherapy malignant stenosis lung cancer effektivitt und toxizitt der endoluminalen high - dose - rate - ( hdr - ) brachytherapie bei zentral lokalisierten tumoren der oberen atemwege ziel : evaluierung von effektivitt und toxizitt der endoluminalen high - dose - rate - ( hdr - ) brachytherapie als alleinige oder kombinierte ( ebrt ) therapie bei zentral sitzenden tumoren der oberen atemwege . patienten und methode : von 1987 bis 1996 wurden 55 patienten behandelt . 
21 patienten ( gruppe a1 : 17 patienten mit nichtkleinzelligem bronchialkarzinom [ nsclc ] , a2 : vier patienten mit metastasen anderer tumoren ) wurden bei lokalrezidiven nach vorheriger perkutaner bestrahlung ausschlielich endoluminal bestrahlt . 
bei 34 inoperablen und vorher unbehandelten patienten ( gruppe b1 : 27 nsclc , b2 : sieben metastasen anderer tumoren ) wurde die brachytheranie als boost nach externer bestrahlung ( 30 bis 60 gy , median 50 ) appliziert . 
ein distanzierbarer spreizkorbapplikator wurde bei 39 / 55 patienten verwendet . ergebnisse : in gruppe a1 wurde ein therapieansprechen ( cr , pr ) in 53% erzielt ( gruppe b1 : 77% )  . 
als prognostisch gnstige faktoren konnten in gruppe b1 ein tumordurchmesser < 20 mm , radiologisch fehlende mediastinale beteiligung , eine komplette remission und ein karnofsky - index > 70 ermittelt werden . 
tumorassoziierte komplikationen kamen in drei fllen in gruppe a ( blutung , tracheomediastinale fistelung , hmoptysen ) und in zwei fllen in gruppe b vor ( blutung , hmoptysen )  . schlufolgerungen : die endoluminale hdr - brachytherapie ist eine effektive therapie mit moderaten nebenwirkungen . 
in kombination mit externer radiotherapie knnen langzeitremissionen bei einem drittel der patienten erzielt werden . schlsselwrter : hdr - brachytherapie maligne stenose bronchialkarzinom o ne of the most distressing symptoms for lung cancer patients is airway obstruction due to the tumor , commonly resulting in dyspnea , postobstructive pneumonia , cough , or hemoptysis . 
besides of the resection in patients suitable for surgery there are several possibilities of recanalization [ 1 , 17 ] : mechanical removement , electrocoagulation , cryosurgery , photodynamic therapy , external and / or endoluminal irradiation . 
to treat sufficiently more distant parts of the tumor volume or regions of subclinical disease it has to be combined with external beam radiotherapy . therefore only in patients with relapsing tumors after prior irradiation or other contraindications to external radiotherapy the regimen should be restricted to a sole endoluminal treatment . 
this retrospective study investigates effect and toxicity of high - dose - rate ( hdr ) brachytherapy as a single or combined ( ebrt ) treatment in a patient series treated by this regimen . patients and methods from 1987 to 1996 , 55 patients ( 15 women , 40 men ) were treated . 
the patients ( mean age : 62 years , range : 36 to 78 ) were divided by treatment intention and histology into 2 groups with 2 subgroups each ( table 1 )  . 
for the second group ( b ) inoperable and previously untreated patients with tumors confined to the bronchial or tracheal wall with a maximum periluminal tumor extension of 3 cm were selected . 
eleven patients had a history of a recent laser vaporization and 2 patients had a stent implantation . in group b , radiotherapy was started by teletherapy with the exception of 2 cases , where an alternating schedule was chosen . 
in the recent history of the 34 patients of group b were 21 laser vaporizations , 3 surgical resections ( microscopically incomplete ) , and 1 stent placement . metastases from colon cancer 2 , hypernephroma 1 , esophageal cancer 1 metastases from hypernephroma 2 , colon cancer 1 , cervical cancer 1 , uterine cancer 1 , esophageal cancer 1 , thyroid cancer 1 table 1 . 
verteilung der tnm - stadien in gruppe b1 ( n = 27 patienten )  . radiotherapeutic technique external beam radiotherapy : as far as patients were treated by external beam irradiation ( group b ) megavoltage equipment was used . 
after computerized treatment planning , therapy was continued to a median dose of 50 ( 30 to 60 ) gy by a 2or 3 - field technique sparing the spinal cord . 
the single dose was 2 gy / fraction ( 1 exception with 2.5 gy ) 5 times a week . endoluminal radiotherapy : endobronchial and tracheal irradiation was performed after local anesthesia and sedation with midazolathe applicator tube , loaded with a ribbon of dummy seeds was positioned under endoscopical and fluoroscopical control . 
in 2 cases ( group a ) a reduction of single doses ( 9 times 3 gy ) was necessary , due to tumor ulcerations in the bronchial mucosa . standard treatment in group b consisted of 50 gy external beam radiotherapy and 3 to 4 times 5 gy hdr brachytherapy . 3 / 17 ( 18 ) ( 25 ) 19 / 27 ( 70 ) ( 14 ) 6 / 17 ( 35 ) 2 / 27 ( 29 ) 4 / 17 ( 24 ) ( 25 ) 3 / 27 ( 11 ) ( 14 ) the patient collective consisted of different histologies and treatment policies , thus the results are reported in 2 ways : therapeutic results in terms of remission for each group ( a1 , 2 ; b1 , 2 )  . 
the most common cause of death was local progression with poststenotic complications in 16 patients , metastases of the disease in 14 cases , and combined local and distant progression in 7 patients . 
the cause of death in the remaining patients is not known . in 23 / 27 patients of group b1 ct scans of the thorax were done before and after external radiotherapy . 
three patients had no control endoscopy . the median local progression free survival ( figure 1 ) estimated by the kaplan - meier method [ 13 ] , was 5 months in group a1 ( 15% 1 - year local progression free survival ) and 40 months in group b1 ( 66% 1 - year , 52% 3 - year , 37% 5 - year )  . the median overall survival was 5 months in group a1 ( 20 months , group b1 )  . 
an excellent result was defined as no clinical symptoms , a good result as minor symptoms of disease . a univariate analysis of factors influencing survival in the group b1 by the log rank test [ 24 ] showed a positive influence of a karnofsky performance status > 70 [ 14 ] , a diameter of the primary tumor < 20 mm , a lack of radiological progressive disease ( % ) 3 / 17 ( 18 ) ( 50 ) 2 / 27 ( 29 ) 1 / 17 1 / 27 ( 14 ) table 3 . 
local progression free surival ( kaplan - meier ) for group a1 ( hdr brachytherapy for recurrent nsclc after external beam irradiation ) and group b1 ( hdr brachytherapy as a boost after external beam irradiation for nsclc )  . 
lokalrezidivfreies berleben nach kaplan - meier in gruppe a1 ( hdr - brachytherapie bei rezidivierendem nichtkleinzelligen bronchialkarzinom [ nsclc ] nach externer radiotherapie ) und gruppe b1 ( hdr - brachytherapie als boost nach externer radiotherapie bei nsclc )  . 
there was no relation between survival and treatment related factors within the used dose range . adverse events the groups a and b were treated uniformly , so it seems to be justified to report the adverse effects for each group , in spite of the different histologies in the subgroups . 
there were no acute side effects during the bronchoscopy and catheter positioning . three patients in group a ( n = 21 ) presented with complications caused by persistent or progressive local disease . 
bronchoscopy confirmed , that the destruction of the bronchial wall was caused by a local recurrence located within the boosted area . a third patient with persistent local tumor after treatment with 52 gy external beam and 4 times 5 gy hdr therapy suffered from hemoptysis requiring no transfusion . 
two locally controlled patients presented with a radiogenic bronchitis ( rtog / eortc , grade 2 ) 28 and 48 months after treatment with 50 gy external beam and 3 ( 2 ) times 5 gy hdr therapy . 
although a differentiation between treatment and tumor related effects is difficult , it seems to be more likely that except for the 2 patients with the radiogenic bronchitis all of the remaining events were caused by tumor progression . 
adverse events could not be related to irradiation parameters in the used range . discussion in the situation of malignant obstruction of the airways endoscopical intervention provides immediate relief of symptoms . 
due to tumor reduction after external beam treatment the following endoluminal boost irradiation encompassed a relatively higher part of the primary tumor . a sole brachytherapy in previously untreated lung tumors , irrespectively of the extrabronchial extension was used in a large series by stout et al . 
the papers compared with our data are outlined in table 5 , where only reports with comparable patient collectives and treatment situations were regarded . reports about a systematical combination of external beam treatment with brachytherapy are rare . 
with an external dose of 50 to 60 gy and a endoluminal dose between 15 and 25 gy they observed in 36% complete remissions and a median survival time of 13 months . they found , as we did , a correlation of mediastinal involvement and treatment outcome . 
the results reported by other authors are outlined in table 5 . our favorable results may be explained by a selected patient collective with small tumor diameters . the discussion about the side effects of hdr brachytherapy is controversial . 
 [ 26 ] reported in an prospective analysis on 50 patients treated with hdr afterloading alone ( 3 times 10 gy ) or in combination with ebrt ( 50 gy , 2 times 10 gy hdr )  . 
in contrast , we observed a much lower rate of fatal events and in all of our patients who expired from fatal events progression of local disease had been proven . 
also pretreatment with laser was suspected for a higher risk of bleeding [ 28 ] , while other authors denied this connection and accused more the length of the irradiated volume [ 15 ]  . 
in our collective this was not discriminable due to the fact , that the majority of patients had tumors located in trachea and main stem bronchus . the high contact doses occurring at the surface of the commercially available thin catheters prompted us to construct an applicator distanciable from the mucosa [ 8 ]  . 
in the remaining patients the diameter of the stenosis was too small to insert the catheter . using this device , which is also accepted by other groups [ 21 ] we observed a relatively low complication rate . 
in the subgroup of previously untreated patients with centrally located tracheobronchial nsclc without gross mediastinal involvement a long - term tumor control can be reached ( 5 - year local progression free survival 37% )  . 
in this situation , a dose prescription of 50 gy externally and 3 times 5 gy endoluminally specified to 1 cm distance from the source axis can be applied safely . 
thus , further prospective randomized studies are required to determine the role and the technical aspects of brachytherapy in the treatment to upper respiratory tract malignancies . strahlentherapie und onkologie urban & vogel 2000 aktuelles forum histologie des primrtumors und metastasenverhalten implikationen fr den radioonkologen anhand von beispielen walter rhomberg1 hintergrund : den beziehungen zwischen der histologie eines primrtumors und der art seiner spteren metastasierung ist bisher wenig aufmerksamkeit geschenkt worden . 
grundlage der bersicht bilden prospektiv zu diesem thema gesammelte literatur der letzten 25 jahre , ein zustzliches literatur - screening in medline ( 1988 bis 1997 ) sowie eigene analysen zum mammakarzino resultate : zwischen der histologie eines primrtumors und der art seiner spteren metastasierung sind bei bestimmten tumoren klare gesetzmigkeiten zu beobachten . 
es werden eine bersicht ber die heute bekannten zusammenhnge bei den wichtigsten soliden tumoren der oberen krperhlfte gegeben und auf einige konsequenzen fr den radioonkologen hingewiesen . schufolgerung : die kenntnis dieser zusammenhnge kann eine hilfe fr die rechte wahl des zielvolumens oder die entscheidung ber die sinnvolle anwendung einer konformalen radiotherapie se sie bildet darber hinaus die grundlage fr eine differenzierte adjuvante therapie und ermglicht eine rationalisierung der nachsorge . 
aufwendige bildgebende verfahren knnen selektiv an orten mit einer hohen metastasierungswahrscheinlichkeit eingesetzt werden . schlsselwrter : histologie metastasierung adjuvante therapie nachsorge therapieplanung histology of the primary tumor and pattern of metastasis . 
implications for the radiooncologist with clinical examples background : in the past , little attention has been given to the relationship of the histology of a primary tumor to its possible subsequent pattern of metastasis . 
the knowledge of these relations , however , is of importance for the radiooncologist for several reasons . materials and methods : a review on the relation between the histology of a primary tumor and the pattern of subsequent metastasis has been worked out . 
the review is based on references personally collected during the past 25 years , a medline screen ( 1988 to 1997 ) and own analyses related to the topic . results : strong relationships seem to exist between the histology of certain primary tumors and their subsequent pattern of metastasis . 
examples demonstrate those relations which are presently known about the main solid tumors of the upper part of the body and the sksome implications for the radiooncologist were pointed out . 
moreover , the data are of considerable importance to the follow - up of patients : imaging procedures may be more accurately applied in the areas with a high probability of recurrence or metastasis . key words : histology of primary tumors patterns of metastasis treatment planning follow - up den beziehungen zwischen der histologie eines primrtumors und der art einer spteren metastasierung ist bisher wenig aufmerksamkeit geschenkt worden . 
die kenntnis solcher zusammenhnge hat unter anderem einflu auf die wahl der einzuschlagenden primrtherapie , beispielsweise auf die wahl des zielvolumens oder die entscheidung ber die sinnvolle anwendung einer konformierenden radiotherapie einer region im einzelfall . 
sie bietet darber hinaus die rationelle grundlage fr eine differenzierte adjuvante therapie ( beispiel : prophylaktische bestrahlung des zentralnervensystems bei leukmien im kindesalter ) und erlaubt schlielich eine gezieltere nachsorge 1abteilung fr radioonkologie , landeskrankenhaus feldkirch , sterreich . eingang des manuskripts : 14 . 
histologie des primrtumors und metastasenverhalten mit einsatz der bildgebenden verfahren am ort der grten rezidivoder metastasierungswahrscheinlichkeit . primitive neuroendokrine tumoren ( pnet ) und ependymome im folgenden wird versucht , die heute bekannten zusammenhnge zwischen der histologie eines primrtumors und seinen potentiellen metastasierungsmustern zunchst bei den wichtigsten karzinomen zu sichten . 
fr eine systematische hereinnahme molekularbiologischer charakteristika in diese bersicht ist es daher noch zu frh , obwohl zum beispiel beim mammakarzinom schon interessante details zur metastasierungswahrscheinlichkeit in die regionren lymphknoten erarbeitet wurden [ 39 , 46 , 73 , 74 ]  . 
die expression von onkogenen hat bisher eher eine allgemein prognostische bedeutung erlangt . es wurden auch genprodukte beschrieben , die mit einem ausbleiben der metastasierung verbunden sind [ 70 ]  . es geht hier also nicht um alle heute erfabaren pathologisch - anatomischen details , sondern zur hauptsache um die klassischen histologischen formen eines tumors und ihre beziehung zur nachfolgenden metastasierung . hirntumoren gliome grad iii und iv diese tumoren metastasieren sehr selten in extrakranielle regionen . 
die extrakranielle ausbreitung ist in der regel ein sptes phnomen im krankheitsverlauf und kommt berwiegend nach einem neurochirurgischen eingriff vor . beim erwachsenen dominieren dann lungenmetastasen und peritoneale absiedelungen , speziell nach liquorshunt - operationen . 
der bericht stimmt mit anderen studien berein , in welchen ein multifokales auftreten des glioblastoma multiforme in 2 bis 10% der flle angegeben wird [ 61 , 66 ]  . 
es stellt sich hier die frage , in welchen fllen eine zusatzbestrahlung der kraniospinalen achse zur prophylaxe von abtropfmetastasen in den rckenmarkskanal indiziert ist . primitive neuroendokrine tumoren der hinteren schdelgrube ( medulloblastome ) erfordern in jedem fall eine kraniospinale bestrahlung . 
auch das boost - volumen an der hinteren schdelgrube mu wegen der hufigen leptomeningealen infiltration um den hirnstamm , die nervenaustrittsstellen und blutgefe grozgig bemessen sein [ 24 ]  . 
strahlendosen unter 50 gy an der hinteren schdelgrube und weniger als 34 gy am spinalkanal reichen zu einer lokalen tumorkontrolle nicht aus [ 32 ]  . bei zerebralen ependymomen und pinealoblastomen wurde die kraniospinale bestrahlung bisher kontrovers diskutiert [ 13 ]  . 
eine zusatzbestrahlung der spinalen achse wird als berflssig betrachtet , da eine meningeale streuung ( hufigkeit 5 bis 15% ) in der mehrzahl der flle ohnehin mit einer fehlenden lokalen kontrolle im bestrahlungsfeld einhergeht [ 12 , 42 , 54 ]  . ganzachsenbestrahlungen werden von einzelnen zentren nur im falle eines radiologisch oder pathologisch nachgewiesen befalls des spinalkanals eingesetzt [ 42 ]  . 
 bei primren zerebralen neuroblastomen scheint eine alleinige fokale strahlentherapie ausreichend zu sein [ 65 ]  . tumoren im kopfund halsbereich die ausbreitung der dominierenden plattenepithelkarzinome erfolgt meist per continuitatem und ber die lymphabfluwege . 
allgemein gilt fr die plattenepithelkarzinome eine eher geringe tendenz ( 10 bis 15% ) zu einer unspezifischen fernmetastasierung [ 50 , 55 ]  . hhere raten an fernmetastasen sind bei den fortgeschrittenen pharynxtumoren , speziell des epipharynx , zu erwarten . beim plattenepithelkarzinom seien drei varianten erwhnt : eine hochdifferenzierte form , das verrukse karzinom ( ackermann - tumor ) , zeigt nur eine geringe metastasierungsneigung [ 4 , 38 , 41 ] und entwickelt sich hufig am larynx oder der wangenschleimhaut . 
der tumor hat eine bessere prognose , doch ist er im vergleich zum normalen plattenepithelkarzinom weniger strahlensensibel und sollte daher mglichst radikal operiert werden [ 4 , 6 , 28 , 41 ]  . 
die von chirurgischer seite immer wieder angefhrte anaplastische transformation verrukser karzinome nach einer bestrahlung darf nach neueren untersuchungen relativiert werden , kommt sie doch auch nach einer alleinigen operation vor und ist berdies nicht hufig [ 48 , 72 ]  . 
typisch sollen perineurale tumorinvasion und aggressive krankheitsverlufe sein [ 16 ] ; im nasopharynxbereich ist die prognose eventuell besser [ 78 ]  . adenound mukoepidermoide karzinome der speicheldrsen sind selten . 
ber spezielle ausbreitungswege dieser formen liegen keine beschreibungen vor ; fernmetastasen sind selten . die adenoidzystischen karzinome ( zylindrome ) sind dadurch gekennzeichnet , da sich ein teil von ihnen entlang der perineuralen lymphspalten des nervus facialis ausbreitet . 
die rate an fernmetastasen scheint bei tumoren mit perineuraler ausbreitung nicht hher als bei tumoren ohne dieses zeichen zu seinsgesamt ist bei einem viertel der zylindrome mit fernmetastasen , vor allem in der lunge , zu rechnen , wobei die rein kribrsen formen seltener als die soliden formen metastasieren [ 63 ]  . schilddrse die gut differenzierten papillren karzinome treten in bis zu 75% multifokal auf . 
rezidive und auch ein primrer lymphknotenbefall sind mit sorgfltigen chirurgischen manahmen und einer radiojodtherapie ausreichend beherrschbar , so da eine perkutane nachbestrahlung als routinemanahme nicht indiziert ist [ 5 , 29 , 79 ]  . 
eine perkutane nachbestrahlung ist bei ausgedehntem lymphknotenbefall oder residualtumor an der schilddrse wahrscheinlich ratsam , doch fehlen hier randomisierte studien sowie gesicherte kenntnisse zur strahlensensibilitt . anaplastische karzinome zeigen ein aggressives lokales wachstum und eine neigung zu frher hmatogener aussaat , wobei sich die metastasen an keine bestimmten organe zu halten scheinen . 
bei den regionr wachsenden formen ist eine aggressive perkutane strahlenbehandlung indiziert , wobei teilweise von der konventionellen fraktionierung , zum beispiel durch zustzliche hohe einzeldosen , abgewichen werden mu , um die resistenz mancher flle zu durchbrechen . 
 die wichtigsten eigenheiten des metastasierungsverhaltens der schilddrsenkarzinome sind in tabelle 1 zusammengefat . histologischer aufbau lokales wachstum regionaler lymphknotenmetastasen befall fernpapillr follikulr medullr multifokal + + + * * unifokal bilateral * anaplastisch aggressiv + + + tabelle 1 . 
histologie des primrtumors und metastasenverhalten mammakarzinom im klinischen alltag sind die zusammenhnge zwischen der histologie des primrtumors und des nachfolgenden metastasierungsmusters aufgrund der vielfalt der histologischen bilder beim mammakarzinom nicht sofort einsehbar , da histologisch verschiedene mischformen und damit oft ubiquitre metastasierungen berwiegen . 
 eine eigene analyse bei 343 patientinnen mit disseminiertem mammakarzinom zeigte , da infiltrierende duktale karzinome ohne produktive fibrose ( zum groteil solide und medullre karzinome nach der lteren nomenklatur von albertini ) eine besondere neigung zur viszeralen metastasierung haben . 
in den grenzzonen dieses diagramms ergeben sich weitere sonderformen : szirrhse adenokarzinome entwickeln oft den sogenannten knochen - e - typ ( kortikalisdestruktion mit weichteilkomponente ) , der auch bei den solid - szirrhsen formen vorkommt . bei der mischung von szirrhus und komedokarzinom tritt berraschenderweise eine starke leberaffinitt auf , und die carcinoma scirrhosum carcinoma solidum alle organe mglich carcinoma adenomatosum carcinoma intraductale mischtyp oligotope knochenmetastasierung abbildung 1 . 
skeletal affinity , skin and serosal involvement ; b : visceral predominance , frequent local recurrences ; c : visceral predominance ; d : high affinity to the liver . mehrzahl der patienten verstirbt mit ikterus und im leberkoma ( unverffentlichte beobachtungen )  . 
in der heute gltigen who - klassifikation [ 80 ] , welche etwa 80% der mammakarzinome nach histogenetischen gesichtspunkten in duktale und lobulre formen einteilt , treffen wir einen guten teil der szirrhsen karzinome bei den lobulren formen wieder . 
sonderformen wie intrazystische papillre adenokarzinome , adenoidzystische karzinome [ 53 ] oder das tubulre karzinom [ 22 ] gehen praktisch nie mit regionren lymphknotenmetastasen einher , so da in diesen fllen auch bei nicht explorierter axilla oder medial gelegenem sitz des primrtumors mit gutem gewissen auf eine mitbestrahlung des lymphabflusses verzichtet werden kann . interessante anstze zur besseren vorhersage einer regionren lymphknotenbeteiligung finden sich in berichten ber hufigere expressionen bestimmter onkogene bei nodal positiven patientinnen gegenber frauen mit negativer axilla [ 39 , 46 , 73 ]  . 
nach vier bis fnf jahren erreichen jedoch die nichtkleinzelligen eine kumulative metastaseninzidenz von 75 bis 80% , welche derjenigen der kleinzelligen karzinome kaum nachsteht [ 51 , 52 , 60 ]  . 
sie erlauben die bemessung besonders knapper zielvolumina ( unverffentlichte beobachtungen )  . beim hufig peripher gelegenen adenokarzinom ist hingegen eine ausgeprgte lokoregionre ausbreitungstendenz mit befall der pleura und brustwand zu beachten . 
dies ist bei der bestrahlungsplanung speziell der brustwandnahen tumoren zu bercksichtigen , auch wenn in der ct - untersuchung zunchst kein befall der pleura sichtbar ist [ 71 ]  . beim bronchoalveolren karzinom wurde schon mitte der 50er jahre erkannt , da eine solitre form mit besserer prognose von einer diffus wachsenden form abgegrenzt werden mu ( bersicht bei [ 44 ] )  . 
histologisch knnen drei subtypen unterschieden werden : muzinse , nichtmuzinse und sklerosierende formen , wobei muzinse und sklerosierende bilder hufig mit der diffusen oder multizentrischen ausbreitung verbunden sind [ 3 ]  . 
 [ 40 ] versuchten als erste eine nhere histologische abgrenzung und beschrieben , da der diffuse , eventuell auch multizentrische typ mit starker makround mikroskopischer muzinproduktion verbunden ist , whrend der solitre typ weniger muzin erkennen lt . die fnf - jahres - berlebenszeit der so unterschiedenen typen war im ersten fall 26% , beim solitren typ 72% . 
als weiteres charakteristikum und mgliche erklrung fr das diffuse wachstum wurde in jngster zeit beim diffusen typ eine exzessive produktion des hepatocyte growth factor / scatter factor beschrieben [ 81 ]  . hautkarzinome basaliome zeigen eine sehr geringe tendenz zur metastasierung . 
lokal aggressive formen findet man auch unter den sklerosierenden basaliomen oder bei zellbildern , die durch schmale , spitz zulaufende zellzge , fehlende differenzierung und eine hyalinisierung des stromas gekennzeichnet sind [ 30 ]  . 
eine desmoplasie beim epidermoiden karzinom ist ein signifikanter negativer prognosefaktor mit hheren raten an lokalrezidiven und fernmetastasen [ 8 ]  . der 1972 erstmals beschriebene neuroendokrine merkelzell - tumor [ 27 ] ist hufig im gesichtsund halsbereich lokalisiert . 
die alleinige operation ist in der regel nicht ausreichend [ 33 , 49 ] , ebensowenig eine chemotherapie [ 23 ]  . lokalrezidive sind meist mit fernmetastasen verbunden [ 45 ]  . das metastasierungsmuster der melanome erscheint variabel und wenig berechenbar . 
uveamelanome unterscheiden sich von den kutanen melanomen dadurch , da sie praktisch nicht in die regionren lymphknoten siedeln und bei einer fernmetastasierung in der regel nur ein organ ( leber , seltener lunge ) befallen [ 18 ]  . 
die prognose wird unterschiedlich bewertet [ 11 , 57 ] : in einer sehr groen australischen serie ist sie nicht verschieden von den anderen kutanen melanomen [ 56 ]  . 
desgleichen gibt es leider keine verllichen prognostischen kriterien fr einen zu erwartenden regionren lymphknotenbefall . abschlieende bemerkungen die bersicht zeigt den heute sicher noch lckenhaften kenntnisstand der beziehung von histologie und metastasierungsmustern bei den karzinomen der oberen krperhlfte . 
in einer qualitativen auswertung wurden die erkennbarkeit und abgrenzung der tumoren anhand einer multireader - analyse beurteilt . ergebnisse : der tumor - zu - hintergrund - kontrast bei zerebralen gliomen war auf den nativen flair - aufnahmen den konventionellen fse - aufnahmen unterlegen . 
nach kontrastmittelgabe stieg das signal bei anreichernden tumoren auf den flair - bildern im mittel um 49% , wodurch der tumor - zu - hintergrund - kontrast den der konventionellen aufnahmen signifikant ( p < 0 , 001 ) bertraf . 
bei patienten mit zerebralen metastasen konnten mittels kontrastmitteluntersttzter flair - aufnahmen signifikant mehr metastasen als mit nativer flairund t2 / pd - gewichteter fse - sequenz , jedoch weniger als mittels kontrastmittelverstrkter t1 se - sequenz erkannt werden . 
vorteil der methode war jedoch wie bei den zerebralen gliomen die gleichzeitige darstellung von anreicherndem tumor und umgebendem de artefakte nahe der liquorrume sind auf flair - bildern hufig , sie strten die bildinterpretation jedoch nicht wesentlich . 
signalhyperintensitten aufgrund physiologischer gliosezonen an den ventrikelrndern sind ebenfalls hufig zu beobachten und mssen in die bildinterpretation einbezogen werden . schlufolgerung : zusammengefat bietet sich die flair - technik als eine wertvolle bildgebungssequenz in der stereotaktischen strahlentherapieplanung von zerebralen tumoren an . 
dieses ist insbesondere fr das einladen der bilddaten in die verwendeten bestrahlungsplanungssysteme von vorteil , da die bilddatenmenge deutlich reduziert , der arbeitsaufwand fr zustzliche bildfusionen vermindert und mgliche fehlerquellen bei der bildfusion vermieden werden knnen . schlsselwrter : strahlentherapieplanung stereotaxie magnetresonanztomographie flair - bildgebung gliome metastasen 1forschungsschwerpunkt radiologische diagnostik und therapie , deutsches krebsforschungszentrum , heidelberg , 2radiologische universittsklinik , heidelberg . eingang des manuskripts : 9 . 
the aim of the study was to assess the value of a flair technique in the planning process of stereotactic radiotherapy in patients with cerebral gliomas and metastases . patients and methods : thirty - five patients with cerebral gliomas and 12 patients with a total of 39 cerebral metastases were examined by t2 / pd - weighted fast spin - echo , fast flair prior and after contrast and contrast enhanced t1weighted spin - echo using identical slice parameters . 
the qualitative evaluation was performed as a multireader analysis concerning lesion detection , lesion delineation and image artifacts . results : in the qualitative evaluation ( tables 3 and 6 ) , all readers found the fast flair images to be superior to fast spin - echo in the exact delineation of cerebral tumors ( p < 0.001 ) and the delineation of enhancing and non enhancing tumor parts . 
the tumor - to - background contrast and tumor - to - background contrastto - noise of the fast flair images were lower than that of t2 - weighted spin - echo images but were significantly increased after the application of contrast media . 
this enables to load a reduced image amount into the radiotherapy planning software , is therefore time saving and reduces potential errors . key words : radiotherapy planning stereotaxie magnetic resonance imaging flair imaging glioma metastases u nter dem begriff stereotaxie werden methoden zusammengefat , mit welchen ein punkt innerhalb des krpers mittels eines extern am patienten angebrachten koordinatensystems bestimmt wird [ 1 ]  . 
die strahlentherapie bedient sich dieser methode zur planung kleinvolumiger , hochdosierter einzeitbestrahlung ( radiochirurgie ) [ 2 , 20 ] und gezielter fraktionierter strahlentherapie ( stereotaktische strahlentherapie ) [ 3 , 24 ]  . 
das ziel der radiochirurgie nach leksell [ 16 ] ist hierbei die zerstrung des gewebes innerhalb des gewhlten zielvolumens bei mglichst vollstndiger schonung des umliegenden gewebes ber die anwendung steiler dosisgradienten . voraussetzung ist hierzu eine mglichst exakte definition des zielvolumens im rahmen der strahlentherapieplanung [ 8 ]  . 
die grundlage hierfr sind die umfassende darstellung der pathologie und die mglichst exakte abgrenzung zum umgebenden normalen gewebe . in der strahlentherapieplanung zerebraler pathologien hat sich die magnetresonanztomographie ( mrt ) aufgrund ihres hohen lsionskontrastes und der mglichkeit einer multiplanaren schichtfhrung als methode der wahl zur darstellung des zielvolumens etabliert [ 4 , 5 , 21 , 29 ]  . 
techniken , die eine erhhung des signals der lsion oder eine unterdrckung des hintergrundes erreichen , fhren somit zu einer verbesserten erkennbarkeit und abgrenzung von lsionen [ 13 , 14 , 28 , 30 ]  . eine mglichkeit der kontrastverstrkung bietet die sogenannte flair - ( fluid attenuated inversion recovery - ) technik . 
durch die kombination einer langen echo - zeit mit der langen inversionszeit in der sequenz erfahren die bilder zustzlich einen t1 - effekt , durch welchen es zu einer absenkung des signals der weien hirnsubstanz im vergleich zum tumor kommt [ 10 ]  . 
frhere studien bei anreichernden gliomen und metastasen konnten zeigen , da eine signifikante kontrastmittelanreicherung im tumor beobachtet werden kann , welche den kontrast tumor und umgebendes gewebe zustzlich verbessert [ 11 , 17 ]  . ziel unserer untersuchungen war es , die wertigkeit der flair - technik fr die bestrahlungsplanung von zerebralen gliomen und metastasen zu bestimmen . patienten und methoden patientenstudien 35 patienten ( 18 frauen , 17 mnner ; alter 16 bis 65 jahre , mittleres alter 34 , 5 jahre ) mit histologisch gesicherten zerebralen gliomen und zwlf patienten ( vier frauen , acht mnner ; alter 29 bis 71 jahre , mittleres alter 45 , 9 jahre ) mit zerebralen metastasen wurden im rahmen der therapieplanung untersucht . 
tumorkontrast und - abgrenzung mit flair - bildgebung die mr - untersuchungen wurden auf einem 1 , 5 - tesla - mrsystem ( magnetom vision , siemens , erlangen ) unter verwendung einer zirkular polarisierten kopfspule durchgefhrt . 
jeweils 23 schichten mit einer matrix von 168 256 mm , einem field - of - view von 180 240 mm , einer schichtdicke von 5 mm und einem schichtabstand von 1 mm wurden in t2 - , pd - , t1und flair - technik unter verwendung identischer schichtparameter durchgefhrt . 
die verwendeten sequenzparameter sind in tabelle 1 zusammengefat ; die parameter der flair - sequenz wurden anhand vorheriger beschreibungen auf einen optimalen lsions - zu - hintergrund - kontrast eingestellt [ 18 ]  . an kontrastmittel wurde bei patienten mit gliomen die standarddosis von 0 , 1 mmol / kg krpergewicht , bei metastasen eine dosis von 0 , 2 mmol / kg krpergewicht intravens verabreicht . auswertung der patientenstudien die erzeugten flair - aufnahmen vor und nach kontrastmittelgabe wurden mit den konventionellen seund tseaufnahmen unter verwendung von quantitativen und qualitativen kriterien verglichen . quantitative auswertung : zur quantitativen auswertung wurden signalintensitten ber eine roi - ( region of interest - ) analyse innerhalb des tumors , der weien hirnsubstanz und des liquors bestimmt . 
ein p - wert von < 0 , 05 wurde als signifikant eingestuft . qualitative auswertung : bei patienten mit zerebralen gliomen wurden folgende qualitative kriterien fr den vergleich der unterschiedlichen modalitten verwendet : die abgrenzung des tumors von seiner umgebung , bei kontrastmittelaufnehmendem tumor zustzlich die abgrenzung der anreichernden von den nichtanreichernden tumoranteilen , auerdem die lsionserkennbarkeit und die lsionsabgrenzung . smtliche auswertungen wurden als multireader - analyse mit hilfe eines standardisierten auswertebogens durchgefhrt . 
zwei erfahrene mr - untersucher beurteilten die aufnahmen unabhngig , bei diskrepanz der beurteilung wurde ein konsensus erreicht . zum vergleich der flair - technik mit konventionellen t2 - gewichteten sequenzen wurde fr die beurteilung der tumorabgrenzung eine drei - punkte - skala mit : + 1 = flair besser , 0 = flair gleich und - 1 = flair schlechter verwendet . fr die abgrenzung von tumor und dem und fr die abgrenzung der anreichernden von den nichtanreichernden tumoranteilen in den unterschiedlichen techniken wurde folgende drei - punkte - skala festgelegt : + 1 = sichere abgrenzung , 0 = abgrenzung mglich , aber nicht sicher und - 1 = keine abgrenzung . 
die kontrastmitteluntersttzten t1 se dienten hierbei als interner goldstandard . die statistische signifikanz fr die erkennbarkeit von lsionen wurde mit einem einseitigen oder zweiseitigen gepaarten t - test durchgefhrt [ 15 ]  . 
die auswertung der lsionsabgrenzung erfolgte wie bei patienten mit gliomen anhand einer punkteskala : + 1 = kontrastmitteluntersttzte flair besser , 0 = kontrastmitteluntersttzte flair gleich und - 1 = kontrastmitteluntersttzte flair schlechter . 
zur quantifizierung der artefakthufigkeit wurde folgende skala angewandt : + 1 = flair oder kontrastmitteluntersttzte flair weniger artefakte , 0 = kontrastmitteluntersttzte flair gleich viele artefakte oder - 1 kontrastmitteluntersttzte flair mehr artefakte . ergebnisse patienten mit zerebralen gliomen insgesamt wurden mr - tomographisch 37 lsionen bei 35 patienten nachgewiesen . 
tumorkontrast und - abgrenzung mit flair - bildgebung tumor liquor weie substanz 1012 176 1047 137 463 61 1199 151 1004 114 828 90 flair 557 116 124 41 298 44 tabelle 2a . 
das liquorsignal auf flair betrgt lediglich 10% des signals in t2und pd - gewichteten sequenzen . die berechneten tumor - zu - hintergrundsowie tumor - zuliquor - kontrastwerte zeigt tabelle 3 . 
der tumor - zu - hintergrund - kontrast ist auf den nativen flair - aufnahmen geringer als auf den t2und pd - gewichteten aufnahmen ( p < 0 , 01 )  . 
tumor delineation in non enhancing gliomas ( n = 14 )  . neren als auch der ueren liquorrume fanden beide leser die flair - aufnahmen in der lsionsabgrenzung den t2und pd - gewichteten fse - bildern berlegen ( tabelle 4 , abbildungen 1a und 1b )  . 
auf kontrastmitteluntersttzten flair - bildern war die differenzierung bei smtlichen lsionen , auf den nativen flairbildern bei 44% der lsionen mglich ( abbildungen 2a bis 2d )  . als vorteil der methode wurde insbesondere die gleichzeitige darstellung der anreichernden und nichtanreichernden tumoranteile angesehen . patienten mit zerebralen metastasen auf kontrastmitteluntersttzten t1 - gewichteten se - bildern konnten insgesamt 39 metastasen bei zwlf patienten aufgezeigt werden . 
primrtumoren waren bronchialkarzinom ( n = 6 ) , melanom ( n = 2 ) , mammakarzinom ( n = 3 ) und nierenzellkarzinom ( n = 1 )  . quantitative auswertung : die mittleren signalintensitten der metastasen auf nativen und kontrastmittelverstrkten flair - aufnahmen zeigt tabelle 5 , die zugehrigen kontrastwerte tabelle 6 . 
hierdurch kam es auch zu einer deutlichen verbesserung des tumorkontrastes . qualitative auswertung : durch die deutliche unterdrckung des flssigkeitssignals sowohl innerhalb der inqualitative auswertung : tabelle 7 zeigt die detektionsrate bei den verschiedenen techniken . 
durch die gabe von kontrastmittel konnte die detektionsrate auf flair - aufnahmen signifikant gesteigert werden ( p < 0 , 01 ) , erreichte jedoch nicht das niveau von kontrastmitteluntersttzten t1 se - bildern . 
bei kleinen lsionen hingegen war die detektionsrate auf nativen flairund fse - bildern sehr gering , die gabe von kontrastmittel verbesserte die detektionsrate bei den flair - bildern signifikant . bei der lsionsabgrenzung der auf allen modalitten sichtbaren metastasen ( n = 18 ) waren kontrastmittelverstrkte flair - aufnahmen in 14 lsionen den nativen flairund fse - bildern berlegen , bei vier lsionen ergab sich kein unterschied . 
bei der abgrenzung der kontrastmittelanreicherung zeigte sich kein unterschied zwischen den flairund t1 - aufnahmen ( siehe abbildungen 4a bis 4c )  . als vorteil von flair - aufnahmen gegenber den t1 sebildern erwies sich das sehr ausgeprgte flow void - phnomen der methode , welches durch die sehr lange echozeit bedingt ist . 
durch die starke verkrzung der t1 - zeit knnen kleinere blutgefe auf konventionellen aufnahmen als parenchymatse kontrastmittelanreicherung und somit als metastasenverdchtig fehlgedeutet werden , insbesondere bei sehr langsamem flu in diesen gefen . 
es konnten bei unseren patienten somit insgesamt fnf suspekte lsionen eindeutig als gefstrukturen identifiziert werden . 18 * , * * 28 * , * * 15 * , * * tabelle 7 . 
bei zerebralen metastasen hat sich die radiochirurgie als primre oder sekundre boosttherapie etabliert ; diese sind mittlerweile gesicherte indikationen , welche sich durch ihre geringe invasivitt im vergleich zu anderen therapieverfahren auszeichnen [ 2 , 3 , 20 ]  . der stellenwert fraktionierter stereotaktischer strahlentherapie in der behandlung von malignen gliomen ist gegenstand wissenschaftlicher untersuchungen [ 9 , 27 ]  . im rahmen der prtherapeutischen diagnostik und insbesondere in der radiochirurgischen therapieplanung haben sich die modernen schnittbildverfahren wie ct und mrt als fester bestandteil etabliert [ 8 ]  . 
bei zerebralen prozessen kommt hierbei der mrt die grte bedeutung zu [ 4 , 8 ]  . aufgabe der im rahmen der therapieplanung durchgefhrten bildgebung sind hierbei die mglichst przise abbildung und definition des zielvolumens und der angrenzenden risikostrukturen [ 2 , 3 , 8 , 20 , 24 ]  . 
die auswahl geeigneter untersuchungsprotokolle ist daher fr die millimetergenaue bestrahlung essentiell . in der erkennbarkeit zerebraler gliome sind t2 - gewichtete und kontrastmitteluntersttzte t1 - gewichtete sequenzen als die sensitivsten bildgebungsmodalitten akzeptiert [ 4 , 5 , 29 ]  . wie bei den meisten anderen pathologien des gehirns fhrt die verlngerung der t2 - relaxationszeiten innerhalb des gesamten tumors zu einem hohen kontrast zwischen tumor und umgebendem gewebe . 
tumorkontrast und - abgrenzung mit flair - bildgebung zung der areale mit erhhtem signal auf t2 - gewichteten sequenzen auch als radiologischer tumorrand definiert [ 4 ]  . die hohe sensitivitt der mrt in der erkennbarkeit von strungen der blut - hirn - schranke auf t1 - gewichteten sequenzen nach kontrastmittel fhrt des weiteren zu einem hohen kontrast zwischen den kontrastmittelanreichernden und nicht kontrastmittelanreichernden tumoranteilen [ 13 , 14 , 21 , 28 , 39 ]  . 
bei patienten mit metastasen ist hingegen das histologische tumorvolumen auf die kontrastmittelanreicherung beschrnkt [ 25 ]  . bei patienten mit zerebralen metastasen sind daher kontrastmitteluntersttzte t1 - gewichtete se - sequenzen entscheidend , wobei hier der lsionskontrast durch die gabe erhhter kontrastmitteldosis , spte aufnahmezeiten oder durch magnetization - transfer - techniken verbessert werden kann [ 13 , 14 , 21 , 28 , 39 ]  . 
kleinere metastasen hingegen , welche sehr hufig kortikomedullr gelegen sind , knnen nur schlecht erkannt und abgegrenzt werden , da sie nicht mit einem dem oder einer raumforderung verbunden sind . in den letzten jahren wurde mehrfach ber eine flair - sequenz berichtet , welche sehr stark t2 - gewichtete sequenzen bei gleichzeitiger unterdrckung des liquors erzeugt [ 6 , 7 , 1012 , 17 , 19 ]  . 
krzlich wurden auch ergebnisse ber die wertigkeit von flair bei patienten mit zerebralen tumoren und den effekt von kontrastmittel auf flair - gewichtete bilder berichtet [ 10 , 11 , 17 ]  . bei patienten mit zerebralen gliomen konnten diese untersuchungen belegen , da die radiologischen tumorrnder abbildung 1a figure 1a abbildung 1b figure 1b abbildungen 1a und 1b . 
t2 ( a ) und flair ( b ) bildgebung bei einem 21jhrigen patienten mit niedergradigem astrozytom des hirnstammes . auf den t2 - gewichteten fse - aufnahmen ist der tumor durch das hohe signal im vierten ventrikel und der umgebenden liquorrume maskiert und somit weder als tumor zu erkennen noch eindeutig abzugrenzen . 
t2 ( a ) and fast flair ( b ) imaging in a 21 - year - old patient with low - grade astrocytoma of the brain steon t2 - weighted images the tumor is masked by the surrounding fourth ventricle and could not be clearly delineated . 
t2 ( a ) , flair ( b ) , kontrastmitteluntersttzte flair ( c ) und kontrastmitteluntersttzte t1 - gewichtete ( d ) sequenzen bei einem 59jhrigen patienten mit anaplastischem astrozytom ( who grad 3 ) der stammganglien und des thalamus rechts . 
t2 ( a ) , fast flair ( b ) , contrast enhanced flair ( c ) und contrast enhanced t1 - weighted ( d ) images of a 59 - year - old patient with anaplastic astrozytoma ( who grade 3 ) of the right thalamus and brain stet2 - weighted and non enhanced flair images only present the radiologic tumor margins and the t1 - weighted images only present the enhancing tumor tissue . 
t2 ( a ) and fast flair ( b ) imaging in a 38 - year - old patient with incomplete resection of a frontal low - grade astrocytoma . the coronal slice orientation present the residual tumor at the caudal and lateral border of the resection cavity and the infiltration of the corpus callosuthe delineation of the residual tumor tissue is best on the fast flair images due to the nearly complete suppression of the csf signal within the resection cavity and the lateral ventricles . auf flair - gewichteten aufnahmen besser detektiert und abgegrenzt werden ( abbildungen 1a und 1b , 2a bis 2d , 3a und 3b )  . 
als vorteile der flair - methode wurden die unterdrckung des liquorsignals , die bessere abgrenzung der makroskopischen tumoranteile und der reduzierte kontrast zwischen grauer und weier hirnsubstanz angesehen [ 10 ]  . diese vorteile erlauben insbesondere eine wesentlich bessere beurteilung von infiltrationen des balkens und der vorderen kommissur , welche das behandlungskonzept wesentlich ndert . in der vorliegenden untersuchung fhrte die unterdrckung des liquors ebenfalls zu einem deutlich besseren tumor - zu - liquor - kontrast , wodurch lsionen an der grenze des ventrikels und lsionen nahe des kortex eindeutiger erkannt und abgegrenzt werden konnten ( abbildungen 1a und 1b )  . 
hierdurch ergaben sich auch vorteile in der abgrenzung von tumorresten nach einem chirurgischen eingriff oder von rezidivtumoren ( abbildungen 3a und 3b )  . die exakte darstellung des restoder rezidivtumors ist fr das therapeutische vorgehen , die definition des zielvolumens und die prognose entscheidend [ 9 ]  . 
t2 ( a ) , contrast enhanced fast flair ( b ) and contrast enhanced t1 - weighted se ( c ) imaging of a 73 - year - old patient with solitary brain metastasis of a lung carcinoma . 
t2 - weighted fse images are not able to clearly delineate the metastasis from the surrounding tissue , which is best seen on the contrast enhanced fast flair images . abbildung 4c figure 4c zielvolumendefinition und zur verlaufskontrolle [ 9 , 27 ] , da von den makroskopischen tumorrndern ungefhr 90% der rezidive ausgehen . intrakranielle metastasen kommen in etwa 25% der patienten mit malignen erkrankungen vor und machen etwa 40% smtlicher hirnneoplasien im erwachsenenalter aus . 
ebenso ist der prognostische wert der anzahl an hirnmetastasen auf das berleben wohl bekannt . die detektion von zustzlichen lsionen ist hierbei stark abhngig von der lsionsgre und dem lsionskontrast . groe metastasen sind hufig mit einem masseneffekt oder einem vasogenen dem assoziiert und knnen daher einfach auf kontrastmitteluntersttzten mroder ct - bildern erkannt werden [ 3 , 4 , 8 , 20 , 24 ]  . 
whrend lsionen > 10 mm mit allen bildgebungsmethoden sehr gut dargestellt werden konnten , war die kontrastmitteluntersttzte flair - technik in der lage , auch kleinere , kortikal gelegene lsionen zu erkennen . 
daher ist die flair - methode sehr gut in der lage , kleinere gefbedingte suspekte lsionen als metastasen auszuschlieen . insgesamt zeichnete sich die flair - technik durch eine exakte abgrenzung von zerebralen metastasen aus , was fr die strahlentherapieplanung von vorteil ist . 
da die radiotherapie bei patienten mit solitren hirnmetastasen als stereotaktische einzeittherapie durchgefhrt wird , bentigt man auch hier eine exakte abgrenzung der metastase vom umgebenden dem und normalen hirngewebe . insgesamt ist die methode in der erkennbarkeit zerebraler metastasen den konventionellen kontrastmitteluntersttzten t1 - gewichteten se - sequenzen unterlegen , weshalb im rahmen des bestrahlungsplanungsprotokolls nicht auf letztere verzichtet werden kann . artefakte , welche durch liquorflu ausgelst sind , wurden bereits in frheren studien ber flair beschrieben und wurden auch bei unseren patienten sehr hufig beobachtet . sie treten vorwiegend in der umgebung des foramen monroi , des vierten ventrikels und des aquduktes auf und sind durch eine selektive prparation hervorgerufen . 
ein beispiel hierzu ist die verwendung einer ekg - triggerung . zusammenfassend lt sich aus den vorliegenden ergebnissen folgern , da die flair - technik eine wertvolle methode in der detektion und abgrenzung von malignen primren und sekundren intraaxialen hirntumoren darstellt . 
 materials and methods : single cell suspensions with or without gd - 157 and / or b - 10 were exposed to thermal neutrons produced by the kyoto university reactor , and standard cell survival curves were obtained . results : under the same molarity , cytocidal effects were 1.5 times greater for gd - 157 than for boron when compared at 10% survival levels . 
the presence of b - 10 enhanced the radiation effect of gd - 157 neutron capture by 1.2 - fold , suggesting that cells were not sufficiently irradiated as a result of neutron fluency attenuation by the presence of excess neutron capture agents in the medium . conclusions : when an equal number of atoms were present , gd - 157 was effective as b - 10 when exposed to an equal number of thermal neutrons . 
further studies are needed to determine optimal gd - 157 and b - 10 concentrations as a function of tumor dimension . key words : gadolinium boron neutron capture therapy vergleichende untersuchungen zu den strahleneffekten von gadoliniumund bor - neutronen - einfangreaktionen hintergrund : analysen des zellberlebens sind durchgefhrt worden , um die effekte ionisierender strahlung zu evaluieren , die durch neutroneneinfangreaktionen mit gadolinium - 157 , bor - 10 und einer kombination aus beiden entstehen . material und methoden : einzelzellsuspensionen mit und ohne gadolinium - 157 und / oder bor - 10 wurden einer bestrahlung mit thermalen neutronen aus dem reaktor der universitt kyoto unterzogen und zellberlebenskurven generiert . ergebnisse : unter quimolaren bedingungen war der effekt auf das zellberleben fr gadolinium - 157 1 , 5mal grer als der von bor - 10 , sofern ein vergleich auf dem 10% - berlebensniveau durchgefhrt wurde . 
bor - 10 verstrkte den strahleneffekt von gadolinium - 157 - neutroneneinfang um das 1 , 2fache . schlufolgerung : gadolinium - 157 und bor - 10 waren gleich effektiv , sofern sie einer gleichen zahl von thermalen neutronen exponiert wurden . 
 schlsselwrter : gadolinium bor neutroneneinfang n eutron capture therapy is a binary process in which the flux of thermal or epithermal neutrons is absorbed by neutron - capturing atoms loaded in the tumor with subsequent radiation emission resulting in tumor cell killing [ 3 , 10 ]  . 
clinical boron ( b ) neutron capture therapy in the 1950s failed to prove its effectiveness [ 6 ] but after new compounds , bsh ( sodium borocaptate ) and bpa ( p - boromophenylalanine ) , became available with a higher affinity to tumor cells compared to normal cells or the blood [ 15 ] , clinical b - neutron capture therapy was restarted in the 1970s . 
in contrast to b - neutron capture , gadolinium ( gd ) neutron capture results in release of gamma rays followed by a series of low - energy conversion and auger electrons [ 2 , 7 ] , a favorable characteristic because the location of the element is not critical with regard to the target cell due to their longer flight ranges . 
monte carlo calculations have suggested that over - all radiation effects are nearly equal for gd - 157 and b - 10 at an equal molecular concentration [ 11 ]  . various b - 10 compounds are under development for neutron capture therapy , but the only available gd - containing compound has been gd - dtpa [ 5 ] which offers an excellent tumor to blood or tumor to normal tissue ratio with its concentration in tissue being measured easily by mri studies . to a low flux of thermal neutrons at the facility . 
for cells after b - neutron capture , best - fitting of the survival data has revealed a shoulder region in the survival curve and that 1.69 1012 / cm2 neutrons are required to achieve 10% survival levels ( figure 1 )  . 
for neutron capture agents , either gd - 157 ( gd - dtpa , magnevist ) or b - 10 ( na2 10b12h11sh , sodium borocaptate = bsh ) or both were added to cell suspensions to yield final concentrations of 800 ppm and 51 ppm , respectively . 
teflon tubes ( 8 mm inner diameter 60 mm long , 1.0 mm thick ) were filled with 2 ml of cell suspensions ( 4 105 cells / tube ) from individual groups . 
 each tube was chilled in ice to prevent metabolic hypoxia prior to neutron exposure , placed perpendicular to the beam , and exposed to thermal neutrons generated by the heavy water facility of the kyoto university reactor ( kur , 5 mw , 2 109 thermal neutrons / cm2 / s ; a gamma dose rate of 1 gy / hour ) [ 10 ]  . 
after exposure , the cells were resuspended , diluted with fresh medium containing 10% fbs , and appropriate numbers of cells were plated onto plastic petri dishes for colony formation . 
dosimetry for neutrons was carried out with gold foil placed at proximal and distal sides of the teflon tube which was filled with gd - 157 and / or b - 10 - containing cell suspensions . 
the survival curves were drawn according to linear quadratic model . the survival curve for cells exposed to thermal neutrons alone is a simple negative exponential function , although the minimal survival level achieved was only 45% . 
this kinetic energy limits the flight range of alpha particles to approximately 10 m , which is comparable to the cell diameter . thus , b - 10 compounds must theoretically be in the cell to inactivate it , although a compound capable of entering specifically into tumor cells is not available at present . 
our data , however , contradict this observation that there was a small shoulder region present , suggesting that not all radiation involved is of high linear energy transfer ( let )  . 
gadolinium and boron neutron capture reactions flight ranges of alpha particles make volume factors negligible in b - neutron capture therapy [ 5 ]  . in the process of gd - neutron capture , photons and electrons of various energy levels are released [ 11 ]  . 
on the other hand , electron effects become significant for smaller treatment volumes as their flight ranges are from 0.1 to 50 m for auger electrons and 14 to 360 m for internal conversion electrons [ 9 ]  . 
 [ 1 ] reported that the contribution of electrons for cell killing was estimated to be 4 times more than that of gamma rays when a 0.6 cm diameter and 6 cm long vessel was used to contain cell suspensions for irradiation . 
monte carlo calculations have been carried out for a 2 to 4 cm diameter tumor containing 100 g / g gd - 157 located at a depth of 8 cm in a head phantom exposed to epithermal neutrons with a tumor - to - normal ratio of 10 . 
these data suggest that significantly enhanced effects can be achieved with gd - 157 [ 11 ]  . there is a significant difference in dose distribution between band gd - neutron capture therapy . 
in our experiments , gd - 157 in the form of gd - dtpa is more effective in cell killstrahlentherapie und onkologie urban & vogel 2000 originalarbeit combined radiochemotherapy with docetaxel in patients with unresectable locally advanced head and neck tumors katja hesse1 , bernhard heinrich1 , frank zimmermann1 , reinhard kau2 , gabriele sommer3 , wolf achterrath3 , michael molls1 , horst jrgen feldmann1 background : as the treatment with docetaxel in metastatic head and neck cancer resulted in an encouraging response rate , the following phase - i study examined the effects of a combined radiochemotherapy with weekly docetaxel in patients with inoperable advanced head and neck tumors . patients and methods : six patients with stage iv head and neck cancer were included into the study . 
within the treatment regimen the primary tumor and the involved lymph nodes were irradiated up to a total dose of 70 gy , the non involved cervical and supraclavicular lymph nodes received 50 gy in conventional fractionation . 
the initial dose was 15 mg / m2 . results : a dose escalation was impossible because of several dose limiting toxicities ( nci - ctc ) already in the first dose level . 
 key words : radiochemotherapy docetaxel head and neck tumor kombinierte radiochemotherapie mit docetaxel bei patienten mit inoperablen fortgeschrittenen hno - tumoren hintergrund : da die behandlung mit docetaxel bei metastasierten hno - tumoren eine gnstige ansprechrate ergeben hat , untersuchte die folgende phase - i - studie die effekte einer kombinierten radiochemotherapie mit wchentlicher gabe von docetaxel bei patienten mit inoperablen fortgeschrittenen hno - tumoren . patienten und methoden : in der zeit von september 1997 bis mrz 1998 wurden sechs patienten mit fortgeschrittenen hno - tumoren im stadium iv in die studie eingeschlossen . 
radiochemotherapy in head and neck tumors d espite many attempts to improve outcome of advanced head and neck tumors the 5 - year survival remains about 20 to 30% [ 8 , 13 , 28 ]  . 
ten to 20% suffer from a second tumor , usually elsewhere in the head and neck area or in the bronchus or esophagus [ 23 ]  . many clinical trials testing simultaneous chemoradiotherapy versus conventional radiotherapy alone showed a modest benefit in terms of response and survival for the combined modality treatment [ 16 , 26 , 35 ] , the most effective of them with 5 fu and platin improved the 5 - year survival rate about 12% [ 13 ]  . 
in contrast induction chemotherapy schemes have not achieved a significant improvement of survival [ 8 , 13 , 26 , 29 ] but have still a role in laryngeal preservation . 
first results showed an encouraging 5 - year survival of 37% [ 23 ] , although the rate of acute toxicity is considerably higher in hyperfractioned treatment schemes [ 27 ]  . inclusion of new cytotoxic drugs into chemoradiation might improve results . 
the overall response in phase - ii trials in the treatment of recurrent disease in head and neck tumors using docetaxel in a dose of 100 mg / m2 every 3 weeks was up to 42% [ 9 , 22 , 30 ] , while carbo - / cisplatin reached only a response rate of 20 to 30% [ 19 ]  . 
this might be the reason for the promising response rate of chemoradiation with taxanes in different entities like the bronchus carcinoma [ 5 , 19 , 24 ]  . therefore we initiated a phase - i trial with docetaxel in a combined chemoradiotherapy for advanced head and neck tumors . 
secondary objectives were response rate and duration . patients and methods patients : the criteria for inclusion and exclusion of patients in the study are listed in table 1 . treatment regimen : head and neck irradiation : the treatment consisted of a total tumor dose of radiation of 70 gy for the primary tumor and involved lymph node areas . 
it was applied as a dose of 2 gy daily on days 1 to 5 during 7 weeks . radiation was performed by a megavolt linear accelerator ( 6 mev )  . 
on days of chemotherapy radiation was given 1 hour after completion of the docetaxel short - time infusion . chemotherapy : on days 1 , 8 , 15 , 22 , 29 , 36 , 43 docetaxel was given intravenously in 1 hour . 
the starting dose was 15 mg / m2 and escalation was planned in steps of 5 mg / m2 , if 3 of 3 or at least 4 of 6 patients do not show any dose limiting toxicity . dose limiting toxicities were defined as mucositis grade 4 and skin side effects grade 4 lasting up to the next infusion date of docetaxel , neurological symptoms grade 3 , irreversible renal and hepatic disorders , thrombocytopenia grade 3 and / or granulocytopenia grade 4 for more than 3 days , as described in nci common toxicity criteria . 
 the study was approved by the local ethics committee . therapy was given with best supportive care including close observation on the ward . follow - up : four and 12 weeks after finishing treatment late side effects and response were documented by clinical examination , taking biopsies , magnetic resonance of the head and neck , chest x - ray and ultrasound abdomen . 
after that the follow - up was repeated every 3 months . results between september 1997 and march 1998 6 patients ( 5 male , 1 female ) with a median age of 52 years ( 34 to 67 years ) were included in the study . 
however , the application of chemotherapy had to be delayed because of a thrombocytopenia grade 3 during simultaneous treatment with fluconazol ( diflucan ) and metamizol ( novalgin )  . 
 inclusion criteria exclusion criteria measurable and evaluable tumor age between 18 and 70 years who - performance status 2 life expectancy of at least 3 months ascites or pericardial or signed informed consent prior to beginning the treatment histologically confirmed head and neck cancer creatinine clearance 60 ml / min presence of distant metastases prior treatment with corticosteroids within 30 days pregnancy pleural infusion preexisting renal , cardial , pulmonary , hepatic , neurological , psychiatric disease active infection prior participation in another study within 30 days prior treatment to the head and neck tumor prior malignancy besides non melanoma skin cancer or excised cervical carcinoma in situ table 1 . 
therapieergebnisse : bersicht ber jeden teilnehmenden patienten an der phase - i - studie mit wchentlicher gabe von docetaxel und simultaner strahlentherapie . dose - limiting toxicities ( table 2 ) : two patients developed a neurologic symptomatology grade 3 , 1 as a repeated reversible retention of urine which disappeared under spasmolytic treatment with carbachol and 1 as peroneal paralysis fever without infection mucositis grade 3 skin grade 1 grade 2 grade 3 infection grade 1 grade 2 grade 1 grade 2 grade 1 grade 2 edema grade 2 diarrhea grade 1 nausea grade 2 neuropathy grade 1 weight loss grade 1 grade 2 anemia grade 1 grade 2 lymphocytopenia grade 3 grade 4 table 3 . 
despite intensive examinations including mri of the central nervous system , examination of liquor and urologic tract no further explanations as a toxic reaction to docetaxel were found for these both symptoms . 
tissue culture studies have proven the ability of the taxanes to block and prolong cells in the g2 / m phase , which is known as the most radiosensitive phase of the cell cycle [ 32 ]  . 
recent publications often use weekly applications , which seem to cause less neutropenia [ 17 , 21 , 24 ]  . without radiotherapy the recommended dose for weekly application of docetaxel within phase - ii studies is 36 mg / m2 [ 17 ]  . 
forty - two patients with postoperative ( tur ) bladder carcinoma who received 68 to 74 gy / 2 gy and cisplatin 30 mg / m2 once a week tolerated docetaxel 40 mg / m2 weekly simultaneously [ 34 ]  . 
in comparison to that another group treating patients with advanced nsclc and esophagus carcinoma , considered a dose of 20 mg / m2 as tolerable [ 24 ] ( table 5 )  . in our study already 15 mg / m2 weekly were dose limiting . the reason for these differences might have been unfavorable constitution of our patients caused by longstanding abuse of nicotine and alcohol which were not visible despite strict inclusion criteria . 
as one explanation some biological and molecular data indicate a rising radiation sensitivity with growing age caused by a reduction of dna repair mechanisms [ 15 ]  . phase - ii study entity and stage number of patients chemotherapy with response docetaxel ( cr + pr ) ( % ) side effects , grade couteau et al . 
vergleich der ansprechraten und nebenwirkungen von phase - ii - studien mit docetaxel in dreiwchentlichem rhythmus / keine bestrahlung bei fortgeschrittenen tumorerkrankungen . author number of entity patients and stage radiotherapy chemotherapy 2 gy / fraction dose limiting side effects , grade toxicity hainsworth et al . 
nsclc 60 gy docetaxel paclitaxel paclitaxel 25 mg / m2 30 mg / m2 70 mg / m2 bladder carcinoma post tur 6874 gy cisplatin 30 mg / m2 , docetaxel 40 mg / m2 esophagitis / pulmonary mucositis 4 esophagitis 4 , neutropenia 3 neutropenia 34 : 8% , stricture of bladder : 4 / 37 , paresthesia : 3 / 37 , mot . 
another reason might be an enhanced damage of nerves ( including vagal nerve ) passing through the irradiation area due to the radiosensitizing effect of docetaxel , although the dose applied to the myelon was limited to 30 gy . referring to the pulmonary complications in our study the most probable reason of the pneumonia is aspiration . 
 [ 31 ] 7 of 14 patients with inoperable lung cancer treated with paclitaxel in a weekly dose of 50 to 86 mg / m2 during simultaneous radiotherapy developed a moderate to severe interstitial pneumonia outside the irradiated area . 
in summary it might be possible , that the risk for docetaxel - induced interstitial pneumonia is increased by simultaneous lymphocytopenia and that weekly application of docetaxel more often induces lymphopenia than the standard dosage . 
the exact correlation between these both symptoms so far remains open . conclusion already in the first dose level of weekly docetaxel parallel to radiation therapy of head and neck tumors several dose limiting toxicities were evident . 
before routinely used in this setting , further work with other dosing schedules has to be performed . strahlentherapie und onkologie urban & vogel 2000 originalarbeit carcinoma of the oropharynx : local failure as the decisive parameter for distant metastases and survival karl t . 
aebersold1 , peter zbren2 objective : how important and predicative are clinical parameters and locoregional failure after radical radiotherapy of oropharyngeal carcinomas for the probability of the occurrence of distant metastases ? patients and methods : from 1 august 1990 to 1 october 1998 , 139 patients with carcinomas of the oropharynx were treated in a prospective study by radical radiotherapy and evaluated in regard to the clinical parameters reflex - otalgia , predominant structure of tumor growth , t - category , presence of involved lymph nodes , and smoking and drinking habits . 
both groups , 62 patients with locoregional therapy failure and 77 patients with locoregionally controlled tumors , were comparable in regard to performance status ( karnofsky index ) , age , gender , tnm - categories , histological differentiation , drinking habits , pretherapeutic diagnostics , total dose ( gy ) , and number of simultaneous chemotherapy cycles . 
at this moment 81% of locoregionally controlled patients are still alive . in 14 / 62 patients ( 23% ) with locoregional failure , distant metastases were detectable against 4 / 77 ( 5% ) of locally controlled patients , p < 0.0026. 
 key words : oropharynx carcinoma radiotherapy clinical parameters local control metastases oropharynxkarzinome : fehlende lokoregionre kontrolle als entscheidender parameter fr fernmetastasen und berleben fragestellung : wie wichtig und wie aussagekrftig sind klinische parameter und lokoregionres therapieversagen nach radikaler radiotherapie von oropharynxkarzinomen fr die wahrscheinlichkeit des auftretens hmatogener metastasen ? patienten und methoden : zwischen 1 . 
1998 wurden 139 konsekutive patienten mit oropharynxkarzinomen in einer prospektiven studie mit einer radikalen radiotherapie behandelt und bezglich der klinischen parameter reflexotalgie , vorherrschende struktur des tumorwachstums , t - kategorie , lymphknotenbefall und genugewohnheiten untersucht . 
die beiden patientengruppen , 62 patienten mit lokalem therapieversagen und 77 patienten mit lokal geheiltem tumorleiden , waren vergleichbar bezglich karnofsky - index , alter , geschlecht , histologischer differenzierung , alkoholkonsum , prtherapeutischer diagnostik , gesamtdosis ( gy ) und anzahl der simultanen chemotherapiezyklen . 
die tumorkontrolle war von den parametern reflexotalgie ( p < 0 , 0078 ) , wachstumsstruktur ( p < 0 , 012 ) , t - kategorie ( p < 0 , 03 ) und rauchen ( p < 0 , 0285 ) signifikant mitbestimmt . 
carcinoma of the oropharynx wurden fernmetastasen nachgewiesen , dagegen nur bei 4 / 77 ( 5% ) der lokoregionr geheilten patienten ( p < 0 , 0026 )  . lokale kontrollwahrscheinlichkeit und fernmetastasierung , am hufigsten lungenmetastasen , erreichten ein plateau nach 24 monaten . 
their well known high incidence of distant metastases [ 1 , 11 , 22 ] makes the simultaneous radio - chemotherapy the treatment of choice for those tumors [ 1 , 22 ]  . 
 patients and methods from 1 august 1990 to 1 october 1998 , a total of 139 consecutive patients with carcinoma of the oropharynx were prospectively evaluated for a radical external beam radiotherapy and had a regular follow - up by clinical examination and imaging . 
the latter was performed in 113 / 139 ( 81% ) patients and 3 patients were diagnosed with an additional malignancy : 1 t1n0 non - small - cell lung cancer , 1 carcinoma in situ of the lung and 1 t1 hypopharynx carcinoma . 
in 29 patients the radiotherapy was accompanied by a simultaneous chemotherapy with cisplatin , 20 mg / m2 5 - fu , 1 , 000 mg / m2 , daily day 1 to 5 and day 29 to 33 . 
 a radical neck dissection was planned for n + patients who had a complete remission of their primary tumors 4 to 6 weeks after the end of radiotherapy and in whom mri and / or clinical examination assumed a tumor rest in the cervical lymph nodes . 
twenty - four out of the 139 patients ( 17% ) did not reach a clinically complete remission at the end of the radiotherapy ( figure 1 ) , and all of them had a tumor progression . 
 all patients were prepared for a megavoltage radiotherapy by thermoplast mask , planning ct , 2d respectively 3d based planning , control by simulator and by portal vision imaging device . 
the median of the total dose delivered was 74 gy ( 64 to 80.5 ) related to the icru - point . total total concomitant chemotherapy was part of the treatment concept for patients with t3 / t4 tumor categories who were medically eligible for cisplatin - based chemotherapy and did not table 1 . 
carcinoma of the oropharynx women smoker nonsmoker alcohol + / alcohol + + age < 57 age > / = 57 t1 + 2 t3 + 4 time ( months ) figure 1 . 
fernmetastasen in abhngigkeit vom behandlungsergebnis und von univariat signifikanten parametern der lokoregionren kontrolle ( * p < 0 , 0026 )  . success failure distant metastases table 2 lists our investigated clinical parameters of influence for locoregional tumor control . 
the parameter with the strongest predictive value for locoregional tumor control was the clinical sign of reflex - otalgia [ 5 ] , p < 0.0078 , followed by predominant pattern of tumor growth , p < 0.012 , smoking habits , p < 0.0285 , and the t - category , p < 0.03. median time to evidence of distant metastases in patients with uncontrolled local tumor was 290 days . 
lokoregionre behandlungsergebnisse und lokalisation der fernmetastasen . causes of death death , all tumor intercurrent 2nd tumor success 26 / 77 4 / 26 14 / 26 8 / 26 failure 43 / 62 39 / 43 3 / 43 1 / 43 table 5 . 
the figures 1 , 3 , and 4 show the different courses of overall survival ( p < 0.01 ) ( figure 3 ) , of disease specific survival ( p < 0.001 ) ( figure 4 ) , and of disease free survival ( p < 0.0001 ) ( figure 1 ) , and in regard to the treatment result ; local control shows a plateau after 2 years . 
 discussion from 1 august 1990 to 1 october 1998 , we treated in a prospective study 139 patients with oropharyngeal carcinomas by radical radiotherapy and a conceptional neck dissection for patients in whom 4 to 6 weeks after the end of the radiotherapy there were indications of tumor rest in cervical lymph nodes either by clinical examination or by imaging techniques . 
 we began our prospective study of oropharyngeal carcinomas in order to evaluate the predictive power of the concomitant clinical symptom of the reflex - otalgia for locoregional tumor control by radical radiotherapy [ 5 ]  . 
in the present univariate analysis , reflex - otalgia still remains our most important parameter for local tumor control ( table 2 )  . further predictive factors for local control , regional control and survival in oropharyngeal carcinomas have been evaluated in some retrospective studies [ 2 , 15 ]  . 
in all these studies including our own prospective analysis tumor size and t - category ( t1 + 2 vs t3 + 4 ) , respectively , are an undisputed prognostic parameter . 
in regard to localization and n - category , the results are equivocal ; as in our study group , other authors confirmed that the probability for local control did not depend on the presence of clinically manifest nodal disease at presentation [ 6 , 10 ]  . 
 in expansion of our study , the predictive parameters for locoregional control are of eminent prognostic impact because the incapability of radical radiotherapy to control oropharyngeal carcinomas proves to be a significant parameter for the probability of the occurrence of distant metastases ( table 3 )  . 
this interdependence of the locoregional tumor control and the probability of occurrence of distant metastases after radical radiotherapy was up to now presented in only 1 detailed study [ 15 ]  . 
in this retrospective study , the authors analyzed the effect of local control on the development of distant metastases in 2 , 648 patients with carcinomas of the head and neck . 
whereas no connection was demonstrated for nasoand hypopharyngeal carcinomas between local regional control and frequency of distant metastases , this interdependence could be established for the other subsites of the head and neck cancers . 
the authors conclude that the improvement of locoregional control might result in higher survival rates and speculate that treatment related factors leading to locoregional tumor control appear to be more powerful in affecting the metastatic outcome than the presence of micrometastatic disease before the diagnosis is established . contrary to the analysis of the patients in the rtog database [ 15 ] , we included in our prospective study to determine the impact of locoregional control for the probability of the occurrence of distant metastases also those 24 patients out of 139 who did not obtain a complete remission after radical therapy and who all died within 17 months of the start of the treatment . 
we found distant metastases in 14 out of 62 ( 23% ) patients with uncontrolled locoregional tumor , predominantly in the lung , as reported by other authors [ 25 ]  . 
in contrast , only 4 out of 77 patients ( 5% ) who were locoregionally cured were found to have distant metastases ( p < 0.0026 , table 3 )  . 
the 4 metastases of locoregionally cured patients were established at a time when 63% of patients with locoregionally uncontrolled tumor had already died because of their disease ( figures 2 and 4 )  . 
the small difference in the rate of distant metastases between the categories t1 + 2 and t3 + 4 in case of failure of the radiotherapy could probably be explained by the earlier death of patients with the higher t - categories ( table 3 )  . the same may hold true for the number of metastases in case of failure for patients with reflex - otalgia ( table 3 )  . 
 [ 15 ] assume in their analysis of the frequency of distant metastases in uncontrolled tumors of the oropharynx that those metastases are the consequence of radiotherapy treatment failure and deduct the assumption that the incidence of distant metastases could be lowered by a better locoregional control . however , the literature published up to date of more aggressive radiotherapy for head and neck carcinomas , including oropharyngeal carcinomas , cannot support this hypothesis . non - randomized studies of simultaneous radio - chemotherapy [ 9 , 13 ] report on similar rates of distant metastases in locoregionally controlled and uncontrolled patients and particularly they report the same frequency of distant metastases as in our patients with uncontrolled tumors . 
the randomized studies to evaluate a concomitant 5 - fu + / - ddp chemotherapy [ 7 , 9 , 13 , 14 , 16 , 17 , 23 , 24 ] all refer to significant higher locoregional control rates , but none of them reports a lower occurrence of distant metastases . 
in regard to a lower rate of distant metastases while trying to improve locoregional control the attempts at maximal acceleration were equally without success [ 8 ]  . we have to assume that the failure of locoregional control after radical radiotherapy characterizes the aggressivity of oropharyngeal carcinomas which is stimulated by biological parameters of tumor growth leading to a significantly higher rate of distant metastases in locally not controlled tumors at a time when the therapy for locoregional control has not begun yet . 
the present available chemotherapy substances can , in combination with radiotherapy , improve the locoregional cure rate ; however , they are still lacking the proof to influence distant metastases . 
 strahlentherapie und onkologie urban & vogel 2000 originalarbeit strahlentherapie von lymphfisteln und lymphozelen burkhard neu1 , gnter gauss1 , wulf haase1 , janine dentz2 , klaus jrgen husfeldt2 hintergrund : die behandlung von sezernierenden lymphfisteln oder von retinierenden lymphozelen im narbenbereich nach operativen eingriffen stellt im klinischen alltag oft ein problem dar . 
wir untersuchten , ob eine niedrigdosierte perkutane strahlentherapie eine behandlungsalternative fr lymphfisteln / lymphozelen neben einer konservativen und operativen therapie darstellen kann . patienten und methode : in unserer klinik wurden im zeitraum von 1989 bis 1998 29 patienten mit sezernierenden lymphfisteln bzw . 
die fraktionierung betrug 4bis 5mal 1 , 0 gy / woche , und die gesamtdosen lagen im bereich von 3 bis maximal 12 gy . ergebnisse : bei 27 von 28 auswertbaren patienten konnte die fistel bzw . 
im rahmen einer lymphfistelbehandlung kann die bestrahlung nach einer erfolglosen oder anstelle einer langwierigen konservativen therapie eingesetzt werden und ist eine alternative zu einer operativen behandlung . schlsselwrter : lymphfistel lymphozele perkutane bestrahlung radiotherapy of lymphatic fistulas and lymphoceles background : the treatment of persistent postoperative lymphatic fistulas or lymphoceles is often a probleapproximately 2% of patients will develop lymphatic fistula after vascular surgery . 
we studied low - dose percutaneous radiotherapy to be used as an alternative treatment in addition to conservative or surgical therapy . patients and methods : between 1989 and 1998 29 patients ( 25 with lymphatic fistulas , 4 with lymphoceles ) received radiation therapy . 
in all patients the fractionation was 4to 5 1.0 gy / week and the dose ranged from 3 to 12 gy depending upon the onset of the radiation therapy effect . results : in 27 of 28 evaluable patients a complete disappearance of the fistula or lymphocele was achieved by radiation during therapy or shortly afterwards . 
man unterscheidet primre lymphfisteln / lymphozelen , die durch embryonale fehlentwicklungen angeboren vorkommen [ 13 ] , von sekundren lymphfisteln / lymphozelen , welche insbesondere nach lymphadenektomien im becken oder retroperitoneum oder nach gefoperationen auftreten . in der literatur wird das auftreten von lymphatischen komplikationen nach operativen eingriffen mit unterschiedlicher hufigkeit angegeben ( tabelle 1 )  . bei gefchirurgischen operationen schwankt die inzidenz von 0 , 5 bis 8 , 1% , abhngig vom ort des eingriffs . 
in der leiste , dem ort der meisten gefchirurgischen eingriffe , zeigt sich eine lymphfistel oder lymphozele als komplikation mit einer inzidenz von durchschnittlich 2% [ 15 , 21 ]  . 
bei diesen patienten besteht durch die anhaltende feuchte sekretion die gefahr einer wundinfektion ( 25 bis 30% der flle ) mit gefhrdung der prothese [ 15 , 28 ]  . 
auch bei vensen ulzera ist bei einer begleitenden lymphsekretion eine spontanheilung kaum zu erreichen [ 4 ]  . folgende therapeutischen mglichkeiten bestehen : als prventive manahmen kommen die anwendung schonender chirurgischer techniken [ 20 ] und der prophylaktische einsatz von fibrinklebern in frage [ 32 ]  . 
diese manahmen auftreten von lymphfisteln / lymphozelen nach gefoperationen , vor allem bypass - prothesen ( inzidenz 0 , 58 , 1% ) [ 28 ] lymphadenektomien ( zervikal , axillr , retroperitoneal , inguinal ) [ 13 ] gynkologischen operationen ( inzidenz 525% ) [ 13 ] urologischen operationen ( radikalen prostatektomien , inzidenz bis 8 , 5% [ 31 ] , hodenoperationen , nephrektomien , nierentransplantationen , inzidenz bis 17 , 3% [ 18 ] ) venenentnahmen ( inzidenz bis 0 , 8% ) [ 2 ] perkutanen transendoluminalen angioplastien ( pta ) [ 23 ] intraaortalen ballongegenpulsationen ( inzidenz bis 2 , 8% ) [ 1 ] sind insbesondere bei gefchirurgischen patienten indiziert und erfolgen im falle einer lymphfistel immer stationr . 
 [ 13 ] beschrieben eine komplette rckbildung einer axillren lymphozele 14 tage nach punktion der zyste mit anschlieender injektion von 4 mci des b - strahlers yttrium - 90 als kolloid . 
zur besseren identifizierung der austrittsstelle wird isosulfanblau oder methylenblau intradermal injiziert [ 21 ]  . bei lymphozelen kann die klassische marsupialisation angewandt werden [ 13 ] , bei retroperitonealen lymphozelen auch in laparoskopischer technik [ 11 ]  . perkutane bestrahlungen von lymphfisteln / lymphozelen sind in der literatur nur sprlich beschrieben worden . 
 erfahrungen mit der bestrahlung von fisteln der unterschiedlichsten genese bestehen aus den anfngen der strahlentherapie lediglich in form von entzndungsbestrahlungen [ 19 ]  . grundlegende pathomorphologische erkenntnisse ber das verhalten von lymphgefen unter einer kobaltbestrahlung liegen von van den brenk [ 29 ] aus dem jahre 1957 anhand von untersuchungen am kaninchenohr vor . 
 croft [ 3 ] berichtete 1978 ber einen patienten , der nach 27tgiger erfolgloser konservativer therapie perkutan in einer fraktionierung von 5mal 3 , 0 gy / woche bis zu einer gesamtdosis von 15 gy bestrahlt wurde . 
 [ 13 ] beschrieben die erfolgreiche behandlung von sechs patienten mit retroperitonealen oder femoralen lymphozelen mit perkutaner radiatio mit einer gesamtdosis von 20 gy ( 5mal 2 gy / woche )  . 
analog wird von makoski [ 16 ] dieses bestrahlungskonzept auch fr lymphfisteln empfohlen . mit dieser arbeit soll der frage nachgegangen werden , was die perkutane bestrahlung zu leisten vermag , welchen stellenwert sie im rahmen der therapiemglichkeiten einnehmen kann und wie ein mgliches bestrahlungskonzept aussehen sollte . 
vor bestrahlungsbeginn mu eine floride bakterielle entzndung im bestrahlungsgebiet ausgeschlossen werden , andernfalls ist nach abstrichdiagnostik eine sofortige antibiotische therapie einzuleiten . bestrahlt wurde mit einem elektronenstehfeld , das die lymphfistel mit einem allseitigen sicherheitsabstand von 4 cm umfate und am linearbeschleuniger direkt eingestellt wurde . 
 bei zwei patienten mit einer uerlich palpablen lymphozele trat diese in einem fall durch eine venenentnahme am unterschenkel zur koronaren bypass - operation , im anderen fall durch eine goretex - prothesen - implantation im bereich der arteria profunda femoris auf . 
in 24 fllen hatte ein operativer eingriff stattgefunden : bei 13 patienten eine bypass - operation mit einer gefrekonstruktion ( goretexprothesen ) , bei vier patienten eine arterielle thrombektomie , teilweise mit venenpatchplastik , bei einem patienten eine hmatomausrumung bei zustand nach arterieller lysetherapie , bei sechs patienten vense operative eingriffe , davon viermal eine vense thrombektomie , bei zwei patienten eine venenentnahme . 19 der 29 patienten litten an einer arteriellen verschlukrankheit im stadium iib bis iv und wiesen das typische risikoprofil ( diabetes mellitus , hypertonie , hypercholesterinmie , rauchen ) auf . die zuweisung der patienten erfolgte in der regel 17 tage nach dem operativen eingriff . 
 die bestrahlungsfelder lagen in 17 fllen im bereich der rechten oder linken leiste , siebenmal im oberschenkelbereich , dreimal am unterschenkel und in zwei fllen retroperitoneal . bestehen unsicherheiten , ob es sich wirklich um eine lymphsekretion handelt , kann eine triglyceridbestimmung in der austretenden flssigkeit vorgenommen werden . 
lymphe gefbypass - operation gefbypass - operation ( 14 ) thrombektomie ( vens ) thrombektomie ( vens ) ( 4 ) thrombendarteriektomie thrombendarteriektomie ( 4 ) venenentnahme venenentnahme ( 3 ) nephrektomie nephrektomie ( 2 ) trauma trauma ( 1 ) hmatomausrumung ( leiste ) hmatomausrumung ( leiste ) ( 1 ) abbildung 1 . 
example of 3d - planning of a retroperitoneal radiation field . behandlung stehenden patienten wurde anhand eines versandten fragebogens durchgefhrt . ergebnisse 28 der 29 patienten waren auswertbar ( ein therapieabbruch wegen initialer wundinfektion )  . 
die fisteln heilten in den folgenden tagen ab , in der mehrzahl der flle ( zwlf patienten ) innerhalb von 30 tagen , im schnitt zwei wochen nach ende der radiatio . 
hohe gesamtdosen implizielymphflu sisitierte unter bestrahlung sistierte unter bestrahlung ( 12 ) sisitierte innerhalb von 30 tagen sistierte innerhalb von 30 tagen ( 12 ) sisitierte innerhalb von 60 tagen sistierte innerhalb von 60 tagen ( 3 ) sisitierte nicht , re - op sistierte nicht , re - op ( 1 ) diskussion ren nicht automatisch ein besseres therapieergebnis . 
deswegen sind individuelle behandlungskonzepte bei tglicher rztlicher kontrolle des patienten notwendig . die fraktionierung , ob 4mal oder 5mal pro woche 1 gy appliziert wurde , hatte keinen einflu auf den bestrahlungserfolg . das therapieergebnis war nicht vom zeitpunkt des bestrahlungsbeginns abhngig . 
patients therapy results related to total doses . lymphflu sistierte unter bestrahlung sistierte innerhalb von 30 tagen sistierte innerhalb von 60 tagen sistierte nicht , re - op total dose gy gesamtdosis ( gy ) nachbarschaft zur lymphaustrittsstelle auf der haut . 
 zwar war die hhe der verwendeten elektronenenergie nicht entscheidend fr einen raschen therapieerfolg drei patienten , die 7 mev erhielten , schnitten nicht schlechter ab als patienten , welche mit hherer energie bestrahlt wurden , aber eine optimierung der bestrahlung wre sicherlich durch lokalisation der leckagestelle und eine tiefenmessung mit entsprechender anpassung der feldgre und energie mglich . wann mit der bestrahlung bei einer lymphfistel begonnen wird , hat zwar keinen einflu auf den therapieerfolg , das heit , auch bei spt zugewiesenen patienten knnen gute therapieergebnisse erzielt werden , aber eine frhzeitige zuweisung verringert die kosten . 
bei der bestrahlung zur ossifikationsprophylaxe wurde in den 90er jahren die gesamtdosis von initial 20 gy um etwa die hlfte reduziert , da damit gleiche behandlungserfolge zu erzielen waren [ 16 ]  . 
aus in - vitro - experimenten wei man , da bei einer niedrigdosierten bestrahlung vielfltige prozesse auftreten knnen , die sich deutlich von vorgngen bei einer bestrahlung maligner tumoren unterscheiden . 
in - vitro - experimente an huvec - endothelzellen ( human umbilical vein endothelial cells ) konnten zeigen , da adhsionen von monozyten und lymphozyten an endothelzellen nach komplizierten stufenschemata ablaufen [ 5 ]  . 
die eingewanderten leukozyten und monozyten knnten neben ihrer antientzndlichen reaktion aber auch an einer stickstoffmonoxid - ( no - ) freisetzung beteiligt se respiratorischen seit nunmehr zehn jahren gewinnt die stickstoffmonoxidforschung in der regulation des gefsystems zunehmend an bedeutung , wie auch die verleihung des medizinnobelpreises 1998 ( ferid murad , houston : no as a signalling molecule in the cardiovascular system ) verdeutlicht . 
bei der erforschung der akuten insuffizienz ( ards = adult respiratory distress syndrome ) zeigte sich , da inhaliertes no in der lage ist , den lymphflu in einer geschdigten lunge durch einen herabgesetzten mikrovaskulren filtrationsdruck zu senken [ 6 , 10 ]  . 
durch zytokine kann in glatten muskelzellen , fibroblasten , neutrophilen granulozyten und makrophagen eine induktion eines ansonsten inaktivierten nos - gens ( nos2 ) bewirkt werden und zu autokrin gebildetem no fhren [ 22 ]  . 
ohne bewiesene neue erkenntnisse sollte auch die positive wirkung einer bestrahlung auf sezernierende lymphfisteln als ein kompliziertes , noch nicht eindeutig geklrtes zusammenspiel von ( anti - ) proliferativen , antientzndlichen und ( anti - ) permeablen wirkungen aufgefat werden . 
allal1 , may monney2 , anna rosset2 , mahmut ozsahin2 , clare guillemin3 background : accelerated radiotherapy delivery has recently been shown to be effective in overcoming repopulation during fractionated radiotherapy . 
thirty - six ( 49% ) patients received induction chemotherapy ( median 3 cycles , range 1 to 4 cycles )  . results : grade 3 or 4 ( rtog ) confluent mucositis was observed in 57 patients ( 77% ) and grade 3 dysphagia in 33 patients ( 44% )  . 
the 5 - year overall actuarial survival was 32% ( 95% ci : 18 to 46 )  . induction chemotherapy was not associated with a more favorable outcome . conclusions : this study demonstrates the feasibility of this schedule in a multicenter setting . 
the oncologic results appear similar to those obtained by other accelerated regimens , while the rate of late complications seems acceptable . five - week accelerated regimens warrant further evaluation , particularly in conjunction with concomitant chemotherapy , in the framework of prospective trials . key - words : accelerated radiotherapy chemotherapy head and neck cancer originalplan einer akzelerierten radiotherapie bei kopf - hals - tumoren stadium iii bis iv . 
das verhltnis zwischen therapeutischem effekt und toxizitt drfte fr fnfwchige schemen besonders gnstig sediese arbeit berichtet ber durchfhrbarkeit und ergebnisse eines bestimmten akzelerierten programms bei karzinomen im otorhinolaryngobereich in einem multizentrischen rahmen . patienten und methode : 74 patienten mit otorhinolaryngokarzinomen in den stadien iii ( 26 patienten ) oder iv ( 48 patienten ) wurden mittels eines fnfwchigen akzelerierten schemas ( 69 , 6 bis 69 , 8 gy in 41 bis 40 fraktionen ber 35 bis 36 tage ) behandelt . 
die therapie begann mit 20 gy in zehn tglichen sitzungen auf die ursprnglich befallenen regionen , gefolgt von einer bifraktionierten bestrahlung ( 2 1 , 6 gy bis 1 , 66 gy pro tag ) auf das grere lokoregionre volumen . 
36 patienten ( 49% ) erhielten eine induktionschemotherapie ( drei zyklen median , bereich 1 bis 4 )  . ergebnisse : eine konfluente mukositis grad 3 oder 4 ( rtog ) wurde bei 57 patienten ( 77% ) und eine dysphagie grad 3 bei 33 patienten ( 44% ) beobachtet . 
die aktuarielle lokoregionre fnf - jahres - kontrollrate betrug 56% ( 95% ci : 42 bis 71 ) , die gesamtberlebensrate 32% ( 95% ci : 18 bis 46 )  . 
accelerated radiotherapy in head and neck carcinomas t he unsatisfactory results obtained in advanced head and neck cancers using standard radiation fractionation [ 8 , 11 ] have led to the development of several innovative treatment strategies . 
while some accelerated programs proved to be ineffective or poorly tolerated and were subsequently abandoned [ 16 , 18 ] , certain other schedules seemed to be both feasible and effective [ 10 , 19 ] , thus leading to their adoption in other centers . 
in this context , we recently described [ 2 ] the feasibility and long - term results of a particular accelerated radiotherapy schedule instituted at geneva university hospital in 1985 . 
favorable clinical impressions led to its use in 2 other swiss institutions , although in geneva it has been superseded by an accelerated concomitant boost program [ 1 ]  . 
this paper reports on the pooled results from the 3 institutions in patients with stage iii to iv head and neck carcinomas . patients and methods from november 1985 through august 1996 , 74 patients with stage iii ( 26 patients ) or iv ( 48 ) head and neck carcinomas were treated at the university hospitals in geneva and lausanne , and at the cantonal radiotherapy department in sion , using the accelerated radiotherapy schedule described below . 
patients presenting with metastatic disease were not included , but some of the patients had multiple ( 4 patients ) or second head and neck primaries ( 3 patients )  . 
the supraclavicular lymph nodes generally received a dose of 45 to 50.4 gy in 25 to 28 fractions . in 81% of patients the boost was delivered by using 2 lateral opposed fields . 
the larger head and neck volume was treated with 2 opposed lateral and 1 anterior field in 82% , and in the rest by using 22 opposed or convergent fields . 
electrons of appropriate energy ( mostly 9 mev ) was used to treat the posterior neck when the cervical spinal cord was blocked . chemotherapy : thirty - six ( 49% ) patients received induction chemotherapy ( median 3 cycles , range 1 to 4 cycles )  . 
patients 58 ( 1887 ) 62 / 12 tumor location oropharynx nasopharynx larynx hypopharynx oral cavity t stage ( uicc 1987 ) n stage histology squamous cell carcinoma undifferentiated table 1 . 
patientencharakteristika. 4 ( 5% ) 9 ( 12% ) 32 ( 43% ) 29 ( 40% ) 19 ( 26% ) 17 ( 23% ) 29 ( 39% ) 9 ( 12% ) chemotherapy and the beginning of radiation therapy was 29 days ( range : 5 to 90 days )  . surgery : no patient received initial surgery to the primary tumor . 
otherwise surgery was reserved for salvage of locoregional failures . statistical methods : the actuarial local and locoregional control rates as well as overall and disease - free survival rates were calculated using the kaplan - meier method [ 9 ]  . 
the median follow - up for the surviving patients was 20 months ( range : 4 to 132 months )  . results in 7 patients radiotherapy was terminated prematurely , 2 because of non - compliance ( at doses of 26 and 36 gy ) , 2 because of acute skin reactions and 3 because of intercurrent disease ( at doses of 60 to 68 gy )  . 
in 16 cases treatment was interrupted temporarily ( median length of split : 7 days , range 1 to 40 days ) , 10 because of acute toxicity or intercurrent disease and 6 for technical reasons . 
grade 3 or 4 ( rtog - eortc ) [ 15 ] late complications were scored in 5 patients ( 10.5% ) and involved skin / soft tissue , mucosa , salivary glands , larynx , and mandible . locoregional control and survival locoregional control was unevaluable in 2 of the 74 patients treated ( 1 patient died at the end of the radiotherapy and 1 patient was lost to follow - up until her death )  . 
the apparent lack of improvement associated with the addition of induction chemotherapy may be at least in part due to its preferential use in patients with more advanced disease . discussion tumor repopulation during radiotherapy is considered to be one of the important mechanisms contributing to poor locoregional control in advanced head and neck carcinomas [ 5 , 20 ]  . 
generally , 3 categories of accelerated fractionation are currently under investigation : very accelerated continuous schedules [ 3 ] , split - course accelerated schedules [ 19 ] and concomitant boost schedules [ 1 , 10 ]  . 
these include the poor tolerability of some highly accelerated schedules [ 14 ] ; the importance of the absolute time to deliver a dose of 70 gy ; and the importance of the effective total dose to be given when a very accelerated schedule is envisioned . 
indeed , in the eortc 22851 study [ 7 ] , a significant gain in locoregional control was obtained in the accelerated arm but at the expense of an unacceptable rate of late complications grade 3 to 4 ( 52% )  . 
especially considering the lack of survival benefit , this study suggests the nonfeasibility of delivering 72 gy in an absolute time of 25 days , even if a gap of 12 to 14 days is introduced to compensate for acute toxicity . 
in the chart study [ 3 ] , a reduction in total dose allowed the administration of a very accelerated schedule without increasing late complications , but no gain was obtained in terms of locoregional control or survival . 
thus , the best compromise might very well be the 5 to 6 week accelerated regimens , since they appear to allow the administration of doses of about 70 gy without dramatically increasing the late complication rate [ 1 , 6 , 15 ]  . in this regard we recently reported the feasibility and longterm outcome of an original accelerated radiotherapy schedule developed in geneva , in which 70 gy were administered in 5 weeks [ 2 ]  . 
the results obtained in stage iii to iv patients by pooling the data from the 3 swiss institutions having had experience with this regimen confirm the previous results obtained in a more heterogeneous group of patients . 
as expected , the acute reactions were dominated by a high rate of mucositis grade 3 to 4 ( 77% ) , with 44% of patients experiencing dysphagia grade 3 . 
the rate of treatment interruption because of toxicity and intercurrent disease ( 13.5% ) appears similar to those observed with standard fractionation or with other 5 - week accelerated regimens [ 3 , 7 , 12 ]  . 
in particular , the 5 - year locoregional control obtained here ( 56% ) can be considered as satisfactory , comparable to that observed in the accelerated arms of 2 recent randomized trials ( 60% for the eortc 22851 and 45% for the chart trial )  . 
the potential importance of the latter was emphasized by 2 recent meta - analyses [ 4 , 14 ] , suggesting a beneficial effect of chemotherapy when administered concomitantly with radiotherapy . 
however , the feasibility of the concomitant administration of the 2 modalities remains to be studied , unlike with standard radiotherpy where this combination is feasible and well established [ 13 ]  . 
since acute reactions appear manageable , and the schedule is convenient to deliver , it should be considered as one of several accelerated radiotherapy programs which might merit prospective study . 
mirimanoff for their review of the manuscript . strahlentherapie und onkologie urban & vogel 2000 originalarbeit treatment of primary tracheal carcinoma the role of external and endoluminal radiotherapy wolfgang harms1 , detlev latz2 , heinrich becker3 , bernd gagel4 , felix herth3 , michael wannenmacher1 background and purpose : in a retrospective study the role of radiation therapy for the treatment of primary tracheal carcinoma was investigated . patients and methods : between 1984 and 1997 , 25 patients with primary tracheal carcinoma were treated with external beam radiotherapy ( 17 squamous - cell carcinoma [ scc ] , 8 adenoid cystic carcinoma [ acc ] , median dose scc 60 gy , acc 55 gy )  . 
persistent or progressive local disease caused complications in 5 patients ( fatal hemorrhage n = 2 , esophagotracheal fistula n = 2 , tracheal necrosis n = 1 )  . conclusion : radiation therapy is an effective treatment for primary tracheal neoplasms . 
stellenwert der perkutanen und endoluminalen strahlentherapie hintergrund und zielsetzung : in einer retrospektiven studie wurde der stellenwert der strahlentherapie im behandlungskonzept des primren trachealkarzinoms untersucht . patienten und methode : zwischen 1984 und 1997 wurden 25 patienten mit primrem trachealkarzinom perkutan bestrahlt ( 17 plattenepithelkarzinome [ scc ] , acht adenoidzystische karzinome [ acc ] , mediane dosis scc 60 gy , acc 55 gy )  . 
 - rezidiv fhrte in fnf fllen zu komplikationen ( fatale blutung n = 2 , sophagotracheale fistel n = 2 , tracheale nekrose n = 1 )  . schlufolgerung : die strahlentherapie ist eine effektive methode in der therapie trachealer neoplasien . 
there exists no general staging system and no gender predominance is known . 50% of cases account for squamous - cell carcinoma and 20% to 35% for adenoid cystic carcinoma [ 27 ]  . 
while adenoid cystic carcinoma has a tendency to arise in the upper third of the trachea , squamous - cell carcinoma has a predilection in the lower part , including the carina [ 8 ]  . 
this retrospective study investigates the role of percutaneous radiation therapy and brachytherapy in the multimodal treatment regimen for primary tracheal carcinoma . patients and methods between 1984 and 1997 , 25 patients ( 9 female , 16 male ) with primary tracheal malignancies were treated . 
in order to ensure 2 homogeneous collectives only patients with squamous - cell carcinoma ( scc , 17 patients ) and adenoid cystic carcinoma ( acc , 8 patients ) were regarded for this investigation . 
because of the different prognosis scc and acc were analyzed separately . in all patients a bronchoscopy and a ct scan were performed for histological diagnosis and for evaluation of tumor extent . 5 / 17 patients with scc ( acc 0 / 8 ) had poorly , 2 ( acc 0 / 8 ) moderately and 2 ( acc 2 / 8 ) well differentiated tumors . 
 twelve patients with scc ( 70 , 6% ) and 2 with acc ( 25% ) had a history of heavy smoking for at least 20 years . treatment ten of 17 patients with scc ( 3 / 8 acc ) were treated initially by laser coagulation or stent implantation . 
the target volume included the trachea , the paratracheal and subcarinal lymph nodes and depending on tumor localization and histology the supraclavicular lymph nodes . first , a dose of 30 gy was delivered with opposing anterior and posterior fields . 
doses above 30 gy were delivered with either 3 - field arrangements ( 16 patients ) or rotation techniques ( 8 patients ) in order to limit dose to the spinal cord . radiation treatment planning was performed with 3d or 2d computed systems ( voxelplan , mevaplan )  . 
median of percutaneous dose was 60 gy for scc with a range of 44 to 66 gy ( acc 55 gy , range 30 to 60 gy )  . an additional brachytherapy boost was carried out in 10 / 25 patients ( scc 5 / 17 , acc 5 / 8 ) with single doses ranging from 3 to 6 gy and 1 or 2 fractions per week . 
five patients received brachytherapy due to a residual tumor mass within the trachea following external beam radiotherapy ( median 50 gy , range : 46 to 50 gy ) and 5 after tumor resection and external radiotherapy with 50 gy ( median , range : 30 to 60 gy )  . 
endobronchial hdr afterloading ( gammamed ili , isotopentechnik sauerwein , haan , germany ; microselectron nucletron , veenendaal , the netherlands ) was carried out using a 192ir stepping source with a nominal 370 - gbq source activity . 
if the lumen was too small for this applicator , a 6 - french bronchus applicator ( length 1500 mm ) was used , which was inserted through a wider tube placed endoscopically before treatment . 
statistical analysis revealed a significantly better survival for patients with acc compared to patients with scc ( figure 1 , log rank test , p < 0 , 05 )  . 
all other parameters tested , like positive resection margins , mediastinal involvement , and tumor localization had no significant influence on survival . patterns of failure an excellent or good relief of clinical symptoms was achieved in 88% of the patients with scc ( 88% acc , see table 1 )  . 
the endoscopical evaluation of treatment response 6 to 12 weeks after treatment revealed a complete remission in 6 / 17 patients with scc ( 7 / 8 acc ) , a partial remission in 9 / 17 ( 1 / 8 acc ) and no change of tumor size in 2 / 17 ( 0 / 8 acc )  . 
six of them had no evidence of disease ( scc 2 , acc 4 )  . one patient with acc was alive with controlled local disease but progressive lung metastases . 
four locally controlled patients died due to intercurrent diseases . all other 13 patients died due to local recurrences ( n = 11 ) or progressive distant metastases ( n = 2 )  . complications there were no acute side effects during the bronchoscopy and catheter positioning . 
treatment of primary tracheal carcinoma complete censored complete censored squamous cell adenoid cystic complete remission partial remission or no change 12 24 48 60 72 84 96 108 120 132 12 24 48 60 72 84 96 108 120 132 time / months time / months figure 1 . 
he has had a substantial destruction of tracheal tissue before treatment due to the local recurrence , attributing to the occurrence of tracheal necrosis . three patients developed a chronic tracheitis ( rtog / eortc , grade 2 , [ 30 ] ) combined with a cicatricial stenosis of the trachea . 
one patient with a tumor that covered nearly the whole trachea developed a cicatricial tracheal stenosis combined with a cartilage necrosis ( rtog / eortc , grade 3 )  . after stent implantation this patient did well . 
another locally controlled patient developed an esophagotracheal fistula ( rtog / eortc , grade 4 ) after multiple laser treatments , resection of the bifurcation and adjuvant radiation therapy ( 55 gy ebrt , 3 times 5 gy hdr )  . 
patienten mit einer kompletten remission sechs bis zwlf wochen nach der therapie zeigten eine signifikant bessere berlebenswahrscheinlichkeit als patienten mit einer partiellen remission oder keinem therapieansprechen . tive radiation therapy is recommended [ 8 , 13 ]  . 
in this situation , radiation therapy is the primary treatment modality , although recent advances in surgical procedures have made tracheal neoplasms more amenable to surgical intervention [ 10 , 11 ]  . 
by using tracheobronchial stents immediate symptomatic treatment for obstruction and occlusion of fistulae is possible [ 4 ]  . most of the series in the literature were collected during a long period of time , and therefore variations in diagnosis and treatment methods are unavoidable . 
only patients with the histological diagnosis of squamous - cell carcinoma or adenoid cystic carcinoma were included into data analysis of the current study . dose / gy 60 < 70 70 < 85 adenoid cystic carcinoma squamous cell carcinoma all patients 1 / 10 1 / 12 2 * * / 3 < 60 1 * / 2 table 2 . 
in the literature , an exact differentiation between the histological subtypes , especially with respect to survival and failure analysis is not always consequently pursued [ 5 ]  . in the current study the histologic tumor type was a major prognostic factor for survival , which corresponds to other studies [ 22 , 31 ]  . 
in our series , patients treated with surgery followed by adjuvant radiotherapy did not have a significantly better median survival ( 83 vs 32 months , radiotherapy alone )  . 
but numbers are small and results may be biased by different operation concepts . some authors indicated a dose - response relationship for tracheal carcinoma [ 5 , 22 ]  . 
thus , only 1 patient with an esophagotracheal fistula suffered from a therapy - related grade 4 complication . there exists only few data concerning the role of brachytherapy in treatment of tracheal carcinoma . 
negative selection may be another reason for the elevated complication rate in this subgroup , since 1 patient was treated for early local recurrence with salvage brachytherapy and 3 patients had previous laser treatments . 
due to the rarity of the disease , the role of endoluminal brachytherapy in the treatment regime of tracheal neoplasms is not yet clearly defined . based on the literature and our own experience we conclude , that radical surgery followed by adjuvant radiotherapy is a potentially curative treatment . 
the optimal treatment regimen of combined percutaneous and endoluminal irradiation . strahlentherapie und onkologie urban & vogel 2000 originalarbeit effekt der 3dgegenber der 2d - bestrahlungsplanung innerhalb eines konventionellen therapieschemas fortgeschrittener bronchialkarzinome peter schraube1 , ute spahn2 , dieter oetzel3 , michael wannenmacher3 hintergrund : es wurde der einflu der 3d - bestrahlungsplanung gegenber der 2d - planung in einem blichen strahlentherapeutischen behandlungskonzept ( beginn mit ap / pa feldern , fortfhrung nach rechnerplanung ) bei nichtkleinzelligen bronchialkarzinomen untersucht . patienten und methoden : fr den rechnergeplanten anteil einer bestrahlungsserie bei einem kollektiv von 20 patienten mit lokal fortgeschrittenen bronchialkarzinomen wurden eine 2dund eine 3d - planung verglichen . 
die ergebnisse der 2d - bestrahlungsplanung wurden anschlieend nochmals 3d nachgerechnet und die mittleren dosen fr zielvolumen und risikoorgane bestimmt sowie die nebenwirkungswahrscheinlichkeiten berechnet . ergebnisse : die eingesetzten bestrahlungstechniken im hinblick auf feldanordnung und wahl von keilfiltern unterschieden sich nicht wesentlich . 
unter der randbedingung einer maximalen rckenmarksdosis von 44 gy erbrachte die 3d - planung im mittel eine leichte , aber statistisch signifikante verbesserung der zielvolumenauslastung von 2 , 1 gy bei einer angenommenen referenzpunktdosis von 50 gy . 
3d - bestrahlungsplanung , ohne sich signifikant zu unterscheiden . unter bercksichtigung der anfnglich eingestrahlten simulatorgeplanten ventrodorsalen felder verringerte sich der vorteil der 3d - planung in bezug auf zielvolumen und herz , blieb aber signifikant . 
31 , 7% war der frhzeitige einsatz einer rechnerplanung im hinblick auf das pulmonale komplikationsrisiko , wenn auch nicht signifikant nachweisbar . schlufolgerung : der vorteil der 3d - planung bei der bestrahlung lokal fortgeschrittener lungentumoren liegt vor allem in der besseren zielvolumenerfassung und fhrt dort zu einer dosissteigerung . 
 patients and methods : in 20 patients with locally advanced non - small - cell lung cancer the computer - planned part of the treatment schedule was calculated 2and 3 - dimensionally . 
further the normal tissue complications were calculated . results : under the prerequisite of 44 gy maximally allowed to the spinal cord and a dose to the reference point of 50 gy a small , but significant advantage with 2.1 gy to the target ( p = 0.004 ) and a reduction of 3.6 gy to the heart ( p = 0.05 ) was achievable for 3d rtp . 
3dgegenber der 2d - bestrahlungsplanung bei bronchialkarzinomen favorable with respect to the mean lung dose and the ntcp ( 18.7% ntcp ipsilateral lung for early onset of 3d planned radiotherapy vs 31.7% for late onset of 3d planned radiotherapy ) but not significantly measurable is the early start of the treatment by computerized rtp . conclusion : the main advantage of 3d rtp in treatment of advanced lung cancer is the better coverage of the target volume . 
sollte sich diese erwartung besttigen , knnten gerade bei erkrankungen mit hoher lokaler rezidivquote , wie dem nichtkleinzelligen bronchialkarzinom , erhhte heilungsraten mglich seallerdings gibt es bislang wenig daten darber , welche mebaren verbesserungen durch die neue bestrahlungsplanungstechnik gegenber der zweidimensionalen bestrahlungsplanung ( 2d - bpl ) in der strahlentherapie von bronchialkarzinomen zu erwarten sind [ 1 , 4 , 14 ]  . 
das modell der bronchialkarzinome erscheint zur beurteilung eines effekts der 3d - bestrahlungsplanung besonders geeignet , da im bestrahlungsplanungs - ct die risikoorganstrukturen , tumorund zielvolumen meist gut zu definieren sind . patienten und methoden fr eine vergleichende bestrahlungsplanung bei der primren bestrahlung von lungentumoren wurden die daten von patienten mit dem am hufigsten zur behandlung kommenden stadium iii ausgewhlt . 
patienten mit atelektasen oder pleuraergssen konnten somit nicht bercksichtigt werden . es handelte sich um 15 patienten mit lungentumoren stadium iiib , vier patienten mit stadium iiia und einen patienten mit postoperativen rezidiv ( drei frauen und 17 mnner )  . 
die patienten waren in gutem allgemeinzustand und hatten eine ausreichende lungenfunktion , die eine standardstrahlentherapie mit einer dosis von 60 gy auf das gesamte tumorvolumen einschlielich elektiver bestrahlung angrenzender lymphknotenstationen erlaubte . 
die strahlentherapie erfolgte so bis zu dosen zwischen 10 und 30 gy ( serie 1 )  . anschlieend wurde die behandlung auf eine 3d - geplante technik umgestellt und bis 50 gy weitergefhrt ( serie 2 )  . sofern es von der tumorkonfiguration sinnvoll erschien , wurde dann bis zur enddosis von 60 gy das behandlungsvolumen nach einem weiteren 3d - plan auf das gross tumor volume ( gtv ) reduziert ( serie 3 )  . 
3dgegenber der 2d - bestrahlungsplanung bei bronchialkarzinomen serie technik applizierte gesamtdosis [ gy ] zielvolumen n patienten ( gesamt n = 20 ) ventrodorsale simulatorgeplante stehfelder 10 30 3d - rechnergeplante 2 oder 3 feldertechnik 20 50 3d - geplanter boost summendosis tabelle 2 . 
die ct - untersuchung fr die bestrahlungsplanung erfolgte in derselben position ber einen bereich von der stimmritze bis zum recessus costodiaphragmaticus mit 10 mm schichtdicke und 15 mm schichtabstand . zielvolumenbestimmung als klinisches zielvolumen wurden die in der bildgebung nachweisbaren manifestationen von primrtumor , lymphknotenmetastasen sowie benachbarten nicht befallenen lymphknotenstationen festgelegt . 
die behandlung wurde hier ber ein separates simulatorgeplantes stehfeld fortgefhrt . 3d - geplante bestrahlungstechnik zur anwendung kamen in fnf fllen 6 mv , in 15 fllen 23 mv ultraharte rntgenstrahlen . 
bei 9 / 20 patienten erfolgte ab 50 gy eine 3d - geplante boost - bestrahlung , eingeschrnkt auf das im ct sichtbare tumorvolumen bis zu einer gesamtdosis von 60 gy . 
anschlieend wurden in diesen bildern individuelle abschirmungen vorgegeben , die im falle des einsatzes dieser planung berdosierungen am rckenmark und eine zu groe volumenbelastung der lunge und des herzens vermeiden sollten . 
zuletzt erfolgte eine rckbertragung der 2d - planung auf den datensatz im 3d - planungssystem mit auswertung von zielvolumenauslastung und belastung der risikoorgane , wobei das 3d eingezeichnete zielvolumen als referenz herangezogen wurde . 
 zustzlich wurde , um den einflu der jeweiligen planungsmethode im durchgefhrten therapieregime bewerten zu knnen , die dosisverteilung der ventrodorsalen stehfelder , ber welche die behandlung begonnen wurde , mit dem 3dbestrahlungsplanungssystem berechnet und mit dem 3dbestrahlungsplan berlagert . qualitative meparameter als meparameter fr die qualitt der bestrahlungsplne wurde die mittlere physikalische dosis zum einen fr das zielvolumen und zum anderen fr die risikoorgane ipsiund kontralaterale lunge und herz herangezogen . 
unter der voraussetzung einer ausreichend homogenen dosisverteilung ( umschlieende isodose mglichst 90% ) erscheint die mittlere dosis am anschaulichsten und wird auch in vergleichbaren arbeiten zu diesem zweck verwendet [ 4 , 8 , 14 ]  . 
zustzlich wurde fr die risikoorgane unter bercksichtigung der biologisch effektiven dosis eine komplikationswahrscheinlichkeit ntcp ( normal tissue complication probability ) ermittelt [ 15 ]  . deren berechnung basierte auf dem von lyman et al . 
erste reihe : dosisverteilung in zentralstrahlebene , zweite reihe : beams eye view ( bev ) und simulatorbilder ; in der 2d - nachplanung wurde der bev aus den simulatorbildern rekonstruiert . 
es zeigt sich , da in der 2d - planung eine ungnstigere zentralstrahlebene gewhlt wurde und die gem simulatoraufnahme konfigurierten abschirmblcke in der 3d - nachplanung zu einer unerwnschten ausblockung des zielvolumens fhrten . 
the effect can be demonstrated in the dose - volume histogram ( arrow )  . komplikationswahrscheinlichkeit zu transformieren , wurde das vier - parameter - modell von lyman et al . 
3dgegenber der 2d - bestrahlungsplanung bei bronchialkarzinomen da es sich bei der klinisch durchgefhrten behandlung um eine gemischte bestrahlungstechnik , beginnend aus ap / pa feldern , rechnergeplanter grovolumiger bestrahlung und in einzelfllen auch boost - bestrahlung , handelt , wurde zum qualitativen vergleich der planungsmethoden der auf tumorvolumen einschlielich elektiver lymphknotenstationen geplante anteil ( serie 2 ) der behandlung herangezogen . der anschaulichkeit wegen wurden diese anteile mit einer dosis von 50 gy im referenzpunkt verglichen . 
anschlieend wurde der effekt der unterschiedlichen planungstechniken nochmals in dem bis 50 gy tatschlich durchgefhrten behandlungsschema ( serie 1 und 2 ) verglichen . ergebnisse gewhlte bestrahlungstechniken bei zwlf patienten erwies sich in der 3d - bestrahlungsplanung eine isozentrische hockeystick - bestrahlungstechnik mit keilfiltern als gnstig . 
bei vier patienten wurde zur schonung des herzens eine nonkoplanare einstrahlrichtung des ventralen feldes gewhlt . lediglich bei zwei patienten ergaben sich anhand des kriteriums der 90% umschlieenden isodose unterschiedliche bestrahlungsmethoden in 2und 3d - bestrahlungsplanung . die gewhlten bestrahlungstechniken sind in tabelle 3 dargestellt . 
bei sechs patienten erfolgte je nach planungsmethode der einsatz von keilfiltern . qualitative bewertung alleinige rechnerplanung : bei isolierter betrachtung der bestrahlungstechniken der serie 2 und einer angenommenen referenzdosis von 50 gy ergab sich eine bessere zielvolumenauslastung durch die 3d - planung bei 17 der 20 patienten im hinblick auf die mittlere physikalische dosis . 
bei keinem der patienten lag die berechnete komplikationsrate ntcp hier hher als 1% . addition simulatorund rechnergesttzte planung : um den realistischen effekt in der 3d - bestrahlungsplanung in dem hier gewhlten behandlungskonzept bewerten zu knnen , wurde die kalkulation nochmals unter bercksichtigung der tatschlich erfolgten bestrahlungstechnik ( beginn ber simulatorgesttzte felder , fortsetzung nach rechnerplan ) durchgefhrt . 
3dgegenber der 2d - bestrahlungsplanung bei bronchialkarzinomen mittlere dosis ( mean dose ) [ gy ] - 10% 2d - bpl ( 2d rtp ) ipsilaterale lunge ipsilateral lung mittlere dosis ( mean dose ) [ gy ] - 10% 2d - bpl ( 2d rtp ) kontralaterale lunge contralateral lung abbildung 2 . 
der vergleichsweise geringe schonungseffekt auf die lungen drfte auf die auch in der 2d - bestrahlungsplanung eingebrachten individuellen abschirmblcke zurckzufhren se ohne die verwendung dieser individuellen abschirmung bei der 2d - bestrahlungsplanung wre ein grerer unterschied in der dosisbelastung der risikoorgane zu erwarten . soweit literaturdaten zur 3d - bestrahlungsplanung bei lungentumoren vorliegen , wird durch die methodik ein ber die benutzerfreundlichkeit und den informationsgewinn [ 7 ] hinausgehender benefit angenommen , der mglicherweise dosiseskalationen zur verbesserung der lokalen behandlungsresultate erlaubt [ 1 , 4 , 8 , 12 ]  . 
die mittlere physikalische dosis setzt sich als vergleichsmastab fr organbelastungen in den letzten jahren vermehrt durch , da die ntcp - berechnungen auf diesem wert beruhen [ 19 ]  . 
die 3d - planungen unter ausschpfung aller technischen mglichkeiten erreichten dabei die hchsten punktzahlen , hher noch als die 3d - standardplne , die in etwa der von uns durchgefhrten 2d - planung mit einer simulatorgesttzten ausblendung von risikostrukturen entsprechen . 
 [ 20 ] , die in ihrer auswertung von 14 patienten allerdings nur kasuistisch ein dosis - volumen - histogramm angaben , das eine reduktion der volumendosis am herzen von 27 auf 7% im bereich der 50% - isodose nachwies . 
mazahl war hier , anders als in der von uns durchgefhrten auswertung , der volumenanteil , der unter der verschriebenen dosis von 70 , 2 gy fr das zielvolumen bzw . 
leider machen die autoren keine angaben ber die einstellung der bestrahlungsfelder , so da nicht beurteilt werden kann , ob die 3d - geplante einstellung am patienten anwendbar gewesen wre . 
gem standardlehrbchern der strahlentherapie wird das bildgebend darstellbare tumorvolumen einschlielich der lymphabfluwege bis zu etwa 50 gy behandelt , anschlieend erfolgt eine boost - bestrahlung auf das gross tumor volume bis ca . 
in neuen anstzen wird dieses konzept verlassen , und man versucht ber die 3d - bestrahlungsplanung ausschlielich das gross tumor volume zu bestrahlen und dort die dosis zu eskalieren [ 10 , 16 ]  . 
bei den meisten der zur strahlentherapie berwiesenen patienten ist das tumorvolumen ohnehin so gro , da dosiseskalationen bis zu 80 oder 90 gy von der volumenbelastung her nicht in frage kommen . 
so bestand auch in unserem patientenkollektiv nur bei 8 / 20 patienten die mglichkeit einer boost - bestrahlung auf ein gross tumor volume . in den brigen fllen war eine verkleinerung des zu bestrahlenden volumens wegen der tumorausdehnung nicht sinnvoll . inwieweit die 3d - bestrahlungsplanung vorteile bei kleinen zielvolumina hat , wurde von mcgibney et al . 
die mittleren dosen fr das zielvolumen lassen sich durch ihren einsatz steigern , die herzbelastung sinkt , die lungenbelastung ndert sich nicht nennenswert . nach den von uns gefundenen ergebnissen und auch nach den daten aus der literatur wird durch eine 3d - bestrahlungsplanung bei primrer strahlentherapie fortgeschrittener lungentumoren eine bessere auslastung des zielvolumens erreicht . 
eine entscheidende schonung des wichtigsten risikoorgans lunge tritt jedoch gegenber einer mit individuellen abschirmblcken optimierten 2d - bestrahlungsplanung nicht eeine dosiseskalation wird daher bei patientenkollektiven mit lokoregionr fortgeschrittenen stadien mit vorsicht zu betrachten seder hauptschliche gewinn der 3d - bestrahlungsplanung wird hier in dem informationszuwachs durch die dosis - volumen - histogramme hinsichtlich der bewertung der bestrahlungsplne und abschtzung des nebenwirkungsrisikos bestehen . 
das nebenwirkungsrisiko von 9% schwerer pneumonitiden erscheint etwas gnstiger als in einem 2d geplanten patientenkollektiv der heidelberger klinik mit niedrigerer gesamtdosis [ 17 ]  . etwas gnstigere ergebnisse mit einem medianen berleben von ca . 
zwei jahren fr das stadium iii bei einer dosisverschreibung von 50 gy auf ein erweitertes und von 69 gy auf ein reduziertes zielvolumen beschrieben graham et al . [ 9 ] , wobei es sich jedoch um ein heterogenes kollektiv mit auch teilweise chemotherapierten patienten handelte . 
mittels primr 3d geplanter technik wurde eine volumenorientierte dosiseskalation auf das gross tumor volume bis zu 90 gy erreicht . ergebnisse zur tumorkontrolle liegen allerdings wegen der kurzen nachbeobachtungszeit noch nicht vor . 
bei der hier untersuchten patientenserie wurde eine rckenmarksbelastung von 40 bis 44 gy als richtlinie fr die umstellung von den simulatorgeplanten stehfeldern zu den computergeplanten feldern gewhlt , die dann , wenn mglich , nochmals fr eine ebenfalls 3d geplante boost - dosis verkleinert wurden . 
vom trend her ist hier auch eine mebare senkung der risikowahrscheinlichkeit von seiten der ipsilateralen lunge zu erwarten . die 3d - bestrahlungsplanung erleichtert unstrittig vor allem durch die option des beams eye view die planungssicherheit . 
allal1 , may monney2 , anna rosset2 , mahmut ozsahin2 , clare guillemin3 background : accelerated radiotherapy delivery has recently been shown to be effective in overcoming repopulation during fractionated radiotherapy . 
thirty - six ( 49% ) patients received induction chemotherapy ( median 3 cycles , range 1 to 4 cycles )  . results : grade 3 or 4 ( rtog ) confluent mucositis was observed in 57 patients ( 77% ) and grade 3 dysphagia in 33 patients ( 44% )  . 
the 5 - year overall actuarial survival was 32% ( 95% ci : 18 to 46 )  . induction chemotherapy was not associated with a more favorable outcome . conclusions : this study demonstrates the feasibility of this schedule in a multicenter setting . 
the oncologic results appear similar to those obtained by other accelerated regimens , while the rate of late complications seems acceptable . five - week accelerated regimens warrant further evaluation , particularly in conjunction with concomitant chemotherapy , in the framework of prospective trials . key - words : accelerated radiotherapy chemotherapy head and neck cancer originalplan einer akzelerierten radiotherapie bei kopf - hals - tumoren stadium iii bis iv . 
das verhltnis zwischen therapeutischem effekt und toxizitt drfte fr fnfwchige schemen besonders gnstig sediese arbeit berichtet ber durchfhrbarkeit und ergebnisse eines bestimmten akzelerierten programms bei karzinomen im otorhinolaryngobereich in einem multizentrischen rahmen . patienten und methode : 74 patienten mit otorhinolaryngokarzinomen in den stadien iii ( 26 patienten ) oder iv ( 48 patienten ) wurden mittels eines fnfwchigen akzelerierten schemas ( 69 , 6 bis 69 , 8 gy in 41 bis 40 fraktionen ber 35 bis 36 tage ) behandelt . 
die therapie begann mit 20 gy in zehn tglichen sitzungen auf die ursprnglich befallenen regionen , gefolgt von einer bifraktionierten bestrahlung ( 2 1 , 6 gy bis 1 , 66 gy pro tag ) auf das grere lokoregionre volumen . 
36 patienten ( 49% ) erhielten eine induktionschemotherapie ( drei zyklen median , bereich 1 bis 4 )  . ergebnisse : eine konfluente mukositis grad 3 oder 4 ( rtog ) wurde bei 57 patienten ( 77% ) und eine dysphagie grad 3 bei 33 patienten ( 44% ) beobachtet . 
die aktuarielle lokoregionre fnf - jahres - kontrollrate betrug 56% ( 95% ci : 42 bis 71 ) , die gesamtberlebensrate 32% ( 95% ci : 18 bis 46 )  . 
accelerated radiotherapy in head and neck carcinomas t he unsatisfactory results obtained in advanced head and neck cancers using standard radiation fractionation [ 8 , 11 ] have led to the development of several innovative treatment strategies . 
while some accelerated programs proved to be ineffective or poorly tolerated and were subsequently abandoned [ 16 , 18 ] , certain other schedules seemed to be both feasible and effective [ 10 , 19 ] , thus leading to their adoption in other centers . 
in this context , we recently described [ 2 ] the feasibility and long - term results of a particular accelerated radiotherapy schedule instituted at geneva university hospital in 1985 . 
favorable clinical impressions led to its use in 2 other swiss institutions , although in geneva it has been superseded by an accelerated concomitant boost program [ 1 ]  . 
this paper reports on the pooled results from the 3 institutions in patients with stage iii to iv head and neck carcinomas . patients and methods from november 1985 through august 1996 , 74 patients with stage iii ( 26 patients ) or iv ( 48 ) head and neck carcinomas were treated at the university hospitals in geneva and lausanne , and at the cantonal radiotherapy department in sion , using the accelerated radiotherapy schedule described below . 
patients presenting with metastatic disease were not included , but some of the patients had multiple ( 4 patients ) or second head and neck primaries ( 3 patients )  . 
the supraclavicular lymph nodes generally received a dose of 45 to 50.4 gy in 25 to 28 fractions . in 81% of patients the boost was delivered by using 2 lateral opposed fields . 
the larger head and neck volume was treated with 2 opposed lateral and 1 anterior field in 82% , and in the rest by using 22 opposed or convergent fields . 
electrons of appropriate energy ( mostly 9 mev ) was used to treat the posterior neck when the cervical spinal cord was blocked . chemotherapy : thirty - six ( 49% ) patients received induction chemotherapy ( median 3 cycles , range 1 to 4 cycles )  . 
patients 58 ( 1887 ) 62 / 12 tumor location oropharynx nasopharynx larynx hypopharynx oral cavity t stage ( uicc 1987 ) n stage histology squamous cell carcinoma undifferentiated table 1 . 
patientencharakteristika. 4 ( 5% ) 9 ( 12% ) 32 ( 43% ) 29 ( 40% ) 19 ( 26% ) 17 ( 23% ) 29 ( 39% ) 9 ( 12% ) chemotherapy and the beginning of radiation therapy was 29 days ( range : 5 to 90 days )  . surgery : no patient received initial surgery to the primary tumor . 
otherwise surgery was reserved for salvage of locoregional failures . statistical methods : the actuarial local and locoregional control rates as well as overall and disease - free survival rates were calculated using the kaplan - meier method [ 9 ]  . 
the median follow - up for the surviving patients was 20 months ( range : 4 to 132 months )  . results in 7 patients radiotherapy was terminated prematurely , 2 because of non - compliance ( at doses of 26 and 36 gy ) , 2 because of acute skin reactions and 3 because of intercurrent disease ( at doses of 60 to 68 gy )  . 
in 16 cases treatment was interrupted temporarily ( median length of split : 7 days , range 1 to 40 days ) , 10 because of acute toxicity or intercurrent disease and 6 for technical reasons . 
grade 3 or 4 ( rtog - eortc ) [ 15 ] late complications were scored in 5 patients ( 10.5% ) and involved skin / soft tissue , mucosa , salivary glands , larynx , and mandible . locoregional control and survival locoregional control was unevaluable in 2 of the 74 patients treated ( 1 patient died at the end of the radiotherapy and 1 patient was lost to follow - up until her death )  . 
the apparent lack of improvement associated with the addition of induction chemotherapy may be at least in part due to its preferential use in patients with more advanced disease . discussion tumor repopulation during radiotherapy is considered to be one of the important mechanisms contributing to poor locoregional control in advanced head and neck carcinomas [ 5 , 20 ]  . 
generally , 3 categories of accelerated fractionation are currently under investigation : very accelerated continuous schedules [ 3 ] , split - course accelerated schedules [ 19 ] and concomitant boost schedules [ 1 , 10 ]  . 
these include the poor tolerability of some highly accelerated schedules [ 14 ] ; the importance of the absolute time to deliver a dose of 70 gy ; and the importance of the effective total dose to be given when a very accelerated schedule is envisioned . 
indeed , in the eortc 22851 study [ 7 ] , a significant gain in locoregional control was obtained in the accelerated arm but at the expense of an unacceptable rate of late complications grade 3 to 4 ( 52% )  . 
especially considering the lack of survival benefit , this study suggests the nonfeasibility of delivering 72 gy in an absolute time of 25 days , even if a gap of 12 to 14 days is introduced to compensate for acute toxicity . 
in the chart study [ 3 ] , a reduction in total dose allowed the administration of a very accelerated schedule without increasing late complications , but no gain was obtained in terms of locoregional control or survival . 
thus , the best compromise might very well be the 5 to 6 week accelerated regimens , since they appear to allow the administration of doses of about 70 gy without dramatically increasing the late complication rate [ 1 , 6 , 15 ]  . in this regard we recently reported the feasibility and longterm outcome of an original accelerated radiotherapy schedule developed in geneva , in which 70 gy were administered in 5 weeks [ 2 ]  . 
the results obtained in stage iii to iv patients by pooling the data from the 3 swiss institutions having had experience with this regimen confirm the previous results obtained in a more heterogeneous group of patients . 
as expected , the acute reactions were dominated by a high rate of mucositis grade 3 to 4 ( 77% ) , with 44% of patients experiencing dysphagia grade 3 . 
the rate of treatment interruption because of toxicity and intercurrent disease ( 13.5% ) appears similar to those observed with standard fractionation or with other 5 - week accelerated regimens [ 3 , 7 , 12 ]  . 
in particular , the 5 - year locoregional control obtained here ( 56% ) can be considered as satisfactory , comparable to that observed in the accelerated arms of 2 recent randomized trials ( 60% for the eortc 22851 and 45% for the chart trial )  . 
the potential importance of the latter was emphasized by 2 recent meta - analyses [ 4 , 14 ] , suggesting a beneficial effect of chemotherapy when administered concomitantly with radiotherapy . 
however , the feasibility of the concomitant administration of the 2 modalities remains to be studied , unlike with standard radiotherpy where this combination is feasible and well established [ 13 ]  . 
since acute reactions appear manageable , and the schedule is convenient to deliver , it should be considered as one of several accelerated radiotherapy programs which might merit prospective study . 
mirimanoff for their review of the manuscript . strahlentherapie und onkologie urban & vogel 2000 originalarbeit carcinoma of the oropharynx : local failure as the decisive parameter for distant metastases and survival karl t . 
aebersold1 , peter zbren2 objective : how important and predicative are clinical parameters and locoregional failure after radical radiotherapy of oropharyngeal carcinomas for the probability of the occurrence of distant metastases ? patients and methods : from 1 august 1990 to 1 october 1998 , 139 patients with carcinomas of the oropharynx were treated in a prospective study by radical radiotherapy and evaluated in regard to the clinical parameters reflex - otalgia , predominant structure of tumor growth , t - category , presence of involved lymph nodes , and smoking and drinking habits . 
both groups , 62 patients with locoregional therapy failure and 77 patients with locoregionally controlled tumors , were comparable in regard to performance status ( karnofsky index ) , age , gender , tnm - categories , histological differentiation , drinking habits , pretherapeutic diagnostics , total dose ( gy ) , and number of simultaneous chemotherapy cycles . 
at this moment 81% of locoregionally controlled patients are still alive . in 14 / 62 patients ( 23% ) with locoregional failure , distant metastases were detectable against 4 / 77 ( 5% ) of locally controlled patients , p < 0.0026. 
 key words : oropharynx carcinoma radiotherapy clinical parameters local control metastases oropharynxkarzinome : fehlende lokoregionre kontrolle als entscheidender parameter fr fernmetastasen und berleben fragestellung : wie wichtig und wie aussagekrftig sind klinische parameter und lokoregionres therapieversagen nach radikaler radiotherapie von oropharynxkarzinomen fr die wahrscheinlichkeit des auftretens hmatogener metastasen ? patienten und methoden : zwischen 1 . 
1998 wurden 139 konsekutive patienten mit oropharynxkarzinomen in einer prospektiven studie mit einer radikalen radiotherapie behandelt und bezglich der klinischen parameter reflexotalgie , vorherrschende struktur des tumorwachstums , t - kategorie , lymphknotenbefall und genugewohnheiten untersucht . 
die beiden patientengruppen , 62 patienten mit lokalem therapieversagen und 77 patienten mit lokal geheiltem tumorleiden , waren vergleichbar bezglich karnofsky - index , alter , geschlecht , histologischer differenzierung , alkoholkonsum , prtherapeutischer diagnostik , gesamtdosis ( gy ) und anzahl der simultanen chemotherapiezyklen . 
die tumorkontrolle war von den parametern reflexotalgie ( p < 0 , 0078 ) , wachstumsstruktur ( p < 0 , 012 ) , t - kategorie ( p < 0 , 03 ) und rauchen ( p < 0 , 0285 ) signifikant mitbestimmt . 
carcinoma of the oropharynx wurden fernmetastasen nachgewiesen , dagegen nur bei 4 / 77 ( 5% ) der lokoregionr geheilten patienten ( p < 0 , 0026 )  . lokale kontrollwahrscheinlichkeit und fernmetastasierung , am hufigsten lungenmetastasen , erreichten ein plateau nach 24 monaten . 
their well known high incidence of distant metastases [ 1 , 11 , 22 ] makes the simultaneous radio - chemotherapy the treatment of choice for those tumors [ 1 , 22 ]  . 
 patients and methods from 1 august 1990 to 1 october 1998 , a total of 139 consecutive patients with carcinoma of the oropharynx were prospectively evaluated for a radical external beam radiotherapy and had a regular follow - up by clinical examination and imaging . 
the latter was performed in 113 / 139 ( 81% ) patients and 3 patients were diagnosed with an additional malignancy : 1 t1n0 non - small - cell lung cancer , 1 carcinoma in situ of the lung and 1 t1 hypopharynx carcinoma . 
in 29 patients the radiotherapy was accompanied by a simultaneous chemotherapy with cisplatin , 20 mg / m2 5 - fu , 1 , 000 mg / m2 , daily day 1 to 5 and day 29 to 33 . 
 a radical neck dissection was planned for n + patients who had a complete remission of their primary tumors 4 to 6 weeks after the end of radiotherapy and in whom mri and / or clinical examination assumed a tumor rest in the cervical lymph nodes . 
twenty - four out of the 139 patients ( 17% ) did not reach a clinically complete remission at the end of the radiotherapy ( figure 1 ) , and all of them had a tumor progression . 
 all patients were prepared for a megavoltage radiotherapy by thermoplast mask , planning ct , 2d respectively 3d based planning , control by simulator and by portal vision imaging device . 
the median of the total dose delivered was 74 gy ( 64 to 80.5 ) related to the icru - point . total total concomitant chemotherapy was part of the treatment concept for patients with t3 / t4 tumor categories who were medically eligible for cisplatin - based chemotherapy and did not table 1 . 
carcinoma of the oropharynx women smoker nonsmoker alcohol + / alcohol + + age < 57 age > / = 57 t1 + 2 t3 + 4 time ( months ) figure 1 . 
fernmetastasen in abhngigkeit vom behandlungsergebnis und von univariat signifikanten parametern der lokoregionren kontrolle ( * p < 0 , 0026 )  . success failure distant metastases table 2 lists our investigated clinical parameters of influence for locoregional tumor control . 
the parameter with the strongest predictive value for locoregional tumor control was the clinical sign of reflex - otalgia [ 5 ] , p < 0.0078 , followed by predominant pattern of tumor growth , p < 0.012 , smoking habits , p < 0.0285 , and the t - category , p < 0.03. median time to evidence of distant metastases in patients with uncontrolled local tumor was 290 days . 
lokoregionre behandlungsergebnisse und lokalisation der fernmetastasen . causes of death death , all tumor intercurrent 2nd tumor success 26 / 77 4 / 26 14 / 26 8 / 26 failure 43 / 62 39 / 43 3 / 43 1 / 43 table 5 . 
the figures 1 , 3 , and 4 show the different courses of overall survival ( p < 0.01 ) ( figure 3 ) , of disease specific survival ( p < 0.001 ) ( figure 4 ) , and of disease free survival ( p < 0.0001 ) ( figure 1 ) , and in regard to the treatment result ; local control shows a plateau after 2 years . 
 discussion from 1 august 1990 to 1 october 1998 , we treated in a prospective study 139 patients with oropharyngeal carcinomas by radical radiotherapy and a conceptional neck dissection for patients in whom 4 to 6 weeks after the end of the radiotherapy there were indications of tumor rest in cervical lymph nodes either by clinical examination or by imaging techniques . 
 we began our prospective study of oropharyngeal carcinomas in order to evaluate the predictive power of the concomitant clinical symptom of the reflex - otalgia for locoregional tumor control by radical radiotherapy [ 5 ]  . 
in the present univariate analysis , reflex - otalgia still remains our most important parameter for local tumor control ( table 2 )  . further predictive factors for local control , regional control and survival in oropharyngeal carcinomas have been evaluated in some retrospective studies [ 2 , 15 ]  . 
in all these studies including our own prospective analysis tumor size and t - category ( t1 + 2 vs t3 + 4 ) , respectively , are an undisputed prognostic parameter . 
in regard to localization and n - category , the results are equivocal ; as in our study group , other authors confirmed that the probability for local control did not depend on the presence of clinically manifest nodal disease at presentation [ 6 , 10 ]  . 
 in expansion of our study , the predictive parameters for locoregional control are of eminent prognostic impact because the incapability of radical radiotherapy to control oropharyngeal carcinomas proves to be a significant parameter for the probability of the occurrence of distant metastases ( table 3 )  . 
this interdependence of the locoregional tumor control and the probability of occurrence of distant metastases after radical radiotherapy was up to now presented in only 1 detailed study [ 15 ]  . 
in this retrospective study , the authors analyzed the effect of local control on the development of distant metastases in 2 , 648 patients with carcinomas of the head and neck . 
whereas no connection was demonstrated for nasoand hypopharyngeal carcinomas between local regional control and frequency of distant metastases , this interdependence could be established for the other subsites of the head and neck cancers . 
the authors conclude that the improvement of locoregional control might result in higher survival rates and speculate that treatment related factors leading to locoregional tumor control appear to be more powerful in affecting the metastatic outcome than the presence of micrometastatic disease before the diagnosis is established . contrary to the analysis of the patients in the rtog database [ 15 ] , we included in our prospective study to determine the impact of locoregional control for the probability of the occurrence of distant metastases also those 24 patients out of 139 who did not obtain a complete remission after radical therapy and who all died within 17 months of the start of the treatment . 
we found distant metastases in 14 out of 62 ( 23% ) patients with uncontrolled locoregional tumor , predominantly in the lung , as reported by other authors [ 25 ]  . 
in contrast , only 4 out of 77 patients ( 5% ) who were locoregionally cured were found to have distant metastases ( p < 0.0026 , table 3 )  . 
the 4 metastases of locoregionally cured patients were established at a time when 63% of patients with locoregionally uncontrolled tumor had already died because of their disease ( figures 2 and 4 )  . 
the small difference in the rate of distant metastases between the categories t1 + 2 and t3 + 4 in case of failure of the radiotherapy could probably be explained by the earlier death of patients with the higher t - categories ( table 3 )  . the same may hold true for the number of metastases in case of failure for patients with reflex - otalgia ( table 3 )  . 
 [ 15 ] assume in their analysis of the frequency of distant metastases in uncontrolled tumors of the oropharynx that those metastases are the consequence of radiotherapy treatment failure and deduct the assumption that the incidence of distant metastases could be lowered by a better locoregional control . however , the literature published up to date of more aggressive radiotherapy for head and neck carcinomas , including oropharyngeal carcinomas , cannot support this hypothesis . non - randomized studies of simultaneous radio - chemotherapy [ 9 , 13 ] report on similar rates of distant metastases in locoregionally controlled and uncontrolled patients and particularly they report the same frequency of distant metastases as in our patients with uncontrolled tumors . 
the randomized studies to evaluate a concomitant 5 - fu + / - ddp chemotherapy [ 7 , 9 , 13 , 14 , 16 , 17 , 23 , 24 ] all refer to significant higher locoregional control rates , but none of them reports a lower occurrence of distant metastases . 
in regard to a lower rate of distant metastases while trying to improve locoregional control the attempts at maximal acceleration were equally without success [ 8 ]  . we have to assume that the failure of locoregional control after radical radiotherapy characterizes the aggressivity of oropharyngeal carcinomas which is stimulated by biological parameters of tumor growth leading to a significantly higher rate of distant metastases in locally not controlled tumors at a time when the therapy for locoregional control has not begun yet . 
the present available chemotherapy substances can , in combination with radiotherapy , improve the locoregional cure rate ; however , they are still lacking the proof to influence distant metastases . 
 strahlentherapie und onkologie urban & vogel 2000 originalarbeit evaluation of the extension of cerebral gliomas by scintigraphy matthias weckesser1 , peter matheja1 , christian rickert2 , jan lttgen1 , stefan palkovic3 , burkhard riemann1 , werner paulus2 , hansdetlef wassmann3 , otmar schober1 background : single photon emission computed tomography ( spect ) with 201tl and 123i - - methyl tyrosine ( 123i - imt ) are routine methods for the evaluation of brain tumors . 
123i - imt transport across the blood brain barrier is mediated by an amino acid carrier , 201tl accumulation is analogous to cerebral potassium uptake . patients and methods : to determine the differences in glioma extension as shown by the 2 methods , 17 patients with malignant gliomas were included in this comparative imaging study : astrocytoma iii : n = 6 , ependymoma iii : n = 1 , oligodendroglioma iii : n = 1 , glioblastoma iv : n = 9 . 
the size of glioblastomas was shown in a comparable manner by the 2 methods ( 977 571 vs 1 , 051 588 , n = 9 , ns , p = 0.57 ) , but there were considerable regional differences between the area of 201tl uptake and amino acid retention . 
thus the differences in the delineation of areas became smaller with increasing 201tl uptake . conclusions : these preliminary data indicate that the extension of gliomas is depicted differently by the 2 methods . 
 key words : glioma scintigraphy amino acid spect blood brain barrier darstellung der ausdehnung zerebraler gliome mit szintigraphischen verfahren hintergrund : die szintigraphische darstellung der verteilung des 201thallium ( 201tl - spect ) und der aminosure 123i - - methyltyrosin ( 123i - imt - spect ) wird zur evaluierung von gliomen eingesetzt . 
ziel der studie war ein vergleich der darstellung der gliomausdehnung mit den beiden verfahren . patienten und methode : 17 patienten mit malignen gliomen wurden mit beiden verfahren untersucht ( astrozytom iii : n = 6 , ependymom iii : n = 1 , oligodendrogliom iii : n = 1 , glioblastom iv : n = 9 )  . 
in der gesamtgruppe ergab sich eine schwache , aber signifikante negative korrelation zwischen der maximalen 201tl - aufnahme einerseits und einem quotienten aus der mit 123i - imt und der mit 201tl dargestellten flche andererseits ( n = 17 , r = 0 , 49 , p < 0 , 05 , abbildung 2 )  . 
da in frheren untersuchungen gezeigt wurde , dass in den meisten fllen eine strung der blut - hirnschranke voraussetzung fr die zerebrale 201tl - akkumulation ist , kann die 123i - imt - spect mglicherweise tumoranteile darstellen , die keine vermehrte endotheliale durchlssigkeit aufweisen . 
mit steigender malignitt und zunehmender 201tl - aufnahme nehmen die genannten vorteile des 123i - imt ab . schlsselwrter : gliom szintigraphie aminosure spect blut - hirn - schranke c erebral gliomas are tumors showing an infiltrating growth which may be difficult to determine by conventional imaging methods . 
additional information is provided by functional imaging methods , which employ radiolabeled compounds associated to tumor metabolis for the determination of tumor malignancy and of the individual patients prognosis the glucose analogue 18f - fluorodeoxyglucose ( 18f - fdg ) is widely used [ 3 , 14 ]  . 
this tracer , however , suffers from the high glucose metabolism of normal gray matter and can not be recommended for the determination of tumor spread [ 31 ]  . 
using positron emission tomography ( pet ) , the amino acid 11c - methionine has been developed which is incorporated in normal brain but to a larger degree in cerebral gliomas [ 8 ]  . 
a major drawback of this compound is the short physical half life of 11c ( 20 minutes ) which restricts the use of 11c - methionine to pet centers with a cyclotron and a radiochemical laboratory . 
 in 1989 123i - - methyl tyrosine ( 123i - imt ) was introduced as a tracer for single photon emission computed tomography ( spect ) of amino acid uptake in gliomas [ 4 ]  . 
this tracer has been shown to be transported across the intact blood brain barrier by a specific transport mechanism [ 18 ] which is probably the l - carrier system [ 26 ]  . 
123i - imt shows tumor extension in a comparable manner as 11c - methionine and pet [ 19 ] and has been shown to be closely correlated to histological tumor extension in an animal model [ 20 ]  . 
123iimt has been shown to be useful in the preoperative evaluation of brain tumors [ 15 , 16 ] and in the diagnosis of tumor recurrence [ 17 ] but despite this evidence , it has not been proven that 123i - imt offers advantages in tumor delineation , when compared to imaging disturbances of the blood brain barrier . 
 another tracer which is currently used for the evaluation of brain tumors is 201tl which is an analogue of potassium [ 2 , 5 , 9 , 10 , 11 , 12 , 23 , 29 , 30 ]  . 
the absence of any cerebral 201tl uptake immediately after injection clearly indicates that the tracer is not rapidly transported across the blood brain barrier and that blood brain barrier disruptions are in most cases a prerequisite of early 201tl retention . 
in accordance to this assumption , a number of authors found 201tl accumulation with few exceptions only in tumors with a disruption of the blood brain barrier as shown by contrast - enhanced magnetic resonance or computed tomography [ 13 , 21 , 27 ]  . the aim of this study was to evaluate the performance of 201tlspect and 123i - imt - spect in delineating the extension of glioma spread . 
due to the theoretical advantages of amino acids in delineating glioma borders and to the association of 201tl to blood brain barrier leakage , we expected to find tumor parts by 123i - imt - spect which are not detected by 201tl . 
 patients and methods seventeen patients with malignant gliomas ( astrocytoma iii : n = 6 , ependymoma iii : n = 1 , oligodendroglioma iii : n = 1 , glioblastoma iv : n = 9 ) were chosen out of 43 consecutive patients referred for the differential diagnosis of space occupying brain lesions . 
201tl - spect is part of the routinely performed investigations in this context . the average age of the patients ( 13 men , 4 women ) was 59.5 years ( range : 31 to 71 years )  . 
tissue specimens were obtained by radical tumor resection in 11 and by stereotactic or open biopsy in 6 of the patients . 123i - imt - spect details of the procedure have been described previously [ 15 , 33 ]  . 
scanning was initiated 15 minutes after intravenous injection of 110 to 130 mbq 123i - imt synthesized as reported previously [ 15 ] ; 96 views were acquired during 32 minutes . 
scintigraphic evaluation of gliomas 201tl - spect imaging was started 15 minutes after intravenous injection of 70 to 80 mbq 201tl - chloride using low - energy all purpose collimators ; the acquisition parameters were identical to those described above . 
in - plane resolution of the reconstructed images was 15 mm , and slice thickness was approximately 7 mthe pixel size was identical in both investigations . data analysis both image sets were matched anatomically using a threedimensional overlay technique ( mpi - tool ; advanced tomo vision ) [ 24 , 25 ]  . 
these image sets were used for visual and quantitative analysis . to determine the extension of the tumors , the transaxial slice showing the largest tumor extension was defined on both image sets separately . 
a semiautomatic method was applied , using a principle which has been reported previously [ 32 ]  . drawing isocontour regions around a tumor with a fixed cutoff related to the magnitude of maximal tumor uptake is biased by the intensity of tumor uptake . 
this reference region was drawn in the contralateral hemisphere or , in case of midline tumors , in the anterior or posterior half of the bra the choroid plexus was not included in the reference region in the 201tl images since it may exhibit a considerable physiological uptake . 
using 201tl - spect , regions around tumors in the proximity of the skull had to be closed manually , since otherwise the complete skull would have been included in the region . 
mean and standard deviation of uptake indices and tumor extension were calculated for the respective 123i - imt and 201tl investigations both for the group of gliomas iii and the patients with gliomas iv . 
since blood brain barrier disruptions might contribute to 123i - imt - uptake , pearsons correlation coefficient was calculated to test whether differences in tumor extension decrease with increasing disturbances of the blood brain barrier as reflected by 201tl uptake . results visual analysis all tumors exhibited significant uptake of both 123i - imt and 201tl . 
anatomically matched images of 123i - imt distribution ( upper row ) and 201tl uptake ( lower row ) ( slice orientation : left : axial , middle : coronal , right : sagittal )  . 
201tl shows a larger tumor volume in this case , but the extension of 201tl uptake is concentric and the larger size may well be caused by spillover due to the higher uptake ratio in 201tl - spect as compared to 123i - imt - spect ( ratio 7.0 in 201tl - spect vs 2.3 in 123i - imt - spect )  . 
anatomisch angepasste schnittbilder der verteilung von 123i - imt ( obere reihe ) und von 201tl ( untere reihe ) ( schichtorientierung : links : axial , mitte : koronal , rechts : sagittal )  . 
in 5 / 9 patients , the extension was larger in 123i - imt - spect and in 4 / 9 , the extension was larger in 201tl - spect . the ratio between area as depicted in 123i - imt - spect and area as depicted in 201tl - spect was plotted against intensity of 201tl uptake . 
furthermore , the distribution of 123i - imt is very similar to that of 11c - methionine , which has been shown to be superior to contrast - enhanced ct in disclosing the true extension of primary brain tumors [ 19 , 22 ]  . 
since glioblastomas exhibited a higher 201tl uptake and less differences in the respective tumor sizes in the 2 scintigraphic modalities , a negative correlation of the 2 parameters was expected . 
ein quotient aus der tumorflche , die durch die 123iimt - spect ermittelt wurde , und der in der 201tl - spect ermittelten tumorausdehnung wurde gegen die maximale 201tl - aufnahme aufgetragen . 
da glioblastome eine hhere 201tl - aufnahme , aber einen geringeren unterschied in der tumorausdehnung zeigen , wurde erwartet , dass eine negative korrelation der aufgetragenen parameter zu finden ist . 
despite all this evidence , it has not been shown so far that 123i - imt is advantageous to contrast enhanced ct or mri in the definition of tumor growth . 
zusammenstellung der ergebnisse mit der maximalen 201tl - aufnahme ( 201tlmax ) , der maximalen 123i - imt - aufnahme ( imtmax ) und der jeweiligen darstellung der ausdehnung ( 201tlarea , imtarea )  . weckesser m , et al . 
scintigraphic evaluation of gliomas barrier disturbances but its uptake has been shown to correspond to contrast enhancement on ct or mri [ 13 , 21 , 27 ]  . 201tl is probably the most common spect tracer for brain tumors . 
in that study the intraoperative estimation of tumor extension was less accurate than the results of morphological imaging . hence , the estimation of tumor extension before operation and presumably before radiotherapy is of considerable clinical interest . tumor extension the detailed analysis of the distribution of the 2 tracers revealed considerable differences in the delineation of cerebral gliomas . 
moreover , the difference in tumor extension decreased with increasing 201tl uptake , which may be due to a reduction of specific amino acid carriers in the course of dedifferentiation . 
one may argue that it is not necessary to include less malignant tumor parts into the therapeutic considerations and that the additional information provided by the amino acid uptake is without relevance . 
the absent visualization of any cortical structure in 201tl - spect makes it difficult to use this method to judge upon tumor location , but the presence of 201tl uptake and its intensity is probably superior to 123i - imtspect in the determination of malignancy . limitations as discussed above cerebral uptake of 201tl is not only related to blood brain barrier disruption . 
 the methodological difference caused by the different physical properties of the 2 tracers should not affect the results presented : the resolution achieved was comparable and the tumor / background contrast was larger in 201tl . 
another important observation which underlines the different information provided by the 2 tracers is the obvious difference in tumor shape as evident in figure 1a . this preliminary study still lacks of verification of the histological tumor borders . 
in addition experimental data indicate that 123i - imt reflects tumor borders accurately [ 20 ]  . furthermore 123i - imt shows tumor extension in a comparable manner as 11c - methionine [ 19 ] which has been shown to reflect tumor extension accurately in a biopsy controlled study [ 22 ]  . 
future investigations comparing 123i - imt - spect to contrast enhanced magnetic resonance tomography and to the true histological tumor extension will show whether the information supplied by this method may become useful in the planning of irradiation or surgical treatment . 
scintigraphic evaluation of gliomas strahlentherapie und onkologie urban & vogel 2000 originalarbeit prostatakarzinom : zur problematik bei der interpretation rektaler dosis - volumen - histogramme hans geinitz1 , frank bodo zimmermann1 , ladawon narkwong1 , 2 , peter kneschaurek1 , ralf wehrmann1 , alexander kuzmany1 , michael molls1 hintergrund : dosis - volumen - histogramme ( dvh ) werden zur vorhersage und berechnung von sptnebenwirkungen verwendet . 
insbesondere die festlegung der kranialen und kaudalen rektumgrenze ist bisher nicht eindeutig geregelt . patienten und methoden : die rektalen dvh von zwlf patienten , die eine konformale strahlentherapie wegen eines prostatakarzinoms erhalten hatten , wurden analysiert . 
fr jedes der 48 dvh wurden die relativen ( v50 , v80 , v95 ) und absoluten ( av50 , av80 , av95 ) volumenfraktionen verglichen , die mehr als 50% , 80% oder 95% der referenzdosis erhielten . ergebnisse : die werte der volumenfraktionen variierten stark fr einen patienten in abhngigkeit davon , wie die obere und untere rektumgrenze gewhlt wurde . 
eine vollstndige trennung zwischen blutenden und nichtblutenden patienten wurde durch keine der volumenfraktionen erreicht . schlussfolgerung : die werte relativer und absoluter volumenfraktionen rektaler dvh variieren stark in abhngigkeit davon , wie die obere und untere rektumgrenze bei der konturierung gewhlt wird . 
eine einheitliche definition zur besseren vergleichbarkeit verschiedener kollektive wre wnschenswert . schlsselwrter : prostatakarzinom dreidimensionale konformale strahlentherapie sptnebenwirkung rektale blutung dosis - volumen - histogramm prostate cancer : problems in the interpretation of rectal dose - volume histograms background : dose - volume histograms ( dvhs ) are used for the prediction and calculation of late radiation side effects . in literature the predictive value of rectal dvhs is controversially discussed . 
in particular the cranial and caudal border of the contoured organ are not uniformly defined . patients and methods : the dvhs of 12 patients who were treated with conformal radiotherapy for prostate cancer were investigated . 
for each of the 48 dvhs the percent volume fractions ( v50 , v80 , v95 ) and absolute volume fractions ( av50 , av80 , av95 ) were calculated that received more than 50% , 80% and 95% of the reference dose . 
none of the volume fractions could totally separate bleeding from non - bleeding patients . conclusion : there is a high variability of absolute and percent volume fractions of rectal dvhs depending on how the rectal borders were defined . 
for the comparison and for the interpretation of rectal dvhs a uniform definition would be helpful . key words : prostate cancer 3 - d conformal radiation therapy late side effects rectal bleeding dose - volume histogram b ei der konformalen , dreidimensional geplanten strahlentherapie des prostakarzinoms wird eine meist allerdings geringfgige peranale blutung mit einer hufigkeit von 6 bis 40% beobachtet , wobei eine abhngigkeit von der applizierten gesamtdosis und der gre des bestrahlten volumens beschrieben wurde [ 1 , 6 , 11 , 12 , 22 , 25 ]  . arbeiten zur wertigkeit rektaler dosis - volumen - histogramme ( dvh ) bei der vorhersage peranaler blutungen liefern bisher widersprchliche ergebnisse . 
 [ 11 ] verschiedene dvh - parameter im dosisbereich zwischen 60 und 75 gy als cutoff - werte an , die zwischen patienten mit und ohne rektaler blutung nach konformaler strahlenthrapie eines prostatkarzinoms unterscheiden knnen . 
ursache hierfr kann unter anderem eine unterschiedliche konturierung des rektums sein : neben der offenen frage , welche strukturen des rektums als risikoorgan definiert werden ( rektumauenkontur , rektumwand , rektumvorderwand ) , gibt es in der literatur bisher auch noch keinen konsens darber , wie die obere und untere rektumgrenze festgelegt wird [ 1 , 8 , 11 , 13 , 17 , 23 ]  . 
in dieser arbeit mchten wir an einer kleinen , hinsichtlich des behandlungskonzeptes sehr homogenen gruppe von patienten mit prostatakarzinom erste ergebnisse zu der frage vorstellen , wie die art der rektumkonturierung die rektalen dvh - parameter beeinflusst . patienten und methoden nach konformaler strahlentherapie des prostatakarzinoms betrgt die hufigkeit nicht transfusionsbedrftiger rektaler blutungen in unserem patientenkollektiv 18% . 
die blutungen traten zwischen vier und 26 monate nach ende der therapie auf . sechs patienten ohne rektale blutung ( alter 71 bis 75 jahre ) mit einer mindestnachbeobachtungszeit von 30 monaten dienten als kontrollgruppe . 
jeder kontrollpatient wurde nach alter sowie art und schwere der begleiterkrankungen ( arterielle hypertonie , degenerative geferkrankungen ) ausgewhlt und einem patienten mit rektaler blutung und gleicher konstellation der begleiterkrankungen zugeordnet ( matched pairs )  . bestrahlungstechnik alle zwlf patienten erhielten eine dosis von 50 gy ber eine vier - felder - box auf die prostata und samenblasen mit einem anschlieenden nonkoplanaren boost auf die prostata von weiteren 20 gy , einzeldosis jeweils 2 , 0 gy ( icru 50 ) , fnf fraktionen / woche . 
um den effekt der unterschiedlichen konturierung zu untersuchen , wurden dvh mit vier verschiedenen oberen und unteren rektumgrenzen fr jeden patienten berechnet : dvh1 reichte vom anus bis zum beginn des colon sigmoideus ( dieser wurde als beginn des horizontalen verlaufs des kolons definiert )  . 
dvh3 reichte vom anus bis zu einer ebene 2 cm oberhalb der prostataobergrenze , und dvh4 erstreckte sich von einer ebene 1 , 5 cm unterhalb der prostatauntergrenze bis zum sigma ( abbildung 1 )  . 
wir untersuchten fr jedes der 48 dvh die relativen ( v50 , v80 , v95 ) und absoluten ( av50 , av80 , av95 ) volumenfraktionen , die mehr als 50% , 80% oder 95% der referenzdosis erhielten . ergebnisse die interindividuelle variabilitt sowohl fr die relativen als auch die absoluten volumenfraktionen war unabhngig von der wahl der rektumgrenzen hoch ( tabelle 1 )  . 
schematic drawing of the different upper and lower rectal borders ( dvh 1 to 4 ) utilized for the rectal dvhs of each patient . keit von der wahl der oberen und unteren rektumgrenze ( intraindividuelle variabilitt , tabelle 1 )  . der medianwie auch der mittelwert des gesamten rektumvolumens , der relativen sowie der absoluten volumenfraktionen lag fr die blutenden patienten ber dem der nichtblutenden patienten unabhngig von der wahl der rektumgrenzen . 
so trat ein v50 von mehr als 90% des rektumvolumens , ein av50 von mehr als 80 cm3 , ein av80 von mehr als 40 cm3 und ein av95 von mehr als 20 cm3 nur bei blutenden patienten auf . 
diese werte knnten als cutoff - wert dienen , sie haben aber mglicherweise aufgrund ihrer extremen lage ( nur jeweils ein bis zwei patienten lagen oberhalb ) eine nur geringe klinische relevanz . 
die maximalwerte des v80 und v95 fanden sich bei patienten der kontrollgruppe . diskussion unsere daten mit einer auswertung von 288 volumenfraktionen aus 48 rektalen dvh bei zwlf patienten zeigen eine hohe variabilitt dieser volumenfraktionen . 
die streuung zwischen den patienten ist sehr gro , und die werte fr blutende und nichtblutende patienten berschneiden sich weit . es findet sich kein cutoff - wert , der sicher zwischen beiden gruppen diskriminieren kann , unabhngig davon , welches dvh ( kraniokaudale begrenzung ) und welche volumenfraktion verwandt werden . 
andere arbeitsgruppen fanden bei der ( retrospektiven ) auswertung von dvh - parametern einer greren anzahl von patienten sogenannte dosis - volumen - kombinationen , die statistisch signifikant zwischen blutenden und nichtblutenden patienten unterscheiden knnen ( siehe unten )  . 
interpretation rektaler dosis - volumen - histogramme wurde fr das jeweilige kollektiv eine bestimmte definition der kranialen und kaudalen rektumgrenze verwandt , zwischen den arbeitsgruppen allerdings differierte die festlegung der grenzen . 
 [ 11 ] untersuchten 41 patienten , die wegen eines prostatakarzinoms mit einer kombination aus photonen und protonen bis zu einer dosis von 75 , 6 kobalt - gyquivalenten ( cge ) behandelt und mindestens vier jahre nachbeobachtet worden waren . 
lagen die dvh - parameter der patienten unterhalb einer getesteten kombination ( das heit , waren sowohl das belastete volumen als auch die dosis geringer ) , wurden sie der niedrigrisikogruppe zugeordnet . 
bei zehn von 128 getesteten dosis - volumen - kombinationen fr die rektumvorderwand ( anus 2 cm oberhalb der prostata ) zeigten sich statistisch signifikante unterschiede zwischen 14 patienten mit und 27 patienten ohne rektale blutung . problematisch an der untersuchung von hartford et al . 
die mindestnachbeobachtungszeit lag allerdings bei nur zehn monaten , so dass die hufigkeit spter effekte nur eingeschrnkt beurteilbar ist . die autoren fanden vier signifikante dosis - volumen - kombinationen fr die rektumwand ( 1 , 5 cm unterhalb der prostata querverlauf des kolons ) , die zwischen patienten mit und ohne schwere blutung ( laserbehandlung , bluttransfusionen ) unterscheiden konnten . 
es wurde auch kein zusammenhang zwischen den dvh - parametern und jeglicher rektaler sptkomplikation grad ii gefunden . in beiden studien erfolgte zustzlich zur bestrahlung der prostata eine bestrahlung des beckens . 
bisher ist nicht klar , wie sich eine bestrahlung grerer darmanteile zustzlich zu den im prostatabestrahlungsfeld erfassten rektumanteilen auf die nebenwirkungsrate am rektum auswirkt [ 24 ]  . in den studien von hartford et al . 
neben zumeist zufllig verteilten ungenauigkeiten bei der patientenlagerung [ 4 , 18 ] kommt es im verlauf der therapie aufgrund unterschiedlicher , systematisch rcklufiger fllungszustnde des rektums und der blase zu einer lagevernderung der beckenorgane relativ zum strahlenfeld [ 10 , 15 , 17 , 20 ]  . 
die in der planungs - ct ermittelte dosisbelastung des rektums spiegelt also abhngig vom ausma der organbewegung und der lagerungsungenauigkeit nur bedingt die tatschliche dosisverteilung whrend der therapie wieder . schlussfolgerungen dvh - parameter des rektums weisen in den von uns untersuchten fllen eine hohe interund intraindividuelle variabilitt auf . 
grabenbauer1 , christoph schick2 , thomas papadopoulos3 , werner hohenberger2 , rolf sauer1 purpose : in ct4 - rectal carcinoma disease - free margins often cannot be obtained by primary surgery , and even if total en bloc resection is accomplished , local failure remains high with surgery alone . 
herein we report on the curative resectability rate , acute toxicities , surgical complications , local control and 5 - year survival rates achieved with a more aggressive multimodality regimen , including preoperative radiochemotherapy . patients and methods : between 1 / 1990 and 12 / 1998 , a total of 31 patients with ct4 - rectal cancer were treated at our institution . 
six weeks after completion of radiochemotherapy , patients were reassessed for resectability . results : after preoperative radiochemotherapy , 29 / 31 patients ( 94% ) underwent surgery with curative intent . 
toxicity of radiochemotherapy occurred mainly as diarrhea ( nci - ctc grade 3 : 23% ) , dermatitis ( grade 3 : 16% ) and leucopenia ( grade 3 : 10% )  . 
with a median follow - up of 33 months , local failure after curative resection was observed in 4 patients ( 19% ) , 3 patients ( 14% ) developed distant metastases . 
the 5 - year overall survival rate for the entire group of 31 patients was 51% , following curative surgery 68% . conclusion : a combination of high - dose preoperative radiochemotherapy followed by extended surgery can achieve clear resection margins in more than 80% of patients with locally advanced ct4 rectal tumor . 
 key words : ct4 - rectal cancer preoperative radiochemotherapy properative simultane radiochemotherapie mit 5 - fluorouracil bei lokal fortgeschrittenen t4 - rektumprimrtumoren ziel : bei ct4 - rektumkarzinomen ist die lokale kontrolle und das berleben nach alleiniger operation unbefriedigend , eine primre r0 - resektion oft nicht mglich . 
wir analysierten die rate an kurativen ( r0 ) resektionen nach properativer radiochemotherapie , die toxizitt der radiochemotherapie , die chirurgische morbiditt sowie die lokale kontrolle und das fnf - jahres - gesamtberleben nach multimodaler therapie . 
sechs wochen nach radiochemotherapie erfolgte die reevaluierung der operabilitt . ergebnisse : nach properativer radiochemotherapie konnten 29 / 31 patienten ( 94% ) in kurativer intention operiert werden , bei 26 / 31 patienten ( 84% ) wurde eine radikale resektion ( r0 ) des rektumtumors erreicht , bei drei patienten verblieb mikroskopisch ein tumorrest ( r1 )  . 
 schlsselwrter : ct4 - rektumkarzinom properative radiochemotherapie a pproximately 5 to 15% of patients with rectal cancer have locally advanced disease with tumors adherent or fixed to pelvic viscera or bones at the time of initial presentation [ 23 ]  . 
even if gross en bloc resection of the tumor including adjacent organs by total pelvic exenteration is accomplished , local failure remains high with 5 - year survival rates of only 20 to 30% following surgery alone [ 5 , 15 ]  . 
given the advantage of the combination of radiotherapy and 5fu - based chemotherapy in postoperative adjuvant rectal cancer trials [ 6 , 9 , 22 ] together with its proven efficacy of tumor downstaging in the preoperative setting [ 18 ] , we designed a protocol of combined high - dose radiochemotherapy prior to extensive surgery in patients with initially irresectable rectal cancer . 
we now present an analysis of 31 patients so treated , with emphasis on regimen tolerability , resectability rate , local control and survival benefits . sacrum , the ventral and lateral borders were chosen so that the tumor region was covered by a 3 - cm margthe distal border extended to the inferior aspect of the obturator foramen . 
shielding of small bowel was routinely performed for simulation of the boost . during the 1st ( days 1 to 5 ) and 5th ( days 29 to 33 ) week of radiotherapy , 5 - fluorouracil ( 5 - fu ) was delivered concomitantly at a dose of 1000 mg / m2 / d ( maximum 1800 mg ) as 120hour continuous infusion . 
in case of severe hematologic or gastrointestinal toxicity ( nci - common toxicity criteria : grade 3 and higher ) a dose reduction ( 25 to 100% ) for the 2nd course of chemotherapy was scheduled according to the extent of toxicity . 
following complete resection , 4 cycles of postoperative maintenance chemotherapy using 5 - fu ( 500 mg / m2 / d , iv bolus on 5 consecutive days ) were applied . 
in case of incomplete resection or contraindications to resection further therapy was individually adjusted according to the patients performance - status . patients and methods patient population and eligibility criteria surgery between january 1990 and december 1998 , a total of 31 patients with locally advanced primary t4 - rectal cancer were treated at our institution . 
conversely , patients who received preoperative radiochemotherapy for clinically resectable t3 - rectal cancer as well as patients with diffuse pelvic disease or pelvic bone destruction , in which treatment was regarded as palliative , were excluded from this study . 
 radiochemotherapy radiotherapy was delivered by a linear accelerator using 6 to 10 mv photons and a 3or 4 - field technique with individually shaped portals and daily fractions of 1.8 gy on 5 consecutive days per week . 
the planning target volume was defined from ct / mri images and included all macroscopically identified disease and locoregional lymph nodes up to the level of the 5th lumbar vertebra . 
the dorsal border encompassed the six weeks after completion of radiochemotherapy , patients were reassessed for resectability by means of chest x - ray and ct / mri scan of the abdomen and pelvis . 
of patients gender ( male / female ) median age clinical stage of tumor ct4 cn0 m0 ct4 cn + m0 ct4 cn0 / + m1 adherence to adjacent organs prostate / seminal vesicles bladder sacrum uterus / vagina pelvic side wall tumor size ( largest diameter ) tumor location ( from anal verge ) < 5 cm 5 10 cm > 10 cm 0 5 cm 4 9 cm > 9 cm 25 / 6 58 ( 3088 ) years table 1 . 
if adjacent organs were found to be involved intraoperatively by clinical exploration and possibly confirmed by frozen - section pathologic evaluation , surgery was extended to partial or total resection of adjacent pelvic organs . 
the log - rank test was used for comparing survival rates between patient groups . median follow - up time was 33 months ( range 8 to 82 ) , no patient was lost to follow - up . results response to radiochemotherapy tumor shrinkage was assessed clinically and by ct / mriscan 6 weeks after completion of radiochemotherapy . 
clinical - to pathologic - stage downstaging ( ct4 ( cid : 2 ) ypt 3 ) by preoperative radiochemotherapy was achieved in 20 of 29 operated patients ( 69% ) , in 1 case no residual neoplasm ( ypt0n0 ) was seen on pathological assessment of the surgical specimen ( table 2 )  . 
prtherapeutische und histopathologische t - kategorie und lymphknotenbefall bei 29 operierten patienten . patients ( 32% ) with pretreatment indication of lymphatic spread ( cn + ) no lymph - node involvement was detected on pathological evaluation ( table 2 )  . rate of curative surgery following preoperative radiochemotherapy following preoperative radiochemotherapy , 29 of 31 patients ( 94% ) were scheduled for radical resection of their pelvic tumor . 
in 26 of 31 patients ( 84% ) a locally radical resection was finally confirmed by microscopic examination of the resected specimen . in 5 of whom , however , no attempt was made to remove distant metastases . 
thus , overall r0 - resection rate for all patients , including 8 patients with distant metastases , was 68% . involvement of resection margins ( r1 ) was detected histologically in 3 patients ( prostatic urethra : n = 1 , periosteum of sacrum : n = 1 , basal resection margin : n = 1 )  . 
preoperative radiation in rectal cancer no operation n = 2 low anterior resection n = 13 extended * resection n = 2 low anterior resection + hemihepatectomy n = 2 abdominoperineal resection n = 7 extended * abdominoperineal resection n = 4 abdominoperineal resection + wedge resection lung n = 1 total n = 31 no operation ( m1 , local r0 ) ( m1 , local r0 ) 21 ( 68% ) 3 ( 10% ) 7 ( 23% ) ( 5 m1 , 2 no operation ) table 3 . 
operationsverfahren und resektionsstatus ( * ausgedehnte chirurgische verfahren mit resektion benachbarter organe ; r0 = operation mit negativen resektions - rndern , r1 = mikroskopisch positive rnder , r2 = makroskopischer tumorrest )  . quired local extended resection of adjacent pelvic organ , including the urinary bladder in 3 , the prostate / seminal vesicles in 2 and the vagina in 1 patient , respectively . 
in 3 of 8 patients with synchronous distant metastases a complete resection of liver metastases ( n = 2 ) and of a single lung metastasis ( n = 1 ) was finally accomplished . toxicity of radiochemotherapy the various levels of treatment - related toxicity following radiochemotherapy are shown in table 4 . 
during the entire follow - up period , 1 patient developed small - bowel obstruction that was managed conservatively . surgical morbidity seven patients ( 24% ) experienced postoperative morbidity . two patients had delay in wound healing due to infection or grade 12 grade 3 grade 4 leucopenia anemia thrombocytopenia diarrhea nausea / vomiting erythema stomatitis cardiac dysfunction 20 ( 64% ) 4 ( 13% ) 2 ( 6% ) 21 ( 68% ) 11 ( 25% ) 19 ( 61% ) 1 ( 3% ) 3 ( 10% ) 7 ( 23% ) 5 ( 16% ) 1 ( 3% ) table 4 . 
no intraor postoperative deaths occurred in this series . survival and patterns of failure the 5 - year overall - survival rate for the entire group of 31 patients was 51% ( figure 2 ) , being significantly higher following curative ( r0m0 ) surgery ( 68% ) as compared to the noncuratively ( no operation / r1 / m1 ) operated group ( p = 0.0006 , figure 3 )  . 
at the last review in october 1999 ( median followup : 33 months ) local failure has occurred in 4 and distant metastases in 3 of 21 curatively operated patients , the local and distant failure rate being 19% and 14% for this group , respectively . 
of the 3 patients with r1 resection , 1 progressed locally 15 months after operation , 1 died from cardiac failure 5 months after operation with no evidence of tumor progression and 1 showed no evidence of disease at the last follow - up 12 months after surgery . 
thus , overall local failure rate for the entire population , defined as local progressive disease after no operation and r1 resection or local recurrence following r0 resection , was 26% with a distant failure rate for all patients of 26% . discussion a number of series has been published [ 3 , 12 , 19 , 28 ] in which combined preoperative radiochemotherapy has been employed for the group of patients with locally advanced and initially irresectable rectal cancer ( table 5 )  . 
overall and complete resectability rates between 79 and 100% and 62 and 94% , respectively , and overall - survival rates in the range of 69% after 3 years and 60% at 4 years have been reported . 
gesamtberleben fr patienten nach kurativer operation ( r0 / m0 : 21 patienten ) im vergleich zu patienten nach nichtradikaler operation ( r1 : drei patienten , m1 : fnf patienten , keine operation : zwei patienten )  . of what renders a tumor irresectable makes comparison between studies difficult , our present results with a resection rate of 94% ( 84% complete ) , a local failure rate of 23% ( 19% after local r0 resection ) and a 5 - year overall survival of 51% for all patients and 68% after curative surgery are comparable with these other reports . if compared to historical radiotherapy - alone series in which rates of resectability between 40 and 88% , local failure rates between 7 and 50% and 5 - year survival rates of 12 to 34% have been published [ 4 , 11 , 13 ] , all these studies suggest that combined - modality treatment with 5 - fu - based ct and radiotherapy are more effective in terms of tumor downstaging , resectability , local control and long - term survival . 
interestingly , data from the 1960s had already shown a survival advantage for patients with locally unresectable rectal cancer treated with combined radiotherapy and 5 - fu vs those treated with radiotherapy alone [ 21 ]  . 
however , the optimal doses of radiotherapy and ct as well as the type of 5 - fu administration and combination with other cytotoxic agents remain to be established . whether bolus dose or continuous infusion of 5 - fu is superior in preoperative regimens has not yet been addressed in any systematic fashion . 
mounting evidence is now arising from studies of adjuvant radiochemotherapy for rectal cancer [ 22 ] and 5 - fubased chemotherapy in metastatic disease [ 14 ] that a prolonged 5 - fu infusion might be more effective in terms of both drug cytotoxicity and optimal interaction with radiation . 
however , despite use of an infusional 5 - fu regimen with higher cumulative doses of 5 - fu and radiotherapy than in most other series , our pathologically complete response rate ( 3% vs 4 to 28% ) and degree of nodal negativity ( 45% vs 73 to 90% , not shown in table 5 ) were markedly lower than in other series . 
moreover , intense histopathological scrutiny of the resected specimen with evaluation of multiple paraffin - embedded tumor tissue blocks and at least 19 ( median 28 , range 19 to 54 ) lymph nodes might have detected residual vital tumor cells in a higher percentage . 
if evaluation of response is restricted to clinical - to pathological tumor downstaging ( ct4 ( cid : 2 ) ypt 3 ) our result of 69% is within the range of the other series ( 63 to 95% , not shown in table 5 )  . 
 as we and others have demonstrated , a clear surgical resection margin remains paramount to achieve long - term cure . to optimize tumor shrinkage prior to surgery high - dose preoperative radiotherapy up to 59 gy was combined with highdose 5 - fu ( 1000 mg / m2 / d ) in the 1st and 5th week of radiotherapy and surgery was delayed until 5 to 7 weeks after completion of radiochemotherapy . 
whether it is possible to further increase resectability and sphincter preservation by combining 5 - fu with agents such as mitomycin [ 1 ] , irinotecan [ 20 ] , cisplatin [ 26 ] or by additional regional hyperthermia [ 24 ] , needs to be investigated in further phase ii and iii studies . 
 strahlentherapie und onkologie urban & vogel 2000 originalarbeit diagnostic radiation oncology : malignant cystosarcoma phylloides peter dionysius eich1 , stefan diederich1 , hans theodor eich2 , oliver micke3 , wolfgang wagner4 background : cystosarcoma phylloides is a rare , mostly benign tumor of the breast . 
histopathology showed a cystosarcoma phylloides measuring 30 ( cid : 2 ) 25 ( cid : 2 ) 19 cm as well as lymph node metastases measuring 9.5 cdespite a r0 resection the patient developed 4 thoracic wall recurrences within 2 years . 
thus postoperative radiation therapy is indicated to prevent local recurrences . key words : cystosarcoma phylloides breast neoplasm computed tomography radiotherapy metastases diagnostische radioonkologie : malignes cystosarcoma phylloides hintergrund : das cystosarcoma phylloides ist ein seltener , meist benigner mammatumor . 
die strahlentherapie ist indiziert bei lokoregionren rezidiven und bei symptomatischen metastasen . patientin : wir berichten ber eine 54 - jhrige frau , die sich mit einer schmerzlosen schwellung der rechten brust vorstellte . 
histopathologisch ergab sich ein 30 ( cid : 2 ) 25 ( cid : 2 ) 19 cm groes cystosarcoma phylloides sowie lymphknotenmetasen von 9 , 5 c obwohl es sich um eine r0 - resektion handelte , kam es innerhalb von zwei jahren zu vier thoraxwandrezidiven . 
the lesions have been classified into benign , borderline , and malignant types [ 15 ] ; the malignant variety is contributing to approximately 25% of cases [ 11 ]  . 
despite this classification the clinical behavior in individual patients cannot be predicted , as even histologically benign tumors may lead to recurrence [ 8 ] and fatal disease [ 15 ]  . 
whereas local recurrence is commonly observed and may be expected in 28 to 46% of cases treated with local excision [ 15 ] , metastases have been estimated to occur in only 3 to 20% of cases predominantly involving lung , pleura and bone [ 3 , 4 , 1315 ]  . 
axillary lymph node metastases have been reported to be extremely rare occuring in only 1.5% [ 2 , 9 , 10 , 14 , 17 , 21 ]  . there are only a few reports in the literature regarding successful radiotherapy in cystosarcoma phylloides [ 16 ]  . 
we present a case of malignant cystosarcoma phylloides with axillary lymph node metastases , as well as chest wall , pleural and pulmonary deposits , treated with different therapeutic modalities . case report a 54 - year - old woman presented with a painless mass in the right breast . 
pathologic examination including immunohistochemistry revealed a cystosarcoma phylloides with a tumor size of 30 ( cid : 2 ) 25 ( cid : 2 ) 19 cm and 7 axillary lymph node metastases measuring up to 9.5 c immunhistology using monoclonal antibodies against cytokeratin and polyclonal antibodies against protein s 100 was negative . 
however , immunhistology for the mesenchymal marker vimentin , expressed by the mesenchymal stroma was positive . although intraoperative and histological findings suggested complete resection , a recurrent tumor with a diameter of 3 cm was found 9 months later within the surgical scar . again complete excision was performed and a recurrent cystosarcoma phylloides was confirmed histologically . 
another 3 months later a second recurrent tumor was detected which did not only involve the skin and subcutaneous tissue but also invaded the pectoralis muscle , ribs and parietal pleura . 
no distant metastases were detected at this stage . therefore , surgical resection of the tumor and chest wall was performed including part of the diaphragthe surgical defect was closed by means of synthetic mesh grahistologically , both recurrences were composed of mesenchymal tissue only . 
computed tomography did not reveal malignant deposits in the left lung or mediastinum . ultrasound of the abdomen and bone scintigraphy did not demonstrate any other lesions to suggest further metastases . as the disease appeared no longer localized , no attempt of surgical excision was made but polychemotherapy instituted . it consisted of 6 cycles of ifosfamide and adriamycin in figure 2 . 
however , 6 months after institution of chemotherapy , significant residual disease remained . six months later the recurrence of the thoracic wall as well as the pulmonary lesions progressed again ( figure 2 )  . 
therefore , the right chest wall was irradiated with a total dose of 50 gy ( 2 gy / fraction ) at a linear accelerator ( x 6 mev ) using tangential opposed fields . 
follow - up of 5 months showed no new local progression of the chest wall disease . discussion typically , cystosarcoma phylloides clinically presents as a slow growing , well defined tumor which as in the patient described may reach a considerable size [ 15 ]  . in most cases cure is possible with complete surgical excision [ 3 , 4 , 8 , 14 , 15 , 17 ]  . 
in up to 46% of patients , however , local recurrences occur , probably due to incomplete resection [ 3 , 4 , 8 , 15 , 17 ]  . 
distant metastases are rare even in large tumors and have been reported in only 5 to 20% of lesions [ 3 , 4 , 14 , 15 , 17 ]  . 
lymphatic spread to axillary lymph nodes as seen in the patient described is extremely rare and has been reported in the literature to occur in approximately 1.5% of cases [ 2 , 9 , 10 , 14 , 17 , 21 ]  . using monoclonal antibodies ae1 / ae3 and k4 gould et al . 
no data , however , is available regarding the prognosis of cystosarcoma phylloides and vimentin expression . genetical studies , as for instance comparative genom hybrid studies ( cgh - analysis ) have not been performed as yet . 
 [ 12 ] demonstrated aneuploidian in cystosarcoma phylloides tumor , although no significant correlation with tumor progress was shown . radiologically cystosarcoma phylloides presents as a soft tissue density , well defined tumor usually with a diameter of several centimeters . 
findings are similar with local recurrences and axillary lymph node metastases [ 4 , 13 ]  . publications on pulmonary metastases in cystosarcoma phylloides reported solitary [ 13 ] and multiple [ 10 , 14 , 17 , 21 ] nodules . 
in the patient described , the unilateral manifestation of pulmonary metastases in the hemithorax with previous surgery suggests not only hematogenous but also lymphatic spread as the source of pulmonary metastases . 
this assumption is further supported by the possibility that previous surgery may have led to communication of lymphatic channels of the chest wall and lung . there are only few reports in the literature concerning radiotherapy of cystosarcoma phylloides . 
in the past cystosarcoma phylloides was thought to be radioresistent [ 1 , 21 ]  . however , in some cases effective treatment has been reported [ 16 ]  . 
some authors recommend the regular use of postoperative radiotherapy in malignant phylloides tumors [ 5 ]  . in correlation to the few data in the literature , it can be stressed that cystosarcoma phylloides is a radiosensitive tumor . 
in the presented case of a recurrent chest wall tumor there was a good response to local radiotherapy , conformal radiotherapy would probably have been a treatment option for the pulmonary tumor masses . strahlentherapie und onkologie urban & vogel 2000 originalarbeit influence of apoptosis on the enhancement of radiotoxicity by ouabain frieda a . 
verheye - dua , lothar bhm1 background : the na + , k + - atpase inhibitor ouabain enhances the toxicity of irradiation and we have previously demonstrated that the drug suppresses repair capacity . 
in the pattern of dna damage responses which are influenced by ouabain we show that the g2 cell cycle delay is prolonged and that early apoptosis events are upregulated in tp53 wild type and tp53 mutant cells . 
it is concluded that apoptosis plays a significant role in the enhancement of radiotoxicity by ouabain . key words : ouabain radiotoxicity apoptosis bedeutung der apoptose bei der verstrkung der strahlentoxizitt durch ouabain hintergrund : die gegenwart des na + - k + - atpase - inhibitors ouabain erhht die strahlentoxizitt . 
die rolle der apoptose ist in diesem zusammenhang nicht bekannt und wurde hier untersucht . material und methodik : sieben humane zellinien mit bekanntem tp53 - status wurden mit 60co - - strahlen in gegenwart von ouabain bestrahlt . 
zellberleben wurde durch den koloniebildungstest , apoptose durch acridine - orangefrbung und zellzyklusnderungen mit hilfe der durchflusszytometrie untersucht . ergebnisse : die erhhung der strahlentoxizitt durch ouabain , berechnet aus dem sf2 - verhltnis gegenber kontrollen , liegt im bereich von 1 , 1 bis 2 , 8 und ist abhnging von der jeweils benutzten zelllinie . 
20 stunden nach bestrahlung bewirkt ouabain je nach zelllinie eine verstrkung der strahleninduzierten frhen apoptoseereignisse um den faktor 1 , 3 bis 1 , 7 . schlussfolgerungen : zugabe von ouabain bei der bestrahlung bewirkt eine markante erhhung der strahlentoxizitt besonders in tumorzellen , unabhngig vom tp53 - status . 
im muster der dna - schadensreaktionen zeigen wir , dass ouabain den strahleninduzierten g2 - block drastisch verlngert und die frhen apoptoseereignisse deutlich erhht , und zwar sowohl in tp53 - wildtypen als auch in tp53 - mutanten . 
apoptosis and enhancement of radiotoxicity i onfluxes in tumor cells are elevated [ 21 , 22 ] and respond strongly to na + , k + - atpase inhibition [ 33 ]  . 
we have previously demonstrated that subtoxic doses of ouabain enhance the toxicity of irradiation and that this effect appears to be selective for tumor cells [ 35 , 36 ]  . 
measurement of repair rates and repair half times furthermore demonstrated that pharmacologically acceptable doses of ouabain suppress repair capacity in tumor cells to a greater extent than in normal cells [ 36 ]  . 
since cell inactivation by irradiation leaves 2 basic response options , repair and apoptosis [ 1 , 2 , 6 ] , we have now studied the role of apoptosis . 
in this approach , we used the 3 previous cell lines a549 , hela and l132 cells , and , for reasons of their well - defined tp53 status , the 2 human melanoma lines , be11 and mewo , and the 2 squamous carcinoma cell lines , 4197 and 4451 . 
the results again highlight the differential response of normal and tumor cells to the radiosensitizing effect of ouabain and demonstrate that ouabain enhances radiation - induced apoptosis . materials and methods cell cultures , drug treatment and clonogenic survival tissue culture requirements , intrinsic cellular radiosensitivity , ouabain treatment and irradiation conditions were as previously described [ 36 ]  . 
clonogenic cell survival data were fitted to the linear - quadratic model as previously described [ 35 ] and served to derive the sf2 ( survival fraction at 2 gy )  . 
survival at the various irradiation doses was adjusted for ouabain toxicity determined in unirradiated controls ( not shown )  . cell cycle analysis perturbations in cell cycle transit after 7 gy 60coirradiation were followed by flow cytometry . 
the cell pellet was resuspended in 100 l of ice - cold pbs , 5 ml of ice - cold 70% ethanol was added vigorously and the sample was vortexed . 
the cells were excited at 488 nm and the emission was collected above 590 nm . the data were analyzed using the modfit cell cycle analysis software ( verity , topsham , me )  . 
 for analysis of dna content , fixed cells were pelleted and resuspended in 1 ml pbs / pi / rnase , composed of 17.6 ml pbs , 400 l propidium iodide ( 1 mg / ml ) and 2 ml rnase ( 1 mg / ml )  . 
the means ( sd ) are plotted . the influence of ouabain on the duration of the g2 delay was investigated by adding 10 - 7 m ouabain at the g2 maximum and sampling cells at various time points followed by flow cytometry . 
 apoptosis exponentially growing cells were trypsinized and plated ( 1 to 3 ( cid : 2 ) 104 cells per plate ) into 35 mm plastic petri dishes ( corning , new york ) containing a 22 mm glass coverslip ( chance propper , england ) to a final volume of 2 ml . 
samples taken at specified time points were fixed in a methanol - acetic acid mixture ( 3 : 1 , v / v ) , airdried and stained with acridine orange - pbs ( final concentration 0.002% ) for about 2 minutes . 
the means are plotted with the corresponding sd . results the survival data in table 1 show that the presence of 10 - 7 m ouabain , added 1 hour before irradiation and removed 3 hours after irradiation , enhances radiotoxicity in a cell - dependent manner . 
the 4197 squamous carcinoma tp53 wild type cell line and l132 normal human lung fibroblast tp53 mutant cell line undergo very little radiosensitization whereas all other cell lines show marked radiosensitization in the presence of subtoxic ouabain doses of 5 ( cid : 2 ) 10 - 8 and 10 - 7 m . enhancement ratios ( er ) calculated from the change of sf2 data indicate that the maximum enhancement ratio of 2.8 is seen in hela cells ( table 1 )  . 
it thus appears that the tp53 status is of little consequence for the ouabain response . since cell cycle delays constitute a major damage response , we assessed the influence of ouabain on the radiation - induced g2 delay . 
a dose of 7 gy produced a clear g2 phase delay between 12 and 20 hours post irradiation depending on the cell line ( figures 2a to 2h )  . when ouabain was added at these time points , the g2 delay was significantly prolonged . 
this is clear from the g2 fractions ( figures 2d , 2f and 2h ) but also from the g1 fractions as judged by the time course after irradiation ( figures 2a , 2c , 2e and 2g )  . 
in hela cells , it is shown that the g1 and g2 fractions have returned to normal 30 to 40 hours post irradiation and that presence of ouabain extends the recovery to well over 70 hours ( figures 2g and 2h )  . 
in 4451 and mewo cells , where the g2 maxima are seen later , these recovery periods are extended to 70 to 100 hours ( figures 2c to 2f )  . 
in the tp53 wild type cell lines , a549 , 4197 and be11 , the influence of ouabain on the cell cycle delays is less pronounced ( results not shown )  . 
ouabain has no effect on cell recovery in the normal lung fibroblast l132 ( figures 2a and 2b )  . the results show that ouabain has a profound delaying effect on cell recovery in tumor cells as judged by the restoration of normal cell cycle distribution . when we examined the influence of ouabain on the apoptotic propensity , we found that the apoptotic response after 7 gy is in the region of 10 to 70% , depending upon cell line and postirradiation time ( figure 3 )  . 
apoptosis was examined at 20 hours post irradiation as membrane alterations and reduced adherence to the microscope slide could underestimate the proportion of apoptotic cells at later timepoints . this could explain the sharp drop in apoptotic propensity seen at about 26 hours in a549 cells and at 45 hours in 4197 cells ( figure 3 )  . 
figure 3 shows that an irradiation dose of 7 gy 60coirradiation results in apoptotic propensity between hela 2 gy 4 gy 6 gy postirradiation time ( hrs ) postirradiation time ( hr ) figure 1 . 
in 4451 , mewo and be11 cells the apoptotic fraction is between 12 and 25% , whereas hela , a549 and 4197 demonstrate an apoptotic fraction of about 8% 20 hours post irradiation . 
figure 3 shows that presence of the drug for 4 hours ( 1 hour before and 3 hours post irradiation ) enhances the proportion of apoptotic cells by 2 to 10% depending upon cell line . 
enhancement ratios ( er apoptosis ) calculated from these data are presented in figure 4 . in view of the fact that a positive influence of ouabain as radiation adjuvant exists , we examined the relationship between ouabain - induced increase of radiotoxicity ( er irradiation ) and ouabain - induced increase of apoptotic propensity ( er apoptosis )  . 
pw and hl - 60 cells transfected with the apoptosis inhibitor bcl2 gene [ 7 , 8 , 10 , 19 , 24 ] were found to be less susceptible to ouabain - induced apoptosis [ 7 ]  . 
other data on pw cells suggest that bcl - 2 acts at the level of the na + , k + - atpase because ouabain restores radiation - induced apoptosis to control levels when the bcl - 2 gene is overexpressed and apoptosis is downregulated [ 7 , 8 ]  . 
studies on a cholestane glycoside from ornithogalum saunderisiae , which is structurally closely related to ouabain , have shown that growth inhibiting activity , evident in promyelocytic hl60 cells , t lymphocytic molt - 4 cells and mitogen stimulated human peripheral blood mononuclear cells ( pbmc ) , was promoted by calcium , which stimulates endonuclease activity required for apoptotic fragmentation of dna [ 13 , 14 ]  . 
morphine which is also structurally closely related to ouabain , induces the fas - receptor [ 38 ] which initiates apoptosis by fas ligand ( fasl ) binding [ 4 ]  . 
apoptosis and enhancement of radiotoxicity the apoptotic response upon proliferative and antiproliferative signals thus is very strong . an interesting observation which has already been reported by us previously [ 35 ] , is the finding that ouabain prolongs the irradiation - induced g2 delay ( see figure 1 )  . 
we speculate that prolongation of the g2 delay in the presence of ouabain arises from inhibition of the na + , k + - atpase and inhibition of k + influx known to be a requirement for entry into s - phase [ 27 ]  . 
the correlation between the prolonged g2 delay and enhanced apoptotic propensity in response to 10 - 7 m ouabain is also consistent with published observations showing that apoptotic levels correlate significantly with dna aneuploidy and s + g2m fractions in primary carcinomas [ 34 ]  . the cytological method employed here for apoptosis detection was chosen because it gives unambiguous results . 
es wurde eine dosis von 7 gy appliziert und die zellen ber einen zeitraum von vier stunden ( von einer stunde vor bis drei stunden nach bestrahlung ) mit ouabain inkubiert ( ( cid : 2 ) ( cid : 2 ) kontrolle , ( cid : 3 ) ( cid : 3 ) 10 - 7 m ouabain )  . 0 5 10 15 20 25 30 35 40 45 50 postirradiation time ( hrs ) 0 5 10 15 20 25 30 35 40 45 50 time ( hrs after 7 gy ) 4197 4451 0 5 10 15 20 25 30 35 40 45 50 55 postirradiation time ( hrs ) postirradiation time ( hrs ) be11 mewo postirradiation time ( hrs ) postirradiation time ( hrs ) hela 0 5 10 15 20 25 30 35 40 45 50 postirradiation time ( hrs ) figure 4 . 
this is supported by the observation that the ouabain - induced enhancement of radiotoxicity reaches 75% at 7 gy , whereas enhancement of apoptosis 20 hours post irradiation is only in the region of 10 to 20% ( see figure 3 )  . the increase of apoptotic propensities ( figure 3 ) nevertheless demonstrates that ouabain enhances apoptosis induced by irradiation . the following additional arguments would support a role of ouabain in apoptosis . 
the na + , k + - atpase maintains intrastrahlentherapie und onkologie urban & vogel 2000 originalarbeit prophylaxe der strahleninduzierten diarrh durch smektit ergebnisse einer doppelblind randomisierten , plazebokontrollierten multicenterstudie jrg hombrink1 , dietmar frhlich2 , michael glatzel2 , alfred krau2 , hans - joachim thiel3 , johann meier3 , dieter hamann4 , ralph mcke4 , felix herbert glaser5 , sabine kst5 hintergrund und ziel : strahlentherapieinduzierte diarrhen und schmerzen sind bekannte nebenwirkungen der beckenund abdominalbestrahlung und knnen in schwerwiegenden fllen zur unterbrechung der strahlenbehandlung fhren . 
die vorliegende untersuchung diente der verifizierung bekannter studienresultate und der erarbeitung einer dosis - wirkungs - beziehung . patienten und methode : zwischen april 1994 und mai 1995 wurde bei 176 patienten mit beckenbzw . 
das hauptzielkriterium der auswertung war der zeitraum bis zum auftreten einer bestrahlungsinduzierten diarrh ( definiert als 3 breiige sthle )  . ergebnisse : alle 176 patienten wurden in der intent - to - treat - analyse ausgewertet . 
 > 837 , 5 ml ( median ) deutet im kollektiv 837 , 5 ml an , dass bei gegebener dosierung ein vorteil fr smektit gegenber plazebo ( 32 versus 18 kalendertage bis zum ersten auftreten einer diarrh ) besteht ; dieser vorteil ist jedoch statistisch nicht signifikant . schlussfolgerung : durch den prophylaktischen einsatz eines smektitprparates als antidiarrhoikum whrend einer bestrahlung des beckenund abdominalbereiches kann die entstehung einer bestrahlungsinduzierten diarrh verzgert werden , eine statistische signifikanz konnte jedoch sowohl im gesamtkollektiv als auch in einer post - hoc - subgruppenanalyse nicht nachgewiesen werden . schlsselwrter : strahlentherapie diarrh prophylaxe smektit prophylaxis of irradiation - induced diarrhea with smectite . 
results of a placebo - controlled investigation purpose : diarrhea and abdominal pain are well - known side effects abdominal or pelvic of radiation therapy that may lead to interruption of treatment in serious cases . 
the presented trial aimed at the verification of earlier studies and the evaluation of a dose - effect relationship . patients and methods : between april 1994 and may 1995 , a total of 176 patients obtaining radiotherapy of the pelvis or the abdomen were evaluated in a double - blind , randomized placebo - controlled investigation regarding the prophylactic effect of smectite ( = colina ) against radiotherapy - induced diarrhea . 
during the whole period of radiotherapy 85 patients obtained 2 ( cid : 2 ) 6 g smectite daily and 91 patients received 2 ( cid : 2 ) 6 g placebo . 
the primary end point of the analysis was the time to the first appearance of diarrhea ( 3 pappy stools )  . results : all 176 patients were evaluated according to an intent - to - treat analysis . 
this benefit was statistically not significant . conclusion : prophylactic application of smectite during irradiation of the pelvis and the abdomen can delay the development of radiotherapy - induced diarrhea , a statistical significance could not be verified neither in the total study group nor in the post - hoc subgroup analysis . key words : radiotherapy diarrhea prophylaxis smectite i m rahmen der strahlentherapie abdominopelviner karzinome sind vor allem die akute und die chronische enteritis als nebenwirkungen anzusehen , die die lebensqualitt des patienten erheblich beeintrchtigen [ 1 , 7 , 9 , 12 , 13 , 15 , 17 , 22 , 23 ]  . als pathophysiologische mechanismen der radiogen induzierten diarrh gelten neben der dosisabhngigen zellatrophie , - dysplasie und zellnekrose mit konsekutiven zellverlust und denudation der villi bis hin zur dekompensation mit fortschreitender zellentblung der basalmembran [ 8 ] auch ein gestrter metabolismus im sinne einer kohlenhydratund fettstoffwechselstrung . 
proteasen der dickdarmflora knnen brstensaumenzyme direkt schdigen , und frei werdende gallensuren knnen durch die dickdarmbakterien dekonjugiert werden und so direkt toxisch auf die darmschleimhaut wirken , was ber eine gesteigerte darmmotilitt zu einer gesteigerten orozkalen transitzeit fhrt . 
das absinken der konjugierten gallensuren unter eine sogenannte kritische mizellre konzentration reduziert die fhigkeit zur mizellenbildung und bedingt eine gesteigerte fettausscheidung [ 9 , 21 ]  . kohlenhydratstoffwechselstrungen manifestieren sich in einer laktosemalabsorption , die die stuhlfrequenz beeinflusst . 
weiterhin besteht die hypothese , dass analog zur sprue durch nichtresorbierte laktose und deren osmotische wirkung die stuhlkonsistenz bis hin zum wssrigen stuhl beeinflusst wird [ 23 ]  . bisher eingesetzte therapien zur behandlung der radiogenen diarrh zielen auf eine peristaltikhemmende wirkung ( loperamid , opiumderivate ) , auf toxinabsorption ( kohle ) oder vergerbende wirkung im bereich der mukosadefekte ( tanninalbuminate ) ab . mit den mglichkeiten der modernen strahlentherapie lassen sich die nebenwirkungen und sptfolgen der bestrahlung von abdominalen , urologischen und gynkologischen tumoren deutlich verringern . aufgrund der anatomischen gegebenheiten liegen bei der bestrahlung von abdominalen , urologischen oder gynkologischen malignomen immer strahlenempfindliche organe wie die harnblase , der dnndarm und teile des kolons innerhalb des bestrahlten volumens und knnen bereits whrend der behandlung in unterschiedlichem ausma akut reagieren [ 1 , 3 , 10 , 23 , 24 , 26 ]  . 
eine effektive prophylaxe der bestrahlungsinduzierten reaktionen dieser organe ist nicht nur fr den patienten in hinblick auf seinen allgemeinzustand von klinischer bedeutung , sondern auch fr die planmige durchfhrung der strahlentherapie von therapeutischem nutzen . diesbezglich existieren neuere untersuchungen , die eine prophylaktische wirkung von smektit , einem inerten schichtsilikat , nachweisen . 
die im rahmen dieser klinischen studie verwendete substanz wird nicht resorbiert und fhrt als hauptnebenwirkung lediglich zu einer obstipation , die jedoch durch eine dosisanpassung beherrschbar ist [ 6 ]  . 
auch die autoren der vorliegenden arbeit konnten bereits in einer frheren untersuchung an patienten , die eine bestrahlung des beckenund abdominalbereiches erhielten , die antidiarrhoische wirkung von smektit bei prophylaktischer gabe nachweisen [ 25 ]  . 
auerdem sollte die frage einer dosisoptimierung dieses schichtsilikates in einer doppelblinden , randomisierten , plazebokontrollierten , multizentrischen studie nher geklrt werden . patienten und methodik von den geplanten 200 patienten wurden im rekrutierungszeitraum von april 1994 bis mai 1995 176 patienten in die studie aufgenommen und nach randomisierung einer der beiden behandlungsgruppen zugeteilt . 
ausschlusskriterien waren patienten mit zeitgleicher morphintherapie , jegliche andere zeitgleiche therapie mit motilittshemmern , adstringenzien und adsorbenzien , antacida , antibiotika und enteral wirksamen mikroorganismen , chemotherapie innerhalb der letzten zwei wochen vor bestrahlungsbeginn , kombinierte radiochemotherapie , patienten mit chronischer obstipation , schwangerschaft , stillzeit und fertile frauen ohne kontrazeption . 
in die mit smektit behandelte gruppe ( colina - gruppe ) wurden 85 patienten ( mnnlich : weiblich = 28 : 57 ) mit einem mittleren alter von 61 , 6 12 , 2 jahren aufgenommen ; die plazebogruppe bestand aus 91 patienten ( mnnlich : weiblich = 30 : 61 ) mit einem mittleren alter von 60 , 1 12 , 6 jahren . 
prophylaxe der strahleninduzierten diarrh durch smektit colina plazebo total cervix uteri corpus uteri rektumkarzinom 17 prostatakarzinom 10 lymphome andere 18 , 8 22 , 3 20 , 0 11 , 8 20 , 0 23 , 1 26 , 4 11 , 0 20 , 8 21 , 0 24 , 4 14 , 8 11 , 4 20 , 5 total 176 100 tabelle 1 . 
diagnosis. die patienten der colina - gruppe erhielten zweimal tglich jeweils 6 g smektit ( 2mal zwei beutel mit je 3 g , tagesgesamtdosis = 12 g ) , die patienten der plazebogruppe entsprechende beutel mit einer mischung aus strke , maltodextrin , glucosehydrat und na - saccharbeide medikamente wurden etwa eine stunde vor oder whrend einer mahlzeit eingenommen . 
obwohl sich durch dieses ausscheiden von patienten die per - protokoll - population der studiengruppen von der intent - to - treat - population unterschied , blieb die vergleichbarkeit uneingeschrnkt erhalten . bestrahlungsparameter alle patienten wurden an linearbeschleunigern mit energien zwischen 9und 16 - mev - photonen bestrahlt . 
tabelle 2 informiert ber die art der bestrahlung , die feldgren 1 und 2 ( zum beispiel feldgren vor und nach notwendiger feldverkleinerung ) , die dnndarmvolumina 1 und 2 ( zum beispiel bestrahlte dnndarmvolumina vor und nach notwendiger feldverkleinerung ) , die fraktionierung und einzelbzw . 
eine getrennte volumenbestimmung zwischen jejunum und ileum wurde nicht durchgefhrt . untersuchungsparameter als primres zielkriterium wurde der zeitraum bis zum auftreten der ersten diarrh ( definiert als 3 ungeformte sthle pro tag ) gemessen . 
prophylaxe der strahleninduzierten diarrh durch smektit stuhlkonsistenz 1 = flssig 3 = breiig 5 = fest tenesmen 0 = keine 2 = oft stuhlinkontinenz 0 = keine 2 = oft allgemeinzustand 1 = gut 3 = schlecht stuhlfrequenz pro tag nebenwirkungen 2 = breiig - flssig 4 = breiig - fest 1 = manchmal 3 = immer 1 = manchmal 2 = zufriedenstellend 4 = sehr schlecht anzahl der sthle pro tag ( mittels eines stuhltagebuches ) dokumentation von nebenwirkungen aller art tabelle 3 . 
sowohl die analyse des hauptzielkriteriums als auch die analyse der subgruppen unter bercksichtigung des bestrahlten dnndarmvolumens wurden nach der kaplan - meier - methode bezglich der wahrscheinlichkeit , keine diarrh zu entwickeln , sowie bezglich des medianen diarrhfreien zeitraumes durchgefhrt . 
neben der intent - to - treat - analyse wurde noch eine per - protokoll - analyse durchgefhrt , das heisst unter ausschlu von patienten , die die einund ausschlusskriterien nicht korrekt erfllten oder sonstige prfplanabweichungen mit einfluss auf die zu untersuchenden zielkriterien aufwiesen . in die intent - to - treat - analyse wurden alle 176 randomisierten patienten aufgenommen . 
29 patienten ( = 16 , 5% ; colina - gruppe 15 = 17 , 6% , plazebogruppe 14 = 15 , 4% ) beendeten die studie vorzeitig oder wurden aus anderen grnden von der per - protokoll - analyse ausgeschlossen . tabelle 4 zeigt die grnde der vorzeitigen studienabbrche . obwohl sich durch dieses ausscheiden von patienten die per - protokoll - populationen der studiengruppen von den intent - to - treat - populationen unterscheiden , blieb die vergleichbarkeit der studiengruppen uneingeschrnkt erhalten . im vergleich der studiengruppen war die tatschlich verabreichte durchschnittliche dosis des studienmedikamentes in beiden gruppen gleich . 
die werte schwankten whrend des studienzeitraumes zwischen tglich 3 , 6 und 3 , 8 beuteln ( = 10 , 8 g bis 11 , 4 g smektit in der colina - gruppe ) beziehungsweise tglich 3 , 7 und 3 , 8 beuteln ( = 11 , 1 g bis 11 , 4 g substanz in der plazebogruppe )  . 
die abweichung von der geplanten dosis von vier beuteln pro tag ( = 12 g prfsubstanz ) beruht auf der tatsache , dass anfngliche obstipationen eine dosisanpassung notwendig werden lieen . hufigkeit und zeitraum bis zum auftreten einer diarrh whrend des behandlungszeitraumes trat bei 51 patienten der colina - gruppe eine diarrh auf , in der plazebogruppe bei 54 patienten . 
der unterschied ist gem wilcoxon - test nicht signifikant ( p = 0 , 363 ) ( abbildung 1 )  . der mediane zeitraum bis zum ersten auftreten einer diarrh war nicht signifikant verschieden und betrug 20 tage ( 17 bis 32 tage , 95% - konfidenzintervall ) in der colinagruppe bzw . 
18 tage ( 15 bis 26 tage , 95% - konfidenzintervall ) in der plazebogruppe . zur bestimmung einer dosis - wirkungs - beziehung in korrelation zum bestrahlten dnndarmvolumen wurde post hoc eine subgruppenanalyse durchgefhrt . 
explorativ wurden die beiden gruppen jeweils am gesamtmedian des bestrahlten dnndarmvolumens 1 gesplittet ; dahinter steht die erwartung , dass sich in der subgruppe mit dem geringeren ausma an bestrahltem dnndarmvolumen ein unterschied zeigen knnte , da die verabreichte menge smektit hier ausreichenden schutz im sinne von mukusstabilisierung und toxinadsorption bieten sollte . der median des bestrahlten dnndarmvolumens 1 ( bestimmt bei 145 patienten ) betrug 837 , 5 ml . 
dieser wert wurde als trennpunkt fr die explorative subgruppenanalyse gewhlt , wobei der zeitraum bis zum auftreten einer diarrh innerhalb der zwei neuen patientenkollektive erneut ausgewertet wurde und dabei eine trennung in ein bestrahltes darmvolumen von 837 , 5 ml bzw . 
die ergebnisse sind in tabelle 5 dargestellt . colinagruppe plazebogruppe total nicht studienbedingt patientenwunsch andere erkrankungen unerwnschte ereignisse verschlechterung des az 1 andere grnde 0% 1 2 , 4% 2 2 , 4% 2 5 , 9% 3 1 , 2% 2 5 , 9% 4 1 , 1% 1 2 , 2% 4 2 , 2% 4 3 , 3% 8 2 , 2% 3 4 , 4% 9 0 , 6% 2 , 4% 2 , 4% 4 , 5% 1 , 7% 5 , 1% total 17 , 6% 14 15 , 4% 29 16 , 5% dnndarmvolumen > 837 , 5 ml zeitraum bis zur diarrh ( tage / median ) 95% - konfidenzintervall dnndarmvolumen 837 , 5 ml zeitraum bis zur diarrhe ( tage / median ) 95% - konfidenzintervall colinagruppe plazebogruppe n = 39 1222 n = 36 n = 33 1225 n = 37 20 offen 1538 tabelle 4 . 
hingegen zeigt sich bei patienten mit einem bestrahlten dnndarmvolumen von 837 , 5 ml eine statistisch nicht signifikante berlegenheit der prophylaktischen wirkung von smektit ( gem wilcoxon - test : p - wert 0 , 203 )  . 
der zeitraum bis zum auftreten einer diarrh wurde im vergleich zu plazebo fast verdoppelt und entsprach praktisch dem gesamten behandlungszeitrau fr das 95% - konfidenzintervall konnte der obere wert nicht berechnet werden . 
die wirkung von smektit bei der prophylaxe einer diarrh in diesem patientenkollektiv kommt auch in der kaplan - meier - kurve zum ausdruck ( abbildung 2 )  . eine statistische signifikanz war in der subgruppenanalyse nicht nachweisbar . 
die ergebnisse werden nachfolgend deskriptiv dargestellt und beziehen sich auf die studiengruppen gem der intent - to - treat - analyse . therapiephase in beiden gruppen auf werte von 2 , 2 bis 2 , 7 sthle pro tag an . im patientenkollektiv mit einem bestrahlten dnndarmvolumen von 837 , 5 ml waren die durchschnittswerte der auf einer fnf - punkte - skala beantworteten beschwerden bei den mit colina behandelten patienten zu allen zeitpunkten leicht niedriger als bei den patienten , die plazebo erhalten hatten ( 1 , 09 bis 2 , 04 fr colina versus 1 , 21 bis 2 , 13 fr plazebo )  . 
 stuhlkonsistenz in der mit smektit behandelten patientengruppe lag der konsistenz - score in der ersten woche bei 4 , 4 ; der wert fr die plazebogruppe betrug 4 , 2 . 
fr die restliche behandlungsdauer lag der konsistenz - score zwischen 3 , 7 und 3 , 8 fr die colinagruppe und zwischen 3 , 3 und 3 , 6 fr die plazebogruppe . im patientenkollektiv mit einem bestrahlten dnndarmvolumen von 837 , 5 ml waren die beurteilungen fr die colinagruppe geringfgig besser als fr die plazebogruppe ( 4 , 2 bis 4 , 9 versus 3 , 7 bis 4 , 5 )  . 
bei den anderen patienten ergaben sich keine wesentlichen unterschiede in der bewertung . stuhlfrequenz die anzahl der tglichen stuhlentleerungen betrug innerhalb der ersten bestrahlungswoche in beiden patientengruppen 1 , 7 sthle pro tag und stieg whrend der sechswchigen stuhlinkontinenz in beiden patientengruppen trat in der ersten woche keine stuhlinkontinenz auf . 
der score stieg dementsprechend in beiden behandlungsgruppen nur geringfgig auf 0 , 1 bis 0 , 2 an . tenesmen auch bezglich tenesmen wurden keine wesentlichen unterschiede zwischen der colina - gruppe und der plazebogruppe festgestellt . 
ausgehend von einem score von 0 , 1 in beiden behandlungsgruppen whrend der ersten woche , stieg der score whrend der bestrahlung auf 0 , 2 in der colina - gruppe und 0 , 4 in der plazebogruppe . auch bei diesem studienparameter ergaben sich im patientenkollektiv mit einem bestrahlten dnndarmvolumen von 837 , 5 ml geringfgig bessere werte fr die colina - gruppe ( 1 , 11 bis 1 , 36 ) als fr die plazebogruppe ( 1 , 16 bis 1 , 53 )  . allgemeinzustand der allgemeinzustand war in beiden gruppen bei der mehrzahl der patienten generell gut und wurde in der ersten woche durchschnittlich mit 1 , 1 bis 1 , 2 bewertet . 
dabei ergaben sich ber den gesamten untersuchungszeitraum nur noch geringfgige vernderungen . nebenwirkungen whrend der studie wurden keine signifikanten unterschiede in der art und inzidenz von nebenwirkungen in den behandlungsgruppen beobachtet . 
an schwerwiegenden unerwnschten nebenwirkungen wurden in der verumgruppe eine lungenembolie festgestellt , in der plazebogruppe ein bauchwandabszess und eine verstrkung postoperativer tenesmen . diskussion die diarrh ist eine der hufigsten nebenwirkungen der adjuvanten oder kurativen strahlentherapie bei tumoren im abdominalen / pelvinen bereich und ist oft von krampfartigen schmerzen begleitet . 
die prophylaxe der diarrh mit einem gut vertrglichen wirkstoff ist sehr wnschenswert , zumal die meisten der zur verfgung stehenden antidiarrhoika einen prophylaktischen einsatz nicht rechtfertigen [ 5 , 12 ]  . das in dieser studie verwendete antidiarrhoikum enthlt als hauptbestandteil smektit , ein schichtsilikat , das eine mukosastabilisierende wirkung auf die darmschleimhaut hat und eine hohe adsorptionsfhigkeit unter anderem auch fr gallensalze , toxische proteasen , mukolytische enzyme und bakterienendotoxine aufweist [ 4 , 6 , 19 ]  . 
diese hohe adsorptionskapazitt beruht vor allem auf der beachtlichen aktiven oberflche des smektits von 700 m2 / g [ 19 ] , wodurch die wirkung zum beispiel gegenber der kohle deutlich erhht ist . 
andere antidiarrhoika wie loperamid , tanninalbuminate , kohle , kaoline ( zweischichtiges silikatmineral ) und pektine greifen nicht so vielfltig in die pathophysiologischen mechanismen der multifaktoriellen genese der radiogenen diarrh ein und eignen sich deshalb weniger zur prophylaktischen anwendung . durch die oben genannten multiplen wirkmechanismen hat sich der wirkstoff smektit in der dosierung von 3mal 6 g in einer 1995 verffentlichten , einfach randomisierten studie als wirksam fr die prophylaxe der radiogenen diarrh erwiesen [ 14 ]  . zur berprfung dieser studienergebnisse wurde die jetzt aktuelle studie doppelblind randomisiert , plazebokontrolliert durchgefhrt , allerdings mit einer reduzierten dosis von 2mal 6 g pro tag , da die erste studie gezeigt hatte , dass mit der gabe von 3mal 6 g strkere obstipationen zu bestrahlungsbeginn auftraten . die vorliegende untersuchung ergibt in der auswertung des gesamtkollektivs mit der dosis von 2mal 6 g smektit keine unterschiede bezglich einer radiogenen prophylaxe zwischen der colina - gruppe und der plazebogruppe . in anbetracht der bisher positiven ergebnisse der prophylaxe mit 3mal 6 g smektit bedurften die aktuellen resultate aus dem gesamtkollektiv einer weiteren auswertung , die mittels einer primr nicht geplanten subgruppenanalyse innerhalb der gesamtgruppe durchgefhrt wurde . fr diese analyse wurde der median des bestrahlten dnndarmvolumens des gesamten kollektivs ( 837 , 5 ml darmvolumen ) herangezogen und die gruppen mit 837 , 5 ml und > 837 , 5 ml gebildet . die aufteilung der subgruppen basiert auf der theoretischen berlegung , dass eine abhngigkeit der prophylaktischen smektitwirkung von der dosierung , das heisst der oberflchenauskleidung des dnndarmepithels beziehungsweise der toxinadsorptionsfhigkeit , gegeben sein knnte , da durch grere abdominelle bestrahlungsfelder mehr schleimhautepithelvernderungen hervorgerufen werden knnen als durch kleinere ; somit knnte eine hhere smektitdosierung fr die prophylaxe bentigt werden . in dieser explorativen post - hoc - analyse zeigt sich , dass auch die subgruppe mit mehr als 837 , 5 ml dnndarmvolumen keinen vorteil von der prophylaktischen smektitgabe hat ; aber in der subgruppe mit 837 , 5 ml dnndarmvolumen konnte das erste auftreten einer diarrh vom 18 . 
in addition to excel lent medical and radiotherapy treatment , psychosocial support has a long tradition in the department and is an integral part of a comprehensive cancer patient man agement strategy [ 12 , 13 , 14 , 21 , 25 ]  . the need for psychosocial support among radiotherapy patients is estimated in the literature at about 1450% [ 6 , 7 , 8 , 9 , 33 ]  . 
cancer distress has been recognized as an important parameter in the success ful selection of patients for focused psy chosocial support and a distress screen ing procedure is therefore widely recom mended . 
this should preferably be con ducted at the patients first visit , in order to improve coherence with treatment , pa tients satisfaction with care and quality of life ( qol ) , as well as to decrease work load and stress for oncology teams [ 4 , 22 , 23 , 34 ]  . large screening studies of cancer dis tress have been performed in europe , with major efforts in germany [ 3 , 8 , 15 , 18 , 19 , 26 , 29 , 35 ]  . 
reference data from austria are sparse and mainly reported for small cohorts and / or specific tumor groups [ 1 , 7 , 30 , 32 , 33 ]  . at the department of radiation on cology , medical university of vienna , a multidisciplinary screening question naire that covers physical , social and psy chological problems and needs was suc cessfully implemented in clinical routine . 
 the aims of the study were to report prev alence rates of physical , social and psycho logical problems , as well as the needs of heterogeneous radiotherapy patients , and to evaluate independent risk factors for critical psychological distress , in order to identify vulnerable subgroups for focused psychosocial support . 
 informed consent for the use of person al information was requested orally and patients were offered the choice of filling out the questionnaire on their own or dur ing an informal personal interview . 
1 distribution of the cohort in different tumor - type groups , with ( m1 ) or without ( m0 , mx ) confirmed distant metastasis breast lung prostate head und neck gynecologic lower gastrointestinal upper gastrointestinal brain sarcoma lymphoma bladder / urothelial leukemia skin benign tumors unknown primary genital organs rare tumors missing medical history total totaln 1 , 500 m0 / m1 ( n ) 358 / 63 77 / 107 153 / 28 96 / 16 90 / 12 53 / 38 42 / 30 69 / 0 48 / 11 10 / 23 9 / 16 15 / 2 1 , 144 / 356 m1 ( %ofsubgroup ) tab . 
for metric da ta , either mean plus / minus standard de viation ( sd ) or median and interquar tile range ( iqr ) is given , depending on the distribution . distant metastases ( m1 ) were only cat egorized if verified in the medical history . 
criti cal psychological distress was defined by ratings above the cutoff level on both of the subscales ( psychological strains of hsi and symptoms of pobado )  . contingencytables for binary data , the phi coefficient of as sociation was tested for significance with a 22 contingency table ( phitest )  . binarylogisticmultivariateanalysis the potential influence of the predictors as independent variables in critical psy chological distress ( the dependent vari able ) was analyzed using a binary logis tic regression model , with all variables a priori specified and entered simultane ously . 
for the predictor variables , odds ratios and their 95% confidence intervals are giv en ; pvalues are considered significant at a level of 5% . results patient cohort the median age of the total cohort was 64 years , with a range of 1896 years ; iqr = 5471 . 
distant metastases ( lymphoma and leukemia excluded ) were confirmed in 24% . prevalence rates of physical , social and psychological problems and needs the mean qol in the total cohort is 5827% ( 100% indicates excellent qol )  . 
the most frequent symptoms were weakness ( 29% ) , sleeping difficulties ( 26% ) and exhaustion ( 23% )  . consequently , 40% were impaired to some degree in their functional sta tus , meaning that adls were not possi ble without restriction . 
 multivariate analysis reveals that patients with impaired physical integrity are at a significantly higher risk of experiencing critical psychological distress . keywords activities of daily living quality of life pain screening fatigue syndrome krperliche und psychosoziale probleme und bedrfnisse bei 1500 patienten zu beginn der strahlentherapie zusammenfassung hintergrund . 
zusammenfassend zeigen patienten mit einer beeintrchtigung der physischen integritt ein signifikant hheres risiko fr kritischen psychischen disstress . schlsselwrter aktivitten des tglichen lebens lebensqualitt schmerz screening erschpfungssyndrom eryday life ; most frequently for help with housework ( 28% ) , followed by assistance with outdoor tasks ( 23% ) , cooking ( 15% ) , indoor mobility ( 11% ) and personal care ( 9% )  . in total , 37% of the patients declared a requirement for additional information . 
low educational level binary : vas 3 clinically relevant pain categorical : stages 15 functional status of adl binary : any support requirements support requirements in daily life metric : number of symptoms patient - reported symptoms binary : m0 vs . 
breaking down the results roughly , it can be said that approxi mately one third 10% of our patients have physical , social and psychological problems and needs , which is in line with the body of evidence in the literature [ 5 , 6 , 9 , 28 , 32 , 33 ]  . 
resources , and for founding evidencebased arguments for the need to create additional staff positions in oncolo gy departments . in total , 22% of the cohort suffers from critical psychological distress . 
with ap proximately 3 , 000 patients seen per year at the department , the team of psychol ogists has to be prepared to support ap proximately 660 highly distressed pa tients . 
pa tients were classified as distressed if they were above the critical level in two sub scales reflecting psychological symptoms and strains , both of which represent a sub stantial burden . as reported in many other studies , fatigue syndrome ( characterized by ex haustion and weakness ) is a leading pa tientreported symptom in the overall cohort [ 5 , 11 , 18 , 20 , 27 ] and seems to go hand in hand with sleeping difficulties [ 2 , 31 ]  . 
putting the study results immediately back into practice , all patients in our de partment are informed about these con comitant symptoms und offered selfhelp instructions . the request of 13% of patients for addi tional information on psychological sup port is low compared to the value of 42% reported by devries , 1998 at the depart ment of radiotherapy in innsbruck , aus tria [ 7 ]  . 
hesitation to actively seek help from a psychosocial team seems to be typi cal for patients from vienna : frisch enschlager reported a very low accep tance of psychosocial support at our de partment 20 years ago , which he attrib uted to certain patient attitudes ( impor tance of personal independence , desire not to burden anyone , tendency to hold back personal interests and feelings ) [ 14 ]  . within a busy oncology outpatient routine , the selection of patients for re ferral to psychosocial support is general ly based on the diagnosis of critical dis tress by the professional teaeither the patient issues a cry for help by exhibiting signs of distress , or the referral is based on consideration of the underlying risk fac tors for psychological distress . for example , it is often assumed that cancer represents a greater burden for younger patients , as a life threatening dis ease might be a more critical event and interrupt family and professional life to a greater degree . 
women are expected to experience a higher level of distress be cause of the double burden of coping with disease , while still fulfilling their respon sibilities to family and work . 
patients with aggressive tumours are suspected to suf fer more distress coping with the limited life expectancy . while univariate analyses in the liter ature show significant differences in criti cal psychological distress between differ ent tumourtype groups [ 5 , 10 , 37 ] , these diminish in the multivariate analysis pre sented here . the significant risk factors show a comprehensive underlying structure , which can be summarized under physi cal integrity . 
the same is true for so ciodemographic data : univariate models in literature consistently report that wom en [ 16 , 24 ] and younger patients [ 10 , 37 ] have higher distress levels . 
one risk factor can be interpreted while keeping all other variables constant . a limitation of the study is the cross sectional design , which takes a snapshot of the patients physical , social and psy chological problems and needs at their first visit to our department . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 372379 doi 10.1007 / s00066 - 013 - 0315 - 4 received : 9 september 2012 accepted : 16 january 2013 published online : 23 . 
 histologically , p - pnet may often be misdiagnosed as the much more frequent central nervous system primitive neuroectodermal tumor ( cns - pnet ) because both entities consist of undifferentiated small , blue , round cells and cannot be distinguished by pure light microscopy [ 4 , 18 , 21 ]  . 
radiologically , however , primary intracranial p - pnet is more likely to be mistaken for meningioma [ 17 ] or meningeal sarcoma , with virtually all cases reported being meningeal - based . 
to provide an overview over the sparse data available to date , we evaluated the treatment and outcome in a small series of 17 patients , some treated at our institutions and others published as case reports between 1998 and 2012 . patients and methods minimal requirements for inclusion of a case in the study were a genetically confirmed diagnosis of p - pnet with an intracranial location , nonmetastatic disease , and sufficient information about treatment and follow - up . 
the 4 patients treated at our institutions ( 3 at fleni institute for neurological research in buenos aires , 1 at hannover medical school ) were presented as case reports at the 15th international symposium on pediatric neuro - oncology ( ispno 2012 )  . literature search strategy and selection criteria we performed a search of pubmed , embase , and the web of science with predefined search terms without time limitation . 
median age at diagnosis was 17 years ( range : 356 years )  . immunohistochemistry and genetic assessment the tumor samples of all patients showed cd99 expression and genetic aberrations 372 | strahlentherapieundonkologie52013 pubmed , web of science and embase search without time limitation : potentially relevant publications from 1957 2012 n = 276 after duplicates and non - english - language articles removed n = 214 full copies retrieved and assessed for eligibility n = 15 case reports included in meta - analysis ( n = 7 , 7 patients ) cases included in analysis ( n = 17 ) excluded by title and abstract review n = 199 excluded , not eligible for this study previously unpublished cases presented at ispno 2012 ( n = 4 ) additional publications identified by hand search ( n = 5 , 6 patients ) typical of the ewing tumor family : in three cases , a rearrangement of the ews region on chromosome 22q12 was reported without the fusion partners being explicitly mentioned . 
in another two cases , the ewserg fusion gene was detected . meningeal origin id ( csf ) cytology ( 7 / 17 = 41% ) , bone scan ( 7 / 17 = 41% ) , as well as bone marrow aspirate and biopsy ( 4 / 17 = 24% )  . first - line treatment of the 17 patients , 11 ( 65% ) initially received a multimodal treatment consisting of surgery , irradiation , and chemotherapy . 
the 6 remaining patients only underwent gross total resection ( gtr ) as firstline treatment , in two cases as a result of a misdiagnosis of meningioma [ 5 , 20 ]  . the tumors were meningeal - based in 13 of the 17 cases ( 76% ) ; in the remaining 4 cases ( 24% ) , a meningeal origin could not be excluded . surgery diagnostic work - up in the majority of cases a thorough diagnostic work - up to exclude primary extracranial or metastatic disease was reported . 
 in at least 10 of the 17 cases ( 59% ) , a computed tomography ( ct ) scan or a positron emission tomography ( pet ) of the body was performed . 
the check - ups were completed by further investigations such as magnetic resonance imaging ( mri ) of the spine ( 7 / 17 = 41% ) , cerebrospinal fluall patients initially underwent surgery . 
incomplete resection ( n = 7 ) or biopsy ( n = 1 ) was performed on 8 of the 17 patients ( 47% )  . adjuvant treatment adjuvant treatment consisting of focal radiotherapy and chemotherapy was administered to 10 of the 17 patients ( 59% )  . 
the most common chemotherapy regimen applied to 4 of 11 patients ( 36% ) consisted of a ewing tumor protocol using vincristine , cyclophosphamide , and doxorubicin ( vcd ) alternated with ifosfamide and etoposide ( ifoe )  . 
 strahlentherapieundonkologie52013 | abstract zusammenfassung strahlenther onkol 2013 189 : 372379 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0315 - 4 k.mllerb.dieza.muggerit.pietschc.friedrichs.rutkowskik.vonhoffa.o.vonbuereni.zwienerf.bruns whats in a name ? intracranial peripheral primitive neuroectodermal tumors and cns primitive neuroectodermal tumors are not the same abstract background . 
combined adjuvant treatment consisting of radiotherapy ( focal , n = 10 ; craniospinal , n = 1 ) and chemotherapy was administered to 11 of the 17 patients ( 59% )  . 
the optimal chemotherapy regimen has yet to be established , with both the ewing tumor and cns - pnet protocols being promising candidates for effective treatment . keywords peripheral primitive neuroectodermal tumor p - pnet intracranial radiotherapy chemotherapy namen sind schall und rauch . 
 eine intensive adjuvante therapie , bestehend aus strahlentherapie und chemotherapie , scheint von entscheidender bedeutung zu seeine statistisch fundierte empfeh l ung fr zielvolumina und dosierung der bestrahlung ist noch nicht mglich . 
cd99 immunopositivity may also be detected in other small , blue , round - cell tumors in which , however , the pattern of staining is often cytoplasmic [ 6 ]  . 
in summary , tumoral immunolabeling for cd99 is helpful in narrowing down the differential diagnoses of p - pnet , but is by no means pathognomonic . demonstration of genetic aberrations the gold standard for diagnosing p - pnet is the demonstration of the chromosomal translocation t ( 11 ; 22 ) ( q24 ; q12 ) , ewsfli1 , which accounts for 85% of all known ewing sarcoma translocations [ 7 ]  . 
in two cases ( 14% ) , the fusion gene ews - erg was detected [ 15 , 19 ]  . exclusion of an unrecognized extracranial primary tumor besides cytogenetic confirmation , reliable diagnosis of primary intracranial p - pnet requires exclusion of an occult extracranial source for the lesion in question [ 1 ]  . 
 in a retrospective chart review of 80 children with primary extracranial p - pnet , metas tatic spread into the cns was reported in 9% of cases [ 9 ]  . 
a t1 - weighted , gadolinium - enhanced , preoperative mri of the brain demonstrates a large , inhomogeneous , partly cystic lesion in the right lateral ventricle with marked local mass effect . 
d t1 - weighted , gadolinium - enhanced mri of the brain demonstrates stable disease after focal radiotherapy ( 59.4 gy ) patientswithfocalradiotherapy andpatientwithcsi four of the 10 patients ( 40% ) who received focal radiotherapy relapsed after 0.75 ( diez ii ) , 1.5 [ 16 ] , 5.3 ( diez iii ) , and 8 years , respectively [ 6 ]  . 
in 97% of cases , they demonstrate a strong membrane expression of the mic - 2 gene product , designated cell surface glycoprotein cd99 [ 2 , 12 , 28 ]  . 
by contrast , cnspnets are mainly reported to be negative original article overall survival incomplete resection + adjuvant therapy progression - free survival sole gross total resection at risk : at risk : time since diagnosis of intracranial mass ( years ) at risk : at risk : time since initial surgery ( years ) fig . 
4 8 progression - free survival of the patients with sole gross total resection and the patients with incomplete resection who all underwent intensive adjuvant therapy mary extracranial p - pnet . 
 by contrast , in two of the excluded cases in which initial pulmonary involvement was reported , the intracranial tumor was either completely surrounded by brain parenchyma [ 14 ] or it was at least not clearly meningeal - based [ 23 ] , indicating the possibility of a primary pulmonary tumor with secondary hematogenous spread into the cns . 
in accordance with a previous review , we underscore the importance of careful initial staging procedures , ideally including a bone scan , a ct scan of the body , and mri of the craniospinal axis to exclude an unrecognized extracranial origin for a suspected primary intracranial p - pnet [ 9 ]  . the median age at diagnosis in our cohort was 17 years . 
 [ 4 ] suggested that the treatment options available for primary intracranial p - pnet are similar to those for extraosseous ewing sarcoma elsewhere in the body , including surgery , radiation , and chemotherapy . role of surgery in extracranial extraosseous ewing sarcoma , it has been shown that the degree of surgical resection is one of the most important prognostic factors [ 24 ] , although additional adjuvant treatment is needed for curative approaches . 
however , all of these patients received intensive adjuvant therapy . role of radiotherapy several authors [ 1 , 4 , 11 , 19 , 23 ] recommend focal irradiation for primary intracranial p - pnet . 
however , at least in 2 of the 5 patients with secondary metastatic disease reported here , meningeal spread along the craniospinal axis has to be assumed [ 6 , 16 ]  . 
the focal doses delivered at the tumor sites ( median : 54 gy ; range : 4160 gy ) were apparently derived from the current radiotherapy protocols for ewing sarcoma , which approve 5560 gy for macroscopic and 4550 gy for microscopic residual disease [ 13 , 28 ]  . 
in summary , a statistically grounded recommendation concerning the appropriate target volumes and dose prescription is not yet possible owing to the paucity of reported cases and their short follow - up periods . role of chemotherapy the standard first - line treatment for localized extraskeletal ewing sarcoma ( ees ) consists of neoadjuvant chemotherapy with combinations of vincristine , doxorubicin and cyclophosphamide , ifosfamide and etoposide , followed by surgery or radiation , or surgery and postoperative radiation directed at the primary site . 
accordingly , it was most frequently chosen for the systemic treatment of the patients in our cohort , being administered to 4 of 11 patients ( 36% ) [ 3 , 4 , 14 , 19 ]  . 
in the first case , the patient had an almost complete resolution of tumor following the first three cycles of chemotherapy [ 14 ] , and in the second case the mri studies even demonstrated complete disappearance of the residual tumor after the third cycle of chemo - therapy [ 19 ]  . 
however , we have to keep in mind that both tumors in which the ees regimen was apparently highly effective were meningealbased and the chemotherapeutic agents did not have to cross the bloodbrain barrier to reach the neoplastic tissue . 
reported a case of intracranial p - pnet in which a cns - pnet chemotherapy protocol consisting of methotrexate , carboplatin , etoposide , cisplatin , vincristine , and lomustine was combined with focal irradiation . 
in summary , the role of chemotherapy in primary intracranial p - pnet has yet to be established , with both ewing sarcoma and cns - pnet protocols being auspicious candidates for effective treatment . outcome the 5 - year overall survival for our small cohort of primary intracranial tumors ( 7614% ) resembles that for localized extracranial p - pnet elsewhere in the body . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 437437 doi 10.1007s00066 - 013 - 0355 - 9 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
kneschaurek , klinik fr strahlentherapie der technischen universitt , klinikum rechts der isar , ismaninger strae 22 , d - 81675 mnchen , telefon ( + 49 / 89 ) 4140 - 4504 , fax - 4881 hellenic society of radiation oncology , p . 
roland felix 75 jahre strahlentherapie und onkologie 5 2013 | original article strahlenther onkol 2013 189 : 364366 doi 10.1007 / s00066 - 013 - 0308 - 3 received : 27 december 2012 accepted : 16 january 2013 published online : 23 . 
mrz 2013 springer - verlag berlin heidelberg 2013 l.dziggel1b.segedin2n.h.podvrsnik2i.oblak2s.e.schild3d.rades1 1 department of radiation oncology , university hospital schleswig - holstein , campus luebeck , lbeck 2 division of radiation oncology , institute of oncology , ljubljana 3 department of radiation oncology , mayo clinic scottsdale validationofasurvivalscorefor patientstreatedwithwhole - brain radiotherapyforbrainmetastases up to 40% of all cancer patients develop brain metastasis during the course of their disease [ 10 ]  . 
whole brain radiotherapy ( wbrt ) alone is the most common treatment for these patients , in particular for those patients with multiple lesions , although other treatment approaches are available for selected patients with a small number of lesions [ 4 , 6 , 9 ]  . 
short - course wbrt such as 5 fractions of 4 gy given in 1 week can be considered preferable to longer - course programs such as 10 fractions of 3 gy in 2 weeks or 20 fractions of 2 gy in 4 weeks for patients with a short survival time [ 6 ]  . 
in contrast , long - term survivors are better treated with longercourse wbrt and lower doses per fraction , since the risk of neurocognitive deficits due to wbrt increases with the dose per fraction [ 1 ]  . 
however , this scoring system , which was based on a study of 1 , 085 patients receiving wbrt alone between 1992 and 2005 , has not yet been validated . 
the present study was performed to validate our score in 350 new patients from germany and slovenia who received wbrt alone for brain metastases . materials and methods results the present study included 350 patients who received wbrt for brain metastases between 2005 and 2011 . 
four groups were formed according to the total score : 910 points ( group a ) , 1113 points ( group b ) , 1416 points ( group c ) , and 1718 points ( group d )  . 
the comparisons of each the prognostic groups a , b , c , and d of the present study to each of the prognostic groups a , b , c , and d of the previous study did not show a significant difference . 
1 survival rates 6 months after wbrt and the corresponding scores survivalat 6months ( % ) score 60 years 61 years karnofskyperformancescore extracranialmetastasesatthetimeofrt intervalfromtumordiagnosistowbrt 8 months > 8 months rt radiotherapy , wbrt whole - brain radiotherapy . 364 | strahlentherapieundonkologie52013 points points fig . 
 [ 1 ] observed neurocognitive deficits only after doses per fraction of 3 gy or higher , patients with a favorable prognosis appear better treated with longer - course wbrt including doses per fraction of < 3 gy . 
the 6 - month survival rates of the four prognostic groups in the 350 patients of the validation cohort were not significantly different from the survival rates observed in the previous study of 1 , 085 patients [ 7 ]  . 
however , both the previous and the present study were based on retrospective data which may have led to hidden biases . the validated score allows grouping the patients according to their survival prognosis . 
patients with a score of 913 points ( groups a and b ) had 6 - month survival rates of less than 25% , and may be treated with 5 fractions of 4 gy in 1 week . 
in patients with a score of 1416 points ( group c ) , short - course wbrt may at least be considered , since about 50% of these patients died within 6 months . 
on behalf of all authors , the corresponding author states that there is no conflict of interest . literatur kommentiert strahlenther onkol 2013 189 : 430430 doi 10.1007 / s00066 - 013 - 0336 - z online publiziert : 4 . 
april 2013 springer - verlag berlin heidelberg 2013 w.hohenberger chirurgischen universittsklinik , erlangen lebermetastasenkolorektaler karzinome3cmknnensicher mitradiofrequenzablation behandeltwerden 10 - jahres - ergebnisse originalbeitrag solbiati l , ahmed m , cova l et al ( 2012 ) small liver colorectal metastases treated with percutaneous radiofrequency ablation : local response rate and long - term survival with up to 10 - year follow - up . 
grundstzlich kann neben der etablierten chirurgischen me tastasenresektion auch die radiofre quenzablation zur lokalen destruktion von lebermetastasen kolorektaler karzi nome mit aussicht auf langfristige kom plette remission eingesetzt werden , even tuell auch in kombination mit der chi rurgischen therapie . 
die auto ren behandelten von 1997 bis 2006 kon sekutiv 99 patienten mit insgesamt 202 metachronen metastasen kolorektaler karzinome ( durchmesser 0 , 84 , 0 cm ; median 2 , 2 cm ) mit einer durch ultra schall gesteuerten , perkutanen radiofre quenzablation ( rfa )  . 
die berlebensra ten nach 3 und 10 jahren entsprechen je nen in den meisten chirurgischen serien . tige langzeitergebnisse wie mit der chi rurgischen resektion zu erreichen sind , muss jedoch eingeschrnkt werden . 
april 2013 springer - verlag berlin heidelberg 2013 p.blecharz1m.reinfuss2j.ry3j.jakubowicz2p.skotnicki4w.wysocki4 1 department of gynecologic oncology , center of oncology maria skodowska - curie memorial institute , krakow 2 department of radiation oncology , center of oncology maria skodowska - curie memorial institute , krakow 3 department of tumor pathology oncology , center of oncology maria skodowska - curie memorial institute , krakow 4 department of oncological surgery , center of oncology maria skodowska - curie memorial institute , krakow radiotherapyfor carcinomaofthevagina immunocytochemicalandcytofluorometric analysisofprognosticfactors primary invasive vaginal carcinoma ( pivc ) represents 12% of all female genitally tract malignancies and 0.10.2% of all malignancies [ 2 , 7 , 9 , 10 , 33 , 34 , 36 , 55 , 58 ]  . 
 radiotherapy is the treatment of choice in the majority of patients with pivc ; it is delivered as intracavitary brachytherapy , interstitial brachytherapy or external beam radiotherapy [ 7 , 10 , 13 , 16 , 20 , 22 , 26 , 27 , 31 , 33 , 37 , 43 , 44 , 50 , 53 , 55 , 56 ]  . the infrequent occurrence of pivc explains why the use of radiotherapy in these patients is still discussed in the literature . 
the aim of this study was to assess the potential prognostic factors ( population - based , clinical , microscopic , immunohistochemical , and cytofluorometric ) in radi cally irradiated patients . patients and methods between january 1985 and december 2005 , 80 patients with pivc underwent radical radiotherapy in the maria skodowska - curie memorial institute of oncology , cancer center in krakw . 
the analysis presented herein includes 77 patients ( 96.3% ) , in whom detailed microscopic , immunohistochemical , and cytofluorometric evaluations were retrospectively performed . the mean age in the analyzed group was 62.48.3 years ( range 3676 years )  . 
 in 37 patients ( 48.1% ) the karnofsky performance score ( kps ) ranged from 80 90 , and in the remaining 40 patients ( 51.9% ) the kps ranged from 6070 . 
in 40 women ( 51.9% ) pivc was initially located in the upper third portion of the vagina , in 14 ( 18.2% ) the middle third , and in 23 ( 29.9% ) the lower third . 
in 46 women ( 59.7% ) the lesion developed in the posterior vaginal wall , in 19 patients ( 24.7% ) the anterior wall , and in 12 ( 15.6% ) the lateral walls . 
in 35 patients ( 45.4% ) the disease involved one third of the vagi nal length , in 25 ( 32.5% ) two thirds , and in 17 ( 22.1% ) more than two thirds . 
eight patients with pivc stage i , but with a primary lesion thicker than 0.5 cm , all 46 patients with stage ii and iii disease , and 6 women with stage iva disease underwent intracavitary brachytherapy with external beam irradiation ( 6 mev , linear accelerator , four field box technique )  . 
total brachytherapy dose for tumor volume was 6570 gy and total external radiotherapy dose for the pelvis was 50 gy ( 5 fractions / week , 2 gy per fraction )  . 
the total dose of 50 gy delivered using the box technique was supplemented by an additional 2025 gy delivered using the shrinking - fields technique ( up to the total dose of 7075 gy )  . 
in 2 women with biopsy - confirmed inguinal node involvement , 20 gy with a 15 mev electron boost for inguinal fields was delivered . histology and special techniques the detailed microscopic , immunohistochemical , and cytofluorometric studies were performed on paraffin - embedded tumor specimens . 
hematoxilin / eosin - stained ( 4 m ) slides were used to assess the following features of the tumor : microscopic type ( according to the who classification ) , grading , mitotic index , lymphatic vessels invasion , lymphocytes / plasmocytes infiltration , focal necrosis and in situ component ( vain3 )  . 
 the analysis of hematoxilin / eosin slides revealed the following features of the tumors : histological type ( according to the who classification ) [ 52 ] : squamous cell carcinomas adenocarcinomas , and undifferentiated carcinomas in 65 ( 84.4% ) , 11 ( 14.3% ) , and 1 ( 1.3% ) tumor , respectively . 
additionally in 31 ( 40.3% ) cases atypical mitoses were observed , in 15 cases ( 19.5% ) lymphatic vessels invasion , in 44 ( 57.2% ) lymphocytes / plasmocytes infiltration , in 33 ( 42.8% ) focal necrosis , and in 21 ( 27.3% ) in situ component ( vain3 )  . immunohistochemistryp53 protein and proliferation - associated antigen ki - 67 ( mib - 1 ) expression p53 overexpression was analyzed immunohistochemically using monoclonal antibodies against two different epitops : bp53 - 12 and p53 - 1801 . 
ki67 proliferation index was assessed by the rate of positively stained nuclei , regardless of the reaction intensity ; 500 , which means 100 cells per 5 fields ( 400 ) were counted in each case . 
protein p53 expression ( epitope bp53 - 12 ) was staged in 29 ( 37.7% ) cases as 03 points according to the remmelle and stegner score , and in the remaining 48 ( 62.3% ) cases as 612 points . 
histogram was defined as diploid , if only one peak of g0 / g1 cells fluorescence was observed ; additional peaks , fraction of cells in the s - phase more than 20% and evidence of a second g2 / m cells fraction qualified histogram as aneuploid . 
rate of cell proliferation , expressed as percentage of cells in the s - phase and as proliferation index ( s + g2 / m ) , was also estimated . 
the s - phase fraction was spf10% in 42 ( 54.5% ) , 10% < spf20% in 23 ( 15 25% ) , and > 25% in 37 ( 48.0% ) , 21 ( 27.3% ) , and 19 ( 24.7% ) tumors , respectively . statistical analysis the 5 - year ned survival rate was used as the end point for this analysis . 
seven factors , statistically significant in the univariate analysis were included into the multivariate analysis of the prognostic factors , which was done using the cox proportional hazards regression model [ 8 ]  . strahlentherapieundonkologie52013 | original article abstract zusammenfassung results strahlenther onkol 2013 189 : 394400 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0291 - 0 p.blecharzm.reinfussj.ryj.jakubowiczp.skotnickiw.wysocki radiotherapy for carcinoma of the vagina . 
significantly better 5 - year ned was observed in patients : < 60 years , kps 80 , figo stage i and ii , grade g12 , mib - 1 index < 70 , s - phase fraction < 10 , and proliferation index < 25 . 
independent prognostic factors in the radically irradiated pivc patients were as follows : age , figo stage , mib - 1 index . keywords primary invasive vaginal carcinoma vaginal neoplasms radiotherapy prognostic factors risk assessment strahlentherapie beim vaginalkarzinoimmunozytochemische und zytofluorometrische analyse prognostischer faktoren zusammenfassung hintergrundundziel . 
die analyse wurde an 77 patientinnen mit pivc durchgefhrt , die in den jahren 1985 bis 2005 im maria - skodowska - curie - gedenkinstitut fr onkologie , im krebszentrum in krakau , behandelt wurden . 
deutlich bessere 5 jahres - nedeffekte wurden bei folgenden patientinnen beobachtet : < 60 jahre , kps 80 , figo - stadium i und ii , grad g12 , mib - 1 - index < 70 , s - phase - fraktion < 10 , proliferationsindex < 25 . 
unabhngige faktoren bei radikal bestrahlten patientinnen mit einem primren invasiven vaginalkarzinom waren wie folgt : alter , figo - stadium , mib - 1 - index . schlsselwrter primres invasives vaginalkarzinom vaginale neoplasien strahlentherapie prognostische faktoren risikoabschtzung in 77 patients , the 5 - year ned survival was 46.8% ( 36 women )  . 
this group included 26 patients who died from reasons closely related to pivc : 10 patients from lung or liver metastases , 16 patients from hemorrhage , ileus , uremia , or sepsis . 
in addition 12 patients died from intracranial hemorrhage ( 5 cases ) , circulatory failure ( 3 cases ) , heart attack ( 2 cases ) , and 2 cases for no obvious reasons , all with symptoms of progression or dissemination of pivc . 
in the literature the majority of evidence support age as an independent prognostic factor in pivc patients treated with radiotherapy : the younger the age , the better the prognosis [ 3 , 14 , 15 , 17 , 18 , 21 , 24 , 25 , 55 , 56 , 58 ]  . 
 [ 10 ] showed age to be prognostic factor for overall survival , but no for 5 - year ned survival ; the same phenomenon was also reported by perez et al . 
staging according to figo is a basic and unquestioned independent prognostic factor in irradiated pivc patients [ 1 , 4 , 7 , 9 , 10 , 12 , 15 , 17 , 18 , 20 , 21 , 24 , 28 , 30 , 31 , 32 , 33 , 37 , 38 , 40 , 41 , 45 , 50 , 51 , 53 , 54 , 55 , 56 ]  . two immunohistochemical factors were assessed for a potential prognostic role : mib - 1 index and protein p53 overexpression . 
mrz 2013 springer - verlag berlin heidelberg 2013 m.ehmannf.wenz klinik fr strahlentherapie und radioonkologie , universittsmedizin mannheim frhepostoperative strahlentherapienachradikaler prostatektomiebeihigh - riskprostatakarzinompatienten weiterhinstandard langzeitergebnissedereortc - studie22911 originalbeitrag bolla m , poppel h van , tombal b et al ( 2012 ) postoperative radiotherapy after radical prostatectomy for high - risk prostate cancer : long term results of a randomised controlled trial ( eortc trial 22911 )  . 
in die randomisiert kontrollierte phase - iii - studie [ 2 ] wurden patienten bis 75 jahre aus 37 europischen lndern eingeschlossen , die ein prostatakarzinom im stadium pt2n0 mit risikofaktoren oder ein pt3n0 aufwiesen . 
es zeigten 198 der 502 patienten nach postoperativer bestrahlung ( 39 , 4% ) und 311 der 503 nur nachbeobachteten patienten ( 61 , 8% ) einen biochemischen oder klinisch manifesten progress oder starben ( hr 0 , 49 ; 95% - ki 0 , 410 , 59 ; p < 0 , 0001 )  . 
auch nach 10 , 6 jahren blieb die verbesserung des biochemischen progressionsfreien berlebens sowie der lokalen kontrolle nach konventioneller postoperativer bestrahlung auf die prostataloge im vergleich zum kontrollarm signifikant , was die ergebnisse des 5 - jahres - nachbeobachtungszeitraums besttigt . 
 die postoperative bestrahlung verbessert das klinische progressionsfreie berleben vor allem bei patienten , die jnger als 70 jahre sind , sowie bei patienten mit positiven schnittrndern . kommentar beim berdenken der dargestellten ergebnisse und schlussfolgerungen fllt folgendes auf : 1 . 
die autoren schlussfolgern unter anderem aus der hheren sterblichkeit der alten patienten ( > 70 jahre ) , dass eine sofortige postoperative bestrahlung in der r0 - situation mglicherweise nachteilig sei und deshalb nicht empfohlen werden sollte . 
da fr prostatakarzinompatienten das durchschnittsalter kontinuierlich ansteigt , verschiebt sich mglicherweise diese problematik auch zunehmend ins hhere alter und die patienten in dieser konstellation profitieren zuknftig doch von der postoperativen strahlentherapie . trug lediglich 60 gy mit einzeldosis von 2 gy . 
als aktueller standard gelten mindestens 66 gy im adjuvanten setting , eine weitere dosiseskalation bis 70 gy scheint die bned ( biochemical no - evidence of disease ) weiter zu verbessern [ 3 ]  . 
denn genau jene patienten mit nicht messbarem , postoperativ nicht nachweisbarem psa , profitierten in der aro - studie [ 4 ] besonders von einer adjuvanten strahlentherapie und hatten signifikant weniger biochemische rezidive . 
wenn aber durch eine adjuvante radiatio das psa - rezidiv mglicherweise verhindert wird und dann auf eine hormonsuppressive thera432 | strahlentherapieundonkologie52013 pie verzichtet werden knnte , wrden auch deren bekannte nebenwirkungen wie osteoporose , hitzewallungen , sarkopenie und verschlechterte lebensqualitt weniger hufig in kauf genommen werden mssen [ 6 ]  . 
 schlielich ist die klinische bedeutung eines psa - rezidivs immer wieder individuell zu bewerten , gerade auch im hinblick auf das steigende lebensalter der patienten , im hinblick auf das gesamtberleben sowie des klinischen progressionsfreien berlebens . 
bei der beantwortung der frage ob adjuvante strahlentherapie oder early - salvage - therapie bediene man sich der raves - studie ( radiotherapy adjuvant versus early salvage , [ 8 ] ) , der radicals - hd - studie ( radiotherapy and androgen deprivation in combination after local surgery - hormone dura tion , [ 9 ] ) sowie der getug - 17 - studie ( groupe detude des tumeurs uro - gnitales , [ 10 ] )  . fazit bisaufweiteresgiltbeipatientenmit prostatakarzinomundhoch - risiko - konstellation , wennnocheinerelevantelebenserwartungbesteht , diefrhepostoperativestrahlentherapiealstherapeutischerstandard . michael ehmann und frederik wenz , mannheim korrespondenzadresse m . 
bolla m , poppel h van , tombal b et al ( 2012 ) postoperative radiotherapy after radical prostatectomy for high - risk prostate cancer : long term results of a randomised controlled trial ( eortc trial 22911 )  . 
siegmann a et al ( 2011 ) dose escalation for patients with decreasing psa during radiotherapy for elevated psa after radical prostatectomy improves biochemical progression - free survival : results of a retrospective study . 
williams mb , hernandez j , thompson i ( 2005 ) luteinizing hormone - releasing hormone agonist effects on skeletal muscle : how hormonal therapy in prostate cancer affects muscular strength . 
48 , salzburg austria f.sedlmayer@salk.at the authors and the publisher regret two typing errors on page 194 . in the second column , first bullet point , the correct text should be ( indicated in bold ) : f after conventional wbi ( 25 fractions of 2 gy ) followed by a tumor bed boost of 10 gy ( 5 fractions of 2 gy ) , the 2 gy per fraction equivalent dose ( 2 gy ed ) in the boost area is 60 gy , and after a booster dose of 16 gy ( 8 fractions of 2 gy ) , the 2gyed amounts to 66 gy , respectively . 
mrz 2013 springer - verlag berlin heidelberg 2013 h.badakhshia.grnc.strombergerv.budachd.boehmer department for radiation oncology , charit university medicine , berlin oligometastases : thenew paradigmandoptions forradiotherapy acriticalreview a new paradigm is increasingly determining clinical practice : the oligometastatic state . 
 traditionally , patients with cancer are assigned either treatment with a curative intent , in cases where the tumour is localised and there is no indication for metastatic manifestation , or they receive palliative therapy because of lesions that have spread beyond the primary tumour . 
in this context , the perception of metastatic cancer is seen in a more differentiating way with focus on the details of disease manifestations with regard to the number and sites of the lesions . 
in the future , metastatic cancer is going to be viewed more as a dynamic spectrum than merely as a definite status [ 2 ]  . for a long time in the previous century , halsteds doctrine of cancer as a localised and orderly process , which might at some stage start a contiguous spreading into adjacent structures , was predominant . 
 it was challenged by the systemic theory , assuming a primary systemic state , in most cases involving a complex spectrum of hosttumour interactions , and claiming that local treatment is unlikely to effect the survival of patients [ 3 ]  . in 1994 samuel hellmann [ 2 ] stated that cancer is a heterogeneous disease that can be thought of as a spectrum of proclivities extending from a disease that remains local and that persistent disease , locally or regionally , may give rise to distant metastases and therefore , in contrast to the systemic theory , locoregional therapy is important . 
in 1995 , referring to this a priori idea , he proposed the existence of a clinically significant state of oligometastases as an interim stage in the natural history of most solid malignancies [ 4 ]  . 
in this review , results from molecular , developmental and cellular biology of metastases are integrated to provide an up - to - date understanding of metastatic capacity of tumours and consequently , to interlace these facts with the clinical discourses of oligometastases . 
in a further step , we show relevant clinical implications of the oligometastatic state and corresponding clinical data for lung , liver , bone and brain lesions , limited in number and site , with special respect to radiotherapeutic procedures . biology of metastases metastases are regarded as the end stage of the patients life . 
 they might be synchronously present at initial diagnosis of the primary tumour or in some cases , they are detected previously , without any primary tumour . metastasising is a multistep process : a primary tumour that is infiltrating the site of its origin ( invasion ) locally will , at some stage , enter the vasculature of lymphatic and blood systems ( intravasation )  . 
 the physical translocation involves the following aspects : circulating tumour cells in blood have to survive many different stress factors , and after finding affinities to a specific tissues ( homing ) , they have to exit the bloodstream and enter the parenchyma of the host organ ( extravasation )  . 
the next step is colonisation : at the new site , the tumour cells invade the microenvironment , thereby evading the innate immune system , and then they must adapt to the new host and initiate proliferation [ 1 , 5 ]  . an intratumoural genetic instability is seen as the basic condition of possibility for invasion and metastasising . 
a higher mustrahlentherapieundonkologie52013 | bersichten tability is seen in those clonal subgroups with an apparently higher rate of metastases [ 6 ]  . the acquisition of an aggressive phenotype is now recognised as a trigger for the metastatic cascade . 
extrinsic suppressive factors include an extracellular matrix , tensional forces , basement membranes , reactive oxygen radicals , immune response , inhibitory cytokines , regulatory ecm peptides , low ph and , especially , local hypoxia . 
this last point is a selective component in this context : the cellular response to hypoxia involves the stabilisation of a hypoxia - inducible factor - 1 ( hif - 1 ) transcriptional complex , which is an activator of genes that promote angiogenesis , survival , anaerobic metabolism and invasion [ 8 ]  . 
tumours with abundant hif - 1 stabilisation tend to spread metastatically [ 9 , 10 ]  . an important source of the intratumoural heterogeneity is revealed by the fact that tumours are organised hierarchically [ 11 ]  . 
the scale of self - renewing stem cells , progenitor cells and fully differentiated end - stage cells seems to be present in malignant tumours [ 12 , 13 ]  . 
two different theories have been proposed : f the stochastic model claims that every cancer cell within a tumour can ultimately acquire the capacity for self - renewal and multilineage potency , and therefore repopulate an entire tumour [ 20 ] ; f the hierarchy model claim that tumours are heterogeneous and that only a minority of cells serve as stem cells , giving rise to tumours and metastases [ 1 ]  . 
both processes depend on the ability of cancer cells to become founder cells that can reproduce unlimited numbers of descendant cells [ 1 ]  . additionally , other characteristics may enhance the impact of stem cells on the metastatic capacity of cells : motility , invasiveness and augmented resistance to apoptosis [ 21 ]  . 
it is an embryologi cally conserved genetic programme by which epithelial cells downregulate intercellular tight junctions , lose polarity , express mesenchymal markers and manifest an aggressive migratory phenotype [ 22 ]  . 
driven by transcription factors ( emt - tf ) , the programme may induce mechanisms for activation of nonstem cells into a stem cell - like state and , additionally , to increase the resistance to apoptosis [ 23 , 24 ]  . 
they have a relatively large diameter ( 2030 m ) that complicates the flow through the tiny capillary system of the lungs , which have a diameter of approximately 8 a large number of circulating cells might be trapped very soon after their release by the primary tumour . 
a complex network of interactions and distinct adaptive processes are seen to be the basis for colonisation [ 1 ]  . specifics of oligometastases continuing improvements in morphological and biological imaging and the wide implementation of regular follow - ups are leading to more sensitive and earlier detection of relapse , which enables clinicians to see limited metastases at an early and therefore controllable stage in the trajectory of the diseases . proposing an intermediate state of metastases , termed oligometastases , hellmann and weichselbaum [ 26 ] stated that in the concept in which the number and site of metastatic tumours is limited , the evolution of metastatic capacity has intermediate states in which spread may be limited to specific organs and metastases might be present in limited numbers . 
highly conformal radiation therapy in particular , stereotactic ablative radiotherapy ( sabr ) and brachytherapy may well provide a higher level of therapeutic efficiency and safety compared to minimal or noninvasive methods with lower morbidity , lower costs and the potential for delivering ablative treatments on an outpatient basis . 
while patients may receive rt for a limited number of metachronous metastases , it has to be discussed whether they are in need of systemic therapy in certain clinical settings . 
the case of early breast cancer in which single or oligometastases may occur long after the primary therapy in bone or brain in a very limited number and size might exemplify the rationale for omitting chemotherapy . 
 after application of local rt and its measurable outcome , one could discuss omission of chemotherapy upon provision of image - based confirmation of absence of any other lesion ; however , these patients have to undergo short - termed follow - up visits [ 32 ]  . 
it is very important to understand potential or hypothesized differences in biological behaviour of those cases with oligometastases within one specified organ and those with oligometastases in two different organs ; however no valid data on measurable clinical differences in regard to outcome are available [ 26 ]  . 
further prospective studies have to discriminate between these two subgroups . radiation oncology is experiencing a shift toward more sophisticated high - tech methods , which are redefining the ballistic technique in order to deliver higher radiation doses to target volumes , whilst sparing surrounding normal tissues of critical structures by means of f intensity - modulated radiation therapy , including volumetric modulation arc therapy and similar rotational approaches , f robotic arm delivery of radiation therapy and f high linear energy transfer ionising radiation delivery as represented by protons and other hadrons . emerging data show that sbrt and brachytherapy in its various treatment models are safe and efficient for local control of limited metastatic lesions . 
it has to be , at least in regard to intention , a curative dose [ 26 , 29 , 31 , 32 ]  . clinical experience and challenges are reviewed and discussed below . lung metastases the lungs are one of the common sites of metastasis of solid tumours from different origins . 
thirty of these patients were treated with curative intent with a preferred dose of 50 gy in 5 fractions ( biological equivalent dose [ bed ] 100 gy )  . 
at a median follow - up of 14 months , those treated with 30 gy in 3 fractions had a local control rate of 70% , those treated with 40 gy in 4 fractions had a 77% local control rate , and those treated with 48 gy in 4 fractions had a 100% local control rate . 
 [ 35 ] reported on 61 patients who were treated with 26 gy in 1 fraction , 22 who were treated with a dose of 45 gy in 3 fractions and 3 who were treated with a dose of 36 gy in 4 fractions . 
a critical review abstract traditional oncology distinguishes between two separate and incommensurable states in the evolution of solid malignancies : the localized disease , which is curable ; and the disseminated status , which is per se palliative . 
 recently , a huge body of evidence suggests a fundamental change in the understanding of cancer , indicating an intermediate state in the trajectory of solid malignancies : the oligometastatic state . 
consecutively , it will try to draw possible clinical consequences for application of radiotherapy in this specific clinical scenario . keywords oligometastases oligometastatic state curative options radiotherapy paradigm shift oligometastasen : neue paradigmen und mglichkeiten fr die strahlentherapie . 
ein kritischer berblick zusammenfassung die traditionelle onkologie trennt hinsichtlich therapeutischer optionen zwei grundlegend unterschiedliche klinische situationen : die lokalisierte erkrankung mit kurativen therapiechancen und die disseminierte situation mit nur noch palliativen lsungen . 
 [ 54 ] 14 , prospective 27 , prospective 140 , prospective 47 , prospective 27 , prospective 1 year : 85% 2 year : 62% 2 year : 30% 12.5 gy in 3 fractions 2560 gy in 3 fractions 24 gy in 6 fractions 1220 gy in 3 fractions 10 gy in 35 fractions 12 gy in 5 fractions localcontrol 6 month : 75% 12 month : 71% 1 year : 100% 2 year : 86% 1 year : 95% 2 year : 92% 24 month : 50 gy : 89% 60 gy : 100% overall , sbrt in this patient group is well tolerated and clinical outcomes in terms of local control and overall survival seem to be achieved with regimes prescribing a bed of 100 gy . 
overall survival , which depends on various factors such as overall dynamics of the disease , performance index and therapeutic regimens preand post - rt , is between 39 and 84% at 2 years . 
comparison with surgery is impossible due to a lack of randomised trials ; the patients treated in the above trials were invariably medically inoperable , which has an impact on overall survival rates . 
however , the results for sabr are encouraging , and this noninvasive approach is a valid alternative . liver metastases the liver is one of the common sites of metastasis of solid tumours , especially from colorectal cancer . 
 brachytherapy based on ct - guided insertion of 192iridium high - dose rate sources in the liver with afterloading technique offers a favourable dose distribution within the lesion , including very large tumours > 10 ccooling effects by adjacent blood vessels are not a concern in brachytherapy , and the method may be used in lesions close to the liver hilum due to the relatively high radiation tolerance of the bile duct [ 40 ]  . 
intra and extrahepatic progression - free survival was 53 , 40 and 27% , and overall survival was 97 , 79 and 60% , respectively . no dose dependency of local tumour control was observed if a minimal dose of 15 gy was applied . 
however , in case of local recurrence , due to the relative independence of brachytherapy to the size of the tumour volume treated and the low impact on liver function , ct - guided brachytherapy could be repeated [ 40 , 41 ]  . 
due to highly complex scenarios in the trajectory of the disease and continuing changes in the regimens of chemotherapy and biologicals , the role of overall survival has to be re - evaluated permanently according to the current standards . brain metastases the optimal conservative treatment for patients with oligometastases of the brain is still controversially discussed [ 42 ]  . 
there is a broad spectrum of techniques and concepts available , including whole brain radiotherapy ( wbrt ) alone , whole brain plus stereotactic radiosurgery ( srs ) boost and stereotactic radiosurgery alone . 
 [ 59 ] 93 , prospective 76 , prospective 10 months : 96.8% 15 months : 90% 84% ( clinical data ) survival doseprescription 24 gy in 1 fraction , 27 gy in 3 fractions , 30 gy in 5 fractions 15.5 gy in 2 fractions 24 gy in 1 fraction 1625 gy in 15 fractions ryu et al . 
although srs alone was associated with increased intracranial progression as compared with wbrt plus srs , no differences in the frequency of neurological deaths and preservation of neurological function were observed . 
similarly , the recent eortc 22952 - 26001 study on the adjuvant wbrt versus observation after srs or surgical resection of 13 cerebral metastases showed that adjuvant wbrt was able to reduce the frequency of intracranial progression but failed to improve the median survival [ 45 ]  . spinal metastases stereotactic radiotherapy is a clinically proven option as primary and postoperative treatment , and as retreatment for previously irradiated patients , with good results on pain control , neurological symptom release and quality of life , although lack of prospective data , especially randomised data , makes it difficult to reach conclusions . 
at the pretreatment baseline , 23% patients were pain free ; at 1 month and 12 months post - sbrt , 44 and 52% patients were pain free , respectively . 
twenty - seven of 32 cases ( 84% ) with a progressive neurological deficit before treatment experienced at least some clinical improvement . local radiotherapeutic treatment is evidently effective and can be safely applied for spinal lesions . bone metastases oligometastases of bone have been reported in prostate and breast cancer . 
 [ 32 ] reported on 85 metastatic lesions in 40 breast cancer patients treated with sbrt , achieving a 2 - year overall survival rate of 76% and a 4 - year overall survival of 59% . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . strahlentherapieundonkologie52013 | bersichten literatur kommentiert strahlenther onkol 2013 189 : 433435 doi 10.1007 / s00066 - 013 - 0334 - 1 online publiziert : 23 . 
mrz 2013 springer - verlag berlin heidelberg 2013 i.a.adamietz klinik fr strahlentherapie und radio - onkologie , marienhospital herne , universittsklinikum der ruhr - universitt bochum , herne lebensqualittnachchirurgie oderradiochirurgievon hirnmetastasenundadjuvanter ganzhirnbestrahlung kurz - undlangzeitprognosedifferenziert dietherapiestrategiebeihirnmetastasen originalbeitrag riccardo s , kocher m , abacioglu um et al ( 2013 ) a european organisation for research and treatment of cancer phase iii trial of adjuvant whole - brain radiotherapy versus observation in patients with one to three brain metastases from solid tumors after surgical resection or radiosurgery : quality - of - life results . 
die phase - iii - studie der eortc verglich nach chirurgischer oder radiochirurgischer behandlung von patienten mit einzelnen ( 13 ) hirnmetastasen solider tumoren ohne extrazerebrale progression die adjuvante ganzhirnbestrahlung ( wbrt ) mit einer nur kontrollierten beobachtung . 
der eortcqlq - c30 - fragebogen umfasste 5 funktionsskalen ( krperliche funktion , rollenfunktion , emotionale funktion , kognitive funktion und soziale funktion ) , 3 symptomatische skalen ( fatigue , belkeit / erbrechen , schmerz ) , 6 einzelskalen ( dyspnoe , schlaflosigkeit , appetitverlust , obstipation , diarrhoe , finanzielle aspekte ) sowie eine allgemeine gesundheitsskala . 
der eortcqlqbn20 wurde speziell fr patienten mit malignen hirnerkrankungen entwickelt und besteht aus 20 fragen , die 4 skalen messen ( visuelle strungen , motorische dysfunktion , kommunikative defizite , unsicherheiten bei der zukunftsplanung ) sowie 7 einzelskalen ( kopfschmerzen , benommenheit , haarverlust , hautjuckreiz , beinschwche , blasenfunktion )  . 
die differenzen waren statistisch signifikant und klinisch relevant , hauptschlich jedoch nur whrend der frhen nachbeobachtungsperiode : physis und fatigue nach 8 wochen , allgemeiner gesundheitsstatus nach 9 monaten , kognition nach 12 monaten . 
ein engmaschiges monitoring mit hilfe der magnetresonanztomographie gilt im hinblick auf die lebensqualitt als bedenkenswerte alternative . kommentar sind studienergebnisse im klinischen alltag mehr wert als die klinische expertise ? eine meiner patientinnen , die ich krzlich vor einer wbrt nach neurochirurgischer entfernung zweier supratentorieller metastasen beraten hatte , gab die meinung ihres operateurs zum weiteren vorgehen folgendermaen an : die einen sagen so , die anderen so . 
 was soll nun ein radioonkologe in einer solchen situation tun ? und wieweit helstrahlentherapieundonkologie52013 | literatur kommentiert fen ihm dabei die ergebnisse der hier zu kommentierenden europischen studie ? diese wichtige studie zeigt interessante daten , die das beobachtete klinische bild nach einer wbrt besttigen : die reduktion der physis ( fatigue ) innerhalb der ersten 2 monate , die verschlechterung des allgemeinbefindens 39 monate nach ende der radiotherapie sowie das auftreten der kognitiven strungen nach ablauf eines jahres sind jedem praktizierenden strahlentherapeuten gelufig . 
bei deren interpretation sollten die leser jedoch einige einschrnkungen der studie beachten . eines der grten probleme ist der rckgang der compliance , die zwar zu beginn der studie sehr hoch war , jedoch bald auf 45% nach 12 monaten abfiel . 
obwohl dies fr studien mit malignen erkrankungen durchaus akzeptabel und teilweise auch besser als in anderen bisher durchgefhrten studien zu hirnmetastasen oder glioblastomen ist , stellen sie doch eine wesentliche limitierung dar . 
das kann , wie von den autoren des artikels treffend beschrieben , ein grund fr das verlassen des lebensqualitts - bewertungsrhythmus se der grund dafr wre ja die verschlechterung des leistungsniveaus . 
auch der langzeiteffekt der wbrt konnte aufgrund des rcklaufs valider fragebgen nicht adquat evaluiert werden [ 4 ]  . eine weitere einschrnkung ist die bewertung der kognitiven funktion der studienteilnehmer . 
obwohl sie mit hilfe des eortcqlq - c30 gemessen wurde , sollte dennoch bedacht werden , dass eine selbstbewertung und eine objektive neurokognitive evaluation von auen meistens nur schlecht miteinander korrelieren . 
diese daten stellen seit jahren den grund fr immer wiederkehrende debatten zwischen den forschergruppen dar , ohne dass dabei jedoch ein allgemeiner konsens htte erreicht werden knnen [ 3 , 4 , 5 , 6 ]  . bei dieser wichtigen frage nach dem stellenwert einer adjuvanten wbrt ist die isolierte betrachtung der lebensqualitt zum teil irrefhrend . 
die wbrt reduzierte das rckfallfreie berleben , bezogen auf die ursprngliche metastasenlokalisation bei den operierten patienten von 59 auf 27% und bei den patienten nach radiochirurgie von 31 auf 19% . 
im beobachtungsarm verstarben 44% der patienten an intrakranieller tumorprogression gegenber nur 28% im bestrahlungsar die adjuvante wbrt reduzierte somit das risiko des hirnmetastasenbedingten todes und der intrakraniellen rckflle , hatte aber keinen einfluss auf die dauer des progressionsfreien intervalls oder das gesamtberleben . 
letzteres betrug median 10 , 7 monate bei beobachtung und 10 , 9 monate nach wbrt [ 2 , 3 , 6 ]  . ob vorrangig die wbrt oder eher ein intrakranieller progress zur verschlechterung des allgemeinbefindens und der neurokognitiven funktion fhrt , ist gegenstand aktueller diskussionen . 
unerfreulicherweise knnen die ergebnisse der heute vorliegenden studien wegen meist geringer patientenzahl und unterschiedlich sensibler messinstrumente nicht eindeutig interpretiert werden [ 3 ]  . aus diesem grunde sollte bei patienten mit unklarer langzeitprognose ( > 912 monate ) nicht auf eine adjuvante wbrt verzichtet werden . 
die entscheidung sollte dann gemeinsam mit den betroffenen getroffen werden . bei den radioonkologen sollte ein in den letzten jahren leider weitgehend in vergessenheit gelangter aspekt der wbrt wieder ernsthaft bedacht werden , nmlich die fraktionierung der wbrt . 
unter dem eindruck der insgesamt schlechten berlebenschancen der patienten mit hirnmetastasen und der oft raschen progredienz des extrakraniellen tumorgeschehens wurden in den letzten jahren vermehrt kurzzeitschemata propagiert , weil einmalbestrahlungen mit 810 gy oder 10 fraktionen zu 3 , 0 gy als gleichwertig bezglich des unmittelbaren lokalen efkorrespondenzadresse i.a. 
hsu f , carolan h , nichol a et al ( 2010 ) whole brain radiotherapy with hippocampal avoidance and simultaneous integrated boost for 13 brain metastases : a feasibility study using volumetric modulated arc therapy . 
kocher m , soffietti r , abacioglu u et al ( 2011 ) adjuvant whole - brain radiotherapy versus observation after radiosurgery or surgical resection of one to three cerebral metastases : results of the eortc 2295226001 study . 
soffietti r , kocher m , abacioglu um et al ( 2013 ) a european organisation for research and treatment of cancer phase iii trial of adjuvant wholebrain radiotherapy versus observation in patients with one to three brain metastases from solid tumors after surgical resection or radiosurgery : quality - of - life results . 
rades d , schild se ( 2012 ) do patients with a limited number of brain metastases need whole - brain radiotherapy in addition to radiosurgery ? strahlenther onkol 188 : 702706 6 . 
insofern muss die hier kommentierte eortc - studie die diskussion befeuern , ob durch eine klinisch sinnvolle unterscheidung von patienten mit ungnstiger kurzund gnstiger langzeitprognose wieder unterschiedliche fraktionierungschemata eingesetzt werden sollten . 
adamietz , bochum strahlentherapieundonkologie52013 | original article strahlenther onkol 2013 189 : 387393 doi 10.1007 / s00066 - 013 - 0316 - 3 received : 6 september 2012 accepted : 16 january 2013 published online : 4 . 
ras is thus a relatively rare complication of bct , but its incidence is likely to increase as more women undergo this treatment [ 12 , 24 , 32 ]  . 
the prognosis of ras patients is poor and the reported 5 - year overall survival ( os ) rate varies from 10 to 38% [ 9 , 13 , 39 ]  . 
in many cases , surgery is unfeasible and even after obtaining negative margins by simple mastectomy , additional local tumors recur in approximately 70% of patients ( 29100% ) [ 3 , 7 , 13 , 16 , 20 , 23 , 28 , 29 ]  . 
results from five randomized trials have shown that the complete response ( cr ) rate for breast cancer recurrences increases from 41 to 59% when hyperthermia is combined with radiotherapy [ 36 ]  . 
multimodal therapies comprising surgery and rert + ht may improve local tumor control in the treatment of angiosarcoma [ 26 ]  . in an attempt to improve lc rates , we have treated ras patients with a combination of surgery wherever this was feasible , and rert + ht . 
results of a retrospective analysis are reported here . materials and methods patient characteristics between 2000 and 2011 , 24 patients with pathologically confirmed ras of the chest wall underwent surgery where feasible , and rert + ht . 
hyperthermia treatments were applied in the erasmus mc - daniel den hoed cancer center ( dhcc , n = 21 ) and the bernard verbeeten institute ( bvi , n = 3 )  . 
of the 24 patients , 23 had been treated for primary breast cancer by modified radical mastectomy followed by either radiotherapy ( n = 4 ) or bct ( n = 19 )  . 
the surgery was scored an r0 resection if no microscopic tumor was found at the margan r1 resection indicates a microscopically positive margin after an otherwise complete resection and r2 resection indicates gross residual disease left behind after mastectoradiotherapy following surgery or recurrence confirmed by biopsy , patients received elective external beam radiation weekly . 
all patients had received prior irradiation and were treated using a radiation technique comprising photons ( 615 mv linear accelerators ) , electrons ( 610 mev ) or a mixture of photons and electrons . 
 field size ranged from 175 to 1125 cm2 ( median : 444 cm2 ) [ 17 , 30 , 38 ]  . hyperthermia hyperthermia treatments at dhcc were given once a week following the radiotherapy , for a total of four treatments . 
temperatures were either measured interstitially and on the skin ( n = 18 ) , or only on the skin ( n = 6 )  . endpoints the primary endpoint of this study was defined by the duration of local control ( dlc )  . 
these patients had previously undergone breast conserving therapy ( bct , n = 18 ) , mastectomy with irradiation ( n = 5 ) or axillary lymph node dissection with irradiation ( n = 1 )  . 
in the subgroup of patients receiving surgery , the 3 - month , 1and 3 - year actuarial local control ( lc ) rates were 91 , 46 and 46% , respectively . 
the present study shows that rert + ht treatmenteither alone or combined with surgeryimproves lc rates in patients with ras . keywords survival rate radiotherapy breast cancer toxicity mastectomy wirkung einer kombination aus chirurgischer therapie , erneuter bestrahlung und hyperthermie auf die lokale kontrollrate bei strahleninduzierten angiosarkomen der brustwand zusammenfassung ziel . 
die wirksamkeit und nebenwirkungen von rebestrahlung und hyperthermie ( rert + ht ) allein oder in kombination mit vorhergehender oder nachfolgender operation wurden bei patienten mit einem ras der brustwand berprft patientenundmethoden . 
ras wurde bei 23 patientinnen mit brustkrebs und bei einer patientin mit malignem melanom , nach frherer brusterhaltender brustkrebstherapie ( n = 18 ) , mastektomie mit bestrahlung ( n = 5 ) und axillrer lymphknotendissektion mit bestrahlung ( n = 1 ) diagnostiziert . 
in der untergruppe von patienten mit chirurgie lagen die 3 - monats - , 1und 3 - jahres - lokalkon trollraten ( lc ) bei 91% , 46% und 46% . 
die vorliegende studie zeigt , dass rert + ht entweder allein oder in kombination mit chirurgie zu einer verbesserten lc - rate bei patienten mit ras fhrt . schlsselwrter berlebensrate radiotherapie brustkrebs toxizitt mastektomie last follow - up examination . 
 these included : the maximum ( tmax ) and the average temperature ( tave ) that was recorded over all temperature probes during the steady state period of each heating session ( beginning 10 min after the start of heating ) ; the temperature exceeded by 90% of all temperature probes during the steady state ( t90 ) and the thermal isoeffect dose expressed in cumulative equivalent minutes at a reference temperature of 43c , based upon the temporal development of t90 in the target ( cem43ct90 )  . 
the formulation for cem43ct90 used in this study has been previously described and used extensively [ 6 , 11 , 14 ]  . statisticalanalysis kaplanmeier analysis was performed for dlc and os duration . 
for analysis , the stata statistical software , release 11 was used ( statacorp , 2009 )  . results median age was 70 years , with a range of 46 to 88 years . 
surgery was perstrahlentherapieundonkologie52013 | original article duration of local control surgery no surgery tients with microscopic disease9 patients ( 56% ) exhibited cr , 4 ( 25% ) partial response , 2 ( 13% ) showed no change and 1 ( 6% ) had progressive disease . 
in the no - surgery group , 3 - months , 1and 3 - year lc rates were 54 , 32 and 22% , respectively and 4 patients had a recurrence on the chest wall between 6 and 51 months . 
none of the parameters showed a significant correlation with dlc , presumably due to the small number of patients included in the study . survival the median latency interval between previous radiation and diagnosis of ras was 106 months ( range : 45212 months )  . 
the 4 patients treated by complete resection and the 7undergoing incomplete resection had median survival times of 9 and 10 months , respectively . at the last follow - up , 5 patients were still alive 18 months after the start of treatment ( mean : 2 months ) ; 1 had distant metastases and 1 had both local failure surgery no surgery logrank p = 0.15 surgery no surgery at risk : months fig . 
 causes of death were locoregional recurrence ( n = 11 ) , distant metastases ( n = 3 ) and a combination of both ( n = 5 )  . toxicity the duration of hospitalization for the surgical procedure in 11 patients varied between 3 and 12 days . 
the other patient required debridement for a chronic wound . discussion secondary angiosarcomas have been associated with previous surgery , irradiation or long - standing extremity edema in stewart treves syndrome [ 19 ]  . 
 nevertheless , due to the multifocal growth of angiosarcoma and residual tumor tissue , nearly two - thirds of these patients developed a local recurrence , even if the surgical margins were considered free . 
 [ 16 ] reported a median os of 81 months for 9 patients in whom the tumor could be widely resected . combination therapy comprising surgery and re - irradiation seems to improve both lc and os in comparison to patients treated by surgery alone . 
 [ 28 ] reported 5 - year lc and os rates of 92% and 75% , respectively , among patients receiving postoperative hyperfractionated accelerated radiotherapy ( hart ) with 1 gy given three times daily to a total dose of 60 gy . 
 in the current study , postoperative hypofractionated rert + ht resulted in a 1and 3 - year lc rate of 46% , which is lower than that reported by palta et al . 
these differences may be due to patient selection criteria . the limitations of the current study are its retrospective nature and the relatively small sample size , which preclude firm conclusions . 
de bruijne m , holt b van der , rhoon gc van , zee j van der ( 2010 ) evaluation of cem43 degrees ct90 thermal dose in superficial hyperthermia : a retrospective analysis . 
hand jw , machin d , vernon cc , whaley jb ( 1997 ) analysis of thermal parameters obtained during phase iii trials of hyperthermia as an adjunct to radiotherapy in the treatment of breast carcinoma . 
herskind c , wenz f ( 2010 ) radiobiological comparison of hypofractionated accelerated partialbreast irradiation ( apbi ) and single - dose intraoperative radiotherapy ( iort ) with 50 - kv x - rays . 
marchal c , weber b , lafontan b de et al ( 1999 ) nine breast angiosarcomas after conservative treatment for breast carcinoma : a survey from french comprehensive cancer centers . 
nestle - krmling c , bolke e , budach w et al ( 2011 ) hemangiosarcoma after breast - conserving therapy of breast cancer : report of four cases with molecular genetic diagnosis and literature review . 
polgar c , strnad v , kovacs g ( 2010 ) partial - breast irradiation or whole - breast radiotherapy for early breast cancer : a meta - analysis of randomized trials . 
sauer r , creeze h , hulshof m et al ( 2012 ) concerning the final report hyperthermia : a systematic review of the ludwig boltzmann institute for health technology assessment , vienna , march 2010 . 
sautter - bihl ml , sedlmayer f , budach w et al ( 2012 ) when are breast cancer patients old enough for the quitclaim of local control ? strahlenther onkol 188 : 10691073 28 . 
seinen jm , styring e , verstappen v et al ( 2012 ) radiation - associated angiosarcoma after breast cancer : high recurrence rate and poor survival despite surgical treatment with r0 resection . 
styring e , fernebro j , jnsson pe et al ( 2010 ) changing clinical presentation of angiosarcomas after breast cancer : from late tumors in edematous arms to earlier tumors on the thoracic wall . 
matuschek c , blke e , roth sl et al ( 2012 ) longterm outcome after neoadjuvant radiochemotherapy in locally advanced noninflammatory breast cancer and predictive factors for a pathologic complete remission : results of a multivariate analysis . 
van der zee j , de bruijne m , mens jw et al ( 2010 ) reirradiation combined with hyperthermia in breast cancer recurrences : overview of experience in erasmus mc . 
vernon cc , hand jw , field sb et al ( 1996 ) radiotherapy with or without hyperthermia in the treatment of superficial localized breast cancerresults from five randomized controlled trials . 
wijnmaalen a , ooijen b van , geel bn van et al ( 1993 ) angiosarcoma of the breast following lumpectomy , axillary lymph node dissection , and radiotherapy for primary breast cancer : three case reports and a review of the literature . 
int j radiat oncol biol phys 26 : 135139 strahlentherapieundonkologie52013 | original article strahlenther onkol 2013 189 : 380386 doi 10.1007 / s00066 - 012 - 0281 - 2 received : 3 august 2012 accepted : 15 november 2012 published online : 23 . 
the use of imrt can significantly improve dose distribution for the breast resulting in reduced heart , lung and contralateral breast doses as well as improving the cosmetic outcome when compared to 3d conformal radiotherapy [ 1 , 4 , 9 ]  . there is great heterogeneity in what is defined as breast - imrt [ 21 ] , ranging from photon - only imrt [ 1 , 31 ] to mixed electron and photon imrt techniques with 2 [ 21 ] to 16 fields [ 30 ] applying various photon and electron beam energies . 
 regarding breast irradiation including regional lymph nodes , conventional 3or 4 - field conformal approaches fail to cover a volume that wraps around the chest wall in close proximity to the heart , lungs and spinal cord [ 22 ]  . 
 [ 3 ] investigated the number of beams necessary for optimal dose coverage of regional lymph nodes in breast and found that 4 - field imrt was a good choice . 
however , 9 and more beams are considered advantageous by others [ 14 , 21 , 31 ]  . rotational imrt techniques have been demonstrated to achieve not only better or comparable plan quality but also largely improve delivery efficiency when compared to step - and - shoot imrt in various indications ( e.g. , [ 6 ] )  . 
although imrt and vmat have been in clinical use for some time , the majority of studies evaluate breast only or breast / chest wall with internal mammary node ( imn ) coverage [ 14 , 21 ]  . 
few publications to date have addressed the role of imrt in lymph nodepositive breast cancer , and fewer involved investigation of vmat ( e.g. , [ 28 ] )  . furthermore , 6 mv is considered the general purpose imrt energy [ 3 ]  . 
regarding obese patients or patients with oversize breast volume ( > 2 , 000 cm3 and breast thickness > 7 cm ) , higher photon beam energy may show advantages over 6 mv . 
the aim of the present treatment planning study was to explore 4 - field imrt and vmat plans with 6 , 10 , and 15 mv photon beams for patients with node - positive left - sided breast cancer . methods and materials target volume delineation and organs at risk we selected ten ct scans of patients with left - sided breast cancer , who underwent breast conserving surgery . 
five patients were considered obese with a breast thickness larger than 7 cm ( range 710.5 cm ) and a breast volume larger than 2 , 000 cm3 ( range 2 , 0003 , 750 cm3 )  . 
patients were positioned in the supine position with arms raised above the head ( breaststep , it - v medizintechnik gmbh , austria )  . for all cases , the clinical target volume ( ctv ) consisted of the left breast , infraclavicular lymph nodes ( level iii ) and supraclavicular lymph nodes . 
the planning target volume ( ptvmc + ln ) was defined to include a 10 mm margin around the ctv in all directions except the posterior direction towards the lung , where a 7 mm margin was added . 
the boost ptvb was defined to include a 720 mm margin around the tumour bed in all directions . the left and right lung as well as the spinal cord were auto - contoured in the treatment planning system ( tps ) pinnacle3 ( v9.0 , philips radiation oncology systems , fitchburg , wi , usa ) using the model based segmentation option . 
additionally , the heart , contralateral breast and the oesophagus were considered as critical structures . treatment planning plans for both vmat and imrt were generated using the same tps , isocenter , dose grid ( 444 mm3 ) , prescriptions , and optimisation objectives in order to ensure fair treatment plan comparison . 
1 9 illustration of vmat ( left ) and four - field imrt ( right ) treatment plans with corresponding examples of segment shapes and digitally reconstructed radiographs for left - sided breast cancer ( red : ptvmc + ln ) sisting of ptvmc + ln and ptvb . 
the prescription dose was 50.4 gy to ptvmc + ln in 1.8 gy fractions and additional 10 gy in 2 gy fractions for ptvb . optimisation aid structures in terms of rings around the target volumes were applied as described previously [ 20 ]  . 
for imrt planning , ptvmc + ln was extended by 10 mm beyond the patient surface ( ptvlarge ) to accommodate the variation due to setup uncertainties and patient breathing . 
dose constraints for target volumes and organs at risk ( oar ) are listed in .tab.1. all plans were generated for an elekta synergy accelerator ( desktoppro rel.7.01 ; mlci with 1 cm leaf width ) using the collapsed cone algorithm of pinnacle3 . imrt plans were generated using four coplanar fields , consisting of two tangential beams and two additional , equidistant fields as illustrated in .fig.1. 
an average of 60 and 15 segments were optimised in typically 2530 iterations for ptvmc + ln and ptvb , respectively , using the direct machine parameter optimisation ( dmpo ) method [ 2 ]  . 
finally , 6 , 10 and 15 mv photon beam imrt plans were created for each patient and target volume . vmat plans were generated using a single rotation including an arc segment of up to 250 at a maximum allowed gantry rotation time of 90 s and gantry spacing at 4 . 
smartarc plan optimisation was performed during 100 iterations ; 6 , 10 and 15 mv photon beam vmat plans were created for each patient and target volume . plan comparison / plan evaluation all plans were normalised to ptvmc + ln and ptvb mean doses , respectively . 
d98% , d50% and d2% , indicating dose to 98% ( near - minimum dose ) , 50% and 2% ( near - maximum dose ) of both target volumes , were recorded . 
 [ 19 ] was evaluated : cipaddick = tv2 ( pitv ) , where tvpi is the target volume ( tv ) within the prescribed isodose volume ( pi )  . the dose to normal tissue was quantified by a volume vring which was introduced earlier [ 20 ]  . 
d2% and dmean were determined for all oar and vring from the composite plan . delivery efficiency was determined in terms of total treatment delivery time ( tt , time between the start of the first beam and the end of the last beam ) and number of monitor units ( mu ) for each target volume per fraction . plan verification for dose measurements , a 2d ionisation chamber array ( seven29 , ptw - freiburg , germany ) was inserted vertically into an octagonal solid water phantom ( octavius , ptw - freiburg ) [ 33 ]  . 
 the percentage of detectors with index < 1 and the mean were evaluated [ 17 ] applying the 3% / 3 mm criteria ( dose difference / distance to agreement ) to quantify dosimetric accuracy . strahlentherapieundonkologie52013 | original article abstract zusammenfassung all results were recorded as continuous variables ; mean and standard deviations were calculated . 
results for the oesophagus show 4 gy higher mean dose for obese breast size patients ( dmean = 30.7 gy ) compared to normal breast size patients ( dmean = 26.3 gy ) for both techniques . averaging all 10 patients , all target volume metrics of vmat plans showed negligible differences between high and low energy photon beams . 
for imrt plans , 6 mv again achieved best results in 17 out of 37 dose parameters , especially in d2% for both target volumes and oars . vmat plans were equal or superior in a pairwise comparison with imrt plans with respect to target coverage , homogeneity and delivery efficiency . 
we found on average 2% more normal tissue irradiated with low doses in vmat than in imrt . the manual and artiview plan evaluation coincided accurately ( difference < 1% ) for most of the observed dose metrics . 
v30 gy 382 | strahlentherapieundonkologie52013 strahlenther onkol 2013 189 : 380386 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0281 - 2 m.paslerd.georgs.barteltj.lutterbach node - positive left - sided breast cancer : does vmat improve treatment plan quality with respect to imrt ? abstract purpose . 
vmat for node - positive left - sided breast cancer retains target homogeneity and coverage when compared to imrt and allows maximum doses to organs at risk to be reduced . 
artiview enables fast and accurate plan evaluation . keywords volumetric modulated arc therapy intensity - modulated radiotherapy breast neoplasms lymph nodes linksseitiges mammakarzinom inklusive lymphabfluss : verbessert vmat die planqualitt gegenber imrt ? zusammenfassung ziel . 
mittels artiview knnen bestrahlungsplne schnell und genau evaluiert werden . schlsselwrter volumenmodulierte arc - therapie intensittsmodulierte strahlentherapie brustneoplasien lymphknoten for the heart was found to be up to 8% smaller and d98% was found to be on average 2.6% higher in the tps when compared to artiview results , respectively . plan verification results for the - index analysis are presented in .fig.3. 
r80% covers the area from 0.7 cm to 2 cm around the target volume , with maximum dose ( dmax ) < 80% of the prescribed dose doseconstraint dmean = 100% dmin95% dmax107% dmean = 100% dmax107% dmax80% dmax90% dmean = 100% ( weight 0.1 ) r80% r90% ptvlarge compositeplanconstraints lung left structure ptvmc + ln ptvboost oesophagus heart spinal cord lung right breast right vring d20% < 30 gy d30% < 20 gy dmean < 16 gy dmean < 28 gy dmax < 48 gy dmean < 9 gy dmax < 40 gy d10% < 20 gy d30% < 3 gy dmax < 30 gy dmean < 4 gy dmax < 10 gy dmean < 3 gy dmax < 6 gy dmean < 7 gy dmax < 35 gy tab . 
better ( + / + + ) or worse ( / ) results in at least 8 / 9 of 10 treatment plans are indicated ; no difference between techniques is shown with 0 . 
in general , imrt plans showed slightly higher dosimetric accuracy than vmat plans . discussion this study compared imrt and vmat plans for node - positive left - sided breast cancer patients using 6 , 10 and 15 mv high photon energy beams . 
this issue has been addressed by several authors [ 20 , 21 , 28 , 35 ] , but the clinical consequences are unknown at present . the large variations found in low doses , especially regarding the heart , might be explained by large variations in patient anatomy . 
although there is great awareness of the potential damage to the heart in left - sided breast cancer rt [ 16 ] , the radiobiology of the heart damage is only partially understood [ 23 ]  . 
there are no known safe levels of radiation to the heart at present [ 14 ]  . low dose irradiation raises the concern of developing a secondary malignancy [ 1 , 5 ] , especially regarding the contralateral breast [ 27 ]  . 
this effect was not found in patient plans with large breast size . the dose to the ipsilateral lung was found slightly increased in vmat plans ; however , v20 gy and v30 gy were always within the tolerance . 
4 8 polar diagram of monitor unit distribution ( red ) and the corresponding 1 / 10 open field area ( black ) for a representative vmat plan of pulmonary complications in radiation treatment for breast cancer is reported to be rare within this tolerance [ 15 ]  . oesophageal toxicity has been correlated with mean doses greater than 34 gy [ 24 ]  . 
 however , larger target volumes of obese breast size patients were found to correlate with higher mean dose to the oesophagus compared to normal breast size patients , again due to unfavourable geometry . in this study , intrafraction motion was taken into account for imrt by using adequate margins in the plan optimisation . 
artificial soft - tissue equivalent expansion of 2 cm of the body in the region of the breast was therefore proposed to account for breast motion during rotational imrt [ 18 , 30 ]  . the monitor unit distribution for a representative vmat plan and the corresponding open field area are illustrated in .fig.4. 
as can be seen , high dose rate fluctuation occurs throughout the plan and only a minimal mu contribution comes from gantry angles 340 to 50 because of oar constraints . 
better ( + / + + ) or worse ( / ) results in at least 8 / 9 of 10 treatment plans are indicated ; no difference between techniques is shown with 0 . 
this may originate from the fact that smartarc uses continuous , variable dose - rates in the optimisation process , whereas the linac under study is bound to binned dose - rates . 
artiview provides fast and accurate plan evaluation . in this study , photon beam energy variation in imrt and vmat for left - sided node - positive breast cancer plans was investigated for the first time . 
 recently , flattening filter free approaches ( fff ) [ 11 ] became clinically available and provide promising results for chest wall radiotherapy [ 25 , 28 ] , which should strahlentherapieundonkologie52013 | 24 . 
singh ak , lockett ma , bradley jd ( 2003 ) predictors of radiation - induced esophageal toxicity in patients with non - small cell lung cancer treated with three - dimensional conformal radiotherapy . 
stock m , kroupa b , georg d ( 2005 ) interpretation and evaluation of the gamma index and the gamma index angle for the verification of imrt hybrid plans . 
stovall m , smith s , langholz b et al ( 2008 ) dose to the contralateral breast from radiotherapy and risk of second primary breast cancer in the wecare study . 
subramaniam s , thirumalaiswamy s , srinivas c et al ( 2012 ) chest wall radiotherapy with volumetric modulated arcs and the potential role of flattening filter free photon beams . 
vandecasteele k , de neve w , de gersem w et al ( 2009 ) intensity - modulated arc therapy with simultaneous integrated boost in the treatment of primary irresectable cervical cancer . 
van esch a , clermont c , devillers m et al ( 2007 ) on - line quality assurance of rotational radiotherapy treatment delivery by means of a 2d ion chamber array and the octavius phantomed phys 34 : 38253837 34 . 
wiezorek t , schwahofer a , schubert k ( 2009 ) the influence of different imrt techniques on the peripheral dose : a comparison between smlm - imrt and helical tomotherapy . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 367371 doi 10.1007 / s00066 - 012 - 0296 - 8 received : 20 august 2012 accepted : 6 december 2012 published online : 4 . 
april 2013 springer - verlag berlin heidelberg 2013 g.faddag.massazzas.zuccas.durzug.meleddum.possanzinip.farace department of radio - oncology , regional oncological hospital , cagliari quasi - vmatinhigh - grade gliomaradiationtherapy introduction radiation therapy of high - grade gliomas is often complex due to the close proximity of tumours to organs at risk ( oar ) such as brainstem , chiasm , optic nerves and eyes . 
the improvements in prognosis for high - grade gliomas achieved by combined chemoradiotherapy [ 1 ] , mean that late radiation effects are becoming an increasingly important consideration . intensity modulated radiation therapy ( imrt ) could represent an effective tool in the treatment of high - grade gliomas [ 2 ]  . 
 however , large - scale implementation and clinical application of imrt is hampered by the impact of the increased planning , delivery and verification times on human and departmental resources [ 4 ]  . intensity modulated arc therapy ( imat ) was proposed as an extension of imrt . 
vmat delivers beams from apertures of varying weights with a single - arc rotation that uses the dose - rate variation of the treatment machine [ 5 ] , which has been investigated for different tumour sites [ 6 , 7 , 8 ]  . 
vmat has also been investigated in high - grade gliomas , where shorter treatment times were demonstrated than for imrt [ 9 ] and target coverage was only a slightly reduced [ 10 ]  . another approach to reducing treatment times is the development of a fast method which uses more beams than is typical for imrt , each beam having only one segment [ 11 ]  . 
even hospitals not equipped with systems capable of vmat delivery ( linacs and treatment planning ) can apply qvmat . in the present study , a qvmat technique was compared with 3d - crt and imrt ( the latter being considered a reference technique ) with regards to the feasibility of large - scale implementation of qvmat for therapy of high - grade gliomas in hospitals with limited departmental resources . materials and methods subjects and volume delineations twelve patients with high - grade gliomas ( who grade iiiiv ) where included in the analysis . 
all of the patients underwent radiochemotherapy with temozolomide and received a total dose of 60 gy in 30 fractions . gross tumour volume was defined as the tumour contrast enhancement in t1weighted magnetic resonance imaging . 
 the gross tumour volume and the postoperative tumour bed were expanded by 2 cm ( in three dimensions ) along anatomic routes of spread to create the clinical target volume ( ctv )  . 
no margin was added to the oars . for all 12 patients included in the study , the ptv overlapped at least one oar and was in close proximity to others . 
downstream of the initial consecutive selection , 2 patients were excluded from the analysis since there was no overlap between ptv and oar ( the patients ctvs were 234 and 200 cm3 and the ptvs were 361 and 304 cm3 , respectively )  . 
where possible , just two perpendicular fields were useda lateral and a superior anterior oblique field ( couch angle of 90 , gantry angles varying from 0 to 90 )  . 
imrt ( without ring ) p < 0.05 comparing qvmat with and without the ring ( around ptv ) objective #p < 0.05 comparing imrt with and without the ring ( around ptv ) objective . length through normal brain and prohibition of exit through the oral cavity [ 14 ]  . 
the beam weights were chosen to maximize dose homogeneity to the ptv , while maintaining the dose received by the oars below the maximum acceptable levels . the qvmat plan comprised 15 coplanar 6 mv photon beams arranged at equi spaced gantry angles . 
the calculation was then iterated 13 times , changing the objective weights to obtain an optimal dose distribution . static step - and - shoot imrt was planned using nine 6 mv coplanar photon beams at equispaced gantry angles . 
in368 | strahlentherapieundonkologie52013 verse planning was performed by dmpo , with a 4 cm2 minimum segment area and a segment weight limited to 4 monitor units ( mu )  . 
the maximum number of segments was limited to 80 , since although a dosimetric gain for more complex cases can be achieved by increasing the number of apertures per beam direction , only modest improvements are observed beyond nine apertures per beam direction [ 15 ]  . 
to compare a quasi - volumetric modulated arc therapy ( qvmat ) with threedimensional conformal radiation therapy ( 3d - crt ) and intensity - modulated radiation therapy ( imrt ) for the treatment of highgrade gliomas . 
3d - crt was planned using 23 non - coplanar beams , whereby the field - infield technique ( fif ) was used to divide each field into 13 subfields to shield the oar . 
inverse planning for qvmat and imrt was performed by direct machine parameter optimization ( dmpo ) to deliver a homogenous dose distribution of 60 gy within the ptv and simultaneously limit the dose received by the oars to the recommended values . 
the qvmat method could be applied in hospitals , for example , which have limited departmental resources and are not equipped with systems capable of vmat delivery . keywords radiotherapy organs at risk hospital radiochemotherapy maximum dose bestrahlung hhergradiger gliome mit der quasi - vmat - methode zusammenfassung ziel . 
quasi volumetrisch modulierte rotationsbestrahlung ( qvmat ) mit einer konformalen 3 - d - bestrahlung ( 3d - crt ) und einer intensittsmodulierten bestrahlung ( imrt ) bei der behandlung von massiven gliomen zu vergleichen . 
die 3d - crt - bestrahlungsplanung erfolgte ber 23 nichtkoplanare felder , wobei zur schonung des risikoorgans bei jedem feld eine feld - in - feldtechnik mit 13 subfeldern angewendet wurde . 
um eine homogene dosisverteilung im ptv von 60 gy bei gleichzeitiger schonung des risikoorgans zu erreichen , wurde die bestrahlungsplanung fr die techniken qvmat und imrt mit der direct machine parameter optimization ( dmpo ) durchgefhrt . 
 the only exceptions were the ipsilateral oars in patients #5 ( eye ) and #10 ( eye , optic nerve and lens ) , where higher values were accepted due to a very close proximity to the ctv . 
no significant difthe maximum dose received by normal brain ( brain tissue outside ptv ) was significantly lower in qvmat and imrt plans in comparison to 3d - crt ( about 2 gy lower on average )  . 
on comparison of qvmat / imrt with 3d - crt , a significant increase in nb dmean was observed , with higher v45 gy and v24 gy but with no significant differences in the lower doses ( 10 gy )  . finally , the calculated treatment times ( mean standard deviation ) were 35732 s , 35918 s and 59750 s , for 3dcrt , qvmat and imrt , respectively . 
 dose delivery by qvmat took no longer than for 3d - crt , whereas the imrt dose delivery time was significantly longer . dose escalation [ 16 ] , boost irradiation [ 17 ] and simultaneous integrated boost irradiation [ 18 ] are topics of continuous investigation for the treatment of high grade gliomas . 
despite this , these methods are still often applied using a conventional fractionation scheme that uniformly delivers 60 gy in 30 fractions to a large target volume encompassing the surgical cavity plus a margin accounting for microscopic infiltration . to compare a 15 - beam qvmat technique with 3d - crt and a 9 - beam static imrt method , the present study applies a conventional 60 gy treatment scheme to 12 patients . 
wagner d , christiansen h , wolff h , vorwerk h ( 2009 ) radiotherapy of malignant gliomas : comparison of volumetric single arc technique ( rapidarc ) , dynamic intensity - modulated technique and 3d conformal technique . 
chan mf , schupak k , burman c et al ( 2003 ) comparison of intensity - modulated radiotherapy with three - dimensional conformal radiation therapy planning for glioblastoma multiforme . 
cardinale r , won m , choucair a et al ( 2006 ) a phase ii trial of accelerated radiotherapy using weekly stereotactic conformal boost for supratentorial glioblastoma multiforme : rtog 0023 . 
macdonald sm , ahmad s , kachris s et al ( 2007 ) intensity modulated radiation therapy versus threedimensional conformal radiation therapy for the treatment of high grade glioma : a dosimetric comparison . 
hermanto u , frija ek , lii mj et al ( 2007 ) intensitymodulated radiotherapy ( imrt ) and conventional three - dimensional conformal radiotherapy for high - grade gliomas : does imrt increase the integral dose to normal brain ? int j radiat oncol biol phys 67 ( 4 ) : 11351144 for a significantly better and more homogeneous ptv coverage than 3d - crt . 
this could be reduced even further by applying a ptv ring objective , which gave rise to higher ci values ( also in the imrt plans ) that were accompanied by only a limited reduction in ptv coverage . for normal brain , v45 gy , and v24 gy were higher in the qvmat and imrt plans ( as reported by other authors [ 3 , 19 ] )  . 
in agreement with other authors [ 21 ] , we did not observe any significant differences in normal brain when comparing different plans at lower doses ( < 10 gy )  . with the exception of the ipsilateral oars in 2 patients , the maximum doses were always maintained below the tolerance levels at oars . 
the comparison of the techniques has to consider both the average values for a patient ( which were slightly lower for 3d - crt ) and the individual values in the more difficult cases ( which were usually higher for 3d - crt )  . our results are in agreement with those previously reported using true vmat by wagner et al . 
however , qvmat can be easily applied in hospitals that are not equipped with systems capable of true vmat delivery ( linacs and treatment planning )  . additionally , qvmat planning may be less dependent on operator ability than 3d - crt planning and the technique does not require any additional time for dose delivery . 
department of internal medicine , universittsmedizin mannheim , medical faculty mannheim , heidelberg university , mannheim 4 institute of diagnostic radiology and nuclear medicine , universittsmedizin mannheim , medical faculty mannheim , heidelberg university , mannheim 5 department of surgery , universittsmedizin mannheim , medical faculty mannheim , heidelberg university , mannheim 6 ii . 
department of internal medicine , university hospital jena adjuvantimrt / xelox radiochemotherapyimproves long - termoverall - anddisease - free survivalinadvancedgastriccancer adjuvant radiochemotherapy has been shown to improve survival rates in patients with locoregionally advanced gastric cancer [ 1 ]  . 
for the first time in a randomised setting , the intergroup study 0116 ( int - 0116 ) demonstrated significant improvements in overall survival ( os ) and disease - free survival ( dfs ) using adjuvant 5 - fluorouracil / folinic acid ( 5 - fu / fa ) and 45 gy locoregional irradiation [ 2 ]  . 
a large non - randomised analysis from korea [ 4 ] also revealed a beneficial effect of adjuvant radiochemotherapy in a patient population that had undergone adequate d2 lymph node dissection . 
since sufficiently large radiotherapy ( rt ) target volumes seemed to be essential in the intergroup trial [ 12 ] , we started using larger intensitymodulated radiation therapy ( imrt ) target volumes and introduced a prospective treatment protocol using modern chemotherapy doublets [ 13 ]  . 
retrospective analy sis of these data reveals improved survival rates in patients with advanced gastric cancer who receive adjuvant radiochemotherapy with imrt plus modern chemotherapy doublets , compared to those receiving three - dimensional conformal radiotherapy ( 3d - crt ) plus conventional chemotherapy [ 14 ]  . the main problems associated with gastric rt include acute side effects that lead to interruption of therapy and also late side effects . 
this provides optimal target coverage , while reducing the total dose and dose per fraction received by the filtering parts of the kidneys [ 17 , 18 ] , as compared to 3d - crt [ 14 , 19 ]  . preliminary analyses of serum creatinine levels and clinical symptoms from our group and others suggest that chronic renal toxicity might be lower using imrt [ 14 ]  . 
however , the relevance of most of these data is limited by short follow - up times and a lack of comprehensive endpoint analysis in terms of renal function . here we report on the long - term outcomes of the two previously analyzed consecutive patient cohorts . 
the latter later cohort ( 1 3dcrtand 27 imrtpatients ) underwent predominantly xelox treatment within the framework of a phase i / ii trial by the mannheim working group for gastrointestinal tumors ( mannheimer arbeitsgruppe fr gastrointestinale tumoren , margit ) and the working group for internal oncology ( arbeitsgemeinschaft fr internistische onkologie , aio ) of the german cancer society . 
briefly , two courses of capecitabine ( 1000 mg / m2 twice daily on days 114 ; repeated from day 22 ) and oxaliplatin ( 130 mg / m2 on days 1 and 22 ) were applied before and after rt with antiemetic prophylaxes as recommended by international guidelines ( 5 - ht3 receptor antagonists and dexamethasone )  . 
in a retrospective analysis , adjuvant intensity - modulated radiation therapy ( imrt ) combined with modern chemotherapy improved advanced gastric cancer survival rates compared to a combination of three - dimensional conformal radiation therapy ( 3d - crt ) and conventional chemotherapy . 
between 2001 and 2008 , 65 consecutive gastric cancer patients received either 3d - crt ( n = 27 ) or imrt ( n = 38 ) following tumor resection . 
chemotherapy comprised predominantly 5 - fluorouracil / folinic acid ( 5 - fu / fa ) in the earlier cohort and capecitabine plus oxaliplatin ( xelox ) in the latter . 
after a median follow - up period of over 5 years , os and dfs were improved in the imrt / xelox treated patients compared to the 3d - crt / 5 - fu / fa group . 
long - term observation revealed no clinical indications of therapy - induced secondary tumors or renal toxicity . keywords radiotherapy chemotherapy renal function gastroesophageal junction toxicity adjuvante imrt / xelox - radiochemotherapie verbessert das gesamtund krankheitsfreie berleben beim fortgeschrittenen magenkarzinom zusammenfassung zielsetzung . 
in einer retrospektiven analyse verbesserte die adjuvante radiochemotherapie mit intensittsmodulierter strahlentherapie ( imrt ) und moderner chemotherapie das berleben von patienten mit lokal fortgeschrittenem magenkarzinom gegenber der kombination aus 3 - dimensionaler konformaler strahlentherapie ( 3d - crt ) und konventioneller chemotherapie . 
die langzeitbeobachtung erbrachte keine klinischen hinweise auf nephrotoxizitt oder therapiebedingte sekundrtumoren . schlsselwrter radiotherapie chemotherapie nierenfunktion gastrosophagealer bergang toxizitt the primary end points of the present evaluation were overall survival ( os ) and disease - free survival ( dfs )  . 
for imrt , daily 3d image guidance employed either cone beam computed tomography ( cbct ) and / or stereotactic ultrasound , aimed at maximal kidney sparing and homogenous dose distribution within the planned target volume ( ptv )  . 
 relapse was diagnosed by cross - sectional imaging and confirmed histologically where possible and clinically appropriate . data analysis and statistics os and dfs were recorded and subject to actuarial analysis . 
os was calculated from the day of surgery until either the day of death ( event ) or the day of the last follow - up ( follow - up censored data )  . 
dfs was calculated from the day of surgery until either the day of relapse or death ( events ) , or the last follow - up without relapse ( censored where patient exhibited no evidence of disease at the last follow - up )  . in order to compare the two treatment groups in terms of a nominal parameter , a 2or fishers exact test was used , as appropriate . 
a test result with 0.05 < p < 0.10 was considered to represent a trend toward significance . late toxicity ( > 90 days ) evaluation was based on clinical symptoms and graded according to the common terminology criteria for adverse events ( ctcae ) scale , v . 
in univariate analysis , only ajcc tumor ( p = 0.0011 ) and nodal stage ( pn , p = 0.0001 ) were found to have a statistically significant influence on os . 
none of the other prognostic factors examinedgender , pathological stage ( pt ) , metastases ( pm ) , number of dissected nodes , tumor location , grade d1 / d2 dissection , vascular or lymphatic vessel invasion and resection statusinfluenced os significantly . 
diarrhea and abdominal distension were suffered by 2 patients ( grade 1 and 2 ) and 1 patient experienced grade 1 nausea . in the imrt group ( 12 patients could be assessed ) , 16% of patients suffered from diarrhea ( 8% grade 1 and 8% grade 2 )  . 
 nausea was experienced by 16% ( 8% grade 1 and 8% grade 3 ) , abdominal distension by 24% ( grades 1 , 2 and 3 ; each 8% )  . 
flatulence was reported by 16% of the patients ( 8% grade 2 and 8% grade 3 ) and abdominal pain by 24% ( grades 1 , 2 and 3 ; each 8% )  . general symptoms reached a maximum of grade 3 in both groups , with anxiety , fatigue and irritability being the main complaints . maximum skin toxicity was grade 2 in both groups ( hyperpigmentation and dry skin in the irradiation field , as well as post - chemotherapy nail symptoms )  . 
the only additional tumor observed in a surviving patient was prostate cancer in a 59 - year - old patient , 4 years after treatment for gastric cancer . chronic renal toxicity based on clinical symptoms and laboratory parameters creatinine levels were available for 4 living patients in the 3d - crt group and 16 living patients in the imrt group . 
 the last available creatinine value was 0.960.15 mol / l ( mean value standard deviation ) in the 3d - crt group ( time after rt 96118 months ) and 0.930.21 mol / l in the imrt group ( 12 107 months post rt )  . no clinical signs of renal toxicity ( hypertension , edema ) were observed in either group . discussion survival of patients with locally advanced gastric and ge junction cancer is not yet satisfactory , but has improved recently . 
the cross study ( in which about 25% of patients had adenocarcinoma of the ge - junction ) reported a survival benefit of preoperative radiochemotherapy in patients with esophageal and ge junction cancer ( predominantly adenocarcinoma ) [ 7 ]  . 
the role of neoadjuvant radiochemotherapy is a topic of controversial discussion that is currently being investigated in the trans - tasman radiation oncology group ( trog ) trial of preoperative therapy for gastric and esophagogastric junction adenocarcinoma ( topgear , trog 0808 ) study in patients with ge junction tumors . long - term follow - up of our series one of the largest retrospective analyses of a clinical series comparing imrt / xelox with 3d - crt / 5 - fu / fa , with the longest follow - up reported to datesuggests that a combination of advanced radiation technique with image - guided imrt and modern chemotherapy doublets improves both os and dfs significantly . 
similar to the recently published southwest oncology group ( swog ) 10 - year data from the int0016 / swog9008 trial [ 3 ] which reports a median dfs of 27 months and os of 35 months for the chemoradiotherapy armour data remain stable with longterm follow - up . 
the 4 - year data available for the magic study report an os of 36% in the chemotherapy arm . a median os of 43 months and a 5 - year survival rate of 39% in the imrt group for t24n + patients is superior to the previously published results of a study with a similar disease - stage distribution ( 5 - year survival rates : pt3 ; 24% , pt4 ; 16% , pn1 ; 36% and pn2 ; 27% ) [ 25 ]  . considering the retrospective nature of this evaluation , the factors having a positive influence on the imrt group cannot be exactly defined . 
although identical rt doses were applied in both cohorts , the ptv was significantly larger in the imrt group , because we hypothesized that it could be expanded without prohibitive kidney exposure . 
morphological and functional ( 1 ) h and ( 23 ) na magnetic resonance imaging ( mri ) has been used for the first time at our hospital to evaluate renal status in patients following 3d - crt and imrt [ 26 ]  . 
evaluation of the whole imrt cohort with this method is currently underway . recently , the adjuvant chemoradiation therapy in stomach cancer ( artist ) trial impressively demonstrated the value of adjuvant radiotherapy for t4 / n + patients . 
this suggests an improvement in these patients , despite statistical tests not reaching significance in this subgroup or the total cohort [ 27 ]  . the imrt treatment approach presented here results in moderate toxicity , such that most patients are able to complete the radiation series and a combination with modern chemotherapy doublets 422 | strahlentherapieundonkologie52013 is possible [ 13 ]  . 
studies employing larger populations are necessary for further investigation . several problems typical for retrospective evaluations preclude meaningful subgroup analyses and hypothesis generating conclusions : the study period was relatively long . 
with a disease process as complex as that of gastric cancer where the relative importance of various prognostic factors is not yet completely clearonly well designed , controlled randomized trials would be able to precisely determine the merit of various adjuvant strategies . 
in all , the work presented here indicates long - term sustainability of the encouraging results initially reported for the combination of imrt and modern chemotherapy doublets in t3 / t4 / n + gastric cancer . 
schuhmacher cp , fink u , becker k et al ( 2001 ) neoadjuvant therapy for patients with locally advanced gastric carcinoma with etoposide , doxorubicin , and cisplatinuclosing results after 5 years of follow - up . 
haneder s , michaely hj , schoenberg so et al ( 2012 ) assessment of renal function after conformal radiotherapy and intensity - modulated radiotherapy by functional ( 1 ) h - mri and ( 23 ) na - mri . 
lee j , lim do h , kim s et al ( 2012 ) phase iii trial comparing capecitabine plus cisplatin versus capecitabine plus cisplatin with concurrent capecitabine radiotherapy in completely resected gastric cancer with d2 lymph node dissection : the artist trial . 
janka , hieber , mhe , degott , winter , schfer , kirsch , slesina , utz , massner , wehrmann , burkart , stein , scholtze , hornung and kleiss for providing clinical information and laboratory values . 
there are no conflicts of interest . original article strahlenther onkol 2013 189 : 401406 doi 10.1007 / s00066 - 013 - 0313 - 6 received : 21 september 2012 accepted : 16 january 2013 published online : 23 . 
mrz 2013 springer - verlag berlin heidelberg 2013 l.zhengj.zhangt.songj.zhangg.yuy.zhang department of oral and maxillofacial surgery , peking university school and hospital of stomatology , beijing 125iseedimplantbrachytherapy forthetreatmentofparotidgland cancersinchildrenandadolescents salivary gland neoplasms are rare in children and adolescents and less than 5% of all salivary gland tumors are found in patients 16 years of age [ 1 ]  . 
the frequency of individual salivary neoplasms is most common in the parotid gland and most parotid gland tumors in children and adolescents are malignant [ 2 , 3 , 4 , 5 , 6 ]  . 
radiation , when recommended in children , has similar indications to those for adult patients [ 2 , 7 , 8 ]  . 125i seed brachytherapy remains an attractive option for radiating limited volumes with higher doses to improve local control in malignant parotid gland tumors [ 9 ]  . 
this paper presents our experience with 12 cases of parotid cancers occurring in children who were treated with 125i seed implant brachytherapy . patients and methods patients between october 2003 and november 2008 , 12 patients ( 7 boys and 5 girls ) aged between 1 and 15 years were included in this retrospective study . 
all patients had malignant tumors as determined by pathological examination of wax sections . no patient had neck dissection because no evidence showed neck lymph node metastasis in clinical examination and ct scan . seed implantation treatment planning treatment planning for all patients was designed by a computerized treatment planning system ( rt - rsi ; beijing atom and high technique industries inc . , beijing , china )  . 
the planning target volume ( ptv ) was defined at 1015 mm beyond the preoperative gross tumor volume ( gtv ) and the postoperative bed from computerized tomography ( ct ) scans in combination with target area as recorded by intraoperative photographs . 
dosages delivered to organs at risk were designed within acceptable limits of tolerance by the computerized treatment planning system . 125i seed implantation the implantation of radioactive seeds was performed at approximately 2 weeks postoperatively in all patients after wound healing had been achieved . 
 the interstitial needles ( 18 - gauge , stainless steel , hollow needles ) were inserted into the target area ( with a 0.5 cm margin ) , 1 cm apart . 
toxicity was graded according to the radiation therapy oncology group ( rtog ) grading system and the national cancer institute common toxicity criteria ( version 3.0 ; [ 10 ] )  . descriptive statistics were calculated for patient and tumor characteristics , treatment features , and toxicities . 
overall and diseasefree survival rates were calculated using the kaplanmeier method . results eight patients with t2 were followed up for 47104 months ( average follow - up period 81 months )  . 
skin effects in all the patients with t2 had recovered within 12 months of seed implantation ( .fig.2d ) , and all the patients with t4b had developed permanent skin pigmentation . 
no keloid scarring was observed in the field of the operation . before treatment , facial nerve function was recorded in all patients with t2 and 3 patients with t4b according to the h - b systetwo patients with t2 and 3 patients with t4b had weakness only of the marginal branch of the facial nerve , corresponding to h - b grade ii paresis . 
three were h - b grade iii , with slight movement of the forehead possible in two , and slight and weak mouth opening with maximum effort possible in the third . 
for parotid gland cancers in children , 125i seed implant brachytherapy may be an acceptable treatment without serious complications and with satisfactory short - term effects . keywords brachytherapy parotid gland neoplasms children adolescents brachytherapie mit 125i - seed - implantation zur behandlung von parotiskarzinomen bei kindern und jugendlichen zusammenfassung hintergrundundziel . 
fr k rebserkrankungen der ohrspeicheldrse bei kindern kann eine brachytherapie mit einer 125i - seed - implantation eine akzeptable behandlung ohne schwer wiegende komplikationen und mit zufriedenstellender kurzfristiger wirkung sein . schlsselwrter brachytherapie ohrspeicheldrse neoplasien kinder jugendliche the patient with temporal branch anastomoses recovered to h - b grade iii . discussion parotid gland malignant tumors are rare in children , and as a result , there is a lack of optimal treatment strategies for the management of this condition . 
the routine treatment of malignant parotid gland tumors in adults involves extensive excision , and if the facial nerve is adherent to the tumor , it is always sacrificed [ 11 , 12 ]  . 
surgery needs to ensure preservation of the facial nerve in children unless the nerve is directly invaded or the intact nerve limits resection [ 7 , 13 , 14 ]  . 
in the present study , the facial nerve was carefully dissected during surgery in 8 patients with t2 , in 1 case the temporal branch was cut and required nerve anastomosis . 
d a typical transverse slice shows the distributions of the 125i seeds and isodose curves of the patient underwent postoperative 125i seed implant brachytherapy system , facial nerve function had recovered to the level of grade iii . radiotherapy is often used in case of residual disease , high - grade tumors , perineural and vascular invasion , soft tissue extension , large lesions , and multiple level nodal metastases [ 7 , 15 ]  . 
it is reported that a case with recurrent high grade mucoepidermoid carcinoma was successfully treated by reirradiation in combination with cetuximab and that accelerated radiotherapy using the concomitant boost technique is feasible in patients with locally advanced head and neck cancer [ 16 , 17 ]  . 
its main advantage over external radiotherapy derives from its enhanced conformality and rapid dose fall off , thus , delivering biologically higher doses to the 404 | strahlentherapieundonkologie52013 tumor while at the same time reducing the dose to adjacent normal structures at a very low dose rate ( 0.070.09 gy / h initial dose rate , t1 / 2 = 60 days ) [ 20 , 21 ]  . 
 [ 22 , 23 ] have shown that the low dose rates achieved by 125i ( 0.070.09 gy / h ) produced less tumor growth delay than that produced by the higher dose rates achieved by pd - 103 ( 0.170.20 gy / h )  . 
during follow - up , all patients who had received seed implantation brachytherapy had no long - term trismus , dentofacial deformity , osteoradionecrosis , or secondary malignant changes . the local recurrence rate of primary parotid carcinoma is 1332% , and most cases have tumor recurrence within 3 years of the initial treatment [ 24 ]  . 
none of the 8 patients with t2 or 3 patients with t4b had tumor recurrence during the follow - up period , and only 1 patient with t4b died of pulmonary metastasis 41 months after the seed implantation . 
although this followup period is relatively short , good control was achieved in all patients . there are some reports in the literature that 510% of children treated for first malignancy have developed subsequent second tumors with long follow - up time [ 25 , 26 ]  . 
the important radiation - induced second malignant tumors are central nervous system tumors , thyroid tumors , osteosarcoma , soft tissue sarcomas , and non - melanoma skin cancer [ 27 ]  . 
in this original article strahlenther onkol 2013 189 : 407416 doi 10.1007 / s00066 - 013 - 0332 - 3 received : 19 december 2012 accepted : 13 february 2013 published online : 5 . 
the focus of research on the survival of patients with pancreatic cancer is dominated by distant metastases [ 1 , 2 ] , but the importance of local control is often forgotten [ 3 , 4 ]  . 
furthermore , radiation dose escalation is possible [ 8 , 9 ] and intensity modulated radiotherapy ( imrt ) was shown to increase the 2 - year local control rate from 38 [ 10 , 11 ] to 59% [ 1 , 7 , 11 , 12 , 13 , 14 , 15 ]  . lymphatic spread is an important prognostic factor of pdac , and the presence of metastatic lymph nodes is a predictor of local failure [ 6 ]  . 
although some radiation oncologists include elective lymph nodes ( elns ) into the target volume [ 16 , 17 , 18 , 19 ] , others only irradiate the primary tumor ( gross tumor volume ; gtv ) without the elns so as to increase the dose delivered to the gtv [ 10 , 20 ]  . 
this debate is very similar to the one for patients with non - small - cell lung cancer where a considerable dose is often delivered incidentally to the high - risk nodal volumes [ 21 ]  . several studies have described how to define the lymph node regions to be treated [ 16 , 17 , 19 , 22 ] , but there is no comparative literature on the extent to which specific elns are anatomically covered by the main ptvs to help choose the appropriate approach . 
 for the oxford ( based on our previous work [ 16 ] ) and radiation therapy oncology group ( rtog ) [ 19 ] methods , the planning target volume ( ptv ) includes the gtv with margins plus additional elns , i.e. , clinical target volume ( ctv ) , while the scalop ( selective chemoradiation in advanced localised pancreatic cancer trial ; nct01032057 , clinicaltrials . gov ) and the michigan methods [ 10 ] only include the gtv without elns . patients and methods we used the planning computer tomography sets ( 2.5 - mm slides ; performed with intravenous contrast in full exhale position ) of 11 consecutive patients with locally advanced , inoperable pdac of the pancreatic head who had undergone concurrent chemoradiation from january 2009 as part of the randomized phase ii clinical trial arc - ii ( eudract 2008 - 00630242 )  . 
the study was approved by the appropriate ethics committee and was performed in accordance with the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . oxford contouring method the gtv , ctv , and ptv were outlined as previously described [ 16 , 17 ]  . 
 similarly to the michigan method , no elns were included in the outlined ptv . to calculate the percentage of ctv coverage by each of the four ptvs ( oxford , rtog , scalop , michigan ) , the volume of ptv that overlapped with the ctv ( ptvctv ) was defined as shown in .fig.1. 
all contoured volumes were calculated in cm3 . statistical analysis the significance of differences between the means was measured with the wilcoxon signed - rank test or anova using the bonferroni test with graphpad prism 4.0. 
 comparison of the percentage of ctv coverage between ( a ) ptv_oxford and ptv_rtog ( both approximately 80% ) and ( b ) between ptv_ scalop and ptv_michigan ( approximately 60% and 50% , respectively ) revealed no statistically significant difference for any of the four peripancreatic ctvs . 
the ctv_para_ox and ctv_ivc_ ox were merged to form the aortocaval lymph nodes ( ctv_paraivc_ox )  . the oxford ctv for the pv was defined similarly to the rtog method [ 19 ] , but on the right lateral side only to the level of the junction of the cystic duct with the common bile duct , which is the craniolateral edge of the lymphatic dissection of the hepatoduodenal ligament . 
 as with the rtog contouring method , a margin of 10 mm was added in all directions , except in the right lateral direction , to create the ctv ( ctv_pv_ox ) in order to protect the liver parenchyma . 
the ct and sma and their corresponding ctvs ( ctv_ct_ox and ctv_ sma_ox , respectively ) were defined and contoured similarly to the rtog protocol except that the posterior ctv margin was restricted to 5 mm within the anterior part of the aorta . 
we have included a detailed description of the step - by - step contouring of the ptv_oxford protocol in the supplementary figures ( .figs.6 , 7 , 8 , 9 )  . contouringofthe peripancreaticlymphnodes although the oxford method does not routinely involve contouring of the peripancreatic lymph nodes , for the purpose of the present study we decided to create the peripancreatic ctvs , because of their importance in the lymphatic drainage of pdac . 
we first contoured the ctv_ pancreas that included the pancreas and the primary gtv to the sagittal plane through the left lateral aortic border ; this plane constitutes the resection margin of a typical whipple procedure . 
the ctv_ pancreas was expanded by 10 mm in the four corresponding directions ( anterior , posterior , superior , inferior ) to create each of the four peripancreatic nodal regions of interest ( rois )  . 
finally , the ctv_pancreas was subtracted from each of the four rois to create the peripancreatic nodal ctvs surrounding the pancreas : anterior ( ctv_antpanc ) , posterior ( ctv_postpanc ) , superior ( ctv_suppanc ) , and inferior ( ctv_infpanc )  . rtog contouring method the ptv ( ptv_rtog ) and the ctvs for the vascular areas were contoured as described recently [ 19 ]  . 
ctvs included the nodes for the aorta ( ctv_para_ rtog ) , the ct ( ctv_ct_rtog ) , the sma ( ctv_sma_rtog ) , and the pv ( ctv_pv_rtog )  . michigan contouring method the ctv consisted of the gtv plus 5 mm without including elns . 
 comparison of the percentage of ctv coverage between ptv_oxford or ptv_rtog and ptv_scalop showed a significant difference only for ctv_postpanc and ctv_infpanc . variability of aortic ctv and anatomical coverage of para - aortic lymph node areas the aorta and the para - aortic ctvs were contoured as shown in .fig.3a. 
 as expected , comparing the percentage of ctv coverage between ptv_ oxford or between ptv_rtog with ptv_michigan and ptv_scalop resulted in a significant difference , for both ctv_para_ox and for ctv_para_rtog . variability of celiac trunk and superior mesenteric artery ctvs and their anatomical coverage the ct , the sma , and their corresponding ctvs were delineated as shown in .fig.5a ( only the ctvs for rtog are shown here )  . 
planning target volumes ( ptvs ) were contoured using planning computed tomography ( ct ) scans of 11 patients with pdac based on the oxford , rtog ( radiation therapy oncology group ) , michigan , and scalop ( selective chemoradiation in advanced localised pancreatic cancer trial ) guidelines . 
potential practical consequences are discussed in detail . keywords pancreatic cancer planning target volume lymph nodes primary tumor guidelines vergleich von vier zielvolumendefinitionen fr das pankreaskarzinobehandlungsrichtlinien fr lymphknotenareale und primrtumor zusammenfassung hintergrund . 
whrend einige gruppen darauf abzielen , nur den primrtumor zu bestrahlen , schlieen andere elektive lymphknotenareale ( elk ) mit edie elks in unmittelbarer nachbarschaft zum primrtumor sind abhngig von der jeweiligen behandlungsphilosophie oft unbeabsichtigter weise im zielvolumen . 
es wurden planungszielvolumina ( ptvs ) auf der grundlage der planungs - cts von 11 patienten mit pankreaskarzinomen nach den oxford - , rtog ( radiation therapy oncology group ) , scalop ( selective chemoradiation in advanced localised pancreatic cancer trial - ) und michi gan - definitionen konturiert . 
a axial images demonstrating the pancreas , the gtv , the peripancreatic node ctvs anterior ( ctv_antpanc ) , posterior ( ctv_postpanc ) , superior ( ctv_suppanc ) , and inferior ( ctv_infpanc ) and the four ptvs , ptv_oxford , ptv_rtog , ptv_scalop , and ptv_michigan . 
a axial images demonstrating the aorta , the ctv for para - aortic lymphatics contoured based on the oxford ( ctv_para_ox ) and rtog ( ctv_para_rtog ) methods , the inferior vena cava ( ivc ) and its nodes based on the oxford ( ctv_ivc_ox ) protocol and the four ptvs : ptv_oxford , ptv_rtog , ptv_scalop , and ptv_michigan . 
a axial images demonstrating the ctv for lymphatics of the ct and sma , based on the rtog method ( ctv_ct_rtog and ctv_sma_ rtog , respectively ) , and the four ptvs : ptv_oxford , ptv_rtog , ptv_scalop , and ptv_michigan . 
comparison of the percentage of ctv coverage by the ptvs for the ct ( d , e ) and sma ( f , g ) areas contoured according to the oxford and rtog methods . 
a axial images demonstrating the pv , the ctv for pv lymphatics contoured according to the oxford ( ctv_pv_ox ) and rtog ( ctv_pv_rtog ) methods and the four ptvs : ptv_ oxford , ptv_rtog , ptv_scalop , and ptv_michigan . 
 comparison of the percentage of ctv coverage between ptv_oxford or ptv_rtog and ptv_ michi gan revealed a significant difference for the ctvs of both the oxford and rtog methods . variability of portal vein ctvs and their anatomical coverage we contoured the pv and the corresponding ctvs as shown in .fig.5a ( only the ctvs for rtog are shown here )  . 
6 8 based on our treatment protocol ( oxford ) , patients with pancreatic cancer will receive a total dose of 50.4 gy in 28 fractions ( 1.8 gy / fraction ) according to planning target volume oxford ( ptv_oxford ; shown below ) , followed by an additional dose of 9.0 gy in 5 fractions according to planning target volume 2 ( ptv2 ; boost dose )  . 
if the planning computer tomography scan is taken in full exhale breath - hold , then ptv2 = gtv + 20 mm caudal , 10 mm cranial , and 15 mm in all other directions . 
 comparison of the percentage of pv ctvs coverage between ptv_oxford or ptv_rtog and ptv_michigan as well as ptv_scalop revealed a statistically significant difference . discussion the inclusion of elns in the radiotherapy of pdac remains debatable . 
this difference can have implications , since the tolerance of gemcitabine - based chemoradiotherapy is related to the size of the ptv [ 24 ] and hence radiation dose escalation will always have to exclude the elns [ 11 ]  . 
on the other hand , the presence of metastatic lymph nodes was shown to be associated with local recurrence ( hr 1.89 ) [ 6 ] , although detailed studies are lacking . we previously analyzed the patterns of regional lymphatic spread in pdac [ 16 ] and showed that the posterior pancreaticoduodenal nodes were at the highest risk for metastasis ( 37% ) , followed by the suprapancreatic head nodes ( 25% ) , the infrapancreatic head nodes ( 24% ) , the anterior pancreaticoduodenal nodes ( 23% ) , nodes in the hepatoduodenal ligament ( 18% ) , and the superior mesenteric nodes ( 10% ) ; all the other nodal areas had less 412 | strahlentherapieundonkologie52013 fig . 
we outline the aorta from the celiac trunk ( include the celiac trunk anteriorly to its bifurcation ) to the inferior mesenteric artery ( for tumors of the lateral two thirds of the pancreatic tail , the inferior border is the lower border of the lower renal vein )  . 
then we add a margin of + 15 mm in all directions except inferiorly ( only 10 mm cranial if planning computer tomography scan taken in full exhale breath - hold )  . 
following this , we outline the inferior vena cava from the level of the inferior mesenteric artery ( for tumors of the lateral two thirds of the pancreatic tail , the inferior border is the lower border of the lower renal vein ) to the level of the celiac trunk . 
then we add a margin + 15 mm in all directions except inferiorly and posteriorly ( only 10 mm cranial if planning computer tomography scan taken in full exhale breath - hold )  . 
we subsequently edit this volume such that the right margin is 15 mm laterally to the right from the right edge of the anterior half of the ivc and 15 mm laterally to the right from the left edge of the posterior half of the ivc , aiming to exclude liver parenchyma . 
in the literature on radical lymph node dissection , a frequency of 1518% and a much higher rate of micrometastasis is reported [ 16 ]  . a comparison of the relative coverage of specific nodal areas according to the delineation criteria yields intriguing data . 
the posterior peripancreatic nodal region has a specifically important role as it presents the highest metastatic rate , it is intricately connected to the para - aortic region , and it is the typical site where microscopic disease ( r1 ) is encountered after pancreaticoduodenectomy [ 22 ]  . 
interestingly , both the scalop and the michigan ptvs covered this region by about 60 and 50% , respectively , whereas anatomical coverage by the oxford and rtog ptvs was approximately 95% . 
however , especially the superior and the inferior pancreaticoduodenal nodes as well as the right lateral nodes are difficult to cover with a high radiation dose because they are close to the duodenum . the largest discrepancies in volume were found for the para - aortic and the interaortocaval nodes . 
however , a very rich lymphatic network connects them directly to the posterior pancreatic region , which is reflected in the high rate of para - aortic micrometastases [ 25 ] , and hence the rtog definition appears to be justified . regarding the pv area , the ptv_ rtog extends more into the hepatic hilum despite there being no significant difference in the total volumes with the ptv_ oxford . 
notably , treatment of this area adhering to strict expansion rules would lead to the entire circumference of the duodenum next to the hepatoduodenal ligament being included into the ptv . 
we advocate trimming this region or treating it with imrt and a locally lower dose . finally , the superior mesenteric region was included to a significant degree in the scalop ptvs ; however , as the superistrahlentherapieundonkologie52013 | original article fig . 
8 8 as a third step , we contour the clinical target volumes for the lymph nodes of the portal vein ( pv ) , celiac trunk ( ct ) , and superior mesenteric artery ( sma ) , as described in patients and methods . 
the oxford ctv for pv ( ctv_pv_ox ) is contoured similarly to the rtog method except that on the right lateral side ctv_pv_ox is delineated only to the level of the junction of the cystic duct with the common bile duct ( described in [ 16 ] )  . 
however , their report confirmed the relatively low rate of metastasis in the ct region , which was included in the oxford definition , mainly because of the proximity to the tumor ptv and the ctv of the hepatoduodenal ligament . practical conclusions can be drawn and a more relaxed position between the proand contra - eln irradiation groups could be achieved by differentiating between nodal areas of high risk andlow risk : the posterior peripancreatic region should always be included , especially in patients with borderline - resectable disease . 
owing to the intricate connections with the para - aortic region and the relative ease of including this region without major consequences on the organs at risk , it is practical to include it between the superior and inferior border of the ptv of the primary tumor . 
on the other hand , inclusion of the nodes of the hepatoduodenal ligament often comes at the price of treatment of the entire circumference of the duodenum and therefore this option should be examined more critically . 
under no circumstances should inclusion of this area compromise application of a high dose to the area of the tumor , especially because of the close contact with the duodenumoreover , the para - aortic regions beyond the level of the tumor ptv are of a lower order of importance in the ranking of elns . based on our experience , we currently advocate radiotherapy according to the oxford contouring guidelines , since it is a feasible method that enables administration of a high dose ( 59.4 gy ) to the primary tumor region and it is associated with good tolerance . 
9 8 as a fourth and final step , we create the ptv_oxford by merging the following structures : ptv2 ( boost region ) , elective nodal regions ( depending on the site of the tumor in the pancreas , as described in [ 16 ] ) and any enlarged lymph nodes . 
depending on the localization of the primary tumor position , we edit the ptv_oxford to enable some sparing of the right lateral wall of the duodenum ( in conjunction with image guidance , such as 4d - computed tomography )  . 
finally , we ensure that the ptv_oxford encompasses ( with a circumferential 1 - cm margin ) the superior mesenteric vein for 3 cm inferior to the confluence of the splenic vein with the superior mesenteric vein our study had some limitations . 
the authors prescribed an external beam radiation dose of 25 gy ( 250 cgy / day , 5 days / week ) by linear accelerator with 3d conformal radiation , encompassing radiographically visible lesions . at 1 - year follow - up , the patient was free of chest pain and his disease was stable . 
he recovered well from brain surgery and was free of symptoms in the sternum area . case study strahlenther onkol 2013 189 : 508509 doi 10.1007 / s00066 - 013 - 0322 - 5 received : 9 november 2012 accepted : 23 january 2013 published online : 20 . 
april 2013 springer - verlag berlin heidelberg 2013 introduction hydatid disease is a zoonotic infectious disease seen mostly in the liver , but which can develop anywhere in the body , such as the mediastinum , pleura , diaphragm , and central nervous system [ 1 ]  . 
rarely , hydatid bone cysts cannot be controlled despite repeated surgery , a situation in which radiation therapy represents a good alternative treatment procedure for refractory osseous hydatidosis . against this background , we report a new case of hydatid disease of the chest that has been treated with radiation therapy after multiple surgical procedures and medical treatment had failed . case report a 62 - year - old man was admitted to the authors center in october 2009 complaining of pain and tenderness in the chest wall accompanied by a history of recurrent chest disease since 2004 . 
1 7 a cystic and lytic lesion destroying and extending the sternum treatment modality ; however , according to the literature , we conclude that rt is not well known in this setting . 
april 2013 springer - verlag berlin heidelberg 2013 d.rades1t.veninga2a.bajrovic3j.h.karstens4s.e.schild5 1 department of radiation oncology , university of lubeck 2 department of radiation oncology , bernard verbeeten institute , tilburg 3 department of radiation oncology , university medical center hamburg - eppendorf 4 department of radiation oncology , hannover medical university , hannover 5 department of radiation oncology , mayo clinic scottsdale , arizona avalidatedscoringsystemto identifylong - termsurvivors afterradiotherapyformetastatic spinalcordcompression it has been reported that selected longterm mscc survivorssuch as patients with oligometastatic diseasecan experience favorable results with conventional rt alone . 
 the present study aimed to develop a scoring system to identify long - term survivors after conventional rt alone with high specificity and a high positive predictive value . patients and methods it has been reported that long - course rt results in better survival than short - course in mscc patients . 
this scoring system was thus developed in mscc patients who had received long - course rt alone , in order to avoid a potential selection bias [ 12 ]  . 
1 8 patients receiving long - course rt ( test group ) : proportion of long - term survivors ( % ) in terms of total score ( 018 points ) the majority of patients with metastatic spinal cord compression ( mscc ) only live for a few months [ 2 , 11 ]  . 
it is not clear whether such long - term survivors are sufficiently treated with radiotherapy ( rt ) alone , or whether they would benefit from more aggressive treatments such as decompressive surgery or high - precision rt ( image - guided intensity - modulated radiotherapy , ig - imrt ; fractionated stereotactic body radiotherapy , sbrt and single - fraction radiosurgery )  . 
recently published evidence - based guidelines were quite reserved regarding these specialized rt techniques for mscc , since the rationale for such methods is based primarily on single - institution retrospective analyses [ 6 ]  . 
furthermore , such treatments can be very time consuming . a randomized study begun in 2003 demonstrated a benefit of upfront decompressive surgery in addition to rt for highly selected patients . 
surgery - related complications such as wound infections , extensive bleeding , postoperative pneumonia and pulmonary embolism occur in 1113% of patients [ 9 , 13 , 14 ]  . 462 | strahlentherapieundonkologie62013 10 11 12 13 14 15 16 17 18 points fig . 
2 8 patients receiving short - course rt ( validation group ) : proportion of long - term survivors ( % ) in terms of total score ( 018 points ) tab . 
ecog - ps and ambulatory status were confounding variables , since non - ambulatory patients generally had an ecog - ps of 34 and ambulatory patients an ecog - ps of 12 . 
the series from each contributing center represented an unselected cohort of patients treated over a defined period of time . rt was generally performed with linear accelerators and delivered through a single posterior field or parallel - opposed fields , depending on the depth of the spinal cord . 
patients received 1232 mg of dexamethasone per day from the time of mscc diagnosis until completion of the rt course . patients surviving longer than 1 year following rt ( long - term survivors ) and patients who died within 1 year were compared with respect to their pretreatment characteristics using a 2 test . 
the proportion of long - term survivors was 10% for scores of 09 points , 1860% for scores of 1014 points and > 90% for scores of 15 18 points . 
this was not central for this study since it aimed to identify long - term survivors with high specificity and positive predictive value . strahlentherapieundonkologie62013 | original article abstract zusammenfassung in order to validate the scoring system , the proportions of long - term survivors in the test group of 1 , 125 long - term survivors was compared to a cohort of 773 patients who had received short - course rt comprising 1 fraction of 8 gy on 1 day or 5 fractions of 4 gy in 1 week ( validation group , .fig.2 ) , for each score of 018 . 
since all patients treated in germany had received long - course rt and all patients treated in the netherlands short - course rt , a selection bias associated with the radiation regimen appeared unlikely . 
the proportions of long - term survivors in the validation group were very similar to those of the test group , thus demonstrating the high validity and reproducibility of this scoring systeat a cutoff value of 15 points , the specificity and the positive predictive values in the validation group were 98 and 91% , respectively . discussion conventional rt alone is the most common treatment for mscc worldwide . 
although most of these patients have a limited survival expectancy , a considerable number of them live for longer than 1 year following treatment and may therefore be regarded as long - term survivors [ 2 , 11 , 12 ]  . 
 for patients with oligometastatic disease and a favorable survival prognosis , it has been reported that good resultsin terms of functional outcome , post - rt ambulatory status and local control of mscccan be achieved using conventional rt alone [ 15 ]  . 
furthermore , single - fraction ig - imrt and radiosurgery led to treatment - associated vertebral 464 | strahlentherapieundonkologie62013 strahlenther onkol 2013 189 : 462466 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0342 - 1 d.radest.veningaa.bajrovicj.h.karstenss.e.schild a validated scoring system to identify long - term survivors after radiotherapy for metastatic spinal cord compression abstract purpose . 
the score proved to be valid and reproducible . keywords intensity - modulated radiotherapy stereotactic body radiotherapy survival prognosis radiosurgery ein validiertes scoring - system zur identifizierung von langzeitberlebenden nach strahlentherapie bei metastatisch bedingter rckenmarkskompression zusammenfassung hintergrund . 
der score erwies sich als valide und reproduzierbar . schlsselwrter intensittsmodulierte strahlentherapie stereotaktische krperbestrahlung berleben prognose radiochirurgie fractures in 039% of patients [ 1 , 3 , 4 , 5 , 7 , 8 , 16 , 17 , 18 , 19 ]  . 
however , no patients in the cohort of 567 long - term survivorswith a median follow up of 17 monthsdeveloped a treatment - related vertebral fracture or myelopathy . however , up until now it has been difficult to identify long - term survivors prior to conventional rt . 
our previous scoring system for estimating the survival of mscc patients was designed to predict the 6 - month survival probability but not to predict a long - term survival of more than 1 year following rt [ 10 ]  . 
this earlier scoring system was based on six prognostic factors : primary tumor type , interval between tumor diagnosis and mscc , other bone metastases , visceral metastases , ambulatory status and the time to developing motor deficits . 
in the validation study , patients were divided into three groups : 2030 points ( poor prognosis ) , 3135 points ( intermediate prognosis ) and 3645 points ( favorable prognosis )  . 
when aiming to identify long - term survivors among patients receiving longcourse rt , applying the previous scoring system to the present study population resulted in positive predictive and specificity values of 73 and 84% , respectively . 
tsai jt , lin jw , chiu wt , chu wc ( 2009 ) assessoriginal article in conclusion , this new scoring system enables identification of long - term survivors after rt for mscc . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 519520 doi 10.1007s00066 - 013 - 0369 - 3 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
20 , d - 65189 wiesbaden , e - mail : prott@bvdst.de personalia neues aus dem berufsverband herrn michael bamberg wurde auf dem estro forum in genf am 19.04.2013 der estro life time achievement award fr sein jahrzehntelanges herausragendes engagement fr die radioonkologie verliehen . 
 in seiner laudatio stellte der prsident der estro vincenzo valentini neben den herausragenden wissenschaftlichen leistungen das besondere engagement von michael bamberg in der grndungsphase der estro , fr die harmonisierung der weiterbildung in der radioonkologie in allen europischen lndern und bei der grndung der degro heraus . aktueller abrechnungs vorschlag imrt / igrt an den spitzenverband der pkv es laufen im moment gesprche des bvdst mit dem spitzenverband der pkv , daraus ergibt sich : der zustzliche aufwand der igrt - leistung mittels portal imaging oder cone beamct muss unabhngig von der anzahl der zu bestrahlenden zielvolumina gleich abgebildet werden . 
 die tomotherapie wird in ihrer vergtung der imrt und igrt am linearbeschleuniger angepasst , da sie vom planungsaufwand und durchfhrung vergleichbar ist es soll steigerungsmglichkeiten der analogziffer 5855 go geben in abhngigkeit von der felderanzahl und der bildgebung . 
eine entsprechende anhrung hierzu fand am 16.04.2013 statt , der text wurde grundlegend revidiert und durch die folgende formulierung ersetzt : in bedienrumen von beschleunigern ist fr die bemessung des strahlenschutzes der hchstwert fr die effektive dosis durch die zustndige behrde festzulegen . 
 dabei orientiert sich die behrde in der regel an den empfehlungen der richtlinie fr strahlenschutz in der mediz neue weiterbildungs ordnung am 23.01.13 fand ein einfhrungs - workshop der bundesrztekammer zur novellierung der musterweiterbildung statt . 
 von seiten des berufsverbandes wurde darauf hingewiesen , dass es nicht sein kann , dass der sogenannte klinische abschnitt von jungen strahlentherapeutinnen und - therapeuten nur noch auf einer strahlentherapeutischen station absolviert werden kann , weil es viel zu wenig einrichtungen dieser art gibt , als dass dadurch eine ausreichende anzahl an strahlentherapeuten ausgebildet werden kann . 
dies ist nach auffassung des bvdst nicht rechtens , denn die anwendung der analogziffer ist nicht auf bsartige tumore beschrnkt , sondern kann auch 520 | strahlentherapie und onkologie 6 2013 original article strahlenther onkol 2013 189 : 448455 doi 10.1007 / s00066 - 013 - 0345 - y received : 26 september 2012 accepted : 6 march 2013 published online : 21 . 
where this is not feasible , other endpointsincluding progression - free survival ( pfs ) , symptom - free survival or even interval free of systemic therapiesare employed [ 2 , 3 , 5 , 6 , 8 , 10 , 13 , 19 , 24 , 26 ]  . 
 however , the duration of such treatments and the significant side effects and frequent reduction in quality of life [ 16 , 27 ] with which they are associated , speak for local therapies . 
following experiences with linear accelerator ( linac ) - based srt to treat oligometastatic patients , a prospective evaluation of the outcomes observed with cbk - str began within the framework of a multicentric collaboration in 2007 [ 14 , 23 ]  . 
results were assessed in terms of toxicity , infield control and overall survival ( os )  . material and methods study protocol this is a prospective study of cbk - srt in oligometastatic cancer patients . 
the ethics committee of our institution was informed of the project . inclusioncriteria inclusion criteria were as follows : adult patients with limited volume cancer ( 1 5 lesions ) , candidates for srt but not for other local therapies ( surgery , cryotherapy , high - intensity focused ultrasound hifu ) and written informed consent . 
total - body staging using total - body computed tomography ( ct ) or 18f - fluorodeoxyglucose positron - emission tomography / ct scan ( 18f - fdg - pet / ct ) was required . 
disease location was divided according to the following categories : primary tumor ( t ) , regional lymph node ( ln ) or distant metastasis ( m )  . when admitting patients to the study , any kind of previous cancer therapy was permissible . 
 however , since the primary endpoints included treatment toxicity ( see below ) , patients in whom not all lesions could be treated with cbk - srt were also included in the analysis . 448 | strahlentherapieundonkologie62013 whole lung ( right + left excluding gtv ) statistical analysis tab . 
a 2 mm margin was added to the gross tumor volume ( gtv ) in order to create the planning target volume ( ptv ) and compensate for the submillimeter detection inaccuracy of the fiducial marker . 
in patients with no fiducial marker , image - based bony anatomy registration supported by the xsight spinetm software module ( accuray , usa ) was applied . the cbk - srt standard dose varied between 24 and 30 gy administered in 3 fractions . 
dose prescription could be personalized : a higher dose per fraction in the case of a single tumor location or a lower dose in instances of re - irradiation or proximity to critically radiosensitive structures such as intestinal loops . 
in the case of re - irradiation , lowering of the constraints was based upon the previous rt plan data . during beam delivery , x - ray images were acquired for every 3 cbk positions ( nodes ) in order to monitor the position of the target ( equivalent to an interval of about 40 s ) [ 28 ]  . 
daily treatment times were kept below 4560 min in order to minimize patient inconvenience and the discomfort of prolonged immobilization , as well as to minimize the risk of intrafraction radiation repair occurring during excessively long individual sessions [ 1 , 9 ]  . patientmonitoring the patients were seen by the radiation oncologist at each cbk - srt session . 
the criteria of the radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc ) were used to evaluate treatment toxicity [ 4 ]  . 
acute toxicity was analyzed in all patients ( toxicity occurring during rt and within the following 3 months ) ; late toxicity was evaluated in the patients with a follow - up longer than 3 months . 
out of 87 evaluable lesions , complete radiological response , partial response , stabilization and progressive disease were observed in 15 ( 17% ) , 25 ( 29% ) , 34 ( 39% ) and 13 ( 15% ) lesions , respectively . 
further investigations should focus on dose escalation and optimization of the combination with systemic therapies . keywords toxicity survival positron - emission tomography computed tomography metastasis robotische bildgefhrte stereotaktische bestrahlung mit dem cyberknife fr oligometastatischen krebs . 
unter 87 auswertbaren lsionen wurde ein komplettes radiologisches ansprechen , ein teilweises ansprechen , eine stabilisierung und ein fortschreiten der erkrankung in jeweils 15 ( 17% ) , 25 ( 29% ) , 34 ( 39% ) und 13 lsionen ( 15% ) beobachtet . 
das 3 - jhrige , lokale progressionsfreie berleben ( lc , lokale kontrolle ) , das progressionsfreie berleben ( pfs ) und das allgemeine berleben ( os ) lagen jeweils bei 67 , 6% , 18 , 4% und 31 , 2% . 
weitere untersuchungen zur dosissteigerung und optimierung der kombination mit systemischer therapie sollten durchgefhrt werden . schlsselwrter toxizitt berleben positronenemissionstomographie computertomographie metastasierung treated site during the follow - up period ( non - complete responders ) , symptoms appearing during follow - up were evaluated case - by - case , in order to classify their etiology ( regarding the presence of tumor or late normal tissue injury )  . the radiological response was classified according to the criteria reported in response evaluation criteria in solid tumors recist , v . 
pfs was defined as the time interval between the first day of cbk - srt and diagnosis of progressive disease ( infield or out - field ) or the last follow - up visit at which there was no sign of progression . 
 complete radiological response , partial response , stabilisation and progressive disease were observed in 15 ( 17% ) , 25 ( 29% ) , 34 ( 39% ) and 13 ( 15% ) lesions , respectively . 
according to this interpolation , every elapsed month between primary diagnosis and cbk - srt increased lc by about 1% . discussion our study included 95 patients ( 118 lesions ) treated over an 18 - month period . 
side effects were generally mild , with the majority of patients not experiencing any toxicity . srt has become an established therapy for the management of oligometastic 452 | strahlentherapieundonkologie62013 cancer patients [ 29 ] and cbk represents an excellent image - guided robotic stereotactic technology [ 11 , 21 ]  . 
to our knowledge , there has not been any other substantial report on cbk - srt in the management of limited volume advanced and / or oligometastatic cancer of organs other than the spine or brain ( apart from our preliminary investigations [ 14 , 23 ] )  . 
the results of our cbk - srt series compare very well to the findings reported with other srt modalities [ 17 , 20 ]  . we are aware that our series has several limitations , including patient heterogeneity , short follow - up times and response evaluation in only about 75% of lesions ( with potential over - evaluation of response rate due to the exclusion of patients with a worse prognosis )  . 
three different cancer lesions were analysed ( t , ln , m ) , as well as different patient categories in terms of primary site , treatment site , treatment intent , extent of disease , previous rt and concomitant therapy . 
such results are of extreme importance in chronic diseases such as metastatic cancer , because they demonstrate that a high - efficacy local therapy might represent a valid alternative strategy when seeking to reduce the burden of the systemic therapies . 
in our series , no strict rules were adopted relating to the concomitant systemic therapy ( the majority of our patients had already started systemic therapy for recurrent disease before being referred to our department )  . 
if one considers that 40% of patients received cbk - srt as re - irradiation , lc rates must be viewed as being extremely high . the geometric precision of cbk - srt allows for excellent sparing of surrounding normal tissue . 
in our series , the vast majority of patients suffered no side effects and in all cases the treatment was delivered on an out - patient basis over a short time period ( median 3 fractions )  . 
 [ 12 ] , observed less acute toxicities and a reduced requirement for further intervention in patients treated for spine metastases with cbksrt compared to the patients that underwent external beam rt . 
the potential of cbk to perform motion - correlated treatment of moving lesions through internal external motion correlation [ 18 , 22 ] further increases the clinical interest in this technology for the local management of extra - cranial diseases . in conclusion , cbk - srt is feasible approach for isolated recurrent primary , lymph node or metastatic cancer , offering low toxicity and durable in - field tumor control in a good proportion of patients . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literatur kommentiert strahlenther onkol 2013 189 : 510511 doi 10.1007 / s00066 - 013 - 0351 - 0 online publiziert : 25 . 
april 2013 springer - verlag berlin heidelberg 2013 w.drr medizinische universitt / akh wien bauchspeicheldrsealsrisikoorgan frdieinduktioneinesdiabetes mellitusbeikindernnach abdominalbestrahlung originalbeitrag de vathaire f , el - fayech c , ben ayed ff et al ( 2012 ) radiation dose to the pancreas and risk of diabetes mellitus in childhood cancer survivors : a retrospective cohort study . 
bei 65 patienten lag ein rztlich besttigter diabetes vor ; dies betraf 5 / 888 patienten ( 1% ) ohne und 60 / 1632 patienten ( 4% ) nach bestrahlung . 
 das diabetesrisiko nahm mit der dosis am pankreasschwanz , in dem sich langerhans - inseln bevorzugt befinden , bis zu einer dosis von 2029 gy steil zu ; fr hhere dosen ergab sich ein plateau . 
rr > 1 : das risiko der ( exponierten ) untersuchungsgruppe ist grer als das risiko der kontrollgruppe ( exposition = risikofaktor )  . als ltere patienten ( p < 0 , 02 ) mit einem rr bei 1 gy von 2 , 1 ( 1 , 44 , 3 ) vs . 
drr w , durante m , van den heuvel f et al ( 2010 ) the allegro project : what is the relevance of second tumours , and which information is required ? radiother oncol 96 ( suppl 1 ) : 183 5 . 
lancet oncol 13 : 961962 in der arbeit bleiben jedoch die patientenzahlen in den einzelnen gruppen , wie auch die zeitrume der jeweiligen rekrutierung unklar . schwchen der untersuchung , die auch in einem begleitenden kommentar betont werden [ 6 ] , sind das fehlen prospektiv durchgefhrter laboruntersuchungen zur charakterisierung und quantifizierung der funktion der - zellen im pankreas und der insulinresistenz , wie auch ein mangel an information bezglich der viszeralen oder subkutanen fetteinlagerung . 
diese mngel ergeben sich zwangslufig aus dem retrospektiven design der analyse . von 1538 der bestrahlten patienten lagen ausreichende angaben zur bestrahlung fr eine individuelle dosisrekonstruktion vor ; bei den restlichen 94 patienten ( 6% ) erfolgte diese fr eine typische behandlung , ohne dass das verfahren nher erlutert wird . 
verwendet wurde das fr derartige fragen entwickelte programm dos_eg , welches entsprechend den angaben der autoren eine genauigkeit der dosisabschtzung von 2% innerhalb und von 10% auerhalb des nutzstrahls erlaubt . 
unklar bleibt ebenso , ob und in welcher form der gesamtzeitraum der strahlenexposition im falle mehrerer bestrahlungsserien ( > 1 bei 26% der patienten , spanne 27 serien ) bei der dosisabschtzung bzw . 
 die ergebnisse einer derartigen auswertung wrden eine przisere festlegung von expositionsgrenzen fr die bestrahlungsplanung untersttzen . zusammenfassend ist festzustellen , dass die autoren eine detaillierte auswertung des umfangreichen datenmaterials durchgefhrt haben . 
 die oben dargestellten mngel in der beschreibung der methodik lassen jedoch weitergehende , quantitative schlussfolgerungen bezglich der strahlentoleranz dieses risikoorgans nicht zu , obwohl davon auszugehen ist , dass die daten derartige weitergehende abschtzungen erlauben wrden . fazit entsprechendderschlussfolgerungder autorensolltenacheinerabdominalbestrahlungvonkindernundjugendlichen dienachbeobachtungbersehrlange zeitrume , bevorzugtsogarlebenslang , erfolgenundeinediabetesdiagnostik einschlieen . wolfgang drr , wien korrespondenzadresse w . 
de vathaire f , el - fayech c , ben ayed ff et al ( 2012 ) radiation dose to the pancreas and risk of diabetes mellitus in childhood cancer survivors : a retrospective cohort study . 
diallo i , haddy n , adjadj e et al ( 2009 ) frequency distribution of second solid cancer locations in relation to the irradiated volume among 115 patients treated for childhood cancer . 
int j radiat oncol biol phys 74 : 876883 strahlentherapieundonkologie62013 | original article strahlenther onkol 2013 189 : 482485 doi 10.1007 / s00066 - 013 - 0312 - 7 received : 8 october 2012 accepted : 16 january 2013 published online : 21 . 
yet , according to a recent analy sis , the benefit from sequential adjuvant chemotherapy is in the range of 10% for overall survival and seems to be limited to grade 3 tumors [ 14 ]  . integration of chemotherapy into preoperative radiotherapy has been explored in the last two decades starting with the use of iododeoxyuridine [ 11 ]  . 
different agents have been applied since then including doxorubicin [ 1 ] , ifosfamide [ 3 ] and cisplatin [ 4 ] or combined regimens [ 6 , 22 ]  . 
at our institution we established an ifosfamide - based , concurrent radiochemotherapy which has been described in the treatment of unresectable lesions [ 7 ]  . another interesting approach is the integration of locoregional hyperthermia [ 2 ] into preoperative treatment of soft tissue sarcoma . 
 recently , a large randomized phase 3 trial demonstrated a survival benefit for hyperthermia combined with sequential chemotherapy in localized high - risk soft tissue sarcoma [ 13 ]  . 
trimodal therapy has been described for pancreatic cancer [ 17 ]  . in this study , we compare the outcome of patients treated with preoperative radiotherapy for soft tissue sarcoma either alone or in combination with concurrent chemotherapy and / or locoregional hyperthermia . patients and methods all patients treated in the center for soft tissue sarcoma , gist and bone tumors of the comprehensive cancer center tbingen between 1999 and 2011 were evaluated retrospectively . 
patients with neoadjuvant radiotherapy and resection for intermediate or high grade tumors were included , whereas patients presenting with metastases , secondary cancers , low grade tumors or treated in prospective trials were excluded from the analysis . 
 with the approval of the ethics committee of our institution ( reference number 621 / 2011a ) we retrospectively reviewed patient records for clinical characteristics , treatment modalities , and survival data . median age of the 28 evaluable patients was 58 years ( range 2281 years )  . 
patients and treatment characteristics stratified by radiation treatment are shown in .tab.1. 482 | strahlentherapieundonkologie62013 biopsyand histological confirmation staging radiotherapy + hyperthermia resection radiotherapy n = 16 radiotherapy + chemotherapy radiotherapy + chemotherapy + hyperthermia multimodal therapy fig . 
2 8 a local control , b distant metastases - free survival , c disease - free survival , and d disease - specific survival were compared for multimodal therapy ( continuous lines ) versus radiotherapy alone ( dashed lines )  . 
multimodal therapy led to a significant increase in disease - specific survival local control ( lc ) , disease - free survival ( dfs ) , distant metastases - free survival ( dmfs ) , disease - specific survival ( dss ) , and overall survival ( os ) were calculated from start of treatment using the kaplanmeier method [ 15 ]  . 
the statistical analysis was performed with the software package spss 19 ( spss inc . , chicago , il , usa )  . results all patients at 3 years , the estimated overall , disease - specific , and disease - free survival was 72 , 81 , and 43% , respectively . 
after a median follow - up of 36 months corresponding median overall , disease - specific and disease - free survival reached 45 months ( 95% confidence interval ( ci ) 3165 months ) , 48 months ( 95% ci 17 79 months ) , and 25 months ( 95% ci 11 39 months )  . 
the median was not reached for lc , for dmfs the median was 28 months ( 95% ci 057 months )  . according to the ajcc staging 7th edition [ 8 ] , most tumors ( n = 16 ) were stage iii , this being the highest risk category for localized disease and 8 patients presented in stage iib . 
stage iia tumors ( n = 4 ) were treated neoadjuvantly only , if located in sensitive areas such as the head and neck , hand or in proximity to critical structures ( e.g. , neurovascular bundles ) with limited resectability . treatment - related outcome risk factors in the two treatment groups were balanced without statistically significant differences . 
differences in use of sequential chemotherapy are due to the inclusion of younger patients with the same prognostic factors in a prospective protocol [ 12 ] not being included in cases presented here to avoid a duplication of results . the superiority of neoadjuvant concurrent radiochemotherapy over neoadjuvant irradiation alone has not yet been demonstrated in a randomized trial . 
our data support this principle in comparison to a control group of our institution . locoregional hyperthermia has been described for different tumor entities such as chest wall recurrence of breast cancer , locally advanced rectal cancer , and cervical cancer [ 18 , 19 ]  . 
locoregional hyperthermia also increased local control when combined with sequential chemotherapy , thus , resulting in a benefit for dfs and even os in the patients having completed protocol induction therapy in the randomized eortc 62961 / esho - rht 95 intergroup study [ 13 ]  . 
our data suggest that multimodal treatment with ifosfamide and / or locoregional hyperthermia in combination with neoadjuvant radiotherapy might improve outcome in high - risk soft tissue sarcomas . keywords soft tissue sarcoma radiotherapy chemotherapy hyperthermia neoadjuvant einfluss von simultaner chemotherapie und hyperthermie auf ergebnisse neoadjuvanter radiotherapie von hochrisiko - weichteilsarkomen zusammenfassung hintergrund . 
die daten dieser serie deuten auf einen mglichen berlebensvorteil durch ifosfamid und / oder lokoregionale hyperthermie hin . schlsselwrter weichteilsarkom strahlentherapie chemotherapie hyperthermie neoadjuvant motherapy and hyperthermia with neoadjuvant radiotherapy . although the influence on dmfs was not statistically significant , the improvement of dss may suggest effects of multimodal neoadjuvant treatment outside the radiation field , e.g. , triggering of anti - tumor immune response . 
the potential link between local effects of radiotherapy and the immune system was evaluated in a phase - 1 study combining neoadjuvant radiation therapy and dendritic cell injection showing an infiltration of t - cells into the tumor and an induction of antitumor immune response [ 9 ]  . 
antigen presentation and the facilitation of a robust immune response by radiotherapy [ 10 ] may serve as a possible explanation for a better control of distant tumor cells and lead to an improved dss . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literatur kommentiert strahlenther onkol 2013 189 : 512513 doi 10.1007 / s00066 - 013 - 0335 - 0 online publiziert : 24 . 
die bereits 2008 erstmals publizierte multizentrische intergroup - studie unter leitung der rtog hatte im vergleich zweier unterschiedlicher radiochemotherapiekonzepte nachteile fr eine kombination aus 5 - fluorouracil ( 5 - fu ) plus cisplatin im vergleich zu 5 - fu plus mitomycin ergeben . 
voraussetzung fr eine studienteilnahme waren ein karnofsky - index > 50% , ein stadium t24 ohne fernmetastasen und hmatologische blutwerte , kreatinin und sonstige organfunktion , welche eine chemotherapie erlaubten . 
der primre studienendpunkt war ein verbessertes krankheitsfreies berleben , wobei 63% nach 5 jahren mit 5 - fu / mitomycin versus 73% mit 5 - fu / cisplatin erwartet worden waren . 
die gesamtbehandlungszeit betrug median 49 tage im 5 - fu / mitomycin - arm , jedoch 101 tage im 5 - fu / cisplatin - arm , dem eine induktionschemotherapie vorgeschaltet war . 
anders als erwartet , war der 5 - fu / cisplatin - arm unterlegen : das krankheitsfreie berleben nach 5 jahren betrug nur 58% im vergleich zu 68% mit 5 - fu / mitomycin ( p = 0 , 026 ) ; fr diesen arm waren bei der studienplanung 63% vorausgesagt worden . 
die simultane radiochemotherapie mit 5 - fu / mitomycin bleibt der bevorzugte standard . kommentar die ausschlielich simultane radiochemotherapie mit 5 - fu / mitomycin erlaubt bei der mehrzahl der patienten einen langfristigen sphinktererhalt , da analkanalkarzinome fr gewhnlich vollstndig auf diese behandlung ansprechen [ 2 , 3 , 5 ]  . 
brooks cj , lee yk , aitken k et al ( 2012 ) organ - sparing intensity - modulated radiotherapy for anal cancer using the actii schedule : a comparison of conventional and intensity - modulated radiotherapy plans . 
fakhrian k , sauer t , klemm s et al ( 2013 ) radiotherapy with or without chemotherapy in the treat ment of anal cancer : 20 - year experience from a single institute . 
kachnic la , winter k , myerson rj et al ( 2012 ) rtog 0529 : a phase 2 evaluation of dose - painted intensity modulated radiation therapy in combination with 5 - fluorouracil and mitomycin - c for the reduction of acute morbidity in carcinoma of the anal canal . 
 in einer aktuellen franzsischen publikation war brigens auch kein vorteil durch induktionschemotherapie zu erkennen gewesen [ 5 ]  . in den meisten onkologischen situationen lsst der gegenwrtige behandlungsstandard mit seinen ergebnissen noch luft nach oben . 
zum einen betrug das krankheitsfreie 5 - jahres - berleben im berlegenen arm mit 5 - fu und mitomycin nur 68% und nicht 100% , ein zugegeben unrealistisches ziel , zum anderen war zumindest die akute toxizitt erheblich . 
ob analkanalkarzinome , die nur partiell ansprechen oder im verlauf rezidivieren , intrinsisch so resistent sind , dass selbst eine intensivere radiochemotherapie bei ihnen letztlich erfolglos bleibt , muss in studien untersucht werden . 
immerhin kann die frhzeitige chirurgische salvagetherapie noch einen teil der therapieversager retten . fazit diesimultaneradiochemotherapiemit 5 - fu / mitomycinbleibtbeiderorganundfunktionserhaltendentherapiedes analkanalkarzinomsderbevorzugte standard.bezglichdeskrankheitsfreien berlebens , desgesamtberlebensund beiderverminderungderbehandlungstoxizittgibtesallerdingsnochreichlich luftnachoben . carsten nieder , bod strahlentherapieundonkologie62013 | literaturkommentiert strahlenther onkol 2013 189 : 516518 doi 10.1007 / s00066 - 013 - 0337 - y online publiziert : 2 . 
mai 2013 springer - verlag berlin heidelberg 2013 e.wenkel radiologisches institut , universittsklinikum erlangen besseremamma - mrt - spezifittbei nichtmalignenbrustlsionendurch zustzlichediffusionsgewichtete sequenzbeikaumverlngerter untersuchungsdauer orginalbeitrag parsian s et al ( 2012 ) nonmalignant breast lesions : adcs of benign and high - risk subtypes assessed as false - positive at dynamic enhanced mr imaging . 
neuere studien bei frauen mit erhhtem mammakarzinomrisiko ergaben sensitivitten von 77100% im vergleich zur mammographie mit 1640% und spezifitten von 8199% im vergleich zur mammographie mit 9399% [ 1 ]  . 
in diese retrospektive studie wurden somit 175 nichtmaligne lsionen von 162 frauen eingeschlossen , die in der mrt nach dem breast imaging reporting and data system primr als suspekt oder hochsuspekt beurteilt worden waren [ 2 ]  . 
die mrts wurden an einem 1 , 5 - t - scanner ( lx , ge healthcare , waukesha , usa ) mit einer dedizierten 8 - kanal - brustspule in axialer schichtfhrung durchgefhrt . 
die hufigsten histologischen befunde entsprachen fibroadenomen ( n = 30 ) , adenosen ( n = 21 ) , fokalen fibrosen ( n = 19 ) und 28 hochrisikolsionen ( atypische duktale hyperplasie [ adh ] n = 23 , lobulre neoplasie n = 5 )  . 
der mittlere diffusionskoeffizient ( adc - wert ) aller nichtmalignen lsionen ( [ 1 , 770 , 45 ] 103 mm2 / s ) war signifikant niedriger als der des normalen drsengewebes ( [ 2 , 130 , 38 ] 103 mm2 / s )  . 
die 28 hochrisikolsionen hatten einen signifikant niedrigeren mittleren adcwert ( [ 1 , 480 , 39 ] 103 mm2 / s ) als die 147 gutartigen lsionen ( [ 1 , 830 , 43 ] 103 mm2 / s )  . 
im vergleich zu einer frheren studie der autoren ergab sich ein abnehmender trend der adc - werte von den benignen , zu den hochrisikound malignen lsionen ( mittlerer adc - wert [ 1 , 30 , 27 ] 103 mm2 / s ; [ 3 ] )  . 
in der vorluferstudie war ein adc - schwellenwert fr benigne und maligne lsionen von 1 , 81103 mm2 / s festgelegt worden , um eine sensitivitt von 100% zu erreichen . 
die auswertung der dw - sequenzen zusammen mit den standardsequenzen hat das potential , die falsch - positiven befunde der mammamrt zu senken , biopsien zu vermeiden und notwendige biopsien dann gezielter durchzufhren . 
 dabei wurden , entsprechend der aktuellen klinischen bedeutung , therapien mit radioaktiven somatostatinrezeptor - liganden und die sirt neu aufgenommen , whrend seltenere therapien nur noch im allgemeinen teil erwhnt werden . auch in anderen kapiteln wurden wichtige neue verfahren aufgenommen , so zum beispiel im kapitel zentralnervensystem die darstellung von amyloid - plaques zur alzheimer diagnostik . 
nur in dem abschnitt zur skelettszintigraphie , die unverndert ein wichtiges und hufig durchgefhrtes verfahren ist , htte die in der alten auflage grere zahl interessanter fallbeispiele und hilfestellungen zur indikationsstellung und befundinterpretation gerne auch beibehalten werden knnen . kurz zusammengefasst , ist den autoren die umfassende berarbeitung fr die 7 . 
 damit festigen sie die bedeutung dieses buches als das einstiegswerk in das gebiet der nuklearmedizin fr studierende der medizin , mtras und assistenzrzte verschiedener fachrichtungen . stephan roth ( dsseldorf ) buchbesprechungen haraldschicha , otmarschober nuklearmedizinbasiswissen undklinischeanwendung schattauer 2013 , 7 . 
auflage von 2007 fallen als erste nderung die jetzt farbig gestalteten abbildungen und farbig unterlegten merkstze ins auge , die die erfassung der wesentlichen inhalte vereinfachen . die wichtigeren vernderungen finden sich aber im inhalt : in vielen bereichen wurden schwerpunkte neu gesetzt und an die aktuellen anforderungen in der nuklearmedizin angepasst . 
 beibehalten wurde die bewhrte untergliederung in einen allgemeinen teil , der physikalische , gertetechnische und radiopharmazeutische grundlagen erlutert , und einen speziellen teil , der sich der klinischen anwendung nuklearmedizinischer methoden widmet . neu im allgemeinen teil ist z.b. 
dabei finden auch die neuen diagnostischen referenzwerte des bfs bercksichtigung . im speziellen teil wurden viele kapitel didaktisch sinnvoll umsortiert und im umfang ihrer aktuellen klinischen bedeutung angepasst . an umfang und inhalt besonders gewonnen hat das kapitel tumoren . 
hier finden sich aktuelle daten zum einsatz verschiedener petund spect - tracer in der tumordiagnostik , sowie aktuelle empfehlungen der strahlenschutzkommission von 2012 zur indikationsstellung fr den einsatz der pet . 
weiterhin wurden die radionuklid tumortherapien , die bisher 518 | strahlentherapieundonkologie62013 review article strahlenther onkol 2013 189 : 445447 doi 10.1007 / s00066 - 013 - 0331 - 4 received : 7 february 2013 accepted : 13 february 2013 published online : 21 . 
the following risk groups are defined : early favourable stages : f patients in stages ia or ib and iia or iib without risk factors . early unfavourable stages : f patients in stages ia or ib and iia with one or more risk factors . f patients in stage iib with elevated erythrocyte sedimentation rate ( esr ) and / or involvement of 3 lymph node areas . advanced stages : f patients in stage iib with risk factors , extranodal involvement and / or bulky mediastinal mass . f patients in stages iiia or iiib . f patients in stages iva or ivb . risk factors are defined as : elevated esr , extranodal involvement , involvement of 3 lymph node areas and bulky mediastinal mass . in general , all patients should be included into clinical trials unless there are exclusion criteria . 
rt alone should not be used to treat patients in early favourable stages as several studies have demonstrated the superiority of ctx followed by rt [ 1 , 2 , 3 ]  . 
the hd8 trial conducted by the german hodgkin study group ( ghsg ) tested whether if - rt is as effective as extended - field radiotherapy ( ef - rt )  . 
the final analysis showed no statistically significant difference between the two treatment modalities , thus if - rtwhich is less toxicis used as standard [ 6 ]  . the recommended rt dose is 20 gy . 
in the final analysis , no statistically significant differences between 20 gy and 30 gy were observed [ 4 ]  . strahlentherapieundonkologie62013 | review article legend ( pso ) f arbeitsgemeinschaft fr psychoonkologie f arbeitsgemeinschaft internistische onkologie ( aio ) f arbeitsgemeinschaft gynkologische onkologie ( ago ) f arbeitsgemeinschaft radiologische onkologie ( aro ) f deutsche gesellschaft fr endoskopie und bildgebende verfahren ( dge - bv ) f deutsche gesellschaft fr innere medizin f deutsche leukmie und lymphomhilfe f deutsche gesellschaft fr nuklearmedizin f deutsche gesellschaft fr pathologie f deutsche gesellschaft fr radioonkologie ( dgim ) ( dgn ) ( dgp ) ( degro ) f deutsche gesellschaft fr ultraschall in der medizin ( degum ) f deutsche krebsgesellschaft ( dkg ) f deutsche rntgengesellschaft ( drg ) f konferenz onkologischer krankenund kinderkrankenpflege ( kok ) f cochrane haematological malignancies group ( chmg ) f deutsche gesellschaft fr medizinische informatik , biometrie und epidemiologie ( gmds ) f deutsche hodgkin studiengruppe ( ghsg ) f deutsches netzwerk evidenzbasierte medizin ( dnebm ) f kompetenznetz maligne lymphome f deutsche gesellschaft fr hmatoonkolo ( kml ) gie ( dgho ) the role of fluorodeoxyglucose positron - emission tomography ( fdg - pet ) in the treatment strategy for patients in early unfavourable stages is being tested in the ongoing ghsg hd16 trial . 
although the high negative predictive value of a negative pet scan is well known [ 7 , 8 , 9 , 10 , 11 ] , pet should not be used as a tool to stratify treatment outside clinical trials . early unfavourable stages patients in early unfavourable stages are treated with a combined - modality approach . 
standard ctx according to the final results of the ghsg hd11 and hd14 trials consists of two cycles of escalateddose bleomycin , etoposide , adriamycin , 446 | strahlentherapieundonkologie62013 cyclophosphamide , vincristine , procarbazine and prednisone ( beacopp ) , followed by two cycles abvd [ 12 , 13 ]  . 
if escalated - dose beacopp cannot be applied due to medical reasons , four cycles of abvd should be given instead . based on the results of the ghsg hd8 trial mentioned above , the standard rt volume is defined as the involved field [ 6 ]  . the standard rt dose is 30 gy , as demonstrated in the final analysis of the ghsg hd11 trial [ 13 ]  . 
the combination of four cycles abvd followed by only 20 gy resulted in inferior progression - free survival compared to the other treatment arms [ 13 ]  . the role of fdg - pet in risk stratification is not well established . 
despite being a well - known independent marker , fdg - pet has not been used outside of clinical studies [ 14 , 15 , 16 , 17 ]  . 
the ongoing ghsg hd17 trial implements fdg - pet and a new rt volumethe involved - node radiotherapy ( in - rt ) conceptinto the treatment stratification [ 18 ]  . 
since the risk of late adverse effects of rt is related to radiation dose and the size of the irradiated volume , the goal is to reduce doses and field sizes as much as possible without reducing the probability of cure . 
other study groups are also testing its value , such as the european organisation for research and treatment on cancer ( eortc ) in their h10 trial [ 19 , 20 ]  . advanced stages standard ctx for patients under 60 years of age in advanced stages of disease consists of six cycles escalated - dose beacopp , based on the final results of the ghsg hd15 trial [ 21 ]  . the role of rt after effective ctx is the topic of controversial discussion . 
up - to - date literature citations provide an overview of current recommendations . keywords radiotherapy chemotherapy positron - emission tomography fluorodeoxyglucose risk factors die deutsche s3 - leitlinie fr das hodgkin - lympho aspekte fr radioonkologen zusammenfassung die vorliegende analyse stellt wichtige strahlentherapeutische aspekte der s3 - leitlinie fr das hodgkin - lymphom zusammen . 
die auflistung der aktuellen literatur gibt einen berblick ber derzeitige empfehlungen . schlsselwrter strahlentherapie chemotherapie positronenemissionstomographie fluorodeoxyglukose risikofaktoren now obsolete techniques that were described [ 24 ]  . treatment volumes for patients in advanced stages are inherent . 
in germany , local rt with 30 gy to initial bulky disease or extranodal lesions is the standard care outside of clinical trials . the ghsg hd12 trial tested whether consolidation rt is needed after ctx . 
 the final analysis shows that patients with residual disease who received consolidative rt had improved progression - free survival rates [ 25 ]  . the hd15 trial used pet for risk stratification in the treatment of patients in advanced stages . 
the negative predictive value of pet was defined as 94% [ 21 , 26 ]  . the ongoing hd18 trial implements an early pet examination after two cycles of ctx into the treatment stratification . 
patients with an fdg - pet - positive result after four to six cycles receive additional local rt with 30 gy , according to the results of the hd15 trial . 
these results still have to be awaited . lymphocyte - predominant hodgkins lymphoma the lymphocyte - predominant hodgkins lymphoma accounts for 5% of all hl and is distinguished from classical hl by its clinical course . 
 this treatment is based on retrospective studies conducted by the ghsg and the eortc , where the if - rt was equal to more extended rt volumes [ 27 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 514515 doi 10.1007 / s00066 - 013 - 0352 - z online publiziert : 24 . 
april 2013 springer - verlag berlin heidelberg 2013 s.hellerm.krause klinik und poliklinik fr strahlentherapie und radioonkologie , universittsklinikum carl gustav carus an der technischen universitt dresden niedermolekularesheparin senktthromboserisiko beichemotherapeutisch behandeltentumorpatienten originalbeitrag agnelli g , george dj , kakkar ak et al ( 2012 ) semuloparin for thromboprophylaxis in patients receiving chemotherapy for cancer . 
in dieser doppeltblinden , multizentrischen studie [ 2 ] wurde die wirksamkeit und sicherheit des ultraleicht - molekulargewichtigen heparins semuloparin zur verhtung venser thromboembolien bei 2312 patienten , welche eine chemotherapie wegen einer krebserkrankung erhielten , untersucht . 
patienten mit metastasierten oder lokal fortgeschrittenen soliden tumoren , welche mit dem ersten zyklus chemotherapie begannen , wurden fr semuloparin ( 20 mg 1 - mal tglich ) randomisiert oder erhielten ein plazebo bis zur nderung des chemotherapieregimes . 
vense thromboembolien traten bei 20 von 1608 patienten ( 1 , 2% ) auf , welche semuloparin erhielten , im vergleich zu 55 von 1608 ( 3 , 4% ) , welche nur ein placebo bekamen ( hazard - ratio [ hr ] 0 , 36 ; 95% - konfidenzintervall [ ci ] 0 , 210 , 60 ; p < 0 , 001 ) , mit gleichbleibender wirksamkeit in den subguppen , welche nach tumorart , stadium und allgemeinrisiko definiert wurden . 
schwere blutungen traten bei 19 von 1589 patienten ( 1 , 2% ) auf , welche semuloparin erhielten und bei 18 von 1583 ( 1 , 1% ) ohne semuloparin ( hr 1 , 05 ; 95% ci 0 , 551 , 99 )  . 
semuloparin reduziert die inzidenz von thromboembolischen ereignissen bei onkologischen patienten , welche eine chemotherapie erhalten , ohne ersichtliche zunahme von schweren blutungen . kommentar vense thromboembolische embolien sind verbreitete komplikationen von tumorerkrankungen , welche mit einer erhhung von morbiditt , letalitt und kosten sowie mit einem mehraufwand in medizinischer versorgung allgemein einhergehen . neben lngerer hospitalisation und operationen wird auch die chemotherapie zunehmend als ein risikofaktor erkannt . 
dabei scheint die metastasierungsrate durch eine interzellulre interaktion via selektin , eine inhibierung der protease heparanase und eine hemmung der angiogenese reduziert zu werden [ 1 ]  . die vorliegende studie [ 2 ] wurde nach hohem standard aufgelegt : hohe patientenzahl , multizentrisch , doppeltblind , randomisiert mit intention - to - treat - analyse , ein unabhngiges bewertungsgremium und eine geringe rate an fehlenden daten . 
kritisch anzumerken bleibt dabei jedoch , dass die auswertung durch sanofi , den hersteller von semuloparin , erfolgte . als primum fanden sich tumoren von lunge , pankreas , magen , kolon , rektum , harnblase oder ovarien . 514 | strahlentherapieundonkologie62013 korrespondenzadresse s.heller klinik und poliklinik fr strahlentherapie und radioonkologie , universittsklinikum carl gustav carus an der technischen universitt dresden fetscherstr . 
der behandlungseffekt zeigte sich auch gleichbleibend ber die anzahl von bestehenden risikofaktoren fr die entstehung venser thromboembolien . die arbeit schloss insgesamt 3212 randomisierte patienten mit einem mindestalter von 18 jahren aus 47 lndern e dies sind deutlich mehr patienten als in einer aus der cochrane - datenbank zusammengefassten analyse von 9 studien ( insgesamt 2857 patienten ; [ 3 ] ) , bei denen neben dem antithrombotischen effekt auch eine antitumorse wirkung untersucht wurde . 
jedoch ergab die cochrane - datenbank - analyse nach 24 monaten ein signifikant besseres os . trotz der signifikanten verringerung des risikos thrombotischer und thromboembolischer komplikationen bleiben mehrere offene fragen , die zum teil auch im zugehrigen editorial gestellt werden [ 4 ] : f bisher liegen keine verlsslichen daten zur lebensqualitt von mit heparin behandelten patienten im vergleich zu kontrollkollektiven vor . 
in der vorliegenden studie konnte eine auswirkung auf das berleben der patienten nach einem jahr nicht besttigt werden . f es ist davon auszugehen , dass das allgemeine thromboserisiko bei verschiedenen tumorarten und - stadien unterschiedlich ist . 
 solch eine klassifizierung knnte jedoch bei unterschiedlicher wirksamkeit sicher zu einer verbesserung der effektivitt des prophylaktischen einsatzes niedermolekularer heparine in der onkologie fhren . f bei den insgesamt sehr niedrigen raten thrombotischer und thromboembolischer komplikationen ist auch eine kosten - nutzen - analyse zu fordern . eine genauere abklrung dieser fragen kann natrlich nur durch weitere studien erfolgen . 
however , with increased doses , both delineation of the target volume and high - precision dose delivery are important to prevent increased toxicity to the surrounding organs [ 8 ]  . radiation therapy ( rt ) after radical prostatectomy offers an overall and biochemical relapse - free survival benefit when applied in adjuvant and salvage settings [ 9 , 10 , 11 , 12 ]  . 
in contrast to published data on prostate motion [ 13 , 14 , 15 , 16 ] , data on patient setup uncertainties and prostate bed motion during postprostatectomy rt are sparse [ 17 , 18 , 19 , 20 ]  . 
small shifts in target volume have the potential to significantly alter the distribution of the dose delivered to adjacent organs . the side effects of postprostatectomy gold marker implantation may differ from those arising after their implantation in the highly vascularized prostate gland . 
based on the low bleeding risk after intraprostatic gold marker implantation [ 5 ] , anticoagulant therapy was continued in one center ( radboud university nijmegen medical centre , runmc ) , but stopped for a week at the other ( medical centre alkmaar , mca )  . 
transrectal ultrasound ( trus ) - guided gold marker implantation was performed by two physicians using a bk medical pro focus 2202 ( bk medical , herlev , denmark ) or a bk medical falcon 2102 exl ultrasound device ( bk medical , wilmington , usa )  . 
using portal imaging and planning ct scans , migration or loss of gold markers from the prostate bed was recorded . recording complications patients received questionnaires directly after the implantation procedure and filled them out during the first week . 
 patients reported whether the implantation was bothersome and scored the pain on a 010 visual analogue scale ( vas , 0 : no pain ; 10 : worst pain imaginable )  . 
complications were defined as : ( 1 ) minor : transient minimal discomfort without medical intervention , ( 2 ) moderate : moderate discomfort or requirement of additional treatment and ( 3 ) major : requiring hospital admission . 
to analyze any bias in recording complications , the retrospectively gathered data were compared to the prospective data . potential risk factors for complications were evaluated by reviewing the medical charts and contacting all patients . 
a secondary hypothesis was that local tumor infiltration and wide surgical excision ; the surgical technique itself ; stricturesfor which endodilatation or bladder neck incision were necessaryor incontinence may have stimulated fibrosis formation and result in more pain upon marker implantation . 
 the initial pathological tumor stage , surgical technique , presence of incontinence or strictures , the time interval since surgery and age were therefore evaluated for their influence on pain during the procedure . statistical analysis of bleeding complications was performed using fishers exact tests to compare categorical variables . 
 differences in vas scores caused by potential risk factors were tested for statistical significance using the parameter - free mannwhitney u test for two groups , or the kruskalwallis test for three groups . 
a two - sided p - value < 0.05 was considered statistically significant . strahlentherapieundonkologie62013 | abstract zusammenfassung strahlenther onkol 2013 189 : 476481 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0323 - 4 j.f.langenhuijsenr.donkerg.m.mccolll.a.l.m.kiemeneyj.a.witjese.n.j.t.vanlin postprostatectomy ultrasound - guided transrectal implantation of gold markers for external beam radiotherapy . 
other complications included rectal discomfort ( n = 2 ) , nausea ( n = 1 ) , abdominal discomfort ( n = 1 ) , and pain requiring analgesics ( n = 4 )  . 
alternatives like cone beam computed tomography ( cbct ) should be considered , but the advantages of gold marker implantation for high - precision postprostatectomy rt would seem to outweigh the minor risks involved . keywords prostate cancer prostate - specific antigen coumarins anticoagulants adjuvant radiotherapy ultraschall gefhrte transrektale implantation von goldmarkierungen fr externe strahlentherapie nach prostatektomie . 
in die studie wurden mnner eingeschlossen , die wegen eines erhhten prostataspezifischen antigens ( psa ) nach einer prostatektomie oder wegen eines hoch - risiko - prostatakarzinoms mit einer strahlentherapie behandelt wurden . 
andere komplikationen waren rektale beschwerden ( n = 2 ) , belkeit ( n = 1 ) , abdominale beschwerden ( n = 1 ) und mit analgetika behandelte schmerzen ( n = 4 )  . 
alternativen wie die cone - beam - ct sollen erwogen werden , aber die vorteile einer implantation fr eine hochprzisions - rt nach prostatektomie erscheinen im vergleich zu den relativ geringen risiken grer . schlsselwrter prostatakarzinom prostataspezifisches antigen cumarin antikoagulantien adjuvante strahlentherapie results between february 2008 and february 2011 , gold markers were implanted in 77 consecutive patients with psa relapse ( n = 70 ) or high - risk disease ( n = 7 ) after radical prostatectomy . 
patients had been operated on using open ( n = 48 ) , laparoscopic ( n = 10 ) or robot - assisted laparoscopic radical prostatectomy ( n = 19 )  . 
questionnaires were filled out retrospectively by 41 patients , at a mean of 18.79.3 months after marker implantation . feasibility of gold marker implantation a substitute marker was received by 1 patient because misplacement into the bladder wall was observed during trus . 
1 complication rates following gold marker implantation in the prostate bed complications patientsn = 76 ( % ) complications minor macroscopic hematuria > 3 days rectal bleeding voiding complaints ( urgency ) moderate pain requiring analgesics rectal discomfort fever nausea other major 0 ( 0% ) 10 ( 13% ) 1 ( 1% ) 4 ( 5% ) 2 ( 3% ) 0 ( 0% ) 1 ( 1% ) 1 ( 1% ) 0 ( 0% ) tab . 
extensive surgery and anastomotic strictures did not increase pain during marker implantation . strahlentherapieundonkologie62013 | original article discussion in this retrospective analysis the ultrasound - guided transrectal implantation of gold markers for postprostatectomy rt was shown to be feasible and associated with a low complications rate . 
discrimination between gold markers and surgical clips during imaging has been suggested to pose problems [ 22 ] , but this was not experienced by our radiation oncologists . this is the first report specifically evaluating the complications of gold marker implantation in the prostate bed in a larger collective of patients . 
in a large patient group , hematuria persisting for more than 3 days was reported in 3.8% of patients and 9.1% had rectal bleeding for an average 2.5 days following implantation of intraprostatic gold markers [ 5 ]  . 
no urosepsis was found in our patients , possibly due to less vascularization of the prostate bed compared to the prostate gland and the low potential for the systemic spread of bacteria . 
 provided the bladder was not empty , the anastomosis site was clearly visible during trus - guided marker implantation , and the chance of urethra perforation with gross macroscopic hematuria was therefore low . 
because bleeding was minor and self - limiting in the presence of anticoagulant medication , this therapy should be continued in patients with a high risk of thrombo - embolic events . 
few moderate complications occurred , but 1 patient reported nausea that could have been caused by bacteremia or ciprofloxacin use . most patients had undergone diagnostic prostate biopsies , which possibly lead to a higher level of acceptance of gold marker implantation . 
a study with differentiated qol assessments for intraprostatic gold markers found no significant differences between preand postimplantation measurements [ 4 ]  . the influence of postoperative strictures on pain during marker implantation was evaluated . 
the prophylactic use of analgesics can therefore be advocated , particularly in young patients . cone beam ct ( cbct ) scans represent a good , less invasive alternative to gold marker - based image - guided rt [ 27 ] , but this technique is not routinely available in every center . 
cbct provides a comprehensive three - dimensional overview of the geometric situation in the pelvis , thus enabling appropriate intervention in the case of dramatic changes in bowel and bladder filling . 
 the role of perineal ultrasound surveillance for primary prostate cancer rt is also currently under investigation , although this is not yet an established tool in the adjuvant or salvage setting . the shortcomings of this study are that questionnaires were completed retrospectively by 41 patients , which may have led to underreporting of complications due to a recall bias . 
only 7 patients received gold markers in an adjuvant setting , therefore these results are mainly valid for the salvage setting . in our centers , trus - guided transrectal implantation of gold markers for post5 . 
pinkawa m , siluschek j , gagel b et al ( 2007 ) postoperative radiotherapy for prostate cancer : evaluation of target motion and treatment techniques ( intensity - modulated versus conformal radiotherapy )  . 
sandhu a , sethi r , rice r et al ( 2008 ) prostate bed localization with image - guided approach using on - board imaging : reporting acute toxicity and implications for radiation therapy planning following prostatectomy . 
int j radiat oncol biol phys 67 : 610619 ( 2006 ) daily variations in the position of the prostate bed in patients with prostate cancer receiving postoperative external beam radiation therapy . 
dehnad h , nederveen aj , heide ua van der et al ( 2003 ) clinical feasibility study for the use of implanted gold seeds in the prostate as reliable positioning markers during megavoltage irradiation . 
henry am , wilkinson c , wylie jp et al ( 2004 ) transperineal implantation of radio - opaque treatment verification markers into the prostate : an assessment of procedure related morbidity , patient acceptability and accuracy . 
park r , martin s , goldberg jd , lepor h ( 2001 ) anastomotic strictures following radical prostatectomy : insights into incidence , effectiveness of intervention , effect on continence , and factors predisposing to occurrence . 
although it should be realized that there are alternatives and that implantation of gold markers is an invasive procedure which could have potentially serious complicationsin our experience , complication rates are negligible . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 467475 doi 10.1007 / s00066 - 013 - 0321 - 6 received : 14 november 2012 accepted : 23 january 2013 published online : 20 . 
combination with hormone treatment is associated with a survival benefit of 10% or greater [ 7 , 8 ]  . metastatic or both metastatic and local disease are found in the majority of patients with biochemical progression who have previously undergone rt . 
the phoenix definition ( a 2 ng / ml increase in absolute psa nadir ) is currently the most commonly applied measure of biochemical failure after rt [ 11 ]  . 
the available options range from watchful waiting to hormone treatment , surgery , brachytherapy and cryoablation [ 12 , 13 , 14 ]  . the addition of hyperthermia to rt may enhance the effect of the latter . 
the thermal enhancement ratio ( ter ) was estimated to be about 1.42.0 [ 15 ] and it has been suggested that the effect is greatest when hyperthermia treatment directly precedes brachytherapy . 
promising results have also been observed by combining interstitial hyperthermia ( iht ) with external beam radiotherapy ( ebrt ) [ 17 , 18 , 19 ]  . in patients with other cancers , results of randomized studies have shown a benefit of rt combined with hyperthermia over rt alone [ 20 , 21 , 22 ]  . 
several nonrandomized studies on the use of both methods in the treatment of prostate cancer are also available [ 17 , 23 ]  . we launched our high - dose - rate ( hdr ) brachytherapy treatment program for prostate cancer at the centre of oncology , krakow in 2006 , and began combining iht with brachytherapy in 2008 . 
here we present the results of a retrospective analysis of the feasibility and early toxicity of iht combined with hdr brachytherapy as both the initial therapy for prostate cancer patients and for previously irradiated patients with local recurrence . patients and methods the analysis included patients treated for prostate cancer using interstitial hdr brachytherapy of the prostate combined with iht between 18 december 2008 and 5 september 2012 at the centre of oncology , krakow . 
a total of 73 patients diagnosed with prostate cancer received the combined treatment during this time frame . patient characteristics in all patients , prostate cancer had been confirmed by biopsy . 
imaging studiespelvic ultrasound , computed tomography ( ct ) or magnetic resonance imaging ( mri ) , chest x - ray or ct and bone scanswere performed to evaluate the clinical disease stage . 
the patients were also advised about standard management options , including prostatectomy or ebrt . the patients characteristics are presented in .tab.1. eligibility criteria for brachytherapy and hyperthermia all the patients met the following eligibility criteria qualifying them for brachytherapy : prostate volume 1260 cc ; pubic symphysis anatomy permissive of applicator insertion ; distance between posterior margin of the prostate and rectum 5 mm and transurethral resection of the prostate ( turp ) 6 months before the procedure . 
contraindications for hyperthermia treatment were metal pelvic implants or bleeding tumors . radiobiological considerations hdr brachytherapy allows for a precise delivery of very high doses to the prostate gland tumor and a relatively small volume of normal tissue in the rectum and the bladder . 
several reports suggested that the / ratio for prostate cancer be as low as 13 gy , which justifies the use of high fraction doses [ 25 , 26 , 27 ]  . 
the equivalent doses in 2 - gy fractions ( eqd2 ) for our treatment schedules using different / ratios ( 1 , 3 and 10 gy ) are summarized in .tab.2. the hyperthermia procedure we performed iht using the bsd500 system ( bsd medical corporation , salt lake city , ut , usa )  . 
the aim of the treatment was to heat the peripheral zone of the prostate to 4143c for 60 min prior to irradiation ( with the exception of 2 patients from the iht + hdr brachytherapy group )  . 
hyperthermia was performed before brachytherapy for two reasons : firstly , because the theoretical premise from the preclinical studies is that this has a better enhancing effect , and secondly for practical reasons , in order not to prolong the duration of the treatment ( brachytherapy planning is more time consuming than hyperthermia planning )  . 
following implantation of the needle catheters , the image of the reference slice with reconstructed needle positions in the prostate is transferred from the brachytherapy planning system to the energy - distribution planning tool . 
regarding the temperature sensors , 12 are placed in the catheters fixed to a transrectal ultrasound probe that remains in the rectum during the procedure ; another 12 are placed in the catheters inserted into the prostate tisabstract zusammenfassung strahlenther onkol 2013 189 : 467475 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0321 - 6 a.m.kukiekam.hetnap.brandyst.walasekt.dbrowskie.plutad.nahajowskir.kudzia interstitial hyperthermia of the prostate in combination with brachytherapy . 
in 54 patients this was the initial therapy for prostate cancer , while the other 19 were treated for local recurrence after previously undergoing external beam radiotherapy ( ebrt )  . 
the most common minor complications were urinary frequency ( grade 1 : 37% ; grade 2 : 22% ) , nocturia ( three times per night : 29% ; fouror more times per night : 20% ) and transient weakening of the urine stream ( grade 1 : 36% ; grade 2 : 11% )  . 
further prospective clinical studies should focus on the effects of combining iht with hdr brachytherapy and the influence of this adjuvant therapy on biochemical disease - free survival , local control and overall survival . keywords prostate cancer radiotherapy prostate - specific antigen nocturia toxicity interstitielle hyperthermie der prostata in kombination mit brachytherapie . 
 ins gesamt 54 patienten wurden wegen eines primrtumors der prostata und 19 patien ten sue in closest proximity to the urethra and the other 24 are located in the prostate tissueoptimally in those areas where the lowest and the highest heat intensities are predicted by the planning tool . 
if there are indications that the depth of subarachnoid anesthesia is decreasing or if the patient moves too much during the procedure , it is acceptable to reduce the duration of hyperthermia . 
die hufigsten milden komplikationen waren pollakisurie ( grad 1 : 37% , grad 2 : 22% ) , nykturie ( 3 - mal pro nacht : 29% , 4 - mal und mehr pro nacht : 20% ) und eine vorbergehende schwchung des harnstrahls ( grad 1 : 36% , grad 2 : 11% )  . 
weitere prospektive klinische studien sollten die effekte der verbindung der interstitiellen hyperthermie mit der hdrbrachytherapie und den einfluss dieser adjuvanten therapie auf das berleben ohne biochemische rezidive , die lokale kontrolle und die gesamtberlebensraten untersuchen . schlsselwrter prostatakrebs strahlentherapie prostataspezifisches antigen nykturie toxizitt dure not be performed at all , since delivery of radiation is the primary goal . 
 the intention was to provide hyperthermia before each fraction of brachytherapy . the brachytherapy procedure the implantation procedure begins with subarachnoid anesthesia , after which the patient is placed in the lithotomy position . 
based on the contoured structures , a physicist plans an initial distribution of catheters ( prepares a pre - plan ) that will meet predetermined dose constraints ( discussed further below )  . 
trus is repeated , whereupon the contours of the prostate , rectum and urethra are verified ; the applicator positions are reconstructed and the final treatment planto be carried out after the iht procedure is completedis prepared . 
the fractions are usually administered at 3 - week ( 21 - day ) intervals . if the disease is limited to the prostate ( t1at2c ) , the clinical target volume ( ctv ) includes the whole prostate gland as visible on 1 mm - separated sonography images , without safety margins . 
if the tumor extends outside the prostate capsule ( t3a ) , the ctv includes the prostate gland and any extracapsular extension of the tumor with a 12 mm margin prostate cancer brachytherapy , the planning target volume ( ptv ) is identical to the ctv . 
 the urethra is defined as the outer surface of the foley catheter and the rectum is defined as the muscle layer outside the mucosa ( muscularis mucosae )  . the aim is to achieve the prescribed dose for 90% of the ptv ( d90 ) , whereby the acceptable level is 95% . 
additional parameters related to the ptvsuch as maximum dose ( dmax ) , mean dose ( dmean ) and the volume of the prostate receiving 100 , 150 and 200% of the prescribed dose ( v100 , v150 and v200 , respectively ) are reported for the purposes of evaluating the treatment plan . 
in critical organs such as the anterior wall of the rectum and the bladder , dmax should not exceed more than 80% of the prescribed dose and in the urethra it should not exceed 120% of the prescribed dose . 
the approved plan was checked independently by a second physicist . external beam radiotherapy previously untreated intermediateand high - risk patients received a course of 50 gy three - dimensional conformal ebrt applied to the prostate , the base of the seminal vesicles and / or the pelvic lymph nodes ( 2 - gy fractions ; 1 fraction per day , 5 fractions per week ) according to a standard four - field isocentric technique . all the patients were immobilized in a supine position . 
in cases of extraprostatic extension ( t3 / t4 ) , the ctv also included extracapsular invasion and / or the whole of the seminal vesicles ( delineation was based on ctmri fusion )  . 
where the risk of lymph node involvement was higher than 15% , the ctv also included the presacral - , the internal iliacand part of the commonand external iliac lymph nodes . 
since 2011 , gold anchor markers have been implanted for the purpose of visualizing the prostate during treatment ( image - guided radiation therapy , igrt )  . androgen deprivation therapy almost all the patients ( 71 out of 73 ) received hormone therapy . 
androgen deprivation therapy ( adt ) consisted of a luteinizing - hormone - releasing hormone ( lhrh ) agonist ( goserelin , triptorelin or leuprolide ) with the addition of an antiandrogen ( in most cases flutamide )  . 
if adt was administered to shrink an excessively large prostate gland to an acceptable size in a low - risk patient , it was started 3 months before the first brachytherapy fraction and continued for 3 months upon completion of the treatment . 
in intermediateand high - risk patients , adt was administered in a neoadjuvant ( 13 months ) or adjuvant setting ( 3 12 months for intermediate - riskand 12 21 months for high - risk patients )  . 
the median duration of hormone therapy was 18 months ( range 495 )  . the iht + hdr brachytherapy group in 3 patients with primary prostate cancer , hdr brachytherapy was administered at a dose of 45 gy in 3 fractions separated by 3 weeks . 
of these patients , 2 were stratified as low - risk prostate cancer patients and 1 as intermediate - risk ( initial psa 11.29 ng / ml , gleason score 3 + 3 , ct2a ; this patient refused ebrt )  . 
hyperthermia was administered to1 of the low - risk patients because of a long interval ( 65 days ) between the second and third brachytherapy fractions ( the patient had been hospitalized for severe pneumonia )  . 
hyperthermia was used within these lesions to enhance the effect of radiation solely in the tumor tissue . the ebrt + ( iht + hdr brachytherapy ) group toxicity assessment this group comprised 51 patients with primary intermediateand high - risk prostate cancer ( psa > 10 ng / ml , gleason score 7 , t stage 2b ) not amenable to radical prostatectomy or brachytherapy alone . 
patients received a combined treatment program that included ebrt ( 50 gy in 25 2 - gy fractions ) as the first stage , followed by a hdr brachytherapy boost21 gy in 2 fractions separated by 3 weeks . 
this program was implemented in january 2011 at the centre of oncology , krakow . the toxicity for the organs of the genitourinary system and rectum was retrospectively assessed according to the common terminology criteria for adverse events ( ctcae ) protocol , version 4.03. 
assessment was based on data from patient records , interviews and international prostate symptom score ( i - pss ) questionnaires , 3 months after treatment . results the median follow - up time was 15 months ( range 346 )  . the iht + salvage hdr brachytherapy group feasibility brachytherapy was the salvage treatment for 19 patients with local recurrence who had previously undergone curative rt for prostate cancer . 
during follow - up , increasing psa levels were found in this group and a trus - guided biopsy confirmed local tumor recurrence ( 17 out of 19 experienced biochemical failure according to the phoenix definition [ 11 ] )  . 
all the patients were treated with a dose of 30 gy in 3 fractions separated by 3 weeks ( the regimen applied by the majority of polish centers using hdr brachytherapy )  . follow - up the follow - up time was measured from the completion of brachytherapy up to the date of the last recorded follow - up visit or the death of the patient . 
the follow - up visits for patients treated with brachytherapy at our institute were scheduled 1 , 6 and 12 weeks after treatment and at 3 - month intervals thereafter . combined treatment comprising iht and hdr brachytherapy is feasible during standard subarachnoid anaesthesia for brachytherapy . 
the duration of the combined procedure is not significantly prolonged ( about 1530 min ) because the heating procedure is performed while the physicist reconstructs the catheter positions and prepares the final brachytherapy treatment plan . 
in 11 cases , the planned procedure was not carried out because of failure of the hyperthermia equipment and in 5 further patients , only saddle - block anaesthesia was achieved . 
 thermometry of the hyperthermia system failed during one course of treatment , as a consequence of which the treatment was discontinued after 15 ma total of 12 patients received one course of hyperthermia , 47 patients underwent two procedures , and 14 had three treatments . 
in 1 patient the treatment ( both brachytherapy and hyperthermia ) was limited to only one session because of a traumatic femur fracture that prevented continuation of brachytherapy . brachytherapy the mean d90 ptv value was 97.2% of the prescribed dose . 
the doses for critical organs and eqd2 values are summarized in .tab.3. temperatures the mean duration of the therapeutic hyperthermia procedure was 49 min ( range 1560 min )  . 
no aggravation of rectal complications was noted in patients previously treated with ebrt and no rectal toxicity was found in patients treated only with brachytherapy combined with hyperthermia . in the majority of patients , perineal , penile or hypogastric pain was self - limiting within the first 24 h following the procedure and required no additional analgesics ( except where these were routinely prescribed by an anaesthesiologist )  . 
 erectile dysfunction was treated with sildenafil or another drug from this group , although the patients were not monitored for sexual dysfunction . discussion hdr brachytherapy is a method that allows radiation doses to be administered accurately within the prostate . 
it is used both as an initial treatment for prostate cancer ( as a boost or definitive treatment ) and as a salvage therapy for cases of local recurrence in patients who have previously undergone irradiation . iht of the prostate may be carried out using the same guiding catheters that will later be used to introduce the 192ir radioactive source . 
a temperature of 41c was maintained in the prostate for 45 m after a 28 - month follow - up , neither biochemical recurrence nor grade 3 reactions were observed [ 34 ]  . a study by prionas et al . 
comprising 31 prostate cancer patients receiving initial treatment and 5 patients with recurring prostate cancer showed that combination of these two methods is feasible and well tolerated [ 35 ]  . in the following section we discuss the safety of other methods for the initial therapy of prostate cancer and the treatment of local recurrence in patients who have previously undergone irradiation . when hdror pulsed - dose - rate ( pdr ) brachytherapy is administered as the initial treatment , acute irritative urinary symptoms are common . 
severe complications ( grade 3 ) occur in less than 15% of patients and are as follows : necrosis ( < 1% ) , urethral stricture ( up to 15% ) and grade 3 rectal mucositis ( 0.32% ) [ 36 , 37 , 38 , 45 ]  . observed for these methods either before , or 1 or 6 months post rt [ 40 ]  . when brachytherapy is used as a salvage treatment for patients who have previously undergone rt , urinary incontinence occurs in about 6% of cases where concomitant hormone therapy is administered . 
no grade 3 reactions were observed [ 41 , 42 ]  . in the van vulpen study , the most frequent complication occurring after combined treatment was pathis was observed in 65% of cases and usually located in the perineal region , although also sporadically in the hipor sacral bone and testes . 
observed no grade 3 reactions in cases where regional hyperthermia plus ebrt was used as the initial treatment for prostate cancer in 144 intermediateto high - risk patients [ 17 ]  . in a study by kalapurakal et al . 
18% chronic g 3 rectum : 5% no g3g4 g4 cystitis : 1 rectal ulcer and fistula : 1 no g3g4 not given no g3g4 no g3g4 original article previouslyirradiated ? tab . 
the profile is also similar to results reported elsewhere [ 45 ]  . the combined hyperthermia plus hdr brachytherapy treatment was well tolerated by the analyzed group and our results correspond to those reported in the literature . a literature search did not yield any analysis that involved a larger number of patients than our study . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 456461 doi 10.1007 / s00066 - 013 - 0346 - x received : 27 july 2012 accepted : 6 march 2013 published online : 28 . 
 recent data show an increased incidence of glioblastoma ( gbm ) in the elderly population , with a peak seen between the ages of 65 and 84 years [ 16 , 18 , 20 ]  . 
since elderly gbm patients have a poorer outcome , a number of authors investigated unusual post - surgical treatment schedules to reduce hospitalization : most studies reported the survival among elderly patients to be 48 months on average [ 37 , 38 , 52 ] and observed a worsening of quality of life ( qol ) after aggressive treatment schedules [ 15 , 27 , 31 ]  . on the other hand , a number of small prospective studies have shown some benefit from chemotherapy [ 2 , 3 , 5 , 9 ] , radiation therapy ( rt ) [ 8 , 37 , 44 ] , and maximal safe resection [ 50 ] in patients aged 70 and older . 
moreover , a retrospective study of 394 elderly gbm patients treated at the memorial sloan - kettering cancer center was published in 2009 [ 26 ] , as a result of which the authors concluded that more aggressive treatment may lead to a survival benefit for elderly patients . there is strong evidence that rt prolongs survival compared with supportive care alone , without compromising qol or cognition in elderly patients with gbm [ 30 , 46 ]  . 
however , treatment lasting 56 weeks may increase the burden of care for patients and their caregivers , despite a lack of influence reported on qol . the accelerated schedule of rt has been studied in the past [ 28 , 29 ]  . 
a randomized three - arm trial , conducted by eortc cooperative group of radiotherapy on 340 patients , compared : ( a ) the standard schedule of rt ( single - day fraction to a 60 gy ) , to ( b ) a three - daily - fractions schedule ( 2 gy / fr , approximately 4 h between doses ) for 5 days with a split of 2 weeks and ( c ) a three - daily - fractions schedule of rt concomitant to a radiosensitizer [ 21 ]  . 
the results are straightforward : no significant differences were found between standard and altered schedules of rt , either in terms of survival or qol . according to the literature [ 28 ] , a hypofractionated rt schedule was offered to elderly people at our institution in the recent past before the widespread adoption of the stupp protocol ( 20002004 )  . 
since the delivery of standard fractionation requires a high number of visits to rt departments for patients and their caregivers and can generate some distress in the elderly population , especially those living at a distance from rt centres , a hypofractionated accelerated rt ( hart ) schedule was offered to elderly patients with the aim of reducing the overall time required for therapy . 
this was intended to avoid decreasing patients and caregivers qol whilst offering the advantage of avoiding the burden of care ( anxiety , cost , and iatrogenic effects of treatment )  . we decided to conduct a retrospective review of elderly gbm patients treated with this alternative schedule rt . the purpose of this study was to verify and confirm the feasibility of shortcourse hart as radiation treatment for gbm patients older than 70 years and with a good kps ( 70 )  . our main aim was to evaluate the tolerability and toxicity of the rt schedule ; secondary endpoints were progression free survival ( pfs ) and overall survival ( os )  . patients and methods retrospective review the neurological carlo besta institute foundation ethics committee board approved this single - centre retrospective study ( record number 26 , of 2012 april 4 )  . a review of the neurological carlo besta institute foundation medical records was undertaken ; patients aged 70 years or older with high - grade glioma having received hart between january 2000 and january 2004 were included in the study . 
1 patient characteristics number ( range ) weighted% baselinecharacteristics gender female male age mean extentofsurgery total resection subtotal resection biopsy salvagechemotherapy bcnu ( 150 mg / m2 every 8 weeks ) 74 ( 7082 ) treatment or had received prior chemotherapy . 
data obtained included age , sex , histological diagnosis , date and type of surgery , radiation treatment characteristics , kps before rt and 3 months after , date of radiological or clinical progression , salvage treatment at progression and date of last known status . radiotherapy split - course hart was started within 24 weeks of surgery and performed on a day - hospital basis for the whole duration of rt in order to evaluate early adverse effects . patients were prescribed to have a total dose ( td ) of 45 gy : td was administered in two cycles ( split 15 days ) , 2.5 gy / fraction , three daily fractions ( inter - fraction time 4 h ) for three consecutive days / cycle . 
before starting the second cycle patients underwent neurological and clinical evaluation : in cases of neurological deterioration the schedule was stopped . the planning target volume ( ptv ) consisted of the contrast - enhanced tumour defined radiographically by preoperative computed tomography ( ct ) or magnetic resonance imaging ( mri ) excluding oedema , plus a 1 - cm margin . the mean volume of ptv was 185 cc ( median 198 cc ; range 38150 cc ; sd83 )  . 
the variables that were considered and evaluated included : extent of surgery ( type : biopsy , subtotal or gross - total resection ) , gender , age at surgery , kps and rpa scores before rt , salvage chemotherapy and the presence or absence of major toxicity during the first 3 months of follow - up . 
in addition , since there was an association between os time and type of surgery , all models were stratified by type of surgery . results patient characteristics between january 2000 and january 2004 , 58 patients aged 70 years or older with a diagnosis of supratentorial high - grade glioma and a kps between 50 and 100 were evaluated for postoperative radiotherapy . 
the extent of resection was based on the neurosurgeons impression and / or postoperative mri : any mri enhancement thought to represent residual tumour after resection was categorized as subtotal resection . 
altogether , 16 patients underwent gross total resection , 13 subtotal and four stereotactic biopsy . at progression , seven patients ( 29.6% ) received reduced - dose nitrosourea - based chemotherapy consisting of intravenous bcnu ( 1 , 3 - bis ( 2 - chloroethiyl ) - 1 - nitrosour ea ) 150 mg / m2 every 8 weeks . 
 all patients had died at the time of analysis . patient characteristics are summarized in .tab.1. toxicity the rt schedule was well tolerated : only one patient ( 3% ) experienced cognitive disturbance , reversible with high - dose steroid - based therapy ( grade 3 )  . 
none of the patients , including those with longer follow - up , developed radiation necrosis . kps evaluation 3 months after completion of rt was stable in 18 patients ( 73% ) , strahlentherapieundonkologie62013 | original article abstract zusammenfassung strahlenther onkol 2013 189 : 456461 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0346 - x l.fariselliv.pinzii.milanesia.silvanim.marchettim.farinottia.salmaggi short - course radiotherapy in elderly patients with glioblastoma : feasibility and efficacy of results from a single centre abstract background . 
our findings suggest that a hypofractionated accelerated schedule can be a safe and effective option in the treatment of gbm in the elderly . keywords hypofractionated radiation therapy glioblastoma elderly kurzzeitstrahlentherapie bei lteren glioblastompatienten : durchfhrbarkeit und effektivitt der ergebnisse einer einzelnen einrichtung zusammenfassung hintergrund . 
die resultate unserer studie zeigen , dass die hypofraktionierte , akzelerierte strahlentherapie eine sichere und wirksame behandlungsoption fr ltere patienten mit gbm sein kann . schlsselwrter hypofraktioniert strahlentherapie glioblastom ltere improved in six ( 24% ) and worse in one ( 3% ) patient . only one of seven patients who received salvage chemotherapy experienced haematological toxicity ( grade2 neutropenia and thrombocytopenia )  . in terms of adverse events , three patients ( 9% ) died with stable disease ( sd ) and one patient ( 3% ) with complete response ( cr ) at 2 , 5 , 6 and 7 months , respectively , from non - tumor - related causes ( heart disease and thromboembolism )  . treatment response and survival the median follow - up was 10 months ( range 224 months , mean 11 months )  . 
due to the small proportion of patients who underwent biopsy only , a com458 | strahlentherapieundonkologie62013 parison to scotts rpa classes 3 or 4 [ 47 ] was intentionally omitted . discussion currently , older age is among the most significant prognostic factors associated with poor prognosis in gbm patients . 
detailed gbm elderly populations have been studied mainly in different small case cohorts of patients [ 14 , 17 , 23 , 37 , 40 , 52 , 53 ]  . 
a previous recursive partitioning analysis of prognostic factors for gbm including 832 patients of all ages demonstrated that patients aged > 65 years had the worst prognosis , independent of the extent of surgical resection or performance status [ 32 ]  . 
other authors studied prognostic factors in 676 gbm patients of all ages and showed no evidence of interactions between the effects of rt and patient age [ 12 ]  . some data on elderly patients with gbm indicated that , even in younger patients [ 11 ] , advancing age , kps and extent of tumour resection were independent prognostic factors [ 14 , 26 , 47 ]  . moreover , emerging data on biological features between primary and secondary glioblastoma further suggest that tumors in older patients may be more aggressive [ 31 , 41 ]  . 
however , in the opinion of a number of authors , this data could be affected by an initial selection bias in overall populations as well as in elderly populations [ 8 , 11 , 45 , 48 , 50 ]  . finally , older age may be associated with a poor prognosis , but elderly patients may achieve improved survival by means of surgery and / or adjuvant or alternative treatments . 
indeed , keime - guilberts randomized controlled study showed prolonged survival in patients > 70 years ( 70 years old or older ) with a kps 70 , treated with 50 gy vs . 
 short - course rt has also been investigated for patients older than 6570 years , with interesting results on survival and without increased toxicity [ 7 , 18 , 21 , 29 , 37 , 40 ]  . 
in a randomized trial , roa [ 44 ] reported no significant change in median overall survival ( mos ) when comparing standard fractionated rt ( 30 frx2 gy , 60 gy in 6 weeks ) to hypofractionated rt ( 15 frx2.66 gy , 40 gy in 3 weeks ) for gbm patients older than 60 years ( mean age 71 years )  . 
the impact of altered rt fractionation in patients aged 70 years have also been evaluated in the past in a number of trials with a mos between 4 and 8 months [ 19 , 34 , 37 , 42 ]  . 
these studies suggest that hypofractionated rt may be a reasonable alternative schedule for elderly gbm patients . therefore , the optimal treatment schedule for elderly patients has yet to be determined [ 2 , 4 , 35 , 39 ]  . 
in our cohort of patients treated with aggressive hypofractionated schedule , os was similar to results in the literature and longer than in the rt - treated arm of keime - guilbert trial [ 30 ]  . 
although the schedule adopted is undoubtedly more aggressive than other schedules , we did not observe any increase in neurological complications during the radiation course and follow - up ; kps was stable or improved in 97% of patients at 3 months , demonstrating the importance of clinical status at the beginning of treatment . one limitation of our study is the weak radiobiological rationale connected to the retrospective analysis of data . nevertheless , the choice of hypofractionation aims to minimize the effect of tumor repopulation and may increase tumor destruction by means of the greater dose per fraction [ 6 ]  . 
although different altered schedules of irradiation have been used over the years , there is a lack of data on toxicity and molecular effects , mainly on cellular repair mechanisms . the other important question of whether the short os in elderly gbm patients may be prolonged by chemotherapy as an alternative , or in addition to rt has not yet been answered satisfactorily : in the noa - 08 and nordic trial [ 13 ] , chemotherapy alone was compared with rt alone , with different results ( similar efficacy in the nordic trial , but not in the noa - 08 ) ; differences in patient features and chemotherapy schedule are probably at the basis of these discrepant results . 
 however , two recent studies reported on the benefit of multimodality therapy in elderly gbm patients , showing an os of as long as 17.2 months [ 46 ] and an odds ratio for death as low as 0.45 ( p < 0.0001 ) [ 26 ] , respectively . in this context , the ongoing eortc trial , which is currently under investigation in our daily practice , will clarify whether concomitant and adjuvant temozolomide associated with hypofractionated rt is able to increase pfs and / or os in elderly gbm patients . the analyzed results of this schedule on mos are similar to results obtained with conventional fractionated rt . 
the extent of surgery was confirmed to have a favourable impact on os , whilst the addition of salvage chemotherapy did not contribute to improved os ( although the low number of treated patients precludes conclusions to be drawn on this point )  . reducing the period of treatment in elderly patients remains a good alternative to standard therapy : our data confirm that rt is also beneficial in the elderly patient population and that the overall treatment time can be considerably shortened without a detrimental effect on clinical outcome . however , future studies need to be performed using diseaseand possibly agespecific instruments for qol measurement and should also include measurement of qol in caregivers . strahlentherapieundonkologie62013 | original article corresponding address v . 
the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 502507 doi 10.1007 / s00066 - 013 - 0324 - 3 received : 17 september 2012 accepted : 13 january 2013 published online : 28 . 
adenoid cystic carcinoma is the predominant histologic type among malignancies of the minor salivary glands [ 20 , 29 ]  . in general , acc is characterized by slow progression , wide perineural invasion , a relatively low probability of regional lymph node metastases , and a pronounced ability to recur over a prolonged period [ 20 , 27 ]  . 
therefore , it is important to control local diseases in order to prolong survival and improve quality of life [ 50 ]  . surgery is generally recommended for acc [ 16 , 19 , 30 , 32 , 48 ]  . 
however , the early and wide invasion associated with this tumor , as well as the complexity of the local anatomy , can make it difficult to obtain negative margins during surgery . 
therefore , many oncologists recommend postoperative radiotherapy ( rt ) for advanced disease , a close or incomplete resection , bone invasion and perineural invasion in an attempt to improve local control [ 2 , 15 , 26 , 48 ]  . 
reports suggest that the 5and 10 - year local control rates for head and neck acc are 4046 and 21 25% , respectively , when treated surgically alone , and increase to 6495 and 6883% , respectively , when treated with surgery and postoperative radiotherapy [ 20 , 36 ]  . however , the management of recurrent and / or locally advanced unresectable acc , particularly for those who have previously had external beam rt , remains a challenge [ 9 ]  . 
although external beam rt alone is a modality for patients with unresectable tumors , the redelivery of effective doses is almost impossible because of the limited tolerance of adjacent normal critical structures [ 1 ]  . 
a systematic review revealed that chemotherapy might have a palliative benefit for a small proportion of patients with recurrent acc of salivary gland origin , though the effects of chemotherapy remain controversial [ 16 , 25 , 48 ]  . brachytherapy may resolve this issue by delivering a high dose of radiation directly to the tumor , while simultaneously sparing adjacent normal tissue [ 11 , 46 ]  . 
 the benefits of brachytherapy for the treatment of malignant tumors have been demonstrated , and a variety of radioactive sources have been used [ 1 , 3 , 11 , 12 , 13 , 26 , 34 , 37 , 41 , 49 ]  . the purpose of this study was to evaluate the feasibility and effectiveness of using 125i brachytherapy alone for the management of recurrent or locally advanced acc of the oral and maxillofacial region . patients and methods a total of 38 patients with recurrent or locally advanced acc of the oral and maxillofacial region received 125i brachytherapy alone at the peking university school and hospital of stomatology between 2001 and 2010 . 
 the tumor size varied from 1.58 cthe histological diagnosis was obtained by incisional biopsy or needle aspiration biopsy before brachytherapy . inclusion criteria were as follows : patients with recurrent and locally advanced unresectable tumor after prior surgery and radiotherapy ; patients with locally advanced tumor with inoperable disease who refused external rt . 
 the prescribed dose target volume ( ptv ) was outlined by oncologists to cover the lesion with a 0.51 cm margthe prescribed dose ( pd , or matched peripheral dose ) of the 125i implant was 100160 gy , which was adjusted according to the dose of prior radiation and the adjacent struc502 | strahlentherapieundonkologie62013 tab . 
the v100 ( the percentage of the target volume receiving at least 100% of the prescription dose ) of each patient was more than 95% , and the v150 ( the percentage of the target volume receiving at least 150% of the prescription dose ) for all cases was less than 50% . 
patients with recurrent disease ( n = 29 ) had a 5 - year lc rate of 57.3% , while those with primary disease ( n = 9 ) had a lc rate of 66.7%. 
1 patient characteristics 54 ( 782 ) characteristics age ( years ) , median ( range ) sex ( n ) male female tumorsite ( no.ofpatients ) major salivary glands ( parotid , submandibular , sublingual gland ) minor salivary glands of oral cavity paranasal / skull base region ( including nasal cavity ) tumorsize ( no.ofpatients ) < 3 cm 36 cm > 6 cm distantmetastasisatfirstvisit ( no.ofpatients ) priortreatmentfortumors ( no.ofpatients ) none surgery radiotherapy ( conventional fractionation , 2 gy / day ) surgery and radiotherapy ( conventional fractionation , 1.82 gy / day ) priorsurgerytimes three or more priorradiotherapytimes priorcumulativeradiotherapydose ( no.of patients ) < 60 gy 6066 gy > 66 gy tures . 
the actuarial d90 ( dose delivered to 90% of the target volume ) was larger than pd in all padistant metastases were present in 9 patients prior to 125i implantation ; 8 patients developed distant metastases after 125i implant . 
the lungs were most frequently involved with distant metastases ( n = 16 ) , followed by the liver ( n = 2 ) , and bone ( n = 1 )  . only 1 patient with a tumor in the oral cavity developed a neck metastasis 14 months after implantation , and subsequently underwent a neck dissection . pain control the pain change scaled according the visual analogue scale ( vas ) system before and after 125i implant occurred in 7 of the 11 patients between 1 and 8 months after brachytherapy . 
pain disappeared in 1 patient who had a tumor in the parotid gland 2 months after implantation ; partial or mild improvement in pain occurred in 6 patients 0.252 months after implantation ; and no obvious changes were observed in 4 patients , all of who had tumors in the oral cavity . complications no severe complications ( rtog grades 34 ) were observed . 
in all , 19 patients experienced temporary minor side effects ( rtog grades 1 and 2 ) , including mild pain and cutaneous pigmentation . discussion surgery is generally recommended for resectable acc [ 16 , 48 ] , and adjuvant external rt is usually administered if there are adverse risk factors , such as close or positive margins , perineural or vascular invasion , lymph node metastases , or if the tumor is in advanced stages [ 2 , 6 , 21 , 24 , 26 ]  . 
overall , 12 tumors were located in the major salivary glands , 12 in the minor salivary glands , and 14 in the paranasal region , the nasal cavity or the skull base . 
125i brachytherapy is a feasible and effective modality for the treatment of locally advanced unresectable or recurrent acc . keywords brachytherapy adenoid cystic carcinoma oral and maxillofacial salivary gland neoplasms head and neck neoplasms alleinige 125i brachytherapie zur behandlung rezidivierter oder lokal fortgeschrittener adenoid - zystischen karzinome in mund - , - kieferund gesichtsbereich zusammenfassung hintergrundundziel . 
bei 12 patienten war die tumorlokalisation in den groen speicheldrsen , bei weiteren 12 patienten in den kleinen speicheldrsen und bei 14 patienten in der paranasalen region , der nasenhhle oder der schdelbasis . 
die 125i - brachytherapie ist praktikabel , wirksam und stellt eine modalitt in der behandlung eines lokal fortgeschrittenem inoperablem oder rezidiviertem acc dar . schlsselwrter brachytherapie adenoid - zystisches karzinom oral und maxillofazial speicheldrsenneoplasien kopfund halsneoplasien claims that postoperative rt does not have any obvious benefits [ 23 , 28 ]  . although acc has been considered relatively radioresistant , external rt has been used alone in patients unfit for surgery or in those with inoperable disease [ 4 , 7 , 22 , 29 , 30 , 31 , 40 , 47 ]  . 
 [ 1 ] reported an average progression - free survival of 52 months in patients with recurrent palatal accs treated with 198au implant brachytherapy , 198au with its short half - life of 2.7 days has been used more frequently to treat squamous cell carcinomas and other tumors that proliferate rapidly [ 11 , 43 ]  . 
125i brachytherapy has increasingly been used for slowly progressive salivary gland malignant tumors , due to its long half - life ( 59.4 days ) , low photon energy ( 2735 kev ) and to the fact that it can be easily screened , thus , protecting adjacent vital structures and attending staff [ 11 , 51 ]  . 
 [ 11 ] reported disease - free survival for cases of head and neck cancer ( 8 of 18 patients were with acc ) of 89 and 53% at 2 and 5 years , respectively , following surgery and 125i implants , which found that 125i implants did not result in any additional complications . 
 [ 51 ] reported a 100% lc rate and no complications ( follow - up 5074 months , median 66 months ) in patients with residual parotid malignant tumors post - surgery treated solely with 125i brachytherapy . 
 [ 17 ] treated recurrent head and neck cancer with 125i implants alone and reported a 5 - year lc rate of 39% . as a monotherapy for acc , external radiotherapy has achieved 5and 10 - year lc rates of approximately 3766 and 3643% , respectively [ 4 , 7 , 30 , 31 ] , and 5and 10 - year os rates of 5679 and 3742% , respectively [ 4 , 7 , 30 , 31 ]  . 
the distant metastases rate , and the interval from 125i implantation to the occurrence of metastases observed in our study , is similar to that reported by other studies [ 5 , 23 ]  . in this study , we presented our experience of treating locally advanced or recurrent acc with 125i implants alone . 
considering the stage of the tumors in the series , the lc and os results are encouraging , and suggest that 125i brachytherapy is a feasible and effective modality for the treatment of unresectable or recurrent acc after prior surgery and radiotherapy , which seems better than external beam radiation . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 486494 doi 10.1007 / s00066 - 013 - 0314 - 5 received : 13 september 2012 accepted : 16 january 2013 published online : 2 . 
all surviving patients might potentially experience some of the late sequelae of the treatment , including stool and urinary incontinence , urgency , dysuria , dyspareunia and erectile dysfunction [ 1 , 2 , 3 , 4 ] ; some of which might have an impact on the patients qol . 
radiotherapy ( rt ) consisted of 3645 gy ( 1.8 gy per fraction ) to the lower part of the pelvis covering the primary tumor bed , perirectal - , presacral - , internal ilical - , external iliacaland inguinal nodes . 
three patients ( 7% ) were treated with rt alone due to t1n0 category ( n = 1 ) , the patients refusal of chemotherapy ( n = 1 ) and age ( n = 1 )  . of these patients , 44 had died and 9 were lost to follow - up . 
one physician interviewed the patients regarding the presence / absence / intensity of relevant side effects during the past 2 weeks . the functional assessment of cancer therapy - colorectal ( fact - c ) tool was used to assess qol . 
this self - report instrument combines common concerns of all cancer patients as addressed by factgeneral ( fact - g ; score range 0108 , with higher scores indicating better general well - being ) with those of colorectal cancer patients . 
fact - c reliability and validity for the assessment of qol in patients with colorectal cancer has been shown in various publications [ 7 , 8 , 9 ]  . 
the questionnaire consists of 34 items in total , with five subscales concerning physical well - being , social / familial well - being , emotional well - being , functional well - being and the colorectal cancer - specific items . 
the fact - c score can range from 0 to 136 , with higher scores indicating a better grade 3 / 4 grade 1 / 2 no symptoms fecal incontinence stool frequency a nal pain a nal he m orrhage d ysuria urinary urge erectile dysfunction urinary frequency urinary incontinence libid o vaginal sy m pto m s d yspareunia fig . 
the y - axis indicates the percentage of patients no significant differences were noted with regard to demographic - , clinicalor treatment characteristics or to the prevalence of cae between patients who agreed to participate in the survey and those who did not ( data not shown )  . the median follow - up time of the patients was 68 months ( range 9 222 months )  . statistical analysis in order to describe differences in the distribution of fact - c scores between the groups , the median and range of the physical , social / familial , emotional , functional and colorectal subscale scores were reported . 
all questions refer to the last week prior to the interview . eight questions concerning demographic characteristics such as marital status , partnership , children , household , education , employment status , economic situation and monthly net income were added . the study was approved by the ethics committee of the faculty of medicine of the technische universitt mnchen . eligible patients were invited to visit our department . 
female patients were asked at the appointment if they had performed the vaginal supportive care ( vaginal creams , vaginal bath ) during , and 8 weeks after the treatment ( possible responses werenot at all , irregularly orregularly )  . for 42 patients , both cae and factc information was available . 
the most common grade 3 cae were dyspareunia and vaginal symptoms ( itching , burning and dryness ) in 35 and 22% of female patients , respectively ; followed by stool incontinence in 13% of all patients , regardless of gender . 
the median scores in the subscales were ( median standard deviation / possible maximum score ) : physical : 246 / 28 , social / familial : 235 / 28 , emotional : 203 / 24 , functional : 226 / 28 and colorectal : 224 / 28 . 
high difstrahlentherapieundonkologie62013 | abstract zusammenfassung strahlenther onkol 2013 189 : 486494 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0314 - 5 k.fakhriant.sauera.dinkels.klemmt.schusterm.mollsh.geinitz chronic adverse events and quality of life after radiochemotherapy in anal cancer patients . 
the most common grade 3 cae were dyspareunia and vaginal symptoms ( itching , burning and dryness ) in 35 and 22% of female patients , respectively , followed by stool incontinence in 13% of all patients ( 6 out of 49 )  . 
in order to improve long - term qol , future strategies might aim at a reduction in dose to the genitalia and more intensive patient support measures . keywords chemotherapy dyspareunia fecal incontinence toxicity survival chronische nebenwirkungen und lebensqualitt nach radiochemotherapie bei analkarzinompatienten . 
the median fact - c score of patients with a follow - up time < 67 months was only 4 points lower than that of patients with a follow - up time 67 months . 
the authors described poor sexual functioning in their cohort of ac patients : 75% reported a lack of sexual interest as a problem ; 71% of patients reported that the inability to relax and enjoy sex was a problem and 72% of patients reported that difficulty in becoming sexually aroused was a probleamong 6 male patients in their group , 4 ( 67% ) reported erectile dysfunction . 
 [ 10 ] were the first investigators to compare the qol of ac survivors ( n = 50 ) with that of healthy volunteers ( n = 50 )  . 
useing the european organisation for research and treatment of cancer ( eortc ) qlq - c30 and qlq - cr38 qol questionnaires , they reported significantly higher scores for overall qol , as well as for physical and sexual functioning scales in healthy volunteers . 
however , only in areas of sexual enjoyment ( a numerical difference of 24 points ) and sexual problems did the differences reach very much changed levels . in line with the studies of jephcott et al . 
it is of note that about two thirds of the female patients in our group reported some degree of vaginal symptoms and dyspareunia . although several reports of vaginal symptoms and dyspareunia after pelvic rt for gynecological cancers indicate a prevalence of 260% [ 12 , 13 , 14 , 15 , 16 ] , female sexual morbidity remains a neglected aspect of routine follow - up and cancer survival . 
 [ 17 ] reported that during follow - up after pelvic rt , physical toxicity assessment was focused mainly on bowel ( 81% ) and bladder ( 70% ) symptoms , whereas vaginal toxicity and sexual issues were explored in only 42% and 25% of consultations , respectively . 
in our group , 7 female patients did not initially want to answer the questions regarding vaginal symptoms and dyspareunia , until a senior female colleague asked them to talk about these issues in a separate session . 
of these 7 patients , 5 had some degree of dyspareunia and found it embarrassing to talk about or report on this issue , despite the anonymous nature of the questionnaire . vaginal symptoms such as dryness , itching and bleeding , as well as sexual morbidity most likely result from late radiation damage . 
a few studies have demonstrated that intensity - modulated radiation therapy ( imrt ) can reduce radiation dose to the genitalia in patients with ac [ 18 , 19 , 20 , 21 ]  . 
nevertheless , additional dosimetric and clinical studies are required to assess whether sophisticated rt techniques and modalities such as tomotherapy and positron - emission tomography / computed tomography ( pet - ct ) for radiation planning [ 22 , 23 , 24 , 25 ] ; or simple supportive positioning instruments such as intravaginal cuffs or cylinders , could allow a reduction in the dose delivered to ( parts of ) the internal and / or external genitalia , and whether this has any impact on the incidence of cae and qol in ac patients . another important undefined issue concerns supportive care to prevent sexual morbidity and the appropriate treatment options . 
the efficacy of conventional supportive care comprising vaginal baths , vaginal creams and vaginal expander sets has been the topic of controversial discussion in the literature [ 14 , 15 , 26 , 27 ]  . 
 while these measures might help in a subgroup of patients , they seem to be insufficient to prevent or treat vaginal symptoms for a considerable portion of patientsincluding 14 ( out of 37 ) female patients in our group ( .tab.2 ) who applied the supportive care at least partially . 
there are a few reports about other types of supportive care and treatment options to prevent late toxicity , such as hyperbaric oxygen therapy [ 28 , 29 ]  . 
however , their role in improvement of gynecologic symptoms is still uncertafuture studies are needed to investigate the role of supportive care ( more intensive or / and new agents ) during and after rct . in a recently published study , welzel et al . 
 [ 6 ] reported that the global health qol in ac patients was comparable to that of previously published reference data from the ( age - adjusted ) general german population [ 30 ]  . 
they assessed qol using qlq - c30 and qlq - cr38 and cae according to the late effects in normal tissues subjective , objective , management , and analytic ( lent / soma ) scale in 52 patients ( 37 female and 15 male ) with a median follow - up interval of 36 months ( range 5137 months )  . 
they described problems relating to cancer - specific psychosocial qol , fatigue , insomnia , urological / gastrointestinal complaints and impairment of sexual function as the five main concerns in their series . 
in their series , marital status significantly influenced female sexual function and employment status was significantly associated with emotional functioning , social functioning , sexual enjoyment and gastrointestinal symptoms in the univariate analysis . 
in our group of patients , high school graduation or a higher level of education was significantly associated with a better qol in the multivariate analysis , but maritaland employment status had no impact on qol ( data not shown )  . in one of the first reported series on qol in ac patients , vordermark et al . 
 [ 3 ] evaluated the late gastrointestinal sequelae of rct and qol ( instrument : gastrointestinal quality of life index , giqol [ 31 ] ) in 22 colostomy - free survivors after a median follow - up time of 3 years . 
 [ 32 ] , who reported the giqol of healthy volunteers ( n = 150 , 121 points ) and patients with other benign anorectal diseases ( n = 325 , 113 points ) , whereby they found qol scores among their ac patients to be similar to those in healthy volunteers and patients with benign disease . 
this is in line with our results , which indicate that patients with a longer follow - up interval ( and thus more time to adapt to symptoms ) have slightly higher qol scores . in another report from the late 1990s , allal et al . 
however , allal and coworkers did not observe any effect of follow - up time on qol ; they found no difference in qol values between patients with a follow - up time of less than 10 years and more than 10 years . 
 one should note that in the study by allal et al . , all patients had a minimum follow - up time of 3 years and the cutoff interval was set to 10 years . 
we hypothesize that the adaptation to symptoms and improvement in qol reported by vordermark and the current study probably occur during the first 2 years after treatmenta period not evaluated by allal et al . 
 [ 33 ] compared the qol in 17 ac survivors who were treated with external beam radiation therapy ( ebrt ) + ebrt boost with that of 17 ac survivors who were treated with ebrt + brachytherapy ( ibt )  . 
they observed higher qol values for patients treated with an ebrt boost compared to an ibt boost ( 86 vs.72 points ) , although this did not reach statistical significance . 
 [ 34 ] conducted a short - term , longitudinal randomized controlled trial , using the qlq - c30 questionnaire to evaluate qol before and 2 months after rct in 119 patients . 
they also observed a significant decrease in insomnia , appetite loss and paunfortunately , the long - term cae and qol values were not published at the time of the current study . 
as rct is the main treatment modality for the management of ac , an important goal for radiation oncologists is to improve or preserve the health - related qol in these patients . 
the median fact - g score of our patients ( 8917 ) is similar to those of published series taken from the general population in the united states ( 8016 ) , australia ( 8615 ) and austria ( 8715 ) , as well as to that of patients that received rct for a variety of other pelvic malignancies ( 8513 ) [ 35 , 36 , 37 , 38 ]  . 
however , a considerable number of ac patients experistrahlentherapieundonkologie62013 | grade death life - threatening consequences ; urgent intervention indicated death life - threatening consequences ; urgent intervention indicated tab . 
4.0 , which were used for this study ( continued ) adverseevent grade1 grade2 grade3 grade4 renal and urinary disorders ; other , specify asymptomatic or mild symptoms ; clinical or diagnostic observations only ; intervention not indicated moderate , local or noninvasive intervention indicated ; limiting instrumental adl severe or medically significant but not immediately life threatening ; hospitalization or prolongation of existing hospitalization indicated ; disabling ; limiting self - care adl life - threatening consequences ; urgent intervention indicated grade death adl activity of daily living . enced late adverse effects ( lae ) of rct , which significantly affected their qol . the correlation between acute and late toxicity has been the topic of controversial discussion in the literature . 
some studies indicate a correlation between acuteand late normal tissue injury after rt in the pelvic region [ 39 , 40 ] , whereas others report no - , or only a weak correlation between the incidence and severity of acute and late reactions [ 41 , 42 ]  . in our series we could not observe any correlation between acute and late toxicity . our series had a number of limitations . 
 firstly , it was a retrospective analysis of a small group of patients , thus the uniand multivariate analyses have to be interpreted cautiouslythey allow for general conclusions , but specific ones might be elusive . 
similarly , patients hormonal statuses were not available to examine if an imbalance exists due to rt in the pelvic region . however , this study indicates a correlation between cae and qol and highlights the necessity of further efforts to prevent cae . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 495501 doi 10.1007 / s00066 - 013 - 0310 - 9 received : 17 october 2012 accepted : 16 january 2013 published online : 24 . 
as sbrt allows precise delivery of high radiation doses in few fractions , it facilitates reduced overall treatment times and is thus an attractive option in patients with a compromised health status . 
fluorodeoxyglucose posi tronemission tomography ( fdg - pet , pet ) is also a valuable tool in posttherapeutic follow - up of nsclc patients [ 18 , 19 , 20 ] , although its role in assessment of local tumor control is controversial . 
moreover , a pilot study reported that glucose metabolism does not predict outcome 12 weeks after sbrt , most likely due to unspecific tracer uptake originating from radiation - induced reactive changes [ 22 ]  . 
however , the relevance of elevated posttherapeutic standard uptake values ( suv ) for predicting local recurrence could not be evaluated in this study , as no local failures occurred in the short followup period [ 23 ]  . 
in 29 patients ( 7 t1 and 22 t2 tumors ) , additional posttherapeutic pet / ct imaging was performed 1 year after radiotherapy ( rt ) in the case of unequivocal ct findings . 
patients received 300 ml imeron contrast medium for ce - ct , unless they had a recent ct ( not older than 2 weeks ) , in which case no iv . 
in the follow - up pet studies , the rois were placed at the same position as in the baseline scan , using the position of the tumor in ct and anatomical landmarks on ct images as references . radiation treatment and planning sbrt was performed as described previously [ 1 ]  . 
gross tumor volume ( gtv ) was defined as the tumor visible in the lung window of the planning ct scan without further margins for the clinical target volume ( ctv )  . 
before each applied fraction , breathing motion was compensated for using a slow , single - slice ct scan to derive an individual margin that was complemented by an additional margin of 10 mm in the longitudinal - , and 5 mm in the axial direction to derive the ptv . 
positioning of the immobilized patient and target location was verified before every treatment fraction by individual scans ; either by way of a ct scan in the treatment position to derive the stereotactic isocenter coordinates , or using on - board cone beam ct ( from july 2008 onward )  . follow - up following hypofractionated sbrt , patients were scheduled for regular followup visits at 46 week , and subsequently 3 month intervals . 
as detailed previously [ 24 ] , fdg - pet / ct functional imaging was only required in cases of locally persistent tumor at 12 months ( or later ) , or where there was clinical suspicion of local failure based on ct scans of the thorax . local tumor response was defined as followed : ( 1 ) complete remission : complete disappearance of tumor or replacement by fibrotic tissue confirmed by a negative pet scan , ( 2 ) partial response : reduction of at least 50% in volume , or where there was any suspicious residual density in ct scans that was not fdgpet positive and ( 3 ) local progression : increase in tumor volume of more than 25% on ct scans , accompanied by metabolic activity in fdg - pet and / or positive histology ( according to our recent publication [ 1 ] )  . 
in the instance of ambiguous findings , ct or pet / ct imaging was repeated at 3 - month intervals before invasive histological confirmation was prompted . statistical analysis for description of the data , mean standard deviation and the range of observed values ( minimummaximum ) are given for quantitative measurements ; absolute and relative frequencies are shown for qualitative data . 
the best cutoff values for discrimination between patients with high and low causespecific hazards were estimated using maximally selected logrank statistics for different events of interest ( death , disease - specific death , local failure , mediastinal failure , distant metastasis )  . 
corresponding p - values were derived from permutation tests comparing the maximum logrank statistics obtained from all possible data splits with maximally selected log rank statistics simulated under the null hypothesis ( no correlation between suvs and hazards , as proposed recently [ 25 ] )  . 
for disease - specific survival , cumulative incidence curves estimating the probability of disease - specific death versus time as are displayed for the identified risk groups [ 26 ]  . 
the ability of standard uptake values ( suvmax , suvmean and posttherapeutic reduction in suv ) to detect local failure and identify patients at a high risk of disease - specific death was evaluated using logrank statistics . 
as posttherapeutic glucose metabolism also correlates with disease - specific survival , pet / ct may help to stratify lung cancer patients for additional treatment 1 year after sbrt . keywords salvage therapy survival local recurrence metastasis glucose metabolism positronenemissionstomographie - ct zum lokalrezidivnachweis bei stadium i - lungenkarzinompatienten 1 jahr nach stereotaktischer bestrahlung zusammenfassung ziel . 
die wertigkeit des posttherapeutischen suvmax , suvmean und der posttherapeutischen abnahme der suv - werte zur detektion von lokalrezidiven und zur stratifizierung von patientengruppen mit erhhtem risiko fr einen krankheitsspezifischen tod wurde mittels log - rank - statistik evaluiert . 
52% ( p = 0 , 025 ) wiesen auf ein lokalrezidiv hdiese parameter zeigten auch eine korrelation mit dem krankheitsspezifischen berleben : suvmean - werte ber 2 , 81 ( p = 0 , 023 ) , suvmax ber 3 , 45 ( p = 0 , 007 ) oder eine abnahme des suvmean oder des suvmax von weniger als 32% ( p = 0 , 015 ) bzw . 
da der posttherapeutische glukosemetabolismus auch mit dem krankheitsspezifischen berleben korreliert , knnte die pet - ct zur stratifizierung von patienten , die von einer zustzlichen behandlung profitieren , hilfreich sein . schlsselwrter salvage - therapie berleben lokales rezidiv metastasierung glukosemetabolismus a two - sided level of significance of = 5% . 
mean times to occurrence of distant metastases and mediastinal failure were 1615 and 1815 months , respectively . metabolic activity in follow - up pet we determined suvmean and suvmax in these patients and compared them to the pretherapeutic values . 
b cumulative incidence of disease - specific death and one minus cumulative incidence for death from other causes in our collective of nsclc patients ure and a high risk of disease - specific death . 
a posttherapeutic suvmean greater than 3.44 ( p = 0.001 ) ; suvmax greater than 5.48 ( p = 0.009 ) or a relative reduction in suvmean or suvmax of less than 43 ( p = 0.03 ) or 52% ( p = 0.025 ) , respectively , was found to be indicative of local recurrence . 
a posttherapeutic suvmean greater than 2.81 ( p = 0.023 ) ; suvmax greater than 3.45 ( p = 0.007 ) or a relative reduction in suvmean or suvmax of less than 32 ( p = 0.015 ) or 52% ( p = 0.013 ) , respectively , correlated with short diseasespecific survival . 
there was also a trend toward correlation between absolute posttherapeutic suvmean or suvmax and mediastinal failure ( p = 0.055 in both cases ) , but statistical significance was not reached . 
the line charts show the change in suvmax ( c ) and suvmean ( d ) in each individual patient and suvmean were lower in the follow - up compared to the pretherapeutic pet / ct in all but one patient . 
this patient had local failure . diagnostic value of follow - up pet / ct discussion logrank tests were performed to obtain cutoff values for posttherapeutic suvmean , suvmax and the change in suv that discriminate patients with local failsbrt is an effective novel treatment for inoperable stage i nsclc . 
several groups have reported inconclusive results regarding the value of post - sbrt follow - up pet scans [ 21 , 22 , 29 , 30 , 31 ]  . 
the group from the md anderson cancer center found a most reliable correlation using measurements taken beyond 6 months after sbrt : suvs greater than 5 exhibited a sensitivity of 100% and a specificity of around 90% for local recurrence [ 30 ]  . 
on the other hand , the tissue response to radiation damage includes reactive processes such as inflammatory changes and macrophage infiltration , and a subsequent increase in glucose metabolism may be present at these time points . 
although the results from studies using fixed time intervals for functional imaging after sbrt are quite intriguing , an optimal strategy for recommending pet / ct examinations following sbrt has not yet been established . 
still , this group did not derive specific suv cutoff values , but rather used suvs greater or equal to pre - sbrt values for the definition of local recurrence . 
in these cases , we were able to define cutoff values indicative of local recurrence : posttherapeutic suvmax greater than 5.4 , suvmean greater than 3.4 , a relative reduction in suvmax of less than 52% or a reduction of suvmean of less than 43% . 
as very high ablative radiation doses are applied in sbrt , one can speculate that although [ 18f ] - fdg is a non - specific marker , it may still hint at an aggressive , more radioresistant phenotype . 
on the other hand , metabolic activity may be partly due to radiation - induced tissue remodeling . additionally , in our series a posttherapeutic reduction of suvmax of less than 62% was associated with an increased risk of mediastinal failure . 
since not all patients with mediastinal failure had documented local failure , this correlation can only partly be attributed to secondary metastatic spread from remaining metabolically active tumor tissue . at this point , a pragmatic approach seems most reasonable : upon suspicious ct findings more than 6 months after sbrt [ 33 ] , pet / ct investigations should be prompted . 
in the case of suvmax exceeding 5 ( [ 30 ] , this data ) or a reduction in suvmax of less than 50% ( this data ) , histological verification of local recurrence should be obtained . 
routine pet followup at specified time points after sbrt is not yet indicated by the available data . disease - specific and overall survival posttherapeutic glucose metabolism correlated significantly with disease - specific survival , indicating that our findings are of prognostic relevance . 
such a prospective trial would also be important to validate the cutoff values proposed by this study in a larger patient collective . original article time in months time in months change in suv mean ( % ) > - 32 ( cid : 100 ) - 32 change in suv mean ( % ) > - 52 ( cid : 100 ) - 52 time in months time in months fig . 
3 8 estimated probability for disease - specific death of patients with post - therapeutic suvmean greater or less than 2.81 ( a ) , post - therapeutic suvmax greater or less than 3.45 ( b ) , a relative reduction in suvmean of less or greater than 32% ( c ) and relative reduction in suvmax of less or greater than 52% ( d ) nsclc , with some series reporting local control rates exceeding 90% for small tumors [ 25 ]  . 
although an intriguing basic concept , the risk of overtreatment of patients with elevated posttherapeutic suvwho may never develop local failureneeds to be considered in a patient group with considerable comorbidity . 
as patients with a posttherapeutic reduction in suvmax of less than 62% have an increased risk of local recurrence and mediastinal failure , this group may benefit from an additional chemotherapy to help control lymph node metastases and tumor tissue surviving sbrt . 
therefore , instead of focusing on local control and local salvage therapies , an alternative approach would be the evaluation of systemic treatment strategies in patients with a high risk of subsequent failure . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 590591 doi 10.1007 / s00066 - 013 - 0363 - 9 online publiziert : 29 . 
mai 2013 springer - verlag berlin heidelberg 2013 j.dunst klinik fr strahlentherapie , universittsklinikum schleswig - holstein campus kiel kardialerisikender adjuvantenradiotherapie beimmammakarzinom originalbeitrag darby sc , ewertz m , mcgale p et al ( 2013 ) risk of ischemic heart disease in women after radiotherapy for breast cancer . 
man konnte ferner eine klare dosis - wirkungs - beziehung ermitteln : pro gray herzdosis stieg das risiko fr ein koronarereignis um 7 , 4% , also um den faktor 1 , 074 . 
die risikoerhhung von 7 , 4% pro gray war der mittelwert ber 20 jahre nachbeobachtung ; der risikozuwachs war in den ersten jahren am hchsten : 16 , 3% pro gray in den ersten 4 jahren , in den jahren 10 19 nur 1 , 2% pro gray . 
lebensjahr an einer khk zu versterben ( death from ischemic heart disease ) fr eine 50 - jhrige frau ohne kardiale risikofaktoren von 1 , 9% ohne strahlentherapie auf 2 , 4% nach bestrahlung mit einer mittleren herzdosis von 3 gy ( also um 0 , 5 prozentpunkte )  . 
die dosis - wirkungs - beziehung erlaubt es , das individuelle risiko zu ermitteln und gegen vorteile der bestrahlung abzuwgen . kommentar die arbeit hat in den usa viel wirbel verursacht . 
die fakten sind nmlich seit langem bekannt , und frau darby selbst hat mit der early breast cancer trialsists collaborative group mehrfach auf dieses thema hingewiesen [ 1 , 3 , 4 ]  . 
clarke m , collins r , darby s et al ( 2005 ) effects of radiotherapy and of differences in the extent of surgery for early breast cancer on local recurrence and 15 - year survival : an overview of the randomised trials . 
early breast cancer trialists collaborative group ( 2000 ) favourable and unfavourable effects on long - term survival of radiotherapy for early breast cancer : an overview of the randomised trials . 
early breast cancer trialists collaborative group ( ebctcg ) , darby s , mcgale p , correa c et al ( 2011 ) effect of radiotherapy after breast - conserving surgery on 10 - year recurrence and 15 - year breast cancer death : meta - analysis of individual patient data for 10 , 801 women in 17 randomised trials . 
des relativen risikos um 7 , 4% , also von 1 , 000 auf 1 , 074 pro gray mittlerer dosis am herzen . zweitens ist das problem bereits lange bekannt , und alle radioonkologen sind mittlerweile so sensibilisiert fr das thema , dass strahlendosen im relevanten bereich praktisch nicht mehr vorkommen , es sei denn , dass dies aufgrund einer individuellen risikokonstellation eindeutig gerechtfertigt ist , z . 
als beweis kann die krzlich abgeschlossene aro - 2010 - 01 - studie gelten , in der bei 151 patientinnen die durchfhrbarkeit einer hypofraktionierten bestrahlung mit integriertem boost geprft wurde . 
different amrr intensities and durations are observed , which generally depend on the dose - intensities determined by dose fractionation schedules and concomitant chemotherapy [ 1 , 6 , 8 , 15 , 16 , 18 , 19 , 20 , 21 ]  . 
long - lasting and intense amrr may cause increasing dietary problems and a consequent decrease in the quality of life [ 11 ] .observation of amrr during treatment should therefore be performed in all patients at regular intervalsat least once a week [ 14 , 21 ]  . there is a well - known phenomenon of accelerated repopulation in acute - responding tissues during radiotherapy that is also observed in healthy mucosa in the head and neck region [ 7 , 10 ]  . 
although there are some clinical trials evaluating amrr toxicity , detailed data concerning the course of amrr are still lacking [ 4 , 9 , 12 , 13 ]  . the purpose of this study was to investigate individual patterns of amrr in head and neck cancer patients who were all treated with radiation therapy alone , but according to four different fractionation schedules . 
results are based on daily , individual evaluation of amrr intensity according to the dische scoring system for acute mucosal reactions [ 2 ]  . the study was approved by the ethics committee and patient consent was obtained before treatment . materials and methods patients a total of 87 consecutive patients with head and neck squamous cell cancer ( mean age 55 years ; range 3674 years ) were recruited into this prospective evaluation of amrr between 1999 and 2006 . 
treatment was performed using either conventional fractionation ( cf ; 33 patients ) , accelerated fractionation ( af ; 33 patients ) , hyperfractionated ( hpefx : 12 patients ) or hypofractionated ( hpofx ; 9 patients ) radiotherapy with radical intent . 
no patient suffered from any other comorbidities that might have influenced the intensity and duration of amrr . treatment all patients were irradiated with megavoltage equipment ( 6and 20 mv linear accelerators )  . 
hpofx fractionation was only used for early and moderately advanced , node - negative laryngeal cancer located in the larynx ( t2n0 ) and comprised doses of 2.5 gy per fraction , 5 days a week for 5 weeks . 
1 dische scoring system for acute mucosal radiation reactions results original article items mucosal reactions area involved edema bleeding ulceration dysphagia , diet pain scores 0 : none ; 1 : slight erythema ; 2 : marked erythema ; 3 : spotted mucositis ; 4 : confluent mucositis 0 : none ; 1 : 25% ; 2 : 2550% ; 3 : 50100% 0 : none ; 1 : slight ; 2 : moderate ; 3 : severe 0 : none ; 1 : slight , incidental ; 2 : slight , multifocal ; 3 : marked , regular 0 : none ; 1 : single , superficial ; 2 : multifocal , superficial ; 3 : single , profound ; 4 : multifocal , profound 0 : normal ; 1 : exclusion of some food ; 2 : soft , pureed food only ; 3 : fluids only ; 4 : tube feeding or intravenous alimentation 0 : none ; 1 : during eating only ; 2 : constant , but moderate , non - steroid analgesics ; 3 : constant , serious , narcotics required tab . 
no interruptions to radiation treatments were recorded . in all patients , verification of the treatment fields was standard procedure and dose delivery was controlled using in vivo dosimetry . mucosal examination all patients were hospitalized in our department . 
examinations were performed for oral , pharyngeal and laryngeal mucosa , but evaluation of amrr intensity according to the dische scoring system was restricted to the volume corresponding to the boost fields ( high - dose volume )  . 
the daily sums of these parameters ( possible maximum of 24 ) were used to draw curves representing the individual amrr course for each patient , which were subsequently analyzed . constant elevation of the curve up until the end of radiotherapy assigned patients into the continual increase course group . 
patients of the decreasing course group had curves showing a decline of 2 or more points after the plateau phase ( but still during radiotherapy ) that continued up until the last day of irradiation . 548 | strahlentherapieundonkologie72013 a latency period between the start of rt and the onset of amrr was observed in all patients and ranged between 3 and 14 days ( 8 days on average )  . 
boost field sizes ranged widelyfrom 28 cm2 for patients with early / moderately advanced cancer without metastatic neck nodes , to 95 cm2 for patients with advanced local and nodal disease ( majority of hpefx patients )  . 
 decreasing course of amrr was observed in at total of 20 / 87 ( 23% ) patients : 11 / 33 ( 33% ) cfand abstract zusammenfassung strahlenther onkol 2013 189 : 547551 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0311 - 8 a.wygodat.rutkowskim.hutnikk.skadowskim.goleb.pilecki acute mucosal reactions in patients with head and neck cancer . 
treatment of 87 head and neck cancer patients comprised either conventional fractionation ( cf ; n = 33 ) , accelerated fractionation ( af ; n = 33 ) , hyperfractionated ( hpefx ; n = 12 ) or hypofractionated ( hpofx ; n = 9 ) radiotherapy with radical intent . 
based on the three different shapes of amrr course curve observed during radiotherapy , three types of amrr course can be described : ( 1 ) a continual increase in amrr intensity until the completion of radiotherapy ; ( 2 ) the incidence of a plateau phase following the increase in amrr ( increaseplateau course ) and ( 3 ) decreasing amrr intensity with a healing phase . 
a further group of patients exists in whom signs of amrr healing are observed during the final stages of radiotherapy . keywords dose fractionation toxicity mucositis erythema healing akute schleimhautreaktion bei patienten mit kopf - hals - tumoren . 
die beurteilung des individuellen verlaufs einer akuten schleimhutreaktion nach der strahlentherapie ( acute mucosal radiation reactions , amrr ) bei patienten mit einer tumorerkrankung im kopfund halsbereich , die nur mit einer strahlentherapie behandelt wurden . 
die behandlung von 87 patienten mit einem tumor im kopf und halsbereich bestand entweder aus einer konventionellen ( cf ; n = 33 ) , einer beschleunigten ( af ; n = 33 ) , einer hyperfraktionierten ( hpefx ; n = 12 ) oder einer hypofraktionierten ( hpofx ; n = 9 ) strahlentherapie . 
die plateauphase wurde bei den meisten der mit cf und af behandelten patienten , bei fast der hlfte der mit der hpofx - methode und bei allen mit der hpefx - methode behandelten patienten festgestellt . 
es ist eine gruppe von bestrahlten patienten vorhanden , bei der man die heilungsmerkmale der akuten schleimhautreaktion bereits whrend der strahlenbehandlung in ihrer endphase diagnostizieren kann . schlsselwrter dosisfraktionierung toxizitt mukositis erythem heilung 9 / 33 ( 27% ) af patients , most frequently during the last week of irradiation . 
 discussion the presented study shows that individual amrr courses over the radiation and post - radiation periods can be grouped into three different patterns that generally reflect the intensity of dose - accumulation during radiation therapy . 
in about a quarter of patients irrastrahlentherapieundonkologie72013 | original article type 1 mean standard deviation 11 16 21 26 31 36 41 46 51 56 61 66 71 days type 2 mean standard deviation 11 16 21 26 31 36 41 46 51 56 61 66 71 days type 3 mean standard deviation the depopulation and exfoliation processes until radiotherapy is complete . the most frequently observed course of amrr was characterized by the existence of a stabilization of acute reactions occurring after the increase phase . 
 the fletcher data suggest that repopulation of mucosal cells can compensate for the effect of approximately 1.8 gy per day toward the end of a 6 - week course of radiation therapy [ 3 ]  . 
although the daily dose per fraction was 2.5 gy in the latter patientswith an accumulated dose per week equal to 12.5 gytarget volume was relatively small as a result of applying this regimen only to patients with early / moderately advanced ( t2n0 ) larynx cancer . 
it is possible that patients of this group had a better recovery potential . duration of the plateau phase was longest in hpefx treatments as result of its early onset and the longest treatment times . 
in some patients , a wavelike pattern may be observed as a consequence of short - lasting changes ( routinely 12 points according to the dische scoring system ) in amrr intensity during treatment . 
however , this does not have an impact on the overall shape of the plateau phase . in some patients treated with cf ( 11 ) and af ( 9 ) regimens , a tendency toward mucosal healing during radiotherapy occurred . 
depicted as a graphical curve based on modified dische scores : type 1 : continual increase of amrr intensity up until the end of radiotherapy ; type 2 : increaseplateau pattern ; type 3 : decreasing intensity with healing phase observed after the plateau phase . 
dashed blue lines shortest and longest time to radiotherapy completion 11 16 21 26 31 36 41 46 51 56 61 66 71 days diated with cf , hpofx and af , amrr curves continually rise after the latency period has elapsed until the end of radiotherapy ( in 2 patients , amrr intensity even continued to increase for a further 23 days )  . 
osullivan jm , hollywood dp , cody n et al ( 2002 ) accelerated radiation therapy , seven fractions per week , for advanced head and neck cancera feasibility study . 
overgaard j , hansen hs , specht et al ( 2003 ) five compared with six fractions per week of conventional radiotherapy of squamous - cell carcinoma of head and neck : dahanca 6 and 7 randomised controlled trial . 
quinn b , potting cmj , stone r et al ( 2008 ) guidelines for the assessment of oral mucositis in adult chemotherapy , radiotherapy and haematopoietic stem cell transplant patients . 
skladowski k , maciejewski b , golen m et al ( 2006 ) continuous accelerated 7 - days - a - week radiotherapy for head - and - neck cancer : long - term results of phase iii clinical trial . 
trotti a , klotch d , endicott j et al ( 1993 ) a prospective trial of accelerated radiotherapy in the postoperative treatment of high - risk squamous cell carcinoma of the head and neck . 
trotti a , bellm la , epstein jb et al ( 2003 ) mucositis incidence , severity and associated outcomes in patients with head and neck cancer receiving radiotherapy with or without chemotherapy : a systematic literature review . 
wolff ha , bosch j , jung k et al ( 2010 ) high - grade acute organ toxicity as positive prognostic factor in primary radio ( chemo ) therapy for locally advanced , inoperable head and neck cancer . 
wygoda a , maciejewski b , skladowski k et al ( 2009 ) pattern analysis of acute mucosal reactions in patients with head and neck cancer treated with conventional and accelerated irradiation . 
these patients may represent a group of individuals with an outstanding potential for early wound healing and tissue recovery . mucosal healing during radiotherapy was not observed in patients treated with hpefx . 
this regimen is routinely used for locally advanced head and neck cancer with metastatic neck nodes , particularly when there are medical contraindications to chemotherapy combined with radiotherapy [ 5 ]  . 
in 2005 and 2006 , the brachytherapy group of the european society for radiotherapy and oncology ( gec - estro ) published recommendations that aimed at supporting developments in this field by providing advanced concepts for structure definition and dosimetry [ 13 , 25 ]  . 
the main focus of recent research was based on the hypothesis that integrating three - dimensional imaging will improve local control rates and reduce morbidity [ 3 , 14 , 15 , 23 , 26 , 27 , 32 ]  . 
evaluation of dosevolume histogram ( dvh ) parameters for the high - risk clinical target volume ( hr - ctv ) ; the grey zones defined as a mixture of residual tumor , edema , fibrosis and gross target volume ( gtv ) and the organs at risk ( oar ) e.g. 
 prospective clinical trials demonstrated that systematic application of image - guided adaptive brachytherapy ( igabt ) was associated with significant improvements in local control , while the rates of adverse side effects remained low [ 8 , 9 , 10 , 11 , 18 , 26 , 27 ] and showed a significant dose dependence [ 5 , 6 , 9 , 10 ]  . late treatment - associated morbidity is one of the major concerns in curative radiotherapy . 
this is primarily because of the clinical aspects , but also due to its significant impact on the quality of life ( qol ) of cancer survivors [ 1 , 17 , 18 ]  . 
actuarial incidence rates assessed by the kaplanmeier method describe the risk of developing a defined maximum grade side effect at least once within a certain time period in a patient population . 
the percentage of patients suffering from late side effects at certain time points . patients and methods patients and treatment between 1998 and 2008 , 225 patients with cervical carcinomas in international federation of gynecology and obstetrics ( figo ) stages ibiva were included in the study . 
contraindications were renal failure , abnormal blood counts , poor medical condition ( karnofsky performace score < 60 ) and age exceeding 80 years . ebrt was performed with a four - field box technique or intensity - modulated radiation therapy ( imrt ) to administer 45 gy in 25 fractions to patients receiving concomitant chemotherapy , and 50.4 gy in 28 fractions to patients without chemotherapy . 
1 summary of late side effects in rectum and urinary bladder after mri - guided adaptive radiotherapy in 225 cervical cancer patients ( crude incidences ) original article latesideeffect rectum bleeding tenesmus / urgency sphincter control / incontinence stool frequency ulceration / fistulae bladder incontinence frequency hematuria dysuria decreased stream residual volume number ( % ) ofpatients grade1 10 ( 4.4 ) grade2 14 ( 6.2 ) grade3 4 ( 1.8 ) 22 ( 9.8 ) 20 ( 8.9 ) 5 ( 2.2 ) grade4 3 ( 1.3 ) 2 ( 0.9 ) total 31 ( 13.8 ) 24 ( 10.7 ) 7 ( 3.1 ) 5 ( 2.2 ) 4 ( 1.8 ) 3 ( 1.3 ) 49 ( 21.8 ) 31 ( 13.8 ) 15 ( 6.7 ) 7 ( 3.1 ) 2 ( 0.9 ) 2 ( 0.9 ) 1 ( 0.4 ) in all patients , mri - guided high doserate ( hdr ) brachytherapyintracavitary or combined intracavitary / interstitial with a planning aim of an equivalent dose in 2 gy fractions at / = 10 ( eqd210 gy ) of 85 gy to 90% ( d90 ) of the hr - ctv was applied in 4 fractions , as described previously [ 19 , 20 , 21 ]  . 
the study was approved by the local ethics committee . the total dose to oars was converted to eqd2 with an / - value of 3 gy ( eqd23 gy ) using the linear - quadratic model [ 21 ]  . 
dose constraints ( mean dose to the most irradiated x cm3 , dx cc ) were set at 75 gy to d2 cc for rectum and 100 gy to d2 cc for bladder . 
after 5 years , follow - up examinations were performed once a year . clinical scoring late side effects were assessed prospectively according to the late effects in normal tissuesubjective , objective , management and analytic ( lent / soma ) scale [ 22 , 24 , 28 , 29 ]  . 
the overall score ( 1 4 ) for each organ was defined by the maximum score of any specific side effect . statistical analysis descriptive statistics were performed using ms excel ( microsoft excel 2002 ; microsoft corp . , redmond , wa )  . 
tab.2. rectum mean d2 cc , d1 cc and d0.1 cc valuesdefined as the minimum dose to the maximally exposed 2 , 1 and 0.1 cm3 of tissue were 6511 , 6913 and 8233 gy , respectively . 
the latter 3 patients required colostomy surgery ( grade 4 ) and the side effects were scored as persistent , since the patients are permanent impaired . mean time to onset of side effects was 148.5 months ( range 334 months ) , while the mean duration was 1917 months ( range 175 months )  . 
 again , these side effects were scored as permanent . mean time to onset was 2721 months ( range 394 months ) and mean duration was 2017 months ( range 162 months )  . 
 in 76% ( 38 / 49 ) of cases , bladder side effects were seen within 3 years after comabstract zusammenfassung strahlenther onkol 2013 189 : 535540 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0365 - 7 p.georga.bonia.ghabuousg.goldnerm.p.schmidd.georgr.ptterw.drr time course of late rectaland urinary bladder side effects after mri - guided adaptive brachytherapy for cervical cancer abstract backgroundandpurpose . 
 side effects ( grade 14 ) in rectum and bladder were present in 31 and 49 patients , 14 and 27 months ( mean time to onset ) after treatment , respectively . 
 the combined presentation of incidenceand prevalence rates provides the most comprehensive information . keywords radiotherapy organs at risk quality of life intensity - modulated radiation therapy toxicity verlauf von sptnebenwirkungen am rektum und an der harnblase nach mri - gesttzter brachytherapie des zervixkarzinoms zusammenfassung hintergrundundziel . 
over the last years , associated topics like the severity of late side effects have rapidly gained attention in clinical research [ 2 , 4 , 11 , 16 , 17 , 30 ]  . the frequency of late side effects is usually represented by actuarial incidence rates . 
therefore , the risk of developing a certain late side effect at a specific time point is an important consideration . the present study clearly demonstrates that late side effects in the rectum and urinary bladder after cervical cancer radiotherapy are partially reversible and hence transient in nature . 
consequently , the prevalence rate was highest 2 years after completion of treatment and had markedly decreased by follow - up year 5 . in contrast , bladder complications continued to develop over a longer time period . 
 strahlentherapieundonkologie72013 | original article incidence rate prevalence rate months after radiotherapy patients at risk ( n ) : events n ( % ) : 12 ( 6% ) 16 ( 11% ) 12 ( 9% ) 6 ( 6% ) 2 ( 2% ) fig . 
the actuarial incidence rates were 16% at 3 years and 19% at 5 years ; the corresponding prevalence rates were 9 and 2% , respectively incidence rate prevalence rate months after radiotherapy patients at risk ( n ) : events n ( % ) : 10 ( 5% ) 18 ( 12% ) 23 ( 18% ) 22 ( 21% ) 18 ( 21% ) fig . 
the 3and 5 - year actuarial incidence rates were 18 and 28% ; the prevalence rates were 18 and 21% , respectively 538 | strahlentherapieundonkologie72013 this can be explained by their later onset and prolonged healing times compared to the rectal side effects , which leads to a correspondingly larger variation in date of onset and side effect duration . 
additionally , the number of patients with a 5 - year follow - up time is limited . improvements in late toxicity rates with longer follow - up times have also been described for other oars . 
for example , in patients treated for head and neck cancer , improved parotid gland recovery ( in terms of salivary flow ) was reported [ 33 ]  . similar differences in the time course of major rectal and urinary tract complications were reported by eiffel et al . 
the highest risk for manifestation of rectal side effects existed during the first 2 years of follow - up , with a subsequent continuous risk of 0.06% per year between years 2 and 20 . 
the actuarial major urinary complication rates were 16% at 3 and almost 26% at 5 years , while for rectum the corresponding rates remained stable at 22% at both 3 and 5 years [ 7 ]  . haie - meder et al . 
 while incidence rates of the first complication ( all organs ) increased up to 70% after 3 years , prevalence rates increased up to only 45% during the first year after treatment and decreased to 30% at 4 years [ 12 ]  . the importance of reporting both prevalence and actuarial incidence rates of late side effects was also demonstrated for prostate cancer patients undergoing radiotherapy [ 30 ]  . 
possible explanations for this might include differences in dose and dose distributions within the bladder and urethra , as well as differences in bladder anatomy / physiology between males and females ( such as sphincter function ) and their differential impact on individual endpoints categorized as adverse genitourinary effects of a certain grade . however , our results are in general agreement with the time course of patient - reported late toxicity following pelvic radiotherapy for gynecological cancer . 
for any prospective assessment of morbidity in clinical studies , it is of utmost importance that patient - reported symptoms be integrated into the scoring system [ 17 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literatur kommentiert strahlenther onkol 2013 189 : 592593 doi 10.1007 / s00066 - 013 - 0364 - 8 online publiziert : 29 . 
mai 2013 springer - verlag berlin heidelberg 2013 i.ernsth.t.eich klinik fr strahlentherapie & radioonkologie , universittsklinikum , mnster zns - bestrahlungbei kindernmitakuter myeloischerleukmie keinnachteildurchdosisreduktion von18auf12gy originalbeitrag creutzig u , zimmermann m , bourquin jp et al ( 2011 ) cns irradiation in pediatric acute myeloid leukemia : equal results by 12 or 18 gy in studies aml - bfm98 and 2004 . 
der stellenwert einer prophylaktischen zns - bestrahlung ( zns - rt ) als bestandteil der therapie fr kinder mit akuter myeloischer leukmie ist unbestritten [ 2 ] , wird aber bei akuter myeloischer leukmie ( aml ) kontrovers diskutiert . 
seit die deutsche studie aml - bfm 87 jedoch einen vorteil hinsichtlich der zns - rezidive im rt - arm aufwies [ 3 ] , ist die bestrahlung auch hier bestandteil der folgestudien . 
die analyse basiert auf 471 patienten ( von 1206 der gesamten studienpopulation ) im alter zwischen 0 und 18 jahren , welche nach erstdiagnose einer aml zwischen juli 1998 und april 2009 in den aml - bfm - 98 , - 98 - interimund - 2004 - studien prophylaktisch mit 18 gy ( n = 219 ) oder 12 gy ( n = 252 ) zns - bestrahlt wurden . 
rezidive traten bei insgesamt 145 kindern auf , wobei 6 im zns lagen ( 5 - mal in der 18 - gy - gruppe , 1 - mal in der 12 - gy - gruppe . ) bei 4 dieser rezidive war das knochenmark beteiligt ( blasten )  . 
in den folgestudien der amlbfm - studiengruppe soll nun der stellenwert einer intensivierten chemotherapie als ersatz fr eine prophylaktische hirnbestrahlung geprft werden . kommentar die aml - bfm - 87 - studie ist die einzige prospektive studie , die den stellenwert einer prophylaktischen hirnbestrahlung evaluierte und mit den nachfolgestudien die mglichkeit zeigte , die dosis fr die schdelbestrahlung von 18 auf 12 gy zu senken , um spttoxizitt zu vermindern bei sonst gleichbleibender effektivitt [ 3 , bei allen multimodalen therapieregimen ist es schwer , einzelne nebenwir592 | strahlentherapieundonkologie72013 18auf12gybeivorliegeneineramlim kindesaltererbringtkeinennachteilbezglichberleben , progressionsfreiem berlebenundrezidivhufigkeit.hingegenscheintdieneurotoxizittgeringerzusein.allerdingssindpatientenzahl undnachbeobachtungszeitnochzugering , umabschlieendeempfehlungen gebenzuknnen.aufjedenfallbesteht deshalbderzeitkeingrund , aufdieprophylaktischezns - bestrahlungzugunsteneinerintensiviertenundvermutlich toxischerenchemotherapieganzzuverzichten . iris ernst und hans theodor eich , mnster korrespondenzadresse h.t. 
abbott bl , rubnitz je , tong x et al ( 2003 ) clinical significance of central nervous system involvement at diagnosis of pediatric acute myeloid leukemia : a single institutions experience . 
creutzig u , ritter j , zimmermann m et al ( 1993 ) does cranial irradiation reduce the risk for bone marrow relapse in acute myelogenous leukemia ? unexpected results of the childhood acute myelogenous leukemia study bfm - 87 . 
creutzig u , zimmermann m , bourquin jp et al ( 2011 ) cns irradiation in pediatric acute myeloid leukemia : equal results by 12 or 18 gy in studies aml - bfm98 and 2004 . 
dongen - melman je , de groot a , dongen jj van et al ( 1997 ) cranial irradiation ist he major cause of learning problems in children treated for leukemia and lymphoma : a comparative study . 
eine prophylaktische zns - bestrahlung von kindern mit leukmie verursacht hufig psychosoziale strungen , obwohl auch bei langzeitig berlebenden kindern mit unterschiedlichsten tumoren nach einer therapie mit alkylantien ebenfalls psychosoziale probleme auftreten , und zwar unabhngig von der art des primrtumors [ 7 ]  . 
betrachtet man diejenigen kinder mit leukmie , die mit chemotherapie und hirnbestrahlung behandelt wurden , ist die rate dieser nebenwirkung hher [ 7 ]  . neurokognitive oder endokrinologische funktionsstrungen sowie skelettanomalien treten nach zns - bestrahlung dosisund volumenabhngig auf [ 5 ]  . 
jude childrens research hospital ber kein znsrezidiv bei 131 patienten [ 1 ]  . fazit dieerniedrigungderdosisbeiderprophylaktischenschdelbestrahlungvon strahlentherapieundonkologie72013 | original article strahlenther onkol 2013 189 : 566572 doi 10.1007 / s00066 - 013 - 0330 - 5 received : 30 july 2012 accepted : 6 february 2013 published online : 30 may 2013 springer - verlag berlin heidelberg 2013 y.dzierma1f.g.nuesken2n.p.licht2c.ruebe2 1 klinik fr strahlentherapie und radioonkologie , universittsklinikum des saarlandes , homburg / saar 2 department for radiotherapy , saarland university medical centre , homburg / saar dosimetricproperties andcommissioningof cone - beamctimagebeam linewithacarbontarget the precision attainable with state - of - the art radiotherapy techniques such as intensity - modulated radiotherapy ( imrt ) and linear accelerator ( linac ) - based radiosurgery requires exact positioning of the patient before and during radiation delivery . 
electronic portal images are increasingly complemented by more advanced techniques offering three - dimensional imaging , most commonly conebeam computed tomography ( cbct , see [ 4 , 26 ] for a review )  . 
the most elegant solution is kv imaging [ 2 , 7 , 15 , 16 , 25 ] , which provides good image quality and soft tissue contrast with a low applied dose that need not be included in the treatment plan ( although it is documented for each image )  . 
the problems of reduced contrast and high imaging dose can be overcome to some degree by lowering the photon energy in a secondary imaging beam line ( ibl ) with a flattening filter - free beam incident on a carbon target ( e.g. , [ 5 , 6 , 21 , 22 , 23 , 24 ] )  . 
this approach enhances soft tissue contrast for the same applied doseor conversely , produces similar contrast at a reduced dose to the patient [ 3 , 9 , 10 , 11 ]  . 
previous studies have investigated the properties of cbct image acquisition systems with regard to both dosimetry and image quality [ 1 , 3 , 4 , 9 , 10 , 11 , 12 , 14 , 17 , 18 , 19 , 20 , 27 ]  . 
this requires consideration of the effects of the imaging dose on the treatment plan , which can be most simply and accurately performed by calculating the imaging dose after commissioning of the ibl in the tps . 
in addition to the technical perspective , we present examples to illustrate the effects of the imaging dose and its inclusion into the treatment plan . materials and methods the siemens artiste installed at our institution can be operated with a treatment beam comprising 6 - mv photons or a flattening filter - free 7 - mv photon beathe ibl with a flattening filter - free beam is incident on a carbon target . 
the nominal energy of this beam line is 1 mv ; the acceleration energy of the electrons is 4.2 mev , as described in the literature [ 9 ]  . 
imaging is performed with an amorphous silicon flat panel detector , similar to standard cbct ( siemens mvision )  . all measurements ( except surface dose ) were acquired in a ptw mp3 water phantom ( ptw , freiburg , germany ) at a source - to - surface distance of 100 cpercent depth dose curves with a 1 - mm step size were generated using measurements made in an pinpoint ionisation chamber ( ptw 31016 )  . 
to exclude field - edge effects , only the inner 90% of the field opening was included in the analysis cross - plane symmetry [ % ] fieldsize [ cm2 ] 1010 2020 2525 in - plane symmetry 566 | strahlentherapieundonkologie72013 depth [ mm ] depth ( mm ) pinpoint chamber in water phantom soft x - ray chamber in acrylic phantom ( depth scaled to water depth ) fig . 
lines display the model fit to the measurements made by the pinnacle3 treatment planning systeb percent depth dose curve measured by the soft x - ray plane parallel ionisation chamber ( black ) , compared to the pinpoint measurements ( green )  . 
the measurements of the soft x - ray chamber were carried out in an acrylic phantom and scaled to water depth 5x5 cm2 data 10x10 cm2 data 20x20 cm2 data model model model 180 150 120 90 in - plane distance from axis [ mm ] cross - plane distance from axis [ mm ] 60 30 120 150 180 180 150 120 90 60 30 90 120 150 180 fig . 
2 8 in - plane profiles ( a ) and cross - plane profiles ( b ) for 55 ( black ) , 1010 ( red ) , 2020 ( green ) and 2525 cm2 ( blue ) field sizes , with error bars corresponding to three standard deviations . 
lines display the model fit to the measurements by the pinnacle3 treatment planning systewhile the modelling is performed on the symmetrised profiles , the dots show the original measurements before symmetrisation sation chamber ( ptw 31010 ) for field sizes of 1010 cm2 and larger , and with a pinpoint chamber ( ptw 31016 ) for smaller fields . 
for the output factors , the reference 1010 cm2 field was measured at the beginning and at the end of the series , as well as several times in between to correct for possible drithe absolute dose output for the 1010 cm2 field was obtained by including the pressuretemperature - , qualityand radius correction factors . 
measurements were taken over a period of 3 months , with a number of repeat measurements to assess the stability of the beam characteristics ( with each profile measured a total of ten times on two successive days in august , and on one day in september and october 2011 )  . 
we therefore performed these measurements using a ptw plane parallel soft x - ray ionisation chamber ( type 23342 ) in an acrylic phantofor each depth step , the table was lowered by 1 mm and 1 mm acrylic was added on top of the phantom . for commissioning , the measurements were averaged and beam profiles symmetrised in the mephysto software ( ptw ) before import into the philips pinnacle3 tps version 9.0. 
the automatic modelling algorithm was run using the arbitrary beam profile modality . dosimetric verification was performed with a semiflex ionisation chamber ( ptw 31013 ) and thermo lif thermoluminescent dosimeters ( tlds ; tldstrahlentherapieundonkologie72013 | original article abstract zusammenfassung 100 read with a harshaw tld system 4000 ; thermo scientific , waltham , ma , usa ) in an acrylic phantom routinely employed at our institution for the verification of imrt plans , i.e. 
brainlab phantom ( brainlab ag , feldkirchen , germany ) aligned at the isocentre ; source - toisocentre distance 100 cthe standard pass criterion for the point dose measurements is less than 5% dose deviation . 
to check the planar dose distribution , measurements were taken on gafchromic ebt2 film ( ashland inc . , covington , ky , usa ) in the central plane of the brainlab phantom , scanned with 12 bits per pixel at a resolution of 0.08 mm by a vidar dosimetry pro advantage ( red ) scanner ( vidar systems corporation , herndon , va , usa ) and compared to the tps dose in the ptw verisoft software version 5.1. results beam properties the percent depth dose ( pdd ) curves calculated for different field sizes are displayed in .fig.1 ( compare [ 11 ] )  . 
the dose maximum is reached at a depth of 10 mm ; the 50% dose value is reached at a depth between 100 ( 55 cm2 field ) and 125 mm ( 2020 cm2 field )  . 
due to the soft energy spectrum , most of the dose is deposited at shallow depths , with a percent surface dose of 44% ( measured by the soft x - ray chamber for the 1010 cm2 field )  . 
 the standard deviation for a number of measurements repeated on the same day is below a 1% maximu for measurements spaced 1 month apart , the deviation between the pdd curves is less than three standard deviations and the distance - toagreement is below 1 mm . a flattening filter reduces the relative amount of low - energy photons , effectively hardening the beatherefore , the ibl works in the flattening filter - free mode , resulting in the characteristic coneshaped beam profiles ( .fig.2 , compare [ 11 ] )  . 
for three successive measurements , the standard deviations are below 1.5% for all field sizes and measurement depths ; the average values are between 0.2 and 1% ( increasing with field size and measurement depth )  . 
measurements repeated after 1 month yield profiles that agree with568 | strahlentherapieundonkologie72013 strahlenther onkol 2013 189 : 566572 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0330 - 5 y.dziermaf.g.nueskenn.p.lichtc.ruebe dosimetric properties and commissioning of cone - beam ct image beam line with a carbon target abstract backgroundandpurpose . 
even if the absolute dose deposited is small , repeated imaging doses may sum up to significant amounts and can shift the position of the dose maximum by several centimetres . keywords intensity - modulated radiation therapy dose distribution organs at risk imaging radiosurgery dosimetrische eigenschaften und kommissionierung der image - beam - line - cone - beam - ct mit einem kohlenstofftarget zusammenfassung hintergrundundziel . 
der absolutbetrag der dosis eines cbct ist klebei hufiger bildgebung kann die akkumulierte dosis signifikant werden und zu einer deutlichen verschiebung des dosismaximums fhren . schlsselwrter intensittsmodulierte strahlentherapie dosisverteilung risikoorgane bildgebung radiochirurgie in less than three standard deviations ; only at the edges of the field do some points deviate by more than this . 
 the difference between two linearly driftcorrected measurements for any field size is less than 1.3 mgy , which corresponds to 0.2%. 1 , 20 1 , 15 1 , 10 1 , 05 1 , 00 0 , 95 0 , 90 0 , 85 0 , 80 starting conditions for spectrum mohan 4 mv spectrum mohan 6 mv spectrum constant spectrum up to 4 mev field width [ cm ] photon energy [ mev ] fig . 
4 8 spectrum inverted from the depth dose curves by the treatment planning systethe red curve was inverted starting from a mohan 4 mv [ 18 ] spectruthe green curve was inverted starting from a mohan 6 mv [ 18 ] spectruthe black curve used a constant fluence of 0.1 for energies up to 4 mev , with a linear decrease to zero between 4 and 5 mev as a starting value for the iteration . 
the most probable photon energy ( corresponding to the maximum of the photon fluence curve ) is 0.4 mev ; the maximum of the energy fluence curve is at 0.8 mev modelling in the tps modelling of the ibl was performed with the pinnacle3 automatic modelling routine . 
this routine automatically optimises the photon model parameters , including electron contamination , spectrum , focal spot size , jaw and multileaf collimator ( mlc ) transmission as well as fluence profiles in a sequence of steps . 
some differences may arise upon use in other tpss , but we believe that the main points pertaining to selection of the starting spectrum and beam profile should also be kept in mind for other tpss and may give a useful outline of the process . in the automatic modelling routine , it is necessary to select the arbitrary beam profiles option , which allows the system to match any beam shape rather than only flat profiles . 
to assess the stability of the inversion in relation to the starting spectrum , we carried out several modelling sequences with a variety of starting spectra to compare the resulting model spectra . 
if higher energies are admitted ( using a mohan 6 mv spectrum [ 18 ] as a starting point for the inversion ) , the high - energy tail is modelled more smoothly , with hardly any difference at lower energies ( up to about 3 mev )  . 
we adopt the inversion run based on the mohan 6 mv spectrum for the commissioning of the machine , since both the inputand output spectra for this situation are the most realistic . 
the average energy is approximately 1 mev , which is the nominal energy for the ibl given by siemens . the percent depth dose ( .fig.1a ) curves are modelled adequately ; the maximum mismatch between the model and the measurements is 1.4% or 1 mm distance - to - agreement . 
however , slight discrepancies of over 5% dose deviation at the edge of the field and in the out - offield dose remain , which can be adjusted manually to improve the fit . 
in particular , we adjusted the width and height of the gaussian used to model the field edges and collimator and mlc transmission for the out - of - field dose of crossand inplane profiles . 
the large - field profiles closest to the surface ( taken at the dose maximum depth of 10 mm ) show the largest divergence in the out - of - field part of the profiles , which are systematically overestimated in the model . 
if the fit of the out - of - field portion of these shallow profiles is improved by manually adjusting the gaussian and transmission parameters , the fit for the deeper profiles declines . 
of the points , 88% pass the gamma criterion ( 5% dose deviation and 3 mm distance - to - agreement ) ; the failing points inside the open field are mostly caused by a small inclination of the phantom fig . 
 we display the slice where the dose maximum of the 200 - degree arc ibl occurs to accept the slight disagreement in outof - field doses for the near - surface profiles in favour of a better fit at greater depths . 
for each patient , the starting angle of the 200 - degree arc can be chosen so as to shift the maximum dose position according to patient anatomy and organs at risk . 
from left to right : ( i ) treatment plan only ( 22 fractions of 180 cgy ) , ( ii ) treatment plan with real imaging scenario ( treatment as in a ; positioning verification with 7 mu at 360 before the first treatment and with 7 mu at 200 twice weekly thereafter ) , ( iii ) treatment plan with extreme case of imaging ( 8 mu at 360 prior to each fraction )  . 
the isodoses with respect to the reference point do not vary markedly between the three scenarios , however , the dose at the reference point and hence the absolute isodose level is increased from 39.5 gy ( treatment only ) to 40.3 gy ( maximum cbct dose )  . 
compensation must also take dose fractionation into account , however , there will still be a detrimental effect on dose distribution , with an increased volume of tissue receiving medium / low doses . 
in the case of imrt , it has been pointed out that inversion should be performed with the fixed imaging dose included in the treatment setup [ 17 , 27 ] , which we agree is the preferable method for obtaining an optimised dose distribution . 
zabel - du bois a , nill s , ulrich s et al ( 2012 ) dosimetric integration of daily mega - voltage conebeam ct for image - guided intensity - modulated radiotherapy . 
many thanks to georg blass for his assistance with the tld measurements , to stephanie kremp for her help in printing out the pinnacle3 results and to achim elzer for providing technical details on the ibl and flat panel . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 594595 doi 10.1007 / s00066 - 013 - 0350 - 1 online publiziert : 9 . 
juni 2013 springer - verlag berlin heidelberg 2013 d.krug abteilung radioonkologie und strahlentherapie , universittsklinikum heidelberg prdiktorenfrein lokoregionresrezidivnach neoadjuvanterchemotherapie beimmammakarzinom ergebnissederkombiniertenanalyse vonnsabb - 18undb - 27 originalbeitrag mamounas ep , anderson sj , dignam jj et al ( 2012 ) predictors of locoregional recurrence after neoadjuvant chemotherapy : results of combined analysis from national surgical adjuvant breast and bowel project b - 18 and b - 27 . 
es wurde eine post - hoc - analyse von insgesamt 3088 mammakarzinompatientinnen , die im rahmen der nsabp - studien b - 18 und b - 27 in den studienarmen mit neoadjuvanter chemotherapie behandelt worden waren , durchgefhrt . 
in der b - 27 - studie gab es darber hinaus zwei weitere gruppen , in denen die patientinnen zustzlich auf eine neoadjuvante oder adjuvante gabe von 4 zyklen docetaxel randomisiert wurden . 
signifikante einflussfaktoren waren der klinische verdacht auf lymphknotenmetastasen vor beginn der neoadjuvanten therapie , das vorhandensein eines invasiven resttumors sowie von lymphknotenmetastasen zum zeitpunkt der operation , das alter ( insbesondere fr brusterhaltend behandelte patientinnen ) und eine tumorgre von > 5 cm ( insbesondere fr mastektomierte patientinnen )  . 
im falle einer pcr , definiert als ypt0 / yptis ypn0 , lag dieses in allen subgruppen zwischen 6 , 2 und 7 , 6% , bei patientinnen mit 13 lymphknotenmetastasen wiederum mit ausnahme der oben genannten niedrigrisikogruppe bei ber 10% . 
das therapieansprechen auf die neoadjuvante chemotherapie liefert wichtige informationen zum lokoregionren rezidivrisiko , die hilfreich zur indikation einer adjuvanten radiotherapie sein knnen . kommentar die adjuvante und neoadjuvante chemotherapeutische behandlung des mammakarzinoms sind bezglich des gesamtberlebens bei lokoregionr begrenzten erkrankungen gleichwertig [ 1 ]  . 
vorteile einer neoadjuvanten chemotherapie sind die mglichkeit zur in - vivo - chemosensitivittstestung , die identifizierung prognostischer faktoren zur individualisierung der therapie , die schnelle etablierung neuer medikamente und therapiekonzepte sowie eine hhere rate an brusterhaltenden operationen , die jedoch mit einer hheren rate an lokoregionren rezidiven vergesellschaftet ist [ 2 ]  . eine pathohistologisch komplette remission ( pcr ) tritt nach neoadjuvan594 | strahlentherapieundonkologie72013 4 . 
baselga j , bradbury i , eidtmann h et al ( 2012 ) lapatinib with trastuzumab for her2 - positive early breast cancer ( neoaltto ) : a randomised , open - label , multicentre , phase 3 trial . 
gianni l , pienkowski t , im yh et al ( 2012 ) efficacy and safety of neoadjuvant pertuzumab and trastuzumab in women with locally advanced , inflammatory , or early her2 - positive breast cancer ( neosphere ) : a randomised multicentre , open - label , phase 2 trial . 
minckwitz g von , untch m , blohmer ju et al ( 2012 ) definition and impact of pathologic complete response on prognosis after neoadjuvant chemotherapy in various intrinsic breast cancer subtypes . 
huang eh , tucker sl , strom ea et al ( 2004 ) postmastectomy radiation improves local - regional control and survival for selected patients with locally advanced breast cancer treated with neoadjuvant chemotherapy and mastectomy . 
mcguire se , gonzalez - angulo am , huang eh et al ( 2007 ) postmastectomy radiation improves the outcome of patients with locally advanced breast cancer who achieve a pathologic complete response to neoadjuvant chemotherapy . 
mamounas ep , anderson sj , dignam jj et al ( 2012 ) predictors of locoregional recurrence after neoadjuvant chemotherapy : results of combined analysis from national surgical adjuvant breast and bowel project b - 18 and b - 27 . 
15% aller patientinnen ein , wobei der anteil abhngig vom patientenalter , von der hormonrezeptorund her2 - expression , der anzahl an chemotherapiezyklen , der tumorgre , der histologie und des gradings deutlich variiert [ 3 ]  . 
hierbei spielt auch die zwischen den fachgesellschaften und studiengruppen variierende definition der pathologischen komplettremission eine nicht zu unterschtzende bedeutung : beispielsweise ist bereits das vorhandensein von nichtinvasiven tumorresiduen ( yptis ) mit einem signifikant schlechteren krankheitsfreien berleben vergesellschaftet [ 6 ]  . gem der aktuellen deutschen s3leitlinie zur diagnostik und therapie des mammakarzinoms richtet sich die indikation zur bestrahlung der thoraxwand und der lymphabflusswege in ermangelung prospektiver daten ausschlielich nach dem initialen tumorstadiudass die adjuvante thoraxwandbestrahlung nach mastektomie und die neoadjuvante chemotherapie in bestimmten subgruppen das lokalrezidivrisiko deutlich senken , wie auch das berleben verbessern knnen , wurde immer wieder gezeigt [ 8 , 9 ]  . 
der verzicht auf die bestrahlung der supraklavikulren lymphknoten resultierte in einer weiteren retrospektiven arbeit mit vermehrten lokalrezidiven [ 9 ]  . eine auf klinischen , histopathologischen und therapieassoziierten faktoren basierende risikoeinschtzung nach neoadjuvanter chemotherapie und mastektomie schlugen fowble et al . 
zusammenfassend weisen die nsabp - b - 18und - b - 27 - studien [ 11 ] das grte und bislang einzige prospektiv untersuchte patientenkollektiv zu dieser fragestellung auf und besitzen den vorteil einer in den protokollen definierten und indizierten strahlentherapie . leider fehlen in der publikation detaillierte informationen zur hormonrezeptorund her2 - expression . 
die publikation der german breast group [ 6 ] lsst jedoch vermuten , dass das erreichen einer pcr in den luminal - aund - b - subgruppen keine zustzlichen prognostischen informationen liefern wird . 
minckwitz g von , untch m , nesch e et al ( 2011 ) impact of treatment characteristics on response of different breast cancer phenotypes : pooled analysis of the german neo - adjuvant chemotherapy trials . 
breast cancer res treat 125 : 145156 strahlentherapieundonkologie72013 | mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 598599 doi 10.1007s00066 - 013 - 0380 - 8 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
20 , d - 65189 wiesbaden , e - mail : prott@bvdst.de personalia jrgen dunst , jahrgang 1958 , hat nach dem medizinstudium in kiel seine facharztausbildung an der universittsklinik erlangen absolviert und sich dort 1992 habilitiert . 
von 1994 bis 2005 war er der direktor der universitts - strahlenklinik an der martin - luther - universitt halle ; seit 2005 ist er professor fr strahlentherapie an der universitt zu lbeck und direktor der strahlenklinik . 
 professor jrgen dunst zum honorary professor for radiation oncology ernannt die medizinische fakultt der universitt kopenhagen hat jrgen dunst ( lbeck ) , beginnend ab dem 1.6.2013 ( befristet fr fnf jahre ) , als mitglied der fakultt aufgenommen . 
die strahlentherapie in naestved ist die nrdliche nachbarklinik der universitt lbeck mit einer sehr gut ausgersteten strahlentherapie ( 3 varian trilogy linacs mit cone beam ct )  . degro ehrenmitgliedschaften anlsslich der 19 . 
 jrgen dunst , bisher klinikdirektor in lbeck , leitet nach der emeritierung von bernhard kimmig jetzt beide kliniken in kiel und lbeck als direktor und arbeitet als chefarzt am campus kiel . 
 herr hollywood war seit 1994 , seit seiner rckkehr aus houston / texas , der mariecurie professor of radiation oncology des trintity college in dublin und director of radiation oncology am st . 
james klinikum in dublunter seiner fhrung wurde die bis dahin schwache und veraltete radioonkologie in irland zu einem modernen und anerkannten fach ausgebaut , welches sicherstellt , dass heute jedem irischen krebspatienten eine strahlentherapie auf internationalem niveau angeboten werden kann . 
sabine anna bucher aus freiburg fr die arbeit f - 18 - fluoromisonidazol - pet zur evaluation der hypoxie in kopf - hals - tumoren im verlauf einer primren radiochemotherapie . 
den mit 3000 dotierten koester - preis fr den besten vortrag der jahrestagung , gesponsort von der hans und hildegard koester - stiftung , erhielt constantin dreher aus heidelberg fr seinen vortrag biologisch - physikalische optimierung von bestrahlungsplnen zur kohlenstoffionen und protonentherapie mit aktivem rasterscanning von patienten mit nicht - resektablem pankreaskarzinom am heidelberger ionen strahlentherapie - zentrum ( hit ) die posterpreise gingen an elisa zienert , dresden ( opasca 500 , - ) , martin thiele , soest ( opasca 250 , - ) , juliane gabriele rieber , heidelberg ( opasca 250 , - ) , arndt - christian mller , tbingen ( takeda 500 , - ) und an sebastian kuger , wrzburg ( elekta 500 , - ) outstanding research award med . 
peter vaupel , seit 2008 professor fr tumor - pathophysiologie an der klinik und poliklinik fr radiotherapie und radiologische onkologie , klinikum rechts der isar der technischen universitt mnchen , ehemals andrew werk cook professor for radiation biology , tumor biology and physiology an der harvard medical school in boston und langjhriger lehrstuhlinhaber am institut fr physiologie und pathophysiologie an der johannes gutenberg - universitt in mainz , wurde im mai in miami ( usa ) whrend der 13 . 
therefore , an increasing number of childhood cancer survivors are at risk of developing permanent consequences of their oncological treatment during adolescence . the aim of the present retrospective investigation was to quantify the incidence of such treatment - related changes in growing tissues in a representative group of patients . 
moreover , the impact of age at treatment and the radiotherapy protocols and doses employed was analysed . patient cohort the study included 146 children treated in the haemato - oncological and radiotherapy departments of the klinikum chemnitz ggmbh , germany ( 28 patients ) or the university hospital dresden ( 118 cases ) during the period between 1970 and 1997 . the aim of the present study was to analyse local effects of radiotherapy . 
these treatment protocols were in accordance with the relevant inter - disciplinary paediatric - oncological therapeutic guidelines in force at the time . reconstruction of radiation doses in the organs at risk ( oar ; bone , soft tissue ) was based on the individual treatment plans . 
all oar doses were converted into equivalent doses delivered in 2 gy fractions , recalculated with an / - value of 3 gy ( eqd23 gy , [ 2 ] )  . 
in the results section , only the parameters that showed a significant effect or at least a trend are reported . pathological findings in the skeletal system and soft tissues were recorded in 75 / 146 patients ( 51% )  . 
the individual symptoms are summarized in .tab.2. effects of age at exposure and dose most pathological findings were reported for patients treated under the age of 6 years ( .fig.1 ) , where substantial changes were seen with low radiation doses . 
 in the group with substantial changes , mean age at exposure and dose ( eqd2 ) were 4.43.6 years and 309 gy ( mean standard deviation ) , respectively ; in the group with minor changes the values were 7.54.7 years and 3711 gy , respectively and in the group without changes they were 11.54.1 years and 4011 gy , respectively . for kyphoscoliosis , a significant inverse dependence on age at exposure was found , while there was only a trend for isolated kyphosis . 
for gradients < 35 gy , a significant dose - dependence ( grade 1 , p = 0.0071 ; grade 2 , p = 0.0350 ) was observed in children aged 6 years or younger at treatment , but not in the other age groups . 
however , the systematic evaluation , documentation and continuous analysis of adverse events in paediatric oncology remains essential , as does the evaluation of novel radio ( chemo ) therapeutic approaches . keywords kyphoscoliosis growth retardation hypoplasia sarcoma scoliosis folgen der strahlentherapie im kindesalter an knochen und bindegewebe . 
die mehrzahl der pathologischen vernderungen traten bei kindern nach behandlung mit einem alter < 6 jahren auf , bei patienten 6 jahren nur nach dosen von > 35 gy ; bei patienten > 12 jahren fanden sich keine erheblichen vernderungen . 
 dennoch bleiben eine systematische erfassung , dokumentation und fortwhrende analyse aller unerwnschten ereignisse in der pdiatrischen onkologie essentiell und unumgng lich , um auch neuartige radio ( chemo ) therapeutische therapieanstze zu beurteilen . schlsselwrter kyphoskoliose wachstumsverzgerung hypoplasie sarkom skoliosen ly . 
the present study was therefore initiated to retrospectively assess these dependencies in a group of 146 children treated between the ages of 2 months and 17 years for various childhood malignancies . 
although the treatment techniques in this group ( treated between 1970 and 1997 according to the up - to - date guidelines of the time ) may not represent the current standards , the dependence of the various normal tissue endpoints on local radiation dose is still representative and valid for modern radio ( chemo ) therapy protocols . the effect of additional chemotherapy was not evaluated due to the highly dynamic changes in chemotherapy protocols during the period over which the pastrahlentherapieundonkologie72013 | original article age at treatment [ years ] vertebral body dose gradient [ eqd23 gy gy ] minor changes substantial changes grade 1 + grade 2 fig . 
the radiation dose was converted into the equivalent dose administered at 2 gy per fraction , with an / value of 3 gy ( eqd23 gy , [ 2 ] )  . 
at a treatment age > 6 years , substantial changes were found only after doses > 35 gy and no changes were seen in the > 12 years age group fig . 
the dose gradient - effect curves were generated for children with an age of 6 years at treatment , with a dose gradient within the vertebral body of 35 gy eqd23 gy . 
data points represent the incidence for groups of patients in the illustrated dose range ( mean standard deviation ) ; logit analyses were based on events in individual patients the results of the present study on the treatment of childhood malignancies with radio ( chemo ) therapy and their relationship to information in the literature are summarised below : 1 . 
 [ 16 ] , who noted a stringent correlation between radiation dose and severe scoliotic changes in 81 patients with wilms tumour : the incidence was > 25% for doses > 30 gy , while no changes were seen 90 100 110 120 local eqd23 gy bone [ gy ] fig . 
data points represent the incidence for groups of patients in the illustrated dose range ( mean standard deviation ) ; logit analysis was performed on the basis of the events in the individual patients tients were treated and thereafter . 
moreover , direct effects of chemotherapy on normal tissue growth result in symmetrical changes and are hence undistinguishable from indirect effects via , for example , hormonal impairment . all children reached a height of at least 90% of the age - adjusted norm values . 
furthermore , no gender differences could be identified in the current analysis , as in agreement with donaldson [ 7 ] , but in contrast to wilimas [ 19 ]  . 
data points represent the incidence for groups of patients in the illustrated dose range ( mean standard deviation ) ; logit analyses were based on events in individual patients local eqd23 gy soft tissue [ gy ] 90 100 110 120 < 26 gy . 
 dose gradients in vertebral bodies : kyphoscoliotic changes result from inhomogeneous dose distributions within the vertebral bodies ( .fig.2 ) , particularly in children aged 6 years or younger at the time of treatment . 
 follow up : all patients in the present study were followed until the end of their growth phase ; hence , no additional cases of scoliosis or growth impairment can be expected . 
for shorter follow - up intervals , this factor needs to be taken into consideration [ 17 ]  . conclusion and practical recommendations the present results indicate that tolerance doses for growing bone of 20 gy [ 5 , 10 ] need to be respected , particularly in children under 6 years of age at the time of treatment . 
however , this does not apply to discrete symmetrical growth impairments of the vertebrae with a consequent minor reduction in body height . the present study included patients treated in two large departments over a period of 27 years . 
however , this fact must not have an impact on the systematic evaluation , documentation and continuous analysis of any treatmentinduced normal tissue effects in paediatric oncology patients , or on the comprehensive assessment of effects of existing and novel chemotherapeutic approaches . 
the authors are grateful to klinikum chemnitz ggmbh , germany ( department of paediatric and adolescent medicine , former director albrecht klinghammer ) and the university hospital dresden , germany ( department of paediatric medicine , former director manfred gahr ) , which represent the two major regional paediatric departments . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . strahlentherapieundonkologie72013 | original article literatur kommentiert strahlenther onkol 2013 189 : 596597 doi 10.1007 / s00066 - 013 - 0338 - x online publiziert : 25 . 
mai 2013 springer - verlag berlin heidelberg 2013 g.psychogiosj.zenk hals - nasen - ohren - klinik , universitt erlangen - nrnberg , erlangen keinkausalerzusammenhang zwischenhumanem papillomavirusund nasopharynxkarzinomen originalbeitrag singhi ad , califano j , westra wh ( 2012 ) highrisk human papillomavirus in nasopharyngeal carcinoma . 
insgesamt 34 ( 76% ) karzinome waren ebv - positiv und hpv - negativ , 7 ( 16% ) ebv - negativ und hpv - negativ und 4 ( 9% ) ebv - negativ und hpvpositiv . 
die p16 - immunhistochemie ist ein zuverlssiger marker , um ebv - assoziierte und hpvassoziierte karzinome des waldeyer - rachenrings zu differenzieren . kommentar das nasopharynxkarzinom stellt eine seltene tumorentitt dar , welche eine seit lngerem bekannte assoziation mit dem ebstein - barr - virus ( ebv ) aufweist . 
bei frhen oropharynxkarzinomen dagegen ist eine prognostische relevanz der hpv - infektion noch fraglich [ 5 ]  . die arbeitsgruppe von singhi hat nun eine retrospektive analyse vorgelegt , um einen eventuellen kausalen zusammenhang des hpv auch mit nasopharynxkarzinomen zu identifizieren . 
eine koinfektion wurde nicht entdeckt , was die theorie eines synergistischen effekts von ebv und hpv in der pathogenese der nasopharynxkarzinome in frage stellt . die schlussfolgerung der autoren ist damit gut nachzuvollziehen , dass hpvpositive tumoren weiterhin spezifisch fr die oropharynxregion sind und im fall der entdeckung eines hpv - positiven nasopharynxkarzinoms der ursprung in benachbarten oropharynx gesucht werden sollte . 
wichtiger fr die tumorgenese im nasopharynx ist aber weiterhin die ebv - infektion . einschrnkungen der gezeigten analysen muss man neben der geringen fallzahl auch wegen der sehr langen beobachtungszeit machen . 
psychogios g , mantsopoulos k , agaimy a et al ( 2012 ) prognostic factors in limited ( t1 - 2 , n0 - 1 ) oropharyngeal carcinoma treated with surgery adjuvant therapy . 
tumor cell expression of erythropoietin ( epo ) and its receptor ( epo - r ) has been reported for several solid tumors [ 2 , 3 , 4 , 5 , 16 ]  . 
our own preceding retrospective studies suggested that higher expression of epo or epo - r is associated with poorer outcomes in patients with esophageal cancer and nonsmall cell lung cancer [ 19 , 21 ]  . 
the present retrospective study investigated the impact of epo expression , epo - r expression , and 11 additional factors on locoregional control ( lrc ) , metastases - free survival ( mfs ) , and overall survival ( os ) in patients with locally advanced scchn . methods and materials tumor cell expression of epo and epo - r was evaluated in tumor samples obtained from tumor resection performed prior to radiotherapy in 144 patients treated for head and neck cancer between 2000 and 2009 . 
the patient characteristics are summarized in .tab.1. immunohistochemistry for epo and epo - r resected tissues were fixed in 4% buffered formalin ( ph 7.0 ) , embedded in paraff the formalin - fixed , paraffin - embedded tumor samples were used for the preparation of a tissue micro array ( tma ) block . 
 the tma block was constructed using a manual tissue arrayer 1 ( beecher instruments , silver spring , md , usa ) with a 1.0 - mm diameter core biopsy needle . 
 endogenous peroxidase was blocked with 0.3% hydrogen peroxidase for 5 m then , the sections were incubated with the anti - human epo polyclonal antibody ( rabbit ; 1 / 30 dilution ; abcam , cambridge , uk ) and anti - human epo - r monoclonal antibody ( mouse , clone mm - 0031 - 6g7 , 1 / 30 dilution ; abcam )  . 
sections were washed with tbs containing 0.1% tween 20 ( ph 7.0 ) and subsequent reaction was performed with the biotin - free horseradish peroxidase enzyme - labeled polymer of the powervision system ( immunologic , duiven , netherlands )  . 
as positive control a sample of renal tissue was used . patients and treatment the data from 144 patients treated with surgery and postoperative radiotherapy for locally advanced scchn between 2000 and 2009 were retrospectively analyzed . 
further criteria for inclusion were successful staining for epo and / or epo - r , histologically proven scc arising from the oropharynx , oral cavity , hypopharynx or larynx , and stage iii or iv disease . 
patients with specific risk factors such as incomplete resection and extracapsular spread of lymph nodes received concurrent chemotherapy with 20 mg / m2 of cisplatin on days 15 and 2933 or with 20 mg / m2 of cisplatin plus 600 mg / m2 of 5 - fluorouracil on days 15 and 2933 . hpv status formalin - fixed , paraffin - embedded tumor probes were analyzed for dna of human papillomavirus ( hpv ) high - risk subtypes 16 , 18 , 31 , 33 , and 51 with in situ hybridization marked with anti - biotin antibody processed in an autostainabstract zusammenfassung strahlenther onkol 2013 189 : 559565 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0320 - 7 n.d.seibolds.e.schildm.p.gebhardf.noackd.rades prognosis of patients with locally advanced squamous cell carcinoma of the head and neck . 
the impact of epo , epo - r , and 11 additional factors on locoregional control ( lrc ) , metastases - free survival ( mfs ) , and overall survival ( os ) was retrospectively evaluated in 144 patients . 
additional factors were age , gender , performance status , preradiotherapy ( pre - rt ) hemoglobin levels , tumor site , histologic grade , t category , n category , human papillomavirus ( hpv ) status , extent of resection , and chemotherapy . 
epo - r expression was an independent prognostic factor for os . keywords head and neck neoplasms radiotherapy erythropoietin receptors , erythropoietin treatment outcome prognose fr patienten mit lokal fortgeschrittenem plattenepithelkarzinom der kopf - hals - region . 
der einfluss von epo , epo - r sowie 11 weiteren prognosefaktoren auf die lokoregionre kontrolle ( lrc ) , das metastasenfreie berleben ( mfs ) und das gesamtberleben ( os ) wurde retrospektiv an 144 patienten untersucht . 
die weiteren faktoren waren alter , geschlecht , allgemeinzustand , hmoglobinwert vor bestrahlung , tumorlokalisation , grading , t - kategorie , n - kategorie , hpv - status , resektionsausma und chemotherapie . 
a tumor was defined as hpv positive , if it showed both a specific p16 pattern as surrogate marker of oncogene activity of e6 and e7 gene , and a positive in situ hpv hybridization result . 
positive control was a squamous - type carcinoma in situ of the cervix uteri of a patient with known hpv subtype ( hpvchip type 3.5 c , chipron gmbh , berlin , germany )  . 
1 9 impact of tumor expression of epo on locoregional control ( top - left ) , metastases - free survival ( top - right ) , overall survival ( bottom ) fig . 
2 9 impact of tumor expression of epo - r on loco - regional control ( topleft ) , metastases - free survival ( top - right ) , overall survival ( bottom ) additional potential prognostic factors tab . 
3 univariate analysis of metastases - free survival at1year ( % ) at2years ( % ) at3years ( % ) in addition to epo expression , epor expression , and hpv status , the following potential prognostic factors were evaluated : age ( 60 versus > 60 years ) , gender , eastern oncology cooperative group ( ecog ) performance status ( 0 1 versus 2 ) , hemoglobin level prior to radiotherapy ( < 12 g / dl versus 12 g / dl ) , tumor site ( oropharynx versus oral cavity versus hypopharynx versus larynx ) , histologic grade ( g12 versus g3 ) , t category ( t1t2 versus t3t4 ) , n category ( n0n1 versus n2n3 ) , extent of resection ( complete versus incomplete ) , and concurrent chemotherapy ( no versus yes )  . statistical considerations patients were followed until death or for a median of 25 months ( range 666 months ) in survivors . 
our own retrospective study of 64 patients with locally advanced esophageal cancer that was published in 2008 suggested that expression of epo and epo - r were negatively associated with treatment outcomes [ 19 ]  . 
in another retrospective study of 62 patients irradiated for stage ii / iii non - small cell lung cancer published in 2011 , epo expression of tumor cells was an independent prognostic factor for locoregional control and survival , and epo - r expression showed a trend towards worse treatment outcome [ 21 ]  . in the present study of patients with locally advanced scchn , epo expression of tumor cells was significantly associated with worse outcomes in terms of lrc , mfs , and os . 
however , there are no prospective studies regarding the impact of epo and epo - r on the outcomes of scchn patients . in addition to lack of expression of epo and of epo - r , improved treatment outcomes were significantly associated with lower tumor stage , favorable tumor site , and higher hemoglobin levels prior to radiotherapy . 
also the tumor site has been previously recognized as an independent prognostic factor for locoregional control and survival in patients with locally advanced head and neck cancer [ 9 , 12 ]  . a negative impact pre - rt hemoglobin levels < 12 g / dl on treatment outcomes has been observed in previous studies of patients with locally advanced scchn [ 9 , 22 ]  . 
these different findings may be explained by the fact that in the present study only patients treated with radiotherapy preceded by surgery and not with radiotherapy alone were included , whereas in the previous study patients receiving definitive radiotherapy or radiochemotherapy were included . 
 the simultaneous integrated boost ( sib ) technique was used to deliver 70 gy ( 2.12 gy per fraction ) to the primary tumor and involved nodes ; 60 gy ( 1.81 gy per fraction ) to the entire nasopharynx and 54 gy ( 1.63 gy per fraction ) to elective lymph nodes in 33 fractions . 
 plans also aimed to keep the mean parotid dose below 26 gy and limit the maximum doses to the spinal cord and brain stem to 45 and 54 gy , respectively . 
mu and treatment times are considerably reduced in arc imrt plans . keywords radiotherapy head and neck cancer intensity - modulated arc therapy organs at risk xerostomia vergleich zweier verschiedener imrt - planungstechniken zur behandlung von nasopharynxkarzinomen . 
bei 10 patienten mit nasopharynxkarzinom , die an die abteilung radioonkologie der universittsklinik istanbul cerrahpasa medical school berwiesen wurden , wurde eine strahlentherapie mit arcund statischer 7 - felder - imrt - technik geplant . 
die sibtechnik ( simultaneuos integrated boost ) wurde verwendet , um den primrtumor und positive knoten mit 70 gy ( 2 , 12 gy pro fraktion ) , den ganzen nasophaynx mit 60 gy ( 1 , 81 gy pro fraktion ) und elektive lymphknoten mit 54 gy ( 1 , 63 gy pro fraktion ) zu bestrahlen . 
die durchschnittliche dosis zur kontralateralen ohrspeicheldrse war 25 , 734 , 27 gy und 27 , 733 , 5 gy ( p = 0 , 008 ) , wohingegen die durchschnittliche dosis zur ipsilateralen ohrspeicheldrse 30 , 656 , 25 gy und 32 , 555 , 93 gy ( nicht signifikant ) bei der arcbzw . 
imrt plans had mu values that were roughly double those ofarcplans.themultiplefieldarrangementandspiltfieldsusedinimrtmean thatthedeliverytimesfortheseplansare significantlylongerthanforimat , since theyincludedeadtimessuchasthetime neededtorepositionthegantryandreprogramthelinearaccelerator ( linac ) ateveryfield.however , planoptimization timeswerelongerimatthanforimrt plans ( 3hverses1h )  . discussion npcisauniquetypeoftumorforwhich radiotherapy is the only curative treatmentoption.formanyyears , npchas beensuccessfullytreatedwithradiotherapyaloneforearlystagesandincombistrahlentherapieundonkologie72013 | original article clpmeanarc clpmeanimrt clp50arc clp50imrt patients patients clp33arc clp33imrt clp66arc clp66imrt patients patients fig . 
doses to 50 , 33 and 66 % of the contralateral parotid gland volume ( d50 % , d33 % , d66 % ) : b contralateral parotid d50 % . 
cozzi l , dinshaw ka , shrivastava sk et al ( 2008 ) a treatment planning study comparing volumetric arc modulation with rapidarc and fixed field imrt for cervix uteri radiotherapy . 
wiehle r , knippen s , grosu al et al ( 2011 ) vmat and step - and - shoot imrt in head and neck cancer strahlenther onkol 187 : 820825 38 . 
lu sh , cheng jc , kuo sh et al ( 2012 ) volumetric modulated arc therapy for nasopharyngeal carcinoma : a dosimetric comparison with tomotherapy and step - and - shoot imrt . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 541546 doi 10.1007 / s00066 - 013 - 0343 - 0 received : 15 october 2012 accepted : 6 march 2013 published online : 25 may 2013 springer - verlag berlin heidelberg 2013 h.yoon1d.oh2h.c.park2s.w.kang4y.han2d.h.lim2s.w.paik3 1 department of health sciences and technology , school of medicine & samsung advanced institute for health sciences and technology , sungkyunkwan university , seoul 2 department of radiation oncology , samsung medical center , sungkyunkwan university school of medicine , seoul 3 department of medicine , samsung medical center , sungkyunkwan university school of medicine , seoul 4 department of radiologic science , korea university , seoul predictivefactorsfor gastroduodenaltoxicitybased onendoscopyfollowing radiotherapyinpatientswith hepatocellularcarcinoma gate predictive factors for gd toxicity in hcc patients . and after rt were ultimately enrolled in the current study . radiation therapy ( rt ) is seldom used for the treatment of hepatocellular carcinoma ( hcc ) due to a lack of experience and understanding of liver tolerance to rt and technical problems associated with the delivery of rt to part of the liver , as it moves during normal breathing . 
with recent advances in rt techniques , such as the development of threeor four - dimensional conformal rt and image - guided rt , many institutions have reported their experiences using rt for hcc [ 8 , 9 , 12 , 15 , 17 , 19 , 20 , 21 ]  . 
the rt doseresponse relationship has been well established in hcc [ 16 ] and patients with responsive tumors have been shown to have better survival rates [ 8 , 9 , 21 ]  . 
gastroduodenal ( gd ) tolerance to rt has been investigated in abdominal malignancies [ 7 , 13 , 14 , 22 ] , but the application of these results to hcc patients requires caution because most hcc patients have liver cirrhosis ( lc ) and portal hypertension , contributing to the development of gd ulcers [ 1 , 11 , 18 ]  . 
thus , it is important to investipreviously , we reported that the percentage of gd volume receiving a rt dose of more than 35 gy ( v35 ) was the most predictive factor for gd toxicity in patients with cirrhosis of the liver [ 10 ]  . 
 thereafter , to strengthen our findings , we have tried to perform esophagogastroduodenoscopy ( egd ) before and after rt based on the protocol for high - risk patients in whom the target volume is in close proximity to the gd . 
in the current study , we analyzed the predictive factors for gd toxicity based on egd findings in hcc patients who were treated with radiotherapy . patients and methods patients a total of 445 patients were treated with rt for hcc between october 2008 and december 2010 at our institution . 
images of respiration aided by a goggle display were acquired using the realtime position management ( rpm ) system ( varian medical systems , palo alto , ca , usa ) to record the respiratory phase . 
1 patient characteristics dosimetric analysis original article characteristics age ( years ) patients n ( % ) median 57 years ( range 3575 years ) 76 ( 84% ) 14 ( 16% ) 77 ( 86% ) 13 ( 14% ) gender male female livercirrhosis childpughclassification mainpvtt intervalbetweenprevioustaceandrt 17 days > 17 days pvtt portal vein tumor thrombosis , rt radiotherapy , tace transcatheter arterial chemoembolization . 78 ( 87% ) 12 ( 13% ) 49 ( 54% ) 41 ( 46% ) 43 ( 48% ) 47 ( 52% ) tab . 
2 endoscopic findings and grade of gastroduodenal ( gd ) toxicity related to radiotherapy gdtoxicityrelatedtoradiotherapy endoscopic findings patients n ( % ) 15 ( 17 ) 14 ( 16 ) 14 ( 16 ) 8 ( 9 ) 52 ( 58 ) 11 ( 12 ) 19 ( 21 ) 8 ( 9 ) duodenitis duodenal ulcer gastritis gastric ulcer ctcae grade gd gastroduodenal , ctcae common terminology criteria for adverse events . the gross tumor volumes ( gtv ) , including the main tumors and / or portal vein tumor thrombosis ( pvtt ) , were delineated at each phase and summed to determine the internal target volume ( itv )  . 
all patients were educated for a minimum 2 - h fast before simulation and treatment to minimize the variation of stomach volume . 542 | strahlentherapieundonkologie72013 gd was delineated from the esophagogastric junction to the second portion of the duodenuthe planning oar volume ( prv ) , which was obtained from the sum of oar at each respiratory phase , was chosen for dosimetric analysis in the stomach ( s - prv ) and duodenum ( d - prv ) to account for organ movement due to respiration . 
 the dosimetric parameters from dvhs were as follows : ( 1 ) dmax : the maximum dose , ( 2 ) d3 ml , d5 ml and d10 ml : the irradiated dose to 3 , 5 and 10 ml of volume , ( 3 ) vdose : the percentage of volume receiving more than the irradiated dose and ( 4 ) avdose : the absolute volume receiving more than the irradiated dose . 
all irradiated doses were converted to the biologically effective dose ( bed ) as described below . mathematical modeling of gd dose the bed to the gd was calculated by considering the various doses per fraction . 
gd toxicity as related to rt was defined as the new development of or the aggravation of endoscopic abnormalities such as an erosive gastroduodenitis or a gd ulcer in close proximity to the rt field following rt . 
for example , if a new gastric ulcer occurred in the fundus of stomach following rt and only the antrum of the stomach and duodenum were included in the rt field , we did not consider it to be gd toxicity as related to rt . 
stomach and duodenum toxicity were evaluated separately and were graded by the common toxicity criteria for adverse events , version 3.0. statistics all dosimetric parameters were analyzed using a receiver operating characteristics ( rocs ) curve . 
the most predictive dosimetric factor and all clinical parameters including gender , age , the presence of lc , childpugh class , the time interval between previous transcatheter arterial chemoembolization ( tace ) and rt , the presence of main portal vein tumor thrombosis ( pvtt ) , smoking history , a past history of gd ulcer , and the use of anti - ulcer drug during rt were analyzed by simple and multiple logistic regression . 
among them , 8 patients used the anti - ulcer drugs during the course of rt . endoscopic findings related to rt findings in the stomach included erosive gastritis in 14 patients ( 16% ) and gastric ulcers in 8 patients ( 9% )  . 
in comparison , findings in the duodenum included erosive duodenitis in 15 patients ( 17% ) abstract zusammenfassung strahlenther onkol 2013 189 : 541546 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0343 - 0 h.yoond.ohh.c.parks.w.kangy.hand.h.lims.w.paik predictive factors for gastroduodenal toxicity based on endoscopy following radiotherapy in patients with hepatocellular carcinoma abstract purpose . 
endoscopic findings showed erosive gastritis in 14 patients ( 16% ) , gastric ulcers in 8 patients ( 9% ) , erosive duodenitis in 15 patients ( 17% ) , and duodenal ulcers in 14 patients ( 16% )  . 
v25 for the stomach and v35 for the duodenum were the significant factors to predict grade 2 gd toxicity . keywords hepatocellular carcinoma radiotherapy gastroduodenal toxicity endoscopy , digestive system vorhersagefaktoren bei magen - darm - toxizitt basierend auf endoskopie mit darauffolgender strahlenbehandlung bei patienten mit leberzellkrebs zusammenfassung ziel . 
die endoskopischen befunde zeigten eine erosive gastritis bei 14 patienten ( 16% ) , magengeschwre bei 8 patienten ( 9% ) , erosive duodenitis bei 15 patienten ( 17% ) und duodenalgeschwre bei 14 patienten ( 16% )  . 
the clinical characteristics of patients who experienced grade 3 toxicity are summarized in .tab.3. dosimetric analysis and clinical factors the results of roc curve analysis for all dosimetric parameters are shown in .tab.4. 
 v25 and v35 were the most predictive factors for grade 2 gd toxicity for the stomach and duodenum , respectively . the gd is the most important doselimiting factor during rt delivery for strahlentherapieundonkologie72013 | original article fig . 
a at 23 days after completion of rt with 35 gy in 10 fractions , endoscopy showed an approximately 1 cm ulceration with whitish exudate on a pylorus ring and a 5 mm shallow ulceration on a duodenal bulb . 
 treatment included argon plasma coagulation with two vials of thrombin spray , followed by a transfusion due to the low hemoglobin level of 6.6 g / dl the treatment of upper abdominal malignancy . 
for the whole stomach , 2 / 3 of the stomach , and 1 / 3 of the stomach , 50 , 55 , and 60 gy , respectively , were suggested for td5 / 5 ( the probability of 5% complication within 5 years )  . 
 [ 14 ] reported that v50 of 16 cm3 may be the best predictor for grade 2 acute gi toxicity . however , these data may not be applicable for hcc patients because most hcc patients have lc and / or portal hypertension , which are known to be predisposing factors for gd ulcers . 
it has been shown that portal hypertension may contribute to an increased risk of gd ulcer as a result of impairment of the gastric mucosal defenses [ 11 ]  . 
these findings were also observed in endoscopy of cirrhotic patients [ 6 ]  . our previous report first showed a dosevolume analysis of gd toxicity in cirrhotic patients with hcc [ 10 ]  . 
 thereafter , gd toxicity has been a concern in hcc patients treated with rt ; thus , we tried to perform egd in highrisk patients to detect the gd toxicity . 
in the current study , we confirmed the dose volume effect for gd toxicity , but there were several differences compared to our previous study : gd toxicity was detected based on egd findings , a bed equivalent of 2 gy per fraction was used to represent the various doses per fraction , and the concept of prv was introduced . 
the use of concurrent chemotherapy , differences in rt volume and prescribed dose , and selection bias for the study population may explain the higher rates of modest complications in the study by chon et al . our study has several limitations . 
however , prv is not able to represent the true irradiated volume during rt because the stay time of each respiratory phase during the beam - on phase of rt could vary . 
kim h , lim do h , paik sw et al ( 2009 ) predictive factors of gastroduodenal toxicity in cirrhotic patients after three dimensional conformal radiotherapy for hepatocellular carcinoma . 
li b , yu j , wang l et al ( 2003 ) study of local threedimensional conformal radiotherapy combined with transcatheter arterial chemoembolization for patients with stage iii hepatocellular carcinoma . 
milano mt , chmura sj , garofalo mc et al ( 2004 ) intensity - modulated radiotherapy in treatment of pancreatic and bile duct malignancies : toxicity and clinical outcome . 
nakamura a , shibuya k , matsuo y et al ( 2012 ) analysis of dosimetric parameters associated with acute gastrointestinal toxicity and upper gastrointestinal bleeding in locally advanced pancreatic cancer patients treated with gemcitabine - based concurrent chemoradiotherapy . 
oh d , lim do h , park hc et al ( 2010 ) early threedimensional conformal radiotherapy for patients with unresectable hepatocellular carcinoma after incomplete transcatheter arterial chemoembolization : a prospective evaluation of efficacy and toxicity . 
seong j , lee ij , shim sj et al ( 2009 ) a multicenter retrospective cohort study of practice patterns and clinical outcome on radiotherapy for hepatocellular carcinoma in korea . 
yamada k , izaki k , sugimoto k et al ( 2003 ) prospective trial of combined transcatheter arterial chemoembolization and three - dimensional conformal radiotherapy for portal vein tumor thrombus in patients with unresectable hepatocellular carcinoma . 
yoon sm , lim ys , won hj et al ( 2012 ) radiotherapy plus transarterial chemoembolization for hepatocellular carcinoma invading the portal vein : long - term patient outcomes . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . case study strahlenther onkol 2013 189 : 586589 doi 10.1007 / s00066 - 013 - 0356 - 8 received : 3 march 2013 accepted : 25 march 2013 published online : 5 june 2013 springer - verlag berlin heidelberg 2013 a.wygoda1t.rutkowski1d.ponikiewska2b.hejduk3k.skadowski1 1 department of radiation and clinical oncology , maria sklodowska - curie memorial cancer center and institute of oncology , gliwice branch , gliwice 2 department of pathology , maria sklodowska - curie memorial cancer center and institute of oncology , gliwice branch , gliwice 3 department of radiology , maria sklodowska - curie memorial cancer center and institute of oncology , gliwice branch , gliwice ewingssarcoma ofthelarynx effectivetreatmentwithorganpreservation ewings sarcoma / primitive neuroectodermal tumor ( es / pnet ) is a rare , but highly malignant neoplasm of mesenchymal origit occurs predominantly in adolescents and young adults between 8 and 30 years of age , with a slightly higher prevalence among males . 
es / pnet usually involves the pelvis , the lower extremities , the chest wall and in rare cases , the upper extremities . es / pnet is a very rare disease in the head and neck regionmost cases are described only sporadically as case reports or small retrospective series . 
primary sites routinely affect mandible , paranasal sinuses , skull and orbits [ 1 , 2 ]  . magnetic resonance imaging ( mri ) and computed tomography ( ct ) are routinely used in diagnostic imaging of the primary tumor : mri to show soft tissue invasion and ct to evaluate bone destruction . 
fluorodeoxyglucose positron - emission tomography ( fdg - pet ) also plays an important role in whole body assessment . the treatment modality always consists of multiagent chemotherapy , which is followed by either wide local excision with postoperative radiotherapy or radiotherapy alone applied to the primary site . 
1 8 endoscopic view of neoplastic infiltration in the anterior part of larynx , occupying anterior commissure , both vocal cords and the laryngeal ventricles with left - sided predominance 586 | strahlentherapieundonkologie72013 fig . 
3 8 micrograph showing a tumor with uniform small round cells with round to oval open nuclei , scanty pale cytoplasm with indistinct cytoplasmic membranes , dusty chromatin and inconspicuous nucleoli . 
4 8 fdg - pet shows a single metabolically active disease site in the anterior part of larynx compared to other sarcomas , ewings sarcomas represent neoplasms that respond well to radiation therapy . 
adjuvant multiagent chemotherapy is strongly recommended because of the high risk of distant , predominantly skeletal and pulmonary metastases . extraskeletal es / pnet ( ees / pnet ) in the head and neck region is extremely rare . 
in all instances , a surgical procedure was part of the multimodality treatment [ 4 , 5 , 6 ]  . we present the successful treatment with organ preservation of a case of ees / pnet arising in the larynx with cartilage invasion . case report a 68 - year - old male patient ( non - smoker and not a user of alcohol ) was referred to our department with a 3 - month history of hoarseness and occasional aphonia . 
within level iia , oval , homogenously contrast - enhanced 10 - mm neck nodes were diagnosed . microscopically , biopsy fragments taken from the laryngeal lesion ( maximal diameter 0.5 cm ) revealed infiltration of uniform , small round cells with round to oval open nuclei and scanty pale cytoplasm with indistinct cytoplasmic membranes . 
immunohistochemistry showed strong , diffuse positivity for cd99 , nse ( .fig.3b and c ) and vimetin , as well as weak focal staining for synaptophys there was high cell proliferation , with approaching 90% of the tumor cells expressing ki67 . 
all other immunostains , includstrahlentherapieundonkologie72013 | case study ing s - 100 protein , desmin , actin , myod1 , myf4 , sma , cd56 , chromogranin , leukocyte common antigen ( lca ) , cd34 , ema and cytokeratin , were negative . 
additionally , in situ fluorescent hybridization performed on paraffin - embedded tissue using a ewings sarcoma gene ( ews ) specific dual color break - apart probe revealed a breakpoint in chromosome 22q12 , demonstrating ews gene rearrangement . 
four weeks later , the patient began radiotherapy comprising a total dose of 60 gy applied in 30 fractions over 6 weeks , and 50 gy in 25 fractions over 5 weeks to the larynx and neck node groups ii - iv , respectively . 
after 30 months of follow - up , patient is free of tumor relapse and in very good condition . discussion ees / pnet is a very rare variant of es / pnet that originates in soft tissue rather than bone and is predominantly observed in children and adolescents . 
 data concerning ees / pnet in the head and neck region are limited , but prognoses are routinely favorable [ 1 , 2 , 3 , 4 , 5 ]  . 
 one of reasons for this may be the early diagnoses that result from early symptom manifestation when the tumor originates in a vital structure . differential histological diagnoses of small , blue , round cell tumors include malignant lymphoma , rhabdomyosarcoma , poorly differentiated synovial sarcoma , primary or secondary neuroblastoma and es / pnet . 
expression of cd99 is particularly useful in confirming an es / pnet diagnosis , although it is not specific ; other tumors , such as lymphoblastic lymphoma , poorly differentiated synovial sarcomas and rhabdomyosarcomas may also show positive staining by antibodies ( o - 13 , mic - 2 or hba - 71 ) to the cd99 antigen ( a product of the mic2 gene present on the x chromosome )  . 
lymphoblastic lymphoma , rhabdomyosarcoma and poorly differentiated synovial sarcoma can by excluded by negative staining for lca , markers of muscle differentiation ( desmin , actin , myod1 , myf4 , sma ) and cytokeratin , and ema , respectively . 
neuroblastoma can be excluded by negative staining for cd56 , chromogranin , synaptophysin , neurofilament and s - 100 protein , as well as by confirming the absence of rosette formation and neurofibrillary matrix . 
effective treatment with organ preservation abstract extraskeletal ewings sarcoma arising in the head and neck region is an extremely rare malignant neoplaswe describe the unusual case of a tumor originating in the larynx of a 68 - year - old male with hoarseness and occasional aphonia . 
to our knowledge , this is the first report of this type of tumor in the larynx with cartilage invasion that documents the effectiveness of radiotherapy as an alternative to surgical management . 
at present , after 30 months of follow - up , the patient is free of tumor relapse and in very good condition . keywords hoarseness aphonia radiotherapy chemotherapy positron - emission tomography ewing sarkom des kehlkopfs . 
wolters kluwer | lippincott williams & wilkins , philadelphia , s 392 therapy for ees / pnet is similar to that for es / pnet and involves multiagent chemotherapy for eradication of microscopic or overt metastatic disease , followed by surgery and / or radiotherapy for control of the primary tumor . 
the most effective chemotherapy regimens include a combination of ifosfamide , cyclophosphamide , doxorubicin , etoposide , vincristine and dactinomycin , which work well for both es / pnet and ees / pnet . 
no significant impact of total radiation dose was observed ; however , patients with lower volume tumors have better survival results [ 11 ]  . local control is essential to reducing the risk of es / pnet dissemination . 
distant metastases routinely involve bones and not the lungs , as is routinely observed in other soft tissue tumors . in patients with typical extremity or trunk tumor locations , fdg - pet is more accurate than other conventional imaging techniques , with a sensitivity of 100% and a specificity of 96% . 
this is particularly true for patients undergoing radiotherapy , where the need for psychosocial support is quoted in literature at about 1450% [ 5 , 6 , 7 , 8 , 22 ]  . 
to effectively identify highly distressed patients , a routine questionnaire - based screening of patients is recommended by a number of national and international agencies [ 3 , 9 , 18 ]  . 
psychological information may be of relevance for clinicians and nurses , but is regarded as additional information of subordinate importance . implementation of a screening tool in daily routine can only be successful if comprehensive , multidisciplinary information for physicians , nurses and psychologists is assessed in a transparent manner that generates relevant information for each profession . 
there is thus a need for a screening questionnairecompiled from well - established subscales of validated assessment toolsthat focuses on high practicability and clinically relevant multidisciplinary information and can be put into practice immediately . the aims of our study are : 1 . 
 to analyze the effectiveness of implementation in clinical routine with qualitative pilot assessment of patients acceptance , analysis of missing data and validation testing . materials and methods compilation of the screening questionnaire compilation of the screening questionnaire focused on a comprehensive approach including patients physical - , socialand psychological problems and needs . 
the questionnaire was compiled in close multidisciplinary cooperation between psychologists , physicians and nurses . the database analysis was approved by the ethical committee of the medical university of vienna , 2011 . 
the project was performed without funding . after minor changes to and shortening of the subscales , the pilot test phase proved the questionnaire to be practical within a busy clinical routine and acceptable for self - assessment . 
 the final versionrestricted to one double - sided sheet to maintain patient effort at an acceptable levelwas implemented in the department of radiotherapy ( available online as supplementary information to this article )  . social information regarding family status , education , current profession and domestic circumstances was assessed . 
pain was evaluated on an 11 - point visual analogue scale ( vas ) with minimum of 0 ( no pain ) and a maximum of 10 ( maximum pain ) [ 20 ]  . 
the questionnaire is strongly based on the expert psycho - oncology basic documentation ( po - bado ) rating scale [ 10 ] , but reformulated into easy terms for patients self - assessment . 
psychological strains were assessed with the hornheide screening instrument ( hsi ) [ 24 , 25 , 26 ]  . the informational needs section offered the patient further information in the form brochures covering seven areas of common interest . 
the section psychological symptoms was based on a po - bado subscale [ 10 ] , again reformulated for patients self - assessment instead of expert rating . patient cohort and screening approach all patients were included consecutively at their first visit to the department of radiotherapy . 
the only exclusion criterion was age under 18 years . the majority of patients were invited personally during their waiting time , by a psychologist subject to training and su574 | strahlentherapieundonkologie72013 pervision . 
the average time required to fill out the questionnaire was around 10 mfor the majority of patients , assessment in an informal personal interview took around 20 min , including initial counseling . where data were provided , these were made available to the treating physician and nurse , who then had a preliminary overview of the patients status . 
these patients were promptly contacted and received the relevant informational material or an offer of psychosocial support upon their next visit to the department . methodology effectivenessofimplementation patient acceptance : qualitative pilot testing to evaluate patient acceptance , we asked 25 patients in an open question how they rate the opportunity to report their physical - , socialand psychological problems and needs before their first visit . 
patients answers were recorded in open format and subsequently subsumed into categories by the consensus of two psychologists . analysis of data quality as the database was used routinely by the team of psychologists , several people had access to data entry . 
the reasons for missing data were collected and analyzed to rule out a potential systematic bias . psychological subscales validation analysis analysis of criterion validity for the hsi psychological strains and po - bado selfassessment psychological symptoms subscales was performed using the hospital anxiety and depression scale , german version ( hads - d ) as an external criterion . 
the hads - d was chosen as it is a well - established international instrument with excellent psychometric properties [ 21 ] , which is often used as a benchmark in validating other distress measurements . 
although requiring additional personnel resources , it can be implemented successfully in clinical routine with benefits for both the patient and the professional team . keywords psychosocial support self - assessment rating scale quality of life activities of daily living validierung und praktische implementierung eines multidisziplinren distress - screeningfragebogens fr krebspatienten zusammenfassung hintergrund . 
er konnte erfolgreich in der routineversorgung implementiert werden , sowohl zum vorteil der patienten als auch des behandlungsteams , erfordert jedoch zustzlichen personalaufwand . schlsselwrter psychosoziale untersttzung selbsteinschtzung beurteilungsskala lebensqualitt alltgliche aktivitten characteristic ( roc ) curves are provided , including c - indices ( relating to the area beneath the curve ) and confidence intervals ( ci ) at a significance level of 5% . 
the sensitivity , specificity and overall accuracy of the model are reported . for the analysis of internal consistency , cronbachs is given . effectiveness of implementation patientacceptance : qualitativepilottesting acceptance of the screening tool was generally high , but some additional critical strahlentherapieundonkologie72013 | original article n = 160 patients planned for admission at the department n = 146 patients admitted for 1st visit n = 110 ( 75% ) patients included in screening n = 36 ( 25% ) patients missing in screening n = 57 personal talk n = 53 with questionnaire n = 29 organizational problems poor general condition ( not able to talk or write ) foreign language ( no translation possible ) refused participation fig . 
1 9 analysis of missing data ( subgroup of n = 160 consecutive patients ) roc curve for distress self - assessment by po - bado roc curve for hsi psychological strains subscale 1 specificity 1 specificity fig . 
2 8 roc curves for psychological subscales compiled using hospital anxiety and depression scale , german version ( hads - d ) data from a subgroup of n = 100 breast and cervix cancer patients . 
summarizing the patients statements , the personal invitation and the offer to talk about well - being and problems were particularly appreciated . analysisofdataquality among the 9750 monitored items , 106 mistakes in data entry were found . 
patients were missed mainly as a consequence of organizational problems , particularly during an overload situation with several patients arriving for their first visit at the 576 | strahlentherapieundonkologie72013 same time . 
for the psychological strains of hsi , the optimal cutoff was set at 1.09 weighted regression score points . the psychological symptoms of pobado show a sensitivity of 0.89 and a specificity of 0.71 , with an accuracy of 0.76. 
these results show conclusively that the po - bado expert rating value can be assessed directly by the patients . regarding hsi , it must be stated that the validation analysis started with the original cutoff value published by the authors [ 25 ]  . 
in the actual sample , this resulted in a disproportionately high number ( 59% ) of positive patients ( sensitivity of 89% , but a low specificity of 51% ; overall accuracy 62% )  . 
consequently , the optimal cutoff value for hsi was recalculated based on the roc curves , which improved sensitivity and specificity significantly . overall , the validation results are comparable to different distress measurements in the literature : the questionnaire on stress in cancer patients revised version 23 ( qsc - r23 ) from herschbach , 2004 [ 11 ] was also validated against hads - d , leading to a sensitivity of 88% and a specificity of 72% . 
jacobson [ 13 ] reported 77% sensitivity and 68% specificity for the distress thermometer in 2005 . a limitation of the validation analysis is that the sample of 100 female ( breast and cervix ) cancer patients cannot be considered fully representative of the population , as it is well documented in the literature that women report more distress and more frequently express a cry for help . 
 sensitivity and specificity values should be therefore regarded with caution . the internal consistency of the psychological symptoms subscale ( po - bado self - assessment ) can be regarded as good ( 0.843 ) , while the psychological strains subscale ( hsi ) remains questionable ( 0.617 ) according to the general rule of thumb for interpretation . 
this means that the single psychological symptoms as captured by the po - bado self - assessment show high intercorrelations , while single psychological strains occur more selectively and independently of each other . the first step of implementation into clinical routine included making a personal approach to the patient , offering the choice of filling out the questionnaire on their own or during an informal personal interview . 
the opportunity to have an informal personal talk was appreciated as shown by the qualitative feedback from the first 25 patientsand more than half of the patients chose this option . in the second step , the treating physician and the nurse received this first comprehensive overview of the patients status . 
this can be regarded as major advantage , as patients increasingly tend toward searching for additional information in the internet , although the quality of the information they find here may be questionable [ 15 ]  . in the third step , data were entered into a database without delay , such that highly distressed patients could be contacted promptly by the team of psychologists . 
this result clearly shows the limitations of screening , even if one person has control of screening all patients , and offering psychosocial support and information at the same time . 
different authors have had similar experiences , concluding that a screening procedure can only be performed with additional staff [ 23 ] and that the additional time and effort required represent significant barriers to its widespread use [ 12 ]  . nevertheless , we conclude that this approach is helpful for patients and optimizes the psychosocial support , even if it does not include all our patients . it is well known that some patients have certain misgivings about psychology [ 9 ]  . 
with the option of a personal approach during the screening procedure integrated into the daily medical routine , patients can be reached without active initiation on their part and contact restraints can be effectively reduced . 
highly distressed patients appreciate this opportunity to talk , which can provide a first emotional relief . the main concern in clinical practice is not to overlook patients in a very poor condition and therefore overestimate psychological status , as often critically discussed in the literature [ 6 , 19 ]  . 
due to the personal commitment of the coworkers who actively approach the patients , the sample can be considered representative for all patients undergoing radiotherapy in our department . this report on practical implementation and validation of the multidisciplinary distress questionnaire compilation is part 1 of a larger cancer screening project . 
we thank all our patients for providing us with information and our team of psychologists barbara mikulas , stefanie klug , antonia nitsch , iris hinker , marlene keil and hannah eberle for their invaluable contributions . 
newell s , sanson - fisher rw , girgis a , bonaventura a ( 1998 ) how well do medical oncologists perceptions reflect their patients reported physical and psychosocial problems ? data from a survey of five oncologists . 
sllner w , devries a , steixner e et al ( 2001 ) how successful are oncologists in identifying patient distress , perceived social support , and need for psychosocial counselling ? br j cancer 84 ( 2 ) : 179 23 . 
walker j , postma k , mchugh gs et al ( 2007 ) performance of the hospital anxiety and depression scale as a screening tool for major depressive disorder in cancer patients . 
 auch zum zeitpunkt der strahlentherapeutischen behandlung erleben patienten psychosoziale belastungen , die noch weit nach der behandlung persistent sein knnen [ 16 , 17 , 18 , 29 , 35 , 37 ]  . 
die dimension der von krebspatienten bentigten psychosozialen hilfsangebote geht dabei von informationen zur erkrankung und fragen zu finanziellen untersttzungsmglichkeiten bis hin zur therapeutischen behandlung psychischer komorbiditten [ 9 , 32 , 34 ]  . 
die positive wirkung psychoonkologischer interventionen auf lebensqualitt und empfundene psychische und psychosoziale belastungen konnte in einer metaanalyse krzlich gezeigt werden [ 7 ]  . die grnde fr die diskrepanz zwischen dem bedarf an psychosozialer untersttzung und der inanspruchnahme sind vielfltig . 
mehrere studien zeigen , dass nur etwa die hlfte der krebspatienten ber die mglichkeit der inanspruchnahme psychosozialer hilfsangebote und deren inhalt informiert sind [ 12 , 18 , 25 , 27 ]  . 
aktuell stellen die berweisung durch die behandelnden rzte , pflegekrfte und die selbstzuweisung der patienten die wichtigsten zugangswege zu psychosozialen hilfeleistungen dar [ 22 ]  . zur vorhersage adquaten gesundheitsverhaltens spielt auch die selbstwirksamkeitserwartung eine wichtige rolle . 
es gibt hinweise darauf , dass sich eine hohe selbstwirksamkeitserwartung , auch unabhngig vom tatschlichen verhalten , positiv auf die lebensqualitt sowie auf ngste und depressionen von krebspatienten auswirkt [ 14 , 21 ]  . 
es erscheint dabei erstrebenswert , dass informationen ber psychosoziale angebote systematisch an den patienten herangetragen werden [ 6 , 23 ]  . ffentliche daten oder experimentelle studien darber , wie krebspatienten aktuell in krankenhusern ber psychosoziale hilfsmglichkeiten informiert werden , liegen derzeit nicht vor . 
 die hier erstmals evaluierte , besonders einfache und kostengnstige mglichkeit , durch informationsschreiben die strahlentherapieundonkologie72013 | beurteilung der eignung ( n = 110 ) alternierend zugeteilt ( n = 108 ) ausgeschlossen ( n = 2 ) - einschlusskriterien nicht erfllt ( n = 2 ) keine ausreichenden deutschkenntnisse zur kontrollgruppe zugeordnet ( n = 54 ) zur intervention zugeordnet ( n = 54 ) originalien daten analysiert ( n = 45 ) - von datenanalyse ausgeschlossen ( n = 9 ) unvollstndiger datensatz ( n = 7 ) therapie nicht abgeschlossen ( n = 7 ) whrend der therapie verstorben ( n = 1 ) daten analysiert ( n = 51 ) - von datenanalyse ausgeschlossen ( n = 3 ) unvollstndiger datensatz abb . 
1 9 flussdiagramm zu einund ausgeschlossenen patientinnen kenntnis der patienten zu steigern , um ihnen die mglichkeit der inanspruchnahme zu erleichtern , scheint dabei noch nicht ausreichend ausgeschpft worden zu seziel der vorliegenden studie war es , herauszufinden , ob sich die systematische bereitstellung schriftlicher informationen ber vorhandene psychosoziale angebote positiv auf die kenntnis und selbstwirksamkeit der patienten sowie die tatschliche inanspruchnahme auswirkt . methode studiendesign die untersuchung wurde als 2 - armige kontrollierte studie im parallelgruppendesign mit einem messzeitpunkt nach abschluss der intervention konzipiert . 
bei einer angenommenen initialen kenntnisrate von 50% liee sich bei einer power von 80% und einem - niveau von 0 , 05 mit dieser stichprobengre ein unterschied von 25% zwischen beiden gruppen als signifikant nachweisen [ 11 ]  . 
10% wurden insgesamt 110 patienten in die studie aufgenommen . stichprobe und rekrutierung in die studie eingeschlossen wurden alle erwachsenen brustkrebspatientinnen , die nach vorangegangener operation , mit oder ohne zustzliche chemotherapie , fr eine ambulante strahlentherapie in der radiologischen universittsklinik heidelberg vorgesehen waren . 
die studie wurde durch die ethikkommission der medizinischen fakultt der universitt heidelberg positiv begutachtet . im verlauf der 4 , 5 - monatigen rekrutierungsphase von september 2009 bis februar 2010 wurden 110 patientinnen hinsichtlich ihrer studieneignung berprft , wovon 2 aufgrund nicht ausreichender deutschkenntnisse ausgeschlossen werden mussten . 
die systematische bereitstellung von informationen hatte einen positiven einfluss auf die kenntnis der psychosozialen angebote ( p = 0 , 042 ; d = 0 , 45 ) und die selbstwirksamkeitserwartung ( p = 0 , 047 ; d = 0 , 42 )  . 
die inanspruchnahme der psychosozialen angebote konnte durch die alleinige informationsbereitstellung nicht gesteigert werden . schlsselwrter psychosoziale angebote inanspruchnahme kenntnis selbstwirksamkeit strahlentherapie effect of systematic information about psychosocial support services during outpatient radiotherapy . 
at two predefined time points before and during radiotherapy , patients in the intervention group received correspondence informing them about psychosocial services ( psycho - oncology , clinical social work and the cancer information service ) .the control group received no systematic information . 
the systematic provision of information in the form of written correspondence can easily be implemented into clinical routine and is an effective way to increase cancer patients knowledge of psychosocial support services . 
dies entspricht einer befragungsquote von 89% . intervention die patientinnen in der interventionsgruppe erhielten vor und nach beginn der strahlentherapeutischen behandlung einen personalisierten brief und ein informationsblatt ber die psychosozialen angebote ( krebsinformationsdienst , sozialdienst und psychoonkologie ) zugeschickt . 
alle patientinnen wurden in der folge medizinisch nach strahlentherapeutischem protokoll behandelt . messinstrumente zur erhebung der kenntnis und der selbstwirksamkeitserwartung sowie der inanspruchnahme psychoonkologischer angebote wurde ein speziell entwickelstrahlentherapieundonkologie72013 | tab . 
der kenntnisstand wurde , getrennt hinsichtlich dreier aspekte ( psychoonkologie , sozialdienst und krebsinformationsdienst ) , jeweils durch die frage kennen sie die genannten untersttzungsangebote ? mit dichotomen antwortmglichkeiten ( ja / nein ) erfasst und zu einem gesamtwert addiert . 
dieser gesamtwert konnte die werte 0 ( = keinerlei kenntnis psychosozialer angebote ) bis 3 ( = alle angebote bekannt ) annehmen . die selbstwirksamkeitserwartung wurde als mittelwert aus zwei spezifisch fr diese fragestellung konstruierten fragen bestimmt ( ich kann selbst etwas zur verbesserung meiner situation beitragen und ich bin selbst dafr verantwortlich , welche informationen ich rund um die erkrankung habe )  . 
zu der frage wie stark stimmen sie diesen aussagen zu ? konnten die patientinnen auf einer 5 - stufigen likert - skala unter folgenden antwortmglichkeiten whlen : gar nicht , wenig , mittel , ziemlich , sehr stark . 
 die reliabilitt ( cronbachs alpha ) der zusammengefassten skala betrug 0 , 66 . die inanspruchnahme wurde getrennt hinsichtlich dreier aspekte ( psychoonkologie , sozialdienst und krebsinformationsdienst ) jeweils durch die frage nehmen sie eine oder mehrere dieser untersttzungsangebote in anspruch ? mit dichotomen antwortmglichkeiten ( ja / nein ) erfasst und ebenfalls zu einem gesamtwert addiert . 
dieser score konnte die werte 0 ( = keinerlei inanspruchnahme psychosozialer angebote ) bis 3 ( = alle angebote in anspruch genommen ) annehmen . als kovariaten wurden soziodemographische daten ( alter und bildung ) sowie der grad der belastung mittels des distress - thermometers [ 19 ] erfasst . 
2 ergebnisse der kovarianzanalysen ( bezglich bildung , alter und belastung adjustierte mittelwerte ) kontrollgruppe interventionsgruppe mittelwert mittelwert standardfeh0 , 18 standardfeh0 , 17 testgre ( df ) p - wert 0 , 12 0 , 13 0 , 45 0 , 042 f ( 1 , 79 ) = 4 , 27 f ( 1 , 84 ) = 4 , 08 kenntnisa selbstwirksamkeitserwartung inanspruchnahme abei der abhngigen variable kenntnis erklrt die kovariate bildung einen signifikanten anteil der gesamtvarianz auf , f ( 1 , 79 ) = 6 , 18 , p = 0 , 0150 zz beinteilung nach cohen ( 1988 ) : d = 0 , 20 kleiner effekt ; d = 0 , 50 mittlerer effekt ; d = 0 , 80 groer effekt f ( 1 , 83 ) = 0 , 26 0 , 047 0 , 661 0 , 42 0 , 10 0 , 11 0 , 12 .tab.2 zeigt die ergebnisse der kovarianzanalysen . 
hinsichtlich der inanspruchnahme psychosozialer angebote zeigte sich jedoch kein effekt der informationsbereitstellung . betrachtet man die untersuchten zielvariablen auf ebene der einzelnen items ( .tab.3 ) , so zeigt sich , dass unterschiede in der kenntnis hauptschlich beim krebsinformationsdienst zu finden sind . 
 bei der psychoonkologie bleibt die inanspruchnahme in beiden gruppen niedrig ( 5 , 9 bis 8 , 9% )  . die korrelation der inanspruchnahme der angebote mit deren kenntnis und selbstwirksamkeitserwartung ergab hinsichtlich des zusammenhangs der inanspruchnahme und kenntnis ein signifikantes ergebnis ( r = 0 , 28 ; p = 0 , 009 )  . 
 dieser zusammenhang lsst sich auch auf der ebene der einzelitems nachweisen : die inanspruchnahme des kliniksozialdiensts hing mit der kenntnis des kliniksozialdiensts zusammen ( 2 ( 1 ) = 10 , 1 ; p = 0 , 001 ) , ebenso die inanspruchnahme des krebsinformationsdiensts mit dessen kenntnis ( 2 ( 1 ) = 9 , 1 ; p = 0 , 002 )  . 
die inanspruchnahme der psychoonkologie hing nur tendenziell mit der kenntnis der psychoonkologie zusammen ( 2 ( 1 ) = 4 , 1 ; p = 0 , 09 )  . 
es bestand kein signifikanter zusammenhang zwischen der selbstwirksamkeitserwartung der patienten und der inanspruchnahme oder der kenntnis der angebote . diskussion die ergebnisse der vorliegenden kontrollierten studie belegen die wirksamkeit einer systematischen bereitstellung von informationen ber psychosoziale untersttzungsmglichkeiten . 
vor dem hintergrund , dass eine hhere selbstwirksamkeitserwartung , also das gefhl selbst etwas zur verbesserung der eigenen situation beitragen zu knnen , positive auswirkungen auf die belastungen von krebspatienten hat [ 13 , 21 ] , ist dieser befund von hoher theoretischer und praktischer bedeutung . 
dies ist umso erstaunlicher , als ber 50% aller studienteilnehmerinnen zum befragungszeitpunkt einen erhhten distress - wert angaben , was auf untersttzungsbedrftigkeit hinweist [ 19 ]  . aus unserer klinischen erfahrung wissen wir , dass viele patienten in der phase einer anstrengenden therapie noch kein aktives interesse an supportiver behandlung haben , sondern hufig zunchst abwarten , ob durch eine erfolgreiche krebsbehandlung auch die psychische belastung von alleine abnimmt . 
ein besonderes augenmerk sollte auf den nebenwirkungen der therapie liegen , da diese teilweise unterschtzt werden [ 13 ] und psychosoziale auswirkungen haben knnen [ 16 ]  . desweiteren zeigen die ergebnisse der vorliegenden studie , dass nur etwa die hlfte der teilnehmerinnen in der kontrollgruppe ber die mglichstrahlentherapieundonkologie72013 | tab . 
3 vergleich der kenntnis , selbstwirksamkeitserwartung und inanspruchnahme zwischen den gruppen kontrollgruppe interventionsgruppe p - wert originalien kenntnis selbstwirksamkeitserwartunga psychoonkologie klinische sozialarbeit krebsinformationsdienst ich kann selbst etwas zur verbesserung meiner situation beitragen ich bin selbst dafr verantwortlich , welche informationen ich rund um die erkrankung habe inanspruchnahme adichotomisiert : werte 3 = ablehnung ; werte 4 = zustimmung psychoonkologie klinische sozialarbeit krebsinformationsdienst anzahl prozent anzahl prozent 48 , 9 66 , 7 42 , 2 48 , 9 68 , 9 26 , 7 62 , 7 68 , 6 64 , 7 64 , 7 68 , 6 19 , 6 17 , 6 statistischertest ( df ) 2 ( 1 ) = 1 , 23 2 ( 1 ) = 0 , 01 2 ( 1 ) = 4 , 79 0 , 27 0 , 90 0 , 03 2 ( 1 ) = 6 , 43 0 , 01 2 ( 1 ) = 2 , 72 0 , 08 2 ( 1 ) = 0 , 27 2 ( 1 ) = 0 , 54 2 ( 1 ) = 1 , 64 0 , 60 0 , 47 0 , 20 keit der inanspruchnahme psychosozialer angebote informiert war . 
unsere untersuchung ergab , dass sich der bekanntheitsgrad zwischen den jeweiligen angeboten unterscheidet , wobei der kliniksozialdienst bei den patienten am strksten reprsentiert war . trotz der positiven ergebnisse ist es nicht gelungen , alle patientinnen der interventionsgruppe ber die existenz psychosozialer angebote zu informieren . 
auch dieser befund steht im einklang mit anderen untersuchungen , bei denen gerade weniger gebildete patienten schlechter ber psychosoziale angebote informiert waren und diese weniger in anspruch genommen haben [ 6 , 22 ]  . 
fr patientinnen mit niedrigerem bildungsniveau scheint die hier gewhlte vermittlung der information also nicht ausreichend zu sein diesem zusammenhang sind weitere manahmen , wie ein belastungsscreening und die zuweisung der patienten durch das medizinische personal notwendig und sinnvoll , um eine bedarfsgerechte psychosoziale versorgung von krebspatienten zu erreichen [ 20 ]  . in der hier vorgelegten studie ging die verbesserte informiertheit der patientinnen ber psychosoziale angebote in der interventionsgruppe nicht mit einer hheren inanspruchnahme der angebote einher . 
demnach sind fr die handlungsumsetzung nicht nur die kenntnis der mglichkeiten sondern auch die subjektive bewertung der eigenen belastung , uere barrieren wie zeitaufwand sowie erwartungen ber ziel und ergebnis mitentscheidend [ 28 ]  . 
in hnlichen studien zur orientierung von patienten ber supportive behandlungsmglichkeiten wurden daher die erwartungen an die intervention ebenfalls nur partiell erfllt [ 5 ]  . insgesamt sollten psychosoziale angebote als integriertes element in der routinemigen onkologischen versorgung von allen patienten und angehrigen wahrgenommen und genutzt werden knnen [ 20 ]  . 
knftige studien sollten daher die allgemeingltigkeit der vorliegenden ergebnisse an weiteren erkrankungsarten und beiden geschlechtern berprfen . eine weitere einschrnkung der studie ist , dass im design keine erhebung der basisraten bezglich vorwissen und inanspruchnahme von psychosozialen angeboten im vorfeld stattfand . 
eakin eg , strycker la ( 2001 ) awareness and barriers to use of cancer support and information resources by hmo patients with breast , prostate , or colon cancer : patient and provider perspectives . 
faller h , schuler m , richard m et al ( 2013 ) effects of psycho - oncologic interventions on emotional distress and quality of life in adult patients with cancer : systematic review and meta - analysis . 
kirchheiner k , nout r , lindegaard j et al ( 2012 ) do clinicians and patients agree regarding symptoms ? a comparison after definitive radiochemotherapy in 223 uterine cervical cancer patients . 
lehmann c , koch u , mehnert a ( 2009 ) die bedeutung der arzt - patient - kommunikation fr die psychische belastung und die inanspruchnahme von unterstutzungsangeboten bei krebspatienten . 
mehnert a , koch u ( 2008 ) psychological co morbidity and health - related quality of life and its association with awareness , utilization , and need for psychosocial support in a cancer register - based sample of long - term breast cancer survivors . 
mehnert a , mller d , lehmann c et al ( 2006 ) die deutsche version des nccn distress - thermometers : empirische prfung eines screening - instruments zur erfassung psychosozialer belastung bei krebspatienten . 
neumann m , galushko m , karbach u et al ( 2010 ) barriers to using psycho - oncology services : a qualitative research into the perspectives of users , their relatives , non - users , physicians , and nurses . 
sieverding m , matterne u , ciccarello l ( 2010 ) what role do social norms play in the context of mens cancer screening intention and behavior ? application of an extended theory of planned behavior . 
z med psychol 19 : 5159 strahlentherapieundonkologie72013 | mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 811812 doi 10.1007 / s00066 - 013 - 0423 - 1 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
20 , d - 65189 wiesbaden , e - mail : prott@bvdst.de jubilare die fachgesellschaften von strahlentherapie und onkologie gratulieren zum geburtstag : 28.09.2013 essen : wolfgang mller , 65 jahre 05.09.2013 berlin : hans j . 
habermalz , 75 jahre 06.09.2013 fockbek : siegfried gbel , 70 jahre 16.09.2013 oberursel : rolf eickel , 70 jahre 25.09.2013 berlin : almuth lessel , 80 jahre 13.09.2013 berlin : hans j . 
mechthild krause / dresden hat den ruf auf die w3 - professur fr translationale radioonkologie des partnerstandortes dresden des deutschen konsortium fr translationale krebsforschung ( dktk ) an der medizinischen fakultt und dem universittsklinikum carl gustav carus technischen universitt dresden angenommen und wurde am 27.06.2013 vom rektor des tu dresden in die professur eingefhrt . 
 die berufung erfolgte gemeinsam durch die medizinische fakultt und das universittsklinikum carl gustav carus der technischen universitt dresden und dem deutschen krebsforschungszentrum ( dkfz ) in heidelberg und dem deutschen konsortium fr translationale krebsforschung ( dktk ) , vertreten durch das dkfz . 
 frau krause leitet zuknftig den neu etablierten bereich translationale radioonkologie des partnerstandorts dresden des dktk , der mit den gleichnamigen bereichen der dresdner klinik fr strahlentherapie und radioonkologie , des oncoray nationalen zentrums fr strahlenforschung in der onkologie und des instituts fr radioonkologie des helmholtzzentrum dresden - rossendorf zusammengefhrt wird . 
hypofractionated concepts have been increasingly used in the last decade [ 2 , 3 ]  . the application of a spacer to increase the distance between the prostate and the anterior rectal wall is an innovative technique that helps protect the rectal wall effectively . 
hyaluronic acid , collagen , an inflatable biodegradable balloon , and hydrogel are potential materials to create the desired effect [ 4 , 5 , 6 , 7 , 8 , 9 ]  . 
the space between the prostate and the anterior rectal wall is well accessible via a perineal approach and transrectal ultrasound ( trus ) guidance [ 9 ]  . treatment planning studies , studies evaluating spacer stability over several weeks , and studies evaluating toxicity and quality of life after radiotherapy for localized prostate cancer with a hydrogel spacer have been published recently [ 10 , 11 , 12 , 13 ]  . 
randomized studies using hydrogel are currently recruiting patients , exploring the effects of photon and hypofractionated proton or carbon ion radiation [ 13 ]  . imaging for treatment planning shortly after hydrogel injection is optimal for practical purposes , reducing the number of appointments for the patient . 
the aim of this study was to evaluate the actual difference between early and late imaging for spacer dimensions and the treatment plan . patients and methods injection of 10 ml spacer gel ( spaceoar system , augmenix inc . , waltham , ma , usa ) was performed under trus guidance via the transperineal approach after dissecting the space between the prostate and rectum with a saline / lidocaine solution . 
treatment planning computed tomography ( ct ) was performed within 1 h after hydrogel injection in 3 patients ( ct1 ) and 12 weeks after injection ( ct2 ) for comparison . 
all patients ( n = 3 ) had intermediate - risk localized prostate cancer with a biopsy gleason score of 7 and psa levels of < 10 ng / ml without neoadjuvant hormonal therapy . 
one of the patients received high - intensity focused ultrasound ( hifu ) therapy before presenting at our department for definitive radiotherapy . hydrogel dimensions were determined in ct1 and ct2 . 
anteriorposterior ( ap ) dimensions were measured at the level of the prostate base ( third most superior slice ) , middle , and apex ( third most inferior prostate slice ) in the midsagittal plane . patients were asked to have a full bladder for the planning ct scans . 
 for the planning target volume ( ptv ) , 8 - mm lateral and anterior , 5 - mm superior and inferior , and 4 - mm posterior margins were added . a total dose of 78 gy was prescribed to the ptv in 2 - gy fractions with 15mev photons and a five - field imrt technique . 
objectives and constraints were based on rtog ( radiation therapy oncology group ) recommendations [ 14 ] : maximum rectum v50 = 50% , maximum rectum v70 = 20% ; maximum bladder v55 = 50% , maximum bladder v70 = 30% . 
 the direct machine parameter optimization ( dmpo ) algorithm was applied for inverse planning with a 4 - cm2 minimum segment area , 5 minimum segment monitor units , and a maximum number of 70 segments . 
 [ 18 ] for grade 2 or 3 rectal bleeding were applied . results a mean planning treatment volume of 104 cm3 ( 82128 cm3 ) resulted for a prostate volume of 37 cm3 ( 2552 cm3 ) in ct1 and 39 cm3 ( 2356 cm3 ) in ct2 . 
.fig.1 shows the hydrogel distribution for a patient , demonstrating a decreasing hydrogel volume , the presence of air bubbles and edema in ct1 in contrast to ct2 . planning constraints were met in all plans . 
the mean v70 and v50 for the rectum including hydrogel volume were 10% ( 913% ) and 29% ( 2334% ) in ct1 and 9% ( 413% ) and 28% ( 2040% ) in ct2 . 
the mean ntcp for severe proctitis , necrosis , fistula , or rectal bleeding was calculated to be 0% in ct1 and ct2 for all plans with the exception of 1 patient in ct2 ( 1% )  . 
the mean ntcp for grade 2 rectal bleeding was found to be 0% in ct1 and ct2 with the exception of 2 patients in ct2 ( 1% , respectively )  . 
1 8 hydrogel distribution on axial ct slices at the prostate base , middle , and apex shortly after ( ct1 ) and 1 week after ( ct2 ) hydrogel injection shifted accordingly , simulating a table adjustment of an igrt treatment . the equivalent uniform dose ( eud ) is defined as the biologically equivalent dose that , if given uniformly , will lead to the same effect in the tumor volume or the normal tissues as the actual nonuniform dose distribution . 
in this expression , n is the number of voxels in the anatomic structure of interest , di is the dose in the ith voxel , and a is the tumor or normal tissue - specific parameter that describes the dosevolume effect . 
treatment planning based on imaging shortly after hydrogel injection overestimates the actual hydrogel volume during the treatment as a result of not - yet - absorbed saline solution and air bubbles . keywords prostate neoplasm conformal radiotherapy intensity - modulated radiotherapy treatment planning spacer gel behandlungsplanung nach hydrogelinjektion whrend strahlentherapie beim prostatakarzinom zusammenfassung hintergrund . 
die auf einer bildgebung kurz nach der hydrogelinjektion basierende bestrahlungsplanung berschtzt das tatschlich whrend der behandlung vorhandene hydrogelvolumen infolge noch nicht absorbierter kochsalzlsung und luftblasen . schlsselwrter prostatakarzinom konformale strahlentherapie intensittsmodulierte strahlentherapie bestrahlungsplanung abstandshalter discussion the advantage of placing a spacer between the prostate and anterior rectal wall has already been shown in several studies . 
the effects of a hydrogel spacer on dose distribution were initially demonstrated in a cadaver study [ 12 ] and subsequently in clinical studies [ 11 , 19 ]  . 
 a separation of the prostate and rectum of > 7.5 mm and a reduction of the rectum volume within the 70 - gy isodose ( v70 ) was shown to be possible in more than 90% of cases [ 11 ]  . 
the rectum v70 could be reduced by more than 50% in comparison to plans without a spacer for the same patients , applying three - dimensional conformal or imrt techniques . 
 the mean ntcp for severe proctitis , necrosis , fistula , or rectal bleeding was also shown to be over 50% lower [ 19 ]  . the rtog constraints for inverse treatment planning are usually considered in our department [ 14 ]  . 
eud - based constraints are increasingly implemented in the planning process in our department , considering the specific association with 798 | strahlentherapieundonkologie92013 rectum ct1 rectum with hydrogel ct1 rectum ct2 rectum with hydrogel ct2 dose / gy fig . 
2 9 dosevolume histogram for the rectum and the rectum with hydrogel volume ( relevant for treatment planning ) toxicity for an organ and affecting the entire dosevolume histogram curve . the aim of this study was to evaluate the actual difference between early and late imaging for spacer dimensions and the treatment plan . 
 in contrast to the base level , there is less space for the fluid to disperse , with a tight restriction by the rectourethralis muscle inferiorly and levator ani muscle laterally . 
the mixing of the diluent solution and accelerator solution is accomplished as the materials pass through the y - connector before passing through the injection needle . the dimensions and displacement of hydrogel during radiotherapy have been analyzed in a recent study [ 8 ]  . 
the mean hydrogel volume increased only slightly ( 17% when comparing imaging before treatment with imaging in the last week of treatment , in 4 of 15 patients > 2 cm3 ) , predominantly at the base ( fewer anatomic space restrictions )  . 
 thus , hydrogel dimensions are representative of the complete treatment if a period of at least 3 days is allowed between injection and imaging . since the injected hydrogel volume is currently 10 ml , the contoured hydrogel volume in the treatment plan has to be around 10 cm3 in a plausible plan . 
larger volumes are associated with larger stress on the rectal wall , and thereby most probably more problems for the patients , for example , tissue damage or increased rectal urgency . 
on the other hand , a volume of 10 ml already ensures a distance of about 1 cm between the prostate and anterior rectal wall and avoids an overlap of the ptv and rectum volume in the majority of cases . 
among long - term survivors of gi cancers , development of diabetes mellitus ( dm ) is not infrequent and often poses a significant problem during the surveillance period . dm as a complication that occurs after pancreatic surgery for chronic pancreatitis is common and has been reported with a prevalence of 1036% in several series [ 1 , 2 , 3 ]  . 
however , clinical data regarding the incidence of dm in cancer patients who had undergone radiotherapy following pancreaticoduodenectomy ( pd ) or pylorus - preserving pancreaticoduodenectomy ( pppd ) are not readily available and as a consequence , predictive factors for the development of posttreatment dm are not yet defined . radiotherapy is responsible for functional deterioration of normal tissue depending on the prescribed dose and targeted volume . 
in patients with lung cancer , some dosevolumetric factors such as percentage of volume receiving specific dose ( i.e. , v20 and v30 ) or mean lung dose are predictive of radiation pneumonitis risk [ 4 , 5 , 6 , 7 ]  . 
in head and neck cancer , sparing the parotid gland from excessive radiation exposure may spare some salivary function and help avoid treatment - related xerostomia to a certain degree [ 8 , 9 , 10 , 11 ]  . 
it is reasonable to infer from these facts that certain dosevolumetric parameters might play a role in the development of dm after postoperative radiotherapy . herein , we analyzed dosevolumetric factors affecting the development of posttreatment dm in long - term survivors of upper gi cancers , who had postoperative chemoradiotherapy ( crt ) following pd or pppd . patients and methods we retrospectively reviewed medical records of patients with upper gi cancer including pancreatic cancer , common bile duct cancer , ampulla of vater cancer , or duodenal cancer who underwent postoperative crt following pd or pppd between january 2006 and december 2008 . we selected all patients who were regularly followed for at least 2 years in order to allow sufficient time for the development of dm , which was defined according to american diabetes association recommendations [ 12 ]  . 
repetitive blood tests measuring the fasting plasma glucose level and / or plasma glucose level after oral glucose tolerance test were performed before the diagnosis of dm . a total of 175 patients had undergone postoperative crt for upper gi cancers during the accrual period . 
in all , 63 patients were excluded as they were followed for less than 2 years , mainly due to disease relapse for 56 patients , and loss to followup for 7 patients . 
2 9 receiver operating characteristic ( roc ) curve of the development of diabetes mellitus for v50 and dmax treatment methods neoadjuvant chemotherapy was given to 14 patients ( 33.3% ) with pancreatic cancer . 
postoperative crt was performed in 67 weeks with a median dose of 50.4 gy ( range 50.459.4 gy ) using three - dimensional conformal radiotherapy ( 40 / 42 patients , 95% ) or intensity - modulated radiotherapy ( 2 / 42 patients , 5% )  . 
patients with clear resection margin were given a total of 50.4 gy in 28 fractions , while the others ( 9 / 42 patients ) with close or positive margins were given an additional dose of 3.69 gy to the tumor bed . 
 four to six cycles of chemotherapy using gemcitabine ( 14 patients , 33.3% ) or 5 - flu754 | strahlentherapieundonkologie92013 orouracil ( 18 patients , 42.9% ) were given after crt . dosevolumetric parameters the preoperative pancreatic volume was determined from preoperative triphasic ct scans with 3or 5 - mm thickness using osiris software ( digital imaging unit , university hospital of geneva , geneva , switzerland )  . 
the non - tumor pancreatic volume was defined by subtracting tumor volume obtained in pathologic specimen ( equation for calculation : volume = 1 / 6 width length height ) , from the preoperative pancreatic volume . 
the receiver operating characteristic ( roc ) curve was used to calculate the area under curve ( auc ) and to determine the cut - off value of tested parameters . 
medical records of patients who underwent postoperative crt following curative resection , either pancreaticoduodenectomy ( pd ) or pylorus preserving pancreaticoduodenectomy ( pppd ) for upper gi cancers including pancreas , biliary , ampullary , and duodenal cancers , between january 2006 and december 2008 were retrospectively reviewed . 
v50 was the only independent factor associated with the development of diabetes and may function as guideline to predict the development of dm in patients receiving crt following curative resection . keywords radiotherapy diabetes mellitus pancreatic volume radiation dose parameters postoperative chemoradiotherapie nach pankreatikoduodenektomie . 
die krankenakten von patienten , die sich zwischen januar 2006 und dezember 2008 einer crt gefolgt von einer kurativen resektion , entweder ei ner duodenopankreatektomie ( pd ) oder einer pyloruserhaltenden duodenopankreatektomie ( pppd ) , wegen krebserkrankungen im oberen verdauungstrakt , einschlielich bauchspeicheldrsen - , bilirem , ampullenund duodenal - karzinomen , unterzogen haben , wurden retrospektiv begutachtet . 
v50 war der einzige unabhngige faktor , der mit der entwicklung von dm assoziiert war und als richtschnur angesehen werden kann , mit deren hilfe das entstehen von dm bei patienten , die nach kurativer resektion mit crt behandelt wurden , vorhergesagt werden kann . schlsselwrter strahlentherapie diabetes mellitus pankreasvolumen strahlendosis parameter in all , 8 patients were diagnosed of dm after postoperative crt . 
as for the primary site , although the difference was not statistically significant between the groups , pancreatic cancers were more common in the non - diabetic group , while common bile duct ( cbd ) cancers were more frequent in the diabetic group . 
 in addition , development of local or regional recurrence during follow - up was not different . dosevolumetric parameters and diabetes mellitus the relationship between dosevolumetric parameters and development of dm are shown in .tab.2. 
 when the mean dose , minimum dose , and maximum dose ( dmax ) to remnant pancreatic volume were analyzed , dmax was significantly associated with the destrahlentherapieundonkologie92013 | original article tab . 
in the current study , despite aggressive treatment modalities including the use of crt and adjuvant chemotherapy , the overall incidence of new onset dm after treatment was 19% with a median follow - up duration of 40 months , which is consistent with historical controls . although the mechanism of developing dm is complex , exposure to radiation can be a possible cause . 
small animal studies showed that pancreatic irradiation results in vacuolization , mitochondrial destruction , reduction of - cell number , and impaired insulin secretion [ 22 , 23 ]  . 
3 8 kaplanmeier curve for the development of diabetes mellitus stratified by a v50 ( p = 0.013 ) and b dmax ( p = 0.031 ) the number of cells , which resulted in the impairment of insulin - secreting ability . 
 [ 23 ] reported pancreatic atrophy and fibrosis in beagle dogs after 25 gy of intra - operative radiotherapy ( iort ) and 50 gy of external beam radiotherapy , suggesting a doseresponse relationship between pancreatic damage and radiation dose of iort . 
these findings are also consistent with our results in that parameters representing pancreatic exposure to high - dose radiation , such as v50 and dmax , were significant predictors for the development of dm . clinical studies [ 24 , 25 ] focusing on the relationship between dm and radiation dose have demonstrated that abdominal irradiation is a factor strongly associated with the development of dm . 
 [ 24 ] demonstrated an increased risk of dm [ odds ratio 2.7 , 95% confidence interval ( ci ) 1.93.9 , p < 0.001 ] in childhood cancer survivors who had abdominal irradiation , compared with their siblings . 
another study [ 25 ] showed increased risk of diabetic death with an odds ratio of 3.79 ( 95% ci 1.212.0 ) when the pancreas is exposed to radiation ranging from 1638 gy . 
in the current study , dosevolumetric analyses revealed that v50 was the only independent factor predicting the development of dm with sensitivity of 0.875 , whereas dmax with identical sensitivity value showed borderline significance with multivariate analysis . after major pancreatic resection , a clear relationship between remnant volume and function of pancreas was reported by yasugi et al . 
in the current study , among the 20 patients with less than 70% of pancreatic tissue removed , 5 patients ( 25% ) had developed dm ( data not shown )  . 
unfortunately , remnant pancreatic volume , which may possibly be a strong predictor for dm , did not show a significant relationship with dm in the current study . results of the present study , especially cut - off values of dmax and v50 , should not be readily applied to patients undergoing postoperative radiotherapy alone , considering the possible effect of concomitant chemotherapy . 
meacham lr , sklar ca , li s et al ( 2009 ) diabetes mellitus in long - term survivors of childhood cancer : increased risk associated with radiation therapy : a report for the childhood cancer survivor study . 
cameron aj , welborn ta , zimmet pz et al ( 2003 ) overweight and obesity in australia : the 1999 2000 australian diabetes , obesity and lifestyle study ( ausdiab )  . 
several risk factors such as age at diagnosis , bmi , gender , race , household income , and physical activity are known to be associated with the development of dm [ 27 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 809810 doi 10.1007 / s00066 - 013 - 0420 - 4 online publiziert : 3 . 
im studienarm mit induktionschemotherapie ( ict ) bekamen sie zunchst 3 zyklen des klassischen tpf - schemas ( 75 / 100 / 1000 ) , gefolgt von einer rct entweder mit docetaxel wchentlich fr patienten in schlechtem allgemeinzustand oder carboplatin wchentlich bei besserem befinden zur bestrahlung mit 7072 gy , teilweise mit konkomitantem boost . 
die autoren berlassen dem kliniker die entscheidung zwischen ict mit rct und einer alleinigen rct , da sie keinen unterschied im berleben zwischen beiden gruppen feststellen konnten . kommentar das berraschende an der endgltigen verffentlichung der daten nach ihrer vorstellung auf der jahrestagung der asco 2012 ist deren kaum nachvollziehbare bewertung und die schlussfolgerung der autoren fr die praxis . 
ist es wirklich ethisch vertretbar , eine toxische therapie wie die ict , die ohne zustzlichen nutzen fr die patienten ist , zu verordnen ? wesentliche vernderungen der ergebnisse wren auch bei mehr patienten in der studie schwerlich zu erwarten gewesen . woher rhrt diese niemals enden wollende vorliebe der internistischen onkologen fr eine intensive chemotherapeutische vorbehandlung ? die rationale fr dosisintensive ict wird schlssig vorgetragen . 
gleichzeitig ist es ein fakt , dass die lokale rezidivrate nach icd deutlich verbessert wird , wie es sich in den tax - studien zeigte [ 7 , 10 ]  . 
forastiere , die damals verglichen wurde mit einer pf - induktionstherapie gefolgt von einer radiotherapie , nur die lokale kontrolle verbessert und das berleben unbeeinflusst gelassen [ 3 ]  . 
die hittstudie sollte bei der bewertung auen vor bleiben , weil ihre nachbeobachtungszeit unter 2 jahren liegt und die populationsdaten im jahre 2009 nur unvollstndig erhoben und bewertet worden waren . aus den 3 anderen studien ergibt sich ein bild , die quo ad vitam keinen zusatznutzen fr eine induktionstherapie belegen . 
alleinig die grte studie beschreibt eine halbierung der fernmetastasierungsrate von 19% auf 10% nach 3 jahren , was in der grenordnung der tax - 324 - studie liegt [ 7 ]  . das eine hauptproblem von induktionstherapie sind die nebenwirkungen , die fr die remission in kauf genommen werden mssen . 
als parameter einer langfristigen toxizitt fanden sich tendenziell mehr nichttumorbedingte todesflle mit der langwierigen ict als whrend der rct in der decide - studie . zudem sind die tumoren trotz vermehrung der verschiedenen zytostatika und der exorbitanten dosen lokal nicht besser unter kontrolle zu bringen : prolongation der gesamttherapie und die postponierung der radiotherapie sind die begrndenden stichworte . 
bereits in der tax - 324 - studie war die gesamtbehandlungszeit der prognostische faktor , die nicht durch die rct mit carboplatin verursacht worden war , sondern allein durch die dauer der induktionstherapie [ 9 ]  . 
ben - josef e , moughan j , ajani ja et al ( 2010 ) impact of overall treatment time on survival and local control in patients with anal cancer : a pooled data analysis of radiation therapy oncology group trials 87 - 04 and 98 - 11 . 
cohen ew , karrison t , kocherginsky m et al ( 2012 ) decide : a phase iii randomized trial of docetaxel ( d ) , cisplatin ( p ) , 5 - fluorouracil ( f ) ( tpf ) induction chemotherapy ( ic ) in patients with n2 / n3 locally advanced squamous cell carcinoma of the head and neck ( scchn )  . 
haddad r , oneill a , rabinowits g et al ( 2013 ) induction chemotherapy followed by concurrent chemoradiotherapy ( sequential chemoradiotherapy ) versus concurrent chemoradiotherapy alone in locally advanced head and neck cancer ( paradigm ) : a randomised phase 3 trial . 
hitt r , grau jj , lopez - pousa a et al ( 2009 ) final results of a randomized phase iii trial comparing induction chemotherapy with cisplatin / 5 - fu or docetaxel / cisplatin / 5 - fu follow by chemoradiotherapy ( crt ) versus crt alone as first - line treatment of unresectable locally advanced head and neck cancer ( lahnc )  . 
paccagnella a , ghi mg , loreggian l et al ( 2010 ) concomitant chemoradiotherapy versus induction docetaxel , cisplatin and 5 fluorouracil ( tpf ) followed by concomitant chemoradiotherapy in locally advanced head and neck cancer : a phase ii randomized study . 
semrau s , schmidt d , lell m et al ( 2013 ) results of chemoselection with short induction chemotherapy followed by chemoradiation or surgery in the treatment of functionally inoperable carcinomas of the pharynx and larynx . 
sher dj , posner mr , tishler rb et al ( 2011 ) relationship between radiation treatment time and overall survival after induction chemotherapy for locally advanced head - and - neck carcinoma : a subset analysis of tax 324 . 
however , based on the background of several analyses of neoadjuvant chemoradiation for locally advanced non - metastasized disease that is unresectable in a curative setting , downsizing of the tumor in a substantial number of patients may lead to secondary resectability : meta - analyses have shown that approximately 30%40% of locally irresectable patients can undergo secondary resection , which significantly improves outcome [ 1 ]  . 
we recently reported that 26% of patients with tumors classified as irresectable show conversion into resectable tumors [ 2 ]  . over time , improvements in radiation techniques have enabled the radiation oncologist to reduce dose exposure to normal tissue and to focus high doses to the defined treatment volumes . 
with intensity modulated radiotherapy ( imrt ) , dose delivery to even complex anatomical structures at very close vicinity to organs at risk ( oar ) became possible ; therefore , the clinical use of imrt has been demonstrated for several tumor entities . 
for tumors of the gastrointestinal ( gi ) tract , beneficial dose distributions with imrt have been published in particular for esophageal , stomach , and anal cancer [ 3 , 4 , 5 , 6 , 7 , 8 , 9 , 10 , 11 , 12 ]  . 
for tumors of the pancreatico - biliary region , early data on toxicity have shown a reduction of dose by implementing imrt compared to 3d radiotherapy for oar such as liver , kidneys , stomach , and the small bowel [ 13 ]  . 
 [ 14 ] supported this hypothesis , demonstrating a significantly reduced rate of upper and lower gi toxicity among patients treated for pancreatic / ampullary tumors with imrt in chemoradiation protocols . 
early reports on imrt for pancreatic cancer have focussed either on adjuvant treatment after surgical resection , or its use as a neoadjuvant treatment in patients with locally advanced disease [ 15 , 16 ] ; prospective clinical trials are currently recruiting patients . several groups have shown in plan comparisons that imrt may reduce dose to oar . 
therefore , in the present work we focussed on outcome analysis after imrt compared to our previously published data on 3d - conformal rt ( 3d - rt ) in patients with lapc treated with rt and chemotherapy as neoadjuvant treatments . 
we compared failure patterns , toxicity , and outcome in our established cohort to define differences between standard and more advanced radiation techniques . patients and methods between 2004 and 2010 , 89 patients were treated and prospectively followed within a tight clinical follow - up program with imrt as neoadjuvant chemoradiation for pancreatic cancer . 
of these , 26 patients were treated within the parc study protocol as neoadjuvant treatment in locally advanced tumors and were therefore excluded from this analysis [ 17 ]  . 
patient characteristics of 57 patients with locally advanced pancreatic cancer treated with imrt and concomitant chemotherapy characteristics gender male female median ( range ) tumor location head head and body body body and tail tail head , body , tail body weight prior to imrt 1 . 
of the remaining patients in which no histological confirmation was obtained prior to treatment , 16 / 57 ( 28% ) patients were confirmed during the course of the disease with ductal adenocarcinoma . 
patient characteristics are shown in .tab.1. treatment planning and radiation therapy for treatment planning , contrast - enhanced ct scans were performed in a supine position in individual fixation including vacuum bags or knee - foot rests . 
 target volume delineation was performed using the siemens oncologist system ( siemens , erlangen , germany ) or the masterplan treatment planning system ( elekta , stockholm , sweden )  . 
two clinical target volumes ( ctv ) were defined : ctv_baseplan included the gtv plus surrounding lymph nodes and areas of lymphatic spread adding about 23 cm in all directions ; for the ctvboost , a margin of 0.5 mm - 1 cm was added to the gtv . 
a planning target volume ( ptv ) was added depending on the treatment machine and patient setup of 35 mthe median ptv_baseplan was 415 ml ( range 218 1121 ml ) , and the median ptv_boost was 120 ml ( range 20431 ml )  . 
treatment planning was performed using the virtuos treatment planning system ( dkfz , heidelberg , germany ) , siemens oncologist software , or tomotherapy planning software ( madison , us )  . 
patients were either treated with step - and - shoot imrt using between seven and nine intensitymodulated beams at a 6 - mv siemens accelerator , or by helical tomotherapy . 
a median total dose of 45 gy to the ptv_baseplan and 54 gy to the ptv_ boost in single doses of 1.8 gy for the ptv_ baseplan and median single doses of 2.2 gy in the ptv_boost was applied . intraoperative radiotherapy ( iort ) was performed on the basis of individual decision - making between the radiation oncologist and the surgeon depending on patient characteristics , resection status , as well as the technical availability of iort . 
 thus , iort was conducted in 11 patients with doses of 10 gy in one , 12 gy in two , and 15 gy in eight patients . chemotherapy in 56 patients ( 98% ) , concomitant gemcitabine ( gem ) was applied at a dose of 300 mg / m2 weekly , followed by full - dose gem cycles . 
for the present evaluation , all cases were re - evaluated to confirm pathological diagnosis as well as resection status . comparison with 3d - treated patient cohort outcomes of the 57 imrt - treated patients was compared to our institutional 3d - treated cohort of patients published previously [ 18 ]  . 
overall survival , progression - free survival , secondary respectability , and toxicity were compared . strahlentherapieundonkologie92013 | abstract zusammenfassung strahlenther onkol 2013 189 : 738744 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0391 - 5 s.e.combsd.habermehlk.kesself.bergmannj.werneri.brechtp.schirmacherd.jgerm.w.bchlerj.debus intensity modulated radiotherapy as neoadjuvant chemoradiation for the treatment of patients with locally advanced pancreatic cancer . 
a median total dose of 45 gy to the ptv_baseplan and 54 gy to the ptv_boost in single doses of 1.8 gy for the ptv_baseplan and median single doses of 2.2 gy in the ptv_boost were applied . 
a significant impact on overall survival could only be observed for a decrease in ca 19 - 9 during treatment , patients with less pre - treatment ca 199 than the median , as well as weight loss during treatment . 
in the future , the improved dose distribution , as well as advances in image - guided radiotherapy ( igrt ) techniques , may improve the use of imrt in local dose escalation strategies to potentially improve outcome . keywords intensity modulated radiotherapy locally advanced pancreatic cancer neoadjuvant treatment toxicity 3d conformal radiotherapy intensittsmodulierte radiotherapie als neoadjuvante radiochemotherapie zur behandlung von patienten mit lokal fortgeschrittenem pankreaskarzino ergebnisanalyse und vergleich mit einer patientenkohorte mit 3 - d - strahlentherapie zusammenfassung hintergrund . 
eine mediane gesamtdosis von 45 gy auf das geplante zielvolumen , ptv_baseplan , und 54 gy auf das ptv_ boost in einzeldosen von 1 , 8 gy fr ptv_baseplan und mediane einzeldosen von 2 , 2 gy auf das ptv_boost wurden appliziert . 
als signifikanter einflussfaktor auf das gesamt berleben wurden lediglich die abnahme des ca 19 - 9 unter therapie , ein niedrigeres ca 19 - 9 als der median vor therapie sowie der gewichtsverlust whrend der therapie identifiziert . 
in zukunft knnten jedoch eine verbesserte dosisverteilung sowie fortschritte in der bildsteuerung als image - guided radiotherapy ( igrt ) den einsatz der imrt fr strategien zur dosiseskalation optimieren . schlsselwrter intensittsmodulierte strahlentherapie lokal fortgeschrittenes pankreaskarzinom neoadjuvante therapie toxizitt 3 - dkonformale strahlentherapie follow - up and outcome assessment an evaluation of treatment response and an assessment of resectability were performed 26 weeks after completion of radiochemotherapy and after one cycle of full - dose gem . 
in most patients , contrastenhanced ct or magnetic resonance imaging ( mri ) was conducted ; additionally , follow - up visits included clinical examination as well as tumor marker analysis . 
in cases of stable disease but non - resectability , full - dose gem was continued and re - assessment of the tumor status was scheduled on a regular basis . overall survival was calculated from the first day of irradiation until death . 
comparison of resection status ( no resection / r2 ) , r1 resection , and complete resection had no impact on overall survival ( b ; p = 0.09 ) mented to compare survival curves evaluating the association between clinical variables of interest and survival . 
all calculations were performed using the statistical software program statistica 6.1 ( statsoft , germany )  . results overall treatment was well tolerated in all patients and imrt could be completed without interruption . adverse effects included hematological toxicity associated with chemotherapy in 27 patients ( 47% ) , which consequently lead to individual adjustment or interruption of chemotherapy ; thus , chemotherapy was administered with a median of five concomitant administrations ( ranging between three and six ) , depending on hematological toxicity . 
the median value directly prior to imrt was 269.7 u / ml ( range 3.34382 u / ml ) , and 122.8 u / ml ( range 3.72182 u / ml ) at initial follow - up . 
4 9 comparison of toxicity rates between 3dand imrttreated patient groups dian decrease of 105.6 u / ml was observed of ca 19.9. clinical and imaging staging for local re - evaluation of resectability revealed stable disease ( sd ) in most patients ( 50 patients , 88% ) , local progressive disease ( pd ) in three patients ( 5% ) , and partial remission ( pr ) in four patients ( 7% )  . during follow - up , the most predominant areas of metastatic disease were the liver , peritoneum , lung , and lymph nodes . 
due to intraoperative extension of the tumor , as well as metastases to the liver and / or peritoneum only visible during surgery , only an explorative laparotomy could be conducted in 17 patients . 
of the remaining patients , 14 were resected : r0 resection was possible in four patients , r1 resection in nine patients , and in one patient the resection status was rx . 
other factors such as gender ( p = 0.49 ) , resection status ( p = 0.09 ) , administration of iort ( p = 0.7 ) , or age ( p = 0.5 ) did not significantly impact survival . 
overall survival with respect to resection status is shown in .fig.2b. progression - freesurvival overall local progression - free survival was 79% after 6 months , 39% after 12 months , and 13% after 24 months for the whole patient group . 
.fig.4 shows toxicity ( hematological , gi , nausea / vomiting and rates of cholangitis ) between the 3dand imrt - treated cohorts . discussion the use of imrt for patients with lapc in the neo - adjuvant setting leads to comparable local control to 3d - rt without an increase in the local recurrence rate ( due to marginal or out - field failure as a consequence of different dose distributions outside the ptv )  . 
previous plan comparative studies have shown that adverse effects to the gi tract , as well as sparing of kidneys and other oar , can be improved with imrt , potentially contributing to improved quality of life ( qol ) , which is currently under evaluation in prospective clinical trials [ 16 , 19 , 20 , 21 ]  . 
additionally , dose escalation strategies can be explored in combination with igrt approaches [ 20 ]  . in general , the clinical benefit of neoadjuvant radiochemotherapy for lapc has been shown by several different groups . 
while surgical resection remains the primary treatment of choice , in over 80% of all patients surgery alone may not lead to long - term tumor control due to infiltration of oar , nerves , and blood vessels [ 22 , 23 ]  . 
the predominant prognostic factors for outcome include resection status , the presence of lymph node metastases , tumor size , and tumor dna content [ 24 , 25 , 26 , 27 ] ; with respect to resection status , only r0 resection seems to provide a major benefit as compared to r1 or r2 resection . 
therefore , strategies to increase the likelihood of complete resection may provide a significant outcome benefit ; in non - resectable or borderline resectable patients , alternatives to radical surgery therefore need to be evaluated . in the past , chemotherapy alone was administered , using substances such as gem or 5 - fu . 
chemoradiation has shown beneficial results with acceptable toxicity : a gitsg study initially defined the role of radiation and chemotherapy with bolus 5 - fu , comparing split - course radiotherapy with 40 gy with chemotherapy to radiation with 60 gy in combination with chemotherapy or radiation alone . 
gem has also been used as a radiation sensitizer in pancreatic cancer [ 29 , 30 , 31 , 32 , 33 ] ; a number of comparative investigations have shown that gem and radiation seem to be equally effective to 5 - fu and radiation [ 34 , 35 ]  . 
there is evidence that the rate of tumor - free resection margins can be increased by preoperative chemoradiation [ 38 ] , even if to date no randomized trial has supported this hypothesis . advanced techniques have lead to improved dose conformality and sparing of normal tissue ; in this respect , imrt through the application of individuallyformed , internally dose - modulated beams has significantly helped increase the therapeutic window with respect to local control ( through possible increase in doseto - target ) and reduce adverse effects ( by sparing normal tissue / oar )  . 
 [ 14 ] in a comparative setting with 3d - rt : the incidence of grade - iii to - iv nausea and vomiting was reduced from 11% to 0% , and for diarrhea from 18% to 3% ; although weight loss was comparable in both groups , this was more related to the tumor itself than to rt . 
the same group reported comparable recurrence patterns in 3d - rt and imrt [ 21 ]  . these results are supported by the present analysis , where outcome was compared to a previously published group of 3d - treated patients [ 18 , 39 ]  . 
additionally , we could show that ctv margins may be reduced in the dorsolateral region towards sensitive oar such as the kidneys , since this region is less likely to be affected by local tumor recurrence [ 40 ]  . 
gillen s , schuster t , meyer zum bc et al ( 2010 ) preoperative / neoadjuvant therapy in pancreatic cancer : a systematic review and meta - analysis of response and resection percentages . 
girard n , mornex f , bossard n et al ( 2010 ) estimating optimal dose of twice - weekly gemcitabine for concurrent chemoradiotherapy in unresectable pancreatic carcinoma : mature results of gemrt - 01 phase i trial . 
shibuya k , oya n , fujii t et al ( 2010 ) phase ii study of radiation therapy combined with weekly lowdose gemcitabine for locally advanced , unresectable pancreatic cancer . 
mukherjee s , hurt cn , bridgewater j et al ( 2013 ) gemcitabine - based or capecitabine - based chemoradiotherapy for locally advanced pancreatic cancer ( scalop ) : a multicentre , randomised , phase 2 trial . 
haddock mg , swaminathan r , foster nr et al ( 2007 ) gemcitabine , cisplatin , and radiotherapy for patients with locally advanced pancreatic adenocarcinoma : results of the north central cancer treatment group phase ii study n9942 . 
pingpank jf , hoffman jp , ross ea et al ( 2001 ) effect of preoperative chemoradiotherapy on surgical margin status of resected adenocarcinoma of the head of the pancreas . 
kessel ka , habermehl d , bohn c et al ( 2012 ) database supported electronic retrospective analyses in radiation oncology : establishing a workflow using the example of pancreatic cancer . 
kessel ka , habermehl d , jger a , floca ro et al ( 2013 ) development and validation of automatic tools for interactive recurrence analysis in radiation therapy : optimization of treatment algorithms for locally advanced pancreatic cancer . 
golden dw , novak cj , minsky bd , liauw sl ( 2012 ) radiation dose 54 gy and ca 19 - 9 response are associated with improved survival for unresectable , non - metastatic pancreatic cancer treated with chemoradiation . 
ben josef e , shields af , vaishampayan u et al original article chemoradiation in patients with unresectable extrahepatic and hilar cholangiocarcinoma or at high risk for disease recurrence after resection : analysis of treatment efficacy and failure in patients receiving postoperative or primary chemoradiation . 
milano mt , garofalo mc , chmura sj et al ( 2006 ) intensity - modulated radiation therapy in the treatment of gastric cancer : early clinical outcome and dosimetric comparison with conventional techniques . 
milano mt , jani ab , farrey kj et al ( 2005 ) intensitymodulated radiation therapy ( imrt ) in the treatment of anal cancer : toxicity and clinical outcome . 
chandra a , guerrero tm , liu hh et al ( 2005 ) feasibility of using intensity - modulated radiotherapy to improve lung sparing in treatment planning for distal esophageal cancer . 
gomez dr , tucker sl , martel mk et al ( 2012 ) predictors of high - grade esophagitis after definitive three - dimensional conformal therapy , intensity - modulated radiation therapy , or proton beam therapy for non - small cell lung cancer . 
jiang zq , yang k , komaki r et al ( 2012 ) long - term clinical outcome of intensity - modulated radiotherapy for inoperable non - small cell lung cancer : the md anderson experience . 
lin sh , wang l , myles b et al ( 2012 ) propensity score - based comparison of long - term outcomes with 3 - dimensional conformal radiotherapy vs intensity - modulated radiotherapy for esophageal cancer . 
wang sl , liao z , liu h et al ( 2006 ) intensity - modulated radiation therapy with concurrent chemotherapy for locally advanced cervical and upper thoracic esophageal cancer . 
welsh j , gomez d , palmer mb et al ( 2011 ) intensity - modulated proton therapy further reduces normal tissue exposure during definitive therapy for locally advanced distal esophageal tumors : a dosimetric study . 
zhang x , zhao kl , guerrero tm et al ( 2008 ) fourdimensional computed tomography - based treatment planning for intensity - modulated radiation therapy and proton therapy for distal esophageal cancer . 
milano mt , chmura sj , garofalo mc et al ( 2004 ) intensity - modulated radiotherapy in treatment of pancreatic and bile duct malignancies : toxicity and clinical outcome . 
crane ch , winter k , regine wf et al ( 2009 ) phase ii study of bevacizumab with concurrent capecitabine and radiation followed by maintenance gemcitabine and bevacizumab for locally advanced pancreatic cancer : radiation therapy oncology group rtog 0411 . 
krempien r , muenter mw , huber pe et al ( 2005 ) randomized phase iistudy evaluating egfr targeting therapy with cetuximab in combination with radiotherapy and chemotherapy for patients with locally advanced pancreatic cancerparc : study protocol [ isrctn56652283 ]  . 
ben josef e , schipper m , francis ir et al ( 2012 ) a phase i / ii trial of intensity modulated radiation ( imrt ) dose escalation with concurrent fixed - dose rate gemcitabine ( fdr - g ) in patients with unresectable pancreatic cancer . 
howard tj , krug je , yu j et al ( 2006 ) a margin - negative r0 resection accomplished with minimal postoperative complications is the surgeons contribution to long - term survival in pancreatic cancer . 
moertel cg , frytak s , hahn rg et al ( 1981 ) therapy of locally unresectable pancreatic carcinoma : a randomized comparison of high dose ( 6000 rads ) radiation alone , moderate dose radiation ( 4000 rads + 5 - fluorouracil ) , and high dose radiation + 5fluorouracil : the gastrointestinal tumor study group . 
varadhachary gr , wolff ra , crane ch et al ( 2008 ) preoperative gemcitabine and cisplatin followed by gemcitabine - based chemoradiation for resectable adenocarcinoma of the pancreatic head . 
int j radiat oncol biol phys 68 : 801808 744 | strahlentherapieundonkologie92013 laudatio strahlenther onkol 2013 189 : 801802 doi 10.1007 / s00066 - 013 - 0422 - 2 online publiziert : 22 august 2013 springer - verlag berlin heidelberg 2013 t.wiegel1r.ptter2 1 klinik fr radioonkologie und strahlentherapie , universittsklinikum ulm 2 department of radiotherapy , comprehensive cancer center ( ccc ) , general hospital vienna ( akh wien ) , medical university vienna ( meduniwien ) , vienna prof.dr.wolfgang hinkelbeinzur emeritierung nach fast 20 - jhriger dienstzeit als direktor der klinik fr strahlentherapie und radioonkologie des campus benjamin franklin der charit universittsmedizin berlin ist wolfgang hinkelbein im alter von 65 jahren in den ruhestand getreten . 
1977 mit einem experimentellen thema am institut fr biophysik und strahlenbiologie der universitt freiburg begann er seine laufbahn in dem bereich , dem er ein langes berufsleben lang treu bleiben sollte , der radioonkologie . seine ausbildung fhrte ihn an der renommierten universittsklinik freiburg von 1978 bis 1984 durch die verschiedenen bereiche der strahlentherapie ( wannenmacher ) , der rntgendiagnostik ( wenz ) und der gynkologischen radiologie ( ladner ) mit abschluss 1983 als facharzt fr radiologie und 1984 als facharzt fr strahlentherapie . 
von 1984 bis 1995 war er oberarzt der abteilung fr strahlentherapie der universittsklinik freiburg , zunchst unter wannenmacher , nach dessen bernahme des lehrstuhls fr radioonkologie an der universitt heidelberg unter frommhold . 
im jahre 1989 habilitierte er sich mit dem thema optimierung der strahlenbehandlung fr eine tumoradaptierte behandlung experimentelle untersuchungen an menschlichen tumoren auf der thymusaplastischen nacktmaus und im koloniebildungstest und erhielt die venia legendi fr das fach strahlentherapie . 
1993 erhielt er den ruf auf den lehrstuhl fr strahlentherapie im fachbereich humanmedizin der freien universitt berlin , verbunden mit der leitung der klinik fr radioonkologie und strahlentherapie am universittsklinikum benjamin franklin ( ukbf )  . 
im rahmen der charit universittsmedizin ( fusion der standorte mitte , virchow - klinikum , benjamin franklin und buch ) war er seit 2003 bis zu seiner emeritierung direktor der klinik fr radioonkologie und strahlentherapie am campus benjamin franklin der charit . wolfgang hinkelbeins wissenschaftliche aktivitten sind vielfltig und betreffen das gesamte spektrum der radioonkologie . 
hervorzuheben ist weiterhin sein engagement in der uro - onkologie , hier insbesondere die etablierung der ersten wirklich interdisziplinren prostatakrebssprechstunde in deutschland , gemeinschaftlich mit kurt miller von der urologischen klinik des ukbf und seine ttigkeit in der leitkommission der deutschen s3 - leitlinie zum prostatakarzinom , die 2007 erstmals publiziert wurnational und international trat er als organisator zahlreicher wissenschaftlicher veranstaltungen hervor . 
hierunter fallen insbesondere die seit mehr als 25 jahren zweijhrlich stattfindenden alpbacher seminare mit kollegen aus sterreich und der schweiz , die ein spezielles themenspektrum beinhalten , welches ber die rein fachbezogenen fortbildungen hinausgeht . 
er war der initiator der berliner international symposia on special effects of radiotherapy , die zusammen mit der charit mitte seit mehr als 15 jahren regelmig abgehalten wurden und jeweils zu einem sonderband der reihe frontiers of radiation therapy and oncology im karger - verlag fhrten . 
2008 war er kongressprsident des gemeinschaftlichen kongresses der degro und gro in wien zusammen mit richard ptter aus wien . in seinem berufsleben wurden wolfgang hinkelbein zahlreiche wissenschaftstrahlentherapieundonkologie92013 | korrespondenzadresse t . 
ptter department of radiotherapy , comprehensive cancer center ( ccc ) , general hospital vienna ( akh wien ) , medical university vienna ( meduniwien ) waehringer guertel 18 - 20 , 1090 vienna sterreich richard.poetter@meduniwien.ac.at laudatio liche auszeichnungen verliehen . 
stellvertretend seien hier erwhnt der wilhelmkonrad - rntgenpreis der deutschen rntgengesellschaft ( 1990 ) , die medaille der medizinischen fakultt der freien universitt berlin sowie die ehrenmitgliedschaft der gro ( 2009 )  . 
common endpoints include symptom relief ( assessed by physicians or the patients themselves ) and survival rates . in terms of symptom relief , some rcts have shown hypofractionated treatment concepts to be equally as effective as or even superior to high - dose regimens [ 5 , 11 , 14 , 15 , 16 , 17 , 20 , 23 , 24 , 25 , 26 ] , while others favor a higher dose concept [ 3 , 7 , 10 ]  . 
 [ 23 ] compare a high - dose arm of 20 gy in 5 fractions with a low - dose arm of 16 gy in 2 fractions . overall survival results are also inconsistent , although the higher total dose concepts seem to be more beneficial [ 3 , 10 , 16 , 21 , 25 ]  . as a downside of higher total dose rt , the majority of trials name an increased number of side effectssuch as dysphagia [ 1 , 15 , 16 , 25 ] and conclude that lower total dose concepts are preferred in terms of rt - induced toxicities . 
in this analysis we have focused on overall survival to compare two palliative treatment concepts25 gy applied in 5 fractions and 50 gy applied in 20 fractionsboth of which are used in our department on a routine basis . patients and methods between 4 october 2004 and 5 september 2012 , two different palliative concepts were used to treat 219 patients with bronchial carcinomas . 
the indications for palliative treatment were stage iv disease or a lower disease stage plus a contraindication for curative treatment . patients mean age at the time of therapy was 69 years ( 4192 years )  . 
further patient characteristics are shown in .tab.1. the dose regimens used for therapy comprised a hypofractionated concept with a single dose of 5 gy , five times a week up to a total dose of 25 gy and a high total dose treatment concept with a single dose of 2.5 gy per fraction , five times a week up to a total dose of 50 gy . 
 the data of 12 reirradiated patients were excluded from the analysis . among the patients whose data was used for the survival analysis , a total of 126 were treated using the hypofractionated concept and 81 were treated with the high total dose regimen . 
patients were allocated to the different dose regimens at the discretion of the attending physician , according to performance status , the extent of distant metastasis and the feasibility of palliative chemotherapy after irradiation . the median follow - up for all patients was 20 weeks ( 19 weeks for patients treated with 25 gy ; 22 weeks for patients treated with 50 gy )  . of the 207 patients included in this study , 48 were still alive at the time of data analysis ( 35 patients treated with 25 gy ; 13 patients treated with 50 gy )  . a subgroup analysis was performed to analyze the effect of dose regimen on survival for patients with a goodfair vs . 
 this contouring strategy and the margins for the resultant planning target volume ( ptv ) were identical in both treatment groups . patients treated with sequential chemotherapy received platinum - based chemotherapy according to tumor histology . 
this interval was selected to ensure that possible rt side effects had disappeared before commencement of chemotherapy . for statistical analysis , kaplan meier curves were calculated to investigate the effect of treatment concept on survival . 
 all data were obtained using the spss package , version 20 ( spss inc . , chicago , il , usa )  . 772 | strahlentherapieundonkologie92013 results survival the median survival times from the beginning of rt were 21 weeks for patients treated with 25 gy in 5 fractions ( 95% confidence interval , ci ; range 16 26 weeks ) and 23 weeks ( 95% ci , range 14.531.5 weeks ) for patients treated with 50 gy in 20 fractions . 
in patients with a poor overall condition these values were 18 weeks ( 95% ci , range 14.521.5 weeks ) and 21 weeks ( 95% ci , range 13.029.0 weeks ) , respectively . 
as this is a retrospective analysis , patients were not ranabstract zusammenfassung strahlenther onkol 2013 189 : 771776 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0360 - z c.schrderm.ivoa.buchali does high - dose radiotherapy benefit palliative lung cancer patients ?  . 
the palliative treatment concept of 25 gy applied in 5 fractions is sufficient for radiation of lung cancer , given that there was no obvious survival improvement in patients treated with the higher total dose regimen . keywords performance status survival quality of life toxicity dysphagia profitieren palliativpatienten mit bronchialkarzinomen von therapiekonzepten mit hoher dosis ?  . 
die mediane berlebenszeit fr alle patienten betrug 21 wochen ( 95% ci 1626 wochen ) bei patienten , die mit 25 gy / 5 fraktionen behandelt wurden und 23 wochen ( 95% ci 14 , 531 , 5 wochen ) bei patienten , die mit 50 gy / 20 fraktionen behandelt wurden ( p = 0 , 334 )  . 
bei patienten mit gutem - mittleren allgemeinzustand betrug die mittlere berlebenszeit 30 wochen ( 95% ci 21 , 839 , 2 wochen ) fr 25 gy / 5 fraktionen und 28 wochen ( 95% ci 14 , 241 , 8 wochen ) fr 50 gy / 20 fraktionen ( p = 0 , 694 )  . 
 bei verwendung des bestrahlungskonzeptes mit einer hheren gesamtdosis von 50 gy war keine verlngerung der mittleren berlebens zeit nachzuweisen . schlsselwrter performance - status berleben lebensqualitt toxizitt dysphagie domized before treatment . 
 nevertheless , this result is largely consistent with reports in the literature [ 1 , 2 , 7 , 12 , 14 , 15 , 19 , 20 , 24 , 25 ]  . however , some published results indicate that the effect of different dose concepts on survival differs according to the patients performance status at time of presentation . 
in our analysis we found strahlentherapieundonkologie92013 | original article survival tota total dose 25 gy 25 gy 50 gy 50 gy 25 gy25 gy - patients alive 50 gy50 gy - patients alive time [ weeks ] fig . 
1 9 kaplanmeier curves showing survival rates for the 25 gy in 5 fractions and the 50 gy in 20 fractions treatment strategies survival tota total dose 25 gy 25 gy 50 gy 50 gy 25 gy25 gy - patients alive 50 gy50 gy - patients alive fig . 
2 9 kaplanmeier curves for the subgroup analysis of patients with a goodfair overall condition treated with the 25 gy in 5 fractions and 50 gy in 20 fractions treatment strategies time [ weeks ] that the treatment concept had no effect on survival for any performance status . this was not unexpected for patients with a poor overall condition at the time of presentation . 
some studies even indicate that more hypofractionated regimens , such as 17 gy in 2 fractions are sufficient for patient palliation and prolong survival times [ 14 , 15 , 19 , 20 , 23 , 25 ]  . a more unexpected result was the absence of a statistically significant effect of different treatment regimens for patients with a better overall condition . 
in sundstrms case it was additionally postulated that there might be a benefit of the normofractionated arm in terms of 3 - year survival , although the number of patients in the study was limited . another retrospective analysis published by appold et al . 
 [ 2 ] compared three dose regimens ( 60 gy in 30 fractions , 40 gy in 20 fractions and 25 gy in 5 fractions ) and consistently found that the treatment concept lost its influence on survival in the subgroup with a good performance status . a more commonly published result is that patients with a good performance status benefit from a higher total dose treatment concept . 
this was published as the result of a medical research council ( mrc ) trial in 1996 [ 16 ] , for example , although the dose regimens used in this study differ from those in the present analysis . 
however , what does seem to be consistent is that a high - dose regimen is correlated with an increased risk of rt - related toxicities , particularly dysphagia [ 1 , 15 , 16 , 25 ] due to the fact that acute esophagitis is one of the main severe radiation - induced toxicities [ 6 ]  . 
dysphagia itself significantly reduces a patients quality of life [ 13 ] , which survival total dose total dose 25 gy 25 gy 50 gy 50 gy 25 gy - patients alive 25 gy - patient 50 gy - patient 50 gy - patients alive fig . 
3 9 kaplanmeier curves for the subgroup analysis of patients with a poor overall condition treated with the 25 gy in 5 fractions and 50 gy in 20 fractions treatment strategies time [ weeks ] is an important parameter in palliative treatment . the difficulties in finding a compromise between the benefits of higher total dose rt in terms of survival and their associated increased risk of rt - induced toxicities is pointed out in the american society for radiation oncology guidelines . 
after reviewing 13 rcts with a total of 3473 patients , they concluded that there seems to be a survival improvement for treatment concepts with a biologically equivalent dose ( bed ) at an / ratio of 10 of at least 35 gy10 . in the present analysis , the hypofractionated arm has a calculated bed of 37.5 gy10 ( for comparison : bed for 50 gy in 20 fractions is 62.5 gy10 ) [ 9 ] , which meets this requirement . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . laudatio strahlenther onkol 2013 189 : 803803 doi 10.1007 / s00066 - 013 - 0421 - 3 online publiziert : 31 . 
juli 2013 springer - verlag berlin heidelberg 2013 j.schultze klinik fr strahlentherapie , universittsklinikum schleswig - holstein ( uksh ) , campus kiel prof.dr.med.dr.rer.nat. bernhardkimmigzur emeritierung qualittssicherung bei der rztekammer schleswig - holstein verbindet er seine fhigkeiten als arzt und physiker . privat gilt seine leidenschaft antiquarischen bchern und der medizingeschichte . 
er besitzt eine auergewhnliche bibliothek und eine groe zahl historischer dokumente , so die originalschrift wilhelm konrad rntgens zur entdeckung der rntgenstrahlen . seine mitarbeiter wnschen ihm einen aktiven ruhestand und mehr zeit fr freunde und die privaten interessen . jrgen schultze , kiel , peter niehoff , kln , und rolf sauer , erlangen korrespondenzadresse dr.j.schultze klinik fr strahlentherapie , universittsklinikum schleswig - holstein ( uksh ) , campus kiel arnold - heller - str . 
kimmig als inhaber des lehrstuhls fr strahlentherapie an der christian - albrechts - universitt zu kiel emeritiert und als direktor der klinik fr strahlentherapie in den ruhestand versetzt worden . bernhard kimmig wurde am 6 . 
dezember 1947 in bad peterstal / baden geboren und besuchte von 1954 bis 1967 die schule in hamburg , wohin sein vater als direktor der universitts - hautklinik berufen worden war . 
 seine weiterbildung in diagnostischer radiologie , nuklearmedizin und strahlentherapie absolvierte er von 1979 bis 1986 in heidelberg und erwarb die facharztanerkennungen fr radiologie und nuklearmedizin unter den professoren kuttig und zum winkel . 
und habilitierte sich 1985 in heidelberg fr das fach klinische radiologie . von 1986 bis 1991 war er oberarzt an der radiologischen universittsklinik heidelberg und leitete eine therapiegruppe in der abteilung spezielle onkologische diagnostik und therapie des deutschen krebsforschungszentrums ( dkfz )  . in anerkennung seiner wissenschaftlichen arbeit auf dem gebiet der strahlentherapie wurde ihm 1990 der holthusen - ring der deutschen rntgengesellschaft verliehen . 1990 erhielt er den ruf auf den lehrstuhl fr strahlentherapie an der universitt innsbruck sowie auf die c4 - professur fr strahlentherapie der universitt kiel , dem er am 1 . 
damit bernahm er als direktor die leitung der neu gegrndeten klinik fr strahlentherapie ( radioonkologie ) , die als eine von drei neuen kliniken nach emeritierung von helmut gremmel aus der ehemaligen radiologischen universittsklinik hervorgegangen war . ber 200 beitrge und publikationen in wissenschaftlichen zeitschriften , monographien und fachbchern umfasst sein werk . neben seiner klinischen ttigkeit bernahm er vielfltige aufgaben in der akademischen selbstverwaltung und im ehrenamt . 
so leitete er von 1992 bis 2010 das tumorzentrum des klinikums , war mehr als 10 jahre lang mitglied des akademischen senats sowie der ethikkommission und engagierte sich von 1998 bis 2008 als vorstandsvorsitzender der schleswigholsteinischen krebsgesellschaft , danach auch als vorstandsmitglied . frhzeitig erkannte er die bedeutung der bildgebenden verfahren fr die bestrahlungsplanung . 
so wurde die klinik fr strahlentherapie in kiel eine der ersten abteilungen , die ber ein eigenes ct zur bestrahlungsplanung verfgte . seiner untersttzung ist es zu verdanken , dass im jahre 2005 die erste universitre palliativstation in der radioonkologie realisiert werden konnte , spter ergnzt um eine weitere , interdisziplinre palliativund schmerzstation als projekt der deutschen krebsgesellschaft . wichtig ist ihm die enge verbindung zur medizinischen physik . 
als leiter der rztlichen stelle zur strahlentherapieundonkologie92013 | literatur kommentiert strahlenther onkol 2013 189 : 806808 doi 10.1007 / s00066 - 013 - 0399 - x online publiziert : 31 . 
juli 2013 springer - verlag berlin heidelberg 2013 e.dikomey hamburg prdiktivemarkerfrdieakute normalgewebetoxizittbei bestrahlungvonnicht - kleinzelligen lungenkarzinomen originalbeitrag guerra jl , gomez d , wei q et al ( 2012 ) association between single nucleotide polymorphisms of the transforming growth factor beta1 gene and the risk of severe radiation esophagitis in patients with lung cancer . 
einschlusskriterien fr die validierungsgruppe waren eine nicht von pausen unterbrochene strahlentherapie ( allenfalls weniger als 7 tage ) , eine erreichte gesamtdosis von 50 , 4 gy , keine operation und das vorliegen von dna - proben . 
 anderson cancer center zwischen 2003 und 2006 mit imrt ( 57% ) oder 3 - d - rt bestrahlt , die validierungsgruppe zwischen 1998 und 2002 mit 3 - d - rt . 
es werden gesamtdosen von median 63 gy , eine zieldosis von 69 gy fr die 2 - mal tgliche bestrahlung und eine spanne im validierungsund testkollektiv von 5084 gy angegeben [ 3 , 7 ]  . 
aus dem blut der patienten wurde die dna isoliert und 3 snps im tgf1 ( rs1800469 : c - 509t , rs1800471 : g915c und rs1982073 : t869c ) mit hilfe der rflpmethode ( restriktionsfragmentlngenpolymorphismus ) analysiert . 
in der multivariaten analyse mit adjustierung fr klinische faktoren ( auer dmax am sophagus ) bestand weiterhin eine signifikante assoziation von snps und re , und zwar mit hherem risiko bei steigender zahl an ungnstigen snps . 
damit kann dieser snp fr nsclc - patienten als prdiktiver marker bei der individualisierung der therapie verwendet werden . kommentar fr patienten mit einem nsclc ist die strahlentherapie bisher mit einem deutlichen normalgeweberisiko verbunden . 
 ziel muss es deshalb sein , genetische marker zu finden , die das risiko fr eine schwere sophagitis vorhersagen , um damit die therapie fr den jeweiligen patienten individuell gestalten zu knnen . 
 hervorzuheben ist vor allem , dass die assoziation , welche zwischen den snps im tgf1 und dem auftreten einer schweren sophagitis in einer ersten testgruppe gefunden wurde , in einer zweiten validierungsgruppe besttigt wurde . 
 die radiogene sophagitis ist ein anspruchsvoller klinischer endpunkt , da die dosis - wirkungsbeziehung nicht sicher bekannt ist , insbesondere welcher der parameter fraktionierung , gesamtdosis , maximale dosis und / oder durchstrahltes volumen ( v50 , v60 , bestrahlte sophaguslnge etc . ) fr die ausprgung der sophagitis fhrend ist . 
entsprechend ist beim vergleich unterschiedlich behandelter patienten die haupteinflussgre dosis schwer quantifizierbar . erschwert wird die interpretation der ergebnisse auch deshalb , weil bei 33 patienten ( 34% ) der testgruppe und 21 patienten ( 21% ) der validierungsgruppe dosimetrische angaben fehlen , aber dennoch in die analysen eingeschlossen wurden . 
die angabe der gesamtdosis ohne bercksichtigung der fraktionierung ist irrefhrend , so dass beim vergleich unterschiedlicher fraktionierungen die angabe der quivalentdosis fr eine einzeldosis von 2 gy ( eqd2 ) ntig ist . 
guerra jl , gomez d , wei q et al ( 2012 ) association between single nucleotide polymorphisms of the transforming growth factor beta1 gene and the risk of severe radiation esophagitis in patients with lung cancer . 
jin h , tucker sl , liu hh et al ( 2009 ) dose - volume thresholds and smoking status for the risk of treatment - related pneumonitis in inoperable nonsmall cell lung cancer treated with definitive radiotherapy . 
niu x , li h , chen z et al ( 2012 ) a study of ethnic differences in tgfbeta1 gene polymorphisms and effects on the risk of radiation pneumonitis in nonsmall - cell lung cancer . 
raabe a , derda k , reuther s et al ( 2012 ) association of single nucleotide polymorphisms in the genes atm , gstp1 , sod2 , tgfb1 , xpd and xrcc1 with risk of severe erythema after breast conserving radiotherapy . 
reuther s , metzke e , bonin m et al ( 2013 ) no effect of the transforming growth factor beta1 promoter polymorphism c - 509t on tgfb1 gene expression , protein secretion , or cellular radiosensitivity . 
yuan x , liao z , liu z et al ( 2009 ) single nucleotide polymorphism at rs1982073 : t869c of the tgfbeta 1 gene is associated with the risk of radiation pneumonitis in patients with non - small - cell lung cancer treated with definitive radiotherapy . 
zhang l , yang m , bi n et al ( 2010 ) association of tgf - beta1 and xpd polymorphisms with severe acute radiation - induced esophageal toxicity in locally advanced lung cancer patients treated with radiotherapy . 
iort evolved as an attempt to improve the therapeutic ratio by achieving highly effective radiation doses while dose - limiting healthy structures are surgically displaced [ 38 ]  . the first experience was documented by comas and prio in 1905 [ 6 ] for a case of endometrial cancer . 
subsequently , other treatments using low energy x - ray setups were described in abdominal , thoracic and head and neck malignancies between the 1930s and 1950s [ 9 ]  . 
the modern approach to iort began with studies by abe at the university of kyoto in the early 1960s [ 1 ] , who used single high doses of gamma rays from a cobalt unit and electrons from a betatron . 
croce and carle , cuneo , italy hospital san giovanni battista , foligno , italy university hospital santandrea , roma , italy hospital santa chiara , trento , italy hospital san francisco de ass , instituto madrileo de oncologa , madrid , spain san filippo neri hospital , roma , italy medical university of lublin , lublin , poland institute of the mediterranean , catania , italy hospital , treviso , italy ramban health care campus , haifa , israel hospital santa maria nuova , reggio emilia , italy regional centre for the fight against cancer ( crlc ) val daurelle , montpellier , france hospital multimedica , castellanza , italy 20062010 20052011 20062009 20092010 20082010 20082010 20052011 20092010 20092010 20092010 2010 19922002 2009 2009 20082011 20092010 20062010 20062010 20082011 20082010 21.8 tion of isiort ( isiort - europe ) was established in 2006 . 
among their other activities , isiort - europe collected and recorded information regarding iort activity at the affiliated centres in its database registry . this article reports the data collected by the database registry of isiort - europe with a focus on the clinical and technical aspects of iort . 
particular attention is given to the dominant tumour sites and the histological types identified . material and methods from 2007 , the isiort - europe centres were invited to record information relating to iort treatments in the database registry available at the isiort - europe website . 
in 2349 cases ( 98.1% ) , iort was a component of radical treatment for primary , newly diagnosed disease and in 46 cases ( 1.9% ) it was an attempt to rescue localized recurrent breast cancer . 
iort was used as single radiation treatment modality with doses of 18 gy ( 8% ) , 20 gy ( 23.8% ) or 21 gy ( 71.1% ) and as a boost before or after ebrt with doses of 812 gy . 
iort was performed either using electrons ( in 92% of patients , treated in 20 centres ) or a 50 - kv x - ray source ( the remaining 8% of patients , treated in a single centre )  . 
iort was performed either by electrons ( in 98% of cases , treated in 12 centres ) or using a 50 - kv x - ray source ( in the remaining 2% of cases , treated in a single centre )  . 
iort was performed either by electrons ( in 90% of cases , treated in eight centres ) or with a 50 - kv xray source ( in the remaining 10% of cases , treated in a single centre )  . 
iort was performed either by electrons ( in 98% of cases , treated in five centres ) or using a 50 - kv x - ray source ( in the remaining 2% of cases , treated in a single centre )  . 
it gives a picture of patient selection methods and treatment modalities , with emphasis on the main tumour types that are typically treated by this technique and may benefit from it . keywords breast cancer rectal cancer sarcoma prostate cancer pancreatic cancer klinische und technische charakteristika von intraoperativen strahlentherapien . 
die hufigste tumorentitt bildete das mammakarzinom mit 2395 fllen ( 63 , 8% ) , gefolgt von rektumkarzinomen mit 598 fllen ( 15 , 9% ) , 221 sarkomen ( 5 , 9% ) , 108 prostatakarzinomen ( 2 , 9% ) sowie 80 pankreaskarzinomen ( 2 , 1% )  . 
the technical characteristics of electron treatments are described in .fig.5. discussion the survey collected data from 21 institutions , which represented 39% of the iort centres active in europe in 2009 [ 9 ]  . 
the number of collaborating centres increased from three in 2007 to 21 in 2011 , demonstrating increased interest in this initiative . breast cancer during the past decades , clinical indications for iort treatment have evolved significantly and expert centres have incorporated this technique into breast cancer therapy . 
this fact may be related to the proportionately higher incidence of breast cancer compared to other tumours amenable to iort and to the launch of large clinical trials exploring iort as a single radiation modality . 
such trails aim to shorten overall treatment times in loco - regional therapy , improve patients quality of life and reduce the waiting lists in radiotherapy centres [ 35 , 37 ]  . 
the efficacy of single - shot iortwhich represents a partial breast irradiation ( pbi ) strategyhas been under investigation during the last few years , particularly for selected groups of patients [ 20 , 31 , 32 ]  . 
in this regard , the european society for radiotherapy and oncology ( estro ) and the american society for radiation oncology ( astro ) formulated quite similar general criteria for the recommendation of pbi [ 22 , 29 ]  . 
however , only 33% of patients treated by a single radiation fraction were included in study protocols , meaning that a large total number of patients were treated and implying that high - dose iort is considered current clinical practice on the basis of preliminary results of clinical trials [ 26 ]  . 
in 192 additional treatments ( 8% ) , a 50 - kv x - ray source was used with a spherical applicator placed in the surgical bed after tumour removal 6 cm ( 33% ) 12 mev ( 33% ) applicator diameter beveled end radiation beam energy dose fig . 
in 22 additional treatments ( 10% ) , a 50 - kv x - ray source was used with a spherical applicator placed in the surgical bed after tumour removal fig . 
5 9 main technical characteristics of intraoperative radiotherapy by electrons for pancreatic cancer a single fraction was also used to treat the surgical bed after local tumour recurrence in a relevant number of patients , i.e. 
 330 cases , representing 13.8% of all breast iort procedures in our survey . iort as a boost technique was used in about half of the patients ( 48% ) outside of clinical trials , meaning that the approach of anticipated boost has been adopted as current practice . 
the relatively low percentage ( 8% ) of x - ray treatments may be due to the fact that in comparison to centres using electrons , only a small fraction of the existing x - ray centres contributed to the registry . rectal cancer iort in rectal cancer aims to improve local control in locally advanced high - risk disease and in recurrent tumours where pelvic relapse is responsible for therapeutic failure . 
in the majority of cases , iort was given with curative intent as a boost intensification dose and was part of a multidisciplinary approach including surgery , ebrt and chemotherapy . numerous studies in the literature show a favourable local effect of iort , with high rates of local control in advanced primary and recurrent tumours [ 5 , 10 , 14 , 18 , 36 ]  . 
however , the only randomized trial comparing conventional preoperative external radiotherapy with the same treatment plus iort failed to show an advantage of the experimental arm [ 8 ]  . 
the european pooled analysis of iort - containing multimodality treatment for locally advanced rectal cancer in 605 patients showed a local recurrence rate of only 12% in a very high - risk group of patients [ 17 ]  . 
a collective effort in the design and enrolment of patients in prospective clinical trials may generate evidence useful for tailoring the indications for iort to rectal cancer [ 34 ]  . 
the technical parameters of our survey were adequate to treat the presacral space and were similar to those reported in the european pooled analysis [ 17 ]  . sarcoma iort is used in the multimodality treatment of sarcoma because it enables the application of high - dose radiation to the target volume using a lower ebrt dose , which results in correspondingly reduced doses to surrounding healthy tissues . 
data in the literature show that iort is able to achieve high control rates in selected cases of soft tissue sarcoma localized to the trunk or extremities [ 4 , 13 , 19 , 21 , 28 ]  . histologically , our analysis showed quite heterogeneous subtypes , as in many other sarcoma series . 
in terms of the technical aspects , soft tissue sarcoma required a wide range of applicator diameters and strahlentherapieundonkologie92013 | original article bevel angles , reflecting the frequently large tumour extension and the postresection tumour bed in soft tissues . 
moreover , many cases required complex irradiations with multiple fields or field - infield techniques with high - energy electrons ( up to 18 mev ) and doses of up to 25 gy . 
similar treatment modalities were described in other reports [ 4 , 13 , 19 , 21 ]  . prostate cancer the rationale for iort dose escalation for prostate cancer is based on the demonstration of a doseresponse relationship and the low / value in the linear quadratic model [ 16 ]  . 
 early data on iort in locally advanced prostate cancer come from kyoto university and the saitama cancer centre in japan , where the authors treated patients without prostatectomy [ 2 , 11 ]  . 
more recent experiences were reported by italian authors using iort in combination with radical prostatectomy and regional lymph node dissection before or after the surgical procedure [ 15 , 23 , 25 ]  . 
 the diameter and bevel end angle of the applicators were selected on the basis of target dimensions , considering a margin of at least 5 mm around the prostate and the necessity to reach the target underneath the pubic arch to spare the bladder . 
dose levels were in the range of those of a recently published series [ 16 ]  . pancreatric cancer iort could be an interesting approach for dose intensification to improve local control in the therapy of locally advanced pancreatic cancer . 
several literature studies have described favourable effects of iort in pancreatic cancer , but the results preclude clear interpretation since this technique was used in the context of multiple treatment strategies [ 24 , 33 ]  . the registry collected data from patients with locally advanced stages ( mainly t2t4 ) , treated in most cases with curative intent after tumour resection . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literatur kommentiert strahlenther onkol 2013 189 : 804805 doi 10.1007 / s00066 - 013 - 0385 - 3 online publiziert : 3 . 
august 2013 springer - verlag berlin heidelberg 2013 a.simeonovaf.wenz klinik fr strahlentherapie und radioonkologie , universittsmedizin mannheim langzeitverlaufderlebensqualitt nachprostatektomieund perkutanerstrahlentherapiebeim lokalbegrenztenprostatakarzinom originalbeitrag resnick mj , koyama t , fan kh et al ( 2013 ) long - term functional outcomes after treatment for localized prostate cancer . 
mnner , die wegen eines lokal begrenzten prostatakarzinoms prostatektomiert oder einer perkutanen strahlentherapie unterzogen werden , leiden unter unterschiedlichen funktionellen einschrnkungen , wobei die unterschiede zwischen den beiden gruppen nach einer kurzen bzw . 
da prostatakarzinompatienten meist lang berleben , sollten diese beobachtungen in die wahl der therapie eines lokal begrenzten prostatakarzinoms einflieen . kommentar die zu erwartende lebensqualitt ist ein wichtiger faktor bei der auswahl der therapie bei patienten mit einem lokal begrenzten prostatakarzinoprostatektomie und strahlentherapie sind auch nach den aktuellen s3 - leitlinien quivalente kurative therapiemethoden , die sich fr solche patienten durchgesetzt haben . 
auffallend ist weiterhin , dass die anzahl der ausgefllten fragebogen bei den patienten nach radiotherapie nach 15 jahren deutlich abnahm ( bis zu 75% weniger ausgefllte fragebgen ) , was sicher das ergebnis beeintrchtigen und ein grund fr die fehlende signifikanz der unterschiede zwischen beiden therapeutischen gruppen in der langzeitbeobachtung sein drfte . 
 dass patienten , die sich einer prostatektomie unterzogen hatten , nach 2 und 5 jahren deutlich hufiger ber harninkontinenz klagten als patienten nach perkutaner strahlentherapie , dieser unterschied aber nach 15 jahren nicht mehr signifikant war , untersttzen die daten von sanda et al . 
 [ 4 ] zeigten statistisch signifikant mehr erektile dysfunktionsstrungen und harninkontinenzraten 6 monate nach prostatektomie , wobei allerdings nach einem jahr die unterschiede nicht mehr signifikant waren . standen schon nach 2 jahren deutlich mehr probleme bei den bestrahlten patienten . 
potosky al , davis ww , hoffman rm et al ( 2004 ) five - year outcomes after prostatectomy or radiotherapy for prostate cancer : the prostate cancer outcomes study . 
madalinska jb , essink - bot ml , de koning hj et al ( 2001 ) health - related quality - of - life effects of radical prostatectomy and primary radiotherapy for screen - detected or clinically diagnosed localized prostate cancer . 
potosky al , knopf k , clegg lx et al ( 2001 ) qualityof - life outcomes after primary androgen deprivation therapy : results from the prostate cancer outcomes study . 
budus l , bolla m , bossi a et al ( 2012 ) functional outcomes and complications following radiation therapy for prostate cancer : a critical analysis of the literature . 
since no survival benefit has been demonstrated for wbrt in addition to surgery or srs , there is interest avoiding the potential neurocognitive sequelae associated with this treatment [ 12 ]  . 
recently , several retrospective reports have demonstrated that stereotactic radiosurgery ( srs ) or stereotactic hypofractionated radiotherapy ( shrt ) directed at the resection cavity can reduce local failure rates [ 19 , 25 ]  . 
most patients were treated with frame - based stereotactic systems such as the gamma knife ( elekta , stockholm , sweden ) or dedicated stereotactic linac systems [ 7 , 10 , 15 ]  . 
frameless image - guided intracranial stereotactic linac radiosurgery for brain metastases has recently been introduced and clinical outcomes are comparable to those after frame - based radiosurgery techniques [ 4 , 11 ]  . 
here we report on clinical outcome and lc in patients who underwent adjuvant frameless imageguided linac - based srs and shrt after resection of brain metastases . materials and methods patients and study design this retrospective study was approved by the local ethics committee . 
acute and late toxicities were evaluated using the common toxicity criteria for adverse events ( ctcae ) version 4.0 grading systeclinical status evaluation and imaging examinations were performed at 36 - month intervals . 
radionecrosis was scored according to late effects in normal tissuesubjective , objective , management and analytic ( lent - soma ) criteria [ 20 ]  . frameless srs and shrt procedures all patients were immobilized using a thermoplastic stereotactic frameless head mask ( brainlab , feldkirchen , germany )  . 
postoperative helical ct images of 1.5 - mm slice thickness were obtained and fused with postoperative t1 contrast - enhanced mprage and t2 - 3d sequences that were not older than 2 weeks prior to irradiation . 
the clinical target volume ( ctv ) was defined as the resection cavity including the surgical defect and any contrast enhancement , plus a 2 - mm margin in all directions . 
we used a conformity index ( ci ) defined according the following formula : ( 1 + volume of tissue outside ptv receiving at least the prescribed dose / volume of ptv receiving at least the prescribed dose )  . 
for srs planning we evaluated the normal brain volume irradiated with 12 gy ( v12 gy ) or 10 gy ( v10 gy ) , according to previously published reports [ 3 , 13 ]  . 
initially , 766 | strahlentherapieundonkologie92013 the dose concept of 64 gy was used for ptvs > 20 cm3 , but in order to increase the equivalent dose in 2 - gy fractions ( eqd2 ) , 40 gy was applied in 10 fractions . 
in this study , the tolerances for the patient setup were 0.8 mm for the three translational axes ( longitudinal , lateral and vertical ) and 1.0 for the three rotational axes ( pitch , roll and couch rotation )  . treatment was delivered using conformal dynamic arcs , intensity - modulated radiation therapy ( imrt ) field techniques and hybrid arcs ( dynamic arcs and imrt fields )  . statistics the analyzed endpoints were lc , distant brain control ( dc ) and overall survival ( os )  . 
all time - to - event endpoints were measured from the beginning of radiotherapy to either the last follow - up mri ( for recurrence rates ) , the beginning of salvage radiotherapy ( for salvage therapy ) or the date of death for os . 
the median time from surgery to irradiation was 40 days ( range 15 73 days )  . treatment parameters of the 44 surgical cavities in the 42 patients in the current study , 23 lesions ( 52% ) were treated with srs . 
the median dose prescription to the ptv margin was 17 gy ( range 1618 gy ) with maximum and minimum median ptv doses of 17.7 gy ( range 1720.4 gy ) and 16.8 gy ( range 14.618 gy ) , respectively . 
a total of 4 patients presented local recurrence : 1 patient after srs treatment with 17 gy and 3 patients after shrt treatment with 46 gy , 64 gy and 104 gy . 
tumor bed stereotactic radiosurgery ( srs ) after resection of brain metastases is a new strategy to delay or avoid whole - brain irradiation ( wbrt ) and its associated toxicities . 
the fractionation schemes applied were : 4 fractions of 6 gy ( 5 patients ) , 6 fractions of 4 gy ( 6 patients ) and 10 fractions of 4 gy ( 10 patients )  . 
frameless image - guided linac based adjuvant srs and shrt are effective and well tolerated local treatment strategies after resection of brain metastases in patients with oligometastatic disease . keywords toxicity metastases survival organs at risk quality of life adjuvante therapie nach resektion von hirnmetastasen . 
stereotaktische radiochirurgie ( srs ) des tumorbettes nach resektion von hirnmetastasen ist eine neuartige strategie , um eine adjuvante ganzhirnbestrahlung ( wbrt ) mit ihren toxizitten aufzuschieben oder zu vermeiden . 
rahmenlose bildgesteuerte adjuvante srs und shrt mit einem linearbeschleuniger sind wirksame und gut vertrgliche lokale behandlungen nach resektion von hirnmetastasen in oligometastatischen patienten . schlsselwrter toxizitt metastasen berleben risikoorgane lebensqualitt strahlentherapieundonkologie92013 | original article tab . 
2 characteristics of patients with a local recurrence toxicity patientno . primary tumor rectal cancer melanoma rectal cancer esophageal cancer 64 gy r0a , piecemeal 25.8 117 gy r0a , piecemeal dose ( gy ) resection status ptv size ( cm3 ) time to recurrence ( months ) salvage treatment wbrt whole brain radiation therapy , srs stereotactic radiosurgery , ptv planning target volume . 
 no acute grade 2 or higher toxicity was observed . discussion in patients with limited brain metastases , the positive effects of wbrt in decreasing the rate of intracranial progression do not translate into survival or quality of life benefits [ 22 ]  . 
 in light of these findings , it is our practice to omit or defer wbrt in favor of srs or shrt in postoperative patients with a limited number of brain metastases . 
 these results are comparable to the lc rates of 7590% achieved previously with adjuvant wbrt [ 17 ]  . frameless image - guided srs and shrt noninvasive patient immobilization and frameless image guidance as applied in srs of brain metastases are techniques that have been recently introduced . 
a number of reports regarding the accuracy of image - guided methods have demonstrated that submillimeter accuracies can be achieved and that accuracy is comparable to the traditional frame - based approach [ 5 , 9 ]  . 
the shrt studies suggest that lc rates of 76 89% can be obtained using regimens of 310 fractions with total doses ranging from 20 to 40 gy [ 6 , 25 , 26 ]  . 
a recent report comparing different dose concepts in shrt showed that eqd2s of 35 gy seem to be the most effective concept in patients with primary or recurrent limited primary brain metastases [ 14 ]  . 
srs stereotactic radiosurgery ( solid line in b ) , shrt stereotactic hypofractionated radiotherapy ( dotted line in b ) target volume at present , there are no well established guidelines concerning the definition of the target after surgical resection of brain metastases . 
 patel and colleagues reported that resection of the tumor in a piecemeal fashion significantly increased the incidence of local recurrence in comparison with en bloc resection [ 17 ]  . 
the resection of metastatic lesions in contact with or involved with the cerebrospinal fluid ( csf ) pathway is associated with a significantly higher incidence of leptomeningeal seeding than resection of tumors separated from the csf pathway by brain parenchyma [ 1 ]  . 
neuropathological studies have shown that infiltration may be responsible for the presence of clinically undetectable cancer islands showing a maximum infiltration depth of 13 mm [ 2 ]  . toxicity choi and colleagues reported the first prospective data showing that the addition of a 2 - mm margin to the resection cavity resulted in a decreased local failure rate at 12 months from 16 to 3% , without increasing toxicity [ 6 ]  . 
prabhu r , shu hk , hadjipanayis c et al ( 2012 ) current dosing paradigm for stereotactic radiosurgery alone after surgical resection of brain metastases needs to be optimized for improved local control . 
soffietti r , kocher m , abacioglu um et al ( 2013 ) a european organisation for research and treatment of cancer phase iii trial of adjuvant wholebrain radiotherapy versus observation in patients with one to three brain metastases from solid tumors after surgical resection or radiosurgery : quality - of - life results . 
sperduto pw , berkey b , gaspar le et al ( 2008 ) a new prognostic index and comparison to three other indices for patients with brain metastases : an analysis of 1 , 960 patients in the rtog database . 
steinmann d , maertens b , janssen s et al ( 2012 ) hypofractionated stereotactic radiotherapy ( hfsrt ) after tumour resection of a single brain metastasis : report of a single - centre individualized treatment approach . 
wang cc , floyd sr , chang ch et al ( 2012 ) cyberknife hypofractionated stereotactic radiosurgery ( hsrs ) of resection cavity after excision of large cerebral metastasis : efficacy and safety of an 800 cgy 3 daily fractions regimen . 
wang and colleagues reported a combined rate of all toxicities ( radionecrosis , prolonged steroid use and new - onset seizures ) of 9% using cyberknife ( accuray , sunnyvale , ca , usa ) hypofractionated srs with 3 fractions of 8 gy daily [ 26 ]  . 
for most lesions , 40 gy in 10 fractions was applied according to the guidelines reported in the previous phase ii trial of shrt , which recommended that the v4 gy per fraction for normal brain should not exceed 20 cm3 [ 8 ]  . 
cerebral radionecrosis ( rn ) after treatment of brain tumors represents a severe and potentially devastating long - term complication that may be associated with considerable morbidity and even mortality [ 24 ]  . 
the importance of functional imaging , including fdg positronemission tomography ( fdg - pet ) and mr spectroscopy , for discrimination between tumor progression and pseudoprogression remains to be discussed [ 7 , 8 , 16 , 23 ]  . 
in adults , the clinical course of rn is variable , ranging from asymptomatic lesions with spontaneous recovery to rapid progression with development of neurological deterioration [ 7 ]  . 
a spectrum of clinical syndromes after cancer treatment directed to the cns in childhood has been described and includes radionecrosis , necrotizing leukoencephalopathy , mineralizing microangiopathy , cavernous hemangioma and secondary brain tumors [ 22 , 27 ]  . 
the aim of this retrospective , observational study was to describe a single - centers experience with rn in children treated for brain tumors over a period of 20 years . patients and methods study population between 1 january 1992 and 1 april 2012 , a total of 107 consecutive children ( 62 male and 45 female , median age 9.4 years ) underwent external photon beam rt for various brain tumors at the dept . 
lackner contributed equally to this work . strahlentherapieundonkologie92013 | original article patients were primitive neuroectodermal tumor ( pnet ) / medulloblastoma ( n = 32 ) , pnet ( supratentorial ) ( n = 13 ) , ependymoma ( n = 10 ) , pontine glioma ( n = 14 ) , astrocytoma ( n = 16 ) , glioblastoma ( n = 5 ) , craniopharyngeoma ( n = 3 ) , intracranial germ cell tumor ( n = 10 ) and others ( n = 4 )  . 
suspicion of rn arose if mri revealed new lesions in cases where signs of rn were already evident , as previously described [ 7 , 16 , 23 ]  . 
in all cases of rn included in this study , relapse or progression of the underlying disease was ruled out by resolution of the lesions during follow - up . analysis of eqd2 over the decades , patients were treated according to different study protocols , with irradiation treatment schemes that differed in terms of total dose , fraction dose and the number of fractions . 
to facilitate comparison of data from the different studies , the tolerance dose of normal brain tissue is presented as the biologically equivalent total dose as applied in 2 gy fractions ( eqd2 ) , as opposed to the physical dose . 
a retrospective singlecenter study was undertaken to describe the incidence and clinical course of rn in a cohort of 107 children treated with external radiotherapy ( rt ) for various brain tumors between 1992 and 2012 . 
during a median follow - up of 4.6 years ( range 0.2920.1 years ) , rn was implied by suspicious mri findings in in 5 children ( 4.7% ) , 5131 months after rt . 
suspicion was confirmed histologically ( 1 patient ) or substantiated by fdg positron - emission tomography ( fdg - pet , 2 patients ) or by fdg - pet and mr spectroscopy ( 1 patient )  . 
treatment of rn included resection ( n = 1 ) , corticosteroids ( n = 2 ) and a combination of corticosteroids , hyperbaric oxygen ( hbo ) and bevacizumab ( n = 1 )  . 
treatment options in patients with symptomatic rn include conservative management ( steroids , hbo , bevacizumab ) and surgical resection . keywords paediatric oncology radiotherapy chemotherapy late effects cerebral radionecrosis inzidenz und klinischer verlauf von radionekrosen bei kindern mit schdeltumoren . 
bei 5 ( 4 , 7% ) von 107 kindern , die in den jahren 1992 bis 2012 wegen unterschiedlicher schdeltumoren eine strahlentherapie erhalten hatten , erhrtete sich whrend des medianen nachbeobachtungszeitraums von 4 , 6 ( 0 , 2920 , 1 ) jahren 5131 monate nach bestrahlung der verdacht auf eine rn . 
dieser wurde entweder histologisch ( 1 patient ) oder mittels fdg - positronenemissionstomographie ( fdg - pet ; 2 patienten ) oder mittels mr - spektroskopie und fdg - pet ( 1 patient ) besttigt . 
die behandlung bestand aus resektion ( n = 1 ) , kortikosteroiden ( n = 2 ) oder einer kombination aus kortikosteroiden , hyperbarer oxigenierung und bevacizumab ( n = 1 )  . 
die behandlungsmglichkeiten bei symptomatischen patienten umfassen konservatives management ( kortikosteroide , hyperbare oxygenierung , bevacizumab ) sowie die chirurgische resektion . schlsselwrter pdiatrische onkologie strahlentherapie chemotherapie sptkomplikation zerebrale radionekrose apy in addition to rt . 
in those patients with rn , the median age at irradiation was 6.9 years ( range 5.215.4 years ) ; the underlying diagnoses were astrocytoma ( n = 1 ) , medulloblastoma ( n = 2 ) , ependymoma ( n = 1 ) and brain metastasis of osteosarcoma ( n = 1 )  . 
in 3 out of 5 patients , subsequently performed fdg - pet showed decreased fdg uptake and in one of these patients , additional mr spectroscopy showed decreased levels of choline . 
treatment of rn included complete resection in 1 patient , dexamethasone in 2 patients and a combination of dexamethasone , bevacizumab and hyperbaric oxygen ( hbo ) therapy in 1 patient [ 1 , 11 , 18 ]  . 
mri lesions resolved in all patients ( .fig.1 ) , although 2 patients ( numbers 3 and 5 ) still require intensive physical rehabilitation due to severe persistent neurological deficits . discussion there is little known about the incidence of rn in children treated for brain tumors . 
these data are comparable to those of our study , where rn was documented in 4.67% of 107 children , after a median interval of 11 months following external photon beam rt . 
the eqd2 biological dose estimation permits comparison of different rt schemes [ 20 , 26 ]  . chemotherapy in addition to rt might support the development of rn [ 24 ]  . 
the spectrum of clinical manifestations of rn is extremely wide , ranging from asymptomatic lesions to spontaneous recovery and progressive neurological deficits that may be irreversible , and sometimes even cause death [ 23 , 24 ]  . 
the lesions are described as a ring - enhancing mass with variable edema and mass effect [ 23 ] , or lesions with a soap bubble or swiss cheese pattern [ 16 ] closely mimicking the pattern of recurrent brain tumor . 
 in lesions highly suspicious for tumor recurrence , biopsy still remains the diagnostic gold standard ; however , its use is limited by its invasive nature and the potential heterogeneity of the lesions . 
functional imaging , including fdg - pet or mr spectroscopy is considered increasingly useful for differentiating rn from tumor recurrence [ 7 , 10 , 16 , 23 ]  . 
in our series , diagnosis of rn was established histologically in 1 patient , suspicion of rn was substantiated by fdgpet showing decreased uptake of radionuclide in 3 patients and mr spectroscopy showed decreased levels of choline in one of the patients who was also examined by pdg - pet . 
 therefore , it must be stated that functional imaging is always associated with a residual risk of misdiagnosis . regarding the doseresponse relationship , the risk of rn was reported to increase with increased total dose and dose per fraction , as well as with increasing tissue volume [ 4 ]  . 
based on several clinical studies of childhood brain tumors , a threshold eqd2 value of approximately 45 gy was estimated for the development of rn , with a steep increase in the risk of rn above 60 gy . 
in patients with neurological symptoms , several conservative treatment options are advocated , including corticosteroids , hbo and more recently , bevacizumab , a monoclonal antibody against vascular endothelial growth factor ( vegf ) [ 1 , 7 , 11 , 18 ]  . 
the rationale for the use of hbo is the hypothesis that it might increase the partial pressure of oxygen ( po2 ) in the tissue and thus enhance angiogenesis [ 1 , 7 , 11 , 19 ]  . 
surgical resection may be necessary in the case of raised intracranial pressure , if symptoms require rapid control or if symptoms show progression under conservative treatment [ 24 ]  . 
urban state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
despite progress in the treatment of other cancers , curative resection still remains the only possibility for a cure in pancreatic cancer . at primary diagnosis , patients often suffer from locally advanced disease due to a typical lack of early symptoms . 
 however , although no distant metastases are seen , curative resection is not possible in the remaining 30%40% of patients due to the involvement of critical structures such as celiac vessels . 
for these latter cases , several studies have shown that neoadjuvant treatment with radiation and chemotherapy can lead to secondary resectability , providing these patients a chance of curative treatment [ 2 , 3 , 4 , 5 ]  . 
 today , gemcitabine is still the most frequently used chemotherapeutic agent for pancreatic cancer [ 6 , 7 ] and can improve survival even after complete surgical resection [ 8 ]  . weight loss is a typical symptom in pancreatic cancer as a result of many potential triggers such as early satiety , nausea , pain , malnutrition , anxiety , depression and / or tumor - mediated changes in metabolism leading to cachexia . 
in contrast , obesity as a possible predictor of perioperative outcome as well as of long - term survival following pancreaticoduodenectomy has been extensively investigated [ 9 , 10 , 11 ]  . 
however , in addition to conventional indirect morphometric parameters such as bmi or waist - to - hip ratio , other recent studies introduced the direct assessment of fat distribution by computer tomography to describe nutritional status [ 11 ]  . the purpose of the present study was to assess weight and subcutaneous fat as surrogates for nutritional status before and after neoadjuvant chemoradiation and their influence on treatment response in pancreatic cancer . methods we analyzed 100 consecutive patients with locally advanced pancreatic cancer treated by neoadjuvant gemcitabine - based chemoradiation at our department . study population the median age on initiation of chemoradiation was 64 years and 51 of 100 patients were female . 
 to bridge the time gap until the first assessment of the treatment response , patients received on average only one of three scheduled gemcitabine 1000 mg / m2 bsa infusions , mostly due to the suppression of bone marrow cells . 
we manually outlined the subcutaneous fat area of a ct slice at the umbilicus level as described previously [ 13 ] using our in - house radiological software ( centricity radiology ra1000 , ge healthcare , barrington , us )  . 
we used age determined as age at begin of chemoradiation , bmi calculated from height and weight at the start of chemoradiation and weight loss as the difference in weight at the start and end of chemoradiation as continuous variables . 
 abstract zusammenfassung strahlenther onkol 2013 189 : 745752 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0393 - 3 p.naumannd.habermehlt.welzelj.debuss.e.combs outcome after neoadjuvant chemoradiation and correlation with nutritional status in patients with locally advanced pancreatic cancer abstract background . 
by categorizing patients according to their bmi based on the who classification as slender , normal , overweight and obese , we found improved but not statistically significant survival among obese patients . 
although the extent of weight loss was not significantly correlated with survival , the observed trend warrants greater attention to nutritional status in the future . keywords locally advanced pancreatic cancer neoadjuvant chemoradiation nutritional status cachexia obesity subcutaneous fat therapieerfolg nach neoadjuvanter radiochemotherapie und korrelation mit dem ernhrungsstatus bei patienten mit lokal fortgeschrittenem pankreaskarzinom zusammenfassung hintergrund . 
daten zur demographie , biometrie , toxizitt und berleben wurden von den letzten 100 patienten mit lokal fortgeschrittenem pankreaskarzinom , die mit einer neoadjuvanten radiochemotherapie ( 45 , 0 gy und boost bis 54 , 0 gy sowie simultan anschlieend gemcitabin ) in unseren abteilung behandelt wurden , erhoben . 
durch gruppierung der patienten nach ihrem bmi in anlehnung an die who - klassifikation in schlank , normal , bergewichtig und adips zeigte sich ein tendenzieller berlebensvorteil fr adipse patienten . 
ct images were searched for transverse slices at the umbilicus level where subcutaneous fat was framed manually and area and density were determined as shown in .fig.2. the ct images of 62 patients were available for evaluation . 
typical reasons for unavailability were imaging performed externally , mri instead of ct follow - up or imaging that only mapped the upper abdomen ( no umbilicus level )  . 
since samples of subcutaneous fat area were not normally distributed according to dagostinos omnibus k2 test , we had to transform the values by taking their common logarithms to obtain gaussian - like distribution before testing for significant differences before and after chemoradiation . interestingly , the average density of subcutaneous fat increased from 86.7 to strahlentherapieundonkologie92013 | original article change in weight + bmi * * * * * * * * change in sf area + sf density * * * * * * * * before after before after before after before after correlation sf area vs . 
within the first 2 years after chemoradiation , survival among slender and obese patients tended to be higher than among normal and overweight patients ; however , differences were not statistically significant . 
with a pearson r of 0.47 there was a slight correlation of higher toxicity with lower performance scale and a marginal correlation ( pearson r of 0.21 ) with the amount of weight loss during treatment . 
due to prolonged emesis and inappetence , 14 of our patients received parenteral nutrition and approximately one third had an additional high caloric liquid diet . outcome of neoadjuvant treatment and surveillance analysis for outcome and surveillance analysis , we categorized patients according to their bmi at the beginning of chemoradiation as slender , normal , overweight and obese as described in themethods section . 
in addition , we grouped patients according to their relative extent of weight loss during chemoradiation and were able to observe that 58 patients ( 62.4% ) lost at least 2.5% of their initial weight and 34 ( 36.6% ) even more than 5.0%. after neoadjuvant chemoradiation , the absolute resection rates among bmi groups were quite similar at approximately 36% . 
in contrast , for the extent of weight loss , we found that 24 of 59 ( 41% ) patients with no or less than 5% weight loss were amenable to secondary resection . 
additionally , we excluded the nine r0 resected patients since complete resection is a major prognostic factor and we wanted to analyze a possible impact of nutritional status on strahlentherapieundonkologie92013 | original article tab . 
despite the lack of statistical significance of survival differences , the authors believe that these data warrant further examination of nutritional status in pancreatic cancer . discussion in the present work , we confirm and corroborate for the first time ( to our knowledge ) the frequent weight loss observed in the clinical setting during the chemoradiation of pancreatic cancer patients . 
although the extent of weight loss was not significantly correlated with survival , the observed trend warrants greater attention to nutritional status . the weight and other biometric parameters of patients with pancreatic cancer are well studied in terms of perioperative outcome and complications following pancreaticoduodenectomy [ 9 , 10 , 11 ]  . 
 in addition , pathological findings such as grading and infiltration of nerves or vessels predict a shorter life expectancy in pancreatic cancer [ 14 , 15 , 16 ]  . 
however , there is little evidence for weight changes in patients receiving chemoradiation for locally advanced pancreatic cancer and still less concerning a possible influence on outcome . in this retrospective random consecutive patient cohort , demographics , tumor characteristics and treatment modalities were relatively balanced , with the exception of tumor location . 
this could be explained by the fact that our patients were primarily inoperable due to tumor contact with abdominal vessels , which in turn are predominantly located adjacent to the pancreatic head . 
 nevertheless , many patients were treated for a diagnosis made on the basis of clinical symptoms considered typical for pancreatic cancer , in combination with pathognomonic radiological imaging and elevated tumor markers ca 19.9 and / or cea . 
although we deem histopathological evidence of the suspected diagnosis as mandatory , the use of endoscopic ultrasound - guided biopsy is controversial and can be false negative [ 5 ]  . 
as a high volume center , we do not always insist on obtaining biopsy confirmation andsubject to decisions made in multidisciplinary meetings ( tumor boards ) proceed with neoadjuvant therapy in order to avoid delaying treatment if clinical symptoms , ct morphology and elevated tumor markers clearly support the diagnosis of pancreatic cancer . we performed gemcitabine - based chemoradiation at a dose of 50.4 gy in single doses of 1.82.2 gy to obtain secondary resectability as described previously [ 4 ]  . 
in contrast , subcutaneous fat area was not biased by extravascularly accumulated fluid and additionally correlated very well with patients bmi as shown previously [ 18 ]  . loss of fat stores is typical for tumor cachexia and begins several months before death and hence can predict survival in advanced cancer patients [ 19 ]  . 
we grouped patients by bmi essentially in accordance with the who classification and found an increased overall surviv750 | strahlentherapieundonkologie92013 al rate after chemoradiation for adipose patients as well as , interestingly , for slender patients . 
in line with these findings , the importance of energy reserves and nutritional care , especially in patients who had undergone major surgical resection such as pancreaticoduodenectomy , was recently described [ 20 ]  . interestingly , subcutaneous fat after chemoradiation proved to become more radiopaque from the perspective of ct morphology . 
initially , we speculated whether the increase in density could be attributable to multiple heparin injections ; however , during radiotherapy for pancreatic cancer our patients usually received their subcutaneous injections in the lower abdomen or the upper leg . 
additionally , many outpatients shirk thrombosis prophylaxis completely , although we regularly recommend prophylaxis since its safety and benefit was shown by the conko - 04 study [ 21 ]  . 
 therefore , we hypothesize an underlying yet unknown change in subcutaneous fat composition during weight loss as a consequence of catabolic or even cachexia - induced lipid mobilization in subcutaneous fat [ 19 ]  . chemoradiation was well tolerated by our study population . 
kps did correlate with the extent of toxicity but we did not see a correlation of bmi to toxicity as published for example for rectal cancer [ 23 ]  . 
in patients with head and neck squamous cell cancer treated by chemoradiation , for example , nutritional support lead surprisingly to a poorer prognosis [ 24 ]  . however , the present study has a number of limitations . 
firstly , it could be biased by virtue of its retrospective character , especially since we selected our last 100 patients with available survival data , maybe leading to more patients who died earlier perhaps due to more aggressive tumors . 
 despite excellent soft tissue contrast allowing lesion detection and local staging , a large variation in sensitivity ( 27 100% ) and specificity ( 3299% ) has been reported for t2 - weighted ( t2w ) mri [ 3 ]  . 
dynamic contrast - enhanced ( dce ) mri [ 5 ] and diffusion - weighted ( dw ) mri [ 6 ] , which respectively visualize the perfusion and diffusion characteristics of tissue , are both widely used . 
furthermore , some recent studies have shown the superiority of multiparametric mri in terms of detection and localisation of primary pca as compared to the use of each single mri technique [ 7 , 8 , 9 , 10 , 11 ]  . another functional imaging technique which offers the possibility to reflect biological tissue characteristics is positron emission tomography ( pet ) [ 12 ]  . 
 a promising tracer in the field of pca is 11carbon ( c ) - choline , as increased uptake of this radiolabelled choline has been observed in prostate tumour sites [ 12 , 13 ]  . 
 although 11c - choline has a short half - life of 20 min and therefore requires an onsite cyclotron to prepare an individual batch for each imaging study , it was preferred over 18f - choline because of its lower urinary excretion . 
11c - choline pet - ct is currently not suitable for patient selection for primary treatment due to its low sensitivity and specificity in localising tumour lesions both at the level of the prostate gland and the lymph nodes . 
in contrast , its value in re - staging of patients with biochemical recurrence by distinguishing those with local versus distant relapse has been demonstrated , thus providing an attractive tool to guide irradiation of local recurrences [ 14 , 15 ]  . the combination of anatomical , physiological and biological information could potentially improve the localisation of primary prostate tumours , thereby enabling image - guided focal radiation dose - escalation to these intraprostatic lesions [ 16 ]  . 
 this more targeted approach could provide a valuable alternative for whole - gland dose - escalation , which despite its positive impact on biochemical progression - free survival , is limited due to an increased risk for normal tissue complications [ 17 , 18 ]  . 
 patients had to have intermediate to high risk pca ( damicos risk criteria [ 19 ] ) and were eligible for radical prostatectomy if they did not show pelvic lymph node involvement on contrast - enhanced ct or bone metastasis on bone scan . 
the median time between mr imaging or 11c - choline pet - ct and radical prostatectomy ( rpe ) was 16 days [ interquartile range ( iqr ) 726 days ] and 14 days ( iqr 622 days ) respectively . 
immediately after injection of 740 mbq of 11c - choline , the scout view ( scan range ) from lung tops to below the scrotum was defined , a contrast - enhanced ct scan ( slice thickness of 3.3 mm ) was performed with 120 ml nonionic contrast agent given intravenously as a bolus ( ultravist , schering ; injection rate of 1.6 ml / s followed by 35 ml nacl 0.9% in 100 s ) followed by the 11c - choline pet emission scan covering the same field of view . 
pet data of the whole - body tracer distribution were then acquired ( 6 bed positions , 5 min scanning time per position ) starting approximately 4 min after injection of 11c - choline . 
in order to analyze 11c - choline pet - ct , the t2w mri images were used as anatomic reference to adequately visualize prostatic anatomy and margins [ 20 , 21 ]  . 
in a first registration step , the ct of the combined whole body 11c - choline pet - ct dataset was manually aligned with the mri dataset along the axial direction so that the pelvic area of both datasets coincided . 
in a second registration step , an algorithm using mutual information and powell optimization automatically aligned the ct and mri dataset by determining the optimal rigid body transformation [ 22 ]  . histopathology prostatectomy specimens were examined microscopically after routine preparation [ 23 ]  . 
afterwards , the tumour regions were outlined on all mri data sets by a radiologist with 8 years of experience in prostate mri , who was blinded to the histopathological findings . 
the criterion for pca detection on the t2w images was a nodular , hypointense lesion in the peripheral zone ( pz ) or a very pronounced hypointense , sickle - shaped lesion in the transitional zone ( tz ) of the prostate gland . 
 on the dw images , nodular foci in the pz and the tz were considered positive for pca when showing low signal - intensity on b - 0 images and high signal intensity on the b - 1000 images combined with a low signal - intensity on the adc map . 
tumour localisation mapping on each of the examined modalities was performed using a grid with 8 regions of interest ( rois ) as shown in .fig.1g , which was manually placed onto every slice and all octants were evaluated for the presence of tumour . this grid was also projected on each of the coregistered 11c - choline pet slices containing prostate tissue . 
we used a quantitative approach for choline pet - ct in order to create an optimal setup to test its additional value , whereas mri scans were visually analyzed in conformity with clinical daily practice . for the histopathology results , a pathologist with 3 years of experience who was blinded to the imaging data , outlined all tumour regions on the haematoxylin and eosin ( h&e ) - stained macrosections . 
a total of 73 patients with biopsy - proven intermediateand high - risk prostate cancer were enrolled in a prospective imaging study consisting of t2weighted ( t2w ) , dynamic contrast - enhanced ( dce ) and diffusion - weighted ( dw ) mri and 11c - choline pet - ct before radical prostatectomy . 
cancerous regions were delineated on the whole - mount prostatectomy sections and on the different mri modalities and analysed in 24 segments per patient ( 3 sections , 8 segments each )  . 
the additional value of 11c - choline pet - ct to mri in localising intraprostatic tumour nodules is limited , especially when multiparametric mri is used . keywords magnetic resonance imaging dynamic contrast - enhanced mri diffusion - weighted mri 11c - choline pet - ct whole - mount histopathology trgt 11c - cholin - pet - ct zur multiparametrischen mr - bildgebung zur lokalisierung von prostatakrebs bei ? zusammenfassung hintergrundundziel . 
insgesamt 73 patienten mit durch biopsie nachgewiesenem prostatakarzinom von mittlerem und hohem risiko nahmen an einer prospektiven bildgebenden studie , bestehend aus t2 - gewichteter ( t2w ) , dynamischen kontrast ( dce ) und diffusionsgewichteter ( dw ) mr und 11ccholin - pet - ct vor radikaler prostatektomie , teil . 
mit t2w , dce und dw - mr wurde jeweils eine hohe spezifitt ( 94 , 7% , 93 , 6% und 92 , 2% ) aber eine relativ geringe sensitivitt ( 31 , 2% , 24 , 9% und 44 , 1% ) fr die tumorlokalisation er zielt . 
der mehrwert von 11ccholin - pet - ct bei der mr zur lokalisierung von intraprostatischen tumorknoten ist begrenzt , vor allem bei der verwendung von multiparametrischer mr . schlsselwrter magnetresonanztomographie dynamisches kontrast mr diffusionsgewichtete mr 11c - cholin pet - ct whole - mount - histopathologie strahlentherapieundonkologie92013 | original article fig . 
1 8 images of a 57 - year - old man with prostate cancer in the left lobe with prostate - specific antigen level of 9.70 ng / ml and gleason score 8 . 
we also calculated suvs standard deviations and compared these between groups ( positive or negative histopathological findings ) using a logistic generalized estimating equations ( gee ) model , to account for the fact that 24 segments were analyzed in the same patient . 
for all analyses ( statistica 10.0 ; statsoft inc , tulsa , ok , usa ) , a p value of < 0.05 was considered statistically significant . patient and tumour characteristics are listed in .tab.2. 
in total , 1 , 752 octants were analyzed ( 73 patients , with 24 octants each ) of which 708 ( 40.4% ) were found to be malignant and 1 , 044 ( 59.6% ) contained benign prostatic tissue . 
t2w t2 - weighted , dce dynamic contrast - enhanced , dw diffusion - weighted , suvmax maximum standardized uptake values , pet positron emission tomography , mri magnetic resonance imaging . 
this table also shows suvmax thresholds ( 3.43.8 ) resulting in the highest sensitivity and specificity levels that can be reached when these parameters are considered of equal importance . discussion the use of functional imaging techniques combining anatomical , physiological and biological information is increasingly being implemented in pca diagnosis , staging and treatment [ 9 ]  . 
although different approaches for data analysis are applied , the majority of authors report good performance when multiparametric mri is used , in particular when cancer arises in the pz [ 7 , 8 , 24 ]  . 
conversely , other authors [ 16 , 25 , 26 ] reported data in favour of the use of choline pet - ct for localisation ( and delineation ) of intraprostatic tumour nodules . 
for instance , selecting a high suvmax threshold will lead to a high specificity and could be adopted to escalate the radiation dose to an intraprostatic lesion with only limited likelihood to irradiate a false positive region . 
serum psa level , tumour volume , tumour stage and gleason score , since any correlation could have important implications for the stratification of individual patients for a particular ( adjuvant ) treatment . 
as for the other clinical parameters , our data are generally in accordance with earlier studies in which no correlations were found between suvs and psa level , gleason score or tumour stage [ 27 , 28 , 29 ]  . 
although we are intuitively inclined to think that multiparametric mri has more potential to accurately detect intraprostatic lesions than choline pet - ct , data to support this reasoning are rare . 
contrary to the latter study , our results show that irrespective of the mri modality that was used , the additional value of choline pet - ct in terms of accuracy was very limited and almost negligible when compared to the mri alone . 
we also observed that when all modalities were combined , sensitivity levels clearly increased but at the cost of specificity . in addition , we noted that it was not possible to define a suvmax threshold that resulted into an improved sensitivity for choline pet - ct compared to mri without giving in on specificity or the other way around . 
 [ 31 ] compared sensitivity and specificity of mri , three - dimensional ( 3d ) mr spectroscopy ( mrs ) , combined mri and 3d mrs , and 11c - choline pet - ct for intraprostatic tumour sextant localisation with histopathological findings as reference standard in 26 patients . 
 [ 32 ] comparing 11c - acetate pet - ct and proton mrs for primary pca laterality in 21 patients , visual analysis on a lobar level also showed a better performance for multiparametric mri . 
 [ 33 ] found that choline petct may provide more accurate information when comparing 11c - choline pet - ct and proton mrs in 20 patients for primary pca laterality . 
the sextant or lobar analysis versus our 24 - segmental analysis per patient . based on these findings , there is no evidence to perform choline pet - ct in addition to mri for primary pca detection or localisation , or to prefer choline petct over mri , especially when multiparametric mri is used . 
however , the addition of multiple imaging techniques for gtv delineation is not as straightforward as compared to the diagnostic setting where the purpose is detection , characterization and staging of the tumour . 
defining the exact tumour boundary , even when all modalities point at the presence of the tumour in a particular location , is often difficult to assess ; in particular when different techniques provide conflicting information [ 4 ]  . 
furthermore , when thinking about dose - painting , more research is needed to identify if particular ( combinations of ) imaging modalities correlate with tumour aggressiveness and radiation sensitivity and many technical challenges will need to be tackled before multimodality imaging could be efficiently implemented for radiotherapy dose - painting [ 38 ]  . our study has some limitations . 
second , it was not possible to perform a 1 : 1 slice correlation because of changes of the size and shape of the prostate due to shrinkage during fixation . 
next , it should be stressed that patients with clinically low - risk pca were not included in the study , implicating that our results cannot be extrapolated to this patient group . 
panebianco v , sciarra a , lisi d et al ( 2012 ) prostate cancer : 1hmrs - dcemr at 3t versus [ ( 18 ) f ] choline pet / ct in the detection of local prostate cancer recurrence in men with biochemical progression after radical retropubic prostatectomy ( rrp )  . 
groenendaal g , borren a , moman mr et al ( 2012 ) pathologic validation of a model based on diffusion - weighted imaging and dynamic contrast - enhanced magnetic resonance imaging for tumor delineation in the prostate peripheral zone . 
bundschuh ra , wendl cm , weirich g et al ( 2013 ) tumour volume delineation in prostate cancer assessed by [ ( 11 ) c ] choline pet / ct : validation with surgical specimens . 
in addition , short - course wbrt mainly with 5 fractions of 4 gy in 1 week or longer - course wbrt programs such as 1415 fractions of 2.5 gy in 3 weeks and 20 fractions of 2 gy in 4 weeks are used . 
patients with a poor expected survival may be appropriately treated with 5 fractions of 4 gy in 1 week instead of 10 fractions of 3 gy in 2 weeks to avoid these patients spending more of their remaining life time with radiotherapy than necessary . 
retrospective studies have suggested that patients with a much more favorable prognosis benefit from longer - course wbrt with total doses higher than 30 gy and doses per fraction of < 3 gy in terms of better outcomes and less neurocognitive deficits [ 2 , 7 , 14 ]  . 
these patients should receive 1415 fractions of 2.5 gy in 3 weeks or 20 fractions of 2 gy in 4 weeks instead of 10 fractions of 3 gy in 2 weeks . 
since different primary tumors may vary with respect to biology and course of the disease , it appears reasonable to create specific survival scores for the most common primary tumors in patients with brain metastasis such as nsclc . patients and methods this study included data of 514 patients who received wbrt alone for brain metab . 
2 univariate analysis of survival at 6 months and at 12 months survivalrateat6 months ( % ) survivalrateat12 months ( % ) pvalue original article wbrtschedule 5 fractions of 4 gy 10 fractions of 3 gy 61 years 62 years gender female male karnofskyperformancescore brainmetastases ( n ) extracranialmetastase intervaltumordiagnosistowbrt < 3 months 3 months 61 vs . 
three groups were formed according to the total score : 59 points ( group a ) , 1112 points ( group b ) , and 15 points ( group c )  . 
the p values were p = 0.30 for the comparison of both groups a , p = 0.92 for the comparison of both groups b , and p = 0.99 for the comparison of both groups c , respectivetab . 
62 years , medi778 | strahlentherapieundonkologie92013 abstract zusammenfassung discussion strahlenther onkol 2013 189 : 777781 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0362 - x wbrt alone is still the most common treatment of brain metastasis [ 6 ]  . 
patients with a poor prognosis would benefit from a short course of wbrt such as 5 fractions of 4 gy given in 1 week , which has been reported to be similarly effective with respect to survival and local control as longer wbrt programs such as 10 fractions of 3 gy in 2 weeks [ 11 ]  . 
patients with a relatively favorable survival prognosis are better treated with longer course wbrt including doses per fraction of < 3 gy , because these patients may live long enough to experience such deficits . 
therefore , it is important to be able to estimate the patients survival prognosis in order to administer the most appropriate treatment regimen . estimating the patients survival time can be facilitated with the help of prognostic scores . 
several survival scores already exist for patients with brain metastasis but have been developed in heterogeneously treated series of patients and in series of patients with many different primary tumors [ 3 , 9 , 10 ]  . 
since the biological behavior of the various primary tumors may be quite different , it appears reasonable to create separate survival scores for the most common tumor entities associated with brain metastasis . 
nsclc is the most common primary tumor in patients with brain metastasis and accounts for about 40% of these patients [ 6 ]  . the current score included three independent predictors of survival , gender , kps , and extracranial metastases . 
in the multivariate analysis of the test group , gender , performance status , and extracranial metastases were independent predictors of survival and , therefore , included in the scoring systethe score for each of the three factors was obtained from the 6 - month survival rate ( in % ) divided by 10 . 
it can help predict the survival of patients with brain metastasis from nsclc . keywords brain metastasis whole - brain radiotherapy non - small cell lung cancer survival prognosis score ein neuer berlebensscore fr patienten mit hirnmetastasen eines nicht - kleinzelligen lungenkarzinoms zusammenfassung hintergrundundziel . 
die berlebensraten nach 6 monaten in der testgruppe waren 9% bei 59 punkten ( gruppe a ) , 54% bei 11 12 punkten ( gruppe b ) und 79% bei 15 punkten ( gruppe c )  . 
er kann dazu beitragen , die berlebensprognose von patienten mit hirnmetastasen eines nsclc abzuschtzen . schlsselwrter hirnmetastasen ganzhirnbestrahlung nicht - kleinzelliges bronchialkarzinom berlebensprognose score vival rates of the three groups were very different . 
patients of group a had the worst survival prognosis with a 6 - month survival rate of only 9% and , therefore , should be considered for short - course wbrt such as 5 fractions of 4 gy in 1 week . 
he surmised that tumor cells exhibit defective mitochondria forcing these cells to ferment glucose to lactate , which he thought to be the origin of cancer [ 15 ]  . 
in recent decades it became clear that tumor cells do not necessarily harbor defective mitochondria , but that most genes involved in glucose transport and glycolysis are consistently up - regulated and / or transactivated ( in 70% of human cancers worldwide glycolytic genes are over - expressed [ 1 ] )  . 
additionally , excessive aerobic glycolysis leads to lactate accumulation in tumors favoring different aspects of tumor progression such as angiogenesis , acidosis , and invasion and metastasis of cells , as well as tumor immune escape [ 5 , 6 ]  . different studies showed that lactate accumulation in tumor tissue is significantly correlated with a poor clinical prognosis in a variety of tumor entities [ 14 , 19 ]  . 
another study showed that therapeutic effectiveness of radiation treatment also seemed to be influenced by lactate accumulation : high lactate content in xenografts of 10 cell lines of head and neck squamous cell carcinomas ( hnscc ) correlated significantly with a higher local tumor control dose after fractionated irradiation [ 10 ]  . 
taken together these studies not only found lactate to be linked to tumor aggressiveness but also to be a prognostic marker for tumor radiation sensitivity . although lactate accumulation correlated with radioresistance , no predictive information of the success of an applied radiation therapy could be deduced for individual tumors . 
as conventional fractionated radiation treatment of hnsccs is given by 2 gy over a period of 57 weeks [ 2 ] , it would be advantageous to predict tumor responsiveness and probable therapeutic success in an early treatment stage to possibly adjust individual tumor therapy . 
metabolites ( especially atp and lactate ) and glycolysis - related gene expression during early treatment phases were studied in tumors that were irradiated in a clinically relevant fractionation scheme of up to 782 | strahlentherapieundonkologie92013 original article time / days excision of tumor irradiation with 2 gy fig . 
especially atp content might easily be determined in a clinical set - up using nmr techniques . materials and methods animals , tumor cell lines , and irradiation the experiments were done using 4 established human hnscc lines : ut - scc - 14 , fadu , sas , and ut - scc - 5 , which have been previously described [ 4 , 16 , 18 ]  . 
animal handling , tumor transplantation , and fractionated irradiation was performed in dresden , where the animal facilities and the experiments were approved according to the institutional guidelines and the german animal welfare regulations . 
when reaching a diameter of 7 mm , tumors were either excised and snap frozen as non - irradiated control tumors or irradiated with 3 , 5 , 10 or 15 equal fractions ( fx ) over 3 weeks and were excised 24 h after the last fraction was given . 
in a parallel study , radiation sensitivity was determined as local tumor control and the dose needed to cure 50% of the tumors [ tumor control dose 50 ( tcd50 ) ] was used to quantify radiation response . 
these results led to the classification of radiosensitive ( ut - scc - 14 ) , intermediately radiationresistant ( fadu ) , and radioresistant tumor xenografts ( sas , ut - scc - 5 ) , which is also used here ( for further details see [ 17 ] )  . induced metabolic bioluminescence imaging metabolic concentrations of atp and lactate in tumor xenografts were determined using induced metabolic bioluminescence imaging ( imbi ) as described earlier [ 6 , 10 ]  . 
briefly , consecutive cryosections were used for metabolic measurements and were brought into contact with an enzymatic solution quantitatively coupling the metabolic degradation of atp or lactate to the enzymatic emission of light . 
 light intensity was calibrated to local metabolite concentration in mol / g tissue in vital tumor areas for all tumors measured using parallel h&e stained cryosections for orientation and overlay . quantitative pcr mrna expression of 6 glycolysis - related genes were determined using quantitative real - time rt - pcr . 
the remaining tissue of xenografts that were used for imbi , were lysed , and mrna was extracted ( nucleospin total mrna - protein extraktion kit , macherey - nagel , due ren , germany )  . 
tbp was used as a reference gene ( hs00427620_m1 ) and showed no changes in mrna expression during the course of a fractionated irradiation ( data not shown )  . 
the acquired data were analyzed following the ct method relative to a calibrator ( mrna from a cell lysate used in every run )  . in this study 1012 xenografts were transplanted for every cell line for each irradiation group . 
statistically significant changes in metabolite content or mrna expression during fractionated irradiation compared to unirradiated or with 3 fx irradiated xenografts ( as indicated ) were determined using students t - test : p < 0.05. results atp and lactate levels of hnscc xenografts ( ut - scc - 14 , fadu , sas , and utscc - 5 ) were measured at five different time points ( after 0 , 3 , 5 , 10 and 15 fx ) during a 3 week treatment . 
in three out of four xenograft cell strahlentherapieundonkologie92013 | original article abstract zusammenfassung strahlenther onkol 2013 189 : 782788 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0371 - 9 k.goetzes.s.meyera.yarominad.zipsm.baumannw.mueller - klieser glycolysis - related gene induction and atp reduction during fractionated irradiation . 
tumors were irradiated with up to 15 fractions of 2 gy over a period of 3 weeks , and atp and lactate levels were measured in vital tumor areas with induced metabolic bioluminescence imaging . 
sensitivity - related differences in the transcriptional response of tumors to radiotherapy may be exploited in the clinic for better individualization of tumor treatment . keywords glucose metabolism transplantation , heterologous carcinoma , squamous cell mrna expression induced metabolic bioluminescence imaging glykolyse - assoziierte geninduktion und atp - absenkung whrend fraktionierter bestrahlung . 
similar observations were made for tumor glucose content ( data not shown )  . to elucidate whether the changes in metabolite concentrations during fractionated irradiation were directly linked to changes in expression levels of glycolysis - related genes , 6 genes ( hk2 , gpi , pfk2 , pkm2 , pdk1 , and mct1 ) were investigated using quantitative real - time rt - pcr . 
although for all tumor lines and irradiation groups 1012 xenografts were transplanted , only four ut - scc - 14 xenografts irradiated with 10 fx yielded enough mrna for further analy sis . 
in three cases ( hk2 , pdk1 , and mct1 ) further irradiation led to a subsequent significant decrease in mrna levels after 5 and / or 10 fx when compared to tumors irradiated with 3 fx . 
 784 | strahlentherapieundonkologie92013 ut - scc - 14 fadu number of fractions number of fractions ut - scc - 5 number of fractions number of fractions 40 ut - scc - 14 fadu number of fractions number of fractions ut - scc - 5 fig . 
circles depict means ( sd ) of all tumors measured ( 513 per treatment group ) ; dotted lines indicate mean of untreated control and continuous lines illustrate changes during fractionated irradiation . 
3 9 lactate content in vital tumor regions of three out of four tested tumor cell lines was significantly reduced after 10 and / or 15 fractions ( a , b , d ) , respectively . 
depicted in circles are means ( sd ) of all tumors measured ( 513 per treatment group , when only 2 tumors were measured the results are shown as single measurements ) ; dotted lines indicate mean of untreated control and continuous lines illustrate changes during fractionated irradiation . 
4 9 relative mrna expression of the glycolysisrelated genes hk2 , pfk2 , and pdk1 increased in radiosensitive and intermediately radioresistant tumor xenografts ut - scc - 14 ( a , c , e ) and fadu ( b , d , f ) after three fractions compared to unirradiated controls . 
circles depict means ( sd ) of all tumors measured ( 413 per treatment group , when only two tumors were measured the results are shown as single measurements ) ; dotted lines indicate mean of untreated control and continuous lines illustrate changes during fractionated irradiation . 
statistically significant changes were determined using students ttest : * p < 0.05 ( irradiated tumors compared to untreated controls ) , #p < 0.05 ( tumors irradiated with 5 , 10 , or 15 fractions compared to xenografts treated with only 3 fractions ) number of fractions number of fractions discussion the study presented herein focused on changes in tumor metabolism during fractionated irradiation using a clinical radiation scheme . 
although tumor size in general differed between radiosensitive and radiation - resistant tumors , the relative amount of vital tumor area decreased in both cell lines significantly and to the same extent during treatment . 
the observed atp reduction therefore represents a decrease in metabolic activity in vital tumor regions in radiosensitive xenografts . although lactate was previously shown to be a prognostic pretherapeutic marker for radiation resistance , the prognostic value of the metabolite was not enhanced during fractionated irradiation . 
5 9 relative mrna expression of the glycolysis - related genes hk2 , pfk2 , and pdk1 in radioresistant tumor xenografts sas ( a , c , e ) and ut - scc - 5 ( b , d , f ) during fractionated irradiation . 
circles depict means ( sd ) of all tumors measured ( 512 per treatment group ) ; dotted lines indicate mean of untreated control and continuous lines illustrate changes during fractionated irradiation . 
statistically significant changes were determined using students ttest : * p < 0.05 ( irradiated tumors compared to untreated controls ) , #p < 0.05 ( tumors irradiated with 5 , 10 , or 15 fractions compared to xenografts treated with only 3 fractions ) number of fractions number of fractions treatment . 
 [ 7 ] measured changes in the lactate / h2o ratio using 1h mrs in non - hodgkin lymphoma xenografts and found a significant reduction after a 15 gy single dose irradiation . 
 [ 11 ] irradiated rat rabdomyosarcoma in a fractionated schedule and a total dose of 75 gy over 5 weeks ( 5 fx of 3 gy per week ) and could show a steady decline in atp content and only slightly changing lactate levels . 
our total radiation dose amounted to 30 gy , and in this range the data were comparable . this study represents the first approach to investigating the metabolic status as well as the mrna expression of glycolysis - related genes in tumor xenografts during fractionated irradiation . 
yaromina a , krause m , thames h et al ( 2007 ) pretreatment number of clonogenic cells and their radiosensitivity are major determinants of local tumour control after fractionated irradiation . 
yaromina a , kroeber t , meinzer a et al ( 2011 ) exploratory study of the prognostic value of microenvironmental parameters during fractionated irradiation in human squamous cell carcinoma xenografts . 
yaromina a , zips d , thames hd et al ( 2006 ) pimonidazole labelling and response to fractionated irradiation of five human squamous cell carcinoma ( hscc ) lines in nude mice : the need for a multivariate approach in biomarker studies . 
ziebart t , walenta s , sattler u et al ( 2010 ) metabolite - induced bioluminescence for tumor prediction : detection of metabolites in tumors of the head and neck region . 
when radiation damage becomes too extensive , the initially increased mrna expression and the elevated atp content cannot be sustained , leading to a concomitant significant reduction in mrna and atp levels in the course of further irradiation . 
radiation - resistant cell lines seem to be able to keep a constant energy level without early changes in mrna expression or atp levels during fractionated irradiation . although changes in lactate content in the present study are not linked to tumor responsiveness and therapeutic outcome , an interrelationship between tumor metabolism and radiation sensitivity can be deduced from the results presented hereas shown earlier the pretherapeutic lactate content in tumor xenografts is correlated with radiation resistance . 
furthermore , as documented here , radiation therapy in turn impacts mrna expression of glycolysis - related genes and atp content in radiosensitive but not radioresistant tumors in the course of a fractionated irradiation scheme . 
by measuring atp levels in tumor biopsies before and after 10 fx and determining pdk1 , pfk2 , and hk2 mrna levels pretherapeutically and after only three fractions it might be possible to personalize and adjust radiation treatment . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 273274 doi 10.1007s00066 - 013 - 0305 - 6 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
kneschaurek , klinik fr strahlentherapie der technischen universitt , klinikum rechts der isar , ismaninger strae 22 , d - 81675 mnchen , telefon ( + 49 / 89 ) 4140 - 4504 , fax - 4881 hellenic society of radiation oncology , p . 
 es handelt sich um den hermann - holthusen - preis , alfred - breit - preis , dissertationspreis , innovationspreis , preis zur hochprzisions - strahlentherapie , gnther - von - pannewitz - preis sowie den koester - preis . informationen : anmeldung : weiterbildungsveranstaltung titel : sterreichische weiterbildungsveranstaltung klinische strahlenbiologie fr rzte in der weiterbildung zum radioonkologen ort : akh wien zeit : 10.13.04.2013 kursdirektoren : wolfgang drr , edgar selzer , richard ptter kontaktadresse : universittsklinik fr strahlentherapie medizinische universitt / akh wien whringer grtel 18 - 20 , a - 1090 wien , sterreich tel . 
 alle relevanten informationen ( vorlufiges programm , anmeldeformular , etc . ) werden auf der internetseite der sterreichischen gesellschaft fr radioonkologie , radiobiologie und medizinische radiophysik ( gro ) , unter in der rubrik „kongresse & veranstaltungen“ zur verfgung gestellt . 
 strahlentherapie und onkologie 3 2013 | mitteilungen der fachgesellschaften personalia die hermann - strebel - medaille , welche die deutsche gesellschaft fr radioonkologie ( degro ) , die sterreichische gesellschaft fr radioonkologie ( gro ) und die scientific association of swiss radiation oncology ( sasro ) alle zwei jahre fr langjhrige , herausragende leistungen auf dem gebiet der brachytherapie im deutschsprachigen raum vergeben , erhielt am 08 . 
seine schwerpunkte waren die elektrotherapie , die phototherapie und eben die brachytherapie . jubilare die fachgesellschaften von strahlentherapie und onkologie gratulieren zum geburtstag : 05.03.2013 mnchen : pd johann kummermehr 75 jahre 21.03.2013 mnchen : gerhard sennewald 75 jahre 29.03.2013 essen : frau marianne engelhard 65 jahre 30.03.2013 essen : ulrich quast 75 jahre 274 | strahlentherapie und onkologie 3 2013 laudatio strahlenther onkol 2013 189 : 262262 doi 10.1007 / s00066 - 013 - 0318 - 1 online publiziert : 9 . 
beisitzer des vorstands die berufspolitischen geschicke des berufsverbands . er hat sich vom beginn seiner vorstandsttigkeit sehr gewissenhaft und mit groem interesse in den vorstandsressorts abrechnungswesen , vertragswesen und weiterbildung engagiert . 
seit 2005 ist herr thiel als vertreter des bvdst zudem vorstandsmitglied in der akademie fr fortund weiterbildung in der radioonkologie der degro und des bvdst und hat hier insbesondere an der erstellung der weiterbildungsordnung fr die fakultative zusatz - weiterbildung fr interventionelle strahlentherapie ( brachytherapie ) und der dazugehrigen prfungsordnung mitgewirkt . 
seit vielen jahren zeigt herr thiel weiterhin sehr groes engagement in der fortbildung der sekretrinnen und assistentinnen aus der radioonkologie im bereich der strahlentherapeutischen abrechnung und schult die mitglieder der oviro e . 
 ( frher degro - office ag ) alljhrig im rahmen eines 2 - tgigen gound ebmabrechnungsseminars in kassel . herr thiel wird von seinen vorstandskollegen ausnahmslos als fachkompetenter und angenehmer gesprchsund diskussionspartner geschtzt . der vorstand dankt herrn prof thiel fr seinen bisherigen einsatz und sein langjhriges engagement fr den berufs262 | strahlentherapieundonkologie32013 original article strahlenther onkol 2013 189 : 216222 doi 10.1007 / s00066 - 012 - 0257 - 2 revised : 19 june 2012 accepted : 17 october 2012 published online : 27 . 
the saliva - producing acinar cells are primarily affected , although the ducts themselves usually remain intact [ 10 ]  . the consequences of xerostomia affect many aspects of the patients life . 
consequently , xerostomia has a profound effect on the patients quality of life ( qol ) and considerable effort goes into reducing this side effect of radiotherapy . studies suggest substantial recovery of parotid gland function is possible if the mean radiation dose to the parotid glands is < 26 gy [ 6 , 22 ]  . 
in one study , radiationinduced damage was reversible when doses of 2030 gy were given , whereas a cumulative dose of > 75 gy resulted in extensive degeneration of the acini along with inflammation and fibrosis of the interstitium [ 5 ]  . 
 [ 4 ] reported the median toxic dose ( td50 ) in patients receiving radiotherapy for head and neck cancer , i.e. , the uniform dose leading to a 50% probability of complications , where a complication was defined as a reduction in the parotid gland flow rate to < 25% of the pretreatment value . 
 one year after radiotherapy , the td50 was 40 gy ; patients who received doses of 25 30 gy had a 1726% probability of experiencing complications at this time point . intensity - modulated radiotherapy ( imrt ) is now a standard practice in radiotherapy [ 16 ] that allows more precise targeting of the tumor and thereby limits toxicity in the adjacent organs at risk . 
helical tomotherapy is a computed tomography - based platform for imrt that aims to deliver the lowest doses to the parotids and other organs at risk , while homogeneously covering the target volume . 
helical tomotherapy has been shown to provide superior target coverage and homogeneity and parotid sparing compared with imrt in patients with head and neck cancer [ 15 ]  . studies often only report the mean radiotherapy dose to both parotid glands , making it difficult to assess the extent of damage to the individual glands and to quantify the clinical benefit to the patient of parotid sparing . 
in such a case , the mean dose to the parotids would be 24 gy , raising the question of whether there is any clinically relevant difference between this patient and another who also receives a mean dose of 24 gy , but in whom neither gland receives more than 26 gy . 
this prospective study was designed to determine whether sparing one or both parotid glands is beneficial for patients with head and neck cancer . methods patients imrt has been routinely used for the treatment of patients with head and neck cancer at our institution for over 10 years . 
 the first two authors contributed equally to the authorship of the manuscript . 216 | strahlentherapieundonkologie32013 between january 2007 , when helical tomotherapy commenced in our institution , and december 2011 , consecutive patients with locally advanced squamous cell carcinoma of the head and neck were prospectively treated with curative intent using this technique . 
patient characteristics , tumor , and treatment data were prospectively collected in a research database and retrospectively evaluated : sex , age , karnofsky performance status , smoking habit , tumor site , t stage , n stage , grade , surgery ( yes / no ) , chemotherapy dose , and radiotherapy dose and fractionation . 
patients received 70 gy in 2 gy fractions to the primary tumor if they had definitive radiotherapy and 6066 gy in 2 gy fractions if radiotherapy was administered after surgery . 
those with definitive radiotherapy received concurrent platinum - based chemotherapy ( cisplatin 100 mg / m2 on days 1 , 22 , and 43 or 30 mg / m2 weekly for the duration of radiotherapy )  . 
in the adjuvant setting , concurrent chemoradiotherapy was given to patients with one major risk factor or 2 minor risk factors according to national comprehensive cancer network guidelines [ 16 ]  . organs at risk were defined during treatment planning and prioritized in the planning algorith the radiotherapy dose was evaluated without compromising homogeneous coverage of planning target volumes ( tumor site , primary neck nodes , and supraclavicular region )  . 
sparing of the parotids was determined during contouring , depending on the tumor site and neck node bulk . helical tomotherapy planning parameters a planning ct scan with 3 mm slice thickness was acquired . 
contouring was performed with cms focal software ( elekta , stockholm , sweden ) , inverse treatment planning with the hiart tomotherapy planning station version 4.0.5 ( tomotherapy incorporated , madison , wi , usa )  . 
acute and late toxicities were systematically evaluated every month for the first 3 months and at 3 - month intervals thereafter and scored according to radiation therapy oncology group acute radiation morbidity criteria and the radiation therapy oncology group / european organisation for research and treatment of cancer late radiation morbidity criteria . 
the data presented here were recorded at the last follow - up visit for each patient . statistical analysis patients were retrospectively classified into two treatment groups : f patients in group a received a dose of < 26 gy to both the left and right parotids ; f patients in group b received a dose of < 26 gy to either the left or the right parotid . statistical calculations were performed with jmp software , version 9.0.2 ( sas institute inc , cary , nc , usa )  . 
to identify statistically significant relationships between both patient groups and clinical parameters , the 2 likelihood test was used for categorical variables and an analysis of variance test was used for continuous variables . 
a logistic regression model was calculated to predict the likelihood of xerostomia after therapy and included the following clinical parameters : surgery , chemotherapy , union for international cancer control stage , and dichotomized radiation dose . 
kaplanmeier analyses and log - rank tests were used to analyze the probability of tumor recurrence and overall survival in both patient groups . patients were followed monthly for the first 3 months and every 3 months thereafter . 
patients with locally advanced squamous cell carcinoma of the head and neck received definitive ( 70 gy in 2 gy fractions ) or adjuvant ( 6066 gy in 2 gy fractions ) curative - intent radiotherapy using helical tomotherapy with concurrent chemotherapy if appropriate . 
sparing both parotids while maintaining target volume coverage and clinical outcome should be the treatment goal and reporting radiotherapy doses delivered to the individual parotids should be standard practice . keywords helical tomotherapy radiotherapy , intensity modulated head and neck cancer survival analysis parotid gland xerostomie nach strahlentherapie . 
patienten mit lokal fortgeschrittenem plattenepithelkarzinom im kopf - hals - bereich wurden primr ( 70 gy , 2 gy pro fraktion ) oder adjuvant ( 60 66 gy , 2 gy pro fraktion ) mit kurativer intention mit der helikalen tomotherapie bestrahlt . 
diese ergebnisse zeigen , dass siginifikant weniger patienten eine xerostomie und dysphagie entwickeln , wenn beide parotiden mit < 26 gy belastet werden , ohne dass das gesamtberleben oder das rezidivfreie berleben negativ beeintrchtigt werden . schlsselwrter helikale tomotherapie intensittsmodulierte strahlentherapie kopf - hals - karzinom xerostomie parotis tab . 
grade 1 xerostomia was significantly higher among those who received a radiotherapy dose < 26 gy to both parotids compared with those in whom only one parotid gland was spared , although the proportion of patients with grade 2 xerostomia was similar in both groups . 
notably , patients in whom only one parotid was spared did not have statistically significantly more advanced disease at baseline than those in whom both parotids were spared during treatment . other consequences of parotid sparing included a significantly reduced incidence of dysphagia and the reduced likelihood of needing a percutaneous endoscopic gastrostomy for feeding at the last followup visit in patients in whom both parotids were spared . 
although these early data appear promising , the follow - up time ( mean 15 months ) is too short to definitively determine any possible impact of parotid sparing on survival and longerterm follow - up is required to realistically estimate local control and survival probability . 
long - term survival with acceptable functional ability is becoming increasingly important for patients with head and neck cancer , although patients have been shown to be unwilling to compromise their survival in return for fewer side effects [ 2 ]  . 
in one study , patients given a choice of radiotherapy or chemoradiotherapy with different outcome scenarios were unwilling to tolerate the less intensive treatment if a reduction in survival of < 5% resulted [ 2 ]  . 
the demographics of head and neck cancer are changing to include a larger proportion of younger patients with better - prognosis human papillomavirus - positive disease [ 19 ] and fewer patients with head and neck cancers related only to the traditional risk factors of cigarette smoking and alcohol consumption [ 13 , 24 ]  . 
therefore , awareness of the late side effects of therapy , in particular salivary function , is becoming increasingly important in planning treatment . other studies have investigated parotid sparing , xerostomia , and survival associated with imrt vs . 
 [ 18 ] reported that imrt ( mean dose of 42 and 41 gy to the ipsilateral and contralateral parotid glands , respectively ) was associated with significantly higher saliva flow rates after treatment for nasopharyngeal cancer compared with conventional radiotherapy . 
others have reported that percutaneous endoscopic gastrostomy dependency was reduced in patients treated with imrt compared with concomitant boost radiotherapy [ 12 ] , although to the best of our knowledge , no such data are available for patients treated with tomotherapy . 
knowing in advance that a percutaneous endoscopic gastrostomy is unlikely to be necessary may save the patient from additional procedures that , although mostly benign , are occasionally associated with complications such as local site infection , tube blockage , and migration or dislodgement . 
therefore , targeted radiation delivery using imrt may help prevent unnecessary interventions in patients with head and neck cancer . multivariate analysis identified two independent factors influencing xerosto220 | strahlentherapieundonkologie32013 100 r + l < 26 gy r or l < 26 gy time after therapy ( months ) r + l < 26 gy r or l < 26 gy time after therapy ( months ) fig . 
1 9 relapse - free survival ( top ) and overall survival ( bottom ) according to radiation dose to the parotid glands in patients with head and neck cancer . 
the multivariate analysis did not identify concurrent chemotherapy as a factor for any grade xerostomia , which is in line with other observations that concurrent chemotherapy did not increase the risk of xerostomia in patients [ 1 ]  . although qol was not investigated in the present study , studies have shown that qol is adversely affected by xerostomia [ 17 , 18 , 25 ] and dysphagia [ 8 , 14 ]  . 
 many patients with locally advanced head and neck cancer , particularly those with tumors in the oropharynx and concomitant infection with human papillomavirus , can now expect prolonged survival [ 24 ]  . 
consequently , preserving qol in these patients is growing in importance , bearing in mind the increasing complexity of treatments available [ 7 , 11 , 20 , 23 ]  . some limitations of the present study should be considered . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . erratum strahlenther onkol 2013 189 : 271272 doi 10.1007 / s00066 - 013 - 0317 - 2 published online : 13 . 
februar 2013 springer - verlag berlin heidelberg 2013 r.sauer1c.wild2 1 department of radiooncology , university erlangen - nuremberg , erlangen 2 ludwig boltzmann institute for health technology assessment , vienna erratumto : shouldhyperthermiabeincludedinthe benefitcatalogueforoncologicindications ? strahlentherapieundonkologie189 : 8186 theonlineversionoftheoriginalarticlecanbefoundatdoi 10.1007 / s00066 - 012 - 0265 - 2 the authors regret a typing error on page 84 in the section authors reply by r . 
brix ( neuherberg ) sauerwein , wolfganga.g. ; wittigandrea ; moss , raymond ; nakagawa , yoshinobu ( hrsg . ) neutron capture therapy principles and applications berlin : springer 2013 , 1 . 
 dabei ist zunchst erforderlich , dass nicht radioaktives lob in ausreichender menge von der tumorzelle aufgenommen wird , das dann durch interferenz mit thermischen neutronen zu der genannten kernreaktion fhrt . 
 die physikalische , chemische , pharmakologische und biologische problematik der anwendung dieser binren bestrahlungsmethode wird in aller ausfhrlichkeit dargelegt , einschlielich bisheriger ergebnisse , laufender studien und zuknftigen anwendungsmglichkeiten , die sich auf maligne meningeome , spinale gliome , kopf - halstumoren , schilddrsen - tumoren , maligne melanome und mamma - karzinome beziehen . insgesamt stellt das buch einen umfassenden querschnitt des aktuellen wissensstandes dieses fachgebietes dar . 
schmitt ( dsseldorf ) buchbesprechungen alexanderkaul ( hrsg ) medical radiological physics , landolt - brnstein numerical data and functional relationships in science and technology group viii volume 7a berlin , heidelberg , new york : springer - verlag 2012 , 300 s . , ( isbn 987 - 3 - 642 - 23683 - 9 ) vor 130 jahren war die welt der physik noch berschaubar und die wichtigsten daten lieen sich in einem schmalen band zusammenfassen . 
die seit 1961 herausgegebene neue serie umfasst bereits mehr als 400 einzelbnde , in denen nicht nur daten zu neuen spezialgebieten zusammengetragen sind , sondern zunehmend auch die fachlichen grundlagen dieser gebiete zusammenfassend dargestellt werden . 
besonders hervorzuheben ist , dass mit ausnahme der beiden dosimetriekapitel durchgngig auf ionisierende und nicht - ionisierende strahlung eingegangen wird , wobei letztere nicht nur elektrische , magnetische und elektromagnetische felder ber den gesamten frequenzbereich ( einschlielich optischer strahlung und laser ) umfasst , sondern auch den ultraschall . 
abgerundet wird das werk durch ein 32 - seitiges glossar . dem charakter des landolt - brnstein entsprechend handelt es sich auch bei dem vorliegenden band nicht um ein lehrbuch , das die grundlagen des fachgebiets systematisch und didaktisch geschickt entwickelt , sondern um ein handbuch , in dem die wichtigsten fakten , beziehungen und daten zusammengestellt sind . 
obwohl sich das umfangreiche werk primr an praktizierende und ange272 | strahlentherapieundonkologie32013 original article strahlenther onkol 2013 189 : 197201 doi 10.1007 / s00066 - 012 - 0283 - 0 received : 30 june 2012 accepted : 15 november 2012 published online : 19 . 
 modification of initial staging has impact on the radiotherapy ( rt ) planning and particularly in terms of m staging on radiotherapeutic intention [ 11 , 21 , 25 ]  . 
both modalities , relaying on certain morphological criteria like size and contrast enhancement pattern , provide anatomic information about locoregional tumor status as well as distant metastases [ 16 , 17 , 19 , 34 ]  . 
 moreover , it was shown that for the palpably n0 neck , for level ii a criterion of 7 mm was optimal , whereas for the rest of the neck , lymph nodes with a minimal diameter of 6 mm should be considered suspicious [ 30 ]  . otherwise , 40% of lymph nodes larger than 1 cm were demonstrated to be benign [ 28 ]  . 
using 10 mm diameter as the threshold , the quoted specificities are as low as 39% and 48% for ct and mri , respectively , for the detection of nodal metastases in hnc [ 4 ]  . 
in the meantime , fluorine18 - 2 - fluoro - 2 - deoxy - d - glucose positron emission tomography ( fdg - pet ) combined with ct in a single device ( fdgpet / ct ) was shown to be highly accurate and efficient diagnostic approach by staging of different tumor entities [ 1 , 2 , 6 , 7 , 33 ]  . 
delivering little information on t - stage following anatomical imaging , fdg - pet / ct provides important additional information concerning n and m stage of disease [ 27 , 32 ]  . 
in case of nodal staging , agreement between the imaging results and pathology findings is stronger for fdg - pet / ct ( 0.95 , 95% confidence interval [ ci ] 0.820.99 ) than for ct imaging alone ( 0.81 , 95% ci 0.630.91 ) [ 27 ]  . 
 [ 3 ] implementation of fdg - pet / ct into tumor volume delineation decreases the standard deviation of interobserver variability by a factor of 4 as compared to noncontrast - enhanced ct . 
 [ 22 ] do not support nodal therapy planning based on fdg - pet / ct alone . taking into account , the scarceness of data available , we attempted to clarify the role of fdg - pet / ct in inoperable hnc patients scheduled for irradiation . 
the aim of this study was to compare hnc staging before and after fdgpet / ct and determine the significance of the stage modifications for radiotherapy planning . patients and methods patients a total of 102 patients with untreated primary hnc scheduled for rt were enrolled in this retrospective study . 
of the 102 hnc patients , 2 were referred in clinical stage i , 2 more in stage ii , 18 ( 17.6% ) in stage iii and 80 ( 78.4% ) in clinical stage iv . 
1 comparison of t staging with and without inclusion of fdg - pet / ct dataa including tstaging fdg - pet / ct withoutinclusionof ain 56 patients ( 54.9% ) , t stage was not affected by inclusion of fdg - pet / ct . 
2 comparison of n staging with and without inclusion of fdg - pet / ct data including nstaging fdg - pet / ct withoutinclusionof ain 67 patients ( 65.7% ) , n - stage was not affected by inclusion of fdg - pet / ct . 
bindicates patients in whom fdgpet / ct resulted in upstaging , cindicates patients with downstaging after fdg - pet / ct . 43 a 15 a 13 c study design conventional staging only patients after completion of pre - rt conventional staging were included . 
tumors were located in the following head and neck regions : nasopharynx ( 15 cases ) , oropharynx ( 29 cases ) , hypopharynx ( 40 cases ) , larynx ( 5 cases were supraglottic , 7 cases were glottis and 6 were subglottic )  . 
in most cases , histology revealed squamous cell carcinoma of mucosal origpatients who had had invasive histology sampling before fdg - pet / ct ( e.g. , neck dissection ) or had begun radiotherapy , chemotherapy or concomitant / sequential chemoradiotherapy , all of which could have altered the recognizable extent of the disease and so biased our assessment of the capabilities of fdg - pet / ct , were excluded from the study . conventional staging of hnc consisted of physical examination , ultrasound ( us ) , contrast enhanced ct , fiber - endoscopy and histologic sampling . 
the quality of this staging was acceptable for further rt planning . 18f - fdg - pet / ct staging all patients underwent fdg - pet / ct for tumor staging and rt planning since this method was included into standard patient care procedures in our institution . 
 the patients were placed in the treatment position on the flat - top couch applied onto the conventional curved diagnostic couch of a pet / ct scanner ( biograph 16 , siemens healthcare sector , knoxville , tn , usa )  . 
the q - fix patient positioning device system ( wfr / aquaplast corporation , avondale , pa , usa ) with specific reference marks was used to support further exact positioning of the patient for fdg - pet / ct as well as rt in the linear accelerator . 
examinations were performed from the proximal thigh to the skull base by six to eight table positions ; acquisition time for each position was 3 msubsequently , diagnostic ct with intravenous injection of 1.5 ml / kg body weight of non - ionic iodinated radiographic contrast medium was performed . 
 in all cases , ct scanning was done from the skull base to the proximal thigh with a reconstructed slice thickness of 3 mm and a matrix of 512512 pixels . 
fdg - pet and ct image sets were at first assessed separately , by one radiologist and one nuclear medicine specialist , followed by joint analysis of the fused fdg - pet / ct images by both radiologist and nuclear medicine specialist . 
definitive tnm staging was agreed upon by them in consensus , taking into account the modifications obtained through the use of fdg - pet / ct . radiotherapy planning based on external conventional staging , treatment recommendation towards radiotherapy were provided by the multidisciplinary head and neck tumor board , which includes an experienced radiation oncologist . 
an alternative decision taking into account additional fdg - pet / ct was also made multidisciplinary if the initial intention had to be adjusted in the light of new findings . 
the impact on patient management was tested by comparing the intention before and after fdgpet / ct . statistical analysis pre - fdg - pet / ct and post - fdg - pet / ct staging data were compared to each other using wilcoxon matched - pairs signed ranks test for t , n , and clinical staging and one - sided mcnemars test for matched pairs for m staging . 
our results were calculat198 | strahlentherapieundonkologie32013 ed with help of the biostatistical software package bias for windows ( epsilon - verlag , germany )  . results t staging modifications significant correction in t stage was needed after inclusion of fdg - pet / ct data ( p = 0.002 ) since fdg - pet / ct showed a tendency to classify tumors to be smaller . 
although the majority of 102 patients ( 88 patients ) remained unchanged with regard to m stage and this with no metastases ( m0 ) , 13 of 102 patients were shifted from m0 to m1 . 
 before fdg - pet / ct there was distant metas tatic involvement identified in only 1 of 102 patients , who was later changed to m0 after fdg - pet / ct . abstract zusammenfassung strahlenther onkol 2013 189 : 197201 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0283 - 0 a.abramyuks.appoldk.zphelm.baumannn.abolmaali modification of staging and treatment of head and neck cancer by fdg - pet / ct prior to radiotherapy abstract backgroundandpurpose . 
a total of 102 patients with untreated primary hnc , who underwent conventional staging and staging including fdg - pet / ct before rt , were enrolled in this retrospective study . 
implementation of fdg - pet / ct in imaging protocol improves selection of candidates for curative and palliative rt and allows further optimization of treatment management and therapy intention . keywords fdg - pet / ct radiotherapy planning head and neck neoplasms therapy intention planning techniques modifikation von staging und therapie bei kopf - hals - tumoren durch fdg - pet / ct vor bestrahlung zusammenfassung hintergrundundziel . 
102 konsekutive patienten mit unbehandelten kopf - halstumoren ( kht ) erhielten nach dem klinischen standardstaging , anhand dessen eine strahlentherapie geplant worden wre , ergnzend eine fdg - pet / ct . 
der einsatz der fdgpet / ct bei patienten mit kopf - hals - tumoren vor strahlentherapie ermglicht eine verfeinerte auswahl der kandidaten fr kurative und palliative bestrahlung und fhrt im vergleich zum konventionellen staging zu einer verbesserten therapieentscheidung . schlsselwrter fdg - pet / ct strahlentherapieplannung kopf - hals - tumoren therapieintention planungstechniken radiotherapy intention modifications rt intention shifted from curative to palliative in 12 of 102 patients . 
overall , the inclusion of fdg - pet / ct led to modification of rt intention decision in 14 patients . discussion the present paper focuses on the impact of fdg - pet / ct based staging exerted on strahlentherapieundonkologie32013 | original article tab . 
3 comparison of m staging with and without inclusion of fdg - pet / ct data a mstaging withoutinclusionof a in 88 patients ( 86.3% ) , m stage was not affected by inclusion of fdg - pet / ct . 
b indicates patients in whom fdg - pet / ct resulted in upstaging , c indicates patients with downstaging after fdg - pet / ct . including fdg - pet / ct 88 a 13 b tab . 
4 comparison of clinical staging with and without fdg - pet / ct data overallstaging withoutinclusionof a in 75 patients ( 73.5% ) , clinical stage was not affected by inclusion of fdg - pet / ct . 
5 comparison of radiotherapeutic intention with and without fdg - pet / ct data radiotherapyintention withoutinclusionof ain 88 patients ( 86.3% ) , radiotherapeutic intention was not affected by inclusion of fdg - pet / ct . 
the results demonstrate an evident benefit from adding a fdg - pet / ct to conventional imaging such as ct and mri in pre - rt staging of patients with locoregionally inoperable hnc . due to anatomical complexity of head and neck regions , generally low specificity in characterization of enhanced peritumoral soft tissues and distinction between tumor infiltration and inflammation or fibrosis [ 5 ] , anatomical imaging have tendencies to overestimate tumor extension . 
 [ 5 ] shows that tumor volume estimated by ct or mri is almost 107% larger and by fdg - pet / ct46% larger as the appropriate macroscopic surgical specimens volume . 
thanks to the capability of fdg - pet / ct to clarify the equivocal findings of ct and other conventional methods , we modified the initial tstage in 45% of patients mainly through its downstaging . normal sized but nevertheless tumor cell - bearing lymph nodes are a potential source of n stage discrepancy between conventional anatomic and metabolic imaging . 
 [ 20 ] , including 23 patients with head and neck squamous cell carcinoma , reports data where the stage was corrected by fdg - pet / ct in 13% for one observer and in 9% for second observer , compared to our 34% modification . 
from among the three different protocols used in that study ( conventional imaging , additional fdg - pet / ct and fdg - pet / ct alone ) fdg - pet / ct presented the most accurate lymph node staging , although lesions < 15 mm in diameter may still be missed . 
 [ 9 ] showing modification of overall staging and radiotherapeutic intention after fdg - pet / ct in 30.9% of previously untreated hnc patients including finding distant and unresectable disease or secondary malignancies . 
nevertheless , they do not consider fdg - pet / ct capable of replacing neck dissection in detecting occult cervical nodal metastases [ 9 ]  . actually , pet is a whole - body technique and as such it can sweep more distant metastases than locoregionally applicable ct and mri are in a position to do . 
most of them ( 12.8% ) initially staged as m0 , but after fdgpet / ct were found to be m1 due to either higher sensitivity of fdg - pet / ct or to simply the all - in - one advantage of its whole body approach . 
it is worth noting that the addition of fdg - pet / ct proved beneficial even for m upstaged patients since their initial staging was in effect corrected and in this way appropriate therapy applied . fdg - pet / ct has an evident impact on patient management , in particularly through initiation of previously unplanned treatment or through correction of a previously planned therapeutic approach [ 12 , 14 , 18 , 27 ]  . 
 [ 15 ] of 36 consecutive patients aimed at rt treatment planning for hnc found 14% and 25% changes in clinical stage and in rt intention respectively , as a consequence of pet - ct . 
in these patients fdg - pet / ct did not yield sufficient additional information for any modification of radiotherapeutic intention . secondary management modifications ( dose and volume changes ) and the impact of pet / ct on outcome have not been investigated in this study which addressed the change in staging and man200 | strahlentherapieundonkologie32013 21 . 
newbold kl , partridge m , cook g et al ( 2008 ) evaluation of the role of 18fdg - pet / ct in radiotherapy target definition in patients with head and neck cancer . 
rades d , meyners t , kazic n et al ( 2011 ) comparison of radiochemotherapy alone to surgery plus radio ( chemo ) therapy for non - metastatic stage iii / iv squamous cell carcinoma of the head and neck : a matched - pair analysis . 
rades d , seibold nd , gebhard mp et al ( 2011 ) prognostic factors ( including hpv status ) for irradiation of locally advanced squamous cell carcinoma of the head and neck ( scchn )  . 
scarfone c , lavely wc , cmelak aj et al ( 2004 ) prospective feasibility trial of radiotherapy target definition for head and neck cancer using 3 - dimensional pet and ct imaging . 
stuckensen t , kovacs af , adams s et al ( 2000 ) staging of the neck in patients with oral cavity squamous cell carcinomas : a prospective comparison of pet , ultrasound , ct and mri . 
brekel mw van den , castelijns ja , snow gb ( 1998 ) the size of lymph nodes in the neck on sonograms as a radiologic criterion for metastasis : how reliable is it ? ajnr am j neuroradiol 19 : 695700 31 . 
veit p , kuhle c , beyer t et al ( 2006 ) whole body positron emission tomography / computed tomography ( pet / ct ) tumour staging with integrated pet / ct colonography : technical feasibility and first experiences in patients with colorectal cancer . 
wiener e , pautke c , link tm et al ( 2006 ) comparison of 16 - slice msct and mri in the assessment of squamous cell carcinoma of the oral cavity . 
since , however , during this procedure resection of the affected nodes would bias the consequent fdg - pet / ct staging , neither neck dissection nor other invasive procedure were performed as part of the initial conventional staging for this study . 
however , overall the study reflects the clinical situation very well , i.e. , where decisions by experienced multidisciplinary teams are made using already existing diagnostic materials . despite the limitations , our study demonstrates essential influence of fdg - pet / ct on tumor staging and therapy intention in hnc patients scheduled for irradiation . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . nachruf strahlenther onkol 2013 189 : 263263 doi 10.1007 / s00066 - 012 - 0302 - 1 online publiziert : 16 . 
17 , 24939 flensburg hjb@strahlentherapie - fl.de fr uns alle unfassbar haben wir erfahren mssen , dass unser beraus geschtzter kollege und lieber freund roch kowalski im jungen alter von 44 jahren von uns gegangen ist . 
trost kann nur erwachsen aus einer positiven rckbesinnung , was uns roch kowalski gegeben hat . geboren in toru / polen war er nach seinem studium in gdask und hamburg ab 1998 zunchst als assistenz - , fachund oberarzt im hermann - holthusen - institut des ak hamburg , st . 
er pflegte intensiv auch den weiteren kontakt mit den ihm anvertrauten patienten . strahlentherapieundonkologie32013 | original article strahlenther onkol 2013 189 : 238245 doi 10.1007 / s00066 - 012 - 0260 - 7 received : 4 july 2012 accepted : 18 october 2012 published online : 25 . 
in case of primary radiochemotherapy , tumour regression during ebrt and concomitant chemotherapy is a major prognostic parameter for the achievement of local tumour control [ 6 , 7 , 8 ]  . 
in terms of morphologic imaging of cervical cancer , magnetic resonance imaging ( mri ) is currently considered as the gold standard [ 9 , 10 , 11 ]  . 
 during ebrt and chemotherapy the mass with high signal intensity corresponding to the primary tumour shrinks and considerably changes into areas with intermediate signal intensity ( grey zones ) probably as a sign of tumour regression [ 12 , 13 , 14 ]  . 
 the primary aim of this study was to systematically detect and measure the gross tumour volume at the time of diagnosis and the gross tumour volume at the time of brachytherapy with and without consideration of the grey zones , in order to quantify tumour regression during ebrt and concomitant chemotherapy , and to estimate the amount of grey zones at the time of bt . 
the secondary aim was to analyze the impact of various prognostic factors on tumour regression . material and methods patients all patients with cervical cancer ( figo stage ib1iva ) treated between 01 / 1998 and 10 / 2009 at the department of radiotherapy of the medical university of vienna with primary radiochemotherapy and igabt were considered for this study . 
the following tumour volumes were defined : fgross tumour volume inital ( gtvinit ) : macroscopic tumour extension at the time of diagnosis visualized as high signal intensity masses in uterine cervix / corpus , parametria , vagina , bladder and rectum , fgtv residual ( gtvres ) : macroscopic residual tumour extension at the time of brachytherapy visualized as high signal intensity masses in uterine cervix / corpus , parametria , vagina , bladder and rectum and fgtvres plus residual pathologic tissue ( grey zones ; gtvres + gz ) : total residual tumour extension at the time of brachytherapy visualized as high - intermediate signal intensity masses in uterine cervix / corpus , parametria , vagina , bladder and rectum , including grey zones defined as area with intermediate signal intensity within the area of initial tumour extension . tumour regression and grey zone analysis tumour regression was calculated with ( rgz ) and without grey zones ( r )  . 
the following formula was applied for estimating rgz : and the following formula was applied for estimating r : the relative proportion of grey zones at the time of first brachytherapy ( g% ) in relation to the total residual tumour volume at the time of brachytherapy was calculated with the following formula : statistical analysis descriptive analysis of all patient - related parameters and tumour regression - related parameters was performed . 
the black arrow indicates the maximum width of the initial tumour volume ( gtvinit ) , the white arrow indicates the maximum width of the residual tumour volume at the time of brachytherapy ( gtvres ) and the black dotted arrow indicates the maximum width of the residual tumour volume with consideration of grey zones ( gtvres + gz )  . 
tumour volumes and tumour regression in this patient : gtvinit 97 cm3 , gtvres 13.4 cm3 , gtvres + gz 40.1 cm3 , r 86% , rgz 59% ic lymph node staging was performed in the majority of cases . 
the slice thickness was 5 mm with 1 mm intersection gap for the mri before the insertion of the applicator and no intersection gap for the mri after insertion of the applicator with a matrix of 256256 . 
axial and para - axial images were obtained from the level above the uterine fundus to the inferior border of the symphysis pubis below any vaginal tumour extension ; sagittal images were obtained between internal obturator muscles . 
for better depiction of the vaginal wall , marking gel was used in the mri prior to ebrt [ 9 ]  . imaging image analysis all patients underwent mri prior to ebrt and at the time of the first brachytherapy fraction with applicator in place . 
fast spinecho technique , with a repetition time of 4500 ms and an echo time of 96 ms for all images were retrospectively evaluated by two investigators ( ms , bm )  . 
the tumour volume was estimated by using the ellipsoid forabstract zusammenfassung strahlenther onkol 2013 189 : 238245 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0260 - 7 m.p.schmidb.mansmannm.federicoj.c.a.dimopoulousp.george.fidarovaw.drrr.ptter residual tumour volumes and grey zones after external beam radiotherapy ( with or without chemotherapy ) in cervical cancer patients . 
grey zones , which are defined as tissue with intermediate signal intensity in the area of primary hyperintense tumour extension , can be seen during radiation with or without chemotherapy on the t2 - weighted mri in patients with cervical cancer . 
t2 - weighted mri datasets of 175 patients with locally advanced cervical cancer ( figo stage ibiva ) , who underwent combined external beam radiotherapy and brachytherapy with or without concomitant chemotherapy were available for this study . 
the gross tumour volume at the time of diagnosis ( gtvinit ) and at the time of first brachytherapy without ( gtvres ) and with ( gtvres + gz ) consideration of grey zones were measured for each patient . 
differentiation of high signal intensity mass and surrounding intermediate signal intensity grey zones may be reasonable . keywords uterine cervical neoplasms magnetic resonance imaging remission induction residual neoplasms image - guided adaptive brachytherapy residuale tumorvolumen und grauzonen nach externer strahlentherapie ( mit und ohne chemotherapie ) bei zervixkarzinompatientinnen . 
sogenannte grauzonen knnen im verlauf der radiochemotherapie auf der t2 - gewichteten mrt bei patientinnen mit zervixkarzinomen als areal mit intermedirer signalintensitt im gebiet des initialen hyperintensen tumors beobachtet werden . 
t2 - gewichtete mrtdatenstze von 175 patientinnen mit lokal fortgeschrittenem zervixkarzinom ( figo - stadien ibiva ) , die mittels kombinierter ebrt und brachytherapie mit und ohne konkomittante chemotherapie behandelt worden waren , waren fr diese studie verfgbar . 
fr jede patientin wurden das gross tumor volume ( gtv ) zum zeitpunkt der diagnose ( gtvinit ) sowie zum zeitpunkt der brachytherapie mit ( gtvres + gz ) und ohne bercksichtigung der grauzonen ( gtvres ) erfasst . 
 eine mr - tomographische unterscheidung des resttumors zum zeitpunkt der brachytherapie in hohe und intermedire signalintensitt erscheint sinnvoll . schlsselwrter uterine zervixkarzinome magnetresonanztomographie remissionsinduktion residuale neoplasien bild - gesttzte brachytherapie pact of various prognostic parameters on tumour regression and grey zones was determined by kruskalwallis h test and mannwhitney u test . 
the change in signal intensity on t2 weighted mr images may be explained by a reduction of the water content within the initial tumour and a subsequent increasing presence of fibrosis , necrosis and blood caused by radiation [ 12 , 13 , 14 ]  . 
 [ 12 ] observed that signal intensity of the tumour on t2 weighted images initially increased during ebrt , and then , after a ebrt dose of 23.459.4 gy became progressively mixed hyperand hypointense . 
the correlation between preoperative mri and histopathological results revealed that the residual tumour after chemotherapy was corresponding to the hyperintense mass on mri , whereas the area of lower signal intensity was dominated by necrosis and hemosiderin deposits . 
 [ 18 ] showed by correlating mri findings and surgicopathologic results after preoperative radiochemotherapy that in case of uncertain imaging findings in terms of radiotherapy induced sequels , fibrosis , suspicious ( but uncertain ) images suggestive of residual diseasewhich may correspond to the grey zone concept in the present studyin 7 of 16 patients residual tumour cells were found . 
similar observations were reported after preoperative radiochemotherapy in rectal cancer , where the differentiation between fibrosis and residual tumour is challenging , leading to overand understaging of mri compared to histopathologic findings [ 19 , 20 ]  . in this study we analysed the gtv at diagnosis , the residual gtv at brachytherapy with and without consideration of grey zones and the corresponding tumour regression rates during ebrt . 
in literature comparable tumour volumes were reported at the time of diagnosis ranging from 33117.1 cm3 [ 8 , 12 , 21 , 22 , 23 , 24 , 25 , 26 , 27 , 28 , 29 ]  . 
 [ 27 ] a precursor study from the medical university of vienna consisting of 49 patients , who were also mainly included in the present studya mean gtvres with consideration of grey zones of 16 cm3 was shown . 
this difference is probably related to the higher number of patients ( n = 175 ) and the high amount of advanced tumours with figo stage iib and iiib in the present study . 
 significant differences were mainly found for gtvinit and gtvres + gz for patients with figo stages ib , iib and iiib , whereas the tumour regression was not significantly different within the different figo stages . 
currently both low and high field imagers conform to the requirements for pre - radiotherapy mri examination and for brachytherapy mri examination in image guided adaptive brachytherapy and are recommended for visualization of tumour regression ( gtv ) , the definition of grey zones indicating residual pathologic tissue in the area of intial tumour extension and for target volume selection . 
evaluation of the published data on tumour volume selection by high and low field mri shows comparable results at the time of diagnosis and at the time of brachytherapy , however a direct comparison is missing . 
comparable clinical results of image guided adaptive brachytherapy using low and high field mri support also the applicability of the present findings [ 17 , 21 , 29 ]  . due to the slice thickness of 5 mm , larger partial volume effects have to be assumedhowever for all examinations in the same way . 
 partial volume effects are expected to be of minor importance for the diameterbased method in comparison to the roibased tumour volume assessment . furthermore , the assessment of tumour regression in initially small tumours is difficult due to the relatively small capacity of tumor shrinkage during ebrt compared to larger tumours . 
therefore the tumour regression in small tumours may be underestimated . further studies are necessary to investigate the relevance of grey zones by functional imaging such as dynamic contrast enhanced mri , diffusion weighted mri or positron emission tomography which may provide new insights [ 35 , 36 , 37 ]  . 
on behalf of all authors , the corresponding author states the following : the department of radiotherapy at the medical university of vienna receives / received financial and / or equipment support for research and educational purposes from nucletron b.v. , varian medical systems , inc . , and isodose control b.v. literatur kommentiert strahlenther onkol 2013 189 : 264265 doi 10.1007 / s00066 - 012 - 0286 - x online publiziert : 16 . 
januar 2013 springer - verlag berlin heidelberg 2013 th.herrmann dresden bestrahlungsdosenund kataraktratebeiberlebenden deratombombe originalpublikation neriishi k , nakashima e , akahoshi m et al ( 2012 ) radiation dose and cataract surgery incidence in atomic bomb survivors , 19862005 . 
die angaben werden sowohl als err ( exzess relative risk ) als auch alles absolutes risiko ( ear ) pro 10.000 personen / jahr und 1 gy exposition dargestellt . zwar signifikante risiken bei diabetes , angina pectoris , niedrigem bildungsstand und hohen bmi , jedoch beeinflussten diese nicht den radiogenen dosis - effekt - zusammenhang . 
da die dosis - effekt - kurve in beiden modellen linear zum nullpunkt verluft , muss von einem kataraktanstieg auch unter 1 gy ausgegangen werden insbesondere dann , wenn die exposition in jungen jahren erfolgte . 
in einer multivariaten analyse zeigten sich die vorliegende untersuchung reiht sich ein in verschiedene mitteilungen aus den letzten 10 jahren , die auf eine weitaus grere strahlensensibilitt der augenlinse hinweisen , als dies in der vergangenheit mit toleranzdosen von etwa 5 gy angenommen wurde . 
so finden sich bei nachuntersuchungen der liquidatoren des havarierten reaktors in tschernobyl ( schwellendosis 0 , 34 ; [ 5 ] ) sowie auch bei den radiologic technologists in den usa ( erste vernderungen bei 60 mgy ; [ 1 ] ) sowie bei piloten ( erste vernderungen bei 2248 msv ; [ 4 ] ) linsentrbungen bei niedriger dosisleistung und deutlich kleineren dosen als frher angenommen . 
nach diesen studien ist die kataraktrate bereits nach strahlenexpositionen von nur 0 , 5 gy statistisch signifikant erhht . die strahlenschutzkommission [ 2 ] hat sich in einer empfehlung aus dem jahre 2009 zu dieser situation geuert . 
von besonderer relevanz ist dabei , dass die ssk bei beruflichen ttigkeiten , die bekanntermaen mit erhhten linsendosen einhergehen knnen ( interventionelle kardiologische und radiologische verfahren ) , fordert , die linsendosis zu erfassen und die betroffenen personengruppen in eine gezielte medizinische berwachung einzubeziehen . 
beim radioonkologen sollten diese niedrigeren toleranzdosen der augenlinse einerseits bei der bestrahlungsplanung und andererseits natrlich bei entsprechenden interventionellen verfahren auch fr das exponierte personal bercksichtigung finden . literatur kommentiert fazit literatur diestrahlensensibilittderaugenlinseistweitaushher ( schwellendosis < 0 , 5gy ) alsindervergangenheitangenommen ( 5gy ) .darberhinausgehend lassendieseergebnissehinsichtlichder richtigkeitdereinstufungderradiogenenkataraktalsdeterministischestrahlenreaktionenzweifelaufkommen , da inderreferiertenarbeitwieauchinanderenuntersuchungendiedosis - effektkurvelinearbiszumnullpunktverfolgbaristeinkriterium , daseinereinordnungderradiogenenlinsenreaktionin diegruppederstochastischenstrahleneffektenahelegt . thomas herrmann , dresden korrespondenzadresse th . 
chodick g , bekiroglu n , hauptmann m et al ( 2008 ) risk of cataract after exposure to low doses of ionizing radiation : a 20 - year prospective cohort study among us radiologic technologists . 
rafnsson v , olafsdottir e , hrafnkelsson j et al ( 2005 ) cosmic radiation increases the risk of nuclear cataract in airline pilots : a population - based case - control study . 
januar 2013 springer - verlag berlin heidelberg 2013 h.christiansen1h.a.wolff2 1 klinik fr strahlentherapie und spezielle onkologie , medizinische hochschule hannover 2 klinik fr strahlentherapie und radioonkologie , universittsmedizin gttingen primrekurative radiochemotherapiebeim nasopharynxkarzinom kumulativecisplatin - dosis prognostischsignifikant originalpublikation loong hh , ma bb , leung sf et al ( 2012 ) prognostic significance of the total dose of cisplatin administered during concurrent chemoradiotherapy in patients with locoregionally advanced nasopharyngeal carcinoma . 
die daten von 241 patienten wurden ausgewertet , davon befanden sich 13 , 7% im stadium ii , 45 , 2% im stadium iii und 41 , 1% im stadium iv , aber ohne fernmetastasen . 
die kumulative dosis von cisplatin ist fr patienten im stadium ii und iii ein unabhngiger prognostischer faktor bei der simultanen rct eines lokal fortgeschrittenen nasopharynxkarzinoms . kommentar bei der primren strahlentherapie lokal fortgeschrittener kopf - hals - tumoren ist die cisplatinbasierte simultane rct der alleinigen rt berlegen , wobei cisplatin hufig als monotherapie appliziert wird [ 6 ]  . 
 [ 6 ] in einer bersichtsarbeit zur rct lokal fortgeschrittener kopf - hals - tumoren nur von einer studie , die keinen effekt der begleitenden cisplatin - chemotherapie gegenber einer alleinigen rt sah . 
buehrlen m , zwaan cm , granzen b et al ( 2012 ) multimodal treatment , including interferon beta , of nasopharyngeal carcinoma in children and young adults : preliminary results from the prospective , multicenter study npc - 2003 - gpoh / dcog . 
lau h , brar s , hao d et al ( 2006 ) concomitant lowdose cisplatin and three - dimensional conformal radiotherapy for locally advanced squamous cell carcinoma of the head and neck : analysis of survival and toxicity . 
lee n , harris j , garden as et al ( 2009 ) intensitymodulated radiation therapy with or without chemotherapy for nasopharyngeal carcinoma : radiation therapy oncology group phase ii trial 0225 . 
loong hh , ma bb , leung sf et al ( 2012 ) prognostic significance of the total dose of cisplatin administered during concurrent chemoradiotherapy in patients with locoregionally advanced nasopharyngeal carcinoma . 
mertens r , granzen b , lassay l et al ( 2005 ) treatment of nasopharyngeal carcinoma in children and adolescents : definitive results of a multicenter study ( npc - 91 - gpoh )  . 
rades d , fehlauer f , sheikh - sarraf m et al ( 2008 ) toxicity of two cisplatin - based radiochemotherapy regimens for the treatment of patients with stage iii / iv head and neck cancer . 
steinmann d , cerny b , karstens jh et al ( 2009 ) chemoradiotherapy with weekly cisplatin 40 mg / m2 in 103 head and neck cancer patients : a cumulative dose - effect analysis . 
wolff ha , rdel rm , gunawan b et al ( 2010 ) nasopharyngeal carcinoma in adults : treatment results after long - term follow - up with special reference to adjuvant interferon - beta in undifferentiated carcinomas . 
j cancer res clin oncol 136 : 8997 literaturkommentiert nisse der kommentierten arbeit [ 4 ] besttigen dies in einem speziellen patientenkollektiv lokal fortgeschrittener nasopharynxkarzinome der stadien ii und iii , die primr mit einer konkomitanten rct behandelt wurden . bei der bewertung der primren rct von lokal fortgeschrittenen nasopharynxkarzinomen ist aber zu beachten , dass diese im vergleich zu den klassichen plattenepithelkarzinomen im kopf - hals - bereich anderer lokalisation ( mundhhle , larynx , oround hypopharynx ) hufig eine andere pathologie ( undifferenzierte , lymphoepitheliale karzinome ) und eine vllig andere pathogenese aufweisen ( ebv - assoziation , fehlen der klassischen risikofaktoren wie nikotinund alkoholabusus )  . 
so werden kinder und jugendliche mit undifferenzierten nasopharynxkarzinomen seit anfang der 1990er jahre in deutschland im rahmen der gpoh - studien ( npc91 - gpoh , npc - 2003 - gpoh ) behandelt [ 1 , 5 ]  . 
interessante aspekte dabei sind die tatsache , dass zum einen die strahlentherapiedosis im gegensatz zu dosen von mindestens 66 gy oder sogar 70 gy bei erwachsenen [ 3 ] auf 60 gy beschrnkt ist und zum anderen , dass bei der rct lediglich 120 mg / m2 ko cisplatin kumulativ erreicht werden ( 20 mg / m2 ko ber 3 tage in woche 1 und 5 der rt )  . 
clara hospital , basel 9 university hospital frankfurt / main 10 university hospital tbingen 11 university hospital mannheim isthesimultaneouslyintegrated boost ( sib ) techniqueforearly breastcancerreadytobeadopted forroutineadjuvantradiotherapy ? statementofthegermanandtheaustrian societiesofradiooncology ( degro / gro ) adjuvant radiotherapy following breast conserving surgery ( bcs ) is usually performed by homogenous irradiation of the whole breast ( wbi ) , using single doses of 1.82 gy up to total doses around 50 gy , mostly followed by a boost to the tumor bed considered as the area of highest subclinical tumor cell contamination [ 19 ]  . 
this tumor bed boost may be applied using external photon and / or electron beams up to cumulative tumor bed doses of 6066 gy in same fractional dose sizes as the preceding wbi . 
alternatively , higher single fractions around 10 gy are commonly used for either brachytherapy or intraoperative tumor bed boosts ( iort )  . during the last few years , a new method of dose escalation to the tumor bed by a simultaneously integrated boost ( sib , concomitant boost ) was proposed [ 11 ]  . 
 the rationale is a localized dose enhancement in the area at highest risk without prolonging treatment duration , thus not only providing improved patient comfort but also exploiting the higher sensitivity of breast tumor cells towards larger single doses , which has long been postulated in the linear - quadratic model . 
after a median follow - up period of 30 months ( 654 months ) grade 2 fibrosis in the boosted area was observed in 8.5% of the patients , chest wall pain in 6.7% , and grade 2 teleangiectasia in 3.7%. 
the authors interpreted their results as in accordance with findings after classical rt with consecutive boosts , although they admitted that the cumulative rates of observed fibrosis were in the upper range of reports . 
to date , clinical intermediateand long - term analyses seem to confirm the above mentioned biomathematical models in terms of assumed alpha / beta ( / ) values of all relevant tissues regarding both , tumor control and cosmetic results . 
nevertheless , longer follow - up remains necessary to confirm these observations by more mature data . another open issue is whether the existing clinical data for hypofractionated wbi can safely be transferred to wbi using sib strategies in general practice . 
generally , sib techniques can be performed within conventionally ( normo - ) fractionated wbi ( single breast doses 1.82 gy , total doses 50 gy ) as well as hypofractionated wbi schedules ( single doses around 2.7 gy , total dose around 40 gy )  . 
therefore , dependent on number and dosage of sib fractions , the lq model predicts somewhat higher rates of late reactions within the tumor bed volume ( see below )  . 
especially in larger breast volumes , they have been associated with significantly higher rates of subsequent development of breast fibrosis with worse cosmetic outcome [ 12 , 16 ]  . 
unlike in sib treatments , these regional overdosages were inadvertent effects caused by patients anatomy and lower depth penetration of photons ( partly cobalt - 60 ) in the absence 194 | strahlentherapieundonkologie32013 of in - field modulation options . 
therefore , caution has to be exercised when a former shortcoming in dose homogeneity , which was systematically optimized by the evolvement of sophisticated ebrt techniques , is purposely re - introduced under the assumption of a biologic superiority . the negative cosmetic impact of larger volumes exposed to higher doses has been described several times [ 7 , 16 , 21 ]  . 
however , data elucidating the role of such dose volume relations are too sparse to permit a reliable estimation of the normal breast tissues costbenefit risk during dose homogeneity modulations [ 17 ]  . 
for instance , some studies on accelerated partial breast irradiation ( apbi ) show markedly higher rates of fibrosis and unacceptable cosmetic results following zonal single doses of 3.85 gy in 10 fractions over 5 consecutive days even without wbi [ 15 ]  . 
this observation was interpreted by bentzen and yarnold [ 3 ] as a possible overestimation of cell repair capacities within the interval of a hypofractionated rt and / or as consequence of overvaluated / ratios for the estimation of cosmetically relevant late effects . 
for estimation of late fibrosis , an averaged / value of 3 gy is used : f after conventional wbi ( 25 fractions of 2 gy ) followed by a tumor bed boost of 10 gy ( 5 fractions of 2 gy ) , the 2 gy per fraction equivalent dose ( 2 gy ed ) in the boost area is 60 gy , and after a booster dose of 16 gy ( 8 fractions of 2 gy ) , the bed amounts to 66 gy , respectively . 
furthermore , these assumptions are merely comparing single and total doses , but do not account for possible time factors of shorter rt schedules . apart from dose considerations , the absolute boost volume is also predictive for the development of a late fibrosis , with increasing incidence along larger volumes , as reported in a long - term subpopulation analysis of the eortc - 22881 study : boost versus no - boost [ 7 ]  . 
prior to this publication , the investigators group had described worse cosmetic results for boost volumes > 200 cm3 ( significant in univariate analysis ; [ 21 ] )  . the choice of an appropriate ebrt technique to achieve a sib effect is of further concern . 
an uncritical application of multifield imrt techniques is highly problematic , since integral doses outside the ptv should be kept as low as possible in order to diminish stochastic tumor induction effects [ 4 , 18 ]  . 
it is assumed that after multifield or rotational sib - imrt , the subsequent risk of ipsilateral lung cancer induction rises significantly in comparison to a tangential beam design [ 8 ]  . clinical evidence of sib techniques for breast cancer a further dutch institution reported a similar experience , with a cohort comprising 1274 patients treated between 2007 and 2009 ( 28 fractions of 1.8 gy wbrt , 2.3 gy sib ; [ 14 ] )  . 
cardial function ( lvef ) was not affected by radiation technique ; lung function ( fev1 ) was reported to be less impaired after sib tomotherapy . sib during hypofractionated wbi ( hf - sib ) ongoing studies chadha et al . 
 [ 5 ] published their first experience in acute toxicity for sib application during hypofractionated rt in comparison with wbi plus boost in normofractionation : 50 patients were treated by 15 fractions of 2.7 gy whole - breast and concomitantly 3 gy tumor bed dose , respectively , whereas 74 patients received 26 fractions of 1.8 gy wbi followed by 7 fractions of 2 gy to the tumor bed . 
 concerning acute toxicity 8 weeks after the end of rt , hypofractionated sib patients experienced significantly less grade 2 fibroses ( p = 0.0015 ) and breast pain . one of the rare long - term reports following hf - sib was published by freedman et al . 
while the dose is kept lower in zones of assumed minimal residual disease , an increased single dose is pursued in those areas at higher risk for microscopic tumor remnants . 
two different hf schedules are tested against a 15 fractions of 2.7 gy regimen , followed by 8 fractions of 2 gy boost , which is now considered as standard in the uk . 
in the first test cohort , the tumor bed is concomitantly irradiated with 3.2 gy , whereas the second arm receives 3.5 gy ( isoeffective to 60 and 69 gy , respectively , towards a 2 gy fractionation at an assumed / value of 3 for late reactions )  . 
there have been no clinical reports up to now . an us - american randomized phase iii trial conducted by the rtog ( 1005 ) investigates patients receiving either sequential or concomitant boosts . 
in the sequential approach , wbi is offered in normo as well as hypofractionated rt ( 25 fractions of 2 gy and 16 fractions of 2.67 gy , respectively ) , followed by 67 fractions of 2 gy tumor bed boost . 
however , the recruitment goal of 2312 patients lies in the distant future ( 1 / 2012 : 200 patients )  . conclusion the proposed sib strategies in adjuvant radiotherapy during bct are of high investigational potential . 
however , the published data are too inconclusive and premature to permit a solid prediction of long - term outcome in terms of tumor control , fibrosis , and cosmesis . 
from the calculations presented above , the use of sib techniques with single tumor bed doses of 2.1 gy for low - risk tumors up to 2.25 gy for constellations with higher risk for local recurrence seem to be within the therapeutic range . 
in case of a distinct seroma after tumorectomy ( > 30 cm3 ) prior to rt , the necessity of re - planning has to be considered after the first two treatment weeks . 
van parijs h , miedema g , vinh - hung v et al ( 2012 ) short course radiotherapy with simultaneous integrated boost for stage iii breast cancer , early toxicities of a randomized clinical trial . 
vrieling c , collette l , fourquet a et al ( 2000 ) the influence of patient , tumor and treatment factors on the cosmetic results after breast - conserving therapy in the eortcboost versus no boost trial . 
yang z , chen j , xie j , et al . ( 2012 ) simultaneous integrated boost in breast conserving radiotherapy : is replanning necessary following tumor bed change ? technol cancer res treat oct 19 ( epub ahead of print ) 24 . 
yarnold j , ashton a , bliss j et al ( 2005 ) fractionation sensitivity and dose response of late adverse effects in the breast after radiotherapy for early breast cancer : long term results of a randomised trial . 
radiother oncol 75 : 917 editorial of radiation oncology ( degro ) explicitly discourages the routine use of higher sib fraction sizes as well as the application of sib during hypofractionated wbi schedules outside clinical trials . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 266268 doi 10.1007 / s00066 - 012 - 0292 - z online publiziert : 20 . 
basierend auf den erfahrungen der hit - 91studie wurde in deutschland ein prospektives phase - iii - protokoll mit der radioonkologischen fragestellung initiiert , ob eine hyperfraktionierte bestrahlung mit lokaler dosiseskalation im vergleich mit einer konventionell fraktionierten bestrahlung die tumorkontrolle verbessern und vor allem das risiko fr sptfolgen senken kann . 
es erfolgte eine 1 : 1 - randomisierung in eine hyperfraktionierte strahlentherapie des liquorraums bis 36 gy , gefolgt von einer aufsttigung der hinteren schdelgrube bis 60 gy und einer lokalen tumorbettaufsttigung bis 68 gy ( 21 , 0 gy pro tag ) oder in die konventionell fraktionierte strahlentherapie mit 23 , 5 gy im liquorraum , gefolgt von einer aufsttigung der hinteren schdelgrube bis 54 gy ( 11 , 8 gy pro tag )  . 
ein grerer residueller tumor nach operation verschlechtert die prognose und erfordert ein gesondertes vorgehen . kommentari die ergebnisse der hit - siop - pnet - 4studie zeigen , dass in europa ein sehr gutes ereignisfreies berleben und gesamtberleben bei kindern mit medulloblastom und standardrisiko erreicht werden kann . 
zwei jahre vor ihrer aktivierung hatte bereits die franzsische gesellschaft fr pdiatrische onkologie ( sfop ) ebenfalls ein prospektives behandlungsprotokoll ( msfop - 98 ) mit der frage initiiert , ob eine hyperfraktionierte bestrahlung , auch ohne chemotherapie , die bisher erzielten behandlungsergebnisse verbessern kann . 
 in das protokoll gingen 48 patienten e nach einer medianen nachbeobachtungszeit von 77 , 7 monaten lagen das ereignisfreie berleben bei 75% und das gesamtberleben bei 78% [ 1 ]  . 
die serie von gupta [ 3 ] besttigte die franzsischen beobachtungen : die hyperfraktionierte bestrahlung ohne chemotherapie erreichte bei 20 patienten eine rckfallfreie 3 - jahres - berlebenszeit von 83 , 5% bzw . 
darber hinaus verstrkt dieses chemotherapieregime die von der radiotherapie bekannte wachtstumsbehinderung der wirbelsule noch zustzlich [ 6 ]  . inzwischen konnten in der studie auch daten zur lebensqualitt ausgewertet und auf dem siop - kongress 2011 erstmalig vorgestellt werden [ 4 ]  . 
beiden kleineren prospektiven serien erzwingen ihre besttigung durch die untersuchung neurokognitiver funktionen der in diesem protokoll behandelten patienten auf europischer ebene . die auswertung von tumormaterial zeigte , dass die prognose der patienten wesentlich von definierten , molekulargenetischen profilen bestimmt wird [ 2 ]  . 
diese weltweit bisher einzigen erkenntnisse aus einer prospektiven , kontrollierten , klinischen studie bedeuten einen wesentlichen , klinisch relevanten durchbruch in der erforschung des medulloblastoms ; sie brachten europa weltweit in eine wissenschaftlich fhrende position . 
j clin oncol 27 : 18791883 clifford sc , rutkowski s , gustafsson g et al ( 2010 ) stratification of children and adolescents with medulloblastoma by histological and biological parameters in siop - europe pnet clinical trials . 
neuro oncol 12 : ii6 gupta t , jalali r , goswami s et al ( 2012 ) early clinical outcomes demonstrate preserved cognitive function in children with average - risk medulloblastoma when treated with hyperfractionated radiation therapy . 
int j radiat oncol biol phys 83 : 15341540 kennedy c , bull k , calaminus g et al ( 2011 ) quality of survival ( qos ) of children in the randomised multicentre pnet4 study of hyperfractionated ( hfrt ) versus standard radiotherapy ( strt ) in children with standard risk medulloblastoma . 
j clin oncol 30 : 31873193 olshan js , gubernick j , packer rj et al ( 1992 ) the effects of adjuvant chemotherapy on growth in children with medulloblastoma . 
zuvor war nmlich noch nicht untersucht worden , ob eine hyperfraktionierte strahlentherapie vorteile gegenber der herkmmlichen , konventionell fraktionierten strahlentherapie fr patienten mit einem medulloblastom bieten knnte , die ein standardrisiko haben . 
es drngt sich also der verdacht auf , dass hier der linearquadratische formalismus an seine grenzen stt . ein wesentlicher punkt der publikation ist aber auch die ototoxizitt bei der kombination von strahlentherapie und chemotherapie ( cisplatin ! )  . 
der boost fr die bestrahlung der hinteren schdelgrube kann mit zwei isozentrischen , gekeilten , schrg von dorsal einfallenden photonenfeldern so realisiert werden , dass nur eines dieser felder jeweils nur eine cochlea erfasst . 
eine analyse der tatschlich angewandten bestrahlungstechniken mit der frage einer etwaigen korrelation zur ototoxizitt wre wnschenswert . die ototoxizitt legt zudem nahe , in zuknftigen behandlungsprotokollen nach machbaren alternativen zum cisplatin zu suchen . 
nach auskunft der autoren korrelierte allerdings die hrschdigung nicht mit der anzahl der applizierten cisplatinkurse . leider kann die vorliegende arbeit noch keine auskunft ber sonstige bekannte nebenwirkungen geben , die bei der bestrahlung eines medulloblastoms auftreten knnen , wie wachstumsbeeintrchtigung , endokrine probleme und vor allem neurokognitive strungen . 
sollte sich im weiteren verlauf der beobachtung ein deutlicher unterschied zugunsten eines der untersuchten behandlungsarme zeigen , wre dies ein wichtiges kriterium fr die auswahl der geeigneten therapiemodalitt . eine wichtige frage fr die klinische forschung drfte weiterhin sein , ob eine bestrahlung unter ausschluss des hippocampus mglich ist . 
carrie c , muracciole x , gomez f et al ( 2005 ) conformal radiotherapy , reduced boost volume , hyperfractionated radiotherapy , and online quality control in standard - risk medulloblastoma without chemotherapy : results of the french msfop 98 protocol . 
n engl j med 361 : 11731178 original article strahlenther onkol 2013 189 : 230237 doi 10.1007 / s00066 - 012 - 0288 - 8 received : 24 august 2012 revised : 26 november 2012 published online : 16 . 
frequency and severity of swallowing problems can depend on different factors : ( 1 ) abuse of tobacco ; ( 2 ) abuse of alcohol ; ( 3 ) immunodepression ; ( 4 ) tumour stage ; ( 5 ) localization ; and ( 6 ) rt ( total radiation dose , fraction size , and target volumes ) that may induce oedema and fibrosis of several normal structures , such as the pharyngeal musculature [ 19 ]  . 
late dysphagia has led some authors to consider the relationship between swallowing - related structures such as pharyngeal constrictor muscles , larynx and oesophagus and factors affecting patients , tumours and treatments [ 3 , 19 , 25 ]  . the aim of this study was to analyse dosevolume histograms ( dvhs ) of the structures deputed to swallowing function and correlate these findings with frequency and severity of swallowing dysfunction in patients affected by head and neck tumours treated with rt by assessing late radiation morbidity and quality of life . materials and methods case selection and outlining of pharyngeal constrictor muscles the original treatment plan of 50 patients with head and neck tumours were retrieved from the digital archive for delineation and dosevolume histogram ( dvh ) calculation of the structures deputed to swallowing function . 
selection criteria were the followings : diagnosis of squamous cell carcinoma ( scc ) of the upper aerodigestive tract , computed tomography rt simulation with 3 mm thickness contiguous slices , treatment with rt to a total dose of at least 66 gy and availability of treatment plan with dvhs . 
patients were excluded if they had persistent / recurrent tumour , were treated with surgery and / or radiotherapy for another head and neck tumour or were treated with palliative intent . 
all patients were treated in a very homogeneous way including the identification of the clinical target volume that was defined as the gross tumour volume plus the potential microscopic spread to the surrounding tissues and to the regional lymph nodes as recommended in recent literature studies [ 9 , 16 , 17 ]  . 
characteristics of the clinical series are listed in .tab.1. based on literature data [ 5 , 19 , 29 ] , for study purposes , five muscles were considered paramount in swallowing and therefore specifically outlined : the superior constrictor muscle ( scm ) , the middle constrictor muscle ( mcm ) , the inferior constrictor muscle ( icm ) , the whole pharyngeal constrictor muscle , the cricopharyngeus muscle ( cpm ) and the oesophagus inlet muscle ( eim )  . 
in brief , the scm was delineated from the caudal tips of the pterygoid plates through the upper edge of hyoid bone , the mcm was delineated from the upper through the lower edge of the hyoid , the icm was delineated from the lower edge of the hyoid through the inferior edge of the cricoid , the whole pharyngeal constrictor muscle was formed by the sum of scm , mcm and icm , the cpm was delineated from the lower edge of cricoid through the upper edge of trachea and the eim was delineated along the first centimetre caudal from the lower border of first trachea ring . 
dvhs of the swallowing structures were obtained and mean dose ( dmean ) , maximum dose ( dmax ) and partial volume receiving a specified dose of 50 gy and 60 gy ( v50 and v60 respectively ) were considered after the revision of literature [ 8 , 10 ]  . assessment of dysphagia all patients included in the present study were called and underwent follow - up visit with the purpose to assess late toxicity and in particular dysphagia using the rtog / eortc scale [ 7 ]  . 
patient - reported clinical swallowing function was assessed also by three validated head - and - neck cancer - related quality - of - life ( qol ) questionnaires administered to the patients during follow - up visits . 
anderson dysphagia inventory ( mdadi ) , consisting of 20 questions with global , emotional , functional , and physical subscales ; and fthe performance status scale for the head and neck patients ( pss - h&n ) of list consisting of 3 subscales : normalcy of diet , public eating and understand ability of speech [ 4 , 20 , 30 ]  . in the first questionnaire , higher score means a worse quality of life , in the second and in the third higher score means a better qol . 
objective assessment of swallowing was performed by barium swallow test , using standard radiographic system , in patients with late grade 3 dysphagia . data about acute dysphagia were assessed based on the notes reported in the clinical records . 
early dysphagia , like other signs of acute toxicity , was assessed during and at the end of the treatment and was re - scored for the present study as grades 04 , according to the common terminology criteria of adverse events ( ctcae version 4.02 ) by at least two radiation oncologists with specific experience in head and neck treatment [ 2 ]  . statistical analysis analysis of variance ( anova ) and post hoc least significant different ( lsd ) test were used to analyse the association between grade of toxicity and dosevolume parameters . 
the u - mann withney or kruskalwallis one - way anova by ranks were used to analyse the association of grade of toxicity with clinical prognostic factors . the clinical and dosimetric variables that resulted significant predictors of late dysphagia at univariate analysis were inserted into a multivariable regression model in order to assess their independent contribution . the pearson correlation coefficients ( r ) was used to correlate dosimetric values and qol parameters . 
percutaneous enstrahlentherapieundonkologie32013 | original article abstract zusammenfassung doscopic gastrostomy ( peg ) tubes were placed in 4 of the 10 patients with grade 3 toxicity during rt at the time of the onset of symptoms based on the assessment of the nutritional status . 
the mean duration of feeding tube placement was 3 months ( range 15 months )  . late dysphagia , according to the rtog / eortc scale , after median followup of 20.5 months ( range 1263 months ) , was scored as grade 0 in 20 / 50 patients ( 40% ) , as grade 1 in 23 / 50 patients ( 43% ) , as grade 2 in 5 / 50 patients ( 10% ) and as grade 3 in 2 / 50 patients ( 4% )  . 
the two patients who experienced grade 3 late dysphagia underwent modified barium swallow testing that showed aspiration in one of them . dosevolume parameters ( dmean and dmax , v50 and v60 ) of the structures involved in swallowing function are reported in .tab.2. 
 as far as the dose level to whole pharyngeal constrictor muscle is concerned , a dose 60 gy was significantly associated ( p = 0.05 ) with dysphagia grade 23 . 
factors that affected late dysphagia grade 23 are summarized in .tab.4. 232 | strahlentherapieundonkologie32013 strahlenther onkol 2013 189 : 230237 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0288 - 8 l.deantoniol.masinim.brambillaf.piam.krengli dysphagia after definitive radiotherapy for head and neck cancer . 
mean dose to superior and middle constrictor muscles ( scm , mcm ) , partial volume of scm and mcm receiving a dose 50 gy dose to the whole constrictor muscles 60 gy and tumour location were associated to late dysphagia at univariate analysis . 
 this finding suggests a potential advantage in reducing the rt dose to swallowing structures to avoid severe dysphagia . keywords head and neck neoplasms dysphagia radiotherapy pharyngeal constrictor muscles late toxicity dysphagie nach strahlentherapie bei kopf - hals - tumoren . 
twenty - five of the 28 patients ( 89% ) with a pss score between 40 and 80 received a mean dose to the mcm > 50 gy . no significant correlation was found between the dose to the pharyngeal constrictor muscles and the degree of dysphagia with the items of the eortc qlqh&n35 and the mdadi questionnaires . discussion radical rt in association with concomitant chemotherapy for locoregional advanced tumours of the upper aerodigestive tract allows high rates of local control and organ preservation [ 26 , 27 ] ; however treatment - related late toxicity may worsen the patients quality of life . 
 [ 12 ] observed aspiration in 62% of patients 7 months after the completion of combined rt and chemotherapy . the onset of acute dysphagia typically occurs 23 weeks after start of rt and can increase up to treatment completion and even a few weeks thereafter . 
in our series , 54% of patients experienced grade 2 and 20% grade 3 acute dysphagia at the end of the treatment and 8% of patients who developed grade 3 acute dysphagia required the placement of peg feeding tube for a mean time of 3 months . 
 [ 25 ] , in a retrospective study on 82 patients treated by imrt , reported the need of peg tube placement in 26% of patients with a mean time to removal of 8 months . the onset of late dysphagia is thought to be related to radiation - induced free radical damage to the pharyngeal constrictor muscles as reported by truong et al . 
 the oxidative stress and the microvascular injury to the endothelium could correlate with the progressive changes in blood strahlentherapieundonkologie32013 | oropharynx hypopharynx nasopharynx larynx g0 late dysphagia oropharynx hypopharynx nasopharynx larynx g1 late dysphagia original article oropharynx hypopharynx nasopharynx larynx g2 - 3 late dysphagia fig . 
1 9 the three graphs represent the distribution of different sites of primary tumour in relation to the grade of late dysphagia ( g0 , g1 , g2 , g3 ) by the kruskalwallis oneway analysis of variance by ranks . 
tumour location in the oropharynx significantly correlated with late dysphagia grade 23 ( p = 0.03 ) flow and blood volume at perfusion ct during rt . ing ( fees ) was systematically performed in the whole patient population [ 14 , 18 ]  . after a median follow - up time of 20.5 months , 57% of our patients experienced late dysphagia of various degree according to the rtog scale ( 43% of grade 1 , 10% of grade 2 and 4% of grade 3 )  . 
this finding could be explained by the use in the fengs series of concomitant chemotherapy with weekly paclitaxel , a neurotoxic agent that could have contributed to the occurrence of dysphagia and by the fact that toxicity was assessed quite early ( 3 months ) after the end of treatment , while we analysed late dysphagia at a minimum follow - up time of 1 year . 
of note , the mean dose to the mcm was found to be a significant parameter also at the multivariate analysis . dose to the pharyngeal constrictor muscles was found to be predictive of swallowing disorders also by other authors [ 1 , 6 , 14 , 18 , 19 ]  . 
the mean doses to the pharyngeal constrictor muscles , above which the risk of dysphagia increases significantly , range between 45 and 60 gy in the quantec analysis [ 29 ]  . 
the authors used different methods to assess dysphagia resulting in different normal tissue complication probability ( ntcp ) values but they were not able to demonstrate a clear dosevolume threshold . 
 [ 8 ] found that a primary tumour site in the larynx , hypopharynx and posterior pharyngeal wall was associated with long - term dysphagia . the present study did not find a statistically significant association between late 234 | strahlentherapieundonkologie32013 tab . 
5 scores from selected items of quality - of - life questionnaires items pss : eating in publica ( 0100 ) pss : normalcy of dieta ( 0100 ) qlq - h&n35 : painb ( 0100 ) qlq - h&n35 : swallowingb ( 0100 ) qlq - h&n35 : social eatingb ( 0100 ) mdadi : global subscalea ( 20100 ) mdadi : emotional subscalea ( 20100 ) mdadi : physical subscalea ( 20100 ) mdadi : functional subscalea ( 20100 ) pss performance status scale [ 20 ] , qlq - h&n european organisation for research and treatment of cancer quality - of - life questionnaires [ 30 ] , mdadi m.d. 
other studies [ 1 , 13 ] did not focus attention on the possible concomitant effect of chemotherapy schedules because all patients received combined chemotherapy and rt . no significant correlation between scores of the quality of life questionnaires and degree of late dysphagia emerged from the present study . 
 [ 1 ] found no correlation between mean dose to pharyngeal constrictor muscles and any of the mdadi parameters but observed a significant correlation between degree of dysphagia and mdadi parameters . 
 this finding was similar to our results : a poor normalcy of diet was significantly associated with higher dose to the scm and mcm . among these studies , the different results of doseeffect relationships to anatomical structures involved in swallowing , can be caused by the differences in the delineation of pharyngeal constrictor muscles . 
 [ 5 ] proposed their institutional guidelines for the delineation of organs at risk involved in radiation - induced swallowing dysfunctions for a reliable comparison and interpretation of results from different studies . potential limitation of the present study may be the method of delineation of the structures deputed to swallowing function that , although performed by experienced radiation oncologist , is not well standardized yet as previously underlined and could represent a bias when comparing our results with those from other series reported in the literature . 
on behalf of all authors , the corresponding author states that there is no conflict of interest . original article strahlenther onkol 2013 189 : 223229 doi 10.1007 / s00066 - 012 - 0289 - 7 received : 16 august 2012 accepted : 26 november 2012 published online : 16 . 
januar 2013 springer - verlag berlin heidelberg 2013 m.lambrechtd.nevenss.nuyts department of radiation oncology , leuvens kankerinstituut , university hospitals leuven intensity - modulatedradiotherapy vs.parotid - sparing3d conformalradiotherapy effectonoutcomeandtoxicityinlocally advancedheadandneckcancer balancing tumor control against toxicity is a great challenge in the management of head and neck squamous cell carcinoma ( hnscc )  . 
the introduction of altered fractionation schedules and the addition of concurrent chemotherapy significantly improved locoregional control ( lrc ) and overall survival ( os ) at the cost of increased acute and late toxicity [ 1 , 2 , 3 ]  . 
however , this high conformality also implies an increased risk for marginal misses and requires adequate compensation for setup uncertainties , appropriate selection and accurate delineation of the tv , proper dose prescription and extensive quality control . 
the field of hnscc has always been at the forefront in the integration of these techniques , with the rapid and widespread implementation of parotid - sparing 3d conformal radiotherapy ( 3dcrt ) and intensity - modulated radiotherapy ( imrt ) [ 4 , 5 ]  . 
 with this study we wanted to retrospectively investigate the effect of introducing imrt compared to a selective 3dcrt approach in the primary treatment of locally advanced hnscc on both outcome and toxicity . material and methods patient selection this retrospective analysis was approved by the local medical ethical commission . 
pretreatment evaluation consisted of complete history and physical examination , routine blood counts , liver function tests , ultrasound scan of the abdomen , chest radiography , esophagogastroscopy and tumor biopsy . 
bone scans , positron emission tomography scans and ct scans of the abdomen or chest were obtained when clinically indicated . simulation and tv delineation all patients were immobilized using a thermoplastic 5 - point mask . 
for the node - negative neck , the upper limit of level ii was placed where the posterior belly of the digastrics muscle crosses the jugular vefor the node - positive neck , the ctv was extended to the base of the skull ( jugular foramen ) and included the retrostyloid space [ 9 ]  . 
the planning target volume ( ptv ) boost and ptv elective encompassed the ctv boost and ctv elective plus a 5 - mm margin , respectively . treatment delivery patients were treated with 6 - mv photons . 
imrt was performed using helios software for inverse imrt planning ( sliding window ) , integrated in the commercial eclipse treatment planning system ( varian medical systems , palo alto , ca )  . 
for patient set - up verification , an online bony anatomy match was performed using both mv and kv imaging on day 1 , 2 and 3 of treatment and weekly thereafter . 
in case of a systematic set - up error > 3 mm , the position was corrected , and the set - up protocol repeated . strahlentherapieundonkologie32013 | original article tab . 
oral cavity , pharyngeal constrictor muscles , esophagus were outlined when appropriate and the dose to these structures was kept as low as reasonably possible without compromising ptv coverage . acute toxicity all patients were evaluated by their treating physician at least once a week dur224 | strahlentherapieundonkologie32013 ing radiotherapy . 
patients were evaluated weekly by a nutritionist , who advised patients on their dietary intake and initiated tube feeding when necessary . late toxicity and response after treatment all patients were followed up at the multidisciplinary outpatient clinic : every 2 months for the first 2 years after treatment , every 3 months for the third year , every 4 months for the fourth year , every 6 months for the fifth year , and yearly thereafter . 
late toxicity was graded according to the radiation therapy oncology group / european organisation for research and treatment of cancer ( rtog / eortc ) late radiation morbidity scoring schedule . 
 response evaluation consisted of physical examination and ct scan 4 months after treatment , thereafter , a ct scan was done yearly or at the discretion of the treating oncologist or ear , nose and throat surgeon . statistical analysis for both treatment groups , patient and tumor characteristics were recorded at the start of treatment . 
follow - up abstract zusammenfassung strahlenther onkol 2013 189 : 223229 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0289 - 7 m.lambrechtd.nevenss.nuyts intensity - modulated radiotherapy vs . 
the introduction of imrt in the radiotherapeutic management of locally advanced head and neck cancer significantly improved late toxicity without compromising tumor control compared to a parotid - sparing 3d conformal radiotherapy technique . keywords head and neck neoplasms intensity - modulated radiotherapy treatment outcome toxicity conformal radiotherapy intensittsmodulierte strahlentherapie versus parotis schonende 3 - dkonformale strahlentherapie . 
insgesamt wurden 245 patienten mit einem plattenepithelkarzinom des kopf - hals - bereichs im stadium iii und iv , die zwischen januar 2003 und dezember 2010 mit einer primren strahlentherapie behandelt wurden , in die studie aufgenommen . 
die einfhrung der imrt als standardtherapie bei der behandlung des lokal fortgeschrittenen kopf - hals - karzinoms hat keinen negativen einfluss auf den onkologische erfolg der behandlung , gleichwohl kommt es zu einer deutlichen verminderung der akuten und spten nebenwirkungen verglichen mit der , die parotis schonenden , 3 - dkonformalen strahlentherapie ( 3dcrt )  . schlsselwrter kopf - hals - tumore intensittsmodulierte strahlentherapie behandlungserfolg toxizitt konformale strahlentherapie pared using a log - rank test . 
cumulative survival and tumor control rates were calculated using the kaplanmeier product - limit ( actuarial ) method and both groups were compatient and tumor characteristics and treatment specifications are summarized in .tab.1. 
4 8 evolution of dysphagia grade 2 after end of treatment discussion with the widespread introduction of imrt into daily practice , there was great concern that the steeper dose gradients and more conformal dose delivery would compromise tumor control [ 11 ]  . 
only one randomized controlled trial has compared toxicity between imrt and conventional rt in general hnscc ; however , the small sample size and short follow - up made it impossible to ascertain differences in clinical outcome [ 12 ]  . 
however , both populations were treated within a short time frame ( 7 years ) in which apart from the technique little or no changes were made in fractionation schedule or indication setting . 
while our outcome falls well within the range of what can be expected in patients with locally advanced hnscc , they are considerably lower than results in the above mentioned studies . 
both of which would have a positive effect on outcome , making it difficult to compare these results . one study observed a favorable outcome on lrc and os in oropharyngeal scc patients treated with imrt compared to conventional rt [ 15 ]  . 
in general with a similar tv definition , ott , concurrent treatment , total dose , and patient positioning protocol , a better outcome is not to be expected when implementing a new radiation technique . 
although indirectly , some studies suggest that the reduced toxicity associated with more conformal techniques might result in a higher number of patients , i.e. , elderly patients , eligible for the optimal curative treatment [ 18 ]  . in our series , the imrt group had significantly less acute mucositis than the 3dcrt group . 
another possible explanation might be that the preservation of salivary gland function itself has a protecting effect with regard to acute mucositis and secondary oral infections [ 19 ]  . in the evaluation of late toxicity , we focused mainly on late xerostomia and dysphagia as these are the most important toxicities after rt for hnscc . 
this is in contrast with , for example , the parsport trial , where the dose was delivered using parallel opposed lateral beams with no intention to spare the contralateral parotid [ 12 ]  . 
the use of imrt , however , enabled us to further reduce the dose to both the ipsilateral and contralateral parotid gland with a further reduction in the incidence of xerostomia . although failing to reach significance , there was a trend toward less dysphagia in the imrt group . 
 [ 15 ] also failed to notice a significant difference in late rtog toxicity , although the exact timing of the late toxicity measurements in this study was not clear . 
2 overview of randomized and nonrandomized studies comparing imrt versus more conventional rt techniques study technique subsite primary / postop ajcc stage ipsilateralparotid ( gy ) contralateral parotid ( gy ) xerostomia lrc ( % ) os ( % ) original article randomizedtrial nutting et al . 
in conclusion , these data suggest that there might be a benefit using imrt on late dysphagia ; however , the real impact of imrt on the incidence of late dysphagia requires further investigation and a clear correlation with dosimetric values . 
 an important aspect , however , is that very similar to xerostomia , dysphagia seems to evolve over time and that in our population the benefit of imrt on dysphagia was only apparent 1824 months after the end of radiotherapy . there are some important limitations to this retrospective , single - institution analysis . 
furthermore , since it is far more difficult to spare the contralateral parotid gland in case of bilateral lymph node involvement , the gain with imrt on toxicity might potentially be even greater . the median follow - up time of the imrt group was significantly shorter than the 3dcrt group ; however , since the majority of locoregional recurrences in hnscc cancer occur within the first 23 years after irradiation , we can safely say that the implementation of highly conformal intensity - modulated rt techniques did not compromise treatment outcome . 
several other evaluation techniques are available ; however , considering the fact that both xerostomia and dysphagia are mainly quality of life issues , patient - reported endpoints are more indicative of the true effect of the technique [ 23 ]  . 
levendag pc , teguh dn , voet p et al ( 2007 ) dysphagia disorders in patients with cancer of the oropharynx are significantly affected by the radiation therapy dose to the superior and middle constrictor muscle : a doseeffect relationship . 
eisbruch a , rhodus n , rosenthal d et al ( 2003 ) how should we measure and report radiotherapy - induced xerostomia ? semin radiat oncol 13 : 226234 8 . 
gregoire v , levendag p , ang kk et al ( 2003 ) ctbased delineation of lymph node levels and related ctvs in the node - negative neck : dahanca , eortc , gortec , ncic , rtog consensus guidelines . 
gregoire v , eisbruch a , hamoir m , levendag p ( 2006 ) proposal for the delineation of the nodal ctv in the node - positive and the post - operative neck . 
nutting cm , morden jp , harrington kj et al ( 2011 ) parotid - sparing intensity modulated versus conventional radiotherapy in head and neck cancer ( parsport ) : a phase 3 multicentre randomised controlled trial . 
lee ny , de arruda ff , puri dr et al ( 2006 ) a comparison of intensity - modulated radiation therapy and concomitant boost radiotherapy in the setting of concurrent chemotherapy for locally advanced oropharyngeal carcinoma . 
chen am , li bq , farwell dg et al ( 2011 ) improved dosimetric and clinical outcomes with intensitymodulated radiotherapy for head - and - neck cancer of unknown primary origint j radiat oncol biol phys 79 : 756762 15 . 
clavel s , nguyen dh , fortin b et al ( 2012 ) simultaneous integrated boost using intensity - modulated radiotherapy compared with conventional radiotherapy in patients treated with concurrent carboplatin and 5 - fluorouracil for locally advanced oropharyngeal carcinoma . 
vergeer mr , doornaert pa , rietveld dh et al ( 2009 ) intensity - modulated radiotherapy reduces radiation - induced morbidity and improves health - related quality of life : results of a nonrandomized prospective study using a standardized follow - up prograint j radiat oncol biol phys 74 : 18 17 . 
toledano i , graff p , serre a et al ( 2012 ) intensitymodulated radiotherapy in head and neck cancer : results of the prospective study gortec 2004 - 03 . 
nguyen np , vock j , chi a et al ( 2012 ) impact of intensity - modulated and image - guided radiotherapy on elderly patients undergoing chemoradiation for locally advanced head and neck cancer . 
langendijk ja , doornaert p , verdonck - de leeuw im et al ( 2008 ) impact of late treatment - related toxicity on quality of life among patients with head and neck cancer treated with radiotherapy . 
dirix p , abbeel s , vanstraelen b et al ( 2009 ) dysphagia after chemoradiotherapy for head - andneck squamous cell carcinoma : dose - effect relationships for the swallowing structures . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 202215 doi 10.1007 / s00066 - 012 - 0275 - 0 received : 18 july 2012 accepted : 8 november 2012 published online : 13 . 
papanikolaou general hospital , thessaloniki cyclind1 , egfr , and akt / mtorpathway potentialprognosticmarkersinlocalized laryngealsquamouscellcarcinoma cancer of the larynx represents the most common location of head and neck squamous cell carcinoma ( hnscc ) with more than 150 , 000 cases annually ; it has the strongest epidemiological relation with smoking and the highest male to female ratio of 6 : 1 [ 1 , 2 ]  . 
despite recent advances in management modalities [ 3 , 4 ] , the prognosis of locally advanced hnscc patients has not improved over the past three decades and the 5 - year survival remains below 50% [ 5 ]  . 
current therapeutic approaches for laryngeal cancer , including organ preservation strategies [ 6 , 7 ] , are associated with acute and late toxicity and often lead to severe functional deficits [ 8 , 9 ]  . 
accordingly , there is an unmet need to estimate prognosis more accurately in order to enhance patient selection for more or less aggressive treatments [ 10 ]  . epidermal growth factor receptor ( egfr ) expression and cancer prognosis have been investigated in many human cancers and although discrepancies have been reported , patients with tumors that show high expression of egfr tend to have a poorer prognosis in general [ 11 ]  . 
egfr activation initiates intracellu202 | strahlentherapieundonkologie32013 lar signaling through multiple pathways , including akt / mtor , thus , regulating not only cell growth , but also cell fate decisions , such as differentiation and survival or death by apoptosis [ 12 , 13 ]  . 
gene amplification and / or protein overexpression of cyclin d1 ( ccnd1 ) , a key regulator of the cell cycle , has frequently been reported in hnscc , not only as a negative prognostic marker , but also as a probable predictor of resistance to chemotherapy [ 14 ]  . in the present study , we retrospectively examined mrna expression of egfr , mtor , ccnd1 , akt1 , akt2 and akt3 and copy number variants ( cnvs ) of egfr and ccnd1 in tumor cells of a cohort of patients with localized laryngeal cancer . 
furthermore , we studied the tumoral immunohistochemical ( ihc ) protein expression of egfr , cyclin d1 , p - mtor , pten , p53 , p - akt308 and p - akt473 and analyzed biomarker correlations with each other , with clinicopathological parameters and their prognostic utility . patients and methods we retrospectively identified patients with localized ( stage iiii ) squamous cell carcinoma of the larynx , managed between may 1985 and june 2008 at the ent department of the aristotle university of thessaloniki with potentially curative surgery and / or radical external beam irradiation . 
patients characteristics are shown in .tab.1. biomarker assessment in total , 289 formalin - fixed paraffin - embedded tumor tissue samples were retrieved from the hellenic co - operative oncology group tissue bank . 
hematoxylin and eosin ( h&e ) sections from the corresponding paraffin blocks were evaluated by an experienced pathologist for tumor cell content and for tissue microarray ( tma ) construction . 
for each gene , two genomic targets were amplified , to ensure informative results . total rna was extracted with the trizol - ls protocol and reverse transcribed with random primers and the superscript iii system ( life technologies ) , whereby 3 g rna was used as the template . 
serial 2 m sections from the tma blocks were cut at the laboratory of molecular oncology of the hellenic foundation for cancer research , aristotle university of thessaloniki school of medicine , mounted on adhesive microscope slides and subjected to ihc labelling using bond max , bond iii ( leica microsystems , germany ) and i6000 ( biogenex , san ramon , ca , usa ) autostainers . 
the quality of ihc staining was evaluated using the internal tma controls . all ihc sections were evaluated by an experienced pathologist ( pk ) , who was blinded to the patients clinical characteristics and survival data . 
the percentage of positive ( p ) tumor cells was graded semiquantitatively and each tumor sample was assigned to one of the following categories : 010% = 0 , 1125% = 1 , 26 50% = 2 , 5175% = 3 , and 76100% = 4 . 
the immunoreactive score ( irs ) was calculated by adding the two scores ( p + i ) to yield the total score ( 07 )  . the number of samples eligible for analysis of each dna , rna and protein marker is shown in .fig.1. statistical analysis the aim of the analysis was to study the prognostic role of the following biomarkers : egfr , mtor , cyclin d1 , akt1 , akt2 , akt3 , pten , and p53 . first , for all continuous biomarker values the quartiles ( 25th , 50th , and 75th percentile ) were examined by means of univariate cox regression analysis , as possible thresholds for prognostic significance in terms of overall survival ( os ) or disease - free survival ( dfs )  . 
in 289 patients with t34 ( 77.8% ) , node - negative ( 84.1% ) tumors of the larynx , high egfr and ccnd1 mrna correlated with no or ex - smoking , ( p = 0.003 and p = 0.029 , respectively ) , while low akt3 mrna correlated with alcohol abuse , n0 stage , total laryngectomy , and absence of neck dissection . 
at a median follow - up of 74.5 months , high mtor mrna expression was marginally associated with shorter disease - free survival ( hazard ratio [ hr ] = 1.54 ; p = 0.093 ) and high akt3 mrna with shorter overall survival ( hr = 1.49 ; p = 0.0786 ) , in univariate analysis . 
in localized laryngeal cancer , clinicopathological parameters and an interaction of high mtor and ccnd1 mrna expression were found to be associated with poor patient outcome . keywords epidermal growth factor receptor akt mtor prognostic factors laryngeal neoplasms cyclin - d1 - , egfrund akt / mtor - signalweg . 
bei einem mittleren follow - up von 74 , 5 monaten war eine hohe mtor - mrnaexpression in der univariaten analyse marginal mit krzerem krankheitsfreiem berleben vergesellschaftet ( hazard - ratio , hr : 1 , 54 ; p = 0 , 093 ) und eine hhere akt3 - mrna mit krzerem gesamtberleben ( hr : 1 , 49 ; p = 0 , 0786 )  . 
bei lokal begrenztem larynxkarzinom stellte sich heraus , dass klinisch - pathologische parameter und eine interaktion von hoher mtorund ccnd1 - mrna - expression mit einem schlechteren verlauf fr den patienten einhergingen . schlsselwrter egfr akt mtor prognostische faktoren larynxkarzinom accordingly high versus low mrna expression of egfr , ccnd1 , mtor , akt1 , akt2 and akt3 , using three possible cut - offs ( 25th , 50th and 75th percentile ) for every biomarker as a categorical variable , were examined for correlations with each other , with the mrna expression of the same biomarkers as a continuous variable , with cnv status of egfr and ccnd1 genes , with immunoreactive scores of egfr , mtor , cyclin d1 , pten , p53 , akt308 and akt473 and with clinicopathological characteristics . 
 a multivariate cox proportional hazards model contained every variable and interaction that was significant and a backward selection procedure with a 15% removal cut - off was used . dfs was measured from the time of diagnosis until verified disease progression , death or date of last contact and os from diagnosis until death from any cause or date of last contact . 
associations between biomarkers and with basic patient and tumor characteristics were examined using the fishers exact test for categorical variables and the mannwhitney or the kruskallwallis tests where appropriate for continuous variables . 
for the continuous mrna expression values , the correlations were done using the pear204 | strahlentherapieundonkologie32013 289 patients with stage i - iii resected laryngeal cancer treated in hecog affiliated centers 1985 - 2008 formalin - fixed paraffin - embedded ( ffpe ) tissue samples were obtained from 289 patients and tmas constructed for ihc sufficient tumor tissue available for rna extraction in 285 patients successful rna extraction of sufficient quality and quantity in 247 patients . cases analyzed : mrna p - akt308 p - akt473 pten p - mtor egfr cyclin d1 egfr mtor akt1 akt2 akt3 ccnd1 egfr ccnd1 fig . 
survival data are presented in more detail in .tab.2. correlations between dna / rna biomarkers and clinicopathological parameters egfr gene amplification was observed in 44.6% , whereas ccnd1 gene amplification was observed in 21% of informative tumor samples . 
there was generally good correlation between egfr and ccnd1 gene amplification and mrna overexpression ( data available upon request )  . mrna descriptives are shown in appendix 3 and in .fig.2b. 
we observed that the mrna expression ( in continuous form ) of cyclin d1 , egfr , and the akt / mtor pathway genes were significantly correlated to each other . 
 all statistically significant correlations among examined biomarkers are summarized in .tab.3. egfr , ccnd1 , mtor , akt1 , akt2 and akt3 mrna expression ( rq values ) was classified as high or low by using three possible cut - offs ( 25th , 50th and 75th percentile ) and was compared with clinicopathological characteristics . 
protein expression for cyclin d1 , egfr , akt strahlentherapieundonkologie32013 | applied biosystems copycaller software v2.0 file : 20101215_lo_rnasep _pl4_an_01_cr.txt , target : ccnd1 ( intron 2 ) , calibrator : cntrl ( l112n ) file : 20101215_lo_rnasep _pl4_an_01_cr.txt , target : ccnd1 ( exon 3 ) , calibrator : cntrl ( l112n ) applied biosystems copycaller software v2.0 file : 20101215_lo_rnasep _pl4_an_01_cr.txt , target : egf rexon 2 , calibrator : cntrl ( l112n ) file : 20101215_lo_rnasep _pl4_an_01_cr.txt , target : egfr_exon10 , calibrator : cntrl ( l112n ) original article akt1 akt2 akt3 ccnd1 egfr erbb2 erbb3 mtor fig . 
results of multivariate analysis for dfs and os are summarized in .tab.7. discussion transition from normal epithelium to squamous cell carcinoma is a complex , multistep genetic process , involving a variable degree of genetic instability and deregulation of multiple intracellular signaling pathways [ 17 , 18 ]  . 
 egfr downstream signaling is mediated , at least in part , through activation of the pi3k / akt / mtor pathway and recent data from our laboratory , involving gene expression signatures in laryngeal cancer , suggest a prognostic role for mtor signaling pathway genes [ 23 ]  . accumulating evidence also indicates that high expression of cyclin d1 , either correlated with or independent from egfr pathway proliferation signals , is associated with prognosis and treatment outcome in head and neck cancer [ 24 ]  . gene expression profiling of messenger rna by means of qrt - pcr provides a quantitative evaluation method that is not affected by observer variability or the widely known ihc technique limitations [ 25 ]  . in our study , we found only marginal adverse prognostic association of high mrna expression of mtor for dfs and akt3 for os in univariate analysis . 
patients with a high expression of both biomarkers simultaneously had a more than two - fold risk for shorter dfs compared to patients with high expression of only one of the biomarkers . there is increasing evidence suggesting molecular interplay between mtor and cyclin d1 in cancer cells . 
mtor inhibitors have direct antiproliferative effects and can cause cell cycle arrest in the g1 phase in certain sensitive cancers , such as endometrial cancers , which frequently exhibit pten loss , but also in tumors in which proliferation is driven primarily by cyclin d1 overexpression , such as mantle cell lymphoma [ 26 , 27 ]  . 
downregulation of cyclin d1 by mtor inhibitors is thought to be mediated by eukaryotic initiation factor 4e - binding protein 1 ( 4e - bp1 ) , an mtorc1 target that regulates translation initiation [ 29 ]  . although egfr mrna expression correlated fairly in our study with egfr protein expression , akt1 and mtor mrna expression and egfr cnvs , we found no statistically significant independent prognostic value of egfr expression in our cohort of patients . it has been postulated that overexpression of egfr may not necessarily reflect the functional state of this pathway . 
 [ 30 ] showed that only the activation of the egfr pathway , as measured using a fret - based assay , showed a correlation with dfs and more importantly that egfr protein expression , found in > 90% of samples , showed no correlation with such activation . 
second , increased egfr downstream signaling may be a result of receptor mutation or the interplay of egfr with the other members of the egfr family , such as her2 , her3 or her4 . 
 [ 33 ] showed that the combination of egfr , her2 and her3 but not her4 was more significant than any individual member in predicting the outcome in patients with oral squamous cell cancer . immunohistochemical evaluation of the activated state of the akt / mtor pathway effectors in our study , failed to reveal any independent prognostic significance . 
phosphoproteins reflect a minuteby - minute record of ongoing signaling , with the phosphorylated state of a protein being a function of the local stoichiometry of associated kinases and phosphatases specific for the phosphorylated residue . 
 excised tissue remains alive and reactive ex vivo with a transient increase in phosphorylation sites due to wound stress , but ubiquitous phosphatases are expected to destroy phosphorylation sites when given enough time . 
thus , phosphoproteins are labile biomarkers and their examination is confounded by the lack of standardized tissue procurement and fixation procedures [ 34 , 35 ]  . other reasons for the failure of biomarkers to reach prognostic significance might be related to the moderate sample size or the actual lack of prognostic utility . 
another reason inherent to our patient cohort might be the fact that the large majority of our patient population ( 84% ) had node - negative , amenable to local treatment laryngeal cancer , with a high cure rate , and thereby stronger clinicopathological prognostic factors may have outweighed weaker metabolic ones . strahlentherapieundonkologie32013 | original article tab . 
glotticsupraglottic ccnd1rq4median - centered one unit rise mtor ( cut - off75thpercentile ) * ccnd1rq4 ( median - centered ) mtor high * ccnd1rq4 ( median - centered ) overallsurvival nodalstage n + vs . 
in einem in der ddr erschienenen studentenlehrbuch , fr dessen strahlentherapieteil strietzel verantwortlich war , wurde durch die dresdner erfahrungen begrndet auf die darstellung interdisziplinrer krebsbehandlung groer wert gelegt und dies auch durch entsprechende autorenschaft belegt . 
diesen interdisziplinren ansatz bertrug er auch auf seine arbeit in rostock und konnte ihn als leiter des tumorzentrums rostock von 1992 bis 1998 weiterentwickeln . professor strietzel bernahm 1984 die chefredaktion der zeitschrift radiobiologia radiotherapia , die er bis zu deren aufgabe im jahre 1990 leitete . 
nachdem er unter den schwierigen bedingungen der damaligen zeit in rostock eine moderne klinik aufgebaut hatte , beschftigte er sich in seinen letzten berufsjahren intensiv mit brachytherapie , insbesondere mit den neuen mglichkeiten der afterloading - therapie . 
diese besondere korrektheit , aber auch seine mitfhlende zuwendung zum tumorpatienten sowie seine konsequente menschliche und undoktrinre haltung auch gegenber kollegen und mitarbeitern sind fr viele seiner schler vorbild fr ihr eigenes wirken in der radioonkologie geworden . anfang mai 2013 wird manfred strietzel sein 85 . 
seine schler danken ihm fr seinen immerwhrenden ausgewogenen rat , den sie auch einfordern konnten , nachdem sie selbst schon in verantwortlichen positionen waren , und wnschen ihm gesundheit , verbunden mit der zusage , dass er in dresden weiterhin stets ein gern gesehener gast ist und dies nicht nur , wenn er als ehrenmitglied der schsischen radiologischen gesellschaft deren jahrestagungen besucht . thomas herrmann und johannes schorcht , dresden korrespondenzadresse th . 
nach seinem zweiten facharztabschluss wechselte er dauerhaft in die strahlentherapie und baute eine der grten ostdeutschen radioonkologischen abteilungen in dresden auf , die er als abteilungsleiter der radiologischen klinik bis 1978 leitete . 
dort konnte er original article original article strahlenther onkol 2013 189 : 246255 doi 10.1007 / s00066 - 012 - 0273 - 2 received : 18 july 2012 accepted : 8 november 2012 published online : 31 . 
tumor hypoxia is recognized as a major problem in radiation therapy since it limits the efficacy of irradiation due to the radiosensitizing effect of oxygen [ 4 , 5 ]  . 
in radiotherapy , several strategies have been pursued to overcome the radioresistance of hypoxic tumors , either by targeting hif - 1 [ 6 , 7 ] or enhancing oxygenation of the tumors during irradiation . 
among the latter are the breathing of hyperbaric oxygen , the pharmacological increase of tumor blood flow with nicotinamide combined with carbogen breathing , and the allosteric modification of hemoglobthe hemoglobin modification is proposed to facilitate the oxygen discharge from hemoglobin in the tissue . 
another approach utilizes oxygen mimetics that are trapped specifically within hypoxic tumor areas where theysimilarly to oxygenpromote fixation of the dna damage ( for review see [ 8 , 9 ] )  . 
a recent meta - study revealed significantly improved locoregional control , disease - specific and overall survival in patients with squamous cell carcinomas of the head and neck receiving hypoxic modifications during radiotherapy [ 10 ]  . several classes of compounds have been considered for the development as oxygen mimetics and hypoxia - selective cytotoxins , such as nitroimidazole - containing compounds [ 2 , 11 , 12 ]  . 
nitroimidazoles have been demonstrated to radiosensitize hypoxic tumor cells in vitro by an enhancement ratio ( er ) of 1.32.6 [ 13 , 14 , 15 , 16 , 17 , 18 ]  . 
studies performed in parallel on cultured cells and tumors xenografted in mice demonstrated similar enhancement factors in vitro and in vivo for 2 - nitroimidazoles [ 14 , 15 , 17 , 18 ] such as misonidazole ( erculture = 1.5 and erxenograft = 1.5 ; [ 14 ] ) or doranidazole ( erculture = 1.41.55 and erxenograft = 1.351.45 ; [ 17 ] )  . 
however , the in vitro and in vivo radiosensitizing effects of misonidazole and etanidazole did not translate into an improved outcome in clinical trials in head and neck , cervix , and lung carcinoma patients [ 20 , 21 , 22 , 23 , 25 , 26 ]  . 
in these trials , markers of clinically relevant hypoxia [ 28 ] and gene expression , as well as hpv status [ 29 ] have allowed to identify patients that benefit from combined nimorazole and radiotherapy . 
a , b jurkat cells were incubated in 21% ( normoxia ) or 0.1% o2 ( hypoxia ) for 48 h and post - incubated for 24 h ( reoxygenation ) both , in the absence ( vehicle ) and presence of increasing concentrations of a f - miso or b prc . 
thereafter , cells were incubated for 48 h either under standard normoxic conditions ( controls ) or under severe hypoxia ( 0.1% o2 ) as applied by the bd gaspak ez pouch system ( becton and dickinson )  . 
thereafter , cells were further incubated for 0.524 h under normoxia ( reoxygenation ) and then prepared for flow cytometry or determination of clonogenic survival . to measure cell death and cell cycle progression , cells were permeabilized and stained ( 30 min at room temperature ) with the dna - specific fluorescence dye propidium iodide ( pi , sigmaaldrich ) in phosphate - buffered saline , containing 0.1% sodium citrate , 0.1% triton x - 100 , and 10 g / ml pi . 
the fraction of dead cells was indicated by the subg1 population of the logarithmic pi fluorescence histogram ( see .fig.2 ) as recorded in fluorescence channel 2 ( fl - 2 , 488 nm excitation and 564606 nm emission wavelength )  . 
the distribution of the cells in g1 , s , or g2 phase of cell cycle was analyzed in the linear pi fluorescence histogram ( see .fig.4 ) as recorded in fl - 3 ( 488 nm excitation and > 670 nm emission wavelength )  . to determine the inner mitochondrial membrane potential ( m ) , t98g glioblastoma cells were trypsinated , washed and incubated at room temperature for 30 min in a nacl solution ( in mm : 125 nacl , 5 d - glucose , 5 kcl , 1 mgcl2 , 1 cacl2 , 32 n - 2 - hydroxyethylpiperazine - n - 2ethanesulfonic acid ( hepes ) titrated with naoh to ph 7.4 ) containing the m specific dye tetramethylrhodamine ethyl ester perchlorate ( tmre , 25 nm , invitrogen )  . 
m was analyzed by flow cytometry in fl - 2 . to test for production of reactive oxygen species ( ros ) , detached t98g cells strahlentherapieundonkologie32013 | original article abstract zusammenfassung were incubated at room temperature for 30 min in nacl solution ( see above ) containing 10 m of the redox - sensitive dye 5 - ( and - 6 ) - chloromethyl - 27 - dichlorodihydrofluorescein diacetate acetyl ester ( cm - h2dcfda , invitrogen ) , and recorded in fl - 1 ( 515545 nm emission wavelength )  . to analyze the apoptosis / necrosis - induced breakdown of the phospholipid asymmetry and necrotic cell death , detached t98g cells were incubated at room temperature for 30 min in nacl solution ( see above ) containing annexin vfluos ( 1 : 100 dilution , roche applied science ) and pi ( 10 g / ml )  . 
 efficacy of the novel 2 - nitroimidazole n , n , n - tris [ 2 ( 2 - nitro - 1h - imidazol - 1 - yl ) ethyl ] amine abstract backgroundandpurpose . 
our in vitro findings suggest that prc might be a promising new 2 - nitroimidazole for improving radiation therapy of hypoxic tumors in vivo . keywords human jurkat lymphoma cells human t98g glioblastoma cells reactive oxygen species flow cytometry clonogenic survival hypoxische zytotoxizitt und strahlensensibilisierung in vitro . 
 effektivitt des neuen 2 - nitroimidazols n , n , n - tris [ 2 - ( 2 - nitro - 1h - imidazol - 1 - yl ) ethyl ] amin zusammenfassung hintergrundundziel . 
diese daten weisen prc als vielversprechendes neues 2 - nitroimidazol aus , das fr die radiotherapie hypoxischer tumore in vivo geeignet erscheint . schlsselwrter humane jurkat - lymphomzellen humane t98g - glioblastomzellen reaktive sauerstoffspezies durchflusszytometrie klonogenes berleben by the averaged plating efficiencies of the respective control situation ( 0 gy )  . statistical analysis a difference of normalized data from 1.0 and differences between two data sets were estimated by one - sample , twotailed t - test , by unpaired two - tailed t - test ( if the standard deviations , sds , of the two groups did not differ ) or welch - corrected t - test ( if the sds were significantly different )  . 
multiple data sets were compared by anova with tukeykramer multiple comparisons post test ( data without differing sds ) or by kruskalwallis non248 | strahlentherapieundonkologie32013 results vehicle vehicle vehicle prc vehicle normoxia hypoxia / reoxygenation normoxia hypoxia / reoxygenation normoxia hypoxia / reoxygenation fig . 
t98g cells were incubated in 21% ( normoxia ) or 0.1% o2 ( hypoxia ) for 48 h and post - incubated for 24 h ( reoxygenation ) both , in the absence ( vehicle ) and presence of prc ( 100 m )  . 
histograms were recorded by flow cytometry under normoxic conditions ( black line ) or after hypoxic stress ( 48 h hypoxia / 24 h reoxygenation , red line )  . 
cells were recorded as in a either under normoxic conditions ( 1st and 2nd bar ) or after hypoxic stress ( 48 h hypoxia / 24 h reoxygenation , 3rd and 4th bar )  . 
 * * * indicates p0.001 , anova parametric anova and dunns multiple comparisons post test ( data with differing sds ) using instat ( graphpad software , inc . , san diego , ca , usa )  . 
notably , prc exerted significant hypoxic cytotoxic effects already at 10 m ( .fig.2d , closed bars ) , while f - miso did so only at 100 m ( .fig.2d , open bars )  . 
 to determine the effect of prc on the clonogenic survival , pcr ( 0 and 100 m ) treated normoxic and hypoxic / reoxygenated t98g cells were sequentially diluted and replated in prc - free culture mediu hypoxia / reoxygenation alone decreased clonogenic survival of t98g cells by about 50% . 
given are vehicle ( a , top and b , left ) and prc ( 100 m ) - treated cells ( a , bottom and b , right ) recorded by flow cytometry under normoxic conditions ( a , left and black lines in b ) and after hypoxic stress ( 48 h hypoxia / 24 h reoxygenation ; a , right and b , red lines )  . 
c , left mean percentage of vehicle ( open bars ) and prc - treated ( closed bars ) cells with dissipated c , right mean tmre fluorescence intensity of the cell population with high m ( se , n = 2123 )  . 
data were recorded as in a , b under normoxic conditions ( left ) and after hypoxic stress ( 48 h hypoxia / 24 h reoxygenation , right )  . 
application of prc , in contrast , significantly decreased the number of hypoxic / reoxygenated t98g cells residing in the g1 phase of the cell cycle and increased the number of cells in s and g2 indicative of a prc - induced g2 / m arrest . 
6 8 prc increases hypoxia / reoxygenation - induced formation of reactive oxygen species ( ros ) a , b histograms showing the 5 - ( and - 6 ) - chloromethyl - 27 - dichlorodihydrofluorescein diacetate acetyl ester ( cm - h2dcfda ) fluorescence as a measure of ros production . 
a vehicle ( black line ) and prc ( 100 m ) - treated ( red line ) t98g cells were recorded by flow cytometry under normoxic conditions and after hypoxic stress ( 48 h hypoxia / 6 h reoxygenation ) , b . 
data were recorded as in a , b in vehicle ( open bars ) and prc - treated ( closed bars ) t98g cells under normoxic conditions ( 1st and 2nd bar ) or after hypoxic stress ( 48 h hypoxia / 6 h reoxygenation , 3rd and 4th bar )  . 
 * * * indicates p0.001 , anova brane was determined in prc ( 0 and 100 m ) - treated normoxic or hypoxic / reoxygenated t98g cells by flow cytometry and annexin - v binding . 
this can be explained by the fact that hypoxia / reoxygenation - associated decline in clonogenic survival ( compare 1st and 3rd bar in .fig.8a ) exceeded the protective effect of hypoxia on ionizing radiation ( ir , 5 gy ) by far ( data not shown )  . 
combined , these experiments indicate a hypoxic cytotoxic and a hypoxic radiosensitizing effect of prc on hypoxia - resistant and - sensitive tumor cells at absent or low toxicity under normoxic conditions . discussion there are several lines of evidence arguing for the development of anticancer therapeutics specifically targeting hypoxic tumor areas . 
second , tumor hypoxia results in radioresistance [ 1 , 31 , 32 , 33 ]  . ionizing radiation may generate dna radicals in the deoxyribose moiety of the dna backbone directly or indirectly [ 34 , 35 ]  . 
in the presence of oxygen , however , oxygen fixes 3 or 5 carbon radicals of the deoxyribose moiety towards strand break precursors [ 37 , 38 , 39 , 40 , 41 , 42 ]  . 
this so - called oxygen effect , radiosensitizes tumor cells by a factor of twoto threefold ( oxygen enhancement factor ) as compared to the hypoxic situation [ 5 , 13 , 43 , 44 ]  . therefore , the development of drugs with selective toxicity towards hypoxic cells which mimic the radiosensitizing effect of oxygen is extremely important for effective anticancer chemotherapy . 
 hypofractionation might lower the tumor re - oxygenation resulting from normal fractionation regimes and might increase the efficacy of adjuvant chemotherapy regimens using hypoxic radiosensitizers . strahlentherapieundonkologie32013 | strategy to increase the hypoxic accumulation and the thiol - depleting efficacy of the molecule . 
although , direct comparisons between these nitroimidazoles and prc are missing , the reported data might suggest that prc exerts a similar hypoxic radiosensitizing effect at 510 times lower concentration . 
a dot plots showing propidium iodide ( pi ) fluorescence as a measure of necrosis and annexin v binding as an indicator of phosphatidylserine exposure at the outer plasma membrane face . 
depicted are vehicle ( upper blots ) and prc ( 100 m ) - treated ( lower blots ) cells recorded by flow cytometry under normoxic conditions ( left ) and after hypoxic stress ( 48 h hypoxia / 24 h reoxygenation ; right )  . 
the numbers in the lower left , lower right and upper right quadrant give the percentage of annexin vand pi - negative cells , of annexin v - positive and pi - negative apoptotic cells , and of annexin vand pi - positive ( secondary ) necrotic cells , respectively . 
b mean percentage ( se , n = 12 ) of annexin v ( left ) and pi ( right ) positive vehicle ( open bars ) and prc - treated ( closed bars ) cells recorded as in a under normoxic conditions ( 1st and 2nd bar ) or after hypoxic stress ( 3rd and 4th bar )  . 
at low oxygen partial pressure , however , nitroimidazoles are further reduced to highly reactive 2 - ( hydroxyamino ) imidazoles that bind to nucleophilic macromolecules leading to cytotoxic accumulation of nitroimidazoles in hypoxic areas [ 45 , 46 , 47 , 48 , 49 ]  . 
b mean surviving fraction ( se , n = 24130 ) of vehicle ( black symbols ) and prc ( 100 m ) - treated ( red symbols ) t98g glioblastoma cells irradiated with the indicated single dose of x - ray under normoxic ( open circles ) and hypoxic ( closed triangles ) conditions . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . case study strahlenther onkol 2013 189 : 256260 doi 10.1007 / s00066 - 012 - 0282 - 1 received : 3 august 2012 revised : 15 november 2012 published online : 19 . 
in addition to such neoadjuvant strategy , intra - operative radiotherapy ( iort ) can be applied to the pelvic area being at risk for microscopic residual disease after tumor resection . 
in current clinical practice , iort has been integrated into the multimodality treatment of patients with larc to optimize locoregional disease control [ 3 , 4 ]  . another stage of rectal cancer that used to be regarded as virtually incurable is peritoneal carcinomatosis ( pc )  . 
this strategy com256 | strahlentherapieundonkologie32013 bines cytoreductive surgery ( cs ) with hyperthermic intraperitoneal chemotherapy ( hipec ) offering an option for long - term survival in selected patients [ 6 , 7 ]  . thus , radical surgery combined with iort or hipec currently provides a new perspective for rectal cancer patients who were previously regarded as untreatable . 
 however , both treatments are associated with considerable morbidity and mortality [ 8 , 9 , 10 , 11 , 12 , 13 ] and are , therefore , reserved for selected patients . 
this report describes five consecutive cases of patients treated with both iort and hipec after cytoreductive surgery for locally advanced rectal carcinoma with synchronous peritoneal carcinomatosis . patients patients and tumor characteristics are listed in .tab.1 , while the patients operative details and postoperative course are summarized in .tab.2. patient 1 was diagnosed with locally advanced rectal cancer invading the presacral fascia . 
because of a threatening obstruction , a deviating stoma was constructed ; however during this procedure , peritoneal spread to the adnex and peritoneum was discovered and the patient was referred to our hospital . 
after 5 fractions of 5 gy radiotherapy , a low anterior resection including a partial resection of the left ureter , an ileocaecal resection , and an uterus extirpation including both ovaries was performed to remove the primary tumor . 
iort was applied to the presacral area , followed by hipec perfusion with 35 mg / m2 mitomycin c . the procedure was complicated by a presacral abscess , which required drainage and treatment with intravenous antibiotics . 
 three years and 2 months after surgery , the patient is still alive without evidence of local recurrence or distant metastases . patient 2 after long course neoadjuvant radiochemotherapy for a locally advanced rectal carcinoma invading the presacral plane , peritoneal metastases were discovered unexpectedly during laparotomy in a 56 - year - old man . 
the abdomen was closed immediately and 6 days later resection of the primary tumor including rectosigmoid resection with total mesorectal excision was performed , directly followed by iort on the presacral plane . subsequently , peritoneal tumor deposits were removed from the appendix , left paracolic area and the right and ventral abdominal wall . 
unfortunately , the patient developed recurrent peritoneal carcinomatosis 10 months after the combined procedure and died 1 month later . patient 3 underwent a laparotomy for obstructive ileus , during which an irresectable locally advanced rectum carcinoma with perforation to the peritoneal cavity was found , with evidence of peritoneal spread . 
the patient received adjuvant chemotherapy and 25 months after surgery the patient has no evidence of recurrent disease . patient 5 a low anterior resection was performed after radiochemotherapy in a 73 - year - old man initially presenting with a larc and signs of peritoneal carcinomatosis on preoperative radiological staging . 
this patient is currently under follow - up and without evidence of disease 12 months after surgery . discussion radical resection is the most important factor influencing the outcomes of patients with rectal carcinoma . 
the introduction of the total mesorectal excision ( tme ) , in which the primary tumor is resected together with the mesorectal fascia and preoperative radiotherapy have both shown to significantly reduce the risk of recurrence [ 14 , 15 ]  . 
currently , extensive neoadjuvant treatment is commonly offered to these patients in order to achieve downstaging of the tumor , thereby facilitating surgical resection [ 1 , 2 ]  . 
iort is delivered as an electron boost to the area at risk for residstrahlentherapieundonkologie32013 | abstract zusammenfassung strahlenther onkol 2013 189 : 256260 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0282 - 1 y.l.b.klaverv.e.p.p.lemmenss.w.nienhuijsg.a.p.nieuwenhuijzenh.j.t.rutteni.h.j.t.dehingh intraoperative radiotherapy and cytoreductive surgery with hyperthermic intraperitoneal chemotherapy . 
this report includes five consecutive cases of rectal cancer patients presenting with larc and synchronous pc who were treated with a multimodality treatment including iort and hipec after cytoreductive surgery . 
this strategy may , therefore , be considered in selected rectal cancer patients presenting with both larc and synchronous pc . keywords neoadjuvant therapy colorectal surgery rectal neoplasms postoperative complications survival intraoperativer radiotherapie und zytoreduktiver chirurgie mit hyperthermer intraperitonealer chemotherapy . 
dieser bericht beinhaltet 5 patienten mit rektumkarzinom , die ein larc und eine pc zeigten und mit einer multimodalen therapie behandelt wurden , die die iort als auch der hipec nach zytoreduktiver chirurgie beinhaltete . 
the radiation dose varies between 10 and 12.5 gy , depending on patient characteristics , radicality of the resection and the proposed depth of irradiation , which ranges from 1422 m the applied energy ranges from 812 mev and the most commonly used applicator diameter is 6 cm . with multimodality treatment including iort for locally advanced rectal cancer , an overall survival of 67.1% after 5 years has been reported in a pooled analysis of four major treatment centers [ 4 ]  . 
in patients with locally recurrent rectal cancer , 5 - year survival rates of around 30% have been reported with multimodality treatment including iort [ 16 , 17 ]  . 
nowadays , iort is increasingly applied , also for other tumors like sarcoma and breast cancer [ 19 , 20 , 21 , 22 ]  . 258 | strahlentherapieundonkologie32013 presently , hipec procedures are offered in various expert centers worldwide for the treatment of pc . 
rationale for this technique is the assumption that peritoneal carcinomatosis is a locoregional spread of disease rather than systemic metastases , thus , being suitable for locally applied treatment strategies . 
in our hospital , hipec is performed at a temperature of 41 c during 90 min using the colosseum ( open ) technique and the performer ht ( rand , italy )  . 
 penetration depth of this treatment is regarded 23 mthis treatment has been shown to significantly prolong survival in patients with peritoneal carcinomatosis from colorectal cancer as compared to palliative treatment [ 6 , 7 ]  . 
furthermore , evidence suggests that hipec can be worthwhile in patients with therapy resistant ovarian cancer with spread to the peritoneum [ 27 , 28 ]  . thus , both iort and hipec offer a chance for cure or long - term survival in selected patient previously regarded as incurable and suitable for palliative treatment only . 
given the fact that no real alternative is present for these patients and that if left untreated life expectancy is short with a low quality of life , we recently started to offer this combined treatment . this series of patients shows that the combination of cytoreductive surgery with hipec and iort is feasible as it was well tolerated by all patients . 
this was probably caused by the high dose of radiation distributed on the presacral plane , impairing local wound healing which may even have been worsened by the application of intraperitoneal chemotherapy . 
the observation that our first patient is free of disease 38 months after presenting with a large primary tumor and extensive peritoneal disease may induce some optimism ; however , another patient died already after 11 months of recurrent pc . to our knowledge , these cases combining iort and hipec are the first reported in the international literature . 
with the increasing life expectancy worldwide , the aging population , and the associated increasing incidence of rectal carcinoma , it is not unlikely that the demand for adjuvant therapies for advanced colorectal cancer will grow within the next few years . 
 since we have shown that combining hipec and iort is feasible and safe , this combination of treatment may be considered in patients with larc and synchronous pc aiming for optimal locoregional disease control and prolonged survival . 
on behalf of all authors , the corresponding author states that there is no conflict of interest . abstracts strahlenther onkol 2013 189 : 10651092 doi 10.1007 / s00066 - 013 - 0458 - 3 springer - verlag berlin heidelberg 2013 17th annual meeting of the scientific association of swiss radiation oncology ( sasro ) 4 6 july 2013 davos , congress center organizing committees local organizing committee ( department of radiation oncology at kantonsspital graubnden ) congress president daniel r . 
zwahlen rob lodder ( chair ) therese boner ( co - chair ) doreth derrer , esther infanger , christoph oehler , bernd polivka , karl rittmann , susanne rossmann , david tapioles , ulrich hans ulmer , erika vogel ( members ) scientific committee radiation oncology daniel zwahlen ( chair ) scientific committee radiation technologists rob lodder ( chair ) scientific committee radiation physics karl rittmann ( chair ) scientific committee oncological nurses barbara stoffel ( chair ) ( michael moseler ) scientific committee radiation biology kathrin zaugg ( chair ) scientific committee psycho oncology gion duno simeon ( chair ) strahlentherapie und onkologie 12 2013 | 1065 content content 1079 abstracts radiation therapy technologists oral 1067 abstracts biology oral 1068 abstracts clinics oral 1073 abstracts physics oral 1080 abstracts nurses oral 1081 abstracts clinics poster 1088 abstracts physics poster 1091 abstracts radiation therapy technologists oral poster 1066 | strahlentherapie und onkologie 12 2013 abstracts biology oral obtained from serial biopsies from an adequate model treated with htrt should be enforced . b01 in vivo profiling of dna damage and repair kinetics after ir : a minimally invasive approach using the dog as a model n . 
effects of different dna damaging agents as well as ddr kinetics have been well characterized in human cells in vitro , but little is known about the kinetics of ddr in vivo . 
herein , fine needle aspirate ( fna ) technique was chosen as a minimally invasive sampling method to address cellular response to dna damaging agents in vivo ( dogs )  . 
these initial findings suggest a high reliability of fna to be used for identification of specific ddr defects in a clinical setting and will contribute to better understanding of dna repair processes in tumor and normal tissues after antineoplastic treatment . b02 impact of variation of cellular repair , fractionation and timing on the synergistic effect of radiotherapy and hyperthermia s . 
the analysis of patient data has shown significant deviations regarding temperature and time gap between heating and rt - fractions during hyperthermia - radiotherapy ( ht - rt )  . 
 the sf - values are varying in the order of a factor 1.44.0 , when the repair constant is changed in a typical range ( 10200 / d )  . 
conditioned media derived from irradiated tumor cells promoted the invasive capacity of nave tumor cells , while conditioned media derived from irradiated , lox - sirna - silenced cells did not stimulate the invasive capacity of nave cells . 
these results indicate a differential regulation of lox - expression and secretion in response to ir and hypoxia , and suggest that lox may contribute towards an escape mechanism in sublethally - irradiated tumor cells . b04 combined radiochemotheraputical strategies for microtubule stabilizing agent ( msa ) - resistant tumors a . 
furthermore , wildtype cells showed an additive antiproliferative response to patupilone in combination with ir and rad001 , respectively , which could not be observed in the patupilone - resistant tumor cells . 
these data demonstrate that the interaction between the tumor cell compartment and tumor microenvironment strongly determistrahlentherapie und onkologie 12 2013 | 1067 abstracts nes the treatment response to different anticancer agents and should be considered as valuable targets especially in a treatment - resistant tumor cell background . b07 relevance of p53 status for response of tumor cells to met inhibitors combined with irradiation b05 secretome profiling for identification of ionizing radiation - activated acquired resistance mechanisms a . 
inherent and / or acquired resistance ( as part of a cell deathescape mechanism ) to the cytotoxic effects of ionizing radiation ( ir ) is increasingly recognized as a significant impediment to the efficacy of radiotherapy . 
for example , we investigated in detail , the effect of ir on expression and tumor cell secretion of platelet derived growth factor a ( pdgfa ) , one of the top hits from array screening . 
the regulation of functional endpoints by these ir - activated factors are now determined , and they will be discussed as potential targets for a combined treatment modality with ir . b06 senescence as a biologic consequence in tumor therapy following met receptor tyrosine kinase targeting in combination with ionizing radiation p . 
medov1 , 2 1department of radiation oncology , inselspital , university of bern , bern , switzerland , 2department of clinical research , radiation oncology , university of bern , bern , switzerland objective . 
cellular senescence is an irreversible cell - cycle arrest that points to a critical role in tumor suppression by blocking tumor growth and the acquisition of additional oncogenic lesions during dna replication and mitosis . 
the met - addicted human gastric cancer cell lines gtl - 16 and hs746t were treated with emd1214063 alone or in combination with ir ( 2 or 4gy ) for 3 and 7 days . 
zimmer1 , 2 1radiation oncology , inselspital , bern , ch , 2dkf , radiation oncology , university of bern , bern , ch , 3medical oncology , inselspital , bern , ch objective . 
recent data indicate that the met - mediated radiosensitization is due to downregulation of an atr - chk1 pathway , which is responsible for intra - s and g2 / m cell cycle arrests following dna damage . 
to further improve the efficacy of radiation treatment , p53 , a major regulator of g1 / s checkpoint arrest was knocked - down in p53 - proficient cancer cells . 
however , those cells tend to be resistant to apoptosis , indicating cell death through an alternative mechanism such as mitotic catastrophe . abstracts clinics oral c01 salvage reirradiation for local failure of prostate cancer after curative radiotherapy : dosimetric and radiobiological modeling of rectal toxicity m . 
even in the absence of clinical signs of toxicity after a 1st rt , rectal mucosa exposed to high rt doses harbors silent 1068 | strahlentherapie und onkologie 12 2013 subclinical damage that may translate in severe side - effects after reirradiation . in our investigation psa bounce is associated with a more favourable biochemical outcome . c02 androgen deprivation and high - dose radiotherapy for oligometastatic prostate cancer patients with less than five regional and / or distant metastases o.f. 
50 pts with synchronous ( n = 7 ) or metachronous ( n = 43 ) oligometastases ( om ) after rp ( 33 pts ) or rtad ( 10 pts ) underwent salvage rt ( median dose 64 gy ) with concomitant ad in all but one pt . 
such a treatment strategy may hypothetically succeed to prolong the failure - free interval between two consecutive ad courses when oligometastatic pts are on intermittent ad salvage and deserves to be further tested in controlled randomized trials . c03 psa bounce after i - 125 prostate brachytherapy correlates with better biochemical outcome p.m. 
from 2001 to 2010 , 714 patients with localized prostate cancer treated with ldr - bt and more than 2 years of follow - up were registered in the database . 
time to bf from bt accounted most reliable between bounce exceeding threshold for bf and psa rise ending in bf or cf . c05 stability of dose to the rectum during salvage radiotherapy with endorectal balloon after prostatectomy t . 
the relative volume changes of the rectal wall exposed to doses > 40gy ( v40 ) , > 60gy ( v60 ) , > 65gy ( v65 ) were calculated . 
thus , we could show that the dose to the rectal wall during treatment was the same or lower compared to the planned dose . strahlentherapie und onkologie 12 2013 | 1069 abstracts c06 clinical course and pattern of failure in long - term survivors with glioblastoma multiforme a . 
roelcke2 1radioonkologiezentrum ksa - ksb , kantonsspital aarau , 2hirntumorzentrum , kantonsspital aarau c08 radiation induced cranial nerve palsy ( ix , xi , xii ) in patients with oropharynx and nasopharynx carcinoma following high dose exposure b.y. 
treatment consisted of macroscopic radical resection ( 12 ) , partial resection ( 4 ) and biopsy only ( 1 ) followed by 60 gy with concurrent and adjuvant temozolamide for 15 patients . 
in 10 patients the recurrence was within 2cm of the initial tumour site , 1 was both local and distant and 1 was distant ( contra - lateral )  . 
a similar analysis is planned for the ksa patients . c07 spot - scanning proton therapy ( pt ) for pediatric parameningeal rhabdomyosarcomas ( pm - rms ) : clinical outcome c . 
with a mean follow - up of 36 months ( range , 7105 ) 11 patients failed : 8 patients experienced in - field local recurrence only , 2 patients developed distant metastasis only and 1 patient developed a meningeal carcinomatosis . 
late effects related to proton therapy include : endocrinopathies ( n = 5 ) , cataract ( n = 3 ) , hearing impairment ( n = 1 ) , soft tissue asymmetry ( n = 1 ) , failure of permanent tooth eruption ( n = 2 )  . 
while the community is aware of the risk for brachial plexus damage due to exposure to high doses radiation ( > 65gy ) , the awareness is less for potential ricnp . 
we retrospectively identified 201 patients with 288 cervical sides radiation exposed to > 65gy to cn lx / xl / xll ( 87 patients with bilateral radiation exposure ) , from 2002 to 2012 . 
84 patients with unilateral and 18 patients with bilateral exposure ( total : 102 cervical sides ) who had loco regional control and a fu of > 24 months [ mean 56 months ( 24111 ) ] were included in this analysis . 
longer fu and a larger sample size may be needed to draw reliable conclusions . c09 pattern of failure after intensity modulated radiation therapy ( imrt ) for squamous cell head and neck ( h&n ) cancer f . 
high rate of marginal failure opens the question of adequate ctv margins . 1070 | strahlentherapie und onkologie 12 2013 c10 acute toxicity in head and neck cancer patients treated with chemoradiation / cetuximab consolidation cetuximab c12 simoultaneous integrated boost ( sib ) - imrt / rapidarc in locally advanced oropharyngeal cancer o . 
own preclinical data suggest that cetuximab consolidation after rt targets tumor cells in irradiated tumor bed [ riesterer , radiother oncol 92 ( 3 ) : 383 , 2009 ]  . 
patients with stage t3 - 4 nx or tx n2b - c ( at least 3 nodes ) and / or gtv > 70cc are treated with crt ( 70 gy , cisplatin 40mg / m2 weekly ) in combination with concurrent cetuximab ( loading dose 400mg / m2 , then 250 mg / m2 weekly )  . 
treatment has been completed in 19 patients , who are evaluable for assessment of acute toxicity [ male / female = 16 / 3 , median age 59y ( 4775 ) ]  . 
the median number of infusions given were : cisplatin : 6 ( 46 ) , concurrent cetuximab : 8 ( 58 ) , consolidation cetuximab : 5 ( 16 )  . 
42 pts with squamous cell carcinoma of the oropharynx , stage iiiiv , were treated with imrt / rapidarc and concurrent chemotherapy ( weekly or 3 - weekly platinum schedule )  . 
fifteen out of 22 pts ( 68% ) in the sib group are alive with a median survival of 59.5 months ( range : 12279 ) ; 5 out of 20 pts ( 25% ) in the sequential one are alive with a median survival of 36 months ( range : 6116 )  . 
we plan to extend this strategy to a larger population of pts in order to build a prospective experience . c11 high resolution fdg - pet / ct in the assessment of retro and parapharyngeal metastases in head and neck squamous cell carcinoma j . 
klaeser2 1department of radiation oncology , 2nuclear medicine , 3orl , head and neck surgery , inselspital , bern university hospital c13 clinical outcome after treatment with highly - conformal modulated beam radiotherapy of patients with operable malignant pleural mesothelioma p . 
the detection of retro / parapharyngeal lymph node metastases ( rplnm ) of head and neck squamous cell carcinoma ( hnscc ) is crucial for correct dose prescription in radiotherapy . 
from 2001 until 2013 , 39 mpm patients were treated with neoadjuvant chemotherapy , extrapleural pneumonectomy ( epp ) , and adjuvant rt ( 56 gy median dose )  . 
the use of imrt increases the probability of local control as compared to 3d - crt , delay thoracic relapse and may impact on disease free survival in the context of radical surgery with epp . strahlentherapie und onkologie 12 2013 | 1071 abstracts c14 outcome of patients with vulvar cancer treated with postoperative imrt n . 
external beam apbi could benefit from ra , increasing ptv dose homogeneity and better sparing of the ipsilateral breast and skthis should be considered for future improvement of this challenging approach . c15 postoperative radiotherapy ( port ) in endometrial cancer : the lausanne experience in 201 consecutive patients o . 
os was 78% ( 95% ci 7284% ) , dfs 72% ( 95% ci 6579% ) , css 84% ( 95% ci 7989% ) , and lrc 84% ( 95% ci 7989% ) , in univariate analyses , significant prognostic factors for os and dfs were age , grade , lymphovascular invasion ( lvi ) , stage , cervical invasion ( ci ) , histology , and lymphadenectomy . 
in the multivariate analysis , independent factors influencing outcome were age ( os , dfs ) , stage ( os , dfs , css ) , lvi ( os , dfs ) , grade ( dfs , css ) , and lymphadenectomy ( os )  . 
pts have been treated on the whole breast to a total dose of 5050.4gy and the booster dose on the surgical bed ranged from 58.7564.4gy in 2528 daily fractions , except in 1 case treated up to 67.6gy due to positive margins . 
we analyzed the acute local toxicity using the eortc / rtog scale : no case with grade 3 , 7 with grade 2a / b and 15 with grade 1a / b highest cutaneous toxicity . 
in our experience imrt / rapidarc sib is feasible even in bilateral breast and well tolerated . 1072 | strahlentherapie und onkologie 12 2013 c18 first year intraoperative radiotherapy with intrabeam ( iort ) for breast cancer at the geneva university hospitals ( hug ) v . 
 no further radiation was given if : age50 years , invasive ductal , mucinous , tubular , medullar or colloid carcinoma , unifocal , no lymphovascular invasion , no extensive in situ component , tumor size = 2m otherwise , additional whole breast radiotherapy ( wbrt ) was given post - operatively . 
among wbrt patients , 11 were evaluable at 2 months after wbrt ( mean follow - up of 6 months postsurgery ) : no patient had heart toxicity , lung symptoms were absent in 10 ( 91% ) patients , grade 1 in 1 ( 9% ) patient . 
we performed a statistical analysis of dvh of ptv ( icru ) , ipsilateral lung ( v20 , v10 , v5 ) , heart ( v10 , v5 ) and skin ( punctual dmax )  . 
their volume equivalence were 8 and 36%.the skin mean maximal punctual dose was 48.5gy , equivalent to 52gy ( a / b10gy ) and 58gy ( a / b2gy ) .mean delivery time was 526sec ( 309893 ) .only 2 patients show a grade 1 skin toxicity . 
breast hypofractionated scheme , previously clinically tested , delivered with td or helical imrt , is feasible and toxicity is negligible . abstracts physics oral p01 phantom based kv - cbct dose plan calculations for re - planning decision : comparison with ct - based dose plans a . 
future investigations on the hu to ed curve and curve stability will be done with the help of a cbct electron density phantom ( cirs )  . p02 first experimental results of motion mitigation by continuous line scanning a . 
line scanning could be shown to mitigate tumour motion of even 10mm as well as discrete spot scanning , while being about three strahlentherapie und onkologie 12 2013 | 1073 abstracts times faster . 
however , even though gitvs and raitvs differ significantly in shape and size , this difference does not necessarily translate into significant differences in the resultant 4d dose distributions . p03 impact of respiratory - correlated ct reconstruction algorithms in the choice of margin definition for free breathing lung treatment s . 
moeckli1 1university institute for radiation physics , centre hospitalier universitaire vaudois ( chuv ) and university of lausanne , lausanne , switzerland , 2university institute for radiation physics , centre hospitalier universitaire vaudois ( chuv ) objective . 
based on the impact of image artifacts and on dose distributions we showed that the mid - ventilation strategy is more robust than the itv - based strategy . p04 adequate margin definition for scanned particle therapy in the incident of intra - fractional motion a . 
4d dose calculations ( 4ddc ) for scanned particle therapy show that in the incidence of motion , it is insufficient to use target contours defined on a reference ct . 
the dose distributions were analyzed and compared according to homogeneity [ hi = ( d2%d98% ) / dprescription * 100% ] and conformity ( ci = prescription isodose volume / target volume ) to the target . 
in comparison to the conventional ff - hybridarc method the dose homogeneity in the target volume is improved , the conformity remains the same , the total number of mus is decreased and the normal tissue sparing is improved . p06 deformation evaluation using cbct for dynamic adaptive radiotherapy ( dart ) in patients with prostate cancer : a planning study c . 
 volumes of prostate , rectum , bladder and seminal vesicle ( sv ) and distances between rectum - symphysis , rectum - bladder and bladder - penile bulb were measured for correlation analysis . 
dynamic adaptive rt ( dart ) for prostate deformation correction has the potential to be beneficial for ptv coverage , particularly in posterocranial direction in supine position . photon techniques but in other cases better sparing was achieved in the low dose region . 
an integrated tp framework was implemented to generate mr / ct based 3d patient models , simulate em and induced heating , optimize temperature , and perform post - processing ( thermal dose quantification , visualization , analysis , reporting )  . 
improved and validated clinical integration and coupling to real - time information is in progress . p08 forward planned modulated electron radiation therapy ( mert ) for different anatomical locations : a comparison with pure photon plans a . 
concerning organs at risk sparing , dvh of mert - based techniques and pure photon techniques showed that in some cases , better sparing was achieved in the high dose region with mert - based techniques compared to pure p09 macro monte carlo interface with beam model for treatment planning in proton therapy m.k. 
based on the beam data of the commissioned beam model and the patient treatment plan , a sampling procedure is defined to provide the particle type , position , direction , energy and weight of the starting particle necessary for the mmc dose calculation . 
stampanoni3 1division of medical radiation physics and department of radiation oncology , inselspital , bern university hospital , and university of bern , switzerland , 2clinic for radiation - oncology , lindenhofspital bern , switzerland , 3institut for biomedical engineering , eth zrich and psi , villigen , switzerland objective . 
for testing purposes , an inverse treatment plan is created for an academic situation and compared to previously obtained forward planning results . strahlentherapie und onkologie 12 2013 | 1075 abstracts results . 
interpretation of the in vivo dose measurements is the near frontier . p13 dosimetric comparison of acuros xb and aaa with compass - ccc calculations for volumetric modulated arc therapy a . 
nicolini1 1iosi oncology institute of southern switzerland , radio - oncology dept , medical physics unit , bellinzona , switzerland , 2yashoda super specialty hospital , hyderabad , india objective . 
to calculate the dose with ccc in compass all fluences were acquired with the imatrixx - 2d detector on a clinac ix ( varian , palo alto , usa ) , 6mv . 
these dose distributions were compared with acuros xb and aaa calculations from eclipse treatment planning system using 3 - d gamma index with distance - toagreement and dose difference criteria set to : 3mm / 3% and 2mm / 2% for targets , organs at risks ( oar ) , 50 and 10% isodose volumes . 
in particular for the ptv the percentage of points passing the 3mm / 3% gamma criteria are 99.70.3% for cccvsacuros , 98.61.0% for cccvsaaa and 97.00.2% for aaavsacuros , averaging all cases . 
this study showed the good agreement of ccc calculations from measured fluences with respect to both acuros xb and aaa algorithms from treatment planning system . p12 pre - treatment qa for vmat flattening filter free beams with portal imager using glaas algorithm p14 sbrt for lung cancer treatments : dosimetric evaluation using fff beams e . 
 nicolini1 1iosi , oncology institute of southern switzerland , medical physics , bellinzona , switzerland , 2kaiser - franz - josef - spital , institut fr radioonkologie , vienna , austria , 3dpartement de cancrologie radiothrapie , crlc val daurelle - paul lamarque , montpellier , france objective . 
the glaas algorithm , already validated to convert pv readings into absorbed dose to water for imrt and ra pre - treatment qa for standard beam , was extended to fff . 
stereotactic treatments for small lung cancer can dosimetrically benefit from the usage of fff relative to the flattened beam , and lower energy would deliver less peripheral dose . p15 towards a more precise dynamic scanned proton treatmentonline deformable motion reconstruction using pca motion model y . 
for 30 breathing cycles ( contain irregular patterns ) , surrogate motion from fiducial markers alone , diaphragm alone and combined are used as predictors to estimate dense motion field . 
our results has shown that online deformable motion reconstruction is feasible , and emphasized the necessity of predicting spatial non - rigid motion and the lost motion in depth due to the bev imaging geometry . 
for template - based 2a plans in 27 cases out of 181 an exceeding of the objectives for one or more oar was found , in 13 cases an overor under - dosage in the ptv in direct comparison to imrt . 
eclipse is able to achieve comparable plan quality for elekta vmat delivery technique to that of imrt in terms of target coverage and critical structure whereas plans with 2 arcs show less exceeding of the objectives than plans with 1 arc . p17 collapsed cone algorithm and its impact on dose distributions in hdr brachytherapy for partial breast irradiations d . 
this work was supported by nucletron . p16 vmat planning for elekta linacs in the varian planning system eclipse : a comparison study of vmat plans with fixed field imrt plans p18 log file based dose calculations as a quality assurance tool in scanned beam proton radiotherapy s . 
our treatment control system consists of an active ( tds ) and passive ( tvs ) part , both driven by steering files generated via the treatment planning syste from these , pre - treatment doses can be reconstructed . 
in addition , post - treatment doses can be reconstructed from log files written by the tvs which the actual measured parameters of the delivery ( position , mu etc )  . 
furthermore , they are a potential tool in the definition of tolerances for quality checks by exploring the clinical significance of possible delivery errors . p19 a breathing anthropomorphic phantom for experimental studies of moving tumors in scanning proton therapy m . 
an external skin motion has been recorded using both an optical distance sensor and the vision rt systefinally , first scanned proton beam tests have been performed with the phantoplanned and delivered doses ( 1gy , measured using gafchromic films ) in the static case agreed well , with a standard deviation of dose in the tumour of 3% . 
this led to reduced residual motion , and excellent dosimetrical results . p21 hypofractionated radiotherapy has the potential for second cancer reduction uwe schneider1 , 2 , jrgen besserer2 , matthias hartmann2 1vetsuisse faculty university of zrich , zrich , 2radiotherapy hirslanden , hirslanden medical center , aarau objective . 
it is also found that tissue which is irradiated using large dose fractions to dose levels lower than 10% of the target dose potentially develop less sarcomas when compared to tissues irradiated to all dose levels . 
additionally , tracked dose distributions were p22 retrospective analysis of target volume dose coverage using cbcts acquired for accelerated hypo - fractionated radiation therapy ( ahfrt ) in lung cancer g . 
dose prescription was 60gy to the ptv ( itv plus 5mm margins ) delivered in 3 , 5 or 8 fractions with rapidarc , using 3 to 5 arcs , 6mv energy beam and the novalis tx linac . 
twenty cbcts were randomly 1078 | strahlentherapie und onkologie 12 2013 selected to re - calculate dose coverage to the target in patients treatment position , having tested the feasibility on phantom ( results presented separately )  . 
this preliminary study showed that good patients positioning leads to dose distribution reproducibility respect to simulation as verified using cbtcs . abstracts radiation therapy technologists oral rt01 proton therapy of ocular tumors ( optis2 ) at psi avoidance of upper orbital bone irradiation during treatment of superiorly located eye tumors p . 
using ac , the mean discrepancy of the liver centre of mass between inhalation and exhalation was reduced by 2.6mm ( p = 0.04 ) in the craniocaudal plane , with residual motion of 6.9mdiscrepancies in the lateral and anteroposterior planes were smaller and not significant . 
such data will help guide the selection of patients that have the most to gain from ac , while sparing those that would not benefit from the discomfort and extended set - up time involved . rt03 development and implementation of a non - invasive stereotactic head frame f . 
to develop and implement a non - invasive head frame for intracranial stereotactic radiotherapy ( srt ) , which is more efficient and easier to use while maintaining and improving treatment accuracy . 
twenty patients ( 140 fractions ) were treated with the cv frame , 19 patients ( 152 fractions ) were treated with the bl systepre and post treatment imaging was performed using cbct . 
intra - fractional motion with the civco frame proved to be slightly less than with the brainlab system while the pitch and roll deviations in initial setup proved to be marginally larger . 
due to the large number of pediatric cases we treat at the usz , and the lack of an igrt kv - imaging protocol for this patient group , we optimized imaging practice while simultaneously reducing the dose applied . 
the following cumulative dose ranges were measured for the 4 various exposure methods : 4.59 mgy with daily unoptimized kv ; 2.253.25mgy with daily optimized kv ; 1500mgy with daily mv setup ; and 500mgy with weekly mv double exposure . 
by optimizing kv imaging exposure we were able to considerably reduce dose by up to 75% for a 3 - year - old child , and 36% for a 6 - year - old . 
a lot of adaptations have been made to optimize the computing financial system . abstracts nurses oral nu01 auswirkungen der therapie bei prostata - ca , auswirkungen auf das mnnliche organ antihormontherapie / bestrahlung / operation , medizinischer hintergrund m . 
in an environment of conflicting expert opinions a decision for a therapy has to be made , which could have irreversible consequences such as incontinence and impotence , incontinence . nu03 continence advice for prostate ca b . 
these are the key points listed which are : basicsrisks and preventive measurestherapeutic approaches to promoting continencematerialssituation at home . nu04 a different approach to be a nurse going new wayspresentation of a project which promote sexual counselling for cancer patients and their partner and education and training for nurses related to intimacy and sexual issues c . 
nursing staff have to introduce appropriate products and include patient preferences to different sunscreen to increase the adherence even a long time after the end of radiotherapy . abstracts clinics poster cp01 early toxicity during postoperative hdrbt for endometrial carcinoma depends on the dose per fraction and on total dose r . 
in the first part of this workshop we will focus on those aspects of a psychosocial assessment that are helpful to be gathered in order to anticipate the patients social situation ( work , social insurances , financial situation , possible family support system etc . ) and what consequences unemployment or other changes of life style may have . 
by using case examples there will be given an overview about psychosocial and psychological effects the specific malignant disease might have and what psychosocial interventions could be recommended . nu06 arbeit und krebs bedeutung der arbeitsunfhigkeit fr patient und familie m . 
by using case examples there will be given an overview about psychosocial and psychological effects the specific malignant disease might have and what psychosocial interventions could be recommended . nu07 skin melanomaa complex disease l . 
progress in the analysis of cellular mechanisms through the development of molecular biology and biochemistry have led to a better understanding of antitumoral immune responses strahlentherapie und onkologie 12 2013 | 1081 abstracts cp02 rtog 1005 breast cancer trial : what is the future standard for fractionated adjuvant radiotherapy ? s . 
with recent technological advances in conformal radiotherapy planning ( rt ) and delivery , there has been an increasing trend towards adjuvant hypofractionated rt in breast cancer ( bc ) as an alternative to 2gy daily dose . 
the number of patients with benign diseases irradiated in our institute has increased from 125 patients in 2009 to 205 patients in 2011 , 15% of our entire patient population . 
the aim of the study is the prospective and objective . cp03 stent as bridging to curative radiotherapy for malignant trachealstenosiscase report cp05 lymphoepithelial carcinoma of the parotid gland : case report of a rare cancer and review of the literature d . 
bronchoscopy showed subtotal tracheal occlusion over 45csurgical resection was impossible due to the longitudinal extent of the stenosis and tumor invasion of the surrounding mediastinu following tracheal desobliteration in a rigid technique , a stent was placed for maintenance of airway patency . 
lec of the parotid gland is a rare disease in caucasian populations ( 5% of published cases in the reviewed literature )  . 1082 | strahlentherapie und onkologie 12 2013 cp06 what is the correct dose and volume definition in palliative radiotherapy beyond simple bone metastases ? cp08 nipple - areolar sparing with prone setup for boost radiotherapy of breast tumor bed k . 
in some cases we found a long - term local remission and / or complete radiological regression after using higher doses , in one case up to 66gy with normal fractionation . 
our cases show exemplary the need for prospective research to define optimal dose and volume concepts in treating patients with metastatic soft tissue involvement . cp07 comparison of 3dcrt , imrt and vmat treatment plans for bilateral breast cancer n . 
prone , as compared with supine , provided the most homogeneous dose distribution to the tumor bed with better sparing of the nac . cp09 radiation - primed cryptogenic organizing pneumonia ( cop ) after whole breast irradiation for dcis : a case report c . 
cryptogenic organizing pneumonitis ( cop ) is a rare and idiopathic clinico - pathological syndrome characterized by a pneumonia - like illness with excessive proliferation of granulation tissue within small airways and alveolar ducts associated with chronic inflammation in the surrounding alveoli . 
bal revealed ymphocytosis ( 18% ) , elevated cd4 / cd8 - quotient , elevated eosinophils ( 5% ) and acute inflammatory cells and tbb fibrinous reaction with foam cells . 
uncovered ln levels ( absolute volumes or quotients ) can be established but their medical significance is unclear . cp10 a new group of breast cancer patients : patients following breast conserving surgery with 12 axillary macrometastases in sentinel procedure without axilla dissection k . 
our first goal was to differentiate between patients ( pts ) who were eligible to the criteria of the ascog z0011 trial and those who were treated according to this trial despite exclusion criteria . 
further investigations are needed to show if the american z0011 patient collective are comparable to the swiss pts who are treated according to the protocol . cp11 dose distribution among level i and ii lymphnodes ( ln ) in breast cancer patients with 12 axillary sentinel macrometastases without axillary dissection treated with tangential fields l.e.j. 
parts of ln levels below the id - 90 were found cranially of the rt field and between the chest wall and dorsal rt border . cp12 do ( chemo ) - radiotherapy patients need other forms of social support for access to cancer care than other cancer patients ? k . 
all patients who came in february 2012 for consultation or ambulant treatment to a centre of the dvo ( dpartement valaisan doncologie ) or to the unique private practice of the region were asked to answer a survey covering several themes as age , kind of treatment , how the patient travelled and which kind of support was necessary to travel . 
amsler1 1radio - onkologie amsler ag , 2medizinische universittsklinik , onkologie , hmatologie , immuntherapien , kantonsspital baselland / liestal , 3onkologie - hmatologie , medizinische universittsklinik , kantonsspital baselland / bruderholz , baselland objective . 
although our small number of patients precludes any conclusion , we believe that capecitabine with or without mitomycin c is a safe alternative to 5fu and achieves excellent locregional results . 
to the best of our knowledge , this is the first clinical trial combining pt and ht in sts . cp14 differential effectiveness of radiotherapy versus radiotherapy and hyperthermia in a soft tissue sarcoma of the extremity : a case study e . 
 bodis1 1radioonkologiezentrum ksa - ksb , kantonsspital aarau , ch , 2department of radiation oncology , university hospital , zurich , ch , 3uniklinik balgrist , zurich , ch , 4department of clinical pathology , university hospital , zurich , objective . 
a 78 - year - old male with a mycosis liposarcoma of 2076.6cm in the upper arm received preoperative rt of 50gy / 25 fr / 5 wks to the entire tumour . 
hyperthermia along rt can lead to appreciable tumour downstaging to enable better limb preservation surgery . cp15 a multi - institutional phase i / ii pilot study of proton radiotherapy with local hyperthermia in adult soft tissue sarcoma n.r. 
a preoperative dose of 5055 gy ( rbe ) or radical dose of 7276 gy ( rbe ) will be delivered at 1.82gy ( rbe ) / fraction for 5 fractions / week . 
at 5 weeks of completion of pt and ht , patients with adequate local tumour regression permitting r0 resection will be considered for surgery within 3 to 6 weeks of pt and ht treatments . 
the pilot study is an attempt to exploit the physical dose distribution advantage of proton beams along with the thermal radiocp16 hyperthermia collaborative research network ( hcrn ) aargau , solothurn and zurich n.r. 
bodis1 1radioonkologiezentrum ksa - ksb , kantonsspital aarau , 2psi , villigen , 3division of radiation oncology , vetsuisse - faculty , zurich , 4university hospital , zurich , 5eth / itis , zurich , 6kantonsspital baden objective . 
hcrn involves ( a ) clinical trials : a phase iib trial is ongoing in bladder cancers while a phase i / ii trial of preoperative ht and proton therapy in soft tissue sarcomas will be launched in mid 2013 . 
the network could be expanded by integrating other interested swiss institutions to form a swiss hyperthermia collaborative research network ( shcrn )  . cp17 prospective evaluation of fractionated stereotactic radiotherapy for brain metastases s . 
national registration of this data set for all patients treated with srt could yield a sufficient cohort to answer these uncertainties . cp18 diffusion tensor imaging to assess tumor infiltration and refine rt planning for patients with gbm j . 
our aim is to reduce the irradiated volume , and hence late effects , by including the demonstrable areas of tumour infiltration and excluding areas at low risk of infiltration . 
gallen , interdisciplinary guidelines in treatment of prostate cancer had been developed , recommending combined radiotherapy and androgen deprivation therapy depending on tumor staging , gleason - score and psa value . 
from february 2010 to january 2013 , 127 patients with different tumor stages ( ct1 - 3b , cnx - n0 , cm0 ) had been assigned to primary irradiation and received a mri of the pelvis for treatment planning . 
 mri - supported treatment - planning should be considered a standard procedure in the management of these patients . cp20 does an mri of the pelvis play a role in the radiation decision procedure in salvage - treatment patients with prostate cancer ? k . 
our results show that routine mri of the pelvis may lead to relevant information on treatment - decision in a substantial number of salvage - treatment patients with prostate - cancer . 
therefore in addition to common treatment - planning procedures , mri should be considered in the work - up in the postoperative setting . cp21 use of 18fdg - pet standard uptake value as a metabolic predictor of bone marrow response to radiation : impact on acute and late hematological toxicity in cervical cancer patients treated with chemo - radiotherapy f.g. 
ozsahin1 1department of radiation oncology , centre hospitalier universitaire vaudois chuv , lausanne , switzerland , 2velocity medical solutions , atlanta usa , 3department of nuclear medicine , chuv , lausanne , switzerland objective . 
our study suggests that delivering 6672 gy to gbm patients with concomitant chemotherapy is feasible with an acceptable risk of acute cns toxicity . cp23 the eoc uroboard , a multidisciplinary approach to the management of patients with urogenital cancer c . 
pesce1 , 2 1radiotherapy and 2medical oncology iosi , 3urology and 4radiology , eoc , bellinzona , 5pathology and cancer registry , locarno , and 6international prostate research group objective . 
the need of a tumour board ( tb ) for urogenital tumors ( ut ) at ente ospedaliero cantonale ( eoc ) derives from the necessity to offer patients ( pts ) a treatment strategy agreed by the relevant specialists . 
the uroboard guarantees a better definition of tailored treatment strategy for urogenital cancer pts , contributes to the updating of tumour - specific guidelines and increases motivation for enrolment in clinical trials . cp24 qart : evaluating the correlation between percentage rate of fall of psa and positioning accuracy c . 
75 patients with hrpc were treated with pelvic rt between 2003 and 2011 at iosi , 54 with exclusive rt and 21 with post - operative adjuvant ( 12 ) or salvage ( 9 ) rt . 
longer follow up will be needed in order to better evaluate the late outcomes . abstracts physics poster pp01 investigation of the dose accuracy and benefits of gated imrt and vmat for clinical implementation a . 
for the tests the phosphor film ( kodak hr ) was inserted in a phantom cassette made of water equivalent plastic and irradiated following the verification plan from eclipse version 10.0 ( varian medical systems )  . 
the cr system showed a good response for relative dose measurements only for high dose regions ( over 1gy ) , but the measurements in absolute dose never reached the gamma agreement index of 95% . 
therefore we will investigate its use for hypo - fractionated and single dose stereotactic treatments . pp03 a non - invasive tumor referencing technique for external beam radiation therapy of intraocular tumors m.b. 
 kowal1 1artorg center for biomedical engineering research , university of berne , 2division of medical radiation physics , berne university hospital , university of berne , 3department of radiation oncology , berne university hospital , university of berne objective . 
for each porcine eye and tilting angle , the corneal epithelium was automatically segmented in 3d using a self - developed algoriththe reconstructed surface of the cornea was finally used to measure rotation and translation of that eye . 1088 | strahlentherapie und onkologie 12 2013 results . 
oct based cornea tracking seems to be an interesting technique for the non - invasive referencing of intraocular tumors during external beam radiotherapy . pp06 total scalp irradiation : traditional and modern techniques j . 
exactrac consists of 2 x ray ( xr ) tubes floor mounted with 2 detectors and an infra - red ( ir ) camera system which controls a 6d robotic table . 
traditional techniques involving junctioned static beams can provide adequate shielding to the organs at risk ( oar ) ; however dose distribution over the scalp is somewhat inhomogeneous , and dosimetric uncertainties can be introduced with the shifting of field junctions . 
the patient was treated with a 7 field imrt plan for the whole scalp ( 40gy ) , with a reduced dose prescribed to the area previously treated ( 36gy )  . 
due to the variability of factors influencing treatment decisions , the treatment technique should always be chosen on an individual patient basis . pp05 influence of a metal reinforced catheter in deep hyperthermia treatment d . 
to verify the treatment beam isocenter with gantry - , couchand collimator - rotation and to verify the coincidence of the beam and the imaging isocenter , a winston - lutz - test ( wlt ) has to be carried out after each mounting of the mmlc . 
a deviation can occur either because of badly calibrated lasers or because of incorrect axes of rotation ( gantry , collimator , couch ) which would then have to be adjusted . 
in the topograms the distance between the most inferior part of the breast and the diaphragm , and the distance from the midline to the left border of the heart were measured . 
in order to overcome the mentioned problems , bh should be used for imaging and irradiation in all cases . pp09 the value of t2 - weighted mr imaging for optimization of postplanning dosimetry after permanent iodine - 125 seed brachytherapy in men with localized prostate cancer n . 
the standard for post - implant dosimetry of permanent radioactive i - 125 seeds implantation of the prostate is a ct - based identification of seeds , prostate and organs at risk ( ct - based )  . 
comparison was made for two energies 6 and 10mv for flattened beam fb and fff beathree different clinical dose rate 600 , 1400 and 1600 mu / min have been used . 
using the above chambers is well suitable for quality assurance under fff beathe two voltage method is too simple to accurately determine the pion and charge multiplication , though the measured results from many authors and this work show using the two voltage method for a dosimetry in clinical application is satisfied . pp11 implementation and validation of pinnacle for stereotactic body radiotherapy with a flattening filter free linac j . 
by removing the flattening filter a higher dose rate and a relative reduction of the out - of - field dose can be achieved which would be an asset for stereotactic body radiotherapy ( sbrt )  . 
fff beams accomplished additional dose sparing for lung and drastically reduced the irradiation time . 1090 | strahlentherapie und onkologie 12 2013 abstracts radiation therapy technologists oral poster rtp01 in - vivo thermo - luminescent dosimetry in patients with breast cancer treated with a volumetric modulated arc therapy ( vmat ) technique d . 
since may 2012 , 9 patients with a non - operable non - small cells lung cancer stagei and size 3cm and having no indication for conventional radiation therapy have undergone a hypofractionated treatment in our centre . 
comparison between preand post - treatment cbcts showed an average movement of 0.13cm in the anterior - posterior direction and no movement in the left - right and superior - inferior directions . 
due to a stable immobilisation system , the speed of delivering with vmat , and the use of igrt , our method of positioning is relatively precise and effective . rtp02 pre - treatment quality assurance ( qa ) for stereotactic cranial plans c . 
a total of 26 dose plans , dca from iplan ( brainlab ) 19 pts and vmat from eclipse ( varian ) 7 pts , were verified with different qa methods . 
using a lucy phantom and a diamond chamber , each treatment field was checked for absolute isocenter dose and gafchromic ebt3 film dosimetry was selected to verify total dose plans in the 2d axial planes . 
deep seated tumours located in the pelvis , abdomen and lower extremities can be heated to temperatures of 4143c using a radiofrequency applicator and so significantly enhance the effects of radio strahlentherapie und onkologie 12 2013 | 1091 nup01 qualified support for h&n patients during eight weeks of radiation therapy with the help of our reference standards j . 
a previous simulator room was divided to house a deep ht system enclosed in a faraday cage , a superficial ht room and a control rooprovision is made for local storage of technical and treatment equipment as well as patient supplies to create an ergonomic working environment . 
the hyperthermia group also profits from ongoing international collaboration with other experienced hyperthermia centres , following on from an initial clinical and technical training program at these institutes . rtp06 evaluation of the accuracy and reproducibility of non - invasive patient immobilisation for cranial stereotactic radiotherapy l . 
in the absence of significant changes to the technique , this can be attributed to a combination of good patient explanation , careful bite block preparation and increased team experience . 
a non - invasive , reproducible , comfortable patient set - up can be achieved for small volume , highly conformal radiotherapy . 1092 | strahlentherapie und onkologie 12 2013 literaturkommentiert strahlenther onkol 2013 189 : 10511053 doi 10.1007 / s00066 - 013 - 0449 - 4 online publiziert : 27 . 
oktober 2013 springer - verlag berlin heidelberg 2013 d.habermehls.e.combs klinik fr radioonkologie & strahlentherapie , universittsklinik heidelberg stereotaktischgefhrte radiotherapiebeim lokalfortgeschrittenen hepatozellulrenkarzinom gepoolteanalyseauszweiphase - i / ii - studien originalbeitrag bujold a , massey ca , kim jj et al ( 2013 ) sequential phase i and ii trials of stereotactic body radiotherapy for locally advanced hepatocellular carcinoma . 
bei der hier zu kommentierenden arbeit handelt sich um eine gepoolte analyse zweier vorangegangener phase - i / ii - studien zur stereotaktischen radiotherapie des lokal fortgeschrittenen hepatozellulren karzinoms ( hcc )  . 
eingeschlossen wurden patienten mit der diagnose eines hcc gem der leitlinien der aasld ( american association for the study of liver diseases ) , also entweder mit bioptischem nachweis , mit nachweis durch 2 unterschiedliche bildgebende modalitten oder durch eine bildgebende modalitt in verbindung mit einem - fetoprotein ( afp ) > 200 nmol / l . 
darber hinaus waren die anzahl an tumoren und die gesamtgre im ersten protokoll nicht limitiert , es mussten lediglich 800 ml nichtbefallenes lebergewebe vorhanden seim zweiten protokoll waren maximal 5 umschriebene tumore mit einem maximalen durchmesser von 15 cm erlaubt ; das nichtbefallene lebervolumen musste hier mindestens 700 ml betragen . 
extrahepatische manifestationen waren in beiden studien kein ausschlusskriteriu in beiden protokollen wurden dosen von 2454 gy ( mediane dosis 36 gy ) in 6 fraktionen verabreicht , wobei zwischen den fraktionen ein tag pausiert wurde . 
die dosisverschreibung erfolgte mit hilfe eines ntcp - modells ( normal tissue complication probability ) unter bercksichtigung des risikos zur entwicklung einer rild ( radia tion induced liver disease )  . 
die stereotaktisch gefhrte radiotherapie mit 6 fraktionen ist wirkungsvoll bei patienten mit lokal fortgeschrittenem hcc und einem child - pugh - score a , wenn keine andere lokal ablative methode verfgbar ist . 
das hauptproblem bleibt der intrahepatische progress auerhalb des bestrahlungsfelds , so dass der fokus zuknftiger studien auf einer kombination lokal ablativer manahmen mit einer systemischen therapie liegen sollte , z . 
dies liegt vor allem darin begrndet , dass nichtzirrhotische hccpatienten einer resektion oder transplantation zugefhrt werden und zirrhotische patienten auerhalb der milan - kriterien vorzugsweise mit interventionell - radiologischen lokal ablativen verfahren wie der tace ( transarterielle chemoembolisation ) oder der rfa ( radiofrequenzablation ) behandelt werden . 
die ergebnisse der dawson - gruppe [ 1 , 2 , 3 ] sind von groer relevanz und besttigen vorangegangene ermutigende kleinere phase - iund - ii - studien , die ebenfalls bei dieser indikation eine hypofraktionierte sbrt zum gegenstand hatten [ 4 , 5 , 6 ]  . 
eine tumorthrombose lag bei 55% , multiple lsionen bei 61% und metastasen bei 12% vor . f es wurden dosen zwischen 24 und 54 gy ( 36 gy im median ) in 6 fraktionen eingesetzt und im individuellen fall mit hilfe eines rild - ntcpmodells berechnet . 
der von den autoren bereits in vorarbeiten etablierte parameter fr das dosiseffektiv bestrahlte lebervolumen ( veff ) wurde als maximalwert zugewiesen ( im protokoll 2 60% ) , bis zu dem schrittweise die einzeldosen von 95 gy reduziert wurden , ausgehend von < 25% [ 1 , 2 , 3 ]  . 
die dosisberechnung ist hierbei nicht trivial und kann nicht einfach an gewohnte kenngren und parameter wie tumorgre / ptv , v30 der leber , mittlere leberdosis , dosierung auf beispielsweise isozentrum oder 80% - isodose adaptiert werden . 
das zugrundeliegende modell ist zwar gut beschrieben und offensichtlich valide , weist jedoch zugegebenermaen eine gewisse komplexitt auf und ist nicht ohne schwachstellen ( in der initialen publikation des modells werden ltere daten von hyperfraktionierungsbehandlungsprotokollen umgerechnet und es wurden primre und sekundre lebertumore eingeschlossen , [ 3 ] )  . 
leider gibt es in der arbeit keine detaillierten angaben , ob nicht gerade diese patienten von der eingesetzten technik und dosis profitiert haben . f es wurden lediglich patienten im child - pugh - stadium a eingeschlossen , so dass die hier gewonnenen erkenntnisse nicht auf die schlechteren stadien b und c bertragbar sind . 
habermehl d , debus j , ganten t et al ( 2013 ) hypofractionated carbon ion therapy delivered with scanned ion beams for patients with hepatocellular carcinoma feasibility and clinical response . 
combs se , habermehl d , ganten t et al ( 2011 ) phase i study evaluating the treatment of patients with hepatocellular carcinoma ( hcc ) with carbon ion radiotherapy : the prometheus - 01 trial . 
mendez romero a , wunderink w , hussain sm et al ( 2006 ) stereotactic body radiation therapy for primary and metastatic liver tumors : a single institution phase iii study . 
liang sx , zhu xd , xu zy et al ( 2006 ) radiation - induced liver disease in three - dimensional conformal radiation therapy for primary liver carcinoma : the risk factors and hepatic radiation tolerance . 
xu zy , liang sx , zhu j et al ( 2006 ) prediction of radiation - induced liver disease by lyman normal - tissue complication probability model in three - dimensional conformal radiation therapy for primary liver carcinoma . 
acta oncol 50 : 11911198 strahlentherapieundonkologie122013 | 1053 original article strahlenther onkol 2013 189 : 10091014 doi 10.1007 / s00066 - 013 - 0467 - 2 received : 5 april 2013 accepted : 16 september 2013 published online : 8 november 2013 springer - verlag berlin heidelberg 2013 l.w.vanbockel1e.m.monninkhof2f.a.pameijer3c.h.j.terhaard1 1 department of radiation oncology , university medical centre utrecht 2 julius center for health sciences and primary care , university medical centre utrecht 3 radiology , university medical centre utrecht importanceoftumorvolume insupraglotticandglottic laryngealcarcinoma at present about 50% of laryngeal carcinoma patients are primarily treated with ( chemo - ) radiotherapy [ 1 ]  . 
since there is a large variation in volume within t - stages [ 10 , 15 , 16 , 17 ] , volume might have additional prognostic value besides t - stage in patients with laryngeal squamous cell carcinoma ( scc )  . the aim of our study was to assess the prognostic value of tv compared to and in addition to t - stage in glottic and supraglottic laryngeal carcinoma on local control ( lc ) , disease - free survival ( dfs ) , and overall survival ( os )  . material and methods patients between 1996 and 2009 , 689 patients were treated for laryngeal scc at the radiation oncology department of our hospital . 
to improve group homogeneity , we included patients with supraglottic and glottic laryngeal scc , who were primarily treated with accelerated radiotherapy according to the aso schedule [ 18 ] or who were included in the arcon study [ 19 ]  . 
delineation was performed using 3d delineation software ( developed in - house ) [ 20 ]  . t - stage in a previous study , division of t - stage 2 in 2a and 2b based on the mobility of the vocal cord was suggested , i.e. , in stage t2a the mobility of the vocal cord is normal and in t2b the mobility of the vocal cord is impaired [ 18 ]  . 
if patients were lost to follow - up in the radiation oncology department , follow - up data were retrieved from other hospitals , general practitioners or municipal databases , up until the time of analysis . 
for statistical analysis , dfs time was calculated as the number of months between the date of diagnosis and the date of death , local or regional recurrence , distant metastasis or censoring , whichever occurred first . 
censoring local control ( lc ) and overall survival ( os ) were also included , as secondary outcomes . statistical analysis baseline characteristics are reported as means for continuous variables or as percentages for categorical or dichotomous variables stratified by patients who developed or did not develop an event . 
we applied crude and multivariable cox regression analysis to relate volume ( continuous ) , t - stage , and the combination to 5 - year dfs , os , and lc . 
we assessed 5 cox regression models : ( 1 ) a crude model with volume only , ( 2 ) with t - stage only , and ( 3 ) with location only , ( 4 ) a model combining volume and t - stage , and ( 5 ) model 4 plus location as covariate . prognostic performance of the models was examined by determination of the models discrimination . 
a summary of the patients characteristics for 150 patients are provided in .tab.1. in 48 patients , 65 events were recorded ( 33 local recurrences , 10 regional recurrences , and 22 distant metastases )  . 
we applied crude and multivariable cox regression analysis to relate volume ( continuous ) , t - stage and the combination to 5 - year dfs , os , and lc . 
perhaps prediction of dfs , os , and lc could be improved by including tumor volume into the staging process . keywords laryngeal neoplasms t - stage treatment outcome survival analysis neoplasm staging einfluss des tumorvolumens beim glottischen und supraglottischen larynxkarzinom zusammenfassung ziel . 
anschlieend wurden die zusammenhnge von tumorvolumen , t - stadium und die kombination beider kriterien mit dem dfs , os und der entwicklung eines lokalrezidivs nach 5 jahren mittels univariater und multivariater cox - regression analysiert . 
eine ergnzung des t - staging mit der untersuchung des tumorvolumens knnte daher zu einer verbesserten voraussage von dfs , os und der entwicklung eines lokalrezidivs fhren . schlsselwrter larynxkarzinom t - stadium behandlungserfolg berlebensanalyse neoplasie - staging strahlentherapieundonkologie122013 | 1011 original article follow - up ( months ) follow - up ( months ) follow - up ( months ) glottic vs supraglottic glottic supraglottic glottisch - censored supraglottisch - censored follow - up ( months ) follow - up ( months ) follow - up ( months ) tstage 1 + is + 2a 1 + is + 2a - censored 2b - censored 3 - censored 4 - censored fig . 
there is no association between location and local control or os . combination of t - stage and tv when we combined tv and t - stage in the cox proportional regression analysis , the significant association between tv and dfs or os is maintained . 
although volume and t - stage have been investigated with respect to outcome ( in univariate and multivariate analysis ; .tab.3 ) , the combination of the two as one predictor has never been investigated . in this study , we compared the predictive value of t - stage and volume and their combination on outcome in patients with laryngeal scc . 
3 results in literature of association between volume and outcome reference location treatment outcome diagnostic modality volume ( mean cm3 ) 10.3 glottic radiotherapy supraglottic mri radiotherapy glottic unknown radiotherapy glottic and supraglottic supraglottic 4.5 ( rtx ) 11 ( surgery ) unknown radiotherapy or surgery radiotherapy supraglottic unknown radiotherapy ljumanovic et al . 
 [ 14 ] van bockel et al . glottic and supraglottic radiotherapy s significant ( p < 0.05 ) , ns non - significant , bs borderline significant , na not assessed . results univariate results multivariate volume t - stage volume t - stage glottic unknown radiotherapy only t3 only t3 better discriminative ability on os . 
for local control , t - stage seems to have a better discriminative ability than tv , but combination of both predictors improved the discriminative ability of the model . for oropharyngeal , oral and hypopharyngeal carcinoma , tumor diameter is included in t - staging . 
thus , further research on how to implement volume in t - stage is warranted . in our study , location did not influence the association between tv / t - stage and local control , os or dfs . 
also , in the netherlands the 5 - year survival is 85% for glottic tumors and 50% for supraglottic tumors ( iknl : integral cancer centre the netherlands )  . 
furthermore , another reason why we did not find a large effect of location on outcome might be the fact that all patients were treated with accelerated radiotherapy schedules instead of conventional schedules . 
in our opinion , it is possible that accelerated radiotherapy counteracts possible differences in glottic and supraglottic laryngeal scc . this study had some limitations , which should be mentioned : using tv in clinical staging could lead to some problems . 
therefore , we tried to diminish this variability by delineating each ct scan with at least two observers . a strength of this study is that we included a relatively large homogenous strahlentherapieundonkologie122013 | 1013 19 . 
janssens go , rademakers se , terhaard ch et al ( 2012 ) accelerated radiotherapy with carbogen and nicotinamide for laryngeal cancer : results of a phase iii randomized trial . 
de stefani e , boffetta p , deneo - pellegrini h et al ( 2004 ) supraglottic and glottic carcinomas : epidemiologically distinct entities ? int j cancer 112 : 10651071 25 . 
cooper js , mukherji sk , toledano ay et al ( 2007 ) an evaluation of the variability of tumor - shape definition derived by experienced observers from ct - images of supraglottic carcinomas ( acrin protocol 6658 )  . 
murakami r , furusawa m , baba y et al ( 2000 ) dynamic helical ct of t1 and t2 glottic carcinomas : predictive value for local control with radiation therapy . 
freeman de , mancuso aa , parsons jt et al ( 1990 ) irradiation alone for supraglottic larynx carcinoma : can ct findings predict treatment results ? int j radiat oncol biol phys 19 : 485489 original article group of patients ( n = 150 ) , with laryngeal scc only , all treated with accelerated radiotherapy . 
there are several other studies that investigated the influence of tv on outcome , but some used different locations of head and neck cancers , or used different modalities for delineation ( mri / ct )  . 
terhaard state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 10611063 doi 10.1007 / s00066 - 013 - 0498 - 8 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
20 , d - 65189 wiesbaden , e - mail : prott@bvdst.de personalia professor michael bau mann mit dem ecco clinical research award der europischen krebs gesellschaft geehrt professor michael baumann , prsident der deutschen gesellschaft fr radioonkologie ( degro ) und direktor der klinik und poliklinik fr strahlentherapie und radioonkologie des universittsklinikums carl gustav carus in dresden , erhlt den ecco clinical research award fr seine erfolgreiche ber 20 - jhrige forschungsttigkeit in der strahlentherapie . 
wir gratulieren unserem prsidenten und freuen uns mit ihm , dass diese hohe europische auszeichnung an einen renommierten deutschen radioonkologen vergeben wird , erlutert professor frederik wenz , direktor der klinik fr strahlentherapie und radioonkologie am universittsklinikum mannheim und pressesprecher der degro die strahlentherapie ist eine der tragenden sulen in der krebstherapie und fester bestandteil fr eine stetige verbesserung der krebsbehandlung . 
 unter professor baumanns leitung wird beispielsweise an der entwicklung von tumormarkern gearbeitet , die wiederum die basis bilden knnen , um mithilfe von medikamenten den tumor empfnglich fr die strahlentherapie zu machen . 
 diese anstze zeigen , wie innovativ die strahlentherapeutische forschung in deutschland ist und welche bedeutung sie im zusammenspiel mit den anderen krebstherapien hat . norbert hodapp , freiburg mit der glocker medaille geehrt die deutsche gesellschaft fr medizinische physik hat ihre hchste auszeichnung , die glocker medaille , an herrn norbert hodapp verliehen . 
 nach seinem anschlieenden eintritt in die abteilung fr strahlentherapie des universittsklinikum freiburg , der er auch heute noch angehrt , widmete er sich schwerpunktmig der entwicklung der dynamischen bestrahlungstechniken sowie den fragen der qualittssicherung in der strahlentherapie . 
 in den jahren 2007 2011 war hodapp mitglied im vorstand der deutschen gesellschaft fr radioonkologie ( degro ) , wo er fr das fach medizinische physik an der programstrahlentherapie und onkologie 12 2013 | 1061 professor peter kneschaurek zum gro ehrenmitglied ernannt jubilare mitteilungen der fachgesellschaften matischen gestaltung der zukunft der deutschen radioonkologie wesentlich beteiligt war . herr hodapp hat sich ber jahrzehnte mit herausragendem engagement und hervorragendem erfolg nicht nur fr die medizinische physik und die dgmp , sondern auch fr die strahlentherapie und die degro eingesetzt . 
der vorstand der degro freut sich daher mit ihm ber die groe ehrung , dankt ihm fr seine wertvolle ttigkeit und gratuliert ihm von herzen . michael baumann prsident der degro peter kneschaurek wurde am 20 . 
die gesellschaft wrdigte damit seine langjhrigen verdienste um die sterreichische radio - onkologie , insbesondere in anerkennung seiner tatkrftigen untersttzung durch zahlreiche hochklassige beitrge bei den alpbacher und sdsteirischen symposien sowie den kongressen der icro - gro . 
 die fachgesellschaften von strahlentherapie und onkologie gratulieren zum geburtstag : 11.12.2013 hannover : ulla tausch - elberskirsch 65 jahre 20.12.2013 amberg : werner berberich , 65 jahre 31.12.2013 duisburg : gerhard schneider , 65 jahre 09.12.2013 veltem - beisem : germaine heeren 75 jahre 39 . 
erlanger weiterbildungsveranstaltung degro - kurs im rahmen der weiterbildung zum arzt fr strahlentherapie erlangen , 14.15.03.2014 themenschwerpunkte : simultane radiochemotherapie therapie mit antikrpern und small molecules leitung der veranstaltung : r . 
27 , 91054 erlangen telefon + + 49 ( 0 ) 9131 85 - 33968 , fax - 33996 st - studiensekretariat@uk - erlangen.de cme - zertifizierung durch die bayerische landesrztekammer beantragt preisverleihungen die jhrlichen gro - preise werden an heimische forscher fr die bestbewerten journalpublikationen fr die kategorien klinische radio - onkologie sowie medizinphysik ausgelobt . 
die preistrger 2013 und ihre prmierten arbeiten lauten wie folgt : medizinphysik 1.preis : steininger p , neuner m , weichenberger h , et al ( 2012 ) automasked 2d / 3d image registration and its validation with clinical cone - beam computed tomography . 
 an vier tagen informieren sich auf diesem grten und wichtigsten deutschsprachigen kongress zur krebsdiagnostik und krebstherapie rund 10.000 experten ber die jngsten entwicklungen und diskutieren die aufgaben von heute und morgen kompakt , intensiv , interdisziplinr und im direkten gesprch von mensch zu mensch . 
die gebndelte kompetenz der beiden organisationen ermglicht es , den dkk thematisch und organisatorisch weiterzuentwickeln . worum es geht : innovationen , inter disziplinaritt , individualisierung drei wesentliche herausforderungen , mit denen sich die krebsmedizin derzeit beschftigt , sind bei der programmplanung im mittelpunkt : verstrkte frderung von interdisziplinaritt , zgige integration und finanzierung von innovationen und zunehmende individualisierung von therapieentscheidungen nach einer molekular - genetischen diagnostik . 
ein thema , das dabei ebenfalls diskutiert werden soll , betrifft die forschung : wie kann man knftig in deutschland eine starke und innovative krebsforschung finanziell und organisatorisch sichern ? zum anderen widmet sich der kongress dem groen thema der optimalen versorgungsqualitt durch leitlinien , zertifizierungen und krebsregister . 
wie entwickelt man die qualittssicherung weiter und gestaltet zugleich die dokumentation effizient und effektiv ? der weg dorthin soll auf dem kongress diskutiert werden . neben dem wissenschaftlichen programm befasst sich der dkk mit gesundheitspolitischen themen . 
in vielen handlungsfeldern wurden bereits ergebnisse erzielt , viele fragen sind aber noch offen , beispielsweise in der psychoonkologie : versorgungsangebote existieren aber wie kommt man zu bedarfsgerechten , einheitlichen versorgungsstandards und einer nachhaltigen finanzierung ? interdisziplinr auch im format : fachbergreifende sitzungen diese und andere politische und wissenschaftliche themen sollen auf dem krebskongress diskutiert werden . 
besonderer wert liegt auf der interdisziplinren zusammensetzung aller diskussionsformate : operateure , strahlentherapeuten und internisten sowie psychoonkologen , palliativmediziner und alle anderen , die an der versorgung des patienten beteiligt sind , werden auf dem dkk 2014 nicht in getrennten sitzungen diskutieren , sondern gemeinsa im besonderen fokus : der klinische nachwuchs dass der dkk 2014 erneut auf groes interesse stt , zeigt die zahl der eingereichten abstracts : 443 . 
der kongress untersttzt dessen begeisterung fr die onkologie : durch eine besondere wrdigung von guten abstracts , durch vielfltige mglichkeiten zur prsentation und zu freien vortrgen oder durch eine innovativ gestaltete postersitzung . 
dann stehen mediziner , fachgesellschaften , vertreter der pflege , selbsthilfegruppen und patientenorganisationen fr gesprche bereit . alle informationen , das vorprogramm und die onlineanmeldung gibt es auf der offiziellen webseite wer sich in krzester zeit auf den neuesten wissenschaftlichen und gesundheitspolitischen stand bringen mchte , der muss zum dkk 2014 kommen . 
aber noch wichtiger als information ist aus meiner sicht der diskurs : lassen sie uns die gelegenheit nutzen , die sich an vier tagen bietet , um ber die brennenden fragen in der onkologie zu diskutieren . 
several significant prognostic factors have already been identified , and several prognostic scores already exist for patients with brain metastasis [ 3 , 8 , 12 , 17 ]  . 
the most relevant prognostic factors that have also been included in most scores are the patients performance status , age , and extracranial metastases . regarding extracranial metastases , the prognostic scores have included only the options yes or no . 
1 patient characteristics ( n = 1146 ) wbrtregimen 20 gy in 5 fractions 30 gy in 10 fractions < 65 years 65 years gender female male karnofskyperformancescore kps < 70 kps 70 primarytumortype breast cancer non - small cell lung cancer small cell lung cancer other tumors numberofbrainmetastases intervalfromcancerdiagnosis towbrt 6 months > 6 months numberofinvolvedextracranialorgans wbrt whole brain radiotherapy . patients n ( % ) 393 ( 34 ) 753 ( 66 ) 669 ( 58 ) 477 ( 42 ) 555 ( 48 ) 591 ( 52 ) 504 ( 44 ) 642 ( 56 ) 196 ( 17 ) 472 ( 41 ) 155 ( 14 ) 323 ( 28 ) 343 ( 30 ) 803 ( 70 ) 573 ( 50 ) 573 ( 50 ) 418 ( 36 ) 358 ( 31 ) 258 ( 23 ) 91 ( 8 ) 21 ( 2 ) 1998 and 2012 were retrospectively analyzed with respect to potential prognostic factors for survival . 
the patient characteristics of the entire cohort are summarized in .tab.1. the univariate analyses of survival were performed with the kaplanmeier method and the log - rank test [ 4 ]  . 
those factors that were found to be significant in the univariate analysis were additionally evaluated in a multivariate analysis ( cox hazards proportional model )  . in addition to the analysis of the entire cohort of 1146 patients , separate univariate and multivariate analyses of the 728 with extracranial metastases were performed to assure that a significant result regarding the number of involved extracranial organs was not solely due to the difference between those with versus without extracranial metastases . in further subgroup analyses of the patients with involvement of one ( n = 358 ) and two ( n = 258 ) extracranial organs , the potential impact of the type of the involved extracranial organ ( s ) was evaluated . 
in those patients with involvement of one extracranial organ , the three most common lesions ( n30 ) , i.e. , lung metastasis ( n = 153 ) , bone metastasis ( n = 82 ) and liver metastasis ( n = 48 ) , and other metastasis ( n = 75 ) were compared . 
in patients treated with palliative intent such as those with brain metastasis , the survival prognosis plays an important role in optimally tailoring the treatment approach to the patients needs [ 13 ]  . 
several prognostic factors have been established for these patients including age , performance status , number of brain metastases , interval from first diagnosis of cancer until treatment of the brain metastases , and extracranial metastases [ 3 , 8 , 12 , 17 ]  . 
 [ 3 ] presented the recursive partitioning analysis ( rpa ) classification that included patients from three rtog trials ( rtog 79 - 16 , rtog 85 - 28 , rtog 89 - 05 ) [ 6 , 9 , 15 ]  . 
rpa class 1 strahlentherapieundonkologie122013 | original article abstract zusammenfassung patients have a kps 70 , age < 65 years , and controlled extracranial disease , rpa class 2 patients have a kps 70 , and at least one unfavorable prognostic factor , and rpa class 3 includes all patients with a kps < 70 [ 3 ]  . 
this score was recently validated [ 2 ]  . the prognostic factor extracranial metastases has been considered in all three scoring systems [ 2 , 3 , 12 , 17 ]  . 
in addition to the number of involved extra cranial organs , seven potential prognostic factors were investigated including wbrt regimen , age , gender , karnofsky performance score ( kps ) , primary tumor type , number of brain metastases , and the interval from cancer diagnosis to wbrt . 
 according to the multivariate analysis , age ( p < 0.001 ) , gender ( p = 0.002 ) , and kps ( p < 0.001 ) were also independent prognostic factors for survival . 
 the number of involved extracranial organs should be considered in future trials designed for patients with brain metastasis . keywords neoplasm metastasis whole - brain radiotherapy number of involved extracranial organs prognosis survival hirnmetastasen . 
 zustzlich zu der anzahl befallener extrakranieller organe wurden 7 weitere faktoren untersucht : wbrt - regime , alter , geschlecht , karnofsky - performance - score ( kps ) , art des primrtumors , anzahl der hirnmetastasen und intervall von der erstdiagnose der tumorerkrankung bis zur wbrt . 
die berlebensraten nach 6 monaten bei befall von 0 , 1 , 2 , 3 und 4 extrakraniellen organen betrugen jeweils 51 , 30 , 16 , 13 und 10% ( p < 0 , 001 )  . 
in der multivariaten analyse blieb die anzahl der befallenen extrakraniellen organe signifikant ( risk ratio 1 , 26 ; 95% - konfidenzintervall 1 , 18 1 , 34 ; p < 0 , 001 )  . 
gem der multivarianzanalyse waren auch alter ( p < 0 , 001 ) , geschlecht ( p = 0 , 002 ) und kps ( p < 0 , 001 ) unabhngige prognosefaktoren fr das berleben . 
die anzahl befallener extrakranieller organe sollte bei zuknftigen studien von patienten mit hirnmetastasen bercksichtigt werden . schlsselwrter krebsmetastasen ganzhirnbestrahlung anzahl befallener extrakranieller organe prognose berleben independent prognostic factor in patients with brain metastasis , which has not been previously demonstrated . 
for example , metastatic sites may have been missed due to incomplete documentation of the metastatic lesions in the patient files , particularly in those patients with a very poor estimated survival time . in addition to the number of involved extracranial organs , improved survival was significantly associated with younger age , female gender , and a better performance status . 
age , performance status , and the number of brain metastases have been previously identified as independent prognostic factors of survival in patients with brain metastasis [ 3 , 8 , 12 , 17 ]  . 
female gender has not yet been recognized as such but is known to be positively associated with survival in patients with other tumors such as lung cancer [ 10 , 16 ]  . 
3 comparison of the types of extracranial organs in patients with involvement of one and two extracranial organs with respect to the survival rates at 6 months and at 12 months has led to improved intracerebral control and survival in patients with a favorable survival prognosis and since previous data have suggested that 20 gy in 5 fractions was equally effective as 30 gy in 10 fractions , only patients who received 20 gy in 5 fractions or 30 gy in 10 fractions were included in this study . 
the selection of this inclusion / exclusion criterion has been supported by the fact that in the present study , the wbrt regimen had no significant impact on survival . the present study found that the number of involved extracranial organs is an strahlentherapieundonkologie122013 | 7 . 
murray kj , scott c , greenberg hm et al ( 1997 ) a randomized phase iii study of accelerated hyperfractionation versus standard in patients with unresected brain metastases : a report of the radiation therapy oncology group ( rtog ) 9104 . 
nieder c , andratschke nh , geinitz h et al ( 2012 ) use of the graded prognostic assessment ( gpa ) score in patients with brain metastases from primary tumours not represented in the diagnosisspecific gpa studies . 
phillips tl , scott cb , leibel sa et al ( 1995 ) results of a randomized comparison of radiotherapy and bromodeoxyuridine with radiotherapy alone for brain metastases : report of rtog trial 89 - 05 . 
rades d , bohlen g , dunst j et al ( 2008 ) comparison of short - course versus long - course wholebrain radiotherapy in the treatment of brain metastases . 
rades d , dunst j , schild se ( 2008 ) a new scoring system to predicting the survival of patients treated with whole - brain radiotherapy for brain metastases . 
rades d , kter jd , gliemroth j et al ( 2012 ) resection plus whole - brain irradiation versus resection plus whole - brain irradiation plus boost for the treatment of single brain metastasis . 
rades d , panzner a , dziggel l et al ( 2012 ) dose - escalation of whole - brain radiotherapy for brain metastasis in patients with a favorable survival prognosis . 
shimada y , saji h , yoshida k et al ( 2013 ) prognostic factors and the significance of treatment after recurrence in completely resected stage i non - small cell lung cancer . 
sperduto pw , berkey b , gaspar le et al ( 2008 ) a new prognostic index and comparison to three other indices for patients with brain metastases : an analysis of 1 , 960 patients in the rtog database . 
schild state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . literaturkommentiert strahlenther onkol 2013 189 : 10541055 doi 10.1007 / s00066 - 013 - 0447 - 6 online publiziert : 27 . 
oktober 2013 springer - verlag berlin heidelberg 2013 m.d.piroth klinik fr radioonkologie und strahlentherapie , universittsklinikum rwth aachen risikenungnstiger kosmetikundtoxizittnach perkutanerakzelerierter teilbrustbestrahlung ( apbi ) interimsanalysederkanadischen rapid - studie originalbeitrag olivotto ia , whelan tj , parpia s et al ( 2013 ) interim cosmetic and toxicity results from rapid : a randomized trial of accelerated partial breast irradiation using three - dimensional conformal external beam radiation therapy . 
randomisiert wurde eine wbi mit 42 , 5 gy in 16 fraktionen ( 82% der flle ) oder mit 50 gy in 25 fraktionen gegen eine pbi mit 38 , 5 gy , eingestrahlt in 10 fraktionen 2 - mal tglich . 
das klinische zielvolumen ( ctv ) basierte auf der resektionshhle und / oder clipmarkierungen plus einen sicherheitssaum von 1 cdas planungszielvolumen ( ptv ) entsprach dem ctv plus 1 ceine regelmige beurteilung erfolgte durch die patientinnen selber sowie zustzlich durch speziell geschulte study nurses und rzte anhand des cosmetic rating system for breast cancer der eortc ( european organisation for research and treatment of cancer , [ 1 ] ) und des breast cancer questionnaire [ 8 , 10 ]  . 
die kliniker wie auch die patienten sollten aufgrund der dargestellten kosmetischen und toxizittsergebnisse gewarnt sein und die perkutane 3d - crt - apbi nicht auerhalb von kontrollierten studien anwenden . kommentar die von olivotto et al . 
 [ 9 ] prsentierten ergebnisse der rapid - studie sind wichtig , da dies der erste randomisierte vergleich von kosmetik und toxizitt zwischen einer 3d - crt - apbi und der wbi ist . 
allerdings stellen die ergebnisse zur kosmetik und toxizitt keine wirkliche berraschung dar , da die verordnete dosis von 38 , 5 gy bei einzeldosen von 3 , 8 gy , 2 - mal tglich appliziert , unter radiobiologischen gesichtspunkten als zu hoch anzusehen ist . 
auf der basis des lq - modells ( / = 3 , 4 ) lge die quieffektive dosis ( eqd2 ) fr das experimentelle schema , bezogen auf eine normfraktionierte , also einmal tglich mit einer einzeldosis von 2 gy durchgefhrte bestrahlung bei 52 gy und somit nur wenig hher als bei einer standard - wbi . 
bentzen sm , ruifrok ac , thames hd ( 1996 ) repair capacity and kinetics for human mucosa and epithelial tumors in the head and neck : clinical data on the effect of changing the time interval between multiple fractions per day in radiotherapy . 
bentzen sm , saunders mi , dische s ( 1999 ) repair halftimes estimated from observations of treatment - related morbidity after chart or conventional radiotherapy in head and neck cancer . 
guttenberger r , thames hd , ang kk ( 1992 ) is the experience with chart compatible with experimental data ? a new model of repair kinetics and computer simulations . 
jagsi r , ben - david ma , moran jm et al ( 2010 ) unacceptable cosmesis in a protocol investigating intensity - modulated radiotherapy with active breath ing control for accelerated partial - breast irradiation . 
olivotto ia , whelan tj , parpia s et al ( 2013 ) interim cosmetic and toxicity results from rapid : a randomized trial of accelerated partial breast irradiation using three - dimensional conformal external beam radiation therapy . 
whelan t , mackenzie r , julian j et al ( 2002 ) randomized trial of breast irradiation schedules after lumpectomy for women with lymph node - negative breast cancer . 
intensity - modulated radiotherapy ( imrt ) has allowed a reduction of dose to the spinal cord during treatment of head and neck ( h&n ) cancer [ 7 ] , but raised several issues . 
 preclinical studies have shown that in the presence of inhomogeneous dose distributions , the spinal cord tolerance of relatively small volumes is strongly affected by low - dose irradiation of adjacent tissue [ 1 , 2 ]  . 
in order to correlate this information to the possible toxicities in cervical spinal cord of humans , we need to exactly locate the actual delivered dose in h&n cancer patients . in a previous study , we analyzed whether daily igrt is necessary in h&n helical tomotherapy [ 3 ]  . 
the aim of this study was to quantify and localize the changes in the actual delivered dose to the spinal cord , relative to the planned dose , during daily igrt and to find predictive measurements that would allow an estimation of the actual delivered dose . methods and materials patient characteristics we retrospectively analyzed 20 h&n cancer patients treated with helical tomotherapy ( ht ; accuray incorporated , sunnyvale , ca , usa ) : 10 nasopharynx cancer patients ( definitive radiotherapy ) and 10 tonsil cancer patients ( postoperative radiotherapy )  . 
sixteen patients underwent concomitant platinum - based chemoradiotherapy . treatment planning and delivery all patients underwent bilateral nodal radiotherapy ( including the supraclavicular nodes ) five fractions per week , with a boost to the high - risk regions ( tumor and involved lymph nodes regions plus safety margins )  . 
the prescribed dose to the planning tumor volume ( ptv ) was 50 gy ( 2 gy / day ) , followed by a boost up to 64 gy ( postoperative case ) or 70 gy ( definitive case )  . 
two patients were treated definitively with a simultaneous integrated boost ( sib ) concept ( 1.8 gy / day up to 59.4 gy to bilateral lymph nodes regions , 2.12 gy / day up to 70 gy to the high - risk regions ) and 1 patient was treated with 3 gy / day up to 48 gy . 
except the last patient , all patients were treated with curative intent . we previously described the treatment planning and delivery of helical tomotherapy for h&n patients treated in our clinic [ 3 ]  . 
the dose constraint for the myelon was set to 35 gy maximum dose ( dmax ) and to 45 gy dmax for the myelon plus 5 mm margin ( additional structure )  . 
1 9 contouring on the planning kvct and mvct of the myelon and schematic drawing of the analyzed quadrants [ anterior right ( ar ) , anterior left ( al ) , posterior right ( pr ) , and posterior left ( pl ) ]  . 
the first three measurements assessed the distance between the treatment table and the posterior part of the dens axis ( m1 ) , the mandibula ( m2 ) , and c4 ( m3 )  . 
we perform regular measurements at the tomotherapy unit and if necessary refresh our ct to density tables [ 5 ]  . for the initial plan , we assessed on the planning ct the maximum dose to the myelon ( plan - dmax ) and its location ( by ct slice number and quadrant , see below )  . 
we assessed for each mvct the actual delivered dmax ( a - dmax ) and the ct slices and the quadrants [ anterior right ( ar ) , anterior left ( al ) , posterior right ( pr ) , posterior left ( pl ) ; .fig.1 ] of strahlentherapieundonkologie122013 | 1027 original article abstract zusammenfassung the myelon which received a higher dose than the plan - dmax . it was hypothesized that changes of the spinal canal curvature ( see measurements m13 in .fig.2 ) and / or soft tissue changes ( measurements m46 in .fig. 2 ) would correlate to the actual delivered dose . 
the lmm approach properly considers the issue of correlated data which would lead to overly optimistic results ( too small standard errors and confidence intervals ) by applying conventional inference approaches such as student t - test or linear regression . 
this could be helpful in assessing whether replanning is necessary in patients with doses close to the known tolerance doses of the spinal cord . keywords image - guided radiotherapy head and neck neoplasms helical tomotherapy intensitymodulated radiotherapy megavoltage ct lokalisation und quantifizierung der applizierten dosis im rckenmark . 
vor allem bei patienten mit einer rckenmarksdosis nahe an der toleranz dosis ist dies fr die entscheidung bezglich einer umplanung hilfreich . schlsselwrter bildgesteuerte strahlentherapie kopfhals - tumor helikale tomotherapie intensittsmodulierte strahlentherapie megavolt - ct gether is depicted in .tab.1. 
the median change in a - dmax was + 0.16%. considering each patient separately , a trend toward consistently showing either a higher or lower a - dmax relative to plandmax was observed in 15 out of 20 patients . 
the difference between the average a - dmax change of the first 3 analyzed fractions and the average a - dmax change of the other 9 fractions was 1.82.7% for the patients with an increase in a - dmax and 0.50.4% for the patients with a decreased a - dmax , respectively . for the remaining 5 patients , the a - dmax was increased or decreased for the half of the fractions each . 
however , most a - dmax values were located in different quadrants than the plan - dmax . the absolute average changes of the spinal canal curvature ( m13 ) and of soft tissue ( m46 ) were : m1 0.240.86 cm ; m2 0.240.23 cm ; m3 0.290.27 cm ; m4 0.560.43 cm ; m5 0.230.21 cm ; m6 0.220.23 cthere were no statistically significant changes in time of any of the analyzed parameters . 
the variance in m1m6 distances did not correlate to the dmax changes ( rho < 0.20 for all parameters )  . discussion in a previous paper we demonstrated that by performing daily igrtas compared to twice - weekly or once - weekly igrt fewer fractions are associated with a change in delivered dose from planned , smaller volumes of the spinal cord receive a higher dose and the increase in dmax is less . 
nevertheless , we showed that despite daily igrt , the dose to the spinal cord can significantly differ from the planned dose [ 3 ]  . limitations of the present study are the small sample size and the retrospective design . the first goal of the present study was to quantify the actual delivered maximum dose to the spinal cord during daily igrt for individual patients , as opposed to average effects across patients ( i.e. , in our study of + 0.16% median change over all fractions and patients )  . 
however , although there was a substantial interpatient variability , the intrapatient variability was small . three hypotheses to account for variations in a - dmax from plan - dmax were considered : systematic setup errors , slight changes in head position ( i.e. , a spinal canal deformation ) and / or soft tissue changes during fractionated radiotherapy could result in a systematic change in the delivered dose to the spinal cord . 
in some cases ( e.g. , for the patient with an increase of 26% ) , the quite sizable dose differences may have been due to steeper dose gradients compared to the other patients . 
in all other patients , small patient setup errors within the mask , small spinal canal deformations , and small changes in the soft tissues may have combined to produce relevant differences in spinal a - dmax from planned . the third aim of the study was to find methods to estimate the actual delivered dose . 
a recalculation of dose on the mvcts of the first treatment week could be sufficient ( with an error of approximately 2% ) to assess the magnitude of the change in delivered dose , as the intraindividual variations in the actual delivered dose are small . 
a possible approach for clinical use would be to perform dose recalculations on the daily mvcts of the first week to assess the direction of the change ( lower or higher ) in each patient , and then to adjust treatment plans . lastly , we also found that if a higher dose was revealed during daily igrt , the higher dose was mostly delivered to the anterior quadrants in the same ct slices . 
 [ 1 , 2 ] demonstrated a high tolerance of small ( i.e. , 2 mm ) shower regions of the spinal cord to irradiation , but that tolerance decreases significantly if the region is surrounded by low - dose bath irradiation . 
there is also a lack of clinical data in humans concernstrahlentherapieundonkologie122013 | 1029 original article anterior right anterior left occurence all fractions more than 50% of the fractions less than 50% of fractions 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 patient number 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 patient number posterior right posterior left 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 patient number 1 2 3 4 5 6 7 8 9 1011 12 13 14 15 16 17 18 19 20 patient number fig . 
 a case report of the lhermitte sign after head and neck imrt suggested a different pathophysiology ; as the dmax was situated anteriorly in this patient , the authors suggested that the lhermitte sign was caused by the irradiation of the anterior spinothalamic tract ( involved in the perception of simple touch , pain , and temperature ) [ 8 ]  . 
 [ 9 ] demonstrated a higher rate ( 21% of the analyzed patients ) of lhermitte sign in patients receiving chemo - imrt , with a clear dose volume effect showing the lhermitte sign to be more likely at cord volumes receiving 40 gy . 
pak d , vineberg k , feng f et al ( 2012 ) lhermitte sign after chemo - imrt of head - and - neck cancer : incidence , doses , and potential mechanisms . 
luijk p van , bijl hp , coppes rp et al ( 2001 ) techniques for precision irradiation of the lateral half of the rat cervical spinal cord using 150 mev protons [ corrected ]  . 
welsh js , lock m , harari pm et al ( 2006 ) clinical implementation of adaptive helical tomotherapy : a unique approach to image - guided intensity modulated radiotherapy . 
kampfer state that there are no conflicts of interest . literaturkommentiert literaturkommentiert strahlenther onkol 2013 189 : 10561057 doi 10.1007 / s00066 - 013 - 0475 - 2 online publiziert : 27 . 
oktober 2013 springer - verlag berlin heidelberg 2013 a.dalprad.m.aebersold universittsklinik fr radio - onkologie , inselspital , universitt bern radiotherapiemitrechtwinkligen feldernimvergleichzu konformalenfeldern wenigertherapieversagerbei hochrisiko - prostatakarzinompatienten originalbeitrag heemsbergen wd , al - mamgani a , witte mg et al ( 2013 ) radiotherapy with rectangular fields is associated with fewer clinical failures than conformal fields in the high - risk prostate cancer subgroup : results from a randomized trial . 
es wurden 164 hochrisiko - patienten aus einer studienpopulation von 266 patienten mit den tumorstadien t14 n0 m0 ausgewhlt , welche randomisiert in einem arm eine rechtwinklige bestrahlung ( n = 79 ) und im anderen arm eine konformale bestrahlung erhielten . 
ein therapieversagen kann mglicherweise dadurch vermindert werden , dass man regionen mit einem vermuteten subklinischen tumorbefall auerhalb der prostata mitbestrahlt . kommentar die autoren adressieren in dieser studie das thema des optimalen bestrahlungsvolumens bei patienten mit einem hochrisiko - prostatakarzinoaus der anatomischen perspektive sind dabei zwei erklrungen der resultate mglich : effekte durch die bestrahlung des periprostatischen gewebes und die rolle der prophylaktischen lymphknotenbestrahlung . die image - guided radiotherapie ( igrt ) erlaubt durch den einsatz der bildgebung am linearbeschleuniger die erfassung und korrektur von positionsabweichungen der prostata und damit die verkleinerung von sicherheitssumen fr die ptv - definition . 
 [ 2 ] eine erhhte rate an biochemischem versagen bei patienten , welche eine markerbasierte igrt erhielten , im vergleich zu patienten , deren positionierung aufgrund der knchernen strukturen erfolgte . der in der hier kommentierten studie berichtete negative effekt einer konformalen bestrahlung knnte auch durch die verminderte dosisbelastung von okkulten lymphknotenmetastasen bei diesem hochrisiko - patientenkollektiv erklrt werden . 
heemsbergen wd , al - mamgani a , witte mg et al ( 2013 ) radiotherapy with rectangular fields is associated with fewer clinical failures than conformal fields in the high - risk prostate cancer subgroup : results from a randomized trial . 
engels b , soete g , verellen d et al ( 2009 ) conformal arc radiotherapy for prostate cancer : increased biochemical failure in patients with distended rectum on the planning computed tomogram despite image guidance by implanted markers . 
morikawa lk , roach m 3rd ( 2011 ) pelvic nodal radiotherapy in patients with unfavorable intermediate and high - risk prostate cancer : evidence , rationale , and future directions . 
die laufende phase - iii - studie 0924 der rtog wird hoffentlich in dieser frage eine antwort bringen . heutzutage gilt fr bestrahlte patienten mit einem hochrisiko - prostatakarzinom eine radiotherapie , kombiniert mit einer hormontherapie , als standard [ 4 ]  . 
es darf wohl davon ausgegangen werden , dass die beobachteten unterschiede der metastasierung zwischen den beiden armen nicht aufgetreten wren , htten die patienten eine nach heutigem standard ausgerichtete kombinationstherapie erhalten jedenfalls nicht innerhalb von nur 34 monaten . so interessant die von den autoren adressierten fragen auch sind , so schwach sind die fe , auf denen die antworten stehen . 
 kommt hinzu , dass in abwesenheit einer stratifikation fr bekannte risikofaktoren relevante ungleichgewichte in der patientenverteilung auszumachen waren ungleichgewichte , die wohl alleine die berichteten unterschiede zwischen den beiden therapiearmen zu erklren vermgen . 
porru department of radio - oncology , regional oncological hospital , via jenner , 09121 cagliari , italy erratum to : bi - tangential hybrid imrt for sparing the shoulder in whole breast irradiation the authors and the publishing editor regret a typing error in the list of authors in strahlentherapie und onkologie 189 : 967 - 971 . the correction in the list of authors is shown in italics : p . 
farace department of radio - oncology , regional oncological hospital , via jenner , 09121 cagliari italy paolofarace@gmail.com 1060 | strahlentherapie und onkologie 12 2013 the online version of the original article can be found at s00066 - 013 - 0428 - 9 editorial strahlenther onkol 2013 189 : 993995 doi 10.1007 / s00066 - 013 - 0459 - 2 received : 15 august 2013 accepted : 11 september 2013 published online : 2 . 
november 2013 springer - verlag berlin heidelberg 2013 r.fietkau1f.putz1g.lahmer1s.semrau1r.buslei2 1 klinik fr strahlentherapie , erlangen 2 neuropathologisches institut des universittsklinikums erlangen und des ccc erlangen canmgmtpromotermethylation statusbeusedasaprognosticand predictivemarkerforglioblastoma multiformeatthepresenttime ? awordofcaution editorial several studies have addressed the prognostic and predictive value of the methylation status of the o6 - methylguaninedna methyltransferase ( mgmt ) gene in patients with glioblastoma multiforme ( gbm )  . 
however , these initial results were partly offset by the results of a five - year analysis published by the same group at a later date [ 8 ]  . 
conversely , mgmt promoter methylation status had no impact among patients treated with radiotherapy alone . consequently , there are now frequent demands for the routine use of mgmt promoter methylation as a predictive and prognostic factor in clinical practice . 
for individuals over 65 years of age , this means that temozolomide chemotherapy alone should be administered in patients with a methylated mgmt promoter and radiotherapy alone in those with an unmethylated mgmt promoter . 
nowadays , more and more studies are being designed for the exclusive inclusion of patients with a specific mgmt status ( compare the centric , ceteg and glarius studies )  . 
 this assumes a widespread availability of standardized , reliable and validated methods for the determination of mgmt promoter methylation status . however , we would like to point out that there are still many uncertainties associated with the practical implementation of mgmt promoter methylation analysis . 
our opinion is supported by a recent review published by berghoff and colleagues in austria [ 1 ]  . what are the current arguments against the routine use of mgmt promoter methylation status in clinical practice ? f various methods for the determination of mgmt promoter methylation status have been developed and are currently available . 
demand a scientific analysis of the reproducibility of these tests , statingthis lack of evidence impedes recommendation of mgmt testing for routine clinical use [ 1 ]  . f the mgmt gene promoter contains a total of 97 potential cpg methylation sites . 
in our opinion , it is therefore problematic to transfer the significance of the mgmt status as defined in the aforementioned studies to alternative methods or different methylation sites in an uncritical manner . 
in the noa08 study , for example , only those tissue samples with a tumor cell content of at least 80% were accepted for analy sis [ 11 ]  . 
this means that , in clinical practice , the mgmt promoter methylation status cannot be determined in a significant proportion of patients due to a lack of suitable sample material . f in the eortc - 26981 - 22981 / ncicce3 study [ 9 ] , the addition of temozolomide to radiotherapy resulted in a small , yet statistically significant survival benefit for gbm patients with an unmethylated mgmt status . 
 [ 5 ] provided evidence demonstrating the predictive value of mgmt status in elderly patients treated with temozolomide alone , whereas the effect of radiotherapy was independent of the mgmt status . 
 f it is unclear which method and which tumor material should or could be used . f it is unclear which methylation sites allow a reliable predictive and / or prognostic assessment . f there are still too few independent studies on the prognostic and predictive value of mgmt promoter gene methylation to permit its use in treatment decisions relating to the use of combined radiotherapy and chemotherapy in elderly gbm patients . therefore , it is imperative that well - defined and reproducible conditions for the determination of mgmt promoter methylation status are established prior to the introduction of mgmt status in routine diagnostics and daily clinical practice ( e.g. , when making treatment decisions for older gbm patients )  . 
 from a radio - oncological perspective , it is necessary to clearly identify the treatment regimens ( e.g. , combined radiotherapy and chemotherapy ) in which mgmt status is really significant . we are confident that mgmt status can play an important role in individualized treatment planning for gbm in the future . 
buslei state that there are no conflicts of interest . literatur kommentiert strahlenther onkol 2013 189 : 10581059 doi 10.1007 / s00066 - 013 - 0476 - 1 online publiziert : 27 . 
die zweite gruppe erhielt 13 zyklen induktionschemotherapie ( cisplatin 100 mg / m2 an tag 1 und 5 - fu 1000 mg / m2 an den tagen 15 ) , gefolgt von einer radiotherapie im fall einer kompletten remission oder einer operation im falle eines tumorresiduums . 
das 10 - jahres - gesamtberleben betrug 13 , 8% fr die chirurgische gruppe und 13 , 1% fr die chemotherapiegruppe , das progressionsfreie berleben dagegen 8 , 5 und 10 , 8% . 
die organerhaltende strategie ermglichte den larynxerhalt in mehr als der hlfte der berlebenden patienten mit vergleichbaren berlebensund tumorkontrollraten , welche aber schlecht blieben . kommentar diese studie behandelt ein sehr wichtiges und komplexes thema der kopfhals - onkologie , nmlich die mgliche verbesserung der onkologischen ergebnisse bei gleichzeitigem funktionserhalt . 
sowohl die operativen als auch die konservativen therapieverfahren zur behandlung von larynxund hypopharynxkarzinomen haben sich in den letzten jahrzehnten weiterentwickelt mit dem ziel , beides zu ermglichen . die arbeitsgruppe von lefebvre hat nun eine zweite publikation mit den langzeitergebnissen aus der prospektiven eortc - 24891 - studie vorgelegt [ 1 ]  . 
dabei konnten fr beide studienarme vergleichbare , aber doch insgesamt schlechte onkologische ergebnisse identifiziert werden : in der gruppe mit induktionschemotherapie hatten nach 10 jahren nur 8 , 7% der patienten einen funktionierenden larynx . 
und in der gruppe mit intendiertem organerhalt erzielt die primre simultane radiochemotherapie ebenfalls bessere onkologische ergebnisse als die sequenzielle chemoradiotherapie [ 2 ]  . zustzlich haben eine reihe von weiterentwicklungen sowohl die konservativen als auch die operativen verfahren deutlich verndert . 
bei lokal umschriebenen tumoren hat die entwicklung von neuen operativen techniken , wie die trans orale mikrolaryngoskopische laserchirurgie ( tlm ) und die transorale roboterassistierte chirurgie ( tors ) , eine weitere reduktion des operativen traumas und der morbiditt bei gleichwertigen onkologischen ergebnissen ermglicht [ 3 ]  . 
lefebvre j - l , andry g , chevalier d et al ( 2012 ) laryngeal preservation with induction chemotherapy for hypopharyngeal squamous cell carcinoma : 10 - year results of eortc trial 24891 . 
pignon jp , le matre a , maillard e et al ( 2009 ) metaanalysis of chemotherapy in head and neck cancer ( mach - nc ) : an update on 93 randomised trials and 17 , 346 patients . 
semrau s , schmidt d , lell m et al ( 2013 ) results of chemoselection with short induction chemotherapy followed by chemoradiation or surgery in the treatment of functionally inoperable carcinomas of the pharynx and larynx . 
oral oncol 49 : 454460 die in der rubrik literatur kommentiert seit 2010 erschienenen beitrge sind online verfgbar unter taten eine deutlich bessere defektdeckung nach ausgedehnten resektionen und eine verbesserung der funktionellen ergebnisse . 
im bereich der radiotherapie hat die entwicklung der imrt ( intensittsmodulierte radiotherapie ) die strahlenbedingte morbiditt deutlich reduzieren knnen , ebenfalls mit gleichwertigen onkologischen ergebnissen . aber auch die induktionschemotherapie entwickelte sich in den letzten jahren zu einer sehr interessanten therapiemglichkeit . 
 acute and late toxicity following conventional photon irradiation are well documented and often constitute dose - limiting factors [ 4 , 17 , 18 , 26 , 30 ]  . 
these authors estimated a tolerance dose ( td ) 5 / 5 of 50 gy for one - third of the total sb volume ( approximately 1800 cm3 ) and a td50 / 5 of 60 gy ( same volume ) for late sb toxicities . 
 these recommendations remained largely unchallenged and have represented the world - wide established consensus for 20 years . however , radiotherapy ( rt ) techniques have developed dramatically during the past two decades , resulting in improved target dose conformity and significantly reduced radiation - induced acute and late sequelae [ 5 , 12 , 20 ]  . 
these authors recommend limiting the absolute volume of irradiated sb to < 120 cm3 for doses above 15 gy if individual bowel loops are outlined , and a reduction of the volume receiving > 45 gy to < 195 cm3 if the entire potential peritoneal space of the bowel is outlined . 
in general , there is paucity of published data concerning the effects of high - dose rt to small , possibly noncircumferential volumes of sb . multiple preclinical comparisons of proton radiation therapy ( pt ) versus modern conformal rt have suggested a reduction in integral dose to normal tissues , i.e. 
sb , by pt [ 3 , 14 , 27 ]  . this retrospective analysis of 31 patients with paraspinal or retroperitoneal tumours correlates target coverage with sb dosevolume histograms based on the initial treatment planning ct scans and clinical tolerance . 
to the best of our knowledge , this is the first evaluation of a pt - treated patient cohort that focuses on sb gastrointestinal tolerance ( gi ) tolerance . patients and methods between september 1997 and december 2008 , 31 patients were treated with highdose spot scanning - based pt at the paul scherrer institute ( psi ) center for proton therapy . 
one patient had longstanding history of crohns disease . the histological tumour diagnosis was chordoma in 81% , soft tissue sarcoma in 16% and meningioma in 3% of the patients tumours were located in the lumbar spine region ( n = 17 ) or confined to the sacrum ( n = 14 )  . 
a total of 54 surgical procedures were performed in these 31 patients prior to pt ; in 13 patients , surgery was performed using a posterior approach exclusively , in 5 patients , approach was exclusively anterior and in 13 patients , both posterior and anterior surgical approaches were used . 
patients were immobilised prone in an individual vacuum mould outside the treatment roodaily control was performed using ct scout views prior to pt to verify correct patient positioning in alignment with the planning ct . 
weekly or biweekly x - ray - based position verification following pt was also performed [ 2 ]  . in the majority of patients , fractionated pt was conducted without repeated soft tissue imaging ( ct ) and alignment was based on bony contours only . 
for the purpose of this retrospective study , the position of the sb was therefore based solely on the positioning information obtained at the time of the planning ct scan . treatment planning was based on proton beam arrangements from posterior and posterior - oblique field angles . 
there1020 | strahlentherapieundonkologie122013 statistical analysis local control ( lc ) and overall survival ( os ) rates were calculated from the pt start date using kaplanmeier estimates [ 10 ]  . 
this resulted in a mean of 87% ( range 55.599.9 ) of the ptv receiving at least 95% of the prescribed dose , whereas a mean of 93.2% of the ptv was covered by at least 90% of the prescribed dose . 
however , high - dose ptv coverage was affected by dose constraints to the following oars : kidneys , generally 30 / 23 gy ( rbe ) to 33 / 66% of the organ , respectively ; spinal cord , 6364 gy ( rbe ) to the surface and 5354 gy ( rbe ) to the centre ; cauda equine , below l4 no constraints , otherwise 70 gy ( rbe ) ; nerve roots , generally 70 gy ( rbe ) except for areas in direct contact with residual tumour . acute and late small bowel toxicity two patients ( 6% ) experienced grade 1 acute toxicity . 
1 8 the composite dose fall - off of a proton beam arrangement from 60 ( ~81% ) to 20 gy ( rbe ) ( ~28% ) at the distal target edge with a prescribed dose of 72.0 gy ( rbe ) ( 100% )  . 
the dose per fraction was standard at a value of 1.82.0 gy ( rbe )  . gross tumour volume ( gtv ) and clinical target volume ( ctv ) had been defined for each patient at the time of pt planning and delivery . 
 review of patient records revealed that organ at risk ( oar ) constraints for sb were not defined in the majority of cases ; otherwise these ranged from a maximum dose of 64 to 76 gy ( rbe )  . project based on the original planning ct scans , the treatment plans of the 31 patients were reanalysed . 
all delineations were retrospectively performed by one physician and independently verified by a second . dosimetric indices showing the sb volumes treated to doses of 5 , 20 , 30 , 40 , 50 , 60 , 70 , 75 and 80 gy ( rbe ) were calculated to give v5 , v20 , v30 , v40 , v50 , v60 , v70 , v75 and v80 values , respectively . 
 late sb toxicity was reviewed as recorded during follow - up and correlated to dosimetric parameters . toxicity analyses acute and late toxicities were defined or retrospectively redefined according to the common terminology criteria for adverse events ( ctcae ) version 4.0. 
late toxicities were evaluated by annual follow - up examinations at our institute , or alternatively , by contacting the responsible physician or individual patient by telephone and e - mail / post . abstract zusammenfassung strahlenther onkol 2013 189 : 10201025 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0432 - 0 r.a.schneiderv.vitolof.albertinit.kochc.aresa.lomaxg.goiteine.b.hug small bowel toxicity after high dose spot scanning - based proton beam therapy for paraspinal / retroperitoneal neoplasms abstract purpose . 
between 1997 and 2008 , 31 patients ( mean age 52.1 years ) underwent spot scanning - based pt for paraspinal / retroperitoneal chordomas ( 81% ) , sarcomas ( 16% ) and meningiom ( 3% )  . 
 despite target doses of > 70 gy ( rbe ) , sb received > 50 and > 60 gy ( rbe ) in only 61 and 54% of patients , respectively . 
this small retrospective study has limited statistical power but encourages further efforts with higher patient numbers to define and establish high - dose threshold models for sb toxicity in modern radiation oncology . keywords organ at risk radiation therapy follow - up chordoma sarcoma hochdosis - spot scanning basierte protonen - strahlentherapie von paraspinalen / retroperitonealen tumoren und dnndarm - toxizitt zusammenfassung hintergrund . 
zwischen 1997 und 2008 erhielten 31 patienten ( durchschnittsalter : 52 , 1 jahre ) mit paraspinalen / retroperitonealen chordomen ( 81% ) , sarkomen ( 16% ) und einem meningeom ( 3% ) eine spot - scanning - basierte pt . 
das durchschnittlich belastete dnndarmvolumen ( cm3 ) innerhalb unterschiedlicher dosisstufen [ gy ( rbe ) ] betrug v5 ( 24 patienten ) : 86 , 5 , v20 ( 24 patien ten ) : 45 , 1 , v50 ( 19 patienten ) : 17 , 7 , v60 ( 17 patienten ) : 7 , 6 , v70 ( 12 patienten ) : 2 , 4 . 
bei entsprechend limitierter statistischer aussagekraft sollten weitergehende untersuchungen mit hheren patientenzahlen durchgefhrt werden , um hochdosisschwellen - modelle fr akute und spte dnndarmtoxizitten in moderner strahlentherapie zu definieren und zu etablieren . schlsselwrter risikoorgan strahlentherapie nachbeobachtung chordom sarkom only one patient reported grade 1 late toxicity . 
this included 18 patients with transabdominal surgical resection . the composite dose fall - off from 60 to 20 gy ( rbe ) at the distal target edge was accomplished within a maximum distance of 2 cm in this patient cohort . 
in these patients , the approximately 3 - cm distance between anterior paraspinal ptvs to the most posterior sb wall was sufficient to reduce the dose levels to below 5 gy ( rbe )  . in the remaining 24 / 31 patients ( 77% ) , the mean maximum dose ( dmax ) to sb was 64.1 gy ( rbe ) at prescribed target doses > 70 gy ( rbe )  . 
for these 24 patients , average values of calculated dosimetric indices are presented in .fig.2 ; mean values , ranges and the maximum doses to sb v75 ( 10 / 31 patients ) are given in .tab.1. 1022 | strahlentherapieundonkologie122013 250 fig . 
two patients developed grade 2 functional neuropathies ( 6.4% ) , resulting in sexual dysfunction in one patient and sphincter dysfunction in the second . other toxicities bone necrosis ( grade 3 ) was diagnosed in one patient . discussion our study raises questions about the relevance and applicability of photon - based and largely historical oar constraints for sb in pt and modern rt techniques . 
both issues are well accepted concepts for other organsspinal cord , brainstem etc . , and notably , for rectuour results indicate that sb tolerance concepts warrant further investigation and should follow more sophisticated oar concepts as already in place for other systems [ 21 , 25 ]  . 
additional contouring of bowel loops in close proximity to target volumes may help to define high - dose thresholds . due to their physical characteristics , protons have the potential to reduce both irradiated sb volumes in general and the high - dose volumes of moving loops in close proximity to the distal edge of the beasb loops with potentially significant interfractional and intrafractional variability may not receive high doses at identical locations and volumes . 
therefore , one - time deterstrahlentherapieundonkologie122013 | 1023 dose ( gy ( rbe ) ) time ( years ) non - gi - related acute and late adverse effects skin toxicity overall , treatment was well tolerated by all patients . 
non - gi - related grade 2 late adverse events were observed in 7 out of 31 patients ( 22.6% ) and 2 patients ( 6.4% ) experienced grade 3 toxicities . 
daily confirmation of bowel loop position using image - guided rt ( igrt ) could determine the true sb dose . however , this report documents that patients tolerated high - dose pt to targets in close proximity to sb exceedingly well . 
additionally , it shows that treatment plans suggested that in a large number of patients , sb received noncircumferentially higher radiation doses than presently recommended for conventional photon therapy [ 21 , 25 ]  . 
neither history of extensive transabdominal surgery nor long - standing crohns disease resulted in a higher toxicity rate in our patient cohort . the two advantages of pt , namely high - dose target coverage and increased normal tissue tolerance contribute to the favourable toxicity profile in our patient cohort . 
further investigation with a larger patient cohort should include a discussion of the risk factors [ 16 ] and expected changes in sb location associated with using prone or supine positioning for pt . in our patient cohort , all entrance fields were directed from posterior or posterioroblique , thereby ranging out into sb in many patients and all patients had doses to sb 60 gy ( rbe )  . 
it is therefore of interest that we have not observed any toxicity that could possibly be related to these issues . conclusion ourdatademonstratetheabilityofptto delivercurativedosesinexcessof70gy ( rbe ) toparaspinalandretroperitoneal tumours ( sarcomas ) withoutanyhighergradesbadverseevents.retrospective sbdosecalculationsbasedontheinitial treatmentplanningctscansof31patientsindicatedradiationdosestosmall corresponding address r.a. 
previous series have correlated poor survival with the presence of hypoxia [ 12 ] and in vitro experiments have shown that in order to elicit the same cytotoxic effects as observed in normoxic cells , radiation doses to hypoxic cells must be multiplied by a factor of three [ 14 ]  . positron - emission tomography ( pet ) with [ 18f ] - fluoromisonidazole ( fmiso ) allows a noninvasive assessment of hypoxia with spatial cartography , which allows an escalation of radiotherapy dose to hypoxic volumes to be considered . 
the prognostic value of hypoxic tracer imaging has already been demonstrated [ 17 ] and a recent publication showed a high reproducibility of tumour hypoxia as evaluated by two fmiso - pet scans acquired within a 48 - hour interval , which is a necessary requirement for dose escalation in radiotherapy [ 13 ]  . however , due to the lipophilicity of fmiso and its slow clearance from normoxic tissues , fmiso - pet images have a low contrast and their use in radiotherapy planning is complicated . 
few data are available on this subject ; one study showed recently that improved contrast was obtained with delayed acquisitions at 4 h after fmiso injection [ 1 ]  . the aims of this study were to confirm that delayed acquisitions are better for fmiso imaging in hnscc and to study different methods of volume segmentation for radiotherapy . 
 different automatic methods for segmentation of pet volumes were then tested . patients and methods patients from june 2009 to july 2012 , 15 male hnscc patients ( median age 55 years ; range 5077years ) were prospectively enrolled in a clinical trial assessing the prognostic value of fmiso imaging at the university hospital of bordeaux . 
fmiso - pet / ct data were reviewed retrospectively to study the contrast of fmiso images and to assess different automatic segmentation methods . this study was approved by the institutional review board and the french health authority . 
the fmiso volume was defined by all voxels with an activity 1.4 ab [ 3 , 7 , 11 , 17 ]  . the second was an adaptive threshold method based on rt / b . 
these ratios differed significantly from each other ( p = 0.003 ) as shown in .fig.1. comparison of automatic segmentation methods the fmiso volumes at 4 h , segmented using the three studied methods of segmentation , are summarized in .fig.2. 
 dosimetric studies have shown that dose escalation to fmiso volumes is possible with a boost of 1020 gy and is associated with improvements in the probability of tumour control [ 7 ]  . 
these early changes in fmiso images during radiotherapy could be promising for selection of the patients who would benefit from dose escalation . however , up until now few data were available concerning the definition of hypoxic volumes for radiotherapy applications . 
positron - emission tomography ( pet ) with [ 18f ] - fluoromisonidazole ( fmiso ) permits consideration of radiotherapy dose escalation to hypoxic volumes in head and neck cancers ( hnc )  . 
three automatic methods of pet image segmentation were tested : fixed threshold , adaptive threshold based on the ratio between tumour - derived and background activities ( rt / b ) and the fuzzy locally adaptive bayesian ( flab ) method . 
die positronenemissionstomographie ( pet ) mit [ 18f ] - fluoromisonidazol ( fmiso ) ermglicht in der strahlentherapie fr kopf - hals - tumore ( kht ) eine dosissteigerung auf hypoxische volumina . 
es wurden drei automatische segmentierungsmethoden von petbildern getestet : ein fester schwellen wert , ein adaptiver schwellenwert , basierend auf dem verhltnis zwischen den tumorsen und den hintergrundaktivitten ( vt / h ) , sowie die fuzzy - locally - adaptive - bayesian - ( flab - ) methode . 
our results confirm those of the latter study and show significantly improved image contrast at 4 h . an important observation in our series is the large difference between the ct and fmiso - pet volumes , irrespective of segmentation method . 
in the absence of a correlation with a histological gold standard , it is difficult to draw conclusions from these results and to the best of our knowledge , no series has yet evaluated the correlation between hypoxia imaging volumes and surgical specimens . 
a previous series , with realistically simulated cases of hnscc and lung cancer , also studied different segmentation methods ( fixed / adaptive threshold and flab method ) [ 10 ]  . 
these simulations were performed for fluorodeoxyglucose ( fdg ) pet images but with low contrast ratios ( up to 1.8 : 1 ) similar to those found in fmiso images . 
the volume errors measured in this study uing simulated pet images were smallest for the flab method , which demonstrates the superiority of this method to the fixed or adaptive threshold approaches in terms of tumour volume delineation . 
this observation suggests that for a clinical application in radiotherapy with fmiso - pet imaging , the use of the flab segmentation method is more appropriate than fixed or adaptive threshold approaches . an alternative to this problematic segmentation of fmiso volumes could be a dose escalation strategy based on dose painting by numbers ( dpbn ) [ 2 , 18 ]  . 
despite the fact that dpbn is more complex to implement in practice and requires further investigation for its clinical validation , the method seems promising ; biological reality is not white or black , hypoxia or no hypoxiathe biological reality is a gradient of microscopic phenomena and tumour cell oxygenation . moreover , despite a recent study published by okamoto et al . 
planning of dose escalations for this time - dependent vessel modification could lead to erroneous radiotherapy planning and more studies are thus needhypoxia is a dynamic phenomenon with the potential to change during radiotherapy because of radioinduced reoxygenation ; several studies with repeated fmiso - pet before and during radiotherapy found decreases in hypoxia and hypoxic subvolumes between the first and 1018 | strahlentherapieundonkologie122013 16 . 
rajendran jg , schwartz dl , osullivan j et al ( 2006 ) tumor hypoxia imaging with [ f - 18 ] fluoromisonidazole positron emission tomography in head and neck cancer . 
zips d , zphel k , abolmaali n et al ( 2012 ) exploratory prospective trial of hypoxia - specific pet imaging during radiochemotherapy in patients with locally advanced head - and - neck cancer . 
the question to answer is whether the dose escalation must be delivered to the initial hypoxic volume , or whether it must change according to the variability of hypoxic areas during radiotherapy . 
lamare state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
however , locoregional control ( lrc ) remains poor especially for tumors with intracranial extension and / or initially high local tumor burden [ 3 , 4 ] , including those with cranial nerve , infratemporal fossa , orbit , hypopharynx , or masticator space involvement , categorized as t4 disease according to the american joint commission on cancer ( ajcc ) [ 5 ]  . 
t4 disease is considered as a significant barrier to achieving successful treatment because of the proximity of a t4 tumor to critical neural structures , which prevents good radiation field coverage and necessitates dose reductions for critical organ tolerance . intensity - modulated radiation therapy ( imrt ) can achieve better dose differentiation between tumorous and normal tissues than two - dimensional or three - dimensional ( 3d ) conformal radiotherapy and facilitates simultaneous delivery of different fractional doses to different targets [ 6 , 7 ]  . 
in all stages of nonmetastatic npc , imrt has the advantage of better tumor coverage because it allows room for dose escalation , while reducing exposure to the parotid gland , temporomandibular joints , and brainstem / temporal lobe [ 7 ]  . 
 thus , imrt is expected to be beneficial for t4 npc , as a way to increase the biologic effect on the tumor by physical dose escalation or accelerated fractionation , while avoiding toxicity to critical tissues . little data specifically addresses the treatment outcome and failure patterns of t4 npc patients treated with imrt . 
the survival and feasibility of salvage treatment for locoregional recurrence after definitive imrt was analyzed to provide a reference for clinical management . materials and methods patients the study was approved by the institutional review board of our institute ( 201211028ric )  . 
subsite localization of the nasopharynx tumor was categorized according to the 6th edition of the ajcc staging criteria [ 5 ] as intracranial extension , cranial nerve involvement , infratemporal fossa involvement , hypopharynx involvement , orbit involvement , or masticator space involvement . 
staging evaluations included magnetic resonance imaging ( mri ) of the nasopharynx and neck , chest radiography , liver sonography , bone scintigraphy , and positron emission tomography ( pet ) / computed tomography ( ct ) , if clinically required . radiotherapy the imrt treatment technique has been previously described [ 6 ]  . 
the target areas received three dose levels with simultaneous integrated boosts ( sibs ) , in accordance with the rtog 0225 protocol [ 1 ] : clinical target volume ( ctv ) - 70 ( 70 gy to the nasopharyngeal gross tumor and lymphadenopathy ) ; ctv - 63 / 60 ( 6063 gy to the subclinical disease and high - risk lymphatic regions , including the entire nasopharynx , retropharyngeal nodal regions , skull base , clivus , pterygoid fossae , parapharyngeal space , sphenoid sinus , and the posterior nasal cavity / maxillary sinuses that includes the pterygopalatine fossa and upper middle neck regions ) ; presented in part at the 54th annual meeting of the american society of radiation oncology ( astro ) , 2831 october 2012 , boston , ma , usa . strahlentherapieundonkologie122013 | 1001 original article tab . 
the planning target volumes ( ptvs ) were evenly expanded using a 4 - mm marg two dose fractionations ( 33 or 35 fractions ) were used , depending on the treat1002 | strahlentherapieundonkologie122013 tab . 
the ptv - 70 , 63 , and 56 received 70 gy at 2 gy per fraction , 63 gy at 1.8 gy per fraction , and 56 gy at 1.6 gy per fractions in 35 fractions , respectively , and the ptv - 70 , 60 , and 54 received 70 gy at 2.12 gy per fraction , 60 gy at 1.82 gy per fraction , and 56 gy at 1.64 gy per fractions in 33 fractions , respectively . the treatment goals were as follows : 100% of the radiation dose should cover 95% of the ptv and the maximum dose should not exceed 110% . 
to avoid imminent overdose to critical structures , this goal could be modified to 95% of the radiation dose should cover 95% of ptv and the maximum dose should be less than 115% . 
the maximum doses to the brain stem , optic nerves / chiasm , eyes and spinal cord were set as 60 , 54 , 50 , and 45 gy , respectively . 
the plans were optimized using the inverse planning algorithm ( direct machine parameter optimization ) and heterogeneity corrections . the imrt was delivered using an elekta synergy accelerator ( elekta , stockholm , sweden ) with a step - and - shoot technique . 
neoadjuvant chemotherapy was given at the discretion of the chemo - oncologist , mainly for patients with obvious intracranial invasion , supraclavicular or bilateral neck lymph node metastasis , or large neck node ( > 6 cm ) [ 2 ]  . 
for patients with locoregional recurrence after definitive radiotherapy , aggressive local treatment may be considered for a better outcome . keywords neoplasm recurrence , local treatment outcome disease management salvage therapy survival intensittsmodulierte strahlentherapie fr t4 - nasoparynxkarzinobehandlungsergebnisse und lokoregionre rezidive zusammenfassung ziel . 
der grad der lokoregio nren rezidivfreiheit , die berlebensrate ohne fernmetastasen oder progressionen und die gesamtberlebensrate ( os ) lagen nach 5 jahren bei 81 , 2 , 72 , 2 , 61 , 9 und 78 , 1% . 
bei 27 patienten kam es zu lokoregionren rezidiven : 85 , 2% in der zuvor betroffenen region , 11 , 1% in der nhe dieser region , 3 , 7% in ei ner entfernten region . 
die schdigungen bis grad 3 in form von ototoxi zitt , fibrose am hals , mundtrockenheit , epistaxis sowie durch bestrahlung verur sachte nekrose des schlfenlappens lagen bei 18 , 2 , 9 , 8 , 6 , 3 , 2 , 1 und 5 , 6% . 
bei patienten mit lokoregionren rezidiven ist zur verbesserung der ergebnisse eine aggressive lokale therapie in betracht zu ziehen . schlsselwrter rezidivierende lokale neoplasmen behandlungsergebnisse krankheitsmanagement salvage - therapie berleben or pf ( 100 mg / m2 cisplatin on day 1 and 1000 mg / m2 fluorouracil on days 13 ) every 3 weeks for 2 or 3 cycles . 
all patients were followed up every 23 months for the first 2 years , every 4 months for the third year , and every 6 months after the third year . 
 the treatment response after radiotherapy was assessed 3 months after completion of treatment by endoscopy and head and neck mri as well as a biopsy of the nasopharynx if indicated . 
the initial recurrence site was defined only by the site of first relapse as local , distant , or synchronous . salvage treatments for locoregional recurrence all patients with locoregional recurrence were first considered for primary surgical management . 
endoscopic potassium - titanyl - phosphate ( ktp ) laser nasopharyngectomy was performed for patients with limited local recurrent tumor , primarily rt1 or rt2 disease [ 10 ]  . 
salvage imrt re - irradiation was considered for all patients with recurrent locoregional disease not suitstrahlentherapieundonkologie122013 | 1003 original article 0.4c overall survival locoregional recurrence - free survival distant metastasis - free survival progression - free survival time ( months ) fig . 
1 9 the outcomes of 154 t4 npc patients treated with intensitymodulated radiotherapy with regard to locoregional control , distant metastasis - free survival , progressionfree survival , and overall survival able for surgery , and concurrent chemotherapy was given in all cases , with a platinum - based regimen if possible . 
a maximum cumulative dose constraint of 50 or 60 gy was implemented for spinal cord or brainstem treatment or the cumulative biological effective dose ( bed ) with an / ratio of 3 was less than 100 or 120 gy , respectively [ 11 ]  . 
patients receiving re - irradiation were followed - up at least every 3 months . statistical analysis statistical analysis was performed using the statistical package for social sciences for windows , version 17.0 ( spss , chicago , il )  . 
actuarial estimates of lrc , distant metastasis - free survival ( dmfs ) , progression - free survival ( pfs ) , and overall survival ( os ) were calculated using the kaplanmeier method . 
at the time of analysis , 1004 | strahlentherapieundonkologie122013 56 patients ( 36.4% ) had recurrence at one or more sites and 29 ( 18.8% ) had died of the disease . 
univariate and multivariate analyses ( .tab.2 ) revealed that old age , imrt alone without concurrent chemotherapy , t4 tumor with both intracranial invasion and cranial nerve involvement , advanced n stage ( n3 ) , and suboptimal total dose ( < 70 gy ) were associated with poor outcomes . locoregional recurrence and feasibility of salvage treatments the clinical characteristics of the 27 patients with locoregional recurrence are detailed in .tab.3. 
two patients required salvage neck dissection for nodal recurrence ( 1 received adjuvant ccrt ) , 2 patients with local t12 recurrent tumor received ktp laser nasopharyngectomy ( 1 received adjuvant ccrt ) , and 9 patients received definitive re - irradiation or chemoradiation as salvage treatments . 
2 9 the outcomes of recurrent npc patients treated with aggressive treatments , including operation or re - irradiation , ( n = 14 ) versus conservative treatments ( n = 13 ) with regard to a distant metastasis - free survival ( p = 0.070 ) and b overall survival ( p = 0.051 ) aggressive treatment conservative treatment p = 0.070 aggressive treatment conservative treatment p = 0.051 distant metastasis - free survival ( months ) overall survival ( months ) tively . 
one patient who received imrt in the neck field was found to have severe stenosis of the right internal carotid artery 47 months after treatment , which was successfully stented . discussion the current study , presently the largest series focused on patients with nonmetastatic t4 npc treated using the modern imrt technique , was effective for studying the efficacy of imrt on locally advanced npc . 
the consensus on radiotherapy dose and fractionation for patients with t4 npc has not been reached [ 12 , 13 , 14 , 15 , 16 , 17 ]  . 
 furthermore , given the entire proportion of t4 disease in our series , it appears that the os of patients treated using imrt was not inferior to that of other series using modern radiotherapy techniques . three of 154 patients ( 1.9% ) in our series developed marginal locoregional recurrence , which is in line with some retrospective studies demonstrating a marginal miss in imrt - treated head and neck cancer patients [ 9 , 18 ]  . 
in our series , marginal failure occurred superiorly at the posterior cavernous sinus , petrous apex , and sphenoid sinus ; posteriorly at the clivus and retroclival dura ; and anteriorly at the pterygoid plate , inferior orbital fissure , and pterygopalatine fossa . 
however , marginal dose coverage at the mentioned regions is inevitable to some extent because of nearby critical neural structures including the brainstem , chiasm , and bilateral optic nerves . 
to avoid marginal miss , accurate target delineation and radiation delivery should be addressed . in our series of 27 patients with locoregional recurrence , 14 received aggressive treatments , including surgical intervention or re - irradiation for locoregional recurrence , and all but 2 of these 14 patients achieved at least stable disease without tumor progression . 
 [ 16 ] present study t34 40% t34 53% t4 100% 70 gy / 33 fx 76 gy / 35 fx 70.2 gy / 30 fx 72 gy / 30 fx 66 gy / 33fx , srt boost 68 gy / 30 fx 70 gy / 3335 local : 91 nodal : local : 91 nodal : local : 98 nodal : 83 ototoxicity : 7 xerostomia : 4 ototoxicity : 42 gr 4 epistaxis : 4 radiological temporal necrosis : 4 ototoxicity : 15 ototoxicity : 4 radiographic temporal necrosis : 12 radiographic temporal necrosis : 12 mucositis : dermatitis : 5 ototoxicity : 18 xerostomia : 6 radiographic temporal necrosis : 6 imrt intensity - modulated radiotherapy , rt radiotherapy , pfs progression - free survival , lrc locoregional control , dmfs distant metastasis - free survival , os overall survival , fx fractions , n / a data not available.adisease - free survival strahlentherapieundonkologie122013 | 1007 19 . 
wang state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . letter to the editor strahlenther onkol 2013 189 : 10491050 doi 10.1007 / s00066 - 013 - 0461 - 8 received : 5 september 2013 accepted : 11 september 2013 published online : 27 october 2013 springer - verlag berlin heidelberg 2013 c . 
biti1 1 department of radiation - oncology , university of florence , italy adenoid cystic carcinoma of the breast the double face of an exocrine gland carcinoma letter to the editor adenoid cystic carcinoma ( acc ) is the most common tumour of the minor salivary glands , but it also represents a rare type of breast cancer , accounting for 0.1 1% of all breast tumours [ 1 , 2 ]  . 
1 distribution of cases according to individual characteristics ( n = 13 ) 51 ( range 3971 ) 9 ( 69.2% ) 4 ( 30.7% ) 1 ( 7.6% ) 5 ( 38.4% ) 7 ( 53.8% ) median age , years t stage tis t1c t2 grade 1 2 n stage pn0 pn2c estrogen receptor status negative positive progesterone receptor status negative positive 9 ( 69.2% ) 4 ( 30.7% ) 9 ( 69.2% ) 4 ( 30.7% ) 11 ( 84.6% ) 2 ( 15.3% ) from 19902007 we treated 13 women affected by acc , all patients underwent to definitive quadrantectomy , 2 patients underwent sentinel lymphnode biopsy and 11 patients axillary lymph node dissection . histology confirmed the presence of acc in all the patients ; however in 3 cases it was intermingled with ductal carcinoma . 
rare are the cases of acc intermingled with other types of breast cancer ; in literature there are some case reports where acc is mixed with other histology as small cell carcinoma [ 3 ] and spindle cell carcinoma [ 4 ]  . 
 [ 7 ] reviewed 140 cases and found only one case positive er . all the patients received adjuvant whole breast radiotherapy ( range 50 60 gy ) and 2 patients underwent adjuvant chemotherapy for positive lymph nodes ; hormonal therapy was administered in 3 out of the 4 cases of positive receptors . 
in our analysis none died from disease . in conclusion , primary treatment of acc of the breast is surgical and quadrantectomy can be a valid approach if followed by radiation therapy on the whole breast [ 8 ] ; unknown is the role of chemotherapy . 
franzese , md department of radiation - oncology university of florence viale morgagni 85 50132 florence , italy ciro.franzese@me.com strahlentherapie und onkologie 12 2013 | 1049 letter to the editor compliance with ethical guidelines conflict of interest . 
biti state that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 10321039 doi 10.1007 / s00066 - 013 - 0451 - x eingegangen : 11 . 
nach der integration von behandlungsplanung , ordination und der organisatorischen abbildung der bestrahlungsplanung [ 14 , 22 ] im abteilungssystem sollten parallel smtliche dokumentenqualitten in die digitale umgebung eingebunden werden . 
zustzlich soll ein extrakt aus der elektronischen patientenakte in form von pdf - dateien mglich sein . material und methode um ein effektives , digitales dokumentenmanagement betreiben zu knnen , ist eine implementierte elektronische patientenakte ( epa ) voraussetzung . 
doch diese alleine reicht nicht aus , da man es mit einer vielzahl verschiedener dokumentenqualitten zu tun hat , die nicht direkt in der eigenen digitalen akte erzeugt werden , aber im endeffekt qualifiziert in die elektronische krankenakte eingepflegt werden mssen , damit der nutzer alle daten zu einem patienten schnell und sicher auffinden kann . 
zudem erhht sich der nutzen und die effektivitt des verfahrens , wenn die etablierung von schnittstellen zu anderen klinischen system mglich ist . dokumentenimport die vorhandenen dokumentenqualitten ( .tab.1 ) wurden durch eine interdisziplinre arbeitsgruppe ( bas - ag ) im detail analysiert . 
dies fhrt zu einer zeitnahen verfgbarkeit der digitalisierten daten und informationen im abteilungssyste da auf diesem weg sehr viele dokumente zu einem patienten in das system aufgenommen werden , ist es essentiell , dass die einzelnen dokumente schnell gefunden und effizient gesichtet werden knnen . 
im folgenden werden die basisvarianten nher vorgestellt . a - dokument das a - dokument ist der klassische ( und hufigste ) fall , typischerweise bei papiergebundenen dokumenten aus externen einrichtungen . 
das dokument wird manuell gescannt , anschlieend erfolgt der import mit qualifizierung und zuordnung zum patienten ber eine integrierte dokumentenschnittstelle des bas . b - dokument das b - dokument unterscheidet sich zum a - dokument durch das vorhandensein einer dokumentenkennung ( barcode oder nummer )  . 
als quelle der dokumentdateien kommen jede art von datentrgern , wie usb - stick , cd , dvd zum einsatz . d - dokument bei dem d - dokument handelt es sich um die digitale form des b - typs ; eventuell muss auch eine digitale formatanpassung erfolgen . bei dokumenten , die in externen dvsystemen wie z . 
es muss sichergestellt sein , dass die benutzer ( meist rztliches personal ) einen schnelstrahlentherapieundonkologie122013 | 1033 zusammenfassung abstract strahlenther onkol 2013 189 : 10321039 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0451 - x h.fahrners.kirrmannf.rhnerm.schmuckerm.hallf.heinemann multimodales dokumentenmanagement in der strahlentherapie zusammenfassung hintergrundundziel . 
ziel dieses vorhabens war es , alle dokumente , unabhngig davon aus welcher quelle sie stammen ( papiergebunden oder digital ) , in das abteilungssystem zu integrieren oder inhalte aus dem bas strukturiert zur verfgung zu stellen . 
die vorhandenen dokumentenqualitten wurden durch eine interdisziplinre arbeitsgruppe ( bas - ag ) im detail analysiert und nach der berprfung und bewertung der abbildungsmglichkeiten in unserem bas in ein flussdiagramm umgesetzt . 
 die erarbeiteten vorgaben wurden durch die klinische und administrative informatik ( kai ) der klinik fr strahlenheilkunde in einer testumgebung umgesetzt und nach genauer multimodal document management in radiotherapy abstract backgroundandpurpose . 
after incorporating treatment planning and the organisational model of treatment planning in the operating schedule system ( bas , betriebsablaufsystem ) , complete document qualities were embedded in the digital environment . 
the aim of this project was to integrate all documents independent of their source ( paperbound or digital ) and to make content from the bas available in a structured manner . 
it was a further aim , if possible , to automate the removal of paper documents from the departmental work flow , or even to make such paper documents superfluous . 
in addition patient record extracts in the form of pdf files for the medical services of the healthcare insurer can be generated . keywords clinic management documents workflow quality assurance , health care patient care planning len und einfachen zugriff auf die dokumente erhalten . 
an den medizinischen dienst der krankenkassen ( mdk ) und andere einrichtungen wie kliniken und praxen [ daten der operationenund prozedurenschlssel ( ops ) in verschlsselter pdf - datei an zuweiser zur abrechnung ] geschickt . 
dokument kolloquium konsil kv - dokument labor operationsbericht patientenpost radiologiebefund extern intern intern intern intern intern intern intern intern intern intern extern extern intern intern intern extern extern extern extern extern extern extern extern ph / ls externer arztbrief interner arztbrief rckverfilmte interne bestrahlungsunterlagen bestrahlungsnachweise brachytherapie bestrahlungsdokumente exactrac unterlagen 1 . 
physikalische kontrolle dosimetrieunterlagen imrt dosimetrieunterlagen portal imaging einverstndniserklrungen forschung und lehre einverstndniserklrungen i.v. - kontrastmittelgabe einverstndniserklrungen strahlentherapie einverstndniserklrungen chemotherapie endoskopiebefunde histologiebefunde aufzeichnungen zur adaptiven igrt aufzeichnungen zu cone - beam - cts dokumentation der positionierung nach igrt z . 
. tumorkonferenzen zak ( elektronisches portal des kis fr konsile ) arbeitsunfhigkeitsbescheinigungen , rezepte laborbefunde operationsberichte korrespondenz mit patienten ct , mrt , konventionelle bildgebung , sonographie lufu , hno , ekg etc . verlaufsbgen gutartige unterlagen zu auswrtigen vorbestrahlungen extern intern extern untersuchung div . verlauf gutartige vorbestrahlung ls leitstelle , ph physik , igrt image guided radiotherapy , lufu lungenfunktion , hno hals - nasen - ohren , ekg elektrokardiogramm , mrt magnetresonanztomographie , ct computertomographie kv kassenrztliche vereinigung tab . 
3 basis - dokumentenqualitten fr den datenimport zielformat verfahren zielort a - dokument b - dokument c - dokument d - dokument qualifizierte kennung nein quellforpapier papier digital digital barcode / nummer nein barcode / nummer / dateiname automatisch nein nein scan scan schnittstelle schnittstelle le konnten wir auch sicherstellen , dass ein patient nach dem patientenrechtegesetz neben der einsicht seiner krankenakte diese auch als ausdruck mitnehmen kann . 
grundstzlich werden alle schritte elektronisch protokolliert , so dass bei bedarf genau nachvollzogen werden kann , wer wann , was und wie ins system eingebracht oder aus ihm extrahiert hat . 
die barcodes werden entweder dynamisch aus kis - daten generiert oder statisch in die formulare eingebettet ( 2 - d - barcodes in der einverstndniserklrung oder einwilligung zur speicherung von daten )  . 
bei dokumenten , die aus mehreren seiten bestehen , wurden eindeutige identifikationsmerkmale eingebunden , damit die dokumentzugehrigkeit jeder einzelseite immer nachvollziehbar ist . exemplarisch wird im folgenden das automatisierte einbringen von dokumenten nher erlutert . 
ct computertomographie , db datenbank , drr digital rekonstruiertes rntgenbild , epi electronic portal image , kis klinikinformationssystem , mr magnetresonanz , pet positronenemissionstomographie , rt radiation therapy rausforderung war der umgang mit arztbriefen , die noch immer postalisch an haus - / fachrzte und zuweiser versendet werden mssen . 
damit ist gewhrleistet , dass niemand auerhalb des vereinbarten personenkreises zugriff auf diese daten erlangen kann . da die dokumentation der behandlung entweder direkt im abteilungssystem vorgenommen oder aus drittsystemen digital bernommen wird , kann auf papiergebundene unterlagen weitgehend verzichtet werden . 
der papiergebundene bestrahlungsnachweis sowie der gesamte prozess der bestrahlungsplanung ist komplett im bas abgebildet , da bestrahlungsplne und deren dokumentation aus den bestrahlungsplanungssystemen extrahiert und als pdf - dokumente eingebunden werden knnen . anforderungsmanagement ein weiteres beispiel fr die vermeidung von papier und die erhhung der effektivitt ist die einfhrung eines digitalen anforderungsmanagements . 
durch die eigenentwicklung eines web - portals ( programmiersprache : php , javascript ; framework : jquery ; datenbank : postgresql , mssql ; kommunikation : ajax / json ; [ 15 ] ) gelang es , das anforderungsmanagement ( .abb.4 ) stark zu vereinfachen . 
die eingabemaske kann schnell ausgefllt werden , da die absenderdaten wie name , e - mail - adresse und telefonnummer nach eingabe der im klinikum zentral etablierten benutzerkennung ( ldap , lightweight directory access protocol ; [ 18 ] ) vom system automatisch ausgefllt werden . 
so ist sichergestellt , dass eine anforderung immer bearbeitet wird . alle relevanten prozesse und arbeitsanweisungen wurden nach den formellen vorgaben unseres klinikumsweiten qualittsmanagementsystems ( ktq ) dokumentiert und sind im qualittsmanagement - ( qm - ) handbuch jederzeit und von jedem mitarbeiter elektronisch einsehbar . 
3 8 dokumentengestaltung fr den automatisierten import abschlieend muss erwhnt werden , dass fr die datensicherheit und - archivierung aufwendige vorkehrungen zu treffen sind , da bei einem vlligen verzicht auf papier alle informationen nur noch in digitaler form vorliegen ; krankenakten knnen somit nicht mehr verloren gehen . 
die schnittstellen zum abteilungssystem ( bas ) waren schon zum zeitpunkt der bas - beschaffung vorhanden . die konzeptphase dauerte von februar bis mai 2010 , die programmierung von juni bis september 2010 und die implementierung inklusive betatest in unserer testumgebung von oktober 2010 bis april 2011 . ergebnisse und diskussion der abteilung ist es unter erfllung der oben genannten kriterien gelungen , alle relevanten dokumente ber kontinuierliche , validierte und qm - konforme prozesse in das abteilungssystem einzubinden . 
neben einer ausgeprgten reduzierung des arbeitsaufkommens und dem wegfall der papiergebundenen krankenakte , erreichten wir durch die zeitnahe und qualifizierte verarbeitung und ablage der dokumente in unserem abteilungssystem eine hohe , effektive und transparente datenverfgbarkeit . 
besides surgery , chemotherapeutic , hormonal and radiooncological treatment are administered [ 2 , 8 , 9 , 10 , 11 , 15 , 16 , 19 , 30 ]  . 
in order to gain a better understanding and subsequently new therapy options , it is necessary to elucidate the molecular causes of endometrial cancer tumourigenesis . multiple tumour entities , e.g. 
one of the cd44 ligands is osteopontin - 1 [ 29 ] , a multifunctional phosphoglycoprotein that is expressed in a secreted and an intracellular form in a broad range of cells [ 24 ]  . 
the highest expression of osteopontin - 1 can be detected in bone , but it is also expressed in kidney , brain , smooth muscle tissue , macrophages as well as multiple other epithelial and cancer cells [ 24 , 28 ]  . 
plasma osteopontin has been reported to be a putative marker of tumour hypoxia in a broad variety of cancers and it is well established that serum levels of osteopontin - 1 are markedly increased in patients with metastatic tumours [ 6 , 22 ]  . more advanced studies revealed that osteopontin - 1 is a glycoprotein that contains an arginineglycineaspartate ( rgd ) motif , which contains a hypersensitive protease cleavage element for thromb this element separates the cd44 binding domain from a further binding domain for integrins [ 23 , 28 ]  . 
 this n - terminal rgd domain is activated after thrombin cleavage and this fragment of osteopontin - 1 is able to bind integrins after its phosphorylation [ 21 ] , whereas the c - terminal part of the osteopontin - 1 molecule binds cd44 receptors [ 23 ]  . 
osteopontin - 1 influences the adhesion and migration of cells [ 7 , 12 ] and therefore can directly impact on diverse processes of tumourigenesis like invasion , metastasis and angiogenesis [ 17 , 24 ]  . furthermore osteopontin - 1 expression is associated with an activation of the pi3 kinase / akt signal transduction pathway in many tumour entities and a subsequent resistance against apoptosis is being discussed [ 13 , 24 ]  . to our knowledge the role for osteopontin - 1 in endometrial cancer has only been functionally characterized with regard to angiogenesis [ 5 ]  . 
the investigations reported here were performed in one cell clone with stable repression of osteopontin - 1 ; therefore an influence of this selection criterion and clonal effects cannot be excluded [ 5 ]  . 
the relative intensity of osteopontin - 1 band was calculated by densitometry ; osteopontin - 1 expression was referred to the relevant - actin expression and normalised to the osteopontin - 1 expression in ishikawa cells ( set to 1 ) according to the suppliers recommendations . 
in order to rule out clonal effects and other unspecific selectional influences all analyses were performed in transient transfected cell populations . reverse transcriptase ( rt ) - pcr analyses tive pcr : 5 - atctcctagccccacagaat - 3 and 5 - catcagactggtgagaatcatc - 3 for full - length osteopontin - 1 , as well as 5 - ctgaggaaaagcagaatg - 3 and 5 - aatggagtcctggctgt - 3 for splice variant c of osteopontin - 1 . western blot whole rna was isolated using rneasy mini kit ( qiagen , hilden germany ) according to suppliers recommendations . 
the following primers were applied in the semiquantitafor immunobloting cells were trypsinized , washed with ice - cold pbs and resuspended in ripa buffer , which contained protease inhibitors ( protease inhibitor cocktail , roche , mannheim , germany )  . 
the membrane was probed for protein detection with specific first antibodies [ anti - spp1 / osteopontin - 1 ( epitomics , burlingame , ca , usa ) ; anti - caspase - 3 ( cell signaling , frankfurt am main , germany ) ; anti - parp ( cell signaling , frankfurt am main , germany ) ; anti - - aktin ( abcam , cambridge , great britain ) ] and peroxidase - conjugated secondary antibody ( anti - rabbit igg ; cell signaling , frankfurt am main , germany ) incubated and then visualized per enzymatic reaction ( immobilon western chemiluminescent hrp substrate , millipore , schwallbach , germany )  . wound - healing assay / wound assay confluent cell cultures cultured in 6 - well plates were injured with a pipette tip . 
the cell culture was rinsed with media and the closing of the wound with growing cells documented with a digital camera at different time points . aliquots of 2105 cells were seeded 18 h after sirna transfection on a matrigel - coated membrane with a pore size of 8 m ( bd bioscience , heidelberg , germany ) in media not containing fcs . 
after incubation for 12 h at 37c cells were scraped from the upper side of the membrane , cells that had migrated into the lower chamber , were fixed and counted after they were stained with crystal violet . clonogenicity assay cells were treated with different doses of radiation 24 h after they had been transiently transfected with sirna . 
it is of note that in ishikawa cells ( model for endometrial cancer with low grade of malignancy ) osteopontin - 1 mrna expression was lowest and that splice variant c was not detectable . 
the strongest expression of osteopontin - 1 full - length transcript and splice variant c mrna was seen in hec - 1a cells ( model for endometrial cancer with intermediate grade of malignancy )  . 
opposed to these findings there was only low expression of both osteopontin - 1 transcripts in an - 3ca cells ( model for endometrial cancer with high grade of malignancy )  . 
the higher the grade , the higher was the detected osteopontin - 1 protein expression . a higher osteopontin - 1 protein expression associated with an increase in tumour grade has been described in other tumour entities [ 27 , 32 ]  . 
our results suggest that a reduced expression of osteopontin - 1 in endometrial cancer could inhibit the development of invasion and metastasis in these cells . keywords osteopontin - 1 endometrial neoplasms radiation therapy neoplasm metastasis rna , small interfering untersuchungen zur rolle von osteopontin - 1 in endometriumkarzinomzelllinien zusammenfassung hintergrund . 
osteopontin - 1 ist in vielen tumorarten ein gut untersuchtes protein , dem eine vielfltige rolle bei den diversen pro zessen der tumorentwicklung wie invasion , metastasierung und angiogenese zugeschrie ben wird . 
zudem deuten unsere ergebnisse darauf hin , dass durch eine inhibition von osteopontin - 1 diverse prozesse der tumorentwicklung , wie invasion und metastasierung bei endometriumkarzinomen , gehemmt werden knnen . schlsselwrter osteopontin - 1 endometriumkarzinom strahlentherapie tumormetastasierung small interfering rna showed increased osteopontin - 1 expression 48 h after transfection . 
in addition , 30 h after transfection a statistically significant reduction of invasion and migration could be detected an3 - ca hec1a ishikawa osteopontin - 1 - actin control an - 3ca hec - 1a ishikawa fig . 
the time points ( 24 , 48 , 72 h ) refer to the length of time after transfection and proteins were separated on a 10% sds - polyacrylamide gel . 
thus , the wound - healing assay as well as the boyden chamber assay showed that the reduction of osteopontin - 1 protein expression leads to a reduction in migration and invasion in endometrial cancer cells . next we investigated the influence of osteopontin - 1 on radiosensitivity of these cells . 
resistance against radiation mediated by osteopontin - 1 has been described in other tumour entities as well [ 3 , 26 ]  . in the next step we investigated whether the expression level of osteopontin - 1 protein correlates with marker proteins of apoptosis like parp and caspase - 3 . 
after inhibition of osteopontin - 1 expression there was no time point where we were able to detect an increase of the 89 kda parp fragment if compared to nontransfected controls ( c ; nontransfected cells )  . 
this observation is in contrast to the results gained in other tumour entities , in which osteopontin - 1 expression is associated with an induction of apoptosis [ 31 ]  . 
in accordance with that we found in the endometrial cell lines we investigated especially in an3 - ca cells a reduction of the parp cleavage product at 24 h after transfection of osteopontin - 1 specific sirna . 
cells not transfected ( a , d , g ) , cells transfected with control sirna ( b , e , h ) and transfected with specific sirna directed against osteopontin - 1 ( c , f , i ) were investigated with respect to invasion and migration . 
cells not transfected ( a , d , g ) , cells transfected with control sirna ( b , e , h ) and transfected with specific sirna directed against osteopontin - 1 ( c , f , i ) were investigated with respect to invasion and migration . 
photographs were taken with a 10 - fold magnification boydenchamber invasion assay with ana - ca ( a ) , hec - 1a ( b ) , and ishikawa cells ( c ) fig . 
cells not transfected ( a , d ) , cells transfected with control sirna ( b , e ) and transfected with specific sirna directed against osteopontin - 1 ( c , f ) were investigated with respect to invasion and migration . 
18 h after transfection with specific sirna directed against osteopontin - 1 ( opn sirna ) respectively with control sirna ( si control ) cells were placed in transwells and after 12 h of incubation their invasive behaviour was analyzed . 
cells were irradiated 24 h after transfection with specific sirna against osteopontin - 1 ( siopn ) respectively controll sirna ( si control ) with the depicted doses and seeded in culture dishes afterwards . 
the number of formed cell clones in each sample were normalized to the nonirradiated controls of each cell line ( the number of formed clones in these nonirradiated sample was set 1 )  . 
the mean values from three independent measurements are presented 1046 | strahlentherapieundonkologie122013 an3 - ca hec1a ishikawa osteopontin - 1 parp 119 kda 89 kda - actin caspase - 3 35 kda - actin an3 - ca sico siopn hec1a c sico siopn ishikawa sico siopn fig . 
proteins from nontransfected cells ( c ) and cells transfected with specific sirna directed against osteopontin - 1 were analyzed at different time points after transfection ( 24 , 48 , 72 h )  . 
proteins from nontransfected cells ( c ) and cells transfected with specific sirna directed against osteopontin - 1 ( siopn ) as well as cells transfected with control sirna ( sico ) were analyzed . 
hnig state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 915916 doi 10.1007 / s00066 - 013 - 0457 - 4 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
early reports suggested poor response and anaplastic transformation following radiotherapy , whereas other publications did not observe this [ 5 , 6 , 7 , 8 , 9 ]  . 
he was treated with primary highdose - rate ( hdr ) brachytherapy using a custom - made intra - oral mold . case an 85 - year - old man was referred to maastro clinic because of a functionally irresectable oral verrucous carcinoma of the left upper alveolar ridge and soft / hard palate extending to the left buccal mucosa . 
intra - oral examination showed an extensive , superficially spreading tumor along the upper alveolar ridge to the retro - alveolar triangle , with infiltration of the left soft and hard palate . 
taking into consideration the tumors behavior , the number of fractions and associated side - effects of external beam radiotherapy ( ebrt ) , as well as the patients age and co - morbidities , we decided to treat this patient with hdr brachytherapy . hdr brachytherapy preparation and treatment in collaboration with a maxillofacial prosthodontist of the department of cranio - maxillofacial surgery , the preparation of the brachytherapy mold started with an impression of the upper alveolar process with alginate . 
from the plaster model created from this impression , an individual impression tray of a light - cur894 | strahlentherapieundonkologie102013 review of literature low dose rate ( ldr ) and pulsed dose rate ( pdr ) brachytherapy techniques have long played an important role in the treatment of head and neck malignancies [ 11 , 12 ]  . 
the main advantages of brachytherapy include the possibility to administer high radiation doses to the tumor , increasing local control , sparing of normal adjacent structures , and maybe an advantageous functional outcome compared to surgery and ebrt [ 13 , 14 , 15 ]  . 
hdr brachytherapy provides better control of the dose distribution by varying the dwell times per catheter , and by increasing the fraction dose shorter overall treatment times can be achieved [ 13 ]  . hdr brachytherapy can be applied to tumors of different histologies originating from various head and neck subsites [ 11 ]  . 
 it is most commonly used as single treatment modality in the primary or recurrent setting , or as a boost in combination with modern ebrt techniques [ 11 , 13 ]  . in patients with lip carcinoma , excellent local control rates of more than 90% can be reached with tumor excision , ebrt or temporary interstitial implant [ 16 , 17 ]  . 
radiation therapy is indicated for large tumors or for lesions involving the commissure to minimize functional morbidity [ 16 ]  . for oral mucosa tumors < 4 cm in diameter and < 1.5 cm in thickness , brachytherapy is a possible alternative to surgical excision [ 16 ]  . 
involvement of the bucco - alveolar sulcus or intermaxillary commissure are contra - indications for brachytherapy [ 16 ]  . in patients with early stage oral tongue cancer ( ct1n0 and ct2n0 , tumor diameter < 4 cm ) brachytherapy is a good treatment option [ 18 ]  . 
images showing regression of confluent mucositis 11 weeks ( b ) , 15 ( c ) , 20 ( d ) , 22 ( e ) , and 24 weeks ( f ) after completing hdr brachytherapy , respectively ing urethane acrylate was made . 
in collaboration with the medical physicist of maastro clinic , a baseplate from erkodur ( erkodent , pfalzgrafenweiler , germany ) was crafted on the plaster model based on this definitive impression . 
the irradiation time per fraction was approximately 2 mthe course of hdr brachytherapy was well tolerated even though a grade iv mucositis occurred in the irradiated area after 8 fractions . 
at that last follow - up visit , there was complete remission of the primary tumor and no lymphadenopathy . case study abstract zusammenfassung the gec - estro guidelines recommended brachytherapy for ct1n0 and ct2n0 floor or mouth tumors < 3 cm in diameter with a distance of more than 5 mm from the mandible . 
tumors between 34 cm and located more than 0.5 cm from the mandible may be treated with either brachytherapy or surgery . ebrt plays an essential role in the treatment of oropharynx cancers to control subclinical lymphatic spread [ 21 ]  . 
 in exophytic tumors with a diameter of 1 cm , previously irradiated sites and for recurrent disease brachytherapy as single treatment may be indicated [ 18 ]  . due to the highly radiosensitive nature of nasopharyngeal carcinoma ebrt is the treatment of choice [ 16 ]  . 
 because of a rapid dose fall - off , its use is limited to tumors with a maximal thickness of 1 cm [ 16 , 18 ]  . role of hdr brachytherapy in maxillary tumors surgery is the preferred treatment in oral verrucous carcinomas with radiotherapy as a good alternative in inoperable patients or functionally irresectable tumors . 
 in the past , the use of hdr brachytherapy with a customized mold in oral cavity tumors was limited because of the irregular anatomical surface in most tumor subsites hampering the use of nonflexible connection catheters [ 22 ]  . 
 [ 23 ] described a case of extensive upper gum carcinoma treated with combined imrt ( 46 gy in 23 fractions ) and customized - mold hdr brachytherapy ( 32 gy in 8 fractions twice daily )  . 
 [ 22 ] reported on 4 patients with a superstrahlenther onkol 2013 189 : 894898 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0412 - 4 k.m.j.vangesteld.j.m.buurmanr.pijlsp.a.w.h.kesslerp.l.a.vandenendea.l.hoffmanne.g.c.troost locally advanced verrucous carcinoma of the oral cavity . 
we present an 85 - year - old man with functionally irresectable ct3n0m0 verrucous carcinoma superficially spreading along the upper alveolar ridge to the retro - alveolar triangle , with infiltration of the left soft and hard palate and buccal mucosa . 
the scarce literature on customized mold hdr brachytherapy in maxillary tumors is reviewed and recommendations for other head and neck tumors are given . keywords hdr brachytherapy verrucous carcinoma oral cavity review lokal fortgeschrittenes verrukses karzinom der mundhhle . 
wir prsentieren einen 85 - jhrigen patienten in inoperablem zustand mit einem funktionell irresektablen , verruksen ct3n0m0 - karzinom , das sich entlang des tuber maxillae zum trigonum retro - molare hin ausbreitete und sowohl den weichen und harten gaumen , als auch die wangenschleimhaut infiltrierte . 
die nur in geringer zahl vorhandene literatur ber hdr - brachytherapie fr tumoren der maxilla mithilfe einer individuellen gussform wird besprochen und es werden empfehlungen zur indikation der hdrbrachytherapie fr andere tumoren im kopfhals - bereich gegeben . schlsselwrter hdr - brachytherapie verrukses karzinom mundhhle review ficial or exophytic tumor of the oral cavity without deep invasion ( ct1 - 2n0m0 ) radically treated with ebrt ( 2240 gy ) followed by hdr brachytherapy with a customized mold ( 2535 gy in 10 fractions twice daily )  . 
troost state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . consent was obtained from all patients identifiable from images or other information within the manuscript . 
in case of underage patients , consent was obtained from a parent or legal guardian . original article strahlenther onkol 2013 189 : 849855 doi 10.1007 / s00066 - 013 - 0389 - z received : 9 may 2013 accepted : 22 may 2013 published online : 21 . 
august 2013 springer - verlag berlin heidelberg 2013 d.rades1n.d.seibold1s.e.schild2m.p.gebhard3f.noack3 1 department of radiation oncology , university of lbeck 2 department of radiation oncology , mayo clinic scottsdale 3 institute of pathology , university of lbeck androgenreceptor expression prognosticvalueinlocally advancedsquamouscellcarcinoma oftheheadandneck despite advances in treatment , patients with locally advanced squamous cell car cinoma of the head and neck ( scchn ) still have a relatively poor prognosis . 
a pathological study of 20 samples of oral scc has sug gested that ar transcripts were less ex pressed in oral scc specimens than in healthy tissues [ 3 ]  . in addition , ar expression has been suggested to be associated with more fa vorable outcomes for gastric cancer , blad der cancer , breast cancer , and prostate cancer in retrospective studies [ 5 , 6 , 10 , 13 , 19 , 20 ]  . 
in contrast , a retrospective study did not find a significant relationship be tween ar expression of tumor cells and treatment outcomes in patients with non small cell lung cancer [ 16 ]  . 
one retrospec tive study of prostate cancer patients has suggested that high levels of ar were as sociated with more aggressive disease and worse biochemical recurrencefree sur vival [ 11 ]  . 
a recent retrospective study of 91 patients with small differentiated thy roid cancer found that ar expression was associated with more aggressive tumors [ 12 ]  . thus , more studies are required to bet ter define the prognostic role of ar ex pression in cancer patients . 
the present retrospective study investigated the im pact of ar expression and additional po tential prognostic factors on treatment outcomes in patients with nonmetastat ic stage iii / iv scchn . materials and methods tumor cell expression of androgen re ceptor was evaluated in resected tumor specimens obtained prior to radiotherapy from 163 patients with locally advanced scchn who were treated with surgery and subsequent radiotherapy or radio chemotherapy and correlated with clinical outcomes . 
the study was approved by the local ethics committee . immunohistochemistry for ar resected tissues were fixed in 4% buffered formalin ( ph 7.0 ) , embedded in paraff the formalinfixed , paraffinembedded tumor samples were used for the prepara tion of a tissue microarray ( tma ) block . 
 the tma block was constructed using a manual tissue arrayer 1 ( beecher in struments , silver spring , md , usa ) with a 1.0mm diameter core biopsy needle . 
antigen retrieval was carried out in 0.01 mol / l sodium ci trate buffer ( ph 6.0 ) for 5 min in a micro wave for estrogen receptor and proges terone receptor expression . 
endoge nous peroxidase was blocked with 0.3% hydrogen peroxidase for 5 msections were incubated with a monoclonal mouse antibody ( clone ar441 ; 1 / 100 dilution ; dako , glostrup , denmark ) for andro gen receptor expression . 
sections were washed with tbs containing 0.1% tween 20 ( ph 7.0 ) and subsequent reaction was performed with the biotinfree horserad ish peroxidase enzymelabeled polymer of the powervision system ( immunolog ic , duiven , the netherlands )  . 
a tissue sample of adult testis served as the posi tive control . patients and treatment the data from 163 patients who received surgery and postoperative radiotherapy for locally advanced scchn were ret rospectively analyzed . 
further criteria for inclusion were successful staining for ar , histologically proven scc of the oro pharynx , oral cavity , hypopharynx or lar ynx , and stage iii or iv disease . 
patients with specific risk factors such as incomplete resection and extracapsular spread of lymph nodes received concurrent chemotherapy with 20 mg / m2 of cisplatin on days 15 and 2933 or with 20 mg / m2 of cisplatin plus 600 mg / m2 of 5fluorouracil on days 15 and 2933 . hpv status formalinfixed , paraffinembedded tu mor probes were analyzed for dna of hpv highrisk subtypes 16 , 18 , 31 , 33 , and 51 with in situ hybridization marked with antibiotin antibody processed in an auto stainer . 
a tumor was defined as hpv positive , if it showed both a specific p16 pattern as a surrogate marker of oncogene activity of e6 and e7 genes and a positive in situ hybridization result . 
positive control was a squamous type carcinoma in situ of the cervix of a patient with known hpv subtype ( hpv chip type 3.5c , chipron gmbh , berlin , germany )  . 
the impact of ar and 11 additional factors on locoregional control ( lrc ) , metastases - free survival ( mfs ) , and overall survival ( os ) was retrospectively studied in 163 patients with nonmetastatic stage iii / iv scchn . 
tumor cell expression of ar was an independent prognostic factor for mfs and os and should be considered in future prospective trials . keywords head and neck neoplasms radiotherapy radiochemotherapy androgen - receptor expression treatment outcome androgenrezeptor - expression . 
der einfluss der ar - expression sowie 11 weiterer faktoren auf die lokoregionale kontrolle ( lrc ) , das metastasenfreie berleben ( mfs ) und das gesamt berleben ( os ) wurde retrospektiv an 163 patienten mit einem nichtmetastasierten scchn im stadium iii / iv untersucht . 
die tumorzellexpression von ar war ein unabhngiger prognosefaktor fr das metastasenfreie berleben und das gesamtberleben und sollte in zuknftigen prospektiven studien bercksichtigt werden . schlsselwrter kopf - hals - tumore strahlentherapie radiochemotherapie androgenrezeptorexpression behandlungsergebnis statistical considerations patients were followed until death or for 666 months ( median 24 months ) in sur vivors . 
2 univariate analysis of locoregional control at1year ( % ) at3years ( % ) at5years ( % ) original article arexpression no yes 60 years > 60 years gender female male ecogperformancescore 01 hemoglobinlevelpre - rt < 12 g / dl 12 g / dl tumorsite oropharynx oral cavity hypopharynx larynx histologicgrade g12 g3 tcategory 12 34 ncategory 01 23 hpvstatus negative positive extentofresection complete incomplete chemotherapy no yes n.a. 
hpv positivity ( rr 2.46 ; 95% ci 0.7115.52 ; p = 0.18 ) and complete tumor resection ( rr 1.61 ; 95% ci 0.842.95 ; p = 0.14 ) were not significant . discussion patients with locally advanced scchn have a relatively poor prognosis . 
the prognostic role of the tumor cell expression ar in patients with lo cally advanced nonmetastatic scchn with respect to lrc , mfs , and os has not yet been investigated . 
several retrospective studies investigated the role of ar expres p = 0.11 time to recurrence ( months ) p = 0.06 time to metastases ( months ) ar expression no ar expression ar expression no ar expression ar expression no ar expression p = 0.032 time to death ( months ) fig . 
1 9 impact of tumor expression of ar on locoregional control ( top ) , metastases - free survival ( middle ) , overall survival ( bottom ) sion in breast cancer patients . 
in contrast , another study of prostate cancer patients suggested that a high level of ar expression was associated with a more ag gressive disease and a lower biochemical recurrencefree survival ( p = 0.005 ) [ 11 ]  . 
 our own previous study of 64 patients with nonsmall lung cancer did not show a significant correlation between ar ex pression and treatment outcomes in terms of lrc , mfs , and os [ 16 ]  . taking into account the data from the literature , it becomes obvious that further studies are required to define the prognos tic role of ar expression for different can cer types . 
ad ditionally , multivariate analyses were per formed in order to correct for imbalances related to several other prognostic factors and further decrease the influence of un controlled biases . in addition to ar expression , im proved treatment outcomes were signifi cantly associated on multivariate analysis with lower tumor stage ( t category and n category ) , favorable tumor site , better performance status , and higher hemoglo bin levels prior to radiotherapy . 
3 univariate analysis of metastases - free survival at1year ( % ) at3years ( % ) at5years ( % ) original article arexpression no yes 60 years > 60 years gender female male ecogperformancescore 01 hemoglobinlevelpre - rt < 12 g / dl 12 g / dl tumorsite oropharynx oral cavity hypopharynx larynx histologicgrade g12 g3 tcategory 12 34 ncategory 01 23 hpvstatus negative positive extentofresection complete incomplete chemotherapy no yes n.a. 
tumor stage , tumor site , per formance status , and the extent of resec tion have been previously recognized as independent prognostic factors for treat ment outcomes in patients with locally advanced headandneck cancer [ 2 , 4 , 7 , 8 , 17 ]  . 
also a negative impact of prert hemoglobin levels < 12 g / dl on treatment outcomes was demonstrated for patients with locally advanced scchn [ 4 , 17 ]  . 
noack state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . historie strahlenther onkol 2013 189 : 908914 doi 10.1007 / s00066 - 013 - 0438 - 7 online publiziert : 25 september springer - verlag berlin heidelberg 2013 g.moser institut fr geschichte und ethik der medizin , universitt heidelberg vor75jahrenentzogder ns - gesetzgeberrztinnen undrztendiestaatliche berufszulassung bestallungen ( approbationen ) jdischer rzteerlschenam30.september1938 vorwort der gesellschaftsprsidenten im jahr 2010 beauftragte die deutsche rntgengesellschaft e . 
 ( degro ) trat im hinblick auf die gemeinsame vergangenheit von drg und degro diesem projekt im jahr 2012 bei . die weitreichenden forschungen mosers zeichnen den verbrecherischen einsatz der rntgenstrahlung im dienste nationalsozialistischen rassenwahns nach und dokumentieren wissenschaftliche karrieren . 
sie umfassen aber auch die oftmals schwierige bergung von biografien verfolgter und ermordeter radiologinnen und radiologen . die hier vorgelegte dokumentation der 1938 ihrer rztlichen approbation beraubten und aus der drg ausgeschlossenen , jdischen kolleginnen und kollegen bildet anlsslich des 75 . 
v. : michael baumann , dresden vor 75 jahren entzog der ns - gesetzgeber rztinnen und rzten die staatliche berufszulassung mit dem inkrafttreten der vierten verordnung zum reichsbrgergesetz vor 75 jahren hrten jdische rzte auf , arzt zu sein , wie ein einschlgiger aufsatz des deutschen rzteblattes im august 1938 fr ende september ankndigte [ 4 ]  . 
blutschutzgesetz die deutschen staatsbrger willkrlich sortiert und die deutschen juden und jdinnen zu rassisch fremden erklrt hatten [ 3 ] , griff diese verordnung fundamental die berufsrechtlichen grundlagen des rztestandes an . 
die bestallungsentziehung der jdischen rzte sollte , so das amtsblatt der reichsrztekammer und der kvd , den schlustein der ausschaltung der juden aus jeglicher rztlicher ttigkeit bilden [ 6 , 8 , 9 ]  . auch fr viele strahlendiagnostisch und - therapeutisch ttigen rztinnen und rzte bedeutete die entziehung der approbation das ende ihrer beruflichen laufbahn im nationalsozialistischen deutschland . 
unter den 1296 mitgliedern der deutschen rntgengesellschaft ( drg ) des jahres 1936 waren mindestens 159 rztinnen und rzte von dem entzug der staatlichen zulassung zur ausbung des arztberufs betroffen.1 nur wenige dieser entrechteten rzte wurden , zudem nur fr eine kurze zeit und in jederzeit widerruflicher form , von der reichsrztekammer als sog . 
12.05.1992 in new york / usa berlin , emigration in die schweiz , san francisco / usa frankfurt / main hannover berlin berlin , emigration in die usa breslau , deportation ghetto / kz theresienstadt . 
1949 rckkehr nach deutschland mnchen , emigration 1940 in die usa berlin , emigration in die niederlande , deportation 21.04.1943 nach ghetto / kz theresienstadt , weiter nach kz auschwitz . 
28.12.1962 in london / grobritannien 1902 1929 1915 1923 1908 1932 1906 1923 1929 1924 1915 1901 1923 1918 1914 1901 1924 1924 1915 1925 1903 1906 1893 1910 1924 1896 1902 tab . 
28.09.1963 in new york / berlin , emigration in die sowjetunion , 1936 in die usa mnchen , emigration 1935 nach london / grobritannien berlin , emigration in die usa . 
auer den archivalischen quellen und den bereits oben genannten publikationen sind die folgenden titel herangezogen worden : ash , mitchell g . / alfons sllner ( eds . ) : forced migration and scientific change . 
2 zerrissene biographien [ 2 ] auf dem gebiet des rztlichen berufswesens hatte die juden diskriminierende , rassische gesetzgebung [ 5 ] mit dem gesetz zur wiederherstellung des berufsbeamtentums vom 20 . 
nach auskunft von rebecca schwoch , hamburg , forschungsprojekt medizinische versorgung von juden fr juden 19381945 gab es 1939 im gesamten deutschen reich fr alle medizinischen fachgebiete zusammen nur 285 krankenbehandler . gonnen , das den ausschluss jdischer und politisch missliebiger rztinnen und rzte von ttigkeiten in einrichtungen in ffentlicher trgerschaft bezweckte . 
der schritt in die emigration bedeutete fr viele ein wagnis [ 10 ] , das besonders in der anfangszeit im exilland nicht nur mit dem verlust sozialer kontakte verbunden war , sondern oft genug auch mit materiellen einbuen , weil examen nicht anerkannt und prfungen wiederholt werden mussten , von der bis oktober 1941 erhobenen reichsfluchtsteuer ganz zu schweigen . 
der anteil der whrend der ns - zeit emigrierten , strahlendiagnostisch oder - therapeutisch ttigen kollegen an der gesamtzahl der jdisch stigmatisierten mediziner dieses fachs lag damit bei rund 47% . etwas ber einen monat nach der approbationsentziehung fand die reichspogromnacht am 9 . 
 september 1938 finden sich deren namen nicht mehr im mitgliederverzeichnis der gesellschaft . auch wenn sich heute nicht mehr eruieren lsst , ob ein austritt der betroffenen oder der ausschluss durch die zustndigen gremien der drg zum ausscheiden der jdisch stigmatisierten mitglieder fhrte , sind die erduldete diskriminierung und das erlittene unrecht der ehemaligen kollegen zu bedauern . 
das folgende verzeichnis soll daher 75 jahre nach dem erlittenen unrecht dem namentlichen gedenken an die schicksale der rzte dienen , die als juden oder jdinnen oder aufgrund ihrer politischen 5 in die gesamtzahl der stigmatisierten sind auch 5 personen eingerechnet , die vor der bestallungsentziehung am 30.09.1938 verstorben waren : paul krause ( 1934 ) , gustav joseph , karl bacharach ( 1935 ) , otto silberberg ( 1937 ) und henri hirsch ( 1938 )  . haltung opfer von diskriminierung , vertreibung und ermordung im nationalsozialismus wurden . gabriele moser , heidelberg korrespondenzadresse g . 
for early stage laryngeal cancer , ( laser ) surgery and radiation therapy ( rt ) have been shown to be similar in terms of efficacy in non - randomized comparisons [ 1 , 2 ]  . for locally advanced laryngeal carcinomas , treatment modalities have evolved over the years : total laryngectomy ( tle ) with postoperative rt has been replaced largely by organ - preservation strategies . 
 in the pivotal va trial [ 3 ] , it was demonstrated that neo - adjuvant chemotherapy followed by rt in responding patients was equal to tle in terms of overall survival . 
 more recently , the rtog 91 - 11 trial [ 4 , 5 ] proved that concurrent radiochemotherapy ( rcht ) led to higher larynx - preservation rates than either standard - fractionated rt alone or the regimen using induction chemotherapy followed by rt . 
in the march meta - analysis , it was shown that altered - fractionated rt was superior to standard - fractionated rt for all sites of hnscc including the larynx [ 6 ] for both accelerated fractionated rt ( af - rt ) and hyperfractionated rt ( hf - rt ) , especially for younger patients ( < 50 years ) and in 834 | strahlentherapieundonkologie102013 good general condition both in terms of local control and survival . the argument for upfront non - surgical and organ - preserving treatment modalities ( i.e. , rt or rcht ) has always been that a patient can still be salvaged with surgery ( tle ) in case of local relapse , although the rate of surgical complications after rt might by higher [ 7 ]  . the aim of this cohort study was to analyze our results regarding the treatment of laryngeal cancers , using definitive primary radiation . 
 in particular for locally advanced laryngeal carcinomas , we investigated the success rates of salvage therapy by studying the effects of locoregional relapse on ultimate locoregional control and overall survival . methods and material patient population for the purpose of this study , we selected from our institutional database 732 consecutive patients treated between january 2000 and december 2011 for laryngeal squamous cell carcinoma . 
excluded from the current analysis were patients treated with primary surgery with or without postoperative radiotherapy ( n = 144 ) , with radiation and planned additional neck surgery ( n = 2 ) , with the arcon ( accelerated radiotherapy , carbogen breathing , and nicotinamide [ 8 ] ) regimen ( n = 14 ) , and with chemoradiation schedules including concurrent , induction , and / or adjuvant regimens ( n = 17 )  . 
in addition , patients with previous head and neck cancer or patients undergoing re - irradiation or receiving treatment elsewhere ( n = 45 ) were also excluded as well as patients with distant metastasis at presentation ( n = 7 ) or patients receiving no or only palliative treatment ( n = 46 )  . 
we also excluded patients with t4b irresectable tumors ( n = 4 ) , since for these patients there were no therapeutic alternatives rather than non - surgical therapy and no surgical salvage options in case of recurrence after definitive in the present analysis , 435 ct1ct4a laryngeal carcinoma patients were included , treated with definitive primary radiation alone between january 2000 and december 2011 . 
this retrospective analysis was approved by the institutional review board ( no.120614 / 03 - intern - 6850 )  . initial evaluation and staging were performed according to national guidelines , including physical examination , panendoscopy under general anesthesia with biopsy and histopathological evaluation of the tumor , computed tomography ( ct ) scan of the head and neck , ultrasonography of the neck ( if necessary with fine needle aspiration cytology ) , and chest x - ray . 
patients with ct4 laryngeal carcinoma were regarded as candidates for primary radiation treatment , if the larynx was clinically judged to remain functional in terms of speech and swallowing after therapy . radiotherapy treatment all patients were treated with a continuous course of radiotherapy delivered by 46 mv linear accelerators . 
since 2004 , all head and neck cancer patients ( excluding t1 glottic cancer ) underwent 18f - fdgpet - ct scan in the immobilization mask for treatment planning . patients were treated with fractionation schedules in line with the state - ofthe - art practices : early glottic laryngeal cancers ( t1n0 and t2n0 with very limited supraglottic extension only into the base of the sinus morgagni ) in patients 70 years or older were treated locally and received a slightly hypofractionated dose of 60 gy in single daily fractions of 2.40 gy over 5 weeks . 
glottic ct2n0 tumors and ct1n0 supraglottic tumors were treated locally only with af - rt to 68 gy in 34 fractions of 2 gy in an overall treatment strahlentherapieundonkologie102013 | abstract zusammenfassung strahlenther onkol 2013 189 : 834841 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0414 - 2 f.hoeberse.riose.troostp.vandenendek.krossm.lackor.lalisangb.kremerj.dejong definitive radiation therapy for treatment of laryngeal carcinoma . 
for ct34 tumors treated with rt alone , initial local control rates are moderate , and in 60% of recurring cases salvage surgery is attempted , with ultimate local control being achieved in only a subset . 
for voluminous , locally advanced laryngeal tumors , more aggressive treatment modalities should be considered , including upfront laryngectomy or radiochemotherapy . keywords laryngeal carcinoma radiotherapy chemoradiation surgery laryngectomy primre strahlentherapie zur behandlung des larynxkarzinoms . 
die kumulative frequenz von lokalrezidiven hing vom ct - stadium ab : ct1 - tumore 10% , ct2 18% , ct3 23% und ct4 36% ( p < 0 , 001 )  . 
die endgltige lokale kontrolle nach 5 jahren ( einschlielich salvage - behandlung ) betrug jeweils 98 , 98 , 87 und 68% fr ct1 - , ct2 - , ct3 und ct4 - tumoren ( p < 0 , 001 )  . 
fr voluminse , lokal fortgeschrittene larynxkarzinome sollten aggressivere behand lungsmodalitten in erwgung gezogen werden , einschlielich primrer larynxextirpation oder radiochemotherapie . schlsselwrter larynxkarzinom strahlentherapie radiochemotherapie chirurgie laryngektomie time ( ott ) of 3738 days , whereby the first 23 fractions were administered daily , and the remaining 10 fractions twice daily . for the locally advanced and / or nodepositive laryngeal carcinomas , the target volume encompassed the primary laryngeal tumor and the elective bilateral neck nodes of at least level 24 up to 4650 gy . 
the radiation treatment technique evolved over the years : from 2000 onwards patients were treated with a 3d conformal technique using compensators , whereas in 2006 intensity modulated radiation therapy with a simultaneous integrated boost ( imrt - sib ) technique was gradually introduced . statistical analysis prognostic factors evaluated were age , gender , tumor location ( glottic or nonglottic ) , tumor grade , ct stage , cn stage , tnm stage , gtv , and pretreatment he836 | strahlentherapieundonkologie102013 t - status t1 - censored t2 - censored t3 - censored t4 - censored t - status t1 - censored t2 - censored t3 - censored t4 - censored log rank test , p < 0.001 local relapse free survival ( months ) fig . 
the gtv of the primary tumor was measured as contoured in our radiation treatment - planning syste this data was only available in ct3t4 tumors , since for the earlier stages the gtv was not always contoured . 
hemoglobin levels were categorized as lower than the lower limit of normal ( lln ) or equal to / higher than the lln ( 8.5 mmol / l for men , 7.5 mmol / l for women )  . 
age and gtv were analyzed as continuous variables . the endpoints were local relapse - free survival ( lrfs ) , ultimate local control ( lc ) and overall survival ( os ) , calculated from the start of radiotherapy . 
failure of ultimate lc was defined as local recurrent disease and included the results from salvage therapy . a multivariate cox proportional hazard regression analysis was performed to establish factors that independently contributed to treatment outcome . 
analyses were performed using spps ( version 19.0 ; spss inc , chicago , il , usa )  . results patient , tumor , and treatment characteristics the patient , tumor , and treatment characteristics are shown in .tab.1. 
af - rt , considered to be one of the optimal strategies when treating with rt alone , was delivered to 64% of all cases and to 86% of cases with ct3 t4 tumors , with a median ott of 37 days ( range 3357 days )  . 
the 2 and 5 - year rates were 92 and 88% for ct1 tumors , 84 and 78% for ct2 , 71 and 65% for ct3 , and 61 and 51% for ct4 , respectively . salvage surgery for local persistent / recurrent disease was performed in 59 of 78 patients ( 76% )  . 
in the remaining 24% of cases , no salvage was performed due to several reasons including irresectable recurrent disease , worsening general condition of the patient , or patients refusal . 
the 2and 5 - year rates were 99 and 98% for ct1 tumors , 99 and 98% for ct2 , 87 and 87% for ct3 , and 77 and 68% for ct4 tumors , respectively . 
 for the 78 patients who developed local recurrence , the 2and 5 - year ultimate local control rates were 88 and 80% for ct1 tumors , 88 and 88% for ct2 , 55 and 55% for ct3 , and 46 and 26% for ct4 tumors . os was 78% at 2 years and 63% at 5 years for all patients . 
the multivariate hazard ratios , confidence intervals , and significance levels are shown in .tab.3. for lrfs , only higher ct stage prevailed as independent prognostic factor of unfavorable outcome in the multivariate analysis . 
for os , higher ct stage and nodal involvement lost significance in the multivariate analysis and only age ( p = 0.001 ) and pretreatment hemoglobin levels ( p = 0.013 ) remained as independent prognostic factors , in addition to gtv . discussion in this single - center analysis on the results of definitive rt for laryngeal cancer , we have demonstrated that the lrfs rates for ct1ct2 tumors are about 80 90% , and that patients with recurrent disease can be salvaged leading to ultimate local control rates of over 95% . 
however , the initial local control after ( accelerated - fractionated ) rt for locally advanced tumors is less favorable with 5 - year local relapse - free survival rates of 65 and 51% for ct3 and ct4 tumors , respectively . 
furthermore , not all patients with local relapses received salvage tle : 63% of patients with ct3 tumors underwent this procedure and 57% of patients with ct4 tumors , indicating that only in about 6 / 10 patients an attempt is made for salvage surgery after initial organ - preserving rt . 
we also showed that patients with locally recurrent disease have worse overall survival compared to patients with initial disease control , which mayat least partially be explained by the fact that salvage therapies can be unsuccessful . 
2 outcome by ct stage 5 - yearlocal relapse - freesurvival ( % ) allpatients curative treatment oflocalrelapse ( % ) 5 - yearultimatelocal control allpatients withlocal 5 - yearultimatelocal control ap values from log rank testing , comparing overall survival for patients with and without local relapse . relapse 5 - year overall survival nolocal relapse 5 - yearoverallsurvival withlocal relapsea 64 ( p = n.s. ) 74 ( p = n.s. ) 27 ( p = 0.07 ) 16 ( p = 0.002 ) rates for ct1 tumors of approximately 80 90% [ 9 ] and 7585% for ct2 tumors [ 10 ]  . for patients with ct3ct4 tumors , the local relapse - free survival rate equals the larynx preservation endpoint used in other studies because in case of recurrent disease tle was performed . 
 [ 4 ] demonstrated larynx preservation rates at 2 years of 70% for standard fractionated rt alone , 75% for induction chemotherapy followed by rt , and 88% for treatment with concurrent rcht . 
this appears less favorable , although it has to be recognized that in the rtog 9111 trial strict selection criteria were applied , patients had to be eligible for rcht , and ct2 tumors were included ( about 10% )  . 
on the other hand , patients with large volume ct4 disease , defined as extension through thyroid cartilage or more than 1 cm involvement of the base of tongue were excluded from the rtog 9111 trial . 
in our series , patients with extensive cartilage involvement and / or extralaryngeal growth were discussed in the multidisciplinary head and neck tumor board and regarded as candidates for organ preserving rt when the larynx was judged as functional after rt . 
because of the retrospective study design , we were unable to investigate whether extensive thyroid cartilage involvement and / or extra - laryngeal growth were responsible for the majority of local recurrences . in 2006 , the asco guidelines on the treatment of laryngeal cancer stated that evidence supported larynx preservation approaches for appropriately selected patients without compromised survival [ 11 ]  . 
 [ 13 ] found lower survival rates after rcht compared to tle in a national hospital - based cancer registry study on over 7000 patients , suggesting that the findings of clinical trials with highly selected patients might not be applicable to the broader population . 
for stage iii patients in both series , there was no difference between surgical therapy and rcht , but rcht was superior to rt alone [ 13 , 14 ]  . 
from the above , it can be concluded that broad population - wide application of organ - preservation strategies ( rt / concurrent rcht ) for unselected locally advanced larynx cancer appears to compromise survival rates . the goal of nonsurgical therapies for advanced laryngeal cancer is organ and function preservation . 
 the likelihood of severe swallowing complications defined as prolonged feeding tube dependency and aspiration is associated with extensive laryngeal cartilage destruction and tumor extension beyond the larynx into the soft tissues of the neck [ 15 , 16 ]  . 
similar to findings in our present study , gtv is one of the main determinants associated with worse local control not only after radiation as single treatment modality [ 17 ] but also after rcht [ 18 , 19 ]  . 
therefore , in terms of patient selection , individuals with bulky laryngeal tumors , extensive laryngeal cartilage destruction and tumor extension beyond the larynx into the soft tissues of the neck should probably not be offered organ preservation strategies as the first treatment option . the question remains which treatment strategy is most successful if one chooses organ preservation [ 20 ] ? there is level 1 evidence for locally advanced laryngeal carcinoma favoring concurrent rcht [ 4 , 5 ]  . 
in a recent retrospective series from rotterdam [ 19 ] on ct3 larynx cancer , it was also demonstrated that concurrent rcht was superior to af - rt alone in terms of local control . 
in the recent gortec 99 - 02 randomized trial [ 21 ] , it was shown that progression - free survival after conventional rcht was superior to a very accelerated rt regimen , delivering 6264 gy in 2223 days . 
furthermore , the addition of standard cisplatinbased chemotherapy to af - rt did not improve outcome compared to conventional rcht . for the future , we anticipate that the clinical decision making for an individual patient will become more difficult as knowledge regarding predictive and prognostic factors grows [ 22 , 23 ]  . 
because the number of factors to take into account is larger than a clinician can handle , we will need the support of nomograms generating outcome predictions based on the characteristics of the individual patient . 
egelmeer ag , velazquez er , de jong jm et al ( 2010 ) development and validation of a nomogram for prediction of survival and local control in laryngeal carcinoma patients treated with radiotherapy alone : a cohort study based on 994 patients . 
de jong state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . literatur kommentiert strahlenther onkol 2013 189 : 899901 doi 10.1007 / s00066 - 013 - 0425 - z online publiziert : 22 . 
august 2013 springer - verlag berlin heidelberg 2013 v.strnad1r.sauer1p.niehoff2 1 strahlenklinik , universittstklinikum erlangen 2 klinik fr strahlentherapie , kliniken der stadt kln bewertungder ( ballon - ) brachytherapiezur teilbrustbestrahlungbeim mammakarzinomanhand aktuellermetanalysen originalbeitrge smith gl , xu y , buchholz ta et al ( 2012 ) association between treatment with brachytherapy vs whole - breast irradiation and subsequent mastectomy , complications , and survival among older women with invasive breast cancer . 
jama 307 : 18271837 presley cj , soulos pr , herrin j et al ( 2012 ) patterns of use and short - term complications of breast brachytherapy in the national medicare population from 20082009 . 
aus der medicare - abrechnungsdatenbank wurden patientinnen mit mammakarzinom , die lter als 66 jahre waren und postoperativ bestrahlt worden waren , selektiert und deren daten verglichen : patientinnen mit brachytherapie ( bt ) mit oder ohne konventionelle strahlentherapie gegenber patientinnen mit nur einer konventionellen ganzbrust - strahlentherapie ( wbi )  . 
 [ 5 ] wurden bei 34 , 3% der patienten mit bt komplikationen kodiert , verglichen mit 27 , 3% nach wbi ( p < 0 , 001 )  . 
im 5 - jahresgesamt berleben gibt es keinen unterschied . kommentar die hier kommentierten verffentlichungen [ 5 , 9 ] haben bereits vor monaten fr kontroverse diskussionen und kritische anfragen von nicht - radioonkologen gesorgt . 
 eine weitere entscheidende limitierung der aussagekraft beider arbeiten ist der unglaubliche methodische ansatz der autoren , nebenwirkungen eines therapeutischen verfahrens retrospektiv anhand von abrechnungsziffern gegenber den krankenkassen erheben zu wollen . 
was soll man darunter verstehen ? in den prospektiven phaseiiund - iii - studien mit der apbi in europa [ 11 , 12 ] wird lediglich ber infektionsraten in der grenordnung 35% berichtet . 
cuttino lw , white jr , rabinovitch r et al ( 2012 ) accelerated partial - breast irradiation : trial by media or by science ? int j radiat oncol biol phys 83 : 10751077 2 . 
hannoun - levi jm , gourgou - bourgade s , belkacemi y et al ( 2013 ) gerico - 03 phase ii trial of accelerated and partial breast irradiation in elderly women : feasibility , reproducibility and impact on functional status . 
niehoff p , polgr c , ostertag h et al ( 2006 ) clinical experience with the mammosite radiation therapy system for brachytherapy of breast cancer : results from an international phase ii trial . 
presley cj , soulos pr , herrin j et al ( 2012 ) patterns of use and short - term complications of breast brachytherapy in the national medicare population from 20082009 . 
polgr c , major t , fodor j et al ( 2011 ) accelerated partial - breast irradiation using high - dose - rate interstitial brachytherapy : 12 - year update of a prospective clinical study . 
polgr c , fodor j , major t et al ( 2007 ) breast - conserving treatment with partial or whole breast irradiation for low - risk invasive breast carcinoma five - year results of a randomized trial . 
polgr c , van limbergen e , ptter r et al ( 2010 ) gec - estro breast cancer working group patient selection for accelerated partial - breast irradiation ( apbi ) after breast - conserving surgery : recommendations of the groupe europen de curiethrapie - european society for therapeutic radiology and oncology ( gec - estro ) breast cancer working group based on clinical evidence . 
smith gl , xu y , buchholz ta et al ( 2012 ) association between treatment with brachytherapy vs whole - breast irradiation and subsequent mastectomy , complications , and survival among older women with invasive breast cancer . 
strnad v , hildebrandt g , ptter r et al ( 2011 ) accelerated partial breast irradiation : 5 - year results of the german - austrian multicenter phase ii - trial using interstitial multicatheter brachytherapy alone after breast conserving surgery . 
vicini f , beitsch p , quiet c et al ( 2011 ) five - year analysis of treatment efficacy and cosmesis by the american society of breast surgeons mammosite breast brachytherapy registry trial in patients treat ed with accelerated partial breast irradiation . 
husain za et al ( 2011 ) accelerated partial breast irradiation via brachytherapy : a patterns - of - care analysis with astro consensus statement groupings brachytherapy 10 : 479485 strahlentherapieundonkologie102013 | original article strahlenther onkol 2013 189 : 867873 doi 10.1007 / s00066 - 013 - 0413 - 3 received : 14 april 2013 accepted : 17 june 2013 published online : 5 september 2013 the autor ( s ) 2013 . 
this article is published with open access at link.springer.com advanced stage head and neck cancer ( hnc ) is known for generally unfavorable outcome with only ~4050% 3 - year overall survival [ 1 , 2 , 3 ]  . 
 in addition , the inor exclusion of very advanced ct4 any nm0 into curatively aimed treatment regimens remains quite subjective . the aim of this analysis was to further stratify ct4 stage squamous cell hnc disease using volumetric staging . 
overall survival ( os ) , disease - free survival ( dfs ) , locoregional control ( lrc ) , and distant metastasis - free survival ( dmfs ) rates were calculated using kaplanmeier curves . 
demographic data and tumor characteristics are listed in .tab.1. all patients underwent modulated radiation therapy using simultaneously integrated boost techniques [ sib - imrt / sib - volumetric modulated arc therapy ( sib - vmat ) ]  . 
in 84% , concomitant cisplatin chemotherapy ( 40 mg / m2 / radiation week ) or cetuximab ( loading dose 400 mg / m2 , followed by concomitant doses of 2250 mg / m2 / radiation week ) was administered . 
in 36 patients with very advanced disease of questionably curable stage , tpf ( docetaxel , cis platin , 5 - fluorouracil ) - based induction chemotherapy was given as a decision aid to add or not curatively intended radiation . 
the remaining 16% of patients were treated with radiation only because of age or substantial comorbidity . all gtvs were contoured or reviewed by at least one of the authors on all relevant axial computerized images without using interpolation ; in most cases the contouring was also reviewed by a third staff physician . 
1 7 overall survival rates of 201 ct4 patients staged by total tumor volume ( ml ) > 130ml overall survival rates ( os ) p < 0.0001 months strahlentherapieundonkologie102013 | original article tab . 
1 patient and tumor characteristics parameters patients ( n ) gender ( female : male ) meanage ( range ) mean / medianfolllow - up ( range ) histology diagnosis nstage totalgrosstumorvolume ( tgtv ) concomitantsystemic therapy 25% : 75% 62 ( 3891 ) years 31 / 23 ( 1116 ) months 116 ( 58% ) 42 ( 21% ) 24 ( 12% ) 19 ( 9% ) 43 ( 21% ) 61 ( 30% ) 88 ( 44% ) 9 ( 5% ) 64 ml ( 7216 ) 15 ( 7% ) 108 ( 54% ) 62 ( 31% ) 16 ( 8% ) 31 ( 15% ) 112 ( 56% ) 25 ( 12% ) 33 ( 16% ) squamous cell carcinoma mesopharynx hypopharynx oral cavity larynx n12b mean none cisplatin only cetuximab only cisplatin switched to cetuximab range 115 ml 1670 ml 71130 ml > 30 ml inductionchemotherapy 36 ( 17% ) tab . 
a detailed description of the applied sib modulated techniques and contouring of gross tumor volume ( gtv ) and planning target volumes ( ptvs ) has formerly been published [ 7 ]  . 
 in several patients with very large gtvs , dose compromises were performed delivering 6668 gy to the boost volume , while the 70 gy dose volume was limited to the gtv . statistical analysis statistical calculations were performed using the statistics program implemented in statview ( version 4.5 ; sas institute , cary , nc , usa )  . 
the volumetric system itself is considered robust with respect to interobserver gtv contouring , as its cut offs values differ markedly ( 15 ml / 70 ml / 130 ml ) [ 4 , 7 ]  . 
the potential benefit of the assessed stratification lays in its more precise prediction of disease control in irradiated ct4 patient cohorts , and therefore more accurate characterization of ct4 cohorts for intercenter comparison purposes . a weakness of this study is its retrospective stratification approach , which however applied a prospectively tested staging system [ 4 , 5 , 6 , 7 ]  . 
four [ 17 , 18 , 20 , 25 ] of the 31 listed reports were based on two or three cut - off values , our abstract zusammenfassung strahlenther onkol 2013 189 : 867873 the autor ( s ) 2013 . 
between january 2002 and january 2013 , a total of 201 ct4 stage squamous cell cancer ( scc ) hnc patients referred to our center for curative definitive radiation were consecutively irradiated . 
total gross tumor volumes ( tgtv : primary + nodal tumor volume ) of all patients have retrospectively been stratified using a prospectively evaluated volumetric staging system which bases on 3 cut - offs ( 15 / 70 / 130 ml ) , translating into 4 prognostic subgroups [ v1 : 115 ml ( n = 15 ) , v2 : 1670 ml ( 108 ) , v3 : 71130 ml ( 62 ) , v4 : > 130 ml ( 16 ) ]  . 
volumetric staging allowed a highly statistically significant stratification of ct4 hnc stages into prognostic subgroups , which offers the chance of better intercenter comparability of irradiated advanced stage hnc cohorts . keywords volumetric staging ct4 stage tumors head and neck neoplasms neoplasm staging prognosis volumetrische stratifizierung von kopf - hals - tumoren im ct4 - stadium zusammenfassung hintergrund . 
 das gesamttumorvolumen ( tgtv : primrtumor + lymphknotenmetastasen ) aller patienten wurde retrospektiv mittels eines prospektiv getesteten volumetrischen staging - systems mit 3 schnittwerten ( 15 / 70 / 130 ml ) stratifiziert , was zu 4 prognostischen subgruppen fhrt [ v1 : 115 ml ( n = 15 ) , v2 : 16 70 ml ( n = 108 ) , v3 : 71130 ml ( n = 62 ) , v4 : > 130 ml ( n = 16 ) ]  . 
volumetrisches staging erlaubte eine statistisch hochsignifikante stratifizierung in prognostisch unterschiedliche untergruppen , was eine bessere vergleichbarkeit von resultaten verschiede ner zentren nach primrer intensittsmodulierter strahlentherapie ( imrt ) von ct4 kht ermglichte . schlsselwrter volumetrisches staging ct4 - tumorstadium kopf - hals - tumore tumorstaging prognose strahlentherapieundonkologie102013 | original article 870 | strahlentherapieundonkologie102013 strahlentherapieundonkologie102013 | original article own system included . 
glanzmann state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . open access this article is distributed under the terms of the creative commons attribution license which permits any use , distribution , and reproduction in any medium , provided the original author ( s ) and the source are credited . literatur kommentiert strahlenther onkol 2013 189 : 902903 doi 10.1007 / s00066 - 013 - 0417 - z online publiziert : 16 . 
beobachtete erkrankungen im vergleich zur erwarteten hufigkeit , in einer normalpopulation ohne brustkrebs und mittels multivariatem cox - regressionsmodell berechnet , um die hazard ratio ( hr ) bestrahlter frauen ( rt - kollektiv ) unter bercksichtigung des alters bei diagnose und der systemtherapie im vergleich zu nichtbestrahlten frauen zu ermitteln . 
es traten insgesamt 2358 zweitmalignome ( auer mammakarzinome ) auf , davon bei bestrahlten frauen 226 flle ( 191 erwartete ) im rt - feld oder dessen nachbarschaft , am hufigsten bronchialkarzinome . 
die hr fr bestrahlte frauen lag bei 1 , 34 ( 95%ci 1 , 111 , 61 ) gegenber nichtbestrahlten , mit einer signifikanten erhhung 10 jahre nach der behandlung . 
beim vergleich mit der reduktion der lokoregionren rezidive durch rt berwiege jedoch der nutzen das risiko . kommentar der medizinische fortschritt hat zwar die heilungsraten onkologischer erkrankungen verbessert , damit jedoch auch die anzahl von zweittumoren erhht ; viele faktoren knnen hierfr urschlich sein [ 7 ]  . 
ein drittel erhht ( hr 1 , 34 ) , jedoch bezieht sich dies auf eine sehr niedrige absolute anzahl von zweittumoren im rt - volumen oder dessen nachbarschainsgesamt entwickelten 226 patientinnen ein zweitmalignom , dies entspricht 0 , 95% des gesamten bestrahlten kollektivs . in bereinstimmung mit der literatur [ 1 , 5 ] traten rt - assoziierte sarkome im thoraxbereich ebenfalls hufiger ( hr 2 , 96 ; 95%ci 1 , 176 , 18 ) auf , insgesamt jedoch nur in 16 fllen . 
leider gibt es in der vorliegenden 902 | strahlentherapieundonkologie102013 studie keine angaben ber die anzahl der raucherinnen ; die autoren schtzen den anteil rauchender dninnen in den 1980er jahren jedoch auf etwa 45% . 
aus dieser beobachtung wurde sogar die empfehlung abgeleitet , raucherinnen explizit ber dieses zustzliche risiko aufzuklren [ 4 ]  . zwei drittel waren jnger als 60 jahre , bei nichtbestrahlten nur etwa die hlfte . 
hingegen betrug bei den jngeren frauen die erwartete tumorinzidenz nur 191 , dies ergibt im vergleich mit den beobachteten 226 zweittumoren eine sir von 1 , 18 . ein weiterer unterschied zwischen den beiden kollektiven bestand bei der adjuvanten systemtherapie . 
interessanterweise stieg die hr fr rt - assoziierte tumoren auf 1 , 63 ( 95% ci 1 , 03 2 , 59 ) fr patientinnen , die zustzlich zur rt eine chemotherapie erhalten hatten . geht man davon aus , dass eine von 200 bestrahlten frauen potentiell an einem radiogenen zweittumor erkrankt , so liefert dies sicher die motivation , durch kontinuierliche verbesserung der rt - technik die dosis am normalgewebe noch weiter zu minimieren . 
so wurde in der jngsten metaanalyse der ebctcg ( early breast cancer trialists collaborative group ; [ 2 ] ) durch die rt nach brusterhaltender operation die rezidivrate halbiert und die tumorbedingte sterblichkeit um ein sechstel reduziert . 
berrington de gonzalez a , gilbert e , curtis r et al ( 2013 ) second solid cancers after radiation therapy : a systematic review of the epidemiologic studies of the radiation dose - response relationship . 
early breast cancer trialists collaborative group ( ebctcg ) , darby s , mcgale p , correa c et al ( 2011 ) effect of radiotherapy after breast - conserving surgery on 10 - year recurrence and 15 - year breast cancer death : meta - analysis of individual patient data for 10 , 801 women in 17 randomised trials . 
grantzau t , mellemkjaer l , overgaard j ( 2013 ) second primary cancers after adjuvant radiotherapy in early breast cancer patients : a national population based study under the danish breast cancer cooperative group ( dbcg )  . 
nestle - krmling c , blke e , budach w et al ( 2011 ) hemangiosarcoma after breast - conserving therapy of breast cancer : report of four cases with molecular genetic daignosis and literature review . 
august 2013 springer - verlag berlin heidelberg 2013 m.baumann klinik fr strahlentherapie und radioonkologie und oncoray - zentrum fr medizinische strahlenforschung und onkologie , universittsklinikum carl gustav carus an der technischen universitt dresden zumgedenkenan prof.dr.kianang der optimierung von dosis und fraktionierungskonzepten ber die radiochemotherapie bis zur einfhrung der ersten molekularen , wirksamen substanz , cetuximab , in die radioonkologie reichten . 
fest mit seinem namen verbunden sind unsere heutigen kenntnisse zur strahlentoleranz und erholungsfhigkeit des rckenmarks , der nachweis der relativen strahlenempfindlichkeit hpv - positiver plattenepithelkarzinome des kopf - hals - bereichs und ein groes spektrum von untersuchungen zum spezifischen einsatz molekular gerichteter substanzen in kombination mit bestrahlung . 
fr seine herausragenden leistungen in der radioonkologischen forschung wurde kian ang mit den wichtigsten wissenschaftspreisen unseres fachgebiets , darunter die regaudgold - medal der estro und die astrogold - medal , ausgezeichnet . zur europischen und deutschen radioonkologie hatte kian ang auch aus den usa heraus ausgesprochen enge und freundschaftliche bindungen . 
als mitglied einer reihe wissenschaftlicher beratungsgremien war es hufig kian ang , der mit seiner reputation vertreter anderer onkologischer disziplinen und drittmittelgeber davon berzeugen konnte , wie wesentlich die radioonkologische forschung im kontext der allgemeinen krebsforschung ist . 
viele junge strahlentherapeuten und strahlenbiologen bekamen durch einladung von kian ang die gelegenheit am md anderson cancer center klinische hospitationen und forschungsaufenthalte durchzufhren stimulierende eindrcke die spter an den heimatinstitutionen forschung und klinische ttigkeit enorm bereicherten . 
es ist sicher nicht bertrieben , zu sagen , dass kian ang eine tragende brcke der radioonkologie ber den atlantik war . fr viele von uns war kian ang aber nicht nur ein herausragender vertreter unseres fachs , sondern auch ein enger persnlicher freund mit viel witz , charme , verbindlichkeit und ausgeprgter bodenhaftung . 
er liebte reisen zusammen mit seinen freunden , tennis , schnelle autos , musik und abendliche unterhaltungen bei einem guten glas wein . kian ang hinterlsst seine ehefrau sunny und seine kinder angelica mit ramzi und dimitri mit kimberly . 
kian ang war einer der weltweit fhrenden radioonkologen und krebsforscher und seit 2008 ehrenmitglied der degro . kian ang wurde in china geboren und wuchs in indonesien auf , bevor er medizin an der katholischen universitt in leuven , belgien , studierte . 
im anschluss an die weiterbildung folgte er einem ruf an das md anderson cancer center der university of texas in houston , wo er die letzten 29 jahre als kliniker und forscher arbeitete . 
zuletzt hatte er den gilbert - fletcher - distinguishedmemorial - lehrstuhl inne . kian ang war zweifelsohne ber die letzten jahrzehnte der international fhrende radioonkologe auf dem gebiet der kopf - hals - tumoren . 
hier hat er bahnbrechende klinische studien initiiert , die von original article strahlenther onkol 2013 189 : 825833 doi 10.1007 / s00066 - 013 - 0437 - 8 published online : 5 september 2013 the autor ( s ) 2013 . 
clara hospital , basel 9 university hospital tbingen 10 university hospital mannheim 11 university hospital erlangen degropractical guidelines : radiotherapy ofbreastcanceri radiotherapyfollowingbreastconserving therapyforinvasivebreastcancer the evidence for the benefits of postoperative radiotherapy to the whole breast ( wbi ) has been further substantiated since the last recommendations on the basis of updated meta - analyses , systematic reviews , and randomized controlled trials . 
a total of 10 , 801 patients with pt12 tumors were recorded : the majority of whom ( n = 7287 ) were node negative , 1050 were node positive , and in 2464 patients the nodal status was unknown . the effect of radiotherapy on 10 - year recurrences of any type and their relation to the 15 - year breast cancer death rates were studied in correlation to various prognostic parameters and treatment characteristics . 
in contrast , the absolute benefit from radiotherapy substantially depended on the patient characteristics in terms of prognostic factors . comments and conclusion of the degro panel f this important large - scale metaanaly sis impressively confirmed that prevention of locoregional recurrences by postoperative radiotherapy translates into improved survival . radiotherapy in the elderly the indication for wbi for women over 70 years with low risk tumors is an ongoing issue of international debate with partially antipodal interpretations [ 77 ]  . 
the updated recommendations of the european society of breast cancer specialists ( eusoma ) [ 14 ] and the latest german s3 guidelines define no age limitation for postoperative rt for healthy elderly patients . 
albeit the absolute benefit of adjuvant treatment is smaller in advanced age , the proportional risk reduction by half is constantly observed [ 3 , 17 , 22 , 24 , 27 , 41 , 66 , 68 , 69 , 75 , 84 , 88 , 89 , 93 , 94 , 96 ]  . 
therefore , omission of rt in patients of advanced age even with favorable prognostic factors ( pn0 , er - positive , low grade ) should only be considered in presence of comorbidities with a substantial reduction of life expectancy . 
this decision has to be properly documented [ 9 , 35 , 38 , 75 , 81 , 85 ]  . comments and conclusion of the degro panel f chronological age alone is not an appropriate criterion for decision against or in favor of adjuvant treatment . f no subgroup of elderly patients has yet been identified that did not profit from rt in terms of local control . f the degro breast cancer expert panel explicitly discourages determination of a certain age for the omission of postoperative rt in healthy elderly women with low risk breast cancer . f in frail elderly women omission of postoperative rt should be individually decided on the basis of geriatric assessment . tumor bed boost statementrt2d [ 74 ] a local dose escalation ( boost ) to the tumor bed reduces local recurrence rates without demonstrating a survival advantage . 
the beneficial impact of an additional 16 gy boost dose to the tumor bed by either fractionated external beam treatment or brachytherapy was corroborated in a follow - up analysis of the eortc trial data , where local recurrence rates were consistently shown to be halved in every patients age group compared to wbi alone [ 4 , 8 , 67 ]  . 
in this trial , higher local control rates achieved by boost radiotherapy did not translate into better survival . annual recurrence rates have decreased steadily during the last 10 years , due to quality progress in diagnostics , surgery , pathologic work up , frequent use of modern systemic therapy , and particularly , rapid innovation in radiotherapy . 
 interim reports of the ongoing prospective young boost trial ( nct0021212 ) or closed eliot trial ( wbi group ) [ 62 ] describe low recurrence rates of estimated 0.5% after 4 years ( age group < 50 years ) and 0.7% after 5 years , respectively [ 7 , 65 ] , pointing at the value of further dose augmentation in the tumor bed . the following techniques are used for boost treatment : external beam photons abstract zusammenfassung strahlenther onkol 2013 189 : 825833 the autor ( s ) 2013 . 
the aim of the present paper is to update the practical guidelines for postoperative adjuvant radiotherapy of breast cancer published in 2007 by the breast cancer expert panel of the german society for radiooncology ( deutsche gesellschaft fr radioonkologie , degro )  . 
a comprehensive survey of the literature concerning radiotherapy following breast conserving therapy ( bct ) was performed using the search terms breast cancer , radiotherapy , and breast conserving therapy . 
data from lately published metaanalyses , recent randomized trials , and guidelines of international breast cancer socie ties , yielding new aspects compared to 2007 , provided the basis for defining recommendations according to the criteria of evidencebased medicine . 
after breast conserving surgery , no subgroup even in low risk patients has yet been identified for whom radiotherapy can be safely omitted without compromising local control and , hence , cancer - specific survival . 
in most patients , this translates into an overall survival benefit . keywords breast conserving therapy whole breast irradiation partial breast radiotherapy boost radiotherapy fractionation degro - leitlinien fr die radiotherapie des mammakarzinoms i . 
die degro - expertengruppe mammakarzinom fhrte eine literaturrecherche aktueller klinisch kontrollierter studien , systematischer reviews und metaanalysen sowie leitlinien internationaler gesellschaften im hinblick auf neue aspekte gegenber 2007 durch , wobei sie sich an den kriterien evidenzbasierter medizin orientierte . 
von den zahlreichen publikationen , die im intervall seit den letzten degro - empfehlungen erschienen sind , stellt der rezente ebctcg - bericht aus dem jahr 2011 die bislang zahlenmig grte metaanalyse dar . 
nach brusterhaltender operation invasiver mammakarzinome konnte selbst bei niedrigrisiko - patientinnen bislang keine subgruppe identifiziert werden , bei der auf eine nachfolgende radiotherapie verzichtetet werden kann , ohne die lokale tumorkontrolle und in weiterer folge das krebsspezifische berleben zu beeintrchtigen . 
berdies resultiert bei den meisten patientinnen durch die bestrahlung ein berlebensvorteil . schlsselwrter brusterhaltende therapie ganzbrustbestrahlung partialbrustbestrahlung boostbestrahlung fraktionierung strahlentherapieundonkologie102013 | original article and electrons , interstitial and endoluminal brachytherapy , and intraoperative radiotherapy with electrons ( ioert ) or in selected cases with low - energy photons ( kv )  . 
a subgroup analysis of the eortc boost trial [ 67 ] assessed the outcome of 251 patients with r1 resection who were randomized to receive either a 10 gy or a 26 gy boost . 
extrapo lating these results on patients with complete resection , it seems justifiable to use a 10 gy boost , even though data are less valid than for 16 gy [ 74 ]  . 
in a european survey about current practice in breast rt , one third of the institutions used a 10 gy boost dose [ 90 ]  . in recent years , an additional focus of boost therapy has been placed on accelerated dose integration during the course of wbi , which is possible using different approaches : during simultaneously integrated boosts ( sib , concomitant boost ) , the boost dose is administered by daily zonal dose augmentations [ 32 , 78 ]  . 
this principle was exploited in whole breast radiotherapy ( wbi ) as well as accelerated partial breast irradiation ( apbi ) including intraoperative procedures ( iort ) and sib techniques [ 78 ]  . four randomized clinical trials ( start a , start b , owen , whelan ) investigated hypofractionated wbi schedules ( 39 42.9 gy in single fractions of 2.63.3 gy ) for iso - effectiveness compared to normofractionation ( 50 gy in single fractions of 2 gy )  . 
in summary , 7095 patients were treated within these trials , 89.8% with tumors < 3 cm , 79% node negative , 87% had small or medium - sized breasts . 
the 10 - year followup data were presented at the sabcs 2012 , corroborating the previous reports [ 39 ]  . the canadian trial also confirms these findings in long - term analyses [ 95 ] , with a possible exception of high - graded tumors , where hypofractionated schedules resulted in lower tumor control rates . 
to date , ultrashort wbi courses are tested in the fast trial ( faster radiotherapy for breast cancer ) , where a 5 - fraction schedule of whole breast radiotherapy is compared against the uk standard 15 - fraction regimen in terms of local cancer control and late adverse effects [ 2 ]  . cosmesis after 5 years was evaluated in about half of the patients . 
in a cochrane meta - analysis [ 43 ] , the authors stated that the findings of their review provided reassurance that offering hf to carefully selected patients is unlikely to be detrimental in terms of local control , breast appearance , survival , or late radiation breast toxicity for women with small to medium breasts , aged greater than 50 years , with small , node - negative tumors . 
in accordance with these concerns , the astro consensus and the german guidelines additionally recommend to refrain from hf when a homogenous dose is not achievable [ 74 , 80 ]  . moreover , the impact of hf on late cardiac toxicity is not yet evaluated beyond 10 years [ 57 , 95 ] ; as the latency for clinical manifestation of cardiovascular effects is 15 years or longer , hf might turn out to be critical in cases of relevant dose exposure to the heart , especially in women with a longer life expectancy . conventional fractionation with a total dose of 5050.4 gy in single doses of 1.8 2 gy is still regarded as standard in all current guidelines [ 9 , 56 , 74 ]  . 
divergence exists concerning the appraisal of hypofractionation as a routinely applicable alternative [ 9 , 74 ] or as an option restricted to selected patients [ 74 , 80 ]  . unresolved issues address the effectiveness in selective histologic subtypes ( e.g. , g3 ) , a potentially worse cosmetic outcome in ( very ) large breasts and late normal tissue tolerance , especially in combination with modern chemotherapy regimen . 
radiobiological models and first clinical results seem to predict inferior outcome for the ongoing ultrashort wbi trials [ 2 ]  . comments and conclusion of the degro panel f normofractionated wbi plus sequential boost remains standard . f hypofractionated wbi with single doses up to 2.7 gy in 1516 fractions to total doses of 4042 gy is an option for older women with pt12 pn0 tumors who need no chemotherapy . 
the additional use of a sequential boost is possible . f hypofractionated wbi plus boost either by sib or by hypofractionated sequential application is discouraged outside clinical trials . for wbi , homogeneity requirements in dose distribution as described by the icru reports 50 and 62 are usually achieved by conformally shaped tangential wedged field techniques , mostly with photons at energies of 48 mv . 
for larger breasts , higher energies and / or intensity modulation ( imrt ) within the tangential beams may be appropriate to fulfill the minimum homogeneity criteria [ 6 , 42 ]  . 
multi - angle imrt may be beneficial for patients with difficult anatomical conditions ( i.e. , funnel chest ) where tangential field arrangements would lead to excessive exposure of oars . 
the use of active breathing control , such as computerassisted breath hold in deep inspiration [ 83 , 99 ] provides another possibility of sparing radiation burden to the lungs and for left - sided tumors also to cardiac structures as it increases the distance between target volume and heart [ 49 ]  . for quality control , correct treatment delivery has to be documented with repeated imaging , mostly by epids or kvbased image guidance , alternatively by optical surface scanning techniques [ 34 ]  . radiotherapy following neoadjuvant chemotherapy and breast conserving surgery targeting , treatment planning , and technique for the wbi individual ct - based 3d planning is mandatory . 
several anatomically - based instruction guidelines have been published for definition of the planning target volume ( ptv ) [ 58 , 73 ] which includes the mammary gland and the adjacent chest wall . 
organs at risk ( oar ) like lung and heart ( in left - sided tumors possibly with delineation of the left anterior coronary artery ) [ 30 , 58 ] are contoured and doses documented in dosevolume histograms ( dvh )  . 
hence , and in the absence of randomized prospective trials , indications for radiotherapy following bcs are not altered by the time sequencing of the systemic medications . a major goal of neoadjuvant chemotherapy in advanced breast cancer cases is to facilitate breast conserving treatment without compromising local control ( lc ) and survival rates . 
omission of surgery resulted in higher lr rates [ 51 ]  . during the last decade , data on lowest locoregional recurrence ( lrr ) rates following postoperative radiotherapy after neoadjuvant ct were provided by two retrospective studies [ 13 , 20 , 21 ]  . 
wbi was performed in conventional fractionation ( 1.82 gy ) up to a total dose of 45 50 gy , followed by a fractionated tumor bed boost with external electrons with doses between 10 and 20 gy . 
at median follow - up times of 60 months , compiled rates ( mean values ) of lrr , ibr , and distant metastasis amounted to 8 , 4.5 , and 19% , respectively . 
in contrast , results of prospective trials are less favorable , reporting mean ibr rates of about 9.6% after a median followup of 68.4 months ( range 29124 months ) [ 15 , 18 , 19 , 31 , 52 , 72 ]  . 
for patients at a lower risk for local recurrence , apbi has been strongly propagated in recent years as it spares treatment time , costs , and allegedly provides less toxicity [ 54 ]  . 
in analogy to boost settings , these methods differ in terms of physical dose distribution and radiobiologic effects , which has to be considered in outcome analyses [ 55 , 59 ]  . cinical evidence so far , only four phase iii randomized trials and one meta - analysis evaluating apbi have been published . 
in the christie hospital trial [ 70 ] , 708 patients were randomized between apbi and wbi , but lacked appropriate target volume definition criteria ; moreover , many patients outside the low - risk group were entered . 
the hungarian trial comparing wbi with apbi using 830 | strahlentherapieundonkologie102013 hdr implants or electrons ( normal fractionation ) was prematurely stopped after recruitment of 258 women with margin - negative , early - stage breast cancers , thus , lacking sufficient sample size [ 64 ]  . 
 a meta - analysis of these phase iii trials was published in 2010 [ 87 ] compared to wbi , apbi was associated with an increased risk for both local [ pooled odds ratio ( or ) 2.15 ; p = 0.001 ] and regional recurrence ( pooled or 3.43 ; p < 0.001 ) , however , not ( yet ) translating into a survival difference ( or 0.91 ; p = 0.55 ) [ 54 ]  . 
orthovoltage iort as apbi strategy was investigated in the targit trial as the fourth published randomized investigation and is discussed below . intraoperative radiotherapy to date , two major full - dose iort studies are promoted : the targit approach using ortovoltage x - rays and the eliot trial , respectively , testing singleshot electron treatment . 
in 2010 , a first interim analysis was published from the targit trial at a median follow - up time of 24.6 months [ 86 ] .the kaplanmeier estimate of local recurrence at 4 years was 1.2% in the apbi arm and 0.95% in the wbi group . 
first results have been presented , alerting a higher ibtr rate in the iort arm [ 62 ] .outside this trial setting , another 1822 patients were treated using the eliot concept [ 92 ]  . 
true local recurrences are presumed to occur between 40 and 65 months after primary treatment [ 16 , 36 ] , out - quadrant relapses even later than that [ 33 ] when wbi was performed . 
sedlmayer declares the following : research cooperation with elektra , study sponsorship and travel reimbursement received from intraop medical . the accompanying manuscript does not include studies on humans or animals . open access this article is distributed under the terms of the creative commons attribution license which permits any use , distribution , and reproduction in any medium , provided the original author ( s ) and the source are credited . literaturkommentiert strahlenther onkol 2013 189 : 904906 doi 10.1007 / s00066 - 013 - 0424 - 0 online publiziert : 22 . 
august 2013 springer - verlag berlin heidelberg 2013 c.petersen klinik fr strahlentherapie und radioonkologie , universittsklinikum hamburg - eppendorf optimalerzeitpunktfrdie operationbeimrektumkarzinom nachneoadjuvanter radiochemotherapie frwelchepatientenwrewartenbesser ? originalbeitrag perez ro , habr - gama a , sao juliao g et al ( 2012 ) optimal timing for assessment of tumor response to neoadjuvant chemoradiation in patients with rectal cancer : do all patients benefit from waiting longer than 6 weeks ? int j radiat oncol biol phys 84 : 11591165 hintergrund . 
das klinische vorgehen , nach abschluss der rct 6 wochen bis zur operation ( op ) zu warten , beruht im wesentlichen auf den erlanger erfahrungen [ 1 ] , die durch die randomisierte lyon - r90 - 01 - studie [ 2 ] besttigt wurden . 
hier hatte das zeitintervall von 6 wochen ein deutlich hheres ma an tumorschrumpfung bewirkt , verglichen mit einem kurzen zeitintervall bis zur op von nur 2 wochen , ohne dass damit das therapieergebnis gefhrdet worden wre . 
es wurden patienten mit karzinomen ct24 / n02 ( staging mittels mrt ) mit einer tumorlokalisation von maximal 7 cm vom analrand ( rigide proktoskopie ) in das programm eingeschlossen . 
die rct bestand aus einer neoadjuvanten rct bis 45 gy mit 1 , 8 gy pro fraktion ( 3 - felder - technik ) , gefolgt von einem boost mit 9 gy ( 1 , 8 gy ) auf die makroskopische tumorausdehnung . 
die simultane chemotherapie erfolgte mit infusionalem 5 - fu ( 425 mg / m2 , 7 tage ) sowie folinsure ( 20 mg / m2 / tag ) an 5 aufeinanderfolgenden tagen in den wochen 1 und 6 . 
patienten , bei denen sich weder bildgebend noch klinisch ein anhalt fr einen residualtumor ergab , wurden im rahmen eines strikten follow - up - protokolls angeboten , auf die ursprnglich geplante operation zu verzichten . 
alle 91 patienten zeigten nach 6 wochen einen suv - abfall , davon 45 patienten ( 49 , 5% ) einen weiteren abfall nach 12 wochen ( good responders ) , whrend 46 ( 50 , 5% ) einen signifikanten anstieg zwischen 6 und 12 wochen zeigten ( bad responders )  . 
nach 6 wochen konnte beim pet / ct anhand der abnahme des frhen ( 1 h ) zum spten ( 3 h ) suv - wert die zugehrigkeit zu den good responders in 67% vorhergesagt werden ( hohe positiv - prdiktive vorhersagekraft )  . 
mglicherweise knnen knftig die therapieentscheidungen , also sowohl die operationsmethode als auch ein aktives weiterbeobachten , von der vernderung des suvmax - werts ( frh / spt ) nach 6 wochen abhngig gemacht werden . kommentar die neoadjuvante langzeit - radiochemotherapie ( 50 , 4 gy mit infusionalem 5 - fu ) gefolgt von einer qualittsgesicherten tiefen anterioren rektumresektion bzw . 
diese neoadjuvante multimodale strategie hat das lokalrezidivrisiko nach 5 und 10 jahren auf unter 10% gesenkt . trotz des etablierten standards gilt es , weitere verbesserungen der behandlung mit neuen strategien zu entwickeln . 
es scheint , als bese dann die aquisition eines frhen und eines spten suvmax - werts bei der pet / ct - untersuchung einen guten prdiktiven vorhersagewert fr die zu erwartende remissionsrate . 
dual time point imaging ( dtpi ) mglicherweise auch das verhltnis zwischen residualen klonogenen tumorzellen und schon eingetretener strahleninduzierter fibrose abgebildet werden knne . pitfalls der studie , wie die autoren auch selbstkritisch in der diskussion anmerken , beziehen sich auf die tatsache , dass nach 3 jahren sowohl das gesamtberleben als auch das krankheitsspezifische berleben bei den good responders und den bad responders nicht signifikant unterschiedlich waren . 
dieses vorgehen minimiert zwar die interobservervariabilitt , lsst aber die frage offen , wie robust die suvmax - werte zuknftig sind unter bercksichtigung unterschiedlicher untersucher und gerte . die arbeitsgruppe um angelita habrgama aus sao paulo bearbeitet schon seit einigen jahren und zwar auch ohne pet / ct die strategie , bei patienten mit einer klinisch kompletten remission nach neoadjuvanter radiochemotherapie erfolgreich auf eine bliche radikaloperation in den ursprnglichen tumorgrenzen zu verzichten . 
nach einem mittleren follow - up von 60 monaten konnten beeindruckende ergebnisse erzielt werden : gesamtberleben nach 5 jahren von 93% und krankheitsspezifisches berleben von 85% [ 3 , 4 ]  . 
 [ 5 ] anhand eines recht kleinen patientenguts , dahingehend , ob patienten mit kompletter klinischer remission nach neoadjuvanter rtc eine wait - and - see policy angeboten werden kann . 
es verwundert somit nicht , dass die krzlich publizierten esmo consensus guidelines for management of patients with colon and rectal cancer [ 6 ] jenseits des standardvorgehens erstmals die mglichkeit erffnen , bei selektionierten patienten nach neoadjuvanter rct unter zuhilfenahme der von valentini et al . 
 [ 7 ] publizierten normograme individuell auf eine operation zu verzichten . fazit auchwenndiehierkommentiertechirurgischearbeitderarbeitsgruppeum angelitahabr - gamaaussaopaulonoch keinerleinderungdesgutetablierten standardisiertenundmultidisziplinren vorgehensbeimrektumkarzinombestrahlentherapieundonkologie102013 | literaturkommentiert wirkt , zeigtsiedoch , dassdiesuchenach neuenbehandlungsalgorithmenweiterhinerforderlichistunderfolgreichsein kann.mglicherweisehelfenunshierzuknftignebenderdezidiertenbildgebung , wiepet / ctodermrt , auchmolekularbiologischeparameter , wiesieim rahmenderstudiendergermanrectal cancerstudygroupuntersuchtwerden , diechirurgischetherapieweiterzuindividualisieren . cordula petersen , hamburg korrespondenzadresse prof.dr.c.petersen klinik fr strahlentherapie und radioonkologie , universittsklinikum hamburg - eppendorf martinistr . 
francois y , nemoz cj , baulieux j et al ( 1999 ) influence of the interval between preoperative radiation therapy and surgery on downstaging and on the rate of sphincter - sparing surgery for rectal cancer : the lyon r90 - 01 randomized trial . 
habr - gama a , perez ro , nadalin w et al ( 2004 ) operative versus nonoperative treatment for stage 0 distal rectal cancer following chemoradiation therapy : long - term results . 
habr - gama a , perez ro , proscurshim i et al ( 2006 ) patterns of failure and survival for nonoperative treatment of stage c0 distal rectal cancer following neoadjuvant chemoradiation therapy . 
valentini v , van stiphout rg , lammering g et al ( 2011 ) nomograms for predicting local recur rence , distant metastases , and overall survival for pa tients with locally advanced rectal cancer on the basis of european randomized clinical trials . 
while anatomic extension of the tumor seems to be essential for the surgical approach , effectiveness of radiotherapy depends on the number of clonogens which are associated with the tumor volume ( tv ) [ 2 , 4 , 9 , 16 ]  . 
tumor volume is not incorporated in the tnm classification for laryngeal carcinoma and its impact on treatment outcome is still not well defined for tumors of this site [ 26 ]  . 
most of the studies that had been published are based on heterogeneous and small groups of patients [ 11 , 13 , 19 , 21 , 23 , 26 , 29 ]  . the purpose of the study is to describe the relationship between tv and other prognostic factors and to determine how tv may influence the outcome of radiotherapy for patients with t2 laryngeal cancer . methods and material records of 160 patients who underwent radiotherapy ( rt ) between 2002 and 2006 for previously untreated t2 laryngeal squamous cell carcinoma at the maria sklodowska - curie memorial cancer center and institute of oncology , gliwice branch , poland , were reviewed . the group consists of 129 ( 80.5% ) men and 31 ( 19.5% ) women with a mean age of 60 years ( range 3982 years )  . 
the tumor was located in the glottis and epiglottis in 82 ( 51% ) and 78 ( 49% ) patients , respectively . patients were immobilized using a commercially available thermoplastic mask that covered the head and neck . 
 volumetric three - dimensional measurements ( cm3 ) of contoured structures were calculated by the varian treatment planning system ( eclipse ) volume algorith only the primary tumor was involved in the tv . 
 no data on m0 and m1 was available in 42 ( 26% ) and 40 ( 25% ) patients , respectively median duration of symptoms ( ds ) prior to rt was 6 months ( range 1101 months )  . 
most of these studies were , however , undersized and heterogeneous , concerning tumor location , stage of disease , and treatment modalities [ 11 , 13 , 19 , 23 , 25 , 26 ]  . the relationship between tv and os was reported mainly for advanced tumors treated with chemoradiotherapy ( crt )  . 
tv thresholds between 28 and 35 cm3 were 862 | strahlentherapieundonkologie102013 found to be significantly related to lc and os [ 5 , 14 , 18 , 26 ] and tv > 70 cm3 was the predictor for distant metastases [ 36 ]  . in this study , the impact of tv on rt outcome was analyzed in a relatively large and homogenous group of patients with laryngeal cancer exclusively . 
 [ 30 ] found striking tv variability with variation exceeding 100% for tnm definitions of t3 head and neck cancer of different locations . t2 laryngeal cancer seems to be adequately defined from a surgical point of view leaving , however , much room for interpretation for radiation oncologists . 
tumor volume ( tv ) is recognized as a prognostic factor of treatment outcome for head and neck tumors but is not routinely included in the treatment decision - making process . 
the routine estimation of tv prior to therapy may be essential in order to select the best treatment option for patients with t2 laryngeal cancer . keywords tumor volume radiotherapy t2 laryngeal cancer glottis epiglottis prognostische bedeutung des tumorvolumens fr das ergebnis der strahlentherapie in patienten mit t2 - kehlkopfkrebs zusammenfassung hintergrund . 
der tv - median war deutlich niedriger in patienten mit glottistumoren ( p < 0 , 0001 ) , im stadium n0 ( p < 0 , 001 ) und histopatologisch differenzierten tumoren ( p = 0 , 01 )  . 
in der univariaten analyse beeinflusste tv signifikant die lokale kontrollrate ( lc ; p = 0 , 02 ) und das gesamtberleben ( os ; p < 0 , 001 )  . 
data are stratified into three groups : less than the first quartile ( tv 0.66 cm3 , solid thin line ) , between the first and third quartile ( 0.66 cm3 < tv 6.69 cm3 , dashed line ) , and greater than the third quartile ( tv > 6.69 cm3 , solid thick line ) in our patients may verify this hypothesis . 
for this , there is a need for an alternative to exclusive rt treatment options for larger tumors despite the same t stage . inclusion of tv data into the tumor classification system may allow a more rational selection of the optimal treatment strategy . 
 moreover , the percent of the decrease in tv after concurrent crt appeared to be a strong predictor of survival [ 20 ]  . a more complex relationship of tv and rt outcome could also be hypothesized . 
 because blood loss occurs to a limited extent in patients with laryngeal cancer and only few of them were anemic in our study ( 5% ) , another link between low hb concentration and tv may exist . 
these cells are likely to be radioresistant so the rt may fail to sterilize the tumor [ 15 ]  . some authors have revealed an association between weight loss or low initial bmi and inferior outcome for patients with head and neck cancer . 
malnutrition frequently increases during treatment causing a wide range of physiological and clinically relevant side effects [ 3 , 6 , 24 , 27 , 33 , 34 ]  . 
in this group of patients such a relationship was not confirmed . the correlation between tv and the risk of nodal metastases was pointed out by other authors for tumors located in oropharynx or hypopharynx [ 7 , 17 , 37 ]  . 
it was also observed that such large epiglottic tumors often present poor histopathological differentiation or shorter duration of symptoms what may indicate more aggressive biology of tumors located in this level of the larynx [ 22 , 28 ]  . the tumor estimation could be performed by various methods , less or more accurately . 
for these relatively small tumors , tv could not be precisely estimated and the evaluation of the tumor was based on the description of the infiltration and the involvement of anatomical structures . 
because 18f - fluorodeoxyglucose ( fdg ) correlates with cellular proliferation and tumor behavior , it is likely that mtv reflects not only tumor bulk but also its biology [ 31 ]  . 
considering tv in addition to the tumor classification system may allow pretherapeutic identification of a patient subgroup that may benefit from intensified treatment strategies , e.g. , combined with rt systemic therapy which seems to be of special importance for epiglottic tumors . false - positive results [ 12 ]  . 
it may be concluded that , although difficult in clinical practice , the use of more methods results in a more precise tv determination . the retrospective character of the present research restricts conclusions that can be drawn from the study . 
 nevertheless , our results confirm the need of multidirectional interpretation of tv as a reliable prognostic indicator of rt outcome even for patients with early laryngeal cancer especially those located in the epiglottis . 
 maciejewski state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . original article strahlenther onkol 2013 189 : 856860 doi 10.1007 / s00066 - 013 - 0377 - 3 received : 28 february 2013 accepted : 6 may 2013 published online : 20 . 
juli 2013 springer - verlag berlin heidelberg 2013 d.rades1n.d.seibold1m.p.gebhard2f.noack2c.thorns2s.e.schild3 1 department of radiation oncology , university of lbeck 2 institute of pathology , university of lbeck 3 department of radiation oncology , mayo clinic scottsdale impactofthehpv - positivity definitionontheprognosticvalue ofhpvstatusinpatientswith locallyadvancedsquamouscell carcinomaoftheheadandneck introduction materials and methods a clear understanding of prognostic factors is important to optimize personalized cancer care . 
human papilloma virus ( hpv ) status has become a focus of clinical research as an etiology and potential prognostic factor for patients with squamous cell carcinoma of the head and neck ( scchn )  . 
however , according to the current literature , higher accuracy regarding hpv status may be achieved if only those tumors that are positive for both hybridization and p16 immunostaining are considered hpv - positive [ 10 ]  . 
therefore , the data from the 170 patients in our previous study have been reanalyzed using an alternative definition of hpv positivity . the data from 170 patients irradiated for locally advanced scchn were re - analyzed with respect to hpv status . 
in our previous study , a tumor was defined as hpv - positive if it showed a positive in situ hybridization result in at least 10% of tumor cells and / or positive p16 immunostaining as a surrogate marker of oncogene activity of the e6 and e7 genes [ 13 ]  . 
 greater accuracy may be achieved if only those tumors that show both a positive in situ hybridization result and positive p16 immunostaining are considered as hpv - positive [ 10 ]  . 
in non - dysplastic epithelium and dysplasia , large numbers of replicated virus episomes are found in the nucleus and easily recognized using chromogenic in situ hybridization ( cish )  . 
the p16 - ink4a antibody ( mouse monoclonal ) for immunohistochemistry ( clone 16p4 / jc2 ) was purchased from biocarta , san diego , ca . squamous - type carcinoma in situ of the uterine cervix in a patient with a known hpv subtype ( hpv - chip type 3.5c , chipron gmbh , berlin , germany ) was used as a positive control . 
prognostic factors found to be significant ( p < 0.05 ) or of borderline significance ( p0.06 ) in the univariate analysis were included in the updated multivariate analyses ( cox proportional hazards model )  . 
the comparison of the previous study [ 9 ] and the current study with respect to the multivariate analyses of lrc , mfs , and os is given in .tab.3. despite novel treatment approaches , the treatment results of locally advanced scchn still need to be improved [ 2 , 11 ]  . 
in our previous study , hpv positivity was an independent predictor for improved lrc and os , strahlentherapieundonkologie102013 | original article abstract zusammenfassung strahlenther onkol 2013 189 : 856860 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0377 - 3 d.radesn.d.seiboldm.p.gebhardf.noackc.thornss.e.schild impact of the hpv - positivity definition on the prognostic value of hpv status in patients with locally advanced squamous cell carcinoma of the head and neck abstract backgroundandpurpose . 
this study reevaluated the prognostic value of hpv status for loco - regional control ( lrc ) , metastases - free survival ( mfs ) , and survival ( os ) in patients with locally advanced squamous cell carcinoma of the head and neck ( scchn )  . 
in the previous study of the same 170 patients , a tumor was defined as hpv - positive if it showed a positive in situ hybridization result in 10% of tumor cells and / or positive p16 immunostaining . 
applying the new definition of hpv positivity , the impact of hpv status on the prognosis of patients irradiated for locally advanced scchn was more prominent than in our previous study and associated with all three investigated endpoints . keywords head - and - neck cancer radiotherapy , prognostic factors hpv status treatment outcomes einfluss der definition der hpv - positivitt auf den prognostischen wert des hpv - status bei patienten mit lokal fortgeschrittenem plattenepithelkarzinom der kopf - hals - region zusammenfassung hintergrundundziel . 
in dieser studie wurde die prognostische bedeutung des hpv - status hinsichtlich lokaler kontrolle ( lrc ) , metastasenfreiem berleben ( mfs ) und gesamtberleben ( os ) bei patienten mit lokal fortgeschrittenem plattenepithelkarzinom der kopf - hals - region ( scchn ) reevaluiert . 
in unserer vorherigen studie mit denselben 170 patienten wurde ein tumor als hpv - positiv definiert , wenn bei der hybridisierung 10% der zellen positiv waren und / oder wenn immunhistochemisch eine p16 - expression nachgewiesen wurde . 
bei anwendung der neuen definition von hpv - positivitt wurde der einfluss des hbv - status auf die prognose von patienten , die aufgrund eines scchn bestrahlt wurden , deutlicher als in der vorherigen studie und mit allen 3 untersuchten endpunkten assoziiert . schlsselwrter kopf - hals - tumoren strahlentherapie , prognosefaktoren hpv - status behandlungsergebnisse but was not significantly associated with mfs [ 13 ]  . 
using the alternative definition of hpv positivity , the impact of hpv status has become more obvious . regarding the other prognostic factors that were significant in the multivariate analyses of the previous study , the current re - analyses revealed the same findings . 
the prognostic value of performance status , tumor stage , and pre - rt hemoglobin levels have already been described [ 1 , 3 , 7 , 8 , 9 , 14 ]  . 
the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 842848 doi 10.1007 / s00066 - 013 - 0402 - 6 received : 29 may 2013 accepted : 3 june 2013 published online : 18 july 2013 springer - verlag berlin heidelberg 2013 d.milanovi1b.jeremi2a.l.grosu1g.rcker3m.henke1 1 department of radiation oncology , university medical center freiburg 2 division of radiation oncology , university of stellenbosch medical school and tygerberg , hospital , cape town 3 institute of medical biometry and medical informatics , university medical center freiburg reirradiationplusegfrinhibitionin locallyrecurrentandunresectable headandneckcancer finalresultsfromasingleinstitution patients with head and neck squamous cell carcinoma ( hnscc ) may be cured with surgery and / or radiochemotherapy ( rct ) [ 14 ]  . 
in the primary treatment of locoregionally advanced hnscc , rct , as opposed to radiotherapy ( rt ) alone , improved locoregional control and survival [ 25 ] in both the definitive [ 1 , 9 , 17 , 18 ] and postoperative setting [ 4 ]  . 
chemotherapy as a sole therapeutic modality will not result in good long - term response rates in these patients and plays only a role in palliative management [ 12 , 13 ]  . 
an alternative for patients who are not candidates for resection is reirradiation ( re - rt ) and several investigators have demonstrated local control rates of up to 50% , with 5 - year survival of approximately 20% [ 16 ]  . 
the addition of different chemotherapeutical agents to re - rt could improve outcome but increase toxicity [ 10 ]  . during the past 10 years , significant advances have been made in characterizing the molecular biology and genetics of hnscc [ 20 ]  . 
egfr ( epidermal growth factor receptor ) , which belongs to the family of erbb receptor tyrosine kinases [ 27 ] , is frequently overexpressed in hnscc and may contribute to development of radioresistance [ 11 , 15 , 23 ]  . 
it has been shown that the primary treatment of patients with locoregionally advanced hnscc with cetuximab and rt was superior to rt alone in increasing both the duration of locoregional disease control and survival [ 5 ]  . 
other criteria included the following : life expectancy 3 months and ecog performance status 3 ; adequate hematologic , renal , and liver function ; recovery from relevant toxicities of previous treatment . 
the study was approved by the ethics committee of the albert - ludwigs university freiburg and was performed according to the declaration of helsinki . treatment after immobilization with a thermoplastic head - and - neck mask , patients had a planning ct ( 5 mm slice thickness )  . 
to delineate the gross tumor volume ( gtv ) , the pet / ct imaging was fused with the planning ct in 8 patients and the planning ct was used for treatment planning . 
1 characteristics and oncological history of patients with recurrent head and neck squamous cell carcinoma patientnumecog locationatfirst diagnosis stageatfirstdiagnosis relapselocation relapse stage ageat recurrence ( years ) hypopharynx oropharynx oropharynx larynx larynx oropharynx oropharynx larynx oropharynx hypopharynx hypopharynx oropharynx oropharynx oropharynx larynx hypopharynx oropharynx hypopharynx larynx larynx oropharynx oropharynx ct2 cn2 cm0 pt4 pn1 cm0 ct3 cn2c cm0 ct2 cn0 cm0 ct0 pn2b cm0 ct1 cn2c cm0 ct4 cn3 cm0 ct4 cn2a cm0 pt1 pn2b cm0 pt2 pn1 cm0 ct3 cn2b cm0 ct3 cn1 cm0 pt1 pn1 cm0 pt2 pn2b cm0 ct4 cn2c cm0 ct4 cn2c cm0 ct4 cn2c cm0 pt2 pn2b cm0 ct4 cn2c cm0 ct3 cn0 cm0 ct3 cn0 cm0 ct4 cn1 cm0 pt3 pn3 cm0 timebetween primaryrtand re - rt ( months ) hypopharynx lymph node oropharynx hypopharynx oropharynx lymph node oropharynx oropharynx lymph node oropharynx hypopharynx oropharynx oropharynx oropharynx hypopharynx oropharynx oropharynx hypopharynx hypopharynx larynx larynx oropharynx oro / hypopharynx rct3 rcn0 cm0 rct0 rcn1 cm0 rct2 rcn0 cm0 rct4 rcn2b rct3 rcn0 cm0 rct0 rcn1 cm0 rct3 rcn0 cm0 rct4 rcn0 cm0 rct0 rcn1 cm0 rct3 rcn0 cm0 rct4 rcn2c rct2 rcn0 cm0 rct3 rcn2a rct3 rcn0 cm0 rct2 rcn0 cm0 rct2 rcn2 cm0 rct2 rcn1 cm0 rct4 rcn2b rct4 rcn0 cm0 rct2 rcn0 cm0 rct4 rcn0 cm0 rct2 rcn0 cm0 rct4 rcn0 cm0 cup cancer of unknown primary . porated the gtv with a safety margin between 1 and 1.5 cthe prescribed total dose was between 50.4 and 66 gy , at daily fractions of 1.8 gy on 5 successive days per week . 
 rt was delivered by a linear accelerator with a minimum energy of 6 mev using multiple fields . every effort was made to maximally reduce the radiation dose to the previously treated spinal cord . 
 patients were seen weekly and additionally complete blood counts and metabolic panels were performed . follow - up side effect assessment toxicity was recorded at baseline before re - rt , every week during treatment , and then every 3 months . 
side effects were scored using the common terminology criteria for adverse events , version 3.0 ( ctcae ) [ 29 ]  . follow - up time was calculated from the end of re - rt to the date of last patient contact or death . 
ct , mr or pet studies of the neck were performed 8 weeks after re - rt and every 34 months thereafter . endpoints statistical analysis the primary endpoints were the safety and tolerability of the combination re - rt and cetuximab . 
secondary endpoints were overall survival , overall response rate , and progression - free survival . all statistical analyses were performed using the open statistical software environment [ 26 ]  . 
since survival time from the date of completing re - rt was used as the endpoint in this study , it served as the dependent variable in the statistical analyses . 
 the simultaneous relationship of multiple strahlentherapieundonkologie102013 | abstract zusammenfassung strahlenther onkol 2013 189 : 842848 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0402 - 6 d.milanovib.jeremia.l.grosug.rckerm.henke reirradiation plus egfr inhibition in locally recurrent and unresectable head and neck cancer . 
for some patients with recurrent , unresectable , and previously irradiated head and neck squamous cell carcinoma ( hnscc ) , reirradiation ( re - rt ) may be a curative option . 
concomitant egfr blockade ( cetuximab ) was given initially at 400 mg / m2 two days prior to re - rt and weekly ( 250 mg / m2 ) thereafter . 
grade 3 acute side effects were documented for dermatitis ( 35% ) , dysphagia ( 30% ) , acneiform rash ( 30% ) , and mucositis ( 15% )  . 
prolonged intervals from first treatment to re - rt seem to be unfavorable . keywords reirradiation cetuximab head and neck neoplasms epidermal growth factor receptor chemotherapy rebestrahlung und egfr - inhibition beim lokal rezidivierten , nichtresektablen kopf - hals - karzinoabschlieende ergebnisse einer monozentrischen studie zusammenfassung hintergrund . 
eine erneute bestrahlung ( re - rt ) kann fr patienten mit rezidiviertem , nichtresektablem kopf - , hals - karzinom ( hnscc ) eine kurative option darstellen , whrend chemotherapie und inhibition des epidermalen wachstumsfaktorrezeptors ( egfr ) nur eine palliative rolle spielen . 
ein prolongiertes intervall zwischen erster bestrahlung und re - rt erscheint eher ungnstig . schlsselwrter rebestrahlung cetuximab kopf - hals - karzinom epidermaler wachstumsfaktorrezeptor chemotheapie prognostic factors to survival was assessed using the cox proportional hazards model . 
the survival rates were estimated using the kaplanmeier method . results patient characteristics between june 2008 and june 2011 , we treated 23 patients ( 21 men and 2 women ) for locally recurrent , histologically 844 | strahlentherapieundonkologie102013 confirmed hnscc . 
patient and tumor characteristics are presented in .tab.1. treatment compliance , acute and late toxicity in all , 20 of 23 patients completed their prescribed course of re - rt and all received the loading dose of cetuximab in the first week of re - rt followed by further weekly administrations . 
further details on baseline , acute , and late toxicity are presented in .tab.2. response to treatment both clinical examination and mri were used to determine response rates 8 weeks after treatment . 
in all , 3 complete responses ( cr ) , 4 partial responses ( pr ) , 3 stable diseases ( sd ) , and 8 progressive diseases ( pd ) were documented . 
a multivariable analysis using the cox regression model showed significant influence of acneiform rash grade 23 and relapse - free period ( time between the end of first radiotherapy course and diagnosis of local recurrence ; .tab.4 ) on patient survival . discussion the treatment of patients with locoregionally recurrent , unresectable and previously irradiated hnscc is a continuing challenge . 
thus , combined treatment with re - rt and cetuximab , when compared to standard platinum - based chemotherapy plus cetuximab , did not seem to improve survival in these patients . 
however , a strength of our study is that we present the largest data set of these patients treated by external - beam re - rt in the combination with cetuximab . 
on the other hand , our findings are limited by the fact that toxicities were collected retrospectively and that in some patients short follow - up and early death events may cause artificially decreased risk of late toxicity . due to the fact that the predominant cause of death in patients with unresectable , recurrent hnscc is uncontrolled local progression [ 7 ] , it has been supposed that re - rt may play important role achieving local control followed by longer survival . 
a small percentage of previously irradiated patients with recurrent , nonmetastatic , and unresectable hnscc may benefit from re - rt [ 16 ] , but it is not possible to identify these patients a priori [ 35 ]  . 
 [ 19 ] treated 105 patients with unresectable , recurrent hnscc with split - course concomitant twice - daily re - rt in combination with low dose paclitaxel and cisplatmedian survival was 12.1 months but toxicity was high . 
this may be an important issue to consider when optimizing both re - rt and systemic compounds of a combined modality approach in this setting . the overexpression of egfr , which is not only responsible for progression but also for increased resistance toward rt , is one of the most important molecular biological characteristics of hnscc [ 20 ]  . 
comparably , a multinational phase iii study demonstrated a survival benefit in patients who were treated primarily with rt plus cetuximab in comparison to rt alone [ 5 ]  . cetuximab combined with re - rt may open a new therapeutic window to treat recurrent , unresectable hnscc . 
one patient developed a flap necrosis ( grade 4 ) , while the most frequent grade 3 acute side effects were dermatitis ( 30% ) , acneiform rash ( 20% ) , and mucositis ( 10% )  . 
the median overall survival time was 7 months ; the 1 - year overall survival rate was 40% . in our study , 1 patient died due to hypersensitivity reactions during the first cetuximab administration . 
we speculate that these patients suffered from a more aggressive second primary / radiation - induced cancer that may need treatment of elective lymph nodes or a higher re - rt dose . taken together , based on our and published data , we conclude that patients with recurrent hnscc will profit from re - rt or cisplatin / 5 - fluorouracil chemotherapy plus cetuximab . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 887893 doi 10.1007 / s00066 - 013 - 0358 - 6 received : 20 december 2012 accepted : 25 march 2013 published online : 7 . 
juni 2013 springer - verlag berlin heidelberg 2013 external beam irradiation requires repeated , precise patient positioning and continuous monitoring thereof , particularly during a complex sequential arrangement of beams . 
the spectrum of applied methods and the progress in this field has led to development of a diversity of ultra - fast and high - precision range sensing instruments , including optical systems [ 1 , 3 , 5 , 20 , 26 ]  . the evolution of these technologies has not yet come to an end . 
particularly advanced techniqueslike intensity - modulated radiotherapy ( imrt ) with volumetric methods and hadron treatments [ 27 ] require positioning of a patient with the utmost accuracy , thus rendering the integration of image - guided radiotherapy ( igrt ) protocols very important . 
this initial publication describes the basic functionality , geometrical validation and use of the 3d - ss system in a clinical workflow during adjuvant whole - breast irradiation ( wbi ) after breast conserving surgery . materials and methods patients and treatment planning fourteen breast cancer patients with a median age of 60.7 years ( range 3874 years ) were enrolled in the study . 
for treatment planning an averaged ct was performed ( pitch 0.15 , rotation 1 / s ; reconstructed slice thickness and distance 5 mm ) to account for breathing motions . 
based on the ct information , an automatically generated body outline ( > 740 hounsfield units , hu ) was contoured in 3d with a point density of the triangulated mesh of about two vertices / cm2 . 
1 9 newly developed surface scanner mounted on the ceiling of a treatment roo basic components of the 3d scanning system are two standard video projectors ( a ) and two colour cameras ( b )  . 
each surface triangle was mapped to a colour video image of the patients surface to obtain a highly realistic impression of the scene treatment planning planning ct ( averaged ) contouring of structures : skin ( reference ) , ptv , bone , lung conventional simulation ( skin markings ) patient aligned via laser and skin markings patient positioning treatment on linac clinical workflow surface data acquisition first lateral segment ( verification imaging ) remaining lateral segments medial beam first surface scan second surface scan third surface scan treatment session finished fig . 
the routine clinical protocol is drawn in solidline boxes ; dashed - line boxes show complementary 3d surface acquisition , linac linear accelerator 888 | strahlentherapieundonkologie102013 structure during further positioning procedures . 
planning target volumes ( ptvs ) were contoured by the treating physicians ( volumes 3651750 ml , mean 824 ml ) ; skin , lung and bones were contoured automatically , based on hu thresholds . wbi was performed with an isocentric tangential field - in - field technique with 6 and 15 - mv segments ( > 5 segments per portal ) to generate an individually optimized intensity - modulated dose distribution [ 24 ]  . 
in accordance with international commission on radiation units ( icru ) guidelines , the prescribed dose was 50 gy in normofractionation with single fractions of 2 gy ( 12 patients ) , or 40.5 gy in hypofractionation with single fractions of 2.7 gy within a prospective trial protocol ( 2 patients )  . 
the distance from the isocenter to each component was 1.8 2 to calibrate the scan system with respect to the machine coordinate system , the calibration method described by tsai [ 28 ] was used . for scanning the patients surfaces , a gray code [ 12 ] image sequence of black and white stripes followed by a phaseshifted stripe - light image was projected by one source at a time . 
the surface model was created by solving the 3d triangulation problem along the border of dark abstract zusammenfassung strahlenther onkol 2013 189 : 887893 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0358 - 6 c.gaisbergerp.steiningerb.mitterlechners.huberh.weichenbergerf.sedlmayerh.deutschmann three - dimensional surface scanning for accurate patient positioning and monitoring during breast cancer radiotherapy abstract purpose . 
after 2 weeks , a systematic interfraction shift in patient positioning was noted , particularly in the vertical direction ( 4.90.56 mm ) , which was attributed to patients progressively relaxing . 
particularly for more sophisticated irradiation techniques , it helps to improve accuracy in patient positioning during radiotherapy without the exposure to additional ionizing radiation . keywords image - guided radiotherapy intensity - modulated radiotherapy breast conserving surgery patient positioning electronic portal image 3 - d - oberflchenerfassung zur genauen patientenpositionierung und positionsberwachung whrend der strahlenbehandlung des mammakarzinoms zusammenfassung zielsetzung . 
die analyse der tglichen patientenpositionierung ergab eine mittlere abweichung von 0 , 42 , 4 mm lateral , 0 , 31 , 9 mm longitudinal und 0 , 23 , 3 mm vertikal . 
the maximum scan volume was approximately 600700500 mm ( lateral , lat ; longitudinal , lng ; vertical , vrt )  . 3d data registration the 3d body outline derived from the planning ct scan served as the reference surface for every subsequent optical surface registration . 
the method handles six full degrees of freedom and converges monotonically to the nearest local minimum of a mean - square distance metric , if no additional extensions are applied . 
to avoid local minima in the first iterations , only a small number of randomly selected vertices were used and these were restricted to the breast as the region of interest . 
the mean value of all distances between the reference and the actual surface within this region of interest was derived to give the mean target registration error ( mtre )  . treatment protocol and data evaluation throughout the whole study , a daily quality check to ensure sufficient 3d scan accuracy was performed with phantoms after a warm - up phase . 
the tolerance level was set to 1 mthis verification step was performed during the linac warmup period and took only 5 min . all measurements acquired with the optical 3d - ss system were evaluated retrospectively . 
during each treatment session , three portal imaging scans were performed in parallel ( in flat - panel free running mode ; last three frames during beam - on time with a total integration time of 1.3 s were considered )  . 
daily epis in beams eye view ( bev ) projection were used to measure the distance between lung and skin on three predefined planes ( isocenter and 5 cm superior / inferior )  . 
for intrafraction motion analysis , the mean distances at the same measurement points ( 0 , 53 , and 128 s ) were used to compare three consecutive 3d - ss acquisitions during the same fraction to account for motion artefacts caused by , for example , the respiratory cycle , the system supports operation in a fast scan mode , where monitoring is limited to 150 surface points with 5 hz and the amplitude of motion ( breathing curve ) is visualised quantitatively . 
complementary to this , a portal image video mode was used to verify the magnitude of breast motions during breathing . backprojection of colour - coded deviations an innovative application of surface scanners is optical backprojection of positioning deviations onto the patients skin by means of the video projectors in the treatment roofor this feature , an algorithm calculates the projectors perspective of the colour - coded setup deviations on the patient model and relays this image to the projector . 
a bipolar colour palette shows deviations in forward ( out of the patient ) and backward ( into the patient ) directions , with different colours to support intuitive position adjustments . 
such backprojection provides treatment room staff with interactive feedback , as areas of imprecise patient alignment are highlighted in a representative colour , with immediate update after correction . results after the first fraction , only 2 out of 14 patients continued to wear sunglasses during the treatment sessions ; all others abstained . 
4 8 example 3d surface scan of a female right breast in beams eye view perspective with associated electronic portal image ( epi , top ) and transversal ct slice ( middle ) before and after correction . 
the diagram shows the distance during a fraction between the first electronic portal image ( epi ) used as a reference and the surface scans , measured in the image plane . 
 the mean deviation ( 1.2 mm ) after the third scan ( 128 s ) can be explained by sag of the patient time [ s ] after first scan this is in agreement with c . 
only one patient with a large ptv ( 1750 ml ) showed a swelling of 2.1 mm during this time . distance evaluation and rigid registration the mtre before and after 3d registration of the first 3d - ss of each fraction are shown in .tab.1. 
during the whole course of rt , 2 / 14 patients had a mtre of more than 3 monly 5 / 205 registration procedures required a vertical correction of more than 10 mm . according to epi verification findings , patient position was optionally corrected by raising or lowering the treatment table for subsequent fractions . 
the third scan was performed after approximately 2 min and showed an additional drift of 1.20.7 mm ( minimum 0.2 mm ; maximum 6 mm ) with respect to the reference . 
this socalled sag was observed for all patients in the cohort ; 2 / 14 patients systematically moved more than 2 mm . interfraction motion analysis of interfraction motions showed that the position of the patient after 15 days varied by only 0.90.5 mm along strahlentherapieundonkologie102013 | original article lateral longitudinal vertical days [ d ] after first treatment fig . 
because the long - term outcome of patients with hnscc has improved through optimized multimodal approaches , including surgery , radio ( chemo ) therapy , or combinations of both [ 3 , 5 , 19 , 20 , 22 , 23 ] , the incidence of subsequent cancers has become a life - limiting factor [ 2 ] and may also have considerable impact on the primary treatment approach , such as radical surgery vs . 
 organand function - preserving treatment [ 4 ]  . in the past , various screening approaches for patients at high risk , such as those who smoke tobacco or abuse alcohol , provided no benefit with regard to mortality or overall survival [ 8 , 13 , 14 ]  . 
one remarkable exception is a re874 | strahlentherapieundonkologie102013 cent study by the national lung screening trial research team , which showed promising results for patients at high risk for lung tumors who are screened via ct scanning , leading to a highly significant relative reduction in tumor - related mortality [ 1 ]  . in addition to the potential unnecessary psychological stress associated with the superfluous testing of individuals , the cost - effectiveness of additional examinations in large patient cohorts worldwide is another important concern . 
to counter this problem , the optimal strategy is to identify patients at the highest risk for undetected malignancies , followed by curative treatment to obtain improved overall survival rates . 
because large - scale studies failed to successfully solve this problem for an entire population , the aim of the present study was to prospectively test the efficacy of a systematic examination for spm in high - risk patients treated previously for hnscc . materials and methods inclusion criteria and patient characteristics this prospective observational study was intended to be conducted during patients regular follow - up examinations . 
 the study protocol was approved by the institutional review board , and informed written consent was obtained from all patients . after consultation with the department of medical statistics , a sample size of a minimum of 100 patients was defined prior to the start of the study . 
patients who had previously undergone therapy for hnscc with curative intent [ surgery alone ( uicc stages i / ii ) or surgery and adjuvant radio ( chemo ) therapy ( uicc stages iii / iva / b ) ] were included consecutively during routine follow - up care . 
between july 2008 and november 2011 , 118 consecutive patients were eligible and underwent systematic examination for spm ( 13 women , 105 men , median age 62 years , range 3886 years )  . 
all primary treatments were administered between july 1996 and february 2011 ; thus , the interval between the primary treatment and the elective examinations ranged from 1140 months . due to advanced - stage tumors , 84 of the 118 patients had received adjuvant radio ( chemo ) therapy after surgery , whereas 34 patients with early - stage tumors received no postoperative treatment . 
 radio ( chemo ) therapy consisted of normofractionated radiotherapy ( 2 gy / day , five times / week ) targeting the primary tumor ( 64 gy ) , the involved lymph nodes , and the potential drainage sites on both sides of the neck , including the supraclavicular region ( 50 gy )  . 
in 59 of the 84 irradiated patients , a concomitant cisplatinbased intravenous chemotherapy was regularly administered , whereas 25 patients were treated with adjuvant radiotherapy alone , either because of the treatment regimens at that time ( 15 patients ) or because of patient refusal , reduced general condition , or inadequate renal function ( 10 patients )  . 
pretreatment patient characteristics are summarized in .tab.1. examinations during follow - up routine aftercare for patients with hnscc consisted of quarterly clinical examination including an earnosethroat endoscopy ( ent - endo ) , complete blood counts and a computed tomography of the head and neck , if suspicious . 
in case of unsuspicious results , the interval of follow - up examinations was consecutively prolonged according to who guidelines , and finally performed yearly after a time period of 5 years . for the present study , patients without known local failure , distant metastases or clinical symptoms suggesting recurrence were considered for participation at any point of time during their follow - up care . 
if necessary , biopsies were taken from suspicious areas within the aero - digestive area for histological confirmation of tumor growth . to detect spm in the gastro - esophageal region , an endoscopy of the upper git was performed without an additional staining procedure . 
in case of irregular local appearance , biopsies were taken . a low - dose ct scan was performed to screen for intrathoracic spm : all patients underwent 64 - row multidetector precontrast ct of the chest using a vct scanning unit ( ge medical systems , milwaukee , wi , usa )  . 
the scan parameters were 0.8 s revolution time , tube settings were 120 kv at 60 ma , slice collimation was 640.625 mm and image reconstruction was 0.625 mm axial section thickness with 0.625 mm interval using lung filter kernel with a field of view of 300330 mall scans were performed in deep inspiration . 
for the evaluation , the criteria of the fleischner society were used as described previously [ 15 ]  . patients without suspicious findings were returned to routine clinical followup care . 
recently , computed tomography ( ct ) of the chest was shown to significantly decrease the risk of death due to bronchial carcinoma ( bc ) in a cohort of smokers whose risk of bc is increased but might be lower than that of patients previously treated for hnscc . 
between july 2008 and november 2011 , 118 participants underwent a prospective , systematic examination for spm ( 13 women , 105 men , median age 62 years )  . 
patienten , welche bereits aufgrund eines plattenepithelkarzinoms im kopf - hals - bereich ( hnscc ) behandelt wurden , weisen ein hohes risiko fr bsartige zweittumore ( second primary malignancies , spm ) auf . 
in diesem zusammenhang fhrte eine computertomographie ( ct ) der lunge in einer krzlich verffentlichten studie bei rauchern , welche bekanntlich ein erhhtes risiko fr bronchialkarzinome ( bc ) tragen , zu einer signifikanten reduktion der mortalitt durch eben diese tumore . 
zwischen juli 2008 und november 2011 unterzogen sich 118 studienteilnehmer prospektiv einer systematischen untersuchung auf einen zweittumor ( 13 frauen , 105 mnner , medianes alter 62 jahre )  . 
adapting a surveillance scheme including a chest ct is recommended . keywords carcinoma , squamous cell of head and neck neoplasms , second primary low - dose ct radiochemotherapy screening wickelten bisher kein lokalrezidiv oder fernmetastasen . 
eine ergnzung der routinenachsorge durch eine thoraxcomputertomographie wird empfohlen . schlsselwrter plattenepithelkarzinom im kopf - halsbereich zweittumor low - dose ct strahlenchemotherapie screening the effect of the possible prognostic factors on the probability of the incidence of a spm was analyzed by univariate cox regression . 
 because of patient refusal or individual reasons due to prior treatments , the ees was not performed in 19 patients ( 16% )  . for 30 patients ( 25.4% ) , a tumor was strongly suspected in the first examination . 
these patients returned to the routine clinical follow - up care . results of the ent and subsequent procedures overall , 111 of the 118 patients ( 94% ) presented no spm based on the ent - endo . 
of these patients , 6 were treated with curative intent as follows : 2 patients with transoral laser - microresection , 2 patients with resection plus adjuvant radiochemotherapy , and 2 patients with primary radiochemotherapy ( 1 patient because of non - surgical contraindications for a resection and 1 patient because of a concurrent proximal ec )  . 
due to prior radiotherapy , curative treatment 876 | strahlentherapieundonkologie102013 118 patients normal results n = 59 control recommended n = 29 suspected secondary tumor in primary examination n = 30 overall suspected secondary tumor n = 33 refused any further examination n = 3 additionals examinations n = 30 routine follow - up care n = 97 unsuspicious n = 9 histopathological confirmed secondary malingnancy n = 21 fig . 
1 8 flowchart for all 118 participants displaying the overall results of the performed examinations ( computed tomography scan of the chest , earnosethroat endoscopy of the throat and oral cavity , and endoscopy of the esophagus and stomach ) 0 - 20 21 - 40 81 - 100 101 - 120 121 - 140 41 - 60 time interval [ months ] 61 - 80 fig . 
2 9 number of detected secondary malignant tumors ( smt ) according to the elapsed time since primary treatment for hnscc suspected tumor computertomography n = 27 panendoscopy of the head and neck n = 7 endoscopy of the esophagus and stomach n = 4 not confirmed n = 0 ( 0% ) confirmed n = 7 ( 100% ) not confirmed n = 11 ( 40.7% ) confirmed n = 16 ( 59.3% ) not confirmed n = 1 ( 25% ) confirmed n = 3 ( 75% ) treated palliatively n = 1 ( 14.3% ) treated palliatively n = 3 ( 18.75% ) treated palliatively n = 0 ( 0% ) treated curatively n = 6 ( 85.7% ) treated curatively n = 13 ( 81.25% ) treated curatively n = 3 ( 100% ) fig . 
3 8 flowchart of patients with suspected tumors divided by the performed examinations ( panendoscopy of the head and neck , computed tomography scan of the chest and an endoscopy of the esophagus and stomach )  . 
 for another 20 patients ( 20% ) , common diseases , such as esophagitis , duodenitis , varicose veins , reflux , hernia , and adenoids within the duodenum , were detected , conservatively treated and again controlled without any spm suspicion . 
a sample was taken in 4 patients ( 4% ) , 3 of whom had histopathologically confirmed spms ( all squamous cell carcinoma stage ct3 , cn0 , cm0 ) and 1 of whom presented an esophagitis . 
two spms were treated with curative intent with preoperative radiochemotherapy followed by tumor resection , whereas the third patient received curative radiochemotherapy because of a concurrent secondary tumor of the h&n . 
 notably , 2 of these 3 tumors were also detected by the blinded evaluation of the ct scan . ct scan results and subsequent procedures the ct scan yielded normal results in 66 of the 118 patients ( 56% )  . 
of these , 3 were classified as having a suspected tumor . the subsequent 27 examinations or procedures for the patients with suspected spm consisted of resections of suspicious pulmonary foci using video - assisted thoracic surgery or atypical resection ( 10 patients ) , additional bronchoscopies ( 3 patients ) , ees ( 3 patients ) , mri scans ( 2 patients ) , a contrast - enhanced ct scan ( 2 patients ) , a ct - guided biopsy ( 1 pastrahlentherapieundonkologie102013 | original article tient ) , a partial nephrectomy ( 1 patient ) , a palliative irradiation of osseous metastases ( 1 patient ) and a stomach sampling procedure ( 1 patient )  . 
three patients refused any continuing examinations ( 2 with suspected bc and 1 with ec and an additional inoperable hnscc )  . the histopathological processing of the 10 resections resulted in the diagnosis of 6 squamous cell carcinomas ( 4 at stage pt2 , cn0 , cm0 ; 1 at stage pt4 , cn0 , cm0 ; and 1 at stage pt1 , cn0 , cm0 ) , 2 adenocarcinomas ( both at stage pt2 , cn0 , cm0 ) , 1 epitheloid cell granuloma , and 1 aspergilloma . 
 the 2 patients with confirmed non - small cell lung carcinomas ( both pt3 , pn0 , cm0 ) underwent curative resection . the 3 abnormalities of the esophagus were investigated by additional ees , which revealed 2 cases of malignant squamous cell carcinoma ( ct3 , cn0 , cm0 ) and 1 case of esophagitis . the resection of the kidney identified a renal cell carcinoma ( pt1a , pn0 , cm0 ) , whereas the contrast - enhanced ct scans of the lung and both mri scans of the adrenal gland showed no tumors . 
the strongly suspected carcinoma of the stomach could not be confirmed by repeated sampling procedures , and the patient refused a complete resection of the stomach or further examinations . the ct - guided biopsy showed a squamous cell carcinoma of the lung [ ct2 , cn2 , cm1 ( contralateral lung ) ]  . 
because of the extended bc with contralateral metastases , this patient received palliative chemotherapy . one patient decided to receive supportive care only due to an inoperable , previously irradiated tumor in the h&n area and an additional extended tumor in the lung . 
one patient was irradiated palliatively because of osseous metastases in the thoracic spine , which was diagnosed by ct scan . 878 | strahlentherapieundonkologie102013 overall , ct scanning of the chest detected 13 of the 21 histologically proven spin addition , ct was highly cost - effective , with a false - positive rate of 40.7%. histopathological analysis and treatment after histopathological analysis , malignant tumors were confirmed in 21 of the 118 patients ( 18% ) : 10 with bc , 6 with hnscc , 2 with ec , 1 with hnscc and ec , 1 with renal cell carcinoma , and 1 with osseous metastases . 
interestingly , 11 of these 21 patients ( 52% ) were diagnosed during the 1to 20 - month interval between the first hnscc treatment and the elective examinations , whereas the detection of all other tumors was distributed equally throughout the entire 140 - month treatment period . finally , 18 of these 21 patients ( 86% ) with spm were again treated with curative intent . 
most tumors were located in the aero - digestive tract ( 80% , [ 14 ] ; 81% , present study ) and developed with a constant yearly incidence rate of 4% . the obvious explanations for this high prevalence of spm are known risk factors as tobacco and alcohol abuse . 
this difference might be the result of an individual genetic predisposition , which has not been shown for patients with hnscc in the same manner as it has been in other diseases , such as hodgkins lymphoma and polycythemia vera [ 9 , 12 ]  . 
the effect of previous radio ( chemo ) therapy - related risk factors may also be debatable , although no effect was shown in this series of patients . when analyzing the different examination techniques , our results underline the importance of performing a precise entendo , as this detected spms in the h&n area in 7 patients within 20 months after the primary treatment . 
therefore , entendo is strongly recommended as part of the systematic search for a spm during routine surveillance , especially within the first time period after the primary treatment [ 11 , 26 ]  . 
notably , a true - positive histopathological confirmation rate of 100% by biopsy for suspicious findings in our patient cohort was achieved . in contrast , the benefit of a routine ees for the detection of spm remains unclear . 
 [ 13 ] reported an incidence rate of spm within the digestive tract of only 0.59% in 787 patients listed in the national cancer registry of taiwan over a 25 - year period . 
in fact , in the present study , only 1 out of the 118 patients profited from routine ees because 2 of the 3 detected spms were also suspected from the ct scan of the chest . 
this missing proportion could potentially lead to a higher incidence of undetected second primary malignancies , which means that ees would be of a higher benefit for the study patients . overall , ct scanning of the chest was the most powerful examination , as it detected 13 of the 21 histologically proven spin addition , ct was also highly cost - effective , with a false - positive rate of only 40.7%. 
 [ 24 ] described a high rate of false - positive findings ( 92.4% ) in a study with 1 , 520 individuals aged 50 years or older , with a minimum smoking history of 20 pack years , who were screened with yearly spiral ct , chest radiography and sputum cytology examinations over a period of 5 years . 
although the authors concluded that ct is able to detect bc at early stages compared with chest radiography or sputum cytology , a reduction in mortality was not found . further comparable efforts to test other high - risk patient cohorts for repeated treatment options and survival showed no benefit of the various screening approaches [ 8 , 13 , 14 ]  . as a remarkable exception , a study by the national lung screening trial research team found promising results in high - risk patients who were screened with ct scans compared with chest radiographs . 
in this study , 53 , 454 people , aged 5574 years and with a minimum smoking history of 30 packyears , were randomized to receive annual ct scans over 3 years [ 1 ]  . 
the analyses revealed a significant reduction of 20% in tumor - related mortality due to a lung tumor in the group that underwent ct scanning . in this context , the most remarkable finding of the present analysis is that 18 of the 21 patients ( 86% ) with histopathologically proven spms could be treated with curative intent . 
consequently , the effect of the early detection of spm on overall survival may be similar or even greater than that of adjuvant radio ( chemo ) therapy . this intention is even more supported in the present study by the absence of a correlation between the examined possible prognostic factors and the incidence of the spm in univariate regression analysis . 
however , longer follow - up periods and larger randomized studies are needed to test these hypotheses . as in other oncological settings , the early detection and subsequent definitive cure may also impact initial treatment decisions in cases of hnscc [ 10 ] because high mortality rates due to spm as a substantial competing risk factor may favor reduced radicality of the initial surgery and adjuvant treatment , e.g. , laser microsurgery and less toxic radio ( chemo ) therapy [ 4 , 6 , 16 , 21 , 25 , 28 , 29 ]  . 
thus , an analysis of different prognostic factors for the occurrence of spm is difficult to evaluate and might be more substantive in a larger cohort . the percentage of squamous cell carcinoma cases in the group of patients with secondary bc was high , e.g. , compared with aberle et al . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 881886 doi 10.1007 / s00066 - 013 - 0415 - 1 received : 26 march 2013 accepted : 19 june 2013 published online : 6 september 2013 springer - verlag berlin heidelberg 2013 it is widely accepted that the monte carlo method applied to the simulation of radiation transport is able to compute accurate results in radiotherapy problems [ 8 , 13 ]  . 
for clinical applications , several codesin which approximations to the physical interaction and transport models were introducedhave been developed to overcome this limitation [ 6 , 10 , 12 , 19 , 21 ]  . 
a further limitation for the implementation in clinical routine has been the difficulty and effort entailed in preparing , executing , and analyzing a simulation . in this article we shall focus on the simulation of medical linear accelerators ( linacs ) and on the computation of the absorbed dose distribution in patients . 
these tasks require coding the linac geometry , which is a tedious and error - prone task , and the careful selection of certain transport parameters , which demands some knowledge of the physics of the monte carlo code employed . 
to surmount these constraints we have developed the primo syste primo generates the necessary input files for simulating a variety of varian and elekta linacs with the monte carlo code penelope [ 1 , 15 , 16 ] and computes dose distributions in phantoms and computerized tomographies . 
primo combines all these features and functionalities under a friendly graphical user interface , which includes various tools for analyzing and representing the generated data . the end result is a program that handles the process of preparing , executing and analyzing the simulation of a linac and the computed dose distribution without requiring any previous knowledge from end users about the monte carlo method . 
nonetheless , advanced users can have access to the details of the simulation by modifying the configuration files that govern the execution . code layers primo is designed as a layered software structure , which is schematized in .fig.1. 
pengeom is included in the penelope distribution . in penelope , end users are responsible for writing a main program that defines the source of particles , the quantities of interest to be tallied and the variance - reduction techniques to be applied . 
sitting above it , the peneasy code provides the steerprimo linac - glass graphical user interface peneasy linac input files preparation for linacs peneasy main : sources + tallies + vrts fig . 
2 8 screenshot of primo showing the beams eye view of the field with gantry angle of 45 superimposed to the digitally reconstructed radiograph for the example of prostate irradiation ing main program for the monte carlo simulation . the input files required to run the penelope / peneasy system are created during run time by peneasylinac [ 17 ] , which forms the fourth layer of the structure . 
this code accepts as input the linac model and its configuration , which is determined by fwhether the machine is operated in the electron or photon mode , fthe nominal beam energy , fthe position of the jaws , and fthe configuration of the multileaf collimator ( or electron applicator size in electron mode )  . based on these choices , peneasylinac creates a quadric geometry file for pengeom and a configuration file for peneasy . 
this latter file defines the particle source , the values of penelopes parameters governing the transport physics , and the values of the parameters for the applied variance - reduction techniques . the upper code of the scheme is the graphical layer for the automation of the simulation system , designed for the modeled linacs , which we named linacglass . 
this layer is basically an elaborate user interface to operate peneasylinac , to run penelope / peneasy , and to collect the simulation results and produce graphical plots of the data . the parts of the system related to monte carlo simulation are written in fortran , while the analysis tools and the graphical user interface are coded in delphi . 
owing to the latter , primo runs only on windows . primo work flow linac - glass is designed to reduce the users effort to accomplish the steps of simulation setup , execution , and analysis of the results . 
the currently available linacs from varian are clinacs 600 c , 600 c / d , unique , the series 18 , 21 , and 23 , and truebeam , the latter by means of the phasespace files distributed by varian in the iaea format . 
 the shape of the radiation field is further defined by positioning the jaws , multi leaf collimators , or electron applicators according to the linac model and operation mode chosen . primo decides the most adequate variance - reduction techniques to be employed and determines the parameters related to thenotwithstanding , users can modify all parameters that govern the simulation . the simulation of a linac can be used either to tally a phase - space file in the iaea format or a dose distribution . 
simulations can be started either from the primary electron source of the linac , as it has been already described , or from a previously tallied phase - space file . 
primo can use imported phase - space files that have been written by other monte carlo codes using the iaea format . dosetallying dose distributions can be estimated inside a phantom or in a computerized tomography study . 
for the latter , primo imports dicom - ct images ( digital imaging and communication in medicine standard ) from which it can construct a voxelized geometry for the estimation of the dose . 
 the importing process requires the conabstract zusammenfassung strahlenther onkol 2013 189 : 881886 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0415 - 1 m.rodriguezj.sempaul.brualla primo : a graphical environment for the monte carlo simulation of varian and elekta linacs abstract background . 
primo combines ( 1 ) accurate physics from the penelope code , ( 2 ) dedicated variance - reduction techniques that significantly reduce the computation time , and ( 3 ) a user - friendly graphical interface with tools for the analysis of the generated data . 
a prostate treatment , conformed with a high definition millenium multileaf collimator ( mlc 120hd ) from a varian clinac 2100 c / d , is presented as an example . 
it is free software that can be downloaded from keywords dose distribution phantoms , imaging computerized tomography , x - ray planning target volume organs at risk primo : eine graphische benutzeroberflche fr monte - carlo - simulationen von varianund elekta - linearbeschleunigern zusammenfassung hintergrund . 
primo , die hier erstmalig vorgestellte monte - carlo - benutzeroberflche erlaubt mit wenig aufwand die simulation der meisten linearbeschleuniger der firmen varian und elekta , einschlielich ihrer lamellenkollimatoren und elektronentubusse . 
primo kombiniert ( 1 ) die exakte physik des penelope - kodes , ( 2 ) ausgesuchte und fr diese spezielle anwendung entwickelte varianzreduzierende techniken , die erheblich die rechenzeit verkrzen und ( 3 ) eine nutzerfreundliche graphische benutzeroberflche mit einfach zu bedienenden werkzeugen zur analyse der simulationsergebnisse . 
die berechnung der dosisverteilung bei einer voxelgre von 1 , 863 , 001 , 86 mm3 mit einer durchschnittlichen statistischen unsicherheit von 2% bentigt mit einem 8 - kern - intel - xeon 2 , 67 ghz prozessor 1 , 8 h . 
primo ist eine in sich abgeschlossene , eigenstndige , nutzerfreundliche bedienungsoberflche , die eine einfache durchfhrung exakter monte - carlo - simulationen der dosisverteilungen der meisten gngigen medizinischen linearbeschleuniger erlaubt . 
this is done by using the threshold method [ 20 ] interactively aided by the display of a frequency histogram of hounsfield units and of density maps superimposed to the material maps . 
there are 40 materials available for the creation of voxelized geometries . structures such as planning target volumes or organs at risk can be delineated in the computerized tomography volume and used to calculate dosevolume histograms . 
three segments are predefined , namely , the fixed upper components , the movable components of the linac and the dose tallying geometry ( binned phantom or voxelized tomography )  . 
this feature is useful for particle contamination studies or for further optimization of the simulation . dose estimation results are presented as 3d dose distributions superimposed to the computerized tomography volume or phantousers can navigate these volumes through axial , coronal , and sagittal slices . 
a useful feature of primo is the possibility of importing experimental data from a dosimetry systesimulated and experimental data are compared by means of dose profiles , differential plots , and the gamma test [ 11 ]  . an example : prostate irradiation in this section we describe the steps involved in creating and simulating a typical radiotherapy treatment plan with primo . 
a simulation of the upper part of the linac , a varian clinac 2100 c / d , from the primary electron source downstream to a plane located upstream of the jaws was launched . 
therefore , the time devoted to this segment , although reported , is not taken into account to compute the total simulation time . prior to field setup , the set of images stored in dicom - ct format was imported into primo and the corresponding voxelized geometry was generated . 
the planning target volumes and the organs at risk where delineated with primo , including the prostate gland , and the rectum and bladder , respectively . a second simulation segment including the jaws and the multileaf collimator was configured and run . 
the shape of the fields were conformed to that of the prostate gland planning target volume by using a high definition millenium multi leaf collimator ( mlc 120hd ) as shown in .fig.2. 
columns s1 , s2 , and s3 correspond to the simulation time required for segments 1 ( s1 , upper part of the linac ) , 2 ( s2 , lower part of the linac ) , and 3 ( s3 , water phantom or computerized tomography ) , respectively . 
in the case of the truebeam simulation we used the phase - space file distributed by varian for a 6 mv free flattening filter ( fff ) beam , which was tallied just above the jaws . 
in general , s1 is simulated once and for all linac 2100 c / d 2100 c / d 2100 c / d 2100 c / d 2100 c / d unique truebeam sl / i sl / i 2100 c / d mode photon photon photon photon electron photon photon photon electron photon energy 6 mv 18 mv 6 mv 6 mv 6 mev 6 mv 6 fff 6 mv 6 mev 6 mv field 1010 1010 2020 1010 1010 1010 1010 1010 8 fields s2 + s3 ous simulation segment was used as the source of particles . 
regions that will absorb nearly all charged particles are defined as nonskins and the absorption energies of these particles are accordingly set higher in order to avoid a waste of computation time . 
the combined simulation time of segments 2 ( jaws and multileaf collimator 120hd ) and 3 ( computerized tomography ) was 1.8 h , reaching an overall relative standard uncertainty of 2% . in order to put into perspective the simulation time needed for prostate irradiation , we computed the dose distribution in a water phantom for several reference fields . 
it is interesting to note that the computation of the dose in the water phantom for the 1010 cm2 reference field with 6 mv photons takes a time ( 0.9 h ) comparable to that ( 1.8 h ) required for the case of the tomographic volume . 
 this fact indicates that the algorithm handling voxelized structures is efficient and that due to usage of movable skins in the multileaf collimator geometry the time employed in the simulation of this complex structure is moderate . the minimum statistical uncertainty of the absorbed dose that can be reached with a given phase - space file is conditioned by the latent variance [ 18 ] associated to this phase - space file . 
 [ 18 ] , it can be derived that the variance , 2 , of the absorbed dose obtained from a monte carlo simulation of a linac can be expressed as the quantities c1 and c2 , 3 are independent from the simulation time . 
fernndez - varea jm , carrasco p , panettieri v , brualla l ( 2007 ) monte carlo based water / medium stopping power ratios for various icrp and icru tissues . 
sempau j , wilderman s , bielajew a ( 2000 ) dpm , a fast , accurate monte carlo code optimized for photon and electron radiotherapy treatment planning dose calculations . 
the authors gratefully acknowledge varian medical systems international ag ( zug , switzerland ) and elekta limited ( crawley , united kingdom ) for authorizing the distribution of the encoded geometry files related to their linac models . 
 brualla state that there is no conflict of interest . the accompanying manuscript does not include studies on humans or animals . literaturkommentiert strahlenther onkol 2013 189 : 706707 doi 10.1007 / s00066 - 013 - 0382 - 6 online publiziert : 5 july 2013 springer - verlag berlin heidelberg 2013 o.ganslandt neurochirurgischen klinik , universittsklinikum , erlangen spteundverzgerte pseudoprogressionenim seriellenposttherapeutischen mrtdurcheinfhrungneuer chemotherapiekonzeptebeider behandlungmalignergliome originalbeitrag stuplich m , hadizadeh dr , kuchelmeister k et al ( 2012 ) late and prolonged pseudoprogression in glioblastoma after treatment with lomustine and temozolomide . 
nur wenn im weiteren verlauf eine weitere signifikante kontrastmittelzunahme und / oder vergrerung in den flair - sequenzen eintritt , sollte ein tumorprogress angenommen und dann die primrtherapie beendet werden . 
die autoren fhren das spte auftreten von pseudoprogression auf mgliche langzeiteffekte von lomustin zurck und zitieren fr diese annahme eine studie von 21 patienten , bei denen procarbazin , ccnu und vincristin gegeben wurde und bei denen in 60% ein sptes und stabiles ansprechen auch nach einem median von 2 , 7 jahren nach therapieende gefunden wurde . kommentar durch die einfhrung neuer chemotherapiekonzepte bei der behandlung maligner gliome stehen neuroonkologen erstmals vor dem dilemma , dass bisher unbekannte verlufe und vernderungen im seriellen posttherapeutischen mrt beobachtet werden , die das monitoring zunehmend erschweren . 
second - line - therapie knnen den berlebensvorteil durch die inzwischen weitgehend standardisierten neuen therapiekonzepte gefhrden . die bisher angewandten mcdonaldkriterien [ 2 ] fr die einschtzung des ansprechens von gliomen auf die therapie sind seit der einfhrung neuer chemotherapien nicht mehr valide . 
auch wenn die in dieser studie beobachtete patientenzahl sehr klein ist und die arbeit allenfalls als beobachtungsstudie eingestuft werden kann , so mssen wir als klinisch ttige neuroonkologen gewahr sein , dass die entscheidung fr einen abbruch der therapie anhand der rano - kriterien nicht immer gerechtfertigt ist . 
 ihre persnliche merkliste finden sie einen beitrag besonders interessant oder mchten sie ihn fr die sptere lektre vormerken ? auf springermedizin.de knnen sie ganz einfach ihre persnliche merkliste anlegen : ein klick auf das symbol merken am beitragsende gengt und die beitrge erscheinen unter meine merkliste . 
lernen sie die vorzge dieses umfassenden angebots kennen und testen sie e.med 30 tage lang kostenlos und unverbindlich unter eine erfolgreiche recherche wnscht ihnen ihr redaktionsteam fachzeitschriften von springer medizin suchen sie beitrge in einer bestimmten fachzeitschrift ihres fachgebiets ? oder mchten sie englischsprachige journals fr eine interdisziplinre recherche nutzen ? interessieren sie sich fr bersichtsbeitrge oder aktuelle wissenschaftliche studien ? die e.bibliothek wird all diesen anforderungen gerecht : sie umfasst ber 600 deutschsprachige und internationale fachzeitschriften aus allen bereichen der medizin inklusive der medizinischen inhalte von springerlink . 
a key mechanism of mitochondrial inactivation in cancers is inhibition of the enzyme pyruvate dehydrogenase ( pdh ) , which normally converts pyruvate to acetyl - coa to be utilized in the citric acid cycle , by pyruvate dehydrogenase kinase ( pdk )  . 
dca has been shown to shift metabolism from glycolysis to glucose oxidation , to induce apoptosis by lowering the high mitochondrial membrane potential ( m ) and activating kv channels , and to inhibit tumor cell growth [ 3 , 9 , 11 ]  . 
for years , the compound has been in clinical trials as a treatment for certain pediatric mitochondrial diseases with only mild peripheral neuropathies , but it is not approved for cancer treatment . 
a recent study with xenografts from two human squamous cell carcinomas ( hscc ) of the head and neck and one human colorectal adenocarcinoma could not show an effect on tumor growth ( or lactate or hypoxia levels ) of modifiers of glycolysis , although the respective substances had a significant influence on tumor cell metabolism in vitro [ 22 ]  . 
high tumor lactate levels are known to correlate strongly with radioresistance [ 13 , 14 ] , thus the concept of metabolic targeting needs to be investigated in combination with radiotherapy , where apoptosis induction is frequently compromised ( due to mitochondrial dysfunction )  . 
recently , radiosensitization of prostate cancer cells by dca could be demonstrated and was accompanied by a decreased m and an increased rate of apoptosis . in the present study we investigated the in vitro radiosensitization by dca in both normal tissue and tumor cell lines ( assessed in terms of clonogenic survival and apoptosis induction )  . 
additionally , a human colon adenocarcinoma xenograft was assessed for dca response ( growth inhibition ) and induction of hypoxia upon dca treatment ( pinomidazole labeling )  . materials and methods cell lines and culture conditions the origins and culture conditions pertaining to the human cell lines mrc5 ( lung fibroblasts ) , widr ( colon adenocarcinoma ) and ln18 ( glioblastoma ) were described recently [ 25 ]  . 
human umbilical vein endothelial cells ( huvec ; promocell , heidelberg , germany ) were maintained in culture at 37c with 5% co2 in serum - reduced ( 5% fetal calf serum ) modified promocell medium supplemented with 2 ng / ml vascular endothelial growth factor ( vegf ) and 4 ng / ml basic fibroblast growth factor ( bfgf ) and subcultured up to passage 8 . 
b , c , d radiation dependent clonogenic survival of human normal tissue cell lines tk6 ( b ) , mrc5 ( c ) and huvec ( d ) in the presence of 0.1 or 1 mm dca added 6 h prior to irradiation . 
data points represent mean values and standard deviations of at least three independent determinations drug treatment and irradiation clonogenic assay dca stock solutions of 1 mm / 10 mm ( sigmaaldrich ) were diluted in h2o for in vitro experiments and in 1x phosphate buffered saline ( pbs ) for in vivo experiments . 
clonogenic survival of the tk6 cells in suspension was examined using the microtiter plate dilution assay , as described previously [ 15 ]  . apoptosis measurement treated cells , including the culture supernatant , were harvested 24 , 48 and 72 h postirradiation and prepared for sub - g1 dna flow cytometry with propidium iodide staining [ 15 ]  . 
additionally , widr and ln18 cells grown on microscopic slides were stained with 4 , 6 - diamidino - 2 - phenylindol ( dapi ) 48 and 72 h posttreatment . 
the nuclei were inspected for the typical morphological appearance strahlentherapieundonkologie82013 | abstract zusammenfassung strahlenther onkol 2013 189 : 684692 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0354 - x f.zwickera.kirsnerp.peschkef.roederj.debusp.e.huberk.j.weber dichloroacetate induces tumor - specific radiosensitivity in vitro but attenuates radiation - induced tumor growth delay in vivo abstract background . 
inhibition of pyruvate dehydrogenase kinase ( pdk ) by dichloroacetate ( dca ) can shift tumor cell metabolism from anaerobic glycolysis to glucose oxidation , with activation of mitochondrial activity and chemotherapy - dependent apoptosis . 
the interaction of dca with photon beam radiation was investigated in the human tumor cell lines widr ( colorectal ) and ln18 ( glioma ) , as well as in the human normal tissue cell lines huvec ( endothelial ) , mrc5 ( lung fibroblasts ) and tk6 ( lymphoblastoid )  . 
dca treatment led to decreased clonogenic survival and increased specific apoptosis rates in tumor cell lines ( ln18 , widr ) but not in normal tissue cells ( huvec , mrc5 , tk6 )  . 
however , this significant tumorspecific radiosensitization by dca in vitro was not reflected by the situation in vivo : the growth suppression of widr xenograft tumors after irradiation was reduced upon additional dca treatment ( reflected by ki67 expression levels ) , although early tumor cell apoptosis rates were significantly increased by dca . 
further investigations relating to the interplay between tumor cell metabolism and tumor microenvironment are necessary to explain the limited success of metabolic targeting in radiotherapy . keywords citric acid cycle glycolysis irradiation hypoxia apoptosis tumorspezifische radiosensibilisierung durch dichloracetat in vitro bei verminderung der strahlungsinduzierten tumorwachstumsverzgerung in vivo zusammenfassung hintergrund . 
eine inhibition der pyruvatdehydrogenase ( pdk ) durch dichloracetat ( dca ) kann zu einer verschiebung des tumorzellstoffwechsels von der anaeroben glykolyse zur glukoseoxidation mit aktivierung der mitochondrienaktivitt sowie der chemotherapieabhngigen apoptose fhren . 
die interaktion von dca und photonenstrahlen wurde an den humanen tumorzelllinien widr ( kolorektal ) und ln18 ( gliom ) sowie an den normalgewebszelllinien huvec ( endothelial ) , mrc5 ( lungenfibroblasten ) und tk6 ( lymphoblastoid ) untersucht . 
dca fhrt nur in den tumorzelllinien ( ln18 , widr ) , nicht aber in den normalgewebszelllinien ( huvec , mrc5 , tk6 ) zu einem verringerten klonogenen berleben sowie einer gesteigerten spezifischen apoptoserate und somit zu einer signifikanten tumorspezifischen radiosensibilisierung in vitro . 
umgekehrt war die wachstumsverzgerung von widr - xenograft - tumoren nach bestrahlung durch eine zustzliche dcabehand lung , korrespondierend mit der ki - 67expession , geringer ausgeprgt , obwohl die frhe tumorapoptose durch dca signifikant gesteigert wurde . 
 weitere untersuchungen des komplexen zusammenspiels zwischen dem tumorzellstoffwechsel und der tumormikroumwelt sind notwendig , um den begrenzten erfolg des metabolic targeting in der strahlentherapie zu erklren . schlsselwrter zitronensurezyklus glykolyse bestrahlung hypoxie apoptose of chromatin condensation during late apoptosis by means of fluorescence microscopy ( 100x magnification and manual focal plane scanning )  . western blot western blot analysis was performed according to standard protocols , as reported previously [ 1 ]  . 
in brief , following 48 h of dca treatment ( 1 mm ) , ln18 cells were lysed in lysis buffer comprising 1% pmsf ( sigma ) and 4% complete ( roche diagnostics , basel , switzerland ) in stock solution ( 50 m tris - hcl ph = 8 , 120 mm nacl , 5 mm edta ph = 8 , np40 ( 0.5% ) in distilled water ) protein concentrations were assayed by the bradford method [ 2 ]  . 
 protein extracts ( 90 g ) underwent elec686 | strahlentherapieundonkologie82013 ln18 widr control dca 0.1mm dca 1mm control dca 0.1mm dca 1mm dose ( gy ) dose ( gy ) fig . 
2 8 radiation - induced inhibition of clonogenic survival of human tumor cell lines ln18 and widr in the presence of 0.1 or 1 mm dca added 6 h prior to irradiation compared to mock - treated controls . 
the membranes were then incubated for 1 h in blocking buffer ( 5% skimmed milk in pbs - tween ) , followed by incubation with caspase 3 specific primary rabbit antibodies ( cell signaling technology , boston , usa ) at a 1 : 1000 dilution at 4c for 24 h to detect procaspase 3 ( 35 kda ) and the cleavage fragment ( 17 kda )  . 
after being washed four times with tbs - tween buffer , the membrane was incubated with anti - rabbit igg secondary antibody from goat conjugated with horseradish peroxidase ( biorad ) at a 1 : 15 , 000 dilution for 1 h at room temperature . 
the signals were visualized with the supersignal west dura trial kit ( pierce biotechnology inc . , roxford , il , usa ) and autoradiography . xenograft tumor model animal studies were performed according to the rules governing the care and use of experimental animals and were approved by the local and governmental animal care committees . 
widr xenografts were established by injecting 5106 widr cells subcutaneously into the right hind limb of 68 - weekold athymic balb / c nude mice weighing 20 g ( charles river laboratories , sulzfeld , germany )  . 
animals were then randomized into the following four groups : control , dca only , irradiation only , and dca plus radiation ( 16 mice per group , with 3 mice per group scheduled for histology on days 4 and 20 after treatment start )  . 
dca was administered intraperitoneally in pbs ( 150 mg / kg or 3 mg / 20 g or 1 mm ) twice daily for five consecutive days ( days 04 )  . 
tumors were irradiated using a fractionated schedule ( 52 gy ) for five consecutive days beginning on day 0 ( days 04 ) ; all other parts of the mice were spared . immunohistology for the detection of tissue hypoxia ( after 4 days of dca treatment ) , 100 l of pimonidazole hydrochloride ( hypoxyprobe 1 ; chemicon , emd millipore corporation , billerica , ma , usa ) was injected into the tail vein at a dose of 60 mg / kg . 
proliferation , apoptosis and tissue hypoxia were detected by indirect immunofluorescence techniques with frozen sections according to standard protocols . for hypoxia immunofluorescence , cryostat sections ( 6 m ) were fixed with methanol ( 1 min ) and acetone ( 2 min ) at 20c . 
pimonidazole binding was detected by mab1 ( 1 : 50 dilution ; npi solutions inc , san jose , ca , usa ) , followed by an alexa flour 488 conjugated secondary antibody ( 1 : 400 dilution ; invitrogen , carlsbad , ca , usa )  . 
sections were double stained with cd31 ( 1 : 100 dilution ; bd biosciences , san jose , ca ) followed by an alexa fluor 555 conjugated secondary detection system ( 1 : 400 dilution ; invitrogen )  . 
the mean pimonidazole enrichment in tumor was determined by measuring and averaging the pimonidazole fluorescence intensity of each section . for assessment of proliferation by ki67 staining , methanol / acetone fixed cryostat sections ( 6 m ) were incubated with ki67 antibody ( 1 : 50 dilution ; abcam , cambridge , uk ) followed by an alexa fluor 555 labeled goat anti - rabbit antibody ( 1 : 200 dilution ; invitrogen )  . 
3 8 radiation - dependent specific apoptosis in the human normal tissue cell lines mrc5 ( 4 and 8 gy ) , huvec ( 4 gy ) and tk6 ( 1.5 gy ) in the presence of 0.1 or 1 mm dca added 6 h prior to irradiation . 
the cell density per region of interest was determined by counting dapi stained nuclei . digital fluorescent images were obtained using a nikon eclipse e600 mi688 | strahlentherapieundonkologie82013 croscope ( nikon , duesseldorf , germany ) equipped with a nikon digital sight ds - u1 camera . results statistical analysis differences between experimental groups were analyzed for statistical significance using a students t - test . 
4 8 radiation - induced increase in specific apoptosis in human tumor cell lines ln18 ( a ) and widr ( b ) irradiated with 4 and 8 gy in the presence of 0.1 or 1 mm dca added 6 h prior to irradiation . 
apoptosis rate was measured by detecting chromatin condensation by dapi staining 48 and 72 h after radiation or analyzing the sub - g1 population by flow cytometry 24 , 48 and 72 h after radiation . 
data points represent mean values ; bars standard deviations . * indicates statistical significance ( p < 0.05 ) strahlentherapieundonkologie82013 | original article caspase 3 ln18 legend : in vivo radiation effects in the widr xenograft tumor model fig . 
5 8 western blot analysis of caspase 3 ( procaspase 3 , 35 kda ; cleavage fragment , 17 kda ) in dcatreated ln18 cells 48 h after radiation ( 8 gy ) control group dca group rt group dca + rt group wird / mouse 1 . 
dca treatment was performed twice daily with 150 mg / kg ( 1 mm dca injected intraperitoneally , days 04 ) ; fractionated irradiation was applied to the tumor in daily 2 gy fractions ( days 04 ) to a cumulative dose of 10 gy . 
 * indicates a statistically significant difference ( p < 0.05 ) in vitro radiation sensitivity dca ( 0.1 or 1 mm ) had no influence on clonogenic survival after irradiation of the normal tissue cell lines huvec , mrc5 and tk6 ( .fig.1b , c , d )  . 
this differential response of normal tissue compared to tumor cell lines was paralleled by the results of apoptosis measurements by both the sub - g1 analysis and dapi staining ( .fig.3 for the normal tissue cell lines ; .fig.4 for ln18 and widr cells )  . 
7 8 a immunohistochemical evaluation of each treatment ( control , dca alone , radiation therapy alone , dca combined with radiation therapy ) on cell proliferation and apoptosis in widr xenografts . 
tumors were excised and processed as described in materials and methods discussion we found a tumor - specific dca enhancement of radiosensitivity in vitro that did not translate into improved radiation - induced tumor growth delay in vivo . 
the explanation for this puzzling finding is that the increased in vitro radiosensitivity caused by dca in tumor cells is achieved under conditions of sufficient oxygen and adequate glucose supply . 
the demonstration that dca ( 0.5 mm ) reversed this glycolytic phenotype and depolarized mitochondria in cancer but not normal tissue cell lines under normoxic in vitro conditions [ 3 ] is in line with our in vitro results , which demonstrate increased apoptosis upon radiation treatment . 
the only other investigation that has tested the concept of metabolic targeting with radiation treatment used in vitro prostate cancer cells , with a specific emphasis on the role of bcl - 2 family members [ 7 ]  . 
 to some extent , this limits the interpretation of the present results , although the activity of dca as a specific pdk inhibitor has been shown in many experimental model systems [ 10 ]  . however , much of the subsequent work on dca cytotoxicity in vitro has led to a less clear picture , with the emerging view that the limited anticancer effect of dca in vitro may reflect the massive excess of metabolites in cell culture media and that in vitro experimentation in metabolic targeting research may be insufficient at the least [ 10 ]  . strahlentherapieundonkologie82013 | original article our in vivo data from histological examinations of the widr xenograft tumors at early times after irradiation ( 4 days ) showed increased apoptosis rates and diminished cell mitosis activity , which corresponds to the postulated efficacy of dca in targeting pdk and thus restoring mitochondrial function . 
increased hypoxia caused by dca treatment has been described previously for colorectal cancer [ 5 , 6 ] , but was not described for the widr xenograft model used in a more a recent study [ 22 ]  . 
to further dissect the effects of dca on tumor oxygenation and physiology , as well as to assess the effects of its combination with radiation , future studies might combine dca with irradiation in a slow - growing , highly vascularized animal tumors . 
our data may reflect the complicated interaction of isolated cell - specific effects with the microenvironment and the physiological tumor response to radiation and drugs [ 8 , 23 ]  . 
surgery alone is usually associated with a low probability of cure because of both the high risk of close or positive microscopic margins associated with the extralaryngeal extent of the primary tumor and the high incidence of cervical lymph node metastases [ 13 ]  . 
however , in some advanced - disease cases , highdose radiotherapy is attempted when the patient does not consent to total laryngectomy or is unsuitable for general anesthesia , and these two situations are frequently encountered in poland [ 26 , 43 , 45 ]  . although the treatment results of radiotherapy alone in advanced laryngeal cancer are generally worse than after surgery followed by radiation , some clinical studies have shown that t4 laryngeal cancer is a heterogeneous tumor with regard to radiocurabilitythe cure rates range from 10% up to 80% of local tumor control [ 28 , 29 , 45 ]  . 
besides the well - known prognostic factors such as the patients performance status and the type of cancer infiltration ( exoor endophytic ) , an important prognosticator could be the tumors primary location being in the larynx . 
when compared with glottic lesions , the cancer cells of supraglottic lesions usually do not keratinize and are less differentiated ( g23 ) , which implies having a more aggressive tumor growing to a larger volume of the primary tumor and metastases [ 11 , 30 , 47 , 50 ]  . 
the other adverse features are cartilage invasion and subglottic extension of the tumor as well as emergency tracheostomy [ 27 , 36 , 37 ]  . during 19472000 , the institute of oncology maria sklodowska - curie cancer center in gliwice , poland , was an institution using radiation treatment within the upper silesia region of 5 million inhabitants . 
the highest incidence of laryngeal cancer in poland is found in this region ; the standardized average morbidity ratio is 13.2 cases for 100 , 000 inhabitants per year [ 51 ] and the number of laryngeal cancer patients treated with radiation therapy alone often exceeds 100 / year . 
the purpose of this retrospective study is to report the efficacy of high - dose radiotherapy alone in 114 patients with t4 advanced laryngeal cancer , who were treated during the relatively short period of 7 years ( 19901996 ) before the conformal radiation era , and to establish the prognostic value of the size and location of the extralaryngeal tumor extensions as well as of emergency tracheostomy . 
we also attempt to assess the efficacy of the ajcc - 1998 tnm laryngeal cancer classification . patients and methods our group of 114 patients with t4 stage of squamous cell laryngeal cancer accounts for about 10% of all cases of laryngeal cancer treated with definitive radiotherapy in the period 19901996 . 
in most cases ( 68% ) the performance status ( ps ) was assessed as very good ( zubrod 0 ) and the remaining patients were scored as zubrod 1 ps . clinical stage was established on the basis of indirect and direct examination of the larynx according to the tnmajcc system in which t4 tumors were qualified according to their extension beyond the larynx : soft tissue invasion of the neck , extension to the oropharynx or esophagus , or destruction of thyroid and / or cricoid cartilage . 
in the tnm - ajcc classification of 1998 , tumors of the supraglottis invading the mucosa of the base of the tongue , the valleculae , and the medial wall of the piriform recess without vocal cord fixation are staged as a t2 . 
1 distribution of patients with t4 laryngeal cancer prognosticfactor localization status of neck nodes tracheostomy performance status ( zubrod ) m male , f female category median minimum maximum supraglottis glottis numberofpatients 102 ( 89% ) 12 ( 11% ) 57 years 108 ( 95% ) 6 ( 5% ) 55 ( 48% ) 21 ( 19% ) 33 ( 29% ) 5 ( 4% ) 16 ( 14% ) 98 ( 86% ) 78 ( 68% ) 33 ( 29% ) 3 ( 3% ) tab . 
2 distribution of clinical material in t4 laryngeal cancer according to the extent of neck node involvement ( n ) localization supraglottis glottis total extentofnecknodeinvolvement ( numberofpatients ) 51 ( 45% ) 4 ( 3% ) 55 ( 48% ) 21 ( 19% ) 21 ( 19% ) 31 ( 27% ) 2 ( 2% ) 33 ( 29% ) 5 ( 4% ) 5 ( 4% ) total 108 ( 95% ) 6 ( 5% ) 114 ( 100% ) tab . 
3 results of univariate analysis of the relationship between selected clinical factors and 3 - year dfs , lc , and os rates in patients with t4 laryngeal cancer clinicalfactor category 3 - yearlc 3 - yeardfs 3 - yearos localization neck nodes involvement tracheostomy extralaryngeal infiltration supraglottis glottis cartilage hypopharyngeal wall piriform recess base of tongue + glossoepiglottic vallecula piriform recess + glossoepiglottic vallecula + base of tongue 50% ns 50% ns 50% p = 0.067 0% p = 0.000 56% p = 0.034 42% ns 50% ns 45% p = 0.105 0% p = 0.000 51% p = 0.068 59% ns 50% ns 54% p = 0.000 6% p = 0.000 54% p = 0.024 lc local control , dfs disease - free survival , os overall survival tumor infiltration is with helical computed tomography ( ct )  . 
in 16 cases ( 14% ) , emergency tracheostomy was performed before radiation treatment . in the case of extralaryngeal infiltration , the whole piriform recess was most often involved ( in 37 cases ; 33% ) , the base of the tongue and glosso - epiglottic vallecula were both involved in 34 cases ( 30% ) , whereas the hypopharyngeal wall was involved in only 10 cases ( 9% )  . 
clinically uninvolved neck nodes were electively irradiated to a total dose of 50 gy given in 25 fractions at a depth of 2.5 cposterior neck nodes ( level ivv ) were treated with adequate electron fields matched to parallel photon fields . 
in the rest of the 34 patients there were longer gaps lasting at least 3 days or more , caused by severe reactions or other disorders . the main end points of this analysis were : 3 - year local control ( lc ) , diseasefree survival ( dfs ) , and overall survival ( os )  . 
the piriform recess was involved in 37 cases ( 33% ) , the base of the tongue and glosso - epiglottic vallecula in 34 cases ( 30% ) , and the hypopharyngeal wall in 10 cases ( 9% )  . 
actuarial 3 - year local control ( lc ) was noted in 42% of patients , disease - free survival ( dfs ) in 35% , and overall survival ( os ) in 40% . 
emergency tracheostomy is a prognostic factor connected with the worst prognosis . keywords laryngeal cancer radiotherapy extralaryngeal infiltrations emergency tracheostomy prognosis alleinige hochdosierte strahlentherapie bei patienten mit larynxkarzinom im stadium t4 zusammenfassung hintergrundundziel . 
der recessus piriformis war in 37 fllen ( 33% ) , der zungengrund mit vallekula in 34 ( 30% ) und die hypopharynxwand in 10 fllen ( 9% ) betroffen . 
die aktuarische 3 - jahres - lokalkontrollrate ( lc ) betrug 42% fr alle patienten , die krankheitsfreie berlebensrate ( dfs ) 35% und die gesamte 3 - jahres - berlebensrate ( os ) 40% . 
os , dfs , and lc were found to be higher in female than in male patients ( 21 , 7 , and 10% , respectively ) ; however , these differences were not significant . 
the presence of involved neck nodes worsened the likelihood of cureall rates decreased along with increasing n stage , from approximately 50% ( n0 ) to 0% ( n3 )  . 
os overall survival salvage treatment ( total laryngectomy ) was performed on 14 patients ( 20% ) in whom there was treatment failure after radiotherapy . radiotherapy was quite well tolerated . 
all survivors had a good voice quality . discussion our study conducted in a relatively large group of 114 patients revealed that conventional radiotherapy of advanced laryngeal cancer ( t4 n0 - 3 ) is a method of limited effectiveness . 
some authors suggest that higher total doses of radiation may lead to a negligible increase in the probability of cure but at the cost of an increased risk of radiationinduced complications . 
thus , patients with advanced laryngeal cancer have been treated surgically , and radiotherapy has been considered as an adjuvant method for these patients [ 5 , 16 , 45 ]  . generally , radiotherapy alone achieves an lc rate below 50% in this group of patients , and our results are consistent with the data in the literature [ 1 , 10 , 14 , 15 , 19 , 20 , 33 , 39 ]  . 
 [ 14 ] , in a group of 56 patients with t4n0 laryngeal cancer , found 49% 5 - year dfs after radiotherapy and salvage surgery . the extent of neck node involvement ( n + ) significantly worsens the prognosis of radiation cure . 
the risk of neck node metastases is higher in supraglottic cancer , and the results of our study are comparable with many data from the literature [ 22 , 25 , 40 , 46 ]  . 
 [ 45 ] drew attention to the necessity of larger - field irradiation , including the larynx with upper neck nodes , in all patients with supraglottic cancer . the assessment of five directions of extralaryngeal infiltration showed that the least unfavorable prognostic factor was the suspicion of cartilage infiltration ( 56% 3 - year lc )  . 
the significantly lowest lc rate ( 13% ) was noted in the case of massive infiltration including anatomical structures of the hypopharynx ( piriform recess ) and oropharynx ( base of tongue )  . 
 it seems that the unexpectedly good results achieved in the group of patients in whom cartilage infiltration was suspected may be explained as a misdiagnosis of this symptom ( during that time there was no possibility to perform ct examination on all patients )  . 
however , the low percentage of lc rates in the patients with piriform recess and infiltration of the base of the tongue is probably connected to a large mass of frequently ulcerated tumor , strahlentherapieundonkologie82013 | original article tab . 
4 three - year lc in patients with t4 laryngeal cancer according to treatment gap duration 3 - yearlc gapduration 02 days 3 days lc local control , dfs disease - free survival , os overall survival 3 - yeardfs 3 - yearos tab . 
performing these examinations before treatment may help select patients with favorable tumors ( exophytic 636 | strahlentherapieundonkologie82013 and superficial infiltrations in the larynx ) , who have a relatively high chance for cure with voice preservation after radiotherapy alone or chemoradiotherapy [ 12 , 29 , 35 , 41 , 50 ]  . 
emergency tracheostomy may lead to local recurrence in the stoma region , because of inoculation of neoplastic cells during this surgical procedure [ 27 , 36 , 37 ]  . 
it seems obvious that emergency tracheostomy could be generally connected with several other factors such as poor performance status , bulky mass of primary tumor , deep infiltration , and destruction of adjacent structures , which most often means higher tumor radioresistance [ 38 ]  . the analysis of our data ( .tab.1 ) and the literature review [ 29 ] draw attention to the small number of patients with stage t4 glottic cancer treated with radiation alone . 
therefore , it is usually difficult to establish a glottic or supraglottic origin in advanced primary tumor . our analysis also draws attention to the very small number of patients who underwent salvage surgery after radiotherapy alone . 
nevertheless , there is no doubt that this is a serious clinical problem that may need more frequent follow - up , especially during the first 12 months after treatment , and may require more effective methods of early detection of postradiotherapy failures . 
 [ 29 ] , salvage surgery was done in the majority of patients with uncured primary tumor or locoregional recurrence , which significantly improved the ultimate treatment results in patients with advanced laryngeal cancer . careful analysis of the extent of extralaryngeal infiltrations led us to attempt to reclassify the tumor stage . 
in the group of patients with piriform recess extension , we found that in 27 cases ( 73% ) there were massive oneor two - sided infiltrations of the whole recess , with presence of necrosis and vocal cord fixation . 
similarly , with the glosso - epiglottic vallecula and base of the tongue infiltrations , there were 28 cases ( 82% ) of massive infiltration , often with the presence of necrosis and fixation of one or two vocal cords . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 704705 doi 10.1007 / s00066 - 013 - 0386 - 2 online publiziert : 21 . 
juni 2013 springer - verlag berlin heidelberg 2013 m.wilhelm medizinische klinik 5 , nrnberg risikovonvensen thromboembolienbei tumorpatienten , diemit cisplatinbehandeltwerden systematischerreviewundmetaanalyse originalpublikation seng s , liu z , chiu sk et al ( 2012 ) risk of venous thromboembolism in patients with cancer treated with cisplatin : a systematic review and meta - analysis . 
die inzidenz der vtes lag bei 1 , 92% ( 95% ci : 1 , 072 , 76 ) bei patien ten mit cisplatinbasierter chemothera pie und bei 0 , 79% ( 95% ci : 0 , 451 , 13 ) bei patienten , die kein cisplatinbasiertes re gime erhielten . 
patienten mit cisplatinba sierter chemotherapie hatten ein signifi kant erhhtes risiko von vtes ( rr , 1 , 67 ; 95% ci : 1 , 252 , 23 ; p = 0 , 01 )  . 
eine cisplatinbasierte chemotherapie ist bei patienten mit fortgeschrittenen soliden tumorerkrankungen mit einem signifi kant hheren risiko fr vtes vergesell schaftet . krebspatienten haben durch die erkran kung ein 4 bis 8fach erhhtes risiko fr vense thrombembolische ereignisse im vergleich zur altersentsprechenden kon trollgruppe . 
in der hier vorliegenden arbeit wurde jetzt anhand von ber 8000 patienten eindrcklich gezeigt , dass cisplatin das risiko fr das auftreten von vtes zustzlich erhht [ 1 ]  . 
 im besonderen mae traf dies fr patien ten mit einem magen / sophaguskarzi nom ( rr 4 , 84% ) , pankreaskarzinom ( rr 2 , 10% ) oder kleinzelligen bronchialkarzi nom ( rr 1 , 36% ) zu . 
mittels hochauflsender computer tomographie , zurckzufhren . insgesamt handelt es sich um eine sehr relevante fragestellung , da das auftreten von vensen thrombembolischen ereig nissen nicht nur die morbiditt , sondern auch die letalitt von patienten mit fort geschrittenen tumorerkrankungen er hht . 
die pathogenese der durch cis platin induzierten thrombophilie bleibt schen , europischenundamerikanischenleitliniensolltenabertumorpatientenmitakuterhospitalisierung , bettlgerigkeitoderchirurgischeneingriffengrundstzlicheine thromboseprophylaxeerhalten [ 4 , martin wilhelm , nrnberg korrespondenzadresse prof.dr.m.wilhelm medizinische klinik 5 prof . - ernst - nathan - str . 
seng s , liu z , chiu sk et al ( 2012 ) risk of venous thromboembolism in patients with cancer treated with cisplatin : a systematic review and meta - analysis . 
lyman gh , khorana aa , falanga a et al ( 2007 ) american society of clinical oncology guideline : recommendations for venous thromboembolism prophylaxis and treatment in patients with cancer . 
pabinger i , alt - epping b , demarmels f et al ( 2011 ) vense thrombembolien bei tumorpatienten - onkopedia - leitlinie in kooperation mit der gesellschaft fr thromboseund hmostaseforschung e . 
und der deutschen gesellschaft fr palliativmedizhmostaseologie 31 : 281290 aber weiterhin unklar ; mglich sind en dotheliale schdigungen , eine plttchen aktivierung oder eine hochregulation von prothrombotischen faktoren ebenso wie eine cisplatininduzierte nierenfunk tionsstrung . auffallend ist bei dieser studie si cherlich die relativ niedrige inzidenz von vtes im vergleich zu anderen stu dien mit vte als primrem endpunkt . 
gallen taxane - containing inductionchemotherapy followedbydefinitive chemoradiotherapy outcomeinpatientswithlocally advancedheadandneckcancer radiotherapy ( rt ) and concomitant chemotherapy is currently regarded as the standard of care for unresectable locally advanced squamous cell carcinoma of the head and neck ( hnscc ) with an absolute improvement of 8% in 5 - year survival due to concomitant chemotherapy [ 1 ]  . 
recently , the addition of taxanes to induction chemotherapy was investigated by the trials tax 324 ( induction chemotherapy followed by chemoradiotherapy ) and eortc 24971 / tax 323 ( induction chemotherapy followed by rt ) , which both showed a survival benefit of docetaxel , cisplatin , and fluorouracil ( 5 - fu ; tpf ) vs . 
 results from recently published phase iii trials comparing induction chemotherapy with direct chemoradiation or surgery plus adjuvant chemoradiation , however , failed to demonstrate a survival benefit in favor of induction chemotherapy [ 8 , 9 , 10 ]  . in our clinic , patients were referred for induction chemotherapy in case of bulky and / or rapidly progressive primary tumors or lymph nodes where resection was not feasible . 
we report on the toxicity and oncological outcome after induction chemotherapy with tpf and chemoradiotherapy using cisplatin as concomitant agent in conjunction with state - of - the - art imrt in patients with bulky tumors . patients and methods patients and treatment the data of 40 patients who underwent at least one cycle of induction chemotherapy and were scheduled for definitive chemoradiotherapy between july 2004 and november 2010 were retrospectively analyzed . 
induction chemotherapy consisted of docetaxel at a dose of 75 mg / m2 followed by cisplatin 75 mg / m2 and fluorouracil 1 , 000 mg / m2 as continuous infusion for 4 days . for treatment planning , a dedicated computed tomography ( ct ) scan with intravenous contrast material was used . 
we defined two different risk levels of clinical target volume ( ctv ) : ctv72 comprised all gross tumor with an isotropic margin of 1012 mm and was treated to 72 gy ; ctv54 included elective areas and was treated to 54 gy . 
 the resulting ctvs were expanded to planning target volumes ( ptvs ) by adding a symmetric 3 - mm margthe definition of elective nodal target volumes followed the recommendations proposed by eisbruch et al . 
the prophylactic placement of a percutaneous endoscopic gastrostomy before chemoradiotherapy was recommended to every patient . assessments and evaluations remission after induction chemotherapy was assessed according to who criteria by a dedicated head and neck radiologist . 
additionally , treatment interruptions during chemoradiation and the time of feeding tube in situ were calculated . statistical considerations the primary objective of the study was to assess acute and late rt - related toxicity including treatment gaps during chemoradiotherapy ; secondary objectives were response to induction chemotherapy , locoregional recurrence - free survival ( lrrfs ) , overall survival ( os ) , and relevant influencing factors for lrrfs and os . 
statistical strahlentherapieundonkologie82013 | abstract zusammenfassung strahlenther onkol 2013 189 : 618624 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0397 - z j.o.brmmem.schmckinga.arnoldr.gigerd.rauchd.leiserl.plasswilma.geretschlgerp.ghadjard.m.aebersold taxane - containing induction chemotherapy followed by definitive chemoradiotherapy . 
the data of 40 consecutive patients who underwent induction chemotherapy with docetaxel - containing regimens followed by intensity - modulated radiotherapy ( imrt ) and concomitant systemic therapy for unresectable locally advanced hnscc were retrospectively analyzed . 
induction chemotherapy did not compromise the delivery of full - dose rt ; however , the use of three cycles of concomitant cisplatin was impaired . keywords chemoradiotherapy induction chemotherapy radiotherapy head and neck cancer toxicity taxanhaltige induktionschemotherapie gefolgt von definitiver radiochemotherapie . 
wir haben eine retrospektive analyse von 40 aufeinanderfolgenden patienten mit nichtoperablen , lokal fortgeschrittenen kopf - hals - tumoren durchgefhrt , die eine docetaxelhaltige induktionschemotherapie gefolgt von einer intensittsmodulierten rt ( imrt ) kombiniert mit einer systemischen therapie erhielten . 
complete remission after induction chemotherapy was observed in 4 out of 40 patients ( 10% ) , partial remission in 27 patients ( 68% ) , no change in 8 patients ( 20% ) , and 1 patient was not assessable . 
one patient died during chemoradiotherapy because of a feeding tube - related infection after the first cycle of cisplatin . data for acute and late rt - related toxicity were available for 33 and 27 patients , respectively . 
eight patients ( 23% ) received gastrostomy prior to rt because of swallowing deficits , 12 patients ( 35% ) had prophylactic feeding tube placement at the beginning of rt . 
 the median time of feeding tube in situ was 12 months ( range , 238 months )  . five patients experienced local recurrence ; 1 a local tumor persistence , 2 merely regional recurrence , and 4 patients had both local and regional recurrence . 
besides 3 patients who died before undergoing chemoradiotherapy , 2 patients with deterioration of general condition under induction chemotherapy and 1 patient refusing rt subsequently underwent palliative therapy and eventually died of tumor progression . 
one patient died during chemoradiotherapy of a feeding tube complication and 6 patients died during follow - up , 5 because of tumor progression , 1 of pulmonary disease . oneand 2 - year os was 77 and 71% , respectively , with a median os of 34 months . 
one pawe identified considerable rates of rt - related acute and late toxicities after induction chemotherapy followed by chemoradiotherapy in our selected patient cohort with unresectable locally advanced hnstrahlentherapieundonkologie82013 | original article fig . 
very high rates of acute toxicity have been reported in an analysis of patients undergoing tpf induction chemotherapy followed by 3d conformal chemoradiotherapy with grade 3 skin toxicity in 73% and grade 3 mucosal toxicity in 85% of patients [ 12 ]  . 
recently , a large 622 | strahlentherapieundonkologie82013 retrospective trial showed that both techniques yielded the same locoregional control and overall survival but with significantly less toxicity when using imrt [ 14 ]  . 
this compares favorably to tax 324 , where 21% of patients in the tpf arm did not receive full rt [ 5 ]  . to avoid toxicity - related treatment breaks , use of gastrostomy feeding tubes during irradiation of advanced hnssc is standard in our institution , even though this procedure has been discussed controversially [ 15 ]  . 
in our cohort , only 4 patients ( 12% ) had toxicity - related treatment interruptions of 5 days , known to be associated with decreased survival [ 16 ]  . 
a retrospective analysis of patients treated by the same regimen found results of 5% receiving three cycles , 61% receiving two cycles , and 29% receiving one cycle of concurrent cisplatin [ 12 ]  . 
induction chemotherapy thus seems to impair concomitant chemotherapy with cisplatin , but not the delivery of rt once started . data on late toxicity after induction chemotherapy followed by chemoradiotherapy for hnscc are sparse . 
5 univariate cox regression analysis for risk factors influencing overall survival ( n = 40 ) al , only half of the surviving patients could be assessed for the surrogate parameter of presence of tracheotomy ( 7% ) and feeding tube dependency ( 3% ) [ 20 ]  . 
surgical interventions like debridement or even resection and tracheotomy might become necessary , but were not observed in our patient cohort . in our series after induction chemotherapy , we observed a cr in 10% of patients , pr in 68% of patients , and no change in 20% of patients . 
the percentage of patients with a complete response was 17% in the tpf group [ 5 ]  . we found an lrrfs at 1 and 2 years of 72 and 49% , respectively . 
the tax 324 study group [ 5 ] found a median os of 59 months and a 3 year - os of 62% for stage 4 patients treated with tpf induction . 
older phase iii trials investigating the role of induction chemotherapy found no benefit for local control and os , but a significant decrease in distant failure [ 23 ]  . 
these data need careful interpretation , as patients with an uncontrollable locoregional recurrence are usually not screened for distant metastases . in the current study , we found an os benefit for patients with good response to induction chemotherapy ( p = 0.04 ) , with a trend regarding locoregional control . 
the better os in spite of nonsignificant differences in lrrfs for good response might be related to the fact that patients with good remission had longer survival with palliative chemotherapy ( 4 patients ) and rt ( 2 patients ) the most important influence on strahlentherapieundonkologie82013 | 16 . 
fesinmeyer md , mehta v , blough d et al ( 2010 ) effect of radiotherapy interruptions on survival in medicare enrollees with local and regional head - and - neck cancer . 
bourhis j , sire c , graff p et al ( 2012 ) concomitant chemoradiotherapy versus acceleration of radiotherapy with or without concomitant chemotherapy in locally advanced head and neck carcinoma ( gortec 99 - 02 ) : an open - label phase 3 randomised trial . 
van gestel d , van den weyngaert d , schrijvers d et al ( 2011 ) intensity - modulated radiotherapy in patients with head and neck cancer : a european single - centre experience . 
lorch jh , goloubeva o , haddad ri et al ( 2011 ) induction chemotherapy with cisplatin and fluorouracil alone or in combination with docetaxel in locally advanced squamous - cell cancer of the head and neck : long - term results of the tax 324 randomised phase 3 trial . 
ghadjar p , simcock m , studer g et al ( 2012 ) concomitant cisplatin and hyperfractionated radiotherapy in locally advanced head and neck cancer : 10 - year follow - up of a randomized phase iii trial ( sakk 10 / 94 )  . 
studer g , lutolf um , el - bassiouni m et al ( 2007 ) volumetric staging ( vs ) is superior to tnm and ajcc staging in predicting outcome of head and neck cancer treated with imrt . 
studer g , seifert b glanzmann c ( 2008 ) prediction of distant metastasis in head neck cancer patients : implications for induction chemotherapy and pretreatment staging ? strahlenther onkol 184 : 580 24 . 
this aspect is well known from direct chemoradiation [ 24 ]  . remarkably , 3 patients ( 7% ) died in the interval between induction chemotherapy and the start of rt with one death directly attributable to sepsis in neutropenia ; 1 patient died during rt . 
die tumormarker in enger zusammenarbeit mit dem friedrich - miescher - laboratorium des max - planck - instituts . um 1985 waren mehrere attraktive chefarztposten neu zu besetzen , oder es wurden neue abteilungen fr strahlentherapie an groen kliniken geschaffen durch abtrennung von der diagnostischen radiologie . 
2009 trat er als chefarzt wegen erreichens der altersgrenze in den ruhestand . in der deutschen strahlentherapie bekannt wurde er auch durch seine ehrenamtlichen ttigkeiten : nachdem er jahrelang schatzmeister in dem von ihm mit gegrndeten berufsverband deutscher strahlentherapeuten war , bernahm er 1996 bis 2003 relativ bergangslos den vorsitz des verbandes nach akuter erkrankung seines vorgngers makoski . 
als sein nachfolger im berufsverband sehe ich seine leistung mit groem respekt . nach seiner zeit als vorsitzender des berufsverbandes blieb er weiterhin bis heute in der fortbildungsakademie der degro und im degro - ausschuss elektronische krankenakte . 
nach seiner zeit als medizinalassistent begann er als zeitsoldat die weiterbildung zum radiologen am bundeswehrzentralkrankenhaus in koblenz , gemeinsam oder etwas zeitversetzt mit einer anzahl kollegen , die spter in der diagnostischen radiologie und in der strahlentherapie an vorderer stelle stehen sollten . in den folgenden 10 jahren bis 1984 arbeitete er als wissenschaftlicher assislaudatio neben seiner rztlichen und ehrenamtlich ttigkeit ist lutz ahlemann vor allem ein familienmensch : seine zwei kinder sind in medizinverwandten berufen erfolgreich ttig . 
der korrespondierende autor gibt an , dass kein interessenkonflikt besteht . 712 | strahlentherapieundonkologie82013 case study strahlenther onkol 2013 189 : 693696 doi 10.1007 / s00066 - 013 - 0370 - x received : 3 march 2013 accepted : 29 april 2013 published online : 12 . 
a small series of 8 pediatric patients with central nervous system ( cns ) embryonal tumors who received csi ( 5 fractions of 3.4 gy , 3 fractions of 36 gy ) and local boost to cumulative 54 gy in conjunction with temozolomide ( 90 mg / m2 / day ) was presented at the 15th international symposium on pediatric neuro - oncology ( ispno ) in june 2012 . 
no case of severe myelotoxicity had been observed and only one patient had required packed red blood cell ( prbc ) transfusion [ 8 ]  . case report an 8 - year - old girl was diagnosed with a diffuse intrinsic pontine glioma with multiple spinal metastases . 
mri magnetic resonance imaging , tmz temozolomide , n nimotuzumab , sd stable disease , vz varicella zoster , pd progressive disease discussion the treatment of pediatric brain tumors requires a high level of expertise and an interdisciplinary treatment approach [ 11 ]  . 
in a pooled cohort of 97 children with large pontine gliomas who were registered in the hitgbm databases from 19832001 the patients who had undergone radiotherapy depicted a median overall survival of 0.87 years , whereas half of the patients who had not received irradiation died after only 0.23 years [ 13 ]  . 
median survival increased significantly in patients who were treated according to this protocol when compared to a historical cohort of patients who underwent at least local radiotherapy though at the cost of prolonged hospitalization and an increased rate of infections . 
in summary the use of chemotherapy results in a marginal therapeutic benefit at besta fact which deserves honest discussion with the children and their parents . to the best of our knowledge , this is the first report about a patient with primary metastatic dipg who received , based on the hit - hgg 2007 study protocol , an intensified first - line treatment by adding concurrent temozolomide and nimotuzumab treatment during craniospinal radiotherapy . 
however , given the unfavorable situation of this patient , this treatment approach appeared to be justified as a compassionate use treatment . 694 | strahlentherapieundonkologie82013 rationale for added therapies temozolomide - based chemotherapyregimenin combinationwithradiotherapy inthehit - hgg2007trial when the hit - hgg 2007 study was launched in 2007 , the triumph of temozolomide in the treatment of adult high - grade gliomas [ 12 ] had sparked hopes that the drug could also provide a therapeutic benefit for pediatric patients . 
thus , the hit - hgg 2007 study was initially designed as a clinical phase ii trial to define the role of temozolomide in the first - line treatment of pediatric patients with high - grade or diffuse intrinsic pontine gliomas . additionofnimotuzumab immunotherapyto radiochemotherapy in 2003 , the gilbertsons group assessed 28 samples of diffusely infiltrating brain stem gliomas with different histopathological diagnoses ( world health organization ( who ) grade ii , n = 12 ; who grade iii , n = 9 ; who grade vi , n = 7 ) and demonstrated a significant increase in epidermal growth factor receptor ( erbb1 / egfr ) expression in highgrade tumors ( p < 0.001 , grade ii versus grade iii / iv ) [ 6 ]  . 
nimotuzumab is a recombinant monoclonal antibody directed against human egfr and is used alone or in combination with radioand / or chemotherapy for the treatment of malignant diseases [ 7 ]  . 
here , we describe the case of an 8 - year - old girl with primary metastatic dipg who received craniospinal radiotherapy , a local boost , and concurrent temozolomide and nimotuzumab treatment based on an individual therapy recommendation . 
however , concurrent temozolomide had to be disrupted several times due to considerable acute myelotoxicity ( grade iiiiv )  . maintenance immunochemotherapy could be started with a delay of 5 days and was performed according to treatment schedule . 
despite progress with standard treatment comprising maximum surgical resection , conventional external beam radiotherapy , and various kinds of chemotherapy , long - term survival without recurrence is still rare in patients with malignant brain tumors . 
furthermore , there is no standard treatment for relapsed tumors after initial treatment , and treatment options after conventional radiotherapy are usually very limited because of the tolerance dose of normal brain . several recent reports have indicated that stereotactic radiotherapy ( srt ) for recurrent brain tumor may improve survival without causing severe toxicity [ 2 , 3 , 4 , 5 , 6 , 7 ]  . 
found that stereotactic reirradiation of 35 gy in 3.5 - gy fractions was effective for recurrent high - grade glioma [ 2 , 4 , 5 , 7 ]  . 
found an increased risk of radiation - induced normal brain necrosis with an increasing total dose and treatment volume [ 8 ] , which indicates the importance of avoiding irradiation of normal brain tissue by use of the latest technology . 
it has been reported that pbt is superior to x - ray radiotherapy in preserving the normal tissue volume [ 9 , 10 , 11 , 12 , 13 ]  . in this study , we examined the efficacy of reirradiation including conventional radiotherapy ( rt ) , srt , and pbt for recurrent malignant brain tumors in a retrospective analysis of patients who underwent reirradiation at our hospital . patients and methods patients a total of 26 patients with recurrent malignant brain tumor after radiotherapy received reirradiation at our hospital between january 2005 and september 2010 . 
written informed consent was obtained from all patients prior to reirradiation and the use of a particular treatment modality ( rt , srt , pbt ) was determined according to each patients condition . the 26 patients ( 12 men and 14 women ) had a median age of 48 years ( range , 476 years old )  . 
eleven patients underwent tumor removal before reirradiation , including 8 with pathologically confirmed glioblastoma multiforme ( gbm ) , 2 with grade 3 glioma , and 1 with anaplastic ependymoma . 
the other 15 patients were considered to have inoperable tumors before reirradiation , including 7 with pathologically confirmed gbm at the initial surgery , 1 with pineoblastoma ( who grade 4 ) , 4 with who grade 3 glioma , 1 with anaplastic meningioma , and 2 with atypical teratoid / rhabdoid tumors ( at / rt )  . 
the recurrent tumor was within the initial irradiation area in 21 patients and in the marginal region in 5 patients . treatment methods the gross tumor volume ( gtv ) was defined as the area of contrast enhancement on mri or the tumor bed . 
 the prescribed irradiated dose was chosen based on the organs at risk , such as the optic nerve , optic chiasma , and brain stetreatment planning for pbt was based on computed tomography ( ct ) images taken at 3 - mm intervals in the treatment location . 
different radiation schedules were compared using the biologically effective dose ( bed ) [ 16 , 17 ] , which was calculated with a linear quadratic model according to the following equation : bed = nd ( 1 + d / [ / ] ) , where n is the number of fractions , d is the fraction dose ( gy ) , and / is the tissue repair capacity ( gy )  . 
 the actual radiation dose was converted to the equivalent dose in 2 - gy fractions ( eqd2 )  . follow - up procedures and evaluation criteria acute treatment - related toxicities were assessed weekly during treatment in all patients . 
acute and late treatment - related toxicities were assessed using the national cancer institute common criteria , v.3.0 , and the rtog / eortc late radiation morbidity scoring scheme [ 19 ]  . reirradiation was completed in all patients at doses of 3060 gy ( median , 42.3 gy , eqd2 )  . 
treatment periods were 1443 days ( median , 29 days ) , 247 days ( median , 19 days ) , and 14 51 days ( median , 35 days ) for rt , srt , and pbt , respectively . 
the cause of death in all patients was tumor recurrence , including 11 with local recurrence and 4 with recurrence outside the reirradiated area as the initial recurrence after reirradiation . 
the subjects comprised 26 patients with recurrent malignant brain tumors treated with conventional radiotherapy ( rt , n = 8 ) , stereotactic radiotherapy ( srt , n = 10 ) , and proton beam therapy ( pbt , n = 8 ) at our institute . 
further investigation is needed for treatment optimization for a given patient and tumor condition . keywords glioblastoma proton beam therapy radiotherapy reirradiation recurrent erneute bestrahlung mit blicher strahlenoder protonentherapie bei rezidivierendem bsartigem hirntumor . 
bei den probanden handelte es sich um 26 patienten , die mit konventioneller strahlentherapie ( rt , n = 8 ) , stereotaktischer strahlentherapie ( srt , n = 10 ) und protonentherapie ( pbt , n = 8 ) in unserer einrichtung behandelt wurden . 
die rebestrahlungsdosen betrugen 3060 gy ( median 42 , 3 gy ) und die gesamtdosen der ersten und zweiten behandlung 64 , 5150 , 4 gy ( median 100 , 0 gy )  . 
 in this case , we selected conventional rt because the tumor was larger than 3 cm and there was a small volume of normal brain tissue around the recurrent tumor . 
c isodose curves for the second treatment with pbt representing 100 - 10 % of the prescribed dose at 10 % intervals strahlentherapieundonkologie82013 | original article a typical clinical course of a patient treated with pbt is shown in  . 
at 24 months after reirradiation , the tumor was well controlled and no late toxicity had occurred . discussion several recent reports have indicated that reirradiation for recurrent glioma is a feasible and effective treatment option [ 2 , 3 , 4 , 5 , 6 , 7 ]  . 
in general , the dose of initial radiotherapy is about 60 gy in 30 fractions for high - grade glioma and about 3040 gy in several fractions was frequently used as the reirradiation dose . 
our results support the feasibility of reirradiation for recurrent malignant brain tumor using modern treatment modalities and depending on the dose concentration . although srt or srs is often used for treatment of recurrent brain tumors , these methods are usually not applicable to large or irregularly shaped tumors , since an increase in the treatment volume exposes large areas of normal brain tissue to the detrimental effects of a highdose irradiation . 
in our hospital , pbt is available for various kinds of tumors , including large or irregularly shaped tumors [ 9 , 10 , 11 , 12 , 13 , 18 , 20 , 21 ] ; however , definitive selection criteria for the reirradiation method to brain tumors have not been established yet . 
therefore , we select srt , which is low in cost compared to pbt , for small tumors and convention662 | strahlentherapieundonkologie82013 al rt or pbt for larger tumors that are difficult to treat with srt . 
several reports have shown overall survival of approximately 10 months after reirradiation for gbm [ 2 , 3 , 4 , 5 , 6 , 7 ] , and combs et al . 
in this study , the median survival after reirradiation for gbm was 13.1 months , indicating that the outcome using rt , srt , or pbt was similar to that in patients treated with srt or srs . acute adverse events were generally mild in our patients . 
although comparison with other reports is difficult because of the small number of events , all patients completed the planned reirradiation without change in the karnofsky performance score suggesting that reirradiation is feasible at least in the short ter as for late adverse event , 2 patients demonstrated radiation necrosis . 
 although they were controllable in our series , these cases indicate that reirradiation to the recurrence at or close to critical regions such as the brain stem or the optic chiasma is very difficult to achieve while preserving functions . 
however , pbt is generally expensive , and compared with other radiation modalities such as srt or srs , significant clinical benefits of pbt in recurrent brain tumors have not been proved yet . 
this research is partly supported by the funding program for world - leading innovative r&d on science and technology ( first program ) , initiated by the council for science and technology policy ( cstp )  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . letter to the editor strahlenther onkol 2013 189 : 697699 doi 10.1007 / s00066 - 013 - 0353 - y received : 11 march 2012 accepted : 18 march 2013 published online : 24 may 2013 springer - verlag berlin heidelberg 2013 t.junginger1ca.maurer2r.ruppert3h.ptok4j.strassburg5 1 department of general and abdominal surgery , university medical center mainz 2 department of surgery , hospital of liestal , affiliated with the university of basel 3 department of general , visceral and endocrine surgery and coloproctology , municipial hospital of munich - neuperlach 4 department of surgery , carl - thiem - hospital , cottbus 5 department of general and visceral surgery , vivantes - klinikum im friedrichshain , berlin commentontheeditorialof sautter - bihletal.instrahlentherapie und onkologie2013189 : 105110 original publication sautter - bihl ml , hohenberger w , fietkau r et al ( 2013 ) rectal cancer : when is the local recurrence risk low enough to refrain from the aim to prevent it ? strahlenther onkol 189 : 105110 letter to the editor we would like to thank the authors for their interest in the ocum study and would like to clarify a few points : the study ( clinicaltrials.gov nct 01 , 325 , 649 ) is a prospective evaluation of a selective magnetic resonance imaging ( mri ) - based neoadjuvant radiochemotherapy ( nrct ) in patients with rectal carcinoma treated with total mesorectal excision ( tme )  . 
an interim analysis [ 22 ] should evaluate whether participating hospitals meet the essential prerequisites for the study concept . the study is based on the following facts : f preoperative radiotherapy ( nrt ) and radiochemotherapy are each associated with greater risks of shortand long - term adverse effects than tme alone [ 12 ]  . 
given the local recurrence rate to be reduced from 10 to 5% by nrt or nrct , 5% of the population will benefit from the treatment , while 95% are subject to risk ( and cost ) without realizing any benefit . 
 therefore , nrt and nrct should be restricted to patients with a high risk of local recurrence . f postoperative rct is based on the histological determination of the pt and pn category of the resected tumor . 
the application of these criteria as a basis for nrct leads to substantial over - treatment ( 18% ; [ 17 ] ) because no imaging technique can determine the ct category , and particularly the cn category , with enough accuracy . f the distance of the tumor from the circumferential resection margin ( crm ) is an important independent prognostic factor for local recurrence and survival . 
the risk of local recurrence is much higher if the distance is 1 mm or less than if the distance is greater than 1 mpreoperative mri allows the imaging of the tumor , the mesorectal fascia ( mrf ) , which is the potential resection plane ( crm ) , as well as the determination of whether the mrf is free or involved . 
in particular , the negative predictive value ( npv ) of the mrf status exceeds 90% in patients who undergo primary surgery ( 94.0% , [ 7 ] ; 98.5% , [ 14 ] )  . 
high - quality tme surgery is a prerequisite for the high accuracy of preoperative mri , so that the mrf and crm are nearly identical . f preoperative mri allows the identification of patients with a low risk of local recurrence ( in which nrct constitutes over - treatment ) , as well as patients at high risk ( mrf involved , high risk ; [ 10 ] )  . 
in these patients , long - term nrct induces shrinkage of the tumor and negativity of the crm in a high percentage of patients . the ocum study schedules a selective mri - based indication for nrct depending on tumor location , ct category , and mrf status ( i.e. , not on mrf status alone ) : nrct is provided for all ct4 tumors , for tumors of the middle third with involved or threatened mrf , and for all ct3 tumors of the lower third with and without mrf involvement , because at this location the mrf may be poorly to identify [ 13 ] and because tumor spread to lateral lymph nodes ( i.e. , lymph nodes at the intern iliac arteries outside the mesorectum ) exceptionally and exclusively occur in low t3 - tumors [ 23 ]  . the authors of the editorial [ 19 ] stated that the strongest evidence for the impact of radiotherapy on prognosis in lymph node positive patients can be derived from the dutch tme trial and further : even in the era of quality - asstrahlentherapieundonkologie82013 | letter to the editor sured tme , the negative impact of positive lymph nodes on local control and survival can , at least partly , be compensated by preoperative radiotherapy . 
 third , this study is quite far away from providing quality - assured tme : only 180 out of 1530 randomized patients had a detailed description of the rectal specimen . 
and from those , the mesorectum was incompletely removed in 23.9% , only 34% of patients with apr had tme and only 39% of tumors < 5 cm from anal verge had complete mesorectal excision [ 9 ]  . the primary endpoint of the ocum study is the 5 - year local recurrence rate for all patients , for patients after primary surgery , and for patients after nrct . 
for patients with stage piii disease , the values observed in the study cao / aro / aio94 might be valid : 9.5% after nrct and 10.9% after postoperative rct [ 18 ]  . the interim analysis revealed three essential points : a high quality of mri diagnosis ( npv for crm status 134 / 136 , 98.5% ) , a high quality of tme surgery ( mesorectal plane 209 / 230 , 90.9% ; intramesorectal plane 16 / 230 , 7% ; muscularis propria plane 5 / 230 , 2.2% ) , and a low rate of pcrm involvement ( 13 / 230 , 5.7% ) in all participating hospitals . 
the introduction of tme is the best example in this context : there is no randomized controlled trial comparing tme with conventional rectal cancer surgery , and there will never be such a trial . 
if there are sound clues and results that favour the new treatment , a nonrandomized prospective observational ( pilot ) study may be justified to avoid overtreatment and adverse effects for many patients . 
when the standards are high , as shown by recent publications of the participants in the ocum study [ 16 ] , a nonrandomized prospective study can add reliable knowledge about the treatment of rectal carcinoma . interpreting the results of the mrc cr07 and ncic - ctg co16 studies [ 15 ] , sautter - bihl et al . 
comparing preoperative short - course radiotherapy and selective postoperative radiochemotherapy , the absolute value of reduction of local recurrence was 6% for each of the three categories of tme surgical quality . 
on behalf of all authors , the corresponding author states the following : no financial interest , no financial or material support . laudatio strahlenther onkol 2013 189 : 715716 doi 10.1007 / s00066 - 013 - 0401 - 7 online publiziert : 25 . 
die erste deutsche multizentrische therapiestudie in der onkologie ( die damals noch vom bmft gefrderte studie brusterhaltende therapie des kleinen mammakarzinoms ) und hat mit der deutschen rektumkarzinom - studie einen internationalen therapiestandard gesetzt . die dkg ehrt ihn insbesondere auch wegen seiner vielfltigen und nachhaltigen leistungen , die er ber mehr als ein vierteljahrhundert fr die dkg erbracht hat : von 1986 bis 1993 leitete er die arbeitsgemeinschaft radiologische onkologie der dkg , von 1993 bis 1998 den anwendungsprotokoll - prfungsausschuss der dkg , und von 1998 bis 2003 war er mitglied der leitkommission fr klinische krebsforschung der deutschen krebsgesellschaft sowie der deutschen krebshilfe . 
im jahr 2007 grndete er die forschungsgruppe fr klinische hyperthermie der dkg und der deutschen gesellschaft fr radioonkologie ( degro )  . wolff schmiegel , prsident der dkg , stellte in seiner laudatio fest : professor rolf sauer gehrt zu den beeindruckenden persnlichkeiten in der dkg und hat unsere fachgesellschaft mit seinem engagement fr die interdisziplinre zusammenarbeit verschiedener rolf sauer . 
die dkg , die grte deutsche onkologische fachgesellschaft , erinnert mit dieser medaille an den heidelberger chirurgen bauer , den grnder des deutschen krebsforschungszentrums ( dkfz ) und ehrt mit dieser auszeichnung seit 1994 jhrlich ausgewiesene persnlichkeiten der deutschen onkologie . rolf sauer , von 1977 bis 2008 professor fr strahlentherapie und direktor der strahlenklinik an der friedrichstrahlentherapieundonkologie82013 | dargestellt werden . 
die strahlentherapieplanungen fr 32 krankheitsbilder , die nahezu das gesamte spektrum der strahlentherapie umfassen , wird nach weitgehend einheitlichem muster beschrieben : von welchen diagnostischen grundlagen kann man ausgehen ? wie lagert man den patienten bei der diagnostik und auf dem bestrahlungstisch ? wie grenzt der arzt ein zielvolumen ( gtv , ctv , ptv ) mit unterschiedlichem risiko genau ab , damit der physiker bei der planung eine entsprechende dosis zuordnen kann ? die konturierungen und planungen mit isodosen werden mit einer sehr groen zahl von graphisch gut widergegebenen ct - bildern genau beschrieben . 
hier liegt ein fabelhafter leitfaden fr eine konformale und intensitts - modulierte strahlentherapie vor , der den heutigen standard definiert und fr die tgliche praxis nachdrcklich zu empfehlen ist . stephan roth ( dsseldorf ) pleuropulmonale tumoren stellen fr den pathologen ein wichtiges themengebiet dar insbesondere auch unter bercksichtigung aktueller entwicklungen in der molekularpathologischen diagnostik der lungenkarzinome und hiermit verbundener therapieanstze . 
 das vorliegende buch zur diagnostic pathology of pleuropulmonary neoplasia von weissferdt und moran beinhaltet eine umfangreiche darstellung dieser tumoren unter besonderer bercksichtigung der mikroskopischen morphologie . die verschiedenen themenaspekte werden in 14 einzelkapiteln sorgfltig gegliedert vorgestellt . 
 bei der vorstellung der unterschiedlichen tumorentitten wird ein bersichtliches konzept der darstellung gewhlt mit unterteilung in historie , histopathogenese , definition der lsion , klinik , makroskopie , mikroskopie , immunhistochemie und molekularpathologie , differentialdiagnose sowie abschlieend behandlung und prognose . 
 ein besonderer aspekt des 470 seiten umfassenden buches ist die reichhaltige bebilderung mit verwendung von insgesamt 1018 farbigen einzelabbildungen , wobei ganz berwiegend histologisches bildmaterial vorliegt was fr den diagnostischen pathologen entscheidend ist . 
gerade auch seltenere subtypen knnen hierdurch ausfhrlicher 716 | strahlentherapieundonkologie82013 laudatio strahlenther onkol 2013 189 : 713714 doi 10.1007 / s00066 - 013 - 0381 - 7 online publiziert : 25 . 
seine ersten wissenschaftlichen arbeiten wurden durch das hervorragende umfeld der modernen klinik fr strahlentherapie im neuen klinikum der universitt mnster ( leitung schnepper ) und den intensiven klinischen und wissenschaftlichen aktivitten der internistischen und pdiatrischen onkologie ( leitung schellong ) geprgt . 
er war aktiv am aufbau der degro beteiligt und initiierte zusammen mit wolfgang hinkelbein und rolf - peter mller die arbeitsgemeinschaft fr pdiatrische radioonkologie ( apro )  . richard ptter leitet seit bernahme der ordentlichen professur fr strahlentherapie 1993 die universittsklinik fr strahlentherapie am neuen allgemeinen krankenhaus der stadt wien und an der medizinischen universitt wien . 
seine visionen bezglich der bildgefhrten radiotherapie hat richard ptter bereits in der habilitationsschrift 1989 ausgefhrt , die sich mit der reproduzierbarkeit von bestrahlungsfeldern und bewegung von organen unter laufender therapie ( portal imaging ) und der 3d / 4d - adaptation der zielvolumina beschftigte . 
aufbauend auf der installation eines mr in der wiener klinik fr strahlentherapie mitte der 1990er jahre konnte er richtungsweisende entwicklungen vor allem in der gynkologischen brachytherapie initiieren , zusammen mit der wiener gynkologischen arbeitsgruppe und experten des europischen gynkologischen netzwerks , die heute international fhrend sind . 
1975 beendete er das studium der medizin und absolvierte nach einer zweijhrigen dissertation die ausbildung zum allgemeinmediziner und internisten in greven . seine radiologische weiterbildung begann er 1982 an der universittsklinik in mnster unter der leitung von herrn schnepper . 
whrend dieser zeit wurde sein besonderes interesse fr die laudatio keit in sterreich ist die etablierung des medaustron - projektes ( krebsforschungsund behandlungszentrum fr ionen therapie in wiener neustadt , beginn 2015 ) seine stete herausforderung . 
richard ptter ist ber die grenzen von sterreich hinaus um die etablierung und weiterentwicklung der partikeltherapie sowie die schaffung nachhaltiger europischer forschungsstrukturen bemht , auch im rahmen von eu - projekten . fragen zu stellen , erkenntnisse zu erwerben vor allem durch klinische und translationale technologische forschung sowie wissen und erfahrungen an junge kollegen aller berufsgruppen in der radioonkologie und darber hinaus weiter zu vermitteln waren ihm stets besondere anliegen . 
dies zeigt sich insbesondere in der intensiven forschungsund lehrttigkeit der wiener klinik , die durch zahlreiche forschungsgruppen , projekte und persnlichkeiten in der klinischen radioonkologie und der medizinischen strahlenphysik sowie rezent auch in der klinischen strahlenbiologie eine hohe nationale und internationale reputation erwerben konnte . 
als mitglied des exekutiv komitees und als koordinator des kollegiums und aller 22 tumorboards am akh wien nimmt er hier eine bedeutende rolle ein . seit 1993 unermdlich aktiv in estro - teaching - kursen , leitet richard ptter seit 2006 die estro school for radiotherapy and oncology und trgt wesentlich zum erfolg dieser einzigartigen postgraduellen radioonkologischen ausund weiterbildung auf europischer und internationaler ebene bei . 
gemein714 | strahlentherapieundonkologie82013 sam mit internationalen europischen radioonkologen , strahlenbiologen und medizinphysikern hat er sich seit langem als clinical editor fr das green journal engagiert und dieses als eines der fhrenden fachjournale in der internationalen radioonkologie und onkologie mit geprgt . richard ptter wurde durch zahlreiche auszeichnungen nationaler und internationaler fachgesellschaften geehrt . 
 ihm wurde vom estro - physik - komitee der titel honorary physicist 2007 verliehen , eine wrdigung , die alle 2 jahre an nichtphysiker fr ihre verdienste um die frderung der medizinphysik vergeben wird . 
fr seine herausragenden leistungen in der radioonkologie in wissenschaft und lehre wurde er von der estro 2010 mit dem emmanuel van der schueren award ausgezeichnet und wird 2014 bei der estro 33 in wien die klaas breur lecture halten . wir wnschen richard ptter zu seinem 65 . 
geburtstag alles gute , vor allem , dass er sich in den kommenden berufsjahren seine neugier , seinen kritischen geist und seine visionen fr neuentwicklungen in der radioonkologie und onkologie bewahrt . dietmar georg und karin dieckmann , wien korrespondenzadresse d . 
der korrespondierende autor gibt fr sich und seinen koautor an , dass kein interessenkonflikt besteht . literaturkommentiert strahlenther onkol 2013 189 : 702703 doi 10.1007 / s00066 - 013 - 0384 - 4 online publiziert : 16 . 
juni 2013 springer - verlag berlin heidelberg 2013 g.klautke strahlenklinik , sozialstiftung bamberg keineverbesserungder behandlungsergebnissevon operationundpostoperativer strahlentherapiedurcheine neoadjuvantechemotherapiemit tpfbeilokalfortgeschrittenen , primrresektablen plattenepithelkarzinomen dermundhhle originalpublikation zhong lp , zhang cp , ren gx et al ( 2012 ) randomized phase iii trial of induction chemotherapy with docetaxel , cisplatin , and fluorouracil followed by surgery versus up - front surgery in locally advanced resectable oral squamous cell carcinoma . 
zur induktionschemotherapie vor simultaner radiochemotherapie mit und ohne docetaxel ( tax 323 und tax 324 ) zeigten , dass durch die integration von docetaxel in die einer strahlentherapie ( rt ) vorgeschalteten chemotherapie das gesamtberleben der patienten verbessert werden kann . 
die eine gruppe erhielt eine neocht mit tpf ( 75 mg / m2 docetaxel d1 , 22 ; cisplatin 75 mg / m2 d1 , 22 ; 5 - fu 750 mg / m2 d15 , 2226 ) sowie eine anschlieende operation und adjuvante bestrahlung ( 1 , 8 gy / 2 gy bis 5460 gy )  . 
durch die neocht kam es in 80 , 6% der flle zu einer objektivierbaren remission , und in 13 , 4% der flle konnte eine pathologisch komplette remission erzielt werden . 
eine neoadjuvante chemotherapie mit tpf bringt keinen vorteil fr die patienten in den berlebensdaten . kommentar diese studie zeigt erneut , dass das thema der induktionschemotherapie von den internistischen onkologen mit dem ziel der verbesserung des gesamtberlebens bei patienten mit kopf - hals - tumoren immer noch verfolgt wird , obwohl diese , wie auch hier besttigt , dem patienten prinzipiell nur toxizitt bringt . 
zhong lp , zhang cp , ren gx et al ( 2012 ) randomized phase iii trial of induction chemotherapy with docetaxel , cisplatin , and fluorouracil followed by surgery versus up - front surgery in locally advanced resectable oral squamous cell carcinoma . 
kirita t , yamanaka y , imai n et al ( 2012 ) preoperative concurrent chemoradiotherapy for stages iiiv oral squamous cell carcinoma : a retrospec tive analysis and the future possibility of this treatment strategy . 
kuhnt t , becker a , bloching m et al ( 2006 ) phase ii trial of a simultaneous radiochemotherapy with cisplatinum and paclitaxel in combination with hyperfractionated - accelerated radiotherapy in locally advanced head and neck tumors . 
dadurch knnen die lokale kontrolle gegenber einer alleinigen rt um 1015% und das gesamtberleben um 10% verbessert werden ( eortc 22931 , rtog 9501 , aro 96 - 3 )  . 
wre das hier in dieser studie bercksichtigt worden , wre das studienergebnis fr die neoadjuvante tpf - gabe noch vernichtender ausgefallen . durch eine neocht nicht verbessert werden ; in beiden armen waren die r0 - resektionsraten identisch . 
beispielsweise konnten wir in der rostock - hallenser arbeitsgruppe mit einer taxanhaltigen definitiven rct klinisch komplette remissionsraten von 69% erreichen [ 3 ] bei wesentlich fortgeschrittenen , primr inoperablen tumoren . 
durch eine besser vertrgliche neoadjuvante rct mit konventionell fraktionierten 40 gy und nur einem kurs cisplatinbasierter cht konnte schon eine pcr von 21 , 9% erreicht werden [ 1 ]  . 
der einsatz sollte aber nicht in form einer sequenziellen rct erfolgen , wie in der tax 323 , oder als induktionschemotherapie vor definitiver rct , wie in der tax 324 ( fr beide strategien gibt es keine positiven ergebnisse aus phaseiii - studien im vergleich zum standard der definitiven rct ! ) , sondern als simultane rct wie in der rostock - hallenser arbeitsgruppe oder aktuell in der wieder von der deutschen krebshilfe gefrderten paccisstudie . 
goethe university , frankfurt / main 2 clinic for gynecology and obstetrics , university gieen 3 department of radiooncolgy , klinikum lippe 4 department of radiooncology , franziskus hospital , bielefeld 5 clinic herzoghoehe , bayreuth 6 hopa , hamburg 7 department of head and neck diseases , clinic nordhausen 8 institute for transdisciplinary health care research , berlin 9 radiooncology , wiesbaden counselingcancerpatients oncomplementaryand alternativemedicine background , theory , andimplementation ofnationwidecounselingfacilities complementary and alternative medicine ( cam ) is of high importance to cancer patients . 
we use camin accordance with edzard ernsts definitionas an umbrella term for a huge variety of methods in diagnosis , treatment and / or prevention which complement [ s ] mainstream medicine by contributing to a common whole , by satisfying a demand not met by orthodoxy or by diversifying the conceptual frameworks of medicine [ 7 ]  . patients who use cam are more afraid of the side effects of conventional therapy than those who use the latter . 
persons adhering to cam more often believe that psychosocial factors , stress , environment and a deficit in the immune system are causes of their disease [ 13 ]  . 
patients prefer their clinicians and physicians to initiate the talk about cam and wish a nonjudgmental discussion style , which provides an open space to consider cam use with respect to their quality of life [ 20 ]  . 
patients fear that their oncologist might discourage cam use , is not informed about cam or simply think their clinicians do not need to know [ 17 , 18 ]  . on the other hand , only a minority of professionals in oncology feel competent to communicate about cam with their patients [ 9 , 17 ]  . 
 in fact , general physicians only provide information in 15% of all cases and oncologists only in 7% [ 6 ]  . in a survey from canada , patients of a cancer center preferred receiving information on cam from their oncologist but strahlentherapieundonkologie82013 | original article tab . 
nearly half of the patients continued a cam treatment after reading a scientific report showing that this treatment was futile [ 23 ]  . the internet is frequently consulted by patients and professionals , alike , about cam , but several problems are associated with its use as source of information . 
 quality and reliability of information is often questionable , and users need to deal with contradictory recommendations , which may even increase uncertainty [ 3 ]  . 614 | strahlentherapieundonkologie82013 in order to improve patientphysician communication about cam and meet patients needs to discuss safety and efficacy of cam [ 20 ] , professionals need access to reliable and evidence - based information . 
however cam offers the opportunity for patients to become actively involved in their treatment , care for themselves and possibly even reduce adverse effects of conventional cancer therapy [ 1 ]  . 
additionally , preclinical studies point at the synergistic potential of , for example , plant derivatives and other supplements [ 5 , 11 , 21 ]  . several publications acknowledged the wide gap between information and counseling needs of cancer patients regarding cam and the availability of professional services in this field [ 20 ]  . our aim was to develop a framework of a professional network in germany that takes into account all above - mentioned issues in order to improve access to cam counseling for patients and to enhance quality of cancer care . 
however providing information is one of the most important issues to gain patient satisfaction [ 10 ]  . methods we conducted a two - step medline search for publications on cam counseling . 
in the next step we specified our search by concentrating on publications concerning cancer ( and neoplasms [ mesh ] )  . publications were screened by title and abstract whether they refer to the setting of counseling on cam . 
after deriving the essentials from the publications , an expert group from the degro ( deutschen gesellschaft fr radioonkologie ) and the german cancer society consented on recommendations for cam counseling suitable for the needs of cancer patients in germany . 
members of the expert group had to be physicians with long - standing expertise in oncology and complementary medicine , a list of scientific publications in the topic of cam and / or participation in the national guideline program for cancer ( the latter two being proof of experience with evidence - based medicine )  . 
these recommendations were published in the journal for members of the german cancer society in order to encourage discussions [ 12 ]  . after considering all proposals , the expert group consented to a strategy how to establish a model by which evidencebased cam counseling can be offered to all cancer patients within the german health system . results the initial medline search provided 811 publications . 
content of these publications provided information on the current state of knowledge and scientific research on the process of cam counseling and information provision . it was decided to use the publication by schofield et al . 
as most of the underlying scientific work was done in anglo - american context , our group of experts of the working groups akte ( arbeitskreis trace elements ) from the german society of radiooncology and prio ( prevention and integrative oncology ) from the german cancer society adapted these evidencebased recommendations for germany . 
 these recommendations were first published in forum , the journal of the german cancer society , in spring 2012 to facilitate discussion and reach consensus in the scientific community [ 12 ]  . 
2. no objections to our proposal were received , so we set out to define the crucial aspects to consider in a model of consultation facilities . any proposal to provide cam counseling should allow for a nationwide approach . 
data from these articles were analyzed and adapted to the needs of german patients by a group of experts of the degro ( deutschen gesellschaft fr radioonkologie ) and the german cancer society . 
furthermore , provision of information on two different levels allows the effective use of resources ( manpower and financing )  . keywords complementary therapies literature review guideline recommendations germany beratung von krebspatienten zu komplementrer und alternativer medizhintergrund , theorie und umsetzung bundesweiter beratungshilfen zusammenfassung hintergrund . 
qualification of counselors : providing counseling on cam not only requires knowledge about cam but also oncological expertise and competence in communication which must be acquired and maintained by continuous education 3 . 
process of counseling : patients should be asked about their understanding of illness and therapy and encouraged to describe their disease , history as well as their current situation in their own words ( active listening , getting to know emotional relationships )  . 
the counseling needs to consider a broad range of cam methods along with other supportive therapies , measurements to further a healthy lifestyle , physiotherapy , nutrition and physical activity 10 . 
if possible , a follow - up contact should be offered ing cam [ 6 , 8 , 14 , 15 ] , we need a dense network of consultation facilities . 
prerequisites are the local and prompt availability of counseling by qualified and trained professionals . the quality of cam counseling depends on its integration into conventional cancer care in cancer centers and networks . 
the foundation of every consul616 | strahlentherapieundonkologie82013 tation must be scientific data on treatment and evidence obtained from the as complementary therapy accompanies conventional treatment , counseling always has to regard all aspects of conventional therapy . 
a specific challenge is the requirement to integrate provision of highly specialized information about cam with patients needs to discuss and decide upon their conventional treatment at the same time . the core of our proposal is to combine two levels of counseling . 
cam counseling should be available in daily routine provided by oncologists and other specialists ( level 1 ) and in case of particular needs on a cam expert level ( level 2 )  . special training on cam and cam counseling could be offered to oncologists , radiotherapists and other professionals in order to guarantee high quality of counseling . since the most important topics of cam in oncology have remained the same for decades , a basic curriculum needs to be developed . 
this core set of cam in oncology consists of supplements , mistletoe , herbs and some aspects of holistic systems like homeopathy [ 8 , 14 , 15 ]  . 
modules for general practitioners , nurses , pharmacists and other professionals could be developed . these modules can be taught in seminars of 34 days with regular updates every 2 to 3 years . 
in cooperation with cancer societies , the modules could become part of congresses and other educational programs . a pilot version of these modules is held by the authors as part of the german - speaking european society of oncology prograthis seminar includes basic information on the most important methods of cam : vitamins , mistletoe , trace elements . 
communication skills are part of workshops as well as training on how to obtain reliable information on cam . by offering more training facilities , cancer societies will be able to increase physician and caregiver knowledge regarding cam in a short time , and thus , enable them to pass on basic information to their patients . level 2 this system of integrated cam counseling in cancer institutions needs to be comf counseling individual patients with f timeforcounselinginclinicalroutine bined with specialized centers for cam in oncology . 
these will have several tasks : f backing up physicians who are confronted with a more complicated or advanced question , f training oncologists and other profescomplex needs , sionals , f ensuring high quality of the whole system by providing updates and supervision and f engaging in quality management of the whole prograin addition to measuring satisfaction of all participants and patients , evaluation of the projects impact on cancer care , safety and economy will be mandatory . this approach of two levels also takes into account the limited resources in the healthcare systebasic counseling will not take much time as it can be integrated in the process of shared decision - making of the treatment as a whole . 
presuming a local recurrence rate ( lrr ) of 10% that can be reduced to 5% by neoadjuvant radiochemotherapy ( nrct ) , is speculativeor at least improperly extrapolated to the entire group of patients treated in the ocum study , i.e. , including those with stage iii disease . 
in the norwegian colorectal cancer registry , all stage iii patients ( n = 2 , 232 ) had a 5 - year lrr of 16% for pn1 amounting to 30.4% in pn2 patients [ 1 ]  . 
moreover , in a subgroup analysis of the norwegian pt3 patients with a circumferential resection margin ( crm ) > 3 mm ( n = 1 , 217 ) , the 5 - year lrr for pt3pn1 patients was 16.8% and increased to 29% in stage pt3pn2 [ 5 ]  . 
in the dutch tme trial , the 10 - year lrr without rt was 17% [ 24 ] ; in the mrc - c07 study , the 3 - year lrr was 15.4% after primary surgery [ 18 ]  . likewise , the assumption that 95% of the patients are subjected to risk and cost without realizing any benefit seems undue . 
it is beyond dispute that radiotherapy may cause long - term toxicity ; as an example the authors cite the late toxicity data from short - term rt in the dutch trial . 
the remaining risk has to be balanced against the harm resulting from recurrence . in reply to our interpretation of the effect of rt on survival of stage iii patients in the dutch tme study , junginger et al . 
this is in contradiction with the data shown in table 3 of the publication of van gyjn [ 24 ] : in the subgroup of stage iii patients with negative crm , the 10 - year oas was 50% after rt and tme vs . 
qualify the dutch study as being far away from quality - assured tme , we do not feel entitled to comment on this criticishowever , we could not reproduce such a conclusion from the paper cited for substantiation of their assertion . 
also disagree with our interpretation of the crc - c07 study that best surgery yields highest benefit of radiotherapy which is no more than a conclusion from the statement of quirke [ 13 ] , the first author of the paper : our data suggest that the plane of surgery achieved and short - course preoperative radiotherapy have additive effects , indicating that preoperative radiotherapy is beneficial whatever plane of surgery is achieved . 
 further on in patients who received short course radiotherapy ( srt ) and in whom a mesorectal plane resection was achieved , lr was almost abolished [ 13 ]  . 
for substantiation , they cite eight references : f two reviews [ 6 , 23 ] , f one treatment recommendation of the french ligue nationale de cancer [ 9 ] , f one retrospective study of 190 patients ( mean age 70 years ) , for whom nrct was omitted in contrast to the policy of the treating center , however , without specification of the reasons for omission [ 7 ] , f two small retrospective studies including 35 and 48 patients not staged by mri [ 19 , 20 ] , f a pooled analysis of randomized studies using adjuvant rt , including 3 , 791 patients of whom only 179 were treated by surgery alone [ 8 ] , and f the only cited articles referring specifically to mri - based treatment is the observational study of the mercury group , comprising 65 stage ii / iii patients [ 22 ] that we commented in our editorial [ 17 ]  . we cannot reproduce the authors proposition that these articles provide any of the sound clue and results they claim as a justification for implementing a new treatment . we share jungingers view that there may be many ways to gain reliable knowledge . 
this article prompted fierce objections , such as the comment by reeves [ 14 ] : , making arbitrary decisions about the obviousness of the effectiveness of interventions based on observational evidence cannot be the way forward . 
nonsurgical treatment is currently recommended in unresectable disease with severe or progressive symptoms , or upon radiological progression [ 19 , 20 ]  . in the multicenter treatment study for children and adolescents with a low grade glioma hit - lgg 1996 by the german society of pediatric oncology and hematology ( gpoh ) , children aged 5 years and older underwent external fractionated radiotherapy ( efrt ) as firstline nonsurgical treatment . 
a total of 32 of these patients ( 8 with rt as first - line treatment ) did not fulfill the selection criteria and were excluded from the analysis ( 3 patients with spinal location , 6 with initial metastatic disease , 10 who had undergone two or more regimens of chemotherapy before the start of rt , 10 with incomplete data sets , 2 who had received radiosurgery and 1 patient who had been treated with a combination of sbt and efrt )  . 
 strahlentherapieundonkologie82013 | original article complete resection incomplete resection biopsy clinical diagnosis / imaging symptoms / progress nonsurgical treatment 5 years < 5 years stereotactic brachytherapy radiotherapy chemotherapy progression chemotherapy radiotherapy fig . 
2 8 patient selection : 117 hit - lgg 1996 study patients with pilocytic astrocytoma who underwent radiotherapy were eligible in 61 of the remaining 117 cases ( 52% ) a central histological review had been performed . 
iodine - 125 was used either as a permanent or temporary implant . chemotherapy first - line chemotherapy consisted of a 10 - week induction phase with vincristine and high - dose carboplatduring consolidation ( weeks 1353 ) , both drugs were given concomitantly every 4 weeks . doseresponse relationship assessment to enable assessment of the doseresponse relationship with varying single ( range 1.52.0 gy ) and total doses ( range 39.661.2 gy ) , we used the linear quadratic model to calculate the biolog648 | strahlentherapieundonkologie82013 ically effective dose ( bed ) and the normalized total dose ( ntd ) of each radiation regimen . 
all treatment regimens were compared on the basis of ntd values [ 6 , 7 , 24 ]  . statistics survival times were calculated from the start of rt or time of seed implantation onwards . 
for progression - free survival ( pfs ) , events were defined as radiographic evidence of progression , relapse or clearly tumor - related death , whereas death from any cause was relevant for overall survival ( os )  . 
all analyses were performed using spss , version 20 ( spss inc . , chicago , il , usa )  . results patient characteristics eligibility criteria were fulfilled by 117 patients . 
in 75 cases , external fractionated radiotherapy ( efrt ) was administered either as first - line nonsurgical treatment ( n = 58 ) or after progression following primary chemotherapy ( n = 17 )  . 
disease progression after efrt was not influenced by gender , neurofibromatosis type 1 ( nf1 ) status , tumor location ( hemispheres versus supratentorial midline versus posterior fossa ) , age or prior chemotherapy . 
die meisten tumoren befanden sich in der supratentoriellen mittellinie ( 65% ) , gefolgt von der hinteren schdelgrube ( 26 , 5% ) und den grohirnhemisphren ( 8 , 5% )  . 
 in 75 fllen wurde eine externe fraktionierte bestrahlung ( efrt ) entweder als erste nichtchirurgische therapie ( n = 58 ) oder bei progression nach vorheriger chemotherapie ( n = 17 ) durchgefhrt . 
3 efficacy of salvage treatment after failure of first - line nonsurgical treatment consisting of chemotherapy and / or targeted therapy no.ofpatients progression - free survivalrate mediantimeto progression histology remark author / year yalon et al . 
 2011 [ 35 ] various chemotherapy regimes 378% 5 years after second - line chemotherapy 13 / 19 patients had to stop treatment within 1 year ; 10 due to progression median treatment duration 12 months , 13 / 14 patients ( 93% ) had progression after treatment 6 months after initiation of salvage treatment 5 months after the end of bevacizumab pilocytic astrocytoma 9 / 19 ( 47% ) fibrillary astrocytoma 2 / 19 ( 11% ) no histology 8 / 19 ( 42% ) pilocytic astrocytoma 4 / 14 ( 29% ) fibrillary astrocytoma 3 / 14 ( 21% ) pilomyxoid astrocytoma 1 / 14 ( 7% ) no histology 6 / 14 ( 43% ) pilocytic astrocytoma 23 / 50 ( 46% ) low - grade glioma ( not specified ) 7 / 50 ( 14% ) ganglioglioma 7 / 50 ( 14% ) diffuse astrocytoma 1 ( 2% ) oligodendroglioma 1 ( 2% ) no histology 12 ( 24% ) grade i astrocytoma 27 / 38 ( 71% ) ganglioglioma 2 / 38 ( 5% ) pilomyxoid glioma 3 / 38 ( 8% ) oligoastrocytoma 1 / 38 ( 3% ) no histology 5 / 38 ( 13% ) pilocytic astrocytoma 2 / 10 ( 20% ) fibrillary astrocytoma 3 / 10 ( 30% ) pilomyxoid astrocytoma 1 / 10 ( 10% ) no histology 4 / 10 ( 40% ) pilocytic astrocytoma 17 / 17 ( 100% ) packer et al . 2009 [ 30 ] bevacizumab + irinotecan 8 / 9 patients without evidence of progressive disease 9 patients evaluable ; 1 patient had to stop therapy for toxicity after 2 months . 
maximum followup time 22 months present study external fractionated radiotherapy 1.3 years 7511% 5 and 10 years after start of radiotherapy discussion the treatment of pediatric brain tumors requires a high level of expertise and an interdisciplinary treatment approach [ 27 ]  . 
however , in refractory or recurrent disease after chemotherapy , rt still represents a useful salvage treatment , alongside some proven and effective second - line chemotherapy regimens [ 1 , 11 , 12 , 30 , 35 , 37 , 40 ]  . we present a retrospective data analysis from a large homogenous cohort of pediatric patients with nonmetastatic intracranial pilocytic astrocytomas who received either efrt or sbt within a prospective multicenter study . 
for each of the two rt techniques , we demonstrated excellent pfs and os rates . outcome after efrt to the best of our knowledge , this is the first subgroup analysis evaluating the role of rt that focusses on pediatric pilocytic astrocytoma . 
pfs and os rates after efrt were excellent ( 5and 10 - year pfs : 765% , 5and 10 - year os : 962% ) and comparable to previous monoinstitutional lgg series [ 19 ]  . 
3 9 progressionfree and overall survival of all patients with primary intracranial , nonmetastatic pilocytic astrocytoma who underwent stereotactic brachytherapy or external fractionated radiotherapy as firstor second - line nonsurgical treatment fig . 
 [ 25 ] published the outcome of 78 pediatric lgg patients treated between 1997 and 2006 and reported pfs and os rates of 74 and 96% , respectively , 10 years after the start of rt . 
reported the results of stereotactically guided conformal rt ( scrt ) in 14 pediatric lgg patients ( median age 6 years , range 516 years ) treated between 1994 and 1999 . 
the 3 - year local pfs and os rates after scrt were 87 and 100% , respectively [ 34 ]  . evaluation of possible prognostic factors for lgg progression after efrt tumor location the influence of tumor location on disease progression is still subject to discussion . 
 [ 8 ] observed that patients with cerebellar and cerebral hemisphere tumors had a significantly higher pfs than children with tumors at all other sites combined ( in univariate analyses )  . 
 [ 32 ] did not confirm the unfavorable impact of central midline tumor location on disease progression . age at the beginning of rt using cutoffs of 5 and 10 years , we could not find an impact of age on disease progression after efrt in univariate analyses . 
6 9 impact of the normalized total dose ( according to the linear - quadratic model [ 15 ] , / = 10 , single dose 1.8 gy ) on progression - free survival after external fractionated radiotherapy multivariate analyses . 
 in a study assessing 71 children ( 20 nonpilocytic astrocytomas , 22 pilocytic astrocytomas , 20 mixed oligoastrocytomas and 8 oligodendrogliomas ) no difference in pfs was seen between the < 10and 10 - year age groups [ 31 ]  . dose prescription in adult lgg , two prospective randomized trials failed to establish a benefit of doses exceeding 45 gy [ 16 , 36 ]  . in children , no prospective randomized trials evaluating doseresponse relationship have been performed . 
additionally , it can be assumed that the dose prescriptions were strongly influenced by patient age , extent of disease and site of the tumor , with a tendency towards lower doses in younger children with larger tumors . 
however , the optimal efrt dose for pediatric lgg still needs to be defined in a prospective trial . prior chemotherapy data on the efficacy of rt after progression following chemotherapy are scarce . 
on the other hand , the authors also stated that a recurrence rate of 7 / 17 ( 41% ) was not different from the recurrence rates following first - line rt previously described by other authors . 
after interstitial sbt the 5 - year pfs rate was 658% ( 10 - year pfs : 589% ) and the 5and 10 - year os rates were 973% in our series . 
since most of the children who underwent sbt within the hit - lgg 1996 study were treated in the two respective institutions , there are some overlaps between these two reported patient cohorts and our series . limitations of this study a major limitation of the hit - lgg 1996 study is the failure to assess systematically the long - term functional outcome after chemotherapy and rt . 
an important objective of the subsequent siop - lgg 2004 study is to correlate radiation doses in organs at risk with functional outcome in order to generate valid dose constraints . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 639646 doi 10.1007 / s00066 - 013 - 0341 - 2 received : 1 march 2013 accepted : 6 march 2013 published online : 9 june 2013 springer - verlag berlin heidelberg 2013 n.d.seibold1s.e.schild2m.p.gebhard3f.noack3d.rades1 1 department of radiation oncology , university of lubeck 2 department of radiation oncology , mayo clinic scottsdale 3 institute of pathology , university of lubeck prognosticimpactofvegfandflt - 1 receptorexpressioninpatientswith locallyadvancedsquamouscell carcinomaoftheheadandneck personalized treatment is important for patients with locally advanced squamous cell carcinoma of the head and neck ( scchn )  . 
the prognostic value of tumor cell expression of vascular endothelial growth factor ( vegf ) and its receptor fms - related tyrosine kinase 1 ( flt - 1 ) is controversial . 
it has been suggested that vegf expression is negatively associated with patient prognosis in esophageal and head and neck cancer [ 3 , 4 , 18 , 19 ] , whereas no significant prognostic association has been observed in patients with non - small cell lung and epithelial ovarian cancer [ 7 , 15 , 17 ]  . 
regarding flt - 1 expression , studies of esophageal and nonsmall cell lung cancer , as well as of scc of the tongue did not find a significant association with treatment outcome [ 7 , 12 , 15 , 17 , 19 ]  . 
in patients with locally advanced breast and pancreatic cancer , flt - 1 expression has been suggested to be a positive predictor for treatment outcomes [ 5 , 21 ]  . taking into account the available data , it appears that further research is needed to identify the prognostic value of tumor expression of vegf and flt - 1 . 
this study investigated the potential prognostic role of tumor cell vegf and flt - 1 expression with respect to loco - regional control ( lc ) , metastases - free survival ( mfs ) and overall survival ( os ) in patients who received radiotherapy or radiochemotherapy following resection of nonmetastatic stage iii / iv scchn . materials and methods expression of vegf and flt - 1 was evaluated in tumor samples obtained from patients who had been treated with surgery followed by radiotherapy or radiochemotherapy for locally advanced scchn between 2000 and 2009 . 
the study was approved by the local ethics committee . immunohistochemistry resection specimens were fixed in 4% buffered formalin ( ph 7.0 ) and embedded in paraffthe formalin - fixed , paraffin - embedded tumor samples were used for the preparation of a tissue microarray ( tma ) block . 
the tma block was constructed using a manual tissue arrayer 1 ( beecher instruments , silver spring , md , usa ) with a 1.0 - mm diameter core biopsy needle . 
endogenous peroxidase was blocked with 0.3% hydrogen peroxide for 5 mthe sections were then incubated with anti - human vegf polyclonal antibody ( mouse ; 1 / 100 dilution ; santa cruz biotechnology , heidelberg , germany ) and anti - human flt - 1 monoclonal antibody ( mouse , 1 / 30 dilution ; santa cruz biotechnology )  . 
sections were washed with tbs containing 0.1% tween 20 ( ph 7.0 ) and subsequent detection was performed with the biotinfree horseradish peroxidase labeled polymer of the powervision system ( immunologic , duiven , netherlands )  . 
 as a positive control , samples from blood vessels near or within the tumor sample were checked . patients and treatment data from 157 patients treated with surgery and postoperative radiotherapy for locally advanced scchn between 2000 and 2009 were retrospectively analyzed . 
further inclusion criteria were successful staining for vegf or flt - 1 ; histologically confirmed scc arising from the oropharynx , oral cavity , hypopharynx or larynx and stage iii or iv disease . 
1 patient characteristics 78 ( 50 ) 79 ( 50 ) no.ofpatients ( % ) 50 ( 32 ) 107 ( 68 ) 37 ( 24 ) 120 ( 76 ) 103 ( 66 ) 54 ( 34 ) 110 ( 70 ) 36 ( 23 ) 11 ( 7 ) 32 ( 20 ) 117 ( 75 ) 8 ( 5 ) vegfexpression not available flt - 1expression not available 60 years > 60 years gender female male ecogperformancescore hemoglobinlevelpre - rt < 12 g / dl 12 g / dl tumorsite oropharynx oral cavity hypopharynx larynx histologicgrade g12 t - category n - category hpvstatus negative positive extentofresection complete incomplete chemotherapy vegf vascular endothelial growth factor , flt - 1 fms - related tyrosine kinase 1 , ecog eastern cooperative oncology group , pre - rt pre - radiotherapy . 64 ( 41 ) 32 ( 20 ) 23 ( 15 ) 38 ( 24 ) 136 ( 87 ) 21 ( 13 ) 124 ( 79 ) 33 ( 21 ) 66 ( 42 ) 91 ( 58 ) 67 ( 43 ) 90 ( 57 ) 90 ( 57 ) 67 ( 43 ) 61 ( 39 ) 96 ( 61 ) mor plus bilateral modified radical neck dissections . 
patients with specific risk factors such as incomplete resection and extracapsular spread of lymph nodes received concurrent chemotherapy comprising 20 mg / m2 of cisplatin on days 15 and 2933 , or 20 mg / m2 of cisplatin plus 600 mg / m2 5 - fluorouracil on days 15 and 2933 . hpv status formalin - fixed , paraffin - embedded tumor probes were analyzed for the dna of high - risk hpv subtypes 16 , 18 , 31 , 33 and 51 by chromogenic in situ hybridization ( cish ) marked with anti - biotin - antibody ( processed in an autostainer )  . 
positive control was a squamous - type carcinoma in situ of the cervix uteri from a patient with known hpv subtype ( hpv - chip type 3.5c , chipron gmbh , berlin , germany )  . 
prognostic factors found to be significant or almost significant ( p < 0.06 ) in the univariate analysis were included in a multivariate analysis performed using the cox proportional hazards model . results in the univariate analysis , improved lrc was associated with an absence of vegf expression ( .fig.1 , p = 0.005 ) , an absence of flt - 1 expression ( .fig.2 , p = 0.023 ) , female gender ( p = 0.035 ) , better performance status ( ecog 01 ; p = 0.035 ) , pre - rt hemoglobin levels 12 g / dl ( p = 0.012 ) , lower t - category ( t1 t2 ; p < 0.001 ) , lower n - category ( n0n1 ; p = 0.043 ) and hpv positivity ( p = 0.023 ) as shown in .tab.2. 
in the abstract zusammenfassung strahlenther onkol 2013 189 : 639646 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0341 - 2 n.d.seibolds.e.schildm.p.gebhardf.noackd.rades prognostic impact of vegf and flt - 1 receptor expression in patients with locally advanced squamous cell carcinoma of the head and neck abstract backgroundandpurpose . 
the impact of tumor cell vegf and flt - 1 expression plus 11 additional factors on loco - regional control ( lrc ) , metastases - free survival ( mfs ) and overall survival ( os ) was retrospectively evaluated in 157 patients . 
flt - 1 expression was not significant in multivariate analyses . keywords growth factors radiotherapy radiochemotherapy survival prognosis prognostische bedeutung der vegfund flt - 1 - expression bei patienten mit lokal fortgeschrittenem plattenepithelkarzinom der kopf - hals - region zusammenfassung hintergrundundzielsetzung . 
der einfluss der expression von vegf und flt - 1 in tumorzellen sowie 11 weitere prognosefaktoren wurden bei 157 patienten hinsichtlich der lokoregionalen kontrolle ( lrc ) , des metastasenfreien berlebens ( mfs ) und des gesamtberlebens ( os ) retrospektiv untersucht . 
die expression von vegf erwies sich als unabhngiger negativer prognosefaktor hinsichtlich lrc , mfs und os bei patienten , die bei einem lokal fortgeschrittenen scchn eine adjuvante strahlentherapie oder radiochemotherapie erhalten hatten . 
according to our results , vegf expression is an independent prognostic factor for all three investigated endpointslrc , mfs and os whereas the role of flt - 1 remains uncerta although significantly associated with lrc and os in the univariate analyses , flt - 1 expression was not significant in the corresponding multivariate analyses . regarding the results of this study with respect to the prognostic value of tumor cell vegf expression , our findings agree with the majority of studies that have investigated the association between vegf expression and outcomes in patients with scchn . 
 [ 19 ] suggested vegf - c expression to be a predictive factor for regional lymph node recurrence in a series of 73 patients with scc of the tongue : 5 - year survival rates were 94% in vegf - c - negative patients and 52% in vegf - c - positive patients . 
 in a 2011 retrospective study of 90 patients with oral scc , patients with strong vegf - a or vegf - c expression had a significantly worse prognosis than other patients [ 18 ]  . 
patients with a tumor having a high vegf labeling index had a higher proportion of lymph node metastases ( p = 0.022 ) , more advanced clinical stages ( p = 0.046 ) and worse survival rates ( p = 0.016 ) [ 4 ]  . 
 [ 20 ] presented 30 patients with laryngeal cancer and observed a close correlation between vegf expression and lymph node involvement , but did not correlate vegf expression to treatment outcome . 
in contrast , three other retrospective studies did not find a significant correlation between vegf expression and treatment outcomes in patients with nonsmall cell lung cancer and epithelial ovarian cancer [ 7 , 15 , 17 ]  . 
in another retrospective study of 61 patients irradiated for stage ii / iii non - small cell lung cancer , vegf expression was not associated with local control , mfs or os [ 15 ]  . 
 [ 17 ] did not find a significant correlation between vegf expression and progression - free survival or os in a series of 67 patients with epithelial ovarian cancer . regarding the prognostic value of tumor cell flt - 1 expression , the data in the literature are even more heterogeneous than for vegf expression . 
in keeping with the present results , previous retrospective studies did not show a correla644 | strahlentherapieundonkologie82013 tion between flt - 1 expression and treatment outcomes for various tumor types including either epithelial ovarian cancer [ 17 ] , cancer of the tongue [ 19 ] , esophageal cancer [ 7 ] or non - small cell lung cancer [ 15 ]  . 
in another retrospective study of 76 patients with pancreatic adenocarcinoma , low flt - 1 expression was associated with a worse prognosis and more advanced tumor stages than high flt - 1 expression [ 5 ]  . 
 [ 11 ] reported that flt - 1 expression was correlated with lymph node metastasis in a series of 39 patients with differentiated thyroid carcinoma . in addition to an absence of vegfexpression , improved treatment outcomes were significantly associated with a lower tumor stage , a favorable tumor location and higher pre - rt hemoglobin levels . 
additionally , tumor site and pre - rt hemoglobin levels were previously identified as prognostic factors for treatment outcomes in patients with locally advanced scchn [ 1 , 16 ]  . 
the prognostic value of the hpv status is less evident the present study than in our previous report [ 14 ] , which may be explained by the fact that patients treated with definitive radiotherapy or radiochemotherapy were excluded from the present study ( but included in the previous trial )  . 
for unresected disease , the combination of concurrent chemoradiation has been shown to be more effective than sole radiotherapy ( rt ) in several randomized trials and is , therefore , considered standard of care in this situation . 
 although the role of surgery in locally advanced disease is not well defined , many centers prefer surgery of the primary tumor in combination with therapeutic and elective neck dissections , if the expected functional outcome is deemed acceptable for the patient from the surgical perspective . 
as in unresectable scchn , concurrent chemoradiation was also shown to be more effective than sole radiotherapy in three large independent randomized trials in the postoperative setting [ 5 , 10 , 15 ]  . 
a meta - analysis of two of these trials ( rtog 9501 , [ 11 ] and eortc 22931 , [ 5 ] ) indicated that concurrent chemoradiation is especially beneficial in terms of locoregional tumor control and overall survival , if at least one of the following high risk features is present : lymph node involvement with extracapsular tumor extension ( ece ) or close surgical resection margin < 5 mm [ 5 ]  . 
 adjuvant radiotherapy was administered in conventional fractionation ( 5 fractions of 2 gy per week ) to total doses of 64 [ 13 ] up to 66 gy [ 5 , 10 ]  . 
concurrent chemotherapy consisted either of cisplatin 20 mg / m2 and continuous infusion of 5 - fu 600 mg / m2 on days 15 and 2933 , or of cisplatin 100 mg / m2 on days 1 , 22 , and 43 [ 5 , 10 ]  . 
this indicates that more effective approaches , attacking locoregional disease and distant metastases , are needed . in scchn , high levels of epidermal growth factor receptor 1 ( egfr1 ) are almost always expressed . 
animal studies on human scchn presumed additive and synergistic effects for the combination of cetuximab with both radiotherapy and cisplatin [ 20 , 22 ]  . consequently , concomitant administration of cetuximab during 67 weeks of rt was tested in unresected locally advanced scchn , demonstrating improved locoregional tumor control and overall survival [ 7 ]  . 
cetuximab given for 6 weeks concurrently to radiotherapy did not result in a significant reduction of the distant metastases rate . based on these considerations , we evaluated the feasibility and efficacy of adjuvant chemoradiation with concomitant and maintenance cetuximab therapy in patients with high risk of locoregional and distant recurrence in a phase ii trial . 
here , we present the interim results of the open label multicenter phase ii trial focusing on feasibility and acute toxicity of the regimen . patient and methods a multicenter , uncontrolled open - label phase ii trial was performed to evaluate safety and efficacy of post - operative radiochemotherapy ( rct ) in combination with cetuximab in scchn patients . 
the secondary objectives of this study were the 2 - year disease - free survival rate , the incidence of locoregional relapses , progression - free survival , overall survival , the rate of patients with secondary primary neoplasm , and the incidence of late toxicity . the study was conducted at 10 investigational sites recruiting in germany from may 2008 until december 2010 . 
close resection margins < 5 mm ( cm ) or extra capsular extent at the lymph nodes ( ece ) impair the prognosis of patients with squamous cell cancer of the head and neck ( scchn ) scheduled for adjuvant radiochemotherapy . 
cisplatin ( 20 mg / m2 , days 15 and days 2933 ) and 5 - fluorouracil ( 5 - fu ) as continuous infusion ( 600 mg / m2 , days 15 + days 2933 ) were given concurrently . 
of the 55 patients ( 46 male , 9 female , mean age 55.6 , range 2970 years ) who finished radiochemotherapy , 50 were evaluable for acute toxicity concerning grade iii / iv toxicities of skin and mucosa . 
 grade 34 ( ctc 3.0 ) mucositis , radiation dermatitis , and skin reactions outside the radiation portals were documented for 46 , 28 , and 14% of patients , respectively . 
compliance within the first 35 months is moderate . keywords adverse effects clinical trial , phase ii head and neck neoplasms toxicity interim analysis durchfhrbarkeit einer 6 - monatigen cetuximab - erhaltungstherapie nach adjuvanter gleichzeitiger chemoradiotherapie plus cetuximab bei plattenepithelkarzinomen des kopf - hals - bereichs zusammenfassung hintergrund . 
die prognose von patien ten mit plattenepithelkarzinomen im kopf - halsbereich ( scchn , squamous cell cancer of the head and neck ) nach adjuvan ter radiochemotherapie ist weiterhin unbefriedigend , sofern < 5 mm im gesunden reseziert wurde oder an den lymphknoten ein extrakapsulres wachstum ( ece ) nachweisbar war . 
 aus diesem grund fhrten wir eine multizentrische phase - ii - studie zur untersuchung der toxizitten und der wirksamkeit der adjuvanten radiotherapie in kombination mit cisplatin , 5 - fluorouracil ( 5 - fu ) und cetuximab gefolgt von einer erhaltungstherapie mit cetuximab fr 6 monate durch . 
patienten , mit plattenepithelkarzinomen im kopf - hals - bereich , die operiert wurden und bei denen ein hohes risiko fr ein lokalrezidiv bestand ( resektionsrand < 5 mm ; ece ) , wurden in die studie eingeschlossen . 
die strahlentherapie erfolgte mit integrierter boost - imrt - technik ( 1 , 8 / 2 , 0 / 2 , 2 gy , tage 136 ) bis zu einer gesamt dosis von 61 , 6 gy . 
als chemotherapie wurden cisplatin ( 20 mg / m2 tag 15 und tag 2933 ) und 5 - fluouracil ( 5 - fu ) als kontinuierliche infusion ( 600 mg / m2 tag 15 plus tag 2933 ) simultan zur adjuvanten radiochemotherapie gegeben . 
die gabe von cetuximab begann 7 tage vor start der radiochemotherapie mit einer dosierung von 400 mg / m2 durch wchentliche cetuximab - gaben ( 250 mg / m2 ) whrend der kombinierten radiochemotherapie . 
von 55 patienten ( 46 mnner , 9 frauen , durchschnittsalter 55 , 6 jahre , spanne 2970 jahre ) , die die kombinierte therapie ( radiochemotherapie + cetuximab ) beendeten , konnten bei 50 patienten die akuttoxizitten grad 34 an haut und schleimhaut anhand der ctc - 3.0 - kriterien augewertet werden . 
simultan zur kombinierten radiochemotherapie war bei 46% der patienten eine mukositis vom grad 34 , bei 28% der patienten eine hautreaktion vom grad 34 im bestrahlungsfeld und bei 14% der patienten eine hautreaktion auerhalb des bestrahlungsfeldes vom grad 34 zu verzeichnen . 
die compliance bei der erhaltungstherapie mit cetuximab ist innerhalb der ersten 35 monate befriedigend . schlsselwrter unerwnschte nebenwirkungen klinische phase - ii - studie kopf - hals - neoplasien toxizitt interimanalyse strahlentherapieundonkologie82013 | original article tab . 
1 clinical outcome for patients with high risk head and neck cancer eortc #22931 rtog #9501 eortc european organization for research and treatment of cancer , rtog radiation therapy oncology group , aro arbeitsgemeinschaft radiologische onkologie ( association for radiation oncology )  . 5 - yearlocoregionalfailure ( % ) 5 - yeardistantmetastasis ( % ) tab . 
4 patient compliance radiotherapy ( n = 55 ) chemotherapy ( n = 55 ) ( incl . a / b / c ) unknown 95105% of prescripted dose ( 61.6 gy ) n = 49 5 patients : data pending , 1 patient interrupted radiotherapy at 55 gy for unknown reason 100% , n = 37 90% , n = 3 patient 1 : cisplatin : 100% , 5 - fu : 60% ( bradycardia ) patient 2 : cisplatin : 80% , 5 - fu : 80% . patient 3 : cisplatin : 90% , 5 - fu : 90% ( interruption due to port implantation ) 75% , n = 1 cisplatin : 100% , 5 - fu : 75% ( mucositisiii ) 65% , n = 1 cisplatin : 50% ( no 2nd cycle , adverse event : polyneuropathia grade iii ) 5 - fu : 80% ( problems with central line ) 50% , n = 5 1 . 
cisplatin : 50% , 5 - fu : 50% ( no 1st cycle ) 25% , n = 1 cisplatin : 25% , 5 - fu : 0% 7 patients data pending fsubmental nodes ( surgical level ia ) : in cases where the floor of mouth or level ib were involved . fsubmandibular nodes ( surgical level ib ) : all cases except primary palate tumors which did not extend to the tonsil or base of tongue . 
all targets were treated simultaneously using an integrated boost imrt technique . the following guidelines for dose prescriptions to target volumes and organs at risk were provided in the protocol : fno more than 20% of any ptv received > 110% of its prescribed dose . fno more than 3% of any ptv received < 90% of its prescribed dose ( exception : skin with a 23 mm internal margin , if regarded as region of low risk for recurrence )  . fno more than 1% or 1 ml of the tissue outside the ptvs received > 110% of the dose prescribed to the primary ptv . dosevolume histograms ( dvhs ) were generated for all critical normal structures and the unspecified tissues . 
dose constraints to normal tissues were as follows : fplanning organ at risk volume ( prv ) of the brainstem 54 gy / < 1 / 3 of cross sections and < 2 ml : 60 gy , fprv of the spinal cord 45 gy / < 1 / 3 of cross sections and < 2 ml : 54 gy , fprv of the optic nerve 54 gy , fprv of the optic chiasm 54 gy , fprv of the inner ear 54 gy , fprv of the mandible 70 gy , funspecified tissue outside the targets : < 110% of the prescribed dose to ptv 61.6. recommended planning goals of the parotid glands were ( 1 ) mean dose to either parotid < 26 gy , or ( 2 ) at least 50% of the either parotid gland will receive < 30 gy , or ( 3 ) at least 20 ml of the combined volume of both parotid glands will receive < 20 gy . 
other common radiation toxicities included fatigue , weight loss , regional alopecia , xerostomia , hoarseness , transient ear discomfort , hypogeusia , dysgeusia , dysphagia , and skin erythema and desquamation within the treatment fields , and also recorded was whether a feeding tube was placed for nutritional supplementation . 
these data , escpecially late effects will be published later . the interim analysis provided in this publication on the first 55 of 80 planned patients treated in the protocol was restricted to feasibility and acute grade iii / iv side effects . 
the study protocol was approved by the central ethics committee and the institutional review boards of all participating institutions , and each patient provided written informed consent before participating in the study statistical analysis primary endpoints for this planned interim analysis were toxicity and compliance . 
all data were collected in an excel tm ( microsoft corporation , redmond , wa , usa ) datasheet and transferred to the coordination center for clinical trials at the university of dsseldorf . 
concurrent crt plus cetuximab was associated with grade 34 ( ctc 3.0 ) mucositis , radiation dermatitis , and skin reaction outside the radiation portals in 46 , 28 , and 14% of patients , respectively . 
acute toxicity , especially skin and mucosal toxicity as well as incompliance of the patients were the main reasons for cessation of further cetuximab treatment . discussion the disease - free survival of patients with scchn 5 years after surgery and adjuvant chemoradiation is not higher than 36% , if high risk features like extracapsular tumor extension at involved lymph nodes or a close resection margin ( < 5 mm ) is present . 
the reported benefits for the addition of concurrent cetuximab to radiotherapy in unresected locally advanced scchn and for addition of concurrent and maintenance cetuximab to cisplatin and 5 - fu in recurrent and metastatic scchn prompted us to initiate a phase ii trial on adjuvant chemoradiation in combination with concurrent and maintenance cetuximab therapy . the preliminary results presented here indicate that the regimen is feasible with a grade iii / iv acute toxicity within the upper limits of the expected range . 
as anticipated rates of grade iii / iv skin toxicities inside ( 28% ) and outside ( 14% ) the radiation portals were higher than typically reported for adjuvant chemoradiation without cetuximab [ 1 , 10 , 13 ]  . 
the rate of acute grade iii / iv mucositis ( 46% ) was in the upper range compared to the experiences of other groups applying adjuvant chemoradiation alone [ 13 , 16 ]  . 
the concert - 1 trial tested the same concept , but used panitumumab , a fully humanized anti - egfr - antibody binding to the identical epitope of the egfr as cetuximab . 
the number of evaluable patients in these trials ( rtog 0522 : n = 895 ; concert - 1 : n = 150 ) appear to be sufficient to exclude a relevant benefit for patients with unresected locally advanced scchn from the concurrent addition of an egfr antibody to chemoradiation . 
2 8 kaplanmeier estimates the reason of cessation during the study likely that the addition of cetuximab or panitumumab to adjuvant chemoradiation after surgery will result in a clinical benefit for these patients . 
regardless the final oncological outcome of the phase ii trial presented here , the further development of the concept of concurrent cetuximab and chemoradiation seems to be a dead end . the question arises whether maintenance therapy in the clinical setting would do the same . 
a significantly improved survival was reported in recurrent and metastatic scchn for adding concurrent and maintenance cetuximab to cisplatin plus 5 - fu [ 24 ] , whereas no significant survival benefit was observed in the same setting for adding concurrent panitumumab without maintenance therapy to cisplatin plus 5 - fu ( sepctrum - 1 )  . 
since chemoradiation without concurrent cetuximab induces less acute toxicity [ 8 , 17 ] , one would expect that a higher percentage of patients would be able and willing to start maintenance cetuximab after chemoradiation alone . 
once maintenance therapy with cetuximab had been started , adherence to the protocol was quite satisfactory for the first 3 months ( 80% ) , but declined to 63% at 5 months and to 48% at the planned completion of the therapy at 6 months . 
most discontinuations were caused by patients incompliance and some unknown reasons , the latter most likely also as a result of a patients incompliance . the experience with maintenance cetuximab after chemoradiation is otherwise very limited . 
 [ 4 ] tested in a small phase ii trial the addition of cetuximab during induction chemotherapy and during concurrent radiotherapy with cisplatin followed by 6 months maintenance therapy with cetuximab in 39 patients with locally advanced scchn . 
 neutropenic fever ( 10% ) was the most relevant severe toxicity during the induction phase of the protocol , whereas dur630 | strahlentherapieundonkologie82013 ing chemoradiation and concurrent cetuximab grade iii / iv mucositis ( 54% ) was the crucial acute toxic reaction . 
belka received from merck support for translational research within the framework of the accra study , is a speaker at scientific meetings with support from merck , and organizes scientific meetings together with merck . 
giro c , berger b , bolke e et al ( 2009 ) high rate of severe radiation dermatitis during radiation therapy with concurrent cetuximab in head and neck cancer : results of a survey in eortc institutes . 
jordi g , andre f , ricard m et al ( 2012 ) a phase ii , randomized trial ( concert - 1 ) of chemoradiotherapy ( crt ) with or without panitumumab ( pmab ) in patients ( pts ) with unresected , locally advanced squamous cell carcinoma of the head and neck ( lascchn )  . 
thariat j , milas l , ang kk ( 2007 ) integrating radiotherapy with epidermal growth factor receptor antagonists and other molecular therapeutics for the treatment of head and neck cancer . 
vermorken jb , guigay j , mesia r et al ( 2011 ) phase i / ii trial of cilengitide with cetuximab , cisplatin and 5 - fluorouracil in recurrent and / or metastatic squamous cell cancer of the head and neck : findings of the phase i part . 
er hat die deutschen hodgkinstudien im erwachsenenund kindesalter seit 1977 wesentlich mitgestaltet und geprgt . seit 1977 hatte er den lehrstuhl fr strahlentherapie in freiburg inne , nachdem er den ruf nach erlangen und spter auch nach hamburg abgelehnt hatte . 
dadurch prgt er mit groem wissensschatz und viel erfahrung auch heute noch ber seine schlerinnen und schler die radioonkologische landschawir wnschen ihm weiterhin viel freude an den frchten seines erfolges und gesundheitlich alles gute . jrgen debus , heidelberg korrespondenzadresse j . 
ein weiterer wissenschaftlicher schwerpunkt war die kombinierte radiochemotherapie unter dem aspekt der radiosensibilisierung durch zellsynchronisation . besondere bekanntheit in deutschland hat wannenmacher durch die einfhrung der grofeldbestrahlung bei ma708 | strahlentherapieundonkologie82013 laudatio strahlenther onkol 2013 189 : 709710 doi 10.1007 / s00066 - 013 - 0376 - 4 online publiziert : 25 . 
 fnf jahre spter ( 1979 ) nahm er die einladung auf eine gastprofessur am department of therapeutic radiology , radiation biology and physics division des henry ford hospitals in detroit ( usa ) an . 
die ernennung zum c3 - professor und leiter der abteilung fr angewandte physiologie am fachbereich medizin der universitt mainz erfolgte 1983 . aufgrund seines hohen wissenschaftlichen renommees erhielt er 1986 den ehrenvollen ruf als full professor an der harvard university in boston . 
whrend seiner zeit als andrew werk cook professor fr strahlenbiologie , tumorbiologie und physiologie an dieser amerikanischen eliteuniversitt erfolgten rufe auf c4 - professuren an die universitten mnster ( abgelehnt ) und mainz . 
den ruf auf den lehrstuhl fr pathophysiologie im fachbereich medizin der johannes gutenberg - universitt mainz nahm er 1989 an . die amtszeit als ordinarius dauerte bis zur pensionierung im september 2008 . 
peter vaupel , facharzt fr physiologie seit 1996 , setzte sich mit kraft fr eine klinikorientierte ausbildung der studierenden im fach physiologie eseine vorlesungen , seminare und praktika , die er mit hohem engagement und pflzischem timbre hielt , fanden groen anklang . 
so betreute er 41 medizin - doktoranden , 10 biologiediplomanden und 11 habilitanden , 5 davon im fach physiologie , 6 weitere in chirurgie , gynkologie , pdiatrischer onkologie und strahlentherapie . 
auch hieran zeigt sich , dass der wissenschaftliche input von peter vaupel weit ber die engeren fachgrenzen reichte bis hinein in verschiedene disziplinen der klinischen medizsein einsatz fr die mainzer fakultt ist durch seine langjhrige mitgliedschaft im fachbereichsrat medizin sowie seine 10 - jhrige ttigkeit als vorsitzender des bereichsausschusses vorklinik wie auch durch dienste als prodekan des fachbereichs medizin ( 19971999 ) belegt . 
bereits 1969 wurde er mit einer dissertationsschrift aus dem bereich der biophysik promoviert . nach der medizinalassistentenzeit und der approbation als arzt nahm er 1970 das angebot an , als wissenschaftlicher assistent an das damalige physiologische institut der mainzer universitt zu wechseln , das von professor g . 
zu diesen gehren cancer research ( ber 20 jahre ) , international journal of radiation oncology , biology , physics ( 16 jahre ) , strahlentherapie und onkologie und andere . 
weiterhin war er von 1989 bis 2008 vorsitzender des ausschusses fr die zahnrztliche vorprfung und von 1990 bis 2003 mitglied der medizinischen sachverstndigenkommission des instituts fr medizinische und pharmazeutische prfungsfragen ( impp , fachgebiet pathophysiologie )  . die breit angelegten aktivitten von peter vaupel wurden durch zahlreiche ehrungen ausgezeichnet : boehringer - ingelheim - forschungspreis ( 1974 ) , berufung als sachverstndiger der kommission fr humanforschung der akademie der wissenschaften und der literatur zu mainz ( 19831998 ) , vorsitzender der deutschen gesellschaft fr mikrozirkulation ( 1983 , 1991 ) , honorary masters degree ( m.a. ) der harvard university ( 1988 ) , lund science award ( 1989 ) , stiftungsrat der med . 
wulf vater stiftung , mainz ( seit 1996 ) , ordentliches mitglied der akademie der wissenschaften und der literatur zu mainz ( seit 1998 ) , vorsitzender der kommission fr humanforschung an der akademie der wissenschaften und der literatur zu mainz ( 19992003 ) , berufung als mitglied der kommission fr theoretisch - medizinische forschung an der akademie der wissenschaften und der literatur zu mainz ( seit 2003 ) , eshoaward ( 2004 ) , 1st robert f . 
kovach memorial lecture , isott ( 2012 ) , outstanding research award in recognition of contributions to the identification , characterization and targeting of the tumor microenvironment for the advancement of cancer therapy and patient care , miami , usa ( 2013 ) u . 
weiterhin wurden ihm von der scientific associa tion of swiss radiation oncology ( sasro , 2004 ) und der deutschen gesellschaft fr radioonkologie ( degro , 2006 ) ehrenmitgliedschaften verliehen . seit 2008 ist peter vaupel an der klinik fr strahlentherapie und radiologische onkologie der technischen universitt mnchen als gastprofessor ttig . 
die derzeitige arbeitswoche in mnchen ist charakterisiert durch lesen , schreiben , diskussionen inklusive besprechen von experimenten und den allabendlichen rckzug zur nachtruhe ins mnchener haus der redemptoristen , zu denen peter vaupel freundschaftliche kontakte hlt . 
 peter vaupel steht in mnchen in direktem austausch mit klinikern und in kooperation mit biologinnen und biologen , um das groe und wichtige thema tumorpathophysiologie , tumorhypoxie und tumormikromilieu intensiv weiter zu bearbeiten nicht nur , um neue wissenschaftliche erkenntnisse zu generieren , vielmehr auch , um klinisch nutzbare beitrge zu liefern , die in zukunft dem krebskranken von vorteil sind . 
vielleicht ist auch hier eine triebfeder fr seine forschung zu sehen , die ihn in der klinischen onkologie und strahlentherapie zu einem weltweit hoch anerkannten wissenschaftler und gelehrten hat werden lassen . als freund und freunde schtzen wir peter vaupels nachdenklichkeit , verbunden mit dem sinn fr liberalitas , seine pflzische bodenstndigkeit und seinen humor . 
 geburtstag noch viele gesunde , glckliche jahre und eine weiterhin anhaltende kraft fr das von ihm sehr gemochte internationale reisen zu kongressen , zu vortrgen und zum kontakthalten mit weltweit ansssigen freunden . michael molls , mnchen 710 | strahlentherapieundonkologie82013 original article strahlenther onkol 2013 189 : 675683 doi 10.1007 / s00066 - 013 - 0347 - 9 received : 4 june 2012 accepted : 6 march 2013 published online : 20 . 
the mechanism of radiation - induced cell death includes induced apoptosis , and recent studies have revealed that micrornas ( mirnas ) may post - transcriptionally regulate the expression of stress response genes that control cell survival and apoptosis . 
mir - 17 - 92 ( mir - 17 ) is a polycistronic mirna that encodes seven mature mirnas , and was the first characterized mirna to be associated with cancer [ 3 , 4 , 5 ]  . 
mir - 19 , which is a component of the mir - 17 - 92 / oncomir - 1 microrna polycistron , regulates the expression of the antiapoptotic ras homolog b ( rhob )  . 
this process also requires the binding of the human antigen r protein ( hur ) , an au - rich element binding protein , to the 3 - untranslated region of the rhob mrna , in keratinocytes exposed to ultraviolet radiation [ 6 ]  . 
the role that the mir - 17 polycistron plays in response to radiotherapy in oral cancer remains unclear . to address this gap in knowledge , we examined radiation - induced changes in mir - 17 expression and function in oc3 , an oral carcinoma cell line that was established from an oral squamous cell carcinoma in a long - term betel nut chewer who does not smoke [ 7 ]  . 
many studies have revealed that , when gamma - radiation leads to dna damage response , dna - damaging agents activate the p53 signaling pathway and activate cell cycle checkpoints to promote survival or apoptotic cell death . 
we demonstrate that mir - 17 - 5p modulates the expression of the cyclindependent kinase inhibitor ( cdki ) p21 in oc3 cells following irradiation . materials and methods cell culture the oral carcinoma 3 ( oc3 ) cell line was cultivated in combined k - sfm - dulbecco modified eagles medium ( 2 : 1 , v / v , invitrogen ) containing 10% fetal bovine serum . strahlentherapieundonkologie82013 | sham sham 1 gy 1 gy 2 gy 2 gy 3 gy 4 gy 5 gy sham original article sha m 1 gy 2 gy 3 gy 4 gy 5 gy mir17 3p mir17 5p mirmirmirmirmir1 gy 2 gy 3 gy 4 gy 5 gy fig . 
d oc3 cells were irradiated ( 15 gy ; rt ) or remained unirradiated ( sham ) and 6 h later the expression of the mir - 17 - 92 cluster of mirnas was determined by realtime pcr . 
the dose rate was approximately 1 gy / min . quantitative detection of the mir - 17 - 92 cluster the mir - 17 - 92 cluster was detected by using the real - time pcr assay kit ( signosis inc . , sunnyvale , ca , usa )  . 
this approach implements oligoligation and sybr green - based real - time pcr . mir - 17 - 5p and p21 antisense oligonucleotides colony formation assay the 5 - acuaccugcacuguaagcacuuug - 3 2 - o - methyl oligonucleotide ( dharmacon ) was used for anti mir - 175p . 
 the oligonucleotides were resuspended in dnase - free water to form 1 m solutions , and they were mixed with an equal volume ( 10 : 1 ) of transfast for 15 min and then incubated with the cells in serum - free medium . oc3 cells ( 500 / well ) transfected with mir - 17 - 5p antisense oligonucleotides were seeded in six - well plates , and after 24 h they were treated with 5 gy of radiation . 
after an additional 7 days , colonies ( clusters of more than 50 cells ) were counted and digitally photographed . cell transfection and the generation of a stable cell line human pre - microrna expression construct lenti - mir - 17 ( pmirh17aa - 1 , system biosciences , mountain view , ca ) was transfected into the oc3 cell line to 676 | strahlentherapieundonkologie82013 modulate the expression of mir - 17 - 5p , and to study microrna function with the lipofetamine plus reagent ( invitrogen )  . 
a 50 g protein sample was separated by 10% of sodium dodecyl sulfate polyacrylamide ( sdspage ) gel electrophoresis , and then transferred onto a polyvinylidene difluoride ( pvdf ) membrane . 
the signal was visualized on x - ray film after detection with an enhanced chemiluminescent detection systeantibodies to p21 and glyceraldehyde - 3 - phosphate dehydrogenase ( gapdh ) were from santa cruz biotechnology ( santa cruz , ca , usa )  . cell cycle analysis the analysis of the cell cycle stages was performed by quantifying the dna content with propidium iodide staining and by using facscan and the cell quest software ( becton dickinson immunocytometry systems , san jose , ca , usa )  . cell apoptosis determination by annexin v assay cells were collected , washed , and resuspended in 100 l annexin v binding buffer . 
fluorescein isothiocyanate - conjugated annexin v and propidium iodide ( invitrogen ) were added to the cells and incubated for 20 mafter incubation , annexin v binding buffer was added , and the cells were analyzed by flow cytometry ( bd biosciences , san jose , ca )  . 
a combined sybr green - based real - time pcr and oligonucleotide ligation assay was used to examine the expression of the mir - 17 polycistron in irradiated oc3 cells . 
mir - 17 - 5p is induced in irradiated oc3 cells and it downregulates p21 protein expression , contributing to the radioresistance of oc3 cells . keywords mir - 17 - 5p radiation oc3 cells p21 radiation tolerance microrna - 17 - 5p reguliert posttranskriptionell die p21 - expression in mit betelnusskauen assoziierten bestrahlten plattenepithelkarzinomzellen zusammenfassung hintergrundundziel . 
nachdem wir herausgefunden hatten , dass microrna - 17 - 5p ( mir - 17 - 5p ) in oc3 - zellen induziert wird , benutzten wir diese zelllinie , um die biologische rolle dieser microrna bei der reaktion auf die ionisierungsstrahlung zu prfen . 
eine kombinierte sybr - green - bezogende real - timepcr und ein oligonukleotid - ligations - assay wurden benutzt , um die expression des mir17 - polycistrons in den oc3 - zellen zu prfen . 
mir - 17 - 5p wird in bestrahlten oc3 - zellen induziert und regelt die mir - 17 - 5p - expression des p21 - proteins herunter , was zur strahlenresistenz der oc3zellen beitrgt . schlsselwrter mir - 17 - 5p strahlung oc3 - zelle p21 strahlentoleranz strahlentherapieundonkologie82013 | mir175p as scramble subg1 g2 / m original article vehicle mir175p as scramble sham rt ( 5gy ) sham 1023 empty 1023 empty sham + mir 175p as rt + mir 175p as 1023 empty 1023 empty mir 175p as fig . 
oc3 cells were pretreated with mir - 17 antisense odn or scrambled odn for 24 h prior to receiving a 5 gy dose of radiation ( rt ) or remaining unirradiated ( sham )  . 
tumor tissues were removed and dehydrated at 4c by increasing gradients of 5 , 10 , and 15% sucrose in pbs followed by immer678 | strahlentherapieundonkologie82013 sion in a mixture of 15% sucrose - pbs and optimum cutting temperature medium ( 1 : 1 ) overnight . 
samples were embedded in paraffin blocks and sectioned . immunohistochemical assay the slides were re - hydrated in pbs for 15 min and the endogenous peroxidase was inhibited by 3% h2o2 / methanol for 10 min at room temperature . 
slides were incubated with anti - human p21 , or for the terminal deoxynucleotidyl transferase dutp nick end labeling ( tunel ) assay ( r&d systems ) , for 16 h at 4c . 
the peroxidase - conjugated secondary antibody was incubated for 1 h at room temperature and slides were developed by immersing them in 0.06% 3 , 3 - diaminobenzidine tetrahydrochloride ( dako ) , followed by counterstaining with gills hematoxylin v . statistical analysis data are presented as mean standard deviation for the indicated number of mice at each time point and in each group . 
oc3 cells were examined for the expression of the mir17 polycistron using a combined sybr green - based real - time pcr and oligonucleotide ligation assay that allows multiple mirnas to be measured simultaneously . 
the results reveal that in oc3 cells , radiation induced the expression of mir17 - 5p in a dose - dependent manner . inhibition of mir - 17 - 5p expression oc3 cells were pretreated with mir - 175p antisense odn or scrambled odn for 24 h prior to sham treatment or treatment with the 5 gy radiation . 
to evaluate cell survival with the clonogenic assay , images and quantitative results of 7 - day colonies , as shown in .fig.2a and b , revealed that the inhibition of mir - 175p expression by mir - 17 - 5p antisense odn , but not by the scrambled odn , significantly reduced colony formation of oc3 cells . 
to evaluate cell apoptosis , oc3 cells were stained 72 h later with the dna - binding dye propidium iodide , and apoptotic cells were identified by flow cytometry as sub - g1 peaks ( cells containing degraded dna )  . 
 these data show that inhibition of mir17 - 5p expression enhanced the radiosensitivity of the oc3 cells . mir - 17 - 5p regulation of p21 protein expression high - level expression of the mir - 17 polycistron is known to promote cell cycle progression by inhibiting the p21 cdki [ 1 ]  . 
to address this question , we treated oc3 cells with or without mir - 17 - 5p antisense odn and varying doses of radiation and prepared cell extracts to examine the expression of the p21 protein by western blotting . 
these data demonstrated that mir - 17 - 5p regulates radiation - induced p21 expression in oc3 cells . role of p21 in enhanced radiosensitivity oc3 cells were treated sequentially with mir - 17 - 5p and p21 antisense odn and then exposed to 5 gy of radiation . 
quantitation of the flow cytometry results revealed that treatment with the p21 antisense odn inhibited the radiosensitivity of the oc3 cells treated with mir - 17 - 5p antisense odn strahlentherapieundonkologie82013 | original article p21as p21s sham rt + p21as rt + p21s with mir175p antisense oligonucleotides treatment subg1 g2 / m with mir175p antisense oligonucleotides treatment fig . 
a oc3 cells were treated with mir - 17 - 5p antisense odn followed by p21 antisense ( p21as ) or sense odn ( p21s ) prior to being irradiated ( 5 gy ; rt ) or remaining unirradiated ( sham )  . 
after 72 h , cells were analyzed for apoptosis and the cell cycle stage was examined by flow cytometry following a annexin v and b propidium iodide staining , respectively . 
on the other hand , as shown in .fig.4b , a propidium iodide staining assay was used to evaluate the cell cycle stage that cells were in and , meanwhile , the sub - g1 peaks could also reveal the presence of apoptosis . 
quantitative results revealed that the p21 antisense odn treatment inhibited the radiosensitivity of the oc3 cells treated with mir - 17 - 5p antisense odn ( .fig.4b : sub - g1 peaks were observed in 18.82.3% of the cells treated with rt alone and in 10.61.5% of the cells treated with p21 antisense odn / rt )  . 
these results demonstrate that p21 plays a critical role in the mechanism by which the inhibition of mir - 17 - 5p expression increases radiosensitivity in oc3 cells . mir - 17 - 5p regulation of p21 expression cells in which mir - 17 - 5p was knocked down were established by transfecting the human pre - microrna 17 expression construct into the oc3 cell line to modulate the expression of mir - 17 - 5p . 
the mir - 17 - 5p knockdown cells and mocktransfected control cells were injected subcutaneously into the right hind legs of immunocompromised severe combined immunodeficient mice to create ectopic xenografts . 
the data show that tumors from animals injected with mir - 17 - 5p antisense odn - expressing oc3 were more sensitive to radiotherapy than tumors derived from mocktransfected oc3 cells . 
tumors weighed 10514 mg in the sham - irradiated + mock - transfected group , 11018.2 mg in the sham - irradiated + mir - 17 - 5p antisense odn - transfected group , 364.5 mg in the irradiated + mocktransfected group , and 10.51.8 mg in the irradiated + mir - 17 - 5p antisense odn - transfected group . 
the anti - apoptotic effect of the mirna 17 - 5p92 cluster has been found in cancer and , in this study , we evaluated the function of the mir - 17 polycistron in irradiated oc3 cells . 
we showed that the expression of mir - 17 - 5p was induced by irradiation and played a role in suppressing apoptosis . as previously described , micrornas may trigger rna degradation and / or repress mrna translation . 
 [ 11 ] found in the primary neuroblastoma , where increased mir - 17 - 5p expression leads to the downregulation of p21 and of the tumor suppressor gene bim ( bcl - 2 interacting mediator of cell death ) , that this strategy represents a novel oncogenic pathway to explain neuroblastoma progression and its resistance to therapy . 
furthermore , antagomir - 17 - 5p downregulated the expression of p21 and bim in neuroblastoma , and this occurred through a mechanism that involved p21 and led to cell - cycle blockade and bim activation of apoptosis , respectively . strahlentherapieundonkologie82013 | original article radiation treatment enhance mir17 - 5p expression mir17 - 5 antisense oligonucleotides down - regulation of p21 enchance expression of p21 enchance radio - sensitivity insensitive to radiation fig . 
6 9schematic representing the critical involvement of mir - 17 - 5p - mediated p21 expression in radiation - induced cell cycle arrest in oc3 cells while studying the mechanism of p21 suppression by the mir - 17 family , wang et al . 
they compared the expression of p21 mrna in the nucleus and the cytoplasm , between stable c - myc transfectants and control cells , and their results reveal that p21 repression by c - myc occurred at the post - transcriptional level . 
to confirm the relationship between c - my and the mir - 17 family and p21 , they antagonized the expression of each mir - 17 family member with their specific antisense oligonucleotides in transfectants constitutively overexpressing c - myc in the presence of c - myc and showed that restoring p21 expression by this treatment was much stronger . 
 [ 13 ] compared animal survival , apoptosis , proliferation , cell cycle progression , dna damage , and regeneration in the crypts of wild type , p53 knockout , puma knockout , p21 knockout , and p21 / puma double knockout mice in a whole body irradiation model in which intestinal damage was induced by radiation . 
the authors found that the deficiency of p53 or p21 led to shortened survival but accelerated crypt regeneration associated with massive nonapoptotic cell death , including aberrant cell cycle progression , persistent dna damage , rampant replication stress , and genome instability . 
 [ 14 ] investigated the radiosensitization effect of mln4924 , which is an scf ( skp1 , cullins , and f - box protein ) e3 ubiquitin ligase substrate inhibitor , and is known to regulate growth arrest , apoptosis , and dna damage response , and they found that it is a potent radiosensitizing target of breast cancer in the sk - br - 3 breast cancer cell lines . 
furthermore , the authors transfected lncap cells with the precursor mir - 106b to investigate the role of mir - 106b , reporting that mir - 106b expression was able to suppress radiation - induced p21 activation and to override the g2 / m arrest in response to radiation ; this resulted in a transient decrease in the radiation - induced growth inhibition . 
in our study , we also transfected oc3 cells with the precursor mir - 17 - 5p to verify the biological role , and our results also showed that g2 / m arrest occurred in response to radiation and resulted in the inhibition of radiation - induced apoptosis . 
in our animal study , the ihc also revealed that p21 expression or apoptosis were clearly detected in tumor tissues within 4 days after radiotherapy rather than 14 days later , when the molecular responses may have passed , potentially indicating that the change of tumor size are the net effect of the radiotherapy . 
clinical trials and mechanistic studies to identify the appropriate radiosensitizer for oral squamous cell carcinoma radiotherapy are critically need in this scientific field [ 16 , 17 , 18 , 19 ]  . 
yang d , tan m , wang g , sun y ( 2012 ) the p21 - dependent radiosensitization of human breast cancer cells by mln4924 , an investigational inhibitor of nedd8 activating enzyme . 
li b , shi xb , nori d et al ( 2011 ) down - regulation of microrna 106b is involved in p21 - mediated cell cycle arrest in response to radiation in prostate cancer cells . 
kuhnt t , klockenbrink u , knipping s et al ( 2011 ) adjuvant low single dose cisplatin - based concurrent radiochemotherapy of oral cavity and oropharynx carcinoma : impact of extracapsular nodal spread on distant metastases . 
staab a , fleischer m , loeffler j et al ( 2011 ) small interfering rna targeting hif - 1alpha reduces hypoxia - dependent transcription and radiosensitizes hypoxic ht 1080 human fibrosarcoma cells in vitro . 
moergel m , meurer p , ingel k et al ( 2011 ) effectiveness of postoperative radiotherapy in patients with small oral and oropharyngeal squamous cell carcinoma and concomitant ipsilateral singular cervical lymph node metastasis ( pn1 ) : a meta - analysis . 
pignon jp , matre a le , maillard e , bourhis j ( 2009 ) meta - analysis of chemotherapy in head and neck cancer ( mach - nc ) : an update on 93 randomised trials and 17 , 346 patients . 
wang jt , palme ce , morgan gj et al ( 2011 ) predictors of outcome in patients with metastatic cutaneous head and neck squamous cell carcinoma involving cervical lymph nodes : improved survival with the addition of adjuvant radiotherapy . 
kreppel m , drebber u , eich ht et al ( 2011 ) combined - modality treatment in advanced oral squamous cell carcinoma : primary surgery followed by adjuvant concomitant radiochemotherapy . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 664667 doi 10.1007 / s00066 - 013 - 0367 - 5 received : 15 april 2013 accepted : 22 april 2013 published online : 7 . 
the present study aimed to create and validate a survival score specifically for patients with brain metastasis from breast cancer . patients and methods in this study , a total of 230 patients who had been treated with wbrt alone for brain metastases from breast cancer were included . 
breast cancer patients represent the second largest group of such patients and have a more favorable survival prognosis than those patients with brain metastasis from other primary tumors [ 5 ]  . 
other common wbrt regimens include 5 fractions of 4 gy over 1 week , 1415 fractions of 2.5 gy over 3 weeks and 20 fractions of 2 gy over 4 weeks . 
patients with a short remaining life time may be candidates for 5 fractions of 4 gy in 1 week in order to keep the overall treatment time as short as possible . 
in contrast , patients with a very favorable prognosis may be better treated with a wbrt regimen with a total dose higher than 30 gy and doses per fraction of < 3 gy . 
these two prognostic factors were included in the scoring systethe score for each factor was determined by dividing the 6 - month survival rate ( in % ) by 10 as shown in .tab.4. 
additionally , the three prognostic groups a , b and c of the test group were compared to the corresponding prognostic groups of the validation group ( 2 test )  . 
the p values were p = 0.98 for the comparison of both groups a , p = 0.99 for the comparison of both groups b , and p = 0.97 for the comparison of both groups c , respectively . discussion the majority of patients with brain metastasis from breast cancer are treated with wbrt alone [ 5 ]  . 
patients with a poor prognosis should receive a short course of wbrt such as 5 fractions of 4 gy over 1 week , which has been strahlentherapieundonkologie82013 | original article abstract zusammenfassung tab . 
4 survival rates 6 months after wbrt and the corresponding scores survivalat6 months ( % ) score karnofskyperformancescore extracranialmetastases suggested in a retrospective study to be similarly effective as the most common wbrt regimen 10 fractions of 3 gy over 2 weeks [ 10 ]  . 
since the risk of developing late toxicities increases with survival time , patients with a more favorable survival prognosis should receive a longer course of wbrt including doses per fraction of < 3 gy . 
furthermore , a retrospective study has suggested that wbrt with total doses beyond 30 gy and doses per fraction < 3 gy result in better intracerebral control and survival than 10 fractions of 3 gy [ 13 ]  . 
the survival scores that are already available for patients with brain metastasis were created in patients with a variety of primary tumors who had received different treatment regimens [ 3 , 8 , 9 ]  . 
according to the results of the multivariate analysis of the test group , karnofsky performance score and extracranial metastases were included in the scoring systethe score for each factor was obtained from the 6 - month survival rate ( in % ) divided by 10 . 
it can be used to estimate the survival time of patients with brain metastasis from breast cancer receiving wbrt alone . keywords brain metastasis whole - brain radiotherapy breast cancer survival prognosis score ein einfacher berlebensscore fr patientinnen mit hirnmetastasen eines mammkarzinoms zusammenfassung hintergrundundziel . 
die 6 - monats - berlebensraten in der testgruppe betrugen 10% bei 47 punkten , 55% bei 9 punkten und 78% bei 12 punkten ( p < 0 , 001 )  . 
ruge mi , kocher m , maarouf m et al ( 2011 ) comparison of stereotactic brachytherapy ( 125 iodine seeds ) with stereotactic radiosurgery ( linac ) for the treatment of singular cerebral metastases . 
vuong da , rades d , eck at van ( 2013 ) comparing the cost - effectiveness of two brain metastasis treatment modalities from a payers perspective : stereotactic radiosurgery versus surgical resection . 
in this study , such a score has been created and validated for patients with brain metastasis from breast cancer , the second most common primary tumor in patients with brain metastasis [ 5 ]  . 
this new score included only two prognostic factors , the kps and presence / absence of extracranial metastases , and , therefore , is easy to use during daily routine . the 6 - month survival rates of the three prognostic groups of this score were quite different . 
patients of group a , who had the worst survival prognosis , may be considered candidates for a short - course wbrt program such as 5 fractions of 4 gy . 
group c patients who had the best survival prognosis would likely benefit from wbrt with total doses beyond 30 gy and doses per fraction of < 3 gy in terms of better treatment outcomes and fewer neurocognitive deficits . 
for patients of the prognostic groups b and c with only very few brain metastases , radiosurgery wbrt or neurosurgery wbrt may also be appropriate [ 1 , 7 , 11 , 12 , 14 , 15 ]  . this new score has been validated in a group of 115 patients . 
the finding that the 6 - month survival rates of the three prognostic groups of both the test group and the validation group were very similar demonstrates that this score is valid and reproducible . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 717718 doi 10.1007 / s00066 - 013 - 0416 - 0 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
20 , d - 65189 wiesbaden , e - mail : prott@bvdst.de eine ausfhrliche wrdigung professor kian angs wird in einer der nchsten ausgaben von strahlentherapie und onkologie erfolgen . michael baumann , dresden , und rolf sauer , erlangen personalia die deutsche gesellschaft fr radioonkologie trauert um professor kian ang die deutsche gesellschaft fr radioonkologie trauert um ihr ehrenmitglied professor kian ang , houston / texas ( usa ) , der am 20 . 
summer workshop image guided and robotic radiotherapy mannheim , 31.8.2013 , 9 14 uhr ort : vorlesungsgebude alte brauerei , universittsmedizin mannheim , rntgenstrae , 68167 mannheim der eintritt ist frei . 
 die themen unconventional imaging in ion beam therapy status and perspectives in - room pet / ct verification of proton therapy quantitative and visual assessment of pet / ct image reconstruction molecular imaging and cancer theranostics the role of dosimetry in therapeutic nuclear medicine nanoparticle transport and interactions in the airways and bloodstream robotic assisted minimally invasive radiotherapy optimal linac target design for contrast enhanced radiotherapy traditional and alternative methods for modeling outcome predictions after stereotactic body radiotherapy for non - small cell lung cancer strahlentherapie und onkologie 8 2013 | mitteilungen der fachgesellschaften jubilare die fachgesellschaften von strahlentherapie und onkologie gratulieren zum geburtstag : 17.08.2013 ldenscheid : lutz ahlemann 70 jahre 07.08.2013 wien : richard ptter 65 jahre 19.08.2013 berlin : ursula rhl 70 jahre 14.08.2013 varel : henry koch 65 jahre 23.08.2013 potsdam : pd karin koch 65 jahre 29.08.2013 freiburg : norbert hodapp 65 jahre 21.08.2013 mainz : peter w . 
the prostate - specific antigen ( psa ) relapse - free survival rates for low - , intermediate - , and high - risk stages are about 8889% , 7886% , and 6367% , respectively [ 17 , 28 ]  . 
furthermore , androgen deprivation is not tolerated well by most patients and it has many side effects , e.g. , insulin resistance and diabetes , bone loss , fatigue , sexual dysfunction ( erectile impotence , loss of libido ) , symptomatic gynecomastia , hot flushes , anemia , and cardiovascular events [ 13 ]  . 
another analysis showed that 68% of patients with local recurrence developed distant metastases compared with 37% of those with no local disease ( p = 0.025 ) [ 9 , 16 ]  . 
these data suggest the importance of an aggressive and effective local therapy for local recurrence without distant metastases after ebrt for selected patients . favorable factors for salvage brachytherapy are histologically confirmed local recurrence , no clinical or radiologic evidence of distant disease , adequate urinary function , age , overall health indicative of > 5to 10 - year life expectancy , prolonged disease - free interval ( > 2 years ) from primary radiation therapy , long prostate - specific antigen ( psa ) doubling time ( > 12 months ) , gleason score < 6 , clinical t1c or t2a tumor status , pretreatment psa velocity < 2.0 ng / ml per year at the time of initial presentation , interval to psa failure > 3 years , and psa < 10 ng / ml at the time of recurrence [ 5 , 21 ]  . in our analysis we could not address all of these factors . 
it should also be briefly mentioned that we had not treated the patients as part of a prospective or randomized study , but based on an internally defined protocol as mentioned below ( see inclusion and exclusion criteria )  . however , we believe that aggressive treatment of locally recurrent prostate cancer is necessary for selected patients . 
 in 2005 , a prospective protocol was initiated at the university hospital erlangen in order to analyze whether salvage pulseddose - rate ( pdr ) brachytherapy as aggressive local therapy for locally recurrent prostate cancer after radiotherapy failure is a well - tolerable and effective salvage therapy . 
for the present report , data from the first 18 patients who were treated according to this protocol were analyzed , using treatment - related late toxicities as the primary endpoint and psa - recurrencefree survival as the secondary endpoint . patients and methods inclusion and exclusion criteria as selection criteria for the protocolbased image - guided salvage pdr brachytherapy , we defined psa - confirmed and pet - ct - confirmed macroscopic local recurrence without progressive metastatic disease , prostate size < 60 ccm , life ex668 | strahlentherapieundonkologie82013 increasing psa favorable risk factors * antihormonal therapy or chemotherapy palliative radiation therapy ultrasoundguided biopsy pet - ct positive negative local positive & n0 & m0 negative local negative / positive & n1 or m1 salvage brachytherapy observation increasing psa fig . 
 * favorable factors for salvage brachytherapy : life expectancy > 5 years , disease - free interval 12 years , recurrence of psa < 10 20 ng / ml , psa doubling time 6 months pectancy more than 5 years , a karnofsky score of 90100% , and good compliance . patient characteristics between march 2005 and march 2011 , 18 patients with local failure after ebrt or ldr brachytherapy underwent a protocol - based ( .fig.1 ) salvage interstitial pdr brachytherapy with ir - 192 . 
 for 6 patients ( 6 / 18 ) , radical prostatectomy was also performed as initial curative treatment option ; for 5 of these patients ebrt was performed after radical prostatectomy for the first recurrence , and in 1 of these patients postoperative ebrt was accomplished owing to positive resection margins . regarding the initial radiation therapy techniques , most of our patients ( 16 / 18 ) were treated first with ebrt only , 1 patient ( 1 / 18 ) was treated with ebrt combined with permanent j - 125 seed brachytherapy , and 1 patient ( 1 / 18 ) had permanent j - 125 seed brachytherapy only as primary radiotherapy . 
the combination with androgen deprivation ( primary treatment or salvage therapy ) was diverse . both the initial and the salvage therapy characteristics of all patients are described in .tab.1. the local recurrences were detected mostly by increased psa level and choline - pet - ct ( 11 patients )  . 
in nearly all patients distant metastases were excluded , with two exceptions : one patient had para - aortal lymph nodes metastases , which were treated curatively with ebrt immediately before the salvage brachytherapy , and another patient had nonprogressive bone metastases , which were treated with androgen deprivation and local irradiation . 
we estimated the maximum dose ( bladder , rectum ) of the primary radiotherapy on the basis of the cumulative dose that was applied . salvage treatment characteristics brachytherapy we have described our treatment technique in detail elsewhere [ 19 ]  . 
the following structures were delineated in all cases : the prostate or in cases after radical prostatectomy the macroscopic tumor mass as well as the rectal wall and the prostatic urethra . we prescribed a total dose of 60 gy divided into two sessions ( 230 gy ) with a time interval between the sessions of strahlentherapieundonkologie82013 | abstract zusammenfassung strahlenther onkol 2013 189 : 668674 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0373 - 7 g.lahmerm.lotters.kreppnerr.fietkauv.strnad protocol - based image - guided salvage brachytherapy . 
eighteen consecutive patients with locally recurrent prostate cancer ( median age , 69 years ) were treated during 20052011 with interstitial pdr brachytherapy ( pdr - bt ) as salvage brachytherapy after radiotherapy failure . 
the treatment schedule was pdr - bt two times with 30 gy ( pulse dose 0.6 gy / h , 24 h per day ) corresponding to a total dose of 60 gy . 
dose volume adaptation was performed with the aim of optimal coverage of the whole prostate ( v100 > 95% ) simultaneously respecting the protocol - based dose volume constraints for the urethra ( d0.1 cc < 130% ) and the rectum ( d2 cc < 5060% ) taking into account the previous radiation therapy . 
the primary endpoint was treatment - related late toxicities particularly proctitis , anal incontinence , cystitis , urinary incontinence , urinary frequency / urgency , and urinary retention according to the common toxicity criteria . 
salvage pdr - brachytherapy of the prostate following local failure after radiation therapy is a treatment option with a low rate of genitourinary side effects and no late gastrointestinal side effects . 
insgesamt 18 patienten ( medianes alter 69 jahre ) mit lokal rezidiviertem prostatakarzinom nach bereits durchgefhrter strahlentherapie wurden im zeitraum von 20052011 mittels interstitieller pdr - brachytherapie ( pdr - bt ) in form einer salvage - brachytherapie behandelt . 
das behandlungsschema bestand aus pdr - bt mit 2 - mal 30 gy ( einzelpulsdosis 0 , 6 gy / h , 24 h pro tag ) bis zu einer gesamtreferenzdosis von 60 gy . 
das bestrahlungsvolumen wurde mit dem ziel einer optimalen volumenabdeckung der gesamten prostata ( v100 > 95% ) bei gleichzeitiger einhaltung der dosis - volumen - restriktionen fr die urethra ( d0 , 1 cc < 130% ) und fr das rektum ( d2 cc < 5060% ) unter beachtung der bereits vorangegangenen strahlentherapie durchgefhrt . 
das lokalrezidiv nach strahlentherapie ( perkutane strahlentherapie , brachytherapie mit jod - 125 - seeds oder kombinationstherapie ) wurde meist mittels cholin - pet - ct und steigendem psa - wert gesichert . 
no other treatment modalities were performed . endpoints patients were followed up for disease - related parameters and adverse side effects every 3 months in the first 2 years , and in 6 - month intervals for the next 3 years . 
we dispensed with detection of erectile dysfunction , because in our experience it is very difficult to obtain truthful information from the patients about erectile dysfunction . overall survival ( os ) and biochemical psa - recurrence - free survival were defined as the period from the date of salvage brachytherapy until the date of death and as the period from the date of salvage brachytherapy until psa increase > 2 ng / ml over nadir ( phoenix definition ) , respectively . 
progression - free survival ( pfs ) was defined as no progression of disease after salvage brachytherapy . statisticalanalysis the data of patients who underwent complete salvage brachytherapy ( see eligibility criteria ) were analyzed . 
kaplanmeier parameters were calculated at 3 years . results dose parameters of salvage brachytherapy the total doses prescribed on the prostate capsule and the d90 were 60 and 63.30 gy ( median ) , respectively . 
one of the 3 patients , who suffered grade 3 urinary incontinence , was treated in the course of the primary radiotherapy with an estimated dose of 196 gy ( combination of ebrt + j - 125 )  . strahlentherapieundonkologie82013 | original article grade5 grade4 0 / 18 0 / 18 tab . 
4 salvage series study , year salvage therapy dianf / u ( months ) urinary grade reten3 / 4toxtion icity 1333% 30% outcome rectal injury urinary incontinence 4332% 215% 4266% n . 
a. 43% pfs 1527% 50% 035% recurrences stephenson et al . , 2004 [ 26 ] heidenreich et al . , 2009 [ 14 ] amling et al . , 1999 rogers et al . , 1995 [ 24 ] grado et al . , 1999 [ 12 ] allen et al . , 2007 [ 3 ] aaronson et al . , 2009 burri et al . , 2010 [ 6 ] 57% psapresent series rfsp f / u follow - up , pfp progression - free probability , psa - rfsp psa - recurrence - free survival probability , pfs progression - free survival , psa - npr psa nonprogression rate , bdfs biochemical disease - free survival , sbt salvage brachytherapy 3324% psa - npr 63% bdfs 88% bdfs 54% bdfs 34% bdfs 017% n . 
no grade 15 side effects occurred . survival and freedom from tumor progression the median follow - up time after salvage brachytherapy was 21 months ( range , 87 months )  . 
one patient died of a heart attack and the other died of pancreatic cancer . six patients developed metastases ; of them , 2 patients were known to have metastasis before salvage brachytherapy , as mentioned above . 
accordingly , the frequency and grade of side effects of salvage prostatectomy or salvage brachytherapy are of utmost importance both for the patient and for the physician in charge . the most frequent toxicity of salvage prostatectomy is urinary incontinencetypically between 29 and 50% [ 22 ]  . 
most reports on salvage prostatectomy show urinary incontinence rates between 18 and 58% [ 4 , 16 , 26 , 28 ] ( see also .tab.4 ) , which are distinctly higher than in our analysis . 
in our analysis , we saw grade 3 urinary incontinence in 2 patients ( 2 / 18 ; 11% ) , in 1 patient grade 3 urinary frequency / urgency ( 1 / 18 ; 5.5% ) , and 3 patients experienced grade 3 urinary retention as a new event ( 3 / 18 ; 17% )  . 
 [ 11 ] , only 1 of 4 potent patients with salvage prostatectomy who underwent bilateral nerve sparing recovered adequate erection function for intercourse , and the 3 - year actuarial recovery of continence was 30% . other parameters regarding side effects in these studies are perioperative complications and rectal injuries . 
one reason for the low rectal injuries can be that there is a learning curve effect for the implantation of the brachytherapy implant , which caused a lower radiation dose at the rectal wall and therefore led to the low rate of rectal injuries [ 18 ]  . 
if the physician has expert knowledge in brachytherapy for prostate cancer , we believe that he should also be an expert in salvage brachytherapy , because the technical implementation is in principle the same . 
we can state that we have treated more than 400 patients with brachytherapy for prostate cancer in our department from 2000 to 2012 , and the data from first 130 patients have already been published [ 19 ]  . regarding perioperative complications , different grades were reported by 927% patients treated with salvage prostatectomy [ 10 , 14 , 26 , 27 ]  . 
it is self - explanatory that time - consuming surgery like salvage prostatectomy will be indicated in such cases with restraint . regarding the efficacy of salvage therapy , only a limited comparison of salvage prostatectomy and salvage brachytherapy is possible . 
in our patients , only 4 of 18 ( 22% ) developed metastases after brachytherapy1 of them immediately at 2 months after salvage brachytherapy and a second patient at 8 months after salvage brachytherapy . 
 [ 7 ] , the biochemical recurrence - free survival was 48% and the metastasis - free and cancer - specific survival rates after salvage radical prostatectomy were 77 and 83% after 10 years , respectively . 
heidenreich a , richter s , thuer d , pfister d ( 2010 ) prognostic parameters , complications , and oncologic and functional outcome of salvage radical prostatectomy for locally recurrent prostate cancer after 21st - century radiotherapy . 
le fur e , malhaire jp , baverez et al ( 2012 ) impact of learning curve and technical changes on dosimetry in low - dose brachytherapy for prostate cancer . 
lettmaier s , lotter m , kreppner s ( 2012 ) long term results of a prospective dose escalation phase - ii trial : interstitial pulsed - dose - rate brachytherapy as boost for intermediateand high - risk prostate cancer . 
nguyen pl , damico av , lee ak , suh ww ( 2007 ) patient selection , cancer control , and complications after salvage local therapy for postradiation prostate - specific antigen failure : a systematic review of the literature . 
paparel p , soulie m , mongiat - artus p et al ( 2010 ) salvage radical prostatectomy after external radiotherapy for prostate cancer : indications , morbidity and results . 
stephenson aj , scardino pt , bianco fj jr et al ( 2004 ) morbidity and functional outcomes of salvage radical prostatectomy for locally recurrent prostate cancer after radiation therapy . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 982983 doi 10.1007 / s00066 - 013 - 0448 - 5 online publiziert : 3 . 
seit publikation der ukcccrund der eortc - studien [ 2 , 3 ] mitte der 90er jahre des vorigen jahrhunderts , die beide die definitive radiotherapie ( rt ) mit der mitomycin / fu - basierten radiochemotherapie ( rct ) verglichen , stellt letztere die standardbehandlung des analkarzinoms dar . 
insgesamt wurden 940 patienten eingeschlossen , nmlich 472 patienten fr die rct mit mitomycin c / fu ; davon erhielten 246 eine erhaltungschemotherapie mit cisplatin / fu , 222 dagegen keine erhaltungschemotherapie . 
nach einer medianen nachbeobachtungszeit von 5 jahren betrug die komplette remissionsrate nach 26 wochen 90 , 5 % in der mitomycin - crct - gruppe und 89 , 6 % in der cisplatin - rct - gruppe ( p = 0 , 64 )  . 
die rct mit 5 - fu und mitomycin c zusammen mit 28 fraktionen zu 1 , 8 gy ( gesamtdosis 50 , 4 gy ) sollte der behandlungsstandard des analkarzinoms bleiben . kommentar warum immer nur negative studien zu cisplatin / fu ? die erste studie ( rtog 8911 ) , welche die frage nach einer etwaigen verbesserung der krankheitsfreien berlebensrate durch eine rct mit cisplatin / fu stellte [ 1 ] , war noch mit dem makel behaftet , eine unangemessen lange behandlungszeit zu haben , nicht zuletzt infolge einer obligaten induktionschemotherapie . 
so waren seinerzeit die ergebnisse nach rct mit cisplatin / fu im vergleich zur standard - rct tatschlich noch schlechter : das krankheitsfreie berleben und das gesamtberleben blieben mit 58% vs . 
die hier zu diskutierende act - ii - studie scheint , obgleich nicht als quivalenzstudie ausgelegt , am ehesten die gleichwertigkeit beider regime fr den endpunkt komplette remission nach 6 monaten zu zeigen . 
die resultate dieser studie gelten nmlich nur dann als valide , wenn es keinerlei interaktion zwischen den vergleichsgruppen der radiochemotherapie und der erhaltungschemotherapie gibt , fr mich , als mit der statistik nicht so versierter mediziner , unverstndlich . berraschend gut sind die absoluten progressionsfreien berlebensraten nach 3 jahren in dieser studie mit knapp 75% , zumal die autoren angeben , dass berwiegend nichtspezialisierte institutionen zur patientenrekrutierung beitrugen und daher mithin von einem unselektionierten patientengut auszugehen sei . 
die franzsische accord - 03 - studie , welche ausschlielich ein cisplatin / fu - basiertes rct - regime mit und ohne induktionschemotherapie untersuchte , kann im intensivierten arm mit 45 gy plus 2025 gy boost ( allerdings nach 3 wochen pause ) nicht mit einem besseren resultat aufwarten [ 7 ]  . gibt es dennoch problempatienten , die von einer intensivierung der behandlung profitieren knnten ? die autoren geben an , dass patienten mit t3und t4 - tumoren und solche mit nodalem befall in dieser studie mit 63% eine deutlich schlechtere 3 - jahres - berlebensrate aufwiesen ; dies werfe wiederum ( nach auffassung der britischen gruppe ) die fragen der induktionschemotherapie mit taxanen , einer intensivierung der radiotherapie oder auch der integration bio logischer medikamente , gemeint sind egfr - antikrper , auf . 
 nach unseren eigenen erfahrungen [ 4 ] sind insbesondere patienten mit greren perianalen hautkarzinomen im vergleich zum hufig kleineren analkanalkarzinom risikopatienten : hier war die krankheitsfreie berlebensrate nach der standard - rct mit 54% vs . 
die atzelsberg - studiengruppe , die sich mit der klinisch - wissenschaftlichen definition der regionalen tiefenhyperthermie beschftigt , wird demnchst eine studie zur intensivierung der rct des analkarzinoms durch komplementren einsatz der tiefenhyperthermie ffnen . fazit f standardbehandlungdesanalkarzinomsbleibtdiemitomycin / fu - basierteradiochemotherapie . f diestrahlenbehandlungsollhierbeibis50 , 4gy1 , 8gyerfolgen , und zwarohneunterbrechung . f beikontraindikationenfrmitomycinckannimeinzelfalleinecisplatin / fu - basiertercterwogenwerden . f diederzeitigeevidenzlagespricht klargegenjedwedeinduktions - und erhaltungschemotherapie . gerhard grabenbauer , coburg korrespondenzadresse prof.dr.g.g.grabenbauer klinik fr strahlentherapie und radioonkologie , klinikum coburg ketschendorfer str . 
ajani ja , winter ka , gunderson ll et al ( 2008 ) fluorouracil , mitomycin , and radiotherapy vs fluorouracil , cisplatin , and radiotherapy for carcinoma of the anal canal : a randomized controlled trial . 
 o a ( 1996 ) epidermoid anal cancer : results from the ukcccr randomised trial of radiotherapy alone versus radiotherapy , 5 - fluorouracil , and mito mycukcccr anal cancer trial working party . 
flam m , john m , pajak tf et al ( 1996 ) role of mitomycin in combination with fluorouracil and radiotherapy , and of salvage chemoradiation in the definitive nonsurgical treatment of epidermoid carcinoma of the anal canal : results of a phase iii randomized intergroup study . 
grabenbauer gg , kessler h , matzel ke et al ( 2005 ) tumor site predicts outcome after radiochemotherapy in squamous - cell carcinoma of the anal region : long - term results of 101 patients . 
cbct provides three - dimensional ( 3d ) information of the scanned region and provides soft tissue images with good spatial resolution , both potentially increasing the geometric accuracy of radiotherapy delivery [ 7 , 8 , 9 , 10 ]  . 
however , it is also a more complex and time - consuming imaging modality and the additional radiation exposure might increase the risk of secondary cancer [ 11 ]  . due to the absence of distinct anatomical features in breast tissue , the cbct to planning ct alignment mainly relies on the breast contours , chest wall and , if present , surgical clips . 
in this respect , a previous study demonstrated the breast contours on cbct image sets , acquired with the clinically standard settings , to be affected by multiple artefacts [ 12 ]  . 
lowering the cbct tube current and exposure time eliminated this artefact . however , one of the limitations of the above - mentioned study was the absence of a bowtie filter [ 12 ]  . 
 another limitation was the use of polystyrene phantoms , as the described artefacts strongly depend on patient geometry . in this study , the contour accuracy investigation is expanded to cbct imaging with bowtie filtration . 
additionally , absorbed dose measurements were performed for all investigated protocols . materials and methods planning ct and cbct images were acquired for both prone and supine anthropomorphic phantoms and a female cadaver in supine and prone set - up . 
the female cadaver , on the other hand , served as a clinically relevant model . in this study , a thiel cadaver was used since the thiel embalming technique authentically preserves the different tissue layers ( skin , subcutaneous fat and collagen tissue , fascia , muscular , visceral and glandular tissue ) and keeps the complete range - of - motion of all joints intact , allowing for a precise setup ( arrangement ) of the bodys posture in accordance with the corresponding clinical treatment position [ 15 , 16 ]  . 
an extensive description of the prone and supine thoracic phantoms ( polystyrol 495f , basf , germany , = 1.02 g / cm3 ) has already been published [ 12 ]  . 
supine cadavthe first two authors contributed equally to the design and writing of the manuscript . strahlentherapieundonkologie112013 | original article er set - up was supported by a supine arm support tool ( civco medical solutions , orange city , ia , usa )  . 
image acquisition was performed for the left breast in all cases . helical planning ct images of the phantoms and the cadaver were acquired on a toshiba aquillion ct scanner ( toshiba medical systems , tokyo , japan ) with a slice thickness of 2 mm , a tube potential of 120 kvp and a tube current of 150 ma . 
 image reconstruction in the accompanying xvi software ( version 4.5. ) is based on the feldkampdaviskress ( fdk ) conebeam algorithan accurate set - up of the phantoms and cadaver was obtained by aligning the planning ct surface markings with the treatment room lasers . multiple cbct protocols with varying mas , range of projection views and starting angle were studied . 
as the maximum range of projection views amounted to only 205 , all protocols employed a small field of view ( fov ) with a reconstruction diameter of 270 mpreliminary research demonstrated extremely poor image quality using a medium fov ( reconstruction diameter 410 mm ) for a limited range of projection views . 
as the medium fov set - up is obtained by asymmetrically collimating the beam and shifting the detector panel in the corresponding direction , each projection view only partly 946 | strahlentherapieundonkologie112013 samples the reconstructed fov . 
this evaluation was only performed for cbct protocols using tube current and exposure time of 20 ma and 32 ms . for all protocols , the conformity of planning ct and cbct breast contours was visually inspected on the phantom and cadaver images in the xvi viewing and registration software ( version 4.5 , elekta , crawley , west - sussex , uk )  . 
as in clinical practice , all images were visualized using the soft window settings . computed tomography dose index ( ctdi ) measurements were performed to estimate the influence of various cbct acquisition settings ( field of view , tube current and exposure time and angular range of projection views ) on patient radiation dose . 
measurements were performed using an unfors xi platinum ct detector ( 100 mm long pencil beam ctionization chamber , type 146358 , unfors instruments ab , billdal , sweden ) in a cylindrical ctdi phantom ( pmma , diameter 32 cm , length 15 cm )  . 
in order to provide scattered dose along the complete cbct field width , the phantoms length was increased by adding at least 15 cm of polystyrene slabs ( polystyrol 495f , basf , germany , = 1.02 g / cm3 ) at the phantoms superior and inferior side . 
ctdi measurements were performed at the center and four equally distributed peripheral positions in the phantom ( at 0 , 90 , 180 and 270 , distance to the center 10 cm )  . 
the weighted ctdi ( ctdiw ) was then computed as ( elekta : xvi r4.5 ) : in order to investigate the need for patient offset positioning , the frequency of this intervention was compared between the old full - rotation protocol and a 205 - rotation protocol . 
to that purpose , 558 205 - cbcts ( 37 patients ; 13 prone and 24 supine ) and 1272 360 - cbcts ( 102 patients ; 13 prone and 89 supine ) were included . 
prone and supine cbct phantom and cadaver images acquired with a tube current and exposure time of 40 ma and 40 ms , demonstrated an important periareolar tissue deficit ( .fig.1a , marked with dotted lines )  . 
as in the previous study , these cbct contour inaccuracies were completely eliminated by lowering the tube current and exposure time to 20 ma and 32 ms ( .fig.1b , marked with dotted lines )  . 
the cranio - caudal tissue excesses , as detected in the previous phantom study , were still apparent in the polystyrene phantoms , but were hardly detectable in the female cadaver images . secondly , the influence of a further reduction in range of projection views and the x - ray source starting angle was investigated for cbct protocols using a tube current and exposure time of 20 ma and 32 ms respectively . 
 consequently , the concomitant reduction in range of projection views strongly reduces the measured ctdiw : for a tube current and exposure time of 20 ma and 32 ms , the ctdiw of a 205 - s20 protocol amounted to only 66.3% of the full - rotation m20 acquisition . 
prone and supine breast cbct images acquired with a bowtie filter , a small fov , a range of projection views equaling 180 , a tube current of 20 ma and an exposure time of 32 ms , demonstrated adequate contour accuracy and an elimination of the offset cbct isocenter procedure , while this occurred in 40.7% for the old full - rotation protocol . 
the established 180 protocol demonstrated acceptable contour accuracy , eliminated the cbct isocenter offset procedure and reduced patient radiation exposure . keywords contour perception phantom imaging cadaver bowtie filtration computed tomography dose index ( ctdiw ) verbesserte cone - beam - computertomographie fr die radiotherapie der brust in rckenund bauchlage . 
die mit einem bowtie - filter , kleinem fov , einer 180 - rotation , 20 ma rhrenstrom und einer belichtungszeit von 32 ms erhaltenen cbct - bilder in bauchund rckenlage gewhrleisteten eine adquate konturgenauigkeit und vermeiden eine cbct in isozentrumsposition , die bei 40 , 7% in den alten vollrotationsprotokollen erforderlich war . 
das 180 - protokoll zeigt eine akzeptable konturierungsgenauigkeit , vermeidet cbct in isozentrum - position und reduziert die strahlenbelastung fr die patientin . schlsselwrter konturwahrnehmung phantom kadaver bowtie - filter computed - tomography - doseindex ( ctdiw ) strahlentherapieundonkologie112013 | original article fig . 
combination of a 180 rotation , use of small fov , 20 ma , 32 ms , with use of bowtie filter results in a 4.3 - fold dose reduction in ctdiw compared with the preset chest m20 protocol . the frequency of offset patient positioning amounted to 40.7% for the old full - rotation protocol , while this procedure was completely eliminated for the 205180 - rotation protocols . discussion in contrast to the previously studied protocols [ 12 ] , the investigated protocols now involve a bowtie filter , a small fov and a maximum range of projection views of 205 . 
clinical implementation of the half - rotation rotation cbct ( for 558 acquisitions ) did not reveal any relevant clinical differences compared to our test findings . moreover , our results clearly show thateven when using a bowtie filter that has been described to reduce panel saturation effects [ 13 ] attention regard948 | strahlentherapieundonkologie112013 ing these artefacts and their effect on contour accuracy is required . 
adoption of the preset tube current and exposure time for cbct imaging with bowtie filtration , only available for a medium fov , resulted in an important periareolar tissue deficit in both prone and supine breast imaging with a small fov . 
the presence of these artefacts in the cadaver images clearly demonstrate the significance of panel saturation artefacts in a clinically relevant setas in the previous study [ 12 ] , the phantom images still suffered from craniocaudal tissue excesses . 
these tissue excesses were ascribed to errors inherent to the fdk - based reconstruction algorithm and are most pronounced for flat object edges parallel to the imaging module rotation plane [ 17 ]  . 
overall , the thiel embalmed cadaver generally served as a clinically relevant phantom for cbct acquisition : both clips , soft and hard tissue features were clearly visible and strongly resembled real patient geometry and composition . 
the only limitation was the seeping of embalmment fluid into the cadaver lungs , resulting in a denser region near the chest wall on both the cbct and planning ct images . additionally , the use of a small fov has an important impact on patient radiation dose . 
 while the transition from a medium to a small fov for a given protocol resulted in a slight increase in ctdiw , lowering the range of projection views from 360 to 205180 allowed for a more important ctdiw reduction . note , however , that the concept of ctdiw was originally developed for reporting doses from ct acquisitions , representtions using a limited range of projection views obviously do not preserve this axial symmetry . 
the absorbed dose throughout the imaged volume will strongly depend on the location of the narrower entrance beams and the wider but attenuated exit beam , especially in the volumes periphery [ 19 ]  . 
nevertheless , the application of the ctdi concept in this paper was only used to provide a direct comparison between the investigated protocols , rather than quantifying absorbed doses for comparison with other imaging modules . 
to that purpose , a more elaborate investigation of the spatial distribution of radiation dose to the patient is required . furthermore , the use of a bowtie filter in the investigated protocols has been described to strongly reduce radiation dose to the patient [ 13 ]  . 
this effect was found to be the most important in the peripheral regions of the scanned object , but was not investigated in this study . an additional benefit of the use of a limited range of projection views is the avoidance of the offset procedure . 
the cadaver images settings comprised a tube current and exposure time of 20 ma32 ms and a range of projection views of 200 ( i ) , 180 ( ii ) , 160 ( iii ) and 140 ( iv ) ing the integral dose of a single ct slice [ 18 ]  . 
these measurements are generally performed by integrating the dose measured in a 100 mm - long ionization chamber , a technique that has also been adopted for cbct by amer et al . 
they showed that this approach results in a conservative overestimate of the weighted dose across the complete fov , representing an estimate of the dose in the central 100 mm of the fov [ 19 ]  . 
de crop a , bacher k , van hoof t et al ( 2012 ) correlation of contrast - detail analysis and clinical image quality assessment in chest radiography with a human cadaver study . 
amer a , marchant t , sykes j et al ( 2007 ) imaging doses from the elekta synergy x - ray cone beam ct systebrit j radiol 80 : 476482 original article tab . 
the first protocol corresponds to the preset chest m20 protocol meaning medium field of view ( m20 ) filtration fieldofview tubecurrent ( ma ) exposure time ( ms ) ctdiw ( mgy ) aelekta synergy xvi version 4.5. 
the authors would like to thank klaus bacher , ph.d. , and liesbeth eloot , m.sc. , from the department of medical physics and radiation protection at ghent university for providing the tools and assistance for the ctdi measurements . compliance with ethical guidelines conflict of interest . 
 hormonal overproduction and its specific symptoms generally lead to diagnosis of functioning pituitary adenomas . surgical resection is the widely accepted initial treatment for both functioning and nonfunctioning pituitary adenomas , except prolactinomas , which generally respond to medical therapy . 
as nfpas lack signs of hormonal overproduction they tend to be detected at larger sizes and tumor regrowth after surgical resection occurs quite often in this subgroup of patients [ 1 , 2 ]  . 
despite excellent longterm tumor control rates ( well above 90% in many studies ) , reports about complications have resulted in controversy about radiotherapy indications and techniques [ 4 , 7 ]  . 932 | strahlentherapieundonkologie112013 stereotactic radiotherapy techniques , allowing higher dose conformity and sparing of normal tissue , might help overcome the long - term toxicity concerns of conventional radiotherapy . 
single fraction stereotactic radiotherapy , applied as gamma knife radiosurgery or with a modified linear accelerator , has been reported in the management of patients with nfpas but also for hormone - secreting tumors [ 8 , 9 , 10 ]  . 
however , stereotactic radiosurgery ( srs ) is usually offered to selected patients , whereas fractionated stereotactic radiotherapy ( fsrt [ 11 ] ) can be applied irrespective of tumor size or proximity to the optic apparatus . despite advances in microsurgical techniques , recurrent disease or incomplete resection of large lesions are still of concern . 
excellent long - term tumor control can be achieved by using stereotactic radiotherapy immediately after surgery for large or residual pituitary adenomas or in a delayed setting for recurrent disease [ 12 , 13 , 14 , 15 , 16 ]  . the aim of the present study was to evaluate the role of fsrt in the management of nonfunctioning and functioning pituitary adenomas in the postoperative setting , with respect to disease control and side effects of radiotherapy . patients and methods patients we report on 37 consecutive patients , 19 male , 18 female , with a median age of 56 years ( range 1475 years ) with pituitary adenomas treated at the first authors institution . 
three adenomas were classified as adrenocorticotropic - hormone - secreting ( acth ) , 3 as growth - hormone - secreting ( gh ) and 2 were macroprolactinomas . all patients had previously undergone surgery and presented with residual ( 20 patients ) or recurrent disease ( 17 patients )  . 
another patient underwent 4 transsphenoidal operations and one osteoplastic craniotomy , resulting in 5 surgical interventions prior to fsrt . the mean follow - up time was 49 months , median 57 months ( range 2111 months )  . 
1 clinical features of the patients gender female male median age ( years ) histologic type non - functioning acth - secreting sth - secreting macroprolactinomas radiotherapy used for recurrence or progression after surgery residual disease after subtotal resection 18 ( 49% ) 19 ( 51% ) 56 ( range 1475 ) 29 ( 78.4% ) 3 ( 8.1% ) 3 ( 8.1% ) 2 ( 5.4% ) 17 ( 46% ) 20 ( 54% ) treatment planning for treatment planning and radiation delivery an individual thermoplastic head mask ( brainlab ) was modeled for each patient , allowing a positioning accuracy of 0.51.0 mthis mask was attached to a stereotactic localization system on the base of the frame ( brainlab ) to obtain contrast - enhanced computed tomography ( ct ) scans at a slice thickness of 1.52 min addition , gadolinium - enhanced t1 - weighted magnetic resonance imaging ( mri ) with 1.52 mm slices in the axial plane was acquired . 
the co - registration of the mri scans to the planning ct was achieved using a mutual information algoriththe planning target volume ( ptv ) and organs at risk were defined on each slice of a three - dimensional data cube using the treatment planning system brainscan ( brainlab )  . 
the data presented in this study represent the time points before starting radiotherapy and after completion of radiotherapy ( last follow - up visit )  . diagnostic radiology reports , starting with initiation of radiotherapy and during follow - up were analyzed for all patients . 
 patients were reported as being in partial remission , if there was any tumor shrinkage , as stable disease , if there was no tumor shrinkage and progression if there was any tumor growth . 
in order to definitely assess response to therapy we routinely analyzed all diagnostic images ourselves and compared them to the images we initially acquired for treatment planning . results fsrt was well tolerated by all patients and could be completed without interruption . 
 no acute toxicities were observed during fsrt , except for one single case of transient dizziness , headaches reported by 8 patients , and mild sleepiness reported by 5 patients ( all grade 12 )  . 
no serious late toxicity , such as brain necrosis , bleeding , stroke , or radiation - induced tumor was reported . radiological response local tumor control was defined as lack of radiological progression on follow - up gadolinium - enhanced t1 - weighted mri . 
before fsrt partial hypopituitarism was present in 41% of patients , while 35% had anterior panhypopituitarisafter fsrt pituitary function remained normal in 22% , 43% had partial pituitary dysfunction , and 35% had anterior panhypopituitarisvisual acuity was stable in 76% of patients , improved in 19% , and deteriorated in 5% . 
good local tumor control and preservation of adjacent structures can be reached , even for large tumors . keywords pituitary neoplasms fractionated stereotactic radiotherapy non - functioning treatment outcome fraktionierte stereotaktische strahlentherapie in der behandlung von hypophysenadenomen zusammenfassung zielsetzung . 
two years after fsrt he had clinical signs of tumor progression resulting in surgical intervention with decompression of the optic chiasm , because of consecutive visual field impairment , consisting of bitemporal hemianopsia . 
this patient additionally developed partial pituitary insufficiency due to tumor regrowth and consecutive pituitary stalk compression . two other patients with signs of radiological progression , one with intraand suprasellar tumor growth , the second one with involvement of the cavernous sinus , needed radiosurgical salvage treatment . 
one of them had been treated to a total dose of 50.4 gy in 28 fractions and showed initially radiological partial remission until he had signs of tumor regrowth 4 years after fsrt . 
he was then treated by cyberknife radiosurgery in another institution , another 2 years later he had again signs of radiological progression and received cyberknife treatment for a second time at the same institution . 
additionally he recurred radiologically 2 years after fsrt and received cyberknife radiosurgery in another institution but died shortly thereafter . one patient died 4 years after fsrt , at the age of 76 years , cause of death being unrelated to her nfpa , another patient died 2 years after fsrt for nfpa , as a consequence of newly diagnosed glioblastoma at the age of 77 years ( probably the interval is too short to define this tumor as clearly radiation - induced )  . 
during the follow - up ( 1.5 years after fsrt ) , he had been clinically stable with regard to both pituitary and visual function and showed signs of radiological tumor regression . 
another patient with an acth - producing adenoma died 6 months after fsrt as a result of pulmonary embolism . 934 | strahlentherapieundonkologie112013 before fsrt after fsrt 35% 35% 5% 5% number of involved anterior pituitary axis fig . 
1 9 percentages of patients according to the number of involved anterior pituitary axis ( from no involvement to 4 axes ) before and after fsrt ( last follow - up visit ) visual acuity left eye before fsrt visual acuity left eye after fsrt visual acuity right eye before fsrt visual acuity right eye after fsrt fig . 
2 8 visual acuity in absolute numbers , accordingly to the left and right eyes before and after fsrt ( last follow - up visit ) functional response three of the 8 patients ( 38% ) with functioning pituitary adenomas showed complete normalization of hormonal overproduction after a median follow - up of 3 months ( range 024 months ) , one acth - , one gh - secreting and one prolactinoma . 
one of these patients experienced endocrinological and radiological recurrence of disease 4 years after fsrt leading to cyberknife treatment . a reduction of hormonal overproduction was observed in 1 patient with a sthproducing adenoma . 
this patient experienced endocrinological recurrence of disease 1.5 years after fsrt , which could be treated successfully with a gh - receptor antagonist . anterior pituitary function before fsrt , 9 ( 24% , 5 residual tumor , 4 progression after surgery ) patients had normal anterior pituitary function and 15 patients ( 41% , 8 residual tumor , 7 progression ) had evidence of decreased pituitary function , ranging from involvement of one single anterior pituitary hormonal axis to three involved axes , needing hormonal substitution . 
mostly these patients had involvement of thyrotroph and corticotroph pituitary axes , the exact numbers of patients with involvement of one or more anterior pituitary axis , resulting from compression of pituitary stalk by the adenoma are listed in .fig.1. 
after fsrt pituitary function remained normal in 8 patients ( 22% , 4 residual , 4 progression ) , 16 patients ( 43% , 9 residual , 7 progression ) had partial dysfunction of the anterior pituitary gland , 35% ( 13 / 37 , 7 residual , 6 progression ) had complete anterior hypopituitarism . before fsrt , 3 patients with nfpa had elevated prolactin levels . 
no new occurrence of hyperprolactinemia was registered after fsrt . visual acuity after fsrt visual acuity remained stable in 28 / 37 patients ( 76% , 16 residual , 12 progression ) , showed improvement in 7 / 37 ( 19% , 2 residual , 5 progression ) and deteriorated in 2 / 37 ( 5% , 2 residual )  . 
after fsrt visual fields remained stable in 35 patients ( 94.6% , 19 residual , 16 progression ) , improved in 1 patient ( 2.7% , progression after surgery ) and worsened in 1 patient with tumor progression ( 2.7% , residual tumor after surgery )  . discussion pituitary adenomas account for approximately 14% of all intracranial tumors and among them nfpa are the most common type of pituitary neoplasas they lack signs of hormonal overproduction , nfpas generally become evident with symptoms of compression of adjacent structures , such as pituitary stalk , optic nerves , and chiastherefore , being generally asymptomatic at smaller sizes , they often become clinically evident after considerable growth leading to hypopituitarism and / or visual field impairment . 
in the present series , we report on 29 patients with nfpa and 8 patients with functioning pituitary adenomas treated with fsrt for residual or recurrent disease . when it comes to radiotherapy , different application techniques have been used in the past , ranging from conventional fractionated radiotherapy to highly precise stereotactic techniques . 
still , the use of single fraction has been reported to be associated with potential neurologic toxicity to the optic apparatus and normal brain tissue [ 17 , 18 ]  . 
in order to minimize these toxicities the application of srs is generally restricted in current practice to small pituitary adenomas , not located in direct proximity to the optic nerves or chiasfor pituitary adenomas with supra and parasellar involvement and for tumors involving the cavernous sinus , fsrt seems a suitable treatment option , potentially overcoming the limitations of srs . 
the tumor control rate of 91.9% achieved in the present series of patients compares well with these figures . radiation - induced pituitary deficiency requiring hormonal replacement is one of the main toxicities of concern . 
following srs , hypopituitarism has been reported in a similar range of 041% at a variable median follow - up of 660 months [ 8 , 19 , 20 , 21 ]  . 
in our study , hypopituitarism rates remained mostly unaffected by fsrt : 41% of patients had evidence of decreased pituitary function before radiotherapy , ranging from involvement of one single anterior pituitary hormonal axis to three involved axes , needing hormonal substitution . 
after fsrt , 43% of patients had evidence of partial hypopituitarism , meaning that only a single patient with normal pituitary function before fsrt needed hormonal replacement therapy following fsrt . 
the percentage of patients with anterior panhypopituitarism before and at a median follow - up of 57 months after fsrt was constant at 35% in our series . late effects of stereotactic radiotherapy of pituitary adenomas include reduction of visual acuity and visual field defects [ 22 ]  . 
with respect to visual acuity , we found it stable in 76% of patients , while 19% showed improvement and 5% some deterioration during follow - up . when looking at the patients that underwent immediate radiation therapy after incomplete resection and those who received radiation therapy upon progression , we found a tumor control rate of 90% for the patients with incomplete resection vs . 
interestingly the authors state that of 338 patients with surgical intervention only 11 had complete tumor excision [ 5 ]  . regarding endocrinological and visual function , we found no striking difference between both cohorts . 
milker - zabel s , debus j , thilmann c et al ( 2001 ) fractionated stereotactically guided radiotherapy and radiosurgery in the treatment of functional and non - functional adenomas of the pituitary gland . 
starke rm , williams bj , jane ja jr et al ( 2012 ) gamma knife surgery for patients with nonfunctioning pituitary macroadenomas : predictors of tumor control , neurological deficits , and hypopituitaris j neurosurg 117 : 129135 22 . 
rieken s , habermehl d , welzel t et al ( 2013 ) long term toxicity and prognostic factors of radiation therapy for secreting and non - secreting pituitary adenomas . 
radiat oncol 8 : 18 ation therapy after incomplete resection is necessary . we indicated early postoperative radiotherapy in cases where the residual tumor was located nearby critical neurological structures , like optical pathways , leading to neurological deficits . 
even if patients had not yet developed neurological deficits , we treated them in the attempt to prevent it from happening , knowing that neurological deficits in this area could have a serious impact on the quality of live and are often not reversible . 
the risk for endocrinological and visual side effects seems to us comparable for both cohorts , although we are aware of the biometrical shortcoming of the present analy sis . the commonly prescribed dose of 50.4 gy in this series seems to lead to high tumor control rates and at the same time few side effects . 
we systematically analyzed pituitary function before fsrt and during follow - up separately for all hypothalamicpituitary axes with respect to the need of hormone substitution therapy , visual acuity for each eye separately , and humphrey visual fields . 
grosu state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . literaturkommentiert strahlenther onkol 2013 189 : 984986 doi 10.1007 / s00066 - 013 - 0446 - 7 online publiziert : 10 . 
oktober 2013 springer - verlag berlin heidelberg 2013 c.weiss klinik fr strahlentherapie und onkologie , johann wolfgang goethe universitt , frankfurt / main vorhersagelokoregionrerrezidive nachradikalerblasenentfernung vonurothelkarzinomen eineneuerisikostratifikation originalbeitrag baumann bc , guzzo tj , he j et al ( 2013 ) a nov el risk stratification to predict local - regional failures in urothelial carcinoma of the bladder after radical cystectomy . 
fr das urothelkarzinom der harnblase existieren nur wenig be lastbare daten hinsichtlich der lokore gionren rezidivrate nach radikaler zyst ektomie einschlielich pelviner lymph adenektomie , unabhngig von einer zu stzlichen neoadjuvanten oder adju vanten chemotherapie . 
daher untersuchten die autoren der hier zu kommentierenden arbeit [ 1 ] an hand von an der universitt von pennsyl vania zystektomierten patienten verschie dene faktoren , die ein erhhtes risiko fr lokalrezidive vorhersagen knnten . 
ziel war es , auf diese weise patienten zu iden tifizieren , die fr eine studie zur adjuvan ten strahlentherapie nach oder vor zyst ektomie geeignet wren . licher computer oder magnetresonanz tomographie ( ct / mrt ) des beckens . 
in der univariaten analy se erwiesen sich das pathologische tu morstadium t3 , < 10 entfernte lymph knoten , positive resektionsrnder , befal lene lymphknoten , ein nierenstau , eine lymphgefinvasion und eine gemisch te histologie als signifikant fr die vor hersage eines lokoregionren rezidivs . 
die patienten konnten dann in 3 gruppen mit deutlich unterschiedlichem lokalrezidiv risiko aufgeteilt werden : niedriges risi ko ( t2 ) , mittleres risiko ( t3 und 10 entfernte lymphknoten ) und hohes risi ko ( t3 und < 10 entfernte lymphkno ten ) die entsprechenden rezidivraten nach 5 jahren betrugen lokal 8 , 23 bzw . 
baumann bc , guzzo tj , he j et al ( 2013 ) a novel risk stratification to predict local - regional failures in urothelial carcinoma of the bladder after radical cystectomy . 
griffiths g , hall r , sylvester r et al ( 2011 ) international phase iii trial assessing neoadjuvant cisplatin , methotrexate , and vinblastine chemotherapy for muscle - invasive bladder cancer : long - term results of the ba06 30894 trial . 
volkmer bg , kuefer r , bartsch gc jr et al ( 2009 ) oncological followup after radical cystectomy for bladder cancer - is there any benefit ? j urol 181 : 15871593 ( discussion 93 ) 8 . 
weiss c , sauer r , rdel c ( 2012 ) stellenwert der radiochemotherapie beim harnblasenkarzino onkologe 18 : 10031011 logygroup8710 und intergroup0080 studie zur neoadjuvanten chemotherapie bei muskelinvasiven harnblasenkarzino men ergab hinsichtlich der chirurgischen einflussfaktoren , dass immerhin 33% der patienten mit tumoren pt34 noch posi tive resektionsrnder nach zystektomie aufwiesen . 
 eine groe deutsche serie aus ulm mit 1270 engmaschig , auch bildgebend nach verfolgten patienten nach zystektomie be richtet eine gesamtrezidivrate von 38 , 3% nach 5 jahren und ber 44% nach 10 jah ren , aber verteilt ber alle tumorstadien . 
auch erfolgte kei ne differenzierte analyse nach tumorsta dium und resektionsstatus , so dass eine abschlieende beurteilung des lokalrezi divrisikos nicht mglich ist . die hier vorgestellte studie der univer sitt von pennsylvania zeichnet nun durch ihr prospektives bildgebendes nachsorge programm ein verlsslicheres bild des tat schlichen lokoregionren rezidivrisikos [ 1 ]  . 
nach univariater und multivariater analyse verschiedens ter patienten und tumorbezogener para meter erwies sich schlussendlich eine zu ordnung in drei risikogruppen als sinn voll : eine gruppe ( alle patienten pt2 ) mit einem niedrigen lokalrezidivrisiko von 8% nach 5 jahren , eine gruppe ( al le patienten pt3 und 10 lymphkno ten entfernt ) mit einem mittleren lokal rezidivrisiko von 23% und eine hoch risikogruppe ( alle patienten pt3 und < 10 lymphknoten entfernt ) mit einem lokalrezidivrisiko von 42% . 
da zwei gro e randomisierte studien keinen einfluss auf die lokalrezidivrate durch eine neoad juvante chemotherapie zeigten [ 3 , 4 ] , stel len die autoren die berechtigte frage nach einer intensivierung der lokalen therapie , z . 
die hier vorgestellte risikostratifizie rung kann dabei der besseren patienten selektion dienen . zustzlich soll hier noch eine weite re arbeit derselben autorengruppe an gesprochen werden , die sich dem vertei lungsmuster von lokalrezidiven in der selben studienpopulation widmet [ 2 ]  . 
 aus dieser analyse geht hervor , dass das hchste lokoregionre rezidivrisiko fr patienten mit tumoren pt3 und tu morfreien chirurgischen resektionsrn dern in den iliakalen und obturatorischen lymphknotengruppen liegt , whrend fr tumoren pt3 und positiven chirurgi schen resektionsrndern zustzlich das ehemalige blasenbett und die prsakralen lymphknotengruppen ein erhhtes risi ko tragen . 
krperliche symptome , fatigue , belkeit , schmerzen , fertilitt , kognition , delir , suizidalitt , sowie seelisches leid . besprochen werden praxisrelevante einflussfaktoren auf die krankheitsverarbeitung und krankheitsbewltigung und der stellenwert der psychologischen faktoren in der patientenversorgung . 
im stepped care - ansatz , ist wirkungsvoll in der durchfhrung von psychoonkologisch - psychotherapeutischen interventionen . die psychoonkologie ist ein obligater bestandteil einer krebsbehandlung , gleichzusetzen mit anderen therapieelementen wie chemooder radiotherapien und operationen . 
 von ihnen werden 80% geheilt ; sind sie aber auch gesund ? insbesondere der bereich posttraumatische belastungsstrung / somatoforme strungen bedarf in zukunft einer hheren aufmerksamkeit : die diagnose krebs mit der folge einer uerst invasiven onkologischen behandlung , wird von den betroffenen und deren familien nicht nur als schwere belastung mit der folge von verhaltensund anpassungsstrungen erfahren , sondern sehr hufig als existentielle bedrohung erlebt und deshalb traumatisch verarbeitet . 
wird der traumatische hintergrund dieser strungen nicht gesehen , werden nicht verarbeitete traumatische erfahrungen immer wieder angetriggert , retraumatisieren die patienten , verstrken psychische strungen und verhindern eine angemessene krankheitsbewltigung und damit integration der chronischen erkrankung in das selbstkonzept . 
die nichtbehandlung dieser ptbs behindert nicht nur gravierend eine adquate krankheitsbewltigung , sondern fhrt langfristig als sptfolge zu komorbiden erkrankungen wie angststrung , depression , somatoformen dissoziativen strungen , suchterkrankungen und essstrungen . viele nebenwirkungen einer krebstherapie sind erforscht und werden in der nachsorge bercksichtigt . 
langer ( erlangen ) short communication strahlenther onkol 2013 189 : 967971 doi 10.1007 / s00066 - 013 - 0428 - 9 received : 30 april 2013 accepted : 18 july 2013 published online : 10 . 
oktober 2013 springer - verlag berlin heidelberg 2013 p.faracem.a.deiddai.iamundodecurtise.deianar.farigug.lays.porru department of radio - oncology , regional oncological hospital , cagliari bi - tangentialhybridimrt forsparingtheshoulderin wholebreastirradiation considerable morbidity still arises due to effects on normal tissues of treatments for breast cancer . 
even if the reduced risk for local recurrence seems to outweigh the risk for long - term effects for most women [ 1 ] , a substantial proportion of them reported moderate or marked arm and shoulder symptoms . 
these symptoms were largely present in the patient treated by breast conservative therapy , even if they were found to suffer less frequently from this complication than patients treated with mastectomy [ 2 ]  . 
the combination of axillary lymph node ( aln ) dissection and axillary radiation increases the risk of seroma , infection and lymphedema , whereas shoulder symptoms include pain , stiffness and difficulty in raising or moving arm sideways . 
breast cancer surgery and radiotherapy may cause persistent pain in the breast area , arm and shoulder as reported by 3050% of patients after 35 years , lymphedema in 1525% of patients , and restrictions of arm and shoulder movement in 35% [ 4 ]  . these symptoms were significantly associated with the use of breast radiation , as well as with axillary dissection and younger age [ 5 ]  . 
they exhibited significantly reduced range of motion for all movements compared with the non - operated side , but in contrast only flexion was significantly reduced in the non - irradiated patients [ 7 ]  . 
the same pattern was evident for shoulder strength : in irradiated patients all movements except external rotation were significantly reduced , whereas non - irradiated patients exhibited a significant reduction for flexion and abduction , but other movements were less affected [ 7 ]  . in many cases , conventional wholebreast irradiation produces unnecessary and undesirable irradiation of normal tissue . 
in fact , it is well known that standard tangential fields partially include the axilla [ 8 , 9 , 10 , 11 ] , and , as a consequence , they also partially include the shoulder . in the present technical article , we retrospectively analysed 6 patients affected by shoulder pain and reduced functional capacity after conventional whole breast irradiation . 
we analyze the geometrical reason which produced the undesired dose to the shoulder from standard tangential irradiation in the supine position and propose a new bi - tangential technique which would have been able to significantly reduce this dose . materials and methods a total of 6 patients ( 5 right and 1 left sided ) treated for early ( stage iiia ) breast cancer and successively affected by shoulder symptoms were retrospectively analyzed . 
all patients were treated in the supine position by a standard plan using hybrid intensity - modulated radiotherapy ( imrt ) , prescribing 50 gy in 25 fractions to the whole breast , plus a 10 gy electron boost . a breast clinical target volume ( ctv ) was defined to include the whole mammary gland . 
a breast planning target volume ( ptv ) was defined as the ctv plus a margin of 1.0 cm in any direction , with the constraint that the ptv did not extend outside the body contour . 
to assess the dose to the shoulder and axilla , the shoulder muscles ( latissimum dorsi , subscapularis , teres major , teres minor , serratus anterior ) and the axillary level iii lymph node volume were identified , considering only the portion which traversed the open tangential beams . 
the pectoralis major and minor were neglected , since they were almost completely included in the ptv . to retrospectively evaluate the differences in dose distribution with respect to the standard plan used for the treatment , two additional bi - tangential plans were generated . 
the second beam covered the superior portion ( from the isocentre ) , but it was rotated by a 1020 angle with respect to the standard lateral beain the second plan ( double bi - tangential ) , both the lateral and the medial open beams were split as described above . 
the optimal lateral tangential beam ( dashed lines ) in the middle - to - lower portion of the breast ( a ) was split into two beams at isocentre ( b ) , where the edges of the lateral rotated beam were also shown ( continuous lines )  . 
in the upper breast section ( c ) this beam entrance ( continuous lines ) allowed the shoulder to be avoided , which would have been included in the un - rotated beam ( pointed lines )  . 
in the upper breast section , the dose obtained by the standard plan ( d ) to the portion of muscle ( thick black lines ) and axilla ( thin black lines ) , which traversed the standard tangential beams were reduced by applying the single ( e ) and the double ( f ) bi - tangential techniques . 
after proper weighting of these beams ( maximum target coverage avoiding any 107% hot spot , as in [ 12 ] ) , hybrid imrt was performed by applying two additional imrt segments . 
inverse planning was optimized with the following objectives / constraints : pov uniform dose = 50 gy ; pov uniformity > 3% . the following parameters ( and units ) were used to evaluate plan quality : ptv95% ( percentage of volume of ptv receiving more than 95% of the prescribed dose ) , ctv95% and pov95% . 
the considered shoulder muscles and the axillary level iii lymph nodes were assessed by measuring the volume which traversed the open tangential beams , the corresponding mean dose and the volume receiving more than 45 gy . 
for each parameter comparison between the standard and the two bi - tangential plans , statistical significance was calculated by paired t - test . results the geometrical and the dosimetric advantages of the bi - tangential techniques are exemplified in .fig.2. 
the standard tangential plan used for treatment was compared with ( 1 ) a single bi - tangential plan where , to spare the shoulder , the lateral open tangent was split into two half - beams at isocentre , with the superior portion rotated by 1020 medially with respect to the standard lateral beam ; ( 2 ) a double bi - tangential plan , where both the tangential open beams were split . 
this simple technique is valuable for irradiation after axillary lymph node dissection or in patients without dissection due to negative or low - volume sentinel lymph node disease . keywords planning techniques intensity - modulated radiotherapy axilla lymph nodes breast neoplasms bitangentiale hybrid - imrt zur schonung der schulter bei ganzbrustbestrahlung zusammenfassung hintergrundundziel . 
der zur bestrahlung verwendete tangentiale standardbehandlungsplan wurde verglichen : ( 1 ) mit einem einzel - bitangentialen plan , wobei zur schonung der schulter die laterale tangente in zwei felder im isozentrum mittels halfbeam - technik aufgeteilt wurde . 
ptv95% der standardplne ( 91 , 93 , 8 ) zeigten keine signifikanten unterschiede im vergleich zu einzel - bitangentialen plnen ( 91 , 83 , 4 ) ; eine kleine , aber signifikante ( p < 0 , 01 ) abnahme wurde mit dem doppel - bitangentialen plan ( 90 , 13 , 7 ) beobachtet . 
diese einfache technik ist geeignet fr bestrahlungen nach axillrer lymphknotensektion oder aber auch fr patienten , fr die keine sektion vorgenommen wurde , da die sentinellymphknoten nur gering oder gar nicht beeintrchtigt sind . schlsselwrter planungstechnik intensittsmodulierte strahlentherapie axilla lymphknoten brustneoplasien strahlentherapieundonkologie112013 | short communication fig . 
even if lymphedema negatively affects quality of life [ 13 , 14 ] , it has been reported that poor physical quality of life was strongly associated with reduced shoulder abduction rather than with lymphedema [ 15 ]  . 
 there is sufficient evidence of late effects of aln dissection or radiotherapy postbreast cancer to warrant careful attention to shoulder function across time in individuals who have had breast cancer [ 16 ]  . 
a number of studies on women treated for breast cancer have shown limitations in glenohumeral range of movement and a recent report has shown decreased muscle activity in four key muscles ( serratus anterior , upper trapezius , pectoralis major and rhomboid ) acting on the scapula [ 17 ]  . 
the normal biomechanics of the shoulder complex is altered and the muscles affected in the long term and associated with pain and disability can be outside the direct field of surgery or radiotherapy . 
furthermore , for a structure to be considered affected by radiation fibrosis syndrome , it must be either within the radiation fields or have tendons or neurovascular innervation that traverse the field [ 19 ]  . 
single bi - tangential was obtained by splitting only the lateral beams , and could be preferred to double bi - tangential , obtained by splitting both the medial and the lateral beams . 
neuromuscolar and musculoskeletal complication can be observed even in patients typically treated by 30 36 gy , as reported in long - term hodgking lypmphoma survivors [ 19 ]  . 
on the other hand , the effect of doses below / around 20 gy is not fully understood , but they might be not related to shoulder complications . treatment planning was the main core procedure for physicists and required the longest working time for this occupational group during radiotherapy for breast cancer patients . 
some caution has to be used in the patients who omit aln dissection and underwent sentinel lymph node ( sln ) dissection alone , as recently proposed both with metastatic [ 20 ] and negative [ 21 ] sln disease . 
since full nodal irradiation should be considered in the case of positive sln disease [ 22 ] , the bi - tangential technique must be discouraged , as it significantly reduced the dose to level iii lymph nodes . 
however , regional control was high in patients who had low - volume sln disease who did not undergo axillary dissection , regardless of whether the axilla was irradiated [ 23 ]  . 
norman sa , localio ar , potashnik sl et al ( 2009 ) lymphedema in breast cancer survivors : incidence , degree , time course , treatment , and symptoms . 
deutsch m , land s , begovic m , sharif s ( 2008 ) the incidence of arm edema in women with breast cancer randomized on the national surgical adjuvant breast and bowel project study b - 04 to radical mastectomy versus total mastectomy and radiotherapy versus total mastectomy alone . 
nesvold il , foss sd , holm i et al ( 2010 ) arm / shoulder problems in breast cancer survivors are associated with reduced health and poorer physical quality of life . 
giuliano ae , hunt kk , ballman kv et al ( 2011 ) axillary dissection vs no axillary dissection in women with invasive breast cancer and sentinel node metastasis : a randomized clinical trial . 
setton j , cody h , tan l et al ( 2012 ) radiation field design and regional control in sentinel lymph node - positive breast cancer patients with omission of axillary dissection . 
porru state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 987987 doi 10.1007 / s00066 - 013 - 0416 - 0 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
younger age , high karnofsky performance score ( kps ) , higher surgical extent , additional adjuvant treatments and methylguanine dna methyltransferase ( mgmt ) methylation are associated with better outcome [ 9 , 11 , 21 ]  . surgery followed by rt with concomitant and adjuvant temozolomide ( tmz ) based chemotherapy ( ch ) has become the standard of care for newly diagnosed gbm [ 2 , 26 ]  . 
in a randomized trial conducted by the european organization for research and treatment of cancer ( eortc ) and the national cancer institute of canada ( ncic ) , stupp et al . 
the rationale for combined rttmz treatment is based on preclinical data suggesting a synergistic activity that increases the number of radiation - induced double - strand dna breaks and subsequent apoptosis [ 28 ]  . the expression of mgmt ( the dna repair enzyme that removes the cytotoxic o6 - guanine adducts produced by alkylating agents ) mediates resistance to tmz [ 11 ]  . 
the interactions between rt and tmz , which may have important implications for treatment schedules and the development of strategies to improve outcome , remain unclear [ 7 ]  . the relative contribution of concomitant and adjuvant tmz to survival is currently not well defined and no randomized studies exist in the literature to shed light on this issue . 
for this reason , we evaluated toxicity and outcome in two prospective phase ii studies for patients with gbm in which a nonstandard concomitant tmz schedule was used , and compared these with the eortcncic trial . materials and methods eligibility patients over 18 years of age with newly diagnosed and histologically proven gbm ( who grade iv ) ; kps > 70 ; wbc count > 3.510 3 / ul ; platelet count > 150103 / ul ; bilirubin and creatinine levels less than 1.5 times the upper limit of normal and aspartate aminotransferase , alanine aminotransferase and alkaline phosphatase levels < 2.5 times the upper normal limit were eligible for enrolment in the studies . 
dexamethasone ( 24 mg ) was administered daily during rt . chemotherapy tmz at a daily dose of 75 mg / m2 , 5 days a week ( excluding saturday and sunday ) was used concomitantly to rt . 
after a 4 - week break beginning at the end of rt , patients received adjuvant tmz ( 150 200 mg / m2 / day for 5 days every 28 days ) for 612 cycles according to negative or positive mri images . no prophylactic therapy for pneumocystis carinii was used . 
antiemetics including hydroxytryptamine 3 antagonists and anticonvulsants were administered as required . surveillance and follow - up the baseline examination included postoperative gadolinium mri studies , complete blood counts and blood chemical examination . 
gadolinium mri was performed before adjuvant tmz , every three cycles during ch , every 2 months after completion of treatment for the first 2 years and every 3 months thereafter . 
our data support the hypothesis that adjuvant tmz is more important than concomitant chemotherapy ( ch ) and that rt is the more important element of the concomitant treatment schedule . keywords outcome radiotherapy chemotherapy survival toxicity gleichzeitige und adjuvante temozolomid - basierte chemoradiotherapie zur glioblastombehandlung . 
die mediane progressionsfreie berlebenszeit ( pfs ) betrug 9 monate , das gesamtberleben ( os ) lag bei 16 monaten , ohne dass sich ein signifikanter unterschied zwischen den beiden gruppen ergab ( jeweils p = 0 , 5 und p = 0 , 14 )  . 
influence of rpa class , extent of surgery , age ( < 70 and 70 years ) and duration of concomitant tmz on os and pfs was evaluated using a univariate logrank test . 
all calculations were performed using the statistical analysis software package ( spss ) version 13 ( spss inc . , chicago , il , usa )  . results patient characteristics from october 2000 to june 2008 , 104 patients with histologically confirmed gbm diagnoses were treated at our institution : 25 patients ( 24.1% ) were enrolled in rt - tmz - 10.00 and 79 ( 75.9% ) in rttmz - 01.04. 
only 2 / 104 patients ( both in the rt - tmz - 01.04 group ) did not complete rt ; 1 patient owing to acute g4 toxicity and the other patient due to pulmonary embolisadjuvant tmz was completed by 68.3% of patients ( 57 patients received six cycles of tmz and 14 patients more than six ) and interrupted in 33 patients ( 31.7% ; due to disease progression in 22 cases and toxic effects in 11 )  . toxicity concomitant rt plus tmz was well tolerated : only 1 patient discontinued treatment at the rt dose of 52.2 gy due to prolonged thrombocytopenia . 
in the univariate analysis only rpa class correlated with pfs ( p = 0.02 ) , while in multivariate analysis no covariate independently influenced pfs . overall survival all patients in the rt - tmz - 10.00 study group had died by the time of this analysis . 
meta - analysis of ch in patients with high grade gliomas treated with nitrosoureabased chemotherapeutic regimens found a modest survival benefit ( 610% at 1 year ) [ 23 ]  . 
in 2005 , the eortcncic phase iii trial compared rt alone versus rt plus concurrent and adjuvant tmz in patients with newly diagnosed high grade gliomas [ 26 ]  . 
the reasons for discontinuation were disease progression or toxic effects in 35.9% of these patients [ 26 ]  . after the eortcncic trial , several small trials were published confirming the beneficial effect of tmz when given concomitantly during rt [ 16 , 17 ]  . the relative contributions of the concomitant and the adjuvant ch cannot be assessed . 
published a study in which concomitant tmz was prescribed at 50 mg / m2 in 123 patients ( group a ) and at 75 mg / m2 in 37 patients ( group b )  . 
29% at 2 years , respectively ( p = 0.31 ) [ 8 ]  . it is unclear how tmz and rt interact at any level ; whether or not tmz acts as radiosensitizer and which schedules are better for patients . 
tmz is more effective when administered at least 72 h before rt and a high dose of tmz appears to have a greater radiosensitizing potential and be able to interact with rt at earlier time points [ 7 ]  . 
4 uniand multivariate analysis according to prognostic factors and treatment schedules a methylated mgmt promoter have improved pfs and os . original article variable p - value log - ranktest < 70 vs . 
on this basis , we analyzed two prospective phase ii studies for patients with gbm , which combine nonstandard concomitant tmz with rt . the first study started before the stupps data were known . 
at that time , many diseases were treated by rt and concurrent ch at our institution [ 18 , 27 ] and we thus planned the phase ii study with concomitant tmz during the first and last weeks of rt [ 5 ]  . the second study started subsequently . 
considering the lack of data concerning the contribution of concomitant and adjuvant tmz , this study was based on the hypothesis that concomitant tmz , if administered only during 5 days of rt , would achieve the same outcome with less toxicity . 
eligibility criteria and the interval between surgery and the start of rt were the same as for the first study , as reported in .tab.3. treatment was completed as planned by 98% of patients ; only 1 patient prematurely discontinued chemoradiotherapy due to tmz toxic effects . 
however , this conclusion requires further confirmation due to the small sample size and study type . another limitation of our study is the absence of an mgmt test , which was not available at our institution until 3 years ago . 
valentini state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . original article strahlenther onkol 2013 189 : 957966 doi 10.1007 / s00066 - 013 - 0372 - 8 received : 28 february 2013 accepted : 29 april 2013 published online : 23 . 
despite significant advancements in treatment results , overall survival has remained relatively constant for over two decades and continues to be particularly poor for non - resectable tumors and advanced metastatic disease [ 3 , 5 ]  . 
to broaden the therapeutic window , novel approaches are under investigation to selectively augment radiation effects in tumor cells while sparing the surrounding tissue [ 7 , 16 , 23 ]  . 
histone deacetylase inhibitiors ( hdaci ) are epigenetic modulators , which affect different biological processes like cell growth , apoptosis , dna repair , and terminal differentiation [ 10 ]  . 
it is postulated that hdaci may facilitate chromatin relaxation by shifting the balance towards histone acetylation hence increasing dna accessibility for dna - damaging agents [ 11 , 28 , 30 ]  . 
in several in vitro and in vivo experimental models , hdaci have been shown to act as radiosensitizers in a variety of human tumors including gliomas , colorectal carcinomas , and melanoma [ 14 , 15 , 27 ]  . the clinical development of these novel anticancer drugs has been rapid but fundamental questions about the mechanism of anticancer activity and the potential of hdaci as radiosensitizers are still not answered in detail . we have recently reported that the hdaci saha , a potent inhibitor of class i and ii histone deacetylases enhances radiation effects in cultured os cells [ 6 ]  . 
we now sought to take the next step in preclinical development of this treatment concept by analyzing the effect of hdaci on the response of osteosarcoma to radiotherapy in vivo . 
 together , these data suggest the potential of a novel therapeutic strategy for treatment of osteosarcoma . material and methods cells and reagents the khos - 24os and saos2 human os cell lines are derived from human osteosarcomas and were purchased from the american type culture collection ( rockville , md , usa ) and maintained in complete culture medium ( mccoy ) supplemented with 10% fcs ( khos - 24os ) and 15% fcs ( saos2 ) , respectively . 
the khos - 24os cell line contains a single p53 allele with a rare arg to pro mutation at codon 156 ( r156p ) possibly increasing the half life of the protethe somatic rate of r156p is less than 2% and germ rate is zero . 
in the saos - 2 cell line , both p53 alleles are deleted [ 31 ]  . saha was obtained from alexis biochemicals ( lrrach , germany ) , dmso from carl roth biochemicals ( karlsruhe , germany )  . 
two osteosarcoma cell - lines ( khos - 24os , saos2 ) were treated with irradiation ( xrt ) alone or xrt and suberoylanilide hydroxamic acid ( saha )  . 
monolayers were stained with 0.5% crystal violet for 10 mplates were fixed with 0.1 m sodium citrate ( ph 4 ) in ethanol 100% ( 3 : 1 ) for another 10 mafterwards , plates were dried for 4872 h and colonies were counted visually . 
survival was defined as the ability of cells to form colonies ( 50 cells )  . animal model human khos - 24os tumor xenografts were established by subcutaneous ( s.c. ) inoculation of tumor fragments ( diameter 12 mm ) into the hind limbs of 10 - week old scid mice ( cb17 / icr - prkdcscid / icrcrl , charles river , wilmington , ma , usa )  . 
 the mice were maintained under specific pathogen - free conditions ; food and water were available ad libiduhousing and all procedures involving the mice were performed according to the protocols approved by the local responsible government department ( regierungsprsidium karlsruhe , germany )  . when tumors reached 100 mm3 , mice were randomly assigned to one of four treatment groups : vehicle ( dmso ) control ( 23 animals ) , saha alone ( 20 animals ) , radiation alone ( 23 animals ) , or combined saha and radiation ( 20 animals )  . 
saha 100 mg / kg was solubilized in dmso ( 99.5% ) , given intraperitoneally ( i.p. ) , started 24 h before radiation and applied for 5 days a week , 3 weeks in series . 
the radiotherapy dose was selected from the preliminary doseresponse studies in this model ( supplemental .fig.1 ) and was intended to find an intermediate dose range to best detect potential effects of hdaci . 
tumor length ( l ) and width ( w ) were measured and tumor volume calculated ( lw2 / 2 , where l = longest diameter and w = shortest diameter )  . 
animals were euthanized by co2 inhalation followed by cervical dislocation either when tumors reached a volume of 3.0 cm3 , or after severe necrosis had developed , or when the study termination time point 45 days after treatment start had been reached . tumor tissue analysis histochemistry / immunohistochemistry was performed in three tumors per treatment group at the following time points : 24 h , 8 days , 23 days and 45 days after xrt . whole tumor sections ( 3 m thick ) were cut from formalin - fixed , paraffinembedded ( ffpe ) tissue blocks . 
clonogenic survival of human os cell lines as well as tumor growth delay of os xenografts were tested after treatment with either vehicle , radiotherapy ( xrt ) , saha , or xrt and saha . 
hdaci thus emerge as potentially useful treatment components of os . keywords osteosarcoma radiotherapy histone deacetylase inhibition suberoylanilide hydroxamic acid cd95 radiosensitivierung durch histon - deacetylasehemmung im osteosarkom - mausmodell zusammenfassung zielsetzung . 
die autoren sind daher der meinung , dass hdaci eine potenziell wirksame therapiestrategie beim os darstellt . schlsselwrter osteosarkom radiotherapie histon - deacetylasehemmung suberoylanilide hydroxamic acid ( saha ) cd95 areas . 
 apoptosis was detected by an in situ terminal deoxynucleotidyl transferase dutp nick end labeling ( tunel ) based kit , apoptag ( s7100 ; chemicon / millipore , temecula , ca , usa ) according to the manufacturers instructions . 
for further statistical analysis the means for every tumor and treatment group were calculated , respectively . further expression analysis was performed by generating tissue microarrays ( tma ) comprising tumor spots from all xenografts using an automated microarrayer ( beecher instruments )  . 
for immunohistochemical analysis of p21 and p53 expression , the following primary antibodies were employed : rabbit monoclonal anti - p21 ( 1 : 100 , ph 9 , abcam , cambridge , uk ) ; anti - p53 ( 1 : 100 , ph 9 , dako , hamburg , germany )  . 
tumor growth dynamic : a relative and b absolute tumor volumes after treatment with dmso ( control group , 23 animals ) , saha ( 20 animals ) , irradiation ( xrt , 23 animals ) or saha plus xrt ( 20 animals )  . 
the combination of xrt and saha led to a significant tumor growth inhibition as compared to xrt alone from day 23 on ( pd23 = 0.001 , pd31 = 0.001 , pd45 = 0.03 ) ous to xrt . 
cells and medium were harvested 24 , 48 , and 72 h after xrt , centrifuged ( 800g ) , and the cell pellet stained for cd95 , cd95 ligand , and apoptosis analysis as follows : fitc - anti - human cd95 ( biolegend , ca , usa ) or anti - human - cd95 ligand ( bd pharmingen , nj , usa ) were added and incubated on ice for 20 mfor simultaneous detection of apoptotic cells , propidium iodide and dapi were added . 
data are presented either as mean or as median , error estimation was performed by calculation of the standard error of mean ( sem )  . results to examine potential radiosensitizing effects of saha , clonogenic survival was performed in two different osteosarcoma cell lines . 
tumor proliferation as determined by ki - 67 staining was significantly reduced in tumors after all treatments ( except for saha monotherapy on day 8 ) as compared to vehicle treated controls . 
a tumor morphology ( hematoxylineosin , h&e ) , proliferation ( immunhistochemical ki67 staining ) and microvessel density ( cd34 staining ) in osteosarcoma xenografts treated with dmso ( control ) , suberoylanilide hydroxamic acid ( saha ) , irradiation ( xrt ) or saha plus xrt . 
b the combination treatment led to a significantly ( * ) lower median proliferation rate compared to xrt only ( ki - 67 : day 8 p = 0.045 , day 23 p = 0.017 , day 45 p = 0.038 ) and number of microvessels ( cd34 : day 8 p = 0.016 , day 23 p = 0.003 , day 45 p = 0.028 ) beyond day 8 of therapy . 
tumor necrosis showed a trend towards significance after treatment with xrt and saha but did not reach statistical significance at all points of time tal models [ 13 , 25 ]  . 
tumors treated with saha alone or with combined saha and xrt treatment showed elevated apoptosis rates as compared to the control group or the xrt group from day 8 on . 
comparison of irradiated tumors with tumors treated with saha and xrt revealed a significant increase of apoptosis in the combination group at all time points . because p53 plays a key role in the regulation of apoptotic cell death in response to ionizing radiation , chemotherapy , and possibly also hdaci [ 39 ] , we evaluated the expression of p53 and p21waf1 / cip1 by immunohistochemistry . 
a immunohistochemical staining for apoptosis ( tunel ) , p53 , and p21waf1 / cip1 expression in osteosarcoma xenografts treated with dmso ( control ) , suberoylanilide hydroxamic acid ( saha ) , irradiation ( xrt ) or saha plus xrt . 
apoptosis ( tunel , a ) , cd95 receptor ( b ) and cd95 ligand ( c ) were measured by flow cytometry 24 , 48 , and 72 h after irradiation ( xrt )  . 
p53 expression was significantly induced by saha only and saha plus xrt compared to the controls and the xrt treated tumors . the role of cd95 receptor / ligand system in saha induced apoptosis previous reports postulated a key role for cd95 receptor / ligand system apoptosis induced by hdaci and other anticancer agents [ 22 , 26 ]  . 
to investigate the involvement of the cd95 receptor / ligand system in the hdaci - mediated apoptosis expression of cd95 , cd95l , the activation of downstream caspases ( 3 and 8 ) as well as functional studies with cd95 neutralizing antibody were performed in two os cell lines ( khos - 24os , saos2 )  . 
to confirm the functional involvement of the cd95r / l system in the induction of apoptosis in os cells , the effect of either agonistic recombinant cd95l and / or neutralizing anticd95 antibody on apoptosis induction was investigated . 
in addition , caspase 8 activation was used as surrogate for the ligand induced apoptosis and activation of the executing caspase 3 / 7 was measured to detect the overall extent of apoptosis . 
to confirm that suberoylanilide hydroxamic acid ( saha ) mediates apoptosis by activation of the cd95 gene , os cells were either incubated with recombinant cd95 ligand ( rcd95 ligand ) or with neutralizing antibody ( nok - 1 ) and treated with either a dmso ( untreated control ) , b xrt only , c saha only , or d xrt + saha . 
in solid tumors , the full therapeutic potential of hdaci is likely to be achieved when they are combined with other treatment modalities such as radiation [ 8 , 33 , 35 ]  . 
saha is one of the well - established hdaci and has been shown to act as a radiosensitizer in vitro and in vivo in different tumor entities [ 6 , 7 , 14 , 15 , 27 , 29 ]  . as an important novel finding reported here , saha exerts radiosensitizing effects in os in vivo . 
our data clearly show beneficial effects of this combination regimen , i.e. , enhanced antiangiogenic , anti - proliferative , and pro - apoptotic effects translating in significant tumor growth delay as compared to both monotherapies with either saha or xrt alone . 
moreover , addition of radiotherapy does not increase normal tissue toxicity in our experimental model and the animals suffered only from known gastrointestinal side effects attributed to saha therapy , which was reversible after therapy cessation . the significant reduction in the number of microvessels as well as the higher rates of necrosis in tumors treated with combined xrt + saha vs . 
each monotherapy found here is consistent with previous data reporting that hdaci elicit antiangiogenic effects via down - regulation of key proteins involved in the angiogenesis process like hypoxia - inducible factor1 ( hif - 1 ) and its targets vascular endothelial growth factor ( vegf ) , vegf receptor - 1 and - 2 , and cxc chemokine receptor 4 ( cxcr4 ) [ 13 , 24 ]  . induction of apoptosis by hdaci has been reported as one major mechanism but the pathways by which hdaci facilitate programmed cell deathparticularly in osteosarcomaare unknown . 
we observed a significantly higher rate of apoptosis in tumors after combination therapy compared to tumors after irradiation only , confirming our previous results in cultured osteosarcoma cells , which documented that saha treatment results in radiosensitizing effects as well as findings from other groups in different tumor entities [ 15 , 17 , 29 ]  . next , we hypothesized that enhanced apoptosis observed after saha may result from p53 / p21 induced activation of the cd95 systethis assumption was based on recent data reporting inhibition of deacetylation of important apoptosis regulators by hdaci including the tumor suppressor gene p53 [ 20 ]  . 
p53 is one of the most commonly altered transcription factors in cancer and plays a pivotal role in the cellular response to dna - damaging agents [ 36 ]  . 
 a number of studies demonstrate activation of p53 in cells after exposure to hdaci and the ability of hdaci to enhance radiation response in cancer cells through increase of p53 acetylationphosphorylation [ 9 , 21 , 39 ]  . 
moreover , p21 expression is directly linked to several key regulatory processes such as cell cycle control , dna - damage response ( ddr ) , cell senescence , and apoptosis . 
based 964 | strahlentherapieundonkologie112013 original article on these observations , we postulate that hdaci induced activation of the cd95 / cd95 ligand plays a key role in anti - tumor / radiosensitizing properties of saha . in support of our hypothesis , saha potently induced the expression of cd95 receptor and cd95 ligand correlating with enhanced caspase 8 mediated apoptosis of os cells . 
this study was supported by the german krebshilfe ( deutsche krebshilfe , 109665 and max - eder 108876 ) , the german federal ministry of research and technology ( bundesministerium fr bildung und forschung ; bmbf 03nuk004a / c ) and the dietmar hopp stiftung . 
furthermore , we would like to thank ludmilla frick , sylvia trinh , claudia rittmueller , gabriele becker , alexandra tietz , angela funk , and andreas griesbach for their excellent technical assistance . original article strahlenther onkol 2013 189 : 951956 doi 10.1007 / s00066 - 013 - 0427 - x received : 1 may 2013 accepted : 18 july 2013 published online : 4 . 
september 2013 springer - verlag berlin heidelberg 2013 nowadays , vaginal vault brachytherapy ( vbt ) is the post - hysterectomy adjuvant treatment of choice for early endometrial cancer , because it is able to ensure the same local control as external beam radiotherapy ( ebrt ) but with fewer adverse effects , thus , improving quality of life [ 1 , 2 ]  . 
 according to a 2005 published survey [ 4 ] , most members of the gynecologic cancer intergroup did not record the dose to organs at risk ( oar )  . 
3d planning vbt has highlighted technical aspects like the need of oar delineation in each brachytherapy fraction , the dosimetric consequences of the cylinder tilt , and the consequences of different bladder volume distention [ 5 , 6 , 7 , 8 ]  . 
in contrast , rectal volume modification during ebrt has been extensively studied and different maneuvers have been implemented to reduce rectal dose deposition [ 9 , 10 ]  . in a previous analysis of 337 vbt applications , our group [ 11 ] demonstrated that posterior cylinder tilt and rectal distension increased rectal doses during vbt . 
general ricardos , madrid 3 department of radiation oncology , hospital universitari sant joan , reus reductionofrectaldosesby removalofgasintherectum duringvaginalcuffbrachytherapy that the removal of rectum gas pockets is related to the reduction of rectal dose . material and methods patients files of patients treated with vaginal cylinder brachytherapy were retrospectively reviewed . 
brachytherapy was performed with the largest diameter cylinder ( vaginal applicator set # 085350 , nucletron , veenendaal , the netherlands ) that comfortably fit the vaginal vault ; and the position of the cylinders was intended to remain parallel to the patient craniocaudal axis . 
the only instruction given to the patient prior to the procedure was to try to evacuate prior to coming to the hospital for vbt . no formal policy related to gas pockets inside the rectum during vbt existed in our department before this study was performed . 
a total of 14 pairs of ct studies belonging to 11 patients were retrieved ( 3 patients had 2 applications with removal of gas ) from the database . ct simulation all patients underwent pelvic ct scans , with 2 mm slice thickness at 2 mm overlapping intervals in supine position with a bladder foley catheter that instilled dilute contrast medium [ 5 ml of omnipaque350 ( ge healthcare bio - sciences ) in 45 ml of saline solution ] in order to increase bladder visibility during segmentation and volume reproducibility during treatment . 
 no attempt was made to modify vaginal cylinder position . segmentation and planning cts were transferred to a 3d treatment planning system ( oncentra v.4.1 , veenendaal , the netherlands )  . 
to improve comparisons , every image set was re - contoured and re - planned under the same conditions used for an iridium - 192 remote after - loading unit ( microhdr nucletron , veenendaal , the netherlands ) , regardless of the administered treatment . 
the entire bladder volume was delineated , and the rectum was defined from 1 cm superior to the cylinder tip to 1.5 cm below the last activated dwell source position . 
the angle of the vaginal cylinder applicator related to the horizontal line parallel to the craneocaudal patient axis was calculated , positive values meaning a tip directed to the bladder and negative values showing a posterior displacement of the cylinder tip toward the rectum . statistical analysis results are shown as mean ( standard deviation )  . 
dsh were also analyzed , and the following square areas were recorded d1 cm2 , d2 cm2 , d5 cm2 , d10 cm2 , d15 cm2 , d20 cm2 and a5 gy . 
 the second ct study showed an increase of the majority of bladder dosevolume parameters analyzed , d1 cc , d2 cc , d5 cc , and d10 cc that reached significance on paired tests . 
the only difference between pairs of cts was the presence or lack of gas in the rectuthe first ct showed the basal status and the second was carried out after gas removal with a tube . 
it also suggests that other actions directed to empty the rectum could have a similar effect . keywords endometrial neoplasms organs at risk gas pockets dosevolume histogram rectum reduktion der rektumbelastung durch ablassen der rektumluft vor intravaginaler brachytherapie zusammenfassung ziel . 
das rektumvolumen sank erheblich von 77 , 845 auf 55 , 4317 , 6 ml ( p = 0 , 0052 ) , nachdem die luft aus dem rektum entfernt worden war . 
das entfernen von luft aus dem rektum mittels einer sonde ist ein einfaches und kostengnstiges verfahren , um die rektumbelastung bei verwendung der intravaginalen brachytherapie zu senken und damit die therapeutische ratio zu verbessern . 
our study shows that avoidance of gas pockets translates in dosimetric dose improvements . vaginal vault brachytherapy is one of the most usual adjuvant gynecological treatments , especially for treating endometrial carcinoma , despite reports having focused on cervical cancer [ 12 ]  . 
3 8 paired graphs of rectum parameters [ full rectum and post - deflation ( empty ) values ] trials have shown the vaginal vault is the predominant site of relapse and the benefits of brachytherapy . 
 vaginal radiation - induced changes could be easily evaluated with vaginoscopy , but are rarely reported . the widespread use of 3d planning imaging has improved dose distribution knowledge further than that provided by orthogonal radiographs . 
technical issues associated with vbt are the cylinder alignment related to the craniocaudal patient axis , dose point placement , dosimetric consequences of repetitive ct use , dose fractionation , bladder , and rectum distension . 
using orthogonal films , an absolute mean rectal reduction dose of 12.9% was observed when the cylinder was horizontally placed compared with a rectal slant position [ 6 ]  . 
however , two studies have reported a dose increase [ 18 , 19 ]  . dana - farber cancer institute reported an increase in bladder volume [ 19 ]  . 
the increase of bladder volume was a consequence of the procedure duration ( use of a singlerow detector ct scan and rectal catheter placement )  . no reportsother than one previous study from our group [ 11 ] have focused on dosimetric consequences of rectal distention during vbt . 
due to the dosimetric effect of cylinder slant on rectal doses , data were reanalyzed after removal of 2 cases with more than 5 of cylinder angle displacement between cts . 
nevertheless , new emerging factors responsible of dose or organ modifications appeared , e.g. , anatomical displacement related to anal contractions [ 21 ]  . in the ldr brachytherapy setting , rectums were evacuated in the past due to the long - lasting procedure , which required to stay in hospital , and due to the need to locate the icru points on orthogonal rx films . 
 while the abs reports [ 22 , 23 ] do not give any recommendation about the issue , the gec - estro [ 24 ] advise administration of a rectal enema , but without any explanation about its goal . 
a mathematical model found that 2 cm3 rectum dose volume values derived from the outer contour are a good estimator of the 2 cm3 rectum wall dose [ 25 ]  . 
these dosimetric changes also appeared in the higher dose areas although they were more evident in the low dose zones . a major criticism of our study is the limited number of patients included and its retrospective nature . 
sabater department of radiation oncology , complejo hospitalario universitario de albacete ( chua ) c / hnos falc 37 , 02006 albacete spain ssabaterm@gmail.com compliance with ethical guidelines conflict of interest . 
arenas state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . original article strahlenther onkol 2013 189 : 938944 doi 10.1007 / s00066 - 013 - 0441 - z received : 11 july 2013 accepted : 31 july 2013 published online : 27 . 
september 2013 springer - verlag berlin heidelberg 2013 f.stielerf.wenzm.shif.lohr department of radiation oncology , university medical center mannheim , university of heidelberg , mannheim anovelsurfaceimagingsystem forpatientpositioningand surveillanceduringradiotherapy aphantomstudyandclinicalevaluation the surveillance function , the new scanning approach and gating may further improve the accuracy of liver and lung treatments [ 3 ] , provided that the inherent accuracy of the system is sufficient . 
 as a first step , we investigated the basic performance and accuracy of the new scanning method of the catalyst ( c - rad , uppsala , sweden ) system in a non - gated environment . 
these issues were addressed in both phantom experiments mimicking different clinical situations and in a prospective clinical study covering three anatomical regions . materials and methods phantom and clinical studies were performed on an elekta synergy ( elekta ab , stockholm , sweden ) accelerator with cbct . 
instead of using laser light to scan the surfaces , catalyst employs three high - power leds to project light with wavelengths of 405 ( blue ) , 528 ( green ) and 624 nm ( red ) onto the object . 
 an individual region of interest related to the paradigm can be defined . the phantom part of the study analyzed scanning quality , reproducibility image - guided radiotherapy ( igrt ) reduces setup errors and thus minimizes the margin between clinical target volume ( ctv ) and planning target volume ( ptv )  . 
cone - beam computed tomography ( cbct ) has been widely adopt ed and provides the most accurate patient positioning with a relatively low extra imaging dose to the patient [ 1 , 2 ]  . 
the current surface scan is compared to the reference surface ( based on planning ct ) and a shift vector is calculated [ 4 , 5 , 6 , 7 ]  . 
2 8 a color test setup , b shape test setup pinkwhite pink1 pink2 pink3 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 integration time ( s ) non - area detected half - area detected full - area detected graywhite gray1 gray2 gray3 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 integration time ( s ) fig . 
scans with settings that result in values in the blue area are not visible ; scans with results in the red area are fully visible ; green indicates half - visible scans and therefore the inherent accuracy of the system in a static , anthropomorphic situation . 
the influence of body shape and the color of the scanned surface on these parameters was measured and revealed that scan quality depends on the surface color and the surface shape . 
we tested surface detection with series of pink and gray surfaces ( .fig.2a ) and by adjusting the gain ( range 100600% ) and it ( range 1000 7000 s ) parameters . 
these manually applied shifts were compared to the measured shifts of the optical system . after obtaining institutional review board ( irb ) approval and informed patient consent , a total of 224 radiotherapy fractions in 3 patients being treated for head and neck cancer , 5 patients treated for thoracic tumors and 5 patients with pelvic tumors were selected for the clinical evaluation . 
the workflow was as follows : the planning ct dataset was sent to the treatment planning system ( monaco 3.2 ; elekta ab ) ; ctvs , ptvs and organs at risk were contoured and a treatment plan was created . 
 afterwards , the ct images , structure set and treatment plan were sent to a recordand - verify system ( mosaiq 2.41 ; elekta ab ) and the catalyst optical scanner . 
to strahlentherapieundonkologie112013 | abstract zusammenfassung strahlenther onkol 2013 189 : 938944 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 013 - 0441 - z f.stielerf.wenzm.shif.lohr a novel surface imaging system for patient positioning and surveillance during radiotherapy . 
 an institutional review board ( irb ) - approved clinical evaluation encompassing 224 fractions in 13 patients treated in three different regions ( head and neck , thorax , pelvis ) was then performed . 
catalysttm may reduce cbct scan frequency in patients where tumor location is fixed relative to the surface . keywords cone - bean computed tomography imageguided radiotherapy head and neck cancer linear accelerator target volume neues oberflchenbasiertes bildsystem zur positionierung und kontrolle der patienten whrend der strahlentherapie . 
wir evaluierten das potential des systems bezglich genauigkeit und reproduzierbarkeit in phantomtests und analysierten eine durch die irb genehmigte studie , welche 224 fraktionen aus 13 patienten in 3 unterschiedlichen regionen umfasste ( kopf - hals , thorax und abdomen )  . 
catalysttm ermglicht eine reduzierung der cbct - anzahl bei patienten mit fester tumoroberflchenrelation . schlsselwrter cone - beam - computertomographie bildgesteuerte strahlentherapie kopf - halskarzinom linearbeschleuniger zielvolumen compare patient positioning based on surface matching to patient positioning based on cbct matching , the following procedure was adhered to : patients were positioned initially with the room lasers aided by the mismatch projection function of the catalyst systepatients were then scanned with the cbct system and shifted to the planned position based on the location of the target volume in the planning ct . 
afterwards , a catalyst scan was performed and the resulting difference vector automatically derived by the system in three translational directions ( lateral , longitudinal and vertical ) and three rotational axes ( rotation = yaw , roll and pitch ) was recorded . 
an ideal match between surface scan and soft tissue matching results in zero shift vectors . we recorded the shifts to calculate mean values and standard deviations . results the phantom tests quantified positioning accuracy and reproducibility depending on object shape and color , respectively . 
for the pink - white and pink - 1 colors , the surface is not fully detectable when it and gain are beyond certain thresholds ( as indicated by the green halfvisible area )  . 
for pink - 2 , underexposure starts at very low it and gain values , 940 | strahlentherapieundonkologie112013 horizontal plane vertical plane face to catalyst test shapes good resolution resolution 1 resolution 2 resolution 3 vertical plane horizontal plane face to catalyst 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 1000 2000 3000 4000 5000 6000 7000 integration time ( s ) non - area detected half - area detected full - area detected lat - long ( mm ) long - vert ( mm ) lat - vert ( mm ) fig . 
4 9 a setup and different resolutions depending on gain and integration time ( good resolution : gain 200% , it 2000 s ; resolution 1 : gain 200% , it 4000 s ; resolution 2 : gain 200% , it 6000 s ; resolution 3 : gain 200% , it 8000 s )  . 
vert vertical , lat lateral , long longitudinal long manually applied shift measured shift manually applied shift measured shift but overexposure is also possible for high it and gain settings . 
for pink - 3 the surface is only fully detectable at high it and gain ; if it and gain are too low , underexposure occurs and the surface is not visible . 
the darker the surface is , the higher the it and gain settings have to be . based on these semiquantitative diagrams it becomes evident that although scan quality depends on color , it can be improved by manual adjustment of the strahlentherapieundonkologie112013 | original article fig . 
6 9 shift vector in cm or degree , as appropriate , for three translation directions ( lateral , longitudinal and vertical ) and three rotational directions ( rotation , roll and pitch ) for the 224 fractions . 
mean values standard deviations of the resulting shifts ( translations and rotations ) associated with the 224 recorded fractions are shown in .fig.6. no recorded catalyst shifts exceeded a 1 cm deviation from cbct measurements . 
analyzing the cbct with respect to target and overall surface , there was no clinical need to reposition the patient . the absence of fractions with shifts outside the tolerances and mean shift values that are always close to zero show that a systematic error does not exist . mean shifts including standard deviations , separated into scanned regions and as recorded across all patients are shown in .tab.1. 
 [ 4 ] compared the sentinel ( c - rad , uppsala , sweden ) system to cbct and portal imaging based on measurements with a rigid phantoa second study from this group was based on real clinical patients and analyzed thoracic and pelvic target regions separately with a total of 192 fractions [ 8 ]  . 
this system was also evaluated ( under its rebranded name galaxy ; lap laser , lneburg , germany ) in comparison to megavoltage ct ( mvct ) in a tomotherapy ( tomotherapy , madison , wi , usa ) unit in a study based on 200 treatment fractions [ 7 ]  . 
the system analyzed in the present study shows slightly better results ; not for the mean values but for the standard deviations , which means that the statistical error of this system / case study is smaller than the previous laser - based version / study . 
 [ 6 ] performed a clinical head and neck study with the alignrt ( vision rt ltd , london , uk ) systethey found a translational error of 2.44.5 mm and a rotational error of 0.82.2 , thus indicating somewhat worse agreement than our study . 
modern irradiation techniques such as volumetric modulated arc therapy ( vmat ) [ 10 , 11 ] , faster multileaf collimators ( mlc ) or flattening filter free ( fff ) linear accelerators were introduced into the clinical environment to accelerate the patient treatment . 
the optical system introduced in this study needs seconds to scan the patient and calculate the corresponding shift vector , thereby potentially reducing the time required for image guidance . several clinical aspects may influence scanning results . 
portal imaging instead of cbct is not adequate , due to limited soft tissue contrast unless fiducial markers are implanted . a second clinical aspect is patient breathing during positioning and treatment , particularly for lung / liver lesions . 
in order to use optical scanners to survey breathing motion , image quality and scan accuracy must be optimal . to date , the matching algorithm of the described system uses rigid matching of the surfaces . 
this work was supported within the framework of a research cooperation agreement between the department of radiation oncology , mannheim university medical center and c - rad ( sweden )  . compliance with ethical guidelines conflict of interest . 
 lohr state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
claraspital , basel prognosefrschwangere frauenmiteinemprimren mammakarzinom originalbeitrag amant f , minckwitz g von , han s et al ( 2013 ) prognosis of women with primary breast cancer diagnosed during pregnancy : results from an international collaborative study . 
datenregistrierung ( cancer in pregnancy , leuven , belgium ; gbg 29 / big 0203 ) erfolgte ein vergleich der prognose von bcp - patientinnen , die jnger als 45 jahre waren , mit nichtschwangeren patientinnen . 
die analyse erfolgte mit einer cox - proportional - hazards - regression , adjustiert nach alter , stadium , grading , hormonrezeptorstatus , her2neu - status , histologie , art der chemotherapie inkl . 
herangezogen wurden 447 frauen mit einem in der schwangerschaft diagnostizierten mammakarzinom , grtenteils aus deutschland und belgien , von denen 311 ( 69 , 6% ) fr eine auswertung geeignet waren . 
das gesamtberleben von schwangeren patientinnen mit brustkrebs ist vergleichbar mit dem nichtschwangerer patientinnen mit einem primren mammakarzinodiese kenntnis ist wichtig fr die beratung von schwangeren patientinnen und rechtfertigt es , sowohl die schwangerschaft fortzufhren , als auch die behandlung des karzinoms einzuleiten kommentar die studie von amant et al . 
 [ 1 ] ist ein wichtiger beitrag zur prognose von schwangeren mit einem neu aufgetretenen mammakarzinom und zur frage , ob die schwangerschaft dennoch weitergefhrt und trotzdem schon die behandlung eingeleitet werden darf . 
zustzlich waren auch die therapieergebnisse im lndervergleich ganz inhomogen : whrend sich nmlich das os in den beiden kollektiven aus deutschland und belgien identisch darstellte , waren die diesbezglichen daten in den anderen lndern fr die schwangeren deutlich schlechter . 
 whrend der schwangerschaft zeigen sich zwar fr strogene , progesteron und den ilgf ( insulin like growth factor ) signifikant erhhte konzentrationen , hormone also , die einen groen einfluss auf die entwicklung und progression von mammakarzinomen ausben . 
amant f , minckwitz g von , han s et al ( 2013 ) prognosis of women with primary breast cancer diagnosed during pregnancy : results from an international collaborative study . 
amant f , van calsteren k , halaska mj et al ( 2012 ) long - term cognitive and cardiac outcomes after prenatal exposure to chemotherapy in children aged 18 months or older : an observational study . 
of the individuals with grade iii astrocytoma , 27% live for at least 5 years and the most important prognostic factors identified as histology , age , and performance status [ 3 ]  . 
monoclonal antibodies that can locate and destroy tumor cells without harming normal brain cells are also being increasingly utilized for those with recurrent grade 3 or 4 astrocytomas [ 9 ]  . computed tomography ( ct ) and magnetic resonance imaging ( mri ) are the main radiological diagnostic methods . 
its specificity , however , is limited by passive tracer influx through a disrupted bloodbrain barrier and 19f - fet uptake in non - neoplastic brain lesions [ 7 ]  . with few exceptions , astrocytomas are not curable . 
the selectivity of ionizing irradiation , which is often relatively low for tumors , as compared to normal tissue , can be improved by using computer - controlled irradiation protocols with different types of radiation . 
moreover , the effect of irradiation on tumor tissue can be optimized , as mentioned , by the addition of radiosensitizing agents , in order to achieve greater damage to the neoplastic tissue than would be expected from the additive effect of each modality [ 4 ]  . during the 1980s , photodynamic therapy ( pdt ) began to emerge as a promising alternative for the treatment of early and localized tumors in which adequate local surgery is difficult , such as multifocal bladder cancer [ 8 , 17 ]  . 
the technique involves the topical or systemic administration of a photosensitizing agent which is preferentially accumulated or retained by the tumor tissue , followed by illumination of the neoplastic area with light wavelengths specifically absorbed by the photosensitizer [ 8 , 16 , 17 ]  . 
at present , the main photosensitizer in clinical use for pdt treatments is photofrin ii ( axcan , mont - saint - hilaire , canada ) , a complex mixture of porphyrins produced through acid treatment of hematoporphyrin derivative ( hpd ) [ 2 ]  . photofrin ii has recently been approved as a photosensitizing agent in the clinical treatment of selected solid tumors [ 8 , 16 , 17 ]  . 
the preferential affinity displayed by photofrin for tumors as compared to most normal tissues was the driving force in prompting studies aimed at investigating the possible use of porhyrins as tumor sensitizers during radiotherapy . 
 several recently published studies on tissue cultures and on murine tumor models have demonstrated the in vitro and in vivo efficacy of photofrin ii as both a specific and a selective radiosensitizing agent [ 11 , 12 , 13 , 14 , 15 ]  . 
this case report is aimed to focus on a treatment of a woman suffering from an inoperable astrocytoma grade 972 | strahlentherapieundonkologie112013 tial brain fields were used ( with shrinking field technique ) for the treatment of the patient ; the initial gross tumor volume ( gtv ) was defined as the hypodense edema or t2 abnormality , plus approximately 2 cthe boost gtv was defined as the contrast - enhancing tumor only , plus 2 cm ( clinical tumor volume , ctv )  . we chose to apply our boost irradiation at the time of peak photofrin ii concentrations in order to achieve the maximum effect on the tumor tissue . 
pharmakokinetic studies of photofrin ii and past in vivo experiments [ 14 ] have demonstrated the main therapeutic window of photofrin ii to be in the first week of application . 
the methodology applied was a reversed - phase ionpairing high performance liquid chromatography ( hplc ) with fluorescence detection after solid - phase extraction using the pure drug substance of photofrin for calibration [ 18 ]  . 
mri with a standardized protocol was performed immediately after the conclusion of therapy , and every 23 months thereafter ( .fig.2a , b ) , while after 3 years mri was performed every 6 months . 
positron emission tomography ( pet ) was performed before and after the conclusion of therapy , and years after . results the patient was alive without any significant side effect , at a follow - up of 106 months . 
the patient was advised to avoid direct contact with light and to especially protect her eyes in the first few days following therapy due to the known photosensitivity of porphyrins [ 2 , 8 , 16 ]  . 
she received a specially equipped room , which was completely shielded from sunlight and equipped with lighting not stronger than 40 w . she underwent irradiation with 40 + 20 gy boost with fractionation of 2 gy / day , for 5 days / week during septembernovember 2004 . 
the patient was injected with a single intravenous dose in i.v slow infusion ( 30 min ) of 1 mg / kg photofrin ii 24 h prior to radiation therapy . 
ctbased three - dimensional conformal radiation therapy ( 3dcrt ) , in which noncoplanar fields with unique entrance and exit pathways can be mapped on the target , has improved normal tissue sparing . 
skin reactions , such as edema , erythema or other lesions , related to the photosensitizer ( photofrin ii ) were not observed due to the maximal protection of the patient from any light sources stronger than 40 w . the relative serum level of photofrin ii peaked in the first 56 days after intravenous injection , followed by a subsequent steep decrease [ 18 ]  . 
an anaplastic astrocytoma can be a reoccurrence of a lower grade , previously treated , astrocytoma [ 5 , 6 , 9 , 10 ]  . malignant glial neoplasms are the most frequent primary brain tumors and are a leading cause of cancer - related deaths in the general population . 
die ergebnisse der nachbeobachtung fr die anwendung von photofrin ii als effektiver radiosensitizer in der behandlung von nichtoperablen astrozytomen grad iii sind sehr ermutigend . schlsselwrter strahlentherapie selektiver und spezifischer radiosensitizer astrozytom grad iii gliom dihmatoporphyrinether cells that require further treatment in the form of irradiation and chemotherapy . mortality , as defined by the length of a patients history and the odds of recurrence - free survival , are correlated most highly with the intrinsic properties of the astrocytoma in question . 
typical ranges of survival are approximately 10 years from the time of diagnosis for pilocytic astrocytomas ( who grade i ) , more than 5 years for patients with low - grade diffuse astrocytomas ( who grade ii ) , 25 years for those with anaplastic astrocytomas ( who grade iii ) ( if treated with radiation therapy )  . ongoing investigations into molecular control of cell replication and gene transcription hold promise for future control of malignant tumors , creating the possibility of curative surgical tumor excision without tumor regrowth [ 5 , 6 , 9 , 10 ]  . photofrin ii can act as an effective radiosensitizing agent , if applied under appropriate conditions . 
t2 - weighted image before and t1 - weighted image after administration of contrast medium by itself does not lead to a tumor response , it augments the response to ionizing radiation [ 11 , 12 , 13 , 14 , 15 ]  . 
on one hand , photofrin ii enhances the radiolytic activity by reacting with cytotoxic , activated molecules , such as oh radicals , which are produced as a result of the primary interaction of ionizing radiation with water [ 13 ]  . 
in the past , a similar mechanism was demonstrated for gd - tex , which forms a relatively stable radical anion by undergoing a one electron reduction [ 19 ]  . on the other hand , photofrin ii may reduce repair processes , which often limit irradiation - induced cellular damage . 
recent publication showed that a u - 87mg tumor cell population enriched with radiation - resistant tics ( tumor initiating cells ) becomes radiosensitive , and an inhibition of cell proliferation and an increase in apoptosis are found in the presence of photofrin ii . 
furthermore , u - 87mg tumors implanted in mice treated with photofrin ii and radiation exhibit a significant reduction in angiogenesis and vasculogenesis , and an increased percentage of apoptotic tics when compared with tumors grown in mice treated with radiation alone [ 1 ]  . this case report describes a female patient with inoperable astrocytoma grade iii , treated with radiation therapy and photofrin ii as a radiosensitizer . 
she was given a single intravenous dose of 1 mg / kg photofrin ii 24 h prior to the radiation therapy . the patient is still alive without any significant side effects or tumor evidence , with a follow - up of 106 months . 
schaffer state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . case study strahlenther onkol 2013 189 : 977979 doi 10.1007 / s00066 - 013 - 0444 - 9 received : 1 april 2013 accepted : 31 july 2013 published online : 25 november 2013 springer - verlag berlin heidelberg 2013 breast cancer patients develop mild to moderate acute adverse effects of skin and breast during adjuvant radiotherapy . 
a clinical case is presented and the diagnostic and therapeutic options are discussed . a 64 - year - old woman had lumpectomy and sentinel node biopsy for breast cancer pt1c pn0 m0 . 
there was only moderate erythema grade 2 ( common terminology criteria of adverse events ctcae v.4 ; [ 9 ] ) in the upper lateral field region , erythema grade 1 in u.hller1t.schubert1v.budach1u.trefzer2m.beyer2 1 radiation oncology and radiotherapy , strahlentherapie , charit universittsmedizin berlin , ambulantes gesundheitscentrum charit mitte , berlin 2 dermatology , charit universittsmedizin berlin blisters - anunusualskin effectduringradiotherapy the remaining breast and slight edema grade 1 of the entire breast . the patient was referred for dermatologic consultation and therapy . 
a direct immunofluorescence biopsy and test for serum antibodies against desmogleins ( a membrane protein belonging to the cadherin family ) and bullous pemphigoid antigen 1 and 2 ( found as part of hemidesmosomes ) were taken . 
differential diagnoses bullous pemphigoid , pemphigus vulgaris , and bullous impetigo are discussed and treatment described . keywords breast neoplasms radiation acute effect skin toxicity pemphigus impetigo bullae eine ungewhnliche hautreaktion whrend der strahlentherapie zusammenfassung die hautreaktion wird whrend der strahlentherapie kontinuierlich berwacht , um rechtzeitig eine erhhte strahlenempfindlichkeit der patientin / des patienten , eventuelle unerwartete interaktionen mit begleitmedikation oder eine unbemerkte berdosierung zu erkennen . 
1 9 bullous impetigo during radiotherapy of the breast could be found in our case , an autoimmune reaction was highly unlikely . bullous impetigo is a common and highly contagious superficial skin infection caused by staphylococcus aureus or streptococci [ 5 , 11 ]  . 
the major differential diagnoses are bullous pemphigoid , pemphigus vulgaris and bullous impetigo . bullous pemphigoid ( bp ) and pemphigus vulgaris are antibody - mediated autoimmune diseases rarely triggered by radiotherapy [ 1 , 3 , 4 , 7 , 8 , 11 ]  . 
in general , treatment consists of local or systemic steroids and immunosuppression with azathioprine . moreover , in the literature there are fewer than 20 cases of pemphigus vulgaris induced by radiotherapy in conjunction with the detection of autoantibodies . 
hller radiation oncology and radiotherapy , strahlentherapie , charit universittsmedizin berlin , ambulantes gesundheitscentrum charit mitte charitplatz 1 , 10112 berlin germany ulrike.hoeller@charite.de compliance with ethical guidelines conflict of interest . 
beyer state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . literaturkommentiert strahlenther onkol 2013 189 : 161162 doi 10.1007 / s00066 - 012 - 0249 - 2 online publiziert : 21 . 
dezember 2012 springer - verlag berlin heidelberg 2012 k.huber klinik fr strahlentherapie , universittsklinikum schleswig - holstein kiel karzinomdessophagus unddesgastrosophagealen bergangs berlebendurchneoadjuvante radiochemotherapieverbessert originalpublikation hagen p van , hulshof mccm , lanschot jjb van et al ( 2012 ) preoperative chemoradiotherapy for esophageal or junctional cancer . 
an tag 1 , 8 , 15 , 22 und 29 der radiotherapie wurden carboplatin ( auc = 2 ) und paclitaxel ( 50 mg / m2 kof ) intravens appliziert . 
auch das gesamtberleben war signifikant besser in der gruppe mit neoadjuvanter radiochemotherapie ( hr 0 , 657 ; 95% - ki 0 , 4950 , 871 ; 5 - jahres - berleben 47% versus 34% , p = 0 , 003 )  . 
ein systemischer review durch die practice guidelines initiative ( pgi ) des cancer care ontarios program in evidence - based care ( pebc ; [ 2 ] ) empfahl im jahr 2004 die alleinige operation als standardtherapie . 
vor allem nach publikation des magic - trial wurde daher an vielen institutionen , wenn berhaupt , als properative therapie eine alleinige chemotherapie wegen der vermeintlich geringeren toxizitt im vergleich zur radiochemotherapie eingesetzt . 
die einzige studie , in der properative chemotherapie und radiochemotherapie direkt miteinander verglichen wurden , war die in essen durchgefhrte poet - studie , in der sich ein trend ( also nicht signifikant ) zu deutlich bessestrahlentherapieundonkologie22013 | literaturkommentiert ren berlebensraten mit der radiochemotherapie zeigte [ 4 ]  . die jetzt publizierte studie der crossgroup besttigt , dass die radiochemotherapie die vermutlich beste properative therapie darstellt . 
erstens betrug die absolute verbesserung der berlebensraten 13 prozentpunkte ( wie im magic - trial , aber auf hherem ausgangsniveau ) und die 5 - jahres - berlebensrate von 47% ist fr dieses kollektiv herausragend gut . 
dabei ist zu beachten , dass in der cross - studie eine relativ niedrige gesamtdosis in konventioneller fraktionierung ( 41 , 1 gy , 23 fraktionen zu 1 , 8 gy ) appliziert wurde , hnlich wie in der poet - studie , wo es nur 30 gy waren . 
trotz der geringen toxizitt war aber ein guter prtherapeutischer allgemeinzustand ohne kritischen gewichtsverlust eine essentielle voraussetzung fr die vertrglichkeit dieser multimodalen therapie . einige wichtige fragen bleiben noch offen , vor allem die bedeutung molekularer prognosefaktoren im hinblick auf mgliche target - therapieanstze und der einfluss der tumorlokalisation [ 4 , 5 ]  . 
stahl m , walz mk , stuschke m et al ( 2009 ) phase iii comparison of preoperative chemotherapy compared with chemoradiotherapy in patients with locally advanced adenocarcinoma of the esophagogastric junction . 
n engl j med 355 : 1120 162 | strahlentherapieundonkologie22013 original article strahlenther onkol 2013 189 : 123128 doi 10.1007 / s00066 - 012 - 0258 - 1 received : 11 october 2012 accepted : 18 october 2012 published online : 21 . 
in the last decade , different imaging modalities [ magnetic imaging resonance ( mri ) , computed tomography ( ct ) , fluorodeoxyglucose positron emission tomography ( fdg - pet ) , transabdominal ultrasound ] were introduced for image - guided brachytherapy treatment planning [ 2 , 3 , 4 , 5 , 6 ]  . 
currently , mri is considered the gold standard for visualizing the local tumor extension and detecting parametrial involvement [ 6 , 7 , 8 , 9 , 10 , 11 ]  . 
several monoinstitutional studies demonstrated the potential of image - guided adaptive brachytherapy ( igabt ) with repetitive mri in reducing late morbidity and in improving local tumor control and even overall survival . 
hence , it may be assumed that centers and countries with limited financial resources will not be able to perform igabt ( or only in a very limited way )  . 
this means that countries especially in central / eastern europe and the developing world with the highest incidence of locally advanced cervical cancers will at present hardly profit from these therapeutic improvements . by contrast , low - cost imaging modalities , such as ultrasound ( us ) including transrectal us ( trus ) , are available worldwide , particularly in gynecology . 
 [ 12 ] showed , by comparing transabdominal us with mri , that the highly relevant areas of the parametrial space and the posterior uterus surface are also the area of highest uncertainty . in our department , us examinations including transabdominal , transvaginal , and transrectal us were performed in the last decade for gynecologic malignancies at the time of diagnosis as an up - front examination by a senior gynecologist ( ak )  . 
in addition , trus was performed to assess local tumor extension before starting the application and to verify the position of the applicator with or without interstitial needles after the application , if necessary and feasible . 
the primary aim was to retrospectively compare the maximum target width between mri and trus during the course of primary radiochemotherapy . patients and methods patients patients with locally advanced cervical cancer treated from 2009 to 2011 with curative intent by definitive external beam radiotherapy ( ebrt ) and igabt were included in this study . 
the inclusion criterion was the availability of complete mri and trus datasets performed within 7 days during the course of primary radiochemotherapyeither ( 1 ) at the time of diagnosis before the initiation of the ebrt , or ( 2 ) at the time of brachytherapy before insertion of the applicator , or ( 3 ) at the time of brachytherapy after insertion of the applicator . magnetic resonance imaging mri was performed according to our inhouse standard protocol for igabt with a 0.2 - t low - field system ( siemens magnetom open - viva ; siemens ag , munich , germany ) using a pelvic surface coil . 
a fast spin - echo technique , with a repetition time of 4 , 500 ms and an echo time of 96 ms for t2 - weighted images , strahlentherapieundonkologie22013 | original article fig . 
1 8 examples of trus ( a ) and mri ( b ) images of patients with locally advanced cervical cancer in the course of primary radiochemotherapy at the time of diagnosis ( 1st row ) , at the time of brachytherapy without applicator in place ( 2nd row ) and at the time of brachytherapy with applicator and interstitial needles in place ( 3rd row )  . 
the white dotted lines indicate the measured target width ( laterolateral diameter ) and the measured target thickness ( anteriorposterior diameter ) on trus ( c ) and mri ( d )  . 
the slice thickness was 5 mm with a 1 - mm intersection gap for the mri before the insertion of the applicator and no intersection gap for the mri after insertion of the applicator with a matrix of 256256 . transrectal ultrasonography trus was performed by two investigators ( ms , ak )  . 
all trus images at the time of diagnosis were evaluated with 5 mm slice thickness and images were oriented to the cervical axis . trus was performed at the time of brachytherapy on a b&k ultrasound device . 
static transversal images ( gray - scale examination ) were acquired in 5 - mm steps using a stepper unit beginning from the upper third of the vagina to the fundus uteri , if possible . 
correspondingly , the target was defined as the complete macroscopic tumor mass ( in the cervix , parametrial space , rectum , bladder , and vagina ) and the complete remaining cervix . 
subsequently , the target was defined on mri as the area of high signal intensity ( plus any gray zones at the time of brachytherapy ) and any remaining low signal intensity cervical stroma . 
to analyze the concordance of target width and target thickness between trus and mri , a linear regression analysis was performed with trus as predictor variable for the mri outcome . 
r2 estimates the goodness of regression model fit with a 5% significance level , 1 describes the slope of the line , and 0 the intercept to analyze systematical differences between both imaging modalities . 
all statistical analyses were performed using spss 15.0 software ( spss , chicago , il , usa )  . results patients in total , images from 17 patients could be included in this study . 
in 5 patients , images were obtained at the time of diagnosis , in 9 patients at the time of brachytherapy without an applicator , and in 3 patients at the time of brachytherapy with an applicator in place . 
trus and mr images at the time of diagnosis were always acquired before initiation of ebrt , and images at the time of brachytherapy with applicator in place were always acquired on the same day . image analysis all imaging characteristics are presented in .tab.1. 
t2 - weighted mri and trus were performed on patients with locally advanced cervical cancer at the same timepointeither at the time of diagnosis , or at the time of brachytherapy before or after insertion of the applicator . 
comparison of the target width and thickness showed a high correlation between trus and mri , indicating the potential of trus for target definition in image - guided adaptive brachytherapy . keywords cervical cancer radiotherapy image - guided adaptive brachytherapy magnetic resonance imaging transrectal ultrasonography mittlere maximale breite des zielgebiets betrug 4 , 20 , 83 cm fr die mrt und 4 , 20 , 79 cm fr die trus . 
diese vielversprechenden ergebnisse verweisen auf das mgliche potenzial der trus zur zielgebietsdefinition fr die bildgesttzte adaptive brachytherapie . schlsselwrter zervixkarzinom strahlentherapie bildgesttzte adaptive brachytherapie magnetresonanztomographie transrektaler ultraschall strahlentherapieundonkologie22013 | original article tab . 
 mri is cost intensive with regard to both equipment and manpower and is only available for radiotherapy planning at a limited number of institutionsit is lacking especially in central / eastern european countries and the developing world where the highest incidence of locally advanced tumors is observed . 
but even if available , igabt with mri poses logistical challenges : after the application , which is usually performed in an operating theater , the patient has to be transferred to the mri device and in case of inadequate location of the applicator and / or the interstitial needles , the patient needs to be retransferred to the operating theater for repositioning of the applicator , after which imaging has to be repeated . 
such procedures are time consuming , require high flexibility of the treating team ( radio - oncologists , anesthesiologists , physicists , radiotechnologists etc . ) , and are stressful for the patients if the mri is not directly integrated in the brachytherapy / radiotherapy department . 
furthermore , igabt ( especially in cases with a combined intracavitary interstitial application ) as currently practiced involves mainly image - based treatment planning , while the insertion of the applicator and the interstitial needles is mostly clinically guided [ 19 ]  . 
the utilization of trus during the application allows for exact visualization of the movement of the implanted needles as well as of changes in the pelvic topography within the field of view [ 20 , 21 , 22 , 23 , 24 ]  . 
 [ 28 ] compared the tumor volume in patients with early invasive cervical cancer between trus , mri , and the pathology - derived tumor volumes and indicated that the accuracy of trus for the assessment of tumor vol126 | strahlentherapieundonkologie22013 target width target thickness patients ( n = 16 ) linear regression 95% confidence interval patients ( n = 13 ) linear regression 95% confidence interval trus : maximum diameter in cm trus : maximum diameter in cm ume and the detection of parametrial involvement was even superior to mri . 
regarding the application of trus in interstitial brachytherapy for primary and recurring cervical cancer , trus has been described as feasible for the visualization of the needles , thereby allowing accurate needle placement [ 29 , 30 , 31 ]  . in the present study , trus and mri were compared in the course of radiochemotherapy in cervical cancer patients for the first time . 
imaging was performed at different time points ( at the time of diagnosis and at the time of brachytherapy with and without applicator in place ) in patients with different tumor stages and tumor sizes . 
in these various situations , trus and mri showed a high correlation for the measurement of target width and target thickness , indicating that trus is feasible for the assessment of local target extension in cervical cancer treated by radiochemotherapy . 
the retrospective character of the study and the fact that in the majority of patients trus images were acquired with separate transversal slices of 5 - mm distance instead of true 3d volumes did not allow an evaluation to be made of the target height . in 1 patient trus could not be evaluated because of artifacts , which appeared to be related to air in the bowel . 
weitmann hd , knocke th , waldhusl c et al ( 2006 ) ultrasound - guided interstitial brachytherapy in the treatment of advanced vaginal recurrences from cervical and endometrial carcinoma . 
 strahlenther onkol 182 : 8695 original article abstracts strahlenther onkol 2013 189 : 173188 doi 10.1007 / s00066 - 012 - 0284 - z springer - verlag berlin heidelberg 2013 abstracts der 29 . 
annemarie schratter - sehn , smz sd - kaiser franz josef spital wien priuniv . - felix sedlmayer , salzburger landeskliniken pridietmar seewald , lkh vcklabruck abstracts entwicklung der radioonkologie in obersterreich hammer j.1 1abteilung fr radioonkologie , kh barmherzige schwestern , linz nachdem w.c. 
ab januar 2013 bernimmt hans geinitz die leitung der abteilung . im jahr 2008 hat dietmar seewald die leitung des neu errichteten institutes fr strahlentherapie / radio - onkologie am lkh vcklabruck , obersterreich , bernommen . 
diese therapieform soll mit der errichtung des medaustron zentrums fr ionentherapie und forschung in einigen jahren in sterreich verfgbar se christian doppler laboratory for medical radiation research for radiation oncology overview and first results georg d.1 1division medical radiation physics , department of radiooncology & cd laboratory medical radiation research for radiation oncology , medical university of vienna introduction . 
progress in radiation oncology has always been closely linked with innovations in medical radiation physics and computer sciences , morphological and molecular / biological imaging methodologies , and new insights into the radiobiology of both tumors and normal tissues . 
the vision of the christian doppler ( cd ) laboratory for medical radiation research for radiation oncology is to link these developments for the optimization of the treatment outcome of radiation oncology . 
preliminary research achievements in mmi of prostate cancer , technology developments for ultrafast 2d / 3d image registration , flattening filter free photon beams , ion beam treatment planning , as well as pre - clinical animal studies w.r.t. 
die individualisierung der bestrahlungsplanung in der radiotherapie muss auch die zeitliche komponente umfassen , da es im laufe der behandlungsserie zu morphologischen vernderungen und in verbindung damit zu lagerungsabweichungen kommen kann . 
danach werden die konturen mit hilfe eines algorithmus zur elastischen bildregistrierung ( redeform , joanneum research , graz ) auf die aktuelle ct - datensatz bertragen und die bestrahlungsplne ( vmat - technik ) neu optimiert . 
there has been some controversy over the appropriateness of lq model predictions of isoeffect doses whenever the dose per fraction greatly exceeds the conventional 2gy ( 1 , 2 ) , in part due to the conviction that the dose - survival curve is linear at high doses . 
data are examined from three sites ( breast , prostate , and lung ) where hypofractionation or sbrt has been used , and using relevant / values for tumor response and toxicity the size of dose per fraction at which the underestimation of isoeffect doses by the lq model exceeds 10% is estimated . 
wie sieht die zeitgeme therapie des akustikusneurinoms ( akn ) aus ? welchen kriterien folgt die adquate therapiewahl fr den patienten ? gibt es die wahlmglichkeit zwischen operation und bestrahlung ? methode . 
durch mehrmalige bildgebung ( nach jeder tischrotation ) ist eine exakte einstelstrahlentherapie und onkologie 2 2013 | abstracts lung mglich ohne den patienten zu sehr durch die fixation zu belasten . 
nach intraoperativer clipmarkierung der sln - region erhielten 52patientinnen eine ganzbrustbestrahlung ( wbrt ) mittels intensittsoptimierter tangentialer boston - technik ( 49 pat . ) oder mehrfeld - imrt ( 3pat . ) in unterschiedlicher fraktionierung ( 2 , 02 , 7gy ed )  . 
in der sln - region wurden bei 39 / 52 patientinnen ber 95% der vorschreibungsdosis appliziert , bei weiteren zwei patientinnen 90 95% , bei fnf 5070% und bei weiteren sechs unter 50% . 
im rahmen der tangentialen wbrt werden bei bis zu einem fnftel der unmittelbar ersten stationen des axillren lymphabflusses ( sln , aln - level iii ) mit teiloder insuffizienten dosen erreicht . 
im zeitraum januar 2002 bis dezember 2007 wurden 83patientinnen im klinischen stadiumii oder iii identifiziert , die vor der brusterhaltenden operation mit axillrer dissektion eine neoadjuvante chemotherapie mit 36zyklen eines anthrazyklin / taxanehltigen schemas erhalten hatten . 
intraoperativ wurde ein single - shot - boost des tumorbetts mit elektronen in der hhe von 9gy an der 90% referenz isodose vorgenommen , gefolgt von einer ganzbrustbestrahlung in 176 | strahlentherapie und onkologie 2 2013 ergebnis . 
der toxizittsvergleich erfolgte mit jenen patienten die mit i125 als monotherapie behandelt wurden , deren alter und funktioneller ausgangsstatus ( restharn , qmax , ipss , iief , qol ) dem status der kombiniert behandelten patienten vergleichbar war . 
die kombination von interstitieller permanentimplantation mit i125 und externer strahlentherapie ( hormontherapie ) ist von seiten der urogenitalen als auch der rektalen toxizitt durchaus mit der monotherapie mit i125 vergleichbar und somit akzeptabel . 
nach einem mittleren fup von 59monaten ( 3115 ) wurden zwei in - brust - rezidive im vormaligen tumor - index quadranten detektiert , entsprechend einer lokalkontrolle ( lc ) von 98 , 5% nach medianer nachbeobachtungszeit und 91 , 5% aktuariell . 
nach einem medianen fup von 5jahren ergibt sich ein metastasenfreies berleben ( ffm ) von 86 , 8% , ein krankheitsfreies berleben ( dfs ) von 80 , 7% , ein krankheitsspezifisches berleben ( dss ) von 89 , 2% und ein gesamtberleben ( os ) von 86 , 4% . 
die 4 - jahres biochemische kontrollrate dieses hypofraktionierten sib - konzeptes unter tglicher image guidance ist exzellent , bedarf aber noch lngerer nachbeobachtung um ein abschlieendes urteil bilden zu knnen . 
in der univariaten analyse zeigten damit die 70 - gy - patienten eine signifikant schlechtere bned - rate verglichen zur bt ( p = 0 , 001 ) zwischen 74 gy und bt zeigte sich kein signifikanter unterschied ( p = 0 , 6 )  . 
ziel der vorliegenden studie war die untersuchung von interund intrafraktionellen prostatabewegungen sowie residualen setup - fehlern nach positionierung anhand von implantierten markern zur evaluierung von ptv sicherheitssumen fr unterschiedliche lagerungstechniken . 
in einer offline analyse aller kvund mv - bilder wurden die interund intrafraktionelle prostatabewegung , der residuale set - upfehler nach markerbasierter patientenpositionierung sowie der effekt der behandlungszeit auf die intrafraktionelle prostatabewegung untersucht . 
die zur bercksichtigung der intraund intrafraktionellen prostatabewegung und des residualen set - up - fehlers erforderlichen sicherheitssume bei patientenpositionierung anhand von hautmarkierungen betrugen 14 , 13 , 15mm und bei positionierung anhand von knochenstrukturen 10 , 9 , 3 mm in ap , si und lr richtung . 
da sich eine zunahme der fr die intrafraktionelle prostatabewegung erforderlichen sicherheitssume mit zunehmender behandlungszeit zeigte , reduzierten sich sicherheitssume auf 4 mm ( ap ) , 2 , 4mm ( si ) und 2 , 6mm ( lr ) bei einer behandlungszeit 4m schlussfolgerung . 
2568 images gained during 642 fractions ( supine , flat couch , knee support , comfortably full bladder , empty rectum , no intraprostatic marker migrations > 2mm of more than one marker ) were analysed : 95 fractions in the spacer group and 126 fractions in the control group , respectively . 
whereas spacer application leads to a significant dose reduction in the anterior rectal wall , interand intrafractional mobility of the prostate was not affected , which has to be taken into account in safety margin design . 
das ziel der studie war ein retrospektiver vergleich der maximalen durchmesser ( breite , dicke ) des zielgebiets bei patientinnen mit lokal fortgeschrittenem zervixkarzinom zwischen dem transrektalem ultraschall ( trus ) und der magnetresonanztomographie ( mrt ) im verlauf der primren radiochemotherapie . 
 eine gewisse variation ist dabei akzeptabel und nachvollziehbar , da die klinische evaluierung hauptschlich auf objektiven kriterien beruht , whrend patientenberichte auch eine subjektive einschtzung der auswirkungen , beispielsweise auf die lebensqualitt , beinhalten . 
und patientenberichte aus dem lebensqualittsfragebogen eortc - qlq - c30 / cx24 wurden in bezug auf 12symptome in 223 patientinnen ( von 5 zentren ) mit zervixkarzinom drei monate nach ende der definitiven radiochemotherapie im rahmen der laufenden embrace studie verglichen . 
die analyse der diskrepanzen legt nahe , dass nebenwirkungen der strahlentherapie von zervixkarzinomen in der rztlichen beurteilung hufig unterschtzt werden : fast die hlfte aller im lebensqualitts - fragebogen substantiell ausgeprgten symptome wird in der klinischen einschtzung mittels ctcae nicht erfasst ( g0 )  . 
inzidenz ( anzahl neu aufgetretener nebenwirkungen whrend einer definierten zeitperiode ) und prvalenz ( anzahl von nebenwirkungen zu einem bestimmten zeitpunkt ) wurden analysiert . strahlentherapie und onkologie 2 2013 | abstracts ergebnis . 
zwischen 2004 und 2009 wurden 160 nichtselektionierte patienten mit 164 histologisch / zytologisch nachgewiesenen nsclc behandelt ; tumorstadium i / ii / iiia / iiib bei 38 / 6 / 69 / 47 patienten . 
primre fragestellungen der studie sind lokale und regionale tumorkontrollraten nach 2jahren ( > 90% der lokoregionalen rezidive treten innerhalb von 2 jahren auf ) , sekundre fragestellungen sind berlebenszeiten und tolerabilitt . 
zwei patienten erlitten eine akute grad - 5 - toxizitt ( progrediente lungenfibrose bei bereits prtherapeutisch bestehender fibrose ) ; im allgemeinen aber wurden die behandlungen gut toleriert : lunge grad 3 : 4% ; sophagus grad 2 / 3 : 10% / 4% . 
die motivation zur anwendung der rapidarc - technik bei csi war gegeben , als uns eine patientin im rahmen des met - hit - 2000 - ab4 - m2 - 4 - protokolls zur radiotherapie zugewiesen wurde , bei der die auslastung des spinalkanals wegen 180 | strahlentherapie und onkologie 2 2013 manifester spinaler metastasen mit 5000 cgy vorgeschrieben wurde . 
das alter der patienten betrug im mittel 49 , 6jahre ( range 2083 ) , die verwendete mittlere einzeldosis war 2 , 2 gy ( rbe ; range 23 ) , die mittlere gesamtdosis 67 , 4gy ( rbe ; range 4874 )  . 
bei smtlichen 19patienten mit schdelbasischordomen , ist eine exzellente lokale tumorkontrolle erzielt worden , ohne auftreten relevanter nebenwirkungen . merkel - mellkarzinom orasch c.1 1strahlentherapie / radioonkologie klinikum klagenfurt am wrthersee einleitung . 
karnofsky performancestatus ( kps ) und serum laktatdehydrogenase ( ldh ) waren die einzigen unabhngigen prognostischen faktoren fr das gesamtberleben ( hr 3 , 3 [ 95% ci 1 , 66 , 5 ] und 2 , 8 [ 95% ci 1 , 64 , 9 ] )  . 
damit patientinnen und deren angehrige eine entsprechende untersttzung zuteil werden kann , ist es erforderlich , zustzlich zu den onkologischen befunden im rahmen der radioonkologischen nachsorge , weitere informationen ber die aktuelle lebenssituation der patientinnen zu erheben . 
 auswirkungen krperlicher einschrnkungen auf das tgliche leben , stand in der verarbeitung des erlebten , vorhandene ressourcen und vieles mehr stellen die voraussetzung zur einleitung entsprechender sinnvoller rehabilitativer manahmen dar . 
die hemmung der ceramid - synthese erfolgte mit desipramin oder fumonisin , bei einzeitbestrahlung von tag 3 bis zur diagnose / heilung der ulzera , bei einwchiger bestrahlung mit beginn an tag - 3 bis zu testbestrahlung , erstdiagnose bzw . 
bei 355 patienten der klinik fr strahlentherapie der tu dresden aus den jahren 20072010 mit einer strahlendosis in der mundhhle > 40 gy wurden schleimhautreaktionen ( rtog / eortc klassifikation ) und alkoholkonsum vor therapiebeginn und tglich an den bestrahlungstagen erfasst . 
bei trgerinnen des 634g > c polymorphismus ergab die kaplan - meier - analyse ein erniedrigtes risiko fr die entwicklung von fernmetastasen ( p = 0 , 027 ) und in der univariaten cox - analyse betrug die hazard - ratio fr fernmetastasierung 0 , 69 ( 95%ci 0 , 520.92 ; p = 0 , 012 )  . 
ebenso ergab sich fr den ccccc haplotyp , welcher aus 5polymorphismen vor der kodierenden sequenz gebildet wird und auch den 634g > c polymorphismus enthlt , ein signifikanter zusammenhang mit fernmetastasierung ( hr = 0 , 655 , 95% ci 0 , 4870 , 882 ; p = 0 , 004 )  . 
rechenmodelle besttigen dies , weisen aber mit dvh bercksichtigung auf ein vermindertes strahleninduziertes kb - krebsrisiko hdie geringe kbd sollte klinische entscheidungen nicht beeinflussen , da der hauptnutzen in der herzdosisreduktion fr alle patientinnen besteht . 
bei patienten mit einer klinischen und pathologischen komplettremission ( pcr ) ist eine wait - and - see - strategie zu diskutieren , da die prognose in bezug auf ein lokalrezidiv keinesfalls schlechter ist als nach einer operation strahlentherapie und onkologie 2 2013 | abstracts mit pcr und postoperative komplikationen vermieden werden knnen . 
nach einer errechneten dreidimensionalen registrierung ergab sich eine korrektur der patientenposition zwischen einer aktuellen position und einer referenzposition von lateral 0 , 42 , 4mm , longitudinal 0 , 31 , 9 mm und vertikal 4 , 14 , 6 m die differenz zwischen dem aktuellen und der referenzposition nach zwei minuten betrgt 1 , 20 , 7mnach zwei wochen hatte eine interfraktionelle bewegung ( entspannungseffekt ) einfluss auf die patientenpositionierung , speziell auf die vertikale achse ( 4 , 95.1mm ; min 5 , 7mm ; max 17 , 6mm )  . 
the integration into the treatment planning system hyperion is ongoing . mr - gesttzte therapieplanung kleiser r.1 1abteilung fr radiologie , o landes - nervenklinik wagner - jauregg , linz einleitung . 
strahlentherapie , medizinische universitt wien / akh wien , 2ebg medaustron , wiener neustadt , 3christian doppler labor fr medizinische strahlenforschung fr die radioonkologie , medizinische universitt wien , 4univ . 
using a new splitting approach , a minimization routine selects the optimal shape for each sub - bea dose depositions were determined using a look - up table ( lut ) , derived from mc simulations in water using gate6.1. 
in homogeneous phantoms differences between pb and mc increased slightly with material density , resulting in range deviations of 0.6mm for adipose tissue and differences in the shape of the bragg - peak of less than 0.1mm for 150mev / a . 
der grund fr die langsame datenaufnahme liegt darin , dass bei der bildkodierung nur eine beschrnkte anzahl an datenpunkten aufgenommen werden kann , und die messung mehrmals wiederholt werden muss . 
eine mglichkeit , die messzeit zu verringern besteht dari , die anzahl der daten , die verwendet werden um ein bild mit einer definierten auflsung zu rekonstruieren , zu verringern . 
auslser fr die entwicklung einer plugin - orientierten softwarearchitektur fr die strahlentherapie sind die erweiterten anforderungen der neuen klinischen methoden wie z.b. : tracking , gating und neue einsatzgebiete wie z . 
the legs of the c - shaped bow extend in a direction substantially parallel to the longitudinal extension of the patient couch , one end of the c - shaped bow being fixed to a longitudinal end of the patient couch and the other end of the bow being fixed to the robotic arthe robotic arm is configured to position a patient arranged on the patient couch in six degrees of freedom with respect to a medical treatment or examination device . 
die rationale hierfr liegt vor allem in den potentiell schnellen rckkopplungsschleifen , die im vergleich zu volumetrischen aufnahmeprotokollen wie etwa cone beam computer - tomographie ( cb - ct ) , zustzlich wesentlich weniger dosisdeposition implizieren , und mitunter intrafraktionelle kontroll und ausrichtungsprozesse untersttzen . 
in diesem zusammenhang spricht man von der 2d / 3d - registrierung , einem algorithmus , der anhand eines planungs - cts und eines oder mehrerer kv - rntgenbilder des patienten unmittelbar vor oder whrend der bestrahlung am linac mgliche mispositionierungen quantifiziert . 
damit kann die patientenposition und / oder der bestrahlungsplan so adaptiert werden , dass eine im sinne der jeweiligen bestrahlungsplanung bestmgliche therapie appliziert wird . in diesem vortrag wird das derzeitige portfolio unseres instituts bezglich intensittsbasierter 2d / 3d - registrierung umrissen , sowie die klinische validierung des besagten ansatzes prsentiert . 
 darber hinaus skizzieren wir zukunftstrchtige anstze , die zu intrafraktionellen lokalisationsvorgngen beitragen sollen . a new european patent application is presented , describing an innovative imaging solution for igrt : a ceiling mounted robotic system that can be retro - fit installed in any bunker providing much faster dual energy planar as well as volumetric images . the present invention provides an imaging system comprising an imaging ring system with carriage ring fixed to the carriage , first rotatable ring carrying a first imaging unit , and second rotatable ring carrying a second imaging unit , wherein the first and second rotatable rings are configured to be rotated independently from each other on the carriage ring . 
fr das praktikum gibt es gesetzliche vorgaben hinsichtlich des zeitlichen umfanges mindestens 25% der ausbildung ( 1125stunden ) sowie der inhalte . so hat die praktische ausbildung berwiegend im medizinischen untersuchungsund behandlungsbereich stattzufinden . 
die anleitung und kontinuierliche betreuung an der praktikumsstelle muss durch eine fachkompetente person erfolgen ( ausbildungsschlssel 1 : 2 )  . im rahmen der praktischen ausbildung sind untersuchungen und behandlungen unter bercksichtigung strahlenhygienischer manahmen in pflichtbereichen vorzubereiten , durchzufhren , auszuwerten sowie die ergebnisse zu analysieren und hinsichtlich qualitativer richtlinien zu bewerten . fr den bereich der strahlentherapie sind mindestens 15 planungen einschlielich simulation sowie mindestens 35 bestrahlungen in den bereichen teleund brachytherapie durchzufhren . 
die ausbildung wird mit einer bachelorprfung abgeschlossen , die studierenden erhalten den ersten akademischen abschluss sowie die berufsberechtigung als radiologietechnologin , als radiologietechnologe . bestrahlungstechnik rapidarc im hno - bereich pils a.1 1abteilung fr radioonkologie , kh barmherzige schwestern , linz einfhrung . 
der groe vorteil der rapidarc - bestrahlung besteht in der verkrzten behandlungsdauer der einzelnen bestrahlungssitzungen , sowie in einem optimalen bestrahlungsplan und damit verbunden eine bessere schonung der risikostrukturen / organe . 
das resultat dieser bestrahlungsart ergibt eine wesentliche schonung des herzens und der lunge , da die bestrahlung nur in der inspirationsphase erfolgt , in der sich das herz fern der thoraxwand befindet . 
eine deutliche abnahme der rektumdosis mit spacer ist in dieser untersuchung erkennbar . strahlentherapie und onkologie 2 2013 | originalien strahlenther onkol 2013 189 : 111116 doi 10.1007 / s00066 - 012 - 0259 - 0 eingegangen : 18 . 
moderne behandlungstechniken [ 2 , 3 , 17 , 20 ] erhhen die anforderungen an daten [ 4 , 5 , 7 , 8 ] und bildmanagement [ 4 , 9 , 13 , 16 ] sowie den dokumentationsaufwand stndig . 
um dem immer strker werdenden konomischen druck bei gleichzeitiger verbesserung der behandlungsleistung und deren qualitt standhalten zu knnen , hat sich die klinik fr strahlenheilkunde zum ziel gesetzt , alle relevanten arbeitsablufe als volldigitale prozesse abzubilden . 
nach der integration von behandlungsplanung und ordination , sollte die abbildung der bestrahlungsplanung im system erfolgen . besonders anspruchsvoll ist hierbei die integration der bestrahlungsplanung in einen digitalen workflow [ 12 , 19 ] , da zum einen fr diesen komplexen prozess klar definierte bergnge ( schnittstellen ) zu mehreren berufsgruppen festgelegt sein mssen und zum anderen die reproduzierbarkeit und validitt aller teilprozesse gewhrleistet sein muss . 
besonders wichtig waren die behandlungsplne und bestrahlungsprotokolle , da in diesen dokumenten die wichtigsten behandlungsparameter , die entsprechenden verantwortlichen mit unterschrift und die bergange zu den diversen verantwortlichkeiten genau dokumentiert waren . soll nun dieser prozess digital abgebildet werden , muss man sicher stellen , dass alle geforderten eigenschaften der papierbehafteten dokumentation erfllt sind . 
durch ein zuverlssiges datenspeicherungsund archivierungskonzept unter verwendung zukunftssicherer technologien [ 10 , 11 ] muss gewhrleistet werden , dass alle daten auch bis zum ende des derzeit gesetzlich geforderten zeitrahmens von 30 jahren [ 1 , 16 , 18 ] noch zur verfgung stehen . material und methode im rahmen der implementierung unseres betriebsablaufsystems [ 6 ] wurde eine interdisziplinr besetzte arbeitsgruppe ( bas - ag ) gegrndet , die aus rzten , physikern , informatikern , mtras , patientenmanagement und je nach fragestellungen auch aus geladenen gsten besteht . 
diese arbeitsgruppe trifft sich regelmig , erarbeitet alle administrativen prozesse in unserer klinik und setzt die gewonnen erkenntnisse / ergebnisse um . in einem ersten schritt unterzog diese gruppe das bestehende verfahren der bestrahlungsplanung einer genauen analyse . 
wie hierin ersichtlich , bestand die aufgabe nicht nur darin , die behandlungsparameter und vorgaben abzubilden , sondern vor allem die integration der personengebundenen freigaben an den strategisch wichtigen abschnitten innerhalb der bestrahlungsplanung und - durchfhrung vorzunehmen . 
 auerdem musste berprft werden , welche implementierungsformen das von uns eingesetzte betriebsablaufsystem in dieser hinsicht berhaupt zulsst . anhand dieser vorgaben wurden diverse digitale modelle diskutiert und schlielich ein tragfhiges konzept erarbeitet . 
.abb.2 zeigt das flussdiagramm fr den digitalen gesamtprozess der konformalen bestrahlungsplanung , welchen wir letztendlich favorisiert und umgesetzt haben . die abbildung zeigt sehr anschaulich , aus wie vielen einzelschritten und statusbergngen die bestrahlungsplanung besteht . 
1 8 klassischer bestrahlungsnachweis ( din - 6827 - 1 ) ordination ( fa ) ( a / mtra ) " k " ct ( mtra ) bildtransfer + risikoorgane konturieren ( mtra ) ( mtra ) eingabe des zielvolumens + risikoorgane ( fa ) neuer plan termin auf ( fa ) " notiz sperren " physikalische bestrahlungsplanung ( phy ) direkt telefon . " k " in bpl ( phy ) plan evaluieren ( fa ) plan freigeben durch terminsetzung auf bpl - dokument ( fa ) " notiz sperren " ( fa ) plandokumentation ( phy - mtra ) qa : 1 . 
kontrolle ( phy ) simulation vergabe des einstelltermins ( a + mtra ) verifikationlagerungsaufnahmen ( fa ) felder anlegen ( mtra ) kontrolle ( fa ) kontrollen ( phy ) " approven " ( fa ) einstellung am linac portal imaging / igrt ( fa + mtra ) " k " und " notiz sperren " ( fa ) " k " bpl - doku ( mtra ) ordination prfen ( fa ) " nderung " nein " k " sim ( mtra ) erstbestrahlung am linac ( a + mtra ) 112 | strahlentherapieundonkologie22013 abb . 
a arzt ( assistenzarzt , fachkundiger arzt , oberarzt ) , fa fachkundiger arzt , oberarzt , phy medizinphysikexperte , mtra medizinisch technische ( r ) rntgenassistent ( in ) , bpl bestrahlungsplanungsliste , ct computertomographie , sim simulator des bestrahlungsplanungssystems dar . 
 des weiteren mussten wir gewhrleisten , dass bei vorliegen verschiedener planvarianten zu einem patienten im bestrahlungsplanungssystem immer nur der plan in das abteilungssystem importiert wird , der auch zur anwendung am patienten kommt . 
da es immer wieder vorkommt , dass nderungen oder gar neuplanungen notwendig sind , mussten wir auch fr diese mglichkeiten vorsorge treffen ( rote items )  . fr die umsetzung des projekts wurden im abteilungssystem neben den physikalisch echten , mit gertschaften bzw . 
dieses vorhaben stellt fr ein prozessmanagement eine der grten herausforderungen dar , da zum einen fr diesen komplexen prozess klar definierte bergnge ( schnittstellen ) zu den beteiligten berufsgruppen festgelegt sein mssen und zum anderen die reproduzierbarkeit und validitt aller teilprozesse gewhrleistet sein mssen . 
die vorhandenen ablufe und gesetzlichen anforderungen der bestrahlungsplanung wurden durch eine interdisziplinre arbeitsgruppe ( bas - ag ) im detail analysiert und nach der berprfung und bewertung der abbildungsmglichkeiten in unserem betriebsablaufsystem in ein flussdiagramm umgesetzt . 
nach der fertigstellung des konzepts und implementierung in unserer testumgebung erhielten wir nach der berprfung durch das fr uns zustndige regierungsprsidium die zustimmung fr den einsatz des verfahrens als volldigitalen gesamtprozess . schlsselwrter automatische datenverarbeitung datenspeicherung datensicherheit dokumentation arbeitsablauf integration of the radiotherapy irradiation planning in the digital workflow abstract backgroundandpurpose . 
during the testing phase , our digital workflow was examined and afterwards was approved by the responsible authority . keywords automatic data processing data storage data security documentation workflow strahlentherapieundonkologie22013 | originalien abb . 
5 9 web - portal fr das anforderungsmanagement von bildern 114 | strahlentherapieundonkologie22013 handlung dargestellt , wobei die wechsel zwischen virtuellen und realen rumen gut erkennbar werden . da alle anforderungen und termine in einen zeitlichen kontext eingebunden sind , lassen sie sich auch in dieser hinsicht gut analysieren . 
der einzelne vorgang und die jeweils verantwortliche person sind also ber diese arbeitsweise eng und eindeutig miteinander verknpft , so dass nicht nur jeder einzelne prozessschritt berall und jederzeit einsehbar ist , sondern auch alle personen , die am ablauf wann und wie beteiligt waren , sofort erkennbar sind . 
diese vorgehensweise stellt sicher , dass alle arbeitsschritte im system erfasst und gespeichert sind . hierbei muss erwhnt werden , dass fr die datensicherheit und - archivierung aufwendige vorkehrungen zu treffen sind , da bei einem verzicht auf papier alle informationen nur noch in digitaler form vorliegen . 
im rahmen des groprojekts bas in der strahlenheilkunde des universittsklinikums freiburg fand dieser punkt von vornherein bercksichtigung und ist daher auch fr dieses teilprojekt , vor allem auch in hinblick auf die durch die strahlenschutzverordnung vorgeschriebene datenverfgbarkeit von 30 jahren , sichergestellt . 
die darstellung dieses umfassenden datensicherungskonzepts kann an dieser stelle leider nicht erfolgen ; wir werden aber in einer weiteren publikation dieses modell im detail vorstellen . ein weiterer wichtiger teilprozess ist die auswahl der sequenzen von cts und mrts , die in das planungssystem eingelesen werden mssen . 
1 abfolge virtueller / realer rume ( sequence virtual / real rooms ) beschreibung virtuell raum clinical target volume ( ctv ) definieren definition des zielvolumens ( arzt ) computertomographie ( ct ) bestrahlungsplanung ( bpl ) bpl - analysis ( pla ) bpl - dokumentation ( tdk ) planungs - ct ( mtra , arzt ) physikalische bestrahlungsplanung ( physiker ) analyse des plans ( arzt ) dokumentation der bestrahlungsplanung ( physiker , mtra ) simulation ( mtra , arzt ) 1 . 
plankontrolle ( physiker ) einstellung / bestrahlungsbeginn ( arzt , mtra ) bestrahlungsbehandlung ( mtra , arzt ) bestrahlungsbehandlung ( mtra , arzt ) bestrahlungsbehandlung ( mtra , arzt ) lokalkontrolle ( arzt ) weitere bestrahlungsbehandlungen / lokalkontrollen ( arzt , mtra ) letzte bestrahlungsbehandlung ( mtra , arzt ) smtliche beteiligten berufsgruppen ( rzte , physiker , planungs - mtras ) wurden eingehend auf die neue arbeitsweise geschult . 
3 wochen schulung und diversen probelufen kam das system in den routineeinsatz . die bas - ag fungierte dabei in allen fragen als stndiger ansprechpartner und sorgte , vor allem in der anfangsphase , fr schnelle abhilfe bei problemen . ergebnisse / diskussion die integration der bestrahlungsplanung in den digitalen workflow konnte in der klinik fr strahlenheilkunde erfolgreich abgeschlossen werden und die implementierten prozesse befinden sich mittlerweile seit ca . 
 die sicherheit und datenschutzkonforme speicherung / archivierung der daten sind durch ein modernes hardund softwarekonzept gewhrleistet . fr die erfolgreiche umsetzung des projekts war neben dem umfassenden einsatz eines edv - systems ( bas ) die arbeit der interdisziplinr besetzten basag eine unerlssliche voraussetzung . durch das beschriebene verfahren wurde eine erhebliche verbesserung der transparenz und straffung der arbeitsablufe erreicht , weil sowohl die medizinisimulator ( sim ) physik 1 . 
kontrolle ( ph2 ) linearbeschleuniger ( cli5 ) linearbeschleuniger ( cli5 ) linearbeschleuniger ( cli5 ) linearbeschleuniger ( cli5 ) linearbeschleuniger ( cli5 ) linearbeschleuniger ( cli5 ) linearbeschleuniger ( cli5 ) ne bilderwahl zu einem bestimmten patienten getroffen hat , versendet er seine anforderung einfach und bequem ber dieses web - portal . 
dieses nach auen hin einfach wirkende webportal verfgt ber multiple funktionen , untersttzt noch verschiedene andere vorgnge und wird in einem separaten beitrag verffentlicht werden . nach der implementierung in einer originalgetreuen testumgebung wurden die funktionalitt und qualitt des verfahrens genau berprdanach wurde es in einer beta - umgebung erfolgreich auf routinetauglichkeit getestet und der zustndigen behrde ( in unserem falle das regierungsprsidium freiburg ) zur validierung bergeben . 
 weiterhin wurden alle relevanten prozesse und arbeitsanweisungen nach den formellen vorgaben unseres klinikweiten qualittsmanagementsystem ( ktq ) dokumentiert und sind im qm - handbuch jederzeit und von jedem mitarbeiter elektronisch einsehbar . schen als auch administrativen informationen an allen relevanten arbeitspltzen online zur verfgung stehen und neben den anderen berufsgruppen vor allem der rzteschaft die tgliche arbeit erheblich erleichtern . 
da immer klar ersichtlich ist , wer wann , wie und was am gesamtprozess ( mit ) gestaltet hat und in welchem prozessabschnitt sich ein patient gerade befindet , sind ansprechpartner leicht zu erkennen und knnen ohne lstiges und zeitraubendes suchen kontaktiert werden . 
diese integration schafft zudem auch nennenswerte freirume fr die mitarbeiter , da die prozessbeteiligten innerhalb bestimmter grenzen , bei vollem zugriff auf alle relevanten daten , sowohl bearbeitungsort als auch - zeit fast beliebig frei whlen knnen . 
unser meldeportal im intranet zur weiteren optimierung unserer arbeitsablufe bei . ein weiterer wesentlicher vorteil , der durch die digitale und strukturierte verfgbarkeit der fr die bestrahlungsplanung relevanten daten entsteht , wird an der mglichkeit , die gespeicherten informationen wissenschaftlich und konomisch - statistisch zu verarbeiten , sehr gut sichtbar ; denn man erhlt sowohl die leistungszahlen / - zeiten als auch die medizinischen bzw . 
wolff d , stieler f , hermann b et al ( 2010 ) clinical implementation of volumetric intensity - modulated arc therapy ( vmat ) with ergo + +  . 
boda - heggemann j , fleckenstein j , lohr f et al ( 2011 ) multiple breath - hold cbct for online im age guided radiotherapy of lung tumors : simula tion with a dynamic phantom and first patient data . 
strahlenther onkol 188 : 499506 116 | strahlentherapieundonkologie22013 literatur kommentiert strahlenther onkol 2013 189 : 163165 doi 10.1007 / s00066 - 012 - 0268 - z online publiziert : 9 . 
dezember 2012 springer - verlag berlin heidelberg 2012 s.e.combsj.werner abteilung radioonkologie und strahlentherapie , universittsklinikum heidelberg resektionplusadjuvante chemotherapieverbessert berlebenbeimfortgeschrittenen pankreaskarzinom originalpublikation ren f , xu yc , wang hx et al ( 2012 ) adjuvant chemotherapy , with or without postoperative radiotherapy , for resectable advanced pancreatic adenocarcinoma : continue or stop ? pancreatology 12 : 162169 fragestellung  . 
in 10 dieser studien wurde die adjuvante chemotherapie evaluiert ; 8 studien verglichen eine adjuvante chemotherapie mit einer postoperativen waitand - see - strategie und jeweils 2 studien eine gemzitabin - monotherapie mit einer polychemotherapie . 
hierbei wurde in 2 arbeiten eine chemotherapie mit einer radiochemotherapie verglichen , und in 3 arbeiten eine adjuvante radiochemotherapie mit einer wait - and - see - strategie postoperativ evaluiert . 
die adjuvante radiochemotherapie verlngerte im vergleich zur alleinigen resektion das mediane gesamtberleben ( or 0 , 99 ; p = 0 , 93 ) , das krankheitsfreie berleben ( or 0 , 99 ; p = 0 , 95 ) sowie das 2 - jahres - berleben ( or 0 , 90 ; p = 0 , 57 ) nicht . 
 darber hinaus zeigte die analyse , dass eine monotherapie mit gemcitabine einer kombinationschemotherapie nicht unterlegen ist ( gesamtberleben : or 1 , 13 ; p = 0 , 23 ; krankheitsfreies berleben : or 1 , 08 ; p = 0 , 47 )  . 
die vorliegenden daten untersttzen einen einsatz der radiochemotherapie in dieser klinischen situation nicht . kommentar der stellenwert der chemotherapie und / oder radiochemotherapie bei der behandlung des pankreaskarzinoms ist immer wieder gegenstand kontroverser diskussionen . 
eine komplette resektion ist voraussetzung einer kurativen therapie und sollte bei allen patienten durch erfahrene teams interdisziplinr evaluiert werden [ 2 , 3 , 4 , 5 , 6 ]  . bei patienten mit operablen pankreaskarzinomen ist die adjuvante chemotherapie standard und die datenlage eindeutig . 
in zwei randomisierten phase - iii - studien sowie in einer metaanastrahlentherapieundonkologie22013 | literatur kommentiert lyse zeigt sich das verbesserte langzeitberleben durch eine adjuvante chemotherapie im vergleich zur alleinigen resektion [ 8 , 9 , 10 ]  . 
da das auftreten eines lokalrezidivs die lebensqualitt der patienten deutlich einschrnken kann , sollte die adjuvante chemotherapie grozgig , auch bei lteren patienten und patienten in reduziertem allgemeinzustand indiziert werden . 
die adjuvante chemotherapie ist als monotherapie mit gemcitabine oder 5 - fu / leokovorin gleichwertig ( espac - 3 ) , wobei gemcitabine das nebenwirkungsrmere medikament und deshalb der am weitesten verbreitete standard ist [ 8 ]  . 
kombinationstherapien bringen im vergleich zu den monotherapien keinen vorteil , sind aber deutlich toxischer und deshalb in der regel nicht indiziert [ 8 ]  . im gegensatz zur adjuvanten chemotherapie ist eine adjuvante radiochemotherapie nicht als standard zu empfehlen [ 8 ]  . 
auf basis metaanalysierter daten sowie der espac - 1 - studie wird deutlich , dass kein signifikanter vorteil durch eine adjuvante radiochemotherapie beim pankreaskarzinom zu erwarten ist [ 9 , 11 ]  . 
ltere daten zur alleinigen strahlentherapie schienen hier zwar einen vorteil im berleben zu zeigen [ 12 ] , groe studien zeigten jedoch keinen vorteil gegenber einer alleinigen chemotherapie [ 9 , 13 ]  . 
nach inkompletter resektion , erwogen werden . komplexer sind die aktuellen behandlungsalgorithmen bei lokal fortgeschrittenen , inoperablen patienten , bei denen eine primre kurative resektion aufgrund der ummauerung vitaler gef und nervenstrukturen nicht mglich ist . 
das gewebe ist noch nicht durch eine operative intervention manipuliert worden , und die anatomischen strukturen sind unverndert sowie die oxygenierung des tumors ausreichend , da keine devaskularisationszonen durch eine chirurgische intervention generiert worden sind . 
ein groteil der patienten wrde nmlich durch die zeitliche verzgerung der kurativen chirurgischen therapie dieser dann nicht mehr zugefhrt [ 5 ]  . im gegensatz hierzu belegt eine reihe klinischer studien einen deutlichen vorteil der properativen therapie bei primr inoperablen , lokal fortgeschrittenen pankreaskarzinomen . 
 [ 6 ] konnten 111 studien identifiziert werden , die zwischen 1966 und 2009 publiziert wurden und sich auf neoadjuvante radiochemotherapie , radiotherapie oder chemotherapie zur behandlung von pankreaskarzinompatienten fokussierten . 
ein weiteres review aus dem jahr 2010 von morganti und kollegen identifizierte 13 studien mit insgesamt 510 patienten mit lokal fortgeschrittenen pankreaskarzinomen , bei denen eine neoadjuvante radiochemotherapie evaluiert wurde [ 15 ]  . 
bei diesen patienten verlngerte sich das berleben im median von 10 monaten auf 23 , 6 monate und entsprach somit den ergebnissen nach primrer resek tabilitt [ 2 , 8 , 9 , 10 ]  . 
ren f , xu yc , wang hx et al ( 2012 ) adjuvant chemotherapy , with or without postoperative radiotherapy , for resectable advanced pancreatic adenocarcinoma : continue or stop ? pancreatology 12 : 162169 2 . 
hartwig w , werner j , buchler mw ( 2012 ) prognosis of resected pancreatic cancer : is the refined resection margin status dispensable ? langenbecks arch surg 397 : 859860 3 . 
gillen s , schuster t , meyer zum bc et al ( 2010 ) preoperative / neoadjuvant therapy in pancreatic cancer : a systematic review and meta - analysis of response and resection percentages . 
oettle h , post s , neuhaus p et al ( 2007 ) adjuvant chemotherapy with gemcitabine vs observation in patients undergoing curative - intent resection of pancreatic cancer : a randomized controlled trial . 
klinkenbijl jh , jeekel j , sahmoud t et al ( 1999 ) adjuvant radiotherapy and 5 - fluorouracil after curative resection of cancer of the pancreas and periampullary region : phase iii trial of the eortc gastrointestinal tract cancer cooperative group . 
radiat oncol 7 : 28 strahlentherapieundonkologie22013 | original article strahlenther onkol 2013 189 : 142146 doi 10.1007 / s00066 - 012 - 0240 - y received : 6 july 2012 accepted : 17 september 2012 published online : 21 . 
dezember 2012 springer - verlag berlin heidelberg 2012 o.j.ottc.jeremiasu.s.gaiplb.freym.schmidtr.fietkau department of radiation oncology , university hospital erlangen radiotherapyfor achillodynia resultsofasingle - centerprospective randomizeddose - optimizationtrial achillodynia is a general term for various diseases causing heel pain including , for example , paratenonitis , tendinitis , tendinitis with partial rupture , insertional tendinitis , subachilles and retroachilles bursitis , haglunds deformity , and calcaneal spur . 
typical histological findings , usually 24 cm cranial to the calcaneus , are collagen fiber disorientation without accompanying inflammatory cells , hypocellularity , rarefied blood vessels , necroses , calcification , low perfusion levels , tissue hypoxia , and insufficient cell nutrition [ 3 ]  . achillodynia is more common in males and usually appears after the age of 30 . 
 in the postacute phase , physiotherapeutic approaches such as stretching , muscle de tonization , massages , and ultrasound treatments are recommended [ 3 ]  . for decades , radiotherapy has been successfully applied in the treatment of benign hyperproliferative and degenerative diseases [ 4 , 5 , 6 , 8 , 10 ] including achillodynia [ 15 ] ; however , contrary to painful shoulder or elbow syndrome , clinical outcome data after radiotherapy for achillodynia are very rare , and an optimal radiotherapy regimen is still not clear . 
for the treatment of inflammatory degenerative diseases , single doses of 0.51.0 gy and total doses of 36 gy per series are generally accepted [ 11 , 16 ]  . pain in achillodynia mainly results from inflammation of the achilles tendon or the bursa . 
additional information on patient and treatment characteristics can be found in .tab.1. patients and methods treatment between february 2006 and february 2010 , a total of 116 consecutive patients with achillodynia were treated at the erlangen university hospital . 
 at the time of radiotherapy , the mediall patients underwent radiotherapy with an orthovoltage technique ( siemens stabilipan , 180 kv , 20 ma , 0.2 mm cu filter , focus - skin distance 40 cm ) usually with a single field of 68 cm positioned directly on the achilles tendon insertion area including the distal part of the tendon . 
 rr response rate , cr complete response , pr partial response , nc no change of 6 single fractions delivered in 3 weeks with an interfractional radiation - free interval of 2 days at least . 
pain levels were measured with a standardized questionnaire immediately before and after each radiation treatment , especially right after ( early response ) and during a follow - up visit 6 weeks after completion of radiotherapy ( delayed response )  . 
the pain level was determined using a graphic visual analogue scale ( vas ) with levels from 0 ( no pain ) to 100 ( maximum conceivable pain ) and a modified von pannewitz pain score [ 19 ] adapted from seegenschmiedt and keilholz [ 16 ]  . 
using this score , the treatment response was evaluated with regard to pain symptoms grouped into five categories ( pain at strain , pain at night , persistent pain during daytime , pain at rest , and morning stiffness ) and four grades ( none = 0 points , mild = 1 point , moderate = 2 points , and severe = 3 points )  . 
for statistical comparisons between groups , the mannwhitney u test and pearsons chi - square test were used . strahlentherapieundonkologie22013 | original article abstract zusammenfassung results strahlenther onkol 2013 189 : 142146 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0240 - y the gender distribution of the 112 evaluated patients was 52% ( 58 / 112 ) male and 48% ( 54 / 112 ) female . 
the results of our trial with early and delayed response rates of 84% and 88% are clearly comparable to the results after radiotherapy for other benign degenerative conditions such as calcaneodynia [ 7 ] , painful elbow [ 12 , 16 ] and shoulder syndrome [ 1 , 16 ]  . 
an important finding of our trial is that the response rate ( especially cr ) significantly improved from the end of the treatment ( early response ) to the follow - up examination 6 weeks after completion of radiotherapy ( delayed response )  . 
 [ 7 ] reported on a comparable trial of 130 patients with painful heel spurs that were randomized to receive either single doses of 0.5 gy to a total dose of 3.0 gy over 3 weeks ( low - dose group ; n = 65 ) or single doses of 1.0 gy to a total dose of 6.0 gy over 3 weeks ( high - dose group ; n = 65 )  . 
in 18% ( 24 / 130 ) of cases in the high - dose group and 13% ( 17 / 130 ) of cases in the low - dose group , a second radiotherapy series was performed . 
in 341 patients ( 68% ) , radiotherapy was performed twice a week with a single 610 - mv photon field , while in 161 patients ( 32% ) it was performed three times a week with a single 175 - kv x - ray field . 
pain measurement was performed with the von pannewitz score [ 19 ] , and 61% of the treated patients were still satisfied with the therapeutic effect of the radiation treatment . 
 [ 17 ] compared the clinical effect of three different dose concepts in the radiotherapeutic treatment of painful heel spurs : group a ( n = 72 ) received 12 gy total radiation dose in 3 fractions per week and in 2 series ( 61 gy / series ) separated by 6 weeks ; group b ( n = 98 ) received 3 gy total radiation dose in 10 fractions of 0.3 gy ( n = 50 ) or 5 gy ( 100.5 gy ; n = 48 ) with conventional fractionation in 1 series . 
radiotherapy was very effective : at the last followup , 67% ( group a ) and 71% ( group b ) of patients remained completely free of pa the cr rate was not different between the three radiation concepts . 
more favorable results were achieved in patients receiving a total dose of 5 gy or 12 gy , while patients with a total dose of 3 gy had significantly worse results . 
although tumor induction by ionizing radiation is still under critical discussion [ 18 ] , there are no publications of significant numbers of patients with tumors resulting from radiostrahlentherapieundonkologie22013 | original article early response delayed response fig . 
 in many cases , irradiation with 0.5 gy induced the strongest anti - inflammatory phenotype of the cells , including macrophages , granulocytes , lymphocytes , and endothelial cells [ 13 ]  . 
irradiation of human tnftransgenic mice , who develop severe polyarthritis , with 5 fractions of 0.5 gy led to significantly temporal improved clinical symptoms such as a reduced paw swelling and increased grip strength [ 2 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 166167 doi 10.1007 / s00066 - 012 - 0280 - 3 online publiziert : 12 . 
dezember 2012 springer - verlag berlin heidelberg 2012 c.rdel1g.klautke2 1 klinik fr strahlentherapie und onkologie , universitt frankfurt 2 bamberg lokalekontrollebei t3 - rektumkarzinomen kurzzeitbestrahlungversus radiochemotherapie originalpublikation ngan sy , burmeister b , fisher rj et al ( 2012 ) randomized trial of short - course radiotherapy versus long - course chemoradiation comparing rates of local recurrence in patients with t3 rectal cancer : trans - tasman radiation oncology group trial 01.04. 
bei primr resektablen rektumkarzinomen im uicc - stadium ii und iii verbessern sowohl die properative kurzzeitbestrahlung als auch die radiochemotherapie ( rct ) die lokale kontrolle im vergleich zur alleinigen totalen mesorektalen exzision ( tme )  . 
in die studie wurden patienten mit einem histologisch gesicherten rektumkarzinom bis 12 cm ab anokutanlinie eingeschlossen , die auf grundlage der mrt und / oder endosonographie einen ct3nxm0 - tumor aufwiesen . 
randomisiert wurde zwischen einer kurzzeitbestrahlung mit 5 - mal 5 gy , gefolgt von einer operation nach 37 tagen und einer rct ( 1 , 845 gy + 5 , 4 gy boost ; 5 - fu 225 mg / m2 / tag whrend der gesamten rt ) , gefolgt von einer operation nach 46 wochen . 
alle patienten erhielten eine adjuvante chemotherapie mit 5 - fu ( 425 mg / m2 ) und folinsure ( 20 mg / m2 ) ber 5 tage , 6 kurse im arm der kurzzeitbestrahlung ( rt ) und 4 kurse im arm der rct . 
ein pathologisches downstaging konnte in 45% im arm der rct und in 28% bei der kurzzeit - rt erreicht werden ( p = 0 , 002 ) , eine pcr ( pathologisch besttigte komplettremission ) wurde bei 20 / 157 ( 13% ) in der rct - gruppe erzielt . 
die lokoregionre rezidivrate lag im gesamtkollektiv nach 3 jahren bei 4 , 4% im rct - arm und bei 7 , 5% im kurzzeit - rt - arm ( 95% - konfidenzintervall 2 , 18 , 3% ; p = 0 , 24 )  . 
 fr patienten mit tumoren im distalen drittel ( hier definiert als < 5 cm entfernt von der anokutanlinie ) lag die kumulative inzidenz von lokoregionren rezidiven bei 12 , 5% im kurzzeit - rt - arm und bei 0% im rct - arm ( p = 0 , 21 )  . 
die fernmetastasierungsrate nach 5 jahren war in beiden armen nicht signifikant unterschiedlich ( 27% nach kurzzeit - rt , 30% nach rct ; p = 0 , 89 )  . 
allerdings ergab sich ein vorteil von 3 , 1 prozentpunkten zugunsten der rct , der es bei einem 95% - konfidenzintervall zwischen 2 , 1% und 8 , 3% nicht erlaubt , einen klinisch relevanten vorteil der rct gegenber der kurzzeit - rt auszuschlieen . kommentar die studie der trans - tasman radiation oncology group hatte ein sehr ambitioniertes ziel , nmlich einen unterschied von 10% bei der lokoregionren kontrollrate nach 3 jahren zwischen den zwei properativen rt - regimen nachzuwei166 | strahlentherapieundonkologie22013 5 . 
bujko k , nowacki mp , nasierowska - guttmejer a et al ( 2006 ) long - term results of a randomized trial comparing preoperative short - course radiotherapy with preoperative conventionally fractionated chemoradiation for rectal cancer . 
die annahme , dass bei t3 - tumoren nach 5 - mal 5 gy und optimierter tmechirurgie tatschlich lokoregionre rezidive in einer grenordnung von 15% nach 3 jahren auftreten wrden , ist aus der aktuellen literatur [ 2 ] nicht ableitbar und wohl eher der notwendigkeit geschuldet , die zu rekrutierende patientenzahl auf ein realistisch zu erreichendes ziel zu reduzieren . immerhin konnte die studie einen unterschied von 3 , 1% zugunsten der rct zeigen , was wie die autoren in ihrer diskussion auch konzedieren bei der hier eingeschlossenen patientenzahl und dem weiten 95% - konfidenzintervall eine hhere effektivitt der rct gegenber der kurzzeit - rt nicht ausschliet . 
 interessant ist in diesem zusammenhang die explorative subgruppenanalyse der tiefsitzenden tumoren ( < 5 cm ab anokutanlinie ) : in der kurzzeit - rt - gruppe traten 6 lokoregionre rezidive bei 48 patienten auf , nach rct nur eines bei 31 patienten ( p = 0 , 26 )  . 
dies untermauert erneut die auch in unseren s3 - leitlinien zur behandlung des kolorektalen karzinoms beschriebene empfehlung , bei tiefsitzenden tumoren die properative rct gegenber der kurzzeit - rt zu prferieren [ 3 ]  . interessant ist der vergleich dieser studie mit der 2004 publizierten polnischen studie mit hnlichem design [ 4 ]  . 
 dort waren 316 patienten mit digital - rektal tastbaren t3 / 4 - tumoren eingeschlossen worden und entweder mit 5 - mal 5 gy oder mit 5 - fu - basierter rct vor operation behandelt worden . 
 berraschenderweise lag die kumulative inzidenz von lokalrezidiven in dieser studie ( hier allerdings als sekundrer endpunkt ! ) nach 4 jahren mit 15 , 6% nach rct um 5 prozentpunkte hher als nach 5 - mal 5 gy ( 10 , 6% ; p = 0 , 21 ; [ 5 ] )  . 
bercksichtigt man , dass in der polnischen studie die compliance im rct - arm nur 69% betrug ( 98% im arm mit 5 - mal 5 gy ) , die operation nicht standardisiert erfolgte und eine adjuvante chemotherapie nicht teil des protokolls war , ist die behandlungsqualitt der trans - tasman radiation oncology group 01.04 deutlich besser und erlaubt daher eher rckschlsse auf die ( biologische ) effektivitt der verglichenen therapieregime . 
ngan sy , burmeister b , fisher rj et al ( 2012 ) randomized trial of short - course radiotherapy versus long - course chemoradiation comparing rates of local recurrence in patients with t3 rectal cancer : trans - tasman radiation oncology group trial 01.04. 
schmiegel w , pox c , reinacher - schick a et al ( 2010 ) s3 guidelines for colorectal carcinoma : results of an evidence - based consensus conference on february 6 / 7 , 2004 and june 8 / 9 , 2007 ( for the topics iv , vi and vii )  . 
bujko k , nowacki mp , nasierowska - guttmejer a et al ( 2004 ) sphincter preservation following preoperative radiotherapy for rectal cancer : report of a randomised trial comparing short - term radiotherapy vs . 
radiother oncol 72 : 1524 die in der rubrik literatur kommentiert seit 2010 erschienenen beitrge sind online verfgbar unter strahlentherapieundonkologie22013 | mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 170172 doi 10.1007s00066 - 012 - 0295 - 9 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen adressen deutsche gesellschaft fr radioonkologie e.v. , deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie , lk salzburg universittsklinikum , mllner und radio - onkologie salzburger landeskliniken und paracelsus medizinische hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , fax - 887 telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , scientific association of swiss radiation oncology , pd damien c . 
weber , service de radio - oncologie , hpital cantonal universitaire , ch 1211 genve hpital cantonal universitaire , ch 1211 genve hungarian society of radiation oncology , hungarian society of radiation oncology , a . 
29 , h - 1145 budapest , telefon ( + 36 / 1 ) 251 - 1471 , fax - 1478 , e - mail : mayera@hu.inter.net e - mail : mayera@hu.inter.net deutsche gesellschaft fr medizinische physik , deutsche gesellschaft fr medizinische physik , p . 
kneschaurek , klinik fr strahlentherapie der technischen universitt , klinikum rechts der isar , ismaninger strae 22 , universitt , klinikum rechts der isar , ismaninger strae 22 , d - 81675 mnchen , telefon ( + 49 / 89 ) 4140 - 4504 , fax - 4881 d - 81675 mnchen , telefon ( + 49 / 89 ) 4140 - 4504 , fax - 4881 hellenic society of radiation oncology , hellenic society of radiation oncology , p . 
4446 , gr - 10676 athen , telefon / fax ( + 30 / 1 ) 7244117 telefon / fax ( + 30 / 1 ) 7244117 romanian society of radiotherapy and medical oncology , romanian society of radiotherapy and medical oncology , n . 
 es handelt sich um den hermann - holthusen - preis , alfred - breit - preis , dissertationspreis , innovationspreis , preis zur hochprzisions - strahlentherapie , gnther - von - pannewitz - preis sowie den koester - preis . informationen : anmeldung : 170 | strahlentherapieundonkologie22013 personalia alfred - breit - preis2013 roch kowalski , beraus geschtzter leitender oberarzt der klinik fr strahlentherapie im malteser - krankenhaus st . 
volker diehl 75 jahre der / die verantwortliche bewerber / in adressiert die arbeit in sechsfacher ausfertigung inklusive zusammenfassung , kopie der publikation ( en ) , des patentes bzw . 
mrz 2013 an die deutsche gesellschaft fr radioonkologie prsident jgen dunst hindenburgdamm 30 12200 berlin zum zweiten mal schreibt die degro den von ihrem verstorbenen mitglied professor alfred breit gestifteten preis aus . 
 mit dem preis in hhe von 20.000 ehrt die degro das lebenswerk von alfred breit , der sich besondere verdienste auf dem gebiet der ctund mrtgesttzten strahlentherapie - planung erworben hat . 
als grundlage zur entscheidung fr die preisvergabe dienen publikationen oder patente , aber auch verfahren , die sich in der klinik etabliert haben , ohne dass sie publiziert worden sind . 
die preis - arbeit kann in deutscher oder englischer sprache verfasst sein . strahlentherapieundonkologie22013 | editorial strahlenther onkol 2013 189 : 105110 doi 10.1007 / s00066 - 012 - 0299 - 5 published online : 10 . 
adjuvant radiotherapy ( rt ) with or without chemotherapy ( cht ) reduced local recurrence and became a standard treatment in the 1980s [ 14 ] , which was later on gradually replaced by preoperative rt ( nrt ) [ 9 , 45 ] or neoadjuvant radiochemotherapy ( nrct ) [ 3 , 4 , 10 , 34 , 37 ]  . 
the next step was the introduction of magnetic resonance imaging ( mri ) as a routine preoperative staging tool [ 1 ] facilitating the visualization of the distance between tumor and mesorectal fascia . 
a negative crm ( defined as 1 mm on pathological work - up ) has consecutively been identified and validated as an important surrogate parameter to predict the individual lr risk [ 12 ]  . 
results of the mercury study group ( magnetic resonance imaging in rectal cancer european equivalence study ) whose authors propagated and investigated mri - based treatment for rectal cancer were encouraging [ 23 , 43 ] and promoted similar attempts in the german - speaking community such as the ocum study ( optimized surgery and mri - based multimodal therapy of rectal cancer )  . 
preliminary results were recently published [ 22 , 42 ] and are commented in this editorial . altogether , 230 patients with rectal cancer clinically staged as ct24 , any cn , cm0 were included in this observational study . 
the anticipated crm assessed by mri ( mrcrm ) was used as a decision tool for selecting patients ( n = 230 ) either to undergo primary surgery ( n = 134 ) or to receive nrct ( n = 96 )  . 
for the lower third of the rectum ( defined as < 6 cm from the anal verge , 37% ) , nrct was performed in all ct3 and ct4 tumors , irrespective of the anticipated crm status ; tumors of the middle third ( i.e. , 6 to < 12 cm ) were treated by nrct in case of positive mrcrm only . 
clinically positive lymph nodes did not influence the choice of therapy ; in patients with pathologically positive lymph nodes , chemotherapy was offered according to the standard of the respective centers . 
postoperative rct was restricted to patients with an involved crm ( pcrm 1 mm ) [ 42 ]  . the mrcrm was positive in 74 / 230 patients , 72 in the nrct group and 2 of the patients selected for surgery alone . 
 the authors concluded despite the negative selection of locally advanced rectal cancer cases for nrct , impressive rates of tumor downstaging and eradication of tumor from the mesorectal fascia were achieved . 
moreover , this selective use of nrct spared a considerable percentage of patients with stage ii / iii rectal cancer severe irradiation toxicity [ 22 ]  . what is an acceptable rate of local recurrence ? it is beyond dispute that unnecessary costs and toxicity should be minimized ; however , the question remains to what extent this potential sparing is justified at the expense of an increased lr riskin relation to the achievable local control . 
summarizing the results from recent randomized trials , the addition of radiotherapy to the multimodal concept provides a 5 - year lostrahlentherapieundonkologie22013 | editorial coregional recurrence rate ( lrr ) of only of 58% and < 5% in low risk rectal cancer [ 37 , 40 , 45 ]  . 
a similar threshold is suggested by glimelius [ 11 ] who regards an expected lrr of less than 10 percent ( i.e. , 10% is too much ! ) as appropriate to qualify for a favourite risk group that may justify omission of radiotherapy . 
under these assumptions , several requirements result for clinical studies : f the 5 - year local recurrence rate is the decisive endpoint for estimating the relevance of data from clinical studies proposing surgery alone in stage ii / iii patients . 
surrogate parameters , such as a negative crm , cannot replace this endpoint ; f the noninferiority of surgery alone can not be presumed unless the expected 5 - year lrr is 58% , whereas any excess of this range renders the study design inacceptable ; f unless a publication explicitly specifies 5 - year lrr ( as in the commented papers ) [ 22 , 42 ] , results are not exploitable for clinical decisions ; and f the omission of radiotherapy needs to be explored in a radomized trial before recommendations for treatment can be adopted into clinical practice . can mri predict prognosis ? striving for a more risk - adapted use of nrct , hermanek et al . 
 [ 18 ] published a proposal for an mri - guided treatment decision on the basis of a risk estimation for local recurrence in stage ii / iii patients after guideline - adherent versus mribased selection for ncrt . 
he assumed a local recurrence rate ( lrr ) of 6% after conventional nrct , according to the data of the cao / aro / aio - 94 trial [ 37 ]  . 
for mri - based treatment he calculated a 5% increase of the absolute risk of lr for best case , i.e. , specialized centers and 12% in worst case , i.e. , institutions with lower quality of mri and less expertise in terms of achieving an optimal plane of surgery . the attempt to use mri to optimize preoperative diagnostic work - up was extensively investigated by the mercury 106 | strahlentherapieundonkologie22013 study group who demonstrated the diagnostic accuracy of mri in patients who were either primarily operated or underwent nrct according to the predicted crm [ 29 , 43 ]  . 
of 374 patients followed up in the mercury study , 122 were preoperatively diagnosed as good prognosis group if the following criteria were met : a negative crm predicted in mri , no evidence of extramural venous invasion , as well as an early t - category , i.e. , t2 / t3a / t3b ( no perirectal fat invasion or < 5 mm spread from muscularis propria )  . 
moreover , 57 of those 122 patients ( 47% ) had clinical stage i tumor and would not have received nrct according to current guidelines anyway , and 40 patients ( 33% ) had tumors in the upper third of the rectu the remaining 65 patients of those 122 patients accounted for stage cii ( n = 43 ) / ciii ( n = 22 )  . 
in any case , the quantity of only 65 patients with stage ii and iii disease being relevant for the question ( among those also patients with upper rectal cancer ! ) whether the conventionally indicated radio ( chemo ) therapy can be safely omitted is too small to draw any reliable conclusions . 
thus , despite promising results , this analysis does not provide unequivocal evidence for the appropriateness of using mrcrm as a sole criterion for further treatment choice . does crm predict futility of further treatment ? in this regard it is interesting to analyze the lrr of a risk adapted treatment published to date , such as the britishcanadian multicentre study ( mrc c07 and ncic - ctg c016 ) [ 40 ] that investigated the effect of omitting radiotherapy . 
overall , 1350 patients with resectable rectal cancer ( stage iiii ) were randomized for either preoperative rt or primary surgery with selective postoperative rct , the latter restricted to only those patients whose pathology revealed a distance between tumor and mesorectal fascia of < 1 mm , i.e. , a positive circumferential resection marg mri was not routinely performed and formal training for surgeons had not yet been implemented . 
of the 676 patients randomized for primary surgery , 77 ( 12% ) had a positive crm , 53 patients received rct , and 7 patients rt alone ; additional adjuvant cht was used in 40% with stage ciii in both arms . 
 [ 31 ] , one of the protagonists of the mercury project , analyzed the impact of the plane of surgery in the above described trial [ 40 ] and found that , in multivariate analysis , crm was not predictive for lr . additional information about the impact of treatment in relation to crm can be derived from the 12 - year follow - up analysis of the dutch randomized tme trial [ 45 ]  . 
especially those 81% of patients with a pathologically negative crm experienced benefit from preoperative rt : a reduced 10 - year lrr was observed throughout all stages ( p < 0.0001 ) : f stage ci : 1% vs . 
3% , f stage cii : 4% vs.7% , and f stage ciii : 5 vs.17%. noteworthy , about 10% of the local recurrences occurred beyond 5 years , indicating the necessity of a longer follow - up . 
when is the local recurrence risk low enough to refrain from the aim to prevent it ? abstract recently , preliminary results of the ocum study ( optimized surgery and mri - based multimodal therapy of rectal cancer ) were published and raised concern in the scientific community . 
in this observational study , the circumferential resection margin status assessed in preoperative mri ( mrcrm ) was used to decide for either total mesorectal excision ( tme ) alone or neoadjuvant radiochemotherapy ( nrct )  . 
recurrence rates have not yet been reported , but an impressive rate of downstaging for both t and n stage after nrct was observed , while acute side effects were minimal . 
this is based on the hypothesis that crm is a valid surrogate parameter for the risk of local recurrence and in case of a negative crm , nrct becomes dispensable . 
 as 5 - year locoregional recurrence rate ( lrr ) of only of 58% and < 5% in low risk rectal cancer can be achieved by the addition of rt , the noninferiority of surgery alone can not be presumed unless the expected 5 - year lrr is 58% , whereas any excess of this range renders the study design inacceptable . 
unless a publication explicitly specifies 5 - year lrr , results are not exploitable for clinical decisions . keywords surgery radiation therapy neoadjuvant therapy radiochemotherapy treatment outcome rektumkarzinowann ist das lokalrezidivrisiko so niedrig , dass es nicht mehr beachtet werden muss ? zusammenfassung krzlich wurden vorlufige ergebnisse einer studie ber optimierte chirurgie und mrtbasierte multimodale therapie des rektumkarzinoms ( ocum ) publiziert , deren interpretation unter radioonkologen mit bedenken zur kenntnis genommen wurde . 
in dieser beobachtungsstudie wurde anhand des properativen mri der zu erwartende zirkumferentielle resektionsrand ( mrcrm ) bewertet und daraufhin die entscheidung getroffen , entweder eine alleinige totale mesorektale exzision ( tme ) oder eine neoadjuvante radiochemotherapie ( nrct ) durchzufhren . 
im gegensatz zu den geltenden leitlinien waren weder ein t3 - stadium ( mit negativem crm ) noch bildmorphologisch positive lymph knoten ( lk ) eine indikation zur neoadjuvanten therapie . 
dennoch kamen die autoren zu dem schluss , dass einer erheblichen anzahl von patienten die schwere radiotoxizitt erspart werden knne und sehen ihr konzept der mrcrm als option , zuknftig die indikationsstellung der leitlinien zu ersetzen . 
dem wird die hypothese zugrunde gelegt , dass der crm ein zuverlssiger surrogatparameter fr die vorhersage des lokalrezidivrisikos darstelle und im falle eines negativen crm , die neoadjuvante therapie entbehrlich sei . 
da in kombination mit der strahlentherapie 5 - jahres - lokalrezidivraten ( lrr ) von 58% , bei low - risk - patienten sogar von < 5% erzielt werden , ist zu fordern , dass eine gleichwertigkeit der alleinigen operation nur dann zu postulieren ist , wenn die zu erwartetende 5 - jahres - lrr ebenfalls 58% betrgt . 
 jedes berschreiten dieses schwellenwerts weist auf ein inakzeptables studiendesign hinsbesondere knnen nur dann klinische schlussfolgerungen aus einer studie gezogen werden , wenn die 5 - jahres - lrr angegeben werden . schlsselwrter operation strahlentherapie neoadjuvante therapie radiochemotherapie behandlungserfolg mercury study , disproving the assumption that the advent of proper tme may have overruled the significance of optimizing local control . intriguingly , in a recent methodological analysis of studies published on the accuracy of pretreatment mri to predict negative from positive crm in the operative specimen ( including the mercury data ) , the authors concluded that mri cannot predict tumour involvement of a crm [ 5 ]  . 
in contrast , the meta - analysis of al - sukhni assessed a specificity of 94% [ 1 ]  . is lymph node status no longer related to local failure risk in the era of tme ? the ocum study does not only omit nrct but replaces postoperative rct by chemotherapy alone in node - positive patients irrespective of the number of affected nodes [ 42 ]  . 
this is based on the hypothesis that tme provides complete restrahlentherapieundonkologie22013 | editorial moval of the lymphatic drainage upwards and therefore regional lymph nodes ( except , lateral pelvic nodes ) would no longer remain as origin of lr [ 17 ]  . in an article by hermanek et al . 
moreover , a recently published pooled analysis of five european randomized studies , comparing different preoperative radiotherapy schedules confirmed that lymph node status was a significant predictive factor not only for distant metastases and survival , but also for local recurrences [ 44 ]  . evidence further arises that rt may not only improve local control , but also increase survival , especially in node positive patients . 
in a further publication analyzing the plane of surgery in the mrccr07 patients , quirke described positive lymph nodes as the most important independent risk factor for local recurrence ( hr 1.78 , p < 0.0001 ; [ 31 ] )  . 
thus , the data of this trial suggest that chemotherapy alone is less effective for eradication of lymph node metastases , whereas rt halves the lrr in this subgroup . the strongest evidence for the impact of rt on prognosis in lymph node positive patients can be derived from the dutch tme trial : node - positive patients with a negative pcrm , treated with tme alone , had a 10 - year oas of 57% in stage ii vs . 
these findings indicate that even in the era of quality - assured tme , the negative impact of positive lymph nodes on local control and survival can , at least partly , be compensated by preoperative rt . these findings corroborate the hypothesis that improved local tumor control is not merely prevention of local re108 | strahlentherapieundonkologie22013 currence , but furthermore sterilization of subclinical disease and thus stopping metastases at their source [ 16 ]  . the concept of mri - based omission of preoperative rt in crm - negative patients irrespective of nodal status will exclude node - positive patients from any rt . 
 although the landmark cao / aro / aio94 trial demonstrated that postoperative rct is less effective and more toxic than preoperative rct [ 37 ] , it seems doubtful whether the total omission of rt can be compensated by adjuvant cht alone in stage iii patients . should the level of evidence be neglected ? the scandinavian surgical outcomes research group recently commented on controversies in rectal cancer management as follows : in surgery there is a tendency to disregard the normal scientific methods of evaluation , whereas in medicine it is fully established that a new drug cannot be used without formal assessment according to strict scientific principles [ 35 ]  . the authors of the ocum study [ 42 ] argue that guidelines are increasingly recommending mri as the basis for the indication of nrct even though a prospective study has not been conducted until now . actually , besides the german s3 guideline [ 38 ] , the recently updated european [ 39 ] , american [ 24 ] , canadian [ 7 ] , and english [ 25 ] guidelines indeed advocate mri use for preoperative staging but none of these guidelines recommends basing the further treatment decision on the mri prediction of a positive crm alone . even though the mercury data have brought promising perspectives for the management of rectal cancer , the question remains whether and how soon data from observational studies using a surrogate ( mrcrm ) of a surrogate parameter ( pcrm ) should be adopted into routine practice . 
observational data will not provide an equally solid level of evidence compared to those of randomized trials that built the background for current guidelines . it remains highly desirable to better select those patients for neoadjuvant treatment who are most likely to benefit and to consider primary surgery in subgroups with low anticipated risk factors [ 8 , 11 , 18 ]  . 
 on the other hand , additional risk features such as extramural vascular invasion [ 25 , 41 ] and mucinous carcinoma may contribute to the treatment decision [ 28 ]  . 
 a standardized international classification for the good , the bad , and the ugly [ 11 ] , i.e. , the different risk groups would be helpful to assure comparability of different treatment approaches and better outweigh risk reduction against side effects . 
innovative techniques such as intensity - modulated ( imrt ; [ 20 ] ) and image - guided ( igrt ; [ 13 ] ) radiotherapy will further permit adverse effects to be minimized . 
individual response and toxicity scores [ 47 ] may be another promising tool and new concepts for systemic treatment are warranted for patients at risk of distant metastases [ 6 , 33 , 34 , 46 ]  . doubtlessly , quality optimization of established procedures , such as high resolution mri or tme in the mesorectal plane , should promptly be translated into clinical routine . 
however , major changes of treatment that bear a potential risk of increasing recurrence should preferentially be evaluated in randomized trials , providing standardized specifications for each phase of treatmentand not leaving therapy to the discretion of the treating institution ! the disadvantage of such stricter rules may be a lower rate of accrual and thus a longer interval until results are available . 
 a major concern would be the uncritical adoption of a treatment requiring highest standards of quality - assured multimodal procedures outside specialized centers with trained and experienced teams [ 18 , 19 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . erratum strahlenther onkol 2013 189 : 168169 doi 10.1007 / s00066 - 012 - 0279 - 9 online publiziert : 20 . 
medical department , klinikum rechts der isar , technische universitt mnchen , munich erratumto : radiotherapyinstagei - iiifollicular non - hodgkinlymphoma.retrospective analysisofaseriesof50patients strahlentherapieundonkologie188 : 464471 theonlineversionoftheoriginalarticlecanbe foundatdoi10.1007 / s00066 - 011 - 0057 - 0 the authors regret two typing errors in the original publication . 
22 , 81675 munich germany khfmed@yahoo.com 168 | strahlentherapieundonkologie22013 dieses buch erfllt inhaltlich die kriterien eines lehrbuchs und darber hinaus wird der leser durch den spannenden schreibstil mit interessanten einleitenden kapiteln unter zuhilfenahme modernster didaktik zum durchlesen des gesamten buches von der ersten bis zur letzten seite verleitet . dieses lehrbuch ist fr fachrzte und weiterbildungsassistenten aller an der interdisziplinren therapie der krebserkrankungen im kindesalter geschrieben , und zwar der kinderonkologie , kinderchirurgie , radiologie und strahlentherapie  . christiane matuschek ( dsseldorf ) buchbesprechungen g.maio mittelpunkt mensch : ethik in der medizin ein lehrbuch stuttgart : schattauer 2012 424 seiten ( isbn 978 - 3 - 7945 - 2448 - 8 ) 24 , 95 eur u.wiesing ethik in der medizin ein studienbuch stuttgart : philipp reclam jun . 
125 kommentierten kurzbeitrgen ( isbn 978 - 3 - 15 - 018963 - 4 ) 14 , 80 eur buchbesprechungen zum thema ethik und medizin : ein lehrbuch ( hardcover ) und eine textsammlung ( paperback ) die konomische umformung in der medizin , der pluralismus von theorien / werten / normen oder lebensentwrfen , fragen der mittelverteilung , eigenverantwortung , sterbehilfe , forschung am menschen , tod und hirntod dies sind nur einige stichworte welche in beiden bchern sehr aktuell aber unterschiedlich behandelt werden . 
 interessant ist , dass in beiden bchern mehrfach eingehend auf die prinzipienorientierte medizinethik ( beauchamp und childress 2009 ) mit den vier gleichrangig verbindlichen prinzipien , nmlich patientenautonomie , nichtschaden , frsorge und gerechtigkeit eingegangen wird . 
 ( isbn 978 - 3 - 7945 - 2786 - 1 ) 199.00 eur das buch ist von einem autorenteam mit ausgewiesenen experten der jeweiligen kinderkrebserkrankungen geschrieben . durch die sehr ansprechend geschriebenen und illustrierten einleitenden kapitel ( epidemiologie und geschichte ) , wird der leser automatisch weiter durch das ganze buch gefhrt . 
inhaltlich soll das buch ein lehr und nachschlagewerk fr alle an der interdisziplinren zusammenarbeit beteiligten rzte sein . der strahlentherapeut , der das buch als nachschlagewerk fr indikation und bestrahlungsdosis benutzen mchte , findet jedoch nicht die detailinformationen zur bestrahlung . falls diese angaben nicht gegeben werden , damit der rahmen des buches nicht gesprengt wird und um den lehrbuchcharakter ber viele jahre , auch nachdem die studienprotokolle aktualisiert worden sind , aufrecht zu erhalten , htte man z.b. 
entwicklung der studien hingegen sind zum groben berblick und verstndnis sehr schn dargestellt . sehr positiv an dem buch ist hervorzuheben , dass die beigefgte dvd mit darstellung der verschiedenen operationsverfahren bei soliden tumoren im kindesalter einen einzigartigen einblick in die spezielle onkologische kinderchirurgie gibt . 
da dieses feature erst heutzutage mit der mglichkeit , daten komprimiert auf einer cd - rom abzuspeichern , mglich ist , wirkt das buch damit nicht nur inhaltlich , sondern auch unter formalen gesichtspunkten sehr modern . strahlentherapieundonkologie22013 | original article strahlenther onkol 2013 189 : 137141 doi 10.1007 / s00066 - 012 - 0269 - y received : 28 october 2012 accepted : 8 november 2012 published online : 20 . 
while radiosurgery is reserved for well - circumscribed , small lesions ( < 2.53 cm ) at a certain distance ( 23 mm ) to these structures [ 1 , 2 , 3 ] , conformal radiotherapy is an effective local treatment option for those lesions not fulfilling the above - mentioned criteria [ 4 , 5 , 6 ]  . 
it combines both fractionation and high - precision radiation delivery and thus has the potential to protect organs at risk without losing effectiveness , especially in benign brain tumors [ 10 , 11 ]  . patients and methods from 1993 to 2009 , 29 patients were treated with fractionated stereotactic radiotherapy . 
benign tumors ( grade i meningioma n = 11 , pituitary adenoma n = 10 , grade i suprasellar glioma n = 4 , craniopharyngioma n = 3 ) were the most frequent type . 
tumors were either treated without histopathological diagnosis ( 3 / 29 ) or after biopsy ( 4 / 29 ) or incomplete resection ( 20 / 29 , 69% )  . 
in 15 of 29 patients ( 52% ) , visual acuity or the visual field was impaired , and partial or global hypophyseal insufficiency was present in 8 of 29 ( 28% ) and 3 of 29 ( 10% ) patients before treatment . treatment comprised a linear accelerator ( 6 mev photons , sl25 , elekta ) equipped with a tertiary micro - multileaf collimator ( mrc / siemens , 280 leaves , projected width at isocenter 1.6 mm ) for 25 of 29 ( 86% ) patients or a cylindrical collimator ( leibinger ) for 4 of 29 patients ( 14% )  . 
treatment planning ( virtuoso / leibinger ) and delivery were performed in stereotactic coordinates supplied by the fisher / leibinger stereotactic system attached to the gtc frame by a special adapter plate . 
the gross tumor volume ( gtv ; macroscopic tumor ) was delineated on high - resolution ( 512512 pixels , 2 mm slice thickness ) contrast - enhanced t1weighted magnetic resonance ( mr ) images registered to the planning computer tomography ( ct ) scan by anatomical landmarks . 
any increase in visual acuity ( > 0.1 points ) and / or decrease in visual field defect was regarded as improvement of visual function , while any decrease in visual acuity ( > 0.1 points ) or new visual field defect was clas42 ( 873 ) 4 patients < 18 years 20 / 9 ( 69% / 31% ) 45 ( 10105 ) tab . 
1 patient characteristics age ( years ) gender ( female / male ) follow - up ( months ) tumortype meningioma grade i pituitary adenoma nonsecreting acromegaly glioma grade i craniopharyngioma sarcoma typeofsurgerybeforesrt no surgery biopsy subtotal resection complete resection visualfunctionbeforesrt intact impaired pituitaryfunctionbeforesrt intact partial insufficiency complete insufficiency srt stereotactic radiotherapy 11 / 29 ( 38% ) 10 / 29 ( 34% ) 4 / 29 ( 14% ) 3 / 29 ( 10% ) 1 / 29 ( 3% ) 3 / 29 ( 10% ) 4 / 29 ( 14% ) 20 / 29 ( 69% ) 2 / 29 ( 7% ) 14 / 29 ( 48% ) 15 / 29 ( 52% ) 18 / 29 ( 62% ) 8 / 29 ( 28% ) 3 / 29 ( 10% ) strahlentherapieundonkologie22013 | original article fig . 
the most frequent tumor types were grade i meningioma ( n = 11 ) and pituitary adenoma ( n = 10 , 7 nonfunctioning , 3 growth hormoneproducing )  . 
in 4 of 26 patients ( 15% ) with at least partial pituitary function , new hormonal deficits developed ( actuarial rate 21% at 5 years and 10 years )  . 
fractionated stereotactic radiotherapy for benign tumors of the perioptic and sellar region results in satisfactory response and local control rates and does not affect the visual systethe assumption that patients can be spared hypophyseal insufficiency only holds for small tumors . keywords fractionated stereotactic radiotherapy benign brain tumors skull base optic neuropathy pituitary insufficiency endokrine und visuelle funktion nach fraktionierter stereotaktischer strahlenbehandlung perioptischer tumoren zusammenfassung ziel . 
von1993 bis 2009 wurden n = 29 patienten ( pat . ) behandelt ( berwiegend meningeome grad i , n = 11 , und hypophysenadenome , n = 10 , 7 inaktiv , 3 sth - produzierend )  . 
one patient died of unrelated malignant disease after 16 months , and the patient with the preirradiated pituitary adenoma died after 92 months from progression . in 4 of 26 ( 15% ) patients with normal or partial pituitary function , new hormonal deficits developed ( actuarial rate 21% at 5 years and 10 years )  . 
in our series , we used ( 1 ) a micro - multileaf collimator with a very small leaf width for beam shaping , ( 2 ) treatment planning based on high - resolution ct and mr images coregistered by experienced stereotactic neurosurgeons and radiotherapists , and ( 3 ) conventional fractionation with 1.8 gy fraction size for maximal normal tissue protection . 
these steps resulted in excellent local control rates , no patient developed treatment - related disturbances of the visual function , and a significant number of patients with impaired pretherapeutic vision improved . 
the expectation that patients can be spared hypophyseal insufficiency , however , only held for small tumors . the most clear - cut evidence that fractionated stereotactic radiotherapy has the potential to cure benign brain tumors in the vicinity of critical organs comes from the treatment of optic nerve sheath meningiomas [ 10 , 12 , 13 , 14 , 15 , 16 , 17 , 18 , 19 ] and optic gliomas [ 20 ]  . 
most of the authors used fractionated stereotactic radiotherapy with doses of 5055 gy at conventional fractionation and observed a minor deterioration of visual function in 510% of the patients and an improvement in 2040% . 
as the organ at risk is included in the ptv in a significant proportion of patients , it seems unlikely that these results can be improved by any irradiation technique . in most of these cases , the pituitary gland is too far away from the ptv to be affected , but particularly patients with pituitary adenomas and craniopharyngiomas often suffer from hypophyseal insufficiency , either as a consequence of the disease or as a side effect of surgery or ra140 | strahlentherapieundonkologie22013 diotherapy . 
in those patients not suitable for radiosurgery , even after fractionated stereotactic radiotherapy using the most elaborate techniques , up to 2040% will eventually develop new hormonal deficits [ 11 , 16 , 20 , 22 , 24 , 27 , 28 , 29 , 30 , 31 ]  . 
these observations and the present investigation suggest that irradiating a larger tumor in the perioptic or parasellar region will always carry the risk of disturbing hypophy seal function , probably because damage to the vascular and nervous pathways between the hypothalamus and pituitary cannot be avoided . a new technique was introduced by using robotic radiosurgery ( cyberknife ) for hypofractionated stereotactic radiotherapy of benign brain tumors [ 40 , 41 , 42 , 43 , 44 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 129136 doi 10.1007 / s00066 - 012 - 0272 - 3 received : 20 july 2012 accepted : 8 november 2012 published online : 9 . 
however , patients that present with locoregional ( lr ) advanced disease of borderline resectability and / or lr recurrence after nephrectomy represent a clinical and therapeutic challenge associated with a poor prognosis with no standard treatment defined [ 1 , 2 ]  . 
in cases in which curative resection is technically feasible , the number of 5 - year survivors is small and , therefore , a clear improvement is needed [ 3 , 4 , 5 , 6 ]  . 
complete negative margin resection sometimes cannot be achieved because of the tumors proximity to , or its proven invasion into , adjacent unresectable structures such as the major vessels and / or vertebral bodies . 
selected patients with isolated lr recurrence after nephrectomy or lr advanced primary rcc ( except for nonradical resection ) were treated with a multimodality approach consisting of maximal resection and intraoperative electron radiotherapy ( ioert ) with or without perioperative external beam radiotherapy ( ebrt )  . 
an update with an evaluation of long - term outcomes provides extensive information in terms of patterns of cancer recurrence and late normal tissue tolerance . patients and methods from january 1983 to december 2008 , 25 consecutive patients ( n = 25 ) who had pathologically confirmed lr advanced primary and lr recurrent rcc underwent multimodal treatment at the clinica universidad de navarra ( pamplona , spain ) and the hospital general universitario gregorio maraon ( madrid , spain )  . 
patients underwent pretreatment staging , typically consisting of the following : physical examination ; complete blood count , liver and renal profile tests ; computed tomography ( ct ) of the chest , abdomen , and pelvis ; bone scan ; abdominal ultrasound ; and / or brain imaging at the discretion of the attending physicians . 
fifteen patients received perioperative ebrt ( either preoperatively , n = 3 ; or postoperatively , n = 12 ) to the macroscopic lesion , tumor bed , and regional lymphatics delivered using megavoltage photons ( median dose , 40 gy )  . 
a variety of sizes ( circular diameter from 6 to 15 cm ) and bevels of lucite applicators ( 1545 ) were used to encompass the clinical target volume ( ctv )  . 
patients were transferred from the operating room to the ioert rooioert was delivered in a single fraction , with the dose selected on the basis of the amount of residual disease , the presence of critical structures , and the dose of preoperative and / or anticipated postoperative ebrt . 
potential factors associated with lrc , progression - free survival ( pfs ) , and overall survival ( os ) were evaluated in a univariate analysis using the log - rank test . 
 fifteen patients had lr advanced primary disease with extensive retroperitoneal nodal involvement ( n = 4 ) , adrenal gland involvement ( n = 4 ) , vena cava involvement ( inferior , n = 3 ; superior , n = 3 ) , renal vein involvement ( n = 3 ) , and / or radical nephrectomy with positive margins ( n = 12 ) proven with frozen sections . 
the first site of relapse was lr failure ( lrf ) in 2 patients , lrf and distant failure ( df ) in 2 , and df only in 15 . 
 six patients ( 24% ) experienced acute or late grade 3 or greater toxicity potentially related to the treatment , including need for blood transfusion ( n = 2 , grade 3 ) , severe peripheral sensitive neuropathy ( n = 1 , grade 3 ) , pancreatitis ( n = 1 , grade 3 ) , duodenal fistula requiring elective reintervention ( n = 1 , grade 3 ) , and one fatal event ( n = 1 , grade 5 ) secondary to sepsis within 30 days of surgery and ioert . discussion locally advanced and recurrent rcc is a challenge in the decision - making process . 
 several institutions have reported durable disease - free survival after surgical resection alone and even more in combination with radiation therapy [ 1 , 2 , 3 , 4 , 5 , 6 ]  . 
from 1983 to 2008 , 25 patients with lr recurrent ( n = 10 ) or lr advanced primary ( n = 15 ) rcc were treated with this approach . 
in patients with lr recurrent or lr advanced primary rcc , a multimodality approach consisting of maximal surgical resection and ioert with or without adjuvant ebrt yielded encouraging local control results , justifying further evaluation . keywords intraoperative radiation therapy locally advanced or recurrent disease renal cell carcinoma surgical resection outcomes intraoperative ebrt und resektion bei nierenzellkarzino ergebnisse nach 20 jahren zusammenfassung ziel . 
 die chirurgische resektion gelang bei 6 patienten ( 24% ) als r0 - resektion ( mit negativen rndern ) und bei 19 ( 76% ) als r1 - resektion ( mikroskopische residualerkrankung )  . 
in 4% der flle ( n = 1 ) trat der tod innerhalb von 30 tagen nach operation und ioert ebei 6 patienten ( 24% ) traten akute oder spttoxizitten grad 3 nach den national cancer institute common toxicity criteria ( nci - ctcae ) , version 4 , auf . 
bei patienten mit lokoregional rezidivierendem oder lokoregional fortgeschrittenem primrem rcc fhrte der multimodale ansatz aus maximaler chirurgischer resektion und ioert adjuvante ebrt zu vielversprechenden ergebnissen bei der lokalen kontrolle , was seine weitere evaluation rechtfertigt . schlsselwrter intraoperative strahlentherapie lokal fortgeschritten oder rezidivierend nierenzellkarzinom chirurgische resektion ergebnisse strahlentherapieundonkologie22013 | original article tab . 
2 individual detailed description of clinical , pathological , and therapeutic features ( contd . ) initial initial stage pathologicalextentof resection mor grade ebrtcomponent maximum primary maximum recurrent tumor dimension ( cm ) tumor mension ( cm ) radical phrectomy margin status radical phrectomy margin status current margin stasoft tissue retroperitoneal tissue ( positive ) , vena cava ( positive ) soft tissue retroperitoneal tissue ( positive ) , regional lymph nodes ( positive ) regional lymph nodes ( positive ) , vena cava ( positive ) , aorta artery ( positive ) soft tissue retroperitoneal tissue ( positive ) soft tissue retroperitoneal tissue ( positive ) vena cava ( positive ) ajcc7th ajcc 7th callyadvanced / locally recurrent locally recurrent locally recurrent locally recurrent locally recurrent locally recurrent locally recurrent pt2an0m0 pt2an0m0 pt3an0m0 pt2bn0m0 pt3bn0m0 pt2bn1m0 studyauthors tab . 
3 outcomes after surgery and intraoperative radiotherapy for primary or recurrent renal cell carcinoma primary / recurrent 0 / 10 3 / 19 15 / 10 median follow - up ( years ) 22.2 mean iort dose ( gy ) 13.5 mean ebrt dose ( gy ) none 3 - year local control 12 / 12 12 / 14 17 / 22 21 / 25 eble et al . 
early clinical studies have demonstrated that the efficacy of irradiation used as a high single dose is irrespective of tumor histologic features , favorably affecting the response of tumors classically categorized as radioresistant [ 15 , 16 , 17 , 18 ]  . 
some expert institutions have adopted a dose - escalation strategy , combining maximal surgical resection and ioert with or without ebrt , without compromising the tolerance of surrounding radiation dose - sensitive structures . 
investigators from the mayo clinic described the outcomes of 22 patients with lr recurrent ( n = 19 ) or lr advanced primary ( n = 3 ) rcc who were treated with this multimodality approach [ 14 ]  . 
in the present study , with long - term follow - up , the multimodality approach ( combining maximal surgical resection and ioert with or without perioperative ebrt ) was associated with durable lr control , with 4 patients experiencing an lr recurrence . 
 [ 7 ] of 54 patients who underwent resection of isolated lr recurrence of rcc after nephrectomy ( median follow - up , 3.4 years ) , isolated second recurrence in the postoperative bed occurred in 14.8% , with half of these patients requiring further radical resections . 
in an analysis of 16 patients with lr recurrence of rcc after nephrectomy who underwent resection ( median follow - up , 1.3 years ) , local recurrence occurred in 6 ( 38% ) [ 3 ]  . 
in the present study , patients were considered for ioert along with surgical resection because of borderline resectability or adverse features for local recurrence ( .tab.2 ) ; therefore , patients in the present analysis likely had more adverse disease characteristics than those in the above - mentioned series . 
similarly high rates of df , ranging from 50 to 62% , have been reported in other retrospective series of patients with lr recurrence of rcc after nephrectomy [ 7 , 8 ]  . 
in the setting of metastatic rcc , tyrosine kinase inhibitors have demonstrated high response rates with relatively low toxicity ; however , these reports largely predated the discovery of novel tyrosine kinase inhibitors [ 19 , 20 , 21 , 22 ]  . 
now more than ever , the potential for utilization of these therapies in concert with surgery and / or radiation therapy underscores the need for multidisciplinary teams centered on patients with rcc [ 23 ]  . 
in the present experience , the rate of grade 35 toxicity was significant ( 24% ) , although consistent with other studies evaluating salvage surgery alone for lr recurrence of rcc . 
the university of southern california reported 31% ( n = 4 ) fatal toxicity within 6 months of surgery , and 2 of 11 patients undergoing radical resection for recurrent rcc developed significant late complications [ 1 ]  . 
our study had comparable toxicity , suggesting that the addition of ioert with or without perioperative ebrt to salvage surgery did not appear to significantly increase morbidity in patients with lr recurrent or lr advanced primary rcc . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 117122 doi 10.1007 / s00066 - 012 - 0270 - 5 received : 13 september 2012 accepted : 8 november 2012 published online : 19 . 
dezember 2012 springer - verlag berlin heidelberg 2012 m.intveno.reerinkm.e.p.philippens department of radiotherapy , university medical center utrecht diffusion - weighted mriinlocallyadvanced rectalcancer pathologicalresponsepredictionafter neo - adjuvantradiochemotherapy the outcome for patients with locally advanced rectal cancer has improved radically over the last two decades with the introduction of new treatment strategies . 
 until the early 1990s , the standard of treatment was surgery alone with a high 5 - year risk of local recurrence at around 25% and a 5 - year survival of around 42% [ 1 ]  . 
introduction of total mesorectal excision as a standard surgical technique combined with the initiation of neo - adjuvant radiochemotherapy radically reduced the local recurrence risk to less than 10% and increased the overall 5 - year survival to over 65% [ 2 , 3 , 4 , 5 ]  . an important prognostic factor for locally advanced rectal cancer is the pathological response after neo - adjuvant radiochemotherapy . 
the better the pathological response , the better the outcome with a low 5 - year local recurrence risk of 2.8% and a high 5 - year overall survival of 87.6% in pathological complete responders [ 6 , 7 , 8 ]  . 
a more tailored treatment after radiochemotherapy is of obvious interest for these patients , as has been proposed by various authors [ 9 , 10 , 11 , 12 , 13 ]  . in recent years , there has been a growing interest in functional imaging to improve clinical response assessment . 
 besides pet , diffusion - weighted magnetic resonance imaging ( mri ) is another modality that is applied to predict tumor response and is successfully used in several tumor sites , such as the brain and liver [ 15 ]  . 
the measured value , the apparent diffusion coefficient ( adc ) , is related to tissue cellularity , tissue organization , and extracellular space tortuosity and is dependent on the intactness of the cellular membranes [ 16 ]  . 
 moreover , in diffusion - weighted mri , the adc provides a tool for absolute quantitative image analysis that is important for longitudinal studies [ 17 ]  . the present study prospectively assessed the predictive potential of diffusion - weighted mri for selecting patients with a favorable pathological response after radiochemotherapy for locally advanced rectal cancer . patients and methods patients between november 2008 and december 2011 , patients were prospectively included in this study after acquiring informed consent . 
for data analysis , patients with mucinous adenocarcinoma were excluded because of the different radiological aspects compared to nonmucinous tumors [ 18 , 19 ]  . neo - adjuvant therapy and surgery neo - adjuvant radiochemotherapy for 5 weeks was followed by surgery 610 weeks after radiochemotherapy . 
diffusion weighting was achieved by using a singleshot spin - echo echo planar imaging ( ssseepi ) sequence ( tr / te : 7 , 600 ms / 63 ms ; epi factor : 63 ) , with spectral attenuated inversion - recovery ( spair ) fat suppression and isotropic diffusion weighting in three directions with b - values of 0 , 200 , and 800 s / mm2 . 
the total examination time was approximately 25 min with a diffusion - weighted mri sequence of 4 : 08 min . adc analysis adc maps were generated from the diffusion - weighted mr images with b - values of 0 , 200 , and 800 s / mm2 [ 16 ]  . 
a linear regression after a logarithmic transformation of the signal intensity ( lns ) was used to calculate the adc values : ln ( s ) = ln ( a ) badc , where a is the relative amplitude . 
the gr group consisted of patients with pathological complete response ( pcr ) or nearpcr , which was defined as patients with only solitary vital tumor cells in the resection specimen ( mandard trg 2 ) and no tumor - positive lymph nodes . 
paabstract zusammenfassung strahlenther onkol 2013 189 : 117122 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0270 - 5 m.intveno.reerinkm.e.p.philippens diffusion - weighted mri in locally advanced rectal cancer . 
preradiochemotherapy adc values showed a positive predictive value of 42% for pcr and 67% for gr using a similar cut - off value of 0.97 * 103 mm2 / s . 
diffusionweighted mri may be used as an additional tool for selecting good treatment responders after radiochemotherapy . keywords diffusion - weighted imaging pathological response locally advanced rectal cancer neo - adjuvant radiochemotherapy positive predictive value diffusionsgewichtete mrt bei lokal fortgeschrittenem rektumkarzinovorhersage der pathologischen ansprechrate nach neoadjuvanter radiochemotherapie zusammenfassung hintergrund . 
die adc - werte vor rct zeigten einen positiven prdiktiven wert von 42% fr pkr und 67% fr gr mit einem cut - off - wert von 0 , 97 * 103 mm2 / s . 
die diffusionsgewichtete mrt knnte in einem protokoll zur verwendung gelangen , mit dem patienten mit gutem ansprechen nach rct ausgewhlt werden . schlsselwrter diffusionsgewichtete magnetresonanztomographie pathologische ansprechrate lokal fortgeschrittenes rektumkarzinom neoadjuvante radiochemotherapie positiver prdiktiver wert tient and tumor characteristics as well as adc and adc values were compared between the response groups using the mannwhitney u test . 
six patients were excluded from analysis because of refusal of surgery after neo - adjuvant treatment ( n = 2 ) , mri with severe artifacts ( n = 1 ) , or because of mucinous adenocarcinoma ( n = 3 )  . 
preand postradiochemotherapy ( rct ) t2weighted ( t2w ) transversal images ( a , c ) and apparent diffusion coefficient ( adc ) maps ( b , d )  . 
the horizontal dashed line indicates the optimal cut - off value to distinguish between the two groups ( adc = 0.97 * 10 - 3 mm2 / s )  . 
the limited sensitivity for solitary tumor cells can be attributed to the averaging of adc in a voxel with a limited effect of individual tumor cells on the adc . the positive predictive value of relative adc for pcr in our study was between the 37% reported by kim et al . 
apart from rectal cancer , the association between a high adc increase and a good treatment response was also reported for other tumor sites such as the breast , liver , and brain [ 15 ]  . 
this suggests that tumors with higher pre - radiochemotherapy adc levels are more likely to have areas of necrosis , which in turn predicts a poor outcome related to hypoxia - mediated resistance to radiotherapy and chemotherapy [ 28 ]  . 
we were not able to confirm the predictive potential of post - radiochemotherapy adc for pcr or gr [ 25 , 30 , 31 ]  . how to interpret these inconsistent results from the various studies ? several factors could be of influence . 
3 diagnostic performance of pretherapy adc values and relative adc for predicting pathological response conclusion pre - rctadc pcr : non - pcr 0.97 * 103 mm2 / s 0.77 diagnosticvalue cut - off accuracy sensitivity specificity rct radiochemotherapy , adc apparent diffusion coefficient , gr good responders , mr moderate responders , pcr pathological complete response , auc area under the roc curve , ppv positive predictive value , npv negative predictive value relativeadc pcr : non - pcr 41% increase 0.95 gr : mr 0.97 * 103 mm2 / s 0.85 gr : mr 41% increase 0.97 tion as pcr or minimal microscopic disease might be operator dependent in the absence of standardization of reporting [ 32 ]  . 
moreover , reproducibility between centers with different diffusion - weighted mri sequence designs , such as the choice of b - values , and mri spectrometers is not clear . the various results reported in the diffusion - weighted mri response evaluation studies also emphasize the need for standardization of analysis methods in a large prospective multicenter study before diffusion - weighted mri can be implemented in rectal cancer response prediction . 
 [ 12 , 36 ] , who show that omission of surgery is safe in patients with complete clinical response after neo - adjuvant radiochemotherapy , even after long follow - up . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literatur kommentiert strahlenther onkol 2013 189 : 159160 doi 10.1007 / s00066 - 012 - 0278 - x online publiziert : 21 . 
dezember 2012 springer - verlag berlin heidelberg 2012 s.kubicka krebszentrum reutlingen , medizinische klinik i , reutlingen keinvorteildurchfolfox4 frltereundstadium - iikolonkarzinompatienten originalpublikation tournigand c , andr t , bonnetain f et al ( 2012 ) adjuvant therapy with fluorouracil and oxaliplatin in stage ii and elderly patients ( between ages 70 and 75 years ) with colon cancer : subgroup analyses of the multicenter international study of oxaliplatin , fluorouracil , and leucovorin in the adjuvant treatment of colon cancer trial . 
durch diese ergebnisse , die dann durch die nsabpc07 - studie besttigt worden sind [ 2 ] , wurde die oxaliplatinbasierte adjuvante chemotherapie der standard bei patienten mit kolonkarzinom im stadium iii . 
 die frage , ob diese intensivierte chemotherapie auch bei lteren patienten , bei patienten im stadium ii der hochrisikogruppe und bei der standardrisikogruppe die ergebnisse verbessert , ist aber nach wie vor unklar . 
es wurde eine explorative subgruppenanalyse der mosaic - studie durchgefhrt , um den stellenwert der oxaliplatinbasierten chemotherapie bei lteren patienten ( 70 bis < 76 jahre ) sowie bei patienten im stadium ii zu untersuchen . 
das stadium ii wurde in eine hochrisikogruppe ( hr ) eingeteilt , wenn mindestens einer der folgenden kriterien erfllt war : t4 , tumorperforation , darmverschluss , niedriger differenzierungsgrad , vense infiltration sowie weniger als 10 analysierte lymphknoten . 
die explorative subgruppenanalyse der mosaic - studie zeigte keinen statistisch signifikanten vorteil im gesamtberleben oder krankheitsfreien berleben durch folfox4 im vergleich zu lv5fu2 fr das stadium ii ( lr oder hr ) oder fr ltere patienten . kommentar der klinische nutzen einer adjuvanten chemotherapie mit 5 - fu / fs bei kolorektalen karzinomen im uicc - stadium ii strahlentherapieundonkologie22013 | 8 . 
sanoff hk , carpenter wr , strmer t et al ( 2012 ) effect of adjuvant chemotherapy on survival of patients with stage iii colon cancer diagnosed after age 75 years . 
haller dg , tabernero j , maroun j et al ( 2011 ) capecitabine plus oxaliplatin compared with fluorouracil and folinic acid as adjuvant therapy for stage iii colon cancer . 
lediglich die groe randomisierte quasar - studie konnte einen signifikanten berlebensvorteil fr die patienten im stadium ii durch eine adjuvante 5 - fu / fs - therapie zeigen ( hr 0 , 82 ; 95% - ki 0 , 700 , 95 ; p = 0 , 008 ; entsprechend einem absoluten berlebensvorteil von 3 , 6% ; [ 6 ] )  . 
trotz der groen methodischen mngel der quasar - studie kann aufgrund dieser daten aktuell eine adjuvante therapie mit 5 - fu / fs oder capecitabine im stadium ii durchgefhrt werden , wobei aber die rolle der therapieintensivierung durch folfox4 , insbesondere fr das hochrisikostadium ii , unklar war . 
die aktuelle subgruppenanalyse der mosaic - studie zeigt jetzt , dass auch fr das hochrisikostadium ii eine eskalation durch eine oxaliplatinbasierte adjuvante chemotherapie nicht sinnvoll ist . whrend der positive effekt einer adjuvanten fluoropyrimidin - monochemotherapie auch bei lteren patienten im stadium iii unstrittig ist , bleibt die rolle der kombinationschemotherapien mit oxaliplatin bei lteren patienten in dieser situation weiterhin unklar . 
andr t , boni c , mounedji - boudiaf l et al ( 2004 ) multicenter international study of oxaliplatin / 5 - fluorouracil / leucovorin in the adjuvant treatment of colon cancer ( mosaic ) investigators . 
tournigand c , andr t , bonnetain f et al ( 2012 ) adjuvant therapy with fluorouracil and oxaliplatin in stage ii and elderly patients ( between ages 70 and 75 years ) with colon cancer : subgroup analyses of the multicenter international study of oxaliplatin , fluorouracil , and leucovorin in the adjuvant treatment of colon cancer trial . 
gill s , loprinzi cl , sargent dj et al ( 2004 ) pooled analysis of fluorouracil - based adjuvant therapy for stage ii and iii colon cancer : who benefits and by how much ? j clin oncol 22 : 17971806 6 . 
jackson mccleary na , meyerhardt j , green e et al ( 2009 ) impact of older age on the efficacy of newer adjuvant therapies in 12 , 500 patients with stage ii / iii colon cancer : findings from the accent database . 
j clin oncol 27 : 170s ( suppl ; abstr 4010 ) 160 | strahlentherapieundonkologie22013 original article strahlenther onkol 2013 189 : 147154 doi 10.1007 / s00066 - 012 - 0262 - 5 received : 4 june 2012 accepted : 18 october 2012 published online : 22 . 
dezember 2012 springer - verlag berlin heidelberg 2012 o.p.erpolat1p.u.gocun2m.akmansu1g.ozgun2g.akyol2 1 department of radiation oncology , medical school of gazi university , ankara 2 department of pathology , medical school of gazi university , ankara hypoxia - related moleculeshif - 1 , ca9 , andosteopontin predictorsofsurvivalinpatients withhigh - gradeglioma despite recent advances in current treatment approaches , the prognosis of highgrade gliomas is still poor [ 1 ]  . 
it plays a significant role in tumor recurrences , metastasis , and poor response to treatment including radiotherapy ( rt ) , chemotherapy , and antiangiogenic treatment [ 6 ]  . 
the strong effect of hypoxia in these processes makes it an attractive therapeutic target for high - grade glioma [ 2 ] , and clinicians are very interested in identifying new molecules involved in hypoxia in order to select patients for modified treatment in the future [ 7 , 8 ]  . recently , molecules involved in the hypoxic response of tumor cells were identified as endogenous hypoxia markers [ 2 , 7 ] using noninvasive and cost - effective methods to determine the condition of tumor hypoxia [ 9 , 10 ]  . 
hypoxia - inducible factor - 1 alpha ( hif - 1 ) and carbonic anhydrase 9 ( ca9 ) are the most consistently upregulated molecules under hypoxic conditions [ 7 ]  . 
their over - expression has been found in various cancers including gliomas [ 2 , 7 ] and is related to a more aggressive tumor behavior , rt resistance , and poor survival [ 11 , 12 , 13 ]  . 
another new molecule , osteopontin ( opn ; a tumor - associated phosphorylated glycoprotein ) is overproduced by tumor cells and plays an important role in tumor growth through the enhancement of angiogenesis in glioma cell lines [ 14 , 15 ]  . 
because there are few reports investigating the expression pattern and prognostic role of opn in high - grade glioma , we aimed to assess the expression pattern of opn with the potentially intrinsic hypoxia markers such as hif - 1 and ca9 and to correlate the expression levels of these markers with clinicopathologic characteristics and patient outcome . patients and methods patients and tissue samples patients were eligible for immunohistochemical staining . 
the patients files were reviewed for gender , age , performance status , status of resection , histological differentiation , rt , chemotherapy , treatment response , and patient outcome . 
tissue samples of 92 presented at the study was presented as a poster abstract at the ecco 16 annual meeting , 2327 september 2011 , stockholm . strahlentherapieundonkologie22013 | original article tab . 
the expression was determined by assessing the percentage of positive tumor cells ( 110% = 1 + , 11 49% = 2 + , 50% = 3 + ) and the staining intensity ( weak = 1 + , moderate = 2 + , inten148 | strahlentherapieundonkologie22013 sive = 3 + )  . 
this cut - off expression level was chosen on the basis of the median score . statistical analyses all statistical analyses were performed using spss 15.0 software package for windows ( spss inc . , chicago , il , usa )  . 
a cox regression model was used for multivariate survival analysis . results clinicopathologic characteristics of the patients the median age of the patients was 49 years ( range , 1877 years )  . 
 twenty - five ( 27% ) patients received teabstract zusammenfassung strahlenther onkol 2013 189 : 147154 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0262 - 5 o.p.erpolatp.u.gocunm.akmansug.ozgung.akyol hypoxia - related molecules hif - 1 , ca9 , and osteopont predictors of survival in patients with high - grade glioma abstract purpose . 
the expression results of these markers were combined to form a hypoxic profile , and high hypoxic scores ( expression of two or three markers ) were significantly correlated to poorer overall survival . 
it may be necessary to utilize the hypoxic score in selecting patients for targeted therapy in the future . keywords high - grade glioma hypoxia osteopontin survival prognostic factors hypoxiemarker hif - 1 , ca9 und osteopont berlebensprdiktoren bei patienten mit hochgradigem gliom zusammenfassung ziel . 
bei der zusammenfassung der expressionsergebnisse dieser marker zur erstellung eines hypoxischen profils korrelierten die flle mit hochhypoxischen werten ( expression von zwei oder drei markern ) deutlich mit schlechterem gesamtberleben . 
mglicherweise ist es notwendig , zuknftig den hypoxischen wert zu nutzen , um patienten fr eine gezielte therapie zu ermitteln . schlsselwrter hochgradiges gliom hypoxie osteopontin berleben prognosefaktoren mozolomide concurrent to rt and then received it in an adjuvant setting ( mean , six cycles )  . 
six weeks after completion of treatment and 3 months thereafter , patients were evaluated with cranial magnetic resonance imaging for treatment response . hif - 1 , ca9 , and opn expressions in malignant glioma tissues while hif - 1 expression was observed both in the cytoplasm and nucleus , ca9 and opn expression was observed only in the cytoplasm of tumor cells . 
positive staining of cytoplasmic and nuclear hif - 1 , ca9 , and opn was found in 76 ( 82.5% ) , 68 ( 74% ) , 73 ( 79% ) , and 40 ( 43.5% ) of the tumor samples , respectively . 
1 8 negative ( a , 400 ) and positive ( e , 400 ) expression of cytoplasmic hif - 1 ; negative ( b , 400 ) and positive ( f , 400 ) expression of nuclear hif - 1 ; negative ( c , 400 ) and positive ( g , 400 ) expression of ca - 9 ; negative ( d , 400 ) and positive ( h , 400 ) expression of opn in representative examples of malignant gliomas ticularly seen in perinecrotic ( 70% , 73% , and 72% , respectively ) areas . 
no correlation was observed between the expression levels of the markers ( data not shown )  . since expression of hif - 1 was observed both in the cytoplasm and nucleus , localization of each hif - 1 expression was taken into consideration when composing hypoxic profiles . 
the two hypoxic profiles , i.e. , hypoxic profile 1 ( including cytoplasmic hif - 1 , ca9 , and opn ) and hypoxic profile 2 ( including nuclear hif1 , ca9 , and opn ) , were evaluated . 
by using this scoring system , a high hypoxic profile - 1 score was observed in 63 ( 68.5% ) tumor samples , whereas a high hypoxic profile - 2 score was found in 67 ( 73% ) samples . 
the results of the expression patterns of the hypoxia markers are shown in .tab.1. correlation of hif - 1 , ca9 , and opn expression and hypoxic scores with clinicopathologic variables there was no significant association between cytoplasmic and nuclear hif - 1 expression and any of the following clinicopathologic variables : gender , age , karnofsky performance status ( kps ) , recursive partitioning analysis ( rpa ) classification , extent of surgery , postoperative residual disease , histological tumor differentiation , treatment response , and survival status . 
high hypoxic score 2 was significantly associated with age of more than 50 years ( p = 0.029 ) , an rpa class higher than 4 ( p = 0.011 ) , gbm histology ( p = 0.001 ) , presence of residual tumor ( p = 0.009 ) , poor tumor response ( p = 0.001 ) , and poor survival sta150 | strahlentherapieundonkologie22013 log - rank tab . 
these results are statistically significant and data are shown in .tab.2. to determine the independent predictors of survival , the significant factors in univariate analysis were used as covariates in the multivariate analysis . 
considering the prognostic significance of the expression of hypoxic molecules on os , a high hypoxic score 1 was the only independent negative prognostic factor ( p = 0.028 , 95% ci )  . 
the results of the multivariate survival analysis are summarized in .tab.3. after a median follow - up of 16 months ( 283 ) , the median overall survival ( os ) time was 15.8 months for all patients . 
in univariate survival analysis , median os discussion hif - 1 itself and hif - 1 - regulated genes are considered as potential therapeutic strahlentherapieundonkologie22013 | original article p = 0 . 
2 8 overall survival time ( months ) regarding negative and positive expression of cytoplasmic / nuclear hif - 1 , ca9 , opn , and low and high hypoxic score 1 and 2 152 | strahlentherapieundonkologie22013 tab . 
 despite some contradictory results in the literature [ 22 , 23 ] , positive expression of hif - 1 , ca9 , and opn was localized in perinecrotic areas that mark the areas of avascularity and hypoxia as previously reported for high - grade glioma , particularly in gbm [ 7 , 24 , 25 ]  . in concordance with several studies [ 10 , 23 , 24 , 25 , 26 ] , in our study , staining of hif - 1 was observed both in the cytoplasm and nucleus , whereas staining of ca9 and opn was seen in the cytoplasm of tumor cells . 
although positive expression of hif - 1 and ca9 was found in most of the tumor samples , opn positivity was found in 43.5% , which is quite lower than that of other markers . 
using different antibodies with different ihc protocols may cause variability in staining and in the interpretation of results . although over - expression of hif1 and ca9 was observed in high - grade brain tumors [ 2 , 4 , 22 ] , there are few data on opn expression in these tumors . 
their findings showed that opn and ca9 were the most consistent in response , in terms of mrna over - expression , related to duration and severity of hypoxia especially in gbm . 
in vitro studies showed that overexpression of opn induces cell migration [ 27 ] and directly stimulates angiogenesis , which may play an important role in tumorigenesis [ 28 ]  . 
 one of the studies showed that the opn expression level was found to be equal in both normal brain and malignant astrocytoma tissue by using ihc and western blot analysis [ 30 ]  . 
although gbm samples were significantly positive for ca9 and opn expression when compared to aa , positive staining of cytoplasmic and nuclear hif - 1 was not significantly different between the two histology results . 
 besides histological findings , most of the factors that have been shown as important determinants of clinical outcome in patients with malignant glioma , namely , patient age , kps , rpa classification , extent of surgery , and residual tumor [ 1 , 31 ] , were significant in our study . in univariate survival analysis , positive expression of all hypoxic markers was associated with worse os , and positive expression of ca9 and opn was associated with worse pfs . 
in korkolopoulou and coworkers [ 24 ] study , ihc analysis of hif - 1 , ca9 , and vegf was performed for 96 patients with glial brain tumor ( 20 , 12 , and 64 patients had grade ii , iii , and iv tumors , respectively )  . 
the authors observed that increased hif - 1 , ca9 , and vegf expression was correlated with shortened survival but also noted that the significance disappeared when the tumor grades were separated and reassessed . 
in the study of irie and colleagues [ 22 , 23 ] , the hif - 1 expression level in 60 patients with gbm who were treated with postoperative rt was evaluated and a strong expression of hif - 1 was found to be correlated with pfs . 
the expression of opn , hif - 1 , and ca9 was evaluated by ihc in 34 tumor samples of patients with advanced head and neck cancer treated with rt [ 9 ]  . 
os time was not significantly correlated with opn expression ; however , when the results of opn , hif - 1 , and ca9 expression were combined into a hypoxic profile , a strong and statistically significant impact on os was observed . 
wykoff cc , beasley n , watson ph et al ( 2001 ) expression of the hypoxia - inducible and tumor - associated carbonic anhydrases in ductal carcinoma in situ of the breast . 
wang y , yan w , lu x et al ( 2011 ) overexpression of osteopontin induces angiogenesis of endothelial progenitor cell via the av3 / p13k / akt / enos / no signaling pathway in glioma cells . 
jang t , savarase t , low hp et al ( 2006 ) osteopontin expression in intratumoral astrocytes marks tumor progression in gliomas induced by prenatal exposure to n - ethyl - n - nitrosourea . 
ding q , stewart j jr , prince cw et al ( 2002 ) promotion of malignant astrocytoma cell migration by osteopontin expressed in the normal brain : differences in integrin signaling during cell adhesion to osteopontin versus vitronectcancer res 62 : 53365343 31 . 
cefaro ga , genovesi d , vinciguerra a et al ( 2011 ) prognostic impact of hemoglobin level and other factors in patients with high grade glioma treated with postoperative radiochemotherapy and sequential chemotherapy based on temozolomide : a 10 year experience at a sinle institution . 
hui ep , chan atc , pezzella f et al ( 2002 ) co - expression of hypoxia - inducible factors 1 and 2 , carbonic anhydrase ix , and vascular endothelial growth factor in nasopharyngeal carcinoma and relationship to survival . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . case study strahlenther onkol 2013 189 : 155158 doi 10.1007 / s00066 - 012 - 0261 - 6 received : 1 july 2012 accepted : 18 october 2012 published online : 21 . 
dezember 2012 springer - verlag berlin heidelberg 2012 b.berger1m.bamberg1d.zips1t.schlunk2 1 department of radiation oncology , university of tbingen 2 department of palliative medicine , paul - lechler - krankenhaus , tbingen multiplemalignancies inasinglepatient aglimpseinto30yearsof interdisciplinaryoncology in february 2007 , an 80 - year - old woman with a pelvic mass was seen at our cancer center for evaluation of neoadjuvant chemoradiation ( rct )  . 
until recently , she was medically fit and was able to run her household autonomously . presentation of case a look at the patients voluminous medical records revealed the following oncologic history ( .tab.1 ) : at the age of 51 years , the patient was diagnosed with rectal cancer , located 6 cm above the sphincter level . 
on pathological examination , a moderately differentiated papillary adenocarcinoma with infiltration of the subserosa was found ( pt3 ) ; eight locoregional lymph nodes were uninvolved ( pn0 )  . 
the pathological analysis showed an early tumor recurrence restricted to the rectal mucosa ( rpt1 ) that was resected safely ( r0 )  . two years after rectal surgery , postmenopausal vaginal bleeding was followed by the diagnosis of a moderately differentiated adenocarcinoma of the uterine endometriu abdominal hysterectomy with bilateral adnexectomy confirmed an intraluminally grown uterine adenocarcinoma infiltrating the endometrium over 0.5 cm ( pt1a )  . 
after surgery , the patient received a vaginal radium instillation administering 40 mg radium over 24 h ( 960 mgeh ) without major toxicity . at the age of 67 and 14 years after treatment for endometrial cancer , the patient noticed a mass within the upper outer quadrant of her right breast . 
the patient underwent breast - conserving surgery with pancreatic cancer 83y leukemia 48y colon cancer 36y breast cancer 46y * rectal cancer 51y , endometrial cancer 54y , breast cancer 67y , colon cancer 67y , sarcoma 75y breast cancer 48y fig . 
2 hereditary cancer syndromes hereditarycancersyndromes syndrome hereditary breast / ovarian cancer localization breast , ovarian , pancreas lynch syndrome i / ii ( hereditary nonpolyposis colon cancer , hnpcc ) lifraumeni syndrome cowdens syndrome peutzjeghers syndrome breast , brain , sarcoma , leukemia breast , thyroid , uterine gastrointestinal , breast , lung , uterine gastrointestinal , uterine gene brca1 , brca2 mlh1 , msh2 , msh6 pten stk11 clinicalcharacteristics childhood cancer mucocutaneous lesions , hamartomas mucocutaneous lesions , polyposis gastrointestinal adenomatosis familial adenomatous polyposis ( fap ) brca ( early - onset ) breast cancer gene , mlh mutl homolog ( dns mismatch repair protein ) , msh muts homolog ( dns mismatch repair protein ) , p53 tumor protein p53 , pten phosphatase and tensin homolog , stk11 serine / threonine kinase 11 , apc adenomatous polyposis coli gene right axillary lymphadenectomy . 
 considering the close resection margins , the patient opted for adjuvant rt and received a cumulative end dose of 66.0 gy realized by a three - dimensional multifield isocentric approach without major acute or late toxicity occurring . four years later , the pelvic mass led to the patients current presentation . 
the pathological specimen confirmed the previously suggested mucinous adenocarcinoma with infiltration of the posterior vaginal wall ( rpt4 )  . one year later and 6 years after sarcoma treatment , a ct scan revealed a 6 - cm mass within the right apical lung with plane contact to the thoracic wall . 
a few weeks later , the patient moved into a nursing home where she died symptomatically well controlled in early january 2010 . discussion of pathology after having completed her sarcoma treatment in 2005 , the patient underwent genetic testing and counseling . 
regarding the metachronous development of two gastrointestinal tumors and two gynecological malignancies , hereditary nonpoly posis colon cancer ( hnpcc ) was suspected [ 7 ] ; however , the corresponding hnpcc diagnostic criteria were not matched completely [ 7 , 12 ]  . 
thus , the patients daughters received an individual care plan focused on gastrointestinal and breast cancer prophylaxis . discussion of management this patient with a suspected yet undetectable inherited tumor syndrome had experienced seven manifestations of at least five different malignancies . 
historical unimodal treatments have been replaced by complex therapeutic strategies requiring the cooperation of surgeons , radiation oncologists , and medical oncologists , leading to improved outcomes in terms of tumor control and overall survival . 
treatment today would consist of neoadjuvant crt followed by oncologic surgery and thus would most probably have prevented the early anastomotic tumor recurrence [ 5 , 10 , 13 ]  . a special feature of the present patient history is the development of exclusively node - negative nonmetastasizing solid tumors . 
in the last few years , the mechanisms of metastasis have been increasingly characterized with epithelial mesenchymal transition ( emt ) representing a crucial step in acquisition of cellular metastatic capability [ 2 ]  . 
however , our knowledge of the microenvironmental and immunogenic factors influencing the early lymphatic or systemic spread of tumor cells still does not suffice to assess the individual cancers metastatic potential . 
the lack of early metastatic spread certainly justified aggressive locoregional treatments leading to effective tumor control and long survival . however , the present case also reflects the drawbacks of multimodal therapy . 
two of the patients tumors could have been potentially treatment - related : the scapular sarcoma close to tissue irradiated 8 years earlier during breast cancer treatment and the rectovaginal adenocarcinoma almost 30 years after vaginal brachytherapy . 
however , competing cofactors make the evaluation difficult and the corresponding risks have to be contrasted with a 20% locoregional control benefit by adjuvant breast rt after 15 years [ 3 ]  . 
in interdisciplinary oncology , it is predominantly the radiation oncologist who must cope with the balancabstract zusammenfassung strahlenther onkol 2013 189 : 155158 doi 10.1007 / s00066 - 012 - 0261 - 6 springer - verlag berlin heidelberg 2012 b.bergerm.bambergd.zipst.schlunk multiple malignancies in a single patient . 
 a glimpse into 30 years of interdisciplinary oncology abstract we report on an 83 - year - old woman who suffered from seven manifestations of at least five different nonmetastasizing malignancies during a period spanning more than three decades . 
in particular , radiation oncologists routinely have to perform a riskbenefit analysis , rendering their work both challenging and fascinating . keywords multiple malignancies genetic tumor syndrome interdisciplinary oncology locoregional treatment case report multiple malignome bei einer patient ein blick auf 30 jahre interdisziplinre onkologie zusammenfassung berichtet wird ber die krankheitsgeschichte einer zuletzt 83 - jhrigen patientin , bei der in einem zeitraum von mehr als 3 jahrzehnten 7 manifestationen mindestens fnf verschiedener nichtmetastasierender malignome auftraten . 
 gerade der radioonkologe ist im alltag gefordert , individuelle risiko - nutzen - analysen zu erstellen , was seine arbeit anspruchsvoll , aber auch faszinierend macht . schlsselwrter multiple malignome genetisches tumorsyndrom interdisziplinre onkologie lokoregionale therapie kasuistik ing act between benefits and risks of additional rt . 
this might be illustrated by the decision to administer adjuvant brachystrahlentherapieundonkologie22013 | mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 9797 doi 10.1007s00066 - 012 - 0294 - x springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
29 , h - 1145 budapest , telefon ( + 36 / 1 ) 251 - 1471 , fax - 1478 , e - mail : mayera@hu.inter.net deutsche gesellschaft fr medizinische physik , p . 
kneschaurek , klinik fr strahlentherapie der technischen universitt , klinikum rechts der isar , ismaninger strae 22 , d - 81675 mnchen , telefon ( + 49 / 89 ) 4140 - 4504 , fax - 4881 hellenic society of radiation oncology , p . 
februar 2013 degro - kurs im rahmen der weiterbildung zum arzt fr strahlentherapie ; seminar der deutschsprachig - europischen schule fr onkologie deso ; cme - zertifizierung durch die bayerische landesrztekammer beantragt leitung der veranstaltung : r . 
27 , 91054 erlangen information und anmeldung : st - studiensekretariat@uk - erlangen.de , die degro schreibt erneut mehrere wissenschaftliche preise aus , die whrend des nchsten jahreskongresses vom 9.5. 
 es handelt sich um den hermann - holthusen - preis , alfred - breit - preis , dissertationspreis , innovationspreis , preis zur hochprzisions - strahlentherapie , gnther - von - pannewitz - preis sowie den koester - preis . informationen : anmeldung : strahlentherapie und onkologie 1 2013 | letter to the editor strahlenther onkol 2013 189 : 8186 doi 10.1007 / s00066 - 012 - 0265 - 2 published online : 2 . 
we are disappointed that the authors did not contact us or write us about the editorial : it is indeed very unusual not to write a letter to the authors ( at least concurrently ) , but to publish an editorial on the hta report [ 2 ] without contacting either the institution or the authors of the systematic review in question beforehand . 
in ( mis - ) using the role of the editor - in - chief , this fact gives the impression that the authors of the editorial do not wish to initiate a scientific debate about methodology , but to openly question an institution , namely the lbihta . 
sauer , head of the department of radiooncology in erlangen , has written this open letter not in his role as editor - in - chief , but as a speaker of the so - called atzelsberg circle , whose members are all providers of hyperthermia in germany . hyperthermia ismost oftenbeing delivered by the devices of the bsd medical corporation , salt lake city / nasdaq listed : bsd - 500 , 2000 , 2000 - 3d , 20003d / mr . 
food and drug administration ( fda ) approval for the treatment of certain tumors , while bsd - 2000 does not concurrently have fda approval except as an investigational device , although it has obtained hud / humanitarian use device designation for use in conjunction with radiation therapy for the treatment of cervical carcinoma patients [ 3 ] [ 4 ] for demonstrating the products safety and probable benefit for the treatment of a disease . 
in the us where the devices are produced , the two more advanced devices , bsd 20003d and 2000 - 3d / mr , have not been approved by the fda at all for any kind of use within the usa . nevertheless , the bsd products have obtained ce - mark certifications necessary for marketing in europe . 
hyperthermia with bsd is being carried out in five to six european countries only [ 5 ] , with the highest geographical concentration in germany ( in nine centers ) and the netherlands ( three centers ) , while in many other countries only one device per country is installedpresumably for research reasons , since they are almost all located in university settings . european research institutions for hyperthermia are f daniel den hoed cancer center of the academisch ziekenhuis ( rotterdam , the netherlands ) , f haukeland university hospital ( bergen , norway ) , f dusseldorf university medical school , tbingen university medical school , essen university hospital , charit medical school of humboldt university ( berlin ) , luebeck university medical school , munich university medical school grosshadern , interne klinik argirov of the munich comprehensive cancer center , university of erlangen ( all in germany ) , f university of verona medical center ( italy ) , f graz university medical school ( austria , no more since 2010 ) , f kantonsspital aarau ( switzerland )  . strahlentherapie und onkologie 1 2013 | letter to the editor may we firstly refer to the current evidence base : hyperthermia has been on the scene for 25 years : clinical trials were mostly carried out in the late 1980s and mid - 1990s [ 6 ] in various cancers . 
because of double and triple publications on the same patients ( as it is done quite often in medicine ) , at first sight the field of hyperthermia looks somewhat researched . 
taking a second look ( excluding double publications ) , it is different : after the publication of the lbi - hta report in early 2010 [ 2 ] , only one phase iii multi - centric trial was published by issels in 2010 [ 7 ] , who is a provider of hyperthermia and an owner of bsd stocks ( coi statement 2007 [ 8 ] )  . 
 between 1987 and 2010 , altogether 11 rcts were published on the following four cancer indications : f cervix ( sharma 1989 , van der zee 2000 , harima 2001 , vasanthan 2005 , franckena 2008 )  . 
unfortunately , hyperthermia providers , primary investigators / researchers , and even authors of review publications [ 9 ] [ 10 ] are all the same 82 | strahlentherapie und onkologie 1 2013 experts , and it proves difficult to find independent publications . 
 in none of the published studies from the respective authors of clinical research with bsd products is a conflict of interest statement declared . although hyperthermia is being carried out in some clinics in the us and europe ( and china ) , in the nccn / national comprehensive cancer network evidence - based guidelines ( update 2012 ) hyperthermia is mentioned ( but not recommended ) only as an option for consideration for two indications ( out of the 11 indications under review ) , namely breast cancer and soft tissue sarcoma cancer . for breast cancer , the nccn guidelines say [ 11 ] the guidelines include consideration of the addition of hyperthermia to irradiation for localized recurrences / metastasis ( category 3 )  . 
while there is heterogeneity among the study results , a series with strict quality assurance demonstrated a statistically significant increase in local tumor response and greater duration of local control with the addition of hyperthermia to radiation compared to radiation alone . 
no differences in overall survival have been demonstrated . for sarcoma , the nccn guidelines say [ 11 ] the results of a recent phase iii randomized trial ( eortc 62961 ) showed that regional hyperthermia ( rht ) increases the benefit of neoadjuvant chemotherapy in patients with localized high - risk sts . 
in this study , 341 patients were randomized to receive either neoadjuvant chemotherapy with etoposide , ifosfamide , and doxorubicin ( eia ) alone , or combined with rht ( eia plus rht )  . 
after a median follow - up of 34 months , among 149 patients with extremity sarcoma , the 2 - year dfs and local pfs rates were 70 and 92% respectively for patients treated with eia plus rht . 
 however , these results need to be confirmed in large cohort studies and the use of rht with preoperative chemotherapy is not recommended in the guidelines . the nci still writes [ 12 ] a number of challenges must be overcome before hyperthermia can be considered a standard treatment for cancer . 
other studies focus on improving hyperthermia techniques . hyperthermia in oncology is obviously not considered standard practice ( yet )  . we would like to respond to the criticism on methodology , raised in the editorial , in more detail : the authors of the editorial ( the atzelberg circle of the german cancer society ) mainly criticize that our ( lbi - hta ) report on hyperthermia was based on the 2005 published g - ba report [ 6 ] on the same interventions , not ourselves considering the published trials before 2005 agaour response : in an era of ever increasing numbers of not only original / primary medical research , but also of secondary analyses / systematic reviews [ 13 ] , the building of ones own evidence synthesis upon existent high quality reviews with an identical research question is a common and methodically accepted practice among hta - / ebm or health care regulatory institutes . 
the prerequisite is a scientifically rigorous review from credible institutions ( credibility is based on transparent methods of searching and extracting data from clinical trials ) [ 14 ]  . 
by criticizing our hta report , the authors of the editorial implicitly question the g - ba report and its scientific rigour . to summarize : all rcts available in german or english language until mid2005 have been included and considered in the g - ba report [ 6 ] , all rcts available in german or english language published between 2005 and january 2010 were included in our lbi - hta report on hyperthermia [ 2 ]  . 
besides the fact that the best available evidence ( rcts ) was considered , many further references , such as observational not - controlled studies , were included as additional supporting material . 
it is therefore of great astonishment to us that our approach that follows the standard principles of evidence - based medicine has been criticised as subjective , selective and flawed in parts . the methodology we applied was a systematic review ( in contrast to a selective review ) : in systematic reviews , literature is systematically searched for in several databases ( medline , embase , cochrane ) , literature is in - / excluded along pre - defined criteria , data ( patient - relevant endpoints and safety data ) are extracted . 
we follow the standards of systematic reviews in all our evidence analyses strictly . in 2005 the g - ba decided , because of the low quality evidence , not to include hyperthermia in the german benefit catalogue for any of the 11 indications [ 16 ]  . 
 similar to germany , austrian decisionmakers decided in 2010 , based on the lbi - hta report , not to invest in hyperthermia again , owing to the lack of convincing evidence . 
interestingly , possibly because of the regulatory decisions in germany ( much later in austria ) not to reimburse hyperthermia , the stocks of bsd fell dramatically between 2007 and 2010 [ 17 ]  . 
the corresponding author declares that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 3340 doi 10.1007 / s00066 - 012 - 0224 - y published online : 23 . 
for patients with earlystage non - small cell lung cancer ( nsclc ) as well as for patients with pulmonary metastases , sabr has been shown to result in very good local control rates , which are comparable to those after surgery [ 2 , 3 , 4 , 5 , 6 , 7 , 8 , 9 ]  . dose escalation trials identified a total dose up to 66 gy in 3 fractions for small tumors and 60 gy in 3 fractions for larger tumors as being safe , resulting in excellent local control rates with rather low toxicity [ 10 ]  . 
 [ 12 ] along with other groups [ 11 ] [ 13 , 14 , 15 , 16 ] concluded that biological effective doses ( bed10 ) of about 100 gy are necessary to reach long - term local control . 
however , the total dose , fractionation , and physical factors , such as the geometry of the dose prescription and dose calculation methods , are very heterogeneous across centers , thereby hampering the comparability of the published dose regimens [ 17 , 18 , 19 , 20 ]  . 
malignancy of the pulmonary nodule was proven by biopsy in 25 of the lesions ( 55% ) ; this was 19 / 29 lesions ( 65% ) in nsclc and 7 / 16 lesions ( 43% ) in metastasis patients . 
in all other patients , diagnosis was determined according to radiological signs of malignancy and / or increase in size and pathologic uptake on fdg - pet / ct scans . patients were treated with a total dose of either 37.5 gy in 3 fractions or 35 gy in 5 fractions in cases with lesions located centrally in the vicinity of critical normal tissues or close to the thoracic wall . 
the investigation was approved by the ethics committee of the university hospital freiburg , germapatient characteristics are summarized in .tab.2. treatment technique all patients received a diagnostic wholebody fdg - pet / ct for staging purposes [ 22 ]  . 
from september 2009 , respiratory gated 4d fdg - pet / ct scans of the tumor region were also acquired . 34 | strahlentherapieundonkologie12013 patients were immobilized using a commercially available vacuum couch on a board with integrated markers [ 23 ]  . 
 planning ct scans with 3 - mm slice thickness were performed by a helical ct scanner ( siemens sensation 16 , siemens , forchheim , germany ) in mid ventilation , as well as in breathhold in inhale and exhale position . to account for respiratory tumor motion , an internal target volume ( itv ) was created , including the gross tumor volumes ( gtvs ) from either the mid - ventilation and breathhold ct or , if a fourdimensional ct was applicable , in maximum inhale and exhale tumor position over the breathing cycle . 
for the planning target volume ( ptv ) definition , a safety margin of 4 mm in all directions was added to the internal target volume ( itv )  . treatment plans were calculated with the oncentra master plan ( nucletron , veenendaal , the netherlands ) , using a type b algorithplans were calculated for and applied by a varian linac ( varian medical systems , palo alto , usa ) using 6 - mv photon energy . 
the ptv was enclosed by the 60% isodose ( on which the dose was prescribed )  . patient positioning was verified using a kv cone beam prior to each fraction [ 24 ]  . follow - up follow - up was done 6 weeks after sabr , then every 3 months . 
sabr was performed with total doses of 35 gy ( 5 fractions ) or 37.5 gy ( 3 fractions ) prescribed to the 60% isodose line encompassing the planning target volume . 
standardization in reporting the dose prescription for sabr is needed to allow comparison of different series in order to determine optimum dosage . keywords stereotactic ablative radiotherapy non - small cell lung cancer optimum dose schedule toxicity metastasis stereotaktische ablative strahlentherapie mit mittlerer dosis bei kleinen lungentumoren . 
die patienten wurden mittels sabr mit einer gesamtdosis von 35 gy ( 5 fraktionen ) oder 37 , 5 gy ( 3 fraktionen ) behandelt , die dosisverschreibung erfolgte auf die 60% isodose am rand des strahlentherapie - planungsvolumens ( ptv , planning target volume )  . 
eine standardisierte darstellung der dosisverschreibung wird vor allem fr die vergleichbarkeit von patientenkollektiven untereinander als notwendig erachtet . schlsselwrter stereotaktische ablative strahlentherapie nichtkleinzelliges bronchialkarzinom optimales dosisschema toxizitt metastase rence could not be definitely excluded by ct , an fdg - pet / ct was performed . 
in six lesions ( 13% , 2 nsclc , 4 pulmonary metastases ) , equivocal findings without clear progression were seen in imaging during the follow - up period . in four lesions in 3 patients ( 8.9% ) , local recurrence after sabr occurred . 
.fig.2 shows the kaplan - meier curve for progression - free survival for all patients , patients with nsclc , and patients with metastases . overall , 15 patients ( 38.5% ) developed distant metastases during follow - up . 
3 response assessment in ct and pet with respect to the revised recist criteria and eortc recommendations ( [ 8 , 38 ] ) pr ( partial response ) cr ( complete response ) ctcriteria complete regression of tumor in size , no lesion visible on ct regression of tumor in size , tumor still visible on ct no change in tumor size or shape equivocal finding on ct , not possible to distinguish between tumor and fibrosis / pneumonitis pd ( progressive disease ) clear progression in tumor size nc ( no change ) ne ( not evaluable ) fdg - petcriteria complete regression of fdg uptake decrease in fdg uptake unchanged findings diffuse fdg uptake in treatment area , indistinguishable between tumor and fibrosis / pneumonitis clear focal increase in fdg uptake consensuscriteria complete regression in tumor size and no fdg uptake regression in tumor size and / or decreased fdg uptake no pr nor pd equivocal findings in ct and diffuse fdg uptake in treatment area , not possible to distinguish between tumor and fibrosis / pneumonitis by either method clear progression in tumor size and / or focal increasing fdg uptake tab . 
4 target volume and dose characteristics of organs at risk alllesions ( n = 45 ) nsclc ( n = 29 ) metastases ( n = 16 ) targetvolumeanddose characteristics median volume gtv ( ml ) median volume itv ( ml ) median med . 
no ctc of grade 2 or higher skin reactions , hematologic changes , or esophagitis were observed . one patient with nsclc treated for a tumor close to the thoracic wall reported chest wall pain in the scapula region during the first 6 months after sabr . 
no grade 3 or higher eortc / rtog late pulmonary toxicity was observed . discussion the favorable results shown in our patient population are in line with literature reports by other groups . 
they reported a total response rate of 80% with 33% complete responses and 47% partial responses with mild toxicity [ 21 , 28 ]  . other authors also reported favorable results concerning local control and toxicity after the application of higher doses and / or other ways of dose prescription . 
published a dose escalation trial in 20 patients with nsclc and 41 patients with pulmonary metastases , in which 3 fractions of 10 gy , 3 fractions of 1212.5 gy to the 65% isodose , or 1 fraction of 26 gy to the 80% isodose encompassing the ptv were compared . 
reported on a dose escalation trial of 47 patients with medically inoperable stage - i lung cancer , beginning at 24 gy in 3 fractions prescribed to the 80% isodose encompassing the ptv . 
as shown by several investigators , fdg - pet / ct has a high negative predictive value in the differential diagnosis of tumor recurrence after radiotherapy [ 38 , 39 , 40 , 41 ]  . 
therefore , beyond ct criteria , response assessment was made using criteria including the fdgpet information in analogy to the current eortc recommendations [ 25 , 26 ]  . some limitations have to be addressed concerning the data presented here . 
however , as this evaluation serves to broaden the database of the internationally published clinical data on sabr , we felt it was necessary to publish this series . as in other series , the dose prescription in our patients was not uniform , which led to a certain inhomogeneity of the cohort . 
some authors [ 33 , 42 ] even advocate an isotoxic dosage concept without a fixed dose regimen to the tumor . strahlentherapieundonkologie12013 | 72 gy in tumors larger than 5 cm [ 14 ]  . 
irradiated 91 patients with peripheral lung tumors with a mean dose of 54 gy in 3 fractions , and central lesions with 45 gy in 5 fractions , prescribed to the 7585% isodose . 
 [ 32 ] observed favorable overall survival rates and acceptable toxicity in patients with centrally located tumors treated by stereotactic radiotherapy . overall , comparably favorable local control and survival rates were reached in our cohort . 
this is of interest , since , as shown in .tab.1 , the single and total dose , the method of prescription , and therefore the bed in all published series differ considerably . 
 [ 33 ] posed the question of whether the very high dose concepts in sabr might be regarded as overkill and if the application of lower doses might also lead to satisfying treatment results . 
the data of our small retrospective series may support such an argument . the literature on sabr of lung metastases is clearly smaller in comparison to the research reports on early - stage nsclc . 
in our view , for patients with lung metastases , local aggressive treatment will only be of benefit in a mono or oligometastatic situation , where therapeutic control of any other site of malignancy has been achieved . 
in our cohort of patients selected according to this philosophy , we observed local control and survival results similar to those in nsclc advocating the use of sabr also for this indication . in line with the literature , toxicity in our patients was well tolerated . 
onishi h et al ( 2010 ) stereotactic body radiotherapy ( sbrt ) for operable stage i non - small - cell lung cancer : can sbrt be comparable to surgery ? int j radiat oncol biol phys 81 : 13521358 8 . 
palma d et al ( 2010 ) impact of introducing stereotactic lung radiotherapy for elderly patients with stage i non - small - cell lung cancer : a populationbased time - trend analysis . 
onishi h et al ( 2007 ) hypofractionated stereotactic radiotherapy ( hypofxsrt ) for stage i non - small cell lung cancer : updated results of 257 patients in a japanese multi - institutional study . 
int j clin oncol 9 : 352355 time ( months ) literaturkommentiert strahlenther onkol 2013 189 : 9596 doi 10.1007 / s00066 - 012 - 0248 - 3 online publiziert : 10 . 
november 2012 springer - verlag berlin heidelberg 2012 g.goldner klinik fr radioonkologie , medizinische universitt wien signifikanteverbesserung derlokalenkontrollebei melanompatientennach lymphadenektomieund adjuvanterstrahlentherapie originalpublikation burmeister bh , henderson ma , ainslie j et al ( 2012 ) adjuvant radiotherapy versus observation alone for patients at risk of lymph - node field relapse after therapeutic lymphadenectomy for melanoma : a randomised trial . 
bei einem medianen followup von 40 monaten ergab sich eine signifikante reduktion der lokalen lymphknotenrezidivrate durch die adjuvante strahlentherapie : 20 / 109 rezidive im rt - arm versus 34 / 109 rezidive im beobachtungsarm ( p = 0 , 041 )  . 
die adjuvante radiotherapie nach lymphadenektomie verbessert bei patienten mit erhhtem lokalrezidivrisiko die kontrollrate signifikant und sollte solchen patienten immer angeboten werden . kommentar der stellenwert einer adjuvanten bestrahlung bei melanompatienten war bislang umstritten . 
 aus einzelnen kliniken , und deren ergebnisse kontrovers [ 4 , 5 ]  . basierend auf den resultaten einer vorangegangenen phase - ii - studie zur adjuvanten radiotherapie nach lymphadenektomie bei melanompatienten ( trog 96.06 ; [ 2 ] ) wurde die aktuell publizierte studie initiiert . 
erstmalig konnte nun mit einem randomisierten vergleich klar nachgewiesen werden , dass durch eine zustzliche bestrahlung zur lymphadenektomie das risiko eines lk - rezidivs nach 3 jahren signifikant reduziert wird , hier nmlich von 31% auf 19% . 
 es ist zu erwarten , dass sich in der folge durch die optimierte lokale kontrolle auch die lebensqualitt verbessern wird , nmlich durch vermeidung von lymphdem , ulzera und bewegungseinschrnkung . 
doch die auswertung der spttoxizitt und lebensqualitt stehen noch aus . im weiteren krankheitsverlauf wird sich auch zeigen , inwieweit sich durch die etablierung einer effektiven systemtherapie diese durch den einsatz der adjuvanten radiotherapie verbesserte lokale kontrolle auch in einer signifikanten verlngerung des progressionsfreien bzw . 
burmeister bh , henderson ma , ainslie j et al ( 2012 ) adjuvant radiotherapy versus observation alone for patients at risk of lymph - node field relapse after therapeutic lymphadenectomy for melanoma : a randomised trial . 
burmeister bh , smithers bm , burmeister e et al ( 2006 ) a prospective phase ii study of adjuvant postoperative radiation therapy following nodal surgery in malignant melanoma trans tasman radiation oncology group ( trog ) study 96.06. 
fuhrmann d , lippold a , borrosch f et al ( 2001 ) should adjuvant radiotherapy be recommended following resection of regional lymph node metastases of malignant melanoma ? br j dermatol 144 : 6670 5 . 
head neck 19 : 589594 die in der rubrik literatur kommentiert seit 2010 erschienenen beitrge sind online verfgbar unter 96 | strahlentherapieundonkologie12013 original article strahlenther onkol 2013 189 : 1825 doi 10.1007 / s00066 - 012 - 0236 - 7 received : 19 june 2012 accepted : 17 september 2012 published online : 15 . 
november 2012 springer - verlag berlin heidelberg 2012 k.fakhriant.sauers.klemmc.bayerb.hallerm.mollsh.geinitz klinikum rechts der isar , technische universitt mnchen , munich radiotherapywithorwithout chemotherapyinthetreatment ofanalcancer : 20 - yearexperience fromasingleinstitute squamous cell anal cancer ( sq - ac ) is a rare disease and comprises only 13% of all digestive system malignancies . 
today , defini tive rct with 5 - fluoruracil ( 5 - fu ) and mitomycin c ( mmc ) is considered to be the gold standard in the treatment of anal cancer . 
the results of three phase iii trials in the 1990s supported this concept , demonstrating a favorable outcome and a preservation of the anal sphincter function in a majority of the patients [ 7 , 8 , 9 , 10 ]  . 
 the aim of our study was to report the efficacy and toxicity of rct for sq - ac at a single center and to evaluate the prognostic factors influencing outcome . patients and methods patient population the medical records of all patients treated with rct for anal carcinoma in our department between 1988 and 2011 were retrospectively reviewed . 
inclusion criteria were histologically proven squamous cell carcinoma of the anal canal and / or anal margin , no distant metastases , and external beam radiation treatment with or without chemotherapy . 
the staging evaluation included the history , physical examination ( digital rectal exam and palpation of the groin ) , endoscopy with biopsy , and computed tomography of the chest / abdomen / pelvis . 
of the 85 living patients , 49 ( 37 women and 12 men ) could be contacted and interviewed regarding persisting chronic side effects . 5 - fu + mmc chemotherapy was administered to 116 patients ( 84% ) , 2 patients ( 1% ) received 5 - fu alone , and 1 patient ( 1% ) received mmc only . 
nineteen patients ( 13% ) were treated with radiotherapy alone because of comorbidities ( n = 9 ) , t1n0 category ( n = 4 ) , patients refusal ( n = 3 ) , and age ( n = 3 )  . 
follow - up evaluations were performed every 34 months for the first 2 years , and then annually by clinical examination , endoscopy , and computed tomography ( ct ) / magnetic resonance imaging ( mri )  . treatment statistical methods a two - dimensional conventional technique ( n = 13 patients , 9% ) was used in the 1980s and early 1990s . 
three - dimensional conformal radiotherapy ( n = 108 patients , 78% patients ) , intensity - modulated radiotherapy ( imrt ; n = 9 patients , 7% ) and helical tomotherapy ( ht ; n = 8 patients , 6% ) were established in 1993 , 2009 , and 2009 at our department , respectively . 
 radiotherapy consisted of 3645 gy ( 1.8 gy per fraction ) to the lower part of the pelvis covering the primary tumor bed as well as the perirectal , presacral , internal iliac , external iliac , and inguinal nodes . 
disease - free survival ( dfs ) was defined as the time interval between the start of the treatment and a new locoregional failure , metastasis , or death from any cause . 
in 4 patients , there was no information registered regarding the clinical response , recurrence , or distant metastasis after the treatment but information about the date of death and absence / presence of a colostomy were available . 
cx concomitant chemotherapy , 2d 2d conventional radiotherapy , 3d 3dconformal radiotherapy , ecog eastern cooperative oncology group performance status before treatment , conv 2d conventional planning , conf conformal planning ( 3d , imrt , ht ) , os overall survival , dfs disease - free survival , cfs colostomy - free survival , cuinc . 
lr cumulative incidence of local recurrence ain 12 patients grading could not be further defined according to medical charts bpatients with treatment discontinuation before a radiation dose of 50 gy ( n = 6 ) were excluded from this group caccording to tnm classification , 7th edition results recurrence colostomy - free survival ( cfs ) was defined as the time interval between start of the treatment and colostomy or death . 
the cumulative incidence function for colostomy and local recurrence , considering death as a competing risk , were estimated using the library cmprsk of the statistical software r , version 2.14.1 ( r development core team , vienna , austria )  . 
a two - sided level of significance of = 5% was used for all statistical tests . median follow - up time for surviving patients from the start of rct was 98 months ( range 1236 months )  . 
in 19 patients ( 14% ) , a distant metastasis was diagnosed after a median time of 19 months ; the most common site of distant metastasis was the liver ( n = 11 ) followed by the lung ( n = 5 )  . patterns of failure are demonstrated in .fig.4. 
local recurrence was observed in a total of 16 patients after a median time of 19 months ( 2127 ) ; and additional inguinal involvement in 2 patients ; in 1 case the inguinal recurrence was in - field . 
the cumulative incidence for local recurrence at 2 and 5 years was 82 and 113% , respectively . univariate and multivariate analyses results of the univariate and multivariate analyses to identify prognostic factors for os , dfs , and cfs are displayed in .tab.1andtab.2. 
t category , uicc clinical stage ( .fig.2 ) , histologic grading ( .fig.3 ) , and ecog performance status were significantly associated with os , dfs , and cfs , radiotherapy techstrahlentherapieundonkologie12013 | abstract zusammenfassung strahlenther onkol 2013 189 : 1825 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0236 - 7 k.fakhriant.sauers.klemmc.bayerb.hallerm.mollsh.geinitz radiotherapy with or without chemotherapy in the treatment of anal cancer : 20 - year experience from a single institute abstract purpose . 
a consecutive cohort of 138 patients with ct1 - 4 , cn0 - 3 , cm0 sq - ac were treated with rct between 1988 and 2011 at our department . 
the survival rates at 2 , 5 , and 10 years were 883 , 824 , and 596% , respectively , with a median overall survival ( os ) of 167 months . 
in the multivariate analysis , uicc ( international union against cancer ) stage i - ii , female gender , eastern cooperative oncology group ( ecog ) performance status of 01 , and good / moderate histologic differentiation ( g12 ) were significantly associated with a better os , dfs , and cfs . 
future studies are needed to investigate the role of a more intensified ( systemic ) treatment for patients with unfavorable prognostic factors such as t3 / t4 , n + , and / or poor cell differentiation . keywords radiotherapy anal carcinoma squamous cell carcinoma anal canal outcome strahlentherapie mit oder ohne chemotherapie bei der behandlung des analkarzinoms : 20 - jhrige erfahrungen einer klinik zusammenfassung zielsetzung . 
eine konsekutive kohorte von 138 patienten mit ct14 , cn03 , cm0 , plattenepithelkarzinom des anus , wurde im zeitraum zwischen 1988 und 2011 mit einer r ( c ) t in unserer klinik behandelt . 
in der multivariaten analyse waren das stadium iii nach uicc ( union internationale contre le cancer ) , ein weibliches geschlecht , ein easterncooperative - oncology - group ( ecog ) - performance - status von 01 und eine gute bzw . 
weitere studien sind ntig , um die rolle einer intensivierten ( systemischen ) therapie fr patienten mit ungnstigen prognostischen faktoren , wie positivem lymphknotenstatus , t3 / t4 und / oder schlechte zelldifferenzierung , zu untersuchen . schlsselwrter radiotherapie analkarzinom plattenepithelkarzinom analkanal ergebnis nique was significantly associated with dfs and cumulative incidence of local recurrence , female gender was significantly associated with dfs , and n category significantly correlated only with os and cfs . 
 since t and n category define the uicc clinical stage , we performed two multivariate analyses , one without the t and n category ( .tab.2 ) and another without the uicc . 
4 8 patterns of failure in 30 of 124 patients with complete remission after radiochemotherel , t and n category replaced the uicc and all other factors ( gender , ecog , and grading ) were included in the analysis as in the first model . 
patients with a lower t category ( p = 0.006 ) or a better performance status ( p < 0.001 ) had a significantly lower estimated cumulative incidence for colostomy . 
patients whose treatment was discontinued and received a radiation dose smaller than 50 gy ( n = 6 ) were excluded to avoid negative selection in the group with lower radiation doses . 
patients with larger tumors ( t3 / t4 ) were treated with higher median doses ( 58 gy ) compared to patients with smaller tumors ( t1 / t2 , 54 gy ) ; thus the poor os for patients with higher doses appears to be due to the higher proportion of patients with advanced disease in this group . 
analysis of the impact of more advanced radiotherapy techniques on outcome was difficult to perform as there was no event observed in the more recently used advanced techniques ( ht / imrt ) , which were applied to 17 patients ( 13% ) with a short median follow - up time of 20 months ( 432 months )  . 
the most common grade 3 chronic side effects were dyspareunia in 35% ( 13 from 37 ) of female patients , vaginal symptoms ( dryness , itching , and burning ) in 22% ( 8 from 37 ) of female patients , fecal incontinence in 13% ( 6 from 47 ) of patients , and increased stool frequency in 8% ( 4 of 47 ) of patients . 
 we did not observe any relationship between the radiation dose and other acute or late toxicity ( data not shown )  . discontinuation of treatment treatment had to be discontinued for 8 patients . 
in 2 patients , radiotherapy ( without concomitant chemotherapy ) had to be stopped after two fractions ( 3.6 gy ) , in 1 of the patients because of acute chest pain and in the other because of continuous excessive tumor bleeding . 
both patients had multiple synchronous disease , comorbidities , and poor general condition ( ecog 3 ) , one suffered from chronic obstructive pulmonary disease and had a history of myocardial infarct and apoplex and diabetes and the other suffered from coronary heart disease with aortic and mitral valve replacement and liver cirrhosis . 
this patient had a local recurrence 2 years later and underwent local excision ; he died 12 years later at the age of 75 independent of sq - ac . colostomy colostomy was performed on 24 patients : in 4 patients prior to rct in order to prevent ileus due to a large obstructive tumor mass , 1 patient due to chronic stool incontinence after rct , 2 patients after 22 | strahlentherapieundonkologie12013 tab . 
a more accurate clinical examination in patients with classic symptoms such as rectal bleeding , anal discomfort , or pain , which are usually attributed to benign conditions such as hemorrhoids , is needed to identify patients in early stages and thereby improve the outcome . 
in our group of patients , only 2% failed to achieve a complete or partial remission and only 11% experienced a recurrence after 5 years , which indicates the high effectivity of rct for sqac . 
in our series , the clinical stage was a significant prognostic factor for os , dfs , and cfs , and the t category as the cofounder of the clinical stage had a stronger impact on outcome than the n category did , which is in line with other studies [ 12 , 13 ]  . 
whereas some authors do not observe any impact of gender on outcome [ 12 , 18 ] , our data support the hypothesis that female patients might have a better outcome than male patients [ 7 , 22 , 23 ]  . 
 in the multivariate analysis of our series , tumors with a good / moderate histologic differentiation ( g1 / g2 ) were significantly associated with better outcomes , which is in line with the reported results of chapet et al . 
as individualized treatment is now in the spotlight , more attention should be placed on the possible impact of histologic and biologic characteristics of tumors to optimize the treatment results . 
nccn guidelines recommend a minimum dose of 45 gy for all patients and an additional boost of 1014 gy to a total dose of 5559 gy for patients with t3 , t4 , or node - positive disease or t2 with no response [ 26 ]  . 
however , the incidence of acute ( hematologic and nonhematologic ) and late toxicity ( anal ulcers , stenosis , and necrosis ) is also dose - dependent and prohibitive [ 31 , 32 ]  . 
we did not observe any improvement in outcome beyond a radiation dose of 54 gy for larger tumors or for smaller tumors , but a significant increase in the incidence of acute toxicity of grade 3 or higher such as radiodermatitis and rectal pathe role of concomitant chemotherapy is the most investigated issue in radiotherapy of sq - ac . 
prospective randomized trials have tried to replace at least one of the two cytostatics with cis platin , whose activitiy against squamous cell carcinoma has been well - known for decades [ 22 , 33 ]  . 
cisplatin - based rct , while offerstrahlentherapieundonkologie12013 | original article ing no advantage in efficacy , offers a viable alternative to mmc because of its different toxicity profile [ 34 ]  . 
in a preliminary report of an rtog phase ii study ( rtog 0529 ) , the outcomes with imrt combined with 5 - fu and mmc were compared with those from the 5 - fu / mmc control arm of the rtog 9811 trial , which used nonconformal radiation techniques [ 40 ]  . 
of note , the patients in the rtog 9811 trial received a radiation dose up to 59 gy , but in the rtog 0529 study the maximum dose for patients with higher stages was 54 gy , which might also have an impact on reduction of acute toxicity . 
in our group of patients , despite a significant higher dfs and lower cumulative incidence for local recurrence for conformal plans , the radiotherapy technique had no significant impact on os or cfs according to univariate analysis . 
nccn guidelines suggest performing a pet scan ( combined with contrast - enhanced ct ) as a component of 24 | strahlentherapieundonkologie12013 the pretreatment staging evaluation for sq - ac [ 26 , 41 ]  . 
although petct might lead to a better capture of involved sites into the target volume , the small number of pet - staged patients in our study and the shorter follow - up time do not allow a conclusive statement to be made regarding the benefit of pet - ct . 
 regardless , there is evidence that a pet scan can alter the management of sq - ac : in a study of 61 patients with sq - ac , pet scaning changed the radiation portals in 13% of patients [ 42 ]  . 
in treatment planning of other tumor entities , pet could reduce the interobserver variability significantly compared to mri [ 43 , 44 , 45 , 46 ]  . in a retrospective analysis of 235 patients with a median follow - up time of 5 years , sunesen et al . 
 [ 47 ] report that after curative - intent radiotherapy or rct , one third of their patients had a tumor - related colostomy , of which one - third were related to therapy . 
almost 70% of their patients did not receive chemotherapy and the rest of the patients were given mostly cisplatin - based chemotherapy , and none of them received mitomycit is well - known that concomitant chemotherapy improves local control and outcome [ 7 , 17 ]  . 
for example , the rtog 9811 trial reported 5 - year incidences of colostomy of 19 and 10% after cisplatin - based and mitomycin - based rct , respectively [ 48 ]  . 
 all phase iii prospective randomized trials in sq - ac sought to clarify the role of chemotherapy and to determine the most effective regimen in the combined treatment of sq - ac . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . nachruf strahlenther onkol 2013 189 : 8788 doi 10.1007 / s00066 - 012 - 0277 - y online publiziert : 28 . 
nie hat er sich auch whrend seines spteren berufslebens irgendwie dieser schweren behinderung wegen geschont , sondern im gegenteil jede herausforderung angenommen , die das klner ordinariat ihm auferlegte und seine fachgesellschaft ihm antrug . wie sein vater entschloss er sich zum medizinstudium , um arzt zu werden , und immatrikulierte sich an der universitt mnster . 
die anerkennung als facharzt fr radiologie erfolgte1979 ; 1980 wurde er zum oberarzt der klinik ernannt . herrn mllers wissenschaftliche interessen betrafen das gesamte spektrum der radiologie , die dynamischen entwicklungen in der schnittbilddiagnostik ( ct ) wie auch in der bildgesttzten therapieplanung und der beschleunigertechnologie . 
seine wissenschaftlichen aktivitten waren diagnostisch , therapeutisch und experimentell ausgerichtet : lymphographie , computertomographie , xeroradiographie ebenso wie die endolymphatische radionuklidtherapie , die strahleninduzierte lungenfibrose und die experimentelle und klinische hyperthermie . 
weitere arbeiten beschftigten sich mit lokalen mikrozirkulationsstrungen nach hochvoltbestrahlung anhand von in - vivo - po2 - messungen und mit der prognostischen bedeutung von zytogenetischen befunden bei einer vielzahl von malignen tumoren . 
 diese forschungen bildeten die grundlage fr die habilitation und die erteilung der venia legendi im jahre 1982 . die beschftigung mit augentumoren war auch der beginn seiner intensiven internationalen ttigkeit , die ihn schon frh in die usa nach philadelphia an die hahnemann university zu luther brady fhrte . 
zwischen beiden mnnern entwickelte sich eine tiefe freundschaft , die spter auch der entwicklung der deutschen radioonkologie wesentliche impulse gab . eine besondere auszeichnung durch die deutsche rntgengesellschaft war 1982 die verleihung des hermann - holthusen - rings . 
1984 koordinierte er als leitender oberarzt den umzug der neuen klinik fr strahlentherapie radioonkologie , insbesondere der teletherapie , in das neue klinikum der wwu in mnster , womit eine moderne strahlentherapie etabliert wurde , u . 
durch einfhrung der ct - gesttzten therapieplanung und der individuell geformten abschirmblcke am therapiesimulator . seine herausragenden leistungen in forschung , lehre und krankenversorgung , wie auch seine engagierte rztliche ttigkeit veranlassten 1985 die universitt zu kln , rolf - peter mller an die dortige klinik und poliklinik fr radioonkologie zu berufen , die er zunchst kommissarisch und ab 1987 dann als direktor in abb . 
 ( mit freundlicher genehmigung von frau barbara mller ) strahlentherapieundonkologie12013 | nachruf der nachfolge von horst sack bis zu seinem tod im september 2012 fhrte . das klinisch - wissenschaftliche engagement von rolf - peter mller umfasste zeitlebens ein breites methodenund themenspektrum und wurde getrieben von immerwhrender neugier und einem enormen innovationsdrang . 
hierbei ragen zwei aktivitten besonders erfolgreich hervor : die weiterentwicklung der therapie des morbus hodgkin und die langjhrige leitung der arbeitsgemeinschaft radiologische onkologie ( aro ) der deutschen krebsgesellschaft , die zahlreiche international vielbeachtete klinische studien im deutschsprachigen raum generieren und begleiten konnte . 
seit 1986 war er ber viele jahre mitglied im board und panel , seit 1998 dann selbst der leiter der referenzstrahlentherapie der ghsg und leiter des teilprojekts strahlentherapie im rahmen des kompetenznetzes maligne lymphome mit dem schwerpunkt qualittssicherung . 
in anerkennung seiner vielfltigen aktivitten ernannte ihn die radiological society of north america ( rsna ) im jahre 2005 zu ihrem ehrenmitglied . der werdegang von rolf - peter mller spiegelt typischerweise auch die entwicklung der deutschen radiologie bzw . 
jahrestagung in baden - baden . mit dem tod von rolf - peter mller verlieren wir eine prgende persnlichkeit 88 | strahlentherapieundonkologie12013 und einen der engagiertesten und konsequentesten kmpfer fr die sache der radioonkologie , vor allem im deutschsprachigen rau er begleitete viele junge menschen auf dem weg in die radioonkologie , und zwar sowohl in der krankenversorgung als auch in forschung und lehre in einer unnachahmlich frdernden und fordernden weise . 
die rztliche verantwortung und betreuung seiner schwerkranken patienten waren ihm immer ein besonderes anliegen und prgten seine klinische arbeit nachhaltig . unser mitgefhl gilt besonders seiner frau barbara , die ihn ber viele jahre treu begleitete und in den letzten lebensjahren auch hingebungsvoll pflegte , und seinem sohn maximilian . eich , pd haverkamp ( mnster ) , ptter ( wien ) , sauer ( erlangen ) korrespondenzadresse h.t. 
november 2012 springer - verlag berlin heidelberg 2012 excellent survival rates after treatment for ( pediatric ) hodgkins lymphoma ( ( p ) hl ) have motivated research efforts toward the minimization of long - term side effects that lead to impaired health - related quality of life [ 21 , 40 , 43 , 44 ]  . 
several clinical trials of the gpoh - hd and more recently the euronet - phl studies treated young patients with combined radiochemotherapy resulting in excellent overall survival [ 37 ]  . 
within different study generations , the target volume ( tv ) has been reduced from extended - field to involved - field ( if ) and since the hd90 trial to modified - involvedfield ( mif )  . 
although positron emission tomography ( pet ) after two cycles of chemotherapy was reported to have a prognostic value regarding treatment outcome [ 15 ] , the target definition for phl is still based on prechemotherapy imaging . 
tv reduction to the remaining pet - positive nodes after chemotherapy is being evaluated by the ongoing ghsg - hd18 adult hl trial [ 16 ] for advanced disease stages . intensity - modulated photon radiotherapy ( imxt ) or protons with multimodality imaging for target definition have so far not been considered in phl studies . 
patients underwent pet / computed tomography ( ct ) on hybrid scanners ( with a ct slice thickness of 3 mm ) at the time of diagnosis and after two chemotherapy cycles ( oepa )  . structure delineation tv and oars were delineated according to two different protocols by a radiation oncologist experienced in phl in consensus with a nuclear medicine physician . 
the standard clinical tv ( ctv1 ) ( reference ) was defined according to the euronet - phl study ( mif technique ) encompassing the involved lymph nodes ( ln ) at the time of diagnosis adapted to the postchemotherapy anatomy . ctv2 was designed utilizing interimpet information , i.e. , ctv2 was based on pet - positive lns after two chemotherapy cycles [ 26 ]  . 
breast tissue and , for prepubertal patients , the mammillae were contoured with an isotropic margin of 5 cm . treatment techniques the prescribed isocenter dose was 19.8 gy ( 11 fractions ) [ 23 ]  . 
the investigated treatment techniques were two opposed 6 - , 10or 15 - mv photon fields ( 2f ; standard technique ) , imxt with seven 6 - mv beams ( 0 , 51 , 103 , 154 , 206 , 257 , 309 ) , and a single anterior proton field ( ps ) ( tvs predominantly located in the anterior left side of the body )  . 
the maximum proton energy was 250 mev , the spacing between the proton energy layers was 0.8 , and the margin to the distal ptv edge was 0.5 cthe lateral spot size and distance between the center of spots were based on previous studies [ 20 ]  . 
for protons , a relative biological effectiveness value of 1.1 was assumed [ 22 ]  . imxt and ps plans were accepted if at least 95% of the ptv was covered by the 95% isodose ; for 2f plans the 90% isodose volume was regarded as sufficient . 
for inverse planning , patient - specific dose volume constraints were applied because of the rather individual anatomy . treatment plan analysis patient - averaged ptv mean ( dmean ) and median doses ( d50% ) , near maximum ( d2% ) , and near minimum doses ( d98% ) were evaluated . 
for quantification of the treatment plan quality , the homogeneity index hi [ 23 ] organ - equivalent dose for secondary malignancy , consideration of the organ - equivalent dose ( oed ) concept was adopted [ 48 ] : where vt is the total organ volume , di the dose in one bin of the dvh , and v ( di ) the volume receiving di . 
the organ - specific doseresponse relationship for carcinoma induction ( red ) was calculated using a mechanistic model [ 49 ]  . and the conformity index ci [ 41 ] , were calculated . 
tvpi represents the ptv subvolume encompassed by the 95% isodose , tv the total ptv , and pi the volume of the 95% isodose . oar doses were compared using dosimetric parameters ( dmean and d2% ) and averaged dose - volume histograms ( dvhs )  . 
for bones , the red function was adapted for sarcoma induction [ 51 ]  . statistical analysis evaluation parameters were compared using the wilcoxon rank - sum test and regarding 2f plans as reference . 
oar - related parameters and significance levels ( with respect to 2f technique ) are summarized in .tab.3and.tab.4. applying ptv2 instead of ptv1 reduced oeds by ~ ( 5410 ) % for all oars ( p < 0.05 , except breasts )  . 
hdvol of the right breast could be reduced to under 0.1% for imxt and for protons , for both ptvs . for 46 of 10 patients ( depending on treatment technique ) no doses were observed at all , explained by undeveloped breast tissue or favorable ptv positions . 
for 10 patients , the planning target volume ptv1 was based on initial ct tumor extension and ptv2 on anatomy - related pet - positive lymph node levels after chemotherapy . 
the treatment techniques investigated ( prescribed dose 19.8 gy ) comprised opposed - field ( 2f ) , intensity - modulated photon ( imxt ) , and single - field ( ps ) proton techniques . 
the combination of an adaptive target volume definition with protons could contribute to future phl treatment concepts . keywords pediatric hodgkins lymphoma intensity - modulated photon therapy protons positron emission tomography / computed tomography long - term side effects kann die behandlung von pdiatrischen hodgkin - lymphomen durch pet - bildgebung und protonenbestrahlung verbessert werden ? zusammenfassung ziel . 
fr 10 patienten wurde das planungsvolumen ptv1 ( planning target volume ) auf der initialen ctbasierten tumorausdehnung und ptv2 auf den anatomischen bereichen , welche petpositive lymphknoten nach chemotherapie umfassten , bestimmt . 
die untersuchten bestrahlungstechniken ( zieldosis : 19 , 8 gy ) umfassten 2 - felder - photonen ( 2f ) , intensittsmodulierte photonen ( imxt ) und einfelderprotonen ( ps )  . 
die verwendung von ptv2 statt ptv1 reduzierte d2% des herzens von 14 auf 9 gy und dmean der schilddrse von 16 , 6 auf 2 , 7 gy fr alle bestrahlungstechniken . 
ps showed a decrease of these parameters by 5 and 25% for ptv1 and ptv2 , respectively . the thyroid showed the highest oed values of all oars but they were comparable for all treatment techniques for a given ptv concept . 
dvhs for the right lung were similar , although dmean was lower by ~2 gy and hdvol by ~55% . ptv2 decreased the ldvol , mdvol , and hdvol by ~50% ( p < 0.05 ) for all techniques . 
oed was slightly reduced using imxt instead of 2f ; ps reduced oed by ~50% . discussion if and mif represent the standard tv definition in phl [ 28 ]  . 
 the most radiosensitive organs regarding secondary cancer probability ( scp ) in children are the breasts and thyroid [ 3 , 24 , 40 , 52 , 54 ]  . 
the part of the breast volume receiving more than 4 gy ( v > 4 gy ) was considered in detail owing to a remarkably increased risk of breast cancer [ 18 ] for these volumes . 
to decrease the risk of secondary breast cancer one could further optimize proton therapy [ 2 ]  . ptv2 led to dose reductions in the thyroid because it was hardly included in the radiation field . 
since increased thyroid cancer risk with rising dose in the low - dose region ( < 20 gy ) is known [ 4 ] , the dose reduction reported in our study needs to be emphasized . lung and heart exposures can lead to organ dysfunction , which affects quality of life . 
valvular defects were reported in children for doses of 3545 gy , but there is no information about the deterministic risks for doses below 20 gy [ 46 ]  . 
changes of the lung , as reported in literature [ 10 ] for doses from 11 to 14 gy , may not be expected , since for both lungs the dmean was lower than 8 gy . for quantification of radiation - induced scp , the oed concept was applied [ 51 ] , which considers mutation , killing , repopulation , repair , and fractionation . 
all fitting parameters applied were derived from patients treated with conventional radiotherapy and have not been validated for imxt so far [ 51 ]  . regarding the induction of leukemia , bone marrow irradiation plays a minor role , since chemotherapy has the largest impact [ 1 , 3 ]  . 
growth arrest should be irrelevant for patients in this study , because it was not reported for doses below 20 gy [ 6 ] and phl is rarely observed in children younger than 6 years . secondary malignancies are observed even after low - dose exposure [ 5 , 12 , 39 ]  . 
v < 6 gy increased using imxt instead of 2f , but was reduced to 1% for ps . irrespective of ptv definition , there is a potential benefit of modern radiotherapy in children [ 42 , 53 ]  . 
unfortunately , limited data are available to quantify the effect of reduced nontarget volume exposure to high doses against the danger of increased low - dose volumes [ 27 ] , which needs special attention . 
moreover , the increased dose at more distant regions [ 11 , 29 , 47 ] is an effect that cannot be quantified by a treatment planning systeproton therapy is known for minimizing low - dose regions [ 35 , 38 ] , although there is a general difference in the neutron and secondary particle contribution depending on the proton - delivery technique [ 7 , 19 , 35 , 47 , 53 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . laudatio strahlenther onkol 2013 189 : 8990 doi 10.1007 / s00066 - 012 - 0267 - 0 online publiziert : 15 . 
dies hat vielen jngeren kollegen eine ebenso anspruchsvolle wie solide ausund weiterbildung zum radioonkologen ermglicht . wegweisend fr die versorgung stationrer patienten war die einrichtung einer interdisziplinren onkologischen tumorstation gemeinsam mit der klinik fr hmatoonkologie der mhh , was nicht nur den patienten , sondern auch den kollegen in der weiterbildung zugutekam und - kommt . 
insbesondere auf dem gebiet der brustkrebsgenetik resultierten hieraus und resultieren weiterhin zahlreiche hochrangige internationale publikationen . im kampf um die studentischen unterrichtsstunden bei der umstellung auf den modellstudiengang ist ihm eine ausgezeichnete prsenz der strahlentherapie in der lehre gelungen . 
auflage vor und dient auch strahlentherapeuten als schnelle orientierung im klinikalltag und jngeren kollegen zur kompakten vorbereitung auf die facharztprfung . durch seine ttigkeiten im ausschuss strahlenschutz in der medizin und als mitglied des din - normenausschusses hat er unserem fachgebiet das notwendige gehr verschafft und bei bedarf fr das notwendige korrektiv gesorgt . 
nicht unerwhnt bleiben soll auch seine initiative zur abfassung des grundlegenden positionspapiers der degro im jahre 2001 zur lage der deutschen strahlentherapie ein warnruf ! die einrichtung der rztlichen stelle niedersachsen / bremen nach strahlenschutzrecht hat er mageblich vorangetrieben und war bis zu seinem eintritt in den ruhestand deren vorsitzender . 
dass er seinem nachfolger eine modern ausgestattete , interdisziplinr vernetzte und zertifizierte abteilung bergeben konnte , dafr hat es von seiner seite kontinuierlicher und beharrlicher anstrengung bedurmit dem notwendigen augenma untersttzte er bereits 4 jahre zuvor die grndung eines medizinischen versorgungszentrums und schuf damit die volaudatio gress in hannover , der unter dem motto radioonkologie , zielgerichtet auf ein leben mit qualitt stand . 
 insbesondere die schlichtungsstelle fr arzthaftpflichtfragen der norddeutschen rztekammern nutzt weiterhin umfangreich seine fachliche expertise . einmal quer durchs land verlief der werdegang von johann karstens von kiel , wo er studiert hatte , ber aachen , wo er an der rwth zum strahlentherapeuten ausgebildet wurde und sich habilitierte , nach hannover und passau , der heimat seiner frau . 
wir wnschen ihm fr die zukunft alles gute , eine weiterhin robuste gesundheit und die ntige gelassenheit , die dinge auch mal laufen zu lassen . michael bremer , andreas meyer und frank bruns , hannover korrespondenzadresse m . 
november 2012 springer - verlag berlin heidelberg 2012 c.nieder department of oncology and palliative medicine , nordland hospital , bod ergebnisseeinerrandomisierten phase - iii - studiezurbehandlung rezidivierterglioblastome novottf - 100aversuschemotherapie originalpublikation stupp r , wong et , kanner aa et al ( 2012 ) novottf - 100a versus physicians choice chemotherapy in recurrent glioblastoma : a randomised phase iii trial of a novel treatment modality . 
nach vollstndiger rasur der kopfhaut und installation der erforderlichen komponenten wurden die patienten in der handhabung des gerts instruiert und nahmen dann die kontinuierliche behandlung im normalen umfeld auerhalb der klinik vor . 
 das mediane berleben war vergleichbar ( 6 , 6 monate im novottf - 100a - arm versus 6 , 0 monate mit chemotherapie ; 1 - jahres - berleben jeweils 20% ; p = 0 , 27 )  . 
im chemotherapie - arm wurden mehr grad - 3und grad - 4 - nebenwirkungen registriert ( 4% hmatologische , 3% gastrointestinale , 3% vaskulre , 7% zns , 6% andere )  . 
dresemann g , weller m , rosenthal ma et al ( 2010 ) imatinib in combination with hydroxyurea versus hydroxyurea alone as oral therapy in patients with progressive pretreated glioblastoma resistant to standard dose temozolomide . 
prados md , schold sc , fine ha et al ( 2003 ) a randomized , double - blind , placebo - controlled , phase 2 study of rmp - 7 in combination with carboplatin administered intravenously for the treatment of recurrent malignant glioma . 
stupp r , wong et , kanner aa et al ( 2012 ) novottf - 100a versus physicians choice chemotherapy in recurrent glioblastoma : a randomised phase iii trial of a novel treatment modality . 
bent mj van den , brandes aa , rampling r et al ( 2009 ) randomized phase ii trial of erlotinib versus temozolomide or carmustine in recurrent glioblastoma : eortc brain tumor group study 26034 . 
bedenkt man das mediane pfs von etwas ber 2 monaten und die tatsache , dass nur wenige patienten dann noch andere therapien erhielten , ist das mediane berleben erstaunlich lang . 
in den letzten jahren mehren sich die anzeichen fr 94 | strahlentherapieundonkologie12013 die bedeutung dieser therapieform [ 2 , 3 ] , wenn auch bisher nicht in form randomisierter studien . 
da nur eine begrenzte stichprobe daten zur lebensqualitt beigetragen hat , wre es interessant zu erfahren , ob die geringere toxizitt der novottf - 100a - behandlung auch dazu fhrt , dass die patienten diesen ansatz einer chemotherapie vorziehen . 
da mit der zulassung des novottf - 100a die ohnehin schon unbersichtliche rezidivtherapie von glioblastomen nicht einfacher geworden ist , darf mit spannung auf den abschluss einer weiteren studie gewartet werden . 
ziel der vorliegenden arbeit ist es , auf basis der vorhandenen evidenz und unter einbeziehung der modernen schrittmacherund icd - technologie ein interdisziplinres sicherheitsprotokoll zu entwickeln , um das patientenrisiko zu minimieren . methoden es wurde eine systematische literaturrecherche in den medizinischen elektronischen datenbanken medline , embase und cochrane library durchgefhrt und durch eine handsuche ergnzt . 
die datenbanken wurden auf die folgenden suchbegriffe hin untersucht : pacemaker ( pacemaker cardiac , pacemaker permanent , pacemaker artificial ) oder implant able cardioverter defibrillator ( implantable cardioverter defibrillator automatic ; defibrillator implantable ) und radiation therapy ( radiotherapy )  . 
2 therapeutische bestrahlung bei patienten mit herzschrittmachern : aapm - empfehlungen ( 1994 ; [ 29 ] ) beschleuniger - typ durchfhrungder bestrahlung keine verwendung eines betatrons es liegen nur daten fr linearbeschleuniger , betatrons und telekobaltgerte vor ; die anwendung anderer strahlentherapiegerte sollte nur nach individueller abwgung und mit vorsicht erfolgen herzschrittmacher sollten nicht im therapeutischen ( direkten ) strahlenfeld lokalisiert sein vor therapiebeginn sollte die am herzschrittmacher zu erwartende dosis abgeschtzt werden falls gesamtdosis > 2 gy : herzschrittmacherabfrage vor therapiebeginn und evtl . 
zu beginn jeder therapiewoche ; zwischen einer kumulativen dosis von 210 gy knnen frhe parametervernderungen auf einen drohenden ausfall des herzschrittmachers hindeuten genaue patientenbeobachtung whrend erster therapiesitzung mit einem linearbeschleuniger patienten - monitoring aapm american association of physicists in medicine , gy gray potentielle auswirkungen therapeutischer bestrahlung auf aktive implantate die auswirkungen einer strahlentherapie auf implantierte herzschrittmacher und defibrillatoren schwanken zwischen keinerlei funktionsnderungen und dem irreversiblen verlust der gertefunktion . 
moderne linearbeschleuniger und nicht mehr gebruchliche betatrone erzeugen zustzlich ein elektromagnetisches feld [ 16 , 23 , 46 ]  . als ionisierende strahlen werden heutzutage vorwiegend ultraharte rntgenoder elektronenstrahlung verwendet . 
ab energien > 5 mev ( mega - elektronenvolt ) zeigen die beiden am besten untersuchten strahlenarten , namentlich gammaund elektronenstrahlung , gleichwertige streffekte auf die komplementren halbleiterbauelemente ( cmos , complementary metal oxide semiconductor ) , die in modernen herzschrittmachern und icds verwendet werden [ 29 ]  . 
im vergleich zu frher ( ~1970 ) gebruchlichen schaltkreisen ist die cmos - technologie verlsslicher sowie platzund energiesparender , weist allerdings gleichzeitig eine erhhte empfindlichkeit gegenber strahlendosen im therapeutischen bereich auf [ 23 , 46 ]  . 
ob und in welcher form sekundre gertestrungen auftreten , ist aufgrund des komplexen aufbaus moderner herzschrittmacher und icds faktisch nicht vorherzusagen [ 23 , 25 , 27 , 46 , 52 ]  . 
kritische fehlfunktionen umfassen eine vernderte wahrnehmung ( sensing ) , eine vernderte stimulationsleistung ( erhhte oder verminderte stimulationsamplitude oder - frequenz ) , vernderte tachyar rhythmietherapien ( bei icds ) , eine vorzeitige batterieerschpfung sowie einen verlust der telemetrie ( .tab.1 ; [ 23 , 25 , 27 , 46 , 50 ] )  . 
die auf einen herzschrittmacher oder icd abgegebene dosis wirkt kumulativ [ 25 , 27 , 46 ]  . je nach strahlengenerator knnen auch elektromagnetische interferenzen zustzlich strend auf die funktion von herzschrittmachern und icds wirken [ 8 , 25 , 46 ]  . 
 allerdings ist das elektromagnetische feld am linearbeschleuniger in der regel vergleichsweise schwach , so dass diese risiken bei der therapeutischen bestrahlung eher hypothetischer natur sein drften . inhalt und aktualitt der aapm - empfehlungen .tab.2 fasst die wesentlichen aspekte der aapm - empfehlungen von 1994 zusammen [ 29 ]  . 
zustzlich zu den herkmmlichen antibradykarden einund zwei - kammer - systemen ist mittlerweile auch die implantation von systemen zur kardialen resynchronisationstherapie ( crt ; synonym fr biventrikulre oder drei - kammersysteme ) fest etabliert . 
 in aktualisierte empfehlungen einflieen zu lassen . in - vitro - studien zielparameter aller durchgefhrten invitro - studien waren funktionsstrungen und / oder - ausflle von herzschrittmachern oder icds , hervorgerufen durch strahleninduzierte schden oder elektromagnetische interferenz . 
bestrahlt wurde , bis auf gesondert betrachtete ausnahmen , an zusammenfassung abstract strahlenther onkol 2013 189 : 517 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0243 - 8 m.dorenkampc.strombergerc.vonheymannw.haverkampp.wustm.roser strahlentherapie bei patienten mit herzschrittmachern oder implantierbaren kardioverter - defibrillatoren . 
es werden konkrete sicherheitsempfehlungen zum patientenmanagement vorgestellt , die ohne weiteres von einrichtungen , die strahlentherapeutische leistungen anbieten , bernommen werden knnen . schlsselwrter implantierbare kardioverter - defibrillatoren ionisierende strahlung elektromagnetische interferenz interdisziplinres gesundheitsteam krankheitsmanagement radiation therapy in patients with cardiac pacemakers or implantable cardioverter defibrillators . 
with increasing numbers of implanted pacemakers and implantable cardioverter defibrillators ( icd ) and a rising incidence of malignant tumors , there is a growing probability of radiation - mediated device dysfunction . 
 the search yielded 147 articles published between 1994 and 2012 of which 45 met the selection criteria and of these studies 34 presented primary data ( 9 in vitro and 25 in vivo studies )  . 
practical recommendations for patient management and safety are presented that can be readily adopted by any institution carrying out radiation therapy . keywords implantable cardioverter - defibrillators ionizing radiation electromagnetic interference interdisciplinary health team disease management strahlentherapieundonkologie12013 | tab . 
 [ 57 ] konnten in den schrittmacherelektroden 8 | strahlentherapieundonkologie12013 strahlentherapieinduzierte spannungspulse bis zu 1 , 2 mv registriert werden ( austritt von ladung an den bestrahlten grenzflchen )  . 
diese gre reicht theoretisch aus , um ein irregulres verhalten des herzschrittmachers zu verursachen ( inhibition der stimulation mit bradykardie / asystolie oder vorhofgetriggerte schnelle ventrikelstimulation ; [ 8 , 57 ] )  . 
die erste klinisch potentiell ernsthafte strung ( stimulationspause > 10 s ) trat bemerkenswerterweise schon bei 0 , 15 gy auf , der erste systemausfall bei 0 , 5 gy ( kompletter stimulationsverlust ; [ 34 ] )  . 
whrend der bestrahlung zeigten 8 / 19 ( 42 , 1% ) der systeme eine inhibierte stimulation , bei 6 der betroffenen systeme trat dieser effekt bei dosisfraktionen < 5 gy auf . 
eine woche nach abschluss der bestrahlungsserie zeigten 5 / 19 ( 26 , 3% ) der ursprnglich ungebrauchten schrittmacheraggregate den eri - ( elective replacement interval ) austauschindikator , also eine vorzeitige batterieerschpfung an . implantierbarer kardioverter - defibrillator ebenfalls aus der arbeitsgruppe von hurkmans et al . 
bis zur maximal applizierten gesamtdosis von 120 gy fielen alle 11 untersuchten systeme aus , 3 / 11 ( 27 , 3% ) bereits bei geringen dosen von 1 , 5 gy . 
 in 4 / 11 ( 36 , 4% ) aller gerte kndigte sich ein ausfall an , wenn die schockenergie auf therapeutisch mglicherweise nicht mehr effektive werte absank ( abfall von nominalen 30 j auf minimal 18 j ) ; bei 2 / 11 ( 18 , 2% ) icds war dies bereits bei einer dosis von 0 , 5 gy der fall [ 18 ]  . 
bei insgesamt 4 / 11 ( 36 , 4% ) aller systeme kam es durch den bestrahlungsvorgang zu ventrikulrem oversensing , welches von den icd - detektionsalgorithmen flschlicherweise als eine maligne ventrikulre tachyarrhythmie ( kammerflimmern und / oder ventrikulre tachykardie ) interpretiert wurde . 
 [ 54 ] demonstrierten in einer subanalyse zur vorgenannten studie , dass eine direkte bestrahlung des icd - aggregats ab einer dosis von 0 , 5 gy regelhaft zu strahleninduzierten artefakten und mitunter zur fehldetektion von kammerflimmern und / oder kammertachykardien fhren kann ( .tab.4 , [ 18 ] )  . 
man beobachtete weder strahlenbedingte elektrische aggregatneustarts ( resets ) noch sich im verlauf manifestierende sptfolgen . smtliche in den in - vitro - studien beschriebenen strungen , sowohl von herzschrittmachern als auch von icds , wurden durch ionisierende strahlung verursacht . 
 [ 6 ] schildert die bestrahlung von rechtsatrialen und - ventrikulren metastasen mit einer gesamtdosis von 37 , 5 gy bei einem patienten mit einem zwei - kammer - schrittmacher . 
die radiotherapie des mammakarzinoms war bei mehreren schrittmachertrgerinnen ebenfalls ohne gertefehlfunktion durchfhrbar ( .tab.5 , [ 5 , 31 , 37 ] )  . implantierbarer kardioverter - defibrillator der erste icd - bezogene bericht stammt von hoecht et al . 
in keinem der flle lag das icd - aggregat im therapeutischen feld , so dass smtliche resets durch streustrahlung verursacht wurden ( dosis < 0 , 5 gy ; [ 11 , 15 , 26 , 51 ] )  . 
 ( kein pm im feld ) 237 , 2 gy ( pm partiell im feld ) < 2 gy ( n = 32 ) , > 2 gy ( n = 5 ) 0 , 1460 gy ( pm partiell im feld ) keine fehlfunktionen 0 , 26 gy ( pm - sonden im feld ) passageres ventrikulres undersensing , keine manifeste fehlfunktion 0 , 231 , 03 gy < 2 gy ( n = 59 ) , > 2 gy ( n = 1 ) keine fehlfunktionen reset mit fallback - modus ( n = 1 ) < 0 , 10 , 3 gy 0 , 1 gy 948 gy ( pm partiell im feld ) keine fehlfunktionen keine fehlfunktion keine fehlfunktion falls nicht anders gekennzeichnet , beziehen sich die ergebnisse auf photonenund / oder elektronenbestrahlungaai vorhof - ein - kammer - schrittmacher ( herzschrittmacherbetriebsart ) , ddd zwei - kammer - schrittmacher ( herzschrittmacher - betriebsart ) , gy gray , gye gray equivalent , hf herzfrequenz , k . 
das auftreten von inappropriaten schocks whrend einer strahlenbehandlung wurde bislang nicht berichtet . alle in - vivo beschriebenen herzschrittmacherund icd - strungen fhren die autoren aller genannten berichte auf die effekte ionisierender strahlung zurck . 
belege fr strungen oder defekte durch elektromagnetische interferenz fanden sich keine , in einem fallbericht wurde lediglich darber spekuliert [ 60 ]  . auswirkungen von neutronen und protonenstrahlen im vergleich zu photonen und elektronen ist die datenlage zu anderen strahlenarten sehr eingeschrnkt . 
a. dosisicd < 0 , 5 gy mammakarzinom 50 gy bronchialkarzinom larynxkarzinom squamses lungenzellkarzinom 56 gy 60 gy 59 , 4 gy ( zieldosis ) exposition der icdsonde < 0 , 5 gy 2 , 5 gy k . 
 ( kein icd im feld ) gelblum [ 11 ] 681 gy 0 , 012 , 9 gy autor hoecht [ 15 ] john [ 19 ] thomas [ 51 ] sepe [ 44 ] nemec [ 36 ] lau [ 26 ] kapa [ 20 ] ferrara [ 9 ] croshaw [ 5 ] soejima [ 45 ] prostatakarzinom betroffene regionen : kopf - hals , thorax , abdomen betroffene regionen : kopf - hals , thorax , abdomen , becken , untere extremitten betroffene regionen : kopf - hals , thorax , abdomen , becken mammakarzinom ( 3 - mal ) betroffene regionen : kopf - hals , thorax , mamma , becken ( gesamtkollektiv ) mammakarzinom 879 , 2 gy keine fehlfunktionen < 1 gy ( n = 6 ) , > 1 gy ( n = 2 ) 3438 , 5 gy 2074 gy ( gesamtkollektiv ) 0 , 991 , 68 gy max . 
0 , 478 gy keine fehlfunktionen keine fehlfunktionen auswirkung reset mit fallback - modus ( n = 1 ) , identische strung nach austausch durch baugleiches icd - aggregat batterieerschpung , schockimpedanz > 125 ( icd - sondenbeschdigung ) reset mit fallback - modus keine fehlfunktion unkontrollierte frequenzzunahme ( runaway icd ; hf 175 / min ) ; induktion einer polymorphen vt , kardiopulmonale reanimation reset mit fallback - modus keine fehlfunktionen reset mit fallback - modus ( n = 2 ; beide icds nicht im strahlenfeld ) menard [ 31 ] alle ergebnisse beziehen sich auf die bestrahlung mit photonenund / oder elektronengy gray , hf herzfrequenz , k . 
trotz einer errechneten protonendosis von jeweils 0 gy an allen schrittmacheraggregaten traten bei 2 patienten fehlfunktionen auf ( elektrischer reset mit aktivierung eines fallback - modus und abweichung von der programmierten stimulationsfrequenz )  . 
dadurch wurden zahlreiche strahleninduzierte gertefehler sichtbar , die man bei einer oberflchlichen standardabfrage mit dem programmiergert nicht entdeckt htte [ 14 ]  . herstellerempfehlungen die hersteller geben teilweise sehr unterschiedliche ausknfte darber , wie im falle einer strahlentherapie bei patienten mit herzschrittmachern oder icds zu verfahren ist , und bis zu welchen kumulativen dosen ihre gerte belastbar sind ( .tab.7 , [ 2 , 4 , 30 , 48 , 49 ] )  . 
jude medical gibt fr schrittmacher dosen von 20 30 gy an , fr boston scientific gibt es keinen dosisschwellenwert , unterhalb dessen eine sichere gertefunktion garantiert werden kann [ 4 , 48 ]  . 
sehr uneinheitlich sind die empfehlungen in bezug auf eine kardiologische evaluation vor therapiebeginn , auf die gerteabfragen vor , whrend und nach einer strahlentherapeutischen sitzung sowie auf das vitalfunktionen - monitoring whrend einer bestrahlung . 
7 empfehlungen von herzschrittmacherund icd - herstellern empfehlung biotronik [ 2 ] medtronic [ 30 ] bostonscientific [ 4 ] st.judemedical [ 48 , 49 ] diskussion bewertung der vorliegenden evidenz ja ( 3 cm ) ja ( 3 cm ) < 10 mev strahlenenergie < 2 gy < 2 gy 2030 gy keine sichere dosis keine sichere dosis < 5 gy < 5 gy originalien gerteverlagerungausdem primrstrahlenfeld tolerierbare gertegesamtdosis abschirmung desimplantiertengerts ( bleischutz ) vortherapiebeginn evaluation durch kardiologen gerteabfrage vortherapiesitzung gerteabfrage whrendtherapiesitzung patienten - monitoring nachtherapiesitzung gerteabfrage icd : therapiedeaktivierung ja ( durch programmierung ) k . 
a. ja ( durch programmierung oder externe magnetauflage ) ja , nach der ersten therapiesitzung ; danach wchentliche abfragen fr die dauer der strahlentherapie pm : abfrage ; bei aufflligkeiten engmaschige kontrollen icd : durchfhrung eines induktionstests seit erscheinen der aapm - empfehlungen von 1994 hat sich die evidenzbasis zu auswirkungen der externen bestrahlung auf implantierte herzschrittmacher und defibrillatoren betrchtlich erweitert ( .tab.3 , 4 , 5 , 6 )  . 
nicht realistischen gerteprogrammierungen ( ventrikulre wahrnehmung von 0 , 18 mv bei herzschrittmachern ) und bestrahlungsprotokolle sowie die unterschiedliche kategorisierung und damit schwierige vergleichbarkeit der gertefehlfunktionen und ausfallendpunkte sein [ 17 ]  . 
in bezug auf die verlaufskontrollen der gerte und die erfassung von gertefehlfunktionen zeigt sich zwischen den studien eine groe spannbreite , die von nicht durchgefhrten abfragen bis hin zum detaillierten auslesen des rohdatenspeichers reicht , so dass die berichtete zahl von fehlfunktionen mglicherweise unterschtzt ist [ 14 , 45 ]  . 
die teilweise limitierte datenqualitt erfordert eine differenzierte betrachtungsweise der ergebnisse , um sie entsprechend werten und klinische 0 aus ihnen ableiten zu knnen . herzschrittmacher vorhanden ? nein aggregat im strahlenfeld oder kumulative dosis am aggregat > 2 gy ? nein schrittmacherabhngigkeit ? verlagerung des aggregats ? nein umprogrammierung vor bestrahlung nicht notwendig abfrage nach jeder bestrahlung umprogrammierung vor bestrahlung ( programmiergert ) o . 
algorithmus zur durchfhrung einer strahlentherapie bei patienten mit herzschrittmachern interdisziplinre sicherheitsempfehlungen insgesamt scheinen unerwnschte ereignisse im zusammenhang mit der bestrahlung von patienten mit herzschrittmachern oder icds selten zu sefr den individuellen patienten knnen gertefehlfunktionen allerdings ernsthafte konsequenzen haben . 
besonders problematisch erscheinen fehlfunktionen , die mit zeitlicher latenz ( wochen bis monate ) nach therapieabschluss der bestrahlung auftreten und sich als pltzlicher totalausfall manifestieren knnen [ 57 ]  . angesichts dieser ausgangslage stellt sich die wichtige frage , wie eine mglichst sichere bestrahlung von patienten mit herzschrittmachern oder icds bei gleichzeitiger effizienz der klinischen ablufe gewhrleistet werden kann [ 3 , 33 , 39 ]  . 
die empfehlungen orientieren sich an folgenden zentralen zielsetzungen : fmglichst allen patienten mit herzschrittmachern oder icds , die einer strahlentherapie bedrfen , soll diese ohne kompromisse in der therapeutischen wirksamkeit ermglicht werden . 
 falls das herzschrittmacheroder icd - aggregat im direkten bestrahlungsfeld liegt , muss frhzeitig mit der kardiologie oder dem implantierenden zentrum kontakt aufgenommen werden , um die mglichkeit einer gerteverlagerung zu evaluieren und ggf . 
bei berschreiten der dosiswerte muss eine gerteverlagerung evaluiert werden ( siehe punkt a2 )  . strahlentherapieundonkologie12013 | originalien debrillator ( icd ) vorhanden ? nein aggregat im strahlenfeld oder kumulative dosis am aggregat > 1 gy ? nein verlagerung des aggregats ? deaktivierung der tachy - therapien vor bestrahlung ( programmiergert ) o . 
 kardiologische vorstellung : komplette gerteabfrage von herzschrittmacher oder defibrillator , feststellung einer schrittmacherabhngigkeit / bestimmung des prozentualen stimulationsanteils , risikoklassifizierung von icd - patienten ( geringes risiko : patienten mit primrprophylaktischer icd - indikation ohne stattgehabte schockabgaben ; hohes risiko : sekundrprophylaktische icd - indikation oder stattgehabte adquate schockabgaben unabhngig von der icd - indikation )  . 
diese empfehlung beruht auf einer generell hheren stranflligkeit von icds gegenber der einwirkung von ionisierender strahlung und deckt sich mit den empfehlungen anderer autoren [ 16 , 44 , 46 ]  . 
bei der strahlentherapeutischen planung sollten die limitationen der planungs - software bei der dosisschtzung an hochdichten objekten bekannt sein sowie mgliche beeinflussungen der strahlengeometrie durch schrittmacheroder icd - sonden bercksichtigt werden [ 12 , 13 , 41 , 58 ]  . 
die entscheidung zu einer gerteverlagerung sollte nach einer interdisziplinren risikoabwgung getroffen werden und prozedurale komplikationen sowie operabilitt bercksichtigen . zu bestrahlungszwecken temporr notwendige umprogrammierungen ( abb.1 , 2 ) knnen mit hilfe des programmiergerts oder durch auflage eines magneten auf das aggregat erreicht werden . 
whrend der magnetauflage kommt es bei herzschrittmachern in der regel zur asynchronen stimulation mit der magnetfrequenz und bei icds zur deaktivierung der antitachykarden therapien ( die antibradykarde funktion des icd bleibt unberhrt )  . 
die magnetauflage sollte nur zum einsatz kommen , falls der anwender mit ihr vertraut ist und eine sichere und stabile magnetlage whrend der gesamten dauer des bestrahlungsvorgangs gewhrleistet werden kann . 
generell sollten patienten nur so lange wie ntig asynchron stimuliert werden , weil durch kompetitive stimulation mit dem eigenrhythmus vorhofflimmern und / oder maligne kammerarrhythmien ausgelst werden knnen ( stimulation in die vulnerable phase des myokards ; [ 8 ] )  . sollten im rahmen einer strahlentherapie gertefehlfunktionen auftreten , so mssen diese kritisch analysiert werden . 
 eine verbesserte evidenzlage knnte zuknftig zu einer entsprechenden anpassung der empfehlungen fhren . zuknftige untersuchungen und ausblick da es sich bei der einwirkung von ionisierender strahlung auf komplexe halbleiterstrukturen um ein stochastisches geschehen handelt , kann man , vergleichbar zu biologischen systemen , keine risikofreie schwellendosis annehmen . 
die sichtung der verfgstrahlentherapieundonkologie12013 | originalien baren daten zeigt auf der anderen seite , dass komplikationen unterhalb gewisser grenzdosen nur in einzelfllen auftreten ( also raritten darstellen ) , so dass unter beachtung der geschilderten allgemeinen sicherheitskautelen ein akzeptabel niedriges restrisiko in kauf genommen werden kann . 
inzwischen sind die strahlentherapeutischen techniken ( tomotherapie , rapid arc , stereotaxie ) so gut steuerbar und przise ( bildsteuerung ) , dass auch die dosisverteilung innerhalb des implantats und seiner einzelnen komponenten betrachtet werden kann . 
so erwarten wir eine relevante strahlenempfindlichkeit nur fr die elek tronischen platinen , die auf dem planungs - ct in verbindung mit herstellerseitigen informationen ( die dem strahlentherapeuten zur zeit nicht ohne weiteres zugnglich sind ) identifiziert werden knnten , und kaum fr die verkapselung ( also den rand des implantats ) oder die batterie . 
allerdings gibt es darber keine daten , da eine differenzierung einzelner bestandteile des implantats blicherweise nicht erfolgt . desweiteren sind bei der einwirkung ionisierender strahlung auf halbleiterbausteine im laufenden betrieb reversible funktionsstrungen ( durch ladungserzeugung ) und / oder irreversible , langfristige beschdigungen ( durch vernderung der kristallstruktur und im besonderen beschdigungen des speichermoduls ) prziser zu unterscheiden . 
eigentlich sollte es 16 | strahlentherapieundonkologie12013 gelingen , grenzwerte von dosisleistungen in zusammenarbeit mit den herzschrittmacherund icd - herstellern zu ermitteln , die ein akzeptabel niedriges risiko fr eine funktionsstrung implizieren . 
da die modernen beschleuniger eine variation der dosisleistung erlauben , wre sogar ein ( protektives ) absenken sowohl der einzeldosis als auch der dosisleistung um einen faktor 210 mglich , wenn dadurch eine weitgehend risikolose bestrahlung ermglicht wird . die kumulation der dosis im laufe einer bestrahlungsserie kann dann im weiteren verlauf zu dauerhaften ( also irreparablen ) strungen der kristallstruktur von halbleitern , insbesondere in den speicherchips , fhren , die mit funktionsstrungen bis hin zum ausfall einhergehen . 
dabei sind jedoch sowohl physikalische erholungseffekte ( auflsung einer aberranten ladungswolke ) als auch herstellerseitige korrekturverfahren fr die speicherinformation ( backup - speicher ) im laufe von stunden bis tagen mglich . 
 ein sonderfall wre die vorzeitige batterieerschpfung , die durch einen erhhten stromfluss zu erklren ist . die meistens tolerierte kumulative strahlendosis knnte recht hoch sein , wobei man bei der kommerziell verfgbaren technologie von einer resistenz bis zu 50 gy und mehr ausgeht . 
 aufgrund der individuellen empfindlichkeit komplexer halbleiterschaltungen wre hier jedoch ein herstellerabhngiger wert durch ein unabhngiges prfverfahren voraussetzung . fr eine weiterentwicklung von praktischen leitlinien , die ber unsere aktuellen empfehlungen hinausgehen , wre es daher insbesondere sinnvoll , standardisierte prfverfahren zu entwickeln , die sowohl reversible ( von der dosisleistung abhngige ) als auch irreversible ( von der kumulativen dosis abhngige ) strungen erfassen und statistische dosisabhngigkeiten fr implantate ermitteln knnen . 
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dickstein k , vardas pe , auricchio a et al ( 2010 ) 2010 focused update of esc guidelines on device therapy in heart failure : an update of the 2008 esc guidelines for the diagnosis and treatment of acute and chronic heart failure and the 2007 esc guidelines for cardiac and resynchronization therapy . 
hudson f , coulshed d , dsouza e et al ( 2010 ) effect of radiation therapy on the latest generation of pacemakers and implantable cardioverter defibrillators : a systematic review . 
lambert p , da costa a , marcy py et al ( 2011 ) pacemaker , implanted cardiac defibrillator and irradiation : management proposal in 2010 depending on the type of cardiac stimulator and prognosis and location of cancer . 
clin oncol 6 : 211212 tensicherheit der degro / dgmp / vmtro sowie fr die gro / gmp und sasro / sgsmp ( 2012 ) rules and regulations applying to incidents in radiotherapy . 
marbach jr , sontag mr , van dyk j et al ( 1994 ) management of radiation oncology patients with implanted cardiac pacemakers : report of aapm task group no . 
sepe s , schaffer p , krimmel k et al ( 2007 ) irradiation treatment of laryngeal cancer in a patient with an implantable cardioverter - defibrillator ( icd )  . 
soejima t , yoden e , nishimura y et al ( 2011 ) radiation therapy in patients with implanted cardiac pacemakers and implantable cardioverter defibrillators : a prospective survey in japan . 
thomas d , becker r , katus ha et al ( 2004 ) radiation therapy - induced electrical reset of an implantable cardioverter defibrillator device located outside the irradiation field . 
tsekos a , momm f , brunner m et al ( 2000 ) the cardiac pacemaker patient might the pacer be directly irradiated ? acta oncol 39 : 881883 54 . 
vardas pe , auricchio a , blanc jj et al ( 2007 ) guidelines for cardiac pacing and cardiac resynchronization therapy : the task force for cardiac pacing and cardiac resynchronization therapy of the european society of cardiology . 
wadasadawala t , pandey a , agarwal jp et al ( 2011 ) radiation therapy with implanted cardiac pacemaker devices : a clinical and dosimetric analysis of patients and proposed precautions . 
in mehreren kleineren studien wurde ber einen zusammenhang von strahlentoxizitt und genetischer variation auf einzelnukleotidebene ( snps , single nucleotid polymorphism , ein - buchstaben - variation in der dna - sequenz , ) berichtet . 
um die wertigkeit der snp - analysen in bezug auf die toxizitt einer strahlentherapie auf normalgewebe zu untersuchen , wurden insgesamt 1613 patienten mit brustund prostatakarzinomen in 92 unterschiedlichen snps genotypisiert . 
die brustkrebspatienten stammen aus dem cambridge imrt trial isrctn21474421 ( n = 976 ) und einer randomisierten , prospektiven toxizittsstudie , die am christie hospital in manchester durchgefhrt wurde ( n = 34 )  . 
die prostatakarzinompatienten ( n = 637 ) wurden im rahmen des mrc rt01 multizentrischen trials cccip ( n = 224 ) bestrahlt oder erhielten eine hypofraktionierte hoch - dosis - imrt ( isrctn97182923 - studie ; n = 413 )  . 
die bislang publizierten snps , die eine normalgewebetoxizitt vorhersagen sollen , erweisen sich als ungeeignet . kommentar eine unter radioonkologen verbreitete vorstellung weist genetischen faktoren eine wichtige rolle fr die vorhersage der entstehung gravierender nebenwirkungen durch die strahlentherapie zu . 
die wichtigsten faktoren in der pathogenese spter strahlenfolgen sind die lokale dosis ( und fraktionsdosis und dosisinhomogenitt ) in bestimmten zielstrukturen des betreffenden organs sowie die dadurch ausgelsten organspezifischen und pathogenetischen folgeprozesse , die gegebenenfalls durch spezifische biologische interaktionen modifiziert werden knnen [ 2 , 3 , 4 ]  . kritisch an der vorliegenden studie ist zu bewerten , dass keine spezifischen und quantifizierten symptome , sondern nur globale scores fr die auswertung der toxizitt ausgewhlt wurden und nur zu einem zeitpunkt , nmlich 2 jahre nach abschluss der strahlentherapie analysiert wurde . die eindrucksvolle studie von barnett ist sicher ein meilenstein in der forschung zur optimierung der strahlentherapie , weil sie neue mastbe setzt . 
barnett gc , coles ce , elliott rm et al ( 2012 ) independent validation of genes and polymorphisms reported to be associated with radiation toxicity : a prospective analysis study . 
nieder c , pawinski a , andratschke nh et al ( 2007 ) does prophylactic breast irradiation in patients with prostate cancer influence cardiac toxicity ? j natl cancer inst 99 : 16461647 literatur kommentiert um die relation zwischen anatomischer dosisverteilung innerhalb kritischer organe ( nicht volumina ! ) und dem entstehen spezifischer symptome sowie komplexe biologische mechanismen durch interventionelle studien abzubilden . es ist zu erwarten , dass die auswahl erkrankungsspezifischer snps fr die prvention bestimmter kritischer strahlenfolgen besser geeignet wre als breit angelegte reihenuntersuchungen von organunspezifischen snps . 
auch in der studie von barnett wird angedeutet , dass trotz nichtsignifikanter datenlage eine erkrankungsspezifische auswahl definierter genetischer marker fr bestimmte patientensubpopulationen in betracht gezogen werden knnte , um das risiko der toxizitt einer strahlentherapie vorherzusagen . 
therefore , it is necessary to know more about qol changes that occur as a consequence of palliative radiotherapy . to date the number of published studies on qol in patients undergoing certain palliative treatments is limited . 
significant others are often involved in patient care and play an important role in addressing patient needs . there is some evidence that proxies show agreement with patients self - ratings of qol [ 2 , 6 , 10 , 16 , 17 ]  . 
in published studies , european organization for research and treatment of cancer ( eortc ) qol or functional assessment of cancer therapy ( fact ) questionnaires were predominantly administered both to patients and to significant others . 
since such a generic instrument does not adequately address the issues relevant to patients with brain metastases , we developed a new questionnaire , the degro brain module ( dbm )  . the dbm instrument for proxy assessment was first applied in a prospective qol pilot study of the german society of radiooncology ( degro ) quality of life working party [ 18 ] to examine the qol of patients with brain metastases before ( t0 ) and 3 months after radiotherapy ( t3mo ) with a very limited number of 3 - month survivors . 
the patient self - ratings are published elsewhere [ 19 ]  . the current study aimed to investigate the correlation between self - ratings ( eortc questionnaires ) and proxy ratings ( dbm )  . 
the qlq - c15 - pal is a shortened form of the qlq - c30 for use in a palliative care setting , containing 15 items for the following nine domains : physical function , emotional function , global qol , pain , fatigue , appetite , dyspnea , constipation , and sleep . 
for the symptom scales and for all scales of bn20 , high scores indicate severe symptoms . degro brain module the dbm ( appendix 1 ) was developed by the senior author ( c.s. ) taking into consideration the established pos and the self - assessment of qol of patients with 48 | strahlentherapieundonkologie12013 eortc questionnaires qlq - c15 - pal and bn20 . 
the following three items of the dbm are classic symptom scales ( nausea , headache , fatigue ) also found in the eortc - qlq forms and demonstrate typical symptoms of patients with brain metastases . 
questions 7 and 8 indicate emotional function like items 13 and 14 of the qlq - c15 - pal . each of the ten items of the new instrument was scaled 0 ( very poor ) to 4 ( very good ) , resulting in a total score of 040 . 
ethics approval was obtained from the ethics committee at the university of wrzburg , germany . patient and treatment characteristics from january 2007 to june 2010 , 166 patients with previously untreated brain metastases of solid tumors were recruited at 14 centers in germany and austria for this prospective multicenter study . 
the high correlation between self - assessment and proxy ratings as well as a similar change over time for both approaches suggest that in patients with brain metastases , proxy assessment using the dbm questionnaire can be an alternative approach to obtaining qol data when patients are unable to complete questionnaires themselves . 
our self - constructed and first applied dbm is the only highly specific instrument for patients with brain metastases , but further tests are needed for its final validation . keywords brain metastases proxies radiotherapy quality of life questionnaire fremdeinschtzung von patienten vor und nach strahlentherapie bei hirnmetastasen . 
der eortc - qlq - c15 - pal - fragebogen und das hirnspezifische modul bn20 wurden verwendet , um die qol von patienten zu beginn der radiotherapie und nach 3 monaten zu erheben . 
aufgrund der hohen korrelation zwischen selbstund fremdeinschtzung und des hnlichen zeitlichen verlaufs der erhobenen werte bei patienten mit hirnmetastasen und ihren angehrigen kann die fremdeinschtzung mit dem degro - hirnmodul eine alternative darstellen , wenn die patienten die fragebgen nicht selbststndig ausfllen knnen . 
allerdings sind noch weitere untersuchungen fr die abschlieende validierung erforderlich . schlsselwrter hirnmetastasen angehrige bestrahlung lebensqualitt fragebogenset statistical analysis the ratings of each item of all questionnaires were linearly transformed to a 0100 scale , withnot at all conforming to 0 andvery much conforming to 100 [ 1 , 7 ]  . 
for comparison with regard to the central trend of summing up score parameters at t0 and t3mo , the wilcoxon test for paired differences was used , and the significance level was set to p < 0.05. 
1 8 total ( a ) and detailed scores ( b ) of proxy assessment with the degro brain module ( dbm ) before radiotherapy ( rt ) of brain metastases and after 3 months of therapy ( higher scores are equal to better function and qol ) ther explorative analyses , the significance level was set to p < 0.01 to adjust for multiple comparisons ( several scales and groups )  . statistical analyses were performed using the software package statistica ( statsoft , inc . , tulsa , usa , 2010 )  . results questionnaire assessment and survival three of the 141 patients with a proxy rating ( < 2% ) filled in the qlq - c15 - pal questionnaire but did not complete the bn20 . 
two proxies with baseline assessment did not assess the qol at 3 months . for the newly developed degro - lq brain module for the assessment by proxies , cronbachs was determined to be 0.85 ( t0 ) and 0.9 ( t3mo ) , suggesting sufficient reliability of this instrument . most significant others who filled in the questionnaire were spouses : 68% before radiotherapy and 69% after 3 months . 
response rates for proxies in this study were higher than in previous studies using longer instruments , e.g. , a combination of the questionnaires eortc - qlq - c30 and bn20 with a total of 50 questions [ 6 ]  . 
however , the dbm appears suitable to substitute patientrated qol questionnaires . in self - ratings with the eortc - c15pal and bn20 questionnaires [ 19 ] , global qol , physical function , fatigue , nausea , appetite loss , drowsiness , weakness of legs , motor dysfunction , and hair loss worsened significantly during the 3 months after start of treatment , whereas headache remained unchanged . 
thus , the time course for these items is similar between the patient and proxy scores within the respective scales and potentially an indicator of the validity of the newly developed instrument . the study of moinpour et al . 
the authors used the spitzer quality of life index and found a decreased proxyrated qol after 3 months , whereas patients themselves reported a better qol , indicating discrepancies between the two approaches . 
the spitzer instrument is a very short test procedure ( five items ) and not a specific instrument for patients with brain metastases , in contrast to our highly specific instrument ( dbm )  . while other studies on proxy qol assessment for patients with brain metastases [ 6 , 10 , 16 , 17 ] used validated eortc - qlq , fact questionnaires [ 2 , 11 ] , or the spitzer quality of life index for both patients and significant others , we developed a new instrument with only ten questions addressing specifically the proxies of patients with brain metastases and concerning the possibility of estimation by a significant other . 
 [ 6 ] observed a lower agreement in the items fatigue and nausea ( r = 0.40 and r = 0.35 ) in a smaller cohort ( 42 brain tumor patients and their proxies )  . the dbm items 7 and 8 reflect emotional functioning and are comparable to questions 13 and 14 of the eortc - qlqc15 - pal . 
correlations between patients and significant others were slightly lower ( before radiotherapy r = 0.47 and 3 months after r = 0.62 ) than for physical symptoms and similar to ( r = 0.47 , r = 0.4 ) [ 2 , 17 ] or higher than those in other studies ( r = 0.31 ) [ 6 ]  . 
a reason for the lower correlations in the study by giesinger and colleagues [ 6 ] could be ( beside the smaller sample size ) the more heterogeneous study group of patients with gliomas of all malignancy grades . 
one of the key reasons for this finding might be the fact that spouses are more likely to live in the same household than nonspouses , e.g. , children , siblings , or parents . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 4146 doi 10.1007 / s00066 - 012 - 0230 - 0 received : 15 june 2012 accepted : 27 august 2012 published online : 10 . 
november 2012 springer - verlag berlin heidelberg 2012 of all primary tumor types leading to me tastatic spinal cord compression ( mscc ) , breast cancer is the most common one ac counting for more than 20% of cases [ 4 , 7 , 12 , 14 ]  . 
pa tients with an extraordinarily limited re maining life time of 2 months or less are certainly not candidates for decompres sive surgery or longercourse radiothera py , which may take up to 4 weeks . 
pa tients with an expected survival time of only a few months may be considered as candidates for shortcourse multifraction radiotherapy such as 5 fractions of 4 gy given in 1 week . 
patients with a relative ly favorable survival prognosis are bet ter treated with longercourse radiother apy , usually 10 fractions of 3 gy given in 2 weeks , as this regimen results in high er local control rates of mscc than sin glefraction and shortcourse multifrac tion regimens [ 9 , 10 ]  . 
recent data have suggested that patients with an extraordi narily good survival prognosis may ben efit from longcourse radiotherapy with 20 fractions of 2 gy in 4 weeks in terms of better local control of mscc and surviv al when compared to 10 fractions of 3 gy [ 11 ]  . in order to choose the optimal regi men for each patient , it is very important to be able to estimate the patients surviv al time . 
each primary tumor type leading to mscc is different with respect to its d.rades1s.douglas1s.e.schild2 1 department of radiation oncology , university hospital schleswig - holstein , lbeck 2 department of radiation oncology , mayo clinic , scottsdale avalidatedsurvivalscoreforbreast cancerpatientswithmetastatic spinalcordcompression biological behavior and prognosis . 
 this study was performed to design and validate a survival score specifically for patients with mscc from breast cancer . patients and methods a total of 510 unselected breast cancer pa tients treated with radiotherapy alone for mscc between 1995 and 2011 were ret rospectively evaluated . 
the data of 381 of these 510 patients had been included in a previous study generating a survival score for patients with more than 30 different primary tumor types [ 8 ]  . 
criteria for in clusion in the present analysis included motor deficits of the legs due to mscc , no prior surgery or radiotherapy to the cur rently involved parts of the spinal cord , adequate diagnostic imaging including spinal computed tomography ( ct ) or spi nal magnetic resonance imaging ( mri ) , and corticosteroid treatment during ra diotherapy for at least 1 week . 
 the irradiated volumes encompassed one normal vertebra above and below the in volved vertebrae . from the database of the entire cohort of 510 patients , the patients were alter nately assigned to the test group ( uneven numbers , n = 255 ) or the validation group ( even numbers , n = 255 )  . 
four groups were formed : group a ( 3035 points , red columns ) , group b ( 3640 points , green columns ) , group c ( 4145 points , blue columns ) , and group d ( 4650 points , orange columns ) strahlentherapieundonkologie12013 | original article tab . 
in addition , the prognostic factors that were significant in the univariate analysis ( p < 0.05 ) were evaluated in a multivariate analysis with the cox proportion hazards model . 
in the multivariate analysis of the test group , ecog performance status ( p = 0.0006 ) , ambulatory status ( p = 0.0002 ) , no oth er bone metastases ( p = 0.015 ) , no visceral metastases ( p < 0.0001 ) , interval from can cer diagnosis to radiotherapy of mscc ( p = 0.027 ) , and the time of developing mo tor deficits ( p = 0.003 ) remained significant and were included in the survival score . 
the results of the multivariate analysis of the test group are summarized in .tab.3. the 6month survival rates and the corresponding score for each of the five significant prognostic factors are given in .tab.4. 
the survival rates of the validation group were similar to those of the test group . discussion in many cases , mscc carries a poor sur vival prognosis [ 7 ]  . 
in the present study , six independent pretreat ment prognostic factors were identified : ecog performance status , ambulatory status before radiotherapy , other bone metastases , visceral metastases , interval from cancer diagnosis to radiotherapy of mscc , and the time of developing motor deficits . 
although the radiation regimen was not a pretreatment prognostic factor , it was included in the multivariate analy sis in order avoid a potential bias caused by this additional prognostic treatment factor . 
the risk of a hidden bias could not be completely excluded owing to the ret rospective nature of the data included in this survival score . in comparison to other solid tumors , breast cancer patients with mscc have a more favorable survival prognosis [ 7 ]  . 
the fact that breast cancer patients have such a favorable prognosis may explain the finding that longercourse radiotherapy with higher total doses resulted in significantly better survival than shortcourse radiotherapy with lower total doses . 
a recent matched pair analysis has suggested that patients with a very good survival prognosis ben efit from an escalation of the total radia tion dose [ 11 ]  . based on the six independent pre treatment prognostic factors , the sur vival score was designed resulting in the designation of four prognostic groups . 
 group a patients had a very poor sur vival prognosis and may be considered for best supportive care including corti costeroids , analgesic drugs , and physio therapeutic measures or singlefraction abstract zusammenfassung strahlenther onkol 2013 189 : 4146 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0230 - 0 d.radess.douglass.e.schild a validated survival score for breast cancer patients with metastatic spinal cord compression abstract background . 
in the test group , eight pretreatment factors ( age , performance status , number of involved vertebrae , ambulatory status , other bone metastases , visceral metastases , interval from cancer diagnosis to radiotherapy of mscc , time of developing motor deficits ) plus the radiation regimen were retrospectively investigated . 
factors significantly associated with survival in the multivariate analysis were included in the scoring systethe score for each factor was determined by dividing the 6 - month survival rate ( % ) by ten . 
in the multivariate analysis of the test group , performance status , ambulatory status , other bone metastases , visceral metastases , interval from cancer diagnosis to radiotherapy of mscc , and time of developing motor deficits were significant for survival and included in the score . 
 therefore , this score was reproducible and can help when selecting the appropriate radiotherapy regimen for each patient taking into account her survival prognosis . keywords breast cancer metastatic spinal cord compression prognosis survival score radiation regimen ein validierter berlebensscore fr brustkrebspatientinnen mit metastatisch bedingter rckenmarkskompression zusammenfassung hintergrund . 
 in der testgruppe wurden acht prtherapeutische faktoren ( alter , allgemeinzustand , zahl befallener wirbelkrper , gehfhigkeit , andere knochenmetastasen , organmetastasen , intervall von der erstdiagnose der tumorerkrankung bis zur strahlentherapie der mscc , entwicklungszeit motorischer defizite ) und das fraktionierungsschema retrospektiv untersucht . 
 die faktoren , die in der multivarianzanalyse signifikant mit dem berleben assoziiert waren , gingen in den score eder score fr jeden faktor wurde ermittelt , indem die 6 - monatsberlebensrate ( % ) durch zehn geteilt wurde . 
in der multivariaten analyse der testgruppe waren der allgemeinzustand , gehfhigkeit , andere knochenmetastasen , organmetastasen , das intervall von der erstdiagnose der tumorerkrankung bis zur strahlentherapie der mscc und die entwicklungszeit motorischer defizite signifikant mit dem berleben assoziiert . 
in der testgruppe betrugen die 6 - monatsberlebensraten 12% bei 3035 punkten , 41% bei 3640 punkten , 74% bei 4145 punkten und 98% bei 4650 punkten ( p < 0 , 0001 )  . 
der score kann dabei helfen , das am besten geeignete bestrahlungsregime fr die einzelne patientin unter bercksichtigung ihrer berlebensprognose auszuwhlen . schlsselwrter brustkrebs metastatisch bedingter rckenmarkskompression prognose berlebensscore bestrahlungsregime strahlentherapieundonkologie12013 | original article tab . 
group b patients had a 6month survival proba bility of less than 50% and can be consid ered good candidates for treatment with shortcourse multifraction radiotherapy such as 20 gy in 5 fractions over 1 week . 
 group b patients are not likely to live long enough to experience a local recur rence of mscc , which is less common af ter longercourse than after shortcourse radiotherapy [ 9 , 10 ]  . 
thus , patients with a more favorable survival prognosis such as group c and group d patients are the ones most likely to benefit from longer course programs in terms of better local control of mscc . 
ten fractions of 3 gy in 2 weeks is the most frequently used longercourse program for mscc world 44 | strahlentherapieundonkologie12013 wide , which we would recommend for group c patients . 
 a recent matchedpair analysis has sug gested that patients with such a favor able survival prognosis benefit from an escalation of the radiation dose beyond 10 fractions of 3 gy . 
 in patients of score groups b , c , and d , the option of upfront decompressive sur gery in addition to radiotherapy may be indicated , since in a small randomized trial of 101 patients , additional upfront decompressive surgery resulted in better ambulatory function and survival than radiotherapy alone [ 6 ]  . 
however , in ac cordance with this randomized trial , de compressive surgery should be limited to patients with a good performance sta tus , involvement of only one spinal seg ment , and paraplegia not lasting longer than 48 h . in contrast to other scoring systems that have been developed for patients with vertebral metastasis or palliative sit uations and that have included many dif ferent primary tumor types , the present survival score focused on patients with motor deficits due to mscc from breast cancer [ 1 , 2 , 3 , 8 , 13 , 15 ]  . 
therefore , this new score takes into account the patients individual situation more than previous scoring systems , which likely contributes to a better personalization of the treat ment regimen for these patients . to validate the scoring system , the four prognostic groups a to d of the test group were compared with the cor responding prognostic groups a to d of the validation group . 
4 test group : 6 - month survival rates and corresponding scores survivalat6months ( % ) score ( points ) ecogperformancestatus ambulatorystatusbeforeradiotherapy not ambulatory ambulatory before rt otherbonemetastases visceralmetastases intervalfromcancerdiagnosistoradiotherapy ofmscc 15 months > 15 months timeofdevelopingmotordeficits 17 days > 7 days tab . 
on behalf of all authors , the corresponding author states the following : dirk rades has received speakers honoraria from amgen and novartis omcology . original article strahlenther onkol 2013 189 : 2632 doi 10.1007 / s00066 - 012 - 0178 - 0 received : 12 january 2012 accepted : 2 july 2012 published online : 18 . 
november 2012 springer - verlag berlin heidelberg 2012 primary subglottic cancer is a rare malignancy that accounts for 18% of all laryngeal cancers [ 5 , 7 , 10 ]  . 
aggressive surgical resection , such as wide large - field laryngectomy and bilateral paratracheal lymph node dissection , has been performed as the standard and most reliable curative treatment for this type of cancer . 
we therefore carried out a retrospective review to assess the efficacy and toxicity of radiotherapy with or without chemotherapy in patients with subglottic cancer . patients and methods patients a total of 319 patients with laryngeal cancer received radiotherapy at our institution between january 1993 and december 2010 , 19 ( 6% ) of whom presented with primary subglottic cancer . 
the clinical stages were thus diagnosed as t1n0m0 in 1 patient , t2n0m0 in 8 , t3n0m0 in 4 , t3n1m0 in 1 , t4n0m0 in 3 , and t4n2bm0 in 2 , based on the tnm classification defined by the international union against cancer [ 31 ]  . patient and tumor characteristics are shown in .tab.1. 
fifteen patients underwent irradiation to the whole neck , usually with the three - field technique : lateral opposed fields to the upper neck and anterior field to the lower neck . 
clinical target volume ( ctv1 ) included the gtv with a 0.5 1 - cm margin and the cervical , retropharyngeal , supraclavicular , and upper mediastinal lymph node areas . 
planning target volume ( ptv1 ) was defined as the ctv1 plus a 0.51 - cm margfor local boost irradiation , ctv2 comprised the gtv with a 0.51 - cm margin , and ptv2 included the ctv2 plus a 0.51 - cm margthe spinal cord was defined as the organ at risk , and the maximum dose was restricted to 45 gy or lower . 
 the t categories of these 4 patients were t1 in 1 patient and t2 in 3 , and none of them had cervical lymph node metastasis . of the 19 patients , 15 received definitive radiotherapy to the primary tumors with total doses of 7070.2 gy in 3539 fractab . 
1 patient and tumor characteristics 4479 numberofpatients gender women age ( years ) range median performancestatus ( ecog ) indicationforradiotherapy definitive therapy preoperative therapy primarytumorsize ( maximum diameter , mm ) 1050 range median clinicalstage t1n0m0 t2n0m0 t3n0m0 t3n1m0 t4n0m0 t4n2bm0 ecog eastern cooperative oncology group fig . 
patients with advanced tumors ( t34n01 ) received more intensive chemotherapy , consisting of two courses of intravenous chemotherapy with methotrexate ( 30 mg / m2 on day 1 ) , cisplatin ( 60 mg / m2 on day 4 ) , fluorouracil ( 600 mg / m2 / day on days 15 ) , and leucovorin ( 20 mg / m2 / day on days 15 ) , concurrently with radiotherapy . 
furthermore , they also received adjuvant chemotherapy with daily oral tegafur / gimeracil / oteracil potassium or uracil / tegafur for 328 months ( median , 11 months ) after the completion of radiotherapy . follow - up and evaluation criteria patients underwent computed tomography ( ct ) and / or magnetic resonance imaging ( mri ) of the neck 1 month after the completion of treatment and were followed up at 13 - month intervals . 
patients were considered to be locally controlled and disease - free if they showed neither growth of the irradiated tumors nor cervical lymph node metastasis , and no recurrence after irradiation , respectively . acute and late toxicities associated with radiotherapy were evaluated using the radiation therapy oncology group ( rtog ) acute radiation morbidity scoring criteria and the rtog / european organization for research and treatment of cancer late radiation morbidity scoring scheme , respectively [ 3 ]  . 
acute toxicities were defined as radiation - induced toxicities that occurred within 3 months after the beginning of radiotherapy , and late toxicities as those occurring after 3 months . actuarial survival and disease - control rates were calculated according to the kaplan - meier method [ 14 ]  . 
all statistical analyses were performed using the statistical software package spss 11.0j ( spss , chicago , il , usa )  . results tumor control and failure patterns of the 15 patients treated with definitive radiotherapy , 10 ( 67% ) had no evidence strahlentherapieundonkologie12013 | tions , with shrinkage of the radiation field for local boost irradiation after whole - neck irradiation with 43.245 gy in 10 patients . 
all their tumors were completely resected en bloc by laryngectomy . chemotherapy of the 19 patients , 5 received no chemotherapy , including 4 early patients and 1 patient with coexisting pneumonia . 
the standard regimen of chemotherapy for patients with earlystage tumors ( t12n0 ) consisted of weekly intravenous injections of carbo platin ( 90130 mg , dose calculated using the area under the curve , according to calverts formula ) , with daily oral administration of original article abstract zusammenfassung of disease during follow - up periods of 0.310.4 years ( median , 5 years )  . 
no patient developed cervical lymph node or distant metastases after radiotherapy . in contrast , of the 4 patients treated with preoperative radiotherapy and total laryngectomy , 2 had distant metastases in the lung at 8 and 9 months after treatment , while the other 2 patients remained disease - free . 
 the use of chemotherapy together with radiotherapy may enhance treatment efficacy and contribute to larynx preservation through good local control . keywords chemotherapy head and neck cancer radiotherapy squamous cell carcinoma subglottis wirksamkeit und toxizitt der ( chemo - ) radiotherapie bei primrem subglottischem karzinom zusammenfassung hintergrundundziel . 
der einsatz von chemotherapie in verbindung mit radiotherapie kann die behandlungseffizienz erhhen und durch gute lokale kontrolle zur erhaltung des larynx beitragen . schlsselwrter chemotherapie kopf - hals - tumor radiotherapie plattenepithelkarzinom subglottis the 5 - year overall and disease - free survival rates in all the 19 patients were 80 and 63% , respectively . 
2 failure patterns for each treatment according to clinical stage treatment no.ofpatients failure none local distant definitivetherapy chemoradiotherapy t1n0 t2n0 t3n0 t3n1 t4n0 radiotherapy alone t2n0 t3n0 preoperative therapy chemoradiotherapy t4n0 t4n2b radiotherapy alone t4n0 toxicity grade hematologic leukopenia anemia thrombocytopenia skin erythema / moist desquamation mucousmembrane mucositis / pain rtog radiation therapy oncology group tab . 
the therapy - related acute toxicities are shown in .tab.3. regarding late treatment - associated toxicities , there were no severe adverse events of grade 3 or higher . discussion in patients with subglottic cancer treated with surgery alone , 5 - year local control and survival rates of 4770% and 4370% , respectively , have been reported ( .tab.4 , [ 4 , 22 , 27 , 29 ] )  . 
however , aggressive surgery usually results in considerable deterioration in the patients quality of life , particularly in terms of their reduced ability to communicate because of the loss of voice [ 1 ]  . radiotherapy is a nonsurgical treatment option for preserving the larynx in patients with subglottic cancer . 
however , previous studies have been limited , and most published reports include data from small numbers of patients or with short follow - up periods , as shown in .tab.5 [ 8 , 12 , 21 , 27 , 30 ]  . 
 total doses of 6072 gy ( mean , 66 gy ) with 2 - gy daily fractions were delivered in all patients , except for 3 who were treated with palliative intent . 
local control was achieved in 24 of the 43 patients at a median follow - up period of 4.2 years , and the 5 - year local control rate was 52% . 
these results suggest that radiotherapy represents a feasible first - treatment option for subglottic carcinoma , at least in its early stage . despite the fact that more than half of the patients in the present study had advanced tumors of t3 , a 5 - year local control rate of 74% was achieved in patients with subglottic carcinoma , and the larynx was preserved without local recurrence in 53% of patients at a median follow - up period of 5 years . 
furthermore , the local control rate at 5 years reached 82% in patients treated with definitive chemoradiotherapy , while that in patients with strahlentherapieundonkologie12013 | original article local control rate disease - free rate overall survival disease - free survival years years fig . 
2 8 local control and disease - free rates in ( a ) all 19 patients , and ( b ) 11 patients with subglottic cancer treated with definitive chemoradiotherapy . 
3 8 overall and disease - free survival rates in ( a ) all 19 patients , and in ( b ) 11 patients with subglottic cancer treated with definitive chemoradiotherapy t1t2 tumors was 100% . 
platinum , represented by cisplatin and carboplatin , has been commonly used worldwide for the treatment of advanced head and neck carcinomas , including glottic and supraglottic carcinomas [ 9 , 15 , 16 , 19 , 24 , 25 , 26 , 28 , 34 ]  . 
 several recent studies found that concurrent chemoradiotherapy contributed not only to better local control , but also to better survival , compared to induction chemotherapy followed by radiotherapy [ 6 , 9 , 23 ]  . 
furthermore , some reports suggested that concurrent chemotherapy with uracil / tegafur or tegafur / gimeracil / oteracil potassium , along with radiotherapy , improved both local control and larynxpreservation rates , even in early - stage t2 glottic tumors [ 17 , 18 , 20 , 33 ]  . 
even a total dose of 70 gy in conventional fractions may possibly be insufficient to eradicate t2 tumors by radiotherapy alone . the optimal radiation field for subglottic carcinomas also remains unknown . 
pathologic examinations following surgery for subglottic carcinoma have suggested that the frequency of lymph strahlentherapieundonkologie12013 | original article node metastasis varies from 4 to 50% , with the paratracheal lymph node being the commonest site of metastasis [ 4 , 5 , 10 , 11 ]  . 
lymph drainage from the subglottis is known to follow three routes : the anterior route penetrates the cricothyroid membrane and drains to the prela ryngeal ( delphian ) and pretracheal lymph nodes , while the remaining bilateral posterolateral routes penetrate the cricotracheal membrane and drain to the paratracheal and superior mediastinal lymph nodes [ 10 , 35 ]  . 
in the current study , we included the whole neck and superior mediastinal lymph node area within the radiation field in most patients and none developed lymph node metastasis after irradiation . 
by contrast , several authors have reported a low incidence ( 7% ) of superior mediastinal lymph node metastasis in patients with subglottic carcinoma [ 10 , 12 , 29 , 32 ]  . 
the optimal radiation field for subglottic carcinoma is thus still controversial , with uncertainty over whether or not prophylactic irradiation with the extended - radiation field improves the prognosis of patients , while prophylactic irradiation to the superior mediastinal lymph node may be unnecessary . conclusion radiotherapywassafeandeffectivein patientswithprimarysquamouscellcarcinomaofthesubglottis , andappeared tocontributetolarynxpreservation throughgoodlocalcontrol.theresults suggestthattheuseofchemotherapy , togetherwithradiotherapy , improvestumorcontrol , particularlyinpatientswith locallyadvanceddisease.however , furtherinvestigationsinlargernumbersof patientsarerequiredtodeterminethe superiorityofchemoradiotherapytoradiotherapyaloneinthetreatmentof subglotticcancer . 32 | strahlentherapieundonkologie12013 corresponding address m . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 7480 doi 10.1007 / s00066 - 012 - 0241 - x received : 12 july 2012 accepted : 17 september 2012 published online : 18 . 
november 2012 springer - verlag berlin heidelberg 2012 several studies have shown a relationship between the administered thermal dose and treatment outcome [ 7 , 10 , 15 , 19 , 25 , 31 , 34 , 38 , 39 ]  . 
htp can be used in two ways : ( a ) for calculation of the starting settings only or ( b ) during treatment for htp - guided application of hyperthermia ( ht ) [ 4 , 24 ]  . 
the clinical feasibility of htp - guided steering in the sigma - 60 has been proved ( bsd medical corporation , salt lake city , usa ) [ 14 ]  . clinical exploitation of the full potential of the sigma - eye is hampered by the complexity of sar control . 
when applying the sigma - eye under htp control , the transla74 | strahlentherapieundonkologie12013 r.a.m.cantersm.m.paulidesm.franckenaj.w.mensg.c.vanrhoon department of radiation oncology , erasmus mc daniel den hoed , rotterdam benefitofreplacing thesigma - 60bythe sigma - eyeapplicator amontecarlo - baseduncertaintyanalysis tion of the sar distribution at the monitor to the patient should be with the lowest uncertainty possible . 
to date , the benefit of the sigma - eye applicator was demonstrated for a very limited number of patient models , and the influence of variation in dielectric and thermal tissue parameters was only marginally taken into account [ 30 ] , as was the influence of uncertainty treatment planning and its importance with an increasing number of degrees of freedom [ 12 , 13 , 36 ]  . therefore , this study extensively investigated the theoretical benefit of replacing the sigma - 60 by the sigma - eye applicator , using htp for both applicators in as many as 20 patient models with locally advanced cervical cancer . 
in addition , the robustness of the predicted increase in thermal dose was assessed for clinical conditions , i.e. , by using a monte carlo approach , to investigate the influence of uncertainties in dielectric and thermal tissue properties as well as water bolus shape . patients and methods electromagnetic modeling htp was performed using models of both applicators in the sigma hyperplan software package [ 20 , 33 ]  . 
2 overview of the parameters used with their uncertainties , with permittivity ( r ) , conductivity ( ) , perfusion ( ) , thermal conductivity ( k ) , specific heat ( c ) , density ( ) , blood temperature ( tblood ) , blood - specific heat ( cblood ) , blood density ( blood ) , air temperature ( tair ) , bolus temperature ( tbolus ) , and heat transfer coefficients ( hair - skin and hbolus - skin ) parameter tblood cblood blood tair tbolus hair - skin hbolus - skin aderived from measurements in muscle tissue by gabriel et al . 
in the sigmaeye , central tumor positioning is sometimes not possible owing to the patient and applicator dimensions , leading to a trade - off between central positioning and antennapatient distance . 
to avoid imminent hotspots , the distance between an antenna and the skin of the patient was always more than 3 cto avoid reducing treatment quality , the distance from the tumor center to the applicator center was always less than 5 cm , which was established to be sufficient by canters et al . 
first , a particle swarm optimization was applied to get close to the global minimum , and second a line search algorithm was used to find the actual minimufor sar optimization , the following goal function is used [ 4 , 5 ] : minimizing htq ( hotspot tumor quotient ) will lead to minimization of the 0.1st volume percentile of sar in healthy tissue , while maximizing the sar in the tumor . 
.fig.1 shows an illustration of a patient model inside the sigma - 60 and the sigma - eye applicators . patient models tetrahedral patient models were constructed from 20 computed tomography ( ct ) scans of the patient in hyperthermia treatment position ( i.e. , with the patient lying in the bsd hammock ) with an average of 209 , 690 tetrahedra . 
thermal parameters were from the sigma hyperplan database that is commonly used for uncertainty analysis uncertainty in dielectric and thermal parameters was assessed using a monte carlo analysis based on parameter uncertainties as indicated in .tab.2 and assuming a gaussian distribution [ 1 , 16 , 21 ]  . 
for 1 patient 1 , 000 samples were taken , and the average htq and t90 for the monte carlo analysis using 200 and 1 , 000 samples were compared to assess the influence of sample size . analysis of the results the optimization results without uncertainty were analyzed using a paired analysis ( paired t test ) for 20 patient models . 
the subsequent monte carlo analysis was made with a one - sample t test over the 200 average differences in htq , t50 , and t90 where the average over the 20 patient models was taken . 
this is unlikely to influence the outcome of the 76 | strahlentherapieundonkologie12013 strahlenther onkol 2013 189 : 7480 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0241 - x r.a.m.cantersm.m.paulidesm.franckenaj.w.mensg.c.vanrhoon benefit of replacing the sigma - 60 by the sigma - eye applicator . 
replacing the sigma - 60 by the sigma - eye applicator resulted in a higher sar in the tumor [ on average a decrease of the hotspot tumor quotient ( htq ) by 24% ; p < 0.001 ] , and higher temperatures ( t90 : + 0.4c , p < 0.001 ; t50 : + 0.6c , p < 0.001 ) using literature values and sar optimization . 
based on this uncertainty analysis , significant and clinically relevant improvements in htq and tumor temperature were achieved when replacing the sigma - 60 by the sigma - eye applicator . keywords applicators cervical cancer hyperthermia treatment planning monte carlo analysis thermal dose vorteil des ersatzes des sigma - 60durch den sigma - eye - applikator . 
auf basis einer unsicherheitsanalyse ergibt sich eine signifikante und klinisch relevante verbesserung der tumorsar und der tumortemperatur , wenn der sigma - 60durch den sigma - eye - applikator ersetzt wird . schlsselwrter applikatoren zervixkarzinom hyperthermietherapieplanung monte - carlo - analyse thermische dosis monte carlo analysis . 
each single result making up the boxwhisker plots is the average of 20 patient models between sigma - 60 and sigma - eye . the first line of text beneath the graph shows the p values of a one - sample t test . 
1 , 000 samples for a single patient for htq ( a ) and t50 ( b ) difference of 20 patient models between sigma - 60 and sigma - eye . 
the p value represents the likelihood that the confidence interval of the average over the 200 samples is equal to zero . the second line of text shows the spread of the 200 samples in terms of median and iqr values of the difference between sigma - 60 and sigma - eye . 
all box whisker plots are the result of averaging over 20 patient models . the results of the monte carlo analysis showed that on average , the htq and temperature differences between sigma - 60 and sigma - eye were significantly different . 
the magnitude of the differences between sigma - 60 and sigma - eye was lower , however , than in the case with only literature values of the parameters taken into account . 
the total necessary input power for the displayed temperatures is displayed in .tab.3. discussion the differences in heating quality expressed in an sar or temperature parameter were investigated for two applicators : the sigma - 60 and sigma - eye . evaluation of the methods in this study , the patient models were in the standard position as used in sigma - 60 treatments ( with a kneefix below the knees , thus bending the legs )  . 
owing to the paired analysis study design , we expect only a small influence on the better performance of the sigma - eye . numerical and positioning errors are not included in the monte carlo analysis , which makes it possible that the influence of uncertainties is underestimated . 
we expect that the influence of positioning errors will be largely the same for sigma - 60 and sigma - eye and only small when errors are kept within 1 cm [ 3 ]  . 
numerical errors are expected to be the same for sigma - 60 and sigma - eye calculations , since the patient models are exactly the same , and thus have only little influence on the applicator comparison . 
our investigation into the sample size for a single patient showed that 200 samples are sufficient to reliably assess the influence of uncertainties . the choice of dielectric parameters from the 4 - cole - cole dispersion model fitted on measurements by gabriel is unequivocal in our opinion [ 17 ]  . 
the spread we found in permittivity and effective conductivity , however , is based only on the measurements in muscle tissue in the frequency range around 100 mhz , and therefore is an estimation . 
if we compare these thermal parameters with literature summaries by mcintosh or the itis foundation tissue database , we find small differences for density , specific heat , and thermal conductivity [ 21 , 26 ]  . 
 the results based on data from the literature are plotted separately ( s - 60 sigma - 60 , s - eye sigma - eye , t temperature , htq hotspot tumor quotient , opt optimization ) evaluation of the results sigma - 60andsigma - eye the results in .fig.2 show that for the 20 models of patients with cervical cancer , the sigma - eye applicator improved the sar and temperature distributions after sar or temperature optimization , respectively . 
additionally , on average , both htq and temperature improved significantly by switching from the 4 - antenna sigma - 60 to the 12 - antenna sigma - eye . uncertainty the uncertainty in dielectric parameters caused an average spread of approximately 25% ( iqr ) in htq , both for sigma - 60 and sigma - eye . 
this study , however , demonstrates that these results are generic for all patients with locally advanced cervical cancer and definitively confirms the increased temperature and sar with increasing number of rings and antennas . 
 [ 12 , 13 ] , we found no increased sensitivity for dielectric and thermal parameters with increasing numbers of antennas per applicator . all differences between sigma - 60 and sigma - eye were the result of a paired analysis ( i.e. , a paired t test )  . 
uncertainties in dielectric parameters , therefore , did cause a spread in htq values , but the median difference between the applicators over all samples remained significant . temperature results after htq optimization showed that the addition of uncertainties in thermal parameters led to t50 and t90 values with a median value of 0.20.4c below the values found with literature parameters . 
this means that , owing to the level of uncertainties , sar modeling is equally effective in optimizing the thermal dose in the target as temperature optimization is , and thus can be effectively used in htp - guided steering in the sigma - eye . 
during complaint - based steering , adaptation due to the most relevant of the sar - based hotspots will lead to an optimum , taking into account factors outside the sar - based optimization . the differences between sigma - eye and sigma - 60 in terms of temperatures are lower when uncertainties are taken into account . 
however , the average t50 or t90 difference between the applicators remains significant , with a median benefit of approximately 0.4c for the patient treatment with the sigma - eye applicator , i.e. , an increase of the temperature by nearly 12% . in htq optimization , power consumption for the sigma - eye was clearly higher than for the sigma - 60 . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 6267 doi 10.1007 / s00066 - 012 - 0238 - 5 received : 24 june 2012 accepted : 17 september 2012 published online : 18 . 
november 2012 springer - verlag berlin heidelberg 2012 b.polat1g.wohlleben1a.katzer1c.s.djuzenova1a.technau2m.flentje1 1 department of radiation oncology , university of wrzburg 2 department of otorhinolaryngology , plastic , aesthetic and reconstructive head and neck surgery , university of wrzburg influenceofosteopontin silencingonsurvivaland migrationoflungcancercells osteopontin ( opn ) is a secreted glycophosphoprotein that is overexpressed in many cancer types [ 3 ]  . 
here , we present data on the outcome of opn silencing in a lung cancer cell line . materials and methods cell culture the human lung adenocarcinoma cell line a549 ( non - small cell cancer ) was purchased from the american type culture collection ( atcc , manassas , va , usa )  . 
pcr was carried out starting with 30 s at 98c , followed by 40 cycles : 10 s at 98c ; 20 s at 57 , 3c ; 40 s at 72c ; pcr was ended by one cycle at 72c for 10 mthe pcr products were separated in a 1% agarose gel , stained with ethi dium bromide . 
pcr conditions are mentioned elsewhere [ 13 ]  . western blot analyses after cell lysation , total proteins were run on 412% bis - tris gradient gels ( invitrogen , karlsruhe , germany ) , electrophoretically transferred to polyacrylamide membranes ( invitrogen ) , and analyzed by western blotting . 
polyclonal rabbit anti - opn antibody 017 ( ibl international gmbh , hamburg , germany ) and mouse monoclonal anti - - actin antibody ( sigma , deisenhofen , germany ) were used as primary antibodies . 
briefly , 1105 cells were seeded onto the membrane of the upper chamber in dmem without fcs at a volume of 200 l ( thincert tissue culture inserts for 24 - well plates with 8 - m pore size ; greiner bio - one gmbh , frickenhausen , germany )  . 
the migrated cells were trypsinized and counted . determination of cell cycle distribution cells were seeded on six - well plates ( 2105 / well ) or petri dishes ( 1106 / dish ) , transfected with opn - specific sirna or nonsense rna . 
the fitc brdu flow kit ( bd pharmingen , san diego , ca , usa ) was used to determine the frequency of dna synthesis and was employed according to the manufacturers advice . 
immunofluorescence was measured with a facscalibur flow cytometer ( becton dickinson , san jose , ca , usa )  . clonogenic survival assay cells were irradiated by graded single doses ( 08 gy ) and their survival was analyzed by performing a standard colony formation assay as described elsewhere [ 10 ]  . 
significant differences are marked with * ; a represents one of three , b represents one of two , and c one of three experiments - actin posure point , four replicates were carried out . 
the mean survival data were fitted to the linear quadratic ( lq ) model : sf = exp ( - x x2 ) , where sf is the survival fraction , x is the irradiation dose , and and are the fitted parameters . statistics all experiments were carried out at least twice and data are presented as means ( standard deviation )  . 
statistics and fitting of experimental curves were performed with the origin software ( microcal , northampton , ma , usa )  . results osteopontin silencing after transfection of a549 cells with specific opn sirna , mrna levels were detected strahlentherapieundonkologie12013 | original article abstract zusammenfassung in a semiquantitative and quantitative way using rt - pcr . 
the sirna - mediated opn inhibition was also confirmed on protein levels by western blot analysis ( .fig.1a , b , c )  . effect on cell proliferation the effect of opn downregulation on cell proliferation alone or in combination with irradiation ( 2 gy or 8 gy ) was investigated by daily counting of the cell numbers of untreated or transfected cells over 3 days . 
the combination of opn silencing and irradiation showed a synergistic effect leading to reduced cell survival . keywords radiosensitivity osteopontin lung cancer migration survival einfluss der osteopontinhemmung auf berleben und migration von lungenkarzinomzellen zusammenfassung hintergrundundziel . 
die kombination der opn - downregulation mit einer strahlentherapie zeigte eine synergistische wirkung , die zu einem verringerten zellberleben fhrte . schlsselwrter strahlensensitivitt osteopontin lungenkarzinom migration berleben influence of opn silencing on cell cycle distribution after transfection there was a significant decrease of cells being in s phase in parallel with an increase in the g2 / m phase compared with control cells . 
irradiation with doses of 2 gy led to an increase in the untreated nonsense 8 gy untreated nonsense untreated nonsense 2 gy 0 gy 0 gy 2 gy 8 gy 0 gy 2 gy 8 gy fig . 
 [ 4 ] showed in 96 non - small cell lung cancer patients that after primary treatment by tumor resection , postsurgery opn levels were significantly reduced when analyzed more than 6 weeks later . 
4 8 cell cycle distribution of ( a ) nonirradiated cells and cells irradiated with ( b ) 2 gy and ( c ) 8 gy by opn downregulation after 24 h . 
 [ 9 ] showed that the integrin - binding domain ( rgd ) of opn was essential for tumor growth and metastasis formation but by contrast this was not mediated through increased migration or invasiveness but through nf - bmediated inhibition of apoptosis signaling . 
they demonstrated , in concordance with our findings , an inhibition of cell proliferation , apoptosis , invasiveness , and induction of g1 cell cycle arrest [ 25 ]  . 
in our experiments we used an sirna - based approach to specifically downregulate wild - type opn that is expressed in a549 cells , leading to a consistent reduction of cell migration over time . 
the combination with irradiation showed a synergistic effect with further decrease in migration and proliferation rates . some groups investigated the role of the different opn splice variants ( opn - a , - b , and - c ) in detail . 
 [ 23 ] isolated opn isoforms in plasma samples from 10 healthy persons and 10 non - small cell lung cancer patients and identified opn - a to be mainly upregulated in cancer patients compared to opn - b and - c levels . 
in lung cancer cell lines also including a549 cells , they demonstrated that expression of opn - a was responsible for induction of proteins advancing the epithelial - mesenchymal transition ( emt ) of tumor cells and finally causing a more aggressive phenotype in contrast to the almost counteracting isoform opn - c [ 12 ]  . in our experiments , opn silencing resulted in a reduced proportion of cells arrested during the s phase cell cycle with more cells being arrested in g2 / m phase . 
this effect was reverted after irradiation with 8 gy and induced a decrease in the g0 / g1 phase and an increase in the g2 / m proportion , which is mainly caused by the high radiation dose and excessive cell damage . 
cell cycle arrest in the g2 / m and the g0 / g1 phase , respectively , induced by opn downregulation and irradiation may be the reason for inhibition of cell growth . 
by contrast , they observed an increase in g0 / g1 phase , which we only saw when opn inhibition was combined with irradiation . in the present study we could demonstrate a significant increase in radiation response in the colony forming assay with a reduction of the surviving fraction at 2 gy ( sf2 ) by 29% . 
 [ 7 ] recently published an article where an induction of opn after irradiation was seen in a549 cells by p53 signaling , which in the end led to an inhibition of the apoptotic stimulus caused by radiotherapy . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 6873 doi 10.1007 / s00066 - 012 - 0245 - 6 received : 13 september 2012 accepted : 17 september 2012 published online : 18 . 
november 2012 springer - verlag berlin heidelberg 2012 106ru eye plaques have been used to treat intraocular malignancies for over four decades [ 5 , 22 , 23 , 24 , 25 , 30 ]  . 
this state of affairs does not impede the application of the clinical procedure because the dose prescription is usually made along this axis on the tumor apex and the sclera , but it is clearly insufficient for a precise determination of the effects on other neighboring tissues . 
partly because of these problems , other irradiation techniques are also used for the treatment of ocular malignancies [ 4 , 34 ]  . the available treatment planning system for 106ru plaques is based on simplified physical models of radiation transport and on a very rough approximation of the anatomy of the eye , which is assumed to be a homogeneous water sphere [ 1 ]  . 
indeed , the monte carlo method is generally accepted as the most accurate approach for computing absorbed dose distributions in radiotherapy patients [ 11 , 14 , 27 ]  . 
this is particularly true in the presence of small radiation fields , like the ones used for eye irradiation , where radiation transport cannot be accurately handled by conventional deterministic algorithms usually employed in treatment planning systems [ 6 , 7 , 8 , 10 , 13 ]  . 
the accuracy attained by monte carlo simulations is limited only by the accuracy of the underlying interaction cross - section models and by the sta68 | strahlentherapieundonkologie12013 l.brualla1j.sempau2f.j.zaragoza2a.wittig3w.sauerwein1 1 ncteam , strahlenklinik , universittsklinikum essen 2 institut de tcniques energtiques , universitat politcnica de catalunya , barcelona 3 klinik fr strahlentherapie und radioonkologie , philipps - universitt marburg accurateestimationofdose distributionsinsideaneye irradiatedwith106ruplaques tistical uncertainty inherent in the method . 
 despite these facts , as far as we know only four publications have been thoroughly devoted to the study of the absorbed dose produced by 106ru plaques using monte carlo simulations [ 9 , 12 , 17 , 26 , 29 ] , and all of them are based on the same simplified homogeneous geometry of the eye described above . the surprisingly small number of published works that rely on monte carlo methods is likely related to the difficulty of the problefor most monte carlo codes , the simulation of the plaques considered here requires adaptation of the code to describe the continuous energy spectrum associated with the beta decay of 106ru . 
in this context , the purpose of this work was to present , for the first time , an accurate dose distribution from some plaques in a realistic anatomical model of the eye using monte carlo simulations . methods simulation codes simulations were run using the generalpurpose monte carlo radiation transport code penelope [ 2 , 28 , 32 ]  . 
the dashed lines correspond to the parts of the lateral profiles that are located in the back of the eye plaque ( shielded by the metal of the applicator )  . 
penelope requires a main steering program that defines the source of particles , the quantities of interest to be scored , and the transport parameters relevant for the physics of the simulated problem and its computation speed . 
however , peneasy is not prepared for simulating a spectrum resulting from the beta decay of the 106ru nucleus , which disintegrates , with a half - life of 368 days , into 106rh producing a beta spectrum with a maximum energy of 39 kev . 
106rh , in turn , decays with a half - life of 29.8 s into stable 106pd producing a beta spectrum with a maximum energy of 3 , 540 mev . 
for each primary particle sampled , an end - point energy was chosen at random according to the probabilities given by the yields and then initial electron energies were sampled at random from the corresponding beta - decay spectruthe beta - decay spectra were generated with an adapted version of the code effy [ 18 ] incorporated into the modified peneasy code . eye plaque geometries the eye plaques considered were models cca and ccb from the manufacturer bebig gmbh ( berlin , germany ) [ 3 ]  . 
 the thicknesses of these layers from the strahlentherapieundonkologie12013 | abstract zusammenfassung strahlenther onkol 2013 189 : 6873 springer - verlag berlin heidelberg 2012 doi 10.1007 / s00066 - 012 - 0245 - 6 l.bruallaj.sempauf.j.zaragozaa.wittigw.sauerwein accurate estimation of dose distributions inside an eye irradiated with 106ru plaques abstract background . 
the monte carlo code penelope , conveniently adapted to simulate the beta decay of 106ru over 106rh into 106pd , was used to simulate radiation transport based on a computerized tomography scan of a patients eye . 
 for example , it was observed that a 4 - mm anterior displacement with respect to a posterior placement of a cca plaque for treating a posterior tumor would reduce from 40 to 0% the volume of the optic disc receiving more than 80 gy . 
 this represents an important step toward an optimized brachytherapy treatment of ocular tumors . keywords monte carlo penelope beta decay brachytherapy uveal melanoma przise bestimmung der dosisverteilung im auge bei der bestrahlung mit 106ru - applikatoren zusammenfassung hintergrund . 
der monte - carlo - code penelope ist zur berechnung des betazerfalls von 106ru ber 106rh zu 106pd geeignet und wurde verwendet , um den strahlungstransport in einem phantom zu berechnen , das auf der computertomographie eines auges basiert . 
so fhrt zum beispiel bei der bestrahlung eines tumors in der nhe des quators eine geringe anteriore verlagerung des cca - applikators um 4 mm dazu , dass 0% der papille eine dosis ber 80 gy erhlt , whrend bei der posterioren position 40% der papille mit ber 80 gy belastet wird . 
the emitter substance does not cover the whole shell ; it only extents up to 0.07 cm from the shell riwith the exception of the outer diameter , all other dimensions are equal for the cca and ccb plaques . 
the distribution of the emitter substance was assumed to be homogeneous throughout the middle shell described above . relative dosimetry both plaques were simulated inside a water phantoabsorbed doses obtained from the simulations were compared with experimental results from other authors [ 21 , 35 ]  . 
 experimental data , which are given in arbitrary units , were scaled to match simulation results at 0.2 cm of depth , that is , 0.2 cm away from the inner surface of the shell . 
all these structures are shown in .fig.1 with the exception of the lacrimal gland , whose volume does not intersect the depicted slice . monte carlo - estimated absorbed doses are expressed in terms of dose per primary particle . 
 in order to obtain dose - volume histograms of the considered anatomical structures in gy , it is necessary to know the activity of the plaque and to determine the irradiation time . 
irradiation time is determined by prescribing a dose of 700 gy to the voxel of the sclera located on the symmetry axis of the plaque and in contact with it . 
hence , the 700 gy prescription was used for the computation of all cumulative dose - volume histograms . results depth doses were tallied along the symmetry axes of the plaques , extending from the inner concave surface into the water phantothe upper panels of .fig.2 show the depth doses for the cca ( left ) and ccb ( right ) plaques compared with experimental data [ 21 , 35 ]  . 
each panel corresponds to each irradiation considered : cca anterior ( a ) , cca equatorial ( b ) , cca posterior ( c ) , ccb equatorial ( d ) main symmetry axis of the plaques , were computed at six depths . voxelized geometry a voxelized phantom was created based on a computerized tomography scan of an anonymized adult patient . 
in order to use the original voxelized phantom in the penelope simulations , the hounsfield units were converted to mass density values via the calibration curve of the computerized tomography scanner . 
for the material assignment three media were considered : water , air , and bone . to obtain an accurate dose distribution in the eye it is necessary to simulate the eye plaque , modeled with quadric surfaces , embedded in the computerized tomography scan , which is a voxelized structure . 
the combination of quadric and voxelized structures in the same simulation is made possible by peneasy , which allows the superposition of both types of geometries seamlessly . three locations on the eyeball were considered for the cca plaque , namely , anterior , equatorial , and posterior . 
cross sections of the plaques are shown in green with the emitter substance in red . segmentation of the computerized tomography scan the various treatment set - ups were assessed through isodose curves and cumulative dose - volume histograms . 
4 8 cumulative dose - volume histograms for the cornea ( a ) , lens ( b ) , optic disc ( c ) , and sclera ( d ) obtained from the monte carlo simulations . 
the lateral profiles tallied at a depth small enough to intersect the plaque are plotted until the point where they reach the plaque and they are then continued behind the plaque . 
the portion of lateral profiles falling behind the plaque , that is , facing its convex surface , are shown with dashed lines . .fig.3 shows the isodose lines for the four considered irradiations , namely , the cca plaque in anterior , equatorial , and posterior placement , and the ccb plaque in equatorial placement . 
therefore , it is expected that the cumulative dose - volume histograms obtained for the sclera for a given plaque are nearly independent of the plaques position . discussion published experimental data for cca and ccb plaques are scarce owing to the difficulties entailed in measuring small irradiated fields . 
however , this fact is not surprising since the experiment of taccini and coworkers is much older , they used radiochromic films , and the reported uncertainty bars of their experiment are considerably larger than the ones in the work of kaulich et al . 
 [ 20 , 21 ]  . our mixed quadric and voxelized geometry approach allowed the dose - volume histograms to be calculated for relevant anatomical structures of the eye , the orbit and structures at risk with unprecedented accuracy . 
reynaert n , marck sc van der , schaart dr et al obtained data , a posterior irradiation with the cca plaque results in a dose higher than 80 gy to 40% of the volume of the optic disc . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literatur kommentiert strahlenther onkol 2013 189 : 342343 doi 10.1007 / s00066 - 012 - 0287 - 9 online publiziert : 14 . 
februar 2013 springer - verlag berlin heidelberg 2013 d.rades klinik fr strahlentherapie , universittsklinikum schleswig - holstein , campus lbeck vorteilederstereotaktischen gegenberderkonventionellen bestrahlungvon wirbelkrpermetastasen originalbeitrag chawla s , schell mc , milano mt ( 2011 ) stereo tactic body radiation for the spine : a review . 
oligometastasierte erkrankung , befall von maximal 2 konsekutiven oder nichtbenachbarten wirbelsulensegmenten , rezidiv nach operation oder bestrahlung , wenig strahlensensibler primrtumor , tumorrest nach operation , operation nicht indiziert oder gewnscht , tumor > 5 mm vom rckenmark entfernt ( optimal ) , lebenserwartung > 6 monate , karnofsky - index > 4050 . 
als kontraindikationen werden genannt : herzschrittmacher , sklerodermie , radionuklidoder chemotherapie in den letzten 30 tagen , strahlentherapie in den letzten 3 monaten , signifikante oder progrediente neurologische defizite , > 25% spinalkanalbeteiligung , instabilitt der wirbelsule , metastatisch bedingte rckenmarkskompression ( mbrk ) , cauda - equina - syndro es wurden diverse fraktionierungsschemata verwendet : bei der srs berwiegend 1 - mal 1624 gy , bei der sbrt berwiegend 5 - mal 67 gy , 3 - mal 89 gy und 2 - mal 12 gy . 
randomisierte studien wren hilfreich , um herauszufinden , ob die sbrt / srs der konventionellen strahlentherapie berlegen ist . kommentar die hochprzisionsbestrahlung von schmerzhaften wirbelkrpermetastasen liegt im trend und gewinnt deshalb zunehmend an bedeutung . 
insofern ist es nicht verwunderlich , dass weltweit , auch innerhalb einzelner studien , zahlreiche verschiedene fraktionierungsschemata verwendet werden , was wiederum die aussagekraft dieser studien hinsichtlich der effektivitt von sbrt und srs erschwert . in der vorliegenden arbeit beschreiben chawla et al . , dass sich durch eine sbrt / srs in bis zu 100% der flle eine lokale kontrolle erreichen lsst [ 2 ]  . 
es gibt nmlich auch arbeiten , in denen die ansprechraten nur zwischen 43% und 67% liegen [ 1 , 16 , 17 ] , also mit denen nach konventioneller strahlentherapie vergleichbar sind [ 3 ]  . von besonderer bedeutung ist die sbrt / srs bei schmerzhaften wirbelkrpermetastasen von wenig strahlensensiblen primrtumoren wie dem malignen 342 | strahlentherapieundonkologie42013 melanom und dem nierenzellkarzino in den studien von gerszten et al . 
in der studie von sahgal ( n = 25 ; [ 17 ] ) war die ansprechrate 88% und lag somit mit ber den ergebnissen ( 6380% ) der konventionellen rebestrahlung mit 1 - mal 48 gy [ 10 , 11 , 18 ]  . allerdings ist die sbrt / srs schmerzhafter wirbelkrpermetastasen nicht frei von risiken . 
und bei einem / - verhltnis von 2 , 5 gy betrgt die equivalente dosis bei fraktionen von 2 gy zwischen 66 gy ( 1 - mal 16 gy ) und 141 gy ( 1 - mal 24 gy ) , also oberhalb der toleranzdosis fr das knochengewebe [ 12 ]  . auch radiogene neurologische sptkomplikationen wurden beschrieben : in den arbeiten von garg et al . 
die rtog - 0631studie , eine phase - ii / iii - studie , vergleicht die srs mit 1 - mal 16 gy mit der konventionellen bestrahlung mit 1 - mal 8 gy hinsichtlich schmerzlinderung . 
dies entspricht den empfehlungen einer internationalen expertengruppe , die in ihrer evidenzbasierten leitlinie deutlich macht , dass die sbrt / srs nicht die primre therapie der mbrk sein sollte [ 14 ]  . 
amdur rj , bennett j , olivier k et al ( 2009 ) a prospective , phase ii study demonstrating the potential value and limitation of radiosurgery for spine metastases . 
garg ak , shiu as , yang j et al ( 2012 ) phase 1 / 2 trial of single - session stereotactic body radiotherapy for previously unirradiated spinal metastases . 
garg ak , wang xs , shiu as et al ( 2011 ) prospective evaluation of spinal reirradiation by using stereotactic body radiation therapy : the university of texas md anderson cancer center experience . 
van der linden ym , lok jj , steenland e et al ( 2004 ) single fraction radiotherapy is efficacious : a further analysis of the dutch bone metastasis study controlling for the influence of retreatment . 
int j radiat oncol biol phys 59 : 528537 strahlentherapieundonkologie42013 | original article strahlenther onkol 2013 189 : 308314 doi 10.1007 / s00066 - 012 - 0304 - z received : 26 august 2012 accepted : 20 december 2012 published online : 28 . 
nevertheless , in most studies the combination of sur gery and radiotherapy revealed better re sults for local tumor control [ 1 , 5 , 6 , 18 , 20 , 21 , 30 , 32 , 38 ]  . 
however , radiotherapy in the pelvis is also particularly associat ed with complications such as colon , rec tum , and bladder damage , exacerbated by previous chemotherapy or pelvic surgery . independent studies indicated that in tensitymodulated radiotherapy ( imrt ) of the pelvis significantly reduces the irra diated volume of bowel , rectum , and blad der , and therefore minimizes acute and late toxicity to organs at risk [ 2 , 15 , 24 , 25 , 29 , 31 , 34 , 37 ]  . 
however , imrt is not com monly used in pediatric radiation oncol ogy due to a dose bath effect , in which in creased volumes of normal tissue are ex posed to low dose radiation . 
this may in crease the incidence of secondary malig nancy in longterm survivors of pediat ric cancers compared to a threedimen sional conformal radiotherapy ( 3dcrt ) [ 16 , 28 ]  . 
imrt and 3dcrt were compared in patients with ewings sarcoma who re quired irradiation in the pelvic area . patients and methods from 20072011 , 8 patients suffering from pelvic ewing sarcoma were treated in the department of radiation oncolo gy at the university of mnster : 6 males and 2 females ( median age 17 years , range 921 years )  . 
in order to achieve a reproducible position , the patients were immobilized in a supine position using an individual ized vacuum molded bag or a knee and foot positioning device . 
ptv1 was defined for 4 patients as the entire bony pelvis , due to disseminated metastases in the pelvis at time of diagnosis . the following organs at risk ( oars ) were delineated : bladder , rectum , bow el , spinal cord , cauda equine from l3 and femoral heads . 
normal tissue was defined as the entire irradiated vol ume from diaphragm to mid thigh within the skin surface minus the ptv . separate plans for the 3dcrt and imrt techniques of radiotherapy were generated for all patients . 
both plans were calculated for use on a siemens linear ac celerator ( primus ) with a multileaf colli mator ( 58 leaves , 1 cm leaf width , and 6 and 15 mv photon beams )  . 
1 patient , tumor , planning target volumes ( ptvs ) , and radiotherapy details localizationofptvs imrttechnique 3d - crttechnique patient age ( years ) , gender 11 , female initiallyaffectedareaandsite ofinitialmetastasis pubis le . 
 + both femoral heads + pubis le . 4 , 953 1 , 078 2 , 021 16 , male pubis ri . metastasis : lung , other small metastases in pelvis ri . 
opposing fields up to 45 gy were cho sen in 3 patients ( patients 1 , 2 , and 4 ) with entire bony pelvis as main ptv ( ptv1 )  . 
for 3dcrt plans , we predominantly used 15 mv pho tons due to better homogeneity within the ptv unless the ptv was adjacent to the skin these cases mixed beam energy of 6 and 15 mv photons were used . statistical analysis in order to compare the two radiothera py techniques , the twotailed wilcoxcon test was used with a threshold for statis tical significance at p = 0.05. 
all analyses were performed using spss 18 for win dows ( spss inc . , chicago , il , usa )  . results comparison of the two techniques includ ing ptv coverage , conformity , and ho mogeneity indices in all patients are pre sented in .tab.2. 
however , the percentages of volumes receiving at least doses of 30 , 40 , 45 , and 50 gy ( v30 to v50 ) were lower for the rectum in imrt plans . 
 thus , dose escalation in the radiotherapy of pelvic ewings sarcoma can be more easily achieved using imrt . keywords imrt 3d - crt ewing sarcoma pelvis plevine ewing - sarkome . 
im vergleich zu den 3dcrt - plnen zeigten imrt - plne deutlich bessere ergebnisse im hinblick auf die dosiskonformitt ( p = 0 , 012 ) und die darmschonung im dosisbereich 30 gy ( p = 0 , 012 )  . 
1 9 planning computed tomography scan of patient 4 with ewing sarcoma of the pubis and disseminated small metastases in the pelvis , as reference in which entire bony pelvis was defined as ptv1 ( 45 gy ) with opposing field arrangements ( a and b ) and boost of primary tumor site up to 54 gy with 4 - field beam arrangements ( c ) fig . 
3 9 two sections of treatment planning scans of patient 6 ( a ) and patient 7 ( b ) with 4 - field beam arrangements as the preferential 3d - crt plans discussion patients with ewing sarcoma of the pelvis have generally poor outcomes due to the difficulty in achieving adequate local con trol . 
according to the ewing 2008 protocol , radiotherapy must be per formed postoperatively even when clear margins and good histological response to chemotherapy exists and especially with tumors > 200 cm3 . strahlentherapieundonkologie42013 | original article fig . 
4 9 axial and coronal sections of treatment planning scan of patient 8 , with a laterally located primary tumor of pelvis , after hemipelvectomy , who required radiation to the primary tumor site and the entire surgical area many studies have proven the advan tages of imrt and its potential to deliv er conformal radiation . 
however , the dose homogene ity was lower in imrt due to prioritizing ptv coverage and oar sparing . gastrointestinal and bladder toxici ty are the main therapeutic side effects of pelvic radiation , particularly in cases of prior abdominal surgery and / or the ad ministration of actinomycin d and an thracyclines [ 35 ]  . uncertainties and contradicting results exist regarding the dosevolume param eters which allow more accurate predic tions of gastrointestinal side effects [ 13 ]  . 
 some authors reported that a lowdose ir radiated volume ( v20 and v25 ) correlated to bowel toxicity , whereas others found a close association between a highdose irradiated volume of the small intestine ( v40 and v50 ) and digestive toxicity [ 14 , 26 , 29 , 34 ]  . 
therefore , we analyzed both high and low doses delivered to the bowel . the presented analysis shows that the use of imrt resulted in better bowel spar ing , not only at high doses ( v40 , v50 ) , but also at low doses ( v10 , v20 ) compared with 3dcrt . 
 [ 12 ] reported that using imrt to treat pelvic tumors reduced the frequency and severity of gastrointesti nal symptoms and the need for diarrhea medication ( grade ll toxicity ) compared to the use of 3dcrt . 
this resulted in substantial sparing of surrounding critical structures . as expected , we had significantly high er volumes of normal tissue receiving low doses ( 2 gy ) of radiation ( p = 0.05 ) in imrt plans compared to 3dcrt . 
 [ 16 ] estimated that in patients surviving 10 years or more , imrt is likely to double the incidence of second ary malignancies compared to conven tional radiotherapy from about 1 to 1.75%. 
 in addition , because imrt involves more fields , a larger volume of normal tissue is exposed to lower radiation doses [ 16 , 36 ]  . despite marked improvement in the survival of ewing sarcoma patients through advances in multidisciplinary management of this disease , the 5year survival rates for patients with localized and metastatic disease at presentation are now approximately 70% and 30% , respec tively . 
therefore , all 8 patients in our col lective were treated with imrt . presently , proton therapy is a topic of high interest , especially in pediatric radio therapythis owing to its potential to de crease irradiation of normal tissue struc tures . 
on behalf of all authors , the corresponding author states that are no conflicts of interest . original article strahlenther onkol 2013 189 : 293300 doi 10.1007 / s00066 - 012 - 0297 - 7 received : 13 july 2012 accepted : 6 december 2012 published online : 28 . 
 [ 2 ] confirmed these results in a meta - analysis including 10 randomi zed comparisons of neoadjuvant rct versus surgery alone ( n = 1 , 209 )  . 
although prospective trials and meta - analy ses do not show any survival benefit of the trimodality therapy ( neoadjuvant rct followed by surgery ) compared to rct alone [ 4 , 5 ] , a better local control after trimodality therapy justifies its administration in medically and technically ( potentially ) operable patients . 
nevertheless , local infield recurrence remains the main reason of treatment failure after all treatment modalities [ 6 , 7 , 8 ]  . another challenging , not uncommon situation for the radiation oncologist is that surgical resection is not possible or the patient rejects surgical intervention after restaging and / or re - evaluation at 46 weeks after rct . 
considering that the tumor cells have been treated with an insufficient radiation dose , they might repopulate during the break for re - evaluation and impede long - term disease control or cure . 
if doses could be delivered in a curative range , cancellation of surgical resection would be less fatal and the mandatory curative surgical resection would theoretically be an optional procedure for patients with complete response . however , employing higher radiation doses to treat esophageal cancer is handicapped through the limited tolerance dose of organs at risk ( oar ) , such as the heart , spinal cord , the lungs , and of course the esophagus itself . 
of note , most of these studies used conventional treatment plans , large treatment volumes with high radiation doses ( up to 75 gy ) and in several cases additional intraluminal brachytherapy boost [ 10 , 11 ]  . 
rt planning , rt techniques , dose calculations , and radiation delivery have undergone immense improvement in the last two decades [ 12 , 13 , 14 , 15 , 16 ]  . 
the aim of this planning study was to investigate whether advanced rt planning enables higher doses to be delivered to the target volume without an increase in the delivered dose to the oar in the neoadjuvant treatment of laec . methods patients a total of 15 consecutive laec patients with ct2 - 4 , cn + were selected for the present study . 
patients characteristics are shown in .tab.1. the gross tumor volume ( gtv ) was delineated using all available resources , including pet / ct data , endoscopic reports , and diagnostic ct images . 
the planning target volume ( ptv1 ) was the ctv plus a margin of 2 cm in the author contributions : fakhrian had full access to all of the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis . strahlentherapieundonkologie42013 | original article tab . 
1 tumor characteristics of the 15 patients 78 cm3 ( 15213 cm3 ) characteristics primary sites , n cervical upper / mid thoracic lower thoracic overlapping lesion length of lesion , n 15 cm > 5 cm > 10 cm volume of gtv , mean ( range ) volume of ptv1 , mean ( range ) volume of ptv2 , mean ( range ) gtv gross tumor volume = the clinical target volume ( ctv ) with extended coverage 3 cm superiorly , 1 cm laterally , and 3 cm inferiorly , ptv1 planning tumor volume 1 = ctv plus a margin of 2 cm in the craniocaudal direction and 1 cm laterally , ptv2 planning tumor volume 2 = ctv plus a margin of 01 cm in all directions . 735 cm3 ( 261 1381 cm3 ) 341 cm3 ( 80 774 cm3 ) tab . 
dose , gy ptv1 median dose , gy ptv2 median dose , gy sd standard deviation . 3d - 45 ( sd ) 134 7121 5019 209 104 1712 2828 109 122 7918 4712 165 1610 1211 123 7518 449 185 1913 2825 1010 415 374 461 451 501 533 451 541 561 3d - 54 ( sd ) 154 7419 5518 2512 124 2014 4031 1917 476 532 551 133 7317 4710 195 104 2014 3126 1514 442 523 551 craniocaudal direction and 1 cm laterally , and the boost volume ( ptv2 ) was the ctv plus a margin of 01 cm in all directions depending on the location of the tumor and surrounding normal tissue . 
for the heart , only the left ventricle was contoured as the oar . treatment planning for all 15 patients , a 3d conformal rt plan with 45 gy at 1.8 gy / fraction was developed , which we generally employ in the neoadjuvant treatment of laec . 
additionally , a 3d boost ( as in the primary rct of ec ) was calculated with 9 gy at 1.8 gy / fraction to ptv2 , which we routinely use in our department for the definitive treatment of laec . 
planning objectives for the 3d plans were a mean dose to the ptv1 of 45 and 9 gy to the ptv2 ( dmean ) [ 13 ]  . a reference point representative for the ptv1 and ptv2 was used for normalization of the 3d - conformal plans , according to icru 50 / 62 . 
for plan comparison , the ht - sib plans were imported into the varian eclipse syste using dosevolume histograms ( dvhs ) , the mean doses to the ptv1 , ptv2 , and gtv were determined . 
mean values and standard devia294 | strahlentherapieundonkologie42013 abstract zusammenfassung strahlenther onkol 2013 189 : 293300 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0297 - 7 k.fakhrianm.oechsners.kampfert.schusterm.mollsh.geinitz advanced techniques in neoadjuvant radiotherapy allow dose escalation without increased dose to the organs at risk . 
for all 15 patients , we created a 3d conformal rt plan ( 3d - 45 ) with 45 gy in fractions of 1.8 gy to the planning target volume ( ptv1 ) , which we usually use to employ in the neoadjuvant treatment of laec . 
additionally , a 3d boost ( as in the primary rt of laec ) was calculated with 9 gy in fractions of 1.8 gy to the boost volume ( ptv2 ) ( dmean ) to a total dose of 54 gy ( 3d - 54 gy ) , which we routinely use for the definitive treatment of laec . 
three plans with a simultaneous integrated boost ( sib ) were then calculated for each patient : sliding window intensity - modulated radiotherapy ( imrt - sib ) , volumetric modulated arc therapy ( vmat - sib ) , and helical tomotherapy ( htsib )  . 
clinical investigations are warranted to study the clinical safety and feasibility of applying higher doses through advanced techniques in the neoadjuvant treatment of laec . keywords planning techniques simultaneous integrated boost radiotherapy , intensity - modulated volumetric modulated arc therapy helical tomotherapy neue techniken in der neoadjuvanten strahlentherapie erlauben dosiseskalation im zielvolumen ohne hhere dosis in den risikoorganen . 
 zustzlich wurde ein 3 - d - plan fr das boostvolumen ( ptv2 ) berechnet mit einer dosis von 9 gy ( dmean ) bei einer einzeldosis von 1 , 8 gy . 
anschlieend wurden fr jeden patienten drei plne mit integriertem boost ( sib ) fr ptv1 und ptv2 berechnet , unter verwendung folgender drei techniken : sliding window intensity modulated radiotherapy ( imrt - sib ) , volumetrisch modu lierte bogentherapie ( volumetric modulated arc therapy , vmat - sib ) und helikale tomotherapy ( ht - sib )  . 
mittelst modernster bestrahlungstechniken ist es mglich , in der neoadjuvanten strahlentherapie des laec eine hhere dosis im zielvolumen zu applizieren , ohne die dosis in den risikoorganen signifikant zu erhhen . 
es sind jedoch weitere untersuchungen erforderlich , um die klinische sicherheit und die anwendung einer hheren dosis fr die neoadjuvante behandlung des laec mittels modernster bestrahlungstechniken eingehender zu erforschen . schlsselwrter planungstechniken simultan integrierter boost intensittsmodulierte strahlentherapie volumetrisch modulierte bogentherapie helikale tomotherapie tions ( sds ) were reported for descriptive purpose . 
except for 2 patients with a maximum dose to the spinal cord of 54 and 52 gy in the 3d - 54 gy group , the maximum dose to the spinal cord was < 50 gy in all plans . 
on the other hand , there are studies that report an acceptable rate of toxicity in the combined treatment modality with higher rt doses ( up to 60 gy ) and salvage esophagectomy [ 19 , 20 ] ; thus , a total dose of 52.5 gy delivered with sophisticated techniques , which spares the oar , should be feasible in daily practice . 
 some authors report a higher peri - operative morbidity [ 21 , 22 ] , which has been linked to radiation exposure of lung volumes during neoadjuvant rct [ 23 , 24 , 25 ]  . 
 [ 22 ] , 16 patients with adenocarcinoma of the gastroesophageal junction received neoadjuvant rct with 40 gy and 2 cycles of 5 - fu and cisplatthe authors report 71% peri - operative complications with 2 treatment - related deaths and a 30 - day mortality rate of 25% , which exceeds most of the reported peri - operative complications after neoadjuvant rct [ 26 , 27 , 28 , 29 ]  . 
these unfavorable results should be interpreted very cautiously , as the study had only 16 patients with no control arfurthermore , the radiation treatment was applied with a mediastinal field , including the complete esophagus , the proximal stomach , and the medial edges of the pleural cavities ( diaphragm ) , which might have resulted in a large target volume . the correlation between the irradiated lung volume and the incidence of acute respiratory distress syndrome and postoperative mortality has been discussed controversially in the literature . 
there are a few studies , which suggest that the volume of lung receiving low radiation doses ( v5 , v10 ) may increase the postoperative pulmonary complications in esophageal carcinoma [ 23 , 24 ]  . 
in a retrospective study of 163 patients with laec , we previously demonstrated no improvement in outcome beyond a radiation dose of 54 gy in definitive rct for laec [ 13 ]  . 
in the current study , we demonstrated that despite a nominal reduction of 1.5 gy in the total radiation dose to the ptv2 ( 52.5 gy instead of 54 gy ) , the median doses in ptv1 and ptv2 in sib plans were simi lar to the 3d - 54 plan . 
the treatment duration is 1 week shorter ( 5 weeks instead of 6 weeks for definitive rct ) using the sib plans , which is not only pleasant for the patient , but also might have a radiobiological advantage and a positive impact on outcome [ 14 , 15 ]  . 
the sib plans resulted in a similar or even better sparing of the v30 and v40 of the heart compared to 3d - 45 or 3d - 54 and also a lower v50 of the heart compared to 3d - 54 . 
however , the improved v20 and v30 of the lung and the better sparing of v30 and v40 of the heart as well as the lower maximum dose to the spinal cord in the ht - sib plan were at the expense of an increased low dose volume to the normal lung parenchyma ( lung v5 )  . 
 considering the v5 of the lung , imrt - sib and vmat - sib were superior to ht - rt in our study , whereas ht - rt was superior considering v20 of the lung , maximal dose to the spinal cord and v30 , v40 , v50 and mean heart dose . there are some reports which indicate that salvage esophagectomy is a more morbid operation than planned esophagectomy after neoadjuvant rct . 
it should be noted , however , that the salvage resection in most of this studies was applied after patients had received doses beyond original article received different induction chemotherapy regimens prior to neoadjuvant rct . 
between the two groups , there were no significant differences between the incidence and severity of acute lung injury and acute respiratory distress syndrome ( rct + surgery : 43% , 43% ; surgery alone : 46% , 38% , respectively )  . 
importantly , the irradiated lung volume in esophageal carcinoma is dependent on several factors , such as the primary location of the tumor , length of the tumor , involved lymph node region ( s ) , which all affect the size of the target volume . 298 | strahlentherapieundonkologie42013 the role of comorbidities , presence of risk factors , surgical technique , and extent of the esophagectomy and lymphadenectomy on the incidence of the post - operative morbidity or mortality and pulmonary complications should not be underestimated [ 29 , 31 , 32 ]  . 
they observed a decrease in the 30 - day death rate , in the hospital death rate , a corresponding decrease in the incidence of postoperative respiratory failure and bronchopneumonia in their patients . 
factors that correlated with low morbidity and mortality during this period of time were no history of smoking and pulmonary disease , less blood loss during the surgery , small number of patients with advanced stage of disease ( stages iii or iv ) and an increase in the use of postoperative epidural analgesia and bronchoscopic clearance of secretions . obviously , the larger the tumor and extent of involvement is , the larger the irradiated lung volume ( especially v5 and v10 ) will be and the larger the extent of the initial tumor involvement is , the larger the extent of the surgical intervention will be ; thus , whether comorbidities or risk factors such as copd , smoking , induction chemotherapy , an unavoidable larger irradiated lung volume by laec , an unavoidable larger surgical resection , or a combination of them all are responsible for postoperative pulmonary complications after neoadjuvant rct cannot easily be answered with dvh models . 
this is in line with our results , which suggest that dose escalation is possible with new techniques without delivering higher radiation dose to organs at risk . recently , welsh et al . 
 [ 7 ] showed in a planning study that the use of simultaneous integrated boost with imrt allows a selective increase in the dose to the gtv ( up to 64.8 gy ) , while reducing the dose to the heart , lung , and liver . 
our data indicate that an increase in radiation dose to the gtv and ctv , which are part of the ptv2 , is possible , without an increased delivered dose to the oar . 
it might be difficult to deliver such a high dose to the gtv in the thoracic region without violating the recommended dose constrains to the lung , especially in neoadjuvant treatment . the employment of advanced techniques is not limited to dose escalation . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . literaturkommentiert strahlenther onkol 2013 189 : 344346 doi 10.1007 / s00066 - 013 - 0307 - 4 online publiziert : 17 . 
februar 2013 springer - verlag berlin heidelberg 2013 g.reinartzh.t.eich klinik und poliklinik fr strahlentherapie radioonkologie , universittsklinikum mnster verbessertdieinvolved - fieldbestrahlungbeikindern mithodgkin - lymphomin komplettremissionnach chemotherapiedasberleben ? originalbeitrag wolden sl , chen l , kelly km et al ( 2012 ) long - term results of ccg 5942 : a randomized comparison of chemotherapy with and without radiotherapy for children with hodgkins lymphoma a report from the childrens oncology group . 
die us - amerikanische childrens cancer group ( ccg ) hat 1995 fr kinder mit hodgkinlymphom die randomisierte studie ccg 5942 gestartet , die den effekt einer niedrigdosierten involved - field - radiotherapie ( ifrt ) auf das ereignisfreie berleben ( efs ) bei patienten mit komplettremission ( cr ) nach chemotherapie untersucht . 
die mehrheit der rezidive trat innerhalb von 4 jahren nach der randomisierung auf , und zwar bei den nichtbestrahlten patienten zu 90% am ort der primrlokalisation ; eine ifrt htte sicher einige dieser rezidive verhindert . die fast zeitgleich in deutschland initiierte multizentrische studie gpoh - hd 95 ( rekrutierung von august 1995 bis juli 2001 ) umfasste in ihren therapiegruppen ( tg ) eine risikoadaptierte chemotherapie und verzichtete bei patienten in cr auf eine weitere therapie [ 2 ]  . 
das gesamtberleben war bei verzicht auf die bestrahlung nicht signifikant verkrzt . im vergleich mit der deutschen gpoh - hd - 95 - studie sind die ergebnisse der us - amerikanischen ccg - 5942studie fr die jeweiligen therapiegruppen gegenstzlich . 
das ereignisfreie 10 - jahresberleben war in der studie ccg 5942 nach einsatz der ifrt in frhen stadien ( i , iia = tg1 mit 4 - mal copp / abv ) signifikant erhht ( p = 0 , 001 )  . 
die ungnstigeren mittleren und fortgeschrittenen stadien ( i , iib , iii = tg2 mit 6 - mal copp / abv und stadium iv = tg3 mit 2 - mal zyklus a / b / c ) zeigten nach hinzunahme der ifrt einen trend zu einem verbesserten ereignisfreien berleben ohne statistische signifikanz . die unterschiedlichen ergebnisse der amerikanischen und deutschen studien resultieren mglicherweise aus den kleinen fallzahlen in subgruppenanalysen oder der auswahl der chemotherapie . 
hierbei kann auch von bedeutung sein , dass die definition einer komplettremission in beiden studien unterschiedlich war : die deutsche studie gpoh - hd 95 forderte dafr eine reduktion des tumorvolumens um mindestens 95% ; demgegenber war in der us - amerikanischen studie ccg 5942 eine tumorvolumenreduktion um mindestens 70% gefordert . ein frhes ansprechen auf die chemotherapie ist auch beim hodgkin - lymphom ein wichtiger prognosefaktor . 
die bewertung des frhen therapieansprechens anhand der anatomischen ( tumorvolumen im ct ) oder funktionalen ( stoffwechselintensitt im fdg - pet ) bildgebung nach ein oder zwei zyklen chemotherapie kann dazu beitragen , die patienten zu identifizieren , die nach einer alleinigen chemotherapie ein nur geringeres rezidivrisiko aufweisen und auch ohne strahlentherapie ausreichend behandelt sind . 
die aktuellen ergebnisse einer anderen us - amerikanischen studiengruppe [ 3 ] besttigen fr junge patienten mit hodgkin - lymphom und gnstiger prognose die bedeutung des frhen ansprechens auf die chemotherapie . 
bei patienten , die nach 2 zyklen vamp eine komplettremission aufwiesen , erfolgte nach abschluss der chemotherapie mit insgesamt 4 zyklen keine bestrahlung mehr , bei den anderen patienten wurde eine ifrt mit 25 , 5 gy appliziert . 
wolden sl , chen l , kelly km et al ( 2012 ) longterm results of ccg 5942 : a randomized comparison of chemotherapy with and without radiotherapy for children with hodgkins lymphoma a report from the childrens oncology group . 
drffel w , lders h , rhl u et al ( 2003 ) preliminary results of the multicenter trial gpoh - hd 95 for the treatment of hodgkins disease in children and adolescents : analysis and outlook . 
metzger ml , weinstein hj , hudson mm et al ( 2012 ) association between radiotherapy vs no radiotherapy based on early response to vamp chemotherapy and survival among children with favorablerisk hodgkin lymphoma . 
 zu jedem onkologischen thema und zu jeder tumorenditt , wie auch jeder indikation bei gutartigen erkrankungen , finden sich in tabellarischer form immens viele informationen , die die autorinnen sehr gut recherchiert und zusammengestellt haben . 
der fachkollege wiederum findet in dem buch eine sehr gute grundlage , seine eigenen indikationsansichten abzuklren und kann , nach meiner meinung , einen groteil der angegebenen informationen direkt in sein eigenes hauskonzept einbringen . ich empfehle das werk wrmstens fr alle strahlentherapeuten und insbesondere auch fr die zuweiser anderer fachrichtungen . 
gademann ( magdeburg ) 346 | strahlentherapieundonkologie42013 original article strahlenther onkol 2013 189 : 329334 doi 10.1007 / s00066 - 012 - 0256 - 3 received : 6 july 2012 accepted : 17 october 2012 published online : 28 . 
februar 2013 springer - verlag berlin heidelberg 2013 o.j.ottc.jeremiasu.s.gaiplb.freym.schmidtr.fietkau department of radiation oncology , university hospital erlangen radiotherapyfor calcaneodynia resultsofasinglecenterprospective randomizeddoseoptimizationtrial calcaneodynia commonly causes inferior heel pain and occurs in up to 10% of the population [ 4 ]  . 
experts believe that the pain is mainly caused by acute or chronic injury to the origin of the plantar fascia from cumulative overload stress [ 1 , 4 ]  . 
most interventions used to manage calcaneodynia have not been studied adequately ; however , shoe inserts , stretching exercises , steroid injection , and custom - made night splints may be beneficial . 
modulations of a plethora of immunological processes by low and intermediate doses of x - ray have been identified with preclinical in vitro and in vivo model systems during recent years [ 26 ]  . 
the present prospective and randomized trial was initiated to determine the optimal single dose in terms of efficacy and radiation protection , as previously conducted for benign painful elbow syndrome [ 23 ]  . patients and methods between february 2006 and april 2010 , a total of 499 consecutive patients with calcaneodynia were treated at erlangen university hospital . 
for statistical comparisons between groups the mannwhitney u test and pearsons 2 test were used . the gender distribution of the 457 evaluated patients was 26% ( 119 / 457 ) male and 74% ( 338 / 457 ) female . 
pain level was determined using a graphical visual analogue scale ( vas ) with levels from 0 ( no pain ) to 100 ( maximum conceivable pain ) and a modified von pannewitz pain score [ 38 ] adapted from seegenschmiedt and keilholz [ 33 ]  . 
with this score the treatment response was evaluated with regard to pain symptoms grouped into five categories ( pain at strain , pain at night , persistent pain during daytime , pain at rest , and morning stiffness ) and four grades ( none : 0 points , mild : 1 point , moderate : 2 points , severe : 3 points )  . 
the mean overall response rate ( cr + pr ) of all published patients was 85% ( range 61100% ) and is in agreement with the results of our trial with early and delayed response rates of 87 and 88% , respectively . 
it is an important finding of our trial that the response rate ( especially cr ) significantly improved ( .fig.3 ) from the end of the treatment ( early response ) to the followup examination 6 weeks after completion of radiotherapy ( delayed response )  . 
3 results after radiotherapy for calcaneodynia author [ reference ] richarz [ 24 ] von pannewitz [ 39 ] cocchi [ 3 ] mitrov and harbov [ 16 ] zschache [ 41 ] mantell [ 13 ] basche et al . 
 [ 11 ] reported on a comparable trial on 130 patients with painful heal spurs that were randomized to receive either single doses of 0.5 gy to a total dose of 3.0 gy / 3 weeks ( low - dose group ; n = 65 ) or single doses of 1.0 gy to a total dose of 6.0 gy / 3 weeks ( high - dose group ; n = 65 )  . 
 in 18% ( 24 / 130 ) of cases of the high - dose group and 13% ( 17 / 130 ) of cases of the lowdose group , a second radiotherapy series was given . 
in 341 patients ( 68% ) , radiotherapy was performed twice a week with a single 610 mv photon field , in 161 patients ( 32% ) three times a week with a single 175 - kv x - ray field . 
 [ 34 ] compared the clinical effect of three different dose concepts in the radiotherapeutic treatment of painful heel spurs : group a ( n = 72 ) received 12 gy total radiation dose in 3 fractions / week and 2 series ( 61 gy / series ) separated by 6 weeks ; group b ( n = 98 ) received 3 gy total radiation dose in 10 fractions of 0.3 gy ( n = 50 ) or 10 fractions of 5 gy ( n = 48 ) with conventional fractionation in 1 series . 
radiotherapy was very effective : at last follow - up 67% ( group a ) and 71% ( group b ) remained completely free of pathe cr rate was not different between the 3 radiation concepts . 
current work aims to identify how the immune status in the peripheral blood of patients treated with 0.5 gy in comparison to 1.0 gy is modulated by low dose radiation therapy . 
therefore , we currently prefer to use single doses of 0.5 gy according to the results of our trial which did not reveal any disadvantage for the patients treated with the lower dose protocol at any time of evaluation . 
 [ 11 ] our trial still supports the hypothesis that radiotherapy with lower single doses of 0.5 gy might be equally effective to single doses of 1.0 by substantially decreasing the potential radiation risk . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . mitteilungen der fachgesellschaften strahlenther onkol 2013 189 : 347348 doi 10.1007s00066 - 013 - 0340 - 3 springer - verlag berlin heidelberg 2013 redaktion : rolf sauer , erlangen adressen deutsche gesellschaft fr radioonkologie e.v. , degro - geschftsstelle , hindenburgdamm 30 , d - 12200 berlin , telefon ( + 49 / 30 ) 8441 - 9188 , fax - 9189 prsident : j . 
sedlmayer , universittsklinik fr radiotherapie und radio - onkologie salzburger landeskliniken und paracelsus medizinische privatuniversitt , mllner hauptstrae 48 , a - 5020 salzburg , telefon ( + 43 / 662 ) 4482 - 3904 , fax - 887 scientific association of swiss radiation oncology , pd damien c . 
kneschaurek , klinik fr strahlentherapie der technischen universitt , klinikum rechts der isar , ismaninger strae 22 , d - 81675 mnchen , telefon ( + 49 / 89 ) 4140 - 4504 , fax - 4881 hellenic society of radiation oncology , p . 
 es handelt sich um den hermann - holthusen - preis , alfred - breit - preis , dissertationspreis , innovationspreis , preis zur hochprzisions - strahlentherapie , gnther - von - pannewitz - preis sowie den koester - preis . informationen : anmeldung : jubilare die fachgesellschaften von strahlentherapie und onkologie gratulieren zum geburtstag : 15.04.2013 gieen : harald von lieven 75 jahre strahlentherapie und onkologie 4 2013 | original article strahlenther onkol 2013 189 : 285292 doi 10.1007 / s00066 - 012 - 0290 - 1 received : 11 july 2012 accepted : 26 november 2012 published online : 20 . 
according to long - term results based on 5 , 206 cases from the international registry of lung metastases , lung metastatectomy was a safe and potentially curative procedure [ 38 ]  . 
 in addition , advanced radiotherapy technologies such as intensity - modulated radiotherapy ( imrt ) with a simultaneous integrated boost ( imrt - sib ) and adaptive re - planning twice during the treatment course ( art ) also result in better tumor control [ 7 ]  . 
 the aim of this retrospective study was to evaluate the feasibility , safety , and effectiveness of sbrt for pulmonary metastases . patients and methods between april 2007 and march 2011 , 87 metastatic lung cancer patients who underwent sbrt were included in this study . 
as to the location of the 189 lesions , they were divided into 88 lesions in upper lobes , 12 lesions in middle lobes , and 89 lesions in lower lobes . based on the 5 - year relative survival rates for cancer patients diagnosed in 20002002 from cancer registries in japan [ 2 ] , these patients were divided into three prognostic groups with some modification due to our clinical experience . 
according to the prognostic risk group due to sites of the primary disease , 17 patients were in group 1 ( breast , testis , ovary , and thyroid ) , 25 patients in group 2 ( head / neck , kidney , bone / soft tissue , bladder , and uterus ) , and 45 patients in group 3 ( intestine , liver , esophagus , and malignant melanoma )  . 
the accuracy needed for image - guided sbrt is achieved by ensuring reliable and reproducible patient immobilization , which is important for image - guided radiotherapy ( igrt ) to fix the patient body as a rigid object , and defining and limiting tumor and organ motion during treatment . 
 however , this method with such a single point detector has several limitations to obtain the accurate respiratory motion . the air - bag system was developed as a novel abdominal compression and respiratory monitoring device which monitors the patients body volume change as an external respiration signal collaborated with the real - time position management system ( rpm , varian medical system , palo alto , ca , usa )  . 
these air flow data are processed by a personal computer and translated into swinging decoy markers displayed on the computer screen so that an infrared camera of the rpm system can capture the marker instead of an infrared reflective marker . 
using this air - bag system , the applicability of the rpm system is not limited owing to enough amplitude and more accurate determination of the magnitude of respiratory motion . amplifying the respiratory waveform , we can easily select the phase of expiratory motion . 
using the respiratory waveform displayed on real - time by the air - bag system ( .fig.1b ) , we divided these ct images into 3 to 4 phases between inspiratory and expiratory phases . 
 therefore , we delineated the internal target volume ( itv ) , and then defined ptv by adding an 8 - mm margin of set - up error to the itv . 
between april 2007 and march 2011 , 87 patients underwent sbrt for pulmonary metastases using the in - house air - bag systemtm to obtain the four - dimensional image for treatment planning and to reduce intrafractional intrathoracic organ motion with abdominal compression to reduce the risk of radiation pneumonitis . 
the 2and 3 - year os rates were 57 and 49% for patients in group 1 , respectively , while the corresponding os rates were 48 and 21% , and 40 and 32% for patients in groups 2 and 3 , respectively . 
concerning adverse respiratory events after sbrt for pulmonary metastases , 14% were grade 0 ( g0 ) , 66% g1 , 13% g2 , 6% g3 , and 1% g4 . 
concerning the adverse respiratory events ( ncictc ) by grade scale , 1and 2 - year cumulative probabilities of radiation pneumonitis were 12 and 20% for g2 and 4 and 10% for g3 / 4 , respectively . 
we propose that the number of pulmonary metastases that can be safely treated with sbrt is 6 ptvs with a cumulative v20 of 30% under the restricted respiratory tumor motion using the air - bag systemtm . 
 sbrt for pulmonary metastases offers locally effective treatment for recurrent or residual lesions after first line chemotherapy . keywords stereotactic body radiotherapy pulmonary metastases air - bag system adverse respiratory event stereotaktische krperstrahlentherapie von lungenmetastasen . 
zwischen april 2007 und mrz 2011 durchliefen 87 patienten die sbrt fr lungenmetastasen unter verwendung eines hauseigenen air - bag - systemstm , um 4 - d - ct - bilder zur erleichterung der behandlungsplanung zu erhalten und die intrafraktionre intrathorakale organbewegung durch abdominelle kompression zu verringern , um so das risiko einer strahlenpneumonitis zu reduzieren . 
die 2und 3 - jahres - os betrugen fr patienten in gruppe 1 jeweils 57 und 49% , fr patienten in den gruppen 2 und 3 jeweils 48 und 21% sowie 40 und 32% . 
bezglich der unerwnschten respiratorischen ereignisse ( nci - ctc ) nach gradskala betrugen die kumulativen 1und 2 - jahreswahrscheinlichkeiten fr eine strahlenpneumonie jeweils 12 und20% fr g2 und 4 und 10% fr g3 / 4 . 
die anzahl an geheilten lungenmetastasen , die mit sbrt behandelt werden konnten , lag bei 6 ptvs mit einem kumulativen v20 von 30% mit eingeschrnkter respiratorischer tumorbewegung durch das air - bag - systedie sbrt fr lungenmetastasen bietet eine effektive behandlungsmglichkeit fr wiederkehrende oder verbleibende lsionen nach der first - linechemotherapie . schlsselwrter stereotaktische krperstrahlentherapie lungenmetastasen air - bag system respiratorisch ungnstiges ereignis ceived higher dose . 
the median number of planning target volumes ( ptv ) was 2 ( range 115 ) , while that of the gross tumor volume ( gtv ) was 2 ( range 120 )  . 
 of 87 patients , 29 ( 33% ) also had radiotherapy to thoracic region , e.g. , mediastinal lymph node , thoracic spine , rib , breast , and chest wall . 
the remaining patients did not undergo chemotherapy due to the contraindication from serious renal disease treated with renal dialysis or personal refusal . strahlentherapieundonkologie42013 | original article overallsurvival causespecificsurvival monthsaftersbrt fig . 
group 3 includes 45 patients with intestine ( 35 ) , liver ( 7 ) , esophagus ( 2 ) , and malignant melanoma ( 1 ) probabilities of survivals , local control ( lc ) and probability of adverse events were calculated by the kaplanmeier method . 
the origin of the disease for these 10 patients were as follows : 3 intestines , 2 breasts , 1 each of thyroid , intrahepatic bile duct , kidney , uterine body , and cervix . 
the mean cumulative v20 were 11.68.5% ( range 140% ) , 29.818.6% ( range 656% ) and 25.712.8% ( range 840% ) in g0 / 1 , g2 , and g3 / 4 , respectively . 
therefore , the number of lung cancer metastases that could be safely treated with sbrt was 6 ptvs or 7 gtvs within cumulative v20 of 30% under the restricted intrafractional respiratory tumor motion using the air - bag system in a variety of treatment modalities for pulmonary metastases with minimally invasive procedures have recently become available , e.g. , video - assisted thoracoscopic surgery ( vats ) , molecular targeting therapy , radiofrequency ablation ( rfa ) therapy , image - guided interstitial brachytherapy , and sbrt [ 4 , 5 , 8 , 10 , 11 , 16 , 17 , 32 ]  . in japan , medical service fees officially cover patients treated with sbrt for primary and metastatic lung cancers in only a limited number of cases with pulmonary tumor sizes of 5 cm , number of the tumors of three or less , and without any organ metastases . 
in this study , hilar lesions were not included , because of the higher risk of radiation - induced bronchial obstruction , hemoptysis and grade 3 or more toxicities treated after hypofractionated sbrt [ 28 , 41 ]  . the present analysis showed that os was 47% , css was 52% , lc rate was 80% , and intrathoracic progression - free survival was 40% at 2 years . 
based on a multiinstitutional phase i / ii trial of sbrt for metastatic lung tumor , 2 - year actuarial lc was 96% at a median follow - up of 15.4 months , and the corresponding os was 39% [ 33 ]  . 
since more than 70% of the patients had multiple pulmonary metastases in the metastatic group , the ratio of ptv number per patient in this group was larger than that in the primary group . 
the number of lung cancer metastases that could be safely treated with sbrt was six ptvs or seven gtvs within cumulative v20 of 30% under the restricted intrafractional respiratory tumor motion using the air - bag system in two to three treatment sessions with gap of more than 3 months poorer condition , e.g. , multiple primary cancers , cardiovascular diseases , and serious co - morbidities . 
most of the patients in the primary group had low pulmonary function , e.g. , chronic obstructive pulmonary disease due to long smoking histories . respiratory motion is an issue that is becoming increasingly important in the era of image - guided radiotherapy ( igrt )  . 
 the respiratory tumor motion is generally 2 cm , and larger in the craniocaudal direction with a maximum movement of 34 cm , when the pulmonary tumor is located just above the diaphragm [ 13 , 18 , 36 ]  . 
 there are several approaches to compete with tumor motion , including respiratory inhibition with abdominal compression [ 1 ] , breath - holding [ 20 , 31 , 40 ] , and respiratory gating [ 15 , 22 , 27 ]  . 
the 4d radiotherapy era has been opened by introduction of the robotic technology [ 25 , 37 ] as well as real - time tumor - tracking radiotherapy ( rt - rt ) [ 34 , 35 ]  . 
an innovative igrt system , which has the capability of dynamic tumor tracking using a novel gimbaled x - ray head and a dual real - time x - ray monitoring system has been developed [ 12 ]  . using the respiratory waveform displayed on real - time by in - house air - bag system , we can divide 4d ct images into 290 | strahlentherapieundonkologie42013 3 to 4 phases between inspiratory and expiratory phases . 
abdominal compression with the air bag reduces the movement of diaphragm , which can decrease the intrathoracic organ motion and resulted in the reduction of the itv . we can estimate the cumulative v20 ( eqd2 ) using shioristm in routine practice . 
in this analysis , however , we simply added the each v20 for the multiple sessions of the sbrt . prediction of radiation pneumonitis as an adverse respiratory event is possible in the 3d treatment for lung cancer using dvh parameters . 
in the non - small cell lung cancer patients treated with radiation alone , serious radiation pneumonitis was developed beyond a v20 of 32% , and much more increased at the level of 40% or more . 
since most patients with pulmonary metastases had residual or recurrent diseases after prior chemotherapy as a first line treatment for pulmonary metastases , it appeared appropriate to consider a v20 of 30% as the dose restriction in the sbrt for metastatic lung cancer . concerning the sbrt for metastatic lung cancer , the adverse respiratory events of g3 ranged from 35% in the literature [ 9 , 26 , 33 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 321328 doi 10.1007 / s00066 - 012 - 0303 - 0 received : 8 september 2012 accepted : 20 december 2012 published online : 28 . 
februar 2013 springer - verlag berlin heidelberg 2013 t.langsenlehner1c.dller1p.winkler1g.gall2k.s.kapp1 1 department of therapeutic radiology and oncology , medical university of graz 2 department of urology , medical university of graz impactofinter - andintrafraction deviationsandresidualset - up errorsonptvmargins differentalignmenttechniquesin3d conformalprostatecancerradiotherapy randomized controlled clinical trials demonstrated a significant improvement in biochemical relapse - free survival with dose escalation in prostate cancer radiotherapy [ 13 , 24 , 33 ]  . 
however , the improved biochemical control rate was associated with an increased risk of late complications , mainly late gastrointestinal toxicity [ 2 ]  . the development of intensity - modulated radiotherapy has enabled the delivery of highly conformal dose distributions , facilitating selective dose escalation while limiting radiation dose to critical organs , resulting in improved local tumor control without increase in normal tissue injury [ 8 , 23 , 25 , 32 ]  . 
nevertheless , accurate target localization remains a crucial factor for optimal target coverage and limiting radiation dose to adjacent organs at risk . a common method to improve the accuracy of daily prostate localization is to implant fiducial markers , which can be visualized on kv or mv images and serve as a reliable surrogate for soft tissue target volume positioning [ 7 , 29 ]  . 
to correct for intrafraction motion continuous online tracking with in - treatment kv - fluoroscopy or implanted electromagnetic transponders would be required [ 14 , 16 , 18 , 22 , 30 ]  . 
however , these techniques are not widely available ; therefore , correction of intrafraction motion is currently rarely performed . the present study was performed to quantify interfraction prostate deviations after skin mark or bony anatomy based patient alignment and to analyze residual set - up errors ( rse ) after implanted marker - based alignment . 
furthermore , intrafraction prostate motion was analyzed and ptv margins for three different alignment techniques were evaluated . methods and materials patients and treatment characteristics a total of 44 patients with nodal negative adenocarcinomas of the prostate treated between may 2009 and september 2010 were analyzed . 
in all patients , four commercially available gold markers ( 3.0x1.2 mm ) had been implanted into the prostate transrectally under ultrasound guidance . to allow for resorption of possible prostate swelling and to ensure a stable position of the markers , planning ct scans were performed at least 2 weeks after placement . 
ct and mri images were then transferred to a 3d dosimetric planning platform ( pinnacle v8.2 ) and fused by matching the fiducial markers . the clinical target volume ( ctv ) included the entire prostate and the base of the seminal vesicles ( sv )  . 
 the rectum was contoured from the sigmoid flexure to the anal verge , the bladder as single solid organ . high energy photons ( 18 mv ) were delivered in a three - field technique using an anterior and two lateral fields to encompass the ptv . 
the total dose prescribed to the icru reference point was 7074 gy delivered in 2 gy / fraction ( 5 fractions / week )  . the study was approved by the institutional ethics review board , and informed consent was obtained from all patients . daily set - up and image guidance all patients were treated on a linac , equipped with an on - board imager ( obi ) kv x - ray system and an amorphous silicon flat panel detector ( portalvision as1000ias3 )  . 
before treatment , two orthogonal strahlentherapieundonkologie42013 | original article kv images ( 0 and 270 ) were obtained and fused with pre - computed digitally reconstructed radiographs ( drrs ) derived from the planning ct that provided the reference location for the implanted markers and the outlined bony structures . online image registration was performed by the radiographers on the obi console with a 3d marker - match software . 
to evaluate intrafraction prostate motion , one mv image of each treatment field ( 0 , 90 and 270 ) was taken during treatment . the additional dose applied to the patients for kv imaging was very low ranging from 2050 mgy for all treatment sessions . 
translational deviations in the ap , si , and lr direction as well as rotational errors around the lr and ap axes were determined . furthermore , pelvic bony anatomy was contoured and an offline image registration based on pelvic anatomy was performed . 
the relative motion between the prostate gland and bony anatomy was calculated by quantifying the best visual match of the positions of intraprostatic fiducials with the position of the bony anatomy . residual set - up error and intrafraction deviation after on - line repositioning , the prostate was expected to be in the planned position . 
the residual set - up error of the pros322 | strahlentherapieundonkologie42013 tate after on - line image registration was defined as the difference between the position achieved after on - line registration and the position obtained by offline image registration of the setup - image pair assessing translational and rotational deviations . 
this error reflected the influence of observer incertainties and rotational errors . to quantify intrafraction motion , the marker positions derived from the mv images were compared with the corresponding drrs . 
intrafraction deviation of the prostate was defined as the difference between the marker positions detected in the during treatment mv images compared with the rse value derived after correction of the residual set - up error by off - line kv image registration as described above . the mean residual marker displacement and the standard deviation over all treatment fractions were calculated assessing both translational and rotational deviations . 
a similar analysis was performed for the intrafraction marker displacement by dividing the treatment period into different time intervals and calculating the distance of the markers to the planned position for each beam position . margin determination and statistical analysis the average of the systematic errors of the whole population was defined as the mean systematic displacement ( )  . 
individual variations are defined as the standard deviation of all displacements relative to the mean position over all fractions and overall random error as the standard deviation of all individual variations . 
for daily online correction based on implanted markers , total errors were calculated as square root of the quadratic sum of the errors for the residual set - up error and the intrafraction motion . the pearson r2 value was calculated to determine the strength of correlations between bladder and rectal volume at the time of the planning ct with set - up errors . results a total of 7 , 273 images ( kv , n = 2 , 936 , mv , n = 4 , 337 ) from 1 , 469 fractions were available for evaluation . 
the mean of prostate interfraction deviations ( ) for skin mark alignment relative to implanted marker alignment was 2.96.1 mm in ap , 0.25.3 mm in si , and 0.36 mm in lr direction , respectively . 
the mean residual rotational error around the lr axis ( 0.94.9 ) was significantly larger than around the ap axis ( 0.21.4 ) and its positive mean value indicates that the prostate base was more likely to rotate toward the posterior direction . 
 abstract zusammenfassung strahlenther onkol 2013 189 : 321328 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0303 - 0 t.langsenlehnerc.dllerp.winklerg.gallk.s.kapp impact of interand intrafraction deviations and residual set - up errors on ptv margins . 
the use of an optimized workflow with faster treatment techniques such as volumetric modulated arc techniques ( vmat ) could allow for a further decrease . keywords prostate neoplasms image - guided radiotherapy planning target volume margins radiotherapy setup errors fiducial markers einfluss interund intrafraktioneller bewegungen und residualer setup - fehler auf ptv - sicherheitssume . 
in einer offline - analyse von 7273 aufnahmen wurden interund intrafraktionelle prostatabewegung , der residuale set - up - fehler nach markerbasierter patientenpositionierung sowie der effekt der behandlungszeit auf die intrafraktionelle prostatabewegung untersucht . 
die zur bercksichtigung der intraund intrafraktionellen prostatabewegung und des residualen set - up - fehlers erforderlichen sicherheitssume bei patientenpositionierung anhand von hautmarkierungen betrugen 14 , 1 mm , 12 , 9 mm sowie 15 , 1 mm und bei positionierung anhand von knochenstrukturen 9 , 6 mm , 8 , 7 mm und 2 , 6 mm in anterior - posteriorer ( ap ) , superiorer - inferiorer ( si ) und rechts - links - ( lr - ) richtung . 
die verwen dung eines optimierten workflows mit schnelleren bestrahlungstechniken wie vmat ( volumetric modulated arc techniques ) knnte zu einer weiteren reduktion der ptv - sicherheitssumen beitragen . schlsselwrter prostataneoplasien image - guided radiotherapy ( igrt ) ptv - sicherheitssume strahlentherapeutische set - up - fehler implantierte marker the observed intrafraction motion was 0.41.8 mm ( ap ) , 0.41.6 mm ( si ) , and 0.10.9 mm ( lr ) , respectively . 
overall mean , systematic and random errors for different alignment techniques are shown in .tab.1. strahlentherapieundonkologie42013 | 100% total original article sagittal plane coronal plane posterior anterior ( mm ) left right ( mm ) fig . 
1 8 scatter plots of overall positioning errors including residual set - up error and intrafraction deviation after implanted marker - based alignment for the a sagittal plane and b coronal plane . 
dots appear superimposed due to the 1 mm graticule the frequency of total intrafraction errors as a function of treatment time after online correction for all patients and fractions is provided in .fig.2 , and the mean translational intrafraction deviations are shown in .fig.3. 
overall mean , systematic and random errors at certain time intervals after completion of the setup procedure are given in .tab.2. for margin calculation , only translational deviations were considered . 
 [ 27 ] , sds of the interobserver delineation error for the target volume should be no less than 1.7 mm in lr , 2 mm in si , and 2 mm in ap direction when ct and mr fusion techniques are used for delineation . 
2 8 frequency of total intrafractional errors as a function of treatment time ( i.e. , time from completion of the implanted marker - based set - up to acquisition of the in - treatment mv image ) time from setup ( min ) 324 | strahlentherapieundonkologie42013 fig . 
with pre - fraction implanted marker - based alignment , margins original article 326 | strahlentherapieundonkologie42013 might further be reduced by additional 5 and 5.9 mm in the ap and si direction . 
 consequently , the effects from delineation uncertainty became more significant with decreasing set - up errors as demonstrated in .tab.3. we are aware that the magnitudes of geometrical uncertainties are different for each radiation therapy facility ; therefore , general recommendations for ptv margins in clinical practice can not be given . the effects from interfraction prostate deviation on treatment precision are minimized by daily pre - treatment online image guidance using implanted markers [ 15 ] and it could be shown that residual translational deviations after online marker - based repositioning were low with a mean not significantly different from zero . 
due to the almost spherical shape of the prostate , the gain in rotation correction has been suggested to be insignificant if the ctv included the prostate only , whereas benefits for rotation corrections have been reported with sv included in the ctv [ 6 , 17 , 21 , 28 ]  . similar to previous studies , interfraction rotational deviations around the lr axis significantly correlated with the rectum volume in the planning ct scan [ 11 ]  . 
 rectal filling at the time of ct simulation also has a significant impact on biochemical and local failure , as well as on rectal toxicity [ 5 , 10 ]  . 
we are aware that the analysis of intrafraction prostate motion with mv images at specific time points during treatment is not as robust as having a continuous tracking device [ 14 , 16 , 18 , 30 ]  . 
however , as the patients were imaged daily and at different positions of the prostate motion cycle , we assume that the recorded data provide an adequate estimation of the intrafraction prostate movement . our data compare well with those reported by li et al . 
 [ 16 ] who showed systematic displacements ( ) of 0.3 mm in the lr direction , 0.8 mm in the si direction , and 0.8 mm in the ap direction . 
with an optimized workflow , the time interval between acquisition of the kv images and the start of irradiation could be shortened ; furthermore , highly reduced delivery times that can be achieved with vmat will have a strong impact on the probability of prostate displacements and lead to a further decrease in ptv margins . the values calculated in the present study represent the minimal margins required for prostate irradiation . 
an additional amount is still necessary to compensate for other uncertainties such as uncertainty in the delineation of ctv , reliability of repositioning systems and target volume deformation , especially , when the sv are included in the ctv [ 17 , 21 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 315320 doi 10.1007 / s00066 - 012 - 0271 - 4 received : 31 july 2012 accepted : 8 november 2012 published online : 28 . 
recent advanced intensity - modulated radiotherapy improved homogeneity of breast targets and resulted in better outcomes than conventional methods with regard to skin reaction and breast appearance [ 7 , 13 ]  . 
in addition , accelerated partial breast irradiation [ 4 , 23 ] and the concomitant boost to the tumor bed [ 11 , 20 ] have raised concerns about the reduction of the treatment interval . 
these methods use multisegments in one field or give a higher dose to limited targets ; therefore , accurate setup is warranted . while frequent and qualified images acquisition in the linac room can help reduce set - up uncertainty , it increases not only machinery and manual work load but also undesirable radiation exposure to patients [ 1 ]  . 
if risk groups for extensive set - up errors are identified , can efficient and personalized guidelines for image - guided radiotherapy ( igrt ) for the breast be made ? previous studies with small samples have not resolved these questions [ 2 , 9 , 10 , 12 , 19 , 21 , 22 , 24 ]  . 
 to establish the customized strategy of igrt for whole breast irradiation , our study measured the set - up errors and assessed risk factors associated with extensive errors in our large population with radiotherapy based on tangential beam directions . methods and materials simulation and planning our institution utilized the brilliance big bore oncology ct system ( philips medical systems , the netherlands ) for virtual simulation and the breastboard ( civco , orange city , iowa , usa ) for immobilization . 
the lower or middle of the clavicle heads was selected as the cranial border according to the supraclavicular lymph node involved and 2 cm below the breast fold were used as the caudal border . 
the ct scans were sliced at a thickness of 3 mthe image set was transferred to the radiation therapy planning system , a varian eclipse version 8.6.1.5 ( varian medical system , palo alto , ca , usa )  . 
on every fraction , proper position was verified through coincidence between skin tattoos and room laser along the axial , coronal , and sagittal intersections , and a tangential set - up followed . 
on the basis of the chest wall ( ribs and lung contour ) , the optimized shifts along the rightleft ( rl ) , superiorinferior ( si ) , and anteriorposterior ( ap ) axes and the rotation of collimator angle ( rcoll ) of each medial and lateral portal were measured through an off - line review . 
a total of 12 experimental set - ups showed that the correlation coefficient between couch movement and the measured error by epi was > 0.9 along all axes and rcoll . patients from september 2009 to april 2012 , 184 breasts of 182 patients received whole breast irradiation after breast - conserving surgery . 
the 5 patients with an elapsed interval from the start to the finish of radiotherapy of over 50 days in case of 28 fractions or 45 days in case of 25 fractions were excluded from our study . 
a total of 914 portals of 176 breasts from the medial direction ( me316 | strahlentherapieundonkologie42013 dian 5 fractions / patient ) and 807 portals of 174 breasts from lateral direction ( median 5 fractions / breast ) were analyzed . 
patients characteristics are summarized in .tab.1. set - up errors and risk factors systematic errors ( ) were defined as the mean deviation of the geometry between the fractionated treatment and a simulation isocenter . 
 also , patients with extensive errors on the initial treatment were defined as risk factors . to evaluate whether the correction of the center according to the center of initial treatment can improve the set - up uncertainty , the shifts between an isocenter of the initial treatment and each treatment were calculated and compared with the shifts between an isocenter of the simulation and each treatment . 
because the data of shifts between an isocenter of the simulation and initial treatment was excluded , patient sets that acquired only three epis were also excluded in these analyses . 
these groups account for 14.6% of the medial directions and 13.9% of the lateral direction . risk factor for the medial portal , tumor location on uoq ( p = 0.012 ) and chest wall thickness 2.0 cm ( p = 0.003 ) were associated with extensive errors . 
the systematic ( ) and random error ( ) of population , and the planning target volume ( ptv ) margin ( 2 + 0.7 ) were calculated for each direction . 
in 2 tests , tumor in upper outer quadrant ( p = 0.012 ) and chest wall thickness 2.0 cm ( p = 0.003 ) for medial portals and age group ( p = 0.036 ) for lateral portals were associated with extensive errors . 
in terms of the set - up uncertainty during breast irradiation , patients with extensive error in the initial treatment should be closely observed with serial image - guided radiotherapy . keywords breast cancer set - up error risk factor electronic portal image image - guided radiotherapy set - up - unsicherheit whrend der brustbestrahlung . 
fr jede richtung wurde der systematische ( ) und der zufllige fehler ( ) der bevlkerungsgruppe sowie die grenze ( 2 + 0 , 7 ) des geplanten zielvolumens ( ptv ) berechnet . 
die medialen und lateralen ptvgrenzen fr die rechten - linken , superioreninferioren und anterioren - posterioren achsen und die rotation des kollimators waren je weils 2 , 6 und 2 , 4 mm , 4 , 6 und 4 , 6 mm , 3 , 1 und 3 , 3 mm sowie 2 , 8 und 2 , 9 . 
in den 2 - tests waren fr mediale portale ein tumor am oberen ueren quadranten ( p = 0 , 012 ) und die brustwanddicke 2 , 0 cm ( p = 0 , 003 ) sowie fr laterale portale die altersgruppe ( p = 0 , 036 ) mit den weitreichenden fehlern verbunden . 
im hinblick auf die setup - unsicherheit bei der brustbestrahlung sollten patienten mit weitreichenden fehlern whrend der anfnglichen behandlung durch serielle bildgesteuerte radiotherapie genauer beobachtet werden . schlsselwrter brustkrebs set - up - fehler risikofaktor elektronisches portalbild bildgesteuerte radiotherapie strahlentherapieundonkologie42013 | tab . 
a similar tendency was observed in another of our institutions analyses for pelvic regional radiotherapy , which showed an association with the first five shifts and baseline and day - to - day shifts [ 27 ]  . 
therefore , initial set - up as a screening method can give much information about the set - up error followed fractions and careful attention to those should be continued . 
however , the isocenter correction according to the initial treatment in overall patients showed a negative effect , so it should not be an absolute navigator . chest wall thickness as a measure of the obesity of chest wall showed a marked increase of set - up uncertainty on both the medial and lateral portals . 
other body characteristics including body mass index , breast size , and various surgical factors ( e.g. , surgical extent and complications ) were not related to set - up uncertainty . 
 [ 12 ] , using helical tomotherapy reported no correlation between breast volume and daily shiin addition , time course did not affect the set - up variation . in the comparison to the epi and cbct , the epi underestimated the actual bony anatomy in 20 breast cancer patients by 2050% [ 18 ]  . 
this method tested in patients with an average set - up error > 5 mm showed an average overestimation of the boost volume by 628% and underestimation of the whole breast by 1739% along the three dimensional axes . 
between kv / mv orthogonal images and cbct , the residual errors were 3 , 4 , and 4 mm along the rl , si , and ap axes and the mean differences of ctv and ptv of v95 were 1 and 4% , respectively [ 8 ]  . cbct that detect the variation of the soft tissue can assess seroma volume changes [ 26 ] and the planning organ at risk volume margin of the heart [ 17 ]  . 
in the study using the simulator and lead markers on center and 4 borders of clinical target volume , the means of the maximal movements along the three dimensional axes were within 2 mm during normal breathing [ 5 ]  . 
in the measurement of central lung distance of the portal images , the maximum movement was 10 mm [ 14 ]  . although our policy is to have patients undergo weekly igrt , this was occasionally violated because of the retrospective nature , workload , and equipment breakdown ( epi ) , etc . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . original article strahlenther onkol 2013 189 : 301307 doi 10.1007 / s00066 - 012 - 0298 - 6 received : 4 april 2012 accepted : 6 december 2012 published online : 20 . 
these patients can be treated with different modalities including transcatheter chemotherapy ( tace ) , radiofrequency ablation ( rfa ) , and percutaneous ethanol injection ( pei ) [ 2 , 3 , 4 , 5 ] , but outcome is unsatisfactory . 
among the reasons for these problems , there is the low tolerance to doses as moderate as 3050 gy ; the volume effect in the liver was investigated concluding that about 700 cm3 of the liver should be spared during irradiation and that the local control could have been increased escalating the total dose above 50 gy [ 6 , 7 , 8 , 9 ]  . 
today , imrt has evolved into a new form , the volumetric modulated arc therapy ( vmat ) pioneered in its rapidarc mode by otto [ 13 ] ; technical details can be found elsewhere [ 14 ]  . 
the role of rapidarc was assessed in a number of studies but its clinical application to the liver has been primarily limited to metastatic indications [ 15 , 16 ]  . 
 [ 17 ] demonstrated that rapidarc could also play a role in hcc . the present study reports the dosimetric and basic clinical results of a retrospective analysis for hcc patients treated with rapidarc . 
more detailed clinical data will be published in a separate analysis . materials and methods study population and treatment characteristics between february 2009 and december 2010 , 138 patients were treated for hcc with rapidarc at the home institute and were retrospectively analyzed to assess tumor response and overall survival . 
the planning target volume ( ptv ) was defined as the ctv plus 0.5 cm in the axial dimension for daily patient setup variation and 12.5 cm in the cranialcaudal dimension to account for liver motion owing to respiration . 
 in case of target volume reduction , three schemes were adopted : ( 1 ) 60 gy total dose in two courses : 40 + 20 gy , ( 2 ) 45 gy in two courses : 36 + 9 gy , and ( 3 ) 45 gy in three courses : 27 + 9 + 9 gy . for those patients with a tumor near the gastrointestinal tract , 45 gy in two or three courses were designed by the shrinkage of the tumor and prevention for gastrointestinal toxicity . 
when organs at risk ( oars ) included the stomach , duodenum , and colon , the 40 + 20 gy scheme was applied . for all patients , oars were outlined : the entire liver , the liver ptv , kidneys , stomach , spinal cord , and lungs . 
planning objectives aimed to achieve the following : for total liver v30 gy < 60% , and for healthy liver ( liver - ptv ) v30 gy < 30% ; for ptv minimum dose > 90% and a maximum dose < 115140% . all patients were treated in the supine position with arms placed overhead and immobilized with an individualized vacuum cushion on the patient tray . 
treatments were performed with 10 mv photons generated by a varian clinac equipped with a standard millennium multileaf collimator . evaluation of dosimetric and technical data for each patient , dosimetric parameters of delivery were scored . 
for initial ptv , target coverage ( minimum as d98% , d99% , maximum as d2% , d1% , and v90% , v95% , standard deviation [ sd ] ) and homogeneity parameters ( mean , median , d5% , d95% , v90% , v95% , v107% ) were recorded ; for final ptv minimum doses ( as d98% and d99% ) were also recorded . 
for oars , the mean dose , the maximum dose ( dx cm3 ) and appropriate values of vx gy ( volume receiving at least x gy ) were scored . 
 guidelines of international commission on radiation units and measurements ( icru ) 83 report were applied as much as possible [ 19 ]  . evaluation of clinical data clinical evaluations were planned during treatment , at 1 , 2 , 3 , and 6 months after treatment completion and more sparsely afterwards . 
visits included laboratory assessment , and ct and mr imaging ( at 2to 3 - month intervals for at least 2 years and at 6 - month intervals thereafter )  . 
basic treatment outcome was measured in terms of in - field local control and overall survival and it was scored continuously with a total follow - up of maximum 28 months . 
non - classical rild was defined as a 5 - time elevation in liver transaminases ( threshold of 175 iu / l for a normal range of 535 iu / l ) and was reported here . results population demographics and clinical stage the characteristics of the patients are reported in .tab.1. 
the patients median age was 66 years ( range 2787 years ) , 83% were treated with 60 gy ( 12% at 45 gy , 6% at 66 gy ) , 62% with cone - down , 98% with multiple arcs . 
kidneys received on average 5 and 8 gy ( left and right ) , while the maximum dose to the spinal cord was 22 gy ; mean doses to esophagus and stomach were 23 gy and 15 gy , respectively . 
clinical results were positive and might suggest , with appropriate care , to consider rapidarc as an additional therapeutic opportunity for these patients . keywords hepatocelluar carcinoma rapidarc vmat radiotherapy radiotherapie mit volumetrisch modulierter bogentherapie fr chirurgische oder ablativ nicht behandelbare hepatozellulre karzinompatienten zusammenfassung ziel . 
das mittlere alter der patienten lag bei 66 jahren ( spanne 2787 jahre ) , 83% wurden mit 60 gy ( 12% mit 45 gy und 6% mit 66 gy ) behandelt . 
die nieren erhielten im mittel 5 und 8 gy ( links und rechts ) , die maximale dosis im rckenmark betrug 22 gy sowie die mittlere dosis in der speiserhre und im magen 23 und 15 gy . 
die klinischen resultate waren positiv und knnen darauf hindeuten , rapidarc , mit der ntigen sorgfalt , als zustzliche therapeutische behandlungsmglichkeit fr diese patienten zu bercksichtigen . schlsselwrter hepotozellulres karzinom rapidarc vmat strahlentherapie the cone - down technique , while 98% were treated with multiple partial arcs and 93% were optimized with a non - coplanar setting . examples of dose distributions in the axial , coronal , and sagittal planes for 3 patients , representing three different ptv sizes , are illustrated in .fig.1 : well below median size ( 66 gy ) , median size ( 60 gy ) , well above median ( 45 gy )  . the results from the dvh analysis for target volumes are shown in .tab.3. 
 [ 17 ] in their planning study and the present study both using rapidarc but with different technical approaches ( number of arcs and coplanarity in particular ) is shown . 
comparison data from kuo using imrt technique are also reported . target coverage ( data are normalized to d95% ) resulted in an average d98% of ~98% for the ptv ( the target receiving the full prescription dose )  . 
1 9 examples of dose distributions in axial , sagittal , and coronal planes for three patients ( a small target , 66 gy , b medium target , 60 gy , c large target , 45 gy )  . 
color wash scale ranges from 5 gy120% of the prescription dose involvement of normal healthy liver as well as of total liver was kept on average within planning objectives ( v30 gy was < 25% for healthy liver ) , although not for all patients . 
crude in - field control was achieved as follows ( percentages are relative to the total cohort and to the assessable fraction [ 109 patients ] , respectively ) : complete response in 12 ( 9% , 11% ) patients , partial response in 58 ( 42% , 53% ) , stable disease in 32 ( 23% , 29% ) , progression in 7 ( 5% , 6% ) ; 29 patients ( 21% of the total ) were not assessable . 
concerning treatment toxicity , nonconventional rild was observed in 18 cases ( 13% )  . discussion this study reported on the treatment of a group of 138 patients for hcc with the rapidarc technique with conventional fractionation and total dose from 45 66 gy . 
clinical results in terms of survival and local control were summarized demonstrating a high level of local control ( 94% of the assessable patients ) and the overall survival at 12 months was 45% . 
the 5 - year survival after surgery ranges from 30 50% but it is severely limited by the extent of disease and cannot be offered to the majority of patients . 
rfa , tace , selective internal radiation therapy ( sirt ) or sorafenib approaches have a survival rate ranging from 4070% at 1 or 2 years [ 2 , 3 , 4 , 5 , 6 , 7 , 8 ] but are limited in applicability to early stages , location , co - morbidities , availability . 
most patients in the present study could not receive any surgery or tace due to their advanced stage and to typically being classified as nontreatable , difficult to treat , or terminal stage cases for their dismal prognosis . 
these results , together with the fact that for earlier stages the survival reported here ranges from 100% ( stage i ) to 83% ( stage ii ) suggest the fact that rapidarc could be applied in sbrt mode to early stage hcc patients and a dedicated protocol will be activated soon at the home institute . strahlentherapieundonkologie42013 | original article ptv_initial rapidarc rapidarc 100 120 140 100 120 140 dose [ % ] dose [ % ] healthy tissue liverptv spinal cord rapidarc rapidarc rapidarc dose [ gy ] left kidney dose [ gy ] right kidney dose [ gy ] stomach rapidarc rapidarc rapidarc dose [ gy ] dose [ gy ] dose [ gy ] fig . 
dashed lines represent the inter - patient variability at 1 standard deviation to further appraise the quality of the plans administered to the patients , the data of this study were compared against the published planning evaluation of rapidarc in hcc from kuo et al . 
results demonstrated that an improvement can be achieved with respect to imrt and coplanar rapidarc for organs at risk and that rapidarc can guarantee at least the same healthy tissue sparing as imrt , with some improvement on v30 gy . 
it is evident that the comparison shall be considered with care given the low number of patients in the planning study . limitations in the present study , no specific strategy was applied to compensate for liver motion due to respiration . 
although it is known that the potential displacement of liver could be as large as a few cm [ 25 ] , the advanced stage of patients suggested to simplify the delivery methods and to incorporate motion compensation into traditional definition of margins . 
fogliata a , clivio a , nicolini g et al ( 2008 ) intensity modulation with photons for benign intracranial tumours : a planning comparison of volumetric single arc , helical arc and fixed gantry techniques . 
scorsetti m , alongi f , castiglioni s et al ( 2011 ) feasibility and early clinical assessment of flattening filter free ( fff ) based stereotactic body radiotherapy ( sbrt ) treatments . 
scorsetti m , bignardi m , alongi f et al ( 2011 ) stereotactic body radiation therapy for abdominal targets using volumetric intensity modulated arc therapy with rapidarc : feasibility and clinical preliminary results . 
kuo yc , chiu ym , shih wp et al ( 2011 ) volumetric intensity - modulated arc ( rapidarc ) therapy for primary hepatocellular carcinoma : comparison with intensity - modulated radiotherapy and 3 - d conformal radiotherapy . 
bignardi m , cozzi l , fogliata a et al ( 2009 ) critical appraisal of volumetric modulated arc therapy in stereotactic body radiation therapy for metastases to abdominal lymph nodes . 
kwon jh , bae sh , kim jy et al ( 2010 ) long - term effect of stereotactic body radiation therapy for primary hepatocellular carcinoma ineligible for local ablation therapy or surgical resection . 
kubas a , mornex f , merle p et al ( 2008 ) irradiation of hepatocellular carcinoma : impact of breathing on motions and variations of volume of the tumor , liver and upper abdominal organs . 
gong gz , yin y , xing l , guo yj et al ( 2012 ) rapidarc combined with the active breathing coordinator provides an effective and accurate approach for the radiotherapy of hepatocellular carcinoma . 
februar 2013 springer - verlag berlin heidelberg 2013 g.g.grabenbauer radioonkologie und strahlentherapie am klinikum coburg konventionellfraktionierte postoperativeradiotherapie bis50 , 4gyfrprogrediente low - grade - gliomebeim erwachsenenweiterhin therapeutischerstandard originalbeitrag shaw eg , wang m , coons sw et al ( 2012 ) randomized trial of radiation therapy plus procarbazine , lomustine , and vincristine chemotherapy for supratentorial adult low - grade glioma : initial results of rtog 9802 . 
eingeschlossen wurden patienten mit einem lowgrade - astrozytom ( who - grad 2 ) , oligodendrogliom oder oligoastrozytom im alter von 1839 jahren nach biopsie oder subtotaler resektion sowie berhaupt operierte patienten ber 40 jahre ohne angaben zum operativen ausma . 
eine post - hoc - analyse unter ausschluss der patienten , die 2 jahre nicht berlebten , zeigte einen berlebensvorteil im kombinierten behandlungsar dies sei ein hinweis darauf , dass der positive effekt der chemotherapie verzgert in erscheinung trte . kommentar ber die letzten 15 jahre wurden zahlreiche studien publiziert , die das ziel der prognoseverbesserung beim low grade - gliom verfolgten . 
die eortcstudie 22845 konnte die frage nach dem wert der unmittelbar postoperativen rt im vergleich zur rt erst im progress dahingehend beantworten , dass lediglich das pfs , jedoch nicht das os durch die wahl des frhen rt - zeitpunkts verbessert wird [ 2 ]  . 
nachfolgende untersuchungen zur geeigneten gesamtdosis der rt zeigten , dass eine dosis - eskalation ber 50 , 4 gy hinaus keinerlei positiven effekt hatte , sondern eher zu einer zunahme der neurotoxizitt fhrte , insbesondere bei einer totaldosis von 64 , 8 gy [ 3 , 4 ]  . 
insofern ist die hier zu diskutierende studie die erste , die sich mit der frage des einflusses einer polychemotherapie zustzlich zur rt beim low - grade - gliom beschftigt . die toxizitt des untersuchten behandlungsschemas mit doch immerhin 6 zyklen pcv wird nach unserem dafrhalten mit 7 zeilen text bei fehlender tabellarischer darstellung der ergebnisse recht oberflchlich behandelt . 
shaw eg , wang m , coons sw et al ( 2012 ) randomized trial of radiation therapy plus procarbazine , lomustine , and vincristine chemotherapy for supratentorial adult low - grade glioma : initial results of rtog 9802 . 
van den bent mj , afra d , de witte o et al ( 2005 ) long - term efficacy of early versus delayed radiotherapy for low - grade astrocytoma and oligodendroglioma in adults : the eortc 22845 trial . 
karim ab , maat b , hatlevoll r et al ( 1996 ) a randomized trial on dose - response in radiation therapy of low - grade cerebral glioma : european organization for research and treatment of cancer ( eortc ) study 22844 . 
shaw e , arusell r , scheithauer b et al ( 2002 ) prospective randomized trial of lowversus highdose radiation therapy in adults with supratentorial low - grade glioma : initial report of a north central cancer treatment group / radiation therapy oncology group / eastern cooperative oncology group study . 
eyre hj , crowley jj , townsend jj et al ( 1993 ) a randomized trial of radiotherapy versus radiotherapy plus ccnu for incompletely resected lowgrade gliomas : a southwest oncology group study . 
unverstndlich , denn unter bercksichtigung der begrenzten lebenserwartung der patienten spielt die frage einer irreversiblen polyneuropathie im hinblick auf die lebensqualitt schon eine gewisse rolle . zur statistik und zum gesamtresultat : die primre hypothese der studie war die verbesserung des 5 - jahres - berlebens von 70% nach alleiniger rt auf 85% nach rt + pcv . 
59% nach 56 jahren strker ( p = 0 , 02 ) , wenngleich nach 6 jahren nur noch knapp 30% der patienten in der nachbeobachtung ( at risk ) sind . 
grabenbauer , coburg die in der rubrik literatur kommentiert seit 2010 erschienenen beitrge sind online verfgbar unter strahlentherapieundonkologie42013 | case study strahlenther onkol 2013 189 : 335338 doi 10.1007 / s00066 - 012 - 0274 - 1 received : 13 july 2012 accepted : 8 november 2012 published online : 28 . 
bloom syndrome is related to dna repair disorders such as fanconi anemia , ataxia telangiectasia , and xeroderma pigmentosupatients with a dna repair disorder may show extreme radiation sensitivity and have severe acute reactions to radiotherapy [ 2 ]  . squamous cell carcinoma of the lung responds well to radiotherapy of 50.4 gy to the tumor , but radiation - induced esophageal stricture may occur with administration of only 30.6 gy to the mediastinum [ 3 ]  . 
similarly , radiotherapy of 60 gy over 6 weeks concurrent with 5 - fluorouracil ( 5 - fu ) and cisplatin may cause severe acute reactions such as bone - marrow suppression , dermatitis , and mucositis [ 4 ]  . 
in contrast , we have shown that proton beam therapy is an excellent method for high - dose irradiation of a tumor with a reduced dose to noncancerous tissues [ 5 , 6 , 7 , 8 ]  . 
here , we describe the first use of proton beam therapy in a patient with bloom syndrome for treatment of oropharyngeal cancer . case report a 32 - year - old woman with bloom syndrome was diagnosed with oropharyngeal cancer staged as t2n2bm0 poorly differentiated squamous cell carcinoma . 
 c newly diagnosed left breast cancer 1 month after proton beam therapy strahlentherapieundonkologie42013 | case study abstract zusammenfassung strahlenther onkol 2013 189 : 335338 springer - verlag berlin heidelberg 2013 doi 10.1007 / s00066 - 012 - 0274 - 1 m.mizumotoh.hashiim.senaritas.sakait.wadat.okumurak.tsuboih.sakurai proton beam therapy for malignancy in bloom syndrome abstract backgroundandpurpose . 
the clinical target volume was defined as the area of the primary tumor and lymph node metastases plus an 8 - mm margafter treatment with 36 gye ( gray equivalent ) in 20 fractions ( 45 fractions per week ) , dietary intake was decreased by mucositis and intravenous hyperalimentation was started . 
we obtained almost complete response for a radiosensitive patient with a deficiency of dna repair , indicating the excellent dose concentration of proton beam therapy . keywords dna repair - deficiency disorders squamous cell carcinoma radiation oropharyngeal cancer severe acute reaction protonentherapie eines bsartigen tumors beim bloom - syndrom zusammenfassung hintergrundundziel . 
bei der patientin handelte es sich um eine 32 - jhrige frau mit bloom - syndrom , bei der ein als gering differenziertes t2n2bm0 - plattenepithelkarzinom klassifiziertes oropharynxkarzinom diagnostiziert wurde . 
nach der behandlung mit einer gesamtdosis von 36 gye ( gray equivalent ) in 20 einzeldosen ( 45 einzeldosen pro woche ) wurde die nahrungsaufnahme infolge von mukositis reduziert und es wurde mit intravenser hyperalimentation begonnen . 
die ver abreichung einer gesamtdosis von 59 , 4 gye in 33 einzeldosen verringerte die gre des primrtumors merklich , verursachte jedoch eine milde mukositis , die die einstellung der protonentherapie erforderlich machte . 
wir erzielten ein beinahe vollstndiges ansprechen bei einer strahlenempfindlichen patientin mit mangelhafter dns - reparatur , was auf die hervorragende dosiskonzentration der protonentherapie hindeutet . schlsselwrter dna - reparaturdefizit - erkrankung plattenepithelkarzinom bestrahlung oropharynxkarzinom schwere akute reaktion fig . 
there was no mucositis in the oral cavity and contralateral pharynx , irradiation of which was avoided by using proton beam therapy cositis ( grade 1 : erythema of the mucosa ) and pain control using opioids was started . 
mock u , georg d , bogner j et al ( 2004 ) treatment planning comparison of conventional , 3d conformal , and intensity - modulated photon ( imrt ) and proton therapy for paranasal sinus carcinoma . 
widesott l , pierelli a , fiorino c et al ( 2008 ) intensity - modulated proton therapy versus helical tomotherapy in nasopharynx cancer : planning comparison and ntcp evaluation . 
one month after proton beam therapy , the size of the primary tumor and the lymph node metastases were markedly reduced ( .fig.1b ) , but multiple lung metastases had occurred . 
at the time of death , the significant reduction in size of the irradiated tumor had been maintained without severe late toxicity . discussion dna repair disorders result in development of malignant tumors and hypersensitivity to radiotherapy [ 1 , 2 , 9 ] , with tumors commonly appearing at an early age and having a poor prognosis [ 2 ]  . 
despite this limited irradiated area , mucositis occurred soon after proton beam therapy was started and became so severe that a break in therapy was required . modern radiotherapy techniques can reduce the dose to normal tissue , but cannot avoid low - dose exposure of normal tissue [ 10 , 11 ]  . 
on behalf of all authors , the corresponding author states that there are no conflicts of interest . laudatio strahlenther onkol 2013 189 : 339339 doi 10.1007 / s00066 - 013 - 0319 - 0 online publiziert : 20 . 
nach der facharztanerkennung fr radioonkologie in ungarn bildete er sich 1975 / 76 in zrich in der mdr - brachytherapie und der ctgesttzten bestrahlungsplanung unter der leitung von professor horst weiter . 
seit 1994 gehrt er als associate professor zum medizinischen lehrkrper an der semmelweis - universitt in budapest . das spezifische interesse von rpd mayer galt immer der brachytherapie in ihren verschiedenen techniken und biologischen wirkungen . 
so hat er sowohl im bereich der ldr - , als auch der selten angewandten mdr - brachytherapie bedeutende wissenschaftliche arbeit geleistet und verbesserte damit besonders in den letzten jahren die anwendung der hdrbrachytherapie in ungarn wesentlich . professor mayer hat neben vielen auszeichnungen durch nationale und internationale gesellschaften eine flle von verantwortungsvollen aufgaben in der ungarischen radioonkologie und in anderen wissenschaftlichen gremien wahrgenommen . 
nicht nur , dass er 1995 das erste ungarische degro - mitglied war , sondern es verbinden ihn enge kollegiale , ja freundschaftliche beziehungen zu den groen deutschen kliniken in leipzig , dresden , essen , tbingen , mnchen und erlangen . 
er hat in seinem berufsleben stets sorge dafr getragen , dass die verbindungen zwischen ungarn und deutschland anfangs zu den beiden deutschen staaten , spter zu gesamtdeutschland immer enger wurden . 
1996 wurde er auch mitherausgeber unserer zeitschrift strahlentherapie und onkologie . diese wrdigung wre nicht vollstndig , wenn hier nicht das besondere interesse rpd mayers an der deutschen kultur erwhnt wrde , besonders seine liebe zur musik richard wagners . 
regelmig ist er deshalb bei den bayreuther festspielen anzutreffen und das wird auch im wagner - jahr 2013 der fall sein . wir danken rpd mayer auch im namen der degro fr seine immer whrenden bemhungen , zwischen der ungarischen und der deutschen radioonkologie brcken zu schlagen und hoffen auch in der zukunft auf viele gute begegnungen mit ihm , und zwar nicht nur auf dem grnen hgel , sondern als aktiver teilnehmer auf den degro - kongressen . thomas herrmann , dresden rolf sauer , erlangen korrespondenzadresse th . 
noch immer ist er an der uzsoki - klinik , dem groen stdtischen krankenhaus in budapest und der grten radioonkologischen klinik in ungarn berhaupt , ttig und gerade mit der konzeption einer grundstzlichen erneuerung der technischen ausstattung der strahlenklinik an diesem krankenhaus beschftigt . rpd mayer wurde in budapest in eine familie hineingeboren , die vielfltige beziehungen zur medizin hatte beide grovter waren rzte . 
eich1 received : 24 june 2019 / accepted : 16 january 2020 / published online : 3 february 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract purpose purpose of this study was to investigate outcome and toxicity of re - irradiation for recurrent primary glioblastoma ( rgbm )  . 
we evaluated a group of patients with rgbm and identical primary treatment comprising adjuvant radiotherapy ( 30 2 gy ) with concurrent temozolomide ( tmz )  . methods in this retrospective study of 46 patients , all received adjuvant or denitive normofractionated radiotherapy to a pretreated area , some with concurrent chemotherapy . 
for mgmt promoter - methylated histology , higher radiation doses improved survival . keywords rgbm radiotherapy brain tumor temozolomide bevacizumab introduction glioblastoma multiforme ( gbm ) accounts for 15.8% of all primary intracerebral tumors and despite many improvements in therapy , the 5 - year overall survival ( os ) is only 5% [ 1 ]  . state of the art is multimodal treatment consisting of surgical resection , radiotherapy using modern local radiation techniques , and chemotherapy . 
the combination of 60 gy radiation with simultaneously applied temozolomide ( tmz ) is regarded as standard therapy for patients up to 70 years of age and has shown benet for even older patients [ 46 ]  . despite these aggressive treatment protocols , tumor recurrence is very high and prognosis is poor , with a median os of 1215 months [ 7 ]  . in case of recurrence , repeated surgical resection is feasible , as long as the patients performance status is appropriate [ 8 ]  . 
because a combined therapy using radiation and tmz is widely accepted as rst - line treatment , the benet 458 strahlenther onkol ( 2020 ) 196 : 457464 of another cycle of tmz after tumor recurrence is a point of discussion [ 12 ]  . 
other prognostic factors mentioned in the literature include age , performance status , tumor size , extent of initial surgery , and surgery in the recurrent situation [ 14 ]  . 
to this end , we evaluated a group of patients with recurrent primary gbm and identical primary treatment ( adjuvant radiochemotherapy comprising 30 2 gy with concurrent tmz )  . methods 46 patients treated in our institution for recurrent primary glioblastoma ( rgbm ) between 2013 and 2016 were included in the study . 
they had all completed adjuvant radiation therapy composed of 60 gy in 2 gy daily fractions with concurrent tmz therapy and at least one subsequent adjuvant tmz cycle for primary disease . 
24 of 40 patients received re - surgery and 30 of 40 received simultaneous systemic therapy . the impact of age , gender , planning target volume ( ptv ) , time to the onset of the second radiation therapy , mgmt promoter and idh mutation status , eastern cooperative oncology group performance index ( ecog ) , extent of surgery , radiation dose , and type of chemotherapy were evaluated . 
all cases were discussed in an interdisciplinary tumor board and all patients gave informed consent . radiation planning was based on ct and mri scans , dening the gross tumor volume ( gtv ) as the contrast - enhancing lesion in the t1 - weighted mri sequence , the clinical target volume ( ctv ) as gtv plus a 0.51 cm margin , and ptv as ctv plus a 12 mm margtreatment planning was performed with respect to prior received doses to organs at risk . 
the characteristics of all patients who completed the planned radiation therapy can be found in table 1 . patients had follow - up visits 68 weeks after completion of radiotherapy and then every 35 months at our institution . 
follow - up mri scans were conducted at outpatient strahlenther onkol ( 2020 ) 196 : 457464 table 1 ( continued ) 10 ( 25% ) 13 ( 32.5% ) 17 ( 42.5% ) location ( n ) , if more than one lobe is affected , the lobe with the largest volume is indicated frontal temporal parietal systemic therapy ( n ) none temozolomide bevacizumab nitrosoureas other no information censored cases ( n ) progression free at end of analysis alive at end of analysis 9 ( 22.5% ) 6 ( 15% ) 5 ( 12.5% ) 14 ( 35% ) 5 ( 12.5% ) 1 ( 2.5% ) 1 ( 2.5% ) 13 ( 32.5% ) n number of patients , ecog eastern cooperative oncology group performance index clinics . 
late toxicities were dened as side effects occurring more than 90 days after the end of radiotherapy . progression - free survival ( pfs ) was dened as the time of rst radiation until radiological or histological proof of recurrence . 
pfs2 was dened as survival after the second radiation treatment to clinical or radiological proof of progression or patients death or was censored at the end of follow - up . overall survival ( os ) was dened as the time from the rst radiation treatment to death or the end of follow - up . overall survival 2 ( os2 ) was dened as the time of reirradiation after objective gbm recurrence to death or was censored at the end of follow - up . statistical analysis was performed using ibm spss25 statistics ( spss inc . , chicago , il , usa )  . 
variables shown by univariate analysis to be associated with better local control or survival were further evaluated via multivariate analysis . results 40 patients ( 18 female , 22 male ) completed radiotherapy for rgbm and met the inclusion criteria . 
1 radiation planning with 95% isodoses for primary ( 30 2 gy , a ) and recurrent disease ( 20 2 gy , b ) of a patient with gbm involving the right parietal and occipital lobe . 
curves indicate no systemic therapy ( blue ) , tmz ( red ) , bevacizumab ( green ) , nitrosoureas ( orange ) , and other substances ( yellow ) ; + indicates a censored case . 
log - rank tests were performed to compare groups , see text for p - values subgroup analysis according to mgmt status in a subgroup analysis of patients with methylated mgmt promoter ( n = 14 , 35% ) , we found higher pfs2 and os2 in the tmz group vs . 
3. impact of dierent factors on toxicity table 3 shows the incidence of acute and late toxicities . local alopecia ( n = 15 ) , fatigue ( n = 7 ) , or focal seizures ( n = 4 ) were the most common acute toxicities . 
for 4 patients , grade 3 adverse events have been reported ( one case of decreased platelet count after adjuvant chemotherapy , one case of wound infection after post - radiation insertion of thermotherapy particles , one case of impaired wound healing after a third tumor resection , and one case of wound infection of the initial resection cavity )  . of 3 patients with acute toxicities grade 3 , 2 had not received systemic therapy and all had received less than 36 gy at the onset of the toxicity . 
3 pfs2 ( a ) and os2 ( b ) in patients who received up to ( blue ) or more than 36 gy ( red ) in the subgroup of patients with positive mgmt promoter methylation status ; + indicates a censored case . 
in this study , the outcome of a group of patients receiving the same primary treatment ( 60 gy in 2 gy doses along with tmz ) with different treatments for disease recurrence was followed . mean os2 in this study was 9.5 months , comparing well to the literature [ 15 ] for fractionated therapies with different single and total doses ( 25 gy and 2040 gy , respectively )  . also , the time between rst and second radiotherapy is similar to other researchers descriptions [ 9 ]  . our data show a signicant impact of mgmt promoter methylation status and time to second treatment ( 12 months or less ) as well as choice of systemic therapy on survival parameters . 
patients aged < 51 years and patients with an ecog of less than 2 showed a trend towards better survival . tumor size and extent of surgery did not show a signicant impact on outcome . 
our ndings are concordant with this scoring tool , even though we evaluated a histologically homogenous group of patients [ 14 ]  . as published in the director study , the patients in this study had a difference in os if wider surgical resection was used [ 16 ]  . additionally , statistical analyses showed a signicant impact of radiation dose on survival after diagnosis of recurrent disease in mgmt promoter - methylated patients . 
caution has to be paid , as treatment dose has to maintain a delicate balance between efcacy and toxicity . if re - irradiation is supported by the interdisciplinary board , all patients should receive at least 30 gy , as many authors described this dose as safe and lower doses are less effective [ 17 , 18 ]  . 
a necrosis rate of brain tissue of about 10% might be expected after bed doses of 90 gy or more [ 19 ] , so most physicians are cautious with higher doses after a rst radiotherapy course of 60 gy . 
in our patient group , the median survival after the second radiation treatment was 10 months , so taking early and late toxicities into account is inevitable . anyhow , the risk for brain necrosis may be overestimated , as even with the time interval between the rst and the second treatment being less than 6 months and some patients receiving more than 90 gy in sum , no brain necroses were reported in this study . 
our ndings correspond with the review of mayer and colleagues , who did not nd an increasing incidence of necrosis with increasing doses in small radiation volumes as they are used with modern radiation techniques or with smaller time intervals between therapies [ 20 ]  . as 3 patients developed grade 3 symptoms during the radiation course , coherence between radiation and sympstrahlenther onkol ( 2020 ) 196 : 457464 toms cannot be excluded . 
as no impact of the total radiation dosage or simultaneously applied systemic therapy was seen , it is unclear whether these symptoms were caused by radiation or the proceeding disease . the evidence of our ndings concerning late toxicities might be limited , as several patients conducted their late follow - up mris with external practices and reports were not continuously brought to the radiation oncology follow - ups . to differentiate between tumor progression and pseudoprogression remains a difcult task with usual mri techniques [ 21 ] , as up to 30% of patients show increased gadolinium uptake in the irradiated region , mostly during the rst 12 weeks after treatment . 
to evaluate the response to treatment , the updated response criteria of the neuro - oncology working group should be consulted [ 22 ]  . deeper insight into the role of gross resection and data on re - irradiation dose concepts are awaited from ongoing studies , such as the dose escalation study dose escalation trial of re - irradiation in good prognosis recurrent glioblastoma ( nct02709226 ) or the ongoing gliocave study , where observation after resection is compared to resection with adjuvant fractionated radiotherapy with 46 or 39 gy [ 23 ]  . the combination of re - radiation and systemic therapies was described as safe and effective by several groups [ 24 , 25 ]  . 
these data are similar to the ndings of scholtyssek et al . , who found a signicant advantage through concurrent tmz in contrast to radiation only or radiation and carboplatin / etoposide [ 26 ]  . 
 [ 10 ] , whereas other groups could not estimate an improvement trough tmz or through ctx in general [ 27 ]  . combs and colleagues did not nd a signicant impact of prior tmz application on survival parameters in a similar group of gbm patients , which underlines our suggestion to consider a second combination of radiation and tmz for recurrent disease [ 24 ]  . the majority of patients in our analysis received nitrosoureas in combination with radiation , which is considered effective and safe [ 28 ]  . 
yet we could not observe a signicant advantage of this therapy versus radiotherapy alone or versus combination with other systemic therapies . even though the vegf antagonist bevacizumab showed no advantage for primary gbm , it is commonly used in clinical practice for recurrent disease [ 29 ]  . 
to interpret the ndings of previous publications , it must be considered that the study populations were often small , with heterogeneous tumor entities and different therapeutic approaches . one limitation of this study is the small study population , which might be caused by the small number of patients being sent to radiotherapy with this respective diagnosis . another weakness is the variety in chemotherapy schemes used for the described patients and the limited information about adjuvant chemotherapy dose and number of cycles . as we saw a strong impact of chemotherapy on survival parameters , with a signicance concerning pfs2 , the very low number of patients , especially in the group receiving tmz , must be taken into account . checkpoint inhibitors have recently gained attention with groundbreaking improvements in survival rates for several tumors , and they are also target of multiple studies on gbm . as promising as these new drugs are , interactions between them and radiation need to be investigated carefully , as , for example , in the study hypofractionated stereotactic irradiation ( hfsrt ) with pembrolizumab and bevacizumab for recurrent high - grade gliomas ( nct02313272 ) , which analyses the toxicity of bevacizumab , pembrolizumab , and re - radiation as a phase i study . re - irradiation for recurrent gbm seems safe and effective . 
simultaneously applied chemotherapy , especially tmz , seems highly effective in the recurrent situation with or without proven mgmt methylation . our ndings suggest that normofractionated radiotherapy leads to good outcomes for patients with recurrent gbm after primary therapy with adjuvant radiation and tmz . 
doses of more than 36 gy should be applied , especially for mgmt promoter - methylated histology , whereas the ideal dose is still to be dened . future research is expected to reveal new insights into the effects of higher radiation doses and the interplay between systemic substances , with special interest in the new checkpoint inhibitors . compliance with ethical guidelines conict of interest a . 
eich declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants or on human tissue were in accordance with the ethical standards of the institutional and / or national research committee and with the 1975 helsinki declaration and its later amendments or comparable ethical standards and modications and in accordance with good clinical practice guidelines . 
suchorska b , weller m , tabatabai g et al ( 2016 ) complete resection of contrast - enhancing tumor volume is associated with improved survival in recurrent glioblastoma - results from the director trial . 
ryu s , buatti jm , morris a et al ( 2014 ) the role of radiotherapy in the management of progressive glioblastoma : a systematic review and evidence - based clinical practice guideline . 
hudes rs , corn bw , werner - wasik m et al ( 1999 ) a phase i dose escalation study of hypofractionated stereotactic radiotherapy as salvage therapy for persistent or recurrent malignant glioma . int j radiat oncol biol phys 43 : 293298 . 
wen py , macdonald dr , reardon da et al ( 2010 ) updated response assessment criteria for high - grade gliomas : response assessment in neuro - oncology working group . 
combs se , bischof m , welzel t et al ( 2008 ) radiochemotherapy with temozolomide as re - irradiation using high precision fractionated stereotactic radiotherapy ( fsrt ) in patients with recurrent gliomas . 
scholtyssek f , zwiener i , schlamann a et al ( 2013 ) reirradiation in progressive high - grade gliomas : outcome , role of concurrent chemotherapy , prognostic factors and validation of a new prognostic score with an independent patient cohort . 
brunner5 jens fleckenstein6 received : 4 january 2020 / accepted : 13 january 2020 / published online : 24 march 2020 the author ( s ) 2020 abstract this review details and discusses the technological quality requirements to ensure the desired quality for stereotactic radiotherapy using photon external beam radiotherapy as dened by the degro working group radiosurgery and stereotactic radiotherapy and the dgmp working group for physics and technology in stereotactic radiotherapy . 
for each part , an expert review for current state - of - the - art techniques and their particular technological quality requirement to reach the necessary accuracy for stereotactic radiotherapy divided into intracranial stereotactic radiosurgery in one single fraction ( srs ) , intracranial fractionated stereotactic radiotherapy ( fsrt ) , and extracranial stereotactic body radiotherapy ( sbrt ) is presented . 
furthermore , process quality requirements in terms of standard operating procedures , interdisciplinary discussion , training , experience , documentation , and reporting for stereotactic radiotherapy were dened . the present expert review provides the background and details for each of the technological quality requirements for stereotactic radiotherapy as described in the consensus statement [ 1 ] , taking into account the current state - ofthe - art clinical practice . 
furthermore , this review discusses and explores further needs for research and development to overcome unsolved problems . expert review for the investigation of existing methods , results and open questions for each technological quality requirement for stereotactic radiotherapy , an expert review was performed and summarized . 
additionally , this review was openly discussed at two working group meetings before and after the group peer review , each with more than 100 participants , and consensus was obtained for remaining critical questions via ballots . technological quality requirements for stereotactic radiotherapy the following technology quality requirements are specied additionally and / or are substantiated specically for stereotactic radiotherapy and do not render other established guidelines for general radiation protection and radiotherapy obsolete . 
in the following sections , we rst present the specic technological quality requirements as dened by the degro / dgmp consensus statement [ 1 ] and then discuss the current state - of - the - art and its limitations based on the literature review . imaging for target volume denition requirement : the target volume and all organs - at - risk are dened using organ - specic imaging modalities and standardized imaging protocols dedicated for stereotactic radiotherapy procedures . 
the use of secondary imaging requires accurate registration with the thin - slice planning computed tomography ( ct )  . the volume denition of intracranial and extracranial stereotactic targets and the denition of organs at risk ( oar ) require the acquisition of organand indicationspecic planning image data . 
in general , high - quality , thinslice ( organ and lesion volume - specic with ( cid : 2 ) 1 mm intracranial and 2 mm extracranial slice thickness [ 2 ] ) noncontrast enhanced ct with maximum possible in - plane resolution ( organ and lesion volume - specic with ( cid : 2 ) 1 mm intracranial and ( cid : 2 ) 1.5 mm extracranial pixel edge length ) is the primary planning imaging modality for target volume and oar denition and dose calculation purposes . 
the selection of scan length should not only consider target structures and radiation - sensitive structures that might be affected by the treatment or be necessary for dose documentation , e.g. , the whole lung for lung treatments , but also consider the treatment technique , e.g. , an extension of the target region of 15 cm in superior and inferior directions for non - coplanar sbrt [ 2 ]  . 
if unambiguous target denition is not possible on primary planning imaging data , secondary image data must be acquired and registered to the primary data to achieve maximum condence in delineating the gross tumor / target volume ( gtv ) and to minimize procedural safety margins [ 3 ]  . 
in the following section , general aspects related to the registration accuracy are summarized , followed by organ - specic paragraphs to review secondary planning imaging modalities . primary and secondary planning image data should be acquired with the patient in treatment position using well - dened , standardized imaging protocols dedicated for stereotactic radiotherapy procedures . 
planning data from external imaging devices are a major source of displacein the patient anatomy ( deviating immobilization ment devices , tabletop , etc . ) , non - standardized image quality , and undocumented artifacts . 
poor image contrast and image artifacts considerably hamper the clinicians capability to perform and verify image registration , but also inuence the accuracy of image registration and , if applicable , the auto - detection of implanted ducial markers [ 4 ]  . 
the receiver bandwidth should be set to the highest value possible that still delivers an acceptable signal - to - noise ratio , as the accuracy of the mri images ( especially in tissue transition zones ) could be a concern for contouring and for simulation [ 3 , 5 ]  . overall , accurate image registration depends on image acquisition settings , sufcient spatial resolution , and image quality . 
in areas of low contrast in the primary planning ct ( e.g. , in the liver ) , ducial markers implanted prior to treatment planning imaging could improve the registration accuracy . 
however , rigid registration algorithms are challenged by non - linear deformations mainly associated with variation of organ position , shape , and volume between the primary and secondary image acquisition . 
some non - linear deformations can be eliminated by the use of individual sub - volumes to optimize the registration process or through different importance factors to selected anatomical regions . in general , deformable image registration may further improve rigid registration results and minimize subsequent safety margins . regardless of the method , image registration requires careful validation before clinical implementation , and caseby - case evaluation due to large variation in the complexity and robustness of the registration approaches is strongly recommended [ 4 , 68 ]  . 
furthermore , the use of automated registration methods or auto - detection algorithms for implanted ducials requires the evaluation of the systems performance for various image acquisition settings ( e.g. , to identify image quality limits where the algorithm fails ) to establish appropriate institutional imaging registration protocols [ 4 , 6 ]  . intracranial since lesions or oar in the brain are often not visible on non - contrast - enhanced ct , mri , or in case the patient cannot undergo mri , contrast - enhanced ct is the standard imaging modality to dene target volumes and oar for intracranial indications . 
mri planning images should be generally acquired with a maximum slice thickness of 11.5 mm and minimum eld strength of 1.5 t [ 3 , 911 ]  . contrast - enhanced t1 - weighted imaging is commonly used for brain metastases or uveal melanomas . 
of note for brain metastases : signicant target volume changes may occur if the time between planning imaging and treatment delivery exceeds 1 week or if new decongestant medication is administered after planning imaging [ 12 , 13 ]  . 
for tumor resection cavities , additional preand direct postoperative ( ( cid : 2 ) 48 h after surgery [ 14 ] ) contrast - enhanced t1weighted sequences are desirable . 
for non - enhancing brain tumors , t2 - weighted and / or uid - attenuated inversion recovery ( flair ) sequences or positron - emission tomography ( pet ) are mainly used for target denition . 
however , specic circumstances of a wide range of benign and malignant brain tumors will require additional specic sequences or the use of pet . target volumes of vascular disorders in the brain such as arteriovenous malformations ( avm ) are dened using stereoscopic 2d digital subtraction angiograms ( dsa ) in combination with registered ct angiograms and / or mri angiograms . 
mri and / or pet may allow for better denition of the tumor lesion within the bone and potential epidural disease extension whereas t2 - weighted mri may provide the highest resolution . 
volumetric t1 - / t2 - weighted mri sequences are generally rigidly registered locally to a thinslice planning ct ( ( cid : 2 ) 12 mm slice thickness depending on target volume and location )  . 
the delineation of the spinal cord can be performed using either t2 - weighted mri or a ct myelogram in cases where the patient is unable to undergo mri or if the spinal cord is not clearly visible on mri , e.g. , due to signicant metal artefacts [ 3 , 1618 ]  . lung / mediastinum ct is the standard imaging modality for target denition of lung tumors and for oar contouring . 
to improve target volume denition , functional imaging such as fdg - pet or intravenous contrast - enhanced ct data ( e.g. , for central tumors ) may be used , desirably time - resolved [ 1921 ]  . 
in addition to gtv denition , the planning image data is also acquired to assess patient - specic target motion and deformation as well as to evaluate correlation consistency of tumor motion in relationship to any internal or external markers prior to treatment . 
the ct acquisition technique ( e.g. , 4d - ct , strahlenther onkol ( 2020 ) 196 : 421443 prospectively gated multiphase ct , breath - hold ct ) has to be chosen according to the motion management strategy applied during treatment delivery , as dened in the motion management section below [ 3 , 16 , 17 , 1923 ]  . discussion liver / abdomen planning ct imaging ( ( cid : 2 ) 2 mm slice thickness ) for abdominal tumors is identical to lung tumors , though it should be noted that organ motion in the abdomen can be signicantly larger than in the lung [ 24 ] and be non - periodic due , e.g. , to digestion [ 25 ]  . 
additionally , ( 4d ) - pet - ct imaging may , depending on the tumor histology , improve target volume delineation in contrast to the surrounding edema and in the presence of organ motion / deformation [ 3 , 16 , 17 , 2527 ]  . prostate target and oar delineation for primary prostate cancer for stereotactic radiotherapy is performed using high - resolution ( ( cid : 2 ) 1.5 mm slice thickness ) ct and mri . 
the scan length should ideally be extended by 15 cm superiorly and inferiorly beyond the prostate to cover the testicles , bladder , sigma , rectum , and lower small bowel [ 2 , 32 ]  . 
additionally , prostate denition based on standard t1 / t2 mrt sequences results in a smaller ctv ( e.g. , in the area of prostate apex and anterior rectal wall ) and thus provides more effective sparing of the rectum and neurovascular bundle and additionally enables delineation and potentially sparing the urethra of high doses [ 3 , 3234 ]  . 
additionally , prostate - specic membrane antigen ( psma ) - pet - ct could increase the denition accuracy of the intra - prostatic lesion if a simultaneous boost for sbrt is considered [ 35 ]  . generally , non - contrast enhanced ct is the primary planning imaging modality , as the use of contrast agents or other imaging modalities could lead to inaccuracies in dose calculation and image registration during treatment . 
many indications for stereotactic radiotherapy require high - resolution mri or contrast - enhanced ct for accurate target and oar delineation , for which in most clinical scenarios accurate registration to the primary planning ct is required [ 3 , 6 , 911 , 1627 ]  . 
however , quality requirements ( e.g. , for optimal contrast , artefact reduction , slice thickness , and registration ) and quality assurance ( e.g. , methods , tools , and interval ) of planning imaging devices are largely lacking for stereotactic radiotherapy . 
additionally , the time delay between planning imaging and treatment plays an important role for brain metastases [ 12 , 13 ] ; yet , for other indications , it is largely unexplored , and in general this factor is largely unreported in the literature . 
radiation reactions is largely lacking , despite already existing studies in the literature [ 3638 ]  . patient positioning and target volume localization requirement : daily in - room image - guidance and online correction of target position errors using on - board ct , supplementary in - room ct or stereoscopic x - ray is required . ( cid : 2 ) for srs , an invasive xation using a stereotactic head frame can be used alternatively to image guidance . ( cid : 2 ) for srs and fsrt , non - invasive xation of the patients head is combined with image guidance . ( cid : 2 ) for sbrt , image - guidance of the target itself ( or a surrogate structure highly correlated with the target ) is required . 
the optimal image - guidance strategy is dependent on the tumor site and location and needs to consider the following principles : in cases of target motion relative to the bony anatomy , image - guidance requires volumetric imaging with or without implanted ducial markers or electromagnetic transponders or requires stereoscopic x - ray imaging 426 strahlenther onkol ( 2020 ) 196 : 421443 of the target itself or of implanted ducial markers as target surrogate . in cases at risk of serial organs - at - risk motion into areas of critical radiation doses , volumetric image guidance is recommended . for treatment delivery , the patient has to be immobilized and positioned identically to the primary treatment planning imaging . 
the target volume itself or appropriate surrogates , if the target is not visible on setup verication imaging ( e.g. , bony anatomy for brain or spinal lesions [ 39 ] or implanted ducial markers for abdominal or prostate lesions [ 3 , 16 , 17 , 25 , 26 , 40 , 41 ] ) have to be localized in the treatment room directly before treatment . 
because of known data on possible intrafractional target motion [ 4245 ] , we strongly recommend to dene an institutional maximum time delay between setup verication image acquisition and start of treatment for all treatment sites , with a time delay as short as possible . 
to meet the accuracy requirements for stereotactic radiotherapy , this time delay should not exceed 5 min for most treatment sites [ 4245 ]  . for patient positioning and target volume localization , there currently exist no state - of - the - art setup devices besides invasive stereotactic head frames that are able to guarantee the needed positioning accuracy for stereotactic radiotherapy without image guidance [ 46 , 47 ]  . 
all image acquisitions for image - guided radiotherapy ( igrt ) are performed inside the treatment room ( in - room ) , either on board of the treatment device or integrated into the xed treatment room coordinate system to guarantee a stable geometric relation between the imaging and treatment position . 
it has to be ensured that the patient does not move due to the change in treatment table position ( e.g. , between ct - onrails acquisition and treatment )  . 
if the target volume is not visible on setup verication imaging , the geometric relation between the target volume and its surrogates has to be extracted from primary treatment planning imaging and has to be assumed constant between planning imaging and treatment . 
if the relation cannot be assumed constant , additional margins have to be applied . intracranial stereotactic radiosurgery and intracranial fractionated stereotactic radiotherapy patient positioning and target volume localization for intracranial stereotactic radiotherapy can be performed with invasive rigid head frames using stereotactic localizers for srs [ 4850 ] or with image guidance for both srs and fsrt [ 3 , 9 , 10 ]  . 
image guidance can be performed using stereoscopic x - ray imaging [ 52 , 53 ] , in - room ct , or on - board ct imaging [ 5456 ]  . 
because of higher mobility of the skull inside thermoplastic masks compared to invasive frame immobilization [ 57 ] , intrafraction head motion monitoring and delivery adaptation in frameless srs / fsrt is required in order to minimize the planning target volume ( ptv ) margins [ 9 , 42 , 58 ]  . 
methods for intrafractional motion monitoring can be found in section motion management . extracranial stereotactic body radiotherapy the intracranial image - guidance methods can be used for extracranial target volumes as well [ 1921 , 2527 , 44 , 59 ]  . for additional information on surrounding critical structures , volumetric imaging is preferred over stereoscopic imaging [ 60 ]  . 
however , those methods are not yet able to replace the state - of - the - art x - ray methods due to a lack of absolute target localization accuracy ( e.g. , ultrasound [ 61 ] , surface scanning [ 62 ] ) or a lack of clinical data for stereotactic treatments ( electromagnetic tracking [ 63 ] )  . 
for targets moving with respiration or digestion , patient positioning and motion management strategies are discussed in the motion management section below . discussion there exist a large range of systems and methods for accurate setup imaging for stereotactic radiotherapy in clinical practice [ 4863 ]  . 
however , the question of which surrogates are appropriate for targets that are not visible on setup imaging [ 6466 ] is beyond the scope of this review and needs further investigation . 
as an example , implanted ducial markers may not always have a xed interand intrafractional geometry with the actual target , and the number of ducials ( i.e. , for rotation tracking ) , the geometric arrangement , and the distance to the target strongly inuence treatment accuracy [ 6770 ]  . 
nevertheless , the current quality requirement as described above explicitly excludes mri - guided stereotactic treatments as a standard , as this technique is considered to be under investigation with rst available geometric and clinical data for mr - guided sbrt [ 7274 ] , but without long - term follow - up . 
particularly for mr - guided intracranial treatments is there currently a lack of clinical experience [ 75 ]  . strahlenther onkol ( 2020 ) 196 : 421443 motion management requirement : systematic assessment and consistent consideration of periodic and non - periodic target motion dur ( cid : 2 ) imaging for treatment planning ; ( cid : 2 ) target volume denition ; ( cid : 2 ) beam - delivery technique planning ; ( cid : 2 ) dose simulation ; ( cid : 2 ) target volume localization & repositioning ; and ( cid : 2 ) dose application using a time - resolved motion management strategy is required . 
compensation of breathing - induced uncertainties can be performed using breath - hold technique , free - breathing with gated beam delivery , free - breathing with continuous beam delivery using the internal target volume ( itv ) or mid - ventilation concept and free - breathing with dynamic tumor tracking . intrafractional target motion describes any motion that occurs during the delivery of a radiation therapy treatment fraction and can be either periodic ( breathing and / or heartbeat induced , relevant for , e.g. , lung and upper abdominal lesions such as liver , pancreas , kidney , and adrenal glands ) [ 24 , 76 , 77 ] or non - periodic ( mainly induced by spontaneous patient or target motion or from digestion , relevant for , e.g. , uveal , spine , intracranial , or prostate lesions ) [ 43 , 44 , 57 ] , which can induce systematic ( e.g. , baseline drifts ) or random treatment errors [ 3 , 4 , 19 , 20 , 2426 , 45 , 46 , 58 , 68 , 72 , 7881 ]  . any form of motion management tries to minimize the relative motion between the target volume and the treatment beabesides patient and / or target immobilization and specic diet protocols to reduce non - periodic motion , two general strategies to actively manage intrafractional target motion during dose application can be applied : tracking and gating [ 3 , 8284 ]  . 
the beam is turned on if the signal is inside a gating window , dened during treatment imaging and planning , and is turned off once the signal exits this gating window . there are three forms of gating : free - breathing periodic motion gating ( e.g. , based on a specic breathing phase or amplitude for lung and liver targets [ 9395 ] ) and nonperiodic motion gating ( e.g. , based on breath - hold under deep inspiration or expiration for lung and liver targets [ 96 , 97 ] or based on spontaneous motion in intracranial , uveal , spinal , and prostate targets [ 98100 ] ) or a combination of both periodic and non - periodic motion gating [ 72 ]  . if no active motion management technique is available for targets with non - periodic motion , additional safety margins should be considered . 
for targets with small periodic motion ( ( cid : 2 ) 5 mm ) , the internal target volume ( itv ) or midhier steht eine anzeige . 428 strahlenther onkol ( 2020 ) 196 : 421443 ventilation ( midv ) approach may be used instead of an active motion management technique . 
for the treatment of targets with larger periodic motion ( > 5 mm ) , an itv / midv approach is the minimum requirement if no active motion management technique is available or feasible [ 3 , 82 ]  . 
the itv / midv approach is a passive motion management technique that integrates time - resolved image information ( internal motion ) into the target volume by unifying all gtvs ( ctvs ) from all breathing phase cts to the itv , or for some cases by using a maximum intensity projection ct dataset derived from the 4d - ct [ 101 ]  . 
the midv concept uses the ct of the breathing phase nearest to the timeweighted mean position of the gtv ( ctv ) and integrates the peak - to - peak amplitude in all three directions into an anisotropic ptv margin [ 102 ]  . 
thereby , the irradiated volume is enlarged such that the prescribed dose is sufciently delivered to the target during treatment , while the midv approach often leads to smaller irradiated volumes than the itv approach [ 102 ]  . 
to reduce the irradiated volume , it can be benecial to reduce the motion amplitude , e.g. , through abdominal compression or active patient breathing training [ 102 ]  . 
the itv / midv approach performed under intrafractional verication of the target or surrogate motion can be considered as gating with a full - amplitude gating window . if for the itv / midv approach intrafractional verication of the target or surrogate motion cannot be performed , additional uncertainty margins should be considered . regardless of the motion management strategy , coaching of breathing patterns ( i.e. , teaching the patient how to breath ) and the training of breathing ( i.e. , repeating the taught breathing patterns ) prior to and the audible and / or visual feedback of breathing during each of the treatment steps for stereotactic radiotherapy can be crucial to reduce treatment time , uncertainties , and errors [ 4 , 103106 ]  . 
however , caution is strongly advised , as focused breathing may also lead to increased tumor motion and the feasibility and usefulness of coaching , training , and feedback should always be evaluated on a case - by - case basis . the choice for one of these motion management strategies denes the necessary requirements for all steps in the treatment chain as described in the following . imaging for treatment planning a free - breathing static ct of the lung and upper abdomen suffers from motion artifacts like blurring of structures and multiple representations of organ boundaries . 
to overcome these problems , respiration - correlated 4d - ct , prospectively gated multiphase ct , or a combination of inspiration and expiration breath - hold ct can be acquired [ 82 ]  . 
however , phase - based sorting is more affected by breathing irregularity - related motion artefacts compared to amplitude - based sorting [ 3 , 2022 ]  . the use of time - resolved imaging allows for an assessment of target motion and deformation as well as consistency validation of the relationship between the target and any surrogate used during dose delivery , regardless of the motion management strategy . 
regardless of the target location and the motion management strategy , special attention to patient preparation ( e.g. , positioning , organ lling , and breathing pattern ) has to be paid in order to reproduce the internal situation of patient anatomy at the time of planning imaging during treatment . target volume denition uncertainties in target position and shape during treatment have to be integrated into the target volume denition . 
using an itv / midv approach , the target representation from all available image data ( e.g. , from 4d ct ) can be integrated therein as described above , while the itv needs an additional ptv margin , which is included in the midv approach . 
for all motion management techniques , the ptv margin has to be enlarged such that all uncertainties from motion representation in planning imaging and all uncertainties related to the particular motion management strategy during treatment previously not considered are covered [ 89 , 107 ]  . 
examples of motion management uncertainties arise from uncompensated residual target motion , rotation , and deformation [ 81 , 108 , 109 ] , differential target and surrogate motion ( e.g. , of target and implanted ducials or diaphragm [ 66 ] ) , targetsurrogate correlation modeling [ 80 ] , motion monitoring and correlation model update frequency [ 110 ] , and motion prediction modeling due to latency times of the motion tracking systems [ 111 , 112 ]  . 
typically for stereotactic radiotherapy , ptv margins range from 02 mm for intracranial / spinal targets to 35 mm for moving extracranial targets . beam - delivery technique planning beam technique factors ( e.g. , beam modulation , mlc leaf travel ) may be considered when treating moving targets . especially in some case scenarios with a low number of fractions ( e.g. , 13 ) in combination with high dose rates ( e.g. , when using atting lter - free beams ) such interplay effects between target motion and moving parts of the delivery system could be signicant and unpredictable [ 113 , 114 ]  . 
however , averaging effects for higher fractionated stereotactic radiotherapy ( e.g. , 5 or more ) generally result in a pure gaussian blurring of the dose distribution that can be strahlenther onkol ( 2020 ) 196 : 421443 compensated by appropriate margins [ 115117 ]  . 
the simplest method to prevent interplay effects can be realized by avoiding modulated treatment sequences altogether . dose simulation the dose delivery process is a time - dependent procedure , but typically modeled as a static procedure with according uncertainty margins in treatment planning . 
there are several emerging approaches to overcome the differences between static treatment planning and dose delivery under target motion ( e.g. , 4d dose calculation [ 118121 ] , 4d dose optimization [ 122 , 123 ] , and robust treatment planning [ 124 ] )  . 
these techniques usually assume reproducibility of the target motion at the time of imaging during treatment , which has to be veried during treatment to evaluate the reliability of the dose simulation . target volume localization & repositioning for dose delivery , the assumptions made for target volume denition and treatment planning have to be fullled . therefore , the target volume itself has to be localized and positioned before each fraction using the methods dened in patient positioning and target volume localization above , adapted to the used motion management strategy . any in - room imaging for target volume localization has to be accurately registered to the primary treatment planning imaging data . 
furthermore , breathing phase information for in - room imaging is required ( e.g. , breath - hold position for on - board or supplementary in - room imaging , or 4d - cbct [ 59 , 125 ] )  . 
the target volume localization based on the methods as described has to be performed repeatedly during treatment under consideration of the additionally applied safety margif during repeated target volume localization deviations from the treatment planning assumptions are detected that are not covered by the additional safety margin as described above , patient or beam repositioning or even plan adaptation is required . dose delivery for all motion management strategies , monitoring of target motion during treatment , taking into consideration the applied safety margins , is required . 
ideally , this may be performed in real time and using non - ionizing volumetric imaging [ 71 , 127 ] ( which is currently only available at a few centers )  . 
for non - periodic target motion , deviations from reference detected by continuous motion - monitoring systems may trigger renewed target volume localization and , if necessary , patient repositioning [ 51 , 52 , 128 ]  . 
if for periodic target motion continuous motion monitoring during treatment is not feasible ( e.g. , due to target visibility or imaging dose constraints ) , accurate correlation modeling between the target and external surrogate signals ( e.g. , surface or articial marker [ 53 , 62 , 85 , 129 ] , spirometry [ 130 ] , etc . ) or verication of the correlation model obtained during planning imaging is strongly advised for stereotactic radiotherapy . 
the motion management strategy must be adapted to the fraction duration , which , in turn , should be kept as short as possible for most applications ( e.g. , by using attening lter - free beams with high dose rates )  . discussion a large variety of technologies and methods for periodic and non - periodic motion compensation for all aspects of the stereotactic radiotherapy treatment chain has been presented [ 82132 ]  . 
however , some of the techniques lack standardized validation methods , mainly due to repeatability during treatment ( e.g. , advanced 4d motion modeling and 4d dose calculation or automatic registration of intrafractional images [ 6 ] )  . 
furthermore , we want to emphasize that using an itv / midv concept for intrafractional breathing motion compensation without verication and monitoring of the actual target motion patterns before and during treatment cannot be considered a best practice for stereotactic radiotherapy of strongly moving targets . 
future directions for motion management strategies for stereotactic radiotherapy will comprise continuous volumetric imaging during dose delivery [ 71 , 72 , 136 ] as well as online adaptation to possible changes in patient anatomy and motion patterns of the target volume . 
usually the lower limit of what is provided by manufacturers today is 45 mit should be noted that the dose gradient is , in principle , steeper for smaller collimator openings as can be shown for stereotactic convergent beam irradiation [ 138 ]  . 
however , the vast majority of mlcs presently used for stereotactic radiotherapy have leaves that are much wider . one planning study compared mlc leaf widths of 2.5 mm and 5 mm using both step - and - shoot intensity - modulated radiation therapy ( imrt ) and intensity - modulated arc therapy ( imat ) techniques on two different phantoms mimicking smalland large - eld head and neck targets [ 140 ]  . 
the study found that for small elds and a small c - shaped target around an organ at risk ( oar ) , improved conformity for the 2.5 mm mlc was observed with a lower maximum for the oar together with lower peripheral doses . 
in contrast , for so - called normal sized head and neck targets , the study did not nd dosimetric benets by using the 2.5 mm instead of the 5 mm mlc . 
additionally , a study comparing a 3 mm mlc leaf width with a 5 mm mlc found that equivalent coverage with both mlcs can be achieved , whereas there was a statistically signicant better conformity for the 3 mm mlc [ 141 ]  . 
however , with both mlcs , the clinical predened dose criteria ( e.g. , rtog dose limits ) could be fullled for all cases . in another planning study on imrt for prostate targets , the inuence of the leaf width using three different mlcs with 2.5 , 5 , and 10 mm leaf width was investigated [ 142 ]  . the study found signicant improvements in dose coverage for the 2.5 and 5 mm mlcs in relation to the 10 mm leaf width , but no signicant gain when reducing the leaf width from 5 to 2.5 msimilar to this , a study comparing three different mlcs with leaf widths of 2.5 , 4 , and 5 mm for imat of spinal targets with volumes between 24 and 220 cm3 concluded that any of these leaf widths can be used for spinal sbrt [ 143 ]  . 
5 mm with respect to different levels of plan complexity , namely 5up to 17 - eld imrt and imat with one or two arcs for the treatment of pituitary adenomas , demonstrated coverage and conformity improvement with the smaller leaves of about 2% for the 5 - eld imrt and only about 0.5% for the two - arc imat technique [ 144 ]  . these studies might be exemplary to show that there is a notable benet in reducing the mlc leaf width from 10 mm , but the benet of using leaves smaller than 5 mm seems only marginal , maybe except for small or very irregularly formed targets . 
however , the differences between treatment platforms can be compensated when using more complex delivery techniques ( e.g. , [ 144 , 145 ] ) , besides other inuences on the comparison , such as calculation grid size . 
part of this ambiguity is likely caused by the fact that mlc leaf width on the one hand is an easily dened quantity , but on the other hand , the mechanical size of the leaves is only one parameter among many in dening the actual geometrical resolution for an mlc . according to sampling theory , the 2080% beam penumbra divided by 1.7 equals the optimal sampling distance , which can be half the size of the leaf width ( achievable , e.g. , by a couch displacement of half the leaf width ) [ 139 ]  . hence , the beam penumbra is crucial for the geometrical resolution of an mlc and the penumbra is mainly dened by the construction of the collimator head . 
manufacturers strahlenther onkol ( 2020 ) 196 : 421443 place the mlc at different positions with respect to the diaphragm ( s ) and , by the same token , to the patient , which can lead to variations in the penumbra by a factor of about 1.5 ( [ 146 ] , the principal differences between manufacturers of newer mlcs are similar )  . 
in addition , ideas exist to reduce the leaf resolution and penumbra for the given mechanical setups , e.g. , by using a so - called virtual isocenter , which adds to the complexity of dening the treatment quality solely based on the mlc leaf width [ 147 ]  . 
another example of a factor inuencing the beam penumbra is the elongated elliptical shape of the beam focus with a relation of 1 to 2 for the axes using an achromatic 270 bending magnet system [ 148 ]  . 
from that , a dependence of the beam penumbra on the diaphragm angle would follow . the importance of the beam focus size as a crucial beam parameter is widely stressed in connection with small eld dosimetry ( e.g. , [ 3 ] )  . 
this leads to the question of how these parameters are correctly implemented into the treatment planning system at all , since in many cases the baseline data , e.g. , beam proles , consist only of measurements of the xed jaws . these considerations illustrate that a certain leaf width alone as a requirement to dene treatment quality might not be meaningful . 
however , in connection with helical treatment , especially for srs , the inherent coplanarity of this modality ( and for others , too ) might be an additional disadvantage [ 155157 ]  . 
when compared with other stereotactic radiotherapy treatment platforms , helical radiotherapy perhier steht eine anzeige . 432 strahlenther onkol ( 2020 ) 196 : 421443 formed worse in some of the studies [ 158 , 159 ] , though not in all cases . 
in a planning study comparing forwardplanned stereotactic conformal radiation therapy ( scrt ) , imrt , and helical radiotherapy , the results demonstrated that helical radiotherapy was superior to scrt , including a better hippocampal sparing for close target lesions [ 159 ]  . additionally , another study claimed that sparing the hippocampus was feasible with four treatment platforms , including one for helical radiotherapy [ 160 ]  . 
furthermore , in one study , helical radiotherapy was even favored over conebased gantry - based linear accelerators in cases where oar prevented the use of non - coplanar beams [ 158 ]  . 
likewise , another study could not show superiority ( or inferiority ) of helical radiotherapy over gantry - based systems for arteriovenous malformations in general , but found advantages for the former for targets with special geometry [ 161 ]  . from a more theoretical point of view , one could apply the argument of the sampling theory regarding optimal leaf resolution especially to helical radiotherapy , because it is rather sampling and not leaf width which denes the resolution of an mlc [ 139 ]  . 
the continuous couch movement , inherent to helical treatment , produces a sample width which is smaller than the eld width parallel to the couch motion direction ( minimal 1 cm ) and the perpendicular leaf width itself , and thus should produce a better resolution than could be expected from mechanical size alone . 
in conclusion , there seems to be sufcient physical rationale to not exclude helical therapy from being used for fsrt . however , for very small targets and situations where noncoplanar beams might be of advantage , the use of helical radiotherapy is not advised [ 155157 ]  . discussion we found that the mlc leaf width may be a simple measure for assessment of the geometrical resolution of treatment platforms and hence serve as a quality requirement for stereotactic radiotherapy based on the literature [ 139148 ]  . however , looking deeper into the treatment plan quality , the mlc leaf width does not directly represent the minimal possible eld size , which is , together with the beam penumbra and its origins ( e.g. , beam spot size ) , also an important parameter to dene the geometrical resolution [ 162 ]  . 
these inuences should be further investigated , especially when looking at srs and fsrt using very small mlc or circular collimator elds with inherent dosimetric inaccuracies , e.g. , due to shielding of the primary source with the collimator . 
for very small elds formed by a dynamic aperture ( mlc or , e.g. , cyberknife iris collimator [ accuray inc , sunnyvale , usa ] ) , the accuracy and reproducibility of leaf ( or aperture ) positioning should also be considered in an analysis of dosimetric reliability . 
another aspect of treatment plan quality is the simple fact that the hardware alone does not make a good treatment plan , which is always a combination of conformity to the target volume , steep dose gradients in the healthy tissue , and the technical applicability under realistic conditions . 
while this has been investigated for numerous indications and well - described methods exist to improve treatment planning [ 167 ] , center or even user credentialing for stereotactic radiotherapy is still lacking in germany . dose calculation requirement : for stereotactic radiotherapy in areas with large density inhomogeneities the use of a dose calculation algorithm that takes into account lateral electron transport to correct for density inhomogeneities is required . 
the maximum grid size for dose calculation should be 12 mm according to the target lesion dimensions and the image resolution for target denition . primarily , the dose calculation for stereotactic radiotherapy applications is performed on the primary treatment planning ct and the accuracy of a dose calculation algorithm is strongly inuenced by the underlying physics modelling the transport of secondary particles ( i.e. , scattered photons and electrons )  . 
while this problem is less relevant for homogeneous situations and eld sizes larger than about 3 3 cm2 ( or associated to the range of electrons ) , it is crucial in areas with high density differences ( e.g. , in thoracic or head and neck regions ) and for small eld sizes especially when combined with high - energy treatment beams . the range of suitable beam energies is considered to be ( cid : 2 ) 10 mv due to the reduced range of secondary electrons , the reduced transmission through the beam dening system , and the reduced neutron production when compared with beam energies larger than 10 mv [ 3 ]  . 
it is important to understand that it is mainly the management of the lateral spread of scattered particles that determines the accuracy level of a dose calculation algoriththis is the background to distinguish between type - a algorithms , which model only the primary particle transport correctly and in which the approximation of the secondary particle transport is generally based on equivalent path length scaling , and type - b algorithms , which include more sophisticated models for the management of secondary particles [ 3 ]  . 
examples of type - a algorithms are ray - trace algorithms , pencil beam algorithms , or fast fourier convolution algorithms , which all ignore changes in lateral electron transport . 
convolution / superposition algorithms as well as collapsed cone convolution algorithms , which take changes in lateral electron transport into account , are examples of type - b algostrahlenther onkol ( 2020 ) 196 : 421443 rithms . 
the anisotropic analytical algorithm ( aaa ) is considered an intermediate type - a / type - b algoriththe more advanced type - b algorithms sometimes also referred to as type - c algorithms , which explicitly consider the lateral particle transport , include monte carlo algorithms as well as solver of the boltzmann transport equation [ 3 , 168 ]  . for radiotherapy applications using photon beams including stereotactic techniques , the dose calculation algorithm determines the absorbed dose within a volumetric element ( dose scoring voxel ) of a given ct dataset representing the patients characteristics . 
the resulting accuracy of the estimated dose distributions for the different dose calculation algorithm depends on the specic situation considered such as eld size , photon beam energy , dose scoring voxel size , and tissue / density heterogeneity ( i.e. , treatment site specic ) , but also on the implementation of the algorithm itself . 
in addition , the accuracy depends on the accuracy of the beam model used by the dose calculation algorithm along with a careful commissioning and validation , especially with the focus of the foreseen clinical application [ 3 ]  . 
this may include additional tasks like verication of output factors for very small eld sizes and the consideration of appropriate dose calculation algorithm quality assurance procedures following updates or upgrades . 
furthermore , it is important to understand not only the approximations used in the dose calculation model , but also its implementation in order to anticipate potential shortcomings for dedicated applications ( e.g. , high resolution of the uence is more important for small than for large radiation elds )  . typically , the accuracy for small eld sizes and large energies is reduced in tissues with densities substantially different from water ( e.g. , lung [ 169 , 170 ] )  . 
for stereotactic applications , an isotropic grid size of smaller than or equal to 2 mm is considered appropriate [ 2 ] ; however , for very small targets , dose grid resolution of 1 mm or better may be needed [ 172 ]  . 
regardless of the dose grid resolution and the dose calculation algorithms used , the resolution of the primary planning imaging on which the dose calculation is performed should always be equal to or better than the dose grid resolution . 
many studies have been performed to investigate the level of accuracy for different dose calculation algorithms involving small eld sizes and tissue inhomogeneities : in summary , type - a dose calculation algorithms lead to dose overestimation in target volumes located in low - density tissue when compared with type - b algorithms or with detailed measurements [ 3 , 173 ]  . 
studies showed that intermediate type - a / type - b algorithms , i.e. , including the aaa algorithm , provided acceptable estimation of dose distributions for stereotactic applications if no lowdensity tissue is present , but they are of limited accuracy in the context of lung sbrt [ 168 , 174177 ]  . 
finally , studies showed that advanced type - b ( or type - c ) algorithms accurately calculate dose for small elds in heterogeneous tissue and are best suited for stereotactic radiotherapy treatment planning , as recommended by the international commission on radiation units and measurements ( icru ) report 91 [ 3 ]  . discussion it is largely agreed upon that dose calculation should be as accurate as clinically feasible and density inhomogeneities can be addressed with modern dose calculation algorithms [ 2 , 168179 ]  . 
furthermore , not only the target volume has to be considered , but the differences that might occur in organs at risk are also important [ 183 , 184 ]  . furthermore , mri is often used due to the high soft tissue contrast and the mr images are then registered to the ct dataset in treatment planning [ 185 ]  . 
while mronly planning is common practice for gamma knife treatments , a synthetic ct is typically generated based on the mr image dataset when using other treatment modalities . however , there are currently still limitations in the mr - only approach for stereotactic radiotherapy , which comprise dose calculation uncertainties due to errors in hu assignments and image distortions [ 186 ]  . 
additionally , beam delivery under mr real - time guidance may necessitate incorporating the mri - based dose distortions into dose calculation , 434 strahlenther onkol ( 2020 ) 196 : 421443 especially in areas with density inhomogeneities . 
thus , additional studies have to be performed on this topic . treatment unit accuracy requirement : a geometric accuracy with three - dimensional spatial dose placement in system - specic end - toend tests requires inaccuracies of at maximum : ( cid : 2 ) 1 mm for srs . ( cid : 2 ) 1.25 mm for fsrt and sbrt in non - moving phantoms . ( cid : 2 ) 1.5 mm for sbrt in moving phantoms . however , for fsrt and sbrt close to radiation - sensitive critical structures the same geometric accuracy requirement as for srs is recommended . a dosimetric accuracy with point - based plan - to - measurement differences of maximum 3% within a target volume of more than or equal to 2 cc , measured in systemspecic end - to - end or delivery - quality - assurance tests with homogeneous phantoms , is required . 
for target volumes smaller than 2 cc , the uncertainties of the measurement may be larger than the desired dosimetric accuracy . the dedicated distributed literature search in pubmed / medline revealed a total of 462 publications for the keywords used . 
after nal abstract screening and after adding well - known guidelines for stereotactic radiotherapy not listed in pubmed / medline , a total of 35 publications and guidelines remained for full data extraction . 
the complete data extracted for the publications and guidelines can be found in table 1 in the supplementary material ( online resource 1 )  . concerning international guidelines , the iaea technical report series 483 advised a geometric accuracy of 2 mm and a dosimetric accuracy of 310% in system - specic end - toend tests [ 154 ] ; however , this advice is for radiotherapy in general and not specically tailored to stereotactic radiotherapy . 
the estro / acrop guideline for lung sbrt on the other hand advised a geometric and dosimetric accuracy of 0.54 mm ( median 1.25 mm ) and 25% ( median 3% ) , respectively [ 20 ]  . 
other notable international guidelines , including the aapm - rss guideline 9a for srs - sbrt , recommended a geometric accuracy of 1 mm for static and 1.5 mm for moving targets with 5% dosimetry accuracy [ 172 ]  . 
on the other hand , the recent comp reports for the same system advised on a geometric accuracy of 0.75 mm for static and 1.0 mm for moving targets based on recent developments in the systems architecture [ 188 ]  . 
interestingly , no guideline reported specically on the overall phantom test uncertainty , but of course the phantom test uncertainty itself plays an important role in the measured overall accuracy of the stereotactic treatment system as well . 
adding recent literature to these guidelines , one can safely assume on one hand that well - calibrated dedicated stereotactic radiotherapy equipment can reach the required level of mechanical precision of 1 mm in system - specic static end - to - end tests for srs [ 189197 ]  . 
additionally , a geometric accuracy of ( cid : 2 ) 1 mm is clearly necessary for srs in order to keep the overall ptv margin ( cid : 2 ) 2 mm when also considering patient motion during treatment before side effects increase signicantly for the high srs doses [ 9 ]  . 
at this point , it should be noted that a ptv margin of 0 mm , which is often used in srs , is geometrically infeasible with the current treatment units under consideration of patient and target motion . 
hence , the use of a 0 mm ptv margin may be derived from clinical decisions and potentially be compensated by higher prescription doses . when looking at non - continuous volumetric imaging alone ( i.e. , cbct ) , there are a number of reports of endto - end tests exceeding the limits of 1 mm [ 3 , 198201 ] , even though the recent comp report on cbct advised achieving a geometric accuracy of < 1 mm [ 201 ]  . 
hence , the accuracy of cbct alone may not necessarily be sufcient for srs , especially when further considering patient motion during treatment ( see the patient positioning and target volume localization and motion management sections above )  . 
on the other hand , for fsrt and sbrt in non - moving organs , the required geometric precision of 1.25 mm should be achievable with well - calibrated cbct systems , which then may be sufcient to keep the overall treatment accuracy below 23 mm when considering patient motion during treatment [ 9 ]  . 
this recommendation is also in line with guidelines and studies including helical therapy and recently introduced integrated mr - linac devices [ 3 , 189 , 190 , 202 , 203 ]  . 
however , when looking at irregular moving targets for sbrt , the geometric accuracy of any system in current clinical use may quickly exceed the required limits of 1.5 mm in moving phantoms [ 172 , 187 , 204 ] , and only careful motion modeling and compensation may allow the overall ptv margins to be kept below 35 mm when additionally considering patient hier steht eine anzeige . motion and local target baseline shifts and deformation during treatment ( see motion management section )  . concerning the dosimetric accuracy of the treatment systems used for stereotactic radiotherapy , high - quality data arise mostly from clinical trial audits . 
in homogeneous phantoms , the dosimetric end - to - end or delivery - quality - assurance accuracy was found to be well below the required 3% limit [ 190 , 197 , 205207 ]  . 
however , when looking at moving targets and especially those targets surrounded by heterogeneous tissue , it becomes apparent that the 3% dosimetric accuracy cannot always be reached without type - c dose calculation algorithms ( see dose calculation section ) [ 205 ]  . discussion all dedicated and well - tuned devices for stereotactic radiotherapy can fulll the obligations for high geometric and dosimetric accuracy during end - to - end tests [ 2 , 3 , 9 , 89 , 172 , 187219 ]  . 
furthermore , clear recommendations for the acceptance of end - to - end tests for moving targets in heterogeneous tissues are currently lacking . furthermore , no data exist to support a recommendation on any system - specic end - to - end or delivery - quality - assurance test for small target volumes ( i.e. , ( cid : 2 ) 2 cc )  . 
additionaly , no clear recommendations on the method and the acceptance criteria of delivery - quality - assurance tests can be given , since the literature including international recommendations is largely heterogeneous and even contradictory to some degree . dedicated quality assurance measures requirement : dedicated quality assurance measures are required : ( cid : 2 ) small eld dosimetry for commissioning . ( cid : 2 ) system specic end - to - end testing for both static and moving target volumes . ( cid : 2 ) regular check of the geometric and dosimetric accuracy according to system - specic guidelines . ( cid : 2 ) day - to - day quality control of the consistency of stereotactic frame and / or the image - guidance system isocenter with the treatment beam isocenter . stereotactic radiotherapy makes use of small radiation elds due to the generally small targets treated [ 3 ]  . 
hence , it becomes necessary to use adequate measurement tools and compensate for measurement uncertainties in small 436 strahlenther onkol ( 2020 ) 196 : 421443 elds specically during system commissioning ( e.g. , using correction methods for output factor measurements for the smallest eld sizes ) , but also for the whole quality assurance chafor small eld dosimetry , the iaea has recently reported a comprehensive practical guideline [ 208 ] and the german institute for standardization ( deutsches institut fr normung [ din ] ) has published a new norm for the dosimetry of small photon beams [ 220 ] , both which we consider mandatory state - of - the - art practice for stereotactic radiotherapy . further , for full commissioning of radiotherapy devices used for stereotactic radiotherapy , dedicated full treatment chain end - to - end tests are required [ 221 ]  . 
in this regard , a full treatment chain end - to - end test phantom validation must include all treatment steps including primary and secondary imaging and its registration and subsequent target volume delineation ( imaging for target volume definition ) , dose calculation ( dose calculation ) , phantom positioning and target volume localization ( patient positioning and target volume localization ) , and target motion compensation ( motion management ) , and must fulll the specied geometric and dosimetric accuracy ( treatment unit accuracy )  . 
there are a wide range of system specic recommendations available which are considered mandatory state - of - the - art practice for each of the systems in description [ 172 , 187 , 188 , 201 , 209 , 221 , 222 ]  . 
parts of these recommendations are specic details on daily quality assurance which minimally requires verication of the consistency of the stereotactic frame and / or the image - guidance system with the treatment isocenter ( which is a modern version of the so called winstonlutz test [ 223 ] , normally reduced in number of inspected axes for a daily check )  . discussion recently , comprehensive small - eld dosimetry and systemspecic quality assurance guidelines have been published for stereotactic radiotherapy [ 172 , 187 , 188 , 201 , 208 , 209 , 220222 ]  . 
however , the translation from the old to the new methods has only just begun and the clinical implications are not yet fully understood ( e.g. , when correcting the output factors and hence changing the absolute dose for high - dose small - eld srs for trigeminal neuralgia )  . 
another point is that contouring based on mri as well as treatment planning are generally not part of the end - to - end test chain , though they clearly should be . 
furthermore , generally only the simplest forms of end - to - end tests are performed , leaving many treatment scenarios unveried ( e.g. , non - isocentric and / or simultaneous multiple lesion treatment techniques and complex moving and / or deforming target volumes with dual periodic , i.e. , respiratory and cardiac motion , and / or non - periodic motion )  . 
additionally , the interval for repeating full treatment chain end - to - end and delivery - quality - assurance tests is not well agreed upon . regardless , independent validation methods and external audits are also lacking specically for stereotactic radiotherapy in germany . conclusion the present expert review from the dgmp working group for physics and technology in stereotactic radiotherapy summarizes technological quality requirements for stereotactic treatments using photon external beam radiotherapy in the form of necessary minimum requirements often complemented by recommendations or suggestions for optimal quality . 
imaging for target volume denition emphasizes the need for indication - adapted treatment planning imaging , gives information on the use of multiple secondary imaging datasets for many treatment sites , and complements this with statements on reliable image registration with the planning ct . in treatment unit accuracy the requirements for interfractional patient positioning and target volume localization based on daily igrt depending on technique ( srs , fsrt , sbrt ) and visibility and anatomic properties of the target volume and nearby critical structures are described . 
thereby , the choice of the motion management technique is considered the most important rst step , as the technique will have strong impact on each individual link in the treatment chain . collimation of the irradiation and beam directions summarizes the requirements on beam collimation and beam directions , with a detailed analysis of the inuence of mlc leaf width and other hardware components on the treatment plan quality . 
adding to that , in dose calculation , the necessity of a dose calculation algorithm suited to the tissue density properties in the target region is strahlenther onkol ( 2020 ) 196 : 421443 emphasized and explained . 
this necessity is extended by a description of the inuence of the dose grid resolution and beam energy on the dose calculation accuracy . the requirements of the geometric and dosimetric treatment unit accuracy with static and moving homogeneous phantoms are given and discussed in treatment unit accuracy . 
moustakis declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
to view a copy of this licence , visit strahlenther onkol ( 2020 ) 196 : 485 correction correction to : long - term endothelial dysfunction in irradiated vessels : an immunohistochemical analysis raimund h . 
neukam1 marco kesting1 carol - immanuel geppert2 falk wehrhan1 published online : 9 january 2020 springer - verlag gmbh germany , part of springer nature 2020 correction to : strahlenther onkol 2018 the original version of this article unfortunately contained a mistake . 
the authors thank carsten kronauer and florian obstmeier for conducting the immunohistochemical staining and detecting the expression of mediators . the online version of the original article can be found under ( cid : 2 ) raimund h . 
grosu8 daniela schmitt5 stephanie tanadini - lang1 christos moustakis9 published online : 24 march 2020 the author ( s ) 2020 abstract stereotactic radiotherapy with its forms of intracranial stereotactic radiosurgery ( srs ) , intracranial fractionated stereotactic radiotherapy ( fsrt ) and stereotactic body radiotherapy ( sbrt ) is today a guideline - recommended treatment for malignant or benign tumors as well as neurological or vascular functional disorders . 
3 , 79106 freiburg , germany 9 klinik fr strahlentherapie , universittsklinikum mnster , munster , germany stereotactic radiotherapy today is a guideline - recommended treatment for malignant or benign tumors as well as neurological functional or vascular disorders . 
despite the highest level of evidence in randomized controlled trials and despite the existence of national and international practice recommendations , there is no generally accepted denition of stereotactic radiotherapy , especially since accurate image guidance has largely replaced stereotactic frames . 
similarly , there are no generally accepted and comprehensive quality requirements for stereotactic radiotherapy . this lack of consensus was identied by the german society for radiation oncology ( degro ) and therefore the degro board mandated the degro working group for radiosurgery and stereotactic radiotherapy to establish a statement about denition and quality requirements of stereotactic radiotherapy . 
previous published guidelines of the degro working group for radiosurgery and stereotactic radiotherapy [ 14 ] , the european society of radiation oncology ( estro ) [ 5 ] , the american college of radi418 strahlenther onkol ( 2020 ) 196 : 417420 ology ( acr ) , the american society for radiation oncology ( astro ) [ 6 , 7 ] and the united kingdom consortium for stereotactic radiotherapy [ 8 ] , as well as international literature and national and international recommendations formed the basis . 
in 2018 , a statement about the denition and general quality requirements for stereotactic radiotherapy was established and published by the degro society . this consensus statement was amended to the current version in collaboration with the german society for medical physics ( dgmp ) working group for physics and technology in stereotactic radiotherapy , taking into consideration the results of an expert review on technological quality requirements for stereotactic radiotherapy [ 9 ]  . definition for stereotactic radiotherapy there are three types of stereotactic radiotherapy , which differ with regard to the spectrum of indication , fractionation and quality requirements : ( 1 ) stereotactic radiosurgery ( srs ) as a treatment of intracranial malignant or benign tumors and functional or vascular disorders with one single irradiation fraction , ( 2 ) fractionated stereotactic radiotherapy ( fsrt ) of intracranial malignant or benign tumors and functional or vascular disorders as well as ( 3 ) stereotactic body radiotherapy ( sbrt ) of extracranial malignant or benign tumors and functional or vascular disorders . generally , stereotactic radiotherapy is dened as 1 . 
for tumors , the target volume is conned to the macroscopic tumor and a small surrounding volume of potential microscopic tumor spread . details to ( 3 ) : all substeps of stereotactic radiotherapy are systematically optimized and appropriate quality assurance measures have been implemented to achieve high precision and accuracy of stereotactic radiotherapy . 
from a clinical perspective , this includes disease staging , the interdisciplinary discussion for indicating stereotactic radiotherapy , the choice of optimal pretreatment imaging with appropriate spatial and temporal resolution for target volumes and organs - at - risk denition and highly conformal radiation treatment planning , frame - based and / or imageguided radiation delivery with active or passive motion management during treatment and close follow - up including dedicated imaging for evaluation of the treatment outcome , preferably by the treating institution . 
from a medical physics perspective , additional and more sophisticated quality assurance procedures and often tighter acceptance limits are necessary for stereotactic radiotherapy as compared to conventional fractionated radiotherapy . details to ( 4 ) : due to extreme hypofractionation , radiotherapy doses in stereotactic radiotherapy are biologically at least as high , often higher , as compared to radical radiation therapy doses using conventional fractionation . details to ( 5 ) : stereotactic radiotherapy doses are delivered in a few ( maximum 12 ) fractions . 
a risk - adapted adjustment of the fractionation and the total dose based on the volume and location of the target is essential . details to ( 6 ) : the primary goal of stereotactic radiotherapy is long - term local tumor control for cancer therapy or the destruction of cell and / or tissue function for functional or vascular indications with minimal risk of side effects . 
these are to be interpreted as minimal requirements which must be fullled to achieve best clinical outcome and treatment quality for stereotactic radiotherapy . for further details on the technological requirements we refer to the expert review of the dgmp working group for physics and technology in stereotactic radiotherapy [ 9 ]  . technological quality requirements ( 1 ) imaging for target volume denition : the target volume and all organs - at - risk are dened using organ - specic imaging modalities and standardized imaging protocols dedicated for stereotactic radiotherapy procedures . 
the use of secondary imaging requires accurate registration with the thin - slice planning computed tomography ( ct )  . strahlenther onkol ( 2020 ) 196 : 417420 ( 2 ) patient positioning and target volume localization : daily in - room image - guidance and online correction of target position errors using on - board ct , supplementary in - room ct or stereoscopic x - ray is required . ( cid : 2 ) for srs , an invasive xation using a stereotactic head frame can be used alternatively to image guidance . ( cid : 2 ) for srs and fsrt , non - invasive xation of the patients head is combined with image - guidance . ( cid : 2 ) for sbrt , image - guidance of the target itself ( or a surrogate structure highly correlated with the target ) is required . 
compensation of breathing - induced uncertainties can be performed using breath - hold technique , free - breathing with gated beam delivery , free - breathing with continuous beam delivery using the internal target volume ( itv ) or mid - ventilation concept and free - breathing with dynamic tumor tracking . ( 4 ) collimation of the irradiation and beam directions : for the respective treatment modalities , collimation and beam direction requires the following characteristics : ( cid : 2 ) srs with multileaf collimator ( mlc ) with leaf width ( cid : 2 ) 5 mm or cylindrical collimators of equivalent size , both at normal treatment distance , and used with systems allowing non - coplanar beam directions . ( cid : 2 ) fsrt with mlc with leaf width ( cid : 2 ) 6.5 mm or cylindrical collimators of equivalent size , both at normal treatment distance . however , for fsrt and sbrt close to radiation - sensitive critical structures the same geometric accuracy requirement as for srs is recommended . a dosimetric accuracy with point - based plan - to - measurement differences of maximum 3% within a target volume of more than or equal to 2 cc , measured in systemspecic end - to - end or delivery - quality - assurance tests with homogeneous phantoms , is required . 
a trained multiprofessional stereotactic radiotherapy project team ( radio - oncology , medical physics , radiation therapists ) for the implementation and application of srs / fsrt / sbrt is required . 
moustakis declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
wirtz1 , 2 susanne temming1 , 3 martin kocher1 sabine kunze1 robert semrau1 , 4 received : 19 july 2019 / accepted : 21 november 2019 / published online : 12 december 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose the role of postoperative irradiation to contralateral non - involved neck nodes in lateralized carcinoma of the head and neck is not clear . 
the contralateral neck failure rate in head and neck carcinoma treated postoperatively with ipsilateral neck irradiation only was evaluated . methods patients with carcinoma of the oral cavity , oropharynx , or hypopharynx without midline extension treated between 1990 and 2016 were analyzed . 
there was no signicant difference in contralateral nodal failure rate with or without performance of contralateral nd . conclusion regional failure of the contralateral neck was low after surgery and ipsilateral neck irradiation in head and neck carcinomas without midline extension , supporting evidence that contralateral neck radiotherapy can safely be omitted in selected cases . keywords head and neck squamous cell carcinoma oropharyngeal cancer unilateral postoperative radiotherapy head and neck cancer contralateral lymph node metastases introduction unilateral neck irradiation ( dened as radiotherapy to the primary site and ipsilateral lymph node areas only ) is adequate for selected patients with oropharyngeal carcinoma mirja m . 
62 , 50937 cologne / koeln , germany 2 department of internal medicine , geisinger medical center , 100 n academy ave , danville , pa 17822 , usa 3 department of radiation oncology , robert - janker klinik , villenstr . 
45 , 53840 troisdorf , germany [ 15 ] in terms of tumor control and reduces morbidity such as xerostomia , dysphagia , hoarseness , atrophy , brosis , and edema compared to bilateral radiotherapy [ 6 , 7 ]  . 
american society of clinical oncology ( asco ) and american society for radiation oncology ( astro ) both recommend unilateral radiotherapy for t1 - t2 and n0 - n1 ( according to tumor node metastasis [ tnm ] classication version 7 ) welllateralized tonsillar carcinomas in their current evidencebased clinical practice guidelines [ 8 ]  . 
for more advanced ipsilateral locoregional disease and patients with other entities , the optimal treatment strategy remains controversial due to the high risk of occult contralateral neck involvement [ 911 ]  . 
whereas the american college of radiology ( acr ) generally recommended bilateral neck irradiation for tonsillar cancer with a nodal stage of n2b or greater in their 2011 guideline [ 12 ] , asco endorses unilateral radiotherapy to patients with n2b lateralized tonsillar carcinomas under certain conditions [ 8 ]  . strahlenther onkol ( 2020 ) 196 : 474484 there are also some differences in handling the neck dissection as a diagnostic and therapeutic procedure . 
an elective neck dissection ( end ) of a clinically negative ipsilateral ( cn0 ) neck is usually recommended [ 13 ] and has proven benecial over therapeutic neck dissection of nodal relapse after watchful waiting [ 14 ]  . 
both sentinel node biopsy [ 15 ] and pet - ct surveillance [ 16 ] may be appropriate alternatives to spare patients with oral cancer morbidity from ipsilateral neck dissection , but these approaches remain experimental . the role of contralateral elective neck dissection in case of a clinically n0 neck is not covered in most clinical guidelines and its value is even more controversial than ipsilateral neck dissection ( nd )  . 
often , contralateral neck dissection in an n0 neck is performed if a substantial risk for contralateral lymph node metastases is present in certain tumor entities ( i.e. , base of tongue or hypopharyngeal tumors ) and in more advanced tumors with pronounced ipsilateral lymphatic spread . 
showed that patients with head and neck cancer undergoing surgery of the primary tumor plus neck dissection ( without receiving postoperative radiation to the pathologically n0 neck ) had 97% control in the unirradiated n0 neck while no signicant therapyinduced adverse effects were noted [ 17 ]  . the clinical evidence for unilateral neck irradiation focuses on a homogenous group of well - lateralized tonsil carcinomas with no or only small inltration of soft palate and base of tongue [ 4 , 18 ]  . 
the present study evaluates the rate of contralateral neck failure in a large cohort of patients with oropharyngeal , hypopharyngeal , and oral cavity carcinomas without midline extension and contralateral stage n0 who were treated postoperatively with unilateral neck irradiation . material and methods patients with carcinoma of the oral cavity , oropharynx , or hypopharynx treated at a major german oncologic center between november 1990 and march 2016 with a dened clinical management approach of ipsilateral neck irradiation only were retrospectively reviewed . 
inclusion criteria were primary diagnosis of carcinoma of the oral cavity , oropharynx , or hypopharynx without midline extension and no evidence of distant metastases , treated with primary surgery and postoperative radiotherapy / radiochemotherapy to the primary tumor and unilateral neck nodes . 
surgery after initial staging included resection of the primary tumor with unilateral or bilateral neck dissection . treatment radiotherapy was delivered postsurgery on linear accelerators using 6 - mev photons after wound healing was completed . 
the presence of acute and late therapy - related toxicity ( dermatitis , xerostomia , dysgeusia , and mucositis ) was assessed at 3 , 6 , and 12 months from the beginning of radiotherapy and annually thereafter . endpoints statistics the primary endpoint of this study was freedom from failure of the contralateral neck as rst event , secondary endpoints were locoregional control , overall survival ( os ) , and disease - free survival ( dfs )  . all outcomes were measured from the rst date of diagnosis and all estimates were generated using the kaplanmeier method . 
os was calculated based on the interval between the rst date of diagnosis and death of any cause , dfs was calculated by using the time difference between the date of initial diagnosis ( reects date of biopsy ) and either death or distant or locoregional tumor recurrence . 
approximately two thirds of all patients were staged t1 or t2 ( 77.1% ) and most patients ( 80.7% ) had lymph node involvement ( tables 1 and 2 )  . all patients underwent surgery of the primary tumor . 
in multivariate analyses , alcohol consumption remained the only statistically signicant factor ( odds ratio [ or ] 0.382 , 95% condence interval [ ci ] 0.1900.767 , p = 0.007 ; table 5 )  . factors associated with locoregional failure there were signicant associations between the freedom from locoregional failure and use of chemotherapy ( p = 0.021 ) and heavy alcohol consumption ( p = 0.003 ) as well as a non - signicant association of smoking ( p = 0.077 ) in univariate analyses . 
this study represents one of the largest series of postoperative squamous cell carcinoma of the head and neck treated with unilateral neck irradiation and extends the available data not only for oropharyngeal carcinomas but also for hypopharyngeal and oral cavity carcinomas . 
3 kaplanmeier plot of disease - free survival ( dfs ) years 480 strahlenther onkol ( 2020 ) 196 : 474484 strahlenther onkol ( 2020 ) 196 : 474484 fig . 
4 kaplanmeier plot of freedom from locoregional failyears however , there was a signicant association between the use of chemotherapy as well as hazardous consumption of alcohol and overall survival in univariate analysis . failure of the contralateral neck several studies on efcacy of unilateral radiotherapy in head and neck carcinomas mainly focus on well - selected squamous cell carcinomas of the tonsil and conrm the low rate of contralateral neck recurrences ( [ 1 , 2 , 4 , 5 , 19 ] ; see table 6 )  . 
as such , in lateralized tumors of the oral cavity , neck control on the contralateral neck was also excellent , justifying unilateral radiotherapy to carcinomas other than the tonsil . 
it led to the recommendation that contralateral neck nodes should be included in the postoperative radiotherapy volume in case of pn2b or pn3 ipsilateral lymph node involvement , which somehow can be conrmed by the fact that in 12 recurrences in the present study , 5 patients were staged ipsilateral pn2b . tumor - dependent factors that lead to contralateral lymph node metastases are not well known . 
the sentinel european node trial ( sent ) , a large sentinel node biopsy study designed for management of the n0 neck in oral squamous cell carcinoma revealed a contralateral node drainage of 12.4% only in lateral tumors , whereas midline tumors were found to spread bilaterally to the neck in 60% of cases [ 15 ]  . 
a higher frequency of midline - crossing lymphatic vessels in certain tumor localizations ( for instance in base of tongue and uvula ) may affect contralateral drainage and frequency of contralateral lymph node metastases [ 21 ]  . 
in a recently reported prospective trial by contreras et al . , 73 patients with cancer of the oropharynx , oral cavity , hypopharynx , and larynx were treated with postoperative unilateral radiotherapy after primary surgery . contralateral neck dissection conrmed a contralateral pn0 neck . 
although 71% had midline - crossing tumors , the rate of contralateral neck failure remained low ( 3% ) [ 17 ]  . primary tumor size and tumor location determine lymphatic metastasis spread . 
recently justied ipsilateral neck treatment for lateralized tumors of the gingiva , our of mouth , the lateral border of the tongue , sinus piriformis , tonsillar fossa without extension to soft palate , and base of the tongue , although prospective data on reduction of treatment volumes in uninvolved neck nodes are scarce [ 23 ]  . 
the german de - intensication radiotherapy postoperative head neck ( direkht ) trial ( nct02528955 ) , a non - randomized phase ii trial , aims to explore the outcome of three different de - intensied radiation dose and target volume protocols , including ipsilateral neck radiation only , depending on postoperative t and n stages [ 24 ]  . contralateral neck dissection in the clinically negative neck is not routinely performed by many groups . 
it favors it in case of a contralateral cn0 neck if oral cavity tumors are staged t3 / t4 or approach the midline and if oropharyngeal carcinomas extend to the midline or involve the posterior pharyngeal wall [ 25 ]  . 
management of the involved and noninvolved ipsilateral neck varies widely between different institutions and countries , depending on clinical tumor stage and location as well as locally recommended treatment guidelines [ 13 ]  . in our cohort , the human papillomavirus ( hpv ) association was only tested in 26.4% of patients and an inuence of hpv on prognosis was not seen . in comparison to other studies , the dfs rate in the present study appears lower than in published data ( see table 6 ) , a fact that may be related to patient selection and inclusion of more advanced tumor stages ( especially higher n stages )  . 
some of these recurrences , especially those occurring after many years , may also be secondary malignancies . conclusion in a large cohort of patients with head and neck carcinoma treated with unilateral postoperative irradiation , the incidence of contralateral lymph node metastasis was low . this is not limited to tonsillar cancer or early nodal stages only . 
the unilateral approach is probably the optimal strategy for postoperative radiotherapy of completely resected lateral tumors of the oropharynx , the oral cavity , and also the hypopharynx without clinical evidence of contralateral nodal disease and has to be proven in prospective evaluations . 
however , due to certain characteristics of the tumor itself , such as specic gene mutations or abnormalities in the tumor immune microenvironment , the efcacy of crt varies among individuals [ 24 ]  . 
therefore , how to identify the relevant characteristics in the tumor and immune microenvironment is a prerequisite for achieving individualized neoadjuvant crt [ 1 ]  . the dna damage response ( ddr ) pathway has been found to be closely related to the occurrence , development , and treatment resistance of various tumors [ 5 ]  . 
the protein participates in the repair of dna damage through the interaction with p53 and atm protein , to maintain the stability and integrity of the genome and regulate cell cycle and apoptosis [ 6 ]  . 
our previous studies have also veried the close correlation between 53bp1 466 strahlenther onkol ( 2020 ) 196 : 465473 expression and the radiosensitivity of colorectal cancers , and found that the loss of 53bp1 could inhibit the radiosensitivity of colorectal cancer by inducing cell proliferation and inhibiting apoptosis [ 7 , 8 ]  . 
based on existing research results , 53bp1 could be regarded as a predictive marker for neoadjuvant therapy efcacy , but it still requires further support with clinical evidence . in addition to the tumors own biological characteristics , the tumor response to treatment depends on the density of tumor - inltrating lymphocytes ( til ) in the microenvironment [ 9 , 10 ]  . 
normally , if tumor can be effectively recognized by the host immune system , a variety of effector cells , such as helper cd3 + t cells , memory cd45ro + t cells , and cytotoxic cd8 + t cells , can be activated to prevent tumor development . 
however , tumors themselves can escape the host immune surveillance , leading to a lack of effector t cell inltration into the tumor microenvironment and inducing therapeutic resistance [ 11 ]  . 
numerous clinical studies have shown that t lymphocyte inltration density in the central region of the tumor ( ct ) and the invasion margin ( im ) is positively correlated with clinical outcomes [ 1013 ]  . 
therefore , the current expert consensus has suggested and established an immunoscore approach based on the density of cd3 / cd8 , cd3 / cd45ro , and cd8 / cd45ro tils in the tumor ct and im area to evaluate treatment response and predict prognosis [ 9 , 14 ]  . increasing literature contributions have revealed the interaction between tumor molecular characteristics and immune inltration in the microenvironment . 
similarly , 53bp1 has been found to serve a key role in maintaining t cell function and the loss of 53bp1 could result in the deciency of t cell function [ 15 ]  . 
thus , we speculated that changes in 53bp1 expression and consequent variations of t cell inltration density in the tumor microenvironment may work together to affect radiosensitivity in colorectal cancer . 
the purpose of this study was to evaluate the correlation of pretreatment 53bp1 expression and the immunoscore based on til density in tumor tissues with a neoadjuvant crt response , to explore the internal connection between 53bp1 and t lymphocyte inltration , and determine the role of these two factors on crt response and prognosis in locally advanced rectal cancer . materials and methods research design and patient enrollment this was a retrospective observational study approved by the ethics committee of huazhong university of science and technology , china . 
patients with locally advanced rectal cancer undergoing neoadjuvant crt and total mesorectal excision ( tme ) from january 2015 to february 2018 were enrolled according to the following criteria : ( 1 ) the patients age was in the range of 18 to 75 years ; ( 2 ) the lower end of the patients tumor was less than 10 cm from the anal margin and pathologically conrmed as rectal adenocarcinoma ; ( 3 ) the patient presented with no distant metastasis ( stage ct3 - 4 and / or n + , m0 ) according to the 7th edition of the american joint committee on cancer ( ajcc ) staging system ; ( 4 ) complete pretreatment magnetic resonance imaging ( mri ) data and pretreatment tissue specimens from the patient were available ; ( 5 ) the patient had undergone standard preoperative crt , tme , and followup ; and ( 6 ) complete postoperative data were collected and postoperative tumor regression grade ( trg ) assessments were performed according to the dworak grading system [ 16 ]  . 
the patients clinical characteristics , including age , gender , tumor differentiation status , primary tumor location , stage , and postoperative trg data , etc . , were collected and analyzed . treatment regimen and ecacy evaluation all patients enrolled in the study received a total radiotherapy dose of 4550 gy ( single doses of 1.8 gy or 2 gy ) , which was administered concurrently with intravenous 5 - uorouracil ( 5 - fu ; king york , tianjing , china ) or oral capecitabine ( roche , shanghai , china )  . 
in all cases , baseline and postradiotherapy efcacy assessments were performed according to the response evaluation criteria in solid tumors ( recist 1.1 ) , and postoperative specimens were used to assess the trg according to the dworak system [ 16 ]  . immunohistochemical analysis the pretreatment 53bp1 expression and cd3 + , cd8 + , and cd45ro + t cell density in tumor tissue were analyzed via immunohistochemistry . 
according to a previous study [ 17 ] , parafn sections were pretreated and incubated with primary anti - cd3 ( abcam , cambridge , ma , usa , ab16669 , 1 : 150 ) , anti - cd8 ( abcam , ab4055 , 1 : 150 ) , anticd45ro ( abcam , ab216024 , 1 : 300 ) , or anti - 53bp1 ( abcam , ab175933 , 1 : 300 ) antibody . 
the expression of 53bp1 localizes to the nucleus of the tumor cells , while cd3 , cd8 , and cd45ro are membrane proteins of immune cells [ 6 , 7 ]  . 
two independent pathologists assessed the data in a single - blind fashion . strahlenther onkol ( 2020 ) 196 : 465473 table 1 patient clinical characteristics and response to neoadjuvant clinical characteristic response ( n = 34 ; % ) nonresponse ( n = 21 ; % ) p - value scoring of the immune status of the central and marginal tumor regions recently , a tumor immunoscore approach was proposed based on the numeration of any two populations of tils in the ct and im of the tumor , such as cd3 / cd8 , cd3 / cd45ro , or cd8 / cd45ro [ 9 ]  . 
the sum scores of the cd3 / cd8 , cd3 / cd45ro , and cd8 / cd45ro in the ct and im regions were calculated as a total score of 04 : a score of 02 was considered a low immunoscore and a score of 34 was considered a high immunoscore . statistical analysis data were analyzed using spss 17.0 statistical software ( ibm , armonk , ny , usa )  . 
the area under the receiver operating characteristic ( roc ) curve ( auc ) and logistic regression analysis were used to evaluate the value of the 53bp1 expression level and immunoscore for predicting the response to crt , and the corresponding sensitivity , specicity , accuracy , and optimal cutoff values were determined . 
the kaplanmeier method and cox regression analysis were employed to determine differences in disease - free survival ( dfs ) and overall survival ( os ) , and the factors inuencing survival between the two groups . 
lymphocyte inltration level was positively correlated with 53bp1 expression : low 53bp1 expression was accompanied by decreased cd45ro + , cd3 + , cd8 + til density and decreased all three kinds of immunoscore . 
among the three kinds of immunoscore , the cd3 / cd8 immunoscore showed the strongest correlation with the 53bp1 expression level ( p < 0.05 ; supplementary table 1 )  . pretreatment 53bp1 expression level and cd3 / cd8 immunoscore enabled eective prediction of response to neoadjuvant therapy because the pretreatment 53bp1 expression level and cd3 / cd8 immunoscore were closely related to the refig . 
the pretreatment expression of cd3 , cd8 , and cd45ro was evaluated in ct and im area by immunohistochemistry , as 1 point for high expression and 0 points for low expression for each marker . 
the scores of cd3 / cd8 , cd3 / cd45ro , and cd8 / cd45ro in two regions were summarized as 04 points , among which 02 points for lower immune group , 34 points for a high immune score group strahlenther onkol ( 2020 ) 196 : 465473 fig . 
after the median follow - up time of 29 months ( ranging from 3 to 48 months ) , four patients developed local recurrence and nine patients had distant organ metastases during follow - up . 
different degrees of 53bp1 deletions have been found during the occurrence and development of multiple tumors , which are closely 470 strahlenther onkol ( 2020 ) 196 : 465473 fig . 
the expression of 53bp1 was signicantly correlated with the treatment response rate . the 53bp1 high expression group showed a high response rate , while the low expression group showed a signicant decrease in the response to crt treatment ; this outcome is consistent with our previous studies and suggests that 53bp1 is an effective biomarker for predicting the efcacy of colorectal cancer crt [ 7 , 8 ]  . in addition to some genetic abnormalities , immunoscore based on the density of cd3 / cd8 , cd3 / cd45ro , and cd8 / cd45ro cells in the ct and im regions has been recognized as another important biomarker for prognosis [ 14 , 1820 ]  . 
a series of clinical trials have conrmed close connections of immunoscore with clinical outcomes , as low immunoscore ( i0 - 2 ) was always accompanied by poor therapeutic effects , while high immunoscore ( i3 - 4 ) was often associated with better therapeutic effects [ 9 , 19 ]  . 
based on the consideration that most previous studies only focused on the inuence of til level on chemotherapy efcacyignoring radiotherapyor emphasized the role of cd3 / cd8 score in therapeutic efcacyignoring the role of cd45ro + t cells in immunoscore [ 14 , 21 ] we evaluated in detail the relationship between the three scores and therapeutic efcacy . 
our results revealed the til level in the tumor area was positively correlated with the therapeutic efcacy , and the cd3 / cd8 score demonstrated the greatest relevance to the trg , with an auc for predicting the response to crt of 0.717 among the three immunoscores . this result is consistent with the expert consensus regarding the cd3 / cd8 score as the most suitable for clinical application . mounting evidence from recent studies has revealed the intimate intrinsic correlation between the immune microenvironment and the dna damage repair pathway in tumor [ 5 , 2224 ]  . 
some gene mutations or deletions in the ddr pathway , such as the breast cancer susceptibility gene 1 ( brca1 ) and ku70 / ku80 , have been found to induce tumor cells upregulating the expression of programmed death - ligand 1 ( pd - l1 ) , which can effectively inhibit the activity of tils in the tumor immune microenvironment , such as cd8 cells , and then lead to tumor escape [ 25 ]  . 
our previous study has conrmed the close relationship among the 53bp1 expression , tumor radiosensitivity , and proliferation , as that the loss of 53bp1 could signicantly enhance the proliferation of tumors and lead to radiation resistance . 
some studies have shown that 53bp1 also plays an important role in the normal development of the immune system , participating in the development and normal functioning of t lymphocytes . 
therefore , we speculated that 53bp1 loss could decrease colorectal cancers radiosensitivity not only by enhancing tumor proliferation , also by inuencing the immune status of the host . 472 strahlenther onkol ( 2020 ) 196 : 465473 thus , we explored the relationship between t cell inltration density and 53bp1 expression in tumor tissues . 
the results show that high 53bp1 expression is always accompanied by extensive t cell inltration , while low 53bp1 expression is accompanied by a lack of t cell inltration in tissues . 
further survival analysis revealed that although the role of 53bp1 in dfs was not affected by the immunoscore , the role of the immunoscore in prognosis was affected by the level of 53bp1 expression ; when cd3 / cd8 immunoscore was ( cid : 2 ) 2 , the dfs duration of patients with low 53bp1 expression was obviously shorter than that of patients with high 53bp1 expression . 
these results all suggest a potential synergistic effect between 53bp1 expression and host immune function , but the exact mechanisms still need to be explored in the future . taken together , in this study , we conrmed that pretreatment 53bp1 expression and cd3 / cd8 immunoscore in tumor tissue could effectively predict crt efcacy , and the level of 53bp1 expression was closely related to the extent of t cell inltration in the tumor microenvironment . 
ma declare that they have no competing interests . ethical standards this study was a retrospective observational study approved by the ethics committee of huazhong university of science and technology , china . 
however , mr images acquired for routine radiological assessment are frequently unsuitable for high - precision stereotactic radiotherapy as the requirements for imaging are signicantly different for radiotherapy planning and diagnostic radiology . 
to assure that optimal imaging is used for treatment planning , the radiation oncologist needs proper knowledge of the most important requirements concerning the use of mri in brain stereotactic radiotherapy . 
in the present review , we summarize and discuss the most relevant issues when using mr images for target volume delineation in intracranial stereotactic radiotherapy . keywords radiosurgery distortion correction local control radiotherapy simulation radiotherapy treatment planning magnetresonanztomographie fr die stereotaktische strahlentherapie des gehirns anforderungen und fehlerquellen eine bersicht the authors f . 
it is because of this long - standing history and the fact that nowadays mri is used in nearly every patient with an intracranial tumor , that the radio - oncologist as a result of a false sense of security stemming from the perceived familiarity with its use may be unaware of the potential dangers and pitfalls associated with using mri in an indiscriminate way in daily clinical practice . 
note also : substantial increase in perifocal edema ( inset : t2 - flair ) in mr images are a good example of a source of treatment error that overshadowed the introduction of mri in radiotherapy [ 24 ] but may still endanger treatment success in high - precision stereotactic radiosurgery of brain metastases today [ 5 , 6 ]  . 
the main reason why some of the perils associated with mri - based radiotherapy treatment planning have still not completely disappeared may be the fact that mri for the most part has been outside the scope of the radio - oncologist . 
while the planning ct is usually located in the radiotherapy treatment facility and is optimized for the requirements of radiotherapy , mri studies for radiotherapy treatment planning are frequently performed in external departments . 
however , the diagnostic radiologist who acquires these mr studies may be less familiar with the specic requirements of radiotherapy treatment planning , as the requirements on imaging for radiotherapy and diagnostic radiology are signicantly different . 
therefore , the radiation oncologist needs proper knowledge of the most important caveats and considerations concerning the use of mri in brain stereotactic radiotherapy . for stereotactic radiotherapy very high and specic technological quality requirements are needed to assure highly precise treatment delivery . 
optimal mr imaging is a crucial element for high overall accuracy in stereotactic radiotherapy and ultimately a necessity for treatment success but is frequently overshadowed by the technological requirements that are more closely related to treatment delivery . 
in light of commonly used gross target volume ( gtv ) to planning target volume ( ptv ) margins of ( cid : 2 ) 1 mm , the requirements for mr imaging are particularly demanding in intracranial stereotactic radiotherapy [ 9 , 10 ]  . accompanying the very important ofcial articles of the degro and dgmp working groups , in the present review , we therefore highlight the important role of optimal mr imaging by summarizing and discussing the most relevant issues arising when using mri in treatment planning for brain stereotactic radiotherapy . time between mr imaging and treatment delivery one of the most crucial parameters for treatment precision is the interval between mr imaging and treatment delivery [ 11 , 12 ]  . 
interestingly , changes were less pronounced for postoperative cases ( up to 4.5% in ptv coverage ) and pretreatment changes were predictive of reduced coverage during treatment [ 17 ]  . 
importantly , as 446 strahlenther onkol ( 2020 ) 196 : 444456 aside from avoiding slight infratentorial tissue deformation , the accuracy of rigid registration may also improve when acquiring the simulation mri in the treatment position [ 6 , 21 ]  . 
in general , uncertainties of ( cid : 2 ) 0.5 mm along the xand y - axis in - plane and of ( cid : 2 ) 1 mm along the z - axis have been reported for normalized - mutual - information based mrict coregistration for a ct slice thickness of 23 mm and a 1 1 2 mm3 3d - t1 - mprage sequence . importantly , when using a ct slice thickness of 5 mm and a 1 1 5 mm3 2d - se sequence the registration uncertainty rose by a factor of 23 [ 22 ]  . 
according to the current consensus imaging with mask immobilization as well as imaging in a routine radiologic setup are both appropriate strategies for mr simulation in intracranial radiotherapy if mr images are registered to a planning ct [ 6 ]  . promises of synthetic ct and mr - only planning synthetic ct , which is the calculation of synthetic ct images from one or multiple mr sequences , promises to remove the need for an additional planning ct and thus any uncertainties with mrct registration [ 26 ]  . 
while eliminating registration uncertainties , the use of synthetic ct may potentially introduce errors into treatment planning , due to bulk assignment of ct numbers to segmented tissues and in some algorithms the use of atlases to generate major bones [ 26 ]  . 
note : substantial reduction in tumor volume and in accompanying edema results in profound shifting of the brainstethe radiotherapy plan was adapted based on the repeated planning mri only 35 fractions were employed in the study by hessen et al . , even more pronounced changes would be expected with more prolonged fractionation schemes . 
at our university medical center in erlangen we usually repeat imaging during prolonged courses of stereotactic treatment of brain metastases or primary brain tumors at least once , especially when risk factors like large edema , hygroma and other similar pathologies are present . patient positioning for simulation mri the simulation mri for intracranial radiotherapy is most frequently acquired in a diagnostic head coil and subsequently rigidly coregistered to the planning ct obtained in the treatment position with immobilization . 
however , acquiring the simulation mri in the treatment position using an immobilization mask similar to the planning ct could decrease errors due to nonrigid tissue deformation , reduce uncertainties related to image registration , reduce motion artifacts and may even serve as the basis for an mr - only workow using synthetic ct . deformation and displacement of brain tissues in different imaging positions is certainly more limited than deformation of organs at most extracranial sites [ 6 , 18 ]  . 
the head is substantially exed in the diagnostic head coil ( amber ) compared to the simulation mri with mask immobilization ( blue ) leading to slight displacement of infratentorial structures ( b , c , white arrows )  . 
d , e reduced motion artifacts in the stereotactic mask system ( d ) compared to the diagnostic head coil ( e ) are at the forefront of current research on synthetic ct and have been shown to outperform other published approaches in terms of mean absolute hu errors in a recent study [ 28 ]  . these solutions could allow for fast and robust synthetic ct generation from standard mr sequences . as mrct registration has been shown to reduce positional errors introduced by mri , minimization of mr distortions becomes even more relevant , when opting for an mr - only workow [ 29 ]  . accounting for distortions in mr images while ct scans can be considered geometrically accurate , several mechanisms may lead to distortions in mr images that endanger precise treatment delivery [ 2 , 3 , 30 , 31 ]  . slight distortions on the order of 12 mm are nearly impossible to identify in mr images , even when coregistering to a planning ct . 
in clinical practice most distortions will therefore be expected to occur at the periph448 strahlenther onkol ( 2020 ) 196 : 444456 3d distortion corrected 2d distortion corrected no correction fig . 
note : while the difference between 2dand 3d - correction is more subtle , the 2d - corrected dataset underestimates the lower border of the tumor ( white arrows )  . 
blue indicates no displacement , red indicates a displacement of 2 mwhile 2d - corrected images ( g ) show fewer residual distortions than uncorrected images ( h ) , distortions of up to 2 mm were still present after 2d - correction . 
additional sources of distortion include magnet imperfections and patient - induced susceptibility - related distortions , which are not visualized here ery of the brain especially near airbone interfaces , which translates among others to the frontopolar and orbitofrontal cortex but also to cranial aspects of the prefrontal cortex and to lateral and inferior parts of the temporal lobe . importantly , distortions in mr images can be substantially reduced when selecting the appropriate settings at the mr scanner . 
however , the diagnostic radiologist , who frequently is the one who obtains the mr images used for treatment planning , may be virtually unaware of the problems associated with distortion - related imaging errors in radiotherapy planning as distortion is far less of a problem in diagnostic radiology . 
in the following section we therefore want to discuss the most important types of distortion in mr images and how they can be minimized . distortions most relevant to mri - based intracranial radiotherapy are those due to nonlinearities of the gradient coils and those due to inhomogeneities in the main magnetic eld ( b0 ) [ 35 ]  . 
these three most relevant types of distortion are usually grouped into system - related ( gradient nonlinearity - related distortions and main magnet imperfections ) and patient - induced ( susceptibility effect - instrahlenther onkol ( 2020 ) 196 : 444456 duced distortions ) but a more practical approach is to differentiate between sequence - independent ( gradient nonlinearity - related distortions ) and sequence - dependent distortions ( inhomogeneities of the static magnetic eld due to magnet imperfections or due to patient - induced perturbations ) [ 24 , 31 , 35 ]  . sequence - independent gradient nonlinearityrelated distortions in mri , three gradient coils superimpose magnetic eld gradients onto the main magnetic eld in the x , y and z dimensions . 
distortions due to gradient nonlinearities therefore do not change with different sequence settings but will differ when using different scanner models [ 2 , 24 , 3032 , 38 ]  . 
however , image distortions due to gradient nonlinearities may change for the same scanner when the patient is positioned differently relative to the gradient elds [ 24 , 32 ]  . 
in fact , vendor - specic 3d distortion correction was regarded as a minimum requirement in a 2016 consensus paper on mri simulation published in radiotherapy and oncology with additional corrections required based on onsite measurements [ 6 ]  . 
importantly , while vendor - specic 3d correction should be the minimum for radiotherapy planning , in our experience most mri sequences acquired in external departments are only 2d corrected . 
as stated therefore in the 2016 consensus paper by paulson et al . , residual distortion after vendor - specic correction should be characterized using phantoms and corrected if necessary [ 6 ]  . multiple authors have described rectifying residual gradient nonlinearity distortions using 3d deformation vector elds obtained via phantom measurements [ 30 , 37 , 41 ]  . sequence - dependent distortions distortion correction via postprocessing congured at the scanner can however not correct distortions because of magnet imperfections or tissue susceptibility [ 2 , 38 ]  . 
also , while gradient nonlinearity - related displacements occur in all three dimensions , b0 inhomogeneity - related distortions in regular 3dsequences only occur in the frequency - encoding dimension . as the slice selection process in 2d - sequences is also disturbed by b0 inhomogeneities , 2d - sequences are more susceptible to b0 inhomogeneity - related distortions than 3d450 strahlenther onkol ( 2020 ) 196 : 444456 sequences [ 2 , 30 , 42 ]  . 
displacements increase at 3 t in comparison to 1.5 t in the absence of other compensating factors [ 2 , 43 ]  . patient - induced perturbations of the main magnetic eld occur because of differences in magnetic susceptibility , which is the physical property of material becoming magnetized inside an external magnetic eld [ 2 , 35 , 44 ]  . 
the greatest susceptibility differences and therefore the most severe distortions occur at airbone interfaces [ 35 , 44 ]  . in the case of intracranial radiotherapy , the most severe susceptibility - related distortions are therefore to be expected near the paranasal sinuses and the mastoid cells [ 42 ]  . 
however , while average displacement was low for the whole imaged volume , average distortions at sinus airbone boundaries was 1.6 mwhile degrading with distance , these distortions extended into the adjacent brain and optic system and still measured 0.8 mm at a distance of 12 mm , which is clinically relevant for rt targets in parts of the brain adjacent to the sinuses and mastoid cells [ 42 ]  . in addition , large susceptibility differences and consecutive distortions may also occur at the site of metallic implants like surgical clips [ 42 ]  . while vendor - specic distortion correction does not correct for distortions due to b0 inhomogeneities , they can be ameliorated with increasing readout bandwidth , using 3dinstead of 2d - sequences [ 45 ] and activating patient - specic active shimming . increasing readout bandwidth , decreases all distortions due to b0 inhomogeneities in a reciprocal fashion [ 35 , 42 , 46 , 47 ]  . 
the downside , however , is that the signal - to - noise ratio ( snr ) also has an inverse relationship to the squareroot of the readout bandwidth [ 47 ]  . 
however , in stark contrast to the preferential settings for routine radiological imaging , mri for radiotherapy planning requires higher bandwidths to reduce distortions from b0 inhomogeneities [ 13 ]  . 
snr loss due to higher bandwidth can be compensated for with strategies that increase snr like increasing measurement time , optimized coil selection and decreased motion artifacts due to immobilization . 
b0 inhomogeneities are rst measured using a patient - based but fast and low - resolution phase difference mapping technique and subsequently reduced with the shim coils [ 42 , 48 ]  . 
however , patient - specic active shimming needs to be available at the scanner and properly congured . if patient - specic active shimming and rt - optimized bandwidth settings are not completely successful in reducing b0 inhomogeneity - related distortions to an acceptable level , additional correction is possible by obtaining an improved higher resolution phase difference map which can be used to correct patient - specic b0 distortion via image postprocessing [ 31 , 49 ]  . 
a reverse gradient method has also been proposed to correct b0 inhomogeneity - related distortions but requires obtaining every sequence two - fold and may lead to degraded image quality in most clinical settings [ 31 , 36 , 50 , 51 ]  . an additional source of patient - related distortions is the chemical shift , with the fatwater shift being the most prominent example . 
this effect is however also minimized by choosing higher bandwidths [ 52 ]  . current consensus denes that total distortions in mri need to be less than 1 mm for stereotactic radiotherapy in the brain [ 6 ]  . 
enabling vendor - specic 3d distortion correction and patient - specic active shimming in the scanner software as well as selecting rt - optimized readout bandwidths before acquisition of the planning mri are steps which are easy to implement and may sufciently eliminate distortions in many cases . it is however important to verify that the geometric accuracy required for brain stereotactic radiotherapy ( < 1 mm ) is indeed achieved by measuring residual distortions . 
in addition 3dsequences are also less susceptible to b0 inhomogeneityrelated distortions than 2d - sequences and image the brain continuously without gaps . it has been shown that the volumetric error will exceed 10% if the gtv is visualized on less than 5 slices , which is particularly relevant for small brain metastases [ 54 ]  . 
a , b impact of slice thickness on gtv size : a 1 mm slice thickness ; b 3 mm slice thickness . coronal reconstruction with axial reconstruction ( inset )  . 
conventional 2d t2 - flair ( 5 mm slice thicknessc ) in a patient with glioma . e visualization of slice gaps present in a routine 2d t1 - tse sequence . 
t1 - space ( t1 3d - tse ) for delineation of brain metastases inversion - recovery gradient echo sequences ( ir - gre ) like the t1 - mprage [ 55 ] have been the most commonly used 3d mr imaging technique for brain tumors and have been included in the standardized brain tumor imaging protocol ( btip ) [ 56 , 57 ]  . 
however , multiple sources suggest that a 3d - turbo - spin - echo ( tse ) t1 - space could be superior to the frequently used t1 - mprage gradient - echo sequence for intracranial radiotherapy target volume delineation [ 56 , 5860 ]  . 
while t1 - space provides less contrast between grey and white matter [ 56 ] , this is negligible in most cases for radiotherapy treatment planning and may in fact even help with the delineation of intracranial metastases , as does the suppression of vessels in the t1 - space [ 60 ]  . 
published in the american journal of neuroradiology , the authors systemstrahlenther onkol ( 2020 ) 196 : 444456 atically compared t1 - mprage , t1 - space and t1 - vibe in 16 brain metastases and 38 gliomas [ 56 ]  . 
gtv denitions based on the t1 - mprage missed a median contrast - enhancing volume of 0.27 cm3 visualized in the t1 - space in 19.9% of cases , whereas only a median contrast - enhancing volume of 0.10 cm3 visualized in the t1 - mprage was missed in 7.4% of cases by the t1space in the reciprocal comparison . 
importantly , the authors addressed the potential impact of different contrast phases by randomizing the order of sequences in each patient and by accounting for the order of acquisition in their analysis [ 56 ]  . 
in metastases < 5 mm , 40.6% of lesions were visualized after 10 min , whereas 75.0% could be seen after 20 min . the remaining lesions were only visualized after an additional bolus of double - dose gadoteridol , indicating the value of increased doses of gbca [ 62 ]  . 
reported similar ndings and found more brain metastases at 15 min after gbca administration as compared to 5 mimportantly , they also found an increase in metastasis volume with imaging at 10 vs . 
for example in a 2013 literature review by anzalone et al . , gadobutrol ( gadovist ) was superior to other gbcas in terms of the number of metastases detected and improved lesion visualization [ 53 ]  . summary mr imaging for radiotherapy treatment planning is an integral part of the radiotherapy planning process whose critical nature for precise treatment delivery is easily overlooked . 
at the same time the potential for clinically relevant errors is substantial when using mr images that have not been optimized for the specic requirements of stereotactic radiotherapy . it is important to assure that suitable mr images are used for treatment planning . 
the most important topics that need to be addressed when using mri in brain stereotactic radiotherapy include the acquisition of distortion - free images , the minimization of the time interval between imaging and treatment delivery and the use of rt - optimized 3d - sequences . acknowledgements we want to thank oliver lenhart , melanie habatsch , matthias drobnitzky and martin requardt ( siemens healthineers ) for their highly valuable assistance during the implementation of a dedicated mri scanner for radiotherapy treatment planning in the imaging science institute ( isi ) erlangen . 
staff from siemens healthineers had no inuence on the decision to publish this manuscript and did not request to make changes to the overall content of the manuscript or its scientic statements . funding open access funding provided by projekt deal . compliance with ethical guidelines conict of interest a dedicated mri scanner for radiotherapy treatment planning was implemented in the imaging science institute erlangen in cooperation of the department of radiotherapy and institute of radiology of the university medical center erlangen and siemens healthineers . 
personnel from siemens healthineers who were clinically , scientically and 454 strahlenther onkol ( 2020 ) 196 : 444456 conceptually involved in implementing the dedicated mri scanner for radiotherapy treatment planning contributed to the manuscript draft but did not request to make changes to the overall content of the manuscript or its scientic statements . 
all studies performed were in accordance with the ethical standards indicated in each case . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
mrz 2020 der / die autor ( en ) 2020 hintergrund die beeintrchtigung des schluckens und der salivation nach einer multimodalen therapie von patienten mit kopf - hals - tumoren ist fraglos gravierend . 
gemeint sind nichtrauchende patienten mit einem hpv - assoziierten oropharynxkarzinoverschiedene strategien werden derzeit parallel untersucht , beispielsweise geringere dosen in der postoperativen und denitiven situation , der gnzliche verzicht auf eine postoperative bestrahlung oder die substitution von cisplatin bei der chemotherapie . patienten und methode gleich mehrere stellschrauben wurden bei einer postoperativen radiochemotherapie ( rct ) innerhalb einer phase - ii - studie gelockert , die an zwei mayo - kliniken durchgefhrt wurde [ 1 ]  . 
patienten , deren lymphknotenmetastasen sich bereits extranodal ausgebreitet hatten , erhielten zweimal tglich 1 , 8 gy als simultan integrierten boost ( sib ) originalpublikation ma dj , price ka , moore ej et al ( 2019 ) phase ii evaluation of aggressive dose - deescalation for adjuvant chemoradiotherapy in human papillomavirus - associated oropharynx squamous cell carcinoma . 
sonst umfasste das 30 gy - ctv bei smtlichen patienten das tumorbett und ausschlielich die ipsilateralen lymphknoten der level ii bis iv mit optionaler erweiterung auf level ib , v und die retropharyngealen lymphknotenstationen . 
mutmalich war die therapie so konzipiert , dass im falle eines rezidivs noch eine voll dosierte salvage - rct durchzufhren war . ergebnisse in den zwei kohorten mit 36 patienten ohne extrakapsulren lymphknotenbefall ( 30 gy ) und 43 patienten mit extrakapsulrer tumorbeteiligung ( 36 gy als sib ) , die im mittel eine dosis von 24 , 8 gy an den mconstrictores und 17 , 8 gy an den glandulae parotideae erhalten hatten , entwickelten erwartungsgem nur wenige patienten eine grad - 3 - toxizitt inform einer enoralen mukositis oder pharyngitis , und dies trotz hyperfraktionierter und akzelerierter bestrahlung . 
alle items der lebensqualitt erreichten das prradiotherapeutische niveau oder verbesserten sich noch darber hinaus . schlussfolgerung der autoren im vergleich zu historischen kontrollen konnten die beschriebenen manahmen der therapiedeeskalation eine deutlich bessere lebensqualitt erhalten , ohne dass einschrnkungen in der tumorkontrolle bemerkt wurden . strahlenther onkol ( 2020 ) 196 : 492494 kommentar die behandlungsergebnisse aus den zwei mayo - kliniken klingen verlockend , bei einem patienten mit einem hpvpositiven oropharynxkarzinom zunchst eine tumortonsillektomie vorzunehmen , dann mit einem reduzierten volumen und einer reduzierten dosis zu bestrahlen und simultan dazu mit einer atoxischen chemotherapie zu behandeln . 
patienten mit tumoren , die in selbiger sitzung nachreseziert werden mussten , was in der breiten routineversorgung ja der alltag ist , oder t4tumoren entwickelten rezidivraten in 15 % der flle und eignen sich somit selbst nach r0 - resektion nicht . 
zudem muss betont werden , dass es sich um eine studie an lediglich 80 patienten handelt , bei der es darauf ankam , einen ersten eindruck von der rezidivhugkeit und vorrangig der zu erwartenden lebensqualitt zu erhalten . 
die gruppe von 43 patienten mit extranodalem tumorwachstum ist dann doch recht klein , sodass auf einen kontrollierten vergleich mit der standardtherapie an einer greren patientenzahl nicht verzichtet werden darf . erinnert sei nur an die tatsache , dass bei einer denitiven radiochemotherapie der ersatz von cisplatin durch cetuximab beim hpv - assoziierten oropharynxkarzinom entgegen aller erwartung zu einer um 7 % schlechteren lokoregionren kontrolle nach 5 jahren und zu einem 6 % und 8 % schlechteren gesamtberleben nach 2 bzw . 
5 jahren fhrte [ 3 , 4 ]  . etwas ist aber anders bei dieser initial stark gedrosselten postoperativen therapiedichte im vergleich mit einer denitiven rct und damit sehr interessant . 
letztlich wird es doch darum gehen , ob sich das therapiekonzept der gedrosselten initialtherapie mit inkaufnahme einer hheren lokalrezidivrate und der option einer rettungstherapie zugunsten einer deutlich verbesserten lebensqualitt in der praxis durchsetzen kann . 
semrau geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
ma dj , price ka , moore ej et al ( 2019 ) phase ii evaluation of aggressive dose de - escalation for adjuvant chemoradiotherapy in hu494 strahlenther onkol ( 2020 ) 196 : 492494 man papillomavirus - associated oropharynx squamous cell carcinoma . 
gillison ml , trotti am , harris j et al ( 2019 ) radiotherapy plus cetuximab or cisplatin in human papillomavirus - positive oropharyngeal cancer ( nrg oncology rtog 1016 ) : a randomised , multicentre , non - inferiority trial . 
mehanna h , robinson m , hartley a et al ( 2019 ) radiotherapy plus cisplatinorcetuximab in low - risk human papillomavirus - positive oropharyngealcancer ( de - escalate hpv ) : an open - label randomisedcontrolledphase 3 trial . 
nichols ac , theurer j , prisman e et al ( 2019 ) radiotherapy versus transoral roboticsurgeryand neck dissectionfororopharyngealsquamouscellcarcinoma ( orator ) : an open - label , phase 2 , randomisedtrial . 
mrz 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund es gibt hinweise , die einen negativen einuss einer antibiotischen therapie auf die wirksamkeit von immuncheckpoint - inhibitoren durch vernderung des mikrobioms im darm nahelegen . 
daher sollten in dieser studie die auswirkungen einer vorherigen oder zeitgleichen antibiotischen therapie auf das gesamtberleben sowie das therapieansprechen bei krebspatienten unter immuncheckpoint - inhibitoren untersucht werden . methoden in eine prospektive kohortenstudie wurden 196 patienten ( 137 mnner und 59 frauen ; mittleres alter 68 [ 2793 ] ) aus zwei klinischen zentren im zeitraum von januar 2015 bis januar 2018 eingeschlossen . 
untersucht wurden das gesamtberleben sowie das radiologische therapieansprechen in abhngigkeit von einer antibiotischen therapie vor oder whrend der immuntherapie . ergebnisse die auswertungen zeigen , dass die 29 patienten , die innerhalb von 30 tagen vor beginn der behandlung mit immuncheckpoint - inhibitoren eine antibiotische therapie erhielten ( patb ) , ein schlechteres gesamtberleben ( os ) aufwiesen ( hr : 7 , 4 ; 95 % - ki : 4 , 312 , 8 ; p < 0 , 001 )  . 
1 , 90419 nrnberg , deutschland te dauernden immuntherapie ( catp ) bei 68 patienten fhrte dagegen zu keiner signikanten verschlechterung ( hr : 0 , 9 ; 95 % - ki : 0 , 51 , 4 ; p < 0 , 65 )  . 
dennoch ist das therastrahlenther onkol ( 2020 ) 196 : 486487 pieansprechen individuell sehr unterschiedlich ; die ursachen hierfr sind bisher nicht ausreichend geklrt . im tumorgewebe nden sich neben den krebszellen zahlreiche krpereigene immunzellen , die verschiedene sogenannte checkpoint - molekle wie pd - 1 und ctla - 4 auf ihrer oberche exprimieren . 
voraussetzung fr den erfolg der therapie ist somit das vorhandensein von funktionellen t - zellen , die ihre effektorfunktionen wahrnehmen knnen . der einuss auf das immunsystem durch das gastrointestinale mikrobiom , also die gesamtheit aller in und auf der darmschleimhaut lebenden mikroorganismen , wurde lange unterschtzt . 
dadurch konnten bereits diverse einsse des mikrobioms auf das angeborene und das adaptive immunsystem belegt werden : bei keimfrei gehaltenen musen wurden eine reduzierte anzahl an granulozyten und eine erhhte rate an schweren infekten gezeigt [ 1 ]  . 
weiterhin hat das mikrobiom im darm einuss auf sowohl immunsteigernde als auch immunhemmende t - zellen , wodurch eine homostase entsteht [ 2 ]  . das mikrobiom bildet sich bereits in den ersten lebensjahren aus und hngt von faktoren wie genetik , umwelteinssen und ernhrung ab . 
die einnahme von antibiotika verndert das mikrobiom jedoch signikant [ 4 ]  . die wiederherstellung des mikrobioms nach der behandlung kann bis zu sechs monate in anspruch nehmen . hinsichtlich des ansprechens auf eine tumorspezische therapie gibt es hinweise auf den einuss eines vernderten mikrobioms . 
im mausmodell und beim menschen hatten sich bereits der positive einuss eines intakten mikrobioms und der nachteilige effekt einer antibiotischen therapie auf den effekt einer immuncheckpoint - inhibition gezeigt [ 6 , 7 ]  . fazit das ergebnis der hier vorliegenden studie entspricht den erwartungen , dass eine vorherige antibiotische therapie das therapieansprechen auf immuncheckpoint - inhibitoren reduziert . 
auch hatte die gleichzeitige gabe mit den immuncheckpoint - inhibitoren keinen einuss . limitiert wird die aussagekraft der studie durch die relativ kleine patientenzahl und dadurch , dass die korrelation zwischen nachgewiesener vernderung des mikrobioms und dem ansprechen auf die therapie nicht untersucht wurde . 
da dies nicht immer mglich ist , knnte in zuknftigen studien untersucht werden , ob nach einer antibiotischen therapie vor beginn einer therapie mit immuncheckpoint - inhibitoren eine fkale mikrobiomtransplantation das therapieansprechen verbessern kann , wie es bereits in experimentellen anstzen durchgefhrt wird [ 8 ]  . anna bauerei und martin wilhelm , nrnberg interessenkonikt a . 
dethlefsen l , huse s , sogin m et al ( 2008 ) the pervasive effects of an antibiotic on the human gut microbiota , as revealed by deep 16s rrna sequencing . 
viaud s , saccheri f , mignot g et al ( 2013 ) the intestinal microbiota modulates the anticancer immune effects of cyclophosphamide . science 342 ( 6161 ) : 971976 6 . 
mrz 2020 der / die autor ( en ) 2020 hintergrund die kombinierte therapiemodalitt ( cmt ) mit 2 zyklen abvd ( adriamycin [ doxorubicin ] , bleomycin , vinblastin und dacarbazin ) und mit konsolidierender involved - eld - radiotherapie ( if - rt ) stellt den aktuellen therapiestandard des hodgkin - lymphoms im frhen gnstigen stadium dar . 
eine positronenemissionstomographie nach 2 zyklen abvd ( interim - pet , pet - 2 ) knnte helfen , individuell das therapieergebnis vorherzusagen und damit einen risikoadaptierten behandlungsweg zu ermglichen . patienten und methoden zwischen november 2009 und dezember 2015 wurden patienten im alter von 18 bis 75 jahren mit einem neu diagnostizierten hodgkin - lymphom im frhen gnstigen stadium ( ohne risikofaktoren ) fr die hier diskutierte , internationale , randomisierte phase - iii - studie rekrutiert . 
die patienten erhielten entweder den therapiestandard mit 2 abvd und 20 gy if - rt ( cmt ) oder es wurde eine positronenemissionstomographie ( pet ) gesttzte behandlung durchgefhrt , bei der bei negativer pet - 2 auf die if - rt verzichtet wurde . originalpublikation fuchs m , goergen h , kobe c , kuhnert g , lohri a et al ( 2019 ) positron emission tomography - guided treatment in early - stage favorable hodgkin lymphoma : final results of the international , randomized phase iii hd16 trial by the german hodgkin study group . 
das gesamtberleben nach 5 jahren ( os ) unterschied sich hingegen nicht signikant ( cmt 98 , 1 % und alleinige systemtherapie 98 , 4 % , p = 0 , 12 )  . 
zum ziel 2 : 693 patienten erhielten insgesamt die cmt , und das 5 - jahres - pfs betrug fr pet - 2 - negative patienten 93 , 2 % und fr die pet - 2positiven patienten 88 , 4 % ( p = 0 , 047 )  . schlussfolgerung der autoren das erste studienziel wurde nicht erreicht : auf eine if - rt kann also auch bei pet2 - negativen patienten nicht verzichtet werden . 
ein pet - 2 - positiver befund nach 2 abvd ging mit einem erhhten risiko fr eine progression des lymphoms einher . kommentar die hd16 - studie [ 1 ] ist eine folgestudie , welche die optimale therapeutische strategie im frhen gnstigen stadium des hodgkin - lymphoms ( ohne risikofaktoren ) weiter untersuchte . 
eine verringerung der rezidive wurde durch den einsatz der cmt [ 5 ] erreicht , und so war in der hd7 - studie [ 3 ] die cmt ( 2 abvd + 30 gy efrt + 10 gy if - rt ) der alleinigen strahlentherapie ( 30 gy ef - rt + 10 gy if - rt ) berlegen . 
der verzicht auf bleomycin verminderte die toxizitt , ging aber mit einem schlechteren onkologischen ergebnis einher , sodass das abvd - schema unverndert appliziert werden sollte . einen anderen ansatz , die rate an therapiebedingten spttoxizitten zu reduzieren , verfolgte der verzicht auf die konsolidierende radiotherapie . 
eine pet / ct hat eine hhere sensitivitt fr resttumor im vergleich zur computertomographie ( ct ; [ 9 ] ) und kann das stadium des lymphoms verndern [ 10 ] , weshalb z . 
die hd15 [ 15 ] und hd18 - studien [ 16 ] bei fortgeschrittenen hodgkin - erkrankungen zeigten jedoch , dass bei pet - negativen patienten auf die radiotherapie verzichtet werden kann . 
es wurden deshalb drei prospektive , randomisierte studien mit der fragestellung durchgefhrt , ob im falle einer metabolischen komplettremission in der pet nach systemtherapie auf die konsolidierende radiotherapie verzichtet werden kann . die internationale hd16 - studie der ghsg [ 1 ] verglich die cmt ( 2 abvd + 20 gy if - rt ) mit einem pet - gesttzten vorgehen , bei dem im falle einer komplettremission nach 2 zyklen abvd auf die konsolidierende radiotherapie verzichtet wurde , whrend pet - 2 - positive patienten bestrahlt wurden . 
die toxizittsrate unter der radiotherapie war gering : nur 2 , 9 % ( 19 von 659 patienten ) zeigten hhergradige akute nebenwirkungen , wobei kein grad 4 festgestellt wurde . 
nach 3 zyklen abvd erhielten pet - positive ( pet - 3 ) patienten einen weiteren zyklus abvd und 30 gy if - rt ( 4 abvd + ifrt )  . 
pet - 3 - negative patienten ( 74 , 6 % aller pet - patienten ) wurden randomisiert und erhielten entweder die konsolidierende radiotherapie ( 3 abvd + if - rt ) oder keine weitere behandlung ( 3 abvd ohne rt )  . 
hier ist allerdings zu ergnzen , dass in beiden studien auch patienten mit fortgeschrittenen tumorstadien eingeschlossen waren . dies fhrt zu der frage , ob die durchfhrung einer pet nach abschluss der systemtherapie berhaupt sinnvoll ist , weil die pet - 2 offenbar keine therapeutischen konsequenzen hat . 
so wird auch in der aktuellen s3 - leitlinie keine evidenzbasierte empfehlung zur anfertigung einer pet / ct nach abschluss der chemotherapie in den frhen stadien ausgesprochen [ 19 ]  . 
entsprechend zeigte hd16 eine verschlechterung des pfs fr pet2 - positive patienten , sodass die autoren den einsatz der interim - pet empfehlen . fazit die hd16 - studie [ 1 ] besttigt letztlich die bisher publizierten daten : der verzicht auf die bestrahlung bei pet2 - negativen patienten verschlechtert das pfs ohne einuss auf das os . die akute toxizitt war in hd16 unter der strahlentherapie gering , und die inzidenz von sekundrtumoren im nachbeobachtungszeitraum nicht erhht . 
so sollte also zusammenfassend bei patienten mit frhen stadien des hodgkin - lymphoms die chemotherapie mit 2 zyklen abvd gefolgt von einer konsolidierenden radiotherapie der therapiestandard bleiben . dessen ungeachtet treten metachrone solide sekundrtumoren eventuell noch 25 [ 4 , 22 ] bis 30 jahre [ 8 , 22 ] nach der primrtherapie auf . 
hildebrandt geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
fuchs m , goergen h , kobe c , kuhnert g , lohri a et al ( 2019 ) hd16 positron emission tomography - guided treatment in earlystage favorable hodgkin lymphoma : nal results of the international , randomized phase iii hd16 trial by the german hodgkin study group . 
dhmke e , franklin j , pfreundschuh m , sehlen s , willich n et al ( 2001 ) hd04 low - dose radiation is sufcient for the noninvolved extended - eld treatment in favorable early - stage hodgkins disease : long - term results of a randomized trial of radiotherapy alone . 
engert a , franklin j , eich ht , brillant c , sehlen s et al ( 2007 ) hd07 two cycles of doxorubicin , bleomycin , vinblastine , and dacarbazine plus extended - eld radiotherapy is superior to radiotherapy alone in early favorable hodgkins lymphoma : nal results of the ghsg hd7 trial . 
engert a , pltschow a , eich ht , lohri a , drken b et al ( 2010 ) hd10 reduced treatment intensity in patients with early - stage strahlenther onkol ( 2020 ) 196 : 488491 hodgkins lymphoma . 
specht l , gray rg , clarke mj , peto r ( 1998 ) inuence of more extensive radiotherapy and adjuvant chemotherapy on long - term outcome of early - stage hodgkins disease : a meta - analysis of 23 randomized trials involving 3 , 888 patients . 
engert a , schiller p , josting a , herrmann r , koch p et al ( 2003 ) hd08 involved - eld radiotherapy is equally effective and less toxic compared with extended - eld radiotherapy after four cycles of chemotherapy in patients with early - stage unfavorable hodgkins lymphoma : results of the hd8 trial of the german hodgkins lymphoma study group . 
noordijk em , carde p , dupouy n , hagenbeek a , krol adg et al ( 2006 ) h7f combined - modality therapy for clinical stage i or ii hodgkins lymphoma : long - term results of the european organisation for research and treatment of cancer h7 randomized controlled trials . 
behringer k , goergen h , hitz f , zijlstra jm , greil r et al ( 2015 ) hd13 omission of dacarbazine or bleomycin , or both , from the abvd regimen in treatment of early - stage favourable hodgkins lymphoma ( ghsg hd13 ) : an open - label , randomised , non - inferiority trial . 
hutchings m , loft a , hansen m , pedersen lm , buhl t et al ( 2006 ) fdg - pet after two cycles of chemotherapy predicts treatment failure and progression - free survival in hodgkin lymphoma . 
bednaruk - mynski e , pienkowska j , skrzak a , makowski b , kulikowski w et al ( 2015 ) comparison of positron emission tomography / computed tomography with classical contrast - enhanced computed tomography in the initial staging of hodgkin lymphoma . leuk lymphoma 56 : 377382 . 
gallamini a , rigacci l , merli f , nassi l , bosi a et al ( 2006 ) the predictive value of positron emission tomography scanning performed after two courses of standard therapy on treatment outcome in advanced stage hodgkins disease . 
rigacci l , puccini b , zinzani pl , biggi a , castagnoli a et al ( 2015 ) the prognostic value of positron emission tomography performed after two courses ( interim - pet ) of standard therapy on treatment outcome in early stage hodgkin lymphoma : a multicentric study by the fondazione italiana linfomi ( fil )  . 
spaepen k , stroobants s , dupont p , thomas j , vandenberghe p et al ( 2001 ) can positron emission tomography with ( 18 ) f - uorodeoxyglucose after rst - line treatment distinguish hodgkins disease patients who need additional therapy from others in whom additional therapy would mean avoidable toxicity ? br j haematol 115 : 272278 . 
engert a , haverkamp h , kobe c , markova j , renner c et al ( 2012 ) hd15 reduced - intensity chemotherapy and pet - guided radiotherapy in patients with advanced stage hodgkins lymphoma ( hd15 trial ) : a randomised , open - label , phase 3 non - inferiority trial . 
borchmann p , goergen h , kobe c , lohri a , greil r et al ( 2018 ) hd18 pet - guided treatment in patients with advanced - stage hodgkins lymphoma ( hd18 ) : nal results of an open - label , international , randomised phase 3 trial by the german hodgkin study group . 
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andr mpe , girinsky t , federico m , reman o , fortpied c et al ( 2017 ) h10 early positron emission tomography response - adapted treatment in stage i and ii hodgkin lymphoma : nal results of the randomized eortc / lysa / fil h10 trial . 
laskar s , gupta t , vimal s , muckaden ma , saikia tk et al ( 2004 ) consolidation radiation after complete remission in hodgkins disease following six cycles of doxorubicin , bleomycin , vinblastine , and dacarbazine chemotherapy : is there a need ? j clin oncol 22 : 6268 . 
nachman jb , sposto r , herzog p , gilchrist gs , wolden sl et al ( 2002 ) randomized comparison of low - dose involved - eld radiotherapy and no radiotherapy for children with hodgkins disease who achieve a complete response to chemotherapy . 
specht l , yahalom j , illidge t , berthelsen ak , constine ls et al ( 2014 ) modern radiation therapy for hodgkin lymphoma : eld and dose guidelines from the international lymphoma radiation oncology group ( ilrog )  . 
murray l , sethugavalar b , robertshaw h , bayman e , thomas e et al ( 2015 ) involved node , site , eld and residual volume radiotherapy for lymphoma : a comparison of organ at risk dosimetry and second malignancy risks . 
april 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund nach brusterhaltender operation vermindert eine perkutane radiotherapie der gesamten brust ( wbi ) mit werktglich einmaligen behandlungen ber 35 wochen die lokalrezidivraten und fhrt zu guten kosmetischen ergebnissen . 
im rapid - trial wurde untersucht , ob eine external - beam - apbi ( eb - apbi ) einer wbi nicht mglicherweise unterlegen ist . methodik an der multizentrischen , randomisierten , auf nichtunterlegenheit angelegten studie beteiligten sich 33 zentren in kanada , australien und neuseeland . 
brusterhaltend operierte 40 - jhrige patientinnen mit dcis ( ductales carcinoma in situ ) oder nodal - negativem mammakarzinom wurden 1 : 1 randomisiert zur therapie entweder in form einer eb - apbi ( 38 , 5 gy in 10 fraktionen , zweimal tglich ber 58 tage ) oder in form einer wbi ( 42 , 5 gy , appliziert in 16 fraktionen , einmal tglich , ber 21 behandlungstage oder 50 gy , appliziert in 25 fraktionen , einmal tglich , ber 35 behandlungstage )  . 
die studie war angelegt auf basis einer erwarteten ibtr - rate von 1 bis 5 % in der originalpublikation whelan tj , julian ja , berrang ts et al ( 2019 ) rapid trial investigators . 
external beam accelerated partial breast irradiation versus whole breast irradiation after breast conserving surgery in women with ductal carcinoma in situ and node - negative breast cancer ( rapid ) : a randomised controlled trial . 
juli 2011 wurden 2135 patientinnen registriert und 1070 in den eb - apbiund 1065 in den wbi - arm randomisiert . von diesen erhielten letztlich 1044 eine eb - apbi und 1047 eine wbi . 
radiogene akuttoxizitten ( grad 2 , innerhalb von 3 monaten nach rt - beginn ) traten seltener auf in der eb - apbi - gruppe ( 300 [ 28 % ] von 1070 patientinnen ) als in der wbi - gruppe ( 484 [ 45 % ] von 1065 ; p = 0 , 0001 )  . demgegenber entstanden radiogene spttoxizitten ( grad 2 , spter als 3 monate nach rt ) huger in der eb - apbi - gruppe ( 346 [ 32 % ] von 1070 ) als in der wbigruppe ( 142 [ 13 % ] von 1065 patientinnen ; p = 0 , 0001 )  . unbefriedigende kosmetische resultate ( deniert als ausreichend [ fair ] oder schlecht [ poor ] ) bestanden huger in der eb - apbials in der wbi - gruppe nach 3 jahren ( absoluter unterschied : 11 , 3 % , 95 % - ci 7 , 515 , 0 ) , nach 5 jahren ( 16 , 5 % , ci 12 , 520 , 4 ) und nach 7 jahren ( 17 , 7 % , ci 12 , 922 , 3 )  . interpretation der autoren in bezug auf die verhinderung eines ibtr war eine eb - apbi einer wbi nicht unterlegen . 
bei geringerer radiogener akuttoxizitt war eine ebapbi jedoch mit einem moderaten anstieg der spttoxizitt und ungnstigerer kosmesis verbunden , was mit der 580 strahlenther onkol ( 2020 ) 196 : 579582 zweimal tglichen applikation zusammenhngen knnte . andere anstze wie eine nur einmal tgliche eb - apbi - behandlung knnten zu einer besseren kosmesis fhren und sollten untersucht werden . kommentar zur minderung des risikos nichtinvasiver oder invasiver in - brust - rezidive ( ibtr ) nach operativer behandlung von patientinnen mit dcis oder invasivem mammakarzinom im lokal begrenzten stadium und mit niedrigem risikoprol werden inzwischen alleinige akzelerierte teilbrustbestrahlungsbehandlungen ( apbi ) als angemessene alternativen zur konventionellen perkutanen bestrahlungstherapie der gesamten verbliebenen brust ( wbi ) angesehen [ 16 ]  . 
diese erkenntnisse werden auch bercksichtigt bei dem auf die tumorregion begrenzten boost - konzept im rahmen einer wbi bei patientinnen mit ungnstiger risikokonstellation . akzelerierte radiotherapieverfahren ( apbi ) wurden in erster linie entwickelt , um die therapiedauer durch jeweilige applikation hoher einzeldosen zu verkrzen und somit die behandlung fr die patientinnen zu vereinfachen . mit derselben zielsetzung werden auch bei der wbi in randomisierten klinischen studien unterschiedliche hypofraktionierungskonzepte erfolgreich eingesetzt . 
40 gy gesamtdosis ( gd ) mit tglichen einzeldosen , verabreicht in 3 wochen . in prospektiven , randomisierten klinischen studien wurden unterschiedliche apbi - techniken ( singleoder multikatheter - brachytherapien , intraoperative rt mit elektronen oder photonen , external - beam - rt [ eb - apbi ] in form einer 3 - d - konformalen [ 3 - d - crt ] oder als intensittsmodulierte ( imrt ) mit linearbeschleunigern ) angewandt und im vergleich zu wbi - verfahren eingesetzt . 
gegenber anderen apbi - verfahren hat die eb - apbi - technik den vorteil , dass sie weltweit verfgbar , nicht invasiv und nicht ressourcenintensiv ist . unter den wenigen vergleichsstudien von alleiniger ebapbi gegenber konventioneller und / oder hypofraktionierter wbi weisen der rapid - trial [ 9 , 10 ] und der uk - import - low - trial [ 11 ] fr einen nichtunterlegenheitstest zur ermittlung von ibtr - raten , berlebensund todeswahrscheinlichkeiten sowie fr toxizittsund kosmesisbeurteilungen statistisch adquate kohortengren auf [ 2 , 3 , 911 ]  . 
zu beachten ist , dass der nsbap - b - 9 / rtog0413 - trial im gegensatz zu den anderen studien auf gleichwertigkeit von eb - apbi und wbi , also eben nicht auf nichtunterlegenheit wie die anderen , angelegt war . 
im hinblick auf die ibrt - risikominderung im rapid - trial ist jedoch eine nichtunterlegenheit von eb - apbi gegenber wbi besttigt worden . in der nsbap - b - 9 / rtog - 0413 - studie waren die ibtrraten nach 10 jahren mit ca . 
die statistisch denierten vorgaben fr eine gleichwertigkeit wurden jedoch nicht erfllt . in der subgruppenanalyse lieen sich insgesamt geringe strahlenther onkol ( 2020 ) 196 : 579582 unterschiede nachweisen , sodass eine unterlegenheit der apbi nicht ausgeschlossen werden kann . 
der dokumentierte vorteil im rezidivfreien berleben nach wbi fhrte allerdings nicht zu unterschieden bezglich fernmetastasenfreiheit und gesamtberleben . im uk - import - low - trial betrugen die in 5 jahren kumulierten ibrt - raten 1 , 1 % in der standard - wbi - gruppe , 0 , 2 % in der experimentellen wbi - gruppe mit auf 36 gy reduzierter gd plus simultaner boost - rt und 0 , 5 % in der eb - apbi - gruppe . 
die hr lag bei ber 2 , 03 ( p = 0 , 003 fr die auf 36 gy gd reduzierte wbi - gruppe und p = 0 , 016 fr die eb - apbi - gruppe , verglichen mit der standard - wbikohorte ) , sodass sowohl eine auf 36 gy gd plus tumorbett - boost auf 40 gy gd als auch eine eb - apbi der standard - wbi nicht unterlegen sind . eine begrenzung des bestrahlungsvolumens auf die region des tumorbetts bei einer alleinigen apbi lie ein gnstigeres kosmetisches langzeitergebnis im vergleich zur wbi erwarten und sollte sich auch in unterschiedlichen radiogenen akutund sptfolgen und kosmetischen resultaten widerspiegeln . 
so traten in der rapid - studie radiogene grad - 2 - akuttoxizitten ( dermatitis , brustschwellung , schmerzen in der brust , pneumonitis ) bei einer eb - apbi im vergleich zur wbi statistisch signikant seltener auf durch weniger dermatitiden und schwellungen . 
als entscheidend sehen sie das mit 6 h zu geringe zeitintervall zwischen den fraktionen bei der eb - apbi an , das keine ausreichende reparatur des gesunden gewebes auf die bestrahlung ermgliche [ 9 , 10 ]  . ein intervall von 24 h oder mehr erweist sich demzufolge als geeigneter . im uk - import - low - trial wurden radiogene sptfolgen ( parameter : aussehen , verhrtungen , verfestigung , verkleinerung der brust , hautvernderungen , schulterversteifung ) nach einer eb - apbi signikant seltener beobachtet als nach einer standard - wbi . 
diese gnstigeren ergebnisse der eb - apbi wurden auch in der gruppe der hypofraktionierten , mit reduzierter gd von 36 gy plus simultan integriertem boost erfolgenden wbi beobachtet . im nsbap - b - 9 / rtog - 0413 - trial erfolgten keine detaillierten untersuchungen hinsichtlich radiogener spttoxizitten und kosmesis zwischen den verschiedenen apbiverfahren untereinander und gegenber der wbi . 
signikante unterschiede in der toxizitt ergaben sich nicht : grad 2 bei 921 ( 44 % ) und grad 3 bei 201 ( 10 % ) patientinnen in der apbi - gruppe gegenber grad 2 in 1193 ( 59 % ) und grad 3 bei 143 ( 7 % ) in der wbi - gruppe . fazit bei patientinnen mit niedrigem rckfallrisiko belegen die drei groen studien trotz ihrer z . 
zwar treten deutlich weniger unerwnschte radiogene sptfolgen bei einer wbi im vergleich zur eb - apbi in der rapid - studie auf und sind in dieser die kosmetischen ergebnis bei der wbi besser , aber durch ausreichend groe zeitintervalle ( 24 h ) knnen gnstigere und in etwa zur wbi gleichwertige ergebnisse mit einer alleinigen ebapbi erreicht werden : offenbar ist das ausma der akzeleration und nicht oder weniger die hhe der einzeldosen bei hypofraktionierungskonzepten radiobiologisch relevanter und entscheidend fr sptfolgen und kosmesis . 
krug d , baumann r , budach w et al ( 2017 ) breast cancer expert panel of the german society of radiation oncology ( degro )  . current controversies in radiotherapy for breast cancer . 
livi l , meattini i , marrazzo l et al ( 2015 ) accelerated partial breast irradiation using intensity - modulated radiotherapy versus whole breast irradiation : 5 - year survival analysis of a phase 3 randomised controlled trial . 
rodriguez n , sanz x , dengra j et al ( 2013 ) five - year outcomes , cosmesis , and toxicity with 3 - dimensional conformal external beam radiation therapy to deliver accelerated partial breast irradiation . 
smith bd , arthur dw , buchholz ta et al ( 2009 ) accelerated partial breast irradiation consensus statement from the american society for radiation oncology ( astro )  . 
strnad v , major t , polgar c , lotter m et al ( 2018 ) estro - acrop guideline : interstitial multi - catheter breast brachytherapy as accelerated partial breast irradiation alone or as boostgec - estro breast cancer working group practical recommendations . 
breast cancer expert panel of the german society of radiation oncology ( degro ) , duma mn , baumann r , budach w et al ( 2019 ) heart - sparing radiotherapy techniques in breast cancer patients : a recommendation of the breast cancer expert panel of the german society of radiation oncology ( degro )  . 
rapid trial investigators , peterson d , truong pt , parpia s et al ( 2015 ) predictors of adverse cosmetic outcome in the rapid trial : an exploratory analysis . 
rapid trial investigators , whelan tj , julian ja , berrang ts et al ( 2019 ) external beam accelerated partial breast irradiation versus whole breast irradiation after breast conserving surgery in women with ductal carcinoma in situ and node - negative breast cancer ( rapid ) : a randomised controlled trial . 
vicini fa , cecchini rs , white jr et al ( 2019 ) long - term primary results of accelerated partial breast irradiation after breast - conserving surgery for early - stage breast cancer : a randomised , phase 3 , equivalence trial . 
tribius5 received : 24 may 2019 / accepted : 19 december 2019 / published online : 31 january 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract background and objective patients with oropharyngeal carcinoma ( opc ) often have difculty swallowing , which may affect quality of life ( qol )  . 
long - term qol is independent on radiation dose . keywords head and neck cancer dose effect long - term study late toxicity intensity - modulated radiation therapy ( cid : 2 ) s . 
tribius , md phd s.tribius@asklepios.com 1 department of radiation oncology , university medical center hamburg - eppendorf , hamburg , germany 2 department of otolaryngology , center for clinical neurosciences , university medical center hamburg - eppendorf , hamburg , germany 3 department of voice , speech and hearing disorders , center for clinical neurosciences , university medical center hamburg - eppendorf , hamburg , germany 4 department of oral & maxillofacial surgery , center for clinical neurosciences , university medical center hamburg - eppendorf , hamburg , germany 5 department of radiation oncology , asklepios hospital st . 
georg , lohmhlenstrae 5 , 20099 hamburg , germany introduction the treatment of head and neck cancer is multimodal , consisting of a combination of surgery , radio ( chemo ) therapy , and / or immunotherapy . 
positive results with regard to tumor control probability ( tcp ) as well as reduction of toxicity by omitting swallowing organs during radiation can be achieved [ 22 ]  . 
it is an assumption that limiting the dose to other structures of the swallowing apparatus , such as strahlenther onkol ( 2020 ) 196 : 522529 the constrictor muscles , reduces the incidence of dysphagia to a similar extent [ 9 ]  . 
approval was obtained from the local ethics committee . all patients provided written informed consent . of these 251 , 54 patients had oropharyngeal carcinoma and were still in follow - up care , and this population provided the basis for this study . 
with respect to the irradiation dose of the constrictor muscles , patients were divided into two groups . cut - off limits were set at 55 gy and < 55 gy [ 15 , 17 ]  . 
the kolmogorovsmirnov test , which conrmed our data analyses , served as a prerequisite for the application of the t - test as a pair correlation test . results this is an analysis of six timepoints ( t0t5 ) of a quality of life study including 54 patients with opc . 
1 a delineation according to the consensus atlas [ 4 ] ( brown : pharyngeal constrictor muscle ) ; b example of planned dose intensity and delineated mpcm ( purple ) of patient ; c example of contouring of the mpcm ( purple ) in axial ct imaging of patient ; d illustration of contoured spcm ( yellow ) , mpcm ( purple ) , and ipcm ( turquoise ) in sagittal ct imaging after contouring in axial scan tomography . 
after the third follow - up appointment qol scores of the study align with the reference population . at the end of radiotherapy ( t0 ) the qol averages at 30.66 while it returns to 71.08 at 2 years ( t5 ) after end of treatment . 
for the ipcm at a dose of 55 gy , 14 ( 64% ) patients developed dysphagia grade ( cid : 2 ) 2 and 8 ( 36% ) patients grade 2 at the end of radiotherapy . 
eighteen months after the end of radiotherapy ( t4 ) , the group with higher irradiation dose ( 55 gy ) , consisting of 19 ( 86% ) patients , experienced dysphagia grade 2 and three ( 14% ) 3 , while at < 55 gy , 31 ( 97% ) patients developed grade ( cid : 2 ) 2 and only one ( 3% ) patient showed grade 3 . 
of patients with radiation dose 55 gy , 29 ( 64% ) developed grade ( cid : 2 ) 2 and 16 ( 36% ) grade 3 right after radiotherapy , while at lower irradiation dose < 55 gy , 7 ( 78% ) patients showed degrees of ( cid : 2 ) 2 and only 2 ( 22% ) 3 . 
as expected in an irradiated population , at the beginning of the follow - up period , patients participating in this study had a signicantly worse baseline global health status and symptom scale score than a similar - aged reference german population [ 18 ]  . 
there appears to be no association between radiation dose to constrictor muscles and qol . with regard to dysphagia , a number of studies of patients with oropharyngeal carcinoma show the relationship between radiation dose to certain anatomical structures and the likelihood of developing clinically signicant acute and / or late radiation - induced dysphagia [ 3 , 5 , 10 , 23 ]  . 
higher radiation dose during treatment appeared to be a signicant predictor of subsequent long - term dysphagia . patients with higher radiation dose ( 55 gy ) show statistically signicantly greater dysphagia levels . 
showed that late dysphagia 1 year after treatment only depends on radiation dose . a dose of > 55 gy to constrictor muscles is associated with the risk of long - term dysphagia grade 3 [ 17 ]  . 
 [ 16 ] contoured the constrictor muscles in their study to analyze the relationship between planned dose and acute dysphagia as well as late dysphagia [ 16 ]  . their study looked at their patients 3 and 6 months afstrahlenther onkol ( 2020 ) 196 : 522529 ter the end of treatment and concluded that ipcm cannot be correlated with acute and late dysphagia . 
however , this study considers follow - up appointments of up to 2 years and , thus , is able to observe changes to late dysphagia in the long run beyond 6 months . 
radiation exposure in the mpcm shows a signicant correlation to late dysphagia over a period of 8 weeks ( t1 ) to 18 months ( t4 ) but not beyond that . 
when considering long - term dysphagia in patients after radiation , it seems invaluable to include a longer timespan than 6 months after treatment to acknowledge full longterm effects . in 2013 , deantonio et al . 
late dysphagia was dened as 1 year after treatment and the median follow - up was 20.5 months ( range 1263 months )  . they showed a signicant relationship between long - term dysphagia and mean doses to spcm , mpcm , and whole constrictor muscles . 
moreover , follow - up was carried out sometime between 12 and 63 months after treatment whereas this study managed to question all patients in set time intervals over 2 years . a study by levendag et al . 
published in 2007 investigated the association between the dose of radiation to pharyngeal constrictors with respect to dysphagia in terms of quality of life in oropharyngeal carcinoma [ 15 ]  . 
on the contrary , radiation exposure to the spcm has no statistical effect on late dysphagia , whereas exposure to the ipcm is signicantly associated with the development of long - term dysphagia . 
mean dose in this study for higher radiation doses ( 55 gy ) lies around 60 gy , while for lower radiation doses ( < 55 gy ) it concentrates at 50 gy across all constrictor muscles . 
however , the differentiation between spcm and mpcm as well as mpcm and ipcm was particularly difcult , as the limits of the three constrictor muscles on ct were difcult to distinguish . 
in certain cases , however , contouring was made more difcult by artefacts as well as by the oropharyngeal tumor itself . conclusion based on these results , an association between dysphagia and radiation dose to pharyngeal constrictor muscles can be found . 
however , in patients with locally advanced opc , the dose to the superior swallowing muscle appears to be of little relevance in the long terlongterm quality of life is independent of radiation dose . 
tribius declare that they have no competing interests . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
we have previously reported on the incidence of sarp among patients with moderate pulmonary dysfunction who received denitive concurrent chemoradiotherapy ( dccrt ) for non - small cell lung cancer ( nsclc )  . methods the clinical outcomes , dosevolume histograms ( dvh ) , and pf parameters of 122 patients ( forced expiratory volume in 1 s [ fev1% ] : 6069% ) receiving dccrt between 2013 and 2019 were recorded . 
logistic regression , receiver operating characteristics curves ( roc ) , and hazard ratio ( hr ) analyses were performed to evaluate the predictive value of each factor for sarp . results univariate and multivariate analysis indicated that the ratio of carbon monoxide diffusing capacity ( dlco% ; odds ratio [ or ] : 0.934 , 95% condence interval [ ci ] 0.8960.974 , p = 0.001 ) and mean lung dose ( mld ; or : 1.002 , 95% ci 1.0011.003 , p = 0.002 ) were independent predictors of sarp . 
prospective studies are needed to validate our ndings . keywords thoracic cancer radiation - induced toxicities risk factor carbon monoxide diffusing capacity mean lung dose the authors ying zhou and tiansheng yan contributed equally to the manuscript . ( cid : 2 ) youling gong , md , phd gongyouling@wchscu.cn 1 department of thoracic oncology and state key laboratory of biotherapy , cancer center , west china hospital , sichuan university , 610041 chengdu , china 2 department of pulmonary and critical care medicine , west china hospital , sichuan university , 610041 chengdu , china 3 department of radiation oncology , cancer center , west china hospital , sichuan university , 610041 chengdu , china introduction denitive concurrent chemoradiotherapy ( dccrt ) is the standard of care in patients diagnosed with locally advanced ( stage iiiab ) non - small cell lung cancer ( nsclc ) [ 1 , 2 ]  . radiation pneumonitis ( rp ) is a common complication of thoracic radiation therapy , and severe acute radiation pneumonitis ( sarp ) of grade 3 may lead to life - threatening complications in certain cases [ 3 , 4 ]  . 
numerous studies have investigated the predictors for rp , including age , smoking status , concurrent chemotherapy , dosevolume histogram ( dvh ) parameters , and others [ 512 ]  . reports suggest that the incidence of lung cancer in those with chronic obstructive pulmonary disease ( copd ) is threeto four - fold higher than that of those without 506 strahlenther onkol ( 2020 ) 196 : 505514 [ 13 , 14 ]  . 
according to international guidelines , pulmonary dysfunction is dened by forced expiratory volume in the rst second to forced vital capacity ( fev1 / fvc ) ratios of less than 0.70 [ 15 , 16 ]  . certain researchers have suggested that baseline parameters ( fev1 and others ) obtained from pulmonary function ( pf ) testing may predict the risk of rp [ 8 , 1719 ]  . 
in a prospective study , fev1 , ratio of carbon monoxide diffusing capacity ( dlco ) , and the exhaled fraction of nitric oxide ( feno ) prior to ccrt was found to be predictive of the incidence of rp in patients with nsclc [ 11 ]  . to date , no studies have evaluated the incidence of sarp among patients with baseline moderate pulmonary dysfunction who received dccrt for lung cancer . 
our study aimed to evaluate the correlation between the incidence of sarp and clinical characteristics , including pre - treatment pf parameters , in this select group of patients . materials and methods patients we retrospectively reviewed the data of patients with pathological diagnoses of nsclc in our hospital between january 2013 and march 2019 . 
moderate pulmonary dysfunction was dened based on the recommendations of the american thoracic society ( ats ) and the european respiratory society ( ers ) , with ratios of actual / estimated rst second of forced expiration ( fev1% ) values in the range of 6069% [ 20 ]  . 
among 632 patients with locally advanced nsclc who completed dccrt , the records of 122 demonstrated evidence of pre - treatment moderate pulmonary dysfunction . denition of clinical and dvh factors the data on the clinical characteristics that were recorded included age , gender , eastern cooperative oncology group ( ecog ) performance status , smoking status , tnm stage , chemotherapy regimens , and radiotherapy techniques . 
the dvh parameters recorded included the lung v5 / 20 and mean lung dose ( mld ) ; they were calculated and obtained from planned dose distributions based on convolution / superposition algorithms . radiotherapy radiotherapy was delivered using intensity - modulated radiation therapy ( imrt ) to a total dose of 6066 gy at 2.0 gy per fraction , at ve fractions per week . 
similar to the descriptions in our previous report , [ 25 , 26 ] , the gtv was dened as the macroscopically identiable tumor including lymph nodes with a margin of more than 1 cm on planning computed tomography images . 
the planning organ at risk volumes ( prvs ) extended for 5 mm around the spinal cord . the dosevolume constraints for the lungs were set as follows : v5 < 65% , v20 < 35% , and mld < 20 gy . 
the maximum doses allowed to the spinal cord and heart prvs were 50 gy and v50 < 25% , respectively , and the mean dose was < 20 gy . chemotherapy regimens all of the patients received concurrent chemotherapy during radiotherapy ; the regimens included paclitaxel with carboplatin ( pc ) and etoposide and cisplatin ( ep ) , in accordance with the national comprehensive cancer network ( nccn ) guidelines [ 27 ]  . 
the chemotherapy dosing and adjustments were performed as per the nccn panel recommendations . pulmonary function parameters the enrolled patients underwent both whole - body plethysmography ( wbp ) and gas ( helium ) dilution ( mbhd ) using the full masterscreen pft system ( jaeger corp , germany ) , which was equipped with a mixing fan , carbon dioxide ( co2 ) absorber , oxygen ( o2 ) and helium supply , gas inlet and outlet , and a water vapor absorber . the pulmonary function parameters recorded included the forced expiratory volume in 1 s% predicted ( fev1% ) , forced expiratory volume in 1 s / forced vital capacity ( fev1 / fvc ) , peak expiratory ow% predicted ( pef% ) , maximum expiratory ow% predicted ( mmef% ) , maximum expiratory ow at 75% of fvc% predicted ( mme75% ) , maximum expiratory ow at 50% of fvc% predicted ( mmef50% ) , maximum expiratory ow at 25% of fvc% predicted ( mmef25% ) , maximal voluntary ventilation% predicted ( mvv% ) , vital capacity% strahlenther onkol ( 2020 ) 196 : 505514 residual volume / total predicted ( vc% ) , lung capacity ( rv / tlc ) , diffusing capacity for carbon monoxide% predicted ( dlco% ) , resistance in airways% predicted ( raw% ) , and specic airway conductance% predicted ( sgaw% )  . endpoint denitions any rp of grade 3 according to the common terminology criteria for adverse events ( ctcae ) , version 4.0 [ 28 ] , during or within 3 months of completion of ccrt , was recorded as sarp . 
the diagnosis of sarp was conrmed by at least two experienced radiation oncologists based on the clinical symptoms , synchronous computed tomography scans of the chest ( to exclude the possibility of tumor progression ) , and evidence of administration of inhalational oxygen and corticosteroids in the medical records . statistical methods univariate logistic regression was performed to evaluate the predictive value of the individual factors for sarp . 
all of the tests were two - sided , and a value of p < 0.05 was considered statistically signicant . results patient characteristics the baseline characteristics of the study population are summarized in table 1 . 
overall , 31 ( 25.4% ) patients were recorded to have sarp ; 20.5% ( 25 patients ) , 3.3% ( four patients ) , and 1.6% ( two patients ) had developed rp of grades 3 , 4 , and 5 , respectively . 
among the pf parameters , dlco% ( or : 0.956 , 95% ci : 0.9250.988 , p = 0.007 ) , fev1 / fvc ( or : 1.043 , 95% ci : 1.0061.082 , p = 0.022 ) , pef% ( or : 1.030 , 95% ci : 1.0041.057 , p = 0.024 ) , mef75% ( or : 1.027 , 95% ci : 1.0051.049 , p = 0.016 ) , and mef50% ( or : 1.027 , 95% ci : 1.0011.055 , p = 0.045 ) signicantly correlated with the in508 strahlenther onkol ( 2020 ) 196 : 505514 table 2 univariate analysis of the dvh parameters / pulmonary function parameters and clinical factors in predicting sarp with sarp ( n = 31 ) median ( iqr ) without sarp ( n = 91 ) median ( iqr ) univariate analysis or ( 95%ci ) p - value dvh parameters total lungs v5 ( % ) v20 ( % ) mld ( cgy ) heart v50 ( % ) mean dose ( cgy ) spinal cord ( cgy ) pulmonary function parameters fev1% fev1 / fvc pef% mmef% mmef75% mmef50% mmef25% mvv% rv / tlc dlco% sgaw clinical factors age ( years ) sex : male vs . 
none of the clinical and pathological features including gender , age , ecog performance status , and chemotherapy regimen demonstrated signicant correlations with the occurrence of sarp in the study population . multivariate analysis was performed using the signicant factors obtained durthese included the v20 , mld , ing univariate analysis ; dlco% , fev1 / fvc , pef% , mef75% , and mef50% . on multivariate analysis , the dlco% ( or : 0.934 , 95% ci 0.8960.974 , p = 0.001 ) and mld ( or : 1.002 , 95% ci 1.0011.003 , p = 0.002 ) were independent predictive factors for sarp in the present cohort ( shown in table 4 )  . as shown in table 3 , spearmans correlation analysis demonstrated relationships between the ventilation parameters . 
compared with patients in the mld - low group ( mld ( cid : 2 ) average value ) , those in the mld - high group ( mld > average value ) had a higher risk of sarp , with a hazard ratio numerous studies have assessed possible predictors of the risk of sarp . 
roc receiver operating characteristics , dlco% diffusing capacity for carbon monoxide% predicted , mld mean lung dose , sarp severe acute radiation pneumonitis obtained from pf testing and dvh analysis , respectively , had potential predictive value for the occurrence of sarp in this selected population ; the combination of these two factors was found to be more meaningful . two dvh - based parameters , namely , mld and vdose , were previously identied to be important predictive factors for the risk of rp in patients with nsclc or other tumor types receiving thoracic radiotherapy . 
reports from martel et al . [ 29 ] , graham et al . [ 30 ] , and hernando et al . [ 31 ] suggested that the risk of rp with radical radiotherapy for lung cancer increased signicantly in cases where the mld was 20 gy . 
in another study on patients with lung cancer , the incidence of symptomatic rp was 15.0% , and the mld ( p = 0.043 ) was statistically signicantly related to rp [ 34 ]  . recent ndings from the study by lee et al . 
that used perfusion single - photon - emission computed tomography and uorodeoxyglucose positron - emission tomography imaging also suggested that the mld ( also functional mld ) was a signicant predictor of grade 2 pneumonitis , with a cutoff value of 13.6 gy ( functional mld : 13.2 gy ) [ 35 ]  . 
mld - low / dlco% - low group strahlenther onkol ( 2020 ) 196 : 505514 several studies have investigated the correlation between the dlco and incidence of rp after thoracic radiotherapy . in 2004 , videtic et al . 
in their cohort of 215 patients , the incidence of toxicity - related interruptions was found to be signicant for dlco values of less than 60% ( p = 0.043 ) [ 36 ]  . 
in a prospective study on 53 patients with nsclc , rp of grade 2 based on the ctcae scale was observed in 40% ( 15 / 37 ) ; the development of rp was significantly associated with several pre - treatment pf parameters including fev1% ( p = 0.02 ) , dlco ( p = 0.02 ) , and feno ( p = 0.04 ) [ 11 ]  . 
found that the correlation between the percent reduction in the dlco and the risk of rp differed signicantly between rp of grades ( cid : 2 ) 1 and 2 ( p = 0.0004 ) [ 37 ]  . 
in a study using a neural network model , the fev1 and dlco% were individually found to be signicant risk factors for rp ( p < 0.05 ) [ 18 ]  . 
indicated that poor baseline pf did not increase the risk of radiation - induced lung toxicity ( rilt ) [ 7 ] ; on multivariate analysis , the mld and age ( 65 years ) were signicantly correlated with the development of symptomatic rilt . 
found that patients with better dlco values had longer overall survival ; they found no signicant association between any parameter of pre - treatment pf and the risk of either grade 2 or 3 radiation pneumonitis [ 38 ]  . 
in this cohort of 483 patients , the radiation technique used was image - guided stereotactic body radiotherapy , which differed from the conventionally fractionated radiotherapy technique used in our study . in their systematic review , chen et al . 
indicated a relation between interstitial lung disease - specic toxicity and treatment - related mortality ; the studied population included patients with early - stage lung cancer [ 39 ]  . from a physiological perspective , the dlco reects the available alveolar surface area , the volume of blood present in the pulmonary capillaries , and the thickness of the alveolar capillary membrane . 
this parameter is helpful in the evaluation of patients with dyspnea , obstructive lung diseases , and restrictive lung diseases , with or without pulmonary parenchymal involvement ; it is also useful for assessing patients with pulmonary vascular diseases . 
in a study on rats , early changes in lung perfusion , the development of hypoxia , and chronic oxidative stress after irradiation were found to be associated with a signicant increase in the activation of macrophages and the continuous production of reactive oxygen species , which stimulated the production of brogenic and angiogenic cytokines [ 41 ]  . 
another study found severe hypoxia to be associated with a signicant increase in macrophage activity , collagen deposition , lung brosis , and levels of tgf - beta , vegf , and cd - 31 endothelial cell markers , suggestive of hypoxia - mediated activation of the pro - brinogenic pathways [ 42 ]  . 
in a recent study [ 46 ] that prospectively analyzed patient - , dose - , and pft - related data before and after thoracic radiation therapy , the ndings suggested that the dlco may be the most reliable indicator for lung tissue damage after thoracic radiotherapy . 
therefore , the dlco hier steht eine anzeige . 512 strahlenther onkol ( 2020 ) 196 : 505514 is likely to play an important role in radiation - induced lung toxicity , including rp . unfortunately , we failed to identify any other dosimetric or clinical factors that correlated signicantly with the risk of sarp . 
reported that the heart mass receiving > 30 gy was a predictor for the risk of rp in combination with the v5 of the left lung ( rs = 0.35 , auc = 0.78 ) [ 47 ]  . 
a study from the memorial sloan kettering cancer center found that the heart dose correlated strongly with symptomatic rp in a large cohort of patients with malignant pleural mesothelioma , where both lungs were treated with intensity - modulated pleural radiation therapy [ 48 ]  . 
although the nccn panel recommended dose constraints for the normal heart , the results of rtog 0617 suggested that lower radiation doses also have a negative impact on patient survival after thoracic rt , and more stringent constraints may be appropriate [ 50 ]  . the present study has several limitations . 
in particular , the pre - treatment pf may have been inuenced by the bulky tumor ( stage t3 or t4 ) ; this may have indicated bias in certain recruited patients who did not have actual moderate pulmonary dysfunction caused by other comorbidities ( such as copd , among others )  . 
in a prospective phase ii trial using a mid - treatment pet / ct - adapted radiation therapy strategy , only three ( 7% ) patients developed grade 3 rp [ 53 ]  . 
therefore , re - simulation and plan modication may be employed in practice for patients with nsclc . the relatively high incidence of sarp in the present study requires further analysis . 
in our opinion , pre - treatment moderate pulmonary dysfunction may explain the high incidence of sarp . in conclusion , the dlco% and mld may be possible predictors of the incidence of sarp in patients with baseline moderate pulmonary dysfunction who receive denitive ccrt for nsclc . 
future prospective studies are warranted to validate our ndings . funding this project was supported by a grant from sichuan provincial science and technology funding to youling gong ( 2018sz0184 )  . this work has been selected to be presented partly in digital poster form at the american society for radiation oncology annual meeting , 2019 . author contribution youling gong conceived and designed the study . yin zhou , tiansheng yan , xiaojuan zhou , peng cao , chunli luo , and youling gong collected the data . 
yin zhou , tiansheng yan , and youling gong analyzed and interpreted the data and drafted the article . lin zhou , yong xu , yongmei liu , jianxin xue , jin wang , yongsheng wang , you lu , and binmiao liang critically revised the paper . 
april 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund und fragestellung als neue erweiterung der multimodalen therapie von glioblastompatienten hat sich die behandlung mit elektrischen feldern ( tumor treating elds [ ttf ] ) zustzlich zur operation , strahlentherapie ( rtx ) und chemotherapie ( ctx ) etabliert . 
die therapie wird durchgefhrt bis zum zweiten radiologischen nachweis eines progresses . in der studie electric fields - 14 ( ef - 14 ) fhrte die zustzliche behandlung mit ttf im vergleich zu einer alleinigen postoperativen radiochemotherapie mit temodal gefolgt von einer temodalerhaltungstherapie zu einer signikanten verlngerung des medianen progressionsfreien berlebens ( pfs ) von 4 , 0 monaten auf 6 , 7 monate und des gesamtberlebens ( os ) von 16 , 0 monaten auf 20 , 9 monate bei patienten mit supratentoriellen glioblastomen und einem karnofsky - index von mindestens 70 % [ 1 ]  . originalpublikation ballo mt , urman n , lavy - shahaf g et al ( 2019 ) correlation of tumor treating elds dosimetry to survival outcomes in newly diagnosed glioblastoma : a large - scale numerical simulation - based analysis of data from the phase 3 ef - 14 randomized trial . 
30 , 26655 westerstede , deutschland 2 klinik fr strahlentherapie und spezielle onkologie , medizinische hochschule hannover , hannover , deutschland interessant ist dabei , dass smtliche subgruppen von den ttf protieren , unabhngig z . 
vom o6 - methylguanin - dna - methyltransferase - promotor ( mgmt ) - methylierungsstatus , alter des patienten oder ausma der tumorresektion . durch die zustzliche ttf - therapie wurden keine zustzlichen nebenwirkungen bis auf hautirritationen durch die langfristige applikation der paster berichtet , insbesondere keine zunahme von krampfanfllen ( 6 % in beiden studienarmen )  . in einer retrospektiven analyse von ef - 14 wurde bereits ein einuss der patientencompliance im sinne der tglichen anwendungsdauer auf die onkologischen ergebnisse gezeigt . in der vorliegenden untersuchung wurde erstmalig versucht , eine dosis - wirkungs - beziehung der ttf durch eine berechnung der absorbierten elektrischen felddosis im tumorbett darzustellen . studienziel und - design die problematik beim versuch einer berechnung einer dosisverteilung fr ttf besteht darin , dass in der standardbildgebung ( ct oder mrt ) elektrische eigenschaften der gewebe nicht direkt messbar oder berechenbar sind . 
deshalb mussten patientenmodelle fr jeden patienten generiert werden , in denen standardisiert festgelegte elektrische eigenschaften ( leitfhigkeit und dielektrizittszahl ) unterschiedlicher gewebe ( haut / unterhaut , schdelknochen , liquor , graue substanz , weie substanz , km - aufnehmender tumor , km - aufnehmendes nichtmalignes gewebe , resektionshhle , tumornekrose , hmatom , ischmie , atrophie , luft ) semiautomatisch 3 - d rekonstruiert wurden . 
zusammen mit der vorgegebenen position der transducer arrays und der durchschnittlichen monatlichen anwendungsdauer konnte nun eine feldintensittsverteilung durch eine spezische software berechnet werden . 584 strahlenther onkol ( 2020 ) 196 : 583585 um die ergebnisse mit der ionisierenden bestrahlungsplanung in der die absorbierte dosis zentrales verordnungsund planungskriterium ist vergleichbar zu machen , wurde die feldintensitt ( die nur die krfte beschreibt , die auf einen dipol wirken ) um die ttfields power loss density ( energieverlustdichte ) erweitert . 
um zu bercksichtigen , dass bei den ttf zwei feldrichtungen stndig wechseln , wurde jeweils das lokale minimum sowohl der feldintensitt ( local minimum eld intensity [ lmifi ] in v / cm ) als auch der energiedichte ( local minimum power density [ lmipd ] in mw / cm3 ) dokumentiert . 
diese werte wurden im tumorbereich mit zustzlich 3 mm saum gemittelt . um den einuss der patientencompliance zu bercksichtigen und damit neben der geplanten auch die tatschlich applizierte energie nherungsweise zu erfassen , wurde die energiedichte lmipd mit der compliance ( durchschnittliche tgliche anwendungszeit in % von 24 h ) multipliziert zur lokalen minimalen dosisdichte ( local minimum dose density [ lmidd ] in mw / cm3 )  . die therapieergebnisse von 340 patienten wurden mit den errechneten physikalischen und dokumentierten complianceparametern korreliert . 
ausgeschlossen aus dem studienkollektiv von ef - 14 wurden 87 patienten , die weniger als 2 monate die ttf anwenden konnten , und 39 patienten , deren mrt qualitativ nicht ausreichten , um die o . 
lmiflund lmipd - werte wurden ermittelt , die um 20 % um den mittelwert streuten und die die patientengruppe mglichst scharf hinsichtlich des os einteilten . ergebnisse im bereich von liquoroder rektionshhlen , die sich durch eine hohe leitfhigkeit auszeichnen , war generell die lokale minimale feldintensitt lmifi gering , whrend die lokale minimale energiedichte lmipd relativ hoch blieb , sodass auch in diesen bereichen viel energie deponiert werden konnte . 
beide parameter blieben prognostisch als auch bei gleichzeitiger bercksichtigung anderer faktoren / patienten - , tumorund therapiecharakteristika wichtig . die deutlichsten unterschiede ergaben sich bei der lmipd mit zustzlicher bercksichtigung der patientencompliance , also der lmidd , die sich der tatschlich applizierten ( und nicht nur der geplanten ) dosis annhert . der cut - off fr diese lokale minimale dosisdichte wurde auf 0 , 77 mw / cm3 gesetzt . 
interessanterweise war die lmidd auch mit der lebensqualitt ( lq ) assoziiert : werte > 0 , 77 mw / cm3 korrelierten signikant mit einer verlngerung des erhalts der lq vor verschlechterung ( infolge eines tumorprogresses ) mit 18 m vs . 
9 , 1 m ( p = 0 , 004 )  . schlussfolgerungen der autoren das vorgestellte konzept beschreibt die ttf - dosis als produkt von ttf - energieverlustdichte in der tumorhhle mit der patientencompliance . 
ber den bereits bekannten effekt der compliance hinaus legen die daten eine korrelation zwischen hoher ttf - dosis und den onkologischen ergebnissen nahe . kommentar die biologischen wirkungen von elektrischen feldern sind qualitativ abhngig von der frequenz der feldnderungen . niedrige frequenzen ( < 1 khz ) fhren zu einer depolarisation von zellmembranen [ 2 ]  . 
mit ansteigenden frequenzen ( mehrere khz bis mhz ) nden diese effekte nicht mehr statt , da die reaktionszeiten der zellbiologischen prozesse zu lang sind , um auf diese stimulationen noch reagieren zu knnen . 
als ein wesentlicher wirkmechanismus in der tumortherapie wird die interaktion der elektrischen felder mit hoch polaren moleklen ( den tubulinlamenten und den spindelapparaten ) whrend der zellteilung angenommen , wodurch die mitose der tumorzellen gestrt , prolongiert und inhibiert wird [ 3 ]  . dieser effekt erinnert biologisch deutlich an die mitotische katastrophe , die whrend der mitose bei durch ionisierende strahlung induzierten dizentrischen chromosomen auftreten kann . 
bei wesentlich hheren frequenzen der elektrischen felder ( > mehrere mhz ) steht dann eine physikalische wrstrahlenther onkol ( 2020 ) 196 : 583585 meentwicklung im vordergrund [ 2 ]  . 
hier gelingt es erstmalig , ber eine mrt - geplante simulation die therapieergebnisse nicht nur mit der feldintensitt , sondern auch mit der energieverlustdichte ( als quivalent fr die applizierte dosis in der ionisierenden radiotherapie ) zu korrelieren . wird dieser begriff um die compliance erweitert , entspricht die so ermittelte local minimum dose density ( lmidd ) nicht nur der geplanten , sondern auch der tatschlich applizierten dosis . 
in dem nachtrglich auf diese werte hin analysierten patientenkollektiv von ef - 14 zeigten sich signikante zusammenhnge mit dem os und pfs auch wenn andere prognostische faktoren zwischen den gruppen mit einer lmidd unter 0 , 77 mw / cm3 vs . 
allerdings bieten sie eine gute grundlage , um entsprechende studien planen zu knnen . hinsichtlich der biologischen wirkung fllt die enge biologische verwandtschaft der effekte der radiotherapie und der ttf in der strung der tumormitosen auf . 
hieraus ergibt sich die klinische fragestellung , ob die effektivitt der multimodalen therapie nicht zustzlich gesteigert werden knnte durch ein vorziehen der ttf in die laufende radiotherapie hnlich wie bei der radiosensibilisierung durch eine simultane chemotherapie . 
diese htte den zustzlichen praktischen vorteil , dass dann im rahmen der radiotherapieplanung auch eine ttf - therapieplanung durch die mit dosisverteilungen , physik und technischem vorgehen am besten vertraute disziplin die radioonkologie erfolgen knnte . 
eine generelle aufwertung der ttf als onkologische behandlungsoption wre dadurch wahrscheinlich . fazit ( cid : 2 ) eine individuelle simulation einer elektrischen dosisverteilung ( hnlich der physikalischen dosisverteilung ionisierender strahlung ) ist mrt - basiert mglich . 
durch bercksichtigung der patientencompliance kann so auf die tatschlich applizierte elektrische energie geschlossen werden ( genannt local minimum dose density [ lmidd ] )  . ( cid : 2 ) die lmidd ist in einer retrospektiven analyse der patienten aus der ef - 14 - studie signikant mit dem os , dem pfs und dem erhalt der lq assoziiert . 
damit ist eine dosis - wirkungs - beziehung der ttf plausibel ( aber noch nicht bewiesen )  . ( cid : 2 ) diese neue vielversprechende physikalische therapieoption knnte in idealer weise das rstzeug der radioonkologie ergnzen . robert michael hermann , westerstede , und roland merten , hannover interessenkonikt r.m. 
stupp r , taillibert s , kanner a et al ( 2017 ) effect of tumor - treating fields plus maintenance temozolomide vs maintenance temozolomide alone on survival in patients with glioblastoma . 
this paper aimed to investigate the role of this hypoxia classier as a prognostic factor for patients with oropharyngeal cancer ( opc ) treated with accelerated chemoradiotherapy . methods p16 and 15 - gene hypoxia classier status , categorising tumours as more or less hypoxic , were determined for 136 opc patients . 
locoregional recurrence rate ( lrr ) and overall survival ( os ) were estimated with cumulative incidence function and kaplanmeier method , respectively , stratied according to p16 and hypoxia status . results p16 - positive patients ( 34.6% ) had signicantly better lrr and os than p16 - negative patients . 
rt induces dna damage within the tumour , but the response of the tumour to this ionising radiation strongly depends upon the presence of oxygen , which can xate the damage [ 1 ]  . 
oxygen deciency , hypoxia , provides the tumour cells a survival advantage , resulting in a major inuence on tumour radioresistance and treatment efcacy . therefore , numerous clinical trials have been devoted to hypoxia modication and the prediction of the oxygenation status of the tumour . 
different strategies to overcome the hypoxic radioresistance have been explored , specically , increasing the oxygen delivery to the tumour , optimising the tumour vasculature or using agents targeting specifically the hypoxic cells [ 2 ]  . 
these latter agents , usually nitroimidazole derivatives , mimic the function of oxygen and therefore , can make the tumour cells more sensitive strahlenther onkol ( 2020 ) 196 : 552560 to ionising radiation [ 1 ]  . 
a meta - analysis of 18 clinical trials with various hypoxic radiosensitisers , misonidazole , etanidazole and nimorazole , showed improved locoregional control ( lrc ) and disease - specic survival when combining hypoxia modication with conventional fractionated or hypofractionated rt [ 2 ]  . 
however , only nimorazole , a hypoxic radiosensitiser with the most favourable toxicity prole , has been implemented in the standard of care in combination with rt for hnscc in denmark since the randomised controlled dahanca 5 showed improved lrc in the experimental arm , rt plus nimorazole [ 3 ]  . 
to predict the benet of nimorazole , a 15 - gene hypoxia classier was developed in the dahanca 5 population and was later validated on independent samples of the dahanca 18 , dahanca 24 and iaea hypox trial [ 46 ]  . 
this manuscript aims to investigate the prognostic value of the 15 - gene hypoxia classier in an oropharyngeal cancer ( opc ) cohort treated with accelerated crt . methods patient and treatment characteristics : one hundred eighty - two opc patients who were included in 2 prospective studies were analysed in the current study . one hundred thirteen patients were originally included in a study looking at the prognostic value of diffusionweighted mri in hnscc between 2004 and 2010 [ 7 , 8 ]  . 
the second group of 69 patients were included in an ongoing trial examining prognostic features of diffusion - weighted mri in opc between 2013 and 2018 ( nct01829646 )  . 
local ethics committee approval was obtained and written informed consent was obtained from all individual participants included in the study . inclusion criteria of this study were patients with histologically proven non - resected squamous cell carcinoma of the oropharynx of all stages . 
an equivalent rt dose of 70 gy in fractions of 2 gy was given in 6 weeks either using a sequential boost or simultaneous integrated boost [ 9 ]  . 
chemotherapy and cetuximab regimens consisted of 3 - weekly intravenous cisplatin 100 mg / m2 or intravenous cetuximab 400 mg / m2 loading dose 1 week before rt followed by weekly infusions of 250 mg / m2 during rt , respectively . 
as we aimed to investigate the role of the hypoxia classier in patients table 1 genes included in the 15 - gene hypoxic classier , their function and the three reference genes gene function stress response glucose metabolism proteinprotein interactions apoptosis apoptosis unknown regulation of hif - 1 activity apoptosis extracellular matrix metabolism stress response extracellular matrix metabolism extracellular matrix metabolism energy metabolism glucose metabolism glucose metabolism aldoa ankrd37 bnip3 bnip3l c3orf28 egln3 kctd11 ndrg1 p4ha1 p4ha2 pdk1 pfkfb3 slc2a1 reference genes rpl37a actr3 ndfip1 treated with accelerated chemoradiotherapy , patients not treated with accelerated rt or platinum - based chemotherapy were excluded from further analyses . follow - up in all patients was performed every 2 months in the rst 2 years , every 3 months in the third year , every 4 months in the fourth year and bi - annually after that . evaluation of recurrence included clinical examination and laryngoscopy . 
imaging ( ct , mri or pet scan ) was performed 3 to 4 months following the end of the rt or if failure was suspected during further follow - up . p16 status p16 immunohistochemistry staining was performed on formalin - xed and parafn - embedded ( ffpe ) tumour tissue or on ne - needle aspiration cytology obtained during diagnostic work - up . 
patients with unknown p16 status were not eligible for analysis . 15 - gene hypoxia classier hypoxia gene expression analyses were performed on ffpe samples as previously described [ 46 ]  . 
the ffpe samples were obtained during the standard diagnostic procedure . seven m slices were sent to the laboratory of the depart554 strahlenther onkol ( 2020 ) 196 : 552560 182 pa ( cid : 2 ) ents with oropharyngeal cancer 12 excluded due to unknown p16 status 109 pa ( cid : 2 ) ents with p16 nega ( cid : 2 ) ve oropharyngeal cancer 61 pa ( cid : 2 ) ents with p16 posi ( cid : 2 ) ve oropharyngeal cancer 3 pa ( cid : 2 ) ents excluded due to no treatment with chemotherapy or accelerated rt 17 pa ( cid : 2 ) ents excluded due to unknown hypoxia status : 9 : no ( cid : 2 ) ssue blocks available 8 : rna degrada ( cid : 2 ) on 1 pa ( cid : 2 ) ent excluded due to no treatment with chemotherapy or accelerated rt 13 pa ( cid : 2 ) ents excluded due to unknown hypoxia status : 11 no ( cid : 2 ) ssue blocks available 2 rna degrada ( cid : 2 ) on 89 pa ( cid : 2 ) ents with p16 nega ( cid : 2 ) ve oropharyngeal cancer 26 more hypoxic 63 less hypoxic fig . 
1 flow diagram of included patients 47 pa ( cid : 2 ) ents with p16 posi ( cid : 2 ) ve oropharyngeal cancer : 12 more hypoxic 35 less hypoxic ment of experimental clinical oncology , aarhus university hospital , denmark . 
total rna was extracted using the tissue preparation system with versant tissue preparation reagents ( siemens healthcare diagnostics , tarrytown , ny , usa ) , a fully automated , bead - based rna isolation method [ 11 ]  . 
the nal mixtures consisted of 3 l pre - amplied cdna , 1 taqman genotyping master mix ( applied biosystems ) and 1 taqman assay in a nal volume of 15 l . 
the genes included in the 15 - gene hypoxia classier are shown in table 1 . measurements of the gene expression were excluded if cycle threshold ( ct ) values were above 35 or if the technical standard deviation of the duplicates was more than 0.3. the entire sample was omitted if measurements from one of three reference genes ( rpl37a , actr3 and ndfip1 ) were excluded . 
the expression values were further normalized to a cohort of patients from previous dahanca trials in order to classify them using the original hypoxia gene classier and to compare them with the published data from the dahanca 5 trial [ 4 , 13 ]  . 
comparisons were performed with the fisher exact test for categorical variables and the mannwhitney u test for continuous variables classication was performed blinded from any patient characteristics or outcome data . statistics patient and tumour characteristics were compared with the fisher exact test for categorical variables and the mannwhitney u test for continuous variables . 
patients on follow - up and patients lost to follow - up were censored at the last date at which they were known to be alive . fine and gray models , univariate and multivariate cox 556 strahlenther onkol ( 2020 ) 196 : 552560 fig . 
2 locoregional recurrence rate ( lrr ) estimated with the cumulative incidence function stratied by p16 status for all included patients ( a ) ; by hypoxic status for all included patients ( b ) ; p16 - negative oropharyngeal cancer ( opc ) only ( c ) and p16 - positive opc only ( d ) proportional hazards regression modelling , respectively , were used to compare the groups and to compute hazard ratios ( hr ) with 95% condence intervals ( ci95% ) and the corresponding p - value . 
univariate analysis concluded that t stage and ajcc stage ( 7th edition ) were in addition to p16 status signicantly associated with os . in multivariate analysis , only p16 status and ajcc stage ( 7th edition ) remained signicant ( table 3 )  . 15 - gene hypoxia classier one hundred and forty - six ffpe samples were sent for hypoxia gene classier determination . 
patient and treatment characteristics of the more and less hypoxic groups were well balanced in the overall opc cohort as well as in the p16 - negative and p16 - positive subgroups ( table 2 , online resource 1 )  . 
given that there were no locoregional events in the more hypoxic group , hr could not be estimated and pepe and mori test was used as an analogue to the fine and gray model . 
a p - value below 0.05 was considered statistically signicant discussion in this paper , the prognostic impact of the 15 - gene hypoxia classier was investigated in an opc population treated primarily with accelerated crt . 
nevertheless , in the overall opc cohort and the p16 - negative opc subgroup , the lrr and os were not signicantly different between the more and less hypoxic opc , as determined by the classier . 
these results are in contrast with previous publications investigating the 15 - gene hypoxia classier as both a prognostic and predictive factor for p16 - negative opc patients treated with conventional fractionated rt [ 5 ]  . 
in the paper of toustrup et al . , p16 - negative opc patients , of which the 15 - gene hypoxia classier showed more hypoxia , had higher lrr rate and more benet of hypoxia modication with nimorazole [ 6 ]  . 
however , the standard of care for locally advanced hnscc , previously conventional fractionated rt , has changed drastically based on two meta - analyses showing the superiority of concomitant crt and rt with altered fractionation [ 14 , 15 ]  . 
therefore , it is relevant to investigate the prognostic impact of the hypoxia classier in a patient population treated with accelerated crt . in agreement with ndings in previous studies , the same frequency of hypoxia was seen in p16 - positive as in p16negative opc [ 6 , 13 ]  . 
interestingly , an in vitro study showed that p16 - positive cell lines display the same response to hypoxia and the same oxygen enhancement ratio as p16 - negative cell lines [ 16 ]  . 
nonetheless , in the paper of toustrup et al . , the hypoxia classier was in the p16 - positive opc not prognostic nor predictive for hypoxia modication [ 6 ]  . a possible explanation is the markedly higher intrinsic radiosensitivity of human papillomavirus - related opc which overcomes the negative effect of hypoxia [ 4 ]  . 
in parallel , we hypothesise that the radiosensitivity of the p16negative opc is affected more by other determinants , including radiosensitisation by chemotherapy and minimising the repopulation of tumour cells by accelerated fractionation , than by hypoxia . one previous research group investigated the prognostic impact of this 15 - gene hypoxia classier in hnscc treated with accelerated or conventionally fractionated crt . in general , they could only observe a signicant lrr difference depending on hypoxia status in tumours with a tumour volume smaller than 19 cm3 [ 17 ]  . 
the strength of our publication is that the 15 - gene hypoxia classier was determined with the original technique and by the research team who developed the classier [ 5 ]  . 
the hypoxic radiosensitiser nimorazole may inuence the prognosis and , as a result , the prognostic value of the 15 - gene hypoxia classier cannot be established in these two trials [ 4 , 19 , 20 ]  . the hypoxia classier was initially not developed as a prognostic tool but as a method to characterise the oxygenation status of a tumour . 
hif - 1 promotes tumour progression by activating the transcription of numerous genes which regulate processes of glucose metabolism , cell proliferation and angiogenesis [ 21 , 22 ]  . 
acceleration of the rt , shortening the overall treatment time , can counter the negative effect strahlenther onkol ( 2020 ) 196 : 552560 of repopulation [ 15 ]  . 
the p16 - negative more hypoxic tumours are not randomised , and these tumours are all treated with the accelerated crt regimen plus nimorazole according to the standard of care in denmark . 
unfortunately , both trials were closed due to insufcient recruitment rate [ 23 ]  . limitations of our study are the non - uniformly treatment regimen , the older patient samples and the limited sample size , especially of p16 - positive opc . 
nevertheless , the original development samples were even older , 20 to 24 years , and we observed the expected frequencies of hypoxia in the p16 positive and negative , reassuring that the data are robust and valid [ 6 ]  . 
finally , although there was a signicant difference regarding lrr in favour of the p16 - positive more hypoxic group , due to the limited sample size and the lack of lrr events in the more hypoxic group , these results are underpowered and thus inconsequential . to conclude , our results suggest that the 15 - gene hypoxia classier may not have prognostic value in an opc patient cohort treated with accelerated crt . funding this project is supported by a grant from stand up to cancer ( kom op tegen kanker ) , the flemish cancer society . compliance with ethical guidelines conict of interest s . 
nuyts declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants or on human tissue were in accordance with the ethical standards of the institutional and / or national research committee and with the 1975 helsinki declaration and its later amendments or comparable ethical standards . 
the close agreement and consistency of data conrmed the merits of direct intercomparisons for assessing rbe differences between particle radiations of different energy [ 3 ]  . strahlenther onkol ( 2020 ) 196 : 586588 obituary obituary for friedrich zywietz l . 
with the territorial changes after the war , the family left neidenburg in 1945 and settled in agathenburg / stade , where friedrich attended high school and studied physics in hamburg . 
in 1966 he was appointed to the research staff of the department of biophysics and radiation biology at the university klinikum eppendorf ( uke ) under professor ha kunkel . zywietz later qualied as rer nat and dr rer nat habil , and was appointed professor of biophysics and radiation biology in 1997 . 
to overcome the problem of reaching deep - seated tumours , he showed that 6 gev bremsstrahlung is very promising both in terms of tissue penetration and radiobiological effectiveness [ 1 ]  . 
however , introduction of fast neutrons quickly changed these prospects when it became known that the depth dose of high - energy neutrons is very similar to megavoltage x - rays . in the ensuing international excitement about the therapeutic promises of high relative biologic effectiveness ( rbe ) and low oxygen enhancement ratio ( oer ) irradiation , many types of neutron sources were explored . 
by comparing the broad - spectrum 6 mev d - be neutron beam in essen with the monoenergetic 14 mev d - t beam at hamburg , zywietz et al . 
1 friedrich zywietz , biophysicist ( 19362019 ) ( prof . friedrich zywietz ) strahlenther onkol ( 2020 ) 196 : 586588 other clinically relevant topics in hamburg were the search for irradiation conditions which would generate g2m cells by cell synchronization . 
however , a lack of cell kinetic data for human tumours made it difcult to attribute this effect to the accumulation of tumour cells in g2m phase [ 4 ]  . 
when hyperthermia emerged as a potent adjuvant to irradiation soon thereafter [ 5 ] , zywietz used his r1h tumour model to achieve close coupling of heat and irradiation and thermal enhancements in the region of 1.4 for ir - a irradiation as the heat source [ 6 ]  . 
using the same model , we showed that the vasoactive drug pentoxifylline enhances tumour oxygenation and tumour control [ 7 ] , while in vitro irradiation of r1h cells exposes a whole range of other cellular responses largely dependent on p53 status [ 8 ]  . in the last years of his experimental work , zywietz studied the inuence of irradiation on the vasculature , showing profound deterioration of the epithelium ( blebbing ) and dependence of tumour hypoxia upon irradiation dose and time [ 9 ]  . 
this work attracted much attention in the group of peter vaupel , as the 45 - gy threshold identied by zywietz on the basis of epithelial demise was also seen by vaupel [ 10 ] as the onset of metabolic deterioration indicated by the decline of atp and increase of glucose in the irradiated tissue . 
understanding of the micromilieu is now at the centre of ultra - high - dose rate ( flash ) radiotherapy [ 11 , 12 ]  . zywietz was supported by the erwin braun foundation and together with bhm by the volkswagenstiftung . to encourage the translation of new mechanistic understanding into the clinic , zywietz donated a dissertation prize for radiation biology and experimental radiation oncology ( to the freundesund frderkreis at uke )  . 
the rst recipient was a student from the group of professor kersten borgmann for a thesis identifying the egfr mutant viii as a marker for the sensitivity of glioblastomas to temozolomide . 
this review discusses pulmonary toxicity in ews patients with pulmonary metastases treated with wli , who received different modes of high - dose chemotheray ( hd - cth )  . methods literature was compiled using the cochrane library , pubmed database , and the national institute of health ( nih ) clinical trials register . 
relevant patient information , including nature of hd - cth , acute and late lung toxicities , and pulmonary function disorders , was selected from the above databases . results nine reports with a total of 227 patients , including 57 patients from a single randomized trial were included in this review . 
no acute or chronic symptomatic pulmonary toxicities were observed in patients that received wli after hd busulfan - melphalan ( hd - bu / mel ) , but 8% of these patients were diagnosed with asymptomatic restrictive lung disease . grade 1 or 2 acute or chronic lung adverse effects were observed in up to 30% of patients that received wli after hd treosulfan / mel ( hd - treo / mel ) or hd etoposide ( e ) / mel . 
radiation doses as well as time between hd - cth and wli were both identied as signicant risk factors for pulmonary function disorders . conclusion the risk of adverse lung effects after wli depends on several factors , including cumulative radiation dose and dose per fraction , hd - cth regimen , and time interval between hd - cth and wli . 
according to the multicenter cooperative ews studies ( cess ) , wli should complement multimodal therapy in pediatric ews patients with complete radiological remission of pulmonary 496 strahlenther onkol ( 2020 ) 196 : 495504 fig . 
the following search terms were used : ewing sarcoma , pulmonary metastases , whole lung irradiation , high - dose chemotherapy , pulmonary side effects databases : cochrane library , pubmed , nih clinical register publication dates : 01 / 01 / 1988 31 / 12 / 2018 publication types : randomized trial , case series primary findings : 117 reports ( electronic sources ) , 1 trial ( nih register ) eligibility assessment 13 articles ( cochrane library , pubmed ) and 1 nih reference nt . 
 data validation 8 articles and 1 randomized trial ( 227 patients ) included in the systematic review metastases following polychemotherapy or after the resection of residual pulmonary metastases [ 6 ]  . however , these studies focussed on survival outcome , not on treatment - related toxicities . 
published data indicate an acceptable tolerability of wli in children , adolescents , and young adults , also in combination with conventional chemotherapy ( cth ) [ 13 , 7 , 8 ]  . however , tolerance of wli combined with high - dose cth ( hd - cth ) has not been sufciently analyzed in published multicentre studies researching therapy and survival in ews patients with pulmonary metastases [ 1 , 2 , 5 , 9 ]  . this systematic review evaluates the risk stratication of pulmonary function disorders , as well as radiogenic acute and late lung toxicities in the combined use of hd - cth and wli in primary and relapsed ews patients exhibiting lung metastases . material and methods study selection this systematic review was structured according to the preferred reporting items for systematic reviews and meta - analyses ( prisma ) reporting guidelines [ 10 ]  . 
1. studies on wli combined with cth or hd - cth that recruited patients with primary ews of any localization exhibiting pulmonary metastases or patients with isolated pulmonary relapse were analysed . 
the following phrases were used for eligibility criteria : articles must be peer reviewed ; articles must be less than thirty years old ; and article must contain qualitative and / or quantitative analyses . 
when searching for articles , the authors directly specied all terms used , i.e. , ewing sarcoma , pulmonary metastases , whole lung irradiation , hd - cth , and pulmonary side effects . data extraction and study quality assessment literature search , selection of studies , and data extraction were separately performed by two trained and certied radiation oncologists ( ss )  . 
the senior author ( hte ) validated the results and resolved any discrepancies concerning data assessment . the following patient information was independently extracted from the databases : age , sex , radiation technique , fraction and cumulative radiation dose for wli , additional boost in case of chest wall primary ews , resection of pulhier steht eine anzeige . monary lesions , mode of hd - cth , post - treatment followup , acute and late lung toxicities , and pulmonary functional test . quality assessment of the selected studies was performed using the cochrane risk - of - bias tool [ 13 ]  . statistical analysis due to signicant heterogeneity within a variety of factors across the studies , including the age of patients , radiotherapy ( rt ) regimen , mode of hd - cth , methods of side - effect estimation , and patient follow - up , a mantel - haenszel random - effect model was used to estimate the mean distribution of acute and late lung toxicity across the studies . the cox proportional hazard regression analysis and the pearson correlation test were used to determine the risk of lung and non - lung - related adverse effects analyzing the following variables : age , sex , cumulative radiation dose , hdcth regimen , time interval between hd - cth and wli , rt technique , and radiation boost ( table 2 )  . 
used hd - cth with busulfan / melphalan ( bu / mel ) in 57 patients with primary pulmonary or single bone metastases with an interval of 6090 days before wli [ 14 ]  . 
reported on hd - cth with either treosulfan / melphalan ( treo / mel ) ( 27 patients ) or etoposide / melphalan ( e / mel ) ( ve patients ) in ews patients with isolated pulmonary relapse . 
a total rt dose ranged between 15 and 18 gy with a daily fractionation of 1.5 gy ( table 1 )  . in two series performed by pape et al . 
there were no data concerning thoracic boost toxicity in other studies . in four studies on a total of 14 patients , resection of lung lesions was performed before hd - cth and wli [ 5 , 14 , 17 , 19 ]  . 
in two reports , data on metastasectomy of lung nodules were not available ( table 1 ; [ 1 , 16 ] )  . analysis of adverse eects the toxicity results are shown in detail in table 1 . follow - up pulmonary function test ( pft ) data were available in three studies for 65 of the 227 patients that received wli . 
generally , restrictive lung disease was found in 20 patients ( 31% ) that had been treated sequentially with hd - cth and wli . of those , severe lung function disorders were observed in two ( 8% ) of 24 patients that received wli after hdbul / mel . 
the patients treated with treo / mel or e / mel and consolidating wli did not develop severe pulmonary functional disorders . pre - treatment pfts were reported only in a paper by scobioala and colleagues [ 5 ] : in ve patients ( 8% ) , mild or moderate lung impairment was diagnosed without further worsening after wli . 
acute or chronic pulmonary toxicity grades 1 and 2 were observed in seven of 27 patients ( 26% ) with pulmonary relapsed ews that received wli after hd - cth with treo / mel or e / mel ( table 1 )  . 
however , in most cases , the mortality was associated with the hd - cth regimen rather than with the wli : the most common causes of death were hemorrhagic or infectious complications , and four patients died from respiratory complications [ 1 , 19 ]  . 
second malignancies noted included acute myeloid leukemia ( three patients ) , myelodysplastic syndrome ( three patients ) , and liposarcoma ( one patient ) [ 15 ]  . risk factors that might inuence therapy - related toxicity in hd - ctx and wli regimens were also analyzed ( table 2 )  . regarding the impact of radiation dose on pulmonary function disorders , the 5% level of signicance was reached for 812 gy and 15 gy in the pearson correlation test ( p = 0.04 and p = 0.03 , respectively ) , but failed in the cox proportional hazard regression analysis . 
the data on radiation boost for thoracic ews were not eligible for the assessment ( tables 1 and 2 )  . discussion a systemic analysis is presented here of wli - related pulmonary toxicities with radiation applied sequentially or concurrently to hd - cth in ews patients with primary lung metastases or pulmonary relapse . past multicenter studies including cess - 81 , cess - 86 , and european intergroup ( ei ) cess - 92 demonstrated a therapeutic benet for wli in pediatric ews patients with primary lung metastases [ 1 , 2 , 6 , 7 ]  . 
improved local control of pulmonary disease as well as a marginal trend toward better progression - free survival make wli an important treatment option that should complement multimodal therapy in patients with lung relapse of ews [ 5 ]  . 
the cumulative doses on the lungs varied from 14 to 18 gy , similarly to the combination with conventional cth . luksch and colleagues combined hd - bu / mel and wli in a large number of ews patients ( n = 57 ) with lung - only metastases and no lung function impairment after hd - cth [ 14 ]  . 
the radiation dose was age - dependent and varied from 12 to 15 gy , which was applied 60 or 90 days after hd - cth . higher risk of additional pulmonary toxicities has limited the use of hd - bu / mel and wli in other cooperative studies [ 2123 ]  . 
however , the cumulative radiation dose with a maximum of 15 gy was lower than in other trials , where wli with a maximum dose of 18 gy was combined with hd - treo / mel or hd - e / mel ( table 1 )  . 
based on this study , a cumulative radiation dose of 15 gy and a time interval of at least 60 days might be recommended for wli after hd - bu / mel in high - risk ews patients with no lung function injury . combination therapy of hd - treo / mel or hd - e / mel and wli is widely used in patients with primary metastatic or relapsed ews [ 5 , 1517 , 19 , 20 ]  . 
generally , the reports presented in table 1 demonstrated a low rate of lung function disorders or lung toxicities using a radiation dose of 18 gy applied 810 weeks after hd - treo / mel or hdstrahlenther onkol ( 2020 ) 196 : 495504 e / mel . 
however , the lack of regular post - treatment pfts and documentation of adverse lung effects , which are most problematic in the studies analyzing simultaneous hd - cth and wli , could lead to an underestimation of lung toxicities ( table 1 )  . in most analyzed studies , survival and not therapy - related adverse effects were the main outcome parameters to be evaluated . 
thus , ndings on tolerability of wli after hd - cth remain extremely limited [ 5 , 7 , 9 , 14 ]  . no severe pulmonary function disorders or acute lung toxicities were reported after wli when applied sequentially following hd - treo / mel or hd - e / mel in analyzed studies ( table 1 )  . 
no correlation between pulmonary side effects and specic hd - cth modality was apparent across the studies . concomitant use of hd - cth and tbi was reported in a number of publications [ 1520 ]  . 
the cumulative radiation dose on the lungs varied between 8 and 12 gy with fractions between 1.5 or 2 gy applied once or twice daily ( table 1 )  . hd - e / mel was used in most of these studies . 
reported improved survival for hd - cth and 12 gy tbi compared to hd - cth alone [ 17 , 19 ]  . regardless , a simultaneous combination of hd - cth and tbi may contribute to high toxicity and increased rates of therapy - related death , as demonstrated in table 1 . 
this suggestion is supported by signicantly higher rates of death after simultaneous use of hde / mel and tbi with 8 gy or 12 gy compared to patients treated sequentially with hd - e / mel and wli delivering doses of 15 gy or 18 gy ( tables 1 and 2 )  . 
the impact of radiation dose in relation to fractionation on the development of pulmonary side effects was not evident in the present analysis . the impact of pulmonary tumor rest resection following hd - cth on radiogenically induced lung toxicities was analyzed in detail in the study by scobioala et al . 
in contrast , some authors observed a correlation between thoracic surgery and the development of pulmonary side effects following induction cth ( vaia or vide ) and wli [ 2 , 28 ]  . in other studies , data concerning lung nodule surgery was available in only a few patients and , for this reason , not eligible for prognostic assessment ( tables 1 and 2 )  . 
similarly , the impact of a radiation boost to the chest wall on adverse lung effects remains unclear due to a limited number of patients treated with a boost in this setting ( tables 1 and 2 )  . however , an additional boost to the thorax region should be considered a risk factor for radiogenically induced pneumonitis and pulmonary brosis . 
the authors found no difference in the frequency and severity of lung toxicities after hd - cth and wli between patients under and over 15 years of age ( table 2 )  . 
these ndings are supported by those of casey et al . , who observed acceptable tolerance of wli in adults with pulmonary metastatic ews [ 3 ]  . late toxicities such as underdevelopment of the chest wall in children or radiation - induced secondary malignancies were not analyzed in this setting . 
lack of treatment homogeneity in terms of different hd - cth and wli regimens , including the nature of hd - cth , methods of side effect estimation , the cumulative radiation dose on the lungs , dose per fraction , and different interval between hd - cth and wli , could account for the underestimation of the risk for lung toxicities . given these ndings , the risk of pulmonary toxicities after hd - cth and wli in ews patients with primary lung metastases or pulmonary relapse should be estimated in a prospective randomized trial . 
for instance , the use of ultra - fractionated wli with a fraction dose of < 0.5 gy could be evaluated for combination with hd - cth based on the hyper - radiation sensitivity phenomenon [ 3234 ]  . 
also , radiotherapy approaches including intensity - modulated radiotherapy ( imrt ) and proton therapy should be evaluated for wli , which may potentially improve the risk of acute and late pulmonary or extrapulmonary adverse effects . 
thus , superior sparing of the heart may be achieved by using a novel imrt prescription dose , termed simultaneous integrated protection for organ at risk , as shown by mazzola et al . 
used anatomic and perfused lung dosimetry for the risk stratication of radiation pneumonitis in patients undergoing denitive thoracic radiation [ 39 ]  . conclusion few relevant conclusions concerning pulmonary toxicity after combination therapy with hd - cth and wli can be drawn due to heterogeneity in study designs and reporting of results . 
meanwhile , the risk of lung disorders and lung toxicities is negligible in patients that received hdcth and wli sequentially , including patients treated with strahlenther onkol ( 2020 ) 196 : 495504 hd - bu / mel . 
based on the analyzed reports , it is difcult to stratify the patients that may be susceptible to pulmonary toxicity , as well as to dene the relationship between hdcth and wli regimens and pulmonary complications . 
for this reason , the risk of lung toxicities should be individually evaluated based on , e.g. , the presence of preexisting lung disorders , use of high cumulative radiation doses , or shortened interval between hd - cth and wli . funding open access funding provided by projekt deal . compliance with ethical guidelines conict of interest s . 
all studies performed were in accordance with the ethical standards indicated in each case . for images or other information within the manuscript which identify patients , consent was obtained from them and / or their legal guardians . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
winter2 stefan welz1 , 4 sergios gatidis4 , 5 dominik nann6 stephan ossowski3 , 7 , 10 thomas breuer8 christian la fougre4 , 9 konstantin nikolaou4 , 5 olaf riess3 , 10 daniel zips1 , 4 christopher schroeder3 daniela thorwarth2 , 4 received : 16 january 2020 / accepted : 9 march 2020 / published online : 24 march 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract purpose the relation between functional imaging and intrapatient genetic heterogeneity remains poorly understood . 
the aim of our study was to investigate spatial sampling and functional imaging by fdg - pet / mri to describe intrapatient tumour heterogeneity . methods six patients with oropharyngeal cancer were included in this pilot study . 
corresponding regions were delineated on pretherapeutic fdg - pet / mri images to extract apparent diffusion coefcients and standardized uptake values . results samples were collected within the primary tumour ( n = 3 ) , within the primary tumour and the involved lymph node ( n = 2 ) as well as within two independent primary tumours ( n = 1 )  . 
our data with a limited number of patients do not support the concept that multiparametric pet / mri features are useful to guide biopsies for genetic tumour characterization . keywords spatial sampling quantitative functional imaging next - generation sequencing radiogenomics oropharyngeal cancer introduction aiming for precision medicine , the understanding of interand intrapatient diversity of tumours might support successfully personalized therapeutic approaches . 
for this purpose , intrapatient tumour heterogeneity can be investigated by imaging features or by next - generation sequencing ( ngs )  . the relevant interpatient heterogeneity of somatic mutations in head and neck squamous cell carcinomas ( hnsccs ) has been shown before [ 35 ]  . 
furthermore , the extent of intrapatient diversity of solid tumours has been intensely investigated recently , as intratumour genetic heterogeneity ( ith ) might substantially contribute to therapy failure and dismal outcome in cancer patients [ 68 ]  . 
mcgranahan and swanton ( 2017 ) reviewed several studies of different cancer types and described distinct patterns of evolutionary trees with regard to ith according to diverse tumour types [ 7 ]  . 
tumours related to exogenous mutagens such as nicotine abuse or ultraviolet light ( lung adenocarcinomas of smokers and melanomas ) showed increased clonal mutational burden compared to other entities , but comparably reduced ith proportion . 
the majority of alterations of these tumours might have been acquired prior to invasiveness and therefore contribute to the large clonal trunk while the trees branches are formed by relatively fewer subclonal mutations [ 7 ]  . 
to investigate tumour diversity , spatial sampling of different biopsies can be applied [ 10 , 11 ]  . imaging features can be used as an additional evaluation of intratumour diversity [ 12 ]  . 
besides genetic diversity , image - based heterogeneity was also found to correlate with worse outcome [ 13 ] and correlations of genetic data and imaging features are gaining increased interest [ 14 ]  . 
however , studies investigating the spatial relationship of these two approaches remain rare [ 12 ]  . functional images can be obtained by magnetic resonance imaging ( mri ) , positron - emission tomography ( pet ) or by hybrid imaging combining both technologies ( pet / mri )  . 
diffusion - weighted mri ( dwi ) allows for quantication of water diffusion which depends on different tissue characteristics such as cell size , cell density and membrane architecture [ 15 ]  . 
besides dwi [ 16 ] , pet imaging with [ 18f ] uorodeoxyglucose ( fdg ) is an emerging technique for tumour characterization [ 17 ] and treatment guidance [ 18 ] in hnscc . 
therefore , our study addressed intrapatient heterogeneity of somatic mutations in hnscc and correlated this data with spatially corresponding functional pet / mri information . materials and methods ten patients with locally advanced oroor hyphopharyngeal hnscc were recruited prospectively for this pilot study ( nct - 02666885 )  . 
however , due to small tumour volumes , spatial sampling of two lesions per patient could be achieved only in six patients who were included in this planned interim investigation . 
the study was approved by the local ethics committee ( reference number 025 / 2015 ) and all patients declared their written informed consent . all patients received tumour resection with intended adjuvant radio ( chemo ) therapy at primary diagnosis and did not undergo any previous treatment . 
ahead of surgery , simultaneous fdg - pet / mri ( biograph mmr , siemens healthineers , erlangen , germany , 3 t ) was performed for anatomical and functional characterization of the tumours . 
for each region of interest ( roi , corresponding to the biopsy sites ) , mean adc as well as mean suv were calculated to investigate correlations with the genetic information . during surgery biopsies for ngs were collected from the surgical specimen in cooperation with the institute of pathology , to ensure sufcient tumour content . 
the tumour cell content was estimated by experienced pathologists . for genetic analyses , we applied a comprehensive panel approach ( 327 genes ) that was designed for hnscc tumours by the german cancer consortium ( dktk ) partner site in berlin [ 27 ]  . 
ethylenediaminetetraacetic acid blood samples of the patients were used for normal tissue controls . for library preparation and exonic region in - solution capture , the agilent haloplexhs technology ( agilent , santa clara , ca , usa ) was used . 
variant - calling and annotation were conducted using strelka2 ( version 2.8.4 ) [ 29 ] and snpeff / snpsift ( version 4.37 ) [ 30 ]  . nonsynonymous , coding mutations or splice region and splice donor variants with an allele frequency ( af ) > 5% were reported and compared to identify ubiquitous versus heterogeneous nonsilent mutations . all reported ubiquitous mutations were found in both samples at the same chromosome position with the identical nucleotide changes . 
all reported variants were visually validated in the raw data and crosschecked with the normal tissue as well as the corresponding other tumour sample . to identify predicted driver mutations , all somatic variants were uploaded to the cancer genome interpreter ( cgi ) [ 31 ]  . 
not available nicotine abuse yes , 30 pack years yes , 40 pack years yes , 45 pack years yes , 30 pack years yes , 40 pack years yes , 70 pack years six male patients ( 5266 years ) were included in this prospective biomarker study . 
the patient and tumour characteristics are summarized in table 1 . the panel sequencing results including heterogeneous and ubiquitous somatic mutations as well as annotated predicted or known driver mutations according to the cgi are shown in fig . 
apart from these variants , a distinct interpatient variability was found . considering intrapatient heterogeneity , in three patients ( patients 1 , 2 and 3 ) , both sequenced samples were collected within the same primary tumour . 
in a further patient ( patient 4 ) , the primary tumour and the corresponding lymph node metastasis were investigated and also showed predominant concordance . in two patients , more than one primary tumour was found . 
patient 5 had two primary tumours , namely a squamous cell carcinoma of the uvula ( partially keratinizing , 4.5 mm ) and of the base of tongue ( basaloid , 10 mm )  . a lymph node metastasis showed extracapsular extension and was morphologically associated with the base of the tongue carcinoma . 
three shared mutations in tp53 , lrp1b and syne1 were found . however , several additional private mutations as well as one predicted driver mutation in pdgfra in the lymph node biopsy were detected . patient 6 had three separate primary tumours . 
table 2 shows the adc and suv values according to the spatial sampling sides and the relative differences between the two biopsy areas per patient as well as the respective genetic variability of the samples . 
of note , the lymph node metastasis of patient 4 showed extensive necrosis , wherefore adc as well as suv values should be interpreted with caution for this patient . the other lesions investigated did not show major necrotic areas . 
5 shows exemplary imaging of patient 5 including the oropharyngeal tumour ( base of the tongue ) and the respective involved lymph node . 546 strahlenther onkol ( 2020 ) 196 : 542551 fig . 
shared and private mutations are shown in the venn diagrams and known or predicted driver mutations according to the cancer genome interpreter ( cgi ) database are printed in bold . 
3 correlation of mean apparent diffusion coefcients ( adcs ) and the genetic heterogeneity between the two samples per patient ( given by the fraction of divergent genetic variants to the total number of genetic variants )  . 
in patient 4 , the high adc value corresponds to a region of interest in a mainly necrotic lymph node and should be interpreted with caution discussion the model of clonal evolution of tumours and associated variant sublines was previously described by p.c. 
however , recent sequencing technologies allow further insight into intrapatient heterogeneity as ubiquitous and private mutations can be determined [ 10 , 33 ]  . for the estimation of genetic intrapatient heterogeneity and correlations between somatic mutations and imaging information , we focussed on coding ( and splice site ) , nonsynonymous single - nucleotide variants or small insertions / deletions with an af > 5% . 
 [ 34 ] , predicted functional changes can be estimated and are of targetable interest , while functional implications of intronic regions , copy number variations ( cnvs ) or noncoding variants are currently not well understood . 
we reported heterogeneous versus ubiquitous mutations based on a panel approach and did not calculate phylogenetic trees as we focussed on functional impact rather than on tumour evolution . strahlenther onkol ( 2020 ) 196 : 542551 fig . 
this is clinically important focussing on precision medicine , target therapies and potential dose painting as our results suggest minor diversity if samples were taken from the same primary tumour and some increasing heterogeneity if the primary tumour and the lymph node metastasis were aligned . especially predicted or known driver gene mutations were predominantly found ubiquitously which indicates common functional changes . 
thus , in some patients , relevant variants might be missed by single sampling but the majority of driver mutations could be detected by a single biopsy in our cohort . our ndings of rather limited intrapatient genetic diversity are in line with a recent publication about metastases in solid tumours that showed only minor functional driver gene heterogeneity between the different metastatic sites [ 34 ]  . 
the vast majority of functionally relevant mutations within individual patients was commonly found in all metastatic lesions . the majority of ubiquitous mutations compared to relatively less heterogeneous variants within the primary tumours may be explained by the long - time exposition to exogenous mutagens as all patients were active smokers for years at time of diagnosis . 
these ndings are well in line with the review of mcgranahan and swanton ( 2017 ) , indicating comparably small ith proportion in exogenous mutagen - driven cancers [ 7 ]  . table 2 apparent diffusion coefcient ( adc ) and [ 18f ] - uorodeoxyglucose ( fdg ) standardized uptake values ( suvs ) of the spatial sampling sides . 
5 showing the oropharyngeal tumour at the base of the tongue and the involved lymph node ( arrows ) : a , b positron - emission tomography , c turbo inversion recovery magnitude ( tirm ) imaging and d , e diffusion - weighted imaging with the apparent diffusion coefcient ( adc ) map due to the complex approach , studies about spatial sampling in patients with primary carcinomas of the oropharynx are rare and of very limited patient numbers . 
reported seven patients with carcinomas of the tongue , the oor of the mouth and the larynx and suggested the heterogeneity may vary with respect to the tumour localization [ 19 ]  . 
however , our results are in line with a report concerning ve patients with oral squamous cell carcinomas showing high interpatient but low intrapatient tumour heterogeneity [ 21 ]  . 
similar results were recently shown in spatial sampling of 13 tumours of the oral cavity , whereas patterns of oropharyngeal ( n = 6 ) , pharyngeal ( n = 3 ) and laryngeal cancers ( n = 1 ) that were matched to paired relapse tumour samples ( recurrence after chemoradiation ) showed greater heterogeneity [ 23 ]  . 
 ( 2016 ) reported six oral , three pharyngeal and four laryngeal carcinomas with relevant mutational similarity between the primary tumours and their corresponding synchronous lymph node metastases [ 22 ]  . 
furthermore , to the best of our knowledge , this is one of the largest cohorts of spatial sampling in patients with oropharyngeal carcinomas reported to date despite of our limited patient number . therefore , with full acknowledgement of the caveat due to our limited sample size , we suggest that intrapatient heterogeneity in oropharyngeal cancer might increase from rather similar mutation patterns within single primary tumours to slightly ascending diversity between the primary tumour and lymph node metastases . 
in some patients , single sampling might be sufcient to identify the functionally relevant , potentially druggable driver mutations , but if clinically and nancially feasible , spatial sampling should be considered . in contrast , two anatomically different primary tumours within one single patient ( oroand hypopharynx ) showed entire heterogeneity and several private driver gene mutations were found . 
only in one subgroup of patients with small cell lung cancer ( sclc ) was a correlation between the surface suv entropy and genetic heterogeneity found in involved lymph nodes . 
in lung tissue of sclc , in adenocarcinomas and squamous cell carcinomas as well as for all other investigated pet features , no distinct correlation between genetic heterogeneity and pet parameters was found . 
several correlations between selected driver genes and diverse mri parameters were reported . in our cohort of hnscc patients , we did not nd conclusive accordance between genetic heterogeneity and heterogeneity in the image - derived parameters adc and suv . 
this could be explained by multiple epigenetic and microenvironmental inuences affecting cell density and energy metaboliseven though biological validation of imaging biomarkers is desirable , not all imaging features might directly correlate with an equivalent pathologic tissue [ 37 ] or genetic prole . 
if our preliminary ndings of independent biomarkers can be conrmed in larger biomarker trials , mutation patterns , dw and pet imaging could be used complementary for tumour characterization . besides the small cohort and limited sample size , the limitations of this study include the use of a dedicated hnscc cancer panel instead of whole - exome or whole - genome sequencing . 
on the contrary , this panel approach focused on previously described , functionally relevant hnscc genes in which a deeper sequencing and detection of low - level mosaicism was feasible improving the reliability of results . 
thus , some minor inconsistencies with regard to the exact anatomic correlation between genomics and image - derived features cannot be ruled out . conclusion interand intrapatient heterogeneity are major challenges for successful tumour treatment . 
goltermann for the language editing . funding this project was funded by the center for personalised medicine ( zpm ) tbingen / germany ( grant number 025 / 2015bo1 )  . kerstin clasen was supported by the fortne / pate program of the medical faculty , eberhard karls university tbingen ( grant number : 2447 - 0 - 0 )  . 
parts of the research leading to these results have received funding from the european research council under the european unions seventh framework programme ( fp / 2007 - 2013 ) , erc grant agreement no . 
schroeder declare that they have no competing interests . ethical standards the study was approved by the local ethics committee ( reference number 025 / 2015 ) and all patients declared their written informed consent . 
objective measurement of salivary ow rate ( sfr ) under unstimulated ( usfr ) and stimulated conditions ( ssfr ) as well as subjective xerostomia assessment according to a patient - rated questionnaire were conducted before each mri . 
variance analysis was used to evaluate dynamic changes of adc , sfr and xerostomia questionnaire summary scores ( xq - sum ) at different timepoints and the correlation between adc and xq - supearsons correlation test was used to evaluate the correlations between preand post - rt changes of adc ( adc ) and sfr ( sfr ) or mean rt dose . results at each timepoint , adcs of pgs were signicantly lower than of smgs , usfr was signicantly lower than ssfr . 
adc1m - post - rt initially increased and changed little to adc3m - post - rt , adc6m - post - rt , adc9m - post - rt , and adc12m - post - rt , then gradually declined over time . 
the dynamic change trends of sfr were negatively paralleled to those of adc , while that of xq - sum was similar . doseresponse relationships were detected between salivary gland mean rt dose and adc . 
in pgs , negative correlations between ssfr9m - post - rt and adc9m - post - rt , and ssfr12m - post - rt and adc12m - post - rt were detected . 
in smgs , negative correlations between ssfr12m - post - rt and adc12m - post - rt , and usfr12m - post - rt and adc12m - post - rt were also detected . 
28 fuxing road , 100853 beijing , china 2 armed police forces corps hospital of henan province , no . 1 kangfu road , 450052 zhengzhou , china 3 department of radiation oncology , china - japan friendship hospital , no . 
28 fuxing road , 100853 beijing , china strahlenther onkol ( 2020 ) 196 : 530541 conclusion as part of routine follow - up mri in npc patients , dwi might be a promising modality for follow - up assessing the dynamic changes of major salivary gland function and might be more powerful in the late post - rt period . keywords diffusion - weighted imaging radiotherapy xerostomia salivary gland dysfunction nasopharyngeal carcinoma introduction nasopharyngeal carcinoma ( npc ) is one of the most common malignancies in southern china and southeast asia , with an extremely high geographical incidence of about 2530 per 100 , 000 persons per year [ 1 , 2 ]  . 
major salivary glands such as parotid glands ( pgs ) and submandibular glands ( smgs ) are both highly radiosensitive and often involved in or adjacent to rt targets designed for npc and apt to injury even after low - dose radiation [ 3 ]  . 
radiation - induced salivary gland injury and consequences such as xerostomia or dry mouth are probably the most common persistent oral sequelae for npc patients who receive therapeutic doses of rt . 
patients with xerostomia have considerable difculties with chewing and swallowing and are impaired in speech and social interactions , which have further implications with respect to quality of life , especially in long - term survivors [ 46 ]  . 
the probability and severity of xerostomia mostly depends on the dose distributions in pgs and smgs [ 7 ]  . lower radiation doses lead to a better - maintained salivary ow after rt . 
management of radiation - induced xerostomia by , e.g. , pharmacological interventions ( e.g. , amifostine , pilocarpine ) or submandibular gland transfer , appears to be benecial with insufcient evidence . 
therefore , the key lies in prevention by radiation dose reduction in major salivary glands . during the past two decades , high - precision intensitymodulated radiation therapy ( imrt ) technology with better conformity and dose homogeneity , such as helical tomotherapy ( ht ) , has been increasingly applied for npc treatment . 
with imrt , substantial dose reductions could be achieved to major salivary glands , resulting in retention of salivary output and amelioration of xerostomia without compromising dose delivery to the tumor [ 911 ]  . 
based on this , long - term follow - up evaluation of the dynamic physiological changes of irradiated salivary glands would be important to better understand the mechanism of radiation - induced injury , which in turn aids the investigation of methods to mitigate symptoms of xerostomia such as optimization of treatment plans before implementing rt . traditionally , radiation - induced salivary gland dysfunction can be assessed subjectively according to a patients symptoms as well as objectively using quantied saliva production or excretion ( scintigraphy and / or saliva ow ) [ 12 ]  . salivary gland scintigraphy ( sgs ) has been shown to be reliable in evaluating salivary gland function [ 13 , 14 ]  . 
salivary ow rate ( sfr ) measurement is the most commonly applied objective method in the clinic to quantify the severity of irradiated salivary gland dysfunction , but its results do not depict any morphological or physiological change of the irradiated salivary glands [ 12 ]  . diffusion - weighted imaging ( dwi ) , which can assess and quantify the structural and pathophysiological changes by visualizing the random thermal motion of water molecule diffusion , has been widely used as one of the routine follow - up mr examinations of npc patients for decades . 
in recent years , initial studies [ 1519 ] of dwi in assessing radiation - induced salivary gland dysfunction have been documented and observed signicant alterations of apparent diffusion coefcients ( adcs ) , the quantitative parameter of dwi , of major salivary glands pre and post rt in npc patients . 
several of these studies [ 1719 ] further found a correlation between preand post - rt changes of adc ( adcpost - pre ) and volume atrophy of pgs as well as ratios of salivary excretion fraction ( ref ) , the quantitative parameter of sgs . 
but until now , most of these initial studies have merely focused on the evaluation of pg dysfunction , whereas severity of xerostomia does not only attribute to the injury of pg but also smg [ 20 , 21 ]  . 
meanwhile , nearly all previous relative studies only compared adcs of major salivary glands at one timepoint after rt with that before rt , continuous observations are scarce . and the correlations between changes in adc and clinical parameters , such as subjective xerostomia degree and sfr , remain unclear . 
besides , to the best of our knowledge , studies assessing salivary gland dysfunction with dwi in npc patients treated with ht have not been documented . it would be interesting to investigate the radiation - induced physiological changes of irradiated pgs and smgs at a lower radiation dose by using ht . therefore , the purpose of this preliminary study was to observe the dynamic changes in adcs of both pgs 532 strahlenther onkol ( 2020 ) 196 : 530541 and smgs in npc patients 1 year post ht , to analyze whether alterations of pg and / or smg adcs correlated with mean radiation dose and changes in sfr under stimulated / unstimulated conditions at six different follow - up timepoints , to further compare adcs among patients with different subjective degrees of xerostomia . materials and methods patients study prospective registered with this number chictr1900024328 in the chinese clinical trial registry was approved by the research ethics board of the chinese pla general hospital . 
written informed consent was obtained from all eligible patients prior to participation . from july 2017 to january 2018 , 31 consecutive patients with pathologically conrmed npc who were scheduled for bilateral neck ht with curative intent were prospectively recruited in this study . 
none of them had received prior rt or surgery to the head and neck region , any previous salivary gland diseases such as sjogrens syndrome , any other medical causes of xerostomia , mri contraindications , or any metal implants in the mouth . all patients underwent six mr examinations with an identical scan protocol each time , namely 23 weeks before rt ( pre - ht ) and 1 , 3 , 6 , 9 , and 12 months after completion of rt ( 1m - post - rt , 3m - post - rt , 6m - post - rt , 9m - post - rt , 12m - post - rt )  . 
meanwhile , measurement of sfr as well as assessment of subjective degree of xerostomia were conducted an hour before each mr examination . treatment all patients were treated with induction chemotherapy followed by concurrent chemoradiotherapy . 
a two - cycle tp or tpf regimen was used in induction chemotherapy , i.e. , docetaxel ( t ) 70 mg / m2 on day 1 and cisplatin ( p ) 40 mg / m2 on days 1 and 2 ; for patients with massive tumors at the primary site , 5 - uorouracil ( f ) 700 mg / m2 on days 15 was added accordingly . 
rt was performed with ht ( tomotherapy ; accuray inc . , sunnyvale , ca , usa ) to the nasopharyngeal lesions , metastatic lymphadenopathy , and the neck lymphatic drainage areas . 
rt was delivered once daily , ve fractions per week , with a total of 30 fractions for six weeks . treatment planning was optimized on the pinnacle 3.8.0 treatment workstation ( philips medical systems , fitchburg , wi , usa ) by the reverse intensity - modulated planning systeall subjects were scheduled for a salivary gland - sparing technique to keep radiation doses to bilateral pgs and smgs as low as possible on the promise of meeting the prescription dose coverage of 95% or more to the treatment volume . 
the mean radiation dose constraints for bilateral pgs were no more than 28 gy , so do smg - spared ( ipsilateral level i b out of high - risk area )  . 
for morphologic evaluation , an axial t1 - weighted spin - echo sequence ( tr / te , 428 / 11.6 ms ) was performed using a matrix of 288 192 , a eld of view ( fov ) of 180 240 mm , and a section thickness of 5 mm with an intersection gap of 1 mthen , fast spin - echo t2 - weighted ( tr / te , 3000 / 59.5 ms ) with fat suppression was obtained in the transverse plane with a matrix of 320 224 , an fov of 180 240 mm , and a section thickness of 5 mm with an intersection gap of 1 mthis sequence was performed as a reference for the following dwi images to improve the delineation of both pgs and smgs . 
the images encompassed the area from the skull base to the level of the glottis , including the full volume of pgs and smgs . thereafter , an axial echoplanar dwi sequence was performed with a tr of 5000 ms , a minimum te of 74.6 ms , a matrix of 128 128 , and excitations . 
eleven to thirteen sections were obtained , and the acquisition time of the dwi sequence was about 2 min . strahlenther onkol ( 2020 ) 196 : 530541 image analysis the data were digitally transferred from the mri unit console to an independent linux workstation with dedicated software ( advantage workstation version 4.3 , ge healthcare )  . 
adc values were calculated using a mono - exponential model : si = s0 exp ( bi adc ) , where si is the signal intensity measured on the i - th b value image , bi is the corresponding b value , and s0 indicates the exact ( without noise ) signal intensity for b = 0 s / mm2 . all the mr images were independently analyzed and measured by two radiologists with more than 8 years of experience in head and neck mr imaging , who were blinded to all clinical information . 
the regions of interest ( rois ) were manually drawn on the largest three contiguous slices of adc images of bilateral pgs and smgs to encompass as much of the gland parenchyma as possible in reference to t2 - weighted images . 
the change rates of adcs were calculated using the following equation : adc.i / mpost - rt = .adc.i / mpost - rt adcpre - rt / = adcpre - rt ( cid : 2 ) 100% where ( i ) m - post - rt represents the exact month after completion of rt , adc ( i ) m - post - rt is the change rate of adc value at ( i ) m - post - rt compared with pre - rt , and adcpre - rt is the adc value before rt . the nal results were recorded as the mean value of two observers measurements . 
adc values of both pgs and smgs were repeatedly measured by one radiologist at an interval of 4 weeks to evaluate the intra - observer reproducibility . whole - mouth sfr measurement whole - mouth sfr measurement , one kind of sialometry , directly measures the function of salivary glands . 
patients were instructed to spit their saliva in a graded tube for 5 min , both at rest and upon stimulation by dipping citric acid of 2% concentration on the tongue tip with a cotton bud once every 20 s . 
the collected saliva volume in the two conditions was recorded and then used to calculate sfr under unstimulated ( usfr ) as well as sfr under stimulated conditions ( ssfr ) as well as their change rates using the following equation : sfr.i / mpost - rt = .sfr.i / mpost - rt sfrpre - rt / = sfrpre - rt ( cid : 2 ) 100% where sfr ( i ) m - post - rt is the change rate of sfr at ( i ) mpost - rt compared with pre - rt , and sfrpre - rt is sfr before patients were asked not to eat or drink for at least 1 h before the examination . assessment of the degree of xerostomia before each sfr measurement , patients were asked to complete a modied xerostomia - specic questionnaire which has been validated previously [ 23 ]  . 
the severity of xerostomia is classied by the summary score ( xq - sum ) : mild xerostomia , xq - sum ( cid : 3 ) 10 points ; moderate xerostomia , 10 < xq - sum ( cid : 3 ) 20 points ; severe xerostomia , xq - sum > 20 points . statistical analysis statistical analysis was performed with spss 24.0 software ( ibm corp . , armonk , ny , usa )  . 
paired two - tailed students t - tests were used to compared mean radiation doses to pgs and smgs , adcs of pgs and smgs , and sfr under different conditions at each timepoint . 
the dynamic changes of adcs and sfr , and the differences in adcs among different degrees of xerostomia were analyzed by repeated measures analysis or one - way analysis of variance with the bonferroni post - test . 
two - sided p - values less than 0.05 were considered as statistically signicant . 534 strahlenther onkol ( 2020 ) 196 : 530541 dwi images of pgs adc images of pgs dwi images of smgs adc images of smgs fig . 
1 diffusion weighted imaging ( dwi ) and apparent diffusion coefcient ( adc ) images of bilateral parotid glands ( pgs ; white solid arrow ) and submandibular glands ( smgs ; white hollow arrow ) of a 49 - year - old male npc patient at different timepoints pre and post rt . 
for both pgs and smgs , adc images illustrated a relatively slightly higher signal at 1m - post - rt and 3m - post - rt compared to that of pre - rt , with a gradually decreasing signal at 6m - post - rt and 12m - post - rt . 
meanwhile , the metastatic lymph nodes ( white arrow ) apparently disappeared after 1m - post results all subjects successfully underwent the whole therapy and follow - up mr examinations . 
the main characteristics of subjects and tumor are presented in table 1 . comparison of pgs and smgs there was no difference in mean radiation dose to bilateral pgs or smgs , whereas the mean radiation dose to smgs was signicantly higher than to pgs ( p < 0.001 ) , as shown in table 1 . 
at each timepoint , adcs of bilateral pgs were similar to each other , the same was true for bilateral smgs , while adcs of pgs were signicantly lower than those of smgs ( p < 0.05 ) , as shown in table 2 . dynamic changes of adc at dierent follow - up timepoints the change trends over time of the adc of pgs and smgs were similar , as shown in fig . 
for both ssfr and usfr , sfr1m - post - rt apparently declined from sfrpre - rt , changed little to sfr3m - post - rt , then gradually increased over time , as shown in fig . 
linear correlations were also found between mean radiation dose to smgs and adc6m - post - rt , adc9m - post - rt , and adc12m - post - rt . 
compared to patients with mild xerostomia , adc1m - post - rt and adc3m - post - rt of pgs and smgs in patients with moderate xerostomia showed no signicant differences , but adc6m - post - rt , adc9m - post - rt , and adc12m - post - rt were all higher , albeit lacking statistically signicant differences ( p > 0.05 for all ) , as shown in fig . 
stimulated salivary production is largely derived from pgs ( approximately 60% of total saliva in stimulated conditions ) , while resting or unstimulated saliva is mostly produced by smgs ( nearly 90% of total saliva in unstimulated conditions ) [ 24 ]  . 
our study using dwi to assess dynamic changes of salivary gland function over time in 1 - year post - rt and particularly to assess pgs and smgs separately , found a strong correlation between preand post - rt changes of adc and those of sfr under unstimulated / stimulated conditions as well as with the degree of subjective xerostomia . 
to the best of our knowledge , this is the rst follow - up research so far 536 strahlenther onkol ( 2020 ) 196 : 530541 ( cid : 2 ) strahlenther onkol ( 2020 ) 196 : 530541 fig . 
line graphs indicate a similar change trend over time for both pgs and smgs , i.e. , adc increased signicantly 1m - post - rt , followed by no obvious change until 3m - post - rt , and then gradually declined fig . 
line graphs indicate a similar change trend over time for both usfr and ssfr , i.e. , sfr decreased signicantly 1mpost - rt , followed by no obvious change until 3m - post - rt , and then gradually increased to explore the correlations of dwi parameters with clinical parameters containing objective sfr measurement and subjective degree of xerostomia simultaneously . pgs and smgs are composed of acinar cells , which produce saliva . 
a previous rat model study [ 25 ] observed an initial drop of acinar cell number of pgs followed by an increase in the late post - irradiation period ( 120240 days )  . regarding the dosage effect , the relationship between radiation dose absorbed by salivary glands and adcpost - pre has previously been investigated . 
 [ 18 ] found a doseresponse correlation between radiation dose to pgs as well as smgs and adcpost - pre from measurement timepoints prior to rt onset and at a mean of 6 months post rt . 
our study further showed signicantly positive correlations between radiation dose and adcpost - pre at ve timepoints from 1 month to 12 months post rt of pgs and adcpost - pre at 6 , 9 , and 538 strahlenther onkol ( 2020 ) 196 : 530541 fig . 
line graph indicating change trend over time of xq - sum shows an initial increase 1m - post - rt with subsequently minor change until 3m - post - rt and then a gradual decrease from 3m - post - rt to 12m - post - rt 12 months post rt of smgs , which indicates a dose - dependent loss of acinar cells and a continuous doseresponse effect over time . sfr measurement remains the benchmark for assessment of salivary gland function . 
this nding corresponds with the study of gupta [ 14 ] , who found a maximal decrease in ref at 3m - post - rt with then functional recovery over time in a cohort of 41 head and neck cancer patients by using quantitative sgs to assess pg function . the difference between sfr12m - post - rt and sfrpre - rt was not statistically signicant , but the differences between sfr12m - post - rt and sfr3m - post - rt of ssfr and sfr12m - post - rt and sfr6m - post - rt of usfr were signicant . 
the results indicated that both usfr and ssfr could recover nearly to the prert level 1 - year post rt , but the time to begin recovery of ssfr was ahead of usfr . one unique feature of our study is the correlation between adc and sfr under different conditions at different follow - up timepoints , which , to the best of our knowledge , has not been investigated before . 
in the study , signicant negative correlations were found between sfr9m - post - rt and adc9m - post - rt , and sfr12m - post - rt and adc12m - post - rt of pgs , as well as sfr12m - post - rt and adc12m - post - rt of smgs in the acid - stimulated condition and sfr12m - post - rt and adc12m - post - rt of smgs in the resting condition . 
the correlations were in accordance with physiological function of saliva production as mentioned above : both pgs and smgs produce the majority of saliva during stimulation , while smgs alone produce the majority of saliva while at rest . 
furthermore , the correlations manifest that dwi can not only evaluate salivary gland dysfunction post rt separating pgs from smgs , but also be quite suitable for assessing it in the late post - rt period . evaluation of the degree of xerostomia is also widely used in assessing salivary gland dysfunction clinically , and can be classied into operator - rated outcomes according to classication systems such as ctcae , the radiation therapy oncology group ( rtog ) toxicity criteria , and patientrated outcomes using questionnaires [ 28 , 29 ]  . 
but recent studies [ 30 ] have found that operator - rated outcomes might underestimate the actual degree of xerostomia and patient - rated outcomes are uniquely able to provide actual information . 
the overall change trend of xq summary scores was in keeping with that of adc , which indicates the consistence of adc changes and subjective xerostomia over time after rt . 
5 comparison of adc of pgs ( a ) and smgs ( b ) among patients with different degrees of xerostomia classied by xqsum ( mild xerostomia , xq - sum ( cid : 2 ) 10 points ; moderate xerostomia , 10 < xq - sum ( cid : 2 ) 20 points ; severe xerostomia , xqsum > 20 points )  . 
meanwhile , patients with moderate subjective xerostomia presented the tendency of higher adcs compared to those with mild xerostomia in the late post - rt period , but statistically signicant differences were lacking , which might be due to the small size of our study . 
based on this , we consider that although dwi is not sufcient to distinguish mild from moderate subjective xerostomia in the early post - rt period , it can fully distinguish severe subjective xerostomia and has the potential to differentiate mild from moderate subjective xerostomia in the late postrt period . it is estimated that at least 1 - year of follow - up is required to determine the effect of rt on xerostomia [ 32 ]  . 
additionally , the interand intraobserver reproducibility of adc of both pgs and smgs was excellent , indicating high reliability of the measurement of dwi parameters of pgs as well as smgs . this preliminary study has some limitations . 
first , despite being larger than previous dwi studies on evaluation of radiation - induced salivary gland dysfunction , the sample size was still small , especially for patients with severe subjective xerostomia . 
many more samples with different degrees of xerostomia should be included in future studies . second , our study employed three continuous slices cover540 strahlenther onkol ( 2020 ) 196 : 530541 ing the largest area of both pgs and smgs to represent the entire salivary glands for analysis rather than including all slices . 
in consideration of intra - tissue heterogeneity , earlier research [ 33 ] reported regional differences in radio - sensitivity inside the salivary glands , so sampling errors could not be avoided . 
the advanced intravoxel incoherent motion dwi ( ivim - dwi ) technique can separate contributions of diffusion and perfusion , which makes it more informative than dwi for assessing radiation - induced salivary gland damage . 
conversely , with the advantages of easily achieved fast acquisition ( usually no more than 2 min ) and simple post - processing operation , dwi is much more convenient for patients . 
last but not least , the impact of chemotherapy on salivary gland function is currently unclear and it is still an open question owing to various antineoplastic drugs , doses , and cycles . 
 [ 31 ] found that concomitant chemotherapy had no impact on xerostomia by univariate analysis in a cohort of 63 head and neck cancer patients ( 44 with npc )  . 
but more samples are needed to verify the results . conclusion this study showed that for both pgs and smgs , during 1 year of follow - up post rt , the dynamic change trends of adc were negatively paralleled to those of objective measurement ( sfr under unstimulated and stimulated conditions ) and in line with those of patient - reported subjective degree of xerostomia ( xq scores ) , indicating that dwi might be a useful modality for follow - up assessing radiation - induced physiological and functional changes of major salivary glands in npc patients . 
ma declare that they have no competing interests . ethical standards this prospective study registered with number chictr1900024328 in the chinese clinical trial registry was approved by the research ethics board of the chinese pla general hospital . 
written informed consent was obtained from all eligible patients prior to participation . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
it appears favorable to undertake further steps to investigate whether patient subgroups behave differently depending on their toxicity prole . methods we retrospectively analyzed 125 consecutive patients with non - metastasized carcinoma of the head and neck who were treated with crt ( cisplatin 40 mg / m2 weekly ) in 2013 / 2014 . 
patients who underwent 5 cycles were associated with prolonged overall survival and metastasis - free survival after crt ( p < 0.02 ; median follow - up 24 months ) , especially patients < 60 years . conclusion acute kidney injury was the most common side effect in patients 60 years , whereas leukopenia characteristically occurred signicantly more often in younger patients . 
hierzu ist wichtig , zu eruieren , ob bestimmte subgruppen von patienten ein unterschiedliches prol ihrer toxizitten aufweisen . methoden es erfolgte eine retrospektive analyse von 125 konsekutiven patienten mit nichtfernmetastasierten kopfhals - tumoren , welche eine crt ( cisplatin 40 mg / m2 wchentlich ) im jahr 2013 / 2014 erhalten hatten . 
vorgesehen waren insgesamt 6 zyklen cisplatzur statistischen analyse wurden chi2 - test , t - test , kaplan - meier - methode und logrank - test verwendet . ergebnisse sechsundachtzig patienten erreichten den geplanten 6 . 
patienten , welche 5 zyklen erhielten , wiesen ein verlngertes gesamtund metastasenfreies berleben nach crt auf ( p < 0 , 02 ; medianes follow - up 24 monate ) , besonders patienten < 60 jahre . schlussfolgerung ein akutes nierenversagen war die hugste nebenwirkung bei patienten 60 jahre , wohingegen eine leukopenie charakteristischerweise huger bei jngeren patienten auftrat . 
eine unterbrechung der cisplatin - therapie war mit einem schlechteren outcome vergesellschaftet , besonders bei patienten < 60 jahren . schlsselwrter kopf - hals - neoplasien kumulativdosis therapieadhrenz leukopenie nierenversagen berleben introduction radiotherapy plays a key role in locally advanced carcinoma of the head and neck ( hnscc )  . 
polychemotherapy was not superior to monotherapy if a platin - based cth was used , which was mostly cisplatin and less often carboplatthis led to the statement that denitive chemoradiotherapy ( crt ) with cisplatin could be the standard treatment for locally advanced hnscc [ 4 ]  . yet important questions remain unanswered . 
what needs to be to be discussed is the optimal treatment regime when using cisplatmoreover , there is no international consensus regarding the minimum recommended cumulative dose . to our knowledge , there is no study investigating the effect of concomitant cisplatin cth in patients with head and neck carcinomas under radiotherapy which also includes postoperative patients and recurrent disease . 
in recent times , more and more studies are focusing on reducing treatment toxicity or investigating its impact on quality of life , e.g. , trough therapy de - intensication in low - risk patients [ 5 ] and exploring patient - reported outcomes [ 69 ]  . 
this study has its focus on investigating the age - dependent toxicity prole of using cisplatin 40 mg / m2 weekly in relation to overall survival , local control , and metastases free survival rates . methods study population in this retrospective study , we selected consecutive patients with non - metastatic cancer of the head and neck who received crt with concomitant cisplatin 40 mg / m2 administered intravenously weekly at a large german university hospital between january 2013 and december 2014 . 
cumulative target dose was 240 mg / m2 and consisted of six cycles . patients with a denitive or adjuvant therapy regime were strahlenther onkol ( 2020 ) 196 : 515521 included , as well as patients with recurrent disease . 
before treatment initiation , baseline audiometry and dental examination were performed . radiotherapy for denitive treatment , patients were planned to receive 57.6 gy prescribed to the planning target volume ( ptv ) of the primary tumor site and the lymphatic drainage area . 
the primary tumor site as well as lymph node metastases were boosted using a simultaneously integrated boost ( sib ) up to 74 gy . planned dose in the adjuvant setting was 54 gy . 
patients with extensive nasopharyngeal carcinoma received a carbon ion ( c12 ) boost to the primary tumor site instead of a photon boost in order to spare organs at risk . 
cisplatin was not applied simultaneously to the carbon ion boost . delineation of the target volume and organs at risk was performed according to the european and north american consensus guidelines [ 10 , 11 ]  . 
mean doses for the submandibular glands and the parotid gland had to be below 39 and 26 gy , respectively [ 14 ]  . chemotherapy patients were planned to receive cisplatin 40 mg / m2 intravenously per week , with a total target dose of 240 mg / m2 . the doses were given together with 250 ml of isotonic saline . 
the antiemetic prophylaxis consisted of 1 mg granisetron , 8 mg dexamethasone , and 150 mg fosaprepitant intravenously or 125 mg aprepitant per os 2 h before starting cisplatin administration . 
on days 2 and 3 , patients received 2 mg granisetron , 8 mg dexamethasone , and 80 mg aprepitant per os ; depending on the risk factors for cisplatin - induced emesis , in some cases , aprepitant / fosaprepitant was omitted . blood values and biochemistry were checked before and after each cycle . 
in case of a leucocyte count below 3 / nl , a platelet count below 100 / nl , or glomerular ltration rate ( gfr ) using the cockcroftgault formula below 60 ml / min , the respective upcoming cycle was delayed or omitted , with no dose modication or hematopoietic stimulation ( e.g. , lgrastim ) being carried out . 
in general , there was liberal use of infusion therapy for nephroprotection . follow - up first follow - up was performed 6 to 8 weeks after completion of crt with a clinical examination by our ent department as well as a contrast uid ct or mri scan of the head and neck . 
1 cisplatin toxicity prole depending on age group and cisplatin cycle number ; a patients < 60 years ( n = 35 ) ; b patients 60 years ( n = 51 ) from then on until 5 years after crt , this procedure took place every 6 months . 
in case of suspicious ndings in examination or imaging , a biopsy was taken to conrm a possible recurrence . statistical methods statistical analyses were done using chi2 test , t - test , kaplanmeier plots and log - rank - test . 
anova with repeated measures was utilized after proving for sphericity concerning leukocyte count and gfr . overall survival ( os ) , local control ( lc ) , and metastasis - free survival ( mfs ) were represented by the time from the beginning of the chemoradiotherapy until death . 
this retrospective study was approved by the ethical committee of the university hospital . results patient characteristics from january 2013 to december 2014 , 125 patients with cancer of the head and neck received crt with cisplatin 40 mg / m2 weekly at the radiooncology department of a large german university hospital . 
for about a fth of the patients , the described crt was a denitive fractionated re - irradiation combined with a simultaneous cisplatin 40 mg / m2 weekly treatment protocol of their local recurrence . 
2 values for glomerular ltration rate ( gfr ; in cl for better comparison ) and leukocyte count decline ( p < 0.05 ) during cisplatin treatment ( cycle 0 = baseline ) strahlenther onkol ( 2020 ) 196 : 515521 fig . 
there was no signicant difference between the two age groups in terms of lc and mfs . discussion in this retrospective study of 125 patients who received crt with cisplatin 40 mg / m2 weekly , we found that especially younger patients below 60 years had a signicantly better os if at least ve cycles of cisplatin were given . 
on the other hand , in terms of concomitant cisplatin chemotherapy in the present study cohort , the united nations denition was the most appropriate cutoff value to point out the age - dependent differences in outcome and toxicity prole . a prolonged overall survival in patients with nasopharyngeal cancer who received more than 200 mg / m2 of cisplatin was shown by peng et al . 
in a recently published study consisting of over 2000 patients receiving cisplatin , age over 60 years was one of the most important predictors of later nephrotoxicity [ 20 ]  . 
this reects our ndings in this study , where 82.6% ( p < 0.01 ) of treatment cancellations due to low gfr occurred in patients who were at least 60 years old . also , the timing of cth cancellation was worthy of remark . 
a cessation of concomitant cisplatin therapy could be more or less predicted in terms of leukocyte count : the more cycles were given the lower the leukocyte count turned out . there was no cancellation of cth because of a low leukocyte count before the fourth cycle . 
concomitant cth improved locoregional control , induction cth had a greater effect on mfs [ 21 ]  . even though the mach - nc meta - analysis did not show a benet for mfs using concomitant cth in general , mfs was signicantly better in the present study in patients who received at least 5 cycles of cisplatin . local control rate in this study was better , but not signicantly , in patients receiving at least 5 cycles of cisplatin . this could be due to the rather short median follow - up of 24 months . 
on the other hand , it could be possible that the modern imrt technique compensates for a dose - reduced concomitant chemotherapy in terms of local control . predominant reasons for cancellation of cisplatin therapy were nephrotoxicity in older patients and leukopenia in younger patients . 
a recent retrospective study showed noninferiority in terms of locoregional control when using carboplatin instead of cisplatin [ 22 ]  . the administration of 100 mg / m2 cisplatin every 3 weeks is the standard protocol in north america , whereas european centers more often use 40 mg / m2 weekly [ 2325 ]  . the toxicity prole and os benet in this study provide a hint that a 40 mg / m2 weekly dose of cisplatin might not be the favorable choice for patients under 60 years . 
when applying these facts to the results of this study , younger patients might benet from an every - three - weeks schedule , since especially younger patients had less nephrotoxic side effects and a higher cumulative cisplatin dose was associated with better os . 
due to its mixed study population in terms of tumor locations and treatment concepts , larger patient cohorts are needed to be able to detect signicant differences concerning the toxicity prole in the small subgroups . 
nonetheless , since consecutive patients where included , it reects the daily clinical reality at a large german university clinic and presents an exciting outlook and reference point for further investigations . the use of concomitant pembrolizumab during radiotherapy could offer a promising scenario for future treatment of advanced head and neck cancer patients [ 3 ]  . 
however , considering possible ( lifelong ) autoimmune side effects and additional economic challenges , it is unclear whether concomitant ( cis ) platin therapy will be replaced by less toxic agents in the near future . 
having been in clinical use for decades now , there have still been stepwise improvements of cisplatin administration , e.g. , antiemetic triple therapy [ 28 ] , which are still ongoing [ 29 ]  . 
we suggest to not stop re - evaluation and improvement of conventional ( cis ) platin therapy . conclusion in this retrospective study , we investigated consecutive patients with non - metastatic cancer of the head and neck who received crt with concomitant cisplatin ( 40 mg / m2 intravenously weekly )  . 
discontinuing cisplatin during crt was associated with a decreased outcome , especially in patients under 60 years of age . strahlenther onkol ( 2020 ) 196 : 515521 conict of interest f . 
april 2020 der / die autor ( en ) 2020 hintergrund seit jahrzehnten besteht die mglichkeit einer organerhaltenden behandlung des muskelinvasiven harnblasenkarzinoms durch transurethrale tumorresektion ( tur ) und radiochemotherapie ( rct )  . 
es ist daher wichtig , immer wieder auf dieses therapiekonzept , das 1982 von den erlangern alfred sigel ( urologie ) und rolf sauer ( radioonkologie ) eingefhrt wurde , hinzuweisen und aktuelle daten zu publizieren , zumal der zustzliche einsatz der regionalen tiefenhyperthermie zur rct einen prognosesprung verspricht . 
die kollegen des universittsklinikums erlangen machen das und haben krzlich berzeugende langzeitdaten vorgelegt [ 7 ]  . patienten und methode zwischen 1982 und 2016 wurden an der strahlenklinik der universitt erlangen - nrnberg 664 patienten mit einem blasenkarzinom lediglich noch transurethral reseziert , also primr nicht mehr zystektomiert , sondern mit dem ziel des organerhalts anschlieend nur noch bestrahlt , spter radiochemotherapiert und in den letzten jahren noch zustzlich hyperthermiert . 
fr die hier kommentierte analyse wurden die therapieergebnisse bei 369 patienten mit oberchlichen high - risk - tumoren ( pta , ptis , pt1 , jeweils mit indikation zur zystektomie ) und t2 - tumoren untersucht , fortgeschrittene tumoren ( ct34 ) originalpublikation merten r , ott o , haderlein m et al ( 2019 ) long - term experience of chemoradiotherapy combined with deep regional hyperthermia for organ preservation in high - risk bladder cancer ( ta , tis , t1 , t2 )  . 
ziel war eine organund funktionserhaltende therapie bei patienten mit der herkmmlichen indikation zur zystektomie . das therapiekonzept bestand aus einer transurethralen resektion ( tur mit dem ziel einer r0 - tur ) und einer radiotherapie sowie anschlieenden salvage - zystektomie bei restoder rezidivtumor . 
die radiotherapie war von 1982 bis 1985 eine alleinige strahlentherapie ( rt ) , ab 1985 eine simultane radiochemotherapie ( rct ) mit cisplatin , spter zustzlich 5 - fu , also eine nur strahlensensibilisierende chemotherapie whrend der radiotherapie ( keine neoadjuvante oder adjuvante chemotherapie )  . 
die strahlendosis betrug 50 , 4 gy im bereich der blase und der regionalen lymphknoten in einzeldosen von 5 - mal wchentlich 1 , 80 gy , gefolgt von einem boost auf die harnblase bis 55 , 8 gy nach r0 - tur bzw . 
ab 2005 wurde whrend der strahlentherapie zustzlich 1 - mal wchentlich eine regionale tiefenhyperthermie mit einem bsd - 2000 - 3d / pc - hyperthermie - system ( rct + rht ) durchgefhrt . 
das mediane follow - up betrug 71 monate . ergebnisse 290 von 369 patienten ( 83 % ) erlebten eine komplette tumorremission bei der kontroll - tur 6 wochen nach radiotherapie . 
die cr - rate betrug 68 % nach alleiniger radiotherapie , 86 % nach radiochemotherapie und 87 % nach radiochemotherapie plus hyperthermie ( p = 0 , 037 )  . 
eine akuttoxizitt grad 3 und 4 betraf fast nur hmatologische nebenwirkungen ( leukopenie grad 3 : 25 % , thrombopenie : 6 % , grad 4 : leukopenie 4 % )  . 
relevante sptfolgen betrafen zystektomien wegen blasenschrumpfung ( 2 % , n = 6 ) und eine reduzierte blasenkapazitt < 200 ml ( 10 % ) , 5 patienten entwickelten operationspichtige darmstenosen . schlussfolgerungen der autoren die multimodale organund funktionserhaltende therapie , bestehend aus tur und radiochemotherapie , ist bei harnblasenkarzinomen sehr erfolgreich . 
die hinzunahme der regionalen tiefenhyperthermie verbessert die erfolgsaussicht auf einen blasenerhalt zustzlich . kommentar radiotherapy and organ preservation in bladder cancer : are we ignoring the evidence ? [ 3 ]  . 
dieser immer noch lesenswerte kommentar von mary gospodarowicz erschien im jahr 2002 im journal of clinical oncology anlsslich einer publikation der erlanger daten ber die organerhaltende behandlung des harnblasenkarzinoms [ 8 ]  . 
es ist erstaunlich , wie wenig sich daran in fast 20 jahren gendert hat ! zurck zum anfang : das urothelkarzinom der harnblase ( nur darum geht es ; die anderen seltenen entitten sind gesondert zu betrachten ) ist ein strahlenempndlicher tumor . 
eine wesentliche verbesserung ( aus meiner sicht der entscheidende durchbruch ) waren die ab ende der 1980er - jahre in boston und erlangen entwickelten konzepte , die die grundprinzipien einer modernen , auf funktionserhalt ausgerichteten organerhaltenden therapie bercksichtigten [ 1 , 8 ]  . 
diese therapiestrategie beinhaltet eine mglichst komplette , aber organerhaltende tumorresektion ( resektion mit adjuvanter therapie ist erfolgreicher als alleinige bestrahlung ) , danach eine simultane radiochemotherapie als wichtigster baustein zur langfristigen tumorkontrolle ( vor allem cisplatin verstrkt die strahlenwirkung relevant ) , anschlieend re - evaluierung des therapieansprechens und beschrnkung der radikal - op auf patienten mit resttumor oder rezidiv . 
die auf diese weise erreichten berlebensraten mit funktionserhalt sind gut und beispielsweise besser als beim larynxkarzinom , bei dem heute ein stimmund kehlkopferhalt angestrebt wird und bei etwa drei viertel der patienten auch gelingt . 
die simultane chemotherapie leistet einen wichtigen beitrag zur lokalen tumorkontrolle ; dies ist auch durch randomisierte studien besttigt [ 5 ]  . die zystektomie bedeutet fr viele patienten eine erhebliche belastung und einbue an lebensqualitt und ist aus meiner sicht in diesem punkt durchaus einer laryngektomie vergleichbar , auch wenn die auswirkungen fr auenstehende weniger offensichtlich sind . 
die von operativer seite als durchbruch gefeierten orthotopen ersatzblasen kommen nur bei weniger als der hlfte der patienten zum einsatz , und 10 % dieser patienten sind dann auch noch inkontinent . 
gerade fr dieses kollektiv an der grenze zwischen kurativer intention und palliativer therapie sollte deshalb ein organerhaltendes konzept mit radiochemotherapie als option der ersten wahl gelten . das besondere an den hier vorgestellten erlanger daten ist der zustzliche einsatz der hyperthermie simultan zur voll dosierten rct [ 6 ]  . 
dunst gibt an , dass kein interessenkonikt beopen access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf strahlenther onkol ( 2020 ) 196 : 576578 literatur 1 . 
efstathiou ja , spiegel dy , shipley wu et al ( 2012 ) long - term outcomes of selective bladder preservation by combined - modality therapy for invasive bladder cancer : the mgh experience . 
fahmy o , khairul - asri mg , schubert t et al ( 2018 ) a systematic review and meta - analysis on the oncological long - term outcomes after trimodality therapy and radical cystectomy with or without neoadjuvant chemotherapy for muscle - invasive bladder cancer . urol oncol 36 : 4353 3 . 
merten r , ott o , haderlein m et al ( 2019 ) long - term experience of chemoradiotherapy combinedwith deep regional hyperthermia for organ preservationin high - risk bladder cancer ( ta , tis , t1 , t2 )  . 
rdel c , grabenbauer gg , khn r et al ( 2002 ) combined - modality treatment and selective organ preservation in invasive bladder cancer : long - term results . 
scrimger ra , murtha ad , parliament mb et al ( 2001 ) muscleinvasive transitional cell carcinoma of the urinary bladder : population - based study of patterns of care and prognostic factors . 
the aim of this retrospective study was to show the validity of the lymankutcherburman ( lkb ) normal tissue complication model for thyroid gland based on clinical results . methods thyroid function was evaluated by measuring thyroid - stimulating hormone and free thyroxine serum levels before radiation therapy , 3 months after the beginning of radiation therapy , and afterwards at each follow - up visit . 
dosevolume histogram , total dose , fractionation schedule , total duration of the treatment , and other parameters were used for normal tissue complication probability calculation based on the lkb model . 
normal tissue complication probability values calculated with mean dose and lyman eud parameters showed the best correlation with our clinical ndings . conclusion empirically based modelling of normal tissue complication probability was valid for our cohort of patients . with carefully chosen parameters , the lkb model can be used for predicting the normal tissue complication probability value . keywords head and neck cancer hypothyroidism volumetric modulated arc therapy lymankutcherburman model normal tissue complication probability ( cid : 2 ) ivana kinclov kinclova@unm.sk 1 oncology centre of jessenius faculty of medicine in martin , comenius university in bratislava and martin university hospital , kollrova 2 , 03659 martin , slovakia east slovak oncology institute , inc . , rastislavova 43 , 04191 koice , slovakia institute of histology and embryology , jessenius faculty of medicine in martin , comenius university in bratislava , mal hora 4 , 03601 martin , slovakia institute of medical physics , biophysics , informatics and telemedicine , faculty of medicine , comenius university in bratislava , sasinkova 2 , 81372 bratislava , slovakia introduction head and neck cancer ( hnc ) patients represent approximately 6% of all cancer cases worldwide [ 1 ]  . 
after radiotherapy , these patients can develop serious acute and late undesired effects , which reduce patients quality of life . among these , the best well - known are xerostomia , dysphagia , or dysgeusia . 
this medical condition can be diagnosed by laboratory tests for thyroid - stimulating hormone ( tsh ) and free thyroxin ( ft4 ) levels in seruclinical hypothyroidism , dened as a reduction in ft4 with an increase in tsh , manifests as tiredness , cold intolerance , dryness of the skin , weight gain , cognitive dysfunction , constipation , hoarseness , edema , reduced hearing , myalgia and pares562 strahlenther onkol ( 2020 ) 196 : 561568 thesia , depression , menorrhagia , and arthralgia . 
subclinical hypothyroidism is characterized by elevated tsh with the presence of normal ft4 and is generally asymptomatic , although it may present with clinical symptoms such as hypercholesterolemia and accelerated atherosclerosis . 
hypothyroidism is treated by replacement of thyroxine [ 24 ]  . a systematic review of the literature on radiation - induced hypothyroidism revealed that various studies showed different incidences of hypothyroidism after irradiation of the thyroid gland , and these varied from 23 to 53% for subclinical hypothyroidism and from 11 to 33% for clinical hypothyroidism in individual studies [ 5 ]  . 
the dosevolume histogram ( dvh ) , corresponding to the percentage of organ volume covered by a specic dose , and the parameters of the model are needed for the calculation . 
according to icru 83 guidelines , dvhs are mandatory in reporting intensity - modulated radiation therapy ( imrt ) treatment plans , while ntcp and equivalent uniform dose ( eud ) are included in level 3 reporting ( i.e. , still investigative ) [ 9 ]  . 
at present , their absolute values are not used clinically to predict the outcome [ 10 ]  . in the present study , the empirical lymankutcher burman ( lkb ) model [ 11 , 12 ] was used , which is the most frequently used ntcp model . 
the set of parameters for clinical hypothyroidism as an endpoint was rst published by burman , based on emamis data : a volume parameter n = 0.22 ; a steepness parameter m = 0.26 , and d50 = 80 gy [ 13 ]  . 
bakhshandeh [ 14 ] , whose study was aimed at a patient cohort irradiated by 3d conformal radiation therapy , published the following values for the parameters : n = 0.49 ; m = 0.24 , and d50 = 60 gy , which was named by these authors lyman eud . 
the simplied mean dose model with n = 1 ; m = 0.27 , and d50 = 60 gy was also proposed in the same study . the aim of this retrospective study was to evaluate the cumulative incidence of hypothyroidism after radiotherapy in the studied group of patients . 
to the best of our knowledge , no publication has yet conrmed the lkb model parameters for hypothyroidism in patients treated by volumetric modulated arc therapy ( vmat )  . methods and materials patients a total of 245 hnc patients were treated at the university hospital martin , slovakia , from january 2014 to july 2017 . patients with both primary and postoperative radiotherapy to the head and neck region were included in the study . the patients who had known thyroid disease before treatment ( 7 patients ) , previous radiotherapy to the head and neck region , or early termination of treatment ( 57 patients ) were excluded from the analysis . 
the cut - off date for analysis of data was november 30 , 2017 . assessment of thyroid gland function the function of the thyroid gland was evaluated based on laboratory values of tsh and ft4 levels in serum before the beginning of radiotherapy , 3 months after the beginning of radiotherapy , and at each follow - up visit . 
all patients treated for hnc take part in a follow - up program which includes a visit to the otorhinolaryngologist every 34 months for the rst 2 years , then every 6 months until 5 years after treatment , and after 5 years , once a year . thyroid gland hormones in serum samples were evaluated with the unicel dxi 800 immunoassay system ( beckman coulter , brea , ca , usa )  . 
statistical software spss [ 17 ] was used for the survival analysis ( imb corp . , armonk , ny , usa )  . treatment normal tissue complication probability patients were treated using vmat radiotherapy , with or without concurrent chemotherapy . 
planning computer tomography ( ct ) scans were acquired using a 128 - slice ct scanner ( ingenuity ; philips healthcare , best , the netherlands ) in a supine position maintained with thermoplastic masks , with a slice thickness of 3 mif not contraindicated , a contrast - enhanced ct scan was performed . 
elective lymph nodes were generally treated with a dose of 59.4 gy ( ipsilateral lymph nodes , intermediate - risk ptv ) and 54.12 gy ( contralateral lymph nodes , low - risk ptv )  . 
in all patients , an adaptive radiotherapy approach was employed , which meant that after 1921 fractions of radiotherapy , a new ct scan was obtained and patients were replanned in order to deliver the dose to the ptv as planned and to spare organs at risk . 
from the dvh , the v40 , v45 , v50 , and v60 doses to the thyroid gland were calculated for the analysis . endpoints the primary endpoint of this study was the incidence of clinical hypothyroidism , i.e. , ctcae grade 2 or higher toxicity occurring 12 and 24 months from the beginning of radiation therapy . 
the secondary endpoint was cumulative incidence of hypothyroidism grade 1 or higher during the rst 2 years from the beginning of radiation therapy . patients without hypothyroidism were censored at the date of last follow - up . 
tolerance dosevolume dependence is characterized by the following relationship : d50 . ( cid : 2 ) / = d50 ( cid : 2 ) ( cid : 2 ) n ; where d50 is the tolerance dose for 50% complications for uniform whole - organ irradiation , n is the parameter to nd the eud in inhomogeneous irradiation using the dvh reduction method proposed by kutcher and burman [ 12 , 13 ] , and 0 < n < 1  . 
the parameters used in the calculation of thyroid gland ntcp grade 2 and higher are shown in table 1 . calculation of ntcp based on the lkb model assumes a dose per fraction of approximately 2 gy . 
bed was calculated by the following formula , which includes reparation and repopulation [ 22 ] : bed = d ( cid : 2 ) k.t tk / ; where ( cid : 4 ) ( cid : 5 ) df is dose per fraction , / is a tissue - specic parameter of the organ according to the linear - quadratic model , t is the total duration of the treatment in days , tk is the time of onset of repopulation from the start of radiotherapy , k is a repopulation factor expressed by k = ln2 / ( / tpot ) , where is 564 strahlenther onkol ( 2020 ) 196 : 561568 table 1 parameter sets used in the calculation of thyroid gland ntcp for complications of grade 2 or higher table 2 characteristics of patients and treatment parameters characteristics no . 
from tted parameters , for thyroid gland : k = 0.3 , tk = 49 days [ 23 ]  . ntcp values were calculated using biogray software ( koice , slovakia ) [ 24 ]  . 
correlation of calculated values with clinical results of a group of hnc patients was calculated with the corrplot package of r software [ 25 ]  . results the study group consisted of 83 patients . 
the summary of patient characteristics is shown in table 2 . median follow - up was 1.2 years as calculated by the reverse kaplanmeier method ( range 981205 days )  . 
of patients ( % ) 0 ( euthyroid ) 1 ( subclinical hypothyroidism ) 2 ( clinical hypothyroidism ) 59 ( 71.1% ) 14 ( 16.9% ) 10 ( 12.0% ) surgery did not show a statistically signicant inuence on the development of hypothyroidism . the biogray software allows for modication of model parameters . 
1 incidence of grade 2 hypothyroidism ( % ) after the beginning of radiotherapy tions with p - value > 0.05 were considered as insignicant , in which case the crosses were added to correlation coefcient values . 
in this example , ntcp was calculated with parameters of emami ( a curve with squares ) , mean dose ( triangles ) and lyman eud ( dots ) tients irradiated with highly conformal vmat radiotherapy . our parameters for the lkb model are : bed50 = 100 gy , n = 0.43 , and m = 0.24 ( lyman eud ) , and bed50 = 100 , n = 1 , and m = 0.27 ( mean dose )  . 
this result was somewhat different to the reported incidence rate of subclinical or clinical hypothyroidism 1 year and 2 years after radiotherapy in the head and neck region delivered by the imrt method , which was 33% and 44.6% , respectively [ 6 ]  . tolerance limits of vgy values for thyroid gland were summarized in the publication of emami [ 26 ]  . 
ntcp values from emamis data do not correlate with clinical ndings , because tting of parameters n and m was based on insufcient data [ 26 ]  . several authors employed models other than lkb to calculate ntcp values for hypothyroidisthe ntcp model of boomsma et al . 
the results showed that thyroid v40 > 85% ( percentage of thyroid volume receiving more than 40 gy not exceeding 85% ) signifstrahlenther onkol ( 2020 ) 196 : 561568 results also show that the thyroid gland can be described as tissue composed of functional units arranged in parallel architecture , which is shown by an n value close to 1 [ 32 ]  . limitations this study has several limitations . 
patients had a short median follow - up 1.2 years , whereas according to published studies , the median time to the onset of hypothyroidism after radiation therapy is 1.41.8 years [ 5 ]  . 
because of a low number of patients , it was not possible to perform a thorough analysis of clinical risk factors which were found to inuence the risk of radiation - induced hypothyroidism [ 33 ]  . conclusion vmat is an advanced form of intensity - modulated radiotherapy that delivers a precisely conformal 3d dose distribution during gantry rotation in a single or multiple arcs . this method allows highly conformal delivery of radiotherapy , which , with a properly dened target and when used together with image - guided radiotherapy and adaptive radiotherapy approaches , can improve treatment outcomes of cancer patients , i.e. , reduce toxicity and potentially improve loco - regional control by increasing the target dose [ 34 ]  . radiobiological models based on a linear - quadratic approach can be used effectively for calculating ntcp values of thyroid gland complications after vmat radiotherapy , provided the referenced / , d50 ( or bed50 in the case that biological effective dose is used instead of physical dose ) , n , and m values are used . we suggest that assessment of thyroid hormones should be a routine part of follow - up examinations in patients after radiotherapy in the head and neck region . 
hautmann1 marius treutwein1 antonio ernstberger4 tobias ettl5 oliver klbl1 christoph s1 matthias hipp2 ulrich neumaier3 felix steger1 silke brockmann1 received : 30 august 2019 / accepted : 14 november 2019 / published online : 29 november 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose osteoarthritis of the ankle and tarsal joints is less common than osteoarthritis of the knee or hip , but the associated disability is at least as severe as that of the other major joints of the lower limb . 
the aim of this survey was to examine the results of low - dose radiotherapy for osteoarthritis of the ankle and tarsal joints . materials and methods the analysis was performed on patients of three german radiotherapy institutions and included 66 irradiated joints . 
all analysed subgroups show a good response to radiotherapy for at least 24 months . keywords ankle ankle joint tarsal joint radiotherapy low - dose radiation introduction ankle osteoarthritis and osteoarthritis of the tarsal joints are less common than osteoarthritis of the other major joints of the lower limb . 
marien amberg , amberg , germany 3 mvz neumaier & kollegen , regensburg , germany 4 department of trauma surgery , klinikum osnabrck , osnabrck , germany 5 department of cranioand maxillofacial surgery , university of regensburg , regensburg , germany of symptomatic arthritis among the adult population , the prevalence of ankle osteoarthritis is approximately 1% of the adult population [ 13 ]  . 
end - stage ankle osteoarthritis has an associated disability which is at least as severe as that from hip or knee arthritis [ 3 , 4 ]  . in contrast to osteoarthritis of the hip , knee or ngers , the ankle is more often affected by secondary arthritis , most of the time due to a local trauma [ 4 ]  . 
the trauma could have been , for example , a fracture of the malleolus , a torsion fracture of the ankle or even a trauma of the ligaments [ 3 ]  . several therapeutic options for treatment of osteoarthritis are in use [ 2 ]  . 
the drug therapy can be systemic , for example with nsaids ( non steroidal antiinammatory 570 strahlenther onkol ( 2020 ) 196 : 569575 drugs ) , or can consist of local injections of anaesthetics or steroids [ 68 ]  . for very advanced stages , ankle arthrodesis is still the gold standard [ 4 ]  . 
especially the revision rate is quite high , and the function of the foot is still impaired [ 4 , 9 ]  . for this reason , joint - conserving therapies play a major role in treatment of ankle and tarsal osteoarthritis . 
the aim of this survey is to document the results of low - dose radiotherapy for ankle and tarsal osteoarthritis and to identify subgroups with major or minor benet from radiotherapy . patients and methods the study was approved by the ethics committee of the university of regensburg . the retrospective analysis was performed on patients of three german radiotherapy institutions . 
we identied the aetiology of the pain , registered possible risk factors for treatment efcacy and correlated them with the response . pain was documented with the numeric rating scale ( nrs )  . 
an arthroplasty was dened as end of follow - up . we did descriptive statistics , calculated median , range and interquartile range ( iqr ) of nrs for all time periods . to analyse signicant differences in the chronological sequence of nrs , the paired wilcoxon test for dependent variables was used . 
66 joints were treated , due to the fact that some patients were irradiated on both limbs . the median age of the patients was 68 years with a range from 37 to 83 years and an iqr from 58 to 74 years . 37 of the patients were female and 12 males . 
most frequently , patients suffered from arthritis of the upper ankle ( 25 joints ) followed by the lower ankle ( 19 joints ; table 1 )  . the majority of the patients had had other therapies for arthritis , mostly long - term medication with non - steroidal strahlenther onkol ( 2020 ) 196 : 569575 anti - inammatory drugs , intraarticular injections and physiotherapy . 
joints were treated with a fractionated dose of 0.5 gy ( 40 joints ) to a total dose of 3.0 gy or with a fractionated dose of 1.0 gy ( 26 joints ) to a total dose of 6.0 gy ( 24 joints ) or 5.0 gy ( 2 joints )  . 
in the majority of cases , the treatment time was 2 weeks ( median 14 days , iqr 12 to 17 days )  . 27 of the joints received a second course of radiotherapy , most of the time within a 6to 12 - week interval after the initial radiation course . 
male and female patients , older or younger than 68 years ( median age of our sample ) , had a signicant reduction in pain ( p < 0.05 for all categories and the entire follow - up )  . 
patients with a duration of pain of more or less than 12 months as well as more or less than 36 months had no signicant difference in response rates . patients were analysed separately for different joints affected by osteoarthritis . 
with less than 60 patients in each study , the statistical power is somewhat limited . there are many retrospective and some prospective studies strongly indicating radiotherapy to be an effective treatment for osteoarthritis . 
for the ankle and tarsal joints , as for other major joints of the lower limb , there is a statement in the guideline that there is a lack of specic literature and therefore no recommendation can be given . the prevalence of osteoarthritis of the ankle and tarsal joints is less frequent than that of the knee or hip . 
nevertheless , the grade of disability induced by osteoarthritis of the ankle is at least as severe as that induced by coxarthrosis [ 3 , 4 , 9 ]  . 
for this reason , joint - conserving therapies have a high priority in the treatment of osteoarthritis of the ankle and tarsal joints . to our knowledge , this sample is the rst in which radiotherapy of osteoarthritis of the ankle and tarsal joints has been examined specically . 
to our knowledge , it is the largest sample published so far . strahlenther onkol ( 2020 ) 196 : 569575 table 2 published studies including patients with osteoarthritis of the ankle or tarsal joints author year joints response rate ( % ) complete or very good response ( % ) partial response ( % ) fried [ 32 ] toschke [ 33 ] cocchi [ 34 ] hess et al . 
furthermore , it is missing important information like the number of joints treated ( [ 40 ] ; table 2 )  . the clinical parameters of the patients in our sample seem to be representative for a collective of patients with osteoarthritis of the ankle [ 3 , 33 , 34 ]  . 
especially the high rate of posttraumatic osteoarthritis , the median age of 68 years and the gender distribution seem to be typical for this disease . the radiation technique and dose concept are equivalent to the recommended concept of the german cooperative group on radiotherapy for benign diseases . 
most of the published samples of osteoarthritis , especially the published samples of the last decades , were treated this way [ 31 ]  . radiotherapy of osteoarthritis of the ankle and tarsal joints has proven benecial to our sample . 
it seems to be unlikely that this missing minor information would change the major results and therefore the message of this survey . the median pain level on the nrs decreases with time and seems to reach a stable low level 6 months after the end of radiotherapy . 
the median follow - up of 31 months allows a statement on long - term results . most of the patients have a response to radiation and about one fth of the patients are free of pain or score very low pain with nrs 1 during the long - term follow - up period . 
this effect lasts for at least 2 years . the overall response rate of our sample ( approximately 65 to 70% ) is within the range or slightly lower than that of most published studies for osteoarthritis of other joints . however , the rate of patients free of pain seems to be slightly lower than for other locations [ 13 , 14 , 30 ]  . 
one possibility for this nding might be the other aetiology of osteoarthritis of the ankle ( posttraumatic ) or the signicant stress on the ankle and tarsal joints in everyday life . all analysed subgroups had a benet from radiotherapy , especially the patients with osteoarthritis of the upper ankle , the lower ankle and the tarsal joints as well as the patients with idiopathic or posttraumatic osteoarthritis . 
for other nonmalignant diseases , we would recommend applying a single dose of 0.5 gy to a total dose of 3.0 gy for reasons of radiation protection [ 4143 ]  . conclusion radiotherapy of osteoarthritis of the ankle and tarsal joints seems to be an effective treatment without relevant side effects . 
zielsetzung der hier diskutierten arbeit war die evaluation der akuten nebeneffekte einer ultrahypofraktionierten stereotaktischen radiotherapie ( sbrt ) mit 5 fraktionen im vergleich zu einer normal oder leicht hypofraktionierten radiotherapie . patienten und methoden patienten mit einem adenokarzinom der prostata und niedrigem oder intermedirem risikoprol ( gleason 4 + 3 ausgeschlossen ) wurden in 37 zentren im verhltnis 1 : 1 randomisiert , und zwar entweder einer normal fraktionierten ( 39 2 gy bis 78 gy ) bzw . 
leicht hypofraktionierten ( 20 3 , 1 gy bis 62 gy ) oder einer stark hypofraktionierten sbrt mit 5 fraktionen zu 7 , 25 bis 36 , 25 gy ( appliziert in 12 wochen ) zugeordnet . eine androgendeprivation war nicht zulssig . 
fr die hier zu diskutierende auswertung der akuttoxizitt wurde der koendpunkt maximale grad - 2 - akuttoxizitt nach rtog an rektum ( gi ) , urethra und blase ( gu ) bis zu 12 wochen nach rt evaluiert . ergebnisse von 2012 bis 2018 wurden insgesamt 874 mnner mit prostatakarzinom randomisiert , davon 441 der konventionell bzw . 
intensity - modulated fractionated radiotherapy versus stereotactic body radiotherapy for prostate cancer ( pace - b ) : acute toxicity ndings from an international , randomised , open - label , phase 3 , non - inferiority trial . 
die maximale akute gi - toxizitt vom grad 2 erreichten 53 ( 12 % ) patienten in der konventionell oder leicht hypofraktionierten gruppe und 43 ( 10 % ) patienten in der extrem hypofraktionierten gruppe ( 95 % - ci 6 , 2 bis 2 , 4 ; p = 0 , 38 )  . 
die maximale gu - toxizitt vom grad 2 wurde von 118 ( 27 % ) der patienten in der konventionell oder leicht hypofraktionierten gruppe und von 96 ( 23 % ) in der extrem hypofraktionierten gruppe berichtet ( 95 % - ci 10 , 0 bis 1 , 7 ; p = 0 , 16 )  . schlussfolgerung der autoren eine substanzielle verkrzung der behandlungszeit auf 12 wochen mit extremer hypofraktionierung ( sbrt ) fhrt nicht zu erhhter akuttoxizitt . kommentar man darf dem royal marsden hospital sowie den afliierten spitlern in england und kanada zur qualitativ hochwertigen durchfhrung dieser multizentrischen studie [ 1 ] gratulieren , die mit relativ anspruchsvollen technischen randbedingungen durchaus beachtlich konzipiert war . 
diese details sind den supplementary tables zu entnehmen und beinhalten beispielsweise dosis - constraints fr das rektum ( v36gy < 1 ccm ) im rahmen der sbrt , wie sie uns beispielsweise aus der gynkologischen brachytherapie vertraut sind . 
die initial wohl ausschlielich mit dem cyberknife - system intendierte sbrt wurde im verlauf der studie offenbar problemlos auf die beschleunigerbasierte vmat ( volumetrische modulierte rotationsbestrahlung ) bernommen , sodass 60 % der sbrt - patienten mit vmat unter entsprechender igrt ( bildgefhrte strahlentherapie ) und zuhilfenahme von goldmarkern ( 73 % ) behandelt werden konnten . dennoch bleibt die frage : sehen wir in unserer klinischen routine wirklich eine rate an akuter gu - toxizitt strahlenther onkol ( 2020 ) 196 : 674675 von knapp 30 % , wie sie hier faktisch in beiden armen beobachtet wurde ? eine rtog - grad - 2 - toxizitt ist nichts banales ( medical management indicated )  . 
von amerikanischen studiengruppen [ 3 ] werden raten von lediglich 1516 % an akuter gu - toxizitt nach normal fraktionierter rt mit dosen bis zu 79 gy ( ed 1 , 8 gy ) beschrieben . 
auch die raten an akuter gi - toxizitt bewegten sich dort nur zwischen 5 und 7 % , whrend der pace - b trial von 10 bis 12 % berichtet . 
auch hier erhellt ein blick in die details der supplementary tables [ 1 ] : mehr als 70 % der patienten im standardarm der paceb - studie wurden nmlich hypofraktioniert mit 20 3 , 1 gy ber 45 wochen bestrahlt . dass nach einer ultrafraktionierten sbrt ( 42 , 7 gy in 7 fraktionen ) eine erhhte akuttoxizitt an urethra und blase zu erwarten ist im vergleich zur wirklich klassisch konventionell fraktionierten rt ( bis 78 gy in 39 fraktionen ) , wurde krzlich von widmark et al . 
brand dh , tree ac , ostler p , van der voet h , loblaw a , chu w , ford d , tolan s , jain s , martin a , staffurth j , camilleri p , kancherla k , frew j , chan a , dayes is , henderson d , brown s , cruickshank c , burnett s , duffton a , grifn c , hinder v , morrison k , naismith o , hall e , van as n ( 2019 ) pace trial investigators.intensity - modulatedfractionatedradiotherapy versus stereotacticbodyradiotherapyforprostatecancer ( pace - b ) : acutetoxicityndingsfrom an international , randomised , open - label , phase 3 , noninferioritytrial . 
michalski jm , moughan j , purdy j , bosch w , bruner dw , bahary jp , lau h , duclos m , parliament m , morton g , hamstra d , seider m , lock mi , patel m , gay h , vigneault e , winter k , sandler h ( 2018 ) effectof standard vs dose - escalated radiation therapy forpatientswith intermediate - risk prostate cancer : the nrg oncology rtog 0126 randomized clinical trial . 
widmark a , gunnlaugsson a , beckman l et al ( 2019 ) ultra - hypofractionated versus conventionallyfractionatedradiotherapyforprostatecancer : 5 - year outcomesofthehypo - rt - pc randomised , noninferiority , phase 3 trial . 
associations of hc in anterior and posterior rectal walls ( arw , prw ) with lcp , acute endoscopic ( aep ) and acute clinical proctitis ( acp ) were statistically evaluated considering as explicative variables the patient general characteristics and the hc . results the mean patients follow - up was 123.5 months ( 24209 )  . 
the median prostatic dose was 72 gy ( 2 gy / fraction )  . for the 41 and 29 patients the arw and prw doses were 64 and 49 gy vs . 
the univariate ( p = 0.02 ) and kaplanmeyer methods ( p = 0.007 ) showed that the gland ( or crypts ) loss in the arw was signicantly associated with lcp . 
to reduce this complication with conventional fractionation , we suggest keeping the mean dose to arw ( cid : 2 ) 4852 gy . keywords radiation proctitis prostate cancer radiotherapy radiotherapy complications rectum vmat ( cid : 2 ) franco campostrini , md fcampostrini@aliceposta.it ( cid : 2 ) andrea remo , md remino76@yahoo.it manuel zorzi , md manuel.zorzi@azero.veneto.it giulia capodaglio , scd giulia.capodaglio@azero.veneto.it alberto buffoli , md radioterapia.icsan@grupposandonato.it gaia moretti , m ph radioterapia.icsan@grupposandonato.it barbara della monica , m ph radioterapia.icsan@grupposandonato.it giuseppe verlato , phd giuseppe.verlato@univr.it 1 department of radiation oncology , mater salutis hospital , legnago , italy 2 department of pathology , mater salutis hospital , via gianella 1 , 37045 legnago , italy 3 veneto tumour registry , azienda zero , padova , italy epidemiological department , azienda zero , padova , italy 5 radiotherapy department , istituto clinico s . 
anna , brescia , italy 6 unit of epidemiology and medical statistics , university of verona , verona , italy 618 strahlenther onkol ( 2020 ) 196 : 617627 assoziation zwischen akuten histopathologischen vernderungen der rektumwnde und einer spten radiogenen proktitis nach strahlentherapie des prostatakarzinoms zusammenfassung zielsetzung der einuss akuter histopathologischer vernderungen ( hv ) des rektums auf die entwicklung einer spten klinischen proktitis ( skp ) nach perkutaner strahlentherapie ( rt ) des prostatakarzinoms ist kaum untersucht und war primrer endpunkt dieser prospektiven studie . methoden bei 70 patienten wurden 15 hv in frhen biopsien des rektums nach rt identiziert , wobei 41 patienten mit einer konventionellen 2 - dund 29 patienten mit einer 3 - d - konformalen technik bestrahlt wurden . 
die assoziationen von hv in den anterioren und posterioren rektumwnden ( arw , prw ) mit skp , akuter endoskopischer ( aep ) und akuter klinischer proktitis ( akp ) wurden statistisch evaluiert , wobei die allgemeinen eigenschaften der patienten und die hv als erklrende variablen herangezogen wurden . ergebnisse das durchschnittliche follow - up betrug 123 , 5 monate ( 24209 monate )  . 
die univariate analyse ( p = 0 , 02 ) und der kaplan - meier - test ( p = 0 , 007 ) zeigten , dass ein verlust von drsen ( oder krypten ) im bereich der arw signikant mit der skp korrelierte . 
in der multivariaten analyse korrelierten aep statistisch signikant mit hmorrhoiden ( p = 0 , 014 ) und neutrophilie in arw ( p = 0 , 042 )  . schlussfolgerungen frh nach der rt ist ein erheblicher verlust an drsen im bereich der arw prdiktiv fr eine skp . um diese komplikation bei konventioneller fraktionierung zu vermeiden , empfehlen wir , im bereich der arw die mittlere dosis im bereich der arw ( cid : 2 ) 4852 gy zu halten . schlsselwrter radiogene proktitis strahlentherapie des prostatakarzinoms strahlentherapieassoziierte komplikationen rektum vmat introduction in spite of the latest advances in external radiotherapy ( rt ) for prostate cancer , rectal toxicity remains a major clinical concern . 
indeed , according to a selection of recent randomized or prospective studies , radiation - induced late clinical proctitis ( lcp ) ( i.e. , established only clinically , beyond 6 months after rt ) grade 2 ( g2 ) or g3 occurs in the range of 417.7% [ 16 ] and < 13.3% [ 2 , 3 , 7 ] , respectively , of cases treated with conventional ( 1.82.0 gy / fraction ) and moderate hypofractionated rt ( 2.44.0 gy / fraction )  . 
for extreme hypofractionated rt ( sbrt ) ( 610 gy / fraction ) , the incidence of g2 cases is nil or 1% , while g2 toxicity , which can nevertheless affect the patients quality of life , is reported in 120% of cases [ 8 , 9 ]  . 
when also considering cases of g1 toxicity , overall impact of chronic symptoms has been reported in up to 18% of cases [ 10 ] while clinical and dosimetric predictive factors of late radiation proctopathy have been extensively studied and illustrated [ 11 , 12 ] , the basic histological abnormalities that can lead to this syndrome are still not well explored . the primary purpose of the present study was to prospectively analyze the association between rectal histopathological changes on completion of rt and the occurrence of lcp in a consecutive series of patients treated for prostate cancer . 
the analysis of the same associations with radiationinduced acute clinical proctitis ( established only clinically , within 3 months of the completion of rt ) and endoscopic proctitis ( ascertained by proctoscopy clinically ) were the secondary end points . methods as previously reported [ 13 ] , from january 1997 to march 2009 , a series of 130 patients with prostate cancer underwent anterior and posterior rectal wall biopsies , within 90 days ( median 6.0 days , standard deviation 12.4 ) from the completion of rt , in anatomic points corresponding to the prostatic target . 
specimens were xed in a 10% solution of neutral buffered formalin parafn , embedded , sectioned , and stained at 4 m with hematoxylin and eosin ( h&e ) for histological assessment . six - monthly patient follow - ups were scheduled during the rst 3 years and at 1 - year intervals thereafter . 
this investigation was approved by the local health authorities and informed written consent was obtained from all patients . at the time of the research , histological material was available from 84 patients ; however , 14 specimens were excluded due to their inadequate quality . 
in short , on a set of ct images of patients in supine position , the prostate ( plus seminal vesicles in a few cases ) and the organs at risk ( i.e. , empty rectum from the middle anal canal to the sigmoid junction , bladder and femoral heads ) were contoured . 
ptv was established by adding a 10 mm expansion in any direction to the ctv ( dened as the entire prostate seminal vesicles ) except for 6 mm posteriorly and a further 5 mm margin to account for beam penumbra . 
all treatment was administered with the classic four - eld box technique using 6 mv photons delivered by two siemens linac : mevatron for the 41 patients with cv 2d - rt and primus for the 29 patients undergoing 3d - crt . 
doses were calculated at icru ( international commission on radiation units ) point , which was located in full prostatic volume or in the prostatic bed ( in cases of prostatectomy ) in 96% of cases . 
due to a 2009 updating of our institutional archives , the treatment plans of the 29 patients were not retrievable for this research in order to separately calculate the mean doses of the anterior ( arw ) and posterior ( prw ) rectal walls . 
in short , starting from 2012 , we considered the rst 10 patients , with minimum 3 - year follow - up , irradiated for prostate cancer at this institution and the technical characteristics of the abovementioned 29 3d - crt plans were faithfully reproduced to create a dummy treatment . 
the arws were contoured ( 35 mm of rectal wall until midline , from the upper and lower points of rectum delineation ) and the nal plans were reprocessed by a tps eclipse for a linac dhx ( rapidarc ) , and 6 mv photons . 
the prw mean doses were obtained from the relative dvhs ( dosevolume histograms )  . the prescribed dose to the icru point was 72 gy ( 2 gy / fraction )  . 
the anterior rectal wall ( contour blue ) mean dose was 49 gy to be the respective halves of the rectum considered as an ideal cylinder . furthermore the real rectal doses of these previously treated 10 patients were re - calculated by adding the arw contours . 
the vmat technique ( volumetric - modulated arc radiotherapy ) had been used with two 360 arcs and cone beam ct support , delivering 70 gy in 28 fractions on the target with a hypofractioneted simultaneous integrated boost ( sib )  . 
the preliminary outcomes for these 10 patients are also included here . histological changes and their scoring blind revision of all the slides was performed by two expert gastrointestinal pathologists who initially identied a series of 15 histological changes ( hc ) representative of acute histological proctitis according to the nomenclature adopted from a specic literature , where more detailed descriptions can be found [ 1921 ]  . 
these elements were the following : neutrophilic , eosinophilic , lymphoplasmacytic , macrophage inltrate , nuclear atypia , gland ( or crypt ) loss , mucin depletion , brosis of lamina propria , brosis of submucosa and brosis of perirectal fat , which were scored with three degrees of intensity ( absent , moderate presence , high presence ) and eosinophilic microabscess , neutrophilic microabscess , erosions / ulcers , gland disarray , gland distortion , for whom two degrees of intensity ( absent or present ) were judged more appropriate . 
for neutrophilic and eosinophilic inltrate the terms moderate and high morphologically corresponded to an interor intraglandular presence . diagnosis and scoring of radiation - induced proctitis the diagnoses of radiation - induced acute clinical proctitis ( acp ) and late ( or chronic ) clinical proctitis ( lcp ) were dened by two radiation oncologists according to the rtog / eortc scoring [ 22 ] plus our minor additions . 
grade 2 : excessive rectal mucus or intermittent bleeding responding to simple outpatient management with lifestyle ( performance status ) unaffected . urgency and / or incontinence and / or pain with lifestyle impairment . 
grade 3 : obstruction or bleeding requiring hospitalization for diagnosis or minor surgical intervention . grade 4 : necrosis or stula requiring major surgical intervention or prolonged hospitalization . the presence of radiation - induced acute endoscopic proctitis ( aep ; our personal denition for this research ) was established by the two skilled gastroenterologists , who had performed the proctoscopies , based on both the vienna rectoscopic score [ 18 ] and the esge ( european society for gastrointestinal endoscopy ) classication [ 13 , 23 ]  . 
hence aep was diagnosed in the presence of at least one of the following six signs at proctoscopy : ( 1 ) multiple teleangectasias , ( 2 ) diffuse congested mucosa , ( 3 ) diffuse hyperemia , ( 4 ) multiple micro , - ulcerations or a single ulceration > 1 cm2 , ( 5 ) multiple petechiae , and ( 6 ) organic stricture . statistics we used the mcnemar test to compare the differences of the histological changes ( hc ) between the anterior and postestrahlenther onkol ( 2020 ) 196 : 617627 table 2 technical and dosimetric characteristics of the three different treatments treatment general data dose to icru point ptv : ctv expansion ( mm ) patients ( n ) periods of treatment plans linac , energy mean rectal dose ( gy ) % dose vs . 
a patients series of general characteristics and the mentioned hc were the explicative variables ( ev ) statistically analyzed to establish their association with the development of the three types of proctitis here considered . the quality of information about other ev ( use of anticoagulants , diabetes , hypertension ) was low and therefore were excluded from the analysis . 
the associations between these ev and both acute and endoscopic proctitis were analyzed at the univariate level through the mantelhaenszel 2 test , or by the fishers exact test when three grades of hc were present and subsequently with a multivariate logistic regression model . 
for the associations between all the ev and late clinical proctitis ( lcp ) , the univariate cox regression test was used and the parameter signicance was evaluated by the probability ratio test . 
analyses were performed with sas 9.4 statistical software ( sas institute , cary , nc , usa )  . results mean follow - up of surviving patients was 123.5 months ( range 24209 months )  . 
table 1 shows the general characteristics of all 70 patients , overall as well as for those who developed any acute or late proctitis . dosimetry for all 70 cases the median dose at the icru point was 72 gy ( range 7074 gy )  . in the 41 patients treated with conventional ( cv ) 2d - rt the median isodose lines crossing the anterior and posterior rectal walls ( arw and prw ) turned out to be 64 gy ( range 5672 gy ) and 49 gy ( range 4256 gy ) respectively , while the mean rectal dose was not calculable . 
table 2 includes all data concerning the three categories of conformational treatment above illustrated . general histological changes the inammatory and degenerative histological changes ( hc ) found are listed in table 3 , and exemplied in fig . 
on the whole , 80% of patients had bleeding while the remaining 20% complained of urgency and / or incontinence and / or paat univariate cox test no signicant associations were detected among patients who developed late toxicity with respect to general patient characteristics , thereby no multivariate analysis was performed . acute endoscopic and clinical proctitis took place in 14.3% ( 10 / 70 ) and 55.7% ( 39 / 70 ) of patients , respectively . strahlenther onkol ( 2020 ) 196 : 617627 fig . 
a biopsy of a mucosa with normal architectural morphology ( hematoxylin and eosin [ h&e ] , 100 )  . b demonstration of conspicuous gland ( or crypt ) loss , and evanishing glands ( black arrows ) , plus mucin depletion ( yellow arrow ) , associated with an interglandular inammatory inltration ( h&e , 200 )  . 
gland loss was considered high when more than one eld ( 200 ) showed this histology . c some nuclear atypias ( yellow arrow ) and a microabscess of granulocytes in an evanishing gland ( black arrow ) ( h&e , 200 )  . 
d a marked cryptic eosinophilic microabscess ( black arrow ) ( h&e ; 400 ) at the univariate level while the acute endoscopic damage was statistically more frequent in patients with hemorrhoids and in those treated with 70 gy and cv 2d - rt , by multivariate analysis this association was conrmed only with hemorrhoids ( p = 0.014 , table 1 )  . 
indeed the risk of late radiation proctitis at 2 , 5 and 10 years was 20% ( 95% ci 941% ) , 25% ( 95% ci 1249% ) and 32% ( 95% ci 1656% ) , respectively , among patients with gl vs . 
considering the posterior wall only mucin depletion achieved a borderline signicant association with the occurrence of late proctopathy ( p = 0.059 , not shown )  . at univariate level patients with the endoscopic form of acute proctitis had signicantly more neutrophilic inltration , mucinous depletion and neutrophilic microabscesses in the anterior wall than patients with normal mucosa ( table 3 ) and the same histological ndings were signicantly higher posteriorly , ( p = 0.005 , p = 0.027 and p = 0.001 , respectively ) , as well as a gl ( p = 0.049 ) ( not shown in table 3 )  . 
conversely , none of the histological injuries , in either of the walls , was associated with acute symptoms . 624 strahlenther onkol ( 2020 ) 196 : 617627 cular bed to the bowel cavity and this process could be predictive of late rectal toxicity [ 31 ]  . regarding the category of degenerative changes , in our specimens no signs of brosis , which is generally dened a slow and delayed phenomenon , were recognizable . 
in contrast , traces of this mucosal and submucosal alteration were noted by some authors in the acute phase after rt [ 21 , 26 , 28 , 30 ]  . 
this change [ 20 , 21 , 29 ] could represent the evolution of vascularendothelial damage that has been traditionally recognized to play a prominent role in the pathogenesis of acute and late clinical symptoms of rectal damage [ 12 , 28 ] and is similar to the late stage of ischemic colitis . 
finally , in agreement with the reduced exposure to radiation , none of the changes discovered in the posterior rectal wall turned out to be a prognostic factor for late symptoms g2 , both with plain cv 2d - rt [ 15 , 17 ] and 3d - crt treatments [ 24 ]  . secondary endpoints in the patients a signicant association of neutrophilic inltration in the anterior rectum with acute endoscopic signs of proctitis has been ascertained by the multivariate analysis , thus , conrming the intense inammatory process of the rectal wall which lies very close to the posterior prole of the prostate and is at major exposure to the risk of radiation damage . 
conversely no association of the histological abnormalities ascertained with acute symptoms was found , conrming the insidious nature of late proctitis that may become clinically manifest when the damage is irreparable and clinical interventions can have only a symptomatic effect . clinical implications for conformational rt of prostate cancer , a range of dvh ( dosevolume histograms ) to protect whole rectum have been recommended [ 11 , 32 ]  . 
3 cumulative risk of late clinical proctitis ( lcp ) according to the presence of gland loss discussion among the 70 patients with prostate cancer in this study , with a mean follow - up of more than 10 years , the onset of radiation - induced late clinical proctitis ( lcp ) g2 was recorded at an average time of 33 months since the completion of rt and in about a third of cases the symptoms occurred after 60 months . 
other authors evaluating large series of patients with long - term follow - up found no improvement [ 4 ] or even a continuous increase of number of patients affected by delayed proctitis [ 3 ]  . 
in the current research , the analysis of mutual associations among histological injuries , rectal doses received by the patients and the delayed proctitis is new information , potentially more relevant to understand the pathogenesis of this type of proctopathy . basic histological changes in our series of 70 specimens , the most representative cells were , in decreasing order : lymphocytesplasma cells , eosinophils , macrophages and neutrophils which are characteristic of an acute inammatory process . 
postradiation mucosal abundance of eosinophils is the most constant histological change ( hc ) reported in the literature , as shown in table 4 [ 20 , 21 , 2530 ]  . 
a specic causal role has been experimentally proposed only for neutrophils , in the assumption that in acute intestinal disorders they transmigrate from the vasstrahlenther onkol ( 2020 ) 196 : 617627 table 4 present and previous research evaluating rectal doses of radiation and related histopathological changes author , year [ ref . ] patients primary malignancy dose to primary malignancy present study prostate 7074 gy prominent mucosal hc bladder , cervix not specied ( approximately 3540 gy to rectum ) rectum 45 gy sigma - rectum 10 patients : 15002500 r 1 patients : 150 r pelvic malignancies 6 patients : not specied 4 patients : 5088 gy bladder , prostate 5052.6 gy prostate , bladder , endometrium 5466 gy prostate 7274 gy rectum 34 patients : 25 gy 18 patients : 45 gy gelfand md 1968 [ 25 ] tepper m 1968 [ 26 ] weisbrot im 1975 [ 27 ] haboubi ny 1988 [ 28 ] sedgwick dm 1994 [ 29 ] hovdenak n 2000 [ 20 ] karamanolis g 2013 [ 30 ] leupin n 2002 [ 21 ] hc histopathological changes 1 r = 0.0099 gy lymphoplasmacyticeosinophilicmacrophagic inltration gland ( or crypt ) loss decreased mucus production epithelial changes eosinophilic crypt abscesses neutrophilic depletion epithelial changes decreased mucus production eosinophilic cryptabscesses epithelial changes decreased mucus production some submucosal brosis eosinophilic inltration with microabscesses neutrophilic depletion epithelial changes eosinophilic inltration epithelial changes fibrosis of lamina propria eosinophilic inltration with microabscesses crypt loss eosinophilicneutrophilic inltration with microabscesses decreased mucus production epithelial changes gland loss neutrophilic inltration with microabscesses epithelialglandular changes fibrosis eosinophilic inltration with microabscesses neutrophilic depletion epithelial changes fibrosis , gland loss to 60% with doses to the arw less than 70 gy and beyond 75 gy , respectively , in 154 patients treated with cv 2d - rt . the prevention of lcp is crucial when doses of 80 gy to the prostatic target are given , or in patients undergoing a regimen of re - irradiation who are burdened with a high incidence of g2g3 proctitis [ 34 ]  . 
since in the 70 patients a substantial loss of glands in the mucosa of the anterior rectum with doses 60 gy was predictive of lcp g2 , it seems appropriate to maintain a dose level signicantly lower ( through specic contouring ) to decrease the risk of anatomical damage . 
thus , the rear wall should be subject to an even lower or nil risk of toxicity , due to the obvious dosimetric decline in the anteriorposterior direction , ranging from 17 to 35% ( [ 24 ] , table 2 )  . 
in this regard , it has been shown that xed eld imrt ( intensity modulated radiation therapy ) can deliver 76 gy to the target without exceeding the limit of 54 gy to the arw [ 24 ]  . as for toxicity , in patients given imrt with conventional or hypofractionated schemes , a pool of recent randomized trials shows percentages of g2 proctitis ranging from 4 to 21% [ 13 , 5 , 6 ]  . 
the more recent and advanced vmat ( volumetric modulated arc radiotherapy ) is a dynamic technique that is rapidly replacing imrt in radiotherapy departments . vmat can provide highly conformal treatment with dose delivering times signicantly lower than using imrt [ 35 ]  . however , in the eld of prostate cancer the difference in terms of critical organs sparing is not that clear between the two techniques . 
in a recent randomized trial of 118 patients treated with ultrahypofractionated wmat / imrt techniques the long - term 626 strahlenther onkol ( 2020 ) 196 : 617627 rectal toxicity g2 was 1% [ 36 ]  . 
additionally , in the 10 patients included in this study who were irradiated by vmat with a bed2 of 78 gy to the target and at the 3 - year follow - up , no cases of cancer relapse or rectal toxicities were recorded . 
in these patients the mean doses on the anterior rectal walls was 46 ( 4 ) gy , thus , supporting the possibility of maintaining a safe dose on the rectum , while radically treating the prostate cancer . brachytherapy ( bt ) is conceptually a powerful means for increasing the dose to the prostatic target while minimizing intestinal toxicity . 
indeed one current dose - constraint for rectum is a bed2 ( cid : 2 ) 75 gy to a small anterior volume ( cid : 2 ) 2 cc , around which the dose rapidly falls . 
ldr ( low dose rate : < 2 gy / h ) and hdr ( high dose rate : > 12 gy / h ) bt regimens may be offered as monotherapies to low risk and lowintermediate risk patients and , as regards the outcomes , not randomized trials of large series reported a rare incidence of late proctitis , ranging from 0.8 to 2% , but including mostly grade 3 toxicities [ 37 , 38 ]  . 
conversely , the most evident limitations are the uncertainties in re - evaluating rectal dosimetry , which depend on the kind of techniques and equipment used during treatment . conclusions radiation - induced late clinical proctitis ( lcp ) is a progressive and insidious proctopathy requiring long - term followup . 
in the 70 patients of this investigation irradiated for prostate cancer , a substantial gland loss in the mucosa of the anterior rectal wall after delivering 60 gy was a signicant predictor of lcp g2 . 
von klot2 roland merten1 received : 14 november 2019 / accepted : 23 january 2020 / published online : 10 february 2020 the author ( s ) 2020 abstract purpose this retrospective study aims at investigating the effects of moderately hypofractionated radiation therapy ( hrt ) on acute and late toxicities as well as on early biochemical control and therapeutic efciency compared to conventional radiation therapy ( crt ) in prostate cancer . patients and methods we analyzed 55 hrt patients irradiated with the total dose of 60 gy in 20 fractions delivered over 4 weeks . 
external beam radiation therapy ( ebrt ) was conducted using daily image - guided ( cone beam ct ) volumetric modulated arc therapy ( vmat ) and a simultaneously integrated boost ( sib ) for both groups to protect the rectuacute toxicities were evaluated according to common terminology criteria for adverse events ( ctcae ) v5 , whereas chronic toxicities were assessed in accordance with lent - soma . 
in addition , we calculated average treatment effects ( ate )  . thereby , propensity score matching ( psm ) based on nearest - neighbor matching considering age , comorbidities , and risk stratication as covariates was applied . 
the statistical analysis was conducted using stata 14.2 ( statacorp llc , tx , usa )  . results as conrmed by the descriptive tests , the ate revealed that the intensity and occurrence of urinary frequency ( p = 0.034 ) and proctitis ( p = 0.027 ) signicantly decreased for the hrt group , whereas all other acute toxicities did not differ signicantly between the hrt and crt groups . 
also , no signicant difference was found regarding the decrease in prostate specic antigen ( psa ) after a median follow - up of 13 months ( range 228 months ) , which indicates biochemical freedom from progression . conclusion hrt offers several medical and economic advantages and should therefore be considered as a useful alternative to crt . keywords localized prostate cancer moderately hypofractionated radiotherapy simultaneous integrated boost genitourinary toxicity gastrointestinal toxicity introduction whilst a variety of different treatment options for localized prostate cancer ( lpca ) exist , external beam radiation ( cid : 2 ) stratos vassis stratos.vassis@outlook.de 1 department of radiation oncology , hannover medical school , carl - neuberg - str . 
1 , 30625 hanover , germany institute for environmental economics and world trade , leibniz university , knigsworther platz 1 , 30167 hanover , germany therapy ( ebrt ) is considered one of the primary therapies for patients of all risk classications [ 1 , 2 ]  . 
in recent years , a variety of technical improvements of ebrt such as volumetric intensity - modulated radiotherapy ( vmat / imrt ) and imageguided radiotherapy ( igrt ) have been developed . 
in order to protect adjacent sensitive tissues such as the bladder and rectum , imrt can additionally be combined with simulstrahlenther onkol ( 2020 ) 196 : 598607 taneous integrated boost ( sib ) , allowing distinct radiation doses to be delivered to the cancer site and bordering organs during a single session [ 68 ]  . fractionation schedules of radiotherapy can either be conventionally fractionated or hypofractionated . 
hypofractionated radiotherapy ( hrt ) generally applies single doses of 2.43.1 gy directed at the prostate and seminal vesicle , whereas effective single doses are lower for conventional radiation therapy ( crt ) [ 5 , 9 ]  . 
 [ 10 ] estimate the / ratio for pca to range from 1 to 1.8 gy , vogelius and bentzen [ 11 ] estimate the / ratio to be 1.2 gy ( 95% ci : 0.81.7 gy ) and 2.7 gy ( 95% ci : 1.63.8 gy ) , concluding that moderate hrt is consistent with a low value of the / ratio . 
in contrast , the value for adjacent organs such as bladder or rectum is 35 gy [ 12 ]  . recent studies comparing hypofractionation and conventional fractionation in phase iii trials conclude that hrt leads to similar or even improved late genitourinary ( gu ) and gastrointestinal ( gi ) toxicities [ 13 , 14 ]  . 
in addition , hrt confers improved availability , decreased costs , and shortened treatment duration , and thereby provides relief , especially for patients of advanced age or those suffering from multiple comorbidities . 
countries such as the united states of america , canada , united kingdom , the netherlands , and italy have already established hrt as the clinical standard for radiotherapy of lpca [ 1518 ]  . we conducted a non - randomized retrospective clinical trial to verify that moderate hrt is a treatment alternative with high potential to improve cancer control by evaluating its effects on acute and late toxicity in a cohort of 110 patients . 
the achieved decrease in toxicities reects its high practical relevance.1 patients and methods patients the present retrospective analysis examined 55 patients diagnosed with lpca and treated with moderately hypofractionated radiotherapy in the time period between july 2016 and december 2018 at the institute of radiation therapy and special oncology , hanover medical school . before consenting to enroll in the study the patients were informed about the current scientic status of hrt and 1 parts of the results have been orally presented at the degro annual meeting 2019 in mnster . possible side effects with respect to genitourinary toxicities . 
patients with radical prostatectomy , lymphadenectomy , prior history of radiotherapy , evidence of pelvic nodal disease , and presence of distant metastases were excluded from the study ; patients with biopsy - proven pca t1b to t3b dened by the tnm system without evidence of distant metastasis were found eligible . 
the previously larger sample of crt patients was further ltered using characteristics such as damico risk classication for pca , charlson comorbidity index ( cci ) , androgen deprivation therapy ( adt ) , and age , to ensure comparability and resulting high quality of matching ( crt n = 55 )  . the share of patients classied as high ( intermediate ) risk according to damico classication was 46% ( 49% ) in the hrt group and 42% ( 51% ) for crt patients . 
the most frequently occurring diseases captured by the cci [ 19 ] included diabetes , myocardial infarct , congestive heart failure , peripheral vascular disease , moderate and severe renal diseases , and additional tumors with similar distributions in both groups ( table 1 )  . methods ebrt for lpca employed intensity - modulated vmat combined with sib . 
in contrast , crt patients obtained a total dose of 50.459.4 gy delivered in 1.82 gy fractions to the prostate and seminal vesicle combined with a sib to the prostate to 66 gy , followed by an additional boost ( sequential boost ) to the prostate up to 7278 gy delivered in 2.0 gy fractions over 8 weeks total treatment time . all hrt patients received daily igrt , whereas the vast majority of the crt group obtained igrt 2.3 times per week on average . 
igrt was provided including a cone beam ct ( cbct ) mounted on the gantry of a linear accelerator ( versahd ) using an elekta x - ray volume imager ( xvi )  . in our study , gross tumor volume ( gtv ) equals the prostate since the tumor burden from mri and psma - pet was not available for all patients . 
table shows the baseline characteristics in hrt and crt groups adt androgen deprivation therapy , hrt hypofractionated radiation therapy , crt conventional radiation therapy 3 mm from gtv to clinical target volume ( ctv ) and 5 mm from ctv to planning target volume ( ptv )  . 
the larger ptv includes prostate and seminal vesicle , whereas the sib - ptv only contained the prostate without the seminal vesicle to protect the rectum as shown in fig . 
acute adverse events were categorized retrospectively according to ctcae version 5 [ 21 ] , whereas the chronic adverse events were assessed in accordance with lent - soma tables [ 22 ]  . 
1 reduction of planning target volume ( ptv ) of prostate and proximal vesicle ( green ) to ptv of simultaneous integrated boost ( sib ) prostate without proximal vesicle ( orange )  . delineation of rectum as a region of interest is not included in the graphic to improve visualization of the relevant anatomic features statistical evaluation descriptive statistics were generated to characterize the study cohort . 
for continuous variables , the groups were compared by implementing the student t - test and wilcoxon mannwhitney - test ; for categorical and binary variables the two - sided fishers exact test was applied , because the expected frequencies are rather small and the fishers exact test does not require a certain sample size [ 23 ]  . 
since the ate can be biased in nonrandomized observational trials like the present study , propensity score matching ( psm ) is applied to mimic a randomized trial and enable unbiased analysis [ 24 , 25 ]  . 
thereby , the propensity score ( ps ) describes the probability of treatment assignment dependent on observed patients traits as covariates , namely damico risk stratication , adt , cci , and age . a logit model estimates the ps [ 24 , 25 ]  . 
in the next step , patients from the treatment and control groups are paired according to nearest - neighbor matching : treated patients are matched to those from the control group who are closest in terms of their ps with a caliper corresponding to 26% of the standard deviation of the ps . 
no data regarding the late toxicities were collected for two patients of each group during follow - up . response and local control to capture the secondary endpoints , psa values were measured after 3 months , 6 months , 12 months , and later than 1 year . 
after 3 months , values for psa bounces were available for all patients and dropped by 6.1 ng / ml for the crt group and 5.7 ng / ml for the hrt group . 
values measured after at least 12 months showed a decrease of 7.6 for the crt group and 7.1 for the hrt arthe t - test and wilcoxonmannwhitney test revealed no signicant differences between the treatment and control groups with respect to freedom from biochemical or clinical failure according to the phoenix denition [ 27 ]  . 
mean follow - up was 16 months for the crt group and 10 months for the hrt group . toxicity we tested differences in acute gi toxicities ( proctitis , colitis , diarrhea , defecation frequency , colonic obstruction ) and acute gu toxicities ( urinary frequency , dysuria , noninfective cystitis ) using ctcae ( table 3 and 4 )  . 
for late adverse gu and gi toxicities we stratied subcategories according to lent - soma tables as follows : bladder / urethra , skin and subcutaneous tissue , small intestine , and colon . out of the crt group , 78% patients reported incidences of acute toxicities grades 13 compared to 62% of the hrt group . 
crt patients suffered from proctitis grade 2 ( 13% ) , urinary frequency grade 1 ( 46% ) , and urinary frequency grade 2 ( 13% ) more frequently than hrt patients , who reported values of 0% , 36% , and 4% , respectively ( table 3 )  . 
the results of the ate support the previous results of the fishers exact tests : as illustrated , differences between the therapy and the control groups are only signicant for proctitis and urinary frequency . 
for all other symptoms ( acute as well as late ) , the differences were not statistically signicant and , hence , hrt does not intensify the side effects . furthermore , since the larger ptv volume ( prostate and seminal vesicle ) and sib - ptv ( prostate ) differed between fig . 
despite a possible clinical causal relation , the analysis revealed no signicant correlations in both patient groups . discussion in our study we compared the treatment effectiveness of moderate hrt performed with modern techniques ( imrtigrt - sib ) to crt by analyzing the occurrence and intensity of acute and late toxicities . 
the ndings showed improved treatment effects regarding irradiation - related acute gi and gu toxicity , namely for proctitis and urinary frequency , whereas hrt proved to be an equivalently efcient treatment method when compared with crt regarding its effect on all other toxicities . 
a decrease in psa values in the follow - up care was achieved for both the hrt and crt arms , which implies biochemical tumor control in both groups . several previous studies have explored the effects of hrt . 
conclude that in the investigated trials , such as the profit [ 14 ] , ire [ 2831 ] , rtog [ 30 ] , chhip [ 17 ] , and hypro [ 32 ] studies , hrt leads to similar or even improved results regarding biochemical outcomes and toxicity . 
using fractionation schedules of previous studies as an orientation , we applied a modied dose of 50.0 gy to the prostate and seminal vesicle with an additional 10.0 gy as a sib directly to the prostate in 20 fractions ( eqd2 77.0 gy , / = 1.8 gy ) over a period of 4 weeks , to reduce rectum and bladder complications . the control group received a total dose of 50.459.4 gy delivered in 1.82 gy fractions to the prostate and seminal vesicle combined with a sib to the prostate to 66 gy , followed by an additional boost ( sequential boost ) to the prostate up to 7278 gy delivered in 2.0 gy fractions over 8 - weeks total treatment time . 
the implementation of analogous imrt - igrt - sib plans for both groups allowed an efcient treatment cohort comparison . regarding dose constraints , yu [ 35 ] and hoffman et al . predict that smaller dose constraints , especially with respect to the rectal doses , lead to enhanced cancer control and less acute gi toxicity rates . 
in contrast , the occurrence and intensity of all other late and acute toxistrahlenther onkol ( 2020 ) 196 : 598607 cities do not differ signicantly between the hrt and crt arms . 
the average treatment effects conrmed these results ( table 5 ) and simultaneously proved the robustness of the ndings by counteracting the selection bias persistent in nonrandomized trials through propensity score matching . these results correspond with the ndings of other studies [ 36 ] , and the implementation of sib and modern techniques and restricted dose constraints further prevents increased gi adverse events . 
the study adds to the existing state of the art by integrating these modications , which results in signicantly reduced occurrence and intensity of proctitis and urinary frequency . several limitations of this study should be considered . the ndings of the present analysis predominantly apply to intermediateand high - risk lpca patients with multiple comorbidities and high age . 
due to advanced patient age and the current data base , the follow - up was relatively short ( 16 months for the crt group and 10 months for the hrt group )  . 
thus , hrt offers several medical and economic advantages and should therefore be considered as clinical standard , also in germany . funding open access funding provided by projekt deal . compliance with ethical guidelines conict of interest s . 
merten declare that they have no competing interests . ethical standards this study is compliant with the ethical standards of the committees on human experimentation ( institutional and national ) and with the helsinki declaration . 
all patients gave their informed consent before participating in the study . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
april 2020 der / die autor ( en ) 2020 hintergrund und ziel der arbeit die prospektive biomarkerstudie von chera und kollegen hatte zum ziel , den stellenwert von im blutplasma zirkulierender hpvtumor - dna zur diagnose eines rezidivs bei patienten mit hpv - positiven plattenepithelkarzinomen des oropharynx zu bestimmen [ 1 ]  . patienten und methoden in dieser prospektiven einarmigen studie wurden von mrz 2016 bis august 2018 insgesamt 115 patienten mit einem nicht metastasierten hpvassoziierten plattenepithelkarzinom des oropharynx eingeschlossen , die mittels denitiver radiooder radiochemotherapie ( rct ) behandelt wurden . 
der primre endpunkt der studie war die ermittlung des negativen ( npw ) und positiven prdiktiven werts ( ppw ) von zirkulierender hpvtumor - dna zur vorhersage eines histologisch gesicherten tumorrezidivs . ergebnisse nach einer medianen nachbeobachtungszeit von 23 monaten entwickelten 15 der 115 eingeschlossenen patienten ein lokoregionres rezidiv oder eine fernmetastasierung . 
3 , 79106 freiburg , deutschland 2 deutsches konsortium fr translationale krebsforschung ( dktk ) , partnerstandort freiburg , deutsches krebsforschungszentrum ( dkfz ) , freiburg , deutschland entwickelten 15 von 16 patienten , bei denen zwei aufeinanderfolgende positive hpv - tumor - dna - nachweise vorlagen , ein histologisch gesichertes rezidiv . 
der ppw fr zwei konsekutive positive hpv - tumor - dna - tests betrug demzufolge 94 % , whrend der npw fr negative hpv - tumor - dna im plasma bei 100 % lag . 
durchschnittlich vergingen 3 , 9 monate zwischen dem nachweis von zirkulierender hpv - tumor - dna und der diagnose eines tumorrezidivs . schlussfolgerung der autoren der nachweis von zirkulierender hpv - tumor - dna in zwei aufeinanderfolgenden untersuchungen bei patienten mit einem hpv - assoziierten oropharynxkarzinom hat eine sehr hohe sensitivitt und spezitt fr die detektion eines tumorrezidivs nach denitiver rct . 
auf der anderen seite ist die abwesenheit von zirkulierender hpv - tumor - dna im plasma mit einem rezidivfreien berleben nach zwei jahren von 100 % verbunden . kommentar in der vorliegenden studie wurden 1006 blutproben von 115 patienten mit einem nicht fernmetastasierten hpv - positiven oropharynxkarzinom vor und nach denitiver rct analysiert und damit das potenzial von zirkulierender hpvtumor - dna als biomarker in der rezidivdiagnostik von patienten mit hpv - positiven oropharynxkarzinomen gezeigt . 
die studienautoren verwendeten hierfr ein patentiertes pcr - verfahren ( navdx , naveris , waltham , ma , usa ) , das von tumorzellen freigesetzte hpv - dna von nicht tumorassoziierter hpv - dna unterscheiden kann [ 2 ]  . insbesondere die tatsache , dass hpv - assoziierte oropharynxkarzinome tendenziell spter fernmetastasieren und huger atypische extrapulmonale metastasierungsorte aufweisen , lsst eine biomarkerbasierte rezidivdiagnostik gegenber einer alleinigen bildgebenden nachsorge vorteilhaft erscheinen [ 3 ] : die lokalisation der rezidive in der vorliegenden studie zeigt , dass viele tumormanifestationen strahlenther onkol ( 2020 ) 196 : 676678 interessant nicht in der regulren nachsorge bzw . 
so befanden sich in dieser studie 4 der 15 rezidive in krperregionen auerhalb des scanbereichs der eingesetzten bildgebung . anhand der hier diskutierten studienergebnisse scheint eine testung von hpv - tumor - dna im blutplasma gegenber dem hpv - dna - nachweis in speichelproben fr die rezidivdiagnostik vorteile zu bieten ; insbesondere scheint die distante metastasierung besser detektierbar zu sein [ 4 ]  . in der vorliegenden studie erscheint uns auch die tatsache , dass etwa 10 % der patienten posttherapeutisch einen vorbergehenden anstieg der hpv - tumordna zeigten , welcher im weiteren nachsorgeverlauf jedoch verschwand . 
whrend sich weder die pd - l1expression noch die tumormutationslast zwischen den beiden tumortypen unterscheidet , lsst sich eine hhere anzahl an tumorinltrierenden t - lymphozyten bei hpvassoziierten tumoren zumindest in einigen studien beobachten [ 5 ]  . 
zudem ist das therapieansprechen hpvpositiver oropharynxkarzinome bei immuncheckpoint - inhibitoren besser als bei hpv - negativen tumoren [ 6 , 7 ]  . zu diesem themenkomplex und konkret dem in dieser studie beobachteten phnomen des transienten hpv - tumor - dna - nachweises mit nachfolgender clearance sind allerdings sicherlich weitere studien ntig . in weiteren studien muss ferner untersucht werden , ob eine frhzeitige detektion eines tumorrezidivs auch in verbesserten onkologischen ergebnissen mndet . 
theoretisch knnte mit dieser biomarkerbasierten nachsorge ein hherer anteil sowohl von patienten mit oligometastasierung als auch von patienten mit einem lokoregionren rezidiv detektiert werden , bei denen potenziell kurative situationen vorliegen . 
die autoren haben zudem in einer anderen krzlich publizierten studie zeigen knnen , dass auch die kinetik der hpv - tumordna unter laufender rct mglicherweise einen prdiktiven wert hinsichtlich des lokoregionren therapieansprechens bei hpv - positiven oropharynxkarzinomen hat [ 2 ]  . trotz der beeindruckenden daten der hier diskutierten studie mssen wenige kritikpunkte angemerkt werden . 
die tatsache , dass der ppw und npw erst fr zwei konsekutiv positive hpv - tumor - dna - tests und nicht bereits fr ein positives testergebnis berechnet wurde , war eine post - hoc durchgefhrte nderung des endpunkts : von den 28 patienten mit lediglich einem posttherapeutischen hpv - tumordna - nachweis entwickelten 15 patienten ein tumorrezidiv , sodass der ppw hierfr nur 54 % betrug . 
die bereits erwhnte gegebenheit , dass hpv - assoziierte oropharynxkarzinome zu sptrezidiven neigen , lsst die mediane nachbeobachtungszeit von knapp 2 jahren in dieser studie als zu kurz erscheinen , um die wertigkeit von negativen hpvtumor - dna - tests zu beurteilen . aufgrund der tatsache , dass sich ein teil der studienpopulation zustzlich in einer deeskalationsstudie befand , war die studienkohorte hinsichtlich der bestrahlungsdosis inhomogen . 
das intervall zwischen den hpv - tumor - dnatests war ebenfalls nicht einheitlich und lag zwischen 6 und 9 monaten , was bei einer medianen zeit von knapp 4 monaten zwischen hpv - tumor - dna - detektion und rezidivnachweis als zu lang angesehen werden muss . 
zwar knnte das patentierte pcrverfahren zur spezischen detektion von tumorassoziierter hpv - dna eine standardisierte anwendung in anderen behandlungszentren ermglichen , jedoch mssen die kosten dieser tests gegenber dem erwarteten nutzen abgewogen werden . 
in anbetracht des relativ neuen testverfahrens ist es essenziell , dass eine multizentrische studie die reproduzierbarkeit dieser ergebnisse evaluiert . fazit die vorliegende biomarkerstudie zeigt das potenzial von zirkulierender hpv - tumor - dna in der rezidivdiagnostik von patienten mit hpv - positiven oropharynxkarzinomen und knnte somit zu einer frheren und sufzienteren erkennung von behandlungsrckfllen fhren . auf der basis dieser ergebnisse knnten zuknftig die nachsorgeintervalle verlngert und die anzahl von schnitt678 strahlenther onkol ( 2020 ) 196 : 676678 bilduntersuchungen vermindert werden , um die belastung der patienten zu vermindern und auch kosten einzusparen . es bleiben jedoch noch die langzeitergebnisse dieser hier diskutierten studie sowie weitere konrmierende studien mit greren patientenzahlen abzuwarten , bis ein routinemiger einsatz dieses biomarkers in der nachsorge von patienten mit hpv - assoziierten oropharynxkarzinomen zu empfehlen ist . alexander rhle und nils h . 
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the dosimetric inuence of this margin was retrospectively calculated by analysing systematic and random components of inter and intra errors of 31 consecutive intermediateand high - risk localized pca patients using daily cone beam computed tomography and kv / kv ( kilo - voltage ) imaging . 
for each patient inter variation was assessed by observing the rst 4 treatment days , which led to an ofine art - based treatment plan in case of larger variations . results : systematic inter uncertainties were larger ( 1.12 in lr , 2.28 in si and 1.48 mm in ap ) than intra systematic errors ( 0.44 in lr , 0.69 in si and 0.80 mm in ap )  . 
same ndings for the random error in si direction with 3.19 ( inter ) and 2.30 mm ( intra ) , whereas in lr and ap results were alike with 1.89 ( inter ) and 1.91 mm ( intra ) and 2.10 ( inter ) and 2.27 mm ( intra ) , respectively . 
ofine and online art strategies , such as ofine planning target volume ( ptv ) modication , ofine dose compensation and online plan adaption , have been introduced to diminish systematic and random errors [ 2 , 3 ]  . 
they dealt with systematic errors generated 648 strahlenther onkol ( 2020 ) 196 : 647656 table 1 patient data , including age at treatment time , patients with localized pca , tnm stage [ 42 ] , gleason score [ 43 ] , damico risk stratication [ 44 ] and psa level variable indication for radiotherapy , n ( % ) primary treatment ( % ) postoperative treatment age ( years ) mean ( range ) tnm stage ( n ) gleason score ( n ) 810 damico risk group ( n ) intermediate risk high risk psa level ( ng / ml ) ( cid : 2 ) 4 > 4 to ( cid : 2 ) 10 > 10 to ( cid : 2 ) 20 n = 31 11 ( 35.5% ) 20 ( 64.5 ) 71 ( 6280 ) tnm classication of malignant tumors ; pca prostate cancer ; rt radiotherapy ; psa prostate - specic antigen by interfractional setup uncertainties and intrafractional target motion . the importance of intrafractional target motion for external beam radiation treatments ( ebrt ) increases as treatment margins are reduced due to igrt [ 6 , 7 ]  . 
therefore , at the university hospital erlangen , patients treated for pca receive planning computed tomography ( ct ) and radiotherapy treatment based on a lled bladder and endorectal balloon ( erb ) protocol in order to minimize target motion and spare dose to organs at risk ( oar ) [ 817 ]  . 
prior to treatment , pca patients are rst localized with kv / kv - orthogonal image pairs ( oip ) based on the position of ducial markers ( fm )  . 
using daily cbct for patient positioning is a widely understood method for art procedures [ 2 , 3 , 1822 ]  . the aim of the present analysis was to investigate the dosimetric impact of the clinically used ctv - to - ptv margin by retrospectively assessing daily interfractional setup and intrafractional prostate motion uncertainties . 
to our knowledge , this ofine intervention based on an erb and lled bladder protocol has not been published in the literature before . materials and methods patients the data presented are of 31 patients diagnosed with intermediateor high - risk pca who were treated at the university hospital erlangen between july 2015 and september 2016 . 
eleven of these patients received radiotherapy as primary , i.e. , denitive , treatment while the remaining 20 patients underwent radical prostatectomy before radiotherapy . the patients had a mean age of 71 9 years and tnm stage of ct1 ( 6.5% ) ct2 ( 29% ) for primary radiotherapy and pt2 ( 29% ) pt3 ( 35.5% ) as well as r0 ( n = 12 ) or r1 ( n = 8 ) for postoperative patients . 
no patient experienced biochemical failure having a median biochemical follow - up of 18 months ranging from 333 months [ 23 , 24 ]  . pretreatment protocol three gold anchor ducial markers 0.28 mm in diameter and 1020 mm in length ( naslund medical ab , vassvagen , sweden ) were implanted transperineally under ultrasound ( us ) guidance into apex , and base region of the prostate 5 2.5 days prior to ct simulation ( sensation open ct scanner , siemens healthcare , erlangen , germany )  . 
all patients had a planning ct ( 1 mm slice thickness , 120 kv voltage , 400 ma x - ray tube current ) in supine position immobilized with knee , leg , and head pads . 
one hour prior to imaging and each radiation treatment , patients had ( a ) enemas ( microlax , johnson & johnson gmbh , neuss , germany ) and were ( b ) asked to defecate . 
in addition , the clinical protocol also required the patients to ( c ) drink 1 liter of water to ensure a constant bladder lling , and ( d ) an erb ( rsch ag , kernen , germany ) was inserted to the rectum and inated with 65 cm3 of air . strahlenther onkol ( 2020 ) 196 : 647656 fig . 
1 the scheme of clinical steps involving fm ( ducial markers ) implantation , ct ( computed tomography ) and mri ( magnetic resonance imaging ) , segmentation , treatment planning , patient setup , patient treatment and verication of intratreatment fm positioning . 
shift is applied when fm alignment exceeds 5 mm contouring and treatment planning oars , i.e. , rectum , anterior rectal wall , bladder , femoral heads , ctv and ptv were dened on the planning ct by radiation oncologists using iplan radiotherapy ( rt ) image 4.1.1 ( brainlab ag , munich , germany )  . 
briey , the clinical target volume ( ctv ) consisted of the prostate and seminal vesicles as dened on the planning mri ( magnetic resonance imaging )  . for the ptv , 15 mm were added to the ctv in all directions . 
in brief , inferiorly the ctv extended to the genitourinary diaphragm and superiorly included the vas deferens or seminal vesicle remnants , lateral boundaries were the levator ani and the internal obturator muscles , respectively . 
the dose constraints are described in supplementary i table 1 and a standard 7 - eld imrt dose distribution in axial , coronal and sagittal plane can be seen in supplementary i fig . 
1 ( a , b , c )  . patient setup before each treatment , patients were positioned using an image guidance system ( exactrac , brainlab ag , munich , germany ) consisting of two kv tubes ( shimadzu corp . , kyoto , japan ) and two amorphous silicon detectors ( paxscan 4030a ; varian medical systems , palo alto , ca , usa )  . 
the system was used to acquire a kv / kvoip and a volumetric cbct data set using a clockwise rotation ( 31545 ) of one kv - imager with the following parameters : ~100 kv , 100 ma , 5 s ; 3 mm slice thickness and 512 512 matrix size . 
prior to the last eld of the treatment radiation , a kv / kv - oip was performed to locate the fm for further intrafractional prostate motion analysis . the full sequence of clinical steps starting with fm implantation and followed by ct and mri imaging , segmen650 strahlenther onkol ( 2020 ) 196 : 647656 fig . 
in a , a patient with a low setup error and in b a patient corresponding to larger positioning variation are displayed . for b ofine art was applied . ptv planning target volume , erb endorectal balloon tation , treatment planning , patient setup , patient treatment and lastly verication of intratreatment fm positioning is summarized in fig . 
2a displays a high ct / cbct agreement , which means the erb and anterior rectal wall exhibited small shifts but were within the dened rectal volume ( green contour ) structure . 
if the setup errors revealed that the erb and anterior rectal wall are outside of the rectal volume delineation , i.e. , the patient subject to larger setup uncertainty as shown in fig . 
for critical cases , such as patients with larger setup uncertainty , setup and intrafraction kv / kv - oips were looked at additionally along with cbcts to better understand how well fm , erb and rectal wall were correlating with each other . an in - house software tool based on insight segmentation and registration toolkit ( itk ) was used to quantify interfractional patient setup errors according to erb displacements in cbcts . 
for more details about the erb and fm segmentation , please refer to supplementary ii segmentation of erb and fm . interfractional leftright ( lr ) , superiorinterior ( si ) and anteriorposterior ( ap ) shifts were analyzed by comparing a reference cbct to the remaining 27 cbcts acquired for each patient ( 1 cbct / fraction equals 28 cbcts in total )  . the reference cbct was identied using the location of fm and erb centroids which were dened in each cbct and the planning ct . 
the centroid of the fms was calculated by taking the mean of x , y and z coordinates and the centroid of erb was extracted by using the in - house software tool . 
then the absolute distance ( ( cid : 2 ) dabsolute ) between the two centroids ( fm and erb ) was examined in each data set ( ct and cbct ) , as illustrated in fig . 
in a , left and right cbct and itk - based images represent the marker extraction , whereas the images in b indicate a segmented erb ( light blue )  . 
on the left image in a , the black errors demonstrate the position of fm ( ducial markers ) in the planning ct and on the right the location of fm are displayed as white dots in the binary image . 
image c describes how to assess the absolute distance ( dabsolute ) between the fm and erb ( endorectal balloon ) centroids ( red crosses ) which denes the reference cbct of a cohort of 28 cbcts for each patient distance ( ( cid : 2 ) dabsolute ) had to be below 1 mm between the planning ct and at least one cbct data set to quantify high geometrical accuracy and to fulll the condition for further analysis . 
the group systematic deviations ( ) , standard deviation ( sd ) , systematic deviation ( inter ) and random deviation ( inter ) were calculated to investigate lr , si and ap motion between the reference cbct and the cohort of 27 cbcts for each patient . 
more details about how the group systematic deviations ( ) , standard deviation ( sd ) , systematic deviation ( inter ) and random deviation ( inter ) were derived can be found in section supplementary iiidenition of statistics . to determine intrafractional fm motion in lr , si and ap direction , kv / kv - oips were taken after patient setup and prior to the last eld of treatment for each fraction and each patient . 
for statistical analysis , sd , intra and intra were used to assess lr , si and ap motion . additionally , for a subcohort of 11 denitive pca patients , the dosimetric impact of daily interfractional erb setup errors and intrafractional fm motion on the ptv coverage and oar dose was investigated by comparing treatment plans as per tps ( i.e. , the clinically applied plan with no additional motion applied ) against treatment plans based on daily interand intrafractional motion . 
the treatment plans as per tps and interand intrafractional errors were assessed by using the in - house software tool to generate treatment plans based on daily interand intrafractional variations . 
the latter data were summarized in a dosevolume histogram ( dvh )  . also , a ctv - to - ptv margin was calculated to estimate its magnitude when daily setup errors and intrafractional motion was applied and compared against the ctv - toptv margin which was used for treatment planning . 
can be found in supplementary ivmargin recipe . inter + 2 inter + 2 regarding patients which followed the adaptive plan procedure , initial and adapted treatment plans were compared to determine the magnitude of interfractional erb setup error by using , sd , inter and inter for lr , si and ap motion . 
 [ 29 ] formulas to examine the impact of adapted treatments . statistical analysis in this study the similarity of prostate , anterior rectal wall , and rectum dose coverage inuenced by interand intrafractional motion was statistically evaluated to the treatment plan as per tps . 
 [ 29 ] lr leftright ; si superiorinferior ; ap anterior - posterior ; group systematic deviations ; sd 1 standard deviation ; systematic deviation ( 1 standard deviation ) ; random deviation ( 1 standard deviation ) ; kv / kv - oip kilovoltage / kilovoltage orthogonal image pairs ; ct computed tomography ; cbct cone beam computed tomography the data to be normally distributed . 
the sample size was 119 which is equivalent to a resolution of one data point per 0.5 gy and may correspond to a larger sample size [ 31 ]  . results table 2 represents interfractional setup errors of erb and intrafractional prostate motion uncertainty in lr , si and ap direction as well as ptv margin calculation involving a cohort of 31 patients ( 868 cbcts , 1736 kv / kvoips and 31 planning cts )  . 
both dvhs are compared against each other and involve data of 11 patients with denitive radiotherapy ( 308 cbcts , 616 kv / kv - oips and 11 planning cts )  . 
differences were not statistically signicant . the variation ( 1 standard deviation ) of the dvh curves for prostate and rectum volumes demonstrated analogous results . six patients out of 31 patients ( 168 cbcts , 6 initial planning cts and 6 re - planned cts ) with larger setup uncertainties received ofine art . 
interfractional patient positioning accuracy for initial and adapted treatment plans were examined as well as ctv - to - ptv margins were calculated which can be seen in table 3 . 
in terms of ap motion , adapted ( 1.73 mm for and 3.20 for ) and initial ( 1.67 mm for and 3.21 for ) plans were observed to be alike . 
4 the dosevolume histogram displays the mean dose ( gy ) for prostate ( ctv ) , anterior rectal wall , and rectum volumes ( % ) affected by interand intrafractional motion ( dotted line ) and the original treatment plan ( solid line ) for 11 patients with primarily denitive radiotherapy . 
gtv gross target volume , fm ducial markers , erb endorectal balloon table 3 summary of setup errors and ctv - to - ptv margin computation for 6 patients where ofine art was performed on translation in mm interfraction setup error ctv - ptv margin calculation : oehler et al . 
 [ 29 ] lr leftright ; si superiorinferior ; ap anteriorposterior ; group systematic deviations ; sd 1 standard deviation ; systematic deviation ( 1 standard deviation ) ; random deviation ( 1 standard deviation ) come ranging 68 mm comparing initial and adapted plans , whereas lr and si margins of adapted plans appear to be 2 mm ( 56 mm and 78 mm ) and 3 mm ( 78 mm and 1011 mm ) smaller than those based on the initial plans . discussion igrt addresses patient positioning errors but cannot completely compensate for patient - specic variations [ 32 ]  . 
art is the ideal intervention to account for specic interfractional discrepancy , as it has been reported that art correction strategies reduce systematic and random errors [ 1 , 2 , 22 , 32 ]  . 
furthermore , in 6 out of 31 patients an ofine art method was used clinically and data were evaluated with regards to interfractional variations . the erb contributes to rectal wall dose sparing by keeping the posterior wall distant from the high dose region , which is one reason for choosing erb for our clinical workow and it is widely applied in the literature [ 6 , 15 , 33 ]  . 
 [ 35 ] examined that sporadically stool trapped by the erb and muscular contraction and relaxation of patients after their positioning increases the interfraction setup error of the prostate location , but it is not related to intrafractional motion . 
it implies that systematic and random errors can be reduced by adopting patient setup or by calculating a cumulative dose for each treatment fraction using the anatomy of the day . 
ofine art shows a drop of systematic and random errors in lr and si directions by adapting the contours and treatment plan according to a new planning ct , which met the expectation of other studies . 
still , most of the patients tolerated the insertion of erb , which is also supported by several reports in the literature [ 8 , 37 ]  . in terms of calculating a ctv - to - ptv margin for initial and ofine art treatment plans , 78 mm , 1011 mm and 68 mm and 56 mm , 78 mm and 68 mm in lr , si and ap directions , respectively , could be expected . 
additionally , the calculated ctv - to - ptv margin for initial and adapted plans would not have an impact on ctv ( prostate ) dose coverage since the initial ctv - to - ptv margin also compensates for larger daily uncertainties . it can be argued for the reason of using an ofine intervention looking at the data of this analysis , since the size of the initial ptv structure is large enough to cover positioning and treatment uncertainties . 
the aim in the future will be to gradually reduce the size of the ptv margin to be able to spare more dose to oar and still keep the prescribed dose to the target volume [ 1 , 4 , 34 , 3840 ]  . 
therefore , the feasibility of ofine art was introduced to prevent larger patient positioning errors having a larger impact on the future smaller ptv . the present article neglected the rotational inuence of prostate motion . 
erb deformation may occur due to the existence of stool and gas alongside the erb , inconsistent bladder lling and the use of neo - adjuvant hormone therapy [ 32 , 34 ]  . 
therefore , pca patients , in this manuscript , were treated with a lled bladder and empty rectum to reduce the presence of stool and gas and to keep the size of the bladder uniforpatients were not held on a strict diet during the treatment process , which may lead to the effect of spontaneous stool and gas complications and increased rectum and prostate shifts . 
furthermore , using a 100 cm3 air - lled erb can have the same effect of decreasing rectum and prostate movements but might increase mild erb discomfort to patients due to the larger size of the erb [ 41 ]  . 
the motion and dosimetric inuence of the seminal vesicles was not analyzed but it may be the subject of a future article . conclusion our current ctv - to - ptv margin of 15 mm in lr and si and 510 mm in ap direction takes into account the interand intrafraction uncertainties . 
in this manuscript , reducing systematic and random interfractional errors by applying ofine art strahlenther onkol ( 2020 ) 196 : 647656 based on adapting the contours and treatment plan according to a new planning ct was feasible . acknowledgements the presented work was performed in partial fulllment of the requirements for obtaining the degree rer . 
bert declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
aebersold2 clemens albrecht3 dirk bhmer1 michael flentje4 ute ganswindt5 stefan hcht6 tobias hlscher7 arndt - christian mller8 peter niehoff9 michael pinkawa10 felix sedlmayer11 daniel zips8 thomas wiegel12 prostate cancer expert panel of the german society of radiation oncology ( degro ) and the working party radiation oncology of the german cancer society ( dkg - aro ) received : 5 february 2020 / accepted : 18 february 2020 / published online : 12 march 2020 the author ( s ) 2020 abstract aim to provide an overview on the available treatments to prevent and reduce gynecomastia and / or breast pain caused by antiandrogen therapy for prostate cancer . methods the german society of radiation oncology ( degro ) expert panel summarized available evidence published and assessed the validity of the information on efcacy and treatment - related toxicity . results eight randomized controlled trials and one meta - analysis were identied . 
two randomized trials demonstrated that prophylactic radiation therapy ( rt ) using 1 10 gy or 2 6 gy signicantly reduced the rate of gynecomastia but not breast pain , as compared to observation . 
a randomized dose - nding trial identied the daily dose of 20 mg tamoxifen ( tmx ) as the most effective prophylactic dose and another randomized trial described that daily tmx use was superior to weekly use . 
two other randomized trials described that tmx was clearly superior to anastrozole in reducing the risk for gynecomastia and / or breast paone comparative randomized trial between prophylactic rt using 1 12 gy and tmx concluded that prophylactic tmx is more effective compared to prophylactic rt and furthermore that tmx appears to be more effective to treat gynecomastia and / or breast pain when symptoms are already present . 
a meta - analysis conrmed that both prophylactic rt and tmx can reduce the risk of gynecomastia and / or breast pain with tmx being more effective ; however , the rate of side effects after tmx including dizziness and hot ushes might be higher than after rt and must be taken into account . 
less is known regarding the comparative effectiveness of different radiation fractionation schedules and more modern rt techniques . ( cid : 2 ) pirus ghadjar , md pirus.ghadjar@charite.de 1 department of radiation oncology , charit saarlouis , germany 6 xcare praxis fr strahlentherapie saarlouis , xcare gruppe , universittsmedizin berlin , corporate member of freie universitt berlin , humboldt - universitt zu berlin , and berlin institute of health , berlin , germany , augustenburger platz 1 , 13353 berlin , germany inselspital , bern university hospital , university of bern , bern , switzerland 3 klinikum nrnberg nord , nrnberg , germany 4 universittsklinikum wrzburg , wrzburg , germany 7 universittsklinikum carl gustav carus , technische universitt dresden , dresden , germany 8 universittsklinikum tbingen , tbingen , germany sana klinikum offenbach , offenbach , germany 10 mediclin robert janker klinik , bonn , germany 11 landeskrankenhaus , universittsklinikum der paracelsus medizinischen privatuniversitt , salzburg , austria innsbruck medical university , innsbruck , austria 12 universittsklinikum ulm , ulm , germany 590 strahlenther onkol ( 2020 ) 196 : 589597 conclusions prophylactic rt as well as daily tmx can signicantly reduce the incidence of gynecomastia and / or breast patmx appears to be an effective alternative to rt also as a therapeutic treatment in the presence of gynecomastia but its side effects and off - label use must be considered . keywords gynecomastia breast pain prostate cancer antiandrogen therapy treatment introduction androgen deprivation therapy ( adt ) is commonly used in metastatic prostate cancer ( pca ) or combined with primary radiation therapy ( rt ) for patients with localized pca with intermediateto high - risk features , locally advanced pca or biochemically recurrent prostate cancer [ 13 ]  . a common side effect of adt , due to the disturbed balance between estrogens and androgens throughout the body , can be swelling of the male breast called gynecomastia and / or breast pain ( mastodynia )  . 
generally , stimulation of estrogen receptors in the breast tissue stimulate growth , while stimulation of androgen receptors inhibits growth . nonsteroidal antiandrogens like bicalutamide or utamide block androgen receptors , which through a feedback loop increase the secretion of luteinizing hormone ( lh )  . 
as androgen receptors are blocked by nonsteroidal antiandrogens , the increased level of estrogen stimulating the estrogen receptor in breast tissue stimulates growth , leading to gynecomastia and / or breast pain [ 4 ]  . gynecomastia and / or breast pain can be observed in up to 85% of patients after therapy with high - dose nonsteroidal antiandrogens , negatively impacting patients quality of live ( qol ) and treatment compliance [ 1 ]  . the use of enzalutamide , an androgen receptor signaling inhibitor , besides binding to the androgen receptor inhibiting also dna binding and coactivator recruitment , has likewise been shown to be associated with a 49% rate of gynecomastia and 21% rate of nipple pain within 2 years [ 5 ]  . 
a lower rate of gynecomastia and / or breast pain of only around 1322% is observed , when combined androgen blockade is used [ 1 ]  . for apalutamide , a new selective androgen signal inhibitor , gynecomastia is not described as a drug - related side effect . adt - related gynecomastia and / or breast pain can be treated by antiproliferative low - dose rt to the breasts . 
alternatively , gynecomastia and / or breast pain can be treated by drug intervention using either tamoxifen ( tmx ) which blocks the estrogen receptor , or theoretically by anastrozole which inhibits the peripheral aromatization of androgens into estrogens . 
the literature supporting the use of these treatment approaches is reviewed in the following . materials and methods complete reports of randomized controlled trials or metaanalysis of rcts of rt and / or drug interventions to prevent gynecomastia and / or breast pain ( prophylactic treatment ) or to treat existing gynecomastia and / or breast pain ( therapeutic treatment ) in patients receiving adt for prostate cancer were searched in may 2019 using medline , current contents , pubmed , and references from relevant articles . the search strategy included the terms prostate cancer , androgen deprivation therapy , hormonal therapy , antiandrogen therapy , gynecomastia , breast pain , mastodynia , treatment , alone or in combination . the primary objective was efcacy to treat gynecomastia and / or breast pain as well as treatment - related toxicities . original articles written in english language and published in peer - reviewed journals after the year 2000 were included . 
49.2% rt - related adverse events were experienced by 17 of 52 patients ( 33% ) who received rt ( breast / nipple erythema , breast / nipple tenderness , or skin irritation ) adverse events were mild and observed in 6 or 8 patients per treatment arm adt androgen deprivation therapy , qol quality of life , rt radiation therapy , or odds ratio , ci condence interval , n.a. 
not available no randomized trials were found using surgery as treatdrug therapy ment modality for gynecomastia and / or breast pain . radiation therapy the two identied randomized controlled trials are summarized in table 1 testing the effect of radiation therapy for adt - related gynecomastia and / or breast pain . one randomized trial was conducted in a double blind , sham - controlled fashion . 
the dose was directed to a 5 - cm diameter circle of tissue centered around each nipple and a minimum dose of 90% was required between the skin and the chest wall using 612 mev . 
the dose was prescribed to the 90% isodose line covering the supercial 34 mm of the pectoral muscle using 6 to 12 mev [ 7 ]  . the ve identied randomized controlled trials testing the effect of drug therapy for adt - related gynecomastia and / or breast pain are summarized in table 2 . in a placebo - controlled randomized doseresponse study , tmx was tested as prophylactic treatment in 282 prostate cancer patients undergoing bicalutamide therapy [ 8 ]  . patients were randomized to different doses of tmx ( 1 , 2.5 , 5 , 10 , or 20 mg / day ) or placebo given for 12 months during bicalutamide therapy , followed by 12 months where bicalutamide was given alone . 
an increased incidence of dizziness and hot ushes was observed with prophylactic tmx [ 8 ]  . in another trial in which prostate cancer patients underwent bicalutamide treatment patients were randomized into either 20 mg daily tmx continuously or 20 mg daily tmx for the rst 8 weeks , then at a single weekly dose of 20 mg thereafter for a total of 36 months ( or for 24 months in selected patients ) in both arms . 
there was no difference in treatment - related toxicity between the trial arms . 592 strahlenther onkol ( 2020 ) 196 : 589597 table 2 characteristics of prospective randomized controlled trials evaluating the role of drug therapy for adt - related gynecomastia and / or breast pain trial design interventions and results publication / author patients fradet et al . 
 [ 8 ] study period 11 / 2002 06 / 2003 randomized , placebo controlled side effects and / or dizziness and hot ushes increased by tmx no difference in treatment - related toxicity dizziness increased by tmx treatment was well tolerated and the incidence of toxicity was higher in the anastrozole arm ( 69.5% of patients ) as compared to placebo ( 37.5% ) or tmx ( 35.1% ) no signicant difference between the trial arms patients were randomized to different prophylactic doses of tmx ( 1 , 2.5 , 5 , 10 , or 20 mg / day ) or placebo given for 12 months . 
at 24 months ( i.e. , after 12 months of bicalutamide monotherapy ) , a high incidence of breast events ( > 90% ) was seen in all groups patients were randomized to prophylactic daily tmx 20 mg or daily tmx 20 mg for 8 weeks and weekly tmx 20 mg thereafter . 
resolution of gynecomastia and breast pain for therapeutically treated patients occurred in 65.4% in the tmx group , 71.8% of patients in the placebo group ( who received tmx ) and 18.8% of patients in the anastrozole group patients were randomized to 48 weeks of prophylactic daily tmx 20 mg or daily anastrozole 1 mg or placebo . 
gynecomastia developed in 73% of patients in the bicalutamide group , 10% of patients in the bicalutamide - tmx group , and 51% of patients in the bicalutamide - anastrozole group ( p = 0.001 ) ; breast pain developed in 39% , 6% and 27% of patients , respectively ( p = 0.006 ) patients were randomized to 1 year daily 20 mg tmx within 1 month from the onset of gynecomastia and / or breast pain ( arm a , therapeutic treatment ) or 1 year prophylactic daily 10 mg tmx ( arm b )  . 
the differences in prevalence of gynecomastia and breast pain between the 2 arms both favored tmx prophylaxis ( p = 0.0001 and p = 0.001 , respectively ) bedognetti et al . 
included 107 patients with prostate cancer who received bicalutamide therapy in a randomized placebo - controlled trial comparing 3 months of prophylactic daily 20 mg tmx with daily 1 mg anastrozole or placebo with the primary endpoint being gynecomastia and / or breast pain after 3 months . 
when gynecomastia and / or breast pain was observed during this period , tmx or anastrozole where given again for 3 months or for patients of the placebo group 20 mg of daily tmx was applied . 
interpretation of the results at 6 , 9 , and 12 months after randomization was confounded by the retreatment of some patients with tmx or anastrozole for gynecomastia / breast pain developing before these timepoints , and therefore not presented . 
resolution of gynecomastia and breast pain occurred in 65.4% of patients in the tmx group , 71.8% of patients in the placebo group ( who received tmx ) and 18.8% of patients in the anastrozole group [ 10 ]  . 
although serum testosterone levels in the tmx group were higher than those in the placebo group during the prophylactic phase of the clinical trial , any adverse impact of combination therapy on cancer control as assessed by psa levels could not be observed during the trial [ 10 ]  . in a placebo - controlled randomized trial on prostate cancer patients who received bicalutamide therapy , 114 patients were randomized into 48 weeks of prophylactic daily 20 mg tmx , or daily 1 mg anastrozole or placebo . 
patients were randomized to either 1 year daily 20 mg tmx within 1 month from the onset of gynecomastia and / or breast pain ( arm a , therapeutic treatment ) or 1 year prophylactic daily 10 mg tmx ( arm b )  . 
although tmx was quite effective in the majority of patients of arm b , the action of the drug was slow , with only 18.5% of patients having a clinical response after 3 months of therapy . 
drug therapy table 3 summarized the identied randomized controlled trial comparing radiation therapy and drug therapy with two randomizations for adt - related gynecomastia and / or breast pain . a randomized controlled trial on 102 prostate cancer patients who underwent bicalutamide treatment randomized patients in a control arm or to receive prophylactic daily 10 mg tmx over 24 weeks or prophylactic rt using 1 12 gy . 
rt was administered as an electron beam directed to irradiate a 5 cm diameter circle of tissue centered around each nipple and was designed to deliver a minimum dose of 90% between the skin and the chest wall . 
an appropriate electron energy of 612 mev was selected to cover the depth of tissue . patients from the control arm who developed gynecomastia and / or breast pain were subsequently randomized to tmx or rt [ 13 ]  . of the control group 67% of patients developed gynecomastia compared with 8% after prophylactic tmx and 34% after prophylactic rt . 
there was no difference of treatment - related toxicity or psa control between the two arms [ 13 ]  . data from the latter trial were published again but with more included patients and with similar main results [ 14 ]  . 594 strahlenther onkol ( 2020 ) 196 : 589597 table 3 characteristics of prospective randomized controlled trials comparing radiation therapy and tamoxifen for adt - related gynecomastia and / or breast pain publication / author patients trial design study period di lorenzo et al . 
 [ 13 ] randomized controlled 01 / 2002 02 / 2004 interventions and results patients were randomized no additional treatment ( control arm ) or prophylactic daily 10 mg tmx over 24 weeks or prophylactic low dose rt using 1 12 gy . 
patients from the control arm who developed gynecomastia and / or breast pain were subsequently randomized to tmx or rt . of the control group 67% of patients developed gynecomastia compared with 8% after prophylactic tmx and 34% after prophylactic rt . 
in patients of the control group who had gynecomastia and / or breast pain a signicant decrease in symptoms was achieved in those receiving tmx ( p = 0.05 ) for further information compare below ( perdon et al . ) same trial as di lorenzo et al . , published with a larger number of patients but basically the same results side effects and / or there were no signicant differences between the groups with respect to toxicthere were no signicant differences between the groups with respect to toxicperdon et al . 
 [ 14 ] randomized controlled 01 / 2002 02 / 2004 adt androgen deprivation therapy , qol quality of life , rt radiation therapy the 35 patients allocated in the control arm ( initial randomization ) who developed gynecomastia and / or breast pain were subsequently randomly assigned to tmx ( n = 17 ) or rt ( n = 18 )  . 
after 6 months and 9 months , breast pain was reported in 4 of 14 patients assigned tmx compared with 12 of 15 assigned rt . a recent meta - analysis included ve randomized trials [ 68 , 11 , 14 ] with a total of 777 patients to explore the effects of prophylactic low - dose rt or tmx for patients who underwent adt for prostate cancer [ 15 ]  . 
the incidence of adverse effects ( erythema , pruritus or hyperpigmentation ) were highest in the rt arms ( 45 / 155 ; 29% ) compared with observation arms ( 48 / 175 ; 27.4% ) , resulting in an absolute risk increase to harm of 1.6% and number needed to harm of 62.5. 
the authors concluded that tmx was two times more effective in preventing gynecomastia ; however , low - dose rt represents an effective and safe treatment option , to take into account mainly in patients with cardiovascular risk factors or thrombotic diathesis [ 15 ]  . discussion the incidence of gynecomastia and / or breast pain after treatment with nonsteroidal antiandrogens or more recently also with enzalutamide is high and effective prophylactic and therapeutic treatments are important . 
prophylactic rt ( 1 1012 gy or 2 6 gy ) is generally well tolerated and can signicantly reduce gynecomastia and to a lesser extent breast pasecondary cancers are generally a risk after every rt ; however , the risk after usage of lower - doses , usually used for treatment of benign diseases , renders the treatment strategies for gynecomastia and breast pain development of second cancers , to the best of our knowledge , very unlikely [ 16 ]  . 
likewise , in a registry - based study on prophylactic rt of the breast in prostate cancer patients , the risk of second cancers was not increased [ 17 ]  . daily 20 mg tmx is also a well - established approach and appears to be more effective than rt for prophylaxis and therapeutic treatment for gynecomastia and / or breast pain [ 1315 ]  . 
tmx , however is associated with a welldocumented rate of side effects , mostly dizziness [ 8 , 10 ] and hot ushes [ 8 ] , whereby the latter might be additive to those produced by adt , which would adversely affect tolerability of adt . 
in addition , the risk of thromboembolic events is signicantly increased in older ( 71 years ) male patients who undergo tmx treatment for breast cancer [ 18 ]  . 
regarding the risk of secondary cancers due to tmx treatment , in females an increase of endometrial cancers is well - documented , long - term data for prostate cancer patients receiving tmx is not available to estimate the risk of secondary cancers in men . 
there was no evidence in any of the randomized controlled trials that there is a negative effect of tmx on psa control , at any assessment compared to placebo [ 812 ]  . the resolution rate for gynecomastia is strictly related to the duration of therapy with bicalutamide [ 14 ]  . 
resolution of gynecomastia and breast pain occurred in round about two thirds of patients who were therapeutically retreated with 3 months of 20 mg daily tmx , or in patients with manifest gynecomastia and / or breast pain who were treated with 3 months of 20 mg daily tmx for the rst time [ 10 ]  . as expected , based on the pharmacologic mechanisms involved , the benets of prophylactic tmx 20 mg do not persist once therapy was discontinued [ 10 ]  . 
therefore , it is probably required to remain on tmx throughout the course of adt treatment to maintain a prophylactic effect [ 8 ]  . notably , the use of tmx in prostate cancer patients is an off - label use and liability issues may apply for prescribing doctors . although low - dose breast rt is usually well tolerated and allows patients to avoid year - long exposition to tmx , late cardiac effects and secondary malignant disease might be of some concern following the delivery of this treatment , especially in the individuals with longer life expectancies , like those who are candidates to receive bicalutamide as an adjuvant treatment [ 19 ]  . 
this can however be reduced to a minimum when the appropriate electron energy is chosen . a comparative histologic examination of breast tissue one year after rt with 12.5 gy ( 3 fractions ) and normal tissue without previous rt found a signicantly improved but not completely inhibited diethylstilboestrol - induced gynecomastia [ 20 ]  . 
gynecomastia can be characterized into two distinct subtypes ( type i , increased number of ducts and marked proliferation of ductal epithelia ; and type ii , minimal proliferation but changes to the stroma and structural components of the breast ) [ 21 ] , it is possible that rt only prevents the proliferative change ( type i )  . 
thus , more studies using different schedules of fractionation achieving higher biological doses with conformal rt techniques should be performed to further reduce the incidence of gynecomastia and / or breast pain without increasing the risk of toxicity associated with rt [ 15 , 22 ]  . for clinical practice , besides the comparative effectiveness of tmx and rt also side effects have to be considered . although rt appears to be less effective than tmx as prophylactic treatment , side effects of rt are only modest and of short duration , whereas the side effects of tmx are usually lasting throughout the whole course of therapy . 
patients need to be counseled well regarding this and it might also be an option to start prophylactic rt and switch to tmx , when rt should turn out to be not effective enough . due to the associated high incidence of gynecomastia and / or breast pain , prophylactic treatment should only be offered to patients undergoing treatment with nonsteroidal antiandrogens or enzalutamide but not to patients undergoing treatment with other forms of adt . 
currently , gynecomastia is not an issue with the new antiandrogen apalutamide . unfortunately , there is no evidence from randomized trials available regarding different fractionation schedules of rt neither as a prophylactic or therapeutic treatment . 
today , besides the established 1 1012 gy single shot treatment , or the 2 6 gy schedule , commonly hypofractionated schedules with 35 fractions of 3 gy are applied , as recently reviewed by the guideline for radiotherapy of benign diseases published by the german society for radiation oncology ( degro ) and others [ 23 , 24 ]  . therapeutic treatment of existing gynecomastia and / or breast pain again , tmx is more effective than rt ; however , treatment - associated side effects and their duration also have to be considered in decision making and discussed with patients . for therapeutic rt of existing gynecomastia and / or breast pain even higher doses of around 3040 gy total dose are used and recommended [ 23 ] , but there is no data available supporting this strategy and more data is needed to conrm that this higher dose approach is associated with increased effectivity . anastrozole has been shown to be ineffective for the prophylactic treatment of gynecomastia and / or breast pain and should therefore not be used [ 10 , 11 ]  . long - standing gynecomastia resulting from the brotic changes in the adipose tissue appears to be best managed by surgery [ 25 ]  . 
however , breast surgery can be associated with complications such as doughnut deformity , nipple necrosis , nipple atting , and loss of sensation [ 26 ]  . 596 conclusions prophylactic rt as well as daily tmx can signicantly reduce the incidence of gynecomastia and / or breast pain . tmx appears to be an effective alternative to rt also as a therapeutic treatment in the presence of gynecomastia but its side effects and off - label use must be considered . funding open access funding provided by projekt deal . compliance with ethical guidelines conict of interest p . 
wiegel declare that they have no competing interests . ethical standards the accompanying manuscript does not contain any studies carried out by the authors on humans or animals . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
biochemical recurrence - free survival rates ( brfs ; psa < 0.2 ng / ml ) were calculated according to kaplanmeier and survival curves were compared using the log rank test . 
even though slnd and slnrt are regularly performed , there is sparse comparative data regarding benecial effects on survival outcomes . in a recent systematic review on slnd , wide ranges of 2and 5 - year biochemical recurrence - free survival rates ( brfs ) between 23 to 64% and 6 to 31% , respectively , have been described . 
however , it has to be stated that templates 638 strahlenther onkol ( 2020 ) 196 : 637646 of slnd varied signicantly between the currently available studies , as did adjuvant treatment , endpoints , and study populations , and present evidence is mostly based on small single - centre case series [ 4 ]  . likewise , few studies on slnrt were identied in a recent review : patients with pelvic and / or extra - pelvic nodes were either treated by stereotactic body radiotherapy ( sbrt ) ( 55% ) or elective nodal radiotherapy ( enrt ) ( 45% ) to a lymph node region or the whole pelvic lymphatic pathways [ 5 ]  . 
in patients treated with enrt 3 - year progression - free survival ranged from 61.8 to 75% [ 6 ] , whereas in patients with sbrt to pet - positive lymph nodes 3 - year progression - free survival ranged between 26 and 33% [ 5 ]  . 
this retrospective analysis was performed in compliance with the principles of the declaration of helsinki and its subsequent amendments [ 13 ]  . 68ga - psma labelling and pet / ct imaging radiolabelling of psma - hbed - cc was performed with 68ga3 + from a 68ge / 68ga generator system ( galliapharm , eckert & ziegler ag , berlin , germany ) using an automated synthesis module ( grp , scintomics gmbh , munich , germany ) and prepacked cassettes ( abx gmbh , radeberg , germany ) as described previously for a different psma ligand by weineisen et al . 
in absence of contraindications , 20 mg furosemide was injected almost simultaneously with 68gapsma injection to lower tracer retention in the bladder . pet images were reconstructed with an axial 168 168 matrix based on the truex algorithm ( 3 iterations , 21 subsets ; biograph 64 ) or on the vue point fx algorithm ( 2 iterations , 36 subsets ; discovery 690 )  . image interpretation pet / ct images were interpreted by a consensus read of two nuclear medicine physicians and two radiologists in the sense of a clinical report - based analysis . 
pet - positive lesions were visually identied by 68ga - psma uptake above background level and not associated with physiologic uptake [ 15 ]  . radiotherapy all patients received enrt by intensity - modulated radiotherapy ( imrt ) or volumetric arc therapy ( vmat ) and image - guided radiotherapy techniques ( igrt , 25 times / week )  . 
patients were regarded free of adt inuence after a minimum time - period of 5 months after last application of adt . statistical analysis brfs ( psa ( cid : 2 ) 0.2 ng / ml ) was dened as the primary study endpoint . 
overall , a median of 8 ( 144 ) lymph nodes were removed at time of slnd . evidence of pca was pathologically conrmed in a median of 1 ( 016 ) lymph node . 
in total , there were 4 patients with a clavien grade ii ( 2 paralytic ileus , 2 lymphorrhea ) and 2 patients with a clavien grade iiia ( 2 pulmonary artery embolism ) complication ( table 2 )  . adt was recommended to all patients with slnrt due to the evidence of pet - positive lymph nodes for 2 years [ 20 , 21 ]  . 
consequently , 59 / 67 ( 88% ) patients were started on adt before initiation of slnrt , 42 / 67 patients ( 63% ) discontinued after a median time of 7 ( 241 ) months due to patients preferences . 
acute grade 3 urogenital toxicity occurred in 1 / 67 ( 2% ) patients with evidence of urethral stenosis . late grade 2 toxicity was overall seen in 24 / 67 ( 36% ) patients with mainly signs of erectile dysfunction and increased urinary frequency . 
slnrt was signicantly associated with brfs ( regression coefcient 1.473 , hazard ratio 4.360 , 95% ci 1.66511.418 ; p = 0.003 ) ( table 5 and supplemental table 1 )  . discussion management of lymph node recurrence after rpe is a challenging clinical scenario , and there is sparse comparative data regarding the benecial effects of slnd and slnrt on survival outcomes . 
to further homogenize the table 5 multivariate analysis of factors associated with biochemical recurrence - free survival after salvage lymph node dissection / salvage lymph node radiotherapy association with brfs ( < 0.2 ng / ml ) regression coefcient slnd vs . 
in total , 100 patients ( n = 33 slnd , n = 67 slnrt ) were included in the nal analysis , of whom all slnrt patients were treated with enrt with simultaneous integrated boost ( sib ) to the pet - positive lymph nodes . 
as expected , patients with slnd were primarily patients with psa recurrence ( 73% ) , whereas the slnrt cohort encompassed mostly patients with biochemical persistence ( 73% )  . 
overall , brfs of the present slnd cohort compares nicely to this range and similar pfs ranges are known for sbrt cohorts [ 5 ]  . this proportionally lower brfs rate of the current patient cohort with slnd is comparable to a recent retrospective , multicentre analysis on sbrt vs . 
like non - extensive slnd , sbrt treats only the pet - positive lymph nodes , whereas enrt , as it was performed in the current cohort , not only treats the pet - positive , affected nodes , but the whole lymphatic drainage , for instance the entire pelvic lymphatic pathway as well as in general the prostatic fossa especially in patients with locally advanced disease or positive surgical margins . 
these ndings suggest again that the current imaging modalities are not yet sensitive enough for a restricted node - based surgical or radiotherapy approach [ 32 ]  . based on lymph node recurrences detected by choline pet / ct following primary treatment for pca , de bruycker et al . 
correspondingly , they found that with enrt more patients were theoretically fully covered ( p < 0.02 ) and the total number of covered lesions was higher ( p < 0.001 ) when compared to all types of slnd , except for superextended slnd , which was comparable to enrt . 
the authors concluded that limited or standard extended slnd might be insufcient as a salvage treatment approach and enrt or superextended slnd should be preferred [ 33 ]  . mdt to recurrent lymph node metastases is still controversial and there is an ongoing debate whether it denitely changes the disease outcome in the long - run or represents just psa cosmetics that comes at a cost of potential toxicity [ 34 ]  . 
this might lead to a more favourable brfs in some patients , although the majority ( 50 / 67 ; 75% ) had no adt at last follow - up and 42 / 59 ( 71% ) of those with adt concomitantly to rt had discontinued it a median of 27 months ( range 048 months ) before last follow - up . 
this might partly explain the lower brfs in slnd patients and might lead to the conclusion that slnd should primarily be undertaken in patients without locally advanced disease or positive surgical margins when adjuvant radiotherapy of prostatic fossa is withheld . the aim of this comparative study was to explore the possible treatment options for patients with psma petpositive , oligorecurrent nodal disease : with all its inherent aws of such an retrospective analysis , slnrt seems to be the preferred treatment option for patients with nodal recurrences after previous radical prostatectomy especially when undergoing a combination of slnrt in the form of an enrt as it is performed in our institution and concomitant adt with overall an acceptable toxicity prole . the present results cannot be transferred to other surgical approaches like superextended slnd . 
despite its limitations , the current study depicts real - world data from a tertiary - care reference centre and might be hypotheses - generating for future phase ii trials . in the current study , rare comparative data from a contemporary patient cohort diagnosed within the psmapet / ct era are provided . 
findings need to be conrmed in a prospective randomized trial . author contribution all authors contributed to the conception and design of the retrospective study , data acquisition , analysis and interpretation of the data . 
fendler received nancial support from the german research foundation ( deutsche forschungsgemeinschaft , dfg , grants fe1573 / 1 - 1 / 807122 and fe1573 / 3 - 1 / 659216 ) , mercator researach center ruhr ( mercur , an - 2019 - 0001 ) , ifores ( d / 10781260 , d / 107 - 30240 ) , doktor robert peger - stiftung , and wiedenfeld - stiftung / stiftung krebsforschung duisburg . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
the aim of the present retrospective study was to report the preliminary clinical results and toxicity of a mono - institutional series of patients re - irradiated with linac - based sbrt in recurrent prostate cancer . methods inclusion criteria were previous denitive or adjuvant / salvage rt , evidence of biochemical recurrence and radiological detection of local relapse ( magnetic resonance imaging or psma / choline - positron emission tomography ) , and ipss < 10 . 
toxicity was assessed according to common terminology criteria for adverse events v4.0. results between 12 / 2014 and 12 / 2019 , 24 patients with median age 75 years ( 6589 ) underwent re - rt for pc recurrence . median follow - up was 21 months ( 268 )  . 
all patients were treated with sbrt to a median total dose of 30 gy ( 2536 gy ) in 56 fractions , and simultaneous androgen deprivation therapy was administered in 4 patients . 
long - term data are pending . keywords re - irradiation prostate stereotactic body radiotherapy volumetric modulated arc therapy local relapse introduction recent advances in technology have led to a remarkable improvement in both the diagnostic and therapeutic pathways for prostate cancer ( pca )  . 
new imaging tools including multiparametric magnetic resonance imaging ( mri ) or metabolic tracers for positron emission tomography ( pet ) - imaging like c - choline or ga - prostate specic ( cid : 2 ) francesco cuccia f.cuccia1@virgilio.it 1 advanced radiation oncology department , irccs sacro cuore don calabria hospital , negrar , verona , italy 2 radiation oncology department , lmu , munich university hospital , munich , germany 3 university of brescia , brescia , italy membrane antigen ( psma ) have signicantly improved the ability to detect clinically evident disease [ 13 ]  . at the same time , modern radiotherapy ( rt ) techniques allow the safe delivery of dose - escalated treatments along with the widespread adoption of hypofractionated schedules [ 46 ]  . nonetheless , local recurrence after radiotherapy occurs in 3054% of cases in either curative or postoperative settings . 
the most appropriate therapeutic approach for this clinical scenario remains a matter of debate [ 7 ]  . as international guidelines suggest life - long androgen deprivation therapy ( adt ) as the standard of care , local approaches are becoming more attractive , as they represent a potential alternative for controlling disease without overloading the patient with the side effects of long - term hormone therapy [ 8 ]  . according to the capsure study , local therapies are proposed for a small number of patients who recur after strahlenther onkol ( 2020 ) 196 : 628636 primary rt ( estimated at approximately 20% of cases ) , with a preference towards observation or adt as the rst options [ 9 ]  . salvage treatments after rt may include brachytherapy , cryoablation , or high - intensity focused ultrasound ( hifu ) , for which small series report promising results in terms of biochemical control [ 10 ]  . given the typically advanced age of the patients , the role of salvage surgery is limited to a niche of subjects , despite recent evidence supporting better outcomes compared to the abovementioned techniques , albeit at the price of severe post - surgery sequelae [ 11 ]  . traditionally , the use of external beam radiotherapy ( ebrt ) in recurrent disease after primary rt has been regarded with extreme caution , due to concerns over severe toxicity incidence [ 8 ]  . nowadays , image guidance and new - generation linacs have increased the safety of ebrt [ 12 , 13 ]  . 
nevertheless , the rst experiences with prostate re - irradiation are based on the use of robotic stereotactic body radiotherapy ( sbrt ) via cyberknife ( ck ; elekta , stockholm , sweden ) [ 1417 ]  . at rst , in a cohort of 32 patients , zerini et al . 
the authors observed no g3 acute or late adverse events and , notably , with a median follow - up of 21.3 months , almost half of the cohort had no evidence of disease [ 18 ]  . in more recent preliminary studies , linac - based re - irradiation with sbrt has been reported as a safe and effective strategy for delivering a potentially noninvasive curative treatment that may also postpone the start of systemic therapies and thus slow the natural course of the disease towards metastatic status [ 19 , 20 ]  . 
mri , ga - psma , or choline - pet was performed for staging assessment depending on the psa levels below or above the threshold value of psa = 1 ng / ml . 
inclusion criteria were prior rt for pc ( both denitive or postoperative ) , diagnosis of local readt androgen deprivation therapy , brt brachytherapy , ebrt external beam radiotherapy , eqd2 equivalent dose in 2 gy fractions , sbrt stereotactic body radiotherapy 630 strahlenther onkol ( 2020 ) 196 : 628636 the benet of concomitant / adjuvant adt administration was discussed with each patient . 
to obtain reproducible bladder lling and an empty rectum , patients were required to perform a eet enema 2 h before the ct imaging and to drink 500 ml of water 35 min before the simulation . 
the same preparation procedure was applied for the treatment . the clinical target volume ( ctv ) consisted of the entire prostate gland or the pet - tracer avid area within the prostate bed . 
to generate the planning target volume ( ptv ) , a 5 - mm margin in all directions and a 3 - mm posterior margin were added , excluding the urethra in case of prostate bed recurrence . image fusion with metabolic imaging or mri ( when available ) was performed to improve the accuracy of ctv delineation . 
the femurs , rectum , bladder , urethra , penile bulb , and intestinal loops were delineated as organs at risk ( oars )  . for oars cumulative bed assessment , a rigid image fusion with the rst rt planning ct was performed applying a soft - tissue anatomy match , and rectum was then delineated from the anal verge to the rectosigmoid exure , the bladder from the base to the dome . 
assuming an / ratio = 3 for bladder and rectum , the median cumulative bed values were calculated for dmax ( i.e. , maximal point dose ) , dmin ( i.e. , the smallest dose in dened volume ) , and dmean ( mean dose within the volume )  . treatment plans were generated for the rapidarctm ( varian medical systems , palo alto , ca , usa ) vmat technique in order to deliver a median total dose of 30 gy ( range 2536 ) in 56 fractions . 
the planning objectives were to cover 98% of the ctv with at least 98% of the prescribed dose and 95% of the ptv with at least 95% of the prescribed dose , accepting hotspot areas > 107% only if within the ctv . 
for the oars , the following constraints were applied : v18gy 35% , v28gy 10% , dmax < 35 gy for the rectum ; dmax < 35 gy for the bladder ; dmax < 35 gy for the urethra [ 25 ]  . the treatment was delivered with fff beam delivery and the rapidarctm vmat technique by means of a truebeamtm linac ( varian medical systems , palo alto , ca , usa )  . 
acute toxicity was dened as any adverse event occurring within 90 days from the start of treatment and late toxicity as any adverse event occurring after 90 days from the start of treatment . follow - up after re - irradiation consisted of a physical examination and psa blood testing every 3 months for the rst 2 years and every 6 months thereafter . 
metabolic imaging or mri were performed in case of psa persistence or biochemical progression . study endpoint and statistical analysis toxicity assessment was the primary endpoint of the study . the secondary endpoints were biochemical relapse - free survival ( brfs ) , distant progression - free survival ( dpfs ) , and overall survival ( os )  . 
a p - value 0.05 indicated a signicant association . results patient and treatment characteristics between december 2014 and december 2019 , 24 patients with recurrent pca were treated with vmat resbrt . primary staging according to the damico classication was low risk in 13% ( n = 3 ) , intermediate risk in 46% ( n = 11 ) , and high risk in 41% ( n = 10 )  . 
the rst rt courses were as follows : denitive ebrt in 11 patients ( median total dose 72 gy , range 7080 gy ) delivered with conventional fractionation ; postoperative ebrt ( either with adjuvant or salvage intent ) in 11 cases ( median total dose of 66 gy , range 6670 gy ) delivered with conventional fractionation , including one patient who also received a brachytherapy boost ; and brachytherapy alone in two patients . 
for bladder and rectum , the median cumulative bed values are reported in table 2 . moreover , the treatment was scheduled in consecutive fractions for six patients and on every other day for the remaining 18 cases . 
death occurred after 39 and 48 months from the second rt course . the median psa nadir after resbrt was 0.23 ng / ml ( range 0.074.27 ng / ml )  . 
all patients relapsed with oligometastatic disease in the pelvic lymph nodes ( ve cases ) or bone metastases ( two cases ) , and were treated with sbrt to all active disease sites . 
at univariate analysis , no clinical parameter was found to be predictive for survival outcomes . table 3 acute genitourinary and gastrointestinal toxicity in detail table 4 late genitourinary and gastrointestinal toxicity in detail genitourinary urinary tract pain urinary urgency hematuria gastrointestinal diarrhea rectal tenesmus rectal bleeding genitourinary urinary tract pain urinary stenosis hematuria gastrointestinal diarrhea rectal tenesmus rectal bleeding 632 fig . 
2 1and 2 - year overall survival rates strahlenther onkol ( 2020 ) 196 : 628636 acute gu acute gi late gu late gi g1 g2 g3 discussion lately , brachytherapy has been the most frequently used option for the treatment of pca local recurrences after an initial rt course , since it theoretically allows the delivery of high radiation doses to the target with a minimal exposure of nearby healthy structures . 
nonetheless , despite reporting satisfactory outcomes in terms of brfs , a non - negligible proportion of patients experienced grade 3 or higher toxicity , including macroscopic hematuria or bladder stulas [ 26 , 27 ]  . of note , brachytherapy also requires invasive procedures that are not always feasible in elderly patients . technological improvements in ebrt delivery have led to an increasing interest in its use in the re - irradiation setting , especially with hypofractionated schedules . 
in fact , as reported by zilli et al . , the use of conventional fractionation in re - irradiation may be detrimental not only in terms of low disease control , but also an increased risk of normal tissue injury [ 28 ]  . this was also conrmed by a preliminary study by rutenberg et al . 
in a small cohort of 11 patients treated with conventionally fractionated re - irradiation after primary brachytherapy , observing a 36% incidence of grade 2 gu toxicity [ 29 ]  . thus , in recent years , evidence in support of sbrt reirradiation has grown , mainly based on the use of robotic sbrt . 
 [ 33 ] collected data from 100 locally recurrent pca patients treated with either ck ( n = 81 ) or linac - based sbrt ( n = 19 ) , showing encouraging results in terms of biochemical control and two cases of grade 3 toxicity ( table 5 ; [ 1618 , 20 , 3034 ] )  . to date , limited evidence for linac - based sbrt in prostate re - irradiation is available . 
interestingly , scheduling the treatment on alternate days instead of consecutive days might have resulted in a safer toxicity prole , even if the present correlation was not statistically signicant , likely due to the small study population . 
notably , unlike dagostino et al . , we did not consider grade 3 toxicity after primary rt as an exclusion criterium for resbrt , as two patients in our sample experienced grade 3 toxicity after the rst radiotherapy course . 
nevertheless , both patients reported no serious adverse events after re - irradiation , reinforcing the safety prole of linac - based sbrt . despite being early , the biochemical control rates reported in the present series are encouraging and in agreement with previously published experiences . 
we must underline that three oligometastatic patients , who are more likely to develop further metastases , were treated with sbrt at all the active disease sites and were included in our study . due to the small sample size , no potential predictive factors for clinical outcomes have been identied . nonetheless , it is worth noting that only a few patients received concurrent adt ( four out of 24 )  . 
this supports the use of re - irradiation as a reliable treatment strategy for delaying the start of adt , as adt is known to negatively impact quality of life due to the large number of related toxicities [ 35 , 36 ]  . 
conversely , all patients who developed distant progression were treated with a new course of sbrt , including one patient who presented a further prostate bed relapse and underwent a second sbrt retreatment . 
adt with sbrt was administered in four cases of disease progression based on high psa relapse levels , resulting in 1and 2 - year adt - free survival rates of 87 and 75% , respectively . 
lastly , no quality of life assessment was performed . conclusion to the best of our knowledge , this is one of the largest series of linac - based sbrt for re - irradiation of prostate cancer . 
the present study aimed to evaluate outcome and early and late toxicity in a cohort of patients with lowand intermediate - risk pc treated prospectively with linear accelerator ( linac ) - based sbrt . patients and methods patients with lowor intermediate - risk ( nccn criteria ) pc were included . 
endpoints were toxicity , biochemical relapse - free survival ( brfs ) , metastatic progression - free survival ( mpfs ) , and overall survival ( os )  . results from 2012 to 2018 , 178 patients were treated . 
gi toxicity positively correlated with prostate volume . conclusion at long - term follow - up , linac - based sbrt continues to be a valid option for the management localized pc . biochemical control remains high at 5 years , albeit with some concerns regarding the optimal schedule for unfavorable intermediate - risk pc . 
considering the excellent prognosis , patient selection is crucial for prevention of severe late toxicity . keywords sbrt gantry radiotherapy prostate - specic antigen linac ( cid : 2 ) assistant professor ciro franzese , md ciro.franzese@hunimed.eu 1 radiotherapy and radiosurgery department , humanitas clinical and research hospitalirccs , via manzoni 56 , rozzano , milan , italy 2 department of biomedical sciences , humanitas university , rozzano , via manzoni 113 , 20089 , milan , italy prostate cancer ( pc ) is the second most common cancer in men [ 1 ]  . 
nowadays , management of pc includes various approaches and techniques , such as observation , surgery , standard radiotherapy ( rt ) , and androgen deprivation therapy ( adt )  . 
these methods are either used exclusively or in strahlenther onkol ( 2020 ) 196 : 608616 combination , depending on stage and risk assessment [ 2 ]  . in recent years , many radiobiology studies have shown that the alpha / beta ratio value of pc is very low , suggesting that hypofractionated rt with higher daily doses may lead to a better or equivalent therapeutic response , while simultaneously reducing the risk of toxicity to surrounding healthy tissues [ 35 ]  . newer technologies such as intensity - modulated rt ( imrt ) and image - guided rt ( igrt ) have helped physicians to achieve this goal by maintaining an acceptable therapeutic ratio with excellent dose conformity . 
consequently , stereotactic body radiation therapy ( sbrt ) with a daily dose equal to or higher than 5 gy per fraction is now emerging as a denitive therapeutic option . 
sbrt already offers a standard alternative to surgery for local treatment in many anatomic locations and types of cancer [ 68 ]  . to date , many phase ii single - institution studies , the majority including cyberknife ( accuray , sunnyvale , ca , usa ) series , are available to show the effectiveness and safety of sbrt in patients with lowand intermediate - risk pc [ 9 ]  . 
however , due to a lack of long - term follow - up and the absence of late toxicity data , this treatment is not universally accepted . the aim of the present study was to evaluate outcomes and early and late toxicity in a large cohort of patients prospectively treated with linac - based sbrt . patients and methods study population this monocentric analysis included patients with a diagnosis of prostate adenocarcinoma classied as lowor intermediate - risk disease according to national comprehensive cancer network ( nccn ) criteria [ 10 ]  . 
the stratication of patients was performed according to nccn guidelines ( version 4 , 2019 ) as follows : ( cid : 2 ) low risk : patients with initial psa ( ipsa ) ( cid : 2 ) 10 and gleason score ( gs ) ( cid : 2 ) 6 and stage t1t2a ; ( cid : 2 ) favorable intermediate risk : one of the nccn intermediate - risk factors , gs 3 + 3 or 3 + 4 , psa 1020 ng / ml , and less than 50% of biopsy cores positive ; ( cid : 2 ) unfavorable intermediate risk : two or three of the nccn intermediate risk factors and / or gs 4 + 3 and / or less than 50% of biopsy cores positive . the study was conducted in accordance with good clinical practice guidelines as well as the ethical principles of the declaration of helsinki and local regulations . 
patients were treated with a rapidarc ( varian medical systems , palo alto , ca , usa ) technique and attening lter - free ( fff ) beams with one or two full arcs . 
in case of a full bowel or empty bladder , patients were invited to complete their preparation and then reveried . response assessment follow - up evaluation was performed every 3 months for the rst year and every 6 months thereafter . 
toxicity was regularly recorded during treatment and follow - up . 610 statistical analysis endpoints of the present study included biochemical relapse - free survival ( brfs ) , metastatic progression - free survival ( mpfs ) , and overall survival ( os )  . 
prostate specic survival ( pss ) was dened as the time from sbrt to death from pc or last follow - up . univariate analysis was performed with the log - rank test and cox proportional hazards regression was used to estimate hazard ratios ( hr )  . 
multivariable cox regression analysis was performed to evaluate the association between clinical factors and survival , with a signicance level of p < 0.05. the pearson productmoment correlation coefcient was used to evaluate the strength and direction of association existing between two continuous variables ( organs at risk and target parameters against incidence of toxicity )  . 
statistical calculations were performed using stata , version 14 ( statacorp , college station , tx , usa )  . results data from 178 patients treated from march 2012 to november 2018 were included in the analysis . 
the rst 13 ( 7.3% ) patients of the series underwent ultrasound - guided positioning of spaceoar hydrogel ( augmenix , inc . , bedford , ma , usa ) between rectum and prostate before rt ; recruitment was continued without spaceoar thereafter , mainly for dosimetric reasons . 
we observed 41 ( 23% ) , 13 ( 7.30% ) , and 1 ( 0.56% ) patient reporting grade 1 , 2 , and 3 late gu toxicity , respectively . 
2 kaplanmeier curves for biochemical relapse - free survival ( brfs ) for the whole population ( a ) , brfs according to international society of urological pathology ( isup ) grade group ( b ) , metastases progression - free ( mpfs ) survival ( c ) , and overall survival ( os , d )  . 
3 shows scatter plots of acute gi toxicity against bladder , rectal , and ctv volume . discussion the present study conrms the long - term efcacy of sbrt in the management of localized pc . 
recently , the hypo - rt - pc trial [ 13 ] included 1200 localized pc patients treated with a sevenfraction sbrt regimen or conventional rt ( crt )  . 
while 2 - year brfs for the entire cohort was 92% , it was 97 and 85% , respectively , for the isup 2 and 3 groups . the major american association of rt , oncology , and urology ( astro , asco , and aua ) has recently produced an evidence - based guideline for hypofractionation in rt for pc [ 16 ]  . 
no data are reported on the association of acute toxicity with disease and organs at risk characteristics . a prospective study on dose escalation was recently published by zelefsky et al . 
neither grade 3 or 4 acute rectal toxicities nor urinary toxicities were observed . patients included in the present analysis had a median ctv volume of 61 cm3 ( range : 27141 cm3 )  . 
the only patient who reported grade 3 gi toxicity had a ctv volume of 112 cm3 , compared to a mean volume of 87.8 cm3 for patients experiencing grade 2 and 59.5 cm3 for patients reporting grade 1 side effects . considering the good outcomes in terms of disease control , the quality of life of pc patients should be subject to attention even at long - term follow - up . 
we had 1 ( 0.56% ) grade 3 gu strahlenther onkol ( 2020 ) 196 : 608616 included population only , we decided to include only physician - reported toxicity in the study . conclusion even at long - term follow - up , linac - based sbrt seems to be a valid option for the management localized pc . 
april 2020 der / die autor ( en ) 2020 hintergrund der zustzliche nutzen der adjuvanten radiotherapie bei patientinnen mit niedrigrisikomammakarzinom im vergleich zu einer alleinigen endokrinen therapie nach brusterhaltender therapie in bezug auf die verhinderung eines lokalrezidivs ist mehrfach belegt durch randomisiert - kontrollierte studien . 
die vorliegende arbeit prsentiert nun die 10 - jahres - daten der abcsg - 8a - studie aus sterreich . patienten und methodik die abcsg - 8a - studie ist eine randomisiert - kontrollierte phase - iii - studie und stellt eine substudie der abcsg - 8 - studie dar , in der randomisiert 5 jahre tamoxifen mit 2 jahren tamoxifen , gefolgt von 3 jahren anastrozol , verglichen wurde . 
anhand dieser kriterien ( her2 - positiv oder ki67 > 20 % ) wurden 8 % der patientinnen als hochrisikopatientinnen eingestuft . ergebnisse die mediane nachbeobachtungszeit betrug 9 , 9 jahre . 
das lokalrezidivfreie berleben ( lrfs ) nach 10 jahren lag im bestrahlungsarm bei 97 , 5 % , verglichen mit 92 , 5 % nach alleiniger endokriner therapie ( hazard ratio 0 , 27 ; p < 0 , 001 )  . 
neben der radiotherapie war der einzige weitere signikante prognosefaktor hinsichtlich des lrfs das grading , nicht aber die tumorbiologie ( bei allerdings < 10 % hochrisikofllen )  . schlussfolgerungen die autoren schlussfolgern , dass die adjuvante bestrahlung der operierten brust auch bei mammakarzinomen mit einem niedrigen risiko das lokalrezidivfreie wie auch das krankheitsfreie berleben signikant verbessert . 
allerdings bertrgt sich dieser vorteil nicht in ein verlngertes gesamtberleben . originalpublikation fastner g , sedlmayer f , widder j et al ( 2020 ) endocrine therapy with or without whole breast irradiation in low - risk breast cancer patients after breast - conserving surgery : 10 - year results of the austrian breast and colorectal cancer study group 8a trial . 
eur j cancer 127 : 1220 kommentar ( cid : 2 ) david krug david.krug@uksh.de 1 klinik fr strahlentherapie , campus kiel , universittsklinikum schleswig - holstein , arnold - heller - str . 
3 , haus l , 24105 kiel , deutschland jena , deutschland die adjuvante radiotherapie der operierten brust nach brusterhaltender operation senkt das lokale rezidivrisiko und verbessert das brustkrebsspezische und das gesamtberleben [ 1 ]  . 
schon in den metaanalysen der early breast cancer trialists cooperative group wurde aber gezeigt , dass der absolute vorteil hinsichtlich der vermeidung eines lokalrezidivs und damit die number needed to treat deutlich vom risikoprol abhngt und fr niedrigrisiko672 strahlenther onkol ( 2020 ) 196 : 671673 patientinnen kein gesamtberlebensvorteil resultiert [ 1 ]  . eine vielzahl randomisiert - kontrollierter studien untersuchte daher den stellenwert der radiotherapie zustzlich zu einer endokrinen therapie im vergleich zur alleinigen endokrinen therapie in diesem setting ( zumeist pt12 [ < 3 cm ] pn0 , hormonrezeptor - positiv , g12 , alter variabel ; [ 27 ] )  . 
in einer metaanalyse dieser studien war der verzicht auf eine adjuvante radiotherapie mit einem 6 , 8fach hheren risiko fr ein lokalrezidiv vergesellschaftet ; allerdings bestand kein nachteil hinsichtlich des gesamtberlebens [ 8 ]  . 
bislang hatte nur eine studie , nmlich die nordamerikanische calgb - 9343 - studie , langzeitergebnisse nach einer mittleren nachbeobachtungszeit von 12 , 6 jahren prsentiert [ 5 ]  . 
verglichen mit den 5 - jahresdaten kam es hier zu einem anstieg der lokalrezidivrate von 1 auf 2 % im bestrahlungsarm , aber von 4 auf 10 % bei alleiniger endokriner therapie . 
gegenber den 5 - jahres - daten [ 6 ] stieg die lokalrezidivrate von 0 , 5 auf 2 , 5 % im bestrahlungsarm an , verglichen mit 5 , 1 und 7 , 6 % nach alleiniger endokriner therapie . 
eine verbesserung des krankheitsfreien berlebens konnte bislang nur in der kanadischen studie gezeigt werden , die allerdings vielfach kritisiert wurde , da knapp 20 % der patientinnen einen negativen oder unbekannten hormonrezeptorstatus und > 30 % einen niedrigen oder unbekannten differenzierungsgrad aufwiesen [ 4 ]  . die ergebnisse der abcsg - 8a - studie sind insofern wichtig , weil sie besttigen , dass der vorteil der adjuvanten radiotherapie mit steigender nachbeobachtungszeit nicht ab - , sondern zunimmt . 
die beobachtung , dass die dfs - verbesserung durch die bestrahlung bei patientinnen mit slne statistische signikanz erreichte , nicht aber nach erfolgter axilladissektion , ist zustzlich interessant . die autoren vermuten , dass dies durch falsch - negative ergebnisse der slne bedingt sein knnte und die okkulten lymphknotenmetastasen durch die tangentiale radiotherapie miterfasst und dadurch eliminiert werden [ 10 ]  . 
durch den verzicht auf die slne in der insemastudie , wird diese annahme prospektiv auf den prfstein gestellt werden . fazit die ergebnisse der abcsg - 8a - studie besttigen die effektivitt der adjuvanten radiotherapie bei patientinnen mit niedrigrisikomammakarzinom auch bei lngerer nachbeobachtungszeit , wobei der absolute vorteil mit steigender nachbeobachtungszeit zunimmt . 
duma geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
early breast cancer trialists collaborative group ( ebctcg ) , darby s , mcgale p et al ( 2011 ) effect of radiotherapy after breastconserving surgery on 10 - year recurrence and 15 - year breast cancer death : meta - analysis of individual patient data for 10 , 801 women in 17 randomised trials . 
blamey rw , bates t , chetty u et al ( 2013 ) radiotherapy or tamoxifen after conserving surgery for breast cancers of excellent prognosis : british association of surgical oncology ( baso ) ii trial . eur j cancer 49 : 19 . 
fyles aw , mccready dr , manchul la et al ( 2004 ) tamoxifen with or without breast irradiation in women 50 years of age or older with early breast cancer . 
hughes ks , schnaper la , bellon jr et al ( 2013 ) lumpectomy plus tamoxifen with or without irradiation in women age 70 years or older with early breast cancer : long - term follow - up of calgb 9343 . j clin oncol 31 : 23822387 . 
ptter r , gnant m , kwasny w et al ( 2007 ) lumpectomy plus tamoxifen or anastrozole with or without whole breast irradiation in women with favorable early breast cancer . 
tinterri c , gatzemeier w , costa a et al ( 2013 ) breast - conservative surgery with and without radiotherapy in patients aged 5575 years with early - stage breast cancer : a prospective , randomized , multicenter trial analysis after 108 months of median follow - up . ann surg oncol 21 : 408415 . 
matuschek c , blke e , haussmann j et al ( 2017 ) the benet of adjuvant radiotherapy after breast conserving surgery in older patients with low risk breast cancera meta - analysis of randomized trials . radiat oncol 12 : 6068 . 
borm kj , oechsner m , dsberg m et al ( 2020 ) irradiation of regional lymph node areas in breast cancerdose evaluation according to the z0011 , amaros , eortc 10981 - 22023 and ma - 20 eld design . 
this study reports a minute - by - minute association and calculates the impact of this displacement on duration - dependent margins using real - time intra - fractional position data monitored by four - dimensional transperineal ultrasound ( 4d tpus )  . materials and methods a total of 55 patients were recruited prospectively . 
linear regression analysis was then performed on the overall margins against time and direction . results the mean intra - fractional position was 0.76 mm inferior ( inf ) , 0 mm lateral ( lat ) and 0.94 mm posterior ( post ) at the 15th minute . 
a minimum margin expansion of 2.42 mm ( superior / inf ) , 1.02 mm ( left / right ) and 2.65 mm ( anterior / post ) was required for an 8 - minute treatment compared to 4.29 mm ( sup / inf ) , 1.84 mm ( lt / rt ) and 4.63 mm ( ant / post ) for a 15 - minute treatment . 
the required margin increases linearly in all directions within the 15 - min duration ; thus , the margin will depend on the duration of the technique chosen ( imrt / vmat / 3dcrt / proton )  . keywords margins intra - fractional prostate displacement prostate cancer real - time tracking transperineal ultrasound part of the ndings in this manuscript was presented at astro 2019 conference in chicago , usa , in a poster entitled : estimation of duration - dependent margins for prostate radiotherapy . ( cid : 2 ) eric pei ping pang , phd eric.pang.p.p@nccs.com.sg faculty of medicine , nursing and health sciences , department of medical imaging & radiation sciences , monash university , wellington road , clayton vic , 3800 melbourne , australia 3 duke - nus graduate medical school , 8 college road , 169857 singapore , singapore 1 division of radiation oncology , national cancer centre singapore , 11 hospital crescent , 169610 singapore , singapore 4 division of medical sciences , national cancer centre singapore , 11 hospital crescent , 169610 singapore , singapore 658 introduction integral to modern precision radiotherapy , accuracy in treatment delivery remains one of the popular research areas in prostate radiotherapy . 
the importance of accounting for such intra - fractional prostate displacement has been highlighted in hypo - fractionated stereotactic body radiation therapy ( sbrt ) regimes [ 2 , 3 ]  . 
although pre - treatment correction is performed online based on the arbitrary position captured by cone - beam computed tomography ( cbct ) , patients experience continuous intra - fractional displacement of the prostate while lying on the treatment couch during the imaging and verication phase . 
we believe that the lapsed duration while performing the image verication before treatment should be accounted for , as the variance of motion increases in a linear fashion temporally [ 4 ]  . 
in addition , the duration of imaging and verication can be longer than the actual treatment delivery [ 7 ]  . previous studies have reported an intra - fractional prostate displacement trend towards the inferior and posterior directions [ 5 , 8 ]  . 
the clinical motivation of this paper is to provide insights and characterise the trend of margin required with respect to overall duration ( including during both the imaging and treatment phase )  . 
this study reports our experience in estimating a minute - by - minute ( up to 15 min ) duration - dependent margin using real - time intra - fractional prostate displacement monitored by fourdimensional transperineal ultrasound ( 4d tpus )  . materials and methods ethics approval was obtained through the local ethics committee in november 2014 and informed consent was obtained from each patient . 
all the patients were instructed to comply with a bladder preparation protocol by voiding their bladder followed by drinking strahlenther onkol ( 2020 ) 196 : 657663 400 ml of water and waiting for 30 min to obtain a comfortably full bladder . 
the rationale for this was that when the study commenced , cbct was the gold standard for correction of setup errors ( internationally as well as in our department )  . the aim of this study was to evaluate whether tpus could replace or complement cbct . 
until such time as we had evidence to support a change in practice , cbct continued to be used for correction of setup errors for all study participants . intra - fractional monitoring and margin estimation a non - invasive and non - ionising 4d tpus clarity system ( elekta ab , stockholm , sweden ) was used to supplement and provide real - time monitoring ( central frequency of 4.5 mhz ) of the intra - fractional prostate position . 
once a week , patients were asked to remain in the treatment position after vmat treatment for an extended 7 min of monitoring to simulate a prolonged imrt treatment duration . 
the cumulative displacements of prostate position up to the 15th minute timepoint illustrated in table 2 were prepared for margin calculation . table 3 compares the percentage of intra - fractional prostate displacement that occurred between various thresholds from 3 mm , 4 mm and 5 mthe overall percentage of position was highest in the lt / rt direction for all thresholds and a minimum of 95% of the motion lies within 4 mm in all directions . ( ) / inferior ( + ) , left ( ) / right ( + ) and anterior ( + ) / posterior ( ) directions . 
linear regression analysis was performed on the overall margins against time and direction . distribution of intra - fractional prostate motion 6 , 389 , 866 displacement values were analysed and a histogram was plotted . 
2 prostate displacement across time 660 strahlenther onkol ( 2020 ) 196 : 657663 trend of duration - dependent margin the mean intra - fractional prostate displacement was 0.76 mm ( sup / inf ) , 0 mm ( lt / rt ) and 0.94 mm ( ant / post ) at the 15th minute . 
3 , a linear relationship was observed among the required margin over the 15 - minute period for the respective directions . a linear regression of overall margins was modelled against time and direction . 
further exploration of the interaction term between time and direction suggests its signicant role ( p < 0.01 ) , indicating a difference in the rate of increase of the required margins among the different directions . 
the required margin as ( 4.534.73 mm ) , a function of time increased linearly in all directions ( r2 = 0.99 for all positions )  . from the plot of margins against time in fig . 
3 , it was observed that the margin values respective of time duration in the sup / inf and ant / post directions were much higher than those in the lt / rt direction . 
however , no signicant difference ( p = 0.10 ) in the overall margins was observed between sup / inf and ant / post directions . discussion cbct is often regarded as the gold standard imaging modality for daily pre - treatment localisation of prostate cases . 
the rationale is due to the on - going intrafractional position changes during image acquisition and verication , a process longer than actual treatment delivery but not captured by cbct . 
even with the emergence of magnetic resonance imaging - guided ( mri - guided ) radiation therapy , where the patient is imaged using cine mode ( continuous ) mri to quantify internal displacement while waiting for online adaptation to be completed , real - time imaging would help the radiation therapists to ensure that the target has not shifted after the period of delay in re - planning . 
this would avoid reliance on outdated geometrical information that was captured several minutes before initiating the treatment . the ndings from this study provide insights into the trend and magnitude of minimum planning margins as a function of time up to a 15 min duration . 
on the other hand , the adoption of techniques with shorter treatment times will reduce motion uncertainties , and technological capabilities such as the use of vmat and attening lter - free ( fff ) techniques may be regarded as the new conventional standard in the near future . the need for duration - dependent margins was also reported by sihono et al . 
in addition , endorectal balloons were used , but the consistency and daily position of the endorectal balloons was not assessed . an earlier paper by adamson and wu [ 11 ] also cautioned potentially exaggerating the magnitude of intra - fractional motion using pre - and post - treatment imaging . 
for instance , a gross transient magnitude of 68 mm ( lasted for one second ) detected in the superior direction in this paper would not have triggered the need for any motion management strategies in practice . 
additionally , a minimal dosimetric impact is expected due to the outliers , given the small percentage ( 1.11% ) of prostate position data that lies beyond 6 mm in fig . 
with gating or tracking techniques , the potential reduction of the ptv margins is possible , particularly in the sup / inf and ant / post directions for long fraction duration reported in this study . 
one of the prerequisites for the availability of automatic tracking lies in the compatibility of the motion management interface of the linear accelerators with the 4d tpus system used in this study . 
the duration - dependent margin reported in this study may provide an alternative motion mitigation solution in the absence of the technology - laden solutions such as mlc tracking or mri - linac . 
however , the potential impact of the tpus probe pressure at the perineum stabilizing the prostate and consequently limiting the intra - fractional prostate motion and overall displacement was not investigated here . 
however , this technique is recommended only for lowto intermediate - risk patients and the invasive nature of this procedure may pose injectionrelated complications and may be subject to the operators experience and consistency [ 15 ]  . 
nonetheless , some form of tracking or beam - holding should be considered if the applied planning margin is smaller than the recommended margin for hypo - fractionated sbrt regimes . 
besides , the ability to automatically beam hold during motion tracking is hugely pertinent to overcome the issues of transient gross displacement during treatment with a magnitude of displacement beyond 1 cm for all directions as reected in table 1 . 
lastly , from a cost - efciency perspective , to mitigate target displacement , duration - dependent margins may be applied safely and are not limited by clinical indications . the approach of the study to employ duration - dependent margins has some inherent limitations . 
pre - emptively , physicians should consider an appropriate margin to apply during target delineation based on a mean imaging duration and treatment delivery time estimated from the treatment plan . 
besides , the duration - dependent margin also assumes that gross random prostate displacement from individual patients is transient and has minimal impact on the overall dosimetry and treatment delivery . 
ideally , automatic beam - holding interface is the desirable motion management strategy , where a reduced margin can be applied independent of the durationdependent margin recommendation from this study . conclusion we reported our initial experience in deriving the minimum duration - dependent margin to generate the required planning target volume for prostate radiotherapy . 
the duration - dependent margins would provide an alternative form of motion mitigation solution . acknowledgements the authors express their appreciation to elekta pte ltd for providing the 4d tpus clarity equipment and in - house training . 
chua reports personal fees from astellas ; personal fees from janssen ; grants and personal fees from ferring ; grants , personal fees and non - nancial support from varian ; non - nancial support from astrazeneca ; non - nancial support from genomedx biosciences ; non - nancial support from medlever inc ; non - nancial support from pvmed inc . ; outside the submitted work . 
kirschner2 received : 12 october 2019 / accepted : 11 january 2020 / published online : 31 january 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract purpose merkel cell carcinoma is highly sensitive to both radiation and immunotherapy . 
moreover , concurrent radioimmunotherapy may capitalize on anti - tumor immune activity and improve merkel cell treatment response , although an enhanced immune system may cross - react with native tissues and lead to signicant sequelae . methods here we present a case study of a patient with metastatic merkel cell carcinoma treated with radiotherapy concurrent with pembrolizumab . results after radioimmunotherapy , the patient developed sensory neuropathy , visual hallucinations , and mixed motor neuron ndings . 
neurologic dysfunction progressed to profound gastrointestinal dysmotility necessitating parenteral nutrition and intubation with eventual expiration . conclusion this case represents a unique autoimmune paraneoplastic neurologic syndrome , likely specic to neuroendocrine tumors and motivated by concurrent radioimmunotherapy . 
recognition of the potential role of radioimmunotherapy may provide an advantage in anticipating these severe sequelae . keywords checkpoint inhibitor autoimmunity radioimmunotherapy paraneoplastic neurologic syndrome merkel cell carcinoma introduction merkel cell carcinoma ( mcc ) is an aggressive radiosensitive cutaneous neuroendocrine malignancy occurring in older adults . 
recent phase ii data have shown > 50% response rates with checkpoint inhibition for metastatic mcc leading to food and drug administration ( fda ) approval of avelumab and pembrolizumab [ 14 ]  . 
hypotheses for these promising responses to immunotherapy include the clonal integration of the merkel cell polyomavirus in up to 80% of cases , as well as a high ultraviolet light - driven mutational burden in tumors without polyomavirus [ 5 , 6 ]  . 
multiple observations corroborate the clinical importance the immuno - oncologic axis in mcc , including a reduction in mcc - specic survival with systemic immunosuppression , a reduction in overall survival with high viral load , and an improvement in overall survival with high intratumoral cytotoxic t cells [ 7 , 8 ]  . interestingly , however , even this highly immunogenic tumor can become resistant to immunotherapy , and in this setauthor contributions all authors contributed to the study conception and design , data collection , and interpretation . 
mechanisms of this synergy include radiation - induced generation of neoantigens and neoepitopes , radiation modulation of the t - cell receptor repertoire , and anti - cancer tumor microenvironmental changes secondary to radiation [ 1115 ]  . however , while these data are promising , a therapeutically enhanced immune system , further bolstered by radiotherapy , can also attack native tissues , as immune augmentation is not specic to malignant cells and can obstruct host efforts at maintaining self - tolerance . 
such off - target t - cell activation as a result of immunotherapy has been frequently observed as a low - grade toxicity of the skin , lungs , or gastrointestinal system , although severe toxicities of other organ systems have been reported [ 16 , 17 ]  . 
the forearm was treated with 9 mev electron beam radiotherapy with a 1 cm bolus to a dose of 50.4 gy in 28 fractions ( prescribed to 90% isodose line ) with concurrent carboplatin and etoposide , based on available data at that time [ 18 ]  . seven months after treatment , interval pet / ct demonstrated right axillary nodal avidity , conrmed pathologically in 1 / 33 nodes after dissection . 
this was treated with denitive photon - based three - dimensional conformal rt to a cumulative dose of 60 gy in 33 fractions with concurrent carboplatin / etoposide . chemotherapy was held for 1 week during admission for neutropenic fever . three months post chemoradiotherapy , the patient had biopsy - proven recurrent mcc in the right forearm inferior to the antecubital fossa and the right proximal upper extremity . 
during imrt , he was diagnosed with a cutaneous mcc nodule on the lateral aspect of the right upper abdominal quadrant and a synchronous nodule at the inferior border of right breast tissue . 
these foci were treated with imrt twice daily to a dose of 45 gy in 30 fractions . two months after imrt , he recurred with gross cutaneous nodules on the right chest and axilla , all within the radiation portal of previous treatments . 
after continued local progression , he was treated with shortcourse high - dose imrt to 30 gy in 5 fractions concurrent with a third dose of pembrolizumab , since short - course 666 strahlenther onkol ( 2020 ) 196 : 664670 fig . 
1 gastric dysmotility evaluated by axial ct abdomen showing a circumferential thickening in the distal esophagus ( arrow ) and b gastric distention ; c upper gastrointestinal series showing multifocal esophageal narrowing high - dose rt had been reported to achieve durable palliation and an abscopal effect in metastatic mcc as well as a need to reduce the risk of reirradiation [ 19 ]  . 
his lesions responded well to rt , but all tumor - directed therapy was held for 3 months due to transfusion - dependent anemia , thrombocytopenia , red cell aplasia , and pneumonitis managed with prednisone . 
since he was not a candidate for chemotherapy due to thrombocytopenia and because he initially responded well to pembrolizumab , he received concurrent radioimmunotherapy with 24 gy in three nonconsecutive fractions of 9 mev electron beam with a 1.5 cm bolus ( prescribed to 95% isodose line ) to the right shoulder and one dose of pembrolizumab . on the last treatment day , the patient reported new shooting neuropathic pain of the right upper extremity and was prescribed gabapentin and hydrocodone / acetaminophen . three days later , he was admitted with visual hallucinations , deteriorating mobility , and constipation . 
he had hyperreexia in the left upper extremity ( right upper extremity was bandaged and not assessed ) , as well as hyperreexia with nonsymmetric lower extremity clonus ( left lower extremity : 15 + beats ; right lower extremity : 3 beats )  . brain mri with contrast was unremarkable except for a small focus of enhancement within the anteromedial left cerebral peduncle lacking t2 hyperintensity or edema ; this was stable compared to previous scans and interpreted as artifactual . 
cerebrospinal uid was notable for mildly elevated total protein , albumin , and iggindex ( 0.85 ) without oligoclonal immunoglobulmayo clinic laboratories csf paraneoplastic autoantibody panel ( mayo clinic laboratories , rochester , mn , usa ) was negative . after spontaneous improvement with supportive care and discontinuation of medications with potential to exacerbate his symptoms , steroids were deferred , and he was discharged . 
this dysfunction manifested on the nal day of radioimmunotherapy with nonlocalizable upper and lower motor neuron dysfunction and sensory neuropathy , without imaging correlates , that progressed to fatal enteric plexus neuropathy refractory to immunosuppression . 
although enteric neuropathy was apparent on imaging , no anatomic abnormalities were identied endoscopically . taken together , these ndings suggest an autoimmune , paraneoplastic neurologic syndrome specic to mcc and potentially motivated by combination radioimmunotherapy . similar autoimmune paraneoplastic neurologic syndromes have been reported in metastatic mcc treated with immunotherapy , but never in the context of radioimmunotherapy [ 2022 ]  . 
combined checkpoint inhibition , rather than single - agent immunotherapy , is linked to an increased risk of immune - related adverse events , suggesting a proportional relationship between immunostimulation and toxicity [ 23 ]  . 
rt , as an immunomodulator , can generate endogenous anti - tumor vaccines through immunogenic cell death , as tumor antigens are made available by radiotherapy for immune - stimulating presentation [ 24 ]  . 
because of this property , concurrent radioimmunotherapy may be plausibly employed to attempt to induce the abscopal effect , whereby distant tumor foci regress after local rt due to anti - tumor immunity [ 2527 ]  . 
however , just as efcacy is increased by synergism , combination radioimmunotherapy may also increase immune - related toxicity , such as that manifested in our patient [ 28 ]  . 
furthermore , it is also possible that these effects were simply a result of a paraneoplastic syndrome induced by the cancer itself and unrelated to either treatment . further preclinical and clinical study of the interaction between radiation , immunotherapy , and mcc is necessary to more conclusively establish causality and offer evidencebased recommendations . due to multiple overlapping courses of radiation , we retrospectively reviewed cumulative dosimetry to evaluate the possibility of radiation - induced ileus or enteric toxicity ( table 2 )  . 
1 , 2 and 3 , lessening the likelihood of this diagnosis [ 2932 ] .1 as a neuroendocrine tumor sharing a neural crest embryologic origin with enteric neurons , mcc may express neural antigens that increase the risk of paraneoplastic neurologic autoimmunity [ 3336 ]  . 
immunologic recognition of neural antigens presented by tumor cells may be fueled in the setting of checkpoint blockade , which suppresses im1 timmerman r ( 2014 ) personal communication mune regulatory pathways that normally function to promote self - tolerance , leading to neurologic sequelae [ 37 ]  . similar autoimmune paraneoplastic neurologic syndromes have been reported in melanoma and small cell lung cancer , which share similar neural embryologic origins [ 38 , 39 ]  . however , a humoral mechanism of disease , either primary or in addition to cellular autoimmunity , cannot be ruled out in this patient , although typical mcc paraneoplastic autoantibodies were undetectable [ 40 ]  . recommendations notably , our patient reported a globus sensation roughly 3 months after initiating radioimmunotherapy . 
as autoimmune paraneoplastic syndromes continue to be studied in mcc treated by immunotherapy , early clinical signs such as these may serve as markers of impending disease before irreversible neurologic dysfunction and plexus destruction . conclusion diagnosing paraneoplastic autoimmunity is a unique challenge . 
5k12ca090625 - 18 from the vanderbilt clinical oncology research development program . funding this study did not receive any specic grant from funding agencies in the public , commercial , or not - for - prot sectors . compliance with ethical guidelines conict of interest m.h. 
kirschner declare that they have no competing interests . strahlenther onkol ( 2020 ) 196 : 664670 ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
die in 2020 verffentlichte pout - studie ( peri - operative chemotherapy versus surveillance in upper tract urothelial cancer ) stellt nun die grte multizentrische , prospektive und randomisierte phase - 3 - studie zur wirksamkeit einer adjuvanten chemotherapie nach nephroureterektomie ( nue ) bei patienten mit utuc dar . originalpublikation birtle a , johnson m , chester j et al ( 2020 ) adjuvant chemotherapy in upper tract urothelial carcinoma ( the pout trial ) : a phase 3 , open - label , randomised controlled trial . 
21 , 24105 kiel , deutschland patientengut und methoden einschlusskriterien fr die studie waren : metastasenfreiheit ( m0 ) , lokal fortgeschrittenes tumorstadium oder lymphknotenbefall sowie eine glomerulre filtrationsrate ( gfr ) von mindestens 30 ml / mdas therapiekonzept bestand aus einer adjuvanten chemotherapie mit 4 zyklen zu jeweils 21 tagen , die innerhalb von 90 tagen nach der nue ( plus exzision klinisch / radiologisch aufflliger lymphknoten ) begonnen wurde . 
bei niedrigerer gfr wurde cisplatin durch carboplatin ersetzt . sowohl die interventionsals auch die kontrollgruppe wurden in regelmigen abstnden ber im median 30 monate klinisch und radiologisch kontrolliert , die unerwnschten nebenwirkungen der therapie erfasst und ein standardisierter fragebogen zur lebensqualitt ausgefllt . 
sekundre endpunkte waren das gesamtberleben , die compliance , die kurzfristige und langfristige toxizitt der behandlung sowie die lebensqualitt . ergebnisse im zeitraum von juni 2012 bis november 2017 wurden 261 patienten an 57 studienstandorten rekrutiert , wovon in der randomisierung 132 patienten der chemotherapiegruppe und 129 patienten der kontrollgruppe zugeordnet wurden . 
die gfr der patienten lag bei 64 % aller teilnehmer bei 50 ml / min . auf empfehlung des unabhngigen datenberwachungskomitees wurde die patientenrekrutierung vorzeitig beendet , nachdem bereits frhzeitig das kriterium der wirksamkeit erreicht worden war . 
die adjuvante chemotherapie reduzierte dabei das 838 strahlenther onkol ( 2020 ) 196 : 837840 risiko fr das auftreten von rezidiven um 55 % ( hazard ratio [ hr ] = 0 , 45 , 95 % - kondenzintervall ( 95 % - ki ) 0 , 30 , 68 , p = 0 , 0001 )  . 
im vergleich der schtzungen des krankheitsfreien 3 - jahres - berlebens prsentierte die chemotherapiegruppe mit 71 % ( 95 % - ki : 6178 ) wesentlich bessere werte als die kontrollgruppe mit 46 % ( 95 % - ki : 1138 )  . 
in der subgruppenanalyse zeigte sich ein signikanter effekt nur bei patienten der gemcitabin - cisplatin - gruppe ( hr = 0 , 35 , p = 0 , 0002 )  . 
zum zeitpunkt der aktuellen analyse waren in der chemotherapiegruppe 24 todesflle und in der kontrollgruppe 38 todesflle aufgetreten . innerhalb der chemotherapiegruppe traten mit 44 % mehr unerwnschte therapiebedingte ereignisse ( ctcae grad 3 ) auf im vergleich zu 4 % in der kontrollgruppe . 
deshalb wurden diesbezglich zugunsten der durchfhrbarkeit in der pout - studie keinerlei vorgaben gemacht , trotz der gefahr eines under staging durch bersehen von mikrometastasen . kommentar die bisherige literatur zur systemischen therapie des utuc hatte zwar bereits auf die vorteile einer perioperativen chemotherapie hingewiesen [ 13 ] , basierte aber vornehmlich auf retrospektiven studien sowie einzelnen prospektiven studien mit geringen fallzahlen [ 8 ]  . 
in studien zur anwendung der adjuvanten chemotherapie beim utuc prsentierten sich uneindeutige ergebnisse : whrend einige studien signikante berlebensvorteile einer adjuvanten therapie beschrieben [ 10 , 14 ] , zeigten andere keinen effekt auf die prognose der patienten [ 11 , 15 ]  . 
metaanalysen von nichtrandomisierten studien zur adjuvanten chemotherapie beim utuc deuteten auf signikante verbesserungen des gesamtsowie des krankheitsfreien berlebens durch eine adjuvante chemotherapie hin [ 8 ] auerdem knnen durch den einsatz von neoadjuvanten therapieschemata bei utuc - patienten ein signikantes downstaging und pathohistologische remissionen erreicht werden [ 16 , 17 ]  . 
in der summe war die datenlage aber nicht ausreichend , um eindeutige empfehlungen zu geben . bei der pout - studie handelt es sich um die erste prospektive randomisierte phase - 3 - studie zur anwendung einer perioperativen chemotherapie beim urothelkarzinom des oberen harntraktes [ 19 ]  . 
angesichts des mangels an hinlnglichen studien liefert die pout - studie damit zum ersten mal daten zur adjuvanten chemotherapie beim utuc , die aufgrund des studiendesigns in geringerem mae von systematischen fehlern ( bias ) betroffen sind . jedoch mssen bei der beurteilung der ergebnisse einige einschrnkungen innerhalb der studie betrachtet werden : zum einen gab es keine klaren vorgaben zur ( erweiterten ) lymphknotendissektion . 
ein einheitliches vorgehen wre hierbei wnschenswert gewesen , um eine verlssliche aussage dazu treffen zu knnen , ob die adjuvante chemotherapie in der lage ist , auch bei weiter fortgeschrittenen erkrankungen und mikrometastasen eine verbesserung des krankheitsfreien berlebens zu erzielen . 
wie schon von den autoren der pout - studie selbst angesprochen , brchte die neoadjuvante chemotherapie einige vorteile mit sich , sofern es gelnge , die patienten adquat zu selektionieren [ 21 ]  . in den adjuvanten therapieansatz wurden ausschlielich patienten mit einer gfr 30 ml / min eingeschlossen . 
legte man den blichen grenzwert zur gfr von 60 ml / min fr den einsatz von cisplatin zugrunde [ 19 ] , so knnte es sich zeigen , dass nach dem operationsbedingten abfall der gfr ca . 
der altersgipfel der inzidenz des utuc liegt auerdem bei 7090 jahren [ 1 ] , also in einer gruppe , die besonders stark vom postoperativen gfr - abfall betroffen ist und daher hug kontraindikationen sowohl gegen die prals auch die postoperative chemotherapie darstellt [ 22 ]  . in der subgruppenanalyse war ein signikanter effekt nur bei patienten der gemcitabin - cisplatin - gruppe nachweisbar . 
man kann also fr diese subgruppe eigentlich keine empfehlung zu einer adjuvanten chemotherapie aussprechen , da ein vorteil fr das progressionsfreie berleben in dieser speziellen gruppe zunchst erst einmal belegt werden msste . 
sie schliet auch mit mvac ( methotrexat , vinblastin , doxorubicin und cisplatin ) eine weitere chemotherapeutikakombination ein , die beim blasenkarzinom und beim metastasierten utuc in manchen studien ein deutlich verbessertes gesamtberleben im vergleich zur kombination gemcitabin / cisplatin zeigte [ 23 , 24 ]  . und zuletzt konnte wegen der vorzeitigen verffentlichung wesentlicher daten der pout - studie der effekt der adjuvanten chemotherapie auf das gesamtberleben leider noch nicht evaluiert werden . 
mit diesem trick lsst sich aus der signikanten verbesserung des krankheitsfreien berlebens in der pout - studie auch auf eine verbesserung des gesamtberlebens dieser patientengruppe schlieen . fazit es ist sinnvoll , utuc als eigenstndiges krankheitsbild vom urothelkarzinom der blase abzugrenzen und dementsprechend zu behandeln . die forderung der autoren , das adjuvante therapieschema mit gemcitabin / cisoder carboplatin als neuen goldstandard in der behandlung des fortgeschrittenen utuc anzusehen , ist berechtigt , und die daten sollten bei zuknftigen empfehlungen und leitlinien bercksichtigt werden . es besteht noch forschungsund optimierungsbedarf bezglich der patientenselektion und des optimalen therapieregimes . 
dunst geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
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schoppmann1 gerd jomrich1 ivan kristo1 reza asari1 erwin rieder1 andrea beer2 received : 24 july 2019 / accepted : 3 february 2020 / published online : 13 february 2020 the author ( s ) 2020 abstract purpose neoadjuvant radiochemotherapy ( rcth ) is proven to be highly effective in the treatment of esophageal cancer ( ec )  . 
we investigated oncological outcome and morbidity in patients treated with a modied cross protocol followed by esophagectomy at our institution . methods patients with ec receiving neoadjuvant rcth with paclitaxel and carboplatin and concurrent radiotherapy ( 46 gy ) followed by esophagectomy were included in this retrospective analysis . 
histopathological response , overall survival ( os ) and recurrence - free interval ( rfi ) as well as perioperative morbidity were investigated . results thirty - six patients ( 86.1% male , mean age 61.3 years , standard deviation 11.52 ) received neoadjuvant rcth before surgery . 
median os and rfi were not reached . conclusions neoadjuvant radiotherapy with 46 gy and concomitant chemotherapy with paclitaxel and carboplatin for the treatment of locally advanced esophageal carcinoma is safe and effective . 
the results of this modied radiotherapy protocol are encouraging and should be considered in future patient treatment and study designs . keywords neoadjuvant radiochemotherapy esophagus esophageal resection cross protocol prognosis background esophageal cancer ( ec ) is a rare tumor entity associated with a dramatically growing incidence [ 1 ]  . 
schoppmann , md , facs sebastian.schoppmann@meduniwien.ac.at 1 department of surgery , upper gi service , comprehensive cancer center get - unit , medical university of vienna , spitalgasse 23 , 1090 vienna , austria 2 department of pathology , comprehensive cancer center get - unit , medical university of vienna , vienna , austria 3 clinical division of oncology , department of medicine i and comprehensive cancer center , get - unit , medical university of vienna , vienna , austria 4 department of radiation oncology , comprehensive cancer center get - unit , medical university of vienna , vienna , austria provement in therapy , patients are still confronted with poor prognosis [ 2 ]  . 
in locally advanced stage , the multimodal approach gained signicant relevance in the treatment of ec [ 3 , 4 ]  . importantly , the randomized controlled cross trial emphasized the advantage of a neoadjuvant radiochemotherapy ( rcth ) regimen with paclitaxel and carboplatin and concurrent radiotherapy with 41.4 gray ( gy ) over surgery alone [ 5 ]  . 
based on their ndings , the authors encouraged extrapolation of the cross treatment into daily practice [ 6 ]  . 780 strahlenther onkol ( 2020 ) 196 : 779786 as a consequence , the cross scheme has also been established at our tertiary academic referral center enriching our perioperative treatment concepts . 
five years after the implementation of this neoadjuvant protocol at the medical university of vienna , this retrospective study was performed to evaluate oncological results such as pathological response rates and survival data as well as the impact of rcth on perioperative outcomes . methods patients all patients , who underwent neoadjuvant radiochemotherapy and / or esophageal resection for esophageal cancer after neoadjuvant treatment according to the modied cross protocol at the department of surgery , medical university of vienna , between the years 2013 and 2018 , were included in this analysis . clinical data were obtained from an institutional prospective database . 
in order to optimize data accuracy and reduce the number of patients lost to follow - up , patients were contacted to evaluate the current status if information was missing . 
the ethic commission of the medical university of vienna approved the study ( ek2248 / 2017 ) and the study was conducted in accordance with the declaration of helsinki principals . 
tumor staging was performed according to the tumor , node , metastasis ( tnm ) classication of the 7th edition of the ajcc cancer staging manual [ 8 ]  . 
concerning ac location was classied following the siewert classication of the adenocarcinoma of the esophagogastric junction ( aeg ) [ 10 ]  . eligibility criteria all patients who underwent neoadjuvant rcth followed by esophageal resection for esophageal carcinoma ( ac as well as scc ) were included in this analysis . 
rcth was applied according to international guidelines on treatment of esophageal cancer [ 11 , 12 ]  . deep inspiration breathhold technique was used for planning - computed tomography and during radiotherapy whenever the patient tolerated it . three dimensional ( 3d ) treatment planning was based on the contouring of target volumes and organs at risk . imaging used was a computed tomography scan in treatment position . 
the following organs at risk were contoured : lungs , heart , spinal cord , kidneys , liver , stomach and peritoneal cavity ( representative for small and large bowel )  . 
thirty - four ( 94.4% ) patients had a 3d conformal treatment planning , 1 patient received a volumetric modulated arc therapy ( vmat ) and in 1 patient the treatment technique is unknown . 
a total dose of 46 gy , specied at the international commission on radiation units ( icru ) 50 / 62 reference point , was given in fractions of 2 gy , 5 days a week with a linear accelerator ( beam energy 10 mv )  . radiotherapy ( rt ) was combined with a radiosensitizing medication ( paclitaxel 50 mg / m2 body surface and carboplatin 2 mg ml 1 min1 area under the curve up to a total of 5 cycles at weekly intervals )  . strahlenther onkol ( 2020 ) 196 : 779786 fig . 
modied cross neoadjuvant chemoradiotherapy plus surgery versus surgery alone for esophageal or junctional cancer ( cross trial ) , sakk swiss group for clinical cancer research phase ii trial ( sakk 75 / 08 ) , xelox capecitabine and oxaliplatin , eox epirubicin , oxaliplatin and capecitabine surgery statistics all esophageal resections were performed at our tertiary center . 
according to tumor location patients underwent either abdominothoracic esophageal resection ( ivor lewis esophagectomy ) , including hybrid minimal invasive esophagectomy , thoracoabdominocervial resection ( mckeown esophagectomy ) or transhiatal extended gastrectomy [ 1315 ]  . 
morbidity was classied according to the clavien / dindo ( c / d ) classication [ 16 ]  . age is described as mean and standard deviation ( sd )  . other continuous variables are described as medians and quartiles due to nonnormal distributions . 
 ( % ) adenocarcinoma squamous cell carcinoma clinical tumor staging ct4a clinical nodal staging results demographics cross neoadjuvant radiochemotherapy ; asa american society of anesthesiologists values in parentheses are percentages unless indicated otherwise ; values are mean ( standard deviation ) avalues are median ( interquartile range ) fifty - two patients underwent neoadjuvant rcth . 
one patient was treated with 34.2 gy due to toxicity of chemotherapy , 1 patient had 41.4 gy , 1 patient had 50 gy , 1 patient had 46 gy with external beam therapy plus additional high dose rate ( hdr ) brachytherapy to the events of grade 3 events according to ctcae leukopenia thrombopenia infection other reason for reduced cth delay without toxicity all ( n = 36 ) 12 ( 33.5% ) 2 ( 5.6% ) 1 ( 2.8% ) 2 ( 5.6% ) ctcae common terminology criteria for adverse events values in parentheses are percentages residual tumor . 
the reduction of chemotherapy cycles was caused by leukopenia in 12 patients ( 33.3% ) , by thrombopenia in 2 patients ( 5.6% ) , in 1 patient ( 2.8% ) due to infection and in 2 patients ( 5.6% ) the reduction of cycles was caused by delay ( without treatment toxicity )  . 
there were no radiotherapyassociated side effects ( acute or chronic ) exceeding adverse events grade ii . perioperative details and morbidity patients without tumor progression proceeded to surgery within a median of 7 weeks ( range 227 weeks ) after completion of radiochemotherapy . 
this study shows that introduction of a modied study protocol into daily practice is safe and feasible . comparing our ndings with earlier studies , the presented results are in line with the current literature [ 5 , 17 ]  . dosage of rt differs throughout literature in neoadjuvant settings [ 18 , 19 ]  . 
this does not only result in difculties comparing studies precisely , it may also impact clinical pathologic tumor stage ypt0 ypt1 ypt2 ypt3 ypt4a pathologic nodal stage ypn0 ypn1 ypn2 ypn3 tumor grading well differentiated ( g1 ) moderately differentiated ( g2 ) poorly differentiated ( g3 ) surgical margin status clear microscopically involved ( r1 ) macroscopically involved ( r2 ) tumor regression grade ( mandard ) trg 1 trg 2 trg 3 trg 4 13 ( 36.1 ) 2 ( 5.6 ) 6 ( 16.7 ) 15 ( 41.7 ) 22 ( 61.1 ) 9 ( 25 ) 3 ( 8.4 ) 2 ( 5.6 ) 13 ( 36.1 ) 10 ( 27.8 ) 35 ( 97.2 ) 1 ( 2.8 ) 13 ( 36.1 ) 13 ( 36.1 ) 7 ( 19.4 ) 3 ( 8.3 ) values in parentheses are percentages ; modied cross , neoadjuvant radiochemotherapy trg mandard tumor regression grade results . 
the dosage used in this study ( 46 gy ) was comparable with the dose used in the neoscope phase ii trial ( 45 gy ) [ 18 ]  . 
recently , a study reported no impact of varying interval ( time to surgery < 8 weeks compared to > 8 weeks ) on oncological outcome or postoperative morbidity after rcth [ 21 ]  . subsequently , a meta - analysis did not show any benet of a prolonged interval ( mainly cutoff of 78 weeks ) between rcth and surgery [ 22 ]  . 
moreover , this systematic review concluded that a prolonged period might increase the risk for anastomotic complications . regarding the cr rate , the results in this study are comparable to earlier studies [ 5 , 17 ]  . 
the dutch - based sano study group published a sophisticated study protocol , which might prove surveillance as a possible alternative to esophagectomy in this patient group [ 23 ]  . beyond dosage other parameters of radiotherapy may impact oncological and perioperative outcome . 
radiotherapy led to a reduction of locoregional recurrences from 34% ( surgery ) to 14% ( radiotherapy + surgery ) , but still half of these recurrences ( 8% ) were found at the edge or outside the radiation volume . 
however , lowering these recurrences by increasing radiation volumes has to be put against the risk of worsening perioperative morbidity [ 24 ]  . radiotherapy technique itself might inuence the risk of local recurrence and long - term morbidity . 
found on a large cohort ( n = 676 ) better overall survival , better locoregional control , fewer noncancer - related and cardiac deaths for imrt [ 25 ]  . in our study treatment was mainly 3d conformal radiotherapy . 
compared morbidity rates in the heart and lungs in a proton group versus an x - ray group and found lower morbidity rates in the proton group , consistent with lower doses to heart and lungs in the proton group [ 26 ]  . 
proton treatment would offer reduced dose to organs at risk adjacent to the planning target volume , but unfortunately proton therapy was not available for esophageal treatment during study period . 
however in this study , the beam arrangement was optimized to spare dose to the heart and deep inspiration breathhold technique was used to reduce dose to the lungs . it is important to stress several limitations associated with a retrospective single center experience . 
nevertheless , the perioperative and surgical technique as well as the radiotherapy technique at the medical university of vienna did not change during the study period and reects a stable treatment algorithm . still , a subgroup analysis is not reasonable for this cohort . 
however , including patients in a consecutive manner limited a potential selection bias . however , the aim of the study was to evaluate the impact of rcth on surgery and its postoperative course . 
we were able to demonstrate that the extrapolation with a minor adaption of a new treatment protocol can be safely done in a tertiary setting . still , there are questions which need to be answered : rst , it is not known if rcth plays a permanent part in the neoadjuvant therapy of ac of the esophagus [ 27 ]  . 
second , dosage in rcth somewhat differs throughout the literature . furthermore , there are several other aspects ( e.g. , denition strahlenther onkol ( 2020 ) 196 : 779786 of gross tumor volume and planning target volume ) which inuence rt and its impact on oncological and perioperative outcome . 
it has been well acknowledged that the local recurrence may be further decreased by the delivery of a boost of 1016 gy to the tumor bed after 50 gy to the whole breast [ 6 , 28 ]  . 
theoretically , a dosimertric study has already demonstrated that wbi combined with sib could reduce the volume of the nontarget breast tissues outside the tumor bed receiving high - dose irradiation and shorten overall treatment time by 12 weeks [ 34 ]  . bantema - joppe et al . 
in a statement of the breast cancer expert panel of the german society of radiation oncology ( degro ) , it has been mentioned that the application of normofractionated sib seems to be in the therapeutic range , whereas longer observation is still mandatory [ 29 ]  . it was demonstrated by van der laan et al . 
that the application of inversely planned imrt - sib showed further dosimetric superiority compared to 3dcrt - sib , especially for specic subgroups of patients with overlap between heart and breast planning target volume and those with a relatively large boost ptv volume [ 35 ]  . 
although breast imrt - sib is an area of great interest , long - term prospective clinical data are lacking . since 2010 in our department , patients having previously undergone breast - conserving surgery were irradiated with inversely planned imrt - sib , as previously described [ 37 ]  . the aim of this present study was to evaluate the 5 - year clinical outcomes and to present toxicities related to radiotherapy and patient - reported cosmetic outcomes in a cohort of women with node - negative breast cancer treated with imrt and sib irradiation after breast - conserving surgery . between july 2011 and december 2014 , 467 consecutive node - negative breast cancer patients receiving adjuvant radiotherapy following bcs were enrolled in a single institutional phase 2 prospective trial at fudan university shanghai cancer center . 
all patients underwent adjuvant radiotherapy with sib delivered with imrt technology started within 6 weeks after completion of surgery and 4 weeks after the last cycle of chemotherapy . the clinical trial was registered on ( identier : nct01394575 )  . protocol eligibility criteria included the following : 1870 years old , ecog score < 2 , invasive cancer or ductal carcinoma in situ ( dcis ) , negative microscopic margins , no evidence of distant metastasis and negative nodal status determined by sentinel node biopsy or axillary dissection . axillary staging is not required for patients with dcis . 
excluded were patients with previous invasive or concomitant malignancies ( except nonmelanoma skin cancer , carcinoma in situ of the cervix , and invasive carcinoma of the colon , thyroid , cervix , or endometrium treated 5 years prior to study entry ) , patients with previous thoracic irradiation , patients contraindicated in radiation therapy and patients treated with neoadjuvant chemotherapy . 
all patients were staged as per the american joint committee on cancer ( 7th edition )  . for radiotherapy treatment regimens , the postoperative tumor bed was delineated based on the clips and seroma combined with other postoperative changes . 
the clinical target volume of tumor bed ( ctv - tb ) was dened by uniformly adding a margin of 10 mm around the tumor bed . the planning target volume ( ptv - tb ) was dened as ctvtb with an additional margin of 5 mthe breast clinical target volume ( ctv - breast ) included the apparent glandular breast tissue on ct scan . 
both ptv - breast and ptv - tb were limited anteriorly 5 mm under the skin surface . these patients were irradiated with 25 fractions of 1.8 gy to the whole breast and 2.4 gy to the tumor bed . 
the plans aimed to deliver 45 gy to 95% of ptv - breast and 60 gy to 95% of ptv - tb , while the volume of ptv receiving greater than 110% of the prescribed dose was limited . 
the dose constraints of organs at risk ( oar ) were listed as follows : the mean dose to heart ( cid : 2 ) 6 gy ( dmean ( cid : 2 ) 6 gy ) ; ipsilateral lung v5 ( cid : 2 ) 40% , v10 ( cid : 2 ) 30% , v20 ( cid : 2 ) 20% ; contralateral breast dmean ( cid : 2 ) 1 gy and contralateral lung dmean ( cid : 2 ) 1 gy [ 36 ]  . 766 strahlenther onkol ( 2020 ) 196 : 764770 table 1 patient and tumor characteristics the primary endpoint of the study was to record radiation toxicity and cosmetic effect . 
the secondary endpoint was the evaluation of clinical outcomes in terms of local recurrence and overall survival . during treatment and until 1 year after radiotherapy , toxicities related to radiotherapy were recorded according to common terminology criteria for adverse events ( ctcae ) version 4.0. 
the anthracycline - based regimen ec ( epirubicin and cyclophosphamide ) or fec ( 5 - uorouracil , epirubicin and cyclophosphamide ) and the non - anthracycline - based regimen tc ( doxdocetaxelcyclophosphamide ) were commonly used in the postoperative setting . 
survival curves , including the unadjusted 5 - year actuarial rates of locoregional control ( lrc ) , distant metastasis - free survival ( dmfs ) , and overall survival ( os ) were estimated with the kaplanmeier method . results patient characteristics between 2011 and 2014 , 467 patients with 406 invasive breast cancer ( 358 invasive ductal carcinoma , 48 other pathologic types ) and 61 dcis were treated . 
we could consider this radiological nding as a grade 1 pneumonitis strahlenther onkol ( 2020 ) 196 : 764770 table 2 locoregional recurrence patient number tumor grade tumor size ( cm ) tumor stage t2n0 subtype time to local recurrence luminal a 50 months t1n0 luminal b 56 months t1n0 luminal b 28 months t2n0 32 months her2 positive locoregional recurrence site regional nodes ( including ipsilateral axillary nodes , imn and supraclavicular nodes ) ipsilateral recurrence ( outside the boost ptv ) ipsilateral recurrence ( outside the boost ptv ) ipsilateral recurrence ( close to the boost ptv ) imn internal mammary nodes , ptv planning target volume according to ctcae v . 
among these patients , 335 women ( 86.6% ) declared good or excellent cosmetic outcome , 52 patients ( 13.4% ) classied their results as fair or poor ( fair in 48 patients and poor in 4 patients )  . clinical outcomes no patient with dcis had a local recurrence or distant metastasis . among 406 invasive breast cancer patients , only 3 patients developed isolated local recurrence . 
three patients developed isolated lung metastasis , including 1 patient with lung metastasis in conjunction with ipsilateral supraclavicular table 3 pattern of failures among invasive breast cancer patients ( n = 406 ) first event number of patients local recurrence regional recurrence distant metastasis breast cancer specic death death of all causes nodal metastasis . 
the pattern of failures is listed in table 3 . in total , 10 patients developed non - breast second malignancies during follow - up , including 5 thyroid cancers , 2 lung cancers , 1 glioma , 1 liver cancer , 1 endometrial cancer . 
the other cause of death is unknown ( n = 1 )  . contralateral breast cancer was noted in 2 patients . the survival curves of patients with invasive breast cancer ( n = 406 ) are shown in fig . 
compared to 3d - crt , imrt provides excellent coverage of the target volume with lower volumes of oar receiving high doses . in a consecutive series of patients from the netherlands , experience with breast imrt using hypofractionated sib is reported [ 5 ]  . 
furthermore , our local recurrence rate is similar to the reports of other recent studies in patients after breastconserving surgery treated with different technologies [ 1 , 20 , 25 ]  . to date , the results of radiotherapy toxicity of patients treated with breast imrt - sib are promising [ 5 , 9 ]  . 
a multivariable prediction model was developed using age , v55 ctv breast and dmax for predicting the incidence of grade 2 brosis after breast cancer radiotherapy using a 3d - crt - sib technique [ 16 ]  . in elderly patients , the presence of comorbidities and the breast volume > 700 cc has been shown to be related to grade 2 acute skin toxicity [ 15 ]  . concerning cosmetic results , the patient - rated good / excellent cosmetic results were 86.5% at the 12 month follow - up in our series . 
in the publication of bantema - joppe et al . , the physician - rated fair to poor cosmetic outcome was 39.7% at the 3 year followup [ 3 ]  . 
in a study conducted by kindts et al . , breast cancer - specic quality of life ( qol ) did not differ between different boost techniques over time , and esthetic outcome was unfavorable in 28% of patients at the 2 - year follow - up [ 20 ]  . radiation - induced pulmonary toxicity of patients treated with adjuvant radiotherapy for breast cancer varies widely , ranging between 4.5 and 63% [ 17 , 18 , 22 ]  . 
in this study , a diffuse reticular accentuation of the interstitium was recorded in about 25% of the patients according to x - ray exam [ 9 ]  . although no coronary events have been recorded in our study , it is well acknowledged that reducing mean heart dose is associated with lower radiation - induced heart toxicities [ 8 , 27 , 33 ]  . 
the use of deep inspiration breath hold ( dibh ) as the best heart - sparing technique is highly encouraged to reduce all parameters associated with heart toxicity induced by radiotherapy [ 11 ]  . 
however , specic breathing techniques such as dibh or gating were not routinely used for these patients . the median age at diagnosis of breast cancer in our cohort was 46 years , while it was 4850 years in china and 64 years in the usa , with 57% of women diagnosed before the age of 50 years [ 13 ]  . 
according to another study integrating hospital - based and population - based databases , the median age of breast cancer at diagnosis was 48 in china , which indicated racial differences in genetics and lifestyle [ 30 ]  . in our study , contralateral breast cancer was noted in 2 patients , which was consistent with our previous publication [ 38 ] and the paper of bantema - joppe et al . 
our results provide further new evidence supporting the use of the imrt - sib technique among breast cancer patients after breast - conservative surgery ( bcs )  . major limitations of our study were as follows : first , our trial was restricted to women who had node - negative , invasive breast cancer or ductal carcinoma in situ ( dcis ) patients with clear margins of excision after lumpectomy . it is not clear whether our results can be extrapolated to women with node - positive disease . 
second , cosmetic outcome was only recorded by the patients themselves , without assessment by the physicians or photographic record . finally , long - term toxicity such as skin brosis after radiotherapy which might be related to hypofractionated tumor bed area should be noted . 
da beim tnbc keine bekannten hormonoder wachstumsfaktorrezeptoren vermehrt exprimiert werden , die fr eine gezielte therapie genutzt werden knnten , ist eine konventionelle chemotherapie bisher die einzige zugelassene systemische therapie [ 1 , 7 ]  . 
bei frhen , nichtmetastasierten tnbc wird aktuell eine neoadjuvante anthrazyklin - / taxanbasierte chemotherapie empfohlen [ 7 ]  . das hohe rezidivund metastasierungsrisiko des tnbc im vergleich zu anderen mammakarzinomsubtypen und das prognostisch ungnstige metastasierungsmuster mit vorwiegend viszeralen und zentralnervsen metastasen verdeutlicht die notwendigkeit weiterer , spezischer therapiemglichkeiten [ 1 , 5 ]  . 
ziel der vorliegenden studie keynote522 war es , herauszunden , ob durch den neoadjuvanten einsatz von pembrolizumab zustzlich zu einer etablierten neoadjuvanten chemotherapie signikant mehr pathologische komplettremissionen ( pcr ) und ein lngeres ereignisfreies berleben ( efs ) erreicht werden knnen . 
die pcr gilt als surrogatmarker fr eine lngere berlebenszeit [ 2 ]  . originalpublikation schmid p , cortes j , pusztai l et al ( 2020 ) pembrolizumab for early triple - negative breast cancer . 
21 , 24105 kiel , deutschland patientenkollektiv und methoden um den mglichen gewinn eines zustzlichen einsatzes von pembrolizumab zu untersuchen , wurden in dieser randomisierten , doppelblinden phase - 3 - studie patienten mit einem erstdiagnostizierten , unbehandelten tnbc im stadium ii oder iii in eine neoadjuvante und eine adjuvante therapiegruppe randomisiert ( ratio pembrolizumabzu plazebogruppe : 2 : 1 )  . eingeschlossen wurden patienten mit nichtmetastasiertem tnbc ( ct1c und n12 oder ct24 und n02 ) ohne aktive autoimmunerkrankungen , immundefekte oder immunsuppressive therapien innerhalb der letzten 2 wochen . eine gruppe ( n = 784 ) erhielt 4 zyklen pembrolizumab ( jeweils 200 mg ) alle 3 wochen plus paclitaxel und carboplatin , die andere ( n = 390 ) 4 zyklen plazebo alle 3 wochen plus paclitaxel und carboplatbeide gruppen erhielten 4 weitere zyklen pembrolizumab bzw . 
als sekundre endpunkte wurden pcr , efs und das gesamtberleben ( os ) unter den patienten mit pd - l1 - positiven tnbc bestimmt . ergebnisse die beurteilung der pcr - rate erfolgte an den 602 ersten randomisierten patienten . 
gem des vorher berechneten signikanzwertes von p = 0 , 003 fr die geplante interimsanalyse war die pcr damit signikant hher zugunsten der pembrolizu842 strahlenther onkol ( 2020 ) 196 : 841843 mabchemotherapiegruppe . 
ein vergleichbarer unterschied wurde sowohl bei betrachtung der sekundren endpunkte in der gruppe der pd - l1 - positiven tnbc als auch bei den tumoren mit niedrigem pd - l1 - status beobachtet . die progressionsraten nach 18 monaten nach kaplan meier ergaben fr 91 , 3 % der patienten der pembrolizumabchemotherapiegruppe und fr 85 , 3 % der plazebogruppe ein efs ohne erneutes lokales oder disseminiertes wiederauftreten des primrtumors und ohne sekundrtumor ( hazard ratio : 0 , 63 ; 95 % - ki : 0 , 430 , 93 )  . 
dort stagnierte das efs und bildete ein plateau . behandlungsassoziierte nebenwirkungen vom grad 3 traten in 76 , 8 % der patienten der pembrolizumabchemotherapiegruppe und 72 , 2 % der plazebogruppe auf und fhrten zu 3 bzw . 
zu den nach pembrolizumab vermehrt auftretenden nebenwirkungen zhlten exantheme , infusionsreaktionen und immunittsbedingte adrenale insufzienzen . der keynote - 086 - studie trat in der kohorte vorher schon einmal behandelter patienten ebenfalls kein signikanter unterschied im pfs oder os in bezug auf den pd - l1status auf [ 4 ]  . 
allerdings zeigte sich ein besseres therapieansprechen , wenn pembrolizumab in der erstbehandlung von pd - l1 - positiven tumoren eingesetzt wurde [ 13 ]  . der behandlungsvorteil durch pembrolizumab , auch bei niedriger pd - l1 - expression , zeigt , dass die fehlende expression von biomarkern kein ausschlusskriterium fr eine therapie oder studienteilnahme sein muss [ 6 ]  . 
sowohl die keynote - 522als auch die der keynote - 086 - studiengruppe planen weitere analysen der biomarker in ihrem patientenkollektiv , was vor diesem hintergrund notwendig und sinnvoll erscheint [ 3 , 12 , 13 ]  . 
weitere befunde erhoben werden , die dazu beitragen knnten , evtl . immunvermittelte , irreversible nebenwirkungen zu vermeiden . schlussfolgerung der autoren pembrolizumab fhrt zu einer signikanten zunahme der pcr bei patienten mit frhem tnbc . 
die erhhte pcr - rate tritt in allen subgruppen und ebenfalls in der patientengruppe mit einer niedrigen pd - l1 - expression auf . fazit kommentar aufgrund der guten ergebnisse der keynote - 522 - studie bezglich pcr und os scheint pembrolizumab eine sinnvolle ergnzung zur chemotherapie als momentan einzig zugelassene neoadjuvante behandlung zu sein [ 4 , 9 ]  . 
auch wegen der charakterisierung des tnbc als immunogenen tumor , mit hug erhhten cd8 + - t - zell - werten und einer hug erhhten pd - l1 - expression , scheinen immuncheckpointinhibitoren der richtige ansatzpunkt fr eine mehr zielgerichtete therapie zu sein [ 4 ]  . 
positiv ist ebenfalls die kongruenz der ergebnisse mit der phase - 2 - vorstudie ispy2 , in der bei neoadjuvanter gabe von pembrolizumab bei frhen tnbc sogar eine verbesserung der pcr um 40 prozentpunkte erreicht werden konnte [ 3 , 11 ]  . auch bei der behandlung von metastasierten tnbc mit pembrolizumab als monotherapie konnte in der phase - 1studie keynote - 12 ein gesamtansprechen von 18 , 5 % erreicht werden [ 4 , 8 , 9 ] sowie in der phase - 2 - studie keynote - 086 ebenfalls hnliche ergebnisse bezglich des progressionsfreien berlebens ( pfs ) und des os . 
obwohl der gewinn bezglich des langzeitberlebens noch kritisch bewertet werden muss [ 3 ] , sind der signikante unterschied im efs und das dabei erreichte plateau starke indizien fr eine positive einschtzung hinsichtlich os und heilung . 
dunst geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschrifstrahlenther onkol ( 2020 ) 196 : 841843 ten erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
schneeweiss a , denkert c , fasching pa et al ( 2019 ) diagnosis and therapy of triple - negative breast cancer ( tnbc ) recommendations for daily routine practice . 
cortazar p , zhang l , untch m et al ( 2014 ) pathological complete response and long - term clinical benet in breast cancer : the ctneobc pooled analysis . 
nanda r , liu mc , yau c et al ( 2020 ) effect of pembrolizumab plus neoadjuvant chemotherapy on pathologic complete response in women with early - stage breast cancer . 
the presence of predictive factors and cut - off points were investigated to achieve acceptable lung doses in esophageal cancer ( ec ) treatment . methods virtual rt volumes of supracarinal ec were delineated . 
roc analysis showed that lung / ptv ( planning target volume ) volume ratio ( auc [ area under curve ] : 0.91 , 95% ci : 0.830.99 , p = 0.000 ) and bilateral lung volume ( auc : 0.81 , 95% ci : 0.700.92 , p = 0.000 ) have diagnostic power to predict the suitability of rt plans according to quantec ( quantitative analyses of normal tissue effects in the clinic ) for lung dose constraints . 
the patients with lung / ptv ratio and lung volume above these cut - off points may be candidates for treatment with tomotherapy . keywords esophageal cancer neoplasms normal tissue sparing dosimetric effects helical tomotherapy dose - volume parameters introduction esophageal cancer ( ec ) is a rare type of cancer and it has critical importance among the cancer types due to the high mortality rates . 
in this study , the superiority of 50 gy radiation therapy ( rt ) and four cycles of 5 - uorouracil plus cisplatin over 64 gy rt have shown 5 - year survival rates of 26% versus 0% [ 3 ]  . 
in the int 0123 ( radiation therapy oncology group 94 - 05 ) trial , although the same chemotherapeutic agents were used in both study arms , the superiority of highdose rt over 50.4 gy rt could not be demonstrated [ 4 ]  . the dose escalation studies are still ongoing to investigate whether dose escalation increases treatment effectiveness or not , but currently , 50.4 gy is accepted as the standard dose [ 46 ]  . the esophagus has a central location within the thorax . irradiation of the esophagus , which is surrounded by lungs and heart , always brings the risk of cardiopulmonary toxicity [ 7 ]  . 
during the past decades , in order to decrease toxicity 806 strahlenther onkol ( 2020 ) 196 : 805812 and increase treatment response , 2d - rt was rstly replaced by 3d - conformal rt ( 3dcrt ) , and 3dcrt was replaced by step and shoot intensity - modulated rt ( imrt ) [ 2 ]  . the modulated dose distribution decreased the dose exposure around the target tissue . 
it also enables imageguided rt with integrated computed tomography ( ct ) [ 11 ]  . regarding target conformity , dose homogeneity , and lung v20 values , helical rt plans in ec are superior to 3dcrt [ 12 ]  . 
even though the gross tumor volume in ec is only a few centimeters long , the area to be irradiated is longitudinally large because the craniocaudal margin given for ctv ( clinical target volume ) is 35 cm [ 13 ]  . 
examined the irradiation of thoracic ec by a volumetric arc treatment ( vmat ) technique as well as the effect of free - breathing or deep breath - hold techniques on the lung and heart doses . 
for this purpose , virtual rt volumes were delineated for supracarinal ec irradiation . the relationship between the ptv and the lung volume and their effect on the lung doses obtained from the plans were evaluated . 
the presence of predictive factors and cutoff points were investigated to obtain a good starting point in the rt planning strategy with ht in order to achieve acceptable lung doses and save planning time . 
thus , we tried to determine which cases can be more suitable for methods patient selection sixty - ve patients with the following features were selected for the study : scans with non - metastatic ec , no inltrative lesion in the lungs , expanding lesion in the supracarinal esophagus , or large lymph node ( > 1 cm ) in the mediastinuall patients were immobilized in the supine position with both arms up on the t - board . 
according to our clinical protocol , slow helical ct was performed using a maximum gantry rotation speed of 1 s / rotation and a reduced pitch value of 0.45. delineation of virtual volumes for esophageal irradiation the delineation was performed independently of the primary disease characteristics . 
in all cases , ctvesophagus , ptv - esophagus , and organs at risk ( oar ) were delineated by the radiation oncologist in the focal contouring system v.4.62 ( elekta , stockholm , sweden )  . 
was used for ctv delineation [ 13 ]  . the steps during contouring were as follows : ( cid : 2 ) oar ( lungs , heart , esophagus , spinal cord ) were delineated . ( cid : 2 ) the supracarinal esophagus was delineated as there was a hypothetical esophageal tumor . ( cid : 2 ) a 1 cm radial margin from the outer esophageal wall was given to encompass the peri - esophageal lymph nodes . then the vertebral bodies were entirely excluded from the ctv . 
this ctv was expanded , including bilateral second and fourth stations , third station , and seventh station , according to the iaslc ( international association for the study of lung cancer ) staging map [ 15 ]  . ( cid : 2 ) since the lung doses were evaluated , no supraclavicular region was added to these virtual volumes . 
moreover , the extra longitudinal margin was not given since the whole supracarinal esophagus was included in the ctv . ( cid : 2 ) an 8 mm ptv margin was given to the ctv for ht treatment with daily onboard mv - ct ( mega voltage - computed tomography ) imaging . helical tomotherapy planning after all of the volumes had been dened , the images and structures were transferred to the tomotherapy planning system ( tps ; accuray inc . , madison , usa )  . 
during planning we used our clinical protocol based on quantec ( quantitative analyses of normal tissue effects in the clinic ) dose limits ( spinal cord ( cid : 2 ) 45 gy , mean lung dose < 20 gy , lung v20 < 35% , lung v5 < 65% , mean heart dose < 30 gy , heart v30 < 46% , heart v25 < 10% ) [ 16 ]  . 
a patient with a small - volume lung , b patient with a large - volume lung histogram ( dvh ) constraints and penalties were adjusted during the optimization to obtain adequate ptv coverage and minimize lung , spinal cord , heart doses . 
final dose calculations were set to be completed after 200 iterations for each plan . v5 , v20 , and mean lung dose of the bilateral lung that were obtained from the rt plans were categorized according to whether they were within quantec dose limits or not [ 16 ]  . 
the plans in which all of the parameters ( lung v5 , v20 , mean lung dose ) were in the dose limits of quantec were considered as an appropriate plan for the patient . 
the data were then processed in spss in order to nd out the variables which would be useful for predicting whether or not the plans would be able to meet quantec dose constraints . statistical analysis statistical analyses were performed with spss 18.0 ( statistical package for the social sciences ; spss inc . , chicago , usa )  . 
a p - value of less than 0.05 was considered statistically signicant . results a total of 65 patient datasets ( 27 , 41.5% , female ; 38 , 58.5% , male ) were used in the study . 
the sensitivity , specicity , and positive and negative predictive data of the cut - off points are given in table 2 . the mannwhitney u test results are shown in tables 3 and 4 . 
because of the low frequency of ec in western countries , the number of patients in the majority of studies on real patient data is decient [ 14 , 1719 ]  . 
in this study , the lung v10 , v20 , v30 , and v40 values as well as mld obtained from the patients with the deep breath - hold method , which provides a larger lung volume , were found to be statistically lower than in the free - breathing patients . lung v5 values were not signicantly reduced [ 14 ]  . 
in our study , a statistically signicant decrease in mld and lung v5 , v15 , and v20 values were obtained in the patients with lung volume 3500 cc and lung / ptv 7 . in our study , the factors that were taken into consideration in evaluating whether the rt plans were within quantec dose limits or not were lung v5 and v20 values and mld . 
we excluded lung v10 values , because the lung v10 [ 17 , 20 ] values were higher in helical and full - arc irradiation techniques than in other restricted - arc techniques . 
it was determined that there was a signicant decrease in the lung doses with the blocking method of ht for ec compared to non - blocked plans [ 21 ]  . 
in a study of 15 cervical ec patients by ito et al . , rt volumes , including upper mediastinal lymphatic stations and the seventh station , were delineated similarly to our study . 
as a result , a signicant decrease in lung mean v5 , v10 , and v20 values was obtained in the blocked plans without compromising ptv conformity , dose homogeneity , or heart doses [ 22 ]  . 
according to our results , a 10% reduction for v5 and an 8% reduction for v10 could be obtained for the patients with the lung / ptv ratio 7 and the lung volume 3500 cc ( p = 0.002 ) without using blocking methods . 
a statistically signicant increase in dmean , v5 , v10 , v40 , and v45 values of the heart was found between the groups given a 2 cm margin versus a 4 cm margin ( p < 0.05 ) [ 19 ]  . 
tomotherapy is reported to be the best technique to reduce heart dose in studies comparing 3dcrt , imrt , imrt&arc , and rapidarc techniques in the literature [ 12 , 17 ]  . 
also , in our study , it has been shown that heart doses ( dmean , v5 , v20 , v30 , v45 ) can be signicantly reduced in supracarinal ec patients with appropriate lung / ptv and lung volume values , although only the basis of the heart usually enters into the rt eld . 
according to the results of all these studies , it should be considered that ht can be the most effective method in a patient whose heart should be protected . in our study , there was no correlation between increased lung / ptv ratio , lung volume , and spinal cord max doses . in the literature , previous studies have shown that imrt , vmat , and ht do not affect spinal cord max dose [ 14 , 17 , 19 , 23 , 24 ]  . 
however , it should be kept in mind that if the lung doses are decreased by using blocking methods in ht , this may result in a slight increase in spinal cord max dose [ 21 , 22 ]  . the treatment period is shorter in vmat techniques , whereas ht takes a few minutes longer [ 14 ]  . 
in our study , the mean treatment duration was approximately 5 mthe duration of treatment was similar between the groups according to the lung / ptv ratio . one of the strengths of our study is the delineation of standard virtual volumes in the selected patient scans . moreover , ht plans were made with standard optimization criteria , and this situation served to get homogenous data . our study is the rst study that reveals some cut - off points for the use of tomotherapy in ec treatments . 
as a result , the rt device should be selected by considering all the advantages and disadvantages of existing rt techniques . conclusion the lung / ptv ratio 7 and bilateral lung volume 3500 cc cut - off points are predictive of whether tomotherapy plans may meet quantec lung dose limits in patients with supracarinal esophageal cancer . 
for the patients with low lung volumes and low lung / ptv ratios , tomotherapy plans with blocking techniques or vmat with deep inspiration breath - hold can be tried . compliance with ethical guidelines conict of interest m . 
frhere klinische studien hatten gezeigt , dass die schonung der neuroregenerativen zone des hippocampus unter verwendung einer intensittsmodulierten ganzhirnbestrahlung ( ghb ) zu einer signikant geringeren einschrnkung der neurokognition fhrt [ 2 , 3 ]  . 
zudem konnte in einer phase - 3 - studie ein verbesserter erhalt der neurokognition nach ghb durch memantin erreicht werden [ 4 ]  . patienten und methode die phase - 3 - studie von brown et al . 
schloss erwachsene patienten mit neu diagnostizierten hirnmetastasen unterschiedlicher solider primrtumoren ein und verglich eine hippocampusschonende ghb ( hs - ghb ) plus memantin mit einer konventionellen ghb plus memantden primren endpunkt stellte die zeit bis zu einer messbaren einschrnkung der neurokognition mittels einer denierten testbatterie dar . 
zu den sekundren endpunkten gehrten das gesamtberleben ( os ) , das intrakraniale progressionsfreie berleben ( pfs ) , die toxizitt und die von den patienten angegebene symptomatik . ergebnisse zwischen juli 2015 und mrz 2018 wurden 518 patienten randomisiert . 
das risiko einer kognitiven einschrnkung war nach hs - ghb plus memantin signikant niedriger als nach ghb plus memantin ( hazard ratio 0 , 74 ; 95 % - ki : 0 , 580 , 95 ; p = 0 , 02 )  . 
dieser unterschied war auf eine geringere verschlechterung der exekutivfunktion nach 4 monaten ( 23 , 3 % gegenber 40 , 4 % ; p = 0 , 01 ) und des lernens und gedchtnisses nach 6 monaten ( 11 , 5 % gegenber 24 , 7 % [ p = 0 , 049 ] und 16 , 4 % gegenber 33 , 3 % [ p = 0 , 02 ] ) zurckzufhren . 
verglichen mit patienten , die eine ghb plus memantin erhielten , berichteten patienten mit hs - ghb plus memantin nach 6 monaten ber weniger fatigue ( p = 0 , 04 ) , gestrtes erinnerungsvermgen ( p = 0 , 01 ) , schwierigkeiten beim sprechen ( p = 0 , 049 ) sowie ber eine geringere beeintrchtigung durch neurologischen symptome bei tglichen aktivitten ( p = 0 , 008 ) sowie weniger kognitive symptome ( p = 0 , 01 )  . 
die behandlungsgruppen unterschieden sich nicht signikant im gesamtberleben ( os ) , intrakranialem progressionsfreien berleben ( pfs ) oder der toxizitt . schlussfolgerung der autoren die hs - ghb plus memantin sollte fr die behandlung von patienten in gutem allgemeinzustand , die keine metastasen in der hippocampusregion haben , als standard eingesetzt werden . 
eine hs - ghb plus memantin erhielt die kognitive funktion zwar besser und die patienten berichteten ber weniger symptome , doch unterscheiden sich das intrakraniale pfs und das os bisher nicht . kommentar originalpublikation brown pd , gondi v , pugh s et al . 
sie ist ein gelungenes beispiel fr die umsetzung anfnglich biologisch basierter hypothesen durch schrittweise frhe klinische untersuchungen bis hin zu einer komplexen randomisierten studie , die schlielich ein positives ergebnis lieferte [ 4 , 5 ]  . 
dennoch mchten wir bei all dieser euphorie einige kritische punkte hervorheben , strahlenther onkol ( 2020 ) 196 : 844846 die im zusammenhang mit den studienergebnissen geklrt werden mssen , bevor wir die hs - ghb in kombination mit memantin als neuen behandlungsstandard fr patienten mit neu diagnostizierten hirnmetastasen einfhren knnen : 1 . 
in anbetracht dieser hohen dosen sind wir besorgt , dass bei langfristigen nachuntersuchungen mikrovaskulre vernderungen und eine ausdnnung der kortikalis festgestellt werden knnten , die mit einer langfristigen neurokognitiven beeintrchtigung einhergehen [ 6 ]  . die im anhang ( tabelle a1 ) der arbeit von brown et al . gezeigte dosis - volumen - analyse des zielvolumens und der risikoorgane mit einer nicht spezizierten akzeptablen variation von 26 , 3 % bzw . 
krzlich haben wir eine automatisierte methode zur behandlungsplanung verffentlicht , welche das ziel verfolgt , die gesamtdosis fr das gehirn im vergleich zur rtog 09337 signikant zu reduzieren [ 7 ]  . 
2 studien zur prophylaktischen ganzhirnbestrahlung knnen etwas licht auf diesen aspekt richten : die nvalt11 - studie untersuchte die pci ohne hippocampale schonung bei nsclc - patienten und zeigte einen hheren prozentsatz niedriggradiger neurokognitiver beeintrchtigungen im vergleich zum beobachtungsgruppe [ 9 ]  . 
die multizentrische , randomisierte phase - 3 - studie ( nct01780675 ) widerspricht hingegen einem positiven effekt einer hippocampusschonenden pci gegenber einer pci mit gegenfeldern bei sclc - patienten [ 10 ]  . 
es konnte kein unterschied in der anzahl der patienten , die eine einschrnkung der hippocampusspezischen kognition zeigten , beobachtet werden . fazit unter bercksichtigung aller dieser vorbehalte mchten wir dazu ermutigen , zunchst die ergebnisse langfristiger neurokognitiver und bildgebender untersuchungen abzuwarten , bevor die hs - ghb in kombination mit memantin als standardtherapie fr patienten mit hirnmetastasen in voller breite eingesetzt wird . michael mayinger und nicolaus andratschke , zrich interessenkonikt m . 
brown pd , gondi v , pugh s et al ( 2020 ) hippocampal avoidance during whole - brain radiotherapy plus memantine for patients with brain metastases : phase iii trial nrg oncology cc001 . 
gondi v , hermann bp , mehta mp , tom wa ( 2012 ) hippocampal dosimetry predicts neurocognitive function impairment after fractionated stereotactic radiotherapy for benign or low - grade adult brain tumors . 
brown pd , pugh s , laack nn et al ( 2013 ) memantine for the prevention of cognitive dysfunction in patients receiving whole - brain 846 strahlenther onkol ( 2020 ) 196 : 844846 radiotherapy : a randomized , double - blind , placebo - controlled trial . neuro oncol 15 : 14291437 5 . 
gondi v , pugh sl , tome wa et al ( 2014 ) preservation of memory with conformal avoidance of the hippocampal neural stem - cell compartment during whole - brain radiotherapy for brain metastases ( rtog 0933 ) : a phase ii multi - institutional trial . 
krayenbuehl j , di martino m , guckenberger m , andratschke n ( 2017 ) improved plan quality with automated radiotherapy planning for whole brain with hippocampus sparing : a comparison to the rtog 0933 trial . 
mayinger m , kraft j , lohaus n et al ( 2020 ) leukoencephalopathy after prophylactic whole - brain irradiation with or without hippocampal sparing : a longitudinal magnetic resonance imaging analysis . 
sauer1 breast cancer expert panel of the german society of radiation oncology ( degro ) received : 20 february 2020 / accepted : 19 march 2020 / published online : 29 april 2020 the author ( s ) 2020 abstract purpose this consensus statement from the breast cancer working group of the german society for radiation oncology ( degro ) aims to dene practical guidelines for accelerated partial - breast irradiation ( apbi )  . methods recent recommendations for relevant aspects of apbi were summarized and a panel of experts reviewed all the relevant literature . 
panel members of the degro experts participated in a series of conferences , supplemented their clinical experience , performed a literature review , and formulated recommendations for implementing apbi in clinical routine , focusing on patient selection , target denition , and treatment technique . results appropriate patient selection , target denition for different apbi techniques , and basic rules for appropriate apbi techniques for clinical routine outside of clinical trials are described . 
detailed recommendations for apbi in daily practice , including dose constraints , are given . conclusion guidelines are mandatory to assure optimal results of apbi using different techniques . keywords breast cancer partial breast irradiation guideline apbi early breast cancer introduction to date , the gold standard for local treatment of patients aged 50 years or more with early breast cancer ( pt12 , pn0 ) and low - risk factors is breast - conserving surgery followed by postoperative whole - breast irradiation ( wbi ) , typ ( cid : 2 ) v . 
marien - krankenhaus siegen , siegen , germany 7 vivantes hospital neukoelln , berlin , germany 8 university hospital , jena , germany st . - vincentius - hospital karlsruhe , karlsruhe , germany 10 st . 
pbi is a treatment approach able not only to shorten the course of radiation therapy ( rt ) , but also to reduce the radiation exposure to the lung , the heart , the breasts , and the skin signicantly , depending on the treatment technique [ 911 ]  . over the past 20 years , different modalities of pbi have been tested , mostly successfully , in a number of phase 2 and 3 clinical trials . 
the studied techniques are external beam radiation ( photons , protons ) , singleand multicatheter brachytherapy , electronic brachytherapy , seed brachytherapy , non - invasive brachytherapy , and intraoperative radiation techniques ( iort ) either with electrons or with 50 - kv photons . 
today , results from over 15 , 000 patients recruited within phase 3 trials testing partial - breast irradiation are available [ 1 , 2 , 5 , 6 , 1219 ] and as a consequence , selected pbi techniques have been introduced into daily clinical routine . 
however , only small trials deal with pbi techniques using protons , brachytherapy ( bt ) using seeds , non - invasive bt , or numerous single - catheter devices . 
thus , for the purpose of this guideline , we only analyzed techniques tested in randomized phase 3 trials . 750 strahlenther onkol ( 2020 ) 196 : 749763 hier steht eine anzeige . methods the authors evaluated the relevant literature , identied established and controversial topics via working conferences , circular emails , and meetings , and supplemented this information with their clinical experience to formulate the current guidelines . 
currently available phase 3 trials are listed in table 1 . results external beam radiation therapy the use of external beam radiation therapy ( ebrt ) for pbi appears to be very attractive , because this technique is broadly available worldwide . 
in two small randomized trials from barcelona and florence [ 5 , 16 ] with 105 and 520 patients , respectively , patients were either treated with using intensity - modulated ebrt for pbi or using wbi . in general , similar efcacy ( local recurrence rate , diseasefree survival , and overall survival ) , toxicity , and cosmetic outcome were reported . 
patients were randomly assigned to receive 40 gy in 15 fractions of whole - breast radiotherapy ( control ) , 36 gy in 15 fractions of whole - breast radiotherapy with a simultaneous integrated boost to 40 gy to the tumor bed ( reduceddose group ) , or 40 gy to the partial breast only ( partialbreast group ) also in 15 daily treatment fractions . 
for localization of the tumor bed , surgical clips were preferably used , but if this was not possible , ultrasound , mri , or ct was used [ 20 ]  . 
field - in - eld intensity - modulated radiotherapy was delivered using standard tangential beams that were simply reduced in length for the partial - breast group . the protocol specied forward - planned eld - in - eld imrt delivered by standard medial and lateral tangential beams reduced in length but not in width . 
after a median follow - up 72.2 months , the cumulative 5 - year local relapse incidence was 1.1% in the control group , 0.2% in the reduced - dose group , and 0.5% in the partial752 strahlenther onkol ( 2020 ) 196 : 749763 breast group ; hence , a non - inferiority of pbi using 2.66 gy in 15 fractions in 3 weeks was conrmed . 
patient and clinical assessments recorded similar adverse effects after reduced - dose or partial - breast radiotherapy , including two patient domains achieving statistically signicantly lower adverse effects ( change in breast appearance [ p = 0.007 for partial - breast ] and breast harder or rmer [ p = 0.002 for reduced - dose and p < 0.0001 for partial - breast ] ) compared with whole - breast radiotherapy . 
because the same regimen is used , differences in treatment outcome can be attributed to differences in treatment volume [ 2 ]  . in the rapid trial [ 13 , 18 , 21 ] with altogether 2135 patients and a median follow - up of 8.6 years , patients aged > 40 years with invasive or in situ breast cancer ( cid : 2 ) 3 cm were randomly assigned after breast - conserving surgery to 3dcrt apbi or wbi . 
wbi was delivered daily to 42.5 gy in 16 fractions or 50 gy in 25 fractions using tangential elds . additional boost irradiation of 10 gy in four to ve fractions after wbi was based on criteria such as young age or close margins . 
the clinical target volume was the tumor bed on computed tomography , including the surgical clips plus a 1 - cm margin inside breast tissue . the planning target volume was the clinical target volume plus a 1 - cm margthe dose - evaluation volume was the subvolume of the planning target volume inside breast tissue . 
in this trial , the intent - to - treat and as - treated analyses could not refute the hypothesis that pbi is inferior and cannot declare that wbi and pbi are equivalent in controlling local in - breast tumor recurrence . 
in the rapid as well as in the nsbap - b - 39 / rtog 0413 trial , despite similar ptv denitions , treatment delivery was more conformal by the use of several non - coplanar elds , thus encompassing less tissue . 
unfortunately , none of the authors have so far provided absolute dimensions of treated volumes for the study patients . brachytherapy the use of multicatheter interstitial brachytherapy for apbi has been tested in two phase 3 trials so far . strahlenther onkol ( 2020 ) 196 : 749763 polgar et al . 
however , the statistical power of the trial regarding non - inferiority is limited due to the number of randomized patients . in the group europen de curiethrapie / european society for radiotherapy and oncology ( gec - estro ) multicentric phase 3 trial [ 1 , 3 , 4 ] , a total of 1184 patients were randomized to wbi or apbi using multicatheter brachytherapy . 
patients were considered eligible for the trial if they were aged 40 years or older ; had ptis or pt12a ( lesions of ( cid : 2 ) 3 cm diameter ) , pn0 / pn1mic , and m0 breast cancer ( stage 0 , i , and iia ) ; had undergone local excision of the breast tumor with microscopically clear resection margins of at least 2 mm in any direction ( in cases of invasive lobular carcinoma or dcis , at least 5 mm ) ; and had no lymph or blood vessel invasion ( l0 , v0 )  . 
the size of the safety margin ( calculated as the sum of the width of the clear pathological surgical margin plus the radiation safety margin ) had to be at least 20 mm , and this margin was dened individually for every patient . 
a total dose of 32 gy in eight fractions ( 8 4.0 gy ) or 30.3 gy in seven fractions ( 7 4.3 gy ) , with fractionation twice a day , was used for hdr brachytherapy . 
addressing non - inferiority , the analysis of this trials ndings was not primarily based on the intention - to - treat principle , because this approach sometimes introduces bias towards no difference , which is anticonservative in this setting , i.e. , would exaggerate estimates of equivalence . 
finally , detailed analysis of quality of life questionnaires in this trial during follow - up showed that global health status was stable in both groups , but a moderate , statistically signicant difference between the groups in the breast symptoms scale was found . 
breast symptom scores were signicantly higher , i.e. , worse , after whole - breast irradiation than after apbi [ 4 ]  . for single - catheter devices , the evidence is currently limited . 
as described above , the rst results of this trial were presented at the san antonio breast cancer symposium 2018 ; however , at the time of writing the presented guideline , corresponding subgroup analyses were not available . 
for other brachytherapy apbi techniques , no phase 3 data are available . intraoperative radiotherapy with electrons in the eliot study [ 15 ] , 1305 patients between 48 and 75 years of age and with tumors smaller than 2.5 cm were randomized to receive either single - dose intraoperative radiotherapy with electrons ( ioert ) with 21 gy ( 90% isodose ) as pbi ( experimental arm ) or adjuvant wbi with 50 gy in 25 fractions followed by an external electron boost of 10 gy in 5 fractions ( standard arm )  . 
in particular , the milanese group investigated the outcome in 1822 out - trial patients treated solely by ioert for low - risk breast cancer patients who were classied as suitable or good candidates according to the estro / astro guideline . 
patients were eligible if they were 45 years old , had a tumor size ( cid : 2 ) 3.5 cm , and were candidates for breast - conserving surgery . 
using a riskadapted approach , patients in the experimental arm could receive additional whole - breast radiotherapy in case of further risk factors ( lobular invasive cancer , extensive intraductal component )  . 
the authors separately assessed the risk of local recurrence in the prepathology ( iort given simultaneously during surgery ) and post - pathology ( iort given after surgery as a second procedure by reopening the wound after the initial excision ) strata . 
to account for the relatively short median follow - up , the authors presented subgroup analyses for pre - pathology cohorts with a median follow - up 44 months ( 1450 patients ) and 60 months ( 817 patients ) , yielding similar absolute differences in 5 - year local recurrence rates compared to the whole pre - pathology cohort . 
there were only two local recurrences , resulting in a 5 - year local recurrence rate of 0% ( one recurrence after 70.3 months ) for the experimental arm and 1.1% for the control arm ( one recurrence after 4.5 months in a patient refusing all forms of adjuvant treatment )  . 
duration of follow - up : the median follow - up of 29 months is immature and only 35% of the patients had 5 - year follow - up at the time of the analysis . 
non - inferiority design : the estimate used for the local recurrence rate of 6% at 5 years in the standard arm is strahlenther onkol ( 2020 ) 196 : 749763 considerably higher than what would be considered acceptable today . 
the targit - a authors used binomial proportions of local recurrence ( i.e. , number of recurrences divided by the number of patients ) rather than kaplanmeier estimates of local recurrence rates . 
the use of binomial proportions has been criticized , since it does not take into account that only 1222 patients had a median follow - up of 5 years , which might lead to a dilution of the treatment effect . 
furthermore , as described in the nice report 2018 [ 37 ] , the targit - a investigators quantied the difference in the kaplanmeier estimates of local recurrence , and its 95% ci , using two different methods . 
the integrated difference method presented by the investigators is not commonly used , provided more favorable results for intrabeam , and was not pre - specied in the targit - a protocol . 
use of whole - breast radiotherapy in the experimental arm : the trial used a risk - adapted approach for apbi . thus , whole - breast radiotherapy could be added to apbi , which was the case for 15% of patients in the experimental arthere were some pre - specied criteria for additional whole - breast radiotherapy , but each center could also add further criteria . 
the use of additional whole - breast radiotherapy was considerably higher in the pre - pathology stratum ( 21.6% ) than in the post - pathology stratum ( 3.6% ) , which might also have contributed to the better outcomes in the pre - pathology subgroup . 
this creates uncertainty as to whether iort alone is a safe treatment option in certain patient subgroups . in conclusion , in the face of these shortcomings , several international guidelines have discouraged the use of 50kv iort outside of clinical trials [ 39 , 40 ]  . 
this degro expert panel concluded that because of the uncertainty of interpretation in the evidence available , the 50 - kv system ( intrabeam ) cannot be recommended for routine adjuvant treatment of early invasive breast cancer after breast - conserving surgery and should preferentially be used in the context of a clinical trial . 
clinicians wishing to undertake apbi with 50 - kv photons should ensure that patients understand the uncertainties about the procedureparticularly , patients should be counseled that follow - up is too short for general recommendations ; that in corresponding clinical trial , still after very short not adequate follow - up , the risk of local recurrence was higher with apbi ; and be informed about alternative treatment options [ 22 , 37 ]  . 
when used , it should be restricted to women with all of the following criteria : invasive cancer , aged > 70 years , tumor < 2 cm , resection margins > 2 mm , grade 1 2 , pn0 , er positive , her2 negative , l0 , v0 , and eic negative . recommendation general issues we recommend that pbi with multicatheter brachytherapy or external beam radiation therapy after breast - conserving surgery ( bcs ) should be completed preferably in less than 12 weeks ( typically within 610 weeks ) and no later than 20 weeks , as better local tumor control and survival can probably be expected by keeping a shorter interval between bcs and radiotherapy [ 4148 ]  . 
of note , a recent analysis illustrated that starting radiation therapy shortly after bcs seems not to be associated with a better long - term outcome [ 49 ]  . 
if patients receive chemotherapy , pbi can be started after systemic treatmentin this scenario , we recommend starting pbi within 4 weeks after chemotherapy . it is also possible to start pbi before systemic treatment within 12 weeks . 
radiation therapy can also be given in the interval between the chemotherapy courses . in general , the physicians who indicate pbi have to reect on the fact that level 1 evidence for non - inferiority of pbi in comparison to whole - breast irradiation is given for external beam techniques and for multicatheter brachytherapy [ 8 , 50 ]  . 
if the patient is interested in pbi with iort techniques , the patient should be counseled in detail that there are uncertainties in the two available pbi phase 3 trials [ 14 , 15 ]  . 
one of the crucial problems of both pbi methods is that due to the lack of a nal pathology report at the time of iort , no denitive selection criteria could be applied at the time of pbi . 
lowenergy x - ray iort for pbi should be used within the context of a prospective registry or clinical trial ; when used , it should be restricted to certain conditions , as discussed above . selection criteria patient selection for pbi alone after bcs in patients with early breast cancer has been described in detail in euro756 strahlenther onkol ( 2020 ) 196 : 749763 pean and us guidelines many times [ 22 , 39 , 5155 ] , and the credibility of different selection criteria has been proven in corresponding contemporary phase 3 trials [ 1 , 2 , 5 , 6 , 1215 ]  . 
considering the fact only those apbi trials using strict selection are positive trials [ 1 , 2 , 12 , 13 ] as well as corresponding deliberations in study protocols and current recommendations [ 22 , 56 ] , we recommend for daily routine , outside of any clinical trials , to only consider patients for pbi if all of following selection criteria are fullled : 1 . 
in particular , the presence of lymphovascular invasion ( lvi ) and an extensive intraductal component ( eic ) cannot be fully ruled out on preoperative core needle biopsy and intraoperative frozen section , leaving a margin of uncertainty for nal eligibility . 
ws whole scar ( green ) , imtv imaging - correlated target volume ( dark blue ) , etb estimated tumor bed ( yellow ) , ctv clinical target volume ( orange ) , ptv ( brachy ) planning target volume for brachytherapy ( dark - red ) , ptv ( ebrt ) planning target volume for external beam radiation therapy ( light red ) , ptveval planning target volume for evaluation ( light - blue ) target denition for apbi with multicatheter brachytherapy or ebrt for target denition and delineation , irrespective of whether ebrt or brachytherapy techniques for pbi are intended , the estro recommendations depending on the used bcs technique should be used [ 57 , 58 ]  . the following basic rules should be respected : 1 . 
target denition and delineation after closed - cavity surgery , oncoplastic cavity surgery , and after open - cavity surgery differ . target denition and delineation after closed - cavity surgery the target is related to the scar inside the breast and to the surgical clips . 
delineation of ptv ( planning target volume )  . while delineation of the skin scar and the clips does not need further explanation , the delineation of next structures requires more attention . 
in summary , the whole surgical scar ( ws ) means delineating the whole visible surgical bed including the visible scar tissue inside the breast and all the clipsthe whole path of surgeons inside the breast tissue , starting on skin scar and ending at the deepest point on the thoracic wall . 
denition and delineation of imtv ( imaging - correlated target volume ) can be done using only preoperative imaging and is based on the tumor size and tumor localization inside the breast . 
the ctv is dened as etb plus corresponding total safety margins20 mm minus individual surgical margin in the corresponding direction , but at least 10 mm ( for example : a surgical margin of 7 mm requires a safety margin of 13 mm )  . 
in this case we recommend as standard to add an additional margin of 10 mm for the ptv , and the thoracic wall and skin can be parts of the ptv . 
if multicatheter - based apbi is planned , then typically ctv = ptv , and only in the case of an absence of clips or impaired visibility of surgical scar or cavity do we recommend adding an adapted ptv margin ( 510 mm ) in the region of doubt ( excluding thoracic wall and skin )  . 
for more details , please see the corresponding guidelines [ 57 ]  . target denition and delineation after oncoplastic surgery an important precondition here is that the position of surgical clips be intra - parenchymal and that placement occurs before the rotation of glandular tissue . 
as a consequence the preliminary ctv is dened , similar to the situation described above , as a clipped area plus corresponding total safety marginsmeaning 20 mm minus the smallest individual surgical margin , but at least 10 mm ( for example : a surgical margin of 2 mm requires a safety margin of 18 mm in all directions )  . 
if multicatheter brachytherapy is intended , the nal ctv after oncoplastic surgery is dened as the preliminary ctv + 10 mif ebrt is intended , ptv is dened as the preliminary ctv + 20 mconcerning thoracic wall and skin , the same rules as those described above should be applied . target denition and delineation after open - cavity surgery the target is related to the lumpectomy ( seroma ) cavity inside the breast and to the surgical clips , and use of ct imaging is standard . 
lumpectomy cavity boundaries have to be dened by a combination of breast tissue changes apparent on ct images , in terms of tumor pathology and preoperative imaging , uid collection within the lumpectomy cavity , and surgical clips when available . 
the ctv is dened as lumpectomy cavity plus corresponding total safety margins20 mm minus individual surgical margin in the corresponding direction , but at least 5 mm ( for example : a surgical margin of 6 mm requires a safety margin of 14 mm )  . 
for more details see please the corresponding guidelines [ 58 ]  . target denition for apbi with iort with electrons iort with electrons is performed after tumor excision and conrmation of negative margins , before oncoplastic reconstruction . 
the target volume has to encompass at least 20 mm in any direction with the exception of the skin , which is completely out of the irradiated volume , and the chest wall , which is usually protected by a shield disc . 
tube diameters have to be chosen accordingly ; diameters less than 56 cm are discouraged . the target volume thickness is assessed by intraoperative ultrasound or by inserting a needle probe at one or more 758 strahlenther onkol ( 2020 ) 196 : 749763 representative points of the parenchyma , depending on the shape of the tumor bed and chest wall curvature . 
according to measurements , electron beam energies are selected to cover the depth with at least 90% of the prescribed dose ( usually energies between 4 and 1012 mev )  . 
of note : in comparison to external techniques , no safety margins for set - up have to be considered . target denition for apbi with iort with low - energy photons ( intrabeam ) beam ct [ 71 ]  . 
image - based verication of reproducibility and precision should be performed before each fraction of apbi . the prescribed dose should be specied respecting icru 50 and icru 62 at reference point ( typically corresponding with isocenter ) , and dosevolume histogram analysis of target coverage should conrm that 100% of the prescribed dose covers > 90% of the ptv / ptv - eval . restrictions for surrounding tissues should be respected . using ebrt for apbi , the dose constraints for the target and for organs at risk are identical to those described below for brachytherapy and are summarized below . in principle , using iort with the intrabeam device , the target volume is predetermined by the surgical approach . complete macroscopic excision of the tumor is required . furthermore , based on histological examination of frozen sections , freedom of margins and negative status of sentinel nodes is required . 
then , after insertion of the adequate spherical applicator ( see above ) , the targeted volume corresponds to the volume adapted to the sphere and is determined by the size of the sphere . techniques external beam radiation therapy for external beam radiation - based apbi in supine and prone patient positions , different 3d external beam techniques with non - coplanar or with mini - tangent beams in combination with an en face electron eld , step and shoot ( ss ) and sliding window ( sw ) intensity - modulated radiotherapy ( imrt ) techniques , and vmat / intensity - modulated arc therapy techniques have been used in several prospective trials [ 2 , 12 , 13 , 5969 ]  . 
typically , the 3d - crt plans are created with four or ve wedged conformal noncoplanar elds from tangential directions , the imrt plans with ve or six coplanar elds , and the intensity - modulated arc therapy plans consist of two or more coplanar arcs . adequate target volume coverage and acceptable doses to the organs at risk are achievable with all techniques . 
when , as strictly recommend , surgical clips are in situ , 2d imaging is often sufcient to achieve appropriate positioning and the kv - kv planar imaging method is recommended . 
without surgical clips in situ , 3d images should be acquired , and the recommended method of verication is the kv cone brachytherapy brachytherapy techniques represent the most investigated irradiation techniques for apbi . 
today there are several brachytherapy techniques availablemulticatheter brachytherapy ; single - entry intracavitary devices like the mammosite balloon ; singleentry multilumen catheter devices like savi ( strut - adjusted volume implant , cianna medical , aliso viejo , ca ) , contura multi - lumen balloon ( bard biopsy systems , tempe , az ) , or clearpath ( northamerican scientic inc . , chatsworth , ca ) ; electronic brachytherapy , seeds brachytherapy , and non - invasive brachytherapy [ 7281 ]  . among all these techniques , level 1 evidence is only available for multicatheter brachytherapy [ 1 ]  . image - guided multicatheter brachytherapy - based apbi , we recommend in general to respect basic rules of image - guided interstitial brachytherapy for breast cancer [ 82 , 83 ]  . 
treatment planning and catheter insertion depend in detail on the availability of appropriate imaging facilities ( x - ray , ct , mri , ultrasound ) and on the kind of breastconserving surgery ( open cavity , closed cavity , plastic reconstruction )  . 
furthermore , the catheter reconstruction , normalization of dose distribution , dose specication , dose prescription , optimization methods , and quality management issues should be implemented in line with this guideline [ 84 ]  . iort with electrons technical details of ioert have been published repeatedly [ 85 , 86 ]  . 
ioert is nowadays mostly performed on mobile linear accelerators with tube sizes of 58 cm in diameter and electron energies usually ranging from 412 mev according to a given target volume ( see above )  . strahlenther onkol ( 2020 ) 196 : 749763 table 2 the most common dosevolume parameters used for reporting partial - breast irradiation . 
however , in most patients , the normal thickness of the chest wall ( muscle and rib cage ) may provide adequate shielding . pd prescribed dose , ptvpd volume in planning target volume receiving at least the pd dosevolume parameters and dose constraints iort with 50 - kv photons the intrabeam device provides a point source of 50 - kv x - rays at the center of a spherical applicator . 
subsequently , the subcutaneous tissues will be gathered with a purse - string suture over the sphere to adapt the target breast tissue well to the surface of the applicator sphere . 
also , at the bottom of the resection cavity , the breast tissue should be adapted to the applicator surface , i.e. , contracting the tissue using a purse - string suture , if necessary . the skin , but not the breast tissue , should be kept away from the applicator using , e.g. , a piece of wet gauze to prevent direct contact . 
for tumors near to the skin ( ( cid : 2 ) 1 cm ) , an elliptical piece of overlying skin should be excised . for an objective assessment of any treatment plan , quantitative parameters have to be analyzed and reected . 
table 2 lists the most common dosevolume parameters used in pbi with interstitial multicatheter breast brachytherapy and ebrt . based on the estro - acrop guideline [ 84 ] and nsabp protocol b - 39 / rtog 0413 [ 87 ] , we recommend the following target - related dosevolume limits : 1 . 
dose homogeneitymaximal dose should not exceed 110% of prescribed dose ( only for ebrt ) 760 strahlenther onkol ( 2020 ) 196 : 749763 the recommended dosevolume limits for oars [ 10 , 84 , 87 ] , according the current available data , are presented in table 3 . for ioert , the following dose reports and constraints are recommended : the dose is prescribed at dmax ( 100% ) or at d90 . 
v90 can be calculated by the formula of a rotating ellipsoid ( 4 3.14 / 3 a2 b )  . during ioert , the skin is outside the treated area and thus not affected by radiation . 
likewise , exit doses to lung andin case of leftsided bcheart structures amount to less than 1 gy , which is not considered as clinically relevant . dose schedule external beam radiation therapy the recommended schedules with ebrt are : 1 . 
total dose 40 gy , 2.66 gy in 1 fraction / day ~15 fraction over 3 weeks over 10 days brachytherapy the recommended schedule with pdr brachytherapy is total dose 50 gy , pulsed - dose 0.50.8 gy / pulse , scheduled every hour , 24 h per day , total treatment time 45 days . the recommended schedules for hdr brachytherapy are 8 4 gy , 10 3.4 gy , and 7 4.3 gy , twice per day , with an interval between fractions of at least 6 h , and with a total treatment time of 45 days . other fractionations can be used . 
thus , the tumor bed typically receives 20 gy , at the surface this attenuates to 57 gy at a depth of 1 cm . the dose to the skin should be < 7 gy . 
this can be realized by keeping the skin 1 cm away from the sphere . conclusion apbi has been tested in a total of nine phase 3 trials with more than 15 , 000 patients over the past 10 years [ 1 , 2 , 5 , 6 , 1216 ]  . 
these trials show that for strictly selected patients with early breast cancer , pbi by ebrt , multicatheter brachytherapy , or iort with electrons is non - inferior to the results of whole - breast irradiation in terms of local control , disease - free survival , and overall survival , and is in some aspects superior regarding late side effects and quality of life . furthermore , we conclude that pbi requires expertise encompassing : 1 . 
sauer , and degro declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
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schild16 annett maderer17 markus moehler17 received : 9 april 2020 / accepted : 23 may 2020 / published online : 12 june 2020 the author ( s ) 2020 abstract purpose to investigate the efcacy and toxicity of cetuximab when added to radiochemotherapy for unresectable esophageal cancer . methods this randomized phase 2 trial ( clinicaltrials.gov , identier nct01787006 ) compared radiochemotherapy plus cetuximab ( arm a ) to radiochemotherapy ( arm b ) for unresectable esophageal cancer . 
arm a was considered insufciently active if 2 - year os was 40% ( null hypothesis = h0 ) , and promising if the lower limit of the 95% condence interval was > 45% . 
for denitive and neoadjuvant treatment of locally advanced disease , radiochemotherapy with cisplatin and 5 - uorouracil ( 5fu ) has been the standard regimen for more than 20 years [ 2 ]  . 
combinations of radiotherapy or radiochemotherapy with newer systemic therapies such as antibodies to the epidermal growth factor receptor ( egfr ) provide additional options . overexpression of egfr is frequent and associated with a poor prognosis in patients with squamous cell carcinoma ( scc ) of the esophagus or adenocarcinoma of the gastroesophageal junction [ 46 ]  . 
these data led to the present trial that investigated the efcacy and feasibility of cetuximab added to radiochemotherapy for unresectable esophageal cancer . patients and methods this multicenter open - label , randomized phase 2 trial evaluated radiochemotherapy plus cetuximab in patients treated for unresectable esophageal cancer between 09 / 2011 and 12 / 2016 . 
inclusion and exclusion criteria are listed in table 1 . patients were randomly assigned to radiochemotherapy plus cetuximab ( experimental group , arm a ) or radiochemotherapy alone ( control group , arm b )  . 
this applied to 8 patients ( 25% ) of the experimental group and 17 patients ( 47% ) of the control group ( p = 0.079 , fishers exact test )  . 
generally , the initial clinical target volume ( ctv ) included the gross tumor volume ( gtv ) plus margins of 35 cm in the superiorinferior direction and 1 cm in the lateral and anteriorposterior directions . 
the margin from the ctv to the planning target volume ( ptv ) was 0.51.0 cin accordance with the quantec ( quantitative analyses of normal tissue effects in the clinic ) data , the mean doses for heart , lung , liver , and kidney ( bilateral ) should be < 26 gy , 7 gy , < 3032 gy , and < 15 gy , respectively [ 13 ]  . 
moreover , the dose to the spinal cord should not exceed 45 gy . a brachytherapy boost was not implemented in the protocol , since this is not a standard therapy for the primary treatment of esophageal cancer . 
two cycles of 750 mg / m2 / d of 5 - fu ( over 96 h ) were administered after radiotherapy , 5 and 9 weeks after the second course . 
if the observed 2 - year os rate was 40% ( null hypothesis h0 ) for the experimental therapy ( arm a ) , this therapy would be deemed insufciently active to pursue in further research . 
the probability of accepting the experimental therapy as promising ( 2 - year os > 45% ) when the true os rate was 40% , was 5% ( type i error )  . 
the probability of rejecting the experimental therapy as insufciently active ( 40% ) when the true os rate was promising ( > 45% ) , was 20% ( type ii error , power of 80% )  . secondary objectives included determination of 1 - year os , progression - free survival ( pfs ) , locoregional control 798 strahlenther onkol ( 2020 ) 196 : 795804 ( lc ) , metastases - free survival ( mfs ) , overall response ( or ; recist v11 [ 18 ] ) , and toxicities ( ctcae v4.03 [ 19 ] )  . 
for pfs , the event was dened as rst occurrence of radiologically proven or clinical progression or death due to progressive disease . locoregional failure was dened as progressive primary tumor and / or regional lymph nodes on endoscopy , endoscopic ultrasound , or computed tomography . 
for mfs , the event was dened as rst occurrence of distant metastasis . both groups were compared for these endpoints using the kaplanmeier method and the log - rank test . 
the comparisons of toxicities were performed with the fishers exact test . when using a standard single - stage phase 2 design according to fleming [ 20 ] , 124 evaluable patients were required to determine efcacy . 
to cover potential dropouts , 134 patients should be recruited . the trial was terminated after randomization of 74 patients ( 35 arm a , 39 arm b ) due to slow accrual . 
median follow - up was 18 ( 061 ) months in the entire cohort , and 26 ( 761 ) months in patients alive at last contact . results two - year os rates were 71% in arm a ( 95% ci : 5587% ) vs . 
all allergic reactions were managed and resolved without sequelae . two patients in arm b died during the treatment phase due to underlying disease and cardiovascular disorders , respectively . in arm a , cetuximab was discontinued after the loading dose due to allergic reactions in 4 patients . 
therefore , h0 was rejected and radiochemotherapy plus cetuximab was deemed promising . two - year os was also higher in arm b than in the reference studies [ 2 , 16 , 17 ]  . 
in the scope - 1 trial , patients were randomized to radiochemotherapy with 50 gy in 25 fractions plus four cycles of cisplatin 60 mg / m2 / d1 and capecitabine 625 mg / m2 twice daily / d1 - 21 , or to the same regimen plus cetuximab ( 400 mg / m2 / d1 followed by 250 mg / m2 weekly ) [ 25 ]  . 
it compared chemotherapy ( two cycles of 75 mg / m2 docetaxel and 75 mg / m2 cisplatin ) followed by radiochemotherapy ( 45 gy in 25 fractions plus weekly 20 mg / m2 docetaxel and 25 mg / m2 cisplatin ) and surgery to the same regimen plus cetuximab ( neoadjuvant : 250 mg / m2 weekly ; adjuvant : 500 mg / m2 every second week )  . 
in the present trial , signicantly more aes ( any grade ) were found in the experimental arm for leucopenia , hypocalcemia , hypomagnesemia , acneiform rash , radiation dermatitis , maculopapular rash , and allergic reactions . 
3 comparison of the two treatment groups ( kaplanmeier analysis and log - rank test ) with respect to overall survival ( a ) , progression - free survival ( b ) , locoregional control ( c ) , and metastases - free survival ( d ) reactions that resolved without sequelae . 
this is consistent with the majority of prospective studies that rated radiochemotherapy plus cetuximab for esophageal cancer as feasible or well tolerated [ 15 , 2934 ]  . in contrast , one randomized and four non - randomized studies concluded that radiochemotherapy plus cetuximab was associated with considerable toxicity [ 28 , 30 , 31 , 35 , 36 ]  . 
in two studies , radiochemotherapy included cisplatin and irinotecan , in one study preoperative oxaliplatin / 5fu followed by postoperative docetaxel , and in one study induction chemotherapy with epirubicin , cisplatin , and capecitabine [ 3740 ]  . 
the scope - 1 trial included two cycles of induction chemotherapy with cisplatin and capecitabine followed by radiochemotherapy with two concurrent cycles , which is also different from the most common regimens in use today [ 2 , 3 ]  . 
this may be explained by the fact that in the leopard - 2 trial , no patient in the cetuximab arm required interruption of radiotherapy for > 7 days , and only 9.4% of the patients did not receive radiotherapy . 
in the scope - 1 trial , radiotherapy was not given to 19% of patients in the cetuximab arm , and interruptions of radiotherapy appeared more frequent in the cetuximab group . 
although this regimen was associated with more grade 3 toxicities , many patients received the planned treatment due to intensive patient care including administration of chemotherapy and cetuximab under inpatient conditions . since different radiochemotherapy regimens were used in the available trials , the treatments were performed in different settings , and patient characteristics varied , it is difcult to compare the results of the leopard - 2 and other trials . 
additional limitations included lack of a central review , the fact that less than 20% of the patients had adenocarcinomas , no assessment of the expression of egfr and mutations in the vast majority of the patients , and lack of standardized procedures of treatment planning and quality assurance . 
due to these limitations , the results of the present study appear less meaningful than the results of previous larger trials [ 2528 ]  . conclusion given the limitations of the leopard - 2 trial , radiochemotherapy with cisplatin / 5 - fu plus cetuximab is feasible for unresectable esophageal cancer . 
larger studies are required to better dene the role of the addition of cetuximab to radiochemotherapy for unresectable esophageal cancer . authors contributions all authors contributed to study conception and design . 
all authors read and approved the nal manuscript . funding the leopard - 2 trial was funded by merck serono gmbh , an afliate of merck kgaa , darmstadt , germany . 
the authors are fully responsible for the content of this manuscript , and the views and opinions described in the publication reect solely those of the authors . funding open access funding provided by projekt deal . compliance with ethical guidelines conict of interest d . 
moehler declare that they have no competing interests . ethical standards the study has been approved by the ethics committee of the university of lbeck ( reference : 11 - 104 )  . 
informed consent was obtained from all individual participants included in the study . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
combs1 , 2 , 5 marciana - nona duma6 lisa marr1 benedikt feuerecker3 hendrik dapper1 rickmer braren4 received : 23 february 2020 / accepted : 28 april 2020 / published online : 19 may 2020 the author ( s ) 2020 abstract purpose in patients undergoing chemoradiation for esophageal squamous cell carcinoma ( escc ) , the extent of elective nodal irradiation ( eni ) is still discussed controversially . 
this study aimed to analyze patterns of lymph node metastases and their correlation with the primary tumor using 18f - udeoxyglucose positron emission tomography / computed tomography ( fdg - pet / ct ) scans . methods 102 escc patients with pre - treatment fdg - pet / ct scans were evaluated retrospectively . 
after exclusion of patients with low fdg uptake and patients without fdg - pet - positive lymph node metastases ( lnm ) , 76 patients were included in the nal analysis . 
all lnm were assigned to 16 pre - dened anatomical regions and classied according to their position relative to the primary tumor ( above , at the same height , or below the primary tumor )  . 
duma contributed equally to the manuscript . availability of data and materials the datasets used and / or analyzed during the current study are available from the corresponding author on reasonable request . ( cid : 2 ) med . 
22 , 81675 munich , germany partner site munich , german cancer consortium ( dktk ) , munich , germany 3 department of nuclear medicine , klinikum rechts der isar , technical university munich , ismaninger str . 
the most common sites of lnm were paraesophageal ( 63% of patients , 37% of lnm ) and paratracheal ( 33% of patients , 20% of lnm ) , while less than 5% of patients had supraclavicular , subaortic , diaphragmatic , or hilar lnm . with regard to the primary tumor , 51% of lnm were at the same height , while 25% and 24% of lymph node metastases were above and below the primary tumor , respectively . 
for thirty - three lnm ( 19% ) , the distance to the primary tumor was larger than 4 cno signicant difference was seen between lct / eus ( median 6 cm ) and lpet ( median 6 cm , p = 0.846 ) conclusion 18f - fdg - pet can help to identify subclinical lymph node metastases which are located outside of recommended radiation elds . 
this multidisciplinary approach increases the rate of complete tumor resection , overall survival ( os ) , and progression - free survival ( pfs ) compared to surgery alone [ 13 ]  . 
for patients with irresectable tumors or those unt for or declining surgery , denitive chemoradiation ( dcrt ) is the recommended treatment of choice [ 4 , 5 ]  . over the past decades , the longitudinal safety margins in neoadjuvant or denitive chemoradiation for escc have been continuously reduced [ 1 , 3 , 68 ]  . 
today , elective nodal irradiation ( eni ) is not recommended in case of neoadjuvant chemoradiation [ 1 , 8 ] , while it is still a matter of debate in case of dcrt [ 9 ]  . 
it is obvious that the reduction of longitudinal safety margins and consideration of involved - eld irradiation ( ifi ) requires reliable diagnostic and imaging techniques to identify the primary tumor and metastatic lymph nodes . 
furthermore , 18f - udeoxyglucose positron emission tomography / computed tomography ( fdg - pet / ct ) is often performed in order to rule out distant metastases before starting curative treatment . 
because fdg - pet / ct has also demonstrated promising sensitivity , specicity , and accuracy regarding the detection of lymph node metastases as well as the detection of the primary tumor [ 10 , 11 ] , implementation of pet into the radiation planning process might change the resulting target volumes , as it has already been demonstrated for other tumor entities like prostate cancer or squamous cell cancer of the tongue [ 12 , 13 ]  . the purpose of this study was to analyze the fdgpet / ct - based pattern of lymph node metastases , their distance from the primary tumor , and correlations with the primary tumor extension in patients with escc . patients and methods patients medical records and imaging information of 102 escc patients who underwent pet / ct for staging purposes between 2011 and 2016 were retrospectively reviewed . 
5 patients ( 5% ) without sufcient fdg uptake , of whom 4 patients had early tumor stages ( tis or t1 ) , and 21 patients without lnm ( n = 6 ) or lnm which were only seen by endoscopic ultrasound ( n = 15 ) were excluded from the analysis . 
in the end , a total of 76 patients were included in the analysis . tumor location was classied according to the upper end of the primary tumor within the esophagus . 
thereby , reading and interpretation of pet / ct was done by at least two experienced nuclear medicine physicians and radiologists , also taking other available information such as clinical signs and patients symptoms , endoand gastroscopic images and reports , and , if applicable , diagnostic ct images into account . 
images were interpreted using the syngo workstation ( siemens , syngo mmvvp version ve36a ; siemens healthineers , erlangen , germany ) and sectra pacs ( sectra ids7 , linkping , sweden )  . in the following , all lnm were assigned to one of 16 predened lymph node regions ( right cervical , left cervical , right supraclavicular , left supraclavicular , retrosternal , right paratracheal , left paratracheal , subaortic , subcarinal , paraesophageal above the carina , paraesophageal below the carina , right hilar , left hilar , diaphragmatic , gastric , and celiac )  . 
thereafter , the longitudinal distance between lnm and the upper primary tumor margin ( for lymph nodes above the primary tumor ) or the lower primary tumor margin ( for lymph nodes below the primary tumor ) was measured within the ct dataset . primary tumor length to analyze the impact of pet imaging on visualization of the primary tumor , two different approaches were independently pursued . 
at rst , the length of the primary tumor was assessed using all available diagnostic information ( endoscopy , computed tomography , biopsy results ) except pet imaging ( lct / eus )  . 
in a second approach , the length of the primary tumor was measured after rigid fusion of ct and attenuation - corrected pet scans ( lpet )  . in case of skip metastases or multiple tumor lesions , tumor length was dened as the distance from the upper margin of the most cranial lesion to the lower margin of the most caudal lesion . statistical calculations were performed using spss 18.0 software ( spss inc , chicago , il , usa )  . 
thereby , lct / eus was longer than lpet in 5 patients ( 71% )  . discussion we evaluated the fdg - pet / ct - based pattern of lymph node metastases and their distance to the primary tumor in patients with escc . 
no difference in terms of visualization of the primary tumor length was seen in this study . the sensitivity of pet for identication of lnm varies in the literature , but it is higher than that of ct [ 10 ]  . 
in addition , when using pet , most ( 57% ) false - positive lymph nodes are seen in the hilar region due to granulomatous diseases [ 16 ]  . 
when considering pet / ct imaging , unsuspected lymph node metastases were detected in 4 additional patients compared to ct alone . in our study , most lnm were located paratracheally and paraesophageally , and the pattern of lnm depended on primary tumor location , which is in line with the results of other trials [ 1820 ]  . 
gastric for patients with tumors in the upper third of the esophagus ( n = 31 ) , the most common sites of lnm were paraesophageal above the carina ( 58% of patients ) and left paratracheal ( 42% of patients )  . 
in contrast , for patients with primary tumors in the middle third of the esophagus ( n = 36 ) , patients most commonly presented with paraesophageal lnm above ( 33% of patients ) and below the carina ( 33% of patients ) , but patients rarely presented with supraclavicular , retrosternal , gastric , or hilar lnm ( < 5% of patients )  . 
4 length of the primary tumor as assessed by ct / endoscopy and pet . ct computed tomography , pet positron - emission tomography strahlenther onkol ( 2020 ) 196 : 787794 carina , most often had lymph nodes in the supraclavicular ( 27% ) , upper paratracheal ( 11% ) , lower paratracheal ( 13% ) , and retrotracheal ( 17% ) regions . 
however , in patients with upper thoracic tumors , only a small number of lnm were located below the carina ( 18% ) , which seems to be comparable to our results . 
in patients with lower thoracic tumors , in the study of garcia et al . , the most commonly involved lymph nodes were located paraesophageally below the carina ( 19% ) and abdominally ( 54% )  . 
 [ 18 ] further analyzed the distance of lnm to the primary tumor : 11% ( for upper thoracic tumors ) and 58% ( for lower thoracic tumors ) of the paraesophageal lymph nodes were non - adjacent to the primary tumor . 
in our study , 89% of patients had tumors in the upper or middle third of the esophagus and 49% of lnm were non - adjacent . this lower rate of non - adjacent lnm described by garcia et al . 
in addition , the median distance between lnm and the primary tumor was 0 cm for upper thoracic tumors and 1.5 cm for lower thoracic tumors , which is smaller than in our study . 
however , this difference is explained by the fact that the distance to the primary tumor was calculated by including all lymph nodes in the study by garcia et al . , while in our study the median distance was calculated for lnm above and below the primary tumor only . 
because pet strongly correlates with eus and histopathologic results [ 24 , 25 ] , this probably also explains the strong correlation between tumor length as assessed by pet and ct / endoscopy in our study . it has already been demonstrated that pretherapeutic staging using pet / ct imaging is associated with prostrahlenther onkol ( 2020 ) 196 : 787794 longed recurrence - free survival ( rfs ) in escc patients undergoing neoadjuvant or denitive chemoradiation [ 26 ]  . since pet imaging increases the detection rate of distant metastases compared to ct [ 27 , 28 ] , some patients who are only staged with ct might have undetected distant metastases which affect rfs . 
however , based on our results , one could speculate that consideration of pet imaging for radiation planning also improves rfs by identifying metastatic lymph nodes which are located outside of standard ptvs . 
in the already mentioned study by leong and colleagues [ 17 ] , morphologically unsuspected lymph nodes with pathologic fdg uptake which were also located outside the ct - based treatment volume were identied in 3 of 21 patients ( 14% )  . the omission of eni not only revealed promising results in case of neoadjuvant chemoradiation [ 1 ] , but there was also no difference regarding os or local control between eni and ifi in case of denite chemoradiation [ 9 , 29 ]  . 
in addition , ifi can reduce the dose distribution to the lungs and the rate of pulmonary toxicities [ 29 , 30 ] , while a concurrent reduction of the doses to the heart can decrease the rate of symptomatic or asymptomatic pericardial effusion [ 31 ]  . 
this should be kept in mind before considering eni , even in patients who did not undergo pet staging . nonetheless , in 20% of our patients , some lnm were more than 4 cm away from the primary tumor . this study has some limitations . 
this assumption is conrmed by the fact that pet / ct only identied lnm in 76 of 91 patients ( 84% ) who were staged as n + by eus . this is probably caused by the limited spatial resolution of pet . 
since this is only a problem for lnm adjacent to the primary tumor , the rate of lnm located at the same height as the primary tumor might also be underestimated . 
nonetheless , these lymph nodes do not represent a problem in the planning process due to the circular safety marganother limitation is that lnm were identied by pet / ct imaging only . as discussed earlier , this bears the risk of including falsepositive lnm . 
in this context , we should also state that due to the retrospective nature of the study , no standardized suvmax value was used to identify lnm , which impacts the comparability and also affects sensitivity and specicity . nonetheless , all imaging data were assessed by experienced nuclear physicians and / or radiologists . in conclusion , 18f - fdg - pet can help to identify subclinical lymph node metastases which are located outside of recommended radiation elds . 
pet - based involved - eld irradiation might be the ideal compromise between small treatment volumes and decreasing the risk of undertreatment of subclinical metastatic lymph nodes and should be further evaluated . funding this research did not receive any specic grant from funding agencies in the public , commercial , or not - for - prot sectors . author contribution sm collected and interpreted data , performed statistical analysis , and drafted the manuscript . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
duma1 , 5 received : 19 december 2019 / accepted : 9 may 2020 / published online : 2 june 2020 the author ( s ) 2020 abstract objective tangential eld irradiation in breast cancer potentially treats residual tumor cells in the axilla after sentinel lymph node biopsy ( slnb )  . 
so far , the impact of hypofractionation on the effect of incidental lymph node irradiation has not be addressed . materials and methods biological effective dose ( bed ) and tumor control probability ( tcp ) were estimated for four different hypofractionated radiation schemes ( 42.50 gy in 16 fractions [ fx ] ; 40.05 gy in 15 fx ; 27 gy in 5 fx ; and 26 in 5 fx ) and compared to conventional fractionation ( 50 gy in 25 fx )  . 
subsequently , we assessed bed and tcp in 431 axillary lymph node metastases . results the extent of incidental lymph node irradiation and the fractionation scheme have a direct impact on bed and tcp . 
hypofractionation led to a signicant reduction of mean tcp of lymph node metastases for all schedules . conclusion our data indicate that hypofractionation might affect the effectiveness of incidental radiotherapy in the axilla . this is particularly relevant for patients with positive sentinel lymph nodes who receive slnb only . keywords biological effective dose tumor control probability incidental axillary dose sentinel node ( cid : 2 ) marciana n . 
1 , 85764 neuherberg , germany 5 department of radiotherapy and radiation oncology , friedrich schiller university hospital , bachstrae 18 , 07743 jena , germany introduction the z0011 trial [ 1 ] demonstrated that use of sentinel lymph node biopsy ( slnb ) alone compared with axillary lymph node dissection ( alnd ) does not result in inferior survival in patients with one or two positive sentinel lymph nodes . interestingly , the regional recurrence rate after slnb alone was very low ( < 1% ) even though approximately 27% of patients had lymph node metastases in the undissected axillary nodes . 
since tangential eld irradiation delivers a relevant dose to the axillary levels , adjuvant radiotherapy contributes to eradication of microscopic disease in the undissected axilla and accounts for the good oncologic outcomes after slnb only . 
the ma20 [ 3 ] and eortc 22922 - 10925 [ 4 ] studies have shown that elective lymph node irradiation ( supra / infraclavicular and internal mammary ) is effective in lowering regional 772 strahlenther onkol ( 2020 ) 196 : 771778 table 1 patient characteristics patient age ( years ) ataken at the nipple line 26.6 kg / m2 26.0 kg / m2 20.6 kg / m2 bust girtha 98 cm 107 cm 85 cm breast volume 763 cm3 1201 cm3 329 cm3 materials and methods in a previous study , 580 f18 - fdg - pet / ct - positive lymph node metastases of breast cancer patients were detected and mapped in a ct template [ 16 ]  . 
the dosimetric data was then transferred to spss ( ibm statistics version 25 , ibm corp . , armonk , ny , usa )  . treatment planning planning cts of the three patients were acquired on a somatom emotion scanner ( siemens medical solutions , erlangen , germany )  . 
contouring of the planning target volume ( ptv ) and organs at risk ( oar ) was performed according to the rtog breast - contouring atlas [ 17 ] in all ct scans . 
this has a direct impact on the biological effective dose ( bed ) and tumor control probability ( tcp ) of microscopic disease in the axillary lymph nodes [ 911 ]  . nowadays , moderate hypofractionated radiotherapy ( 4042.5 gy in 1516 fractions [ fx ] ) is the recommended therapy for adjuvant radiotherapy after breast - conserving surgery for most patients [ 1 , 1214 ]  . 
since the study remains in follow - up , results are pending . nonetheless , two different approaches have changed simultaneously in breast cancer treatment : hypofractionation is considered a standard therapy and at the same time , deescalation of axillar surgery is conducted for an increasing number of patients . 
a p - value < 0.001 was dened as statistically signicant . bed and tcp results in 2009 , planatiotis and dale [ 11 ] published a study in the international journal of radiation oncology , biology , physics linking bed to tcp based on the existing randomized trials of rt vs . 
non - rt in breast cancer including hypofractionated rt schedules . for calculation of bed and tcp , excel ( microsoft corporation , version 16 , redmond , washington , united states ) and spss ( ibm statistics ) were used . 
1. bed = fx ( cid : 2 ) d ( cid : 2 ) ( cid : 3 ) correspondingly to the study of planatiotis and dale [ 11 ] , we used an / value of 4 gy for breast cancer cells . the bed for every lymph node ( representing areas at risk of containing microscopic disease ) in the three patients was calculated in dependence of the fractionation schedules ( table 2 )  . 
the dose in the lymph nodes estimation of bed and tcp during incidental lymph node irradiation both the extent of incidental irradiation and the fractionation schedules had an important impact on the bed . the bed curves for the different fractionation schedules are presented in fig . 
the highest bed values ( bedmax = 75.0 gy ) were measured for the conventional fractionation schedule and the lowest ( bedmax = 59.8 gy ) for the fast - forward schedule . 
a biological effective dose ( bed ) in dependence of the extent of incidental lymph node irradiation ( 0100% ) compared to the prescribed dose ; b function and curve linking bed to tumor control probability table 3 percent of prescribed dose in the lymph nodes located in the axillary lymph node levels iiii . 
in 2018 an updated american society for radiation oncology ( astro ) evidence - based guideline was published , recommending hypofractionation as the standard scheme during whole breast irradiation [ 1 ]  . 
furthermore , in the z0011 trial , which is one of the foundations of todays guidelines , high tangents were used in approximately 50% of the patients and 17% received supraclavicular elds [ 17 ]  . 
hence , the outcome of patients treated with slnb only receiving hypofractionated radiotherapy to the breast remains unclear . the tcps in our study were calculated according to a model by plataniotis and dale [ 10 ]  . 
when interpreting our data , it needs to be taken into consideration that tcps most likely do not correctly reect the actual expected tumor control in axillary lymph nodes . firstly , because the model was calculated for local breast cancer recurrences not for axillary recurrences . 
a pre - rt average clonogen number per tumor of 59.2 was assumed , which does not necessarily reect the clonogen in the axillary lymph nodes in case of residual tumor . 
even though the model might not predict the exact control probability in the lymph nodes , it clearly helps to understand the effect of hypofractionation during incidental irradiation . in accordance with other studies , the model by plataniotis and dale suggest an s - shape of the tcp curve , with increasing slope from low to moderate beds and increasing slope from moderate to high beds [ 10 , 20 ]  . 
nevertheless , taking the results from the ma - 20 [ 3 ] and eortc studies [ 4 ] into account , treatment of microscopic disease in the lymph node system has a potential effect on distant metastases and disease - free survival . 
thus , it is unclear whether the ( theoretical ) reduction of tcp has a ( measurable ) clinical impact in early breast cancer patients and hypofractionation remains the standard regimen for most patients . as tangential eld irradiation is the standard technique for breast radiotherapy in many departments [ 21 , 23 ] , we analyzed the dose distribution to the axillary lymph nodes during tangential eld irradiation . 
differently from our study , most previous studies estimated the dose distribution in the lymph node areas as dened by rtog or estro guidelines [ 5 , 6 , 9 , 11 , 24 , 25 ]  . 
however , these guidelines dene a treatment volume and do not necessary reect the whole axillary lymph node drainage system and both primary lymph node metastases and lymph node recurrences occur outside the estro and rtog margins [ 16 , 26 ]  . 
the 2018 published 3d lymph node atlas [ 16 ] allows dose evaluation and calculation of the tcp for actual areas at risk in which lymph node metastases frequently occur . 
still , it should be considered that detected areas at risk in the lymph node atlas ( including also recurrent and metastatic breast cancer patients ) might not be representative for primary early breast cancer patients receiving slnb only . the total treatment time between conventional fractionation and the analyzed hypofractionated schemes differed by up to 28 days . 
however , the presumed time effect conicts with the results of the ontario trial testing 42.5 gy in 16 fractions without any differences in long - term outcome . furthermore , the literature regarding the impact of a treatment delay are inconsistent and the repopulation kinetics of microscopic breast cancer are known to be slow [ 28 ]  . 
even though the subject remains controversial , neglecting the potential impact of overall treatment time in the tcp formula ( and therefore in our calculations ) can be seen strahlenther onkol ( 2020 ) 196 : 771778 as a relevant limitation of our study . 
given the limitations of the tcp calculation , the level of signicance was set at < 0.001 to keep statistical uncertainties as low as possible . for a better accuracy of the model , we analyzed only schemes with 5 fx per week . 
since the uk - fast trial showed promising results after 3 years of follow - up , extreme hypofractionation with higher single doses could become more important . thus , the potential effect of hypofractionation in the axillary lymph nodes should be considered for further prospective studies as well as during interpretation of results . conclusion according to the available radiobiological models , hypofractionated rt leads to lower tcps in areas of risk containing microscopic disease in the axilla compared to normofractioned rt . 
combs : advisory boards / advisor : bms , astra zeneca , roche , novocure , daiichi sankyo , icotec ; speaker honoraria : bms , astra zeneca , roche , novocure , daiichi sankyo , icotec , brainlab , varian , accuray , zeiss meditec , sennewald , elekta , merck darmstadt , medac . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
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juni 2020 der / die autor ( en ) 2020 hintergrund die orale mukositis ( om ) ist eine huge und stark beeintrchtigende nebenwirkung der strahlentherapie ( rt ) bei kopfund halstumoren , die fast immer eine intervention im rahmen von supportivmanahmen erfordert . das ziel dieser multiinstitutionellen , randomisierten , doppelblinden phase - iib - studie war es , die wirksamkeit und sicherheit von gc4419 , eines superoxiddismutasemimetikums zur reduktion oraler mukositis , gegenber einem placebo zu eruieren [ 1 ]  . patientengut und methoden in die multizentrische , prospektive studie wurden insgesamt 223 patienten aus 44 institutionen in den usa und kanada mit einem lokal fortgeschrittenen mundhhlen - / oropharynxkarzinom eingeschlossen . 
alle patienten wurden einer denitiven oder postoperativen radiochemotherapie ( rct ) unterzogen . die gesamtstrahlendosis am oropharynx betrug 6072 gy ( minimale dosis an mindestens zwei lokalisationen der oralen schleimhaut > 50 gy )  . 
simultan wurde cisplatin ( wchentlich oder alle 3 wochen ) verabreicht . alle patienten erhielten vor jeder imrt - fraktion entweder gc4419 intravens als 60 - mintige infusion oder ein placebo . 
randomisiert wurde zwischen einer dosierung von 30 mg ( n = 73 ) oder 90 mg ( n = 76 ) sowie placebo ( n = 74 )  . der who - grad der om wurde whrend der behandlung originalpublikation anderson cm , lee cm , saunders dp et al ( 2019 ) phase iib , randomized , double - blind trial of gc4419 versus placebo to reduce severe oral mucositis due to concurrent radiotherapy and cisplatin for head and neck cancer . 
der primre endpunkt war die dauer der schweren om , die fr jede aktive dosisstufe gegenber dem placebo getestet wurde ( zweiseitige intention - to - treat - analyse bei p = 0 , 05 )  . 
die 30 - mg - dosierung zeigte werte , die zwischen der hheren dosierung und placebo lagen . das nebenwirkungsprol war in allen armen vergleichbar . eine spezische toxizitt von gc4419 wurde nicht festgestellt . 
die 2 - jahres - nachbeobachtung der tumorkontrolle ist noch nicht abgeschlossen . schlussfolgerungen der autoren gc4419 mit einer tglichen dosis von 90 mg fhrt zu einer signikanten , klinisch relevanten reduzierung der radiogenen oralen mukositis ( dauer , inzidenz und schweregrad )  . 
eine nachfolgende phase - iii - studie ( roman ) hat begonnen [ 2 ]  . strahlenther onkol ( 2020 ) 196 : 834836 kommentar behandlung der radiogenen mukositis mit mimetika der superoxiddismutase ( sod ) sinn oder unsinn ? die zweite randomisierte studie zur wirksamkeit von gc4419 zeigt sehr gute ergebnisse [ 1 ]  . 
behandlung der radiogenen mukositis ? die iatrogene orale mukositis bei patienten mit kopfhals - tumoren , charakterisiert durch entzndung , atrophie und abbau der schleimhaut oder der auskleidung der mundhhle , gehrt zur tglichen strahlentherapeutischen erfahrung . 
die damit assoziierten schmerzen , odynodysphagie , dysgeusie , verminderte orale nahrungsaufnahme und systemische infektionen stellen alle strahlentherapeuten vor therapeutische herausforderungen und kompromittieren gelegentlich den onkologischen behandlungserfolg . die behandlung der radiogenen mukositis ist multifaktoriell . 
die manganhaltige verbindung gc4419 gehrt zusammen mit amifostin , palifermin und rrx - 001 zu den radioprotektiva mit potenziellem oder geprftem klinischem effekt [ 3 ]  . eine bermige bildung von reaktiven sauerstoffspezies wie superoxid ( radikales o2 ) spielt eine zentrale rolle in der pathogenese der mukositis . 
die absorption von ionisierender strahlung unterbricht direkt chemische bindungen in zellmoleklen oder verursacht schden durch bildung von radikalen , die mit nahegelegenen moleklen reagieren und proteine , lipide und nukleinsuren schdigen . 
die befrworter der substanz argumentieren jedoch , dass gc4419 superoxid selektiv in ein h2o2 - molekl zerlegt , das selbst ein eigenstndiges oxidationsmittel ist und somit ebenfalls einen zytotoxischen effekt am tumor entfalten kann . strahlenbiologischen erkenntnissen folgend , spielt die vernichtung basaler stammzellen der schleimhaut eine entscheidende rolle bei der entstehung der radiogenen mukositis . 
sollte gc4419 diese wirkung entfalten , knnte es trotz recht aufwendiger applikation knftig eine wichtige rolle in der multifaktoriellen behandlung der radiogenen mukosaschden einnehmen . fazit die aufgabe des radioonkologen ist in erster linie die tumorbekmpfung und erst in zweiter linie die kontrolle der radiogenen mukositis . 
adamietz gibt an , dass kein interessenkonikt open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
anderson cm , lee cm , saunders dp , curtis a , dunlap n , nangia c , lee as , gordon sm , kovoor p , arevalo - araujo r , barad v , peddada a , colvett k , miller d , jain ak , wheeler j , blakaj d , bonomi m , agarwala ss , garg m , worden f , holmlund j , brill jm , downs m , sonis st , katz s , buatti jm ( 2019 ) phase iib , randomized , double - blind trial of gc4419 versus placebo to reduce severe oral mucositis due to concurrent radiotherapy and cisplatin 836 strahlenther onkol ( 2020 ) 196 : 834836 for head and neck cancer . 
holmlund j , brill jm , lee cm , saunders d , sonis st , downs m , anderson cm ( 2019 ) roman : reduction in oral mucositis with avasopasem manganese ( gc4419 ) phase 3 trial in patients receiving chemoradiotherapy for locally - advanced , non - metastatic head and neck cancer . 
oronsky b , goyal s , kim mm , cabrales p , lybeck m , caroen s , oronsky n , burbano e , carter c , oronsky a ( 2018 ) a review of clinical radioprotection and chemoprotection for oral mucositis . 
anderson cm , sonis st , lee cm , adkins d , allen bg , sun w , agarwala ss , venigalla ml , chen y , zhen w , mould dr , holmlund jt , brill jm , buatti jm ( 2018 ) phase 1b / 2a trial of the superoxide dismutase mimetic gc4419 to reduce chemoradiotherapy - induced oral mucositis in patients with oral cavity or oropharyngeal carcinoma . 
okunieff p , swarts s , keng p , sun w , wang w , kim j , yang s , zhang h , liu c , williams jp , huser ak , zhang l ( 2008 ) antioxidants reduce consequences of radiation exposure . 
we aimed to explore the natural course of oligometastatic colorectal cancer and to investigate how sbrt of lung metastases can delay the progression to polymetastatic disease ( pmd )  . methods 107 lung oligometastases in 38 patients were treated with sbrt at a single institution . 
genetic biomarkers such as egfr , kras , nras , braf , and microsatellite instability were investigated as predictive factors for response rates . results median follow - up was 28 months . 
at median follow - up , 7 patients were free from disease and 31 had progression : 18 patients had sequential oligometastatic disease ( somd ) and 13 polymetastatic progression . 
median overall survival ( os ) was 39.5 months ( range 2664 months ) and 2 - year os was 71.1%. conclusion the present results support local ablative treatment of lung metastases using sbrt in oligometastatic colorectal cancer patients , as it can delay the transition to pmd . 
patients who progressed as somd maintained a survival advantage compared to those who developed pmd . keywords metatases directed therapy stereotactic ablative radiotherapy sabr gastrointestinal cancer polymetastatic disease ( cid : 2 ) luca nicosia lucanicosia.rg@gmail.com 1 advanced radiation oncology department , irccs sacro cuore don calabria hospital , cancer care center , via don sempreboni 5 , 37034 verona , negrar , italy 2 radiation oncology department , asst spedali civili di brescia , brescia university , brescia , italy 3 department of radiation oncology , ospedale di esine , asl valle camonica - sebino esine , esine , italy 4 radiation oncology department , university hospital , lmu munich , munich , germany 5 university of brescia , brescia , italy introduction colorectal cancer is the fourth most common cancer in humans and the second leading cause of cancer death in western countries [ 1 ]  . 
if the oligometastatic disease is considered potentially curable and the polymetastatic disease is amenable to palliative therapies , the ability to keep patients in an oligometastatic stage for as long as possible could determine a further survival advantage [ 5 ]  . stereotactic body radiation therapy ( sbrt ) or stereotactic ablative radiation therapy ( sabr ) is a well - established and well - tolerated technique for the treatment of metastases of solid tumors and usually obtains local control rates up to 9095% , depending on histology . 
moreover , patients with solely lung metastases might have longer survival than those with extrapulmonary metastases [ 10 ]  . in order to improve local sbrt efcacy , several predictive factors were recently identied [ 11 , 12 ]  . 
nevertheless , the available evidence for colorectal metastases remains scare and indicates that a high biological effective dose ( bed ) of > 200 gy and a small treated volume are related to improved local control rates [ 9 , 10 ]  . 
in other histologies , for example , breast and nsclc , there is more robust evidence supporting a potential correlation of her2 and egfr with the response to srs [ 13 , 14 ]  . 
moreover , according to our internal protocol , patients were discussed in a multidisciplinary tumor board ( including a thoracic surgeon , oncologist , radiation oncologist , radiologist , nuclear medicine physician , pulmonologist , and pathologist )  . pre - treatment evaluation included clinical examination , total body computed tomography ( ct ) scan , and 18 - uorodeoxyglucose positron - emission tomography ( fdgpet / ct ) in suspicious cases . the current retrospective study was carried out according to the declaration of helsinki ( 1964 ) and was approved by the internal review board ( department of advanced radiation oncology , irccs sacro cuore don calabria hospital , negrarverona )  . 
the maximum intensity projection was reconstructed from the 10 - phase 4d - ct images and used to delineate the internal target volume ( itv ) and the gross tumor volume ( gtv )  . 
dose was prescribed at the median ptv dose , assuring 95% of the prescribed dose to at least 95% of the ptv and a nearmaximum dose not superior to 107% of the prescribed dose [ 15 ]  . 
constraints for organs at risk ( oars ) were utilized according to the fractionation schemes and the tumor location [ 16 ]  . all plans were performed by volumetric intensity - modulated radiotherapy ( vmat ) with attening lter free ( fff ) beams [ 17 ]  . 
before each fraction , image - guided radiotherapy was performed by means of cone beam computed tomography ( cbct )  . follow - up and response assessment the rst follow - up was performed within 90 days after the end of treatment and included a thoracic ct . 
subsequent follow - up was performed using fdg / pet - ct every 3 months for the rst 2 years after sbrt and every 6 months thereafter . moreover , physical examination and basal blood chemistry analyses were performed at each follow - up . 
after sbrt , when disease progression was observed during the follow - up period , patients were evaluated to receive either further local ablative therapy , systemic therapy , or best supportive care , based on the physicians choice . 
treatment - related adverse effects were prospectively recorded according to the common terminology criteria for adverse events ( ctcae ) v 5.0. strahlenther onkol ( 2020 ) 196 : 813820 study endpoints and statistics table 1 patient characteristics ( n = 38 ) the primary endpoint was to estimate the time to pmd conversion ( ttpmc ) after sbrt . 
moreover , lpfs , os , progression - free survival ( pfs ) , and sequential somd rate were evaluated . ttpmc was dened as the time from sbrt to the occurrence of > 5 new metastatic lesions . 
moreover , in - eld recurrence was dened as any recurrence that occurred within the 95% isodose curve and marginal recurrence as any recurrence that occurred within the 50% isodose curve . 
somd rate was dened as the occurrence of 5 new metastatic lesions after sbrt . survival was estimated using the kaplanmeier method . prognostic factors such as age , sex , egfr , kras , nras , braf , number of treated lesions , lesion diameter , gtv size , ptv size , type of response , and somd were included in the statistical analysis . 
multivariate analysis ( mva ) was performed with the multiple logistic regression method and the log - rank test to identify predictive factors ; we included all the clinically relevant variables in the analysis . 
1 kaplanmeier curve showing cancer - specic survival stratied for type of progression , calculated from the rst stereotactic body radiotherapy italicized values indicate signicant correlations ttpmc time to polymetastatic conversion , lpfs local progression - free survival , os overall survival , css cancer - specic survival , pfs progression - free survival , somd sequential oligometastatic disease , n . 
at the last follow - up , 7 out of 38 patients ( 18.4% ) had no evidence of disease . among the remaining 31 patients , at rst relapse after sbrt ( pfs - 1 ) , 18 patients ( 58% ) had somd and 13 patients ( 42% ) had developed pmd . 
patients with somd were treated with a second sbrt course , while pmd patients were evaluated for systemic therapy ( st ) with or without palliative rt ( 10 ) or best supportive care ( bsc ; 3 ) , according to physicians choice . 
some authors hypothesize that the higher radioresistance may rely on the origin of radioresistant cell clones selected by neoadjuvant radiotherapy for primary tumor , particularly for secondary rectal lesions [ 22 ]  . this issue was also recently investigated in a study by ahmed et al . 
they also assessed the role of the radiosensitivity index ( rsi ) , a validated gene signature for tumor radiosensitivity , with the purpose of developing a genomically adjusted radiation dose , proposing the need for higher sbrt doses far beyond the well - established minimum threshold of bed = 100 gy [ 24 , 25 ]  . 
observed a profound difference in terms of / ratio between colorectal and non - colorectal histologies , suggesting the need to increase not only the total dose , but also the fractional dose [ 9 ]  . in our retrospective series , we reported an excellent 2 - year lpfs rate of 80% , which is similar or higher compared to other experiences [ 27 , 28 ]  . 
our very promising results support the impact of higher bed schedules , given that our median bed10 was 105 gy . we also observed a signicant correlation between local control and braf wildtype status , which is reported to favorably impact on clinical outcomes [ 29 ]  . 
the role of braf mutational status has also been investigated in other tumor subtypes , with studies reporting controversial results , as the braf mutation was found to be predictive for local control in melanoma brain metastases treated with radiosurgery , while regarding thyroid cancer , in vitro studies demonstrated that a braf mutation promotes cellular mechanisms and leads to higher radioresistance [ 30 , 31 ]  . there is growing effort in the scientic community to determine the potential prognostic signicance of genetic mutations for clinical outcomes in several cancer subtypes [ 32 , 33 ]  . 
despite the small sample size , this study focuses on the need to further investigate whether examination of mutational status can inuence the choice of the best therapeutic combination with radiotherapy [ 34 ]  . to date , radiotherapy the optimal combination of and systemic therapy for the oligometastatic disease is still a matter of debate . 
the latest available prospective ndings show that the addition of radiotherapy in the oligometastatic setting leads to improved survival rates both in oligometastatic de novo patients [ 3 ] and in oligoresidual patients after systemic treatment [ 35 ]  . 
more specically for colorectal cancer , some authors hypothesize that sbrt alone may delay the start of systemic treatments , thus postponing the detrimental impact of chemotherapy on quality of life without compromising clinical outcomes [ 36 , 37 ]  . 
on the other hand , the synergistic effect of sbrt and simultaneous chemotherapy is favorably reported by thibault et al . , as it achieves better results in terms of os 818 strahlenther onkol ( 2020 ) 196 : 813820 and local control [ 38 ]  . 
accordingly , the japanese radiation oncology study group supported the role of chemotherapy after sbrt as a positive prognostic factor for local control in a retrospective series of pulmonary oligometastases from colorectal tumors [ 39 ]  . we observed a median pfs of 7 months ( range 49 months )  . 
only 7 patients had no evidence of disease after sbrt at the time of the analysis , while the remaining patients showed progression with sequential oligometastatic disease in 18 cases and polymetastatic disease in 13 cases . 
interestingly , within this subgroup , 5 patients progressed again with polymetastatic disease , while 5 were free of disease , and the remaining 8 patients received a further course of sbrt , given the repeated oligometastatic progression . 
these results are in line with previous experiences that showed that repeated local therapy may impact survival [ 40 ]  . keeping in mind the small sample size of the present series , this is in agreement with the recent ndings of greco et al . 
these authors postulated a three - tiered categorization of the natural history of oligometastatic disease , hypothesizing different phenotypes of the oligometastatic status in which the chances of obtaining a curative effect from local ablative treatments depend on the activity of the regulatory pathways leading to the polymetastatic condition [ 41 ]  . this could be crucial for management of oligometastatic colorectal patients , since postponing the transition to the polymetastatic state has a remarkable impact on os . 
identication of further intermediate states between the oligoand the polymetastatic disease , like the so - called sequential oligometastatic disease ( somd ) , will likely provide a longer interval before systemic dissemination takes place [ 42 ]  . the present study has some limitations . 
nonetheless , we have collected excellent results in terms of local control , with a positive predictive power of the braf wildtype status , thus strengthening the role of local ablative treatments as a therapeutic pathway that combines high local control rates with a favorable impact on survival outcomes . conclusion the present study supports the role of sbrt in the treatment of lung oligometastases arising from colorectal cancers . 
rbe1 received : 3 september 2019 / accepted : 7 january 2020 / published online : 31 january 2020 the author ( s ) 2020 abstract purpose 53bp1 foci detection in peripheral blood lymphocytes ( pbls ) by immunouorescence microscopy ( ifm ) is a sensitive and quantiable dna double - strand break ( dsb ) marker . 
in addition , high - resolution transmission electron microscopy ( tem ) with immunogold labeling of 53bp1 and dsb - bound phosphorylated ku70 ( pku70 ) can be used to determine the progression of the dna repair process . 
in addition , tem was used to quantify gold - labelled pku70 dimers and 53bp1 clusters within euchromatin and heterochromatin of pbls . results ifm analyses showed that during radiation therapy , persistent 53bp1 foci in pbls accumulated with increasing numbers of administered rt fractions . 
this 53bp1 foci accumulation was not inuenced by the irradiation technique applied ( 3d conformal radiotherapy versus intensity - modulated radiotherapy ) , dose intensity per fraction , number of irradiation elds , or isodose volume . 
the action of both seems to depend on their ability to induce mutagenic and clastogenic dna damage , including crosslinks , strand breaks , replication errors , and base adducts [ 2 , 3 ] , which can induce cell death . 
precise dose distributions to the planning target volume ( ptv ) by highly conformal techniques are critical for minimizing side effects in adjacent organs at risk . dna damage repair mechanisms protect against adverse effects of carcinogenic therapies . 
while the likelihood of rt - induced side effects in organs at risk can be reli822 strahlenther onkol ( 2020 ) 196 : 821833 ably assessed by dosimetric calculations , peripheral blood lymphocytes ( pbl ) , especially in patients who received radiochemotherapy ( rct ) , are exposed to an erratic amount of events that may cause dna damage . 
during nonhomologous end joining ( nhej ) , the major mammalian dsb repair pathway , the ku70ku80 heterodimer recognizes dsbs and maintains the broken dna ends in close proximity until the dsb is rejoined [ 4 ]  . 
in addition , the phosphorylated histone variant of h2ax , h2ax , recruits repair proteins such as 53 binding protein 1 ( 53bp1 ) to the chromatin surrounding the dsb [ 5 , 6 ]  . 
53bp1 is an important regulator in the cellular damage response to dsbs , promoting the binding of the distal dna ends which occurs during variable diversity joining ( v ( d ) j ) , class - switch recombination ( csr ) , or fusion of the unprotected telomeres . recruitment of 53bp1 to the site of damaged chromatin also promotes nonhomologous end joining - mediated dsb repair ( nhej ) while preventing homologous recombination ( hr ) [ 710 ]  . 
specic primary and uorescent secondary antibodies against 53bp1 localized to dsb repair foci [ 8 , 11 ] may be used as markers to quantify dsb repair by immunouorescence microscopy ( ifm )  . assuming that each 53bp1 focus corresponds to one dsb , the number of foci in the nucleus can be applied to measure dna damage caused by radiation exposure [ 1218 ]  . 
in addition , the hematopoietic system is radiosensitive and lymphocytes and their subpopulations are well characterized in terms of phenotype and function [ 1922 ] and can be reliably isolated from blood [ 23 ]  . 
moreover , pbls are in the resting state ( g0 ) of the cell cycle [ 24 , 25 ] , thereby resulting in a prolonged presence of dna damage [ 2628 ]  . due to the limited resolution of ifm , 53bp1 visualization does not provide full - scale information regarding individual repair points and radiation sensitivity . 
the detection of both 53bp1 and the dsb - bound phosphorylated ku70 ( pku70 ) would signal incomplete nhej repair sites . here , high - resolution transmission electron microscopy ( tem ) with gold - labeled pku70 and 53bp1 [ 29 , 30 ] was used to determine the suitability of this analysis for assessing individual pbl radiation sensitivity in patients with different tumor entities ( head and neck or rectal cancers ) , isodose volumes , irradiation techniques ( intensity modulated radiotherapy , imrt or 3d - conformal rt , 3d - crt ) , and treatment approaches ( rt or rct )  . materials and methods patients and treatment conditions this study was conducted in accordance with the helsinki declaration and with approval of the local ethics committee ( rztekammer des saarlandes )  . 
patients meeting the following inclusion criteria were enrolled between march 2011 and may 2012 : aged between 18 and 80 years ; karnofsky index > 70% ; completely resected head and neck squamous cell cancer ( oral cavity , oropharynx , hypopharynx , or larynx ) with postoperative rt indicated with or without chemotherapy ; or diagnosis of rectal cancer with an indication for neoadjuvant or adjuvant pelvic radiotherapy ( with or without chemotherapy )  . 
imrt with a predened ptv arrangement of seven coplanar beam angles with 70 beam segments and standardized objectives based on the icru report 83 [ 31 ] and constraints for normal tissues ( brainstem , spinal cord , parotid glands , esophagus ) based on quantec data [ 32 ] with individualized clinical assessments was mandatory for patients with head and neck cancer ( n = 4 )  . 
a 60 gy reference dose was prescribed to primary tumor sites and lymph node metastases in cervical regions and 50 gy to non - involved cervical and supraclavicular lymph node regions . 
patients with rectal cancer ( n = 5 ) were treated in a prone position on a belly board by means of three 3d - conformal coplanar portals ( 0 , 90 , 270 ) with a total reference dose of 50.4 gy ( optional 5.4 gy boost to the primary tumor after 45 gy ) and a single dose of 1.8 gy ( once daily , 5 fractions / week )  . 
all patients were irradiated with a linear accelerator ( oncor or artiste ) from siemens ( erlangen , germany ) , using photons of 6 mv for imrt of head and neck cancers or 18 mv for 3d - crt of rectal cancers . 
the analysis of rtrelated parameters included assessment of blood volume contained within the 50% isodose line ( derived from volumetric computation of delineated blood vessels > 1 cm in diameter ) , body volumes surrounded by the 10 gy , 20 gy , strahlenther onkol ( 2020 ) 196 : 821833 30 gy , and 45 gy isodose lines ( v10isov45iso ) , and coverage of the ptv ( d80 , d90 )  . blood sampling for ifm analysis , blood samples were collected from a cubital vein in heparin - containing vials at 37 c and diluted 1 : 2 with prewarmed roswell park memorial institute ( rpmi ) 1640 medium ( biochrom ; berlin , germany ) for immediate processing . 
nonirradiated pbls from the same donor served as control . blood sample preparation for ifm and tem briey , blood samples in heparin tubes were diluted with 6 ml rpmi and incubated at 37 c . 
blood samples were layered on percol 400 and centrifuged at 1200 g for 20 m5 ml pbs was added to the resulting interphase and centrifuged at 300 g for 10 mthe separation yielded ~80% pbls , ~15% monocytes , and ~5% granulocytes . for ifm , pbls were xed in 100% methanol for 0.5 h and permeabilized in 100% acetone for 1 min at 20 c . after washing cells in pbs with 1% fetal calf serum for 1 10 min at room temperature , samples were incubated with 53bp1 antibody ( anti - 53bp1 , mouse monoclonal ; merck , darmstadt , germany ) followed by a secondary uorescent antibody ( alexafluor - 488 , invitrogen , karlsruhe , germany )  . 
samples were mounted using vectashield mounting medium ( vector laboratories , burlingame , ca , usa ) with dapi ( 40 , 6 - diamidino - 2 - phenylindole )  . 
ultrathin 70 nm slices were sectioned off the samples using a microtome ultracut uct ( leica , biel , switzerland ) , picked up on pioloform - coated nickel grids , and processed for immunogold labeling . 
afterwards , following rinsing , sections were incubated with different primary antibodies ( 53bp1 or pku70 [ anti - pku70 , rabbit polyclonal , pser5 ; abcam , cambridge , uk ] ) overnight at 4 c . 
the same primary antibodies used in uorescence microscopy were applied in combination with gold - labeled secondary antibodies for tem experiments in order to visualize pku70 and detect incomplete dna damage repair sites . 
when using gold - labeled secondary antibodies in the same ifm approach , this focus consists of two 53bp1 clusters , each one with a diameter of only 500 nm ( supplementary figure 8b ; red circles )  . in tem analysis , this focal area can be subdivided further into euchromatic and heterochromatic compartments ( supplementary figure 8c ) and thus allows for reliable detection and quantication of dna repair factors ( supplementary figure 8d ; pku70 , 10 nm , gold beads colored in red ; 53bp1 , 6 nm , colored in green ) and their localization within different chromatin compartments . after rinsing , goat secondary antibodies conjugated with 6 and 10 nm gold particles ( ems ) were applied to the sections on the grids and then incubated for 1.5 h at room temperature . 
for quantication , we identied pku70 dimers ( two 10 nm gold particles ) and 53bp1 bead clusters ( 6 nm ) visually at 48 , 00086 , 000 magnication and counted these in 50 randomly chosen nuclear sections . 824 statistical analysis a one - sided mannwhitney test was performed using the statistical software originpro ( version 8.5 , originlab corporation , northampton , usa ) to evaluate potential differences between data groups . 
the criterion for statistical signicance was p ( cid : 2 ) 0.05. the dispersion index test was used to determine the deviation of foci per cell distribution at the 0.5 h datapoint from poisson statistics to demonstrate thatin the setting of partial body irradiation to the head and neck or pelvic regiononly a proportion of pbls was exposed to irradiation [ 33 , 34 ]  . 
the test was performed with the software dose estimate , version 3.0 ( chilton , uk )  . results to characterize the ongoing dna repair process , pbls from nine individuals with head and neck or rectal cancer ( 5 patients received rct and 4 rt without chemotherapy ) were analyzed by ifm and tem . 
to show the inuence of chemotherapy on dsb formation , patients were further divided into those who received chemotherapy ( n = 5 ) and those who did not ( n = 4 )  . 
in total , 40 samples from patients with head and neck cancer and 45 from patients with rectal cancer ( three technical replicates per sample ) were analyzed . quantication of initial foci induction by ifm was completed on samples taken 0.5 h after the rst rt fraction . 53bp1 foci were not detected in 39 of 432 pbls ( ~10% ) from patients with head and neck cancer and in 50 of 517 ( ~10% ) from those with rectal cancer , conrming that partial - body irradiation causes limited pbl exposure ( table 2 )  . in contrast , no 53bp1 foci could be detected in 85% of the unirradiated pbls ( in total 2735 from 3222 cells ) taken before the rst fraction . to compare the appearance of 53bp1 foci among samples from different treatment types , we looked at the ptv size , radiation duration , and exposed blood volume from delineated blood vessels ( > 1 cm diameters ) encompassed by the 50% isodose line . 
a imrt was mandatory for patients with head and neck cancer , with a predened arrangement of seven coplanar beam angles ; b for patients with rectal cancer , through 3d - crt with three coplanar portals . 
this 53bp1 foci distribution did match the poisson statistic , as shown in table 2 ( supplementary table 3 )  . in addition , a linear doseresponse relationship up to 2.0 gy was demonstrated 0.5 h after homogeneous irradiation ( 0.54.0 gy ) , consistent with the literature [ 35 , 36 ]  . representative images of cells xed 0.5 h post irradiation with doses 0 , 1 , 2 , and 4 gy are shown in fig . 
on the contrary , the number of heterochromatic pku70 dimers initially rose from 0.10 pku70 / m3 ( 0.1 h post - ir ) to 0.80 pku70 / m3 ( 0.25 h post - ir ) and to 1.41 pku70 / m3 ( 0.5 h post - ir )  . 
subsequently , the pku70 dimers began to decrease in numbers 2.5 h after irradiation to 0.66 pku70 / m3 ( ~47% ) , to 0.32 pku70 / m3 ( ~23% ) after 8 h , and to 0.16 pku70 / m3 ( ~11% ) after 24 h . 
a the number of 53bp1 foci per pbl nucleus was counted before ( non - ir ) and 0.5 and 24 h after the rst dose fraction ( 1 ) as well as 24 h after a predened number of additional in vivo irradiation fractions ( 5 to 30 ) to the head and neck ( n = 4 ) or rectal ( n = 5 ) regions . 
data are presented as mean values of three technical replicates per patient standard error ; the background number of foci / cell ( control in week 1 before irradiation ) was subtracted from the data . 
4 visualization of pku70 ( 10 nm beads , pseudo - colored in red ) and 53bp1 ( 6 nm beads , pseudo - colored in green ) 0.5 h after 1 gy irradiation in a representative tem image . 
framed regions shown higher magnication in adjacent images matic pku70 dimers , with an increase from 0.10 53bp1 / m3 ( 0.1h post - rt ) to 0.80 53bp1 / m3 ( 0.25h post - ir ) and 1.41 53bp1 / m3 ( 0.5h post - ir )  . 
6a , b show representative tem micrographs . visualization of 10 nm ( pku70 dimers ) and 6 nm gold beads ( 53bp1 cluster ) was improved by overlaying with red and green circles , respectively . 
to do this , we quantied 53bp1 foci formation [ 13 , 14 ] in irradiated pbls , and found that not every 53bp1 focus equates to an unrepaired dsb . ifm is a well - established method to visualize and analyze dna repair proteins . 
quantication of pku70 dimers and 53bp1 clusters ( quantied in 50 nuclear sections ) in euchromatin ( red ) and heterochromatin ( green ) 0.5 h after irradiation with different doses ( a , b ) and at different timepoints after irradiation with 2 gy ( c , d )  . 
however , when lr gold resin - embedded pbl sections are investigated and quantied using tem , it is critical to always consider that only planar sections of the nucleus are examined and not the entire cell nucleus . 
to gain greater insight into the number of gold - labeled repair proteins in the entire nucleus , the labeling in 50 - nuclei sections per dose or repair timepoint was quantied . 
additionally , nonhomogeneously distributed pku70 dimers and 53bp1 clusters in the cell nucleus over the number of nuclei sections was captured as reliably as possible by counting all 10 nm ( pku70 ) and 6 nm ( 53bp1 ) gold beads . 
the primary antibodies and the uorochrome - coupled secondary antibodies penetrated the xed cells and cell nuclei due to the permeabilization step ( acetone , 1 min at 20 c )  . 
in ifm , the degree to which cell structures were preserved after this chemical treatment was not detectable 830 strahlenther onkol ( 2020 ) 196 : 821833 pbls , which are often used for biological dosimetry [ 39 ] and for determination of individual radiosensitivity [ 40 , 41 ] , do not go through the cell cycle but remain in the g0 phase . 
several studies have shown that pbls sometimes undergo apoptosis 1224 h after irradiation , which is characterized by signicant chromatin condensation [ 35 , 42 ]  . this apoptotic chromatin condensation within human pbls may prevent decomposition of residual dna repair foci , which were observed in pbls 24 h after irradiation [ 43 ]  . 
moreover , pulsedeld gel electrophoresis and confocal laser microscopy experiments have shown that in normal human broblasts , repair of existing dsbs does not correspond with the counted 53bp1 foci [ 44 ]  . 
3a , after an increasing number of applied fractions , is probably due to a mixture of newly induced dsbs per daily fraction and the generation of persistent chromatin changes after unnished or defective dsb repairs . 
however , as an overall ( but not linear ) increase in the number of 53bp1 foci was observed , especially 24 h postir between the rst ( 1 ) and last ( 25 or 30 ) fraction , it is reasonable to assume that at this timepoint , accumulation of persisting 53bp1 foci was signicantly involved , whereas during the previous 24 h , more repairable dsbs were eliminated . 
a continuous but not smooth increase in 53bp1 foci was detected throughout the entire treatment periodpossibly due to a mixing of the opposing events of dsb induction , their repair , and the appearance of residual 53bp1 foci within a period of 24 h . 
at the time of blood sampling , these may have crossed the irradiation eld only once or even not at all , which is why , accordingly , no or only initial 53bp1 foci were detected in these pbls . 
6 visualization of pku70 ( 10 nm beads , pseudo - colored in red ) and 53bp1 ( 6 nm beads , pseudo - colored in green ) in peripheral blood lymphocytes ( pbls ) 24 h after rst rt ( a ) and rct ( b ) by means of the dapi signal . 
permeabilization was not necessary , as antigens were found freely accessible near the surface . all cell structures ( membranes , mitochondria , etc . ) were perfectly visible in tem and optimally preserved . strahlenther onkol ( 2020 ) 196 : 821833 fig . 
as such , occurrence and repair of dna damage in the pbls of patients is determined by a range of inuencing factors that are in turn inuenced by external parameters ( different techniques for application of radiation , isodose volumes , dose applied , duration of radiation application , and concomitant chemotherapy ) and internal inuencing factors ( immune system , individual capacity for dna repair ) [ 45 , 46 ]  . 
3b , we show higher 53bp1 foci levels for all patients who received rct , independent of the collective . the cytotoxic effects of chemotherapy drugs have been described at length in the literature , whereby their objective is to induce dna damage and activate apoptosis [ 47 , 48 ]  . by using the higher resolution of tem in combination with the immunogold labeling of pku70 and 53bp1 within the intact nuclear cell ultrastructure , we were able to detect a higher number of pku70 dimers in the euchromatin and heterochromatin of pbls in rct patients than in those of patients after a single rt 24 h post - ir . 
thus , the number of dsbs in pbls was not signicantly inuenced by the irradiation technique ( imrt or 3d - crt ) or the size of the irradiation eld . 
this , however , could be due to the possibility that effects induced by imrt , in which a smaller ptv is irradiated over a longer period of time , counterbalance those induced in 3d - crt , in which a larger volume is irradiated over a shorter time period . based on these data , we propose that persisting dsbs ( pku70 dimers ) represent more severe damage induced by rct ( 1 , 2 , or more pku70 dimers representing multiple dna lesions )  . 
a large - scale study is necessary to be able to better study the cause of this observation , in particular 832 strahlenther onkol ( 2020 ) 196 : 821833 to clarify how the concomitant chemotherapy prolongs the dwell time of existing dsbs in pbls that are located in the g0 phase of the cell cycle . 
in addition , as persistent dsbs were detectable only at certain times > 0.5 h after irradiation and always at the edge of heterochromatic domains , we suspect that cellular processes , such as the opening of densely packed heterochromatic regions containing one or more dsbs , delay repair . 
the funders had no role in study design , data collection and analysis , decision to publish , or preparation of the manuscript . author contribution cer and yl conceived and designed the experiments . 
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februar 2020 der / die autor ( en ) 2020 hintergrund und ziele in der therapie des metastasieren nichtkleinzelligen lungenkarzinoms ( nsclc ) werden neben der klassischen chemotherapie und den kinaseinhibitoren auch immuncheckpoint - inhibitoren , wie der pd - 1inhibitor pembrolizumab , eingesetzt . 
bei der kombination von pd - 1 / pd - l1 - inhibitoren und strahlentherapie gibt es aus der prklinischen forschung gute daten hinsichtlich der induktion von lokalen und abskopalen antitumor - immunantworten ( zusammengefasst in [ 2 ] )  . 
es soll die hypothese berprft werden , ob durch die immunologischen vorgnge in der bestrahlten metastase die systemische immunreaktion und damit das therapieansprechen der patienten verbessert werden kann . originalpublikation bauml jm , mick r , ciunci c , aggarwal c et al ( 2019 ) pembrolizumab after completion of locally ablative therapy for oligometastatic non - small cell lung cancer : a phase 2 trial . 
2019.1449. theelen wsme , peulen hmu , lalezari f , van der noort v ( 2019 ) effect of pembrolizumab after stereotactic body radiotherapy vs pembrolizumab alone on tumor response in patients with advanced non - small cell lung cancer : results of the pembro - rt phase 2 randomized clinical trial . 
primrer endpunkt der studie war das progressionsfreie berleben ( pfs ) , gemessen zum einen nach beginn der lokal ablativen therapie und zum anderen nach beginn der therapie mit pembrolizumab . 
lebensqualitt wurde mit dem factl - fragebogen bestimmt . ergebnisse ( bauml et al . ) zwischen februar 2015 und september 2017 wurden 51 patienten in die studie eingeschlossen , von denen 45 mit pembrolizumab behandelt wurden . die analysen der studie beziehen sich nur auf die 45 patienten , die pembrolizumab erhielten . 
pembrolizumab scheint das pfs nach lokal ablativer therapie beim nsclc zu verbessern , ohne die lebensqualitt einzuschrnken . 290 strahlenther onkol ( 2020 ) 196 : 289292 patienten und methoden ( theelen et al . ) in der der multizentrischen pembro - rt - studie wurden patienten mit metastasiertem bronchialkarzinom nach progress auf erstlinien - chemotherapie behandelt . 
er erfolgte eine randomisation auf entweder pembrolizumab - monotherapie ( 200 mg absolutdosis , q21d ) oder die kombination aus pembrolizumab und stereotaktischer bestrahlung einer einzelnen metastase mit 3 8 gy . 
studienhypothese war die verbesserung der orr nach 12 wochen von 20 auf 50 % mit p < 0 , 10 . ergebnisse ( theelen et al . ) insgesamt wurden 76 patienten randomisiert , im kontrollarm 40 patienten und im prfarm ( kombination mit bestrahlung ) 36 patienten . 
das mediane progressionsfreie berleben lag im kontrollarm bei 1 , 9 monaten und im prfarm bei 6 , 6 monaten ( hazardratio 0 , 71 ; 95 % ci 0 , 421 , 18 ; p = 0 , 19 )  . 
die ergebnisse legen dennoch die durchfhrung einer greren studie nahe . kommentar pembrolizumab ist zur behandlung des metastasierten bronchialkarzinoms zugelassen , wobei die zulassung an das vorhandensein des prdiktiven parameters pd - l1 gebunden ist . 
so steht patienten im metastasierten stadium neben der klassischen chemotherapie und den kinase - inhibitoren nun mit den pd - 1 - inhibitoren eine neue therapieoption zur verfgung . bei patienten mit therapieansprechen auf die initiale chemotherapie und oligometastasierung , in dieser studie deniert mit bis zu 3 metastasen , konnte krzlich auch eine signikante verbesserung des berlebens durch konsequente lokaltherapie gezeigt werden [ 1 ]  . 
leider werden in der publikation nur die gesamten vortherapien der patienten angegeben und nicht die aktuell angewendeten lokaltherapie - verfahren , sodass nicht unterschieden werden kann , wie viele patienten strahlentherapeutisch und wie viele chirurgisch lokal behandelt wurden . mit der kombination aus lokaltherapie und pembrolizumab wurde aber ein beachtliches pfs von 19 , 1 monaten erreicht , das der historischen kontrolle mit alleiniger bestrahlung weit berlegen war . 
auch wenn bisher nur daten aus phase - ii - studien vorliegen , scheint eine intensive lokaltherapie bei patienten mit oligometastasierung nicht nur in kombination mit chemotherapie , sondern auch in kombination mit immuntherapie ein hoch effektives therapieverfahren zu sein . hinsichtlich strahlentherapie und pd - 1 - inhibitoren gibt es zahlreiche prklinische daten , dass sich beide verfahren nicht nur wie in obiger studie gut kombinieren lassen , sondern auch gegenseitig in ihrer wirkung verstrken . 
es ist lange bekannt , dass strahlentherapie neben den klassischen zelltod ber die akkumulation von dna - schden auch den tumorzell - phnotyp und das tumormikromilieu verndert [ 2 ]  . 
so konnte in prklinischen experimenten bei kombination von strahlentherapie und pd - 1 / pd - l1 - inhibitoren neben der lokalen wirkung auch eine verstrkung der systemischen wirkung erreicht werden . in der studie von theelen et al . 
in dieser studie wurde eine metastase mit 3 8 gy bestrahlt und innerhalb von 7 tagen die therapie mit pembrolizumab eingeleitet . ob eine andere sequenz der behandlungen oder eine andere bestrahlungsdosis mglicherweise besser zur induktion immunologischer effekte geeignet ist , konnte bisher nicht geklrt werden . 
in der studie konnte die ansprechrate auf pembrolizumab von 18 auf 36 % verdoppelt werden , jedoch nicht statistisch signikant ( p = 0 , 07 )  . die fehlende statistische signikanz ist bei der zugrundeliegenden fallzahlkalkulation mit der annahme einer verbesserung von 20 auf 50 % kalkuliert , mit p < 0 , 10 nicht verwunderlich . 
dennoch kann das ergebnis dieser phase - ii - studie als deutliches signal gewertet werden , dass eine lokale bestrahlung auch systemische effekte bewirken kann , die die wirksamkeit einer immuntherapie verstrken . 
da pdl1 der wichtigste prdiktive parameter fr die therapie mit pd - 1 - inhibitoren ist , ist es nicht verwunderlich , dass von der bestrahlung insbesondere patienten mit primr pd - l1negativen tumoren protieren . 
auch gilt es zu bedenken , dass zum testen des pd - l1 - status biopsien nach initialer bestrahlung genommen werden sollten , da diese stark die expression von pd - l1 beeinussen kann [ 6 ]  . trotz dieser beeindruckenden daten zur systemischen wirkung der lokalen bestrahlung muss beachtet werden , dass beim diesjhrigen asco eine fast identische phaseii - studie bei kopf - hals - tumoren diskutiert wurde , die keine systemische wirkung der lokalen strahlentherapie nachweisen konnte [ 7 ]  . 
in zehn deutschen studienzentren wird derzeit im rahmen der importance - studie ein hnliches konzept kombination von fraktionierter bestrahlung und pembrolizumab in der erstlinientherapie von metastasierten kopf - hals - tumoren untersucht . 
auf das ergebnis darf man gespannt sein . fazit bei patienten mit oligometastasierung eines nsclc scheint die intensive lokaltherapie nicht nur in kombination mit chemotherapie , sondern auch mit immuntherapie sehr gute ergebnisse zu erzielen . eine erste phase - ii - studie liefert hinweise auf systemische effekte einer lokalen strahlentherapie , die das therapieansprechen auf pd - 1 - inhibitoren verbessern knnten . markus hecht , udo s . 
hecht hat an advisory boards von msd , merck serono und bms teilgenommen , forschungsfrderung von msd , astrazeneca und novartis und reiseuntersttzung von merck serono , msd und teva erhalten . 
fietkau hat an advisory boards von merck serono , astrazeneca , msd , novocure , brainlab , fresenius kabi und bms teilgenommen und forschungsfrderung von merck serono , astrazeneca , msd , novocure , brainlab , fresenius kabi , sennewald und bms erhalten . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
gomez dr , tang c , zhang j , blumenschein gr jr . , hernandez m , lee jj , ye r , palma da , louie av , camidge dr , doebele rc , skoulidis f , gaspar le , welsh jw , gibbons dl , karam ja , kavanagh bd , tsao as , sepesi b , swisher sg , heymach jv ( 2019 ) local consolidative therapy vs . 
maintenance therapy or observation for patients with oligometastatic non - small - cell lung cancer : long - term results of a multi - institutional , phase ii , randomized study . 
derer a , frey b , fietkau r , gaipl us ( 2015 ) immune - modulating properties of ionizing radiation : rationale for the treatment of cancer by combination radiotherapy and immune checkpoint inhibitors . 
hecht m , buttner - herold m , erlenbach - wunsch k , haderlein m , croner r , grutzmann r , hartmann a , fietkau r , distel lv ( 2016 ) pd - l1 is upregulated by radiochemotherapy in rectal adenocarcinoma patients and associated with a favourable prognosis . 
lim yj , koh j , kim s , jeon sr , chie ek , kim k , kang gh , han sw , kim ty , jeong sy , park kj , wu hg ( 2017 ) chemoradiation - induced alteration of programmed death - ligand 1 and cd8 ( + ) tumor - inltrating lymphocytes identied patients with poor prognosis in rectal cancer : a matched comparison analysis . 
mcbride sm , sherman ej , tsai cj , baxi ss , aghalar j , eng j , zhi wi , mcfarland dc , michel ls , spielsinger d , zhang z , flynn j , dunn l , ho al , riaz n , pster dg , lee ny ( 2018 ) a phase ii randomized trial of nivolumab with stereotactic body radiotherapy ( sbrt ) versus nivolumab alone in metastatic ( m1 ) head and neck squamous cell carcinoma ( hnscc )  . 
we assessed freedom from biochemical relapse ( ffbf ) , 5 - year biochemical recurrence - free survival ( 5 - brfs ) , distant metastasis - free survival ( 5 - dmfs ) , and cancer - specic survival ( 5 - css ) as well as acute and late genitourinary ( gu ) and gastrointestinal ( gi ) toxicity . results among our cohort , 11.4% were low - risk , 50% intermediate - risk , and 38.6% high - risk patients according to the damico criteria . 
no toxicity > grade 3 was observed . conclusion risk - adapted dose - escalated igrt with helical tomotherapy of up to 84 gy is a feasible and well - tolerable treatment scheme with promising oncological results . keywords prostate cancer primary radiation therapy dose - escalation image - guided radiation therapy tomotherapy introduction primary radiation therapy ( rt ) is an established treatment option for patients with localized prostate cancer . 
dose intensication to a total dose of 78 gy and beyond has been shown to improve biochemical recurrence - free survival ( brfs ) , particularly among intermediateand high - risk patients [ 24 ]  . 
this came along with the introduction of image - guided rt ( igrt ) conducted by means of portal imaging or online cts ( cone beam or megavoltage ct )  . 
the tomotherapy treatment system provides online megavoltage cts ( mvct ) of high 230 strahlenther onkol ( 2020 ) 196 : 229242 resolution and contrast , which enable identication of the prostate and surrounding soft tissue and registration on this basis . 
previous publications report on strategies for improving tumor control while maintaining or reducing toxicity levels by applying escalated doses only to subvolumes via a simultaneous integrated boost ( sib ) technique to the prostate alone [ 9 ] or intraprostatic lesions [ 12 ]  . in order to further improve the therapeutic ratio , at our institution we have developed a treatment scheme which combines risk - adapted dose escalation to conned volumes with daily igrt using helical tomotherapy . methods patient selection from the introduction of our new treatment scheme in february 2009 until november 2010 , 88 consecutive patients with localized prostate cancer and no clinical signs of lymph node metastases received primary igrt using helical tomotherapy . 
patients were categorized as low - , intermediate - , or high - risk according to the damico risk classication system [ 16 ] , with the intermediate - risk group further divided into a favorable group and an unfavorable group on the basis of t - stage , gleason - score , and initial prostate - specic antigen ( psa ) level , which other authors have also proposed [ 17 ]  . 
this retrospective study was approved by the ethics committee of our institution . treatment planning ct scan and radiation therapy were administered to patients in supine position with a comfortably lled bladder and a voided rectudaily igrt was carried out using the integrated mvct of the tomotherapy system ( accuray , sunnyvale , ca , usa )  . 
the planning target volume ( ptv ) was created by expanding the clinical target volume ( ctv ) by 5 mm in all directions , except for the dorsal direction where it was reduced to 3 mthe rectum and bladder were always excluded from ctvs . for low - risk patients , the ctv was dened as the prostate alone . 
for favorable intermediate - risk patients , ctv1 included a margin of 5 mm around the prostate to include periprostatic tissue deemed to carry a substantial risk of microscopic tumor spread . 
adt was prescribed at the discretion of the referring urologist . statistical analysis we retrospectively analyzed our data with the aim of calculating freedom from biochemical failure ( ffbf ) , biochemstrahlenther onkol ( 2020 ) 196 : 229242 ical recurrence - free survival ( brfs ) , distant metastasis - free survival ( dmfs ) , and cancer - specic survival ( css ) , as well as acute and late genitourinary ( gu ) and gastrointestinal ( gi ) toxicity rates . for fbff , brfs , dmfs , and css , the time was calculated from the rst day of radiotherapy until the respective event or last contact . 
for dmfs , events were either diagnosis of distant metastasis of prostate cancer ( by ct , mri , pet , or skeletal scintigraphy ) or death from any cause , whichever occurred rst . 
for css , only deaths caused by the progression of prostate cancer were considered events . the kaplanmeier method was applied to calculate actuarial ffbf , brfs , dmfs , and css . 
in addition , gu toxicity and associated quality of life ( qol ) were quantied using the international prostate symptom score ( ipss )  . patients were assessed for baseline symptoms on their rst visit before beginning rt . 
the time of event and followup were calculated from the date of the rst fraction . continuous data are presented as means ( standard deviation )  . results patient characteristics table 1 provides a detailed overview of the distribution of patient characteristics including pretreatment psa , damico risk classication , gleason score ( gs ) , t classication , age , pelvic nodal irradiation , dose to prostate ( ctv ) , and application of adt . 
1 , 2 , 3 and 4 show the respective kaplanmeier curves . distant metastasis - free survival distant metastases occurred in 4 patients : none in the lowrisk group , 1 in the intermediate - risk group , and 3 in the high - risk group . 
there were no deaths among patients in the low - risk group , 5 deaths in the intermediate - risk group ( of which 1 was related to prostate cancer ) , and 10 deaths in the high - risk group ( of which 3 were related to prostate cancer )  . 
7 and 8 show the kaplanmeier curves for css for each of the applied stratications . cox regression analysis did not reveal any signicant factors inuencing outcome . baseline and acute toxicity a detailed overview of baseline and acute gu and gi toxicity is provided in tables 2 and 3 . 
all other cases of grade 2 gu toxicity were by denition the result of the prescription of either tamsulosin or trospium chloride . there was 1 ( 1.1% ) instance of acute grade 3 gu toxicity in a patient who had already reported strong gu symptoms at baseline ( ipss = 33 ) and underwent a transurethral resection of the prostate ( tur - p ) shortly after rt . with regard to gi toxicity , at baseline , only 1 ( 1.1% ) patient reported grade 1 symptoms . 
as with gu toxicity , there was a shift towards higher grades of acute toxicity , although this was less pronounced , with 11 ( 12.5% ) patients experiencing grade 2 gi toxicity . 
there were no cases of acute gi toxicity of grade 3 or higher . late toxicity a detailed overview of late gu and gi toxicity is provided in tables 2 and 3 . 
the highest cumulative late gu toxicities we observed over the entire course of follow - up were grade 2 and 3 toxicity in 17 ( 19.3% ) and 4 ( 4.5% ) patients , respectively . 
of the patients experiencing grade 3 toxicity , 3 required urethrotomy with no resulting complications and 1 a tur - p and subsequently a suprapubic catheter , which was still in use at the time of the last follow - up . the last data on late gu toxicity grades available for all patients showed a decreasing trend , with 12 patients ( 13.6% ) experiencing grade 2 and no patients experiencing grade 3 toxicity . 
the highest level of overall toxicity for the respective categories was reached during the acute phase , with the exception of urinary incontinence , which reached its peak during the late phase , suggesting a different time course for the onset and amelioration of this toxicity . a similar pattern was observed for late gi toxicity . 
after reaching their peak during the acute phase , toxicity levels generally shifted back towards baseline over the course of time , particularly grade 2 and 3 toxicities , which , with the exception of 4 ( 4.5% ) patients with grade 2 fecal incontinence , did not exceed levels of 1.1%. 
as with urinary incontinence , fecal incontinence occurred and reached peak levels during the late phase , as opposed to other toxicities which tended to shift back towards baseline levels nearing the last follow - up . 
levels remained stable over the course of follow - up , with 4 ( 4.5% ) patients reporting grade 2 gi toxicity at last follow - up and no further incidence of grade 3 toxicity . 
1 kaplanmeier curves for freedom from biochemical failure according to damico risk group ; patients censored at time of last contact or death by any cause ( months ) fig . 
2 kaplanmeier curves for freedom from biochemical failure according to favorable and unfavorable intermediate - risk group ; patients censored at time of last contact or death by any cause ( months ) 234 strahlenther onkol ( 2020 ) 196 : 229242 fig . 
4 kaplanmeier curves for biochemical recurrence - free survival according to favorable and unfavorable intermediate - risk group ; patients censored at time of last contact ( months ) strahlenther onkol ( 2020 ) 196 : 229242 fig . 
6 kaplanmeier curves for distant metastasis - free survival according to favorable and unfavorable intermediate - risk group ; patients censored at time of last contact ( months ) 236 strahlenther onkol ( 2020 ) 196 : 229242 fig . 
7 kaplanmeier curves for cancer - specic survival according to damico risk group ; patients censored at time of last contact or death by cause other than prostate cancer ( months ) fig . 
 [ 6 ] report actuarial 5 - year psa relapse - free survival rates of 98% , 85% , and 70% for low - , intermediate - , and high - risk patients , respectively . 
 [ 9 ] included data of a subcohort of 233 patients treated with imrt , 160 of whom received a dose of 78 gy and 73 of whom received a dose of 73.8 gy to periprostatic tissue and a simultaneous integrated boost of 82 gy to the prostatethe latter being similar to our scheme . 
our data are in line with these ndings for lowand intermediate - risk patients with 5 - year css rates of 100% and 97.4% , and only slightly inferior for high - risk patients with a rate of 89.8%. in summary , we were able to produce comparable results to the oncological endpoints reported by the abovementioned studies . 
this comparatively low outcome is possibly due to a disproportionately high number of deaths unrelated to prostate cancer which occurred in this subcohort . keeping the limitations of a retrospective analysis of a relatively small cohort in mind , our results seem to indicate that the subdivision of intermediate - risk patients into favorable and unfavorable groups with differing cumulative doses as practiced at our institution is viable . 
this altogether seems to suggest that both limiting the dose to 80 gy for the favorable subcohort and escalating it to 84 gy for the unfavorable subcohort is justied . while it is not disputed for high - risk patients , it is a matter of controversy whether or not the combination of both dose escalation and adt provides benets in terms of outcome for intermediate - risk patients . 
the prospective randomized dart01 / 05 gicor trial [ 20 ] ( n = 355 ) showed a benet for long - term adt in addition to rt with 78 gy only for high - risk patients , not for intermediate - risk patients . 
the eortc trial 22991 [ 21 ] ( n = 819 ) tested shortterm adt in addition to rt to 70 , 74 , or 78 gy for intermediateand high - risk patients and showed a benet in favor of adt for both risk groups ; however , no statistically signicant difference by dose was found . 
 [ 13 ] the latter holding particular validity as a large prospective randomized trialdemonstrated outcomes comparable to ours without the addition of adt . in our cohort , 38 of 44 ( 86.4% ) intermediate - risk patients table 5 genitourinary ( gu ) toxicity reported in previous imrt dose - escalation studies study dose in gy acute gu toxicity by grade ( in % ) late gu toxicity by grade ( in % ) cahlon et al . 
when intraprostatic lesions were detectable ( 118 patients ) an additional sib up to 8182 gy was delivered to these bcumulative rate of toxicity > grade 2 provided csubcohort of 233 patients treated with imrt , acute toxicity according rtog criteria , late toxicity according to fc - rtog - lent criteria , cumulative rate of grade 24 toxicity provided dpatients from dose - escalated arm 240 strahlenther onkol ( 2020 ) 196 : 229242 table 6 gastrointestinal ( gi ) toxicity reported in previous imrt dose - escalation studies study dose in gy acute gi toxicity by grade ( in % ) late gi toxicity by grade ( in % ) cahlon et al . 
when intraprostatic lesions were detectable ( 118 patients ) an additional simultaneous integrated boost ( sib ) up to 8182 gy was delivered to these bcumulative rate of toxicity > grade 2 provided csubcohort of 233 patients treated with intensity - modulated radiation therapy , acute toxicity according rtog criteria , late toxicity according to fc - rtog - lent criteria , cumulative rate of grade 23 for late toxicity provided dpatients from dose - escalated arm were treated with adt , which , bearing in mind the wide range of side effects and negative impact on qol [ 22 ] , may be considered overtreatment . in terms of toxicity , this retrospective study demonstrated results similar to comparable dose - escalation studies . 
in our study , 39.8% of patients experienced grade 2 , and 1.1% experienced grade 3 acute gu toxicity , which positions our results within the range of the outcomes of the aforementioned studies . with regard to acute gi toxicity , cahlon et al . 
 [ 9 ] demonstrate that acute gi toxicity , which used to be an eminent problem during primary rt of prostate cancer , can be reliably reduced to low , tolerable levels through the application of modern radiation techniquesin our case without the use of ducials to doses as high as 84 gy . for late gu toxicity , cahlon et al . 
in the case of our cohort , we observed grade 2 late gi toxicity in 3.4% and grade 3 late gi toxicity in 1.1% of patientsresults which compare favorably with the studies presented above . a detailed overview of acute and late gu and gi toxicity rates observed by previous studies is provided in tables 5 and 6 . in addition to cumulative late toxicity , ghadjar et al . 
at last follow - up ( median follow - up 5 years , range 37 years ) , they observed rates of 10% and < 1% of grade 2 and 3 late gu toxicity , respectively . 
at last follow - up , we observed a similar incidence , with 13.6% of patients experiencing grade 2 late gu toxicity and no cases of grade 3 late gu toxicity . it therefore seems reasonable to conclude that , irrespective of the occurrence of acute gu toxicity , low and welltolerable levels of toxicity were achieved over the longer course . 
this is also reected by the patient - reported ipss and ipss - qol scores of our patients , which showed a trend towards improvement between the time of initial evaluation and the last follow - up . 
 [ 8 ] , who reported no signicant worsening of ipss and ipss - qol among their cohort . in summary , the rates of toxicity in our study compare well to previously published studies . 
however , levels of acute grade 2 gu toxicity and late grade 3 gu toxicity do slightly stand out against an otherwise excellent outcome . strahlenther onkol ( 2020 ) 196 : 229242 since our study was not conducted as a prospective trial , there was no protocol which dened how and when symptoms under rt should be treated . 
at our institution we have a policy of treating acute gu toxicity early , which in our experience improves both quality of life and compliance . this is reected by the fact that of all 33 patients treated for gu toxicity with either tamsulosin or trospium chloride , 10 patients ( 30.3% ) received their prescription within the rst 15 days and a total of 21 patients ( 63.6% ) received prescriptions within the rst 22 days after the beginning of rt . the median duration of rt was 60 days . 
regardless , we objectively categorized acute gu toxicity as grade 2 in accordance with ctcae denitions whenever a prescription was noted in the patients le . a possible predictor of late gu toxicity has been identied by ghadjar et al . 
while late gu toxicity occurred at an acceptable rate within our cohort , we hope to further decrease its incidence by implementing the ndings of ghadjar et al . [ 24 ] in our planning standards . in addition , a further reduction of toxicity levels can likely be achieved by contracting the dose - escalated volume to intraprostatic lesions as identied by mri or psma - pet scans . 
 [ 12 ] demonstrated such an approach to be viable and we are planning to implement this strategy in our treatment scheme . conclusion using a risk - adapted scheme of dose - escalated igrt , we were able to achieve rates of ffbf , bfrs , dmfs , and css comparable to previous studies . 
the aim of this retrospective study was to evaluate the oncological outcome and pattern of recurrence in patients treated with stereotactic body radiation therapy ( sbrt ) to lymph node metastases . methods in this multi - institutional analysis , patients with a maximum of ve lymph node metastases from pca treated with sbrt were included . 
primary endpoints of the analysis were local control ( lc ) , out - of - eld nodal progression - free survival ( npfs ) , overall progression - free survival ( pfs ) , and overall survival ( os )  . results 109 patients and 155 lymph node metastases were evaluated . 
in - eld progression of disease was observed in 11 ( 7% ) lesions . oneand 3 - year npfs was 59% and 29% , and median npfs was 15 months . 
prospective trials are necessary to better select patients who benet most from this ablative focal treatment and better dene the recurrence patterns . keywords prostate cancer stereotactic body radiotherapy oligometastasis metastases - directed therapies radiotherapy rezidivmuster nach stereotaktischer radiotherapie beim oligometastasierten prostatakarzinom : eine multiinstitutionelle analyse zusammenfassung zielsetzung fr patienten mit oligometastasierten , oligorezidivierten oder oligoprogressiven lymphknotenmetastasen bei prostatakarzinom ( pca ) stellt die zielgerichtete behandlung mittels extrakranieller krperstereotaxie ( sbrt ) eine neue therapiestrategie dar . 
ziel dieser retrospektiven studie war die analyse des onkologischen outcomes sowie eine rezidivmusteranalyse nach sbrt von lymphknotenmetastasen beim prostatakarzinom . ( cid : 2 ) filippo alongi prof.lippoalongi@gmail.com 3 radiation oncology department , university hospital , lmu munich , munich , germany 1 radiation oncology , irccs sacro cuore don calabria 4 university of brescia , brescia , italy hospital , negrar - verona , italy 2 radiotherapy and radiosurgery department , humanitas clinical and research hospital , milan - rozzano , italy 5 radiation oncology department , irccs sacro cuore don calabria hospital , cancer care center , via don sempreboni 5 , 37034 verona , negrar , italy 214 strahlenther onkol ( 2020 ) 196 : 213221 methoden in dieser multizentrischen analyse wurden patienten mit maximal fnf lymphknotenmetastasen eines pca eingeschlossen , welche mit sbrt behandelt wurden . 
endpunkte der analyse waren die lokale kontrolle ( lc ) , das progressionsfreie berleben auerhalb des bestrahlungsfelds ( npfs ) , das progressionsfreie gesamtberleben ( pfs ) und das gesamtberleben ( os )  . ergebnisse es wurden 155 lymphknotenmetastasen von 109 patienten mit einer sbrt behandelt . 
insgesamt wurde eine bestrahlungsdosis von 25 bis 48 gy in 47 fraktionen appliziert ; die mittlere bed1 , 5 gy war 198 gy ( spanne 108 , 3432 gy )  . 
die mediane zeit bis zur einleitung einer systemischen behandlung nach sbrt betrug 7 , 8 monate ( spanne 1 , 754 , 8 monate )  . schlussfolgerung bei der behandlung von lymphknotenmetastasen des pca ist die sbrt eine wirksame und gut vertrgliche therapieoption . 
prospektive studien sind notwendig , um dieses vielversprechende therapiekonzept genauer zu untersuchen . schlsselwrter prostatakarzinom extrakranielle krperstereotaxie oligometastasierung metastasengerichtete therapien strahlentherapie to improve time - to - progression and delay the onset of systemic therapies [ 13 , 14 ]  . the aim of the present study was to retrospectively evaluate the efcacy of sbrt in the treatment of lymph node metastases in a population of patients affected by oligometastatic pca . 
patient selection was based on the following inclusion criteria : ( cid : 2 ) histological diagnosis of adenocarcinoma of prostate ; ( cid : 2 ) performance status ecog ( eastern cooperative oncology group criteria ) ( cid : 2 ) 2 ; ( cid : 2 ) controlled primary tumor diagnosed with choline / psma ( cid : 2 ) ( cid : 2 ) 5 lymph node metastases at the time of treatment diagnosed with pet - tc ; ( cid : 2 ) serum testosterone level ( cid : 2 ) 50 ng / ml during adt ; ( cid : 2 ) no other active sites of distant metastases diagnosed with pet ; pet - tc ; ( cid : 2 ) administration of sbrt with a biological effective dose > 100 gy , using alpha / beta ratio of 1.5 gy ; ( cid : 2 ) minimum follow - up of 6 months after sbrt . introduction lymph node metastases are a common presentation of prostate cancer ( pca ) [ 1 ]  . 
in case of nodal relapse , the standard treatment approach includes androgen deprivation therapy ( adt ) in hormone - nave patients or systemic therapies in castration - resistant disease . 
despite its demonstrated efcacy , patients treated with adt only will relapse at a certain point , developing a castration - resistant disease during pca progression [ 2 ]  . pca metastases are characterized by a high intratumoral heterogeneity ; therefore , it is conceivable that different cells of the same disease may present a different sensitivity to hormonal deprivation and therefore develop a relapse at different timepoints [ 3 ]  . 
this concept presents clinically as a limited spread of disease , a so - called oligometastatic state , in which the administration of local ablative treatments could have a strong rationale [ 36 ]  . 
several studies on the use of sbrt for the treatment of oligometastatic lymph nodes from pca reported 2 - year local control rates ranging from 84 to 92.8% , with limited side effects [ 1012 , 26 ]  . 
it was also shown that metastasesdirected therapies ( mdt ) , including sbrt , might be able strahlenther onkol ( 2020 ) 196 : 213221 exclusion criteria were : ( cid : 2 ) use of new androgen receptor - targeted agents ( such as abiraterone or enzalutamide ) or chemotherapy before or during the sbrt course ; ( cid : 2 ) patients already castration resistant at the time of detection of metastases . patients could have received adt previous to or during sbrt . 
the study was conducted in accordance with good clinical practice guidelines and with the ethical principles of the declaration of helsinki . treatment characteristics all patients were simulated in a supine position using personalized immobilization devices , including combifix ( civco radiotherapy , ia , us ) , with or without a body thermoplastic mask , based on the site of the involved lymph node to treat . 
the clinical target volume ( ctv ) was equal to gross tumor volume ( gtv ) and an isotropic margin of 5 mm was added to the ctv to obtain the planning target volume ( ptv )  . 
details on technical aspects of the adopted radiation therapy technique were described in a previous experience of several authors of the same group [ 15 ] and are hereafter briey described . prescription dose was dened as the mean dose to the ptv , aiming to cover the ptv with 95% of the prescribed dose . 
if organs at risk tolerance doses did not allow that coverage , the prescription was then applied to the mean dose to the ctv , aiming to cover the ctv with 95% of the prescribed dose and the ptv with 80% of the same prescribed dose . 
maximum dose was to be kept below 107% of the prescription . the patients position was veried , and corrected if necessary , using daily cone - beam ct imaging before each treatment session . follow - up , denitions , and statistics oligometastatic status was dened as follows : oligorecurrence was the occurrence of lymph node metastases in hormone - nave patients ; oligoprogression was the occurrence of lymph node metastases during adt . 
progression after sbrt was dened as the increase in psa value and / or by the occurrence of active sites of disease in choline / psma - pet . in case of further oligoprogression after mdt , a new course of sbrt was usually proposed in case of ( cid : 2 ) 3 new lesions outside the previous eld of irradiation . 
local control was analyzed at the site of oligometastatic disease treated with sbrt , dened as the time from the beginning of sbrt to the progression of the treated metastases or last follow - up and identied by an increase in psa and metabolic uptake in choline / psma - pet . 
univariate analysis was performed with the log - rank test to correlate survival with the following independent variables : number of treated lymph nodes , age , sex , ps ( ecog ) , gleason score at diagnosis , primary treatment to the prostate , psa value before rt , lesion diameter , gtv volume , total prescribed dose , dose per fraction , use of concomitant adt , and sensitivity to hormone therapies ( castration - sensitive versus castration - resistant disease )  . 
the threshold of lymph node size related to sbrt response and survival was determined with the roc curve method , calculating the highest product of ( sensibility * specicity )  . 
surgery was the treatment of choice for the primary tumor in 76% of cases , while it was radical radiotherapy in 11% of patients and hifu in 13% of lesion diameter ( mm ) range ( mm ) ( cid : 2 ) 20 mm > 20 mm lymphnode site pelvic extrapelvic sbrt regimen median dose ( range ) median dose / fractions ( range ) median bed ( / = 1.5 ) concomitant adt 345 117 ( 75.5% ) 38 ( 24.5% ) 56 ( 70 ) 24 ( 30 ) 36 ( 2548 ) 7 ( 512 ) 198 ( 108.3432 ) 50 ( 45.8 ) 59 ( 54.2 ) sbrt stereotactic body radiotherapy , bed biological effective dose , adt androgen deprivation therapy cases . 
a total of 106 patients received a pet scan before sbrt : 76 patients had choline - pet and 30 had psma - pet . median lymph node diameter was 13 mm ( range 345 )  . 
see lesion and treatment characteristics in table 2 . local , nodal control , and pattern of relapse median follow - up time was 16 months ( range 6101 )  . 
at the median follow - up , 40 ( 36.6% ) patients were free from any disease , 51 ( 46.8% ) patients had oligoprogression after the rst course of sbrt , while 18 ( 16.5% ) had a diffuse metastatic progression . 
we didnt observe any correlation between the use of adt and any of the outcome parameters , nor a statistical difference between the number of lesions treated and outcomes . moreover , no difference in terms of outcome was observed according to the kind of imaging performed before sbrt . we reported 6 ( 5.4% ) cases of grade 1 acute toxicity overall , consisting of 3 ( 2.7% ) cases of grade 1 diarrhea , fig . 
according to the literature , median pfs after sbrt in lymph node pca patients varies from 8.1 to 21 months [ 11 , 21 ] , and it was shown that the majority of relapses occur in lymph nodes near to previously irradiated sites in an oligoprogressive manner [ 11 ]  . 
in a retrospective multicenter italian study [ 10 ] , 100 oligorecurrent / oligoprogressive prostate cancer patients , both hormone nave and castration resistant , were treated with sbrt to 139 lymph node metastases . 
2 kaplan - meier curve showing out - of - eld nodal progression - free survival ( npfs ) of treated metastases 2 ( 1.8% ) cases of grade 1 fatigue , and 1 ( 0.9% ) case of grade 1 dysuria . 
in case of metastatic recurrent pca , the adoption of mdt by means of sbrt is able to modify the natural history of the disease in terms of local control , distant progression - free survival , and systemic therapies free - survival [ 19 ]  . 
3 kaplanmeier curve showing progression - free survival ( pfs ) of treated metastases for all patients ( a ) and according to prostate - specic antigen ( psa ) value ( b ) strahlenther onkol ( 2020 ) 196 : 213221 precociously to very small lesions could instead have a signicant amount of microscopic disease that may be revealed in the nearest follow - up . the toxicity reported in our study was very limited , with no events higher than grade 1 . 
local failure does not mean systemic failure of the treatment ; therefore , a local treatment aimed at ablating the progressive disease may allow continuation of the systemic treatment and , eventually , prolong survival . 
strengths of the study are the large population , the homogeneity of treatments in terms of radiation therapy technology , the systematic use of metabolic imaging , and the use of ablative doses of rt ( bed > 100 gy ) in the entire population . further prospective studies are warranted to assess the survival benet of this multimodal approach and the role of the re - challenge with further courses of sbrt when new oligoprogression occurs . conclusion in the present experience , a high rate of lc and a mild toxicity prole were reported . 
more specically , the possibility of postponing the beginning of systemic treatment with mdt through sbrt seems to be an intriguing strategy , in line with other similar other experiences . 
4 kaplanmeier curve showing androgen deprivation therapy ( adt ) - free survival 26.6% , respectively , with a median adt - free survival of 20.9 months and a 2and 3 - year adt - free survival of 47.3% and 31% , respectively . 
moreover , the increasing use of pet and the detection of small lymph nodes at very low levels of psa ( 50% detection rate with pet - psma when psa < 0.5 ng / ml ) [ 28 , 29 ] should be considered with caution . 
early diagnosis and treatment of small lymph nodes may not detect the real extension of metastatic disease ; therefore , patients treated 220 strahlenther onkol ( 2020 ) 196 : 213221 conict of interest l . 
januar 2020 der / die autor ( en ) 2020 hintergrund und ziel der arbeit als ziel setzten sich die autoren die identikation prtherapeutischer faktoren , um den erhalt der potenz nach einer hochdosierten protonentherapie wegen prostatakarzinom vorherzusagen . methode und patienten in der prospektiven kohortenstudie wurden die potenzraten und die auswirkung dieser auf die lebensqualitt mit hilfe von etablierten fragebgen ( epic [ expanded prostate index composite ] , iief [ international index of erectile function ] und ipss [ international prostate symptome score ] ) erfasst [ 1 ]  . 
von 1159 patienten , die von august 2006 bis mai 2010 eine hochdosierte protonentherapie bei prostatakarzinom erhalten hatten , wurden nach ausschluss der patienten mit hormontherapie die daten von 1005 patienten ausgewertet . 
anschlieend wurde anhand von baseline - faktoren ein nomogramm zur einschtzung der langfristigen erhaltung der potenz erstellt und anhand einer patientenkohorte aus einer prospektiven studie [ 2 ] validiert . 1 gy ( rbe ) : strahlendosis in gy , korrigiert fr die unterschiedliche relative biologische wirksamkeit ( rbe ) der partikeltherapie . 
bei protonen wird standardmig eine durchschnittliche rbe von 1 , 1 angenommen . originalpublikation holtzman al et al ( 2019 ) patient - reported sexual survivorship following high - dose image - guided proton therapy for prostate cancer . 
die potenzraten der gesamten kohorte betrugen zu beginn der behandlung 67 % , nach 6 monaten 61 % , nach 2 jahren 54 % und nach 5 jahren 46 % . 
in einer univariaten analyse mit kovariatenstratikation konnten folgende faktoren , die die potenz der 1005 mnner signikant beeinussen , identiziert werden : der epic sexual summary score , der iief sowie patientenbezogene faktoren , wie alter , eine vorliegende herzerkrankung , hypertonie , hyperlipidmie und diabetes mellitus . der body mass index ( bmi ) , beziehungsstatus , ethnie , t - stadium , gleason - score und psa ( prostata - spezisches antigen ) - wert sowie die bestrahlungsdosis beeinussten hingegen die potenz nicht statistisch signikant . 
durch rekursives partitionieren wurde ein nomogramm erstellt und die patienten anhand von 2 faktoren in 3 patientenkategorien eingeteilt : eine gruppe mit sehr guter erektionsfhigkeit mit potenzraten von 80 % ( n = 137 , p = 0 , 83 ) nach 5 jahren , eine intermedire gruppe mit potenzraten um 62 % ( n = 145 , p = 0 , 86 ) und eine gruppe mit schlechten potenzraten von 37 % ( n = 117 , p = 0 , 19 )  . 
bercksichtigt wurde hierbei die fhigkeit , eine erektion auszubilden ( mittels der einzelnen frage epic q57 ) sowie das vorliegen einer ( unspezizierten ) herzerkrankung . schlussfolgerung der autoren die erfassung der potenz vor einer strahlentherapie sowie der kardialen begleiterkrankungen ermglichen eine vorhersage der erektilen funktionsfhigkeit im verlauf nach der strahlentherapie . das miterfassen der komorbiditten im epic - fragebogen knnte es dann ermglichen , die sexualitt im langzeitverlauf mittels nomogrammen abzuschtzen und damit den patienten bei der wahl der therapie zu helfen . 294 kommentar patienten , die eine bestrahlung eines lokal begrenzten prostatakarzinoms erhalten , weisen sehr gute berlebenszeiten auf [ 3 ]  . 
um betroffenen mnnern bei der wahl der therapie zu helfen , wurde im rahmen der hier kommentierten studie ein einfaches nomogramm erstellt , um die 5 - jahres - erektionsfhigkeit nach hochdosierter strahlentherapie mit protonen vorherzusagen . 
eine zustzlich externe validierung wre im rahmen weiterer studien wnschenswert . da nur patienten mit einer protonenbestrahlung untersucht wurden , wre ein vergleich mit patienten nach photonenbestrahlung sowie vor allem nach operation oder kombinierter operation und nachfolgender bestrahlung sehr interessant . 
ein nomogramm , dass sowohl eine abschtzung der erhaltenen potenz nach bestrahlung als auch nach operation ermglicht , wre eine praktikable , einfache methode , um die posttherapeutischen nebenwirkungen vergleichbar abwgen zu knnen . 
einen unterschied in der beeinussung der potenz wrden wir zwischen einer bestrahlung mit photonen und mit protonen nicht erwarten , da die zielvolumina identisch sind . in der prostqa - studie wurden 2 - jahres - potenzraten von 40 % fr operierte , 58 % fr bestrahlte und 63 % fr patienten mit einer brachytherapie festgestellt [ 4 ]  . 
das junge patientenalter sowie der zugang zu einer protonentherapie , welche zumindest im herkunftsland der studie in der regel eher soziokonomisch besser gestellten patienten , denen meist eine gute medizinische versorgung , z . 
auch mit potenzmedikamenten , zur verfgung steht , strahlenther onkol ( 2020 ) 196 : 293295 knnten mgliche einussfaktoren fr die guten potenzraten sein . die univariate analyse zeigt auerdem , dass eine erhaltene potenz vor allem von komorbiditten ( herzerkrankungen , hypertonie , hyperlipidmie , diabetes mellitus ) und einer prtherapeutisch erhaltenen erektionsfhigkeit abhngt . da mehrere faktoren die potenz signikant beeinussen , wre an dieser stelle eine multivariate analyse aufschlussreich . interessanterweise konnte kein signikanter einuss auf die potenz durch tumorspezische faktoren ( t - stadium , gleason - score , psa - wert ) sowie strahlentherapeutische faktoren ( bestrahlungsdosis ) festgestellt werden . 
erklrung fr die differenten ergebnisse knnte die applizierte bestrahlungsdosis sein , da die mediane dosis bei 14 gy ( < 173 gy ) lag und weniger als 2 % eine dosis von 52 , 5 gy am bulbus penis erreichten . fazit die studie umfasst die grte kohorte zur sexuellen funktion von patienten , die eine protonenbestrahlung der prostata erhalten hatten . 
krause geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf strahlenther onkol ( 2020 ) 196 : 293295 literatur 1 . 
holtzman al et al ( 2019 ) patient - reported sexual survivorship following high - dose image - guided proton therapy for prostate cancer . radiother oncol 134 : 204210 2 . 
roach m et al ( 2004 ) penile bulb dose and impotence after threedimensional conformal radiotherapy for prostate cancer on rtog 9406 : ndings from a prospective , multiinstitutional , phase i / ii dose - escalation study . 
beyer2 matthias hipp3 ulrich neumaier4 felix steger1 barbara dietl1 received : 16 march 2019 / accepted : 27 june 2019 / published online : 15 july 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract background humeral epicondylitis is a common elbow disease . 
as the results of a re - irradiation have not been systematically analyzed , the aim of this study was to document the results of repeated radiation treatment and to identify those patients who will benet . material and methods the analysis was performed on patients from three german radiotherapy institutions and included 99 re - irradiated elbows . 
all subgroups , notably those with no response , partial response and recurrent pain had a signicant reduction of pain . conclusion re - irradiation of humeral epicondylitis is an effective and safe treatment . 
marien amberg , regensburg , germany amberg , germany private clinic for radiotherapy , mvz neumaier & kollegen , regensburg , germany 5 department of pathology , university of regensburg , regensburg , germany strahlenther onkol ( 2020 ) 196 : 262269 rebestrahlung bei epicondylitis humeri retrospektive analyse von 99 ellenbogen zusammenfassung hintergrund die epicondylitis humeri ist eine der hugsten erkrankungen des ellenbogens . 
da eine strukturierte auswertung der rebestrahlung bisher nicht existiert , war das ziel dieser arbeit , die ergebnisse einer wiederholten strahlenbehandlung zu dokumentieren und patienten zu identizieren , die von einer rebestrahlung protieren . material und methode ausgewertet wurden patienten aus drei strahlentherapeutischen institutionen . 
die schmerzintensitt wurde mit hilfe der numerischen ratingskala ( nrs ) quantiziert und zu den zeitpunkten vor bestrahlungsbeginn , direkt nach radiatio , 6 und 12 wochen sowie 6 , 12 und 24 monate nach bestrahlung erfasst . 
grund der rebestrahlung war in 39 , 7% kein ansprechen und in 41 , 0% ein unzureichendes ansprechen auf die erste bestrahlungsserie sowie in 19 , 3% rezidivierte schmerzen . ergebnisse es zeigte sich fr das gesamtkollektiv eine signikante schmerzreduktion . 
the drug treatment can be systemic , for example with nonsteroidal anti - inammatory drugs ( nsaids ) or can consist of local injections of anesthetics or steroids [ 4 , 5 ]  . 
 [ 5 , 726 ]  . there are several studies including some randomized trials with about 2000 published patients in total , which show the effectiveness [ 5 , 12 , 13 , 15 , 27 ]  . 
mostly a second or third irradiation course was given because of recurrent pain or partial or no response after the initial radiation course [ 10 , 12 , 1517 ]  . 
additionally , it should help to identify those patients who will benet from re - irradiation . patients and methods the study was approved by the ethics committee of the university of regensburg . 
1 consort diagram how patients were selected for this survey irradiated pa ( cid : 2 ) ents with humeral epicondyli ( cid : 2 ) s n = 241 irradiated elbows with humeral epicondyli ( cid : 2 ) s n = 263 exclusion of elbows receiving just one course of radiotherapy ( n = 157 ) re - irradiated elbows n = 106 were questioned about the current status and constantly clinically examined . 
etiologically the pain was caused by radiohumeral epicondylitis in 58 cases ( 75.3% ) , by medial humeral epicondylitis in 10 cases ( 13.0% ) and combined humeral epicondylitis in 9 cases ( 11.7% ) ( table 1 )  . radiotherapy was performed with a linear accelerator using 6 mv photons in opposing elds . 
treatment time was mostly 23 weeks ( two or three times per week ) , 62.6% of the elbows were re - irradiated over 2 weeks and 33.3% were re - irradiated over 3 weeks . 
acute or long - term side effects did not occur in this sample . results general response the median pain before the initial irradiation was 8 on the nrs ( iqr 69 )  . 
pain reduction compared with the pain level before re - irradiation was signicant with p < 0.0001 for the entire follow - up . analysis of dierent subgroups male and female patients , older or younger than 51 years had a signicant reduction in pain ( p < 0.001 for all categories and the entire follow - up )  . 
if these subgroups are compared for absence of pain and remaining nrs level , there was no signicant difference in the response rates except for the time 24 months after re - irradiation . concerning the results due to the reason for re - irradiation patients were analyzed separately based on the reason for re - irradiation . 
for those elbows with recurrent pain the median nrs was 6 ( iqr 58 ) before reirradiation , 3 ( iqr 14 ) directly after re - irradiation and 3 ( iqr 1 - 4 ) 6 weeks after re - irradiation . 
patients re - irradiated with 0.5 gy single dose to a total dose of 3.0 gy as well as those re - irradiated with 1.0 gy single dose to a total dose of 6.0 gy had a signicant response from treatment with p < 0.001 for the entire follow - up . 
patients with no response after the initial series are colored dark blue , patients with partial response blue and patients with recurrent pain light blue ( cid : 2 ) before reirradia ( cid : 2 ) on a ( cid : 3 ) er reirradia ( cid : 2 ) on 6 weeks 12 weeks 6 months 12 months 24 months no response [ nrs ] par ( cid : 2 ) al response [ nrs ] recurrent pain [ nrs ] with 6 times 1.0 gy ( p > 0.05 for the entire follow - up )  . 
for samples using generally two courses of radiation for humeral epicondylitis separated by 6 weeks , no specic analysis was done for the second course alone [ 20 , 21 ]  . 
for re - irradiation it is even more challenging as it is a very selected sample . bureaucratic obstacles and great efforts combined with the difculty to obtain nancial sponsorship to cover expenses have to be considered beside the difculties associated with research . 
although the von - pannewitz score might improve the comparability to other samples treated with irradiation for humeral epicondylitis , the nrs was analyzed because it is used in clinical routine in all three institutions . 
most of the patients had a response to re - irradiation and approximately 40% of the patients were free of pain or score low pain with nrs 1 for the long - term follow - up of at least 2 years . 
because of the multiple pretreated sample and the sample of just re - irradiated patients , a spontaneous remission exactly 612 weeks after re - irradiation seems to be very unusual , especially in such a high percentage . 
furthermore , for the continuing followup no more signicant changes in the level of pain could be detected , which makes a spontaneous remission even more 268 strahlenther onkol ( 2020 ) 196 : 262269 unlikely . 
the long - term response rate of approximately 70% in our re - irradiated sample is at least comparable to those data . if you have a look at the few and unstructured data for re - irradiation published so far , some information could be found from hess et al . 
ketterer just presented data directly after a second radiation course with a distinct improvement of 40% ( 70 out of 175 elbows ) and an absence of pain in 3% of the elbows ( 5 out of 175 ) [ 30 ]  . 
it has been proven in the literature that the time directly after radiotherapy cannot give a real idea of the long - term results [ 11 , 25 , 28 ]  . 
for samples , where generally two courses of radiation separated by 6 weeks were used for humeral epicondylitis , each one with a total dose of 6.0 gy , better results could not be found compared with a single course of 5.0 gy in total [ 20 , 21 ]  . for reasons of radiation protection a general application of two courses of radiotherapy for humeral epicondylitis has to be carefully evaluated as to its risk . 
as it is recommended for the initial series of radiation a single dose of 0.51.0 gy and a total dose of 3.06.0 gy , twice or three times weekly , should be used for re - irradiation of humeral epicondylitis [ 5 , 8 , 15 , 29 ]  . 
a single dose of 0.5 gy and a total dose of 3.0 gy over 23 weeks seems to be recommendable for reasons of radiation protection , based on the data of ott et al . 
all patients , male and female of all age categories , left and right elbows , those with radiohumeral epicondylitis and medial humeral epicondylitis showed positive responses to re - irradiation mainly without signicant differences among those subgroups . 
the fact that we could not nd signicant results for patients with medial humeral epicondylitis for all follow - up data , seems to be due to the relative small amount of patients with medial humeral epicondylitis . 
interestingly the dominant arm seems to respond better to reirradiation than the non - dominant arthere was no signicant difference for the patients re - irradiated over a 2 or 3 week period . 
patients with partial response to the initial radiation had the best chance to achieve absence of paonly some authors mention a third radiation series for humeral epicondylitis [ 16 , 30 ]  . 
as all our patients showed a response to the second re - irradiation , it seems to be ethical to irradiate patients a third time although there is no evidence for it . conclusion re - irradiation of humeral epicondylitis is an effective and safe treatment . 
schratter - sehn online publiziert : 4 february 2020 springer - verlag gmbh germany , part of springer nature 2020 strahlenther onkol ( 2020 ) 196 : 296314 vortrge gro oe01 unterschiede zwischen mrt und klinik beim staging des lokal fortgeschrittenen zervixkarzinoms j . 
schmid1 1universittsklinik fr strahlentherapie / medizinische universitt wien , wien , sterreich 2university medical centre utrecht , utrecht , niederlande 3department of radiotherapy , gustave - roussy , villejuif , frankreich 4department of oncology , aarhus university hospital , aarhus , dnemark 5mount vernon cancer centre , northwood , uk 6department of radiation oncology , tata memorial hospital , mumbai , indien 7department of oncology , institute of oncology ljubljana , ljubljana , slowenien 8department of oncology , the norwegian radium hospital , oslo university hospital , oslo , norwegen 9department of oncology , cross cancer institute and university of alberta , edmonton , kanada 10department of radiotherapy and oncology , postgraduate institute of medical education and research , chandigarh , indien 11leeds cancer centre , st jamess university hospital , leeds , uk 12radiation oncology department , radiotherapy group , arnhem , niederlande 13department of radiation oncology , university hospitals leuven , leuven , belgien 14department of radiotherapy , amsterdam university medical centers , university of amsterdam , amsterdam , niederlande 15clinic of oncology and womens clinic , st . 
olavs hospital , trondheim , norwegen 16oncology centre , cambridge university hospitals nhs foundation trust , addenbrookes hospital , cambridge , uk 17department of radiation oncology , leiden university medical center , leiden , niederlande einleitung : ziel der studie war die unterschiede zwischen klinik ( ausschlielich gynkologische untersuchung + urographie endoskopie ) im vergleich zur mrt beim staging des lokal fortgeschrittenen zervixkarzinoms im rahmen der embrace studie zu untersuchen . methodik : alle eingeschlossenen patientinnen wurden vor therapiebeginn klinisch untersucht und erhielten ein mrt des beckens . 
in dieser kohorte ergeben sich 26 tnm untergruppen . oe02 mammaria interna bestrahlung bei linksseitigem brustkrebs : knnen wir das risiko fr sekundrmalignome und ischmische herzerkrankungen mit modernen strahlentherapietechniken reduzieren ? s . 
alongi2 1klinik fr strahlentherapie , lmu mnchen , mnchen , deutschland 2klinik fr strahlentherapie , irccs sacro cuore don calabria hospital , negrar - verona , italien 3institut fr strahlenmedizin , helmholtz zentrum mnchen , mnchen , deutschland einleitung : in randomisierten studien konnte gezeigt werden , dass die bestrahlung der lymphabflusswege bei nodal - positivem brustkrebs die lokale kontrolle und das berleben verbessern kann . 
ziel dieser studie war es zu untersuchen , inwieweit unterschiedliche bestrahlungstechniken ( imrt vs 3dcrt ) das risiko fr herzerkrankung und strahleninduzierte sekundrmalignome ( lunge und kontralaterale brust ) bei der lymphabflusswegbestrahlung von linksseitigem brustkrebs beeinflussen . 
ein besonderer schwerpunkt der studie lag hierbei auf den auswirkungen der mammaria interna bestrahlung ( imc )  . methodik : es wurden insgesamt 40 bestrahlungsplne mit einer zielvolumendosis von 50 , 0 gy in 25 fraktionen generiert : ein 3d - konformaler bestrahlungsplan ( 3dcrt ) und ein intensittsmodulierter bestrahlungsplan ( imrt ) , jeweils unter einschlu der regionalen lymphabflusswege + / mammaria interna bestrahlung . 
hiervon wurde das relative risiko ( excess relative risk , err ) und das 10 - jahres absolute risiko ( excess absolute risk , ear ) fr sekundrmalignome ( lunge und kontralaterale brust ) , sowie fr ischmische herzerkrankungen ( cvd ) mit hilfe von linearen , linear - exponentiellen und plateau - modellen berechnet . 
statistische analysen wurden mit hilfe von wilcoxon signed - rank tests durchgefhrt . ergebnisse : die hinzunahme der imc - bestrahlung zur lymphabflussbestrahlung erhhte die dosisbelastung von herz , lunge und kontralateraler brust signifikant , sowohl in 3dcrt , als auch in imrtplnen ( p = 0 , 002 )  . 
dennoch war selbst bei verwendung der imrt - technik das geschtzte zustzliche absolute 10 - jahresrisiko fr cvd durch die imc - bestrahlung gro ( bis zu 4 % ) , was den nutzen der imc - bestrahlung fr patienten mit hohen kardiovaskulren basisrisiken einschrnkt . 
im hinblick auf die err fr sekundren kontralateralen brustkrebs , gab es einen signifikanten anstieg der err durch die hinzunahme der imc ( p = 0 , 002 ) , jedoch ohne einen einfluss der verwendeten rt - technik . schlussfolgerung : bei der hinzunahme der imc zur lymphabflussbestrahlung bei linksseitigem brustkrebs kommt es zu einer signifikanten dosisbelastung der risikoorgane , welche mit einem deutlich erhhten risiko fr schwere koronare ereignisse und strahleninduzierte sekundrmalignome ( lunge und kontralaterale brust ) einhergehen . 
in dieser situation erscheint die durchfhrung der bestrahlung mittels imrt im vergleich zu 3dcrt vorteilhaft . 4uniklinikum linz , linz , austria 5krankenhaus hietzing - lainz , vienna , austria 6landeskrankenhaus feldkirch , feldkirch , austria 7kaiser - franz - josef - spital , vienna , austria 8universittsklinikum graz , graz , austria 9landesklinikum wiener neustadt , wiener neustadt , austria 10klinikum klagenfurt , klagenfurt , austria 11medizinische universitt wien , vienna , austria strahlenther onkol ( 2020 ) 196 : 296314 oe03 erste klinische anwendung der augmented digital imaging methode zur objektiven beurteilung und dokumentation der wirksamkeit topischer hautprparate bei radiodermatitis r . 
kapp universittsklinik fr strahlentherapie radioonkologie , medizinische universitt graz , graz , sterreich einleitung : die beurteilung des schweregrades einer akuten radiodermatitis erfolgt in der klinischen routine mittels visueller inspektion der haut . 
 ziel dieser proof of consept studie war die erste klinische testung der von uns entwickelten augmented digital imaging methode zur sensitiven und quantitativen messung der effektivitt zweier topischer prparate zur behandlung der radiodermatitis . methodik : 100 patientinnen mit mammakarzinom wurden nach brusterhaltender operation einer adjuvanten radiotherapie unterzogen . 
zur verarbeitung wurden die aufnahmen in den l * a * b * farbraum transformiert und fr die jeweiligen farbparameter mittelwerte berechnet . ergebnisse : die beurteilung nach ctcae ergab eine statistisch signifikante interobservervariabilitt in der dokumentation von grad1 , 2 und 3 ( p < 0 , 001 )  . 
die objektive messung ergab einen hheren rtungsgrad mit einem anstieg des a * parameters um 4.15 ( 95 %ci : 5.972.33 , p < 0.001 ) durch die anwendung mit lactokiner1r2 . schlussfolgerung : diese daten zeigen , dass die subjektive beurteilung der radiodermatitis nach ctcae ungeeignet ist , um die effektivitt der testprodukte zu vergleichen . 
fr die benutzereinfachheit steht bereits eine app fr smartphones ( scarletredvision ) zur verfgung , die eine kostenund zeitsparende anwendung ermglicht . oe04 allstar ( austrian radiooncological lung cancer study association registry trial ) : treatment concepts for nsclc stage iii and their impact on clinical outcome in austria a multicentre registry study f . 
dieckmann11 1paracelsus medizinische privatuniversitt , uk fr radiotherapie und radio - onkologie , salzburg , austria 2wilhelminenspital , vienna , austria 3universittsklinikum krems , krems , austria background : in 2016 , approximately 5000 new lung cancer cases were reported in austria , 80 % of which were non - small cell lung cancers ( nsclc )  . 
the standard treatment is concomitant chemo - radiotherapy ( crt ) , which can be tolerated by merely one third of the patient population because of co - morbidities or bad general condition . 
the aim of this registry trial is to document the various treatment options currently used in austria and to assess their impact on loco - regional control and toxicities . methods : patients with pathologically proven nsclc stage iii are included . 
the co - primary endpoints are loco - regional control and toxicities . results : thus far ( 2019 / 09 ) , eight radiation oncological centres have decided to participate . 
based on an unpublished survey among these institutions , it seems realistic to recruit 300 patients within two years . conclusions : the allstar project is the first prospective web - based oegro registry . 
at the current stage it is meant to contribute to the discussion of three key issues : ( 1 ) treatment sequence of crt , ( 2 ) radiation dose escalation and ( 3 ) the addition of checkpoint inhibitors after completion of crt . oe05 prognose und geschlechtsspezifische unterschiede nach einzeitiger oder hypofraktionierter radiochirurgie j . 
zudem sollte das geschlecht als unabhngiger prognostischer faktor fr das gesamtberleben untersucht werden . methodik : dies ist eine retrospektive analyse von 281 aufeinanderfolgenden patienten welche eine radiochirurgie bei einzelnen oder multiplen hirnmetastasen erhalten haben . 
der prdiktive wert verschiedener prognostischer faktoren wurde mittels harrells c beurteilt . ergebnisse : das mediane gesamtberleben betrug 11 monate sowohl nach srs ( 95 % ki : 7 , 514 , 5 ) als auch nach hfsrt ( 95 % ki : 8 , 3 13 , 7 monate ; p = 0 , 99 )  . 
nach exklusion von patienten mit mammakarzinomen und propensity score - matching betrug das mediane gesamtberleben 16 monate fr frauen und 8 monate fr mnner ( p < 0 , 01 )  . 
die evaluation der prognosescores ergab die beste korrelation mit dem berleben fr bsbm ( harrells c = 0 , 68 ) , gefolgt sir ( 0 , 61 ) , gpa ( 0 , 60 ) , rpa ( 0 , 58 ) und rades etal . 
tubin sabr for unresectable pancreatic cancer : a monoinstitutional experience institut fr radioonkologie / kabeg klinikum klagenfurt , klagenfurt , austria background : loco - regional tumor control achieved with standard of care rt - cht for pancreatic cancer is poor . 
we analyzed our cohort of patients treated by sabr for pancreatic cancer in terms of feasibility , tolerability and local control . methods : 32 patients with unresectable pancreatic cancer of head ( 85 % ) and body - tail ( 15 % ) were included . 
in patients irradiated with bed10 > 100 only 1 local failure appeared , while among those irradiated with bed10 g2 was recorded . conclusions : sabr for unresectable pancreatic cancer appears safe and effective . 
insgesamt zeigten sich bei 21 % der patientinnen auffllige screening - werte , wobei patientinnen mit hals - kopf ( 37 % ) sowie uterus - / ovarial - ca ( 36 % ) die hchsten raten aufflliger werte zeigten . 
knapp 13 % der patientinnen gaben einen subjektiven po behandlungsbedarf an , wobei patientinnen mit brust ( 20 % ) und lungen - ca ( 19 % ) diesen am hufigsten uerten . 
 insgesamt zeigte sich in 83 % der flle eine bereinstimmung zwischen hsi - cut - off und behandlungswunsch , wobei die sensitivitt je nach tumorentitt variierte : whrend bei patientinnen mit hmoblastosen ( 94 % ) und rektum - ca ( 92 % ) die bereinstimmung sehr hoch war , lag sie bei patientinnen mit hals - kopf ( 62 % ) und kolon - ca ( 67 % ) verhltnismig niedrig . schlussfolgerung : ein veritabler anteil der onkologischen patientinnen berichten zu beginn der strahlentherapie von klinisch relevanten belastungen . 
die implementierung von po - screenings kann dabei helfen , betroffene patientinnen zu identifizieren , wobei die sensitivitt innerhalb der tumorentitten zum teil stark variiert . oe08 do radiation oncologists talk about sexual health and dysfunction with their cancer patients ? e . 
schratter - sehn2 1ordensklinikum linz , abteilung fr radio - onkologie , linz , austria 2kaiser franz josef spital , institut fr radio - onkologie , vienna , austria background : increasing survival rates of cancer patients lead to also focus on aspects of quality of life , due to the long - term effects of cancer and its treatment . 
the aim of this survey was to invite radiation oncologists to self - assess whether sexual health care and dysfunction are an issue in daily routine . methods : at the austrian annual meeting in 2017 92 physicians working in the field of radiation oncology participated and got a questionnaire . 
 participants were also asked about additional medical qualifications and trainings : none of the physicians had training in sexual medicine . conclusions : for the first time this survey draws a rough picture of sexual health care by austrian radiation oncologists . 
as doctor shortage is a problem in the observed country other kind of networks and counselling possibilities should be evaluated . 300 oe09 hyart - sib in lansclc is an effective dose escalation strategy h . 
zehentmayr2 1sonderabteilung fr strahlentherapie , kh hietzing , vienna , austria 2universittsklinik fr radiotherapie und radio - onkologie , landeskrankenhaus salzburg , salzburg , austria background : the standard treatment for locally advanced non - small cell lung cancer is concomitant radiochemotherapy with 60 gy . 
this mono - centre analysis presents patients treated with a hypofractionated dose - escalation regimen ( hyart - sib : hypofractionated accelerated radiotherapy with simultaneously integrated boost )  . methods : between 12 / 2006 and 4 / 2019 128 patients ( 48 f , 80 m ) were treated with hyart - sib . 
the rates of relevant pneumonitis , esophagitis and hemorrhage were 1 , 6 % ( n = 2 ) , 9 , 4 % ( n = 12 ) , and < 1 % ( n = 1 ) resp . conclusions : given that this analysis presents real world data , clinical outcome and toxicity of hyart - sib are comparable to concomitant radiochemotherapy . 
tubin phase2 study of innovative stereotactic body radiotherapy targeting partial tumor hypoxic ( sbrt - pathy ) clonogenic cells in unresectable bulky non - small cell lung cancer : profound non - targeted effects by sparing peri - tumoral immune microenvironment strahlentherapie / kabeg klinikum klagenfurt , klagenfurt , austria background : we present a novel concept of sbrt - based partial tumor irradiation targeting exclusively hypoxic clonogenic cells ( sbrt - pathy ) to treat unresectable bulky nsclc patients . 
multi - variate analysis for cancer specific survival was significant for treatment effect with sbrt - pathy ( p < 0.001 ) independent of age , sex , ecog status , histology , nsclc stage , treated bulky site and tumor diameter . 
georg medaustron ion therapy centre , wiener neustadt , sterreich einleitung : die therapie von patientinnen mit meningeomen , welche optische strukturen verdrngen , stellt hinsichtlich erhalt der lebensqualitt , insbesondere der beibehaltung der sehleistung eine herausforderung dar . 
die testzeitpunkte waren vor therapiebeginn , am therapieende , sowie 3 , 6 und 12 monate ( mo ) spter ( t1t5 ) ; auswertung mittels spss - 24 . ergebnisse : 47 patientinnen ( 37w / 10 m ) , 2482jahre alt ( mean = 52 ) , wurden eingeschlossen . 
soelkner risikomanagement in der strahlentherapie universittsklinik fr strahlentherapie , akhwien / medizinische universitt wien , wien , sterreich strahlenther onkol ( 2020 ) 196 : 296314 einleitung : risikomanagement ist ein kontinuierlicher prozess im dienste der patientensicherheit und fr die radioonkologie zustzlich in der medizinischen strahlenschutzverordnung ( medstrschv , 1617 ) explizit vorgeschrieben . 
demnach sind alle vertretbaren manahmen zu ergreifen , um die wahrscheinlichkeit und das ausma unfallbedingter medizinischer expositionen und unbeabsichtigter expositionen so gering wie mglich zu halten , sowie ein entsprechendes system zur aufzeichnung und analyse von ereignissen [ ] zu verwenden , um untersuchungen von risiken zu ermglichen . 
darber hinaus bietet risikomanagement die chance zu einer gelebten sicherheitskultur beizutragen sowie optimierte behandlungsmethoden durch einfhrung neuer hochprzisionstechnologien zu initiieren . methodik : reaktive risikoanalye : um informationen ber tatschliche und beinahe vorflle zu erhalten , ist ein internes strahlentherapiespezifisches meldesystem notwendig . 
darber hinaus wird fr zwei projekte zur erhhung der patientensicherheit durch implementierung neuer behandlungstechniken eine fmea vor inbetriebnahme durchgefhrt : mr - gesttzte radiotherapie : mrt bietet aufgrund des verbesserten weichteilkontrasts deutliche vorteile in der definition von tumorausdehnungen gegenber ct . 
 hieraus knnen manahmen zur optimierung des workflows und erhhung der pateintensicherheit abgeleitet werden . schlussfolgerung : das risikomanagement kann manahmen vorschlagen , um potentielle fehler zu reduzieren , arbeitsablufe zu optimieren und dadurch die patientensicherheit zu erhhen . 
hierfr muss sowohl der zeitliche als auch der personelle aufwand fr alle berufsgruppen im rahmen der personalplanung durch die klinikleitung bercksichtigt werden . vortrge rt rt01 intrafraktionelle bewegung in offenen und geschlossenen masken n . 
am institut fr radioonkologie strahlentherapie des landesklinikums wiener neustadt steht ein maskensystem zur verfgung , welches sowohl fr nicht - stereotaktische bestrahlungen ( zb hno ) als auch fr kranielle stereotaxien verwendet wird . 
diese arbeit untersucht , ob ein unterschied der intrafraktionellen bewegung zwischen offenen und geschlossenen masken , wobei beide typen fr stereotaktische patienten zum einsatz kommen , besteht . methodik : es wurden insgesamt 164 sitzungen ( von 40 patienten ) des zeitraums oktober 2017 bis juni 2019 ausgewertet . 
der mann - whitney - u - test ergab die folgenden wahrscheinlichkeiten ( p - werte ) : vertikal 0 , 030 , longitudinal 0 , 391 , lateral 0 , 053 , pitch < 0 , 001 , roll 0 , 737 , rotation 0 , 962 . schlussfolgerung : die intrafraktionelle bewegung in offenen und geschlossenen masken zeigte insgesamt nur geringe unterschiede . 
visionrt , london , uk einleitung : da die zahl stereotaktischer applikationen ( insbesondere im schdelbereich ) nicht zuletzt dank neuer technischer entwicklungen stetig ansteigt , wird die mglichkeit einer lckenlosen und hochprzisen berwachung der patientenposition whrend dieser behandlungen zunehmend wichtiger . 
implementierung und umsetzung eines markerlosen workflowsund atemgetriggerter bestrahlung mit aligne rt ( visison rt ) in die klinische routine werden dargestellt . methodik : die schrittweise umsetzung des konzepts mit entsprechenden qualittsberprfungen mit erstellung der sops sollen skizziert werden . 
zudem stellen wir den prozess der einfhrung der atemgetriggerten bestrahlung mit dem oberflchscannersystem dar . ergebnisse : die umstellung von hautmarkierungen auf markerlos hat eine hhere behandlungsgenauigkeit , ist weniger fehleranfllig . 
die patientenzufriedenheit der patienten ist sher hoch und die mtra und mitarbeiter hanen das konzeot der markerlosen einstellung gut angenommen . schlussfolgerung : markerlose einstellung und behandlung ist ein neuer standard in der strahlentherapie geworden . 
aufgrund der nachfrage an speziellen intraoperativen bestrahlungen und der einschrnkungen an den linearbeschleunigern im haus , kommt nun ein mobiles bestrahlungsgert im hybrid - op auf der chirurgie zum einsatz . methodik : fr den aufbau des ioert - teams wurden 6 radiologietechnologinnen und 7 physiker / innen von der firma sit eingeschult . 
fr die anfallenden behandlungen wurde eine spezielle sop in zusammenarbeit mit dem gesamten chirurgie - team ausgearbeitet um die lagerung der patienten zu regeln und so einen festgelegten ablauf zu schaffen . ergebnisse : die intraoperativen bestrahlungen mit dem mobilen bestrahlungsgert funktionieren sehr gut . 
immer wieder stt das gesamte ioert - team auf herausforderungen , die in zusammenarbeit mit der chirurgie ausgesprochen gut und stets mit erfolg gelst werden knnen . schlussfolgerung : jede intraoperative bestrahlung im hybrid - op ist speziell und bei keiner ist vorherzusehen , wie gut oder schlecht die einstellungen funktionieren . 
manchmal ist auch die interdisziplinre zusammenarbeit gefragt , um den weg zu finden , der fr den patienten die bestmgliche behandlung ermglicht . rt03 relevanz des zusammenspiels von bestrahlungsplnen und lagerungsmglichkeiten n . 
klinikum fr strahlentherapie - radioonkologie graz , graz , sterreich einleitung : erhebung der umsetzbarkeit von bestrahlungsplnen in abhngigkeit von lagerungsmglichkeiten und daraus resultierende auswirkungen auf die belastung der risikoorgane . methodik : erfassung von daten anhand klinischer beispiele aus der tglichen routine . ergebnisse : es zeigten sich unterschiedliche auswirkungen auf die risikooraganbelastung in abhngigkeit der komplexitt des plans und der reproduzierbarkeit der patientenlagerung . schlussfolgerung : der bestrahlungsplan ist nur so gut wie die reproduzierbarkeit der tglichen patientenimmobilisierung . strahlenther onkol ( 2020 ) 196 : 296314 mp01 p . 
 klinikum graz , graz , sterreich einleitung : die arbeitsgruppe radiochirurgie und stereotaxie ( degro ) und der arbeitskreis physik und technik in der stereotaxie ( dgmp ) haben ein dokument in form eines reviews verfasst , das sich eine detaillierte ausformulierung und diskussion der minimalen technischen qualittsanforderungen in der stereotaxie zum ziel setzt . 
es werden sowohl intracranielle stereotaxie als auch sbrt behandelt . im rahmen dieser prsentation werden die inhalte des review - artikels dargestellt und anmerkungen , die im rahmen der begutachtung des manuskripts aufgeworfen wurden , diskutiert . methodik : fachexperten der dgmp , gmp und der sgsmp waren eingeladen , an der begutachtung des manuskriptes mitzuarbeiten , bevor dieses fr den druck freigegeben wurde . 
dazu wurden die im review formulierten empfehlungen anhand der aktuellen literatur validiert und aus sicht der klinischen anwendbarkeit und umsetzbarkeit analysiert . ergebnisse : generell ist dieser review von degro und dgmp ein sehr grndlich recherchiertes und gut strukturiertes dokument . 
sehr konkret im sinne einer richtlinie wird das dokument hingegen etwa bei den empfehlungen hinsichtlich der strahlkollimation , der dosisberechnungsalgorithmen oder der toleranzen bezglich der mechanischen genauigkeit . schlussfolgerung : der review technische qualittsanforderungen fr die stereotaktische strahlentherapie ist ein sehr umfassendes dokument , das als leitlinie zur klinischen implementierung der stereotaxie herangezogen werden kann und somit ein wichtiges und aktuelles hilfsmittel fr die klinische praxis darstellt . mp02 evaluation of the interand intrafraction motion for head and head and neck patients at the particle therapy centre medaustron based on the comparison of different commercial immobilisation devices a . 
stock1 1medaustron ion therapy centre , wiener neustadt , austria 2university clinic for radiotherapy and radio - oncology , paracelsus medical university , salzburg , austria background : in december 2016 the clinical operation started at the particle therapy center medaustron , wiener neustadt , austria . 
these immobilisation devices are a combination of table tops ( qfix bos headframe , elekta headstep ) , pillows ( moldcare , headstep pillow ) and thermoplastic masks ( klarity green , qfix fibreplast , headstep icast double )  . 
for each patient image - guided therapy is performed by acquiring orthogonal x - ray imaging and 2d3d registration and the application of the resulting 6 - degree of freedom ( dof ) correction vector on the robotic couch . methods : the interand intrafractional motions of 101 patients are evaluated and compared among each other regarding stability during each fraction and reproducibility during the entire treatment . 
for the comparison , statistical methods ( shapiro wilk test , mann whitney u - test ) are applied on the correction vectors as well as on the difference correction vectors before and after the fraction . 
based on these results the actual planning target volume margins of 3 mm are evaluated via robustness calculations of 12 different translational offset scenarios and the van herk formula . results : statistically significant differences between the immobilisation devices are found , but they turn out to be clinically not relevant . 
 the setup margin for head patients is 0.8 mm ( lateral ) , 1.2 mm ( cranio - caudal ) and 0.6 mm ( ap ) , and for h&n patients it is 1.7 mm ( lateral ) , 1.4 mm ( cranio - caudal ) and 1.4 mm ( ap )  . conclusions : based on these values and a hounsfields units ( hu ) uncertainty of 3.5 % , robustness evaluations of selected head and head and neck patients showed the validity of the currently used ptv margins . mp03 srs mapcheck implementierung und erste praktische erfahrungen in der stereotaxieqa k . 
etzelstorfer abteilung fr radio - onkologie , barmherzige schwestern , ordensklinikum linz , linz , sterreich einleitung : ziel war die implementierung einer qualittskontrolle ( qa ) fr die stereotaktische bestrahlung kleiner zielgebiete mit hohen dosen . 
dies wurde insbesondere getrieben durch die anschaffung einer neuen software fr stereotaktische bestrahlungsplanung ( elements von brainlab ) , welche unter anderem die optimierung der dosisverteilung einzelner ( srs cranial ) und multipler metastasten ( multiple brain mets srs ) in einem plan erlaubt . methodik : einen wesentlichen teil dieser qa stellt die verifikationsmessung von bestrahlungsplnen mit kleinen feldern dar , was die verwendung eines messmittels mit hoher rtlicher auflsung bedingt . 
dieses erst seit mai 2018 neu am markt verfgbare gert erfllt als einfach zu handhabendes messsystem mit ortsauflsung im mm - bereich die fr unsere messaufgaben geforderten bedingungen . ergebnisse : die ersten schritte fr die anwendung erfordern die korrekte kalibrierung des messmittels in bezug auf die empfindlichkeit des messarrays und die dosis . 
diese arbeit zeigt die praktischen erfahrungen bei der implementierung des messsystems fr die qa stereotaktischer bestrahlungsplne in unserer abteilung , beginnend mit den ersten schritten und lernprozessen bei der kalibrierung ber die messung einfacher testplne bis hin zur verifikation komplexer multimets - plne . 
ziel war es die 304 strahlenther onkol ( 2020 ) 196 : 296314 eine methode zu finden , die die beurteilung eines komplexen dhvs beschleunigt und eine bersichtliche dokumentation ermglicht . methodik : aus dem planungssystem wird das dvh exportiert und anschlieend mittels excel eingelesen und verarbeitet . 
das volumen und ebenso die dosis knnen relativ oder absolut beurteilt werden . gleichzeitig ist auch ein eqd2 - rechner implementiert der die umrechnung beliebiger einzeldosisvorschreibungen auf die 2 gy referenz dosis ermglicht . ergebnisse : durch diese methode steht der abteilung eine zeitsparende und bersichtliche auswertung von dvh - daten zur verfgung . 
 pain relief was measured during follow - up . results : in all , 598 evaluable patients ( 394 female , 204 male ) with a mean age of 61.4 years ( range , 3381 ) were recruited . 
in general , rt had a better effect on enthesiopathies than on arthrosis . conclusions : low - dose rt is a very effective treatment for the management of painful benign skeletal disorders . 
 klinikum graz , graz , sterreich einleitung : die morphea der brust ist eine autoimmunreaktion des subkutanen bindegewebes , die unter anderem durch die therapie mit ionisierenden strahlen getriggert wird . 
ziel dieser studie war die inzidenz einer morphea nach adjuvanter radiotherapie der brust zu erheben um mehr evidenz fr die hufigkeit dieser schweren komplikation zu generieren . methodik : retrospektive auswertung von patientinnen , die zwischen 20092018 nach brusterhaltender tumorresektion einer adjuvanten radiotherapie unterzogen wurden und die ihnen empfohlenen nachsorgeuntersuchungen in unserer klinik in anspruch genommen haben . 
fr numerische daten wurde der median und die spannweite , fr kategorische daten absolute und relative hufigkeiten berechnet . ergebnisse : von insgesamt 5129 bestrahlten patienten nahmen 2268 die nachsorgekontrollen war . 
bei 2236 ( 98 , 6 % ) dieser patienten wurde die brust konventionell fraktioniert bestrahlt mit einer gesamtdosis von 50 gy + tumorbettboost von 1014 gy , 32 ( 1 , 4 % ) erhielten eine gesamtdosis von 40 , 05 gy in 15 fraktionen . 
dies legt den verdacht nahe , dass bei einer betrchtlichen patientenzahl die erkrankung im initialen stadium als infektion und im weiteren verlauf als postradiogene fibrose fehlinterpretiert wird . untersuchung spezifischer einflussfaktoren auf die internetrecherche zu gesundheitsthemen von patientinnen mit der diagnose krebs e . 
dieplinger3 1universittsklinik salzburg radiotherapie und radioonkologie , salzburg , sterreich 2universittsklinik fr strahlentherapie radioonkologie , medizinische universittsklinik graz , graz , sterreich 3institut fr pflegewissenschaft und - praxis , pmu salzburg , salzburg , sterreich einleitung : zur informationsbeschaffung zu gesundheitsrelevanten inhalten ist das internet zu einem integralen bestandteil geworden . 
 ziel dieser masterarbeit ist es , herauszuarbeiten , inwieweit sich diese patientinnen online zu ihrer krankheit informieren . methodik : 100 konsekutive patientinnen , die sich wegen einer malignen tumorerkrankung an der universittsklinik fr radiotherapie und radioonkologie am lkh salzburg einer strahlentherapie unterzogen haben , wurden in die auswertung einbezogen . 
soziodemografische parameter wie alter , geschlecht , bildung und wohnortgre sowie die hufigkeit und die qualitt der internetnutzung wurden dabei erhoben und statistisch ausgewertet . ergebnisse : 66 % der befragten nutzten das internet zu gesundheitsthemen . 
ob online recherchiert wird oder nicht , war geschlechtsunabhngig , jedoch recherchierten frauen hufiger hinsichtlich themen wie vernderungen des lebensstils und im falle leichterer erkrankungen . schlussfolgerung : das internet ist eine wichtige informationsquelle , die von mnnern wie auch frauen gerne herangezogen wird . 
schwierigkeiten sehen die hlfte der patientinnen in der identifizierung qualittsvoller online - information , sodass handlungsbedarf in der erlangung von grerer medienkompetenz besteht . postoperative stereotaxie der resektionshohle bei hirnmetastasen prospektive untersuchung der lokalen tumorkontrolle , des gesamtberlebens und der neurokognitiven funktion r . 
kapp1 1universittsklinik fr strahlentherapie radioonkologie , medizinische universitt graz , comprehensive cancer center , graz , sterreich 2fh joanneum graz , graz , sterreich einleitung : behandlungsoptionen intrakranieller metastasen beinhalten in abhngigkeit von anzahl , lage , gre , allgemeinzustand und neurologie die neurochirurgische resektion , die stereotaktische radiochirurgie , die fraktionierte stereotaktische radiotherapie ( fsrt ) und die ganzhirndurchflutung ( wbrt )  . 
ziel der vorliegenden studie ist den einfluss einer adjuvanten fsrt der resektionshhle auf lokalkontrolle , gesamtberleben und neurokognitive funktionen zu untersuchen . methodik : patientinnen mit isolierten intrakraniellen metastasen wurden nach chirurgischer resektion in die prospektive studie eingeschlossen . 
die merkfhigkeit wurde mittels hopkins verbal learning test ( hvlt ) und die wortassoziationsfhigkeit mittels controlled oral word association ( cowa ) jeweils an den zeitpunkten unmittelbar vor fsrt , einen monat und sechs monate nach abschluss der bestrahlung erfasst . ergebnisse : das mediane gesamtberleben der 31 patientinnen lag bei 20 monaten ( 12 - monats - berlebensrate 70 % )  . 
 nach 6 monaten steigerte sich die gemerkte mittlere wortanzahl um 2 , 5 wrter ( p < 0 , 01 ) , sowie zwischen monat1 versus monat6 um 1 , 3 wrter ( p = 0 , 04 )  . 
auch im cowa erhhte sich die anzahl der assoziierten wrter nach einem monat von 9 , 6 auf 12 , 9 ( p = 0 , 01 )  . schlussfolgerung : durch eine postoperative fsrt der intrakraniellen resektionshhle knnen gute lokale kontrollraten bei maximaler schonung angrenzender hirnareale erzielt werden . 
eine beeintrchtigung der neurokognitiven funktionen ( gedchtnis und wortassoziation ) wurde durch die fsrt nicht gemessen , da die dosis des hippocampus sehr gering war . vertebral metastases of vaginal paraganglioma treated with radiation therapy : case report and review of literature b . 
sedlmayer radioonkologie / uniklinikum salzburg ( salk ) / universittsklinik fr strahlentherapie und radio - onkologie , salzburg , austria background : paragangliomas , also known as extra - adrenal phaeochromocytomas , are very rare and slow - growing tumors of the autonomous nervous system , which hardly ever metastasize . 
this is the first case report describing radiotherapy for a spinal metastasis of a vaginal paraganglioma by intensity - modulated radiotherapy with simultaneous integrated boost ( sib - imrt )  . 
while being the nineth case report on this disease ours is the first involving radiation therapy as a primary treatment modality . results : in the follow - up visits at four , eight and twelve weeks after the end of the irradiation , the patient did not report any treatment related toxicity . 
the fdg - pet / ct performed 6 months after radiotherapy showed tumor regression in the pelvis , lungs and vertebral metastases with a 25 % decrease in metabolic activity in the both irradiated vertebrae . conclusions : in summary , studies that investigate the role of radiotherapy in the treatment of malignant paraganglioma are few in number . 
however , most reportsincluding oursdescribe good tumor control and thereby substantiate the role of radiotherapy as an effective curative treatment option for metastatic vaginal paragangliomas . withdrawn interimsanalyse zur digitalen erfassung und berechnung strahleninduzierter hautvernderungen mit scarletred vision r . 
klinik fr strahlentherapie - radioonkologie , medizinische universitt graz , comprehensive cancer center , graz , sterreich 306 strahlenther onkol ( 2020 ) 196 : 296314 2dislozierte einrichtung der univ . 
ziel dieser studie ist die weltweit erste anwendung von scarletred vision zur nicht invasiven objektiven hautanalyse im radioonkologischen routinebetrieb . methodik : in diese prospektive studie wurden von 12 / 20186 / 2019 an der univ . 
die interimsanalyse fr bestrahlungen von brust ( 45 % ) und kopf - hals ( 6 , 9 % ) ergab eine messbare vernderung der parameter a * ( rtung ) und l * ( pigmentierung ) ber die bestrahlungszeit . 
fr den daraus generierten algorithmus ( l * max l * ) x a * ( standard erythema value ) konnte ein anstieg dargestellt werden . schlussfolgerung : diese fr den klinischen patientenbetrieb neue methode zur nicht invasiven , objektiven und sensitiven digitalen hautanalyse liefert informationen ber lokale hautvernderungen . 
theodorou advances in radiotherapy for brain tumors ( malignant , benign and pediatric ) at the bank of cyprus oncology center bank of cyprus oncology center nicosia , nicosia , cyprus background : treatment of brain tumors is challenging as they are sometimes inoperable due to their anatomical location . 
radiation therapy with the latest techniques igrt ( image guidance radiotherapy ) and vmat ( volumetric modulated arc therapy ) is considered to be a good solution for such cases , as high doses can be delivered to the tumour bed whilst sparing organs at risk , especially in cases where the patient has received previous radiation locally . 
comparing the 3d - conformal radiotherapy technique with the vmat - igrt techniques the coverage of the target and the conformality is higher and at the same time the dose for the organs at risk is lower . 
the decision for radiation therapy is taken by a multidisciplinary tumour board for cns tumours . methods : comparing 3d - conformal techique with vmat for brain tumors specially the coverage of target and the dose for organs at risk . results : in conclusion it is recommended that vmat ( volumetric modulated radiotherapy ) technique for radiotherapy for brain tumors compared the 3d - conforaml technique is advisable due to the good coverage of the target and the good safety at the same time for the organs at risk . 
most of the brain tumors have indication for reradiation due to progression , so the vmat technique occurs more safety for the organs at risk in case of reradiation later . 
lower dose for the organs at risk means less radionecrosis risk fro the patient . conclusions : in conclusion it is recommended that vmat ( volumetric modulated radiotherapy ) technique for radiotherapy for brain tumors compared the 3d - conforaml technique is advisable due to the good coverage of the target and the good safety at the same time for the organs at risk . 
most of the brain tumors have indication for reradiation due to progression , so the vmat technique occurs more safety for the organs at risk in case of reradiation later . 
folgende eingriffe wurden zumindest einmal durchgefhrt : vaginalzylinder 57 % der befragten , stift / ring 43 % , stift / ring mit nadeln 26 % , ldr / hdr der prostata 23 % , interstitielle mammaimplantation 26 % , savi / mammosite 14 % , haut ( valencia / leipzig ) 11 % . 
hug medaustron ion therapy center , wiener neustadt , austria background : despite the long experience with radiotherapy for the treatment of pancreatic cancer , several points remain controversial , instrahlenther onkol ( 2020 ) 196 : 296314 cluding the optimal technique , dose , fractionation , organ motion coping strategy and target volume definition . 
risk of nodal metastasis as reported in pathology series of operated pancreatic cancer was examined ( employing the japanese pancreas society definition of upper abdominal lymph node stations )  . 
the contouring strategy will follow that employed at national institute of radiological sciences in japan . results : two clinical target volumes will be used , a larger ctv1 that will account for risk of microscopic spread and a smaller ctv2 . 
according to jps classifications , for tumor of the head stations number 8 , 13 , 14 , 16 , 17 will be included , for tumors of the body / tail stations number 8 , 9 , 11 , 14 , 16 , 18 will be included . 
the neuroplexus will be included in ctv1 extending the contour dorsally / posteriorly to include the anterior wall ( rim ) of vertebral bodies / discs and laterally to include 1 cm left of the aorta and at least the left half of the inferior vena cava . conclusions : medaustron contouring strategy enables future dose escalation to the macroscopic tumor while still treating a large area at risk of microscopic infiltration carbon ion dose constraints for organs at risk at medaustron p . 
hug medaustron ion therapy center , wiener neustadt , austria background : medaustron started clinical operation with protons in december 2016 and with carbon ionradiotherapy ( cirt ) in july 2019 . 
 dose constraints for organs at risk ( oars ) in carbon ion radiotherapy have been established in the clinical routine of already treating facilities but are , up to now , not completely harmonized . 
in cirt , as compared to photons and protons rt , it is less straightforward to derive dose constraints for oars from published data especially because of the different rbe models employed . 
dose constraints based on the analysis of clinical outcome in patients treated with cirt in japan are available for : visual pathways , brainstem , brain , skin , rectum , duodenum and maxillary bone . 
the translation of mmkm constraints into lem - i values is being extensively studied in cnao . methods : all these data were reviewed and were used to estimate dose constraints to be used in medaustron with cirt , employing both a fractionation similar to hit ( 3 gy rbe per fraction at 5 fractions per week to a total of 2022 fractions ) and a fractionation similar to japanese centers after conversion for different rbe models as performed in cnao ( 4.14.8 gy rbe per fraction at 4 fractions per week to a total of 16 fractions ) results : cirt dose constraints used at medaustron are displayed in table 1 . conclusions : cirt dose constraints can be based on clinical data but extra care is needed to account for different rbe models used by different facilities . implementation of carbon ion protocols in clinical practice at medaustron p . 
hug medaustron ion therapy center , wiener neustadt , austria background : medaustron is a synchrotron based dual particle therapy facility that started carbon ion radiotherapy ( cirt ) in july 2019 . methods : during the first two years clinical activity will follow established protocols , in the attempt to reproduce clinical results obtained in germany and in japan . 
conversion of prescribed dose from the japanese rbe model to lem - i will be based on simulations performed on geometric targets with the same approach employed in the italian facility ( cnao )  . results : all indications for cirt require gross residual disease . 
bone and soft tissue sarcomas in the axial body and local recurrence in the pelvic wall from primary rectal cancer will also be treated with a 16 fraction schedule derived from japanese experience . 
with the availability of organ motion mitigation strategies , hypo - fractionated cirt will be used in pancreatic cancer patients with 12 fractions for locally advanced cancer ( lapc ) and 8 fractions for preoperative treatment . 
innere medizin , gkk ambulatorium graz , graz , sterreich einleitung : aminotransaminasen , einschlielich der aspartat - aminotransaminase ( ast ) und der alanin - aminotransaminase ( alt ) , spielen eine zentrale rolle im metabolismus von krebszellen und wurden mit der prognose von verschiedenen tumorentitten assoziiert . 
in der vorliegenden studie wurde die prognostische bedeutung der prtherapeutischen ast / alt ratio bei patienten und patientinnen mit plattenepithelkarzinomen der mundhhle und des oropharynx untersucht . methodik : in die retrospektive studie wurden 515 patienten , die an der univ . 
linzer effects of radiotherapy in scchn patients on the expression of activatory nk cell receptors klinik und poliklinik fr radio - onkologie und strahlentherapie , klinikum rechts der isar mnchen und helmholtz - zentrum mnchen , munich , germany background : every year approximately 500.00 new cases are diagnosed with squamous cell carcinoma of the head and neck ( scchn )  . 
for a better understanding of immune modulatory effects of rt , the immune phenotype of peripheral blood lymphocytes of patients with scchn was determined before , during and after rt and compared to that of healthy volunteers . methods : differential blood counts , total lymphocyte counts and the immune phenotype were analysed in the blood of scchn patients ( n = 16 ) 4 weeks prior to rt ( t0 ) , after 30 gy ( t1 ) , after approximately 67 gy at the end of rt ( t2 ) , and in the follow - up period 6 weeks ( t3 ) and 3 months ( t4 ) after therapy . 
the t0 values of scchn patients were compared to that of healthy human volunteers ( n = 20 )  . results : compared to a healthy control group , the expression density of the activatory nk cell receptor nkg2d was significantly lower in scchn patients at diagnosis . 
the absolute numbers of cd3 - / cd19 + b cells as well as different nk cell subpopulations ( cd56 , cd94 , nkg2d , nkp30 , nkp46 ) decreased during rt but recovered at t3 . 
the expression density of different activatory nk receptors reached a maximum at the end of rt ( t2 ) and returned to initial levels at t4 . conclusions : the expression density of the activatory nk cell receptor nkg2d is significantly lower in scchn patients at diagnosis than in healthy human volunteers . 
zakaria charakterisierung der effektivitt von photonenstrahlen auf etablierte 2dund 3d - osteosarkomzellen medizinische universitt wien , applied and translational radiobiology ( atrab ) , wien , sterreich einleitung : mit einer weltweiten , jhrlichen inzidenz von 3 , 4millionen menschen ist das osteosarkom die dritthufigste primre krebserkrankung bei jugendlichen . 
daher steht im vordergrund dieser arbeit die etablierung und charakterisierung von osteosarkom - konstrukten , um die effekte einer rntgenbestrahlung auf diese tumorzellen und ihre tumormikroumgebung zu untersuchen . methodik : zum einen wurde das klonogene zellberleben von mg - 63 tumorzellen mittels koloniebildungstest nach einer rntgenbestrahlung mit 0 gy , 2 gy , 4 gy , 6 gy , 8 gy untersucht und als berlebenskurve dargestellt . 
zum anderen wurden dreidimensionale tumorsphroidmodelle aus zustzlichen zelltypen , wie humanen osteoblasten und mesenchymalen stammzellen , in ula - mikroplatten ( ultra low attachment plates ) konstruiert und mit 0 gy , 2 gy , 4 gy , 6 gy , 8 gy bestrahlt . 
drei endpunkte ( tag0 , 14 , 21 ) wurden festgelegt und mittels wachstumskurve und immunhistochemischer untersuchungen dargestellt . ergebnisse : die berlebenskurven zeigen , dass fr mg - 63 eine kontinuierliche reduktion des zellberlebens mit zunehmender dosis ein310 strahlenther onkol ( 2020 ) 196 : 296314 hergeht . 
 ebenfalls wurde festgestellt , dass eine aktivierung der mesenchymalen stammzellen zu tumor - assoziierten fibroblasten ausschlielich in sphroiden mit einer zusammensetzung von 50 % mg - 63 , 30 % msc und 20 % humanen osteoblasten in 100 %igem emem - nhrmedium zu beobachten ist . 
die verteilung der einzelnen zelltypen in sphroiden wurde durch immunhistochemische frbungen mit antikrpern , die spezifisch fr die einzelnen zelltypen sind ( collagenx fr mg - 63 ; cd105 fr mesenchymale stammzellen ; bsp fr humane osteoblasten ) evaluiert und eine wachstumskurve erstellt , bei der abhngig von der dosis zunchst eine zellreduktion der sphroide ab tag9 zu beobachten ist und eine anschlieende erholung und beginnendes zellwachstum ab tag15 zu bemerken ist . schlussfolgerung : zusammenfassend soll eine effiziente therapie des osteosarkoms , nicht nur auf die tumorzellen , sondern auch auf die tumormikroumgebung etabliert werden . 
kowaliuk einfluss einer systemischen gabe von thalidomid auf die frhe und chronische strahlenreaktion der harnblase ( maus ) medizinische universitt wien , wien , sterreich einleitung : die strahlentherapie von beckentumoren birgt ein gewisses risiko an komplikationen an der harnblase , welche auf strahleninduzierten entzndungsreaktionen und deren auswirkungen basieren . 
frhe nebenwirkungen treten meist im laufe der strahlentherapie auf und knnen konservativ behandelt werden , whrend chronische folgen meist nach einer mehrjhrigen latenzzeit auftreten und in einer progressiven fibrose enden . 
in dieser prklinischen studie wird die rolle von nf - b und dessen gezielter hemmung mittels thalidomid untersucht . methodik : die erfassung funktioneller vernderungen an der harnblase erfolgt nach lokaler einzeitbestrahlung ( 5 dosisgruppen ) mittels transurethraler zystotonometrie zur ermittlung des harnblasenvolumens und der analyse der miktionsfrequenz . 
 histologische proben werden tglich in der frhphase und in 30 - tages - abstnden in der sptphase entnommen . ergebnisse : histologische daten weisen auf eine 2 - phasige aktivierung von p50 und p65 ( nf - b - domnen ) hin , und demonstrieren eine hemmende wirkung von thalidomid . 
 beide frhapplikationen von thalidomid reduzieren frhe und spte funktionsstrungen deutlich und signifikant , die spte gabe dagegen nicht . schlussfolgerung : nf - b spielt eine wichtige rolle in der frhen und chronischen phase strahlen - induzierter komplikationen an der harnblase . 
die frhe gabe von thalidomid mildert die frhe strahlenzystitis und reduziert das ausma an ( konsekutiven ) chronischen konsequenzen . entwicklung eines tumor - normalgewebs - modells fr das pankreaskarzinom einfluss des tumormikromilieus auf die strahlenreaktion v . 
hier beschreiben wir die charakterisierung und strahlenbiologische untersuchungen eines neuen , heterogenen in vitro 3d - modells des pankreaskarzinoms , welches tumorzellen mit normalgewebsbestandteilen kombiniert . methodik : drei heterogene konstrukte werden aus pankreas - tumorzellen ( panc - 1 ) , sternzellen , fibroblasten und epithelzellen in unterschiedlicher zusammensetzung kombiniert . 
der effekt der unterschiedlichen kombinationen auf die strahlenreaktion ( 150 kv rntgenstrahlung ) wird nach einzeitbestrahlung ( 214 gy ) und spter auch in fraktionierungsexperimenten ermittelt . ergebnisse : immunhistologische untersuchungen besttigen die erfolgreiche kombination aller zelltypen zu vitalen und proliferativen sphroiden . 
kowaliuk etablierung und charakterisierung eines multizellularen 3d - sphroid models des osteosarkoms medizinische universitt wien , universittsklinik fr strahlentherapie , wien , sterreich einleitung : das osteosarkom ( os ) ist der hufigste primre knochentumor , welcher vor allem kinder und jugendliche unter 20jahren betrifos zeichnet sich durch aggressives wachstum , frhzeitige metastasierung und schlechte heilungschancen aus . 
die vorliegende studie beschftigt sich mit der etablierung und charakterisierung eines neuartigen dreidimensionalen ( 3d - ) multizellulren sphriodmodels , um die interaktionen zwischen tumor und normalgewebszellen zu untersuchen . strahlenther onkol ( 2020 ) 196 : 296314 methodik : fr die etablierung des multizellulren 3d - sphroidmodels wurde die saos - 2 osteosarkom - zelllinie verwendet . 
um unterschiedliche , im os vorliegende , heterogene tm - bedingungen nachbilden zu knnen , wurden saos - 2 zellen mit den primren normalgewebszellen ( humane osteoblasten und msc ) in unterschiedlichen verhltnissen gemischt und die sphroide immunhistochemisch ( ihc ) mit zellspezifischen markern charakterisiert . 
der einfluss der sphroid - zusammensetzung auf die strahlenreaktion wurde nach bestrahlung ( 150 kv rntgenstrahlung ) mit gestaffelten dosen hinsichtlich des wachstums analysiert . ergebnisse : die sphroide mit unterschiedlichen tumor - stroma anteilen zeigten ein kontinuierliches wachstum ber den beobachteten zeitraum von 4 wochen . 
erste bestrahlungsversuche deuteten auf ein moduliertes wachstumsverhalten der heterogenen sphroid - konstrukte im vergleich zu reinen tumor - sphroiden h besonders konstrukte mit hherem stromalen anteil scheinen ein schnelleres wachstum und eine erhhte strahlenresistenz aufzuweisen . 
 die ergebnisse der charakterisierung sowie der ersten bestrahlungsversuche werden prsentiert . schlussfolgerung : die vorliegende studie liefert erste hinweise , dass die 3d ko - kultivierung von saos - 2 zellen mit humanen osteoblasten und msc zu in - vivo hnlichen bedingungen fhrt . 
borneman3 1surgical research laboratories / department of surgery / medical university of vienna , vienna , austria 2department of environmental health sciences , fielding school of public health , university of california , los angeles , usa 3department of microbiology and plant pathology , university of california , riverside , usa 4department for radiologic technology , university of applied sciences wiener neustadt for business and engineering ltd . , wiener neustadt , austria 5department of biomedical imaging and image - guided therapy , medical university of vienna , vienna , austria 6departments of pathology and environmental health sciences , university of california , los angeles , usa 7institute of pathophysiology and allergy research , medical university of vienna , vienna , austria background : few studies have examined whether the intestinal microbiota can modulate the effects of exogenous carcinogenic factors , such as exposure to ionizing radiation [ 1 ]  . methods : changes in intestinal microbiota following high linear energy transfer ( let ) irradiation were determined in murine mucosal cells and feces from conventional microbiota ( cm ) mice and a murine line bearing an anti - inflammatory restricted microbiota ( rm )  . results : irradiation ( ir ) - altered gene expression was observed for tumor necrosis factor - alpha ( tnf - ) and chemokine c - c motif ligand 20 ( ccl20 ) in bone marrow and small intestine . 
the abundance of bacterial indicator phylotypes post - ir was correlated with those in the rm mouse model conclusions : the investigation of intestinal microbiota composition was set post the acute radiation injury time within six weeks post total body ir to estimate long - term side effects of radiotherapy . 
to analyze if an app - based follow - up would be accepted by elderly cancer patients , we conducted a single - center prospective feasibility study ( nct03196050 )  . materials and methods cancer patients ( 60 years ) without concurrent uncontrolled severe medical conditions and a karnofsky performance status ( kps ) 70 were eligible if they were able to use the smartphone app . 
the primary endpoint was compliance over 1 year , calculated as patient - specic and study date - specic response rate to questions sent as push notications ; in this interim analysis , we report on 4 - month data . 
secondary outcomes included a comparison of a subjective health status item ( sphs ) with the physician - rated kps . results out of 225 patients screened , 54 patients agreed to participate and 29 activated the app and participated in the study . 
the average percentage of patients who sent answers at least weekly was 75.0% ( sd = 14.8% ) and declined from 100% in week 1 to 53.8% in week 17 post - enrollment . 
further trials should aim at an increased participation rate . keywords app - based follow - up mobile health electronic health assessment patient - reported outcomes app - based reporting prospektive studie zum telemonitoring mit smartphones bei geriatrischen krebspatienten zusammenfassung hintergrund und ziel in randomisierten studien konnte gezeigt werden , dass das elektronische erfassen von patient - reported - outcomes die therapieergebnisse bei krebspatienten verbessern kann . 
mit der monozentrischen prospektiven telegraph - studie untersuchten wir , ob eine appgesttzte nachbeobachtung von geriatrischen krebspatienten machbar ist ( nct03196050 )  . material und methoden ltere krebspatienten ( 60 jahre ) ohne schwere / unkontrollierbare begleiterkrankungen und mit einem karnofsky - index ( kps ) von 70 konnten eingeschlossen werden , sofern sie in der lage waren , die smartphone - app zu bedienen . 
sekundre endpunkte beinhalten den vergleich des subjektiven gesundheitsstatus ( sphs ) mit dem rztlich erfassten kps . ergebnisse von 225 patienten , die hinsichtlich der studieneignung untersucht wurden , erklrten sich 54 bereit , teilzunehmen . 
die mittlere wochenspezische compliance , deniert als mindestens eine rckmeldung pro woche , lag bei 75 , 0 % ( sd = 14 , 8 % ) und reduzierte sich von 100 % in studienwoche 1 auf 53 , 8 % in studienwoche 17 . 
die auswertung der sekundren endpunkte ergab , dass der appbasierte eortc - qlc - c30 von patienten akzeptiert wird ; weiterhin zeigt sich eine moderate signikante korrelation zwischen sphs und kps ( r = 0 , 566 ; p < 0 , 001 )  . schlussfolgerung unsere daten deuten darauf hin , dass eine appbasierte nachbeobachtung unter einbeziehung von eortc - fragebgen bei lteren krebspatienten mit akzeptabler compliance mglich ist ; zuknftige studien sollten die erhhung der teilnehmerrate zum ziel haben . schlsselwrter appgesttzte nachbeobachtung smartphoneuntersttztes reporting elektronische nachbeobachtung mobile gesundheitsdatenerfassung appbasierte datenerfassung the major concern raised about the implementation of mobile technology into routine cancer care is that older patients will miss out many of its benets [ 4 ]  . 
this is of specic relevance , as more than half of the total cancer incidence and most of the cancer mortality occurs among the elderly [ 5 ]  . to nd out whether elderly patients can be acquainted with a digital app - based follow - up , we conducted a prospective trial assessing the compliance of elderly cancer patients using handheld devices for symptom and quality of life ( qol ) reporting during or after radiotherapy . introduction patient - centered applications are being implemented into clinical cancer care more often , as they bear the promise of delivering cost - effective real - life images of shortand long - term responses to cancer treatments [ 1 ]  . 
recently , two randomized trials have demonstrated that web - based follow - up with threshold - triggered intervention can result in an increase in overall survival as compared to routine follow - up [ 2 , 3 ]  . 
adherence is dened as the rate of response to daily push notications sent to patients ; in case of non - adherence , patients were not contacted via other channels . 
in this preliminary report , we analyze the rst 4 months after enrollment ( month 03 ; i.e. , 120 - day compliance )  . two secondary outcome measures were dened : first , a descriptive longitudinal evaluation of health - related quality of life ( hrqol ) as measured by the eortc - qlqc30 questionnaire ( with permission of the eortc ) and second , a comparison between the subjective perception of the health status ( sphs ; see supplementary table 1 ) and the physician - rated patient status as measured by the karnofsky performance status ( kps )  . 
for the interim analysis reported here , we analyzed the timeframe from day 0 to day 120 ; patients with non - adherence prior to day 120 who re - connected after > 120 days were not counted as permanent dropouts but only counted as non - compliant during the actual time of non - compliance . patients had to activate the app at least once after agreeing to participate to be included in the study . for the primary endpoint , we calculated two types of compliance rates : first , an individual compliance rate was calculated as the ratio of all answered daily questions to all push notications that were sent during the timeframe ; e.g. , if a certain patient survived until day 86 , 86 daily push notications would have been sent . 
if 43 answers had been submitted , the individual compliance rate would be 50% . empty messages were allowed as negative answers to the question of whether unexpected events had occurred ; furthermore , if a patient did not answer a push - notication but did answer another questionnaire ( sphs or eortc - qlqc30 ) sent on the very same day , this was also counted as compliant . 
second , daily compliance rates were calculated as the ratio of all received answers from different patients on a certain day after enrollment to all push notications that were sent on that day ; e.g. , if on day 95 , 25 push notications were sent to patients and 20 answers submitted , the daily compliance rate would be 80% ; again , a patient could also answer the sphs or the eortc - qlq - c30 questionnaire to fulll the compliance endpoint . 
for the comparison 208 strahlenther onkol ( 2020 ) 196 : 205212 between sphs and the physician - rated kps , we calculated a mean sphs value , which included the same - day value ( if obtained ) and / or the values obtained on 2 days prior and after the physician assessment . 
the association between the sphs item and the physician - rated kps was calculated using spearmans nonparametric correlation coefcient ; the same approach was used to determine if there was an association of the individual compliance rate with baseline patient factors ( exploratory analysis )  . results patient screening and enrollment patient screening started in october 2016 and ended in september 2018 . 
out of 209 patients with whom the study was discussed , 127 declined to participate ( 60.8% ) and 28 patients ( 13.4% ) did not own a smartphone and declined to use the offered study device . 
out of these , two ( 3.8% ) were screening failures and did not meet the inclusion criteria ; 23 ( 42.6% ) patients never activated the app , primarily because fig . 
details on the nal study cohort are compiled in table 1 . a criminal investigation ( further details unknown ) , and technical issues which occurred during the ongoing study ( n = 2 ) but could not be resolved . 
we could not identify a pattern to predict extreme divergence between kps and sphs ranks ( i.e. , comparably low kps and high sphs or vice versa , data not shown )  . 26 out of 29 patients ( 89.7.1% ) answered all of the eortc - qlq - c30 items at the rst questionnaire ( month 1 , days 030 ) ; the number declined to 17 patients ( 58.6% ) who answered all questions at the fourth month . 
4 ; all other scales from the eortc - qlq - c30 questionnaire and detailed numbers of patients who answered are shown in the supplementary appendix ( supplementary table 2ab )  . 
as an example , on day 67 , the rst patient was censored ; therefore , 28 patients remained uncensored on trial ; at the end of the interim period , 4 patients were censored , 25 patients remained uncensored on treatment . 
the last full week for the weekly compliance ended on day 118 , with 26 uncensored patients and 14 patients who responded to questionnaires , resulting in a weekly compliance at the end of the interim period of 53.8% ( 14 / 26 ) adult population owns a smartphone and capturing health issues with patient - owned devices thus appears largely feasible , carrying the hope of increased patient compliance and a more robust reporting of health - related issues [ 10 ]  . 
specifically , remote monitoring of adverse events and symptoms indicative of cancer progression has recently been shown to improve overall survival in clinical trials [ 2 , 3 ]  . elderly patients are the cohort most affected by cancer [ 5 ] and radiation therapy is routinely performed in advanced ages [ 11 ] , albeit at an increased risk of intolerance [ 12 ]  . 
patient data from europe on smartphone ownership in seniors showed considerable differences between countries [ 14 ] , with the lowest numbers in southern europe of 8.8% and the highest in norway of 43.1%. 
the distribution of individual patient compliance over the 120 - day study period cated that 64% of patients aged 5075 years , but only 30% of patients older than 75 years owned a smartphone [ 13 ]  . 
patients were not asked for details if they did not wish to participate and only a minority specically detailed the lack of a smartphone as a reason ; therefore , it is likely that some patients who declined to participate due to unknown reasons also did not own a smartphone . 
on the other hand , the elderly population using a smartphone is growing in all regions , likely leading to improved acceptance of app - based follow - up in future trials [ 13 ]  . 
previous studies suggested that income levels between cancer patients who participate in clinical trials differ from those who do not participate in trials [ 15 ] ; however , we did not evaluate such factors for this interim analysis . more than half ( 55.6% ) of the patients still sent at least one update per week at the end of the interim phase of 120 days ; limited data from an app - based intervention study in asthma patients resulted in a similar adherence rate of 54% after a 30 - day observation period [ 16 ]  . 
this might also be disease specic , with weekly or monthly updates being optimal for malignancies with longer progression - free intervals and daily updates for patients suffering from more aggressive tumors . 
on the other hand , as suggested by the declining compliance in our study , daily notications combined with questionnaires every other day might have been too much of an effort for many patients with cancer ; therefore , weekly notications or questionnaires combined with the possibility for patients to use the app as a tool to get in touch with their caregivers might be a preferable approach . furthermore , it might be easier for some patients to report strahlenther onkol ( 2020 ) 196 : 205212 fig . 
hrqol was measured by the general qol / hrqol scale of the eortc - qlq - c30 questionnaire ; other scales are shown in the supplementary appendix answers to a multiple - choice questionnaire instead of freetext responses . secondary endpoints in our study indicated that even longer questionnaires such as the eortc - qlq - c30 are relatively well accepted on a monthly basis in the participating patient cohort . 
the moderate strength of physicianscored kps and patient - reported sphs is in line with other reports indicating that physicians tend to underestimate the symptom burden reported by patients [ 1719 ]  . 
because of the initial patient selection , our ( participant ) cohort may not truly reect typical elderly patients , as 87.1% of screened patients never activated the app , leading to a selected elderly cohort . furthermore , due to the feasibility character of the study , i.e. , the small number of participants , the heterogeneous trial population , and the missing control group , we did not analyze clinical efcacy endpoints . despite these weaknesses , our data clearly show that out of the low number of smartphone owners in this cohort , a relevant percentage of elderly patients can be recruited for an app - based follow - up model ; furthermore , compliance rates of participants are likely sufcient for an app - based follow - up in larger trials in elderly patients . 
additionally , increased weekly response numbers in comparison to the daily response rates indicate that a tailored , possibly disease - specic notication interval might lead to increased compliance rates . 
finally , non - adherent patients could also be contacted via other channels , e.g. , follow - up calls by study nurses could be added to the protocol to potentially increase compliance rates . conclusion this is the rst report on the feasibility of an app - based follow - up in a patient cohort including exclusively elderly patients . 
our data indicate that the participation rate is low , but the compliance rate might be sufcient to establish an app - based follow - up which includes eortc questionnaires in larger trials in elderly cancer patients . acknowledgements we thank all patients and their families for their participation in this trial . 
wenz reports grants and personal fees from elekta ab , sweden , personal fees from roche pharma ag , grants , personal fees , and other from carl zeiss meditec ag , personal fees from celgene gmbh , personal fees from eli lilly and company , and personal fees from ipsen pharma gmbh outside the submitted work . 
giordano reports grants and personal fees from noxxon pharma ag , grants and personal fees from carl zeiss meditec ag , personal fees from bristol - myers squibb , personal fees from roche pharma ag , personal fees from msd sharp and dohme gmbh , personal fees from astrazeneca gmbh , grants and travel compensation from elekta ab , and shares from implacit gmbh . 
data of 103 patients were fully recorded and cox regression analysis was used to analyze the correlations of potential risk factors with 5 - year overall survival ( os )  . 
die daten von 103 patienten wurden vollstndig aufgezeichnet und die cox - regressionsanalyse wurde verwendet , um die korrelationen des potenziellen risikofaktors mit dem 5 - jahres - gesamtberleben ( os ) zu analysieren . 
post - rt - nlr zeigte eine gute prognoseleistung in der validierungskohorte ( konkordanzindex = 0 , 73 , standardfehler 0 , 10 ; p = 0 , 02 , wilcoxon - test )  . schlussfolgerung post - rt - nlr ist ein unabhngiger prognosefaktor fr das os bei lanpc - patienten . 
die dynamische nderung der routinemig getesteten entzndlichen variablen knnte dazu beitragen , geeignete behandlungsoptionen und follow - up - strategien zu entwickeln . schlsselwrter verhltnis von neutrophilen zu lymphozyten komplettes blutbild nasopharynxkarzinom prognosefaktor strahlentherapie introduction nasopharyngeal carcinoma ( npc ) has a distinct epidemiology and natural behavior from other head and neck squamous cell cancers , with remarkably high incidence rates in southeastern china [ 1 ]  . 
due to the development of intensity - modulated radiotherapy ( imrt ) and the incorporation of concurrent chemotherapy with rt , the therapeutic outcomes of npc patients have signicantly improved during the past decades . 
additional biomarkers are needed to further stratify patients and facilitate individualized therapy . the complex crosstalk between cancer cell and tumor microenvironment ( tme ) may have a signicant inuence on patient prognosis [ 4 ]  . 
the usual review board requirement of written informed consent was waived because the study was retrospective in design . 254 treatment details of the initial evaluation and diagnosis , radiotherapy technique and methodology , chemotherapy dose modication , and follow - up assessment were described in our previous report [ 10 ]  . patients in the training cohort received sequential chemoradiotherapy : imrt proceeded by two cycles of induction chemotherapy ( ic ) and followed by two cycles of adjuvant chemotherapy : gemcitabine 1000 mg / m2 on days 1 and 8 , plus cisplatin 25 mg / m2 on days 1 to 3 , every 3 weeks . 
patients in the validation cohort received two cycles of ic ( docetaxel 6075 mg / m2 on day 1 , cisplatin 75 mg / m2 on day 1 ) followed by concurrent chemoradiotherapy ( cisplatin 75 mg / m2 every 3 weeks for twice during rt )  . data collection baseline patient and tumor characteristics , including age , sex , pathological type , and treatment strategies including rt dose and type of chemotherapy were collected from the hospital information systeall patients diseases were ( re ) staged based on tnm stage according to the 7th edition of international union for cancer control / american joint committee on cancer ( uicc / ajcc ) cancer staging system for npc . 
all above - mentioned information was prospectively recorded for the training cohort and retrospectively collected for the validation cohort . complete blood counts ( cbc ) were assessed within 3 days before each chemotherapy cycle , and liver and renal functions were assessed within 1 week before each chemotherapy cycle . 
blood samples were collected in k2edta evacuated plastic tubes and were then analyzed using a sysmex xn - 9000 ( sysmex co . , kobe , japan ) automated hematology analyzer , within 10 min from sample collection . 
the diagnosis of anemia was based on the world health organization criteria : hemoglobin ( hb ) < 130 g / l ( men ) or < 120 g / l ( women )  . 
thrombocytopenia is dened as blood platelet < 100 109 / l , and thrombocytosis is dened as blood platelet > 300 109 / l . survival times were calculated as the time between the date of the beginning of induction chemotherapy and the rst event of interest , whichever came rst . 
events were death from any cause for overall survival ( os ) , death or tumor progression for progression - free survival ( pfs ) , lostrahlenther onkol ( 2020 ) 196 : 252261 coregional recurrence for locoregional control ( lrc ) , and distant metastasis for distant control ( dc )  . 
a two - tailed pvalue < 0.05 was considered statistically signicant . results patient characteristics out of the 112 patients in the training cohort , we excluded 9 patients because of missing cbc data during treatment . therefore , 103 patients were included in the nal analysis . 
for the validation cohort , of the 236 patients in total , 7 patients were excluded for missing cbc data , 29 patients for receiving weekly concurrent cisplatin during rt , and 5 for not receiving chemotherapy due to comorbidities . 
the baseline clinicopathological characteristics of the 133 discarded patients are displayed in supplementary table 1 . survival and relapse in the training cohort , the median follow - up was 70 months ( range 36116 )  . 
twenty - nine ( 28.2% ) patients had disease recurrences : 15 had locoregional recurrences ( lr ) , 10 had distant metastases ( dm ) , and 4 had both lr and dm . 
1 kaplanmeier survival curves of a overall survival and b progression - free survival of patients in the training cohort and validation cohort ( solid line , training cohort ; dotted line , validation cohort )  . 
mva identied patient age > 50 years old ( hr = 3.4 , p = 0.02 ) , weight loss during rt > 7.5% ( hr = 3.2 , p = 0.03 ) , and post - rt peripheral nlr > 7.05 ( hr = 2.5 , p = 0.04 ) as independent unfavorable prognostic factors for os . 
besides , the requirement of biopsy tissues for the testing of these markers restricts the feasibility of evaluation at multiple timepoints . on the other hand , the peripheral nlr is an easily measured , cost - effective , and objective surrogate marker of systemic inammation in daily clinical practice . 
a neutrophil - to - lymphocyte ratio ; b platelet count ; c hemoglobin at timepoints of pre - ic , pre - rt , and post - rt ; d lactate dehydrogenase , and e albumin level at timepoints of pre - ic and post - rt . 
ns no signicant difference , asterisk p < 0.05 , double asterisk p < 0.01 , triple asterisk p < 0.001 , ic induction chemotherapy , rt radiotherapy , ldh lactate dehydrogenase , plt platelet count genesis , neutrophils exert an anti - tumor activity directly via reactive nitrogen species ( ros ) , tumor necrosis factor ( tnf - ) , tnf - related apoptosis - inducing ligand ( trail ) , antimicrobial protein , or antibody - dependent cell - mediated cytotoxicity ( adcc )  . 
then , in the cancer progression process , neutrophils inhibit the adaptive immune response and promote tumor angiogenesis , the endothelial to mesenchymal transition ( emt ) , and metastases [ 1618 ]  . 
although the underlying basis is not altogether clear , it could be theoretically inferred that an elevated nlr might be associated with a more pro - tumoral tme , thus leading to poorer prognosis . 
besides , a marked systemic inammatory response could also be associated with patient - related factors such as nutritional , functional , and immunological decline [ 20 ]  . a considerable amount of evidence has been accumulated that nlr is associated with an unfavorable prognosis in various types of cancers including colorectal , gastric , esophageal , pancreatic , liver , renal , and gynecologic cancers as well as oropharyngeal and nasopharyngeal carcinoma [ 5 , 17 , 19 , 21 , 22 ]  . 
a meta - analysis including six studies with a total of 4359 npc patients showed that elevated pretreatment nlr was associated with poorer os ( hr = 1.74 , 95% ci = 1.452.10 ) and pfs ( hr = 1.48 , 95% ci = 1.301.69 ) [ 22 ]  . 
with the wake of recent therapeutic breakthroughs in the eld of immunotherapy , an emerging concept is that disease progression and treatment also strongly depend on external signals from the tumor microenvironment [ 23 ]  . 
rt can induce the upregulation of tumor - associated antigens and major histocompatibility complex class i expression . after a transient local lymphocyte depletion , immune cells were then recruited into the tumor bed after rt . 
therefore , rt turns cold tumors into hot ones , with the activation of innate and adaptive immune cells such as t lymphocytes and monocytes which later differentiate into tumorassociated macrophages [ 24 , 25 ]  . 
in the clinical setting , in a study of oral cavity cancer patients , neoadjuvant concurrent chemoradiotherapy was shown to drive the composition of inammatory cells in both peritumoral stromal and intraepithelial compartments toward a prognostically favorable direction [ 26 ]  . 
therefore , the post - ( chemo ) radiotherapy nlr , representing the post - treatment balance of proand anti - tumor inammatory activities in the host , might be a meaningful factor to predict the prognosis of patients after rt . 
indicated that the use of different cut - off values for nlr ( < 3 or 3 ) did not affect the consistent prognostic value of nlr for os or pfs [ 32 ]  . 
first , the blood counts data were collected retrospectively in both cohorts from the electronic information system and blood tests were not systematically carried out for the purpose of the present study at specic timepoints . 
therefore , post - rt blood routine was tested 3 weeks after the second cycle of concurrent cisplattherefore , 260 strahlenther onkol ( 2020 ) 196 : 252261 although the applied chemotherapeutic approach may indeed have an impact on the whole leucocyte count , the impact may not be very signicant , as the myelosuppression toxicity of both chemotherapy regimens may have mostly alleviated at the timepoint of the blood testing . 
thirdly , the follow - up time of the validation cohort was relatively short , and for this reason , quite a number of patients were censored after month 36 , which may potentially bias the survival outcomes . 
another caveat is that plasma epstein - barr virus ( ebv ) dna load was not systematically tested in the current study cohorts because it had not yet been established as standard at our institution during the period of investigation ( 20052015 )  . 
however , quantitative polymerase chain reaction ( pcr ) assays to test the dna copy numbers can yield large variability in results without harmonization , even when conducted in experienced institutions [ 35 ]  . 
this simple and objective prognostic assay right after ( chemo ) radiotherapy could help physicians make a timely clinical decision change , such as whether or not to add adjuvant chemotherapy in the patients with high nlr level or make a more cautious follow - up plan for these patients . 
aim of this study was to quantify skin dose variation and to assess the need of planning adaptation ( art ) to counteract it . methods planning cts of 32 patients treated with helical tomotherapy ( ht ) according to a simultaneous integrated boost ( sib ) technique delivering 54 / 66 gy in 30 fractions were deformably co - registered to mvcts taken at fractions 15 and 30 ; in addition , the rst fraction was also considered . 
negative changes were correlated with the presence of any overlap between ptv and sl at planning and were explained in terms of how the planning system optimizes the ptv dose coverage near the skacute toxicity was associated with planning dvh and this association was not improved if considering dvhs referring to fractions 15 / 30 . conclusion about half of the patients treated with sib with ht for hnc experienced a skin - sparing effect during therapy ; only 6% experienced an increase . 
our ndings do not support skin - sparing art , while suggesting the introduction of improved skin - sparing planning techniques . keywords head and neck cancer skin toxicity adaptive radiotherapy tomotherapy radiotherapy planning berwachung von vernderungen der hautdosis whrend der bildgesteuerten helikalen tomotherapie bei patienten mit kopf - hals - tumoren zusammenfassung zweck eine erhhung der hautdosis whrend der strahlentherapie von kopf - hals - tumoren ( hnc ) ist potenziell gefhrlich . 
negative nderungen korrelierten mit der anwesenheit einer berlappung von ptv und sl bei der planung und wurden dahingehend erklrt , wie das planungssystem die ptv - dosisabdeckung in der nhe der haut optimiert . 
unsere erkenntnisse untersttzen keine hautschonende plananpassung ( art ) , schlagen jedoch die einfhrung verbesserter hautschonender planungstechniken vor . schlsselwrter kopf - hals - tumoren hauttoxizitt adaptive strahlentherapie tomotherapie strahlentherapie - planung introduction despite the signicant improvements in planning and delivery , mainly due to the introduction of intensity modulation ( imrt ) and daily image - guidance ( igrt ) , radiotherapy ( rt ) of head and neck cancers ( hnc ) is still associated with clinically signicant side effects [ 13 ]  . 
among them , skin toxicity often occurs in the early phase , and may severely affect the patients quality of life ( qol ) during and immediately after rt [ 47 ] , causing potentially detrimental treatment interruptions . 
the quantitative skin doseeffect relationship remains largely underexplored [ 3 ] , although it is expected to exist [ 10 , 11 ] ; on the other hand , clinical guidelines for the prevention and treatment of acute and late skin reactions are well established [ 1214 ]  . the widespread availability of highly effective and feasible intensity - modulated igrt techniques [ 1520 ] may pave the way for more rened skin - sparing techniques . 
in addition , hnc patients are subject to substantial anatomical changes during rt , and these may result in unplanned variations of the dose distribution , potentially associated with an increased risk of complications . 
the possibility of implementing adaptive radiotherapy ( art ) with the aim of avoiding skin overdosing has never been explored , nor has the extent of such modications been quantied . 
skin dose changes may critically depend on the combination of body contour modications and the position of the skin relative to the incident uence patterns , and are largely dependent upon planning / delivery techniques as well as the dimension / shape / position of clinical and planning target volumes ( ctv / ptv )  . the evaluation of skin dose changes during rt requires a robust and sufciently accurate dose - of - the - day method . 
an in - house approach optimized for computation of the dose - of - the - day in helical tomotherapy ( ht ; accuray , sunnyvale , ca , usa ) was recently developed and validated by our group [ 21 , 22 ] , based on the deformable image registration ( dir ) of the planning ct to the daily mvct followed by the direct dose calculation on the resulting deformed ct ( ctdef )  . the aims of this investigation were to quantitatively evaluate the changes of skin dose during ht for hnc in a group of patients sufciently large to detect clinically relevant trends of dose variation during therapy and to assess the potential need for art to avoid skin overdosing during ht . in addition , as acute toxicity data were available for these patients , we preliminarily analyzed the association between skin dosevolume histograms ( dvh ) at planning and during therapy against the risk of moderate / severe acute cutaneous toxicities . 
this analysis was performed also with the aim of quantifying any possible improvement in predicting the risk of skin toxicity provided by the dvhs calculated during therapy compared to planning dvh . materials and methods study population this study involved 32 randomly chosen patients treated in the period 20072016 with a simultaneous integrated boost strahlenther onkol ( 2020 ) 196 : 243251 ( sib ) approach delivering 54 / 66 gy in 30 fractions to lowrisk lymph nodes ( ptv1 ) and tumor / positive lymph nodes ( ptv2 ) , respectively , with ht ( using an unattened beam at a xed energy 6mv )  . 
mvcts were available for all of them , fully including ptv2 ( i.e. , avoiding cutting portions of the high - dose skin volume )  . of note , according to our practice , mvct dose was not considered in the planned / delivered dose : the additional dose due to on - board imaging was estimated to be around 0.3% of the totally delivered dose . for selected patients , an additional concomitant boost to fdg - pet - positive volumes delivering 69 gy / 30 fraction was also administered . 
ptvs were generated by expanding the corresponding ctvs by 5 mm ; in case ptvs showed part of their volumes in air , they were cropped using margins from body external contour between 0 and 2 mm , as chosen by the radiation oncologist . 
deformed images ( ctdef ) were then imported to the dqa ( delivery quality assurance ) station module of the tomotherapy planning system ( tps ) , by considering the images as phantoms . 
subsequently , ctplan and ctdef with their own dose distributions were exported to mim , where the skin contouring was performed . the skin was automatically generated as the inner ring of the body contour segmented with mim by the expand / contract contour and whole body tools , respectively . in this way , the skin , dened as a 2 - mm skin layer ( sl ) structure , was segmented in ctplan and ctdef referring to fractions 15 and 30 ( ctdef15 and ctdef30 )  . 
dvhs of the inner rings were calculated in mim and exported for analysis . a thickness of 2 mm was chosen as representative of the epidermis and the dermal shell thickness [ 26 ] , including the basal epidermal cells and the dermal micro - vessels of the papillary layer supplying the epidermis . 
our dose - of - theday method was previously validated [ 21 , 22 ] by comparing dose distributions calculated on ctdef to those calculated on a gold standard diagnostic ct taken on the same day . regarding skin dose changes , the method was found to be superior to the direct mvct calculation [ 22 ]  . analysis of skin dose changes during therapy once the ctplan was deformed on mvct15 / mvct30 , the dose distribution was recalculated on the deformed series ct15def / ct30def and the corresponding sl dvhs were extracted . 
skin dose variations were assessed by comparing sl dvhs during therapy to the planning sl dvhs , and the statistical signicance of these differences was assessed by paired t - test applied on the whole range of doses ; the method has already been widely used in the literature ( see for instance [ 28 ] )  . 
subsequently , the volume of sl receiving 95% of the prescribed dose ( 62.7 gy ) was arbitrarily taken as representative of the high - dose region and its variation during therapy ( ( cid : 2 ) sl95% ) was analyzed in more detail . positive variations indicate an increase of skin dose during therapy ; conversely , negative ( cid : 2 ) sl stands for a skinsparing effect . 
due to possible anatomical changes between the planning ct and the start of the therapy likely to depend on the time between planning ct and therapy ( ( cid : 2 ) t ) , the correlation between ( cid : 2 ) sl95% and ( cid : 2 ) t was also investigated . 
in addition , the skin dose at the rst fraction was also recalculated for all patients and the correlation between changes at the rst fraction and during treatment was investigated . 246 strahlenther onkol ( 2020 ) 196 : 243251 correlation between sl planning / therapy dvhs and skin toxicity results the correlations between dvh of sl calculated at planning ( ct ) , halfway ( ctdef15 ) , and end ( ctdef30 ) of therapy were preliminarily analyzed against available toxicity data . 
acute skin toxicity of all patients was prospectively scored according to the ctcae v40 [ 30 ] , assessed as the peak score during treatment and after the treatment within 3 months from its end . 
for the remaining 15 / 32 patients , changes were within 1 cc . table 1 mean , median , and standard deviation ( sd ) values of sl50% , sl70% , sl80% , sl90% , sl95% , sl100% , sl105% at planning , halfway ( fraction 15 ) , and at end therapy ( fraction 30 )  . 
1 correlation between the volume variation of sl receiving 95% of the prescribed dose ( ( cid : 2 ) sl95% ) at treatment midpoint ( ( cid : 2 ) sl95% , fr15 ) and end ( ( cid : 2 ) sl95% , fr30 ) strahlenther onkol ( 2020 ) 196 : 243251 fig . 
2 patients sl variations ( cc ) receiving 95% of prescription dose ( ( cid : 2 ) sl95% ) at treatment midpoint ( black ) and end ( grey ) , according to the experienced toxicity fig . 
a , c 95% isodose ( corresponding to 62.7 gy ) , b , d dose recalculated on ct30def correlation between ( cid : 2 ) sl95% and treatment parameters when considering the three classes of patients ( positive changes , negative changes , no changes ) , some regular patterns which were detected could explain the observed variation . 
interestingly , the patient with the largest ( cid : 2 ) t value ( 40 days compared to mean / interquartile range values equal to 21 and 1525 days ) was the one with the largest ( cid : 2 ) sl95% positive value , appearing as an outlier strahlenther onkol ( 2020 ) 196 : 243251 fig . 
4 between patients with g0 / g1 and g2 / g3 toxicity concerning planning / half / end of therapy . the association is signicant in the range of approximately 5064 gy , with no important differences between the three timings patient against ( cid : 2 ) t ; results are shown in the supplementary material ( figure s1 )  . 
4 , both planning and therapy dvhs of patients with g2 / g3 toxicity were signicantly different compared to those of patients with g0 / g1 toxicity in the range 5064 gy , without any difference between the three timings as shown by fig . 
5. interestingly ( see supplementary material ) , negative variations at therapy midpoint and end for dose values around sl95% were associated with an increased risk of toxicity , although with a higher p - value compared to dvhs . 
firstly , it is important to underline that the convolution / superposition algorithm implemented in the accuray tomotherapy planning system is known to be highly accurate , with reported local discrepancies between measured and calculated values generally well within 5% in the rst few millimeters from the body contour [ 17 , 27 ]  . 
interestingly , one study on in vivo skin dosimetry reported larger uncertainty and the tendency to have systematic underdosing during therapy [ 28 ] , consistent with the prevalent skin dose - sparing effect reported in our work . in addition , we recently investigated the impact of dose calculation uncertainty in the rst few millimeters from body surface [ 32 ]  . 
of note , the component of the residual error ( after bony match correction ) due to some lack of immobilization and / or to the matching uncertainty should be much smaller than the component due to anatomical deformations . the study tried to quantify the skin dose variations during therapy . 
the arbitrary denition of sl95% as a good surrogate for skin dose variation comes from the evidence that skin dose toxicity is expected to be correlated with high daily doses . the initial hypothesis was to detect positive variations that could benet from skin - sparing art replanning . 
skin 250 strahlenther onkol ( 2020 ) 196 : 243251 dose variations effectively occurred during the tomotherapy treatment of hnc patients treated with a sib approach . these changes depended on ptv dimension , shape , and proximity to the skin , while they did not depend on the time between planning ct and therapy . the dvh of sl was seen to change signicantly in approximately half of patients due to anatomical modications . 
the results showed that few patients experienced a dose increase ( in terms of ( cid : 2 ) sl95% : 6% ) , while most changes were negative ( 47% )  . 
this result , apparently counterintuitive , was quantied for the rst time , and may mostly be explained by the way plan optimization works to deliver the dose to the portion of ptv next to the skin fact , in case of supercial ptv , the tomotherapy tps provides a full coverage of ptv , even in the rst layers of skin , altering uences in the non - electronic equilibrium region [ 15 , 27 ]  . 
this is here suggested as the main reason why many patients experienced a skin - sparing effect during rt : the sl of many patients received less dose during therapy compared to the planned one , because the uence patterns compensating for the lack of electronic equilibrium were mostly outside the actual body shape due to the shrinkage of body contours , as shown in fig . 
3. very importantly , this phenomenon involves only the very rst few millimeters from body outline , leaving substantially unaltered the dose delivered at depths larger than 23 mm ; consequently , the reported effect is not expected to have relevant impact on the dose received by the ctv ; however , this is not the purpose of the current work and may merit further investigation . this effect is not particular to tomotherapy , and may in principle also occur with other systems , if specic actions to limit the skin dose without increasing the risk of missing the target ( for instance using virtual bolus during plan optimization [ 31 ] ) are not planned . interestingly , a recently published study by a french consortium of centers reporting results for hnc patients treated with the same clinical protocol [ 3 ] showed a signicantly higher incidence of severe acute skin toxicities when delivering the treatment with tomotherapy compared to volumetric arc techniques using virtual bolus approaches , which is consistent with higher dose to skin due to the unavailability of tools ( like virtual boluses ) able to spare the skin without increasing the risk of missing portions of the ctv during treatment delivery . another signicant result of our study is the clear association between the risk of acute toxicity and the planning dvh of sl , to our knowledge quantied here for the rst time . 
the extension of current results to a wider population was important to assess constraints that could be applied to spare the skin for the patients at risk without introducing the additional ( nontrivial ) risk of underdosing the tumor [ 32 ]  . quite interestingly , the trend for skin dose changes with respect to planning is likely to be detected at the rst fraction . 
prada1 juan cardenal1 ana garca blanco1 jon andreescu1 mara ferri1 javier anchuelo1 ivan diaz de cerio1 nicolas sierrasesumaga1 andrs vzquez2 maite pacheco2 samuel ruiz arrebola2 received : 9 april 2019 / accepted : 25 november 2019 / published online : 15 january 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract background this study aimed to evaluate the outcomes and the toxicity of focal high - dose - rate ( hdr ) brachytherapy in selected localized prostate cancer patients . methods fifty patients were treated with focal high - dose - rate brachytherapy between march 2013 and november 2017 , representing 5% of the cases treated by our group during this period . 
valdecilla s / n , 39008 santander , cantabria , spain 2 department of radiation physics , hospital universitario marqus de valdecilla , santander , cantabria , spain ( cid : 2 ) pedro j . 
der mittlere anfngliche psa betrug 6 , 9 ng / ml ( spanne 1 , 913 , 4 ng / ml )  . bei der letzten nachuntersuchung betrug der mittlere psa - wert 3 ng / ml ( spanne 0 , 488 , 11 ng / ml )  . schlussfolgerung die fokale hdr - brachytherapie bei ausgewhlten patienten mit prostatakrebs mit niedrigem mittlerem risiko knnte hinsichtlich des rckfallfreien berlebens die gleichen befriedigenden ergebnisse erzielen wie die herkmmliche gesamt - prostata - brachytherapie ohne toxizitt . schlsselwrter fokale brachytherapie hohe dosisrate prostatakarzinom toxizitt ergebnisse background standard whole - gland prostate therapy , such as radical prostatectomy , external beam radiation , and brachytherapy , was mainly based on the large experience gathered by the detailed pathological analysis of prostatectomy samples . 
this analysis had shown that preoperative biopsies often underestimate the real prostatic tumor involvement . in a signicant proportion of cases , the removed prostate showed at times important foci of carcinoma in areas where biopsies had failed to show any tumor involvement . focal therapy was introduced with the aim of reducing the morbidity associated with standard whole - gland treatment , and based on the concept of treating the index or largest tumor representing more than 90% of the total tumor volume and assuming that the selective destruction of this lesion would thus prevent cancer progression . 
moreover , several authors have reviewed the percentage of unifocal tumors in prostatectomy cases and reported a 1338% rate of unifocal lesions [ 5 ]  . focal prostate therapies could reasonably be expected to bring a number of advantages : ( cid : 2 ) they will overcome the limitations of active surveillance , when it is not accepted psychologically by some patients . ( cid : 2 ) they may provide a reasonable answer to accusations of overtreatment , when the tumor involvement is limited . ( cid : 2 ) focal therapy is associated with no toxicity to noncancerous tissue and spares key structures , such as the neurovascular bundles and the external urinary sphincter . ( cid : 2 ) another advantage of this approach is the possibility of re - treatment ( brachytherapy , specic techniques of external irradiation , or salvage surgery )  . most authors advise to only offer this treatment a carefully selected subpopulation among low - risk localized prostate cancer patients . 
but recent paper presenting focal therapy as future treatment for prostate cancer [ 6 , 7 ]  . a number of techniques have been proposed ( cryotherapy , high - intensity focused ultrasound , photodynamic therapy , laser - activated nanoparticles , and focal brachytherapy )  . the hospital universitario marqus de valdecilla ( humv ) , focal hdr brachytherapy was initiated in march 2013 , according to a protocol approved by the ethics committee , with all patients required to sign an informed consent . in the present article , we report our preliminary results on the rst 50 patients who were treated with a focal highdose - rate brachytherapy by our group . materials and methods selection of patients fifty patients were treated between march 2013 and november 2017 . 
focal treatments thus represented only 5% of the total number of the implants performed . patients were staged according to the american joint committee on cancer 7th edition clinical staging guidelines [ 8 ] , using a directed history , physical examination , transrectal ultrasound ( trus ) , and multiparametric magnetic resonance imaging ( mp - mri )  . 
all patients underwent serum prostate - specic antigen ( psa ) determination and gleason score histological grading . patients with localized disease were further selected as follows : ( cid : 2 ) age 18 years . ( cid : 2 ) clinical stage t1c - t2a , n0 , m0 mri . ( cid : 2 ) prostate - specic antigen ( psa ) ( cid : 2 ) 15 ng / ml . ( cid : 2 ) gleason score less than or equal to 7 . ( cid : 2 ) unilateral disease . 224 table 1 patient and tumor characteristics ( n = 50 ) strahlenther onkol ( 2020 ) 196 : 222228 no . 
the mean prostatic volume at implantation was 39 ( 1080 ) cc . tumor characteristics are shown in table 1 . technique treatment all patients received one implant and one fraction of hdr . fraction dose was 24 gy . brachytherapy procedures were done under spinal anesthesia with the patient in the lithotomy position . 
axial cross - sections were captured in 5 - mm steps and transferred to the treatment planning software . prostate gland , normal structures ( urethra and rectum ) , and needle positions were identied and mapped based on the ultrasound image . 
dose optimization was done on the reconstructed applicator geometry using dose point and manual optimization algorithms to determine dwell positions and times . two treatment scenarios were considered in the focal brachytherapy setting : ( cid : 2 ) in patients with positive biopsies on the mri image tumor ( t2a by mri ) , the chosen volume to be treated was ultra - focal and brachytherapy , including the gross visible tumor on mri plus a margin to compensate for uncertainties in image registration and treatment delivery . 
this group represents 22% of the total ( 11 patients ) and the mean prostatic tumor volume considered for treatment was 9 ( 238 ) cc . ( cid : 2 ) in patients with unilateral positive biopsies but no visible tumor on the mri , the chosen volume to be treated was focal ( hemi - gland )  . 
this group represents 78% of the total ( 39 patients ) and the mean prostatic volume treated was 14 ( 530 ) cc . a double contour was performed ; the whole prostate rst and then the chosen volume to be treated . 
in the ultra - focal group using treatment planning systems to match and fuse the magnetic resonance image to the ultrasound image . the ultra - focal or focal volume was then dened as the planning target volume ( ptv ) to be treated with the prescribed dose ( pd )  . 
based on the dosevolume histogram ( dvh ) data , the quality of plans and implants was evaluated using following indicators : ( cid : 2 ) the rectal dose was calculated at the anterior edge of the trus probe and was limited to ( cid : 2 ) 75% of the prescription dose . ( cid : 2 ) the dose to any segment of the urethra was limited to ( cid : 2 ) 110% of the prescription dose . 
v120 and d100 of the prostatic urethra were determined ( volume that received a dose of 120% and dose delivered to 100% of the urethra )  . ( cid : 2 ) the ptv v90 , v100 , v150 , and v200 ( % of ptv receiving 90% , 100% , 150% , and 200% of the pd ) were recorded . ( cid : 2 ) d90 ( dose delivered to 90% of the ptv ) was calculated . strahlenther onkol ( 2020 ) 196 : 222228 table 2 dosimetric value of the target volume ( ptv ) v90 ( % ) v150 ( % ) v200 ( % ) d90 ( gy ) vi00 ( % ) mean median minimum maximum all patients were discharged from the center on the same results day of the procedure between 6 and 8 h of implantation . implant parameters follow - up follow - up visits were arranged at 4 weeks after completion of the treatment and every 4 months for the rst year , every 6 months for the second year , and yearly thereafter . 
the mean duration for transperineal implantation using a real - time technique was 60 min . dosimetric parameters urinary toxicity was evaluated using the ipss and the international continence score ( icq - sf )  . 
rectal toxicity was registered according to the national cancer institute common toxicity criteria . these questionnaires were lled out by the physician . the mean focal d90 in our series was 23 gy ( range 1626 gy )  . 
the maximum point doses in rectum and urethra were 17 and 25 gy , respectively ( table 2 )  . statistical considerations acute and chronic urinary toxicity descriptive statistical considerations include absolute and relative frequencies for categorical variables and the mean and standard deviation for quantitative variables . all patients tolerated the implantation procedure very well with minimal discomfort . 
biochemical failure was dened according to the phoenix denition [ 9 ] consensus panel statement . estimated likelihood of events was calculated by the kaplanmeier method from the time of completion of radiotherapy . 
no acute or late urinary retention was seen . at the same timepoints , the mean ipss scores and variations were not signicantly different between the groups with ultra - focal or focal treatment . when the icq - sf score was 0 at the end of the treatment , it remained nil thereafter at 1 and 2 years for all patients . slight increase in urinary irritation ( urethritis ) may occur in the days following the treatment , but disappears in the few days . no other chronic toxicity , such urethral narrowing , was observed after treatment . 226 strahlenther onkol ( 2020 ) 196 : 222228 fig . 
tfs tumor - free survival , os overall survival biochemical control local control at risk months sexual function erectile function was assessed at baseline and 17 ( 34% ) patients were identied as potent . 
of these patients , 14 were identied as potent at last follow - up , score was 22 ( 2224 )  . the other three patients had a very slight decrease of the mean iief5 ( score 19 )  . 
at 6 , 18 , and 24 months the mean iief5 registered was 14 , 13 , and 13 , respectively . lower gastrointestinal toxicity no rectal toxicity was reported at 3 , 6 , and 12 months . the 14 patients with a follow - up greater than 32 months also reported no rectal toxicity . 
psa decrease in all cases along 1 year . for the entire cohort of 50 patients , 7 had evidence of biochemical relapse , 5 had positive biopsies , and there were no deaths from prostate cancer ; 1 patient died of other illnesses . 
out of 5 patients with positive biopsies , three upgraded the disease to gleason 7 or more . biopsy control a systematic histologic follow - up is planned in our study , with post - implant biopsies to be performed after biochemical relapse ( patients systematically refuse to be biopsied )  . two patients had positive biopsies in previously negative contralateral lobes , revealing newly diagnosed cancers , and three patients had positive biopsies involving both lobes . 
in two patients with biochemical relapse , the treatment was ultra - focal . biochemical outcome the overall survival according to kaplanmeier estimates was 100% at 3 years and 92% ( 1% ) at 5 years . 
this focal therapy is associated with less toxicity to normal tissue and better quality of life , is an alternative to active surveillance when this is not accepted psychologically by some patients , and is a possible salvage treatment . 
we must also assess the possible benet strahlenther onkol ( 2020 ) 196 : 222228 of radiotherapy treatment , which can stimulate the immune system , and the fact that radiation is capable of inducing tumor - specic immunity or immunogenic cell death [ 10 ]  . these cytotoxic t cells circulate through the blood stream and are thus able to destroy remaining tumor cells in distant parts of the body which were not irradiated . 
as a result of this synergy , an effect is described at distant points , which is known as the abscopal effect . our report is the rst in the medical literature in patients with favorable - risk prostate cancer with hdr focal brachytherapy as monotherapy in one fraction of 24 gy . 
a few other groups have used focal low - dose - rate brachytherapy ( f - ldr - pb ) , but long - term outcomes are unknown [ 11 , 12 ]  . focal hdr brachytherapy is associated with encouraging outcomes . 
the present series represents the longest oncologic and functional follow - up of patients treated with this treatment for clinically unilateral , low intermediaterisk prostate cancer . in our series , seven patients had evidence of biochemical relapse , ve had positive biopsies . 
the treatment was ultra - focal in two patients . in our study , ipss , iief - 5 , and rectal toxicity data conrmed the minimal effect of f - hdr - pb . 
on the other hand , the psa decreased in all cases along 1 year ( the mean value dropped was 3.6 ng / ml )  . it is possible for f - ldr - pb to achieve similar results [ 13 , 14 ] , but f - hdr - pb with 192 - ir as monotherapy has a number of advantages . 
besides , hdr improves the dose distribution because of the possibility of accurately controlling the source and varying the source dwell time during treatment . the intraoperative optimization used with hdr allows better source position targeting with the potential for limiting toxicity . 
in addition , mri study after treatment is not impaired by the artifacts induced by the titanium shell of the seeds [ 15 ]  . cryotherapy is another possible focal treatment option for localized prostate cancer . 
when we review the results published in the literature , we observe a biochemical control between 71 and 98% , and an overall post - treatment positive biopsy rate between 8 and 25% . different series reported continence rates after cryotherapy at 96100% and the rates of erectile dysfunction varied between 0 and 42% . 
the operating theater time was less than one hour and a half in all our cases . the analysis of the pre - implant dosimetric parameters shows satisfactory focal constraints ( d90 , v90 , v100 , v150 , v200 , rectal dose , and urethral doses ) and could be achieved in all cases . a prudent comparison can be made between the urinary and the sexual toxicities observed in this preliminary series of 50 focal hdr brachytherapy patients and the ones registered in two previous series of 60 patients . 
for each of the series , the treatment by ( whole - gland ) high - dose - rate interstitial brachytherapy in one fraction of 19 and 20.5 gy , respectively , in the same institution by the same group suggests an advantage in terms of urinary toxicity and erectile function [ 16 , 17 ]  . our results conrm than hdr brachytherapy is currently possible to treat a well - dened partial prostatic volume with a high and precise dose . 
focal brachytherapy could stand as one of the best focal techniques to be proposed to carefully selected patients with very little tumor burden and could achieve the same results in terms of biochemical control as conventional whole - prostate hdr or ldr brachytherapy in selected patients , with less toxicity . 
another advantage of this approach is the possibility of salvage re - treatment with hdr brachytherapy , ldr brachytherapy , specic techniques of external irradiation , or salvage surgery . conclusion hdr focal brachytherapy in selected patients with low intermediate - risk prostate cancer could achieve the same satisfactory results in terms of relapse - free survival as conventional whole - prostate brachytherapy with less toxicity . 
noguchi m , stamey ta , mcneal je et al ( 2003 ) prognostic factors for multifocal prostate cancer in radical prostatectomy specimens : lack of signicance of secondary cancers . 
januar 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund die zugelassenen inhibitoren der cyclin - abhngigen kinasen 4 / 6 ( cdk4 / 6i ) palbociclib , ribociclib und abemaciclib verbessern das progressionsfreie berleben von patientinnen mit hormonrezeptor - positivem ( hrpos . ) , her2 - negativem ( her2 - neg . ) mammakarzinom in kombination mit einer endokrinen therapie deutlich . 
3 , 24105 kiel , deutschland ergebnisse das mediane os war im experimentalarm noch nicht erreicht und lag im standardarm bei 40 , 2 monaten , dieser unterschied war statistisch signikant ( hazard - ratio [ hr ] 0 , 71 ; p = 0 , 009073 )  . 
ein signikant verbessertes os wurde nur fr patientinnen gezeigt , die einen ai erhalten hatten , wobei die subgruppe der mit tamoxifen behandelten patientinnen nur ein viertel des gesamtkollektivs ausmachte . 
die einzige gruppe , die ein ergebnis zu ungunsten des experimentalarms zeigte , waren patientinnen mit einem progressionsfreien intervall von mehr als 12 monaten nach ende der vorangegangenen ( adjuvanten ) endokrinen therapie . 
der anteil der patientinnen , die 42 monate nach einschluss noch keine chemotherapie erhalten hatten , war im experimentarm mit 65 , 8 % signikant hher als im placeboarm ( 49 % ; hr 0 , 6 )  . 
vor einfhrung der cdki war bereits die kombination aus exemestan und everolimus als endokrin - basierte kombinationstherapie in der zweitlinie verfgbar . strahlenther onkol ( 2020 ) 196 : 286288 die cdki mit den vertretern palbociclib , ribociclib und abemaciclib erfreuen sich seit der markteinfhrung in den vergangenen jahren , basierend auf einer substanziellen pfs - verbesserung gegenber der alleinigen et in der palliativen erstund zweitlinientherapie , enormer beliebtheit . 
trotz einer hoch signikanten verbesserung des progressionsfreien berlebens und teils auch des gesamtberlebens durch hinzunahme der cdki zur endokrinen therapie wurde in der berwiegenden zahl der analysierten subgruppen kein zusatznutzen bescheinigt . 
durch die amerikanische arzneimittelbehrde fda wurde der pi3k - inhibitor alpelisib fr patientinnen mit pi3k - mutiertem mammakarzinom aufgrund der pfs - verbesserung in der solar - 1 - studie [ 3 ] bereits zugelassen . 
auch der parp - inhibitor olaparib ist durch die fda fr mammakarzinom - patientinnen mit brca - mutation , unabhngig vom hr - status , zugelassen worden [ 4 ]  . 
im rahmen einer phase - iii - studie wurde durch die kombination von fulvestrant + anastrozol ein signikanter os - vorteil von 7 , 9 monaten gegenber der monotherapie mit anastrozol trotz einer crossover - rate von 45 % . 
zum vergleich : in der hier vorgestellten studie waren es im ribociclib - arm allein > 60 % grad - iii / iv - neutropenien . aus strahlentherapeutischer sicht bleibt zu erwhnen , dass es bislang nur wenige erfahrungswerte zur kombination von cdki und palliativer bestrahlung gibt . 
thill m , jackisch c , janni w et al ( 2019 ) ago recommendations for the diagnosis and treatment of patients with locally advanced and metastatic breast cancer : update 2019 . 
cristofanilli m , turner nc , bondarenko i et al ( 2016 ) fulvestrant plus palbociclib versus fulvestrant plus placebo for treatment of hormone - receptor - positive , her2 - negative metastatic breast cancer that progressed on previous endocrine therapy ( paloma - 3 ) : nal analysis of the multicentre , double - blind , phase 3 randomised controlled trial . 
chowdhary m , sen n , chowdhary a et al ( 2019 ) safety and efcacy of palbociclib and radiation therapy in patients with metastatic breast cancer : initial results of a novel combination . 
figura nb , potluri tk , mohammadi h et al ( 2019 ) cdk 4 / 6 inhibitors and stereotactic radiation in the management of hormone receptor positive breast cancer brain metastases . 
the present study compared imrt alone with imrt in combination with chemotherapy in elderly npc patients . methods between january 2011 and december 2014 , 102 patients aged > 65 years with npc who received imrt alone ( imrt group ) or imrt in combination with chemotherapy ( imrt / ct group ) were enrolled . 
however , the incidences of grade 3 vomiting / nausea ( p = 0.000 ) , leukopenia / neutropenia ( p = 0.000 ) , thrombocytopenia ( p = 0.041 ) , and anemia ( p = 0.040 ) were signicantly higher in the imrt / ct group compared with the imrt group . 
no grade 4 toxicities were observed . conclusion imrt alone was similar to imrt / ct in treating elderly npc patients ( age > 65 years ) , with comparable survival outcomes and less grade 3 toxicities . keywords > 65 years intensity - modulated radiation therapy chemotherapy elderly patients nasopharyngeal carcinoma age ( cid : 2 ) wei jiang weijiang@glmc.edu.cn 1 department of radiation oncology , afliated hospital of guilin medical university , 15 lequn road , 541001 guilin , china 2 department of oncology , baise people hospital , 533000 baise , china 3 department of otolaryngology - head and neck surgery , afliated hospital of guilin medical university , 541001 guilin , china 4 department of oncology , nanxishan hospital of guangxi zhuang autonomous region , 541004 guilin , china 5 department of radiation oncology , wuzhou red cross hospital , 543002 wuzhou , china 6 department of radiation oncology , liuzhou general hospital , 545006 liuzhou , china strahlenther onkol ( 2020 ) 196 : 270279 vergleich zwischen intensittsmodulierter strahlentherapie allein und intensittsmodulierter strahlentherapie in kombination mit chemotherapie bei lteren patienten ( ber 65 jahre ) mit nasopharynxkarzinom zusammenfassung zielsetzung die wirksamkeit und vertrglichkeit einer zustzlich zur strahlentherapie durchgefhrten chemotherapie in einer zeit intensittsmodulierter radiotherapie ( imrt ) bleibt bei lteren patienten mit nasopharynxkarzinom ( npc ) umstritten . 
die vorliegende studie verglich imrt allein mit imrt in kombination mit einer chemotherapie bei lteren npc - patienten . methoden zwischen januar 2011 und dezember 2014 wurden 102 ber 65 jahre alte npc - patienten , die nur imrt ( imrtgruppe ) oder imrt in kombination mit chemotherapie ( imrt / ct - gruppe ) erhielten , in die studie einbezogen . 
die hugkeit von grad - 3 - erbrechen / belkeit ( p = 0 , 000 ) , leukopenie / neutropenie ( p = 0 , 000 ) , thrombozytopenie ( p = 0 , 041 ) und anmie ( p = 0 , 040 ) war allerdings in der imrt / ct - gruppe im vergleich zur imrt - gruppe jeweils signikant hher . 
es wurden keine grad - 4 - toxizitten beobachtet . schlussfolgerung die behandlung lterer npc - patienten ( ber 65 jahre ) war mit imrt allein hnlich wie mit imrt / ct , mit vergleichbaren berlebensergebnissen und weniger grad - 3 - toxizitten . intensittsmodulierte strahlentherapie chemotherapie ltere patienten nasopharynxkarzinom schlsselwrter alter > 65 jahre introduction nasopharyngeal carcinoma ( npc ) remains one of the most endemic cancers in southeast asia and southern china , with a high occurrence rate of approximately 3050 per 100 , 000 persons [ 1 , 2 ]  . 
radiotherapy ( rt ) alone is acceptable for treating early - stage npc [ 3 , 4 ] , but concurrent chemoradiotherapy ( ccrt ) is recommended for advanced npc [ 5 ]  . 
however , in most clinical trials , elderly patients ( aged > 65 years ) with npc were either excluded or accounted for only a few patients [ 68 ]  . 
thus , the optimal treatment schedule for elderly patients with npc remains unclear . in the era of two - dimensional rt , certain retrospective studies found that the addition of chemotherapy to conventional rt could improve survival rates of elderly npc patients [ 9 , 10 ] ; however , a low proportion of elderly npc patients ( aged > 65 years ) had received ccrt ( < 40% ) in these studies . 
therefore , the clinical features and prognosis of elderly npc patients could not have been accurately reected , and toxicities such as leukopenia and neutropenia were more common in the ccrt group , which is particularly concerning for elderly npc patients [ 11 , 12 ]  . 
moreover , there is a lack of prospective randomized trials to evaluate the effects of ccrt in elderly npc patients . since the development of imageology and rt techniques , several studies have found that chemotherapy in combination with rt is not superior to rt alone during early or advanced stages of npc . 
a study by sun [ 14 ] in china showed that patients who received imrt alone had similar 5 - year dss , lrrfs , relapse - free survival ( rfs ) , dmfs , and progression - free survival ( pfs ) rates compared to those who received imrt in combination with chemotherapy for locoregionally advanced npc patients . 
on the other hand , lin [ 15 ] reported that imrt in combination with chemotherapy offered no signicant survival benets compared to imrt alone , with similar os rates but lower dmfs and dfs rates . 
this could also 272 strahlenther onkol ( 2020 ) 196 : 270279 help establish the standard schedule of imrt for elderly patients with npc . based on these considerations , the present study was conducted with the aim to evaluate the efcacy of imrt in combination with chemotherapy versus imrt alone in terms of survival and toxicity among elderly npc patients ( aged > 65 years )  . treatment all patients from both groups received imrt , which was delivered using 6 mev linear accelerators . 
clinical target volumes ( ctvs ) included high - risk areas ( ctv1 ) such as sites from 0.81 cm outside the gtv , potential local inltration areas which require prophylactic irradiation , and low - risk areas ( ctv2 ) such as the entire nasopharyngeal cavity , clivus , parapharyngeal space and skull base , sphenoid sinus , and pterygoid fossae and lymph node draining area . 
irradiation was performed ve times a week at 2.02.2 gy per fraction per day for 67 weeks . during induction or adjuvant chemotherapy , patients received 12 cycles of uorouracil ( 600800 mg / m2 on days 15 ) or paclitaxel ( 135 mg / m2 on day 1 ) plus cisplatin ( 25 mg / m2 on days 13 )  . 
during concurrent chemotherapy , patients received single cisplatin ( 75 mg / m2 on day 1 ) concurrently with rt every 3 weeks . follow - up and clinical assessment follow - up care for patients with npc included clinical examination , blood tests , and mri / intensive ct of the nasopharynx and skull base , recorded before and after treatment every 3 months for the rst 2 years , followed by every 6 months in the next 2 years , and annually thereafter . 
chest and liver ct scans or bone scans were performed to diagnose distance metastasis . tumor response rate was evaluated using the response evaluation criteria in solid tumors ( recist ) version 1.0. adverse events were evaluated according to the common terminology criteria for adverse events ( ctcae ; version 4.0 ) , and rt - related toxicities were evaluated using the radiation morbidity scoring criteria of the radiation therapy oncology group . statistics the primary endpoint was overall survival ( os ) , calculated as the time from the day of diagnosis to the day of death from any cause or censored at the latest follow - up . 
secondary endpoints were disease - free survival ( dfs ) , locoregional relapse - free survival ( lrrfs ) , and distant metastasis - free survival ( dmfs ) , calculated as the time from the day of diagnosis to the day of relapse , distant metastasis , or patients and methods patients this was a multicenter retrospective study conducted in southern china . 
we reviewed records of 1272 consecutive patients between january 2011 and december 2014 from the digital hospital database of four radiation oncology institutions in china : afliated hospital of guilin medical university , wuzhou red cross hospital , nanxishan hospital of guangxi zhuang autonomous region , and liuzhou general hospital . 
eligibility criteria were patient age > 65 years , newly diagnosed , nonmetastatic ( m0 ) , measurable , histologically conrmed npc , and eastern cooperative oncology group ( ecog ) performance status ( ps ) of 02 . 
written informed study consent was obtained from all participants , and the study protocol was approved by individual research ethics committees at all four institutions . elderly patients ( aged > 65 years ) treated with the imrt alone regimen ( imrt group ) were matched to those treated with imrt combined with chemotherapy regimen ( imrt / ct group ) in a 1 : 1 ratio . 
overall , data of 51 elderly npc patients who received imrt alone were collected from the four radiation oncology institutions between january 2011 and december 2014 , and elderly npc patients ( with similar conditions ) who received the imrt / ct regimen were enrolled into a matching control group from the data registry of the four institutions during the same period . 
all factors had to be matched between two matched patients ; if an exactly matched patient was unavailable , the matching criteria would be extended until the right one was found . 
finally , 51 patients who received imrt / ct were included in the matching control group . the npc patients underwent disease staging according to the seventh edition of the american joint committee on cancer ( ajcc ) staging system . strahlenther onkol ( 2020 ) 196 : 270279 death from any cause ; the time from the day of diagnosis to the day of relapse ; the time from the day of diagnosis to the day of distant metastasis or death ; respectively . 
for the purpose of analysis , the chi square test and fishers exact test were applied to evaluate associations between patients clinical characteristics between the imrt group and the imrt / ct group . 
moreover , 95 ( 91.1% ) had a ps score of 01 ; 97 ( 95.1% ) patients had histological conrmation of non - keratinization undifferentiated carcinoma ; 39 ( 38.2% ) had t4 stage npc , 36 ( 35.2% ) had t3 stage npc , 63 ( 61.8% ) had n2 stage npc , and 19 ( 18.6% ) had n1 stage npc . 
baseline characteristics were balanced between the groups ( table 1 )  . treatment and compliance all patients were treated with imrt on schedule without a break ; of the 51 patients in the imrt / ct group , 17 ( 33.3% ) received induction chemotherapy ( ic ) plus ccrt , 13 ( 25.5% ) patients received ic plus imrt alone , 19 ( 37.2% ) received ccrt , and 2 ( 4.0% ) patients received ccrt plus adjuvant chemotherapy . 
overall , 29 ( 56.9% ) patients from the imrt / ct group had a chemotherapy treatment delay ( no more than 2 weeks ) because of severe leukopenia / neutropenia and vomiting / nausea . response and survival at 3 months after treatment completion , rates of complete remission ( cr ) in both groups were 100% . 
with a median follow - up of 43 months , disease progression was observed in 17 patients ( 33.3% ) from the imrt group ; among them , 4 ( 7.8% ) patients revealed locoregional recurrence and 13 ( 25.5% ) had distant metastases . 
in the imrt / ct group , disease progression was observed in 16 ( 31.4% ) patients ; among them , 1 ( 2.0% ) patient had locoregional recurrence and 15 ( 29.4% ) patients had distant metastases . 
no statistically signicant differences were observed in skin reactions ( radiation - related ) , mucositis ( radiationrelated ) , and dry mouth between both groups ( p > 0.05 ; table 3 )  . 
there were no reports of nephrotoxicity , hepatotoxicity , or grade 4 acute toxicity in either group . multivariate analysis univariate analysis revealed that t stage ( p = 0.016 ) and tnm stage ( p = 0.019 ) were signicant prognostic factors for dfs . 
the results are summarized in table 5 . discussion given the increase in the aging population in china , the burden of npc is increasing [ 9 , 17 ]  . 
according to the development of radiation technology from two - dimensional conventional radiotherapy ( 2d - rt ) to three - dimensional conformal radiotherapy ( 3d - crt ) and intensity - modulated radiation therapy ( imrt )  . 
imrt was associated with a significantly lower incidence rate of toxicity than 3drt ; however , no statistically signicant differences were found in terms of survival rate between imrt and 3dcrt [ 18 , 19 ]  . 
moreover , the standard schedule of imrt for elderly patients with npc has not been established yet , and two - dimensional rt in combination with chemotherapy can produce high toxicity [ 20 ]  . 
in the era of imrt , whether the addition of chemotherapy to imrt could further improve survival remains uncertaoncologists should carefully balance the advantages and disadvantages of imrt in combination with chemotherapy in elderly npc patients [ 21 ]  . 
taken together , factor age ( years ) 6570 7175 male female t category t12 t34 n category n01 n23 tnm stage iiiii stage ivaivb stage strahlenther onkol ( 2020 ) 196 : 270279 these ndings indicate that the imrt alone regimen has similar survival efcacy to the imrt / ct regimen in elderly npc patients . we would continue to report the 5 - year survival outcome of elderly patients who received different chemotherapy regimens in the crt group . in the era of two - dimensional rt , numerous studies demonstrated the survival benets of ccrt as the treatment of choice for elderly npc patients [ 12 , 2426 ] ; however , in the present study , the imrt alone regimen was noninferior to the imrt / ct regimen as rst - line treatment in terms of survival benets for elderly npc patients . 
first , the statistically signicant survival benets achieved with the imrt / ct regimen could be primarily attributed to the modality of two - dimensional rt ; also , with the progress of imageology and rt techniques , imrt has greatly enhanced treatment effects of npc [ 27 , 28 ]  . 
second , in the two - dimensional rt era , most studies included a larger proportion of patients aged 6065 years [ 24 , 29 ] ; with considerable tolerance , such patients could have received sufcient doses of chemotherapy and may have beneted more from the ccrt regimen . 
however , patients aged > 65 years may have received less cycles or lower doses of chemotherapy owing to poor tolerance and , thus , the effects of chemotherapy would have been decreased [ 9 ]  . 
thus , the imrt / ct regimen did not improve survival of elderly npc patients compared to the imrt alone regimen possibly because of the development of rt technology , which was used in both treatment groups , and a decline in organ function of elderly patients , necessitating lowering of chemotherapy cycles or doses administered . some aspects in our research were worth to be considered . 
as to an impact of heterogeneity among the chemotherapy protocols in this study , some reports demonstrated that survival benet in different treatment modes , such as concurrent chemoradiation with induction chemotherapy , concurrent chemoradiation with adjuvant chemotherapy , concurrent chemoradiation , are similar , but differed in toxicity [ 3133 ]  . 
whats more , in terms of toxicities , the incidence of hematologic toxicities such as thrombopenia and neutropenia and nonhematologic toxicities such as vomiting / nausea and anemia was higher in the imrt / ct group . 
given the metabolic changes in elderly patients , the more comorbidities they have , the more severe treatment - related toxicities they suffer [ 10 ] ; moreover , decrease in organ function has an impact on the pharmacokinetics of chemotherapeutic agents , thus making toxicities less predictable [ 35 ]  . 
in europe indicated that an increase in toxicities was closely associated with worsening of prognosis in elderly cancer patients [ 36 ]  . the imrt alone regimen could be an alternative treatment option for elderly npc patients ( > 65 years ) , particularly for male patients or patients with a poor physical condition . based on results of the present study , we recommend that imrt alone could be economical and effective ( with lesser toxicities ) for treatment of elderly patients with npc . to our knowledge , this is the rst study to compare efcacy and toxicity between imrt combined with chemotherapy and imrt alone in elderly patients with npc . 
first , this is a retrospective study , which may have led to potential biases . second , the follow - up duration was short and the sample size was small . 
despite study limitations , the results of this study still revealed that addition of chemotherapy to imrt did not provide any signicant survival benets for elderly npc patients . conclusion in our trial , no signicant differences were noted between imrt alone and imrt / ct regimens in terms of survival outcomes of elderly patients with npc ( age > 65 years ) ; however , the incidence of grade 34 acute toxicities was lower with the imrt alone regimen . 
the aim of this study was to compare the cinsarc signature of preand posttreatment biopsies of sarcoma patients treated within a phase i trial evaluating preoperative sunitinib and irradiation . methods we retrieved 14 pairs of formalin - xed parafn - embedded blocks from pretreatment biopsies and posttreatment resection specimens and performed expression proling of the 67 cinsarc signature genes . results in 5 / 14 patients , both probes were unsuitable for expression analysis because there was no ( vital ) tissue left in biopsies or resection specimens . 
comparing the cinsarc risk classication before and after treatment in the remaining patients , 2 / 9 shifted from a highto a low - risk classication for metastatic disease after preoperative treatment with radiation therapy plus sunitinib and 7 / 9 pairs of preand posttreatment biopsies revealed identical results . conclusion concurrent radiation therapy and sunitinib leads to diverging results of prognostic gene array testing in a relevant proportion of sarcoma patients . 
ziel dieser studie war es , zu untersuchen , inwieweit eine properative therapie mit bestrahlung und sunitinib einuss auf das cinsarc - ergebnis hat . methoden in 14 korrespondierenden paaren von formalinxierten und parafneingebetteten tumorproben ( prtherapeutische biopsie und posttherapeutisches resektat ) erfolgte die expressionsanalyse der 67 cinsarc - signaturgene . ergebnisse bei 5 / 14 probenpaaren war ein vergleich der cinsarc - signatur nicht mglich , da nach diagnostischer aufarbeitung bzw . 
diese unterschiede knnen auf therapieeffekte oder tumorheterogenitt zurckgefhrt werden und sollte bei der probenauswahl und testinterpretation von prognostischen signaturen bercksichtigt werden . schlsselwrter weichgewebesarkom strahlentherapie sunitinib adjuvante chemotherapie biopsie introduction soft tissue sarcomas ( sts ) are rare malignant tumors . 
however , preliminary results from a randomized trial of the european organization for research and treatment of cancer ( eortc ) show that intraabdominal recurrence - free survival may not be improved by preoperative irradiation in all retroperitoneal sts subtypes ( clinicaltrials.gov identier : nct01344018 )  . 
metaanalyses of randomized trials demonstrated a trend towards improved survival , while the most recent and largest trial did not demonstrate a survival advantage in the chemotherapy group [ 4 , 5 ]  . 
the reason for these negative results in randomized chemotherapy trials is most probably a failure to select only patients with a relevant risk for metastatic disease . cinsarc ( complexity index in sarcomas ) is a gene expression signature comprising 67 genes which are involved in mitotic control and chromosomal integrity [ 6 ]  . cinsarc straties into low ( c1 ) and high ( c2 ) risk for metastatic disease and death , and outperforms fdration nationale des centres de lutte contre le cancer ( fnlcc ) histological grade as a prognostic factor for soft tissue sarcomas [ 79 ]  . 
cinsarc or other gene signatures may thus be suitable to serve as selection criteria for a risk - based recommendation for adjuvant chemotherapy . the combination of rt with targeted agents or immunotherapy may increase treatment efcacy [ 10 ]  . 
radiation therapy alone and in combination with systemic treatment as administered within the gisg 03 trial may have a relevant impact on the expression of genes included in prognostic signatures such as cinsarc [ 14 ]  . 
the aim of this study was to compare the cinsarc prognostic signature before and after neoadjuvant radiation therapy plus sunitinib in soft tissue sarcoma . methods the protocol and results of gisg 03 have been published in detail previously [ 11 , 13 ]  . 
the gisg 03 study was approved by the ethics committee ii of the university of heidelberg , germany , and the german federal institute for drugs and medical devices ( bfarm )  . the study demonstrated that combined sunitinib and rt was tolerable for locally advanced sts patients regardless of tumor location . 
an additional cohort of sts patients 282 strahlenther onkol ( 2020 ) 196 : 280285 strahlenther onkol ( 2020 ) 196 : 280285 was treated according to the gisg 03 protocol but not included into the trial due to inclusion criteria ( e.g. , local recurrence , solitary , metastatic disease , or second malignancy ) [ 12 ]  . 
pairs of parafn blocks from pretreatment biopsy and posttreatment resection specimens were retrieved . methods of rna extraction and expression quantication have been described in detail previously [ 68 ]  . 
the detailed including protocol for mrna transcript quantication , sample preparation , hybridization , detection , and scanning , followed the manufacturers recommendations , using the ncounter prepstation ( nanostring , amersham , uk ) and ncounter digital analyzer ( nanostring )  . 
1 workow for formaldehyde - xed parafn - embedded tissue ( ffpe ) blocks of biopsies and resection specimens results we retrieved formaldehyde - xed parafn - embedded tissue ( ffpe ) blocks of 14 patients treated with preoperative rt and sunitinib . 
in both cases , the amount of 284 strahlenther onkol ( 2020 ) 196 : 280285 rna was too small for further analysis and they were excluded from the following analysis . 
only the rst may be avoided by biopsy sops that include the withholding of tumor tissue for gene expression analysis . in general , there was a good correlation of the expression of the 67 cinsarc genes in biopsies and resection specimen . 
nevertheless , two patients shifted from a high risk ( biopsy ) to a low risk ( resection ) for metastases when classied according to cinsarc ( supplementary le 1 )  . these differences in gene expression and the risk classication may be attributed to tumor heterogeneity . 
the evaluation of a comparable prognostic gene signature using posttreatment samples in gastric cancer also points to a signicant inuence of systemic therapy on test validity [ 15 ]  . 
this question needs to be answered by larger trials . in conclusion , this translational study demonstrates that preoperative treatment with rt and sunitinib may have a relevant impact on gene expression and risk classication by the cinsarc prognostic gene signature . 
although randomized trials did not prove the efcacy of adjuvant chemotherapy for all sts patients , recent data suggest that patients with a high risk of recurrence prot from adjuvant chemotherapy [ 16 ]  . 
routine clinical parameters summarized in prognostic nomograms may be used additionally to calculate the risk for recurrence and guide the decision for adjuvant treatment [ 16 , 17 ]  . acknowledgements gisg03 was designed at the eortc / aacr workshop at flims , switzerland . funding this research was funded by the german research foundation ( grant ja 2030 / 1 - 1 ) and the ruprecht karl university of heidelberg , germany . compliance with ethical guidelines conict of interest j . 
le guellec declare that they have no competing interests . ethical standards the gisg 03 study was approved by the independent ethics committee ii of the university of heidelberg , germany , and the german federal institute for drugs and medical devices ( bfarm )  . all procedures performed in this study were in accordance with the ethical standards of the institutional research committee and with the 1975 helsinki declaration and its later amendments . 
september 2020 der / die autor ( en ) 2020 ziel der arbeit das auftreten einer spten kardiotoxizitt im zusammenhang mit strahlentherapie bei brustkrebs und hodgkin - lymphom ist gut bekannt . 
fr diese publikation wurden die inzidenz , der beginn und die langzeitberlebensresultate von hochgradigen kardialen ereignissen untersucht , die nach strahlentherapie in einer groen kohorte von patienten mit sophaguskarzinom auftraten [ 2 ]  . patientengut und methode zwischen mrz 2005 und august 2017 wurden 479 patienten mit sophaguskarzinom aus einer prospektiven institutionellen datenbank am md anderson cancer center in houston analysiert . 
ausgewertet wurde jedes grad3 ( g3 ) oder hhergradige ( g3 + ) kardiale ereignis gem ctcae , version 5.0. ergebnisse kardiale g3 + - ereignisse traten bei 18 % der patienten im median nach 7 monaten auf bei einer medianen nachbeobachtungszeit von 76 monaten . 
vorbestehende herzerkrankung ( p = 0 , 001 ) und bestrahlungsmodalitt originalpublikation wang x , palaskas nl , yusuf sw , abe j - i , lopez - mattei j , banchs j , gladish gw , lee p , liao z , deswal a , lin sh ( 2020 ) incidence and onset of severe cardiac events after radiotherapy for esophageal cancer . 
darber hinaus waren herzereignisse g3 + mit einem schlechteren gesamtberleben verbunden . schlussfolgerungen der autoren schwere kardiale ereignisse waren relativ hug mit einem frhen ausbruch bei sophaguskarzinompatienten nach strahlentherapie assoziiert , insbesondere bei patienten mit bereits bestehenden herzerkrankungen und hheren strahlendosen im herzen . es sollten optimale behandlungsanstze gewhlt werden , um die kumulativen dosen auf das herz , insbesondere bei patienten mit vorbestehender herzerkrankung , zu reduzieren . kommentar krzlich wurde die erste randomisierte studie publiziert , die protonen vs . 
hier zeigte sich ein vorteil der protonentherapie in den kumulativen gewichteten toxizitten und postoperativen komplikationen [ 1 ] , der berwiegend auf die reduktion der postoperativen kardialen und pulmonalen komplikationen nach der protonentherapie zurckzufhren zu sein schien . 
der primre endpunkt , kardiale ereignisse g3 + , wurde nach ctcae klassiziert und enthielt arrhythmien , herzstillstand , 1140 strahlenther onkol ( 2020 ) 196 : 11391141 bei einer tumorart , in der hnlich wie beim lungenkarzinom ein hoher prozentsatz der patienten eine oder mehrere kardiale vorerkrankungen aufweist , haben diese daten eine sehr groe bedeutung . 
die autoren der hier kommentierten arbeit empfehlen , eine mittlere herzdosis von maximal 15 gy einzuhalten . fazit es handelt sich um eine der grten studien zu den schweren kardialen ereignissen nach strahlentherapie des sophaguskarzinoms und die erste , die einen vergleich zwischen der strahlentherapie mit protonen und denen nach imrt anstellt . 
krause gibt an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . herzinsufzienz , akute koronarereignisse , perikarditis und perikarderguss . 
patienten nach imrt hatten ein signikant hheres risiko , ein kardiales ereignis g3 + zu erleiden , im vergleich zu patienten nach protonentherapie ( hazard ratio [ hr ] = 1 , 746 ; 95 % - ci 1 , 0652 , 862 ; p = 0 , 027 )  . 
in der analyse der dosimetrischen daten waren univariat die v5gy und die mittlere herzdosis , multivariat die mittlere herzdosis signikant mit g3 + kardialen ereignissen vergesellschaftet ( hr = 1 , 034 ; 95 %ci , 1 , 0061 , 062 ; p = 0 , 015 )  . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf 1 . 
wang k et al ( 2017 ) cardiac toxicity after radiotherapy for stage iii non - small - cell lung cancer : pooled analysis of dose - escalation trials delivering 70 to 90 gy . 
sarria3 received : 14 june 2020 / accepted : 27 july 2020 / published online : 20 august 2020 the author ( s ) 2020 abstract background the covid - 19 pandemic outbreak has set the emergency services in developing countries on major alert , as the installed response capacities are easily overwhelmed by the constantly increasing high demand . 
the decit of intensive care unit beds and ventilators in countries like peru is forcing practitioners to seek preventive or early interventional strategies to prevent saturating these chronically neglected facilities . case presentation a 64 - year - old patient is reported after presenting with covid - 19 pneumonia and rapidly progressing to deteriorated ventilatory function . 
compassionate treatment with a single 1 - gy dose to the bilateral whole - lung volume was administered , with gradual daily improvement of ventilatory function and decrease in serum inammatory markers and oxygen support needs , including intubation . 
procedures of transport , disinfection , and treatment planning and delivery are described . conclusion whole - lung low - dose radiotherapy seems to be a promising approach for avoiding or delaying invasive respiratory support . 
on - going prospective trials will elucidate the effectiveness of this approach . keywords covid - 19 low - dose radiotherapy viral pneumonia intensive care cytokine storm introduction the coronavirus disease 2019 ( covid - 19 ) pandemic outbreak in late 2019 eventually imposed upon developing countries a major problem for public health systems , due to a lack of installed attention capacity [ 1 ]  . 
examples from european countries such as spain or italy , who saw their emergency and hospitalization systems rapidly overwhelmed despite a greater response capacity [ 2 ] , raised major concern in latin american countries . 
despite these efforts and as of may 25 , the contagion incidence curves seem to still be increasing , with an average of more than 4000 new cases daily since the rst ofcial case was reported on march 6 [ 3 , 4 ]  . currently , in light of the lack of evidence for a specic or effective medical treatment , hospitaland especially intensive care unit ( icu ) - based support management have been left as the only options for the expected 5% of advanced cases [ 5 ]  . 
according to this and in addition to the previously described situational features , the fragile balance between patients admission and attention capacity should be approached from a preventive perspective . the anti - inammatory effect of low - dose radiotherapy ( ld - rt ) was tested for infectious respiratory conditions in former times ; however , this practice fell into decline after the advent of medical treatments [ 6 ]  . 
pre - clinical and clinical data regarding toxicity and effectiveness of such treatstrahlenther onkol ( 2020 ) 196 : 10861093 1087 ments have been published , showing an acceptable safety prole [ 7 ]  . herein , we present the case of a patient treated at our institution , describe the followed biosecurity and disinfection protocol , and review the available evidence regarding this topic published to date . case description we here report on a 64 - year - old male patient with a prior history of pulmonary tuberculosis successfully treated in 1975 . 
after rapid worsening of symptoms and onset of dyspnea , he presented in the emergency department , where covid - 19 was conrmed by polymerase chain reaction ( pcr )  . 
baseline vital signs were : heart rate ( hr ) 93 bpm , respiratory rate ( rr ) 22 bpm , temperature ( t ) 37.7 c , blood pressure 133 / 93 mm hg , oxygen saturation level ( spo2 ) 89% . oxygen support therapy was started with a non - rebreather mask at 10 l / min output ( fio2 100% ) pa / fio2 193 , with immediate spo2 improvement to 99% . 
chest ct scan revealed a bilateral multifocal ground - glass pattern , with a predominant central and subpleural component . type i respiratory insufciency secondary to the viral infection was diagnosed and multidrug treatment including ceftriaxone 2 g intravenous ( iv ) 24 h , hydroxychloroquine 400 mg per oral ( po ) twice daily ( bid ) rst day , then 200 mg po bid for 10 days , azithromycin 500 mg po rst dose , then 250 mg po per day for 10 days , and enoxaparin 60 mg subcutaneous ( sc ) per day was started . 
daily laboratory and arterial blood gas ( abg ) analyses from therapy installation are summarized in tables 1 and 2 . during the second day of hospitalization , the dyspnea worsened further and was present at rest . 
a 1 - gy prescription was opted for and planning with the vmat technique was performed . procedure duration included 10 min of patient positioning , 1 : 20 min cbct imaging verication , and 1 : 30 min beam - on time . 
medical therapy was intensied with hydroxychloroquine 400 mg bid and azithromycin 500 mg bid ; additionally , the enoxaparin dose was intensied ( 60 mg sc bid )  . three days after rt ( sixth hospitalization day ) , the patient showed improvement in respiratory patterns and a persistent , although ameliorated , cough . 
abg parameters showed pao2 90.5 mm hg and pa / fio2 226.25. seven days after treatment the patient was discharged from the icu to continue management in a lower - complexity area . 
in addition , the target coverage and oar dosimetry details can be seen in table 3 . literature review and discussion this rst reported case to our knowledge in our country and the region raises the question of the effectiveness of rt to treat covid - 19 pneumonia patients . 
lessons obtained from preclinical and clinical studies , the former performed for the rst time over 100 years ago , have already established the basis for this treatment modality [ 11 ]  . 
on the contrary , no greater difference was observed with exposure after 48 h , suggesting a major improvement in cytokine release syndrome ( crs ) regulation with early treatment onset [ 12 , 13 ]  . 
a more recent investigation assessed the impact of a 1 - , 2 - , and 3 - gy single fraction in a murine model , in order to simulate the impact of radiation exposure in astronauts . 
after 2 - year followup , neither of the selected doses caused caspase - 3 overexpression nor ceramide species accumulation , which directly induce pneumocyte apoptosis and subsequent brosis [ 14 ]  . the radiobiological rationale for adopting rt as an approach to counteract crs encompasses a variety of mechanisms . 
covid - 19 severe acute respiratory syndrome ( sars ) pathogenesis is directly related to t helper 1 cell ( th1 ) activation , which subsequently initiate the dysregulated inammatory cascade through different factors such as granulocyte colony - stimulating factor ( g - csf ) , il - 6 , il - 7 , il - 10 , and tumor necrosis factor ( tnf - ) amongst others , and in addition to phagocytic activity , contribute to upregulating the cytokine storm [ 1517 ]  . 
an observed pattern in severe cases points to major damage to tissues expressing high concentrations of angiotensin - converting enzyme 2 ( ace2 ) , mainly type ii pneumocytes ; therefore , the reninangiotensinaldosterone cascade is consequently fig . 
evident worsening of the inammatory process can be observed ; however , a dissociation between these nding and the good clinical evolution of the patient is to be noted radiotherapy physics and planning considerations a chest ct scan with 2.5 mm thick slices was acquired for planning purposes , accounting for a total set of 143 images . the hands - up position was determined and non - forced expiration was intended . 
2 1 - gy isodose volume distribution and dosevolume histogram showing a conformal and homogeneous distribution prole on the desired target volume added as an extra factor by further activating macrophages and granulocytes and promoting continuous interstitial inammation [ 18 , 19 ]  . 
the anti - inammatory properties of rt include polarization of macrophages to an m2 phenotype ( leukocyte adhesion mediator ) , and downregulation of nitric oxide , tnf - , and tgf -  . 
besides , the upregulation of heme oxygenase , il - 10 , tnf - , nf , and apoptosis mechanisms , as well as t - regulatory cell enhancement , have been postulated as co - adjuvant mediatory reactions [ 2022 ]  . 
moreover , ld - rt might prevent accelerated viral drug - related mutation , which has been recently described due to increased selective pressure , while potentially improving the immune response by means of the previously described mechanisms and enhanced rna damage compared to antiviral therapy [ 23 , 24 ]  . in the clinical setting , data about nonmalignant pathologies were published during the past century . 
an example is the study published by oppenheimer in 1943 . satisfactory clinical outcomes were obtained after treating 56 patients with a 0.5 - gy equivalent , doses that were previously reported to satisfactorily treat bacterial lung conditions by chamberlain [ 26 ]  . 
no fatalities were recorded [ 27 ]  . it is also to be remarked that the overall covid - 19 intubation - related mortality rate varies between 30 and 70% , according to specic geographical regions [ 5 , 15 , 16 ]  . 
no major data are available at the moment in terms of lung injury secondary to mechanical ventilation , although this still carries inherent risks [ 28 , 29 ]  . 
it has been previously demonstrated that noninvasive ventilation and delayed intubation , when indicated , could also yield lethal consequences in sars management [ 30 , 31 ]  . regarding irradiation technique selection , a three - arc vmat plan was preferred over appa and imrt - based elds , in order to guarantee whole - lung tissue coverage and oar ( mostly cardiovascular structures ) sparing , while simultaneously maintaining the beam - on time as short as possible [ 3234 ]  . 
it should also be noted that positioning and verication times must be accounted for ; therefore , expected target coverage , oar exposure , and image verstrahlenther onkol ( 2020 ) 196 : 10861093 1091 fig . 
furthermore , it is important to highlight that the exposure threshold remains controversial for translation into clinical effects . previous differing publications have described either none or developing of detrimental effects after delivering a 0.5 gy mean dose to the heart [ 35 , 36 ]  . 
weighing up all these considerations and due to the rapid deterioration of these patients status , prioritizing the management of the acute event , in order to potentially save the patients live , is of major relevance . the compassionate treatment offered to the patient and the possible related response in terms of avoiding invasive maneuvers showed clinical improvement from day 2 after rt . 
the initial elevation of serum markers has been described previously , potentially establishing the rst downregulator signal and starting point for further inammatory control ; however , this should be further elucidated [ 38 ]  . 
similarly , the observed mild lymphopenia could be derived from the same phenomenon , although the development of covid - 19 has also been reported as a direct cause of this alteration , as for other viral infections [ 39 ]  . 
the intervention decision should be taken on a multidisciplinary basis and with express consent of the patients , balancing potential benets and risks , preferably encompassed by a prospective clinical protocol . 
recently published evidence from different groups has demonstrated not only the lack of effectiveness but also the risks of employing hydroxychloroquine and azithromycin [ 4044 ]  . despite the previously presented evidence and pathophysiological plausibility , and on the basis of this novel situation , no agent - specic clinical data addressing the possible long - term secondary effects of treating this particular 1092 strahlenther onkol ( 2020 ) 196 : 10861093 group of patients are available , nor is it known if a synergy between the covid - 19 - induced crs and rt could impact the incidence of long - term secondary events . 
this may be taken into consideration when prescribing rt in this setting . the importance and responsibility of establishing properly designed study protocols to clarify this hypothesis falls to the multidisciplinary team and joint efforts from leading scientic societies . 
results from ongoing trials ( nct04377477 , nct04380818 ) will elucidate the effectiveness of this therapeutic tool regarding improvement in pa / fio2 parameters , hospital stay , and icu admission rates . 
sarria reports grants and personal fees from carl zeiss meditec ag , not related to the submitted work . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
marion schneider15 torsten feldt16 bjrn erik ole jensen16 dieter hussinger16 wolfram trudo knoefel17 detlef kindgen - milles18 alessia pedoto19 olaf grebe20 martijn van griensven21 wilfried budach1 jan haussmann1 freddy - joel djiepmo - njanang1 balint tamaskovics1 received : 9 july 2020 / accepted : 12 august 2020 / published online : 10 september 2020 the author ( s ) 2020 abstract purpose covid - 19 infection has manifested as a major threat to both patients and healthcare providers around the world . radiation oncology institutions ( roi ) deliver a major component of cancer treatment , with protocols that might span over several weeks , with the result of increasing susceptibility to covid - 19 infection and presenting with a more severe clinical course when compared with the general population . 
the aim of this manuscript is to investigate the impact of roi protocols and performance on daily practice in the high - risk cancer patients during this pandemic . methods we addressed the incidence of positive covid - 19 cases in both patients and health care workers ( hcw ) , in addition to the protective measures adopted in rois in germany , austria and switzerland using a specic questionnaire . results the results of the questionnaire showed that a noteworthy number of rois were able to complete treatment in sars - cov - 2 positive cancer patients , with only a short interruption . 
the range of protective measures included the creation of working groups , instituting home ofce work and protection with face masks . regarding the therapeutic options offered , curative procedures were performed with either unchanged or moderately decreased schedules , whereas palliative or benign radiotherapy procedures were more often shortened . 
non - university - based rois seemed to be more willing to change their treatment options for curative and palliative cases than university - based rois . conclusion most rois reported a deep impact of sars - cov - 2 infections on their work routine . 
by now , most countries in the world have been affected by this pandemic viral infection [ 17 ]  . the sars - cov - 2 infection poses a signicant threat to cancer patients as they can be more susceptible to the pathogenic complications associated with the infection compared to the general population [ 2 ]  . 
furthermore , oncological treatments including chemotherapy , radiotherapy and the use of additional systemic agents might be associated with lymphopenia and result in an impaired immune response to viral infections [ 9 ]  . 
additionally , cancer fever and other nonspecic symptoms may mask the signs of early covid19 infections . early reports from china suggested an increased incidence of covid - 19 in patients with active cancer and major complications ( such as the need for mechanical ventilation or death ) might be 34 times higher in this population [ 10 ]  . 
reports from italy conrmed that at least 16.5% of all deceased cases had in retrospect a history of cancer within the last 5 years [ 11 ]  . radiation oncology institutes ( rois ) present a unique challenge at the present time . 
immune compromised patients with life - threatening diseases must visit these facilities daily to receive their treatment , being exposed to caregivers and fellow patients who can be asymptomatic carriers of the disease . 
caregivers including radiation therapy technicians ( rtts ) , nurses , physicians and physicists have a higher incidence of exposure to the virus and contribute to further spreading the disease among coworkers and families . 
the rtts generally meet about 3050 patients per linear accelerator per day . this work aims to quantify the incidence of covid - 19 in these departments , to measure and analyze the countermeasures taken by rois to decrease the risk of infection for both patients and healthcare workers ( hcw ) , and to evaluate changes in treatment policy during the pandemic . material and methods questionnaire we invited all registered rois of the german society for radiation oncology ( degro ) ( n = 292 ) and the austrian society for radiation oncology ( gro ) ( n = 16 ) to participate in an anonymous online survey on the covid19 outbreak and its clinical implications in their institutions . 
a link to the questionnaire was embedded in e - mail messages sent between 26 and 27 april 2020 . additional invitations were sent on 57 may 2020 to all registered rois of the swiss society for radiation oncology ( sro , ssro ) ( n = 37 )  . 
the number of rois is based on the dirac database of the international atomic energy agency ( iaea ) [ 12 ]  . the questionnaire was designed to capture the specic numbers of covid - 19 infections of both patients and caregivers and to report what measures were taken to prevent covid - 19 infections . 
overall , the questionnaire consisted of 25 questions : 6 addressing how many patients and staff were infected , 9 screening procedures as well as the use of personal protective equipment ( ppe ) and other prevention strategies , and 10 investigated changes in oncological treatments and follow - ups due to the pandemic . 
released 2013 ( ibm corp , armonk , ny , usa [ 14 ] )  . questionnaire , provided in german and english , can be found in the electronic supplementary material . 
the highest 10% of the distances were further compared . german covid - 19 incidences were taken from the robert koch institute ( rki ) accessed on 22 may 2020 [ 13 ]  . 
the austrian incidence of the infection was obtained from while for the swiss was used , including the absolute numbers obtained as of 22 may 2020 . results baseline results the questionnaire was open from 26 april until 22 may 2020 . 
nearly two thirds of the answers were provided within the rst 2 days . tables 2 , 3 and 4 show the number of responding institutions distributed by country and type of roi . 
the response rates were 28.4% ( 83 / 292 ) for germany , 81.2% ( 13 / 16 ) for austria and 29.7% ( 11 / 37 ) for switzerland . 
the largest number of responses ( n = 31 ) came from rois in hospital departments , followed by rois within medical care centers ( n = 28 ) , rois in university clinics ( n = 24 ) and private practices ( n = 23 )  . of the 106 rois , 24 reported a total of 46 sarscov - 2 positive patients . 
taking the temperature was performed in 26.3% rois , while o2 saturation ( 2.0% ) , pulse rate ( 4.0% ) and swab testing ( 9.1% ) where done less frequently . 
the majority of institutions reported smaller work groups for rtts ( 66.3% ) , physicists ( 59.3% ) and physicians ( 51.2% ) , whereas nurses ( 32.6% ) mainly remained in the same teams . 
4ae shows the analysis of changes in therapeutic strategy to shorter treatment schedules , postponement or omission of radiation therapy by type of roi and whether the institution reported positive patients . we detected that curative schedules were more likely to stay unchanged , whereas moderate or ultra - hypofractionated treatment regimens were applied more in patients with palliative concepts . 
positive covid - 19 cases did not affect the changes in whole sample ; however , non - university clinics with positive patients reported signicantly more changes to follow - up visits by telephone . discussion the analysis of this online survey provides a cross - sectional assessment of rois in three european countries between the end of april and the end of may 2020 , during the covid19 pandemic . 
3 comparison of mean number of patients treated per roi per day before and during the pandemic separated by country , incidence , type of roi and occurrence of positive cases . 
d institutions with ( red ) or without ( blue ) sars - cov - 2 positive patients in university clinics 1074 strahlenther onkol ( 2020 ) 196 : 10681079 ins ( cid : 2 ) tu ( cid : 2 ) ons with or without sars - cov - 2 pos . 
6 changes in follow - up : mean number of changes to either no change , postponement of follow - up visit , switch to telephone call or video call . 
a changes in follow up , all institutions , institutions with ( red columns ) or without ( blue columns ) sars - cov - 2 positive patients ( univrsitary and non universitary clinics both together )  . 
b changes of follow up , non - university clinics , institutions with ( red columns ) or without ( blue columns ) sars - cov - 2 positive patients in non universitary clinics . c changes of follow up , university clinics , institutions with ( red columns ) or without ( blue columns ) sars - cov - 2 positive patients in universitary clinics population ( 0.25% ) , reecting the presence of higher risk population in rois . 
serious outbreaks in multiple rois have been avoided most likely because of the protective measures implemented by each institution in compliance with published reports and recommendations [ 1521 ]  . 
in march 2020 , aro , degro and the professional association for radiation oncology during the covid - 19 pandemic ( des - berufsverbandes - zur - strahlentherapie - waehrend - dercovid - 19 - pandemie ) released a statement with suggestions on the treatment of patients suspected of sars - cov - 2 infection . 
these recommendations were in agreement with the current recommendations of the german rki and local hygiene commissions . these documents highlight the need to maintain the safety of both patients and hcws by avoiding or rescheduling treatments if the risk of being infected with covid19 outweighs the benet of treatment , and shortening therapies as much as possible . 
american centers appear to have implemented stricter screening procedures ( 98% screen patients and 91% hcw ) compared to their european counterparts ( 82% screen patients and 60% hcw ; our data : 51% screen patients and 23% hcw )  . 
concomitant systemic therapy , however , had no statistically signicant inuence on survival , non - cytotoxic ( or = 1.04 ) and cytotoxic effects ( or = 1.47 ) , suggesting that omission of systemic therapy is probably unnecessary and should be strongly weighed against the potential benets . 
who reported that patients undergoing any systemic anticancer treatment during the last 4 weeks including cytotoxic chemotherapy ( or = 1.18 ) and radiotherapy ( or = 0.65 ) had no increased risk of death according to an univariate and a multivariate analysis [ 25 ]  . 
reported an increased mortality after chemotherapy ( or 3.51 ) with no effect of radiotherapy [ 26 ]  . evidence for drastically higher mortality among sarscov - 2 - positive cancer patients undergoing active therapy is controversial as data showing an increase are mostly retrospective and hampered by confounding factors . 
specically , radiation therapy as a cancer treatment modality is not linked to higher mortality from covid - 19 ; however , there is growing evidence on the additional harm from the 1076 strahlenther onkol ( 2020 ) 196 : 10681079 covid - 19 infection in untreated malignant diseases with an increased morbidity and mortality [ 27 , 28 ]  . 
especially , tumortreatment often requires timely diagnosis and the participation of different medical departments . our survey shows that most of the curative treatment protocols were not affected by covid - 19 , with infected cancer patients being able to continue their treatments , which demonstrated an intact infrastructure of the responding rois . 
for example in italy , in areas severely affected by the pandemic , the recommendations have been to postpone all non - urgent therapy and cancel palliative radiotherapy when other alternative protocols are equally effective [ 15 ]  . 
hygiene measures as well as constant ventilation of the treatment rooms have also to be considered . similar to our experience , the swiss survey reported an increase of hypofractionation , even though with a lower percentage compared to ours ( 518% and 25.642.1% , respectively ) [ 29 ]  . 
it will be interesting to see whether rois will continue using the shorter treatment protocols , especially for curative treatments of breast or prostate cancers . in these sites , the use of moderate hypofractionated or ultrahypofractionated regimens might still be lower compared to countries like the united kingdom or canada . 
one could speculate that some of these modications in protocols will remain in practice as found to have improved patient outcome with less toxicity than anticipated . we acknowledge several limitations of our survey . 
asymptomatic , yet infectious cases could have been present , but not detected [ 31 , 32 ]  . this survey might be considered as a starting point for future studies . 
data could be collected on the medical and nancial repercussions of prevention strategies in different rois , or at the regional or national level , on the assessment of risky behavior and their consequences , with the identication of the responsible factors . conclusion this survey demonstrated a signicant effect of the covid19 pandemic on the responding rois , with implementation of safety measures and changes of their treatment protocols . the rois were able to perform curative treatments and persisted to mainly continue radiotherapy to sars - cov - 2 positive patients . 
haussmann declare that they have no competing interests . ethical standards there was no ethics approval necessary because this was a questionnaire among health care workers . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
oktober 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund karzinombezogene kognitive einschrnkungen ( cancer - related cognitive impairment [ crci ] ) knnen unter adjuvanter chemotherapie auftreten und persistieren . 
die tailorx - studie bot die mglichkeit , prospektiv die von patientinnen mit frhem brustkrebs unter adjuvanter chemoendokriner ( ct + e ) oder alleiniger endokriner ( e ) therapie berichteten crci abzuschtzen und hier den alleinigen beitrag der chemotherapie zu crci zu quantizieren . ergebnisse die fact - cog - pci - scores waren signikant niedriger nach 3 , 6 , 12 , 24 und 36 monaten im vergleich zu den ausgangswerten in beiden therapiegruppen . 
das ausma der pci - score - nderungen war grer bei ct + e gegenber e nach 3 monaten , dem vorher denierten primren studienendpunkt , und auch nach 6 monaten , nicht jedoch nach 12 , 24 und 36 monaten . 
tests zur mglichen interaktion zwischen menopausalstatus und therapieform ergaben keine signikanten zusammenhnge . methodik patientinnen mit einem mittleren wert ( 1125 ) eines auf der basis eines biomarkers ( 21 - gen - expressionsassay ) beruhenden rckfallrisikoscores wurden in die tailorx - studie eingeschlossen und erhielten randomisiert eine ct + e oder alleinige e . 
die kognitiven einschrnkungen wurden bei einer subgruppe von 552 auswertbaren patientinnen unter verwendung eines 37 punkte erfassenden fragebogens ( functional assessment of cancer therapycognitive function [ fact - cog ] ) ermittelt , ausgehend von einem basiswert vor randomisierung sowie 3 , 6 , 12 , 24 und 36 monate danach . 
als klinisch sinnvoll erachtete vernderungen waren im vorhinein deniert ; lineare regressionen wurden zur modellierung der pciscores beim ausgangs - pci , der therapieform und weiteren faktoren verwendet . originalpublikation wagner li , gray rj , sparano ja et al ( 2020 ) patient - reported cognitive impairment among women with early breast cancer randomly assigned to endocrine therapy alone versus chemoendocrine therapy : results from tailorx . 
diese ergebnisse weisen darauf hin , dass eine chemotherapie frhe , jedoch nicht dauerhafte kognitive einschrnkungen im vergleich zur e hervorruft , und knnen damit kliniker und patientinnen beschwichtigen , bei denen eine adjuvante chemotherapie zur reduktion des rckfallrisikos indiziert ist . kommentar als karzinombezogene kognitive einschrnkungen ( cancer - related cognitive impairment [ crci ] ) werden vernderungen und ein nachlassen der kognitiven funktion im zusammenhang mit der diagnose und / oder therapie von tumorerkrankungen verstanden . 
sie gehren zu den am meisten gefrchteten behandlungsfolgen einer tumortherapie , sind verbunden mit verminderung der gesundheitsbezogenen lebensqualitt ( health - related quality of life [ hrql ] ) und schrnken soziales und beruiches funktionieren ebei an brustkrebs erkrankten wird die prvalenz zwischen 16 % und 75 % abhngig von den verwendeten quantizierungsparametern geschtzt . 
umgangssprachlich wurde der terminus crci auch als chemobrain verstrahlenther onkol ( 2020 ) 196 : 11421144 1143 wendet unter der annahme eines ausschlielichen zusammenhangs mit einer erfolgten chemotherapie [ 1 ]  . sen ( 2 % nach 10 jahren ) und lsst keinen effekt durch eine adjuvante chemotherapie erwarten [ 3 , 4 ]  . die vorliegende tailorx - pro - studie prsentiert als substudie zur 4 / 2006 bis 10 / 2010 rekrutierenden randomisierten trial - assigning - individualized - treatment - options ( tailorx ) - studie die resultate von aufgetretenen crci bei patientinnen mit brustkrebs vor und nach deren adjuvanter systemtherapie , die die betroffenen selbst aus ihrer sicht berichtet und quantiziert haben ( patientreported outcomes [ pro ] )  . 
die dabei auf grundlage der functional - assessment - of - cancer - therapy - cognitivefunction ( fact - cog ) - fragebgen ausgewerteten kognitiven einschrnkungen ( perceived cognitive impairment [ pci ] ) vor randomisierung und im verlauf eingetretene nderungen werden mit einem fact - cog - pci - score erfasst auf einer pci - skala von 0 bis 80 . 
je hher ein pci - score auf der pci - skala ist , desto geringer sind die empfundenen kognitiven einschrnkungen und vice versa . die methodik zur erfassung von pro wird als goldstandard fr die quantizierung symptomatischer therapieeffekte angesehen [ 2 ]  . 
durch das randomisierte design der tailorx - studie zur evaluation unterschiedlicher adjuvanter therapien bei brustkrebspatientinnen ergab sich die einzigartige gelegenheit zur quantizierung von crci ( insbesondere von kognitiven einschrnkungen , aber auch fatigue sowie verstrkungen unerwnschter behandlungsfolgen einer endokrinen therapie ) als folge einer alleinigen adjuvanten chemotherapie . 
die tailorx - studie verwendete einen solchen score als parameter fr eine biomarkerbasierte entscheidungsstrategie : das rckfallrisiko wurde anhand eines spezischen biomarkers , des 21 genexpressionen umfassenden assays oncotype dx ( vormals : genomic health inc , aktuell : exact sciences corporation , madison , wi 53719 , usa ) , innerhalb eines bereichs von 0 bis 100 ermittelt . 
demgegenber ist ein niedriger score ( 010 ) prognostisch gnstig fr eine sehr geringe wahrscheinlichkeit von fernmetastadie prospektive tailorx - studie sollte klren , ob oncotype dx prognostisch ausreichend valide fr eine individualisierte abschtzung des rckfallrisikos im mittleren rckfallrisikobereich , deniert mit scores von 11 bis 25 , und somit klinisch tauglich fr eine empfehlung fr oder gegen eine adjuvante systemische chemotherapie bei brustkrebspatientinnen im frhstadium ist . 
sie erhielten randomisiert als adjuvante systemtherapie entweder eine kombinierte , zumeist sequenzielle chemound endokrine ( ct + e ) oder eine alleinige endokrine therapie ( e ; [ 3 ] )  . 
im ergebnis wies die tailorx - studie hnliche effekte von ct + e gegenber e mit geringen vorteilen fr > 50 - jhrige postmenopausale patientinnen bei einer ct + e nach [ 3 ]  . 
damit erweiterte die tailorx - studie die patientinnengruppe mit hormonrezeptor - positivem frhem brustkrebs , der eine zustzliche chemotherapie erspart werden kann . die tailorx - pro - substudie geht bei der fortlaufenden erhebung von fact - cog - pci - scores im wesentlichen der frage nach , ob ein ersparen einer adjuvanten chemotherapie auch eine verminderung des risikos fr crci zur folge hat . 
damit sind im vergleich zur alleinigen e sowohl ein strkerer einuss einer aktuell erfolgenden chemotherapie auf die crci als auch dessen zeitliche begrenztheit hinsichtlich des ausmaes der crci belegt . insgesamt knnen die verminderungen der pci - scores in beiden gruppen nach 3 monaten auf 63 ( ct + e ) bzw . 
auf 65 , 5 ( e ) und letztlich auch die unterschiede in den pciscore - vernderungen dennoch als relativ gering beurteilt werden , da sie sich im verlauf nicht substanziell fortsetzen und nach 36 monaten weiterhin in etwa in gleicher hhe liegen , jedoch stets unter den jeweiligen ausgangswerten ( ct + e : 63 , 0 , e : 63 , 9 )  . in den graken zeigt sich , dass bei prmenopausalen patientinnen die pci - scores bei der ct + e - gruppe nach 3 monaten gegenber dem ausgangswert strker abelen 1144 strahlenther onkol ( 2020 ) 196 : 11421144 im vergleich zur e - gruppe . 
dennoch ergaben tests auf mgliche interaktionen zwischen menopausenstatus und therapiearm nach einschtzung der autoren keine signikanten unterschiede . das persistieren niedriger pci - scores unter e allein im langzeitverlauf ist besonders beachtenswert und unzweifelhaft als ( weiterer ) beleg fr den klinisch relevanten nebeneffekt auch endokriner adjuvanter systemtherapien und ihres kausalzusammenhangs mit crci anzusehen . weiterhin wichtig erscheint mir auch , dass das patientenalter nicht mit crci - vernderungen assoziiert war und dass in den altersgruppen keine unterschiede in den dokumentierten therapiebeeintrchtigungen in beiden behandlungsarmen bestanden . bei der interpretation der ergebnisse der tailorxpro - studie ist auch zu bercksichtigen , dass aufgrund eines fehlenden vergleichs mit kohorten gesunder frauen kaum normative daten von pci - scores vorliegen und somit die klinische relevanz langzeitig anhaltender therapieassoziierter kognitiver beeintrchtigungen nur eingeschrnkt beurteilbar ist [ 5 ]  . 
beide adjuvanten systemtherapieformen ( ct + e und e ) sind behaftet mit risiken langzeitiger kognitiver einschrnkungen : eine adjuvante chemotherapie ( hier berwiegend taxanhaltige kombinationen ) verursacht strkere kognitive einschrnkungen in der aktuellen therapiephase als alleinige endokrine therapien . 
sparano ja , gray rj , makower df et al ( 2018 ) adjuvant chemotherapy guided by a 21 - gene expression assay in breast cancer . n engl j med 379 ( 2 ) : 111121 . 
paik s , tang g , shak s et al ( 2006 ) gene expression and benet of chemotherapy in women with node - negative , estrogen receptorpositive breast cancer . 
kessel1 , 2 , 3 uwe thiel4 stefan burdach4 severin kampfer1 received : 11 november 2019 / accepted : 7 july 2020 / published online : 3 august 2020 the author ( s ) 2020 abstract background and purpose radiotherapy ( rt ) is persistently gaining signicance in the treatment of pediatric tumors . however , individual features of a growing body and multifocal stages complicate this approach . 
here we report on toxicity incidence and outcome of tomotherapy with a focus on multitarget rt ( mtrt )  . materials and methods from 2008 to 2017 , 38 children diagnosed with sarcoma were treated with tomotherapy . 
toxicity was graded according to the common terminology criteria for adverse events v.4.03 and classied into symptoms during rt , acutely ( 06 months ) and late ( > 6 months ) after rt , and long - term sideeffects ( > 24 months )  . results the main histologies were ewing sarcoma ( n = 23 [ 61% ] ) and alveolar rhabdomyosarcoma ( n = 5 [ 13% ] )  . 
although localized sarcomas can commonly be cured using chemotherapy in combination with surgeryand radiotherapy - based local therapy , metastatic spread is often present at diagnosis [ 1 , radiotherapy ( rt ) is persistently gaining signicance in the treatment of pediatric tumors [ 3 ]  . 
furthermore , new treatment concepts for multifocal stages of pediatric sarcomas include the application of high - dose chemotherapy , such as busulfan and melphalan , which are suspected to highly interact with rt and cause severe side effects but also improve the diagnosis and outcome of ewing sarcoma [ 4 , 5 ]  . 
these longterm side effects include endocrine dysfunctions , growth delay , and development disorders [ 6 ]  . nevertheless , there is a higher risk of developing second malignancies compared to adult patients , which may lead to a decrease in overall survival and quality of life after treatment [ 79 ]  . 
imrt allows precise irradiation of tumor sites by accumulating the irradiation dose in the dened target volume and minimizing dose to nearby organs at risk [ 10 ]  . furthermore , image - guided radiation therapy ( igrt ) increases the accuracy of rt based on daily imaging of the tumor sites and adjusting the patients position . 
thus , igrt adapts to the position of the patient by comparing images of , e.g. , computed tomography ( ct ) , with the original images of the planning ct before each fraction of rt [ 11 ]  . helical intensity - modulated rt ( tomotherapy ) with integrated image guidance can be used to hit multiple targets in one session and offers treatment with a low risk of side effects by reducing the exposed healthy tissue . 
while the patient is continuously translated into the gantry , the fan beam rotates continuously around the patient , allowing irradiation of large and anatomically complex tumor volumes [ 12 ]  . rt enhances not only the local control of tumors but also improves the outcome of high - risk patients with radiosensitive ewing sarcoma and rhabdomyosarcoma [ 13 , 14 ]  . 
however , rt also inuences the outcome of patients with radioresistant osteosarcomas , where the surgical local control of lesions is difcult or as a treatment method for palliative pain relief [ 15 , 16 ]  . 
a particular focus lies on survival data and toxicity after multitarget rt ( mtrt ) of children with multifocal tumor stages . patients and methods patients between 2008 and 2017 , a total of 38 children diagnosed with sarcoma were treated with tomotherapy at our department . 
in this retrospective evaluation , children with age up to 19 years and a diagnosis of sarcoma were included . a different entity , an age older than 19 years , and irradiation other than tomotherapy led to an exclusion . 
the local ethics committee of the medical faculty of the technical university mnchen ( tum ) approved the study ( vote numbers : 470 / 17 s )  . treatment characteristics all patients were treated with helical intensity - modulated radiotherapy ( tomotherapy hi - art , accuray , sunnyvale , ca , usa )  . 
the rotating gantry system allows the best target coverage for multitarget , complex , and very long volumes , which can be targeted from any angle to deliver a highly conformal dose distribution to the target while simultaneously sparing healthy tissue [ 17 ]  . 
for treatment planning , a contrast - enhanced planning ct was generally used to dene organs at risk and the gross tumor volumes . target volume denition was performed with the goal of small treatment regions to avoid normal tissue toxicity , especially in patients with higher numbers of targets . therefore , the concept was based on euro - ewing , but with strahlenther onkol ( 2020 ) 196 : 11031115 1105 table 1 the prevalent types of sarcomas histological types of sarcomas ewings sarcoma rhabdomyosarcoma embryonal rhabdomyosarcoma alveolar rhabdomyosarcoma osteosarcoma nonrhabdomyosarcoma soft tissue sarcoma synovial sarcoma desmoid sarcoma unclassied sarcoma fibromyxoid sarcoma n ( % ) 23 ( 61% ) 6 ( 16% ) 1 ( 3% ) 5 ( 13% ) 2 ( 5% ) 7 ( 18% ) 2 ( 5% ) 2 ( 5% ) 2 ( 5% ) 1 ( 3% ) much smaller safety margins of approximately 5 min detail , the gross tumor volume ( gtv ) with an additional margin of approximately 5 mm resulted in the clinical target volume ( ctv )  . 
all 6 patients diagnosed with rhabdomyosarcoma ( alveolar and embryonal ) were treated with a median total dose of 50 gy ( range 4450 gy ) and a single dose of 2 gy . 
patients who were diagnosed with other soft tissue sarcomas ( n = 7 ) received rt with a median total dose of 60 gy ( range 5066 ) and a single dose of 2 gy . 
the indication for rt was set for each patient individually depending on age , entity , anatomic location , stage of disease , and the possibility of surgical removal . seven patients ( 18% ) received neoadjuvant rt to improve the success of surgical removal . 
if indicated , rt was applied adjuvantly after surgery ( n = 23 [ 61% ] ) , because lesions were not resectable with clear margins and had microscopically residual disease . 
depending on the entity , chemotherapy was performed either within the euro - ewing study protocols ( n = 22 ) or according to the cws ( cooperative weichteilsarkomstudie ) guidance ( n = 13 )  . 
one patient received previous treatment as a very - high - risk patient within the cws study 2004 , another 4 patients were included in the very - high - risk group of the cws study 2002 , and 7 others received treatment according to the cws 2007 hr protocol . 
two patients with osteosarcoma were included in the euroamoss - 1 / cross study , and 1 patient with a multifocal ewing sarcoma was treated according to the aews0031 study protocol . 
after rt , 17 patients ( 45% ) underwent stem cell transplantation . most patients ( n = 35 ) were treated with curative intent , while 3 patients ( 8% ) with recurrences received palliative care . follow - up and toxicity the occurring toxicity mentioned either during the radiotherapy session or within the follow - up period was protocolled prospectively in our institutional database or the patients chart . 
during the rst year , regular assessments were performed every 3 months , then every 6 - 12 months depending on the clinical need of the patient and the prognosis . 
toxicity during and after rt was graded according to the common terminology criteria for adverse events ( ctcae ) version 4.03 and classied into symptoms during rt , acutely ( 06 months ) and late ( > 6 months ) after rt , and long - term side effects ( > 24 months after rt )  . 
patients were asked to estimate their quality of life ( qol ) on a scale from 1 to 7 according to the european organization for research and treatment of cancer ( eortc ) quality of life questionnaires ( qlq c30 ) version 3.0 , with 1 indicating worst and 7 best qol at the follow - up examination . 
the patients general health status and independence were mea1106 strahlenther onkol ( 2020 ) 196 : 11031115 table 2 patient characteristics characteristics gender tumor site / histology male female median age head and neck thorax abdomen and pelvis extremities treatment intention chemotherapy radiation treatment primary disease recurrent disease before rt concomitant rct median single dose median total dose simultaneous boost sequential boost neoadjuvant rt adjuvant rt denitive rt stem cell transplantation therapy rt radiotherapy , rct radiochemotherapy ewings sarcoma rhabdomyosarcoma desmoid sarcoma unclassied sarcoma ewings sarcoma rhabdomyosarcoma osteosarcoma unclassied sarcoma ewings sarcoma rhabdomyosarcoma osteosarcoma unclassied sarcoma ewings sarcoma rhabdomyosarcoma synovial sarcoma fibromyxoid sarcoma desmoid sarcoma n ( % ) 23 ( 60.5% ) 15 ( 39.5% ) 15 ( 1619 ) years 7 ( 18% ) 2 ( 29% ) 3 ( 43% ) 1 ( 14% ) 1 ( 14% ) 24 ( 63% ) 17 ( 71% ) 5 ( 21% ) 1 ( 4% ) 1 ( 4% ) 21 ( 55% ) 13 ( 62% ) 5 ( 24% ) 2 ( 8% ) 1 ( 4% ) 17 ( 45% ) 10 ( 59% ) 3 ( 18% ) 2 ( 12% ) 1 ( 6% ) 1 ( 6% ) 28 ( 74% ) 10 ( 26% ) 36 ( 95% ) 29 ( 76% ) 2 gy ( 1.802.27 gy ) 54 gy ( 40.566.0 gy ) 26 ( 68% ) 5 ( 13% ) 6 ( 16% ) 23 ( 61% ) 8 ( 21% ) 17 ( 45% ) sured according to the karnofsky performance status scale ( kps )  . 
4 kaplanmeier estimator of progression - free survival of patients treated with mtrt for primary disease differentiated by entity table 3 severe toxicity during and acutely after multitarget radiotherapy ( mtrt ) during rt ( n = 20 ) grade 3 absolute ( % ) grade 4 absolute ( % ) acutely after rt ( n = 18 ) grade 3 absolute ( % ) grade 4 absolute ( % ) toxicity nausea / vomiting loss of appetite radiodermatitis mucositis dysphagia diarrhea urogenital infection pain hematological pericarditis pericardial effusion pneumonitis enterocolitis gastritis 2 ( 10% ) 1 ( 5% ) 3 ( 15% ) 1 ( 5% ) 2 ( 10% ) 1 ( 5% ) 1 ( 5% ) 2 ( 10% ) 10 ( 50% ) 1 ( 5% ) 8 ( 40% ) 2 ( 11% ) 1 ( 6% ) 1 ( 6% ) 1 ( 6% ) 1 ( 6% ) 1 ( 6% ) 1 ( 6% ) disease of an ewing sarcoma ( n = 12 ) had a mean pfs of 39.7 months ( 95 ci 21.757.6 months ) , of whom 5 patients showed tumor progression ( 42% )  . 
mucositis grade 4 of a patient receiving rt of the head and neck among other regions was the only non - hematological grade 4 toxicity that occurred during rt . most patients ( n = 18 [ 90% ] ) developed severe hematological toxicities during mtrt but with no signicant relation to rt characteristics , see supplementary le 3 . 
none of the patients indicated impairments ( < 6 / 7 ) of qol or their health status for more than 2 years after mtrt . single - target radiation therapy most patients with single - target rt ( n = 8 [ 44% ] ) had stage iv disease at diagnosis , 2 patients ( 11% ) were in stage iii , and 5 patients ( 28% ) in stage ii . 
the prevalent types of sarcomas were ewing sarcoma ( n = 9 ) , osteosarcoma ( n = 2 ) , alveolar rhabdomyosarcoma ( n = 1 ) , and six other soft tissue sarcomas ( desmoid sarcoma [ n = 2 ] , synovial sarcoma [ n = 2 ] , bromyxoid sarcoma [ n = 1 ] , unclassied sarcoma [ n = 1 ] )  . 
both osteosarcoma patients , 3 patients with ewing sarcoma , and 3 patients with other soft tissue sarcomas ( desmoid sarcoma [ n = 2 ] , bromyxoid sarcoma [ n = 1 ] ) were treated for recurrences ( n = 8 [ 44% ] )  . 
all of the recurrences were local relapses , but 3 patients had rt for systemic relapsed metastasis : 1 patient received rt for a vertebral metastasis of osteosarcoma and 2 patients with ewing sarcomas had rt for each lung metastasis or an osseous metastasis in the iliac bone . 
patients with recurrent disease of ewing sarcoma ( n = 3 ) had a mean pfs of 70.3 months ( 95 ci 15.7124.9 months ) , also with 1 patient with local failure ( 33% )  . 
the 1 patient with the primary disease of alveolar rhabdomyosarcoma showed a pfs of 101 months . all patients with soft tissue sarcomas had a mean pfs of 49.4 months ( 95 ci 18.979.8 months ) , but 2 patients showed tumor progression . 
patients with a primary disease ( n = 3 ) had a mean pfs of 65.3 months ( 95 ci 30.799.9 months ) and patients with recurrent disease had a mean pfs of 27 months ( 95 ci 648 months )  . 
5 kaplanmeier estimator of overall survival of patients treated with single - target rt differentiated by entity table 4 severe toxicity during and acutely after single - target radiotherapy ( rt ) toxicity radiodermatitis dysphagia pain hematological mucositis loss of appetite during rt ( n = 18 ) grade 3 absolute ( % ) 4 ( 22% ) 1 ( 6% ) 1 ( 6% ) 8 ( 44% ) grade 4 absolute ( % ) 1 ( 6% ) 4 ( 22% ) 2 ( 13% ) 1 ( 7% ) 1 ( 7% ) acute after rt ( n = 15 ) grade 3 absolute ( % ) grade 4 absolute ( % ) 1112 strahlenther onkol ( 2020 ) 196 : 11031115 fig . 
6 kaplanmeier estimator of progression - free survival of patients treated with single - target rt differentiated by entity and nausea and vomiting ( n = 9 [ 50% ] )  . 
both were diagnosed with ewings sarcoma and received rt in the abdominal and pelvic region with a median dose of 55 gy ( range 5456 gy ) and a single dose of 2 gy . 
however , to our knowledge , this is the rst study to present the outcome and toxicity rates of tomotherapy in pediatric patients with a focus on mtrt of sarcomas . 
have already compared different radiation techniques for selected pediatric patients and stated helical tomotherapy to be a satisfactory treatment method for pediatric patients with large complex - shaped tumors near organs at risk [ 25 ]  . 
at the time of rt , most patients had stage iii or iv disease ( n = 30 [ 79% ] ) , which is generally associated with poor outcome [ 2628 ]  . 
since various entities located in different areas of the body were included in this study , it is unfeasible to compare the general os and pfs of this study with the survival data of other studies . 
analyzed the outcome of pediatric ewing sarcomas and stated a 5 - year os of 27% for patients with metastatic disease and 85% for localized disease , where again our abovementioned outcome for multifocal ewing sarcoma has to be highlighted [ 30 ]  . 
regarding localized disease , patients receiving single - target rt had a noteworthy 5 - year os rate of 75 10.8% and mostly included ewing sarcoma ( n = 9 ) and nonrhabdomyosarcoma soft tissue sarcoma ( n = 6 )  . 
however , due to small numbers of patients and the included different entities as well as primary and recurrent diseases , a comparison to survival rates of other studies might not be conclusive . 
despite this , the mean os of 3 patients with a relapsed disease of ewing sarcoma of 59.3 months ( 95 ci 0121.9 months ) after singletarget rt seems noticeably auspicious considering the poor 5 - year os of < 15% shown by bacci et al . 
patients with metastatic rhabdomyosarcoma had a 5 - year os of 20% 17.9% that is comparatively similar in context to rudzinski et al . , who indicated an approximate os of 2040% , and breneman et al . , who mentioned a 3 - year os of 39% ( 95% ci 3048% ) [ 34 , 35 ]  . 
besides , a good outcome and little toxicity of imrt in comparison to other rt techniques were demonstrated by qui et al . in pediatric nasopharyngeal carcinoma [ 36 ]  . 
particularly in the eld of radiation oncology , proton beam therapy offers another approach in the local treatment of pediatric cancers by irradiating sensitive tumor sites very precisely with only a low dose to surrounding healthy tissue and nearby organs at risk [ 37 , 38 ]  . 
due to the excellent dose distribution in proton beam therapy , studies show promising results with low toxicity rates , but also indicate the need for further studies on the long - term toxicity of proton therapy in pediatric patients [ 39 , 40 ]  . besides , proton therapy seems to mitigate the risk of developing second cancers as long - term toxicity after radiation compared to photon therapy [ 41 ]  . 
in this study , however , the incidence of severe toxicity caused by tomotherapy was noticeably low , with no signicant difference between both groups ( single - target rt and mtrt )  . 
such low rates of non - hematological grade 4 toxicity are even more surprising considering the poor prognosis of most patients with a need for aggressive rt ( median dose 54 gy ) and concomitant chemotherapy ( 76% )  . 
when comparing both subgroups concerning 1114 strahlenther onkol ( 2020 ) 196 : 11031115 hematological toxicity , the percentage of patients receiving mtrt ( n = 18 [ 90% ] ) was higher than that of patients with single - target rt ( n = 12 [ 67% ] )  . 
in patients with mtrt , the duration of rt in minutes was signicantly related to the kps of the patient , due to the size of target lesions and , therefore , the severity of disease . 
only 1 patient who had a multifocal unclassied soft tissue sarcoma suffered from several non - hematological grade 4 toxicities ( gastritis , pericarditis , and pericardial effusion ) acutely after mtrt . 
the same applies to severe toxicity as a late effect , with 1 patient suffering from severe grade 3 dyspnea after receiving mtrt for a multifocal and pulmonary spread ewing sarcoma . 
another patient had a grade 3 pericardial effusion as a late effect after mtrt for an alveolar rhabdomyosarcoma in the posterior mediastinupatients with single - target rt did not show any severe toxicity as a late effect . this study is unique regarding the analysis of long - term sideeffects of tomotherapy . 
however , 2 patients showed growth retardation ( < 3 percentile under the growth curve ) after single - target rt for ewing sarcomas in the abdominal and pelvic region , and 1 patient indicated restrictions in qol and health status after receiving singletarget rt for an ewing sarcoma in the coccyx . 
especially children and adolescents are affected by the long - term side effects of rt and the dangers of developing second neoplasms and , therefore , mortality [ 42 , 43 ]  . 
we are aware that a median follow - up period of 29.7 months ( 95% ci 15.348.2 months ) in this study only allows a limited statement on long - term toxicity and second neoplasms . 
nevertheless , none of the 14 patients evaluable for long - term toxicities within a follow - up range up to 104.5 months ( supplementary le 1 ) have developed second neoplasms after photon therapy so far . 
it would also be helpful to analyze toxicities regarding different tumor sites as well as tumor entities , making a higher number of patients necessary . in conclusion , our results show acceptable levels of acute and late toxicities considering the highly advanced diseases and multimodal treatment . 
combs declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee ( ethics committee of the technical university munich ( tum ) ) and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
oktober 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund das melanom weist bei der erstdiagnose im fortgeschrittenen stadium bei mehr als einem drittel aller patienten eine hohe rate an hirnmetastasen auf [ 1 ]  . 
whrend die resektion und die stereotaktische radiochirurgie wirksame lokale behandlungen fr patienten mit einer geringen anzahl von melanomhirnmetastasen sein knnen , besteht trotzdem weiterhin ein hohes risiko fr eine distante intrakranielle progression . 
um die zu verhindern , ist eine wirksame therapie erforderlich , und die rolle der ganzhirnbestrahlung ( wbi ) wurde deshalb in einigen randomisierten studien systematisch untersucht [ 2 ]  . 
leider waren aber , obwohl das melanom sehr hug hirnmetastasen ausbildet [ 3 ] , solche patienten in den relevanten studien mit weniger als 10 % des untersuchungsguts deutlich unterreprsentiert [ 4 , 5 ]  . die hier vorliegende multizentrische und randomisierte phase - iii - studie sollte also die rolle einer adjuvanten ganzhirnbestrahlung speziell fr patienten mit 13 hirnmetastasen metastasierter melanome untersuchen . 
radiochirurgie oder operation mit anschlieender adjuvanter wbi im interventionsarm . originalpublikation hong am , fogarty gb , dolven - jacobsen k , burmeister bh et al ( 2019 ) adjuvant whole - brain radiation therapy compared with observation after local treatment of melanoma brain metastases : a multicenter , randomized phase iii trial . 
einschlusskriterien waren ein guter bis leicht reduzierter allgemeinzustand ( eastern cooperative oncology group 02 ) , eine geschtzte lebenserwartung von mindestens 6 monaten und eine extrakranielle histologische sicherung eines melanoms . 
die initiale detektion von ein bis 3 hirnmetastasen erfolgte mittels mrt ; die lokale behandlung entweder chirurgisch oder radiochirurgisch . die adjuvante ganzhirnbestrahlung sollte mit mindestens 30 gy in 10 fraktionen innerhalb von 8 wochen nach erfolgter lokaltherapie stattnden . 
die randomisierung erfolgte im 1 : 1 - verhltnis ( interventionsgruppe : n = 107 , beobachtungsgruppe : n = 108 )  . die studie wurde vorzeitig wegen rekrutierungsproblemen mit 215 statt geplanten 220 teilnehmern ( 04 / 2009 bis 09 / 2017 ) gestoppt . 
ber den gesamten beobachtungszeitraum von 48 , 1 monaten lag die distante rezidivrate bei 52 % im interventionsarm und 57 , 9 % im kontrollarm ( or : 0 , 79 ; p = 0 , 39 )  . 
die zeit bis zum auftreten von distanten hirnmetastasen lag im median bei 26 , 4 monaten in der inter1146 strahlenther onkol ( 2020 ) 196 : 11451147 kungs - beziehung wurde bereits von popp et al . 
eine andere erklrung fr die in der vorliegenden studie prsentierten ergebnisse wre natrlich auch die weiterhin aktive hmatogene metastasierung , auch nach durchgefhrter wbi , also eine erneute metastatische aussaat ins hirngewebe . 
das gesamtberleben blieb wie bereits angefhrt kongruent in allen studien unbeeinusst [ 2 ]  . eine klare limitation der vorliegenden studie ist der lange rekrutierungszeitraum von fast 9 jahren , in dem sich die systemische therapie des malignen melanoms dramatisch verbessert hat . 
beispielsweise konnte eine kombinationsbehandlung mit dem anti - ctla - 4 - antikrper ipilimumab und dem pd - 1 - inhibitor nivolumab eine komplette remission bei etwa einem viertel der patienten mit zerebralen melanomhirnmetastasen erzielen ; insbesondere wurde bei 64 % der teilnehmer eine intrakranielle progression fr mehr als 6 monate verhindert [ 9 ]  . diese ergebnisse sind in einer palliativen kohorte mit hirnmetastasen besonders relevant , da eine intrakranielle progression zu erheblichen neurologischen symptomen , funktionellen und kognitiven beeintrchtigungen fhrt sowie eine antidematse therapie erfordert . 
anzunehmen , dass eine stereotaktische radiochirurgie mglicherweise eine adquate lokalkontrolle gewhrleistet . nach aktuellem therapiestandard kommt bei der zerebralen metastasierung eines malignen melanoms eine lokaltherapie ( operation oder stereotaktische strahlentherapie oder beides ) gefolgt von einer immuntherapie zum einsatz . 
11 , 5 monate in der beobachtungsgruppe ( p = 0 , 20 ) , wohingegen die lokale rezidivrate nach der adjuvanten ganzhirnbestrahlung mit 20 , 0 % im vergleich zu 33 , 6 % ohne therapie signikant reduziert werden konnte ( p = 0 , 03 )  . im interventionsarm erfolgte bei 95 % der patienten eine adjuvante wbi mit 30 gy in 10 fraktionen . 
die wbi war mit einer hheren rate an akuten toxizitten ( grad 12 ) verbunden . schlussfolgerungen der autoren eine adjuvante ganzhirnbestrahlung verbessert bei patienten mit 13 behandelten hirnmetastasen eines malignen melanoms die onkologischen ergebnisse nicht . 
es wurde kein signikanter unterschied zwischen interventionsund beobachtungsarm hinsichtlich der distanten intrakraniellen kontrolle oder des gesamtberlebens binnen 12 monaten beobachtet . kommentar die primre oder adjuvante stereotaktische radiotherapie etablierte sich auf der basis mehrerer phase - iii - studien mit und ohne ganzhirnbestrahlung als first - line - therapie bei patienten mit 13 ( 4 ) hirnmetastasen [ 47 ]  . 
die hinzunahme der adjuvanten ganzhirnbestrahlung nach der lokaltherapie verbesserte allerdings trotz der reduktion von lokalen und distanten intrakraniellen rezidiven das gesamtberleben nicht , hatte aber eine messbare verschlechterung der kognitiven leistungen zur folge [ 2 , 4 ]  . 
allerdings basieren die bisher vorliegenden daten auf kollektiven mit metastasen gemischter histologie , vorwiegend von bronchialund mammakarzinomen . die ergebnisse der hier kommentierten studie weichen nun von denjenigen vergleichbarer und wegweisender vorgngerstudien mit gemischten entitten von hirnmetastasen deutlich ab . 
das kann einerseits durch die bekannte strahlenresistenz des malignen melanoms erklrt werden : 30 gy / 3 gy ( bed : eqd2 fr tumor / = 10 , 32 , 5 gy ) reichen nicht aus , um eine mikrometastasierung im hirn zu beseitigen . 
eine solche dosis - wirstrahlenther onkol ( 2020 ) 196 : 11451147 1147 fazit eine adjuvante ganzhirnbestrahlung nach sufzienter lokaltherapie vermindert bei vorliegender hirnmetastasierung eines malignen melanoms das auftreten distanter intrakranieller rezidive nicht und hat keinen einuss auf die zerebral bedingte todesrate . 
tsao mn , xu w , wong rk et al ( 2018 ) whole brain radiotherapy for the treatment of newly diagnosed multiple brain metastases . cochrane database syst rev 1 ( 1 ) : cd3869 . 
kavouridis vk , harary m , hulsbergen afc , lo yt , reardon da , aizer aa , iorgulescu jb , smith tr ( 2019 ) survival and prognostic factors in surgically treated brain metastases . 
brown pd , jaeckle k , ballman kv , farace e , cerhan jh , anderson sk , carrero xw , barker fg 2nd , deming r , burri sh , mnard c , chung c , stieber vw , pollock be , galanis e , buckner jc , asher al ( 2016 ) effect of radiosurgery alone vs radiosurgery with whole brain radiation therapy on cognitive function in patients with 1 to 3 brain metastases : a randomized clinical trial . jama 316 ( 4 ) : 401409 5 . 
kocher m , sofetti r , abacioglu u , vill s , fauchon f , baumert bg , fariselli l , tzuk - shina t , kortmann rd , carrie c , ben hassel m , kouri m , valeinis e , van den berge d , collette s , collette l , mueller rp ( 2011 ) adjuvant whole - brain radiotherapy versus observation after radiosurgery or surgical resection of one to three cerebral metastases : results of the eortc 22952 - 26001 study . j clin oncol 29 ( 2 ) : 134141 6 . 
chang el , wefel js , hess kr , allen pk , lang ff , kornguth dg , arbuckle rb , swint jm , shiu as , maor mh , meyers ca ( 2009 ) neurocognition in patients with brain metastases treated with radiosurgery or radiosurgery plus whole - brain irradiation : a randomised controlled trial . 
aoyama h , shirato h , tago m , nakagawa k , toyoda t , hatano k , kenjyo m , oya n , hirota s , shioura h , kunieda e , inomata t , hayakawa k , katoh n , kobashi g ( 2006 ) stereotactic radiosurgery plus whole - brain radiation therapy vs stereotactic radiosurgery alone for treatment of brain metastases : a randomized controlled trial . 
popp i , rau s , hintz m , schneider j , bilger a , fennell jt , heiland dh , rothe t , egger k , nieder c , urbach h , grosu al ( 2020 ) hippocampus - avoidance whole - brain radiation therapy with a simultaneous integrated boost for multiple brain metastases . 
tawbi ha , forsyth pa , algazi a , hamid o , hodi fs , moschos sj , khushalani ni , lewis k , lao cd , postow ma , atkins mb , ernstoff ms , reardon da , puzanov i , kudchadkar rr , thomas rp , tarhini a , pavlick ac , jiang j , avila a , demelo s , margolin k ( 2018 ) combined nivolumab and ipilimumab in melanoma metastatic to the bran engl j med 379 ( 8 ) : 722730 weiterfhrende literatur 10 . 
brown pd , gondi v , pugh s , tome wa , wefel js , armstrong ts , bovi ja , robinson c , konski a , khuntia d , grosshans d , benzinger tls , bruner d , gilbert mr , roberge d , kundapur v , devisetty k , shah s , usuki k , anderson bm , stea b , yoon h , li j , laack nn , kruser tj , chmura sj , shi w , deshmukh s , mehta mp , kachnic la ( 2020 ) hippocampal avoidance during whole - brain radiotherapy plus memantine for patients with brain metastases : phase iii trial nrg oncology cc001 . 
j clin oncol 38 ( 10 ) : 10191029 radiotherapy and covid - 19everything under control or just the start of a long story ? strahlenther onkol ( 2020 ) 196 : 10651067 editorial ursula nestle1 , 2 , 3 mechthild krause4 , 5 , 6 , 7 , 8 the author ( s ) 2020 this pandemic is an imposition ! we all are exhausted by repeated discussions on the current situation . 
almost forgotten : the initial panic that radiooncology could no longer operate according to law under pandemic conditions was quickly and effectively countered by an unprecedented concerted response from the authorities . then we had all these practical questions : how to deal with potentially limited personnel resources ? how to treat potentially infected patients in routine care ? to this end , at a very early stage , the german society for radiooncology ( degro ) , together with the working group for radiooncology ( aro ) of the german cancer society and the national association of german radiotherapists ( bvdst ) , compiled two helpful statements and recommendations [ 13 ]  . at a previously unimagined speed , we then dealt with hygiene concepts , made friends with hypofractionation , optimized our workow , discussed home ofce solutions , formed staff groups , and reorganized the aftercare outpatient clinics . 
overall , in germany , only a relatively small number of covid - positive patients have had to be treated by ( cid : 2 ) ursula nestle ursula.nestle@mariahilf.de 1 klinik fr strahlentherapie und radioonkologie , kliniken mariahilf mnchengladbach , mnchengladbach , germany 2 klinik fr strahlenheilkunde , universittsklinikum freiburg , freiburg , germany 3 german cancer consortium ( dktk ) partner site freiburg and german cancer research center ( dkfz ) , heidelberg , germany 4 german cancer consortium ( dktk ) partner site dresden and german cancer research center ( dkfz ) , heidelberg , germany radiotherapy so far . 
at least we are very well preparedboth with concepts and organizational skillsfor higher infection rates . three aspects may change our working life beyond the pandemic : ( cid : 2 ) changing workows , home ofce capabilities , digital collaboration . 
this is what the group from bellinzona [ 5 ] vividly describesa model for the future ? ( cid : 2 ) hypofractionation , which before corona entered our german routine only slowly for many tumor entities , will certainly retain greater importance . 
as already stated in the degro statement , it is crucial that herefor published dose / fractionation schedules from randomized phase iii studies are used and that in every institution the introduction of new concepts is closely monitored clinically and organizationally . 
a living overview of published hypofractionated radiation regimens for many indications ( including the corresponding normal tissue constraints ) is available at : 1kicemu_zz5rcpcemndelqcdodyqz4imzh64bx36 ac58 ( cid : 2 ) our methods for radiooncological aftercare may also change : degros respective statement from back in 2015 already considers telephone interviews [ 6 ]  . 
now , 5 oncoray - national center for radiation research in oncology : faculty of medicine and university hospital carl gustav carus , technische universitt dresden , helmholtz - zentrum dresden - rossendorf , dresden , germany 6 dept . 
of radiation oncology , faculty of medicine and university hospital carl gustav carus , technische universitt dresden , dresden , germany institute of radiooncology - oncoray , helmholtz - zentrum dresden - rossendorf , dresden , germany 8 national center for tumor diseases ( nct ) , partner site dresden , germany : german cancer research center ( dkfz ) , faculty of medicine , university hospital c.g. carus dresden and helmholtz - zentrum dresden - rossendorf , dresden , germany 1066 strahlenther onkol ( 2020 ) 196 : 10651067 thanks to the current boost of digitalization , online consulting is also increasingly possible . 
preclinical and clinical studies are ongoing internationally , 16 clinical studies on low - dose irradiation and covid - 19 are already registered in the register platform clinicaltrials.gov and the topic is also being discussed in germany . 
however , beyond a not yet prospectively proven effect on the course of viral pneumonia , some important aspects must be kept in mind during the evaluation and discussion of this idea : ( cid : 2 ) is an inhibition of the pulmonary inammatory response in covid patients really relevant for prognosis or are the vascular complications more likely to be decisive for the outcome ? ( cid : 2 ) are there alternative , e.g. , drug - based , therapeutic approaches that can be realized with less effort , at least in health care systems like ours , for patients requiring intensive care ? ( cid : 2 ) what about the increasing lifetime risks for malignancies ( 0.64 excess lung cancer / 100 patients ) and cardiovascular deaths ( 0.87.6 extra death / 100 patients ) , if we burden the radiation - sensitive thoracic organs of younger benign patients with 0.31 gy ? [ 12 ]  . ( cid : 2 ) how can oncological patients and radiotherapy staff be optimally protected from infection and competition for equipment and personnel resources in the event of planned radiation , if many severely ill covid cases should receive radiotherapy ? as least : radiooncology is subject to speedy developments , even in times of pandemics ! in our opinion , the most important thing is the continuous contribution to the optimal care of cancer patients , with and without covid19 . 
a certain diagnostic gapdue to the lack of preventive examinations and reduced patient willingness to visit a doctormight already be disadvantageous enough . potentially confronted with increasing numbers of covid - 19 infections in the coming autumn and winter , our solidarity will be necessary : before shortages of resources caused by the pandemic may cause unplanned breaks , treatment discontinuations , or long delays in radiotherapy onset , we must activate our existing neighborhood cooperation agreements and therefore test the resilience of our professional network . 
krause declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
vordermark5 received : 2 june 2020 / accepted : 22 october 2020 / published online : 30 october 2020 the author ( s ) 2020 abstract purpose the coronavirus pandemic is affecting global health systems , endangering daily patient care . 
the aim of this survey amongst experts on radiation therapy ( rt ) for lymphoma and leukemia is to delineate typical clinical scenarios and to provide counsel for high - quality care . methods a multi - item questionnaire containing multiple - choice and free - text questions was developed in a peer - reviewed process and sent to members of the radiation oncology panels of the german hodgkin study group and the german lymphoma alliance . 
answers were assessed online and analyzed centrally . results omission of rt was only considered in a minority of cases if alternative treatment options were available . hypofractionated regimens and reduced dosages may be used for indolent lymphoma and fractures due to multiple myeloma . 
even in case of critical resource shortage , panelists agreed to start emergency rt for typical indications ( intracranial pressure , spinal compression , superior vena cava syndrome ) within 24 h . 
possible criteria to consider for patient triage are the availability of ( systemic ) options , the underlying disease dynamic , and the treatment rationale ( curative / palliative )  . conclusion rt for hemato - oncological patients receives high - priority and should be maintained even in later stages of the pandemic . 
clinical presentation shows great heterogeneity , from asymptomatic courses to typical pneumonia symptoms like fever , cough , and dyspnea , but also includes nausea , diarrhea , and kidney injury , which may require intensive care [ 24 ]  . 
focusing on hematological malignancies , reports from europe and the united states displayed case - fatality rates of up to 40% [ 1012 ]  . data from new york city reveal an increased rate of intubation amongst cancer patients with covid - 19 , although augmented mortality was limited to patients < 50 years of age [ 13 ]  . 
against this background , infection risks have to be weighed against the possible disadvantage of postponed or omitted therapy [ 14 , 15 ]  . although the exact impact of covid - 19 on cancer patients is yet to be determined , many specialists in radiation oncology have already formulated emergency guidelines and recommendations for treatment of oncological patients during the pandemic [ 1521 ]  . 
still , there is an unmet need for treatment recommendations , which prompted us to form an expert panel consisting of the main radiation oncologists of the german hodgkin study group ( ghsg ) and the german lymphoma alliance ( gla )  . 
the rst scenario ( phase 1 ) describes an early situation during the pandemic in which sufcient personal and treatment capacities are available , although meanwhile , the disease is spreading and thereby endangering patient care . 
the survey was conducted as an online interrogation with a local adaption of the lime survey ( lime survey , hamburg , germany )  . data were analyzed with microsoft excel 2016 ( microsoft corporation , redmond , usa )  . results overall , 10 participants answered the questionnaire . 
most departments have taken protective measures for hematooncological rt patients ( 9 ; 90% ) , including the wearing of face masks by patients and staff and rigid basic hygiene ( disinfection of treatment rooms , social distancing , reduction of waiting time ) ( table 2 )  . 
dose - reduced concepts were proposed especially for scenario 6 ( 7 ; 70% ) , the majority of suggestions being 2 * 2 gy . in case of a covid - 19 infection before the onset of treatment , most participants agreed to postpone treatment for cases 6 ( 8 ; 80% ) , 1 ( 6 ; 60% ) , and 4 ( 5 ; 50% ) , with less than 50% approval for postponing treatment for the remaining three other cases . 
similar cases were found to be eligible for interruption of treatment until covid - 19negativity is established ( case 1 and 6 : 60% , respectively )  . phase 2 in contrast to phase 1 , considerations for reduction of patients increased ( 3 ; 30% yes versus 4 ; 40% no ; table 2 )  . factors for clinical triage are largely disease dependent , for example the onset of symptoms , curative versus palliative treatment concept ( 7 ; 70% each ) , and the availability of alternative ( systemic ) treatments ( 6 ; 60% ) , whereas patientrelated risk factors ( smoking , hypertension , diabetes , age ) were of less importance ( 4 ; 40% )  . 
the patients immune status , immunosuppressive potency of therapy , and the possibility to carry out treatment in an outpatient setting were deemed even less essential ( 3 ; 30% each )  . there was a broad consensus to commence emergency rt within 24 h for most given examples ( 7 ; 70% for superior vena cava syndrome , spinal cord compression , and amaurosis due to intraorbital disease ; 6 ; 60% for intracranial pressure due to central nervous system lymphoma ) , except for the case of pain caused by vertebral involvement ( 2 ; 20% )  . 
1 overview of answers concerning postponement and omission of radiotherapy as provided by the participants for clinical cases in phase 1 of the pandemic ( n = 10 ) omission postponement case 1 case 2 case 3 case 4 case 5 case 6 no answer given strahlenther onkol ( 2020 ) 196 : 10961102 1099 fig . 
heterogeneous answers were received with regard to the question of which patients to postpone , focusing on cases 1 and 6 ( 5 ; 50% each ) as well as cases 3 and 4 ( 4 ; 40% each )  . 
ranking the different scenarios showed signicant differences regarding urgency , with the highest priority for case 2 ( 4 ; 40% ) and the lowest priority for case 6 ( 6 ; 60% )  . 
median ranks , taking into account only complete answers , were : 4 , 1 , 2.5 , 3 , 2 , and 6 for cases 16 , respectively , which denes scenario 2 and 5 as the most prioritized cases . discussion the hereby presented survey mirrors the complexity of hemato - oncological patient care in radiation oncology facing a pandemic . 
it emphasizes the importance for rt treatment for most clinical scenarios and illustrates feasible alternative concepts . cancer patients are dened as one group of persons at risk for a severe course of covid - 19 infection [ 22 ]  . 
they rely on consequent basic hygiene and social distancing , which have been implemented in nearly all departments for patient and staff protection . the immunosuppressive state of many oncological patients renders them susceptible to infection with increased rates of morbidity and mortality . 
in accordance with this nding , a retrospective analysis of 28 cancer patients with covid - 19 identied anti - cancer treatment within the last 14 days as a risk factor for severe events ( only one patient received rt in this group ) [ 9 ]  . 
although rt has traditionally been regarded as an immunosuppressive treatment , recent studies in radiobiology rather suggest a complex immunomodulatory role , acting on both the cellular and humoral level of the immune system [ 23 , 24 ]  . due to the increased risk prole of hemato - oncological patients , it may be attractive to increase screening efforts and to avoid supplementary toxicities . 
a recent review from guys hospital failed to determine the use of steroids as a risk factor for covid - 19 patients and even pointed towards a positive role when used in early stages of infection [ 25 ]  . 
importantly , ct signs of covid - 19 , like ground - glass opacities and consolidations , are unspecic and may also be caused by inuenza or can be confused with radiation pneumonitis [ 2628 ]  . 
consequently , a medical indication is needed , as thoracic ct scans neither replace laboratory tests nor should they be used as a screening method [ 2628 ]  . recently , the ilrog published emergency guidelines for the treatment of leukemia and lymphoma patients in times of a pandemic , which dene three key strategies : omission , delay , or shortening of rt [ 15 ]  . abandonment of rt may be possible for a palliative setting in which alternative options are at hand , as indicated in clinical scenario 1 . 
regarding multiple myeloma , there were various concepts ranging from 1 * 8 gy , over 5 * 4 gy to 1012 * 3 gy . although hypofractionation is feasible , the respective concepts have to be considered within the clinical context and adapted to the individual patient . 
demonstrated superior neurological recovery for myeloma patients with spinal cord compression by using rt doses of 30 gy [ 29 ]  . additionally , solitary plasma cell lesions such as single osseous plasmocytoma or extramedullary plasmocytoma may 1100 strahlenther onkol ( 2020 ) 196 : 10961102 benet from dose escalation , with a dose recommendation of 4050 gy provided by the ilrog [ 3032 ]  . the questionnaire also aimed at judging the use of a chemotherapy - only regimen for early - stage hodgkin lymphoma ( case 3 ) , which has been addressed by three treatment multicenter trials . 
noninferiority of unimodal could not be proven , so combined - modality treatment of 23 cycles of abvd followed by involved - site or involved - node rt remains standard of care for early - stage patients [ 3335 ]  . 
this corresponds to the low percentage of panelists who agreed to this chemotherapy - only strategy . de - escalation of rt doses for lymphoma patients has been of interest in recent years , especially for indolent lymphoma [ 36 , 37 ]  . 
further studies elaborated on the feasibility of this concept for extranodal indolent lymphoma [ 3841 ]  . this rationale encouraged the suggestion of 2 * 2 gy as an alternative treatment strategy for scenario 6 . 
other options may be the postponement of rt for 1 up to 3 months , which reached a high consent , or a wait - and - see strategy till the onset of symptoms . this is contrasted by the aggressive biology of diffuse large b - cell lymphoma described in cases 4 and 5 [ 42 ]  . delay in treatment delivery for these patients is only acceptable when facing a critical shortage of resources . 
furthermore , hypofractionated concepts lack study validation , being based mainly on calculated equivalent biological efcacy [ 15 ]  . overall , treatment of leukemia and lymphoma patients is prioritized and shortage of treatment for these patients is neglected in most situations . 
moreover , tbi , as an established conditioning modality before allogenic stem cell transplantation , should not be discarded even in advanced pandemic stages [ 43 ]  . however , adequate triage remains challenging both at the medical and the ethical level , being a multifactorial process . 
panel members consented to integrate the distinction between curative and palliative regimens , onset of symptoms / biology of the underlying disease , and the availability of ( systemic ) alternatives in the decision process . 
it is the authors strong belief that access to high - quality rt has to be sustained for all patients , while maintaining treatment equality and personal dignity as delineated by the german federal ethic commission [ 44 ]  . this survey bears several limitations , as only a limited number of radiation oncology experts in lymphoma treatment were consulted . 
restriction of the survey to predened scenarios facilitated the evaluation process , but may be prone to oversimplication of the complex clinical reality . nevertheless , this article provides concepts for typical indications for rt in hemato - oncological patients which are of interest for everyday clinical practice . 
altogether , treating physicians should focus on both maintaining public health by limiting virus spread within the population and guaranteeing state - of - theart hemato - oncological cancer care . conclusion covid - 19 will most likely remain a challenge for health systems at the national and international level in the months to come . 
eich declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
on 25 february 2020 , the rst swiss patient with covid19 was diagnosed in southern switzerland ( canton ticino )  . since then , southern switzerland has been one of the regions most affected by the pandemic [ 3 ]  . in order to cope with the presence of covid patients , hospital management reorganized departments to minimize the risk of transmission for patients and staff . 
radiation oncology departments faced two urgent requirements : ( i ) protect cancer patients and medical / paramedical staff from the risk of viral infection and ( ii ) guarantee radiation treatment that requires very specic skills and xed time schedules [ 46 ]  . the global response to this crisis started with the hashtag #stayathome , to stress the importance of the rst healthcare measure adopted to mitigate sars - cov - 2 infection . worldwide , the lockdown forced the implementation of remote and teleworking . 
however , several patient - related activities in particular treatment planning , reviewing les , multidisciplinary consultations , as well as research and quality assurance do not require physical presence at work , making so - called smart working feasible [ 79 ]  . in our radiation oncology clinic at the oncology institute of southern switzerland , we reorganized the daily routine following who and national statements . 
this novel set - up allowed optimal social - distancing measures and staff protection , proved by the absence of cross infection . in addition , the daily staff meeting was converted to a teleconference meeting in order to discuss ( i ) upcoming patients and radiotherapy strategy , ( ii ) implementing hypofractionation if clinically indicated [ 6 , 10 ] , and ( iii ) procedure update . 
a slight appointment reduction of 10.3% daily ( p = 0.004 ) could still signicantly increase downstream planning ct scheduling ( p = 0.00001 ) and performance ( p = 0.0001 ) , resulting in an absolute 20.1% ( p = 0.009 ) increment of ct performance while avoiding overbooking practices . 
integrating strict testing guidelines , a distancing regimen for staff and patients , hygiene regulations , and precise appointment scheduling , no sars - cov - 2 infection in 164 tested radiation oncology service inpatients was observed . conclusion in times of reduced medical infrastructure capacities and resources , controlling infrastructural time per patient as well as optimizing facility utilization and personnel workload during treatment evaluation , planning , and irradiation can help to improve appointment compliance and quality management . 
active patient ow management in high - risk covid - 19 regions can help radiation oncologists to continue and initiate treatments safely , instead of cancelling and deferring indicated therapies . keywords covid - 19 , sars - cov - 2 radiation oncology disease transmission , infectious radiation dose hypofractionation stereotactic radiosurgery ( cid : 2 ) dennis akuamoa - boateng , mba dennis.akuamoa - boateng@uk - koeln.de 1 department of radiation oncology , center for integrated oncology , university hospital cologne , cologne , germany 2 department of nuclear medicine , university hospital essen , essen , germany 3 department of hospital pharmacy , university hospital cologne , cologne , germany introduction the continued global spread of the severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 ) and the associated risk of pulmonary manifestations of coronavirus disease - 19 ( covid - 19 ) posed a challenge to all human societies in late 2019 and early 2020 [ 19 ]  . 
primarily , three horizontal transmission pathways are discussed which have an impact on the contact guidelines from the societies of radiation strahlenther onkol ( 2020 ) 196 : 10801085 1081 oncology [ 20 , 21 ] : droplet infection , contact infection , and airborne transmission [ 11 , 13 , 22 ]  . 
in the absence of targeted treatment options such as specic antiviral medication or vaccines , primary prevention in the form of isolation , quarantine , social distancing , and community containment have been key response mechanisms to control the pandemic [ 17 ]  . 
due to the late symptom onset alongside high numbers of asymptomatic manifestations , it has been widely reported that controlling viral transmission is crucial to reduce nosocomial disease spread between personnel and patients , especially in healthcare facilities [ 23 ]  . as a population at risk during the ongoing pandemic [ 24 ] , cancer patients and their healthcare providers must constantly balance the risks of sars - cov - 2 infection associated with diagnostic or therapeutic procedures against the risk of a potential delay in treatment , while medical infrastructure capacities and medical resources are reduced . for patients undergoing external beam radiation therapy ( ebrt ) , most regimens are fractionated and require sequential visits . 
active patient ow management was implemented early , at the onset of the pandemic , to adapt to the potential shortage of staff , supply , and government - regulated reduction in hospital treatment capacity [ 15 , 25 ] instead of cancelling indicated therapies . in 2019 , a total of 2174 patients were treated in the department of radiation oncology of the university hospital of cologne , of whom 52% were male and 48% female . 
the university hospital of cologne is a maximum medical care provider and regional covid - 19 treatment center at the center of europe , located close to germanys rst pandemic hotspot in heinsberg . 
telemedical appointments were offered during and after radiation treatment . to abide by strict ofcial disinfection [ 9 ] , hygiene [ 27 ] , contact , and distancing regulations at the university hospital of cologne , personnel and patients wear a face mask across the entire campus and must keep a minimal distance of 1.5 meters to each individuum . shift uctuation of personnel was reduced to secure regular personnel and patient setups by long - term shift assignment and reduced cross - team personnel uctuation . 
exceptions were individually discussed and mainly applied to legal medical attendants . all sorts of business trips were cancelled and personnel with transnational travelling history were required to abide by a 14 - day campus access prohibition ruling . 
staff showing symptoms of upper respiratory tract viral infection were prohibited from entering the campus until 48 h after reconvalescence alongside negative sars - cov - 2 pcr testing . appointments were individually rescheduled to reduce peaks of patients by separating patient ows and reclassifying severity groups . 
protocols were performed according to standard of care practices , preferring hypofractionation where applicable . overbooking of appointments to control for potential patient no - shows was suspended to increase patient and staff safety . 
to increase departments efciency while simultaneously reducing the number of patients in common waiting spaces , patients were urged to wait outside the facility and allowed to enter the facility just shortly before any appointment using strict individual timeslots . 
to reduce the time per patient spent in the facility , patients were grouped into four time categories ad of short , medium , long , and extra - long expected planning ct timeslots , respectively , to control the time per patient and to ensure time to comply with hygiene and disinfection guidelines . prescreening of patients full - track records reduced the number of multiple appointments and helped in assigning patients to severity groups ad , estimating the potential time spent within the facility and the case complexity for treatment discussion , planning , and radiation sessions . every inpatient received a covid - 19 pcr test on the day of admission and was required to hold a negative test 1082 strahlenther onkol ( 2020 ) 196 : 10801085 result not older than 72 h at the beginning of every elective invasive medical procedure , such as ducial , port , intrauterine device , or feeding tube implantation . 
in this case , special hygiene protocols had to be applied to secure safe operation and prevent asymptomatic viral spread . a detailed post - interventional analysis of the outpatient working routines was performed , totaling a 37 - working day observation period of 2019 and 2020 for calendar weeks 1219 year - to - date . 
testing a total number of 74 patients or all individual 164 in - hospital cases from march 15 to may 07 , no positive rt - pcr test result for any probe analyzed was observed . discussion healthcare providers must increasingly integrate supply chain management routines into their workows . 
quality management and prediction can drive hospital efciency , care provider productivity , and patient satisfaction [ 10 ]  . during the sars - cov - 2 pandemic , cancer patients form a major risk group for severe complications [ 3 , 24 ]  . 
oncologists must weigh up potential risks of covid - 19 morbidity and mortality against the advantages of intended therapies [ 5 ] , as delaying potentially curative treatments affects oncologic outcomes . 
the vast majority of 95% of surgeons believe that timely multimodal treatments should be performed according to standard therapy indications for colorectal carcinomas despite the covid - 19 pandemic [ 1 ]  . for every month of radiotherapy deferral , head and neck cancer patients mortality risk increases by 16% , and a 4 - week delay in adjuvant chemotherapy for colorectal and breast cancer is associated with poorer overall survival [ 5 ]  . rather than cancelling indicated treatments , the current authors implemented new workow designs managing to initiate and continue treatments safely . underutilization of medical resources has negative impacts by increasing healthcare costs , decreasing access to care , and reducing efciency and productivity of care providers [ 7 ]  . 
as shown in this study , it is possible to remodel the ct progradespite reducing the number of patients , it was possible to signicantly increase the number of cts scheduled by 20.1% ( p = 0.0001 ) and performed by 13.9% ( p = 0.0001 ) , whilst controlling the time of ct machine occupation per patient during the whole shift . the most common reasons for missing medical appointments are known to be forgetting ( 35.5% ) and miscommunication ( 31.5% ) [ 28 ]  . 
while predictive models propose overbooking approaches to signicantly reduce patient waiting by at least 6% , 27% on overtime , and 3% on total costs compared to at - overbooking methods [ 7 ] , the authors department focused early on actively controlling appointment compliance while avoiding overbooking . it has been published elsewhere that pre - appointment reminder calls can effectively decrease no - show rates by 19% [ 12 ]  . 
during the pandemic , active calling helped to ensure radiation treatment initiation and continuation , alleviating patients anxiety and insecurity . patients with deferrable treatments were rescheduled after having actively been discussed in interdisciplinary cancer board meetings . 
this led to a reduced time per patient for completion of the desired treatment and was later recommended by radiation oncology specialist societies [ 4 , 15 , 18 , 20 , 29 , 30 ] , for example for bone metastases ( 1 8 gy and 5 4 gy ) and mild simultaneous integrated boost ( sib ) hypofractionation for localized prostate cancer ( pt1bt3an0m0 ) , analogously to the phase iii chhip trial [ 2 ]  . the primary transmission mode of sars - cov - 2 is described as human to human [ 16 ]  . 
it was reported that 1084 strahlenther onkol ( 2020 ) 196 : 10801085 1080 health workers in wuhan were infected and among 138 hospitalized patients diagnosed with covid - 19 , 41% were suspects of nosocomial transmission , resulting in 26% intensive care unit treatments and a mortality rate of 4.3%. 
to reduce potential nosocomial infections , the authors department aimed to avoid patient clustering , as stochastic models have identied the efcacy of reducing inter - personnel contacts [ 6 ]  . despite dedicated testing of all inpatients , neither positive tests for staff nor for patients were observed , while exploratory analyses of the rst 72 , 000 cases of covid19 in china report 3.8% of cases detected among healthcare personnel , leading to a 0.3% death rate of healthcare workers . 
despite this , the lack of observed nosocomial infections among patients and personnel and the absence of symptoms of acute respiratory distress syndrome ( ards ) within an explicit german hotspot area and regional covid - 19 treatment center lead the authors to have condence in the true nature of the results . 
these mechanisms are not subject of this analysis . conclusion during the upcoming period of recovery and increasing number of treatment facility reopenings within healthcare services , radiation oncologists will be challenged with pivotal process reconsiderations . 
as the covid - 19 pandemic is still ongoing , it will be a top priority to design actionable workows that can best prevent nosocomial infections of patients and personnel to safely continue and start radiation instead of cancelling or deferring indicated therapies . further investigation should be performed to identify noninferior treatment regimes to hypofractionate and accelerate radiation fractionation schedules and hence reduce overall facility time per patient and the associated nancial impact . 
restructuring key processes using automation might be benecial for healthcare providers to implement adapted patient ow management into future medical routines . acknowledgements the outstanding daily efforts of every single member of the radiation oncology team and its associated services cannot be expressed by words . 
expressions of gratitude belong to the team of robert vogelsang and katrin wendling for contributing actionable ideas to remodel the ct scheduling program . author contribution dennis akuamoa - boateng has rst authorship . funding open access funding enabled and organized by projekt deal . compliance with ethical guidelines conict of interest d . 
all studies performed were in accordance with the ethical standards indicated in each case . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
september 2020 der / die autor ( en ) 2020 hintergrund die bestrahlung der kraniospinalen achse ( csi ) ist seit jahrzehnten ein elementarer bestandteil bei der behandlung von kindern mit medulloblastoje nach alter des kindes und dosierung geht die behandlung jedoch mit einem erheblichen risiko fr einbuen der gedchtnisleistung und negativen auswirkungen fr die weitere psychosoziale entwicklung einher [ 1 ]  . 
eine risikoadaptierte reduktion der bestrahlungsdosis sowie eine anpassung des boost - volumens wirken sich positiv auf die gedchtnisleistung aus , ohne den onkologischen behandlungserfolg zu gefhrden [ 2 ]  . 
die protonenbestrahlung kann aufgrund ihrer vorteilhaften physikalischen eigenschaften im vergleich zur photonenbestrahlung die vom gesunden hirngewebe absorbierte dosis auerhalb des zielvolumens weiter reduzieren und somit auch potenziell das ausma der neurokognitiven einschrnkung verringern . 
 [ 3 ] doch wesentlich dazu bei , den stellenwert der protonenbestrahlung im hinblick auf das neurokognitive outcome zu klren . patienten und methode fr diese retrospektive analyse wurden 79 pdiatrische patienten des hospital for the sick children ( toronto , kanada ) und des texas childrens hospital ( houston , usa ) bercksichtigt , die im zeitraum originalpublikation kahalley ls , peterson r , ris md , janzen l , okcu mf , grosshans dr et al ( 2020 ) superior intellectual outcomes after proton radiotherapy compared with photon radiotherapy for pediatric medulloblastoma . 
die standardtherapie fr das us - kollektiv ( n = 37 ) war im untersuchungszeitraum die protonenbestrahlung , mangels verfgbarkeit der protonentechnik wurden alle kanadischen patienten ( n = 42 ) mit photonen bestrahlt . 
die bestrahlung der neuroachse erfolgte risikoadaptiert im rahmen aktueller multimodaler therapiekonzepte ( sjmb03 / clinicaltrials.gov identier : nct00085202 oder sjmb12 / clinicaltrials.gov identier : nct01878617 ) nach resektion entweder dosisreduziert mit 1523 , 4 gy oder regulr mit 30 , 639 , 6 gy . 
das boostvolumen umfasste bei keinem patienten die gesamte hintere schdelgrube , es wurde vielmehr nur das tumorbett mit einem ctv - saum von 5 bis 10 mm bis zu einer kumulativen gesamtdosis von 51 , 0 bis 59 , 4 gy behandelt . 
auch augenmerk auf einzelne subdomnen wie etwa sprachverstndnis , wahrnehmungsgebundenes logisches denken , arbeitsgedchtnis und verarbeitungsgeschwindigkeit gelegt . ergebnisse es wurden die longitudinalen ergebnisse der neurokognitiven testungen von 79 kindern untersucht , davon 37 nach protonenbestrahlung und 42 nach photonenbestrahlung . 
im hinblick auf ihre klinischen und demograschen charakteristika ist hervorzuheben , dass sich die beiden kohorten sowohl bei der verschreibungsdosis fr den boost als auch beim sicherheitssaum fr den boost signikant unterschieden . 
whrend bei der photonenbestrahlung ausnahmslos ein ctv - saum von 10 mm verwendet wurde , waren es bei 37 , 8 % der patienten in der protonengruppe lediglich 5 mm . die mediane boost - dosis war mit 55 , 8 gy im photonenarm hher als im protonenarm ( 54 gy )  . 
die weiteren charakteristika , wie etwa geschlecht , alter oder dosis der neuroachse , zeigten keine relevanten unterschiede . 1136 strahlenther onkol ( 2020 ) 196 : 11351138 kinder , die mit protonen behandelt wurden , zeigten im verlauf keine vernderung des globalen iqs im vergleich zur baseline . 
im gegensatz dazu wurde bei der photonenkohorte ein statistisch signikanter verlust von durchschnittlich 0 , 9 iq - punkten pro jahr festgestellt . bei der untersuchung des sprachverstndnisses zeigte sich in beiden gruppen weder zur baseline noch im weiteren verlauf eine signikante vernderung . das wahrnehmungsgebundene logische denken hingegen verbesserte sich sogar nach protonenbestrahlung um durchschnittlich einen punkt pro jahr , whrend nach photonenbestrahlung tendenziell eine verschlechterung von durchschnittlich 0 , 8 punkten pro jahr beobachtet wurde , jedoch ohne statistische signikanz zu erreichen . bei der analyse des arbeitsgedchtnisses blieben die ergebnisse whrend des nachbeobachtungszeitraums fr protonen unverndert zum ausgangsbefund , wohingegen nach photonenbestrahlung eine signikante verschlechterung von 2 , 2 punkten pro jahr festgestellt wurde . im gegensatz zu den anderen subdomnen zeigte sich die verarbeitungsgeschwindigkeit in beiden behandlungsgruppen gleichermaen beeintrchtigt und nahm im untersuchungszeitraum um durchschnittlich 0 , 9 punkte pro jahr smtliche tests wurden auch separat fr die sjmb03kohorte ( n = 65 ) ausgewertet . 
im vergleich zum gesamtkollektiv zeigte sich bei nunmehr gleichen rahmenbedingungen ( chemotherapie , boost - dosis und ctv - saum ) ein hnliches ergebnis : vorteile fr die protonenbestrahlung bei arbeitsgedchtnis und wahrnehmungsgebundenem logischem denken und keine vernderung bei der verarbeitungsgeschwindigkeit in beiden gruppen . 
im gegensatz zur kombinierten auswertung wurden in der protonengruppe im verlauf signikant bessere scores fr das sprachverstndnis erzielt , jedoch ging der zuvor statistisch relevante vorteil fr den globalen iq verloren . interpretation der autoren die auswirkungen einer protonenoder photonenbasierten behandlung von pdiatrischen patienten mit medulloblastom auf das neurokognitive outcome wurden erstmals mit vergleichbaren und aus demselben behandlungszeitraum stammenden protokollen untersucht . 
die ergebnisse untermauern die rationale , protonen bei der behandlung von hirntumoren mit dem ziel der bewahrung der gedchtnisleistung anzuwenden . kommentar in den letzten jahren konnte sich die protonenbestrahlung insbesondere bei der behandlung von hirntumoren im kindesalter als therapieoption der ersten wahl etablieren . trotz einer international rasant ansteigenden anzahl neuer einrichtungen stellt eine mangelnde verfgbarkeit oftmals die hauptursache dar , wenn die behandlung dennoch mit photonen durchgefhrt wird . 
ob sich jedoch die konformalere behandlung und die geringere niedrigdosis im umliegenden gesunden gewebe tatschlich in klinisch relevante vorteile bersetzen , konnte noch nicht fr alle postulierten indikationen zweifelsfrei belegt werden und wird z . 
dies ist aber von essenzieller bedeutung , denn dank stetiger verbesserungen bei diagnostik , therapie und nachsorge besiegen in deutschland ber 80 % der pdiatrischen patienten ihre onkologische erkrankung und werden zu langzeitberlebenden [ 7 ] ; 1975 waren es nur knapp 50 % . 
die rationale zur lokalen bestrahlung von tumoren des zentralen nervensystems oder der schdelbasis mittels protonen ist deshalb weithin akzeptiert , existieren doch fr viele klinisch relevante endpunkte klare dosis - wirkungs - beziehungen . so haben beispielsweise vatner et al . 
im umkehrschluss kann der benet der geringeren dosisbelastung des hypothalamus oder der hypophyse durch die verwendung von protonen bei vorliegender vergleichsplanung mit photonen abgeschtzt werden . deutlich schwieriger gestaltet sich der eindeutige beleg fr ein verbessertes neurokognitives outcome nach protonenbestrahlung . 
bereits in einer vorarbeit feststellen , dass es nach protonenbestrahlung zu keiner verschlechterung des iqs kam , jedoch erreichte die abnahme von 1 , 1 punkten pro jahr nach photonenbasierter bestrahlung keine statistische signikanz [ 9 ]  . 
fanden heraus , dass sich eine protonenbestrahlung bei der behandlung kindlicher hirntumoren im vergleich zur konventionellen bestrahlung positiv auf das neuropsychologistrahlenther onkol ( 2020 ) 196 : 11351138 1137 sche outcome auswirkt [ 10 ]  . 
wenngleich zunehmend evidenz fr eine gleichbleibende neurokognitive leistungsfhigkeit nach protonenbestrahlung geschaffen wird [ 11 , 12 ] , muss jedoch kritisch bemerkt werden , dass die aussagekraft der ergebnisse zum teil limitiert ist , da sie sich entweder auf einen historischen vergleich mit photonen beziehen oder mglicherweise einem selektionsbias unterliegen , da der soziokonomische status im protonenkollektiv deutlich erhht war . 
die kahalley - arbeit berwindet eben diese limitationen , da der vergleich zu fairen bedingungen stattfand : es kamen moderne photonenverfahren mit den gleichen ( zeitgenssischen ) protokollvorgaben im hinblick auf zielvolumendenition und dosierung bei einem im hinblick auf demograsche , klinische oder soziokonomische charakteristika vergleichbaren kollektiv zum einsatz . besonders bemerkenswert ist , dass der positive einuss nicht an einem kollektiv mit rein fokaler bestrahlung gezeigt wurde , sondern vielmehr bei patienten mit kraniospinaler bestrahlung . 
ebenso relevant drfte aber auch die anpassung des zielvolumens bei der boost - bestrahlung hin zur tumorbettbestrahlung anstelle der gesamten hinteren schdelgrube sewie es scheint , ist aber nicht nur die zerebellre integraldosis , sondern vielmehr auch die vom supratentoriellen gehirn absorbierte dosis ausschlaggebend fr das funktionale ergebnis . 
und genau da kann die protonenbestrahlung dank ihrer vorteilhaften physikalischen eigenschaften zu einer relevanten reduktion und damit einer geringeren beeintrchtigung der gedchtnisleistung beitragen . fazit allen bekannten limitationen retrospektiver analysen zum trotz liefert die arbeit von kahalley et al . 
harrabi gibt an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
moxon - emre i , bouffet e , taylor md , laperriere n , scantlebury n , law n et al ( 2014 ) impact of craniospinal dose , boost volume , and neurologic complications on intellectual outcome in patients with medulloblastoma . 
kahalley ls , peterson r , ris md , janzen l , okcu mf , grosshans dr et al ( 2020 ) superior intellectual outcomes after proton radiotherapy compared with photon radiotherapy for pediatric medulloblastoma . 
harrabi sb , bougatf n , mohr a , haberer t , herfarth k , combs se et al ( 2016 ) dosimetric advantages of proton therapy over conventional radiotherapy with photons in young patients and adults with low - grade glioma . 
clair wh , adams ja , bues m , fullerton bc , la shell s , kooy hm et al ( 2004 ) advantage of protons compared to conventional x - ray or imrt in the treatment of a pediatric patient with medulloblastoma . 
adeberg s , harrabi sb , bougatf n , verma v , windisch p , bernhardt d et al ( 2018 ) dosimetric comparison of proton radiation therapy , volumetric modulated arc therapy , and three - dimensional conformal radiotherapy based on intracranial tumor location . 
vatner re , niemierko a , misra m , weyman ea , goebel cp , ebb dh et al ( 2018 ) endocrine deciency as a function of radiation dose to the hypothalamus and pituitary in pediatric and young adult patients with brain tumors . 
kahalley ls , ris md , grosshans dr , okcu mf , paulino ac , chintagumpala m et al ( 2016 ) comparing intelligence quotient change after treatment with proton versus photon radiation therapy for pediatric brain tumors . 
gross jp , powell s , zelko f , hartsell w , goldman s , fangusaro j et al ( 2019 ) improved neuropsychological outcomes following proton 1138 strahlenther onkol ( 2020 ) 196 : 11351138 therapy relative to x - ray therapy for pediatric brain tumor patients . neuro - oncology 21 ( 7 ) : 934943 ation in pediatric patients with brain and central nervous system tumors . 
yock ti , yeap by , ebb dh , weyman e , eaton br , sherry na et al ( 2016 ) long - term toxic effects of proton radiotherapy for paediatric medulloblastoma : a phase 2 single - arm study . 
ryckman jm , ganesan v , kusi appiah a , zhang c , verma v ( 2019 ) national practice patterns of proton versus photon therapy in the treatment of adult patients with primary brain tumors in the united states . 
the treatment response for each rt technique was monitored as a secondary endpoint . patients and methods 22 patients were treated either with 140 - kv orthovoltage x - rays ( n = 11 ) or a 6 - mv linac ( n = 11 ) with two weekly fractions of 0.5 gy for 3 weeks . 
the treatment response was assessed before and 3 months after rt using a ve - level functional calcaneodynia score . results rt for painful heel spurs induced a very mild but signicant increase of h2ax foci in patients leukocytes . no difference between the rt techniques was observed . 
this trial was terminated preliminarily after an interim analysis ( 22 patients randomized )  . conclusion low - dose rt for painful heel spurs with orthovoltage x - rays or a 6 - mv linac is an effective treatment option associated with a very low and comparable radiation burden to the patient , as conrmed by biodosimetric measurements . keywords radiotherapy benign disease heel spur biodosimetry h2ax introduction the successful treatment of benign inammatory and degenerative conditions like calcaneodynia ( painful heel spur ) and painful shoulder or elbow syndrome with low - dose radiation therapy ( rt ) has a longstanding history in germany and accounts for more than a third of all rt patients treated annually [ 1 ]  . 
clinical studies documented comparable positive results for treatment schedules with single fractions of 0.5 gy or 1 gy applied twice a week for 3 or 6 weeks [ 35 ]  . 
accordingly , the iso - effective single dose of 0.5 gy over a course of 3 weeks ( cid : 2 ) sebastian zahnreich zahnreic@uni - mainz.de 1 department of radiation oncology and radiotherapy , university medical center , mainz , germany is used for radiation protection purposes to reduce the radiation burden to the patient and the risk of potential radiation - induced ( ri ) stochastic late effects such as radiation carcinogenesis [ 6 ]  . 
the risk of adverse late effects induced by low - dose rt for benign diseases is generally considered to be negligible and the benet for the patient outweighs [ 79 ]  . 
 [ 10 ] using an effective dose concept for a cumulative dose of 6 gy administered in six fractions of 1 gy predict rough estimations for the risk of ri fatal tumors of 2040 per 1000 patients for heterotopic ossication , 1.5 per 1000 patients for gonarthrosis , 0.5 per 1000 patients for heel spurs , and 1 per 1000 female patients for hidradenitis suppurativa . 
other predominant factors that inuence the risk of radiation carcinogenesis besides the target dose are the eld size , photon energies , the exposed anatomic region / organs , sex , and age at exposure . 
in general , such risk estimates are fraught with large uncertainties in the order of a factor of 2 and are expected to be much less for lowdose rt of benign diseases , since this treatment is predomstrahlenther onkol ( 2020 ) 196 : 11161127 1117 inantly performed in elderly patients with a strongly and up to nine - fold reduced excess lifetime risk for ri solid tumors when compared to young adults [ 1012 ]  . calcaneodynia is observed in 1015% of the population and is associated with severe heel pain causing restrictions and reduced quality in everyday life [ 13 , 14 ]  . 
in germany , approximately 10 , 000 heel spur patients per annum are treated by low - dose rt in about 340 active facilities offering rt for benign diseases [ 15 ]  . 
treatments are usually conducted with a medical linear accelerator ( linac ) and megavoltage ( mv ) photons or orthovoltage devices delivering x - rays in the range of 100400 kev , with a prevalence for linacs [ 15 ]  . 
compared to an orthovoltage device , rt with a linac achieves a more homogeneous dose distribution in the target volume , which has been discussed to have improved therapeutic effectiveness [ 16 ]  . 
however , the penetration depth of mv photons from a linac exceeds the cross - section of the patient and causes reections in the rt bunker that contribute to an inevitable dose burden to the patients normal tissue outside the target volume . 
socalled out - of - eld doses are also generated by scattering and leakage from the linac treatment head , collimation devices , and , to a lesser extent , by scattering from within the patients body [ 17 ]  . 
orthovoltage rt with low - energy photons has an inferior dose distribution but allows for protection of the patients healthy tissue by lead shielding which cannot be applied for high - energy photon units due to the generation of scatter radiation within the shielding equipment . 
however , for linac rt , treatment planning including eld collimation can be conducted to protect the patients healthy tissue outside the target volume . besides conventional physical measurements to determine the patients radiation exposure , the detection of biological indicators of ri deoxyribonucleic acid ( dna ) damage in peripheral leukocytes has been frequently applied for biodosimetric purposes in patients undergoing various radiologic procedures or rt [ 2029 ]  . 
immunostaining and uorescence microscopic quantication of socalled h2ax or 53bp1 foci at the level of single cells is proportional to the number of ri dsbs and therefore increases linearly with radiation dose after ex vivo and in vivo exposure with a detection threshold of a few mgy [ 22 , 26 , 27 ]  . however , it is hitherto unknown whether the largely random application of linac or orthovoltage rt for the treatment of painful heel spur is associated with a varying unwanted but inevitable radiation exposure of the patients normal healthy tissue to out - of - eld doses and differing therapeutic effectiveness . 
therefore , we conducted this prospective randomized trial as a biodosimetric approach to assess the radiation burden of heel spur patients treated either with orthovoltage x - rays or a linac by quantitation of the dsb marker h2ax in peripheral leukocytes . 
as a secondary endpoint the analgesic effectiveness was monitored based on a ve - level function calcaneodynia score ( cs ) before and 3 months after rt . patients and methods patients and radiation therapy patients suffering from painful heel spur were enrolled based on the following inclusion criteria : radiologic evidence of spur formation , anamnesis of a painful heel and functional impairment , painful symptoms for a least 3 months , age 40 years , overall condition allowing for repeated venous blood sampling , and a signed an informed consent form approved by the local ethics committee . 
the following exclusion criteria were applied : known gene defects associated with compromised dna repair ( e.g. , ataxiatelangiectasia , werner syndrome , or bloom syndrome ) , age < 40 years , previous rt or trauma in the treated anatomical region , any exposure to ionizing radiation less than 5 days before the start of rt , any additional inammatory or rheumatic disease , pregnancy , breastfeeding , intellectual disability or psychiatric disorder , legal care in health matters , and lack of a signed informed consent form approved by the local ethics committee . 
based on these criteria , 22 patients ( 36% ) of a total number of 61 entered the study between august 2016 and august 2019 , and were randomized into two groups : 11 patients ( 50% ) were treated with orthovoltage x - rays ( 140 kv , d3150 x - ray therapy system , gulmay ltd . , byeet , uk ) and 11 patients ( 50% ) were treated with a linac ( 6 mv , clinac dhx , uniquetm or truebeam varian medical systems , palo alto , ca , usa ) at the department of radiation oncology and radiation therapy at the university medical centre mainz , germany . 
for linac rt the treatment eld was dened by the aperture with no collimation , since no computed tomography - based treatment planning was strahlenther onkol ( 2020 ) 196 : 11161127 performed . 
the study was approved by the ethics committee of the medical association of rhinelandpalatinate , number 837.216.15 ( 9984 ) on 07 / 30 / 2015 , and by the expert committee of the degro ( german society for radiation oncology )  . 
according to the results of our previous biodosimetric studies based on h2ax foci quantication in peripheral leukocytes after fractionated rt of prostate and breast cancer patients [ 26 , 27 ] , 60 patients are required to detect a difference of 25% with a power of 80% and an error probability of 5% . 
to detect a difference of 10% in the cs scores with a power of 80% and an error probability of 5% , we estimated a total number of 120 participants . 
this trial was terminated preliminarily after an interim analysis ( 22 patients randomized )  . treatment response the treatment response was documented based on standardized questionnaires using a ve - level functional cs score according to [ 3 , 31 ] before and 3 months after the rst course of rt . 
data were available for 20 patients pre - rt and 19 patients post rt . blood sampling and ex vivo irradiation venous blood collection , irradiation of whole blood , and isolation of leukocytes were performed as described previously [ 26 , 27 ]  . 
1 exemplary representation of radiation therapy ( rt ) for plantar fasciitis treated either by a orthovoltage x - rays performed with a round mechanical applicator with a diameter of 15 cm or b linac rt . 
2 immunouorescence staining for h2ax ( green ) in dapi - stained ( blue ) nuclei of peripheral leukocytes 30 min after a sham irradiation , b the rst fraction of radiation therapy ( rt ) or c , d homogeneous ionizing radiation ( ir ) exposure ex vivo . 
d nuclei extracted from c as used for manual counting of h2ax foci at the level of single cells taken before rt were sham irradiated or exposed to a test dose of 0.5 gy x - rays and analyzed 30 min after irradiation to assess the individual yield of basal or ri dsbs by h2ax foci quantitation , respectively . 
ex vivo irradiation of whole blood was performed with a d3150 x - ray therapy system ( gulmay ltd . , byeet , uk ) at 140 kv and a dose rate of 3.6 gy per min at room temperature . 
shamirradiated cells were kept under the same conditions in the radiation device control room . h2ax foci quantication fixation of leukocytes , h2ax immunostaining , uorescence microscopy , image capturing , and scoring of foci was performed as described previously [ 26 , 27 ]  . 
the formula was applied to each treatment eld to obtain an integrated dose that was divided by the patients weight to obtain the ewbd . data and statistical analysis for quantication of h2ax foci in leukocytes a single sample was available and analyzed per datapoint for each patient . 
average numbers of h2ax foci per leukocyte in sham - irradiated cells before radiotherapy ( rt ) and a 30 min after ex vivo exposure to 0.5 - gy x - rays or b 30 min after rt for each patient as well as the respective mean standard deviation ( sd ) of all patients ( n = 18 ) and patients treated by orthovoltage ( n = 10 ) or linac ( n = 8 ) rt . 
c average numbers of radiation - induced h2ax foci per leukocyte 30 min after the rst fraction of rt in all patients and patients treated by orthovoltage rt or linac rt only . 
d comparison of the average yield of radiation - induced h2ax foci per leukocyte in all heel spur patients of the present study and in tumor patients as obtained in our previous studies [ 26 , 27 ] in dependence of the administered equivalent whole - body dose . 
error bars represent the sd tracted from the yield after ex vivo or in vivo irradiation . summarized patient data are provided as the mean and standard deviation unless stated otherwise . 
all levels of signicance were set at p < 0.05. results h2ax foci before radiation therapy and after irradiation ex vivo to examine the individual basal level of dsbs and the ex vivo radiation response in patients leukocytes , blood samples obtained before rt were sham irradiated or exposed to 0.5 gy x - rays and analyzed 30 min post radiation . 
thus , despite large variations in the individual background number of h2ax foci in patients leukocytes , a more uniform and comparable response after homogeneous ex vivo exposure to ionizing radiation was observed . 
there was no signicant difference in the average yield of basal ( p = 0.625 ) or ex vivo ri ( p = 0.223 ) h2ax foci per leukocyte between the two rt groups . h2ax foci after radiation therapy after the rst session of rt the frequency of h2ax foci per leukocyte exceeded the background rate in 78% ( 14 / 18 ) of all patients . 
3d shows the mean frequencies of ri h2ax foci 30 min after rt from this work related to data from our previous biodosimetric studies 30 min after rt of breast or prostate cancer patients with an average single dose of 2 gy [ 26 , 27 ]  . 
4 variation of the summed calcaneodynia score ( cs ) before and at 3 months after radiotherapy ( rt ) for a each patient and compiled for all patients or orthovoltage rt or linac rt only . 
5 shows the distribution of patients classied in the performance categories excellent ( cs sum score 90100 ) , good ( cs sum score 7085 ) , moderate ( cs sum score 4565 ) , or poor ( cs sum score 040 )  . 
information on patient characteristics is provided in table 1 . discussion in the present study we measured ri dsbs by h2ax foci quantication in peripheral leukocytes of painful heel spur patients treated with a 140 kv orthovoltage device or a 6mv linac to assess the patients radiation burden for radiation protection purposes . 
based on this outcome as well as low participation and inclusion rates , the trial was terminated preliminarily after an interim analysis ( 22 patients randomized )  . strahlenther onkol ( 2020 ) 196 : 11161127 1123 1124 strahlenther onkol ( 2020 ) 196 : 11161127 dsbs are potently induced by ionizing radiation and represent the most deleterious dna lesion causing cell death , chromosomal rearrangements , and malignant transformation [ 33 ]  . 
the by far most prominent biomarker of ri dsbs is the phosphorylated histone variant h2ax , which has been applied in numerous studies to evaluate the in vivo radiation exposure of patients after low - dose radiologic examinations like computed tomography ( ct ) ( e.g. , [ 20 , 22 , 23 , 34 ] ) and mammography [ 21 , 25 ] , or after high - dose rt of tumor patients [ 24 , 2629 ]  . 
the present study is the rst , at least to our knowledge , to apply this method with a biodosimetric intention in patients treated by low - dose rt for benign inammatory and degenerative diseases with pain relief as the second clinical endpoint . 
rt of this medical condition is very well received and frequently used in german - speaking regions but is barely applied in other , particularly anglo - american , countries [ 1 ]  . 
such geographical differences are due to fear of ri late adverse effects , which , however , are estimated to be very low or negligible for this type of local low - dose rt [ 7 , 8 ]  . 
various studies on the rt of heel spurs showed equal effectiveness for single doses of 1 gy or 0.5 gy administered twice a week for 3 or 6 weeks [ 35 , 16 ]  . 
depending on the institutional equipment , benign diseases are treated either with a linac and mv photons or with an orthovoltage device operating in the low - energy kv range . 
this instrumentation - specic difference might be associated with varying therapeutic effectiveness [ 16 ] but also with divergent exposures to undesirable out - of - eld doses [ 17 ]  . 
based on this rationale , we investigated both endpoints in this prospective randomized trial after low - dose rt of calcaneodynia patients with a linac or orthovoltage unit for a treatment schedule of 0.5 gy given twice a week over a course of 3 weeks . 
 [ 3 ] , we observed high response rates and pain reduction in up to 89% of patients at 3 months follow - up in line with improvement rates of previous studies ranging between 65100% [ 16 ]  . 
 [ 16 ] performed a retrospective study on the long - term treatment success of low - dose rt for painful heel spurs in 502 patients treated either with 610 - mv photons twice per week or with 175 kv x - rays three times per week at four different facilities in germany . 
although a better distribution of dose is achieved in the target volume for linac rt , it may increase the radiation burden of the patient through higher peripheral doses outside the primary beam caused by radiation scattering , leakage , and reections [ 17 ]  . 
besides physical dosimetry , biodosimetric attempts have been made to compare the inherent radiation exposure of different rt techniques [ 2729 ] or ct protocols [ 35 ] based on the quantication of ri h2ax foci in peripheral leukocytes . 
thresholds for this highly sensitive assay to monitor the induction of ri dsbs in vitro and in vivo have been set at 1 mgy and 3 mgy , respectively [ 22 , 36 ]  . 
so far , only few comparable studies on foci quantication of dsb repair proteins in systemic lymphocytes after a planned medical ir exposure in vivo are available for the low ewbds of the present work , which were able to demonstrate dose - dependent increments or even differences between radiation techniques . 
 [ 35 ] reported on signicantly reduced levels ofh2ax foci in peripheral leukocytes 30 min after multidetector coronary ct angiography performed with a dose - reducing sequential protocol compared to a conventional helical protocol in line with physical dose estimates . 
for otherwise identical parameterization , a higher ssd for linac rt caused an average 1.9 - fold reduction of the integral dose compared to orthovoltage rt and , conversely , the higher half - value thickness for linac rt resulted in a six - fold increment of the integral dose than for orthovoltage rt . 
this value also applied for calculated ewbd , since there were no signicant differences in the distribution of the patients bodyweight between the two radiation modalistrahlenther onkol ( 2020 ) 196 : 11161127 1125 ties . 
we observed a general slight but signicant increase of h2ax foci per cell after rt for all patients but no difference between the rt techniques nor a correlation with the ewbd . 
30 min after rt the numbers of excess h2ax foci per cell were in a low range of 0 to 0.685 , with a median of 0.104. in our previous studies on the quantication of h2ax foci in peripheral leukocytes of breast and prostate cancer patients after rt , we have shown linear doseresponse relationships and good approximations of the administered whole - body dose based on ex vivo calibration data [ 26 , 27 ]  . 
but assuming that the number of foci of dsb repair proteins in peripheral leukocytes after rt is a quantitative measure of the patients dose burden and correlates with the risk of adverse side and late effects of medical radiation exposure , it is expectedly and signicantly far lower in heel spur patients than for tumor patients . however , as we reported in our previous work [ 26 , 27 ] , the induction of dsbs in peripheral leukocytes during rt depends on various radiation and physiological parameters , which strongly limits such direct comparisons . 
although the yield of h2ax foci in peripheral leukocytes during rt of cancer patients is primarily governed by general rt parameters such as the planning target volume or the administered ewbd , we described volumeand dose - independent variations of radiation biomarkers in leukocytes among different rt techniques for breast cancer treatment which were heavily dominated by the absolute beam - on time [ 27 ]  . 
therefore , the radiation parameters between the two rt techniques of the present study , such as the eld size or the dose rate , were adjusted as well as possible to achieve comparable exposure scenarios and beam - on times , to detect the impact of diverse out - of - eld doses only . 
besides , a strong dependency of foci induction in systemic leukocytes on physical variables such as the regional blood volume and kinetics of leukocyte circulation in the exposed anatomic region has to be considered for any comparative tactic [ 22 , 24 ]  . 
these confounding factors also greatly deteriorate the accuracy of radiation biomarkers for dose estimates after rt , in particular in the range of very low doses . taken together , using a biodosimetric approach to monitor the radiation burden of heel spur patients after the rst fraction of rt with a single dose of 0.5 gy administered with a 140 - kv orthovoltage device or a 6 - mv linac , we observed a marginal but signicant overall increase in the dsb surrogate marker h2ax in peripheral leukocytes , with no difference between the rt techniques . 
schmidberger declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
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we implemented the method of failure mode and effects analysis ( fmea ) via questionnaires in our institution and introduced an adapted scale applicable for radiation oncology . methods failure modes in physical treatment planning and daily routine were detected and stratied by ranking occurrence , severity , and detectability in a questionnaire . 
the majority of interviewed experts found the analysis by using the ors easier and expected a saving of time as well as higher intraand interobserver reliability . conclusion the introduced rating scale together with a questionnaire survey provides merit for conducting fmea in radiation oncology as results are comparable to the use of vrs and the process is facilitated . keywords risk assessment quality and safety radiation protection failure analysis strahlenschutzverordnung introduction during the last few years , quality assessment in modern radiation therapy gained importance to provide adequate therapeutic options for patients [ 13 ]  . 
to secure this for german radiation oncology departments , the requirement for a risk analysis was recently implemented via the german radiation protection ordinance ( strahlenschutzverordnung ) [ 4 ]  . 
the german society for radiation oncology provided a scale in 2015 which was based on the latter [ 8 ]  . high workload in daily routine might lead to few opportunities to conduct interdisciplinary discussion rounds [ 13 , 14 ]  . 
in addition , in small institutions building of committees or even inclusion of experts on quality management might be not possible due to small numbers of employees . in this context , investigation via questionnaire surveys can serve as a feasible option to conduct the analysis [ 10 ]  . 
we repeated the investigation using our own adapted ordinal rating scale ( ors ) which we developed for german radiation oncology purposes . we compared the results investigating type and ranking of stated failure modes as well as completeness of surveys and level of agreement . 
an expert team of physicists ( n = 2 ) , physicians ( resident and senior doctors , n = 3 ) and radiotherapists ( n = 1 ) dened possible failure modes . 
corresponding to the alterations in the strahlenschutzverordnung ( german radiation pertection ordinance ) the assembled failure modes concerning radiation treatment for staff and patients and radiation planning were re - evaluated twice in 2019 . 
the methods and results of these are hereby presented . as the focus of this investigation was the implementation of a feasible rating system , details on measures for risk prevention are not reported here . three categories were dened : category 1 ( during radiation treatmentpatients safety ) , category 2 ( during physical radiation planningpatients safety ) , and category 3 ( during radiation treatmentstaffs safety )  . 
three values have been acquired : ( o ) the probability of occurrence , ( s ) the severity of possible consequences if the failure is not detected , and ( d ) the ability to detect the failure itself . a subjective score from 1 to 10 on a visual analogue rating scale ( vrs ) was given to quantify probability , severity , and detectability for every failure ( table 1 )  . 
the values of ( o ) , ( s ) , and ( d ) from all questionnaires were used to calculate the rpns , the mean rpn , and the standard deviation ( sd )  . we implemented an ordinal rating scale ( ors ) in this process and repeated the investigation . 
to evaluate the ors , a 5 - point likert scale was used . all involved experts have been interviewed about subjective easiness , expected time saving , and intraas well as interobserver reliability using the ordinal scale after completing the questionnaires . table 1 visual rating scale for rating of occurrence ( o ) , severity ( s ) and detectability ( d ) during fmea . 
 ( designations for extreme values were adapted from the literature [ 15 ] ) occurrence very rare severity none detectability almost certain regularly catastrophic absolutely uncertain table 2 ordinal rating scale for rating of occurrence ( o ) , severity ( s ) and detectability ( d ) during fmea . 
 ( the scale was developed after a literature search and adapted from the literature [ 6 , 8 , 10 , 12 ] ) 1130 occurrence severity very rare , 1 / 10 years rare , 1 / 2 years time to time , 15 / year often , 1 / month regularly , 1 / week detectability no effect or very little effect nonpermanent effects , medical treatment needed or little discrepancy to radiation plan nonpermanent effects , intensive medical treatment needed or discrepancy to radiation plan with little effect permanent effects with clearly health - threatening consequences or strong discrepancy to radiation plan with severe consequences deadly effects easy to detect , control check - ups implemented ( 1 / 100 cases might be undetected ) rather easy to detect , might stay unnoticed ( ~1 / 100 cases might be undetected ) difcult to detect , only few routine check - ups available ( 215 / 100 cases might be undetected ) very difcult to detect , no control possibilities ( > 15 / 100 cases might be undetected ) impossible to detect data were analyzed using spss statistics version 25 ( ibm , indianapolis , in , usa )  . 
according to the policy activities that constitute research at the clinic for radiation oncology , this work met criteria for operational improvement activities exempt from ethics review . a process tree for the clinical work was drawn and 7 main steps were dened during the workow : ( 1 ) a patients rst appointment at our institution including physical examination , information about the therapy and possible side effects , ( 2 ) a conference between all physicians where the radiation therapy concept is dened , ( 3 ) virtual simulation and denition of organs at risk and target volumes , ( 4 ) treatment preparation through a physicist , ( 5 ) treatment routine , results strahlenther onkol ( 2020 ) 196 : 11281134 fig . 
ptv planning target volume , ct / mri computed tomography / magnetic resonance imaging , q&a questions and answers ( 6 ) simultaneously given systemic therapies , ( 7 ) follow - up visits . 
of those , 11 were related to radiation delivery and considered a risk for a patient ( category 1 ) and 8 were related to physical treatment planning ( category 2 )  . ten were related to radiation delivery and considered a risk for the staff ( category 3 )  . failure mode evaluation we evaluated the elaborated failure modes through an expert group interview using a vrs ( scale 110 )  . 
mean rpn for the process category 1 ( during radiation treatmentpatients safety ) was 42.1 , for the process category 2 ( during physical radiation planningpatients safety ) 58.2 , and for the process category 3 ( during radiation treatmentstaffs safety ) 102.2. total mean rpn was 67.5. we repeated the expert interview after developing an ors as indicated in table 2 . 
failure modes with the highest rpns using the ors where obese patient / disabled patient , difcult positioning , inability to cope with work with critically ill patients , inability to cope with high workload and daylight lacking . assessment of the implemented scale a survey of four questions to evaluate the newly developed scale was attached to the questionnaires and was lled out by every member of the expert round ( answer rate 100% )  . results are shown in table 5 in the supplementary material . of 6 experts , all found the rating via ors to be much easier ( n = 4 ) or easier ( n = 2 ) than via vrs . 
in all , 5 experts expected a signicant saving ( n = 4 ) of time or rather a saving of time ( n = 1 ) , and 4 expected a clearly higher and 2 higher interobserver reliability . 
four expected a clearly higher and 1 higher intraobserver reliability through the ors . discussion recently , with the actualization of german radiation protection ordinance ( strahlenschutzverordnung ) [ 4 ] , a risk analysis for the use of linear accelerators in german radiation oncology is mandatory and can be conducted using the failure mode and effect analysis ( fmea ) , a tool widely used in private enterprise [ 8 ]  . fmea might be conducted in an open expert round meeting up in multiple sessions and discussing possible failure modes [ 9 , 11 ]  . 
another approach , as described by the tg - 100 working group of the aapm , is the independent evaluation by every member of the round and merging of the outcomes for example in a nal steering round [ 6 ]  . these methods are still costly in terms of time and personnel , which makes the process difcult to include in the time - consuming daily work of radiation oncology [ 12 , 17 , 18 ]  . 
our approach now represents a compromise by identifying failure mode in an expert round and evaluating those via questionnaire survey . unfortunately , this method might be restricted due to low response rate [ 10 ]  . 
also with such a method , a change in the opinions of experts due to discussions during completion of the survey cannot be excluded , but intraobserver reliability in surveys for fmea might be rather high as described by frewen et al . 
for these reasons , we clearly recommend inclusion of this professional category into the fmea process . for rating of o , s , d , and rpn , investigators might use scales as described by , for example , hug et al . 
on the other hand , several of these scales offer a valuable reference point , such as the scale in the degro recommendation which describes the occurrence quite intuitively with words like monthly [ 8 ]  . to make a rating possible for our round of six colleagues from different working areas , we used a vrs in our rst evaluation which was adapted to an existing scale [ 12 ] with reference points for the values of 1 and 10 and a rating scale in between . 
in our newly implemented scale , we dened the three values by dening groups of values ( 12 ; 34 ; 57 ; 89 , and 10 ) with denitive specication of occurrence . this might result in high interobserver reliability as denitions like rather often or rarely might be interpreted differently . 
in our scoring system , we included the possible toxicities according to the ctcae criteria as well as the important information about the effects to be acute or long - lasting . 
furthermore , we included information whether a failure mode might affect the optimal oncologic treatment through changes in dose distribution , which similarly has been described before [ 6 , 21 ]  . 
the latter aspect , which we also included in our scale , might be especially relevant for failure modes with low or very low occurrence of which the detectability in the rare case of occurrence is difcult to estimate . one limitation of our evaluation is the rather low number of failure modes in total ( n = 29 ) compared to other reports [ 9 , 11 ]  . 
this might be due to the fact that we focused on only two subprocesses in the treatment routine even though the numbers of failure modes clearly differ even between publications that describe the whole planning and treatment process [ 22 ]  . 
some of the dened failure modes in our collection can be seen as aggregations which could be split into several single failure modes ( e.g. , emergency kit missing or defect , no physician next to treatment room )  . 
we need to underline the fact that the hereby presented re - evaluation of o , s , and d was restricted to the failure modes which were described in 2017 in our rst failure modes evaluation . 
this limitation facilitated the comparison between two scales , but clearly , with every repetition of the method , several new failure modes might be taken into concern . however , with repeating usage of the method , the number of detected failure modes is expected to increase as experience with the method and growing awareness for nearmisses will lead to increased numbers . 
who also reported that fmea failed to identify many incidents which were observed by an incident learning system [ 9 , 22 ]  . a comparison between the results of the two surveys must be seen critically , as reasons for differences between rpns in the two surveys can not be clearly identied through this method . 
an example in our case is the evaluation of the risk through loud noises , as our rst survey took place during a construction phase and the rpn was clearly higher . 
the even higher sd in some rpn values might be attributed to the fact that the rpn is calculated as a multiplication product of three initially named values from 110 . 
furthermore , even though most ratings showed a decrease in sd with the use of the new scale , there are still three failure modes with a very clear increase in sd . two of those belong to category 3 ( insufcient coping of work with critically ill patients , insufcient coping of high workload )  . 
these ndings compare well to other reports whereeven though values between 1 and 1000 would be possible with the fmea methodmostly values up to 400 where reached as maximum [ 6 , 9 ]  . 
these ndings are similar to the report of yang et al . , who found approximately 90% of failure modes to be ranked with an rpn less than 100 [ 11 ]  . 
according to the recommendations of the tg 100 working group , at least the top - ranked ( 2025% ) failure modes need to be addressed with measures and the german guidelines even recommend to aim for values of less than 30 for all rpns [ 6 , 8 ]  . in our evaluation of the implemented scale , all participating experts expected a clearly higher or higher interobserver reliability using the ors . 
in addition , a clearly higher level of agreement was reached with the new scale , where a signicant agreement was shown for the rating of o , s , and rpn in all three categories . 
the higher agreement supports the thesis that use of a scale with well - dened values facilitates the process and can lead to higher reliability , even though already the cutback from ten to ve categories might lead to higher agreements . 
the group reported about very good agreement through their delphi - round - based investigation using a 4category - based scale and also about very high intraobserver reliability through different survey rounds [ 10 ]  . 
both effects can facilitate re - evaluation of the processes , e.g. , with different composi1134 strahlenther onkol ( 2020 ) 196 : 11281134 tion of experts rounds or altered numbers of experts . 
since we proposed the fmea via questionnaires to imply a time saving which makes it easier to integrate quality management into work routine , we recommend the use of the adapted ordinal scale to optimize this effect . conclusion we report the implementation of a method of failure mode and effects analysis ( fmea ) in german radiation oncology . we showed the use of a questionnaire - based evaluation of failure modes to be feasible and developed an applicable ordinal rating scale ( ors ) for the use in evaluation and reevaluation of processes in radiation oncology . 
we suggest the implementation of our scale for risk analysis in multiple radiation oncology departments to compare outcomes and improve the method . compliance with ethical guidelines conict of interest a . 
from the data , logistic - regression models were learned for establishing tumor stage , gleason score , level of prostate - specic antigen , and risk stratication , and for predicting biochemical recurrence . 
performance of the learned models was assessed using the area under the receiver operating characteristic curve ( auc - roc ) or the area under the precision - recall curve ( auc - prc )  . results results suggest that the histogram - based energy and kurtosis features and the shape - based feature representing the standard deviation of the maximum diameter of the prostate gland during treatment are predictive of biochemical relapse and indicative of patients at high risk . conclusion our results suggest the usefulness of cbct - based radiomics for treatment denition in prostate cancer . keywords prostate cancer radiomics cone - beam computed tomography biochemical recurrence radiotherapy introduction prostate cancer is among the most prevalent cancers worldwide . 
with treatment recommendation based on risk stratication , patients are still known to sometimes suffer from heterogeneous and unexpected outcomes [ 1 ] , which sugtrial registration number ce project - id 2019 - 00161 ice 3441 data sharing statement research data are stored in an institutional repository and will be shared upon request to the corresponding author . ( cid : 2 ) davide giovanni bosetti , md davidegiovanni.bosetti@eoc.ch 1 radiation oncology clinic , oncology institute of southern switzerland , via gallino , 6500 bellinzona , switzerland information and communications technology , ente ospedaliero cantonale , bellinzona , switzerland 3 medical physics , imaging institute of southern switzerland , 4 dalle molle institute for articial intelligence research , bellinzona , switzerland lugano , switzerland gests a need for additional tools to improve risk stratication and optimize effective treatment . for tumor staging and radiotherapy ( rt ) planning , imaging techniques such as computed tomography ( ct ) , magnetic resonance imaging ( mri ) , and positronemission tomography ( pet ) are widely used . 
the emerging eld of radiomics involves the automatic extraction of a range of quantitative features from such images to arrive at a comprehensive quantication of tumor phenotypes for the prediction of treatment response and outcome . 
in prostate cancer , radiomics is believed to have the potential to meet the need for increased knowledge of a presenting tumor [ 3 ] through better integration of clinical , morphological , and metabolic characteristics , and to thereby drive patient - based treatment decisions [ 47 ]  . however , methodological and technical challenges to using radiomics to this end remain [ 8 ]  . 
although some experiences with mri - based radiomics have been reported , these showed a large variability in image acquisition and challenges in image interpretation , especially in early - stage 944 strahlenther onkol ( 2020 ) 196 : 943951 table 1 characteristics of the 31 patients included in the study patient characteristic category number of patients ( n = 31 ) disease [ 9 ]  . 
better reproducibility and robustness were reported for ct - based radiomics features [ 2 , 10 , 11 ]  . computed tomography is commonly used for both virtual simulation and image - guided radiotherapy [ 12 ] , with cone - beam computed tomography ( cbct ) being performed for daily set - up verication . 
risk stratication and prediction of treatment outcome based on cbct - based radiomics features would be benecial for the individual patient , as it would require patients to no longer be exposed to additional radiation and personal stress ; in addition , it would reduce healthcare costs . 
the purpose of our study therefore was to investigate if cbct - based radiomics features correlated with clinical tumor stage ( t ) , gleason score ( gs ) , level of prostate - specic antigen ( psa ) , risk category , and biochemical recurrence . 
to the best of our knowledge , ours is the rst study to address the value of cbct - based radiomics for patient - based risk stratication and prognosis . age ( years ) risk group [ 14 ] gleason score t stage [ 13 ] psa value median ( range ) intermediate high 3 + 3 = 6 3 + 4 = 7 4 + 3 = 7 4 + 4 = 8 t2bt2c t3b < 10 ng / ml 1020 ng / ml > 20 ng / ml 6 months > 6 months median ( range ) median ( range ) ( 5480 ) 2 ( 6.4% ) 18 ( 58.1% ) 11 ( 35.5% ) 12 ( 38.7% ) 4 ( 13.3% ) 5 ( 16% ) 5 ( 16% ) 5 ( 16% ) 14 ( 41.2% ) 4 ( 13.3% ) 11 ( 35.1% ) 1 ( 3.2% ) 1 ( 3.2% ) 9 ( 31.9% ) 17 ( 54.8% ) 5 ( 13.3% ) 4 ( 13.3% ) 5 ( 16% ) 22 ( 70.7% ) 21 ( 67.7% ) 10 ( 32.3% ) 28 ( 90.3% ) 3 ( 9.7% ) 70 months ( 6096 ) 45 months ( 3167 ) androgen deprivation therapy with lhrh agonists pelvic lymph node rt biochemical recurrence follow - up ( years ) time to failure ( years ) for each characteristic , the average and percentage over all patients per category are reported , except for age , follow - up , and time - to - failure , for which the median and range are reported psa prostate - specic antigen , t tumor , rt radiotherapy , lhrh luteinizing hormone - releasing hormone peristalsis are known to affect the calculation of radiomic features [ 16 ] , 10 patients with such streaking artifacts on their images were excluded from the primarily selected study population . 
two more patients were excluded because of the presence of a urinary catheter that showed on the cbct image as a bright structure inside the prostate gland . finally , four patients were excluded because the prostate gland was partially outside the cbct eld of view , leaving us with a population of n = 31 patients for our study . 
table 1 summarizes the clinical details of the 31 patients thus enrolled . extraction and selection of radiomics features at the time of accrual , cbct scans were performed in our institute on a weekly basis . 
all images available for our materials and methods study population patients with localized prostate adenocarcinoma who had received radical radiotherapy ( with or without androgen deprivation therapy ) in our institute between 2009 and 2013 were retrospectively enrolled in our study . 
the study protocol was approved by the local ethics committee ( ce project - id 2019 - 00161 ice 3441 ) and all involved patients signed an ad hoc informed consent . 
baseline clinical data per patient , including age , histological grade , t - stage , n - stage , and psa , were extracted from their respective medical record . 
the rst step is identication of the region of interest ( roi ) and segmentation , where the roi is taken as the whole prostate gland drawn on each cbct slice . 
the contouring tool of the eclipse treatment planning system ( varian eclipse system tps , version 13.7 ) was used by an experienced radiation oncologist to manually segment the prostate gland on each cbct scan . 
based on intensity and shape , 31 features remained . since stability of image features at a single timepoint is of primary importance for correlating variation over time with treatment response [ 18 ] , the stability of each radiomics feature was evaluated through a testretest procedure [ 19 ]  . this procedure was applied to nine pairs of consecutive cbct scans from patients who had received a second scan within the same rt session because of improper bladder and rectal preparation . 
out of the 31 radiomics features based on intensity and shape , 15 features were identied as stable ( table 2 )  . these features were subsequently discretized into four bins table 2 the stable radiomics features included in the study radiomics feature type feature name histogram - based features 90percentile energy kurtosis maximum range rootmeansquared skewness totalenergy majoraxis maximum2ddiametercolumn maximum2ddiameterrow maximum2ddiameterslice maximum3ddiameter minoraxis surfacevolumeratio shapeand size - based features the features were selected through a testretest procedure based on two consecutive cbct scans from 9 patients who received two scans within the same rt session . 
a detailed description of the features can be found in the appropriate literature [ 17 ] 946 strahlenther onkol ( 2020 ) 196 : 943951 through unsupervised equal - frequency binning , to reduce the risk of overtting and to mitigate small sample size effects [ 20 ]  . 
this binning procedure amounted to sorting the established feature values into four intervals of equal frequency , which were subsequently taken as re - scaled values for our further analysis . per patient , up to ve cbct scans were selected , resulting in longitudinal series of at most ve values per feature . as 15 stable features were selected by the testretest procedure and each of these was observed at potentially ve different times , a total of 75 unique features were dened . in addition , for each of the original 15 stable features , 15 synthetic features were derived over the longitudinal series of values , which are the minimum value , the maximum value , the standard deviation , the range of the ve values , the mean over the ve values , and the numerical difference between each pair of values ( such as the value at time 4 minus the value at time 2 )  . 
all in all , a total of 300 radiomics features ( the 75 primarily dened features plus the 225 derived synthetic ones ) were used in our analysis . statistical analysis the information content of each ( discretized ) radiomics feature separately and of all feature pairs were analyzed with respect to tumor stage , gleason score , psa level , and risk group related to the tumor , and for predicting biochemical treatment failure . 
for each separate feature and each feature pair , a logistic regression classication model was tted to the data , using a stratied crossvalidation scheme with three folds and ten replications [ 22 ]  . with the cross validation , a stratication scheme was employed to account for the small number of patients with biochemical treatment failure by constructing three folds over the study population , with each fold including a single patient in whom treatment had failed . 
the classication performance of each constructed model was evaluated by its area under the receiver operating characteristic curve ( auc - roc ) or its area under the precision - recall curve ( auc - prc ) , where the auc - roc was the performance measure of choice for balanced datasets and the auc - prc was the measure chosen for unbalanced datasets [ 23 ]  . 
with each area under the curve , a 95% condence interval was computed from the t distribution using a corrected deviation from the sample mean to account for dependences arising from replication [ 24 ]  . for comparison purposes , also non - informative logistic regression models without any features were evaluated by their area under the curve . 
to test whether or not a constructed radiomics - based model had a signicantly higher area under the curve than its associated non - informative model , one - sample student t - testing was employed , once again using the corrected variance [ 24 ]  . 
as model performances worse than that of a non - informative model are not of ( clinical ) interest , upper - tailed testing was used , at the level of signicance = 0.01. 
to correct for the testing of multiple hypotheses , bonferroni correction was used . results table 3 lists the best - performing logistic regression models for identifying specic categories from among the range of possible categories for the risk group associated with the tumor , the clinical tumor stage , the gleason score , and the psa level , respectively , and for predicting biochemical recurrence . 
each row in the table reports the best model found for a specic category and states its performance along with the performance of the non - informative model for the same category . 
since for the category of psa lower than 20 ng / ml and for biochemical recurrence , data from just 5 and 3 patients , respectively , were available , the models constructed for these categories were evaluated using the area under the precision - recall curve ( auc - prc ) for imbalanced datasets . for the category of tumor stages up to and including stage t2c , information was available from just 2 patients and no model was constructed . 
with each reported area under the curve , the associated 95% condence interval is indicated ( except for the model for predicting biochemical recurrence , which will be discussed presently )  . 
2 illustrates the roc curves obtained from the best - performing models constructed for risk stratication , tumor stage , gs , and psa level using in - sample evaluation . for each model presented in table 3 ( except for the model for biochemical recurrence ) , the null hypothesis of it having a performance at most equal to the associated non - informative model was rejected at the adopted level of signicance = 0.01 ; in fact , the probability of obtaining the observed difference in performance if the null hypothesis were true was found to be smaller than 0.00001. each of the constructed models involves two synthetic radiomics features . 
the models included histogramand shape - based radiomics features in roughly equal propostrahlenther onkol ( 2020 ) 196 : 943951 948 strahlenther onkol ( 2020 ) 196 : 943951 fig . 
2 receiver operating characteristic curves obtained from the best - performing models constructed for risk stratication , tumor stage , gleason score , and prostate - specic antigen ( psa ) level , using in - sample evaluation rtions , where histogram - based features constituted 56% of the total of involved features and shape - based features amounted to 44% of the total . 
among the selected features , the histogram - based energy feature and the shape - based maximum2ddiameterslice feature occurred most often . for predicting biochemical recurrence , logic regression models were constructed using information from 30 patients instead of 31 : the information from a single patient was removed from the dataset because of a missing value . since from among the remaining 30 patients just 3 patients experienced biochemical treatment failure , the constructed models were evaluated using the area under the precisionrecall curve ( auc - prc )  . 
each of these models includes a pair of synthetic radiomics features . the models included histogramas well as shape - based radiomics features , where the histogram - based features constituted 80% of the total of involved features and the shapebased features amounted to 20% . 
as the ten models for predicting biochemical recurrence showed an auc - prc equal to 1 for each fold in each replication , averaged performance was associated with zero variance and , hence , no condence interval could be established and no meaningful t test could be performed . discussion with radiomics rapidly gaining scientic interest for its potential clinical implications in general , the current study was the rst to explore the value of cbct - based radiomics in prostate cancer . 
as medical imaging for treatment setup is common practice in this eld , using cbct - based radiomics for both diagnostic and prognostic purposes has the advantage of not having to expose patients to additional radiation and personal stress . the potential of radiomics features extracted from cbct images has been addressed before in non - small cell lung cancer ( nsclc ) patients . 
 [ 25 ] tested the reproducibility of cbct - based radiomics features for ncslc patients and found that when the employed imaging protocol was consistent and cbct images were limited to those with less than 1 cm of tumor motion , some radiomics features were robust to noise and poor image quality . 
 [ 26 ] showed that comparable prognostic information can be derived from cbct images acquired prior to the rst fraction of treatment as from ct images for non - small cell lung cancer patients . 
the results from our study suggest that both histogramand shapebased features have the ability to classify prostate cancer , with especially the histogram - based energy feature and the shape - based maximum2ddiameterslice feature standing out for this purpose . 
the best - performing models for establishing the gs , clinical tumor stage , and risk group included radiomics features related to the shape variation among the cbct scans performed at the beginning , during , and in the last week of treatment . 
in ct images , the intensity of the voxel , captured by the histogram - based radiomics features , corresponds to the hounseld units ( hu ) linked to the tissue density travelled by the x - rays , which are widely used for delineation of tumor volume and organs at risk [ 10 ]  . with respect to biochemical recurrence , especially the histogram - based radiomics features appear to have predictive value , with the range feature standing out . 
however , also the shape - based maximum2ddiameterslice.std feature describing the standard deviation of the maximum diameters of the prostate gland during treatment occurs among the best - performing models of biochemical recurrence , suggesting that it may be predictive of treatment failure . 
as high - risk patients are typically associated with a worse prognosis , this nding may be indicative of the added value of shape - based radiomics features for patient risk stratication . 
with interim medical imaging being performed occasionally to decide on treat950 strahlenther onkol ( 2020 ) 196 : 943951 ment escalation or on adapted rt planning [ 3 ] , this nding moreover suggests further tailoring of prostate cancer treatment by adjusting the duration of androgen deprivation therapy , which is currently withheld from low - risk patients and is administered for 6 months and up to 2 years for patients with intermediate and high risks , respectively [ 3133 ]  . the relatively large number of models that were able to perfectly predict biochemical treatment failure suggests that the logistic regression procedure may have overtted the models to the small patient sample used for our study , which involved just 3 patients with biochemical recurrence . as an explanation for the perfect performance of the model reported in table 3 , fig . 
the gure shows that the 3 patients with biochemical treatment failure could be identied by small values for both features , where all patients with a successful treatment outcome presented with a high ( er ) value for at least one of the two features . 
the impact of this nding on the potential of cbct radiomics needs further investigation , especially because cbct images are generally less accurate compared to conventional ct images [ 26 ]  . thus far , studies analyzing the performance of cbctbased radiomics addressed the prognostic value of the rst cbct scan performed compared to the planning ct [ 26 ]  . our study now suggests the potential of radiomics features extracted from longitudinal series of cbct images . 
despite the good performance of the models constructed in our study , the inclusion of such features has to be interpreted with caution , given the retrospective nature of the study , the limited sample size , and the small number of patients with a biochemical recurrence . 
on the other hand , however , all patients involved in the study referred to a single center , with a homogeneous treatment modality and cbct images acquired with the same linear accelerator . 
also the exclusion of patients with cbct images unsuitable because of artifacts , the presence of a urinary catheter , or the prostate gland being partially outside the eld of view cannot have introduced any selection bias into the study results because none of the reasons for these exclusions are correlated with the clinical parameters investigated . 
still , further studies with larger numbers of patients and a longer follow - up are called for before any denite conclusions about the potential of radiomics in prostate cancer can be drawn . compliance with ethical guidelines conict of interest d.g. 
deantonio declare that they have no competing interests . ethical standards the study protocol was approved by the local ethics committee ( ce project - id 2019 - 00161 ice 3441 ) and all patients declared their written informed consent . 
tissue markers derived from tumor biopsies usually represent only a small tumor subregion at a single timepoint and are therefore often not representative of the tumors biology or the biological alterations during and after treatment . 
in total , 25 studies that explored the ability of radiomics to predict tumor biology and phenotype in hnscc and 28 studies that explored radiomics to predict post - treatment events were identied . 
all studies to date were retrospective and none of the above - mentioned radiomics signatures have been validated in an independent cohort using an independent software implementation , which shows that transferability due to the numerous technical challenges is currently a major limitation . 
however , radiomics is a very young eld and these studies hopefully pave the way for clinical implementation of radiomics for hnscc in the future . keywords prognostic biomarkers quantitative image analysis computed tomography positron emission tomography magnetic resonance imaging introduction the term squamous cell carcinoma of the head and neck ( hnscc ) represents a highly heterogeneous group of malignancies , arising mainly from the oral cavity , pharynx , and larynx . 
they contribute 46% of all cancer cases , with a globally rising incidence over the last decades [ 1 , 2 ]  . outcome is still unsatisfactory , not exceeding 60% overall survival , especially for advanced stages [ 3 ]  . 
aside from well - established clinical biomarkers such as smoking history , which seems to be of both prognostic and predictive value [ 7 , 8 ] , and the standardized uptake value ( suv ) in fdg - pet - ct , which is prognostic and used for guiding treatment ( e.g. , neck dissection after radiotherapy ) [ 9 , 10 ] , only human papillomavirus ( hpv ) status , programmed death - ligand 1 ( pd - l1 ) , and immune cell inltration are validated and broadly recognized . 
all three show some limitations and only the rst two are routinely used . hpv status is at the present time the strongest prognostic biomarker in hnscc , but its relevance is limited to strahlenther onkol ( 2020 ) 196 : 868878 oropharyngeal cancer [ 11 ] , where it has already been introduced into clinical staging [ 12 ]  . 
at this specic disease subsite , hpv and its surrogate p16 upregulation , detected via immunohistochemistry , are strongly prognostic for all situations ( primary diagnosis or after progression [ 13 ] ) irrespective of the primary treatment , i.e. , chemoradiotherapy [ 7 ] or surgery [ 14 ]  . 
however , there still exist hpv - positive subgroups with distinct prognoses based on further clinical and biological factors , such as smoking or cd8 cell inltration [ 7 , 15 ]  . 
pd - l1 expression , as a mediator of t cell inhibition , has an ambiguous prognostic role , which is partially explained through differences in the assessment ( i.e. , tumor cells only versus immune cell versus combined ) [ 16 ] , but has a clear positive predictive role regarding the response to immunotherapy [ 17 ]  . the search for novel tissue biomarkers continues with unreduced intensity , and through implementation of elaborated modern techniques , promising targets could already be identied : targeted next - generation sequencing ( tngs ) for dna analysis revealed the prognostic role of among others tp53 , notch1 , kdr [ 18 ] and tumor mutational burden ( tmb ) [ 19 ]  . 
nanostring technology ( nanostring technologies , inc , seattle , wa , usa ) and other transcriptome analyses developed signatures inuencing outcome , closely related to hypoxia , stem cell markers [ 20 ] , and immune micromilieu ( cytokine signaling , t cell function , interferon gamma ) [ 21 ]  . 
a prospective validation of such biomarkers is currently under way . additionally , a rapidly growing research eld is the identication of blood or so called liquid biopsy biomarkers , which require only minimally invasive blood sampling and could speed up decision making for diagnosis and treatment of hnscc . 
several retrospective studies distinguished among others an enhanced neutrophil to lymphocyte ratio , elevated c - reactive protein ( crp ) , and circulating tumor cells to be related to negative prognosis [ 22 ]  . an evolving new type of tumor marker derived from quantitative image analysis referred to as radiomics . 
this research eld is mostly driven by computational advances in the analysis of a large amount of imaging data [ 2 ] and the availability of diagnostic images ( ct , mri , pet ) for basically every cancer patient . 
radiomic features to describe tumor tissue include tumor shape , rst - order features quantifying the distribution of voxel intensities within the tumor volume , higher - order features such as the tumors texture , and features calculated on transformed images . in a proof of principle , in a retrospective analysis of large patient cohorts treated with radiotherapy by aerts et al . from the maastricht group , radiomic features representative for tumor heterogeneity correlated with tumor stage and were found to be prognostic across different cancers , including hnscc [ 23 ]  . 
the authors validated their radiomics signature using two independent hnscc patient cohorts from different institutions and subsequently in a third independent cohort of patients with oropharyngeal cancer [ 24 ]  . tumor heterogeneity is a well - known and important prognostic factor in hnscc : tumor hypoxia measured by oxygen electrodes or immunohistochemistry is a robust prognostic marker and is characterized by high spatial and temporal heterogeneity [ 2527 ]  . 
tumor hypoxia can also be measured in liquid biopsies based on secreted markers such as osteopontin [ 28 ]  . importantly , radiomics has a great potential to overcome the classical limitations of tissueand blood - derived tumor markers . 
tissue markers derived from tumor biopsies usually represent only a small tumor subregion at a single timepoint and are therefore often not representative of the tumors biology or the biological alterations during and after treatment . 
this very limited information is likely a major reason why the majority of tissue markers investigated in preclinical and clinical studies by immunohistochemical approaches were of low reproducibility in the past [ 28 ]  . similarly , liquid biopsies give an overall picture of the tumors secreted factors but completely lack any spatial resolution . 
radiomics has the potential to give complete threedimensional information regarding tumor make - up and , in addition , allows for non - invasive repetitive analysis based on follow - up images that are increasingly used in clinical routine for treatment adaptation . in this review , we aim to summarize available radiomics studies in hnscc with a focus on prognostic markers , correlation to tumor biology , and inherent limitations of the radiomics approaches used so far . materials and methods to assess the correlation of radiomics to tumor biology and treatment outcome in hnscc , we conducted a comprehensive literature search in pubmed using the keywords radiomic and head and neck cancer . the search results were screened for their appropriateness based on title and abstract . 
for the correlation of radiomics with tumor biology , studies reporting results on the correlation of radiomics analysis with tumor biology , biomarkers , or phenotypes in hnscc were included . 
for the correlation of radiomics with treatment outcome , studies reporting results on local tumor control , locoregional control , overall survival , progression - free survival , and side effects were included . 
reviews were screened to nd additional studies and data . 870 results correlation of radiomic biomarkers with tumor biology in hnscc we identied a total of 25 studies that explored the ability of radiomics to predict tumor biology and phenotype in hnscc , with the majority using hpv status ( n = 9 ) or the possibility to differentiate malignant from normal tissue ( n = 9 ) as the endpoint . 
studies were mostly characterized by small patient numbers , with only 9 out of 25 studies investigating > 100 patients , three studies 50100 patients , and the remaining 13 studies < 50 patients . 
only two studies reported a negative outcome : one study could not nd a correlation with hpv status [ 39 ] and one study did not nd a correlation to tp53 and kmt2d . table 1 studies investigating the correlation of radiomic biomarkers with tumor biology raja et al . 
 [ 29 ] a , b , d hpv status dna methylation subtypes genomic features and / or expression subtypes nsd1 notch1 cdkn2a pik3ca hypoxia pd - l1 expression cell count tp53 ki - 67 fat1 kmt2d meyer et al . 
 [ 50 ] bd auc area under receiver operating characteristic astudies that found no correlation of radiomics and the investigated endpoint bstudies that included < 50 patients cstudies that included 50100 patients dstudies without a validation cohort . 
if reported , quality measures of the models ( auc , specicity , sensitivity , or accuracy ) are included crispin - ortuzar et al . [ 28 ] c , d ( auc = 0.833 ) chen et al . 
 [ 49 ] c , d ( auc = 0.71 ) strahlenther onkol ( 2020 ) 196 : 868878 table 2 studies investigating the correlation of radiomic biomarkers with treatment outcome endpoint treatment outcome ( local control , lc ; locoregional control , lrc ; progression - free survival , pfs ; overall survival , os ) predictive signature overall survival ( radiomic and clinical features ) detection of subvolumes with treatment failure xerostomia prediction weight loss sensorineural hearing loss radiation - induced trismus bogowicz et al . 
 [ 70 ] ( auc = 0.70 ) thor et al . [ 77 ] b , d ( auc = 0.85 ) auc area under receiver operating characteristic astudies that found no correlation between radiomics and the investigated endpoint bstudies that included < 50 patients cstudies that included 50100 patients dstudies without a validation cohort . 
if reported , quality measures of the models ( auc , concordance index [ c - index , ] or precision ) are included however , the same study found a correlation to fat1 [ 29 ]  . for all clinical and biological endpoints investigated , the used imaging modalities as well as number of patients are summarized in table 1 . prognostic radiomic biomarker for hnscc we identied 28 studies that explored the ability of radiomics to predict post - treatment events ( treatment outcome or side effects ) in head and neck cancer ( table 2 )  . 
the main radiotracer used in pet imaging was uorodeoxyglucose ( fdg ) , with one exception where uorothymidine ( flt ) was used in an exploratory study in a small cohort of patients [ 52 ]  . in total , three studies investigated multifactorial prognostic models on large cohorts of patients , where radiomic features were combined with clinical factors . 
 [ 55 ] showed that a multifactorial nomogram resulted in better prediction of overall survival ; however , this study did not include hpv as one of the clinical prognostic factors . 
so far , only one study reported on the predictive value of radiomics for combined treatments with radiotherapy and systemic agents in head and neck cancer [ 56 ]  . 
the authors were able to identify sub872 strahlenther onkol ( 2020 ) 196 : 868878 groups of patients treated with cetuximab who responded as well as patients treated with cisplathowever , this study lacks external validation . 
a development in the eld is the introduction of deep learning , which may outperform radiomics - based models in the future [ 58 ]  . in the domain of side effects prediction , the following endpoints have been investigated : xerostomia , weight loss , sensorineural hearing loss , radiation - induced trismus . 
although radiomic features from all the imaging modalities ( ct , mr and pet ) were shown to correlate with xerostomia , none of the radiomics models performed better than or showed added value to the dose parameters . technical challenges in dening radiomic biomarkers for hnscc in our extensive literature search for radiomics signatures correlated with tumor biology or treatment outcome , we have observed that the modality of choice for radiomics analysis in head and neck cancer is ct . 
in prospectively collected data , this problem may be solved by the use of iterative metal artifact reduction reconstruction in ct [ 81 , 82 ] and dedicated mr sequences [ 83 ]  . despite the large variety of pet radiotracers , we found only two radiotracers other than 18f - fdg studied in the context of hnscc radiomics . 
1 the main technical challenges in robust radiomics models are delineation differences , metal artifacts , the ct to pet mismatch due to different positioning or swallowing or respiratory motion , and the imaging at different timepoints after contrast injections . 
in the case of hnscc , the delineation agreement of three independent observers was reasonably high ( dice coefcient = 0.72 ) and different contours resulted in reduced but acceptable feature stability ( 60% stable of 1404 features ) [ 84 ]  . 
the consequence is a lack of knowledge about radiomic feature stability and performance in the presence of motion in hnscc . in the process of diagnosis and staging in hnscc , multimodality imaging is acquired . 
thus far , studies have shown that deformable image registration does not fully account for different head positioning [ 86 ]  . discussion this review found that radiomics has the potential to inuence treatment decisions in hnscc . 
to date , none of the above - mentioned radiomics signatures have been validated in an independent cohort using an independent software implementation , which shows that transferability due to the numerous technical challenges is currently a major limitation . 
one technical advancement is distributed learning approach that have shown promising results to enable easier sharing of data between institutions and large - scale radiomics analysis [ 87 ]  . an ideal biomarker is non - invasive , prognostic , predictive , has a high spatial and temporal resolution , and is cheap . 
for radiomic biomarkers the spatial resolution depends on the voxel size of the imaging modality and is higher for ct and mr imaging compared to pet imaging . for pet imaging , it was shown that more aggressive subvolumes of the tumor can be determined using radiomics , which might be a target for intensication of local treatment 874 strahlenther onkol ( 2020 ) 196 : 868878 fig . 
only slightly more than half of the studies were performed using a validation cohort ( vc ) and many studies had less than 100 patients ( < 100 ) included . 
this enables a more comprehensive characterization of the disease and the individual patient situation , and enables a better weighting of treatment options . tissue biomarkers such as hpv status and pd - l1 have already been validated as prognostic and predictive markers in prospective clinical studies [ 11 , 16 ]  . 
validation of new biomarkers is a multi - phase process , starting from exploration and ideally leading to a routine clinical practice . a safe introduction of imaging biomarkers was recently suggested in a consensus guideline by oconnor et al . 
this can be done by distributed learning approaches that make data sharing and privacy protection easier . there are currently six studies open and registered at clinicaltrials.gov prospectively evaluating radiomics as a prognostic biomarker in hnscc . 
without the support of methods from the eld of articial intelligence ( ai ) and machine learning , a complete evaluation of the available image information is hardly feasible in clinical routine . 
besides detection and segmentation of lesions , ai allows the extraction of a vast number of quantitative imaging features from structural or functional imaging data that are typically not accessible by means of human perception . 
within the large eld of ai , radiomics is the subdiscipline that deals with the extraction of quantitative image features as well as the generation of predictive or prognostic mathematical models . 
this review gives an overview of the basics , methods , and limitations of radiomics , with a focus on patients with brain tumors treated by radiation therapy . keywords articial intelligence machine learning deep learning textural features radiotherapy multiparametric positron emission tomography / magnetic resonance imaging ( pet / mri ) introduction the diagnosis of brain tumors and the assessment of response to radiotherapy [ 14 ] are mainly based on the results of modern neuroimaging techniques and , essentially , the histomolecular examination of tissue samples collected during tumor resection or biopsy . 
for decades , brain tumor patients have been diagnosed by means of structural neuroimaging techniques such as contrast - enhanced computed tomography ( ct ) or magnetic resonance imaging ( mri )  . 
in combination with the anatomic information , these methods provide functional and metabolic parameters that are of great benet in the assessment of , e.g. , treatment response or estimation of prognosis . 
however , with the increasing amount of data available for diagnosis , a complete , accurate , and timely evaluation of the data in clinical routine is almost impossible without considerable computer support . since methods from the elds of articial intelligence ( ai ) and machine learning allow for a partial or full automation of various steps within the diagnostic routine , it is not surprising that these methods are investigated extensively and have already been applied in clinical routine in some cases . 
these features can be combined with conventional imaging parameters from structural and molecular neuroimaging as well as with clinical data such as the patients age or molecular markers to develop predictive or prognostic mathematical models that are subsequently used to answer clinical questions , such as the assessment of treatment response to radiation therapy or the non - invasive diagnosis of molecular parameters [ 7 ]  . 
the extraction of quantitative imaging features as well as the generation and evaluation of mathematical models for diagnosis is termed radiomics and can be regarded as a special application of ai [ 812 ]  . however , the use of these computer - based methods must be carefully and critically evaluated . 
this review article gives an overview of the basics , methods , and limitations of radiomics , with a special focus on feature - based radiomics in brain tumors treated by radiation therapy . radiomics radiomics aims at the extraction of quantitative parameters from routinely acquired medical imaging data , thereby allowing additional data analysis at low cost . 
in classic radiomics approaches , sometimes also called feature - based radiomics , the radiomics features to be extracted are predened and calculated from a manually or semi - automatically segmented image . 
furthermore , image segmentation is not necessarily required for deep learning - based radiomics , despite providing image segmentations usually improves model performance . although most of the radiomics models have to prove their value in the clinical setting , the process of feature extraction applies semior fully automated methods from advanced statistics and machine learning and may as such lead to 850 strahlenther onkol ( 2020 ) 196 : 848855 more robust , reproducible , and reliable results compared to the reader - dependent clinical interpretation of imaging data . feature - based radiomics to calculate radiomics features , manual or semi - automatic segmentations of the region of interest ( roi ) or volume of interest ( voi ) are mandatory . 
however , including information contained in the inltration zone of the lesion by also considering signal abnormalities on t2 - weighted or uid - attenuated inversion recovery ( flair ) mri provides a more realistic representation of the whole tumor and allows the radiomics analysis to be performed on a larger segment , potentially encoding more information and resulting in a better diagnostic performance . 
although the number of studies using amino acid pet images for radiomics analysis is still low , especially the combined analysis of amino acid pet and mri radiomics encodes more diagnostic information than either modality alone [ 13 , 14 ] and might gain clinical relevance . in patients with brain tumors , image segmentation in clinical routine is usually performed manually on ct or mri for the purpose of radiotherapy planning or volumetric assessment of therapy response . 
however , a manual , three - dimensional differential segmentation of tumor regions with contrast enhancement , necrosis , and perifocal edema is laborious , time consuming , and strongly dependent on the performing physician . 
methods from the eld of ai including textural feature analysis and deep learning - based methods are already available and currently under investigation for routine clinical application [ 1521 ]  . as mentioned above , radiomics aims at the extraction of quantitative imaging features from routinely acquired imaging data . 
one of the rst preprocessing steps is interpolation of the imaging data to isotropic voxel spacing , which allows for a better comparison of heterogenous , multi - institutional imaging data . 
while upsampling introduces articial information and might increase image noise , downsampling conversely incurs information loss . consequently , there is currently no clear recommendation for either of the two procedures [ 22 ]  . discretization or quantization of image intensities is of particular importance to allow for comprehensible feature extraction [ 22 ]  . 
the rst method performs a discretization of the image intensities to a xed number of bins , which allows for a direct comparison of feature values across different patients and partly performs an image normalization , which is of importance for imaging procedures such as structural mri that are usually acquired in arbitrary units . however , no correlation to the original image intensities can be established . 
of note , the image discretization has a substantial impact on the extracted radiomics features and , hence , on the reproducibility of the results [ 22 ]  . normalization of the image intensities ensures a better comparability of the results between different scanners , protocols , and patients . 
other typical preprocessing steps include , but are not limited to , spatial smoothing , noise reduction , spatial resampling , brain extraction , and corrections of mri eld inhomogeneities . following image preprocessing and segmentation , radiomics features can be calculated , most of which reect tumor heterogeneity . 
since the radiomics features are mathematically predened and based on a huge number of slightly different mathematical denitions , a large number of radiomics features ( usually more than 1 , 000 ) can be extracted from medical images . 
textural features or second - order statistics : textural features represent the statistical relationship between the intensity levels of neighboring pixels or voxels or groups of pixels or voxels within the segmented lesion strahlenther onkol ( 2020 ) 196 : 848855 and , thereby , quantify image heterogeneity . 
the most commonly used matrices for calculation of textural features are the gray - level run - length matrix ( glrlm ) , which encodes the size of homogenous runs for each image intensity [ 26 ] , the neighborhood gray - level different matrix ( ngldm ) , which corresponds to the difference of intensity levels between one voxel and all of its neighbors in three dimensions , and the gray level co - occurrence matrix ( glcm ) [ 27 ] , which represents the frequency of occurrence of two intensity levels in neighboring pixels or voxels within a specic distance along a xed direction . 
higher - order statistics features are computed after the application of specic mathematical transformations or lters that aim at highlighting certain aspects of the segmented lesion such as repeating patterns , edges , histogram - oriented gradients , or local binary patterns . typical mathematical transformations used for the extraction of higher - order statistics features are wavelet or fourier transforms , fractal analysis , minkowski functionals , or the laplacian transform of gaussian - ltered images ( laplacian of gaussian ) [ 28 ]  . in summary , a large number of features can be calculated from a single segmented lesion , leading to the problem of distinguishing the parameters relevant to the clinical problem under investigation from the irrelevant and redundant ones . 
this so - called feature selection is of high importance for generating a meaningful predictive or prognostic model from the computed features , especially if the number of available datasets is limited . 
feature selection uses advanced statistical methods to identify a subset of features that are neither redundant , constant , duplicated , irrelevant , nor highly correlated [ 12 ]  . it should be noted that improper feature selection can also lead to overtting , i.e. , if a very homogenous dataset from the same scanner acquired with the same protocol is used for feature selection , the features identied as relevant in this particular setting may not be relevant in other settings . 
here , overtting denotes the generation of a model that corresponds too closely or exactly to a particular set of data , whereby it fails to reliably predict outcomes from so far unseen observations . 
one way to overcome this limitation is to perform feature selection on multicenter datasets ideally representing a large variety of scanners and acquisition protocols , whereby the probability of selecting only locally relevant features , hence , the risk of overtting is reduced . 
unfortunately , in most studies , large multicenter datasets are not available . generally , two types of feature selection techniques are used in radiomics studies , unsupervised and supervised feature selection [ 29 ]  . 
unsupervised feature selection methods such as principal component analysis ( pca ) or cluster analysis aim at the identication and removal of redundant features from the feature space , whereby class labels are not considered [ 12 ]  . 
supervised feature selection techniques also take into consideration the relation of the features to the class labels , i.e. , features that contribute most to the diagnostic problem are preferred . 
different unsupervised feature selection methods exist , of which lter methods , wrapper methods , and embedded methods are those most prominent in radiomics . filter methods are also called univariate methods and statistically evaluate the relation between the features without considering their correlations and interactions . 
univariate methods are , for example , the chi - squared score , the students t - test , the wilcoxon rank sum test , or the fisher score [ 30 , 31 ]  . wrapper methods , also called multivariate methods , partly overcome the limitations of univariate methods by taking into consideration correlations and interactions among the radiomics features . 
while univariate methods only investigate the statistical relationship between the radiomics features , wrapper methods create a subset of features , apply this subset to a predictive model , and evaluate the quality of its performance . 
these methods include bidirectional search , exhaustive feature selection , forward feature selection , or backward feature elimination [ 30 , 31 ]  . embedded methods combine the advantages of lter and wrapper methods . 
additionally , since feature selection is performed during the training phase of the machine learning models and does not require an additional predictive model solely for performance evaluation of the different subsets of features , embedded methods are computationally faster than wrapper methods and less prone 852 strahlenther onkol ( 2020 ) 196 : 848855 to overtting . 
examples of embedded feature selection methods are tree - based algorithms such as the random forest classier , the least absolute shrinkage and selection operator ( lasso ) , or ridge regression [ 30 , 31 ]  . now that a subset of relevant features with low redundancy has been identied by feature selection , a mathematical model for the prediction of a known , underlying ground truth can be generated . 
among the machine learning algorithms and classiers most commonly used for radiomics analysis are linear and logistic regression , decision trees , e.g. , random forests , neural networks , support vector machines , or the cox proportional hazards model in case of censored survival data . 
model generation includes the iterative search for a set of optimal parameters that dene the general structure of the model , a process called hyperparameter tuning . in order to identify the best possible machine learning algorithm for the diagnostic problem , the selected model has to be evaluated on a subset of data . 
to avoid the risk of overtting by generating and testing the mathematical model on the same subset of data , the available dataset is ideally subdivided into a training and a validation dataset . 
if the model was trained and evaluated on the same subset of data , a perfect classication of results could be easily achieved by an algorithm that simply repeats the labels of the training data . 
it should be noted , that the distribution of samples of each class remains approximately the same after data splitting , i.e. , if 40% of samples were diagnosed with a recurrent tumor , and 60% were diagnosed with treatment - related tissue changes in the original dataset , this proportion of diagnoses should also remain approximately the same in the training and the validation dataset ( stratied split of data ) , which is particularly important for small datasets . 
the test dataset represents the data the model would face when applied in clinical routine . consequently , every radiomics model should prove its performance , robustness , and reliability on the test dataset , but the test dataset should never be used for tuning of model hyperparameters . the described workow for model generation and evaluation including splitting of the data into three subgroups obviously requires large datasets . 
unfortunately , oncological studies including studies in the eld of radiation oncology usually contain a maximum of several hundred datasets . however , machine learning also offers methods such as bootstrapping or cross - validation to assess model performance even without the availability of a test dataset . 
finally , to assess the overall model performance , the classication accuracy from each iteration is averaged . deep learning - based radiomics deep learning generally describes the process of applying deep neural network architectures for problem solving , which are particular types of machine learning algorithms . originally , articial neural networks that provide the basis for more advanced architectures were inspired by the working principle of the human visual systeby adding layers of hidden neurons beyond the simple input and output layers from articial neural networks , a new level of complexity was added that enabled deep learning . 
deep learning - based radiomics automatically identies and extracts high - dimensional features from the input images at different levels of scaling and abstraction , resulting in models especially useful for pattern recognition or classication of high - dimensional non - linear data [ 32 ]  . 
the usefulness of deep learning - based methods for the automated identication and segmentation of brain metastases and gliomas for radiation therapy planning has been demonstrated in several studies [ 1721 ]  . deep learning - based radiomics uses a workow that is very different from the feature - based radiomics approach described above . 
instead of using mathematically predened features , different architectures of neural networks such as convolutional neural networks ( cnns ) or auto - encoders are used to generate and identify the most important features from the input data . 
in particular , autoencoder networks , which are a special , unsupervised variant of cnns , aim at compression of the image content and mapping onto a relatively short but representative feature vector [ 33 ]  . 
in general , deep learning - based radiomics uses a cascaded system of single - layer neural networks which are trained to learn and identify structures of relevance for the classication problem in the imaging data [ 34 ]  . 
in a nal step , the identied features can be used for classication by the neural network itself , or leave the network and undergo the process of model generation similar to the feature - based radiomics approaches described above using different classiers from conventional machine learning such as decision trees , restrahlenther onkol ( 2020 ) 196 : 848855 gression models , or support vector machines . 
of note , while feature - based radiomics always requires segmented images for feature extraction , deep learning - based radiomics , especially cnns , also function on unsegmented images . since the features are generated and extracted directly from the underlying data and a subset of best performing features is automatically extracted , feature selection is rarely performed . 
in transfer learning , a neural network is used that has already been pre - trained on a different , but closely related task , e.g. , a neural network for brain tumor segmentation that was originally trained on imaging data from patients with brain metastases might also provide useful results for the segmentation of glioma patients [ 35 ]  . 
hereby , both the amount of data necessary to identify a relevant feature subset and the computational demand are reduced . limitations despite the promising results and the potential of radiomics , the repeatability , reproducibility , and transferability of radiomics features is still an issue and often depends on the used imaging modality , sequence , spatial resolution , size of the image , image quality , reconstruction and correction parameters , as well as motion artefacts and other factors . repeatability is commonly assessed by the extraction of radiomics features from repeated acquisitions of images under identical or near - identical acquisition and processing parameters . 
such systematic review articles focusing on the repeatability and reproducibility of radiomic features are still scarce but of major importance for advancing toward a better standardization of the results from radiomics studies . 
the image biomarker standardization initiative ( ibsi ) provides image biomarker nomenclature and denitions , reporting guidelines as well as benchmark datasets and benchmark values , to enable study groups working in the eld of radiomics to verify their image processing and feature extraction [ 22 ]  . in terms of repeatability and reproducibility , deep learning - based radiomics may be advantageous , as the self - learning neural networks show a better capability for generalization and transfer than feature - based approaches . 
although different open - source software packages for feature - based radiomics , ( pyradiomics [ 38 ] , mazda [ 39 ] , and lifex [ 40 ] ) , as well as open - source frameworks for deep learning - based radiomics ( keras [ 41 ] , tensorflow [ 42 ] , pytorch [ 43 ] ) are available , the workow used in most studies is still complex and often not reported in sufcient detail , so that it is almost impossible for other research groups to fully comprehend the presented results , not to mention reproducing them . another limitation to the application of radiomics models in clinical routine is the problem of interpretability of the extracted features and the generated models . 
however , some methods to improve the interpretability of radiomics analyses have been developed , such as graph - based approaches for feature - based radiomics [ 44 ] or visualization tools for deep learning - based radiomics that highlight regions of the segmented tumor according to their importance for the prediction of the generated classier [ 45 ]  . efforts to overcome the mentioned shortcomings are ongoing [ 22 , 46 , 47 ]  . conclusion the number of studies evaluating the potential of featurebased as well as deep learning - based radiomics for application in radiation oncology is increasing . 
especially in combination with established sources of diagnostic information such as clinical , histomolecular , or conventional imaging parameters , radiomics may contribute signicantly towards an improved diagnosis and treatment management in patients with brain tumors and other solid tumors . 
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juni 2020 der / die autor ( en ) 2020 hintergrund und ziel der arbeit die simultane radiochemotherapie ( rct ) gilt als standardtherapie fr patienten mit analkarzinom , ist allerdings auch mit nicht unerheblichen nebenwirkungen assoziiert , die u . 
auerdem sollten faktoren identiziert werden , die mit einer verminderten compliance assoziiert sind . patienten und methoden in der ontario cancer registry wurden zwischen 2007 und 2015 insgesamt 1125 patienten mit analkarzinom identiziert , welche eine standard - rct in kurativer intention erhielten . 
die radiotherapie galt als nichtkomplett , wenn als gesamtdosis nicht zumindest 45 gy erreicht wurden ; als vollstndig durchgefhrte simultane chemotherapie galten zwei gaben von 5 - fluorouracil im mindestabstand von 2 wochen und zumindest eine gabe von mitomycin oder cisplatin . in einer multivariablen analyse wurden das alter , das geschlecht , die komorbiditt , der soziokonomische status , der hiv - status sowie das tumorstadium adjustiert . originalpublikation raphael mj , ko g , booth cm et al ( 2020 ) factors associated with chemoradiation therapy interruption and noncompletion among patients with squamous cell anal carcinoma . 
patienten mit hherem komorbidittsscore ( risk ratio [ rr ] 1 , 54 ; 95 % - ci 1 , 032 , 310 ) und solche im alter von ber 70 jahren wiesen im vergleich zu solchen von < 50 jahren ( rr 0 , 60 ; 95 % - ci 0 , 250 , 70 ) eine signikant niedrigere wahrscheinlichkeit auf , die rct komplett zu erhalten . 
die inkomplette durchfhrung der rct , nicht aber die unterbrechung von > 7 tagen war mit einem signikant hheren risiko fr eine erforderliche abdominoperinealen exstirpation sowie einem schlechteren krankheitsspezischen und gesamtberleben assoziiert . schlussfolgerung der autoren da ein nicht unerheblicher anteil an patienten keine komplette rct erhalten kann , sind initiativen zur verbesserung der qualitt der behandlungsdurchfhrung notwendig . kommentar bei der vorliegenden arbeit handelt es sich um eine retrospektive auswertung eines groen patientenkollektivs mit analkarzinom , basierend auf dem krebsregister von ontario . 
auffllig ist , dass fast ein viertel ( 23 % ) der patienten behandlungsunterbrechungen von mehr als 7 tagen aufwies und dass die schwankungsbreite zwischen den beteiligten kliniken diesbezglich von 9 bis 55 % reichte . 
die sowieso schon relativ niedrige gesamtdosis von 45 gy als kriterium fr die vollstndigkeit der rt erreichten im gesamtkollektiv nur 82 % der patienten , erneut mit schwankungen zwischen 66 und 93 % je nach klinik . dass ltere patienten ( > 70 jahre ) und solche mit mehr komorbiditten eine niedrigere wahrscheinlichkeit hatten , die komplette rct zu erhalten , ist wenig berraschend . interessanterweise besttigt diese arbeit aber erneut , dass eine hiv - erkrankung nicht mit unterbrechungen oder instrahlenther onkol ( 2020 ) 196 : 952953 kompletter rct assoziiert ist und daher die standard - rct bei hiv - patienten mit analkarzinom gem den aktuellen behandlungsleitlinien ohne einschrnkung und ohne dosiskompromisse empfohlen wird [ 1 ]  . 
weitere grnde fr die kompromittierte rct knnen aufgrund der registerdaten leider nicht genannt werden . aus strahlenbiologischen erwgungen ist die unterbrechung einer strahlentherapie wegen des bekannten phnomens der akzelerierten repopulierung [ 3 , 4 ] potenziell nachteilig . 
dies konnte fr die rct des analkarzinoms bei patienten der rtog - 87 - 04und rtog - 98 - 11 - studien gezeigt werden : eine verlngerte gesamtbehandlungszeit war mit einer signikant schlechteren prognose assoziiert [ 5 ]  . unklar ist allerdings , warum in der hier diskutierten arbeit kein einuss von therapieunterbrechungen und einer damit verbundenen verlngerung der behandlungszeit auf die onkologischen endpunkte gezeigt wurde . 
es ist deshalb zu mutmaen , dass das nichterreichen der zieldosen zunchst der therapieunterbrechung geschuldet war , die schlielich nicht in einem wiederaufnehmen der therapie mndete . demnach kann man davon ausgehen , dass die patienten mit unterbrechungen trotz pause ( n ) eher eine ausreichende bestrahlungsdosis und chemotherapiedosis erhalten hatten , was auch als signikanter einussfaktor in der sekundren auswertung der rtog - studie gezeigt wurde . fazit supportive manahmen sind integraler bestandteil der behandlung von krebspatienten [ 6 ]  . 
die hier kommentierte arbeit unterstreicht dies erneut und verlangt ein engmaschiges monitoring , damit die notwendigkeit einer supportiven therapie erkannt und frhzeitig eingeleitet werden kann , beispielsweise fr patienten , die wegen analkarzinom und sicher einer vielzahl weiterer tumorentitten eine rct erhalten . 
fokas geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
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amini a , jones bl , ghosh d et al ( 2017 ) impact of facility volume on outcomes in patients with squamous cell carcinoma of the anal canal : analysis of the national cancer data base . 
ben - josef e , moughan j , ajani ja et al ( 2010 ) impact of overall treatment time on survival and local control in patients with anal cancer : a pooled data analysis of radiation therapy oncology group trials 87 - 04 and 98 - 11 . 
abramowitz1 alan dal pra1 alan pollack1 radka stoyanova1 received : 3 july 2020 / accepted : 7 august 2020 / published online : 21 august 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract radiomics , as it refers to the extraction and analysis of a large number of advanced quantitative radiological features from medical images using high - throughput methods , is perfectly suited as an engine for effectively sifting through the multiple series of prostate images from before , during , and after radiotherapy ( rt )  . 
multiparametric ( mp ) mri , planning ct , and cone beam ct ( cbct ) routinely acquired throughout rt and the radiomics pipeline are developed for extraction of thousands of variables . 
in this review , we summarize the radiomics efforts and discuss several promising concepts such as delta - radiomics and radiogenomics for utilizing image features for assessment of the aggressiveness of prostate cancer and its outcome . 
we also discuss opportunities for quantitative imaging with the advance of instrumentation in mri - guided therapies . keywords radiogenomics delta - radiomics multiparametric mri cone beam ct introduction contemporary radiation treatment ( rt ) of prostate cancer is associated with large - scale image acquisition . 
multiparametric magnetic resonance imaging ( mpmri ) , computed tomography ( ct ) , and cone beam ct ( cbct ) are acquired at multiple steps of the course of rt , starting with patient diagnosis and then for treatment planning , delivery , and follow - up . 
radiomics , as it refers to the extraction and analysis of advanced quantitative information , converts imaging data into a high - dimensional mineable feature space using a large number of automatically extracted data - characterization algorithms [ 1 ]  . the main hypothesis behind the radiomics effort is that the imaging features capture distinct phenotypic differences of ( cid : 2 ) radka stoyanova rstoyanova@med.miami.edu 1 department of radiation oncology , university of miami miller school of medicine , 1121 nw 14th st , miami , fl 33136 , usa the tumors and may have diagnostic , prognostic , and predictive power [ 2 ]  . 
among the chief questions in the treatment of prostate cancer are the choice of rt fractionation schedule ( hypoor conventional fractionation ) and the use , timing , and duration of androgen deprivation therapy ( adt )  . depending on the risk category , a considerable number of patients treated with rt present biochemical failure , suggesting that additional strategies are needed for dening and treating patients based on improved risk stratication . mpmri has emerged as a major tool for prostate cancer detection and risk stratication [ 3 , 4 ]  . 
an mpmri examination is incorporated at all stages of disease management , including screening , improving diagnostic accuracy , risk stratication , guiding treatment , and post - treatment evaluation . 
to standardize the evaluation and reporting of mpmri , the european society of urogenital radiology ( esur ) published guidelines based on expert consensus in 2012 , termed pi - rads [ 6 ]  . 
this reporting system utilizes a 15 score for each mpmri sequence ( t2 - weighted [ t2w ] mri , dynamic contrast - enhanced [ dce - mri ] , and diffusion - weighted imaging [ dwi ] ) and provides an overprostate cancer radiomics fig . 
the two zones of the prostate have different intensities : the t2 signal is bright on the peripheral zone ( yellow contour ) due to the fact that the peripheral zone contains mainly prostatic acini and ducts and the prostatic uid in their lumina causes a strong signal . 
dce - mri highlights the tumor vasculature and areas of the tumor are of higher intensity all score for each region of interest ( roi ) , with higher scores relating to a higher risk of aggressive cancer . 
for the relatively short time of its existence , the system has undergone several modicationspi - rads ( v2 ) [ 7 ] and pirads ( v2.1 ) [ 8 ] and admittedly , there is still signicant inter - reader variability related to readers experience [ 9 ]  . 
pirads was not designed for 3d tumor volume delineation and with respect to rt , pi - rads has limited application in dening volumes ( gross tumor volumes [ gtvs ] ) for radiotherapy boost . 
finally , the ve - point system does not tap into the wealth of quantitative imaging information contained in the multiple sequences of mpmri , nor does it elucidate interand intra - lesional spatial heterogeneity of prostate cancer . 
in contrast , the radiomics approach extracts large amounts of advanced quantitative mpmri features in a format that is amicable for building descriptive and predictive models relating image features to gene / protein signatures or radiotherapy outcomes [ 10 ]  . the most widely used imaging modality in radiation oncology is ct , which assesses tissue density . 
cbct images are commonly used to check patient alignment prior to receiving the treatment dose and important quantitative imaging information can be extracted from them [ 1315 ]  . in this review , we discuss the impact of radiomics efforts in rt of prostate cancer . 
first , the two main imaging modalities for prostate imaging , mri and ct , are described . then , the individual elements of the radiomics pipeline as tailored for rt are reviewed . 
finally , we review promising applications of radiogenomics , delta - radiomics , and the opportunities for serial image analysis from mri - guided radiotherapy ( mrigrt ) for prognostic assessment and treatment management . imaging modalities for prostate cancer rt multiparametric mri of the prostate with its superior soft tissue contrast compared to x - raybased imaging methods , mpmri has become routinely used in the radiation oncology clinical workow for pre - treatment planning and follow - up assessment [ 16 ]  . 
mpmri combines functional ( perfusion via dce - mri and diffusion via dwi ) [ 1820 ] and anatomical information ( t2w - mri ) [ 21 ] that enhances diagnostic reliability . 
image acquisition : imaging modalities , multiparametric mri ( mpmri ) , computed tomography ( ct ) , and cone bean ct ( cbct ) from the same prostate cancer patient are shown . 
the red arrow points at the tumor . segmentation : prostate , urethra , peripheral zone ( pz ) , and transition zone ( tz ) , as shown in the top panel , are contoured . 
data integration : radiomics features are integrated with other available biomarkers , such as data from clinical records , genomic proling , proteomic screening , and physiological analysis . application in rt : integrated data / models are used to aid in diagnostic assessment , to facilitate patient - individualized treatment strategizing , and improve predictive and prognostic accuracy microstructure in relative benign prostatic tissue to differentiate malignant lesions . the correlation of radical prostatectomy histopathology with mpmri sequences is illustrated in fig . 
there is no other imaging modality that has demonstrated the same sensitivity and specicity for distinguishing intraprostatic cancer of higher grade ( gleason score [ gs ] 7 or above ) [ 4 , 22 ]  . there is a burgeoning literature on the use of external beam radiotherapy to treat the dominant intraprostatic lesion ( dil ) with mpmri - directed rt [ 2325 ] , including favorable preliminary toxicity results from flame , a randomized clinical trial [ 26 ]  . 
therefore , targeting dominant nodules can still miss the most aggressive disease , causing misinformed treatment decisions [ 29 ]  . tumor heterogeneity can be elucidated by mapping subregions of the lesion with differential imaging characteristics , called habitats [ 3032 ]  . 
simply detecting tumors may not be enough ; the full degree of tissue heterogeneity must also be understood . we proposed the prostate tumor habitat risk scoring ( hrs ) system , which scores the voxels in the prostate by level of aggressiveness [ 33 ]  . 
second , a quantitative adc score is also assigned to each pixel , based on identied optimal apparent diffusion coefcient ( adc ) thresholds for automatic delineation and risk assignment of prostatic lesions [ 36 ]  . 
mri units are not directly related to electron density and although attempts have been made to generate dose calculations from mri by generating synthetic ct images [ 3740 ] , ct continues to be the standard modality for rt dose calculation . 
recently , the modality has been used to extract radiomic features in prostate cancer . radiomics pipeline of prostate cancer rt the steps in the radiomics pipeline for rt of prostate cancer are shown in fig . 
for mpmri , the t2w , dwi at high b - value ( 1000 s / mm2 ) , adc , and the early - enhancing image in the dce - mri are shown . the segmentation of volumes of interest ( voi ) is a key process because it species the region from which radiomic data will be extracted . 
the area of the tumor is clearly depicted and further delignated by the contour of hrs6 . the volume , dened by pixels with hrs = 6 , was in good agreement with radical prostatectomy lesion volumes [ 33 ] and we chose hrs6 to serve both as voi for extraction of radiomics variables as well as for automatic segmentation of volumes for gtv for rt dose boost . 
briey , morphological features describe the form and structure of the voi , which can range from geometrical descriptions that are simple , such as volume , to metrics that are complicated , such as fractal dimensions [ 4547 ]  . 
semantic features are quantitative descriptors derived empirically by the radiologist when assessing mpmri for improved detection , location , and risk stratication in patients with prostate cancer , such as those dened in pirads [ 7 ]  . 
first - order statistical features are related to the intensity histogram of the voi , whereas higher - order statistical features are rst encoded into different matrix types describing how collections of grey levels within the voi relate to one another [ 4851 ]  . 
transform - based features are features extracted following a kernel transformation of the voi , which includes but is not limited to the fourier transform , gabor transform , wavelet transform , and laplacian transforms of gaussian bandpass lters [ 5254 ]  . 
many applications in rt of prostate may be possible , including aiding and improving diagnostic establishment , patient - individualized treatment , predictive accuracy , and prognostic accuracy . overview of radiomics efforts for prostate cancer the radiomics publications in prostate cancer are summarized in table 1 ; this summary is updated from our 2016 and 2018 radiomics reviews [ 31 , 42 ]  . 
at the time of writing of this review , we are only partially through the year and the number of publications is already nearly equal to the previous year . a variety of radiomics features are considered in assessing prostate cancer aggressiveness . 
often studies are not limited to a single category of radiomics features . statistical features were used alone in 45% of these publications , with 91% of them considering statistical radiomics features in some forconsequently , statistical radiomics features are by far the most commonly used category . the majority ( 86% ) of radiomics approaches used gs as an analysis endpoint . 
 [ 11 ] used gs in combination 904 strahlenther onkol ( 2020 ) 196 : 900912 table 1 summary of radiomic manuscripts in prostate cancer , grouped by modality reference modality feature category analysis endpoints performance tumor segmentation wibmer et al . 
in addition , the benet of dce - mri for prostate cancer characterization is still a matter of debate ( in the current pi - radsv2.1 [ 8 ] , the dce sequence is used in only determination )  . even though ct images are highly repeatable , only two ct - based radiomics studies of prostate cancer to date were statistical , transform - based statistical morphological , statistical morphological morphological , statistical , transform - based morphological , statistical , transform - based statistical statistical , transform - based morphological , statistical statistical statistical , transform - based statistical statistical morphological statistical , transform - based statistical morphological , statistical , transform - based statistical , transform - based prostate cancer radiomics fig . 
3 summary of publications to date that assessed tumor aggressiveness of prostate cancer using radiomics by a the number of publications per year and b the percentage of publications per modality . 
these exploratory studies indicate possible areas of future research and prognostic potential using ct - based radiomics of prostate cancer . the performance of the models is summarized in the last column of table 1 . 
4 a pie chart showing the proportion of publications to date according to the radiomic feature categories used to assess tumor aggressiveness of prostate cancer using radiomics below we summarize novel concepts and efforts in the eld with emphasis on their utilization in rt of prostate cancer . found [ 11 , 12 ]  . 
the authors clarify that the modest performance of the validation datasets may be due to a small number of patients and class imbalances in the validation datasets [ 11 ]  . 
 [ 12 ] evaluated radiomics features of ct perfusion and found classiers that distinguished well between gs = 7 vs . gs > 7 ( auc = 0.81 ) and moderately between gs = 3 + 4 vs . 
six image fusions are carried out : indicated in the gure ( 1 ) using prostate anatomical matching , the diagnostic mri is fused with the planning mri ; ( 2 ) the planning mri is fused to the planning ct , using ducial matching ; ( 3 ) using ( 1 ) and ( 2 ) , the diagnostic mri is fused to the planning mri for target volume contouring ; ( 46 ) the post - rt mris ( at 3 and 9 months ) and the one before the endpoint biopsy ( 2.02.5 years after completion of all therapy ) are fused with both the pre - rt planning and diagnostic mri quantitative radiomics features . 
prior to the treatment planning ct simulation , radio - opaque ducial markers are placed in the prostate to enable on - board cbctbased set up for subsequent radiation treatment . 
a planning mri , acquired at the same time as the ct simulation , facilitates fusion #3 of the diagnostic mpmri to the planning ct via fusion #1 of the diagnostic and planning mris and ducial - based fusion #2 of the planning mri and ct . 
the post - treatment mris at 3 and 9 months and the nal mri at 22.5 years are fused ( #46 ) to the pre - treatment mris . radiomic features are thus readily extracted from regions of interest on mris over multiple timepoints before and after radiotherapy . 
6 are the extracted values of adc and ve ( relative volume of the extravascular extracellular space ) for the gtv , natz and napz , and preand post - rt . 
since intracellular water diffusion is more restricted inside the cell than in the interstitial space , a loss in cellularity results in an increase in adc , and of course the increase in interstitial space results in increased ve . 
the pathophysiologic mechanism underlying this and other apparent trends in the data will be the subject of future work . cone beam ct radiomics features from cbct images may provide an opportunity to efciently capture early tumor response to therapy and allow for adaptive treatment decisions , although there are image quality challenges . 
however , cbct image quality in comparison to diagnostic ct has known limitations in the form of more beam hardening , motion , scatter , and other artifacts [ 6366 ]  . 
in a pilot study , we studied the repeatability of cbct - based radiomic features of 20 cbct testretest image pairs and the reproducibility of radiomic features between the planning ct and the rst - fraction cbct for 20 patients . 
for other cancer sites , like nonsmall cell lung cancer , well - performing prognostics models using cbct - based radiomics have been documented [ 14 , 15 ]  . 
considering the previous studies of cbct radiomic quality and the potential shown in cancer sites , cbct radiomics may yet be viable for prediction of treatment outcome . mri - guided radiotherapy the integration of the mri scanner with the linear accelerator radiation delivery machine has launched a new era of radiotherapy [ 69 ]  . 
on - board mri - guided radiotherapy ( mrigrt ) not only provides increased setup accuracy but also affords improved motion management as well as the capacity for on - table adaptive re - planning based on the anatomy of the day . 
precise localization of the tumor and nearby organs at risk in real time has allowed for safe tumor dose escalation on hybrid mri / rt machines [ 70 ]  . 
5 , radiomics features are extracted from gross tumor volume ( gtv ) and normal - appearing transition and peripheral zones ( natz and napz ) at 3 months and 9 months after rt and 22.5 years after end of all therapy . 
boxplots of apparent diffusion coefcient ( adc ; a ) and percent of extravascular extracellular space ( ve ; b ) prognostic assessment of cancer patients via mri setup images that are acquired daily on these machines . 
prior to the advent of hybrid mri / rt treatment platforms , mr images were typically acquired only preand post - treatment clinically , and perhaps once or twice during treatment in the clinical research setting . 
daily mr images from mrigrt now provide a wealth of image data during the entire course of treatment with vastly improved temporal resolution , offering a potentially valuable new assessment tool via delta - radiomics . 
recent studies conducted on low - eld ( 0.35 t ) hybrid mri / rt machines have shown the promise of mri - derived radiomic biomarkers to predict response in rectal [ 71 ] and pancreatic cancer [ 72 ]  . 
future studies will determine whether radiomics analysis of daily images from mrigrt can similarly add prognostic value to prostate cancer treatment . radiogenomics tumor - underlying molecular and genomic characteristics can provide patient - tailored treatment stratication and prediction of therapy response that goes beyond the gleason scores prediction of aggressiveness . 
in the rst radiogenomics study , we demonstrated signicant correlation of mpmri radiomics with prostate cancer risk - gene expression proles in mpmri - guided biopsy tissues [ 32 ]  . 
another group using a proliferation gene signature found similar results [ 73 ] , supporting a role for the radiomics features associated with gene expression patterns in quantitative imaging algorithms . the presence of hypoxia in the tumor microenvironment , associated with a more aggressive tumor phenotype [ 74 , 75 ] , often underlies the resistance to rt in compar908 strahlenther onkol ( 2020 ) 196 : 900912 fig . 
the two main clusters of genes were driven by the biopsy cores ( n = 3 ) from two patients with high risk ( marked with red boxes , patient a and patient b ) hypoxic genes , such as hif3a , epas1 , cul2 , ep300 , are upregulated in the tissue from patient a and , vice versa , downregulated in the tissue from patient b . 
c dce curves in the tumors , referenced to dce signal in muscle ( gluteus maximus )  . the tumor dce - curves in patient a are characterized by slower contrast uptake and moderate enhancement , characteristic for hypoxic tumors . 
thus , in vivo knowledge of the spatial distribution of hypoxia in tumors may provide prognostic information and can possibly improve treatment planning ( e.g. , intensity - modulated radiotherapy ) [ 78 ]  . 
dce - mri can characterize the microenvironment in solid tumors by determining areas of inadequate or heterogeneous perfusion with hyperpermeable vasculature which are related to the degree of hypoxia [ 79 ]  . 
analysis of the dce - mri curves conrmed that the patients had dramatically different contrast uptake patterns , suggesting the potential of dce radiomics to predict for hypoxia . gene expression signatures , such as decipher ( decipherdx , san diego , ca , usa ) [ 8184 ] , prolaris cell cycle progression ( ccp ; myriad genetics , salt lake city , ut , usa ) [ 8590 ] , and genomic prostate score ( gps ; genomic health , redwood city , ca , usa ) [ 9093 ] add to clinical - pathologic risk factors and have the potential to become integral to risk stratication and management . 
developing tools and pipelines for optimal extraction of radiomics features holds the promise for improved prognostic and predictive assessment for prostate cancer [ 96 ]  . rt of prostate cancer also poses specic questions that are not readily answered with the existing imaging and radiomics workows . 
while there is a gradation of treatment intensication options that are effective , optimized criteria are lacking for recommendations concerning rt dose , rt fractionation , the use , timing , and duration of adt , and the use of additional systemic agents ( e.g. , abiraterone , chemotherapy )  . these questions frame the role of imaging in the identication of early markers of patient outcome . 
prostate cancer has an exceptionally long natural history and the lack of mature datasets with available outcome endpoints poses a particular challenge for these studies . one area of prostate cancer radiomics research that holds particular promise is delta - radiomics . 
with the advent of mrigrt , we now have access to daily mri patient setup images for patients treated on mrigrt machines in addition to daily cbct images for patients treated on conventional linear accelerators . 
there is tremendous potential in mining this wealth of imaging data to discover trends in radiomics features during treatment that could be exploited for predicting treatment response or normal tissue toxicity . correlating these trends with patient outcome could lead to predictive models that the radiation oncologist would use to guide possible changes in treatment early on , thus realizing the vision of personalized care tailored to the individual patient . 
however , this approach is not without challenges . development of reliable predictive models using machine learning typically requires an order of hundreds of patients to use as input for building the model , in addition to a similar number of patients in an independent dataset for model validation . 
use of retrospective image data can be problematic , as it is well known that radiomic features can be sensitive to image acquisition parameters and reconstruction algorithms , which vary over institutions and even from patient to patient within a given clinic . 
efforts are underway to determine which mriand cbct - based radiomic features are repeatable ( i.e. , robust to test / retest on a given machine ) and reproducible ( i.e. , constant across machine platforms )  . 
while repeatability and reproducibility of radiomic features are necessary and desirable , the ultimate test is the ability of radiomic features used in a model to reliably predict patient outcome . in conclusion , this review paper has summarized ongoing radiomics efforts for analysis of imaging studies acquired from prostate cancer imaging prior , during , and after radiation treatment . 
juni 2020 der / die autor ( en ) 2020 hintergrund und ziel der arbeit nachdem fr selektive strogenrezeptormodulatoren ( serm ) , wie tamoxifen , bereits eine signikante langzeitwirkung in der brustkrebsprvention bei frauen mit einem hohen risiko fr brustkrebserkrankungen nachgewiesen werden konnte [ 1 ] , wurde in der ibis - ii - studie die prventive wirkung des aromataseinhibitors ( ai ) anastrozol bei postmenopausalen risikopatientinnen untersucht . 
die aktuelle publikation ist ein update der studie mit lngerem follow - up . patientinnen und methoden bei der ibis - ii - studie handelt es sich um eine internationale , randomisierte , doppelt verblindete und placebokontrollierte interventionsstudie . 
weniger originalpublikation cuzick j , sestak i , forbes jf , dowsett m , cawthorn s , mansel re et al ( 2020 ) use of anastrozole for breast cancer prevention ( ibis - ii )  . 
21 , 24105 kiel , deutschland ernste nebenwirkungen wurden nicht weiter bercksichtigt . zur analyse der endpunkte wurden hazard ratios basierend auf dem cox - regressionsmodell mit korrespondierenden 95 % - kondenzintervallen sowie eine berlebenszeitanalyse nach kaplan und meier durchgefhrt . ergebnisse nach einem medianen follow - up von 131 monaten konnte eine reduktion des auftretens von brustkrebs um 49 % ( hr 0 , 51 , 95 % - ki 0 , 390 , 66 , p < 0 , 0001 ) nachgewiesen werden . 
in der anastrozolgruppe nur 2 patientinnen an brustkrebs verstarben , konnte bezglich einer letalittssenkung durch den ai kein signikanter unterschied nachgewiesen werden . schlussfolgerung der autoren der in der ersten publikation der studie festgestellte rckgang an brustkrebserkrankungen durch anastrozol hlt auch nach mehr als 5 jahren an . die prventive anastrozoleinnahme senkt also auch langfristig bei frauen mit einem hohen brustkrebsrisiko dieses risiko nachhaltig , wobei die nebenwirkungen geringer als diejenigen von tamoxifen sind . kommentar brustkrebs ist die weltweit hugste krebserkrankung bei frauen mit mehr als 2 mio . 
whrend die medikamentse prvention bei hochrisikopatientinnen in den usa und in grobristrahlenther onkol ( 2020 ) 196 : 954955 tannien bereits einzug in ofzielle therapieempfehlungen gefunden hat [ 4 , 5 ] , spielt sie in deutschland bislang noch keine rolle . 
in einer studie mit dem ai exemestan wurden ber einen zeitraum von 5 jahren hnliche ergebnisse wie hier mit anastrozol erreicht [ 7 ]  . die langzeitwirkung des carry - over - effekts einer prventiven brustkrebstherapie wurde bislang lediglich fr den selektiven strogenrezeptormodulator tamoxifen untersucht [ 1 ]  . 
die jetzt in der ibis - ii - studie durch anastrozol bewirkte reduktion des auftretens um 49 % bertrifft somit die ergebnisse mit tamoxifen deutlich . die nnt von anastrozol in den ersten 12 jahren nach therapieabschluss schtzen die autoren auf 29 , whrend die von tamoxifen bei 58 lag . whrend im rahmen der tamoxifenprophylaxe eine erhhte zahl an karzinomen des endometriums und auch thromboembolischen ereignissen registriert wurde [ 1 ] , konnten bei der behandlung mit anastrozol keine ernsten unerwnschten reaktionen beobachtet werden . 
dennoch darf man die whrend der therapie signikant erhhten risiken an muskuloskeletalen und vasomotorischen beschwerden sowie an denen des trockenen auges und des arteriellen hypertonus [ 2 ] bei der abwgung des nutzenrisiko - verhltnisses nicht auer acht lassen . die potenzielle toxizitt wiegt besonders schwer , da weiterhin keine daten zur mortalittssenkung durch den aromataseinhibitor vorliegen . 
schenke geben an , dass kein open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
cuzick j , sestak i , forbes jf et al ( 2014 ) anastrozole for prevention of breast cancer in high - risk postmenopausal women ( ibis - ii )  . 
cuzick j , sestak i , baum m et al ( 2010 ) effect of anastrozole and tamoxifen as adjuvant treatment for early - stage breast cancer . 10 - year analysis of the atac trial . 
juli 2020 der / die autor ( en ) 2020 hintergrund und fragestellung die wahl der optimalen behandlung des lokal begrenzten prostatakarzinoms ( pca ) wird von verschiedenen faktoren bestimmt : tumoreigenschaften , zu erwartende rezidive , lebenserwartung , komorbiditten , unerwnschte nebenwirkungen sowie wunsch des patienten . 
die aussagen bisheriger studien , die die auswirkungen verschiedener therapieoptionen bezglich funktioneller einschrnkungen und der lebensqualitt verglichen haben , kranken an einigen einschrnkungen : vor allem verglichen sie berwiegend ltere behandlungsverfahren , nicht aber aktuell bliche therapieformen wie roboterassistierte prostatektomie , intensittsmodulierte strahlentherapie und die verschiedenen fraktionierungsrhythmen der strahlentherapie . 
deshalb wurde die comparative effectiveness analysis of surgery and radiation studie ( ceasar ) durchgefhrt , um ber die auswirkungen der aktuellen behandlungsformen des pca auf die lebensqualitt zu informieren in der hoffnung , daraus neue behandlungsempfehlungen entwickeln zu knnen [ 4 ]  . patienten und methode die hier zu kommentierende multizentrische und bevlkerungsbezogene kohortenstudie enthlt die daten von > 2000 mnnern , die zwischen 2011 und 2012 mit einem lokal begrenzten pca aus fnf surveiloriginalpublikation hoffman ke , penson df , zhao z et al ( 2020 ) patient - reported outcomes through 5 years for active surveillance , surgery , brachytherapy , or external beam radiation with or without androgen deprivation therapy for localized prostate cancer . 
21 , 24105 kiel , deutschland lance - epidemiology - and - end - results - program - registern ( seer ) und aus der us prostate cancer registry ausgewhlt wurden . die studie unterteilte die patienten nach ihrem risikoprol in zwei kohorten : teilnehmer mit gnstigem risikoprol ( n = 1386 ; stadium ct1 - 2bn0m0 , psa 20 ng / ml und who - grad 12 ) erhielten eine nervenerhaltende prostatektomie ( n = 675 ; 49 % ) , anschlieend eine active surveillance ( n = 363 , 26 % ) oder eine alleinige perkutane strahlentherapie ( ebrt ) ohne androgendeprivation ( adt ; n = 261 ; 19 % ) oder eine low - dose - rate ( ldr ) - brachytherapie ( n = 87 ; 6 % )  . 
teilnehmer mit ungnstigem risikoprol ( n = 619 ; stadium ct2cn0m0 oder psa 2050 ng / ml oder who - grad 35 ) erhielten eine intensivere therapie , entweder eine prostatektomie ( ohne nervenschonung , n = 402 ; 65 % ) oder eine ebrt in kombination mit adt ( n = 217 ; 35 % )  . die umfragen zur lebensqualitt erfolgten jeweils zu beginn der studienteilnahme , dann nach sechs monaten , einem jahr , drei jahren und fnf jahren . 
beide bewertungssysteme sind von 0 bis 100 skaliert mit der besten funktion bei beiden scores von 100 [ 4 ]  . ergebnisse die daten von insgesamt 2005 mnnern erfllten die einschlusskriterien und nahmen an mindestens zwei umfragen teil . 
die nur beobachteten oder nur mit ebrt behandelten mnner mit gnstigem risikoprol waren lter und zeigten bei der studienaufnahme mehr komorbidit960 strahlenther onkol ( 2020 ) 196 : 959962 ten als diejenigen , die eine prostatektomie erhalten hatten . die behandlungsergebnisse wurden an die startvoraussetzungen sowie die kovariablen adjustiert . funktionelle unterschiede der verschiedenen behandlungsformen zeigten sich insbesondere bei der sexualfunktion sowie den nebenwirkungen an den harnwegen . 
diese waren nach prostatektomie im vergleich mit der active surveillance schlechter ( adjustierte mittlere abweichung minus 15 , 2 ; p < 0 , 01 in jahr 3 ) , ebenso die nach ldr - brachytherapie ( minus 10 , 1 , p < 0 , 01 in jahr 1 )  . 
ebenso fand man bei den prostatektomierten im vergleich mit den bestrahlten ein klinisch relevant schlechteres outcome bei der sexualfunktion ( minus 10 , 4 [ 95 % - ki 14 , 4 bis 6 , 4 ] ; p < 0 , 01 in jahr 3 ; [ 4 ] )  . 
50 % der mnner , die beim einschluss in die studie beim geschlechtsverkehr noch eine ausreichende erektion erlebten , erhielten diese funktion oder erlangten sie wieder . dabei gab es keine signikanten unterschiede zwischen den verschiedenen gruppen mit denitiver therapie . die studie ergab auch relevante inkontinenzprobleme nach der prostatektomie ber fnf jahre hinweg im vergleich zu den anderen behandlungsoptionen . 
auch bezglich der allgemeinen lebensqualitt bestanden keine signikanten unterschiede , weder in der gruppe mit gnstigen noch in der mit ungnstigen risikoprolen . schlussfolgerung der autoren die externe strahlentherapie ( ebrt ) weist gegenber der prostatektomie klinisch relevante vorteile auf bei beiden risikogruppen bezglich harninkontinenz und erhlt zustzlich die sexualfunktion in der gruppe mit ungnstigem risikoprol weitgehend . die festgestellten unterschiede in den ergebnissen gegenber den vorangegangenen hnlich gestalteten studien z . 
in der protect - studie fhren die autoren auf ihre strkere einbeziehung von diversen kovariablen und die nutzung der neuesten bestrahlungsund operationstechniken zurck . kommentar in den bereits erwhnten vorluferstudien bestand bereits konsens , dass patienten , die einer prostatektomie unterzogen wurden , postoperativ grere probleme mit einer harninkontinenz haben als solche nach anderen behandlungsoptionen inkl . 
das machte neue und spezizierte erkenntnisse zu den nebenwirkungen der aktuellen behandlungsoptionen mglich . wegen der zunehmenden bedeutung des shared decision - making ist es wichtig , den rzten und patienten mglichst genaue informationen zu den wirkungen und nebenwirkungen bei aktuellen behandlungsmglichkeiten zu geben , um damit die therapieentscheidung zu erleichtern . 
damit werden die unterschiedlichen nebenwirkungen und deren auswirkungen auf die lebensqualitt zum oft ausschlaggebenden faktor . eine der grten strken der ceasar - studie ist im gegensatz zu den lteren studien , dass nur die auswirkungen aktuell empfohlener behandlungsmethoden ( imrt und roboterassistierte prostatektomie ) untersucht wurden , da der technische fortschritt durchaus bessere therapieergebnisse erwarten lsst . 
dazu , dass in der ceasarstudie bei keiner behandlungsoption eine klinisch - relevante beeintrchtigung der lebensqualitt beobachtet wurde . ebenso wichtig war , dass die autoren die patienten mit einem lokal begrenzten pca in zwei risikogruppen unterteilten . 
es spricht alles dafr , den einsatz der strahlentherapie beim lokal begrenzten pca strker als die prostatektomie zu empfehlen : nach der ceasar - studie spielen ja bei der strahlentherapie denkbare nebenwirkungen wie harnwegsund darmirritationen keine groe rolle mehr . 
die patienten sollten sich , eine rckhaltlose aufklrung der urologischen kollegen vorausgesetzt , beim shared decision - making strker fr die perkutane strahlentherapie entscheiden . strahlenther onkol ( 2020 ) 196 : 959962 zustzlich liefern hoffmann et al . 
mit ihrer arbeit erste aussagen zu den nebenwirkungen der ebrt verglichen mit der prostatektomie bei hochrisikopatienten mit pca , zu denen es laut der aktuellen s3 - leitlinie von 2019 noch keine randomisierten studien gab [ 7 ]  . 
erwhnenswert dabei ist sicherlich auch der bessere erhalt der sexualfunktion sowie der harnkontinenz nach ebrt , was sicher zustzlichen einuss auf die therapiewahl der zuknftigen patienten haben wird . zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf fazit literatur die wohlgewhlte einteilung des lokal begrenzten prostatakarzinoms in zwei risikogruppen erlaubt den patienten eine spezischere darstellung der nebenwirkungen von ebrt vs . 
dunst geben an , dass kein inteopen access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link 1 . 
chen rc , basak r , meyer am et al ( 2017 ) association between choice of radical prostatectomy , external beam radiotherapy , brachytherapy , or active surveillance and patient - reported quality of life among men with localized prostate cancer . 
punnen s , cowan je , chan jm et al ( 2015 ) long - term health - related quality of life after primary treatment for localized prostate cancer : results from the capsure registry . 
hoffman ke , penson df , zhao z et al ( 2020 ) patient - reported outcomes through 5 years for active surveillance , surgery , brachytherapy , or external beam radiation with or without androgen deprivation therapy for localized prostate cancer . 
through years of training , physicians thus learn to interpret clinical signs , laboratory values , and medical images in order to come to a probable diagnosis , to plan a useful treatment , and to estimate the outcome . technical developments in recent years support the view that many of these steps can be performed by computer programs that are based on models which have been trained on digitalized medical data . 
the largest amount of data is generated by medical imaging and it thus comes without surprise that the automated detection and classication of radiological ndings is one of the fastest growing elds in this research area . 
however , due the enormous importance of medical imaging for radiotherapy planning , radiation delivery , and outcome assessment , radiation oncology is especially suited for the application of these automated methods . in radiation oncology , the rst step is usually to identify the tumorous tissue to be irradiated , a procedure which is called image segmentation . 
in computerized image analysis methods , segmentation is based on the detection of a high - dimensional set of imaging features ( sometimes also called texture ) which are present in the tumor but absent in the normal tissue . 
once the typical features have been identied , radiomics can be used to detect tumor areas suitable for dose escalation , to correlate molecular markers with imaging features , to predict response and oncological outcome , and to differentiate treatment - related tissue changes from tumor recurrences . a multitude of computerized mathematical and statistical methods stemming from the modern era of computational bioinformatics and machine learning exist that make these analyses possible . 
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juni 2020 der / die autor ( en ) 2020 hintergrund vergleiche der dosisverteilungen bei der radiotherapie ( rt ) von linksund rechtsseitigen mammakarzinomen knnen die effekte einer hheren im vergleich zu einer niedrigeren kardialen dosis aufzeigen . patienten und methodik die kardiale letalitt wurde anhand individueller patientendaten von 1.934.248 frauen mit brustkrebs in 22 lndern analysiert . 
die analysen wurden stratiziert nach zeit seit der ed , alter bei der ed , kalenderjahr der ed und nationalitt . ergebnisse bei allen drei behandlungsmodalitten zeigten sich effekte bei der patientenauswahl . 
bei patienten , die vor 1990 bestrahlt wurden , war die kardiale letalitt nach rt eines linksseitigen mammakarzinoms hher als nach rt eines rechtsseitigen ( rr 1 , 13 , 95 % - kondenzintervall 1 , 091 , 17 )  . 
whrend bei frauen , die eine chemotherapie erhielten , die rr links versus rechts originalpublikation henson ke , mcgale p , darby sc et al ( 2020 ) cardiac mortality after radiotherapy , chemotherapy and endocrine therapy for breast cancer : cohort study of 2 million women from 57 cancer registries in 22 countries . 
18 , 07745 jena , deutschland 1 , 42 betrug ( 95 % - kondenzintervall 1 , 131 , 77 ) , war die rr bei frauen ohne chemotherapie 1 , 10 ( 1 , 051 , 16 ; 2pdifferenz = 0 , 03 )  . schlussfolgerungen der autoren der relative anstieg der kardialen letalitt durch kardiale strahlenexposition ist bei jngeren frauen grer bis ins dritte jahrzehnt nach der exposition hinein und ist grer , wenn zustzlich eine chemotherapie verabreicht wurde . kommentar die postoperative radiotherapie ( rt ) nach brusterhaltender operation senkt das lokale rezidivrisiko und verbessert das gesamtberleben [ 1 ]  . ein risikoorgan , bei dem sich immer wieder die frage der spttoxizitt der systemund der radiotherapie stellt , ist das herz . 
es zeigte sich eine erhhte sterblichkeitsrate ( rr = 1 , 27 ) durch ischmische herzerkrankungen bei frauen , die eine strahlentherapie erhalten hatten , im vergleich zu denen , die nur operiert worden waren [ 2 ]  . 
das scheint sich in der 2011 verffentlichten aktualisierung der ebctcg - daten ( 10 - jahres - rezidiv und 15 - jahres - sterblichkeit an brustkrebs ) nicht mehr zu besttigen [ 1 ]  . 
verglichen wurden patientinnen die sich einer strahlentherapie unterzogen hatten , mit patientinnen , die nur eine operation erhielten ( rr = 1 , 09 ; 95 % - ki 0 , 971 , 22 ; p = 0 , 14 )  . 
die meisten patientinnen wurden in den 1990erund frhen 2000er - jahren mit einer 2 - d - strahlentherapie behandelt [ 5 ]  . seitdem sind sich die onkologen zunehmend der kardialen risiken einer therapie bewusst geworden , sodass den frauen , die bereits an einer herzerkrankung litten , mglicherweise weniger hug eine strahlentherapie zugemutet und empfohlen wurde . die aktuelle , hier kommentierte studie weist diesen trend auch eindeutig nach . 
das knnte darauf hindeuten , dass entweder patientinnen mit 60 + huger begleiterkrankungen hatten , die ein hochrisiko fr komplikationen am herzen darstellten , oder sie fter als eine gruppe mit niedrigem rezidivrisiko betrachtet wurden . diese vermutung besttigt sich , wenn man bestrahlte mit nichtbestrahlten frauen vergleicht : in der brusterhaltgruppe ( bestrahlt versus nichtbestrahlt ) wurde ein relatives risiko fr die kardiale letalitt von 0 , 70 nachgewiesen . 
in dieser gruppe ist davon auszugehen , dass die tnm - stadien hher waren , die notwendige therapie deshalb aggressiver und kaum / oder nur bei wenigen patientinnen auf die rt verzichtet wurde . eine weitere frage bleibt offen , ob nmlich das herz der jungen patientin oder das der lteren durch eine strahlentherapie gefhrdeter ist . 
eine niedrigere um etwa 50 % bei frauen , die im alter von < 40 jahren bestrahlt wurden , um 20 % bei frauen im alter von 40 bis 59 jahren und um 10 % bei frauen , die im alter von 60 + jahren bestrahlt wurden . nach 1990 konnte dieser trend nur noch bei jngeren patientinnen beobachtet werden , was mglicherweise auf die verteilung innerhalb der gruppe , vor allem aber wohl auf die verbesserung der rt - techniken zurckzufhren ist . sechs frhere studien hatten auch die kardialen risiken durch strahlentherapie bei brustkrebs in abhngigkeit vom alter untersucht . 
47 % pro gy bei erwachsenen ( im alter von 40 bis 59 jahren ) wahrscheinlich zutreffend sind . jedoch ist wahrscheinlich das risiko pro gy fr frauen , die im alter von 60 + jahren bestrahlt werden , etwa um den faktor zwei kleiner und das risiko pro gy fr frauen unter 40 jahren etwa 2 , 5 - mal grer . schlielich zeigt die aktuelle studie , dass die kardialen risiken einer strahlentherapie bei frauen , die auch eine chemotherapie erhalten , grer sind und dass die systemtherapie mglicherweise die strahlenbedingten schden potenzieren kann . 
die kardiotoxizitt der anthrazykline ist dosisabhngig , ber die jahre progressiv und irreversibel [ 9 ]  . fazit das risiko einer strahlentherapie fr kardiale toxizitten ist heute gering , bei patientinnen mit brusterhaltender therapie sogar gnstig fr die radioonkologie : rr 0 , 70 ; nach mastektomie minimal erhht : rr 1 , 24 . die ergebnisse der hier diskutierten studienauswertung sind aber aus drei anderen gesichtspunkten interessant : 958 strahlenther onkol ( 2020 ) 196 : 956958 1 . 
sie besttigen zum ersten mal das altersabhngige risiko fr die kardiale toxizitt der strahlentherapie und relativieren das risiko fr die 60 + patientinnen . dadurch rcken die aktuellen studienergebnisse vor allem die junge patientin mit ( neo - ) adjuvanter anthrazyklinhaltiger systemtherapie und strahlentherapie der regionalen lymphknoten entlang der a . 
duma gibt an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
darby s et al ( 2011 ) effect of radiotherapy after breast - conserving surgery on 10 - year recurrence and 15 - year breast cancer death : meta - analysis of individual patient data for 10 , 801 women in 17 randomised trials . 
early breast cancer trialists collaborative group ( 2000 ) favourable and unfavourable effects on long - term survival of radiotherapy for early breast cancer : an overview of the randomised trials . 
in this fast - growing eld of research , radiomics may allow for a more sophisticated analysis of imaging data , far beyond the qualitative evaluation of visible tissue changes . 
through use of quantitative imaging data , more tailored and tumour - specic diagnostic work - up and individualized treatment concepts may be applied for oncologic patients in the future . 
this is of special importance in cross - sectional disciplines such as radiology and radiation oncology , with already high and still further increasing use of imaging data in daily clinical practice . 
with the introduction of online target surveillance with implanted markers , 3d - ultrasound on conventional linacs and hybrid magnetic resonance imaging ( mri ) - linear accelerators , individualized adaptive radiotherapy is heading towards realization . 
the use of big data such as radiomics and the integration of articial intelligence techniques have the potential to further improve image - based treatment planning and structured follow - up , with outcome / toxicity prediction and immediate detection of ( oligo ) progression . 
bettina baessler , md bettina.baessler@usz.ch 1 department of radiation oncology , university hospital mannheim , medical faculty of mannheim , university of heidelberg , theodor - kutzer ufer 13 , 68167 mannheim , germany 2 department of radiation oncology , medical faculty and university hospital cologne , university of cologne , kerpener str . 
in this fast - growing eld of research , radiomics may allow for an all - encompassing analysis of quantitative imaging data , far beyond the qualitative evaluation of visible tissue changes . 
through use of multiparametric , quantitative imaging data , a more tailored and tumour - specic diagnostic work - up and individualized treatment concepts may be applied for oncologic patients in the future . the scope of current research in this innovative eld is to identify and critically discuss possible application forms of radiomics , which is why this review tries to summarize current knowledge about interdisciplinary integration of radiomics in oncologic patients . 
this review specically focusses on investigations on radiotherapy in patients with liver cancer , including the ( radio ) - oncologic workow from disease diagnosis , treatment planning , delivery and patient follow - up . strahlenther onkol ( 2020 ) 196 : 888899 radiomics includes not only the commonly known quantitative data features derived from the pixel grey - level histogram , i.e. 
mean , maximum , minimum and median parameters , but also the analysis of imaging data based on computerized mathematical and statistical feature extraction , describing further quantitative characteristics of the segmented regions with regard to tissue heterogeneity , compacity etc . 
radiomic analysis of quantitative imaging parameters may further characterize both tumour and normal tissue and even predict tumour response and toxicity by incorporating these data into statistical or advanced machine learning models [ 25 ]  . there are already some promising data about radiomics clarifying mammographic ndings suspicious for cancer [ 6 ] or predicting mutational status in glioblastomas [ 7 ]  . 
recent radiomics studies demonstrated for the rst time the predictive value for different liver tumours , such as the grade of hepatocellular carcinoma ( hcc ) or the differential diagnosis of other primary or secondary liver tumours and benign liver lesions [ 913 ]  . 
a short section on radiomics for monitoring and follow - up will then be followed by a summary of radiomics in the imaging of the post - treatment liver . finally , we will give a short overview about current limitations in the eld of radiomics . indications for radiotherapy with the introduction of image guidance and conformal radiotherapy techniques , the treatment of both primary and secondary liver tumours has experienced signicant improvement over the past few years , leading to increased local control rates and decreased normal tissue toxicity [ 1419 ]  . recent clinical data indicate that additional local therapy to each metastatic lesion can prolong the overall survival of oligometastatic patients [ 2022 ]  . 
furthermore , immunotherapy enables new treatment options for several tumour entities , especially in combination with radiotherapy [ 23 ]  . the present review article aims at summarizing the work which has been done in the eld of radiomics in liver imagin patients with oligometastatic disease , especially hepatic metastases exhibit different treatment courses . 
 [ 11 ] to evaluate the accuracy for classication of hepatic tumours wu et al . [ 12 ] to predict histopathological grading for hcc cases 37 hccs , 23 metastatic tumours , and 33 hhs combination of quantitative adc histogram parameters and li - rads categorization yielded the best prediction accuracy for distinction of hcc compared to icc and combined hcc - icc radiomics - based assessments could be used to distinguish between hcc and hh on precontrast images , thereby allowing noninvasively efcient identication and minimizing errors from visual inspection using texture analysis or topological data analysis allows for classication of the three hepatic tumours with considerable accuracy a computed radiomics signature itself or combined with clinical factors could help to classify the patients into high - grade or low - grade hcc the columns aims and conclusion are directly based on the original work as cited in the column author ( wording partly adapted )  . cect contrast - enhanced computed tomography , er early recurrence , hcc hepatocellular carcinoma , li - rads liver imaging reporting and data system , mri magnetic resonance imaging , mvi microvascular invasion 890 strahlenther onkol ( 2020 ) 196 : 888899 with up to ve lesions are increasingly treated with aggressive metastasis - directed treatment options , improving survival in some patients , even in case of recurrent liver metastases [ 24 , 25 ]  . 
in comparison to other locally ablative treatment options , resection is anticipated for patients with isolated liver metastases , although being characterized with an increased post - procedure morbidity [ 24 , 26 ]  . consequently , minimally invasive options like transarterial chemoembolization ( tace ) and radiofrequency / microwave ablation ( rfa / mwa ) have been evaluated , demonstrating good high local control rates and safety records [ 2730 ]  . 
nevertheless , ongoing technical improvements provide promising data , especially in the case of sbrt of liver metastases , with median overall survival rates of 31.5 months in colorectal cancer patients [ 32 ]  . primary liver cancers are generally intended to be resected . 
furthermore , there is increasing evidence that sbrt may even be superior to tace regarding survival and recurrence , and especially after prior tae / tace treatment [ 36 , 37 ]  . 
in case of sbrt in cholangiocellular carcinoma ( ccc ) patients , 3 - year os rates are about 21% , with increasing local control rates depending on delivered dose ( biological effective radiation dose [ max ] > 91 gy [ / = 10 gy ] ) [ 38 ]  . although rfa is regarded as the main alternative treatment option in unresectable hcc , retrospective data indicate the possible superiority of sbrt as compared to rfa with regard to tumours > 2 cm [ 18 ]  . 
if transplantation is indicated , a combination of neoadjuvant sbrt and tace provides promising remission and reasonable overall survival rates [ 40 , 41 ]  . radiomics for treatment planning target volume denition : automatic segmentation of target volumes and organs at risk the functional capability of the liver to regenerate and proliferate has been used for a long time in liver surgery [ 42 ]  . when it comes to a healthy liver , 80% of the organ can be removed . 
although the whole liver exhibits a low radiation tolerance , potentially leading to the serious condition of radiotherapy - induced liver disease ( rild ) [ 4349 ] , the regenerative potential and the parallel radiobiological character of the liver allows for application of high doses to a dened volume without compromising liver function [ 50 ]  . patients with liver metastases usually have a functionally healthy liver . 
in contrast to liver metastases , most patients with primary liver tumours have liver cirrhosis , which limits local ablative and surgical treatments due to the subsequently impaired liver function [ 53 , 54 ]  . 
current understanding of the radiation - induced impairment of liver function sees hepatic veno - occlusive disease as the pathological hallmark of liver injury [ 55 ] , while at the same time , the vulnerability of ( hepato ) biliary structures has to be taken into account , especially for centrally located liver cancer [ 56 , 57 ]  . tolerance doses / dose constraints for therapy planning in organs at risk have been investigated for decades , which is why tolerance doses also rely on data being gained with different radiotherapy techniques andmost importantlywith irradiated volumes signicantly larger than the volumes in modern radiotherapy techniques such as sbrt [ 58 ]  . 
consequently , organs at risk ( oar ) constraints have to be re - evaluated in order to allow for more tailored treatment concepts and monitoring during treatment on the basis of clinical and multiparametric quantitative imaging data . 
with sbrt being characterized by different biological efcacy as compared to standard radiotherapy , dose escalation may be performed under consideration of dose constraints based on analyses on clinical toxicity [ 5963 ]  . radiomic analysis and its use during treatment planning might further contribute to improved dose escalation schemes and allow for future automation and increased robustness of target volume delineation . 
in addition , a more reliable identication of high - risk regions with possible tumour inltration ( clinical target volume [ ctv ] ) might be enabled by radiomics , since radiomics extends beyond the visible tumour inltration and provides quantitative data on potential tumour extension [ 64 , 65 ]  . 
in addition , several promising studies ( table 2 ) have been conducted in liver tumours , where microscopic characteristics could be identied based on radiomics , thus potentially enabling the detection of microscopic tumour inltration of strahlenther onkol ( 2020 ) 196 : 888899 fig . 
high - level statistical modelling involving machine learning is applied for disease classication , patient clustering and individual risk stratication healthy liver tissue with the inherent potential of more precise clinical target volume delineation in the future . 
using a radiomics approach based on contrast - enhanced t1 - weighted mri in the hepatobiliary phase , t - cell inltration in the tumour and peritumoural margin could be quantied [ 71 ]  . 
ex - vivo investigations in mice demonstrated the detection of microscopic tumour inltration locations by the radiomic histogram feature skewness in liver single - photon emission ct ( spect ) imaging [ 72 ]  . 
thus , further specication of regions with a high risk of liver tumour inltration may be enabled by radiomics in the future [ 70 , 71 ]  . independently of current research on standardization of dose prescription , target volume denition is increasingly based on functional imaging , such as metabolic imaging with positron - emission tomography ( pet ) and functional sequences of mri , including diffusion - weighted imaging ( dwi ) [ 73 , 74 ]  . 
pet - imaging allows for quantitative evaluation of metabolic function in the liver tumour and normal liver tissue , thus leading to the possibility of adapted target delineation and dose reduction in the normal liver tissue [ 75 ]  . 
in contrast to pet - based image - guided treatment planning , contrast - enhanced mri ( including with liver - specic agents ) is already part of daily clinical practice in treatment planning for patients with liver cancer [ 76 ]  . contrast - enhanced t1 - weighted sequences allow for morphological target delineation , but functional imaging sequences such as dwi provide additional information about perfusion fractions by intravoxel incoherent motion ( ivim ) , cellularity by the adc and even tissue complexity by kurtosis evaluation [ 7784 ]  . 
besides this , liu et al . showed that synthetic ct datasets can be generated from mri to ensure accurate liver sbrt [ 86 ]  . adding to radiomics , the increasingly used deep learning methods are able to learn directly from the data , thus circumventing the need for handcrafting of discriminative imaging features representing the key concept behind radiomics . 
recently , automatic ctv segmentation has been shown by using convolutional neural networks ( cnn ) , which appear to be especially useful for image segmentation tasks [ 8789 ]  . 
deep learning - based auto - contouring of the tumour volume has been shown to be at least as efcient as manual contouring of the oar for mri - guided adaptive radiotherapy [ 90 , 91 ]  . 
 [ 65 ] strahlenther onkol ( 2020 ) 196 : 888899 adaptive radiotherapy : dose painting the idea of adaptive radiotherapy summarizes the goals of patient - specic and tumour - tailored treatment concepts , allowing for both adapted treatment planning with locally volitional dose escalation in malignancies and reduction of dose exposure in the surrounding normal tissue . 
however , daily image guidance with cone beam computed tomography ( cbct ) scans and consecutive plan adaptions request a high cost in resources while only providing low - resolution cbct images . 
the latest introduction of hybrid mr - guided radiotherapy gadgets might nally allow for online imaging and plan adaption based on high - resolution images , especially with respect to the soft tissue of upper abdominal organs [ 93 ]  . 
furthermore , this also allows for taking into account tumour heterogeneity based on quantitative , functional imaging data , exceeding the purely morphological characteristics and potentially allowing for earlier evaluation of tumour response and local control failure already at the beginning of radiotherapy and in the meantime ( table 3 ; [ 91 , 94 ] )  . independent of general outcome analysis , the incorporation of radiomics into treatment planning may further improve the analysis and prediction of normal tissue toxicity , as proposed by the quantec group ( quantitative analysis of normal tissue effects in the clinic ) [ 95 , 96 ]  . there are already promising data with regard to toxicity after radiotherapy of head and neck and lung cancers [ 97 , 98 ]  . 
generally , toxicity analysis in healthy liver tissue should be improved even more , since mri enables accurate liver function analysis and radiomics analysis allows for accurate staging of liver brosis and may prevent and , vice versa , predict rild [ 101104 ]  . monitoring / follow - up first promising results regarding the predictive potential of radiomics for local response after radiotherapy and tace have recently been demonstrated [ 105107 ] and are listed in table 4 . 
demonstrated that three delta - radiomics texture features extracted from low - eld mri during sbrt in liver were able to differentiate between local disease control and local control failure the columns aims and conclusion are directly based on the original work as cited in the column author ( wording partly adapted )  . cect contrast - enhanced computed tomography , er early recurrence , hcc hepatocellular carcinoma , mri magnetic resonance imaging , mvi microvascular invasion 894 strahlenther onkol ( 2020 ) 196 : 888899 conclusion imaging modality number , ( training ( t ) and validation ( v ) set , where available ) cemri table 4 radiomics for monitoring / follow - up author aims reimer et al . 
even in case of cholangiocarcinoma , preoperative mri was able to predict early recurrence , especially in combination with immunohistochemical markers [ 109 ]  . imaging of the post - treatment liver in addition to a temporary / reversible decline in metabolic function , liver tissue is characterized by distinct macroscopic , microscopic and ct / mr - morphological changes after radiotherapy ; exemplary changes are given in fig . 
repetitive imaging during and after radiotherapy demonstrated that changes in metabolic liver function are also accompanied by distinct changes in quantitative imaging data of the liver tumour and the normal liver tissue [ 53 , 111114 ]  . nevertheless , there are still few data about quantitative imaging encompassing the whole treatment course of liver tumours , especially with respect to normal tissue alterations . 
multiparametric imaging might allow for both specication in staging examinations and acceleration by the use of quantitative imaging parameters , potentially replacing extensive amounts of qualitative imaging sequences for visible , mainly qualitative evaluation of the tumour and normal tissue . 
sequences such as dwi with quantitative adc maps are characterized by these possibilities and allow for functional analysis of the tumour response after sbrt [ 115 ]  . as a consequence , integration of this quantitative data might lead to an improvement of oncologic patient management in future , especially with respect to the large amount of radiological data in image - guided radiation oncology . 
with regard to radiation oncology , the so - called radiomics concept with computerized algorithm - based parameters may be successfully integrated into daily clinistrahlenther onkol ( 2020 ) 196 : 888899 fig . 
white arrows highlight the region of interest including the hepatic metastasis in the right liver lobe and the peritumoral changes after sbrt cal practice , supporting decision - making and improving the workow of radiation therapy . current limitations of radiomics as reviewed above , radiomics for radiotherapy of liver tumours is highly promising , but we are still in need of further data about its validity and optimal usage for a reliable translation to daily clinical practice . 
the correct and robust application of radiomics analysis has to be investigated , since the algorithm - based analysis of quantitative date is not standardized within different institutions , or even within single institutions , and can easily be performed differently . 
independently of softwareand hardware - induced variability [ 116121 ] , texture analysis is also hindered by uncertainties in patient immobilization and organ movements , especially with regard to mri examinations [ 122 , 123 ]  . 
on top of this , its usage for treatment decisions and treatment planning has to be investigated in prospective trials including ex - vivo , in - vivo volunteer and in - vivo patient examinations allowing for founded conclusions about its usage . 
furthermore , the analysis of radiomics necessitates sufcient informational technique ( it ) infrastructure with high data storage capacity and computational performance in image analysis , which is why the introduction of radiomics analysis in radiation oncology requests an it structure similar to the one in radiology institutions . independent of providing sufcient software and hardware , incorporation of radiomics into radiation oncology also necessitates interdisciplinary teams , including medical doctors ( clinical radiation oncologists , clinical radiologists ) , medical physicists and most importantly , computer scientists . 
the evaluation of radiomics on the basis of incorporating the imaging data together with clinical and histological data into articial intelligence techniques , such as deep convolutional neural networks , is of utmost importance . 896 conclusion due to the introduction of modern radiation treatment techniques such as sbrt and igrt , radiotherapy is capable of successfully treating both primary and secondary liver tumours , with promising local control rates . 
with the possibilities of multiparametric , quantitative data , including the deeper radiomics analysis , information exceeding qualitative evaluation of visible changes may be included into oncologic radiology and radiation oncology . 
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if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
by providing a three - dimensional characterization of the lesion , models based on radiomic features from computed tomography ( ct ) and positron - emission tomography ( pet ) have been developed to detect nodules , distinguish malignant from benign lesions , characterize their histology , stage , and genotype . 
deep learning models have been applied to automatically segment organs at risk in lung cancer radiotherapy , stratify patients according to the risk for local and distant recurrence , and identify patients candidate for molecular targeted therapy and immunotherapy . 
moreover , radiomics has also been applied successfully to predict side effects such as radiationand immunotherapy - induced pneumonitis and differentiate lung injury from recurrence . radiomics could also untap the potential for further use of the cone beam ct acquired for treatment image guidance , four - dimensional ct , and dose - volume data from radiotherapy treatment plans . 
over time , radiologists have identied a relatively small number of qualitative visual physical characteristics to differentiate benign and malignant lesions , for example , the historical use of speculation , lesion size , attenuation , and perilesional cystic airspaces . 
radiomic features are image - based descriptors able to quantitatively capture shape , size or volume , and texture of tumor or normal tissue regions ; they can be combined with articial intelligence applications into predictive and prognostic models [ 3 , 4 ]  . the current challenge for radiomic applications to the thorax is twofold : first , systems must be developed to accurately extract phenotypic characteristics from images , and second , systems must determine which features , among ( cid : 2 ) michele avanzo mavanzo@cro.it 1 department of medical physics , centro di riferimento oncologico di aviano ( cro ) irccs , via f . 
gallini 2 , 33081 aviano , pn , italy 2 guerbet sa , villepinte , france thousands of phenotypic characteristics , correlate with the underlying genotype and disease behavior , thus aiding in the prognosis and clinical management of disease [ 5 ]  . perhaps one of the earliest works showing correlation of imaging biomarkers , or radiomic features , to a patients prognosis or response to therapy was in nwogu et al . [ 6 ] , who found a correlation between the energy feature and time to progression . 
 [ 7 , 8 ] , where computed tomography ( ct ) - based textural features of nonsmall cell lung cancer ( nsclc ) were correlated to tumor metabolism , positron emission tomography ( pet ) tumor stage and histopathology of lung tumor . deep learning networks or convolutional neural networks ( cnn ) are multi - layer feed - forward neural networks that accept 3d images as input and can be trained end - to - end in a supervised method while learning highly discriminative image features ; this eliminates the requirement of handcrafted radiomic features of images . 
the machine learnt features produced by the cnn from analysis of the raw data can also be studied for associations with the endpoint or for training machine learning ( ml ) classiers [ 9 ]  . 
the opportunity to mine large databases , i.e. , big data , and the use of machine / deep learning is paving the way to a wider adoption of these techniques , especially as a virtual image880 strahlenther onkol ( 2020 ) 196 : 879887 based biopsy [ 10 ] to minimize the risk of pneumothorax , obtain a three - dimensional characterization of the lesion , and support the use of companion diagnostics in personalized / target therapies . although radiomics has been applied to many diseases , lung tumors are the most extensively studied and characterized malignancies through radiomics so far [ 11 , 12 ]  . 
in fact , due to several unmet clinical needs in the theragnostic chain , lung cancer often represents a scenario where a radiomics method can be tested , compared , or rened , whether in feature selection [ 13 ] or ml methods [ 14 ] , or for assessing the feasibility of novel imaging techniques such as cone beam computed tomography ( cbct ) [ 15 , 16 ]  . the main goal of this article is to provide an update on the current status of lung cancer radiomics , addressing issues related to its widespread applications in nodule detection , segmentation , characterization , and prediction of patients outcome . radiomics in lung cancer detection , segmentation and characterization cancer detection , contouring , and characterization pulmonary imaging presents unique challenges to both radiologists and radiomics systems , because lung nodules can be small and appear similar to other structures in the lung such as blood vessels or benign processes such as focal organizing pneumonia [ 17 ]  . 
for these reasons , lung cancer screening based on ct has a high false - positive rate [ 5 ]  . the accuracy of detection of tumor lesions can be improved signicantly by combining the extraction of radiomic features with ml . 
using the low - dose cts from the national lung screening trial ( nilst ) database , it was shown that radiomic features can improve the accuracy in detection of nodules compared to size and shape [ 18 ]  . 
in the same database , a random forest classier using 23 radiomics features from low - dose ct obtained a low falsepositive rate ( 911% ) in cross validation [ 2 ]  . 
a support vector machines ( svm ) classier was developed to distinguish adenocarcinoma from focal organizing pneumonia using combined clinical and radiomic variables , with 87.6% accuracy [ 17 ]  . 
because malignant lung lesions have radiomic textural characteristics in ct that are distinct from benign lesions [ 19 ] , ct - based radiomic signatures score high accuracy in distinguishing malignant lesions [ 20 , 21 ]  . deep learning was useful in recognition of small lung nodules on ct from the lung image database consortium and image database resource initiative ( lidc - idri ) , with an accuracy of 97.6% [ 22 ] , classifying pulmonary nodules without the need for tumor segmentation [ 9 ] and identifying adenocarcinomas in patients with solitary sub - solid pulmonary nodules [ 23 ] also in low - dose ct [ 24 ]  . handcrafted or machine learnt features can be integrated in a nomogram including also ct - based subjective ndings . 
this method improved accuracy of differentiation of invasive from minimally invasive lesions [ 25 ]  . segmentation of regions of interest in lung cancer in radiomics studies of lung tumor , the lesion is often manually delineated by an experienced radiologist or radiation oncologist , e.g. , [ 21 , 2628 ]  . 
however , automatic or semi - automatic segmentation increases reproducibility [ 29 ] , yielding more stable radiomic features compared to those extracted from manual segmentations [ 30 ]  . 
semiautomatic segmentation methods , such as region growing [ 31 ] or multi - seed methods [ 32 ] , start from seed pixels chosen from the operator inside the tumor or region of interest ( roi ) encompassing the lesion on a single slice [ 33 ]  . in positron - emission tomography ( pet ) , where segmentation is affected by the image noise , lung tumor can be semi - automatically delineated by a relative threshold method [ 13 , 34 ] or variational approaches , attempting to exploit the gradient differences between the foreground lesion and the background [ 35 ]  . 
fully automated segmentation methods in pet have also been proposed , using fuzzy random walk [ 36 ] or mutual information of ct and pet to identify nsclc [ 37 ]  . cnn have been applied to automatically segment organs at risk in lung cancer radiotherapy [ 38 ]  . 
u - net , one of the most popular architectures of cnn for image segmentation , has proven capable of segmenting lung parenchyma [ 39 ]  . u - net has been proposed for segmentation of lung tumor , with improved accuracy due to the use of the morphological and metabolic information provided by pet - ct hybrid imaging [ 40 ]  . prediction of histology and tumor stage the main challenge to correlate image phenotype to histological results consists of the sampled nature of biopsy , which intrinsically limits the characterization of the whole lesion . 
on the other hand , for many excised lesions , full histological characterization per slice is available , hence the possibility of mapping the excised lesion to the radiological shape and creating a prediction model . 
1. a nave bayess classier was trained to predict histopathology from radiomic features selected by means of relief feature selection and showed an area under the curve ( auc ) of 0.72 in the validation cohort [ 26 ]  . 
radiomic features of nsclc extracted from ct are also related to pet tumor stage [ 7 ] as well as micropapillary patterns in lung adenocarcinoma [ 42 ]  . tumor genotype the identication of tumor genotype , especially gene mutation , plays a key role in selecting appropriate treatment strategies for nsclc patients , as tumors which overexpress oncogenes such as the epithelial growth factor receptor ( egfr ) have a higher response rate to molecular targeted therapies such as egfr tyrosine kinase inhibitor ( tki )  . since some ct radiomic features are correlated with egfr mutation [ 43 ] , radiomics holds the promise of decreasing the cost of identication of egfr mutation status as well as a full three - dimensional assessment of the tumor . 
more recently , a ct radiomic signature of three variables ( one histogram and two glcm and grey - level run length matrix [ glrlm ] , textural features ) predicted egfr mutation [ 45 ]  . 
in petbased radiomics , radiomic features could detect egfr mutation status , but were unable to nd a signature correlating to kirsten rat sarcoma viral oncogene homolog ( kras ) mutations [ 46 ]  . chromosomal rearrangements that lead to gene fusions are also of clinical interest , as fusion - positive patients may benet from targeted drugs . 
radiomics can also select lung cancer patients with anaplastic lymphoma kinase ( alk ) rearrangement , potentially making them candidates for crizotinib , a multi - targeted tki with potent activity against alk [ 47 ]  . 
significant associations were also revealed between prognostic radiomic features extracted from ct and gene expression patterns measured for 21 , 766 genes identied using gene set enrichment analysis in a lung cancer cohort ( gsea ) [ 21 ]  . the deep learning features extracted for mortality risk stratication were correlated to global gene expression patterns identied using a pre - ranked gene set enrichment analysis ( gsea ) [ 50 ]  . 882 strahlenther onkol ( 2020 ) 196 : 879887 prediction of treatment outcome survival because radiomic features can describe histology [ 26 ] and genetic footprint [ 32 , 48 ] of the tumor , which are correlated with tumor aggressiveness and potential curability , they can be used to build models to predict the outcome , in terms of local / distant control or survival , of cancer therapy performed with various therapeutic options ( radio - , chemotherapy , targeted molecular therapy , immunotherapy ) or a combination of them . complete response and local control stereotactic body radiotherapy ( sbrt ) is now a standard of care option for patients with lung cancer , especially those who are not candidate for surgery . 
several combinations of feature selection and ml classiers based on ct images were compared to predict recurrence in sbrt patients , and the best result was obtained with random forest and nearzero variance feature selection [ 52 ]  . by applying supervised principal component analysis , features from hybrid pet - ct imaging were found to improve prediction of recurrence after sbrt [ 53 ]  . 
 [ 54 ] , a radiomic signature with one feature from pet and one from ct resulted in high specicity and sensitivity for recurrence after sbrt in a validation dataset . distant metastases radiomic models to predict the development of distant metastases ( dm ) from nsclc in lung cancer patients treated with sbrt were developed using features from ct [ 28 ] or from pet - ct [ 53 ]  . 
a radiomic signature of four features based on a laplacian of gaussian ( log ) lter consisting of wavelet hhl skewness , glcm cluster shade , and log 5 mm 2d skewness , combined with clinical data , was prognostic for both dm and survival in locally advanced adenocarcinoma [ 55 ]  . the peritumoral space around the tumor , dened as a region extending radially from the nodule boundary up to roughly 12 cm , can provide valuable information regarding the risk of distant failure , as more invasive tumors may have different morphologic patterns in the tumor periphery due to the presence of microscopic disease [ 56 ]  . 
analysis of the peritumoral space radiomic features by a svm classier predicted distant failure , achieving an accuracy of 0.83 in a validation dataset [ 57 ]  . most of the radiomics studies on lung cancer have focused on providing prognostic signatures , that is , combinations of radiomic features capable of predicting survival of patients or stratifying patients according to the expected survival . a signature with ve ct - based features selected using the relief method was predictive for survival , and , after training of a decision trees classier , resulted in an accuracy of 77.6% in the leave - one - out cross validation [ 11 ]  . a radiomic signature consisting of a combination of four features from ct obtained in a retrospective lung cancer cohort of 422 lung cancer patients was predictive for survival and was successfully tested on cohorts of different cancer types ( lung , head and neck cancer ) , thus demonstrating a certain level of translational capability of radiomics to different cancers [ 21 ]  . although less frequently investigated , pet - based radiomic features have also been proven to be of prognostic value for lung cancer patients . 
one textural feature calculated from the gray - level co - occurrence matrix ( glcm ) in the pretreatment pet identied using the lasso procedure was an independent predictor of overall survival [ 58 ]  . 
the overall performance of prognostic signatures is highest when combining radiomic , genetic , and clinical information [ 49 ]  . deep learning models applied to time series ct scans were signicantly predictive of survival and cancer - specic outcomes ( progression , dm , and local - regional recurrence ) [ 59 ]  . transfer learning , an approach where pretrained networks on images from other domains are tuned on a new dataset , can address the issue of a limited sample size . 
in the work of rahul et al . , the features learnt by a pretrained deep learning network were combined with radiomics and traditional quantitative features and used in a decision trees classier which achieved an accuracy of 90% for prediction of survival in adenocarcinoma patients [ 60 ]  . deep learning has also been proposed to stratify nsclc patients according to mortality risk using standard of care ct . 
in a retrospective study of 1194 patients from 7 institutions , authors found a signature made of deep learning features for survival ( > or < 2 years ) after radiotherapy or surgery [ 50 ]  . a model based on changes in intensity in intra - tumor partitions outperformed radiomics for predicting overall survival status after 2 years [ 61 ]  . response to chemoand molecular targeted therapy chemotherapy response dened according to response evaluation criteria in solid tumors ( recist ) and time to progression were studied in a cohort of patients treated strahlenther onkol ( 2020 ) 196 : 879887 with pemetrexed - based platinum doublet chemotherapy . radiomic features were extracted from the tumor and peritumoral compartment around the nodule dened automatically by dilation of 15 mm from the tumor and resulted in an auc of 0.77 in an independent set [ 62 ]  . 
in a retrospective multicohort study , an eight - feature radiomic signature predictive of the presence of cd8 t cells , which is related to the tumor immune phenotype , was developed from contrastenhanced ct images using an elastic net regularized regression method . 
early prediction of tumor recurrence , which typically manifests after 1 year , can be performed by radiomics from ct scans acquired at approximately 3 and 6 months from sbrt [ 65 ]  . radiomic features were mined to describe the outcome of nsclc patients after sbrt . 
the feature wavelet llh range , measuring the range of voxel intensity values in the wavelet - ltered image and related to tumor heterogeneity , was prognostic for developing dm . 
ct and pet - derived features were included in radiomic signatures that predicted overall survival , disease - specic survival , and regional control [ 53 ]  . twelve radiomic features were extracted from contrastenhanced ct images of patients from a training cohort ( n = 147 ) treated with surgery and an independent validation cohort ( n = 295 ) treated with sbrt . 
the resulting model was signicantly associated with both overall survival and dm [ 66 ]  . prediction of side eects radiomics - based models can help identify the development of side effects early . 
the preto post - treatment ( at 3 , 6 , and 9 months ) changes in ct radiomic features signicantly correlated with post - sbrt radiation - induced lung injury ( rili ) and were also found to be correlated with dose and fractionation [ 67 ]  . a logistic regression - based classier was constructed to identify patients who will develop grade 2 radiation pneumonitis among those who received rt for esophageal cancer [ 68 ]  . 
the addition of ct radiomic features extracted from the total lung volume offered superior model performance with respect to traditional dosimetric and clinical predictors of radiation pneumonitis ( rp ) , suggesting that pre - treatment ct radiomic features should be considered in the context of rp prediction [ 69 ]  . 
dosiomics , or integration of dose features from the dose distribution in the irradiated lung calculated in the planning ct , has also shown to be predictive of rp [ 71 ]  . identication of post - treatment recurrence the differentiation of tumor recurrence from benign radiation - induced changes in follow - up images can be a major challenge for the clinician [ 72 ]  . 
a radiomic signature consisting of 5 ct - based features demonstrated a high discriminative capability to differentiate recurrence of lung tumor from consolidation and opacities in sbrt patients [ 73 ]  . adding radiomic features to conventional prognostic factors improves nsclc patient risk stratication [ 74 ]  . 
the change in feature values between the two scans was strongly predictive of treatment response , and the same features were also highly stable for testretest [ 75 ]  . 
features calculated from pretreatment and weekly intra - treatment cts were found to signicantly change during radiation therapy ( rt ) for nsclc [ 76 ]  . considering that cbct is now widely adopted for precise patient setup of rt , delta radiomics performed on the cbct images acquired for image guidance would allow large - scale study of tumor response to total dose , fractionation , and fraction dose . 
it has been shown that , reproducible features can be extracted from cbct [ 16 ] which are also predictive as much as features from ct for overall survival in nsclc patients [ 15 ]  . 
despite much effort in assessing feasibility and reproducibility [ 78 ] , one study failed to demonstrate an increase of predictive power when adding longitudinal cbct features to ct features [ 79 ]  . since lung tumors are subject to respiratory motion , fourdimensional ( 4d ) ct allows the 3d imaging of every phase of the respiratory cycle , and 4d radiomic features can be extracted from 4d - ct , allowing for richer characterization of tumor phenotype . 
the stability of radiomic features across different phases has been investigated in a group of 20 nsclc patients , resulting in shape features being the most stable , and a three - feature signature obtained by selecting the features most stable in 4dct was predictive for survival [ 80 ]  . because the dose from the radiotherapy treatment is correlated at the voxel level to tumor response as well as to the risk for complications such as radiation - induced lung injury [ 81 ] , radiomic features extracted from the distribution of dose could be of predictive value . 
this approach has recently been termed dosiomics , and has been successfully applied to predict radiation pneumonitis [ 71 ] its integration with other - omics data could be promising . multicenter efforts and databases radiomics is expected to increasingly affect the clinical practice of treatment of lung tumors , optimizing the endto - end diagnosistreatmentfollow - up chafor the models to be robust to any data variability , it will be crucial to develop them by involving multicenter training based on data with a large variety of attributes . 
the introduction of distributed learning [ 82 ] , also known as federated learning , will open the way to the possibility of involving many centers globally , while preserving privacy constraints . 
on the other hand , validation of the model must be based on multicenter studies , so as to validate the robustness of the results to local attributes as well . 
in some cases , when products are developed , some national regulatory agencies require the training ( or at least the validation ) of the model using also local data . 
it has to be noted that many national agencies are discussing the framework to clear articial intelligence solutions ( including radiomics based ) , hence the possibility of showing the safety and efcacy of a given solution within the local population plays a key role . large publicly available datasets include the aforementioned national lung screening trial ( nilst ) and the cancer imaging archive , which have been used for training [ 2 , 18 ] and validation [ 83 ] of models . 
a dataset consisting of 31 sets of repeated ct scans acquired approximately 15 min apart is now publicly accessible through the reference image database to evaluate therapy response ( rider ) , which allows testretest analysis , a comparison of the results from images acquired within a short time on the same patient [ 84 ] , for selecting the most stable features [ 21 ]  . 
multicentric studies with retrospectively collected data pose the risk of multicenter reproducibility , e.g. , different acquisition and reconstruction settings which may result in limited performance of radiomics models or biased results [ 85 ]  . 
harmonization techniques such as the combating batch effect ( combat ) can reduce the differences in lung cancer features among patient cohorts from institutions using different imaging protocols . conclusion radiomics can reveal key components of lung tumor phenotype of diagnostic , prognostic , and predictive value , signicantly augmenting the evidence - based humans capabilities . radiomics holds the potential to revolutionize conventional tumor characterization and replace classic approaches based on macroscopic and microscopic ( biopsy and histopathology ) analyses . 
lung cancer is the area where radiomics is expected to affect the clinical practice in the nearest future , given the huge efforts to satisfy the unmet clinical need still present . 
a word of caution should be spent to highlight the importance of the explainstrahlenther onkol ( 2020 ) 196 : 879887 ability of the deep learning models compared to the intuitive nature of explanation of feature - based approaches such as radiomics . 
ruge2 , 4 norbert galldiks1 , 3 , 4 philipp lohmann1 , 2 received : 29 march 2020 / accepted : 22 april 2020 / published online : 11 may 2020 the author ( s ) 2020 abstract background magnetic resonance imaging ( mri ) and amino acid positron - emission tomography ( pet ) of the brain contain a vast amount of structural and functional information that can be analyzed by machine learning algorithms and radiomics for the use of radiotherapy in patients with malignant brain tumors . methods this study is based on comprehensive literature research on machine learning and radiomics analyses in neuroimaging and their potential application for radiotherapy in patients with malignant glioma or brain metastases . results feature - based radiomics and deep learning - based machine learning methods can be used to improve brain tumor diagnostics and automate various steps of radiotherapy planning . 
in glioma patients , important applications are the determination of who grade and molecular markers for integrated diagnosis in patients not eligible for biopsy or resection , automatic image segmentation for target volume planning , prediction of the location of tumor recurrence , and differentiation of pseudoprogression from actual tumor progression . 
in patients with brain metastases , radiomics is applied for additional detection of smaller brain metastases , accurate segmentation of multiple larger metastases , prediction of local response after radiosurgery , and differentiation of radiation injury from local brain metastasis relapse . 
importantly , high diagnostic accuracies of 8090% can be achieved by most approaches , despite a large variety in terms of applied imaging techniques and computational methods . conclusion clinical application of automated image analyses based on radiomics and articial intelligence has a great potential for improving radiotherapy in patients with malignant brain tumors . 
most of the available local treatment options , including radiotherapy and neurosurgery , heavily depend on precise knowledge of tumor type , location , and extent that can only be derived from modern imaging methods such as magnetic resonance imaging ( mri ) and positron - emission tomography ( pet ) [ 1 ]  . 
conventional mri techniques are t1 weighted , t2 weighted , and uid attenuated inversion recovery ( flair ) images , while advanced mri methods include perfusion - weighted imaging ( pwi ) , diffusion - weighted imaging ( dwi ) including its variants such as diffusion - tensor imaging ( dti ) , and mr spectroscopy ( mrs )  . 
the applied machine learning methods mainly comprise feature - based radiomics , where modeling is based on a mathematically predened set of features extracted from a manually segmented image , and deep learning approaches where the complete model is trained on the imaging data and does not necessarily require a segmented input . 
the following review aims at providing an overview of the results that were achieved by different machine learning approaches for patients with malignant glioma and metastases . glioma pre - therapeutic classication and molecular characterization in 2016 , the world health organization ( who ) published revised guidelines for the classication of tumors of the central nervous systethe most important glioma types in which radiotherapy is integrated into the treatment concept are who grade ii diffuse astrocytomas and oligodendrogliomas , who grade iii anaplastic astrocytomas and anaplastic oligodendrogliomas , and who grade iv glioblastomas . 
the classication is based on both tumor histology as well as the presence of a mutation in the isocitrate dehydrogenase ( idh ) gene and the loss of heterozygosity ( loh ) of the 1p / 19q chromosome arms , which allows an integrated diagnosis according to the who classication 2016 [ 2 ]  . 
possible treatment strategies for radiotherapy of glioma patients including concomitant and adjuvant chemotherapy are predominantly based on the who grade and , more importantly , on molecular characteristics of the tumor [ 3 ] , namely the idh genotype [ 4 ] , the 1p / 19q status [ 57 ] , and the o6 - methylguanine - dna methyltransferase ( mgmt ) promoter methylation status [ 810 ]  . 
however , approximately 15% of glioma are unresectable [ 11 , 12 ] , and stereotactic biopsy carries a measurable risk for morbidity , especially in the older population [ 13 ]  . 
therefore , several studies have investigated the application of radiomics for determination of who grade [ 1421 ] and molecular characteristics [ 2240 ] in glioma . results of selected reports applying radiomics or other machine learning methods on conventional mri , advanced mri , and pet are reported in more detail in the following sections . determination of who grade in patients with newly diagnosed gliomas ditmer and colleagues [ 15 ] investigated the diagnostic accuracy of histogram - based radiomics analysis of post - contrast t1 - weighted mri for the differentiation of high - grade from low - grade gliomas in 94 patients . 
however , the dataset was highly unbalanced and parameter combinations were not investigated . cho and colleagues [ 14 ] applied a radiomics approach using different machine learning classiers for glioma grading based on 285 datasets from the brain tumor segmentation ( brats ) challenge 2017 [ 41 ] comprising preand postcontrast t1 - weighted , t2 - weighted , and flair mri . 
after calculation of 468 radiomics features , 5 were selected for use in a random forest classier that showed the highest auc of 0.92 after vefold cross validation . besides conventional mri , several groups have also used advanced mri methods in combination with radiomics analyses for glioma grading . 
besides mri radiomics , pyka and colleagues evaluated the ability of amino acid pet radiomics using the tracer o - ( 2 - [ 18f ] uoroethyl ) - ltyrosine ( fet ) for glioma grading [ 40 ]  . 
the combination of textural features calculated from the grey - level neighborhood difference matrix and the metabolic tumor volume yielded a diagnostic accuracy of 85% for the differentiation of who grade iii and iv gliomas . yang and colleagues [ 21 ] investigated the usefulness of deep learning - based radiomics using convolutional neural networks ( cnns ) for glioma grading in a group of 113 patients . 
second , the networks were used with the connection weights already pretrained on a dataset of 1.2 million non - medical images from imagenet , a largescale natural image database , and were only netuned by retraining the rst convolutional layer and the nal fully connected layers on the mr images . 
in summary , assessment of who grade in newly diagnosed gliomas by means of machine learning methods achieves an accuracy of approximately 90% and may thus be of clinical benet in patients unsuitable for resection or biopsy . determination of idh genotype and 1p / 19q status in patients with newly diagnosed gliomas once the diagnosis of a diffuse glioma has been made , usually from tissue sampling , the treatment plan , including dose , type , and fractionation of radiotherapy as well as the sequence of chemotherapy , is mainly determined by the molecular characteristics of the tumor based on the who classication [ 3 ]  . 
many groups have shown that these may also be derived non - invasively from imaging by application of machine learning [ 2225 , 3335 , 38 , 39 , 42 , 43 ]  . zhang and co - workers [ 43 ] used conventional mri as well as dwi and extracted a total of 2970 features from 120 patients with who grade iii and iv gliomas . 
finally , a subset of 386 features was used to build a model based on a random forest classication , resulting in an accuracy of 89% for idh prediction in the validation dataset . 
a multi - level machine learning model based on support vector machine classiers was used and allowed classication of idh and 1p / 19q status with accuracies of 88% and 96% , respectively . 
a subgroup analysis of 28 patients measured on a high - resolution brainpet scanner showed the highest accuracy of 86% after 10 - fold cross validation . again , deep learning - based radiomics approaches have also been investigated for prediction of molecular characteristics in gliomas . 
chang and co - workers [ 22 ] used a residual cnn for idh genotype prediction on conventional mri from a large cohort of 496 glioma patients from three different institutions and achieved an accuracy of 86% in an independent test set . 
eichinger and colleagues [ 24 ] used a set of local binary pattern features extracted from t2 - weighted mri and dti for training of a cnn with a single hidden layer . 
these results suggest that radiomics has the potential to substitute neuropathological assessment of idh mutation and 1p / 19q loh status in glioma patients in whom tissue sampling is not feasible . determination of mgmt promoter methylation status the methylation status of the mgmt promoter is of great value for predicting the response to alkylating chemotherapy and has also been determined using advanced image analyses . 
koratis and colleagues [ 28 ] predicted the mgmt promoter methylation status in patients with glioblastoma with a sensitivity of 80% and a specicity of 81% using a four - parameter model based on t2 - weighted mri . 
xi and co - workers [ 36 ] calculated 1665 radiomics features from conventional mri and generated a model from a subset of 36 features , resulting in an accuracy of 87% in the validation data and 80% in a test dataset . similarly , li and colleagues [ 31 ] extracted 1705 radiomics features from conventional mri and built a predictive random forest model using a subset of six features . 
the model achieved an auc of 0.94 in the validation and 0.86 in the test cohort . by means of a bidirectional , recurrent cnn that leverages the spatial aspects of three - dimensional mri scans , han and kamdar [ 25 ] obtained an accuracy of 67% in the validation dataset and 62% in the test data . 
koratis strahlenther onkol ( 2020 ) 196 : 856867 and colleagues [ 29 ] compared three different residual deep neural network ( resnet ) architectures for the prediction of mgmt promoter methylation status based on conventional mri data from 155 patients . 
thus , promising results also exist regarding non - invasive , image - based assessment of mgmt promoter methylation status . image segmentation and delineation of planning target volumes malignant gliomas tend to grow in typical patterns and induce a number of characteristic tissue changes . 
the main tumor compartments , also called segments in image processing , comprise the necrotic core , contrast - enhancing tumor , non - enhancing tumor , and perifocal edema . 
fast and reliable labeling ( contouring ) of these segments is a crucial task in many areas of neuro - oncology such as radiotherapy and image - based follow - up [ 44 ]  . 
numerous algorithms have been developed for this purpose [ 45 ] and a periodically held challenge ( the multimodal brain tumor image segmentation benchmark , brats ) has been set up to compare their efcacy [ 41 , 46 ]  . 
today , the best - performing tools are usually based on cnns [ 47 , 48 ] , which achieve high segmentation accuracies ( dice similarity coefcients ) where almost 90% of the voxels are correctly labeled , which is the order of magnitude that experienced physicians can achieve [ 44 ]  . 
in radiotherapy planning for malignant glioma , delineation of gross tumor volume ( gtv ) and clinical target volume ( ctv ) could in principle be automatically performed by these software tools [ 49 ]  . 
a basic requirement is that segmentation should not only work for untreated tumors but also in less well - dened situations , e.g. , after tumor resection , which is the most common situation in radiotherapy for malignant glioma . 
a powerful segmentation toolkit for scientic use is publicly available at : brats - toolkit . prediction of local relapse location after radiotherapy in malignant glioma , approximately 8090% of recurrences that develop after macroscopic tumor resection and postoperative local irradiation with doses of approximately 60 gy are located within a distance of 2 cm to the margin of the resection cavity and will occur within 69 months after initiation of radiotherapy [ 5054 ]  . 
this observation was used for recommending the size of the geometrical margin between the ctv and the gtv in both european and north american guidelines [ 55 , 56 ]  . 
however , this procedure still results in considerably large volumes of irradiated brain , and almost all attempts to escalate the radiation dose up to 8090 gy within a geometrically dened ctv have failed to improve the prognosis of these patients [ 5760 ]  . 
assuming that the direction of tumor spread is foreseeable and that a doseresponse relationship exists for malignant glioma , prediction of the precise location of a recurrence would be of signicant value . 
ideally , a so - called tumor inltration map of the peritumoral region should be generated that depicts the areas with the highest risk of recurrence , which , in turn , could be targeted by higher doses . 
several approaches including conventional imaging analysis methods and radiomics have been applied to achieve this goal . amino acid pet was used for denition of the ctv in a small study with focal dose escalation to 72 gy . 
although the results were encouraging in terms of survival [ 61 ] , there was only a small overlap between the pet signals at recurrence and the pet signals used for dose planning [ 62 ]  . 
however , it was shown that the gtvctv margins could be reduced by 4 mm for the pet - dened gtv in comparison to the mri - dened gtv in order to include 100% of the recurrences . in addition to pet , advanced mr imaging techniques have been applied for predicting the spread of glioma cells . by use of dwi and dti , regions with restricted diffusion due to increased cellular density can be identied . 
indeed , fractional anisotropy ( fa ) , a measure of directed diffusion , was found to be signicantly lower in regions with later tumor recurrence [ 64 ]  . 
also , areas of the preoperative peritumoral region with a lowered apparent diffusion coefcient ( adc ) overlapped with the region of the later recurrences by 60% [ 65 ]  . 
by this approach , it was shown that tumor growth follows the tracts to some extent [ 66 ] and that this fact can be used to foresee which brain regions are predominantly affected by recurrent tumor growth [ 67 ]  . however , the most promising approaches are probably those that use advanced , multiparametric mr imaging in conjunction with radiomics and machine learning . 
in a series of investigations , a group from the university of philadelphia applied conventional and advanced mr techniques ( preand post - contrast t1 - weighted mri , t2weighted mri , pwi , and dti ) to determine fa , radial diffusivity , axial diffusivity , adc , relative cerebral blood volume , and a number of associated rst - and second - order features in each voxel of the peritumoral region . 
a model was trained to predict the voxels risk for being involved 860 strahlenther onkol ( 2020 ) 196 : 856867 in a recurrent tumor , which resulted in a tumor inltration map that had an overall accuracy of approximately 90% [ 6870 ]  . 
if these maps were routinely available , postoperative radiotherapy of malignant glioma could be far more individualized compared to the present practice . prediction of progression - free and overall survival in radiotherapy planning , not only the putative location of a future recurrence , but also the time interval to progression is of major importance . 
methods including radiomics and machine learning have therefore also been used to predict progression - free ( pfs ) and overall survival ( os ) , which are both closely related to the time to progression . 
when using radiomic features from standard preoperative mri of the primary tumor or the postoperative peritumoral region , predictive models for pfs and os were developed that outperformed those based on clinical features alone [ 71 , 72 ]  . also , the performance of these models improved significantly when using advanced mr imaging features , e.g. , from pwi or dti , and combining them with clinical factors [ 7376 ]  . 
however , kickingereder and colleagues demonstrated in a cohort of idh - wildtype glioblastoma patients with known mgmt methylation status that the addition of radiomic features to a comprehensive model comprising clinical , therapeutic , and molecular features could still improve the prediction accuracy [ 74 ]  . dierentiation of tumor progression from pseudoprogression the term pseudoprogression describes the occurrence of a progressive enhancing lesion on mri within 12 weeks after radiotherapy alone or radiotherapy with concomitant and adjuvant temozolomide chemotherapy in patients with malignant gliomas with spontaneous improvement without any treatment change [ 77 , 78 ]  . 
due to its clinical importance , this time - dependent denition of pseudoprogression was included in the recommendations of the response assessment in neuro - oncology ( rano ) working group [ 79 ]  . several studies have already demonstrated the usefulness of amino acid pet as well as pwi for this challenging clinical task [ 77 , 8082 ]  . 
however , radiomics and machine learning might add important diagnostic information to further improve the diagnostic performance . hu and colleagues [ 83 ] used conventional and advanced mri including dwi and pwi for differentiation of tumor progression from pseudoprogression in 31 patients who underwent radiochemotherapy after surgical resection . an eight - dimensional feature vector was constructed , and a support vector machine classier yielded an auc of 0.94 ( sensitivity 90% ; specicity 94% )  . 
the nal logistic regression model used three textural features and yielded a diagnostic accuracy of 92% after 10 - fold cross validation in the training and 86% in the test dataset . 
akbari and colleagues [ 89 ] also used multiparametric mri data consisting of conventional mri as well as dwi and pwi in a cohort of 63 patients where detailed histopathological conrmation of the diagnosis was available for all patients . 
recently , li and co - workers [ 90 ] introduced a novel featurelearning method based on deep convolutional generative adversarial networks ( dcgan ) and a cnn ( alexnet ) , termed dc - al gan . 
tumors were segmented manually and 1303 radiomic features were calculated on contrast - enhanced mr images . the best classier that showed a high predictive performance in the test cohort ( auc 0.90 ) was a support vector machine algorithm that used the least absolute shrinkage and selection operator ( lasso ) for feature selection . 
also , the classier showed a better performance than experienced neuroradiologists . artzi and colleagues [ 94 ] extracted 760 radiomics features from contrast - enhanced mr images of 439 patients with brain metastases or glioblastoma . 
interestingly , the authors identied the same support vector machine algorithm as the study by qian and colleagues described above to have the highest predictive performance in the test cohort ( auc 0.96 ) for the differentiation of brain metastases from glioblastoma . brain metastases detection and automatic segmentation of brain metastases nowadays , the dominant type of radiotherapy for a limited number and limited total volume of brain metastases is radiosurgery [ 95 ]  . 
automatic segmentation of brain metastases for use in radiosurgery planning differs in several aspects from that of gliomas . as metastases are thought to have a low inltrative potential , denition of the gtv is mainly based on the t1weighted , contrast - enhanced mr images with no or only small gtvctv margins , while other tumor segments are usually not considered . 
therefore , automatic segmentation algorithms should be able to both reliably identify brain metastases ( measured by the detection rate and the falsepositive rate ) and to accurately contour them ( measured by the dice similarity coefcient )  . 
liu and colleagues applied a modied version of the widely used deepmedic cnn for use with small metastases ( < 1.5 cm ) and achieved an average dice coefcient of 0.67 on contrast - enhanced mr images [ 96 ]  . 
in summary , the contouring performance of these automated systems seems to be at the edge of suitability for clinical use , while secure detection of small metastases is at present only possible if a considerable number of falsely labeled non - tumor regions is accepted . prediction of local response after radiosurgery of brain metastases it is widely believed that the main determinants of local response to radiosurgery are tumor volume and prescription dose ; however , the response to radiosurgery is still difcult to predict in a subset of brain metastases . 
this may be partly due to the more radioresistant tumor cells residing at the border of a necrotic core that is present in a proportion of the metastases , and to differences in the tumor vasculature that takes part in promoting the response to single highdose irradiation [ 98 ]  . 
indeed , simple features such as the presence of a necrotic core [ 99 ] , the fraction of contrast - enhancing tumor tissue [ 100 ] , or the extension of the perifocal edema [ 101 ] have been shown to impact on response or survival . 
radiation injury is usually suspected if new contrast - enhancing lesions appear in or adjacent to the gtv and is often indistinguishable from local brain metastasis relapse using conventional mri alone . 
the pathological mechanisms involved in these two processes differ substantially [ 105 ] and should therefore be distinguishable by a radiomics analysis of the associated image changes . peng and colleagues [ 106 ] evaluated the usefulness of mri radiomics for this important question . 
fifty - one radiomics features ( 3 shape features , 14 histogram - based features , and 34 textural features ) were extracted for each lesion on each mri contrast . 
on the contrary , experienced radiologists could only classify 73% of the cases , with a sensitivity of 97% and a specicity of only 19% . similarly , zhang and colleagues [ 108 ] used preand post - contrast t1 - weighted mr images , t2 , and flair from 87 patients after gamma knife ( elekta , stockholm , sweden ) radiosurgery to calculate 285 radiomics features . 
changes in radiomics features ( so - called delta radiomics ) from one follow - up timepoint to the next were evaluated and used for differentiation of radiation necrosis and tumor progression . 
again , no separate test dataset was available . besides mri , amino acid pet has also been investigated to evaluate radiomics for the differentiation of treatment - related changes from brain metastasis recurrence . 
it has been demonstrated that evaluation of the timeactivity curves ( tac ) that represent the tracer uptake over time is helpful for differentiation of treatment - related changes from brain metastasis recurrence [ 109 ]  . 
fifty - two patients with newly or progressive contrast - enhancing lesions on mri after radiotherapy were additionally investigated using fet pet . after feature selection , logistic regression models limited to a maximum of ve parameters to avoid over - tting were generated for the combined pet / mri features and for each modality separately and validated using cross validation ; no test dataset was available . 
in summary , both mriand pet - based radiomics achieve classication accuracies far above chance for differentiation of radiation injury from tumor recurrence and thus demonstrate the potential of this approach . conclusion feature - based radiomics and deep learning - based machine learning methods can be used to facilitate and automate many of the diagnostic and therapeutic steps needed in radiotherapy of malignant brain tumors with high accuracy . a common problem associated with the application of the derived models is the large variability and the lack of standardization of both image acquisition and computational methods [ 112 ]  . 
lohmann declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
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abramowitz1 alan pollack1 radka stoyanova1 received : 23 august 2019 / accepted : 10 march 2020 / published online : 27 march 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract purpose develop a deep - learning - based segmentation algorithm for prostate and its peripheral zone ( pz ) that is reliable across multiple mri vendors . methods this is a retrospective study . 
the dataset consisted of 550 mris ( siemens - 330 , general electric [ ge ] - 220 )  . a multistream 3d convolutional neural network is used for automatic segmentation of the prostate and its pz using t2 - weighted ( t2 - w ) mri . 
while the siemens model underperformed on the ge dataset and vice versa , the combined model achieved robust performance on both datasets . conclusion the proposed network has a performance comparable to the interexpert variability for segmenting the prostate and its pz . 
combining images from different mri vendors on the training of the network is of paramount importance for building a universal model for prostate and pz segmentation . keywords prostate segmentation peripheral zone deep learning convolutional neuro network introduction accurate prostate segmentation on mri datasets is required for many clinical and research applications . 
in addition , due to the different imaging properties of the peripheral ( pz ) and transition zones ( tz ) of the prostate , accurate zonal ( cid : 2 ) radka stoyanova , phd rstoyanova@med.miami.edu 1 department of radiation oncology , sylvester comprehensive cancer center , university of miami miller school of medicine , miami , fl , usa 2 university of miami miller school of medicine , miami , fl , usa segmentation is also necessary . 
in a series of applications , prostate contours are fused with ultrasound images to guide prostate biopsies . automatic segmentation of the prostate , pz and tz on mr images provides an opportunity to broaden the current scope of research by facilitating studies that include large populations of subjects or studies that incorporate serial imaging of the prostate to attain a longitudinal picture of disease progression and response . 
our group also evaluated the performance of an atlas - based approach for prostate and prostate zones segmentation using data from different mri scanstrahlenther onkol ( 2020 ) 196 : 932942 ners and acquisition parameters [ 10 ]  . 
in this work , we implement a multistream 3d u - net and analyze its performance for the automatic segmentation of the prostate and pz in a multivendor mri setting . as with our atlas - based approach [ 10 ] , the goal of the described developments was to segue towards a universal approach that can segment the prostate and prostate zones , regardless of acquisition protocols , magnetic eld strength or type of scanners . 
a core contribution is made by the preprocessing of the images in order to harmonize the data and optimize the network performance when training and testing is carried out in an image dataset from two different mri vendors . biopsy - proven prostate cancer . 
a total of 220 eligible patients with mri exams carried out on discovery mr750 3t mri ( ge , waukesha , wi , usa ) between 2012 and 2018 were identied . 
in addition , 330 mri exams , publicly available from the spie - aapm - nci prostatex challenge , acquired on two different types of siemens 3t mr scanners , the magnetom trio and skyra ( siemens , erlangen , germany ) were considered [ 16 ]  . 
all mri exams included acquisition of t2 - weighted ( t2 - w ) mri in the axial , coronal and sagittal orientations using fast spin - echo ( fse ) sequence with acquisition parameters ( for the axial orientation ) given in table 1 . 
t2 - w sequence was acquired as a part of multiparametric ( mp ) mri exam of the patients , including diffusion weighted imaging ( dwi ) and dynamiccontrast enhanced ( dce - ) mri and prior to contrast administration . 
prostate and pz were manually contoured on axial t2 - w mri in mim ( mim software inc , cleveland , oh , usa ) by imaging experts ( rs , ab , ng ) with more than 25 years combined expertise in prostate imaging . 
similarly to our previous work [ 10 ] , a crisscross design was used to evaluate the network performance : each of the three models for prostate and pz segmentation was tested on ge and siemens dataset . preprocessing of images and contours the preprocessing steps for the mris consist of bias correction using the n4itk algorithm [ 17 ]  . 
n4itk corrects for low frequency intensity nonuniformity that is present in the imaging data by least - squares b - spline data approximation . the 1 and 99% of the image intensities were normalized to an interval of [ 0 , 1 ]  . 
the proposed method estimates 2d contours in - between slices of the axial plane and computes them instrahlenther onkol ( 2020 ) 196 : 932942 dependently for every two consecutive slices . 
2 shows an example of the optical ow obtained between two horizontal slices and the resulting interpolated 3d volumes using this method . three - dimensional cnn architecture the proposed cnn consist of a 3d multistream architecture that follows the encoding and decoding path of the 3d u - net [ 20 ]  . 
the original network was modied by implementing batch normalization [ 22 ] and dropout of 20% [ 23 ] after each convolution in the decoding phase only ( due to memory constrains in the gpu used )  . the number of lters were cut from 192 to 128 in the largest convolutional layer ( after the rst concatenation ) reducing the number of parameters from to 995 k to 663 k . these changes cut the training time in half . 
all convolutional layers use a lter size of 3 3 3 and rectied linear unit ( relu ) as the activation function except the last layer which uses a lter size of 1 1 1 and sigmoid as the activation function to match the resolution of the input mri series . 
the estimated accumulated memory requirement is displayed in gigabytes ( gb ) below each layer data augmentation is performed on the y by ipping the images in the x - axis and blurring them using 3d gaussian lter randomly with 0 ( cid : 2 ) ( cid : 2 ) 3 , the size of the lter is four times  . 
each data augmentation method is applied with a random chance of  . training the selected optimization algorithm is stochastic gradient descent ( sgd ) with a learning rate = 0.001 , momentum of 0.9 and decay of 106 after conducting a hyperparameter search ( see results section )  . 
the loss function is formulated is the negative dsc [ 24 ] : loss = pi ti j = 1 j = 1 j = 1 i + " where n is the total number of voxels in the image , pi the voxel values for the prediction of the network , ti the true voxel values of the prostate or pz masks , and = 1 for all the models . 
note that the predicted probabilities , pi , are used directly in the dsc calculation ( so called soft dice ) instead of thresholding and converting them in a binary mask . for each model the data was split at random 90 : 10 for training / validation . 
training was performed on a desk936 strahlenther onkol ( 2020 ) 196 : 932942 top computer with an intel xeon ( r ) e5 - 2609 cpu and a geforce gtx 1080 ti nvidia gpu . 
the average training time for each model , independently if carried out for the prostate or the pz , is ~ 7.5 h , the overall training time for the six models is about two days . postprocessing the cnn outputs a 3d volume of the same size of the roi , in our case 1683 and each voxel gets the probability of belonging to the area of interest ( prostate or pz ) versus the background . 
to infer into the network layers , the activations maps of a single test input volume were visualized using keras and tensor flow libraries [ 27 ]  . statistical analysis the performance of each model ( three for the prostate and three for the pz ) was assessed via dsc and 95% hausdorff distances between manual and network contours . 
dscs distribution and 95% hausdorff distances in the segmented ge and siemens datasets were summarized with descriptive statistics and compared using mannwhitney u test . the dscs / 95% hausdorff distances were computed from the validation set when the model is evaluated on the same mri data , and are calculated from the whole dataset when the model is evaluated with data of a different mri scanner . 
signicance of p was determined using probability values of p < 0.005 ( to account for multiple comparisons ) from two - tailed tests . in table 1 the mri acquisition parameters for axial t2w mri are presented . 
the results ge data is more heterogeneous also in terms of acquisition parameters . the hyperparameter selection for stochastic gradient descent ( learning rate , momentum and decay ) was performed by a semi - random search on the ge training dataset . 
using 10% from the ge dataset , the performance of the hyperparameters were evaluated on two primary metrics : ( i ) the average dsc value of the network tested on the validation set at the specic epoch of 100 ; and ( ii ) the overall average dsc value of the network at the end of training . 
the values were varied semi - randomly by adding increments in the order of b * 10a with the coefcient b selected randomly from 1 to 9 and the coefcient a selected randomly from 1 to 5 for momentum and from 4 to 10 for decay , ten training runs per trial . 
after this search , with more than 50 different momentum and decay values , we determined that momentum and decay did not signicantly impact performance across the two metrics established above . 
the end result was that while network performance varied across metric ( i ) , overall dsc scores in metric ( ii ) were similar , the biggest change is visible on the time that takes the network to converge . 
5 shows the middle axial slice for the lowest , closest to mean , and highest dsc obtained for the segmentation of the pz on the siemens and ge dataset . in table 4 spearman correlations coefcients of the dcs and four acquisition parameters : pixel size , echo time , echo train length and repetition time are displayed . 
4 prostate segmentation for the cases with the lowest , closest to mean , and highest 3d dsc for the siemens ( top ) and ge ( bottom ) datasets . these segmentations are obtained with the combined network model . 
5 peripheral zone segmentation for the cases with the lowest , closest to mean , and highest 3d dice similarity coefcients ( dsc ) for the siemens ( top ) and ge ( bottom ) datasets . 
ground truth ( gt ) pz contours are displayed in red , predicted contours ( nn ) in cyan , and prostate contours in yellow examples of activation maps for different layers are shown in fig . 
some structures , such as the prostate , pelvic bone , obturator muscle can be identied across multiple views as the network has strahlenther onkol ( 2020 ) 196 : 932942 table 4 spearmans rank coefcient ( ) between the dice similarity coefcients ( dsc ) and mri acquisition parameters . 
a a single axial test input ; b activation maps at 2nd layer ( 84 84 16 ) from the axial input stream after convolution ; c activation maps at 5th convolution layer ( 42 , 42 , 128 ) after joining of the multistream network ; and d 14th ( 168 , 168 , 16 ) layer after convolution before fully connected output combined the three initial streams . 
the average dscs of all the pz models are lower than the coefcients for segmenting the prostate , which is expected as segmenting the pz is a more challenging task . 
while intuitively self - evident , this factor is often ignored in the quest for higher dsc scores . a robust performance of a segmentation with dcs in the 0.85 range may be more desirable than a dsc > 0.9 of a model trained in a homogeneous dataset . 
in the case of pz , the siemens model performs better on ge lower image resolution , which is expected as it is trained on images with lower resolution . meanwhile , the ge trained model reached a more modest dsc for ge data ( dsc ~0.88 ) but performed quite robustly on siemens data . 
as a test , we ran images at 2003 and the network segmented the data successfully ( data not shown )  . deep learning models are sometimes considered black box methods because it difcult to understand how the networks work and which features of the model have some biological meaning [ 39 ]  . 
similarly , investigating the correlations of the dsc coefcients with the image acquisition parameters ( table 4 ) contributed to the understanding of how image contrast and resolution affect the network performance . this study has some limitations . 
the siemens and ge datasets are of different sizes and splitting the datasets in training , validation and testing of the same size would possibly provide for better comparison of the models . 
while the networks were trained on a very large dataset , there is no guarantee that this dataset encompasses strahlenther onkol ( 2020 ) 196 : 932942 all possible variations related to anatomical variability between subjects , as well as variability in imaging data . the established network could be used as a basis and then ne tuned to a particular classier on top of this cnn for a new dataset [ 40 ]  . 
in addition , early stopping of the network will be evaluated on a separated dataset rather than on the training set . acknowledgements prostate mr imaging for the prostatex challenge was performed at the radboud university medical centre ( radboudumc ) in the prostate mr reference center under supervision of barentsz . 
radiomic features were extracted from 107 patients whose pre - operative mri data are available in the cancer imaging archive ; 85 and 22 of these patients were assigned to the training and testing cohort , respectively . the least absolute shrinkage and selection operator ( lasso ) was applied to select optimal radiomic features to build the radiomic signatures for extrapolating the inltration levels of immune cells in the training cohort . 
the developed radiomic signatures were examined in the testing cohort using pearsons correlation . results the inltration levels of b cells , cd4 + t cells , cd8 + t cells , macrophages , neutrophils and dendritic cells negatively correlated with overall survival in the 516 patient cohort when using univariate coxs regression . 
however , the same treatment regimens lead to variable survival in lgg patients , ranging from 1 to 15 years [ 46 ]  . brain tumours have long been regarded as an immunoprivileged sanctuary with limited inltration of peripheral immune cells . 
for example , tumour - associated macrophages ( tams ) which are recruited to the glioma tumour microenvironment ( tme ) can suppress anti - tumour immunity by releasing growth factors and cytokines . 
gliomas contain more cd8 + t cells than cd4 + t cells , and the proportion of cd8 + t cells seems to increase with the grade [ 7 ]  . 
these studies suggest that immune inltration parameters could become prognostic factors in the treatment of gliomas . as lggs are highly heterogeneous tumours , it is difcult to obtain biopsies with representative molecular information . 
radiomics has the potential to address this problem as it extracts phenotypic information by analysing quantitative features from radiological images for the whole tumour or tumour subregions [ 11 ]  . 
studies have shown that radiomic features can be used to predict the isocitrate dehydrogenase 1 and 2 ( idh1 / 2 ) mutation status [ 12 ] , egfr expression [ 13 ] and survival [ 14 ] for patients with lggs . 
recently , an eight - feature radiomic signature extracted from computed tomography ( ct ) images [ 15 ] has been reported as an indicator of tumour - inltrating cd8 + cytotoxic t cells in advanced solid tumours , which may serve as a potential imaging marker for immune - based combination therapy . 
however , so far , no radiomic studies revealing the immune environment in lggs have been reported . in this study , we estimated the levels of inltration of 6 types of immune cells , including b cells , cd8 + t cells , cd4 + t cells , neutrophils , macrophages and dendritic cells , in cohorts of lgg patients based on rna sequencing ( rna - seq ) data using tumor immune estimation resource ( timer ; [ 17 ] )  . 
in addition , we aimed to strahlenther onkol ( 2020 ) 196 : 913921 develop mri - based radiomic signatures to noninvasively extrapolate the inltration levels of these six immune cell types . patients and methods patients and rna - seq data the primary tumour rna - seq data from 516 patients with lggs were obtained from the cancer genome atlas ( tcga , cancergenome.nih.gov ) using the tcga2stat package in r software ( version 3.3.1 , org / ) , and then the inltration levels of six types of immune cells were estimated using timer [ 17 , 18 ] based on these rna - seq data . 
the values determined by timer do not exactly reect the proportion of the different immune cell subtypes ; they are estimators to compare between samples . mri - based radiomic features radiomic features extracted from preoperative mri scans of 108 patients with lggs were downloaded from the cancer imaging archive ( tcia , net ) [ 19 , 20 ]  . 
in this cohort , the preoperative mri data of patients included at least modalities of t1 - weighted precontrast ( t1 ) , t1weighted postcontrast ( t1 - gd ) , t2 - weighted precontrast ( t2 ) and t2 - weighted uid - attenuated inversion recovery ( t2 - flair )  . 
the lgg tumour subregions included the following : ( 1 ) the enhancing part of the tumour core ( et ) , ( 2 ) the nonenhancing part of the tumour core ( net ) and ( 3 ) the peritumoural oedema ( ed )  . 
in total , 724 radiomic features were extracted from manually revised labels in three - dimensional ( 3d ) space , which comprised ( i ) intensity ( n = 24 ) , ( ii ) volumetric ( n = 27 ) , ( iii ) histogram - based ( n = 120 ) and ( iv ) textural parameters , including global features ( n = 36 ) , gray - level co - occurrence matrix ( glcm , n = 108 ) , gray - level run - length matrix ( glrlm , n = 156 ) , gray - level size zone matrix ( glszm , n = 156 ) and neighbourhood gray - tone difference matrix ( ngtdm , n = 60 ) , as well as ( v ) spatial information ( n = 11 ) and ( vi ) glioma strahlenther onkol ( 2020 ) 196 : 913921 diffusion properties ( n = 26 ) extracted from glioma growth models . 
detailed information on all 724 features can be found in table 4 of the following references [ 20 , 30 ]  . further information about the collection , preprocessing and segmentation process of the mri radiomic data of this cohort is given in the following reference [ 20 ]  . among all 724 features from the tcia database , the brain volume and the features with missing data were excluded from analysis . 
thus , 256 radiomic features ( supplemental table 1 ) were considered for further feature selection analysis . patient cohort for extracting the radiomic and rnaseq data among the 516 lgg patients with rna - seq data from the primary tumours and the 108 patients with preoperative mri - based radiomic data from tcia , for 107 patients both datasets were available . 
these 107 patients with lggs were randomly separated to the training ( 80% , 85 patients ) and the testing cohorts ( 20% , 22 patients ) , and then the inltration levels of six types of immune cells were extrapolated from the radiomic features . 
we performed univariate coxs regression and multivariate coxs regression using the likelihood ratio with backward selection method to analyse the relationship between clinical features , genomic features and inltration levels of six types of immune cells and patients survival . 
of note , gender , age , karnofsky performance scale ( kps ) , histological type , who grade , whether radiation was received or not , idh status , 1p19q co - deletion status and the inltration levels by six types of immune cells ( based on timer ) were initially included in the process of variable selection in the multivariate coxs regression analysis . 
if the hazard ratio is less than 1 , then the feature is a negative prognostic factor , and if the hazard ratio is greater than 1 , then the feature is a positive prognostic factor . 
when assessing the prognostic value of the immune cell inltration levels , the inltration levels were rst dichotomized into high and low inltration levels , based on the median values . to extrapolate the inltration levels of immune cells based on radiomic features , all radiomic features were normalised using z - score normalisation before analysis . 
then , we performed the least absolute shrinkage and selection operator ( lasso ) with linear regression ( 10 - fold cross - validation ) to separately select the optimal radiomic features to estimate the inltration level of each immune cell type in lgg tumours . 
bnxn is the radiomic signature for one certain type of immune cells , a is the intercept of the radiomic signature function , x1 , x2 ... xn are the radiomic predictors , b1 , b2 ... 
by this method , most of the coefcients were reduced to zero and the remaining nonzero coefcients were selected by lasso . pearsons correlation was performed to test the relationship between the inltration levels of different cell types estimated based on radiomics and timer , respectively , in the training and the testing cohort . strahlenther onkol ( 2020 ) 196 : 913921 we applied multivariate linear regression using the likelihood ratio with forward selection method to analyse if clinical and genomic features add any predictive information to the radiomic analysis in predicting immune cell inltration . 
the strength of the relationship between the inltration level and the features ( model performance ) was evaluated by using the coefcient of determination ( denoted r squared , r2 ) and the adjusted r squared ( adjusted r2 ) , which has been adjusted for the number of predictors in the model . 
lgg lower - grade glioma , tcga the cancer genome atlas , mri magnetic resonance imaging , tcia the cancer imaging archive , timer tumor immune estimation resource , lasso least absolute shrinkage and selection operator 516 lggs with rna - seq data ( tcga ) 108 lggs with preoperative mri ( tcia ) estimation of six immune cell types by timer clinical and genomic features regression prognosis 107 lggs with both rna - seq data and preoperative mri randomly separated training cohort : 85 lggs testing cohort : 22 lggs ref . [ 20 ] downloaded mri - based radiomic features levels of six immune cell types by timer use lasso to select the optimal radiomic features to extrapolate radiomic signatures for six immune cell types lect the predictors among clinical factors , genomic features and levels of immune cell inltration , based on timer , for survival prediction . 
note that the values determined by timer do not exactly reect the proportion of the different types of immune cells ; they are estimators to compare between samples tcga database ( without missing data )  . 
age , kps and the who grade were the most important clinical features that were selected by multivariate coxs regression ( table 3 )  . the idh mutant status was also selected by multivariate coxs regression ( table 3 )  . 
the radiomic features of both training cohort and testing cohort were extracted as described in the patients 918 strahlenther onkol ( 2020 ) 196 : 913921 table 2 the role of inltration levels of immune cells estimated by timer on overall survival in the whole cohort ( 516 patients with lower - grade gliomas ) table 3 predictors for patients survival analysed by multivariate cox regression in 243 patients with lower - grade gliomas without missing data table 4 correlation coefcients and p values for the six radiomic signatures and the performance of these signatures in testing dataset cell subsets comparison univariate cox regression analysis p - value 95% ci for hr lower b cell cd4 t cell cd8 t cell macrophage neutrophil dendritic cell high vs . 
the plots showing the effect of the hyperparameter on the mean square error and the diagnostic plots of the linear regression models of these six signatures are shown in supplemental fig . 
1. evaluation of the radiomic signatures in the testing cohort when examining these six radiomic signatures in the testing cohort , the estimated inltration levels ( based on the radiomic signatures ) of four cell types ( b cells , cd8 + t cells , neutrophils and macrophages ) were signicantly correlated with those levels estimated by timer ( table 4 , pearsons correlation )  . 
interestingly , for all immune cell subtypes , the radiomic signature was still selected as a strongly predictive feature for the immune cell inltration ( see column 2 of table 5 )  . 
combining the clinical / genomic parameters with the radiomic signature only slightly improved the prediction of immune cell inltrations ( evaluated by the r2 and the adjusted r2 ) ( last 3 columns of table 5 )  . 
interestingly , we found that the idh status was signicantly negatively correlated to cd8 + t cell inltration in multivariate linear regression analysis . the who grade was not selected by multivariate analysis . 
therefore , we applied univariate linear regression for the who grade to predict the inltration levels and we found that the correlation strength between them was weak , although a higher who grade is signicantly correlated with higher inltration levels of the six types of immune cells ( supplemental table 4 )  . discussion in the present study , we established mri - based radiomic signatures to extrapolate the tumour immune inltration levels in patients with lggs . 
our study suggests that radiomics could become an efcient , noninvasive way to evaluate the immune status of patients with lggs . recent studies have revealed the crucial role of the tme for cancer patients [ 24 , 25 ]  . 
built a ct - based radiomic signature ( including eight variables ) to assess cd8 + t cell inltration determined by 920 strahlenther onkol ( 2020 ) 196 : 913921 rna - seq data [ 15 ]  . 
we used timer to estimate the inltration levels of six types of immune cells in lggs , and we applied mri - based radiomics to predict theto our knowledge , our study is the rst one that investigated the possibility of extrapolating the inltration levels of immune cells in lggs using radiomics . 
in addition , it may allow the discovery of novel predictive response biomarkers for both conventional and immune - directed therapies . notably , we found the independent , negative prognostic value of the inltration level of neutrophils by multivariate coxs regression . 
assessment of the neutrophil inltration in the tme of lggs may be very helpful for clinical decision - making and understanding the progression of lggs . the lower cd8 + t cell inltration level that we found in lggs patients with idh mutation ( table 5 ) is consistent with a previous study [ 28 ] showing that the reduced cd8 t cell inltration in idh - mutant gliomas is due to a reduced expression of the t cell - attracting chemokine cxcl10 . mri is a routine examination method for patients with lggs before , during and after therapy . 
in our study , we found that mri - based radiomic features could reveal the inltration levels of six different immune cell types in the tme of patients with lggs ( 85 patient training cohort )  . 
the inltration levels of four cell types , including b cells , cd8 + t cells , neutrophils and macrophages , could be estimated by radiomic signatures in both the training and the testing cohort . one limitation of our radiomic study is that the immune cell inltration was estimated from rna - seq data , which are available in the database only for the whole tumour and not for subregions . 
however , theoretically , one great advantage of radiomics is the analysis of tumour subregions . therefore , it would be of interest to conduct radiomic studies based on immune inltration levels for different tumour subregions . 
furthermore , all textural features were correlated to survival data to build two separate predictive models for progression - free survival ( pfs ) and disease - specic survival ( ds - os )  . 
lowand high - risk groups were identied by maximizing the separation by means of the youden method . results in the total cohort ( 77 , 75.5% , males ; and 25 , 24.5% , females ; median age 76.6 years ) , 15 patients presented nodal progression at the time of analysis ; 19 patients ( 18.6% ) died because of disease - specic causes , 25 ( 24.5% ) died from other reasons , 28 ( 27.5% ) were alive without disease , and 30 ( 29.4% ) with either local or distant progression . 
non - small cell lung cancer ( nsclc ) represents approximately 8085% of lung cancers , with 19% of cases presenting with localized early - stage disease [ 2 ]  . 
given the advancements in medical imaging and the growing adoption of screening protocols for high - risk patients , earlystage nsclc diagnoses are expected to increase in the near future [ 3 ]  . 
surgery is the standard treatment for early - stage nsclc ; however , a signicant proportion of patients are inoperable due to , e.g. , age , comorbidities , or poor respiratory reserve [ 4 ]  . 
in inoperable patients , stereotactic body radiation therapy ( sbrt ) has become the gold standard , thanks to high rates of local control , excellent tolerance , and infrequent toxicity [ 5 ]  . 
this partially explains the average 30% disease recurrence ( 10% regional , 20% distant ) that is commonly reported in sbrt series for early - stage nsclc [ 610 ]  . 
adjuvant chemotherapy after sbrt could reduce relapse rates and increase survival , although results are still unclear [ 11 ] , suggesting that the benet , if it exists , could be limited to unidentied subpopulations . 
apart from tumor size , no other parameter was identied as a possible predictor for nodal and distant relapse . the concept of radiomics , originally pioneered by lambin and aerts [ 1214 ] , has been extensively applied to the case of lung cancer . 
van timmeren [ 15 ] , in a study based on 141 patients ( and three external validation sets of 94 , 61 , and 41 patients ) with lung cancer , evaluated the change of radiomic features extracted from cone beam computed tomography ( ct ) images acquired during the radiation treatment . 
a similar investigation was carried out on combined positron emission tomography and ct ( pet / ct ) images acquired prior to and during the treatment by buizza [ 16 ] , who investigated the importance of considering features derived from successive zones , depending on the distance to the tumor border . de jong [ 17 ] studied the interoperability of radiomicbased prognostic models trained on early stages of disease when applied to advanced stages . 
although with lower performance compared to the original study for stage iiii , the performance of the model applied to stage iv resulted as positive and suggested the possibility for better prognostic assessment of patients . ramella [ 18 ] also applied radiomics as a classier tool for the selection of patients as candidates for adaptive therapy in the case of tumor reduction during treatments . 
the study was carried out on 91 advanced - stage nsclc patients and demonstrated the potential role of radiomics in the personalization of treatment care . kirienko [ 19 ] proposed predictive models based on ct , pet , or a combination of the two modalities for the prediction of disease - free survival in nsclc undergoing surgery , reporting promising results with area under the curve ( auc ) of the receiver operating characteristic curve ( roc ) of 0.75 for the ct - based signature . kirienko [ 20 ] also investigated the ability of ctor pet - based radiomics to differentiate between primary and metastatic lung lesions . 
similarly , radiomics features enabled the classication of primary tumors into the various histological subtypes . the use of ct - based radiomics for the prediction of treatment outcome in early - stage nsclc patients treated with stereotactic ablative radiotherapy was investigated by starkov [ 21 ] from high - order wavelet features . 
patients were excluded from this analysis if they had already been irradiated in the same area or if they had had other malignancies in the last 5 years before the lung cancer diagnosis . 
to homogenize and to reduce selection biases , we included in this analysis only patients treated for peripheral lesions with a total dose of 48 gy in 4 fractions . histological conrmation was obtained whenever possible ; however , radiological diagnosis was deemed acceptable in patients not suitable for biopsy . 
the retrospective study was approved by the ethical committee by written notication , and all patients signed at admission an informed consent to the use of their data for scientic scopes . 
all data were fully anonymized prior to access and use . the sbrt radiation treatment was performed by means of volumetric - modulated arc therapy in its rapidarc from ( varian medical systems , palo alto , ca , usa ) with two partial arcs with 6or 10 - mv attening lter - free photon beams . 
in particular , the dose to the ( joint ) lungs was subject to the following constraints : v5gy < 30% , v10gy < 20% , v20gy < 10% , dmean < 4 gy . patients were evaluated every 3 months for the 2 years after sbrt , every 4 months in the third year , every 6 months until 5 years , then annually thereafter . 
histological conrmation of local recurrence was required only when patients were candidates for a further local treatment ( reirradiation or salvage surgery )  . textural analysis all ct series were acquired in the same session with timeresolved scanning ( 4dct )  . 
contrast - free and with - contrast ct scans were acquired consecutively in the same imaging session and the datasets resulted automatically co - registered since shared the same dicom coordinates . 
the radiomics textural features were derived from the gross tumor volume ( gtv ) dened on the contrast - enhanced planning ct and propagated onto contrast - free ct datasets . 
the same senior radiation oncologist performed the manual segmentation of all the gtvs specically for the radiomics investigation . the entire segmentation and propagation processes were performed within the eclipse treatment planning system ( varian medical systems , palo alto , ca , usa )  . 
no inter - observer tests were performed on the segmentation , this being out of the scope of the investigation . no specic ltering or artifact correction methods were applied to the dataset . 
these included the gray - level co - occurrence matrix ( glcm ) , the neighborhood gray - level different matrix ( ngldm ) , the gray - level run length matrix ( glrlm ) , and the gray - level zone length matrix ( glzlm )  . 
from the intensity distributions , we derived : the minimum , maximum , mean , and standard deviation of the hu distribution , as well as the skewness , the kurtosis , the entropy , and the energy . 
tumor stage , sex , and age were added as covariates to the radiomics set . strahlenther onkol ( 2020 ) 196 : 922931 statistical analysis the 102 patients available for the study were randomly split into two subgroups of 70 and 32 patients ( approximately 7030% )  . 
the larger group was used for the predictive model training , the second group for the independent validation , i.e. , as required by the transparent reporting of a multivariable prediction model for individual prognosis or diagnosis ( tripod ) type - 2 study [ 25 ]  . the lymph node classier was built by means of the robust classication method of the lda with stepwise backward features elimination . 
the performance of the model was assessed by means of the area under the curve ( auc ) of the receiver operating characteristic ( roc ) and standard metrics derived from the confusion matrix ( sensitivity , specicity , and accuracy )  . the outcome predictive models ( using one single random split ) were built with the same logic for the two survival classes . 
the subclass of signicant ones at univariate cox regression ( done on the training set only , and with correction for multiple testing with a false discovery rate tolerance of 0.2 ) were further reduced to a minimal set with elastic net regularization . this process aims to identify the most signicant independent covariates [ 26 ]  . 
for each residual feature , the concordance index was used to measure their predictive performance and was computed with repeated cross validation . these features were then used to train a multivariate cox model and the ones kept in the model after backward selection , with minimization of the akaike information criterion ( aic ) , were dened as the nal radiomics signature . 
the predictive model was used to identify the highand lowrisk groups of patients with the best separating threshold set according to the youden method [ 27 ]  . the models were then tested against the validation group . the entire process was , as mentioned , repeated for the pfs and ds - os analyses . a signature interoperability test was performed to investigate the correlation between the radiomic signatures and the outcome metrics . 
in practice , both ds - os and pfs were also studied by applying the signature from the other ( i.e. , ds - os with the signature from pfs and vice versa )  . this test aimed to determine if metric - specic signatures are needed or if it would be possible to use single signatures for all metrics given the possible correlation between os and pfs . the entire statistical analysis was carried out using the open source r platform ( version 3.5 ) [ 28 ]  . table 1 descriptive statistics for the training and validation subgroups . 
the accuracy exceeded 85% for both the training and the validation cohort ; auc was 0.84 for the training and 0.73 for the validation group , respectively ( table 2 )  . table 3 presents the list of features concurring to dene the radiomics signature for the ds - os and pfs prediction surviving the univariate and elastic net selection and the multivariate cox regression , as well as the normalized coefcients to calculate the radiomics score . 
the median , mean , and 95% condence interval for the ds - os and pfs actuarial analyses are reported in table 4 for the whole group and for the highand low - risk subgroups . 
no statistical signicance was found in survival between the training and validation sets ( panels a and d ) , while a signicant difference was found between the stratied subgroups for both ds - os and pfs , conrming the predictive value inferred from the concordance index ndings . 
in particular , for pfs , all features presented a lower mean value in the low - risk compared to the high - risk group , while for the os , this was observed for the short run low grey emphasis from the glrlm matrix ( glrlm_srlge )  . 
identifying predictive biomarkers for nodal and distant relapse in early - stage nsclc could ll the gap between standard surgical intervention and sbrt , maintaining the advantages of the latter treatment in terms of limited invasiveness and toxicity . 
using these biomarkers in the setting of a multidisciplinary tumor board , the risk of occult nodal disease could be weighted and drive the nal decision towards surgery or sbrt . 
in another scenario , using radiomic signatures predicting a poorer prognosis , patients could be candidates for further adjuvant therapies , like chemotherapy , immunotherapy , or targeted therapy . with a relatively small cohort of patients ( 102 ) , and about 25% cases of progression ( nodal or distant ) and about 19% disease - specic deaths , it was possible to utilize radiomics features to discriminate patients at risk of progression or treatment failure and develop predictive models . three specic signatures and models were identied and trained for each endpoint ( the classier for risk of progression and the predictive models for os and pfs )  . 
from a conceptual point of view , this is the approach which should lead to better results , but it is not strictly mandatory . to validate the possibility of applying simpler approaches , i.e. , using one signature for multiple endpoints , we applied an interoperability test . 
the area under the curve ( auc ) resulted as being comparable for both the os and pfs models and the discrepancy between training and validation is compatible within 1 standard deviation the use of crossed radiomic signatures resulted , as shown in fig . 
2 ( panels c and f ) , in predictions and stratications similar to those achieved when the specic signatures were used in the models ( panels b and e )  . 
2 kaplanmaier curves for the training and validation ( validat ) groups for the pfs and ds - os cohorts of patients ( panels a and d ) and for the lowand high - risk stratication from the predictive models from the radiomic signatures ( panels b and e )  . 
panels c and f show the pfs and ds - os curves obtained from the interoperability tests ( i.e. , applying the pfs radiomic signature to os and vice versa )  . 
no statistical difference was observed for os and pfs in the unstratied analysis groups was slightly inferior when swapped signatures were used . the limited number of patients in the study is acknowledged as one of the limitations of this pilot investigation , as suggested , e.g. , by the relatively large uncertainty in the performance metrics for the lda classier . 
this might be due to some sensitivity to the random selection of the groups . the main reason is identied in the relatively low number of nodal progressions , which might end up in undersampled progression cases in the training . 
for example , the investigation from huang [ 29 ] was conducted on 282 consecutive patients and identied a radiomics signature signicant for the estimation of disease - free survival . 
the data from the present study are also limited by the single - institute nature of the collection and therefore should be validated with independent external sets ( as required by tripod type - 3 studies [ 25 ] ) with the caveats deriving from this . 
the authors , using datasets from four different institutes collecting 138 patients in total , observed that the individual cohorts differed substantially in the patient characteristics and possibly inconsistent imaging parameters . 
recently , yu [ 31 ] performed a retrospective study using 147 training patients ( treated with surgery ) and an independent validation cohort of 295 patients treated with stereotactic therapy and demonstrated that a model based on kurtosis and homogeneity radiomics features allowed for signicant risk stratication for overall survival . 
the same model also resulted as signicant for distant metastasis and borderline for regional recurrence . this suggests the possibility of avoiding the denition of specic predictive models for each endpoint and the possibility of using a single model for multiple predictions . in general , one of the additional challenges in radiomics is the difculty of identifying features stable and signicant across the similar studies . 
our study was also somehow affected by this issue , since the two signatures prognostic for os and pfs were different , and only one textural feature was present in both cases . 
the short - run low grey - level emphasis is a measure of the distribution of short homogeneous sequences with low grey levels ( and it is computed as an average over the 13 different directions in a 3d space )  . 
this metric increases when the texture is dominated by many short runs ( sequences ) of low grey values ( higher values indicates ner textures )  . this nding is consistent with that reported by huynh [ 22 ] , where the same feature was correlated to overall survival , suggesting the possibility of building models with good generalization power if enough data from more institutes would be used for the model training . 
looking in more detail at the interpretation of the features in the signature from this study , in general , all were suggestive of higher heterogeneity of the tumor tissue in the high - risk group . 
in fact , for pfs , the ngldm_coarseness measures the spatial rate of change in intensity and the glrlm_lgre measures the distribution of the low grey - level runs similarly to the glzlm_lgze which applies to the zones ( a 2d extension of a mono - dimensional run )  . 
in the case of os , the shape_compacity ( the degree to which the region analyzed is compact ) and the glcm_homogeneity ( the homogeneity of the grey - level voxel pairs ) while the glzlm_zlnu which measures the nonuniformity of the grey levels in the homogeneous zones . 
for all the features , the ndings in terms of mean values and distribution point to the fact that the high - risk class of patients presented with increased tissue heterogeneity and shape irregularity , while the low - risk patients had ( on average ) less pronounced ne textural patterns . 
another indirect conrmation derives from another investigation from our institution [ 26 ] , where coarseness and compacity appeared in the signature for os or pfs in head and neck cancer patients . concerning the methods of analysis and the choice of features , this study was inspired by the principles of simplicity already detailed in [ 20 , 26 ]  . 
in practice , only intensity and unltered features were investigated , and the feature selection was performed by means of sequential univariate analysis , elastic net regularization , and multivariate cox regression . 
it might be of course reasonable to include higher - order features if this would improve the models , and we acknowledge this as another potential limitation of this study . the youden best - cut threshold methods [ 27 ] was applied in the stratication of the lowand high - risk subgroups and applied also by other groups [ 32 ]  . 
this method aims to maximize the separation between the groups but is exposed to the risk of unbalanced populations among the classes , a factor of greater importance when the samples are small . we recognize this as a potential limitation of our investigation , although none of the resulting groups were not extremely underpopulated , especially in the validation group . an alternative , more conservative , method would consist of splitting the subgroups according to the median of the prediction [ 26 ]  . 930 strahlenther onkol ( 2020 ) 196 : 922931 thawani published a comprehensive review of the radiomics investigations in lung cancer [ 33 ] and outlined some of the main current limitations : lack of standardization of the acquisition parameters , inconsistent radiomic methods , and lack of reproducibility . in particular , the stability of the features in the thoracic region , where breathing is a factor of concern , should be investigated with care . 
larue [ 34 ] showed that 4dct images ( from eight breathing phases ) could be used to assess the stability of the radiomics features in the thoracic region and concluded that unltered features resulted as being more stable than wavelet - based features . in our study , the selection of only phase 0 , the beginning of the inspiration cycle , aimed to standardize and increase the robustness of the features , since this phase should be more consistent among patients . still , in terms of stability of the features , the segmentation of the region of interest is another major issue . 
no specic pre - processing or artefact corrections were applied to the images ( mitigated by the 4dct acquisition methodology )  . conclusion radiomics analysis , based on planning ct images , allowed a classier and predictive models capable of identifying patients at risk of nodal relapse and at a high risk of a bad prognosis to be built . 
juni 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund die entwicklungen sowie die verfgbarkeit von untersuchungen im bereich der molekularen bildgebung erffnen nicht nur in der diagnostik , sondern auch in der therapie von onkologischen erkrankungen neue mglichkeiten . 
ziel der pet - plan - studie von nestle et al . [ 1 ] war es , erstmals zu prfen , ob eine reduktion des zielvolumens ( zv ) mit untersttzung einer 18f - fluordeoxyglukose ( 18f - fdg ) - pet - bildgebung machbar und zuverlssig ist im vergleich mit einer konventionell geplanten radiochemotherapie ( rct ) des fortgeschrittenen nichtkleinzelligen bronchialkarzinoms ( nsclc ) inklusive einer elektiven lymphknotenbestrahlung . patienten und methoden die prospektive , randomisierte und multizentrische studie pet - plan ( aro - 2009 - 09 ) rekrutierte an 24 deutschen , sterreichischen und schweizer kliniken zwischen 2009 und 2016 insgesamt 311 noch nicht behandelte patienten > 18 jahre mit einem inoperablen , lokal fortgeschrittenen nsclc , bei denen eine rct indiziert war ( ecog - status < 3 )  . 
es wurden 205 / 311 patienten zur zv - denition 1 : 1 auf 2 gruppen randomisiert : originalpublikation nestle u , schimek - jasch t , kremp st et al ( 2020 ) imaging - based target volume reduction in chemoradiotherapy for locally advanced non - small - cell lung cancer ( pet - plan ) : a multicentre , open - label , randomised , controlled trial . 
primrer endpunkt war die zeit bis zum lokoregionren progress ab randomisierung in der annahme , dass die 18f - fdg - pet - basierte planung der konventionellen planung nicht unterlegen ist . das kollektiv , bei dem die vorgehensweise per protokoll erfolgte , wurde in die primranalyse aufgenommen . 
das safety - kollektiv enthielt alle patienten , die irgendeine studienspezische behandlung erhielten . ergebnisse es wurden 205 von 311 patienten auf die conventional target group ( n = 99 ) und die 18f - fdg petbased target group ( n = 106 ; die intention to treat group ) randomisiert . 
damit war die lokoregionre progressionsrate in der experimentellen gruppe um fast die hlfte niedriger als in der conventional target group . die hugsten nebenwirkungen mit einem grad 3 waren die sophagitis bzw . 
dabei kann eine 18f - fdg - pet - basierte volumenreduktion der zielvolumina im sinne einer involved eld radiation therapy ( ifrt ) die lokale kontrolle verbessern , ohne die toxizitt zu erhhen . 
die in der pet - plan - studie denierte , volumenreduzierte konturierung knnte damit der neue standard of care ( therapiestandard ) bei der rct des fortgeschrittenen nsclc werden . kommentar die im lancet oncology publizierte studie von nestle et al . [ 1 ] zeigte , dass mit einer 18f - fdg - pet - basierten konturierung und zielvolumendenition eine volumenreduktion ohne unterlegenheit bei der lokoregionren kontrolle im vergleich zu einer grovolumigeren , elektiven lymphknotenbestrahlung ( enrt ) mglich ist . 
selbst dann , wenn es formal wegen des nichtunterlegenheitdesigns nicht angebracht ist , eine berlegenheit der volumenreduzierten 18f - fdg - pet - planung zu zeigen , ist diese studie doch als practice conrming fr die ifrt anzusehen [ 2 , 3 ]  . bisherige studien zeigten bereits , dass die ifrt bei der elektiven nodalen bestrahlung beim nsclc bevorzugt werden sollte , da mit der ifrt vermutlich kein erhhtes risiko fr einen lokalen relaps besteht , aber das risiko fr therapieassoziierte nebenwirkungen reduziert werden kann [ 46 ]  . 
die pet - plan - studie ist nun die erste ihrer art , die eine 18f - fdg - basierte volumenreduktion im randomisierten setting evaluierte und eine nichtunterlegenheit im vergleich zu einer konventionellen ifrt zeigen konnte . 
variationen bei den bildparametern knnten ansonsten bei verschiedenen semiautomatisierten verfahren und auch bei der manuellen konturierung zu einer abweichung von > 50 % fhren [ 9 ]  . vorangegangene dosiseskalationsversuche , wie beispielsweise in der rtog 0617 - studie , bei der eine simultane , dosiseskalierte rct bis 74 gy durchgefhrt worden war , verbesserten das outcome nicht [ 10 ]  . 
zu bercksichtigen ist dabei , dass in rtog 0617 ein xes dosiskonzept vorgegeben war , wohingegen in der pet - plan - studie eine schrittweise und isotoxische dosierung angewendet wurde . dieses vorgehen ermglichte eine studienspezische , aber dennoch patientenspezisch - individualisierte dosiseskalation . 
dies fhrte zu einer etwas breiteren und moderateren dosisverteilung als beispielsweise in der rtog 0617studie , was deren negativen ergebnisse erklren knnte im vergleich zur pet - plan - studie . 
in letzterer wurde auch keine erhhte toxizitt durch die moderate dosiseskalation beobachtet , was durch die isotoxische radiotherapieplanung , aber auch die geringeren zielvolumina in der experimentellen gruppe zu erklren ist . 
eine krzlich verffentlichte gepoolte , retrospektive analyse aus 16 studien untermauerte diese erfahrung ; die ifrt war mit einer signikant geringen rate an grad - 3 - nebenwirkungen verbunden und zeigte bei einer dosierung von 60 gy auch ein verbessertes outcome im vergleich zur enrt oder hheren dosiskonzepten ( > 60 gy ; [ 11 ] )  . 
zusammengenommen verdeutlichen diese ergebnisse , wie relevant die normalgewebsbelastung in der behandlung thorakaler tumoren fr das berleben ist und dass eine dosiseskalation nur dann sinn macht , wenn dies nicht mit einer erhhung der toxizitt einhergeht , die offenbar empndlich das outcome beeintrchtigt . 
die post - hoc - analyse zeigte die anzahl der im 18f - fdg - pet / ct befallenen lymphknotenstationen als einen unabhngigen prognosefaktor fr das berleben , was sich allerdings nicht auf das jeweilige nodale stadium bertragen lie . strahlenther onkol ( 2020 ) 196 : 743746 die ergebnisse der bereits 2009 initiierten pet - planstudie fallen nun in die ra der immuntherapie , die seit der verffentlichung der pacific - studie [ 13 ] ein fester bestandteil der primrtherapie des nsclc geworden ist . prklinische wie klinische studien konnten zeigen , dass der antitumorse effekt der immuntherapie durch eine lokaltherapie , wie es die bestrahlung ist , noch verbessert werden kann [ 14 ]  . 
neben den direkt zytotoxischen effekten der rt knnen zustzlich auch eine reihe weiterer mechanismen das tumormilieu verndern [ 15 ] , und es knnen sich synergistische effekte ergeben bei der kombination von rt und immuntherapie [ 16 ] , die sogar ber lokale effekte hinausgehen , sog . 
es besteht aber unklarheit ber die optimale dosierung , fraktionierung und sequenz der therapien , wobei die rt sowohl immunstimulatorisch als auch immunsuppressiv wirken kann . auch in der pet - plan - studie muss sich die verbesserte lokale kontrolle nicht alleine mit der moderat hheren dosis in der experimentellen gruppe erklren lassen . 
eine experimentelle studie zeigte bereits am mausmodell , dass die bestrahlung des lymphabusses die induktion von cd8 - t - zell - vermittelter immunantwort in der kombination mit checkpointinhibitoren verhindert . 
die enrt kann also durch die grochige bestrahlung des lymphabusses zu einer immunsuppression fhren , was wiederum zu einer vernderten zytokinexpression und verminderten cd8 - t - zell - funktion fhrt . 
die pet - plan - studie lieferte damit bereits indirekt antworten auf fragen , die es bei der konzeption der studie noch nicht gab . fazit die pet - plan - studie zeigt , dass die ifrt auf der basis der 18f - fdg - pet mglich und sicher ist , bei daraus resultierender reduktion der zielvolumina und ggf . 
in der ra der immuntherapie wird ein neuer standard gesetzt , wobei sich das volle aussa der vorteile dieses vorgehens erst in zuknftigen studien zeigen wird . denise bernhardt und stephanie e . 
nestle u et al ( 2020 ) articles imaging - based target volume reduction in chemoradiotherapy for locally advanced non - small - cell lung cancer ( pet - plan ) : a multicentre , open - label , randomised , controlled trial . 
de ruysscher d et al ( 2017 ) european organization for research and treatment of cancer ( eortc ) recommendations for planning and delivery of high - dose , high precision radiotherapy for lung cancer . 
fleckenstein j , kremp k , kremp s , palm j , rbe c ( 2015 ) imrt and 3d conformal radiotherapy with or without elective nodal irradiation in locally advanced nsclc : a direct comparison of petbased treatment planning . 
sulman ep , komaki r , klopp ah , cox jd , chang jy ( 2009 ) exclusion of elective nodal irradiation is associated with minimal elective nodal failure in non - small cell lung cancer . 
li r et al ( 2016 ) involved eld radiotherapy ( ifrt ) versus elective nodal irradiation ( eni ) for locally advanced non - small cell lung cancer : a meta - analysis of incidence of elective nodal failure ( enf )  . radiat oncol 11 : 124 7 . 
schimek - jasch t et al ( 2015 ) verbesserung der zielvolumendenition durch einen dummy run mit interventionellem konturierungstraining beim lokal fortgeschrittenen nicht - kleinzelligen lungenkarzinom : reduktion der interobserver - variabilitt in klinischen multizenterstudien . 
bradley jd et al ( 2015 ) standard - dose versus high - dose conformal radiotherapy with concurrent and consolidation carboplatin plus paclitaxel with or without cetuximab for patients with stage iiia or iiib non - small - cell lung cancer ( rtog 0617 ) : a randomised , twoby - two factorial phase 3 study . 
schild se et al ( 2019 ) toxicity related to radiotherapy dose and targeting strategy : a pooled analysis of cooperative group trials of combined modality therapy for locally advanced nonsmall cell lung cancer . 
theelen ws , de jong mc , baas p ( 2020 ) synergizing systemic responses by combining immunotherapy with radiotherapy in metastatic non - small cell lung cancer : the potential of the abscopal effect . 
golden eb , demaria s , schiff pb , chachoua a , formenti sc ( 2013 ) an abscopal response to radiation and ipilimumab in a patient with metastatic non - small cell lung cancer . 
krug8 received : 21 january 2020 / accepted : 15 april 2020 / published online : 4 may 2020 the author ( s ) 2020 abstract purpose medical students knowledge of radiation oncology ( ro ) is of increasing importance with a rising prevalence of malignancies . 
however , ro teaching in medical schools is heterogeneous and has not been analyzed at a federal level yet . therefore , the following survey aims to provide a national overview of ro teaching in germany . methods a questionnaire containing multiple - choice and free - text questions covering the extent and topics of ro teaching was sent to ro departments of all university hospitals in germany and was answered by the heads of department / main lecturers . results 24 / 35 ( 68.6% ) ro departments returned completed forms . 
notably , all departments offered at least a partial rotation in ro in conjunction with radiology and / or nuclear medicine departments in the last year of medical school , while only 70.8% provided a complete rotation in ro . 
with around 50% of oncological patients having an indication for radiation therapy ( rt ) during their course of disease [ 2 , 3 ] , knowledge of radiation oncology ( ro ) has cardinal importance for both oncological disciplines as well as for general practitioners to provide patients with adequate counsel . 
however , there are common misbeliefs about ro and its treatment spectrum , which persist until the end of medical school [ 4 ] , demanding an improvement in teaching . 
innovative concepts such as internships or interdisciplinary classes could be of additional value [ 4 , 5 ] , but are not obligatory across germany . at the same time , the introduction of the new german national competence - based learning objectives catalogue ( nklm ) [ 6 ] calls for interdisciplinary and practice - orientated teaching formats . 
despite the need for reformed and innovative teaching , a survey by a working group of the german society of ro ( young degro ) revealed that only around 20% of young radiation oncologists are able to perform teaching activities within the regular working hours [ 7 ]  . 
the obvious discrepancy between the demand for restructured curricula and the uncertainties concerning formal requirements prompted our working group to perform a survey on the current situation of ro teaching in germany . the aim of this study is to describe the state - of - the - art of ro medical education in germany , to identify potential elds of further development , and to delineate future challenges ahead . strahlenther onkol ( 2020 ) 196 : 699704 materials and methods a detailed questionnaire assessing extent and topics of ro teaching was designed by the working group of the german society for ro ( young degro ) in a peer - review process . the questionnaire contained both open and multiple - choice questions and was sent in written form and / or electronically to all academic ro departments at university hospitals in germany ( see supplementary 1 for full questionnaire )  . 
the main topics covered in ro teaching are general ro ( 100% ) , radiation biology ( 91.7% ) , side effects ( 87.5% ) , and radiation physics fig . 
concerning the different organ systems , gynecological ( 87.5% ) , urogenital ( 79.2% ) , gastrointestinal ( 75% ) , head and neck , and lung tumors ( 70.8% each , respectively ) ranked highest . 
there is a possibility for an internship during the nal practical year in ro at all faculties , but only 70.8% offer a complete rotation ( 4 months )  . elective teaching courses are offered at 75% of faculties covering additional subjects of ro . 
some medical faculties perform seminars and lectures in one semester only or have no obligatory lecture at all , whereas others have developed extensive curricula with representation of ro in all clinical semesters . consequently , the spectrum of topics differs greatly . whereas ro in general / introductory lectures are always held , only 70% of curricula include lung , head and neck , or imaging in radiation oncology . 
it is particularly striking that only 1 / 3 of medical faculties include benign diseases in their curricula . interestingly , a comparable survey in 19 european countries , involving 32 academic institutions , showed a similar thematic selection with large heterogeneities in teaching extent ( 260 h of ro teaching ) , the responding german institution being in the lower third [ 9 ]  . 
another analysis conducted in australia and new zealand unveiled a worse situation , with at least 50% of faculties , including 81% of students , not receiving training in basic principles of ro [ 10 ]  . 
in summary , this minor role in the current curriculum does not adequately reect the cardinal importance of the eld in oncological patient care . a disparity in knowledge of different entities persists even in ro residency , as displayed by a survey of the young degro [ 11 ]  . 
the implication may be discussed controversially : regarding the fact that many medical students will not choose oncological residencies , haagedorn and de vries argued for a change in teaching practice addressing the general practitioners need for basic oncology education rather than focusing on details of biology and treatment [ 12 ]  . what is the amount of ro teaching that is essential for every medical student ? which tumor entities should be mandatorily included in the curriculum of medical schools ? these questions , amongst others , remain debatable and are currently being discussed by a new working group of the degro ( see below )  . 
it can be summarized that there is increasing consensus that a basic ro education for medical students should at least comprise the main oncological entities ( breast , prostate , lung , head and neck , metastases in different locations ... ) in germany , as indicated by the cancer report of the robert koch institute [ 1 ]  . 
moreover , it is our strong belief that practical training in oncological anamnesis , empathic counseling and guidance , and focused physical examination should be integrated . in contrast to the vivid discussions on the overall scope of basic ro education during medical school , the teaching of ro techniques and concepts appears homogenous , with all faculties imparting the principles of modern image - guided and intensity - modulated rt . 
only a minority of medical schools in germany ( < 30% ) present particle therapy or heavy - ion therapy , which may be due to the limited distribution of the respective treatment facilities . the abovementioned heterogeneity may be attributed to the different concepts of medical education . 
while the regular course teaches ro within the module imaging procedures , radiation treatment , and radiation protection together with radiology and nuclear medicine , the reformed or model curriculum ( e.g. , model curricula in aachen , berlin , hannover , and heidelberg and reformed curricula in cologne and muenster ) aims at a concept - based education . 
accordingly , organ - specic modules are established in which interconnectivity between the oncological disciplines takes center stage . these challenges are being met by the degro by the formation of a new working group focusing on the redefinition of learning objectives and key abilities in light of the new masterplan medizinstudium 2020 . 
additionally , a reciprocal dialogue between ro and other disciplines , like surgery and internal medicine et cetera , will ultimately lead to a new interdisciplinary clinical schedule , strengthening cardinal aspects of ro . the survey is restricted due to the rate of incomplete responses ( 2 / 3 responders ) , with a possible selection bias , as faculties more involved in teaching might have been more responsive to the survey . 
furthermore , the evaluation and opinions offered for this survey may not represent a consensus of the whole teaching staff at the respective sites , as the survey was sent to the heads of the departments . 
thus , the survey has to be seen as a punctual observation , which nevertheless may give suggestions for further improvements of ro teaching and implementation of new teaching concepts . recently , the german government introduced the masterplan medizinstudium 2020 , summarizing a package of measures for structural reorganization [ 14 ]  . 
its main goals include the vertical integration between clinical and undergraduate subjects , the deepening and consolidation of scientic knowledge , as well as the introduction of competence - based learning [ 14 ]  . 
therefore , it corresponds with global trends towards competence - based medical education in accordance with todays medical students desire for personalized , interconnected , and team - based learning [ 15 , 16 ]  . the formal requirements , as listed in the nklm [ 6 ] , call upon medical faculties and their teaching staff ( esstrahlenther onkol ( 2020 ) 196 : 699704 pecially habilitated members ) to thoroughly review their timetables , i.e. , to change learning objectives from pure knowledge acquisition to practical application . 
additionally , interdisciplinary formats , which cover different subjects and at the same time bridge clinical and undergraduate education , may gain even more importance in the future by providing an introductory multimodal overview [ 1618 ]  . 
a recently published example is the course anatomy and imaging at the university of muenster transferring anatomy knowledge to its clinical application , like in ro [ 5 , 20 , 21 ]  . the strategy of early integration of ro teaching may also be suitable to avoid misbeliefs in ro . 
a multi - institutional survey in the us showed deciencies in knowledge concerning ro indications , toxicity , and techniques affecting rst - year and fourth - year medical students [ 4 ]  . an ro rotation could improve responses in all categories [ 4 ]  . 
it is noteworthy that structured didactic sessions for clerkships could improve both students knowledge and interest in the eld , but also lead to better evaluation results [ 2225 ] , and should therefore be considered for the ro rotations in germany . future efforts of the ro community should focus on an appropriate as well as interesting presentation of the discipline to medical students to avoid misconceptions , but also to attract potential ro residents . 
corresponding to this , free - text comments within the current analysis revealed a spectrum of elective teaching formats offered to interested students , covering palliative care , pediatric radiation oncology , neuro - oncology , and more . 
this demonstrates the creativity of the ro teaching community in germany as well as the vivid interest in implementing state - of - the - art teaching formats . conclusion the current survey displays heterogenous curricula across germany and emphasizes the need for a shift towards interdisciplinary and competence - based teaching formats . 
krug has received honoraria from merck sharp & dome , outside of the submitted work . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
the aim of this study was to investigate the outcome of radiation therapy in a group of so - called oldest old cancer patients ( 85 years )  . materials and methods we retrospectively reviewed data from patients aged 85 years , treated between 2010 and 2015 for any tumor histology at the university hospital zurich , switzerland . 
overall survival ( os ) , relapse - free survival ( rfs ) , performance status ( ecog ) , charlson comorbidity index ( cci ) and treatment tolerance were assessed . results we identied and included 100 patients with a mean age of 88 years ( range : 85102 years )  . 
the charlson comorbidity index ( cci ) had a predictive value for overall survival ( cci > 10 , p = 0.0001 ) in the curative group . conclusion the number of older cancer patients will increase considerably in the next decades because of demographic changes . 
the 684 strahlenther onkol ( 2020 ) 196 : 683690 national institute on aging and the national institute of health ( nih ) dene three categories of patients according to chronological age : young old ( 6574 years ) , older old ( 7585 years ) , and oldest old ( 85 years ) [ 4 ]  . 
nevertheless most studies used an age threshold of 70 years and the group of oldest old was underrepresented . age - specic differences in the tolerability of different organs are known . 
several eortc trials have shown that elderly patients undergoing radiation therapy in the head and neck region experience more acute toxicity such as mucositis and weight loss , and have more long - term side effects after esophageal and thoracic radiation compared to younger patients [ 6 ]  . 
other studies , however , showed that treatment tolerance in head and neck patients aged > 80 years is high and comparable to that of younger patients when modern radiotherapy techniques such as volumetric modulated arc therapy ( vmat ) are used [ 7 ]  . 
data are even more scarce for the group of oldest old cancer patients . herein , we aim to evaluate our institutional experience within the group of oldest old patients receiving radiation as part of their cancer treatment by assessing treatment and patient - specic parameters , toxicities , and oncological outcome . survival or date of death was collected by contacting the currently treating physicians . 
the treatment plans were all calculated in the varian treatment planning system eclipse ( external beam planning system , varian medical systems , palo alto , ca , usa )  . 
various irradiation techniques and energies were used , such as 3d - conformal irradiation technique , intensity - modulated radiation therapy ( imrt ) , and volumetric modulated arc therapy ( vmat ) , with energies of 612 mv . 
the applied mean dose was 55 gy ( median : 55.6 gy ; range 2470 gy ) in the group of curatively treated patients , with indications ranging from involved - site radiotherapy for non - hodgkin lymphoma with 24 gy to a curative - intent primary radiotherapy in head and neck cancer ( table 1 )  . 
the reason for not completing radiotherapy was a decline in general health status , which was related to tumor progression in two patients and patients wish in the other two cases . most patients experienced low - grade acute toxicity grade iii ( table 2 and 3 )  . 
the most common dose regimen was 20 gy in 5 fractions ( 25% ) followed by 30 gy in 10 fractions ( 19.4% ) , or 8 gy single fractionation dose , but also prolonged schemes such as 15 3 gy were used . 
in the palliative group one patient did not nish radiotherapy and stopped after a single fraction of 3 gy because of pain and subsequent impossibility of positioning during the treatment . comorbidities the most common comorbidities were cardiovascular diseases ( 20% ) , followed by chronic kidney disease ( 15% ) , peripheral arterial disease ( 11% ) , and diabetes without endorgan damage ( 9% )  . 
an important bias could be the difculty to access a radiotherapy unit for patients who live in more rural regions , which is especially relevant for older patients with reduced mobility . 
also , different so100% strahlenther onkol ( 2020 ) 196 : 683690 table 3 late toxicity for the curative group late toxicity grade 0 grade i grade ii grade iii grade iv 63 ( 98.4% ) 62 ( 96.9% ) 63 ( 98.4% ) 61 ( 95.3% ) 61 ( 95.3% ) 1 ( 1.6% ) 2 ( 3.1% ) 1 ( 1.6% ) 3 ( 6.1% ) 2 ( 3.1% ) 1 ( 1.6% ) curative , n telangiectasia xerostomia fatigue dyspnea , cough , pneumonitis other ( e.g. , xed glottis , lymphedema ) fig . 
2 kaplan meier curve for correlation between overall survival ( os ) and charlson comorbidity index ( cci ) p = 0.00012 cci > 10 cci <= 10 time [ months ] number at risk cci > 10 cci <= 10 time [ months ] cial aspects might inuence the primary decision to seek information on radiation options , including the availability of family members who are taking care and escorting patients to treatments and consultations . 
finally , the primary physician might be reluctant to refer patients of this age group to high - care treatments and rather opt towards a more supportive treatment path , simply based on old age . treatment strategies were adapted to this vulnerable patient cohort : only three patients received concomitant chemotherapy and no trimodal therapy was administered , i.e. , administration of radiotherapy , chemotherapy , and surgery . 
in our interpretation , overall survival rates were high in both groups in consideration of the mean age of 88 years and it underlines once more the patient selection bias . 
a pragmatic and helpful approach could be a score for identifying patients at risk that does not only focus on overall survival as an endpoint , but a more patient - centered endpoint like hospitalization rates and quality of life . 
this has been done with the qtwist ( qualityadjusted time without symptoms of disease progression or toxicity of treatment ) , rst proposed by gelber and goldhirsch in 1986 , which includes the time without toxicity or progression and therefore focusses on quality of life [ 18 ]  . 
this is most likely explained by the small patient number in our cohort . reection on comorbidities is easily done and should be performed in clinically routine , possibly through electronic tools [ 23 ]  . furthermore , comorbidities have a higher prevalence in aged patients , predisposing them to less tolerance to a curative treatment . 
especially in geriatric patients , in addition to functional status , it is of immense importance to consider development of dementia or depression , social status , degree of mobility , nutritional status , and comorbidities . helpful tools are geriatric assessments , such as the comprehensive geriatric assessment ( cga ) [ 24 ]  . 
recommended are performance of the instrumental activities of daily living ( idl ) and g8 questionnaires , cci , and registration of the social situation [ 17 , 26 ]  . for a systematic evaluation of the elderly data and additional knowledge a geriatric assessment ( ga ) is appropiate . 
there are some data that show an improved outcome when a ga is used . the ga detects additional decits that would otherwise be misunderstood , such as fatigue , nutritional decits , and cognitive decits [ 27 ]  . 
in addition , in some cancers there is a correlation between assessment outcome and the occurrence of severe toxicities ( grade 3 / 4 ) and overall survival of older cancer patients . 
results from a randomized trial conducted in lung cancer showed that treatment selection based on a comprehensive geriatric assessment ( cga ) signicantly reduced toxicity [ 28 ] , although this study failed the primary endpoint of improvement of treatment failurefree survival . 
in our retrospective analysis , ga was not available for the entire patient cohort . it should be noted at this point that there is still little prospective data on this topic . we have to admit typical limitations , which are often recorded in retrospective studies analyses in dependence of recordkeeping . 
finally , we cannot retrospectively conclude that patients were referred for radiation treatment and excluded due to their general condition , inducing a bias in this population . in conclusion , radiotherapy can be applied safely and efciently in the oldest old patients as a therapeutic option in either a curative or palliative oncological setting and should be discussed in interdisciplinary tumor boards as a valid option . 
guckenberger declare to have no competing interests . 690 happy birthday , klaus - rdiger ! heartfelt appreciation on the occasion of the 80th birthday of professor klaus - rdiger trott strahlenther onkol ( 2020 ) 196 : 747748 laudatio stephanie e . 
an empathic and supremely supportive teacher , a dedicated historian , theater and opera acionado , caring spouse , and tireless discussant ! professor klaus - rdiger trott will reach a milestone in july 2020his 80th birthday . 
his engine still runs on high energy , with no compromise . when klaus - rdiger went to medical school in munich , he was almost immediately drawn to radiation sciences . this led him in the late sixties to the radiation biology lab of otto hug at the ludwigs - maximilians university ( lmu ) in munich and the newly formed institute of biology at the gesellschaft fr strahlenforschung ( gsf ) in neuherberg , which is now the zentrum fr gesundheit und umwelt ( hmgu )  . 
a characteristic of this early era was his willingness to revolutionize knowledge in the eld by challenging almost every preconceived notion by looking at problems from the clinical and biological perspective . 
in reality , he was a serious and signicant contributor to developing the policy for deep storage of nuclear waste , a concept that fell out of favor at the end of the century , but which , 50 years later , has returned as national policy . during his munich years , klaus - rdiger developed a strong connection to the dresden university radiobiology group through his dear friend thomas herrmann . this led him to forge ties with the gdr , where he was considered the international expert to explain all issues that dresden was in german . 
although politics meant a relative backwater in international science at this time , 50 years later , it is now a major internationally recognized player . research in the mid - 80s focused on radiation effects on the heart , a eld very contrary to textbook learning . 
klausrdigers work challenged the concept that the heart was a radiation - resistant organ , and nally , 50 years later , this is the generally accepted theory . ever the anglophile , klaus - rdiger nally saw the light and moved to london at the end of the 80s as professor for radiation biology at st . 
here , he found a new home and created a successful radiobiology lab , networked within london , the united kingdom , europe , and the rest of the world . 
at ucl , he founded the european masters course in radiation biology , sometimes called klaus trotts travelling circus , because of his idea to bring the students to the teacher rather than the traditional alternative . 
students were allowed to 748 strahlenther onkol ( 2020 ) 196 : 747748 rotate across europe , receiving very intense teaching from an international faculty of the leading european radiation researchers . 
ex - students are now positioned as leaders in the eld , spread across the world , holding appointments in well - recognized institutions such as the german cancer research center ( dkfz ) in heidelberg , the international atomic energy agency ( iaea ) in vienna , the world health organization ( who ) in geneva , as well as several european and noneuropean universities and governmental agencies . 
it has been said that the article 31 expert group of the european commission is in fact a klaus - rdiger - family get together . when klaus - rdiger ofcially retired from ucl in london , he of course continued teaching and overseeing the ucl msc course . 
however , together with his lovely wife uta - elisabeth , he diverted most of his private life back to munich , to the bavarian alps and lakes , and to his wifes hometown of nurnberg . with the advent of tuition fees in the uk , it was clear that the majority of students could no longer afford the course . klaus - rdiger came up with a logical , if somewhat unusual solution : move the course to home . 
this was realized in 2016 when the technical university of munich ( tum ) was able to offer a 2 - year masters degree in radiation biology . it has taken almost 50 years to complete this circle , but through powers of persuasion , logical arguments , and a lot of very hard work , the course started teaching in 2016 . of course , one of the key lecturers is the untiring klausrdiger trott , who somehow manages the lions share of the teaching whilst still maintaining a fatherly eye over the welfare of the students , with , of course , considerable behind - the - scenes work from uta - elisabeth . 
today , he can still be found in the labs and clinics almost on a daily basis , and the students love their knowledgeable and caring professor . together with his wife , uta - elisabeth , who serves as a continuous and critical observer of klaus - rdigers career , and as a lector of his essays and publications , he nds some time to enjoy art and music . 
regular visits to london are packed with visits to the coliseum , covent garden , galleries , and exhibitions , as well as regular bicycle rides through regents park and the royal botanic gardens . 
back in germany it is gasteig , the staatstheatre , and the many museums that take their interest , and the english garden is of course the scene of the bicycle tours . 
probably unknown to most is klaus second academic life , where under the tutelage of uta , they have researched , documented , catalogued , and published the family history of uta - elisabeths family . 
clearly from the hand of the trotts , the exhibition featured an equal mixture of art and science . one word can be used to sum up the contribution of klaus - rdiger trott to radiation biology . 
if you look this up , you will see that it means family as in extended family as in bloodrelated and adoptive and international ; especially , it means nobody will be left behind . funding open access funding provided by projekt deal . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
in biopsy specimens obtained before chemoradiotherapy or radiotherapy , greater inltration of cd8 + t cells ( p = 0.001 ) and foxp3 + t cells ( p = 0.003 ) were signicant predictors of better overall survival ( os )  . 
radiotherapy also acts as an immune adjuvant [ 36 ] and the same is true for chemotherapy [ 7 ]  . however , there is insufcient information about the inuence of radiotherapy or chemoradiotherapy on various cells and molecules related to tumor immunity in patients with uterine cervical cancer , interfering with our understanding of the role of immunological changes in the treatment of this tumor . at our institution , preoperative radiotherapy or chemoradiotherapy had been performed before radical hysterectomy to improve tumor resectability [ 8 ]  . 
in the present study , we evaluated radiation - induced or chemoradiotherapy - in726 strahlenther onkol ( 2020 ) 196 : 725735 duced alterations in the expression of various proteins related to tumor immunity and changes of tumor - inltrating cd8 + t cells ( cytotoxic t cells ) by immunohistochemical analysis of paired pre - radiation biopsy specimens and post - radiation resected tumor specimens . 
in addition to cd 8 + t cells , we examined the expression of programmed death ligand 1 ( pd - l1 ) , programmed death 1 ( pd - 1 ) , human leukocyte antigen class i ( hla - 1 ) , and forkhead box p3 ( foxp3 ) in tumor tissues . 
the subjects were 104 patients with squamous cell carcinoma of the uterine cervix who underwent preoperative radiotherapy or chemoradiotherapy ( chemoradiotherapy ) and surgery at our institution between january 2000 and december 2011 . their characteristics are listed in table 1 . 
these tissues contained positive and negative staining elements for each protein and were therefore suitable controls to conrm that the assay was performed properly . all hematoxylin and eosin - stained slides were evaluated to select the most representative slide for immunohistochemistry . 
as the postoperative specimen , a slide with a large component of residual tumor was selected for immunohistochemistry . pd - 1 and foxp3 were not evaluated in the biopsy samples of 2 patients or in the surgical samples of 4 patients , since the specimens were inadequate . to assess pd - l1 and hla - 1 , tumors and stroma in the whole slide were analyzed . 
for cd8 , foxp3 , and pd - 1 , three representative elds of view of the tumor and contiguous peritumoral stroma were chosen and positive cells were manually counted in the high - power view ( x400 )  . the average number of positive cells in the three elds was calculated . 
pd - l1 - expressing tumor cells ( pd - l1 tc ) and pd - l1 - expressing tumor - inltrating immune cells ( pd - l1 ic ) were analyzed separately by modication of a previous approach [ 12 , 13 ]  . 
we also scored tumor - inltrating immune cells expressing pd - l1 as a percentage of the tumor area : ic3 was 10% , ic2 was 5% and < 10% , ic1 was 1% and < 5% , and ic0 was < 1% [ 12 , 13 ]  . for all markers , receiver operating characteristic ( roc ) curves were generated on the basis of the level of stain728 strahlenther onkol ( 2020 ) 196 : 725735 ing and the corresponding prognosis . 
the same cutoff value was used for samples obtained before and after radiation therapy , and cutoff values for each marker are described in supplementary figure e3 and supplementary table e1 . 
cd8 positivity was dened as 80 cd8 - positive cells and pd - 1 positivity was dened as 13 cells as the average number of positive cells in three elds . 
for foxp3 , we counted the number of positive cells associated with intratumoral and contiguous peritumoral stroma , with foxp3 positivity being dened as 60 foxp3 - positive cells on average . the results of immunohistochemical staining were evaluated by two researchers ( including one pathologist ) who were blinded to the treatment of each patient . lated by the kaplanmeier method and the log - rank test was used to compare survival curves . 
fine and gray competing risks regression model was used for univariate analyses for the cumulative incidence of recurrence . all the p - values were two sided and signicance was set at a p - value of 0.05. 
because we used six immunohistochemical staining parameters ( pd - l1 tc , pd - l1 ic , cd8 , hla - 1 , foxp3 , and pd - 1 ) , we performed adjustment for multiplicity with bonferroni correction and p = 0.0083 was dened as signicant in survival analyses and table 2 . all of the statistical tests were performed using xlstat version 2019.1.3 ( addinsoft , paris , france ) and ezr software ( version 1.33 ) [ 15 ]  . treatment results the treatment eld extended from the l4 / l5 disc space to the mid - pubic level . 
in 3 patients , intracavitary radiotherapy with 137cs was performed after external radiotherapy and the total dose ( calculated at point a ) was 7.530 gy ( median 23 gy ) delivered in 12 fractions . 
radical hysterectomy was performed a median of 22 days after completion of radiotherapy ( table 1 )  . statistical analysis the median follow - up period was 64 months ( range 1162 months )  . 
the overall survival ( os ) rate was calculated from the date of surgery to the date of death from any cause or date of the last follow - up visit . 
the wilcoxon signed - rank test was used to analyze differences of changes in the expression of tumor immunity - related proteins by tumor cells and immune cells after radiotherapy . 
overall survival was calcuthe clinical outcome is shown in supplementary figure e4 . there was no recurrence in 74 patients , 19 patients showed out - of - eld failure , 13 patients had in - eld recurrence , and 2 patients had both out - of - eld and in - eld recurrence . representative patterns of tumor staining for pd - l1 , pd - 1 , cd8 , foxp3 , and hla - 1 are shown in fig . 
however , the signicance of these factors was lost after bonferroni correction , except for cd8 and foxp3 ( table 2 )  . the same analyses were also performed using surgical specimens resected after radiotherapy in patients without pathological cr ( non - pcr ) , since pd - l1 and hla - 1 expression by tumor cells could not be assessed in cr patients due to lack of tumor cells . 
in contrast , pd - l1 ic , cd8 , hla - 1 , foxp3 , and pd - 1 expression were not signicantly related to os ( table 2 )  . 730 strahlenther onkol ( 2020 ) 196 : 725735 fig . 
found that pd - l1 tc and cd8 + t cells both increased after chemoradiotherapy by paired analysis of pre - chemoradiotherapy biopsies and corresponding post - chemoradiotherapy resected tissues in rectal cancer patients undergoing chemoradiotherapy followed by surgery [ 23 ]  . 
our results did not agree with those of enwere about radical chemoradiotherapy for cervical cancer , since they found that neither expression of pd - l1 nor the density of cd8 + t cells was associated with progression - free or overall survival [ 28 ]  . 
this seemingly paradoxical observation , in which expression of an immunosuppressive molecule is correlated with improved outcomes , may suggest that upregulation of pdl1 in the tumor microenvironment should not necessarily fig . 
4 cumulative incidence of out - of - eld recurrences according to the expression of pd - l1 in tumor cell ( pd - l1 tc ) after radiotherapy next , the relationship between the site of recurrence and pd - l1 tc in surgical specimens resected after radiotherapy was examined . 
evidence suggests that tumors present neoantigens to promote the release of ifn by tumor - inltrating cd8 + t cells , after which ifn upregulates pd - l1 expression on immune cells and tumor cells , leading to signicant relationships among tumor - inltrating cd8 + t cells , pd - l1 tc , and pd - l1 ic [ 1720 ]  . 
radiotherapy creates a proinammatory tumor microenvironment by releasing danger signals and activating tumor - specic adaptive immunity , leading to upregulation of pd - l1 expression by both immune cells and tumor cells [ 1 , 2 ]  . 
recently , it was reported that induction of double - stranded dna breaks by radiation upregulates pd - l1 expression via the atm / atr / chk1 pathway [ 22 ]  . 
these results suggest that radioimmunotherapy using immune checkpoint inhibitors , such as anti - pd1 or anti - pd - l1 antibodies , could be benecial . in the present study , the number of tumor - inltrating cd8 + t cells showed a signicant decrease after radiotherstrahlenther onkol ( 2020 ) 196 : 725735 be interpreted as indicating dominance of immunosuppression , because upregulation of pd - l1 is also associated with inammation . 
immuneactivating danger - associated molecular patterns ( damps ) and pro - inammatory cytokines are released after radiotherapy , resulting in a tumor microenvironment that favors the maturation and activation of immune cells . 
radiotherapy can induce immunogenic cell death , which could release neoantigens and hpv - derived antigens and also trigger the uptake of these antigenic components by dendritic cells , thus activating t cell - mediated immunity with expansion of antigenspecic cytotoxic t cells and production of tumor - specic monoclonal antibodies [ 32 ]  . 
however , further investigations will be needed to verify our ndings , possibly leading to development of the optimal combination of radiotherapy with immunotherapy . platinum - based chemotherapy was administered to 58 of 104 patients during radiotherapy in our study . 
in vivo , fractionated radiation in combination with dacarbazine induced pd - l1 expression by melanoma cells , suggesting that surface expression of pdl1 differs and is partially linked to ifn - gamma expression and il - 6 release in dependence on the tumor and time after treatment [ 33 ]  . important limitations of the present study include a relatively small sample size and heterogeneity of the patient prole and treatment due to its retrospective design . 
furthermore , pd - l1 and hla - 1 expression were quantied using the whole slide , but cd8 , foxp3 , and pd - 1 were assessed in three representative elds of view with high expression ( so - called hotspots )  . 
surgical specimens obtained after radiotherapy or chemoradiotherapy often have little residual tumor , and it was difcult to strictly evaluate intratumoral tissue and stroma , so we measured expression at hotspots mainly present in the tumor margin and in the vicinity of the stroma . 
although this method may not necessarily reect the status of immunity throughout the tumor , it assessed the maximum immune response within a heterogeneous tumor and the antigenicity of the tumor cells . 
although preoperative radiation therapy is not usually given for cervical cancer , our results could provide useful information for developing an appropriate combination of immunotherapy and radical radiotherapy or postoperative radiotherapy . in summary , radiotherapy for cervical cancer induced an immunologic shift with an increase of pd - l1 tc . 
in surgical specimens resected after radiotherapy , higher pd - l1 tc was the only signicant predictor of better os and was related to a signicantly lower risk of out - of - eld recurrence . this strong relationship of pd - l1 expression by tumor cells after radiotherapy to the prognosis suggests that radiotherapyor chemoradiotherapy - induced immunological effects may inuence the results of treatment for uterine cervical cancer . 
georgakilas5 soile tapio6 received : 15 april 2020 / accepted : 5 may 2020 / published online : 9 may 2020 the author ( s ) 2020 abstract in the current dismal situation of the covid - 19 pandemic , effective management of patients with pneumonia and acute respiratory distress syndrome is of vital importance . 
due to the current lack of effective pharmacological concepts , this situation has caused interest in ( re ) considering historical reports on the treatment of patients with low - dose radiation therapy for pneumonia . 
this concise review aims to critically review the evidence for low - dose radiation treatment of covid - 19 pneumopathy and discuss whether it is worth investigating in the present clinical situation . keywords sars - cov - 2 low - dose radiation therapy pneumonia covid - 19 anti - inammatory introduction covid - 19 is caused by the severe acute respiratory syndrome coronavirus 2 ( sars - cov - 2 )  . 
the spectrum of clinical symptoms of patients with sars - cov - 2 infection is broad and encompasses asymptomatic infection , ( cid : 2 ) franz rdel franz.roedel@kgu.de 1 department of radiotherapy and oncology , universittsklinikum frankfurt am main , goethe - university , theodor - stern - kai 7 , 60590 frankfurt am main , germany 2 department of radiation oncology , hospital universitari sant joan de reus , university of rovira i virgili , tarragona , spain 3 department of radiation oncology , universittsklinikum erlangen , erlangen , germany 4 department of biophysics , gsi helmholtzzentrum fr schwerionenforschung , darmstadt , germany 5 dna damage laboratory , physics department , school of applied mathematical and physical sciences , national technical university of athens ( ntua ) , athens , greece institute of radiation biology , helmholtz zentrum mnchen , german research center for environmental health gmbh , neuherberg , germany 7 department of radiation oncology , technical university of munich , munich , germany mild and moderate to severe illness of the upper respiratory tract , severe pneumonia , acute respiratory distress syndrome ( ards ) , respiratory failure , and death . 
severe courses are often associated with comorbidities such as hypertension [ 1 ] and a severe respiratory symptomatic stage goes along with a high viral load occurring during the early phase of disease [ 2 , 3 ]  . 
high viral load could be the result of low immune responses against the virus , but also due to high expression of the cell - entry receptor for sars - cov - 2 ( the angiotensin - converting enzyme 2 [ ace2 ] receptor ) [ 4 ]  . 
although a multitude of pharmacological studies are underway , no effective treatment ( except supportive oxygen breathing and mechanical ventilation systems ) appears to be available and intensive care units which provide these options are severely limited . 
this situation has caused interest in ( re ) considering the historical treatment of patients with low - dose radiation therapy for pneumonia . evidence on low - dose irradiation for treatment of pneumonia remarkably , in 2013 , calabrese and dhavan published a report on how radiotherapy was historically used to treat pneumonia : could it be useful today ? , which may serve as a basis for current considerations [ 5 ]  . 
this review on 15 reports covers 863 patients with severe pneumonia of 680 strahlenther onkol ( 2020 ) 196 : 679682 different pathogeneses , including two studies of viral origin treated with low doses of kilovoltage x - rays . 
as compared to present standards , they are of low - level evidence , some cover low numbers of patients , and in many cases appropriate control groups are lacking . 
in addition , for more than seven decades , not a single report has been published on low - dose radiotherapy for pneumonia , further hampering recommendations for decision - making based upon clinical and scientic knowledge . 
in a cohort of 130 patients treated for post - partum mastitis with single doses of 0.20.5 gy up to a total dose of 11.5 gy , herrmann reported on a cure rate of over 90% if given within the rst 24 h of the rst signs of inammation , but a decline to 50% if given at full blown inammation [ 7 ]  . the biological mechanisms underlying the effectiveness of these doses have been subjected to intensive research during the past 30 years . 
these include , among others , modulation of the inammatory properties of leukocytes , macrophages , broblasts , and endothelial cells , as well as of the secretion of cytokines / chemokines and growth factors ( reviewed in [ 8 , 9 ] )  . 
radiation doses required for effective treatment are very low ( < 1% of doses used for anti - cancer radiotherapy ) and do not exceed the tolerance doses of the critical organs in the irradiated volume such as heart , thyroid , stomach , or kidneys . 
furthermore , the risk of late and very late radiation damage in adjacent organs from such low - dose radiation treatment which needs to be considered is induction of cancer after latencies of > 10 years . 
cautious estimates suggest risks to be well below 1% [ 12 ]  . if considering a clinical study , however , a major obstacle is the appropriate timing of irradiation . 
in general , early control of viral replication by , particularly , type i interferons ( ifns - i ) , limits viral spread within the host during the early phases of disease . 
ifns - i increase the expression of interferon - stimulated genes , which results in stimulation of effector functions of cells of the innate and adaptive immune systehowever , sustained expression of ifns - i might also result in viral persistence [ 13 ]  . 
severe cases of sars have further been reported to be associated with high serum levels of pro - inammatory cytokines and increased accumulation of innate immune cells in the lung , nally resulting in extensive lung damage [ 14 ]  . 
recent analyses have conrmed that severe cases of covid - 19 are associated with increased interleukin - 6 ( il - 6 ) levels in the serulow - dose irradiation does not decrease the viability of virus directly , yet it may increase the effectiveness of anti - viral immune responses . 
an additional prominent risk factor for severe disease progression is d - dimer > 1 g / ml in the serum [ 1 ]  . in the early to medium stages of sars - cov - 2 infection , treatment with low - dose radiotherapy of the lungs might be benecial to ameliorate the establishing inammation and to slow down its chronication . 
at chronic stages of disease characterized by cytokine release syndrome ( crs , cytokine storm ) , low - dose irradiation might not be as efcient as in the early progressive stage , as also reported in historical publications . 
however , one has to consider that in the recovery phase of covid19 patients , particularly activated cd38and hla - dr - expressing cd4 + and cd8 + t cells are increased in the patients alongside igm and igg sars - cov - 2 - binding antibodies [ 16 ]  . 
this stresses the point that timing of irradiation has to be carefully chosen to avoid attenuation of disease - resolving immune response , e.g. , by stimulating ifns - i . 
the strahlenther onkol ( 2020 ) 196 : 679682 indication for low - dose radiotherapy should be based on lung function , i.e. , progression of respiratory distress . another point to consider is that low doses of irradiation in the infected lungs , even at doses up to 0.5 gy , are expected to induce a low number of rna damage events and mutations in the virus and be of a low selective pressure . 
in addition , as discussed in a recent manuscript [ 20 ] , any antiviral drug treatment against sarscov - 2 would probably result in a more intense selective pressure on the virus . conclusion in the current dismal situation of the covid - 19 pandemic , effective management of these seriously ill patients is crucial . 
gaipl declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
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hautmann1 franz josef putz4 michael behr5 oliver klbl1 felix steger1 philipp rechner2 ulrich neumaier3 christoph s1 barbara dietl1 received : 12 august 2019 / accepted : 28 november 2019 / published online : 23 december 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose osteoarthritis is a common disease , with a prevalence of symptomatic disease of 8.9%. 
there is a discussion on whether the treatment results achieved with a linear accelerator are comparable to those with the orthovoltage technique . the aim of this study is to analyze the results of radiotherapy for osteoarthritis with a linear accelerator and compare the results with reference to different joints . materials and methods the analysis was performed in patients of two german radiotherapy institutions and included 295 irradiated joints . 
all investigated subgroups had a signicant reduction of pain . conclusion radiotherapy of osteoarthritis with a linear accelerator is an effective treatment which is very well tolerated . all analyzed subgroups show a good response to radiotherapy for at least 24 months . 
further investigations should be performed for a denitive answer to this question . keywords osteoarthritis osteoarthrosis arthrosis radiotherapy linear accelerator introduction osteoarthritis is a common disease , especially in elderly people . 
hautmann , pd , md matthias.hautmann@ukr.de 1 department of radiotherapy , university of regensburg , 94042 regensburg , germany privat clinic for dentistry , kreps , ergoldsbach , germany 3 mvz neumaier & kollegen , regensburg , germany 4 department of nephrology , university of regensburg , regensburg , germany 5 department of prosthetic dentistry , university of regensburg , regensburg , germany about 8.9% among the adult population [ 1 ]  . 
as life expectancy is rising and the prevalence of risk factors for osteoarthritis like overweight or inactivity is growing , an increasing prevalence of osteoarthritis can be expected in the future [ 3 ]  . several therapeutic options for treatment of osteoarthritis are in use [ 2 ]  . 
the drug therapy can be systemic , for example with nsaids ( non - steroidal anti - inammatory drugs ) , or can consist of local injections of anesthetics or steroids [ 69 ]  . 716 strahlenther onkol ( 2020 ) 196 : 715724 one effective non - invasive treatment for osteoarthritis is radiotherapy [ 1031 ]  . 
like for several other bone and joint disorders , low - dose radiation has shown an anti - inammatory effect [ 10 , 13 , 3240 ]  . most of the published samples were treated with orthovoltage therapy [ 35 , 4143 ]  . 
some others were irradiated with telecobalt devices or cesium devices [ 18 , 28 , 30 , 44 ]  . only a few relatively small samples exist where patients were treated with a linear accelerator [ 21 , 40 , 45 , 46 ]  . 
detailed information is missing in some of these manuscripts and the objective was different than that of our survey . there is one retrospective trial comparing the results of orthovoltage therapy versus radiotherapy with a linear accelerator just for osteoarthritis of the knee [ 47 ]  . 
this trial is only available in german language and has not been published in a magazine so far . many radiotherapy institutions do not use orthovoltage therapy anymore [ 4850 ]  . 
the therapy with telecobalt devices is obsolete in developed countries . the objective of this survey is to document and analyze the results of radiotherapy for osteoarthritis with a linear accelerator and to compare these results with those of orthovoltage therapy . a second ongoing discussion is whether small or large joints respond better to radiotherapy . 
for this reason , the other objective of this analysis was to compare the results upon treating different joints or joint regions with radiotherapy , with the main focus on the comparison of small and large joints . patients and methods the study was approved by the ethics committee of the university of regensburg . the retrospective analysis was performed on patients of two german radiotherapy institutions . 
some joints were cumulated to certain regions , like heberden or bouchard arthrosis , upper and lower ankle joint , or omarthritis and acromioclavicular arthritis . the patients data from the regular follow - up were analyzed . 
we identied the etiology of the pain and registered possible risk factors for a lack of response to radiation . pain was documented with the numeric rating scale ( nrs )  . 
an arthroplasty was dened as end of follow - up . we performed descriptive statistics , calculating median , range , and interquartile range ( iqr ) of nrs for all time periods . 
1 median pain on the numeric rating scale ( nrs ) during the follow - up we dened several subgroups by gender , age ( separated by the median age of 65 years ) , etiology , and the other parameters listed in table 1 . hip , knee , ankle , and shoulder were classied as large joints , whereas the nger , thumb , and big toe were categorized as small joints . results in total , 159 patients could be identied , questioned , and clinically examined . 
295 joints or joint regions were treated due to the fact that some patients were irradiated on more than one joint or region . the median age of the patients was 65 years with a range from 21 to 91 years and an iqr from 56 to 73 years . 
most of the time patients had taken non - steroidal drugs for a long time , had had intraarticular injections with hyaluronidase , or had used orthoses . the median follow - up was 19 months . radiotherapy was performed with a linear accelerator ( siemens primus and elekta synergy ) using 6or 15 - mv photons . 
male as well as female patients older and younger than 65 years ( median age of our sample ) had a signicant reduction in pain ( p < 0.0001 for all categories and the entire follow - up )  . patients were analyzed separately for different joints affected by osteoarthritis . 
despite this , there are data about measurable shrinkage of bakers cyst after rt for osteoarthritis of the knee , which represents a surrogate marker for the effect of rt in this indication [ 55 ]  . with less than 60 patients in each study , the statistical power is somewhat limited . 
furthermore , details about radiation technique , especially the machine used for treatment , are lacking and could not be inquired about . there are many retrospective studies and some prospective studies strongly assuming radiotherapy to be an effective treatment for osteoarthritis . 
beside this , there are prospective trials showing the effectiveness of low - dose radiotherapy by means of objective response criteria [ 55 , 56 ]  . there are many presently unanswered questions . 
all in all , there is need for further investigation . to our knowledge , this sample is one of the rst and largest in which radiotherapy of osteoarthritis with a linear accelerator has been systematically examined . 
kaltenborn focused on rhizarthritis , and in the survey of keilholz , only seven patients with hip arthritis had been treated with a linear accelerator . summarizing the patients of all published samples of radiotherapy of osteoarthritis with linear accelerators we could identify , our sample seems to be larger than the sum of all other samples . among other parameters , the dose rate , depth dose , and energy are different between orthovoltage devices and linear accelerator . 
there is a discussion on whether the published results can be transferred for treatment of osteoarthritis with a linear accelerator [ 57 ]  . nevertheless , many german radiotherapy institutions use linear accelerators for treatment of osteoarthritis . 
beside this , most of the orthovoltage devices were quite old , with a median age of 17 years [ 58 ]  . a retrospective comparison between orthovoltage therapy and treatment with a linear accelerator has already been done for heel spur syndrome and humeral epicondylitis . 
nevertheless , these results cant easily be transferred to radiotherapy of osteoarthritis , because it is a different disease with different target volumes and target structures . our sample seems to be comparable to other published samples with respect to patients parameters . 
for example , the median age of 65 years is nearly equal to that of the samples of micke et al . , a clinical quality assessment ( average age 63.3 years ) [ 46 ]  . 
also , the proportion of male to female patients with a ratio of approximately 1 : 2 is representative [ 46 , 53 ]  . the radiation technique and dose concept are equivalent to the recommended concept of the german cooperative group on radiotherapy for benign diseases . 
most of the published samples , especially the published samples of recent decades , were treated that way [ 61 ]  . radiotherapy of osteoarthritis with linear accelerators has proven benecial to our sample . 
the median follow - up of 19 months allows a statement of longterm results . most of the patients have a response to radiation and about one quarter of the patients are free of pain or score 720 strahlenther onkol ( 2020 ) 196 : 715724 table 2 summary of the published manuscripts concerning low - dose radiotherapy for osteoarthritis and case - related analysis author and year device joints response rate ( % ) complete or very good response ( % ) partial response ( % ) joint region mixed mixed mixed mixed mixed mixed mixed mixed mixed mixed mixed mixed knee knee mixed mixed mixed knee mixed hip , knee mixed knee hip , knee knee hip , knee knee hip , knee knee knee mixed hip , knee mixed mixed knee hip , knee mixed mixed knee knee heidenhein ( 1923 ) [ 66 ] kreuzwald ( 1926 ) [ 67 ] kahlmeter ( 1930 ) [ 68 ] fried ( 1934 ) [ 69 ] balike ( 1939 ) [ 70 ] toschke ( 1941 ) [ 71 ] cocchi ( 1943 ) [ 72 ] reichel ( 1949 ) [ 73 ] glauner ( 1951 ) [ 74 ] fuchs ( 1951 ) [ 27 ] pape et al . 
this effect lasts for at least 2 years . the overall response rate of our sample ( approximately 65% ) is within the range or slightly lower than that of most other published studies ( case - related average 77.7% ) and seems to be comparable with the results of orthovoltage therapy . because of the different anatomical regions , it is difcult to give a universal recommendation for target volumes and radiation dose or technique . 
for other non - malignant diseases , we would rather recommend applying a fractionated dose of 0.5 gy to a total dose of 3.0 gy for reasons of radiation protection [ 6264 ]  . whether orthovoltage therapy is superior to treatment with a linear accelerator is an interesting question . 
he states that it was a small sample and therefore does not have enough power to detect a difference . for that reason , we did a case - related analysis of the published samples irradiated because of osteoarthritis . 
9802 patients were veriably treated with orthovoltage therapy , 429 patients ( excluding our sample ) were treated with photons or gamma rays ( table 2 )  . most of the 429 patients were irradiated with a telecobalt or cesium device . 
we could identify only 149 cases , published in three samples , for which it is clearly stated that they were treated with a linear accelerator [ 40 , 45 , 47 ]  . 
we performed statistical comparison with the chi2 test . for all published samples in the literature the average response rate was 78% , for the joints treated with orthovoltage therapy it was 77.7% , for all other ( photons and gamma ray ) , including our sample , it was 60% . 
beside different dose concepts , inclusion criteria , and radiation techniques , the response criteria were also different , as are the follow - up periods and the timepoints at which the response was evaluated . over all published samples , excluding our sample , a signicant difference between the samples treated with orthovoltage therapy compared to those treated with photons or gamma rays in favor of orthovoltage therapy could be found . 
the lack of a signicant difference upon comparing the newer studies since 1995 might be due to the relatively small number of cases with sufcient information in this period . it might be interesting to conduct a prospective trial comparing orthovoltage therapy and radiotherapy with photons by a linear accelerator . differences between orthovoltage therapy and photon therapy are the different peak energies , dose distributions ( mostly due to different absorption ) , and dose rates , among others . 
one reason for the possible superiority of orthovoltage therapy might for example be the higher absorption of x - rays within the tissuein particular the bone tissuecompared to photons . another reason might be the higher absorption in the soft tissues , with a better anti - inammatory effect of the surrounding organs . 
also , the dose rate might be one possible explanation . further investigations of the nding that orthovoltage therapy might be superior to photons in the radiotherapy of osteoarthritis seem to be reasonable . 
a prospective study to clarify a possible different effect of these modalities should be performed . a signicant difference in the response between small and large joints could not be detected . 
the remaining lower nrs level for small joints 12 and 24 months after radiotherapy might be randoa certain joint or joint region with clear better or worse response to radiotherapy could not be detected in our survey . 
it appears , that radiotherapy of osteoarthritis can be offered to patients independently of the localization of the degenerative affected joint or joint region . radiotherapy of osteoarthritis with a linear accelerator is widely used and is an effective treatment which is very well tolerated . 
aim of this study was to analyze treatment efcacy and recurrence patterns after rit in early - stage nodal and extranodal fl . methods we reviewed 107 patients who were treated with combined rit in two centers . 
5 - year os was 98.1%. rit was tolerated well , with mainly grade 12 acute side effects . conclusion the real - world efcacy of rit is comparable with the results of the mir study . 
additionally , this analysis shows that extranodal involvement and grade 3a histology are not associated with inferior pfs . keywords radioimmunotherapy immunotherapy indolent lymphoma cd20 antibody grade 3a follicular lymphoma ( cid : 2 ) med . 
ten - year progression - free survival ( pfs ) rates in different studies of the pre - rituximab era , using involved eld ( if ) , extended eld ( ef ) , and total lymphatic irradiation ( tli ) , ranged from 38 to 72% [ 28 ]  . however , extensive radiation protocols are associated with signicant toxicities , e.g. , grade 3 and 4 adverse events concerning the hematopoietic system in 22% of patients 706 strahlenther onkol ( 2020 ) 196 : 705714 table 1 patients , tumor , and treatment characteristics number of patients / lesions [ 7 ]  . 
therefore , the national comprehensive cancer network ( nccn ) guidelines recommend radiation treatment of the pathologically involved regions only ( involved - site radiation therapy [ is - rt ] ) without prophylactic treatment of additional lymph node areas . 
a recently published randomized trial showed a superior pfs with ifrt and combined immunotherapy with r - cvp compared to if - rt only , showing that additional rituximab - comprising systemic therapy reduces out - of - eld relapses and therefore might be an important component [ 13 ]  . 
the combination of localized standard - dose radiotherapy and rituximab showed a high efcacy , with low recurrence rates and preserved quality of life [ 15 ]  . this retrospective study evaluates the effect and toxicity of radioimmunotherapy ( rit ) treatment analogue to the mir study under real - world conditions and also conducts a detailed recurrence pattern analysis . 
in contrast to the mir study , this cohort not only includes patients with nodal but also those with extranodal disease and histological grade 3a ( who grading ) fl . materials and methods patients and tumor characteristics patient records and follow - up ( fu ) imaging of 107 patients who had been treated with combined rit according to the mir concept were reviewed in two centers ( university hospital heidelberg and university hospital ulm )  . 
not applicable strahlenther onkol ( 2020 ) 196 : 705714 details of patient , tumor , and treatment characteristics are shown in table 1 . treatment and follow - up treatment was applied according to the mir study [ 15 , 16 ]  . it consisted of four once per week administrations of rituximab ( 375 mg / m2 ) upfront . 
four further weekly administrations of rituximab were given in weeks 912 during the radiation treatment period . radiotherapy of the involved lymph node regions was initiated in week 9 and applied in 2 gy single doses ( ve times per week ) up to a total dose of 30 gy . 
in case of remaining lymphoma after initial rituximab therapy in week 7 , the residual region was boosted with an additional 10 gy ( 5 2 gy ) in week 12 to a total dose of 40 gy . patients were followed up regularly with clinical examinations and ct or mr imaging . 
response evaluation was performed using the response criteria for lymphoma [ 17 , 18 ] classied into complete remission ( cr ) , partial remission ( pr ) , stable disease ( sd ) , and progressive disease ( pd )  . 
toxicity was classied according to the common terminology criteria for adverse events v4.03 ( ctcae ) 812 weeks after rit ( acute toxicity ) or 36 months after rit ( late toxicity )  . statistical analysis and ethics we reviewed patient records , planning documents , and imaging scans to assess response , current status of the disease , and following therapies . 
progression - free survival ( pfs ) was calculated in months from the beginning of therapy until the diagnosis table 2 chronological response rates after treatment of recurrent disease or death . 
the analysis was approved by the local ethics committee ( s - 106 / 2019 )  . results patients and treatment from 12 / 2005 until 11 / 2017 , 107 patients ( 55 female / 52 male ) were treated with combined rit . 
ninety - ve percent of the patients received all eight planned cycles of rituximab and rt was either applied with a 3d - conformal technique ( 71% ) or intensitymodulated rt ( imrt ; 29% )  . 
five patients with a longer period until the start of rit ( > 12 months ) were treated with a watch - and - wait strategy due to their own wish . 
various patient , tumor , and treatment characteristics ( age , sex , grading , stage , extranodal manifestation , localization , type of involvement , number of applied cycles of rituximab , rt technique ) were analyzed as prognostic factors for pfs . 
two patients died due to chronic heart failure . rit was tolerated well , with mild ( grade 12 ) acute side effects in 85.0% of the patients and only 0.9% grade 3 toxicity ( one patient with acute mucositis , which needed temporary medical intervention )  . 
for elderly patients or patients in a reduced general condition , active surveillance might be considered . upfront radiotherapy has proven to be effective and improved both disease - specic and overall survival based on a large national cancer data base analysis [ 20 ]  . 
several trials , among others the aro 98 - 01 trial , used large treatment elds and showed a higher effectiveness compared to smaller irradiation elds , since most recurrences developed outside of irradiated areas [ 3 , 7 , 21 ] , implicating that occult microscopic disease might be present in early - stage fl patients . 
thus , several studies showed that combined treatment comprising radiotherapy and systemic chemotherapy and / or immunotherapy with rituximab were benecial over radiotherapy alone , but with high toxicity rates [ 9 , 13 , 22 , 23 ]  . 
although the current analysis has its limitations owing to the retrospective nature , it conrms the results of the mir trial with a comparable 5 - year pfs of 87.6%. 
the current data strengthen the hypothesis that patients with fl grade 3a might also benet from the strahlenther onkol ( 2020 ) 196 : 705714 combined treatment approach as do patients with fl grade 1 or 2 . furthermore , rituximab enhances radiation sensitivity in vitro [ 24 ] and several studies proved that rituximab eliminates minimal residual disease ( mrd ) [ 25 , 26 ] , underlining an abscopal effect . 
a limitation of this study is that mrd was not assessed and several studies recently emphasized the importance of molecular disease monitoring as positive bone marrow pcr at baseline highly correlates with poorer outcome [ 15 , 26 ]  . we could identify several positive prognostic factors for pfs in covariate analysis : response to rituximab after four cycles and after combined rit were both associated with higher pfs rates . 
response to rituximab might therefore be a useful parameter for a response - adapted treatment . furthermore , patients with lower tumor burden ( tumor size < 7 cm , which was an inclusion criterion in the mir study ) and completely excised lymphoma manifestation showed better pfs . 
as already shown by our group , ldrt might be an effective and potentially curative option in recurrent disease , with long - lasting remissions [ 27 ]  . similar to the mir study , most of the recurrences were detected outeld , emphasizing the importance of systemic therapy on the one hand but also the effectiveness of local radiotherapy on the other . 
however , the latest prospective reports about the combination of local radiotherapy and systemic therapy used 3040 gy [ 13 , 15 ]  . moreover , there have been several retrospective analyses that evaluated low - dose radiotherapy ( ldrt ) regimens with 2 2 gy in a retrospective manner : all publications showed high orr , but most of the patients were treated in mainly a palliative setting [ 29 , 30 ]  . 
a prospective german multicenter study ( gazai study ) that will investigate ldrt of 4 gy in combination with the cd20 antibody obinutuzumab in patients with early - stage nodal follicular lymphoma is currently ongoing [ 31 ]  . 
this study will investigate a responseadapted treatment approach considering response to rituximab upfront , which this analysis has shown to be a prognostic factor for pfs . for certain extranodal lymphomas , e.g. , orbital lymphomas , ldrt only is associated with excellent control rates with very low local and distant recurrence rates [ 32 , 33 ] , so that additional rituximab in this patient cohort will probably yield only small benecial effects . current guidelines recommend fdg - pet for staging purposes due to the higher sensitivity and specicity [ 3436 ] , because a remarkable number of patients show a stage shift when performing fdg - pet [ 37 ]  . 
the foll05 trial identied an increased number of nodal involvement in 32% of fdg - pet staged patients and the impact of fdg - pet staging was highest with limited stages ( 62% upstaging with fdg - pet ) [ 37 ]  . furthermore , two recent studies emphasized the prognostic role of fdg - pet - ct regarding outcome . 
on the one hand , outcome appears to be better for patients having received pet - ct compared to historical series ( 5 - year pfs and os 69% and 96% ) [ 38 ]  . 
as a subsequent trial , the gazai study uses fdg - pet for staging as well as for ( metabolic ) response evaluation and therapy adaption . the mir study showed that combined rit is tolerated well , with low toxicity and without compromising quality of life [ 15 ]  . 
although evaluated retrospectively , acute toxicity rates in our analysis were low , with mostly mild ( grade 12 ) acute side effects in 84.5% of the patients and only 1.8% grade 3 toxicity ( 4% grade 3 toxicity in the mir study )  . a retrospective study compared involved regional rt to a smaller involved - site rt in 237 patients . 
the most common pattern of failure was distant failure , but with no 712 strahlenther onkol ( 2020 ) 196 : 705714 difference after 10 years between the rt volumes ( regional rt 38% , involved site 32% ) and a 5 - year pfs of about 6570% [ 40 ]  . 
hence , reducing rt elds may not compromise long - term outcomes and the international lymphoma radiation oncology group ( ilrog ) also adopted this in their current guideline [ 41 ]  . 
the superior 5 - year pfs rate in our analysis ( 87.3% ) might be due to the advantageous treatment of combined rit . vide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
to view a copy of this licence , visit conclusion combined rit in follicular lymphoma is an effective treatment option , with high response rates and long - lasting remissions as well as low toxicity rates . 
although this is a retrospective analysis , we were able to conrm the results of the mir study under real - world conditions and , furthermore , also investigated the efcacy of rit in extranodal manifestations and who grade 3a fl . funding this work was supported by a heidelberg university young investigator grant to lk . 
all the authors were responsible for data interpretation , participated in manuscript revisions , and approved the nal manuscript . funding open access funding provided by projekt deal . compliance with ethical guidelines conict of interest k . 
debus declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants or on human tissue were in accordance with the ethical standards of the institutional and / or national research committee ( heidelberg ethics committee ( s - 106 / 2019 ) ) and with the 1975 helsinki declaration and its later amendments or comparable ethical standards . 
koerber1 , 2 , 3 gerald major1 , 2 , 3 markus alber1 , 2 , 3 sati akbaba1 , 2 , 3 jrgen debus1 , 2 , 3 , 4 , 5 juliane hrner - rieber1 , 2 , 3 , 5 received : 23 october 2019 / accepted : 7 january 2020 / published online : 30 january 2020 the author ( s ) 2020 abstract purpose magnetic resonance - guided radiotherapy ( mrgrt ) has recently been introduced in our institution . 
as mrgrt requires high patient compliance compared to conventional techniques and can be associated with prolonged treatment times , feasibility and patient tolerance were prospectively assessed using patient - reported outcome questionnaires ( pro - q )  . materials and methods forty - three patients were enrolled in a prospective observational study and treated with mrgrt on a low - eld hybrid magnetic resonance linear accelerator system ( mr - linac ) between april 2018 and april 2019 . for assistance in gated breath - hold delivery using cine - mri , a video feedback system was installed . 
pro - qs consisted of questions on mr - related complaints and also assessed aspects of active patient participation . results the most commonly treated anatomic sites were nodal metastases and liver lesions . 
the mean treatment time was 34 min with a mean beam - on time of 2 : 17 mgated stereotactic body radiotherapy ( sbrt ) was applied in 47% of all patients . 
almost two thirds of patients ( 65% ) complained about at least one item of the pro - q ( score 4 ) , mainly concerning coldness , paresthesia , and uncomfortable positioning . 
all patients reported high levels of satisfaction with their active role using the video feedback system in breath - hold delivery . conclusion mrgrt was successfully implemented in our clinic and well tolerated by all patients , despite mr - related complaints and complaints about uncomfortable immobilization . 
currently , image guidance is mainly based on kilovoltage or megavoltage computed tomography ( ct ) imaging as the standard of care , which is routinely incorporated in most modern radiotherapy units . 
however , onboard ct imaging only offers poor soft tissue contrast and hence primarily enables image guidance based on bony anatomy [ 4 ]  . magnetic resonance ( mr ) imaging , with its superior soft - tissue contrast , facilitates enhanced differentiation between cancerous and healthy tissue as well as functional assessment of treatment response [ 5 , 6 ]  . 
given the technical challenges in integrating mr imaging ( mri ) into a linear accelerator , rst studies on mr - guided radiotherapy ( mr692 strahlenther onkol ( 2020 ) 196 : 691698 grt ) focused on ofine solutions and reported efcacy and feasibility for this technique [ 710 ]  . recently , devices integrating an mri scanner with a treatment delivery system have become clinically available [ 1115 ]  . 
these new hybrid systems for mrgrt do not only offer three - dimensional mri for soft tissue target and organ at risk visualization , but also allow for continuous cine - mri before as well as during treatment [ 12 , 13 ]  . 
in the current analysis , we describe our institutional experience with the implementation of mrgrt within a highvolume clinical center after 1 year of patient treatments , and review patient - reported outcomes . materials and methods after obtaining written informed consent , all analyzed patients were included in a prospective observational clinical trial , which had been approved by the local ethics committee . 
for the period from april 2018 to april 2019 , the trial database was interrogated for clinical information , including demographic data , dates of treatment , disease sites treated , dose and fractionation , and treatment duration . simulation and planning free breathing or in inspiration breath - hold , followed by planar cine - mri in a sagittal plane to evaluate target motion characteristics . 
following simulation , mri and ct datasets were transferred to the tps and deformably registered using the vendor - supplied deformation algorithm , which for multimodal deformable image registration iteratively tries to minimize a dissimilarity measure computed from mutual information . 
depending on the region to be treated , clinical target volumes ( ctv ) were expanded from the gtv using margins of 1 mm ( for example pelvic lymph nodes ) to 5 mm ( for example hepatic metastases )  . 
an isotropic planning target volume ( ptv ) margin of 4 mm was added in order to account for technical inaccuracies . for all patients , the simulation mri datasets were chosen as primary image sets for treatment planning , in order to facilitate same - modality image registration during daily treatment . 
step - and - shoot treatment plans were generated using the dedicated tps , where dose calculation was always performed via monte carlo dose calculation taking into account the static magnetic eld . treatment all patients underwent mr simulation directly at the treatment machine . 
thereby , not only were mr images for treatment planning generated , but tolerability of immobilization and placement of receiver coils , patient compliance to breathing instructions , and ability to perform inspiration breath - hold were also assessed . 
depending on the treatment region , 3d simulation mr images were acquired either in daily image guidance was performed for each fraction by onboard 3d mri using identical settings ( eld of view , duration , pulse sequence , breathing instructions ) as during mr simulation . 
soft tissue - based registration with the reference mr scan was applied , usually registering directly on the gtv , and the couch shifted accordingly . real - time mr gating was used for all patients for whom respiratory movement of the target was detected during strahlenther onkol ( 2020 ) 196 : 691698 mr simulation . 
a gating target ( region of interest , roi ) was dened ( either the tumor / resection cavity or a surrogate , e.g. , vessel , bronchus in close proximity ) , and the gating boundary was selected as a numerical margin added to the target ranging between 3 and 4 mm at the discretion of the treating physician . 
due to uncertainties in deformable registration and image noise possibly causing errors in contour tracking [ 17 ] , a small percentage of target outside of the predened boundary without triggering a beam - off event was allowed ( threshold - roi% ) [ 17 ]  . 
instead , the treatment was always interrupted and a repeat volumetric mri scan was performed to allow a 3d positional correction . during gated delivery , patients were provided with visual guidance via an in - room screen displaying the live sagittal cine - mr image with an overlay of gating target and boundary , thus enabling them to steer their repeated breath - holds to the right position . 
in addition to respiratory gating , the gating functionality of the system was also used for target tracking on patients in whom the target did not move with respiration , in - room screen used for live visual patient feedback during fig . 
1 gated treatments in order to ensure that no other movements happened during treatment [ 21 ]  . design of the patient - reported outcome questionnaire patient - reported acceptance of the whole treatment procedure was documented using an in - house developed patient - reported outcome questionnaire ( pro - q ; see table 1 ) , which was completed after the rst fraction , weekly during the treatment , and after the last fraction . 
items were scored using a ve - point scale . in addition to the experience reported by the patients , the staff on the system ( therapists and physicians ) were questioned about overall patient compliance for each patient after the rst and last fraction . 
they were asked to score the overall compliance of the patient with the treatment procedure on a scale from 1 ( very uncomplicated ) to 10 ( very complicated )  . statistical analysis data analysis was performed with the help of excel 2010 ( microsoft corporation ; redmond , usa ) as well as spss ( version 20.0 ; ibm , armonk , usa )  . 
signicance was noted for p - values of ( cid : 2 ) 0.05. results patient and treatment characteristics from april 2018 to april 2019 , 43 patients were treated on the mridian linac system , with a total of 428 fractions . 
patients had a mean age of 64 years ( range 3287 ) at the beginning of treatment , were mainly male ( 58% ) , and had a median karnofsky performance score of 80% . 
mrgrt was selected for these patients due to a variety of reasons , including superior soft tissue contrast or gated dose delivery and mostly for a combination of these factors . 
for ve patients with bony lesions , a benet of soft tissue contrast was assumed because the lesions were only limitedly visible on ct scans and had been diagnosed with positronemission tomography ( pet ) or scintigraphy before . 
holding your breath during rt ? were you anxious during treatment ? only for patients with respiratory gated delivery was it difcult to control the target by holding your breath ? was it disturbing to watch your tumor on the monitor ? how did you like the possibility to have an active role in controlling the duration of treatment ? very positive completely sufcient very friendly very short very comfortable in size very comfortable very easy very quiet very warm very warm did not occur easy to understand easy to do not at all not at all not at all very helpful very negative totally insufcient not friendly at all extremely long extremely narrow quite uncomfortable quite difcult very loud very cold very cold occurred very much very difcult to understand very difcult to do very much very much very much not helpful at all patients with centrally located pulmonary lesions were also treated on the mridian linac , as daily mri facilitated better distinction of the target volumes from the mediastinustereotactic body radiotherapy ( sbrt ) was applied in 20 patients ( 47% )  . 
total applied doses ranged from 4 to 66 gy , with single doses ranging from 2 to 15 gy . the mean number of fractions per patient was nine ( range 233 )  . 
for another 23 patients , mrgrt was initially foreseen but could not be performed due to different reasons ( see table 3 )  . gating was applied for all patients treated with sbrt ( n = 20 ) as well as for eight additional patients . 
for all patients , the mean treatment time ( time from start of acquisition of the rst mri sequence until completion of dose delivery ) amounted to 34 min , with a mean beam - on time of 2 : 17 mfor patients treated with gated radiotherapy , the mean treatment time amounted to 40 min , while a shorter mean treatment time of 24 min was observed if no gating was applied . 
the mean duty cycle for respiratory gated treatments , dened as the net beam - on time per fraction divided by the overall time when the system was ready to beam during this fraction , was 72% . 
in about 15% of all fractions , cine - mr during treatment indicated a patient shift which then required repetition of the 3d mr - scan and repositioning of the patient before treatment could be resumed . patient - reported outcomes completed questionnaires were available for 34 patients . 
patients mainly complained about the temperature in the room ( 24% ) and of some particular body parts ( 27% )  . furthermore , 18% of the patients experienced paresthesia during treatment and 12% rated the positioning as well as having to lie still for at least half an hour during treatment negatively ( score 4 )  . 
except for 4 patients with fatigue ctcae grade ii , no acute toxicity ctcae grade ii was detected . 11 patients did not describe any aggravation of pre - existing symptoms or the occurrence of new symptoms after rt . table 3 screening failures for mrgrt after mr simulation reason number ( n = 23 ) discussion poor general condition , breath - hold not sufcient distant progress evident in simulation mri no benet for gating , rotational imrt superior newly implanted metal implant or artifacts claustrophobia miscellaneous mri magnetic resonance imaging , imrt intensity - modulated radiotherapy mrgrt has been successfully introduced into clinical practice at our institution . 
this is important because aside from the technical difculties coming along with the integration of medical linear accelerators with mr scanners , the introduction of dedicated devices for mrgrt also implies new challenges for operating staff as well as patients . 
patients at the mr - linac are not only immobilized , but also need to 696 strahlenther onkol ( 2020 ) 196 : 691698 after the rst fraction ( n = 34 ) mean ( range ) at the end of treatment ( n = 34 ) mean ( range ) p - value table 4 results of the patient - reported outcome questionnaires how do you rate ... ... 
it is known that patients can experience claustrophobia and anxiety in an mr scanner [ 23 , 24 ] , and the rate usually increases with longer and narrower bore openings [ 23 , 25 ]  . 
due to the split - magnet design [ 14 ] , the mridian linac has a tunnel length of about 232 cm , which is longer than at contemporary diagnostic mr scanners and could potentially contribute to anxiety [ 25 ]  . 
while the absolute numbers of diagnostic mr scans terminated early due to claustrophobia or anxiety are generally small , in the range of 12% [ 24 ] , early termination of fractions in radiation therapy for this reason needs to be prevented as effectively as possible . in our cohort , all fractions could be administered safely , without patient - induced early terminations , and , as expected , without any treatment - related severe toxicities . the pro - q results shown in this manuscript conrm that treatment at the mr - linac is generally well tolerated by patients , which is in accordance with results previously published by tetar et al . 
compared to their rate of mr - related patient complaints of 29% , the value of 65% in our study is considerably higher , while , on the other hand , none of our patients reported considerable anxiety . the fact that despite a 65% complaint rate , mainly about temperature , paresthesia , and immobilization in general , the patients in our study still rated the total experience as at least tolerable , and that no patient reported considerable anxiety , might be due to the increased attention they receive from the mr - linac staff [ 27 , 28 ]  . 
mr simulation on the mr - linac seems to also help in the context of patient anxiety , as it allows patients to get acclimatized with the whole procedure [ 28 ]  . 
however , thorough patient screening is still necessary in order to avoid early treatment termination due to patient noncompliance . a limitation of this study is the relatively small number of patients . 
hence , the full potential of mri for target delineation ( particularly with the help of perfusionor diffusion - weighted images ) could not be exploited . furthermore , diagnostic planning mri sequences were not acquired in the treatment position , so that the co - registered images were only of limited use for target delineation , and deformable registration would have introduced additional uncertainties . 
in addition , future studies need to assess the question of which additional pulse sequences apart from the truefisp sequence are needed for low - eld mrgrt systems and how they compare to 1.5 t - systems [ 29 ]  . we have shown that mr - guided respiratory gating in breath - hold is feasible and , combined with a real - time austrahlenther onkol ( 2020 ) 196 : 691698 diovisual feedback system , was very well tolerated and appreciated by patients . 
cine - mr - enabled gating in breath - hold is also effective ; we observed a mean gating duty cycle of 72% , similar to the range of 67% to 87% published by van srnsen de koste et al . 
compared to their study , we have used slightly larger gating boundaries of up to 4 mm but , on the other hand , considerably smaller threshold - roi% values . 
apart from the paper by van srnsen de koste et al . [ 17 ] , a few phantom studies on the accuracy and inuencing factors of mr - guided gating using low - eld mrgrt systems have been published [ 30 , 31 ]  . 
however , the impact and different contributing effects still need to be studied using real patient data on a larger scale . besides respiratory gating , cine - mr - based structure tracking can also be used to monitor targets that do not move with respiration , for example the prostate . 
first published results show that this facilitates safe administration of mr - guided ultra - hypofractionated prostate treatments , potentially enabling margin reduction while eliminating the need for ducial or transponder implantation [ 32 ]  . a number of authors have reported on on - table adaption of treatment plans using mrgrt devices [ 11 , 3337 ] and also on assessing which patients benet most from adaptive mrgrt [ 35 , 3844 ]  . 
 [ 4 ] have reported on physician - rated organ at risk and target visualization in onboard mr compared to onboard cone - beam ct , and visualization in mri was rated better for 71% of all structures . 
there is a need for further evaluation of this aspect as well as for the opposing scenario , i.e. , online adaption of treatment plans using conventional igrt techniques . head - to - head comparative studies of ct - guided and mr - guided adaptive radiotherapy applying standard doses and fractionation might not be sufcient , as mr - guided adaptive radiotherapy allows for high - dose radiotherapy under circumstances in which treatment would not have been possible with conventional techniques [ 34 ]  . 
akbaba declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
juni 2020 der / die autor ( en ) 2020 ziel der arbeit phase - 2 - studien zeigten vielversprechende ergebnisse zur wirksamkeit einer induktionschemotherapie mit cisplatin in kombination mit gemcitabin bei patienten mit lokal fortgeschrittenen nasopharynxkarzinomen . die vorliegende analyse untersucht daher den einsatz dieser induktionschemotherapie , gefolgt von einer anschlieenden konkomitanten radiochemotherapie , die als alleinige behandlung den aktuellen therapiestandard darstellt . patienten und methode in dieser multizentrischen phase3 - studie wurden patienten mit histologisch gesicherten , lokal fortgeschrittenen nasopharynxkarzinomen eingeschlossen . 
die interventionsgruppe erhielt 3 zyklen induktionschemotherapie mit gemcitabin ( 1 g / m2 kof ( krperoberche ) , tage 1 und 8 ) und cisplatin ( 80 mg / m2 kof tag 1 ) q3w , gefolgt von einer radiochemotherapie ( rct ) mit cisplatin ( cisplatin 100 mg / m2 kof q3w ) in imrt - technik . 
primrer endpunkt war das rezidivfreie berleben ( rfs ) , das gesamtberleben ( os ) wurde als sekundrer endpunkt erhoben . ergebnisse in oben genannte analyse gingen insgesamt 480 patienten ein ( 242 patienten in der interventionsgruppe , 238 patienten in der standardgruppe )  . 
nach einem medianen nachbeobachtungszeitraum von 42 , 7 monaten zeigte sich das rfs nach 3 jahren mit 85 , 3 % in der gruppe mit induktionschemotherapie und 76 , 5 % in der standardgruporiginalpublikation zhang y , chen l , hu gq et al ( 2019 ) gemcitabine and cisplatin induction chemotherapy in nasopharyngeal carcinoma . 
11 , 4 % in der gruppe mit standardtherapie . schlussfolgerung der autoren der zustzliche einsatz der beschriebenen induktionschemotherapie , gefolgt von einer standardmigen rct verbessert das rezidivfreie berleben und das gesamtberleben signikant im vergleich zur alleinigen rct bei patienten mit lokal fortgeschrittenen nasopharynxkarzinomen . kommentar die simultane radiochemotherapie ( rct ) ist therapie der wahl zur behandlung von patienten mit fortgeschrittenem nasopharynxkarzinodurch die hinzunahme einer platinbasierten chemotherapie zur radiotherapie konnte eine relevante verbesserung des rezidivfreien berlebens ( rfs ) und des gesamtberlebens ( os ) erzielt werden [ 1 , 2 ]  . 
in einer groen metaanalyse aus dem jahr 2015 mit 19 randomisierten studien und insgesamt 4806 patienten zeigte sich eine verbesserung des 5 - jahres - berleben um 6 , 3 % [ 3 ]  . 
trotz etablierung der kombinierten rct und der verbesserung der bestrahlungstechniken durch einfhrung der imrt kam es bei knapp 1 / 4 der patienten zur fernmetastasierung nach 5 jahren [ 4 ]  . es stellte sich somit die frage , ob fr die gruppe der patienten mit hohem risiko eine weitere intensivierung der therapie zu einer verbesserung des onkologischen outcomes fhren kann . 
in der eortc 24971 / tax 323 zeigte der einsatz von tpf als induktionschemotherapie zwar ein lngeres os und rezidivfreies berleben , jedoch traten grad - 5 - toxizitten ( 5 , 5 % ) auf [ 8 ]  . 
die niederlndische condor - studie untersuchte tpf als neoadjuvante chemotherapie vor konventioneller rct oder kombinierter , akzelerierter radiotherapie mit cisplatdiese studie wurde vorzeitig beendet , da aufgrund der akuttoxizitt nur 32 % der patienten die verschriebene dosis von cisplatin im rahmen der anschlieenden rct erhalten konnten [ 9 ]  . wegen der insgesamt schlechten vertrglichkeit von tpf untersuchte man alternative chemotherapieprotokolle wie cisplatin und gemcitabeine phase - 2 - studie mit 2 zyklen reduzierter cisplatindosis ( 25 mg / m2 tage 13 ) und gemcitabin ( 1000 mg / m2 , tage 1 , 8 q3w ) zeigte nach 3 jahren eine niedrigere rate an grad - 3 - / - 4 - toxizitten , eine lokoregionre kontrollrate von 94 , 9 % , ein metastasenfreies berleben von 86 , 2 % und ein gesamtberleben von 87 , 7 % [ 10 ]  . 
im anschluss konnte bei 97 , 9 % eine simultane rct durchgefhrt werden , jedoch nur 63 von 239 ( 26 , 4 % ) der patienten erhielten in der interventionsgruppe die geplante kumulative dosis von 540 mg / m2 cisplatauch in der standardgruppe gab es deutliche abweichungen , denn nur 74 , 7 % der patienten erhielten die vorgesehenen 3 zyklen konkomitanter chemotherapie . 
95 , 8 % der patienten , die in die standardgruppe randomisiert wurden , erhielten mindestens 200 mg / m2 cisplatin konkomitant zur fazit im hinblick auf das onkologische outcome erscheint eine therapieintensivierung mit einer induktionschemotherapie vor der konkomitanten rct bei patienten mit nasopharynxkarzinomen sinnvoll . 
walter geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
wee cw et al ( 2015 ) locoregionally advanced nasopharyngeal carcinoma treated with intensity - modulated radiotherapy plus concurrent weekly cisplatin with or without neoadjuvant chemotherapy . radiat oncol j 33 ( 2 ) : 98108 3 . 
blanchard p et al ( 2015 ) chemotherapy and radiotherapy in nasopharyngeal carcinoma : an update of the mac - npc meta - analysis . lancet oncol 16 ( 6 ) : 645655 4 . 
lin jc et al ( 2003 ) phase iii study of concurrent chemoradiotherapy versus radiotherapy alone for advanced nasopharyngeal carcino742 strahlenther onkol ( 2020 ) 196 : 740742 ma : positive effect on overall and progression - free survival . 
sun y et al ( 2016 ) induction chemotherapy plus concurrent chemoradiotherapy versus concurrent chemoradiotherapy alone in locoregionally advanced nasopharyngeal carcinoma : a phase 3 , multicentre , randomised controlled trial . 
li wf et al ( 2019 ) concurrent chemoradiotherapy with / without induction chemotherapy in locoregionally advanced nasopharyngeal carcinoma : long - term results of phase 3 randomized controlled trial . 
driessen cm et al ( 2016 ) induction chemotherapy with docetaxel / cisplatin / 5 - uorouracil followed by randomization to two cisplatinbased concomitant chemoradiotherapy schedules in patients with locally advanced head and neck cancer ( condor study ) ( dutch head and neck society 08 - 01 ) : a randomized phase ii study . 
in general , it is an acutely resolved viral respiratory illness that presents with high - grade fever , cough and dyspnoea , with bilateral pneumonia on imaging [ 1 , 2 ]  . 
the plasma levels of cytokines like interleukins ( il2 , il7 , il10 ) , platelet - derived growth factor ( pdgf ) , vascular endothelial growth factor ( vegf ) , and tumour necrosis factor alpha ( tnf ) are usually elevated , with the levels being higher in patients who require intensive care or are categorised as having severe disease [ 1 ]  . 
nearly every sixth patient develops acute respiratory distress syndrome , which is predisposed by older age and known comorbid conditions , and which may worsen rapidly , leading to eventual death [ 2 ]  . 
management involves empirical and supportive therapy , but no standard of care has been established yet . historically , low doses of x - radiation were used in the rst half of the twentieth century to treat pneumonia , including viral pneumonia , with subjective response and objective resolution [ 3 ] based on the ability of low - dose radiation to induce an anti - inammatory phenotype [ 4 ]  . 
low - dose radiotherapy decreases expression of molecules for cell adhesion , produces anti - inammatory mediators like il10 and transforming growth factor beta 1 ( tgf - 1 ) , increases apoptosis , and secondarily reduces leucocyteendothelial cell interaction and vasodilation by inhibiting the expression of inducible nitric oxide synthase ( inos ) , which contributes to reduced nitric oxide levels [ 57 ]  . 
a single fraction of low - dose radiotherapy is cost and time effective and could potentially alleviate symptoms of respiratory distress quickly , helping to reduce mortality without signicant long - term sequelae . 
this , in turn , facilitates early discharge from hospital and reduces costs of in - patient hospitalisation , ultimately leading to better resource utilisation in the face of a global emergency . 
for a pandemic that originated in hubei , one can look to the chinese philosopher confucius for words of wisdom : study the past if you would dene the future . 
juni 2020 springer - verlag gmbh germany , part of springer nature 2020 fragestellung und hintergrund patienten mit einem lokal begrenzten prostatakarzinom , die unter bercksichtigung ihrer begleiterkrankungen und lebenserwartung von einer kurativen therapie protieren drften , knnen unter verschiedenen optionen whlen , wobei in der multidisziplinren beratung z . 
wie von der arbeitsgruppe der deutschen gesellschaft fr radioonkologie ( degro ) unter bercksichtigung internationaler richtlinien krzlich berichtet wurde , kann abhngig von der risikostratizierung eine kombination aus androgendeprivationstherapie ( adt ) und externer strahlenbehandlung indiziert sein [ 1 ]  . in einer aktuellen kanadischen studie wurden zwei unterschiedliche strategien bzw . 
sequenzen der kurz dauernden adt ( 6 monate ) verglichen , jeweils kombiniert mit einer dosiseskalierten strahlenbehandlung [ 2 ]  . material und methodik es wurde eine zweiarmige randomisierte phase - iii - studie durchgefhrt . 
in einem arm ( a ) bestand die behandlung aus 4 monaten neoadjuvanter adt , gefolgt von simultaner originalpublikation malone s , roy s , eapen l , choan e et al ( 2019 ) sequencing of androgen - deprivation therapy with external - beam radiotherapy in localized prostate cancer : a phase iii randomized controlled trial . 
die strahlenbehandlung erfolgte in 3 - d - konformaler technik ( bildgefhrt mit wchentlicher kontrolle , 76 gy in 38 fraktionen , davon 28 fraktionen , bei denen die proximalen 10 mm der samenblasen inkludiert waren )  . 
es konnte eine differenz von 15 % detektiert werden ( 90 % power , 2 - seitiges = 5 % )  . ergebnisse zwischen 2002 und 2012 wurden 432 patienten eingeschlossen . 
die tumorspezische letalitt war sehr gering ( 2 % nach 10 jahren )  . schlussfolgerung der autoren es wurden bezglich des primren und der sekundren endpunkte keine statistisch signikanten unterschiede gefunden , sodass sowohl die neoadjuvante und konkomitante adt ( arm a ) als auch die konkomitante und adjuvante adt ( arm b ) als akzeptabler therapiestandard angesehen werden kann . strahlenther onkol ( 2020 ) 196 : 738739 kommentar fazit die kanadische studie wurde mit einer langen nachbeobachtungszeit publiziert , wobei die abbildungen der kaplanmeier - kurven auch 15 - jahres - ergebnisse inkludieren . 
natrlich hatten sich in diesem langen zeitraum auch nderungen der strahlenbehandlungstechnik ergeben ( hhere przision , bessere schonung der risikoorgane , andere optionen der fraktionierung ; [ 3 , 4 ] )  . 
da die adt bekanntermaen auch unerwnschte nebenwirkungen mit sich bringt , gibt es bestrebungen , sie individualisierter als bisher einzusetzen ( 46 monate , zum teil auch alleinige strahlenbehandlung )  . am anderen ende des spektrums wird eine intensivierung der endokrinen therapie untersucht ( neuere substanzen , die aus der behandlung des kastrationsresistenten prostatakarzinoms kommen ) oder eine kombination mit klassischer chemotherapie . 
in diesen subgruppen wrde man auch auf die bedeutung des pet - stagings hinweisen , die gerade in einer randomisierten und hochrangig publizierten studie ( the lancet ) besttigt werden konnte [ 5 ]  . 
das nebenwirkungsprol war in beiden armen vergleichbar , allerdings bietet die konformale 3 - d - technik weniger mglichkeiten der rektumschonung als modernere verfahren , falls es denn eine relevante verkleinerung der prostata im neoadjuvanten arm gegeben hat . die studie besttigt die guten resultate nach kombinierter behandlung mit einem 10 - jahres - brfs von mindestens 80 % und einer tumorspezischen letalitt von 2 % . 
beck m , bhmer d , aebersold dm et al ( 2020 ) role of combined radiation and androgen deprivation therapy in intermediaterisk prostate cancer : statement from the degro working group on prostate cancer . 
malone s , roy s , eapen l et al ( 2020 ) sequencing of androgendeprivation therapy with external - beam radiotherapy in localized prostate cancer : a phase iii randomized controlled trial . 
martin jm , supiot s , keall pj et al ( 2018 ) moderately hypofractionated prostate external - beam radiotherapy : an emerging standard . br j radiol 91 : 20170807 4 . 
hofman ms , lawrentschuk n , francis rj et al ( 2020 ) prostate - specic membrane antigen pet - ct in patients with high - risk prostate cancer before curative - intent surgery or radiotherapy ( propsma ) : a prospective , randomised , multi - centre study . 
dearnaley d , syndikus i , mossop h et al ( 2016 ) conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : 5 - year outcomes of the randomised , non - inferiority , phase 3 chhip trial . 
august 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund und fragestellung bei der bestrahlung ( rt ) von patienten mit hno - tumoren ist eine radiogene belastung von speicheldrsen oft onkologisch unvermeidbar mit der folge von chronischer hyposalivation und xerostomie und der entsprechenden beeintrchtigung der lebensqualitt . 
mit der vorliegenden studie wurde prospektiv geprft , ob nach einer kurativen rt eine mechanische stimulation der restfunktion der speicheldrsen durch das regelmige kauen eines kaugummis einen klinisch signikanten effekt auf den verlauf der xerostomie hat . patienten und methode erfolgreich bestrahlte patienten mit histologisch nachgewiesenem oropharynxund mundhhlenkarzinom wurden fr die studie in einem zeitraum von 2 jahren gescreent . 
ausschlusskriterien waren ein bereits bestehender gebrauch von kaugummi und eine vollprothese . die patienten wurden 2 : 1 randomisiert ( nach stratikation fr alter und tumorlokalisation ) in die interventionsgruppe ( arm a : 5 - mal tglich kauen eines studienkaugummis fr mindestens 5 min zustzlich zu den vorher durchgefhrten manahmen fr die xerostomie ) vs . 
beobachtungsgruppe. in dieser wurde der vor studieneinschluss gewohnte georiginalpublikation killerup kaae j , stenfeldt l , hyrup b et al ( 2020 ) a randomized phase iii trial for alleviating radiation - induced xerostomia with chewing guradiother oncol 142 : 7278 ( cid : 2 ) med . 
30 , 26655 westerstede , deutschland 2 klinik fr strahlentherapie und spezielle onkologie , medizinische hochschule hannover , hannover , deutschland brauch von wasser , speichelersatz oder anderen speichelstimulanzien weitergefhrt . 
der geschmacklose und zuckerfreie kaugummi war zuvor in einer pilotstudie zusammen mit betroffenen patienten entwickelt und getestet worden hinsichtlich gre ( 1 g ) , weicher textur und effektivitt [ 1 ]  . er enthielt keine pharmakologischen wirkstoffe . 
die studiendauer betrug einen monat . primrer endpunkt der studie war eine vernderung des xerostomiescores im eortc quality of live questionnaire head and neck 35 ( qlq - h&n35 ) , explizit der frage 41 did you have a dry mouth ? , kategorisiert in reductions in symptoms , no change und increase in symptoms . 
weiterhin wurde die vernderung der viskositt des speichels nach der 5 - mintigen stimulation untersucht . ergebnisse zwischen 2016 und 2018 wurden 257 patienten in dnischen zentren gescreent , von denen 109 in die studie aufgenommen und randomisiert werden konnten , 68 in arm a , 41 in den kontrollarm b . 
die drop - out - rate ber die studiendauer von einem monat betrug 17 % . klinische , pathologische und therapieassoziierte charakteristiken und risikofaktoren waren in beiden gruppen gleich verteilt , ebenfalls fanden sich keine signikanten unterschiede in der mittleren dosisbelastung der risikostrukturen parotis , submandibularis und mundhhle . die patienten waren im mittel ca . 
61 jahre alt , zu > 65 % mnnlich , in fast 40 % nichtraucher und berwiegend instrahlenther onkol ( 2020 ) 196 : 10581061 1059 nerhalb der 2 jahre vor studieneinschluss an einem hpvassoziierten oropharynxkarzinom erkrankt . 
6 % der patienten eine symptomverschlechterung . bei den anderen qol - werten des h&n35 schlucken zeigten sich keine signikanten unterschiede zwischen gruppe a und der kontrolle b whrend der studiendauer . die scores fr essen im sozialen kontext verbesserten sich in beiden gruppen signikant , whrend die werte fr zhssigen speichel nur in der gruppe a signikant abnahmen . 
in der kontrollgruppe blieben hingegen die werte im wesentlichen unverndert . allerdings zeigten sich keine signikanten unterschiede beim vergleich der jeweiligen items zu den prspezizierten zeitpunkten zwischen beiden studiengruppen . die objektiven speichelussmessungen zeigten in beiden gruppen durch die kaugummistimulation einen deutlichen anstieg . 
hnliche effekte wurden fr die viskositt des speichels beobachtet : durch die stimulation reduzierte sich diese signikant , doch zeigten sich nach 4 wochen kaugummi keine relevanten statistischen vernderungen in der unstimulierten oder stimulierten zusammensetzung . schlussfolgerungen der autoren in der subjektiven erfassung der mundtrockenheit wurde eine signikante linderung durch den regelmigen gebrauch der kaugummis gezeigt . 
insgesamt lindert die verwendung eines solchen geschmacksund zuckerfreien kaugummis die xerostomiesymptomatik nach rt deutlich . kommentar in der therapie der die lebensqualitt deutlich einschrnkenden xerostomie nach rt sind verschiedene wege gegangen worden : eine direkte radioprotektion durch den radikalfnger amifostin ist mehrfach untersucht worden , da sich dieser wirkstoff bevorzugt in den speicheldrsen anreichert . 
zwar ist amifostin als kurzinfusion 1530 min vor der tglichen bestrahlung in dieser indikation zugelassen , jedoch fand ein aktuelles cochrane - review ber 11 studien nur eine geringe evidenz fr eine langfristige schonung der speicheldrsen [ 2 ]  . 
fr akupunktur ergab sich dabei bei schwacher evidenzlage eine geringe stimulation des speichelusses , jedoch zeigten sich auf demselben evidenzniveau keine unterschiede zwischen akupunktur und placeboakupunktur in hinblick auf mundtrockenheit . 
auch fr eine elektrostimulation wurde keine ausreichende evidenz gefunden . als hilfsmittel sind seit den 1970er - jahren speichelersatzlsungen ( knstlicher speichel ) entwickelt worden , die mglichst alle funktionen des natrlichen speichels ersetzen sollen ( nachhaltiges benetzen der schleimhute und zhne , regulation des ph - werts , reduktion der vulnerabilitt der oralen schleimhute [ 4 ] )  . 
aber auch mit diesen mitteln ist jeweils nur eine kurzfristige linderung der xerostomie zu erzielen . vor diesem hintergrund ist der versuch der nichtpharmakologischen stimulation der restfunktion der speicheldrsen mithilfe von kaugummikauen hoch interessant . 
schon seit den 1990er - jahren hatte sich gezeigt , dass sich das kauen zuckerfreier kaugummis gnstig auf die salivation und die mundhygiene ( kariesprvention ) bei unter xerostomie leidenden menschen auswirkt [ 5 ]  . 
fr das sjgren - syndrom oder andere rheumatische erkrankungen ( bersicht in der hier kommentierten studie )  . tatschlich hat es dann aber 20 jahre gedauert bis der versuch unternommen wurde , diese mechanische stimulation der restsalivation auch bei xerostomie nach einer kurativ intendierten rt einzusetzen . 
auf den ersten blick ist dieses zgern verstndlich : bei oft schlechtem zahnstatus , bei empndlicher und schmerzhafter oraler schleimhaut aufgrund von aphten und anderen lsionen , bei trockenem mund und zhssigem speichel erscheint die aufforderung zum regelmigen gebrauch eines kaugummis a priori wenig plausibel . 
neben diversen anderen studienbedingten und onkologischen ursachen mag dabei auch eine rolle gespielt haben , dass viele patienten das regelmige kauen als zu schmerzhaft oder unmglich empfunden haben . bei den patienten , denen eine teilnahme mglich war , fhrte der kaugummi zu einer signikanten reduktion der subjektiven xerostomie , wobei sich objektiv durch fnfmintiges kauen eine deutliche induktion des speichelusses bei verbesserung der viskositt nachweisen lie . 
auf der anderen seite stieg der anteil der patienten mit dem subjektiven eindruck einer symptomverschlechterung auf 13 % mit kaugummi an , whrend er in der kontrollgruppe mit 6 % nur halb so hoch lag . 
h. , dass bei einem nicht geringen anteil der patienten whrend des kauens mehr speichel bentigt wird , die restkapazitt der speichelproduktion aber nicht ausreicht , was zu einem besonderen leiden unter dem symptom mundtrockenheit fhrt . 
dabei wird die restfunktion der speicheldrsen durch das kauen direkt und effektiv angeregt . ( cid : 2 ) langfristige und nachhaltige vernderungen in der speichelussrate und der viskositt sind nach nur einem monat der anwendung noch nicht zu erwarten . ( cid : 2 ) von dieser therapie kann nur ein teil der patienten protieren , da viele das kaugummikauen a priori nicht tolerieren und bei einigen von ihnen auch die beschwerden der xerostomie verstrkt werden knnen . robert michael hermann , westerstede , und hans christiansen , hannover interessenkonikt r.m. 
kaae jk , stenfeldt l , eriksen jg ( 2016 ) xerostomia after radiotherapy for oral and oropharyngeal cancer : increasing salivary ow with tasteless sugar free chewing gufront oncol 6 : 111 2 . 
furness s , bryan g , mcmillan r et al ( 2013 ) interventions for the management of dry mouth : non - pharmacological interventions . cochrane database syst rev 8 : cd9603 strahlenther onkol ( 2020 ) 196 : 10581061 1061 4 . 
aagaard a , godiksen s , teglers pt et al ( 1992 ) comparison between new saliva stimulants in patients with dry mouth : a placebo - controlled double - blind crossover study . 
there was no correlation between the occurrence of acute and late toxicity . conclusion with proper technique , a combined approach using ebrt and hdrebt was associated with acceptable toxicity in medically inoperable rectal cancer patients . keywords high dose rate endorectal brachytherapy rectal cancer medically inoperable toxicity rectal brachytherapy introduction total mesorectal excision with or without neo - adjuvant ( chemo - ) radiation is the standard of care in rectal cancer patients [ 1 ]  . 
palliative external beam radiotherapy ( ert ) is often offered as an alternative ; however , the treatment effect is disappointing [ 4 ]  . ( cid : 2 ) cl chiang chiangcl@hku.hk kong , china hong kong , china hong kong , china china china 1 department of clinical oncology , tuen mun hospital , hong 2 department of clinical oncology , university of hong kong , 3 department of clinical oncology , queen mary hospital , 4 department of surgery , tuen mun hospital , hong kong , 5 department of surgery , queen mary hospital , hong kong , 6 clinic for radiation oncology , university hospital essen , essen , germany radiation dose escalation has been shown to improve local control in patients who received nonsurgical treatment [ 5 ]  . 
high - dose - rate endorectal brachytherapy ( hdrebt ) is a promising technique to provide very high dose radiation to the tumor with limited radiation to nearby normal tissue [ 6 ]  . 
in a recently published phase i trial , a promising response rate of ~90% was noted but the late grade 3 + toxicity was reported in 40% of patients [ 7 ]  . 
this manuscript reviewed the safety prole of 18 patients who received this combined external and internal radiotherapy . patients and methods patients data of patients who were treated with combined ert and hdrebt boost at tuen mun hospital and queen mary hospital were collected in a prospective database . 
1 plan from the oncentra treatment planning system ( elekta ab , stockholm , sweden ) in axial , sagittal and coronal views shows the applicator in situ ( top panels )  . 
double brachy - balloon technique ( bottom panel ) was developed to move the target volume away from the high - dose gradient and to compress the thickness of the target while displacing the contralateral normal mucosa away from high dose tologically conrmed adenocarcinoma of rectum who were medically unt for operation . 
the tumors had clinical stage t2 - 4n0 - 2 and were located ( cid : 2 ) 12 cm from the anal verge . exclusion criteria were tumor below dentate line , circumferential involvement > 270 , prior history of radiation to pelvis , or surgery to rectal cancer , eastern cooperative oncology group ( ecog ) performance status > 2 , or life expectancy < 6 months . 
pretreatment evaluation included digital rectal examination , endoscopy , computed tomography ( ct ) of the thorax and abdomen , and magnetic resonance imaging ( mri ) of the rectum . treatment external beam radiotherapy patients underwent computed tomography ( ct ) conformal planning . 
dose distribution was in accordance with the recommendations of the international commission on radiation units and measurements report 62 [ 8 ]  . brachytherapy high - dose - rate endorectal brachytherapy ( hdrebt ) was started at 8 weeks upon completion of ert . 
we performed mri and endoscopic assessment of tumor status at a week prior to hdrebt ; markers will be placed via endoscope at tumor borders to guide the target contouring . 
all patients were planned on oncentra treatment planning system version 4.5.3 ( elekta ab , stockholm , sweden ) for delivery on the microselectron hdr 192 - iridium remote after - loader ( elekta , veenendaal , the netherlands )  . 
organs - at - risk including normal rectal mucosa , strahlenther onkol ( 2020 ) 196 : 993997 table 1 patient , tumor , treatment , and dosimetric characteristics table 1 ( continued ) patient characteristics median age in years ( range ) male female performance status ecog 01 ecog 2 ecog 3 charlson comorbidity score comorbidities cardiovascular pulmonary long - term anti - coagulant use tumor characteristics tnm classication t3n0m0 t3n1m0 t3n2m0 t2n0 / n + m0 distance from anal verge 05 cm > 510 cm mrf status mrf > 1 mm mrf ( cid : 2 ) 1 mm degree of circumferential involvement ( cid : 2 ) 180 > 180270 81.5 ( 7095 ) 12 ( 66.7 ) 6 ( 33.3 ) 0 ( 0 ) 10 ( 55.6 ) 8 ( 44.4 ) 9 ( 50.0 ) 9 ( 50.0 ) 14 ( 77.8 ) 1 ( 5.6 ) 1 ( 5.6 ) 6 ( 33.3 ) 9 ( 50 ) 2 ( 11.1 ) 1 ( 5.6 ) 4 ( 22.2 ) 14 ( 77.8 ) 8 ( 50% ) 8 ( 50% ) 11 ( 61.1 ) 7 ( 38.9 ) bladder , and small bowel were also contoured . 
at least 95% of the gtv volume should receive the prescribed dose and no mucosal dose was allowed to exceed 30 gy per fraction . in the present study , 6 patients were treated with 1 , 2 , or 3 weekly fraction ( s ) of 10 gy boost , respectively . evaluation we prospectively followed patients at 3 months , 6 months , and then every 6 months after hdrebt . 
median age was 82 years ( range 7095 years ) ; 8 ( 44.4% ) and 9 ( 50% ) patients had ecog 3 performance score and charlson comorbidity score 3 , respectively . 
median eqd2 ( / = 10 gy ) delivered was 66 gy10 ( range 4892 gy10 )  . details of patient , tumor , treatment , and dosimetric characteristics are shown in table 1 . 
first , the depth of hdrebt prescription as deep as 2 cm was allowed in the dutch reported series , which resulted in the very high dose ( 60 gy ) to the mucosa . 
on the other hand , we limited the mucosa dose to 30 gy per fraction and the prescription depth rarely was > 1 csecond , we deployed the double balloon technique : the rst balloon served to push the contralateral rectal mucosa away from the high - dose region , while the second balloon ( on tumor side ) displaced the target volume away from the high dose gradient , also it further compressed the thickness of the target volume . 
taken together , the dose to the mucosal front of the tumor received a much lower dose in our cohort than that in the herbert trial , which may explain the better toxicity prole in our communication . 
the retrospective nature of our series may lead to underreporting of toxicities ; despite the data being retrieved from a prospectively collected database , the bias cannot be entirely eliminated . 
indeed , our series was limited by the retrospective nature , small sample size , short follow - up time , and heterogeneous dose - fractionation regime . another promising technique of dose escalation is the use of low - energy ( 50 kv ) contact x - ray ( cxr ) therapy ( papillion treatment ) [ 10 ]  . 
recent data also suggested cxr boost for residual tumor could achieve excellent clinical response and low local regrowth rate , and thus provide an alternative strategy for patients who are unt or refuse surgery [ 12 ]  . 
yet , one of the major challenges for papillion treatment is related to its collimator design which limits its application to only small ( < 5 cm ) and distal tumors . 
comparatively , the multichannel rectal applicator allowed us to adapt the dose distribution better to individual tumors and to treat tumors larger in length . strahlenther onkol ( 2020 ) 196 : 993997 conclusion with proper radiation technique and patient selection , combined ebrt and hdrebt was associated with acceptable toxicity in medically inoperable rectal cancer patients . 
our ndings suggest the importance of limiting the mucosal dose with the aim to reduce the late toxicity . funding sources this research did not receive any specic grant from funding agencies in the public , commercial , or not - for - prot sectors . ethical consideration conict of interest c.l. 
endpoints included cumulative incidence of severe toxicity , locoregional recurrence - free survival ( lrrfs ) , progression - free survival ( pfs ) , and overall survival ( os )  . 
hazard ratios ( hrs ) were pooled in the meta - analysis using the random - effects model . results six studies of eight cohorts were included in the quantitative synthesis . 
bt allows for the delivery of a high dose of radiation to the cervical tumor while sparing the adjacent organs at risk ( oar ) due to the steep dose fall - off . 
grade 3 or 4 toxicity following 2d - bt has been reported to range from 5 to 30% for bowel and bladder domains [ 24 ]  . new methods that take advantage of computed tomography ( ct ) or magnetic resonance imaging ( mri ) have been used to develop three - dimensional image - guided bt ( 3dbt )  . 
gec - estro evaluated 3d - bt in locally advanced cervical cancer in an international study ( image - guided intensity - modulated external beam radiochemotherapy and mri - based adaptive brachytherapy in locally advanced cervical cancer , embrace )  . 
also , a prospective trial comparing 2d - bt and 3d - bt , the french soutien aux techniques innovantes et coteuses ( stic ) , concluded that 3d - bt improved local control with half the toxicity observed with 2d - bt [ 8 ]  . 3d - bt has been broadly adopted in the radiation oncology eld for treatment of cervical cancer [ 9 ]  . 
however , only a limited number of centers perform 3d - bt in korea , and even more , 2d - bt is only available in 32.5% of radiation oncology centers in korea . 
due to the low national health insurance reimbursement , most bt centers suffer a decit for operating bt , and the proportion of centers offering bt has decreased since 2006 . 
to foster the wide utilization of 3d - bt in korea , we performed a systematic review and meta - analysis to evaluate the impact of 3d - bt on toxicity and survival compared to that of 2d - bt in cervical cancer patients . methods the present systematic review and meta - analysis followed the preferred reporting items for systematic reviews and meta - analyses ( prisma ) guidelines [ 11 ]  . 
the research question of the present meta - analysis was as follows : would 3d - bt reduce severe toxicity and improve survival outcomes compared to those of 2d - bt in patients with cervical cancer ? literature search pubmed and embase databases were searched up to april 16 , 2019 . 
the references of retrieved articles were also checked to search the additional relevant studies . the inclusion criteria were based on the patient / intervention / comparator / outcome / study design ( picos ) criteria [ 11 ] : ( 1 ) patients with cervical cancer ; ( 2 ) 3d - bt as the intervention ; ( 3 ) 2d - bt as the comparator ; ( 4 ) cumulative incidence of severe toxicity ( grade 3 ) , locoregional recurrence - free survival ( lrrfs ) , progression - free survival ( pfs ) , and overall survival ( os ) as outcome ; and ( 5 ) study design as original articles or brief report . 
the exclusion criteria were as follows : ( 1 ) not in the eld of interest , ( 2 ) containing information on single bt technique , and ( 3 ) planning study without clinical information . data extraction and quality assessment a standardized form was used to extract ( 1 ) study characteristics including rst author , year of publication , institution , the period of enrollment , study design ( prospective or retrospective / consecutive enrollment ) , number of groups , and number of patients ; ( 2 ) clinicopathological characteristics including age , pathology , stage , toxicity scoring system , and follow - up period ; and ( 3 ) treatment characteristics instrahlenther onkol ( 2020 ) 196 : 973982 cluding the aim of radiotherapy ( denitive or perioperative ) , rate of concurrent chemotherapy , dose / technique of external beam radiotherapy ( ebrt ) , the modality of 3d image guidance , use of interstitial bt , and rate / dose of bt . 
if published articles did not provide data for quantitative analyses , we contacted the authors individually . the methodological quality of included studies was assessed using the quality in prognostic studies ( quips ) tool [ 12 ]  . 
severe toxicity was dened as an adverse event grade 3 using common terminology criteria for adverse events ( ctcae ) or radiation therapy oncology group and the european organization for research and treatment of cancer ( rtog / eortc ) criteria . 
except for these two cohorts , the others included in the quantitative synthesis had rt for denitive ainevertheless , we included these preoperative groups for this analysis and provided a supplementary le in which these cohorts were excluded . 
we included these results in the meta - analysis , but 8% of the patients in the imrt / 3d - bt arm actually received 2d - bt with imrt . 
as the majority of patients included in the other ve studies did not use needles for 3d - bt , we included the cohort without needles for the 3d - bt arm ( n = 60 )  . 
the shortest follow - up period was about 24 months in two studies [ 8 , 20 ] , while the others reported follow - up times over 44 months . 
the sole excluded study was charra - brunaud et al . , because of the paucity of data for meta - analysis ; they reported similar os between the 2d - bt and 3d - bt groups ( p = 0.27 ) [ 8 ]  . pooled hr of 3d - bt compared to 2d - bt was 0.65 ( 95% ci 0.401.06 ) , and moderate heterogeneity was found ( i2 = 66% )  . 
although half of the six studies were not included for meta - analysis of toxicity , the excluded studies also reported meaningful reductions of grade 3 toxicity in 3dbt patients . 
regarding prognostic factor measurement , one study had a moderate risk of bias as it did not report continuous variables for age , follow - up time , or information on major clinicopathological factors such as pathology and ebrt dose [ 20 ]  . 
3 forest plots for hazard ratios comparing 3d - brachytherapy ( 3d - bt ) to 2d - brachytherapy ( 2d - bt ) regarding a cumulative incidence of severe toxicity , b locoregional recurrence - free survival , c progression - free survival , d and overall survival . 
ci condence interval , hr hazard ratio , te estimated treatment effect , sete standard error of treatment estimate studies evaluating mri - based 3d - bt have shown favorable results . 
the 2 - year actuarial probability of severe vaginal morbidity was 3.6% , which was less than has been reported from earlier studies of ~30% [ 4 , 23 ]  . 
likewise , late severe rectal toxicities were rare ( 1.7% ) and strongly related to dosimetric parameters ( e.g. , d2cm3 ) which were available through 3d image guidance [ 24 ]  . 
the incidence of women diagnosed with cervical cancer in their 20s increased from 1993 through to 2002 [ 25 ] , and the younger population tends to be more affected by severe toxicity owing to their long life expectancy , so the rapid introduction of 3d - bt should be promoted . lrrfs was also considerably improved with 3d - bt , and this might contribute to the improvement of pfs . 
4 funnel plots representing hazard ratios of brachytherapy technique ( 3d versus 2d ) regarding a cumulative incidence of severe toxicity , b locoregional recurrence - free survival , c progression - free survival , d and overall survival hort . 
a recent embrace report also found that the nodal failure rate after concurrent chemoradiotherapy and 3d - bt was 11% , with a median follow - up time of 34 months , one quarter of which was diagnosed with simultaneous local recurrence [ 27 ]  . the present study failed to show improvement of os in patients treated with 3d - bt compared to 2d - bt . 
the guideline from the american brachytherapy society recommends high - dose - rate interstitial bt for patients with bulky tumors , a narrow vaginal apex , inaccessible cervical os , tumor invasion into the lateral parametria or pelvic sidewall , and extension into the lower vagina [ 28 ]  . 
interstitial bt could be more widely used and could lead to improvement of os . in addition , ~40% of patients included in the present meta - analysis received ct - based 3d - bt . 
mri provides superior soft tissue delineation compared to ct , so that there has been a concern that target volume might differ between ct and mri [ 29 , 30 ]  . 
increasing the use of mri - based brachytherapy could also lead to improvement of survival and toxicities . the use of 3d - bt does carry added cost compared to 2d - bt . 
not only costs for cross - sectional imaging , but also additional time , availability of imaging machines , and longer planning time should be taken into consideration . therefore , cost - effectiveness could be another issue . 
a costeffectiveness analysis performed in the us using a markov state - transition model based on 3 - year survival estimates and severe complication rates from previous studies concluded that 3d - bt is a cost - effective option compared to 2d - bt , and supported routine use of 3d - bt in locally advanced cervical cancer [ 31 ]  . 
although the exact costs differ between the united states and korea , the result suggests that the adoption of 3d - bt could save medical costs . with growing evidence , 3d - bt is becoming a new standard worldwide . 
in the us there was an increased percentage of using ct for bt from 55 to 95% or mri for bt from 2 to 34% between 2007 and 2014 [ 32 ]  . 
a 2015 survey in japan found that only 16% of facilities had adopted 3d - bt , but 53% of facilities had plans to adopt 3d - bt in the future [ 33 ]  . 
bt could be applied to other cancers in addition to cervical cancer , such as for malignancies in the prostate , breast , head and neck , respiratory tract , and digestive organs . 
furthermore , the number of studies for meta - analysis was small , and due to the lack of provided data , only three studies were included for meta - analysis of the cumulative incidence of toxicity and pfs . 
meta - regression analysis could be used to evaluate the impact of these factors ; however , this was impossible in the present study due to the limited number of studies and available data . 
eine niederlndische randomisierte studie von al - mamgani und kollegen verglich in diesem kontext zwei radiotherapieregime . lokal patienten und methodik es handelt sich um eine zweiarmige phase - iii - studie an 6 niederlndischen zentren . fortgeschrittenes oder einschlusskriterien waren : fernmetastasiertes plattenepithelkarzinom des oropharynx , hypopharynx oder larynx , ein guter allgemeinzustand ( ecog 02 ) und keine indikation fr eine kurativ intendierte lokaltherapie . 
primrer endpunkt war die zeit bis zur lokoregionren originalpublikation al - mamgani a , kessels r , verhoef cg et al ( 2020 ) randomized controlled trial to identify the optimal radiotherapy scheme for palliative treatment of incurable head and neck squamous cell carcinoma . 
whrend das mediane progressionsfreie berleben 5 monate beziehungsweise 8 monate betrug , lag das mediane gesamtberleben in arm 1 bei knapp 9 monaten und in arm 2 bei knapp 15 monaten ( p = 0 , 2 )  . 
aufgrund der geringeren toxizittslast und statistisch nicht signikant unterschiedlichen onkologischen ergebnisse strahlenther onkol ( 2020 ) 196 : 10621064 1063 knnte das kurzzeitregime ( 6 6 gy ) jedoch gegenber dem langzeitregime ( 16 3 , 125 gy ) favorisiert werden . kommentar patienten mit einem kopf - hals - tumor ohne kurative option berleben im median weniger als ein jahr [ 1 ]  . 
al - mamgani und kollegen sind in ihren bemhungen zu beglckwnschen , diese lcke zu schlieen . ihre randomisierte phase - iii - studie verglich ein kurzzeitregime ( 6 6 gy ) mit einem langzeitregime ( 16 3 , 125 gy ) zur palliativen radiotherapie von kopf - hals - tumoren . mehrere aspekte lassen es lohnenswert erscheinen , diese studie nher zu reektieren . erstens wurde die studie frhzeitig abgebrochen . 
dies veranschaulicht deutlich , wie schwierig es ist , in dieser therapiesituation randomisierte strahlentherapeutische studien durchzufhren , und knnte ein spiegel der groen heterogenitt bei begrenzter fallzahl sein . zweitens bertrifft das erreichte mediane gesamtberleben von 9 bzw . 
der gute allgemeinzustand der eingeschlossenen patienten ( 75 % ecog 01 ; 25 % ecog 2 ) knnte dies begrnden ; er deckt sich allerdings nur zum teil mit unseren eigenen alltglichen klinischen erfahrungen . 
ein weiterer gesichtspunkt : eine simultane systemtherapie zur radiotherapie war im protokoll zwar nicht vorgesehen ; inwieweit jedoch eine anschlieende chemound / oder immuntherapie eingesetzt wurde und das berleben beeinusst haben knnte , wird in der publikation nicht berichtet . auch wenn die statistische auswertung bei 34 patienten rein deskriptiv ist , zeigte sich drittens zwar ein numerischer vorteil im langzeitregime bezglich lokaler kontrolle und gesamtberleben , dieser war jedoch statistisch nicht signikant . 
letzteres wre wichtig , um den wert der palliativen radiotherapie von kopf - hals - tumoren zu sichern , der zum teil bereits infrage gestellt worden ist [ 10 ]  . 
aus diesem grund haben wir eine prospektive multizentrische beobachtungsstudie mit dem primren endpunkt der gesundheitsbezogenen lebensqualitt initiiert ( drks00021197 )  . fazit zusammenfassend liegen die herausforderungen in der palliativen radiotherapie von kopf - hals - tumoren in dem heterogenen patientenkollektiv und der individuell abzuwgenden balance zwischen toxizitt und antineoplastischer effektivitt . 
krug erhielt honorare von merck sharp & dome . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
burtness b , harrington kj , greil r et al ( 2019 ) pembrolizumab alone or with chemotherapy versus cetuximab with chemotherapy for recurrent or metastatic squamous cell carcinoma of the head and neck ( keynote - 048 ) : a randomised , open - label , phase 3 study . 
lokker me , offerman mpj , van der velden l - a et al ( 2013 ) symptoms of patients with incurable head and neck cancer : prevalence and impact on daily functioning . 
mayland cr , ingareld k , rogers sn et al ( 2020 ) disease trajectories , place and mode of death in people with head and neck cancer : ndings from the head and neck 5000 population - based prospective clinical cohort study . 
shahid iqbal m , kelly c , kovarik j et al ( 2018 ) palliative radiotherapy for locally advanced non - metastatic head and neck cancer : a systematic review . 
fortin b , khaouam n , filion e et al ( 2016 ) palliative radiation therapy for advanced head and neck carcinomas : a phase 2 study . int j radiat oncol biol phys 95 : 647653 . 
al - mamgani a , tans l , van rooij phe et al ( 2009 ) hypofractionated radiotherapy denoted as the christie scheme : an effective means of palliating patients with head and neck cancers not suitable for curative treatment . 
candias6 received : 12 february 2020 / accepted : 12 may 2020 / published online : 9 june 2020 the author ( s ) 2020 abstract background in this exploratory study , the impact of local irradiation on systemic changes in stress and immune parameters was investigated in eight patients treated with intensity - modulated radiation therapy ( imrt ) or stereotactic ablative body radiotherapy ( sabr ) for prostate adenocarcinoma to gain deeper insights into how radiotherapy ( rt ) modulates the immune system . patients and methods rt - qpcr , ow cytometry , metabolomics , and antibody arrays were used to monitor a panel of stressand immune - related parameters before rt , after the rst fraction ( sabr ) or the rst week of treatment ( imrt ) , after the last fraction , and 3 weeks later in the blood of imrt ( n = 4 ) or sabr ( n = 4 ) patients . 
effect size analysis was used for comparison of results at different timepoints . results several parameters were found to be differentially modulated in imrt and sabr patients : the expression of tgfb1 , il1b , and ccl3 genes ; the expression of hla - dr on circulating monocytes ; the abundance and ratio of phosphatidylcholine and lysophosphatidylcholine metabolites in plasma . 
more immune modulators in plasma were modulated during imrt than sabr , with only two common proteins , namely gdf - 15 and tim - 3 . conclusion locally delivered rt induces systemic modulation of the immune system in prostate adenocarcinoma patients . imrt and sabr appear to specically affect distinct immune components . keywords immunophenotyping ionizing radiation biomarkers of radiation exposure prostate cancer systemic immune modulation b . 
grenoble alpes , inserm , cea , irig - bci - umr_s1036 , 38054 grenoble , france 8 national public health center , 1097 budapest , hungary 3 maria sklodowska - curie national research institute of oncology , gliwice branch , 44 - 102 gliwice , poland 9 hq science limited , 5 the quay , pe27 5ar st . 
intensity - modulated radiation therapy ( imrt ) and stereotactic ablative body radiotherapy ( sabr ) are used to perform a more precise irradiation of the tumor volume [ 2 ]  . 
rt has long been regarded as local therapy , but this point of view changed when data on systemic effects of locally delivered radiation were collected [ 3 ]  . 
these bioindicators include genes such as fdrx ( coding for ferredoxin reductase , a mitochondrial protein involved in electron transport ) , ddb2 ( coding for the damage - specic dna binding protein 2 , involved in dna repair ) , mdm2 ( coding for the mouse double minute 2 proto - oncogene , involved in the regulation of p53 degradation ) , and sesn1 , gadd45 , and ccng1 ( coding , respectively , for the sestrin 1 protein , the growth arrest and dna damage - inducible protein 45 , and the cyclin g1 protein , involved in the inhibition of cell cycle and growth arrest in stressful conditions )  . 
interestingly , the expression of some inammatory genes such as arg1 ( coding for arginase 1 , involved in amino acid metabolism and cell proliferation ) , bcl2l1 ( coding for a protein of the bcl2 family , involved in the control of apoptosis ) , and myc ( coding for the myc proto - oncogene , involved in cell cycle progression , apoptosis , and cellular transformation ) is also found to be dysregulated [ 8 ]  . 
tumor cells can , for example , up - regulate their expression of immune checkpoint molecules such as programmed death ligand 1 ( pd - l1 ) , making them , e.g. , less susceptible to killing by cytotoxic t lymphocytes . 
it has been proposed that the anti - tumor efciency of rt can benet from a synergy of concomitant re - activation of the immune system [ 1113 ]  . systemic effects of ionizing radiation could also be observed at the level of the proteome , including cytokines , and metabolome in the blood of cancer patients treated with rt [ 14 ]  . 
early changes in the plasma level of a collection of cytokines were , for example , associated with toxicity in patients treated for lung cancer , and this response was modied by the combination of chemotherapy with rt [ 15 ]  . 
the intensity of radiation - induced toxicity , including the inammatory response , is one key factor affecting rt - related changes in the blood proteome [ 16 ]  . 
rt - related changes could be also detected in the serum lipidome and dynamic radiation - induced changes in the levels of phosphatidylcholines ( pcs ) and lysophosphatidylcholines ( lpcs ) were observed in patients treated for head and neck cancer [ 17 ]  . 
lpcs are pro - inammatory lipids involved in atherosclerosis [ 18 ] and an increased plasma lpc / pc ratio has been reported in certain pro - inammatory conditions [ 19 ]  . 
it was recently reported that the lpc / pc ratio increased in the serum of whole - body - irradiated mice [ 20 ]  . hence , this parameter represents a potential inammationrelated metabolomic marker of the response to radiation . 1020 strahlenther onkol ( 2020 ) 196 : 10181033 however , only few data exist on joint analyses of the manifold stress and immune changes that might occur following local treatment of solid tumors such as prostate adenocarcinoma . 
such information could shed further light on how a distinct rt scheme impacts at the systemic level and might help to improve multimodal therapies in the future . in this exploratory study , we therefore complementarily analyzed the expression of stress - response and inammatory cytokine genes , the modulation of immune cell populations , changes in metabolites , and changes in cytokines levels in the blood of a group of 8 patients undergoing rt for prostate adenocarcinoma . 
as a rst attempt to nd out whether modulation of these parameters at the systemic level depends on factors such as the irradiated volume , the dose delivered per fraction , the dose rate , and the total dose received , biomaterial of patients who were treated with two markedly different rt modalities , namely imrt and sabr , was used for the analyses . materials and methods patients and rt treatment male patients diagnosed with prostate adenocarcinoma aged from 63 to 83 years ( median 70 years ) were recruited for the exploratory study . 
four patients were treated with photon imrt ( volumetric arc therapy , vmat ; energy 6 mv , dose rate 3 gy / min ) with a daily fraction of 2 gy , according to the conventional ve times a week irradiation scheme . 
the total radiation dose delivered to prostate and half of seminal vesicles ( clinical target volume , ctv ) was 78 gy ; during the rst 22 days of rt , the ctv additionally included the region of the pelvic lymph nodes ( total dose of 44 gy )  . 
another four patients were treated with sabr using a cyberknife ( accuray inc . , chesapeake terrace sunnyvale , ca , usa ) treatment unit according to the scheme 5 fractions of 7.25 gy every second day ( energy 6 mv , dose rate 9 gy / min )  . 
one imrt patient died from a non - cancer - related cause 3 months after rt completion ; the seven other patients are still alive 3 years after treatment ( supplementary table 1 )  . strahlenther onkol ( 2020 ) 196 : 10181033 1021 fig . 
sabr stereotactic ablative body radiotherapy , imrt intensity - modulated radiation therapy whole blood of the patients was collected within a week before the start of treatment ( sample a ) , approximately 40 h after the fth imrt fraction ( cumulative dose 10 gy ) or after the rst sabr fraction ( sample b ) , within 6 h after the last fraction ( sample c ) , and approximately 5 weeks after the last fraction ( sample d )  . 
the blood collection times and doses are specied for each patient in table 1 , while a full description of the patients , their pathology , and the treatment is provided in supplementary table 1 . 
this study was carried out in accordance with the bioethical committee in the maria sklodowska - curie institute , warszawa , approval number 27 / 2015 from 18 / 08 / 2015 . rna isolation and reverse transcription total rna from samples collected in paxgene tubes from rt patients was extracted with the paxgene blood mirna kit ( qiagen , preanalytix gmbh , hilden , germany ) using a robotic workstation qiacube ( qiagen , manchester , uk )  . the quantity of isolated rna was determined by spectrophotometry with a nd - 1000 nanodrop and quality was assessed using a tapestation 220 ( agilent technologies , santa clara , ca , usa )  . 
cdna was prepared from 350 ng of total rna using the high capacity cdna reverse transcription kit ( applied biosystems , fostercity , ca , usa ) according to the manufacturers protocol . 
alternatively , total rna was reverse - transcribed using the hs - rt100 kit ( sigmaaldrich , lisle dabeau , france ) with anchored oligo dt priming according to the manufacturers protocol . quantitative real - time polymerase chain reaction two different quantitative pcr ( qpcr ) protocols were used . 
first , qpcr was performed using a rotor - gene q ( qiagen , hilden , germany ) with perfecta multiplex qpcr supermix ( quanta bioscience , inc . , gaithersburg , md , usa )  . 
the samples were run in triplicate in 10 l reactions with 1 l of the cdna synthesis reaction together with six different sets of primers and uorescent probes at 300 nm concentration each . 
36 - carboxyuorescein ( fam ) , 6 - hexachlorouorescein ( hex ) , atto 680 , atto 390 , texas red ( eurogentec ltd . , fawley , hampshire , uk ) , and cy5 ( sigma - aldrich , poole , dorset , uk ) were used as uorochrome reporters for the probes analyzed in multiplexed reactions with six genes per run including a housekeeping gene . 
the reactions were performed with the following cycling conditions : 2 min at 95 c , then 45 cycles of 10 s at 95 c and 60 s at 60 c . 
for these genes , amplication was performed in a c100 thermal cycler ( biorad , marnes - la - coquette , france ) equipped with a cfx 384 real - time systesamples were run in triplicate 10 l reactions containing 5 l of luminoct sybr green qpcr readymix ( sigma - aldrich ) , 2 m of each primer , and 2 l of 1 / 8th - diluted cdna . 
after 2 min of denaturation at 95 c , reactions were performed for 40 cycles consisting of 5 s of denaturation at 95 c and 20 s of elongation at 60 c . 
expression of each gene , corrected for primer efciency , was normalized to the expression of hprt and 36b4 housekeeping genes amplied concurrently on the same plate [ 21 ]  . 
briey , direct antibody staining of whole blood samples was performed without previous isolation of peripheral blood mononuclear cells . this allows detection of all circulating immune cells including the granulocytic compartment with multicolor ow cytometry and also reduces the required preparation steps . we here used the ipt5 assay with four measuring tubes , focusing on absolute cell count , general immune status , t cells , and dendritic cells in more detail . 
to assess the signicance of changes between consecutive samples of each patient , the paired t - test was employed with p < 0.05 as the signicance level . human cytokine antibody array analysis the proteome proler human xl cytokine array kit ( r&d systems , lille , france ) allows simultaneous quantication of 105 cytokines and inammatory mediator proteins in one sample . 
the values of duplicate spots representing one protein were averaged , and the background signal was subtracted . data for each array were then normalized to the positive control signals to adjust for between - plate effects . 
each background - subtracted intensity signal was multiplied by a normalization factor dened as the ratio of the average signal intensity of the positive control spots on all analyzed arrays to the average signal intensity of the positive control spots located on the particular array being normalized . results are illustrated as mean signal ( pixel ) intensity for a given protein in each sample . 
due to the very low quality of an array for imrt sample d ( only 20% of antibodies detected ) , all arrays for that patient were ltered out from further analysis . 
subsequently , antibodies which were detected on at least 28 arrays ( 93% of all arrays ) were chosen for further continuous data analysis , resulting in 48 antibodies to analyze . 
linear regression for known dose points was performed , and the obtained model served as the reference for signal estimation ( i.e. , in the case of a 7.25 gy value approximation , a linear model between 0 gy and 10 gy measurements was constructed )  . 
subsequent statistical analysis of measurements in common dose points was analogous to the one described above . eect size interpretation cohens d effect size values 1.2 were interpreted as indicating at least a very large effect [ 25 ] , and the values 0.8 as the evidence for at least a large effect . 
in the case of effect size measured by rank - biserial coefcients of correlation ( both ru and rw ) , the critical value for at least a large effect was set to 0.5. 
for example , an at least large effect sizecohens d 0.8implies that at least 79% of observations from one group will have a higher value than the mean of the second group . data analysis and visualization was performed in r [ 29 ]  . the basic data analysis pipeline results all statistical analyses were performed on normalized data . classical statistical inference was supported by the effect size analysis to minimize the impact of small sample size and low power of statistical tests [ 25 , 26 ]  . 
we applied restrictive thresholds of at least large effect size for reporting differences between subjects under comparison , to minimize the small - sample impact . in the case of between - therapy comparisons , the mann whitney u test was performed with the benjaminihochberg correction for multiple testing . 
a wendts rank - biserial coefcient of correlation [ 27 ] ( denoted as ru ) was calculated to estimate the effect size . for time / dose series analysis , the repeated - measures analysis of variance ( anova ) test for paired observations was performed . 
following this validation , the expression of genes coding for a selection of cytokines was analyzed in these samples , together with the gene coding for cyclin g1 as a second stressresponsive gene . 
similarly , expression of the pro - inammatory cytokine il1b gene was induced during the course of treatment and stayed high in the following weeks when compared to the pretherapy sample , but only in imrt patients ( d < 1.4 for all pairwise comparisons )  . 
in contrast , a decrease in expression of the gene coding for the c - c motif chemokine ligand 3 ( ccl3 ) , an inammatory factor involved in recruitment and activation of granulocytes , during rt between samples b and c was observed only in sabr patients . 
expression of il6 , coding for a pro - inammatory mediator with multiple activities , and il8 , another chemokine involved in neutrophils recruitment , was consistently detected only in imrt and sabr patients , respectively . 
2 gene expression of fxdr , sesn1 , gadd45 , ddb2 , and mdm2 in blood of prostate adenocarcinoma patients treated with imrt ( a ) and sabr ( b ) , respectively . 
blood was collected before the start of the treatment ( blood collection point a ) , after 5 fractions for the imrt group and after the rst for the sabr group ( blood collection point b ) , after the last fraction ( blood collection point c ) , and 1 month after the last fraction ( blood collection point d )  . 
all comparisons found signicant by the tukey hsd test also show large or very large effect sizes , which is not shown on the graph for reasons of clarity strahlenther onkol ( 2020 ) 196 : 10181033 1025 fig . 
3 gene expression of ccng1 , ddb2 , ccl3 , il1b , tgfb1 , and il6 or il8 in blood of the prostate adenocarcinoma patients treated with imrt ( a ) and sabr ( b )  . 
blood was collected before the start of the treatment ( blood collection point a ) , after 5 fractions for the imrt group and after the rst for the sabr group ( blood collection point b ) , after the last fraction ( blood collection point c ) , and 1 month after the last fraction ( blood collection point d )  . 
altogether , these observations and calculations suggest that the expression of il1b and tgfb1 genes is progressively induced during imrt . we additionally compared the modulation of inammatory gene expression in both therapies . 
thus , the expression of these three genes is clearly more induced during imrt compared to sabr . the differential upregulation was maintained in the weeks following rt completion for ccl3 and tgfb1 , while it was only transitory for il1b . 1026 strahlenther onkol ( 2020 ) 196 : 10181033 fig . 
as expected for a systemic immunological response after rt , a decrease of b cells , t cells , and nk cells in the peripheral blood was observed following imrt . however , such a decline was only observed in 2 / 4 patients following sabr , and in 2 patients , the neutrophils and monocytes increased following sabr . 
one common feature of both treatments was an increased expression of the inhibitory changes in metabolic products during rt to obtain further deeper insights in distinct systemic modulations following imrt and sabr , 137 metabolites were quantied in sera of the cancer patients ( listed in supplementary table 2 )  . 
there were more pcs affected by rt in the imrt group than in the sabr group ( in general , 18% of detected pcs were rt affected in either group and sample )  . 
the lpc / lc ratio returned to the pre - rt value in the post - rt sample d that was collected 1 month after the end of treatment in imrt patients . strahlenther onkol ( 2020 ) 196 : 10181033 1027 fig . 
samples from patients subjected to imrt and sabr are compared in the following classes : phosphatidylcholines ( pc ; 67 compounds in total ) , lysophosphatidylcholines ( lpc ; 9 ) , sphingomyelins ( sm ; 13 ) , acylcarnitines ( acylc . ; 11 ) , amino acids ( aa ; 21 ) , biogenic amines ( amines ; 16 )  . 
hash indicates comparisons showing at least a very large effect size ( |d| 1.2 ) modulation of cytokines , inammatory proteins , and immune regulators abundance in plasma during finally , the modulation of the level of a collection of 105 cytokines and proteins was analyzed in the serum of the cancer patients during the course of rt by using dedicated antibody arrays . 
this analysis was restricted to a subgroup of 48 proteins which gave a measurable signal in at least 26 of the 28 antibody arrays analyzed ( one array / sample for each patient )  . 
to identify those modulated during the course of rt with the highest level of condence possible in our setting , we selected only those proteins for which at least three of the six possible pairwise comparisons between the four samples resulted in very large effect sizes , indicating differences between at least three samples . 
altogether , with these criteria , 15 out of the 48 proteins detectable on the antibody array membranes were found to be modulated during imrt , but only 3 during sabr . 
at least large effect sizes ( |ru| 0.5 ) were indicated with an @ and a sign for positive and negative ru values , respectively were modulated in both treatments : growth and differentiation factor 15 ( gdf - 15 ) and tim - 3 . only 3 of the 15 factors modulated during imrt , namely crp , gdf - 15 , and the sex hormone - binding globulin ( shbg ) were found to be increased in sample b when compared to pre - rt sample a , whereas four ( baff , cfd , ddpiv , and resistin ) were decreased . 
the serum level of 10 of these factors ( baff , chitinase 3 - like 11 , crp , cfd , dppiv , insulin - like growth factor binding protein3 ( igfbp 3 ) , matrix metallopeptides 9 ( mmp9 ) , resistin , thrombospondin - 1 , tim - 3 ) was higher in sample c compared to sample b , indicating an increase in their serum concentration during the course of rt . 
however , for a large subgroup including baff , crp , dppiv , gdf - 15 , mmp9 , regulated on activation , normal t cell expressed and secreted ( rantes ) , thrombospondin - 1 , cd31 , tim - 3 , and vascular cell adhesion molecule 1 ( vcam - 1 ) , the level of expression in sample d was higher than in sample a , indicating that the induction of the expression of these cytokines / factors is long lasting and persists at higher levels in the weeks following rt completion compared to the pre - rt samples . only three factors were modulated during the course of sabr . 
tim - 3 was expressed more highly in sabr compared to imrt patient samples a , b , and d , but more expressed in imrt than sabr patient samples at timepoint c . 
for gdf - 15 , a mirrored pattern was observed : gdf - 15 was more highly expressed in imrt patient samples a , b , and d , but not in sample c . 
thus , here , it appears that sabr induced the serum level of gdf - 15 to a greater extent than imrt . discussion this exploratory study presents for the rst time a detailed analysis of several stress and immune parameters at a systemic level that might be modulated in vivo following local exposure to ionizing radiation in a small group of patients treated for prostate cancer by rt using imrt and sabr . both rt modalities have similar anti - tumor efciency [ 30 ] and a low level of acute toxicity was observed in our patients : only one of the imrt patients exhibited grade 2 gastrointestinal toxicity . 
therefore , the observed modulations of immune or immune - related parameters reported in this study can be considered to reect the effects of locally applied ionizing radiation on systemic immune alterations in patients with prostate adenocarcinoma rather than differences in radiation - induced toxicity . overall , the exposure of imrt and sabr patients differed in terms of the total dose delivered over the rt course , the dose per fraction , the number of fractions , the dose rate , and the irradiated ctv . 
however , no effects of adt on the homeostasis of b , t , and nk cell subsets in the peripheral blood of treated patients were observed in a comparison of healthy donors and treated patients [ 33 ]  . 
the use of a restrictive threshold ( at least a large effect size ) allowed identication of the strongest differences and variations between samples with a high level of condence . in this study , a large array of stress and immune parameters at the systemic level in the blood of imrtand sabr - treated prostate cancer patients was analyzed . 
the average total dose delivered to the patients blood during rt in the treating center ( with an estimation based on the individual treatment plans , assuming that the blood volume corresponds to 8% of the irradiated body mass and that there is a homogenous vascularization of irradiated tissues ) was 0.035 gy per 100 ml and 0.009 gy per 100 ml in the case of imrt and sabr patients , respectively . 
the level of transcription of selected p53 - dependent genes was shown to be a good candidate for both total and partial body exposure over a wide range of ionizing radiation doses [ 34 ]  . 
our analyses revealed a transient increase in the expression of fdxr and ddb2 in both imrt and sabr patients during the course of rt , with , however , different kinetics . 
it further increases until a cumulative dose of 36.25 gy , suggesting similar induction mechanisms during the course of sabr and imrt treatments . in contrast , the effects of local radiation exposure on immune parameters at the cellular and humoral levels were different in patients treated with imrt and sabr . 
evolution of the lpc / pc ratio , a postulated metabolomic indicator of inammation [ 19 , 20 ] , was strikingly different during the course of imrt and sabr . 
in all patients , an increase in the percentage of pd - 1 - expressing cd4 + t lymphocytes was for example observed at the end of the treatment . the impact of even low doses of ionizing radiation on the expression of activation markers by immune cell subsets has already been observed [ 9 ]  . 
modulation of antitumor immune responses by interfering with pd - l1 / pd - 1 interactions has systemic effects on the t cell compartment . thus , an increase in circulating pd - 1 + cd4 + t cells ( and in myeloid - derived suppressor cells ) following rt completion was , for example , associated with reduced t cell activity in colorectal cancer patients [ 35 ]  . 
however , on the other hand , rt can also result in an increased frequency of circulating tumor - specic t cells in the cd8 + population , as observed in colorectal and prostate cancer patients [ 36 ] , and the frequency of circulating hla - drhi monocytes is a strong predictor of progression - free and overall survival in response to therapy in stage iv melanoma patients [ 37 ]  . 
it was already described in 1999 that even though rt reduces immune cell numbers in the peripheral blood , the remaining lymphocyte function was still within the normal range [ 38 ]  . 
in addition , the results of this explorative study providefor the rst timeindications that different rt protocols and application methods such as imrt and sabr modulate several components of the immune system differently , as well as their dynamics . 
thus , local radiation exposure partially exerts its systemic effects by altering immune cell subsets , their activation status , and also their microenvironment . the immunological consequences of dna damage are becoming more and more evident [ 39 ]  . 
similarly , the serum concentration of the inammatory cytokines and proteins modulated during imrt was mostly upregulated only between samples b and c , but not in sample b compared to the pre - rt sample a . 
this delay in the induction of stress - response genes and of inammatory parameters in the peripheral blood cells suggests that these events are differentially regulated in blood cells with individual dynamics . 
it may be that inammatory genes are not directly induced by radiation , but rather that their up - regulation is a consequence of the biological effects elicited by radiation exposure , namely tumor cell death and the death of at least a fraction of irradiated circulating blood cells [ 40 ]  . irrespective of their identity , these mechanisms and their outcome ( s ) are complex , as shown by the ndings that both il - 1 , a prototypic pro - inammatory cytokine , and tgf1 , a prototypic anti - inammatory cytokine , were coregulated during imrt . 
in the rare cases of a similar factor being modulated in patients treated with either imrt or sabr , this modulation appears to be in opposite directions in the different rt modalities , as shown in our study of gdf - 15 and tim - 3 . 
its expression is associated with cellular stress conditions like irradiation in human pbls [ 42 ] , primary broblasts exposed ex vivo [ 43 , 44 ] , and murine splenocytes following whole - body exposure [ 45 ]  . 
this difference may be linked to the different initial levels of gdf - 15 in both groups of patients , or to differences in cell death / stress or tissue damage . 
we did indeed observe regulation of several factors denoting endothelial dysfunction ( cd31 , vcam , thrombospondin ) and tissue remodeling ( mmp9 , chitinase 3 - like 1 ) in imrt , but not in sabr patients . 
the other differently regulated protein common to both groups of patients is tim - 3 , a negative regulator of th lymphocytes and innate immune cell activation when expressed on the cell surface [ 46 ]  . 
in vitro , tim - 3 has been found to be shed by adam proteases from the surface of human tlr - activated cd14 + monocytes [ 47 , 48 ]  . 
here , we observed a low but detectable persistent increase in the circulating level of tim - 3 in the weeks following the end of the treatment in both imrt and sabr patients . 
so far , no function has been attributed to this soluble tim - 3 protein , but its increase may reect innate immune cell activation during imrt and sabr treatments . even though this explorative study was already quite comprehensive , future studies should be even more detailed and include more immune parameters such as danger signals that reect radiation - induced immune damage response [ 49 ] or hsp70 abundance [ 50 ] , which give indications about the tumor status . strahlenther onkol ( 2020 ) 196 : 10181033 1031 in addition , future studies should also consider additional endpoints such as dna damage , including complex and oxidative lesions , apoptosis , the use of sensitive methods such as enzyme - linked immunosorbent assay ( elisa ) to measure the modulation of circulating inammatory cytokines , and of course clinical outcome . 
it was also shown that dna damage could be detected in non - irradiated , out - of - eld tissues in a different cohort of patients treated by rt or rt + chemotherapy for lung cancer [ 51 ]  . 
this abscopal effect is similarly observed in preclinical mouse models locally exposed to a single dose of high - dose - rate synchrotron radiation [ 52 , 53 ]  . 
in mice , the generation of genotoxic lesions at distant sites was found to depend on a functional immune system and was attenuated in the absence of the ccl2 / mcp - 1 cytokine . 
it would be interesting to nd out whether the different modulation of immune parameters that we observe in imrt and sabr patients translates into a differential pattern of genotoxic stress at distant sites according to rt modality in patients . pre - clinical mouse studies could be designed to investigate the eventual relations between dose , dose rate , repeated exposure , immune modulation , and genotoxic effects at distant sites in the context of local irradiation of normal tissue or tumors . in conclusion , the data presented herein depict that localized irradiation results in systemic modulation of a large range of cellular and humoral immune parameters . 
the radiation - induced effects on inammatory gene transcription , immune cell homeostasis , and serum concentration of lipids and cytokines appear to be different in patients treated by different rt modalities . 
these differences are qualitative ( e.g. , genes induced only in imrt , more cytokines modulated in imrt , myeloid cells modulated only in sabr ) and quantitative ( e.g. , different evolution of lpc / pc ratio )  . 
this exploratory study suggests that rt modalities with similarly high therapeutic efciency and low clinical toxicity can have different effects on immune system homeostasis and activation at the systemic cellular and molecular level for up to 5 weeks following rt completion . 
late effects of rt such as a decrease in circulating cd3 + t lymphocytes have previously been observed in prostate cancer patients 12 months post treatment [ 54 ]  . 
thus , the ndings presented here need to be conrmed in larger groups of patients in the future , also taking into account further analyses at even later timepoints after completion of rt . funding this work received funding from the european unions seventh framework programme from the operra project ( euratom / fp7 ) under grant agreement no . 
candias declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
schmig - markiefka4 , 5 received : 1 march 2020 / accepted : 4 may 2020 / published online : 19 may 2020 springer - verlag gmbh germany , part of springer nature 2020 abstract purpose for many decades , endometrial cancer ( ec ) has been considered as a homogenous tumor entity with good prognosis . 
treatment recommendations differ considerably from country to country . materials and methods the cancer genome atlas ( tcga ) research network has shown that ecs should be reclassied into four novel molecular prognostic groups , with the potential of changing adjuvant management of ec patients : ultra - mutated , hyper - mutated , copy - number low , and copy - number high . 
the european society of gynaecological oncology ( esgo ) guideline for endometrial cancer takes the new classication system into consideration for adjuvant treatment decisions and will be published this year . results in the near future , we expect new treatment recommendations that may differ considerably from the clinicopathologically driven recommendations on the basis of our deeper insight and better understanding of molecular markers in endometrial cancer . 
the portec 4a study is the only recruiting study which randomizes patients to adjuvant or no adjuvant treatment on the basis of the aforementioned new classication system . conclusion the aim of the new classication is a more personalized adjuvant radio ( chemo ) therapy decision and better oncologic outcomes or avoidance of overtreatment . keywords uterus carcinoma risk classication adjuvant radiation brachytherapy survival introduction for many decades , endometrial cancer ( ec ) has been considered as a homogenous tumor entity with good prognosis . it was not until 1983 that bokhman described two distinct ( cid : 2 ) med . 
62 , 50937 cologne , germany 2 department for specialized laparoscopic surgery , asklepios clinic hamburg - altona , hamburg , germany 3 medical faculty , department of gynecology , university clinic bonn , bonn , germany 4 medical faculty , institute of pathology , university cologne , 5 center for integrated oncology cologne bonn ( cio ) , bonn , cologne , germany germany types of ec [ 1 ]  . 
he divided the endometrial cancer into a good one ( type 1 , estrogen dependent ) with better prognosis and the bad one ( type 2 , non - dependent on estrogen , with worse prognosis )  . 
loss of er or pr expression is related to higher - grade tumors and impaired disease - free survival [ 2 ]  . the increasing incidence of endometrial cancer in developing and industrialized countries matched this type1 / 2 system and has been attributed to the increasing availability of industrially processed food with high calorie intake , subsequent obesity , and diabetes . 
nowadays , the increasing numbers of type 2 cancers in non - hispanic black 964 strahlenther onkol ( 2020 ) 196 : 963972 women in the us give rise to further questions . 
furthermore , treatment recommendations differ internationally [ 10 , 11 ]  . current classification system the currently valid risk stratication considers clinical and pathological factors like lymph node involvement , figo ( international federation of gynecology and obstetrics ) , age of the patient , grading , myometrial inltration , lvsi , and tumor size . 
cf immunohistochemical loss of staining with mlh1 and pms2 ( stained lymphocytes as positive internal control ) , while msh2 and msh6 show nuclear staining . this is a case of an endometrial cancer with stage pt3b , l0 , v0 , pn0 , r0 ; immunohistochemical loss of dna proteins mlh1 and pms2 comparable with a microsatellite instable tumor . 
this was conrmed by molecular testing proving msi - h status . additional molecular testing detected mlh1 promotor methylation , conrming a sporadic tumor strahlenther onkol ( 2020 ) 196 : 963972 fig . 
pole mutations are more frequently found in tumors of relatively young women with lower body mass index ( bmi ) and higher - grade endometrioid endometrial tumors compared to pole - wildtype ec . for the copy - number low group , no specic driver mutation was identied ( nsmp = no specic molecular prole )  . 
nsmp tumors show a low mutational burden , they are mostly endometrioid type g1 / 2 , and often carry ctnnb1 mutations and pi3k pathway alterations [ 13 ]  . 
this subclass contains a heterogeneous set of tumors , which complicates the distinction of favorable or unfavorable tumors [ 14 , 15 ]  . msi - positive tumors ( 2040% of all ec patients ) are correlated with an intermediate prognosis , but are very responsive to immunotherapy . 
msi + tumors are characterized by a lack of expression of mismatch repair enzymes ( mlh1 , msh2 , msh6 , etc . ) and a high number of tics , but associated with negative prognostic factors such as higher histologic grade , presence of lvsi , and with older age and advanced stage ( iii / iv )  . 
the knowledge on the heterogeneity of endometrial cancer biology matches with the disturbing clinicians experience of misjudging the prognosis of some ec patients 966 strahlenther onkol ( 2020 ) 196 : 963972 fig . 
this is a case of a high - grade endometrioid endometrial cancer stage pt1b , pn0 , l0 , v0 , r0 with detection of two hotspot mutations in pole in exon 13 and exon 14 . 
this is a case of another high - grade endometrioid endometrial cancer , estrogen - receptor negative , stage pt1b , pn0 , l0 , v0 , r0 with p53 mutation , proven with molecular testing . p53 - mutated tumors are assumed to have a worse outcome , but again do not show a specic morphological pattern table 1 overview on molecular pathway alterations , prognosis , and potential targeted treatment options [ 28 ] frequency in ec description prognosis potential targeted therapies dna repair dna repair excellent intermediate pd - 1 / pd - l1 immune checkpoint inhibitorsa pd - 1 / pd - l1 immune checkpoint inhibitorsa parpi ; platinum derivatives n / aa tumor suppressor cell adhesion / signaling protein hormone receptors wnt signaling pathway pi3k / akt / mtor signaling pathway epidermal growth factor receptor tumor suppressor poor poor good poor endocrine therapy ( with pi3k / mtor inhibitors ) intermediate goodintermediate pi3k , akt , mtor inhibitors monoclonal antibodies , protein kinase inhibitors goodintermediate ezh2 inhibitors ec endometrial cancer , n / a note available athe addition of parp inhibitors ( parpi ) has been explored for several molecular alterations ; however , evidence of efcacy is still limited molecular ( pathway ) alteration pole mutation mmrd tp53 mutation licam overexpression er / pr expression wnt - - catenin pathway pi3k - akt - mtor pathher2 / neu overexpression aridia mutation 612 2040 929 1628 7295 1815 1447 3040 hier steht eine anzeige . in two directions : the patient who was considered as a lowrisk case with rapid progression and the patient with advanced disease and long - term survival without recurrence . looking back at the study landscape on adjuvant treatment in endometrial cancer , it is noticeable that almost all studies suffer from inappropriate patient selection . 
the mixture of patients with different clinicopathological risk factors led to inconclusive results in gog - 99 , portec - 2 , portec - 3 , gog 122 , gog 249 , and gog 258 , and no clear evidence - based recommendations [ 1620 ]  . even patients with conventional high - intermediate risk ( hir ) factors are at a higher risk of being underor overtreated . 
approximately 15% of high - intermediate risk patients had unfavorable features ( substantial lvsi , p53 mutant , and / or > 10% l1cam ) , 50% favorable features ( pole mutant , nsmp being microsatellite stable , and ctnnb1 wildtype ) , and 35% intermediate features ( msi or ctnnb1 mutant ) [ 21 , 22 ]  . clinical cases case 1 fig . 
1af shows the specimen of an endometrial cancer patient with stage pt3b , l0 , v0 , pn0 r0 and immunohistochemical loss of dna proteins mlh1 and pms2 comparable with a microsatellite instable tumor . 
6 a endometrial cancer - related survival for pole - mutated patients ( blue ) , patients with no other specied molecular prole ( orange ) , patients with microsatellite instability ( green ) , and patients with tp53 mutation ( red ) ; b pelvic recurrence rate in patients with risk factors after vaginal brachytherapy ( red ) and ebrt ( green ) , compared with patients without risk factors receiving vaginal brachytherapy ( orange ) and after vaginal brachytherapy ( blue ) [ 18 ] fig . 
b msi - negative ( mmr procient ) with ( orange ) and without ( blue ) radiotherapy [ 23 ] rmed by molecular testing proving msi - h status . 
2a - e shows a case of an relapsed low - grade endometrial carcinoma , estrogen receptor - positive with known lynch syndrome , immunohistochemically and molecularly proven msi - h status on the recurrent rpt1a , l0 , v0 , pnx , and an additionally known colon carcinoma . 
4a , b illustrates a patient with another high - grade endometrioid endometrial cancer , estrogen receptor - negative , stage pt1b , pn0 , l0 , v0 , r0 , but with a conrmed p53 mutation , proven with molecular testing . p53 - mutated tumors are assumed to have a worse outcome but , again , do not show a specic morphological pattern . this is a patient with a high risk for recurrence . 
the question of whether this patient benets from chemotherapy is still unclear and should be evaluated in future studies . prediction of response to adjuvant treatmenta new world in addition to the prognostic value of genetic proles , the question whether the genomic prole might have a predictive value for any adjuvant treatment is of great interest . 
how we can explain the fact that none of the pole mutant patients in portec1 / 2 were diagnosed with recurrence ? data suggest that the accumulation of deleterious mutations ( error catastrophe ) acts as a strong immunogenic stimulus , which might be responsible for the excellent prognosis without any adjuvant treatment [ 24 ]  . new study landscape as a logical consequence , the portec 4a study was initiated to compare the impact of molecular markers on treatment decisions and outcome in a randomized study . 
patients are randomized ( 2 : 1 ) to the experimental arm and treatment decision based on molecular prole and a standard arm with the recommendation for vbt only [ 25 ]  . 
asterisk high - intermediate risk ( hir ) endometrial cancer : stage ia ( with invasion ) and grade 3 ; stage ib , grade 1 or 2 ; with either age 60 or substantial lymph - vascular space invasion ( lvsi ) ; stage ib , grade 3 without lvsi ; or stage ii ( microscopic ) with grade 1 . 
10 old ( left ) and new molecular risk classication ( right ) as a basis for treatment recommendations ( esgo guideline group , personal communication ) the experimental arm , no adjuvant treatment will be recommended for pole - mutant tumors and patients with mmrd and ctnnb1 wildtype . 
sequential chemotherapy and radiation is an option and chemotherapy alone is an alternative option with regard to overall survival , but with a higher risk of locoregional failure when omitting ebrt . 
in patients with intermediate - risk endometrial cancer ( stage ib endometrioid , grade 12 , 50% myometrial invasion ; or stage ia endometrioid , grade 3 , < 50% myometrial invasion , all with lvsi mild or negative ) , adjuvant brachytherapy is recommended to decrease vaginal recurrence . 
further studies with overlapping risk parameters for their patients came to conicting conclusions ( chemotherapy + vbt comparable with ebrt only [ 26 ] or chemotherapy and chemoradiation comparable in terms of os [ 27 ] ) , which makes a consistent treatment recommendation difcult . conclusion in the near future we expect new treatment recommendations that may differ considerably from the clinicopatho972 strahlenther onkol ( 2020 ) 196 : 963972 logical recommendations on the basis of our deeper insight and better understanding of molecular markers in endometrial cancer . 
1 , 30625 hannover , germany 4 medical practice for radiotherapy and radiation oncology , treibesstrae 11 , 31134 hildesheim , germany 5 department of radiation oncology , university of lbeck , ratzeburger allee 160 , 23562 lbeck , germany strahlenther onkol ( 2020 ) 196 : 10061017 1007 introduction the cornerstone of treatment for non - castrated metastatic prostate cancer ( mpca ) is androgen deprivation therapy ( adt ) , which has remained unchanged over the past years [ 1 ]  . 
there is increasing evidence that patients with a limited number of metastases have a better prognosis than patients with widespread metastatic disease , and data outside large prospective trials suggest that metastasis - directed therapies ( mdts ) for mpca patients with a so - called oligometastatic status , based on a generally accepted imaging - based cut - off of ve metastases , improve the clinical outcome [ 2 , 6 ]  . 
the recent introduction of psma ligand pet has substantially improved the diagnostic accuracy of staging at low prostatespecic antigen ( psa ) levels [ 711 ] , allowing rened and well - monitored individualized radio - oncological treatment concepts that aim to improve psa kinetics , prolong progression - free survival , defer the initiation of adt , and potentially cure the patient [ 25 , 12 ]  . 
however , approximately half of the patients will develop oligoprogressive disease after mdt [ 13 ] , making these patients amenable to repeated mdt and further improving the psa kinetics and delaying the initiation of adt [ 16 ]  . 
a positive visual assessment of increased focal tracer uptake higher than the surrounding background activity was used as the criterion for malignancy [ 9 ]  . radiotherapy treatment patients with lymph node metastases or relapse in the prostatic fossa were treated with conventionally fractionated rt ( cf - rt ) and patients with bone metastases were treated with slightly hypofractionated rt ( hf - rt )  . 
in the case of lymph node metastases , the clinical target volume ( ctv ) encompassed the lymph drainage vessel to the next bifurcation without the whole ipsilateral lymphatic drainage vessel ; the dose was 50.0 gy ( single dose 2.0 gy ) , followed by a sequential cf - rt boost of 10.0 gy ( single dose 2.0 gy ) to the lymph node metastases . 
the planning target volume ( ptv ) for lymph node metastases , bone metastases , and local relapse in the prostatic fossa included the ctv plus a 10 - mm safety margin in all directions to account for setup errors . 
image guidance was conducted at least twice a week with megavoltage cone - beam ct . visceral metastases were treated with image - guided stereotactic body radiation therapy ( sbrt ) and a total dose of 37.5 gy ( single dose 12.5 gy ) to the encompassing 67% ptv isodose . 
the ptv included the internal target volume ( itv ) plus a 4 - mm safety margin in all directions to account for setup errors . follow - up and endpoints all patients had periodic urologic follow - up evaluations , which included psa measurements every 3 months . 
patients with extensive disease ( 6 metastases ) received systemic therapy according to the urologists choice . in general , outcomes were dened from the last day of rt . the outcome parameters were biochemical progression - free survival ( bpfs ) , adt - free survival ( adt - fs ) , overall survival ( os ) , and toxicity . 
we used the paired students t - test to compare pre - rt with post - rt parametric parameters and the wilcoxon signed - rank test when the data were not normally distributed . 
factors for rt treatment failure were analyzed with the log rank test in univariate analyses and signicant factors were further assessed with multivariate analyses to identify independent variables for brfs and adt - fs . 
at risk : directed rt resulted in a cumulative ineld relapse rate of 3.4% ( 4 / 119 ) and in a cumulative outeld relapse rate of 96.6% ( 115 / 119 )  . 
the four ineld relapses occurred in the right iliac lymph nodes ( 25% , 1 / 4 ) , in a rib metastasis ( 25% , 1 / 4 ) , and in pelvic bone metastases ( 50% , 2 / 4 )  . the median follow - up time was 39.5 months ( 1860 )  . one out of 32 ( 3.1% ) patients died after 47 months of progressive mpca . 
table 3 shows the detailed results of uniand multivariate analyses for bpfs_1 and bpfs_2 . at the last follow - up , 28.1% ( 9 / 32 ) of patients did not need adt . 
late grade iii gastrointestinal toxicity occurred in 3.1% ( 1 / 32 ) of patients and grade ii genitourinary toxicity occurred in 3.1% ( 1 / 78 ) of patients . discussion the implementation of psma ligand pet imaging has substantially improved the diagnostic accuracy of detecting metastatic pca at low psa levels [ 7 , 8 , 20 ]  . 
furthermore , there is 1014 strahlenther onkol ( 2020 ) 196 : 10061017 still controversy about the optimal timing to initiate palliative adt for asymptomatic metastatic patients because of the lack of prospective trials in the psa era [ 1 ]  . 
furthermore , adt offers no curative potential [ 1 ] and signicantly impairs qol in a relevant number of patients [ 22 ]  . smaller prospective trials with heterogeneous patient cohorts , including one with choline pet imaging [ 13 ] , one with psma ligand pet imaging [ 14 ] , and one with sodium uoride ( na - f ) pet imaging [ 15 ] , showed encouraging results for mdt in oligometastatic prostate cancer . 
to the best of the authors knowledge , there are no published data comparing mdt alone versus mdt plus adt with regard to hard endpoints such as prostate carcinoma - specic survival . 
in our opinion , patients must be well informed that adt is the standard of care and any type of mdt is an individual treatment concept outside the current guidelines , although the optimal timing of initiation of adt at low psa levels remains unknown [ 1 ]  . 
nevertheless , approximately half of the patients will develop oligoprogressive disease after mdt alone [ 7 ] , making these patients amenable to a second mdt and further delaying the start of adt [ 13 , 23 , 24 ]  . 
additionally , due to the lack of data from prospective trials , the current guidelines do not reect the diagnostic accuracy of psma ligand pet staging at low psa levels to select patients who should or should not receive adt [ 1 ]  . to the best of our knowledge , a second rt for oligorecurrent pca on the basis of psma ligand pet staging and restaging has never been reported . 
none of the published data [ 13 , 23 , 24 ] included psma ligand pet staging for mdt that led to mdt at higher psa levels , particularly increasing the likelihood that patients had an underestimated extent of lymph node metastases [ 11 , 22 ]  . in addition , the initiation of adt based on the urologists choice at low psa levels might be a confounder for adtfs and , therefore , hamper the comparison of these retrospective data . we found that the type of irradiated metastases at oligorecurrence was the most important clinical parameter for adt - fs . 
population - based data supported our ndings because patients with bone metastases have a worse prognosis and lower cancer - specic survival ( css ) than those with lymph node metastases [ 25 , 26 ]  . 
a recently published seer database analysis suggested that patients with stage m1a tumors receive signicantly greater clinical benets from local therapies to the prostate than patients with stage m1b tumors [ 27 ]  . 
until now , the evolutionary history of metastatic prostate cancer of monoclonal versus polyclonal cell seeding leading to a linear versus branching pattern of metastatic spread [ 28 ] at low psa levels remains unknown . 
many genomic and nongenomic biomarkers have been investigated in mpc [ 29 , 30 ] , but none of these markers are available outside of dedicated study protocols for clinical routine . 
on the other hand , exploratory analyses of patients with limited tumor burden according to the chaarted criteria revealed no os benet for escalated systemic therapy using either the combination of adt + docetaxel [ 31 ] or adt + enzalutamide [ 32 ] compared to adt alone , indicating a different biology . 
showed that patients with non - castrate mpca and one metastasis plus a psa - dt > 3 months had a 5 - year css rate of 100% , whereas patients with a psa - dt < 3 months plus > 1 metastasis had a 5 - year css rate of only 8% [ 33 ]  . 
data from the choline pet era conrmed that choline pet underestimated the extent of lymph node metastases [ 34 ] , which is reected by the fact that approximately two out of three patients treated with sbrt for pelvic lymph node metastases relapsed with lymph node metastases [ 25 , 35 ] , leading to a higher relapse rate than that after elective node irradiation ( eni ) , although the relapse rate concerning bone and visceral metastases seems to be comparable between sbrt and eni [ 36 ]  . 
therefore , we do not recommend eni because the initiation of systemic therapies according to highand low - burden disease and the corresponding prognosis do not depend on lymph node metastases , but on bone and visceral metastases [ 1 ]  . 
these results may indicate that eni may have been a necessary compensator for the poor detection rate of lymph node metastases of choline pet scans . some limitations of this study should be acknowledged . the retrospective nature has inherent limitations and might have introduced selection bias , although the presented cohort had a strict follow - up schedule and staging was performed only with psma ligand pet . 
therefore , fewer metastases should be missed with this method than with conventional imaging and choline pet [ 11 , 20 , 35 ] , leading to well - selected patients [ 37 ]  . 
moreover , the second psma ligand pet for restaging purposes allows assessment of the metabolic response after rt , leading to a reliable discrimination of new metastases and successfully irradiated metastases [ 38 ]  . 
in addition , the study included a selected cohort with only high - risk and very high - risk patients . therefore , caution should be taken when generalizing the observed results for patients with intermediateor low - risk oligorecurrent pca . 
von klot declare that they have no competing interests . ethical standards this retrospective analysis was approved by the local ethics committee . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
the present study compares the clinical utility of mri - based active bone marrow ( bmact ) delineation with that of ct - based bone marrow total ( bmtot ) delineation for predicting hematologic toxicity . methods a prospective cohort study was performed . 
linear regression models were generated for the nadirs and receiver operating characteristic ( roc ) curves for the occurrence of grade 3 / 4 hematologic toxicity . results thirty - ve patients were enrolled . 
models for the prediction of alcnadir% ( v5 - v20bmtot , v5 - v30bmact ) and platelet nadir ( pltnadir% ; v5 - v10bmtot , v5 - v20bmact ) were statistically signicant . 
in the roc curves , a baseline lymphocyte level of 1.81 103 / ml was adopted as the cutoff for predicting grade 3 / 4 lymphopenia , with specicity of 77.8% and sensitivity of 73.1%. 
kopernika w odzi , pabianicka 62 street , 93 - 513 dz , poland 2 department of external beam radiotherapy , regional cancer center , copernicus memorial hospital of lodz , zakad teleradioterapii , wojewdzkie w.w.c.o.it. 
im. kopernika w odzi , pabianicka 62 street , 93 - 513 dz , poland 3 department of biostatistics and translational medicine , medical university of lodz , zakad biostatystyki i medycyny translacyjnej , cenrum mazowiecka 15 street , 92 - 215 dz , poland 4 department of uro - oncology , maria sklodowska - curie memorial cancer centre and institute of oncology warsaw , klinika nowotworw ukadu moczowego , centrum onkologii - instytut imarii skodowskiejcurie ul . roentgena 5 , 02 - 781 warszawa , poland rectal cancer is the seventh most common cancer among men and the tenth most common among women , with approximately 704 , 000 new cases and 301 , 000 deaths estimated in 2018 worldwide [ 1 ]  . 
preoperative chemoradiotherapy forms part of the multidisciplinary treatment protocol for stage ii and iii of the union for international cancer controls ( uicc ) classication rectal cancer [ 2 ]  . the immune status of patients with cancer has gained prominence over recent years . 
as approximately half of the active bone marrow in adults is located in the pelvis , radiotherapy ( chemoradiotherapy ) of this region may result in hematologic toxicity [ 3 ]  . 
as with other cancers , absolute lymphocyte count ( alc ) before , during , and after radiotherapy ( chemoradiotherapy ) is known to serve strahlenther onkol ( 2020 ) 196 : 9981005 as a predictive and prognostic marker in rectal cancer [ 57 ]  . in addition , alc can affect the incidence of complete clinical response , which allows implementation of a promising , cost - effective watch - and - wait strategy [ 6 , 8 ]  . previous studies have found the dosevolume parameters of total bone marrow ( bmtot ) of the pelvis to be associated with hematologic toxicity arising as a result of radiotherapy or chemoradiotherapy of rectal cancer [ 3 , 9 ]  . 
in addition , studies based on positron - emission tomography ( pet ) have examined possible correlations between the dosevolume parameters of active bone marrow ( bmact ) in gynecological malignancies and anal canal cancer [ 1015 ]  . 
however , pet has limited value in the staging of rectal cancer [ 2 ]  . magnetic resonance imaging ( mri ) is routinely used for locoregional staging of rectal cancer [ 2 ]  . 
active and inactive bone marrow differ with regard to their chemical and cellular content : bmact ( 40% fat , 40% water , and 20% protein ) has a slightly higher or similar signal to skeletal muscle in t1 - dependent mri images , while inactive marrow ( 80% fat , 15% water , and 5% protein ) is hyperintensive [ 1618 ]  . 
mri allows clear differentiation between hematologically active and inactive bone marrow [ 16 ] ; it may therefore be useful in planning radiation therapy , as the obtained dosevolume constraints of bmact can be used to optimize treatment planning and reduce hematologic toxicity . its use in the pelvic region has previously been evaluated , but the only study did not analyze the ndings with regard to bmtot [ 19 ]  . 
therefore , the aim of the present study was to assess the clinical utility of a t1 - weighted mri sequence as a tool for delineating active bone marrow in the pelvic region and to compare this method with objective ct - based delineation of total bone marrow ( bmtot ) by analyzing the relationship between the dosevolume parameters of bmact and bmtot and hematologic toxicity . materials and methods study design and participants a prospective single - arm phase ii cohort study was performed . 
exclusion criteria included any contraindication to chemoradiotherapy , the presence of clinically signicant cardiovascular history , renal or liver dysfunction , pregnancy , previous radiotherapy to the pelvic area , systemic cancer therapy ( including neoadjuvant chemotherapy ) , or hematologic disorders . 
the study was approved by the national bioethical commission . procedures staging and qualication to treatment were performed according to present nccn guidelines and approved by a multidisciplinary cancer center board . 
all patients underwent radiotherapy planning ct in the prone position with 5 mm slice thickness . total bone marrow ( bmtot ) was dened as the volume limited by external contour of all bones in the pelvic region , visualized on ct , as proposed by mell et al . 
the bones in the pelvic region were dened as the volume containing the hip bones , ischium , pubic bones , acetabulum , and proximal femur , from the upper border of the femoral heads to the lower border of the ischial tuberosity , the lumbosacral spine up to the height of the upper border of iliac crest . in addition , all patients underwent a 1.5t mri transverse t1 - weighted sequence encompassing all pelvic bones , as described above ( eld of view [ fov ] = 400 mm , matrix size 384 384 , repetition time [ tr ] = 691 ms , echo time [ te ] = 9 ms , slice thickness 5 mm , phase oversampling 50% ; parameters were modied as required by mri software in response to anatomy of the patient )  . 
the fat tissue can be identied based on its short t1 relaxation time and high signal in t1 - weighted sequence , and yellow ( inactive ) bone marrow can be contrasted with active bone marrow based on its high fat content [ 16 , 21 ]  . 
bmtot and bmact were not regarded as the organ at risk and the dose was not intentionally reduced . all patients underwent 5 - uorouracil - based chemoradiotherapy to 50.454 gy in two stages . 
three cycles of two - day 5 - uorouracil ( 400 mg / m2 / d ) with leucovorin ( 20 mg / m2 / d ) were admin1000 strahlenther onkol ( 2020 ) 196 : 9981005 fig . 
1 contouring method of active bone marrow based on magnetic resonance imaging . a t1 - weighted transverse mri image , b t1 - weighted transverse image with active bone marrow contour istrated concurrently with radiotherapy every 14 days . complete blood count samples were collected every week , and a renal and liver function test was performed every 2 weeks . according to nccn guidelines , the main irradiation technique was 3d conformal radiotherapy ; dynamic irradiation techniques ( intensity - modulated / arc radiotherapy ) were reserved for unique clinical situations such as those associated with uncommon anatomy [ 2 ]  . endpoints and statistical analysis the size of the sample was estimated prospectively : 34 patients were required . 
occurrence of grade 3 / 4 ctcae ( version 4 ) hematologic toxicity and peripheral blood parameter nadirs were adopted as basic endpoints . nadirs were specied as percentage of baseline value ( lymphocytes : alcnadir% ; neutrocytes : ancnadir% ; platelets : pltnadir% ; red blood cells : rbcnadir% )  . 
the following clinical data items , indicated to be potentially signicant by previous studies , were included in the analysis : age , gender , body mass index ( bmi ) , who / ecog performance status , duration of chemoradiotherapy , use of arc irradiation techniques . 
spearmans rank correlation test or the mannwhitney u test was used to determine the relationship between clinical data and dosevolume parameters and hematologic toxicity , depending on the type of clinical data . 
dosevolume parameters were v5 - v45bmact and v5 - v45bmtot , specied as volume of bmact and bmtot receiving 5 to 45 gy , respectively ( in percentages of whole volume of bmact or bmtot )  . 
additionally , roc curves were generated for the occurrence of grade 3 / 4 hematologic toxicity . cut - off was determined based on the youden index . statistically signicant results obtained in univariate analysis were included in multivariate linear regression models with stepwise selection using backward elimination . 
all patients completed the planned treatment ; one patient did not reach half the middle cycle of concurrent chemotherapy due to infection not related to treatment . time of treatment was 37 to 44 days ( me : 38 days ) and was not associated with any blood parameter nadirs . 
older age was associated with a lower proportion of bmact / bmtot ( r = 0.34 , p < 0.05 ) , but not with baseline or nadir levels of alc , anc , plt , or rbc . 
due to the low number of patients with stage ii disease , no statistical analysis was performed regarding clinical cancer stage . twenty - six patients were irradiated using the static 3d conformal technique and nine using the arc technique ( either in one or both stages )  . 
two separate models for predicting alcnadir% and pltnadir% were generated . all statistically signicant factors for alcnadir% from univariate models ( v5bmtot , v10bmtot , v15bmtot , v20bmtot , v5bmact , v10bmact , v15bmact , v20bmact , v25bmact , v30bmact , gender ) were included in the multivariate regression model for alcnadir% . 
all statistically signicant factors for pltnadir% from the univariate model ( v5bmtot , v10bmtot , v5bmact , v10bmact , v15bmact , v20bmact ) were included in the multivariate regression model for pltnadir% . 
the initial model had r2 = 0.20 , table 3 multivariate linear regression model for alcnadir% ( backward elimination method ) model adjusted r - square r - square change statistics f change sig . 
as the mri - based bmact volume is smaller than bmtot obtained by ct , it could offer greater potential as an organ at risk for plan optimization during 3d / imrt radiotherapy planning . 
in view of the above , recent studies have been able to delineate bmact using the following imaging modalities : 18f - uorothymidine positron - emission tomography ( fltpet ) [ 10 , 13 ] , 18f - uorodeoxyglucose positron - emission tomography ( fdg - pet ) [ 1012 , 14 , 15 , 2325 ] , and mri [ 19 ]  . our results conrm that an association exists between the dosevolume parameters of pelvic bmtot and hematologic toxicity , as noted previously [ 26 ]  . 
found dosevolume parameters from low dose ranges ( v5bmact ) to be associated with wbcnadirs and pltnadirs in a multivariate linear regression model ; however , the study used a different chemotherapy regimen based on oxaliplatin , which is currently not recommended in neoadjuvant chemoradiotherapy of rectal cancer [ 2 ] , and delineated bmact in a different range than in other studies ( ptv + 2.5 cm ) [ 19 ]  . 
in the present study , both the bmact and bmtot dosevolume parameters were found to be associated with platelet and lymphocyte nadirs , which is similar to data obtained by pet - based bmact contouring . 
fdg - pet - based bmact and bmtot dosevolume parameters were found to be associated with hematologic toxicity in cervical and anal canal cancers , suggesting that bmact contouring could be a valuable method [ 11 , 23 ]  . 
however , similar studies regarding the dosevolume parameters of both bmtot and bmact and hematologic toxicity in anal canal cancer indicated that bmact parameters , dened by fdg - pet , failed to improve models [ 15 ]  . as reports on the clinical value of bmact and bmtot contouring are conicting , the present study identies the most valuable predictors of hematologic toxicity , in order strahlenther onkol ( 2020 ) 196 : 9981005 1003 to avoid the effect of collinearity of variables ( dosevolume parameters )  . 
no such signicance was reported in the previous studies . our results suggest that the dosevolume parameters of mri - based bmact parameters may have greater clinical utility in predicting hematologic toxicity . 
the intertecc - 2 trial of a cohort of cervical cancer patients found bone marrow - sparing radiotherapy based on pet - bmact to demonstrate lower toxicity than ct - bmtot delineation ; however , the authors note that reduction of toxicity could not be fully explained , because the pet - bmact sparing group had unintentionally also demonstrated better dosevolume bmtot parameters [ 12 ]  . an additional part of the study was the analysis of clinical data affecting hematologic toxicity . 
however , it is unknown whether female gender is an independent risk factor for hematologic toxicity or if women demonstrate worse dosevolume parameters due to the different shape of the pelvis , thus being more prone to hematologic toxicity . 
our data suggest that although there were no differences in ptv volume between genders , women demonstrated smaller bmact and bmtot volumes and , due to the spatial location , poorer dosevolume parameters . 
in addition , the multifactorial analysis performed in the present study also indicates that female sex is an independent risk factor . baseline blood parameters ( alc0 , anc0 , plt0 , rbc0 ) are a strong factor associated with reduced nadirs in the present paper and several previous studies [ 28 , 29 ]  . 
similarly , in the largest prospective study accessing hematologic toxicity in prostate cancer patients undergoing radiotherapy , alc0 1.83 103 / ml allowed prediction of grade 3 ctcae lymphopenia [ 28 ]  . 
in view of our present ndings and those of sini et al . , it seems justied to report nadirs as a proportion of initial value , as in the current study [ 28 ]  . finally , lymphocyte toxicity is gaining importance in the era of understanding the immune mechanisms responsible for cancer development and treatment . 
the relationship between radiotherapy and immunotherapy is under investigation , and the results of clinical trials assessing the combination of radiotherapy and immunotherapy have recently been published [ 30 ]  . 
in colorectal cancer , baseline alc and the ratio of lymphocytes to neutrocytes is are prognostic factors affecting overall and progression - free survival [ 5 , 31 , 32 ]  . 
hence , the present study assesses whether contouring of active bone marrow based on mri , which , in principle , is partly subjective , may be clinically useful . patients with rectal cancer were included in the prospective selection of the study cohort for three reasons : lymph node irradiation and mri are routinely used in this indication , and 5 - uorouracil - based chemotherapy has low myelotoxic potential . 
the chemotherapy regimen with low myelotoxic potential minimizes the effect of this treatment on hematologic toxicity in combination chemoradiotherapy . this enables more objective assessment of the effect of radiation therapy on myeloid toxicity . 
patients 1004 strahlenther onkol ( 2020 ) 196 : 9981005 undergoing radiotherapy / chemoradiotherapy after surgery procedures ( endometrial , rectal , prostate cancer ) were excluded due to the possible impact of surgery on peripheral blood parameters associated with perioperative and postoperative complications . 
prostate cancer patients were not included due to conicting data on pelvic lymph node irradiation . nevertheless , this is the rst study to compare the objective method of bmtot contouring with the promising but partly subjective mri - bmact contouring method . 
our study cohort was homogenous and was not affected by surgery . in addition , the employed chemotherapy regimen has less myelotoxic potential than those including cisplatin or mitomycin in cervical and anal cancer patients . 
another strength of our study is its use of mri , which , unlike pet - ct , is routinely used in the diagnosis of pelvic tumors . conclusion the dosevolume parameters of bmact predict alcnadir% and pltnadir% more accurately than bmtot . 
fijuth declare that they have no competing interests . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
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schmid6 received : 20 december 2019 / accepted : 13 june 2020 / published online : 3 july 2020 the author ( s ) 2020 abstract objective to prospectively compare the interobserver variability of combined transrectal ultrasound ( trus ) / computed tomography ( ct ) vs . 
magnetic resonance imaging ( mri ) only - based contouring of the high - risk clinical target volume ( ctvhr ) in image - guided adaptive brachytherapy ( igabt ) for locally advanced cervical cancer ( lacc )  . methods five patients with lacc ( figo stages iibiva ) treated with radiochemotherapy and igabt were included . ct , trus , and t2 - weighted mri images were performed after brachytherapy applicator insertion . 
the ctvhr ( based on the gec - estro recommendations ) was contoured by ve investigators on the three modalities ( ctvhr_ct , ctvhr_trus - ct , and ctvhr_mri )  . 
the mean ctvhr_ct volume of all observers was 71% larger than the mriref volume , whereas the mean ctvhr_trus - ct volume was 15% larger . conclusion hybrid trus - ct as an imaging modality for contouring the ctvhr in igabt for lacc is feasible and reproducible among multiple observers . 
trus - ct substantially reduces overestimation of the ctvhr volume of ct alone while maintaining similar interobserver variability . keywords locally advanced cervical cancer image - guided adaptive brachytherapy transrectal ultrasound contouring mri ( cid : 2 ) maximilian p . 
neustadt , austria 3 christian doppler laboratory for medical radiation research for radiation oncology , medical university of vienna , vienna , austria 6 department of radiation oncology , comprehensive cancer center , general hospital of vienna , medical university of vienna , whringer grtel 1820 , 1090 vienna , austria 984 introduction in image - guided adaptive brachytherapy ( igabt ) of locally advanced cervical cancer ( lacc ) , magnetic resonance imaging ( mri ) with applicator in place is currently considered as the gold standard for tumor visualization and dose optimization [ 19 ]  . 
mri is , however , not always available in centers with fewer resources , which is why computed tomography ( ct ) has been evaluated as alternative , as most radiotherapy departments are equipped with a ct scanner [ 10 ]  . 
contouring on ct enables excellent visualization of the applicator and organs at risk ( oar ) , but also generally leads to an overestimation of the target volume compared to mri [ 10 ]  . increasing evidence shows that transrectal ultrasound ( trus ) might be a more promising and inexpensive alternative . 
trus is extensively used in prostate brachytherapy , but apart from tumor assessment and conrming tandem placement , it has not been generally adopted in lacc brachytherapy to date [ 11 ]  . 
first studies investigating trus for target denition in lacc brachytherapy indicated that trus appears non - inferior to mri for assessing the highrisk clinical target volume ( ctvhr ) dimensions [ 12 , 13 ]  . as trus and ct are widely available in radiotherapy departments , combining their assets could possibly provide an equivalent for mri in contouring target volumes in igabt for lacc . 
a clinical workow for combined trus / ct treatment planning in lacc brachytherapy has already been successfully simulated in a patient [ 14 ]  . if trus is further developed as a treatment planning modality , a trus / ct - based target delineation protocol should be developed to allow for volumetric trus - based contouring in routine clinical practice . 
as ultrasound is known for its observer dependence and previous studies on trus for lacc brachytherapy were performed only with a single observer , further research with multiple observers is mandatory as a key step towards development of trus - based brachytherapy . 
two patients had figo stage iib disease , three had stage iiic2 ( local : iib , iiib , iva , respectively ; figo version 2018 [ 15 ] )  . 
a somatom plus s scanner was used for ct ( siemens , erlangen , germany ) , in 2 - mm slice intervals without contrast mediut2 - weighted mri was performed with a 0.35 t system ( magnetom c , siemens ) with 5 - mm slice thickness , acquiring axial , para - axial , sagittal , and coronal images . trus system trus was performed with a dedicated prototype system developed for lacc brachytherapy allowing for 3dtrus imaging with automatic applicator reconstruction by optical tracking of the applicator ( medcom , germany ; elekta ; acmit , austria )  . 
the main principle of the system is that the trus probe and the applicator are xed to each other by a dedicated positioning arm and that tracking tools are positioned at specic reference geometries , which can be identied by the optical tracking systeoverall , the prototype consists of ( 1 ) a mobile cart with a pc equipped with ( 2 ) an imaging software ( gynus v2.0 , medcom ) ; ( 3 ) a 510 - mhz integrated trus transducer ( biopsee , medcom ) with a biplanar probe ( bipc6.5 / 10 / 128 , bipl7.5 / 70 / 128 ) , mounted to ( 4 ) a stepper unit ( ecrm , elekta ) with afxed ( 5 ) tracking tools ( acmit ) containing factory ndi trackers ( single - faced rigid bodies ) tracked by ( 6 ) a ceiling - mounted polaris spectra system ( ndi , canada ) ; and ( 7 ) multi - dof passive positioning arms connecting the applicator to the stepper unit ( baitella , switzerland ) , and connecting the complete imaging unit to the operating tables side rail ( mfa , isys medizintechnik , austria )  . 
further technical details have been published elsewhere [ 16 , 17 ]  . trus imaging and tracking procedure after applicator insertion , the trus probe with the stepper unit and loose mfa arms was placed manually in the strahlenther onkol ( 2020 ) 196 : 983992 rectum at the optimal depth and angle according to the position and exure of the uterus / applicator . 
the mfa arm was locked and the stepper unit subsequently connected to the applicator with the second positioning arimage acquisition was performed during automated rotation of the trus probe , generating a 3d volume using the longitudinal array of the probe from the level of the ring applicator to the fundus of uterus , if reachable . 
the reconstruction process was veried within a plausibility check based on several reference structures ( tandem , posterior curvature of the ring , rotation of the ring as indicated by the holes , interstitial needles ) and ne - tuned , if necessary . 
for trus - based contouring , only one observer was experienced . all investigators were given an introductory course on trus contouring by the experienced investigator and two test cases were contoured by all investigators . 
after approval of these cases , the study cases could be contoured . investigators were provided with the following material : clinical information of each patient , a pelvic mri at diagnosis , and a 3d clinical drawing of the gynecological examination at diagnosis and at the time of brachytherapy [ 18 ]  . all investigators contoured each case independently following the workow dened in fig . 
first , the ctvhr was contoured on ct ( ctvhr _ct ) according to the consensus guidelines for ct - based brachytherapy , dened by the complete mass ( cervical + parametrial ) at intermediate fig . 
trus transrectal ultrasound , ct computed tomography , bt brachytherapy , mri magnetic resonance imaging , mriref reference high - risk clinical target volume ( ctvhr ) on density ( grey / white )  . 
the ctvhr height on ct was determined by the gtv height on the mri at diagnosis [ 10 ]  . secondly , the ctvhr was contoured on trus ( ctvhr_trus ) , dened by a hypoechogenic mass ( cervical + parametrial ) on grey - scale imaging [ 13 ]  . 
after contouring this preliminary target volume on trus , the structures were resampled to ct and adapted according to the oar depicted on ct ( ctvhr_trus - ct )  . 
the ctvhr height on trus - ct was determined by the gtv height on the mri at diagnosis . next , the ctvhr was contoured on mri ( ctvhr_mri ) according to the recommendations for mr - based brachytherapy as the whole cervix and any residual disease at time of brachytherapy including grey zones [ 19 , 20 ]  . finally , a reference contour on mri ( mriref ) was generated for each patient , attained by reaching consensus amongst all observers . analysis of contouring deviations for each imaging modality , the maximum width ( maximum latero - lateral diameter found in all para - axial slices ) , the maximum thickness ( maximum antero - posterior diameter found in all para - axial slices ) , the maximum height ( maximum cranio - caudal diameter found in all sagittal slices ) , and the total volume of each ctvhr from every observer was measured for each patient . ct and mri images were automatically registered with trus - ct images based on the applicator position , serving as a common reference coordinate system dened on the tps [ 21 ]  . 
to assess interobserver variations , all images and contours were exported to the slicerrt software system , version 4.5.0 - 1 ( slicerrt community and percutaneous surgery laboratory , queens university , canada ) [ 22 ]  . 
contours of every observer were compared with one another and with the mriref . the coefcient of variation ( cov ) was dened as the standard deviation divided by the mean value and is larger with increasing variability ( more dispersion in the data )  . a generalized conformity index ( cigen ) was dened as the ratio of the sum of all overlapping volumes between pairs of observers and the sum of all overlapping and all additional volumes between the same pairs [ 23 ]  . 
contours from all observers are projected on the ct dataset : mri contours in pink , trus contours in green , ct contours in blue results the proposed workow of hybrid trus - ct with optical tracking of the applicator was successfully applied . 
4 relative over - / underestimation of the mean volume of the high - risk clinical target volume ( ctvhr ; a ) and mean width of the ctvhr ( b ) on ct ( black ) and on trus - ct ( grey ) compared to the reference ctvhr on mri for all patients . 
pt patient , ct computed tomography , trus - ct transrectal ultrasound combined with computed tomography discussion contouring uncertainties due to poor target volume visualization have a substantial impact on tumor coverage and dose to oar . 
mri is currently considered the gold standard for target volume contouring in igabt in lacc because of the high tissue contrast in pelvic anatomy [ 10 , 20 ] , but is not always accessible due to its cost . 
therefore , ct could serve as a plausible alternative , but literature on the comparison of ctand mri - based contouring showed a substantial overestimation of ctvhr volume on ct [ 18 , 24 , 25 ]  . 
recently , trus has been considered as an imaging modality for igabt , since it provides excellent soft tissue contrast and has already proven its advantages in prostate cancer brachytherapy [ 26 ]  . 
suggested implementing trus in the preand intraoperative setting to assess the ctvhr before applicator insertion , for preplanning purposes , and for trus - guided tandem and needle insertion [ 12 ]  . 
a comparison of the target volume dimensions between trus and mri showed no statistically signicant difference for the ctvhr width , indicating the high potential of trus for igabt in lacc [ 13 ]  . 
 [ 14 ] , showing that trus - ctbased volumetric contouring and treatment planning is feasible and may be clinically comparable to the mri - based approach . in this report , volumetric contouring for lacc on 3dtrus with multiple observers was investigated for the rst time . 
the previously described workow for trus - ct treatment planning proved feasible within this prospective pilot study and all observers managed to follow a contouring protocol for combined trus - ct - based ctvhr contouring . 
particularly the trus probe positioning and imaging process using a table - mounted exible stepper unit in combination with xation devices was a substantial improvement in comparison to the system used in our previous studies . 
it appears that with such a system , the previously reported substantial proportion ( ( cid : 2 ) 20% ) of patients not suitable for trus imaging with applicator could be signicantly reduced . 
since the location of the applicator , particularly the ring - component , cant be dened on trus with reasonable accuracy for subsequent treatment planning , optical tracking of the applicator was implemented in the system to allow for automatic applicator reconstruction in the trus dataset . 
extensive phantom and clinical tests were performed in advance to learn and improve the tracking procedure ; however , optical tracking is sensitive to various interferences and shows limitations in daily clinical practice for lacc brachytherapy in its current fornevertheless , automatic applicator reconstruction using applicator library models was successfully performed , with some minor manual adjustments , in all patients in this study . 
further optimization and investigation of alternative tracking modalities , such as electromagnetic or mechanical tracking , are necessary . in accordance with our previous study , the mean maximum width of the ctvhr on trus - ct was smaller than on ct alone and comparable to mri , indicating the reproducibility of these previous ndings with multiple observers . 
as expected , the variation for the mri contours was smaller ( mean cov = 0.1 and mean cigen = 0.75 between all observers and with regard to the mriref volume ) , whereas the mean ctvhr volume was similar between trus - ct ( 46 cm3 ) and mri ( 43 cm3 )  . 
performance of trus appears to have a similar impact on interobserver variation as a pre - brachytherapy mri scan , but with the advantage of having the applicator already in place as a reference structure . 
especially the limited depth of insertion of the transrectal probe in the presence of the applicator hampers depiction of the most cranial parts of the uterus , as was the case for the presented cases . 
also , the anterior border of the ctvhr adjacent to the bladder was more difcult to assess , due to the distance from the probe and acoustic shadowing by the applicator , resulting in a wider range in the maximum thickness on trus - ct compared to mri . 
the presence of the trus probe can also cause compression of the uterus , leading to a reduced thickness of the ctvhr as shown in our previous study [ 13 ]  . 
the posterior and lateral parts of the cervix were well dened on trus , resulting in a consistently comparable range in the maximum width on trus - ct and mri . 
in two patients , the maximum width on trus - ct was smaller compared to the mriref contour ( 15% and 3% in patients 4 and 5 , respectively ) , which should be interpreted with caution as the absolute differences are minor ( 8 mm 2 mm for patient 4 and 1 mm 2 mm for patient 5 ) , but needs to be taken seriously , as this could result in a potential topographical miss by trus - ct . 
a similar learning curve as described for trusbased prostate brachytherapy can be assumed for trus in lacc brachytherapy [ 29 , 30 ]  . the present study covers interobserver contouring using trus - ct as one step further in the development of trus as a possible treatment modality in igabt . 
however , other key questions remain to be answered , in particular regarding optimization of the imaging and tracking procedure , the performance of trus by multiple observers , and the actual treatment of patients by any form of trus - based brachytherapy within a clinical study . conclusion trus - ct - based contouring in igabt for lacc with automatic applicator reconstruction by optical tracking is feasible after a minimal amount of training , is consistent amongst multiple observers , and leads to reduced volumes compared to ct alone . 
this prospective interobserver analysis could be the next step in the shift from trus being just an aid for tumor assessment and tandem placement verication during the procedure , to an accessible alternative to mri for ctvhr contouring . funding the department of radiotherapy at the medical university of vienna receives / received nancial and / or equipment support for research and educational purposes from nucletron , an elekta company . this work was supported by acmit , the austrian center for medical innovation and technology , which is funded within the scope of the strahlenther onkol ( 2020 ) 196 : 983992 comet , competence centers for excellent technologies , program and funded by the federal government ( bmvit and bmwfw ) and the governments of lower austria and tyrol , austria . 
this project was funded in part via a research contract from elekta . funding open access funding provided by medical university of vienna . compliance with ethical guidelines conict of interest s . 
schmid declare the following : the department of radiotherapy at the medical university of vienna receives / received nancial and / or equipment support for research and educational purposes from nucletron , an elekta company . 
this work was supported by acmit , the austrian center for medical innovation and technology , which is funded within the scope of the comet , competence centers for excellent technologies , program and funded by the federal government ( bmvit and bmwfw ) and the governments of lower austria and tyrol , austria . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
august 2020 springer - verlag gmbh germany , part of springer nature 2020 hintergrund und fragestellung mangelnde krperliche belastbarkeit ( belastungsintoleranz ) ist in der allgemeinbevlkerung insbesondere mit herzinsufzienz assoziiert . hier ist dieses symptom negativ korreliert mit der lebenserwartung . hinsichtlich der prvalenz und der bedeutung der krperlichen belastbarkeit bei langzeitberlebenden von krebserkrankungen im kindesalter gibt es jedoch nur wenige daten . 
kardialer mortalitt gut bekannt , ob jedoch die krperliche belastbarkeit eine hnliche korrelation zur mortalitt aufweist wie in der normalbevlkerung , ist bislang nicht untersucht . krperliche belastbarkeit setzt sich aus einer vielzahl physiologischer und pathophysiologischer faktoren des kardiovaskulren , pulmonalen , muskulren und neurosensorischen systems zusammen sowie aus lebensgewohnheiten und psychologischen einstellungen . die studie von ness et al . 
untersuchte die prvalenz der belastungsintoleranz bei langzeitberlebenden pdiatrischer krebserkrankungen , die einer kardiotoxischen therapie ausgesetzt waren , und verglich die funktionalitt veroriginalpublikation ness kk , plana jc , joshi vm et al ( 2019 ) exercise intolerance , mortality , and organ system impairment in adult survivors of childhood cancer . 
aus diesem kollektiv wurden 1041 patienten rekrutiert , die im zentrum zwischen 1962 und 2007 behandelt wurden , zum zeitpunkt der studie > 18 jahre alt waren , die tumorerkrankung 10 jahre berlebt hatten und keine angeborene herzerkrankung aufwiesen . 
um die statistische aussagekraft zu verbessern , wurden die teilnehmer vor rekrutierung stratiziert nach kardiotoxischer therapiebelastung ( thorakale bestrahlung , kumulative anthrazyklindosis ) , um einen healthy participation bias zu vermeiden . als vergleichsgruppe wurden zustzlich n = 285 probanden ohne pdiatrische tumorerkrankung in der vorgeschichte aus dem umfeld des zentrums und der patienten rekrutiert . die untersuchungen bestanden aus anthropometrischen messungen , erfassung des lebensumfelds und der konsumgewohnheiten ( risikofaktoren wie rauchen und trinken , aber auch qualitt der ernhrung )  . 
als belastungsintoleranz wurde eine relative maximale sauerstoffaufnahme ( vo2max in ml / kg / min ) von < 85 % des normwerts deniert , eine niedrige kardiopulmonale fitness als maximale aerobe leistungsfhigkeit von < 7 , 9 met ( 1 met entspricht der sauerstoffaufnahme unter ruhebedingungen von 3 , 5 ml / kg / min )  . 
auch wurde die muskelkraft ermittelt ( quadrizeps ) und eine neurologische befragung und untersuchung durchgefhrt zur erhebung der modied total neuropathy scale ( mtns )  . um die belastbarkeit zwischen den berlebenden zu vergleichen , wurde eine multivariable regression der erhobenen daten durchgefhrt . 
es wurde die gruppe , die mit einer kardiotoxischen therapie exponiert war ( ex - gruppe ) , der gruppe , die nicht exponiert war ( n - ex - gruppe ) und der gesunden vergleichsgruppe gegenbergestellt . 
ebenso wurden die zusammenhnge zwischen der ehemaligen therapie , den organfunktionen sowie der belastungsintoleranz und der letalitt statistisch bewertet . ergebnisse von den 1041 rekrutierten und untersuchten patienten waren n = 666 hinsichtlich einer kardiotoxischen therapie exponiert gewesen , n = 375 nicht . 
zwischen der ex - gruppe und der n - ex - gruppe bestanden keine signikanten unterschiede im body - mass - index und anderen anthropometrischen werten , allerdings zeigte die gesunde vergleichsgruppe mit einem geringeren krperfettanteil im vergleich zu den patienten gnstigere anthropometrische werte . 
51 , 5 % der ex - gruppe war im bereich des thorax mit im mittel 26 gy ( 2035 gy ) bestrahlt worden , 45 , 8 % dieser gruppe hatten ( im vergleich zu 8 , 8 % der n - ex - gruppe ) eine abdominelle radiatio erhalten . 
64 % in der ex - gruppe , mit 56 % in der n - ex - gruppe und mit 26 % in der kontrolle . eine niedrige kardiopulmonale fitness war messbar mit ca . 
die fr diverse risikofaktoren adjustierte hazard ratio fr die gesamtmortalitt betrug 3 , 93 ( 95% - ki 1 , 0914 , 14 ) fr berlebende mit belastungsintoleranz im vergleich zu patienten ohne belastungsintoleranz . der einuss der stattgehabten therapien auf die endpunkte wurde ebenfalls untersucht . 
so war beispielsweise eine reduzierte mittlere maximale sauerstoffaufnahme assoziiert mit > 350 mg / m2 anthrazyklinen , > 30 gy thorakaler bestrahlung , > 20 gy kranieller bestrahlung und carboplatin den korrelationen der verschiedenen in der echokardiographie erhobenen parameter war auffllig , dass eine erhhte gls , aber nicht eine reduzierte ef mit der belastungsintoleranz assoziiert war . schlussfolgerungen der autoren eine belastungsintoleranz bei 35 - jhrigen erwachsenen nach erfolgreicher behandlung pdiatrischer tumoren , die so ausgeprgt ist wie bei 70bis 80 - jhrigen vergleichskollektiven , ist ein unabhngiger prdiktor fr mortalitt . weiterhin scheint die echokardiographische bestimmung der gls bei asymptomatischen patienten einen besseren hinweis auf eine solche symptomatik geben zu knnen als die bestimmung der ef . neben behandlungsbedingten kardialen einschrnkungen erhhen pulmonale und muskulre beeintrchtigungen das risiko einer belastungsintoleranz . 
mit aufwendigen , validierten verfahren wurde die oft nur subjektiv wahrgenommene verschlechterung der krperlichen leisstrahlenther onkol ( 2020 ) 196 : 10551057 1057 thrazykline , haben langfristige einschrnkungen verschiedener organfunktionen zur folge . 
diese knnen sich auch bei klinisch unaufflligen patienten als belastungsintoleranz manifestieren . ( cid : 2 ) diese belastungsintoleranz ist bei ber 60 % der jungen erwachsenen langzeitberlebenden in der kommentierten studie so ausgeprgt wie bei gesunden erwachsenen im alter von 70 und 80 lebensjahren . ( cid : 2 ) die belastungsintoleranz scheint direkt mit dem gesamtmortalittsrisiko in dieser patientengruppe assoziiert zu sein wie brigens auch in der gesamtbevlkerung . ( cid : 2 ) asymptomatische berlebende von krebserkrankungen im kindesalter , die einer bestrahlung im thoraxoder schdelbereich oder anthrazyklinen , alkylanzien oder platin ausgesetzt waren , sollten deshalb auf solche vernderungen untersucht werden , bevor eine verstrkte krperliche bettigung und verschiedene aktivittsmanahmen empfohlen , durchgefhrt oder erwartet werden . ( cid : 2 ) langzeitnachsorgeprogramme knnen fr diese risikokohorte in deutschland angeboten werden . diana steinmann , hannover ; thorsten langer , lbeck ; tienush rassaf , essen und robert michael hermann , westerstede interessenkonikt d . 
gebauer j , baust k , bardi e et al ( 2020 ) guidelines for long - term follow - up after childhood cancer : practical implications for the daily work . 
so wurden zur charakterisierung der belastungsintoleranz eine standardisierte spiroergometrie und weiterfhrende kardiopulmonale testungen eingesetzt . dabei stellte sich heraus , dass neben den bekannten faktoren fr eine mortalitt in dieser population wie rckfall , zweittumoren , kardiovaskulre und pulmonale erkrankungen oder inaktivitt auch als neuer risikofaktor die belastungsintoleranz deniert werden kann . 
die inzidenz dieses symptoms mit 64 % in der ex - gruppe erschreckend hoch wird in der studie wahrscheinlich sogar noch unterschtzt , da berlebende , die die kardiopulmonale testung nicht abschlieen konnten , fr die analyse ausschieden . 
die dynamik einer solchen entwicklung , konnten somit nicht beurteilt werden . die korrelation zwischen belastungsintoleranz und fast 4 - fach erhhtem mortalittsrisiko erscheint plausibel , auch wenn die nachbeobachtungszeit , auf die sich die kalkulation der hazard ratio fr das mortalittsrisiko bezieht , mit 4 jahren und relativ wenig ereignissen recht kurz erscheint . 
in multivariate analysis , an increased number of oligometastases and untreated primary pc were negative predictors for os ; advanced clinical tumor stage , untreated primary pc , bed3 value of 108 gy , and mdt with conventional fractionation were negative predictors for pfs . 
no patient experienced grade 3 acute toxicity , but one patient had a late grade 3 toxicity of compression fracture after spinal sbrt . conclusion 68ga - psma - pet / ct - based mdt is an efcient and safe treatment for oligometastatic pc patients . 
after initial curative treatment , approximately 20% of patients have disease recurrence and less than 5% of prostate cancer patients have metastatic disease at diagnosis [ 2 , 3 ]  . 
however , there is a subset of patients with a limited number of metastases , described as an oligometastatic state by hellman and weichselbaum [ 5 ] , who may benet from local ablative treatments . 
synchronous or metachronous oligometastatic disease is a transitional state between localized and widespread metastatic disease with the presence of 3 to 5 or fewer metastatic sites on imaging . there is a great interest in obtaining prolonged remission and possibly cure in this patient population . 
recently , the phase ii randomized sabr - comet study demonstrated an overall survival ( os ) benet of stereotactic body radiotherapy ( sbrt ) in oligometastatic patients compared to standard - of - care systemic therapy [ 6 ]  . 
two phase ii randomized clinical trials also showed improved progression - free survival ( pfs ) in oligometastatic pc patients treated with metastasis - directed therapy ( mdt ) using sbrt compared to surveillance [ 14 , 15 ]  . the efciency of mdt depends on the accuracy of imaging methods in detecting all oligometastatic disease sites , while avoiding unnecessary treatment of patients with highvolume metastatic disease . 
in other words , it is critical to dene which patients truly have oligometastatic disease . technological advances in prostate imaging over the past decade have increased the sensitivity of detecting even the miniscule metastases which were previously undetectable by conventional imaging modalities . 
functional imaging techniques like positron - emission tomography ( pet ) scans of 18f - uciclovine and 11c - choline have higher sensitivity and specicity for detection of pc recurrence ; however , these tracers have limited sensitivity for detection of recurrence [ 16 , 17 ]  . 
the gallium prostate - specic membrane antigen ( 68ga - psma ) ligand , which is a transmembrane glycoprotein enzyme predominantly located in the extracellular space and highly expressed in pc cells , has emerged as a promising pet tracer for pc patients . 
furthermore , 68ga - psma - pet / ct is more sensitive in detecting lymph nodes and distant metastases than conventional imaging modalities and other pet tracers [ 18 ]  . 
the role of 68gapsma - pet / ct in treatment decision making , radiotherapy planning , and identifying recurrence after prostatectomy or denitive rt has been previously reported in patients with locally advanced pc [ 1922 ]  . 
however , the data are limited regarding the effect of mdt based on 68gapsma - pet / ct in oligometastatic pc patients [ 13 , 2325 ]  . while there is no consensus on the number of metastases for oligometastatic disease denition , 3 metastases was mostly accepted as oligometastatic pc [ 7 , 13 , 14 , 24 ] and in rare cases , 5 metastases were used as oligometastatic pc [ 23 , 26 ]  . based on these ndings , the aim of this study is to assess the outcomes of 68ga - psma - pet / ct based mdt in synchronous or metachronous oligometastatic pc patients with 5 bone and / or lymph node metastases . 
in addition , the prognostic factors effecting survival were analyzed . materials and methods patient selection in this multi - institutional turkish radiation oncology group ( trog ) study , clinical data of 176 biopsy proven pc patients treated between 2014 and 2019 were collected from 10 institutions . in this multi - institutional trog study , a standard database sheet was sent to each institution for patient enrollment . 
patients with synchronous or metachronous bone and / or lymph node metastasis limited to 5 sites detected with 68ga - psma - pet / ct and with a minimum of 3 months follow - up after mdt were analyzed . 
patients included hormone - nave , hormone - sensitive , or castration - resistant disease , and concurrent adt and / or chemotherapy at the time of sbrt was allowed . 
patients with eastern cooperative oncology group ( ecog ) performance status of 2 or higher and patients treated previously with radiotherapy to the same oligometastatic site were excluded . the study was approved by the central ethical committee at hacettepe university ( go19 / 674 ) and had local approval from each department at which this was required . 68ga - psma - pet / ct imaging before mdt , all patients had pet imaging with a 68gapsma - targeting ligand . 
the median activity of intravenously injected 68ga - psma was 150 mbq ( range 78199 mbq )  . during the distribution phase , patients were asked to lie in the supine position in a quiet roocombined image acquisition began 60 min after 68ga - psma injection . 
in selected patients , contrast agents were used if the patients had no contraindications . the tumor was judged positive when focal tracer uptake of 1036 strahlenther onkol ( 2020 ) 196 : 10341043 the tumor was higher than that of the surrounding tissue [ 29 ]  . results patient outcomes radiotherapy planning the decision on mdt technique and radiotherapy dosing scheme had been made according to institutional protocols . institutions that were unable to treat patients with sbrt during the study period preferred to use intensity modulated radiation therapy ( imrt ) for mdt . 
psa failure was dened as psa nadir plus 2 ng / ml for those treated with denitive rt to the prostate primary , or psa of greater than 0.2 ng / ml for those who underwent prostatectomy . common criteria for adverse events ( ctcae ) version 4.0 was used for evaluation of acute toxicity and rtog / eortc late radiation morbidity scoring schema for late toxicity . statistical analysis statistical analysis was performed using spss 20.0 software ( spss for windows , ibm corp . , armonk , ny , usa )  . descriptive analysis was performed by calculating the mean , standard deviation , range , and median . 
time to progression after initial treatment for prostate cancer was calculated as the time period between the last day of surgery or radiotherapy , whichever was performed , and the diagnosis date of oligometastatic disease . 
time to death or progression was calculated as the period from the last date of mdt to the date of death or the rst clinical or imaging evidence of disease recurrence , whichever happened rst . 
the effect of age , gleason score , clinical t and n stages , use of adt , location and number of metastases , primary tumor treatment , mdt technique , time to oligometastasis , and biologically effective dose ( bed ) for mdt as potential prognostic factors for os and pfs were evaluated . 
seventy - ve patients ( 42.6% ) had bone only , 61 patients ( 34.7% ) had lymph node only metastasis , while 40 patients ( 22.7% ) had both bone and lymph node metastasis . 
of 101 patients with lymph node metastasis , 71 ( 70.3% ) had pelvic lymph node metastasis and 30 ( 29.7% ) had para - aortic lymph node metastasis . with a median follow - up time of 22.9 months ( range 3.377.8 months ) , 152 patients ( 86.4% ) were alive and 24 patients ( 13.6% ) had died ( 22 [ 12.0% ] of their disease ; 2 [ 9.6% ] of other causes ) at the time of publishing . 
of the 117 patients with relapse ( 66.5% ) , 28 patients ( 47.5% ) had diffuse metastatic relapse , 22 ( 37.2% ) had oligorecurrence , and 9 ( 15.3% ) had biochemical failure only . of 59 patients with progression after mdt , 18 continued to adt , 15 patients received systemic chemotherapy together with adt , 8 patients switched to next - generation hormonotherapy ( abiraterone or enzalutamide ) , 11 patients received mdt to the oligometastatic site , 5 patients were treated with palliative radiotherapy , and 2 patients had lutetium - 177 psma therapy . the 2 - year os rate was 87.6% and median os was not reached . 
clinical tumor stage , number of oligometastasis , oligometastasis treatment technique , lower bed of mdt , and treatment status of primary prostate cancer were prognostic factors for pfs in univariate analysis ( table 2 )  . 
in multivariate analysis , advanced clinical tumor stage , untreated primary , lower bed , and mdt with conventional fractionation were signicant negative predictors for pfs ( table 3 )  . eects of mdt technique in patients treated with sbrt ( 129 patients , 73% ) , median fraction number was 3 ( range 15 ) , median fraction and total doses were 9 gy ( range 524 gy ) and 27 gy ( range 1540 gy ) , respectively . 
mdt was performed with sbrt in 62 patients ( 48.1% ) with bone metastases , 40 patients ( 31.0% ) with lymph node metastases , and 27 patients ( 21.9% ) with bone and lymph node metastases . 
the median fraction number for patients treated with conventional radiotherapy was 28 ( range 2539 ) , and median fraction and total radiation doses were 2 gy ( range 1.82.0 gy ) and 60 gy ( 4078 gy ) , respectively . 
only 6 patients ( 3.4% ) had grade 1 and 3 patients ( 1.7% ) grade 2 late toxicities . only one patient had a compression fracture of vertebra 11 months after completion of mdt . 
this patient had a single metastasis at the thoracic vertebra and was treated with a single dose of 24 gy using sbrt technique . in this multi - institutional study , we demonstrated that 68ga - psma - pet / ct - based mdt in metachronous or synchronous oligometastatic pc patients is effective and well tolerated . 
with a median follow - up of 22.9 months , median pfs was 39.3 months , which is more than recent studies and may be related to synergistic effects of mdt and concurrent adt ( 79.5% had adt during mdt )  . 
only one patient had late grade 3 toxicity which was a vertebral compression fraction after single - dose 24 gy sbrt . the standard management of metastatic pc is systemic treatment with adt with or without docetaxel [ 4 ]  . 
however , the oligometastatic state previously described by hellman and weichselbaum [ 5 ] may benet from localized therapies , and mounting prospective evidence supports the inclusion of radiotherapy in the metastatic paradigseveral retrospective and prospective studies have demonstrated the os overall survival , pfs progression - free survival , rt radiotherapy , sbrt stereotactic body radiotherapy , bed biologically equivalent dose diation technique and bed of mdt had no signicant effect on os . 
seven of 9 patients with recurrence at the oligometastatic site treated with mdt had conventional fractionation therapy , while only 2 patients treated with sbrt had local recurrence at the treated site . 
all patients with local recurrence at the mdt site received bed 108 gy . strahlenther onkol ( 2020 ) 196 : 10341043 1039 table 3 multivariate analysis of prognostic factors for overall and progression - free survival variables risk factors hr ( 95% ci ) p - value overall survival number of metastasis primary tumor treatment progression - free survival number of metastasis clinical tumor stage primary tumor treatment metastasis treatment modality absent vs . 
2 kaplanmeier patient survival estimates : overall survival in patients with single metastasis and > 1 metastasis ( a ) , 13 metastases and 45 metastases ( c ) ; progression - free survival in patients with single metastasis and > 1 metastasis ( b ) , 13 metastases and 45 metastases ( d ) 1040 strahlenther onkol ( 2020 ) 196 : 10341043 feasibility of mdt in oligometastatic pc patients [ 6 , 7 , 10 , 1215 , 25 ]  . 
 [ 7 ] analyzed 33 oligorecurrent pc patients after single - dose 20 gy sbrt to the oligometastatic lesion and showed that 2 - year adt - free survival was 48% . 
furthermore , these studies showed that while mdt is effective in delaying progression , complete eradication of micrometastases is not applicable , since most of the patients do not have a complete psa response after mdt . 
in a review by ost et al . [ 31 ] with 450 patients receiving mdt and 61% of patients with adjuvant adt , the authors demonstrated that 51% of patients were progression free . 
although os rates were close to previous series [ 30 ] , median pfs was somewhat longer than previous studies , which may be due to the fact that the majority of patients received adjuvant adt . 
we could not demonstrate a signicant difference between patients receiving adjuvant adt and those not having adt , because of heterogeneity in the adt period and discordance in patient numbers between the two groups . 
however , in the current study , adt was continued in 41 of 59 patients with progression after mdt , of whom 18 patients received only adt , 15 patients received systemic chemotherapy together with adt , and 8 patients switched to next - generation hormonotherapy ( abiraterone or enzalutamide )  . 
physicians preferred to switch to chemotherapy in more patients compared to nextgeneration hormonotherapy , which may be largely due to the discordance in the observation period of the study and the approval time of next - generation hormonotherapy in turkey . 
although the standard approach for patients with progression after mdt is not yet known , numerous ongoing studies will shed light on this situation . in order to dene true oligometastatic disease and treat all involved disease sites appropriately , imaging modalities are crucial . 
traditional staging techniques , which used bone scintigraphy and ct , frequently lead to understaging due to poor sensitivity and specicity for detection of metastases , particularly in small lymph nodes , and they are suboptimal for detection of bone metastases [ 32 ]  . 
few studies have evaluated the feasibility of 68ga - psma - pet / ct - directed mdt in oligometastatic or oligorecurrent pc patients ( table 4 ; [ 13 , 2325 ] )  . 
the authors developed a risk classication for biochemical relapsefree survival after psma - pet - guided mdt , and found that patients with psa < 0.8 ng / ml and local relapse only had the most promising survival . 
the results of previous studies display variations due to a wide range of doses and fractionations used for sbrt delivery , different numbers of metastases , and various metastatic sites . 
although there is no consensus on the number of metastases in oligometastatic patients and most studies accept 3 metastases , we and other recently published series using 68ga - psma - pet / ct prefer to use 5 for denition of oligometastasis [ 15 , 23 ]  . 
 [ 13 ] ln or bone ( 88% ) rt ( 12% ) prospective brfs pre - sbrt 2 ng / ml poor prognono grade 2 acute or late toxicity strahlenther onkol ( 2020 ) 196 : 10341043 1041 table 4 published studies evaluating the outcomes of 68ga - psma - pet / ct - based metastasis - directed therapies guler et al . 
a recent review of 14 studies including 661 patients and 899 lesions treated with sbrt demonstrated no in - eld recurrences when radiotherapy doses exceeded a bed of 108 gy [ 34 ]  . in the current study we found no in - eld recurrence in the mdt region in patients receiving bed > 108 gy , and only 2 patients treated with sbrt had in - eld recurrences . 
furthermore , treating the primary is also a signicant prognostic factor for better os and pfs , as was demonstrated in the recently published stampede trial [ 35 ]  . our study is not without inherent limitations because of its retrospective nature and associated selection biases . moreover , we could not perform histological verication in metastatic sites detected with 68ga - psma - pet / ct ; thus , we could not exclude psma - pet false - positive areas . 
in contrast to high specicity in detecting lymph node metastases , the reported sensitivity of 68ga - psma - pet / ct was 60% to 70% , due to lower detection rates of small lymph nodes , necessitating caution when interpreting negative scans . 
due to the retrospective nature of the study conducted in different centers , we were unable to gather data on whether the patient was castration sensitive or castration resistant at the time of mdt . 
despite these inherent limitations , this study is remarkable due to its relatively high number of patients and homogeneous patient population because only patients with bone and / or lymph node metastases with homogenous distribution were analyzed , while patients with visceral metastases were excluded . 
additionally , with a longer median follow - up , we could analyze prognostic factors for both os and pfs for oligometastatic pc patients treated with 68ga - psma - pet / ct - based mdt . conclusion in this study of a large cohort with relatively long follow - up , we demonstrated that 68ga - psma - pet / ct - based mdt is an efcient and a safe method for oligometastatic or oligoprogressive pc patients . 
higher bed to the oligometastatic site , sbrt technique , and lower clinical t stage improves pfs . complete consolidation of metastatic disease detectable by 68ga - psma - pet / ct decreases the risk of subsequent metastatic spread , suggesting an alteration in the traditional algorithms . 
in the no - pmrt subset , we compared various lymph node ( ln ) staging systems abilities to predict 5 - year overall and locoregional - free survival ( os / lrfs )  . methods we retrospectively enrolled 548 women with t1 - t2pn1 bc undergoing mastectomy and axillary ln dissection . depending on pmrt delivery , the participants were divided into the pmrt and no - pmrt groups . 
based on cox regression modelling , the number of positive lns ( pln ) , negative lns ( nln ) , ln ratio ( lnr ) , log odds of pln ( lodds ) , and modied lnr ( mlnr ) were modelled , each respectively , with os model covariates ( age , grade iii , lymphovascular invasion [ lvi ] , tumor size , hormone receptor [ hr ] status ) and lrfs model covariates ( age , grade iii , lvi )  . 
the c - statistic , akaike information criterion , and likelihood ratio 2 of the models were compared . results median follow - up was 60.5 ( 1882 ) , 61 ( 2882 ) , and 60 ( 1880 ) months for the entire cohort , pmrt , and no - pmrt group , respectively . 
in the no - pmrt group , lnr - based os / lrfs models exhibited superior prognostic performance . conclusion in early - stage bc patients undergoing mastectomies , ln dissections and no pmrt , we propose lnr - based multivariable models to predict os / lrfs with superior accuracy . keywords survival analysis mastectomy lymph node excision radiation treatment lymph node ratio introduction in the majority of early - stage breast carcinoma ( bc ) patients , reasonable local control of disease is maintained by breast - conserving surgery ( bcs ) followed by whole - breast radiotherapy ( rt ) [ 1 ]  . 
however , if the tumor is multifocal , inammatory , or large relative to breast size ; if there are ( cid : 2 ) domagoj kustic domagoj.kustic.d@gmail.com 1 department of nuclear medicine , clinical hospital center rijeka , rijeka , croatia 2 clinic for surgery , clinical hospital center rijeka , rijeka , diffuse microcalcications in the breast or positive margins remaining after wide local excision where further resections are not feasible , a mastectomy is advised [ 2 ]  . 
for the accurate assessment of prognosis , different ln staging systems have been proposed , including the american joint of committee on cancer ( ajcc ) pn system , the total number of positive lns ( plns ) , negative lns ( nlns ) , the ln ratio ( lnr ) , the log odds of plns ( lodds ) , and the modied lnr ( mlnr ) [ 4 , 712 ]  . croatia strahlenther onkol ( 2020 ) 196 : 10441054 1045 postmastectomy radiotherapy ( pmrt ) to the chest wall is an appropriate treatment for patients with t3 - t4 bc , with 4 plns , skin involvement , or positive margins of the mastectomy specimen [ 12 ]  . 
for selection of those among the latter suitable for pmrt , different risk factors are considered , especially younger age , plns , lymphovascular invasion ( lvi ) , and the total number of removed lns ( rlns ) [ 2 , 5 , 12 ]  . the objective was to investigate strategies concerning the use of pmrt at our institution in early - stage bc patients with limited ln involvement who underwent mastectomy and axillary ln dissection between 2007 and 2014 . we aimed to evaluate the prognostic capacity of various ln staging systems , modelled with common clinicopathological features producing collaborative effects on overall and locoregional - free survival ( os , lrfs ) , and select those with the best prognostic potential to guide further monitoring of t1 - t2pn1 bc patients who received no pmrt [ 1719 ]  . materials and methods patients and treatment we retrospectively enrolled 548 women with bc who underwent a mastectomy and axillary ln dissection at the clinical hospital center rijeka ( chcr ) between 2007 and 2014 . 
the inclusion criteria were newly diagnosed t1 - t2 bc , with no clinical or ultrasonographic evidence of regional ln involvement and no distant metastases at diagnosis , a mastectomy and axillary ln dissection with a total of 13 plns , negative margins after mastectomy , and receipt of the phenotype - based adjuvant systemic treatment according to the current st . 
patients with bilateral or recurrent bc and those with any other malignancies or who were receiving neoadjuvant rt or systemic therapy were not included . depending on pmrt delivery , the participants were divided into the pmrt and no - pmrt groups . 
a radiation dose of 50 gy in 25 daily fractions ( 2 gy per fraction ) was delivered using a siemens oncor impression linear accelerator ( siemens medical systems , erlangen , germany )  . 
the lymphatic regions received a dose of 30 gy by 6 - mv photons and 20 gy by electron beams . survival modelling and statistics the lnr was calculated as plns / rlns . 
as jin ml et al . [ 18 ] have proposed , the mlnr was calculated by adding 2 to the denominator of the standard lnr , as plns / ( rlns + 2 )  . 
the proportions of subjects experiencing events at 5 years were reported along with the corresponding 95% condence intervals ( 95% ci )  . predictors of os / lrfs were calculated for the no - pmrt group only . 
the variables considered as predictors were bc laterality , histologic type ( lobular or ductal ) , histologic grade , hr , her2 status , ki - 67 ( < 20% or 20% ) , the presence of lvi , and extranodal extension ( ene ) as categorical variables , in addition to age at diagnosis , tumor size , and ln involvement represented by ve staging systems , pln , nln , lnr , mlnr , and lodds , as continuous variables . for model construction , the variables mentioned above were evaluated by univariate cox regression analyses for os / lrfs . 
for ln staging systems , the evaluate cutpoints application ( r foundation for statistical computing , vienna , austria ) was employed to determine cutoffs based on the signicance of correlation with survival . 
based on these cutoffs , no - pmrt patients were dichotomized into risk categories and kaplanmeierbased log - rank testing was used to compare os / lrfs between the categories . hazard ratios with 95% cis were reported for the os / lrfs model predictor variables . 
model performances were evaluated in terms of discriminatory ability , predictive accuracy , and homogeneity using the concordance statistic ( c - index ) , akaike information criterion ( aic ) , and the likelihood ratio 2 test , respectively . 
the best performing os / lrfs models were selected based on the highest c - index , the highest likelihood ratio 2 , and the smallest aic value , representing the optimum prognostic stratication and predictive accuracy , and subjected to internal validation using bootstrapping with 1000 repetitions . 
based on the average predicted probability and the average observed probability of the outcome within each of the ten groups , scatter plots ( decile calibration plots ) were generated for the selected os / lrfs models . 
further , scatter plots were made representing the relationships of the ln staging system in the best performing model with the ln staging system from the second best and the ln staging system from the third best performing model . 
median follow - up was 60.5 ( 1882 ) , 61 ( 2882 ) , and 60 ( 1880 ) months , for the entire cohort , pmrt , and no - pmrt group , respectively . 
patients and tumor characteristics are summarized in table 1 . adjuvant chemotherapy was administered to 433 women ( 78.83% ) as either six cycles of cyclophosphamide , 5 - uorouracil , and an anthracycline , or four cycles of cyclophosphamide and an anthracycline followed by paclitaxel . 
multicollinearity among the ve ln staging indices was resolved by including them each into a separate multivariable cox proportional regression analysis to represent the ln involvement covariate , modelled with age , grade iii , and lvi as covariates in lrfs models , and with age , grade iii , lvi , tumor size , and hr status as covariates in os models ( table 4 )  . based on the highest c - index and the lowest aic value , the os model containing lnr and the lrfs model containing lnr performed best in predicting os / lrfs , both when tested on the entire no - pmrt cohort and when the analyses were restricted to those patients of the no - pmrt with 10 rlns . 
the differences between lrr rates reported by the meta - analysis and the rates observed in the more recent studies , including ours , were likely due to the more effective adjuvant systemic treatments and more extensive axillary ln clearance in the subjects of the later research [ 2531 ]  . no systematic attempt has been made to investigate whether consistent criteria had been used at our institution before 2015 in selecting appropriate candidates for pmrt among t1 - t2pn1 bc patients undergoing a mastectomy and axillary ln dissection . 
the participants receiving pmrt in this study were more likely to be aged 50 years and to have higher - grade tumors , with ki - 67 20% , lvi , ene , hr , her2 + status , more plns , and fewer nlns , as compared to the no - pmrt group . 
these observations are comparable to those made in previous research on larger samples [ 2629 ]  . lrfs of the subjects receiving no pmrt was negatively affected by younger age , grade iii , lvi , and ln involvement [ 8 , 26 , 30 ] , all of which were among variables previously mentioned as those prevailing in the patients selected for pmrt , indicating that the risk of lrr may be underestimated with low utilization of pmrt . 
among different ln staging systems representing ln involvement modelled with other clinicopathologic features affecting os / lrfs of no - pmrt patients , the lnr exhibited the best performance in predicting os and lrfs . the ajcc pn system has been criticized for limited discriminatory power in predicting the prognosis of bc subjects . 
some have suggested that the lnr may be used along with the traditional pn staging for t1 - t2pn1 bc patient risk stratication [ 8 , 39 ]  . the optimal lnr cutoff best separating the high - risk from the low - risk participants without pmrt in terms of os was 0.158 , and in terms of lrfs 0.154 , which was somewhat lower than that which kim si et al . 
however , diversity in ln staging cutoff values has been evident across studies , as a result of different methods used to determine the best cutoffs coupled with unbalanced sample sizes and different study designs . 
1 calibration plots comparing the observed and predicted probabilities of the binary outcomes for a the best performing overall survival and b the best performing locoregional recurrence - free survival model in t1 - t2 breast carcinoma patients with 13 positive axillary lymph nodes who received no postmastectomy radiotherapy ; c scatter plot showing consistency in the relationship between the lymph node ratio and the modied lymph node ratio as the best and the second best performing model in predicting survival of t1 - t2pn1 breast carcinoma patients who received no postmastectomy radiotherapy and d scatter plot showing consistency in the relationship between the lymph node ratio and the log odds of positive lymph nodes as the best and the third best performing model in predicting survival of t1 - t2pn1 breast carcinoma patients receiving no postmastectomy radiotherapy the signicance of continuous variables , ln staging indices were categorized based on the optimal cutoffs and models were tted with categorical variables . the lnr and its modication introduced to avoid zero values , the mlnr [ 18 ] , represented ln involvement covariates in the two models showing almost equal performances in os / lrfs prediction and being the best among the prognostic models tested on the entire no - pmrt cohort with any number of rlns . 
when we restricted the analyses to the subset of no - pmrt patients with 10 rlns , lnr and mlnr exhibited the best and the second best performance in predicting os / lrfs again , being almost equally successful in their survival predictions . 
similar observations have been reported recently [ 18 ]  . as has been acknowledged , the lnr system showed a decrease in prognostic accuracy with very high or low lnr values , as well as with an insufcient number of rlns ( < 10 ) in various malignant tumors , which may further lead to tumor stage underestimation [ 40 ]  . 
in contrast , not affected by the insufcient number of rlns , the lodds system has been recognized for its superior discriminatory power , distinguishing risk groups within the pn1 category of rectal , colon , pancreatic , and gastric cancer better than other staging systems , thus reducing the risk of staging migration [ 40 , 41 ]  . 
in the existing literature on bc , lodds was declared an independent prognosticator , with more reliable survival predictions compared to the pln and pn systems [ 7 , 10 ]  . 
in the no - pmrt group , both overall and limited to those participants having 10 rlns , the os model containing lodds and the lrfs model contain1052 strahlenther onkol ( 2020 ) 196 : 10441054 fig . 
in the no - pmrt group , the nlns showed a better ability to predict lrfs as compared to the pln systethe nlns outperformed the pln system in predicting lrfs also when we restricted the analyses only to the no - pmrt subset with 10 rlns [ 7 ]  . 
however , predictions made by the nln - based os prediction model were the least accurate . the retrospective methodology , the single - center nature , and the small sample size are the main limitations of this study . 
due to the small number of patients who received pmrt , the pmrt group was underrepresented , which may have limited the statistical relevance . in conclusion , among t1 - t2pn1 bc patients who previously underwent a mastectomy with axillary ln dissection and received phenotype - based adjuvant systemic treatment according to the current st gallen recommendations [ 19 , 20 ] without receiving pmrt , we identied the subset at higher risk of lrr , dened by grade iii , lvi , younger age , and ln involvement represented by different axillary ln staging systems . 
dezember 2019 springer - verlag gmbh germany , part of springer nature 2019 hintergrund das hepatozellulre karzinom ( hcc ) weltweit die dritthugste ursache , an krebs zu versterben . es neigt dazu , in das portalvense system einzubrechen und portalvenen - tumorthromben ( pvtt ) zu bilden . 
whrend die stereotaktische radiotherapie ( sbrt ) im vergleich zum sorafenib in allen anderen klinischen situationen zu einem lngeren berleben fhrte , bestand in einer aktuellen groen matched - pair - analyse bei vorliegen einer pvtt kein signikanter berlebensunterschied mehr [ 1 ]  . 
ziel der hier kommentierten studie war es , die berlebensergebnisse nach einer neoadjuvanten 3dkonformalen strahlentherapie ( rt ) , gefolgt von einer heoriginalpublikation wei x , jiang y , zhang x et al ( 2019 ) neoadjuvant three - dimensional conformal radiotherapy for resectable hepatocellular carcinoma with portal vein tumor thrombus : a randomized , open - label , multicenter controlled study . j clin oncol 37 ( 24 ) : 21412151 . 
voraussetzung war , dass die primrtumoren resektabel waren und eine pvtt des typ ii / iii nach cheng vorlag , was einem einbruch entweder in den rechten ast , den linken ast oder in den hauptstamm der pfortader entspricht . die patienten wurden randomisiert zu einer neoadjuvanten rt gefolgt von einer hepatektomie ( n = 82 ) oder zu einer alleinigen hepatektomie ( n = 82 )  . 
das makroskopische tumorvolumen ( gtv , gross tumor volume ) entsprach dem tumorvolumen in der arteriellen phase zusammen mit dem pvtt - volumen , das sich als fllungsdefekt in der portalvensen phase darstellte . 
eine expansion des gtv um 510 mm ergab das klinische zielvomumen ( ctv , clinical target volume ) und um weitere 510 mm das planungszielvolumen ( ptv , planning target volume )  . 
es wurden bildgefhrt ( conebeam - ct ) und mit atem - gating 6 3 gy in tglichen fraktionen bis zu einer gesamtdosis von 18 gy verschrieben und 3d - konformal geplant . 
die patienten im neoadjuvanten arm hatten ein restaging 4 wochen nach abschluss der rt und die resektion wurde innerhalb von fnf tagen durchgefhrt , wenn die patienten keine kontraindikationen gegen eine operation aufwiesen . 
die expression von interleukin - 6 ( il - 6 ) im patientenserum vor rt und in chirurgischen proben wurde mit der reaktion auf rt korreliert . ergebnisse von 237 patienten , die die einschlusskriterien erfllten , wurden 73 ausgeschlossen : 25 patienten , weil sie die einschlusskriterien nicht erfllten , und 48 patienten , strahlenther onkol ( 2020 ) 196 : 194196 weil sie das einverstndnis zur studienteilnahme zurckzogen . 
zwei patienten hatten nach der rt eine grad - 3lebertoxizitt und schieden daher fr die resektion aus . weitere zwei patienten mit grad - 2 - leberenzymerhhungen hatten eine normalisierung ihrer leberwerte nach einwchiger therapie mit glutathion und bicyclol . 
von diesen hatten 12 patienten ein downstaging von cheng - typ iii zu ii oder von ii zu i . bei 9 patienten im neoadjuvanten arm traten kontraindikationen gegen eine operation auf . 
die postoperative morbiditt und letalitt waren in beiden armen vergleichbar . die os - raten fr die neoadjuvante rt - gruppe betrugen nach 6 , 12 , 18 und 24 monaten je 89 , 0 % , 75 , 2 % , 43 , 9 % bzw . 
in multivariablen cox - regressionsanalysen reduzierte die neoadjuvante rt die hcc - spezischen mortalittsund hccrezidivraten signikant im vergleich zur alleinigen operation ( hazard ratio [ hr ] 0 , 35 ; 95 % - kondenzintervall [ ki ] 0 , 230 , 54 ; p = 0 , 001 und hr 0 , 45 ; 95 % - kl 0 , 310 , 64 ; p = 0 , 001 )  . 
erhhte expressionen von il - 6 im pr - rt - serum und - tumorgewebe waren signikant mit einer resistenz gegen die rt assoziiert . schlussfolgerung der autoren bei patienten mit resezierbaren hcc und pvtt lieferte die neoadjuvante rt signikant bessere postoperative berlebensergebnisse als eine operation alledie il - 6 - expression kann bei diesen patienten ein ansprechen auf rt vorhersagen . kommentar uicc - stadiengruppierung ( muicc ) vorgesehen [ 5 ]  . 
patienten mit hbvbedingtem hcc haben in der regel eine gute leberreserve , aber gleichzeitig eine rasche tumorprogression unter sorafenib im vergleich zu hcc - patienten auf dem boden von anderen lebererkrankungen . 
in ihr wurden 2093 patienten mit resektion mit 4381 patienten ohne resektion in einer propensityscore - analyse ( propensity - score matched - pair analysis ; [ 6 ] ) verglichen . 
solange in dieser studie die pvtt auf den zweig erster ordnung beschrnkt war ( cheng typ i / ii ) , war eine leberresektion mit einem lngeren berleben verbunden als bei einer nichtchirurgischen behandlung . 
bei vorliegen einer pvtt des cheng typ ii / iii hingegen ist die en - bloc - resektion des tumors zusammen mit der pvtt erschwert , sodass in dieser situation ein neoadjuvanter therapieansatz die prognose verbessern knnte . da systemische , neoadjuvante therapieanstze bei gleichzeitigem vorliegen einer pvtt wenig erfolgversprechend und auch andere lokal apparative verfahren schwierig einzusetzen sind , wurde in der vorgestellten studie der zustzliche wert einer vorgeschalteten rt getestet . die hypothese bei der studienplanung war , dass ... ( cid : 2 ) die rt zu einem downstaging der pvtt fhren knnte , ( cid : 2 ) das risiko einer intraoperativen tumorzellverschleppung reduziert wrde und ( cid : 2 ) darber hinaus die wahrscheinlichkeit einer kompletten resektion ( r0 ) ansteigen knnte . der behandlungsalgorithmus des hcc folgt in europa weitgehend den bclc - leitlinien [ 2 ]  . 
in asien , wo das hcc eine weit grere rolle spielt als in der westlichen hemisphre , wird die rt schon seit lngerer zeit regelmig und weitverbreitet fr die behandlung des hcc eingesetzt . 
diese beobachtung wird untersttzt von klinischen hinweisen auf eine gute wirksamkeit der rt in verbindung mit transarterieller chemoembolisation ( tace ) und intraarterieller chemotherapie bei pvtt [ 8 ]  . 
in einer randomisierten studie berichteten yoon und 196 strahlenther onkol ( 2020 ) 196 : 194196 mitarbeiter , dass im vergleich zum standardarm mit sorafenib eine kombination aus tace und rt bei jeweils 45 patienten zu einem besseren progressionsfreien berleben , einer hheren ansprechrate und besseren rezidivfreien berleben ( rfs ) fhrte [ 9 ]  . die hier vorgestellte randomisierte studie basiert auf einer retrospektiven analyse von 95 patienten , von denen sich 45 patienten in der neoadjuvanten rt - gruppe befanden . 
bei 12 dieser 45 patienten trat eine signikante verkleinerung der pvtt auf und berlebensanalysen zeigten , dass die neoadjuvante rt gefolgt von der resektion im vergleich zur alleinigen resektion mit einer signikanten lebensverlngerung und einer verlngerung des krankheitsfreien berlebens ( dfs ) verbunden war [ 10 ]  . 
die niedrige dosis von nur 18 gy in einzeldosen von 3 gy wurde fr die studie gewhlt , um mglichst wenig toxizitt am gesunden lebergewebe hervorzurufen und das intervall zwischen der neoadjuvanten therapie und der operation mglichst kurz zu halten . 
die studie von wei und mitarbeitern besttigte eine gute vertrglichkeit der neoadjuvanten rt sowie ein verlngertes berleben durch die verringerung des tumorvolumens in der pvtt , welches als schlechter prognostischer faktor nach einer resektion bekannt ist . 
das vorhandensein einer mikrovaskulren invasion war in der multivariaten analyse mit einer hr von 2 , 42 verbunden fr das risiko eines krankheitsspezischen todes und gleichzeitig der strkste negative prognostische faktor unter allen untersuchten parametern , whrend die neoadjuvante rt mit abstand der strkste positive prognostische faktor war ( hr 0 , 35 )  . 
so knnte dieser marker als prdiktiver faktor fr das ansprechen einer neoadjuvanten rt herangezogen werden . fazit die hier vorgestellte prospektive und randomisierte studie zeigt , dass eine neoadjuvante rt gefolgt von einer tumorresektion bei patienten mit hcc und pvtt eine lebensverlngerung und eine verlngerung des krankheitsfreien berlebens bewirkt . 
wenngleich diese ergebnisse noch nicht verallgemeinert werden knnen , weil patienten mit hcc auf dem boden einer hcv ausgeschlossen waren , kann diese studie dazu beitragen , den wert der rt bei der behandlung von patienten mit hcc mit evidenz zu belegen . 
bettinger d , pinato dj , schultheiss m , sharma r , rimassa l , pressiani t et al ( 2019 ) stereotactic body radiation therapy as an alternative treatment for patients with hepatocellular carcinoma compared to sorafenib : a propensity score analysis . 
european association for the study of the liver ( 2019 ) easl clinical practice guidelines : management of hepatocellular carcinoma . j hepatol 69 ( 1 ) : 182236 ( pubmed pmid : 29628281 ) 3 . 
le treut yp , hardwigsen j , ananian p , saisse j , gregoire e , richa h et al ( 2006 ) resection of hepatocellular carcinoma with tumor thrombus in the major vasculature . 
shi j , lai ec , li n , guo wx , xue j , lau wy et al ( 2010 ) surgical treatment of hepatocellular carcinoma with portal vein tumor thrombus . 
kokudo t , hasegawa k , matsuyama y , takayama t , izumi n , kadoya m et al ( 2016 ) survival benet of liver resection for hepatocellular carcinoma associated with portal vein invasion . 
shui y , yu w , ren x , guo y , xu j , ma t et al ( 2018 ) stereotactic body radiotherapy based treatment for hepatocellular carcinoma with extensive portal vein tumor thrombosis . 
radiation dose in biologically effective dose ( bed ) ( / = 10 ) was categorized as < 72 gy ( 261 patients ) and 72 gy ( 62 patients )  . 
additionally , propensity score matching was performed . results median follow - up time for patients who were alive at the time of analysis was 47 months ( range 18189 months )  . median overall survival after radiotherapy was 14 months . 
die strahlendosis in biologisch wirksamer dosis ( bed ; / = 10 ) wurde in die kategorien < 72 gy ( 261 patienten ) und 72 gy ( 62 patienten ) unterteilt . 
zustzlich wurde die propensity - score - matching - methode angewendet . ergebnisse die durchschnittliche follow - up - dauer fr patienten , die zum zeitpunkt der analyse am leben waren , betrug 47 monate ( spanne : 18189 monate )  . 
das durchschnittliche gesamtberleben nach der strahlentherapie betrug 14 monate . in der multivariaten analyse war bed 72 gy ein unabhngiger prdiktor fr eine gnstige lffr ( hazard ratio , hr : 0 , 32 ; 95% - kondenzintervall , 95% - ki : 0 , 140 , 72 ; p = 0 , 006 ) und pfr ( hr : 0 , 67 ; 95% - ki : 0 , 450 , 98 ; p = 0 , 04 )  . 
bei der strahlentherapie fr unvollstndige tace von hcc sollte die dosiseskalation mit sib - imrt bercksichtigt werden , um das onkologische ergebnis zu verbessern . schlsselwrter hepatozellulres karzinom transarterielle chemoembolisation strahlendosis - eskalation strahlentherapie intensittsmodulierte strahlentherapie introduction transarterial chemoembolization ( tace ) is the standard of care for barcelona clinic liver cancer intermediate stage [ 1 ] ; however , as shown in patterns of care studies , tace is also popularly used in cases beyond the intermediate stage [ 2 ]  . 
however , some studies have shown that single tace does not induce complete tumor necrosis , and repeated tace frequently becomes ineffective at some point during therapy [ 5 ]  . 
therefore , in order to overcome the weaknesses of tace , additional local treatment is required [ 6 ]  . radiotherapy ( rt ) can be an effective treatment option in adjunction to incomplete tace . 
tumor cells at the periphery , which remain viable through the blood supply from collateral circulation or recanalization of the embolized artery after tace , could be eradicated by rt [ 7 ]  . 
however , most of the previous studies adopted limited rt doses in order to preserve the surrounding gastrointestinal organs and nontumor - bearing liver parenchyma . recent developments in rt technology allowed application of higher rt doses to the tumor while sparing healthy liver tissue [ 22 ]  . 
at our institution , rt dose escalation has been applied to enhance its therapeutic effect using advanced rt technology , such as simultaneous integrated boost - intensity modulated radiation therapy ( sib - imrt )  . this study aimed to evaluate whether the escalated rt dose could improve oncologic treatment outcomes without increasing toxicities in patients with inoperable hcc who underwent tace but had an incomplete response . patients and methods patient selection we identied 323 patients with inoperable hcc who underwent rt after incomplete tace from february 2001 134 strahlenther onkol ( 2020 ) 196 : 132141 fig . 
physical doses of 75 and 60 gy in 25 fractions were prescribed to the internal target volume ( red contour ) and planning target volume ( blue contour ) , respectively . c ct scan at 4 months after sib - imrt showing the tumor shrinkage ( arrow ) to october 2016 . 
the inclusion criteria were as follows : ( 1 ) incomplete uptake of iodized oil based on enhanced computed tomography scan performed within 46 weeks after tace or newly seen enhancing soft tissue within post - tace lesion based on enhanced computed tomography scan performed within 3 months after tace , and rt was administered to the lesion previously treated by tace ; ( 2 ) childpugh class a or b disease ; ( 3 ) eastern cooperative oncology group performance status of 0 to 2 . 
the exclusion criteria were as follows : ( 1 ) presence of distant metastases , ( 2 ) other malignancies , ( 3 ) history of rt to abdominal area , ( 4 ) incomplete rt ( biologically effective dose [ bed ] < 40 gy ) due to patient refusal or poor general condition , and ( 5 ) stereotactic body radiotherapy with fractionated physical dose > 8 gy . 
this retrospective study was approved by the institutional review board of yonsei cancer center . radiotherapy protocols the denitions of target volumes and typical dose prescription are described in supplementary table 1 . 
gross tumor volume , as determined by dynamic enhanced computed tomography or magnetic resonance imaging , included enhanced tumor areas , complete tumor areas lled by lipiodoldoxorubicin or - cisplatin mixture , and tumor areas reecting complete tissue necrosis after tace . 
a 5 - mm margin around gross tumor volume was dened as clinical target volume , and a 5 - mm margin around clinical target volume was dened as planning target volume . 
four - dimensional computed tomography - based planning was adopted since 2010 ; internal target volume was delineated considering the tumor movement for every respiratory phase , and an additional 5 - mm margin around internal target volume and clinical target volume were dened as clinical and planning target volume , respectively . rt doses were customized to maximize the dose delivered to tumor while satisfying the normal organ dose constraints ( supplementary table 2 )  . 
gross tumor volume or internal target volume received a physical dose of 5075 gy in 2025 fractions using central sib technique , while the surrounding planning target volume received a lower physical dose of 4560 gy in 2025 fractions . 
for selected tumors with sufcient distance from luminal organs , gross tumor volume minus 1 cm was treated with central sib of 100 gy in 25 fractions ( physical dose )  . 
local failure - free rate ( lffr ) and outeld intrahepatic failure - free rate were calculated using the dened tumor progression inside and outside the rt eld , respectively . 
lffr , outeld intrahepatic failurefree rate , distant metastasis - free rate , progression - free rate ( pfr ) , and overall survival ( os ) were dened as the time between rt start date and rst event . 
classic radiation - induced liver disease ( rild ) was dened as elevated alkaline phosphatase levels ( more than twice the upper limit of normal or baseline value ) with anicteric hepatomegaly and ascites that developed within 3 months after rt . 
non - classic rild was dened as elevated liver transaminase levels ( more than ve times the upper limit of normal ) without documented disease progression or hepatitis b virus reactivation within 3 months after rt [ 24 ]  . statistical analysis for equal comparisons of dose effects of various fractionations , the maximum prescribed dose to tumor was calculated as bed ( / = 10 )  . 
to nd the optimal cut - off point for bed , we used the highest value of youden index ( sensitivity + specicity 1 ) and the corresponding cut - off point . youden index is a frequently used summary measure in the receiver operating characteristic curve , which enables the selection of an optimal threshold value [ 25 ]  . 
as a result , bed 72 gy was determined as the optimal cut - off point for predicting local control . propensity score generation and matching were performed by using the r package matchit [ 26 ]  . 
propensity score estimates were generated separately for each bed subgroup by using a logistic regression model derived from covariates inuencing treatment assignment and outcomes including age , sex , viral etiology , childpugh class , tumor size , number of tumors , gross vascular invasion , barcelona clinic liver cancer stage , treatment - naive , alpha - fetoprotein level , and prothrombin induced by vitamin k absenceii level . 
following propensity score generation , each patient in the high - dose group was matched to one patient in the low - dose group using nearest neighbor ( greedytype )  . 
after that , we assessed the differences in baseline covariates between the two groups using mcnemars test , mcnemarbowkers test , or paired t - test , as appropriate . survival rates were calculated using kaplanmeier method and compared using log - rank test . 
in multivariate analysis of all patents , bed 72 gy was a favorable prognostic factor for lffr ( hr 0.32 ; 95% ci 0.140.72 ; p = 0.006 ) and pfr ( hr 0.67 ; 95% ci 0.450.98 ; p = 0.04 ) , but it lost its signicance for os ( hr 0.83 ; 95% ci 0.581.17 ; p = 0.28 ; table 2 )  . propensity score matching analysis after propensity score matching , 62 patients in the lowdose group were matched to the 62 patients in the highdose group , and all relevant covariates including patient and tumor factors were well - balanced ( table 1 )  . 
in the highdose group , 1 patient had acute grade 3 radiation - related gastrointestinal bleeding at 2 months after rt completion , and 1 patient had late grade 3 gastrointestinal bleeding at 1 year after rt completion . 
in the low - dose group , one had acute grade 2 , one had acute grade 3 , two had late grade 2 , and 15 patients had late grade 3 radiation - related gastrointestinal bleeding . 
in addition , such favorable outcomes with rt dose escalation were achieved without increasing toxicity . the therapeutic advantage and safety of combining rt with tace have previously been proven in various reports [ 921 ]  . 
a meta - analysis of 25 trials involving 2577 patients found that patients treated with tace plus rt had improved tumor response and survival compared to patients treated with tace alone [ 19 ]  . 
when performing imageguided rt , daily cone - beam ct was taken , and lipiodol uptake remaining after tace could act as an internal ducial marker to ensure accurate localization . 
also , we applied a sib technique , which allows delivery of an ablative physical dose of 75100 gy to the center of the tumor , while maintaining the conventional dose for the surrounding subclinical spread region . 
despite application of a high dose to the intrahepatic tumor , rt planning was performed strictly within the range of our institutions dose constraints protocol ( supplementary table 2 )  . 
as a result , the mean liver dose and treatment - related toxicities did not signicantly increase in the high - dose group compared to the low - dose group . 
in addition , treatment - related toxicities were comparable to those previously reported [ 921 ]  . in patients using sib - imrt , the bed to the tumor core is 97.5140 gy , which is comparable to that of stereotactic body rt ( sbrt )  . 
in the high - dose group , the 1 - year lffr was 94% ( median size , 3 cm ) and this outcome is comparable to that of sbrt series with medium - sized tumors . a retrospective study reported 1 - year lffr of 88% in 42 recurrent hcc ( median size , 4 cm ) treated with sbrt [ 30 ]  . prospective phase i and ii trials of sbrt for hcc ( median size , 7 cm ) reported 1 - year lffr of 87% and showed acceptable toxicity [ 31 ]  . 
however , sbrt has strict contraindications involving proximity to the gastrointestinal tract and remnant liver volume less than 700 ml , in which conventional fractionation could rather be chosen using advanced techniques such as sib - imrt . although local failure was reduced in the high - dose group , intraand extra - hepatic metastasis accounted for the majority of failure patterns . 
while lffr substantially 140 strahlenther onkol ( 2020 ) 196 : 132141 improved , the outeld intrahepatic failure - free rate and distant metastasis - free rate did not improve with increased rt dose . 
since unresectable hcc is prone to intraand extrahepatic metastasis , combinations of local treatment and systemic targeted agents , such as sorafenib , may further improve os , although future trials assessing their efcacy are required . this study had several limitations , including its retrospective nature . 
to eliminate such confounding factors , we performed various statistical adjustments , including multivariate analysis and propensity score matching , but unrecognized biases may still exist . therefore , our ndings should be interpreted with some caution . in conclusion , rt dose escalation with bed 72 gy was associated with improved lffr and pfr . 
these improved treatment outcomes in the high - dose group were achieved without increasing treatment - related toxicity , which may have resulted from more frequent use of advanced rt technology , such as sib - imrt and image - guided rt . 
our results invite further prospective randomized trials to test the potential benet of rt dose escalation in combination with tace . funding this study was supported by the national nuclear r&d program through a national research foundation of korea ( nrf ) grant funded by the ministry of science and ict ( grant number : nrf2017m2a2a7a02070426 )  . compliance with ethical guidelines conict of interest h.k. 
schmidt5 birte friedrichs6 inga grnewald7 wolfgang hartmann7 georg lenz6 eva wardelmann7 normann willich1 hans theodor eich1 received : 1 september 2019 / accepted : 23 october 2019 / published online : 15 november 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract objective to evaluate clinical , histopathologic , and radiation ( rt ) dose parameters in patients with extranodal low - grade ( enlg ) non - hodgkin lymphoma ( nhl ) and their possible impact on local control ( lc ) and survival . materials and methods the medical records of 159 patients with 181 histologically conrmed enlg - nhl lesions treated at our institution were reviewed retrospectively . results the predominant histological subtype ( 73% ) was marginal zone lymphoma ( mzl )  . 
thirty - three ( 20% ) lesions were treated with reduced - dose rt ( ( cid : 2 ) 30.6 gy ) and 148 lesions ( 80% ) with conventional - dose rt ( > 30.6 gy ) , with an overall median dose of 39.6 gy ( range 463 )  . 
the median follow - up period was 72 months . the 10 - year local control ( lc ) , progression - free survival ( pfs ) , and overall survival ( os ) rates were 96 , 65 , and 82% , respectively . 
in the multivariate analysis , rt dose and timing ( upfront or salvage ) were related to lc , whereas age , histology , and complete response ( cr ) to rt were associated with pfs . 
patient age and radiation eld size impacted os . conclusion rt is an effective and curative local treatment for early - stage fl and mzl at conventional and reduced radiation doses . 
age , histology , and response to rt may inuence the pfs . keywords gastrointestinal tract skin head and neck orbit intensity - modulated involved - site radiotherapy ke and gr contributed equally . this study was presented at the annual meeting of the german society for radiation oncology , muenster , germany , june 1316 , 2019 . muenster , germany muenster , germany 4 department of dermatology , university hospital muenster , 3 department of ophthalmology , university hospital muenster , ( cid : 2 ) med . 
pathologically , fl originates from a germinal center and consists of cells coexpressing cd10 , cd20 , and b cell leukemia / lymphoma 2 ( bcl2 ) protein in about 85% of patients [ 2 ]  . 
mzl of mucosa - associated lymphoid tissue ( malt ) is a distinct extranodal b - cell lymphoma in which b cells frequently accumulate in response to chronic infection or autoimmune process [ 3 ]  . 
mzls involve most commonly the gastrointestinal tract ( git ) , ocular adnexa , and skin [ 3 , 4 ]  . radiotherapy ( rt ) remains an important treatment modality for patients with enlg - nhl . 
ultra - low - dose radiotherapy ( 4 gy in two fractions ) is an optional approach for symptom relief and durable control that can last approximately 18 months in selected patients with earlyor advanced - stage disease [ 913 ]  . due to enlg - nhl case heterogeneity and the lack of prospective trials , there is substantial variation in rt volumes and doses across treatment centers [ 1 ]  . 
lc , systemic relapse , and survival rates were compared across enlg - nhl histology subtypes in a large single - institute study consisting of 159 patients followed for up to 24 years . materials and methods we conducted a retrospective review of the medical records of 159 patients ( 86 males , 73 females ) with 181 histologically conrmed enlg - nhl lesions treated at our center between 1992 and 2018 ( table 1 )  . 
of the 59 patients with git lesions , 52 ( 88% ) had upper git ( stomach / duodenum ) lesions , and 7 ( 12% ) had lower git ( small and large intestine ) lesions . the majority of patients presented with early - stage disease . seventy percent of patients had stage i , 18% had stage ii , 3% had stage iii , and 9% had stage iv disease . 
among cutaneous nhl , 58% were t1 , 28% were t2 , and 14% strahlenther onkol ( 2020 ) 196 : 117125 were t3 according to the tnm classication [ 14 ]  . 
in the whole cohort , rt was performed as extended - eld rt ( efrt ) for 35 lesions ( in 35 patients ) , as involved - eld rt ( ifrt ) for 43 lesions ( in 42 patients ) , and as involved - site rt ( isrt ) for 103 lesions ( in 82 patients )  . 
common terminology criteria for adverse events version 4.0 was used to assess the toxicities . statistical analysis kaplanmeier time - dependent event curves were generated and compared with log - rank tests . 
only seven cutaneous lesions were treated with ultra - low - dose rt ( 4 gy )  . the overall response rate ( orr ) was 97% ( complete response [ cr ] rate [ crr ] : 91% )  . 
2 kaplanmeier curve - derived estimates of local control ( a and c ) and progression - free survival ( b and d ) according to histology and lesion site strahlenther onkol ( 2020 ) 196 : 117125 fig . 
mzl patients had a signicantly longer median pfs ( 18 years ; p = 0.008 ) and a signicantly higher 10 - year pfs ( 70% ; p = 0.008 ) compared with fl patients ( 9 years and 46% )  . 
os did not differ signicantly among types of radiation eld , although a nonsignicant trend ( p = 0.20 ) toward a higher 10 - year os rate was observed following isrt ( 95% ) versus ifrt ( 85% ) and efrt ( 74% )  . toxicity rt was well tolerated with no grade 4 / 5 toxicities . 
the incidence rates of acute grade 1 , 2 , and 3 toxicities were 81 , 30 , and 3% , respectively , with erythema , mucositis , and fatigue being the frequent ones . 
notably , there were no grade 3 acute toxicities in the reduced - dose group . cox proportional hazards model age at the time of rt , gender , histology , stage , rt dose , radiation eld , the timing of rt , prior therapies , adjuvant treatments , and cr after rt were included in a cox proportional hazards model . 
in the follow - up multivariate analysis , rt dose and timing of rt ( upfront or salvage ) remained signicantly related to lc , whereas age , histology , and cr to rt remained considerably related to pfs . 
this study elaborated ve key ndings : ( 1 ) rt is a successful treatment for enlg - nhl , with 91% of treated lesions exhibiting cr . ( 2 ) mzl patients showed a better pfs rate than fl patients . ( 3 ) higher orr and crr were observed in patients treated with conventional - dose regimens than in those treated with reduced - dose regimens , without any signicant difference in rate of local relapses ( 4 ) radiation eld reduction using isrt did not compromise lc and os . 
 ( 5 ) finally , in the multivariate analysis , rt dose and timing were identied as signicant determinants of lc , whereas young age , mzl histology , and cr to rt were identied as predictors of pfs . overall , studies struggle to dene the optimal rt treatment for enlg - nhl , which are highly radiosensitive [ 15 ]  . similar to our ndings , lowry et al . 
 [ 16 ] did not observe a loss of efcacy when 24 gy was delivered to indolent lymphomas relative to 4045 gy , with a trend toward lower toxicity rates in the reduced - dose arthe only randomized study investigating the role of different doses of rt in low - grade nhl consisting of both marginal and follicular lymphomas demonstrated a superior cr rate and pfs following 24 gy in comparison with 4 gy [ 17 ]  . mzl is a group with generally better outcome and different biology than the fl . 
a team from the memorial sloan kettering cancer center reported outcomes for 490 patients with stage i and ii extranodal mzl of whom 244 patients were treated with rt alone . 
they had a slightly shorter median follow - up of 5.2 years and , unlike here , did not evaluate the association between rt dose , rt volume , and lc [ 18 ]  . 
in a retrospective study with long - term followup ( median 70.5 months ) conducted at stanford university medical center , a median rt dose of 39.6 gy was found to be tolerable in 40 patients with extranodal non - orbital indolent lymphoma of the head and neck . 
further analysis regarding the doseresponse relationship of our cutaneous lymphoma patients was carried out and will be published separately by oertel et al . de - escalation is also seen in rt eld - setup modality , with isrt limiting radiation exposure to organs at risk , avoiding associated toxicities and maintaining systemic treatment options [ 1 , 20 ]  . 
traditionally , efrt is a safe and effective treatment for git lymphoma ; however , radiation eld reduction seems to yield a more favorable toxicity prole [ 2123 ]  . 
we detected a comparable lc and os between the different radiation elds , while in multivariate analysis , the os was better following isrt , probably due to the minimal toxicity prole and advances in the systemic therapy of nhl . 
the 10 - year pfs of patients with git lesions in our study ( 76% ) was relatively low compared to recently reported 10 - year pfs rates obtained with modern 124 strahlenther onkol ( 2020 ) 196 : 117125 rt regimens , probably due to advances in radiation technique over the long study period [ 5 , 24 , 25 ]  . 
in the present study , for the 103 lesions in 82 patients subjected to isrt , we obtained 10 - year lc , pfs , and os rates of 93 , 60 , and 95% , respectively , which support the effectiveness of isrt in primary as well as in salvage cases . 
regarding radiation safety , no moderate or severe toxicities were observed . in contrast to the aforementioned limited stages , patients with advanced - stage ( iiiiv ) disease require a systemic treatment such as immunochemotherapy [ 2729 ]  . 
concerning cellular therapies , chimeric antigen receptor t cells ( cart ) have emerged as a highly effective treatment for patients with relapsed or refractory aggressive or transformed b - cell lymphomas , with an objective response rate of 82% and cr rate of 54% [ 32 ]  . 
further studies to clarify the role of cart in the treatment algorithm of low - grade lymphoma are needed and currently ongoing . advancements in diagnostic measures focus on uorodeoxyglucose ( fdg ) positron - emission tomography ( pet ) , which may improve management of indolent nhl as patients presenting with high fdg - standardized uptake values have increased risks of transformation and mortality [ 33 ]  . 
in this study , stage ii disease ( in contrast to stage i ) and bcl2 expression positivity were associated with less favorable pfs in fl patients treated with denitive rt for localized disease [ 30 ]  . 
such ndings suggest that pet - ct monitoring after rt warrants further exploration as a possible method of identifying patients who should be referred for additional systemic treatment . regarding rt timing , we detected longer lc and pfs following upfront rt . 
notably , we were able to administer multiple rt series in some patients without signs of increased toxicity in comparison with upfront the present study has limitations related to its retrospective nature and inhomogeneity of the individual entities . furthermore , many clinical characteristics , molecular , and genetic markers were not available for all patients as potential factors that may inuence treatment outcomes . 
multiinstitutional prospective studies are needed to provide further evidence regarding the proper management of enlgnhl patients and , especially , on how rt can be integrated into systemic treatment approaches in this patient population . 
a german study ( clinicaltrials.gov nct03341520 ) is underway to evaluate the rate of cr after ultra - low - dose isrt with 2 fractions of 2 gy in combination with obinutuzumab in early - stage nodal fl . 
further investigations of radiation variables in addition to genomic alterations may provide valuable information to guide optimized and personalized treatment planning in the era of targeted therapies . conclusion primary involved - site radiotherapy was found to be a very effective treatment with minimal toxicity in patients with low - grade nhl . 
reduced - dose radiotherapy extranodal with ( cid : 2 ) 30.6 gy exhibited effectiveness similar to that of conventional - dose regimens , without signicant differences in pfs rates . 
dezember 2019 springer - verlag gmbh germany , part of springer nature 2019 hintergrund die standardtherapie bei lokal fortgeschrittenen plattenepithelkarzinomen der kopf - hals - region ( locally advanced head and neck squamous cell carcinoma , la - hnscc ) ist die primre operation , gefolgt von adjuvanter radio ( chemo ) therapie , oder die denitive radiotherapie mit konkomitanter systemtherapie . 
sowohl fr die primre radiochemotherapie ( rct ) mit cisplatin [ 1 ] als auch fr die bioradiotherapie ( brt ) mit cetuximab [ 2 , 3 ] liegen daten aus phase - iii - studien vor , die einen berlebensvorteil durch die addition der jeweiligen systemtherapie zur radiotherapie zeigten . 
die vorliegende publikation verglich das gesamtberleben ( overall survival , os ) sowie frhund spttoxizittsraten in einer multizentrischen , retrospektiven kohorte von us - amerikanischen lahnscc - patienten , die entweder mittels denitiver brt oder rct behandelt wurden . patienten und methoden die patientendaten entstammen der datenbank des landesweiten us - amerikanischen veteranen - krankenhaussystems . 
in die auswertung eingeschlossen wurden 4520 patienten mit der diagnose eines hnscc der mundhhle , des oro - , hypopharynx oder laoriginalpublikation bauml jm , vinnakota r , anna park yh et al ( 2019 ) cisplatin versus cetuximab with denitive concurrent radiotherapy for head and neck squamous cell carcinoma : an analysis of veterans health affairs data . 
zur balancierung der patientencharakteristika in beiden kohorten wurde eine propensity - score ( ps ) methode angewandt . hinsichtlich der therapienebenwirkungen wurde zudem zwischen hochdosis - cisplatin ( hdc , 80120 mg / m2 , q3w ) und niedrigdosis - cisplatin ( ldc , 3050 mg / m2 , q1w ) unterschieden . ergebnisse patienten , die cisplatin erhielten , waren jnger , huger aktive raucher und hatten mehr laryngeale und hypopharyngeale tumoren . 
whrend cisplatin mit hheren raten von nierenversagen , belkeit , durchfall und hrminderungen assoziiert war , waren patienten mit cetuximab huger von hautausschlag und mukositis betroffen . schlussfolgerung der autoren die gabe von cisplatin im rahmen der primren rct ist gegenber der gabe von cetuximab beim la - hnscc mit einem signikanten vorteil im os assoziiert . 
schwchen sind der fehlende p16 / hpv - status ( human papillomavirus , hpv ) der patienten mit oropharynxkarzinomen , die fehlenden angaben zur bestrahlungsdosis , ein mglicher bias durch analyse eines kollektivs , das sich ausschlielich aus veteranen der us - armee rekrutierte , sowie der retrospektive charakter der arbeit mit signikanten unterschieden zwischen den beiden gruppen bezglich patientenzahlen und komorbiditten . nach verffentlichung der zulassungsstudie von cetuximab im jahr 2006 [ 2 ] wurde dieser antikrper im rahmen der primren radiotherapie hug bei patienten mit kontraindikationen gegen cisplatin oder bei tumoren mit niedrigem risikoprol in der erwartung angewandt , die rate schwerer langzeitnebenwirkungen mit konsekutiver verschlechterung der lebensqualitt zu senken [ 4 ]  . 
im jahr 2019 erschienen nun zwei phase - iii - studien , die den einsatz von cisplatin direkt mit cetuximab in einem denierten patientenkollektiv verglichen . die nrg oncology rtog 1016 sollte die nichtunterlegenheit hinsichtlich des os von cetuximab im vergleich zu einer cisplatinbasierten rct zeigen [ 5 ]  . 
anzumerken ist , dass in anlehnung an die rtog0129 - studie nur kumulativ 200 mg / m2 cisplatin statt der sonst weit verbreiteten 300 mg / m2 vorgesehen waren , welche 93 % der patienten auch erhielten . 
eine nichtunterlegenheit von cetuximab konnte somit nicht nachgewiesen werden ( hazard ratio [ hr ] 1 , 45 ; einseitiges 95 % - kondenzintervall 1 , 94 ; p = 0 , 506 )  . 
die dysphagierate nach 24 monaten war in beiden armen hnlich und die unterschiede in der lebensqualitt gem des eortc - qlq - c30 - fragebogens erreichten zu keinem zeitpunkt klinische signikanz . beide prospektiven studien knnen komplementr interpretiert werden und zu der frage fhren , ob der radiosensibilisierende effekt von cetuximab hauptschlich auf die hpv - negativen tumoren , die den egfr ( epidermal growth factor receptor ) strker exprimieren , limitiert ist , oder ob diese kombination generell weniger wirksam als cisplatin simultan zur bestrahlung ist ? gegen ersteres , also eine vom hpv - status abhngige wirksamkeit von cetuximab , sprechen die ergebnisse der sekundranalyse der imcl - 9815 - studie durch rosenthal et al . , bei welcher der radiosensibilisierende effekt in beiden subgruppen signikant war [ 8 ]  . 
sowie auch ergebnisse einer frheren , randomisierten studie [ 10 ] mit generell schlechteren ergebnissen bei radiotherapie mit cetuximab gegenber cisplatin . eine weitere , kleine phase - ii - studie von magrini et al . , die nur 70 der 130 vorgesehenen patienten rekrutierte , hatte als primre endpunkte die therapiecompliance sowie die rate an akutnebenwirkungen . 
diese studie randomisierte zwischen der radiotherapie mit ldc und cetuximab [ 11 ]  . fr beide endpunkte war der cetuximab - arm unterlegen . dazu war die rate schwerer unerwnschter nebenwirkungen inklusive therapieassoziierter todesflle im cetuximabarm signikant hher ( 19 % versus 3 % , p = 0 , 044 ; [ 7 , 11 ] )  . die in der hier kommentierten arbeit beschriebenen nebenwirkungen sind mit der literatur kohrent und betreffen vorwiegend nierenund ototoxizitt bei cisplatin und eine hhergradige dermatitis und mukositis bei cetuximab . diese ergebnisse besttigen also erneut , dass cetuximab keineswegs eine nebenwirkungsarme therapieoption darstellt . so bleibt die frage nach mglichkeiten zur deeskalation / cisplatinfreien regimen , zumindest fr die prognostisch besseren hpv - positiven kohorten , zunchst ungelst . strahlenther onkol ( 2020 ) 196 : 197199 ein guter ansatz knnte die leichte reduktion der bestrahlungsdosis in kombination mit neueren chemotherapeutika wie paclitaxel seein solcher ansatz erwies sich als effektiv in einer phase - ii - studie [ 12 ] und knnte theoretisch sowohl das auftreten von spttoxizitten wie dysphagie vermindern als auch cisplatinspezische nebenwirkungen wie otound nephrotoxizitt eliminieren . 
der einsatz von paclitaxel mit einer herkmmlichen bestrahlungsdosis wre auch eine option fr patienten aus hheren risikogruppen , die aber aufgrund von komorbiditt nicht fr cisplatin infrage kommen . fazit die vorliegende publikation besttigt in einer groen kohorte von veteranen der us - armee mit la - hnscc die bereits prospektiv in phase - iii - studien gezeigte berlegenheit von cisplatin gegenber cetuximab simultan zur denitiven bestrahlung . 
analog aktueller leitlinien sollte cisplatin daher weiterhin bei tumoren der mundhhle , des oro - / hypopharynx sowie des larynx und in jeder risikogruppe bevorzugt eingesetzt werden [ 13 ]  . 
adelstein dj , li y , adams gl , wagner h jr . , kish ja , ensley jf , schuller de , forastiere aa ( 2003 ) an intergroup phase iii comparison of standard radiation therapy and two schedules of concurrent chemoradiotherapy in patients with unresectable squamous cell head and neck cancer . 
bonner ja , harari pm , giralt j , azarnia n , shin dm , cohen rb , jones cu , sur r , raben d , jassem j , ove r , kies ms , baselga j , youssouan h , amellal n , rowinsky ek , ang kk ( 2006 ) radiotherapy plus cetuximab for squamous - cell carcinoma of the head and neck . 
bonner ja , harari pm , giralt j , cohen rb , jones cu , sur rk , raben d , baselga j , spencer sa , zhu j , youssouan h , rowinsky ek , ang kk ( 2010 ) radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
machtay m , moughan j , trotti a , garden as , weber rs , cooper js , forastiere a , ang kk ( 2008 ) factors associated with severe late toxicity after concurrent chemoradiation for locally advanced head and neck cancer : an rtog analysis . 
gillison ml , trotti am , harris j , eisbruch a , harari pm , adelstein dj , sturgis em , burtness b , ridge ja , ringash j , galvin j , yao m , koyfman sa , blakaj dm , razaq ma , colevas ad , beitler jj , jones cu , dunlap ne , seaward sa , spencer s , galloway tj , phan j , dignam jj , le qt ( 2019 ) radiotherapy plus cetuximab or cisplatin in human papillomavirus - positive oropharyngeal cancer ( nrg oncology rtog 1016 ) : a randomised , multicentre , noninferiority trial . 
ang kk , harris j , wheeler r , weber r , rosenthal di , nguyen - tan pf , westra wh , chung ch , jordan rc , lu c , kim h , axelrod r , silverman cc , redmond kp , gillison ml ( 2010 ) human papillomavirus and survival of patients with oropharyngeal cancer . 
mehanna h , robinson m , hartley a , kong a , foran b , fultonlieuw t , dalby m , mistry p , sen m , otoole l , al booz h , dyker k , moleron r , whitaker s , brennan s , cook a , grifn m , aynsley e , rolles m , de winton e , chan a , srinivasan d , nixon i , grumett j , leemans cr , buter j , henderson j , harrington k , mcconkey c , gray a , dunn j , de ehpvtg ( 2019 ) radiotherapy plus cisplatin or cetuximab in low - risk human papillomaviruspositive oropharyngeal cancer ( de - escalate hpv ) : an open - label randomised controlled phase 3 trial . 
rosenthal di , harari pm , giralt j , bell d , raben d , liu j , schulten j , ang kk , bonner ja ( 2016 ) association of human papillomavirus and p16 status with outcomes in the imcl - 9815 phase iii registration trial for patients with locoregionally advanced oropharyngeal squamous cell carcinoma of the head and neck treated with radiotherapy with or without cetuximab . 
riaz n , sherman e , koutcher l , shapiro l , katabi n , zhang z , shi w , fury m , wong r , wolden s , rao s , lee n ( 2016 ) concurrent chemoradiotherapy with cisplatin versus cetuximab for squamous cell carcinoma of the head and neck . 
giralt j , trigo j , nuyts s , ozsahin m , skladowski k , hatoum g , daisne jf , yunes ancona ac , cmelak a , mesia r , zhang a , oliner ks , vanderwalde a ( 2015 ) panitumumab plus radiotherapy versus chemoradiotherapy in patients with unresected , locally advanced squamous - cell carcinoma of the head and neck ( concert - 2 ) : a randomised , controlled , open - label phase 2 trial . 
magrini sm , buglione m , corvo r , pirtoli l , paiar f , ponticelli p , petrucci a , bacigalupo a , crociani m , lastrucci l , vecchio s , bonomo p , pasinetti n , triggiani l , cavagnini r , costa l , tonoli s , maddalo m , grisanti s ( 2016 ) cetuximab and radiotherapy versus cisplatin and radiotherapy for locally advanced head and neck cancer : a randomized phase ii trial . 
chen am , felix c , wang pc , hsu s , basehart v , garst j , beron p , wong d , rosove mh , rao s , melanson h , kim e , palmer d , qi l , kelly k , steinberg ml , kupelian pa , daly me ( 2017 ) reduced - dose radiotherapy for human papillomavirus - associated squamous - cell carcinoma of the oropharynx : a single - arm , phase 2 study . 
brink3 , 5 received : 24 december 2018 / accepted : 12 september 2019 / published online : 26 september 2019 the author ( s ) 2019 abstract purpose previous literature has reported contradicting results regarding the relationship between tumor volume changes during radiotherapy treatment for non - small cell lung cancer ( nsclc ) patients and locoregional recurrence - free rate or overall survival . 
the aim of this study is to validate the results from a previous study by using a different volume extraction procedure and evaluating an external validation dataset . methods for two datasets of 94 and 141 nsclc patients , gross tumor volumes were determined manually to investigate the relationship between tumor volume regression and locoregional control using kaplanmeier curves . 
for the rst dataset ( n = 94 ) , automatically determined tumor volumes were available from a previously published study to further compare their correlation with updated clinical data . results a total of 70 out of 94 patients were classied into the same group as in the previous publication , splitting the dataset based on median tumor regression calculated by the two volume extraction methods . 
non - adenocarcinoma patients receiving concurrent chemotherapy with large tumor regression show reduced locoregional recurrence - free rates in both datasets ( p < 0.05 in dataset 2 )  . 
boulevard 29 , 5000 odense , denmark 160 strahlenther onkol ( 2020 ) 196 : 159171 tumorregress whrend strahlentherapie bei patienten mit nicht - kleinzelligem bronchialkarzinom mittels cone - beam - computertomogrammen zusammenfassung zielsetzung zum verhltnis zwischen vernderungen des tumorvolumens whrend der strahlentherapie und der lokoregionalen rezidivfreien rate ( locoregional recurrence - free rate ) oder dem gesamtberleben ( overall survival ) bei patienten mit nicht - kleinzelligen bronchialkarzinomen ( nsclc ) gibt es widersprchliche ergebnisse in der bestehenden literatur . 
das ziel dieser studie ist , mithilfe eines alternativen verfahrens zur tumorvolumenberechnung ergebnisse einer dieser bereits publizierten studien zu besttigen und in einem externen datensatz zu validieren . methoden das makroskopische tumorvolumen ( gross tumor volume , gtv ) wurde fr zwei datenstze mit jeweils 94 und 141 nsclc - patienten manuell festgestellt . 
makroskopische tumorvolumen des ersten datensatzes ( n = 94 ) wurden zustzlich mit einem bestehenden verfahren zur automatischen tumorvolumenberechnung bestimmt und mit aktualisierten klinischen daten verglichen . ergebnisse nach jeweiliger aufteilung der patienten in zwei untergruppen basierend auf dem median der tumorvolumen wurden 24 / 94 patienten mithilfe der zwei verschiedenen verfahren zur tumorvolumenberechnung unterschiedlich klassiziert . 
patienten mit nicht - adenokarzinomen mit kombinierter chemotherapie ( concurrent chemotherapy ) mit hoher tumorregression zeigen geringe lokoregionale rezidivfreie raten in beiden datenstzen ( p < 0 , 05 im zweiten datensatz )  . im zweiten datensatz ( dataset 2 ) ist das gegenteil fr patienten ohne chemotherapie zu beobachten , welcher signikant fr das das gesamtberleben ( p = 0 , 01 ) , aber nichtsignikant fr die lokoregionale rezidivfreie rate war ( p = 0 , 13 )  . schlussfolgerung das verhltnis zwischen dem patientenspezischen behandlungsergebnis und der tumorregression ist grtenteils abhngig von der art der chemotherapie . 
diese faktoren knnen einen beitrag zur konzipierung zuknftiger studien zur vollstndigen aufklrung des verhltnisses zwischen dem patientenspezischen behandlungsergebnis und der tumorregression leisten . schlsselwrter cone - beam - ct nicht - kleinzelliges bronchialkarzinom tumorregress makroskopisches tumorvolumen gesamtberleben introduction tumor volume is a known prognostic factor for non - small cell lung cancer ( nsclc ) patients [ 13 ]  . 
a recent systematic review reports that the majority of retrospective studies found a signicant correlation between gross tumor volume ( gtv ) prior to radiotherapy and overall survival ( os ) [ 1 ]  . 
most studies used computed tomography ( ct ) or 18f - fdg positron - emission tomography imaging to evaluate the changes [ 4 ]  . cone - beam computed tomography ( cbct ) images are generally acquired daily or weekly prior to radiotherapy for treatment set - up purposes . 
comparable ndings were found in a larger study [ 9 ] : a signicantly reduced locoregional recurrence - free rate ( lrfr ) for patients with large tumor regression during radiotherapy treatment , and worse os for non - adenocarcinoma patients . in the study performed by brink et al . 
 [ 9 ] , tumor regression was estimated using an automated workow including a deformable registration of cbct images on the corresponding planning ct image followed by the calculation of jacobian determinants , from which tumor volume restrahlenther onkol ( 2020 ) 196 : 159171 gression during treatment could be derived . 
the study was approved by maastro clinics institutional review board . data collection was approved by each institutional ethics committee . all patients in both datasets were treated radically with ( chemo ) radiation . 
patients with a prior history of lung cancer , simultaneous treatment of brain metastases , stereotactic body radiation treatment ( sbrt ) , and patients who received less than 45 gy of radiotherapy dose were excluded from the analysis . 
moreover , only patients with cbct images acquired regularly during the course of radiotherapy treatment were included . patient and treatment characteristics of dataset 1 and dataset 2 were compared using the wilcoxon rank - sum test for continuous variables and fishers exact test for categorical variables . 
differences in patient characteristics between the datasets in the current study is an advantage , since it allows for possible explanations for the intuitively contradicting previous results ; in particular the difference in chemotherapy could inuence the resultssee below . to investigate the potential inuence of different patient characteristics on both lrfr and os , a univariable analysis was performed for the clinical parameters , including gender , age , tumor stage , and radiotherapy dose . 
for variables that were shown to be signicantly associated with outcome , an extended analysis of the confounding effect of this variable on the relationship between tumor regression and patient outcome was performed . 
the gross tumor volume ( gtv ) , which was delineated on the treatment planning ct , was used to evaluate tumor volume ( regression ) , containing only the primary tumor and not including lymph nodes . 
one exception was made in dataset 1 , where the entire disease site was contained in lymph node station ve , and therefore the combined volume was evaluated for this patient . 
possibly , tumor regression was underestimated for these patients . volume extraction tumor volume was extracted from all cbct images in both datasets using the gtv segmentation method as described above ( i.e. , the manual method )  . 
for dataset 1 , the tumor volumes were previously derived from all available cbct images using an automated procedure as described in [ 9 ] ( i.e. , the automatic method )  . 
all available data points were used to perform an exponential t in order to estimate the tumor volume at day 50 of treatment for dataset 1 [ 9 ] and day 40 for dataset 2 , which approximately corresponded to the end of the radiation treatment . patient outcomes two endpoints were investigated : overall survival ( os ) and locoregional recurrence - free rate ( lrfr )  . 
information on locoregional recurrence was available for all patients in dataset 1 and for 136 / 141 patients in dataset 2 . for dataset 2 , the time - xed follow - up ct scans ( and / or chest x - rays ) were made 3 months after radiotherapy and then yearly , complemented with a pet / ct when indicated , supplemented with ct scan and / or x - ray scans on clinical suspicion of recurrence ; thus , the imaging frequency 162 strahlenther onkol ( 2020 ) 196 : 159171 was much larger in clinical practice than just the time - xed scans . 
log - rank tests were used to test for a signicant split of the kaplanmeier curves . note that all patient outcomes were updated for the current analysis compared to the previous publication . validation 1 : comparison of two volume extraction methods in order to validate the previous results obtained with the automatic method [ 9 ] , absolute tumor volumes and tumor volume changes were compared against the manual method for all timepoints at which a manual delineation of the gtv on the cbct image was available in dataset 1 . 
the effect was most pronounced for non - adenocarcinoma patients ; therefore , the kaplanmeier plots for these patients were recalculated to compare the automatic and manual volume extraction methods . inuence tumor volume changes during radiotherapywe were able to distinguish a group of patients who did not receive any chemotherapy and a group that received concurrent chemoradiotherapy . 
the interval between completion of chemotherapy and commencement of radiotherapy has previously been shown to inuence tumor growth [ 12 ] ; thus , the number of patients who received chemotherapy in each dataset could potentially inuence the sign of the relationship between tumor regression and patient outcome . although evaluated subgroups , such as regime of chemotherapy , contain fewer patients than the entire cohort , they are able to provide information on the possible reason for the current conicting information in published papers on the relationship between tumor regression during radiotherapy and treatment outcome . 
therefore , besides chemotherapy , we evaluated the inuence of potential confounders that were found to be signicantly correlated to outcome in the univariable analysis ( see patients )  . 
if the effect is also present within a given level , the effect can obviously not be explained by confounding , and it is very unlikely that the overall effect then is related to confounding . 
confounding from continuous variables was evaluated as in the previous publication [ 9 , appendix b ]  . for each continuous variable , a linear regression of the tumor regression based on the continuous variable was performed . 
using the residual as new tumor regression values , kaplanmeier survival analysis was repeated to validate that the original observed effect was also present in data with no correlation to the continuous variable . validation 2 : external validation dataset absolute tumor volume and patient outcome the availability of a dataset from a different institution allows us to validate the results of the previous study that patients with larger tumor regression show decreased os and lrfr . 
for instance , chemotherapy is expected to since baseline tumor volume is a well - investigated prognostic factor [ 3 ] , some additional analyses were performed for completeness of the current study . 
for dataset 1 , the interval between the start of chemotherapy and the start of radiotherapy is signicantly longer than in dataset 2 : the patients in dataset 1 often started earlier with the concurrent chemotherapy to prevent patients waiting for treatment while radiotherapy planning was being performed . 
1b was reproduced with the sole inclusion of patients with at least 2 years of follow - up ( supplementary information s1 fig )  . table 2 shows the results of the univariable analysis . 
the level of the categorical variables not indicated in the table were used as reference categories . age , who status 2 / 3 , t - stage 2 , overall stage ii , and histology subtype non - adenocarcinoma were signicantly associated with os . 
therefore , for age , who performance status , t - stage , n - stage , overall stage , and histology subtype , the confounding effect was examined . images supplementary information s2 fig shows a histogram representing the number of cbct images used during treatment to perform the gtv segmentations using the manual method . 
in total , 454 cbct images were included in dataset 1 and 823 cbct images in dataset 2 , with a median [ range ] of 5 [ 45 ] and 6 [ 57 ] cbct images per patient for datasets 1 and 2 , respectively . validation 1 : comparison of two volume extraction methods for each timepoint , the majority of automatically determined tumor volumes in dataset 1 was estimated to be larger than using manual delineations , as indicated in the blandaltman plots ( supplementary information s3 fig )  . moreover , the difference between both methods visually increases with time during treatment . 
2 shows the kaplanmeier plots for lrfr ( a ) and os ( b ) for all non - adenocarcinoma patients of dataset 1 for the purpose of comparing the manual and automatic methods . 
2c represent the patients that were classied differently , being 24 / 94 ( 26% ) patients and 18 / 60 ( 30% ) non - adenocarcinoma patients . validation 2 : external validation dataset fig . 
since t - stage , n - stage , overall tumor stage ( i , ii , or , iii / iv ) , and who performance status were signicant in the univariable analysis , these variables could be potential confounders for the observed splitting in fig . 
3c is observed within all subgroups , although not statistically signicant for all of them due to the very limited number of patients in such a sub - analysis ( supplementary information s8 fig )  . thus , overall tumor stage does not explain the difference observed in fig . 
also tand n - stage do not explain the observed difference , since statistically signicant splitting based on the tumor regression is observed within individual tand n - stage groups , as show in supplementary information s9 fig . 
patients with large tumor regression had who performance status 0 ( n = 1 ) , 1 ( n = 15 ) , or 2 ( n = 5 ) , whereas patients with small tumor regression only had who performance status 1 ( n = 11 ) or 2 ( n = 11 )  . potential confounding from age and absolute tumor volume was evaluated as described in the methods section . 
4b and c do not change when using the residuals of the linear regression with tumor volume instead of using the tumor regression at the end of treatment . the results of outcome as a function of tumor regression for the patients who had chemotherapy are shown in fig . 
3d and 4d comprise the following chemotherapy regimens : 50 had chemotherapy prior to radiotherapy , 5 had only chemotherapy during radiotherapy , and for 5 , no knowledge of chemotherapy prior to radiotherapy was available . 
3d and 4d , 58 patients had overall stage iii or iv , thus a sub - analysis like those in supplementary information s8 fig and s9 fig was not possible for this group . 
who performance status was equally distributed among the largeand small - regression groups , with 6 , 22 , and 3 patients in the large - regression group and 5 , 22 , and 2 in the low - regression group for who performance status 0 , 1 , and 2 / 3 , respectively . 
3 and 4 ( supplementary information s10 and s11 )  . the group of patients in dataset 1 without chemotherapy is very small ( n = 11 ) , which makes it hard to conclude on that subgroup , but otherwise the results are in line with the data presented for dataset 2 . absolute tumor volume there is a signicant split in the os kaplanmeier curves for absolute tumor volume higher or lower than the median at the start of treatment ( p = 0.040 ) at week 2 ( p = 0.018 ) and at week 5 ( p = 0.044 ) for dataset 2 ( supplementary information s5 fig )  . 
kaplanmeier curves for the non - adenocarcinoma patients ( n = 60 ) of dataset 1 , which indicate a difference in lrfr ( a ) and os ( b ) for patients with a tumor regression at the end of treatment larger or smaller than the median , indicated for the automatic ( black ) and manual ( red ) methods . 
the dataset evaluated in the previous study , as well as a second dataset from a different institute , were evaluated using a manual volume extraction method to investigate the relationship between tumor regression and os and lrfr . 
data from dataset 2 , split based on the median relative tumor regression at the end of treatment . a all patients ( n = 141 ) , b patients who received concurrent chemotherapy ( n = 90 ) , c patients who did not receive chemotherapy ( n = 43 ) , and d non - adenocarcinoma patients who received concurrent chemotherapy ( n = 60 ) able from the previous study to validate the manual volume extraction method . the observation of brink et al . 
both the manual and the automatic method show that non - adenocarcinoma patients of dataset 1 with large regression at the end of treatment have reduced lrfr compared to patients with smaller regression , with pvalues of p = 0.057 and p = 0.029 for automatic and manual methods , respectively . despite the discrepancy in absolute volumes between the two methods , 70 / 94 patients were assigned to the same tumor regression group . 
first of all , the number of data points available to perform the t was much lower for the manual method . therefore , the accuracy of the t can be largely inuenced by one outlier from the manual method . 
an advantage of the automatic method is that this method is not user - dependent , as it is commonly known that there are large inter - observer variabilities in tumor segmentations [ 14 , 15 ]  . 
a all patients ( n = 141 ) , b patients who received concurrent chemotherapy ( n = 90 ) , c patients who did not receive chemotherapy ( n = 43 ) , and ( d ) non - adenocarcinoma patients who received concurrent chemotherapy ( n = 60 ) intensive . 
the lack of a ground truth for tumor segmentations makes it difcult to specify which method is best , which , in turn , likely depends on the specic aim of measuring volume changes . 
the regression of lymph nodes might potentially be a better indicator of treatment response . for the overall population in dataset 2 , no splitting related to the amount of tumor regression could be found , which could be related to differences within and between datasets as shown in the results ( e.g. , who performance status , radiotherapy schedule , chemotherapy schedule , and histology )  . 
also , for overall tumor stage , t - stage , and n - stage , splitting of survival curves was observed within the specic levels , indicating that the main result is not due to confounding of these variables . 
although the investigated subgroups were small , the results indicate that it is unlikely that these parameters were confounding factors . nonetheless , a prospective study would enable the selection of a more homogeneous patient population in order to further investigate the inuence of these factors . 
nevertheless , the current study was able to showin agreement with the previous studythat patients receiving chemotherapy prior to and during radiotherapy treatment with large tumor regression have worse os and lower lrfr in both datasets , despite the fact that the datasets are largely heterogeneous . 
on the other hand , patients who did not receive any chemotherapy show the inverse relationship between tumor regression and patient outcome . chemotherapy type and regimen have not always been taken into account in great detail in previously published analyses . 
chemotherapy regimens and their specic timing with respect to the radiation treatment could be the main explanation for the contradicting results of previous studies relating patient outcome to tumor regression during radiotherapy . 
 [ 8 ] , patients received different regimens : 16% did not receive chemotherapy , 60% received concurrent chemotherapy , 10% received sequential chemotherapy , and 14% received both concurrent and sequential chemotherapy . 
the results of the current study show the impact of chemotherapy on the tumor volume behavior during treatment : the tumor regression pattern during chemoradiotherapy is the result of irradiation , but largely depends on the delivered chemotherapy schedule . 
a possible inuence of radiotherapy regime , e.g. , hypo - fractionated radiotherapy [ 17 ] , on the relationship between patient outcome and the degree of tumor regression could be of interest , but was outside the scope of the current paper . besides the inuence of chemotherapy , the relationship between gtv changes during treatment and patient outcome is more pronounced for non - adenocarcinoma patients . the impact of histology has been shown before [ 18 ] and is another factor that should be taken into account in future analyses . 
lastly , tumor volume at the start of treatment has an inuence on these results as well , as it was shown to be related to os [ 3 ]  . 
this would make it possible to more accurately derive the exact relationship between tumor volume regression during treatment and patient outcome , and also to dene subgroups of patients who would benet from an adjusted treatment . 
in the current study , the exact date of a locoregional recurrence is unknown in both datasets , and the follow - up protocols were also different in each institute . although a similar result was found in both datasets regarding the relationship between tumor regression and lrfr , we cannot exclude the possibility that the local follow - up program might inuence the observed locoregional recurrence rate . 
moreover , a similar observation was seen in a validation dataset for a subgroup of non - adenocarcinoma patients receiving concurrent chemoradiotherapy despite the heterogeneities within and between both datasets , conrming the counterintuitive relationship between tumor regression during radiotherapy and patient outcome . 
januar 2020 der / die autor ( en ) 2019 fdg - pet / ct zum ausschluss von zervikalen lymphknotenmetastasen bei kopf - hals - tumoren in der klinischen n0 - situation hintergrund die therapie von kopf - hals - karzinomen ist v . 
auch nden sich nach resektion in einem n0 - hals bei bis zu 50 % pathologische lymphknoten in der kontrastmittel - computertomographie ( ct ; [ 3 ] )  . 
nachdem auch eine magnetresonanztomographie ( mrt ) oder sonographie keine hinreichende diagnostische sicherheit ergeben , werden additive methoden wie eine sentinel - lymphonodektomie oder das fdgpet / ct ( fluordeoxyglukose - positronenemissionstomographie / computertomographie ) bentigt . 
die acrin - studie [ 4 ] untersuchte nun die zuverlssigkeit der fdg - pet / ctstrategie fr zervikale lymphknoten bei kopf - hals - tumoren . patienten und methoden die studie untersuchte 287 patienten mit plattenepithelkarzinomen ct24 im kopf - halsbereich , die operiert werden sollten . 
die pathologischen befunde der ( konventionellen ) cn0 - halsseite wurden dann mit den fdg - pet / ctergebnissen verglichen und ein negativer vorhersagewert daraus abgeleitet . ergebnisse der negative vorhersagewert des fdg - pet / ct betrug 0 , 87 fr die visuelle auswertung . 
der verzicht auf eine neck dissection in solchen situationen sollte in studien prospektiv untersucht werden . originalpublikation lowe vj , duan f , subramaniam rm et al ( 2019 ) multicenter trial of [ 18f ] uorodeoxyglucose positron emission tomography / computed tomography staging of head and neck cancer and negative predictive value and surgical impact in the n0 neck : results from acrin 6685 . 
3 , 72076 tbingen , deutschland kommentar die acrin - studie belegt mit einer hohen patientenzahl und einer klinisch - pathologischen korrelation das diagnostische potenzial einer fdg - pet / ct zum ausschluss von lymphknotenmetastasen an einem konventionell diagnostizierten n0 - hals . 
hierbei wird ein negativer vorhersagewert von 94 % bei der beurteilung der suvmax - werte erreicht . dies liegt im bereich der ergebnisse von sentinel - nodestrahlenther onkol ( 2020 ) 196 : 200201 strategien [ 1 ] und ist deutlich besser als bei anderen bildgebenden verfahren . 
es fehlen angaben zum untersuchungsablauf , welche fr die beurteilung der pets nach suvmax - werten relevant sind , die ohnehin zwischen zentren differieren . weitere kritikpunkte betreffen : ( cid : 2 ) die fdg - pet / ct beeinusste das chirurgische vorgehen . 
eine korrelation mit gesamtberleben und lokalen kontrollraten ist notwendig . ( cid : 2 ) im lymphknotenlevel iia , mit den statistisch hugsten lymphknotenmetastasen ber die untersuchten hnolokalisationen , waren die falsch - positiven resultate mit 26 % am hchsten . dennoch gibt die studie aufschluss ber das potenzial der fdg - pet / ct beim prtherapeutischen staging , nicht zuletzt auch durch die detektion von 14 % weiteren befunden ; diese befunde waren allerdings nicht primrer studieninhalt . 
radiochemotherapie bereits gelungen [ 5 ]  . fazit die fgd - pet / ct zum ausschluss von zervikalen lymphknotenmetastasen bei kopf - hals - tumoren liefert bei einem ( konventionell erhobenen ) klinischen n0 - status vielversprechende ergebnisse . 
zips geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
civantos fj et al ( 2010 ) sentinel lymph node biopsy accurately stages the regional lymph nodes for t1t2 oral squamous cell carcinomas : results of a prospective multi - institutional trial . 
lowe vj et al ( 2019 ) multicenter trial of [ 18f ] uorodeoxyglucose positron emission tomography / computed tomography staging of head and neck cancer and negative predictive value and surgical impact in the n0 neck : results from acrin 6685 . 
aebersold2 clemens albrecht3 michael flentje4 ute ganswindt5 stefan hcht6 tobias hlscher7 arndt - christian mller8 peter niehoff9 michael pinkawa10 felix sedlmayer11 daniel zips8 sebastian zschaeck1 , 12 volker budach1 thomas wiegel13 pirus ghadjar1 the prostate cancer expert panel of the german society of radiation oncology ( degro ) and the working party radiation oncology of the german cancer society ( dkg - aro ) received : 30 october 2019 / accepted : 14 november 2019 / published online : 29 november 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract objective this article aims to provide an overview of the role of combined radiation and androgen deprivation ( adt ) therapy in patients with intermediate - risk prostate cancer . materials and methods the current german , european , and nccn ( national comprehensive cancer network ) guidelines as well as relevant literature in the pubmed database which provide information on sub - classication within the intermediate - risk group and the use of adt in terms of oncological outcome were reviewed . results different recommendations for risk - group assessment of patients with localized prostate cancer are available . subdivision of intermediate risk into a favorable and an unfavorable group seems to be justied to allow for a more individualized therapy in a quite heterogenous group of patients . 
therefore , taking into account the increased rate of toxicity associated with adt , dose - escalated rt alone might be justied , especially in favorable intermediate - risk patients . conclusion dose - escalated rt alone appears to be an appropriate treatment in favorable intermediate - risk patients . improve outcomes in unfavorable intermediate - risk patients . addition of short course adt ( 46 months ) might a previous version of this article in german language has already been published as an expert opinion article by some of the above - mentioned authors [ 7 ]  . 
the majority of those patients ( 78% ) were treated by prostatectomy while about 20% received denitive radiation therapy ( rt ) [ 2 ]  . the current german s3 guideline for prostate cancer recommends for denitive rt in the intermediate - risk setting a combination of rt ( 7480 gy ) with short - term androgen deprivation therapy ( adt ) of 46 months ( table 1 ; [ 3 ] )  . in accordance with the german s3 guideline , the european society of urology ( eau ) and the european society for radiotherapy and oncology ( estro ) guidelines stratify the risk groups of pc on the basis of the three - step classication of damico ( table 2 ; [ 35 ] )  . the national comprehensive cancer network ( nccn ) guideline uses a similar system , however supplemented by additional sub - grouping of the gleason grade group ( tables 2 and 3 ; [ 6 ] )  . materials and methods a literature review using the pubmed databank and the upto - date guidelines in world wide web was carried out . 
a previous version of the article in german language has already been published as an expert opinion article by some of the above - mentioned authors [ 7 ]  . the present article is an updated and extended version in collaboration with the prostate cancer expert panel of the german society of radiation oncology ( degro ) and the working party radiation oncology of the german cancer society ( dkg - aro )  . german s3 , eau - estro , and nccn guidelines were included in our review [ 3 , 4 , 6 ]  . 
furthermore , the publications results of 10 randomized trials , one meta - analysis of randomized trials , one prospective cohort study as well as the results of six retrospective studies were included . 
all these publications provide critical information to foster discussions on the role of combined rt and adt , potentially evolving into improved risk stratication resulting in new individualized therapeutic strategies , as presented below . discussion new risk stratication in intermediate - risk prostate cancer in contrast to the german s3 and the european eau - estro guidelines , the nccn guidelines use a subclassication of the low - , intermediate - , and high - risk pc groups , based on increasingly more subtilized outcome analyses during the past few years . 
published a critical discussion about the general necessity of combined adt and rt which takes into consideration the possible heterogeneity of patients with intermediate - risk pc [ 8 ]  . 
in two randomized trials ( clinicaltrials.gov identier nct00116220 and rtog 9408 ) , a combined treatment with 6 months of adt and 70 gy rt , or 4 months of adt and 66.6 gy , respectively , achieved an improvement of biochemical control , metastasis - free , cancer - specic , and overall survival ( os ) versus rt alone ( os : 74% versus 61% , p = 0.01 , after 8 years [ nct00116220 ] ; os : 62% versus 57% after 10 years , p = 0.03 [ rtog 9408 ] ) , at the cost of a slightly increased rate of erectile dysfunction . 
this appeared , however , to be limited to patients with a relevant cardiovascular risk prole as determined in an unplanned subgroup analysis [ 810 ]  . for long - term adt , an increased risk of developing adt - associated toxicities like bone loss , metabolic syndrome , gynecomastia , muscle loss and hot ushes , reduced libido , erectile dysfunction , and an assumed increased cardiac risk is well documented [ 11 ]  . 
on the basis of a subdivision of the intermediate - risk pc group , an individualized therapy with either dose - intensied rt in case of favorable intermediate - risk pc and combination of rt and adt in unfavorable intermediate - risk pc patients is used in mskcc patients ( table 4 ; [ 8 ] )  . the authors also published results of 1024 intermediaterisk pc patients who received 81 gy rt with or without combined adt which validated the new treatment stratication . in the multivariate analysis , gleason 4 + 3 = 7b in comparison to 3 + 4 = 7a ( hr = 5.23 ; p < 0.0001 ) , a 50% percentage of positive biopsy cores ( ppbc ) ( hr = 2.72 ; p = 0.0007 ) , or multiple intermediate - risk factors ( hr = 2.20 ; p = 0.008 ) were signicant predictors for developing distant metastases . 
the subgroup of patients with an unfavorable intermediate - risk pc had a signicant worse psa control rate ( hr = 2.37 ; p < 0.0001 ) , rate of distant metastases ( hr = 4.34 ; p = 0.0003 ) , and a higher prostate cancer - specic mortality ( hr = 7.39 ; p = 0.007 ) in contrast to patients with favorable intermediate - risk pc [ 17 ]  . consequently , damico , the developer of the classic three - step pc risk classication , valued the new classication as a promising tool to individualize pc treatment [ 18 ]  . another validation of the new stratication was done in a retrospective analysis of 2248 pc patients , with an observed signicant worse outcome for patients with unfavorable intermediate - risk pc and an outcome similar to low - risk patients in the favorable intermediate - risk pc patients . 
these results suggest that patients with favorable intermediate - risk pc should rather be treated like lowrisk patients , while in case of an unfavorable intermediaterisk constellation , treatment might be escalated for instance by addition of short - term adt . 
consequently , the new stratication of intermediaterisk pc was implemented in the nccn guidelines ( table 2 ; [ 6 ] )  . dose - intensied radiation therapy in combination with or without androgen deprivation therapy several randomized trials repeatedly showed an improved oncological outcome for the combination of rt + adt . strahlenther onkol ( 2020 ) 196 : 109116 table 4 memorial sloan kettering cancer center treatment algorithm for denitive radiotherapy in patients with intermediate - risk prostate cancer memorial sloan kettering cancer center treatment algorithm favorable intermediate - risk prostate cancer clinical characteristics : one intermediate - risk factor and gleason score of 3 + 4 = 7 or less and < 50% positive biopsy cores recommended radiation options : dose - escalated external beam radiotherapy alone brachytherapy alone in select cases ( e.g. , ( cid : 2 ) 3 positive cores , none with > 50% involvement ) unfavorable intermediate - risk prostate cancer clinical characteristics : several intermediate - risk factors or gleason score of 4 + 3 = 7 or 50% positive biopsy cores recommended radiation options : dose - escalated external beam radiotherapy and short - term androgen deprivation combined brachytherapy and external beam radiotherapy with or without short - term androgen deprivation therapy considering todays standard of care , the applied radiation doses in these trials were apparently moderate , apart from other technical shortcomings affecting and compromising rt tolerance . 
hence , it is not clear whether an application of higher rt doses with presently available modern rt techniques outbalances the need for a cytoreductive combination with adt to achieve similar outcomes . 
as early as in 2009 , a meta - analysis of dose - intensied rt in all risk groups was able to show an improvement in biochemical control [ 20 ]  . therefore , the data of the eortc 22991 trial using a combination of different rt doses ( 70 gy , 74 gy , or 78 gy ) with a short - term adt of 6 months in intermediateand high - risk patients are of special interest . 
patients in the control arm received the respective rt doses without adt . regardless of the applied rt dose , the additional use of adt resulted in improved biochemical control and clinical progression - free survival . 
these data conrmed the benet of a combination of adt even with dose - intensied rt . however , a signicant deterioration of sexual function and activity was registered for addition of adt and no os benet was detectable . 
a clear drawback of this trial is the biochemical control endpoint and the relative short followup duration [ 21 ]  . the former retrospective monocentric trial by zumsteg et al . 
intermediate - risk patients also beneted from additional adt in matters of biochemical control , metastasis - free survival , and prostatespecic survival [ 22 ]  . however , it is important to bear in mind the potential higher rate of toxicities and decline in quality of life associated with an additional adt . 
in particular , there is a risk of overtreating intermediate - risk pc patients if additive prognostic factors are ignored [ 11 , 16 ]  . here , the recently published rtog 0126 trial provides important evidence for individualized treatment in intermediate - risk pc patients , especially when addressing the question of necessity of additional adt . 
the trial randomized exclusively patients with intermediate - risk pc between standard - dose rt with 70.2 gy in 39 fractions versus dose - intensied rt with 79.2 gy in 44 fractions . 
however , a signicant improvement of biochemical control ( biochemical recurrence after 8 years 35% [ 70.2 gy ] versus 20% [ 79.2 gy ] , p < 0.001 ) and lower rate of metastases ( 6% [ 70.2 gy ] versus 4% [ 79.2 gy ] after 8 years , p = 0.05 ) was observed in the dose - intensied rt group . 
besides providing the rst randomized evidence for decreasing the rate of metastases with the use of dose - escalation in intermediate - risk pc patients , the results showed promising biochemical control without using adt . 
the rates of metastases ( 4% ) and cancer - specic mortality ( 2% ) are comparable to the rates in the rtog 9910 trial ( 10 years follow - up , metastases : 6% and cancer specic - mortality : 5% )  . 
this trial tested the duration of adt ( 16 versus 36 weeks ) in combination with standarddose rt ( 70.2 gy ) [ 23 , 24 ]  . these ndings justify the assumption that at least a subgroup of intermediate - risk pc patients could be adequately treated with dose - intensied rt without adt , thus avoiding the toxicities and the decline in quality of life associated with adt [ 16 ]  . in this context , the results of a recently published randomized phase iii trial ( hypo - rt - pc ) comparing ultra - hypofractionation ( 42.7 gy in 7 fractions ) with conventionally fractionated dose - intensied rt ( 78 gy in 39 fractions ) are interesting . 
89% intermediate - risk and 11% high - risk pc patients were treated in both arms without additional adt . with a reported 5 - year failure - free survival of 84% ( 95% ci 8087 ) in both arms and an 5 - year os of 94% ( 95% ci 9296 ) in the ultra - hypofractionation group versus 96% ( 95% ci 9598 ) in the conventionally fractionated group , the data show a promising oncological outcome without using adt in mostly intermediate - risk patients [ 25 ]  . 
however , increased rates of toxicity are frequently associated with the use of simple radiation techniques , whereas modern rt techniques like intensitymodulated rt ( imrt ) and image - guided rt ( igrt ) are able to more effectively shield organs at risk . 
in rtog 0126 , only a third of patients were treated with modern imrt techniques [ 23 , 27 , 28 ]  . individualization of therapy in intermediate - risk prostate cancer a recently published analysis of the national cancer data base ( ncdb ) examined the data of 18 , 598 patients with favorable intermediate - risk pc and corroborated the assumption that additional adt in favorable intermediaterisk patients could be omitted . 
in the brachytherapy arm , a signicant improvement of biochemical control was observed , whereas brachytherapy was associated with higher rates of acute and late genitourinary toxicities and a decline in quality of life [ 3033 ]  . a further retrospective analysis of the ncdb analyzed 14 , 126 patients with intermediate - risk pc . 
an additional subgroup analysis was , however , able to detect an os benet by use of adt in patients meeting all three intermediaterisk criteria ( hr = 0.61 , p = 0.026 ) [ 34 ]  . these ndings afrm that unfavorable groups of intermediate - risk pc patients benet from the application of adt , outweighing adverse events associated with hormonal therapy . on the basis of the present data , a modied treatment recommendation as introduced by the nccn guidelines and the mskcc concept seems to be a promising tool for more adequately addressing an individualized choice of treatment within the large group of intermediate - risk pc patients ( tables 1 and 3 ; [ 6 , 8 ] )  . analogous to the stratication presented above , favorable intermediate - risk pc patients could be treated exclusively with dose - intensied rt , whereas unfavorable patients would benet from a combination therapy of rt and ( at least short - term ) adt . 
additional factors like age , general condition , comorbidities , and the assumed life expectancy are meaningful cofactors for treatment decisions . so far , the german s3 guideline and the european eauestro guideline do not yet consider this subdivision into favorable and unfavorable intermediate risk and the respective consequences for a more individualized treatment ( table 2 ; [ 3 , 4 ] )  . 
thus , currently the treating physician has different treatment options , each conrmed by the divergent guideline recommendations , reected by a wide spectrum of possible therapies in intermediate - risk pc patients . 
a recent ncdb analysis on the use of adt as an adjunct to rt for intermediateand high - risk pc revealed quite heterogenous results . in intermediate - risk pc , the application of adt decreased from 50% in 2004 to 38% in 2012 . 
on the other hand , with 91% of cases , the concept of dose - intensied rt seems to be a common practice in the us [ 35 ]  . lastly , with continuously growing evidence of discrimination factors and especially by the help of advanced genomic proling , the choice of therapy will be further rened [ 36 ]  . in this context , eagerly awaited evidence will be provided by the rtog 0815 trial of dose - intensied rt with or without adt in intermediate - risk pc [ 37 ]  . conclusion rt with and rt without adt are treatment options for patients with intermediate - risk pc . 
new stratication concepts , as implemented in the nccn guideline but not currently used in the german s3 and european eau - estro guidelines , are promising developments toward a more individualized treatment as demonstrated by several clinical analyses and a few randomized trials . 
hence , dose - escalated strahlenther onkol ( 2020 ) 196 : 109116 rt alone in favorable intermediate - risk and its combination with short - course adt ( 46 months ) in unfavorable intermediate - risk patients seems to be an adequate individual treatment option . 
ein randomisierter vergleich zwischen primr radiotherapeutischem oder chirurgischem vorgehen bestand bislang jedoch noch nicht . dies untersuchte die orator - studie . patienten und methodik in diese multizentrische , kanadisch - australische phase - ii - studie wurden patienten in gutem allgemeinzustand ( ecog 02 ) mit einem plattenepithelialien oropharynxkarzinom ( tnm : t12 ; n02 , ( cid : 2 ) 4 cm , ohne extrakapsulres wachstum ; m0 ) eingeschlossen . 
die primre rt bestand aus einer imrt ( intensittsmodulierte radiotherapie ) oder vmat - technik ( volumenmodulierte arctherapie ) mit 70 gy in 35 fraktionen ber 7 wochen auf makroskopische tumoranteile sowie 56 gy auf niedrigrisiko - lymphabusswege und optional 63 gy auf hochrisikolymphabusswege . 
nodal - positive patienten erhielten eine simultane chemotherapie , bevorzugt mit 100 mg / m2 cisplatin alle drei wochen oder alternativ mit wchentlichem originalpublikation nichols ac , theurer j , prisman e et al ( 2019 ) radiotherapy versus transoral robotic surgery and neck dissection for oropharyngeal squamous cell carcinoma ( orator ) : an open - label , phase 2 , randomised trial . 
sekundre endpunkte waren gesamtberleben ( os ) , progressionsfreies berleben ( pfs ) , toxizitt , objektive schluckfunktion ( functional oral intake scale , fois ) sowie die allgemeine gesundheitsbezogene lebensqualitt . ergebnisse von den eingeschlossenen patienten im rtarm erhielten 72 % eine simultane rct . 
bei den primr operierten patienten war wiederum in 47 % eine postoperative rt und in 24 % eine postoperative rct erforderlich . die lebensqualitt , bezogen auf die schluckfunktion , war nach primrer r ( c ) t ( mdadi - score : 86 , 9 ) signikant besser ( p = 0 , 042 ) als nach tors ( mdadi - score : 80 , 1 )  . der signikante unterschied hielt ber ein jahr hinaus bis zum ende der beobachtungszeit nach vier jahren an . fr den mdadi - score wurde die schwelle des klinisch bedeutsamen unterschieds zwar insgesamt nicht erreicht , in 2 von 4 unterkategorien bestand jedoch zustzlich zum statistisch signikanten auch ein klinisch bedeutsamer unterschied zugunsten des radiotherapie - arms . 
die mittels fois untersuchte orale nahrungsaufnahme war bei 100 % der primr radio ( chemo ) therapierten und bei 84 % ( p = 0 , 055 ) der primr operierten patienten uneingeschrnkt mglich . 
dieses war bei p16 - positiven patienten hochsignikant besser als bei p16 - negativen patienten . schlussfolgerungen der autoren die patienten sollten ber die grundstzlich gleichwertigen therapieoptionen bei unterschiedlichem toxizittsprol multidisziplinr beraten werden . kommentar die durchfhrung prospektiver randomisierter studien zum vergleich der lokalen therapieverfahren operation und strahlentherapie ist notorisch schwierig . 
interessant ist die subgruppenanalyse , die keinen signikanten effekt der adjuvanten r ( c ) t auf das schlechtere abschneiden der patienten im tors - arm hinsichtlich der mdadi - werte zeigt . 
eine 2018 verffentlichte randomisierte studie zeigte jedoch ein signikant erhhtes rezidivund todesrisiko nach laparoskopischer operation im vergleich zur offenen operation [ 5 ]  . bei insgesamt vergleichbarem toxizittsausma unterschieden sich die toxizittsprole der therapiearme der orator - studie deutlich . 
insgesamt liegt es nahe , dass die ergebnisse im tors - arm durch die hohe anzahl an patienten mit adjuvanter therapie verzerrt worden sein knnten , auch wenn dies anhand der daten nicht belegbar ist . 
die mglichkeit von radiogenen zweitmalignomen wird in diesem zeitrahmen ebenfalls nicht erfasst . die primre r ( c ) t des oropharynxkarzinoms ermglicht eine tendenziell bessere schluckfunktion und damit bessere lebensqualitt als die tors . 
die therapieoptionen bei oropharynxkarzinomen primre r ( c ) t oder tors sollten nun auf der grundlage der orator - studie in abhngigkeit von den prferenzen der patienten und eines individuell angepassten toxizittsprols diskutiert werden . alexander fabian und david krug , kiel interessenkonikt a . 
cracchiolo jr , baxi ss , morris lg , ganly i , patel sg , cohen ma et al ( 2016 ) increase in primary surgical treatment of t1 and t2 oropharyngeal squamous cell carcinoma and rates of adverse pathologic features : national cancer data base . 
holsinger fc , ferris rl ( 2015 ) transoral endoscopic head and neck surgery and its role within the multidisciplinary treatment paradigm of oropharynx cancer : robotics , lasers , and clinical trials . j clin oncol 33 ( 29 ) : 32853292 5 . 
melamed a , rauh - hain ja , ramirez pt ( 2019 ) minimally invasive radical hysterectomy for cervical cancer : when adoption of a novel treatment precedes prospective , randomized evidence . 
noronha v , joshi a , patil vm , agarwal j , ghosh - laskar s , budrukkar a et al ( 2018 ) once - a - week versus once - every - 3 - weeks cisplatin chemoradiation for locally advanced head and neck cancer : a phase iii randomized noninferiority trial . 
parhar hs , gausden e , patel j , prisman e , anderson dw , durham js et al ( 2018 ) analysis of readmissions after transoral robotic surgery for oropharyngeal squamous cell carcinoma . 
dhanireddy b , burnett np , sanampudi s , wooten ce , slezak j , shelton b et al ( 2019 ) outcomes in surgically resectable oropharynx cancer treated with transoral robotic surgery versus denitive chemoradiation . 
four treatment plans were created for each patient : an imrt and a vmat plan with planning ct ( anatomical plans ) , and an imrt and a vmatplan which integrate the additional information from lung perfusion scintigraphy ( function plans )  . 
dosimetric parameters were compared between all plans for ptv parameters and normal tissue preservation , focusing on optimizing the lung volume receiving at least 20 gy ( v20gy )  . results compared to anatomical plans , functional imrt and functional vmat plans reduced functional lung v20gy in all cases of local and diffuse hypoperfusion patterns of spect defects . 
there were no signicant differences in conformity or heterogeneity indices or ptv median doses between either pair of anatomical and functional plans . conclusion the incorporation of functional imaging for radiotherapy planning in non - small cell lung cancer is feasible and appears to be benecial in preserving a functional lung in non - small cell lung cancer . keywords non - small cell lung cancer lung perfusion single - photon emission computed tomography intensity - modulated radiation therapy volumetric modulated arc therapy introduction the reduction of treatment side effects while achieving lung cancer reasonable local control of non - small cell ( nsclc ) and sustaining its curative potential is an ongoing challenge faced by radiation oncologists and interdisciplinary treatment teams . attempts at dose escalation are limited by radiation damage to normal lung tissue causing radiation pneumonitis ( rp ) , cell death associated inammation , brosis , and de ( cid : 2 ) faegheh s . 
the incidence of radiation pneumonitis is dose and volume dependent and correlates with lung volume receiving a dose of at least 20 gy ( v20gy ) with a risk of pneumonitis higher than 10% when v20gy exceeds 30% [ 14 ]  . 
this side effect seriously impacts quality of life , especially considering the fact that most lung cancer patients frequently have respiratory comorbidity , particularly chronic obstructive pulmonary disease ( copd )  . 
to realize optimal radiotherapy treatment planning , target volume delineation and the methods to maximize sparing of normal tissue must be optimized . lung perfusion single - photon emission computed tomography ( spect ) provides three - dimensional functional information concerning regional perfusion of the lung tissue . 
all had undergone lung perfusion spect and 18f - uorodeoxyglucose ( 18f - fdg ) positron - emission tomography ( pet ) as well as pfts ( pulmonary function tests ) within 3 weeks prior to starting radiotherapy . 
the ct and spect scans were co - registered manually in the tps and fusion was visually evaluated and approved by a nuclear medicine physician and a radiation oncologist . all patients in this study had an abnormal spect perfusion test . 
patients were divided in two groups by a radiation oncologist based on visual evaluation : localized or diffuse hypoperfusion . in this study , all contours , including gross target volume ( gtv ) , clinical target volume ( ctv ) , planning target volume ( ptv ) , and organs at riskwith the exception of functional lung ( fl ) and non - functional lung ( nfl ) were imported from clinically approved plans . 
a new contour of functional lung ( fl ) was created from spect imaging using a threshold of 30% of the maximum uptake for each patient , as well as a new contour of non - functional lung ( nfl ) dened as whole lung ( wl ) minus functional lung ( fl )  . radiotherapy planning two coplanar imrt plans and two coplanar vmat plans were generated for each patient . 
one imrt and one vmat plan used only ct images ( anatomical plans ) and the other two plans were corresponding plans using contours of functional lung volumes derived from co - registered spect images ( functional plans )  . imrt optimization is user dependent [ 10 ]  . 
imrt plans were generated based on a beam angle optimization feature of the treatment planning systethis module starts with a xed number of 72 beams and reduces the number of beams down to a number of 5 to 9 using inverse planning based on the given constraints . this multidimensional optimization algorithm supports the choice of imrt beam angles based on a dosevolume histogram ( dvh )  . 
this was purely a plan simulation study ; therefore , none of the patients were treated using the plan produced . the following constraints were used : ptv : 60 gy to 50% of the ptv ( d50% , icru 83 ) [ 10 ] , spinal canal ( cid : 2 ) 45 gy , mean dose of heart < 26 gy , mean dose of esophagus < 34 gy , and esophagus v55 < 30 gy . 
for the lung we used the following constraints : ( cid : 2 ) anatomical plans : minimize the whole lung volume re ( cid : 2 ) functional plans : minimize the functional lung volume ceiving 20 gy ( wl v20 ) receiving 20 gy ( fl v20 ) although there are various constraints regarding lung v20gy , lung v30gy , and lung dmean , the optimization was performed only with respect to the standard lung v20 constraint , in order to demonstrate the effect of the incorporation of functional information more clearly . data collection and assessment of plans the goal of this study was to compare the difference in radiation dose to functional lung when using anatomical imrt and functional imrt as well as anatomical vmat and functional vmat plans . 
to evaluate the quality of the plans , conformity index ( ci ) heterogeneity index ( hi ) as well as the median dose to the ptv were recorded [ 11 , 12 ]  . the following data were collected from each plan : wl dmean , functional lung v20 ( fl v20gy ) , functional lung v30gy ( fl v30gy ) , functional lung dmean ( fl dmean ) , non - functional lung v20gy ( nfl v20gy ) , non - functional lung v30gy ( nfl v30gy ) , non - functional lung dmean ( nfl dmean ) , dmean and v55gy of esophagus , and dmean of heart . statistics to compare the different planning parameters , the wilcoxon signed - rank test was used ( due to the small size of the collective , this nonparametric test was preferred to the t - test )  . statistical signicance was dened as p < 0.05. 
1 comparison of functional lung volume receiving a dose of at least 20 gy ( fl v20 ) using anatomical imrt ( intensity modulated radiotherapy ) and vmat ( volumetric modulated arc therapy ) and functional imrt and vmat plans using spect ( single - photon emission computed tomography )  . 
five out of 13 patients had patterns of localized hypoperfusions while eight had diffuse hypoperfusion in spect . the conformity and heterogeneity indices were similar between both pairs of anatomical and functional plans . 
a anatomical imrt ( intensity modulated radiotherapy ) plan , b functional imrt plan , c anatomical vmat ( volumetric modulated arc therapy ) plan , d functional vmat plan . 
in this case , the avoidance of the hypoperfused lung was clearly at a cost of conformity loss functional plans achieved lower fl v30 and fl mean as well as lower fl v5 and fl v10 in the whole collective . a signicant increase in nfl v20gy , nfl v30 , and in nfl dmean resulted in both functional plans ( table 2 )  . dose to oars complied with widely accepted clinical tolerance levels . 
for all plans , maximum dose to the spinal canal was less than 45 gy , which is considered a safe dose according to quantec report guidelines [ 13 ]  . 
when compared with anatomical plans , the functional plans resulted in in a signicant increase of dosimetric parameters to the esophagus . the dose distribution of the anatomical and functional plans for case 1 is shown in fig . 
we evaluated the potential benet of such an approach by comparing the dose distribution and dosimetric parameters between anatomy - based and functional - based plans . several studies have related lung v20gy , lung v30gy , and mean lung dose to the rates of symptomatic radiation pneumonitis [ 1 , 4 , 1418 ]  . 
however , it could 156 strahlenther onkol ( 2020 ) 196 : 151158 be postulated that radiation damage to the functional areas of the lungs would have more deleterious effects on overall pulmonary function and on the incidence of rp [ 18 , 19 ]  . we have optimized the radiotherapy plans concerning fl v20gy in order to demonstrate the effect of the incorporation of functional information more clearly , and observed that in comparison to anatomical plans , functional plans resulted in a reduction in fl v20gy and an increase in nfl v20gy . 
in fact , normal lung function is similar to a spectrum [ 24 ] , the use of 30% or 40% cutoff point creates fl and nfl does not match reality . 
in all patients , irradiated volume of the two highest - functioning spect regions were reduced , whereas irradiated volume of the two lower - functioning regions were increased [ 8 ]  . 
a prospective study by farr et al . [ 24 ] in 58 patients was the rst to show that spect - based dfhs have a stronger association with clinical rp after curative imrt than the commonly used standard ct - based dosevolume parameters , and they found that patients who had fl dmean > 16 gy , fl v20gy > 30% , and fl v30gy > 23% went on to develop radiation pneumonitis . 
in our group of patients , we did not observe a difference among diverging patterns of spect hypoperfusion defects ; this may be due to the benets of a dynamic treatment technique that allows for better sparing of well - perfused regions of the lung located within diffuse hypoperfusion , or it could be due to the small size of our collective . to our knowledge , this is the rst study that compares imrt and vmat techniques based on functional imaging of the lung . 
we think that this is a result of localized well - perfused areas which are protected best by choosing radiation beams that do not strike functional lung areas , as localized poorly perfused regions are a preferred pathway for radiation beams targeting the tumor . limitations and future directions this study has notable limitations . 
although the treatment position of all patients was the same during both scans and the manual fusion was evaluated as accurately as possible by a nuclear medicine physician and a radiation oncologist , there is a potential risk of misregistration and in the worst case , it can result in the opposite effect that means higher dose to more functional normal tissue regions . 
additionally , in order to streamline this process , enabling the importation of the dicom modality nm into all treatment planning systems would simplify the incorporation of spect data into radiotherapy planning , thereby increasing its efciency . another limitation of directly using perfusion spect images for planning is that some regions of the lung are temporarily hypoperfused due to mechanical effects of tumors such as bronchial obstruction and large vessel compression , but could potentially recover during rt treatment . 
however , if the potentially recoverable lung had received a higher radiation dose due to classication as non - functional on prestrahlenther onkol ( 2020 ) 196 : 151158 treatment imaging , the chance for recovery could be lost [ 2730 ]  . 
therefore , adaptive radiotherapy planning based on lung perfusion spect may enable the sparing of functionally recoverable lung tissue and tumor - induced hypoperfusion areas observed during pre - rt spect . another source of weakness lies in the fact that we considered a perfusion value of 30% or more of the maximum radioactivity in perfusion spect to be functional and the remaining regional lung was not . 
whether a selected threshold is clinically relevant should be investigated in future studies . conclusion that our data suggest the implementation of perfusion spect into treatment radiotherapy planning in non - small lung cancer is feasible and appears to be benecial in lung . 
vanderhelst1 received : 21 february 2019 / accepted : 22 june 2019 / published online : 12 july 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose to evaluate alterations in pulmonary function indices after helical tomotherapy and explore potential associations with biologically corrected dosimetric parameters . patients and methods in 64 patients with inoperable locally advanced non - small cell lung cancer , pulmonary function tests before and within 6 months after radiotherapy were evaluated retrospectively . 
in 44 patients , late pulmonary function changes ( 6 months after radiotherapy ) could also be assessed . results in the entire patient group , there were signicant declines in forced expiratory volume in 1s ( fev1 ) ( average change 4.1% predicted ; p = 0.007 ) , in forced vital capacity ( fvc ) ( 4.9% predicted ; p = 0.002 ) , total lung capacity ( tlc ) ( 5.8% predicted ; p = 0.0016 ) and dlco ( diffusing capacity of the lung for carbon monoxide corrected for hemoglobin level ) ( 8.6% predicted ; p < 0.001 ) during the rst 6 months . 
v5 gy or v10 gy did not contribute to any of the lung function changes . conclusions the decline in pulmonary function indices after helical tomotherapy was of similar magnitude to that observed in studies reporting the effect of conformal radiotherapy on lung function . 
bei 44 der 64 patienten konnten auch lngerfristige funktionelle vernderungen ( 6 monate nach strahlentherapie ) ermittelt werden . ergebnisse im gesamten patientenkollektiv wurden innerhalb der ersten 6 monate signikante verminderungen der einsekundenkapazitt ( fev1 ) ( durchschnittliche nderung 4 , 1% / %sollwert ; p = 0 , 007 ) , in forcierte vitalkapazitt ( fvc ) ( 4 , 9% / %sollwert ; p = 0 , 002 ) , totale lungenkapazitt ( tlc ) ( 5 , 8% / %sollwert ; p = 0 , 0016 ) und dlco ( diffusionskapazitt ) ( 8 , 6% / %sollwert ; p < 0 , 001 ) gemessen . 
die entsprechende verminderung von fev1 , fvc , tlc und dlco in der gruppe mit spteren messungen ( im durschnitt 11 , 3 monate ) waren 5 , 7 , 7 , 4 , 7 , 0 , 9 , 8% / %sollwert . 
die multivarianzanalyse unter bercksichtigung von v5 gy , v10 gy , v20 gy , v40 gy , v60 gy , mittlere lungendichte ( mld ) , makroskopische tumorvolumen ( gtv ) und planungszielvolumen ( ptv ) als mgliche kovariablen zeigte , dass das gtv den strksten einuss hatte . 
v5 gy und v10 gy trugen nicht zur verschlechterung der lungenfunktion bei . schlussfolgerung nach helikaler tomotherapie verschlechterten sich die lungenfunktionsparameter in hnlicher weise wie in den studien mit konformaler strahlentherapie . 
keine der vernderungen in der lungenfunktionsprfung war abhngig vom lungenvolumen , das geringen strahlendosen ausgesetzt war . schlsselwrter lungenfunktionsparameter bestrahlungsschden geringe strahlendosen intensittsmodulierte strahlentherapie inoperables nicht - kleinzelliges lungenkarzinom introduction more than one - third of patients with non - small cell lung cancer ( nsclc ) present with locally advanced tumors ( stage iiia or iiib ) at initial diagnosis [ 1 ]  . 
for the majority of patients concurrent chemoradiation is still considered the cornerstone of treatment in order to offer the highest potential for prolonged progression - free and overall survival [ 3 , 4 ]  . 
more recently , the pacific trial demonstrated a survival advantage of the programmed death - ligand 1 ( pd - l1 ) inhibitor durvalumab as consolidation treatment for patients with stage iii , unresectable nsclc who have not progressed following chemoradiotherapy [ 7 ]  . conventional fractionated radiotherapy ( crt ) is known to be associated with signicant decline in lung function up to 12 months after treatment , as assessed by pulmonary function tests . 
studies of lung function changes after conformal radiotherapy in nsclc patients consistently report reductions of the absolute value of carbon monoxide diffusing capacity ( dlco ) ranging from 10 to 15% with respect to baseline [ 8 , 9 ]  . 
parameters reecting obstruction and restriction such as fev1 and fvc are less frequently affected by radiotherapy , and it has been suggested that this could be due to concomitant tumor response [ 9 ]  . new radiation techniques are being developed in order to reduce lung toxicity by preserving surrounding normal tissues . 
 [ 11 ] , imrt reduced the lung volume receiving at least 20 gy ( v20 gy ) and mean lung dose ( mld ) by approximately 15% , compared to 3d - crt in patients with node - positive tumors . 
however , concerns have been raised since imrt exposes larger volumes of normal lung 144 strahlenther onkol ( 2020 ) 196 : 142150 tissue to low radiation doses ( low - dose bath ) increasing lung volume receiving at least 5 gy ( v5 gy )  . 
 [ 13 ] raised the concern that imrt may augment the risk for radiation pneumonitis in these low - dose areas when it was combined with chemotherapy . vmat ( volumetric arc therapy ) , another arc - based therapy , has been associated with an even higher risk for radiation pneumonitis [ 14 ]  . 
these rates may be even higher in real life since patients with early radiographic signs of pneumonitis were excluded in that trial . the objectives of the present study were to assess shortand longer - term changes in pulmonary function tests after helical tomotherapy and to look for potential associations of lung function decline with biologically corrected dosimetric parameters . materials and methods patient characteristics we conducted a retrospective analysis of changes in pulmonary function tests ( pft ) of patients enrolled in 2 prospective trials using helical tomotherapy in unresectable nsclc . 
participants had locally advanced disease ( stage iii according to ajcc 7th edition staging ) or were deemed inoperable , due to comorbid medical illness , poor pulmonary function or tumor extent . 
initial workup consisted of bronchoscopy , pft , computed tomography ( ct ) of the thorax , fdg - positron emission tomography ( pet ) , magnetic resonance imaging ( mri ) of the brain , and additional imaging studies as indicated . 
the primary clinical target volume ( ctv ) consisted of a 5 mm margin around the gross tumor volume ( gtv ) in the lungs or airways without bone , vessel , or other mediastinal organs , unless there was proven tumoral invasion . 
the planning target volume ( ptv ) for the primary tumor was an isotropic expansion around the ctv , of 5 mm for tumors located in upper / middle lobe , or 8 mm for tumors in the lower lobe . 
in both cases , we used the helical tomotherapy hiart ii system ( tomotherapy inc . , madison , wi , usa ) which combines a rotational imrt technique and image - guidance using megavoltage computed tomography . 
in the planning process , we aimed at a v20 gy for lungs of 30% and an mld of 17 gy , a maximal dose of 53 gy to the spinal cord , maximal dose of 63.8 gy to the esophagus . 
we used a chemotherapy regimen with cisplatin ( 20 mg / m2 / week ) and docetaxel ( 20 mg / m2 / week ) analogous with other studies [ 17 ]  . pulmonary function tests pfts were obtained according to european respiratory society guidelines [ 18 ]  . 
lung function measurements consisted of forced expiratory volume in 1 s ( fev1 ) , forced vital capacity ( fvc ) , total lung capacity ( tlc ) and carbon monoxide transfer factor ( dlco )  . 
dlco values were rst adjusted for hemoglobin level , using the multiplicative correction factor 1.7 hb / ( 9.38 + hb ) ( female ) or strahlenther onkol ( 2020 ) 196 : 142150 1.7 hb / ( 10.22 + hb ) ( male ) , assuming hb is expressed in g / dl [ 19 ]  . 
the resulting index of lung volume corrected diffusing capacity ( expressed in the same units as dlco ) was named dlco , corr . at each visit , all parameters were expressed as a percent of the predicted value for each subject ( % predicted ) , based on recent reference equations [ 21 ]  . cova was performed by maximization of adjusted r2 and backward elimination to correct for multicollinearity , to determine the dosimetric variables to be retained as potential predictors in the statistical model . 
all statistical analyses were veried for normality of the residues using kolmogorovsmirnov and shapirowilk tests . statistical analysis first , lung function variables were inspected for signicant differences from baseline by repeated measures anova with bonferroni correction . 
third , an anresults the cohort of patients with cytologically or histologically conrmed inoperable non - small cell lung cancer treated with radio ( chemo ) therapy ( rct ) between november 2006 fig . 
ct computed tomography , pft pulmonary function tests 112 patients with non - small cell lung cancer 12 excluded for missing values < 4 months before start rt 2 excluded for missing values after rt 5 excluded for pleural effusion on planning ct 93 patients 77 patients 64 patients = group a 44 patients = group b 16 excluded for progressive disease in the first six months 13 excluded for missing value < 6 months after rt 13 patients died before the 6months pft measurement 7 excluded for progressive disease after six months 146 strahlenther onkol ( 2020 ) 196 : 142150 ( p = 0.009 ) ( p = 0.02 ) ( p < 0.001 ) ( p = 0.007 ) ( p = 0.002 ) 10 11 12 13 14 15 10 11 12 13 14 15 time a ( cid : 2 ) er radiotherapy ( months ) time a ( cid : 2 ) er radiotherapy ( months ) ( p = 0.02 ) ( p = 0.014 ) ( p < 0.001 ) ( p = 0.002 ) ( p < 0.001 ) 10 11 12 13 14 15 10 11 12 13 14 15 time a ( cid : 2 ) er radiotherapy ( months ) time a ( cid : 2 ) er radiotherapy ( months ) fig . 
a forced expiratory volume in 1 s ( fev1 ) , b forced expiratory volume ( fvc ) , c total lung capacity ( tlc ) , d diffusing capacity ( dlco ) and february 2014 , included in this study is illustrated in fig . 
of these patients , 46 ( 72% ) received platinum - based concurrent chemotherapy , 12 patients ( 19% ) were treated with sequential chemoradiation therapy and 6 patients ( 9% ) received radiotherapy in monotherapy . 
when relating such dlco decreases to an average patient in our study , a grade 1 and 2 toxicity corresponds to a dlco decrease of respectively 1322% predicted and > 2235% predicted . 
purely based on dlco decline , 11 of our patients ( 17% ) would thus be attributed toxicity grade 1 and 6 patients ( 9% ) grade 2 during follow - up over the rst 6 months . relationship of pft to dosimetry table 2 shows the correlation coefcients between pft decline that was available in all patients ( i.e. , the lung function change from baseline to < 6 months ) and all dosimetric parameters considered in the multivariate analysis . 
only in the case of fev1 is this gtv effect counteracted by a small contribution from ptv ( due to colinearity of ptv and gtv ) , but the net effect is that of a negative impact of gtv on fev1 . 
v40 gy also independently contributes to fev1 decline , but no low dose volume ( v10 gy , v5 gy ) was retained in the multivariate model for fev1 , nor for any other lung function decline . 
average decreases in spirometric fev1 and fvc were somewhat smaller than the dlco decrease , possibly due to reopening of formerly obstructed airways in the context of tumor response . similar results were reported in a prospective study by schrder et al . 
 [ 25 ] conducted a retrospective analysis comparing lung function changes after rt delivered with three different radiation therapy techniques ( 3d - crt , imrt and proton beam therapy )  . 
a median dlco change of 17% baseline was observed at three different time intervals ( 04 , 58 and 912 months ) , regardless of technique . in these previous studies [ 22 , 25 ] , decline in pft following radiotherapy was expressed as a percentage of the patients baseline value ( prior to radiotherapy ) , which is low in these patient populations . 
to accommodate the low baseline lung function in patients with obstructive lung disease , improvement or loss of lung function after intervention is usually expressed in terms of % predicted for any given patient . 
however , these results are still a matter of debate [ 24 ]  . long - term studies of lung function after radiotherapy are scarce because unresectable non - small cell lung cancer has a poor outcome with overall 5 - year survival of 520% . 
 [ 27 ] performed a ( small ) prospective clinical study with longer follow - up times ( up to 38 months ) to look for long - term changes . they observed a decline in all pft values 6 months after treatment with a plateau by 12 months . 
 [ 28 ] , comparing lung function changes in patients with nsclc , sclc and esophageal carcinoma treated with two different techniques : imrt ( irradiation of a lower volume with a greater dose ) versus vmat ( irradiation of a greater volume with a lower dose )  . 
 [ 25 ] , i.e. , no correlation of pft with v5 gy in their study , yet , they did nd a correlation between dlco decline and gtv , mld , v20 gy and v40 gy . 
in our tomotherapy study , the only signicant correlate of dlco decline was gtv , calculated as the sum of gtv for the primary tumor and the nodes ( table 3 )  . 
hence , the tumor volume seems to be the best parameter to predict lung damage after radiotherapy in this patient population . a potential limitation of this study is the heterogeneity of the patient population treated with radiotherapy , in terms of whether they had concomitant or sequential chemotherapy . 
in the corresponding observation period ( 2.8 months on average ) grade 3 acute pneumonitis only occurred in 2 of out 64 patients , and grade 4 in none of the patients . 
hence this effect ( and the cumulative effect of treatment for pneumonitis ) could not be rigorously studied here . in conclusion , declines in pulmonary function indices during the rst 6 months after helical tomotherapy are similar to those observed in studies following conformal radiotherapy . 
with the role of low - dose regimens such as 2 2 gy being uncertain , we compared conventional - dose rt to a low - dose approach and investigated outcome and toxicities . materials and methods we retrospectively reviewed the medical records of 26 patients with 44 cutaneous lesions treated at our institution between 2007 and 2017 , comprising 22 marginal zone lymphoma ( pcmzl ) lesions and 22 follicle center lymphoma ( pcfcl ) lesions . 
however , the response rates were signicantly lower for this group and ldrt may therefore not be recommended as standard treatment . keywords low - dose rt skin lymphoma toxicity clipi 2 2 gy deeskalierte strahlentherapie beim indolenten primr kutanen b - zell - lymphom zusammenfassung zielsetzung die strahlentherapie ( rt ) hat eine etablierte rolle in der kurativen behandlung indolenter primr kutaner b - zell - lymphome ( pcbcl )  . 
allerdings waren die ansprechraten signikant niedriger , sodass die ldrt nicht als standard empfohlen werden kann . schlsselwrter niedrigdosis - strahlentherapie hautlymphom toxizitt clipi 2 2 gy background materials and methods primary cutaneous b - cell lymphomas ( pcbcl ) represent approximately 20% of all primary cutaneous lymphoma and are dened by a restricted disease spread to the skin without evidence of extracutaneous involvement at diagnosis [ 15 ]  . 
they encompass three main types : primary cutaneous marginal zone lymphoma ( pcmzl ) , primary cutaneous follicle center lymphoma ( pcfcl ) , and primary cutaneous diffuse large b - cell lymphoma , leg type ( pcdlbcl , lt ) , of which the rst two entities are indolent [ 1 , 36 ]  . radiotherapy ( rt ) is part of the therapeutic mosaic for pcbcl and recommended by both national and international guidelines for a localized disease pattern , conferring high local control rates with a conservative approach [ 3 , 5 , 7 , 8 ]  . 
curative doses cover a range of 1854 gy [ 918 ]  . there is accumulating evidence for a possible de - escalation of rt dose while maintaining high response rates and thereby opening a role for low - dose rt ( ldrt ) , which has been successfully shown for other indolent non - hodgkin lymphoma [ 13 , 14 , 1923 ]  . 
however , the rarity of pcbcl and retrospective nature of studies make a denitive dose recommendation troublesome . the following analysis demonstrates the use and longterm effectiveness of different rt doses with regard to local control rate and relapse patterns . 
the study also evaluated toxicity data of the rt regimens , thereby providing a clinical decision - making aid for rt of pcbcl . we retrospectively reviewed the medical records of 26 patients with 44 cutaneous lesions treated at our institution between 2007 and 2017 ( see table 1 for details )  . 
all patients were still alive at the end of the study . statistical analysis time - dependent event curves were generated by the kaplanmeier method and compared with log - rank tests . 
concerning clipi , no patient had low risk ( score 0 ) , eight patients ( 31% ) had intermediate risk ( score 1 ) , 13 patients had high risk ( 50% ; 12 score 2 and one score 3 ) , and 5 patients risk group was unknown . 
thirty - three lesions were treated with electrons ( 75% ) and 11 ( 25% ) lesions were treated with photons . the overall response rate ( orr ) was 91% ( complete response rate [ crr ] : 75% )  . 
it further points out the potential role of ldrt , which may have an emerging role and may offer a strategy for re - treatment in case of refractory or relapsed pcbcl . overall , crr after rt reaches 75% in this analysis , which is in accordance with the excellent results from the literature differing between 75 and 100% [ 10 , 11 , 13 , strahlenther onkol ( 2020 ) 196 : 126131 fig . 
2 kaplanmeier curves of progression - free survival for intermediate ( blue ) and high risk patients ( red ) according to cutaneous lymphoma international prognostic index ( clipi ) in months . 
clipi encompasses three variables ( elevated lactate dehydrogenase , > 2 lesions , nodular disease ) dening three risk categories ( low risk : 0 factors , intermediate risk : 1 factor , high risk : 23 factors ) 1719 , 22 ]  . 
anyhow , previous studies struggled in dening the minimal dose for adequate treatment response , as dose comparisons are rare , include only few patients , or report only a short follow - up [ 12 , 14 , 19 ]  . 
further deescalation was performed by pashtan et al . , who proposed 30 gy / 30.6 gy as no recurrence occurred in this treatment group after 5 years [ 16 ]  . 130 strahlenther onkol ( 2020 ) 196 : 126131 table 2 overview of low - dose rt concepts for pcbcl with treatment data and results study lesions rt dose in gy median ( range ) akhtari [ 19 ] 30 ( 439.6 ) orr / crr in 100 / 100 median follow - up 29 months lc in % > 95% low - dose : 4 ( 412 ) goyal [ 13 ] knig [ 25 ] neelis [ 22 ] present study 40 ( 450 ) low - dose : low - dose : 19 months 47 months 21 months 13 months 76 months low - dose : 52 months 100 / 94.1 90 / 82 86 / 75 91 / 75 low - dose : 86 / 29 low - dose : 100 ( 2 years ) 93.3 ( 1 year ) 91.1 ( 2 years ) n . 
a. acute grade i / ii : 61% / 9% acute grade i / ii : 14% / 0% response rates and local control for the study of knig et al . 
data not available considerable efforts have been made in investigating the role of 4 gy as a rt treatment option both for nodal und extranodal indolent lymphomata [ 13 , 14 , 20 , 25 , 26 ] , which was also the dose of this studys ldrt group ( see table 2 for an overview on low - dose rt for pcbcl )  . 
however , followup in most of the aforementioned studies is shorter than 3 years ( see table 2 ) , whereas the present study demonstrates a long - term observation which may better reect the indolent course of pcbcl . 
it has to be kept in mind that ineld progression or recurrence is not necessarily prevented by dose escalation [ 11 , 18 ] and that re - treatment could be performed safely ( see [ 29 ] for review )  . 
concepts for re - treatment include 4 gy , 30 gy [ 19 , 26 ] , or hypofractionated regimens [ 22 ]  . recently , the international extranodal lymphoma study group established a prognostic index ( clipi ) encompassing three variables ( elevated ldh , > 2 lesions , nodular disease ) and dening three risk categories ( low risk : 0 factors , intermediate risk : 1 factor , high risk : 23 factors ) for diseasefree survival and pfs [ 24 ]  . 
no signicant risk stratication could be established for the study collective , although the patient numbers may be too small to demonstrate this . the presented study shows some limitations , being a retrospective , monocentric study . 
additionally , pcdlbcl , lt was intentionally left out of the study collective to avoid confounding due to this entitys distinctive biology with an aggressive behavior and worse prognosis [ 6 , 11 , 17 , 18 ]  . in the future , the inclusion of pcbcl in multicenter studies or clinical registers is highly recommended to further delineate interdisciplinary treatment . 
with the advent of novel treatment agents like the brutons kinase inhibitor ibrutinib , which is already used off - label for pcbcl [ 3 , 7 ] , putative combinations with rt are at hand . 
they may further help in decreasing rt intensity while maintaining high response rates . eventually , this will help in lifting the fog to reveal the cryptic minimal necessary rt dose . conclusion this long - term analysis conrmed that rt is an effective treatment with excellent survival rates and minimal toxicities in the management of primary indolent cutaneous lymstrahlenther onkol ( 2020 ) 196 : 126131 phoma . 
our objectives were to compare efcacy between hyperfractionated thoracic radiotherapy ( trt ; 1.5 gy 2 times per day [ bid ] in 30 fractions ) and hypofractionated trt ( 2.5 gy once per day [ qd ] in 22 fractions ) , and to explore prognostic factors inuencing the prognosis , such as the timing of trt . methods patients enrolled in two independent prospective studies were combined and analyzed . 
time ( days ) from the start of chemotherapy to the end of trt ( ser ) ( cid : 2 ) 63 ( hr 0.50 , 95% ci 0.320.80 ; p = 0.003 ) and prophylactic cranial irradiation ( hr 0.43 ; 95% ci 0.290.63 ; p = 0.000 ) were favorably related to os . 
the incidence of acute esophagitis was signicantly higher in the hyperfractionated arm . keywords lung cancer , small cell limited stage thoracic radiotherapy radiation dose prognosis xiao hu and bing xia contributed equally to this study as co - rst authors . ( cid : 2 ) xiao - long fu xlfu1964@126.com ( cid : 2 ) ming chen chenming@zjcc.org.cn 1 department of radiation oncology , cancer hospital of the university of chinese academy of sciences , department of radiation oncology , zhejiang cancer hospital , zhejiang provincial key laboratory of radiation oncology , institute of cancer research and basic medical sciences , chinese academy of sciences , 1 banshan road east , 310022 hangzhou , china 2 department of radiation oncology , hangzhou cancer hospital , hangzhou , china 3 department of radiation oncology , cancer hospital of fudan university , shanghai , china 4 department of radiation oncology , the first afliated hospital of sun yat - sen university , guangzhou , china 5 department of medical oncology , cancer hospital of the university of chinese academy of sciences , department of medical oncology , zhejiang cancer hospital , institute of cancer research and basic medical sciences , chinese academy of sciences , hangzhou , china 6 department of radiation oncology , shanghai jiao tong university afliated chest hospital , 241 huaihai road west , 200030 shanghai , china strahlenther onkol ( 2020 ) 196 : 172181 der zeitpunkt der thorakalen strahlentherapie ist wichtiger als die dosisintensivierung bei patienten mit limitiertem stadium des kleinzelligen lungenkarzinoms : ein paralleler vergleich von zwei prospektiven studien zusammenfassung zielsetzung die optimale dosis fr die radiotherapie des kleinzelligen lungenkrebses ( sclc ) im begrenzten stadium ist nicht genau deniert . 
hier sollen die wirksamkeit der hyperfraktionierten thoraxradiotherapie ( trt ; 1 , 5 gy zweimal pro tag [ bid ] in 30 fraktionen ) mit der hypofraktionierten trt ( 2 , 5 gy einmal pro tag [ qd ] in 22 fraktionen ) verglichen und prognostische faktoren , wie der zeitpunkt der trt , untersucht werden . methoden die daten von patienten , die an zwei unabhngigen prospektiven studien teilnahmen , wurden gepoolt analysiert . 
mithilfe einer multivariaten cox - regressionsuntersuchung wurde erkannt , dass die zeit ( in tagen ) vom beginn der chemotherapie bis zur trt ( tct ) ( cid : 2 ) 43 mit einem verbesserten lrc assoziiert war ( hazard ratio [ hr ] 0 , 39 ; 95 % - ki 0 , 200 , 76 ; p = 0 , 005 )  . 
eine akute strahlensophagitis vom grad 2 / 3 wurde mit 37 , 0 % bei patienten im hyperfraktionierten und mit 17 , 7 % im hypofraktionierten arm beobachtet ( p = 0 , 003 )  . schlussfolgerung in dieser untersuchung erzielten die hyperfraktionierte sowie die hypofraktionierte trt beide eine gute lrc und os bei patienten mit sclc im beschrnkten stadiudie einhaltung von tct ( cid : 2 ) 43 und ser ( cid : 2 ) 63 fhrten zu einer besseren prognose . 
das auftreten einer akuten sophagitis war im hyperfraktionierten arm signikant huger . schlsselwrter kleinzelliger lungenkrebs limitiertes stadium thorax - strahlentherapie strahlendosis zeitpunkt der strahlentherapie introduction small cell lung cancer ( sclc ) , which accounts for approximately 13% of all bronchogenic carcinomas [ 1 ] , is one of the most malignant tumors with rapid proliferation . 
systemic chemotherapy is the basis of treatment for sclc [ 2 ]  . for most patients with limited - stage sclc , thoracic radiotherapy ( trt ) combined with concurrent chemotherapy is the standard of care at present [ 3 ]  . 
however , the optimal dose / fraction scheme and timing of trt remain controversial . the results of a large - scale prospective randomized study , convert / nct00433563 , that compared hyperfractionated trt ( 1.5 gy twice daily to 45 gy ) with highdose conventional fractionated trt ( 2 gy once a day to 66 gy ) administered concurrently with chemotherapy were recently published [ 5 ]  . 
the results , however , suggested that high - dose conventionally fractionated trt did not improve prognosis compared to standard hyperfractionated trt . twice - daily trt ( 45 gy in 30 fractions ) indicated no statistically signicant difference of os and pfs between the two arms [ 6 ] , there is no prospective phase iii study available comparing the efcacy of hypofractionated or hyperfractionated trt up to now . recently , xia et al . 
the 2 - year progression - free survival rate was 49.0% , the median survival time was 28.5 months , and the 2 - year os rate was 58.2%. this hypofractionated trt scheme is now being compared with conventionally fractionated trt in a phase iii trial ( nct02990780 )  . 
in the meantime , we have carried out a prospective trial ( nct01731548 ) [ 8 ] using the same hyperfractionated radiotherapy schedule as the convert study [ 5 ]  . 
this trial has been closed recently . although many efforts have been made to increase the dose of radiotherapy in order to achieve better prognosis , pijls - johannesma et al . 
 [ 10 , 11 ] addressed the importance of timing of trt in the treatment of limited - stage sclc . although a phase ii norwegian trial that compared oncedaily hypofractionated trt ( 42 gy in 15 fractions ) with thus , in the present study , we retrospectively compared these two contemporaneous prospective trials [ 7 , 8 ]  . 
the 174 strahlenther onkol ( 2020 ) 196 : 172181 main purpose was to study which factor was more important for prognosis : the higher radiation efcacy achieved by the hypofractionated trt or the timing of trt ? diotherapy artrt was administered concurrently with the second or third cycle of chemotherapy . bed calculation materials and methods patient selection the inclusion criteria of the two prospective studies were identical . 
we enrolled patients with histologically or cytologically veried sclc and radiologically ( including brain ct / mri , chest and abdomen contrasted ct , and bone scintigraphy ) conrmed limited - stage ( including bilateral supraclavicular , bilateral mediastinal , and ipsilateral hilar lymphadenopathy ) sclc , with no malignant pleural or pericardial effusion . 
the patients were between 18 and 75 years old ; without previous trt , chemotherapy , or biotherapy ; eastern cooperative oncology group performance status 0 to 1 ; and adequate hematologic , cardiac , pulmonary , renal , and hepatic function . 
in the hyperfractionated radiotherapy arm , patients received 1.5 gy twice daily in 30 fractions over 19 days to 45 gy [ 8 ] , while in the hypofractionated radiotherapy arm , patients received 2.5 gy once a day in 22 fractions over 30 days to 55 gy [ 7 ]  . the study was approved by the clinical ethics committee of our institution . thoracic radiotherapy techniques three - dimensional conformal radiotherapy ( 3d - crt ) or intensity - modulated radiotherapy ( imrt ) was used . 
involved - eld radiotherapy was applied in both studies . chemotherapy chemotherapy in the hyperfractionated radiotherapy arm consisted of etoposide ( 100 mg / m2 on days 1 to 3 ) and cisplatin ( 80 mg / m2 on day 1 ) administered intravenously at 3 - week intervals for 4 to 6 cycles . 
trt was administered concurrently with cycle 3 of chemotherapy . the hypofractionated radiotherapy arm received etoposide ( 70 mg / m2 on days 1 to 4 ) and cisplatin ( 25 mg / m2 on days 1 to 3 ) administered intravenously at 3 - week intervals for 4 to 6 cycles . 
however , the interval was extended to 4 weeks during concurrent trt in the hypofractionated rafor calculation of the biologically effective dose ( bed ) , the following formula was used : bed = ( nd ) [ 1 + d / ( / ) ] ( 0.693 / ) [ ( t tk ) / tpot ] , where n is the number of fractions , d is the fraction size , t is the overall trt time ( days ) , and factors / ratio , , tk , and tpot were assumed to be 10 gy , 0.3 gy , 21 days , and 3 days , respectively . follow - up scheme patients were periodically reviewed 1 month after treatment and every 3 months until 2 years , every half a year for 3 years , and then once a year thereafter . 
late toxicities of the lung were evaluated according to rtog / eortc criteria [ 12 ] 3 to 4 months after trt . statistical analysis lrc was calculated from the time of induction chemotherapy to the date of local / regional progression . 
a statistical software package spss 13.0 ( ibm , somers , ny , usa ) was applied and the kaplanmeier method was used to estimate survival data . the distribution of the survival time between the arms was tested using the log - rank method . 
all p - values were based on a two - sided test , and the differences were regarded as statistically signicant when p < 0.05. results patient characteristics between march 2005 and may 2014 , 92 patients were enrolled into the hyperfractionated radiotherapy arbetween strahlenther onkol ( 2020 ) 196 : 172181 table 1 characteristics of the patients according to treatment hyperfractionated ( n = 92 ) no . 
among patients in the hyperfractionated radiotherapy arm who received pci , 14 ( 23.3% ) patients received 30 gy in 15 fractions and 46 ( 76.7% ) patients received 25 gy in 10 fractions . 
2 the overall survival of patients who received hyperfractionated or hypofractionated radiotherapy tumor response evaluation tumor response was evaluated 1 month after completion of trt and chemotherapy with enhanced ct scans of the chest and abdomen . 
late lung injury was comparable and moderate in both arms . clinical features that potentially aect lrc and os possible clinical features that might affect lrc and os were analyzed using the univariate cox proportional hazards regression model . 
stage iii was a negative factor for os ( hr , 3.44 ; 95% ci , 1.269.35 ; p = 0.01 ; table 4 )  . the mean values of tct ( cid : 2 ) / > 43 days and ser ( cid : 2 ) / > 63 days of the hyperfractionated and hypofractionated radiotherapy arms are summarized in table 5 . discussion in this retrospective study , we compared standard hyperfractionated radiotherapy with hypofractionated radiotherapy combined with concurrent chemotherapy for limitedstage sclc . 
subsequent studies have shown that intensication of the dose of trt could improve survival [ 1316 ]  . a series of prospective studies have tried to improve survival of limited - stage sclc patients by increasing bed of conventional fractionated radiotherapy . 
subsequently , cancer and leukemia group b ( calgb ) conducted a series of prospective studies ( 39808 , 30002 , and 30206 ) [ 1820 ] on the use of this dose in combination with concurrent chemotherapy . 
however , the intensication of bed did not translate into better outcomes , even if patient characteristics of the two arms were comparable . therefore , intensication of the trt dose alone might not improve the prognosis of limited - stage sclc ; other factors that could inuence the efcacy of radiotherapy should be considered . a number of studies have shown that an accelerated repopulation of tumor cells was observed after induction chemotherapy and radiotherapy [ 2224 ]  . 
the timing of trt has been a hot area of research for years [ 9 , 10 , 2531 ]  . in this study , although hyperfractionated trt was designed to start with the third cycle of chemotherapy ( time from chemotherapy to thoracic radiotherapy , tct = 43 days ) , and hypofractionated trt was designed to start with the second ( tct = 22 days ) or third cycle of chemotherapy ( tct = 43 days ) , treatment - related toxicities and logistical problems caused the delayed initiation of trt , thus making tct > 43 days . 
while in multivariate analysis , the ser ( cid : 2 ) 63 days ( hr , 0.50 ; 95% ci , 0.320.80 ; p = 0.003 ) remained a favorable prognostic factor for os . a south korean phase iii study compared trt ( 52.5 gy in 25 fractions over 5 weeks , bed = 54.3 gy ) administered with either the rst or the third cycle of chemotherapy for patients with limited - stage sclc . 
 [ 11 ] used individual patient data meta - analysis to compare the impact of earlier or later trt and shorter or longer ort on os of limited - stage sclc patients . 
this is consistent with the results of the present study , that ser ( cid : 2 ) 63 days can signicantly improve os . at present , we do support the notion that thoracic radiotherapy should be performed as early as possible . 
considering that in both arms more than 90% of patients were stage iii , the 5 - year os rates of about 27% were still satisfactory . accelerated hyperfractionated radiotherapy can complete treatment in a relatively short period of time , overcome tumor cell repopulation , and spare late - response organs , but signicantly increased acute esophagitis [ 33 ]  . despite of the benets , hypofractionated radiotherapy might have an impact on late - response organs . 
 [ 10 ] suggested that tct and ser less than 30 days could signicantly improve survival , we did not nd that that result had an obvious effect on lrc and os in this study using multivariate cox regression analysis . 
second , the impact of salvage therapy on os after disease progression was not analyzed in this study , and recurrent sclc still benets from second - line chemotherapy [ 35 ]  . 
third , the follow - up time was relatively short for some patients ; consequently , the radiation - induced late response of the lung may not have been observed . 
additionally , the late toxicities of the heart and esophagus were not recorded in this study . last but not least , about a third of patients who achieved cr or pr after chemoradiotherapy refused pci , with concerns regarding potential neurotoxicity , despite the fact that pci is favorably associated with improved survival . this retrospective study indicated that both hyperfractionated and hypofractionated trt administered with concurrent ep chemotherapy could achieve good lrc and os , although there were no signicant differences between the two schedules . 
the treatment - related toxicities were comparable except for acute esophagitis , which was more frequently observed in the hyperfractionated aron the basis of the results of de ruysscher et al . 
the project presented here investigates and improves a rapid method to detect such errors by performing online dose verication through the analysis of electronic portal imaging device ( epid ) images . methods to validate the method , a respiratory phantom with inhomogeneous insert was examined under various scenarios : no - error and error - simulated measurements . 
both for phantom and patient cases , dose distributions were compared using the gamma index method according to analysis protocols in the target volume . results the comparison of error - introduced epid - measured images to reference images showed no signicant differences with 3% / 3 mm gamma evaluation , though target coverage was strongly underestimated . 
thus , the approach / prototype provides a fast and easy quality assurance procedure for treatment delivery verication . keywords electronic portal imaging device stereotactic body radiation therapy quality assurance in vivo dosimetry real time transit dosimetry these authors contributed equally to this work : c . 
therefore , it is essential to effectively monitor the target to ensure that the tumor is within the beam aperture . research has illustrated that clinically approved plan quality can differ signicantly [ 310 ]  . 
however , traditional pre - treatment qa is not able to detect changes in patient anatomy and there is still the possibility of systematic and random delivery uncertainties between / during each fraction . 
nevertheless , when dealing with dynamic tumors , difculties are still encountered with 3d matching in terms of clearly depicting the tumor and identifying and reproducing its location [ 14 ]  . studies on tumor motion reported the majority of respiration movements to happen in the superiorinferior ( si ) direction , especially the lower lobe of the lung exhibits the most considerable amount of motion [ 15 , 16 ]  . 
therefore , transit dosimetry can play a key role in the verication procedure chain . to some extent , the quality and safety of treatment have been investigated by a widely available electronic portal imaging device ( epid ) [ 20 , 21 ]  . 
some errors during three - dimensional conformal radiation therapy ( 3dcrt ) and intensity - modulated rt ( imrt ) that could not be noticed by pre - treatment qa were detected by means of epid - based in vivo dosimetry [ 28 ]  . 
the detectability threshold of the process was studied under comparisons of improved and local gamma index method using different analysis protocols for various delivery techniques . materials and methods phantom study and treatment delivery a dynamic 4d phantom , quasar programmable respiratory motion platform ( modus medical devices , ontario , canada ) , was used to verify the uncertainties of epid tracking . 
1 grammable respiratory motion phantom ( modus medical devices , ontario , canada ) with b cedar lung insert in which an offset polystyrene target 3 cm diameter is embedded 184 strahlenther onkol ( 2020 ) 196 : 182192 fig . 
a sinusoidal curve with amplitude of 2 cm and 5 s per breathing cycle , b a natural respiratory curve with amplitude of 1.3 cm and 5 s per breathing cycle more than 2 cm is relatively unusual [ 29 ]  . 
the rst phase was by applying a sinusoidal pattern with peak amplitude of 20 , 10 , 5 , and 0 mthe period for breathing cycle was constant for all amplitudes . 
4dct imaging was used to generate itv and in accordance with the rtog 0915 protocol , the planning target volume ( ptv ) was then created by expanding a uniformly isotropic 3 mm margin from the itv . 3dcrt , sliding - window imrt , and volumetric - modulated arc therapy ( vmat ) plans were created in each breathing cycle for each ct slice thickness . 
all plans were generated with a 10 - mv attening lter - free ( fff ) beam using a dose rate of 2400 mu / mthree - eld 3dcrt plans with gantry angles of 0 , 240 , and 280 , also for imrt a three - eld plan with 230 , 270 , 330 angles , were generated . 
during ct simulation , patients were immobilized with the bluebag bodyfix cushions ( elekta , stockholm , sweden ) vacuum systethe gross tumor volume was determined for lung lesions using the lung and for liver lesions using the soft tissue window , as described in the international commission on radiation units and measurements report 91 [ 30 ]  . 
the german society of radiation oncology ( degro ) guideline recommends contrast - enhanced ct scans or , ideally , contrastenhanced magnetic resonance imaging ( mri ) to dene target volumes in liver lesions [ 31 ]  . 
all patients underwent either four - dimensional ct ( 4dct ; n = 10 ) or 4d positronemission tomography - ct ( pet - ct ; n = 42 ) to quantify respiratory motion and to delineate the internal target volume ( itv )  . 
prior to each fraction , patients were localized with free - breathing cone beam ct ( fbcbct ) and registered with the free - breathing planning ct ( average 4dct )  . 
a pre - treatment verication was performed for all patients treatment plans according to clinical routine , with a 2d - array ( imrt matrixx , iba dosimetry )  . 
epid response was scaled such that one calibrated unit corresponds to 100 mu delivered by a 10 10 cm2 open eld at 100 cm ssd . calibration validation was done in weekly routine . 
when the dose feedback difference was larger than 2% , a new calibration was carried out . in order to evaluate epid sensitivity and specicity in detecting interand intra - fractional motions , patient - related errors were simulated on the phantointentional errors were introduced by shifting the target during treatment delivery . 
the introduced shifts were either larger or smaller than the movestrahlenther onkol ( 2020 ) 196 : 182192 ment of the target in the baseline ( no error ) plan . 
epid images were acquired for all baseline plans and error - introduced plans per individual arc / eld ( a total of 162 ) in each fraction . the clinical workow for patients who underwent verication varied minimally from regular patients . 
during the treatment , the epid was set to acquire . epid image analysis to incorporate the effect of inter - setup and target motion , each fraction was delivered after introducing the inter - target motion . 
epid images from the baseline plan for the phantom study as well as the image from the rst treatment fraction of the patient study were used as reference images . the clinical impact of the errors was analyzed with dedicated ariatm portal vision software within the eclipsetm treatment planning system ( version 15.5 , varian medial systems , usa )  . 
the gamma - index method quantitatively evaluates the similarity of two dose distributions , point by point , using dose differences ( dd ) combined with distance - to - agreements ( dta ) and the gamma criterion . 
in order to assess the effects of the modications , local and improved gamma passing rates ( %gp ) between the no - error and error - simulated measurements were evaluated . 
according to the varian portal dosimetry ( pd ) reference guide , this sampling limitation may result in overestimation of the gamma value at the evaluation point . therefore , the improved option allows the evaluation to interpolate between neighboring points . 
for all criteria , three approaches to dene the region of interest were employed : eld , mlc complete irradiation area outline ( ciao ) + 1 cm and mlc - ciao + 1 cm with a threshold of 5% of maximum dose . 
mlc - ciao + 1 cm corresponds to the opening envelope of the mlc incremented by 1 cm . the regions with doses higher than 5% of the maximum dose ( low - dose threshold ) and the area of mlc - ciao were included to investigate the inuence of low doses on the gamma parameters . 
the nonparametric statistical friedman two - way analysis of variance by ranks was used to evaluate the data . results a small tumor volume ( ctv : 3.26 cm3 , ptv : 5.37 cm3 ) was purposely chosen for phantom measurements to evaluate the feasibility of epid - based real - time transit dosimetry for small elds . to estimate the dose distribution in the target volume for baseline plans , the phantom was irradiated in 18 fractions . 
each irradiation modality included motion simulation ( 20 , 10 , 10 , 20 mm ) in the si direction , normal breathing rhythm , and a static reference condition . 
the results were evaluated in terms of gamma index ( 3% / 3 mm , 2% / 2 mm , 1% / 1 mm ) , which is calculated using spatial and dosimetric limits of dta and dose difference . 
3% / 3 mm criteria with strahlenther onkol ( 2020 ) 196 : 182192 mlc - ciao + 1 cm threshold 5% showed a slightly lower pass rate in 3dcrt plans but not signicant enough to discriminate errors . 
the rather loose criteria could not detect any induced intentional errors by imrt plans . the improved gamma pass rate of 95% with 2% / 2 mm considering mlc - ciao + 1 cm ( threshold 5% ) criteria could manifests changes for each introduced - error measurements in imrt technique . table 3 presents the median improved / local gamma pass rates for epid measurements in vmat plans . 
by varying the analysis protocol from 1% / 1 mm / improved to 1% / 1 mm / local and considering the tighter area of mlc - ciao + 1 cm ( threshold 5% ) , the error detection sensitivity of epid could be signicant . 
for example , if non - stringent gamma criteria are used ( as reported in tables 2 and 3 ) , treatment plans would pass the gamma evaluation even though target displacement was added up to 2 cm in maximufig . 
4 represents the comparison of epid - measured images between the rst fraction and one table 3 the results indicate the fractions median pass rate under different gamma criteria in vmat . 
4 comparison of epid - measured planar dose distribution showing gamma evaluation results ( b , e ) between two different fractions ( a , c ) and line prole agreement ( d ) for an arc of vmat technique of the other fractions by applying motion - simulated errors for the vmat technique . patient irradiations were analyzed using 467 portal dosimetry images applying the roi methods to every treatment eld . 
signicant 190 strahlenther onkol ( 2020 ) 196 : 182192 the mlc - ciao + 1 cm was used instead of the eld and more signicantly for mlc - ciao + 1 cm ( threshold 5% )  . there were noticeable changes in sensitivity for the 2% / 2 mm criterion by using mlc - ciao + 1 cm ( threshold 5% ) and a more signicant reduction with 1% / 1 mm . neither asymptotic signicant nor exact signicant differences were found between all irradiated fractions and plans ( table 5 )  . 
statistical analysis showed that p - values for all comparisons , amongst three sets of dta and dd as well as amongst sub - divisions of each criterion , are less than 0.001. discussion in this study , we presented and assessed a relatively simple method for online verication of lung sbrt treatment . a rapid real - time transit dosimetry approach was investigated , which obtains information from epid image data . exit uence variation due to patient intraand inter - fractional anatomy changes were quantied using quasar phantothe aim was to investigate the accuracy of synchronization of measured image sets during treatment deliveries , check prediction model accuracy for transit patient images using integrated image evaluation , check the initial results for patient treatment verication , and determine the challenges to clinical adoption of real - time transit epid dosimetry systems . this method is straightforward to perform and does not need any implementation of sophisticated analytical or epid modelling approaches . 
gamma index analysis has been commonly implemented as an efcient tool in clinical routine [ 32 , 33 ]  . thereby , it is essential to understand the limitations and sensitivity of the gamma method and the epid . 
the results concern the detection threshold of simulated errors . in general , even if the epid was designed for imaging , it was able to quantify errors when using tighter gamma tolerance than 3% / 3 mour results showed that the use of a combination of criteria might provide an effective way of improving the overall sensitivity of epid . 
the results obtained in 3dcrt revealed that the 2% / 2 mm criterion for any roi in both local and improved normalization had sensitivity to any delivered inaccuracies . the prevention of errors and the delivery of high - quality radiation treatments are basic principles in radiotherapy departments . 
a further study from the netherlands cancer institute disclosed that 9 out of 17 serious errors recognized in 4337 patients would have been missed without in vivo verication of radiation delivery [ 23 ]  . 
in the near future , the authors aim to reconstruct the epid images with precise algorithms and provide 3d dose distribution , which can be compared with the planned dose . 
some recent works have enabled measured images by back - projecting to planes or volumes within the patient , so the dose inside the patient can be reconstructed in 2d [ 40 ]  . we observed that the changes in dose distribution could be recognized in small tumors ( less than 5 cm ) by tighter gamma evaluation , which were combined with roi criteria . consequently , local gamma evaluation should be considered for the vmat technique to provide an effective way of improving the overall sensitivity of epid . in vivo dosimetry has been recognized as one of the next milestones in radiation oncology . 
we developed a patient rapid real - time transit dosimetry method with epid , which is validated for hypofractionated treatments with fff beams , as a step toward epid in vivo dosimetry . 
by increasing the use of sbrt combined with substantial dose deliveries in 1 to 5 fractions as well as the biological responses of tumor to radiation , there is a high need for monitoring systems and detecting treatment delivery errors . 
the commonly used criterion of 3% / 3 mm was inadequate for discovering target motion errors . further work is required to develop a real - time verication system which provides an additional tool that can assist with the prevention of signicant mistreatments in radiation therapy . 
obviously , in vivo dosimetry improves the potential of detecting delivery errors , but it is still limited in its capacity to prevent errors before clinically signicant errors occur [ 42 ]  . conclusion this study demonstrates the feasibility of epid for detecting the interplay effects . 
thus , the approach / prototype provides a fast and easy qa procedure for treatment delivery verication . new software generations will allow reconstruction of the dose inside the patient and , if errors are found , will analyze their clinical relevance . 
november 2019 springer - verlag gmbh germany , part of springer nature 2019 hintergrund trotz multimodaler therapie ist die prognose des lokal fortgeschrittenen nicht - kleinzelligen bronchialkarzinoms ( nsclc ) schlecht : das 5 - jahres - berleben erreicht auch in prospektiven studien mit selektion von jngeren patienten in gutem allgemeinzustand bestenfalls 40 % . 
das berleben wird sowohl durch lokoregionre rezidive als auch durch fernmetastasierung limitiert . material und methoden die pacific - studie [ 1 , 2 ] ist eine internationale randomisierte phase - iii - studie , in der patienten mit inoperablem nsclc im stadium iii nach abgeschlossener radiochemotherapie ( rct ) in einem verhltnis von 2 : 1 zu durvalumab ( 10 mg pro kg krpergewicht , alle 2 wochen , maximal ein jahr ) oder plazebo randomisiert wurden . 
eine plattenepithelhistologie lag bei 46 % vor . das tumorstadium war iiia bei 53 % oder iiib bei 45 % . eine induktionschemotherapie wurde bei 27 % der patienoriginalpublikation antonia sj , villegas a , daniel d et al ( 2018 ) overall survival with durvalumab after chemoradiotherapy in stage iii nsclc . 
nach einer medianen nachbeobachtungszeit von 25 monaten wurde im durvalumab - arm ein signikant verbessertes 2 - jahres - os beobachtet : 66 , 3 % im vergleich zu 55 , 6 % ( hazard ratio [ hr ] 0 , 68 )  . 
grad - 3oder - 4 - nebenwirkungen wurden bei 30 , 5 % im durvalumab - arm und bei 26 , 1 % im kontrollarm beobachtet . schlussfolgerung der autoren eine therapie mit dem pdl1 - antikrper durvalumab nach rct und fehlendem progress fhrt beim inoperablen nsclc im stadium iii zu einer verbesserung des os . kommentar endlich ! jahrzehntelange war die klinische forschung beim lokal fortgeschrittenen nsclc durch stagnation und frustration charakterisiert . 
eskalation der bestrahlungsdosis [ 3 ] , egfr - inhibition durch cetuximab [ 3 ] , radiotherapie zustzlich zur chemotherapie und operation [ 4 ] und operation zustzlich zur rct [ 5 ] konnten in randomisierten studien keine verbesserung des berlebens erreichen , so dass die cisplatin - basierte rct in konventioneller fraktionierung und mit standarddosis bis heute der therapiestandard war . pacific prfte nun als erste und bisher einzige studie die kombination aus radiotherapie , chemotherapie und immuntherapie . 
durvalumab sollte heute allen patienten nach abgeschlossener rct und fehlendem progress angeboten werden . strahlenther onkol ( 2020 ) 196 : 9597 klinische relevanz eine simultane statt sequentielle rct verbessert das berleben mit einer hr von nur 0 , 84 [ 6 ] und verfnffacht das risiko fr eine schwere sophagitis . eine adjuvante chemotherapie nach resektion des nsclc verbessert das berleben mit einer hr von 0 , 86 [ 7 ]  . 
im historischen vergleich ist der berlebensvorteil von durvalumab mit einer hr von 0 , 68 daher als quantensprung zu bezeichnen , gerade auch deshalb , weil er ohne zustzliche schwere nebenwirkungen fr die patienten einhergeht . 
und der vorteil scheint sich auch tatschlich in eine verbesserte heilung mit langzeitberlebern zu bertragen , wie die ergebnisse vom asco - kongress 2019 mit einem medianen follow - up von 33 monaten und unverndert separierten berlebenskurven andeuten [ 8 ]  . plausibilitt der vorteil einer zustzlichen immun - checkpoint - inhibition ( ici ) nach rct ist plausibel : eine alleinige immuntherapie ist bei hoher pd - l1 - expression die erstlinientherapie der wahl im metastasierten stadium des nsclc [ 9 ] und in der kombination mit zytotoxischer chemotherapie ist die ici auch bei fehlender oder niedriger pd - l1expression eine erstlinientherapie [ 10 ]  . 
in der pacific - studie ist das verbesserte os somit die konsequenz aus einer reduktion von fernmetastasten , sowohl zerebral als auch extrazerebral , sowie einer reduktion von lokoregionren rezidiven . anwendbarkeit die pacific - studie war in ihrem design pragmatisch , was ( fehlende ) anforderungen an bestrahlungstechnik , bestrahlungsdosis , wahl der platinbasierten chemotherapie und die option einer induktionschemotherapie angeht . 
der nachweis eines fehlenden lokalen oder systemischen progresses nach rct sollte pragmatisch erfolgen , da eine ici in dieser situation in der mehrzahl der nsclc - patienten ohne aktivierende treibermutation eine therapieoption ist . zulassung durvalumab ist entsprechend den einund ausschlusskriterien der pacific - studie zugelassen . 
ein expertenpanel hat diese einschrnkung diskutiert und kritisiert [ 12 ]  . argumente gegen diese einschrnkung sind , dass die analyse der pacific - studie mit einem pd - l1 - cut - off von < 1 % eine ungeplante subgruppenanalyse darstellen wrde , der pd - l1 - status nur bei 63 % der patienten vorhanden war und folglich nur 148 patienten tatschlich einen pdl1 - status von < 1 % hatten . 
hinzu kommt , dass der pd - l1status vor der radiotherapie bestimmt wurde , der vorteil von durvalumab bezglich pfs in allen subgruppen , auch mit pd - l1 < 1 % , ersichtlich war und das os in der patientengruppe mit unbekanntem pd - l1 - status im durvalumabarm ebenfalls verbessert war . 
daher besteht die sorge , dass patienten mit fehlender pd - l1 - expression und insbesondere patienten mit zu wenig gewebe fr die bestimmung der pd - l1 - expression eine effektive und gut vertrgliche therapie vorenthalten wird . gibt es konsequenzen fr die durchfhrung und indikation der rct ? von der pacific - studie wurden patienten ausgeschlossen , wenn eine sequentielle rct durchgefhrt wurde . 
die radiotherapie sollte deshalb moderne techniken verwenden , um akute nebenwirkungen zu minimieren : fdg - pet zur involved - eld - zielvolumendenition , 4d - ct - bildgebung und atembewegungskompensation , intensittsmodulierte und mit cone - beamct gefhrte strahlentherapie [ 13 ]  . 
eine nebenwirkungsarme rct wird darber hinaus einen frhen beginn der durvalumab - therapie ermglichen , was in der subgruppenanalyse der pacific - studie vorteilhaft erscheint . die pacific - studie hat patienten mit lokal fortgeschrittenem nsclc eingeschlossen , die interdisziplinr im lokalen tumorboard als inoperabel eingestuft worden waren . die unscharfe denition einer klinischen und technischen inoperabilitt beim stadium iiia des nsclc ist bekannt [ 14 ] und resultiert in einer hohen internationalen variabilitt . 
randomisierte studien aus der pr - immuntherapiera konnten keine unterschiede zwischen operation und strahlentherapie zeigen , wenn diese lokalen therapien jeweils mit einer chemotherapie kombiniert wurden [ 4 , 5 ]  . 
auch wenn heute in einzelund grenzfllen die entscheidung zwischen operativer und radioonkologischer strategie durch die positiven ergebnisse der pacific - studie beeinusst wird , so kann eine systematische verschiebung aktuell ohne entsprechende klinische studien nicht empfohlen werden . fazit wie lsst sich die radioimmuntherapie weiter optimieren ? aus biologischer sicht durch die kombination aus ici und strahlenther onkol ( 2020 ) 196 : 9597 radiotherapie wenn ( a ) eine doubleund nicht eine singleici [ 15 ] erfolgt , ( b ) die bestrahlung hypofraktioniert und mit hheren einzeldosen durchgefhrt wird [ 16 ] , ( c ) keine bestrahlung der drainierenden lymphabusswege erfolgt [ 17 ] und ( d ) die radioimmuntherapie simultan und nicht sequentiell durchgefhrt wird [ 18 ]  . 
dieser widerspruch kann durch eine schwierige bertragbarkeit von prklinischen ergebnissen in die klinische anwendung , auf ein hohes verbesserungspotenzial der radioimmuntherapie analog pacific , auf eine hohe robustheit der radioimmuntherapie gegen den obigen parameter oder eine kombination der argumente erklrt werden . 
es sind daher weitere studien notwendig und gleichzeitig vielversprechend , um die radioimmuntherapie systematisch zu optimieren [ 19 ]  . zusammenfassend wurde durch die sequentielle rct , gefolgt von einer ici nach jahrzehnten erstmals wieder ein fortschritt in der behandlung des lokal fortgeschrittenen nsclc erzielt . 
bradley jd , paulus r , komaki r et al ( 2015 ) standard - dose versus high - dose conformal radiotherapy with concurrent and consolidation carboplatin plus paclitaxel with or without cetuximab for patients with stage iiia or iiib non - small - cell lung cancer ( rtog 0617 ) : a randomised , two - by - two factorial phase 3 study . 
pless m , stupp r , ris h - b et al ( 2015 ) induction chemoradiation in stage iiia / n2 non - small - cell lung cancer : a phase 3 randomised trial . 
eberhardt wee , pttgen c , gauler tc et al ( 2015 ) phase iii study of surgery versus denitive concurrent chemoradiotherapy boost in patients with resectable stage iiia ( n2 ) and selected iiib nonsmall - cell lung cancer after induction chemotherapy and concurrent chemoradiotherapy ( espatue )  . 
auprin a , le pchoux c , rolland e et al ( 2010 ) meta - analysis of concomitant versus sequential radiochemotherapy in locally advanced nonsmall - cell lung cancer . 
peters s , dafni u , boyer m et al ( 2019 ) position of a panel of international lung cancer experts on the approval decision for use of durvalumab in stage iii non - small - cell lung cancer ( nsclc ) by the committee for medicinal products for human use ( chmp )  . 
de ruysscher d , faivre - finn c , moeller d et al ( 2017 ) european organization for research and treatment of cancer ( eortc ) recommendations for planning and delivery of high - dose , high precision radiotherapy for lung cancer . 
postmus pe , kerr km , oudkerk m et al ( 2017 ) early and locally advanced non - small - cell lung cancer ( nsclc ) : esmo clinical practice guidelines for diagnosis , treatment and follow - up . 
hsiao6 received : 8 november 2018 / accepted : 29 march 2019 / published online : 26 april 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose the current study aimed to assess patterns of failure ( pof ) in anaplastic glioma ( ag ) patients managed with intensity - modulated radiation therapy ( imrt ) and their relationship to molecular subtype . methods the outcomes of ag patients managed between 2008 and 2014 and entered into a prospective database were assessed , including pof . 
ag was initially dened using the who 2007 classication , but for analysis , patients were subsequently recategorised based on who 2016 as anaplastic oligodendroglioma ( aod ) , astrocytoma isocitrate dehydrogenase ( idh ) mutant ( aamut ) or astrocytoma idh wildtype ( aawt )  . 
management involved imrt and temozolomide ( tmz ) , including from 2011 patients with an idh mutation ( idhmut ) planned with 18f - uoroethyltyrosine ( fet ) and 18f - uorodeoxyglucose ( fdg ) positron - emission tomography ( pet )  . 
fr diese studie wurden die patienten nach who 2016 als anaplastisches oligodendrogliom ( aod ) , astrozytom mit isocitrat - dehydrogenase - ( idh - ) mutation ( aamut ) oder wildtyp - astrozytom ( aawt ) rekategorisiert . 
die behandlung bestand aus imrt und temozolomid ( tmz ) , wobei seit 2011 fr patienten mit idh - mutationen ( idhmut ) eine 18f - fluoroethyltyrosin ( fet ) und eine 18f - fluorodeoxyglukose - ( fdg - ) positronenemissionstomographie ( pet ) teil des planungsprozesses waren . 
ein rezidiv mit einer 6 - jahres - rfs von jeweils 75 , 0 % , 48 , 8 % und 2 , 5 % fr aod , aamut and aawt entwickelten 68 % ( p < 0 , 001 )  . es bestand eine komponente fr ein lokales rezidiv in 68 % , fr ein marginales rezidiv in 19 % und fr ein entferntes rezidiv in 37 % der flle . 
in der multivariaten analyse blieb die assoziation zwischen fernrezidiv und aamut ( p < 0 , 002 ) und bis zum zweiten rezidiv verzgerter imrt ( p < 0 , 001 ) bestehen . schlussfolgerung obwohl patienten mit idh - mutiertem ag bessere ergebnisse erzielen , gab es einen relativ hohen fernrezidivanteil innerhalb der ersten beiden jahre seit imrt . schlsselwrter isocitrat - dehydrogenase rckfall strahlentherapie temozolomid berleben recent improvements in molecular classication of highgrade gliomas have identied a favourable subset of anaplastic glioma tumours harbouring mutations in the isocitrate dehydrogenase genes idh1 and idh2 , which have been shown to be associated with a median survival beyond 1015 years when managed with combined modality therapy comprising limited surgery , radiation therapy and chemotherapy [ 13 ]  . although they have a favourable prognosis , these tumours may often be quite extensive at initial presentation , with mri demonstrating widespread t2 - weighted uid - attenuated inversion recovery ( t2 flair ) change surrounding the initial t1 dense or enhancing mass [ 4 ]  . 
technological improvements in diagnostic imaging , nuclear medicine and radiation therapy can potentially deliver a more targeted dose of radiation to the tumour and spare normal brain tissue [ 57 ]  . 
awareness of the relapse pattern may also inuence the design of future treatment protocols , including the initial radiation therapy volumes that are used . whilst the patterns of relapse and salvage in glioblastoma patients are well documented [ 8 , 9 ] , there is a paucity of data describing relapse patterns in the large clinical trials commenced in the 1990s that demonstrated the durable survival in the group of patients with favourable ag [ 2 ]  . this study audits the early patterns of relapse in anaplastic glioma patients , with a specic comparison based on the idh1 / 2 mutation . methods consecutive adult patients diagnosed with anaplastic glioma were entered into a prospective database , as approved by the institutional ethics review board . 
these patients were formally managed with denitive intensitymodulated radiation therapy ( imrt ) by one clinician over a 7 - year period between january 2008 and december 2014 . post - treatment mri surveillance was protocolised and patterns of relapse were recorded in relation to the initial tumour site and radiation therapy dose distribution . patient selection patients eligible for the anaplastic glioma database were newly diagnosed or rt - naive relapsed patients managed with imrt . 
an anaplastic glioma was dened as a pathological diagnosis corresponding to the world health organization ( who ) 2007 criteria as a grade iii pathology [ 10 ] or patients with a known who 2007 grade ii pathology from prior diagnosis but with recent radiological or metabolic progression consistent with anaplastic change . the latter group included evidence of new gadolinium enhancement on mri , sequential mri t1 progression within a 6 - month period or new uorodeoxyglucose ( fdg ) uptake within a known grade ii glioma on fdg positron - emission tomography ( pet )  . strahlenther onkol ( 2020 ) 196 : 3139 pathological subgroup classication histopathological classication was initially recorded as anaplastic astrocytoma ( aa ) , anaplastic oligoastrocytoma ( aoa ) or anaplastic oligodendroglioma ( aod ) , based on the who 2007 classication [ 10 ]  . 
molecular factors such as 1p19q codeletion , idh1 / 2 mutation status ( evaluated by immunohistochemical and protein sequencing techniques ) and atrx mutation status were recorded where available . the availability of these results varied over the years of the database , as new molecular pathology techniques were sequentially introduced into clinical practice . with the introduction of the who 2016 classication , patients were subsequently recategorised according to the presence of an idh1 / 2 mutation , including historical patients who were tested later [ 11 ]  . 
patients with anaplastic glioma pathologies other than aa or aod were included as a separate subgroup ( oth )  . radiological procedures gadolinium - enhanced 3t mri was the principal diagnostic procedure at initial diagnosis and rt planning . 
the lower - dose region ( gtv54 ) included this volume as well as that dened by t2 - flair and fet uptake outside of this volume [ 5 ]  . 
the addition of adjuvant tmz commenced in early 2012 , following release of long - term results of the radiation therapy oncology group ( rtog ) and european organization for research and treatment of cancer ( eortc ) studies showing improved median survival for patients with oligodendroglial tumours receiving adjuvant procarbazine , lomustine and vincristine ( pcv ) chemotherapy [ 12 , 13 ]  . 
in the clinical trial the duration of adjuvant tmz was 12 months , whilst off - trial a 6 - month duration was offered . no pcv was offered during this study period . post - treatment surveillance patients were evaluated at 1 month post - imrt with mri , and then commenced a surveillance programme with generally 3 monthly mri for years 12 , then 4 monthly in year 3 followed by 6 monthly until year 5 . endpoints relapse - free survival strahlenther onkol ( 2020 ) 196 : 3139 table 1 patient and treatment characteristics subgroup all patients ( % ; n = 156 ) relapse - free survival ( rfs ) was calculated from the date of commencement of imrt to either the date of death or censure of data on december 31 , 2017 . 
within 18 months of completion of imrt , in which uncertainty existed regarding whether the mri changes were related to the tumour or treatment effect , sequential mris were used to conrm diagnosis , but the date of relapse was taken from the initial mri if subsequently conrmed . 
similarly , patients with asymptomatic small - volume ventricular enhancement were not immediately classied as recurrent disease unless there was a 50% increase persisting for a period of 6 months . 
this was to exclude a late periventricular radiation treatment effect presumed to be low - grade inammation or focal demyelination [ 15 ]  . site of relapse the relapse site was categorized in relation to the imrt - dened gtv ( gtv59.4 or gtv54 if imrtib ) and dened as : local ( > 50% within gtv59.4 / 54 ) ; marginal ( > 50% within 20 mm of gtv59.4 / 54 ) ; distant ( > 50% beyond 20 mm from gtv59.4 / 54 ) ; or combined ( synchronous sites of relapse )  . additionally , involvement of the ventricular system was reported if a distant relapse was evident . statistical considerations all patients had clinical and dosimetric data entered into an excel ( microsoft , redmond , wa , usa ) database , which was regularly updated for outcome events . 
baseline patient characteristics are detailed in table 1 . an initial approach involving rt avoidance was applied in the management of 44% of patients , with 26% being managed at rst relapse and 18% at second or later relapse . overall , 33% had two or more craniotomies prior to referral for rt . 
of the cohort , 118 patients ( 75% ) had an idh - mutated glioma , with 61 and 57 patients with aod and aamut , respectively ; whilst 30 ( 19% ) were aawt . 
the remaining 8 patients had oth pathologies with anaplastic change ; 6 being classied as neuronal or mixed neuronal / glial tumours . with regard to management , 80% of patients had a craniotomy immediately prior to imrt , whilst the remainder were managed after presumed higher - grade radiological progression determined by mri or pet imaging . radiologically evident gross residual disease was present in 74% of patients prior to imrt . 
this was predominantly non - enhancing , with only 26% having gross enhancement ( dened as > 10 mm ) on preoperative or pretreatment imaging ; and 22% of patients had > 50 mm residual disease . 
in relation to the who 2016 pathological classication , residual disease was evident in 84% of patients with aawt , compared with 74% of patients with aod or aamut and 50% of oth . imrt was delivered as planned in all patients . 
in the oth subgroup of 8 patients there was only one relapse . for the univariate analysis to determine factors associated with rfs , only tumours with idh - wildtype molecular status predicted greater relapse compared to idh - mutated or other glial tumours . 
3 , the ratio of distant to local failures altered over early to later follow - up . idhwt tumours had a predominant early relapse pattern which was mainly local failure . 
both , aamut and aod had a higher proportion of distant failure in the rst 2 years , with local relapses occurring later , usually after 4 years . factors associated with relapse pattern for patients with an idh1 / 2 mutation the 118 patients with tumours harbouring an idh1 / 2 mutation were analysed as to the pattern of failure and timing of failure . 
there was no difference in local relapse between the two subgroups with an idh1 / 2 mutation . other factors were examined for their ability to predict local or distant relapse in this cohort of idh - mutated tumours ( table 3 )  . 
however , 14 patients had a pseudoprogression or necrosis event , with a more than 25% increase in enhancement occurring during the 3 years after imrt that did not proceed to conrmed relapse . 
of these cases , 3 patients required surgical debulking with pathology conrming necrosis , whilst 2 patients required management with bevacizumab . strahlenther onkol ( 2020 ) 196 : 3139 overall survival following relapse for the whole study cohort of 156 patients , there were 52 deaths at the time of data censure and a 6 - year os estimate of 62.3%. 
this includes 44% of patients who had denitive management delayed until rst or subsequent relapse . however , within this favourable subgroup , the patients who do relapse early ( nominally within the rst 2 years after imrt ) demonstrate an unusual pattern of tumour progression , with predominantly distant sites of relapse , often involving ventricular sites . 
there is effective tumour control within the local region irradiated , but later progression as multifocal deposits in distant regions of the brain or extending along the ventricular wall with subependymal spread of tumour . 
this then subsequently predicts for poor salvage , with only a 12 - month median survival after radiological evidence of progression . the pof in this favourable group differs from the patients with anaplastic glioma without an idh1 / 2 mutation , whose relapse pattern parallels glioblastoma relapse , with predominantly local failure that occurs earlier and within the initial involved region of the brain and the high - dose radiation region [ 8 , 9 ]  . whilst there are limitations of this retrospective analysis regarding generalisability of outcome from this patient cohort , the pof should be a focus for validation and further exploration . 
this may be further improved by assessing the relationship of relapse to the actual radiation therapy dose levels , rather than to the initial tumour target volume as performed in this study . there is a paucity of data describing the pof in this favourable subgroup from the historical reported series . 
exploring the data from patients managed in eortc 26951 with combined therapy shows 3 - year progression rates of approximately 20 and 65% in codeleted and non - codeleted tumours , respectively , which correlates with a 3 - year death rate of 15 and 60% in the same patient subgroups [ 13 ]  . 
this may not reect any altered pof induced by surgical dissemination of tumour , but rather simply reect a longer natural history of malignant transformation prior to eventual denitive management . over the course of this study , the protocols for systemic therapy changed and may not be consistent with current guidelines . 
the analysis demonstrated no impact on rfs or pof related to use of systemic therapy ; however , this may be related to the selection factors for systemic therapy changing in the current study . 
prior to publication of the rtog and eortc studies in 2012 , which outlined the long - term outcome benet of addition of systemic therapy in aod [ 12 , 13 ] , chemotherapy was not offered . 
however , given the continued local control in years 35 , there would have been further distant failures expected in these latter years ; but the rate of distant failure actually plateaus . 
an additional interpretation of this data may be that within this favourable subgroup of idh - mutated glioma , there may be a further smaller subgroup that harbours other mutations or molecular drivers which predict for more inltration along subependymal or ventricular pathways ; or perhaps that there may be another aggressive phenotype that is radiation sensitive but inltrative recurrence occurs outside of the high - dose rt portals . analysing progression - free survival curves in other larger series of patients with anaplastic glioma and an idh1 / 2 mutation reveals an incidence of initial early relapse that would not be expected in patients with this relatively radiation responsive tumour subgroup [ 16 ]  . 
identifying the patients with a possible aggressive phenotype and searching for other molecular drivers with genetic sequencing is a source of future study in our current patient series . it is important to note that in the current series , the majority of patients had a large residual tumour bulk with evidence of inltrative t2 - flair change . 
exploring improved diagnostic techniques with mri or amino acid pet in such patients to determine the presence of early inltrative disease will minimise any risks of geographical miss with imrt [ 7 , 17 ]  . 
in the cohort managed with fet / pet - guided planning there was good ineld control and no marginal relapse , but still distant failures , suggesting that the diagnostic techniques need to be further optimised . 
a greater impact of these imaging procedures may possibly be observed in the patients managed by a practice of deferred radiation management of diffuse low - grade glioma until malignant transformation . 
these patients were often referred with bulky and progressive t2 - flair changes , and earlier recognition may impact on outcome . with radiological follow - up of patients , it is important to recognise the potential late and usually asymptomatic radiation - related appearances that occur on mri imaging , especially with more frequent and better mri sequences [ 18 ]  . 
potential late rt - related demyelination , evident on mri imaging , may present as focal areas of contrast enhancement at adjacent periventricular sites and could be misdiagnosed as relapse . 
in this study , such episodes were strahlenther onkol ( 2020 ) 196 : 3139 determined not to be related to recurrent disease by utilising sequential mri scans to conrm a lack of progression or regression over a 6 - month period without intervention . conclusion based on the analysis of outcomes in this patient group with anaplastic glioma , an association of molecular pathology was noted not only with rfs , but also with the pof and timing of relapse . 
the early distant relapse pattern occurring in selected patients with an idh - mutated tumour , particularly in the subgroup of aamut , should be further validated and made a focus of further research . compliance with ethical guidelines conict of interest m . 
combs1 , 2 , 3 received : 31 july 2019 / accepted : 23 october 2019 / published online : 13 november 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose lymph node irradiation in breast cancer has gained complexity due to recently published studies and technical innovations which then led to changes in international guidelines . 
we sought to determine real - time variability in lymph node irradiation in clinical practice in german - speaking countries . methods the department of radiation oncology , technical university of munich ( tum ) , developed an online - based questionnaire focusing on the indication , target denition , and treatment technique of lymph node irradiation in patients with breast cancer . 
the results of the survey were exported from the online platform into spss for a detailed analysis . results in total , 100 physicians completed the questionnaire between 05 / 2019 and 06 / 2019 . 
despite the existence of several treatment and contouring guidelines , we observed large variability of lymph node irradiation : the guideline recommendation for internal mammary irradiation is not consistently implemented in clinical practice and irradiation of the axilla after positive slnb ( sentinel lymph node biopsy ) or alnd ( axillary lymph node dissection ) is handled very differently . 
furthermore , in most clinics , the estro ( european society for therapeutic radiology and oncology ) contouring consensus is not used , and ptv ( planning target volume ) denitions and margins vary considerably . conclusion further clinical studies should be performed with a particular focus on radiotherapy for lymphatic drainage to support and amend the existing guidelines . 
quality assurance should enforce broad implementation of consensus recommendations . keywords lymph node irradiation breast cancer variability patterns of care survey introduction lymph node irradiation is a crucial component in the adjuvant treatment of high - risk breast cancer patients . 
according to these studies , rni ( including the supra - / infraclavicular and the internal mammary region as well as parts of the axilla ) leads to better regional control rates as well as better distant metastases - free survival and disease - specic survival in high - risk patients [ 13 ]  . 
this has changed over the past 5 years based on the excellent results of the two randomized studies and a prospective population cohort study from denmark showing a survival benet for imi in addition to strahlenther onkol ( 2020 ) 196 : 1522 supra - / infraclavicular irradiation ( sii ) [ 1 , 2 , 5 ]  . 
so far , it is unclear whether the recommendations to include the internal mammary region in rni are implemented in clinical practice . another crucial point that has been altered in recent years in the guidelines is the treatment of the axilla . 
the 10 - year data of the z0011 conrm that complete alnd may be omitted in breast cancer patients in case of positive ( ( cid : 2 ) 2 ) sentinel lymph nodes without compromising locoregional control or survival [ 6 ]  . 
the current ago ( arbeitsgemeinschaft gynkologische onkologie ) guideline ( 2019 ) is the rst to recommend irradiation of the axilla up to the axillary veins , since a large number of patients in the z0011 study received high tangential external beam irradiation [ 7 ]  . interpreting the existing data and translating the results into daily clinical practice is challenging . 
most of the randomized studies were initiated in the 2d era , and technical improvements such as 3d - planning , intensity - modulated radiotherapy ( imrt ) , and image - guided radiotherapy ( igrt ) have fundamentally changed treatment since then . comprehensive treatment guidelines and contouring atlases for breast cancer have been published [ 711 ]  . 
the aim of the current study was to reveal aspects in rni that need increased efforts in continuing medical education or clarication in future studies and scientic discussions . methods a pattern - of - care questionnaire regarding rni in breast cancer was developed at the department of radiation oncology at the technical university of munich ( tum )  . 
the questionnaire was implemented in the online platform survio.com and the corresponding link was sent via e - mail to all members of the german society of radiation oncology ( degro )  . 
the data obtained on the online platform was exported to spss ( ibm statistics , version 25 , armonk , ny , usa ) and analyzed . results in total , 100 questionnaires were completed at the online platforthe majority of participants ( 92.9% ) were specialists in radiation oncology ; the remaining participants ( 7.1% ) were residents in radiation oncology . 
the current study represents at least 52 centers out of ( approximately ) 455 centers in germany [ 12 ]  . indication for lymph node irradiation when the participants were asked for their primary aim of rni , the most frequent answer was to prevent regional lymph node recurrences ( n = 84 ) , followed by improvement of overall and / or disease - specic survival ( n = 75 ) and reduction of distant metastases ( n = 54 )  . the questionnaire listed potential reasons for sii , and the participants were asked in which situation they would perform sii . 
the majority of participants perform sii in case of positive supra - / infraclavicular lymph nodes ( 85% ) , 4 positive lymph nodes ( 85% ) , or in case of 13 positive nodes and additional risk factors ( 75% )  . for most radiation oncologists , rni does not regularly comprise sii and irradiation of the internal mammary region ( imi )  . 
only 9% saw the technical requirements and the time effort as an obstacle for imi . current guidelines ( ago 2019 ) advise against imi in case of cardiac risk and concomitant administration of trastuzumab . 
the most commonly used contouring guideline is the rtog ( radiation therapy oncology group ) consensus guideline ( 71% ) followed by the estro ( european society for therapeutic radiology and oncology ) consensus guideline ( 25% )  . 
86% agreed that the axillary level iii should be included in the supra - / infraclavicular ctv ( clinical target volume ) and 31% include in addition to this also level ii in the clinical target volume for sii . further results regarding the target delineation were : 1 . 
the techniques used for imi and sii are summarized in table 1 . image guidance for lymph node irradiation is performed with either 2d x - rays ( 44% ) , cbcts ( conebeam computed tomography ) ( 47% ) , mvct ( megavoltage computed tomography ) ( 9% ) , or surface scanners ( 9% )  . 
2d strahlenther onkol ( 2020 ) 196 : 1522 x - rays , cbct , and mvct are mostly performed once a week ; surface scanners are often used daily ( 75% )  . discussion we performed a survey among german - speaking radiation oncologists who are members of degro regarding indications for rni , target volume denition , and choice of technique in patients with breast cancer . 
based on these results , the nccn ( national comprehensive cancer network ) guidelines recommend irradiation of infraclavicular and supraclavicular areas , internal mammary nodes , and any part of the axillary bed that may be suspicious in case of 4 positive nodes ( category 1 ) and 13 positive nodes ( category 2a )  . 
the german guidelines ( s3 , ago , degro practical guidelines ) differ from the nccn guidelines in several points regarding rni [ 7 , 10 , 13 , 14 ]  . 
due to the design of these trials it is not possible to attribute the positive effect on subvolumes within the lymphatic drainage system ( e.g. , contribution of imi )  . 
a randomized french trial on the other hand failed to show a signicant benet for addition imi during postmastectomy irradiation [ 15 , 16 ]  . the nccn guidelines state that imi should be strongly considered when delivering regional nodal irradiation . 
in addition to this , many physicians doubt an additional effect if imi is performed . since the rationale for rni is mainly based on the results of the ma.20 and eortc studies and modern treatment techniques ( deep - inhalation breath - hold , wide tangents , imrt ) allow better sparing of organs at risk ( oars ) compared to these randomized trials , the guideline recommendations to include the internal mammary region are comprehensible and omission of imi should be limited to individual cases . the german guidelines cite cardiac risk and concomitant trastuzumab as reasons against imi . 
as shown in our results , the interpretation of cardiac risk factors in clinical practice is very different , and not all radiation oncologists agree that imi plus concomitant trastuzumab should be avoided . 
instead of using strict contraindications , it might be helpful to assess the actual dose distribution in the oars resulting from imi using the best available technique ( e.g. , deep inhalation breath hold [ dibh ] )  . 
even if the authors state that exceeding these constraints may be unavoidable and justiable in case of comprehensive regional irradiation , the values can help to dene constraints for rni . in case of positive slnb without alnd , 30% of radiation oncologists participating in the questionnaire would always treat the axilla and another 30% only if the z0011 strahlenther onkol ( 2020 ) 196 : 1522 criteria are not met . 
given the fact that most patients in the z0011 received high doses in the ( lower ) axillary levels iii , irradiation might be justied even if the z0011 criteria are met [ 18 ]  . 
according to the german guideline , irradiation of the axilla after alnd is only indicated in case of suspected residual tumor after axillary dissection [ 7 , 9 , 10 ]  . 
even though not recommended in the current german guidelines , one quarter of the participants treat the axilla in case of > 3 ln or < 10 dissected lymph nodes . 
this is supported by the nccn guidelines stating that irradiation of any part of the axillary bed at risk is recommended [ 9 ]  . target denition is a crucial step in 3d radiotherapy . 
this has an impact on the effectivity and the toxicity of the treatment . differences regarding target volume denition among the randomized rni trials impede interpretation of the study results [ 13 , 19 ]  . 
the estro contouring consensus [ 20 ] was published in 2015 . it represents a vessel - based approach that results in smaller target volumes compared to the rtog ( 2009 ) contouring guideline . 
nevertheless , only 25% of the participants use this contouring guideline in clinical practice . even if the ctvs are dened based on the same contouring guidelines , target volumes can vary due to different safety margins and denition of the lymph node areas ( e.g. , of the infraclavicular region )  . 
considering that the intrafractional movement of the internal mammary region can be up to 5 mm , this may be critical , and careful image guidance should be performed to verify the patient position [ 24 ]  . daily imaging improves patient positioning but usually comes at the price of additional radiation ( x - ray or ct imaging )  . 
however , this technique is only available in a few centers to date . the vast majority of participants use normofractionated schemes for irradiation of the lymph node systethis represents the current consensus of the american and german guidelines [ 7 , 9 , 10 ]  . 
recently published a randomized trial showing that postmastectomy hypofractionated radiotherapy , including rni , is non - inferior and had similar toxicities compared to conventionally fractionated radiotherapy [ 26 ]  . for irradiation of the lymph node system , imrt and vmat ( volumetric modulated arc therapy ) are the most frequently used techniques in german - speaking countries . still , 45% ( 18% ) of the participants use also anterior photon elds for the supra - / infraclavicular ( or the internal mammary ) region . 
thus , it might be a good option for centers in which imrt is not available for irradiation of the internal mammary region [ 27 ]  . conclusion as consequence of numerous treatment and contouring guidelines for breast cancer treatment , we observed large variability in rni . 
the current guideline recommendations ( s3 , ago , nccn ) for imi are not implemented adequately in clinical practice and irradiation of the axilla after positive slnb or alnd remains controversial . 
november 2019 springer - verlag gmbh germany , part of springer nature 2019 hintergrund leberchirurgische eingriffe werden bei primren und sekundren lebertumoren hug durchgefhrt . die datengrundlage besteht in aller regel aus wenigen prospektiven studien und selektionierten kohorten aus groen zentren . 
ber die ergebnisse in der breiten klinischen praxis ist bislang wenig bekannt . patienten und methode es wurde eine analyse der entlassdaten aus dem krankenhaus aus der datenbank des statistischen bundesamts von 20102015 durchgefhrt . 
3 , haus l , 24105 kiel , deutschland tagestherapiezentrum , interdisziplinres tumorzentrum , universittsmedizin mannheim , medizinische fakultt mannheim , ruprecht - karls - universitt heidelberg , mannheim , deutschland 3 klinik fr strahlenheilkunde , universittsklinikum freiburg , freiburg im breisgau , deutschland 4 klinik fr strahlentherapie , universittsklinikum magdeburg , magdeburg , deutschland 5 klinik fr strahlentherapie und radioonkologie , universittsmedizin mannheim , medizinische fakultt mannheim , ruprecht - karls - universitt heidelberg , mannheim , deutschland ergebnisse in die analyse gingen daten von 110.332 patienten ehiervon wurden ca . 
75 % aufgrund einer tumorerkrankung operiert , hierunter 48.882 patienten mit lebermetastasen eines kolorektalen karzinoms ( mcrc ) , 8364 patienten mit hepatozellulrem karzinom ( hcc ) und 4667 patienten mit intrahepatischem cholangiokarzinom ( icc )  . 
verglichen mit patienten im alter < 50 jahre ( n = 15.704 ; sterblichkeit 2 , 2 % ) war das sterblichkeitsrisiko fr patienten von 5069 jahren ( n = 49.966 ; 4 , 3 % ) bzw . 
groe eingriffe mit der notwendigkeit einer biliodigestiven anastomose ( 1831 % ) , simultaner darm ( 16 , 3 % ) , magen ( 26 , 8 % ) oder pankreasresektion ( 27 , 2 % ) gingen erwartungsgem ebenfalls mit einer deutlich erhhten mortalitt einher . 
ein drittel der patienten erhielt bluttransfusionen und hatte eine signikant hhere mortalitt ( 14 , 9 % ) , wobei der anteil der patienten mit bluttransfusion ber den zeitraum von 20102015 abnahm . schlussfolgerung der autoren die autoren fordern eine zentralisierung der leberchirurgie in deutschland und allgemein verbindliche qualittsstandards und verweisen auf eine entsprechende initiative der deutschen gesellschaft fr allgemeinund viszeralchirurgie sowie eine initiative strahlenther onkol ( 2020 ) 196 : 98100 der eortc [ 1 ]  . 
weiterhin wird darauf verwiesen , dass die hohen mortalittsraten den onkologischen vorteil der leberchirurgie gefhrden . kommentar die operationsbedingte mortalitt und morbiditt durch die leberchirurgie wird oft stark unterschtzt , was auch die erfahrung vieler von uns aus diskussionen in tumorboards sein drfte . 
zu bercksichtigen ist darber hinaus , dass die publizierten daten nur die in - hospital - mortalitt beschreiben , todesflle aber nach der entlassung aus dem aktuellen aufenthalt bercksichtigen ebenso wenig wie die sterblichkeit nach wiederaufnahme . 
zum anderen lassen die daten die frage aufkommen , inwieweit die technische machbarkeit und das damit verbundene risiko mit einem guten onkologischen ergebnis korreliert bzw . welche alternativen behandlungsverfahren in frage kommen . 
oder anders formuliert : gesetzt den fall , die technisch machbare resektion von 15 lebermetastasen eines mcrc fhrt zu einer r0 - resektion : welches disease - free - survival drften wir erwarten ? wie hoch wre die heilungschance ? welche alternativen zur operation gbe es ? dies sind fragen , die jenseits der technischen frage nach r0resektabilitt gestellt werden mssen , wenn wir den individuellen patientenfall diskutieren . 
es ist in dieser hinsicht zwingend , bei klar denierten patientengruppen auch verfahren wie die operation in prospektiven randomisierten studien zu berprfen auch und gerade mit dem zielkriterium von patient - reported outcomes . unsere aufgabe sollte es sein , auch auf nichtinvasive verfahren wie die stereotaktische radiotherapie ( sbrt ) bei oligometastasierten erkrankungen oder die optimierte , ggf . 
caballero c , burock s , carrion - alvarez l et al ( 2019 ) building a collaboration to improve surgical research through eortc / esso 1409 - climb study : a prospective liver metastasis database with an integrated quality assurance prograeur j surg oncol : 16 . 
andratschke n , alheid h , allguer m et al ( 2018 ) the sbrt database initiative of the german society for radiation oncology ( degro ) : patterns of care and outcome analysis of stereotactic body radiotherapy ( sbrt ) for liver oligometastases in 474 patients with 623 metastases . 
klement rj , abbasi - senger n , adebahr s et al ( 2019 ) the impact of local control on overall survival after stereotactic body radiotherapy for liver and lung metastases from colorectal cancer : a com100 strahlenther onkol ( 2020 ) 196 : 98100 bined analysis of 388 patients with 500 metastases . 
brunner tb , blanck o , lewitzki v et al ( 2019 ) stereotactic body radiotherapy dose and its impact on local control and overall survival of patients for locally advanced intrahepatic and extrahepatic cholangiocarcinoma . 
palma da , olson r , harrow s et al ( 2019 ) stereotactic ablative radiotherapy versus standard of care palliative treatment in patients with oligometastatic cancers ( sabr - comet ) : a randomised , phase 2 , open - label trial . 
the discrimination and calibration abilities of the prediction algorithm were assessed ; if additional factors were identied as independent prognostic factors , updated models were developed using the data from two hospitals and were externally validated using the third hospital . 
models were internally validated using cross - validation and bootstrapping . presented at the 15th meeting of the asian society for neuro - oncology , october 2017 , osaka , japan . 
in multivariable cox regression analysis , mri - dened total resection had a greater impact on os than that shown by the original nomogram , and two additional factorsidh1 mutation and tumor contacting subventricular zonewere newly identied as independent prognostic values . 
ein aktualisiertes nomogramm , das diese neuen variablen enthlt , ist gut kalibriert und war dem ursprnglichen nomogramm ( c - index bei 6 , 12 , 24 und 36 monaten : 0 , 728 ; 0 , 688 ; 0 , 688 und 0 , 685 ) berlegen . 
die externe validierung mit einer unabhngigen kohorte ist gut kalibriert und ergab c - indizes von 0 , 787 ; 0 , 751 ; 0 , 719 und 0 , 702 bei jeweils 6 , 12 , 24 und 36 monaten . schlussfolgerungen mit einem aktualisierten und validierten nomogramm , welches aktualisierte parameter bercksichtigt , ist es mglich , die individuelle berlebensfhigkeit von patienten mit einem glioblastom mit grerer genauigkeit abzuschtzen . schlsselwrter modell validerung subventrikulare zone idh1 - mutation ausma der resektion introduction glioblastoma ( gbm ) is the most common primary malignant brain tumor in adults , with two - thirds of patients expiring within 1 year of diagnosis [ 25 ]  . 
however , despite current standard multimodality therapies , the median os does not exceed 1.52 years [ 15 , 33 ]  . the most important prognostic factors consistently identied in previous studies are age and karnofsky performance status ( kps ) [ 17 ]  . 
aside from these clinical and therapeutic parameters , various molecular alterations including methylguanine - dna methyltransferase ( mgmt ) gene methylation and a mutation in the gene encoding isocitrate dehydrogenase 1 ( idh1 ) were more recently recognized as prognostic factors [ 12 , 23 , 35 ]  . 
an emerging strahlenther onkol ( 2020 ) 196 : 5869 body of literature also demonstrates a notable relationship between tumors contacting the subventricular zone ( svz ) and decreased survival [ 10 ]  . in addition , there remains a need for more reliable prognostic classication models , owing to the underlying heterogeneity of clinical outcomes in patients with gbm . 
the initial approach to analyzing survival in such patients was published in 1993 , and involved the use of recursive partitioning analysis ( rpa ) within distinct prognostic groups based on combinations of variables . 
before the wide adoption of temozolomide ( tmz ) and the use of molecular prole analysis such as mgmt or idh1 mutation statues , rpa was mainly based on clinical factors such as age and performance status . 
the latest rpa model categorized half of the patients into the poorest outcome group ( those with a median os of half a year ) and 40% into a separate group with a median os of 1 year , and includes four variablesage , kps , extent of resection , and neurologic functionthe rst two of which are the most critical [ 17 ]  . 
although incorporating idh1 mutation status enhances prognostic classication [ 35 ] , 65% of patients were still classied as class ii , with a limited ability to predict individualized survival probability . in this context , a nomogram , which is a simple graphical representation of a statistical predictive model , was recently proposed . 
a recently developed nomogram using more than 1000 patients from the nrg oncology ( a newly constituted national clinical trials network group comprising the national surgical adjuvant breast and bowel project [ nsabp ] , the radiation therapy oncology group [ rtog ] , and the gynecologic oncology group [ gog ] ) 0525 and 0825 trials is the most reliable model for predicting the surviving probabilities to date , and incorporates ve variables : age , sex , kps , extent of resection ( eor ) , and mgmt status [ 7 ]  . 
incorporating the newly recognized predictors ( e.g. , idh1 mutation and svz involvement ) in the nomogram and ranking them in order of relative importance ought to be explored to improve the models performance . to address this , we undertook a collaborative effort involving the yonsei university health system ( yuhs ) , seoul national university hospital ( snuh ) , and snu bundang hospital ( sbh ) , three large - volume hospitals in korea , to validate and optimize the nomogram . methods patient selection and data collection following institutional review board ( irb ) approval from each institute , we retrospectively reviewed patients from three institutions : yuhs , snuh , and sbh . 
patients who had been histologically diagnosed with gbm ( world health organization grade 4 ) from 2006 to 2016 were screened . patients treated with concurrent chemoradiotherapy with tmz following surgery using the stupp regimen [ 34 ] and assessed with perioperative mri evaluation were included . patients were excluded if mgmt methylation status was unknown or if they showed leptomeningeal seeding at diagnosis , had been previously diagnosed with a primary cns tumor , or had unavailable follow - up images . 
after applying these exclusion criteria , 837 patients were ultimately analyzed . treatment and follow - up treatment and follow - up for every patient were performed by a multidisciplinary neuro - oncology board . 
tumors were removed following the maximal safe resection protocol , except for in patients who underwent stereotactic biopsy . after preoperative evaluation with mri , most patients underwent navigation - guided surgery . 
diffusion tensor image tractography was used for navigation in patients with tumors that were proximal to areas of motor , vision , and language functions ( i.e. , the eloquent area ) , to minimize possible sequelae . 
all mris were composed of the following sequences : gadoliniumenhanced t1 - weighted , t2 - weighted uid - attenuated inversion recovery , diffusion - weighted , and perfusion - weighted images . 
the extent of surgery was evaluated using immediate post - operative gadolinium - enhanced t1 - weighted mri and categorized as total ( absence of visible contrastenhanced portion ) , subtotal ( at least 90% of the tumor removed ) , partial ( less than 90% of the tumor removed ) , or biopsy ( in case of stereotactic biopsy ) [ 28 ]  . 
radiotherapy ( rt ) was either conventionally fractionated with a median total dose of 60 gy in 30 fractions ( 87.7% ) or hypofractionated with a median total dose of 45 gy in 15 fractions ( 12.3% ) at the physicians discretion . 
patients with old age ( more than 70 years old ) [ 27 ] or poor performance status ( less than kps 70 ) were treated with a hypofractionated regimen . 
patients restrahlenther onkol ( 2020 ) 196 : 5869 ceived either intensity - modulated or 3d conformal rt ; the use of intensity - modulated rt has been increasing since 2011 , owing to changes in national insurance reimbursement ( national unpublished data )  . 
all patients underwent rt plus continuous daily tmz ( 75 mg / m2 of body surface area per day , 7 days per week , from the rst to the last day of rt ) within a median of 3 weeks after surgery . after concurrent chemoradiotherapy , six cycles of adjuvant tmz ( 150200 mg / m2 for 5 days during each 28 - day cycle ) followed . 
most patients underwent mri 1 month after the planned rt as well as every 3 months for the rst 2 years and every 612 months thereafter . table 1 patient characteristics according to the study cohort mgmt promoter methylation and idh1 mutation the dna methylation status of the cpg islands on the mgmt promoter was determined by methylation - specic polymerase chain reaction as previously described , with some modications . 
immunohistochemistry with anti - idh1 r132h ( monoclonal antibody h09 ) or peptide nucleic acid - mediated clamping polymerase chain reaction was used to conrm the idh1 r132h mutation ( idh1 mutation ) status . svz involvement preoperative mri was used to assess the svz involvement of each tumor . 
1 calibration plots in quintiles for the original nrg nomogram at 6 months ( a ) , 12 months ( b ) , and 24 months ( c )  . 
height of each plot indicates the probability of death events in specic timepoints introduced by lim and colleagues [ 20 ] and subsequently used by several other investigators . statistical analysis students t - tests ( normally distributed data ) were used to compare the continuous variables . 
covariates included age at diagnosis , sex ( male or female ) , preoperative kps ( ( cid : 2 ) 70 , 80 , or 90 ) , extent of resection ( total , subtotal / partial , or biopsy ) , mgmt promoter methylation status ( unmethylated or methylated ) , idh1 r132h mutation status ( positive , negative , or unknown ) , and svz involvement ( involvement or non - involvement )  . first , we tested the validity of the nrg oncology nomogram using the cohorts from all the hospitals . 
calibration plots for 6 - , 12 - , and 24 - month survival probabilities , as well as discriminatory potential using harrells concordance index ( c - index ) , were assessed for the original nomograthe calibration plots were obtained graphically by dividing patients into quintiles according to their predicted death events at each timepoint . 
in this analysis , the bootstrap method with 1000 resamples was used to derive optimism - adjusted estimates . an updated nomogram model was then formulated using the data from two hospitals , and independently validated using the data from the third hospital . 
the coefcients introduced into the multivariate cox regression model were used to generate the updated nomograa nal nomogram was also internally validated , and individual predicted survival probabilities at 6 , 12 , and 24 months , as well as at 36 months , were generated . 
however , no satisfactory agreement was reached for the 12month ( 0.618 ; 95% ci 0.5760.659 ) and 24 - month ( 0.606 ; 95% ci 0.5790.633 ) survival probabilities compared to the 6 - month survival probability . 
the median survival was 20.0 ( 95% ci 18.221.7 ) months for the development set and 19.9 ( 95% ci 16.523.3 ) months for the validation set , with no signicant difference between datasets ( p = 0.864 , online resource 1 )  . patients of older age and those with tumors contacting the svz showed poorer outcomes on multivariate analysis . mgmt promoter methylation and idh1 mutation correlated positively with survival ; additionally , mri - dened total resection was a favorable prognostic factor ( table 3 )  . there was no difference in os according to rt volume , dose fractionation scheme , or modality . 
 [ 24 ] , who showed that the actual survival in the top four quintiles of 309 gbm patients from three institutions was higher than the predicted survival rate . based on our data , these ndings might be attributed to the different denitions used for total resection . 
the eor , which was rst dened by a neurosurgeon , was adopted in a 2008 nomogram by the european organisation for research and treatment of cancernational cancer institute of canada ( eortc - ncic ) as well as in the recent nomogram developed by nrg oncology . 
additionally , random survival forest analysis ranked the eor as least important among the ve covariates in the nrg nomograsimilarly , eor had no inuence on the subset of patients treated with modern standard trimodal treatments who were assessed for mgmt status ( n = 103 ) in the eortc - ncic nomograhowever , the mri - dened eor strahlenther onkol ( 2020 ) 196 : 5869 fig . 
4 kaplanmeier survival curves for all patients stratied according to the original nrg nomogram ( a ) and the updated nomogram ( b ) in quintiles based on 12 - month nomogram predictive survival ( nps ) was fourth in its relative importance among seven variables in the updated nomogram . in the present study , eor was trichotomized into total resection ( removal of 100% of the brain mri gadolinium - enhancing tumor ) , subtotal / partial resection ( removal of 90% or less ) , and biopsy . 
raised the possibility that assessing uid attenuated inversion recovery abnormalities is superior to assessing the t1 contrast - enhancing tumor [ 18 ]  . in this context , the question is now whether using different cut - off points or different imaging modalities to categorize eor is most optimal ; in either case , our ndings strongly indicate that using objective and quantitative eor information is indispensable for constructing reliable predictive models for patients with gbm . 
in clinical trials investigating the efcacy of experimental treatments , surgeon - dened eor resulted in heterogeneity in patient characteristics that may have obscured the effect of intervention . another important nding in our study was that idh1 mutation retained its prognostic value ( hazard ratio of 4.26 ) independent of the existing ve variables , and was then successfully incorporated into the updated nomogram even though approximately 7% of patients were positive for this mutation ( who were available with results of idh1 mutation )  . 
patients with both these genetic aberrations ( n = 13 ) and patients who had a good kps ( 90 ) with gross total resection ( n = 39 ) were grouped into class i , which yielded a median os of 67 months . 
similarly , other novel prognostic genetic biomarkers ( e.g. , telomerase reverse transcriptase , c - met , and braf v600e mutation ) other than mgmt are expected to be incorporated into the nomogram [ 1 ]  . tumor contact with the svz , which lines the lateral ventricles and houses neural stem cells , was also independently associated with os in this study ; patients with svz involvement experienced worse os than patients without . 
the underlying mechanisms of increased invasiveness and stronger recruitment of migratory progenitor cells in tumors contacting the svz remain to be fully claried , as does the impact of svz irradiation [ 5 , 32 ] ; however , our ndings with respect to svz involvement are notable . 
further integrations of radiogenomics proling into the nomogram could provide more reliable information to physicians [ 9 , 11 ]  . after including mri - dened eor , idh1 mutation status , and svz involvement in the updated nomogram , the magnitude of the effect of sex and kps decreased substantially compared to the original nrg nomogram [ 7 ]  . on the other hand , the inuence of the eor increased ; moreover , the distinction between total and subtotal resection became clearer . 
furthermore , all patients were asians , an ethnicity that has one of the longest life expectancies in the world [ 6 ] ; therefore , the results may not be directly generalizable to other populations . there may also have been institutional variations in postrecurrence patient management . 
for example , re - irradiation with systemic chemotherapy was preferentially considered as salvage treatment in recurrent patients at one institution [ 16 ] , while molecularly targeted agents ( i.e. , anti - vascular endothelial growth factor antibody ) was preferred at the other institutions . 
however , our eligibility criteria , which included patients treated with a standard trimodal primary treatment , contributed to the homogeneity of our cohort and are relevant to current clinical practice . despite these limitations , our updated nomogram model was validated internally with bootstrapping , and cross - validated independently using an external dataset . 
the strengths of our study include a large sample size ( n = 837 ) with excellent follow - up records and the use of reliable assessments of eor by immediate postoperative brain mri . 
finally , the updated nomogram provides a 36 - month survival probability , which might be more clinically relevant for predicting long - term survivors . in conclusion , both the nrg nomogram and the updated nomogram proved their ability to predict survival probabilities in patients with newly diagnosed gbm . 
however , the updated nomogram rened by mri - based eors , incorporating idh1 mutation and svz involvement , showed acceptable accuracy even in long - term survival probabilities . continued efforts to rene and validate the nomogram prediction tool by optimizing the use of available resources are necessary to realize the goal of assisting glioblastoma patients and their physicians to appraise the anticipated course of disease and aid decision - making in terms of individualized treatment . 
suh declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants or on human tissue were in accordance with the ethical standards of the institutional and / or national research committee and with the 1975 helsinki declaration and its later amendments or comparable ethical standards . 
november 2019 springer - verlag gmbh germany , part of springer nature 2019 hintergrund die ausdehnung des postoperativ zu bestrahlenden volumens bestimmt mageblich die erwartbare toxizitt bei patienten mit kopf - hals - tumoren und kleinere volumina fhren im ergebnis zu einer langfristig verbesserten lebensqualitt . 
in der vorliegenden phase - ii - studie wurden die auswirkungen einer reduktion des postoperativen bestrahlungsvolumens auf die pathologisch befallene halsseite ( bei auslassung der pathologisch tumorfreien seite ) analysiert [ 1 ]  . methodik die studienkohorte umfasste patienten mit plattenepithelkarzinomen im kopf - hals - bereich , bei denen nach tumorresektion und unioder bilateraler neck - dissection ( nd ) aufgrund von risikofaktoren eine postoperative bestrahlung indiziert war . 
zustzlich wurde die lebensqualitt zu unterschiedlichen zeitpunkten mit zwei standardisierten fragebgen erfasst , nmlich nach md anderson dysphagia inventory und michigan patient - reported xerostomia questionnaire . ergebnisse es konnten 73 patienten eingeschlossen werden , wovon 72 in der auswertung bercksichtigt wurden . originalpublikation contreras ja , spencer c , dewees t et al ( 2019 ) eliminating postoperative radiation to the pathologically node - negative neck : long - term results of a prospective phase ii study . 
die tumorlokalisationen verteilten sich auf mundhhle ( 14 - mal ) , oropharynx ( 37 - mal ) , hypopharynx ( 4 - mal ) , larynx ( 16 - mal ) und eine unbekannte primrtumorlokalisation . 
bei 17 patienten ( 24 % ) wurde bei pathologisch tumorfreien bilateralen lymphabusswegen ( pn0 ) lediglich das tumorbett bestrahlt . nach einer durchschnittlichen nachbeobachtungszeit von 53 monaten zeigte sich bei 2 patienten ein therapieversagen der nichtbestrahlten , zuvor pathologisch tumorfreien halsseite . 
die 5 - jahres - raten fr die lokale kontrolle , die lokoregionre kontrolle , das progressionsfreie berleben sowie das gesamtberleben betrugen jeweils 84 % , 93 % , 60 % bzw . 
24 monaten ( p > 0 , 05 )  . schlussfolgerung der autoren der verzicht auf eine postoperative bestrahlung der pathologisch tumorfreien halsseite fhrte bei plattenepithelkarzinomen im kopf - hals - bereich zu exzellenten tumorkontrollraten ohne verschlechterung der langfristigen lebensqualitt . kommentar 1 klinik fr strahlenheilkunde , universittsklinikum freiburg , robert - koch - str . 
3 , 79106 freiburg , deutschland die generelle notwendigkeit sowie die ausdehnung der postoperativen bestrahlung der lymphabusswege bei patienten mit kopf - hals - karzinomen orientieren sich fr ge102 strahlenther onkol ( 2020 ) 196 : 101103 whnlich am risiko fr eine okkulte metastasierung in die lymphknoten . 
whrend eine unilaterale bestrahlung in mehreren konsensusarbeiten nur bei kleinen , klar lateralisierten tumoren , insbesondere im bereich von oropharynx und mundhhle , als akzeptabel diskutiert wurde , stellte bisher ein erreichen der mittellinie durch den primrtumor eine klare indikation zur ausgedehnten bilateralen bestrahlung der zervikalen lymphabusswege dar [ 2 , 3 ]  . die vorliegende studie von contreras und kollegen legt jetzt trotz der offensichtlichen limitationen daten vor , die die klinisch praktizierte risikobewertung einer mittellinienbeteiligung fr die zervikale metastasierung berdenken lassen . 
obwohl eine deutliche mehrheit der eingeschlossenen patienten eine beteiligung oder ein berschreiten der mittellinie durch den primrtumor aufwies , konnte im lngerfristigen follow - up von fast 5 jahren nur bei 2 patienten ein regionres rezidiv an der nichtbestrahlten , initial nodalnegativen halsseite nachgewiesen werden , zumal bei beiden patienten jeweils auch ein lokales rezidiv vorlag . 
obwohl das risiko auf der basis frherer arbeiten mit mehr als 12 % deutlich hher vermutet wird , zeigen ltere untersuchungen zur zervikalen lymphanatomie keine klaren hinweise fr eine verbindung mit den kontralateralen lymphknotenstationen [ 4 , 5 ]  . 
bemerkenswert an den vorliegenden daten ist auerdem , dass bei einer bilateralen pn0 - situation bei etwa einem viertel der patienten komplett auf die bestrahlung der zervikalen lymphabusswege verzichtet wurde . 
dabei ist allerdings zu bercksichtigen , dass mehr als 90 % der eingeschlossenen patienten bilateral ausgedehnt chirurgisch gestaged wurden und zwar in einem ausgewiesenen tumorzentrudie verbliebenen 10 % erhielten bei fehlendem pathologischen nachweis von lymphknotenmetastasen zumindest eine unilaterale neck - dissection und zustzlich eine zervikale [ 18f ] fdg - pet / ct - bildgebung . 
das therapieversagen im bereich der nichtbestrahlten halsseite bei zwei patienten diskutieren die autoren vor allem in hinblick auf das jeweils parallel aufgetretene lokale rezidiv , das zu einer erneuten tumoraussaat gefhrt haben knnte . dies ist insofern plausibel , als die rezidivierung im bereich des nichtbestrahlten halses jeweils deutlich verzgert nach der therapie auftrat . 
andererseits msste das problem einer sekundren verschiebung des abusses zur gegenseite auch bei ausgedehnter lymphatischer tumorlast bercksichtigt werden , so dass bei ausgedehntem ipsilateralem lymphknotenbefall und verzicht auf die kontralaterale bestrahlung die regionren rezidivraten auch kontralateral erhht sein knnten . 
in der vorliegenden studie waren im mittel nur 2 von durchschnittlich 28 , 5 dissezierten lymphknoten vom tumor befallen . obwohl diese vielversprechende studie das dilemma einer mglichen bertherapie in der postoperativen strahlentherapie bei kopf - hals - tumoren klar aufzeigt , unterliegt ihre interpretation den natrlichen limitationen einer monozentrischen phase - ii - studie . 
dennoch bietet die arbeit zum ersten mal berzeugende und prospektiv erhobene ergebnisse einer limitierten bestrahlung der zervikalen lymphabusswege fr ein hochrisikokollektiv von patienten mit kopf - hals - tumor . die reduktion des behandlungsvolumens ging in der vorliegenden arbeit mit einem zu erwartenden deutlichen erhalt von therapiebezogener lebensqualitt einher . 
weder in der globalen lebensqualitt noch in den verschiedenen getesteten funktionellen domnen konnte eine nachhaltige verschlechterung im vergleich zur ausgangssituation vor bestrahlung festgestellt werden . insbesondere die xerostomieraten , die sich in den ersten 6 monaten noch erhht zeigten , lagen im lngerfristigen verlauf nicht mehr signikant ber dem ausgangsniveau . allerdings ist einschrnkend zu sagen , dass der einschluss in die studie und damit auch die erhebung der ausgangswerte fr die lebensqualitt erst nach abgeschlossener operation erfolgten , so dass die chirurgischen einschrnkungen trotz guter ergebnisse fr die strahlentherapie mglicherweise dennoch nachhaltig die lebensqualitt der analysierten patienten beeintrchtigten . 
legt den schluss nahe , dass bei der multimodalen therapie von kopf - halskarzinomen ein verzicht auf die postoperative bestrahlung der nichtbefallenen halsseite ( n ) unter bestimmten voraussetzungen eine sichere und effektive tumortherapie bietet , jedenfalls dann , wenn ein chirurgisches staging der zervikalen lymphknoten vorausging . 
neben noch zu besttigenden therapieanstzen zur deintensivierung von begleitender chemotherapie und bestrahlungsdosen knnte die reduktion des behandlungsvolumens auch helfen , die toxizitten der strahlentherapie zu verringern und die lebensqualitt zu erhalten . erik haehl und nils h . 
navran a et al ( 2019 ) the impact of margin reduction on outcome and toxicity in head and neck cancer patients treated with imageguided volumetric modulated arc therapy ( vmat )  . 
 ( 19592019 ) klaus - rdiger trott1 published online : 11 december 2019 springer - verlag gmbh germany , part of springer nature 2019 neuherberg to work for his phd . 
it permitted daily evaluation of radiation responses and exible experimental designs , was very precise , and associated with minimal toxicitythe animals even gained weight during experimental follow - up . the model was based on irradiating a eld of 3 3 mm in the lower surface of the mouse tongue with 29 - kv x - rays , thus sparing the upper surface and , in consequence , pain during eating . 
his phd thesis in 1997 entitled untersuchungen zur strahlenreaktion des unbehandelten und stimulierten zungenepithels der maus ( studies on the radiation response of the untreated and the stimulated epithelium of the murine tongue ) was an epitome of clarity and inventiveness . 
to the diverse program of the gsf experimental radiotherapy group , wolfgang contributed his expertise in veterinary medicine , taking part in the development of novel models for normal tissue studies in organs such as heart , lung , stomach , and rectum in rats , mice , and also large animals . in 1995 , on the invitation of thomas herrmann , wolfgang became leader of the normal tissue research group in the large and dynamic radiobiology research division of the dresden radiotherapy department . 
wolfgang sat in the clinical conferences to understand the problems faced by clinicians and then designed experimental protocols to explore the underlying biological mechanisms . his work on the radiobiology of oral mucositis culminated in the creation of a clinical service and research program for oral hygiene in patients treated with radiotherapy for head and neck cancers . 
his wife elke drr not only ran this service , she was the stronghold in his restless life in radiobiology . in dresden , the spectrum of his research expanded to other organs . 
other physiological techniques to measure functional radiation effects were developed , often in close wolfgang drr was only 59 years old when he died of heart failure on 13th october 2019 . wolfgang was one of the outstanding clinical and translational radiobiologists of his generation , more innovative and productive than most of his peers . 
his inuence on our understanding of the pathogenesis and biology of side effects of radiotherapy in organs and tissues can hardly be overestimated . wolfgang was born on 29th november 1959 , close to the bavarian border with the former gdr in frbau near hof . 
after graduation , in 1985 , he joined the experimental radiotherapy group at the institute of radiation biology at the gsf ( cid : 2 ) klaus - rdiger trott klaustrott@yahoo.it 1 mnchen , germany 108 strahlenther onkol ( 2020 ) 196 : 107108 cooperation with the dresden tumor response group of michael baumann . 
wolfgang was also principal investigator in key projects of international , in particular european , research programs , such as cardiorisk and allegro . it was in dresden that he discovered his talent for teaching . 
his lectures on pathogenesis , fractionation sensitivity , and the effects of biological and pharmacological interventions in radiation - induced normal tissue damage shaped the understanding of concepts of translational radiobiology in hundreds of young radiation oncologists throughout europe . 
an objective sign of his great role in clinical radiobiology is the fact that of the 27 chapters of the popular textbook basic clinical radiobiology , he is author or co - author of seven . 
the current phd students whom he left behind will have to prove that his teaching lives on . in 2007 , wolfgang moved to vienna to develop a new program of applied and translational radiobiology with great support from the head of clinical radiation oncology there , richard ptter . 
on the website of the medical university , this appointment was hailed as an endowed professorship to secure a long - term translational collaboration between the university and the proton and carbon ion center at medaustron . 
yet , four years later , the medical university decided to terminate translational radiobiology research in the department of radiation oncology and change the remit of the laboratory into molecular radiotherapy within the vienna biocentre . 
more than 200 original publications and reviews , numerous letters to the editor and comments on papers published by others , and many hundreds of abstracts , teaching lectures , and seminar talks spread his research and his ideas . 
he edited and wrote ve books and wrote 42 book chapters . wolfgang was member of the editorial boards of various journals , including radiotherapy and oncology , radiation and environmental biophysics , and was section editor for radiobiology of strahlentherapie und onkologie . 
wolfgang was on committees of important radiobiological institutions : he was council member and president ( 20032004 ) of the european radiation research society , council member and president ( 20022006 ) of the german society for biological radiation research , member of the radiobiology committee of the european society for radiotherapy and oncology , council member of the german society for radiation oncology , and council member of the austrian society for radiation oncology , radiobiology , and medical radiation physics ( gro ) , being awarded honorary membership of gro in 2011 . 
a systematic review of upper abdominal re - i was performed with the aim of exploring the cumulative dose , toxicity , and outcomes . methods a computerized search was undertaken in medline , embase , ovid , and the cochrane database . 
dannunzio university , via dei vestini , 66100 chieti , italy 2 department of radiation oncology and nuclear medicine , state hospital mater salutis aulss 9 , 37045 legnago ( vr ) , italy 3 uoc radioterapia oncologica , dipartimento di diagnostica per immagini , radioterapia oncologica ed ematologia , fondazione policlinico universitario a . 
gemelli irccs , roma , italy proton therapy unit , department of oncology , azienda provinciale per i servizi sanitari , apss , 38123 trento , italy 5 department of radiotherapy , azienda u . 
della valle daosta , 11100 aosta , italy 6 radiation oncology section , university of perugia and perugia general hospital , 06156 perugia , italy 7 department of oncology and radiotherapy , azienda ospedaliero universitaria ospedali riuniti , ancona , italy strahlenther onkol ( 2020 ) 196 : 114 results sixteen studies met the inclusion criteria , with the total patients numbering 408 . 
es wurde eine systematische berprfung der oberbauch - re - i durchgefhrt , mit dem ziel , kumulative dosis , toxizitt und ergebnisse zu untersuchen . methoden eine computergesttzte suche wurde anhand von medline , embase , ovid und der cochrane - datenbank durchgefhrt . 
es wurden nur studien mit angabe der toxizitt und / oder gefahrlosigkeit als ergebnis bercksichtigt . um die vergleichbarkeit der verschiedenen re - i - regime zu verbessern und den zusammenhang zwischen strahlentherapie ( rt ) - dosis und toxizitt zu beurteilen , wurde die quivalentdosis in 2 - gy - fraktionen nach dem linear - quadratischen modell berechnet . ergebnisse sechzehn studien erfllten die einschlusskriterien bei einer gesamtzahl von 408 patienten . 
bei 66 , 9% der patienten wurde eine verbesserung der schmerzsituation verzeichnet . schlussfolgerung trotz der einschrnkungen aufgrund weniger beweise und aufgrund der vorwiegend retrospektiv gestalteten studien spricht unsere berprfung dafr , dass oberbauch - re - i durchfhrbar ist , was schwere toxizitt bei guter lokaler kontrolle und linderung der symptome anbelangt . schlsselwrter rebestrahlung abdomen gastrointestinale malignome toxizitt kumulative dosis introduction survival from most types of cancer has improved in recent years , even for some of the more lethal cancers ( esophagus , liver , and pancreas ) [ 1 ]  . 
the number of patients experiencing loco - regional recurrence and / or second primary tumors in previously irradiated areas and the subsequent demand for re - irradiation ( re - i ) have therefore both increased . for example , it has been estimated that for patients with pancreatic adenocarcinoma , local recurrence ( lr ) occurs in 80% of cases within 2 years of curative - intent therapy , and 30% of these lr are isolated , without distant metastases [ 2 ]  . in several cases of abdominal malignancies , radical reresection represents the most effective treatment and could be considered as the rst therapeutic choice . 
unfortunately , less than half of the patients with lr show cases of resectable disease and surgery may not always be possible due to patient comorbidities and clinical conditions . ultimately , re - i remains a much debated topic as a result of the possible radio - resistance of recurrent cancer and the probable toxicities of previously irradiated surrounding tissues . 
in particular , the tolerability of organs such as the strahlenther onkol ( 2020 ) 196 : 114 liver , small bowel , stomach , and spinal cord could limit the dose to the tumor . 
for these reasons , re - i of gastrointestinal tumors has historically been associated with few benets and poor outcomes . more recently , re - i could be considered a therapeutic option in this setting [ 36 ] thanks to the availability of modern radiation techniques including stereotactic rt ( srt ) , intensity - modulated radiation therapy ( imrt ) , and / or proton therapy ( pt ) , which permit a steep decrease in dose gradients and maximum sparing of the surrounding organs at risks ( oars )  . although mainly retrospective , several studies have been performed to evaluate the efcacy and safety of re - i . 
they show a benet in local control ( lc ) , symptom relief , and preservation of good qol in many cancer types [ 79 ]  . however , based on current knowledge , only one study referring to abdominal malignancies proposes dose constraints for re - i , reporting the cumulative dose used in the retreatment strategy [ 9 ]  . 
for these reasons , the optimal dose of re - i related to a good tolerance of abdominal re - irradiated oars is poorly understood and it is almost impossible to predict the risk of normal tissue complications from re - i in clinical practice . based on these considerations , this reviewconducted on behalf of the re - irradiation working group of the italian association of radiotherapy and clinical oncology ( airo ) aims to analyze the cumulative doses of previous radiation treatment and re - i , related toxicities , and outcomes , whilst focusing on gastrointestinal tumors in the upper abdominal site . methods study selection a computerized search of the literature was performed using the medline , embase , ovid , and cochrane databases from the time of inception to 2018 . 
the computer search was supplemented manually using reference lists for all available review articles , primary studies , meeting abstracts , and bibliographies of books to identify studies not encountered in the computer search . 
the present systematic review was performed following recommendations from the preferred reporting items for systematic reviews and metaanalyses ( prisma ) [ 10 ]  . inclusion and exclusion criteria studies included were prospective or retrospective by means of analyzing more than 10 patients re - irradiated after 1995 . 
abstracts , letters , proceedings from scientic meetings , editorials , expert opinions , reviews without original data , case reports , studies lacking toxicity and / or safety outcomes , repetitive data , non - english language papers , and animal studies were excluded . review of the trials a methodological assessment of the quality of studies was performed with a checklist for quality appraisal of case series studies produced by the institute of health economics ( ihe ) and modied to improve applicability [ 11 ]  . to improve the comparability of the different re - i regimens and to assess the relationship between radiation dose and toxicity , when not reported in the study , the equivalent dose in 2 - gy fractions ( eqd2 ) was calculated according to d ( d / n + / ) / ( 2 + / ) , and taken from the linear quadratic model . 
to determine the pooled g 3 toxicities rate , overall survival ( os ) , local recurrence - free survival ( lrfs ) , and pain relief , a meta - analysis of several singlearm studies was performed . 
we used random - effects models because there was great subjectivity given the lack of related control groups in the non - comparative studies and a tendency towards high heterogeneity . results the literature search identied 60 citations . 
the median quality assessment of diagnostic accuracy assessment scoring criteria 2 ( quadas - 2 ) was 13 out of a possible 18 ( range 1015 ) , as shown in table 2 . 
in all cases , the reported locations of re - irradiated lesions were within at least the 50% isodose of the previous rt plan and often within the highdose region . 
previous rt was delivered with a median dose of 50.4 gy , ranging from 45 to 74.5 gy , using conventional fractionation in all studies but one [ 21 ] , wherein an srt boost was delivered after conventional external beam rt . the mean time elapsed since previous irradiation ranged from 2 to 162 months , the median being 15 months ( range 932 months )  . 
preliminary experimental and clinical data have shown that a variety of normal tissues recover from occult radiation injury , although studies on animal kidneys have suggested progression of radiation - induced toxicity rather than recovery from it [ 27 ]  . moreover , a possible radio - resistance of recurrent cancer has been reported . 
as an example , concerning rectal cancer , pathologic complete responses were reported in only 9% of re - irradiated patients with lr , compared to up to 20% of patients with locally advanced primary tumors after longcourse chemoradiation [ 28 ]  . it is still unclear to this day whether dose intensication in re - i improves the chance of lc and survival , and even the optimal dose of re - i related to the tolerance of reirradiated abdominal oars is still poorly understood . dose constraints for re - i are currently not available , except for a proposal in small bowel , rectum , and bladder based on data coming from only one series of patients treated by srt [ 9 ]  . 
3 pooled toxicity prole using 3d - imrt ( 3 dimensional - intensity modulated radiation therapy ) , srt ( stereotactic radiation therapy ) , protons , brachytherapy ( a ) , and using hypo - fractionation ( b ) and normoor hyper - fractionation ( c )  . 
es effect size , ci condence intervals dose of 110 gy3 with a maximum of 10 cc tissue for the bowel was used and the treatment resulted in a median cumulative dose given to the bowel of 98 gy3 . 
there was no g4 or 3 acute or late toxicity , and re - i proved to be effective in terms of tumor and symptom relief ( pain and bleeding ) , showing a response rate of 96% . the aim of this review was to investigate the cumulative doses of previous radiation treatment and re - i , related toxicities , and outcomes , focusing on gastrointestinal tumors . the included studies were shown to be widely heterogeneous for doses , fractionations , and re - i techniques , and the distinction between curative and palliative intent was often not clear . 
moderate hypofractionation regimens were delivered when highly conformal techniques such as imrt [ 15 , 22 , 24 , 26 ] and srt [ 9 , 17 , 18 , 21 , 23 , 25 , 26 ] were used . 
4 pooled objective 1 year overall survival ( a ) , 1 year local recurrence free survival ( b ) , pain relief ( c ) in re - irradiated patients for included studies . 
es effect size , ci condence intervals pancreatic cancer the interest in srt use for pancreatic cancer re - i arises from the difculty of obtaining lc in this disease . 
overall , modest hypofractionation of srt ( 35 fractions ) to limited volumes reported acceptable g3 acute gastric and bowel toxicities ( less than 10% ) [ 17 , 21 , 23 ]  . 
in a series of 23 patients re - irradiated with srt , all gastric toxicities were identied in patients who received high doses ( 54 and 60 gy ) within the rst radiation treatment [ 23 ]  . 
severe late toxicity was reported in 7% or fewer patients overall [ 17 , 18 , 21 ]  . pt also showed good tolerability in a prospective study of 15 patients [ 6 ]  . 
one patient developed gastric obstruction from disease progression conrmed with biopsy . concerning liver tolerance , some studies reported that the main factors related to the risk of hepatic toxicities could be identied in a tailored selection of re - i patients . 
indeed , in a series of 36 patients with hepatocellular carcinoma ( hcc ) who received re - i through imrt or srt , rild ( transient and permanent ) was reported in 13 patients ( 36% )  . 
residual liver function using a pretreatment childturcottepugh score 6 was the only clinical parameter predictor of rild [ 22 ]  . liver re - i was also investigated in a moderately large retrospective series of 49 patients with hcc and / or liver metastases [ 26 ]  . 
overall , the low rate of rild ( 4.1% ) observed in this study did not allow for statistical signicance in the correlation of treatment and clinical parameters with toxicity to be reached . esophagus three studies reported acute and late severe esophageal toxicities . 
despite the lower radiation doses used in the study conducted by yamaguchi et al . , 6 patients ( 20% ) suffered from severe esophageal toxicities , although in 2 patient cases , esophageal perforation ( g34 ) occurred within the uncontrolled loco - regional tumor [ 16 ]  . 
advanced t stage at the time of re - i and re - irradiated esophagus volume extension receiving 90% of the prescribed dose or more were recorded as being signicantly correlated with g3 or higher esophageal toxicity . these data are in accordance with those shown in a small series of 16 patients affected by unresectable esophageal recurrences re - irradiated by pdr - brt [ 14 ]  . 
a g3 acute esophagitis was reported in 1 patient , whilst , contrastingly , g4 complications were reported in 3 patients with uncontrolled loco - regional disease ( esophago - tracheal stulae in 2 patients and fatal arterial bleeding in 1 patient )  . 
the authors suggested that total dose should be limited to 15 gy in the palliative setting . finally , in the prospective trial of 14 patients treated by pt , acute non - hematologic toxicities g3 and g5 were reported in 4 patients ( 29% ) and 1 patient ( 7% ) , respectively , whereas late g3 toxicities and late g5 esophageal ulcers were identied in 4 and 1 patients , respectively , and appear to be more related to tumor progression rather than to treatment [ 5 ]  . the authors of all of the studies considered concluded that whether severe g4 toxicities are related to treatment or progressive disease remains unclear . 
taking into account the heterogeneity of patient population and treatment intent , individualized treatment options could be offered to each patient . overall , our review reported a pooled result of severe toxicity ( g3 ) of 12% ( 95%ci : 7.619% ) , and this rate is comparable to other curative treatments for abdominal gastrointestinal malignancies . 
however , these results appear to be of interest if we consider that patients undergoing re - i usually have a very unfavorable prognosis and are often not eligible for re - resection due to comorbidities , clinical conditions , or unresectable disease . 
furthermore , in the prospective trial on pt for pancreatic recurrences , os at 1 year was 67% and the median os was 16.7 months ( 95% ci , 4.736 ) [ 6 ]  . 
these data appear quite favorable compared with outcomes reported in the re - i study by srt [ 18 , 26 ] , as well as compared to historical methods of control for denitive chemoradiation in primary treatment for locally advanced pancreatic cancer [ 29 ]  . the pooled 1 - year lrfs rate was 66.5% ( 95% ci : 58.775.4% ) and , therefore , it seems to be promising . 
however , patient selection criteria as well as dose and volume choices should be conservative , due to the risk of severe bowel toxicity described in the other series [ 15 , 17 , 21 , 25 ]  . a large proportion of patients included in the considered studies suffered from pain prior to therapy . 
the pooled analysis showed that 66.9% of patients experienced pain relief , conrming a potential role of re - i in the palliative setting . critically , several limitations exist in our systematic analysis . 
first , because no randomized trials or comparative studies with re - i have been conducted , included studies were completed using single - arm trials , with potential performance bias . 
all other studies incorporated were retrospective , with a small number of patients ( only 4 studies with > 30 patients ) and large inclusion criteria variability ( primary cancers with or without distant metastases )  . moreover , data concerning toxicity of organs at risk from cumulative dosevolume histograms are lacking and dosevolume constraint references for abdominal re - i cannot be provided . strahlenther onkol ( 2020 ) 196 : 114 despite an inability to draw upon recommendations due to the limitation of literature , our data can suggest the use of srt with hypofractionation . 
systematic recordings , collections , and the analysis of outcomes will undoubtedly improve our knowledge on this topic and contribute to a renement of retreatment strategies . a reliable clinical tool for measuring the effectiveness and safety of re - i is in fact still unavailable . 
 ( re - treatment volumes value for prediction of effects of re - irradiation ) project was created in italy , under the guidance of the re - irradiation working group of the italian association of radiotherapy and clinical oncology ( airo ) , as a partner network to exchange experiences in re - i , while retrospective data collection in a large multi - institutional setting is currently ongoing [ 30 ]  . conclusion highly conformal techniques , especially srt and pt , have shown promising results , with high rates of local tumor and symptom control in re - i for abdominal gastrointestinal malignancies , and could play a role in treating patients with curative or palliative intent . 
november 2019 springer - verlag gmbh germany , part of springer nature 2019 zielsetzung pravacur , eine phase - ii - studie , untersuchte die wirksamkeit von pravastatin als antibrotisches medikament bei patienten mit manifester kutaner und / oder subkutaner fibrose nach einer komplettierten strahlentherapie oder radiochemotherapie [ 3 ]  . patienten und methode haupteinschlusskriterien fr die patienten waren ein plattenepithelkarzinom der kopf - halsregion in remission , eine radiogene fibrose ( rif ) vom grad 2 nach den kriterien der national cancer institutecommon toxicity criteria v4.0 ( ctcae ) , kutan oder subkutan , und keine vorausgegangene therapie mit statinen oder fibraten . 
sekundre endpunkte beinhalteten die reduktion des schweregrads der rif nach den ctcae - kriterien , die vertrglichkeit von pravastatin und die lebensqualitt . ergebnisse zwischen februar 2011 und april 2016 wurden 60 patienten mit einer rif in die studie eingeschlossen , die bei 37 , 22 und einem patienten jeweils einen grad 2 , 3 und 4 nach ctcae - kriterien erreichte . 
insgesamt 18 paoriginalpublikation bourgier c , auperin a , rivera s , boisselier p , petit b , lang p , lassau n , taourel p , tetreau r , azria d , bourhis j , deutsch e , vozenin mc ( 2019 ) pravastatin reverses established radiation - induced cutaneous and subcutaneous fibrosis in patients with head and neck cancer : results of the biology - driven phase 2 clinical trial pravacur . 
44 , 39120 magdeburg , deutschland tienten hatten eine behandlung mit pravastatin ber nur < 11 monate aus folgenden grnden : bei 8 patienten ( 13 % ) wurde es wegen nebenwirkungen grad 2 und bei 5 patienten wegen eines widerrufs der einwilligung abgesetzt ; darber hinaus hatten 5 patienten ein rezidiv bzw . 
nach 12 monaten war der schweregrad der rif bei 50 % der patienten geringer als vor beginn der studienmedikation ( n = 21 ; 95 % - ki 34 , 265 , 8 % )  . 
pravastatin wurde gut vertragen und hatte nur eine niedrige rate an grad3 ( n = 1 , myalgie ) und grad - 2 - toxizitten ( n = 3 , myalgie / arthralgie und sophagitis )  . schlussfolgerung der autoren diese prospektive phase - iistudie untersttzt die hypothese der umkehrbarkeit einer strahleninduzierten fibrose . 
sie zeigt , dass pravastatin ( 40 mg / tag ber 12 monate ) bei patienten mit kopf - halstumoren und einer ( sub ) kutanten fibrose vom grad 2 nach strahlentherapie antibrotisch wirksam ist . kommentar radiogene brotische vernderungen stellen eine unerfreuliche chronische therapiefolge dar , und alle derzeit verfgbaren therapeutischen manahmen sind dagegen nahezu wirkungslos . 
unter den medikamenten , die mit dem ziel eingesetzt wurden , eine rif therapeutisch anzugehen , benden sich so unterschiedliche substanzen wie superstrahlenther onkol ( 2020 ) 196 : 104106 oxiddismutase , vitamin e , pentoxifyllin oder zielgerichtete inhibitoren des transforming growth factor ( tgf - 1 ) , platelet - derived growth factor ( pdgf ) und seines rezeptors ( pdgf - r ) , connective tissue growth factor ( ctgf ) und inhibitoren des rho / rock intracellular signallin pathway , unter die auch die statine fallen [ 1 ]  . statine gehren weltweit zu den hugsten verschriebenen medikamenten und werden zur verringerung des risikos fr kardiovaskulre erkrankungen wie myokardinfarkt und apoplex eingesetzt , wobei atorvastatin gefolgt von pravastatin in dieser eigenschaft am wirksamsten sind [ 2 ]  . 
diese medikamente hemmen die hmg - coa - reduktase und senken das ldl - cholesterdaneben blockieren statine aber auch den rho / rock - signalweg durch eine inhibierung der isoprenylierung . 
die blockade der umdifferenzierung von fibroblasten in myobroblasten ist einer der mechanismen , die dafr als wichtig erachtet werden , denn myobroblasten produzieren extrazellulre matrix und aktivieren das wundheilungsprogramm chronisch . 
diese radiobiologische erkenntnis am darm wurde in der vorgestellten studie wegen der klinisch besseren quantizierbarkeit des antibrotischen effekts an patienten mit kopf - hals - tumoren und rif eingesetzt . trotz der heute deutlich verbesserten bestrahlungstechniken durch die imrt , etc . 
lag in einer studie von nevens [ 4 ] die hhergradige fibroserate ( > grad 2 ) bei patienten mit einer vorausgegangenen neck - dissektion 6 monate nach abschluss der radiotherapie immerhin bei 71 % . 
die klinische bedeutung einer fibrose ergibt sich aus bewegungseinschrnkungen des halses , aus lymphdemen , trismus und dysphagie . die besondere bedeutung der hier kommentierten studie liegt darin , dass es sich um die erste prospektive phase - iistudie zur behandlung einer durch strahlentherapie induzierten fibrose mit statinen handelt . 
bei dieser patientenzahl wre ein randomisiertes vorgehen nicht zielfhrend gewesen . eine weitere strke der studie ist die wahl des primren endpunkts der reduktion der fibrosedicke in der messung des hochfrequenzultraschalls nach 12 monaten . 
bei 14 der 19 untersuchten patienten zeigte die pathohistologische untersuchung von hautstanzen eine kutane und subkutane normalisierung , die gekennzeichnet war von einer reduktion von immunzellen und einer restitution der dicke der epidermis . 
zurzeit rekrutieren drei studien , die den einsatz unterschiedlicher ace - hemmer zur prophylaxe der radiogene lungenbrose testen . fazit die studie macht erstmals in einer prospektiven untersuchung darauf aufmerksam , dass rif reversibel sind . 
gresser u , gathof bs ( 2004 ) atorvastatin : gold standard for prophylaxis of myocardial ischemia and strokecomparison of the clinical benet of statins on the basis of randomized controlled endpoint studies . 
haydont v , bourgier c , pocard m , lusinchi a , aigueperse j , math d , bourhis j , vozenin - brotons mc ( 2007 ) pravastatin inhibits the rho / ccn2 / extracellular matrixcascade in human brosis ex106 strahlenther onkol ( 2020 ) 196 : 104106 plants and improves radiation - induced intestinalbrosis in rats . 
nevens d , duprez f , daisne jf , laenen a , de neve w , nuyts s ( 2017 ) radiotherapyinduced dermatitis is a strong predictor for late brosis in head and neckcancer . 
this prospective multicentre study was designed to compare the qol of patients with limited ( 13 ) brain metastases treated with either whole brain ( wbrt ) or stereotactic radiotherapy ( srt )  . methods from 01 / 200703 / 2011 , 90 limited brain metastases patients who were previously untreated ( n = 77 ) or had undergone primary surgery ( n = 13 ) were recruited at 14 centres in germany and austria . 
1 , 30625 hannover , germany 2 department of radiation oncology , martin luther university halle - wittenberg , halle ( saale ) , germany 3 department for dermatology and allergology , helios klinikum berlin - buch , berlin , germany strahlentherapie 360 , praxis am sana - klinikum duisburg , duisburg , germany 5 department of radiation oncology , tu mnchen , munich , germany 6 medical faculty , department of radiation oncology , cyberknifeand radiation therapy , university of cologne , cologne , germany 7 department of radiation oncology , st . 
elisabeth hospital straubing , straubing , germany 8 department of radiation oncology , hospital landshut , landshut , germany 9 department of radiation oncology , krankenhaus barmherzige schwestern linz and medical faculty , johannes kepler university linz , linz , austria strahlenther onkol ( 2020 ) 196 : 4857 results fifty - two patients ( 58% ) received wbrt and 38 ( 42% ) received srt . 
motor dysfunction ( p < 0.001 ) , communication decits ( p = 0.002 ) and leg weakness ( p < 0.001 ) declined signicantly only in patients treated with wbrt . 
comparing the two radiotherapy techniques over time , the results showed signicant differences in symptom scores for future uncertainty , fatigue and appetite loss . conclusions qol data as an outcome of the paper should be considered in decision making on the irradiation technique in patients with small number of brain metastases . 
in dieser prospektiven , multizentrischen studie wurde die lq von patienten mit limitierten ( 13 ) hirnmetastasen , die entweder mit ghrt oder stereotaktischer bestrahlung ( srt ) behandelt wurden , verglichen . patienten und methoden von 01 / 200703 / 2011 wurden 90 patienten mit bisher unbehandelten ( n = 77 ) oder primr chirurgisch versorgten ( n = 13 ) limitierten hirnmetastasen an 14 zentren in deutschland und sterreich rekrutiert . 
die lq wurde mit dem eortc - qlq - c15 - pal und dem hirn - modul bn20 vor beginn der strahlentherapie und 3 monate danach gemessen . ergebnisse 52 patienten ( 58 % ) erhielten eine ghrt und 38 ( 42 % ) eine srt . 
die motorische dysfunktion ( p < 0 , 001 ) , kommunikationsdezite ( p = 0 , 002 ) und beinschwche ( p < 0 , 001 ) verschlechterten sich signikant nur bei patienten mit ghrt . 
over the past several years , there has been a shift from treating these patients with whole brain radiotherapy ( wbrt ) towards applying hypofractionated stereotactic radiotherapy ( hfsrt ) [ 19 , 35 ] , stereotactic radiosurgery ( srs ) [ 42 ] , novel cytotoxic agents and other targeted therapies [ 1 ]  . studies comparing treatment combinations showed that wbrt with srs resulted in better intracranial and local control but not in better overall survival ( os ) than srs alone [ 3 , 6 , 12 , 32 ]  . 
a matched pair analysis showed that treatment outcomes were not signicantly different after wbrt and srs compared with surgery with additional strahlenther onkol ( 2020 ) 196 : 4857 wbrt and local boost radiotherapy . 
a meta - analysis concluded that patients with limited bm have no os benet with wbrt plus srs boost compared with srs alone [ 43 ]  . therefore , srs alone should be considered a routine treatment option due to favourable neurocognitive outcomes , less risk of late side effects , and no adverse effects on a patients performance status [ 43 ]  . the radiation therapy oncology group ( rtog ) 9508 analysed patients with 1 , 2 or 3 bm treated with wbrt and srs versus wbrt alone . 
however , in patients with high graded prognostic assessment ( gpa ) scores ( 3.54 ) , there is a survival advantage regardless of whether they have 1 , 2 , or 3 bm . this benet did not extend to patients with lower gpa scores [ 37 ]  . concerns over wbrt regarding limited treatment response , cognitive decits , neurological decits and reduced qol [ 2 , 29 ] motivate researchers to adopt more focused radiotherapy options , such as srs or hfsrt [ 2 , 23 ] , in cases of limited bm . 
to the best of our knowledge , no publication to date has focused on comparing the qol between patients treated with wbrt and patients treated with stereotactic radiotherapy ( srt )  . 
information on health - related qol could help physicians , patients and family members make appropriate decisions between the various treatment options . overall , the number of published articles regarding qol in patients with bm is limited [ 40 ] , and most studies report qol outcomes in patients who have received wbrt [ 2 , 14 , 20 , 24 ]  . 
the discussion pertaining to whether patients with limited bm benet more from wbrt or local radiotherapy with regard to maintained or improved qol led us to address this question prospectively within a time frame of three months after radiotherapy . patients and methods recruitment patients with limited ( 13 ) bm of solid tumours were recruited at 14 radiation oncology centres from february 2007 to march 2011 . 
patients were excluded if they had received previous radiotherapy of the cranium or if chemotherapy was planned during the time of irradiation . furthermore , patients were excluded from this study if their physical or cognitive function was not sufcient to complete the questionnaire . 
informed consent was obtained from all individual participants included in the study . general eligibility criteria included age 18 years , karnofsky performance status ( kps ) 50 , sufcient compliance , satisfactory german language skills and no major psychological impairment . 
if a boost was indicated , it was applied after a three - dimensional ( 3d ) - planning procedure . the dose of hfsrt was determined based on the localization and size of the metastasis , the irradiated whole brain volume and the different institutional protocols . 
in hfsrt , the tumour lesion in the fused axial t1 - weighted contrast enhanced magnetic resonance images ( mri ) or the tumour bed in the postoperative mri was dened as gross tumour volume ( gtv ) , and a 4 - mm safety margin was chosen for the planning tumour volume ( ptv )  . srs was applied only in denitive situations and in cases of lesions up to 3 cm or greater than 3 cm with 20 or 18 gy ( 95% enclosing isodose ) , respectively . 
doses were reduced near the brain stem . qol was assessed before radiotherapy using the european organization for research and treatment of cancer ( eortc ) questionnaires , qlq - c15 - pal and qlq - bn20 ( see below )  . 
important patient and tumour characteristics were also collected , such as kps score and barthel index [ 25 ] , the number of brain metastases , recursive partitioning analysis ( rpa ) and gpa class [ 15 , 36 ] , primary tumour characteristics , and extracranial disease . 
ethics approval was obtained from the ethics committee at the university of wuerzburg , germany and from the medical school hannover , germany . quality - of - life questionnaires the qlq - c15 - pal is a validated shortened version of the qlq - c30 [ 16 ]  . 
the qlq - c15 - pal contains 15 items for the following nine domains : physical function , emotional function , global qol , pain , fatigue , appetite , dyspnoea , constipation and sleep . each item is scored from 1 to 4 ( not at all , 1 ; a little , 2 ; quite a bit , 3 ; and very much , 4 )  . 
the scores for each symptom or function on the bn20 and qlq - c15 - pal questionnaires were transformed to numbers from 0100 , where 0 represents not at all and 100 represents very much [ 41 ]  . to determine the clinical relevance of changes in healthrelated quality - of - life ( hrqol ) scores , the method of osoba et al . 
on a scale from 0 to 100 , a difference of 10 points was classied as the minimum clinically meaningful change in the mean value of a hrqol parameter [ 28 ]  . 
the signicance level was set to 0.05. clinically relevant changes were dened as follows : changes had to be statistically signicant ( p < 0.05 ) , and mean score changes had to be 10 points for moderate changes and 20 points for large clinical changes [ 28 ]  . statistical analyses were performed using the statistical package for social sciences ( spss ; version 22 )  . results patient and treatment characteristics from january 2007 to march 2011 , 90 patients with limited ( 13 ) bm were recruited at 14 centres in germany and austria . 
patient and treatment characteristics , including the pretreatment kps score and barthel index , are presented in table 1 . survival data and intracranial control survival status was known in all 90 patients . 
twenty - three patients ( 25.6% ) died within 3 months after the beginning of radiation therapy ( 16 patients treated with wbrt and 7 patients treated with srt )  . 
as shown in table 2 , there were signicant differences in baseline physical function , hair loss and nausea between the wbrt and srt groups before the start of radiotherapy , with better physical functioning and less nausea in the srt group and less hair loss in wbrt patients . we calculated qol due to all symptoms and scales and observed no difference according to gpa classication . evaluation of the qol scores : changes after 3 months within and between groups in all , 63 patients completed the questionnaires at both time points . 
the response rate of 3 - month survivors was 63 of 67 ( 94% ) , including 32 of 37 patients treated with wbrt ( 87% ) and all 31 surviving patients treated with srt . 
whereas 79% of patients with wbrt suffered from appetite loss ( 20 points decrease ) , only 37% of patients with srt declared this high level . discussion studies on how the qol of patients with bm is affected by radiotherapy have been previously reported [ 8 , 38 , 44 ]  . nevertheless , this is one of the rst comparisons of qol effects between patients undergoing srt or wbrt for limited ( 13 ) bm using a brain - specic tool . in general , srt delivers a high dose of focal irradiation to the tumour while minimizing irradiation to healthy brain tissue . 
therefore , better cognitive function , qol , and local control results are expected after this treatment [ 19 , 21 ]  . at our study , most symptoms and domains showed signicant declines after three months in both the wbrt and srt groups . 
the differences were statistically signicant and clinically relevant mostly during the early follow - up period ( for global health status at 9 months , physical functioning at 8 weeks , cognitive functioning at 12 months , and fatigue at 8 weeks ) [ 34 ]  . 
investigated qol on the basis of the bn - 20 questionnaire and the qlq - c30 in patients with extensive disease small - cell lung cancer ( ed - sclc ) [ 33 ]  . 
 [ 22 ] compared srs alone with srs and wbrt to evaluate the theoretical benets of intracranial tumour control with adjuvant wbrt against its possible side effects using quality - adjusted life expectancy ( qale )  . 
in our study , qol after superior srt for bm did not elicit signicantly higher qol scores in most qol parameters as strahlenther onkol ( 2020 ) 196 : 4857 table 3 rate of patients experiencing deteriorations from baseline up to 3 months parameter wbrt n = 28 n = 27 total n = 55 global quality of life ( cid : 2 ) 20 points decrease emotional function ( cid : 2 ) 20 points decrease fatigue 20 points increase hair loss 20 points increase appetite loss 20 points increase wbrt whole brain radiotherapy , srt stereotactic radiotherapy calculated in the study of lester - coll et al . 
patients treated with srt reported better attention and memory function than patients treated with wbrt , although they also showed deterioration over time ( 6 weeks , 3 months and 6 months after rt )  . 
cognitive - deterioration - free survival was longer in patients assigned to srs than in patients assigned to wbrt , and cognitive deterioration at 6 months was less frequent in patients who received srs than in those who received wbrt [ 7 ]  . the study by chang et al . 
 [ 9 ] was terminated because the patients who received srt plus wbrt were signicantly more likely to show a decline in learning and memory function 4 months after rt than patients assigned to receive srs alone . 
 [ 4 ] detected steady deterioration in performance in the mini - mental status examination over time , but they did not detect a signicant group difference between patients treated with wbrt plus srs or srs alone . another main nding in our study was the difference in the score for future uncertainty over time according to treatment modality . 
stated that providing non - medical support for the aforementioned topics ( e.g. , handing out information , suggesting support groups , establishing connections with respective authorities , setting up appointments with social services , and assisting in dealing with insurance companies ) could improve qol and decrease distress [ 18 ]  . 
first , we have to consider that the reliability of patients declarations could be biased since follow - up qol questionnaires were not completed during a control visit but were returned by mail . therefore , we could not assess a patients general condition ourselves . 
additionally , completion of the questionnaires in the hospital was not observed . second , despite the multicentre study design , 67 survivors is a relatively small sample , reecting the difculty of studies in this eld . 
however , the return rate of the questionnaires was very high ( 94% ) compared to that in other studies [ 34 ]  . another signicant limitation is the lack of prior randomization . 
patients undergoing wbrt had lower kps scores , a higher rpa class , more corticosteroid use , more than one metastasis , and received postoperative radiotherapy . therefore , further studies with randomization are necessary . conclusion overall , the qol of patients with 13 brain metastases was negatively affected by wbrt and srt with respect to physical function , fatigue , appetite loss , nausea , drowsiness , hair loss , and itchy skmotor dysfunction , communication decits and leg weakness decreased signicantly only in patients treated with wbrt . 
gerstein for their good ideas in initiation and analysis of this study and helping to recruit patients . funding the study was supported by a foundation of the equal opportunities ofce of the medical school hannover . compliance with ethical guidelines conict of interest d . 
geinitz declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
at a median follow - up of 12 years ( range 216 years ) , local control ( lc ) , hearing capacity , trigeminal and facial nerve function , and toxicity were assessed . 
35 ( 73% ) patients were treated with srs alone , in the remaining 13 ( 27% ) patients , srs was performed as salvage therapy for recurrent or progressive tumors after previous microsurgery . 
although the median administered dose ( 16.5 gy ) was rather high , the only factor which signicantly inuenced late toxicity was koos tumor grade iiiiv . keywords vestibular schwannomas koos tumor grade radiosurgery late toxicity hearing preservation zwlfjahresergebnisse der linac - basierten radiochirurgie fr vestibularisschwannome zusammenfassung ziel bericht der langzeitergebnisse von 53 patienten mit vestibularisschwannomen ( vs ) , die sich in unserer einrichtung einer einzigen hochdosierten linac - radiochirurgie ( srs ) unterzogen haben . methoden insgesamt 48 ( 92% ) patienten waren fr klinisches und magnetresonanztomographie - ( mrt - ) ansprechen sowie fr sptere toxizitt auswertbar . 
nach einem medianen follow - up von 12 jahren ( spanne 216 jahre ) wurden die lokale kontrolle ( lc ) , die hrkapazitt , die trigeminusund die gesichtsnervenfunktion sowie die toxizitt bewertet . 
die hrkapazitt wurde nach der gardner - robertson - skala klassiziert , in der die patienten der klasse iii die funktion hrfhiges hren hatten . ( cid : 2 ) ernesto maranzano , md e.maranzano@aospterni.it 1 radiotherapy oncology centre , s . 
di joannuccio , 1 , 05100 terni , italy strahlenther onkol ( 2020 ) 196 : 4047 ergebnisse die mittlere srs - dosis betrug 16 , 5 gy ( spanne 1320 gy ) und das mittlere tumorvolumen 1 , 7 cm3 ( spanne 0 , 097 , 4 cm3 )  . 
es wurden 35 ( 73% ) patienten nur mit srs behandelt , in den verbleibenden 13 ( 27% ) wurde srs als salvage - therapie fr rezidivierende oder progressive tumore durchgefhrt . 
obwohl die mittlere verabreichte dosis ( 16 , 5 gy ) ziemlich hoch war , war der einzige faktor , der die spttoxizitt signikant beeinusste , der koos - tumorgrad iiiiv . schlsselwrter vestibularisschwannome koos - tumorgrad radiochirurgie spte toxizitt introduction vestibular schwannomas ( vs ) are benign tumors usually arising from a vestibular component of the vestibulocochlear nerve . 
hearing loss is the most common initial presenting symptom and is usually followed by tinnitus , disequilibrium , trigeminal nerve dysfunction , vertigo , headache , facial nerve dysfunction , and diplopia [ 2 ]  . treatment protocols range from observation to surgical resection ( generally microsurgery ) or radiosurgery ( srs ) [ 3 ]  . 
demonstrated that results of microsurgery and srs are comparable in terms of local control , but srs , which better preserves hearing function , should be considered the treatment of choice for vs of less than 3 cm in diameter [ 5 ]  . early reports have shown positive ( > 90% ) growth control rates with the use of high marginal doses ( 1520 gy ) , but at the expense of poor hearing and other cranial neuropathy outcomes [ 6 ]  . 
during the past couple of decades , many centers have reported equivalent tumor control with signicantly improved hearing preservation and neuropathy rates using lower doses ranging from 12 to 14 gy [ 7 ]  . 
many of these studies had limited follow - up [ 6 , 7 ] , and concerns remain about possible late relapses with these lower doses . moreover , the promising early hearing outcomes could not be maintained at a longer follow - up . the present analysis reports on results obtained in 53 patients with vs , treated with single high - dose srs in our institution . 
at a median follow - up of 12 years , our aim was to evaluate long - term treatment outcomes , focusing on local tumor control , hearing preservation , and late toxicity . materials and methods from our database we have retrospectively selected only patients with a potential follow - up period of 10 years . 
at the time of treatment , all cases were preliminarily discussed in a multidisciplinary meeting with a radiation oncologist , a neurosurgeon , and a neuroradiologist to dene the clinical indications . 
informed consent was obtained according to the rules of our institution . extension of the tumor was classied according to the koos categories : grade i , purely intracanalicular ; grade ii , extended into the cerebellopontine angle without brainstem contact and a maximum diameter of 20 mm ; grade iii , extended to cerebellopontine cistern without brainstem displacement ; grade iv , compressing the brainstem and displacing cranial nerves [ 8 ]  . 
thus , we dened serviceable hearing when patients were able to discriminate words ( i.e. , class i , good discrimination ; class ii , useful discrimination ) and non - serviceable hearing when patients were not able to discriminate words or could not hear at all ( i.e. , class iii , low ; class iv , poor ; and class v , no discrimination )  . 
patients strahlenther onkol ( 2020 ) 196 : 4047 with non - serviceable hearing were asked about their hearing ability after srs , and in case of reported improvement , audiograms were performed to better assess the response . facial function was graded using the housebrackmann scale ( grade i : normal function ; grade ii : mild dysfunction ; grade iii : moderate dysfunction ; grade iv : moderately severe dysfunction ; grade v : severe dysfunction ; grade vi : total paralysis )  . trigeminal nerve function was assessed by asking the patient about face pain / paraesthesia both before and after srs . 
the gross tumor volume ( gtv ) consisted of the radiographically evident contrast - enhancing gross disease in t1 - weighted sequences , and no expansion was added for the clinical target volume ( ctv )  . 
in this cohort of patients , the median administered dose was 16.5 gy ( range 1320 gy )  . generally , 8 mg of dexamethasone and h2 - antihistamines for gastric ulcer prophylaxis were given 1 h before and 12 h after treatment . 
the patients were followed up by a radiation oncologist and / or a neurosurgeon after treatment . mri of the brain was performed 4 months after srs and at 1 , 2 , and 3 years thereafter , and then every 23 years , or as clinically indicated for assessment of local tumor control . local control ( lc ) was dened in the case of disease stability ( no increase in tumor diameter ) or reduction of maximum tumor diameter . 
temporary tumor necrosis ( central tumor necrosis on mri with temporary increase in tumor size with or without new or worsened neurological symptoms ) not requiring surgical treatment was also considered lc . 
local failure was dened as permanent progressive tumor growth with associated symptoms requiring additional surgical treatment . the lc and treatment - related complications were calculated using the kaplanmeier method [ 10 ]  . 
variables that showed signicant values were further re - entered into a multivariate cox proportional hazard regression model to analyze the hazard ratio ( hr ) of potential prognostic indexes for these outcomes [ 11 ]  . 
of these 48 eligible patients , only two had fewer than 10 years of follow - up , both due to death for myocardial infarction , 2 and 6 years after srs . 
patients with serviceable hearing were offered surgery , but about half of them ( 23 , 48% ) preferred srs . consequently , 35 ( 73% ) patients underwent srs alone . 
in remaining 13 ( 27% ) patients5 ( 10% ) already submitted to a total resection and 8 ( 17% ) to a subtotal resectionsrs was performed as salvage therapy for recurrent or progressive tumor . regarding tumor extension , 11 ( 23% ) patients had koos grade i , 16 ( 33% ) grade ii , and 15 ( 31% ) and 6 ( 13% ) grades iii and iv , respectively . 
it is important to note that 9 of 21 patients with koos tumor grade iii and iv before srs had received prior microsurgery . strahlenther onkol ( 2020 ) 196 : 4047 table 1 characteristics of evaluable patients variable gender male female location right left n koos grade symptoms at presentation hearing loss trigeminal paraesthesias trigeminal pain facial nerve impairment tinnitus ataxia / disequilibrium hearing function serviceable non - serviceable prior surgery type of surgery total subtotal srs radiosurgery n ( % ) 24 ( 50 ) 24 ( 50 ) 20 ( 42 ) 28 ( 58 ) 11 ( 23 ) 16 ( 33 ) 15 ( 31 ) 6 ( 13 ) 44 ( 92 ) 4 ( 8 ) 2 ( 4 ) 7 ( 14 ) 8 ( 17 ) 10 ( 21 ) 23 ( 48 ) 25 ( 52 ) 13 ( 27 ) 35 ( 73 ) 5 ( 10 ) 8 ( 17 ) the majority of patients ( 44 of 48 , 92% ) presented hearing loss as an initial symptom and 25 ( 52% ) had nonserviceable hearing . 
ataxia / disequilibrium , tinnitus , and trigeminal paraesthesia were presenting symptoms in 10 ( 21% ) , 8 ( 17% ) , and 4 ( 8% ) patients , respectively . 
seven ( 15% ) patients had symptoms of facial nerve involvement at presentation . local tumor control after srs , lc of disease was obtained in 100% of cases . at last follow - up , 19 lesions ( 39% ) were stable and 25 ( 52% ) decreased in size with a partial ( 23 cases ) or complete ( 2 cases ) remission of disease . 
transient enlargement ( median 3 mm , range 24 mm ) due to central tumor necrosis with a gradual return to initial volume was observed in 3 ( 6% ) of 48 treated lesions . 
twenty - one ( 44% ) had stable symptoms , with mri showing stable disease ( 10 cases ) , transient enlargement due to central tumor necrosis ( 3 cases ) , or partial remission ( 8 cases )  . 
seventeen ( 35% ) worsened compared to their pretreatment symptoms , having a deterioration which was transient in 12 and persistent in 5 . hearing preservation hearing function was evaluated in the 46 ( 96% ) patients with a minimum follow - up of 10 years . 
the 23 ( 50% ) non - serviceable hearing patients were rated in the gardnerrobertson classes as follows : 13 ( 57% ) in class iii , 4 ( 17% ) in class iv , and 6 ( 26% ) in class v . 
no patients with non - serviceable hearing recovered useful function after srs , even though 2 patients improved their residual hearing function , passing from class iv to iii . of the 23 ( 50% ) patients with serviceable hearing , 2 ( 9% ) worsened from gardnerrobertson class ii to v , 6 and 12 months after srs ; 2 ( 9% ) patients improved from class ii to i ( the pure tone average increased from 50 to 20 db in one case , from 45 to 25 db in the other )  . 
median tumor size in serviceable - hearing patients , was 12 mm ( range 5.121 mm ) and median administered dose was 16.5 gy ( range 1420 gy )  . 
in this case , the tumor compressed the brainstem ( koos tumor grade iv ) , had a diameter of 20.9 mm , and received 14 gy . four ( 11% ) patients developed incomplete and intermittent ipsilateral facial nerve palsy which regressed in a median time of 6 months . 
they had koos tumor grade ii , iii and iv in 1 , 2 and 1 case , respectively , a median tumor volume of 3.3 cm3 , a median diameter of 18.4 mm , and received a median dose of 17 gy . before srs , 2 ( 4% ) vs patients had a typical trigeminal neuralgia ( one of them also had a trigeminal neuroma ) and 4 ( 8% ) a trigeminal paraesthesia . 
eleven ( 11 / 48 , 23% ) patients with koos tumor grade iii and iv , submitted to a median dose of 17.5 gy ( range 1717.5 gy ) , developed radiation - induced trigeminal toxicity within the rst 12 months after srs . 
in 6 patients , trigeminal toxicity was transient , in 4 patients , toxicity was classied as ctcae grade ii and remained mild / stable during follow - up , and in 1 patient toxicity was severe . 
growth rates for small lesions can be of 13 mm per year and hearing reduction can be observed between 40 and 60% with the wait - and - see strategy over time [ 14 ]  . the principal endpoint of the treatment is local control , possibly with minimal neurological impairment , especially in terms of hearing loss . 
preservation of serviceable hearing is reported to be higher after srs ( 3098% ) [ 15 , 17 , 18 ] than after surgery ( 3050% ) [ 13 , 15 , 16 ]  . 
a large italian experience was recently published by boari et al . , who treated 523 patients with gamma knife srs at a median margin dose of 13 gy ( range 1115 gy )  . 
the overall rate of preservation of functional hearing at the long - term follow - up was 49% , and other treatment - related complications were only a transient worsening of pre - existing symptoms [ 20 ]  . in the literature , there are only two studies on vs treated with linac - based srs with a long follow - up ( median 120 months ) [ 15 , 21 ]  . 
radiosurgery , which was given at a median dose of 13 gy ( range 1020 gy ) to the 80% isodose , resulted in a local control rate of more than 90% , with trigeminal and facial nerve late toxicities of about 20 and 5% , respectively . in our series , after a median follow - up of 12 years , vs patients treated with linac - based srs had an excellent tumor control rate ( 100% )  . 
more than one - half of the lesions ( 25 , 52% ) slowly regressed , 19 ( 39% ) remained stable , and 3 ( 6% ) had a transient enlargement . 
a reversible srs - induced facial nerve palsy was registered in 11% of cases , whereas srs - induced trigeminal toxicity was recorded in 23% cases , reversible in 13% and permanent in 10% . it is worthy of note that all patients who developed permanent trigeminal toxicity had larger tumors ( 18 mm ) and were treated with relatively high doses ( 16.5 gy ) , which can represent a population at a major risk of iatrogenic toxicity . 
starting from these considerations , it is reasonable to consider that in the presence of tumors with diameters of 18 mm , lower srs doses ( ( cid : 2 ) 13 gy ) should be prescribed to limit late toxicity . 
at a minimum follow - up of 3 years and using a median marginal dose of 13 gy , no radiation - induced brainstem or cranial nerve toxicity was observed , and tumor control was obtained in 90.7% of patients [ 22 ]  . 
in another trial including 270 vs strahlenther onkol ( 2020 ) 196 : 4047 patients treated with linac - based srs at a median prescribed dose of 12 gy ( range 1120 gy ) , srs resulted as feasible , with high tumor control and a considerable hearing preservation rate with a low toxicity prole [ 23 ]  . 
reported data on 557 vs patients of any koos grade treated with gamma knife srs alone or in combination with microsurgery at a median dose of 12 gy / 50% isodose . koos grade ( iiiiv versus iii ) signicantly inuenced the hydrocephalus risk ( p < 0.001 ) without impact on lc and hearing preservation . 
in accordance with fishers results [ 24 ] , our ndings are that srs is safe when vs does not have brainstem contact , whereas it could be associated with a higher risk of late side effects in patients with brainstem displacement or compression . 
regarding fsrt , several schedules have been reported , ranging from 4 to 30 fractions [ 2529 ]  . with fsrt , the radiobiological properties of repair provide a benecial risk prole also for larger - volume vs , with the possibility of obtaining a lc rate comparable to srs [ 15 , 30 , 31 ]  . conservative management can be recommended in asymptomatic patients , especially with smaller lesions . considering a growth dynamic between 1 to 3 mm per year , a wait - and - see approach with close clinical and imaging follow - up can be adopted as an alternative to treatment . generally , an active approach with microsurgery or srs in this asymptomatic population is questionable , in consideration of the possible iatrogenic hearing damage . 
however , even in the wait - and - see population , an overall meaningful decrease of hearing function has been reported in the elderly population [ 3236 ]  . 
usually , srs - induced hearing loss gradually develops over time during follow - up [ 18 , 3841 ] , and patients with good hearing have higher preservation rates than patients suffering from reduced hearing function [ 15 , 20 , 23 , 24 , 38 , 42 , 43 ]  . 
after a median prescribed dose of 12 gy and a median cochlear dose of 4.1 gy , hearing preservation rates were 49 , 24 , and 12% at 60 , 120 , and 180 months after treatment , respectively . 
authors concluded that age 65 years , large tumor volume 8 cm3 , and higher cochlear dose > 4.2 gy were unfavorable factors for hearing preservation [ 44 ]  . 
in our series , about one half of patients ( 23 , 48% ) had serviceable hearing , which worsened only in 2 ( 9% ) cases , obtaining a 10 - year hearing preservation rate of 91% . 
our data conrm the feasibility of srs in the treatment of vs , also in patients with serviceable hearing , with a high rate of hearing preservation . the main limitation of our study was the retrospective nature and the relatively low number of recruited cases . however , patients had a long follow - up ( median 12 years ) and were accurately monitored for response and toxicity using periodical mri , audiograms , and clinical evaluation of neurological functions . conclusion tumor control and hearing preservation after linac - based srs were excellent . 
although the median administered dose ( 16.5 gy ) was rather high , the only factor which signicantly inuenced late toxicity was koos tumor grade iiiiv . compliance with ethical guidelines conict of interest p . 
maranzano declare that they have no competing interests . ethical standards all procedures performed in this study involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
we now present the rst - in - patient treatment using ( crs / ra ) for vt in germany . methods a 78 - year - old male patient with dilated cardiomyopathy and signicantly reduced ejection fraction ( 15% ) presented with monomorphic vt refractory to poly - anti - arrhythmic medication and causing multiple implantable cardioverter - debrillator ( icd ) interventions over the course of several weeks , necessitating prolonged treatment on an intensive care unit . 
based on the evm , crs / ra with a single session dose of 25 gy ( 83% isodose ) was delivered to the vt substrate ( 8.1 cc ) using a c - arm - based high - precision linear accelerator on november 30 , 2018 . david krug and oliver blanck contributed equally . 
3 , 24105 kiel , germany 2 klinik fr innere medizin iii , kardiologie , abteilung fr elektrophysiologie und rhythmologie , universittsklinikum schleswig - holstein , kiel , germany institut fr pathologie , universittsklinikum schleswig - holstein , kiel , germany institut fr pathologie sektion fr hmatopathologie , universittsklinikum schleswig - holstein , kiel , germany strahlenther onkol ( 2020 ) 196 : 2330 results crs / ra was performed without incident and dysfunction of the icd was not observed . 
histopathologic examination of the heart as part of a clinical autopsy revealed diffuse brosis on most sections of the heart without apparent differences between the target area and the posterior cardiac wall serving as a control . conclusion crs / ra appears to be a possible treatment option for otherwise untreatable patients suffering from refractory vt and electrical stora relevant reduction in vt incidence and icd interventions was observed , although long - term outcome and consequences of crs / ra remain unclear . 
clinical trials are strongly warranted and have been initiated . keywords radioablation electrical storm structural heart disease catheter ablation arrhythmia introduction ventricular tachycardia ( vt ) that arises around myocardial scars can be treated by catheter ablation of the arrhythmia substrate if anti - arrhythmic drug treatment fails [ 13 ]  . catheter ablation was shown to improve the composite endpoints of death , the occurrence of vt storm , and the burden of implantable cardioverter debrillator ( icd ) shock intervention after 30 days compared to dose - escalated drug therapy [ 4 ]  . 
however , even after successful initial catheter ablation of vt , up to 50% of the patients experience disease recurrence within 6 months after treatment [ 5 ] and the short - term morbidity and mortality rate of the ablation procedures is not neglectable [ 6 ]  . 
both recurrence and toxicity rates , as well as the number of patients not eligible for catheter ablation due to comorbidities or location of the vt substrate , indicate that there is a need for alternative treatment approaches to treat patients with refractory vt . stereotactic body radiotherapy ( sbrt ) in a single session to the heart , also called cardiac radiosurgery ( crs ) or radioablation ( ra ) in the literature , may offer such an alternative , as it overcomes the general limitation of energy deposition problems of endocardial or epicardial ablation techniques [ 7 ]  . 
in 2012 , after a variety of exploratory animal studies [ 8 , 9 ] , the rst clinical crs / ra treatment of a patient with vt was performed in the usa ( reported in 2015 ) [ 10 ] , followed by a second case treated in 2014 in europe [ 11 ]  . 
the two patients received a single - fraction radiation dose of 25 gy to the vt substrate , as dened by electroanatomical voltage mapping ( evm ) , and showed only limited to no toxicity , with a marked reduction in vt burden and icd shock interventions after treatment . more recently , a group from st . 
louis reported on the use of crs / ra in a series of ve patients who either had recurrent vt after or were ineligible for catheter ablation [ 12 ]  . 
however , one patient with atrial brillation and several risk factors for thromboembolic events who did not receive anti - coagulants due to contraindications suffered a fatal stroke during follow - up [ 12 ]  . 
the subsequent clinical phase i / ii trial with 19 patients conrmed the initial results with a vt burden reduction of 75% or more in 89% of the patients , a reduction of dual anti - arrhythmic medication from 59 to 12% , a signicant improvement in quality of life , and a favorable overall survival at 1 year of 72% , with 10.5% of the patients developing a severe adverse event ( grade 3 ) in the rst 90 days after treatment [ 13 , 14 ]  . we now report the rst patient treatment of crs / ra for vt in germany . case description a 78 - year old male patient presented to the cardiology department with dilated cardiomyopathy with severely reduced left ventricular ejection fraction of 15% and reduced right ventricular function . 
furthermore , the patient had undergone clipping of the mitral valve due to severe mitral regurgitation in 2013 and he suffered from pulmonary hypertension and coronary heart disease with previous placement of two bare metal stents . 
due to impending global heart failure , the implantation of a coupled cardiac resynchronization and icd system was performed in 09 / 2018 . during the following period , the patient developed recurrent episodes of hemodynamically relevant vt with resulting anti - tachycardia pacing and icd shocks despite maximal anti - arrhythmic medication ( metoprolol 285 mg / day , amiodarone 400 mg / day , mexiletine 1200 g / day )  . 
the critical vt isthmus was identied in the interventricular septum close to the cardiac apex , but due to the extensive scar formation and the thickness of the myocardium , no catheter ablation was attempted . 
after thorough evaluation by the clinical ethics committee , all treatment options were discussed with the patient and he gave his informed consent for crs / ra . treatment for treatment planning , a 4d computed tomography ( 4d ct ) without contrast agent was performed on a somatom sensation open s64 ct scanner ( siemens healthcare gmbh , erlangen , germany ) using the varian real - time position management ( rpm ) respiratory gating system ( varian medical systems , palo alto , ca , usa )  . 
an electrocardiogram ( ecg ) - triggered ct with intravenous contrast agent performed prior to the evm procedure was co - registered to the planning 4d ct in order to clearly visualize the ventricle wall . 
using the information from the highresolution evm procedure and following interdisciplinary discussions between the involved specialists , the target area strahlenther onkol ( 2020 ) 196 : 2330 ( in analogy to the clinical target volume in oncological cases ) was delineated using different 3d views of various cardiac structures in the eclipse external treatment planning system ( version 13.7 , varian medical systems inc )  . to account for uncompensated breathing and cardiac motion , an internal target volume ( itv ) was created based on the ecg - triggered and the planning 4d ct . 
no vacuum bag or abdominal compression could be used due to the poor clinical condition of the patient . crs / ra was performed on november 30 , 2018 , under close cardiologic ecg monitoring and emergency team stand - by using a truebeam stx linear accelerator ( varian medical systems inc )  . 
the icd was kept on during the whole procedure without special reprogramming according to guidelines for 6 mev photon irradiation without the icd in the main beam line [ 16 ]  . 
apart from nausea and a single episode of vomiting which occurred during the transfer from the icu to the treatment room and several hours after the procedure , treatment was tolerated well , and other side effects were not noted . follow - up in the days following crs / ra , complete cessation of the ventricular arrhythmia was noted and the general condition of the patient improved signicantly , resulting in transfer to the general ward 6 days after treatment . 
coinciding with crs / ra , we noticed an increase in cardiac troponin - t ( from approximately 30 ng / ml to > 60 ng / ml ) as well as in nt - pro brain natriuretic peptide ( bnp ; from approximately 1500 ng / ml to > 8000 ng / ml )  . 
cardiac troponin - t returned to pre - interventional values of approximately 3035 ng / ml within a week while nt - pro - bnp remained elevated ( > 3000 ng / ml )  . 
besides the elevated cardiac enzymes and the initial nausea at the day of treatment , no other radiation - induced side effects were noted during short - term follow - up and echocardiography showed no further deterioration of left ventricular function . thirty - three days after crs / ra , the patient was transferred to a geriatric rehabilitation clinic . 
4 histopathologic examination of the posterior cardiac wall ( a ) and the cardiac radiosurgery target region ( b ) in the anterior septal region revealed extensive myocardial scarring ( white asterisk )  . 
a small area of fresh necrosis was identied in the cardiac radiosurgery target region ( c )  . the white bar corresponds to 200 m strahlenther onkol ( 2020 ) 196 : 2330 lar function , but the general condition of the patient further deteriorated . 
after thorough discussion of the limited therapeutic options , the family opted for best supportive care . the patient nally died on january 26 , 2019 , 57 days after crs / ra , due to sepsis - associated cardiac circulatory failure . a clinical autopsy was carried out and conrmed cardiac circulatory failure as the leading cause of death . 
the second crs / ra treatment in germany , a rescue procedure for a patient with an electrical storm from persistent ventricular brillation , has also been recently reported [ 19 ]  . 
in all cases reported up to this point [ 1013 , 1719 ] , ours included , a marked reduction in vt burden and hence necessary anti - arrhythmic medication , anti - tachycardia pacing , and icd shock therapy was noted after crs / ra with only mild [ 10 , 11 , 1719 ] or limited severe [ 12 , 13 ] treatment - related adverse events . 
mild nausea and a discrete increase in specic cardiac markers seem to be typical for this kind of treatment and volume and location of the target region [ 18 ]  . 
furthermore , crs / ra in patients with icds appears to be safe with 6 mev photons , even without reprogramming and with the icd turned on during treatment , as in our case . 
this is in agreement with current guidelines and recently published data [ 16 , 20 ]  . nevertheless , a discussion on the optimal indication and on the right outcome measures for crs / ra is important . 
in our case , the patient had no options for interventional treatment and his anti - arrhythmic medication was already maximized while he continued to experience vt - related icd interventions . 
his prognosis was limited by his severe heart failure ; however , he was not a candidate for heart transplant due to his age and the kidney tumor , and had declined placement of a left ventricular assist device . 
furthermore , mexiletine and amiodarone cause cardiodepressant effects in patients with severe left ventricular dysfunction , which may additionally lead to cardiac deterioration , drug - induced interactions , and signicant side effects . 
most patients treated with crs / ra so far had ischemic cardiomyopathy as the underlying structural heart disease ; however , the reported case series and the phase i / ii trial from st . 
whether crs / ra may play a role in the treatment of other cardiac arrhythmia , like atrial brillation [ 21 ] , remains doubtful [ 2224 ] , even though patients have already been treated [ 25 ]  . the main issue regarding crs / ra is the target volume denition and the underlying biological effects of the delivered dose . 
while this approach was practiced in the initial studies on crs / ra [ 10 , 11 , 18 ] , likely due to a cautious approach to this new procedure , the colleagues from st . 
they performed external electrocardiographic mapping of the induced vt and included the vt exit site as well as the myocardial scar as dened by available imaging ( contrast - enhanced mri or single - photon - emission ct ) into the target volume [ 12 , 13 ]  . results from a randomized controlled trial of catheter ablation in patients with vt have shown that ablation of the whole arrhythmogenic substrate may be superior to ablation of the clinical vt [ 26 ]  . 
however , it is not clear if this approach is applicable in the setting of crs / ra . there are inherent limitations of the external mapping technique [ 27 ] and evm systems in general [ 28 ]  . 
louis [ 12 , 13 ] recently analyzed their treated patients and found a decrease in the size of the target volume over time [ 14 ] , suggesting a learning curve in the target volume denition for crs / ra . 
in the end , only additional clinical data , benchmark studies , and a reliable transfer procedure of the evm data to the treatment planning systems will allow harmonization of crs / ra target volume denition . regardless , the mechanism of action and the time to effect of crs / ra is poorly understood . 
in our case , we also did not nd any clear evidence of a scar induced by the procedure , despite the clear reduction in vt burden , although the time from treatment to autopsy was limited in both cases . 
preclinical data showed that 2530 gy delivered to cardiac muscle tissue in a single fraction does not result in a quickly and clearly dened scar [ 22 , 23 ] , opposite to what was reported from previous animal studies [ 9 , 21 ] , and the actual effects of crs / ra at a cellular level on either healthy or already scarred myocardium remain unknown . 
the small region of necrosis found near the crs / ra target area in our patient was judged to presumably represent a reaction to regional prenal perfusion decits rather than a reaction to the crs / ra itself , especially with respect to the long latency between crs / ra and time of death , as well as the absence of any other obvious histomorphological changes . 
nevertheless , additional preclinical studies and systematic analytical approaches are needed to determine the effects of crs / ra at a cellular level . furthermore , the effect of treatment - related parameters , such as the actual treatment time ( i.e. , by the dose delivered to the target per timeframe ) [ 24 ] , which is inherently different between robotic - based [ 10 , 11 , 17 , 18 ] or c - armbased ( [ 12 , 13 , 19 ] ; our case ) linear accelerators is unknown . 
on the other hand , a difference in plan quality [ 29 , 30 ] and delivery accuracy [ 31 ] for complex moving targets cannot be noticed for high - end radiosurgery systems anymore , even though some recent crs / ra planning studies may have suggested this [ 32 ]  . 
robotic radiosurgery systems with tracking of the icd leads or gantry - based delivery with respiratory gating will most likely yield a lower cardiac dose exposure . we believe patients with structural heart disease , who suffer from refractory vt with recurrent icd interventions and are either ineligible for or have failed catheter ablation , to be ideal candidates for crs / ra and have initiated a multi - center clinical trial for those patients ( nct03867747 )  . 
the primary outcome measure for the radiosurgery for the treatment of refractory ventricular extrasystoles and tachycardia ( raventa - ) trial is safety , as there are only limited data on the toxicity of crs / ra today . 
secondarily , we will investigate the effects on vt burden , icd interventions , and quality of life , as we believe these to be the main clinical endpoints for future crs / ra trials to come [ 13 ]  . conclusion we report the rst clinical treatment of crs / ra for refractory vt in germany , demonstrating a quick reduction in vt burden with minimal side effects . 
long - term follow - up in clinical trials such as raventa is strongly warranted and a large number of open questions for the harmonization of crs / ra has been identied . acknowledgements the authors would like to thank annette rogge ( clinical ethics committee , kiel , germany ) for ethical counseling in the context of the treatment of the patient . compliance with ethical guidelines conict of interest d . 
the aim of this study was to investigate the mechanism of the oral epithelial differentiation process , during ir alone and in combination with ds treatment in the same mouse model . methods fractionated ir 5 3 gy / week was given to the snouts of mice over two weeks , either alone ( ir ) or in combination with daily ds treatment of 4 mg / kg ( ir + ds )  . 
their tongue was excised and subjected to immunohistochemical processing . results in the p16 analysis as a proliferation marker , the difference between ir alone and ir + ds in the germinal ( proliferation ) layer was not signicant , not stimulating the proliferation process . 
for the p21 analysis as a differentiation marker on the functional ( differentiation ) layer , the difference between ir alone and ir + ds arms was signicant , indicating that ds inhibited the differentiation process . 
radiation research for radiation oncology , applied and translational radiobiology , medical university / akh vienna , whringer grtel 1820 , 1090 vienna , austria 3 department of radiation oncology , faculty of medicine , dokuz eylul university , inciralti , 35340 izmir , turkey introduction oral mucositis is a frequent , often dose - limiting early adverse effect of head and neck cancer radio ( chemo ) therapy [ 1 , 2 ] , especially when the oral cavity and major salivary glands are in the radiotherapy treatment eld [ 3 ]  . 
stem cells physiologically divide into one new stem cell ( a self - renewstrahlenther onkol ( 2020 ) 196 : 8594 ing system ) and one non - stem daughter cell . 
the latter can , as a transit cell , undergo a limited number of cell divisions before terminal differentiation and loss at the surface [ 6 ]  . the cell production , either from stem cell proliferation or transit cell division , is limited to the basal layer and the deeper parts of the spinos layer ; these are depicted as a germinal layer ( stratum germinativum )  . 
during differentiation , cells increase in size and atten towards the supercial layer . a nely regulated differentiation program process is characterized by the sequential expression of different proteins , coincident with the phenotypic evolution from basal cell to the mature , nonviable stratum layer [ 8 ]  . 
murine oral mucosa presents as a multilayered squamous epithelium composed of a germinal layer , a functional layer , and a supercial layer , and is largely comparable to human oral mucosa [ 11 ]  . 
however , the molecular mechanisms governing mucosal differentiation are still largely unknown [ 8 ]  . typical early ir effects are found in turnover tissues , where physiologically permanent cell loss from the differentiated , post - mitotic compartments of the tissue is well balanced by proliferation in the germinal parts of the tissue [ 12 , 13 ]  . 
as a consequence of the proliferative impairment , the reduced cellular supply to the differentiated tissue layers results in progressive hypoplasia and , eventually , incomplete cell depletion [ 15 ]  . 
ds plays an important role in wound healing , like other glycosaminoglycans ( gag ) , and it binds to broblast growth factor ( fgf ) - 2 , which stimulates cell proliferation in response to injury [ 16 ]  . 
fgf - 2 has been reported to be connected to ds and activated by ds [ 17 ] , and it functions as a mitogen that signals mesenchymal cell migration , proliferation , and differentiation [ 5 ]  . 
therefore , both male and female mice were included in this study . mice were housed in a conventional environment with controlled temperature ( 22 2 c ) and humidity ( 55 10% ) and a day / night rhythm of 12 / 12 h . 
the animals were housed in makrolon cages , 1284l eurostandard type iil , with a oor area of 530 cm2 ( techniplast gmbh , hohenpeienberg , germany ) , maximum 5 animals per cage , on aspen wood bedding ( abedd - lab & vet - service gmbh , vienna , austria ) and had free access to standard diet ( sniffspezialditen - gmbh , soest , germany ) and freshwater ad libitum from standard perspex drinking bottles . 
the age of the mice at the onset of the experiments ranged from 8 to 12 weeks [ 11 ]  . irradiation technique and dermatan sulfate treatment the study comprises two experimental arms : daily fractionated ir alone and in combination with daily systemic administration of ds ( ir + ds ) ards was administered to the ir + ds group over two weeks , from day 3 to 11 , ir started at day 0 . 
in two - day intervals , groups of animals ( n = 3 ) were immobilized with 60 mg / kg pentobarbitone sodium , injected intraperitoneally , and were sacriced by neck dislocation . 
ir was performed with an x - ray device ( yxlon - y.tu320d03 , yxlon - international gmbh , hamburg , germany ) , with a voltage of 200 kv , a tube current of 20 ma , a focus size of 5.5 mm , and a beam lter of 3 mm beryllium ( be ) and 3 mm aluminum ( al )  . 
the unanesthetized animals were guided into plastic tubes ( inner diameter 2 cm ) and their snouts were positioned in the conical hole ( 10 mm ! 6 pm ) in a perspex block , which closed the front end of the tubes . 
additionally , the staining intensity , corresponding to the amount of protein expressed , was assessed semi - quantitatively with an arbitrary score from 0 ( no signal ) , 1 ( weak signal ) , 2 ( intermediate signal ) , to 3 ( strong signal )  . 
intra - observer variability was found to be negligible [ 20 ]  . statistics for statistical analysis , the spss 17 statistical software ( spss inc . , chicago , il , usa ) , for graphical representation , graphpad prism 5 ( graphpad software , inc . , ca , usa ) was used . 
the analysis of variance ( one - way anova [ analyis of variance ] ) was used to test for the signicance of a difference between the mean values of experimental arms . 
a p - value of < 0.05 was regarded as statistically signicant [ 20 ]  . results representative histophotographs of immunohistochemical staining for p16 , p21 , and ck in untreated control mucosa on day 0 and on day 14 are presented in fig . 
at two - day intervals , 3 animals were sacriced per experimental group , 3 untreated mice ( day 0 ) served as controls animals was positioned in a standardized way in the central beam of the ir device . 
the bodies of the animals were shielded by a 12 mm thick collimator plate consisting of lead equivalent mcp - 96 ( hek - medizintechnik , lbeck , germany )  . 
representative histophotographs of p16 - , p21 - , and ck - stained lower mouse tongue epithelia were taken on day 0 ( unirradiated and untreated controls ) and day 14 . 
the staining signal intensity was scored semi - quantitatively with an arbitrary score of 0 ( no signal ) , 1 ( weak ) , 2 ( intermediate ) , or a maximum of 3 ( strong )  . 
the staining signal intensity was scored semi - quantitatively with an arbitrary score of 0 ( no signal ) , 1 ( weak ) , 2 ( intermediate ) , or a maximum of 3 ( strong )  . 
the minimum values were as follows : for the ir - only arm 83.2% on day 14 and for the ir + ds arm 89.5% on day 0 and day 14 . 
staining intensity was signicantly higher in the ir + ds arm until the 10th day when compared with the ir - only arit was observed that the values strahlenther onkol ( 2020 ) 196 : 8594 fig . 
the staining signal intensity was scored semi - quantitatively with an arbitrary score of 0 ( no signal ) , 1 ( weak ) , 2 ( intermediate ) , or a maximum of 3 ( strong )  . 
there is no strong signicance between ir - only and ir + ds arms for total , germinal , and functional cell numbers . discussion oral mucositis refers to erythematous and painful ulcerative lesions of the oral mucosa observed in patients with head and neck cancer who are treated with chemoand / or radiotherapy [ 22 ]  . 
one of the basis mucosal protective property of ds anticoagulant activity , which increases blood support in areas where vascular structures are narrowed , is thought to reduce inammation [ 17 ]  . 
our study focused to observe effects of ds on radiation - induced oral mucositis and due to this aim immunohistochemical staining planned on cell proliferation marker ( p16 ) , cell differentiation marker ( p21 ) , and indicative of cellular skeletal integrity antibody fig . 
the activity of p16 in the phases of the cell cycle has been investigated , and it has been associated with the s - phase which indicates proliferation [ 25 ]  . 
in our study , p16 did not make a signicant difference in the germinal ( proliferation ) layer when the experimental arms compared . this supports the knowledge from the hertzendorfer et al . study that ds did not stimulate the proliferation process [ 19 ]  . 
p21 is involved in the process of terminal differentiation [ 26 ] and inhibits the activity of cyclin - dependent kinase which controls the transition from g1 to s - phase during the cell cycle [ 27 ]  . 
in our study , the percentage of p21 - positive cells decreased for the functional ( differentiation ) layer in the ds - applied arthe oral mucosal protective feature of ds is considered to inhibit the differentiation process by stimulating the junction . 
in this case , cells whose cellular differentiation is inhibited cannot escape from the layer in which they are located to the surface , and the number of cells before ir will be prevented by this effect . 
radiation induces damage to the epithelium , with the release of ck resulting in cell death and inhibition of basal cell proliferation [ 2931 ]  . these epithelial changes possibly lead to differential expression of ck in each phase [ 32 , 33 ]  . 
keratins are the predominant cytoskeletal protein of stratied keratinized epithelial cells and are the most sensitive markers of epithelial differentiation and proliferation [ 3436 ] , because their expression is both region specic and differentiation specic [ 37 ]  . 
observed that increased ck expression can be associated with the reactive proliferation of the epithelium and increasing resistance of the oral mucosa during the initial phases of ir [ 38 ]  . 
the results of our study for the percentage of ck - positive stained cells , the ds - applied arm strahlenther onkol ( 2020 ) 196 : 8594 superior to ir - only arm in both germinal and functional layers , which shows that ds supports mechanical strength at the cellular level . 
besides , when the signicance between germinal and functional layers is compared for each experimental arm , the effect of ds on the mechanism of inhibition of differentiation made a signicant difference in the functional ( differentiation ) layer in favor of the ir + ds arm . but still , the percentage of positive cells did not fall below the control group range of percentage of positive cells for either experimental arthis effect supports the positive activity of fractionated ir on junctions [ 20 ]  . 
investigated the effect of ds on breast cancer tumor cell samples instead of normal tissues and showed that ds often causes adverse effects on breast cancer cells , and high doses of ds lead to a decrease in breast cancer cell proliferation . 
the results of this study clearly demonstrated the complex role of ds in the cancer setting and revealed the anti - cancer potential of gag [ 39 ]  . conclusion dermatan sulfate inhibits differentiation by stimulating the junctions and supports mechanical strength at the cellular level and creates the integrity of the epithelial layer , while does not stimulate the proliferation . 
reported the anti - cancer potential of ds on breast cancer samples . the promising features of ds including the mechanisms of the mucosa - protective activity , anti - cancer potential , inhibition of differentiation and not effecting the proliferation could be examined on the head and neck tumour sections , via proliferation and differentiation markers for further research . compliance with ethical guidelines conict of interest n . 
niyazi1 , 3 received : 23 may 2019 / accepted : 11 september 2019 / published online : 4 october 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract background and purpose radiation necrosis is a possible adverse event after cranial radiation therapy and can cause severe symptoms , such as an increased intracranial pressure or neurological deterioration . 
the vascular endothelial growth factor ( vegf ) inhibitor bevacizumab ( bev ) has been shown to be a feasible therapeutic option for symptomatic radiation necrosis , either when traditional antiedematous steroid treatment fails , or as an alternative to steroid treatment . 
this retrospective monocentric case study evaluates patients who received bev due to radiation necrosis , with a specic focus on the respective clinical course . methods using the internal database for pharmaceutical products , all patients who received bev in our department were identied . 
patients who either improved in symptoms , received less dexamethasone after treatment , or both were considered to have a benet from the treatment . results twenty - one patients who received bev due to radiation necrosis were identied . 
in 14 patients ( 66.7% ) the dexamethasone dose could be reduced during therapy , 5 patients ( 23.8% ) received the same dose of dexamethasone before and after the treatment , and 2 patients ( 9.5% ) received a higher dose at the end of the treatment . 
patients seem to benet from this treatment by improving symptomatically or through reduction of dexamethasone . keywords stereotactic radiosurgery high - grade glioma antiedematous treatment vascular endothelial growth factor brain metastases ( cid : 2 ) med . 
symptoms of rn strahlenther onkol ( 2020 ) 196 : 7076 mostly consist of cephalgia , nausea , vertigo , seizures , or other area related neurological symptoms [ 4 ]  . the pathogenesis of rn has been well described by gonzalez et al . 
as a continuous process in which endothelial cell dysfunction leads to tissue hypoxia and necrosis , with the concomitant liberation of a vasoactive compound , such as the vascular endothelial growth factor ( vegf ) [ 5 ]  . 
vegf leads to a dysfunction of the bloodbrain barrier and therefore causes cerebral edema [ 4 ]  . so far , the primary treatment for rn consists of antiedematous drugs , such as dexamethasone or mannitol [ 7 ]  . 
alternatively , surgical decompression can also serve as an invasive but benecial palliative treatment option in well - selected cases when non - invasive treatments fail [ 7 , 8 ]  . 
in order for insurance companies to cover the costs of bev as a treatment for rn , this cost coverage must be applied for rst , by proving the treatments necessity for this individual patient . 
therefore , the diagnosis of rn must be secured and traditional treatment must have been tried previously . the indication for bev is symptomatic rn diagnosed either by biopsy or imaging , which usually consists of contrast media - enhanced mri or ( in selected cases and according to availability ) uoroethyl - l - tyrosine positron emission tomography ( fet - pet ) [ 10 , 11 ]  . 
differentiation between rn and progressive tumor is still a clinical challenge , since therapeutic approaches are dependent on the diagnostic validity [ 12 , 13 ]  . clinical experience with bev is still quite scarce . 
to support these data , real - life studies , which report on clinical experience with bev , are needed . this retrospective study analyzed all patients with cerebral radiation necrosis who were treated with bev at a single center . methods progressive tumor and rn often cannot be distinguished easily on follow - up mri following radiotherapy . 
as far as no response was seen or a steroid - refractory state was reached , the interdisciplinary tumor board assessed whether bev application could be an alternative treatment option . for data acquisition , the internal database for pharmaceutical products of the university hospital of munich , zenzy ( heni software , kirchzarten , germany ) , was searched for all patients who received bev . 
patients who received bev therapeutically , e.g. , as concurrent systemic therapy during reirradiation in recurrent malignant glioma , were excluded . general patient characteristics , treatment parameters for bev , and dosimetric data of the radiation therapy were derived from patient charts . 
the symptoms were graded using the ctcae version 5.0. all patients were graded regarding neurological symptoms ( 0 = no symptoms ; 1 = light symptoms ; 2 = moderate symptoms ; 3 = severe symptoms ; 4 = life - threatening symptoms ; 5 = death )  . 
overall , 11 patients ( 52.4% ) were irradiated for cerebral metastases , 7 ( 33.3% ) had the diagnosis of glioma , 2 ( 9.5% ) patients presented with a meningioma , and 1 patient ( 4.7% ) was treated for a nasopharyngeal carcinoma with brain invasion . 
concerning denistrahlenther onkol ( 2020 ) 196 : 7076 tive radiotherapy , 6 patients ( 28.6% ) were treated with conventional three - dimensional conformal radiotherapy ( 3dcrt ) ( mostly gliomas ) , 1 patient ( 4.7% ) with volumetric arc therapy ( vmat ) , 10 patients ( 47.6% ) with stereotactic radiosurgery ( srs ) , and 3 patients ( 14.3% ) with brachytherapy using iodine - 125 seeds . 
five patients received an additional rt prior to the rn ( 1 vmat , 2 srt , and 2 3drt ) and 1 patient received two additional rts ( both seeds )  . all patients received a bev dosage of 7.5 mg / kg every 3 weeks . 
the patient characteristics are presented in table 1 . in 10 patients ( 47.6% ) all symptoms improved , while 11 patients ( 52.3% ) did not improve symptomatically during treatment . 
symptomatic improvement was seen in 4 patients with symptoms of intracranial pressure ( 3 recovered completely ) , 5 patients with paresis ( 3 recovered completely , 2 only partially ) , and the patient with seizures ( no further seizures )  . 
nevertheless , in 14 patients ( 66.7% ) , the dexamethasone dose could be reduced during therapy , 5 patients ( 23.8% ) received the same dose of dexamethasone before and after the treatment , and 2 patients ( 9.5% ) received a higher dose after the end of bev treatment . 
concerning adverse effects , 2 patients ( 9.5% ) had an episode of epistaxis ( ctcae grade i and grade ii ) during bev therapy , one of whom was treated with electrocoagulation . 
the gray columns show the according subgroups of patients . bev bevacizumab , dex dexamethasone ( cid : 2 ) bev bevacizumab , rt radiation therapy , 3d - crt three dimensional conformal radiation therapy , vmat volumetric arc therapy benet through bev less dex ; improved symptoms same dex ; improved symptoms more dex ; improved symptoms less dex ; unchanged symptoms no benet through bev same dex ; unchanged symptoms strahlenther onkol ( 2020 ) 196 : 7076 fig . 
the red x in picture i indicates the isocenter , the blue dot in picture j indicates the dose reference point . the patient suffered from headache and vertigo and needed 12 mg dexamethasone / day at the time of diagnosis . 
after receiving four applications of bev she recovered from the symptoms receive a follow - up mri had a reduced performance status and received best supportive care without any further mr imaging . 
2. strahlenther onkol ( 2020 ) 196 : 7076 overall , 6 patients ( 28.6% ) received a further two cycles and 3 patients ( 14.3% ) received a total of four bev administrations . 
after these cycles , no patient received any further cycles similar to the patients in the trial of levin et al . , in which not more than four cycles were applied [ 9 ]  . 
in these hypoxic areas , the hypoxia - inducible factor - 1 ( hif - 1 ) is released and regulates the expression of pro - angiogenic factors , vegf being the most important one . 
the biological hypothesis of the exact effect is reduction of the vascular leakage by preventing vegf from reaching its vascular target and thus reducing the cerebral edema . due to this promising theoretical effect , bev has been tested in recent years in clinical practice . 
clinical evidence mostly consists of retrospective studies with small cohorts or non - randomized prospective studies or case reports . these , however , showed promising clinical and radiological improvements [ 5 , 1417 , 19 ]  . 
in contrast to our study , only patients with a karnofsky index of 60 or higher were included into the prospective study of levin et al . , which might explain the better overall outcome concerning clinical improvement . 
in contrast , the percentage of radiographic response was signicantly smaller in the present study ( 68.4% ; n = 19 ) than in comparable studies , as in sadraei et al . 
in this context , it is important to note that the incidence of rn is more frequent in patients treated with re - irradiation and that bev could possibly reduce this risk and result in a more favorable outcome . moreover , the inhibition of vegf could increase the radiosensitivity of the tumor cells and therefore lower the required radiation dose [ 23 ]  . 
was able to demonstrate that dexamethasone intake compromised overall survival in patients with glioblastoma undergoing radiochemotherapy and that bev did not have any inuence on overall survival , while having a good antiedematous effect [ 25 ]  . 
thus , bev might not only be of use for prophylactic or therapeutic treatment for radiation necrosis , but also for management of cerebral edema in general . while this study shows promising results , further data are needed to demonstrate an overall benet of bev in the treatment of radiation necrosis . 
in future , it might also be possible that drugs are able to target proteins which regulate vegf expression , like hypoxiainducible factor 1 - alpha ( hip - 1 ) or the vegf receptors , strahlenther onkol ( 2020 ) 196 : 7076 directly [ 18 ]  . 
but until then , bev seems to be a reasonable treatment option for rn . conclusion of all patients who received bev for the treatment of radiation necrosis , the majority had a clinical benet , either in terms of improvement of symptoms or a reduction of dexamethasone or both . 
in the context of the present experience and current data , bev might be offered as a treatment option to patients with symptomatic radiation necrosis . compliance with ethical guidelines conict of interest r . 
niyazi declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants or on human tissue were in accordance with the ethical standards of the institutional and / or national research committee and with the 1975 helsinki declaration and its later amendments or comparable ethical standards . 
here , we examined the impact of this treatment on patient quality of life and outcome . patients and methods forty - four patients with mycosis fungoides ( mf ) or sezary syndrome ( ss ) received 48 tsebt courses with a median dose of 12 gy within the past 8 years at our institute . 
patient and treatment characteristics for these cases as well as the impact of tsebt on quality of life and duration of response were retrospectively analyzed and compared . results the median modied severity - weighted assessment tool score before the start of tsebt was 44 . 
hier untersuchten wir den einuss dieser behandlung auf die lebensqualitt der patienten und das ergebnis . patienten und methoden vierundvierzig patienten mit mycosis fungoides ( mf ) oder szary - syndrom ( ss ) erhielten 48 tsebt - durchlufe mit mittlerer dosis von 12 gy an unserem institut . 
patientenund behandlungscharakteristika fr diese flle sowie der einuss von tsebt auf die lebensqualitt und remissionsdauer wurden retrospektiv analysiert und verglichen . ergebnisse der mittlere mswat - wert ( modied severity - weighted assessment tool ) vor dem start von tseb betrug 44 . 
patienten , die eine erhaltungstherapie erhielten , hatten lngere pfs ( p = 0 , 01 )  . schlussfolgerung die tsebt verbesserte die krankheitssymptome und die emotionalen bereiche der lebensqualitt von patienten mit mf oder ss . 
darber hinaus zeigen unsere ergebnisse , dass die erhaltungstherapie nach tsebt die pfs verbessern kann . schlsselwrter hautlymphom juckreiz lebensqualitt erhaltungstherapie immunity background cutaneous t cell lymphomas ( ctcls ) are a group of extranodal non - hodgkin lymphomas which originate from skin - homing cd4 + t lymphocytes . 
recently , low - dose total skin electron beam therapy ( tsebt ) has been applied to two types of ctclsmycosis fungoides ( mf ) and szary syndrome ( ss )  . the results of these treatments have been highlighted in prospective and retrospective studies [ 37 ]  . 
in addition to excellent response rates , low - dose tsebt regimens are associated with a minimal risk of adverse events in comparison to conventional radiation doses and systemic therapies [ 8 , 9 ]  . 
according to guidelines established by the european organisation for research and treatment of cancer ( eortc ) , maintenance treatment may improve treatment outcome , although randomized trials have not been conducted [ 13 ]  . 
assessment of health - related quality of life ( hrql ) is currently a standard procedure for patients with mf and ss , since these patients often experience a decrease in quality of life due to severe itching , infections , skin disguration , and psychological problems [ 1517 ]  . 
these symptoms can impact the families of mf and ss patients as well [ 15 , 17 ]  . here , we retrospectively examined the impact of lowdose tsebt on the hrql of mf / ss patients , as well as the impact of maintenance treatments after radiotherapy ( rt ) on outcome . 
we hypothesized that low - dose tsebt has the potential to improve quality of life for mf / ss patients . materials and methods a total of 48 low - dose tsebt courses were administered to 44 patients with mf or ss at our institution between 2011 and 2018 ( table 1 )  . 
treatment toxicities were assessed weekly during treatment periods and at the 4 - week follow - up appointment according to the common terminology criteria for adverse events , version 4 . pruritus was assessed with a visual analogue scale ( vas )  . evaluation of treatment response skin clinical response was assessed according to the modied severity - weighted assessment tool ( mswat )  . 
deftherapies table 2 therapies administered within 3 months after low - dose total skin electron beam therapy topical steroids bexarotene systemic chemotherapy ( methotrexate = 4 , gemcitabine = 2 , doxorubicine = 1 , chop = 1 , carmustine = 1 ) systemic steroids puva interferon novel agents ( zanolimumab = 1 , brentuximab = 1 , and vorinostat = 1 ) strahlenther onkol ( 2020 ) 196 : 7784 nosed with large - cell transformation and 7 / 40 ( 17% ) were diagnosed with folliculotropic mf . 
the median hemoglobin value was 12.7 g / dl ( range 9.616 ) and the median lactate dehydrogenase ( ldh ) value was 246 u / l ( range 78669 )  . 
the median absolute cd3 , cd4 , cd8 , cd19 , and natural killer ( nk ) cell counts were 896 cells / l ( range 5453940 ) , 620 cells / l ( range 663508 ) , 219 cells / l ( range 29582 ) , 105 cells / l ( 14309 ) , and 216 cells / l ( range 7411 , 968 ) , respectively . the median cd4 : cd8 ratio was 2.4 ( range 120 ) and the median duration of treatment was 19 days . n ( % ) 36 ( 75 ) 17 ( 35 ) 16 ( 33 ) 9 ( 19 ) 7 ( 15 ) 6 ( 12 ) 4 ( 8 ) 4 ( 8 ) 3 ( 6 ) 12 ( 25 ) chop cyclophosphamide , hydroxydauromycin ( doxorubicin ) , oncovin ( vincristine ) , prednisone ; puva psoralen and ultraviolet a ; ecp extracorporeal photopheresis clinical response to tsebt inition of response criteria , time to response ( ttr ) , and duration of response ( dor ) were in accordance with a recent consensus statement that denes clinical endpoints and response criteria for mf and ss cases [ 21 ]  . treatment technique all of the patients in our cohort were treated with a median dose of 12 gy ( range 624 gy ) that was delivered according to our modied six - dual - eld technique [ 22 ]  . 
univariate and multivariate analyses were performed with a cox regression model . results patient characteristics characteristics of the patients with mf or ss who received low - dose tsebt at our institution were examined ( table 1 )  . 
subgroup analyses identied an orr of 71% ( cr 14% ) for the cases with folliculotropic mf ( n = 7 ) , and an orr of 100% ( cr 50% ) for the mf patients with large cell transformation ( n = 8 )  . 
among the entire cohort , the median dor and pfs periods were 10 months ( 95% condence interval [ ci ] : 515 ) and 9 months ( 95% ci : 711 ) , respectively . 
approximately half of the patients developed grade 1 toxicities only ( 27 / 48 , 56% ) , while 17 / 48 ( 35% ) patients developed grade 2 toxicities and 5 / 48 ( 10% ) patients developed grade 34 adverse events . 
in addition , 5 ( 10% ) patients developed skin infections during rt and 1 ( 2% ) patient developed squamous cell carcinoma of the scalp 2 months after tsebt . 
1 kaplanmeier estimate of progression - free survival by maintenance therapy administration ( yes [ n = 36 ] versus no [ n = 12 ] ) two groups of patients . 
meanwhile , the results from the fact - g assessment showed a trend towards subjective improvement ( 7 15 ; p = 0.07 ) , with signicant improvements observed in the emotional domains ( p = 0.03 ) of the questionnaire after tsebt . 
in addition , a clinically meaningful difference in the social ( p = 0.08 ) , physical ( p = 0.13 ) , and functioning domains ( p = 0.14 ) were observed after tsebt . hematologic and immunogenic changes a total of 23 patients underwent regular posttherapeutic blood examinations . 
2 mean and 95% condence interval values of a dermatology quality of life index and b skindex - 29 scores prior to and after low - dose total skin electron beam therapy ( tseb ) strahlenther onkol ( 2020 ) 196 : 7784 ter development is not related to rt due to the relatively short interval after irradiation . discussion low - dose tsebt for mf / ss patients has been found to be a very effective modality , with an orr ranging from 8796% , a cr rate of approximately 35% , and a median interval to clinical response of 8 weeks [ 47 ]  . 
for patients with refractory or advanced - stage disease , higher radiation doses may be needed [ 23 ]  . it has previously been reported that conventional - dose tsebt ( i.e. , 30 gy ) combined with adjuvant therapies has provided clinical benets [ 6 , 14 ]  . 
in a prospective study conducted by morris et al . [ 7 ] , no signicant benet was observed when maintenance treatments after 12 gy tsebt were applied to 14 patients . 
this may be due to selection bias and differences in the treatments delivered ( i.e. , 5 patients received interferon alpha , 7 patients received bexarotene , and 2 patients received methotrexate )  . 
in contrast , maintenance / adjuvant treatments following low - dose tsebt in the present cohort were found to have a signicant impact on pfs , while also being associated with a trend toward longer dor . 
furthermore , low - dose tsebt was found to improve symptom burden according to hrql measures . to the best of our knowledge , the present analysis represents the rst demonstration of a hrql benet from lowdose tsebt . 
these results suggest that cd4 : cd8 ratio may represent a valuable biomarker to optimize radiation treatment decisions [ 26 ]  . currently , immunotherapy is gaining interest regarding its potential to prolong remission in previously treated patients [ 12 ]  . 
for example , in a prospective randomized trial , administration of the monoclonal antibody brentuximab vedotin improved the objective response rate for cd30 + mf patients compared to methotrexate and bexarotene [ 10 ]  . 
recently , immune checkpoint inhibitors have exhibited significant antitumor activity in patients with mf and ss with an orr up to 38% and a 1 - year pfs rate reaching 69% [ 11 , 25 , 27 , 28 ]  . in addition , iph4102 is an antibody which targets the killer cell immunoglobulin - like receptor 3dl2 ( kir3dl2 ) , which is aberrantly expressed in neoplastic cells of patients with ss and transformed mf [ 29 , 30 ]  . 
therefore , it is possible that a combination of radioimmunotherapy with a checkpoint inhibitor or vaccination may overcome counteracting immunosuppression mediated by tumor cells [ 23 , 32 , 33 ]  . 
allogeneic hematopoietic stem cell transplantation ( sct ) is another treatment option to consider for cases of mf and ss , and may provide a long - lasting effect despite a high risk of severe adverse effects . 
moreover , it is possible that tsebt could be used as a bridging therapy and for debulking prior to sct [ 2 , 13 , 34 , 35 ]  . there are several limitations associated with the present study . 
third , disease response was scored based on clinical examinations that were performed before and after each tsebt course , and this may have introduced bias into the observations associated with each case . 
therefore , the clinical effectiveness of the maintenance and adjuvant therapies and possible prognostic factors described in this study remain to be validated in large prospective trials . conclusion low - dose tsebt improved disease symptoms and emotional domains of hrql in patients with mf or ss . 
future studies are warranted to assess the efcacy of low - dose tsebt in combination with other novel immunotherapies to enhance the clinical benets . author contribution ke was involved in formal analysis , research methodology , and rst manuscript drafting . 
ethical approval : all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
februar 2020 der / die autor ( en ) 2020 hintergrund die direkt postoperative ( adjuvante ) radiotherapie der prostataloge bei postoperativem psa ( prostataspezisches antigen ) im nullbereich , aber vorhandenen risikofaktoren wie r1 und / oder t3 ist zur verbesserung der biochemischen kontrolle eine evidenzgesicherte behandlungsoption beim lokalisierten prostatakarzinom nach radikaler prostatektomie [ 13 ]  . 
frher salvage - radiotherapie nach radikaler prostatektomie vorgestellt : die radicals - studie ist eine randomisierte phase - iii - studie , die eine direkte adjuvante radiotherapie mit einer berwachung und frhen salvageradiotherapie im falle eines psa - rezidivs nach radikaler prostatektomie vergleicht . 
die artistic - metaanalyse analysiert neben den radicals - daten noch die daten der vergleichbaren studien raves und getug - afu 17 . methoden radicals - rt patientengut ( nct00541047 ) ist eine randomisierte phase - iii - studie , die 1396 patienten mit postoperativem psa ( cid : 2 ) 0 , 2 ng / ml und mindestens einem risikofaktor ( pt3 / 4 , gleasonscore 710 , positive resektionsrnder oder properatives psa 10 ng / ml nach radikaler prostatektomie ) einschloss . mnner wurden nach dem zufallsprinzip der adjuvanten radiotherapie der prostataloge oder einer berwachung mit einer frhen salvage - radiotherapie der prostataloge im falle eines psa - rezidivs ( psa 0 , 1 ng / ml oder 3 aufeinanderfolgende anstiege ) zugeteilt ( berwachungsarm )  . 
der primre endpunkt war fernmetastasenfreiheit , wobei die studie so angelegt war , eine berlegenheit der adjuvanten radiotherapie von 90 auf 95 % nach 10 jahren festzustellen . das biochemische progressionsfreie berleben , die abwesenheit einer antihormonellen salvage - therapie und die behandlungstoxizitten sind sekundre endpunkte , welche die autoren krzlich auf der esmo - 2019 - konferenz prsentierten . 
in der studie wurde nach gleason - score , resektionsstatus , rt - schema ( 52 , 5 gy / 20 f , 66 gy / 33 f ) und strahlenther onkol ( 2020 ) 196 : 406409 zentrum stratiziert und die patienten zwischen oktober 2007 und dezember 2016 in grobritannien , dnemark , kanada und irland rekrutiert . die artistic - collaboration - metaanalyse umfasste drei randomisierte studien , welche jeweils eine adjuvante radiotherapie der prostataloge mit einer berwachungsstrategie und einer frhen salvage - radiotherapie der prostataloge im falle eines psa - rezidivs bei mnnern nach radikaler prostatektomie verglichen : radicals ( isrctn40814031 ) , getug - afu 17 ( nct00667069 ) und raves ( nct00860652 )  . 
primrer endpunkt war das ereignisfreie berleben , wobei fr die ravesstudie nur die biochemische kontrolle als endpunkt vorlag . ergebnisse in der radicals - studie erhielten 93 % ( 649 / 697 ) der mnner in der adjuvanten behandlungsgruppe ihre radiotherapie innerhalb von 5 monaten . 
66 % prozent ( 166 / 649 ) der mnner in der adjuvanten behandlungsgruppe und 31 % ( 71 / 228 ) der mnner im berwachungsarm erhielten eine zustzliche antihormonelle therapie . nach einer medianen nachbeobachtungszeit von fnf jahren betrug das biochemische progressionsfreie berleben in der adjuvanten bestrahlungsgruppe 85 % und 88 % im berwachungsarm ( hazard ratio [ hr ] 1 , 10 ; 95 % - kondenzintervall [ ki ] 0 , 811 , 49 ; p = 0 , 56 )  . 
das biochemische progressionsfreie berleben nach 5 jahren in der adjuvanten bestrahlungsgruppe betrug 85 % im vergleich zu 88 % im berwachungsarm ( hr 1 , 10 ; 95 % - ki 0 , 811 , 49 ; p = 0 , 56 )  . 
radiotherapie und 94 % im berwachungsarm ( hr 1 , 24 ; 95 % - ki 0 , 762 , 01 ; p = 0 , 39 )  . die von den patienten selbstberichtete ( patient - reported outcomes ) harninkontinenz war nach einem jahr mit 5 , 3 % der patienten nach adjuvanter radiotherapie ausgeprgter als mit 2 , 7 % im berwachungsarm ( p = 0 , 008 )  . 
bei 8 % der adjuvant bestrahlten patienten und bei 5 % der patienten im berwachungsarm ( p = 0 , 03 ) wurde eine harnrhrenstriktur ( grad 3 / 4 ) nach rtog - kriterien festgestellt , wobei der gesamte nachbeobachtungszeitraum bercksichtigt wurde . 
fr die beurteilung des gesamtberlebens und des primren studienendpunkts freiheit von fernmetastasen ist eine lngere nachuntersuchung erforderlich , sodass diese daten noch ausstehen . die ergebnisse der artistic - metaanalyse basieren auf allen 2151 mnnern , die in den drei studien eingeschlossen wurden , von denen 1074 einer adjuvanten radiotherapie zugefhrt wurden und 1077 mnner eine berwachung mit frher salvage - radiotherapie im falle eines psa - anstiegs erhielten . 
die mediane nachbeobachtungszeit betrug 4761 monate . basierend auf 245 ereignissen ergaben sich in der metaanalyse keine hinweise darauf , dass eine adjuvante radiotherapie das ereignisfreie berleben verbessert im vergleich zur berwachung mit frher salvage - radiotherapie ( hr 1 , 09 ; 95 % - ki 0 , 861 , 39 ; p = 0 , 47 )  . 
der potenzielle absolute unterschied im ereignisfreien berleben nach 5 jahren betrug 1 % zugunsten des berwachungsarms . schlussfolgerung der autoren radicals erste ergebnisse der radicals - rt - studie zeigen keinen vorteil fr die adjuvante radiotherapie nach radikaler prostatektomie , wobei das risiko von urogenitalen nebenwirkungen nach adjuvanter radiotherapie erhht ist . 
lngere nachbeobachtungszeiten sind zur beurteilung des fernmetastasenfreien gesamtberlebens notwendig . eine berwachungsstrategie mit frher salvage - radiotherapie im falle eines psa - anstiegs wird als standardbehandlung nach radikaler prostatektomie empfohlen . artistic diese metaanalyse legt nahe , dass eine berwachungsstrategie mit frher salvage - radiotherapie bzw . 
fr eine metaanalyse des metastasenfreien berlebens ist eine lngere nachbeobachtung erforderlich . kommentar da die radikale prostatektomie bei den meisten patienten mit lokalisiertem prostatakarzinom die primrbehandlung darstellt , wird eine postoperative radiotherapie nach prostatektomie , entweder adjuvant aufgrund von risikofaktoren oder als salvage - radiotherapie bei persistierendem oder steigendem psa , huger durchgefhrt als eine primre strahlentherapie der prostata . 
allerdings liegen im 408 strahlenther onkol ( 2020 ) 196 : 406409 vergleich fr die postoperative situation deutlich weniger ergebnisse von randomisierten studien vor . die erfolgreiche durchfhrung der studien radicals , getug - afu 17 und raves ist eine beachtliche leistung der jeweiligen studienteams und erlaubt den ersten prospektiven , randomisierten vergleich der behandlungsergebnisse nach einer adjuvanten radiotherapie verglichen mit einer berwachungsstrategie mit frher salvage - radiotherapie nach radikaler prostatektomie . 
die histologische aufarbeitung der operationsprparate der patienten in der grten randomisierten studie zur adjuvanten radiotherapie ( eortc 22911 ) identizierte einen positiven resektionsrand ( r1 ) als wichtigsten parameter zur vorhersage eines gnstigen ansprechens ( bessere biochemische kontrolle ) nach adjuvanter radiotherapie [ 10 ]  . 
histopathologischen kriterien zur risikoabschtzung mglicherweise sinnvoll ergnzen . fazit wenn es nach prostatektomie ohne weitere therapie zu einem psa - rezidiv kommt , scheinen die patienten keinen nachteil davon zu haben , wenn erst dann eine frhe salvage - radiotherapie vorgenommen wird anstatt einer direkten adjuvanten radiotherapie . 
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wiegel t , bartkowiak d , bottke d et al ( 2015 ) prostate - specic antigen persistence after radical prostatectomy as a predictive factor of clinical relapse - free survival and overall survival : 10 - year data of the aro 96 - 02 trial . 
van der kwast th , bolla m , van poppel h et al ( 2007 ) identication of patients with prostate cancer who benet from immediate postoperative radiotherapy : eortc 22911 . 
bottke d , golz r , strkel s et al ( 2013 ) phase 3 study of adjuvant radiotherapy versus wait and see in pt3 prostate cancer : impact of pathology review on analysis . 
abdollah f , suardi n , cozzarini c et al ( 2013 ) selecting the optimal candidate for adjuvant radiotherapy after radical prostatectomy for prostate cancer : a long - term survival analysis . 
zhao sg , chang sl , spratt de et al ( 2016 ) development and validation of a 24 - gene predictor of response to postoperative radiotherapy in prostate cancer : a matched , retrospective analysis . lancet oncol 17 ( 11 ) : 16121620 . 
giordano1 elena sperk1 received : 13 july 2019 / accepted : 23 september 2019 / published online : 22 october 2019 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose to investigate long - term oncological outcome and incidence of chronic side effects in patients with breast cancer and intraoperative radiotherapy given as an upfront boost ( iort boost )  . methods retrospective analysis of 400 patients with an iort boost with low - energy x - rays ( 20 gy ) , subsequent whole - breast irradiation ( 4650 gy ) , and annual oncological follow - up . 
side effects scored grade 2 at least three times during follow - up were judged to be chronic . results the median age was 63 years ( 3085 ) and the median follow - up was 78 months ( 2180 ) after iort boost . 
side effects were similar or less than expected from an external beam boost . conclusion iort boost appears to be a highly efcient and safe method for upfront delivery of the tumor bed boost in high - risk breast cancer patients . keywords intraoperative radiotherapy ( iort ) side effects toxicity sequela fibrosis langzeitergebnisse nach intraoperativem boost bei brustkrebs zusammenfassung ziel untersuchung der onkologischen ergebnisse in der langzeitnachsorge und der hugkeit chronischer nebenwirkungen bei patientinnen mit brustkrebs , die eine intraoperative strahlentherapie als vorgezogenen boost ( iort - boost ) erhielten . methoden retrospektive analyse von 400 patientinnen mit iort - boost mit niederenergetischen rntgenstrahlen ( 20 gy ) , anschlieender ganzbrustbestrahlung ( 4650 gy ) und einer jhrlichen onkologischen nachsorge . 
nebenwirkungen mit einer bewertung von grad 2 , die mindestens dreimal whrend der nachbeobachtung auftraten , wurden als chronisch eingestuft . ( cid : 2 ) elena sperk , md elena.sperk@umm.de 1 university medical center mannheim , medical faculty mannheim , department of radiation oncology , heidelberg university , theodor - kutzer - ufer 13 , 68167 mannheim , germany 2 university medical center mannheim , medical faculty mannheim , department of gynecology and obstetrics , heidelberg university , mannheim , germany 3 university medical center freiburg , freiburg , germany 350 strahlenther onkol ( 2020 ) 196 : 349355 ergebnisse das mediane alter betrug 63 jahre ( spanne 3085 jahre ) und die mediane nachsorgezeit 78 monate ( spanne 2180 monate ) nach iort - boost . 
die kumulativen errechneten raten fr eine chronische fibrose lagen bei 19 , 1 % und 21 , 1 % nach 5 und 8 jahren , fr chronische schmerzen bei 8 , 6 % nach 4 jahren , fr ein chronisches brustdem bei 2 , 4 % nach 2 jahren , fr ein chronisches lymphdem des arms bei 0 , 0 % nach 5 und 10 jahren und fr eine chronische hyperpigmentierung bei 0 , 5 % nach 2 jahren . 
die ausprgung an nebenwirkungen war hnlich oder el geringer aus als die erwarteten effekte nach einem perkutenen boost . schlussfolgerung der iort - boost scheint eine hochefziente und sichere methode fr einen vorgezogenen boost des tumorbetts bei hochrisikopatienten mit brustkrebs zu sein . schlsselwrter intraoperative strahlentherapie ( iort ) nebenwirkungen toxizitt sptkomplikation fibrose introduction breast - conserving surgery ( bcs ) followed by externalbeam radiotherapy ( ebrt ) of the breast ( whole - breast irradiation [ wbi ] ) with an additional radiation dose applied to the tumor bed ( boost ) [ 4 , 9 , 27 ] is considered the current standard - of - care therapy for breast cancer patients with risk factors . 
wbi may be applied in a hypofractionated fashion with doses exceeding 2.0 gy per fraction ( usually up to total doses of 40 gy ) or as normofractionated radiotherapy with daily doses of 1.82.0 gy ( up to 50 gy total dose )  . 
as most local recurrences arise in close proximity to the tumor bed [ 12 ] , patients exhibiting specic risks for local recurrence should receive a boost to the tumor bed . 
classical modalities of tumor bed boosting include sequential ebrt boost with 2 gy per fraction up to 1016 gy , simultaneous integrated boost during wbi , brachytherapy ( in multichannel catheter or balloon technique ) , or as intraoperative radiotherapy ( iort ) with low - energy x - rays or electrons . current results of 1879 cases treated with electron , photon , or brachytherapy boost and a median follow - up of 13.1 years showed no difference in recurrence rates between the three techniques [ 14 ]  . the boost to the tumor bed decreases the risk of local recurrence [ 4 , 8 , 21 ] but increases the risk for side effects without improving overall survival [ 13 ] , likely due the high efcacy of salvage therapies . 
nevertheless , recurrence also occurs after boosting and it has been discussed whether or not the classical practice of landmark - oriented application ( e.g. , boosting the scar ) weeks after surgery may pose a risk for a geographical miss of the tumor bed [ 5 ]  . delivery of an upfront boost by the use of iort ( iort boost ) reduces the risk of a geographical miss and bridges the gap between surgery and wbi [ 24 ]  . 
compared to classical sequential boosting , iort boost reduces the overall treatment time ( usually by 8 fractions ) and is able to spare dose to organs at risk such as heart or lung [ 2 ]  . 
an eligibility analysis showed that up to 65% of all breast cancer patients could be offered an iort boost [ 20 ] , underlining the need for robust outcome data for this modality . 
to date , most studies on iort boost focused on local recurrence and acute / late side effects that occurred up to 5 years , while there are no reports on long - term ( > 10 years ) effects [ 6 , 7 , 10 , 1517 , 22 , 23 , 25 , 26 ]  . we here present the rst long - term data ( up to 15 years after iort boost ) on side effects and oncological outcomes in a representative cohort of patients who underwent iort boost with low - energy x - rays . methods cohort between february 2002 and september 2014 , 400 consecutive patients with breast cancer with a diameter up to 3.5 cm from one center were treated with upfront iort boost followed by wbi . 
all patients gave informed consent for analysis and publication of relevant data and all analyses were performed in accordance with the approval of the local irb . surgery , iort , wbi following routine surgery and margin diagnosis using frozen sections ( no ink on tumor ) , iort was applied using a mobile low - energy x - ray system ( intrabeam , carl zeiss meditec ag , oberkochen , germany ) , with a median dose of 20 gy prescribed to the applicator surface . 
in 26 patients , a lower dose was applied ( 12 gy ) , either due to a skin / applicator distance < 1 cm or due to other technical issues . 
the applicator sizes ranged from 25 to 50 mm , with outcome after iort boost in breast cancer table 1 tumor characteristics ( n = 400 treated with iort boost ) tumor size 0 mm 15 mm 610 mm 1115 mm 1620 mm 2125 mm 2630 mm > 30 mm missing tumor stage missing lymph nodes missing 2 ( 0.5% ) 7 ( 1.75% ) 73 ( 18.25% ) 122 ( 30.5% ) 90 ( 22.5% ) 80 ( 20% ) 14 ( 3.5% ) 7 ( 1.75% ) 5 ( 1.25% ) 2 ( 0.5% ) 292 ( 73% ) 105 ( 26.25% ) 1 ( 0.25% ) 302 ( 75.5% ) 75 ( 18.75% ) 17 ( 4.25% ) 5 ( 1.25% ) 1 ( 0.25% ) metastasis histology invasive - lobular mucinous spindle - shaped invasive - tubular medullary adenoid - cystic grading g23 missing margins missing 396 ( 99% ) 4 ( 1% ) 282 ( 70.5% ) 96 ( 24% ) 8 ( 2% ) 1 ( 0.3% ) 6 ( 1.5% ) 6 ( 1.5% ) 1 ( 0.3% ) 65 ( 16.25% ) 232 ( 58% ) 88 ( 22% ) 2 ( 0.5% ) 13 ( 3.25% ) 377 ( 94.25% ) 10 ( 2.5% ) 13 ( 3.25% ) her2neu missing positive negative missing positive negative missing invasion of lymphatic vessels missing invasion of blood vessels missing 180 ( 45% ) 128 ( 32% ) 33 ( 8.25% ) 57 ( 14.25% ) 2 ( 0.5% ) 349 ( 87.25% ) 50 ( 12.5% ) 1 ( 0.25% ) 324 ( 81% ) 74 ( 18.5% ) 2 ( 0.5% ) 294 ( 73.5% ) 91 ( 22.75% ) 15 ( 3.75% ) 284 ( 71% ) 11 ( 2.75% ) 105 ( 26.25% ) nst no special type ; r resection margin ; er estrogen receptor ; pr progesteron receptor ; l lympatic vessel invasion ; v vessel invasion treatment times between 18 and 48 min , depending on the size of the applicator . 
wbi was performed according to the local standard , with a total dose to the whole breast of 4650 gy and conventional fractionation ( 2 gy per fraction ) using standard linear accelerators . in 16 patients , doses needed to be modied ( 4456 gy ) for various reasons . follow - up assessment of side eects side effects of the radiotherapy were scored using the late effects in normal tissuessubjective , objective , management , and analytic scales ( lent - soma ) [ 1 ] , with slight modications for telangiectasia and retraction ( dened as present or absent , with no differentiation in grades )  . 
side effects that were scored at least three times during the whole period of follow - up per patient were dened as chronic and were dated by the rst time they appeared for analysis using the kaplanmeier method . 
all statistical analyses were done with spss version 24 ( ibm , armonk , ny , usa )  . during the rst 2 years of follow - up , all patients were followed every 6 months . 
mammography and ultrasound as well as a standard clinical examination were part of follow - up assessments . oncological outcomes results cohort any tumor arising within a distance of 2 cm to the tumor bed was dened as a local recurrence . 
survival data were also collected , whereas absolute and estimated incidence rates of events were calculated using the kaplanmeier method . the median age at the time of iort boost was 63 years ( range : 3085 years )  . 
this cohort of patients was not a lowrisk group , with about a quarter of patients with lesions > 2 cm , grade 3 , or node positivity , and about a third needing chemotherapy ( table 1 )  . 
1 kaplanmeier curves for ( a ) local recurrences after iort boost and ( b ) all ipsilateral in - breast recurrences ( local and secondary ipsilateral breast tumor recurrences ) after iort boost . 
2 kaplanmeier curves for overall survival after iort boost at a median follow - up of 78 months ( 2180 months ) , we detected a total of 15 local and 4 ipsilateral axillary recurrences . 
3 estimated incidence rates for chronic higher - grade brosis after iort boost non - breast cancer - related reasons ( abscess , recurring mastitis , sarcoma , high - grade brosis , and prophylactic mastectomy after detection of a brca mutation ) , and 1 patient due to an unreported reason . 
scar retractions , regardless of whether this was caused by surgery or radiotherapy , occurred in roughly one third and telangiectasia in 10% of patients ( data not shown )  . discussion breast cancer is the most common cancer in women and is usually treated with breast - conserving surgery followed by radiotherapy . 
previous analyses of a smaller cohort with shorter follow - up suggested a low incidence of local recurrence and promising survival rates after upfront iort boost [ 6 , 25 ]  . 
we here report on the outcomes of a much larger collective with long - term follow - up . we saw low rates of local recurrences , secondary breast cancers , axillary recurrences , and metastasis , which consequently resulted in an overall survival rate of 81% at 354 strahlenther onkol ( 2020 ) 196 : 349355 15 years . 
our data thus compare well to the largest prospective trial to date on the outcome after external - beam boosting performed by the eortc , known as the boost vs . 
showed no local recurrences or deaths after iort boost in 55 patients , although the median follow - up was only 40 months [ 7 ]  . similar efciency was seen in trials evaluating iort boost with electrons , although all of these trials included patients with no to only few risk factors . 
the local control rate in a pooled analysis of 1109 patients performed by the isiort ( international society for intraoperative radiotherapy ) was 99.2% ( the median follow - up was 72.4 months ) [ 11 ]  . 
trials with more mature follow - up revealed local recurrence rates of 4% at a median follow - up of 9 [ 18 ] and 6 years [ 28 ]  . we saw the majority of side effects ( especially breast edema , hyperpigmentation , telangiectasia ) as well as pain arising during the rst 3 years after iort boost . 
the most commonly observed chronic side effects in our cohort were brosis and pathe estimated incidence rate of moderate to severe ( grade 2 ) brosis after iort boost reached a maximum of roughly 20% at 10 years , which is slightly superior to the incidence of moderate / severe brosis after external - beam boost performed in the eortc trial ( 28.1% at 10 years ) [ 3 , 4 ]  . with all limitations of a retrospective analysis , iort boost with low - energy x - rays appears to be an efcient and safe method for boost delivery in high - risk breast cancer patients . conclusion acknowledgements the authors thank all patients and families participating in this study . 
study endpoints were efcacy of this fractionation in terms of local control ( lc ) , overall survival ( os ) , toxicity , and prognostic factors affecting os and lc . results between february 2010 and december 2016 , we enrolled 202 patients , with a total of 268 unresectable liver metastases . 
selection of cases may improve survival and lc . keywords hepatic metastases radiotherapy stereotactic ablative radiotherapy ablation oligometastases rolle von stereotaktischer krperbestrahlungstherapie in der behandlung von lebermetastasen : klinische befunde und prognostische faktoren zusammenfassung zielsetzung bewertung von durchfhrbarkeit und wirksamkeit von sbrt ( stereotactic body radiation therapy ) , fr nichtresezierbare lebermetastasen bei oligometastatischen patienten . methoden oligometastatische patienten mit bis zu 3 lebermetastasen mit einem maximalen durchmesser von 6 cm wurden mit sbrt behandelt . 
eine fallauswahl kann die berlebensrate und die lc verbessern . schlsselwrter lebermetastasen strahlentherapie stereotaktische ablative strahlentherapie ablation oligometastasen introduction oligometastatic disease is an intermediate stage between absence of metastases and systemic dissemination [ 1 ]  . 
according to recent literature , oligometastatic patients are characterized by up to 5 metastases at 13 sites , all suitable for ablative treatment [ 2 ]  . the liver is one of the sites more often affected by metastases from solid malignancies . 
colorectal cancer ( crc ) is one of the most frequently occurring tumors with solitary or oligometastatic liver disease [ 3 , 4 ]  . in crc liver metastasis , the introduction of polychemotherapy has increased response rates and median overall survival ( os ) to 4057% and 1520 months , respectively [ 5 ]  . 
afterwards , surgical resection of liver metastases improved os , with 1and 5 - year os rates of 9095% and 3060% , respectively , and with a median os of 4053 months [ 69 ]  . 
the role of surgery of non - crc liver metastases is controversial : some papers have shown a better prognosis only in a subgroup of neuroendocrine metastases [ 1013 ]  . 
in these selected patients , surgery may offer a real benet in terms of survival . however , only 1020% of patients were suitable for surgical resection because of technical difculties , unfavorable tumor factors , or patient comorbidities [ 7 , 8 ]  . 
in the past decade , minimally invasive loco - regional approaches were introduced as an alternative to surgery , including radiofrequency ablation ( rfa ) , microwave ablation ( mwa ) , transcatheter arterial chemoembolization ( tace ) , and selective internal rt ( sirt ) [ 15 , 16 ]  . 
five - year survival rates following rfa vary between 17 and 51% . these minimally invasive approaches were characterized by some limitations : lesions greater than 3 cm in diameter or in the proximity of major blood vessels and main biliary tract or gallbladder . 
these minimally invasive approaches were characterized by some limitations : lesions greater than 3 cm in diameter or in the proximity of major blood vessels and main biliary tract or gallbladder . historically , the role of radiotherapy ( rt ) was only palliative , due to the low whole - liver tolerance to rt . 
a high dose of radiotherapy to a large volume of healthy hepatic tissue was a risk for radiation - induced liver disease ( rild )  . according to the radiobiological model , the liver is a parallel organ , so the risk of rild is proportional to the mean radiation dose delivered to normal hepatic tissue . 
this treatment was well tolerated , with a low risk of rild , and very effective , with local control rates at 1 year of 70100% . materials and methods patient data were retrospectively analyzed after the approval of our ethical review committee . study endpoints were to evaluate the efcacy of liver sbrt in terms of local control , overall survival ( os ) , and radiation treatment - related toxicity . 
prognostic factors affecting os and local control ( lc ) were investigated . inclusion criteria , which were dened in our previously published study , were as follows : liver metastases considered not suitable for surgery , technically or medically inoperable , or because of patient refusal ; maximum tumor diameter less than 6 cm ; no more than 3 liver lesions ; normal liver volume greater than 1000 cm3 ; no evidence of progressive or untreated gross disease outside of the liver ; no prior radiation therapy to the target area ; adequate liver function ; no concurrent chemotherapy allowed , either within 14 days before sbrt or until the rst follow - up evaluation thereafter ; no active connective tissue disorders ; karnofsky perstrahlenther onkol ( 2020 ) 196 : 325333 formance status 70 ; minimum age 18 years ; and written informed consent . stereotactic body radiation therapy requires highly precise dose planning and delivery . 
a 4 - dimensional ct ( 4dct ) is acquired if the lesion is located in the posteriorsuperior segments , or with a shift greater than 5 mm on the different phases of ct . 
multi - modal imaging with contrast - enhanced magnetic resonance imaging ( mri ) and / or positron - emission tomography ( pet ) is used in doubtful or special cases for better target denition . 
the internal target volume ( itv ) , for all patients who underwent 4d - ct scan , is dened as the envelope of all gtvs in the different respiratory phases . 
the planning target volume ( ptv ) is generated from either the gtv or the itv by adding an overall isotropic margin of 5 mm ( from itv ) or of 710 mm in the cranialcaudal axis and 46 mm in the anteriorposterior and lateral axes . treatment planning sbrt requires a highly conformal dose distribution , with multiple beams using either coplanar or non - coplanar geometries . 
in selected patients , surgical clips or outcomes of previous treatments are used as ducial markers . the prescription dose was 75 gy in three consecutive daily fractions of 25 gy each . 
the plan objective was to cover at least 98% of the ctv ( itv ) volume with 98% of the prescribed dose ( v98% = 98% ) and v95% = 95% for the ptv . 
regarding constraints for organs at risk , we applied a critical dosevolume model according to the surgical and radiotherapy studies [ 20 , 21 , 24 , 25 ]  . 
spinal cord , heart , and gastrointestinal organs ( stomach , duodenum , and small bowel ) must receive less than 18 gy , 30 gy , and 21 gy in three fractions , respectively . 
of prior systemic treatment regimens extrahepatic disease at sbrt time prior liver - directed therapy treatment lesions diameter ( mm ) ( cid : 2 ) 30 mm > 30 mm dose prescription ( per lesion ) full dose ( 75 gy ) sbrt stereotactic body radiation therapy no . 
follow - up was performed every 3 months , which included ct imaging and , in selected cases , mri . when a pet scan was available pre - treatment , it was also required after 6 months to conrm metabolic response or progression . statistical considerations actuarial lc and os curves were generated using the kaplanmeier method . 
all analyses were performed using stata version 1 software and a p - value was considered signicant if < 0.05. results between february 2010 and december 2016 , we analyzed 202 patients with 268 liver metastases from solid tumors treated with sbrt . 
baseline patient and treatment characteristics are listed in table 1 . seventy - two patients ( 35.6% ) had synchronous metastatic the time of diagnosis and 44 ( 21.8% ) had disease at metachronous liver metastases with disease - free interval ( dfi ) ( cid : 2 ) 12 months . 
we found that 115 patients ( 56.9% ) had a diagnosis of out - eld liver progression and 111 patients ( 59.4% ) had the appearance of extra - hepatic metastases after sbrt . at the time of analysis , 61 patients ( 30% ) were alive . median follow - up was 21 months ( 95% ci 1824 )  . 
2 shows the kaplanmeyer curves for os . at univariate analysis , 4 out of 10 examined variables were signicant prognostic factors of survival : sex , primary disease histology , intra - , and extra - hepatic progression , as shown in fig . 
most frequent acute toxicities were g2 fatigue in 38% of patients and g2 transient transaminase increase in 24% of patients . in all cases , the increased values normalized within the 36 months after sbrt . 
one case of g2 gastric ulcer was recorded after 2 months of the end of sbrt during esophagus gastroduodenoscopy for epigastric pain terms of chronic adverse effects , we recorded two cases of g2 rib fractures after 7 and 11 months of the end of sbrt . discussion this is a report on a large cohort of patients treated with sbrt for unresectable liver metastases , using the ablative high dose of 75 gy in three fractions . considering the outcome of local control , in our analysis , a few factors affected local response rate , but not lesion diameter . 
in the phase iii trial of rusthoven et al . , a dose escalation of 3660 gy in three fractions was analyzed for liver metastases with a maximum diameter < 6 cm [ 20 ]  . 
factors affecting overall survival ( os ) are primary histology ( b , p < 0.0001 ) , extra - eld liver progression ( pd ; c , p < 0.004 ) , and systemic progression ( d , p < 0.05 ) ; others pancreas and biliary tract , kidney , head and neck results of a phase ii study on liver sbrt using a higher prescription dose of 75 gy in three fractions showed the safety and the efcacy of this fractionation , without differences in lc related to lesion size [ 21 ]  . 
in 2013 , the preliminary results of a phase ii study on liver sbrt using a higher prescription dose of 75 gy in three fractions showed the safety and the efcacy of this fractionation . 
the relationship between dose and size response was not conrmed [ 21 ]  . our experience in a larger cohort of patients with a longer follow - up conrmed the efcacy of dose escalation in the treatment of liver metastases from different primary histologies , with a rate of lc at 3 years of 84% . hepatic lesions from colorectal cancer are correlated with a lower local control rate of 79% at 3 years , which is , however , comparable to the response rate achieved with other local ablative therapies . 
the authors assessed rsi in liver metastases and clinical outcomes after sbrt - based on primary histology . colorectal adenocarcinoma metastases were determined to be more radioresistant than other histologies such as anal squamous cell cancer , breast , and lung adenocarcinoma [ 29 ]  . another factor related to worse local control in our study was prior local liver therapies . 
in non - colorectal nonneuroendocrine liver metastases ( ncnnlm ) , the indication for hepatic surgery is controversial , owing to the low number of cases and the heterogeneity of the primary disease [ 31 ]  . 
considering the good results of surgery , an increasing number of experiences about sbrt on breast and gynecological cancer liver metastases have been published [ 40 , 41 ]  . recently , andratschke et al . 
median overall survival was 24 months . authors conrmed that overall survival is mainly inuenced by histology [ 42 ]  . the second factor correlated to a worse overall survival was progression of disease after sbrt . 
median overall survival was 25.4 months in patients with local failure after sbrt versus 30.6 months in patients without progression . number of lesions , metastases diameter , and extra - hepatic disease at the time of sbrt are not statistically signicant for os rates . 
erste studien verglichen bei vorhandensein von risikofaktoren die strahlentherapie mit einer alleinigen chemotherapie und konnten keinen berlebensvorteil zugunsten der chemotherapie im vergleich zur alleinigen strahlentherapie nachweisen [ 1 , 2 ]  . eine studie von randall et al . 
diese studie hatte jedoch groe methodische probleme und sollte deshalb nur mit zurckhaltung interpretiert werden . konsens ist , dass das hochrisikoendometriumkarzinom sowohl ein hohes risiko fr einen lokoregionalen progress als auch fr fernmetastasen aufweist . 
die idee hinter der portec - 3 - studie war deshalb logisch , eine alleinige strahlentherapie mit einer simultanen radiochemotherapie ( rct ) , gefolgt von einer adjuvanten chemotherapie , zu kombinieren , um beide themen zu adressieren , in bezug auf das lokoregionre und das distante rezidivrisiko . 
zum vergleich wurde die alleinige perkutane strahlentherapie als standardarm gewhlt . originalpublikation de boer sm , powell me , mileshkin l , katsaros d , bessette p , haie - meder c , ottevanger pb , ledermann ja , khaw p et al ( 2019 ) adjuvant chemoradiotherapy versus radiotherapy alone in women with high - risk endometrial cancer ( portec - 3 ) : patterns of recurrence and post - hoc survival analysis of a randomised phase 3 trial . 
62 , 50937 kln , deutschland patientengut und methodik die portec - studie [ 4 , 5 ] ist eine internationale , randomisierte phase - iii - studie , die an 103 zentren patientinnen rekrutierte . 
der radiotherapie allein bei patientinnen mit hochrisikoendometriumkarzinomen der figo - klassikation von 2009 im stadium i , vom endometrioiden typ grad 3 mit tiefer myometriuminltration oder lymphovaskulrer invasion oder beidem bzw . 
endometrioiden typen im figo - stadium ii und iii oder figostadium i und iii bei serser oder klarzelliger komponente . die portec - 3 - studie wurde gepowert , um eine differenz von 10 % im 5 - jahres - gesamtberleben zu identizieren . koendpunkt war das disease free survival ( dfs )  . operativ wurde eine totale abdominale oder laparoskopische hysterektomie mit bilateraler salpingen - oophorektomie durchgefhrt . 
das ausma der lymphonodektomie war den zentren berlassen , was dazu fhrte , dass lediglich 40 % der patientinnen eine lymphonodektomie bekamen . dies hat implikationen fr die stadieneinteilung und interpretation der ergebnisse spter . 
die patientinnen wurden randomisiert , entweder zu einer alleinigen strahlentherapie ( 1 , 8 bis 48 , 6 gy ) oder zu demselben strahlentherapieprotokoll mit simultan cisplatin 50 mg / m2 kof in woche 1 und 4 whrend der strahlentherapie , gefolgt von 4 weiteren adjuvanten zyklen chemotherapie , bestehend aus carboplatin auc 5 und paclitaxel 175 mg / m2 . 
zwischen 2006 und 2013 wurden 660 patientinnen inkludiert ( strahlentherapie : n = 330 , rct + chemotherapie : n = 330 )  . ergebnisse die adhrenz zur therapie war exzellent in beiden gruppen . 
das 5 - jahres - gesamtberleben betrug 81 , 8 % im kombinierten arm und 76 , 7 % im radiotherapiearsomit war der primre endpunkt verfehlt . strahlenther onkol ( 2020 ) 196 : 410413 das 5 - jahres - dfs betrug 75 , 5 % in der rct - gruppe vs . 68 , 6 % in der radiotherapiegruppe ; dies ist statistisch signikant . 
ein viertel der patientinnen , die kombiniert behandelt worden waren , berichtete ber taubheit im sinne einer polyneuropathie nach 2 jahren , verglichen mit nur 6 % nach alleiniger radiotherapie . schlussfolgerung der autoren die kombination von adjuvanter simultaner rct , gefolgt von chemotherapie , kann bei patientinnen mit hochrisikoendometriumkarzinomen im vergleich zur alleinigen strahlentherapie das gesamtberleben insgesamt nicht verbessern . 
subgruppenanalysen zeigen jedoch , dass insbesondere patientinnen im stadium iii eine signikante verbesserung im dfs erleben durch die kombinierte behandlung ; diese ist klinisch relevant und bersteigt die kalkulierte verbesserung von 10 % . kommentar die kombinationstherapie verbesserte also das gesamtberleben der patientinnen nicht . 
die therapie im kombinierten arm war signikant lnger und zeigte 5 - mal mehr hochgradige toxizitt im vergleich zur strahlentherapie allein . in der subgruppenanalyse fllt auf , dass patientinnen mit sersen oder klarzelligen karzinomen , lvsi - positiven tumoren und solchen ohne lymphonodektomie sowie patientinnen > 70 jahre und solche im figo - stadium iii insbesondere von der kombinationstherapie protierten . eine groe schwche der studie ist der patientinnenmix aus niedrigen lokalen tumorstadien , karzinomen mit hochrisikofaktoren sowie lokal fortgeschrittenen tumoren . 
es handelt sich zunchst um gog - 249 , welche 600 patientinnen im stadium i / ii mit high - intermediateoder high - risk - faktoren mit endometrioider oder sers klarzelliger tumorkomponente inkludierte . 
eine berlegenheit der vaginalen brachytherapie gefolgt von chemotherapie im vergleich zur perkutanen strahlentherapie konnte dabei nicht festgestellt werden . die akuttoxizitt war deutlich hher im kombinierten therapiearm , die chronische toxizitt aber gleich . 
interessant ist in diesem zusammenhang , dass die pelvine und paraaortale nodale rezidivrate bei den patientinnen , die lediglich eine vaginale brachytherapie und chemotherapie erhalten hatten , immerhin 9 % betrug ; dies im vergleich zu lediglich 4 % bei den patientinnen , die eine perkutane strahlentherapie erhalten hatten . 
die autoren schlussfolgerten , dass die strahlentherapie allein eine effektive , gut tolerierbare und angemessene adjuvante therapie bei der hochrisikopatientin im frhen stadium in allen subtypen des endometriumkarzinoms darstellt . die zweite randomisierte studie , die in diesem zusammenhang zu diskutieren wre , ist gog - 258 . 
es erfolgte der randomisierte vergleich zwischen alleiniger postoperativer chemotherapie , bestehend aus 6 zyklen carboplatin ( auc 6 ) plus paclitaxel 175 mg / m2 alle drei wochen , und kombinierter rct mit simultaner gabe von 50 mg / m2 am tag 1 und 29 , gefolgt von carboplatin ( auc 56 ) plus paclitaxel 175 mg / m2 alle 21 tage fr 4 zyklen ( analog portec - 3 )  . der einschluss von patientinnen mit postoperativen resttumoren war erlaubt , sie durften aber nach einschtzung des operateurs < 2 cm sedie pelvine und paraaortale lk - biopsie oder - dissektion war auch in dieser studie optional . 
2 % 412 strahlenther onkol ( 2020 ) 196 : 410413 der patientinnen nach alleiniger perkutaner bestrahlung . lokal das heit , dass in dem hochrisikokollektiv mit fortgeschrittenen tumoren , ggf . 
auch in gog - 258 waren die lokalen vaginalen rezidive mit 2 % im perkutan bestrahlten arm deutlich niedriger als mit 7 % im brachytherapiearauffallend ist die fast doppelt so hohe rate pelviner und paraaortaler lk - rezidive mit 20 % im patientenarm , dessen patientinnen postoperativ lediglich eine chemotherapie adjuvant erhalten hatten , im vergleich zu den perkutan bestrahlten patientinnen mit 11 % . schlussfolgerungen fr die tgliche arbeit 1 . 
insbesondere fr stadium - iii - patientinnen muss klar sein , dass die kombination aus strahlentherapie und chemotherapie , gefolgt von einer adjuvanten chemotherapie , das dfs signikant verbessert im vergleich zur alleinigen postoperativen strahlentherapie . 
das ziel der adjuvanten therapie sollte immer auch die vermeidung von lokalen und lokoregionren rezidiven sedenn nicht alle rezidive knnen spter einer sufzienten und erfolgreichen salvage - therapie zugefhrt werden . 
bei patientinnen im stadium i mit hochrisikooder high - intermediate - risk - faktoren ist die perkutane strahlentherapie verglichen mit der vaginalen brachytherapie gefolgt von drei zyklen chemotherapie zur rezidivprophylaxe gleich effektiv im hinblick auf das gesamtberleben . 
die strahlentherapie ist wiederum effektiver bei der vermeidung von lokalen rezidiven . fazit fr hochrisikopatienten mit endometriumkarzinom kann die chemotherapie oder die perkutane strahlentherapie oder die radiochemotherapie gefolgt von einer sequenziellen chemotherapie genutzt werden . 
marnitz geben an , dass kein interessenkonikt besteht . open access dieser artikel wird unter der creative commons namensnennung 4.0 international lizenz verffentlicht , welche die nutzung , vervielfltigung , bearbeitung , verbreitung und wiedergabe in jeglichem medium und format erlaubt , sofern sie den / die ursprnglichen autor ( en ) und die quelle ordnungsgem nennen , einen link zur creative commons lizenz beifgen und angeben , ob nderungen vorgenommen wurden . die in diesem artikel enthaltenen bilder und sonstiges drittmaterial unterliegen ebenfalls der genannten creative commons lizenz , sofern sich aus der abbildungslegende nichts anderes ergibt . 
sofern das betreffende material nicht unter der genannten creative commons lizenz steht und die betreffende handlung nicht nach gesetzlichen vorschriften erlaubt ist , ist fr die oben aufgefhrten weiterverwendungen des materials die einwilligung des jeweiligen rechteinhabers einzuholen . weitere details zur lizenz entnehmen sie bitte der lizenzinformation auf literatur 1 . 
maggi r , lissoni a , spina f , melpignano m , zola p , favalli g , colombo a , fossati r ( 2006 ) adjuvant chemotherapy vs radiotherapy in high - risk endometrial carcinoma : results of a randomised trial . br j cancer 95 : 266271 2 . 
susumu n , sagae s , udagawa y , niwa k , kuramoto h , satoh s , kudo r , japanese gynecologic oncology g ( 2008 ) randomized phase iii trial of pelvic radiotherapy versus cisplatin - based combined chemotherapy in patients with intermediateand high - risk endometrial cancer : a japanese gynecologic oncology group study . gynecol oncol 108 : 226233 strahlenther onkol ( 2020 ) 196 : 410413 3 . 
randall me , filiaci vl , muss h , spirtos nm , mannel rs , fowler j , thigpen jt , benda ja , gynecologic oncology group s ( 2006 ) randomized phase iii trial of whole - abdominal irradiation versus doxorubicin and cisplatin chemotherapy in advanced endometrial carcinoma : a gynecologic oncology group study . 
de boer sm , powell me , mileshkin l , katsaros d , bessette p , haie - meder c , ottevanger pb , ledermann ja , khaw p , colombo a et al ( 2018 ) adjuvant chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer ( portec - 3 ) : nal results of an international , open - label , multicentre , randomised , phase 3 trial . 
de boer sm , powell me , mileshkin l , katsaros d , bessette p , haie - meder c , ottevanger pb , ledermann ja , khaw p , colombo a et al ( 2016 ) toxicity and quality of life after adjuvant chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer ( portec - 3 ) : an open - label , multicentre , randomised , phase 3 trial . 
randall me , filiaci v , mcmeekin ds , von gruenigen v , huang h , yashar cm , mannel rs , kim jw , salani r , disilvestro pa et al ( 2019 ) phase iii trial : adjuvant pelvic radiation therapy versus vaginal brachytherapy plus paclitaxel / carboplatin in high - intermediate and high - risk early stage endometrial cancer . 
matei d , filiaci v , randall me , mutch d , steinhoff mm , disilvestro pa , moxley km , kim ym , powell ma , omalley dm et al ( 2019 ) adjuvant chemotherapy plus radiation for locally advanced endometrial cancer . 
in addition , h - imrt in step - and - shoot mode was also calculated to assess its achievability with fff beams . results all hybrid plans achieved the expected target coverage . 
for breath - hold patients , the h - vmat plan is superior to h - imrt for hypofractionated dose regimens , with reduced mu and treatment delivery time . keywords breast neoplasms radiotherapy photons radiotherapy , intensity - modulated radiation dose hypofractionation introduction radiation therapy ( rt ) is part of multimodal treatment approaches for breast cancer patients . 
adjuvant whole - breast rt following breast - preserving surgery reduces local recurrence and elicits survival improvements equivalent to mastectomy in early - stage breast cancer patients [ 13 ]  . 
moreover , an escalated dose to the lumpectomy cavity volume as a simultaneous integrated boost ( sib ) was shown to be more advantageous than sequential boost delivery [ 1012 ]  . 
this requires reduction of rt - associated problems such as cardiac toxicity , pulmonary complications , and contralateral breast ( cb ) secondary cancer risk [ 13 ]  . whole - breast with boost volume rt planning is challenging , due to the erratic shape of the target and surface irregularities [ 14 ]  . 
on the other hand , advanced treatment modalities such as intensity - modulated radiation therapy ( imrt ) and volumetric modulated arc therapy ( vmat ) are capable of improving dose homogeneity and strahlenther onkol ( 2020 ) 196 : 376385 conformity and restricting the high - dose irradiation to normal tissues ( nt ) compared to 3dcrt . 
hybrid plans afford balanced results for planning target volume ( ptv ) and organs at risk ( oar ) dosimetric parameters , by accumulating the benets of each technique [ 13 ]  . a recent trend in the linear accelerator facility is the use of attening lter - free ( fff ) photon beams in hypofractionated dose treatments . 
the improved dosimetric potential of fff beams has been described in many articles [ 2325 ]  . published studies have reported on clinical use of fff beams for breast rt [ 2629 ]  . 
most of the studies employed imrt and vmat to generate hybrid plans and restricted the use of open - beam 3dcrt techniques for fff beams . despite 3dcrt sparing oars at low dose levels , fff beams and sib techniques encourage the use of a modulated beapublished data have reported on the benet of 3dcrt as a base - dose plan in hybrid techniques using atbeam photons for breast rt [ 13 , 16 ]  . 
the purpose of the present study is to explore the feasibility of fff beams in a large - eld 3dcrt - based hybrid technique and perform a dosimetric comparison of hybrid imrt ( h - imrt ) and hybrid vmat ( h - vmat ) plans for left - sided whole - breast rt incorporating sib target volumes using a hypofractionated dose regimen . materials and methods patient preparation and delineation twenty - ve patients with early - stage left - sided breast cancer ( median age 49 years ) who had received adjuvant rt were replanned with h - imrt and h - vmat for this dosimetric comparison study . 
a planning computed tomography ( ct ) scan ( discovery iq 16 slice ct scanner ; ge healthcare , chicago , il , usa ) had been performed for all patients positioned in customized vacuum bags in supine position with their arms raised above the head . 
the ct scans were generated with 2.5 - mm slice thickness under deep inspiration breath - hold ( dibh ) using a real - time position management ( rpm ) system ( varian medical systems , palo alto , ca , usa )  . clinical target volumes ( ctvs ) that included the whole breast and lumpectomy cavity boost were delineated by an experienced radiation oncologist based on the radiation therapy oncology group ( rtog ) guidelines [ 30 ]  . 
the whole - breast ptv ( ptvwb ) and boost ptv ( ptvboost ) were then generated by expanding by 5 mm around ctvs and brought within 5 mm of the skin surface . 
in order to include erratic breast movement between treatment fractions , an optimization ptv ( ptvwb - opt ) was generated from the ptvwb - eval , encompassing 5 mm outside of the body region and a 10 - mm water equivalent optimization bolus was applied to the body surface beside ptvwb - opt according to [ 31 ]  . 
the oars delineated were heart , left anterior descending coronary artery ( lad ) , ipsilateral lung ( il ) , contralateral lung ( cl ) , contralateral breast ( cb ) , skin , and normal tissue ( nt ) , denoted as the external body volume excluding the ptvs . 
in addition , a ring structure consisting of a 1 - cm thick wall around the ptvwb was used to avoid high doses to nt . treatment planning hybrid treatment plans were generated using the eclipse version 13.6 treatment planning system ( tps ) modeled for the truebeam stx linear accelerator ( varian medical systems ) equipped with high - denition multileaf collimators ( mlc )  . 
in addition , h - imrt in step - and - shoot mode ( h - imrtss ) was compared with routine dynamic mode to explore its ability in an fff beam technique . 
1 field arrangements in a three - dimensional conformal radiation therapy ( two elds , f1f2 ) , b intensity - modulated radiation therapy ( eight elds , f1f8 ) , and c volumetric modulated arc therapy ( four arcs ) plans . 
delineation of ptvboost ( red line ) , ptvwb ( orange line ) , ipsilateral lung ( cyan ) , contralateral lung ( dark blue ) , heart ( light green ) , contralateral breast ( violet ) , spinal cord ( megenta ) and external body ( green ) the 3dcrt plan consisted of two coplanar open tangential elds through an isocenter placed at the center of ptvwb in craniocaudal direction and axially at the lungptvwb interface . 
the gantry angles were based on ptv curvature and heart and il involvement with collimator angles 0 . these tangential elds were extended 2 cm outside of the body to accommodate for breast setup error . 
volume dose was calculated for 2.2 gy ( approximately 70% of ptvboost prescription dose ) using the analytical anisotropic algorithm ( aaa ) with a 2.5 - mm dose grid matrix . 
all 3dcrt plans were normalized to deliver the mean dose to ptvboost equal to the prescription dose . the imrt and vmat plans were generated with the same isocenter as 3dcrt and prescribed the remaining dose of 1 gy ( approximately 30% of ptvboost prescription dose )  . 
the imrt plan consisted of eight elds with xed gantry angles of 330 , 0 , 30 , 70 , 100 , 160 and two tangential angles used for 3dcrt . 
both imrt and vmat optimizations were executed using the photon optimizer ( po , version 13.6 ) algoriththe jawtracking feature and normal tissue objective ( nto ) in automatic mode were turned on and the 3dcrt plan was kept as a base - dose plan . 
2 dose distributions in a hybrid intensity - modulated radiation therapy ( h - imrt ) and b hybrid volumetric modulated arc therapy ( h - vmat ) plans for a patient case . 
the h - imrt , h - imrtss , and h - vmat plans were then generated by adding 3dcrt to imrt , imrtss , and vmat plans , respectively . dosimetric evaluation ptv dosimetric indices such as coverage ( d95% ) , homogeneity index ( hi ) of ptvboost and ptvwb - eval , conformity index ( ci ) of ptvboost and ptvwb , and gradient index ( gi ) of ptvwb were evaluated for the planning comparison.. 
the ci was dened as : ci = vptv vptvref ( cid : 2 ) vref vptvref where vptv is the volume of ptv , vptvref is reference isodose ( 95% ) volume within the ptv , and vref is the volume of reference isodose ( 95% ) [ 32 ]  . 
the hi was calculated as : where d2% and d98% are the doses received by 2% and 98% of the ptv , respectively , and dp is the prescription dose [ 33 ]  . 
3 comparison of average dosevolume histograms ( dvh ) between hybrid intensity - modulated radiation therapy ( h - imrt ) and hybrid volumetric modulated arc therapy ( h - vmat ) plans . ptvboost boost planning target volume , ptvwb - eval whole - breast minus boost planning target volume for evaluation , il ipsilateral lung , cl contralateral lung , cb contralateral breast , nt normal tissue where v50% is the 50% isodose volume and vptv is the volume of the ptv [ 34 ]  . 
in addition , total mus and treatment time ( tt ) , dened as time taken from rst eld beam - on to last eld beam - off were recorded . 
the acceptance limit was a relative gamma agreement index ( gai ) of more than 95% between the calculated and measured dose matrix with passing criteria of 3% dose difference and 3 mm distance - toagreement . for statistical analyses , a non - parametric mannwhitney u test was performed for paired groups of h - imrt vs . h - vmat and h - imrt vs . 
all statistical tests were two - tailed and the threshold for statistical signicance was p < 0.05. results the average volumes of ptvboost , ptvwb , il , heart , and lad are presented in table 2 . 
though ptvboost coverage and hi were slightly better in h - vmat ( p < 0.002 ) and ptvwb - eval coverage and hi were marginally improved in h - imrt ( p < 0.001 ) , these results were clinically comparable . 
though ptvwb - eval is an individual volume out of ptvboost , the high dose gradient of ptvboost falling into ptvwb - eval worsens its hi compared to ptvboost hi . 
the il v5gy and v35gy were signicantly smaller in h - imrt plans ( p < 0.01 ) , whereas mean dose and v20gy results were similar in both plans . 
they found that personalized cb dose estimates based on minimum breast distance ( dened as cb distance from tangential beam of treated breast ) and breast - to - breast distance ( dened as distance between cb and treated breast in axial slice ) were highly correlated . this approach may help in making clinical decisions and in studies on cb secondary cancer risks . dosimetric comparison studies using different hybrid planning techniques for whole breast with a lumpectomy cavity boost volume rt are sparse . 
in this dosimetric comparison study , h - imrt and h - vmat plans were explored using a hypofractionated dose regimen and fff photon beams for left - sided whole - breast irradiation with a sib discussion target . 
for instance , the uk standardization of breast radiotherapy ( start ) trial a explored dose regimens of 39 gy and 41.6 gy in 13 fractions over 5 weeks [ 38 ] , while start trial b suggested a dose prescription of 40 gy in 15 daily fractions over 3 weeks and the canadian trial recommended a prescription dose of 42.5 gy in 16 daily fractions over 3.5 weeks [ 39 ]  . 
for the hypofractionated sib dose , the german aro - 201001 trial ( hyposib ) reported a dose of 48 gy to the boost volume and 40 gy to whole breast in 16 daily fractions over 3 weeks [ 6 ]  . 
 [ 42 ] recommended a sib prescription dose of 48 gy to the tumor bed and 40.5 gy to whole breast in 15 daily fractions over 3 weeks . this study utilized the sib dose regimens according to scorsetti et al.s [ 42 ] protocol . traditionally , two tangential 3dcrt elds have been used for whole - breast only rt . 
most of the planning studies have used 3dcrt elds as a base - dose plan in combination with imrt or vmat [ 13 , 1618 ]  . some other studies used a combination of imrt and vmat in their hybrid study , particularly when fff beams were used [ 19 , 22 , 29 ]  . 
in spite of using an optimization bolus and ptv expansion , the inuence of changes in breast shape , setup , and breathing uncertainties is greater in imrt than in 3dcrt [ 43 ]  . with a widened skin ash margin and higher dose weightings , 3dcrt beams efciently limits these uncertainties . in addition , it was feasible to use fff beams with openbeam 3dcrt elds . 
this fact helped in reducing the skin dose , which might improve cosmetic outcomes . as part of the hybrid component , the number and design of arcs in vmat plans were based on ramasubramanian et al.s study [ 44 ]  . 
 [ 45 ] suggested tangential imrt ( timrt ) compared to eld - in - eld ( finf ) , multi - eld imrt ( m - imrt ) , and continuous vmat ( c - vmat ) for wholebreast alone rt . 
nevertheless , h - imrt with more mu transports leakage and scattered radiation to out - of - eld regions [ 49 ]  . though dibh can reduce dose to the heart and lad , this technique might not be feasible for all patients , particularly for elderly patients who are unable to hold their breath for a long time [ 13 ]  . 
the tt plays an important role with regards to patient comfort , breath - hold consistency , and minimization of patient movement during treatment . the h - vmat with reduced mu provided a signicantly reduced tt for a hypofractionated dose , which facilitates the dibh technique without much complication . robust clinical trials on reducing the risk of breast rt complications such as heart disease , lung pneumonitis , and radiation - induced secondary cancers have set dose constraints using conventional fractionation schemes and atbeam photons [ 4953 ]  . 
februar 2020 springer - verlag gmbh germany , part of springer nature 2020 fragestellung und hintergrund patienten mit einem hodgkin - lymphom knnen in prognostisch unterschiedliche subgruppen unterteilt werden [ 1 , 2 ]  . 
in einigen dieser gruppen sind die berlebensraten nach multimodaler therapie bereits so hoch , dass eine reduzierte therapieintensitt untersucht wird , da man sich vorteile bezglich verschiedener nebenwirkungen , beispielsweise der rate von sekundrmalignomen , erhofft [ 35 ]  . 
eine amerikanische [ 6 ] und auch die hier vorgestellte hd16 - studie konzipiert [ 7 ]  . patienten und methode es wurde eine randomisierte multicenterstudie der phase iii mit dem progressionsfreien berleben ( pfs ) als primrem endpunkt durchgefhrt . einschlusskriterien : alter 1875 jahre , klassisches hodgkin - lymphom im stadium i oder ii oder nodulres lymphozytenprdominantes hodgkin - lymphom im stadium i , iia oder iib . 
es sollte die nichtunterlegenheit des deeskalierten arms gezeigt werden ( absolute differenz von 10 % im 5 - jahres - pfs )  . ergebnisse zwischen 2009 und 2015 wurden 1150 patienten eingeschlossen . 
das 95 % - ki der hazard ratio von 1 , 78 lag bei 1 , 02 bis 3 , 12 und inkludierte den vorher festgelegten wert von 3 , 01 als grenze der nichtunterlegenheit . 
auf der basis langjhriger forschung zum thema bildgesteuerte vorhersage eines guten therapieansprechens [ 8 , 9 ] wurde das pet - 2 - resultat herangezogen , um das weitere vorgehen nach 2 zyklen abvd - chemotherapie zu bestimmen . die pet - adaptierte therapie im frhen stadium des hodgkin - lymphoms wurde auch von anderen gruppen untersucht [ 10 , 11 ]  . 
das vorliegen eines positiven pet - 2 mit deauville - score 4 deutet jedoch auf ein vergleichsweise hohes rezidivrisiko hneue systemische therapien knnten in dieser subgruppe vielleicht von nutzen sewie krzlich berichtet , gibt es unterschiedliche therapieprferenzen seitens der patienten und auch der onkologen [ 12 ]  . 
zum beispiel gilt es , alter , familienplanung und risiko fr sekundrmalignome zu bercksichtigen . nach sorgfltiger abwgung wird oftmals die entscheidung zur effektivsten erstlinienbehandlung getroffen , welche auf der basis der hd16 - studie eine ifrt einschliet . in einer skandinavischen studie mit langer medianer nachbeobachtung von 16 jahren fand sich keine erhhte sterblichkeit im vergleich zur generellen population nach einer risikoadaptierten therapie mit 2 oder 4 zyklen abvd und einer strahlentherapie ( limitiertes feld im gegensatz zu ifrt , dosis 30 gy ; [ 13 ] )  . 
diese patienten wurden zu einer zeit behandelt , als es noch keine oder nur begrenzte moderne technologie zur optimierung der dosisverteilung gab [ 14 , 15 ]  . fazit die pet - 2 - adaptierte hd16 - studie besttigt die guten resultate mit 2 zyklen einer abvd - chemotherapie gefolgt von ifrt . 
franklin j , eichenauer da , becker i et al ( 2017 ) optimisation of chemotherapy and radiotherapy for untreated hodgkin lymphoma patients with respect to second malignant neoplasms , overall and progression - free survival : individual participant data analysis . cochrane database syst rev 13 ; 9 : cd8814 5 . 
straus dj , jung sh , pitcher b et al ( 2018 ) calgb 50604 : risk - adapted treatment of nonbulky early - stage hodgkin lymphoma based on interim pet . 
fuchs m , goergen h , kobe c et al ( 2019 ) positron emission tomography - guided treatment in early - stage favorable hodgkin lymphoma : nal results of the international , randomized phase iii hd16 trial by the german hodgkin study group . 
andre mpe , girinsky t , federico m et al ( 2017 ) early positron emission tomography response - adapted treatment in stage i and ii hodgkin lymphoma : final results of the randomized eortc / lysa / fil h10 trial . 
brckelmann pj , mcmullen s , wilson jb et al ( 2019 ) patient and physician preferences for rst - line treatment of classical hodgkin lymphoma in germany , france and the united kingdobr j haematol 184 : 202214 13 . 
lagerlf i , holte h , glimelius i et al ( 2019 ) no excess long - term mortality in stage iiia hodgkin lymphoma patients treated with abvd and limited eld radiotherapy . 
edvardsson a , kgele m , alkner s et al ( 2019 ) comparative treatment planning study for mediastinal hodgkins lymphoma : impact on normal tissue dose using deep inspiration breath hold proton and photon therapy . 
provider decision regret was declared in 12 patients ( 36% ) : 2 patients with grade 3 pneumonitis , 3 patients with a short survival ( radiotherapy during the last 30 days of life ) , and 7 patients with progression . 
decision regret was declared only in patients with eastern cooperative oncology group ( ecog ) performance status ( ps ) 2 or 3 and was associated with a time interval to re - irradiation < 6 months . conclusion our data support the usefulness and acceptable side effects prole of palliative re - irradiation for lung cancer . patients with reduced ps are at increased risk of futile treatment . 
evaluation of provider decision regret has the potential to improve the way we learn from retrospective databases and should also be considered for other scenarios where high - quality prospective outcome data are lacking . keywords lung cancer radiotherapy re - irradiation symptom palliation decision regret re - irradiation for symptom palliation has long been used in a large number of different clinical scenarios [ 1 ] , including advanced lung cancer [ 2 ]  . 
it has also been shown that selected patients with non - small cell lung cancer ( nsclc ) are able to tolerate high - dose re - irradiation , which aims beyond relief of symptoms [ 35 ]  . 
evidence is derived mainly from a few small single - arm prospective studies and a consid ( cid : 2 ) carsten nieder , md carsten.nieder@nlsh.no 1 department of oncology and palliative medicine , nordland hospital , 8092 bod , norway 2 department of clinical medicine , faculty of health sciences , university of troms , 9037 troms , norway erable number of retrospective analyses . 
most of these reported limited data about the overall usefulness of palliative re - irradiation and did not fully answer the following questions : did re - irradiation result in symptom relief or prolong the time without worsening of the thoracic tumor ? was survival long enough to justify re - irradiation as compared to simpler palliative and supportive interventions ? did re - irradiation cause high - grade toxicity ? we were interested in analyzing the usefulness of re - irradiation based on a composite endpoint integrating all the aspects mentioned above , resembling the concept of uncomplicated cure in rst - line settings . 
survival was calculated from the rst day of reirradiation . patients and methods results this is a retrospective single - institution study based on a previously described database that is maintained in order to analyze the quality of care for patients with lung cancer at our institution [ 7 ]  . 
all patients re - irradiated for in - eld or marginal recurrence to overlapping thoracic target volumes between 2011 and 2018 were identied from the database and included in the study . 
we arbitrarily decided that grade 3 toxicities other than pneumonitis might be acceptable if compensated by a benet from re - irradiation , but we acknowledge that patient - reported data and judgements would be preferable to conrm this perspective . 
re - irradiation was offered on a case - by - case basis , irrespective of target volume size , time interval , and previous dose , and without applying any standardized dose constraints , except for spinal cord where we used our previously published risk model to ensure the patients had a low or intermediate risk of myelopathy [ 8 ]  . 
dose was prescribed to the reference point , and the clinical target volume received at least 95% of the prescribed dose , unless coverage was reduced to protect normal tissues . 
date of death was also registered in these thirty - three patients were analyzed ( 22 males ; two largest histology groups : 19 with squamous cell , 6 with small cell [ sclc ] tumors )  . 
more than 10 different fractionation regimens were used in rst line ( median dose 39 gy ) , e.g. , 2 fractions of 8.5 gy ( day 1 and 8 ; 21% ) , 10 fractions of 3 gy ( 15% ) , and 15 fractions of 2.8 gy ( 12% )  . 
all patients completed their prescribed course of re - irradiation . the median age at re - irradiation was 70 years ( range 4786 ) and 12 patients ( 40% ) were 75 or older . 
eastern cooperative oncology group ( ecog ) performance status ( ps ) was 01 in 7 patients ( 21% ) , 2 in 15 patients ( 45% ) , and 3 in the remaining 11 patients ( 33% )  . 
the reason for re - irradiation was superior vena cava compression ( n = 2 ) , nodal relapse at the margin of the previous target volume ( n = 1 ) , consolidation of chemotherapy response ( n = 1 ) , thoracic pain ( n = 7 ) , lung symptoms ( dyspnea , cough , hemoptysis ; n = 9 ) , and in - eld imaging progression ( n = 13 )  . 
eleven patients ( 33% ) were not in contact with the hospital in the nal phase before death , and therefore the cause of death was dened as unknown after review of the patient records . the median overall survival time was 5.2 months ( 95% condence interval 3.47.0 months ) and 4 patients ( 12% ) were alive 1 year after the start of re - irradiation . 
grade 12 esophagitis , fatigue , and asthenia were recorded in up to 30% . the retrospective chart review resulted in provider decision regret in 12 patients ( 36% )  . 
two of these decisions were triggered by grade 3 pneumonitis , three by short survival ( radiotherapy during the last 30 days of life ; in one case combined with lack of efcacy ) , and seven by lack of efcacy . 
 ( 1992 ) [ 15 ] gressen et al . ( 2000 ) [ 16 ] kramer et al . ( 2004 ) [ 17 ] ebara et al . ( 2007 ) [ 18 ] cetingoz et al . ( 2009 ) [ 19 ] kruser et al . ( 2014 ) [ 20 ] huh et al . ( 2014 ) [ 21 ] schlampp et al . ( 2019 ) [ 22 ] present study discussion strahlenther onkol ( 2020 ) 196 : 315324 table 3 treatment characteristics ( previous studies ) author initial rt dose , gy ( median ) re - rt dose , gy ( median ) 4065 ( 53 ) 654 ( 35 ) rt elds and / or volume cumulative rt dose , gy ( median ) 60166a ( 82 ) rt eld size , cm2 ( median ) % patients receiving average , 80 5061 ( 55 ) 2030 ( 30 ) 7090 ( 85 ) 2866 ( 60 ) 1557 ( 30 ) 43122a ( 88 ) tumor only = 76% uninvolved mediastinum = 24% volume encompassing the disease causing symptoms large eldsb = 425 patients tumor only = 30 patients tumor + 12 cm n . 
not stated ; 3d three - dimensional rt ; gtv gross tumor volume ; ctv clinical target volume ; ptv planning target volume ; imrt intensity - modulated rt aincludes patients re - irradiated twice bincludes various eld sizes including ipsilateral hilum , contralateral hilum , mediastinum , and ipsilateral supraclavicular fossa despite increasing numbers of systemic treatment options and continuous improvement of local therapies , many patients with lung cancer relapse [ 911 ]  . 
yet , internationally accepted models of response prediction are not available in this setting . decision - making also has to acknowledge the potential of serious toxicity from thoracic radiotherapy . in the absence of patient - reported data , we were interested in exploring alternative ways of judging the usefulness of palliative thoracic re - irradiation . 
those included short survival ( radiotherapy during the last 30 days of life , an endpoint also evaluated in different other recent studies [ 12 , 13 ] ) , lack of efcacy ( dened as immediate thoracic disease progression without a period of stable or shrinking disease ) , and serious toxicity ( myelopathy , any grade 45 , selected grade 3 )  . 
however , the present criteria may serve as a starting point from which future recommendations can be derived , if the radiation oncology community agrees that this type of chart review adds value to the way we learn from real - world databases . based on the present decision regret criteria , we found that we would not offer re - irradiation again to 36% of the patients who actually received it . 
only 3 ( 9% ) and 2 patients ( 6% ) had received 322 strahlenther onkol ( 2020 ) 196 : 315324 table 4 treatment outcome from palliative re - irradiation ( previous studies ) author months 1 - year os % % of patients showing symptom improvement dyspnea hemoptysis cough overall % of patients with toxicities chest pain n . 
s. esophagitis : 20% skin : 13% pneumonitis : 3% grade 5 ( fatal ) : 4% g2 esophagitis : 4% g2 pneumonitis : 7% g3 pneumonitis : 7% g12 esophagitis : 77% g3 esophagitis : 4% n . 
s. g5 ( fatal ) : 2% g4 ( surgery ) : tracheoesophageal stula ( 2% ) g3 esophageal stenosis ( 2% ) g2 pneumonitis : 16% g3 pneumonitis : 3% g2 pneumonitis : 3% g3 pneumonitis : 6% g12 esophagitis : 30% present study n . 
in general , overall survival and toxicity prole do not discourage palliative thoracic re - irradiation . we did not perform detailed analyses of cumulative doses and correlations of outcome and dosimetric data in this relatively small cohort with heterogeneous treatment approaches , due to limited statistical power and lack of ability to validate our ndings . 
however , it appears that regimens such as 17 gy in 2 fractions and 3039 gy in 1013 fractions are feasible , even in our population of mostly elderly patients with compromised ecog ps . 
ultimately , fractionation should be chosen taking into account the aim ( symptom relief or tumor cell kill ) , survival prognosis , and tolerance of critical structures . as shown in table 2 , 3 and 4 , previous studies reported quite heterogeneous outcomes after re - irradiation to median doses that were often in the range of 3040 gy . 
median dose of the hypofractionated schedule was 32 gy ( range 442 gy ) , with a median fraction size of 4 gy ( range 2.54.2 gy ) delivered 35 times per week . 
since brachytherapy is limited to patients with accessible endoluminal disease , this approach will not be discussed either . few studies have provided data on predictive factors for radiation pneumonitis after palliative re - irradiation . 
multivariate analysis revealed that mean lung dose ( mld ) of the initial plan , v5 of the composite plans , and overlap - v5 / re - v5 were independent predictors for grade 3 pneumonitis . 
even if our experience is limited to two patients ( numbers 13 and 14 , table 1 ) who received pd1 inhibitors between rst and second radiotherapy , toxicity problems such as pneumonitis were not encountered . despite inherent limitations of small retrospective studies , our data showed that even patients with ecog ps3 did not have a uniformly poor prognosis . 
the fact that patients with retrospective provider decision regret were scheduled to spend no more than 10 working days on re - irradiation suggests that the prescribing physician was aware of the serious prognosis and potential for futile treatment . 
a previous study performed in the rst - line palliative irradiation setting revealed that ps , serum lactate dehydrogenase , c - reactive protein , liver / adrenal gland metastases , and extrathoracic disease status signicantly predicted survival [ 7 ]  . 
it would be interesting to analyze whether or not blood biomarkers or other parameters , e.g. , imaging features , also could be helpful in predicting futile re - irradiation . 
in conclusion , this 324 strahlenther onkol ( 2020 ) 196 : 315324 study supports the usefulness and acceptable side effects prole of palliative re - irradiation for lung cancer and encourages research towards prediction of immediate disease progression ( the prevailing cause of decision regret )  . compliance with ethical guidelines conict of interest c . 
haukland declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
combs1 , 2 , 3 received : 1 december 2019 / accepted : 16 january 2020 / published online : 3 february 2020 the author ( s ) 2020 abstract background there are different contouring guidelines for denition of the clinical target volume ( ctv ) for intensitymodulated radiation therapy ( imrt ) of anal cancer ( ac )  . 
we conducted a planning comparison study to evaluate and compare the dose to relevant organs at risk ( oars ) while using different ctv denitions . methods twelve patients with a primary diagnosis of anal cancer , who were treated with primary chemoradiation ( crt ) , were selected . 
dose parameters of the planned target volume ( ptv ) and oars were evaluated and compared , too . results the mean volume of the four ptvs ranged from 2138 cc to 2433 cc . 
22 , 81675 munich , germany partner site munich , deutsches konsortium fr translationale krebsforschung ( dktk ) , munich , germany institute for radiation medicine ( irm ) , helmholtz zentrum mnchen , ingolstdter landstr . 
1 , 85764 neuherberg , germany strahlenther onkol ( 2020 ) 196 : 368375 rtog radiation therapy oncology group vmat volumetric arc therapy background anal cancer ( ac ) is a relatively rare malignant tumor of the lower gastrointestinal tract . 
chemoradiation ( crt ) has been established as an organ - preserving standard approach in non - metastatic disease and is associated with good overall survival rates [ 1 , 2 ]  . 
so far , the most relevant prognostic factors correlating with survival endpoints are locoregional lymph node ( ln ) involvement , primary tumor size > 5 cm , and pathological complete response [ 3 ]  . 
these were published by the radiation therapy oncology group ( rtog ) , the australasian gastro - intestinal trial group ( agitg ) , and the authors and collaborative groups of the british national guidance ( bng ) [ 46 ]  . 
in a recent pet imagingbased analysis of patterns of ln involvement in primary ac , we ( the lead institution ) were able to demonstrate that the three guidelines differ in their hypothetical effectiveness to cover microscopic ln metastases . 
however , typical complications such as dermatological , genitourinary , and gastrointestinal side effects , and others like vaginal stenosis , hip osteoarthritis , or sexual dysfunction play a decisive role and should always be considered during treatment planning [ 1115 ]  . in order to be able to estimate the efciency regarding locoregional control rates and potential side effects of the different guidelines , we conducted a comparative study on the various ctvs and determined the dose to oars . methods we selected 12 patients with the primary diagnosis of squamous cell ac who were treated with crt at our institution between 2012 and 2018 . 
in all patients , we retrospectively generated the three different ctvs of the established guidelines and a fourth ctv using our own guidelines ( li ) on the original planning ct scan with a slice thickness of 3 mm ( all prone position )  . 
all guidelines are very similar regarding their recommendations for delineation of the elective ln regions in the pelvis ( internal / external iliac , pre - sacral , internal obturatoric )  . 
with regard to uncertainties leaving room for interpretation of the different denitions of the target volume , formulations such as should be contoured as a compartment , we tried to refer as much as possible to the respective atlases published . 
afterwards , mostly based on the pelvic normal tissue atlas of rtog , the vulva , scrotum , femoral heads , small bowel , rectum , sigmoid colon , and the urinary bladder were dened [ 16 ]  . 
for the main plan , the dose prescription was 36 gy ( 1.8 gy single dose ) to ptv1 ( ptvpelvic + ptving ) , which included the ptr and the elective pelvic and inguinal lns . 
the dose was prescribed to the median of the ptv ( icru83 ) [ 18 ]  . the software used for structure denition and dose comparison was eclipse treatment planning system 13.0 ( varian medical systems , palo alto , ca , usa )  . a friedman test using spss 25.0 ( spss inc , chicago , il , usa ) was applied to identify signicant differences between the four plans with regard to all dose parameters of the ptv and the oar . 
median bmi was 28 kg / m2 ( range : 1741 )  . ptv volumes and plan value the mean volumes of the ptvs of the rtog , agitg , bng , and li groups amounted to 2138 cc , 2407 cc , 2419 cc , and 2433 cc , respectively . 
all volumes were signicantly larger ( ( cid : 2 ) 10% ) compared to the volume of the rtog , whereas no signicant differences between the three ptv volumes of the agitg , bng , and li groups could be identied . 
1 differences in inguinal clinical target volumes using four different contouring guidelines for intensity - modulated radiotherapy of elective target volumes in primary treatment of anal cancer ( ac ) ( a axial , b coronal )  . 
the mean v40 gy of the urinary bladder did not reach more than 40% and the mean v30 gy of the femoral heads was 50% or less . the dose parameters to the genitalia and the skin , unlike those to the pelvic and abdominal risk structures , showed signicant differences . 
2 differences in inguinal dose distribution using the clinical target volume ( ctv ) denition of the radiation therapy oncology group ( rtog ; a and c ) and the british national guidance ( bng ; b and d )  . 
ctv of bng expands more caudally and medially and leads to a signicantly greater dose to the skin and the genitalia both sexes was about 20 gy in all plans . 
concerning the vulva ( eight patients ) , the dose parameters did not differ greatly . the skin turned out to be the organ showing the greatest differences between the dose parameters of the four target volumes . 
the v10v20 gy values were signicantly lower in the rtog ( 358 cc and 80 cc ) compared to the three other guidelines ( 388398 cc and 96107 cc )  . 
although current contouring atlases refer to imrt , the common constraints are often related to 3d conformal irradiation [ 20 ]  . pelvic region : the recommendations of the various guidelines concerning the radial margins of the ctv for the pelvis differ only marginally ( table 1 )  . 
in our study , the dose parameters were slightly higher than the constraints of 30 gy ( 200 cc ) and 35 gy ( 150 cc ) , respectively , recommended by rtog 0529 [ 12 ]  . 
the lns were possibly not properly covered by the elective clinical target volume ( ctv ) recommendations of the radiation therapy oncology group ( rtog , red outline ; d ) and the australasian gastrointestinal trials group ( agitg , turquoise outline ; e ) , but completely included in the ctv of the british national guidance ( bng , purple outline ; f ) v40 gy have been identied as signicant dose parameters regarding acute gastrointestinal toxicity using imrt in anal cancer patients . 
a further argument for the rather high dose prescription for the pelvic lymph drainage is in our opinion the fact that in four patients , the ptv was slightly above the bifurcation of the iliac artery due to extensive locoregional ln involvement . 
in a previous study , we were able to show that the anatomical relationships between these soft tissue structures and bony structures differ signicantly between patients [ 10 ]  . 
therefore , evidence - based recommendations for target volume denition of the inguinal region in anal cancer are needed . the fundamentally dreaded side effects of radiotherapy to the groin are lymphatic edema caused by inguinal brosis . 
even if the absolute dose to the testicles is relatively low , we recommend considering special protection of the genitals . the d50% of the vulva was below 17 gy in each group ( rtog 0529 constraints : 30 gy )  . 
the university of florida presented long - term toxicity in 164 patients after elective radiation ( > 70% of the patients with 45 gy ) of the groin in pelvic 374 strahlenther onkol ( 2020 ) 196 : 368375 cancers . 
only three of them developed mild genital edema [ 24 ]  . the greatest relative and absolute differences concerning the dose parameters between the different ctvs related to the skwe authenticated a correlation between the skin dose and the inguinal ptv volumes . 
identied 13 of 164 patients ( 8% ) with inguinal brosis after elective radiation ( > 70% of the patients with 45 gy ) of the groin . none of these cases was severe or correlated with a decrease in quality of life [ 24 ]  . to make clear recommendations for contouring of the inguinal region , results of studies dealing with the site of locoregional failure after imrt of ac patients should be taken into consideration . 
in daily practice , physicians perform a risk - adapted contouring of individual cases with individual anatomy , which will certainly differ from the different guidelines . moreover , it is difcult to standardize terms like the inguinal region should be contoured as a compartment with any identied nodes . 
in order to avoid inguinal recurrence and to protect relevant oars , further investigations are needed to generate uniform standards for the denition of the elective clinical target volume in the inguinal region . funding this research did not receive any funds from funding agencies in public , commercial , or not - for - prot sectors . authors contribution sc treated the patients and provided the data and study infrastructure . 
the complete dataset can be obtained from the authors by interested readers upon formal request . funding open access funding provided by projekt deal . compliance with ethical guidelines conict of interest h . 
combs declare that they have no competing interests . ethical standards the study was performed in accordance with the ethics standards at the technical university of munich ( ethical vote : 385 / 18 s )  . 
name of committee : ethikkommission der technischen universitt mnchen . open access this article is licensed under a creative commons attribution 4.0 international license , which permits use , sharing , adaptation , distribution and reproduction in any medium or format , as long as you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons licence , and indicate if changes were made . 
if material is not included in the articles creative commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use , you will need to obtain permission directly from the copyright holder . 
vavricka1 , 2 benjamin misselwitz1 , 5 norbert lombriser4 simon btikofer1 georg keilholz4 helmut kranzbhler4 received : 27 may 2019 / accepted : 17 october 2019 / published online : 24 january 2020 springer - verlag gmbh germany , part of springer nature 2019 abstract purpose radiochemotherapy is the standard treatment for anal carcinoma ( aca )  . 
ob diese vorteile auch einen klinischen benet bringen , wurde bis jetzt nur ungengend untersucht . methodik es erfolgte eine retrospektive analyse von 82 patienten mit der neudiagnose eines aca , mit einem vergleich zwischen patienten , die mit imrt versus mit der traditionell durchgefhrten 3d - konformalen radiotherapie ( 3d - crt ) behandelt wurden . 
es wurde der einuss der imrt auf das erreichen einer klinischen remission sowie auf rezidivrate und nebenwirkungen untersucht . ergebnisse die remissionsrate 1 jahr nach ende der bestrahlung der patienten lag in der imrt - gruppe bei 97 , 5 % ( 39 / 40 ) vs . 
in the 1970s , nigro and colleagues demonstrated the efcacy of combined radiochemotherapy [ 3 ] , offering the possibility of cure with an excellent functional outcome without the necessity of a permanent colostomy . since then , surgery has been reserved for cases with persistent or recurrent disease . 
radiochemotherapy as standard of care was conrmed by additional randomized controlled trials , with radiochemotherapy being superior to radiotherapy alone [ 49 ]  . 358 strahlenther onkol ( 2020 ) 196 : 356367 radiation of the anal region is challenging due to its proximity to dose - sensitive structures such as skin / genitalia , bladder , rectum , small bowel , bone ( pelvis and femoral head ) , and bone marrow . 
the selectivity of radiation techniques has improved tremendously during recent decades , rst by replacement of 2d planning by 3d ct - guided radiochemotherapy techniques [ 10 , 11 ]  . 
imrt allows reduction of radiation dose to adjacent organs , thereby potentially limiting toxicity and allowing application of higher doses within a shorter overall treatment time [ 2 , 18 ]  . 
however , to the best of our knowledge , there has been no randomized trial comparing conformal 3d radiotherapy with the new imrt technique and the potential benets of imrt have been insufciently documented . 
our aim was therefore to compare imrt and conventional 3d ct - guided radiation in terms of efcacy and acute and chronic side effects in a retrospective single - center study . patients and methods we performed a retrospective analysis of all patients referred to triemli hospital , a tertiary care center and teaching hospital in zrich , switzerland , from 1999 until 2013 for treatment of anal carcinoma . 
patients were identied by an automated search within the internal clinical information systehistological prove of anal carcinoma was a requirement for inclusion and all patients with rectal carcinoma were excluded . 
the study protocol was approved by the local ethics committee of zurich county ( registration kek - zh 2010 - 0555 ) and the requirement for informed consent from individual patients was waived by the local ethics committee . 
the study was performed according to the declaration of helsinki . treatment of anal carcinoma consisted of radiotherapy over a course of 28 days , either conventionally planned ( three - dimensional conformal radiotherapy , 3dcrt ; 19992008 ) , or as intensity - modulated radiation therapy ( imrt ; 20082013 )  . 
3d - crt followed a sequential regimen with 25 fractions of 1.8 gy to a total dose of 45 gy to the primary tumor with regional lymph nodes plus a boost of 5 fractions of 1.8 gy to a total dose of 9 gy , directed at the primary tumor . 
the elected lymph drainage region ( inguinal and pelvic lymph nodes ) was treated with 30 fractions of 1.5 gy to a total dose of 45 gy . furthermore , patients received 5 - uoruracil ( 5 - fu ) using a dose of 1000 mg / m2 per day on days 14 ( week 1 ) and days 2932 ( week 5 ) as a continuous 24 - hour intravenous infusion , and a dose of 10 mg / m2 of mitomycin as an intravenous bolus at day 1 and 29 ( maximum single dose 20 mg )  . data collection and denitions our cohort of aca patients has been described previously [ 19 , 20 ]  . 
tumor classication followed the seventh edition of the american joint committee on cancer tnm staging [ 21 ]  . after end of therapy , patients were clinically assessed after 3 , 6 , and 12 months , then every 6 months up to 3 years , then yearly until death or loss to follow - up . 
complete response ( cr ) was dened as lack of evidence of any residual disease in all investigations including history , clinical examination , imaging , and endoscopy at 6 months after the end of therapy . 
for some patients , suspicious residual lesions remained at 6 months ; however , for all these individuals , follow - up at 12 months conrmed complete response and the response rates at 6 and 12 months were identical . one patient died during radiochemotherapy due to sepsis , and in one patient , metastases were detected immediately after therapy ; these two patients were included in the analysis and counted as treatment failures . 
therefore , 82 patients were available for the analysis of side effects but only 79 for the follow - up analysis . regarding time , the date of diagnosis ( histology ) was used as a reference : the date was expressed as days after january 1 , 2000 . 
comorbidities were dened as relevant medical conditions requiring ongoing management including congestive heart failure , hiv infection , copd , diabetes , or history of neoplasia . strahlenther onkol ( 2020 ) 196 : 356367 fig . 
1 flowchart of our study . 3d - crt three - dimensional computational radiotherapy , imrt intensity - modulated radiotherapy entered radiotherapy : n = 95 pallia ( cid : 2 ) ve intent : treatment of recurrent disease : n = 6 first therapy & cura ( cid : 2 ) ve intent : n = 82 included into inten ( cid : 2 ) on - to - treat analysis 3d - crt n = 42 imrt n = 40 n = 82 included into analysis on acute toxicity lost to follow up : n = 3 n = 79 included into analysis on late toxicity and outcome data analysis to calculate differential effect of radiation techniques , patients treated with imrt were compared to patients treated with 3d - crt . 
calculations were performed using prism ( graphpad , san diego , ca , usa ) version 6.0. for the multivariate analysis , data were imported into a table in matlab ( version r2017b ; mathworks , natick , ma , usa )  . 
a cox proportional hazard model was calculated using the matlab coxphit function , controlling for the same confounders as for the generalized linear model . literature research a literature search was performed on january 29 , 2018 in pubmed , using the search terms ( anal cancer or anal carcinoma ) and imrt . 
all publications comparing 3d - crt with imrt in either an observational or interventional setting with data on oncological outcome ( overall survival , progression - free survival , and / or locoregional tumor control ) and / or side effects ( general , gastrointestinal , or skin toxicity ) were included . 
our pubmed search revealed 151 publications , of which 8 publications fullled all inclusion criteria [ 2330 ] , plus one additional publication via the google search [ 31 ]  . 
demographic data , tumor staging , and key parameters of oncological therapy are presented in table 1 . 42 patients were treated with 3d - crt ( years 19992008 ) , 40 patients with imrt ( years 20082013 )  . 
in the 3d - crt group , radiation was terminated early in three patients at 32.4 , 34 , and 40 gy , respectively , due to severe side effects . 
in a multivariate regression analysis , only t stage of the tumor and imrt treatment were signicantly associated with cr at 1 year ; other potential confounders such as age , time of treatment , gender , tumor tnm stage , comorbidities , radiation dosage , sib , vmat ( volumetric - modulated arc therapy ) , 5 - fu , and mitomycin treatment were not signicantly associated with cr ( table 3 )  . at the end of follow - up , 81% of patients were free of detectable disease . 
for all predictions , the number of eligible patients , the p - value of the model as well as the estimate and p - value for each predictor are indicated . 
if the analysis was restricted to recurrences , no predictors could be detected . after complete response at 1 year , 6 recurrences of aca were observed ( 2 after 3d - crt and 4 after imrt )  . 
recurrences were mainly observed at distant sites ( 2 / 2 after 3dcrt , 3 / 4 after imrt ) in the liver , brain , small intestine , and lung . 
only in a single case ( after imrt ) was tumor growth in the anal canal and inguinal lymph nodes observed [ 19 ]  . acute side eects of treatment relevant side effects were reported by the majority of patients . 
rates of diarrhea were higher for imrt treatment ( supplementary figure s2a ) and imrt was associated 362 strahlenther onkol ( 2020 ) 196 : 356367 table 4 prediction of complete response at the end of the study . 
a multivariate analysis conrmed protective effects of imrt treatment for more skin toxicity ( p = 0.00092 , table 3 )  . length of hospitalization radiochemotherapy was performed as an in - patient procedure for most patients ( 70 / 80 , 77% ; rates for in - patient treatment : 87.5% with imrt , 65% with 3d - rct , not signicant )  . 
several chronic problems including proctitis ( 14% ) , anal pain ( 18% ) , anal ulcerations ( 12% ) , intermittent chronic diarrhea ( 18% ) , some degree of incontinence ( 26% ) , and stulae ( 7% ) were noted ( table 2 , supplementary figure s3 )  . 
the rates of these side effects did not differ signicantly between imrt and 3d - crt , and no multivariate regression analysis was performed . systematic literature search our systematic literature search for studies comparing effects and side effects of 3d - crt and imrt revealed 10 publications ( table 5 ; [ 17 , 2331 ] )  . 
we report better tumor control , less skin toxicity , and a trend toward shorter hospitalization in patients treated with imrt . strikingly , skin toxicity was signicantly reduced upon imrt treatment and this difference remained robust in a univariate and a multivariate analysis . 
skin toxicity upon imrt was reported in our study and in seven previous studies comparing imrt with 3d - crt ( table 5 ; [ 17 , 2329 ] )  . reduction of skin toxicity ( dened as grade 2 or 3 ) was signicant in three studies [ 17 , 24 , 28 ] , with a clear trend towards lower skin toxicity in imrt in four of the other publications . 
is the largest and most detailed , comparing prospective data from the rtog - 0529 trial with imrt to historical 3d - crt data of the rtog - 9811 trial [ 17 ]  . reduced skin toxicity is likely due to better focusing of radiation , avoiding the integument . 
in our study , reduced skin toxicity appears remarkable in light of the more aggressive treatment performed in the imrt group : radiation dosage was increased , along with a higher fraction of individuals receiving 5 - fu and mitomycin treatment , and a lower fraction of individuals with a 5 - fu dose reduction . since skin affections frequently limit radiation treatment , imrt might have enabled more aggressive treatment in some patients . however , not all side effects of radiation treatment were superior in the imrt group . 
one possible explanation could be a different disstrahlenther onkol ( 2020 ) 196 : 356367 364 strahlenther onkol ( 2020 ) 196 : 356367 tribution of radiation in the small intestine . 
 [ 32 ] , there was less highdose radiation to the small intestine on imrt , whereas lowdose radiation ( e.g. , 30 gy dose bath ) was more extensive in imrt than in 3d - crt . 
this difference , together with higher treatment rates and dosages for 5 - fu and mitomycin in the imrt group , might to some extent explain the increase in acute diarrhea in the imrt group . gi toxicity was also reported in 6 previous studies with mixed results [ 17 , 23 , 24 , 26 , 28 , 29 ]  . 
three studies reported on gi side effects in general [ 17 , 23 , 24 ] , the others also reported on single symptoms such as diarrhea and / or rectal bleeding [ 26 , 28 , 29 ]  . 
in contrast , lower hematological toxicity for imrt compared to 3d - crt for the treatment of cervical cancer was demonstrated in some [ 33 ] but not all studies [ 34 ]  . altogether , the combination of benecial effects of imrt and a more aggressive treatment approach might result in a similar overall tolerability of imrt treatment , indicated by a trend toward shorter duration of hospitalization . 
while the average length of hospitalization was shorter upon imrt treatment , and especially long - term hospitalizations beyond 58 days did not occur in the imrt group , this difference failed to reach statistical signicance . a signicantly reduced risk of hospitalization in the rst 6 months after therapy was noted for imrt in a previous study ( hazard ratio 0.70 ; 95% ci 0.580.84 ; p < 0.0002 ) [ 30 ] and a shorter treatment time was reported in a large database analysis [ 35 ]  . our data suggest better local tumor control upon imrt treatment . 
out of 39 patients treated with 3d - crt , no complete response at 1 year was achieved in 8 , compared with only 1 patient without cr treated with imrt . 
apparently , imrt allows a more localized focus of radiation in the primary tumor area which might have received more radiation volume and / or more homogenous radiation over its entire volume for maximum oncological effects . 
however , we cannot exclude that higher rates and intensities of 5 - fu and mitomycin treatment in the imrt group contributed to better tumor control . in line with good local tumor control in the imrt group , tumor progression was detected within the 6 months after treatment in 6 individuals with 3d - crt vs . 
of note , most recurrences occurred at systemic sites ( 2 / 2 for 3d - crt , 3 / 4 for imrt ) , conrming good local control of the tumor after radiochemotherapy . strahlenther onkol ( 2020 ) 196 : 356367 to the best of our knowledge , there is no randomized controlled comparison for imrt vs . 
better local tumor control , progressionfree survival , and overall survival were reported in one previous study [ 23 ] ; however , most studies reported highly similar oncological outcomes for imrt and 3d - crt ( table 5 ; [ 2428 , 30 ] ) , with an overall survival at 23 years of 7193% , and a progression - free survival of 6782% [ 2426 ]  . 
it should be noted that in the single study with favorable oncological outcome upon imrt treatment vs . 3d - crt , the outcome of the 3d - crt group was considerably worse ( 52% overall survival after 3 years ) than in all other studies , including ours [ 23 ]  . 
improvement of local tumor control in our study upon imrt treatment is encouraging ; however , it remains unclear why this effect has not been observed in most previous studies . 
this suggests that better local control will translate into small improvements in overall outcomes , detectable only in very large analyses . radiochemotherapy was accompanied by long - term side effects in a signicant fraction of patients . 
sexual dysfunction was common in males and females but did not differ between imrt and 3d - crt treatment . treatment of aca continues to evolve , and besides the improveintroduction of imrt , a number of potential ments in aca therapy have been advanced in recent years . dose escalation in primary radiochemotherapy has been suggested ; however , no benet was apparent in a recent randomized controlled trial ( unicancer accord 03 trial ) [ 36 ]  . 
the checkpoint inhibitor nivolumab , used in treatment of many different malignancies such as melanoma and head and neck cancers [ 37 , 38 ] , has been successful in treatment of metastatic anal cancer [ 39 , 40 ] , with response in up to 24% of patients . 
cetuximab , an epidermal growth factor improve response to receptor ( egfr ) antibody , might treatment ; however , the high toxicity prevents it from general use apart from in highly selected populations [ 42 , 43 ]  . deep regional hyperthermia is another potential add - on modality , which has , in small studies , shown a benecial effect when added to conventional chemoradiotherapy [ 44 , 45 ]  . 
we therefore cannot entirely exclude the possibility that in addition to imrt , other treatment variables were improved in parallel , incrementally affecting outcome and side effects . for this reason , time was included as a confounder in all multivariate analyses , but imrt was consistently found to explain any given variation better than the continuous variable time . 
nevertheless , our data provide a real - world experience on how switching from imrt to 3d - crt might change outcome and side effects in radiochemotherapy for anal carcinoma . in summary , our data show that imrt can reduce local side effects of radiochemotherapy such as skin toxicity and enable a more aggressive radiochemotherapy . 
we found better tumor control rates with imrt at 6 months to 1 year after the end of treatment , suggesting signicant oncological benets of imrt over 3d - crt . acknowledgements the authors would like to thank brian lang , department of biosystems science and engineering , eth basel , for help with the statistics . author contribution msa , bm , sv , nl : study design . 
current treatment consisted of sbrt alone ( n = 15 ) or selective transarterial chemoembolization ( tace ) followed by sbrt to the same lesions ( n = 21 )  . 
eight patients received additional local treatments to different lesions . liver function was predominantly moderately restricted ( child a : 29 , child b : 6 , child c : 1 )  . 
treatment planning was based on 4d - computed tomography , dose / fractionation varied depending on location and size , most commonly 3 fractions of 12.5 gy ( 65% isodose ) and 5 fractions of 8 gy ( 80% isodose )  . results median follow - up was 15 months . 
new hepatic lesions occurred in 19 patients ( 52% ) , 1and 2 - year freedom - from - hepatic - failure ( ffhf ) was 39% and 32% , respectively . only the number of treated lesions was predictive for ffhf . 
sixteen patients have died , resulting in 1and 2 - year overall survival ( os ) of 64% and 41% , respectively , signicantly impacted by the number of treated lesions and childpugh class . 
6 patients ( 17% ) received liver transplantation ( olt ) after sbrt , of whom 5 showed pathological complete remission . conclusion sbrt ( tace ) in highly pretreated hcc is effective and associated with excellent lc and low toxicity . sbrt may be used as denitive or bridging treatment prior to olt . 
15 , 81377 munich , germany 4 ccu molecular radiation oncology , german cancer research center , heidelberg , germany 5 department of radiotherapy and radiation oncology , paracelsus medical university salzburg , landeskrankenhaus , mllner hauptstrae 48 , 5022 salzburg , austria strahlenther onkol ( 2020 ) 196 : 334348 stereotaktische bestrahlungstherapie bei patienten mit hepatozellulrem karzinom im rahmen multimodaler behandlung zusammenfassung ziel ziel war die retrospektive evaluation der bestrahlungstherapie mittels krperstereotaxie ( sbrt ) beim hepatozellulren karzinom ( hcc )  . methoden die retrospektive analyse umfasst 36 patienten ( 45 lsionen ) , welche zwischen 2011 und 2017 behandelt wurden . 
die therapieplanung erfolgte mittels 4 - d - computertomographie , die dosis / fraktionierung war abhngig von lokalisation und gre , blicherweise 3 12 , 5 gy ( 65% - isodose ) oder 5 8 gy ( 80% - isodose )  . ergebnisse die mediane nachbeobachtungszeit betrug 15 monate . 
der einzige signikante prdiktive faktor war die verwendung einer bauchpresse . bei insgesamt 19 patienten ( 52% ) traten neue hepatische lsionen auf , das leberspezische krankheitsfreie einund 2 - jahres - intervall ( ffhf ) betrug 39% bzw . 
bei 6 patienten ( 17% ) wurde eine lebertransplantation nach sbrt durchgefhrt , hiervon zeigten 5 eine komplette pathologische remission . schlussfolgerung die sbrt ( tace ) bei multipel vorbehandeltem hcc ist effektiv , toxizittsarm und erzielt eine exzellente lokalkontrolle . 
unfortunately , many patients are not suitable for resection due to comorbidities , poor liver function , major vascular involvement or multifocal spread of disease [ 1 , 3 ]  . according to common guidelines , locoregional therapies should be considered in these patients as denitive treatment or as bridging in patients awaiting liver transplantation [ 4 ]  . 
locoregional treatments are broadly categorized into arterially directed therapies ( transarterial chemoembolization [ tace ] , transarterial chemoembolization with drugeluting beds [ deb - tace ] , or selective internal radiother336 strahlenther onkol ( 2020 ) 196 : 334348 apy [ sirt ] ) and into local ablative techniques like radiofrequency ablation ( rfa ) , percutaneous alcohol injection , microwave ablation , or minimally invasive stereotactic body radiotherapy ( sbrt )  . 
each of these treatments has its limitations and must be weighed in particular against the anticipated remaining liver function , the extent and location of the disease , and the existing co - morbidities . 
for example , lesions directly adjacent to major vessels or bile ducts are not well suited for rfa [ 5 , 6 ] and patients with portal vein thrombosis are not eligible for tace [ 2 , 6 ]  . 
radiotherapeutic treatment paradigms have changed in the last decades in favor of highly conformal and precise treatment techniques such as intensity - modulated radiotherapy ( imrt ) and stereotactic body radiation therapy ( sbrt )  . 
it sufciently spares dose to adjacent organs at risk due to its sharp dose fall - off outside the target , resulting in low toxicity rates , especially regarding radiation - induced liver disease ( rild ) , compared to the historical reports using conventional radiation therapy techniques [ 710 ]  . 
due to the enhanced biological effectivity of large single doses , adequate tumor control is maintained , as shown by the experience from other body sites [ 1113 ]  . for example , in stage i lung cancer , sbrt has shown to result in at least equal local control and overall survival rates compared to surgery [ 14 ]  . 
several retrospective studies have shown encouraging outcomes , with low to moderate toxicity and high local control rates ( 1 year lc : 90100% ) [ 1 ] , but no randomized trials comparing sbrt to other local treatment options have been conducted so far and only scarce prospective data on the employment of sbrt in the treatment of hcc are available . 
we therefore report our experience with sbrt with or without prior selective tace to the same lesion in patients with hcc . methods sbrt has been implemented for hcc treatment at our center in 2011 . 
for the current analysis , we retrospectively analyzed all hcc patients who underwent sbrt to 12 liver lesions . patient evaluation pretreatment investigations included at least mri and / or contrast - enhanced multiphasic liver ct , ct staging to exclude distant metastases , and liver function tests . 
the indication for sbrt was seen in patients ineligible for other local treatment options ( except tace ) or in case of multifocal hcc in combination with other local treatments . 
the decision for listing was made by an interdisciplinary transplant board ( without the presence of a radiation oncologist ) based on internationally accepted criteria ( milan criteria , model for end - stage liver disease = meld score ) and legal considerations regarding transplant surgery . 
the strategy for bridging was chosen based on the size , localization , and number of lesions as well as on patient - related factors such as tolerability of surgery , comorbidities , and performance status , taking into account all possible advantages and disadvantages of the available techniques on an individual basis . treatment treatment of the irradiated lesions consisted of sbrt alone in 15 patients , while 21 patients received selective tace to the same lesions upfront of sbrt ( within 6 weeks )  . 
27 / 36 patients had a median of 2 ( range 18 ) previous local treatments ( surgery , rfa , tace , or sirt ) , only 9 patients were treatment nave . 
1 number of treated patients per year from 2011 to 2017 was implemented in 2014 , and since then , only discarded in patients not able to tolerate compression ( for example , patients with large herniations after previous surgery )  . 
gross tumor volume ( gtv ) was contoured as the visible tumor on the free - breathing ct and on all respiratory phases of the 4d - ct supplemented by information from mri , if available . 
the most common schemes were 3 fractions of 12.5 gy prescribed to the 65% isodose ( 64% ) and 5 fractions of 8 gy to the 80% isodose ( 22% ) delivered every other day . 
treatment was performed using daily cbct image guidance . follow - up examinations ( including physical examination , laboratory tests and mri / ct of the liver ) regularly took place at our department or the departments of gastroenterology / oncology every 3 months for the rst year , every 6 months for the second year , and annually thereafter . statistical and legal considerations acute and late toxicity was scored according to ctcae v4.03. 
acute toxicity included events from the time of sbrt until 90 days after ; late toxicity was dened as events occurring after more than 90 days from sbrt until disease progression . 
biologically effective dose ( bed ) at isocenter ( maximum dose ) was calculated according to the formula bed = nd [ 1 + d / alphabeta ] with n being the number of fractions , d the single dose , and alphabeta = 10 for tumor control . 
freedom - from - hepatic - failure ( ffhf ) was dened as absence of tumor progression in the liver . all time - to - event data were calculated from the rst day of sbrt using the kaplanmeier method . 
median age was 63 years ( 3183 ) , 72% were male and the median karnofsky performance score ( kps ) was 90% ( 60100% )  . hcc was based on liver cirrhosis in all patients , with a moderately restricted liver function in the majority ( child a : 29 [ 81% ] , child b : 6 [ 17% ] , child c : 1 [ 3% ] )  . 
the main causes of the underlying liver cirrhosis were toxic ( 28% ) and infectious ( hepatitis b / c ) liver damage ( 31% ) , 2 patients had autoimmune hepatitis ( 6% ) and the remaining 13 ( 36% ) had cryptogenic liver cirrhosis . 
similar results were obtained if the 6 patients with olt were excluded from analysis ( data not shown )  . ct - guided ducial placement was feasible without any severe acute complications . 
aside from mild side effects of grade 1 in 14% and grade 2 in 8% ( mainly fatigue and gastrointestinal symptoms like nausea or abdominal pain ) , only one patient ( 3% ) developed a severe acute toxicity . 
two showed marked deterioration of liver function , with a decline in cp class from a ( 6 points ) to class b ( 8 points ) scored as grade 3 ; one of them also showed symptoms of fatigue , ascites , and abdominal pain clinically consistent with rild symptoms , scored as grade 3 . 
however , our predened dose constraints ( dened as mean liver dose minus gtv < 18 gy and > 700 ml of liver receiving less than 15 gy ) were met in both patients . 
4 overall survival ( a : entire cohort , b : according to child pugh class ) 344 strahlenther onkol ( 2020 ) 196 : 334348 ( continued ) overall surfig . 
4 ( continued ) overall survival ( e : according to the number of actually overall treated lesions ) a centrally located large hcc developed cholangitis and a stricture of the proximal common hepatic bile duct . 
he was treated by antibiotics and repeated stent placement , but this side effect nally resolved ( toxicity scored as grade 3 )  . maximum dose to the central biliary tract was 37.5 gy in 3 fractions in this patient . 
causes of the underlying liver cirrhosis were alcohol related in 2 patients , infectious ( hepatitis b / c ) in 2 patients , and the remaining 2 patients had autoimmune hepatitis . 
all patients fullled easl criteria for diagnosis and milan criteria for olt eligibility . olt was performed after a median interval of 6 months ( range 18 months ) from sbrt . 
all patients remained locally and distantly controlled until olt . in 5 / 6 patients and 6 / 7 lesions , no residual hcc ( pathologic complete response ) was found in the explanted liver . 
one patient died shortly after olt due to postoperative complications ( septic shock ) and one due to distant failure 9 months after olt , resulting in 1and 2 - year os rates of 66% . 
 [ 24 ] observed a 1 - year lc control rate of 87% in the largest published prospective ( phase i / ii ) trial including 102 hcc patients , which showed similar 346 strahlenther onkol ( 2020 ) 196 : 334348 patient characteristics to our cohort with regard to lesion size and number . 
the high ( so - called ablative ) doses used within this approach seem to effectively destroy all malignant cells in the vast majority of the treated lesions , as shown by the high pathological complete response rate of 86% achieved in our patients who received olt later on . 
abdominal compression has been shown to reduce respiratory motion of the liver [ 33 ] , thus resulting in smaller itv and ptv volumes , which might have prompted a more adequate target volume coverage . however , this nding should be regarded very cautiously given the low number of events in our study . 
in contrast , we could not conrm the prognostic value of several factors described by others like dose , fractionation , and lesion size [ 9 , 21 , 23 ] , probably again due to the small sample size and the low number of events . regarding os , we observed 1and 2 - year rates of 64% and 41% . 
these ndings are in the range of published series describing 1 - year survival rates of 3294% [ 9 , 1631 ] , although the wide range clearly indicates the inclusion of inhomogeneous patient groups in the published reports . 
 [ 27 ] analyzed 132 chinese patients retrospectively and reported a non - signicant but remarkable decrease in 2 - year os of 85% , 77% , and 63% in patients with 1 , 2 , or 3 lesions . 
however , they included only patients with up to three lesions with a single diameter < 6 cm and reported a signicant decrease in os for patients with a cumulative gtv diameter of > 5 cm , indicating that patients with more than one lesion may be at a higher risk for death . 
for example , marrero et al . [ 34 ] analyzed 239 patients and found that bclc stage had the best prognostic stratication compared to several other commonly used staging systems . in contrast to the encouraging results with regard to lc and os , we observed a high number of liver outeld failures translating into rather poor 1and 2 - year ffhf rates of 39% and 32% , respectively . 
 [ 28 ] enrolled 101 patients in a phase ii trial combining tace and sbrt and found a 3 - year intrahepatic - failure - free rate of only 34% , although only patients with a single lesion were eligible . 
this may implicate that patients with multiple lesions detected on imaging have a higher risk for further subclinical disease in general and might not be ideal candidates for sbrt or other local treatments . 
however , most of our patients had already been treated with other local treatments and received sbrt only because they were deemed ineligible for other treatments except tace or systemic agents . 
in this heavily pretreated cohort , the risk for developing further recurrences might be simply increased compared to treatment - nave patients due to selection of an unfavorable biology . toxicity with the possibility of outeld failures and the need for salvage treatments after locally ablative therapies , preservation of liver function and toxicity issues gain importance in the decision process for specic treatments . 
distinctly higher rates ( 1329% ) of a decline in cp class after sbrt have been reported by others [ 18 , 24 , 35 ] , although some authors described a marked recovery over time [ 24 ]  . 
however , in the absence of randomized trials and with limited data from prospective studies , retrospective evaluation seems a suitable way to gain more information in a heterogenous patient group treated with a variety of slightly different approaches . sbrt as bridging to transplant conclusion olt is the most effective treatment for hcc with underlying cirrhosis [ 37 ]  . 
therefore , effective treatments have to be offered in between to maintain disease control until availability of a donor organ ( so - called bridging ) [ 37 ]  . 
similarly to denitive treatment , different methodsincluding rfa , tace , sirt , and sbrtare currently in use , depending on the location and size of the lesion and patients comorbidities [ 37 ]  . 
in our cohort , we observed a pathological complete response ( pcr ) in the explanted liver in 5 / 6 ( 83% ) patients treated with olt after sbrt at a median interval of 6 months . 
a longer time interval from sbrt to olt may theoretically also result in higher pcr rates ; however , our median interval ( 6 months ) was in the range of the mentioned studies ( 48 months ) [ 3840 ]  . 
however , given the small number of patients , it cannot be fully ruled out that the difference occurred simply by chance or was triggered by other factors . sbrt in highly pretreated patients with hcc resulted in excellent lc and acceptable os with low toxicity . 
sbrt can be used as denitive treatment or as bridging to olt . author contribution sg performed data acquisition and participated in patient treatment , statistical analysis , and in drafting the manuscript . ch participated in treatment of the patients and statistical analysis . 
fr participated in data acquisition , statistical analysis , treatment of the patients , drafting the manuscript and critically reviewed the data and the manuscript . compliance with ethical guidelines conict of interest s . 
rder declare that they have no competing interests . ethical standards the study was approved by the ethics committee of the university of munich ( lmu ) , reference number 617 - 16 . 
informed consent was obtained from all individual participants included in the study . strahlenther onkol ( 2020 ) 196 : 405 correction correction to : timing of thoracic radiotherapy is more important than dose intensication in patients with limited - stage small cell lung cancer : a parallel comparison of two prospective studies xiao hu1 bing xia2 , 3 yong bao4 yu - jin xu1 jin wang1 hong - lian ma1 fang peng4 ying jin5 min fang1 hua - rong tang1 meng - yuan chen1 bai - qiang dong1 jia - nan jin1 xiao - long fu3 , 6 ming chen1 published online : 20 february 2020 springer - verlag gmbh germany , part of springer nature 2020 correction to : strahlenther onkol 2019 the original version of this article unfortunately contained a mistake . 
we assessed the impact of different clinical , prognostic , and treatment - related factors on selected items from c30 and br23 using a dependence analysis . results out of 315 patients treated with prt / pcrt in the years 1991 to 1999 , 203 patients were alive at long - term follow - up after a mean of 17.7 years ( range 1421 )  . 
37 patients were lost to follow - up and 61 patients refused to be contacted , leading to 105 patients ( 64 patients after bcs and 41 after me ) being willing to undergo further clinical assessment regarding qol outcome . 
historically , preoperative radiotherapy ( prt ) has predominately been used in primarily unresectable disease , prior to a planned mastectomy ( me ) [ 4 , 5 ] or in inoperable cases . 
but until now , the concept of prt has been tested mainly in prospective or retrospective cohorts without adequate control arms [ 613 ]  . only one randomized trial has compared adjuvant radiotherapy ( rt ) , neoadjuvant rt , and mastectomy ( me ) alone [ 14 , 15 ]  . 
however , the authors found no long - term differences in recurrence - free and overall survival between the preand postoperative rt arms . in recent years , shifting the systemic therapy to the preoperative setting in localized disease has resulted in equivalent oncological results with the potential to individualize the adjuvant treatment based on the pathological response to the initial therapy . 
the integration of neoadjuvant radiotherapy into this new treatment approach has several theoretical advantages [ 20 ]  . the addition of rt improves downstaging of the primary tumor and results in a higher number of pathological complete responses at the time of surgery , which might facilitate easier approaches in conserving the affected breast [ 21 ]  . 
the cosmetic reconstruction could be improved as the adverse effects of postmastectomy radiation are omitted . rt to the implant can result in capsular brosis , reconstruction failures , and reduced patient satisfaction with the reconstructed breast [ 22 ]  . nevertheless , the cosmetic outcome could be improved in bcs patients , since the heavily irradiated breast tissue ( especially high - dose irradiation in partial - breast treatment ) will be surgically removed after preoperative rt . 
furthermore , analysis of the effects of rt on the surgically removed tumors offers a great opportunity for translational research . however , the impact of preoperative rt on quality of life is not well studied . 
in particular , concerns about impaired wound healing following tumor resection in an area of inammation and altered vascular supply may lead to poorer cosmetic , functional , and symptomatic outcome . 
singlecenter series reported a high surgical complication rate of up to 45% [ 23 ]  . regarding these concerns , we recently published esthetic results of our patient cohort after neoadjuvant prt / prct , which were good to excellent in over 80% of the cases [ 24 ]  . 
apart from the aspect of objectively assessable cosmetic results , the measurement of patient - related outcomes is currently of great interest in clinical research and focuses on the development , evaluation , and application of quality of life ( qol ) measures [ 25 ]  . 
in view of the fundamental importance of patient - related outcomes , we now report on the qol measures of a patient cohort treated with prt / pcrt from 1991 to 1999 , focusing on the comparison with an age - matched healthy control group . materials and methods patient cohort patients with localized or locally advanced breast cancer were treated at the university hospital dsseldorf , germany , and the community hospital of gerresheim , germany , from 1991 to 1999 . 
briey , radiotherapy ( rt ) treatment consisted of neoadjuvant external beam radiation therapy ( ebrt ) with tangential elds to the breast / chest wall and the supra - / infraclavicular lymph nodes with 50 gy in 25 fractions . 
applied energy depended on the breast size : 6to 10 - mv photons in larger or 60co in smaller breasts . in case of medial tumor localization , a mammary chain eld ( combination of photons and electrons ) was added . patients undergoing bcs received a boost , with either interstitial brachytherapy of 10 gy and local hyperthermia or an electron boost of 5 2 gy . 
the regimens consisted of nitoxantrone or anthracycline - based chemotherapy ( doxorubicin or epirubicin combined with cyclophosphamide )  . 388 strahlenther onkol ( 2020 ) 196 : 386397 endocrine therapy with tamoxifen or lhrh agonists was given to hormone receptor - positive patients , while patients with hormone receptor - negative tumors did not receive any endocrine therapy . 
the decision regarding the most suitable type of surgical management was based on the original tumor size and was either a simple or a modied mastectomy with or without reconstruction or a breastconserving surgery with optional support by a latissimus dorsi ap as an autologous volume replacement . 
surgical interventions were performed at both centers . quality of life assessment this study reports on the long - term quality of life of assessable patients treated with neoadjuvant prt / pcrt . 
the qlq - c30 version 3.0 consists of 30 questions categorized in functional and symptom scales and provides a global score through two general questions concerning health and quality of life . qlq - br23 is a standard instrument for measuring qol in patients with breast cancer . 
the original questionnaire was developed in 1996 and has been subsequently updated . the questionnaire has 23 items with four possible answers each , ranging from not at all , a little , and quite a bit , to very much . 
results are reported using functional scales ( body image , sexual functioning , sexual enjoyment , and future perspective ) and symptom - related items ( systemic therapy side effects , breast symptoms , arm symptoms , and upset by hair loss )  . 
it is also common practice to classify the summary scores into four distinct categories with functional scales ( 025 : bad ; 2650 : moderate ; 5175 : good ; 76100 : excellent ) and symptom scales : ( 015 : excellent ; 2650 : good ; 5175 : moderate , 76100 bad ) [ 25 ]  . in order to further analyze our results , we compared them to a reference group of the german female general population [ 28 ]  . 
statistical differences were assessed using students t - test . the inuence of different clinical and treatment variables on general quality of life , fatigue , and pain according to qlq - c30 and qlq - br23 body image and breast and arm symptom scores was assessed using chi - square ( for normally distributed variables ) and spearmans rho correlation ( for other distributions )  . 
these variables were selected prior to the analysis as they were deemed to represent the most relevant endpoints and were most affected by rt . to further investigate the impact on global qol in bcs patients , we looked at the distribution of qol scores between different subgroups . 
to compare two normally distributed subgroups , a students t - test was used and an analysis of variance ( anova ) with a subsequent bonferronicorrected subgroup analysis was performed , if signicance was detected . 
this analysis was not possible for the me group , as the data for this population were not collected . for all calculations , the statistical analysis system spss ( statistical package for the social science , ibm , armonk , new york , usa ) , version 24 was used . results an overview of the different characteristics of patients treated with bcs or me after neoadjuvant treatment is shown in supplementary tables 5a , b . 
since not all patients of the initial study cohort were available and willing to undergo clinical assessment regarding qol after a median follow - up beyond 17 years , we compared the present cohort to the originally treated population . 
this was evident in a trend towards lower numbers of t4 tumors and hormone receptor - negative patients . qol was assessed in 105 patients , 64 who had received breast - conserving therapy and 41 patients following mastectomy . 
we also found a good qol in the other functional subscales , with values ranging from 7997% for good or excellent scores . likewise , the symptomatic summary scales also demonstrated good or excellent results in a majority of patients ( ranging from 72100% )  . 
this information was not available for me patients . in the correlation analysis of the three subscales of c30 ( global , pain , fatigue ) and the three subscales of br23 ( body image , breast and arm symptoms ) , we used multiple clinical characteristics as probable prognostic factors ( table 2 )  . 
as expected , age was signicantly correlated with global health status and pawe also found multiple statistically signicant correlations between type of surgery and global health status , fatigue , pain , and breast and arm symptoms . 
in contrast , the cosmetic global score had a signicant impact on body image and breast symptoms . for the bcs group we were able to investigate additional clinical features and their inuence on global health status ( qlq - c30 )  . 
on the right side are the pairwise comparisons using bonferroni corrections for multiple testing for tumor locations showing worse qol for lower outer quadrant tumors bmi body mass index , fu follow - up points , as their impact on absolute risk reduction is usually modest [ 2931 ]  . 
this has been increasingly recognized in recent years , which is reected in a rapid increase in publications on qol and their integration into large multicenter prospective trials . in this series , we report on the long - term qol results in women with localized or advanced breast cancer who underwent neoadjuvant chemotherapy and radiotherapy . 
we found that this cohort had higher functional and similar symptomatic qol as a healthy , age - matched reference control , suggesting that preoperative rt has no measurable negative impact on patients wellbeing . in contrast to the reported literature , bcs patients of the present cohort tended to have inferior qol results compared to those who underwent me . 
this procedure is no longer common practice today and reects the older surgical techniques used during the study to treat larger tumors with tissue replacement to optimize the cosmetic results . 
in accordance with previously published data , we detected no difference in qol between cobaltand linear accelerator - based radiation therapy [ 33 ]  . the dependence analysis showed an impact of reconstruction ( as a measure of asymmetry ) after mastectomy on qol , which is supported by the result that global subjective cosmetic results were also associated with improved qol scores . 
this is consistent with the prospective study by dujmovic and colleagues of 100 breast cancer patients who underwent surgical and adjuvant oncological treatment [ 34 ]  . they found that qol , measured by qlq - c30 and qlqbr23 , was highly impacted by breast asymmetry . analysis of the bcs patient subgroup showed that patients with tumors in the lower outer quadrants experience signicantly worse qol compared to other locations and this irrespective of ap support . 
however , it remains unclear whether this aspect is correlated to prct or not . the relatively high values for functional and symptombased qol in our cohort , compared to healthy age - matched references , is somewhat surprising . 
two effects can inuence the evaluation of long - term qol over 17 years after prt / prct . first , with prolonged follow - up , qol can improve due to strahlenther onkol ( 2020 ) 196 : 386397 the resolution of side effects . 
secondly , the basis of self - assessment in qol improves over time , this effect is known as response shift [ 37 ]  . according to this theory , patients adapt to their disabilities over a longer time and are glad that they are still alive after experiencing the high burden of cancer diagnosis and treatment [ 35 , 36 ]  . 
also reported a signicantly improved global health status in their cohort of bcs and adjuvant rt patients [ 37 ]  . likewise , the improved scores in pain and fatigue reported in our analysis might be attributable to these changes , which were seen by other experiences [ 38 ]  . 
the long time interval may make it difcult to assess the individual impact of chemotherapy or endocrine therapy , as well as different rt details , as the most clinically apparent side effects associated with these therapies have already disappeared . obvious caveats of this study are its retrospective nature , the lack of a comparison group , and the small numbers of patients . 
where available , the extent of comorbidities appeared to be small and probably would not have affected the present results . due to a lack of published data , a formal qol comparison between prct and the standard regimen of adjuvant rt and systemic therapy was not possible . 
a numerical comparison across trials shows better qol measures for postoperative treatment in comparison to our cohort [ 37 ]  . however , it is very likely that both cohorts included patients with different clinical and prognostic factors , which is why a comparison is hardly meaningful . taken together , the present study showed a good to excellent qol after a median follow - up of 17 years after preoperative chemoradiotherapy and different techniques of breast cancer surgery . 
comparative analysis of the qol of this patient cohort with an age - matched healthy control group demonstrated no disadvantages in qol except for diarrhea and appetite loss , which are not known to be associated with breast radiotherapy . 
therefore , preoperative radiotherapy followed by breast cancer surgery appears to conserve long - term qol . author contribution cm , cnk , eb , and wb had the idea , coordinated the work , and wrote parts of the manuscript . 
matuschek declare that they have no competing interests . ethical standards there was no ethics approval necessary , because in this meta - analysis , we were pulling numbers from the published manuscripts and pooling results . 
intraoperative radiotherapy ( iort ) during breast - conserving surgery for early breast cancer is an innovative technique applying low energy x - ray to the tumor bed immediately after removal of the tumor . iort is considered to reduce the risk of local tumor recurrence by directly targeting cells of the tumor bed and altering the local microenvironment . 
aim of this study was to investigate whether iort affects the outgrowth potential of breast adipose tissue - derived msc ( basc ) as part of the tumor bed . materials and methods after surgical tumor resection , biopsies of the tumor bed were taken before ( pre iort ) and after iort ( post iort ) and processed applying well - established protocols for asc isolation and characterization . results in all , 95% of pre iort tumor bed samples yielded persistently outgrowing basc with typical asc characteristics : broblastoid morphology , proliferation , adipogenic and osteogenic differentiation and asc surface marker expression . however , none of the post iort samples yielded persistent outgrowth of basc . conclusions after breast - conserving surgery , approximately 90% of local recurrences emerge in close proximity to the initial tumor bed , potentially reecting a signicant contribution of the tumor bed to relapse . 
this effect on tumor bed stromal cells might contribute to reduce the risk of tumor relapse and metastases . keywords intraoperative radiotherapy mesenchymal stromal cells adipose stromal cells tumor bed breast cancer the authors s . 
wuhrer contributed equally to the manuscript . parts of this work have been presented as poster and oral abstracts and are published as conference abstracts : p09 - 17 uhlig s , wuhrer a , stterlin m , tuschy b , berlit s , bieback k . intraoperative radiotherapy for breast cancer treatment efciently prevents breast adipose tissue - derived mesenchymal stromal cells outgrowth . 
germanstemcellnetwork 5th annual conference 2017 . vs - 6 - 4intraoperative radiotherapy of breast cancerinuence on mesenchymal stromal cells and the tumor beds micromilieu . anne wuhrer , stefanie uhlig , benjamin tuschy , sebastian berlit , marc stterlin , karen bieback . 
the idea of using local radiotherapy in general is to eliminate potentially remaining tumor cells in the tumor bed after surgery , considered as a major source for relapse [ 2 ]  . 
with irradiation taking place in the wound cavity directly after having removed the tumor , the risk of local or temporal miss is hypothetically nonexistent . as supported by the seed and soil theory , the wound healing process after surgery is likely to provide favorable growth conditions not only for the healthy tissue , but also for residual tumor clusters [ 3 ]  . 
furthermore , the fact that local control is correlated with an improvement in overall survival in an oncological disease with early metastatic spread implies that systemic progress might be substantially affected by mechanisms in the tumor bed [ 4 ]  . 
in the scope of breast cancer therapy , the impact of iort on the tumor bed stroma under in vivo conditions is scarcely investigated , mainly focusing on the wound uid and not on the cellular part of the tumor bed tissue [ 5 , 6 ]  . mesenchymal stromal cells ( msc ) , as a potential part of the tumor bed stroma , comprise a heterogeneous population of multipotent stem / stromal cells that can be isolated from a variety of different tissues including adipose tissue ( adipose stromal cells , ascs ) [ 7 ]  . 
yet , what presents itself as a benet on the one hand could be considered as a drawback for the oncological outcome , since these protective effects could not only support normal tissue but also tumor cells treated with radiotherapy [ 9 ]  . in allogeneic bone marrow transplant setting , stromal cells remain host - derived irrespective of the condition regime intensity [ 10 ]  . 
in fact , ex vivo cultured msc / asc are resistant to radiation withstanding even high radiation doses [ 11 ]  . the aim of this work was to analyze whether iort affects the outgrowth potential of basc , indicative for an effect on the tumor bed stroma . 
outgrowing cells were characterized against msc criteria . materials and methods patients and intraoperative radiotherapy a total of 20 breast cancer patients undergoing breast - conserving surgery with ( study collective ) and 21 without ( control collective ) iort were recruited after written informed consent was obtained . 
in women of the study collective , tumor bed biopsies were taken before ( pre ) and after ( post ) iort . iort was performed according to the targit - a protocol [ 4 ] : the intrabeam system ( carl - zeiss meditec ag , oberkochen , germany ) was used for intraoperative irradiation ( 50 kev x - ray )  . 
after excision of the tumor and pathoanatomical conrmation of free margins via frozen 400 strahlenther onkol ( 2020 ) 196 : 398404 section , the spherical intrabeam applicator was adjusted in the wound cavity . 
in patients undergoing breast - conserving surgery without iort , biopsies of the tumor bed were taken pre and post sentinel node biopsy ( snb ) to ensure a comparable time interval of approximately 30 min between both biopsies . 
biopsies were taken using conventional scissors . of course , patients of the control collective also underwent irradiation but in contrast to the study collective solely 3 to 4 weeks after surgery via conventional whole breast radiotherapy . histological subtypes and molecular phenotype of were comparable for iort and controls ( not shown )  . asc isolation and characterization twenty - four hours after biopsy , breast asc ( basc ) were isolated using an established method [ 7 ]  . 
the cell suspension was then centrifuged ( 1200 g , 10 min , rt ) and then optionally treated with erythrocyte lysis buffer ( 1 , 10 min , centrifugation 1200 g , 10 min , rt )  . 
cells were plated in a t25 ask ( nunc easy flask ) in dmem low glucose , penicillin / streptomycin ( sigma aldrich ) , l - glutamine ( gibco ) and 10% human ab - serum ( german red cross blood donor service )  . 
remaining cells were seeded as passage 1 ( p1 ) cells at 200 cells / cm2 . asc growth rate was monitored recording cell number at every passage by calculating cell doublings ( cd ) and doubling time ( dt ) : tic adherence , trilineage differentiation capability into adipocytes , chondrocytes and osteoblasts as well as the characteristic surface molecular marker expression , dened by the absence of hematopoietic markers and the presence of cd73 , cd90 , and cd105 ( 14 , 15 )  . 
growth curves were calculated in p1 and p2 . dierentiation assays osteogenic and adipogenic differentiation was performed as described previously [ 7 ] using osteogenic and adipogenic induction / maintenance medium ( lonza )  . 
briey , after 21 days of induction , cells were stained with oil red o and von kossa stain as described . immunophenotyping multicolor immunophenotyping was also performed as described before [ 7 ]  . 
finally , sytox blue was added to exclude dead cells and cells were analyzed using a facs canto ii analyzer running facs diva software ( becton dickinson )  . statistical analysis analysis was performed using graphpad prism 7 . 
the sample weight was where fcn is nal cell number and icn the initial cell number . to dene multipotent mscs , the international society for cell and gene therapy has suggested a characteristic combination of functional properties and the specic surface marker phenotype . 
the hallmarks include plastable 1 isolation success in percent non - iort ( n = 21 ) iort ( n = 20 ) post 12 ( 57% ) 14 ( 66% ) 19 ( 95% ) 1 ( 5% ) no prolonged proliferation number and percentage of samples where basc ( breast adipos stromal cells ) were isolated iort intraoperative radiotherapy strahlenther onkol ( 2020 ) 196 : 398404 fig . 
b exemplary gures of adipogeneic ( ada , oil red o stain ) and osteogenic ( oda , von kossa stain ) differentiation results displaying the negative controls ( top rows ) and the adipogenic / osteogenic - differentiated samples ( bottom rows )  . 
in all , 95% of the pre iort samples and 57% and 66% of the pre and post noniort samples yielded msc cultures , growing beyond passage 2 ( table 1 )  . 
the proliferation potential of non - iort basc , both pre and post , was comparable to asc isolated from subcutaneous fat [ 7 ]  . basc from pre iort samples proliferated signicantly slower ( table 2 )  . 
basc from two exemplary cultures could be cultured up to 67 passages until reaching replicative senescence , without an indication of excessive or prolonged proliferation indicative of malignant transformation or tumorigenic origin ( not shown )  . dierentiation assay differentiation assays and immunophenotyping were performed to verify the msc - like nature of bascs . 
other endothelial markers such as cd144 ( ve - cadherin ) and cd106 ( vcam ) , however , were not expressed . in p2 , cd34 was not expressed , although asc may express cd34 early after isolation [ 13 ]  . 
mean uorescence intensity on positive cells , however , was highly comparable . discussion our results indicate that iort entirely abolishes the adhesion and proliferation potential of basc , suggesting radiosensitivity of basc , at least in situ . 
since iort is performed with 20 gy prescribed to the applicator surface in a single session , supporting data that doses higher than 10 gy radiosensitize msc [ 9 , 14 ]  . 
they showed that the few surviving clones , however , retained differentiation capacity tting to previously published data suggesting a radioresistant subpopulation [ 14 ]  . despite the nearly high isolation success rate , pre iort samples showed decelerated proliferation compared to noniort controls . 
the lower mean breast size in non - iort women ( exclusion criterion for iort ) and the likely different breast composition with a higher proportion of connective tissue , which was often observed in non - iort samples , may explain the differing success rates . 
nevertheless , within the groups there was no difference , so that we consider this effect as negligible . our data on osteogenic and adipogenic differentiation potential suggest that within the 30 min period after resecting the tumor and closing , the wound affects the differentiationbut not the outgrowth and proliferationproperties of basc . 
at the present stage , we cannot exclude that the extended stress caused by surgical tumor resection and iort irradiation and subsequent biopsy affected basc outgrowth rather than the iort itself . 
we regard it important that the entire iort procedure is effective in targeting the tumor niche . strahlenther onkol ( 2020 ) 196 : 398404 growth , morphology , differentiation , and immune phenotypic characterization documented that basc fullled criteria of mscs . 
iort ultimately abolished the outgrowth capacity of basc , indicating basc radiosensitivity in situ . these data support the notion that iort exerts an ablative effect within the tumor bed , not only affecting potential residual tumor cells , but also the tumor bed . 
by this , the iort concept of localized radiation targeting residual tumor cells in the tumor bed to reduce the risk of relapse appears to be validated with respect to tumor bed - derived basc . 
they may further argue towards a reduced risk of breast cancer metastasis [ 17 ]  . it was beyond the scope of this study to assess the effect of radiation of expanded msc [ 9 , 11 , 14 ] and to investigate the potential impact of ionizing radiation on de novo recruitment of circulating msc to the tumor bed as previously suggested [ 18 , 19 ]  . 
the question , if and how iort may affect the recruitment of cells to the tumor bed and its local microenvironment , offers potential for future investigations . conclusion after breast - conserving surgery , approximately 90% of local recurrences emerge in close proximity to the initial tumor bed , potentially reecting a signicant contribution of the tumor bed to relapse . 
our results indicate that iort , besides the proven effect on breast cancer cells , entirely abolishes the adhesion and proliferation potential of basc , suggesting radiosensitivity of basc at doses of 20 gy . 
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to view a copy of this licence , visit strahlentherapie und onkologie original article acute arterial hemorrhage following radiotherapy of oropharyngeal squamous cell carcinoma jens greve1 , 2 , murat bas3 , patrick schuler1 , 2 , bernd turowski4 , kathrin scheckenbach2 , wilfried budach5 , edwin blke5 , christoph bergmann1 , stephan lang1 , diana arweiler - harbeck1 , gtz lehnerdt1 , stefan mattheis1 , henning bier3 , thomas k . 
6 / 10 patients ( all hospitalized ) survived the episode , however , lethal outcome in 4 / 10 patients ( outpatients ) was related to asphyxia as a result of blood aspiration or exsanguination . 
none of the patients revealed evidence of persistent or recurrent tumor disease as proven by biopsy / autopsy and imaging technique . conclusion : vascular erosion following primary or adjuvant r ( c ) t represents a rare and potentially life - threatening complication requiring immediate emergency treatment involving head and neck surgeons , anesthesiologists and neuroradiologists . 
for patients with oropharyngeal neoplasms treated by r ( c ) t and showing recurrent bleeding episodes and mucosal ulceration particularly after the acute treatment phase , hospitalization with prophylactic surgical ligature or embolization of affected arteries is recommended . key words : hemorrhage radiotherapy head - neck cancer ligation embolization strahlenther onkol 2010 ; 186 : 26973 doi 10.1007 / s00066 - 010 - 2114 - 5 fatale arrosionsblutung nach bestrahlung oropharyngealer plattenepithelkarzinome hintergrund und ziel : schdigungen von blutgefen stellen eine seltene , jedoch potentiell lebensbedrohliche komplikation nach strahlentherapie dar . 
die autoren berichten ber akute arterielle blutungen und deren therapie nach strahlentherapie von oropharyngealen tumoren . patienten und methodik : zehn patienten mit einem oropharyngealen plattenepithelkarzinom jeglichen tumorstadiums entwickelten 346 monate ( 14 , 4 5 , 1 monate ) nach primrer ( 5 / 10 ) oder adjuvanter radio ( chemo ) therapie ( r [ c ] t ) eine akute arterielle blutung ( tabelle 1 )  . ergebnisse : alle patienten zeigten in ihrer vorgeschichte kleinere blutungsepisoden und litten unter tiefen schleimhautulzerationen im pharynx auch auerhalb der primrtumorregion ( abbildung 1 )  . 
die therapie umfasste die notfallmige intubation oder tracheotomie und tamponade des rachens , gefolgt entweder von einer ligatur ( abbildung 2 ) und / oder embolisation des 1department of otorhinolaryngology , university of duisburg - essen , essen , germany , 2department of otorhinolaryngology , university of dsseldorf , germany , 3department of otorhinolaryngology , technical university of munich , germany , 4department of radiology , university of dsseldorf , germany , 5department of radiooncology , university of dsseldorf , germany . received : december 12 , 2009 ; accepted : february 16 , 2010 published online : april 26 , 2010 strahlenther onkol 2010 no . 
keiner der patienten zeigte zum zeitpunkt der blutung bildmorphologisch oder histologisch einen residualoder rezidivtumor . schlussfolgerung : gefschdigungen infolge primrer oder adjuvanter r ( c ) t stellen eine potentiell lebensbedrohliche komplikation dar , die einer unmittelbaren notfallmigen interdisziplinren behandlung durch kopf - hals - chirurgen , ansthesisten und neuroradiologen bedarf . 
bei patienten mit oropharyngealen karzinomen , die nach einer r ( c ) t unter wiederkehrenden pharyngealen blutungsepisoden und schleimhautulzerationen leiden , sollte eine stationre berwachung mit einer eventuellen prophylaktischen unterbindung oder einem neuroradiologisch - interventionellen verschluss ( abbildung 3 ) der betroffenen gefe in erwgung gezogen werden . schlsselwrter : arrosionsblutung strahlentherapie kopf - hals - tumoren ligatur embolisation introduction head and neck squamous cell carcinomas ( hnscc ) are among the most frequent malignancies in the upper aerodigestive tract . 
radio ( chemo ) therapy ( r [ c ] t ) , in several combinations [ 16 ] , alone or together with surgery is an established method in treatment protocols of hnscc [ 11 ]  . common side effects of r ( c ) t are erythema , erosion and ulceration of the skin and mucosa , xerostomia , interstitial lymphedema , fibrosis of the soft tissue , and , in severe cases , necrosis of bone or cartilage [ 8 ]  . 
it is discussed , that radiation - induced late effects like chronic inflammation , organ dysfunction , fibrosis and necrosis are driven , in part , by chronic oxidative stress [ 21 ]  . furthermore , vascular alterations are occasionally observed . 
vascular changes contain premature atherosclerosis with stenosis [ 14 ] , adventitial fibrosis , and weakening of the arterial wall caused by obliteration of the vasa vasorum [ 4 , 13 ]  . 
most of the vascular erosions of cervical arteries appear in patients with complications like recurrent tumors , wound infections , or pharyngocutaneous fistulas [ 1 , 6 , 7 , 19 ]  . here , we present a series of ten patients with oropharyngeal carcinomas suffering from acute and life - threatening arterial bleeding after primary or adjuvant r ( c ) t without evidence of above - described comorbidity or residual as well as recurrent tumor burden . patients and methods patients data were collected during a 4.5 - year period and involved individuals affected by oropharyngeal squamous cell carcinoma who developed acute arterial hemorrhage after primary or adjuvant r ( c ) t . 
all suffered from an oropharyngeal squamous cell carcinoma , classified t1 through t4 , most of them with cervical lymph node metastasis ( 8 / 10 patients ) , all without distant metastasis . 
one of them ( patient 2 ) , with an n2c cervical lymph node metastasis , received a salvage neck dissection due to persistent cervical nodes 9 months after irradiation . 
 in one case the bulb of the common carotid artery ( patient 2 ) , in seven patients external branches ( patients 1 , 3 , 4 , 5 , 6 , 9 , and 10 ) , and in two individuals the internal trunk ( patients 7 and 8 ) of the carotid artery was affected . all patients had a history of recurrent episodes of minor pharyngeal bleeding attacks and showed mucosal ulceration of the lateral wall of the pharynx and also outside the primary cancer region ( figure 1 )  . four of ten patients died , all of them before arriving at the trauma room , because of exsanguination or asphyxiation related to blood aspiration , due to the long access route up to the clinic . 
the other six patients were hospitalized and emergency treatment comprised , in close cooperation with anesthetists , stabilization of the circulatory system by intravenous application of vasoactive drugs and blood substitution therapy , intubation ( 2 / 6 ) or tracheotomy ( 4 / 6 ) to prevent blood aspiration . 
arterial hemorrhage following radiotherapy of oropharyngeal tumors discussion acute arterial hemorrhage following primary or adjuvant r ( c ) t is particularly dangerous when located in the upper aerodigestive tract . 
radiation - induced vascular changes varied from atherosclerosis to necrotizing vasculitis characterized by fragmentation of the internal elastic lamellae , focal medial necroses or edema and inflammatory infiltration predominantly by polymorphonuclear leukocytes of adventitia , media and intima [ 8 ]  . 
mitigation or treatment of chronic radiation damage has been shown experimentally in multiple organ systems , with different pharmacological agents , like angiotensin - converting enzyme inhibitors , pentoxifylline and superoxide dismutase mimetics , or gene therapeutic strategies [ 17 ]  . 
unfortunately , the mechanistic basis for most of the experimental successes has not been established , and assessment of the utility of these agents for clinical use has been slow . 
however , since only ligation and not resection of the bleeding artery was performed in some patients ( patients 2 , 4 , 9 , and 10 ) , there is no histopathologic proof of this hypothesis . some patients displayed a mucosal defect outside the primary tumor region but inside the radiation field , which argues against vascular erosion by tumor but for a radiation side effect . 
this was the case in a patient with an oropharyngeal tumor having a late onset of vascular erosion ( common carotid artery ) at the level of the hypopharynx . the first - line treatment of acute arterial hemorrhage consists of emergency stabilization of the respiratory and cardiovascular system and cessation of the bleeding by packing the pharynx followed by immediate arterial embolization [ 5 , 12 ] or surgical ligature [ 20 ]  . 
 however , interruption of blood flow of the internal carotid artery carries significant risk for cerebral ischemia , which was not the case in our series of patients . in general , patients with oropharyngeal cancer who received rt and display recurrent minor bleeding attacks as figure 1 . 
 all successfully treated patients survived without neurologic deficits . 6 months after arterial ligation , patient 9 died of heart failure without a connection to previous therapy or evidence of tumor recurrence . 
evaluation of prognostic factors and two radiation techniques in patients treated with surgery followed by radio ( chemo ) therapy or definitive radio ( chemo ) therapy for figures 3a and 3b . 
arrosion der linken arteria carotis communis vor ( a ) und nach ( b ) einlage eines ummantelten stents . well as mucosal defects should undergo angiography by an experienced neuroradiologist to detect possible damages to the vascular wall early enough to prevent a life - threatening bleeding . 
if such a damage is detected , prophylactic therapy like selective endovascular occlusion or surgical ligature of altered arteries or bridging of the damaged vascular part by angiographic insertion of covered stents ( figure 3 ) has to be considered [ 2 , 3 ]  . conclusion vascular erosion following primary or adjuvant r ( c ) t represents a rare and potentially life - threatening complication requiring immediate emergency treatment involving head and neck surgeons , anesthesiologists , and neuroradiologists . 
an improvement in survival rates may be obtained , if prophylactic embolization , ligation or stenting of affected vessels is performed particularly in those individuals who display recurrent bleeding attacks as well as mucosal defects after r ( c ) t . strahlentherapie und onkologie original article reirradiation with alternating docetaxel - based chemotherapy for recurrent head and neck squamous cell carcinoma update of a single - center prospective phase ii protocol bernhard berger1 , claus belka2 , martin weinmann1 , michael bamberg1 , wilfried budach3 , thomas hehr4 purpose : to report follow - up data and results of a dose escalation within a prospective phase ii protocol scheduling alternating chemoreirradiation for patients with unresectable locoregional recurrence of head and neck cancer after previous curative - intent radiotherapy . patients and methods : chemoreirradiation was initially performed in 27 patients by 40.0 gy split - course reirradiation ( re - rt ) alternating with three cycles of docetaxel 50 mg / m2 day 1 and cisplatin 15 mg / m2 days 25 ( first cohort )  . 
 irrespective of the cohort , severe treatment - related toxicities occurred in about one third of patients . conclusion : the treatment results confirm the efficacy and the safety of escalated re - rt doses in this chemoreirradiation protocol . key words : recurrent head and neck cancer reirradiation radiochemotherapy chemoradiation docetaxel strahlenther onkol 2010 ; 186 : 25561 doi 10.1007 / s00066 - 010 - 2082 - 9 dosiseskalierte alternierende radiochemotherapie fr lokoregional rezidivierende hno - plattenepithelkarzinome nach vorausgegangener strahlentherapie . 
follow - up einer prospektiven phase - ii - studie ziel : berichtet werden das follow - up einer phase - ii - studie zur alternierenden reradiochemotherapie lokoregional rezidivierender , inoperabler hno - plattenepithelkarzinome sowie die auswirkungen der in ihrem rahmen erfolgten dosiseskalation . patienten und methodik : das ursprngliche therapieprotokoll umfasste drei zyklen chemotherapie ( docetaxel 50 mg / m2 tag 1 , cisplatin 15 mg / m2 tage 25 ) in den wochen 1 , 5 und 7 , alternierend mit einer split - course - rebestrahlung bis 40 , 0 gy ( tglich 2 , 0 gy in den wochen 2 + 3 und 5 + 6 )  . 
nach einer zwischenauswertung im jahr 2002 ( erste kohorte , n = 27 ) erhielten weitere 30 patienten ( zweite kohorte ) in woche 6 einen konkomitanten boost bis 49 , 6 gy . 
im juli 2008 wurden die studienendpunkte separat fr beide kohorten sowie fr das gesamtkollektiv ( n = 57 ) analysiert . ergebnisse : im gesamtkollektiv betrugen das 1und 2 - jahres - berleben 52% und 24% ( medianes berleben 13 , 4 monate )  . 
etwa ein drittel der patienten erlitt schwere behandlungsassoziierte toxizitten , und dies war unabhngig von der patientenkohorte . schlussfolgerung : die behandlungsergebnisse besttigen die effektivitt und sicherheit einer dosiseskalation im rahmen dieses therapieprotokolls . schlsselwrter : rezidivierende hno - plattenepithelkarzinome rebestrahlung reradiatio radiochemotherapie docetaxel 1department of radiation oncology , university of tbingen , germany , 2department of radiation oncology , ludwig maximilians university of munich , germany , 3department of radiation oncology , university hospital dsseldorf , germany , 4department of radiation oncology , marienhospital stuttgart , germany . received : september 8 , 2009 ; accepted : march 5 , 2010 published online : april 26 , 2010 strahlenther onkol 2010 no . 
chemoreirradiation for recurrent head and neck cancer introduction locoregional recurrence in a previously irradiated area is the main source of treatment failure in advanced head and neck squamous cell cancer ( hnscc )  . 
 treatment options comprise salvage surgery , reirradiation ( re - rt , either by external rt or brachytherapy ) , chemoreirradiation , or chemotherapy alone ( including molecular targeted therapies ) [ 1 , 610 , 24 ]  . 
aggressive local treatment is mandatory to achieve locoregional control ( lrc ) that is linked to freedom from distant metastasis ( ffdm ) and overall survival ( os ) [ 19 ]  . with respect to chemoreirradiation , phase i / ii trials have been performed showing considerable variability in patient selection , re - rt doses / performance , and chemotherapy concepts [ 8 , 10 ]  . 
compared to the rtog 9610 study , the final analysis of 105 patients revealed a significantly improved outcome ( 2 - year os 24.9% ) [ 11 ]  . in 1997 , we started a single - center prospective phase i / ii protocol on chemoreirradiation that , for the first time , included cisplatin and docetaxel . 
the protocol scheduled split - course re - rt to a moderate dose ( 40.0 gy ) alternating with three cycles of docetaxel and cisplatafter a median follow - up time of 42 months for patients alive , the first analysis showed promising results ( 2 - year os 23% ) and acceptable toxicities [ 6 ]  . 
in addition to follow - up data of the first cohort , we here report on outcome and tolerability of 30 consecutive patients treated according to the modified protocol . patients and methods treatment protocol 1 and cisplatin 15 mg / m2 days 25 in weeks 1 , 4 , and 7 . 
due to grade 3 / 4 hematologic toxicity , the docetaxel dose was reduced from 60 mg / m2 to 50 mg / m2 after the treatment of twelve patients , and this dosage was maintained for all following patients . 
as confirmed by evaluation of the previous rt records , the lifetime spinal cord or brain stem dose was not allowed to exceed 40.0 gy if the time interval between initial rt and re - rt was < 12 months , 55.0 gy if the interval was 1224 months , and 60.0 gy if the interval was > 24 months [ 6 ]  . 
for boosting , the ptv was defined as gtv without safety margins . after our first report mainly had focused on toxicity and feasibility of the protocol [ 6 ] , the objective of this follow - up analysis was to specify its therapeutic efficacy . 
the treatment - related toxicities were scored according to the common terminology criteria for adverse events ( ctcae , version 3.0 ) with late toxicity evaluation commencing after 3 months . 
informed consent and permission for data abstraction were obtained from all patients , and the treatment protocol was approved by the university of tbingen ethics commission . since 1997 , 27 patients with locoregional hnscc recurrence had undergone chemoreirradiation ( first cohort ) [ 6 ]  . 
 the follow - up of the first cohort did not significantly modify the kaplan - meier estimates as reported before [ 6 ]  . treatment results 52 of 57 patients ( 91% ) could be assessed for treatment response . 
a comparison of treatment features identified the re - rt dose as being the only differing factor between the two cohorts ( p < 0.001 ; table 2 )  . univariate analysis of the covariates mentioned above revealed a statistically significant prognostic impact of the following on lrc and os : re - rt dose ( figure 2 ) , chemotherapy dose and overall treatment response ( pr / cr )  . 
at the time of the present analysis , 21 patients of the second cohort ( 75% ) had died ; seven patients were alive , of which five were without treatment and evidence of disease . 
with a median follow - up time of 39 months for patients alive ( range , 11.565.3 months ) , the median os of patients of the second cohort was 17.4 months ( 95% ci , 13.321.5 ) ; the corresponding 1and 2 - year os rates were 67% ( se , 0.086 ) and 31% treatment - related toxicity severe acute and late treatment - related toxicities are listed in table 3 . 
as for acute nonhematologic toxicity , grade 3 dysphagia was the most prevailing effect requiring gastrostomy tubes in four patients ( 24% of those 17 patients who did not have tube - dependent dysphagia before )  . 
compared to our first report [ 6 ] , tumor control and survival estimates have been further improved ; accordingly , an intercohort comparison showed significantly better os estimates for patients of the second cohort . 
the impact of the re - rt dose is corroborated by contemporary reviews indicating a re - rt doseresponse relationship in chemoreirradiation for recurrent hnscc [ 12 , 18 , 22 ]  . concomitant chemoradiation generally yields better results than a sequential course in primary treatment of hnscc [ 5 , 19 ]  . 
kaplan - meier - kurve fr die wahrscheinlichkeit einer grad - 3 / 4 - spttoxizitt ( fr konsekutive spttoxizitten wurde eine erstmanifestation nach 3 monaten angenommen )  . has been routinely performed concomitantly [ 3 , 4 , 11 , 15 , 17 , 18 , 20 ]  . 
apart from the rtog studies mentioned above [ 11 , 20 ] , the largest patient collective treated concomitantly has been reviewed by a recent meta - analysis [ 18 ]  . 
in our series , minor deviations from chemotherapy led to a low overall compliance to protocol ( 46% ) ; although comparable to that reported by the rtog 9911 study [ 11 ] , this rate remains unsatisfactory and highlights the need for improvement of surveillance and support strategies . trismus grade 3 late tumor bleeding requiring surgery late pharyngocutaneous fistula 1 ( 4 ) aindicating patients who needed to supplement more than one half of their diet with gastrostomy tube feedings before re - rt increased use of 5 - fu in primary treatment , its standard administration was abandoned in favor of cisplatin and a taxane . 
concerning late toxicity , the overlapping of changes originating from previous therapeutic procedures with those induced secondarily hampers a reliable toxicity assessment [ 3 , 12 , 22 ]  . 
chemoreirradiation for recurrent head and neck cancer than reported in comparable series ( 1030% ) [ 11 , 18 , 20 ] ; by contrast , however , the majority of those changes was scored to be grade 3 , and there were only few life - threatening late complications . 
on the basis of current toxicity data [ 3 , 11 , 12 , 18 , 20 , 22 ] , one might argue that the risks of re - rt outweigh the survival benefit compared to chemotherapy alone [ 5 , 24 ]  . 
future efforts should be aimed at the improvement of tolerability using imrt [ 3 , 12 , 22 ] , innovative re - rt delivery techniques such as helical tomotherapy [ 16 , 21 , 26 ] , and optimized support strategies . conclusion the escalation of re - rt doses has been shown to be effective characterizing this alternating chemoreirradiation concept as valuable alternative to split - course concomitant chemoreirradiation protocols . strahlentherapie und onkologie review article advanced - stage iii / iv follicular lymphoma treatment strategies for individual patients frank heinzelmann1 , hellmut ottinger2 , marianne engelhard3 , martin soekler4 , michael bamberg1 , martin weinmann1 background : in patients with advanced - stage iii / iv follicular lymphoma ( fl ) , there are many treatment options available . 
 the use of autologous hematopoietic stem cell transplantation ( hsct ) for patients in first remission or chemosensitive relapse prolongs progression - free survival while the effect on overall survival remains unclear compared to standard chemotherapy . 
 in the palliative setting , low - dose involved - field irradiation constitutes an effective treatment option in order to control local symptoms with potential long - lasting response . conclusion : in case of advanced - disease fl , asymptomatic patients can be managed expectantly . 
for younger patients with chemoresistant / relapsed disease , allogeneic hsct might be considered , since advances in supportive care and better patient selection have resulted in improved outcomes . key words : advanced - stage follicular lymphoma chemo - , radioimmunotherapy radiotherapy autologous transplantation allogeneic transplantation strahlenther onkol 2010 ; 186 : 24754 doi 10.1007 / s00066 - 010 - 2091 - 8 follikulre lymphome in fortgeschrittenen stadien iii / iv . 
die herausforderung besteht darin , eine optimale behandlungsstrategie fr den einzelnen patienten auszuwhlen . methodik : es wurde eine literaturrecherche unter verwendung der pubmed - datenbank zu therapiestrategien bei patienten mit fortgeschrittenen stadien eines fl durchgefhrt . ergebnisse : fr fortgeschrittene stadien iii / iv eines fl betrgt das mediane berleben 810 jahre . 
die anwendung der autologen transplantation in erster remission oder bei chemosensitivem rezidiv kann im vergleich zur konventionellen chemotherapie das progressionsfreie berleben verlngern , der einfluss auf das gesamtberleben ist noch ungeklrt . 
im rahmen der palliation stellt eine niedrigdosierte involved - field - strahlentherapie eine effektive lokale behandlungsoption mit potentiell lang anhaltender remission dar . 1department of radiation oncology , university of tbingen , germany , 2department of bone marrow transplantation , university of essen , germany , 3department of radiation oncology , university of essen , germany , 4department of internal medicine ii , university of tbingen , germany . received : august 15 , 2009 ; accepted : january 29 , 2010 published online : april 26 , 2010 strahlenther onkol 2010 no 5 urban & vogel heinzelmann f , et al . 
bei jngeren patienten mit chemoresistenter erkrankung oder rezidiv eines fl kann eine allogene transplantation erwogen werden , da ein optimales management die mortalittsrate der allogenen stammzelltransplantation gesenkt hat . schlsselwrter : fortgeschrittenes follikulres lymphom chemo - , radioimmuntherapie radiotherapie autologe transplantation allogene transplantation introduction follicular lymphoma ( fl ) is the second most common subtype of non - hodgkins lymphoma worldwide in adults ( ~ 2025% ) arising from follicle center b lymphocytes . 
since three randomized trials demonstrated that the prognosis is not affected by immediate treatment versus an initial policy of observation until symptomatic disease progression ( e.g. , bulky lymphadenopathy , compressive disease , marrow compromise , splenomegaly ) , delayed treatment is a feasible approach [ 2 , 8 , 92 ]  . 
in spite of the exploration of different conventional chemotherapy strategies resulting in 7590% response rate [ 13 , 46 , 56 ] , the prognosis of fl improved only marginally over decades , with a median survival of 810 years [ 34 ]  . 
however , more recently , a significant prolongation of survival was reported due to the introduction of novel therapeutic strategies like chemoimmunotherapy / radioimmunotherapy [ 17 , 47 ]  . 
this review will discuss different treatment approaches addressing the issues of current first - line and salvage strategies in patients with advanced - stage iii / iv fl . first - line treatment strategies in advanced stages iii / iv internationally , there is not yet a consensus regarding optimal first - line therapy in patients with advanced - stage fl , but different promising treatment strategies have evolved . 
binding of rituximab to the cd20 surface antigen which is expressed by > 90% of fls leads to complementmediated lysis , antibody - dependent cell - mediated cytotoxicity and induces apoptosis . 
 chemoimmunotherapy enhanced response rates and significantly improved progression - free survival ( pfs ) and overall survival ( os ) when compared to chemotherapy alone [ 32 , 33 , 51 , 69 ] ( table 1 )  . 
 chop : cyclophosphamid , doxorubicin , vincristin , prednison ; chvp - i : cyclophosphamid , adriamycin , etoposid , prednisolon , interferon ; cr : komplette remission ; cvp : cyclophosphamid , vincristin , prednison ; efs : ereignisfreies berleben ; mcp : mitoxantron , chlorambucil , prednison ; nr : nicht erreicht ; orr : gesamtansprechrate ; os : gesamtberleben ; r - chop : rituximab , cyclophosphamid , doxorubicin , vincristin , prednison ; r - chvp - i : rituximab , adriamycin , etoposid , prednisolon , interferon ; r - cvp : rituximab , cyclophosphamid , vincristin , prednison ; r - mcp : rituximab , mitoxantron , chlorambucil , prednison ; ttf : zeit bis therapieversagen . 
 chop : cyclophosphamid , doxorubicin , vincristin , prednison ; cr : komplette remission ; ns : keine angabe ; orr : gesamtansprechrate ; pfs : progressionsfreies berleben ; r - chop : rituximab , cyclophosphamid , doxorubicin , vincristin , prednison . first author , year patients ( n ) therapy follow - up ( months ) orr ( % ) cr ( % ) pfs ( % ) demonaco , 2005 [ 15 ] kaminsky , 2005 [ 38 ] leonard , 2005 [ 45 ] shipley , 2005 [ 75 ] press , 2006 [ 61 ] r - chop , 90y - ibritumomab tiuxetan tositumomab , 131i - tositumomab fludarabine , tositumomab , 131i - tositumomab r , r - chop , 90y - ibritumomab tiuxetan chop , tositumomab , 131i - tositumomab 95 91 87 , 5 of rituximab maintenance therapy following first - line induction with chemoimmunotherapy is currently being evaluated in international phase iii randomized trials ( prima study , osho / glsg trial )  . 
in the era before rituximab , maintenance therapy with interferonwas shown to prolong remission duration and os [ 65 ] , but poor tolerance has prevented its widespread use . another new treatment approach in patients with advanced fl was the introduction of radioimmunotherapy ( complexing radioisotope to a monoclonal anti - cd20 antibody )  . 
the efficacy and safety have been evaluated as single - agent therapy and as part of multimodality treatment regimens resulting in high response / os / pfs rates ( table 2 )  . 
a recent phase iii trial ( fit trial ) compared the efficacy of consolidation therapy 90y - ibritumomab tiuxetan with no further therapy in patients who achieved at least a partial remission ( pr ) after different induction chemotherapy regimens ( ~ 15% rituximab - based )  . 
interestingly , in the subgroup of patients who received rituximab - based induction chemotherapy , pfs was not different between treatment arms [ 54 ]  . to exploit the comparably high intrinsic chemosensitivity of lymphoma cells early in the course of the disease , the efficacy and safety of high - dose therapy followed by autologous hematopoietic stem cell transplantation ( autologous hsct ) have been investigated in three randomized phase iii trials . 
the german low - grade lymphoma study group ( glsg ) reported on 240 patients achieving at least a pr by induction chemotherapy who were either randomized to autologous hsct consolidation or interferonmaintenance . 
 after a median follow - up of 4.2 years , 5 - year projected pfs was found to be significantly superior after autologous hsct ( 64.7% ) when compared to interferon maintenance ( 33.3% ) while results on os have not yet been available [ 43 ]  . 
more recently , the groupe detude des lymphomas de ladulte ( gela ) trial compared standard chemotherapy ( 6 chvp [ cyclophosphamide , doxorubicin , teniposide , prednisone ] plus interferon ) with an experimental arm consisting of four cycles of chop ( cyclophosphamide , doxorubicin , vincristine , prednisone ) followed by autologous hsct . 
in conclusion , long - term results demonstrated an effect on pfs but no clear survival benefit in favor of autologous hsct as consolidation therapy in first remission when compared to conventional treatment approaches . 
therefore , the prognostic relevance of autologous hsct is under investigation in a phase iii trial of the glsg ( ri - chop trial ) : after induction treatment with six cycles of r - chop patients will be randomized either to autologous hsct and rituximab maintenance or to rituximab maintenance alone . 
 rituximab application helped to prevent relapses by elimination of minimal residual disease and this effect may translate into improved event - free survival ( efs ) / os [ 10 ]  . taken together , in symptomatic patients , use of chemoimmunotherapy is the preferred first - line treatment based on several randomized trials with no consensus on the best chemotherapy arm [ 32 , 33 , 50 , 51 , 69 ]  . 
in order to evaluate the best first - line treatment in patients with advanced fl , the us intergroup trial compares r - chop with chop followed by 131i - tositumomab in an ongoing randomized phase iii trial . treatment strategies in relapsed / refractory disease in patients with relapsed or recurrent fl , conventional chemotherapy is not able to induce a stable second remission with a continuous pattern of relapses characterized by decreasing progression - free intervals resulting in a median survival of 45 years from first relapse [ 37 ]  . 
therefore , different approaches have been evaluated : chemoimmunotherapy , radioimmunotherapy , autologous and allogeneic hsct . the concept of chemoimmunotherapy has been evaluated both in rituximab - naive and rituximab - pretreated patients . 
a clear benefit in terms of remission induction , pfs / os and an additional advantage of maintenance rituximab treatment could be observed when compared to chemotherapy alone [ 19 , 83 ]  . the implementation of radioimmunotherapy in relapsed / recurrent fl produces convincing overall response rates ( orrs ) ranging from 73% to 83% with tolerable toxicity [ 26 , 8688 , 90 ]  . 
in one of these trials , a randomized study comparing 90y - ibritumomab tiuxetan regimen with rituximab monotherapy , orr / cr were significantly higher with the radioimmunoconjugate [ 88 ]  . 
a recent analysis showed that a single dose of 90y - ibritumomab tiuxetan even prolonged survival in a substantial number of patients in whom previous therapies had failed [ 89 ]  . several phase ii studies have shown that salvage autologous hsct achieves prolonged disease - free survival ( dfs ) / os compared to conventional chemotherapy in patients with recurrent fl [ 1 , 4 , 6 , 9 , 20 , 66 ]  . 
however , slow patient accrual , small patient number ( n = 89 ) being randomized to a three - arm study design and short follow - up limit the definite interpretation of these data [ 72 ]  . 
 in addition , this trial was performed before the introduction of chemoimmunotherapy regimens which are now considered to be the treatment of choice in the salvage situation [ 19 ]  . 
interestingly , in a recent trial by sebban et al . , a salvage regimen containing rituximab with subsequent autologous hsct led to a dramatic improvement of 5 - year pfs / os [ 73 ]  . since cure of advanced fl by chemo - , radioimmunotherapy and autologous hsct has not yet been established , there is an increasing interest in exploring the role of allogeneic hsct . 
as compared to autologous hsct , the allogeneic stem cell source provides a pluripotent progenitor pool free of contaminated tumor cells and includes t cells capable of promoting the graft - versus - lymphoma ( gvl ) effect as part of an alloreactive mechanism [ 44 , 84 ]  . 
in this context , total - body irradiation ( tbi ) plays a key role in the conditioning regimen prior to allogeneic hsct [ 23 , 31 , 60 , 63 , 71 ] in order to eradicate malignant clonogenic cells and to achieve a sufficient immunosuppression [ 12 ]  . 
 ns : keine angabe ; os : gesamtberleben ; pfs : progressionsfreies berleben ; tbi : ganzkrperbestrahlung ; trm : therapiebedingte mortalitt . patients tbi - based conditioning follow - up ( months ) trm relapse rate ( % ) pfs first author , year van besien , 1995 [ 82 ] mandigers , 1998 [ 49 ] van besien , 1998 [ 80 ] verdonck , 1999 [ 84 ] forrest , 2002 [ 18 ] yakoub - agha , 2002 [ 91 ] hosing , 2003 [ 35 ] kiss , 2003 [ 41 ] peniket , 2003 [ 58 ] van besien , 2003 [ 79 ] toze , 2004 [ 77 ] van besien , 2005 [ 78 ] 10 15 113 15 24 16 44 25 29 80 82 8 81 55 0 68 93 70 up to now , the value of conventional myeloablative allogeneic hsct in patients with relapsed / refractory fl has intensively been evaluated as summarized in table 3 [ 18 , 35 , 41 , 49 , 58 , 7780 , 82 , 84 , 91 ]  . these data show that this treatment modality has the potential for cure in relapsed / refractory fl due to low recurrence rates after transplant ( 020% ) , although long - term follow - up data for allogeneic hsct are still pending . 
however , the high trm ( 20 40% ) , severe graft - versus - host disease ( gvhd ) and infections limit its use to patients < 50 years . 
noteworthy , the incidences of acute / chronic gvhd are not reduced after ric and the risk of relapse is increased after ric compared to myeloablative hsct [ 78 ]  . 
currently , the role of rt is poorly defined , since novel strategies like chemoand radioimmunotherapy lead to substantially improved pfs / os rates with tolerable toxicity in the first - line treatment of advanced fl . in the palliative setting , low - dose involved - field rt ( 4 gy given in two fractions ) has been reported to provide a long - lasting response with minimal side effects [ 21 , 25 , 29 , 36 , 55 , 70 ]  . 
in case of failure of low - dose rt , full - dose involved - field rt ( 3040 gy ) plays a key role in providing symptom relief and local control [ 7 , 22 ]  . 
currently , nontoxic involved - field rt ( 2 2 gy ) is compared with standard chemotherapy chlorambucil in the phase iii randomized hovon 47 / eortc 20013 trial in previously untreated patients [ 28 ]  . conclusion in advanced fl , asymptomatic patients can be managed expectantly . 
in elderly patients with symptomatic disease and / or relevant comorbidities , single - agent rituximab monochemotherapy or low - dose involved - field rt might be appropriate . strahlenther onkol 2010 no 5 heinzelmann f , et al . 
however , although advances in supportive care and better patient selection have resulted in improved long - term os / dfs due to reduced trm and acute gvhd , conventional allogeneic hsct is restricted to younger patients with good kps . 
the role of rt as additional local treatment in case of high - risk situations like bulky disease and / or incomplete morphological remission is poorly defined with regard to the differing systemic treatment strategies . 
possibly , local consolidation may be beneficial in selected patients [ 3 ]  . strahlentherapie und onkologie original article clinical implementation of volumetric intensitymodulated arc therapy ( vmat ) with ergo + + dirk wolff , florian stieler , brigitte hermann , katharina heim , sven clausen , jens fleckenstein , martin polednik , volker steil , frederik wenz , frank lohr1 background and purpose : volumetric modulated arc therapy ( vmat ) has the potential to deliver dose distributions comparable to the established intensity - modulated radiotherapy techniques for a multitude of target paradigms . 
prior to implementing vmat into their clinical routine in december 2008 , the authors evaluated the dose calculation / delivery accuracy of 24 sample vmat plans ( prostate and anal cancer target paradigms ) with film and ionization dosimetry . 
after the start of the clinical program , in vivo measurements with a rectal probe were performed . material and methods : the vmat plans were generated by the treatment - planning system ( tps ) ergo + + ( elekta , crawley , uk ) and transferred to a phantofilm dosimetry was performed with kodak edr2 films , and evaluated with dose profiles and ( cid : 74 ) - index analysis . 
the ionization chamber was used with localization of the measurement volume based on positioning cone - beam computed tomography . results : plans were transferred from ergo + + to the record and verify ( r&v ) system / linear accelerator ( linac )  . 
the first in vivo measurements confirm the reproducible precision of the delivered dose during clinical treatments . key words : volumetric intensity - modulated arc therapy ( vmat ) ergo + + prostate cancer anal cancer in vivo dosimetry strahlenther onkol 2010 ; 186 : 2808 doi 10.1007 / s00066 - 010 - 2071 - z klinische einfhrung von volumetrisch intensittsmodulierter arc - therapy ( vmat ) mit ergo + + hintergrund und ziel : die volumetrisch modulierte arc - therapie ( vmat ) bietet die mglichkeit , fr einige planparadigmata zur bisher etablierten intensittsmodulierten strahlentherapie vergleichbare dosisverteilungen zu generieren . 
vor der im dezember 2008 erfolgten einfhrung von vmat in die eigene klinische routine berprften die autoren dosisberechnung und be strahlungsgenauigkeit anhand von 24 vmat - plnen ( analund prostatakarzinomplanungsparadigmata ) mittels filmund ionisationsdosimetrie . 
erste patientenbestrahlungen wurden mittels rektaler in - vivo - dosimetrie verifiziert . material und methodik : die vmat - plne wurden mit dem planungssystem ergo + + ( elekta , crawley , uk ) generiert und in einem phantom verifiziert . 
ein cone - beam - computertomogramm wurde fr die lokalisation des messvolumens der ionisationskammer im rektum verwendet . ergebnisse : die plne wurden durchgngig fehlerfrei von ergo + + an das record and verify - ( r&v - ) system und an den beschleuniger bertragen . 
die in - vivo - messungen ergaben nach erfolgreicher positionierung im hochdosisbereich eine mittlere abweichung zwischen berechneter und applizierter dosis von 2 , 09% 2 , 4% . schlussfolgerung : vmat - plne knnen auf basis der klinisch zugelassenen kette aus planungs - , r&vund bestrahlungssystem nach adquater kommissionierung reproduzierbar erzeugt und zuverlssig bestrahlt werden . 
die ergebnisse der individualplanverifikation 1department of radiation oncology of the university medical center mannheim , university of heidelberg . received : july 8 , 2009 ; accepted : march 5 , 2010 published online : april 26 , 2010 strahlenther onkol 2010 no . 
erste in vivo ermittelte dosen besttigen die przision der dosisapplikation im klinischen einsatz . schlsselwrter : volumetrisch intensittsmodulierte arc - therapy ( vmat ) ergo + + prostatakarzinom analkarzinom in - vivo - messungen introduction dose - escalated radiotherapy is the treatment standard for locally advanced prostate cancer and is also a viable treatment option for early - stage tumors [ 20 , 25 , 26 ] , with intensity - modulated radiotherapy ( imrt ) being an important means to provide safe dose delivery [ 7 , 8 , 16 , 19 , 31 , 47 , 48 ]  . 
while the efficiency of conventional step - and - shoot , dynamic imrt approaches and tomotherapy has dramatically improved during the last years , a rotational treatment paradigm seeking to reduce treatment time by allowing more degrees of freedom such as variations in gantry speed , dose rate , collimator angle in addition to dynamically changing field shapes may be another means to reach this goal [ 3 , 23 , 45 ]  . 
 while a considerable number of patients have already been treated with modulated rotational approaches [ 1 , 11 , 12 , 46 ] , these treatments have been planned with investigational treatment - planning systems ( tps ) [ 11 , 12 , 45 ]  . 
with commercial planning and delivery software now being clinically available from different vendors , it is essential to evaluate the new commercial tps in terms of plan quality , treatment efficiency and accuracy and compare them to existing techniques and systems , because vmat with its simultaneous variation of gantry position , gantry speed , leaves and jaw positions mandates tight and efficient surveillance and management of linear accelerator ( linac ) parameters . a second recent development , online image - guided radiotherapy ( igrt ) , has facilitated reliable intracorporeal in vivo dosimetry by providing precise localization data of measurement devices [ 22 , 39 ]  . the goal of the present study was to investigate the dosimetric accuracy of this new complex technique based on a clinically approved and commissioned tps and delivery system with end - to - end tests , thus assessing the complete workflow from the tps via the dicom export process to the record and verify ( r&v ) system and finally to the linac . 
assessment of daily reproducibility was based on image - guided in vivo dosimetry . material and methods delineation computed tomography ( ct ) datasets of nine patients with prostate cancer and eight patients with anal cancer who received multileaf collimator - ( mlc - ) based imrt in our department and that had previously been selected for a comparative planning study of vmat versus established imrt versus conventional techniques [ 33 , 34 , 42 , 43 ] formed the basis of the preclinical dosimetric evaluation of the new technique . 
treatment plans were generated for an elekta synergy ( elekta group , crawley , uk ) with a standard mlc of two leaf banks with 40 leaves with 1 cm leaf width at the isocenter and an energy of 6 mv . 
the planning procedure starts with the definition of the intial setup of the static control points and anatomy - based aperture definition of the fluence maps and then proceeds with the zero solution of dose calculation ( all fluence maps have the same weight ) based on pencil - beam algorithafterwards , dose constraints of target volume and oars are edited in the amoa tool . 
beispielhafte dosisverteilung fr einen anal ( oben ) und prostatafall ( unten )  . dose constraints to be chosen in the planning process were : dmax and dmin for target volumes , dmax for oar , penalties , and required percentage volume . two different vmat strategies for the prostate and anal paradigm were calculated and delivered , either with one single rotation or multiple rotations . 
both strategies yielded the intended plan quality for the prostate paradigm [ 42 , 43 ] , but only two rotations reproducibly produced plans with the desired characteristics for the anal cancer paradigm [ 33 , 34 ]  . 
 im mittleren bereich der berlagerung die typische form einer prostata ; dieser bereich ist der hochdosisbereich . the setup ( number of arcs , monitor units [ mu ] ) of the final patient treatment plans was copied to the ct datasets of the phantoms . 
to accommodate the large field sizes used for the anal cancer paradigm , we used an ellipsoid pelvic phantom ( model 002h5 , cirs inc . , norfolk , va , usa )  . 
both phantoms are manufactured of water - equivalent material and are composed of 1 cm thick plates in the central region which enables placement of single films between the plates . 
ionization chamber measurements can be acquired using a hole along the axis of the cylinder ( for the ptw phantom ) or water - equivalent interchangeable rod inserts ( for the cirs phantom ) , where semiflex ionization chamber can be inserted . 
absolute ionization chamber - based dosimetry was performed with a semiflex ionization chamber ( 0.125 cm3 ) by ptw freiburg and film dosimetry was performed with radiographic films adapted for an extended dose range ( edr2 , eastman kodak corp . , rochester , mn , usa ) [ 44 , 49 ]  . 
a calibration between optical density of the used edr2 films and dose which is also used for clinical imrt routine was performed with film cal version 2.2 strahlenther onkol 2010 no . 
figure 2 shows a sample matching of calculated and treated dose distributions in verisoft with the bright area indicating the region where film and phantom are superimposed on each other . 
for the smaller head and neck phantom it was necessary to cut the film in two halves so that it fits into the phantoat the cutting edges light exposure was possible which led to dark areas at the border of the films . 
 ( cid : 74 ) - analyse ( inklusive hochund niedrigdosisbereich ) fr einen referenzplan ( oben ) , einen beispielhaften prostataplan ( mitte ) und einen beispielhaften analplan ( unten ; akzeptanzkriterien 1% / 1 mm 2% / 2 mm 3% / 3 mm 4% / 4 mm 5% / 5 mm 5% / 10 mm )  . 
the coordinates of the effective point of measurement relative to the isocenter were determined with the measurement tool of the xvi software in coronal , axial and sagittal planes of the ct data . 
measured doses were compared to the corresponding dose values of the calculated dose in the treatment plans . results phantom measurements doses measured with the ionization chamber showed good agreement between calculated and treated values for all verification plans . 
der rote pfeil markiert den messpunkt im anterioren rektum . and calculated the percentage of pixels passing the respective criteria . in vivo measurements dosimetric accuracy was further assessed by 14 in vivo measurements for the first three patients . 
figure 3 shows a sample comparison between calculated dose matrix and treated film in verisothe analysis of the - index for the prostate and the anal cases showed no deviations > 3% for the high - dose region , as also displayed in figure 4 . 
table 2 shows the mean , maximum and minimum values and the standard deviation for different - indices of the highand low - dose region , and further includes the values for the reference measurement . 
two film measurements of the prostate cases were excluded because two films offered large dark areas due to light exposure , which gave wrong - values . in vivo measurements for three patients , 14 in vivo measurements in the rectum were performed as shown in figure 5 . 
 this kind of errors gives no robust estimate regarding the precision of the tps or calculation algorithm , because even minimal dislocations of the probe during the measurement and even the relatively larger chamber volume may result in an overall insecurity of around 0.1 gy at any given position in the low - dose region . 
 the results of the in vivo measurements are displayed in detail in figures 6 a and 6b . discussion in preparation of the clinical implementation of vmat , we analyzed and compared the accuracy of vmat dose delivery for prostate and anal cancer paradigms to the calculated treatment planes . 
we found good agreements for the absolute dose values measured with an ion chamber and also for the relative dose profiles recorded with edr2 films as quantified by - analysis . 
well known are field size and depth dependency for radiologic films [ 18 , 24 ] and scanning inhomogeneities for the gafchromic ebt film ( international specialty products , chatham , nj , usa ) [ 30 ]  . 
clinical implementation of vmat with ergo + + measurement in low - dose region measurement in low - dose region number of measurements intrafractional probe motion ( mm ) figures 6a and 6b . 
reported for experimental clinical implementations of vmat [ 5 , 11 , 12 , 38 , 46 ] and are also in the range of what is recommended for imrt techniques that have already become routine such as step - and - shoot as well as dynamic imrt [ 14 ]  . this initial analysis of the relative dose distribution was performed using radiographic films , following verbakel et al . 
two - dimensional arrays will , however , be used for routine qa in the future . a comprehensive numerical and objective comparison of the relative dose distribution is only possible with the - index analysis . 
although the most frequently used - index is the 3% / 3 mm , reports or recommendations for the interpretation of a - value matrix were scarce until recently [ 35 ]  . 
they inserted diodes ( scanditronix rectal probe containing five n - type photon - detecting diodes ) in the anorectum during pelvic radiotherapy and found dose deviations of up to 7% in the target region , which was probably secondary to some uncertainty regarding probe placement when referenced to bony landmarks . 
using cbct as described previously [ 39 ] , we could determine the position of the ionization chamber reliably within a range of 2 mm . the absolute dose deviations measured in vivo were similar to the results from the preclinical qa measurements and also to those for static imrt by wertz et al . 
secondary to intrafractional probe motion were not seen in our series because of the plateau region of the dose being prescribed to extend a few millimeters more into the anterior rectum for the vmat plans [ 42 ]  . conclusion the preclinical , phantom - based dosimetric evaluation of vmat delivery for prostate and anal cancer paradigms showed good agreement with calculation . 
these data were reproducibly confirmed upon in vivo dosimetry during the first clinical treatments . acknowledgments we gratefully acknowledge the help of roberto pellegrini , manuela duglio , yvette bellingham , nick linton , alison metcalfe and kevin brown of elekta group for the close collaboration during the implementation and initial evaluation of ergo + + and vmat . strahlentherapie und onkologie original article stereotactic body radiotherapy for lung tumors at the pulmonary hilum yoshiko oshiro1 , 2 , takashi aruga2 , koji tsuboi1 , 3 , kan marino4 , ryusuke hara5 , yasushi sanayama6 , jun itami7 background and purpose : high - dose irradiation to the pulmonary hilar region is generally considered to be of high risk in causing bronchial injury . 
the aim of this retrospective study is to investigate the safety and efficacy of stereotactic body radiotherapy ( sbrt ) for patients with lung tumors in the pulmonary hilum . patients and methods : 21 patients who underwent sbrt for lung tumors within 2 cm from a major bronchus were retrospectively analyzed . 
severe late toxicity ( grade 3 ) was seen in three patients of whom two had previously received repeated radiotherapy . conclusion : sbrt for lung tumors located in the pulmonary hilar region may be tolerable and acceptable , if multiple treatments to the same major bronchus are avoided , and irradiated volumes are carefully taken into consideration . key words : radiotherapy stereotactic body radiotherapy lung pulmonary hilum bronchial stenosis strahlenther onkol 2010 ; 186 : 2749 doi 10.1007 / s00066 - 010 - 2072 - y stereotaktische strahlentherapie bei lungentumoren im hilum pulmonis hintergrund und ziel : die hochdosierte bestrahlung der lungenhilusregion gilt im allgemeinen als groes risiko in bezug auf die verursachung von bronchialverletzungen . 
ziel dieser retrospektiven studie ist die untersuchung der sicherheit und wirksamkeit der stereotaktischen strahlentherapie bei patienten mit lungentumoren im hilum pulmonis . patienten und methodik : 21 patienten , die sich einer stereotaktischen bestrahlung von lungentumoren im abstand von bis zu 2 cm zu einem hauptbronchus unterzogen , wurden retrospektiv analysiert . 
die tumoren wurden mit biologisch wirksamen gesamtdosen im bereich von 50 , 7 bis 157 , 5 gy ( median : 100 gy ) bestrahlt . ergebnisse : die gesamtberlebensraten 1 und 2 jahre nach der stereotaktischen strahlentherapie lagen bei 90 , 0% bzw . 
schwere spttoxizitt ( grad 3 ) wurde bei drei patienten beobachtet , von denen sich zwei in der vergangenheit mehreren strahlentherapien unterzogen hatten . schlussfolgerung : eine stereotaktische strahlentherapie bei lungentumoren in der gegend des lungenhilus ist mglicherweise vertrglich und vertretbar , wenn mehrere behandlungen des gleichen hauptbronchus vermieden und bestrahlte volumen sorgfltig bercksichtigt werden . schlsselwrter : strahlentherapie stereotaktische bestrahlung lunge lungenhilus bronchostenose 1department of radiation oncology , university of tsukuba , ibaraki , japan , 2department of radiation oncology , international medical center of japan , shinjuku - ku , tokyo , japan , 3department of neurosurgery , university of tsukuba , ibaraki , japan , 4department of radiation oncology , university of yamanashi , chuo - ku , japan , 5department of radiation oncology , chiba medical center , chuo - ku , japan , 6department of radiation oncology , chiba university , chuo - ku , japan 7department of radiation oncology , national cancer center , chuo - ku , tokyo , japan . received : august 7 , 2009 ; accepted : march 5 , 2010 published online : april 26 , 2010 strahlenther onkol 2010 no . 
sbrt to the pulmonary hilum introduction stereotactic body radiotherapy ( sbrt ) has been increasingly applied as an emerging modality for the treatment of early - stage non - small cell lung cancer ( nsclc ) and metastatic lung tumors because of its efficacy in delivering high - dose radiation to the minimum area [ 3 , 11 , 14 , 15 , 17 , 19 , 21 , 26 , 29 , 31 , 33 , 34 ]  . 
one of the reasons for this is that the risk of bronchial injury followed by secondary atelectasis has been reported to be higher when the pulmonary hilar region was irradiated with a high dose [ 26 ]  . in our facility at the international medical center of japan , sbrt for lung tumors including tumors at the pulmonary hilum was started in 1998 . 
we herein describe our retrospective review of patients with pulmonary tumor located within 2 cm from the main bronchus to clarify the tolerance and feasibility of sbrt for patients with tumors in this region . patients and methods patient and tumor characteristics from august 1998 to january 2009 , 181 patients with 229 malignant lung tumors were treated by sbrt at the international medical center of japan . 
some patients who refused surgery and patients in whom surgery was not indicated were considered for sbrt , to achieve local control if prophylactic or lymph node irradiation was not required . 
 by reviewing these 229 tumors , we could find that 22 tumors in 21 patients were located in the region within 2 cm from the major bronchus on computed tomography ( ct ) images , and they were retrospectively analyzed in this study . the patient and tumor characteristics are shown in table 1 . 
the clinical stages of the 14 patients with nsclc were as follows : stage ia : n = 1 , stage recurrent ( r ) ia : n = 3 , stage rib : n = 1 , stage riia : n = 1 , and stage iv : n = 8 , according to the tnm classification of the international union against cancer [ 22 ]  . 
briefly , simulation during the end - expiratory phase was performed with the patient lying on the cradle made for each patient after ct had been taken ; then , multiportal , noncoplanar irradiation planning was conducted . 
the information concerning the respiratory movement detected by a laser displacement monitor ( keyence , tokyo , japan ) placed on the patients chest was sent to the respiratory gating system , and the treatment beams were delivered only during the end - expiratory phase . 
since july 2004 , sbrt has been performed with the clinac 21ex accelerator and a real - time position management system ( rpm ; varian , palo alto , ca , usa ) with patients immobilized by individually shaped body casts ( vac - loc ; med - tec , orange city , ia , usa )  . 
ct images of 2 mm thickness were taken in the treatment position during the expiratory phase and the data were sent to a treatment planning system ( eclipse tm ; varian )  . 
the clinical target volume ( ctv ) was contoured as the gross tumor volume ( gtv ) , and an additional 5to 7 - mm margin was added to cover the ctv as a ptv . 
bed : biologisch wirksame dosis ; conv : konventionelle strahlentherapie ; ibrt : intrabronchiale strahlentherapie ( brachytherapie ) ; sbrt : stereotaktische strahlentherapie . plan - meier method [ 13 ]  . 
one patient with apocrine cancer received sbrt to the bilateral pulmonary hilar region ( table 2 )  . radiation dose total doses ranging from 25 to 60 gy in one to 13 fractions were given ( median , 50 gy in five fractions ) to the patients . 
 as various fractionation regimens were used , the biologically effective dose ( bed ) was calculated for comparison using the linear - quadratic model with ( cid : 68 ) ( cid : 18 ) ( cid : 69 ) ratios assumed to be 10 ( bed10 ) for tumors and 3 ( bed3 ) for normal lung tissue [ 4 ]  . 
acute and late toxicities associated with treatments were evaluated by the national cancer institute common toxicity criteria for adverse events ( ctcae ) version 3.0 [ 28 ] and the radiation therapy oncology group / european organization for research and treatment of cancer late radiation morbidity scoring scheme , respectively [ 2 , 18 ]  . statistical analysis statistical analysis was performed on data including the maximum tumor diameter , dose - volume histogram , clinical and imaging follow - up , as well as overall survival rate and local control rate . 
 however , v20 is usually assessed in conventional fractions of 2.0 gy per fraction radiotherapy and its application to sbrt in the same way is controversial [ 5 , 20 ]  . 
therefore , we calculated the bed3 which corresponds to 20 gy in 30 fractions in each patient ; for example , it is almost equal to 13 gy in five fractions , and to 7.2 gy in one fraction . 
repeated balloon dilatation relieved these symptoms in 2 months . another patient who had previously received two courses of thoracic radiotherapies died of hemoptysis ( grade 5 ) 18 months after sbrt with 87.5 gy in bed10 ( patient # 16 in table 2 )  . 
previous treatments in this patient consisted of intrabronchial brachytherapy for the bilateral pulmonary hilar regions ( bed10 : 38.4 gy ) and sbrt for apical lesion in the same lobe ( bed10 : 120 gy )  . the third patient who received three courses of radiotherapy for bilateral lung tumors before sbrt for the hilar lesion suffered from grade 3 dyspnea and required domiciliary oxygen therapy 18 months after sbrt ( patient # 10 in table 2 )  . 
this patient had previously received sbrt to the right middle lung with a bed10 of 100 gy , conventional radiotherapy followed by intrabronchial brachytherapy to the left lingular segment ( bed10 : 89.4 gy ) , and sbrt to the right pulmonary hilum ( bed10 : 100 gy )  . survival and local control rates at the time of the analysis in january 2009 , nine patients were alive . 
there were four complete responses ( cr ) , 13 partial responses ( pr ) and five stable diseases ( sd ) in 6 months , and the resulting objective response rate ( cr plus pr ) was 77% . 
of the twelve patients who deceased during follow - up , nine died of cancer progression , and remaining three patients died of hemoptysis , infectious pneumonia , and epidural hemorrhage , respectively . 
polymerase chain reaction of the sputum from the patient who died of infectious pneumonia showed a high level of pneumocystis jirovecii dna , and the serum level of aspergillus antigen was high . 
the pneumonia shown on ct images was outside of the irradiated field , and the radiation fibrosis seen 2 weeks before he died had not changed for 6 months . discussion sbrt has been increasingly applied to primary nsclc and metastatic lung tumors [ 14 , 15 , 19 , 21 , 26 , 34 ] , however , its feasibility to the pulmonary hilar lesions is still controversial . 
gesamtberlebensund progressionsfreie berlebenskurven der patienten mit tumoren im bereich des lungenhilus , die sich einer stereotaktischen strahlentherapie unterzogen . after this landmark report cautioned us against using sbrt to tumors within 2 cm from the main bronchus , a few reports have been published recently which are affirmative for sbrt to the pulmonary hilum [ 1 , 12 , 27 ]  . 
however , sbrt with their regimen may not be suitable in curative intent because long - term survival can frequently be associated with major airway injury [ 12 ]  . 
this advanced image - guided technique yielded excellent local control , and was associated with a low incidence of severe toxicities within a median follow - up period of 17 months [ 1 ]  . in our present study , radiation - induced bronchial obstruction was observed in one patient who underwent sbrt as a primary treatment , and there were two cases of grade 3 toxicities in reor multitreated cases . 
it has been reported that the occurrence of bronchial stenosis is in a range from 7.5% to 80% in periods from 2 months to 4 years after high - dose - rate endobronchial brachytherapy and / or high - dose external radiotherapy [ 12 , 16 , 23 , 24 ]  . 
based on these reports and outcomes observed in this study , the indication of sbrt to hilar lesions should be carefully determined when there is an overlap with the previous treatments even in palliative intent . our study is limited by its retrospective design and , as a result , comprises patients with both nsclc and metastatic lung tumors with various stages of disease . 
considering that 20 of 21 patients had recurrent tumor or stage iv disease and surgery was indicated in none of them , the authors believe that sbrt to the pulmonary hilar region could potentially yield survival benefits . 
especially when other treatment modalities including surgery are not indicated due to poor pulmonary function or other systemic complications , sbrt can be a final option . as mentioned above , sbrt to pulmonary hilar lesions should currently be conducted with caution , because long - term follow - up in larger numbers of patients is lacking . 
for example , more precise techniques such as image - guided sbrt monitoring both intraand interfractional changes [ 9 , 20 , 25 , 31 , 32 ] are suitable candidates . 
 with these improvements in techniques , sbrt can be a useful modality not only for primary lesions in curative intent but also for recurrent lesions with reducing treatment period in palliative intent . 
although the sample size may be small , we believe that the data presented here can contribute to improving efficacy of sbrt in the future . conclusion sbrt for lung tumors located in the pulmonary hilar region may be tolerable and acceptable , if multiple treatments to the same major bronchus are avoided , and irradiated volumes are carefully taken into consideration . 
prospective studies of sbrt for lung tumors located in the pulmonary hilar region are strongly expected to prove its efficacy . strahlentherapie und onkologie original article high - grade acute organ toxicity as positive prognostic factor in primary radio ( chemo ) therapy for locally advanced , inoperable head and neck cancer hendrik andreas wolff1 , jan bosch1 , klaus jung2 , tobias overbeck3 , steffen hennies1 , christoph matthias4 , clemens f . 
roedel4 * , hans christiansen1 * purpose : to test for a possible correlation between high - grade acute organ toxicity during primary radio ( chemo ) therapy and treatment outcome in patients with locally advanced head and neck squamous cell carcinoma ( hnscc )  . patients and methods : from 05 / 1994 to 01 / 2009 , 216 hnscc patients were treated with radio ( chemo ) therapy in primary approach . 
thereby , multivariate analyses revealed that the correlation was independent of other possible prognostic factors or factors that may influence treatment toxicity , especially concomitant chemotherapy and radiotherapy technique or treatment - planning procedure . conclusion : these data indicate that normal tissue and tumor tissue may behave similarly with respect to treatment response , as high - grade acute organ toxicity during radio ( chemo ) therapy showed to be an independent prognostic marker in the own patient population . 
therefore , their hypothesis should be further analyzed on biomolecular and clinical levels and other tumor entities in prospective trials . key words : locally advanced squamous cell head neck cancer radio ( chemo ) therapy toxicity prognosis strahlenther onkol 2010 ; 186 : 2628 doi 10.1007 / s00066 - 010 - 2136 - z hhergradige akuttoxizitt als positiver prognostischer faktor bei der primren radio ( chemo ) therapie lokal fortgeschrittener , inoperabler kopf - hals - tumoren hintergrund und ziel : nach primrer radio ( chemo ) therapie lokal fortgeschrittener kopf - hals - tumoren kommt es bei einigen patienten zu einer kompletten remission , bei anderen lediglich zu einer partiellen remission mit frhem rezidiv . 
im rahmen dieser arbeit wurde geprft , ob patienten , die hhergradige akutreaktionen entwickeln , im vergleich zu patienten , bei denen diese nicht auftreten , eine bessere prognose haben . patienten und methodik : von 1994 bis 2009 wurden 216 patienten mit lokal fortgeschrittenen plattenepithelkarzinomen im kopf - hals - bereich in der eigenen klinik primr radiotherapiert ( 70 gy )  . 
akuttoxizitt grad 3 wurde vor beginn der analyse als cutoff value gewhlt , da es ab dieser toxizitt zu einer signifikanten einschrnkung der lebensqualitt der patienten kommt . * both authors share senior authorship . 1department of radiotherapy and radiooncology , university medicine gttingen , germany , 2department of medical statistics , university medicine gttingen , germany , 3department of haematology and oncology , university medicine gttingen , germany , 4department of otorhinolaryngology , university medicine gttingen , germany . received : february 23 , 2010 ; accepted : march 5 , 2010 published online : april 26 , 2010 strahlenther onkol 2010 no . 
high - grade acute organ toxicity during rct as predictor of outcome in locally advanced hnscc ergebnisse : das gesamtberleben sowie die lokoregionre kontrolle nach 5 jahren betrugen 18% bzw . 
es fand sich dabei eine statistisch signifikante korrelation zwischen hhergradiger akuter organtoxizitt und der prognose : in der gruppe der patienten mit hhergradiger akuter organtoxizitt betrugen das gesamtberleben und die lokale kontrolle nach 5 jahren 44% und 74% im vergleich zu 8% und 56% bei den patienten ohne akute hhergradige nebenwirkungen ( p < 0 , 01 , p = 0 , 04 )  . 
diese korrelation war in multivariater analyse statistisch unabhngig von anderen faktoren , die mglicherweise die toxizitt beeinflussen , wie begleitende chemotherapie oder strahlentherapieplanung ( konventionell / dreidimensional )  . schlussfolgerung : hhergradige akute organtoxizitt ist im untersuchten kollektiv ein unabhngiger positiver prognostischer faktor . 
der zusammenhang zwischen hhergradiger akuter organtoxizitt unter radio ( chemo ) therapie und der prognose sollte in prospektiven studien weiter evaluiert werden . schlsselwrter : lokale fortgeschrittene kopf - hals - tumoren radio ( chemo ) therapie toxizitt prognose ( in the following termed as conventional treatment planning ) : parallel opposed lateral portals were applied that matched to a single anterior portal encompassing the primary tumor and associated nodal drainage sites until 50 gy . 
finally , a three - dimensional ( 3 - d ) conformal external - beam radiotherapy technique was used for the boost up to a total dose of 70 gy , including the primary tumor and involved lymph nodes . 
patientencharakteristika. introduction locally advanced tumors ( uicc stages iii and iva / b ) are often inoperable because of huge volume or infiltration into adjacent tissue [ 15 ]  . 
thereby , the use of concomitant radiochemotherapy is standard nowadays , as several meta - analyses and randomized trials have shown that concomitant use of chemotherapy and radiotherapy is superior to radiotherapy alone leading to improved overall survival and locoregional control rates [ 1 , 5 , 11 , 14 , 16 , 19 ]  . 
however , the addition of chemotherapy to radiotherapy does not only improve prognosis but also increases the risk of higher ( common toxicity criteria [ ctc ] grade 3 ) treatment - related acute organ toxicity , in case of radiochemotherapy of head and neck squamous cell carcinoma ( hnscc ) mainly mucositis , skin reaction , and dysphagia [ 9 , 10 ]  . 
there is , however , an obvious interpatient variability in the development of acute organ toxicity during therapy from nearly no toxic reaction to even life - threatening adverse reactions [ 13 ]  . 
until now , only few reports analyzed treatment - related toxicity with respect to treatment outcome [ 3 , 4 , 7 , 8 , 12 , 17 , 18 , 22 , 23 ]  . 
therefore , the aim of the present study was to test for a possible correlation between high - grade acute organ toxicity ( ctc grade 3 ) during radio ( chemo ) therapy for inoperable hnscc and prognosis ( overall survival and locoregional control )  . patients and methods patient characteristics between 05 / 1994 and 01 / 2009 , 216 patients with primary inoperable hnscc without distant metastases were treated at our department . 
high - grade acute organ toxicity during rct as predictor of outcome in locally advanced hnscc from 12 / 1999 to 10 / 2008 ( 145 patients , in the following termed as 3 - d treatment - planning procedure ) , normofractionated ( 2 gy / d , five times / week ) 3 - d conformal external - beam radiotherapy was given from the beginning of radiotherapy . 
thereby , the primary tumor including involved lymph nodes and potential drainage sites on both sides of the neck including the supraclavicular region were covered with 50 gy in a first phase followed by a boost up to a total dose of 70 gy , including the primary tumor and involved lymph nodes . 
 overall , the spinal cord was limited to a maximum of 45 gy . from 05 / 1994 to 07 / 2005 , concomitant chemotherapy consisted of continuous infusion of 5 - fluorouracil ( 600 mg / m2 / total - body surface area [ tbsa ] / d on days 15 of radiotherapy ) and mitomycin c ( 10 mg / m2 / tbsa intravenously on days 5 and 36 of radiotherapy )  . 
in summary , 111 patients received this schedule in the respective time period , 65 patients refused concomitant treatment or chemotherapy could not be applied due to reduced general condition . 
thus , radiotherapy alone was carried out in these patients . from 10 / 2005 to 10 / 2008 , 40 patients were subjected to receive concomitant intravenous cisplatin 6 mg / m2 / tbsa on every radiotherapy day . 
for further analysis , acute organ toxicity was scored as high - grade side effect , if in one or more of the items mucositis , dysphagia or skin reaction were graded as ctc 3 . 
 before data analysis , acute organ toxicity grade 3 was chosen as cutoff value , because in patients with toxicity grade 3 , quality of life is significantly impaired . statistical analysis survival times were calculated from the day of histological diagnosis until the end of study . 
 collectively , the estimated 3and 5 - year locoregional control rates were 69% and 62% ( figure 1 )  . toxicity acute toxicity was subdivided as follows : 215 of 216 patients developed mucositis during radiochemotherapy ( 57 grade 1 ; 115 grade 2 ; 43 grade 3 ) , a skin reaction was seen in 216 patients ( 76 grade 1 ; 126 grade 2 ; 14 grade 3 ) , and dysphagia was noted in 166 patients ( 89 grade 1 ; 61 grade 2 ; 16 grade 3 )  . 
thereby , we showed that the correlation was independent of tumor stage or histopathologic grading and especially also of concomitant chemotherapy ( yes / no ) and radiation treatment - planning procedure ( conventional / 3 - d )  . 
high - grade acute organ toxicity during rct as predictor of outcome in locally advanced hnscc kaplan - meier estimate 95% confidence band kaplan - meier estimate 95% confidence band months months figures 1a and 1b . 
gesamtberleben , eingeteilt in patienten mit hhergradiger akuter organtoxizitt ( eine oder mehrere nebenwirkungen von mukositis , hautreaktion oder dysphagie ctc ( cid : 116 ) 3 ) oder ohne hhergradige nebenwirkungen in subgruppenanalysen fr patienten mit alleiniger radiotherapie ( a ) oder konkomittierender radiochemotherapie ( b )  . high - grade acute organ toxicity p = 0.01 high - grade acute organ toxicity p < 0.01 months months figures 4a and 4b . 
high - grade acute organ toxicity during rct as predictor of outcome in locally advanced hnscc discussion our data show a statistically significant correlation between high - grade acute organ toxicity during radio ( chemo ) therapy and prognosis . 
thereby remarkably , the correlation was independent of other possible prognostic factors or factors that may influence treatment toxicity , which may bias the univariate analysis , especially concomitant chemotherapy or radiation treatment - planning procedure in multivariate analysis : the fact that the described correlation between high - grade acute organ toxicity and prognosis was verified in subgroup analyses in multivariate analyses concerning concomitant chemotherapy as well as treatment - planning procedure emphasizes the data . our data suggest that normal tissue and tumor tissue may behave similarly with respect to treatment response . 
however , local factors might also be involved , e.g. , induction of a cytokine cascade in cases of acute reactions in normal tissues as well as in tumor tissue . 
nevertheless , our hypothesis is supported by other studies as follows : similarly to the data presented for locally advanced hnscc in this study , we have also recently found a statistically significant correlation between high - grade acute organ toxicity and overall survival in 72 patients with anal carcinoma treated with primary radiochemotherapy in curative intent [ 23 ]  . 
in that study , patients with organ toxicity ctc grade 3 ( cystitis , proctitis , or skin reaction ) had a 5 - year overall survival rate of 97% compared to 30% in patients without toxicity and locoregional control rates of 97% compared to 48% . 
 detailed analysis showed high - grade acute organ toxicity as an independent prognostic factor in multivariate analysis in that study as well . furthermore , we have also recently reported on a statistically significant correlation between high - grade acute organ toxicity ( one item of enteritis , proctitis or cystitis ctc grade 2 ) during preoperative radiochemotherapy and complete tumor regression after total mesorectal excision in multimodal treatment of locally advanced rectal cancer [ 22 ]  . 
in that study , the probability to achieve complete tumor regression after neoadjuvant treatment of patients with high - grade acute organ toxicity was more than three times higher than for patients without toxicity in multivariate analysis . similarly , dahl et al . 
 [ 4 ] found that individual radiosensitivity as determined with lymphocytes using a chromosomal assay after in vitro irradiation can be used to predict the risk of acute side effects during radiotherapy . 
however although multivariate analysis showed that acute toxicity was an independent prognostic factor , a possible influence of cofactors cannot be definitely excluded due to the retrospective nature of the study . 
therefore , these results should be considered hypothesis - generating and encourage prospective clinical research for identification of the biomolecular mechanisms underlying this finding in radiochemotherapy for head and neck cancer as well as other tumor entities . strahlentherapie und onkologie original article 18f - fet - pet - based dose painting by numbers with protons mark rickhey1 , zdenek morvek1 , christoph eilles2 , oliver koelbl1 , ludwig bogner1 purpose : to investigate the potential of 18f - fluoroethyltyrosine - positron emission tomography - ( 18f - fet - pet - ) based dose painting by numbers with protons . material and methods : due to its high specificity to brain tumor cells , fet has a high potential to serve as a target for dose painting by numbers . 
for precise treatment planning of such a prescribed dose , an intensity - modulated radiotherapy ( imrt ) algorithm including a monte carlo dose - calculation algorithm for spot - scanning protons was used . 
the resulting dose distributions were evaluated by means of dose - difference and dose - volume histograms and compared to imrt data . results : the mtf for protons was constantly above that for photons . 
die geplanten dosisverteilungen wurden mittels differenzdosisund dosis - volumen - histogrammen ausgewertet und mit imrt - daten verglichen . ergebnisse : die mtf fr protonen war stets oberhalb der von photonen . 
18f - fet - pet - based dose painting with protons introduction including biological imaging into radiotherapeutic treatment planning with low - let ( linear energy transfer ) radiation in the sense of dose painting by numbers ( dpbn ) [ 15 ] potentially leads to an inhomogeneous dose prescription . 
 conventional dose painting by simultaneously integrated boosts ( sib ) tries to consider this by optimizing homogeneous dose distributions in one or more boost subvolumes [ 8 , 29 , 32 ]  . 
dpbn follows a new concept by including biological information from positron emission tomography ( pet ) , single - photon emission tomography ( spect ) or magnetic resonance spectroscopy ( mrs ) to derive a voxel - by - voxel dose prescription . 
optimizing such a dose prescription needs a specialized inverse treatment - planning syste different attempts have been made to achieve a dose prescription from biological imaging [ 1 , 6 ] , and photons have already proven their abilities to modulate a three - dimensional dose prescription [ 12 , 26 , 31 ]  . 
in a dose - escalation model , assuming a linear tracer uptake - to - dose dependency , the abilities of a dose escalation by intensity - modulated radiotherapy ( imrt ) to tracer - accumulating regions were demonstrated by the authors in an earlier publication [ 27 ]  . as spot - scanning proton beams deposit their energy according to a bragg peak , there should be a potential to improve dpbn . 
the advantages of intensity - modulated proton therapy ( impt ) over imrt with photons have been demonstrated in different publications [ 2 , 13 , 14 , 18 , 28 , 30 , 31 , 34 , 35 ]  . the purpose of this work is to demonstrate the feasibility of an 18f - fluoroethyltyrosine - ( fet - ) pet - based dose painting approach with protons . 
as this tracer is a surrogate for elevated amino acid transport within neoplastic tissue , we interpret the accumulation of 18f - fet as a measure of the vitality of the tumor . 
in three brain tumor planning studies , we demonstrate the implementation of a voxel - by - voxel dose painting with protons based on 18f - fet - pet imaging . 
the optimization of the proton plans was done using the inverse monte carlo treatment - planning system ( imctps ) iko ( inverse kernel optimization ) developed at our department [ 3 , 21 ]  . 
finally , the results are compared to previously published photon plans [ 27 ]  . material and methods inverse monte carlo treatment planning treatment planning was carried out using the imctps iko [ 3 , 21 ]  . 
in iko , the monte carlo dose calculation algorithms vmcpro [ 11 ] for protons and xvmc [ 9 ] ( including the head model vefm [ 10 ] ) for photons were implemented . 
in case of protons , the voxel - scanning facility ( gantry i ) of the paul scherrer institute ( villigen , switzerland ) was used for the head model [ 23 ] , while in case of photons , the head model was adapted to a primus ( siemens ) linac with 1 cm leaf width related to the isocenter plane . the size of the gaussian - shaped proton pencil beam was set to a standard deviation of 5 min the plane perpendicular to the beam , the distances between the spots were set to 5 mm in each direction . 
the energies of the proton beams and , therefore , the ranges of the bragg peaks were determined in steps of 5 mm by geigers rule [ 4 , 21 ]  . 
in total , 16 , 928 proton spots were defined inside the mtf phantom and between 15 , 000 and 18 , 000 proton spots were defined in the patient study . 
in an earlier paper , the authors applied the modified mtf concept to investigate the ability of the imctps iko to follow the dose prescription in case of tiny periodic structures [ 26 ]  . 
formula 1 was only applied to the voxels inside the target volume , while the dose prescription to the voxels outside the target volume was set to zero . the dose prescriptions were implemented into iko as described in an earlier publication [ 27 ] , and proton plan optimization was performed . 
as standard evaluation methods like dose - volume histograms ( dvhs ) must fail in this context of heterogeneous dose prescriptions , we compared the optimized dose voxel by voxel with the dose prescription . 
 the dose - difference distribution is statistically evaluated by means of average values and standard deviations . due to the fact that the organs at risk ( oars ; hypophysis , brain stem , and chiasm ) in all cases were too far away from the target volume to receive a noticeable dose , a shell - like volume around the ptv with approximately 2 cm width was used for evaluation . 
the values d5% and d50% , which are the doses received by 50% and 5% of the volume , respectively , were determined for evaluation . results modulation transfer function figures 1a and 1b . 
the data points at 1 cm and 3 cm of the photon data were not considered in the fit , as the high peak - to - valley values at these points could be attributed to synchronization effects of the mlc to the calculation grid . 
der abstand k zwischen den zielvolumina variierte zwischen 1 , 25 cm und 6 , 0 cdie dosisverschreibung betrug 1 gy in den zielvolumina und 0 gy im rest des phantoms . 
die datenpunkte bei 1 cm und 3 cm der photonendaten wurden bei dem fit nicht bercksichtigt , da das hohe peak - to - valley - verhltnis auf synchronisationseffekte von mlc zum rechengitter zurckzufhren ist . 
as no experimental or clinical data were available that mapped the suv to the presence of tumor cells , we estimated the suv limits by evaluating the activity distribution inside the target volume , as conventionally defined by a physician . 
the data points at 2 and 3 cm of the photon data were not considered in the fit , as the high peak - to - valley values at these points could be attributed to synchronization effects between multileaf collimator ( mlc ) and calculation grid . 
this is a first hint at the better modulation ability of protons . 18f - fet - pet - based dose painting by numbers in figure 3 , the resulting dose distributions obtained by dpbn with protons are presented exemplarily in one transverse slice per patient . 
for each escalation level and patient the proton dose distributon was closer to the dose prescription than the photon dose distribution . the dvhs of the ptv are presented to visualize the stepwise increase of the maximum dose to the 18f - fet - accumulating subvolumes . 
compared to the previously published photon data , the dose to the normal tissue was smaller in case of impt than in case of imrt . oar and d5% discussion in this work , we presented the feasibility of 18f - fet - pet - based dose painting with protons . 
 [ 22 ] published a comparison of fdg ( fluorodeoxyglucose ) and fet uptake in brain tumors using the lesion - to - white matter ratio , which might turn out to be more significant than the suv . 
in this case , the demonstrated model can be adapted easily . for our purpose we modified the mtf in order to get a tool to measure how well a heterogeneous dose prescription can be accomplish by a treatment - planning system using different treatment modalities . 
statistical evaluation of the dose - escalation study with intensity - modulated proton therapy : d is the mean standard deviation ( sd ) of the dose - difference distributions of all esoar the mean calation levels . 
d50% oar ist der gemittelte d50% oar - wert . oar der entsprechende mittlere d5% might be caused by the fact that the mtf also depends on the parameters of the treatment machine ( width of mlc leafs or proton spot diameter )  . 
18f - fet - pet - based dose painting with protons the dose - escalation study accentuated the higher precision of proton beam dose deposition , resulting in steeper dose graoar values for dients to the surrounding normal tissue . 
alternatively , a higher escalation of the dose in the tracer - accumulating subvolumes would be possible while the dose in the surrounding tissue and the oars would be kept at an almost constant level . in this contribution , we only focused on the discussion of the physical dose . 
once an improved biological model will be available , it can be easily implemented into our system . biologically adaptive radiotherapy has the potential to improve treatment outcome , but there is an increased demand for high - precision radiotherapy to precisely hit the tiny subvolumes within each fraction . 
due to this aspect , we did our investigation on brain tumors , where intraand interfractional movements play a minor role . the dose modulation with protons and photons would become more precise if the fluence matrix had a higher resolution , and if the proton pencil beams had a smaller lateral and longitudinal width , respectively . 
the best results were obtained by a dose painting concept with spot - scanning protons . conclusion the results show that both treatment modalities , protons as well as photons , are applicable to a three - dimensional dose modulation in the sense of dpbn . 
unlike photon beams , the dose deposition of proton beams is not only restricted in the two lateral dimensions , but according to the sharp distal fall - off also restricted in the third dimension . 
 strahlentherapie und onkologie original article prognostic impact of vegf and vegf receptor 1 ( flt1 ) expression in patients irradiated for stage ii / iii non - small cell lung cancer ( nsclc ) dirk rades1 , cornelia setter1 , juergen dunst1 , olav dahl2 , 3 , steven e . 
schild4 , frank noack5 background and purpose : the prognostic value of the tumor expression of vascular endothelial growth factor ( vegf ) and vegf receptor 1 ( flt1 ) is still unclear . 
this study investigated the impact of tumor expression of vegf and flt1 on outcomes in 61 patients irradiated for stage ii / iii non - small cell lung cancer ( nsclc )  . material and methods : the impact of tumor vegf and flt expression and twelve additional potential prognostic factors on locoregional control ( lc ) , metastases - free survival ( mfs ) , and overall survival ( os ) were retrospectively evaluated . 
diese studie untersuchte den einfluss der tumorexpression von vegf und flt1 auf die prognose nach strahlentherapie von 61 patienten mit einem nichtkleinzelligen bronchialkarzinom ( nsclc ) im stadium ii / iii . material und methodik : der einfluss von vegf und flt sowie zwlf weiteren mglichen prognosefaktoren auf die lokoregionale kontrolle ( lc ) , das metastasenfreie berleben ( mfs ) und das gesamtberleben ( os ) wurde retrospektiv evaluiert . 
diese faktoren waren alter , geschlecht , allgemeinzustand , histologie , histologisches grading , t - kategorie , n - kategorie , operation , chemotherapie , pack - years , rauchen whrend strahlentherapie und hmoglobinwerte whrend strahlentherapie ( tabelle 1 )  . ergebnisse : in der univariaten analyse war eine bessere lc mit niedrigerer t - kategorie ( p = 0 , 046 ) , niedrigerer n - kategorie ( p = 0 , 047 ) und nichtrauchen whrend strahlentherapie ( p = 0 , 012 ) assoziiert ( tabelle 2 )  . 
vegf ( p = 0 , 26 ) und flt1 - expression 1department of radiation oncology , university of lbeck , germany , 2section of oncology , institute of medicine , university of bergen , norway , 3department of oncology , haukeland university hospital , bergen , norway , 4department of radiation oncology , mayo clinic , scottsdale , az , usa , 5institute of pathology , university of lubeck , germany . 
in der univariaten analyse war ein besseres mfs mit niedrigerer t - kategorie ( p = 0 , 034 ) , niedrigerer n - kategorie ( p = 0 , 027 ) und fast mit hmoglobinwerten 12 g / dl ( p = 0 , 053 ) assoziiert ( tabelle 3 )  . 
in der multivarianzanalyse blieb die n - kategorie ( p = 0 , 011 ) signifikant . schlussfolgerung : die tumorexpression von vegf und flt1 scheint keinen signifikanten einfluss auf die prognose nach bestrahlung aufgrund eines nsclc im stadium ii / iii zu haben . schlsselwrter : nichtkleinzelliges bronchialkarzinom vegf - expression flt1 - expression prognose introduction uncertainty exists regarding the prognostic value of tumor expression of vascular endothelial growth factor ( vegf ) and the vegf receptor 1 ( flt1 ) with respect to outcomes of cancer treatment . 
tumor expression of vegf has been suggested to be a negative prognostic factor in retrospective studies of esophageal cancer and head and neck cancer [ 16 , 20 , 23 , 25 ]  . 
however , it was not found to be a prognostic factor in patients with stage i / ii non - small cell lung cancer ( nsclc ) and epithelial ovarian cancer [ 6 , 22 ]  . 
the present study investigated the effect of vegf and flt1 tumor expression on locoregional control ( lc ) , metastases - free survival ( mfs ) , and overall survival ( os ) in patients irradiated for stage ii / iii nsclc . 
modern radiotherapy techniques , fractionation regimens , and novel anticancer drugs have been included in the treatment strategies and are the subject of many clinical studies in lung cancer patients [ 12 , 17 , 18 , 24 , 28 ]  . 
resected nsclc tissues were fixed in 10% buffered formalin ( ph 7.0 ) , embedded in paraff the formalin - fixed , paraffin - embedded tumor samples were used for the preparation of a tumor tissue microarray ( tma ) block . 
the tma block was constructed using a manual tissue arrayer 1 ( beecher instruments , silver spring , md , usa ) with a 1.0 - mm diameter core biopsy needle . 
endogenous peroxidase was blocked with 0.3% hydrogen peroxidase for 5 m then , the sections were incubated with the antihuman vegf polyclonal antibody ( mouse ; 1 / 100 dilution ; santa cruz biotechnology , heidelberg , germany ) and antihuman flt1 monoclonal antibody ( mouse , 1 / 30 dilution ; santa cruz biotechnology )  . 
 sections were washed with tbs containing 0.1% tween 20 ( ph 7.0 ) and subsequent reaction was performed with the biotin - free horseradish peroxidase enzyme - labeled polymer of the powervision system ( immunologic , duiven , the netherlands )  . 
 sections were counterstained with hematoxylaccording to a previous report [ 20 ] , the tumors were considered as expressing vegf and flt1 if at least 10% of the tumor cells were positive . material and methods treatment the expression levels of vegf and flt1 were evaluated in tumor samples obtained before radiotherapy from 61 patients who were irradiated for nsclc at the university of lbeck , germany , between 01 / 2000 and 12 / 2005 . 
these patients are a subgroup with available tissue samples and successful staining for vegf and / or flt1 of our preceding study of prognostic factors in nsclc [ 21 ]  . 
all patients were smokers at the time radiotherapy was performed after computed tomography - ( ct - ) based three - dimensional treatment planning with a linear accelerator and 6to 18 - mv photons . 
the target volume included the primary tumor and the locoregional lymph nodes with a margin of 2 cthe total dose given as the equivalent dose in 2 - gy fractions ( eqd2 ) ranged between 54 gy and 70 gy and did depend on the treatment schedule favored at our institution strahlenther onkol 2010 nr . 
flt1 : vaskulrer endothelialer wachstumsfaktor - rezeptor 1 ; rt : strahlentherapie ; scc : plattenepithelkarzinom ; vegf : vaskulrer endothelialer wachstumsfaktor . patients during different periods of time and on the extent of resection performed in patients having surgery . 
the eqd2 was 6670 gy after r2 resection ( macroscopically residual tumor ) or for definitive treatment , 6066 gy after r1 resection ( microscopically residual tumor ) , 5460 gy after r0 resection ( no residual tumor )  . 
the majority of hemoglobin levels during radiotherapy were either at least three of five levels , at least four of six levels ( the situation that three of six levels were < 12 g / dl did not occur ) , or at least four of seven levels . 
the potential prognostic factors found to be significant or of borderline significance ( p 0.06 ) in the univariate analysis were additionally evaluated in a multivariate analysis performed using the cox proportional hazards model . 
patients were followed until death or for a median of 20 months ( range : 1261 months ) in those alive at last evaluation . results a locoregional failure occurred in 26 of the 61 patients after a median of 9 months . 
in the entire cohort , the lc rates at 1 year 65 years > 65 years gender female male karnofsky performance score 70 > 70 histology adenocarcinoma large cell carcinoma histological grade g12 t - stage n - stage surgery chemotherapy pack - years 50 > 50 unknown smoking during rt hemoglobin levels during rt < 12 g / dl 12 g / dl vegf expression unknown flt1 expression unknown strahlenther onkol 2010 nr . 
lower t - category ( rr : 1.25 ; 95% ci : 0.811.92 ; p = 0.31 ) and surgery ( rr : 1.35 ; 95% ci : 0.563.33 ; p = 0.50 ) were not significant in the multivariate analysis of lc . distant metastases occurred in 33 of the 61 patients after a median of 8 months . 
on univariate analysis , improved os was significantly associated with lower t - category ( p = 0.028 ) , lower n - category ( p = 0.003 ) , not smoking during radiotherapy strahlenther onkol 2010 nr . 
 lower t - category ( rr : 1.27 ; 95% ci : 0.861.89 ; p = 0.22 ) and surgery ( rr : 1.90 ; 95% ci : 0.874.61 ; p = 0.11 ) were not significant in the multivariate analysis of os . discussion the prognostic impact of tumor cell expression of vegf and its receptor flt1 is controversial . 
similarly did not observe a significant association between expression of vegf and progression free survival or os in a retrospective series of 67 patients with epithelian ovarian cancer [ 22 ]  . 
suggested vegf - c expression to be a predictive factor for regional lymph node recurrence in a series of 73 patients with scc of the tongue [ 25 ]  . 
reported significantly ( p = 0.04 ) poorer survival for patients with vegf - positive tumors in a retrospective series of 117 patients with scc of the esophagus at various tumor stages [ 23 ]  . the prognostic value of flt1 is also not clear . 
found a significant association between low expression of flt1 and both poor prognosis and advanced tumor stage in a series of 76 patients with pancreatic adenocarcinoma [ 5 ]  . in contrast to expression of vegf or flt1 , treatment outcomes were associated with n - category and lc nearly with smoking during radiotherapy . 
 improvement of lc in patients who stopped smoking before radiotherapy is most likely due to better tumor oxygenation as a result of improved oxygen - carrying capacity of hemoglobin due to less carboxyhemoglobin [ 7 , 10 , 11 , 29 ]  . 
presented a retrospective study of 286 patients with superficial transitional cell bladder carcinoma and observed that patients who continued smoking had a significantly worse lc than ex - smokers or patients who quitted smoking before radiotherapy [ 8 ]  . 
it is possible that these receptors may have some importance when assessing patients treated with agents that specifically target the vegf pathways . strahlentherapie und onkologie originalarbeit die situation der angehrigen von strahlentherapiepatienten eine bestandsaufnahme felix momm1 , sabine lingg1 , carola xander2 , sonja adebahr1 , anca - ligia grosu1 , gerhild becker2 hintergrund und ziel : untersuchungen haben gezeigt , dass die angehrigen aus patientensicht einen sehr hohen stellenwert bei der entscheidungsfindung zur durchfhrung medizinischer behandlungsmanahmen einnehmen . 
durch eine gezielte befragung der nchsten angehrigen von strahlentherapiepatienten wurde daher die situation dieser personengruppe im sinne einer bestandsaufnahme untersucht . befragte stichprobe und methodik : mittels eines neu entwickelten fragebogens wurden in einem definierten erhebungszeitraum von 6 wochen insgesamt 470 angehrige von strahlentherapiepatienten ( auswertbarer rcklauf : n = 287 , rcklaufquote = 61% ) ber die zufriedenheit mit ihrer einbindung in den therapieablauf befragt . 
des weiteren wurden bei der befragten stichprobe ausknfte ber die spezifischen bedrfnisse von angehrigen sowie vorschlge zu konkreten verbesserungsmglichkeiten im kontext einer strahlentherapeutischen behandlung erhoben . ergebnisse : insgesamt waren die angehrigen mit ihrer einbindung in die therapieablufe und mit der betreuung der patienten zufrieden . 
 unmittelbare verbesserungsmglichkeiten ergaben sich jedoch im bereich der interdisziplinren information ber onkologische themen sowie beim organisationsablauf . schlussfolgerung : die situation der angehrigen von strahlentherapiepatienten war in der bestandsaufnahme insgesamt zufriedenstellend . 
als vorbild knnen strukturen aus der palliativmedizin dienen . schlsselwrter : strahlentherapie angehrige patienteninformation patientenbetreuung lebensqualitt strahlenther onkol 2010 ; 186 : 34450 doi 10.1007 / s00066 - 010 - 2111 - 8 the situation of radiation oncology patients relatives . 
therefore , the situation of this group was investigated in the sense of a stocktaking by interviewing the closest relatives of radiotherapy patients . interviewed persons and methods : in a defined span of time ( 6 weeks ) , a total of 470 relatives ( evaluable : n = 287 , 61% ) of radiotherapy patients were interviewed by a newly developed questionnaire about their contentment with their inclusion in the therapy course . 
further , they gave information about specific needs of relatives as well as proposals for direct improvements in the context of a radiation therapy . results : in total , the relatives were satisfied with their inclusion in the radiotherapy course and with the patient care . 
nevertheless , direct possibilities for improvements were found in the interdisciplinary information about oncologic topics and in the organization of the therapy course . conclusion : in the stocktaking the situation of radiotherapy patients relatives was generally satisfactory . 
antibiotischer therapie oder parenteraler ernhrung berleben tumorpatienten fr immer lngere zeit und mssen somit in zunehmendem mae mit ihren krankheitsbedingten problemen in ihr soziales umfeld ( re ) integriert werden . 
 eine ausnahme stellt in diesem bereich die pdiatrische onkologie dar : bereits frh wurden die eltern und geschwister krebskranker kinder psychologisch , mit informationsveranstaltungen und selbsthilfegruppen untersttzt [ 7 , 12 , 13 ]  . 
untersuchungen an strahlentherapeutischen und anderen onkologischen patienten zeigen jedoch , dass die angehrigen aus patientensicht einen sehr hohen stellenwert bei der entscheidungsfindung und krankheitsverarbeitung haben [ 1 , 11 , 19 , 21 ]  . 
alle patienten bei der erstvorstellung vor therapiebeginn , whrend der therapie ( ambulant und stationr ) sowie die patienten in der nachsorge , um die mitarbeit bei dieser untersuchung gebeten . 
6 antwort ja / nein 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert 6p - likert jeweils 6p - likert freitext freitext momm f , et al . 
bei der entwicklung des fragebogens wurde besonders darauf geachtet , die tendenz sozial erwnschter antworten im sinne des social desirability bias gering zu halten sowie die tendenz zur mitte ( error of central tendency ) und andere systematische antwortverzerrungen zu minimieren [ 3 , 4 ] : einige fragen wurden bewusst negativ formuliert , um der sog . 
fragenformulierungen , positionseffekte ( effekte , die aus der reihenfolge der fragenitems resultieren , indem eine vorher gestellte frage einen einfluss auf die bewertung der folgenden frage hat ) und andere systematische fehlerquellen geprnach testung des fragebogens wurde die befragung von einer nicht in die klinische patientenbetreuung involvierten medizinischen doktorandin ( s.l. ) durchgefhrt , um eine verzerrung durch interviewermerkmale zu minimieren . 
die bgen wurden vertraulich und in faktisch anonymisierter form ausgewertet , um sowohl eine verzerrung durch sozial erwnschte antworten als auch negative einflsse auf das arzt - patienten - verhltnis zu minimieren . datenverarbeitung und statistik die elektronische dateneingabe erfolgte manuell durch zwei unabhngige personen mit einem anschlieenden 1 : 1 - abgleich . 
 der studie wurde nach begutachtung und erteilung eines positiven votums durch die ethikkommission der albert - ludwigs - universitt freiburg durchgefhrt . ergebnisse demographische daten die demographischen daten der angehrigen sind in tabelle 3 zusammengefasst . 
die mehrheit der befragten waren angehrige von nachsorgepatienten . patientenbetreuung , einbindung der angehrigen die antworten der angehrigen auf die fragen bezglich der zufriedenheit mit der patientenbetreuung und der einbindung angehriger sind in abbildung 1 zusammengefasst . 
 von der betreuung der patienten in der klinik hatten die angehrigen insgesamt einen guten eindruck : lediglich etwa 5% der befragten stimmten der aussage hier in der klinik wird mein kranker angehriger gut betreut nicht zu . 
als indikator fr eine vorliegende depression : sie wurde sehr unterschiedlich beantwortet , wobei insgesamt eher eine mittlere stimmungslage zu erkennen war . organisation einer der wichtigsten fragenkomplexe mit unmittelbarem zusammenhang zur alltagsroutine war der bereich der organisation ( abbildung 2 )  . 
den grten informationsbedarf gaben die angehrigen im bereich strahlentherapie an , der sie zur zeit der befragung direkt betraf . freitext : negative und positive erlebnisse , kritik und lob die freitextfrage bezglich der negativen erlebnisse bzw . 
results : general questions n = 287 ; questions about patient information n = 218 ( relatives who were present during the information talk )  . insgesamt wurde die klinik von den angehrigen aber eher gelobt . 
nahezu 90% der positiven antworten bezogen sich direkt auf die freundlichkeit des personals ( rzte , mtras , pflegekrfte ) und auf die guten , pnktlichen und reibungslosen organisationsablufe der klinik . diskussion wenn ich einem neuen patienten in der praxis oder auf station zur begrung die hand gebe , muss ich wissen , dass dies schon mein erster irrtum ist . 
angehrige von strahlentherapiepatienten durch ihre untersttzung wesentlich zum erfolg einer therapie und vor allem zur krankheitsverarbeitung und - bewltigung beitragen kann [ 2 , 22 ] , was wiederum in direktem zusammenhang mit der lebensqualitt steht [ 1416 , 24 , 25 , 28 ]  . im klinischen alltag erleben wir hufig , dass patienten ausknfte zu ihrer erkrankung und sogar entscheidungen ber therapiemanahmen an ihren lebenspartner , ihre kinder oder andere nahe angehrigen delegieren [ 21 ]  . 
whrend bei unkomplizierten akuten erkrankungen und medizinischer routineversorgung die einbeziehung der angehrigen weniger erforderlich erscheint , wchst die bedeutung der angehrigen mit der schwere der erkrankung [ 5 ]  . mit der grndung von tumorzentren und einem zunehmend ganzheitlichen blickwinkel auf die patienten wird den angehrigen schwer erkrankter patienten zunehmend mehr aufmerksamkeit zuteil . 
dies hat auch rckwirkungen auf den patienten selbst ; untersuchungen konnten zeigen , dass die sorge um die angehrigen von schwer erkrankten patienten neben der kontrolle krperlich belastender symptome als das wichtigste problem angegeben wurde [ 10 ]  . 
dies deckt sich mit den in der literatur bekannten daten , die ein hohes informationsbedrfnis nicht nur von patienten , sondern auch von angehrigen zeigen [ 10 , 29 ]  . 
 bei den durch uns befragten angehrigen von strahlentherapiepatienten waren die themen der gewnschten informationsveranstaltungen weit gestreut und betrafen auch whrend der strahlentherapie nicht nur das eigene fachgebiet , sondern fast in gleichem mae ebenfalls chemotherapeutische optionen , schmerztherapie oder psychoonkologische themen . 
ein solches zustzliches informationsangebot kann dann von den patienten gemeinsam mit den angehrigen genutzt werden und ergnzt vielfltige andere informationsquellen [ 8 , 17 , 18 , 20 ]  . 
so sind die angehrigen der patienten zwar zum weit berwiegenden teil bereit , auch lngere anfahrtswege fr eine strahlentherapie zu akzeptieren , beklagten sich jedoch in den sehr aufschlussreichen freitextteilen z.b. 
solche organisatorischen probleme knnen sehr schnell angegangen werden , im konkreten fall durch ein verbessertes parkplatzmanagement mit rigorosen kontrollen , so dass durch relativ wenig aufwand ein deutlicher zuwachs an zufriedenheit bei den angehrigen erreicht werden kann . fr die meisten angehrigen war es sehr wichtig , dass die patienten einen festen , planbaren bestrahlungstermin zugeteilt bekamen . 
die zuverlssigkeit der bestrahlungsgerte ein ganz wesentlicher faktor . des weiteren verbessern elektronische betriebsablaufsysteme die situation des komplexen terminmanagements in der strahlentherapie ganz wesentlich [ 9 , 23 ]  . selbst wenn die groe mehrheit der angehrigen sich positiv ber die betreuung uert , muss man die kleine untergruppe mit problemen erkennen und entsprechend versorgen . 
6 strahlentherapie und onkologie current discussion retrospective study of neoadjuvant versus adjuvant radiochemotherapy in locally advanced noninflammatory breast cancer survival advantage in ct2 category by neoadjuvant radiochemotherapy * stephan ludwig roth1 , werner audretsch2 , hans bojar3 , innokentij lang1 , reinhart willers4 , wilfried budach1 purpose : this retrospective study compares patients treated between 1991 and 1998 with neoadjuvant radiotherapy chemotherapy ( rct ) or adjuvant rct for locally advanced noninflammatory breast cancers ( labc ) in terms of pathologic complete response ( pcr ) , 10 - year relapse - free ( rfs ) , and overall survival ( os )  . patients and methods : preoperative rct in 315 and adjuvant rct in 329 cases consisted in 50 gy ( 5 2 gy / week ) to the breast and the supra - / infraclavicular lymph nodes . 
101 neoadjuvant patients received in case of breast conservation a 10 - gy interstitial boost with 192ir afterloading before and 214 neoadjuvant patients a preoperative electron boost after external - beam radiotherapy . 
in the adjuvant rct group , chemotherapy was applied to 44 patients before surgery and to 166 after surgery ; 119 had no chemotherapy . results : breast conservation became possible in 50.8% after neoadjuvant rct for labc with a pcr rate at surgery of 29.2%. 
 a complete nodal remission ( pn0 ) after rct was observed in 56% ( 89 / 159 ) of the cn + ( clinically node - positive ) neoadjuvant patients . 
for patients with ct2 tumors the rfs and os were statistically significantly better ( hr = 0.5090 ; p = 0.0130 for rfs ; hr = 0.4390 ; p = 0.0026 for os ) after neoadjuvant compared to adjuvant rct . conclusion : neoadjuvant rct achieved a pcr rate of 29.2% and a statistically significantly better rfs and os in patients with ct2 - category breast cancer . key words : breast cancer neoadjuvant radiotherapy chemotherapy retrospective study strahlenther onkol 2010 ; 186 : 299306 doi 10.1007 / s00066 - 010 - 2143 - 0 retrospektive studie einer neoadjuvanten versus adjuvanten radiochemotherapie beim lokal fortgeschrittenen mammakarzinoberlebensvorteil fr die ct2 - kategorie durch eine neoadjuvante radiochemotherapie ziel : die studie untersucht retrospektiv die daten von patientinnen , die in den jahren 19911998 wegen eines lokal fortgeschrittenen , nichtinflammatorischen mammakarzinoms ( labc ) behandelt wurden . 
verglichen werden eine neoadjuvante strahlentherapie chemotherapie ( rct ) mit einer adjuvanten rct hinsichtlich der pathologisch kompletten remission ( pcr ) , der 10 - jahres - erkrankungsfreiheit ( rfs ) und des gesamtberlebens ( os )  . patienten und methodik : bei 315 patientinnen mit einer properativen rct und bei 329 patientinnen mit einer adjuvanten rct wurden 50 gy ( 5 2 gy / woche ) auf die brust und die supra - / infraklavikulren lymphknoten appliziert . 
101 neoadjuvante patientinnen erhielten im fall einer brusterhaltung einen interstitiellen 10 - gy - boost mit 192ir - afterloading vor und 214 neoadjuvante patientinnen einen 10 - gy - elektronenboost nach externer strahlentherapie . 
die chemotherapie wurde in der neoadjuvanten * presented at the 2009 asco annual meeting , orlando , fl , usa [ 26 ]  . 1department of radiotherapy , university of dsseldorf , germany , 2breast center , marien - hospital , dsseldorf , germany , 3institute for oncologic chemistry , university of dsseldorf , germany , 4computer center , university of dsseldorf , germany . received : march 11 , 2010 ; accepted : march 19 , 2010 published online : may 21 , 2010 strahlenther onkol 2010 nr . 
im gesamtkollektiv war zwar die neoadjuvante der adjuvanten therapie hinsichtlich rfs und os nur tendenziell berlegen ( hazard - ratio [ hr ] = 0 , 85 ; p = 0 , 09 fr rfs ; hr = 0 , 8130 ; p = 0 , 1037 fr os ) , bei patientinnen mit einer ct2 - kategorie erwiesen sich jedoch rfs und os nach einer neoadjuvant rct als signifikant besser als nach einer adjuvanten rct ( hr = 0 , 5090 ; p = 0 , 0130 fr rfs ; hr = 0 , 4390 ; p = 0 , 0026 fr os )  . schlussfolgerung : eine neoadjuvante rct erzielte eine brusterhaltung bei 50 , 8% der labc , eine pcr - rate von 29 , 2% und bei cn + eine pn0 - rate von 56% . 
bei patientinnen mit einer ct2 - kategorie waren rfs und os nach einer neoadjuvanten versus einer adjuvanten rct statistisch signifikant berlegen . schlsselwrter : mammakarzinom neoadjuvant radiotherapie chemotherapie retrospektive studie introduction interdisciplinary guidelines for the treatment of breast cancer recommend neoadjuvant radiotherapy , possibly in combination with systemic therapy , only for inoperable stage iii , if the disease remains inoperable following systemic therapy [ 11 , 19 , 28 , 30 ]  . 
neoadjuvant chemotherapy alone is recommended in these indications , because patients , who achieve a pathologic complete remission ( pcr ) , have a superior chance of survival as compared to patients without pcr [ 3 , 6 , 8 , 9 , 14 , 22 , 25 , 31 , 34 ]  . the aim of the current retrospective , nonrandomized , monocenter study was to present the 10 - year results of neoadjuvant radiotherapy plus chemotherapy ( rct ) locally advanced noninflammatory breast cancers ( labc )  . patients and methods patients between 1991 and 1998 , 315 labc patients without distant metastases received neoadjuvant rct at the university hospital of dsseldorf and the interdisciplinary breast center ibc , sana hospital , dsseldorf , germany . 
eligibility criteria included untreated , histologically confirmed , invasive adenocarcinoma of the breast not amenable to breast - conserving surgery ( tumor size relative to breast volume , unfavorable location of the tumor bed , or multifocal t1 , and extended intraductal component [ eic ] ) , stages iiaiiic according to the international union against cancer ( icru ) criteria . 
stage distribution was comparable in neoadjuvant versus adjuvant patients : stage 2 : n = 160 versus 155 ; stage 3 : n = 155 versus 174 . treatment systemic treatment chemotherapy in the neoadjuvant rct group , chemotherapy consisted of 4 ec ( epirubicin , cyclophosphamide ) in 53% , mitoxantrone in 35.6% , 4 ac ( adriamycin , cyclophosphamide ) in 6.7% , no chemotherapy in 3.2% , 3 cmf ( cyclophosphamide , methotrexate , 5 - fluorouracil ) in 0.3% , 6 cmf in 0.3% , and 6 ec in 0.3%. 
patientencharakteristika von 644 retrospektiv ausgewerteten brustkrebspatienten aus dsseldorf , deutschland . neoadjuvant radiotherapy chemotherapy adjuvant radiotherapy chemotherapy patients ( n ) 50 years > 50 years ct - categories ct1 + ct2 cn - categories pathologic t - categories 3 97 78 46 4 11 82 1 62 86 4 13 51 79 strahlenther onkol 2010 nr . 
119 patients had no chemotherapy . hormonal therapy in the neoadjuvant group , 241 patients received additional hormonal treatment with tamoxifen or a luteinizing hormone - releasing hormone ( lhrh ) agonist . 
preoperative radiotherapy consisted of one course of external - beam radiotherapy of 50 gy ( icru ) to the breast and the supra - / infraclavicular lymph nodes , using 5 2.0 gy / week via tangential fields . 
the energy depended on the breast size : 6to 10 - mvx photons in large breasts ( n = 161 ) versus 60co in small breasts ( n = 154 )  . 
214 neoadjuvant patients ( 82 / 100 patients with ct1t2 tumors , 84 / 137 patients with ct3 tumors , and 48 / 78 patients with ct4 tumors ) received only an electron boost after external - beam radiotherapy and no interstitial boost . surgery the original tumor location was marked with ink and documented by photographs prior to treatment . 
the extent of the resection depended on the relative volume of the tumor prior to rct and of the breast - tumor relationship . pathology tumor response pathologic tumors with an epithelial malignant residual component strictly in situ or representing < 5% of the breast tumor mass without any mitosis were classified in the group of in - breast pcr . 
since pcr did take histological nodal status into account , patients with pcr after neoadjuvant rct had no positive breast tumor cells and no axillary lymph nodes at surgery . statistical analysis for all patients with neoadjuvant rct , the preoperative ct - category and cn - category were known . 
primary endpoint were the pcr , pt0 and pn0 rates , as well as the 10 - year overall ( os ) and relapse - free survival ( rfs ) rates of patients with neoadjuvant versus adjuvant rct . 
the os period was defined as the elapsed interval between the start of treatment and the date of death regardless of etiology , and the date of end of follow - up , respectively . 
circumstances for the calculations of rfs included all local , regional , or distant recurrences , whereas occurrences of contralateral breast cancer , other second primary cancer , and deaths without recurrence were treated as censoring circumstances . the survival probability was estimated by the actuarial method [ 18 ]  . 
preoperative versus adjuvant radiochemotherapy in labc discussion breast conservation although , in general , the patients suffered from labc , breast - conserving surgery could be performed on 160 / 315 neoadjuvant patients ( 50.8% ) with tumor - specific reconstruction [ 2 , 24 ]  . tumor remission rates in our series , complete tumor remission after neoadjuvant rct was observed in 37% of patients ( 116 / 315 )  . 
 [ 29 ] reported an even higher primary tumor downstaging of 45% after neoadjuvant simultaneous rct with cmf or ec or ac . nodal remission rates a complete nodal remission ( pn0 ) after neoadjuvant rct was observed in 56% of our node - positive ( cn + ) patients ( 89 / 156 )  . 
this implies that achieving a better degree of control of the primary tumor and of regional metastases in the radiation field may ultimately lead to better survival rates . relapse - free survival and overall survival advantage after neoadjuvant versus adjuvant radiotherapy this series is the first in the literature to compare long term rfs and os after neoadjuvant rct and adjuvant rct in labc or surgically unfavorable breast cancer . 
obwohl der klinische tumordurchmesser bei den patientinnen mit einer pt2 - kategorie bei den neoadjuvant behandelten grer war , konnte trotzdem durch eine neoadjuvante rct in 59% pn0 erzielt werden vs . 
yet 59% of the 97 neoadjuvant ct2 cases were pathologically node - negative after rct versus 31% of the 180 ct2 cases in the adjuvant group ( figure 6 )  . 
for a tumor control probability of 75% , 80100 gy must be applied [ 23 , 33 ]  . the advantage of combined rct compared to chemotherapy alone is presumed to be due to the higher tumoricidal effect against the stem and progenitor cells in the mammary gland [ 12 , 17 ]  . 
if the disease is limited to the breast and the regional nodes , the radiotherapy field may include the whole primary tumor and the occult regional nodal disease and radiation field may destroy more occult stem cell metastases [ 5 , 32 ]  . 
 strahlentherapie und onkologie original article new multileaf collimator with a leaf width of 5 mm improves plan quality compared to 10 mm in step - and - shoot imrt of hnc using integrated boost procedure felix zwicker1 , 2 , henrik hauswald1 , simeon nill3 , bernhard rhein3 , christian thieke2 , falk roeder1 , 2 , carmen timke1 , 2 , angelika zabel - du bois1 , 2 , jrgen debus1 , peter e . 
huber1 , 2 purpose : to investigate whether a new multileaf collimator with a leaf width of 5 mm ( mlc - 5 ) over the entire field size of 40 40 cm2 improves plan quality compared to a leaf width of 10 mm ( mlc - 10 ) in intensity - modulated radiotherapy ( imrt ) with integrated boost for head and neck cancer . patients and methods : a plan comparison was performed for ten patients with head and neck cancer . 
for each patient , seven plans were calculated : one plan with mlc - 10 and nine beams , four plans with mlc - 5 and nine beams ( with different intensity levels and two - dimensional median filter sizes [ 2d - mfs ] ) , and one seven - beam plan with mlc - 5 and mlc - 10 , respectively . 
mean values of common plan parameters over all ten patients were estimated , and plan groups of mlc - 5 and mlc - 10 with nine and seven beams were compared . results : the use of mlc - 5 led to a significantly higher conformity index and an improvement of the 90% coverage of ptv1 ( planning target volume ) and ptv2 compared with mlc - 10 . 
within the nine - beam group with mlc - 5 , a reduction of the segment number by up to 25% at reduced intensity levels and for increased 2d - mfs did not markedly worsen plan quality . 
interestingly , a seven - beam imrt with mlc - 5 was inferior to a nine - beam imrt with mlc - 5 , but superior to a nine - beam imrt with mlc - 10 . conclusion : the use of an mlc - 5 has significant advantages over an mlc - 10 with respect to target coverage and protection of normal tissues in step - and - shoot imrt of head and neck cancer . key words : imrt multileaf collimator 5 mm leaf width conformity index ( ci ) head and neck cancer ( hnc ) strahlenther onkol 2010 ; 186 : 33443 doi 10.1007 / s00066 - 010 - 2103 - 8 ein neuer multileafkollimator mit einer lamellenbreite von 5 mm verbessert die planqualitt im vergleich zu einer lamellenbreite von 10 mm bei der step - and - shoot - imrt mit integriertem boostverfahren bei kopf - hals - tumoren ziel : gegenstand dieser untersuchung war , ob bei der intensittsmodulierten radiotherapie ( imrt ) von kopf - hals - tumoren mit integriertem boost ein neuer kommerzieller multileafkollimator mit einer lamellenblende von 5 mm ( mlc - 5 ) ber eine feldgre von 40 40 cm2 zu einer verbesserung der planqualitt im vergleich zu einer lamellenblende von 10 mm ( mlc - 10 ) fhrt . patienten und methodik : der planvergleich wurde an zehn patienten mit kopf - hals - tumoren durchgefhrt . 
neun und sieben feldern miteinander verglichen . ergebnisse : der einsatz eines mlc - 5 fhrt im vergleich zu einem mlc - 10 zu einer signifikanten verbesserung des konformittsindex und zu einer erhhung von v90 des ptv1 ( planungszielvolumen ) und ptv2 ( tabellen 14 , abbildung 3 )  . 
innerhalb der neun - felder - plangruppen mit mlc - 5 fhrte eine verringerung der 1department of radiation oncology , university of heidelberg , germany , 2clinical cooperation unit radiation oncology , dkfz , heidelberg , germany , 3division of medical physics in radiation oncology , dkfz , heidelberg , germany . received : november 19 , 2009 ; accepted : march 18 , 2010 published online : may 21 , 2010 strahlenther onkol 2010 nr . 
5 - mm mlc in imrt of hnc segmentanzahl um 25% durch reduktion der intensittslevel und / oder des 2d - mfs nicht zu einer verschlechterung der planqualitt ( abbildung 2 )  . 
eine sieben - felder - imrt mit mlc - 5 war einer neun - felder - imrt mit mlc - 5 unterlegen , aber besser als eine neun - felder - imrt mit mlc - 10 . schlussfolgerung : die verwendung eines mlc - 5 weist gegenber einem mlc - 10 signifikante vorteile bezglich der zielvolumenabdeckung und der normalgewebsschonung bei der step - and - shoot - imrt von kopf - hals - tumoren mit integrierter boostapplikation auf . schlsselwrter : imrt multileafkollimator 5 - mm - leafbreite konformittsindex kopf - hals - tumoren introduction intensity - modulated radiotherapy ( imrt ) gains increasing acceptance in radiation therapy of head and neck cancer ( hnc ) due to the homogeneous target volume coverage and protection of organs at risk ( oars ) like spinal cord , brain stem or parotid glands [ 2 , 8 , 13 , 19 ]  . 
another advantage of imrt is the possibility to integrate a boost , which saves time and leads to a slightly higher , biologically more effective single dose in the boost volume [ 14 ]  . 
however , phantom studies have demonstrated that more than eleven fields cannot further improve plan quality ; the same applies to a leaf width < 3 mm [ 1 , 911 ]  . 
newer commercial collimators integrate thinner leaves either by the introduction of an additional micro - mlc into the beam or by the insertion of thinner leaves into the central area of the mlc and preservation of the usual 10 - mm leaves in the outer area ( e.g. , dynamic imrt with varian 120mlc or hd - 120mlc )  . 
in these collimators , the maximum field size with a smaller leaf width of 5 mm ( mlc - 5 ) is up to 22 22 cm2 . the irradiation of patients with hnc frequently requires the inclusion of the entire cervical lymphatic drainage , causing radiation fields with a length of up to 25 cm extending from the base of the skull to the clavicle . the first mlc - 5 with an entire field size of 40 40 cm2 ( 160mlc , siemens ) has become commercially available in 2008 . 
with this collimator it is possible to deliver a step - and - shoot imrt with 5 mm leaf width over the whole treatment volume . the goal of this study was to compare mlc - 5 with traditional mlc - 10 in hnc cases . 
under otherwise same conditions , the improvement of plan quality in step - and - shoot imrt of hnc via integrated boost procedure was analyzed . patients and methods patients a comparison of imrt plans with mlc - 5 over 40 40 cm2 and mlc - 10 was performed on ten patients with hnc undergoing imrt in 2008 . all patients were male ; the mean age was 55 years ( range , 4270 years )  . 
locations of the tumors were the oropharynx ( n = 5 ) , the tongue ( n = 2 ) , the tongue root ( n = 1 ) , the hypopharynx ( n = 1 ) , and the larynx ( n = 1 )  . therapy imrt was the primary treatment in six cases and given as adjuvant treatment after surgery in four other cases . in all cases , the entire cervical lymph drainage and the primary tumor or the postoperative tumor bed were irradiated using an integrated boost procedure . 
in all cases , concurrent chemotherapy was applied [ 12 , 18 ]  . technique the planning system virtuous , an in - house development of the german cancer research center , was used for treatment planning and comparison of the plans [ 4 ]  . 
plan optimization was performed by the inverse treatment - planning program konrad ( siemens )  . both , a linear accelerator with an mlc - 10 ( primus , siemens ; p ) and mlc - 5 over 40 40 cm2 ( artiste , siemens ; a ) were implemented , validated and in daily use . a head mask and a whole - body vacuum cushion were used . 
the boost volume ( ptv1 ) contained the macroscopic primary tumor or the tumor bed and a clinically tumor - free margin of 0.51 c the volume of the cervical lymphatic drainage ( ptv2 ) generally contained the levels iv , except submental lymph nodes . 
 the mean ptv1 was 226.7 cm3 ( range , 79643 cm3 ) , and the mean ptv2 was 1 , 456.1 cm3 ( range , 1 , 0772 , 149 cm3 ) including an additional safety margin of 0.5 cm for positioning error . 
5 - mm mlc in imrt of hnc the ptv coverage complied with the recommendations of the international commission on radiation units [ 5 ]  . the maximum dose for the spinal cord was limited to 40 gy and for the brain stem to 50 gy . 
patient positioning was verified by mv - cone - beam ct or kv - in - room ct [ 15 , 16 ]  . approach to the comparison of plans treatment planning and therapy were performed with 6 - mv photons . 
the mean field length was 22 cm ( range , 2024 cm ) in all ten patients . initially , an optimal mlc - 10 plan with nine isocentric coplanar fields with gantry angles from 0 to 320 in steps of 40 was performed in all cases . 
the optimizer constraint parameters used in the imrt inverse planning system , which were considered optimal for one patient , were kept constant for all further plans of this patient ( see example in figure 1 )  . 
 thus the comparison considered only the influence of the leaf width . the two - dimensional median filter size ( 2d - mfs ) determines how many neighboring beam elements ( bixels ) are taken into account when calculating the median for each bixel position , resulting in a smoother intensity profile . 
both parameters control the number of segments that are created per beam . initially , the same intensity level ( 5 ) and 2d - mfs ( 3 ) were used for the generation of a comparable mlc - 5 plan with nine beams ( a9 ) , leading to an increase of the segment number in all cases . 
to reduce the number of segments in the mlc - 5 plan , alternative plans were generated by changing 2d - mfs and intensity level parameter values : a9 ( 5 / 7 ) corresponding to an mlc - 5 plan with intensity level 5 and 2d - mfs 7 ; a9 ( 4 / 3 ) to an mlc - 5 plan with intensity level 4 and 2d - mfs 3 ; a9 ( 4 / 7 ) to intensity level 4 and 2d - mfs 7 . in addition , one mlc - 5 and mlc - 10 plan with the same constraints and settings ( intensity level 5 and 2d - mfs 3 ) , each with seven isocentric coplanar fields ( 0 , 52 , 103 , 154 , 206 , 257m and 309 ) , were calculated ( a7 and p7 )  . the treatment time is the time for delivery of all subsegments of the plan without the time for rotating the gantry . for each patient and for each plan , normalization of the dose prescription was performed at the median value of ptv1 , corresponding to 100% . for comparison of the plans , the minimum , maximum and mean relative dose in ptv1 and the minimum and mean relative dose in ptv2 have been considered . 
the first character denotes the linac type ( a for artiste with a multileaf collimator with 5 mm leaf width and p for primus with 10 mm ) , followed by the number of beams , the number of intensity levels , and the two - dimensional median filter pixel size ; e.g. , a9 ( 5 / 3 ) stands for the artiste with nine beams , five intensity levels , and a two - dimensional median filter size of 3 . 
das erste symbol steht fr den linac - typ ( a fr artiste mit einem multileafkollimator mit einer lamellenbreite von 5 mm und p fr primus mit 10 mm lamellenbreite ) , gefolgt von der anzahl der bestrahlungsfelder , der anzahl der intensittslevel und der zweidimensionalen medianfiltergre ; z.b. 
 ci was calculated according to ci = v90 / v90 ( treated ) , where v90 ( treated ) is the total volume treated by the 90% dose level . for the oars spinal cord , brain stem and contralateral parotid , the maximum and mean absolute dose resulting from the prescribed total dose were determined . the relative and absolute doses were averaged for all ten patients and all plan types and the standard deviation ( sd ) was determined . 
a paired t - test for the comparison of the plan types was performed with the software sigmaplot ( version 10.0 systat software , usa )  . the actual radiation treatment of the patients was performed with the optimal treatment plan in relation to the individually tolerated treatment time . results segments in general , mlc - 5 ( a ) plans resulted in a higher number of segments than the corresponding mlc - 10 ( p ) plans . 
the number of segments decreased for mlc - 5 and the nine - field plans to 124.8 6 by the reduction of the intensity level value to 4 and the increase of the 2d - mfs value to 7 ( figure 2 )  . ptv1 there were only few significant differences in the mean values of the maximum and minimum relative dose in ptv1 between the different plan groups ( table 1 )  . 
the same applies to seven fields : the plan group a7 ( 5 / 3 ) was significantly superior to group p7 ( 5 / 3 ) ( table 3 )  . the doses to the oars for the mlc - 5 groups were , in general , equal or less compared to the mlc - 10 groups , with p - values for the difference often not reaching statistical significance . 
within the nine - beam group with mlc - 5 , a decrease of up to 25% in the segment number by a reduction of the intensity level ( from 5 to 4 ) and / or increase of 2d - mfs ( from 3 to 5 or 7 ) resulted , in general , in no significantly inferior plan quality . 
a seven - beam imrt with mlc - 5 was inferior to a nine - beam imrt with mlc - 5 in terms of v90 and ci , but superior to a nine - beam imrt with mlc - 10 . our results for the clinically practiced step - and - shoot imrt technique for large volumes in the head and neck area demonstrate that the use of a full - size mlc - 5 ( 40 40 cm2 ) leads to a clear improvement of the dose distribution and of the plan quality compared to a conventional mlc - 10 . it had been shown that intensity levels > 5 can only minimally improve imrt plans [ 6 , 7 ]  . it should be noted that the constraint settings in the inverse planning program were optimized for the 10 - mm plans , and the 5 - mm plans were generated without modification to these settings . 
further tweaking of the constraint settings for the mlc - 5 might have led to even better plans [ 3 ] , however , this was not necessary to demonstrate the clear superiority of the mlc - 5 over the mlc - 10 in terms of plan quality . in a comparison study by topolnjak et al . 
 [ 17 ] with a virtual mlc , it was shown in seven patients that 5 mm leaf width reduced dose in parotid glands compared to 10 mm leaf width strahlenther onkol 2010 nr . 
the upper left panel shows the plan with nine beams and 10 mm leaf width ( p9 ) , the lower left panel the plan for seven beams and 10 - mm leafs ( p7 ) , and the right panels depict the respective plans with 5 mm leaf width ( a9 / a7 )  . 
ptv1 ( red ) , ptv2 ( light red ) , spinal cord ( yellow ) , and right / left parotid glands ( pink / green ) are shown as outlines . 
die mediane dosisverschreibung auf den boost ( = ptv1 ) betrug 70 , 4 gy ( 100% ) und 57 , 6 gy ( 82% ) auf die zervikalen lymphabflusswege ( = ptv2 ) mit einzeldosen von 2 , 2 gy bzw . 
oben links ist der plan mit neun feldern und einer lamellenbreite von 10 mm ( p9 ) , unten links der sieben - felder - plan mit einer lamellenbreite von 10 mm ( p7 ) dargestellt , und rechts sind die entsprechenden plne mit einer lamellenbreite von 5 mm ( a9 / a7 ) zu sehen . 
in that study , different planning systems were used and planning constraints were changed in each plan to reach the planning criteria for ptv ; other plan criteria were not described . in a study applying dynamic imrt ( 120mlc varian ) , fiveash et al . 
 [ 3 ] investigated the influence of 5 mm and 10 mm leaf width in three hnc patients and also found a reduced dose in parotid glands when using 5 mm leaf width . the improved plan quality of mlc - 5 is obtained at the price of a higher segment number : the plan groups a9 ( 5 / 3 ) and a9 ( 4 / 7 ) have an average of 164 and 125 segments , compared to p9 ( 5 / 3 ) with 107 segments . 
however , even with fewer beams and / or intensity levels ( and consecutively fewer segments ) the mlc - 5 is superior to the mlc - 10 [ e.g. , a7 ( 5 / 3 ) with 117 segments is superior to p9 ( 5 / 3 ) ]  . due to the high performance of the new mlc - 5 , the increased number of segments does not cause any significant prolongation of the treatment time . 
the new mlc - 5 can deliver approximately 30% more segments per minute compared to the conventional mlc - 10 . overall , the use of nine or seven beams leads to a qualitatively good dose distribution in a clinically acceptable treatment time . 
neither an increase in number of beams above eleven , nor a leaf width of < 3 mm has been shown to further improve the imrt plan quality [ 9 , 10 ]  . conclusion mlc with a leaf width of 5 mm over a field size of 40 40 cm clearly improves plan quality in step - and - shoot imrt with the integrated boost concept of hnc . 
based on our results , we recommend the use of the mlc - 5 with a nineor seven - field step - and - shoot imrt technique for hnc treatment . strahlentherapie und onkologie original article computed tomography as a source of electron density information for radiation treatment planning witold skrzynski1 , sylwia zielinska - dabrowska2 , marta wachowicz2 , wioletta slusarczyk - kacprzyk1 , pawe f . 
measurement data were compared with the standard hu - el relationships predefined in two commercial treatment - planning systems ( tps )  . results : the hu - el relationships obtained with all of the general - purpose ct scanners operating at voltages close to 120 kv were very similar to each other and close to those predefined in tps . 
for nontypical imaging systems ( e.g. , cbct ) , the relationship can be significantly different and , therefore , it should always be measured and carefully analyzed before using ct data for treatment planning . key words : radiotherapy computed tomography electron density strahlenther onkol 2010 ; 186 : 32733 doi 10.1007 / s00066 - 010 - 2086 - 5 ct - systeme als datenquelle der elektronendichte in bestrahlungsplanungssystemen ziel : vergleich verschiedener computertomographie - ( ct - ) systeme zur bestimmung der elektronendichte ( el ) fr die bestrahlungsplanung . material und methodik : die relation des ct - werts zur elektronendichte wurde an verschiedenen modernen ct - scannern ( single - slice , multislice , wide - bore multislice ) ermittelt , fr die therapiesimulatoren mit einem single - slice - ct und kv - cbct - ( cone - beam - ct - ) optionen sowie fr linearbeschleuniger mit kvund mv - cbct - systemen . 
die messdaten wurden mit den standardumrechnungsformeln zweier marktblicher therapieplanungssysteme ( tps ) verglichen . ergebnisse : die hu - el - relationen , die in allen modernen ct - systemen vorhanden sind , waren untereinander sehr hnlich , ebenso wie zu den vorgegebenen relationen in den tps . 
die ergebnisse des mv - cbct unterschieden sich aufgrund des unterschiedlichen energiespektrums der rntgenstrahlen signifikant von denen der kv - systeme . schlussfolgerung : die im tps vorgegebene hu - el - relation kann bei modernen ct - systemen mit einer rhrenspannung im bereich von 120 kv genutzt werden . 
deshalb sollte bei solchen systemen immer gemessen und sorgfltig analysiert werden , bevor die ct - daten fr die therapieplanung herangezogen werden . schlsselwrter : radiotherapie computertomographie elektronendichte 1medical physics department , center of oncology , warsaw , poland , 2medical physics department , holycross cancer center , kielce , poland . received : september 4 , 2009 ; accepted : march 5 , 2010 published online : may 17 , 2010 strahlenther onkol 2010 nr . 
x - ray computed tomography ( ct ) has been used as a basic source of such data for over 30 years now [ 17 ] , and is used as a base for treatment planning even in less common radiotherapy techniques , such as helical tomotherapy [ 22 ] or radiotherapy with proton beams [ 5 ]  . 
other imaging modalities are sometimes used as an addition to ct , as they may offer better visualization of target volume ( e.g. , magnetic resonance imaging [ 18 ] , positron emission tomography [ 1 ] , or both of them [ 26 ] )  . 
nevertheless , the role of x - ray ct is fundamental , as it provides information on the attenuation of radiation by the patients tissues in a form of ct numbers , expressed in hounsfield units ( hu ) as in the following equation : hutissue = [ ( tissue water ) / water ] 1 , 000 , where is the linear attenuation coefficient of water and of the tissue . 
it is known that precise calculation of dose distribution in radiotherapy can be performed on the basis of knowledge of the electron density of the tissues [ 20 ]  . 
treatment - planning systems ( tps ) usually convert hu values to el ( relative electron density , normalized to water ) by means of the predefined relationship between the two quantities , e.g. , one given by kns et al . 
in some tps the relation is fixed , in others the user is allowed to change it . it should be remembered that hounsfield numbers for a given tissue depend on the quality of the x - ray beam ; therefore , the values can differ between scanners . 
as a result , the dose calculated by tps can change by as much as 2% if ct scans are obtained using 80 kv instead of 130 kv while using the same hu - el relationship [ 7 ]  . 
the hu - el relationships can be measured with the use of phantoms with tissue - equivalent materials [ 3 ] , i.e. , materials that have an atomic composition similar to human tissues [ 8 ]  . 
data obtained with such phantoms for the particular ct scanner operating at a particular kv can then be introduced into the tps to make the calculations more precise . however , different manufacturers of commercial electron density phantoms use different tissue - equivalent materials . 
it is known that solid ( resin - based ) bone - equivalent materials give systematically lower hu values than water solutions of cacl2 of the same electron density [ 24 ]  . 
even for a single ct unit and a single scanning protocol differences of 0.075 in el can be observed depending on the choice of phantom ( all resin - based ) , leading to differences of the calculated dose in the order of 12% [ 6 ]  . hu values observed for a given material also depend on the dimensions of the phantom [ 6 , 9 ] and on the positioning of the phantom , especially the presence and the type of patient support [ 4 ] or location on / off axis [ 9 ]  . 
some uncertainty of el data seems therefore to be unavoidable , especially as patients also differ between themselves in dimensions and in the composition of their tissues . it is suggested that one universal hu - el relationship can be used for all ct scanners operating at typical voltages ( 120 140 kv ) , leading to dose calculation errors not greater than 1% [ 24 ]  . 
these errors are comparable to those caused , e.g. , by use of uncorrected contrast - enhanced ct scans , which leads to change in dose calculation of 1% on average ( 3% maximum ) in the lung [ 2 ] , or of 0.67% on average ( 1.8% maximum ) in the brain [ 28 ]  . 
larger errors in dose calculations can , however , be expected if applying standard predefined hu - el relationships to data obtained with nontypical ct scanners , e.g. , cone - beam ct ( cbct ) systems installed onto radiotherapy linear accelerators or radiotherapy simulators . 
it is known , that such systems are more prone to inaccuracies of hu values than conventional ct systems because of the higher effect of x - ray scatter associated with cone - beam geometry [ 21 ]  . 
 three of them are general - purpose ct scanners and are routinely used as a source of electron density data , the other four are designed as radiotherapy verification tools . 
the systems present a wide range of designs , from single - slice x - ray ct to megavoltage cbct . electron density phantoms of four sizes made by two manufacturers were used in the measurements as listed in table 2 . 
for each phantom , several tissue - equivalent inserts were available , covering a wide range of tissue densities and compositions ( lungs , soft tissues , bones )  . 
6 estro [ 13 ] were adopted , i.e. , it was assumed that the values of el calculated by tps should not differ from the known true values by more than 0.05 for el < 1.5 and by more than 0.1 for el > 1.5. 
the influence of scan parameters ( e.g. , kv ) and of the choice of phantom on the results was also evaluated . results general - purpose ct scanners figure 1 presents results obtained with rmi 465 phantom for three general - purpose x - ray ct scanners operating at various kv settings . 
for el between 0 and 1 ( air , lungs , soft tissues ) , all datasets did not seem to differ , while for el > 1 ( bones ) , the results were dependent on kv setting , and for a given kv , they were different between scanners . for each scanner operating at the most common voltage setting ( 120 kv ) , the dependence of the results on the choice of other parameters was also investigated with rmi 465 . 
the parameters included tube current , slice width , imaging mode ( axial / spiral ) , pitch in spiral mode , position of the inserts within the phantom , and positioning of the phantom in the gantry ( i.e. , on - axis or few centimeters off - axis )  . 
the range of hu values obtained for each material for the ge hispeed unit was generally smaller than 20 hu , only for high - density bones ( el > 1.4 ) it reached 50 hu . 
for both siemens units , larger differences were observed , reaching 5060 hu for lung tissue and 100170 hu for high - density bones . figure 2 presents the dependence of the results obtained for the ge hispeed scanner on the choice of phantom and field of view ( fov ; all the other parameters remaining the same )  . 
bersicht der phantome , an denen die elektronendichte in dieser studie gemessen wurde . phantom dimensions description rmi 465 33 cm ( body ) el phantom , 16 inserts ( 2.8 cm each ) : tissue - equivalent inserts , water , four solid - water rods in various locations ( for uniformity check ) , titanium quality assurance phantom , can simultaneously accommodate up to three inserts from rmi 465 el phantom , eight tissue - equivalent inserts ( 3.05 cm each ) and water 16 cm ( head ) 18 cm ( head ) rmi 463 cirs 062 ( inner section ) cirs 062 ( both sections ) 33 27 cm ( body , elliptic ) el phantom , consists of inner and outer sections , each section with identical set of eight tissue - equivalent inserts tissue - equivalent inserts simultaneously . 
the phantom has some internal structures designed for assessment of image quality , however , they are not located very close to the inserts and they do not cause artifacts in the image . 
when used together , the two sections simulate a patients torso . the relationships measured for different ct units were compared with each other and with default relationships implemented in two commercial tps , namely oncentra masterplan [ 16 ] and varian cadplan [ 27 ]  . 
variabilitt der hu - werte ( hounsfield - einheiten ) fr drei allzweck - computertomographie - ( ct - ) scanner . altered parameter constant parameters range of observed hu values ( maximumminimum ) lung bone soft tissue phantom protocol scanner scanner scanner ct scanner , phantom ct scanner , 120 kv ct scanner , 120 kv , phantom 47 80 kv , phantom 140 kv , phantom 120 kv , phantom 63 23 observed . 
 this can be explained as , for that particular scanner , different beam filtration is automatically chosen for large fov rather than for a small one , resulting in different beam quality . table 3 presents data on the variability of the hu values for three general - purpose ct scanners . 
 die relationen wurden in zwei tps implementiert und zum vergleich dargestellt . inserts placed in different positions of the phantom ranged from 208 hu to + 13 hu ( for general - purpose ct scanners the values would be identical within a few hu )  . kv cbct measurements on two kv cbct systems were performed with cirs 062 phantom ( figure 4 )  . 
for varian obi and inner section of the phantom ( head ) , the results were almost in agreement with the relationships predefined in tps , significant differences were observed only for lung - equivalent materials . 
some dependency on dimension of fov was observed , which could be explained as an effect of differences in acquisition geometry and beam quality for small fov ( 25 cm and smaller ) a full - fan acquisition was used , while for larger fov half - fan geometry and a different bow - tie filter was used . 
hu values for two identical tissue - equivalent inserts simultaneously placed in outer and inner sections of the phantom differed by more than 300 hu . another kv cbct system included in the study was nucletron simulix evolution radiotherapy simulator . 
ct as a source of el information for radiotherapy titanium was 4 , 000 , which is basically the maximum hu value used in that ct unit . discussion table 4 presents maximum differences between real values of el ( as given by the manufacturers of the phantoms ) and el calculated from the measured ct numbers with use of unmodified cadplan calibration curve . 
it should also be noted , that for the same scanners and the same voltages ( but different phantom , or different settings ) the differences were lower than 0.05. 
data measured with electron density phantom can , of course , be used to modify the relationship ( provided that the tps allows it ) , however , some uncertainty of el data will remain as there is no obvious way to eliminate dependencies on size and shape of the phantom ( or patient )  . the results for the radiotherapy simulator were not very different from those obtained for general - purpose ct scanners , however , the information on el was much less precise because of the decidedly worse uniformity of images . 
messergebnisse mit dem cirs - 062 - phantom an zwei kv - cbct - systemen : varian obi ( 125 kv ) und nucletron simulix evolution ( 100 kv )  . 
however , it is known that image quality can be substantially improved by correction of uniformity and by optimization of system settings [ 14 ]  . unfortunately , it was not possible to measure the hu - el relation for each ct scanner for a full range of selectable parameters and with use of all phantoms . 
the results showed that the predefined relationships can be used for those scanners , even if some variability of the results on choice of phantoms was observed for bone - equivalent materials . 
for nontypical ct scanners ( radiotherapy simulators , cbct systems ) , less extensive evaluations were done , in some cases with only one phantom , or with only one set of acquisition parameters . 
nevertheless , this was enough to show that inaccuracies of el values are obviously larger than those observed for general - purpose ct scanners , and that they occur in the whole range of electron densities . conclusion the results obtained for two tps showed that the hu - el relationships predefined in tps can be used for general - purpose ct systems operating at voltages close to 120 kv . 
for nontypical imaging systems ( e.g. , cbct ) , the hu - el relationship can differ significantly from the predefined ones and , therefore , it should be measured and carefully analyzed before using ct data for treatment planning . 
some uncertainty of el data is always unavoidable , as even for general - purpose ct scanners , the hu values for a given tissue can differ depending on the dimensions of the scanned object , either phantom or patient . 
in the latter case , pci was given immediately after the end of thoracic radiotherapy and prior to the last cycles of chemotherapy to a total dose of 30 gy in 2 - gy fractions to the whole brathe results were evaluated with regard to 4 - year rates of overall survival , disease - free survival , and brain metastases - free survival . 
additionally , the prognostic role of pci application and its time delay in relation to survival rates and incidence of brain metastases was estimated . results : the 4 - year survival rates were 25.5% for overall survival , 26.8% for disease - free survival , and 67.8% for brain metastases - free survival . 
during the observation period , 32 patients ( 24.8% ) developed brain metastases , which occured in 20 of 43 patients ( 46.5% ) without and only in twelve out of 86 patients ( 14% ) with pci . 
 early pci is more effective than pci applied after combined therapy . key words : small cell lung cancer prophylactic cranial irradiation radiotherapy brain metastases strahlenther onkol 2010 ; 186 : 3159 doi 10.1007 / s00066 - 010 - 2088 - 3 vergleich der effektivitt von spter und frher prophylaktischer ganzhirnbestrahlung bei patienten mit kleinzelligem bronchialkarzinom im limited - disease - stadium ziel : evaluation der effektivitt einer korrekten zeitlichen planung einer prophylaktischen ganzhirnbestrahlung ( pci ) bei patienten mit kleinzelligem bronchialkarzinom im limited - disease - stadium ( ls - sclc )  . patienten und methodik : zwischen 1995 und 2004 wurden 129 patienten mit ls - sclc in zwei aufeinanderfolgenden phase - ii - studien behandelt , in denen zu unterschiedlichen zeitpunkten eine kombinationstherapie verabreicht wurde . 
86 patienten ( 66 , 7% ) , die eine positive reaktion im thorax entwickelten , wurden einer pci unterzogen , wobei diese in 45 fllen ( 52 , 4% ) nach der radiochemotherapie ( spte pci ) und in den restlichen 41 fllen ( 47 , 7% ) whrend derselben ( frhe pci ) durchgefhrt wurde . 
in letzterem fall wurde die pci unmittelbar nach beendigung der thoraxbestrahlung vor den letzten chemotherapiezyklen in einer gesamtdosis von 30 gy in 2 - gy - fraktionen auf das gesamte gehirn verabreicht . 
zustzlich wurde die prognostische rolle der pci - anwendung und deren zeitlicher verzgerung im hinblick auf berlebensraten und inzidenz von hirnmetastasen bewertet . ergebnisse : die 4 - jahres - berlebensraten betrugen 25 , 5% fr das gesamtberleben , 26 , 8% fr das krankheitsfreie berleben und 67 , 8% fr das hirnmetastasenfreie berleben . 
bei 32 patienten ( 24 , 8% ) traten whrend des beobachtungszeitraums hirnme1breast and chest department , center of oncology maria skodowska - curie memorial institute , krakow , poland , 2clinical biochemistry department , center of oncology maria skodowska - curie memorial institute , krakow , poland . received : october 29 , 2009 ; accepted : march 5 , 2010 published online : may 21 , 2010 strahlenther onkol 2010 nr . 
 die hirnmetastasenfreie 4 - jahres - berlebensrate betrug bei einsatz der pci 81 , 8% gegenber 32 , 2% bei den patienten , die keine pci erhielten ( fr p = 0 , 0000 )  . 
der richtige zeitpunkt der durchfhrung einer pci erwies sich als wichtiger faktor fr die abnahme der inzidenz von hirnmetastasen . schlussfolgerung : eine pci senkt die inzidenz von hirnmetastasen signifikant und verzgert deren entwicklung bei patienten mit ls - sclc . 
patients should be treated with four to six cycles of etoposide - cisplatin , which leads to complete or partial response within the thorax in 7080% of patients , with 4060% of them showing complete response . 
additional thoracic radiotherapy improves the results by increasing complete response rates ( about 1425% ) , extending remission , and prolonging overall survival [ 5 , 11 , 14 , 22 , 2426 ]  . an about 14% reduction of thoracic failure is observed in patients who received combined therapy . 
in several patients , a higher dose was administered , whereas a lower dose was given to patients who had refused to consent to continuation of treatment . in 96 out of 129 patients ( 74.4% ) , complete response in the thorax was observed after treatment . 
the causes of death were development of distant metastases ( n = 81 ) , exacerbation of coexistent diseases ( n = 5 ) second primary cancer ( n = 2 ) , and unknown ( n = 14 )  . the 4 - year survival rates were 25.5% for overall survival , 26.8% for disease - free survival , and 67.8% for brain metastases - free survival . figure 1 depicts the curves of brain metastases - free survival in relation to whether pci was used or not . the analysis showed a statistically significant improvement of results in relation to the rate of brain metastases - free survival . 
in the latter case , pci was given immediately after the end of thoracic radiotherapy and prior to the last cycles of chemotherapy to a total dose of 30 gy in 2 - gy fractions to the whole brain . the results were evaluated with regard to 4 - year rates of overall survival , disease - free survival , and brain metastases - free survival . 
the median time to occurrence of brain metastases was 14.3 months after pci , and 5.2 months in patients in whom this procedure was not performed . the timing of pci appeared to be an important factor in terms of decreasing the incidence of brain metastases . 
additionally , in patients who received pci , brain metastases developed later ( by a factor of 2.5 ) than in patients without pci . results presented by kiricuta & bohndorf showed that pci is capable of reducing the incidence of cerebral metastases and delaying this kind of failure [ 10 ]  . 
they showed that pci not only decreases the incidence of brain metastases ( from 54% to 30% within 2 years after treatment ) but also delays their development [ 9 , 32 ]  . on the other hand , auperin et al . 
in patients who received pci they observed a decrease in the incidence of brain metastases ( 25% gain ) , as well as an improved overall survival ( 5.4% gain ) and disease - free survival ( 8.8% gain ) [ 3 ]  . its application , however , is subject to certain restrictions due to the risk of developing symptoms of neurotoxicity [ 15 , 30 , 32 ]  . the search which aimed to improve the pci efficacy refers to total dose and delay of pci performance in relation to chemoradiotherapy . 
 this dose is considered to be efficient and safe [ 10 , 13 , 20 , 22 , 30 , 34 , 36 ]  . another object of studies in the effectiveness of pci is the time of pci initiation . 
the latter presented a nearly linear dose - response relationship regarding reduction in brain metastases , demonstrated for early pci in the dose range from 0 up to 35 gy . 
additionally , pci applied at the beginning of chemoradiotherapy reduces the incidence of brain metastases by about 80% [ 27 , 28 ]  . in our study , pci was performed in 86 patients , with 41 ( 48% ) receiving early and 45 ( 52% ) late pci . 
early pci is more effective than pci applied after combined therapy . strahlentherapie und onkologie original article volumetric modulated arc therapy for advanced pancreatic cancer wietse eppinga , frank lagerwaard , wilko verbakel , ben slotman , suresh senan1 background : intensity - modulated radiotherapy ( imrt ) allows for improved sparing of organs at risk ( oars ) in advanced pancreatic cancer . 
a planning study evaluated if volumetric modulated arc therapy ( rapidarc [ ra ] ) could be used as an alternative to imrt in such cases . patients and methods : in ten patients , five - field imrt ( 5f - imrt ) plans with fixed gantry positions were compared to ra plans using similar constraints for planning target volume ( ptv ) and oars . 
the delivery time for ra was < 3 min . conclusion : ra planning achieved superior ci for pancreatic tumors compared to 5f - imrt , and modestly reduced oar doses . 
fast treatment delivery using ra may decrease the risk of intrafractional organ motion . key words : pancreatic cancer volumetric modulated arc therapy intensity - modulated radiotherapy planning study organs at risk strahlenther onkol 2010 ; 186 : 3827 doi 10.1007 / s00066 - 010 - 2094 - 5 volumetric modulated arc therapy bei lokal fortgeschrittenem pankreaskarzinom hintergrund : durch intensittsmodulierte radiotherapie ( imrt ) ergibt sich die mglichkeit einer niedrigeren dosisverteilung hinsichtlich der risikoorgane ( oar ) bei patienten mit lokal fortgeschrittenem pankreaskarzinodie vorliegende planungsstudie soll die frage beantworten , ob volumetric modulated arc therapy ( rapidarc [ ra ] ) eine alternative zur imrt sein knnte . patienten und methodik : bei zehn patienten wurden fnf - felder - imrt - plne mit fester gantryposition und ra - plnen bei nahezu identischen beschrnkungen bezglich planungszielvolumen ( ptv ) und oar verglichen . 
dosiskalkulationen erfolgten anhand im wasserphantom gemessener koronaler dosisverteilungen . ergebnisse : ra - plne zeigten einen gnstigeren ci von 1 , 09 0 , 02 ( 1 sd [ standardabweichung ] ) gegenber 1 , 20 0 , 10 bei 5f - imrt ( p = 0 , 003 )  . 
die gesamtbestrahlungszeit betrug < 3 min . schlussfolgerung : mittels ra - planung lsst sich im vergleich zur 5f - imrt sowohl ein gnstigerer ci als auch moderate dosisreduktion in den oar erreichen . 
durch die rasche dosisapplikation vermindert sich das risiko intrafraktionrer bewegung der oar . schlsselwrter : pankreaskarzinom volumetric modulated arc therapy intensittsmodulierte radiotherapie planungsstudie risikoorgane 1department of radiation oncology , vu university medical center , amsterdam , the netherlands . received : october 7 , 2009 ; accepted : february 24 , 2010 published online : june 24 , 2010 strahlenther onkol 2010 no . 
ra for advanced pancreatic cancer introduction in locally advanced pancreatic cancer , primary chemoradiotherapy appears to be superior to best supportive care and high - dose radiotherapy alone [ 14 ]  . 
in selected patients , neoadjuvant treatment can result in downstaging of pancreatic tumors and nodal spread [ 32 ] and adjuvant chemoradiotherapy should be considered after irradical resections [ 20 ]  . 
late toxicity after chemoradiotherapy to the upper abdomen includes bowel strictures [ 16 , 27 ] and radiation - induced nephropathy , which may manifest months to years post - treatment [ 7 , 15 ]  . 
measures to reduce toxicity include omitting prophylactic radiotherapy of regional lymph nodes [ 27 ] , decreasing mobility margins by individualized assessment and incorporation of target mobility [ 33 ] , and the use of more conformal radiotherapy techniques . 
in particular , use of intensity - modulated radiotherapy ( imrt ) is associated with lower renal and bowel doses compared to conventional planning [ 2 , 4 , 23 , 24 , 31 , 34 , 37 ]  . rapidarc ( ra ; varian medical systems , palo alto , ca , usa ) is a volumetric modulated arc technique which allows for rapid planning and delivery of highly conformal intensity - modulated dose distributions using one or two 358 rotations of the gantry of the linear accelerator . 
the planning algorithm uses progressive sampling optimization by simultaneously changing the shape of the treatment aperture , dose rate , and rotation speed of the gantry [ 28 ]  . 
the use of ra has been previously reported for patients with tumors of the head and neck [ 35 ] , multiple brain metastases [ 22 ] , lung cancer [ 36 ] , benign intracranial tumors [ 21 ] , and prostate cancer [ 19 , 29 ]  . in this study , we compared ra planning with conventional five - field imrt ( 5f - imrt ) in ten patients who had undergone chemoradiotherapy for tumors of the pancreas . 
the ability of ra and conventional imrt to reduce doses to the kidneys , the liver , and the small bowel was evaluated . patients and methods a retrospective planning study was performed in ten consecutive patients who had undergone concurrent gemcitabine - based chemoradiotherapy for locally advanced pancreatic carcinoma at our center . 
briefly , clinical target volumes ( ctv ) , consisting of the pancreatic tumor and enlarged regional lymph nodes , were contoured on all phases of a planning four - dimensional computed tomography ( 4dct ) scan that was generated during quiet respiration . 
the interval between the ct phase bins was 1 / 10 of the average breathing cycle time , and the axial slice thickness and reconstruction index was 2.5 mduring 4dct acquisition , no oral or intravenous contrast was administered , because a recently acquired diagnostic contrast - enhanced ct or magnetic resonance imaging scan was available for all patients . 
the planning target volume ( ptv ) was derived from the addition of a margin of 1 cm to the itv in order to correct for variations in respiratory - driven tumor motion and patient setup errors . 
a small - bowel region was defined which consisted of the abdominal content after subtracting the ptv , all oars and the vertebral bodies , with the posterior border extending to the dorsum of the lumbar vertebral body , but excluding the retroperitoneal space [ 30 ]  . 
an earlier planning study had revealed that , for a number of these patients , the present 5f - imrt plans allowed for reduced doses to oars in comparison to the 4f - imrt described previously [ 34 ] ( data not shown )  . planning was primarily optimized for ptv coverage and for limiting each kidney volume receiving 15 gy ( v15 )  . 
doses to the small bowel were not considered in the optimization . ra planning was performed using two simultaneously optimized volumetric arcs ( rapidarc version 8.6.3 , varian medical systems ) as described previously [ 35 ]  . 
similar constraint sets were used for both ra and 5f - imrt plans . dose - volume histograms were analyzed with respect to ptv coverage , conformity indices ( ci ; the ratio between the volume covered by 95% of prescription dose and the ptv ) , and number of monitor units ( mu ) needed to deliver the dose . 
comparisons were performed using paired t - tests in spss v.15.0 , and significance was assumed when p < 0.05. after completion of this planning study , a patient with pancreatic cancer who underwent chemoradiotherapy was treated using ra . 
as is routine for all clinical ra treatments at our center , dosimetric verification of the plan was performed in a solid - water phantom on a trilogy linear accelerator ( varian medical systems ) prior to the start of treatment . 
both mean doses and v30 for all other studied oars , including the liver , stomach , small bowel and duodenum , were significantly lower with ra planning than with 5f - imrt ( table 3 , figure 2 )  . 
average dose - volume histograms ( dvh ) for the right and left kidney of ten patients , achieved with ra ( solid line ) and 5f - imrt ( dashed line )  . 
dosis - volumen - histogramme ( dvh ; kumulierter durchschnitt ) der rechten und linken niere von zehn patienten fr ra ( durchgezogene linie ) und 5f - imrt ( gestrichelte linie )  . 
the beam - on time ( after the completion of patient setup ) for each fraction was < 3 min for ra , compared to 8 min for 5f - imrt . discussion several publications on pancreatic cancer have demonstrated the superiority of imrt in reducing radiation doses to surrounding normal organs in comparison to three - dimensional conformal radiotherapy [ 2 , 4 , 23 , 24 , 34 ]  . 
average dose - volume histograms ( dvh ) for the bowel , liver , and stomach , achieved with ra ( solid line ) and 5f - imrt ( dashed line )  . 
dosis - volumen - histogramme ( dvh ; kumulierter durchschnitt ) des darms , der leber und des magens von zehn patienten fr ra ( durchgezogene linie ) und 5f - imrt ( gestrichelte linie )  . 
ra has now been clinically implemented , with the delivery of each fraction requiring < 3 min . the ptv encompassing the most common locations for nodal metastases , which are the peripancreatic and pancreaticoduodenal areas . the main goal of our study was to investigate whether the increased speed in treatment planning and delivery obtained with ra would compromise the conformity and normal - organ sparing compared to conventional imrt . 
our study as well as recent publications in a range of tumor sites [ 9 , 19 , 21 , 22 , 29 , 35 , 36 ] have clearly shown data to the contrary . 
we realize that it may be difficult to draw firm conclusions on the comparison between ra and imrt because of differences in optimization methods , and the use of more than five imrt fields may change the comparison . when considering dosimetric differences between ra and imrt , it is also important to address motion management for abdominal tumors , as craniocaudal pancreatic motion of up to 25 mm has been reported [ 6 , 12 ]  . 
mean pancreatic motion on 4dct of our patients was only 9 mm , however , with extremes of up to 15 minadequate margins for motion may lead to significant underdosing , in particular when highly conformal treatment techniques are used . 
the former approaches can substantially prolong delivery times , which can increase the risk of tumor displacement during treatment delivery , particularly as surrogate markers such as abdominal wall and diaphragm poorly correlate with tumor mobility [ 12 ]  . 
earlier reports suggest that respiration - gated imrt ( or carbon ion therapy ) leads to only very limited dosimetric benefits for upper abdominal tumor sites [ 25 , 33 , 34 ]  . 
in addition , a combination of respiratory gating with arc therapy is technically not possible in the current version of ra . the observed dosimetric benefit of ra over 5f - imrt was reflected in a lower ci of ra plans and significant reduction in the v20 of the right kidney . 
our data show a superiority of ra for all doses > 15 gy ( figure 2 )  . our protocol calls for omission of prophylactic regional node irradiation , and only enlarged nodes were encompassed in the ctv . 
other groups have considered elective nodal irradiation to be appropriate due to a high likelihood of lymph node involvement in approximately 7580% of patients who underwent surgical resection for pancreatic tumors [ 5 , 18 ]  . 
nevertheless , our approach results in ra treatment delivery time was < 3 min in our patient , and this compares favorably with 5f - imrt delivery which takes approximately 10 min on a varian linear accelerator . 
 besides improving patient comfort and departmental efficiency , the reduced treatment delivery will also decrease the likelihood of intrafractional changes in patient position [ 13 ]  . conclusion ra planning for advanced pancreatic cancer results in significantly higher conformity plans than can be achieved using 5f - imrt , which allows for increased sparing of most surrounding oars . 
based on these results and the increased speed of planning and treatment delivery , we have adopted ra as our standard treatment modality for patients with advanced pancreatic cancer . strahlentherapie und onkologie review article osteonecrosis of the jaws clinicopathologic and radiologic characteristics , preventive and therapeutic strategies vassilios vassiliou1 , nikolaos tselis2 , dimitrios kardamakis3 background : bisphosphonate ( bp ) use has increased dramatically in recent years , becoming an integral part of the overall antineoplastic management of patients with metastatic bone disease . 
even though their application has shown to be effective in reducing pain and minimizing the risk of skeletal - related events , their administration may bring also adverse events such osteonecrosis of the jaws ( onj )  . methods : after a thorough review of the literature , important aspects of the pathophysiology , diagnosis , prevention , and treatment of onj are presented . results : onj is evident in up to 10% of patients receiving intravenous bp treatment . 
in the event of onj , stage i or ii should be managed conservatively , whereas more advanced stages ( iii and iv ) should be treated surgically . conclusion : onj is a well - defined clinical entity that all medical and dental doctors should be aware of , since if it is not dealt with readily and effectively , it may deteriorate the clinical status and quality of life of affected patients . key words : osteonecrosis of the jaws bisphosphonates imaging radiotherapy surgery strahlenther onkol 2010 ; 186 : 36773 doi 10.1007 / s00066 - 010 - 2066 - 9 osteonekrosen des kiefers . 
ihr erfolgreicher einsatz in der schmerzreduktion ossrer lsionen sowie der prvention skelettaler komplikationen steht jedoch auch in assoziation zu osteonekrosen des kiefers ( onj [ osteonecrosis of the jaw ] )  . methodik : in einem bersichtsartikel werden die relevanten aspekte der pathophysiologie , diagnostik , prvention und behandlung von onj erlutert . ergebnisse : tiologie und pathogenese sind nicht hinreichend geklrt , und onj unter bisphosphonatbehandlung knnen entweder spontan oder nach zahnextraktion bzw . 
die behandlung von onj sollte in den stadien i und ii konservativ , in den hhergradigen stadien ( iii und iv ) operativ erfolgen . schlussfolgerung : onj stellen eine schwerwiegende komplikation mit dem risiko einer deutlichen einschrnkung der lebensqualitt dar . 
eine engmaschige patientennachsorge ist fr eine frhzeitige und effektive behandlung von elementarer bedeutung . schlsselwrter : osteonekrosen des kiefers bisphosphonate bildgebung radiotherapie chirurgie 1department of radiation oncology , bank of cyprus oncology centre , nicosia , cyprus , 2department of radiation oncology , klinikum offenbach , germany , 3department of radiotherapy , university of patras medical school , greece . received : july 16 , 2009 ; accepted : october 26 , 2009 published online : april 26 , 2010 strahlenther onkol 2010 no . 
osteonecrosis of the jaws introduction the clinical use of bisphosphonates ( bps ) in patients with metastatic bone disease and multiple myeloma has increased dramatically in recent years , becoming an integral part of their overall therapeutic management [ 1 , 14 , 30 , 55 ]  . 
through clinical trials bps have proven to be effective both in reducing metastatic bone pain [ 7 , 8 , 24 , 26 ] and in significantly decreasing the risk of potential skeletal - related events ( pathologic fracture , hypercalcemia of malignancy , radiation or surgery to bone , spinal cord or nerve root compression ) [ 2 , 9 , 12 , 26 , 39 , 46 ]  . 
furthermore , bps have shown to improve the quality of life [ 37 , 50 ] of affected patients [ 7 , 17 , 18 ] and retard the progression of metastatic bone disease [ 3 , 29 , 41 , 48 ]  . bps have a selective activity on osteoclasts , bringing about a decrease in their activity and viability [ 54 ]  . 
moreover , their use is associated with potential adverse events such as a flu - like syndrome ( bone pain , pyrexia ) , hypocalcemia and osteonecrosis of the jaws ( onj )  . 
in view of the relatively high incidence and severity of onj , all medical and dental practitioners should be aware of the associated clinical and radiologic features , so that onj is diagnosed early and managed readily . 
 additionally , all indicated preventive measures should be followed as closely as possible and patients should be followed up and evaluated thoroughly both before and during treatment with bps . in the current review , we discuss in detail the mode of action of bps in relation to their chemical structure , the pathophysiology of onj and associated risk factors , the clinical and radiologic features of onj , and , finally , both preventive and therapeutic strategies . 
 the first - generation compounds ( clodronate and etidronate ) have a weak antiresorptive activity as a result of the simple constituents of the central carbon atom ( figure 1c ) [ 45 ]  . 
the most potent bps are those of the third generation , containing either a tertiary amine in their ring structure ( zoledronate , figure 1e ) , or a nitrogen atom in a pyridyl ring ( risedronate )  . 
the potency among the three generations differs significantly with the relative potency between clodronate , ibandronate and zoledronate being 1 : 857 : 16 , 700 , respectively [ 25 ]  . 
table 1 presents the characteristics of the most commonly used bps . bps bind avidly to mineralized bone matrix , concentrating selectively on bone resorption surfaces where bone mineral exposure is high [ 33 ]  . 
the inhibition of these enzymes causes the loss of prenylated proteins that are essential for the posttranslation of lipid modification of small guanine triphosphates such as ras , rho , and rac [ 23 ]  . 
these proteins play a key role in the regulation of important osteoclast cellular functions such as membrane ruffling , endosomal control , cellular structure and morphology , intracellular signaling , and function of the proton atpase [ 28 ]  . bisphosphonates before discussing the pathophysiology of onj , one should have a thorough understanding of the mode of action of bps . 
 their structure is similar to pyrophosphates that have a p - o - p configuration ( figure 1a ) , and in the typical bp composition the central carbon atom replaces the oxygen , enabling the accommodation of two side chains , r1 and r2 ( figure 1b )  . 
charakteristika der am hufigsten rezeptierten bisphosphonate ( bps )  . bp relative potencya dose per administration ( mg ) frequency of administration route of administration vassiliou v , et al . 
osteonecrosis of the jaws first - generation bps clodronate second - generation bps pamidronate ibandronate third - generation bps zoledronate 20 857 16 , 700 adata acquired from green et al . 
 [ 25 ] 1 , 600 6 4 osteonecrosis of the jaws definition and pathophysiology osteonecrosis that is associated with bp use was reported to affect only the upper and lower jaw bones ( mandible and maxilla ) , and to date , only one patient was shown to develop osteonecrosis of the auditory canal after receiving bp treatment [ 40 ]  . 
the exact pathophysiology of onj is not known , however , bp - associated onj is defined as an unexpected appearance of exposed necrotic bone in the maxillofacial area of patients who receive bps and have not been irradiated [ 26 ]  . 
 onj occurs either spontaneously , with the absence of healing after a period of 6 weeks , or in association with dental surgery or tooth extraction [ 57 , 58 ]  . the jawbones are under a process of active and constant remodeling due to the microfractures and bone damage , which are a result of mastication , swallowing and speech . 
it has been suggested that both the lack of bone resorption and remodeling and the diminished surface of bone formation play a key role for the development of onj [ 27 , 38 , 51 ]  . 
moreover , it has also been suggested that prolonged bp use results in an accumulation of bps in alveolar bone , and upon dental extraction or other surgical manipulation , the local release of accumulated bps results in toxicity of the overlying epithelium and impaired healing [ 43 ]  . 
an in vitro study that reonce daily oral once in 34 weeks once in 34 weeks once daily intravenous intravenous oral once in 34 weeks intravenous inforces this postulation is that by landesberg et al . 
who showed that pamidronate brings about a dose - dependent inhibition of keratinocytes in culture [ 31 ]  . risk factors by reviewing the literature , several risk factors that are associated with the development of onj were identified . 
such factors include the length of bp exposure , traumatic dental procedures , the use of poorly fitting dentures , female gender , advanced age , low hemoglobin levels , coagulopathy , excessive alcohol or tobacco use , treatment with chemotherapy , periodontal disease and immunosuppressed states , as in the case of corticosteroid use [ 5 , 16 , 20 , 27 , 34 , 49 ]  . 
additionally , the type of bp seems to affect the development of onj , since patients managed with zoledronate or pamidronate were found to have a higher risk as compared to those receiving ibandronate [ 5 ]  . 
table 2 presents risk factors that have been associated with onj development . clinical features and staging the typical findings at clinical oral cavity examination are an exposed necrotic alveolar bone ridge , accompanied in most cases with a foul - smelling discharge . 
bps : bisphosphonate ; ctx : chemotherapie . local factors traumatic dental procedures exostoses and tori periodontal disease poor oral cavity hygiene dental infections poorly fitting dentures systemic conditions treatment with bps or ctx female gender advanced age low hemoglobin levels or coagulopathy corticosteroid use or immunosuppressed states excess alcohol or tobacco use strahlenther onkol 2010 no . 
the differential diagnosis of onj includes conditions such as periodontal disease , osteomyelitis , gingivitis , sinusitis , neuralgia associated with cavitational osteonecrosis and primary tumor of bone or metastasis . 
radiation therapy of the head - neck region [ 10 , 11 , 42 ] can also bring about bone necrosis ( osteoradionecrosis ) , the characteristic of which is the presence of a hypoxic - hypercellular tissue that fails to heal [ 26 ]  . a useful clinical staging was proposed by methora & ruggiero in an attempt to standardize the management of onj according to stage [ 34 ]  . 
finally , stage iii disease is defined as exposed bone complicated with pathologic fracture and soft - tissue infection that cannot be managed with antibiotics [ 34 ]  . radiologic and scintigraphic evaluation radiologically , onj can only be detected in already advanced cases and the presence of exposed necrotic bone . 
dental panoramic radiography is recommended for routine dental assessment of patients who are at risk of developing onj or have already done so [ 32 ] , since it can readily detect osteolytic lesions with cortical bone involvement . 
computed tomography ( ct ) provides a more detailed imaging of the affected anatomic area , being especially helpful for the differential diagnosis between onj and metastatic bone disease [ 6 ]  . 
in onj cases where an increased radionuclide uptake is demonstrated in the mandible or maxilla , ct imaging depicts an extensive periosteal bone reaction with soft - tissue edema , whereas in the case of metastatic disease , no periosteal reaction is evident [ 52 , 53 ]  . 
figures 2 and 3 present the orthopantomogram and ct images of a patient with bp - associated mandibular onj . bone scintigraphy is the most sensitive imaging modality for the detection of onj at an early stage . 
interestingly , it has been shown that scintigraphic evaluation with technetium - 99m - methylene diphosphate was superior to both ct and magnetic resonance imaging ( mri ) for establishing the diagnosis of onj [ 13 ]  . 
figure 4 depicts the scintigraphic findings in a patient with onj . prevention and therapeutic management the overall evaluation , management and follow - up of patients who are on bp treatment or those who have developed onj , should be done by an expert dental professional . 
orthopantomogramm mit lytischer destruktionszone im bereich der zahnextraktionshhle an der linksseitigen mandibula ( skizziertes areal )  . tive measures are recommended prior to , during and after the onset of therapy [ 32 , 34 , 35 ]  . before the onset of treatment with bps , all patients should undergo a thorough dental examination and preventive dentistry , which should aim at the best possible state of oral and dental health . 
the initial evaluation should include periodontal treatment , extraction of teeth with a negative prognosis with respect to restorative needs or periodontal condition , caries control , and instructions should be given for good oral hygiene practices at home . 
apart from the intraand extraoral assessment , whenever available , patients should be advised to undergo baseline periapical and panoramic radiographs [ 35 ]  . once patients start bp treatment , maintenance hygiene appointments are recommended every 36 months . 
however , when extraction cannot be avoided ( as in the case of persistent infection after conservative treatment , or in the case that root canal treatment cannot be performed ) , the use of antibiotics such as penicillin v - k or clindamycin for a few weeks can decrease the risk of local complications [ 32 , 35 , 58 ]  . in the event of onj , treatment should aim for the elimination of infection by the use of antibiotics , debridement of necrotic bone tissue , and maintenance of a good oral hygiene with frequent antimicrobial rinses . 
moreover , the application of hyperbaric oxygen therapy and the neodymium - doped yttrium aluminum garnet ( nd : yag ) laser have been reported as effective alternatives for the management of onj [ 22 , 56 ]  . another issue that needs to be discussed is the usefulness of discontinuing bp treatment after the development of onj . 
migliorati has recently suggested to continue bp use in patients for whom the control of metastatic bone disease and hypercalcemia is important , and to withhold treatment in case that bps are used prophylactically until disease reactivation is diagnosed [ 35 ]  . conclusion and future perspectives onj is a potentially severe complication that may develop in patients receiving bp treatment . 
all medical and dental practitioners , but especially oncologists , should be aware of this condition , including its pathophysiology , associated risk factors , clinical and radiologic characteristics , and indicated preventive and therapeutic measures . 
the extensive use of bps in oncologic patients makes this necessity even more imperative . even though several risk factors and mechanisms have been suggested for the development of onj , no definite conclusion has been reached yet . 
knochenszintigramm mit erhhter radioisotopaufnahme im bereich der linksseitigen mandibula ( pfeil )  . superior bone penetration and a wider spectrum of bacterial coverage , antibiotics for anaerobic bacteria such as metronidazole may be used in cases resistant to treatment . 
migliorati for their critical comments . strahlentherapie und onkologie review article combined - modality treatment for anal cancer current strategies and future directions ingeborg fraunholz , daniela rabeneck , christian wei , claus rdel1 background : concurrent chemoradiotherapy ( crt ) with 5 - fluorouracil ( 5 - fu ) and mitomycin c ( mmc ) is the treatment of choice for anal carcinoma . 
the most appropriate radiation ( rt ) dose , fractionation , techniques , and the most effective chemotherapy regimen ( agents , number of neoadjuvant , concomitant , adjuvant cycles ) remain to be established . material and methods : this review article focuses on recent randomized trials designed to improve standard 5 - fu / mmc - based crt through the inclusion of ( induction , concurrent , maintenance ) cisplatin , and describes developments in combining rt with other chemotherapeutic drugs and targeted therapies . 
current phase i / ii studies are evaluating the use of capecitabine , oxalipatin , and the egfr ( epidermal growth factor receptor ) inhibitor cetuximab . conclusion : concurrent 5 - fu / mmc - crt without induction or maintenance chemotherapy remains the standard of care for anal cancer patients . key words : anal cancer chemoradiotherapy induction chemotherapy maintenance chemotherapy cisplatin strahlenther onkol 2010 ; 186 : 3616 doi 10.1007 / s00066 - 010 - 2162 - x kombinationstherapie des analkarzinoms . 
derzeitige strategien und zuknftige entwicklungen hintergrund : die simultane radiochemotherapie ( rct ) mit 5 - fluorouracil ( 5 - fu ) und mitomycin c ( mmc ) ist die standardbehandlung des analkarzinoms . 
die adquate dosis der radiotherapie ( rt ) , deren fraktionierung und technik sowie das effektivste chemotherapieregime ( substanzen , zahl der neoadjuvanten , simultanen und adjuvanten zyklen ) mssen noch etabliert werden . material und methodik : dieser bersichtsartikel beschreibt die aktuellen randomisierten studien , deren ziel es war , die standard - rct mit 5 - fu / mmc durch hinzunahme von cisplatin ( als induktionstherapie , simultane oder adjuvante chemotherapie ) zu verbessern , sowie die kombination der rt mit anderen chemotherapeutischen substanzen und zielgerichteten therapien . 
aktuelle phase - i / ii - studien testen den einsatz von capecitabin , oxaliplatin und dem egfr - inhibitor ( epidermaler wachstumsfaktor - rezeptor ) cetuximab . schlussfolgerung : die simultane rct mit 5 - fu / mmc ohne induktionsoder erhaltungschemotherapie bleibt die standardbehandlung fr patienten mit analkarzinom . schlsselwrter : analkarzinom radiochemotherapie induktionschemotherapie erhaltungschemotherapie cisplatin 1department of radiation oncology , j.w. 
goethe university , frankfurt / main , germany . received : april 16 , 2010 ; accepted : april 27 , 2010 published online : june 24 , 2010 strahlenther onkol 2010 no . 
combined - modality therapy is now the mainstay of a curative approach , with surgery reserved as salvage for nonresponders or recurrent disease [ 1 , 4 , 10 , 11 ]  . 
before the 1980s , radical surgery with abdominoperineal resection was the most frequently recommended treatment , as early results obtained with radiotherapy ( rt ) alone varied considerably with respect to oncologic results , and rt - related complications were considered unacceptable . 
the earliest report on concomitant crt for anal cancer with modest doses of rt ( 30 gy / 15 fractions ) administered concomitantly with continuous infusion 5 - fluorouracil ( 5 - fu ; 1 g / m2 d14 , 2831 ) and mitomycin c ( mmc ) bolus injection ( 1015 mg / m2 d1 ) was by nigro et al . 
however , it soon became doubtful whether radical surgery was necessary , because the majority of resected specimens were completely free of tumor on pathologic examination . since then , several series and prospective trials have demonstrated the feasibility and efficacy of this approach , however , the most appropriate rt dose , fractionation , techniques , and the most effective chemotherapy regimen ( agents , number of neoadjuvant , concomitant , adjuvant cycles ) remain to be established [ 2 , 5 , 8 , 13 , 19 , 21 , 27 , 29 ]  . 
new imaging and radiation techniques , such as intensity - modulated rt for anal carcinoma , are beyond the scope of this article [ 17 ]  . role of rt combined with 5 - fu / mmc versus rt or 5 - fu - rt alone two european phase iii trials compared combined crt with rt alone ( table 1 )  . 
the eortc trial required a locally advanced tumor ( t34 or t1 / 2 n + ) , whereas the ukcccr trial included patients with any stage of disease [ 4 , 10 ]  . 
although no overall survival benefit was observed , both studies revealed increased tumor regression and a significantly improved local control rate with combined - modality treatment using continuous infusion 5 - fu and bolus mmc . 
 this was confirmed by the recently published late follow - up data of the ukcccr trial [ 24 ]  . the intergroup study ( ecog / rtog ) examined the importance of mmc in the standard regimen [ 11 ]  . 
as shown in table 1 , the addition of mmc to 5 - fu significantly reduced local failure rates and improved colostomy - free and disease - free survival rates compared with 5 - fu - based crt alone . 
cis : cisplatin ; cr : complete response ; crt : concurrent chemoradiation therapy ; 5 - fu : 5 - fluorouracil ; fx : fractions ; mmc : mitomycin c ; pr : partial response ; rt : radiotherapy . 
cis : cisplatin ; cr : komplettes ansprechen ; crt : simultane radiochemotherapie ; 5 - fu : 5 - fluorouracil ; fx : fraktionen ; mmc : mitomycin c ; pr : partielles ansprechen ; rt : radiotherapie . 
a total of 682 patients with t24 nx m0 anal cancer were randomized to receive either rt with standard concurrent 5 - fu and mmc in the 1st and 5th week , or two cycles of induction chemotherapy 5 - fu and cisplatin , followed by rt with concurrent 5 - fu and cisplatin in the 1st and 5th week ( figure 1a )  . 
rather than concluding that cisplatin is inferior to mmc , the results of rtog 98 - 11 suggest that the concept of induction chemotherapy is inferior to concurrent crt alone . 
preliminary analysis also showed no significant differences in recurrence - free ( hazard ratio 0.89 , 95% confidence interval 0.681.18 ; p = 0.42 ) and overall survival rates ( hazard ratio 0.79 , 95% confidence interval 0.561.12 ; p = 0.19 ) with or without maintenance chemotherapy . 
thus , it was again concluded , that 5 - fu / mmc - crt without maintenance chemotherapy remains standard of care for anal carcinoma . the third phase iii randomized trial ( accord 03 ) was a four - arm study comparing induction chemotherapy with 5 - fu / cisplatin with immediate 5 - fu / cisplatin - crt and moderateto high - dose rt in 307 patients with locally advanced figures 1a to 1d . 
a one - stage fleming design was applied with the aim to exclude a response rate < 75% ( one - sided type i error 10% , 90% power , 40 patients needed in each arm )  . 
 with respect to treatment compliance , 79.5% in the 5 - fu / mmc - crt arm , but only 48.6% in the cisplatin / mmc - crt arm ( p = 0.005 ) were fully compliant ( defined as drug dose intensity > 80% , > 54 gy , < 67 days overall treatment time )  . 
the objective response rate was 79.5% ( 31 / 39 patients ) with 5 - fu / mmc - crt , and 91.9% ( 34 / 37 patients ) with cisplatin / mmc - crt . 
with a median follow - up of 2 years , the 1 - year progression - free survival was 76.3% in the 5 - fu / mmc - crt arm , and 94.2% in the cisplatin / mmc - crt ar the authors highlight the promising response rate of cisplatin / mmc - crt , but also acknowledge that , given the limited compliance , this schedule might be difficult to take into phase iii testing . 
 role of other chemotherapeutic drugs other potential chemotherapy regimen , apart from 5 - fu , mmc and cisplatin , have not yet been extensively tested for anal cancer treatment . 
a multicenter phase ii study from the uk demonstrated the feasibility and moderate toxicity of an oral regimen of capecitabine ( 825 mg / m2 bid , monday through friday ) plus intravenous mmc ( 12 mg / m2 d1 ) , a phase iii study was recommended [ 12 ]  . 
anderson cancer cen ter investigated the combination of capecitabine ( 825 mg / m2 bid , monday through friday ) and oxaliplatin ( 50 mg / m2 weekly ) with rt ( 45 gy for t1 , 55 gy for t2 , and 59 gy for t3t4 lesions )  . 
squamous cell carcinoma in other tumor sites strongly expresses the epidermal growth factor receptor ( egfr ) , and egfr overexpression has consistently been demonstrated as negative prognostic factor [ 18 , 28 ]  . 
only few studies have been performed for anal cancer , but these studies indicate that egfr is overexpressed in the majority of cases ( figure 2 ) [ 3 , 15 , 16 , 30 , 31 ]  . 
complete control rates at 2 months ranged between 74% and 86% , actuarial 3 - year local control between 80% and 97% , and cancer - specific survival between 79% and 89% , with no significant differences for all endpoints between the four arms . 
 thus , given the results of all three randomized phase iii trials , neither induction chemotherapy or maintenance chemotherapy with 5 - fu / cisplatin nor rt dose escalation improved the outcome of concurrent crt in anal carcinoma . to investigate the combination of mmc plus cisplatin and rt , the eortc piloted a phase ii study , which demonstrated favorable results regarding acute toxicity and yielded a complete response rate of 91% [ 7 ]  . 
based on this promising data , a randomized phase ii trial ( eortc 22011 - 40014 ) was launched to compare concurrent 5 - fu / mmc - crt with concurrent cisplatin / mmc - crt for patients with locally advanced anal cancer ( t2 > 4 cm to t4 n + m0 ) ( figure 1d ) [ 20 ]  . 
treatment for anal cancer with metastatic anal cancer showed promising response rates using cetuximab monotherapy or cetuximab / irinotecan combination therapy [ 16 , 26 ]  . a phase i study of cetuximab in combination with 5 - fu , cisplatin and rt for locally advanced anal cancer has recently been reported ( figure 3 ) [ 25 ]  . 
cetuximab combined with cisplatin / 5 - fu - crt is currently evaluated in phase ii anal cancer trials by the eastern cooperative oncology group ( nct00316888 ) , the fdration nationale des centres de lutte contre le cancer ( nct00955240 ) , and the aids associated malignancies clinical trials consortium ( nct00324415 )  . 
 strahlentherapie und onkologie originalarbeit automatisierte leistungsbermittlung in der strahlenheilkunde michael sauer1 , steffen volz2 , markus hall3 , fred rhner3 , hermann frommhold3 , anca - ligia grosu3 , felix heinemann3 hintergrund und ziel : fr die erzielung von erlsen muss im bereich der strahlentherapie jede teilbestrahlung ( fraktion ) verschlsselt werden , und zwar unter angabe von datum und uhrzeit der jeweiligen manahme . 
bei im schnitt 30 fraktionen pro patient und 2 500 neuen patienten im jahr wchst das verschlsselungsvolumen allein im bereich der bestrahlungsnahen therapieschlssel schnell auf werte von 70 000 und mehr . 
das hier vorgestellte verfahren ist ein gemeinschaftsprojekt der klinik fr strahlenheilkunde , der klinikumsverwaltung und des klinikrechenzentrums ( krz ) des universittsklinikums freiburg . material und methodik : das hier beschriebene projekt besteht aus einzelnen modulen , welche im zusammenspiel die angestrebte automatisierung hinsichtlich der bermittlung von beschleunigernahen leistungen ermglichen . 
im weiteren verlauf spielt dabei eine matchingtabelle eine zentrale rolle , da sie es ermglicht , die einzelnen leistungen kostentrgerabhngig in die gltigen abrechnungsschlssel ( wie go , ebm oder ops ) zu berfhren . 
im letzten schritt werden diese daten dann an das abrechnungssystem bertragen . ergebnisse und schlussfolgerung : nach einer erfolgreichen umsetzung und implementierung der einzelnen module wurde im mrz 2006 ein erster betatest vorgenommen , um die prinzipielle lauffhigkeit und das zusammenspiel der einzelnen komponenten zu berprfen . 
this is a joint project of the department of radiotherapy , the administration department , and the central it department of the university hospital of freiburg . material and methods : the project consists of several modules whose collaboration makes the projected automated transfer of treatment codes possible . 
bei im schnitt 30 fraktionen pro patient und 2 500 neuen patienten im jahr wchst das verschlsselungsvolumen allein im bereich der bestrahlungsnahen therapieschlssel schnell auf werte von 70 000 und mehr . 
vor diesem hintergrund wurde in der klinik fr strahlenheilkunde freiburg ein verfahren entwickelt und implementiert , welches die bermittlung und die verarbeitung dieser therapieschlssel automatisiert . teilung in sinnvolle gruppen findet ( abbildung 1 ) [ 8 ]  . 
der benutzer ( meist mtra ) whlt dabei leistungen manuell im scheduling - modul des abteilungssystems ausschlielich ber diese klartextlisten aus , der zustzlich hinterlegte interne code ( leitziffer ) ist fr ihn weder relevant noch sichtbar . 
durch den einsatz interner ( eigener ) leitziffern knnen auch spezielle behandlungstechniken wie imrt ( intensittsmodulierte radiotherapie ) [ 1 , 17 , 23 ] und rapidarc / vmat ( volumetric modulated arc therapy ) so abgebildet werden , dass sie je nach erlaubter abrechnungsmodalitt ( krankenkasse , ambulant , stationr und privat ) bercksichtigung finden . 
eine generelle arbeitsanweisung das hier vorgestellte verfahren ist ein gemeinschaftsprojekt der klinik fr strahlenheilkunde , der klinikumsverwaltung und des klinikrechenzentrums ( krz )  . material und methode um leistungsdaten prozedural extrahieren zu knnen , mssen diese digital zur verfgung stehen , und zwar in gltiger und , wenn mglich , lckenloser forfr die dokumentation von strahlentherapeutischen behandlungen gibt es umfangreiche gesetzliche anforderungen , denen entsprochen werden muss [ 6 , 16 , 20 , 22 ]  . 
in der klinik fr strahlenheilkunde wird im abteilungssystem mosaiq fr jede mgliche leistung ein schlssel mit dazugehriger , semantisch geschickt gewhlter bedeutungsphrase vorgehalten , wobei sich hier zustzlich noch eine unterstrahlenther onkol 2010 no . 
automatisierte leistungsbermittlung in der strahlenheilkunde fr alle personen , die an der leistungserbringung beteiligt sind , besteht darin , dass alle erbrachten leistungen dokumentiert werden mssen , und zwar unabhngig davon , ob diese leistungen abrechnungsfhig sind oder nicht [ 2 , 14 ]  . auf dieser datenbasis baut das im folgenden beschriebene verfahren auf . das projekt besteht aus einzelnen softwaremodulen , welche im zusammenspiel die angestrebte automatisierung hinsichtlich der bermittlung von beschleunigernahen leistungen ermglichen . das erste modul extrahiert die erbrachten leistungsdaten aus unserem abteilungssystem ( mosaiq ) ; dabei werden nur leistungen extrahiert , die als erbracht markiert sind ( charged - flag )  . 
data structure of the automated delivery of codes for charge . feldtyp numeric character character date numeric date time numeric date time feldname beschreibung patid patname patvorname patgebdat lekostst ledate letime lecode uedate uetime patientenidentifikationsnummer patientenname patientenvorname patientengeburtsdatum kostenstelle des leistungserbringers datum der leistung zeitpunkt der leistung leistungscode datum der leistungsbermittlung zeitpunkt der leistungsbermittlung entsprechenden gesetzlichen schlsselwerken ( ops , go , ebm ) [ 7 , 9 , 24 , 25 ] anwendung , sondern es werden eigens hierfr erstellte interne leistungscodes ( leitziffern ) benutzt . mit einem zweiten modul werden im darauffolgenden schritt die leistungsdaten tglich ( nachts ) ber ein proprietres format , welches mit dem krz abgesprochen wurde , via ftp an das krz bermittelt ; die daten in hl7 - messages umzuwandeln und ber eine hl7 - schnittstelle [ 5 , 10 , 12 , 13 , 18 , 19 , 26 ] an das krz zu bermitteln , wre eine leicht zu implementierende alternative . 
dieser schritt stellt sicher , dass jede leistung eindeutig dem fr die leistung gltigen kostentrger zugeordnet werden kann , selbst wenn der patient whrend seiner aktuellen behandlung die krankenkasse gewechselt hat ; fr jeden leistungstrger ist bekannt , nach welchen schlsselwerken und fr welche leistungen eine abrechnung erfolgen darf . 
in diesem zusammenhang und im weiteren verlauf kommt eine ausgeklgelte matchingtabelle ins spiel ; sie ermglicht es , dass die einzelnen leistungen , kostentrgerabhngig , in die jeweils gltigen abrechnungsschlssel ( wie go , ebm oder ops ) berfhrt werden knnen ( tabelle 2 )  . 
scheme of the automated delivery of codes for charge . ergebnisse und diskussion nach einer erfolgreichen umsetzung und implementierung der einzelnen module wurde im mrz 2006 ein erster betatest vorgenommen , um die prinzipielle lauffhigkeit und das zusammenspiel der einzelnen komponenten zu berprfen . 
 auch die implementierung des gesamten verfahrens in anderen kliniken oder einrichtungen wre innerhalb weniger wochen mglich , da dieses modell seine routinetauglichkeit bis heute tglich unter beweis stellt , alle notwendigen schritte bekannt / erprobt sind und die zustzlichen softwaremodule an andere gegebenheiten adaptiert werden knnen ; dies gilt auf jeden fall fr institutionen , die mosaiq nutzen und ber ein bergeordnetes kis verfgen . da vom kis die einzelnen internen codes ( leitziffern ) ber diese matchingtabelle in abhngigkeit von der gerade gltigen krankenkassenzugehrigkeit den entsprechenden codes der go oder des ebm zugeordnet bzw . 
die nativen ops weitergegeben werden , erreicht man , dass spezielle und vor allem immer wiederkehrende und zeitraubende nutzerschulungen ( rzte , mtras und physiker ) vor ort mit all den bekannten unwegsamkeiten und problemen berflssig werden . 
diese vorgehensweise sichert einer groklinik wie der universittsklinik freiburg in vorzglicher art die erlse , schafft zustzlich die notwendige flexibilitt , um auf die sich stetig verndernden gegebenheiten adquat und elegant reagieren zu knnen , und trgt entscheidend zur minimierung der belastung unseres rztlichen personals durch patientenferne ttigkeiten bei . 
7 strahlentherapie und onkologie original article dosimetric evaluation of high - dose - rate interstitial brachytherapy boost treatments for localized prostate cancer georgina frhlich1 , 2 , pter goston2 , jzsef lvey2 , andrs somogyi2 , jnos fodor2 , csaba polgr2 , tibor major2 purpose : to quantitatively evaluate the dose distributions of high - dose - rate ( hdr ) prostate implants regarding target coverage , dose homogeneity , and dose to organs at risk . material and methods : treatment plans of 174 implants were evaluated using cumulative dose - volume histograms ( dvhs )  . 
dose - volume parameters for target ( v90 , v100 , v150 , v200 , d90 , dmin ) and quality indices ( dnr [ dose nonuniformity ratio ] , dhi [ dose homogeneity index ] , ci [ coverage index ] , coin [ conformal index ] ) were calculated . 
maximum dose in reference points of rectum ( dr ) and urethra ( du ) , dose to volume of 2 cm3 of the rectum ( d2ccm ) , and 0.1 cm3 and 1% of the urethra ( d0.1ccm and d1 ) were determined . 
for urethra dose characterization , the use of d1 volumetric parameter is recommended . key words : prostate hdr brachytherapy dvh evaluation dose to organs at risk strahlenther onkol 2010 ; 186 : 38895 doi 10.1007 / s00066 - 010 - 2081 - x dosimetrische auswertung von boostbestrahlungen des lokalen prostatakarzinoms mittels interstitieller high - dose - rate - brachytherapie ziel : quantitative auswertung der dosisverteilungen von high - dose - rate - ( hdr - ) brachytherapie - multikatheterimplantaten bezglich zielvolumenerfassung , dosishomogenitt und dosisbelastung kritischer organe . material und methodik : zur beurteilung wurden die dosis - volumen - histogramme ( dvh ) der bestrahlungsplne von 174 patienten herangezogen . 
dosis - volumen - parameter fr das zielvolumen ( v90 , v100 , v150 , v200 , d90 , dmin ) und die qualittsindizes ( dnr [ dose nonuniformity ratio ] , dhi [ dosishomogenittsindex ] , ci [ coverage index ] , coin [ konformittsindex ] ) wurden berechnet ( tabelle 5 )  . 
sowohl die maximale dosis in referenzpunkten des rektums ( dr ) und der urethra ( du ) als auch die dosis im absoluten volumen von 2 cm3 des rektums ( d2ccm ; abbildung 2a ) und die dosiswerte fr volumina von 0 , 1 cm3 und 1% der 1school of phd studies , semmelweis university , budapest , hungary , 2department of radiotherapy , national institute of oncology , budapest , hungary . received : september 28 , 2009 ; accepted : february 16 , 2010 published online : june 24 , 2010 strahlenther onkol 2010 no . 
anschlieend wurde eine parameterfreie korrelationsanalyse zwischen diesen parametern durchgefhrt . ergebnisse : es wurden im mittel 16 nadeln pro applikation implantiert , das mittlere volumen der prostata ( vp ) wurde mit 27 , 1 cm3 bestimmt . 
die spearman - rangkorrelationskoeffizienten fr die volumendosis von rektum und urethra ergaben sich mit r ( dr , d2ccm ) = 0.69 ( abbildung 3 ) , r ( du , d0.1ccm ) = 0 , 64 und r ( du , d1 ) = 0 , 23 ( abbildungen 4a und 4b )  . schlussfolgerung : die ultraschallbasierte bestrahlungsplanung fr die hdr - brachytherapie der prostata ermglicht die genaue definition der implantatgeometrie und liefert akzeptable dosisverteilungen . 
fr die charakteristische dosisbeschreibung an der urethra wird der dosisvolumen - parameter d1 empfohlen . schlsselwrter : prostata hdr - brachytherapie dvh - auswertung dosis in risikoorganen introduction the incidence of prostate cancer is very high in developed countries , and it is the fourth leading cause of cancer mortality in hungarian male population [ 19 ]  . 
it is well known from previous studies , that dose escalation improves local and biochemical control for locally advanced prostate cancer but can significantly increase the rate of side effects [ 13 , 14 , 22 , 44 , 45 , 49 ]  . 
in brachytherapy ( bt ) , the safety margin can be completely omitted , since the planning target volume ( ptv ) is equal to the clinical target volume ( ctv ) , and a higher degree of protection of organs at risk ( oars ) can be reached because of the smaller treated volume [ 17 ]  . two bt modalities are used for prostate cancer : permanent implantation with low - dose - rate ( ldr ) seeds using 125i or 103pd isotopes [ 3 , 32 , 34 , 35 , 41 ] , and temporary implantation with high - dose - rate ( hdr ) or pulsed - dose - rate ( pdr ) technique using 192ir isotope [ 1 , 2 , 810 , 18 , 21 , 25 , 30 , 39 , 43 ]  . the treatment protocol for intermediateand high - risk , clinically nonmetastatic prostate cancer at our institution includes the combination of three - dimensional conformal rt and bt boost using hdr afterloading technique with 192ir source . the purpose of the present study is to quantitatively evaluate the dose distributions of prostate hdr - bt implants regarding dose conformity , homogeneity , and dose to oars . material and methods at our institute , 174 intermediateor high - risk patients with clinically localized prostate cancer treated with a combination of three - dimensional conformal rt and hdr - bt boost treatment were selected into this study . 
teletherapy was performed with 18 - mv photon beams using a four - field box technique , and the prescribed dose ( pd ) to the whole pelvis was 4446 gy ( in fractions of 2 gy / day ) ; then , the prostate and the vesicle seminals were treated up to a total dose of 60 gy using smaller fields . 
an additional 10 gy was given to the prostate with bt . implantation technique the hdr - bt boost with one fraction was performed in the first 4 weeks of teletherapy . 
the plato brachytherapy planning system v14.2.6 ( nucletron , veenendaal , the netherlands ) was used for treatment planning , and the patients were treated with a microselectron v2 afterloading machine ( nucletron )  . treatment planning the contoured ptv was the whole prostate gland without safety margin recommended by gec / estro - eau publication [ 26 ] ( figure 1 )  . 
on each axial image , the rectum reference point was placed at 0.5 cm from the outer surface of the us probe in anterior direction ( figure 2a )  . 
the rectum volume was defined as a shell with 5 mm thickness following the curvature of the us probe ( figure 2a ) , and the urethra contour was outlined around the foley catheter with a 1 - mm margin representing the outer surface of the urethra wall ( figure 2b )  . 
dosimetry of temporary prostate brachytherapy during treatment planning , geometrical optimization was used followed by graphical optimization method in order to achieve a suitable dose distribution . dosimetric evaluation the dose plans were quantitatively evaluated with cumulative dose - volume histograms ( dvhs )  . 
volume and dose parameters , and quality indices ( coverage , conformity , and homogeneity ) were calculated as follows : ( i ) volume and dose parameters ( in percent ) : v90 , v100 , v150 , v200 : the volume of the ptv receiving 90% , 100% , 150% , and 200% of the pd . d90 : the minimum dose delivered to 90% of the ptv . dmin : the minimum dose in the ptv . ( ii ) indices : dnr = v150 / v100 , dose nonuniformity ratio , where v100 and v150 are the absolute volumes in cm3 irradiated by 100% and 150% of the pd [ 12 ]  . dhi = ( v100v150 ) / v100 , dose homogeneity index [ 23 ]  . ci = v100 / 100 , coverage index [ 23 ]  . coin , conformal index [ 4 ] , figure 1 . 
the light blue line is the urethra contour , the green line represents the isodose line , which irradiates 1% of the urethra , and the light blue point is the reference point of the urethra . 
the implantation is usually made under transrectal us guidance , and the treatment planning is also based on transverse us images [ 5 , 12 , 23 , 29 ]  . 
using plastic needles , fractionated treatment delivery and treatment planning based on computed tomography and magnetic resonance imaging have become feasible as well [ 7 , 29 , 31 , 51 ]  . 
published parameters and their values dealing with hdr prostate bt are shown in detail in tables 4 and 5 . in prostate bt , the ptv , generally , is the whole prostate , but with respect to homogeneity of the dose distribution , there are significant differences in the literature [ 26 ]  . 
the authors conclude that a needle number around 1518 results in suitable dose distribution in most cases , though the ideal number of needles depends on the size and shape of the ptv , as well as on the position of the urethra . 
literaturbersicht zur dokumentation von dosis - volumen - parametern bei der high - dose - rate - brachytherapie der prostata . b : blase ; oars : risikoorgane ; r : rektum ; u : urethra ; brige abkrzungen s . 
 [ 48 ] came to a similar conclusion , when they found increased genitourinal toxicity with a higher number of needles . there is no universally accepted method to describe the dose to oars . 
 [ 20 ] described the dose to bladder and rectum with a volume receiving 75% of the pd ( v75 ) , and they used v125 to characterize the dose to urethra . 
the rectum reference points are placed on the surface of the contoured volume ( figure 2a ) , and the maximum point dose is usually equal to the maximum dose in the rectum volume , since the reference points among any points of the rectum volume are those closest to the needles . 
in other points in the rectum , the doses are lower because of the increased distance from needles , but all parts of the 2 - cm3 volume are near to or around the reference points . in case of the urethra , however , the situation is different . 
 here , the reference points are in the center of the urethra contours ( figure 2b ) , and for geometrical reasons the maximum dose in the whole urethra volume develops somewhere else on the contour . 
this is clearly shown by our results , since dose values for the most exposed 0.1 cm3 and 1% of the urethra ( on average 126% and 140% ) are significantly larger than the maximum dose in the reference points ( on average 119% )  . 
 the d1 ( 140% ) values are closer to the real maximum doses in the urethra volume than the lower d0.1ccm ( 126% ) and du ( 119% ) values . conclusion the us - based treatment planning supported by dose optimization algorithms in prostate bt results in suitable dose distribution regarding homogeneity and conformity in most cases , and the dose to oars can be kept under acceptable limits . 
dose to rectum can approximately be described by the dose in reference points , but volumetric evaluation using the gec / estro - eau guidelines is recommended to enable comparability of the results with others . 
for determination of dose to urethra , the d1 volumetric parameter is recommended . acknowledgment we express our gratitude to michael niekamp for the german translation . strahlentherapie und onkologie original article long - term outcome of mitomycin cand 5 - fu - based primary radiochemotherapy for esophageal cancer * maria wolf1 , franz zehentmayr1 , maximilian niyazi1 , ute ganswindt1 , wolfgang haimerl1 , michael schmidt2 , dieter hlzel3 , claus belka1 background and purpose : for definitive radiochemotherapy , 5 - fluorouracil / cisplatin protocols have been considered the standard of care for esophageal carcinoma over the last 2 decades . 
52% ( 102 / 196 ) in the 5 - fluorouracil / mitomycin c group had tumor stages comparable to the rtog 85 - 01 study cohort ( t13 n01 m0 )  . 
the median survival in this subgroup was 18.2 months , 3and 5 - year survival rates were 22.7% ( 21 / 102 ) and 15.0% ( 13 / 102 ) , respectively . conclusion : despite being nominally inferior to platinum - based radiochemotherapy , the overall survival rates are in a similar range . 
 however , there is no randomized trial available in order to prove the equality . key words : esophageal cancer radiochemotherapy 5 - fluorouracil and mitomycin c strahlenther onkol 2010 ; 186 : 37481 doi 10.1007 / s00066 - 010 - 2137 - y langzeitergebnisse nach primrer radiochemotherapie mit mitomycin c und 5 - fluorouracil bei sophaguskarzinom hintergrund und ziel : radiochemotherapie mit 5 - fluorouracil und cisplatin gilt seit 2 jahrzehnten als standard fr die primre behandlung des sophaguskarzinoms . 
retrospektiv wurde geprft , zu welchen ergebnissen das angewandte regime im vergleich zur standardtherapie fhrte . patienten und methodik : retrospektiv wurden tumorstadium , therapieform und das outcome der patienten mit sophaguskarzinom , die zwischen 1982 und 2007 behandelt wurden , erhoben ( tabelle 1 )  . 
primrer endpunkt war das gesamtberleben ( abbildungen 1a bis 1c )  . ergebnisse : 298 patienten ( 16 , 8% adenokarzinome [ 50 / 298 ] , 77 , 5% plattenepithelkarzinome [ 231 / 298 ] ) wurden primr behandelt . 
bei diagnosestellung wiesen 61 , 7% ( 184 / 298 ) uicc - stadien iiiiv , 54 , 4% ( 162 / 298 ) einen positiven lymphknotenstatus sowie 26 , 5% ( 79 / 298 ) fernmetastasen auf . 
102 / 196 patienten ( 52% ) in der radiochemotherapiegruppe hatten tumorstadium t13 n01 m0 , entsprechend * parts of the data were presented ( poster presentation ) at the 15th annual meeting of the german society of radiation oncology ( degro ) in bremen , june 1114 , 2009 . 1department of radiation oncology , university hospital munich , lmu , germany , 2institute for biometry and epidemiology , university hospital munich , lmu , germany , 3tumor registry munich , university hospital munich , lmu , germany . received : march 1 , 2010 ; accepted : march 11 , 2010 published online : june 24 , 2010 strahlenther onkol 2010 no . 
 schlussfolgerung : obwohl in diesem unselektionierten kollektiv der standardtherapie mit cisplatin / 5 - fluorouracil nominell unterlegen , sind die berlebensraten in einem vergleichbaren bereich ( tabelle 3 )  . 
eine radiochemotherapie mit 5 - fluorouracil und mitomycin c scheint hnlich effektiv wie die standardtherapie zu seallerdings gibt es keine randomisierte studie , um dies zu beweisen . schlsselwrter : sophaguskarzinom radiochemotherapie 5 - fluorouracil und mitomycin c introduction based on the results of the rtog 85 - 01 trial , the use of radiochemotherapy with cisplatin and 5 - fluorouracil ( 5 - fu ) is a well - accepted standard for the definitive treatment of esophageal cancer [ 21 ]  . 
although being a well - established radiosensitizer for the treatment of head and neck cancer [ 9 , 20 ] , cancer of the anal canal [ 17 ] , pancreatic carcinoma [ 7 , 37 ] , vulvar and cervical cancer [ 5 , 27 , 38 , 39 ] the drug has not only lost acceptance in the treatment of esophageal cancer , but its effectiveness has been seriously called into question [ 19 ]  . patients and methods radiochemotherapy with 5 - fu / mmc has been the standard of care for cancer of the esophagus at the department of radiation oncology , university hospital , ludwig maximilian university ( lmu ) munich , germany , for the last 2 decades , based on the clinical experience made by using the coia protocol [ 13 ]  . in a retrospective approach , the following data were systematically retrieved from the patient files as well as from the munich tumor registry : tumor stage , treatment , and outcome of all patients with either squamous cell carcinoma ( scc ) or adenocarcinoma ( ac ) of the thoracic esophagus , excluding ac with cardia and gastric involvement , treated between 1982 and 2007 at the department of radiation oncology , university hospital of the lmu munich . 
patients who received adjuvant or neoadjuvant radio ( chemo ) therapy or brachytherapy were excluded , as well as those in whom treatment was aborted prematurely or whose data were incomplete . 
72 patients received neoadjuvant or adjuvant radio ( chemo ) therapy , in 65 , treatment was stopped prematurely , 20 patients with other aforementioned exclusion criteria and 49 patients with missing data were excluded . 
the predominant tumor sites were the middle third of the esophagus with 29.9% ( 89 / 298 ) and the lower third with 34.2% ( 102 / 298 )  . 
15.1% ( 45 / 298 ) had second malignancies , independent of esophageal cancer . the radiation dose was at least 54 gy in 80.5% of the cases , 49.7% of the patients ( 148 / 298 ) received doses between 60 and 65 gy . 
3 - year survival was 3.9% ( 4 / 102 ) in the radiotherapy - alone arm , in contrast to 16.8% ( 33 / 196 ) in the combined - modality group . 
the log - rank comparison of the survival rates revealed a statistically significant difference with a p - value < 0.0001 ( hazard ratio [ hr ] 0.77 ; 95% confidence interval [ ci ] 0.680.87 ; figure 1b )  . 
 no significance was seen using 3 - d versus 2 - d planning , for age at diagnosis and tumor site ( see table 4 )  . including histology , grading , tand n - stage , dose level > 54 gy and concomitant chemotherapy in the multivariate cox regression analysis , only histology and n - stage did not remain significant . a subgroup of 102 / 298 patients ( 34% ) with t13 n01 m0 who received radiochemotherapy with 5 - fu and mmc showed 2 - year , 3 - year , and 5 - year overall survival rates of 37.5% ( 36 / 102 ) , 22.7% ( 21 / 102 ) , and 15% ( 13 / 102 ) , respectively . 
remarkably , several findings already indicated comparable patient characteristics and overall survival rates also observed in this retrospective analysis [ 2 , 3 , 14 , 16 , 18 , 24 , 31 , 34 , 41 ] ( table 3 , figure 1a )  . 
the predominant regimen with 5 - fu and mmc used in a definitive approach during the last 2 decades at the university hospital of the lmu munich does not yield results similar to standard therapy in so far as an overall survival rate of 15% at 5 years is nominally inferior to an overall survival rate of 27% at 5 years reported by using cisplatin and 5 - fu [ 21 ]  . 
 our results confirm the importance of radiochemotherapy in improving survival of patients with unresectable esophageal cancer [ 1 , 8 , 13 , 14 , 21 , 25 , 40 ] ( figures 1b and 1c )  . 
the latter can be administered with little toxicity in a range of solid tumors , but it seems to be less efficient than cisplatin [ 13 , 19 , 21 ]  . there may be two reasons for the less favorable outcome in this study as compared with the literature : worse patient selection and lower efficiency of mmc . 
additionally , a high rate of discontinuation of treatment , therapy - related mortality , and the fact that more than one third ( 102 / 298 ) of the patients did not receive concomitant chemotherapy because of comorbidities show a negatively biased selection of patients with poor prognosis . 
 a very high rate of scc represents an association with tobacco and alcohol abuse , hence a low socioeconomic status with manifest comorbidities as described in epidemiologic studies [ 6 , 15 ]  . 
value of mmc / 5 - fu - based therapy in esophageal cancer vanced stage , which also contributed to worse outcome than described in the literature [ 15 , 25 ]  . another reason could be the lower efficiency of mmc compared to cisplatin , which in fact has never been evaluated head to head in a randomized clinical trial , yet radiobiological estimations may help out here . 
in a systematic overview of preoperative radiochemotherapy trials including 1 , 012 patients with 311 pathologic complete remissions , the influence of mmc was not found to be significant [ 19 ]  . overall survival in the radiotherapy - alone group was poor and did not exceed 5% ( 4 / 102 ) at 3 years , which is comparable to other studies [ 32 , 36 , 40 ] even when taking into acall patients overall survival ( months ) all patients radiotherapy vs . radiochemotherapy rctx survival ( months ) radiotherapy vs . radiochemotherapy with 5 - fu and mmc rctx ( 5 - fu / mmc ) survival ( months ) all patients radiation dose < 54 gy > 54 gy survival ( months ) figure 2 . 
os bei strahlendosen 54 gy und > 54 gy : signifikant besseres os bei einer strahlendosis > 54 gy ( p = 0 , 002 ; hr 0 , 62 ; 95% - ci 0 , 460 , 82 )  . count that the randomized trials did not include metastatic patients . 
therefore , our data do not confirm the results of the int 0123 trial , which showed no benefit from dose escalation [ 4 , 29 ] , but suggests an impact of radiation dose on outcome figures 1a to 1c . 
ac : adenokarzinom ; f : weiblich ; 5 - fu : 5 - fluorouracil ; hr : hazard - ratio mit 95 - konfidenzintervall ( ci ) ; m : mnnlich ; mmc : mitomycin c ; rct : radiochemotherapie ; rt : radiotherapie ; scc : plattenepithelkarzinom . comparison univariate p , hr ( 95% ci ) multivariate p , hr ( 95% ci ) m vs . 
7 like several other reports do [ 10 , 26 , 32 , 36 ]  . as stated by coia et al . , concurrent radiochemotherapy by addition of 5 - fu and mmc to radiotherapy improves overall survival and even achieves long - term cure also in unfavorable tumor stages as shown here [ 13 ]  . 
the addition of chemotherapy increased the survival rate from 10% to 38% at 2 years ; the median survival was 8.9 months as compared with 12.5 months in the radiochemotherapy group . a subgroup of patients ( 102 / 298 ) in our study cohort had t13 n01 m0 , which is similar to the patient selection in the rtog 85 - 01 trial . 
 [ 14 ] , although the number of long - term survivors may be too small to draw conclusions . conclusion overall survival observed in this unselected collective is comparable with data of published trials . 
an overall survival rate of 15% at 5 years in the patient group receiving 5 - fu and mmc is nominally inferior to reported results by using cisplatin and 5 - fu . 
hence , as long as there is no randomized trial available in order to prove the equality , radiochemotherapy with 5 - fu and mmc instead of cisplatin may only be applied in case of contraindications to cisplatin . strahlentherapie und onkologie original article intraoperative radiotherapy ( iort ) with low - energy photons as a boost in patients with early - stage oral cancer with the indications for postoperative radiotherapy treatment feasibility and preliminary results tomasz rutkowski1 , andrzej wygoda1 , marcin hutnik1 , krzysztof skadowski1 , jerzy wydmanski1 , adam maciejewski2 , cezary szymczyk2 , janusz wierzgon2 , andrzej orlef3 , bogusaw maciejewski1 purpose : to evaluate the feasibility and preliminary results of intraoperative radiotherapy ( iort ) with low - energy photons as a boost in patients with early - stage oral cancer with the indications for postoperative radiotherapy . patients and methods : between 2003 and 2006 , 16 patients with early - stage cancer of mobile tongue ( n = 10 [ 63% ] ) or floor of the mouth ( n = 6 [ 37% ] ) treated at maria skodowska - curie memorial cancer center and institute of oncology , gliwice branch , poland , were evaluated for iort boost with the intrabeamsystem ( carl zeiss surgical gmbh ; iort - prs ) because of the high risk of local recurrence due to positive margins on frozen pathologic section . 
no late adverse effects were observed . conclusion : this preliminary report has demonstrated the feasibility of iort - prs for patients with early oral cancer with the indications for postoperative radiotherapy . 
this method may be considered an alternative boost technique , although additional studies are needed to establish long - term results in a larger group of patients . key words : oral cancer intraoperative radiotherapy photon radiosurgery system head and neck cancer boost strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2117 - 2 intraoperative radiotherapie ( iort ) mit niedrigenergetischen photonen als boost bei patienten mit einem mundhhlenkarzinom in einem frhen klinischen stadium , bei denen indikationen zur postoperativen radiotherapie bestehen . 
therapeutische anwendbarkeit und erste ergebnisse ziel : auswertung der anwendbarkeit und ersten ergebnisse der intraoperativen radiotherapie ( iort ) mit niedrigenergetischen photonen als boost bei patienten mit mundhhlenkarzinom in einem frhen klinischen stadium , bei denen indikationen zur postoperativen radiotherapie bestehen . patienten und methodik : in den jahren 20032006 wurden im onkologischen zentrum am maria - skodowska - curie - institut in gliwice , polen , 16 patienten mit mundhhlenkarzinom in einem frhen klinischen stadium behandelt . 
risiko1department of radiation oncology , maria skodowska - curie memorial cancer center and institute of oncology , gliwice branch , poland , 2department of surgery , maria skodowska - curie memorial cancer center and institute of oncology , gliwice branch , poland , 3department of physics , maria skodowska - curie memorial cancer center and institute of oncology , gliwice branch , poland . received : december 18 , 2009 ; accepted : may 20 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 urban & vogel rutkowski t , et al . 
als risikofaktoren wurden schmale oder positive absetzungsrnder , infiltration der lymphgefe und / oder der blutgefe durch das karzinom , perineurale karzinominfiltration , ungnstiger infiltrationstyp , tiefe der infiltration und geringgradige histopathologische differenzierung des karzinoms eingestunach chirurgischer entfernung des karzinoms wurde der applikator auf das tumorbett aufgesetzt . 
die frhreaktionen der mundschleimhaut auf die strahlentherapie wurden nicht hher als grad 3 nach dem rtog / eortc - score eingestudie mediane zeit bis zur kompletten ausheilung von frhreaktionen lag bei 35 tagen . 
sptreaktionen nach strahlentherapie wurden nicht beobachtet . schlussfolgerung : die ergebnisse der studie besttigen die anwendbarkeit von iort - prs bei patienten mit einem frhen mundhhlenkarzinom , bei denen indikationen zur postoperativen strahlentherapie bestehen . 
weitere studien sind jedoch erforderlich , damit die langzeitergebnisse in einer greren patientenpopulation ausgewertet werden knnten . schlsselwrter : mundhhlenkarzinom intraoperative radiotherapie photon radiosurgery system karzinom des kopf - hals - bereichs boost introduction oral cancers in early stages are usually treated with single - modality surgery or radiotherapy . 
in some cases , however , complementary radiotherapy is indicated due to the high risk of local recurrence [ 2 , 7 , 13 , 22 , 23 , 28 , 29 ]  . 
in this group of patients , similarly to more advanced cases , postoperative external - beam radiotherapy ( ebrt ) is often employed with escalated dose to the tumor bed ( boost ) [ 1 , 13 , 18 , 20 , 25 , 30 ]  . 
there are different techniques of boost delivery [ 5 , 8 , 9 , 11 , 16 , 17 , 21 , 24 , 26 , 33 ] and intraoperative radiation therapy ( iort ) is one of thethis treatment option particularly due to substantial advantages over others could be beneficial for such patients . iort refers to the delivery of single , high - dose radiation to selected anatomic areas identified during the surgical procedure as of high risk of recurrence and / or of residual disease . 
most clinical experiences of iort are based on electron beam ( eiort ) produced by linear accelerator [ 5 , 17 , 19 , 21 , 26 , 27 ] or high - energy photons ( brachytherapy ) [ 11 ]  . the prs400 photon radiosurgery system ( carl zeiss surgical gmbh ) , also called intrabeam , is designed to provide a high dose of low - energy photon radiation . 
 the device has been used as an innovative approach to partial - breast irradiation ( targeted intraoperative radiotherapy [ targit ] ) [ 30 ] and for radiotherapy of brain tumors [ 6 , 14 ]  . this study was initiated to determine the feasibility of iort - prs as a boost in patients treated surgically for early - stage oral cancer requiring additional radiotherapy due to a high risk of local recurrence . patients and methods in 2003 , an institutional ethics committee approved protocol of the study . 
between 2003 and 2006 , 16 patients with previously untreated early - stage oral cancer received iort - prs at the maria sklodowska - curie memorial cancer center and institute of oncology , gliwice branch , poland . 
 ebrt to the tumor bed was given to all patients and cervical nodes were irradiated , if not operated or after nodal resection according to pathologic involvement . details of patient characteristic , tumor stage distribution and surgical procedure are shown in table 1 . 
acute mucosal reaction was assessed each week for 1 month after iort or unless ebrt was completed and was graded according to the rtog scale . surgical procedure surgery was performed under general anesthesia with maximum transoral tumor resection of all visible disease . 
a radiation dose of 5 gy , 7 gy , or 7.5 gy specified at the reference point at a distance of 5 mm from the applicator surface was applied according to tumor volume and margin status . 
details of iort - prs in individual patients are shown in table 2 . the area at the highest risk of tumor recurrence was delineated by the surgeon and radiation oncologist . 
conformal photon irradiation with an energy of 6 mv was used . patient diameter of applicator ( cm ) contact dose ( gy ) reference dose ( gy ) treatment time ( min ) results rutkowski t , et al . 
in this place , a thick layer of fibrosis appeared later on . in seven out of ten patients treated with ebrt , grade 3 acute mucosal reaction related to ebrt was observed . 
positionierung und fixierung des applikators im tumorbett . the operating roothe whole treatment was completed in up to 40 min . ebrt discussion in all patients , the primary tumor bed was involved in the target volume of ebrt . 
an escalated dose up benefits of combination of surgery and postoperative radiotherapy for advanced head and neck cancer ( hnc ) are well established [ 1 , 20 , 30 ]  . 
iort - prs in oral cancer mor is reported in the range of 332% , even despite negative resection margins the strongest predictor of local recurrence [ 12 , 15 , 28 , 32 ]  . 
complementary radiotherapy usually includes dose escalation ( boost ) to the areas , where the risk of recurrence is considerable . the most popular techniques of boost delivery include additional ebrt fractions given in conventional , accelerated or concomitant schedule [ 1 , 9 , 13 , 20 , 30 ] , brachytherapy and some iort techniques [ 5 , 8 , 11 , 13 , 16 , 20 , 23 , 33 ]  . iort has several potential advantages over ebrt and brachytherapy . 
margins of cancer resection can be treated at the time of surgery with immediate sterilization from cancer cells , while normal tissues are retracted or shielded from the irradiated volume . 
since tumors are usually composed of individual cells that differ in radiosensitivity according to position in the cell cycle and oxygen tension , fractionated radiation therapy may be superior to a single high dose of iort . 
with fractionated radiation therapy , cells in relatively radioresistant phase of the cell cycle have an opportunity to progress into a more radiosensitive phase before subsequent radiation fraction is delivered . 
high - energy electrons are preferred due to some physical characteristics , as uniform dose depth and rapid dose fall - off below the depth defined by electron - beam energy . 
sophisticated methods of constant and adequate monitoring and management of a patient under general anesthesia during irradiation are therefore required . the iort - prs , a relatively new device generating low - energy x - rays , enables to omit some logistic disadvantages of eiort . 
the prs machine contains a miniaturized battery - powered linear accelerator producing a broad spectrum of low - energy x - rays , which are generated by directing an electron beam into a thin gold target and consist of bremsstrahlung . 
for this , the iort - prs machine could be placed in a standard operating roo the procedure is relatively simple and not time - consuming . several studies report the results of eiort for hnc . 
addition of eiort to resection and its combination with postoperative ebrt seems to improve local control in this group of patients [ 5 , 17 , 19 , 27 ]  . 
a good palliative effect was obtained in patients treated for extensive recurrence in previously irradiated fields [ 22 , 26 ]  . reports considering clinical application of iort - prs refer mostly to breast cancer ( targit ) [ 31 ] , primary , metastatic [ 6 ] , or recurrent brain tumors [ 14 ]  . 
physical and radiobiological characteristics of iort - prs demonstrate this method as potentially attractive for hnc treatment . dose distribution characteristic for photons , unique relative biological effectiveness ( rbe ) of iort - prs and biologically effective dose for large single fraction should be taken into account when calculating the iort - prs fraction dose . 
for clinically relevant 2 - gy fractions , the iort - prs exhibits rbe of 3.3 and for the dose of 15 gy , rbe of 1.9 should be taken into account . 
the rbe of iort - prs increases as the radiation dose from the iort - prs decreases , so the change in biologically weighted dose ( physical dose rbe ) decreases with depth more slowly than the physical dose does [ 4 ]  . 
in theory , this may enhance the biological effect at greater distance from the source . due to a high single fraction of radiation normal tissues are at higher risk of developing late complications as described by the / ratio . 
additionally , the potential for radiation - induced bone injury should be taken into account due to the preferential energy absorption in bone caused by photoelectric process . physical characteristics of that kind of radiation and its radiobiological attributes make iort - prs potentially useful in the management of hnc not only for palliative purposes , but also for boost delivery in radical treatment . 
this way of boost delivery appeared to be feasible in a selected group of patients with early - stage oral cancer requiring postoperative radiotherapy . conclusion this preliminary report has demonstrated the feasibility of iort - prs in patients treated surgically for early - stage oral cancer requiring additional radiotherapy due to a high risk of local recurrence . 
the method may be considered an alternative boost technique in a selected group of patients , although additional studies are needed to confirm the results in a larger group of patients . strahlentherapie und onkologie original article clinical results of proton - beam therapy for locoregionally advanced esophageal cancer masashi mizumoto1 , 2 , shinji sugahara1 , 2 , hidetsugu nakayama1 , 2 , haruko hashii2 , akira nakahara3 , hideo terashima4 , toshiyuki okumura1 , 2 , koji tsuboi1 , 2 , koichi tokuuye1 , 5 , hideyuki sakurai1 , 2 purpose : to evaluate the efficacy and safety of proton - beam therapy for locoregionally advanced esophageal cancer . patients and methods : the subjects were 51 patients with esophageal cancer who were treated between 1985 and 2005 using proton beams with or without x - rays . 
the other 18 patients received proton - beam therapy alone ( median 79 gye , range 6298 gye )  . results : treatment interruption due to radiation - induced esophagitis or hematologic toxicity was not required for any patient . 
of the 51 patients , 40 ( 78% ) showed a complete response within 4 months after completing treatment and seven ( 14% ) showed a partial response , giving a response rate of 92% ( 47 / 51 )  . 
further studies are required to determine the optimal total dose , fractionation schedules , and best combination of proton therapy with chemotherapy . key words : proton - beam therapy esophageal cancer pattern of failure complication radiotherapy strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2079 - 4 klinische ergebnisse der protonenstrahlentherapie bei lokoregionr fortgeschrittenem speiserhrenkrebs ziel : evaluierung der wirksamkeit und sicherheit der protonenstrahlentherapie bei lokoregionr fortgeschrittenem speiserhrenkrebs . patienten und methodik : es handelte sich um 51 patienten mit speiserhrenkrebs , die zwischen 1985 und 2005 mit protonenstrahlen allein oder kombiniert mit linac - photonen behandelt wurden . 
bis auf eine ausnahme hatten alle patienten ein plattenepithelkarzinovon den 51 patienten erhielten 33 eine kombination von photonen ( median 46 gy ) und protonen ( median 36 gye ) als boost . 
die anderen 18 patienten wurden ausschlielich mit protonenstrahlentherapie behandelt ( median 79 gye , spanne 6298 gye )  . ergebnisse : bei keinem patienten war eine behandlungsunterbrechung aufgrund strahleninduzierter sophagitis oder hmatologischer toxizitt erforderlich . 
die aktuarische gesamtberlebensrate der 51 patienten lag bei 21 , 1% in 5 jahren und die mediane berlebenszeit 20 , 5 monate ( 95% - konfidenzintervall 10 , 930 , 2 )  . 
von den 51 patienten erreichten 40 ( 78% ) innerhalb von 4 monaten nach behandlungsende eine komplette remission und sieben ( 14% ) eine partielle remission , was eine ansprechrate von 92% ( 47 / 51 ) ergibt . 
die lokale kontrollrate nach 5 jahren betrug bei allen 51 patienten 38 , 0% und das mediane lokalrezidivfreie intervall 25 , 5 monate ( 95% - konfidenzintervall 14 , 636 , 3 )  . schlussfolgerung : die protonenstrahlentherapie ist eine wirksame behandlung fr patienten mit lokal fortgeschrittenem speiserhrenkrebs . 
weitere studien sind notwendig , um optimale gesamtdosis , fraktionierung und die beste kombination von protonenstrahlenmit chemotherapie zu ermitteln . schlsselwrter : protonenstrahlentherapie speiserhrenkrebs rezidivmuster komplikation strahlentherapie 1proton medical research center , university of tsukuba , ibaraki , japan , 2department of radiation oncology , university of tsukuba , ibaraki , japan , 3department of gastroenterological medicine , university of tsukuba , ibaraki , japan , 4department of surgery , university of tsukuba , ibaraki , japan , 5department of radiology , tokyo medical university , shinjuku , tokyo , japan . received : november 4 , 2009 ; accepted : march 25 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 urban & vogel mizumoto m , et al . 
surgery as a standard therapy has achieved a 5 - year survival rate of 74% for patients with stage i esophageal cancer [ 12 ] , and chemoradiotherapy , surgery and combination therapy of chemoradiotherapy followed by surgery are used for patients with advanced - stage esophageal cancer [ 1 , 3 , 4 , 9 , 10 , 1517 , 21 , 24 , 27 ]  . 
in radiotherapy , the standard external - beam schedule used in japan is 60 gy in 30 fractions with concurrent chemotherapy using 5 - fluorouracil and cisplatin [ 19 ] , and ishikura et al . 
in the rtog 94 - 05 trial , the median survival time and local control rate did not differ for patients in the low - dose ( 50.4 gy ) and high - dose ( 64.8 gy ) arms [ 17 ]  . 
therefore , the efficacy of dose escalation for patients with esophageal cancer remains unclear , although a beneficial effect with hyperfractionated radiotherapy plus concurrent chemotherapy has been reported [ 30 , 32 ]  . new radiotherapy techniques such as intensity - modulated radiation therapy ( imrt ) , pbt and heavy - particle radiotherapy permit concentration of the radiation dose on the tumor with avoidance of critical organs [ 2 , 8 , 11 , 31 ] , and these techniques may allow effective dose escalation in treatment of esophageal cancer . 
pbt takes advantage of bragg peak properties to allow dose localization at the tumor while avoiding organs such as the lung , heart and spinal cord [ 5 , 18 , 29 ]  . 
we use high - dose pbt in a final attempt to improve survival and local control in these patients , and here , we retrospectively evaluate the efficacy and safety of high - dose pbt for advanced esophageal cancer . patients and methods patients 51 patients with carcinoma of the esophagus were treated at our hospital from november 1985 through december 2005 , and met the following eligibility criteria for the study : ( 1 ) histologically confirmed diagnosis of squamous cell carcinoma or another malignant carcinoma of the esophagus ; ( 2 ) world health organization ( who ) performance status ( ps ) of 02 ; ( 3 ) clinical stage t1 n1 m0 or t24 n0 / 1 m0 according to a computed tomography ( ct ) scan and endoscopy ; ( 4 ) provision of written informed consent for treatment ; and ( 5 ) an absence of uncontrolled malignant disease . 
during the same period , eight patients were excluded from the present review because of concurrent malignancy found during treatment ( n = 2 ) , pbt for recurrent tumors after photon therapy or chemotherapy ( n = 4 ) , planned resection after pbt ( n = 1 ) , and decreasing ps from 2 to 3 immediately before pbt ( n = 1 )  . the 51 patients comprised 47 men and four women , and had a median age of 72 years ( range 4795 years )  . 
t1 was defined as superficial , t2 was protruded or ulceration without circular stricture , t3 was circular structure or deep ulceration , and t4 was aortic invasion or tracheobronchial tree invasion by esophagoscopy . 
pretreatment evaluations included complete blood counts , liver function tests , esophagoscopy using the lugol dye method [ 23 ] , esophagography , chest x - rays , ct scans of the chest and upper abdomen , and bronchoscopy when necessary . 
endoesophageal ultrasonography was performed optionally , and bone scans were obtained when indicated . radiotherapy between 1985 and 2001 , 29 patients received pbt at up to 250 mev generated by a booster synchrotron at the high energy accelerator research organization . 
proton beams at this facility were available for clinical use for only 4 h each day for about 120 days / year , with frequent interruptions because of scheduled breaks for administrative reasons [ 26 ]  . 
from 2001 , proton beams became available for clinical use every day at a new facility of the proton medical research center . treatment planning was based on ct images taken at 5 - mm intervals with the patient in the treatment position . 
therefore , the treatment protocol was modified to a combination of photon and proton beams . in the combination treatment , the initial x - ray irradiation volume was planned based on esophagograms and chest ct scans . 
to define the location of the tumor clearly on fluoroscopy , in situ fiducial markers ( iridium chips of 0.5 mm in diameter and 3.0 mm in length ) were implanted endoscopically at the cranial and caudal boundaries of the primary tumor ( figure 1 )  . 
the cephalic and caudal borders of the initial radiation field were 3 cm from the primary tumor and the lateral borders of the field were 2 cm from the primary tumor . 
the median total dose of pbt was 36 gye ( range 760 gye ) , and the median total dose of combined x - rays and pbt for the 33 patients was 80 gye ( range 7090 gye ) over a median treatment period of 59 days ( range 4391 days )  . for pbt alone , the initial field was designed in the same manner as that for x - ray irradiation . 
the median total dose for the 18 patients was 79 gye ( range 6298 gye ) over a median treatment period of 57 days ( range 3364 days )  . 
proton - beam therapy for advanced esophageal cancer evaluation after treatment patients underwent endoscopy or esophagography to evaluate the initial tumor response immediately after the completion of treatment and 1 month later . 
complete response was defined as complete disappearance of all detectable tumors , without development of a new lesion in the esophagus , as confirmed by another evaluation performed 4 weeks later . 
calculation of the local control rate was based on the date on which tumor progression was found or the time of the last examination in cases with no esophageal tumor after treatment . 
the influence of age , t - classification , tumor length , n - classification , equivalent dose , and coexisting disease as possible prognostic factors for survival and local control was examined in univariate ( log - rank test ) and multivariate ( cox proportional hazards model ) analyses [ 7 ]  . results toxicity no patients had a treatment interruption attributable to radiation - induced esophagitis or hematologic toxicity , but pbt at 61.6 gye in 28 fractions had to be discontinued in one patient due to recurrent aspiration pneumonia . 
acute treatmentrelated toxicities were generally mild : 35 patients experienced grade 1 dermatitis in the irradiated skin ; 25 and nine suffered from acute esophagitis of grades 1 and 2 , respectively ; and six developed grade 3 esophagitis . 
as a late toxicity , one patient died due to hemorrhage from an esophageal ulcer at the site of irradiation without recurrence of the primary tumor considered grade 5 toxicity . 
postirradiation esophageal ulcers occurred in nine of 27 patients ( 33% ) who received < 80 gye and in 16 of 24 patients ( 67% ) who received 80 gye , with a significant difference between these two groups ( p = 0.03 by fishers exact test )  . 
no symptomatic late complications were observed in the tracheobronchial trees , the heart , or the spinal cord . survival the median follow - up period was 23 months for the twelve patients who were still alive at the last follow - up . 
of the 51 patients , 39 had died at the time of writing in january 2009 : 20 from uncontrolled primary diseases including metastases ; four from hemorrhage from esophageal ulcers at the site of irradiation ; and 15 for other reasons , including bronchogenic carcinoma ( n = 2 ) , hepatocellular carcinoma ( n = 1 ) , brain bleeding ( n = 2 ) , pulmonary disease ( n = 5 ) , cardiac failure ( n = 1 ) , liver failure ( n = 1 ) , pancreatitis ( n = 1 ) , unknown ( n = 1 ) , and treatment - related salvage chemotherapy ( n = 1 )  . 
the complete response rates were 100% ( 17 / 17 ) for patients at the t1 or t2 stage , 77% ( 20 / 26 ) for t3 , and 38% ( 3 / 8 ) for t4 , with a significant difference in complete response between stages t13 and t4 ( p = 0.008 by fishers exact test )  . 
ergebnis nach strahlentherapie mit lokalisation der rezidive . progression - free primary tumor lymph node inside irradiated area lymph node outside irradiated area distant metastases patients n ( % ) 22 ( 43 ) 17 ( 33 ) 6 ( 12 ) 1 ( 2 ) 5 ( 10 ) prognostic factors the effects of possible prognostic factors on local control and survival were examined in univariate and multivariate analyses . 
in univariate and multivariate analysis of the potential prognostic factors , only t - stage was associated with survival ( table 4 ) and no factors showed a significant association with local control . discussion chemoradiotherapy is the established treatment for locoregionally advanced esophageal cancer , and ishikura et al . 
a simple comparison of these data suggests that our results are slightly inferior , which may be because our patients were old , and had complicating diseases and a poor general condition , with 14 of the 39 deaths due to a reason other than esophageal cancer . 
die progressionsfreie berlebensrate betrug jeweils 45 , 5% , 24 , 6% und 13 , 6% und die lokale kontrollrate 64 , 5% , 42 , 8% und 38 , 0% . sites shown in table 3 . 
17 of the 29 patients had recurrence of the primary tumor , six had recurrence at a lymph node inside the irradiated area , one had metastasis to a lymph node outside the irradiated area , and five had distant metastases . 
 [ 6 ] reported a 5 - year survival rate of 26% for patients with stage t13 n0 / 1 m0 esophageal cancer treated by chemoradiotherapy , but 0% for those treated with radiotherapy alone . 
collectively , the current and previous findings suggest that pbt without chemotherapy may not be suitable as the standard therapy for patients with locoregionally advanced esophageal cancer , but may have an advantage for patients who cannot be treated with chemoradiotherapy or surgery . 
therefore , chemotherapy schedule was not unified and the information was insufficient to discuss the efficacy of chemotherapy . the median pbt dose with or without radiotherapy was 80 gye in the current study . 
we anticipated that high - dose pbt would improve local control , but the radiation dose was not significantly associated with local control in multivariate analysis and recurrence of the primary tumor was most common , as in previous reports [ 13 , 17 , 32 ]  . 
 these results indicate that dose escalation for esophageal cancer reaches a maximum level for improvement of local control and combined therapy such as chemo - pbt is needed to achieve a better treatment effect . 
in our previous report , t1 and t2t4 were in halves , on the other hand only 16% ( 8 / 51 ) were t1 in this report . late toxicity seemed to be reduced in our study compared to those performed with standard chemoradiotherapy , in which heart and lung late toxicity is common [ 13 , 17 ]  . 
we did not observe lung and heart late toxicity of grade 3 , which is due to the excellent dose localization of a proton beam that avoids damage to the lung and heart . 
in our study , the most common late toxicity was esophageal ulcer , with one death due to hemorrhage from an esophageal ulcer at the site of irradiation without recurrence of the primary tumor and four cases of refractory ulcer . 
however , the minimum dose for an equivalent therapeutic effect to that achieved at 80 gye is unclear , and it will be important to determine the optimal pbt schedule that reduces the risk of esophageal ulcer without decreasing the anticancer efficacy . challenges for the future include proper identification of the indication for pbt as a treatment modality for esophageal cancer . 
chemoradiotherapy followed by surgery has been established as an important therapy for advanced - stage esophageal cancer [ 1 , 3 , 4 , 9 , 10 , 1517 , 21 , 24 , 27 ]  . 
pbt has a better dose distribution than traditional radiotherapy [ 31 ] , so a simple change to pbt from traditional radiotherapy has the potential to reduce toxicity and improve treatment outcome , and we have now begun tests of the efficacy of chemo - pbt compared to chemoradiotherapy . 
further prospective studies are needed to determine the optimal schedule for pbt and to establish this therapy as a treatment modality in combination therapy . acknowledgment the study was supported in part by a grant - in - aid for cancer research ( 15 - 9 ) from the ministry of health , labor , and welfare of the japanese government . strahlentherapie und onkologie original article brachial plexopathy after chemoradiotherapy for head and neck squamous cell carcinoma nele platteaux1 , piet dirix1 , robert hermans2 , sandra nuyts1 purpose : to evaluate late brachial plexopathy after primary chemoradiotherapy for locally advanced head and neck squamous cell carcinoma . patients and methods : consecutive 43 disease - free patients were evaluated by a specifically developed 26 - item questionnaire . 
 retrospectively , the brachial plexus was delineated and the dose - volume histograms were calculated . results : after a median follow - up of 24 months , no radiation - induced brachial plexopathy was reported in these 43 patients . conclusion : no radiation - induced brachial plexopathy was seen in the patient group , although 72.1% of the brachial plexuses received doses > 60 gy . 
these findings should prompt further prospective studies and also stress the importance of trying to keep the doses to the brachial plexus as low as possible while covering the target volumes well . key words : head and neck cancer chemoradiotherapy brachial plexopathy imrt strahlenther onkol 2010 ; 186 : 51720 doi 10.1007 / s00066 - 010 - 2099 - 0 brachiale plexopathie nach radiochemotherapie wegen plattenepithelkarzinom im hno - bereich ziel : untersuchung zur hufigkeit einer radiogenen funktionsbeeintrchtigung des armplexus nach primrer radiochemotherapie wegen eines lokal fortgeschrittenen plattenepithelkarzinoms in der kopf - hals - region . patienten und methodik : hufigkeit und ausma neurologischer funktionseinschrnkungen des plexus brachialis wurden konsekutiv bei 43 therapierten krankheitsfreien patienten anhand eines speziell entwickelten fragebogens mit 26 einzelpunkten ( tabelle 1 ) ermittelt . 
die beidseitigen armplexus wurden retrospektiv konturiert und fr diese die jeweiligen dosis - volumen - histogramme erstellt . ergebnisse : nach einer medianen nachbeobachtungszeit von 24 monaten trat bei den 43 patienten kein einziger fall einer radiogenen brachialen plexopathie auf . schlussfolgerung : obwohl 72 , 1% der im bestrahlungsvolumen miterfassten armplexus gesamtdosen von > 60 gy erhielten , wurden in der eigenen patientengruppe keine radiogenen brachialen plexopathien beobachet . 
sie unterstreichen die wichtigkeit , die dosen am plexus brachialis so niedrig wie mglich zu halten und dennoch die zielvolumina ausreichend zu erfassen . schlsselwrter : kopf - hals - tumoren radiochemotherapie brachiale plexopathie imrt introduction intensification of radiation treatment for advanced head and neck squamous cell carcinoma ( hnscc ) through the use of altered fractionation and concomitant chemotherapy has resulted in significantly improved locoregional control and survival rates [ 1 , 2 , 19 , 2123 , 26 ]  . 
clearly , the organ - sparing potential of imrt and other highly conformal radiotherapy techniques relies heavily on the appropriate selection and accurate delineation of the critical organs at risk ( oars ) , with the application of rigorous constraints during planning [ 5 , 28 ]  . radiation - induced brachial plexopathy ( ribp ) is a relatively common complication after radiotherapy for breast or lung cancer , but any patient receiving radiotherapy in the vicinity of the brachial plexus ( bp ) is at risk for subsequent plexopathy [ 6 , 12 ]  . 
since the target volumes for advanced hnscc regularly extend to the lower neck , concerns over the development of ribp 1department of radiation oncology , leuvens kankerinstituut ( lki ) , university hospitals leuven , campus gasthuisberg , belgium , 2department of radiology , leuvens kankerinstituut ( lki ) , university hospitals leuven , campus gasthuisberg , belgium . received : october 29 , 2009 ; accepted : april 29 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 no . 
radiation - induced brachial plexopathy among head and neck cancer patients have prompted the radiation therapy oncology group ( rtog ) to include the bp as an oar in many recent protocols . 
historical data gathered mostly on breast cancer patients suggest a value for a 5% ribp risk at 5 years of 62 , 61 , and 60 gy and a value for a 50% risk at 5 years of 77 , 76 , and 75 gy for one third , two thirds , and the whole organ , respectively [ 4 ]  . 
showed that hnscc patients often receive a bp dose > 60 gy , with 70% and 30% of patients receiving doses of > 66 and > 70 gy , respectively [ 9 ]  . the aim of this study was to review consecutive 43 disease - free patients who received chemoradiotherapy in our department , to quantify the dose delivered to the bp and to correlate this dose to the presence of ribp . patients and methods 43 disease - free patients , treated between 2005 and 2008 for locally advanced hnscc , were included for this retrospective study . 
briefly , patients were treated according to a hybrid fractionation schedule ( consisting of 20 fractions of 2 gy [ once daily ] followed by 20 fractions of 1.6 gy [ twice daily ] ) to a total dose of 72 gy in 6 weeks , and received chemotherapy ( cisplatin 100 mg / m2 ) during the 1st and 4th week . 
at the time of treatment , the bp was not considered an oar and , consequently , it was not delineated nor included in the treatment - planning process ( no constraints were implemented ) in any of the patients . evaluation of brachial plexopathy patients were assessed at the outpatient clinic for evaluation of brachial plexopathy at a median and mean of 24 months after the end of treatment ( range , 545 months )  . 
negation of impaired hand functions appeared to reliably rule out ribp , with a sensitivity of 80% [ 11 ]  . additionally , we included questions from the european organizastrahlenther onkol 2010 no . 
radiation - induced brachial plexopathy tion for research and treatment of cancer ( eortc ) chemotherapy - induced peripheral neuropathy ( cipn20 ) quality of included four questions from the nine - item sensory scale and three questions from the motor scale as well as two questions on pain and swelling , which are common symptoms in ribp . life questionnaire [ 20 ]  . 
we the patients were asked to rate each problem as none at all , slight , moderate , or pronounced on a four - point likert scale [ 11 , 20 ]  . brachial plexus delineation the original planning computed tomography ( ct ) scans together with the 3d - crt or imrt treatment plans of the 43 previously irradiated patients were retrieved from the planning system ( eclipse , varian inc , palo alto , ca , usa ) for retrospective delineation and dose - volume histogram ( dvh ) calculation of the left and right bp separately . 
for example , the v50 was defined as the volume of the bp receiving a dose 50 gy . guidelines for contouring the bp on axial ct scans were recently developed by hall et al . 
however , it should be noted that the bp usually is difficult to identify on ct , but is better visible on t1 - weighted magnetic resonance imaging ( mri ) sequences [ 9 , 25 ]  . 
it was extended from the lateral aspect of the spinal canal to the space between the anterior and middle scalene muscles and delineated inferiorly as the posterior aspect of the neurovascular bundle just below the clavicular head [ 10 ]  . 
the mean of the mean and maximum doses to the bp was 44.14 gy ( range , 19.1062.43 gy ) and 64.20 gy ( range , 44.0279.47 gy ) , respectively . 
problems raising the arm were reported in three patients due to intercurrent pathologies such as a previous cerebrovascular accident ( n = 1 ) , periarteritis of the shoulder ( n = 1 ) , and a previous trauma with paralysis of the right arm ( n = 1 )  . impaired hand functions were reported by two patients also due to intercurrent pathologies , i.e. , a previous cerebrovascular accident and a previous trauma with paralysis of the right arm . second , on all other 24 questions none of the patients reported moderate or severe complaints . at the time of analysis , none of the patients presented any clinical sign of brachial plexopathy . discussion ribp typically presents with symptoms of shoulder and arm pain , and / or weakness and atrophy of the muscles of the hand . 
case studies in humans and experimental studies found vascular lesions consisting of necrosis and hyalinization of the media of small arteries and extensive thickening of epiand perineurium [ 10 ]  . 
the incidence of severe ribp ranges from 1% to 5% in women receiving radiotherapy following mastectomy , but less severe ribp may be present in an additional 9% of patients . 
radiation - induced brachial plexopathy in our study , none of the patients presented with ribp , although in 72.9% of cases , the bp received doses > 60 gy with a risk of 5% for ribp [ 4 , 9 ]  . 
it also stimulates further efforts to try to keep the doses on the bp as low as possible without compromising the coverage of the target volumes by using modern irradiation techniques like imrt . conclusion no ribp was seen in our patient group , although 72.1% of the bps received doses > 60 gy . 
until then , it is advisable to keep the doses to the pb as low as possible to reduce the risk of brachial plexopathy while covering the target volumes well . strahlentherapie und onkologie review article the use of fdg - pet to target tumors by radiotherapy guido lammering , dirk de ruysscher , angela van baardwijk , brigitta g . 
baumert , jacques borger , ludy lutgens , piet van den ende , michel llers , philippe lambin1 fluorodeoxyglucose positron emission tomography ( fdg - pet ) plays an increasingly important role in radiotherapy , beyond staging and selection of patients . 
especially for non - small cell lung cancer , fdg - pet has , in the majority of the patients , led to the safe decrease of radiotherapy volumes , enabling radiation dose escalation and , experimentally , redistribution of radiation doses within the tumor . 
it should be emphasized that using pet is only safe when adhering to strictly standardized protocols . key words : pet radiotherapy treatment planning target delineation strahlenther onkol 2010 ; 186 : 47181 doi 10.1007 / s00066 - 010 - 2150 - 1 der einsatz der fdg - pet bei der behandlung von tumoren mittels strahlentherapie die fluordesoxyglucose - positronenemissionstomographie ( fdg - pet ) spielt eine zunehmende bedeutung in der strahlentherapie , neben der bereits etablierten bedeutung fr tumorstaging und patientenselektion . 
insbesondere bei nichtkleinzelligen lungenkarzinomen fhrt der einsatz der fdg - pet in der mehrzahl der flle zu einer unbedenklichen abnahme des strahlenvolumens , wodurch dosiseskalationen und auf experimenteller ebene selbst dosisumverteilungen der strahlendosis im zielvolumen mglich werden . 
der einsatz der fdg - pet sollte nur nach streng standardisierten protokollen erfolgen . schlsselwrter : pet strahlentherapie bestrahlungsplanung zielvolumeneinzeichnung 1maastro clinic , radiation oncology , maastricht , the netherlands . received : march 25 , 2010 ; accepted : july 5 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 no . 
the probability for radiotherapy to achieve tumor control is dependent on two crucial issues : dose and treatment time on the one hand and precise delivery of that dose on the tumor on the other . 
indeed , theoretically , when extremely high radiation doses ( e.g. , 200 gy ) could be given to the tumor only , thus sparing normal tissues , a virtually 100% probability to achieve local tumor control would emerge , without toxicity . 
an incorrect definition of the gross tumor volume ( gtv , i.e. , detectable tumor ) or clinical target volume ( ctv , tumor plus a margin for microscopic extension ) is a source of systematic errors , which can lead to undertreatment and reduces the probability of tumor control . perfect delineation of the tumor requires apart from optimal diagnostic accuracy ( cancer or not ) also the capability to sharply identify the anatomic borders of the tumor . 
all this should be done in radiotherapy position , in order to avoid mismatching , image warping and other image manipulations , which all increase the chance of errors . a weak point in current tumor delineation protocols is its manual component . 
automated tools are therefore needed . positron emission tomography ( pet ) and , certainly , integrated pet - ct ( computed tomography ) have many potential advantages for radiotherapy planning . 
they combine anatomic and biological information in an identical patient position as radiotherapy will be delivered , there is no time interval between pet and ct scan , the ct can be used for attenuation correction , and ct densities can be used for radiation dose calculation . although not the aim of this article , it should be stressed that , as with any other imaging and therapeutic modality , also pet in radiotherapy should be calibrated thoroughly as well as used in strict clinical protocols . 
volume assessment with pet is crucially dependent on technical factors and huge mistakes can only be avoided by sticking to well - established protocols [ 9 ]  . pet with fluorodeoxyglucose ( fdg ) as tracer in radiotherapy planning has been investigated in many cancer types , of which non - small cell lung cancer ( nsclc ) is the most widely applied in clinical practice . 
in other tumor types , such as head and neck cancer , neurological tumors , esophageal carcinoma , rectal cancer , lymphoma and cervical carcinoma , radiotherapy planning using fdg - pet has a role to play . for each of these tumor types , the following questions will be addressed : ( 1 ) does pet scanning allow accurate tumor delineation ? does pet scanning change gtv , ctv and / or the ptv ( planning target volume ) , both for the primary tumor and the local and regional lymph nodes ? ( 2 ) does pet scanning allow improvement of treatment outcome ? lung cancer non - small cell lung cancer ( nsclc ) pet for defining tumor volumes ( figure 1 ) nodal target volume accurate identification of nodal metastases is crucial for planning curative radiotherapy , particularly as routine elective nodal irradiation is no longer recommended in nsclc [ 64 ]  . 
fdg - pet scan has a higher sensitivity , specificity and accuracy for detection of lymph node involvement and distant metastases in nsclc than ct scan and , therefore , results in a more accurate staging [ 75 ]  . in several planning studies , it was shown that pet or pet - ct influences the gtv [ 50 , 51 ]  . 
these results were subsequently confirmed in another , similar prospective study from the netherlands cancer institute [ 6 ] , but not in a us retrospective series [ 68 ]  . 
although pet - defined mediastinal radiotherapy fields appear to be safe , because of a false - positive rate of approximately 30% and a false - negative rate of about 7% , depending on the patient population , ideally , pathologic confirmation of pet - positive mediastinal nodes should be obtained by mediastinoscopy or endoscopic ultrasound - guided fine - needle aspiration ( eus - fna )  . target volume for primary tumor at present , fdg - pet scans offer little additional advantage over ct or mri ( magnetic resonance imaging ) scans for staging of the primary tumor because of its lack of precise anatomic localization . 
the spatial resolution of modern ct scanners ( typically about 1 mm ) is far superior to that of current pet scanners ( 68 mm ) , so that the extra gain with fusion is expected not to be large , unless pet scans can reliably address tumor delineation caused by atelectasis or intratumor heterogeneity . 
this clearly affects patient outcome , for it spares toxic therapy in individuals who will not benefit from it . the pet volumes were , in general , smaller than with ct . 
 the incorporation of pet in radiotherapy planning has , as previously shown , the potential to allow radiation dose escalation without increasing side effects , namely because of the reduction of radiation fields [ 14 , 72 ]  . 
in a phase i / ii trial , it was shown that this prerequisite is indeed true [ 71 ]  . whether this radiation dose increase will ultimately lead to higher cure rates is a matter of current research . pet scans may also allow the identification of therapyresistant areas within the tumor that could be given a higher radiation dose and hence lead to a better outcome [ 2 , 3 ]  . small cell lung cancer ( sclc ) pet scan for radiotherapy of limited - disease small cell lung cancer literature is sparse on the role of pet in limited - disease small cell lung cancer ( ld - sclc )  . 
although after ct - based radiotherapy planning , isolated nodal recurrences may be seen in > 10% of the patients , selective nodal irradiation based on pet scans proved to result in only 3% of isolated nodal failures in a prospective study [ 74 ]  . conclusions for nsclc , fdg - pet allow more thorough staging , thus avoiding unnecessary treatments . 
in most patients , it reduces radiation treatment volumes because of the avoidance of mediastinal lymph nodes that are pet - negative and hence reduces toxicity with the same radiation dose or enables radiation dose escalation with the same toxicity . 
pet also reduces interobserver variability for delineating tumors and opens perspective for more automated delineation parts in radiotherapy planning , as well as innovative radiation treatment delivery . primary brain tumors compared with other organ systems , fdg - pet imaging of the brain presents unique challenges because of the high background glucose metabolism of normal gray matter structures . 
this method was on its turn to be less prone to variability than pet - ct [ 70 ]  . as pet acquisition takes several minutes , tumor motion due to respiration or cardiac action results in pet gtvs that incorporate at least some effects of this motion . 
respiration - gated pet acquisition techniques have been developed [ 23 , 49 ] and are , at present , evaluated in clinical studies . clinical target volume in view of the relatively poor spatial resolution of pet scans , it does not come as a surprise that at the time of writing , no clear advantages of pet to define the microscopic extensions strahlenther onkol 2010 no . 
they have the tendency to recur locally and to undergo malignant degeneration in which case pet can have added value during follow - up . low - grade glioma functional imaging with modern tracers such as 11c - met ( methionine ) results in good visualization of low - grade gliomas . 
 baseline amino acid uptake on 18f - fet - pet in a diffuse versus circumscribed tumor pattern on mri is a strong predictor for the outcome of patients with low - grade glioma [ 20 ]  . 
comparing fdg - pet with mri in 14 patients with predominantly low - grade glioma , pet volumes were larger than , equal to , or smaller than mri - derived tumor volumes in seven , four , and three patients , respectively [ 53 ]  . 
 [ 37 ] found 11c - met superior to 18f - fdg and 18f - flt ( 18ffluoro - 3 ' - deoxy - 3 ' - l - fluorothymidine ) respectively , in delineating low - grade glioma . 
for low - grade glioma , an amino acid tracer is the tracer of first choice in radiotherapy planning . pituitary adenoma the value of 18f - fdg and 11c - met in addition to mri was investigated in a population of 57 patients comprising a variety of tumors including ten pituitary adenomas [ 41 , 42 ]  . 
in recurrent adenoma after surgery , 11c - met may distinguish between active tumor and fibrosis , which is essential to define an optimal target volume for radiotherapy purposes [ 8 ]  . high - grade glioma ( figure 2 ) studies comparing tumor volumes based on pet ( both 18f - fdg and 11c - met ) and other imaging modalities usually show that pet scan volumes are smaller than mriand ct - based volumes [ 24 , 27 ]  . 
in a study of 57 patients treated by radiosurgery for 72 target volumes , an abnormal uptake of fdg or 11c - met on pet was seen in 86% of the targets , leading to a change in target volume in 69% of these cases compared to mri delineation [ 41 ]  . 
in 36% of these patients , the pet - based volume was fully encompassed with the mri - based volume , while in 18 cases , pet showed a target volume outside the mri - based delineation . using fdg - pet , in 22 out of 27 patients with glioblastoma , the tumor volumes were at least 25% smaller on fdg - pet than on mri [ 69 ]  . 
 da das normale gehirn generell eine hohe fdg - aufnahme zeigt , sind klare unterscheidungen zwischen tumor und normalem hirngewebe schwierig . study confirmed a decrease in mean volumes on fdg - pet as compared to mri ( t1 - weighted images with gadolinium ) [ 24 ]  . by contrast , an increase in gtv with the use of 11c - met in 79% of the patients compared to mri was reported [ 25 ]  . 
a first study comparing patients with recurrent high - grade gliomas reirradiated using 11c - met - pet - based tumor delineation versus ct / mr images for treatment planning showed an improvement in survival [ 27 ]  . 
whether 11c - met - pet - defined tumor volumes for radiation treatment planning and , as a consequence , extended radiation fields will have a significant influence on outcome in terms of overall survival , has to be proven in future studies . additionally , pet can reduce interobserver variability in delineation of brain tumors . 
regions with abnormal tracer uptake ( reported for fdg or fet [ 18f - fluoroethyltyrosine ] ) are at risk for first tumor progression and could therefore be a target for dose escalation [ 59 , 65 , 79 ]  . 
 areas of fet uptake on fet - pet - ct for radiotherapy planning were being observed up to 20 mm outside the area of gadolinium enhancement on mri [ 79 ]  . meningioma a small study of ten patients treated with fractionated stereotactic radiotherapy showed a significant increase of the gtv , when 11c - met - pet was used for tumor delineation [ 26 ]  . 
 68ga - dotatoc - pet delivered additional information concerning tumor extension in all investigated patients planned for fractionated stereotactic radiotherapy of meningiomas [ 46 ]  . in 73% of the patients , the planning tumor volume was significantly modified , and in one patient , no tumor was exactly identified on ct / mri but was visible on pet . another tracer currently being tested is 18f - tyrosine . 
the 18f - tyrosine anomalies completely overlapped with the mr image in 54% , extended beyond the mri lesion in 38% , and were smaller in 8% of the tumors . 
 meningiomas of the skull base are clearly visualized using 18f - tyrosine pet , even after radiotherapy . conclusions fdg - pet is mainly used in brain tumors for definition of tumor grading and prognosis as well as differentiation between recurrence and radionecrosis . 
therefore , the tracer is not very suitable for the imaging of most intracerebral malignancies . for lowand high - grade gliomas and meningiomas , 11c - met or other amino acid tracers such as tyrosine are currently the tracers of first choice in radiotherapy planning . 
performed ct and fdg - pet for radiation treatment planning in 25 patients with esophageal carcinoma ; 18 of the 25 patients also had eus for comparison [ 39 ]  . 
pet - ct detected disease in eight patients that was not detected by ct scan : four of these patients were found to have metastatic disease and four had regional nodal disease . 
in 16 of 21 patients who proceeded to the radiotherapy planning phase of the trial , 69% had pet - ct - positive disease that would have been excluded , if ct alone had been used for radiation treatment planning . do pet scans change the outcome of patients with esophageal cancer treated with radiotherapy ? well - performed fdg - pet improves the selection of patients with esophageal cancer for potentially curative surgery , especially in stages iiiiv [ 76 ]  . 
fdg - pet to target tumors by radiotherapy out increasing side effects , namely because of the reduction of radiation fields . conclusions a well - performed fdg - pet - ct is important to detect distant metastases and hence to select patients suitable for local therapy . 
if validated , the use of fdg - pet might result in a smaller target volume , which would reduce the toxicity or enable radiation dose escalation with the same toxicity . rectal cancer pet for defining tumor volumes ( figure 3 ) nodal target volume studies investigating the role of fdg - pet for the initial staging of rectal cancer suggest that pet is useful in the diagnosis of the primary tumor , but it is of limited value for detecting regional lymph node metastases , with a sensitivity of only about 30% [ 1 , 36 ]  . irradiated volumes should therefore not be reduced based on negative fdg - pet results . 
however , as the positive predictive value was approximately 90% , fdg - pet - positive disease should be included in the irradiated volume . target volume for primary tumor fdg - pet represents the imaging technique of choice to discriminate between benign or malignant tumors of presacral residual postsurgical masses in rectal cancer patients [ 19 ] , although infection can lead to false - positive findings . 
evaluated the value of pet - ct on radiotherapy planning for patients with tumors at several sites , including carcinoma of the rectum ( six patients ) and carcinoma of the anus ( seven patients ) [ 12 ]  . 
 however , even if pet can provide additional functional information , its usefulness in the treatment of rectal cancer is still questionable and needs to be evaluated in prospective trials with strict methodology . 
however , it may become important , when higher doses in relevant biological regions need to be achieved with boost techniques [ 55 ]  . several studies have demonstrated the substantial variability among radiation oncologists in defining the target volume using ct images . 
at the time of writing , it remains unclear as to whether pet - based delineation accurately represents the real macroscopic tumor extension . clinical target volume in general , the current treatment regimens for rectal cancer question the additive value for the use of pet - ct in the definition of the ctv , since the total mesorectum included in the ctv will be surgically removed anyway . do pet scans change the outcome of patients with rectal cancer treated with radiotherapy ? the incorporation of pet in radiotherapy planning has the potential to allow radiation dose escalation without increasing side effects , this because of the reduction of radiation fields . 
 whether this radiation dose increase will ultimately lead to higher cure rates or less surgical resections with , as a result , less complications is a matter of current research . 
a more individualized approach based on early treatment response might have the advantage of a response - adjusted radiation treatment with the goal of more complete tumor responses . this could then help to avoid unnecessary surgical resections , thereby improving outcome and quality of life . 
since pet - ct is able to predict the final outcome , it may be used to guide treatment regimens in the near future , thereby better individualizing treatment while improving the patients outcome . conclusions although fdg - pet - ct is of limited value for detecting regional lymph node metastases , its high positive predictive value may change irradiation volumes . 
in spite of the fact that the current radiotherapy treatment of rectal cancer includes the whole mesorectum , which will be surgically removed anyway , future developments may involve fdg - pet in patient selection suitable for nonsurgical therapy as well as for more sophisticated radiation treatment delivery . lymphoma pet for defining tumor volumes fdg - pet is superior to ct or mri for the staging of both non - hodgkins and hodgkins lymphoma [ 16 ]  . 
early assessment of fdg uptake in the tumor during chemotherapy is highly predictive for subsequent outcome , as is residual fdg avidity after treatment [ 38 , 63 , 82 ]  . 
with the concept of involved - node irradiation in hodgkins disease [ 17 , 22 , 81 ] , increased interest has emerged to include fdg - pet scan information for defining target volumes [ 21 ]  . 
after chemotherapy , the initial fdg - pet helped the delineation of involved - node radiotherapy fields due to the identification of lymph nodes that were undetected on ct in 36% of the patients . 
prechemotherapy fdg - pet data were thus essential for correctly implementing the involved - node radiotherapy concept . do pet scans change the outcome of patients with lymphoma treated with radiotherapy ? no trials have been completed thus far that address this question , but in view of the decreased irradiation volumes [ 81 ] and , at the same time , the decreased probability of geographic miss [ 21 ] , it is very likely that the inclusion of fdg - pet information improves the outcome of patients with hodgkins disease . conclusions in hodgkins disease , fdg - pet is essential for involved - node irradiation and leads to decreased irradiation volumes while also decreasing geographic miss . cervical carcinoma pet for defining tumor volumes ( figures 4 and 5 ) target volume for primary tumor the sensitivity of fdg - pet for detecting local disease ranges between 91% and 100% . 
due to the limitations in spatial resolution , pet imaging is inaccurate for assessing local tumor extension in adjacent structures such as the parametriufor this purpose , mri is the modality of choice [ 7 ]  . nodal target volume due to the small risk of lymphatic spread in early - stage cervical cancer , the sensitivity of pet is low [ 80 ]  . 
fdg - pet to target tumors by radiotherapy head and neck cancer pet for defining tumor volumes in - depth comparison between fdg - pet , mri and ct scans with the histology of resection specimen showed that fdg - pet may be the most accurate of the three for the detection of head and neck cancer [ 52 ]  . 
tumor volume determined by fdg - pet tends to be smaller than the volume determined by the other modalities , but most closely approximates the pathologic tumor volume [ 13 ]  . 
pet - based delineation of the primary tumor is , at present , not ready for clinical routine [ 57 ]  . pet for defining nodal volumes fdg - pet often changes the nodal staging in head and neck cancer [ 56 ]  . 
however , as the results are largely dependent on the pet segmentation tool used , until proper validation with pathology , fdg - pet cannot be recommended for target volume definition of metastatic lymph nodes in routine radiotherapy . do pet scans change the outcome of patients with head and neck cancer treated with radiotherapy ? besides for staging purposes , such as for carcinoma with unknown primary [ 35 ] , for purely radiotherapy purposes , fdg - pet has not shown to be beneficial for head and neck cancer patients . conclusions fdg - pet - defined tumor volumes are more closely related to pathology than those determined by ct and mri , but both overand underestimation still occur . 
die behandlung bestand aus einer tumorresektion , gefolgt von einer konsolidierenden high - dose - rate - brachytherapie auf das tumorbett . the radiation treatment volume and / or total dose in locally advanced disease . do pet scans change the outcome of patients with cervical cancer treated with radiotherapy ? at present , no randomized study has been performed to answer this question . 
however , in view of the detection of otherwise unrecognized nodal disease in the para - aortic region that can be irradiated with curative intent , a significant gain can reasonably be expected . although definite conclusions cannot be drawn yet on determining cutoff values for suvmax ( standardized uptake value ) , integration of suvmax in clinical studies as an additional prognostic marker seems warranted . 
so far , changes in metabolic response observed during treatment did not correlate with survival outcome , whereas posttreatment evaluation seems to be a reliable measure for treatment outcome enabling decision - taking regarding additional salvage treatment . conclusions general conclusions currently , fdg - pet is the imaging modality of first choice for assessing lymphatic spread in locally advanced disease . 
its role in providing additional prognostic information with impact on primary treatment decision - making needs to be evaluated in prospective clinical trials . fdg - pet plays an increasingly important role in radiotherapy , beyond staging and selection of patients . 
especially for nsclc , fdg - pet has led to the safe decrease of radiotherapy volumes , enabling radiation dose escalation and , experimentally , redistribution of radiation doses within the strahlenther onkol 2010 no . 
pet for high - grade gliomas is investigational . for esophageal and rectal cancer , the main advantage of fdg - pet is the detection of otherwise unrecognized lymph node metastases . 
besides for staging purposes , fdg - pet is not recommended for routine radiotherapy delineation purposes . it should be emphasized that using pet is only safe , when adhering to strictly standardized protocols . strahlentherapie und onkologie original article pattern of failure after helical tomotherapy in head and neck cancer ashraf farrag , mia voordeckers , koen tournel , peter de coninck , guy storme1 background and purpose : helical tomotherapy ( ht , hi - art tomotherapy ) is a recently developed radiation device delivering highly conformal dose with a rotational gantry resulting in more uniform target doses and better avoidance of organs at risk . 
 treatment failure patterns in head and neck cancer ( hnc ) patients treated with ht were analyzed . patients and methods : 63 patients with a biopsy - proven hnc were treated with ht . 
future work on dose escalation to the highest risk regions is recommended . key words : helical tomotherapy pattern of failure head and neck cancer strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2130 - 5 rckfallmuster nach helikaler tomotherapie bei tumoren der kopf - hals - gegend hintergrund und ziel : bei der helikalen tomotherapie ( ht , hi - art tomotherapy ) handelt es sich um ein neuartiges bestrahlungsgert , welches mit hilfe einer rotierenden gantry hochkonformale dosisverteilungen erreicht . 
rckfallmuster bei patienten mit tumoren in der kopf - hals - gegend ( hnc ) , die mit ht behandelt worden waren , wurden analysiert . patienten und methodik : 63 patienten mit bioptisch bewiesenen hnc wurden mit ht behandelt . 
mit hilfe der analyse von dosis - volumen - histogrammen ( dvhs ) wurde das vf eingeteilt in in - field ( inf ; innerhalb des ursprnglichen zielvolumens ) , marginal ( mf , randrezidiv ) oder outside - field ( outf , auerhalb des ursprnglichen zielvolumens ) , wenn sich jeweils 95% , 2094% oder < 20% des vf innerhalb der 95% - isodose befanden . ergebnisse : die mediane nachbeobachtungszeit betrug 25 monate ( 95% - konfidenzintervall 19 , 428 monate )  . 
weitere studien ber dosiseskalationen in regionen mit hohem rezidivrisiko werden empfohlen . schlsselwrter : helikale tomotherapie rckfallmuster kopf - hals - tumoren 1department of radiation oncology , oncologic center uz brussel , brussels , belgium . received : february 1 , 2010 ; accepted : february 18 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 urban & vogel farrag a , et al . 
tomotherapy in head and neck cancer introduction treatment of head and neck cancer ( hnc ) with conventional radiation is associated with severe and distressing side effects such as xerostomia , difficulty in speech and feeding with the consequence of impaired quality of life [ 20 , 26 ]  . 
several critical organs , such as parotids , spinal cord and esophagus , are located close to target volumes which make head and neck irradiation challenging , delivering the highest dose surrounding the above - mentioned critical organs . conformal and intensity - modulated radiation therapy ( imrt ) show improvement in target coverage and sparing of normal structures allowing radiation dose escalation and better tumor control [ 2 , 6 , 13 , 29 ]  . helical tomotherapy ( ht ) is a recently developed radiation device delivering highly conformal doses with a rotating gantry [ 18 ] resulting in more uniform target doses and better avoidance of organs at risk ( oars ) due to additional degrees of freedom in radiation entry and exit paths [ 21 ]  . 
it allows precise imrt in standard cases and offers new treatment options in a variety of difficult cases [ 23 ]  . using ht in hnc has led to better sparing of oars , especially parotid glands [ 28 ]  . 
an important question remains : does sparing of critical organs compromises target coverage and patient outcome ? the steep dose fall - off outside the targets volumes can be associated with an increased risk of marginal misses . 
errors in selection and delineation of targets volumes could lead to recurrences outside the conformally shaped planning target volume ( ptv ) [ 27 ]  . to address this issue , treatment failure patterns in hnc patients treated with ht at uz brussel , brussels , belgium , were analyzed . 
the study aim is to investigate the adequacy of target volume definitions and treatment techniques used . patients and methods patient and tumor characteristics between june 2005 and march 2008 , 63 consecutive patients with biopsy - proven hnc were treated with ht ( hi - art tomotherapy , madison , wi , usa ) at the uz brussel . patients were evaluated by history , physical examination , blood count , hepatic and renal profiles , panendoscopy , biopsy , and histopathologic examination . 
radiologic studies such as head and neck computed tomography ( ct ) , magnetic resonance imaging ( mri ) and fluorine - 18 - labeled deoxyglucose positron emission tomography ( fdg - pet ) scan were performed . tumors were staged according to the tnm classification ( 2002 ) [ 11 ]  . 18 patients ( 29% ) received concomitant chemoradiotherapy ( ccrt ; cisplatin 100 mg / m2 , three cycles ) according to the hnc protocol of the department ( age < 65 years , who [ world health organization ] performance status 01 , normal renal function )  . 
treatment planning was based on contrast - enhanced ct images with slice spacing and thickness of 3 m delineation of the primary tumor , pathologic and elective lymph nodes was performed using co - registration of the ct scan with 18fdg - pet scan and / or mri [ 10 , 17 ]  . 
after delineation of the tumor and the pathologic lymph nodes ( = gross tumor volume : gtv1 ) , an expansion of 5 mm , taking anatomic margins such as skin or bone into account , was made ( = clinical target volume : ctv1 )  . 
tomotherapy in head and neck cancer primary tumor crossed the midline or in case of pathologic lymph nodes , the neck was irradiated bilaterally . timation of survival rates [ 15 ]  . 
kaplan - meier - kurven des gesamtberlebens ( os ) und krankheitsspezifischen berlebens ( css ) der 63 patienten . dose prescription radiotherapy was delivered with ht ; a simultaneous integrated boost scheme was used [ 8 ]  . 
note that with tomotherapy the icru reference point cannot be defined and , thus , dose reporting is volume - based . treatment technique the hi - art tomotherapy system is a treatment modality in which imrt is delivered in a helical fashion using a rotating 6 - mv linac and a simultaneously moving couch . 
positioning is integrated into the system by a ct detector mounted opposite of the beam , allowing the treatment beam to acquire a megavoltage ct scan ( mv - ct ) prior to treatment . 
 by co - registration of these mv images to the kilovoltage planning ( kv - ct ) images , positioning based on volumetric imaging is performed resulting in high - precision positioning [ 23 ]  . transfer of failure volume to the planning ct dataset for all patients with local or regional failure , the volume of failure ( vf ) was determined by using one or more diagnostic tools ( ct , mri , and / or pet )  . 
this contoured vf was then co - registered with the initial planning ct . recurrences were categorized as local or regional . the radiation dose delivered to the vf was calculated and analyzed using dose - volume histograms ( dvhs )  . 
in function of the received dose they were classified as in - field failure in which 95% or vf was located within the 95% isodose ( inf ) , marginal failure if 2094% of vf was within the 95% isodose ( mf ) , or outside - field failure if < 20% of the vf was inside the 95% isodose ( outf )  . 
 overall survival ( os ) , disease - free survival ( dfs ) , cause - specific survival ( css ) , locoregional control , and metastases - free survival ( mfs ) were calculated at the time of death , relapse or last follow - up . 
the v95 , v107 , mean , minimum and maximum doses to the ptv1 are given in table 2 . tumor relapse in the head and neck region was observed in 13 patients . 
in more than half of the cases ( n = 7 ) , the primary tumor site was the oral cavity or oropharynx , eleven patients ( 85% ) presented with advanced stage ( iii or iva )  . 
tomotherapy in head and neck cancer in our patient group ( n = 63 ) , surgery ( tumorectomy and / or neck dissection ) preceded radiotherapy in nine cases . distant metastases ten out of 63 patients developed distant metastases . 
the use of chemotherapy failed to show a significant difference in 2 - year mfs ( figure 3 )  . discussion an interesting concern of new radiotherapy techniques is to reduce the dose to normal structures and to decrease complications after radiotherapy . 
although the priority was to cover tumor ptv , doses to critical structures especially parotids and spinal cord were within acceptable ranges . our results are in concordance with reported patterns of failure from other centers where most of the recurrences were in the high - dose region which confirms that ptvs have been adequately chosen [ 1 , 35 , 7 , 24 ]  . the two mfs were seen in patients who underwent surgery before radiotherapy . 
this patient should have been irradiated bilaterally ( t2 sinus piriformis tumor ) to avoid contralateral nodal relapse . in our study , locoregional control at 2 years was 77% which was comparable with other studies using other imrt techniques ( from 69% to 85% ) [ 1 , 3 , 5 , 7 , 24 ]  . 
 [ 24 ] reported that 32% , 59% , and 25% of their patients had postoperative radiotherapy , respectively . a higher 2 - year locoregional control was achieved by daly et al . 
in many clinical cases , the best technique has been found on a patient - to - patient basis [ 16 ]  . the relatively high number of systemic metastases observed must be interpreted with caution . 
 however , the increasing tendency to systemic failure compared with local failure in hnc patients treated with combined chemoradiation was also observed in other studies [ 25 ]  . a recent meta - analysis of chemotherapy in hnc confirmed the benefit of concomitant chemotherapy on locoregional outcome ; on the systemic level ( mfs ) , the use of concurrent chemotherapy did not improve survival [ 19 ]  . 
although this may be due to the relatively small sample size , the question arises regarding the value of chemotherapy when using high - dose intensified radiotherapy as in our technique . 
 [ 22 ] who found that intensified radiotherapy limits the additional benefit of simultaneous chemotherapy . conclusion the majority of locoregional failures were in high - dose regions , i.e. , target definition and coverage were adequate . 
 strahlentherapie und onkologie original article a planning comparison of dynamic imrt for different collimator leaf thicknesses with helical tomotherapy and rapidarc for prostate and head and neck tumors vesna jacob1 , wolfgang bayer1 , sabrina t . 
treatment plans made in rotational techniques ( helical tomotherapy [ ht ] and rapidarc ) were compared with sliding - window imrt ( dimrt ) on a conventional linear accelerator using different leaf thicknesses ( 2.5 mm , 5 mm , and 10 mm )  . 
the influence of the different planning techniques on the coverage of planning volume and sparing of organs at risk ( oars ) was investigated . patients and methods : nine patients with localized prostate and nine patients with head and neck cancer were chosen for this study . 
treatment plans were compared according to target volume coverage and sparing oars , as well as by conformity and homogeneity index . results : for both investigated tumor sites , the dosimetric effects of leaf widths between 2.5 mm , 5 mm and 10 mm were shown to be small in regard to target coverage . 
there was no significant difference ( p > 0.05 ) in sparing of oars between the dimrt plans with different leaf widths neither for prostate cancer nor for head and neck cancer . conclusion : for prostate and head and neck cases , all investigated imrt techniques provide highly conformal treatment plans in terms of both target coverage and critical structure sparing . key words : imrt rapidarc helical tomotherapy prostate cancer head and neck cancer strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2124 - 3 planvergleich zwischen dynamischer imrt fr unterschiedliche leafbreiten , helikaler tomotherapie und rapidarc am beispiel von prostatakarzinom und kopf - hals - tumoren ziel : es wurde eine vergleichsanalyse der drei modernsten fr die photonentherapie kommerziell erhltlichen imrt - techniken ( intensittsmodulierte radiotherapie ) durchgefhrt . 
bestrahlungsplne , die mit rotationstechnik erstellt wurden ( helikale tomotherapie [ ht ] und rapidarc ) wurden mit dynamischer ( sliding - window ) imrt ( dimrt ) fr einen konventionellen linearbeschleuniger mit unterschiedlichen lamellenbreiten ( 2 , 5 mm , 5 mm und 10 mm ) verglichen . 
der einfluss der unterschiedlichen planungstechniken auf parameter fr die zielvolumenabdeckung und die schonung von risikoorganen wurde untersucht . patienten und methodik : es wurden jeweils neun patienten mit prostatakarzinom und mit kopf - hals - tumor fr die untersuchung ausgewhlt . 
 bestrahlungsplne wurden hinsichtlich der zielvolumenabdeckung und der schonung von risikoorganen sowie anhand des konformittsindex und des homogenittsindex verglichen . ergebnisse : fr beide untersuchten tumorentitten war der dosimetrische effekt unterschiedlicher leafbreiten ( 2 , 5 mm , 5 mm und 10 mm ) hinsichtlich der zielvolumenabdeckung gering . 
weder fr prostatakarzinome noch fr kopf - hals - tumoren zeigte sich ein signifikanter unterschied bezglich der schonung der risikoorgane zwischen den dimrt - plnen unter verwendung unterschiedlicher lamellenbreiten ( p > 0 , 05 )  . 1department of radiotherapy und radiologic oncology , klinikum rechts der isar , technical university of munich , germany , 2institute of medical statistics and epidemiology , klinikum rechts der isar , technical university of munich , germany . received : january 18 , 2010 ; accepted : may 28 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 urban & vogel jacob v , et al . 
rapidarc schlussfolgerung : mit allen untersuchten imrt - techniken war es fr patienten mit lokalisiertem prostatakarzinom und fr patienten mit kopf - hals - tumor mglich , hochkonformale bestrahlungsplne mit guter schonung der risikoorgane zu erzeugen . schlsselwrter : imrt rapidarc helikale tomotherapie prostatakarzinom kopf - hals - tumoren introduction an appropriate choice of the irradiation technique may significantly improve the patients quality of life after treatment without compromising the effect on the tumor . 
delivery of imrt is possible using different methods : for example , in slice - by - slice rotational therapy using binary collimation like tomotherapy [ 17 ] or computer - controlled multileaf collimators ( mlcs ) in static ( smlc for segmental mlc ) [ 12 ] or dynamic ( dmlc or sliding - window ) mode [ 16 , 31 ]  . 
another rotational imrt technique was proposed by otto [ 19 ] combining one gantry rotation and aperture changes for intensity - modulated arc therapy ( rapidarc , varian )  . the influence of the mlc leaf width on radiotherapy treatment planning has been studied by several authors . 
 [ 10 ] compared imrt plans between 5 and 10 mm mlc leaf width in three cranial head and neck cases , observing better sparing of parotid gland and optic structures when using 5 - mm leaf mlc . 
they showed advantage of micro mlc in sparing more bladder and rectum . rotational delivery has a number of potential advantages : in being able to deliver radiation from 360 , it may offer more conformal dose distributions relative to imrt using only a limited number of fields and gantry directions . 
by obviating questions of beam number and direction , plan optimization becomes simpler . several studies have been published comparing helical tomotherapy ( ht ) with other imrt modalities [ 2 , 3 , 6 , 9 , 20 , 21 , 23 ]  . 
ht has generally yielded better results in terms of plan quality due to higher target dose homogeneity and superior normal - tissue sparing compared to these static imrt techniques . several planning studies comparing between rapidarc and ht plans [ 2 ] or rapidarc and imrt plans [ 11 ] have been published . 
up to now , there is no study comparing all three imrt techniques for the same patients . prostate and head and neck cancer belong to the cancer sites typically treated with the imrt technique [ 26 ]  . 
the goal of this study is to distinguish strengths and weaknesses of three intensity - modulated delivery techniques : dynamic imrt technique ( dimrt ) with three different mlc leaf width thicknesses ( 2.5 mm , 5 mm , and 10 mm ) , rapidarc and ht for those cancer sites . patients and methods the imrt plans for different mlc leaf widths and rapidarc plans were retrospectively recreated for nine patients with prostate and nine patients with head and neck cancer . 
treatment plan comparisons , according to the target dose coverage and critical structure sparing , were performed . patients all patients were randomly selected from patients with prostate and head and neck cancer that had received radiation therapy treatment between 2007 and 2008 at our department . 
 they were scanned on a helical ct ( computed tomography ) scanner ( siemens sensation 16 , siemens medical solutions , erlangen , germany ) with 3 mm slice thickness . for nine prostate cancer patients , irradiation plans containing a simultaneous integrated boost ( sib ) were generated . 
the prescription dose was 70 gy prescribed to 95% of the ptv70 ( 95% of the ptv70 are getting 70 gy ) , and 76 gy to 95% of the ptv76 ( 95% of the ptv76 are getting 76 gy ) in 35 fractions . nine patients with adjuvant radiotherapy for head and neck tumors were selected . 
the dose was prescribed so that 95% of the ptv are getting 50 gy in 25 fractions . helical tomotherapy planning for each patient , plans were calculated using two jaw widths of 10 mm and 25 mm and a same pitch of 0.287. 
details on the ht optimization process can be found in [ 2 , 21 , 31 ] and references therein . imrt planning the sliding - window imrt plans were generated with seven coplanar equidistant fields of 15 - mv and 6 - mv photons for prostate and head and neck cancer patients , respectively . 
in this work , for prostate cases , primary target volumes and oars were within the central portion of the field , but for the head and neck cases , the whole field was used in order to cover the target . 
optimal beam fluences were converted to mlc files for dynamic sliding - window delivery . treatment - planning parameters , such as isocenter location , number of fields , mlc margin , gantry and collimator angles for each beam , and the prescription dose , were the same for each case . constraints for calculation of the imrt plans were chosen to lead to an optimal solution . 
this set of constraints was selected by multiple planning attempts with the leaf thickness 2.5 mwhen one optimal set of constraints for each patient was found , it was saved as a protocol which was then used for generating plans with other leaf thickness . 
in that way , all three imrt plans were made using the same inverse planning constraint conditions and the same number of iterations was used and this number of iterations was chosen in the way that the result was no further dependent very much on the number of iterations ( i.e. , further iterations have not changed the dose - volume histograms [ dvhs ] )  . target coverage was given the highest priority during treatment planning for all techniques . 
after optimization , the dose distribution was calculated with eclipse using the aaa , with a calculation grid of 2.5 mthe rapidarc plan consists of a single counterclockwise full arc from gantry angles 179 to 181 for prostate cancer patients and of two full arcs ( counterclockwise 179 to 181 and clockwise 181 to 179 ) for head and neck cancer patients . 
for ptv , the minimum ( dmin ) and maximum ( dmax ) doses were calculated as dose received by 98% and 2% of the volume , d98 and d2 , and consequently reported . 
the homogeneity of the treatment was expressed in terms of homogeneity index hi = ( d2 d98 ) / dp ( difference between the dose covering 2% and 98% of the ptv divided with the prescription dose ) [ 30 ]  . 
the degree of conformality of the plans was measured with a conformity index , ci90% , defined as the ratio between the patient volume receiving at least 90% of the prescribed dose and the volume of the ptv [ 8 ]  . 
 for oars , the analysis included the mean dose , the maximum dose , and a set of appropriate vx and dy values : for patients with prostate cancer , values d50 ( dose received by 50% of the volume ) and v70 ( volume that receives 70% of the prescribed dose ) for bladder and rectum were evaluated , and for patients with head and neck cancer , v20 ( volume that receives < 20% dose ) for the left and right parotid were evaluated . beam - on times for dimrt and rapidarc plans were calculated in rt chart , aria ( varian medical systems , palo alto , ca , usa ) , assuming the dose rate of 600 mu / mfor ht , beam - on time were given by the tomotherapy planning software . statistical analysis significance of the difference between results obtained for oars for investigated planning techniques was tested . 
no significant difference in dmean , dmin and dmax could be observed between imrt plans for mlc thicknesses 2.5 mm , 5 mm , and 10 mthe same target coverage was achieved in rapidarc plans , by having the advantage of gradually lower dmax than in dimrt plans . 
the values d50 ( dose received by 50% of the volume ) and v70 ( volume that receives 70% of the prescribed dose ) for bladder and rectum are shown in table 1 for all plans and patients . 
examples of dvhs for bladder and rectum also homogeneity and conformity indices did not differ significantly ( p > 0.05 for both hi and ci ) between dimrt plans with different leaf widths ( table 1 )  . 
summary of mean dosimetric parameters for prostate cancer patients for all plans : averaged minimum ( dmin ) , maximum ( dmax ) and mean ( dmean ) doses for ptv70 and ptv76 ; mean d50 and mean v70 for bladder and rectum , mean homogeneity ( hi ) and conformity indices ( ci ) , mean beam - on time . 
zusammenfassung der mittelwerte der dosimetrischen parameter aller plne fr patienten mit prostatakarzinom : durchschnittliche minimale ( dmin ) , maximale ( dmax ) und mittlere ( dmean ) dosis fr ptv70 und ptv76 ; mittlere d50 und mittleres v70 fr harnblase und rektum , mittlere homogenitts ( hi ) und konformittsindizes ( ci ) , mittlere strahlzeit . 
 dose distribution homogeneity was better for ht plans compared with dimrt and rapidarc plans . dose ( gy ) dose ( gy ) dlmrt 2.5 mm dlmrt 10 mm tomo 2.5 cm dlmrt 5 mm tomo 1 cm figures 1a and 1b . 
dvhs fr ptv70 ( a ) und ptv76 ( b ) eines patienten mit prostatakarzino the beam - on time necessary to deliver the total number of mus for the prescribed dose per fraction for all patients and respective treatment plans are presented in table 1 . 
it has to be considered that the treatment time for dimrt is longer than the calculated beam - on time , as additional time is necessary for moving the gantry to the next position and also for loading the fields . case 2 : head and neck cancer table 2 summarizes the mean target coverage for analyzed head and neck cancer patients . 
no significant difference in dmean , dmin and dmax could be observed between imrt plans for mlc thicknesses 2.5 mm and 5 mthe same target coverage was achieved in rapidarc plans , having slightly lower dmax than in dimrt plans . 
the ht plans generally had the lowest dmax and better ptv dlmrt 2.5 mm dlmrt 5 mm dlmrt 10 mm tomo 2.5 cm tomo 1 cm dose ( gy ) dose ( gy ) dose ( gy ) figures 2a to 2f . 
dvhs fr harnblase ( ac ) und rektum ( df ) fr drei von neun untersuchten patienten mit prostatakarzinom . strahlenther onkol 2010 dose ( gy ) dose ( gy ) dose ( gy ) jacob v , et al . 
summary of mean dosimetric parameters for head and neck cancer patients for all plans : averaged minimum ( dmin ) , maximum ( dmax ) and mean ( dmean ) doses for ptv ; mean v20 for left and right parotid gland , mean maximum dose in spinal cord , mean homogeneity ( hi ) and conformity indices ( ci ) , mean beam - on time . 
zusammenfassung der mittelwerte der dosimetrischen parameter aller plne fr patienten mit kopf - hals - tumoren : durchschnittliche minimale ( dmin ) , maximale ( dmax ) und mittlere ( dmean ) dosis fr ptv ; mittleres v20 fr die linke und rechte speicheldrse , mittlere maximaldosis im rckenmark , mittlere homogenitts ( hi ) und konformittsindizes ( ci ) , mittlere strahlzeit . 
dvh fr ptv eines patienten mit kopf - hals - tumor . looking at the dose to the ptv ( table 2 ) , we found slightly more homogeneous dose distributions in the tomotherapy plans . 
generally , tomotherapy plans show better conformity [ 24 ] which could be of benefit when dose escalation to small subvolumes is desirable . the mean beam - on times necessary to deliver the total number of mus for the prescribed dose per fraction for all patients and respective treatment plan category are presented in table 2 . 
the shortest irradiation times were calculated for rapidarc treatments . discussion the results of this study demonstrate that all used imrt techniques are able to provide highly conformal treatment plans in terms of both target coverage and critical structure sparing for both prostate and head and neck cases . 
we have shown that for both investigated tumor sites , the dosimetric effects of leaf widths between 2.5 mm , 5 mm and 10 mm are small with regard to target coverage as already found in previously reported studies [ 1 , 4 , 14 , 18 , 25 ]  . 
rapidarc the ptv in the dimrt and rapidarc plans is higher than for tomotherapy , although those volumes with higher doses ( hot spots ) are very small . besides the physical and clinical advantages , reduced beam - on times and , consequently , reduced effective treatment times have a strong impact on the clinical routine . for prostate cancer patients , the dimrt and rapidarc plans provide improved sparing of the critical structures , especially for the bladder and rectudimrt and rapidarc show plans of similar quality which is in agreement with previous findings [ 20 , 32 ]  . 
the somewhat worse dvhs for bladder and rectum in both tomotherapy plans could be explained by the fact that tomotherapy beam shape has a helical form which adds doses in oars in the vicinity of the cranial and caudal end of the ptv . in the case of head and neck tumors , the differences in dvhs for ptv and oars are minor for the dimrt plans made with different leaf widths . 
 dose to healthy organs not in the proximity of the ptv arises largely from collimator transmission and scatter radiation from the linac , and this dose is proportional to the number of mus [ 28 ]  . 
the collimator transmission and scatter radiation from the linac are the same for the dimrt and rapidarc plans , but beam - on time is significantly shorter in rapidarc plans . 
the actual physical dose delivered to patients could be affected by many other factors such as beam penumbra modeling , setup uncertainty , organ motions , impact of mlc design on peripheral doses [ 29 ] , source to mlc distance , etc . 
this work is a dosimetric study based purely on treatment planning . in addition , the decreased delivery time of rapidarc plans has the potential to reduce the effects of intrafractional motion by prostate cancer patients , as conventional doses of radiation can be delivered in about 1 min . although beam - on times are shorter for dimrt compared to ht for 2.5 cm jaw size , the irradiation times for prostate plans are comparable for these two modalities , because of additional time needed for dimrt to move the gantry to the next position and to load the fields . 
generally , ht plans with jaw size 1 cm have significantly longer irradiation times , without proportional benefit of sparing oars . conclusion this is the first study that describes the quantitative dosimetric differences in dimrt plans using three different leaf widths , tomotherapy and rapidarc plans . 
the rapidarc technique can reduce beam - on time while maintaining dosimetric quality comparable to that of the dimrt approach . if improvements in dvhs of oars achieved in the investigated planning and irradiation techniques are clinically relevant has to be tested and confirmed through long - term follow - up studies . acknowledgment this work is supported by the project no . 
endres1 , brent parker1 , maria pia sormani2 , giuseppe sanguineti1 background and purpose : to prospectively assess the feasibility and efficacy of an accelerated and hyperfractionated intensity - modulated radiation therapy ( imrt ) schedule for intermediate t - stage oropharyngeal cancer . patients and methods : patients with t3 or unfavorable t2 oropharyngeal squamous cell carcinoma were eligible ; a three - dose level simultaneous integrated boost imrt strategy was used , delivering 78 , 69 , and 60 gy to gross disease , high - risk and low - risk target areas , respectively , in 60 twice daily fractions over 6 weeks . 
 grade 3 mucosal and skin toxicity was 100% and 72% , respectively , none of which persisted beyond 12 weeks ; a percutaneous endoscopic gastrostomy tube was temporarily placed in 60% of patients . 
die mittlere nachbeobachtungszeit betrug 41 , 7 monate ( bereich : 3 , 580 , 8 monate )  . ergebnisse : 25 patienten wurden von 11 / 2002 bis 11 / 2005 behandelt . 
die geschtzte lokoregionale progressionsfreie berlebensrate , die fernmetastasenfreie berlebensrate und die gesamtberlebensrate nach 3 jahren betrugen 86 , 3% 7 , 4% , 76 , 4% 9 , 6% bzw . 
im gleichen zeitintervall lag die aktuarische prvalenz der toxizitt des grads 3 + nach ctcae v3.0 bei 26 , 1% . schlussfolgerung : der routinemige klinische einsatz dieses experimentellen bestrahlungsplans wird nicht empfohlen , er kann aber als basis fr zuknftige entwicklungen dienen . schlsselwrter : oropharynxkarzinom alternierende fraktionierung intensittsmodulierte strahlentherapie 1department of radiation oncology , university of texas medical branch , galveston , tx , usa , 2biostatistics unit , university of genoa , italy . received : october 12 , 2009 ; accepted : march 25 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 urban & vogel gunn gb , et al . 
af - imrt for oropharyngeal carcinoma introduction randomized studies have demonstrated improved locoregional control ( lrc ) [ 23 , 28 , 34 ] and a meta - analysis showed a survival advantage [ 8 ] with altered fractionation ( af ) compared to conventional fractionation ( cf ) radiation therapy for advanced head and neck squamous cell carcinoma . 
af is usually achieved by delivering smaller multiple daily fractions ( mdf ) [ 38 ]  . intensity - modulated radiation therapy ( imrt ) for head and neck cancer has become widely implemented into clinical practice , due to potentially better target volume coverage [ 24 ] while sparing selected organs at risk ( oars ) [ 14 , 20 , 42 , 46 ]  . 
simultaneous integrated boost imrt ( sib - imrt ) plans , which are usually preferred over imrt plans with sequential field reductions due to ease of treatment planning and more conformal dose distributions [ 17 , 33 ] , deliver different doses per fraction to each of the target volumes over the same total number of fractions . 
when considering af with mdf using sib - imrt , the dose per fraction should be > 1.0 gy to be tumoricidal [ 38 ] but small enough not to exceed 14 gy accumulated per week [ 1 ]  . 
patients with unfavorable t2 tumors ( > 3 cm or infiltrative ) were also allowed . patients were ineligible for participation for any one of the following reasons : t1 or t4 tumors ; distant metastases ; previous irradiation in the same area ; concurrent or previous chemotherapy ; previous malignancy . 
 this phase i / ii study was approved by the institutional review board of the university of texas medical branch and all patients provided informed consent . treatment schedule treatment was twice daily definitive sib - imrt alone , without chemotherapy . 
the treatment schedule and radiobiological considerations of af - imrt are summarized in table 1 . imrt planning the gtv ( gross tumor volume ) was identified with the help of the diagnostic imaging studies ( ct [ computed tomography ] + mri [ magnetic resonance imaging ] ) as indicated . 
ptv : planungszielvolumen ; roi : region of interest . group cord + 5 mm 1 cm3 1 cm3 brainstem 1 cm3 brain portion overlapping larynx - 1 with ptv1 portion overlapping with ptv1 1 cm3 mandible - 1 unspecified tissue ptv1 ptv2 ptv3 mucosa parotids larynx - 2 mandible - 2 portion not overlapping with any ptv at least one portion outside ptv1 portion outside ptv1 maximum dose 45 gy maximum dose 54 gy maximum dose 60 gy maximum dose 75 gy maximum dose 84 gy maximum dose 84 gy v95% > 95% v95% > 95% v95% > 95% maximum dose 30 gy v30 gy < 50% maximum dose 70 gy maximum dose 70 gy was manually expanded to ctv1 ( clinical target volume 1 ) at the discretion of the treating radiation oncologist ( g.s. ) [ 40 , 41 ]  . 
ctv2 was a further ( manual ) expansion of ctv1 to cover for possible microscopic extension around primary / nodal disease and / or to cover areas at high risk of containing disease , such as nodal abnormalities not fitting the aforementioned description [ 41 ]  . 
ptv1 / 2 / 3 ( planning target volumes 1 , 2 , and 3 ) were obtained by expanding the corresponding ctv1 / 2 / 3 by 5 mwe considered and contoured the spinal cord ( + 5 mm ) , brain , brainstem , parotid glands , mandible , larynx [ 39 ] , oral mucosa [ 40 ] and unspecified tissue as oars . all treatment planning was performed using the pinnacle3 treatment - planning systetreatment was delivered by a step - and - shoot multileaf collimation technique and 6 - mv photons . 
dose objectives on oars are reported in table 2 . we limited the larynx overlapping ptv1 ( larynx - 1 ) to 75 gy in 6 weeks [ 11 ]  . 
to avoid overdosing of the skin at planning [ 30 ] , we used the pretend bolus strategy as described by thomas & hoole [ 45 ]  . clinical assessments patients were evaluated weekly during treatment and afterwards until acute toxicity improvement . 
posttreatment surgery was considered for bulky , resectable nodes at diagnosis ( > 44.5 cm ) regardless of response or for residual disease [ 37 ]  . patients were followed every 23 months up to 1 year , then every 34 months for 2 more years and every 6 months afterwards , and neck ct imaging was obtained at each follow - up . 
clinical examination at each follow - up visit consisted of palpation of the neck , direct visualization of the oral cavity and oropharynx and laryngoscopy with fiberoptic equipment . statistical analysis for the phase i part , the study was actively monitored for limiting toxicity , which was predefined as sustained confluent mucositis or more resulting in dehydration and poor nutrition unresponsive to tube feeding and break from radiation for up to 2 weeks . 
secondary endpoints included overall survival ( os ) , progression free survival ( pfs ) , distant metastases - free survival ( dmfs ) , and acute and late toxicity rates . actuarial survival curves were generated with the kaplan - meier method . 
pfs was calculated from the 1st day of treatment until the first documented progression ( locoregional and / or distant ) or until death from any cause ; for os , death from any cause was considered an event . the study was designed to accrue 40 patients , based on the null hypothesis that lrpfs at 2 years was 50% versus the alternative hypothesis that lrpfs was 70% . 
the study was closed prematurely mainly due to slowed accrual because of decreased patient load at our institution and data showing benefit of adding cetuximab to radiotherapy [ 7 ]  . 
of 1 , 500 scheduled treatment sessions ( 60 for each patient ) , five ( 0.3% ) were not delivered , all five due to refusal of two patients . 
moreover , 120 treatment sessions ( 8.0% ) were not delivered when scheduled ( average of 4.8 per patient , range : 013 ) , mostly due to machine breakdown , though 16 were recuperated during weekends . time ( months ) figure 2 . 
aktuarische prvalenz der toxizitt bei verschlucken grad 3 + nach ctcae v3.0 ( aspiration , dysphagie , gewichtsverlust ; blaue linie ) und der speicheldrsentoxizitt grad 2 + nach ctcae v3.0 ( rote linie )  . local control was achieved in all but one patient who underwent surgical salvage . 
actuarial prevalence of ctcae v3.0 grade 3 + toxicity ( black line ) versus grade 3 + toxicity or disease relapse ( i.e. , locoregional failure , distant failure , or second malignancy ; blue line )  . 
aktuarische prvalenz der toxizitt grad 3 + nach ctcae v3.0 gegenber toxizitt grad 3 + oder krankheitsrezidiv ( lokoregio nales rezidiv , therapiemisserfolg bei fernmetastasen oder zweittumor )  . [ 10 , 13 , 19 , 25 , 31 , 41 , 43 , 47 ]  . 
 [ 29 ] , we studied exclusively oropharyngeal tumors and used a hyperfractionated approach . acute mucositis was as intense as expected given the dose intensity of this regimen ( table 1 ) and the easily visible anatomic primary site ( oropharynx only ) ; 28% of patients required hospitalization during treatment and 60% a peg tube , which are relatively high rates for an af regimen without chemotherapy [ 5 , 27 ]  . 
despite high rates overall , acute toxicity was manageable and treatment compliance was high , supporting the tolerability of the schedule . what seems more concerning is that 2530% of patients were experiencing grade 3 + toxicity at 2 and 3 years . 
also , the rate of grade 3 + late toxicity of the combined chemoradiation arm of the gortec 94 - 01 trial at 5 years was 82% [ 15 ] , and in a review of three rtog trials , 43% of surviving patients receiving concurrent chemoradiotherapy had severe late toxicity [ 32 ]  . strahlenther onkol 2010 gunn gb , et al . 
kumulatives nominales dosen - volumen - histogramm des unterkiefers bei patienten mit ( rot , n = 5 ) oder ohne ( schwarz , n = 20 ) osteonekrose des kiefers . the statistical approach to report and analyze toxicity can be problematic [ 4 , 9 , 36 ]  . 
moreover , since the majority of acute reactions as well as some late reactions are transient , an approach that describes prevalence rather than incidence would be more appropriate [ 36 ]  . 
by adopting an actuarial approach that computes prevalence [ 35 ] and by using ctcae v3.0 , we were able to estimate the rate of experiencing toxicity among survivors at different time points during and after treatment . six patients in our study developed osteoradionecrosis , five of the mandible and one of c2 vertebral body . 
moreover , we suspect that in our particular patient population , dental extractions shortly after treatment ( one patient ) and poor compliance to fluoride treatment ( three patients ) along with widespread poor oral hygiene and limited access to dental care , may have played a major role as well and this highlights the importance of careful patient selection for similar regimens . 
dissimilarly to bone damage , persistent swallowing toxicity was relatively modest ( figure 3 ) , as all living patients in our study had their peg tube eventually removed . how these data fit with the current standard of care is complicated by the fact that there are multiple options available for intermediate t - stage oropharyngeal cancer [ 7 , 16 , 23 , 27 ]  . 
since oropharyngeal carcinoma is now frequently related to a viral etiology , which may portend a more favorable outcome [ 21 ] , the present schedule seems too aggressive for patients who may have favorable disease and we do not recommend its use in clinical practice . the pattern of failure in this study ( figure 1 ) showed that distant failures were more likely than locoregional failures , highlighting the need for systemic therapy . 
however , we found that grade 3 + toxicity events were more likely than any disease failure ( figure 2 ) , so the therapeutic window for combining additional therapies with this regimen would be relatively small [ 6 ]  . 
the nominal total dose to the gross disease would be 72 gy in 6 weeks , similar to the classic concomitant boost schedule developed at md anderson [ 27 ] , but with the advantages of sib - imrt planning and delivery [ 33 ] and the possibility to explore the addition of systemic treatment as well [ 7 ]  . conclusion we have found that hyperfractionated and accelerated imrt to 78 gy in 6 weeks is feasible and associated with favorable lrc rates for intermediate t - stage oropharyngeal cancer . 
 however , because of its narrow therapeutic window and particularly high rates of osteoradionecrosis , this approach should be considered investigational and the basis for future developments . strahlentherapie und onkologie case study small cell carcinoma of vulva curative multimodal treatment in face of resistance to initial standard chemotherapy franziska eckert1 * , tanja fehm2 , michael bamberg1 , arndt - christian mller1 * background and purpose : extrapulmonary small cell carcinoma ( epscc ) is a rare disease , which has a slightly better prognosis than small cell lung cancer , but still dismal . 
however , of five reported cases of vulvar manifestation only one patient was disease - free at the time of publication with limited follow - up . case report : the authors describe a case of locally advanced small cell vulva carcinoma infiltrating the anal sphincter and urethra with spread to inguinal lymph nodes treated by radiochemotherapy and regional hyperthermia . 
despite the disadvantageous situation with inguinal lymph node metastases and chemoresistance , the multimodal therapy yielded a 5 - year disease - free survival . conclusion : thus , the trimodal regimen of radiochemotherapy plus regional hyperthermia offered a curative chance in spite of resistance to the standard chemotherapy for irresectable , locally advanced small cell carcinoma of the vulva . 
therefore , this approach merits further evaluation for limited disease of epscc . key words : extrapulmonary small cell carcinoma vulva radiochemotherapy hyperthermia strahlenther onkol 2010 ; 186 : 5214 doi 10.1007 / s00066 - 010 - 2160 - z kleinzelliges vulvakarzinokuration durch multimodale therapie bei initialer chemotherapieresistenz hintergrund und ziel : extrapulmonale kleinzellige karzinome ( epscc ) sind eine seltene tumorentitt , die eine etwas bessere prognose als kleinzellige bronchialkarzinome besitzt . 
allerdings war von den fnf beschriebenen fllen kleinzelliger vulvakarzinome zum zeitpunkt der auswertung nur eine patientin mit kurzer nachsorge tumorfrei . fallbericht : die autoren beschreiben den fall einer patientin mit lokal fortgeschrittenem kleinzelligen vulvakarzinom , welches den sphincter ani , die urethra und die inguinalen lymphknoten involvierte . 
trotz der ungnstigen ausgangssituation mit lymphogener metastasierung und fehlendem ansprechen auf die initiale chemotherapie konnte mit der multimodalen therapie ein krankheitsfreies berleben von 5 jahren erreicht werden ( abbildung 2 )  . schlussfolgerung : die trimodale therapie mit radiotherapie , chemotherapie und hyperthermie erffnete trotz der initialen resistenz gegenber der standardchemotherapie einen kurativen ansatz bei einem inoperablen , lokal fortgeschrittenen kleinzelligen vulvakarzinodieses ergebnis kann einen ausgangspunkt fr die diskussion der therapieoptionen von lokal begrenzten epscc bilden . schlsselwrter : extrapulmonales kleinzelliges karzinom vulva radiochemotherapie hyperthermie * both authors contributed equally to the study . 1department of radiooncology , eberhard karls university of tbingen , germany , 2gynecologic clinic , eberhard karls university of tbingen , germany . received : april 4 , 2010 ; accepted : april 21 , 2010 published online : august 30 , 2010 strahlenther onkol 2010 no . 
 in analogy to squamous cell carcinoma of the vulva the tumor would have been staged as t4 n1 m0 . treatment surgery was interdisciplinarily excluded as treatment option because of the infiltration of surrounding anatomic structures . 
therefore , systemic therapy consisting of three cycles carboplatin auc4 ( area under the curve ) d1 plus etoposide 160 mg / m2 d13 was initiated to achieve a downstaging . 
thereafter , however , ct and mri indicated only little regressive transformations but overall stable disease with a tumor size of 53 43 36 min this no change situation , we decided to perform an aggressive radiooncologic treatment consisting of radiotherapy to a total dose of > 65 gy plus simultaneous chemotherapy with cisplatin 40 mg / m2 weekly ( six cycles ) in analogy to the treatment of squamous cell carcinomas of the cervix [ 15 ] and vulva [ 6 ] and due to the high significance of platinum in the therapy of small cell histologies . 
three complete and two circulation - related shortened applications of additional regional radiofrequency hyperthermia were performed with a sigma 60 applicator starting at 500 w with temperature probes ( bladder , vagina , rectum )  . multimodal treatment for limited disease of extrapulmonary small cell carcinoma ( epscc ) eckert f , et al . 
multimodal treatment of small cell carcinoma of the vulva introduction extrapulmonary small cell carcinoma ( epscc ) is a rare disease with a slightly better prognosis than small cell lung cancer ( sclc ) , yet still dismal [ 2 , 20 ]  . 
since squamous cell vulvar and vaginal neoplasms also represent an infrequent disease [ 7 ] , the much lesser experience with small cell carcinomas of that region is evident . in general , the treatment strategy in epscc tends more and more to be adjusted to the standard therapy in sclc [ 19 ]  . 
 most patients are treated with a multimodal approach consisting of platinum - based chemotherapy and local treatment , i.e. , surgery or radiotherapy [ 10 , 12 , 19 ] due to the high frequency of metastases in patients with local treatment only . 
we report the case of a patient presenting with initially chemoresistant , locally advanced small cell carcinoma of the vulva completely responding ( cr ) to radiochemotherapy plus hyperthermia for > 5 years . case report a 49 - year - old female patient presented with assumed bartholinitis . 
a diffuse tumorous infiltration of the whole wound extending to the middle vagina was detected , while bladder and rectal mucosa were not involved . histological finding the biopsy specimen yielded a hyperplasia of squamous cell tissue and an infiltrating , malignant , small cell tumor . 
three complete and two circulation - related shortened applications of additional regional radiofrequency hyperthermia were administered . the initial staging comprised of wholebody computed tomography ( ct ) and magnetic resonance imaging ( mri ) of the pelvis . 
der primrtumor ( ptv ) wurde in shrinking - field - technik bis zu einer gesamtdosis von 65 , 4 gy mit photonen und die leistenlymphknotenmetastasen bis zu einer gesamtdosis von 66 , 4 gy mit elektronen aufgesttigt . 
das mrt vor beginn der chemotherapie zeigte eine > 5 cm groe raumforderung ( a ) , die 3 monate nach abschluss der multimodalen therapie nicht mehr nachweisbar war ( komplette remission ) ( b )  . acute toxicity the patient experienced severe skin toxicity ctc grade 3 ( common toxicity criteria version 2.0 ) requiring analgesics , which completely receded until the first follow - up examination . 
relevant hematologic toxicities did not occur . follow - up and late toxicity the follow - up consisted of initially 3 - monthly and , after 2 years , of semito at least annual gynecologic examinations . 
 3 months after treatment , the tumor had disappeared according to the mri except for a suspicious intravaginal lesion which was clinically related to an infection ( figure 2 )  . 
gynecologic examination including transvaginal ultrasound detected no abnormalities . discussion despite the disadvantageous situation with inguinal lymph node metastases and chemoresistance , the multimodal therapy yielded a 5 - year disease - free survival . 
all other described patients died postoperatively or within 2.5 years [ 1 , 4 , 13 , 18 ]  . the successful treatment combined systemic therapy analogous to sclc with local therapy used in cervical cancer . 
a beneficial effect of additional hyperthermia in combination with radiochemotherapy on epscc was also substantiated for small cell esophageal cancer [ 14 ]  . conclusion this is the first report of small cell vulva carcinoma with a long - term disease - free survival of 5 years treated by an encouraging multimodal concept . 
multimodal treatment of small cell carcinoma of the vulva patients with advanced , inoperable and chemotherapy - refractory limited disease of epscc . strahlentherapie und onkologie original article correlation of patient - related factors and dosevolume histogram parameters with the onset of radiation pneumonitis in patients with small cell lung cancer falk roeder1 , 2 , jochen friedrich1 , carmen timke1 , 2 , jutta kappes3 , peter huber1 , 2 , robert krempien4 , juergen debus1 , 2 , marc bischof1 purpose : to analyze the association of patientand treatment - related factors with the onset of radiation pneumonitis in a homogeneously treated cohort of patients suffering from small cell lung cancer ( sclc )  . patients and methods : 242 patients with sclc staged as limited disease , who had been treated with chemotherapy and three - dimensional conformal radiotherapy , were retrospectively analyzed . 
patient ( age , gender , smoking history , performance status , tumor localization , benign lung disease ) and treatment - related parameters ( v10v40 , mean lung dose [ mld ] ) were analyzed using 2 - tests for categorical parameters and logistic regression for continuous variables . results : 33 patients ( 13.6% ) developed a clinically relevant pneumonitis , of whom three patients died . 
 considering treatment - related parameters , a significant correlation of v30 in regard to total lung and v40 in regard to ipsilateral , contralateral and total lung to the risk of pneumonitis was found . 
in contrast , no significant correlation was found for v10 and v20 and only a trend for mld . conclusion : in this series , high - dose radiation volume parameters , i.e. , v30 and especially v40 , were identified as the most important factors for the development of radiation pneumonitis . 
low - dose radiation volume parameters and clinical parameters played an inferior role in predicting the pneumonitis risk . key words : radiation pneumonitis small cell lung cancer dose - volume constraints strahlenther onkol 2010 ; 186 : 149 - 56 doi 10.1007 / s00066 - 010 - 2018 - 4 korrelation von patientenbezogenen faktoren und dosis - volumen - histogramm - parametern mit dem auftreten einer radiogenen pneumonitis bei patienten mit kleinzelligem bronchialkarzinom ziel : berprfung der assoziation von patientenund therapiebezogenen faktoren mit dem auftreten einer radiogenen pneumonitis in einem homogen behandelten patientenkollektiv mit kleinzelligem bronchialkarzinom ( sclc )  . patienten und methodik : 242 patienten mit sclc im stadium limited disease , welche mittels chemotherapie und dreidimensionaler konformaler radiotherapie behandelt waren , wurden retrospektiv analysiert . 
patienten ( alter , geschlecht , rauchanamnese , allgemeinzustand , tumorlokalisation , gutartige lungenerkrankung ) und behandlungsbezogene parameter ( v10v40 , mittlere lungendosis [ mld ] ) wurden mittels 2 - tests fr kategoriale parameter und logistischer regression fr kontinuierliche parameter analysiert . ergebnisse : 33 patienten ( 13 , 6% ) entwickelten eine klinisch relevante pneumonitis , drei patienten starben . 
fr keinen der patientenbezogenen parameter fand sich eine signifikante korrelation 1department of radiation oncology , university of heidelberg , germany , 2clinical cooperation unit of radiation oncology , dkfz , heidelberg , germany , 3department of pulmonary and respiratory care medicine , thoraxklinik heidelberg , university of heidelberg , germany , 4department of radiation oncology , helios clinic berlin - buch , germany . received : march 18 , 2009 ; accepted : november 26 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
niedrigdosis - volumen - parameter und klinische parameter spielten eine untergeordnete rolle bei der vorhersage des pneumonitisrisikos . schlsselwrter : radiogene pneumonitis kleinzelliges bronchialkarzinom dosis - volumen - grenzwerte introduction combined - modality treatment including radiation therapy is the standard of care in patients with small cell lung cancer ( sclc ) staged as limited disease [ 2 , 13 ]  . 
radiation pneumonitis is a severe complication in thoracic radiation therapy [ 35 , 11 , 16 , 17 , 19 , 20 , 23 , 24 , 26 , 28 ] and develops usually 4 weeks to 6 months after completion of radiation therapy [ 11 , 20 ]  . 
treatment usually consists of steroid and antitussant medication [ 20 ] , whereas the use of antibiotics , oxygen or assisted ventilation is restricted to severe pulmonary dysfunction . since the introduction of three - dimensional ( 3 - d ) conformal computed tomography - ( ct - ) based treatment planning , increasing interest was paid to dose - volume histogram - ( dvh - ) related parameters like vdose ( defined as volume of lung receiving at least the treshold dose ) or mean lung dose ( mld ) [ 11 , 15 ]  . 
however , patients with non - small cell lung cancer ( nsclc ) represent the vast majority of participants in most trials and treatment schedules varied extensively in total dose , fractionation , and timing of chemotherapy [ 15 ]  . 
also multiple scoring systems for severity of pneumonitis have been used in the different trials , which further complicates the comparison of the published results [ 15 , 20 ]  . despite multiple studies conducted in the past , there is only limited data available dealing exclusively with this subject in patients with sclc . 
for these reasons , we analyzed the association of patientand treatment - related factors with the onset of radiation pneumonitis in a homogeneously treated group of patients suffering from sclc . patients and methods we retrospectively analyzed the records of all patients with histologically proven sclc staged as limited disease and treated with sequential chemoradiation in our department from 2000 to 2006 . 
the target volume included the postchemotherapy extension of the primary tumor and the involved lymph nodes , the ipsilateral hilum and the bilateral mediastinal nodes with a safety margin of 1 cin patients with a primary tumor localized in the upper or middle lobe , both supraclavicular fossae were also included . 
all patients were routinely followed in the department of thoracic oncology including clinical examination and chest x - ray or thoracic ct scan 6 weeks after treatment and at least every 3 months afterwards . patient characteristics including age , gender , smoking history , severe benign lung disease ( bronchial asthma or chronic obstructive pulmonary disease [ copd ] requiring medication ) , performance status , and localization of primary tumor were extracted from the medical records . 
pretreatment pulmonary function test data ( pft ) were available in 89% of the patients including forced expiratory volume in 1 s ( fev1 ) and vital capacity ( vc ) , whereas diffusing capacity ( dlco ) had not been routinely assessed . 
treatment characteristics including mld , v10 , v20 , v30 , and v40 ( vx : volume of lung receiving at least x gy ) were extracted from the dvhs for each patient . 
pneumonitis was scored according to a modified rtog ( radiation therapy oncology group ) scale and judged clinically relevant ( grade 3 ) , if at least administration of steroids and hospitalization were necessary . 
according to our policy , patients with radiographic signs of pneumonitis and typical symptoms receive steroid medication and hospitalization at the discretion of the treating physician , usually if an interference with activities of daily living is present . 
this includes not only patients with dyspnea at rest ( grade 3 according to rtog ) , but also patients with dyspnea at normal level of activity ( grade 3 according to ctc [ common toxicity criteria ] or who [ world health organization ] )  . 
for detailed patient and treatment characteristics see table 1 . statistical analysis included analysis of correlations between the rate of clinically relevant pneumonitis and the patient - related parameters using the 2 - test . 
the cumulative incidence is shown in figure 1 . patient - related parameters according to lowand high - dose volumes , the entire cohort was divided into quartiles to achieve groups with equivalent numbers of patients . 
to visualize critical borders , a dvh template showing the v20v40 values corresponding to a 10% , 30% , and 50% risk of pneumonitis was calculated according to willner et al . 
no significant correlations between these parameters and the risk of pneumonitis were observed ( see table 2 )  . treatment - related parameters the correlation of treatment - related parameters v10v40 and mld with the risk of pneumonitis was analyzed via logistic regression for total lung ( see figure 2 ) and separately for the ipsi and contralateral lung . 
 looking at the p - values of all logistic regressions , we found a clear trend to more pronounced correlations between high - dose dvh parameters like v30 or v40 and the rate of pneumonitis , whereas low - dose parameters like v10 or v20 showed only a weak or no correlation at all ( see table 3 )  . 
to compare the pneumonitis rates , we divided the patients into quartiles according to v10 and v40 related to total , ipsiand contralateral lung ( see figure 4 )  . 
we found a distinct increase in the pneumonitis rate for the patients in the fourth quartile of v40 values related to total , ipsiand contralateral lung , whereas no uniform trends were found considering the v10 values . 
 for better visualization of the critical borders in dvh parameters , we transferred the values for a 10% , 30% , and 50% pneumonitis risk estimated by the logistic regression models for v20v40 related to the total lung into a dvh template ( see figure 5 )  . mld ( gy ) figure 2 . 
logistische regression fr mld , bezogen auf das gesamte lungenvolumen . discussion smoked or had quit smoking for more or less than 1 year before diagnosis , but none of the comparisons showed statistically consistent with published results for nsclc our study indicates that dosevolume parameters are associated with the risk of pneumonitis [ 15 ]  . 
of the investigated treatment - related parameters , high - dose values v30 and especially v40 were found to be significantly correlated with the incidence of pneumonitis , whereas an association with low - dose values v10 and v20 was not found . 
using a sigmoid - shaped dose - response curve , relationship between volume - dependent radiation dose and acute lung injury can be modeled ( see figure 3 )  . 
considering an irradiated lung volume in a range of 1030% , pneumonitis risk increased only marginally by 2% for v10 and 7% for v20 , moderately by 16% for v30 , but steeply by 78% for v40 . 
thus , a reduction of lung volume irradiated with doses of > 40 gy seems to be more important in preventing a pneumonitis than a volume reduction in low - dose areas . 
 [ 29 ] , who found a direct relationship between pneumonitis rate and increasing high - dose radiation areas starting from v10 with the best correlation for v40 and other groups [ 1 , 7 , 10 ]  . 
for this reason , an association of lower radiation doses and pneumonitis can be assumed . in daily routine , mld as a parameter integrating dose distribution over the complete lung is frequently used as a constraint for treatment planning . 
analyzing both lungs separately , we found a trend to higher effects of irradiated ipsilateral lung ( p = 0.13 ) , supporting the noted influence of high - dose volumes on pneumonitis incidence in our and other series [ 18 , 29 ]  . 
however , as a mean dose value considering the lung as a whole organ , mld gives no information about ratio or influence of highand low - dose regions . low - dose volume parameters like v20 are also frequently used to estimate the risk of pneumonitis . 
some authors found a strong correlation between v20 and the rate of pneumonitis [ 9 , 14 ] , whereas others described a less pronounced association [ 29 ]  . 
in contrast to our findings suggesting a lower influence of low - dose volumes , even v5 as a predictive factor for pulmonary complications was observed by wang et al . 
in this context , it has to be noticed that a wide variation in the incidences of pneumonitis after thoracic radiation treatment is reported in the literature and obviously the rate itself as well as the threshold recommendations for each of the described parameters are influenced by the reported grade and the scoring system used . 
but even considering the use of the same parameter , similar threshold doses and similar grades of pneumonitis , a marked variation for the risk of pneumonitis can be found in different studies . 
radiation pneumonitis in patients with sclc 1st quartile 1644% 2nd quartile 3rd quartile 4th quartile 5057% 4450% 5778% 27% 79% 912% 1228% 1st quartile 1652% 2nd quartile 3rd quartile 4th quartile 5967% 5259% 6798% 411% 1115% 1521% 2142% 1st quartile 336% 2nd quartile 3rd quartile 4th quartile 4250% 3642% 5976% 02% 23% 35% 522% figures 4a to 4c . 
however , if lower grades of pneumonitis would have been included also into our analysis , it cannot be ruled out , that such a correlation could have been found . 
therefore , our results should not be misinterpreted as a signal to abandon the use of these parameters for risk estimation . however , due to the wide range of studies with different patient groups and a variety in methodology it seems difficult to define only one dose - volume parameter as predictive for pneumonitis . 
if , for example , a 20% risk of severe pneumonitis is considered acceptable , the v30 and v40 should not exceed 26% and 13% of the total lung volume , respectively . the incidence of pneumonitis in our study was 13.6% and comparable to several other series [ 7 , 9 , 10 , 14 , 27 , 29 ] ( see table 4 )  . 
a meta - analysis including five rtog trials found a doubling of pneumonitis events in the patient group treated with simultaneous chemoradiation compared to those treated sequentially [ 6 ]  . 
 [ 25 ] combined data on the incidence of pneumonitis from different studies as a function of v20 and found a dose - response curve twice as steep when radiotherapy was applied with chemotherapy . 
therefore , our results should be interpreted with caution considering risk estimation in patients treated with concurrent chemotherapy approaches . literature data concerning treatment - independent parameters influencing the pneumonitis rate are heterogeneous [ 15 ]  . 
of the investigated clinical factors , we found neither significant differences for patient - related factors like gender , copd , performance status and smoking history nor for disease - related factors like tumor localization . 
a nonsignificant tendency to increased complication rates in patients 63 years could be found in our series ( p = 0.11 ) , accordant with some studies that revealed higher patient age as a possible risk factor for frequency and severity of pneumonitis [ 7 , 22 ]  . however , our study population was similar to other studies concerning multimodal treatment of sclc and did not differ between patient groups with and without pneumonitis minimizing the risk of variation in patientor treatmentstrahlenther onkol 2010 no . 
high - dose radiation volume , i.e. , v30 and especially v40 , were identified in our study as the most important factor for development of radiation pneumonitis . strahlentherapie und onkologie original article simultaneous integrated boost intensity - modulated radiotherapy ( sib - imrt ) in nasopharyngeal cancer evangelia peponi , christoph glanzmann , guntram kunz , christoph renner , katja tomuschat , gabriela studer1 purpose : to assess the efficacy and safety of using simultaneous integrated boost intensity - modulated radiotherapy ( sib - imrt ) to treat nasopharyngeal cancer ( npc ) in a caucasian cohort . 
outcome was analyzed with respect to dose - volume histogram ( dvh ) values . patients and methods : between 03 / 2002 and 01 / 2008 , 39 npc patients underwent sib - imrt ( 37 caucasians ; 31 males ; mean age 53 years [ 1678 years ] )  . 
die resultate werden unter bercksichtigung der dosis - volumen - histogramm - ( dvh - ) werte diskutiert . patienten und methodik : zwischen 03 / 2002 und 01 / 2008 wurden 39 npc - patienten mit sib - imrt behandelt ( 37 kaukasier ; 31 mnner ; im mittel 53 jahre [ 1678 jahre ] )  . 
19 patienten wiesen ein gesamttumorvolumen ( gtv ) von 1670 cm3 ( mittelwert 36 cm3 ) , 16 patienten von > 70 cm3 ( 73217 cm3 ; mittelwert 115 cm3 ) auf . 
alle patienten im stadium iiiv erhielten simultan cisplatin . die sib - dosis auf das boost - planungszielvolumen ( ptv ) betrug 70 gy ( 2 , 00 gy / sitzung ) bei 17 , 69 , 6 gy ( 2 , 11 gy / sitzung ) bei 19 und 66 gy ( 2 , 20 gy / sitzung ) bei drei patienten . ergebnisse : mit einer mittleren verlaufsbeobachtung von 30 monaten ( 871 monate ) lagen die 3 - jahres - berlebensraten fr die lokal - , nodalund fernkontrolle bei 86% , 89% und 85% , das krankheitsfreie berleben und das gesamtberleben betrugen 72% und 85% . 
drei patienten zeigten grad - 3 - spttoxizitt ( xerostomie [ n = 2 ] , dysphagie [ n = 1 ] , schwerhrigkeit [ n = 1 ] )  . 1department of radiation oncology , university hospital , zurich , switzerland . received : april 28 , 2009 ; accepted : october 26 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
sib - imrt in nasopharyngeal cancer schlussfolgerung : im vergleich zur imrt - literatur mit groteils asiatischen populationen fanden sich nach chemo - imrt bei der eigenen kaukasischen npc - kohorte mit groem anteil an radioresistentem who - typ 1 hnliche resultate . 
improvement in technical accuracy and radiotherapy delivery has been linked with improved tumor control [ 36 ]  . various methods have been used to improve local control by increasing the dose delivered , including brachytherapy [ 6 , 37 ] , stereotactic radiotherapy [ 13 ] , three - dimensional conformal radiotherapy [ 39 , 42 ] and intensity - modulated radiotherapy ( imrt ) [ 3 , 22 , 40 ]  . 
imrt allows for the simultaneous delivery of different doses to different target volumes , representing an ideal technique for localized dose escalation [ 26 , 31 ]  . who ( world health organization ) histology type is regarded as an independent prognostic factor for survival in npc , with less favorable prognosis in squamous who type 1 [ 5 , 29 ]  . 
also , patients of asian origin are considered to have improved survival when compared to non - asians [ 2 , 24 ]  . dose - volume histogram ( dvh ) comparison between institutions remains difficult , as there does not yet exist an international standardization regarding contouring definition , prescription dose , volume - related dose distribution and imrt fractionation and dose normalization . we evaluate the outcome and toxicity profile of chemo - sib - ( simultaneous integrated boost - ) imrt in our predominantly caucasian collective characterized by a high proportion of unfavorable who type 1 histology . 
results were analyzed with respect to the dvh values resulting from our sib - imrt dose definition . patients and methods patient , disease and staging characteristics between march 2002 and january 2008 , 39 patients underwent imrt for npc at our department . 
all were staged using the 2002 american joint committee on cancer ( ajcc ) criteria [ 9 ]  . pretreatment evaluation included complete history , physical examination , direct flexible fiberoptic endoscopy , magnetic resonance imaging ( mri ) scans of the nasopharynx , skull base and neck , chest computed tomography ( ct ) or x - ray , laboratory studies , and dental evaluation . 
ct images ( 2 mm slice thickness ) were acquired from the top of vertex to the level of the carina . the target volumes were drawn on each axial planning ct slice , based on diagnostic ct images , supplemented with fused diagnostic mri and / or pet - ct scans . 
ptv3 included the clinically negative bilateral cervical lymphatics down to the supraclavicular fossae ( elective ptv )  . organs at risk were outlined in three dimensions with an estimated planning organ - at - risk volume ( prv ) margin of 210 mm . we used an extended - field imrt ( ef - imrt ) technique , where the primary was treated in one phase along with the regional lymph nodes . 
irradiation was delivered with five or seven coplanar beam angles by a 6 - mv dynamic multileaf collimator ( mlc ) system ( sliding - window technique ; varian medical systems , palo alto , ca , usa )  . 
isodose curves of a five - field inverse plan for a patient with t2 n0 ( stage iib ) carcinoma of the nasopharynx displayed on the axial , coronal and sagittal planes through the primary tumor . 
kaplan - meier - kurven des aktuarischen 3 - jahres - berlebens in bezug auf lokale tumorkontrolle ( lrfs ) , nodale kontrolle ( nrfs ) , fernmetastasenfreies berleben ( dmfs ) , krankheitsfreies berleben ( dfs ) und gesamtberleben ( os )  . 
ad : leben mit erkrankung ; dod : tod wegen erkrankung ; ebv : epstein - barr - virus ; imrt : intensittsmodulierte radiotherapie ; sib : simultan integrierter boost ; tgtv : gesamttumorvolumen ; who : weltgesundheitsorganisation . tnm stage stage grouping who histology grading ( g ) ebv status gender ethnicity tgtv volume ( cm3 ) imrt scheme chemotherapy ( cycles ) patient 1 t2 n2 m0 type 1 female caucasian sib2.11 patient 2 t4 n1 m0 type 1 male caucasian sib2.11 patient 3 t1 n2 m0 type 1 male caucasian sib2.11 patient 4 t3 n2 m1 type 3 male chinese sib2.11 patient 5 t4 n0 m0 type 1 male caucasian sib2.11 patient 6 t4 n2 m0 type 1 male caucasian sib2.00 patient 7 t1 n2 m0 type 3 male caucasian sib2.20 concurrent neoadjuvant / adjuvant local failure ( months post treatment ) nodal failure ( months post treatment ) distant metastases ( months post treatment ) outcome ( months post treatment ) persistence initially m1 ad ( 24 ) ad ( 24 ) ad ( 31 ) ad ( 47 ) dod ( 10 ) dod ( 39 ) dod ( 25 ) dod ( 17 ) patient 8 t2 n1 m0 type 1 male caucasian sib2.11 persistence ( 77% ) completed five to seven concurrent cycles . 
in patients in whom cisplatin was contraindicated , carboplatin was substituted ( n = 3 )  . follow - up institutional standards for posttreatment patient assessment included physical examination with additional fiberoptic nasopharyncoscopy at the department of head and neck surgery approximately every 2 months in the 1st year of follow - up , every 3 months in the 2nd year , every 6 months in the 3rd5th year , and annually thereafter . 
 suspected findings were specified with pet - ct and were histologically proven . normal - tissue effects were graded according to the radiation therapy oncology group ( rtog ) / european organization for research and treatment of cancer ( eortc ) radiation morbidity scoring criteria [ 10 ]  . 
xerostomia was subjectively assessed by the patients . the actuarial 3 - year local relapse - free , nodal relapse - free , distant metastases - free and disease - free rates were 86% , 89% , 85% , and 72% , respectively ( figure 2 )  . 
at the time of analysis , 29 patients were alive with no evidence of disease ( 75% ) , four were alive with local and / or distant disease ( 10% ) , four died of disease ( 10% ) , and two died with intercurrent disease ( 5% ; table 3 )  . prognostic factors univariate analysis was performed to examine the impact of various prognostic factors . 
p - values of 0.05 were considered statistically significant . results treatment outcome and patterns of failure analysis was based on follow - up data available as of january 1 , 2009 . 
at the 12 - month postirradiation follow - up , xerostomia grade 3 was assessed in three patients ( 8% ) , while five patients ( 13% ) experienced xerostomia grade 2 . 
there were no cases of temporal lobe necrosis , clinical optic neuropathy , osteoradionecrosis , severe soft - tissue fibrosis , or clinical hypopituitarism . dose - volume analysis tables 4 and 5 show the dvh statistics for the target volumes . 
additionally , regarding optimal effective dose , there is a controversy in the optimal radiation dose , as , for example , in pediatric npc , presenting mainly with who type 3 histology , it has been shown that radiation doses > 60 gy appear necessary to achieve a high rate of locoregional control [ 41 ]  . table 6 shows the dvh statistics for the critical normal structures organized in series , while table 7 outlines the dvh statistics for the normal tissues organized in parallel . 
 [ 22 ] , which may in part explain the low rate of important late effects in our own series . discussion disease control imrt series with altered fractionation schemes report local control rates of 8498% and overall survival rates of 7492% . 
 however , the local failure rate remains still > 10% in patients with t3 / t4 tumors [ 7 , 15 , 16 , 18 , 22 , 27 , 40 , 43 ]  . in our study , the locoregional failure as well as diseasefree survival and overall survival rates are in the range of one patient developed cisplatin - related ( five cycles concurrently ) grade 3 hearing loss . 
the d50 / dmax values to the right and left middle / inner ear of the patient were 38.1 gy / 56 gy and 34.0 gy / 55 gy , respectively . 
one patient with t4 n1 disease developed dysphagia grade 3 , which still persisted at 24 - month follow - up , when he also remained peg - ( percutaneous endoscopic gastrostomy - ) dependent ; in this case , the caudal border of ptv1 was at the level of the glottic larynx . 
 ( 72% ) [ 20 ]  . postfailure analysis of isodose plans showed that all local recurrences were located within the high - dose volume , suggesting that contoured ptvs and the immobilization system were adequate . 
considering the favorable tolerance profile in our cohort , a careful dose increase may be possible ( besides of other theoretical ways to biologically increase effectivity [ 19 , 23 ] )  . all six patients with n0 status remained nodally controlled . 
as previously described [ 35 ] , in spite of our rather restrictive elective ptv definition regarding level i , none of the nodal recurrences were located in level i . 
 [ 22 ] , improved sparing of normal structures ( parotid , temporomandibular joint , ear ) in our study may in part explain the low rate of important late effects . 
3 brain stem spinal cord chiasm temporal lobes optic nerves right left organ parotid gland right left parotid outside ptv right left right left right left peponi e , et al . 
in the intergroup trial [ 1 ] , this number reached the proportion of only 55% in the adjuvant part , with the most frequently mentioned reason for noncompliance the refusal by the patient to undergo additional treatment and / or toxicity . 
a high level of compliance to chemotherapy seems important , as it has been suggested the addition of chemotherapy confers more benefit for who type 1 tumors than for type 3 tumors [ 30 ]  . conclusion the somewhat lower dose delivered to the high - dose ptv in our non - asian npc patients , presenting with less radioresponsive who type 1 histology and predominantly advanced stage , did not translate into a clearly lower disease control , while likely related to the very satisfactory treatment tolerance . 
a recent article proposed an easy - to - use method for the in - clinic validation of new prediction tools with a limited number of patients , a so - called sequential testing approach . 
the present study evaluates this approach in scores related to radiation oncology . material and methods : three different scores were used , each predicting short overall survival after palliative radiotherapy ( bone metastases , brain metastases , metastatic spinal cord compression )  . 
the positive predictive value ( ppv ) was used for validation of the respective score and it was required that the ppv exceeded 80% . results : for two scores , validity in the own local patient population could be confirmed after entering 13 and 17 patients , respectively ( figures 1 and 3 )  . 
for the third score , no decision could be reached even after increasing the sample size to 30 ( figure 2 )  . conclusion : in - clinic validation of new predictive tools with sequential testing approach should be preferred over uncritical adoption of tools which provide no significant benefit to local patient populations . 
in addition , validation is performed continuously as the data are collected . key words : radiotherapy brain metastases bone metastases prognostic score predictive score strahlenther onkol 2010 ; 186 : 169 - 73 doi 10.1007 / s00066 - 010 - 2095 - 4 ein sequentielles testverfahren zur berprfung neuer prognostischer und prdiktiver scores hintergrund und ziel : klinisch ttige onkologen mssen sich angesichts der neuentwicklung zahlreicher scores und nomogramme fragen , ob diese in ihrer eigenen patientenpopulation valide sind und eingefhrt werden sollen . 
dieses sequentielle testverfahren wird hier fr radioonkologisch relevante scores erprobt . material und methodik : als beispiele dienten drei scores , die ein kurzes berleben nach palliativer strahlentherapie von knochenund hirnmetastasen bzw . 
fr den dritten score konnte selbst nach 30 patienten keine entscheidung getroffen werden ( abbildung 2 )  . schlussfolgerung : die eigene berprfung neuer prdiktiver modelle mittels sequentieller evaluierung sollte der unkritischen einfhrung vorgezogen werden , da nicht alle scores auf alle patientenpopulationen anwendbar sind . 
von vorteil ist auch , dass die validierung kontinuierlich erfolgt , whrend neue patienten behandelt und eingeschlossen werden . schlsselwrter : strahlentherapie hirnmetastasen knochenmetastasen prognosescore prdiktiver score 1radiation oncology unit , department of oncology and palliative care , nordland hospital , bod , norway , 2institute of clinical medicine , faculty of medicine , university of troms , norway . received : october 7 , 2009 ; accepted : november 9 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
for practitioners , the question arises how their own patient population differs from that used in these large - scale analyses and whether or not a new score actually is valid at a local level and thus can be implemented . 
have recently discussed the benefits to be conferred by such local assessment , which might lead to greater confidence in a truly effective tool or to the prudent decision not to use an ineffective model [ 1 ]  . 
have understood this dilemma and proposed an easy - to - use method for the in - clinic validation of new prediction tools with a limited number of patients , a so - called sequential testing approach . 
sequentielle berprfung des scores von mizumoto et al . , der das berleben von patienten mit knochenmetastasen in der wirbelsule vorhersagt . to study the sequential testing approach , three different scenarios were used . 
we identified from our database the first 20 patients irradiated for each of these conditions in our department since its opening in june 2007 , who were predicted to have short survival . 
as described by beam et al . , the positive predictive value ( ppv ; the probability that an individual with a positive test will actually show the condition that the test is designed to detect ) was used for validation of the respective score and it was required that the ppv exceeded 80% . 
those interested in even better performance of a predictive tool might select a higher level . results data lower upper patients with bone metastases and anticipated short survival ( scenario 1 ) typically are candidates for short - course irradiation rather than more costly regimens , which do not result in better pain relief . 
the most unfavorable group ( 1014 points ) had slightly less than 10% 6 - month survival ( points were assigned for age , performance status , type of primary tumor , visceral metastases , number of bone metastases , hypercalcemia and previous chemotherapy )  . 
 table 1 shows the characteristics of our first 20 patients who were irradiated for spinal metastases and assigned 1014 points , i.e. , predicted to have 6 - month survival < 10% . 
3 cording to the formula : cumulative ppv = cumulative number of patients predicted to die within 6 months who actually died cumulative number of patients predicted to die within 6 months . 
using statistical theory to limit the probability of a type i error to be no more than 5% and type ii error to be no more than 20% [ 1 ]  . 
table 1 shows the characteristics of our first 20 patients who were irradiated for brain metastases and assigned 910 points , i.e. , predicted to have 6 - month survival < 10% . 
thus , sequential evaluation in this case is not helpful in evaluating a prognostic tool with a small number of patients . the third example is the score developed by rades et al . , which is supposed to predict survival in patients with mscc [ 7 ]  . 
the score is based on primary tumor type , presence of visceral metastases , presence of additional bone metastases outside of the mscc region , interval from first cancer diagnosis to mscc , ambulatory status and time from onset of symptoms cumulative number of patients with metastatic spinal cord compression and predicted survival < 6 months figure 3 . 
figure 3 shows the sequential evaluation of the ppv of the score in our first 20 patients with 2028 points irradiated for mscc ( characteristics shown in table 1 )  . 
most of them have been developed in large patient populations divided into test and validation sets and are meant to guide decision - making in the upcoming era of personalized medicine . 
nevertheless , patients treated at large , specialized oncology centers or those participating in prospective clinical trials might differ from the general population and those seen by many smallor intermediate - sized oncology practices . 
we have focused on prediction of poor prognosis ( survival < 6 months ) by strictly following the methods proposed by beam et al . , including their ppv of 80% and boundaries set to limit the probability of type i error ( error in hypothesis testing when the null hypothesis is rejected when it is true ) and type ii error ( error in hypothesis testing when the null hypothesis is not rejected when it is false )  . 
in their gleason score example and by us in the three scenarios discussed here should be considered a reasonable compromise rather than optimal solution for all possible scores and nomograms . 
it is also possible to repeat such analyses in order to see whether or not a given score remains valid as patient populations change over time . strahlentherapie und onkologie current discussion pineal parenchymal tumors management with interstitial iodine - 125 radiosurgery mohammad maarouf1 * , faycal el majdoub2 * , christian bhrle1 , jrgen voges1 , ralph lehrke1 , martin kocher3 , stefan hunsche1 , harald treuer1 , volker sturm1 purpose : to evaluate the efficacy of interstitial radiosurgery ( irs ) for pineal parenchymal tumors ( ppts )  . patients and methods : 18 consecutively admitted patients ( twelve male and six female , age range 668 years , median age 34 years ) with ppts ( eight pineocytomas , ten malignant ppts ) were treated at the authors institution with irs using stereotactically guided iodine - 125 seed implantation ( 125i - irs ) as either primary or salvage therapy . 
the median follow - up period was 57.4 months ( range 6134 months )  . results : overall actuarial 5and 8 - year survival rates after irs were 100% and 86% for pineocytomas , and the overall actuarial 5 - year survival rate was 78% for high - grade ppts . 
in malignant ppts , irs may be routinely applied in a multimodality treatment schedule supplementary to conventional irradiation . key words : brachytherapy interstitial radiosurgery pineal parenchymal tumors pineoblastoma pineocytoma stereotactic iodine - 125 seed implantation strahlenther onkol 2010 ; 186 : 12734 doi 10.1007 / s00066 - 010 - 2096 - 3 pinealisparenchymtumoren . 
behandlung durch interstitielle radiochirurgie mittels jod - 125 ziel : die wirksamkeit der stereotaktischen interstitiellen radiochirurgie ( irs ) zur behandlung von pinealisparenchymtumoren ( ppts ) wurde analysiert . patienten und methodik : 18 patienten ( zwlf mnnlich und sechs weiblich , alter 668 jahre , medianes alter 34 jahre ) mit einem ppt ( acht pineozytome , zehn maligne ppts ) wurden in der klinik der autoren durch eine stereotaktisch gefhrte interstitielle radiochirurgie mittels implantation von jod - 125 - seeds ( 125i - irs ) behandelt . 
 aufgrund der geringen nebenwirkungen kann sich diese behandlung zu einer guten alternative zur mikrochirurgie bei de novo * both authors contributed equally to the study . 1department of stereotactic and functional neurosurgery , university of cologne , germany , 2department of general neurosurgery , university of cologne , germany , 3department of radiation oncology , university of cologne , germany . received : october 9 , 2009 ; accepted : november 26 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
bei malignen ppts kann diese methode als ergnzung in ein multimodales behandlungskonzept einbezogen werden . schlsselwrter : brachytherapie interstitielle radiochirurgie pinealisparenchymtumoren pineoblastome pineozytome stereotaktische jod - 125 - seed - implantation introduction pineal region tumors ( prts ) are a very heterogeneous group comprising four main categories : germ cell tumors , pineal parenchymal cell tumors ( ppts ) , glial cell tumors , and other miscellaneous tumors and cysts . 
prts are rare and account for < 1% of the primary brain tumors in western countries , and for 2.28% of intracranial tumors in countries of northeastern asia [ 5 ]  . 
 in the world health organization ( who ) classification from 2007 [ 23 ] , ppts are divided into pineocytoma who grade i ( pc ) , ppt with intermediate differentiation who grade iiiii ( pttimd ) , and pineoblastoma who grade iv ( pb )  . according to the brain tumor registry of japan [ 1 ] , pineocytomas mostly develop in adults . 
by contrast , pineoblastomas were recognized more often in children ( 51% of the patients in this registry )  . ppts usually cause an occlusive hydrocephalus by obstruction of the cerebral aqueduct , as well as parinauds syndrome due to tectal compression . pineocytomas and pineoblastomas share the same anatomic region , but differ in biological behavior , metastatic potential and therapeutic requirements . 
patient characteristics regarding histology , extent of resection , additional treatment prior to interstitial radiosurgery ( irs ) , extent of disease at the time of irs , and additional treatment after irs . 
at the time of irs , only two patients , who underwent primary stereotactic biopsy , showed evidence of spinal seeding on staging magnetic resonance imaging ( mri ) scans ( two patients with a pineoblastoma )  . 
table 1 details the patients with their respective histology , extent of resection , additional treatment prior to irs , extent of disease at the time of irs , and additional treatment after irs . the management of these tumors remains unclear . 
the literature recommends a variety of treatment approaches , regardless of the disease stage , ranging from surgery or external irradiation alone to combined treatment with surgery , radiotherapy or chemotherapy [ 5 , 6 , 18 , 24 , 26 , 33 ]  . 
moreover , a number of techniques are recommended , from stereotactic biopsy to complete tumor resection for surgery , and from radiosurgery to craniospinal irradiation for radiotherapy [ 5 , 14 , 16 , 22 , 24 , 32 ]  . it was the objective of this retrospective study to determine the efficacy and safety of interstitial radiosurgery ( irs ) using stereotactically guided iodine - 125 seed implantation ( 125i - irs ) for ppt as either primary or salvage therapy . patients and methods patients between april 1992 and december 2003 , 18 consecutively admitted patients with ppts were treated at our institution . 
all patients ( male / female ratio 12 / 6 , median age 34 years , range 668 years ) had a follow - up of at least 6 months and were considered for the following evaluation . the cohort presented here included four children aged 6 , 11 , 12 , and 15 years . 
4 / 6 patients of the open surgery group underwent an adjuvant all patients were treated with irs using computed tomography ( ct ) and mri as a basis for stereotactic planning and guiding 125i seed implantation as either primary ( n = 12 ) or salvage ( n = 6 ) therapy . 
the median tumor volume was 6 cm3 ( mean 7.8 cm3 , range 0.428.1 cm3 ) , and the median time between diagnosis and irs was 3.3 months ( range 0114 months )  . according to our treatment schedule for gliomas [ 21 , 36 ] , pineocytomas and ppts with intermediate differentiation received permanent implants . 
an adjuvant fractionated radiotherapy was applied in patients with ptt with intermediate differentiation ( brain , range 2536 gy , 1.8 gy / day ) and in patients with pineoblastoma ( craniospine , 36 gy , 1.8 gy / day , with a 50 - gy boost in spinal metastatic disease )  . 
young pineoblastoma patients were also treated by systemic chemotherapy as displayed in tables 1 and 2 . technical data 125i seeds ( amersham buchler gmbh & co kg , braunschweig , germany ) were used in both permanent and temporary implants . 
in patients receiving permanent implants , a cumulative tumor surface dose of 4065 gy was applied at a median initial dose rate of 0.74 gy / day ( mean 0.67 gy / day , range 0.460.74 gy / day )  . 
in temporary implants , 4050 gy were given at a median initial dose rate of 0.75 gy / day ( mean 0.92 gy / day , range 0.571.44 gy / day , table 2 )  . 
the therapeutic isodose curve was prescribed to the surface of the tumor defined on mri and stereotactic ct ( figure 1 )  . during autoclavation of the seeds , the stereotactic device was built up and the burr hole was made . 
an outer nylon catheter ( outside diameter 2.0 mm ; best industries , inc . , springfield , va , usa ) was placed stereotactically and loaded with an inner catheter where the 125i seeds had been placed . 
gesamtberleben nach kaplan - meier aller 18 pptpatienten ( acht pineozytome , drei ppts grad iii , sieben pineoblastome ) , welche mittels stereotaktisch gefhrter 125i - irs behandelt wurden . follow - up after irs , clinical follow - up data were obtained from the patients and the referring physicians for a median period of 57.4 months ( mean 66 months , range 6134 months )  . 
tumor response was classified according to the macdonald criteria [ 25 ]  . results all of the 30 stereotactically guided procedures ( 19 125i seed implantations and eleven biopsies ) were performed without perioperative complications . pineocytoma group ( n = 8 patients ) after a median clinical follow - up of 105 months ( range 6124 months ) , 50% of the patients ( n = 4 ) were free of symptoms . 
mr images ( median follow - up of 87 months ) showed a complete remission in 50% of the patients and a partial remission in the remaining 50% ( figures 4a and 4b )  . 
one patient with a recurrent pineocytoma after surgery and fractionated radiotherapy was treated with temporary irs ; 4 years after partial remission , he showed an out - of - field recurrence , necessitating a second irs , with a local tumor control for 3 years . 
the second patient , a 6 - year - old boy , who had had previous surgery , polychemotherapy , craniospinal radiotherapy and irs for a distant figures 3a and 3b . 
follow - up mri of an 11 - year - old boy with a pineoblastoma prior to irs ( a ) and complete tumor remission 5 years after irs ( b )  . 
concomitantly , mri displayed substantial global brain atrophy 2 years after conformal irs and external - beam irradiation . with a median follow - up of 28 months ( range 6112 months ) , mr images showed complete local remission in 90% of cases and partial remission in 10% ( figures 3a and 3b )  . 
two patients with an initially seeding pineoblastoma showed complete local remission but tumor spread 4 and 20 months , respectively , after irs : in one patient two metastases occurred in the right cerebellopontine angle and in the left cavernous sinus , which were treated with linac radiosurgery and chemotherapy . 
the overall actuarial 5 - year survival rates after irs were 78% ( figure 2 )  . discussion the current results show the considerable safety and efficacy of 125i - irs for the treatment of patients with pineocytoma , ppt with intermediate differentiation , or pineoblastoma . 
with a comparably high median follow - up of > 7 years , all patients showed either complete tumor remission ( 50% ) or partial remission ( 50% )  . 
 four of eight patients ( 50% ) were free of symptoms after irs , and another four showed improved or stable clinical status . also the high - grade ppts ( pttimd and pb , n = 10 ) responded to irs resulting in a high overall actuarial 5 - year survival rate ( 78% )  . 
in case of the third patient ( 6 - year - old boy treated with surgery , polychemotherapy and craniospinal radiotherapy prior to irs ) who developed a slowed motor output and deficient cognitive functions , we assume that the deficits are not related to irs due to the location of the implants in the cerebellum . interstitial brachytherapy for the treatment of malignant diseases is well established [ 7 , 12 , 27 , 28 , 30 , 34 , 37 , 38 ] but reports in the literature addressing interstitial irradiation of these tumors using stereotactic 125i seed implantation are rare . 
the pineocytoma patients ( n = 4 ) had a median follow - up of 41 months , and a local tumor control rate of 100% [ 22 ]  . 
thus , our results are well comparable with those of most contemporary series . however , the definitive therapy of these tumors remains controversial and is generally complicated by their anatomic location adjacent to the midbrain and the deep venous syste the literature recommends different treatment schedules regardless of the disease stage , from surgery , external irradiation or radiosurgery alone to combined treatment with surgery , radiotherapy and chemotherapy . 
contemporary studies report a surgical mortality rate of 47% [ 1 , 5 ] , and the permanent morbidity rate may be as high as 10% [ 5 , 11 ]  . 
although complete surgical resection is only feasible in the minority of cases , recurrences are observed more often than expected from the histological diagnosis of this type of tumor . another treatment option for ppt patients is externalbeam irradiation [ 17 , 20 , 24 , 33 ]  . 
although the efficacy of external - beam irradiation for pineocytoma remains controversial , malignant ppt requires fractionated radiation with a field that includes the ventricular syste a retrospective study on 30 ppt patients ( nine pineocytomas , six ppts with intermediate differentiation , 15 pineoblastomas ) revealed that fractionated radiotherapy , applied primarily or as an adjuvant postoperatively , can control the tumor and increase survival . 
in our study , 2 / 3 patients with initially seeding pineoblastoma showed complete local remission , but distant tumor spread became obvious at 4 and 20 months , respectively . 
thus , initial staging should include examination of the csf and an mri of the spine . the main advantage of irs over conventional radiotherapy is the reduction of the radiation dose to surrounding normal brain while augmenting the radiobiological effect on the tumor volume . 
compared with the results of external radiotherapy for ppts ; our results demonstrate a significantly higher local tumor control rate ( 100% ) with a quite considerable complete tumor remission of 72% and also an increase of survival . a further treatment option is systemic chemotherapy , but its benefits after craniospinal irradiation remain unclear [ 6 , 10 , 17 ]  . a relatively new therapeutic option for ppt is radiosurgery using gamma knife or linear accelerator [ 8 , 9 , 15 , 16 ]  . 
however , for final conclusions longer follow - up periods are required . conclusion irs for ppts has obvious advantages because of its minimal invasiveness , its ability to provide high local tumor control , and its low incidence of treatment - related morbidity . 
hence , stereotactic irs might be an attractive alternative to microsurgery as a safe approach for treating ppt patients , as a primary therapy for small pineocytomas , as salvage therapy after microsurgical decompression of gross symptomatic tumor , and as one arm of a multimodal therapy including conventional irradiation for malignant ppts ( ppts with intermediate differentiation and pineoblastomas )  . 
on the basis of this study , stereotactic management for ppts can be advocated . strahlentherapie und onkologie original article ct density in lung cancer patients after radiotherapy sensitized by metoclopramide a subgroup analysis of a randomized trial einar dale1 , 2 , vanja hrsaker3 , doris t . 
metoclopramide and significant radiation doses to larger lung volumes ( v40gy ) seemed to protect against fibrosis development . key words : radiotherapy lung cancer late toxicity computed tomography strahlenther onkol 2010 ; 186 : 163 - 8 doi 10.1007 / s00066 - 010 - 2040 - 6 ct - dichte von patienten mit bronchialkarzinom nach strahlentherapie in kombination mit strahlensensitivierender metoclopramidbehandlung . 
subgruppenanalyse einer randomisierten studie ziel : computertomographische ( ct ) messung der strahlenreaktion in lungengewebe nach strahlentherapie in kombination mit metoclopramid . patienten und methodik : patienten mit nichtkleinzelligem bronchialkarzinom ( tumorstadium iiia und iiib ) , die in eine randomisierte , multizentrische phase - iii - studie zur untersuchung des strahlensensitivierenden effekts von metoclopramid eingeschlossen waren , wurden mittels wiederholter posttherapeutischer cts untersucht . 
verlaufskontrolldaten bis 100 tage nach beendigung der strahlentherapie einer untergruppe von 16 patienten , die mit einer gesamtdosis von 60 gy , appliziert in tagesdosen von 1 , 82 gy , behandelt wurden , standen fr die analyse zur verfgung . ergebnisse : hohe strahlendosen auf teilvolumina resultierten in hherer ct - dichte im bestrahlten lungengewebe ( p < 0 , 001 )  . 
 im gegensatz dazu korrelierte das mit signifikanter dosis bestrahlte lungenvolumen ( v40gy ) negativ mit der zunahme der ctdichte im bestrahlten lungengewebe ( p = 0 , 003 )  . 
bei patienten , die in den therapiarm mit metoclopramid randomisiert wurden , war eine weniger ausgeprgte zunahme der ct - dichte im bestrahlten lungengewebe zu verzeichnen ( p = 0 , 01 )  . schlussfolgerung : es fand sich ein zusammenhang zwischen der zunahme der gemessenen ct - dichte im bestrahlten lungengewebe , der applizierten strahlendosis und der zeit nach bestrahlung . 
metoclopramid und das mit signifikanter dosis bestrahlte lungenvolumen ( v40gy ) scheinen einen protektiven effekt auf die entwicklung einer lungenfibrose zu haben . schlsselwrter : strahlentherapie bronchialkarzinom spttoxizitt computertomographie 1institute for cancer research , oslo , norway , 2cancer clinic , rikshospitalet - radiumhospitalet medical center , oslo , norway , 3oslo university college , norway , 4norwegian knowledge center for the health services , oslo , norway , 5university of oslo , norway . received : june 2 , 2009 ; accepted : december 12 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
ct density after radiotherapy of lung cancer introduction in patients with localized , inoperable non - small cell lung cancer ( nsclc ) , radical radiotherapy ( rt ) is the treatment of choice . 
since radical rt may be limited by consequential pneumonitis and lung fibrosis , a better understanding of the relationship between the radiation dose and the development of late side effects is needed [ 3 , 4 , 12 , 17 ]  . 
previous studies have established computed tomography ( ct ) as a tool to monitor the development of fibrosis / pneumonitis measured as changes in ct density [ 9 , 10 , 19 ]  . 
dose - effect relationships have been derived for breast cancer and lymphoma patients [ 1 , 18 ] , and for patients with lung cancer [ 13 , 15 ]  . 
some authors have chosen to investigate populations of breast cancer and lymphoma patients , partially because of the well - known obstacles related to investigations of late side effects in lung cancer patients [ 2 , 18 ] : first , the survival of lung cancer patients is low , and consequently , the patient materials are of low figures , and may thus be highly selected . 
nevertheless , certainly also for this patient group , further investigations on post - rt side effects are justified . the enzyme adenosine diphosphate ribosyl transferase is activated by dna - damaging agents . 
a phase i / ii study indicated that metoclopramide could be used safely as a radiosensitizer and that the drug could have positive treatment effects [ 8 ]  . in this retrospective study , the results from an analysis on our institutions follow - up data from a multicenter , randomized phase iii study are presented . 
 patients and methods during 19951998 , 30 nsclc patients from our institution were enrolled in a multicenter , randomized phase iii study aimed at investigating the efficacy , safety and tolerability of intramuscular injections of neutralized metoclopramide 100 mg / ml ( neu - sensamide ) as a radiosensitizing agent [ 6 ]  . 
 neu - sensamide was produced by oxigene europe ab . inclusion criteria were inoperable nsclc , squamous cell carcinoma , stage iiia and iiib , age > 30 years and karnofsky performance scale 80 . 
no follow - up data have been published from the central study group . 16 of the 30 patients from our hospital had sufficient data for a local analysis , i.e. , complete rt records and ct examinations . 
the remaining 14 patients had insufficient follow - up data ( partly because of withdrawal from the study related to rapid disease progression during or shortly after rt and partly because of inadequate rt files )  . radiosensitizer seven patients were randomized to receive intramuscular injections of neutralized metoclopramide , 2 mg / kg given 1 h prior to rt , three times per week . 
four patients complied with the protocol , one patient was not given the sensitizer the last week , and two patients refused to continue with the sensitizer after few injections due to side effects ( fatigue , muscle pain , headache , and indigestion )  . radiotherapy all patients were given megavoltage ( 615 mv ) conformal rt applying two to four , usually three , radiation fields . 
the rt dose planning was performed with treatment management system v3.1 ( helax ) based on ct scans acquired with 10 mm slice thickness and 10 mm distance between the slices . 
after advice from our statistician ( d.t.k. ) , we chose to set a cut off at 100 days when plotting the data and 90 days for the statistical analysis . 
normally , the slice thickness was 5 mm . we chose to present radiation - induced alterations in lung tissue density as changes in the air - filled fraction ( fair ) according to [ 18 ] : strahlenther onkol 2010 no . 
ct density after radiotherapy of lung cancer air = 1 = 0.001 nct , where is the electron density relative to water and nct is the measured ct number in hounsfield units . 
vois identified normal lung tissue in regions of homogeneous dose close to the tumor and were delineated on three adjacent ct slices with the middle slice containing the icru central axis dose . 
the overall mean ct number of the voi was obtained from multiple small circular areas covering the voi ( figure 1 )  . ideally , the fair obtained after rt should have been normalized according to the individuals baseline value obtained prior to rt ( pre - rt )  . 
unfortunately , it was not possible to obtain the baseline ct numbers from the images in the rt planning systetherefore , the fair was normalized according to a global fair of 0.802 , the mean fair from all lung vois receiving a radiation dose < 8 gy . 
a repeated measurement analysis of variance was undertaken using the highest radiation dose ( > 40 gy ) to the voi for each time interval , whether radiosensitizer dose was administered or not , ct post - rt examination time , and voi location ( central , anterior , posterior ) as explanatory variables . p - values from two - sided tests are presented , and should be considered hypothesis - generating as no power calculations had been performed for the comparisons reported in this paper . 
wenn prtherapeutische ct - daten fehlen , ist die relative reduktion der fair ( air - filled fraction ) der gruppe < 8 gy , wie auch in unserer aktuellen studie , im verhltnis zur mittleren hounsfield - einheit normalisiert . 
the reduction in fair increased with radiation dose ( p < 0.001 ) , and the effect was more pronounced for those patients not given metoclopramide ( p = 0.01 ; figure 3 )  . 
im fall von > 1 voi wurde die mittlere fair verwendet . discussion in the present study , we found that the density change ( ) in the lung , measured as an air - filled fraction ( fair = 1 ) change , was dependent on radiation dose . 
the relative reduction in air - filled fraction ( fair ) averaged over voi > 40 gy and time 50100 days , as a function of v40gy , the normal lung volume fractions irradiated with > 40 gy . 
relative reduktion der fair ( air - filled fraction ) fr voi > 40 gy und zeit 50100 tage als funktion von v40gy , normales lungenvolumen mit > 40 gy bestrahlt . 
pearson - korrelationskoeffizient r2 = 0 , 56 ( n = 13 )  . ed with > 30 gy was denser 50100 days after treatment compared to tissue irradiated with smaller doses ( figure 3a )  . 
found a threshold for physician - identified radiographic fibrosis at 3035 gy , but significant density changes were also detected for smaller doses [ 13 ]  . opposed to the positive correlation between local radiation dose to smaller lung volumes , there was a negative correlation between the normal lung volumes irradiated with significant doses ( v40gy ) and the reduction in fair . 
a possible explanation is an antitumor effect of the rt making the conditions for the normal lung tissue more favorable . the ct examinations were performed at various time points after rt but due to the limited patient number , an exact quantification of the relationship between reduction in fair and time was not possible . 
their explanation was a gravity - dependent density gradient causing a relative increase in lung mass ( edema ) in the posterior region after irradiation . there was a statistically significant association between high doses of metoclopramide , and the least reductions in fair . 
 a possible explanation for the relationship between metoclopramide dose and fair is an antitumor effect similar to the negative correlation between normal lung volumes encompassed by the 40 gy isodose ( v40gy ) and the reduction in fair . 
the tumors were mostly centrally located ( stage iiia and iiib ) , and the patients enduring the drug treatment , could get increased blood perfusion and airflow to the neighboring normal tissues in the lung . 
we also thank martin turzer for excellent assistance with the manuscript . strahlentherapie und onkologie original article quantitative assessment of irradiated lung volume and lung mass in breast cancer patients treated with tangential fields in combination with deep inspiration breath hold ( dibh ) brigitte zurl , heidi stranzl , peter winkler , karin sigrid kapp1 purpose : comparison of the amount of irradiated lung tissue volume and mass in patients with breast cancer treated with an optimized tangential - field technique with and without a deep inspiration breath - hold ( dibh ) technique and its impact on the normal - tissue complication probability ( ntcp )  . material and methods : computed tomography datasets of 60 patients in normal breathing ( nb ) and subsequently in dibh were compared . 
with a real - time position management respiratory gating system ( rpm ) , anteroposterior movement of the chest wall was monitored and a lower and upper threshold were defined . 
ntcp for lung was calculated using a modified lyman - kutcher - burman ( lkb ) model . results : mean dose to the ipsilateral lung in dibh versus nb was significantly reduced by 15% . 
the correlation of individual breathing amplitude with ntcp proved to be independent . conclusion : the delineation of a restricted area provides the lung mass calculation in patients treated with tangential fields . 
 dibh reduces ipsilateral lung dose by inflation so that less tissue remains in the irradiated region and its efficiency is supported by a decrease of ntcp . key words : breast cancer lung dose deep inspiration breath - hold technique ntcp strahlenther onkol 2010 ; 186 : 15762 doi 10.1007 / s00066 - 010 - 2064 - y quantitative bestimmung von lungenvolumen und - masse von brustkrebspatientinnen bei einer bestrahlung mit tangentialen feldern unter einsatz einer luftanhaltetechnik in tiefer inspiration ( dibh ) ziel : vergleichende bestimmung von bestrahltem lungenvolumen und bestrahlter lungenmasse in normalatmung ( nb ) und tiefer inspiration ( dibh ) bei patientinnen mit brustkrebs , die mit tangentialen feldern bestrahlt wurden , und ihrem einfluss auf die normalgewebskomplikationswahrscheinlichkeit ( ntcp )  . material und methodik : computertomographiedatenstze von 60 patientinnen wurden in nb und dibh miteinander verglichen . 
die ntcp fr die lunge wurde mit einem modifizierten lyman - kutcher - burman - ( lkb - ) modell errechnet . ergebnisse : die mittlere ipsilaterale lungendosis war in dibh gegenber nb signifikant um 15% reduziert . 
die mittlere lungenmasse ( errechnet nach tabelle 1 ) , die 20 gy ( m20 ) erhielt , war in dibh um 17% reduziert , whrend das lungenvolumen deutlich vergrert war ( tabelle 2 )  . 
der zusammenhang der individuellen atmungsamplitudenzunahme zwischen nb und dibh mit dem vergrerten lungenvolumen konnte dargestellt werden ( abbildung 2 ) , whrend keine korrelation zwischen der individuell erreichten atmungsamplitude mit der ntcp aufgezeigt werden konnte ( abbildung 3 )  . 
bei tiefer inspiration verbleibt ein geringerer anteil an lungengewebe im feld und fhrt zu einer reduktion der ipsilateralen lungendosis , untersttzt durch eine abnahme der ntcp . schlsselwrter : brustkrebs lungendosis atemtriggerung ntcp 1university clinic of therapeutic radiology and oncology , medical university of graz , austria . received : july 15 , 2009 ; accepted : november 26 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
irradiated lung mass in breast cancer introduction in patients with left - sided breast cancer treated with tangential fields in combination with a deep inspiration breath - hold ( dibh ) technique , a decrease of the dose to the heart by increasing the distance from the chest wall has been shown [ 12 ]  . 
 a reduction of absolute volume and dose may translate into a reduction of late effects of radiation and radiation in combination with neoadjuvant , concomitant , or adjuvant cardiotoxic systemic agents ( e.g. , chemotherapy , biologicals ) [ 11 , 27 , 28 ]  . the probability of pulmonary side effects is linked to lung dose , fraction dose and volume [ 13 , 17 ] , but its clinical significance has been shown to correlate with lung mass . 
it has to be kept in mind , however , that a dibh technique increases the volume of lung receiving varying doses , which may drain the gain , if one postulates that volume / dose is the dominant risk factor for lung tissue damage . lung dose calculation in low - density tissue proved to be a challenge for treatment - planning systems , which was discussed in studies implementing lung density corrections [ 2 , 23 ] along with its impact on the prescribed target dose . 
when lung is voluntarily expanded , its density decreases and not volume but irradiated lung tissue mass becomes the predominant parameter to assess the radiation dose applied , irrespective of technique . the purpose of our study was to analyze the amount of irradiated lung mass in a dibh versus normal breathing ( nb ) mode and to quantify the applied doses with the tools a commercial treatment - planning system provides . to the best of our knowledge , this is the first study to also consider the efficiency of dibh by analyzing the correlation between breathing amplitude and normal tissue complication probability ( ntcp )  . material and methods patients between october 2006 and june 2008 , 60 patients with breast cancer who were referred for postoperative irradiation took part in a study approved by the scientific ethics committee of the medical university of graz , austria . 
57 patients received 50 gy ( 2 gy / day , 5 days / week ) ; in three patients the daily dose was reduced to 1.8 gy due to a large breast volume . only if the breathing amplitude is within a predefined upper and lower threshold . all patients were audio - coached [ 10 ] in a dibh technique [ 12 ] to reach their individual maximum of vertical chest wall movement . 
optimization of the tangential fields was achieved by adapting the radiation field size , weighting of fields , multileaf collimator shaping and , if required , wedges . the absorbed dose was calculated for the target , the ipsilateral lung and the heart . 
 although dvhs are useful to compare treatment plans , the change of lung volume due to deep inspiration leads to an overestimation of irradiated volume . to quantify the changing lung density within breathing patterns , butler et al . 
 [ 4 ] recommended the calculation of a dose - mass histogram ( dmh ) , which is likely to provide a better estimation of the actual number of lung cells damaged by radiation than lung volume . 
since conventional planning systems do not normally offer dmhs , the mean density of the ipsilateral lung was calculated from ct voxels . in addition , a smaller restricted region of the lung enclosed by the 10% isodose was delineated , excluding one voxel thickness in the peripheral region to avoid systematic errors from segmentation algorithm and artifacts [ 29 ]  . data analysis ipsilateral mean lung mass and mean density , as well as mean mass and density in the restricted area of the tangential region were tested for nb and dibh . 
the lyman - kutcher - burman ( lkb ) model [ 3 , 15 , 20 ] , widely used to calculate the probability of lung damage , was adopted for ntcp calculation : gating system the real - time position management respiratory gating system ( rpm , varian medical systems , inc . , palo alto , ca , usa ) uses a fiducial marker block placed on the thorax and an infrared camera , which monitors the anteroposterior movement of the chest wall in real time [ 33 ]  . 
irradiated lung mass in breast cancer the modified clinical model [ 16 ] defines md as mean lung dose , td50 = 37.6 gy ( 95% confidence interval [ ci ] , 34.641.4 ) for radiation - induced pneumonitis in the ipsilateral lung and m = 0.35 ( 95% ci , 0.290.43 ) [ 24 ]  . 
the difference of the maximum dose to the ipsilateral lung in dibh with 50.8 gy ( range : 44.254.4 gy ) versus the dose in nb with 50.9 gy ( range : 44.554.8 gy ) was not statistically significant . mean density of the ipsilateral lung was 0.19 g / cm3 ( range : 0.140.34 g / cm3 ) in dibh and 0.32 g / cm3 ( range : 0.210.45 g / cm3 ) in nb mode ( table 1 )  . 
considering only the tangential part of the left lung , mean density changed from mean 0.19 g / cm3 to 0.16 g / cm3 in dibh , whereas in nb a density reduction to 0.25 g / cm3 was observed . 
with an additional voxel - size exclusion in the restricted region , as defined above , mean density was reduced to 0.11 g / cm3 ( range : 0.050.25 g / cm3 ) in dibh and 0.19 g / cm3 ( range : 0.110.31 g / cm3 ) in nb , respectively . 
mass variations in both breathing modes were only 2% . mean lung mass receiving 20 gy ( m20 ) was calculated with the volume receiving 20 gy ( v20 ) with m20 = v20 * restricted region ( g ) gy ( see table 2 )  . 
the estimation of mean mass was associated with a statistically significant reduction of irradiated lung mass in dibh . the calculated ntcp for both breathing modes is shown in figure 1 . 
in dibh , increased lung volume is subjected to individually increased amplitude . patients were audio - coached to reach their maximum reproducible breathing amplitude , and in correlation with ntcp ( figure 3 ) there was no universally valid amplitude height suggesting a lower ntcp . discussion 60 breast cancer patients were included in a study using an rpm gating system which enables dose delivery according to patients individual breathing gate defined in dibh mode . 
 while a dose / volume reduction of the heart has been demonstrated [ 11 , 27 , 28 ] , the consequences of simultaneously increasing the irradiated lung volume are yet insufficiently investigated and hampered by the complexity of lung dose calculations , which include the following : first , lung contains different structures with density changes in lung tissues ranging from 960 hu to 190 hu , which leads to artifacts and additional uncertainties concerning the estimation of hus . 
gegenberstellung der ntcp - berechnung ( % ) aller patientinnen fr dibh und nb . volume ( cm3 ) 1800 1600 1400 1200 1000 to quantify organ dose , mavroidis et al . 
 our commercial treatment - planning system does not provide calculation of a dmh , but solely region - dependent density values with consecutive calculation of mass . since lung density is not homogeneously distributed , with greatest density in the base which decreases toward the apex [ 8 ] , we chose to define the tangential part of the lung within the 10% isodose as region of interest . 
 [ 29 ] , resulted in a difference of mean density of the whole lung versus tangential part in nb of about 42% , whereas in dibh the difference added up to 43% ( table 1 )  . it should be taken into account that dose calculation in low - density tissues is strongly dependent on dose algorithms of the applied treatment - planning systefogliata et al . 
 [ 5 ] and thomas [ 30 ] , and is verified for low - density materials in a small deviation of mus . the incidence of pneumonitis has been shown to correlate with the increase of the mld to the ipsilateral lung [ 34 ]  . 
generally , irradiated lung mass was reduced in 73% of the patients ; therefore , the individual potential benefit should be carefully assessed . another aim of the current study was the quantification of biological lung complication including different breathing patterns . 
considering the volume delineation , pencil - beam calculation and the ntcp model adaption to nonuniform doses by dvh , their values show the benefit of gating , but their given percentage seems to be overestimated . 
these parameters were limiting factors in our trial . some studies [ 6 , 10 , 11 , 14 ] discussed different methods of breathing coaching and irradiation methods to deliver the amplitude ( cm ) figure 3 . 
the level was affected by comfort and reproducibility . to our knowledge , this is the first trial to investigate if our breathing training and our definition of an individual amplitude correlates with ntcp . 
figure 2 shows increased lung volume v to be connected to the breathing amplitude , whereas no direct connection between chest wall amplitude and ntcp can be shown ( figure 3 )  . 
therefore , we conclude that the individual range patients reach in dibh with our audio - coaching training technique changes ntcp ( figure 1 ) favorably . conclusion the delineation of a restricted lung area supports mean density calculation , which allows a good estimation of irradiated lung mass . 
analysis of 60 patient data , treated with tangential breast irradiation , shows that dibh significantly reduces mean ipsilateral lung mass in the vast majority of patients and its efficiency is supported by a decrease of ntcp . strahlentherapie und onkologie original article betulinic acid a radiosensitizer in head and neck squamous cell carcinoma cell lines christina eder - czembirek1 , boban m . 
erovic2 , cornelia czembirek1 , markus brunner2 , edgar selzer3 , richard ptter3 , dietmar thurnher2 background and purpose : betulinic acid , a pentacyclic triterpene , is a new cytotoxic compound active on melanoma , neuroblastoma , glioblastoma and head and neck squamous cell carcinoma ( hnscc ) cells . 
in this study , the radiosensitizing effect of betulinic acid on sequential irradiation was investigated in hnscc cell lines . material and methods : two hnscc cell lines , scc9 and scc25 , were treated with increasing doses of betulinic acid and sequentially irradiated with a single boost of 4 gy from a conventional radiation source . 
the cells were counted , the surviving fraction was determined , and colony - forming assays were performed . results : it could be shown that betulinic acid alone inhibits cell survival , affects cell survival additively in combination with irradiation and decreases clonogenic survival in both cell lines when applied alone . conclusion : betulinic acid could be a promising treatment agent in radioresistant head and neck cancer . 
a combination of betulinic acid with radiotherapy seems to be beneficial . key words : betulinic acid irradiation radiosensitizer head and neck squamous cell carcinoma strahlenther onkol 2010 ; 186 : 1438 doi 10.1007 / s00066 - 010 - 2069 - 6 betulinsure ein radiosensitizer in kopfund halstumorzelllinien hintergrund und ziel : betulinsure , ein pentazyklisches triterpenoid , ist ein neuer zytotoxischer wirkstoff mit wirkung gegen melanom - , neuroblastom - , glioblastomsowie kopfund halstumorzellen . 
in dieser studie wurde untersucht , ob betulinsure ein radiosensitizer bei sequentieller bestrahlung von kopfund halstumorzellen ist . material und methodik : die beiden kopfund halstumorzelllinien scc9 und scc25 wurden mit ansteigenden dosen von betulinsure und sequentieller radiotherapie mit einer einzeldosis von 4 gy ( abbildungen 1a und 1b ) an einem konventionellen bestrahlungsgert behandelt . 
 ergebnisse : es konnte gezeigt werden , dass betulinsure allein das zellberleben inhibiert , additiv in kombination mit radiotherapie agiert und in beiden zelllinien die koloniebildungsfhigkeit herabsetzt . schlussfolgerung : betulinsure knnte ein vielversprechendes chemotherapeutikum bei radiotherapieresistenten kopfund halstumoren seeine kombination von betulinsure und strahlentherapie scheint vorteilhaft . schlsselwrter : betulinsure bestrahlung radiosensitizer kopfund halstumoren introduction the general poor prognosis of advanced head and neck cancer , especially once tumor relapse occurs [ 23 ] , forces research to identify new chemotherapeutic agents and treatment modalities . 
moreover , cancer therapy is faced with two major problems : time - dependent development of ther1department of cranio - , maxillofacial and oral surgery , medical university of vienna , austria , 2department of otorhinolaryngology , head and neck surgery , medical university of vienna , austria , 3department of radiotherapy and - biology , medical university of vienna , austria . received : august 3 , 2009 ; accepted : december 22 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
radiosensitizing effects by betulinic acid apy - resistant cancer cells and nonspecific toxicity toward normal cells . a substance with the ability to specifically sensitize tumor cells to chemoand / or radiotherapy would therefore be an important step toward more efficient anticancer therapy . 
with this aim in mind , different plant - derived polyphenols have been investigated for their sensitizing potency [ 10 ]  . one of these plant polyphenols is betulinic acid , a pentacyclic triterpene discovered and isolated 1995 in the stem bark of the indian jujube and found to be a melanoma - specific cytotoxic agent [ 15 , 19 ] that inhibits the growth of human melanoma in athymic mice [ 15 ]  . 
it exerts potent antineoplastic effects on cell lines and primary cultures derived from neuroectodermal tumors [ 5 ] and also on head and neck cancer cells [ 19 ]  . 
the growth - inhibitory effect of betulinic acid was attributed to an induction of apoptosis in tumor cells [ 5 , 7 , 15 , 19 , 21 ] by directly affecting the mitochondria leading to cytochrome c release . 
cytochrome c regulates the downstream caspase activation determined by the relative amounts of apoptosis - promoting ( bax , bak , bid ) and apoptosis - inhibiting ( bcl - 2 , bcl - xl , mcl - 1 ) proteins , and after activation of caspase - 9 the apoptotic process has entered its irreversible phase [ 4 ]  . 
the cleavage gives rise to a neoepitope in the c - terminal domain of the protethe m30 antibody recognizes this neoepitope and is highly specific for epithelial cells [ 11 ]  . similarly , irradiation indirectly affects the mitochondria combined treatment of irradiation and betulinic acid revealed an additive growth - inhibitory effect on human melanoma cell lines [ 19 ]  . the aim of this study was to investigate the effect of the combinatorial treatment of betulinic acid and irradiation on head and neck cancer cell lines . material and methods drugs betulinic acid ( biomol , vienna , austria ) was dissolved in dimethylsulfoxide ( dmso ) and stored at 20 c at a concentration of 5 mg / ml . 
a dose of 4 gy was found to reduce cell numbers by 50% and was therefore used for all further experiments . cell proliferation assays 5 105 cells were seeded in 10 - cm culture dishes . 
after 48 h the cells were irradiated with a single boost of 4 gy , and 24 h later they were counted using an automated casy1 cell counter and analyzer system ttc ( schrfe , reutlingen , germany ) to determine the number of cells and the surviving fraction . 
all experiments were repeated at least three times . clonogenic survival assays after the above described dose - response experiment 4 102 of the analyzed , surviving cells were plated onto six - well plates for colony - forming experiments . 
then cells were fixed in paraformaldehyde for 34 min , washed three times with distilled water , stained with pure methylene blue and washed agacolonies with more than 50 cells were elected as survivors , counted and synergism graphs on colony reduction were constructed . to detect apoptosis , a mouse monoclonal antibody against the m30 neoepitope was utilized ( monoclonal mouse antibody cytodeath m30 , 1 : 50 , roche , mannheim , germany )  . 
to reduce background signals , samples were treated with 5% bsa ( sigma - aldrich , vienna , austria ) / tris - buffered saline ( tbs ) for 30 mafter the blocking step , slides were incubated with m30 antibody overnight at room temperature . 
samples were incubated with biotinylized anti - mouse antibody ( 1 : 100 , vector laboratories , burlingame , ca , usa ) for 1 h , washed , and incubated with alkaline phosphatase - conjugated streptavidine - ap / 10% human serum ( 1 : 100 , dako , glostrup , denmark ) for 1 h at room temperature . 
error bars represent standard errors of the means ( sem ) of the experiments which were repeated three times . results effect of irradiation on cell survival of scc9 and scc25 cells first , we determined the effect of irradiation on scc9 and scc25 cells . 
at 4 gy , cell numbers were reduced to 51.56% ( sem = 0.76% ) in the scc9 cell line and to 44.08% ( sem = 0.85% ) in the scc25 cells . cell numbers after chemotherapy versus radiochemotherapy in hnscc cell lines scc9 and scc25 second , we compared the numbers of cells treated with betulinic acid alone , radiotherapy alone , or betulinic acid and radiotherapy . 
doses of betulinic acid were between 0 and 8 g / ml medium as used by other authors in different cellular systems [ 5 , 6 , 19 ]  . 
then the amount of redcolored cells was counted for each therapy constellation . statistical analysis statistical analysis was performed using graphpad 4.0 software from prism ( graphpad software inc . , san diego , ca , usa )  . 
die zelllinien wurden mit ansteigenden dosen von betulinsure ( 08 g / ml ) und / oder 4 gy behandelt . ment decreases proliferation significantly at doses between 4 and 8 g / ml betulinic acid ( p = 0.0222 , p = 0.0031 , p = 0.0024 ) compared to 4 gy alone ( figures 2a and 2b )  . effects of combined treatment with betulinic acid and radiotherapy on clonogenic survival combined treatment with betulinic acid and radiotherapy did not show a synergistic nor an additive inhibition of colony formation except the combination of 6 g / ml betulinic acid with 4 gy on scc9 as determined with clonogenic assays ( figures 3a and 3b )  . 
however , higher doses of betulinic acid alone seem to have a comparable clonogenicity reducing capability as irradiation with 4 gy . m30 immunohistochemical staining we employed the m30 antibody for the visualization of apoptotic cells in immunohistochemistry . figures 4a and 4b show representative photomicrographs of scc25 and scc9 cells stained with the m30 antibody after strahlenther onkol 2010 no . 
based on these findings , we investigated whether betulinic acid can enhance the efficacy of standard radiotherapy on hnscc tumor cell lines . our experiments demonstrated that betulinic acid could be a useful chemotherapeutic agent . 
 in addition to this , we could determine that the effect of betulinic acid in combination with irradiation was at least additive . clonogenic survival assays , as an indicator for the long - term effect of treatment on tumor cells , showed that betulinic acid was not of further benefit on the anticlonogenic effect of irradiation [ 14 ]  . 
 these results are contrary to the findings by selzer et al . , who detected an additive effect of betulinic acid and irradiation on melanoma cells in clonogenic assays [ 19 ]  . comparable to the workgroups of schtze et al . 
based on our results , we suggest that betulinic acid might be a useful agent for tumors that are resistant to irradiation without enhancing side effects on normal tissue as do standard chemotherapeutic agents . 
these results are more promising than the ones we could show using nimesulide , a cyclooxygenase - 2 inhibitor , in combination with irradiation on hnscc cells [ 3 ]  . 
 as a consequence , it would make sense to do further investigations on betulinic acids capability in combination with other cancer treatment modalities in different types of tumor tissue and also investigating possible radioprotective abilities on normal tissue [ 22 ]  . strahlentherapie und onkologie original article second malignancies in high - dose areas of previous tumor radiotherapy birgitta welte1 , peter suhr1 , dirk bottke1 , detlef bartkowiak1 , wolfgang drr2 , klaus rdiger trott3 , thomas wiegel1 purpose : to characterize second tumors that developed in or near the high - dose areas of a previous radiotherapy , regarding their frequency , entities , latency , and dose dependence . patients and methods : 9 , 995 / 15 , 449 tumor patients of the radiation oncology department in ulm , germany , treated between 1981 and 2003 , survived at least 1 year after radiotherapy . 
by long - term follow - up and review of treatment documentation , 100 of them were identified who developed an independent second cancer in or near the irradiated first tumor site . 
main second tumors were carcinomas of the upper ( 18% ) and lower ( 12% ) gastrointestinal tract , head and neck tumors ( 10% ) , lymphoma ( 10% ) , breast cancer ( 9% ) , sarcoma ( 9% ) , and lung cancer ( 8% )  . 
the incidence and potential dose - response relationship intermediate will be analyzed by a case - case and a case - control study of the ulm data . key words : retrospective studies radiation - induced neoplasms second tumors strahlenther onkol 2010 ; 186 : 1749 doi 10.1007 / s00066 - 010 - 2050 - 4 zweitmalignome in hochdosisbereich vorangegangener strahlentherapie ziel : zweitmalignome , die sich im oder nahe am hochdosisbehandlungsvolumen einer vorangegangenen strahlentherapie entwickelten , sollten hinsichtlich ihrer hufigkeit , entitten , latenz und dosiskorrelation charakterisiert werden . patienten und methodik : 9 995 / 15 449 patienten , die zwischen 1981 und 2003 in der klinik fr strahlentherapie der universitt ulm behandelt wurden , berlebten mindestens 1 jahr . 
unter diesen patienten wurden durch langzeit - follow - up und berprfung der behandlungsdokumentation 100 flle identifiziert , bei denen sich im oder nahe am ersttumor - bestrahlungsvolumen ein unabhngiger zweittumor entwickelte . 
hufiger beobachtete zweittumoren waren karzinome des oberen ( 18% ) und unteren ( 12% ) verdauungstrakts , des kopf - hals - bereichs ( 10% ) , lymphome ( 10% ) , mammakarzinome ( 9% ) , sarkome ( 9% ) und lungentumoren ( 8% )  . 
die latenz der zweittumoren lag insgesamt bei median 7 , 4 jahren ( 142 jahre ) , fr kolorektale karzinome bei 3 , 5 und fr leukmien bei 4 , 3 jahren , fr sarkome dagegen bei 11 , 7 und fr mammakarzinome bei 17 , 1 jahren . 
15 - jahres - wahrscheinlichkeit , ein zweitmalignom im oder nahe am ursprnglichen behandlungsvolumen , also nach mittleren bis hohen strahlendosen , zu entwickeln , lag bei 0 , 5% bzw . 
inzidenzen und mgliche dosis - wirkungs - beziehungen sollen im rahmen von fall - fallund fall - kontroll - studien an den ulmer daten untersucht werden . schsselwrter : retrospektive studien strahleninduzierte neoplasien zweittumoren 1department of radiotherapy and radiation oncology , university of ulm , germany , 2department of radiotherapy and radiation oncology , radiobiology laboratory , university of technology dresden , germany , 3ucl cancer centre , university college london , uk . received : july 3 , 2009 ; accepted : december 22 , 2009 published online : february 22 , 2010 strahlenther onkol 2010 no . 
 however , the people observed in this study were exposed to acute total - body irradiation , with an average dose of 0.25 gy and only 263 ( 0.3% ) surviving the ld50 of 4 gy [ 20 ]  . 
their frequency may not only depend on the dose - volume relationship but also on chemotherapy and genetic factors [ 1 , 28 ] , and when treatment strategies change over the years , this may influence the risk for tumor induction , too [ 22 ]  . in the department of radiotherapy and radiation oncology , university of ulm , germany , a long - term survey of patients was performed beyond the usual 5 years . 
information was obtained preferentially during interviews with the patients or else from their local practitioners , health insurances or other secondary sources . cases were considered , if second tumors occurred over 1 year after irradiation . 
cases were further analyzed , if second tumors had developed within the high - dose irradiation volume or at its margins ( defined as the region of 5 cm adjacent to the 95% isodose )  . 
recurrences or metastases were excluded from the analysis by histopathology and / or localization of the second tumor . results patient population between march 1981 and december 2003 , 15 , 449 patients were irradiated in the department of radiation oncology , university of ulm , germany . 
82 cases were excluded from the analysis : 51 patients had contralateral breast cancer , localized in the inner or central quadrants ; 31 patients had second head and neck cancers with identical histology , and continual alcohol and / or tobacco consumption . therefore , this study comprises 100 patients with histopathologically independent second cancer . 
further details are compiled in table 1 . irradiation techniques second neoplasms occurred mostly after treatment of the breast or chest wall often including local lymph nodes ( 24% ) , after mantle field or other extended fields in lymphoma ( 22% ) , or after whole pelvic irradiation ( 21% )  . 
in 93% of the patients , the first tumor was in complete remission when the second tumor was diagnosed . first and second malignancies 46% of the second tumors were located within the previously irradiated volume , 23% at the field margins . 
second cancers were 70% carcinomas , 16% hematologic disorders , 7% sarcomas , 3% benign tumors ( meningiomas and cavernomas after childhood acute lymphoblastic leukemia ) , and 4% allowed no clear histological classification . 
correlation of histopathology / location of first and potentially radiogenic second cancers in 100 / 9 , 995 patients ( 66 female , 34 male , among them ten children )  . ad - hyp : adenoma of hypophysis ; al : acute leukemia ; brain : brain tumors ; breast : breast cancer ; gynp : gynecologic tumors of pelvis ; hn : head and neck tumors ( including thyroid ) ; lym : lymphoma ; pca : prostate cancer ; sarc : sarcoma ; thym : thymoma . 
similarly , second meningiomas and cavernomas occurred with a latency of 1316 years ( figure 3 )  . second malignancies developed conspicuously frequent in patients who had received radiotherapy for hodgkins or non - hodgkins lymphoma , involving 4.4% of these patients versus 1.0% in the whole cohort . 
this may to some extent result from the particularly long follow - up of 17.8 years in lymphoma patients . in patients who developed a second tumor in the upper gastrointestinal tract , the median target dose to the first tumor had been 24 gy ( range 2456 gy )  . 
patients with second colorectal carcinoma had previously received a median target dose of 50 gy ( range 36116 gy including brachytherapy ; see figure 4 )  . 5 years after the diagnosis of second cancer , 35% of the patients were still alive . the most frequent second tumors , located in the upper gastrointestinum , had a specifically poor prognosis , with a 5 - year survival of only 5% . in 9 / 100 patients , a third tumor occurred within the former irradiation volume or at the field margin four cases , a mantle field had been irradiated . 
three of these four patients developed bilateral breast cancer sequentially . discussion for the present study , we analyzed over 15 , 000 patients with different malignancies , treated and followed up in one institution and all documented in a database by the same staff . 
die latenz von 100 zweitmalignomen , die im oder nahe am therapievolumen des bestrahlten ersttumors entstanden , lag bei median 7 , 4 jahren mit einer spanne von 142 jahren . the median latency of the 100 second tumors was 7.4 years ( range 142 years , figure 1 )  . 
by contrast , there was a long latency in second breast cancer ( 17.1 years ) and sarcoma breast gynp sarc ad - hyp brain thym other r 0.8 welte b , et al . 
second tumors after radiotherapy high dose any dose familial accumulation of breast cancer and presence of the confounders alcohol or nicotine caused exclusion of cases , other risk factors , specifically cytostatic drugs , have not been considered . 
the short latency period of 1 year was chosen to include cases where radiation may have promoted the progression of existing premalignancies to definitive tumors [ 9 ]  . tumor entities much of the literature on radiation - induced malignancies describes second sarcoma , mostly in case reports . 
the spectrum of second malignancies that we found in high - dose areas of first treatment sites is well in agreement with published data ( reviewed in [ 23 ] )  . first hodgkins disease according to the german hodgkin disease study group hd1 to hd9 ( 19831998 ) , 2.4% of 5 , 367 patients developed a second cancer within a median follow - up of 6 years [ 3 ]  . 
two major studies report the increased risk of secondary malignancies after radiotherapy for hodgkins disease ( hd ) to be related to field size but also to additional chemotherapy [ 15 , 18 ]  . 
 even more so , radiotherapy for childhood hd can establish an overall relative risk as high as 5.2 for any second neoplasm [ 10 ] and 7.0 for breast cancer [ 11 ]  . 
while first breast cancer an extensive analysis in adult women with breast cancer used the american surveillance , epidemiology , and end results ( seer ) database [ 5 ]  . 
in our study , we found six cases of rectal cancer with an average latency of 4 years after prostate irradiation ( among more than 830 patients )  . welte b , et al . 
breast : mammakarzinom : colorec : kolorektales karzinom ; hn : kopf - hals - tumor ; lym : lymphom ; sarc : sarkom ; upgi : karzinom des oberen verdauungstrakts . diotherapy of the hemithorax ( 19731982 ) was 2.7 times more frequent in ipsilateral than in contralateral localization . 
this agrees with a suggested dose - volume relationship for radiogenic second cancer [ 6 , 28 ]  . first gynecologic cancer a large seer - based study on second cancer after endometrial irradiation [ 16 ] points out the increased relative risk of second tumors in neighboring tissues , including the vulva ( 83% ) and colon and rectum ( 43% )  . 
after irradiation of the uterine cervix , 12 / 1 , 495 japanese patients surveyed > 10 years developed second malignancies in the bowel [ 19 ]  . first prostate cancer in the seer data on prostate cancer , 8 years after radiotherapy , the relative risk for bladder carcinoma was 1.5. 
only the latest of three seer analyses [ 2 , 4 , 17 ] found an increased risk of rectal cancer after prosdose dependence of tumor induction many types of second tumors are observed in low - dose areas or at the field margins , whereas second sarcomas often occur in areas of high radiation dose [ 13 ]  . 
in dresden , germany , an analysis was performed in 203 patients , admitted for treatment of a second tumor , which was 0.65% of all 31 , 000 patients irradiated between 1969 and 1989 . 
in a study comprising more than 25 , 000 young patients [ 24 ] , approximately 50% of 196 second tumors occurred in areas that had been exposed to < 1 gy . 
however , the relative risk grew proportional with the dose up to > 30 gy . in the ulm data , the frequent second malignancies of the upper gastrointestinal tract but also lung and breast cancer were associated with moderate nominal doses to first tumor sites ( figure 4 ) , while colorectal cancer but also sarcoma developed in explicitly high - dose areas . 
it should be kept in mind , though , that dose determination for the second tumor site is often difficult , especially at the field margins with their steep dose gradients . modern techniques such as multiportal or intensitymodulated radiotherapy ( imrt ) minimize high - dose irradiation volumes , while volumes with low irradiation doses and total - body dose are increased [ 22 , 3033 ]  . 
the number of second tumors following multiportal irradiation or imrt might more than double in comparison to less sophisticated radiation techniques [ 12 , 13 , 30 ]  . latency period in over 200 publications on second tumors after radiotherapy ( retrieved by medline ) , the reported latency was between 1 and 45 years , with a median of 10 years . 
as part of an ec - funded project , allegro , a case - case and a case - control study will be performed on the ulm data regarding the incidence and dose dependence of second cancer . strahlentherapie und onkologie original article radiotherapy and chemotherapy as therapeutic strategies in extrahepatic biliary duct carcinoma thomas b . 
eccles1 purpose : this report aims to provide an overview on radiotherapy and chemotherapy in extrahepatic biliary duct carcinoma ( bdc )  . patients and methods : a pubmed research identified clinical trials in bdc through april 1 , 2010 including randomised controlled trials , seer analyses and retrospective trials . 
additionally , publications on the technical progress of radiotherapy in or close to the liver were analysed . results : most patients with cholangiocarcinoma present with unresectable disease ( 8090% ) , and more than half of the resected patients relapse within 1 year . 
novel technical advances in radiotherapy may allow for dose - escalation and could significantly improve outcome for patients with cholangiocarcinoma . conclusion : both the literature and recent technical progress corroborate the role of radiotherapy in bdc offering chances for novel clinical trials . 
progress is less pronounced in chemotherapy . key words : bile duct cancer radiotherapy chemotherapy chemoradiotherapy review strahlenther onkol 2010 ; 186 : 67280 doi 10.1007 / s00066 - 010 - 2161 - y radiotherapie und chemotherapie als therapeutische strategien bei extrahepatischen gallenwegstumoren ziel : dieser bericht gibt eine bersicht ber die rolle der radiound chemotherapie beim extrahepatischen gallengangskarzinom ( bdc )  . patienten und methodik : eine pubmed - suche identifizierte klinische studien zum bdt bis 1 . 
april , 2010 und schloss randomisierte kontrollierte studien , seer analysen und retrospektive studien eauerdem wurden arbeiten zum technischen fortschritt der radiotherapie in und nahe der leber analysiert . ergebnisse : die mehrzahl der patienten mit cholangiozellulrem karzinom befindet sich zum zeitpunkt der diagnose bereits in fortgeschrittenen irresektablen tumorstadien , und auch unter den primr operablen patienten kommt es in den meisten fllen zum rezidiv innerhalb eines jahres . 
jedoch zeigen neueste seer - analysen , dass die radiotherapie nicht nur eine besserung der lebensqualitt durch besserung der cholestase bewirkt , nsondern auch das berleben verlngert , weshlab sie als neue standardtherapie angesehen werden sollte . 
neueste technische entwicklungen in der strahlentherapie erffnen die perspektive einer dosiseskalation und knnten die ergebnisse bei patienten mit cholangiozellulren karzinomen dramatisch verbessern . schlussfolgerung : sowohl die literatur als auch der jngste technische fortschritt strken die rolle der radiotherapie beim bdc und erffnen chancen fr klinische studien . 
fr die chemotherapie ist der fortschritt weniger ausgeprgt . schlsselwrter : gallenwegstumoren radiotherapie chemotherapie radiochemotherapie bersicht 1gray institute for radiation oncology and biology , university of oxford , oxford , united kingdom . received : april 14 , 2010 ; accepted : september 16 , 2010 published online : november 30 , 2010 strahlenther onkol 2010 no.12 urban & vogel brunner tb , et al . 
however , only a minority of the patients can be operated and even if a clear resection ( r0 resection ) is possible , the rate of relapse is as high as 6075% [ 50 ]  . 
in addition , the assessment of the respective therapeutic modalities is impeded by the paucity of data ( low patient numbers , only with perspective studies , rarely randomised control groups )  . 
this review aims to deliver an overview of the current knowledge of radiotherapy and chemotherapy in biliary duct carcinoma but also to give an outlook to the high potential for radiotherapy with the advent of intensity - modulated radiotherapy ( imrt ) and imageguided radiotherapy ( igrt )  . 
 methods we conducted a pubmed research on articles published in english , german and french until april 1 , 2010 ( open start date ) with the major mesh headings biliary tract neoplasms and cholangiocarcinoma . 
the two headings were then combined with other search terms and the following numbers of articles were identified with the two major mesh terms respectively : radiotherapy 397 and 355 , randomized controlled trials 83 and 8 , clinical trial ( phase iii ) 5 and 0 , clinical trial ( phase ii ) 118 and 24 , retrospective studies 1165 and 355 , seer 24 and 11 . 
 this is in contrast with the results of a retrospective analysis of 294 us american patients [ 53 ] : neither external - beam radiotherapy ( 48 gy ) nor combined external / intraluminal radiotherapy resulted in a positive effect after r0 resection . 
importantly , this series had a low number of margin - free resections ( 14% ) which might well be relevant for the survival advantage of adjuvant therapy in this study . 
for intrahepatic cholangiocarcinoma a recent seer analysis in over 3 , 800 patients showed that the combination of surgery and adjuvant radiation therapy results in the greatest benefit and median overall survival time ( 9 vs 6 months , p = 0.014 ) [ 57 ]  . 
the largest piece of evidence advocating the use of adjuvant radiotherapy after complete resection is a recent seer analysis ( 19732005 ) on a total of > 1500 patients with locoregional extrahepatic cholangiocarcinoma indicating a modest but significant prolongation in survival ( mean overall survival ( mos ) 26 vs 25 months , table 1 ) [ 24 ]  . 
adj : adjuvant , gy : gray , mos : medianes gesamtberleben , n : patientenzahl , n.a. : nicht angegeben , neo : neoadjuvant , r + : positive schnittrnder , r : tumorfreie schnittrnder , rt : radiotherapie , seer : beobachtung , epidemiologie und endergebnisse . rt dose ( gy ) mos ( months ) 3 - year survival rate n.a. study fuller ( seer ) [ 24 ] shinohara ( seer ) [ 58 ] kopelson [ 39 ] gerhards [ 26 ] cameron [ 7 ] pitt [ 53 ] hughes [ 31 ] nelson 651 701 1372 clear resections rt 275 ( 73% ) 464 ( 71% ) n.a. 
rt and ct as therapeutic strategies in extrahepatic bdc adjuvant chemoradiation ( crt ) on the basis of the radiosensitising effect of several chemotherapeutic agents ( for instance 5 - fluorouracil ( 5 - fu ) ) several trials tested the efficacy of adjuvant simultaneous chemoradiation . 
 [ 37 ] achieved a 5 - year overall survival of 36% for patients after r0 as well as r1 resection combining external radiotherapy ( 40 gy ) with 5 - fu bolus . 
 [ 31 ] compared the 5 - year overall survival after post - operative chemoradiotherapy ( 50.4 gy , concomitant 5 - fu ) with that after surgery alone in distal cholangiocarcinoma and confirmed a slight benefit of 35% vs 27% . 
most of the above given results apply for distal extrahepatic cholangiocarcinoma whereas the evidence to support the use of adjuvant chemoradiation for intrahepatic cholangiocarcinoma is very limited . adjuvant chemotherapy adjuvant chemotherapy has largely failed to show significant survival benefits [ 65 , 66 ]  . 
 among the 508 patients included 118 had resected bile duct carcinoma ( 58 receiving chemotherapy vs 60 in the control group ) and no survival benefit was observed in either the subgroup with clear resections or in the subgroup with residual disease . 
similar observations were made for patients ( n = 49 ) with resected ampullary carcinoma whereas patients with resected gallbladder cancer had a significant prolongation of survival after adjuvant chemotherapy ( 5 - y os 26% vs 14% )  . taking into account that the majority of the relapses occur locally or regionally , the approach of another group from japan appears to be more promising : postoperative intraarterial application of 5 - fu ( hepatic artery ) achieved a significant improvement of 1 - y os ( 76% vs 52% compared with resection only ) as well as the median overall survival [ 63 ]  . neoadjuvant therapy : especially in the case of peri - hilar tumor localizations , a clear resection is often not possible even in early stages . 
after preoperative chemoradiation ( total dose ( td ) 50.4 gy / 5 - fu continuous infusion ) , a rate of clear resections of 100% was reported compared to only 54% in the control group of 40 non - pretreated patients with primary operable tumors . 
another option for selected patients with non - resectable stage iii peri - hilar cholangiocarcinoma and a negative operative nodal staging is chemoradiation to bridge the gap for liver transplantation . 
 [ 29 ] described 1and 5 - year survival rates of 88 and 82% after neoadjuvant combined percutaneous / intraluminal irradiation ( 45 gy / 2030 gy ) and concurrent 5 - fu - based chemotherapy . 
due to short survival times therapy for patients with inoperable cholangiocarcinoma is required to lead to an improvement of quality of life and at the same time to minimise treatment - related complications , e.g. 
the disadvantage of this form of biliary drainage is more discomfort and reduced quality of life as well as the disadvantage of draining bile without the ability of enteric recycling . 
these studies showed that metal stents are more cost effective for patients with an expected survival time of more than 5 months as an effect of a lower number of interventions and shorter hospitalizations . 
however , this hypothesis could not be confirmed with an increased risk of cholecystitis related with covered stents [ 25 , 49 ]  . systemic chemotherapy to date , no chemotherapeutic regimen has consistently shown activity against cholangiocarcinoma . 
similar to earlier stages of the disease the level of evidence of these studies is often limited due to low patient numbers , lack of control groups or a mixture of intra - / extrahepatic cholangiocarcinoma with gallbladder cancers or papillary cancer . 
response rates could be increased to about 30% using combinations of 5 - fu with leucovorin , cisplatin and / or epirubicin hence achieving median overall survival times between 6 and 11 months [ 9 , 17 , 44 , 51 ]  . 
similarly , the combined administration of 5 - fu with doxorubicin and mitomycin c did not improve the efficacy . in contrast to these data , the results of gemcitabine mono or combination therapy are more promising . 
the use of gemcitabine only was reported to result in response rates of up to 60% ( median 30% ) , and the median overall survival time in a prospective phase ii study reported by penz et al . 
while combinations of gemcitabine with irinotecan or docetaxel did not result in increased activity , the combination of gemcitabine with oxaliplatin in patients with a good performance status and sufficient hepatic and renal function resulted in a median overall survival time of 15.4 months [ 2 ]  . 
furthermore , chemotherapeutic agents are enriched in the biliary canaliculi after hepatic excretion . the simultaneous administration of ebrt and 5 - fu into the hepatic artery in 22 patients resulted in a progression - free survival of 50% after 2 years and an overall survival of 20% after 4 years [ 54 ]  . 
 [ 8 ] reported on 30 patients with locally advanced / metastasised cholangiocarcinoma treated with combined intraarterial ( epirubicin , cisplatin ) and systemic ( 5 - fu ) chemotherapy and achieved remission rates and stable disease in 40% ( mpfs 7 months ) and 1yand 2y - os of 54% and 20% , respectively . palliative ( chemo ) radiation there are no large randomised clinical trials in cholangiocarcinoma and many of the reports show therapeutic inhomogeneities ( table 2 ) , however a very recent large seer analysis allows to estimate the effect of radiotherapy [ 24 ]  . 
another seer analysis on almost 400 patients with radiotherapy compared with more than 2200 patients with observation showed also a clear survival benefit for the patients who underwent radiotherapy ( mos 9 vs 4 months , p < 0.0001 ) [ 57 ]  . 
on the other hand , the seer data show that even radiotherapy with simple treatment techniques was able to improve survival giving rise to the prospect of further improvement with modern radiotherapeutic techniques . 
 brachytherapy : the key advantage of intraluminal brachytherapy ( bt ) is the focal delivery of high radiation doses with rapid dose falloff over a short distance from the radioactive source thus avoiding hepatotoxicity . 
after identification of the location and length of the malignant bile duct stricture at cholangiography brachytherapy with sources such as ir - 192 can be performed preferably in a transduodenal endoscopic approach or where this is not possible in a transhepatic technique . 
in case of bt in conjunction with ebrt ( combined radiotherapy ) , a total dose of up to 20 gy in four fractions over 2 days can be given ( 2030 gy at 0.51 cm from the source with ldr ) [ 3 ]  . 
 [ 40 ] reported prolongation of the median survival time to 14.5 months after combined external / intraluminal radiotherapy ( similar data is reported by foo [ 21 ] ) , whereas bowling et al . 
 chemoradiation : more than 3 decades after the first study on crt by kopelson [ 39 ] , there is still only a small number of trials reporting on crt . 
while most of these trials concluded a survival benefit mediated by the addition of chemotherapy [ 1 , 5 , 16 , 21 , 39 ] no significant benefit was reported in a trial from the md anderson cancer center [ 10 ]  . 
in summary , retrospective , nonrandomized data suggest a prolongation of survival after crt compared to stenting alone or radiotherapy alone as suggested by survival times reported in the seer analysis [ 24 ]  . 26 ( 2 years : 37 ) 5 ( 2 years : 12 ) 14 ( 5 years ) b : 30 i : 43 ( 1.5 years ) 33 ( 1 year ) 5 ( 1 year ) dose - response relationship : the relationship between the median overall survival time and the total dose used was reported by alden et al . 
following combined radiation with a total dose > 55 gy , median overall survival time amounted 24 months , with doses less than 55 gy mos dropped to 6 months , being identical with a control group without radiation . 
tumor size was described to be strongly related to overall survival after chemoradiation with a mos time of 20.5 months for patients with smaller tumors 4 cm vs 8.5 months for those with larger tumors > 4 cm , clearly addressing the need for high total doses to optimise local outcome [ 5 ]  . in summary , radiotherapy should be considered for patients with locally advanced tumors without distant metastasis to improve local control . 
this can be achieved with conventional external ( chemo ) radiotherapy , with a combination of external ( chemo ) radiotherapy , intraoperative radiotherapy ( iort ) and intraluminal brachytherapy with ir - 192 hdr as well as stereotactic radiation . 
 future perspectives in external beam radiotherapy ( ebrt ) for cholangiocarcinoma in the past the application of sufficient doses to tumors in the region of the hepatic hilum and in the liver with ebrt was severely restricted by technical difficulties to deliver high strahlenther onkol 2010 no.12 brunner tb , et al . 
 forward planned 3d - conformal radiotherapy plans with multiple segments are labour intensive and timeconsuming whereas automated optimization and inverse imrt planning have proved useful in the generation of treatment plans for partial liver radiation [ 64 ]  . 
in order to overcome difficulties with planning target volume ( ptv ) inhomogeneities the use of the concept of an equivalent uniform dose ( eud ) can be useful [ 46 ]  . 
the comparison of direct machine parameter optimization imrt with conventionally planned conformal radiotherapy showed an improved ptv coverage in about 75% of the patients and dose escalation with an average of 3.8 gy in 33% of the patients [ 18 ]  . 
structures : red = gross tumor volume ( gtv ) , light blue = clinical target volume ( ctv ) , blue = planning target volume ( ptv ) , orange = stomach . 
die strahlwinkel waren so gewhlt , dass die wegstrecken durch die gesunde leber minimiert wurden , was sich von anderen phase i / ii - imrt - studien unterscheidet , in denen eine fest vorgegebene zahl von einstrahlrichtungen in regulren winkelabstnden verwendet wurde . 
figure 1 demonstrates a highly conformal treatment plan for a patient with cholangiocarcinoma , treated on the princess margaret hospital phase i / ii protocol of highly conformal radiotherapy for hepatobiliary carcinoma and liver metastases [ 12 ] with 45 gy in six fractions , showing excellent avoidance of the liver and visceral gi structures . 
moreover , as shown in a recent report , great care must be taken to avoid late effects such as duodenal ulceration [ 38 ] and technical details such as respiratory motion control methods gain high importance in hypofractionated schedules . 
even if reported acute toxicities can be lower with hypofractionated schedules [ 38 , 47 ] , the opposite can be true for late toxicities . charged particle radiotherapy was also used to treat biliary cancers . 
in the light of conflicting data and the generally low level of evidence it is difficult to give therapeutic recommendations but the recent seer analyses corroborate the role of radiotherapy in the treatment of extrahepatic cholangiocarcinoma . 
patients who have undergone a resection without clear margins ( r1 resection ) and who are in a good performance status should be offered adjuvant ( chemo ) radiation , if possible in clinical trials . 
for patients in the palliative situation the following treatment options are at hand : palliative stenting , radiotherapy ( imrt - igrt and / or brachytherapy ) with or without concurrent chemotherapy . 
the respective decision for the approach should be taken based on the performance status of the patient and the tumor characteristics ( size and location of the primary tumor , absence or presence of distant metastasis )  . 
again , we highly recommend to include these patients into clinical trials . acknowledgement supported by the nihr biomedical research centre , oxford and mrc grant g0700730 . strahlentherapie und onkologie review article induction chemotherapy before chemoradiotherapy and surgery for locally advanced rectal cancer is it time for a randomized phase iii trial ? claus rdel1 , dirk arnold2 , heinz becker3 , rainer fietkau4 , michael ghadimi3 , ullrich graeven5 , clemens hess6 , ralf hofheinz7 , werner hohenberger8 , stefan post9 , rudolf raab10 , rolf sauer4 , frederick wenz11 , torsten liersch3 background : in the era of preoperative chemoradiotherapy ( crt ) and total mesorectal excision ( tme ) , the development of distant metastases is the predominant mode of failure in rectal cancer patients today . 
the question that needs to be addressed is how and when to apply systemic treatment with adequate dose and intensity . material and methods : this review article focuses on phase iiiii trials designed to improve 5 - fluorouracil ( 5 - fu ) - based combined modality treatment for rectal cancer patients through the inclusion of concurrent , adjuvant or , most recently , induction combination chemotherapy . 
computerized bibliographic searches of pubmed were supplemented with hand searches of reference lists and abstracts of asco / astro / estro meetings . results : after preoperative crt and surgical resection , approximately one third of patients do not receive adjuvant chemotherapy , mainly due to surgical complications , patients refusal , or investigators discretion . 
in order to be able to apply chemotherapy with sufficient dose and intensity , an innovative approach is to deliver systemic therapy prior to preoperative crt rather than adjuvant chemotherapy . 
emerging evidence from several phase ii trials and , recently , randomized phase ii trials indicate that induction chemotherapy is feasible , does not compromise crt or surgical resection , and enables the delivery of chemotherapy in adequate dose and intensity . 
although this approach did not increase local efficacy in recent trials ( e.g. , pathological complete response rates , tumor regression , r0 resection rates , local control ) , it may help to improve control of distant disease . 
 conclusion : whether this improvement in applicability and dose density of chemotherapy will ultimately translate into improved disease - free survival will have to be tested in a larger phase iii trial . key words : rectal cancer induction chemotherapy chemoradiotherapy strahlenther onkol 2010 ; 186 : 65864 doi 10.1007 / s00066 - 010 - 2194 - 2 induktionschemotherapie vor radiochemotherapie und operation beim lokal fortgeschrittenen rektumkarzinom : zeit fr eine randomisierte phase - iii - studie ? hintergrund : nach einfhrung der properativen radiochemotherapie ( rct ) und der totalen mesoerektalen excision manifestieren sich rezidive beim rektumkarzinom am hufigsten als fernmetastasen . 
 1klinik fr strahlentherapie und onkologie , universitt frankfurt , frankfurt am main , germany , 2klinik und poliklinik fr innere medizin iv , universitt halle , halle , germany , 3klinik fr allgemeinund visceralchirurgie ; universitt gttingen , gttingen , germany , 4strahlenklinik , universitt erlangen , erlangen , germany , 5klinik fr hmatologie , onkologie und gastroenterologie , kliniken maria hilf gmbh , mnchengladbach , germany , 6klinik fr strahlentherapie und radioonkologie , universitt gttingen , gttingen , germany , 7iii . 
medizinischen klinik hmatologie und internistische onkologie , universittsmedizin mannheim , mannheim , germany , 8chirurgische klinik , universitt erlangen , erlangen , germany , 9chirurgische klinik , universittsmedizin mannheim , mannheim , germany , 10klinik fr allgemeinund visceralchirurgie ; klinikum oldenburg , oldenburg , germany , 11klinik fr strahlentherapie und radioonkologie , universittsmedizin mannheim , mannheim , germany . 
 received : may 7 , 2010 ; accepted : september 27 , 2010 published online : november 30 , 2010 strahlenther onkol 2010 no 12 urban & vogel rdel c , et al . 
use of induction chemotherapy in locally advanced rectal cancer material und methoden : der bersichtsartikel beschreibt phase iiiii studien , deren ziel es war , die allein 5 - fu - basierte multimodale behandlung durch hinzunahme einer kombinations - chemotherapie , simultan zur radiotherapie , adjuvant oder als induktionstherapie , zu verbessern . 
dazu diente eine suchabfrage in pubmed , in referenzlisten publizierter arbeiten sowie abstrakts von asco / astro / estro - konferenzen . ergebnisse : nach properativer rct und operation erhalten etwa ein drittel aller patienten wegen postoperativer komplikationen , patientenseitiger ablehnung oder entscheidung des betreuenden arztes keine adjuvante chemotherapie . 
eine vielzahl an phase ii - studien , und zuletzt auch randomisierter phaseii - studien , zeigte , dass dieses konzept durchfhrbar ist , die anschlieende rct und operation nicht kompromittiert sowie die systemische komponente in adquater dosis und intensitt applizierbar macht . 
wenngleich dadurch die lokale wirksamkeit ( histopathologisch besttigte komplettremission , tumorregression , r0 - resektionsrate , lokale kontrolle ) nicht verbessert wurde , knnte sich dieses vorgehen positiv auf die systemische tumorkontrolle auswirken . 
 schlsselwrter : rektumkarzinom induktionschemotherapie radiochemotherapie introduction radiotherapy ( rt ) or chemoradiotherapy ( crt ) and surgical resection are important elements of multimodality treatment for patients with locally advanced rectal cancer . 
the optimum sequence of these modalities has been addressed in several randomized trials , and preoperative rt / crt has been shown to be superior to postoperative treatment for a variety of endpoints [ 24 , 30 , 32 ]  . 
 newer generation chemotherapeutics , such as oral fluoropyrimidines , oxaliplatin , irinotecan , as well as molecularly targeted agents ( cetuximab , bevacizumab ) have been incorporated into phase iii studies for preoperative crt protocols ( for review see [ 21 , 28 ] )  . 
interestingly , early results from the accord 12 / 0405 - prodige 2 and star trial did not confirm a significant improvement of early endpoints , such as the pcr rate , with the addition of oxaliplatin to preoperative 5fu - based crt [ 1 , 13 ]  . 
 given the fact that the cumulative doses of the new drugs reached during preoperative rt are substantially lower than in adjuvant colon cancer trials and are probably not able to sufficiently reduce distant metastases , the question that needs to be addressed is how and when to apply systemic treatment with adequate dose and intensity . 
in the eortc 22921 trial , postoperative chemotherapy with 5 - fu and folinic acid had a nonsignificant influence with improvement of relapse - free and overall survival [ 2 ]  . 
the quasar study tested the value of postoperative 5 - fu / folinic acid chemotherapy versus observation in ( mostly ) stage ii colon ( n = 2291 ) and rectal ( n = 948 ) cancer patients [ 26 ]  . 
there was a significant improvement of recurrence - free ( hr 0.68 , 95% ci 0.520.88 , p = 0.004 ) and overall survival ( hr 0.77 , 95% ci 0.541.00 , p = 0.05 ) with the addition of postoperative chemotherapy for all 948 rectal cancer patients . 
 in patients treated with 55 gy preoperative rt , post - operative chemotherapy has not been evaluated so far but is currently being investigated in a randomized trial ( script , simply capecitabine in rectal cancer after irradiation plus tme )  . 
 another randomized trial ( chronicle ) , which investigated postoperative chemotherapy with capecitabine and oxaliplatin versus observation only after preoperative 5 - fu - based crt , was unfortunately closed due to poor accrual . 
thus , a recent european consensus conference failed to reach a definitive recommendation regarding the use of postoperative chemotherapy after preoperative crt / rt and surgical resection [ 35 ]  . 
 two multicenter phase ii trial ( the core study , and a phase ii study from the german rectal cancer study group ) investigated the feasibility of preoperative concomitant crt with capecitabine and oxaliplatin ( capox ) plus 46 cycles of adjuvant capox chemotherapy following resection [ 27 , 31 ]  . 
the most important findings of the german phase ii trial were that only 60% of the entire cohort of 103 operated patients were able to complete all four postoperative capox cycles ( with or without dose reduction ) ; 27% didfor various reasonsnot receive any adjuvant chemotherapy . 
thus , it is evident that preoperative crt , surgical complications , and the fact that a substantial proportion of patients will have pcr or ytnm stage i and ii tumors due to downstaging effects ( or initial clinical staging errors ) compromise the possibility and willingness of patients ( and physicians ) to tolerate ( or recommend ) postoperative chemotherapy . 
 induction chemotherapy prior to preoperative chemoradiotherapy in order to be able to apply chemotherapy with sufficient dose and intensity , an innovative approach is to deliver systemic therapy prior to preoperative crt rather than adjuvant chemotherapy . 
this strategy , however , may also be associated with its own caveats , such as selection of radioresistant clones , induction of accelerated repopulation , possibly reduced compliance to crt , and a substantial delay of definitive surgery [ 15 ]  . 
the largest series of chau and colleagues ( first published in 2006 with 77 patients , updated 2010 with 105 patients ) examined the use of four cycles of induction capecitabine plus oxaliplation ( capox ) followed by crt with capecitabine [ 7 , 8 ]  . 
5 - fu : 5 - fluorouracil ; mmc : mitomycin c ; cr : complete response ; pr : partial response ; sd : stable disease ; bid : twice daily ; pd : progressive disease ; pcr : pathological complete response ; ct : chemotherapy ; rt : radiotherapy . 
phase - ii - studien mit induktionschemotherapie vor properativer radiochemotherapie mit oder ohne adjuvanter chemotherapie bei patienten mit einem rektumkarzinom . treatment toxicity / surgical morbidity response comments series chau et al . 
 2003 [ 6 ] inclusion criteria t3 / t4 nx / + induction ct ( ict ) : 5 - fu 300 mg / m 12 weeks , mmc 7 mg / m every 6 weeks crt : starting week 13 , 5 - fu 200 mg / m during rt 50.454 gy surgery : 46 weeks after crt adjuvant ( act ) : 5 - fu 300 mg / m 12 wks , mmc 7 mg / m every 6 weeks ict : g3 / 4 : 25% crt : g3 / 4 28% ( skin ) surgery : 1 death ( anastomotic leak with multiorgan failure ) , 5 further complications ict : 1 cr , 9 pr , 26 sd , 0 pd objective response : crt : 6 cr , 23 pr , 5 sd , 2 pd objective response : surgery : 1 pcr , 82% r0 ict : 3 cr , 75 pr , 16 sd , 0 pd objective response : crt : 15 cr , 78 pr , 4 sd , 0 pd objective response : surgery : pcr 20% ; 5 - year progressionfree survival : 64% ict : not given crt : not given surgery : ypt0 : 29% 2224 weeks from start of treatment to surgery : 2 developed m1 before surgery 2224 weeks from start of treatment to surgery : no pd . after amendment for cardiovascular safety , only 1 further fatal pulmonary embolism 1416 weeks from start to surgery . 
 2009 [ 16 ] nonresectable colorectal carcinoma t4nxm0 - 1 ; 41 pts rectal ict : g3 / 4 : 11% diarrhea crt : g3 / 4 : 24% diarrhea . 1 pt died due to myocardial infarction ict : not given crt : 62% cr or pr surgery : 38 / 49 pts received surgery ; ypt0n0 : 13% only 15% of the pts obtained all ct cycles without any dose reduction strahlenther onkol 2010 no 12 rdel c , et al . 
a major concern of this phase ii study , however , is that nine patients had cardiac and thromboembolic toxic effects , leading to four deaths ( plus one death from neutropenic colitis ) during induction chemotherapy . 
although after amendment of the protocol ( patients with a previous history of stable angina , arrhythmia , and coronary syndrome were then excluded ) only one further fatal pulmonary embolism occurred , this high incidence of fatal toxicity may well be associated with a higher susceptibility of patients with bulky pelvic tumors to such complications . 
other trials with induction chemotherapy ( table 2 ) , however , did not confirm such a high number of early fatal events . recently , a spanish randomized phase ii trial was developed comparing the induction chemotherapy approach with conventional preoperative crt followed by surgery and postoperative chemotherapy ( figure 1 ) [ 10 ]  . 
whether this improvement in applicability and dose density of chemotherapy will ultimately translate into improved disease - free survival will have to be tested in a larger phase iii trial . 
 another randomized phase ii study from belgium tested two cycles of modified folfox6 regimen ( oxaliplatin 100 mg / m , folinic acid 400 mg / m , 5 - fu bolus 400 mg / m followed by 2 g / m as continuous infusion , d1 and d15 ) before preoperative crt ( 45 gy with 5 - fu 250 mg / m / day continuous infusion during rt ) versus the same schedule of preoperative crt alone [ 20 ]  . 
thus , the paradigm that induction chemotherapy prior to crt may not increase local efficacyas validated in several tumor sites [ 15 ] may well apply to rectal cancer , too . 
the design of this trial was similar to the german cao / aro / aio - 94 and was launched to demonstrate that preoperative crt is superior to postoperative crt . 
 unlike the german trial , preoperative treatment consisted of induction chemotherapy ( 6 weeks of 5 - fu / folinic acid ) followed by crt ( 50.4 gy plus 5 - fu / lv in week 1 and week 5 of rt ) and surgery plus four adjuvant cycles of 5 - fu / lv . 
 as the 5 - year cumulative incidence of locoregional recurrence was 10.7% in each arm , it is tempting to speculate that the early onset of induction chemotherapy may have contributed to reduce distant recurrences in this trial . 
randomisierte phase - ii - studie : grupo cancer de recto 3 fr patienten mit nach mrt - kriterien ungnstiger prognose ( tumor 2 mm von der mesorektalen faszie entfernt liegend , tief - sitzendes t3 , t3n + , t4 rektumkarzionm ) [ 10 ]  . strahlenther onkol 2010 no 12 rdel c , et al . 
these include the role of short - course rt [ 23 , 36 ] , the omission of preoperative rt / crt for selected patients [ 4 ] or applying neoadjuvant chemotherapy alone without rt [ 11 , 34 ] , less radical surgery [ 12 ] or even a wait - and - see strategy for ( completely ) responding patients [ 17 ]  . 
moreover , clinical factors beyond the tnm stage , e.g. , the circumferential resection margin , as assessed on mri [ 29 ] or pet - ct [ 25 , 37 ] , and molecular markers that may help to stratify patients for the respective alternatives , as currently investigated by the klinische forschergruppe kfo 179 in gttingen [ 14 , 19 ] , remain active and promising areas of clinical investigation . 
 given the fact that the predominant site of failure after combined modality treatment in rectal cancer is systemic rather than local , it is the opinion of the authors to embark on a trial that specifically addresses this very important clinical problem for rectal cancer patients . 
emerging evidence from several phase ii trials and , recently , randomized phase ii trials , indicate that induction chemotherapy for rectal cancer patients is feasible , does not compromise crt or surgical resection , and enables chemotherapy to be delivered in adequate dose and intensity . 
 strahlentherapie und onkologie original article collection and evaluation of incidents in a radiotherapy department a reactive risk analysis maurizio portaluri1 , 2 , fulvio italo maria fucilli3 , emilio antonio luca gianicolo2 , francesco tramacere1 , maria carmen francavilla1 , cristina de tommaso1 , roberta castagna1 , giorgio pili3 purpose : to report on the use of an internal system for incident reporting . patients and methods : from october 2001 until june 2009 , data on incidents were collected in the radiotherapy department ( rt ) by means of an incident reporting worksheet . 
the risk analysis was based on the us navy method of mishap cause investigation , the human factors analysis and classification system ( hfacs )  . results : 37 incidents over 5 , 635 treatments were collected . 
of the incidents , 20 involved deviation of the dose to the patient ; only 6 showed clinical evidence of overdosage , while 2 of them showed permanent evidence of overdosage . 
the highest number of correction procedures was necessary in the phases of dose prescription and dose calculation . conclusion : collecting and analyzing internal incidents improves the operative procedures used in the department . key words : patient safety radiation protection radiotherapy accident radiotherapy error radiotherapy incident quality assurance strahlenther onkol 2010 ; 186 : 6939 doi 10.1007 / s00066 - 010 - 2141 - 2 datenerhebung und evaluation von ereignissen in einer strahlentherapieabteilung : eine reaktive risikoanalyse ziel : bericht ber den gebrauch eines internen systems zur ereignismeldung . patienten und methoden : von oktober 2001 bis juni 2009 wurden daten ber ereignisse in der strahlentherapieabteilung ( rt ) anhand eines arbeitsblattes ereignisbericht gesammelt . 
die risikoanalyse basierte auf der us navy methode der mishap cause investigation , the human factors analysis and classification system ( hfacs )  . ergebnisse : 37 ereignisse bei 5635 behandlungen wurden erfasst . 
davon waren 20 abweichungen von dosierungen , die den patienten verabreicht wurden , nur 6 wiesen klinische anzeichen von berdosierung auf ; zwei von diesen zeigten permanente anzeichen von berdosierung ( tabellen 1 und 2 )  . 
die meisten korrekturen waren in der dosisverschreibungsphase und der dosiskalkulationsphase ntig ( abbildung 4 )  . schlussfolgerung : das erfassen und analysieren von internen ereignissen verbessert die angewandten operativen prozeduren in der abteilung . schlsselwrter : patientensicherheit strahlenschutz ereignisse strahlentherapie fehler strahlentherapie qualittssicherung 1department of radiotherapy , a . 
perrino general hospital , asl brindisi , italy . received : march 3 , 2010 ; accepted : june 14 , 2010 published online : november 30 , 2010 strahlenther onkol 2010 no . 
learning from incidents in rt by means of their reporting introduction according to the international atomic energy agency ( iaea ) safety standards , an incident is any unintended event which includes operative errors , equipment failures , initiating events , accident precursors , near misses or other mishaps , malicious or non - malicious unauthorized acts , the consequences or potential consequences of which are not negligible from the point of view of protection or safety . and true frequency or absolute frequency of incidents may not be determined . 
the investigation of an incident and a near miss is defined as a potential significant event that could have occurred as the consequence of a sequence of actual occurrences , but did not occur owing to the plant conditions prevailing at the time [ 16 ]  . international safety guidelines [ 29 ] have been developed and are regularly updated to deal with radiotherapy ( rt ) errors related to equipment and dosimetry . 
however , there is still no consensus on how to best deal with errors not covered by regular system quality assurance checks . research on rt safety focuses on analyses of adverse events and near misses [ 12 , 13 , 31 ] as these might lead to the identification of latent problems and weak links in a system that lies dormant for some time and then combines with a local trigger to create an incident [ 11 ]  . 
although detailed reports of some major adverse clinical radiation events during the last 30 years [ 5 , 9 , 10 , 17 , 20 , 26 ] have been published , it is likely that many more have occurred but either went unrecognized or failed to be reported to the regulatory authorities or were not published in the literature [ 27 ]  . 
random errors may affect individual patients and are more difficult to discover and prevent . the voluntary reporting system does not represent a true cross - section of all errors that occur . 
learning from incidents in rt by means of their reporting the identification of causal factors may prevent the incident from recurring . in recent years , many tools and methods of incident analysis have been developed with the goal of identifying safetysystem failures and improving protective barriers . 
 in the pro - active approach , critical points in various steps of the existing process and procedures are highlighted [ 68 , 19 , 21 , 28 , 30 ]  . 
this approach permits the identification of all causal factors of an incident [ 3 , 12 , 23 ]  . using the collected data , we performed a study to highlight any failures in the process leading to radiation treatment to test and improve the efficiency of current safety procedures in our rt department and supply information to an online post - incident database . 
a reactive risk analysis was performed on these data , based on the us navy method of investigation and taxonomy of mishap causes , the human factors analysis and classification system ( hfacs ) [ 15 ] , developed based on reasons model of latent and active failures [ 22 ] and adapted to an rt environment . patients and methods data collection an incident reporting worksheet was developed to collect the incidents discovered at our center . 
in order to allow for a complete description of the incident , the worksheet comprised the following variables used to describe every aspect of an incident : body site , machine and energy , phase of rt procedure , description of incident , how discovered , date of incident , date of discovery , staff member involved in incident and staff member who discovered it ( only qualification )  . data analysis the staff involved in the radiation therapy department and in the medical physics department were invited to highlight every type of incident , committed by him - / herself or other colleagues , and to provide a full description of the incident . 
the entire staff was assured that no blame or liability would derive from incident detection . each incident was first analyzed by the head of the medical physics department , then the head of the rt department recorded any dose deviation , avoidance of a harmful incident , the need to partially or totally change a procedure , or occurrence of harm , and its communication to the patient . once discovered , events were classified according to the table 1 . 
events 12 breast 11 head and neck 6 thorax 6 pelvis 1 bone 1 brain 12 prescription 10 dose calculation / data transfer 8 simulation / ct 7 set - up / treatment 17 follow - up 12 set - up / treatment 6 simulation / ct 1 prescription 1 dose calculation / data transfer 16 radiation oncologist 10 medical physicist 10 radiation therapist 1 nurse 25 radiation oncologist 8 radiation therapist 2 medical physicist 2 nurse dose deviation information to the patient correction of internal procedures near misses 20 yes 17 no 25 no 12 yes 20 no 17 yes 24 yes 13 no ed dose to tissues outside the ptv were enrolled in this group . not avoiding a major incident because even if undiscovered , the event would have had no serious consequences ( event not avoiding incident , enai ) , for example , forgetting to make an appointment for the patient after simulation or to schedule portal vision acquisition ; or incomplete ct acquisition which needs repetition . possibility of : risk analysis avoiding a major incident near misses ( nm )  . 
for instance , discovering an erroneous positioning of the isocenter prior to treatment start ; cases with dose deviation , defined as a difference between dose delivered and dose prescribed in the planning target volume ( ptv ) , or with an unintenda risk analysis was performed based on collected data . 
following reasons concept of active and latent failures [ 22 ] , the us navy developed a framework to identify holes in the defense layers of a safety systethis was called the human factor analysis and classification system ( hfacs ) and describes four levels of failure : ( i ) unsafe acts , ( ii ) prestrahlenther onkol 2010 no . 
the main levels are divided hierarchically into sublevels ( figure 1 )  . hfacs is a reactive approach and investigates incidents starting from what happened and going backwards to find the causes . 
unsafe acts closely linked to active failure , generally take two forms : errors ( skill - based , decision , and perceptual ) and violations ( a willful disregard of the rules )  . in this work , the goal is to improve the efficiency of current safety procedures in our rt department and not personnel behavior , so it was decided to ignore violations . results a total of 37 incidents were collected over 5 , 635 treatments . 
 characteristics of the incidents are displayed in table 1 : 25 were collected by radiation oncologists ( ro ) , 8 by radiation therapy technicians ( rtt ) , 2 by medical physicists ( mp ) , and 2 by nurses . 
zahl von enaiund nm - ereignissen entsprechend dem zeitraum ihres auftretens . enai dose prescription contouring dose calculation set - up / portal vision visit in treatment / follow - up figure 3 . 
zahl von enaiund nm - ereignissen entsprechend dem zeitraum ihrer entdeckung . critical phases in which enai occurred are reported in figure 2 in comparison with nm ; dose prescription and dose calculation seem to be the most critical phases of the entire process . 
in particular , 11 nm were discovered during patient set - up / portal imaging verifications and 7 nm were found by means of patient - in - treatment visits . 
the rt phases of the process in which events occurred according to the number of procedure corrections are shown in figure 4 ; dose prescription and dose calculation had the highest number of corrections . enai were discovered on average within 75 days ( range , 0420 days ) from the day of enrollment ; nm were discovered on average within 22 days ( range , 0201 days )  . 
incorrect data input in the rvs ( record and verify system ) and the use of an improper treatment field ( including wrong treatment field size , the wrong treatment field junction , the wrong mlc ( multileaf collimator ) placement and wrong dose normalization for a totally asymmetrical field ) were recurrent causal factors for incidents . according to the hfacs framework , at the unsafe acts level , there strahlenther onkol 2010 no . 
learning from incidents in rt by means of their reporting procedural revision we re two types of incidents linked to faulty treatment : decision errors and skill - based errors . 
skill - based errors ( n = 10 ) were associated with attention failure and memory failure , while decision errors ( n = 20 ) were associated with improper procedural execution . 
 the remaining seven incidents ( mistakes ) were associated with attention failure ( figure 1 )  . at the precondition level , all the incidents were attributed to substandard conditions of operators ( and in particular to the sublevel adverse mental state ) ; specifically , 10 were associated with loss of situational awareness , 24 to distracted / overconfident behavior , and 3 to mental fatigue . at the unsafe supervision level , incidents were associated with inadequate supervision ( failed to provide oversight ) and to planned inappropriate operations ( failed to provide correct data ) ( figure 1 )  . 
incidents were attributed to the last level ( organizational influences ) as follows : organizational climate , organizational process , resource / acquisition management ( figure 1 )  . discussion taxonomies for human performance failures have been used since the middle of the 19th century . 
reason [ 22 ] reviewed the development of such taxonomies and presented his own , very comprehensive systeother taxonomies of note were developed by norman [ 19 ] , rasmussen [ 21 ] , and van der schaaf et al . 
in our data , the most frequent initiating events were incorrect data for dose calculation and incorrect patient dose calculation ( 22% ) , incorrect treatment set - up and incorrect treatment procedures ( 21% ) , incorrect calibration beam ( 14% ) , equipment failure , or equipment design faults ( 12% )  . studies in rt practice have shown that development of a comprehensive quality assurance ( qa ) system , including an explicit and uniform protocol for implementation and timely assessment of error rate , may reduce the level of incidents [ 14 , 33 ]  . 
changes in working practices during that time included the following : relocation of different procedures , increased use of specialist staff , and adaptation of working practices to reflect the requirements of new technology through regular discussions between staff . 
in another institution , real - time audits of 3 , 052 treatment plans over a period of 8 years provided important direct and indirect patient benefits that went beyond normal physidose prescription contouring dose calculation set - up / portal vision figure 4 . 
of all incidents without any known adverse events to patients , 9% ( n = 420 ) were related to the planning stage , 38% ( n = 1732 ) were related to transfer of information , and 18% ( n = 844 ) to the treatment delivery stage . 
the remaining 35% of incidents occurred in combinations of multiple stages [ 15 ]  . systematic minor errors often suggest problems with infrastructure or information management that may carry an inherent risk of more serious errors . 
learning from incidents in rt by means of their reporting [ 29 ] claimed that detection and correction of near misses through practice of a systematic multilayered pretreatment check - up system in their center was preventing the occurrence of about 14 adverse events per 1 , 000 treatment plans . in the experience described in this paper , the ro was the professional figure mostly involved in both making and discovering errors . 
this result was expected and due to the fact that the italian rt liability law demands that the ro control the whole process ; in addition , the ro is involved in most rt process phases . 
20 events consisted of the administration of unintended dosage to the patient ; only 6 had clinical evidence of overdosage with two patients having permanent damage . in addition , 24 collected incidents were nm . 
dose prescription and dose calculation were the phases in which the majority of events occurred and , therefore , deserve greater attention from an organizational point of view . risk analysis by means of hfacs showed that a majority of incidents were due to inadequate supervision ( unsafe supervision level ) , while others were due to a deficiency in the rules ( resource / acquisition management level ) and required correction of some procedures . we agree with the statement that each rt service should individually and regularly examine its risk profile , and incidents as well as near misses should be prospectively collected , measured , and categorized [ 25 ]  . 
in this way high - level decision makers and operators tend to inherit system defects created by poor design , incorrect installation , faulty maintenance , and poor management decisions , rather than being the main instigators of an incident [ 24 ]  . experience has confirmed the usefulness of regular incident collection and analysis in an rt department . 
thus , department meetings have been scheduled for the quarterly analysis , presentation , and discussion of data . procedural improvements commonly involved reinforcing supervision of dose calculation , data transfer , and portal vision revision by means of a double - check systewith regard to the dose prescription phase , the prescription was rechecked in a morning meeting on simulation day and on the day therapy was started . the limitations of the study concern the random collection of incidents . 
this is a characteristic of each reactive system , which could be overcome by implementing proactive systems instituted by the management . acknowledgements we wish to thank alison frank for assistance in revising and editing the english manuscript and antje behrens for editing the german text . strahlentherapie und onkologie editorial intraoperative radiotherapy as accelerated partial breast irradiation for early breast cancer beware of one - stop shops ? marie - luise sautter - bihl1 , felix sedlmayer2 , wilfried budach3 , jrgen dunst4 , rita engenhartcabillic5 , rainer fietkau6 , petra feyer7 , wulf haase8 , wolfgang harms9 , claus rdel10 , rainer souchon11 , frederik wenz12 , rolf sauer6 intraoperative radiotherapy ( iort ) was originally introduced in breast cancer treatment as an anticipated boost during the procedure of breast conserving surgery ( bcs )  . 
under the assumption that the majority of in - breast tumor recurrences ( ibtr ) occur in the originally affected site , accelerated partial breast irradiation ( apbi ) as the sole treatment modality was initiated in several studies and with different techniques , one of which was iort first with electrons , later also with conventional x - rays [ 29 ]  . the question whether and for whom the gold standard of wbi may be replaced by apbi especially iort alone has recently been one of the most controversial issues of adjuvant therapy for breast cancer . 
 [ 35 ] presenting shortterm results of single shot iort with electrons ( eliot ) and with an orthovoltage system ( targit ) , respectively , have further invigorated this discussion as illustrated by several letters to the editor commenting on the targit study . 
 [ 35 ] indicate their results of iort alone as an alternative to wbi for selected patients and one editorial even proclaims it as standard [ 6 ] , all the authors of the respective letters [ 10 , 16 , 27 , 33 ] strongly disagree with this conclusion . 
the calculation of the required sample size was based on the assumption of a 5 - year local recurrence rate ( lrr ) of 6% according to literature data from 1999 . 
after wide local excision , iort was performed with 50 kv x - rays in a single fraction of 20 gy prescribed to the surface of the tumor bed ( 57 gy at 1 cm )  . 
while 854 patients ( 86% ) received apbi alone , 142 patients ( 14% ) had apbi plus wbi ; the control group ( wbi 4056 gy boost 1016 gy ) comprised 1 , 025 patients . 
the kaplanmeier estimate of ibtr at 4 years was 1.2% in the iort arm and 0.95% in the wbi group ( ns ) key words : breast cancer accelerated partial breast irradiation intraoperative radiotherapy whole breast irradiation schlsselwrter : mammakarzinom akzelerierte teilbrustbestrahlung intraoperative strahlentherapie ganzbrustbestrahlung strahlenther onkol 2010 ; 186 : 6517 doi 10.1007 / s00066 - 010 - 8001 - 2 published online : november 29 , 2010 1municipal hospital , karlsruhe , germany , 2university hospital , landeskrankenhaus salzburg , austria , 3university hospital dsseldorf , germany , 4university hospital schleswig holstein , lbeck , germany , 5university hospital gieen and marburg , marburg , germany , 6university hospital erlangen , germany , 7klinikum neuklln , berlin , germany , 8formerly st . 
 [ 36 ] presented results of a clinical study comprising 1 , 822 patients treated according to the eliot concept , but outside the randomized trial which still awaits publication . 
 at 6 years after treatment , an actuarial ibtr rate of 6.4% was observed , 2 / 3 of which were counted as true recurrences , whereas the other 1 / 3 were interpreted as so - called second ipsilateral cancers mainly occurring outside the index quadrant . 
 in the targit trial , patient selection was stricter and additional use of wbi was performed in 15% of the patients originally allocated for apbi when adverse prognostic factors appeared in the postoperative pathologic examination . 
moreover , it is noteworthy that one third ( n = 672 ) of the patients underwent apbi after pathological examination and were , thus , exposed to a second surgical intervention with no other reason than receiving targit treatment comparison of iort and wbi results the authors interpretation of these results as a potential promise to replace standard treatment raises concerns regarding the validity of conclusions drawn after a median follow - up bartelink et al . 
so far , the preliminary results of the targit trial are in line with the experience of the eortc boost trial [ 7 ] for patients > 50 years ( figure 1a )  . 
vergleich der ibtr zwischen ganzbrustbestrahlung + boost und eliot ( a ) und vergleich der ibtr zwischen ganzbrustbestrahlung ( hughes , fyles ) und eliot ( b ) irradiation and a plateau is only reached after 10 years . 
referring to these data , it may be hypothesized that in the targit trial only a minority of events have occurred so far , even more , as most patients received endocrine therapy , which may reduce or delay the onset of local recurrences [ 9 , 13 , 21 ]  . 
this is especially true for patients < 50 years , in whom the recurrence rate is similar to what would be expected with breast conserving surgery without any radiotherapy [ 11 ]  . 
moreover , all patients were exclusively treated with iort , whereas in the targit trial an additional wbi was performed in 14% of the patients , whose final histology report had revealed unexpected risk factors . 
again , the insufficient follow - up does not permit either final interpretation of the results or of the differences between the two trials . time distribution of in - breast recurrences following wbi with doses around 50 gy boost , median times to the appearance of true local recurrences are estimated somewhere between 40 months [ 15 ] and 65 months [ 9 ] , and out - quadrant relapses or second primaries occur even later [ 13 , 15 ]  . 
the william beaumont group [ 21 ] analyzed 1 , 448 patients and found median times to all ibtr of 6.5 years , for tumor bed recurrences 5.7 years , but 7.4 years for lesions remote from the index tumor . 
one might speculate that in both settings , targit as well as eliot , recurrences in remote quadrants will be more frequent and their clinical appearance slightly earlier , since subclinical tumor foci have not been completely eliminated or at least reduced in number and size . 
during the first few years of the follow - up , the incidence of out - quadrant recurrences might be comparable to the results following wbi not last due to the widespread use of systemic therapy with its potential to prolong the interval to clinical detectability clearly beyond 5 years [ 14 ]  . 
the gap to post - wbi results might then widen continuously . in this context , an interesting aspect of the eliot results is the observation of the 1.32% secondary ipsilateral cancers after a median follow - up of 36 months . 
in a recent subgroup analysis of the royal marsden hypofractionation trial [ 15 ] , ibtr were evaluated with the aim to differentiate true lr and new primaries ( np )  . 
internationale einschlusskriterien fr die targit - studie . inclusion criteria for targit international unifocal tumor ( mammography , sonography ) age ( years ) histology axillary nodes risk - adapted wbi > 45 < 3.5 cm germany > 50 < 2.0 cm invasive ductal carcinoma invasive ductal carcinoma second surgery for iort ( post pathology stratum ) permitted not permitted other histology , eic , re - excision for clear margins after iort other histology , eic , re - excision for clear margins after iort close margins < 1 cm , l1 , pn + 3537 months for likely or true local recurrences . 
these intervals suggest that the tumors described as second ipsilateral cancers in the eliot trial may have been misclassified and were in fact tumor foci beyond the range of radiation becoming clinically manifest after a relatively short followup . 
it is assumed that a dose of 20 gy at the applicator surface is equivalent to a fractionated dose of 70 gy [ 35 ]  . as evidence for this hypothetic equivalence , the authors cite their own model calculations [ 17 ] and data from in vitro experiments [ 5 , 8 ]  . 
relevant data for clinical rbe comparison between 50 kv and megavolt radiation do not exist , as orthovolt for tumor treatment was abandoned in the 1960s with the advent of cobalt and accelerators . 
moreover , it is disputable whether the linear quadratic model used for comparison of fractionation schedules is applicable for single fractions > 10 gy [ 20 ]  . ideally assuming , all the hypotheses of the authors were consistent and the physical targit dose of 20 gy would be equivalent to 70 gy of fractionated rt , already at a 1 cm depth , the remaining physical dose of 5 gy could maximally be biologically equivalent to 18 gy ( fractionated rt ) and at 2 cm only to 6.3 gy [ 17 ]  . 
of those , 17% were within a distance of < 2 cm from the tumor , whereas 42% were detected at a distance > 2 cm [ 18 ]  . 
although this investigation contained some patients with an unfavorable risk profile , the data indicate that residual tumor cells may be spatially distributed beyond the area of effective dose coverage which can be delivered especially with orthovolt radiotherapy . in contrast , in the eliot concept a larger volume is irradiated [ 23 ] with higher and more homogenously delivered doses , together with more extensive surgery . 
still with better coverage of the adjacent surroundings , tumor foci at distances > 2 cm as described above may also well be underdosed with iort as a sole treatment modality . 
 [ 35 ] emphasize that one main advantage of apbi is avoiding the time duration of a standard whole - breast irradiation particularly for patients who are working or living at a remote distance from radiotherapy facilities . 
women who sacrifice their breast to circumvent radiotherapy are absolute exceptions !  . hence , for the panel an optimal therapeutic effectiveness with regard to long - term tumor control , safety , and minimal side effects , furthermore , remains the primary goal in breast cancer treatment and is not outweighed by arguments regarding time saving and cost reduction . 
balancing convenience aspects against the continuously improving cure rates and excellent cosmetic results provided by modern techniques of wbi [ 22 , 28 , 34 , 39 ] , no chances should be taken at the expense of patients before equivalence is definitely proven . 
12 comments and conclusions strahlentherapie und onkologie original article high - dose ( 80 gy ) intensity - modulated radiation therapy with daily image - guidance as primary treatment for localized prostate cancer pirus ghadjar , nicole gwerder , peter manser , jacqueline vock , axel madlung , roberto mini , daniel m . 
aebersold1 purpose : to report acute and late toxicity in prostate cancer patients treated by high - dose intensity - modulated radiation therapy ( imrt ) with daily image - guidance . patients and methods : from 06 / 200403 / 2008 , 102 men were treated with 80 gy imrt with daily image - guidance . 
toxicity was scored according to the ctc scale version 3.0. results : median age was 69 years and median follow - up was 39 months ( range , 1661 months )  . 
acute and late grade 2 gastrointestinal ( gi ) toxicity occurred in 2% and 5% of patients , respectively , while acute and late grade 3 gi toxicity was absent . 
at the end of follow - up , the incidence of late grade 2 and 3 gu toxicity decreased to 7% and 1% , respectively . conclusion : gi toxicity rates after imrt with daily image - guidance were excellent . 
gu toxicity rates were acceptable and strongly related to pgum . key words : high dose imrt daily image - guidance prostate cancer strahlenther onkol 2010 ; 186 : 68792 doi 10.1007 / s00066 - 010 - 2180 - 8 intensittsmodulierte hochdosis - radiotherapie ( 80 gy ) mit tglicher image guidance als primrtherapie beim lokalisierten prostatakarzinom ziel : beschreibung der akutund sptnebenwirkungen bei patienten mit prostatakarzinom , die mit intensittsmodulierter hochdosis - radiotherapie ( imrt ) und tglicher image guidance behandelt wurden . patienten und methodik : von 06 / 2004 bis 03 / 2008 wurden 102 mnner mit 80 gy imrt behandelt . 
akute und spte grad - 2 - gastrointestinale ( gi ) nebenwirkungen traten in 2% und 5% der flle auf ; akute oder spte grad - 3 - gi nebenwirkungen wurden nicht beobachtet . 
am ende des nachbeobachtungszeitraumes sank die inzidenz von spten grad - 2 und - 3 - gu nebenwirkungen auf 7% und 1% . schlussfolgerung : die gi nebenwirkungsrate nach imrt mit tglicher image guidance war exzellent . 
gu nebenwirkungsraten waren akzeptabel und standen in engem zusammenhang den urogenitalen beschwerden vor radiotherapie . schlsselwrter : hochdosis imrt tgliche image guidance prostatakarzinom 1department of radiation oncology with division of medical radiation physics , inselspital , bern university hospital , and university of bern , bern , switzerland . received : may 25 , 2010 ; accepted : september 16 , 2010 published online : november 30 , 2010 strahlenther onkol 2010 no . 
high dose imrt for prostate cancer introduction significantly increased gastrointestinal ( gi ) toxicity was the major drawback of three - dimensional conformal radiotherapy ( 3d - crt ) - based dose - escalation in the treatment of prostate cancer ( pca ) [ 1 , 4 , 9 , 15 , 22 , 31 ]  . 
the development of intensity - modulated radiation therapy ( imrt ) allowed better preservation of the organs at risk and significantly decreased gi toxicity compared to 3d - crt [ 6 , 18 , 30 ]  . 
to account for the interfractional and intrafractional movement of the prostate [ 13 , 21 , 22 , 29 ] , image guidance was shown to be essential to avoid large safety margins around the clinical target volume ( ctv )  . 
this report presents the pretreatment gi and genitourinary ( gu ) morbidity ( pgum ) rates as well as acute and late gi / gu toxicity and early biochemical control data of 102 patients treated using high - dose imrt with daily image - guidance . 
 patients and methods patient selection and characteristics a total of 108 consecutive men with histologically proven pca and cn0 cm0 status were treated by imrt with daily image guidance after obtaining informed consent in accordance with the standards of the local ethics committee . 
the pretreatment staging included a digital rectal examination , transrectal ultrasound ( trus ) , biopsy with specification of the gleason score , prostate - specific antigen ( psa ) , computed tomography ( ct ) and / or magnetic resonance imaging ( mri ) , a total - body bone scan , and was defined according to the 2002 american joint committee on cancer tumor , lymph nodes , and metastasis system [ 27 ]  . 
the risk groups were as follows : low , intermediate , and high risk in 21 ( 21% ) , 28 ( 27% ) , and 53 ( 52% ) patients , respectively . 
a total of 24 / 102 ( 24% ) had undergone a transurethral resection of the prostate ( tur - p ) a median of 42 months prior to imrt ( range , 1199 months )  . 
amedian time between tur - p and imrt was 42 months ( range , 1199 months ) , in 9 patients the time interval was < 12 months ; bperiod after completion of treatment . 
adie mediane zeit zwischen tur - p und imrt betrug 42 monate ( 1199 monate ) , bei 9 patienten war das intervall < 12 monate ; bzeitraum nach abschluss der behandlung . 
if the risk for sv invasion was > 15% , as it was the case in 59 patients , the proximal third of the sv was included in the ctv electively . 
the planning target volume ( ptv ) was then delineated by encompassing the prostate with 5 mm safety margins in all directions except dorsally , where a 3 mm margin was added . 
a set of dose constraints were used and localization of the prostate prior to every rt fraction ( daily image - guidance ) was performed as previously described [ 8 , 29 ]  . 
follow - up visits were arranged 24 weeks after completion of imrt and every 36 months for the first 2 years and annually thereafter with a digital rectal examination and a serum psa level obtained at each visit . 
 biochemical no evidence of disease ( bned ) was assessed according to the phoenix criteria , defining a biochemical failure as a psa rise of 2 ng / ml or more above the nadir psa [ 24 ]  . 
pre - tx : pre - treatment ; athe highest toxicity in a patient was counted as a single event ; b during therapy and until 3 months after completion ; c maximal late toxicity > 3 months after completion of therapy ; d incidence of late toxicity at last follow - up visit . 
univariate cox regression and a multiple cox regression model with forward and backward selection was used to determine independent prognostic factors for decreased late results acute and late gastrointestinal toxicity acute grade 1 gi toxicity was experienced in 35 patients ( 34% ) , while grade 2 toxicity was observed in 2 patients ( 2% ) with diarrhea being the most commonly observed sympto acute grade 3 gi toxicity was absent ( table 2 )  . late grade 1 and 2 gi toxicity occurred in 31 ( 30% ) and 5 ( 5% ) patients , respectively , and rectal bleeding was the most commonly observed symptolate grade 3 gi toxicity was absent . 
 at the last follow - up visit , late grade 1 toxicity was present in 19 ( 19% ) patients , and no patient suffered of late grade 2 gi strahlenther onkol 2010 no . 
acute and late gi toxicity was not associated with any dvh parameter tested . acute and late genitourinary toxicity prior to treatment , 15 patients ( 15% ) had grade 2 and 2 patients ( 2% ) suffered of grade 3 pgum ( table 3 )  . 
pre - tx : pre - treatment ; athe highest toxicity in a patient was counted as a single event ; bduring therapy and until 3 months after completion ; c maximal late toxicity > 3 months after completion of therapy ; dincidence of late toxicity at last follow - up visit . 
pre - tx : vor behandlung ; adie maximal erreichte toxizitts eines patienten wurde als 1 ereignis gewertet ; bwhrend und bis 3 monate nach abschluss der behandlung ; cmaximale spttoxizitt > 3 monate nach abschluss der behandlung ; dinzidenz von spttoxizitt beim letzten nachuntersuchungstermin ( grad - 4 - gu toxizitt wurde nicht beobachtet )  . 
 at last follow - up visit , only 7 ( 7% ) or 1 ( 1% ) still complained of late grade 2 or 3 gu toxicity , respectively , being less than strahlenther onkol 2010 no . 
 rr : relative risk , ci : 95% rr confidence intervals , tur - p : transurethral resection of the prostate , imrt : intensity modulated radiation therapy , pgum : pre - treatment genitourinary morbidity . 
rr : relatives risiko , ci : 95% rr konfidenzintervalle , tur - p : transurethrale prostataresektion , imrt : intensittsmodulierte radiotherapie , pgum : urogenitale morbiditt vor behandlungsbeginn . factor univariate cox regression : ptv size > 94 cm3 vs . 
 discussion radical prostatectomy combined with pelvic lymphadenectomy is known to produce comparable tumor control rates compared to conventional dose 3d - crt in localized pca [ 5 , 16 ] , and introduction of nerve - sparing operation technique could significantly reduce the risk of associated severe stress incontinence [ 14 ]  . 
 after a median follow - up of 39 months , our results after high - dose imrt daily image - guidance are encouraging with respect to observed treatment - related toxicity . 
 concerning gu toxicity , notably , our patients suffered of a significant pgum , being of grade 2 and 3 in 15% and 2% , respectively , of the patients prior to imrt . 
 our acute toxicity rates compare favorably with those reported for 111 patients treated with imrt 78 gy within a prospective randomized trial , where the acute grade 2 and 3 gi toxicity was 41% and 8% and the acute grade 2 and 3 gu toxicity was 21% and 2% ( ctc score ) , respectively [ 19 ]  . 
 others have reported the toxicity profile ( ctc score ) after ultrahigh - dose imrt with 86.4 gy after a median follow - up of 53 months and acute grade 2 gi toxicity was 8% , acute grade 2 and 3 gu 22% and 1% , respectively , actuarial late grade 2 gi toxicity at 5 years was 4% and actuarial late grade 2 gu toxicity was 16% at 5 years [ 2 ]  . 
importantly , one has to consider that in our treatment plans the dose coverage of the ptv was defined more strictly , thus , aiming to set the v95 to > 99% ( volume of the ptv receiving at least 95% of the prescribed dose > 99% ) [ 8 ] ; however , the treatment plan criteria for 81 gy or 86.4 gy plans were v95 > 90% or v95 > 85% , respectively [ 18 ] , moreover for 81 gy and 86.4 gy , a lower single fraction dose ( 1.8 gy ) was used . 
in addition , we could also describe not only the pgum rate of our patients and its significant association with acute gu toxicity , but also its role as an independent positive predictor for decreased late gu toxicity - free survival . 
an association between previous tur - p and gu toxicity has been previously described [ 20 ]  . in our patients , ht did not influence the incidence of late gi or gu toxicity . 
 these drugs were received by most of the symptomatic patients during imrt and during follow - up ; thus , this drug therapy at least contributed to the observed decrease of late gu toxicity during time . 
however , all observed events of biochemical relapse ( 12% ) occurred in patients with highrisk features and our actuarial 5 - year biochemical relapsefree survival rates of 100% , 100% , and 68% are comparable with the 5 - year rates of 98% , 85% , and 70% described after ultrahigh - dose imrt for low - , intermediate - , and high - risk patients , respectively [ 2 ]  . we are aware of the obvious limitations of our study , being the retrospective nature of the study and limited followup . 
in the decision making for appropriate local treatment of pca , the patient should not be informed about rt but should be informed about modern rt and its associated low treatment - related acute and late toxicity . strahlentherapie und onkologie originalarbeit prognoseeinschtzung durch mr - verlaufskontrollen whrend der strahlentherapie bei glioblastom - patienten christina leitzen1 , hans h . 
schild1 , birgitta bungart1 , ulrich herrlinger2 , christiana ltter1 , thomas mdder1 , timo wilhelm - buchstab1 , heinrich schller1 ziel : trotz verbesserter therapeutischer mglichkeiten ist der klinische verlauf hhergradiger gliome bislang unbefriedigend . 
ziel war es , zu eruieren , ob dies mithilfe von mrt - verlaufskontrollen unter strahlentherapie mglich ist . patienten und methodik : 33 radiotherapeutisch behandelte glioblastom - patienten erhielten mrt - verlaufskontrollen : vor radiotherapiebeginn , nach ca . 
die mrtuntersuchungsbefunde bei 30 und 60 gy ( drei kategorien : status idem , fraglicher progress , progress ) wurden mit dem klinischen verlauf ber einen medianen zeitraum von 11 monaten korreliert . 
auf dieser grundlage kann zu diesem zeitpunkt eine anpassung der therapie diskutiert werden . schlsselwrter : glioblastom mrt strahlentherapie berleben strahlenther onkol 2010 ; 186 : 6816 doi 10.1007 / s00066 - 010 - 2156 - 8 prediction of clinical course of glioblastomas by mri during radiotherapy purpose : determine the value of mr studies in patients undergoing radiotherapy for glioblastomas pre and during radiotherapy to predict the clinical course . patients and methods : mr follow - up studies were performed in 33 patients with glioblastomas before radiotherapy , after 30 gy , after 60 gy , and in the treatment follow - up . 
findings on mr were categorized into : definite progress , questionable progress , status idepatients were followed clinically ( median for 11 months )  . results : after 30 gy 23 / 33 ( 70% ) of the mr examination showed status ide10 / 33 ( 30% ) demonstrated definite ( n = 6 ) or questionable ( n = 4 ) progress . 
 key words : glioblastoma mrt radiotherapy impact on survival radiologische klinik , fe strahlentherapie , universittsklinik bonn , deutschland , neurologische klinik , neuro - onkologie , universittsklinik bonn , deutschland . received : april 9 , 2010 ; accepted : september 16 , 2010 published online : november 29 , 2010 strahlenther onkol 2010 no . 
auch zur oft schwierigen differenzierung zwischen posttherapeutischen tumorresiduen , rezidiven und narben ist die durchfhrung von mrt - untersuchungen standard und die zustzliche durchfhrung von spektroskopieaufnahmen und perfusions - mrt - aufnahmen wird diskutiert [ 1 , 4 , 5 , 25 , 19 ]  . da sich die tumorerkrankung fast ausschlielich auf den entstehungsort begrenzt , steht die lokaltherapie im vordergrund , zunehmend kombiniert mit chemotherapeutischen manahmen . 
die derzeit aktuellen therapieschemata bestehend aus primrer operation , anschlieender lokaler radiotherapie und simultaner sowie adjuvanter chemotherapie konnten das mediane berleben auf 14 , 6 monate verbessern [ 23 , 24 ]  . 
im rezidivfall werden umstellungen der chemotherapie , re - bestrahlungen , auch als hdr - brachytherapie [ 10 , 26 ] , und operationen eingesetzt . als prognostisch relevante faktoren gelten unter anderem der allgemeinzustand , das patientenalter ( < / > 65 jahre ) [ 9 , 16 ] und das resektionsausma [ 20 ]  . 
auerdem wird ein zusammenhang zwischen der prognose und der mgmt - promotormethylierung sowie von mutationen der isocitrate - dehydrogenase - 1 der tumoren diskutiert [ 3 , 6 , 7 , 17 ]  . 
das mittlere lebensalter der 14 frauen und 19 mnner lag zum diagnosezeitpunkt bei 52 ( 2975 ) jahren . therapie nach den resektionen / biopsien dauerte es im median 3 , 5 ( 16 , 5 ) wochen bis zum beginn der strahlentherapie . 
die strahlentherapie erfolgte dreimal am tomotherapiegert , die brigen 30 patienten wurden am konventionellen linearbeschleuniger behandelt . eine simultane radiochemotherapie mit temozolomid erhielten 26 patienten , diese wurde 19 - mal im anschluss an die bestrahlung weitergefhrt . 
fnf patienten erhielten keine simultane radiochemotherapie . mrt - kontrollen mrt - untersuchungen erfolgten zu verschiedenen zeitpunkten an einem 3.0 - t - mr - system unter verwendung einer 8 - kanal - kopfspule : postoperativ , verlaufskontrollen nach ca . 
der hlfte der geplanten gesamtdosis ( im folgenden als 30 - gy - mrt bezeichnet ) und bei strahlentherapie - abschluss ( im folgenden als 60 - gy - mrt bezeichnet )  . 
das protokoll umfasste hierbei jeweils folgende berwiegend bereits im rahmen der primren tumorabklrung eingesetzte sequenzen : transversale diffusionsgewichtete echoplanar - imaging ( epi ) sequenzen , koronare und transversale fluid attenuated inversion recovery ( flair ) - aufnahmen , transversale t2 - turbo spin echo ( tse ) und transversale t1 - gewichtete spin echo ( se ) - sequenzen vor und nach intravenser kontrastmittelgabe , sowie koronare und sagittale t1 - gewichtete se nach kontrastmittelgabe . 
einmal wurde nach alleiniger biopsie keine erneute mrt - kontrolle durchgefhrt , da ein direkt vor der biopsie angefertigtes mrt als ausreichender ausgangsbefund empfunden wurde . im vergleich zur ausgangsuntersuchung wurden die befunde drei kategorien ( sicherer progress , fraglicher progress , kein progress ) zugeordnet . 
dabei wurden befunde mit zunehmender oder neu aufgetretener bluthirnschrankenstrung ohne eindeutigen tumornachweis als fraglich progredient eingestu zur weiteren auswertung wurden die patienten mit fraglichem und sicherem progress zu der gruppe ( fraglicher ) progress zusammengefasst . die mrt - ergebnisse bei 30 und 60 gy wurden mit dem weiteren erkrankungsverlauf , mrt - kontrollen als bildgebendem kriterium und dem klinischen verlauf korreliert ( abbildungen 1 bis 3 )  . 
analysis of survival time ( kaplan - meier ) of patients showing ( questionable ) progress ( gray ) and patients without change ( black ) in mri at 30 gy . 
 vergleich 30 - gyzu 60 - gy - mrt bei einer in der 30 - gy - mrt als status idem eingestuften kontrolle zeigte sich 4 - mal ein ( fraglicher ) progress nach 60 gy . 
bei zwei patienten war das rezidiv im randbereich ( zwischen gtv und ptv ) des bestrahlungsfeldes entstanden ( randrezidiv )  . die mediane berlebenszeit der patienten betrug 18 monate ( abbildung 6 )  . 
auch hier zeigt sich eine krzere berlebenszeit bei patienten mit progress im 30 - gy oder 60 - gy - mrt im vergleich zu denjenigen mit status idem . dreimal muss das vorliegen eines sogenannten pseudoprogresses in unserem patientenkollektiv in betracht gezogen werden . 
ein sicherer progress wurde bei diesen patienten erst nach mehr als 6 monaten festgestellt . fr die analyse der progressund berlebenszeiten wurde einmal das datum des ersten ( eventuellen pseudoprogresses ) und einmal das datum des spteren ( sicheren ) progresses gewhlt . 
es ergibt sich jedes mal ein frherer weiterer progress und schnellerer tod fr die gruppe der tumoren mit ( fraglichem ) progress im vergleich zu denjenigen mit status idem . diskussion trotz therapieverbesserungen , insbesondere durch integration der chemotherapie [ 8 , 18 , 23 ] , ist die prognose maligner glioblastome meist infaust [ 11 , 12 , 15 ]  . 
eine frhzeitige identifikation der patienten , die von solchen therapieumstellungen profitieren , ist wnschenswert . vor diesem hintergrund war es unser ziel , zu berprfen , ob sich mrt - verlaufskontrollen dazu eignen , die individuelle prognose abzuschtzen . 
 auch sollte , um einen pseudoprogress nicht als progress zu interpretieren , eine zustzliche absicherung durch die magnetresonanzspektroskopie erfolgen . unsere daten zeigen , dass mrt - kontrollen unter strahlentherapie eine prognoseabschtzung durchaus erlauben und zwar bereits nach 30 gy . 
die tumoren mit zu diesem zeitpunkt aufflligen kontrollen ( fraglicher oder sicherer progress ) waren im weiteren verlauf schneller progredient und die patienten verstarben frher als diejenigen mit unvernderten mrt - befunden . 
basierend auf unseren daten wrden wir eine mrt - kontrolle nach 30 gy als referenzuntersuchung zur abschtzung der weiteren prognose empfehlen . eine kontrolle erst nach abschluss der radiotherapie erbrachte in unserem kollektiv keinen zustzlichen informationsgewinn in bezug auf die prognose . 
auerdem ist zu diesem zeitpunkt eine modifikation der radio - ( chemo - ) therapie nicht mehr mglich . unter umstnden erlaubt die mr - spektroskopie eine bessere prognostische einschtzung bereits vor 30 - gy - dosis , da nicht schrankengestrte , niedriggradige tumoranteile anhand pathologischer metabolitenquotienten identifiziert werden knnen . problematisch ist die heterogenitt unseres patientenkollektivs . 
die eingruppierung der patienten in verschiedene untergruppen ergab allerdings keinen hinweis darauf , dass diese faktoren einen einfluss auf unser endergebnis haben . sicherlich mssen in weiterfhrenden studien auch faktoren wie der mgmt - promotor - methylstatus und mutationen der isocitrate - dehydrogenase - 1 mit einbezogen werden . 
 fr die hier vorgestellten patienten lag hierzu jedoch meist keine information vor . schlussfolgerungen mit mrt - verlaufskontrollen ist schon drei wochen nach beginn einer lokalen radiooder kombinierten radiochemotherapie , eine aussage zur individuellen prognose bei glioblastom - patienten mglich . 
bei patienten , die zu diesem zeitpunkt eine ( zunehmende ) bluthirnschrankenstrung oder einen progredienten tumor im vergleich zum ausgangsbefund aufweisen , wird deutlich frher eine manifeste progredienz der erkrankung diagnostiziert . 
12 strahlentherapie und onkologie original article investigations on parotid gland recovery after imrt in head and neck tumor patients markus stock1 , wolfgang drr2 , carmen stromberger1 , ulrike mock1 , susanne koizar1 , richard ptter1 , dietmar georg1 purpose : in recent years , the role of intensity - modulated radiotherapy ( imrt ) for head and neck irradiation has increased . 
the aim of the present study was to investigate changes in parotid gland function and set this in relation to absolute volumes . material and methods : 46 head and neck patients were treated by sparing at least the contralateral parotid gland . 
longer recovery times show higher ed50 values indicating partial regeneration of gland functions . key words : imrt head and neck parotid gland xerostomia scintigraphy strahlenther onkol 2010 ; 186 : 66571 doi 10.1007 / s00066 - 010 - 2157 - 7 untersuchungen zum erholungsverhalten der parotis nach imrt - bestrahlung von kopf - hals tumoren ziel : in den letzten jahren gewann die intensittsmodulierte strahlentherapie ( imrt ) bei der behandlung von kopf - hals tumoren immer mehr an bedeutung . 
ziel dieser studie war es deshalb , funktionsvernderungen zu quantifizieren und mit absoluten volumina zu korrelieren . material und methoden : 46 kopf - hals patienten wurden mit imrt behandelt und dabei wurde die kontralaterale parotis geschont . 
lngere zeitabstnde zur therapie ergaben auch hhere ed50 werte , was auf eine partielle regeneration der speicheldrse schlieen lsst . schlsselwrter : imrt kopf - hals tumore parotis mundtrockenheit szintigraphie 1department of radiotherapy , medical university vienna , vienna , austria , 2university of technology , medical faculty carl gustav carus , department of radiotherapy and radiation oncology , dresden , germany ; guest professor radiation biology , medical university vienna , austria . received : april 13 , 2010 ; accepted : september 16 , 2010 published online : november 30 , 2010 strahlenther onkol 2010 no . 
parotid gland recovery after h&n imrt introduction intensity - modulated radiotherapy ( imrt ) has become a key treatment for head - and - neck cancer due to its potential to shape isodose distributions around concave targets and to improve sparing of organs at risk ( oar )  . 
the latter is driven by inverse planning approaches and computerized optimization modules which require certain input data [ 2 , 5 , 10 , 12 , 13 , 18 , 19 , 29 , 30 , 34 , 35 ]  . 
as different dose distributions can result in the same mean organ dose , threshold dose levels have been also recommended for partial volumes of the parotid gland [ 9 , 27 ]  . 
however , it is custom in external beam therapy to use relative volumes when interpreting dosevolume histograms ( dvh ) , and consequently input parameters for optimization in imrt are based on relative volumes . 
therefore , the aim of the present study was to investigate changes in parotid gland function and parotid gland recovery as a function of absolute volume and dose levels after imrt for head and neck cancer . 
 materials and methods patients in total , 46 patients with carcinomas of the oropharynx or oral cavity , t1t4 , not crossing the midline and without evidence of contralateral neck node metastases ( n0n2b ) were included . 
because the contralateral upper part of ln level ii is at very low risk of occult metastases , this region was spared in order to limit the dose to the parotid gland . all patients were immobilized in a dedicated precision head and neck fixation system [ 11 ]  . 
for definitive rt of patients with n0 staging , a total dose of 70 gy was prescribed to the tumor and 50 gy ( dose group ii ) to the ipsiand contralateral ln . 
for post - operative rt ( dose group iv ) , 60 gy were prescribed to the tumor and the high risk cervical ln levels , and 50 gy to contralateral and / or ipsilateral ln . 
table 1 gives details on the fractionation protocol . imrt planning and dvh analysis imrt was based on the step - and - shoot approach with seven equidistant 10 mv beams . 
parotid gland recovery after h&n imrt parotid gland scintigraphy parotid gland function was quantitated by scintigraphy before and at 3 , 6 , 9 , and 12 months after radiotherapy . 
 die fehlerbalken stellen die standardabweichung fr jeden einzelnen dosispunkt dar . with u max maximum uptake before the stimulation u min minimum uptake after the stimulation e relative saliva excretion rate prior to or ft at t months after end of radiotherapy change in relative excretion rate before and at t months after end of radiotherapy statistical analysis for dose effect analyses , a reduction in scintigraphic activity of the parotid glands by 50% or 75% , respectively , was used as the quantal endpoint . 
this revealed ed50 values , i.e. , doses at which a response is expected in 50% of the glands treated , and their standard deviation ( ) [ 32 ]  . 
relative excretion rate for the relative excretion rate , clear differences between the ipsi ( nonspared ) and the contralateral ( spared ) glands were observed ( see figure 3 )  . 
the most significant correlation was found for the absolute volume that received at least 40 gy ( av40 ) and the change in relative excretion rate after 3 , 6 , 9 , and 12 months . 
a similar correlation was seen with the absolute volume receiving at least the threshold dose of 26 gy ( av26 ) [ 10 ] as well as with the mean dose . doseeffect relationship for a 50% reduction in parotid gland function , a clear and significant dose effect relationship was observed at 3 , 6 , and 9 months ( figure 4 ) , with ed50 values of 23 , 38 , and 34 gy ( table 2 )  . 
doseeffect curves for a reduction in parotid gland excretion by 50% ( solid lines ) and 75% ( dashed lines ) , respectively , at 3 , 6 , or 9 months after radiotherapy . 
dosis - effekt - kurve fr die reduktion der parotis - exkretion um 50% ( durchgezogene linie ) und 75% ( gestrichelte linie ) , 3 , 6 oder 9 monaten nach der strahlentherapie . 
ed50 values and their standard deviation ( ) as well as a p value for the dose dependence of the response were generated by probit analyses without the assumption of a threshold dose . 
 for the ipsilateral , nonspared parotid gland , no recovery took discussion and conclusion impairment of parotid gland function , resulting in xerostomia , is a frequent and dose - limiting side effect of conventional rt in the head - and - neck region [ 4 , 30 ]  . 
in a multicenter randomized study , the parsport trial investigated the advantage of the parotid sparing imrt technique compared to conventional rt in terms of clinical outcome [ 26 ]  . 
these results were supported by a preclinical evaluation leading to mean doses for the contralateral gland of 22 gy with imrt compared to 60 gy planned with a conformal technique [ 15 ]  . 
assessment of salivary flow or salivary gland scintigraphy can be exploited as endpoints for parotid gland function [ 5 , 10 , 17 , 19 , 20 , 25 , 30 , 31 ]  . 
 [ 27 ] suggested the relative volume receiving more than 40 gy ( v40 ) as a predictive value for salivary flow recovery , which can also be used for optimization of imrt plans . 
it is , therefore , suggested that also absolute volumes receiving a certain dose , in parallel to mean dose , can be used for treatment planning . however , it must be noted that the calculation of absolute volumes was based on planning ct information . 
this short - coming in the study could be overcome by image guidance for radiotherapy or by employing the planning organ at risk ( prv ) concept [ 8 ]  . at 3 , 6 , and 9 months after radiotherapy , sufficient data for doseeffect analyses were available . 
for a 50% and 75% threshold , respectively , ed50 values of 2338 gy and 5268 gy were observed , which are in the range of those reported in other studies [ 7 ]  . 
however , the massively expanding amount of information present via internet is taking its toll ; it is increasingly difficult to discern which websites are appropri ate and which are not . 
 undoubtedly , there are websites providing current informa tion professionally , but often medical laymen are overstrained in distinguishing the good from the bad and to avoid the latter [ 11 , 23 ]  . well as consultation hours and floor / road maps . 
service as pects consisted of introduction of staff including pictures or further information on attending doctors , the availability of treatment numbers , information on current events , and fre quently asked questions ( faq )  . 
the extent of medical information on the websites was analyzed by evaluating the amount of articles on the website as well as links to other websites with further information , availability of technical term explanation , and description of radiation treatment procedures . 
evaluationskriterien zur analyse von internetseiten deutscher radiotherapieeinrich tungen . university hospital n = 35 nonuniversity hospital n = 108 medical practice n = 62 total n = 205 material and methods the aim of this study was an explor atory evaluation of german radio therapy institutes websites applying a reproducible evaluation pattern with easytomeasure objective criteria . in june 2009 , all radiotherapy in stitutions in germany with a dataset entry on the degro ( german soci ety of radiation oncology ) homepage were analyzed [ 6 ]  . 
these insti tutions could be divided into 108 non university hospitals , 62 medical prac tices , and 35 university hospitals . as summarized in table 1 , the eval uation list was divided into three objec tively measurable categories , namely basic information , service , and medi cal issues . 
apart from other nonmedi cal references this was mainly based on a project of the medical association of lower saxony ( niederschsische rz tekammer ) called gute medizinische website 2008 [ 2 ]  . 
radiation therapy and internet differences between the websites of universities , medical practices and nonuniversity hospitals were tested for sig nificance using oneway analysis of variance ( anova )  . 
in all other categories of basic information , no statistically significant dif ferences could be found comparing nonuniversity hospitals , medical practices and university hospitals . the service contribution of the internet appearances showed a wide variation : while 85% introduced the medical staff in general , 50.2% supplied the visitors with photos and only 14% with further information on the attending physician like curriculum vitae or special interests . 
analyzing the appearance of faq and treatment numbers , no statistically significant differences could be seen . the mean number of articles with information for patients dealing with irradiation , side effects , cancer in general or tech nical issues was 4.6 ( range : 027 )  . 
a total quantity of 1 , 115 links was found with a mean number of 5.4 per website ( range : 1108 ) of which 8% did not work properly and 2.6% had a commercial background . 
mainly the links to external homepages can be divided into web appearances of support groups , radiotherapy organizations , and medical a detailed description of the treatment procedure explaining the schedule from the first contact , simulation and irradiation up to followup care was provided in 24.9%. 
for patients in general and on cologic patients in particular , internet consultation is ranging between 29% and 52% [ 13 , 18 , 21 ]  . the number of medical mismanaging by internet is stag gering . 
introduced a screening method for likely scientific accuracy revealing a high percentage of in ternet sites with socalled redflag criteria , for instance , avail ability of online purchasing , cancer cure treatments , and treatments with no side effects [ 12 ]  . 
internet sites contain ing those redflag criteria could be bypassed by providing professional information , for example , about new treatment strategies , treatment procedures and handling of side effects on homepages of radiotherapy institutions , as none of our analyzed websites contained any redflag criteria . a wellbalanced offer of links to support groups , medi cal dictionaries or professional homepages with background information on different tumor entities is desirable . 
the great advantage about supplementing patients with external links , information articles as well as description of treatment pro cedures on their homepages is the control of the information flow ; moreover , there is a good chance to respond individu ally to the patients concerns instead of getting lost on other websites . discussing internet information holds an opportunity to create assurance and consolidate patientphysician interac tion [ 20 ]  . 
radiation therapy and internet while the percentage of naming team members is quite high ( 85% ) , only few websites provide additional information like photos , curriculum vitae , or special interests of the physicians . 
another aspect in consolidating patientphysician interaction is the chance to get a direct feedback via emails which most websites did not offer . in some basic information like operating hours , tele phone numbers and introduction of staff , no significant differ ences were seen between the three institution types . 
however , regarding major information criteria like number of external links or description of treatment procedures , we found statis tically significantly better results for university hospitals and medical practices compared to nonuniversity hospitals . 
 other authors and organizations considered design , coloring , general arrangement , readability and quality of language to be taken into account for quality measurement [ 1 , 7 , 10 ]  . 
the lat ter aspects are not measurable objectively ; future studies are needed involving patients questionnaires in order to assess those aspects as well . another example is the webometrics ranking of world universities that evaluated 17 , 261 hospital websites world wide . 
for instance , we notified the opportunity of online appointments , evalua tion mails , downloads of information brochures , interactive route planner , patient blogs or virtual round tours through the institution . 
information about quality of life during therapy , as already evaluated in some studies [ 14 , 19 ] , could also be an important aspect for patients to know before treatment starts . keeping our evaluation criteria in mind , every institution should be able to analyze its homepages agasome nongov ernmental organizations like the health on the net founda tion ( hon ) even provide evaluation forms for medical web sites awarding a socalled code of conduct [ 9 ]  . conclusion analyzing the web appearances of german radiotherapy insti tutions , we found a wide variation of different quality . 
while some web pages provide a great amount of helpful information concerning side effects , treatment schedules or background information , a large percentage are lacking basic information such as operating hours , orientation facilities or introduction of the staff . 
 strahlenther onkol 2010 ; 186 : 53543 ( doi 10.1007 / s00066 - 010 - 2144 - z ) due to a technical error in the publishing process , several figures were inaccurately presented in table 1 . 
12 urban & vogel strahlentherapie und onkologie original article non - small cell lung cancer in stages iiiib long - term results of definitive radiotherapy with doses 80 gy in standard fractionation karl wurstbauer1 , hannes weise1 , heinz deutschmann1 , peter kopp1 , florian merz1 , michael studnicka2 , olaf nairz3 , felix sedlmayer1 purpose : to investigate therapeutic outcome of dose escalation 80 gy in nonresected non - small cell lung cancer ( nsclc )  . patients and methods : 124 consecutive patients with histologically / cytologically proven nsclc were enrolled . 
 58 patients ( 47% ) received induction chemotherapy , in median two cycles prior to radiotherapy . results : median follow - up time of all patients was 19 months , of patients alive 72.4 months ( 69121 months )  . 
apart from one treatment - related death ( pneumonitis ) , acute toxicity according to eortc / rtog scores was moderate : lung grade 2 ( n = 7 ) , grade 3 ( n = 3 ) ; esophagus grade 1 ( n = 11 ) ; heart grade 3 ( n = 1 , pericarditis )  . 
the results for survival and locoregional tumor control seem to at least equalize the outcome of simultaneous chemoradiation approaches , which , at present , are considered state of the art for patients with nonresected nsclc . 
a higher potential of radiation therapy might be reached by accelerated fractionation regimens . key words : non - small cell lung cancer radiotherapy conformal radiotherapy target splitting dose escalation strahlenther onkol 2010 ; 186 : 5517 doi 10.1007 / s00066 - 010 - 2108 - 3 nichtkleinzelliges bronchialkarzinom im stadium iiiib . 
langzeitergebnisse einer radiotherapie mit 80 gy in konventioneller fraktionierung ziel : evaluierung der behandlung mit dosen 80 gy bei nichtoperierter patienten mit nichtkleinzelligem bronchialkarzinom ( nsclc )  . patienten und methodik : 124 konsekutiv zugewiesene patienten mit histologisch / zytologisch verifiziertem nsclc wurden untersucht ( tabelle 1 )  . 
primrtumoren wurden im mittel mit 88 , 2 gy ( bandbreite 80 , 096 , 0 gy ) , makroskopisch befallene lymphknoten mit 69 , 3 gy ( 63 , 088 , 0 gy ) und elektive lymphknotenstationen ( region von etwa 6 cm kranial der makroskopisch befallenen lymphknoten ) mit 56 , 7 gy behandelt ( tabelle 2 )  . 
die lokore1university clinic of radiotherapy and radiation oncology and radart institute for research and development on advanced radiation technologies , paracelsus medical university , salzburg , austria , 2university clinic of pneumology , paracelsus medical university , salzburg , austria , 3heidelberg ion beam therapy center ( hit ) , heidelberg , germany . received : november 26 , 2009 ; accepted : june 28 , 2010 published online : september 30 , 2010 strahlenther onkol 2010 no . 
ein patient verstarb infolge einer pneumonitis , ansonsten war die toxizitt gemessen an den eortc / rtog - scoring - kriterien moderat : pneumonitis grad 2 ( n = 7 ) , grad 3 ( n = 3 ) ; sophagus grad 1 ( n = 11 ) ; herz grad 3 ( n = 1 , perikarditis ; tabelle 3 )  . 
bei keinem patienten trat eine spttoxizitt > grad 1 auf . schlussfolgerung : eine sequentielle , konventionell fraktionierte , hochdosierte bestrahlung mittels target - splitting - technik zeigt eine geringe morbiditt . 
die ergebnisse bezglich berlebenszeit und lokaler tumorkontrolle erscheinen gegenber den resultaten der simultanen chemo - / radiotherapie , die derzeit als state of the art angesehen wird , zumindest als ebenbrtig ( tabelle 4 )  . 
eine weitere steigerung des strahlentherapeutischen potentials drfte mit akzelerierten fraktionierungsschemata mglich sein . schlsselwrter : nichtkleinzelliges bronchialkarzinom strahlentherapie konformale radiotherapie target splitting dosiseskalation introduction globally , lung cancer is the leading cause of death among malignant diseases [ 34 ]  . 
 these patients are potentially curable by radiotherapy with or without chemotherapy . in dose - escalation protocols , tumor dose has been established as an independent predictor for tumor control and survival in the dose range of 60100 gy [ 18 , 21 ]  . 
the conformal target - splitting technique was implemented in 1995 , thus enabling dose escalations for nonresected nsclc patients , considering dose constraints as described below [ 29 , 32 ]  . 
the vast majority was treated with doses > 80 gy . in this report , the long - term outcome of this strategy is presented . patients and methods patient population and staging from december 1995 until march 2002 and from april 2003 until december 2003 , 124 patients with histologically / cytologically proven , nonresected nsclc were treated with doses 80 gy . 
during the last 3 and 4 years of the accrual period , 77 out of 80 patients ( 96% ) and 92 out of 99 patients ( 93% ) respectively , were treated with doses 80 gy and therefore enrolled . 
patient and tumor characteristics are shown in table 1 , comprising tumor stages iiiib ( malignant pleural effusion excluded )  . staging evaluations included a medical history , physical examination , chest x - ray , bronchoscopy , contrast - enhanced computed tomography ( ct ) scans of chest , upper abdomen and brain , and bone scan . 
18 - fluorodeoxyglucose positron emission tomography ( fdg - pet ) became available just at the end of the accrual period ; thus , only seven patients were additionally staged by fdg - pet . radiotherapy patients were set up in vacuum - based cradles . 
planning cts were performed as slow cts from the apex to the base of the lung , with patients freely breathing ( nonspiral ct ; 4 s / slice ; slice thickness 7 mm ) [ 31 ]  . 
the gtv was defined as the primary tumor and lymph node sites with a short - axis diameter > 1 ca ptv for elective treatment was designed for nodal areas 56 cm cranial to macroscopically involved nodes . 
in general , stage i patients received treatment to the primary lesion only . in the majority of the patients , the target - splitting technique was used [ 1 , 24 , 26 , 29 , 32 ] , as described in detail previoustable 1 . 
briefly , in an individually chosen transverse plane , the target is split into a cranial and a caudal volume , enabling the design of completely independent beam arrangements for either part . 
half - collimated , coplanar asymmetric fields ( half beams ) , in general each adjacent to the isocentric splitting ( junction ) plane , allow for highly conformal treatment plans . dose constraints were aimed at the following values : v20 ( volume receiving > 20 gy ) for a single lung 50% , v25 for both lungs 30% , spinal cord 45 gy , esophagus 84 gy ( measured in the center of the esophagus at its most exposed level and a dose 80 gy not exceeding 33% of the entire esophageal length )  . treatments were applied by 25 - mv or 15 - mv photons , treatment parameters including doses are depicted in table 2 . 
 doses were specified according to the icru 50 recommendations . chemotherapy 58 patients ( 47% ) , predominantly in stage iii , received induction chemotherapy , mostly consisting of a doublet of cisplatin or carboplatin combined with gemcitabine , navelbine or docetaxel . 
simultaneous chemotherapy was not allowed . prophylaxis for esophagitis and pneumonitis if parts of the esophagus were within or close to the ptv , an antimycotic prophylaxis was administered using amphotericin b lozengers , four times daily , during the full course of radiotherapy [ 33 ]  . during the initial 36 months of the accrual period , most of the patients also received a prophylactic treatment for pneumonitis , initially by daily oral 25 mg prednisone starting at week 3 post - irradiation in declining dosage , consecutively by inhalative substitution ( budesonide 0.4 mg twice daily ) , both for a duration of 6 weeks . 
 progression was diagnosed , if there was an increase in volume of tumor in comparison with the previous ct scan . acute and late toxicities were scored according to the rtog / eortc criteria except for acute pulmonary toxicity grade 1 , since the corresponding criterion mild symptoms of dry cough or dyspnea on exertion is common in these pulmonary - compromised patients and its differentiation from treatment side effects is difficult [ 7 ]  . 
toxicity was considered late , if persistent or occuring beyond 6 months after the completion of radiotherapy . statistical analysis overall survival and local tumor control rates were calculated with the kaplan - meier method . 
analyzed according to tumor stages i , ii , iiia , and iiib , the overall survival rates at 2 and 5 years amount to 57% , 75% , 33% , 26% and 20% , 13% , 13% , 4% , respectively . 
in analogy to comparable patients of our cohort , pulmonary dose constraints were surpassed due to the large extent of the disease : v20 right lung 72% , v20 left lung 38% , v25 both lungs 41% despite omission of elective radiotherapy . 
the patient showed classic symptoms of a pneumonitis 3 weeks after the end of radiotherapy , and , in spite of treatment with high - dose prednisone and antibiotics , died 5 weeks later . follow - up patients were prospectively assessed for toxicity and tumor control 6 and 12 weeks after the end of radiotherapy , then toxicity ( table 3 ) strahlenther onkol 2010 no . 
renal , laryngeal , esophageal and gastric cancer was diagnosed in one patient each . grade 1 n ( % ) grade 2 n ( % ) grade 3 n ( % ) grade 4 n ( % ) grade 5 n ( % ) 11 ( 9 ) 7 ( 6 ) 3 ( 2 ) 1 ( 1 ) 1 ( 1 ) esophagus lung heart ( pericarditis ) in four patients showing grade 3 symptoms ( three with pneumonitis and one with pericarditis , respectively ) , toxicity resolved after corticoid therapy . esophageal acute side effects were observed only in grade 1 dimension ( eleven patients )  . regarding late toxicity , most patients showed local fibrotic pulmonary alterations , which did not exceed clinical grade 1 symptoms . 
all other side effects described above , occurred in patients with stage > i disease . locoregional tumor control in total , 60 patients recurred locoregionally , 48 of them ( 80% ) within the first 2 years after the beginning of therapy . 
there is no apparent difference in local tumor control with respect to histological subtypes . eleven out of 30 stage i patients failed locally , nine of them within a follow - up time of 2 years , six of them with an initial tumor size > 5 cthe overall locoregional tumor control rate at 2 years for stage i patients is 57% ; for patients with tumors < 5 cm ( n = 20 ) and > 5 cm ( n = 10 ) , it amounts to 72% and 30% , respectively . second malignancies discussion radiation dose escalation kong et al . , enrolling 106 patients in a dose - escalation trial , showed a positive radiation dose - response relationship in the dose range 63103 gy [ 18 ]  . 
comparably , rengan et al . , investigating 72 stage iii patients with gtv > 100 cm3 , reported dose ( apart gtv ) to be an independent predictor of tumor control in the dose range 5084 gy [ 21 ]  . table 4b summarizes the results of four study groups dealing with standard fractionation dose escalation . 
as tumor extensions in patients with nonresected nsclc vary considerably and the level of applicable doses is dependent on doses to healthy tissues , dose escalation was performed within various bins reflecting the amount of irradiated normal tissues , especially of the lungs . 
various parameters to define these bins were used by different investigators , such as the effective lung volume [ 18 ] , the relative mean lung dose [ 3 ] , the normal - tissue complication probability [ 22 ] , or the percentage of the total lung volume receiving doses > 20 gy ( v20 ) [ 5 ]  . in the trial of the university of michigan , usa , starting doses in five predefined bins ranged from 63 to 84 gy [ 16 , 18 ]  . 
 doses were systematically escalated to 102.9 gy in the two groups with the smallest effective lung volume and to 84 gy , 75.6 gy , and 65.1 gy for the other three cohorts . 
from sloan kettering report 70.2 gy as starting point of their escalation trial ; doses up to 90 gy were applied to some patients , but the mtd was assessed to be 84.0 gy [ 22 ]  . 
from the netherlands cancer institute , the overall treatment time was limited to 6 weeks ; if more than 30 fractions were prescribed , patients were treated twice daily [ 3 ]  . 
to our knowledge , our trial is the first to investigate treatment doses 80 gy in all patients for stages i to iiib of a mainly unselected , continuously referred population . 
in our opinion , the feasibility of higher doses for all tumor stages with acceptable morbidity is mainly derived from two facts : first , different dose gradients for primary lesions , involved and elective nodes , and second , the technical developments in treatment planning and dose delivery , as reflected by the use of slow planning cts and the target - splitting technique . 
both items have a high potential to spare normal tissues , discussed in detail in previous reports [ 20 , 29 , 31 , 32 ]  . as described , eight patients in our series died of a pulmonary hemorrhage . 
for our own patients , we were not able to show a clear relationship between the level of the overall dose or the fractional dose ( 2.02.2 gy ) , respectively , and the frequency of hemoptysis . 
for patients in good general condition without weight loss , sequential therapies with moderate radiation doses ( 5666 gy ) yield median overall survival times of about 14 months and are well tolerated , simultaneous therapies result in survival times of about 17 months with increased acute , specifically esophageal toxicity . 
a recent report indicates that approximately 60% of stage iii patients < 75 years of age would not be candidates for a concurrent approach [ 11 ]  . despite promising results in the earlier studies , treatment intensification by adding induction or consolidation chemotherapy and / or targeted therapy to concomitant radiochemotherapy have not yet demonstrated any survival benefit over concurrent radiochemotherapy alone [ 2 , 15 , 17 ]  . 
a definitive answer , if increased radiation doses administered concomitantly to chemotherapy will result in better locoregional control and survival , will be given by the ongoing randomized rtog 0617 trial comparing simultaneously applied 60 gy versus 74 gy . the median survival of 19.6 months in our study compares favorably with the results of the concomitant approach , especially considering the negative prognostic criteria in a large portion of our patients ( 31% with weight loss > 5% , 8% with karnofsky index 60 )  . 
in comparison to simultaneous therapies , a sequential approach with high - dose radiotherapy applied by an appropriate technique seems to at least equalize the results for locoregional tumor control and survival , shows less toxicity and is suitable also for patients in less favorable general conditions . overall treatment time , further developments a disadvantage of escalating the dose with standard fractionation is the long overall treatment time . 
in order to compensate this potential drawback , we performed a consecutive phase i / ii trial of accelerated , high - dose radiotherapy applied twice daily that showed good tolerability in 30 patients [ 30 ]  . 
 [ 3 ] current study a a astage ii / iii included , percentage not specified conclusion high - dose radiotherapy in standard fractionation using the technique of target splitting , sequentially applied after two cycles of induction chemotherapy , in general is well tolerated . 
nonresected nsclc high - dose radiotherapy strahlentherapie und onkologie original article toxicity after intensity - modulated , image - guided radiotherapy for prostate cancer matthias guckenberger , sami ok , blent polat , reinhart a . 
sweeney , michael flentje1 purpose : to evaluate toxicity after dose - escalated radiotherapy for prostate cancer using intensity - modulated treatment planning ( imrt ) and image - guided treatment ( igrt ) delivery . patients and methods : 100 patients were treated with simultaneous integrated boost ( sib ) imrt for prostate cancer : doses of 76.23 gy and 60 gy in 33 fractions were prescribed to the prostate and the seminal vesicles , respectively , for intermediateand high - risk patients ( n = 74 )  . 
the pelvic lymphatics were treated with 46 gy in 25 fractions in patients with high risk of lymph node metastases using an sib to the prostate ( n = 25 )  . 
das vorhandensein von akuter giund gu - toxizitt war mit einer signifikant hheren inzidenz an spten gi ( p = 0 , 0007 ) und gu - nebenwirkungen ( p = 0 , 006 ) assoziiert . schlussfolgerung : radiotherapie mit hohen bestrahlungsdosen resultierte in geringer akuttoxizitt bei anwendung von imrt und igrt ; vorlufige daten zur chronischen toxizitt sind vielversprechend . schlsselwrter : prostatakarzinom perkutane strahlentherapie intensittsmodulierte strahlentherapie ( imrt ) bildgefhrte strahlentherapie ( igrt ) toxizitt 1department of radiotherapy , university hospital wrzburg , germany . received : march 15 , 2010 ; accepted : march 25 , 2010 published online : september 30 , 2010 strahlenther onkol 2010 no . 
imrt and igrt for prostate cancer introduction target definition the practice of primary external - beam radiotherapy ( ebrt ) for prostate cancer has changed dramatically and remains controversial in several fields . 
escalation of the radiation dose beyond 70 gy improved biochemical control in low - , intermediateand high - risk patients [ 2 , 13 , 40 , 52 ] , but rates of rectal toxicity were increased . 
whereas the first analysis of the rtog 9413 trial reported a benefit of whole - pelvis ( wp ) irradiation [ 42 ] , this was unclear with longer follow - up [ 28 ] and the french getug - 01 trial showed no difference between prostate - only ( po ) and wp irradiation [ 41 ] ; however , toxicity was increased with wp irradiation . 
there is now strong evidence for a low / value of prostate cancer [ 33 ] , lower compared to late rectal toxicity [ 9 ] , and clinical results support the use hypofractionated irradiation schemas [ 3 , 27 , 34 , 49 ]  . escalation of the irradiation doses , wp irradiation and hypofractionated schemas all bear the risk of increased toxicity . 
in recent years , intensity - modulated radiotherapy ( imrt ) became available allowing for improved sparing of organs at risk ( oars ) compared to conventional and three - dimensional conformal radiotherapy ( 3d - crt ) [ 22 ]  . 
 image guidance techniques ( igrt ) make verification of the prostate position prior to treatment possible [ 26 ] : it is known that systematic changes of the prostate position between planning and treatment if not corrected by igrt negatively affect outcome [ 15 , 24 ]  . this article describes early clinical outcome after primary radiotherapy for prostate cancer : the pelvic lymph nodes ( lns ) were treated in high - risk patients and dose - escalated irradiation of the prostate was realized via moderate hypofractionation with a simultaneous integrated boost ( sib ) and imrt planning . 
image guidance with linac - integrated cone - beam ct ( cbct ) was practiced in all patients . patients and methods this analysis is based on the first 100 patients treated with intensity - modulated , image - guided radiotherapy since september 2005 . 
an empty rectum was intended by advising the patients to avoid flatulent food . pinnacle ( philips radiation oncology systems , milpitas , ca , usa ) was used for treatment planning . 
the prostate and seminal vesicles were contoured as the clinical target volume ( ctv ) in the planning ct ; the planning mri was mainly used for identification of the prostatic apex . 
the ctv - 1 was the prostate including the proximal 2 cm of the seminal vesicles and the ctv - 2 was the prostate and base of the seminal vesicles ; the amount of seminal vesicles within ctv - 2 was adjusted to the patients individual risk factors and the presence of seminal vesicles involvement in the mri . 
the ctv - 1 was expanded with a three - dimensional margin of 10 mm resulting in the planning target volume 1 ( ptv - 1 ) , to posterior the margin was limited to 7 ma margin of 5 mm was added to the ctv - 2 without rectum overlap resulting in the ptv - 2 . the pelvic lns were irradiated in patients with an estimated risk of ln involvement of minimum 1520% according to the roach formula [ 43 ]  . 
the ptv of the pelvic lymphatic drainage comprised the obturator , perirectal , internal iliac , proximal external iliac , presacral ( s1 and s2 ) and common iliac lns up to l5 / s1 . 
in plan - wp , a minimum sfd of 1.84 gy was planned for the ptv - ln and the ptv - 1 ; by means of an sib , identical planning objectives were used for ptv - 2 as in plan - po . in low - risk patients , 32 fractions of plan - po were prescribed resulting in a mean dose of 73.91 gy to ptv - 2 . 
in intermediateand high - risk patients , 33 treatment fractions were prescribed resulting in a mean dose of 76.23 gy to ptv - 2 ; these 33 fractions were 33 fractions of plan - po for patients with low risk of ln involvement and 25 fractions of plan - wp followed by eight fractions of plan - po for patients strahlenther onkol 2010 no . 
a combined offline and online igrt protocol was practiced : daily imaging was performed at the first five fractions and the skin marks were adjusted to correct for the systematic error after these five fractions [ 14 ]  . 
errors were corrected online prior to treatment every time a cbct was acquired . gastrointestinal ( gi ) and genitourinary ( gu ) toxicity was scored using ctcae v3.0 : assessment of toxicity was performed every 2nd week during treatment , 6 weeks after treatment , and at 6 - month intervals thereafter . correlation between toxicity and clinical / treatment parameters was performed using the 2 - test for categorical variables and the mann - whitney u - test for numerical variables . 
six patients suffered from pretreatment urinary incontinence grade i . during treatment , no acute toxicity was described by 6% , and 46% of the patients developed gu and / or gi toxicity grade 2 . 
this acute toxicity resolved quickly with 12% describing toxicity grade 2 6 weeks after treatment ; 59% were free from any toxicity at this first follow - up ( figure 1 )  . acute gi toxicity was mild : 27% and 8% of the patients complained of grade 1 and grade 2 toxicity at the end of radiotherapy , respectively ; acute gi toxicity grade 3 was not observed . 
imrt and igrt for prostate cancer acute late gi toxicity grade 3 grade 2 grade 1 grade 0 and toxicity grade 2 remained in 11% ( figure 3 )  . 
urinary frequency was the dominant grade 2 and 3 toxicity ( table 2b )  . correlation between acute toxicity and patient / treatment characteristics is shown in table 3 . late toxicity median follow - up for living patients was 26 months ; seven patients have died and cause of death was exacerbation of comorbidities in all patients . 
four patients developed late toxicity grade 3 : stenosis of the ureter requiring repeated stenting ( n = 1 ) , stenosis of the urethra treated with urethrotomy ( n = 2 ) and rectal bleeding requiring transfusion ( n = 1 ; this patient had a long history of hemorrhoids )  . late gi toxicity was rare with 96% of patients free from any late gi toxicity at 24 months ( figure 2 )  . 
proctitis and diarrhea were the most frequent acute toxicities ( table 2a )  . the majority of patients developed acute gu toxicity : grade 2 was observed in 36% at the end of radiotherapy . 
univariate analysis of the correlation ( p - values ) between patient and treatment characteristics with development of acute and late gastrointestinal ( gi ) and genitourinary ( gu ) toxicity . 
po : nur prostata ; ptv : planungszielvolumen ; turp : transurethrale prostataresektion ; wp : gesamtes becken . acute toxicity grade 2 late toxicity grade 2 age ( median ) karnofsky index ( > 80% ) diabetes mellitus coronary heart disease arterial hypertension history of turp volume ptv - 1 ( median ) volume ptv - 2 ( median ) total dose in ptv - 2 wp vs . 
this is considered the benefit of conformal treatment planning using imrt and precise treatment delivery using igrt . treatment regarding po , table 4 indicates that acute gi toxicity is reduced by means of imrt and igrt compared to conventional planning and delivery techniques . 
the seemingly increased gu toxicity grade 2 for imrt and igrt treatment in table 4 should , however , be considered artificial : in a preliminary analysis of the md anderson dose - escalation trial , storey et al . 
the observation that mainly acute gi and not gu toxicity is reduced by imrt is in good agreement with data from the dutch dose - escalation trial , where a subgroup analysis showed significantly reduced rates of acute gi toxicity grade 2 for patients treated with imrt ( 20% ) compared to 3d - crt ( 61% ) [ 1 ]  . for treatment of wp , table 5 shows that rates of acute toxicity grade 3 are consistently < 5% after imrt and igrt . 
 these similar rates of toxicity are seen despite an increase of the total dose by 10 gy on average in the imrt / igrt trials compared to rtog 9413 and getug - 01 . late gu toxicity remained constant from 6 months to 24 months after treatment : grade 1 toxicity varied between 21% and 16% , grade 2 toxicity between 1% and 7.7% , and grade 3 toxicity was maximum 2.7% at 18 months ( figure 3 )  . 
akute gastrointestinale ( gi ) und urogenitale ( gu ) toxizitt in der literatur bei strahlentherapie des prostatakarzinoms ohne behandlung des pelvinen lymphabflussgebiets ; verglichen wurden studien , bei welchen dreidimensionale konformale strahlentherapie - ( 3d - crt - ) planung ohne bildgefhrte strahlentherapie ( igrt ) angewendet wurde , mit studien , bei welchen regelhaft intensittsmodulierte strahlentherapie ( imrt ) und igrt angewendet wurden . patients total dose ( gy ) fractions eqd2 ( gy ) igrt toxicity scoring acute gi toxicity ( % ) acute gu toxicity ( % ) grade 2 grade 3 grade 2 grade 3 study 3d - crt without igrt 61 zelefsky et al . 
this effect of consequential late toxicity was also observed in our patient population , especially for gi but also for gu toxicity . a median follow - up of 26 months is certainly not sufficient for final analysis of late toxicity ; however , preliminary results are favorable and support the hypothesis that reduced acute toxicity translates into low rates of late toxicity . 
contrary to our ntcp ( normal - tissue complication probability ) calculations [ 21 ] , there was trend to increased late gu toxicity after treatment of wp compared to po : in that planning study , all plans were generated with a full bladder , which is known to reduce gu toxicity [ 37 ]  . 
we assume that the patients ability to fill the bladder decreased due to acute toxicity during treatment with the consequence that a larger proportion of the bladder wall moved into the wp target volumes . 
 additionally , androgen suppression was correlated with increased acute and late gi toxicity , a finding which is discussed controversially in the literature [ 17 , 31 , 45 , 48 ]  . both imrt and igrt are required for optimal results in ebrt of prostate cancer . 
imrt clearly improves conformity of the dose distributions with better sparing of bladder and especially small bowel and rectum ; this has been demonstrated in numerous planning studies and dose - volume relationships for rectal and upper gi toxicity are well established [ 18 ]  . 
however , the conformal dose distributions with sharp dose gradients between target and oars ( especially rectum ) increase the susceptibility of these treatments to geometric uncertainties [ 8 ] making precise targeting with image guidance essential . 
image - guided targeting of the prostate is now feasible in daily clinical routine using various techniques and early data suggest that smaller safety margins with igrt strahlenther onkol 2010 no . 
imrt and igrt for prostate cancer translate into lower rates of toxicity after treatment of po [ 6 ] and wp [ 10 ]  . conclusion high - dose radiotherapy for prostate cancer using imrt and igrt resulted in low rates of acute toxicity and preliminary results of late toxicity are promising . strahlentherapie und onkologie original article helical tomotherapy in cervical cancer patients simultaneous integrated boost concept : technique and acute toxicity simone marnitz1 , carmen stromberger1 , michael kawgan - kagan1 , waldemar wlodarczyk1 , ulrich jahn1 , achim schneider2 , uwe ulrich3 , volker budach1 , christhardt khler2 purpose : to evaluate the acute toxicity of simultaneous integrated boost ( sib ) technique for dose escalation with helical tomotherapy ( ht ) in patients with locally advanced cervical cancer . patients and methods : 20 patients ( figo ib1 pn1 - iiib ) underwent primary chemoradiation . 
patients were treated with five weekly fractions of 1.8 gy to a total dose of 50.4 gy to the tumor region and the pelvic ( para - aortic ) lymph node region ( ptv - a ) , and five weekly fractions of 2.12 gy to a total dose of 59.36 gy to the ptv - b . 
19 patients underwent curettage 69 weeks after chemoradiation without any evidence of tumor . conclusion : the concept of sib for dose escalation in patients with locally advanced cervical cancer is feasible with a low rate of acute toxicity . 
whether dose escalation can translate into improved outcome will be assessed after a longer follow - up . key words : chemoradiation helical tomotherapy cervical cancer toxicity simultaneous boost strahlenther onkol 2010 ; 186 : 5729 doi 10.1007 / s00066 - 010 - 2121 - 6 tomotherapie in der therapie des zervixkarzinoms . 
simultanes integriertes boostkonzept : technik und akuttoxizitt ziel : die akuttoxizitt der simultanen integrierten boost - ( sbi - ) technik der helikalen tomotherapie ( ht ) in der primren radiochemotherapie bei patientinnen mit lokal fortgeschrittenen zervixkarzinomen wurde untersucht . patienten and methodik : 20 patientinnen mit zervixkarzinomen ( figo ib1 pn1 - iiib ) erhielten nach laparoskopischer transperitonealer pelviner und paraaortaler lymphonodektomie eine primre radiochemotherapie . 
unter einschluss der pelvinen / paraaortalen lymphknoten und der tumorregion ( ptv - a [ planungszielvolumen ] ) wurden die patientinnen mit fnf wchentlichen einzeldosen von 1 , 8 gy bis 50 , 4 gy bestrahlt . 
die abrasio 69 wochen nach therapieende zeigte bei 19 patientinnen keinen vitalen resttumor . 1department of radiooncology , charit university medicine , berlin , germany , 2department of gynecology charit university medicine , berlin , germany 3department of gynecology and obstetrics , martin luther hospital , berlin , germany . received : january 8 , 2010 ; accepted : may 20 , 2010 published online : september 30 , 2010 strahlenther onkol 2010 no . 
ob die dosiserhhung zu einer verbesserten lokalen kontrolle fhrt , muss evaluiert werden . schlsselwrter : radiochemotherapie helikale tomotherapie zervixkarzinom toxizitt simultaner boost introduction since randomized studies have demonstrated the superiority of chemoradiation over radiation alone , concomitant cisplatin - based chemoradiation is the therapy of choice in patients with locally advanced cervical cancer . 
however , there is considerable acute and late toxicity affecting the small bowel , rectum , and the genitourinary ( gu ) tract [ 3 , 4 , 14 , 15 , 20 , 22 , 28 , 30 , 36 ]  . 
in randomized pivotal trials evaluating chemoradiation in cervical cancer , grade 1 and 2 acute toxicity occurred ; overall , 53.3% experienced hematologic , 45.2% gastrointestinal ( gi ) , and 17.5% gu toxicities [ 11 , 34 ]  . 
even with careful planning , severe grade 3 and 4 gi and gu acute toxicity is reported in about 8% and 1.5% of patients , respectively [ 12 , 16 ]  . intensity - modulated radiotherapy ( imrt ) significantly reduces acute and late toxicity to the organs at risk [ 5 , 21 , 24 , 25 , 27 , 3335 ]  . 
a dose escalation might improve local control , if the target volume can be exactly defined and covered with an appropriate radiation dose [ 9 ]  . since there is no generally accepted recommendation for radiation doses to the organs at risk , a growing body of evidence indicates a strong dose - volume relationship for the development of small bowel toxicity for pelvic tumors [ 1 , 26 ]  . 
using the following constraints , < 40% of the small bowel should receive < 35 gy and < 50% of the rectum should receive at least 45 gy , only one of 54 patients developed grade 3 gi toxicity during an adjuvant chemoradiation for cervical cancer [ 6 ]  . compared with conventional imrt , helical tomotherapy ( ht ) delivers a highly conformal dose distribution with a greater number of independent beam directions . 
while reducing setup errors , the margins of the planning target volume ( ptv ) can be reduced and , as a result , reduce the dose to the small bowel [ 10 ]  . analyzing ht and imrt plans for extended - field irradiation in stage iiic endometrial cancer , lian et al . 
however , the potential benefit of ht over imrt is still being investigated . the aim of this study was to evaluate the acute toxicity of a simultaneous integrated boost ( sib ) technique for dose escalation with ht in combination with intracervical brachytherapy in the primary treatment of patients with locally advanced cervical cancer . 
the study population included one patient with figo stage ib1 pn1 , two with figo stage ib2 , two with figo stage iia , nine with figo stage iib , three with figo stage iiia , and three with figo stage iiib . 
subsequently , a comprehensive pretherapeutic transperitoneal laparoscopic staging , including para - aortic and pelvic lymphadenectomy , biopsies from the vesicocervical septum , and a peritoneal washing was performed , as previously described , in 15 of the 20 patients [ 18 ]  . 
the study has been approved by the institutional ethics committee . treatment planning all patients received a planning ct scan ( ct scanner lightspeed , ge healthcare , general electric company , nyse , ge , schenectady , ny , usa ) in a supine position with i.v. 
in case of para - aortic involvement , the ct scans were done from the diaphragm to the trochanter minor at a slice thickness of 3.75 min histologically proven negative lymph nodes , a ct scan was performed from the second lumbar vertebra to the trochanter minor . 
 for the clinical target volume ( ctv - a ) , 5 mm was added to the gtv and the iliac external , internal , commune , and presacral lymph nodes according to the rtog recommendations [ 13 ]  . 
in patients with negative para - aortic lymph nodes , the upper ptv border was at the level of the l4 / 5 interspace ( see figure 2 )  . 
in patients with para - aortic lymph node metastases , the para - aortic region was included in the ctv - a up to the level of the renal vessels . 
the lower ptv border was marked on the foramina obturatoria ( see figure 3 )  . for the ctv - b definition , the high - risk volume ( parametria and surrounding lymphatic tissue ) was defined using a standardized technique during laparoscopic staging , with titanium clips . 
transversale , koronare und sagittale schichten und dosisverteilung einer patientin mit paraaortalund beckenbestrahlung ( blau : 80% - isodose , grn : 90% - isodose ; gelb 95% - isodose bezogen auf das ptv - a ; rot : 95% - isodose im ptv - b )  . the fascia of the iliopsoas muscle ( figure 1 )  . 
contrast ct : for the upper border , the bifurcation of the common iliac artery , for the lateral border , the iliopsoas muscle , for the medial border , the lateral part of the uterus , for the caudal border , the strahlenther onkol 2010 no . 
the ctv - a included the ctv - b , and the ptv - a included the ptv - b . results dose prescription , planning parameters , and radiation technique a target dose of 1.8 gy was prescribed to the ptv - a and given as conventional fractionation with five weekly fractions , up to a total dose of 50.4 gy after 28 fractions . 
the ct datasets with structures and contours in the eclipse planning system ( varian medical systems , palo alto , ca , usa ) were transferred to the ht planning workstation . 
the planning tools delivered at least 95% of the prescribed dose to the ptvs , while keeping the irradiated volumes of the small bowel , which received 45 gy , as low as possible ( figures 2 and 3 )  . 
additionally , iridium - 192 high - dose - rate ( hdr ) brachytherapy ( brachyplanning , varian , palo alto , ca ) was performed on the basis of a magnetic resonance image ( mri ) prior to brachytherapy that covered the macroscopic tumor visible on the mri with a 5 - gy isodose , one to two fractions per week with an interfraction interval of at least 72 h up to a total dose of 25 gy . 
the goal was to keep nominal maximum dose to the rectum and bladder of five brachytherapy fractions below 20 gy [ 23 ]  . dose - volume histogram ( dvh ) analysis the dvhs were compared with respect to the mean dose to the organs in the radiation fields . 
para - aortic lymph node metastases could be confirmed in 4 / 15 patients who had one to 22 ( median , 9.5 ) metastatic lymph nodes ( see table 1 )  . 
18 / 19 patients completed five cycles of cisplatin 40 mg / m2 body surface on days 1 , 8 , 15 , 22 , and 29 concomitant with radiation therapy . 
the mean dose to 1% of the volume ( d1% ) was 58.3 gy to the bladder and 56.7 gy to the rectuthe conformity number , according to vant riet et al . 
dosis ( gy ) in 1% des organvolumens ( d1% ) ; sd : standardabweichung . transperitoneal staging did not delay the beginning of chemoradiation , which began within 510 days after laparoscopy . 
19 of 20 patients developed vaginal discharge ( 13 grade 1 , and six grade 2 ) and / or vaginitis ( twelve grade 1 , and three grade 2 ) due to tumor treatment ( table 4 )  . 
this data underlines the need for greater local control to improve patient outcomes . since highly conformal techniques can significantly decrease acute and late gi and gu toxicity [ 5 , 21 , 27 , 33 ] , dose escalation without increased gi and gu toxicity may be possible [ 5 , 6 ]  . 
we used ht with sib as a dose escalation in the parametric region which is the area at the highest risk of recurrence . an essential precondition for this new concept is the exact definition of the parametric target volume . 
using this technique , it was possible to increase the dose to this region from 50 gy to 60 gy with an sib . the purpose of this study was to analyze whether this procedure is associated with an increased rate and severity of acute gi and gu toxicity compared with conventional techniques . 
helical tomotherapy in primary chemoradiation of cervical cancer patients first to describe the technique of sib with ht and the resulting acute toxicity in patients with cervical cancer ; hence , there is no literature to compare the ht with , and only little data on , imrt in the treatment of gynaecological cancer [ 5 , 17 , 21 , 25 , 33 ]  . because of the higher volumes covered by low radiation doses , hematologic toxicity could not be decreased using imrt techniques . 
comparing this data , it is noteworthy that the prescribed dose in most of the studies reported was lower because these were in an adjuvant setting , and not primary chemoradiation [ 5 , 21 , 27 ]  . 
we decided to contour the whole peritoneal cavity except for muscles and other organs at risk , and exceeded the ptv by only two ct slices in order to avoid an underestimation of the small bowel dose . 
in particular , the overlapping volume of the small bowel and the ptv should be considered , since this was part of the ptv and a limiting factor for saving the small bowel . 
additionally , patient - related factors like the patients weight , size of the fields , and the use of a para - aortic field may have a large influence on the range . 
in the present study , the overlapping volume was 317 207 cm3 in patients with and without extended - field irradiation . in rectal cancer patients with preoperative irradiation , ht and daily mv - ct led to a reduced small bowel volume ( v15 ) , which correlated with a decreased normal - tissue complication probability ( ntcp ) of 18% for grade 2 diarrhea [ 10 ]  . 
 although the v15 is comparable to that of the above - mentioned study , we saw no grade 2 diarrhea but one patient ( 5% ) experienced grade 3 diarrhea , which is less than could be expected from this ntcp model . 
other data showed a correlation between grade 3 toxicity and a v15 ( small bowel ) of < 150 cm3 with no grade 3 toxicity versus 50% grade 3 toxicity for v15 > 150 cm3 in rectal cancer patients [ 1 ]  . 
again , there was no grade 3 toxicity . conclusion in the present study , we analyzed the acute toxicity of primary chemoradiation using ht in patients with locally advanced cervical cancer . 
whether ht is superior in terms of ptv coverage , conformity , homogeneity , and oncologic results compared with conventional imrt requires further investigation , and was not the focus of the present study . 
bismar for the data collection . strahlentherapie und onkologie current discussion the german s3 guideline prostate cancer aspects for the radiation oncologist frederik wenz1 , thomas martin2 , dirk bhmer3 , stefan martens4 , felix sedlmayer5 , manfred wirth6 , kurt miller7 , axel heidenreich8 , mark schrader9 , wolfgang hinkelbein10 , thomas wiegel11 this report summarizes the relevant aspects of the s3 guideline prostate cancer for the radiation oncologist . 
the relevant literature is cited to allow an overview of the current recommendations . key words : prostate cancer radiation oncology german s3 guideline strahlenther onkol 2010 ; 186 : 5314 doi 10.1007 / s00066 - 010 - 2193 - 3 die deutsche s3 - leitlinie prostatakarzinoradioonkologische aspekte dieser bericht fasst die relevanten aspekte der s3 - leitlinie prostatakarzinom fr den strahlentherapeuten zusammen . 
the following report summarizes the relevant aspects for the radiation oncologist . the german s3 guideline uses the following categories : localized prostate cancer : stages t12 n0 m0 , locally advanced prostate cancer : stages t34 n0 m0 , advanced prostate cancer : stages n13 , metastasized prostate cancer : stage m1 . the localized prostate cancer is classified into three prognosis groups according to risk factors [ 6 ] , which is well established in clinical practice : ( 1 ) low risk : prostate - specific antigen ( psa ) < 10 ng / ml and t1ct2a and gleason score < 7 , 1department of radiotherapy and radiooncology , university medicine mannheim , university of heidelberg , germany , 2group practice for radiotherapy and radiooncology , bremen , germany , 3department of radiotherapy , charit university medicine berlin , campus virchow clinic , berlin , germany , 4department of urology , marien - krankenhaus bergisch gladbach , germany , 5department of radiotherapy and radiooncology , salzburger landeskliniken , salzburg , austria , 6department of urology , university hospital carl gustav carus , dresden , germany , 7department of urology , charit university medicine , berlin , germany , 8department of urology , university hospital aachen , germany , 9department of urology , university hospital ulm , germany , 10department of radiotherapy , charit university medicine berlin , campus benjamin franklin , berlin , germany , 11department of radiotherapy and radiooncology , university hospital ulm , germany . received : may 13 , 2010 ; accepted : june 30 , 2010 published online : september 30 , 2010 strahlenther onkol 2010 no . 
radiooncologic aspects of the german s3 guideline prostate cancer ( 2 ) intermediate risk : psa 10 and < 20 ng / ml or t2b or gleason score = 7 , ( 3 ) high risk : psa 20 ng / ml or > t2b or gleason score > 7 . treatment decision for the newly diagnosed , nonmetastasized prostate cancer randomized phase iii studies comparing all curative treatment options for prostate cancer are not available at present . 
 retrospective analyses demonstrated that external - beam radiotherapy with sufficiently high doses , permanent low - dose - rate ( ldr ) brachytherapy and radical prostatectomy yield comparable results regarding psa control [ 20 ]  . 
permanent ldr brachytherapy is an equivalent option for the low - risk group of patients ( < t2c , gleason score < 7 , psa < 10 ng / ml )  . 
external - beam radiotherapy with endocrine therapy or combined with a high - dose - rate ( hdr ) boost is a primary treatment option for patients with locally advanced prostate cancer . 
there was consensus that all patients with prostate cancer who qualify for curative treatment should be offered the opportunity to discuss advantages or disadvantages of surgery and radiotherapy with an urologist and a radiation oncologist . 
the discussion of potential side effects should always include the functional domains of micturation , gastrointestinal symptoms , and sexual dysfunction . technical performance of external - beam radiotherapy before initiation of radiotherapy , patients with a gleason score 8 or ct3 / 4 stadium should undergo magnetic resonance imaging ( mri ) , first , to evaluate local tumor extension and pelvic lymph node status and , second , for treatment - planning purposes . 
additionally , a bone scan should be done in these patients and patients with a psa 10 ng / ml or bone pabecause of limited sensitivity and specificity of the imaging studies , the use of externally validated nomograms is recommended as well . 
in the intermediate - risk situation , an intensified regimen should be applied either by radiation dose escalation or additional short - term endocrine treatment for 6 months [ 7 , 14 , 19 ]  . 
in several phase iii trials , prolongation of the overall survival was shown after treatment with combined radiation and endocrine therapy in comparison to radiotherapy alone in patients with locally advanced and high - risk prostate cancer ( eortc 22863 , rtog 85 - 31 , rtog 86 - 10 , rtog 92 - 02 [ 4 , 13 , 24 , 28 ] )  . 
to date , optimal dose prescription in localized prostate cancer on the one hand and locally advanced prostate cancer on the other hand , is not precisely determined and is in the range of 7279 gy depending on fractionation , overall treatment time , etc . 
dose escalation in general requires modern radiation oncology concepts to minimize side effects , e.g. , immobilization , preparation of bowel and bladder , thin - slice imaging , inverse treatment planning , image - guided radiotherapy ( igrt ) , and intensity - modulated radiotherapy ( imrt ; e.g. , [ 1 , 3 , 17 , 21 , 25 , 37 ] )  . 
this situation is reflected in diverging national recommendations in other countries . radiation treatment after radical prostatectomy a radical prostatectomy in the ct1t2 situation results in a pt3 stage in 2540% of the cases [ 34 ]  . 
meanwhile , the results of three randomized trials ( swog [ 31 ] , eortc [ 4 ] and aro [ 34 , 35 ] ) with focus on adjuvant radiotherapy in the pt3 situation are available . 
radiation treatment with 6064 gy improves local relapse - free survival at 5 years by about 20% , whereas the kaplan - meier estimates diverge already 23 years after treatment for metastases - free survival and 56 years after treatment for overall survival [ 31 ]  . 
the swog study [ 31 ] showed a significant prolongation of overall survival after adjuvant radiotherapy of about 2 years after a median follow - up of almost 13 years . 
the highest benefit after adjuvant radiation treatment was seen in patients with a pt3 tumor and positive margins ( 30% higher biochemical no - evidence - of - disease [ ned ] rates after 5 years ) [ 32 , 34 , 35 ]  . 
in addition , patients with a pt2 r1 situation should be treated with adjuvant radiotherapy according to the subgroup analysis of the eortc study , which showed similar effects as in pt3 r1 tumors [ 32 ]  . an alternative to adjuvant radiotherapy within 34 months after surgery is the salvage radiotherapy ( srt ) initiated after a psa rise or persistent postoperative psa value [ 29 , 34 , 35 ]  . 
srt should be initiated as early as possible ( psa 0.5 ng / ml ) due to the fact that biochemical ned improves by 1020% as compared to initiation of srt at a psa > 0.5 ng / ml [ 29 , 34 , 35 ]  . 
finally , it should be mentioned , that it is clinically often difficult to differentiate between local relapse and incipient distant metastases because of the limited sensitivity of the imaging modalities in patients with low psa values , to date . brachytherapy is a primary option for patients with ldr monotherapy psa < 10 ng / ml , gleason score < 7 and ct1ct2a tumors . 
randomized trials comparing the different therapeutic concepts do not exist , but there are large cohort studies with psa - free survival rates comparable to a treatment with radical prostatectomy or external - beam radiotherapy [ 27 , 30 , 36 ] and low toxicity rates [ 26 ]  . 
 patients with localized prostate cancer and high - risk factors shall not receive ldr monotherapy . hdr brachytherapy in combination with external - beam radiotherapy is an option for radiation dose escalation . 
hdr brachytherapy is typically applied in two courses with an interval of 1 week and doses of 2 810 gy in combination with a 45to 50 - gy external - beam radiotherapy [ 912 , 15 ]  . 
 due to biochemical relapse - free rates of > 85% after 5 years , this combination is a primary option for treatment of intermediateand high - risk localized prostate cancer and locally advanced prostate cancer . 
also , there is not sufficient data about hdr monotherapy available , which should therefore be used within clinical studies only . synopsis radiotherapy is an equivalent alternative to radical prostatectomy for patients with localized and locally advanced prostate cancer . 
pre vious studies have reported a median survival of 27 months , whereby wholebrain radiotherapy ( wbrt ) constituted the main palliative treatment [ 3 , 11 , 32 , 33 ]  . 
importantly , scarce reports on survival times > 78 months included mainly pa tients with single lesions [ 3 , 33 ]  . several groups have indicated that stereotactic radiosur gery ( srs ) can be a useful alternative approach for the treat ment of patients with brain metastases , with local control ( lc ) and overall survival ( os ) rates comparable to those of surgery ( op ) , in certain cases [ 4 , 5 , 25 , 29 ]  . 
the latter poses a bar rier in getting a better understanding of the precise role of rt and prognostic factors and whether optimization of the current protocols is needed . considering its malignant nature and poor outcome [ 21 ] , an aggressive therapeutic approach for tcc brain metastases would be reasonable . 
furthermore , six important clinical param eters for outcome were analyzed with the aim to detect potential clinical factors for the selection of the appropriate therapy . patients and methods patient characteristics between 1996 and 2007 , 62 patients were treated with either ( 1 ) radiotherapy ( rt , n = 49 ) , including wbrt ( n = 32 ) and / or srs ( n = 17 ) , or ( 2 ) op combined with wbrt ( n = 13 )  . 
further inclusion criteria were : diagnosis of metastases by computed tomography ( ct ) and / or magnetic resonance imag ing ( mri ) , no prior therapy to the brain and administration of steroids . the development of new cerebral lesions constitutes the primary reason of treatment failure in the majority of brain metastases . 
we performed a separate subgroup analysis to compare the differ ent treatments for os and icc in regard to rpa . radiotherapy planning and treatment srs technique was performed as previously described [ 16 , 17 ] and the dose prescribed was according to the rtog criteria [ 4 , 35 ]  . 
wbrt regimen and dose have been also described before [ 12 ]  . patients received their first followup 3 months postrt and thereafter based on their clinical symptomatology to ex clude recurrence and radiation side effects . 
the 1year , 2year , and 3year survival rates from the onset of brain metastases were 17% , 11% , and 8% , respectively . the impact of potential prognostic factors on surviv al is shown in table 3 ( univariate analysis )  . 
on univariate analysis , no significant difference ( p = 0.996 ) in icc was detected between rt and op + rt ( table 4 , figure 2 )  . 
of the patients that developed a recurrence , four re ceived 24 gy ( including two that underwent srs in two and three different regions , respectively ) , seven 18 gy , and one patients 15 gy , while three patients and one patient received 10 3 gy and 20 2 gy wbrt , respectively . patients treated only with rt incorporating srs had a 1 , 2 , and 3year lc probability of 78% , 66% , and 51% . no significant association between lc and any of the po discussion tential prognostic factors was noted . results of univariate subgroup analyses performed sepa rately for rpa class i and iiii patients are shown in table 5 . 
comparison of radiotherapy , including wholebrain radio therapy ( wbrt ) and / or stereotactic radiosurgery ( srs ) , with surgery ( op ) plus wbrt regarding intracerebral control . 
vergleich zwischen ganzhirnbestrahlung ( wbrt ) und / oder stereotaktischer radiochirurgie ( srs ) und resektion ( op ) plus wbrt hinsichtlich der intrazerebralen kontrolle . in metastatic tcc , patients with multiple metastases receiv ing only wbrt have a survival of 24 months [ 9 , 11 , 33 ]  . 
the median os for the entire cohort was 9 months , and the 1 , 2 , and 3year survival rates from the onset of brain metastases were 17% , 11% , and 8% , respectively . 
os rates between rt ( wbrt and / or srs ) and rt + op were not statistically different , indicating the potential of srs in treatment of brain lesions . the advent of new chemotherapy agents and the imple mentation of srs in the treatment of brain metastases have stressed the importance of identifying prognostic factor [ 4 , 23 , 25 , 27 , 29 ]  . 
in tcc patients with cerebral secondaries , how ever , and to the authors best knowledge , no data exist regard ing this issue , probably due to the small number of patients previously studied ( table 1 )  . rpa class has been shown by many authors to be of prog nostic significance in patients with secondary brain tumors [ 4 , 5 , 14 , 29 ]  . 
therefore , srs represents a valuable alternative choice in certain patients [ 25 , 35 ] charac terized by a high lc response rate and low morbidity , as in our present work . 
previous analyses have demonstrated a clear lc and , in some cases , os benefit for srs in patients with a limited number of brain metastases [ 2 , 23 , 25 , 2830 ]  . 
whether srs would demonstrate a survival advantage if only applied in tcc patients with few brain secondaries ( up to three ) in our institute , remains a speculation and a higher number of patients are required to clarify this issue . the rpa parameter is a key determinant of patient sur vival [ 15 , 28 , 29 ]  . 
brain metastases in bladder cancer ferent rpa classes is performed in tcc patients with brain metastases . the opincorporating arm did not show any benefit re garding os , icc , or lc . 
there fore , the value of surgical resection for the treatment of large metastases or those causing mass effects with > 1 cm midline shift and severe acute neurological deficits should not be un derestimated [ 19 ]  . tcc of the bladder is a chemosensitive malignancy [ 8 ]  . 
 the widely applied regimen of methotrexate , vinblastine , doxorubicin and cisplatin ( mvac ) during the 1980s pro longed patients survival up to 14 months and resulted in a slight increase in the reported cases of patients with brain secondaries [ 36 ]  . 
in recent years , gemcitabine combined with cisplatin has substituted the older mvac and it is now consid ered the chemotherapy of choice , because it provided similar response rates associated with less hematologic and mucous toxicity [ 20 , 21 , 38 ]  . 
notably , in the majority of prospective or retrospective analyses that assessed the efficacy of chemother apy in metastatic tcc , patients with brain metastases were either not reported or excluded from the studies [ 8 , 2022 , 38 ]  . 
however , the retrospective nature of the present study limits the ability to draw firm conclusions . grade 3 acute toxicities were found in 3% of patients treated with rt only and in 45% of the op + rt argrade 3 late toxicities occurred in 4% of patients treated with rt and in 56% of op + rt group , which is in line with previous reports [ 4 , 5 , 19 , 28 , 29 ]  . we acknowledge that different factors could potentially influence the present analysis of this retrospective study and bias cannot be excluded . conclusion cerebral metastases in tcc patients remain a lethal disease . 
the identification factors can help stratify patients for more aggressive therapy in selected trials . strahlentherapie und onkologie original article single - arm phase ii study of conformal radiation therapy and temozolomide plus fractionated stereotactic conformal boost in high - grade gliomas final report mario balducci1 , giuseppina apicella1 , 2 , stefania manfrida1 , annunziato mangiola3 , alba fiorentino1 , luigi azario4 , giuseppe roberto dagostino1 , vincenzo frascino1 , nicola dinapoli1 , giovanna mantini1 , alessio albanese3 , pasquale de bonis3 , silvia chiesa1 , vincenzo valentini1 , carmelo anile3 , numa cellini1 purpose : to assess survival , local control and toxicity using fractionated stereotactic conformal radiotherapy ( fscrt ) boost and temozolomide in high - grade gliomas ( hggs )  . patients and methods : patients affected by hgg , with a ctv1 ( clinical target volume , representing tumor bed residual tumor + a margin of 5 mm ) 8 cm were enrolled into this phase ii study . 
radiotherapy ( rt , total dose 6 , 940 cgy ) was administered using a combination of two different techniques : three - dimensional conformal radiotherapy ( 3d - crt , to achieve a dose of 5 , 040 or 5 , 940 cgy ) and fscrt boost ( 19 or 10 gy ) tailored by ctv1 diameter ( 6 cm and > 6 cm , respectively )  . 
the sample size of 41 patients was assessed by the single proportionpowered analysis . results : 41 patients ( 36 with glioblastoma multiforme [ gbm ] and five with anaplastic astrocytoma [ aa ] ) were enrolled ; rtog neurological toxicities g12 and g3 were 12% and 3% , respectively . 
median progression - free survival ( pfs ) was 11 months , in gbm patients 10 months . conclusion : fscrt boost plus temozolomide is well tolerated and seems to increase survival compared to the standard treatment in patients with hgg . key words : malignant glioma stereotactic radiotherapy temozolomide boost strahlenther onkol 2010 ; 186 : 55864 doi 10.1007 / s00066 - 010 - 2101 - x einarmige phase - ii - studie zur konformalen strahlentherapie mit temozolomid plus fraktionierter stereotaktischer konformaler boostbestrahlung bei hhergradigen gliomen . 
die fallzahl wurde mit hilfe eines einfach - proportionalen testverfahrens ( single proportion - powered analysis ) bei 41 patienten bestimmt . 1department of radiotherapy , catholic university of the sacred heart , rome , italy , 2department of radiotherapy , university hospital maggiore della carit , novara , italy , 3department of neurosurgery , catholic university of the sacred heart , rome , italy , 4department of physics , catholic university of the sacred heart , rome , italy . received : november 11 , 2009 ; accepted : april 1 , 2010 published online : september 30 , 2010 strahlenther onkol 2010 no . 
stereotactic conformal therapy boost and temozolomide in hgg ergebnisse : 41 patienten ( 36 mit glioblastoma multiforme [ gbm ] und fnf mit anaplastischem astrozytom [ aa ] ) wurden behandelt ; neurotoxizitt gem rtog - skala g12 bzw . 
die mittlere progressionsfreie berlebenszeit ( pfs ) betrug 11 monate , bei gbm - patienten 10 monate . schlussfolgerung : fscrt - boostbestrahlung plus temozolomid wird gut toleriert und scheint im vergleich zur standardbehandlung die berlebenszeit von patienten mit hmg zu verbessern . schlsselwrter : maligne gliome stereotaktische radiotherapie temozolomid boost introduction high - grade gliomas ( hggs ) have an high tendency to local recurrence , especially within 2 cm of the enhancing edge of the original tumor [ 11 , 19 ]  . 
surgery is limited by the lack of obvious anatomic distinction between tumor and adjacent normal brain tissue and the risk of permanent neurological damage [ 21 ]  . radiation therapy ( rt ) remains the most effective postoperative treatment and a radiation dose - survival relationship has been reported [ 37 ]  . 
dose increased by three - dimensional conformal radiation therapy ( 3d - crt ) is limited by the significant risks of normal brain injury and failed to demonstrate a survival benefit [ 5 , 27 ]  . 
stereotactic rt has been used in the treatment of recurrent gliomas [ 12 , 14 , 33 ] or as a boost in the initial management with encouraging results in retrospective studies [ 3 , 6 , 32 ] with an acceptable toxicity profile in both settings . 
two prospective trials , rtog 93 - 05 and rtog 0023 , failed to demonstrate a survival improvement with stereotactic rt but did not conclude the debate about this therapeutic modality , especially since temozolomide , which , added to rt in concomitant and adjuvant regimen , led to a significant improvement in survival and represents the standard therapy for patients with gbm , was not included in these schedules [ 4 , 34 , 36 ]  . our study was performed in order to assess the impact on survival , local control and toxicity using a fractionated stereotactic boost combined with 3d - crt ( fscrt ) plus temozolomide in the initial management of selected patients with malignant gliomas . patients and methods patients eligibility patients > 18 years of age with a histopathologic diagnosis of supratentorial malignant gliomas ( aa , gbm ) were considered eligible for this study . other inclusion criteria were : no prior cranial rt or chemotherapy ; kps > 70 ; normal hematologic parameters . 
a written informed consent form was required from all patients enrolled . study design all patients were submitted to clinical examination , preoperative and postoperative gadolinium magnetic resonance imaging ( mri )  . patients immobilization was obtained by using a thermoplastic mask ( uni - frame ) during the 3d - crt phase , and by a noninvasive , stereotactic , relocatable immobilization system ( a modified version of leksells frame , by 3d - line s.r.l. , milan , italy ) during the stereotactic phase . image fusion with mri scans was performed for contouring ; ctvs were defined by a radiation oncologist and a neuroradiologist . ctv1 , defined on gadolinium - enhanced t1 - weighted mri scans , was the only volume receiving the stereotactic boost and included surgical cavity contrast enhancement plus residual tumor , if present , plus a 5 - mm margctv2 included ctv1 plus a 10 - mm marg ctv3 was defined with t2 - weighted mri and represented ctv1 plus edema zone . 
 [ 10 ] ; in all patients , however , the oars were outside the ptvs . treatment planning was carried out with the tps eclipse ( varian medical system , palo alto , ca , usa ) for the 3d - crt phase and with tps ergo ( 3d line medical systems , milan , italy ) for the stereotactic treatment . 
in order to reduce acute toxicity in patients with ctv1 > 6 cm ( group b ) , stereotactic boost was delivered only sequentially , in four fractions of 250 cgy each . 
to compare these two schedules with standard radiation dose ( 60 gy ) , we computed the 2 - gy / fraction biologically effective dose ( bed ) according to the linearquadratic model : bed = nd { 1 + [ d / ( / ) ] } where / is 10 for tumor , n is the number of fractions , and d is the dose of fraction . 
2 weeks after the end of rt , temozolomide ( 150200 mg / m2 ) was administered for six cycles or until disease progression / relapse in both groups ( figure 1 )  . 
mri scans were also acquired every three cycles during adjuvant chemotherapy , every 2 months for the first 2 years of follow - up , and every 3 months thereafter . 
the accrual was determined by the single proportion - powered analysis ( systat 11 , spss science , chicago , il , usa ) for testing p0 = 0.265 ( bad response probability , 2 - year survival of the study by stupp et al . ) , p1 = 0.475 ( good response probability of ongoing study ) , = 0.05 , power = 0.8 : a total of 41 subjects were required . 
the analysis of response rate against the h0 ( bad response probability , rtog ) was performed by a single proportion test ( systat 11 , spss science )  . extent of surgery , tumor type , and rpa class were analyzed as potential prognostic factors for os and pfs using the univariate log - rank test [ 22 ]  . 
 the cox proportional hazards model was used for the stepwise multivariate analysis [ 7 ]  . results patients characteristics from november 2003 to march 2008 , 41 patients with histologically confirmed hgg were enrolled . 
thirty - six patients ( 88% ) were affected by gbm , five ( 12% ) by aa . postsurgical mri evaluation showed residual tumor in 28 patients ( 68% )  . toxicity during radiochemotherapy , 12% of patients experienced g12 neurological acute toxicity , such as headache , confusion and seizures , while g3 toxicity was observed in only one patient . 
during adjuvant chemotherapy , g2 hematologic toxicity was seen in 10% of patients and g3 toxicity in 7% of patients , one of which suspended chemotherapy after two cycles . late neurological toxicity included two cases ( 4.8% ) of radionecrosis ( at 14 and 24 months ) in patients submitted to surgery because of the suspicion of a disease recurrence , but without evidence of tumor cells in the histological specimens : of these patients , one died of ovarian cancer after 33 months from the diagnosis of gbm , the other is still alive without evidence of disease . response the 28 patients with subtotal resection were evaluable for response to rt . 
aa : anaplastisches astrozytom ; gbm : glioblastoma multiforme ; rpa : rekursive partitionsanalyse . group a n = 23 3472 group b n = 18 2565 in field ( 95% isodose region ) marginal ( < 80% isodose region ) out of field group a group b total n ( % ) 21 ( 70 ) 3 ( 10 ) 6 ( 20 ) ginal ( 80% , table 3 )  . 
stereotactic conformal therapy boost and temozolomide in hgg discussion despite multimodality therapy for patients with malignant glioma , local control remains the achilles heel , because nearly all patients die of local disease relapse / progression [ 1 , 29 ]  . radiation doses up to 60 gy with old techniques produced considerable incidence of late toxicity ( radionecrosis rate about 18% ) [ 23 ]  . 
3d - crt obtained a reduction of late toxicity but failed to demonstrate a survival benefit , also when using a dose up to 90 gy [ 25 ]  . 
it is important to notice that rtog 0023 trial omits temozolomide , which represents the actual standard chemotherapy . our study is the first prospective , monoinstitutional trial of dose - intense rt using a tailored conformal stereotactic boost plus temozolomide for patients affected by hggs . however , some limits in our study should be underlined . 
 first , we did not compare our results to the previous studies performed with fscrt or radiosurgery , even if our results are better , since none of them included temozolomide in their schedule . 
even if it is hazardous to compare two studies outside a randomized trial , we compared our series with the correspondent subgroup of patients who received a standard radiation dose of 60 gy plus temozolomide in the eortc - ncic trial that , at the moment , represents the standard therapy [ 36 ]  . 
differently by eortc schedule , we chose to underdose temozolomide in both groups ( chemotherapy only in the stereotactic boost - off windows ) to avoid a cumulative neurological toxicity . 
surprisingly , no impact on survival by rpa class was observed in our study : it probably depends on the small size ; therefore , in this context , it has not any clinical relevance . another limit of this study , frequently observed in the literature regarding hggs , could be the presence of a little percentage of aa ( 12% ) , having a more favorable prognosis . 
rtog 93 - 05 and 0023 trials failed to increase outcome when fscrt was used in up - front modality or without temozolomide but they did not definitively solve the role of fscrt boost . in our study , a better outcome is obtained when higher doses ( > 60 gy ) by fscrt are used in combination with temozolomide without worsening the neurological toxicity ( radionecrosis < 5% )  . 
even within the limits of a single - arm phase ii study , the promising results should encourage the start - up of a new prospective trial in gbm patients . strahlentherapie und onkologie original article residual translational and rotational errors after kv x - ray image - guided correction of prostate location using implanted fiducials reinhold graf , dirk boehmer , volker budach , peter wust1 purpose : to evaluate the residual errors and required safety margins after stereoscopic kilovoltage ( kv ) x - ray target localization of the prostate in image - guided radiotherapy ( igrt ) using internal fiducials . patients and methods : radiopaque fiducial markers ( fms ) have been inserted into the prostate in a cohort of 33 patients . 
rotational errors around lr ( x - axis ) , ap ( y ) and si ( z ) have been recorded for the first series of nine patients , and since 2007 for the subsequent 24 patients in addition corrected in each fraction by using the robotic tilt module and varian exact couch . 
die autoren setzten das rntgenbasierte und automatisierte positionierungsund verifikationssystem exactrac / novalis body ( brainlab ag , feldkirchen ) efr die erste serie von neun patienten erfolgten tgliche korrekturen des initalen translationsfehlers in mediolateraler ( ml ) , anteroposteriorer ( ap ) und superoinferiorer ( si ) richtung . 
rotationsfehler um die seitliche ( x ) , vertikale ( y ) und longitudinale achse ( z ) wurden aufgezeichnet und seit 2007 fr die brigen 24 patienten unter verwendung des robotic tilt module und der varian exact couch vor jeder fraktion ausgeglichen . 
noch bestehende residuale fehler wurden aufgezeichnet und erneut winkelgetreu korrigiert . ergebnisse : der residuale translationale fehler betrug in lr , ap und si ( 1 standardabweichung [ sd ] ) 1 , 3 , 1 , 7 und 2 , 2 m ermittelt wurden residuale rotationsfehler ( 1 sd ) um x , y und z von 3 , 2 , 1 , 8 und 1 , 5 . 
die erforderlichen sicherheitsabstnde zwischen klinischem zielvolumen ( ctv ) und planungszielvolumen ( ptv ) wurden in ml , ap und si mit 2 , 3 , 3 , 0 und 3 , 7 mm berechnet . 
nach einem zweiten korrekturschritt konnten diese sicherheitsabstnde auf 1 , 8 , 2 , 1 und 1 , 8 mm verringert werden . schlussfolgerung : auf der grundlage der nach ein ( oder zwei ) lagerungskorrekturen verbleibenden restfehler der patienten dieser studie ist fr das ptv ein sicherheitsabstand von mindestens 2 mm zum ctv erforderlich . 
der beitrag der intrafraktionellen bewegung der prostata fr den lokalisationsfehler verbleibt das thema weiterer untersuchungen . schlsselwrter : bildgesttzte strahlentherapie interne marker sicherheitsabstnde 1department of radiation oncology , charit university medicine berlin , campus virchow - klinikum , berlin , germany . received : march 20 , 2009 ; accepted : july 19 , 2010 published online : september 30 , 2010 strahlenther onkol 2010 no . 
residual errors of the prostate in igrt introduction intensity - modulated radiation therapy ( imrt ) of prostate cancer [ 8 ] leads to steep dose gradients between the planning target volume ( ptv ) and adjacent organs [ 35 ] , which imply the risk of overor underdosing structures on a small - volume scale [ 42 ]  . 
delivery of high doses to the ptv is especially complicated by prostate movement relative to the pelvic bones and skin alignment marks [ 47 ] and motivates the concept of image - guided radiotherapy ( igrt )  . 
clinical application has demonstrated the feasibility of this technique using software - computed table shifts to correct the patient isocenter and rotations to realign the position of the patient prior to every radiotherapy fraction [ 37 ]  . 
 the purpose of this study is to retrospectively assess the magnitude of residual translational and rotational localization errors employing internal markers . patients and methods setup accuracy was measured in a nonrandomized cohort of 33 men undergoing definitive external - beam radiotherapy ( ebrt ) for localized prostate cancer . 
under practical conditions , this time - consuming work was performed in > 60% of fractions , i.e. , in a total of 748 treatment sessions from 2005 until 2008 . two pairs of marker seeds in rapid strand technique were implanted either under ultrasound guidance transperineally by means of a modified biopsy needle or on occasion of a laparoscopic lymphadenectomy . 
since 2007 , each patient has two gold visicoil ( radiomed corp , tyngsboro , ma , usa ) fiducial markers ( fms , 0.75 mm diameter , 3 cm length ) placed into the prostate gland without complications [ 14 ]  . 
in the first four patients , we evaluated the location of the seeds by repeated computed tomography ( ct ) at the end of radiotherapy by measuring the intermarker distances and found that the differences are < 1 mm [ 19 ]  . each patient underwent a treatment - planning ct ( siemens , erlangen , germany ) of the pelvic region in treatment position obtaining volumetric data at 2.5 - mm slice spacing and thickness . 
this limits the accuracy of the marker position in longitudinal direction ( si ) to 2 mm , which , however , matches to the tolerance limits of the system ( see below )  . 
the patients were instructed to fill their bladder in a standardized way and to purge their rectum prior to the planning ct and each radiotherapy fraction , if necessary , by use of an enema . 
the prescribed dose was 72 or 75.6 gy ( icru [ 15 ] ) in the ptv , depending on the risk factors with an integrated boost up to a cumulative dose of 80 or 84 gy in the clinical target volume ( ctv )  . 
 ctv - ptv margins were , in the beginning , 7 , 7 , and 6 mm in the three directions , later we reduced the margins to 5 , 5 , and 3 mm . the details of the x - ray positioning procedure have been described elsewhere [ 38 ]  . 
we did not perform prepositioning using infrared body markers [ 36 ] on a regular basis . position control was performed by the et systefour points representing the centers of the seeds or end of coils were delineated at the et computer station by the radiation oncologist as recognized on the ct dataset . 
then , the difference vector is calculated in six components , i.e. , a set of left - right ( lr , x ) , anterior - posterior ( ap , y ) , and superior - inferior ( si , z ) shift corrections and rotations around the x - , yand z - axis , i.e. , tilt , table , and roll . 
first , the total error is compensated as far as possible by translation , and in a second step the remaining error is reduced by an additional rotation as a second order correction . 
at that time , only translations x , y , z and table rotation ( around y ) have been performed correcting the remaining rotational errors around x and z only approximately ( for 9 / 33 patients )  . after installing the robotics tilt module device ( brainlab ag , feldkirchen , germany ) underneath the table support , also the rotational corrections around x and z could be executed , thus allowing corrections in all six dimensions . 
residual errors of the prostate in igrt if the positional errors exceeded the tolerance limits of the system , i.e. , a translation shift x , y , z of > 2 mm or a rotational correction x , y , z of > 1 , the treatment couch was moved in six coordinates for correction . 
setup deviations were determined and , if necessary , corrected agathese residual correction vectors reflect intrafractional fluctuations of the fm - marked prostate position and therefore indicate the combination of patient movement , intrafraction organ motion and other system - inherent error sources as further evaluated in the present study . 
the ( second ) verification shows , in 90% of fractions , coordinate deviations below the tolerance threshold ( < 2 mm , < 1 ) , and the patient was treated without further adjustment . 
however , we performed no further control using et assuming that the residual errors turn into the tolerance interval after the second correction step . for the whole ensemble , after 784 setup controls and corrections the residual vectors rij were recorded and the mean standard deviation ( sd ) was determined to detect a systematic tendency and to characterize the scatter . 
then , for every single patient j = 1 , , 33 the deviations rij were averaged over all i ( j ) online controls of patient j to achieve the mean systematic error rj for this patient ( see table 1 for definitions )  . 
the sd of this distribution is defined as and represents the contribution of the random residual errors . to calculate the required margin width around the ctv , we used the prescription of van herk et al . 
they estimated the required margin according to the formula 2.5 x , y , z + 0.7 x , y , z to ensure a minimum dose to the ctv of 95% for 90% of the patients allowing significant dose discrepancies in 10% of time ( with sd of systematic errors and sd of random errors )  . descriptive statistical analysis was performed using jmp v7 ( sas institute , cary , nc , usa )  . results a cohort of 33 patients with a random selection of 784 separate radiotherapy fractions ( out of 4042 fractions per patient ) was retrospectively analyzed and 4 , 488 translations along x / y / z axes and rotations around these axes have been recorded in all either three translational coordinates in the first nine patients or the full set of six coordinates in the following 24 patients , and , if necessary , a second set for a further correction . the translational displacements are summarized in table 2 . 
residual translational errors : these are the error vectors ( x , y , z ) i , j remaining after the first setup correction , which starts from the patient position adjusted according to the skin markings . 
residuale translationsfehler : es handelt sich um die fehlervektoren ( x , y , z ) i , j nach der ersten lagerungskorrektur , die nach der patientenlagerung gem hautmarkierungen durchgefhrt wurde . 
residual rotational errors : these are the rotational errors ( x , y , z ) i , j remaining after the first setup correction , which starts from the patient position adjusted according to the skin markings . 
on the right , the standard deviations of the systematic and random rotational displacements around the three main axes for 33 patients ( see table 1 for definition of axes and their orientation )  . 
residuale rotationsfehler : es handelt sich um die rotationsfehler ( x , y , z ) i , nach der ersten lagerungskorrektur , die nach der patientenlagerung gem hautmarkierungen durchgefhrt wurde . 
die rechten spalten zeigen die standardabweichungen der systema tischen und zuflligen rotationsfehler um die drei hauptachsen fr 3 patienten ( siehe tabelle 1 fr definitionen von achsen und deren orientierung )  . 
for the entire group of patients , the standard deviations of systematic errors ( ) and random errors ( ) are listed in every direction after the first and second correction , i.e. , the values 2 mm ( ~ 10% ) above the intervention level are discarded from the distribution after the first run . 
margins of ~ 2 mm ( as estimated after the second run ) are at least required for this technique of image - guidance using exactrac with intraprostatic gold markers . 
fr die gesamte patientengruppe sind die standardabweichungen ( sd ) der systematischen fehler ( ) und zuflligen fehler ( ) in jeder richtung fr die erste und zweite korrektur aufgelistet , d.h. 
die sicherheitsabstnde vom klinischen zielvolumen zum planungszielvolumen in allen drei richtungen werden von den systematischen und zuflligen fehlern gem der formel 2 , 5 + 0 , 7 [ 43 ] berechnet . 
the error is known to be largest in craniocaudal direction , partially caused by prostate movement . the residual rotational errors of the prostate were in the range of 23 and largest around the lr axis ( table 3 ) with 3.2 ( 1 sd )  . 
the residual translational errors , either systematic or random , are well below 1 mm after the second correction . overall , a second correction was necessary in ~ 10% of treatment sessions . 
in 25% ( 8 / 33 of patients ) , an intermediate percentage of 1015% of fractions had to be corrected twice , and only in 15% ( 5 / 33 of patients ) , the percentage of second setup corrections was between 1522% . discussion positioning control is improved by registering bony structures based on a fusion algorithm between planning ct dataset and stereoscopic radiographs , and in the next step by registration of fiducials . 
the random total error regarding fiducials , i.e. , including the motion error , is even 35 mm with a maximum up to 19 mm . other methods to align the patient are based on ultrasound localizations [ 30 ] , electronic portal imaging or xray imaging of implanted markers [ 8 , 11 ] or megavoltage ct fms [ 16 , 20 , 39 ]  . 
the authors describe displacements in the same range as in [ 13 ] , i.e. , especially random errors up to 5 mm . we investigated residual errors after positioning control via intraprostatic fiducials . 
as a result of daily corrections [ 18 ] , systematic errors were in the range of one third of random errors and contributed to treatment margins with < 1 mrandom errors contribute about 2 mm to the localization error . 
 [ 9 ] even threefold . in our study , the residual errors after the first et - guided setup were < 3 mm implying safety margins of 34 ma secstrahlenther onkol 2010 no . 
residual errors of the prostate in igrt ond correction step , which was required with an intervention level of 2 mm in approximately 10% of fractions , lowers the residual errors to < 1 mm and leads to required margins of only 2 mm ( table 4 )  . the predominance of rotational errors around the lr axis ( tilt ) has been described in the literature [ 32 , 41 ] and is confirmed by our study ( table 3 )  . 
 [ 21 ] proposed an alternative strategy : aligning the beam to the patient by repositioning the dynamic multileaf collimator and adjusting the beam weights , termed dynamic compensation . migration of seed strands or markers can be another error source . 
therefore , after a fast second correction of prostate position , we started the radiotherapy . interestingly , larger residual errors ( above the intervention level ) are not equally distributed in all patients . 
while in the majority of patients the error rate is well below 10% , in a specific patient group ( about 15% of patients ) the error rate can be > 15% up to a maximum rate of 22% in our study . 
however , the criteria are not known presently . for the whole daily radiotherapy procedure , lasting up to 1215 min due to imrt , the assessments about intrafractional prostate motion are controversial in the literature . summaries of published results upon intrafraction prostate motion have been compiled by ghilezan et al . 
 [ 28 ] measured smaller intrafractional displacements of the prostate by an ultrasound probe and ascertained sds of 2 mas pointed out elsewhere [ 22 ] , the number and location of prostate surrogates and differences in observation time can explain in part the variation among published prostate intrafraction motion measurements . 
however , even daily repositioning according to anatomic structures fails to achieve a substantial margin reduction in contrast to daily matching internal markers [ 26 ]  . we used the recipe of van herk et al . 
 [ 43 ] and found , according to table 4 , a minimum margin of 2 mm , which is clearly a mean value and not adequate for every patient . 
residual errors are useful to identify a subgroup of 15% of patients requiring higher margins ( see above ) conclusion daily online prostate repositioning via a dedicated x - ray system reduces the setup error to < 2 mresidual errors are supposed to be caused by patient or intrafraction prostate motion , and might be larger in specific patients . 
we guess , however , that criteria can be developed to further reduce margins in most patients . acknowledgment we thank the berliner sparkassenstiftung medizin for very helpful support . strahlentherapie und onkologie original article evaluation of cem43ct90 thermal dose in superficial hyperthermia a retrospective analysis maarten de bruijne1 , bronno van der holt2 , gerard c . 
this study evaluates the cem43ct90 parameter by means of a retrospective analysis of recurrent breast cancer patients receiving reirradiation plus hyperthermia . material and methods : cem43ct90 was calculated for 72 patients who received 8 4 gy reirradiation plus 8 1 h hyperthermia for adenocarcinoma recurrences at the chest wall . 
associations of prognostic factors cem43ct90 and tumor maximum diameter with endpoints complete response ( cr ) , duration of local control ( dlc ) , and overall survival ( os ) were determined . results : a highly significant inverse association between cem43ct90 and tumor maximum diameter ( = 0.7 , p < 1e - 6 ) was found . 
diese studie bewertet die cem43ct90 - parameter durch eine retrospektive analyse vorbestrahlter patienten mit brustkrebsrezidiven , die mit strahlentherapie und hyperthermie behandelt wurden . material und methodik : cem43ct90 wurde berechnet fr 72 patienten mit brustwandrezidiven , welche eine rebestrahlung mit 8 4 gy und 8 1 h hyperthermie erhielten . 
die zusammenhnge der prognostischen faktoren cem43ct90 und maximaler tumordurchmesser mit den endpunkten komplette remission ( cr ) , dauer der lokalen kontrolle ( dlc ) und berleben ( os ) wurden bestimmt . ergebnisse : es fand sich ein hochsignifikanter inverser zusammenhang zwischen cem43ct90 und maximalem tumordurchmesser ( = 0 , 7 ; p < 1e - 6 )  . 
 cr , dlc und os waren nicht signifikant von der thermischen dosis abhngig , wenn fr den maximalen tumordurchmesser angepasst wurde ( p > 0 , 2 )  . schlussfolgerung : in dieser retrospektiven studie konnten keine klaren thermischen dosisziele fr cem43ct90 oder korrelationen mit klinischen endpunkten bestimmt werden . schlsselwrter : lokale oberflchenhyperthermie thermische dosis cem43ct90 brustkrebsrezidiv 1hyperthermia unit , department of radiation oncology , erasmus mc daniel den hoed cancer center , rotterdam , the netherlands , 2department of trials & statistics , erasmus mc daniel den hoed cancer center , rotterdam , the netherlands , received : march 15 , 2010 ; accepted : march 25 , 2010 published online : july 29 , 2010 strahlenther onkol 2010 urban & vogel de bruijne m , et al . 
thermal dose in superficial hyperthermia introduction the identification of quality factors for hyperthermia ( ht ) treatments [ 1 ] has been a central theme in ht research for the last 20 years . 
they range from simple temperature statistics ( e.g. , minimum temperature , median temperature , temperature percentiles , etc . ) to thermal isoeffect dose parameters , which convert the time - temperature data into an isoeffect dose [ 22 ]  . 
several of these have been shown to correlate significantly with complete response ( cr ) , duration of local control ( dlc ) , and overall survival ( os ) [ 3 , 9 , 15 , 18 , 24 ]  . a thermal dose parameter that can be generally adopted should meet the principal requirements of a dose : it should relate to the biological response in a relevant manner , it is a well - defined and measurable quantity , and it can be used as a proper means of comparison [ 8 ]  . 
apart from temperature and duration of treatment other factors may significantly affect the efficacy of ht treatments , for example : ht technique ( e.g. , applicator frequency [ 31 ] , specific absorption rate coverage [ 16 ] ) , previous irradiation ( rt ) [ 11 , 12 ] , tumor size [ 16 , 18 , 20 , 24 , 31 ] and histology [ 18 , 20 ]  . 
since ht is usually applied in combination with rt or chemotherapy , the dose and treatment scheme of the other modality will also influence clinical outcome [ 16 , 18 ]  . 
finally , the quality of the applied thermometry ( number of measurement points , spatial distribution , etc . ) is likely to affect the measured thermal dose [ 24 ]  . 
a quantitative dose measure was introduced to test heatability ( > 0.5 cem43ct90 during the first treatment ) and for the minimum effective dose ( > 10 cem43ct90 for the whole treatment series )  . 
in order to reach this effective dose , a variable number of treatments , and variable treatment lengths were applied . we are now at a point where several randomized clinical trials have demonstrated the significant improvement in clinical response when ht is added to rt , both in fixed schedules [ 11 ] , and in flexible treatment series based on a cem43ct90 thermal dose [ 12 ]  . 
one is : is there a generally applicable minimum effective thermal dose for both approaches ? if cem43ct90 meets the principal requirements of a dose , data obtained in fixed ht schedules should also reflect the effective thermal dose . 
to verify this hypothesis , this study evaluates the cem43ct90 thermal dose parameter by means of a retrospective analysis in a homogeneous group of patients , all of whom received a fixed - schedule superficial ht treatment plus re - rt for breast adenocarcinoma recurrences at the chest wall [ 21 , 23 ]  . material and methods patients and treatments the analysis presented in this paper comprises 72 patients with locoregional breast cancer ( adenocarcinoma ) who received re - rt ( 8 4 gy , twice weekly ) plus ht ( 60 min , after rt ) in our clinic over a period of 5 years . 
a temperature - controlled water bolus was placed between the applicators and the skinterstitial and skin temperatures were measured using stationary singleand multi - sensor fiber - optic probes ( 24 channels )  . 
for more details about the treatment and clinical results , see [ 30 , 31 ]  . prognostic factors two prognostic factors were tested : the thermal dose expressed as cem43ct90 , and tumor maximum diameter . 
the latter , defined as the diameter of the largest tumor lesion in the treatment field , is a representative for tumor physiology , and was included because it proved to be the most significant factor associated with dlc in univariate analysis , and the only significant patient / tumor characteristic in multivariate analysis in a previous analysis of rt plus ht in recurrent breast cancer [ 31 ]  . thermal dose cem43ct90 represents the thermal isoeffect dose expressed in cumulative equivalent minutes ( cem ) at a reference temfigure 1 . 
t90i was determined by linear interpolation in temperature map i ; the t90 rank r in the ordered n - element set of temperatures is r = 0.1 ( n + 1 ) [ 25 ]  . 
 the isoeffect dose acquired over the whole treatment series ( cem43ct90tot ) is the sum of the thermal dose per treatment ( cem43ct90i ) , corrected for treatments for which no data was available : cem43ct90 tot cem43ct90i , ( cid : 0 ) ngiven ndata ( cid : 2 ) ( cid : 0 ) where ngiven is the number of treatments actually given , and ndata the number for which time - temperature data was available . in line with most thermal dose studies in the literature [ 3 , 12 , 15 , 16 , 18 , 24 ] , the analysis was limited to interstitially measured temperatures , since the value of measurements from probes placed between the skin and water bolus was considered questionable [ 34 ]  . two sets of dose parameters were calculated from the clinical data . 
second , it was calculated from all interstitially measured temperatures ( cem43ct90all ) , reflecting the principle that heating macroscopic as well as microscopic tumor is a prerequisite for achieving a lasting clinical response [ 31 ]  . clinical response the aim of the treatments was to achieve local tumor control [ 31 ]  . 
os was defined as the interval between the first treatment and the date of death . statistical analysis due to the skewed distribution of cem43ct90 and tumor maximum diameter values , their logarithms were included in the analysis of prognostic factors . 
figure 3 shows the connection between the number of temperature sensors and cem43ct90tumor and cem43ct90all per treatment . association between prognostic factors as shown in figure 4 , a highly significant negative association was found between tumor maximum diameter and the thermal dose parameters . relation between prognostic variables and clinical response table 2 shows the univariate correlations between the thermal dose parameters and clinical response . 
figure 5 illustrates these trends for dlc and os with kaplan - meier curves for equally sized clusters of low , medium and high cem43ct90tumor . table 2 lists the univariate correlations between tumor maximum diameter and clinical response . 
it can be seen that the trends in figure 6 for maximum diameter are the opposite of the trends in figure 5 for thermal dose , as could be expected from the strong inverse association between the thermal dose parameters and tumor maximum diameter . finally , both prognostic factors were combined in a multivariate analysis . 
the results in table 2 show that the association with thermal dose , when adjusted for tumor maximum diameter , was not significant for either cr , dlc , or os . discussion combined rt and ht is a successful tool in the management of cancer [ 17 , 32 ]  . 
for recurrent breast cancer in previously irradiated areas , cr rates double compared to rt alone ( rt 24 38% ; rt + ht 6878% ) [ 11 , 12 ]  . 
fr cem43ct90tumor betrug die rangkorrelation nach spearman 0 , 70 ( p < 1e - 6 ; n = 62 ) , und fr cem43ct90all 0 , 35 ( p = 0 , 002 ; n = 72 )  . and duration of treatments were fixed , and in schedules where ht duration was varied to reach a certain target dose . 
the current retrospective analysis was performed to investigate whether there is a relation between both approaches in terms of thermal dose . the cr rate of 79% observed in the current analysis shows that the addition of ht was effective , as published cr rates for re - rt alone in comparable patient groups are 2438% [ 11 , 12 , 19 ]  . 
 first , it must be stated that the high ( 79% ) cr rate in the data studied makes the association more difficult to detect statistically given the relatively limited number of patients included . 
third , the interaction between tumor size , number of measurement points , and t90 temperatures may affect the ability of the cem43ct90 quantity to reflect the quality of heating , as will be discussed below . apart from the prospective trial by jones et al . 
 consequently , the published criteria of 0.5 cem43ct90 for heatability and 10 cem43ct90tumor for effective dose [ 12 , 15 ] do not select the responders in our case ( see table 3 )  . 
apparently , quantitative thermal dose measures may have a different impact in different ht centers , due to , e.g. , differences in thermometer placement . strahlenther onkol 2010 de bruijne m , et al . 
raten kompletter remissionen fr untergruppen von patienten , die oder > 10 cem43ct90tumor erhielten ( minimale effektive dosis , n = 56 ) , und von patienten , die oder > 0 , 5 cem43ct90tumor erhielten , whrend der ersten hyperthermiebehandlung ( berwrmbarkeit ; n = 55 , temperaturdaten der ersten behandlung fehlten f r eine patientin )  . criterion total cem43ct90tumor > 10 total cem43ct90tumor 10 cem43ct90tumor first treatment > 0.5 cem43ct90tumor first treatment 0.5 complete response n ( % ) 14 / 18 ( 78% ) 30 / 38 ( 79% ) 20 / 25 ( 80% ) 24 / 30 ( 80% ) mechanism , namely the inverse association between thermal dose and tumor maximum dimension . tumor properties and practical aspects with regard to thermometry and calculation of t90 may contribute to this . 
 first , tumors with a large maximum diameter may represent the more aggressive , faster - growing tumors having better vascularized tissue sections [ 24 ] , adding to the chances of measuring a low t90 , thus a low thermal dose . 
work is currently under way attempting to predict clinical response using treatment - planning models . conclusion our data show a highly significant inverse association between thermal dose and tumor maximum diameter , while no significant association with cr was found . 
from a clinical point of view , no relation between thermal dose and os should be expected , as the vast majority of patients with breast cancer recurrences have metastases elsewhere in the body . 
 [ 24 ] stated that there appears to be no biological rationale why the quality of local treatment would affect os for disease of this type , and suggested that the association would not be caused by any direct effect of the ht treatment . 
we hypothesize that the trends toward better local control and survival for higher thermal doses in the current study can be explained from an underlying tumor selection strahlenther onkol 2010 de bruijne m , et al . 
thermal dose in superficial hyperthermia strahlentherapie und onkologie original article tumor shrinkage assessed by volumetric mri in the long - term follow - up after stereotactic radiotherapy of meningiomas sabrina t . 
astner1 , marilena theodorou1 , mihaela dobrei - ciuchendea1 , florian auer2 , christine kopp1 , michael molls1 , anca - ligia grosu3 purpose : to evaluate tumor volume reduction in the follow - up of meningiomas after fractionated stereotactic radiotherapy ( fsrt ) or linac radiosurgery ( rs ) by using magnetic resonance imaging ( mri )  . patients and methods : in 59 patients with skull base meningiomas , gross tumor volume ( gtv ) was outlined on contrast - enhanced mri before and median 50 months ( range 1192 months ) after stereotactic radiotherapy . 
after fsrt or rs , a mean size reduction of 2545% can be expected within 4 years . key words : meningioma stereotactic radiotherapy therapy response mri strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2138 - x volumetrisch nachgewiesene grenreduktion von meningeomen in der lngerfristigen nachbeobachtung nach stereotaktischer strahlentherapie ziel : evaluation der volumenreduktion von meningeomen in der nachbeobachtung nach fraktionierter stereotaktischer strahlentherapie oder linac - radiochirurgie mit hilfe der magnetresonanztomographie ( mrt )  . patienten und methodik : bei 59 patienten mit schdelbasismeningeomen wurde das tumorvolumen auf den kontrastmittelverstrkten mrt - aufnahmen vor und im median 50 monate ( 1192 monate ) nach stereotaktischer strahlentherapie konturiert . 
die ergebnisse wurden mit den radiologischen befunden verglichen . ergebnisse : die mittlere tumorgre aller 59 meningeome betrug vor strahlentherapie 13 , 9 ml ( 0 , 862 , 9 ml )  . 
in der vorliegenden arbeit konnte gezeigt werden , dass die volumetrische bestimmung 1department of radiotherapy and radiooncology , klinikum rechts der isar , technical university of munich , germany , 2department of neuroradiology , klinikum rechts der isar , technical university of munich , germany , 3department of radiotherapy , university hospital freiburg , germany . received : march 1 , 2010 ; accepted : march 5 , 2010 published online : july 29 , 2010 strahlenther onkol 2010 urban & vogel astner st , et al . 
 nach fraktionierter stereotaktischer strahlentherapie oder radiochirurgie ist innerhalb von 4 jahren eine mittlere grenreduktion von 2545% zu erwarten . schlsselwrter : meningeom stereotaktische strahlentherapie therapieansprechen mrt introduction stereotactic radiotherapy is an established treatment option for meningiomas resulting in local control rates of at least 90% 5 years after treatment [ 2 , 16 , 20 ]  . 
therefore , radiotherapy is indicated as primary treatment or as an addition after incomplete resection ( such as simpson grade iiv )  . linac - based stereotactic radiotherapy offers the advantage of two treatment regimens , radiosurgery ( rs ) and fractionated stereotactic radiotherapy ( fsrt ) [ 1 ]  . 
 however , preexisting symptoms caused by the tumor and aggravation of the symptoms after radiotherapy are challenging , as the differentiation between tumor growth and potential side effects of radiotherapy can be difficult . 
in such cases , it is indispensable to assess the exact tumor volume by cross - sectional imaging , precisely magnetic resonance imaging ( mri ) , in a continuous follow - up series for each individual patient after therapy . data for radiologic response after radiotherapy of meningiomas are heterogeneous , ranging from 13% to 72% of all treated meningiomas [ 2 , 3 , 57 , 1114 , 16 , 17 , 20 , 21 , 23 , 25 ]  . 
moreover , regression of the tumor as assessed by conventional mri seems to differ for rs and fractionated radiotherapy , although local control rates are comparable within the published follow - up time . 
found a higher tumor shrinkage after fsrt than after rs [ 9 ]  . radiologic regression is defined for cancer therapy according to the response evaluation criteria in solid tumors table 1 . 
since all these criteria are not sufficient for irregularly formed tumors , the aim of this study was to quantitatively analyze tumor shrinkage after stereotactic radiotherapy of meningiomas by three - dimensional magnetic resonance imaging ( 3d - mri )  . patients and methods patients 59 patients who received stereotactic radiotherapy between 1999 and 2005 for meningioma in our clinic were invited for a detailed follow - up study using 3d - mri . 
patients were examined using the same mr sequence as it was used for treatment planning . of the 59 patients in our follow - up study , none had progression of the meningioma . 
a summary is shown in table 2 . magnetic resonance imaging mri was performed using a philips 1.5 - t scanner gryoscan acs - nt for radiation treatment planning as well as for follow - up studies . 
axial , spin - echo t1 - weighted sequences were acquired after application of contrast media ( gadolinium - diethylenetriaminepentacetic acid [ gd - dtpa ] , 0.1 mmol / kg body weight )  . 
three - dimensional gradient - echo t1 - weighted sequences with 1.6 mm slice thickness without gap were acquired from foramen magnum to the vertex , perpendicular to the main magnetic field . tumor volume delineation delineation of the tumor volume was performed based on the t1 - weighted mri with gd . 
the tumor margins were delineated on each slice of the preand postradiotherapy mri scans which results in three - dimensional volumes . analysis of diagnostic radiology reports reports of diagnostic radiology from the start of radiotherapy were screened for all patients in the study . 
no standardized protocol was used but included t1 - weighted images after application of gd in at least two planes with slice thickness of 35 m all reports contained measurements of the tumors . 
patients were reported as being in partial remission , if there was any tumor shrinkage , in stable disease , if there was no tumor shrinkage , and in progression , if there was any tumor growth . 
ein falx - cerebri - meningeom vor ( a ) und 6 jahre nach radiochirurgie ( b ) sowie ein schdelbasismeningeom vor ( c ) und 6 jahre nach fsrt ( d )  . 
the difference between the volumes before and after radiotherapy was statistically significant ( p = 0.000 , wilcoxon signed ranks )  . 53 patients underwent fsrt with a median dose of 54 gy ( 41.459.4 gy ) in 30 fractions . 
es zeigt sich kein einfluss einer vorangegangenen operation auf die grenreduktion nach strahlentherapie . time dependency of tumor shrinkage we tested , if tumor shrinkage was time - dependent in the complete patient cohort . 
only six patients showed a size reduction of < 10% ( figure 2 )  . the mean relative tumor shrinkage was 17% , 23% , and 30% for patients treated by fsrt at < 24 , 2448 , and 4872 months after radiotherapy . 
a tendency toward increased shrinkage with longer time after radiotherapy was observed , although the mean relative size reduction was only 26% after > 72 months ( figure 3 )  . 
the median size reduction was significantly less in the time interval up to 48 months compared to later time points ( p = 0.026 ; figure 4 )  . prognostic factors for tumor shrinkage we tested , if tumor shrinkage depended on the absolute tumor volume before radiotherapy and if there was a correlation between tumor shrinkage and patient age or previous surgery . 
furthermore , primary radiotherapy or radiotherapy after previous surgery was not predictive for the magnitude of tumor shrinkage ( figure 6 )  . comparison with radiologic reports all patients in the study underwent a continuous follow - up by regular diagnostic mri scans after radiotherapy . 
in contrast to our volumetric assessment , in 37 patients ( 63% ) the meningiomas were considered to be unchanged in size . discussion we studied the shrinkage of meningiomas at a median of 50 months after fsrt or rs by using volumetric mri . 
unfortunately , different definitions were used such as reduction of at least 50% in the largest tumor dimension , decrease of at least 20% of the pretherapeutic volume , or 2 - mm shrinkage in tumor diameter . the general goal of treating benign tumors by radiotherapy is prevention of further growth . 
this is higher than anticipated from the corresponding rate of conventionally measured radiographic response ( 1427% ) and may be explained by very small size reductions that are not measurable by conventional imaging / measurement techniques . 
 a slow process of remodeling from meningiomas tissue into scar tissue corresponds well to the slow size reduction we could observe in our study . in our study , most of the patients underwent fsrt using a median dose of 54 gy . 
in their study , a reduction in tumor size was seen in all patients 24 months after radiotherapy , which is concordance with our data . in our patients , a relative shrinkage of 25.5% was observed after fsrt using a median dose of 54 gy . 
however , volume reduction was only seen in 15 out of 45 patients ( 33.3% ) , in other words , almost 70% of the tumors were unchanged in size after therapy . 
we claim that volumetric measurement is more accurate than calculating the volume from three diameters . for follow - up care , it is important to find the ideal time interval for mri examinations . 
we did not assess tumor volumes at very early time points such as 6 months after radiotherapy ; however , the time interval after radiotherapy was extended to up to 95 months . 
we observed a statistically significant difference between the median relative tumor volume reduction in the first 48 months and the relative median tumor volume reduction in examinations later than 48 months . 
from this data it might be concluded that shrinkage of meningiomas occurs earlier after rs than after fsrt . it has previously been reported that young age of meningioma patients correlates with higher tumor volume reduction [ 7 ]  . 
additionally , previous surgery did not influence the amount of tumor shrinkage . we saw a discrepancy comparing the results measured by 3d - mri with the regular diagnostic mri reports . 
this shows that 3d - mri is more sensitive to alterations in size and indicates that in patients with newly diagnosed meningioma , who decided for a watchful waiting strategy , volumetric mri can be useful to differentiate tumor progression from stable disease . strahlenther onkol 2010 astner st , et al . 
volumetric mri for follow - up of meningiomas after fsrt conclusion volumetric evaluation of tumor size after radiotherapy of meningiomas using 3d t1gd - mri is a highly precise method to measure tumor regression . 
whether relative size reduction correlates with recurrence - free survival still needs to be determined . strahlentherapie und onkologie case study radiolabeled cetuximab plus whole - brain irradiation ( wbi ) for the treatment of brain metastases from non - small cell lung cancer ( nsclc ) dirk rades1 , roger nadrowitz1 , inga buchmann2 , peter hunold3 , frank noack4 , steven e . 
schild5 , birgit meller2 background and purpose : the addition of systemic drugs to whole - brain irradiation has not improved the survival of patients with multiple brain metastases , most likely because the agents did not readily cross the blood - brain barrier ( bbb )  . 
radiolabeling of cetuximab was performed to investigate whether this antibody crosses the bbb . case report : a patient with multiple brain lesions from non - small cell lung cancer was investigated . 
weekly doses of 250 mg / m2 cetuximab were administered for 3 months . results : the reference lesion showed enhancement of radiolabeled cetuximab ( 123i - erbi ) on scintigraphy ; 123i - erbi crossed the bbb and accumulated in the lesion . 
enhancement of contrast medium was less pronounced . conclusion : this is the first demonstration of cetuximab crossing the bbb and accumulating in brain metastasis . key words : non - small cell lung cancer brain metastases radiolabeled cetuximab blood - brain barrier strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2153 - y radioaktiv markiertes cetuximab plus ganzhirnbestrahlung ( wbi ) bei der behandlung von hirnmetastasen eines nichtkleinzelligen bronchialkarzinoms ( nsclc ) hintergrund und ziel : durch die systemische gabe von medikamenten zustzlich zur ganzhirnbestrahlung wurde bislang keine verbesserung des berlebens von patienten mit multiplen hirnmetastasen erreicht , hchstwahrscheinlich , weil die substanzen die blut - hirn - schranke ( bbb ) nicht adquat berwinden . 
an tag 1 wurden 200 mg / m2 cetuximab ( 0 , 25% heier und 99 , 75% kalter antikrper ) appliziert , an tag 3 erneut 200 mg / m2 cetuximab ( kalter antikrper )  . 
anschlieend wurden wchentlich 250 mg / m2 cetuximab fr 3 monate verabreicht . ergebnisse : in der szintigraphie zeigte die referenzmetastase eine anreicherung des radioaktiv markierten cetuximabs ( 123i - erbi , abbildung 2 )  . 
die kontrastmittelanreicherung war geringer ausgeprgt . schlussfolgerung : erstmals wird gezeigt , dass cetuximab die bbb passiert und sich in einer hirnmetastase anreichert . schlsselwrter : nichtkleinzelliges bronchialkarzinom hirnmetastasen radioaktiv markiertes cetuximab blut - hirn - schranke 1department of radiation oncology , university of lbeck , germany , 2section of nuclear medicine , university of lbeck , germany , 3department of radiology , university of lbeck , germany , 4institute of pathology , university of lbeck , germany , 5department of radiation oncology , mayo clinic , scottsdale , az , usa . received : march 31 , 2010 ; accepted : april 28 , 2010 published online : july 29 , 2010 strahlenther onkol 2010 urban & vogel rades d , et al . 
to date , the addition of systemic drugs has not improved survival of these patients , most likely because the agents did not readily cross the blood - brain barrier ( bbb ) [ 12 , 19 , 20 ]  . 
the most common primary tumor of patients developing multiple brain metastases is non - small cell lung cancer ( nsclc ) , which accounts for about 50% of these patients [ 10 , 1316 ]  . 
in this study , we treated a patient with multiple brain lesions from nsclc with wbi plus cetuximab to answer the question whether cetuximab crosses the bbb and accumulates in the metastases . 
in case of a negative result , it was to be stopped . case report a 49 - year - old man presented with a 4 - week history of progressive weakness , weight loss , headache , nausea , and vomiting . 
 this metastasis was selected the reference lesion for investigating potential accumulation of radioiodinated cetuximab ( 123i - erbi ) , as lesions < 20 mm in diameter are likely to be missed by 123i whole - body scintigraphy including single - photon emission tomography ( spect )  . 
radiolabeling of 1 mg cetuximab was performed with 370 mbq 123i according to our previous investigations [ 18 ]  . after signed informed consent , the loading dose of 400 mg / m2 cetuximab was given intravenously in two doses of 200 mg / m2 for safety reasons . 
123i - erbi whole - body scintiscans ( prism 2000 xp , philips , amsterdam , the netherlands , meuhr collimators , whole - body scan : matrix 256 1 , 024 , time 30 min ) were obtained at 30 min and 2 , 4 , 24 , and 48 h after application of 222 mbq 123i - erbi before and 1 month after wbi . 
additionally , spect of the head ( meuhr collimators , matrix 256 256 , zoom 1.48 , 30 steps , 6070 s / step ) was performed at 24 and 48 h . 
 weekly doses of 250 mg / m2 cetuximab were administered for 3 months ( during and following wbi )  . spect revealed accumulation of 123i - erbi within the reference lesion , while in whole - body scintiscans only large vessels and reticular endothelial system could be visualized . 
 only depilation and a moderate cetuximab - related acneiform rash occurred that resolved after 10 days of oral minocycline administration . discussion patients with multiple brain metastases have a poor prognosis , generally surviving only a few months following wbi . 
spect investigation of the head prior to whole - brain irradiation ( meuhr collimators , matrix 256 256 , 30 steps , 6070 s / step ) , 24 h after administration of 222 mbq 123i - erbi . 
spect - untersuchung des kopfes vor der ganzhirnbestrahlung ( meuhr collimators , matrix 256 256 , 30 steps , 6070 s / step ) , 24 h nach der gabe von 222 mbq 123i - erbi . 
a recent study suggested that in lung cancer kras mutations may not play a significant role for response to cetuximab which appears contrary to the situation with colorectal cancer [ 9 ]  . 
a later study , published in 2001 , included wbi plus cisplatin / vinorelbine that was associated with a 7% rate of treatment - related mortality [ 19 ]  . 
however , taking into account the pharmacological and pharmacodynamic nature of cetuximab , this approach can only be successful , if the radiolabeled cetuximab is stable for at least 48 h . 
this prerequisite of stability for at least 48 h has been documented in our preceding in vitro studies [ 18 ]  . the question whether cetuximab can cross the bbb still remained . 
only depilation and a moderate cetuximab - related acneiform rash occurred that resolved after 10 days of oral minocycline administration ( 50 mg twice daily )  . conclusion radioiodinated cetuximab ( 123i - rbi ) crossed the bbb and accumulated in brain metastasis from nsclc . 
furthermore , the study of novel combinations of therapy such as described here appears warranted . strahlentherapie und onkologie aktuelles forum geriatrie und radioonkologie teil 1 : identifikation des risikopatienten und grundstzliches zur behandlung franziska fels1 , 2 , johannes w . 
grabenbauer1 hintergrund : bis zur jahrhundertmitte werden voraussichtlich 33% der westlichen population 65 jahre alt seder anteil der 80 - jhrigen an der bevlkerung liegt heute bei 5% , er wird sich bis 2050 verdreifacht haben . 
in dieser situation muss der radioonkologe mit den speziellen fragen des geriatrischen patienten mehr und mehr vertraut sein , um interdisziplinr kooperationsfhig zu sein und fr den individuellen patienten ntzliche therapiekonzepte anzubieten . patienten und methodik : in dieser bersichtsarbeit werden grundlegende daten zur definition , identifikation und therapie des geriatrischen tumorpatienten dargestellt . ergebnisse : der geriatrische patient ist durch eine geriatrietypische multimorbiditt ( 15 merkmalskomplexe ) und durch eine alterstypische vulnerabilitt definiert . 
die identifikation des geriatrischen patienten erfolgt anhand eines basisassessments : mit hilfe des barthel - index werden selbststndigkeit und aktivitten des tglichen lebens , mit dem mini - mental - status - test die kognitive leistungsfhigkeit und mit dem timed up&go - test die mobilitt evaluiert . 
im hinblick auf die medikamentse tumortherapie gilt als nachgewiesen , dass etablierte standardtherapien zu erheblich strkerer toxizitt fhren , so dass dosismodifikationen und supportiven manahmen eine besondere bedeutung zukommt . schlussfolgerung : der geriatrische tumorpatient muss zunchst mit hilfe geeigneter messinstrumente identifiziert werden . 
die radiotherapie stellt aufgrund der fehlenden invasivitt und der nicht notwendigen immobilisierung eine zu bevorzugende therapie dar . schlsselwrter : geriatrischer patient chemotherapie radiotherapie strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2045 - 1 geriatrics and radiation oncology . 
part 1 : how to identify high - risk patients and basic treatment principles background : until the mid of this century , 33% of the western population will be 65 years old . 
therefore , radiation oncologists must be familiar with special geriatric issues to meet the increasing demand for multidisciplinary cooperation and to offer useful and individual treatment concepts . patients and methods : this review article will provide basic data on the definition , identification and treatment of geriatric cancer patients . results : the geriatric patient is defined by typical multimorbidity ( 15 items ) and by age - related increased vulnerability . 
best initial identification of geriatric patients will be provided by assessment including the barthel index evaluating self - care and activity in daily life , by the mini - mental status test that will address cognitive pattern , and by the timed up&go test for evaluation of mobility . 
as for chemotherapy , standard treatment was associated with increased toxicity , consequently , dose modifications and supportive treatment are of special importance . conclusion : geriatric cancer patients need to be identified by special assessment instruments . 
im hinblick auf die epidemiologie erscheint es auch fr den strahlentherapeutisch ttigen arzt sinnvoll , sich mit geriatrischem fachwissen zu beschftigen , da diese epidemiologie auch ganz konkreten einfluss auf die prvalenz onkologischer erkrankungen und die medizinische versorgung in der onkologie hat : die anzahl geriatrischer patienten in der strahlentherapie und onkologie wird stark zunehmen , da tumoren mit wenigen ausnahmen eine erkrankung des hheren lebensalters sind . 
ursache dieses altersabhngigen anstiegs der krebserkrankungen ist zum einen , dass im rahmen des alterungsprozesses die dna geschdigt wird , was zu zellentartungen fhren kann ; zum anderen lassen abwehrkrfte gegenber dem tumorwachstum im alter nach . zwischen einer stadiengerechten tumortherapie und der realitt der behandlung alter krebspatienten besteht allerdings eine deutliche diskrepanz . 
so wurde in einer kohortenstudie des krebsregisters rostock gezeigt , dass der relative anteil kolorektaler karzinome mit zunehmendem alter ansteigt , wohingegen der anteil der patienten , die in bereinstimmung mit den derzeit gltigen therapieempfehlungen eine chemooder radiochemotherapie erhalten , mit zunehmendem alter abnimmt ( stadium iii ) [ 14 ]  . 
in einer lteren amerikanischen studie wurde fr ltere patienten mit kolonkarzinom im uicc - stadium iii hnliches festgestellt , wofr folgende grnde angegeben wurden : in den meisten fllen wurde dem patienten die therapie nicht angeboten ( 34% ) , der patient lehnte die therapie ab ( 11% ) , die behandelnden rzte hielten den patienten fr zu alt fr die therapie ( 7% ) , der patient wies zu viele komorbiditten auf ( 5% ) [ 26 ]  . 
fr die radioonkologie , angesichts der datenlage fr das mammakarzinom , die kopf - hals - tumoren , das nichtkleinzellige bronchialkarzinom , das endometriumkarzinom und die kolorektalen karzinome auch betagten patienten eine hochdosierte strahlentherapie nach neuestem stand der technik nicht vorzuenthalten , da lokoregionre rezidive zumeist innerhalb von 24 jahren auftreten und somit vielfach noch erlebt werden [ 41 ]  . der vorliegende artikel soll zunchst eine definition geriatrischer patienten liefern und anschlieend fr einen strahlentherapeuten / onkologen bedeutende altersphysiologische vernderungen vorstellen . 
des weiteren werden das geriatrische basisassessment und seine bedeutung in der onkologie vorgestellt . definition geriatrischer patienten ein blick auf die demographischen daten macht die notwendigkeit einer geriatrischen medizin deutlich , wobei ber die definition geriatrischer patient uneinigkeit herrscht . 
eine arbeitsgruppe aus vertretern der deutschen gesellschaft fr geriatrie , der deutschen gesellschaft fr gerontologie und geriatrie und der bundesarbeitsgemeinschaft der klinisch - geriatrischen einrichtungen einigte sich auf folgende definition geriatrischer patienten : geriatrische patienten sind demnach definiert durch ( cid : 129 ) geriatrietypische multimorbiditt und ( cid : 129 ) hheres lebensalter ( berwiegend 70 jahre )  . die geriatrietypische multimorbiditt ist hierbei vorrangig vor dem kalendarischen alter zu sehen oder als folge eines alters 80 jahre , aufgrund der alterstypischen erhhten vulnerabilitt , z . 
definition geriatrischer patienten ist also die geriatrietypische multimorbiditt , die von solcher wichtigkeit ist , dass auch patienten , die < 70 jahre sind , die also das alterskriterium nicht erfllen , unter die definition fallen , wenn kriterien der multimorbiditt vorliegen . 
nach der gesundheitsberichterstattung des bundes ist multimorbiditt definiert als auftreten mehrerer krankheiten zur gleichen zeit . im jahr 2003 verstndigte sich die gemeinsame arbeitsgruppe der bundesgemeinschaft der klinisch - geriatrischen einrichtungen e . 
laut essener konsensus - konferenz dient die festlegung der merkmalskomplexe zum einen dazu , operationalisierbare kriterien zur beschreibung des geriatrischen patienten festzulegen und in einem weiteren schritt eine zuordnung geriatrischer behandlungsformen zu bestimmten geriatrischen patientengruppen zu erreichen , zum anderen , um im zuge der strahlenther onkol 2010 fels f , et al . 
 ( fortsetzung ) merkmalskomplex ( unterteilt in beispiele der icd - kodierung ) sensibilittsstrungen sensibilittsstrungen der haut krankheiten von nerven , nervenwurzeln und - plexus polyneuropathien und sonstige krankheiten des peripheren nervensystems merkmalskomplex ( unterteilt in beispiele der icd - kodierung ) immobilitt nach medizinischen manahmen altersund / oder morbidittsbedingt ( inklusive paraplegiebedingt ) inaktivittsatrophie sturzneigung und schwindel gangunsicherheit strze , sturzkrankheit schwindel durch strungen der vestibularfunktion kognitive defizite demenz bei alzheimer - krankheit vaskulre demenz delir ohne demenz inkontinenz harninkontinenz drang - / reflex - / berlaufinkontinenz stuhlinkontinenz dekubitalulzera dekubitus ulcus cruris chronisches hautulkus fehlund mangelernhrung kachexie alimentrer marasmus protein - kalorien - mangelernhrung strung im flssigkeitsund elektrolythaushalt dehydratation / volumenmangel sonstige strungen des wasserund elektrolythaushalts dem , anderenorts nicht klassifiziert , auch lymphdem depression und angststrung depressive episode manische episode angststrungen , phobische strungen schmerz schmerz , anderenorts nicht lokalisiert akut chronisch unbeeinflussbar sonstiger chronischer schmerz lokalisierte organbezogene schmerzen gebrechlichkeit , herabgesetzte belastbarkeit frailty - syndrom starke sehoder hrbehinderung presbyopie blindheit und sehschwche sonstiger hrverlust toxisch presbyakusis hrsturz medikationsprobleme uaw bei indikationsgerechter anwendung und korrekter dosierung akzidentelle vergiftung ( berdosierung , einnahme falsches medikament ) hohes komplikationsrisiko unmittelbar vorausgegangene operation vorhandensein knstlicher krperffnungen absolute arrhythmie bei vorhofflimmern verzgerte rekonvaleszenz rekonvaleszenz drg - einfhrung eine abgrenzung geriatrischer leistungsbereiche untereinander und zugleich gegenber unmittelbar angrenzenden leistungsbereichen anderer fachgebiete zu erreichen [ 6 ]  . das alter der altersaspekt ist im hinblick auf die medizinische behandlung von groer bedeutung und kann auch als alleiniges definitionskriterium gelten ( bei patienten 80 jahren )  . 
alter an sich ist ja noch nichts pathologisches , aber es zeigt sich , wie es in der definition heit , eine alterstypische erhhte vulnerabilitt , die das auftreten von komplikationen und folgeerkrankungen begnstigt und die gefahr der chronifizierung sowie das erhhte risiko eines verlusts der autonomie mit verschlechterung des selbsthilfestatus in sich birgt . 
auf wichtige funktionseinschrnkungen der einzelnen organsysteme mit ihrer bedeutung im hinblick auf die alterstypische vulnerabilitt sowie ihre klinischen konsequenzen vor allem im bereich der strahlentherapie / onkologie soll im folgenden kurz eingegangen werden . strahlenther onkol 2010 fels f , et al . 
bei schwerwiegender gefhrdung des patienten durch schrittmacherausfall sollten ein ekg - monitoring whrend jeder therapie und eine anschlieende funktionskontrolle erfolgen [ 19 , 24 ]  . auerdem nimmt bei lteren menschen die zahl der myozyten ab , und begleiterkrankungen wie hypertonie und koronare herzkrankheit beeintrchtigen die herzfunktion . 
 eine mgliche , jedoch kostenintensive alternative stellt der einsatz liposomal verkapselter anthracycline dar , die mit einem deutlich geringeren risiko fr kardiotoxizitt einhergehen und deutlich hhere kumulativdosen erlauben [ 20 ]  . atmungsapparat auch der atmungsapparat zeigt typische altersvernderungen . 
das intrathorakale gasvolumen nimmt dagegen zu , bei mnnern um 170 ml / jahrzehnt , bei frauen dagegen nur um 30 ml / jahrzehnt ( altersemphysem ) [ 40 ]  . 
bei einer therapie mit potentiell pneumotoxischen zytostatika steigt die gefahr der lungenschdigung [ 2 ]  . zudem sind der mukozilire transport und der hustenreflex altersbedingt eingeschrnkt , ebenso die organspezifische abwehr , was sich beispielsweise in einer verzgerten antikrperproduktion gegen pneumokokkenoder influenzavakzine uert [ 45 ]  . 
aufgrund dieser funktionseinschrnkungen treten die hchste altersspezifische inzidenz und letalitt invasiver pneumokokkeninfektionen neben den < 2 - jhrigen vor allem bei den > 60 - jhrigen auf , und auch erkrankungen wie chronische bronchitis und obstruktive atemwegserkrankungen hufen sich im alter . 
diagnostisch wichtig ist , dass mit dem alter die aussagekraft des serumkreatinins als parameter der nierenfunktion abnimmt , da die muskelmasse und damit die endogene kreatininfreisetzung und die kreatininausscheidung im urin mit zunehmendem alter vergleichbar schnell abnehmen und damit der serumkreatininwert trotz eingeschrnkter kreatininclearance hufig im normalbereich bleibt . 
besser ist die berechnung der kreatininclearance nach der cockroft - gault - formel , da in dieser das alter bercksichtigt wird und die gltigkeit der formel als dosierungsrichtlinie in zahlreichen studien untersucht wurde [ 31 ]  . im bereich der onkologie ist eine eingeschrnkte nierenfunktion besonders unter chemotherapie relevant . 
hieraus konnten auf der basis pharmakologischer daten folgende formeln fr die berechnung der dosis in abhngigkeit von der gfr abgeleitet werden : fr nicht mit nephrotoxischen medikamenten vorbehandelte patienten : % der solldosis = ( 0 , 82 gfr ) + 18 ; fr mit nephrotoxischen medikamenten vorbehandelte patienten : % der solldosis = ( 0 , 65 gfr ) + 18 . obwohl die formeln auf die pharmakokinetik von carboplatin zurckgehen , knnen sie auch anhaltspunkt fr die dosierung der anderen hauptschlich renal eliminierten zytostatika sein [ 37 ]  . 
auerdem sollte unter chemotherapie eine gleichzeitige gabe nephrotoxischer substanzen vermieden werden , und insbesondere bei platinhaltiger therapie sollte eine nephroprotektion mit theophyllin oder amifostin erfolgen [ 20 ]  . leber funktionseinschrnkungen der leber werden am ehesten unter belastung manifest , d . 
lebensdekade ( von 1 500 auf 900 cm3 ) [ 44 ]  . eine formel zur berechnung der altersabhngigen leberleistung existiert ( im gegensatz zur berechnung der nierenleistung ) allerdings nicht , so dass als parameter zur abschtzung der leberfunktion genau wie beim jngeren patienten das bilirubin , die glutamat - oxalacetat - transaminase und die alkalische phosphatase dienen . 
 minimale zellzahl im intervall ( nadir ) leukozyten / > 2 000 2 0001 000 < 1 000 thrombozyten / > 100 000 100 00050 000 < 50 000 zytostatikadosis im nchsten zyklus dosissteigerung um 20% mglich keine dosismodifikation dosisreduktion um 20% erforderlich blut zutrifft und sich in einer zunahme von schwere und dauer einer zytopenie uern kann [ 37 ]  . klinisch im rahmen einer zytostatischen chemotherapie bedeutsam ist das fehlen eines verlsslichen , routinemig feststellbaren hmatologischen messwerts , der die regenerationsfhigkeit des knochenmarks prospektiv quantifizieren knnte . 
des weiteren empfiehlt sich der einsatz hmatopoetischer wachstumsfaktoren bei myelosuppressiver chemotherapie bereits prophylaktisch ab dem ersten zyklus [ 20 ]  . nervensystem ein weiteres problem ist der anstieg der demenzerkrankungen im alter . 
die problematik der demenzen liegt darin , dass sie oft einen strenden einfluss auf den verlauf der krperlichen krankheiten und den therapieerfolg zeigen ( problem der non - compliance ) und sich nahezu auf alle handlungen und damit lebensbereiche des patienten auswirken . 
gerade im bereich der onkologie mit langfristigen , nebenwirkungsreichen therapien muss sich der behandelnde arzt der problematik einer mangelnden entscheidungsund einsichtsfhigkeit bewusst sein . die alterung des nervensystems zeigt sich neben einem verlust an neuronen auch in einer verzgerung der nervenleitgeschwindigkeit und der synaptischen bertragung . 
auerdem sollten die gesamtdosis von vincristin auf 2 mg absolut alle 14 tage limitiert sowie die applikationsdauer von vinca - alkaloiden verlngert werden [ 20 ]  . sinnesorgane presbyakusis und presbyopie stellen eine beeintrchtigung der selbststndigkeit des alten menschen dar , weswegen die beiden diagnosen auch zu den merkmalskomplexen der essener konsensus - konferenz zhlen . 
diese wiederum ist ein wichtiger parameter im hinblick auf die frage , ob ein patient krperlich in der lage ist , eine systemische chemotherapie zu verkraften [ 2 ]  . immunsystem schon nach dem 40 . 
bei 25% der frauen > 60 jahre ist die osteopenie schon derart aus geprgt , dass eine osteoporose und damit wirbelkrperdeformierungen auftreten ; bei 8% der frauen im alter von 5080 jahren zeigen sich wirbelkrperfrakturen . 
das relative risiko fr eine osteoporotische hftfraktur steigt alle 5 jahre um den faktor 1 , 42 , 0 [ 1 ]  . muskelatrophie , knochenabbau und gelenksteife sind wesentliche faktoren , die zum sog . 
die mittlere medikamentenzahl bei aufnahme betrug 7 , 5 3 , 8 , knapp 60% der patienten erfllten das gewhlte kriterium der polypharmakotherapie ( mehr als sechs medikamente )  . 
 der behandelnde arzt sollte daher auf diese gesundheitlichen probleme reagieren und zudem auf klare und einfache einnahmeund dosierungsanweisungen achten . psychoonkologische untersttzung neben den behandlungsbesonderheiten im somatischen bereich drfen die vernderungen im psychischen bereich und die sich daraus ergebenden forderungen nicht vergessen werden . 
oft resultieren krankheitsbezogene ngste dabei weniger aus der lebensbedrohung an sich , sondern daraus , dass durch krankheit und behandlung ein verlust der verbliebenen lebensqualitt befrchtet wird [ 9 ]  . 
auerdem ist gerade fr ltere tumorpatienten psychoonkologische untersttzung hilfreich und erfolgversprechend und sollte vor allem dann gefrdert werden , wenn wenig untersttzung von familie und angehrigen geleistet wird [ 9 ]  . das geriatrische basisassessment im folgenden werden das geriatrische basisassessment sowie onkologische testverfahren vorgestellt . das basisassessment hilft , bereiche , in denen bei alten patienten hufig defizite zu finden sind , systematisch zu untersuchen , da diese der etablierten anamneseerhebung und der klinischen untersuchung hufig entgehen [ 42 ]  . 
angewiesen ? ist eine institutionalisierte pflege erforderlich ? mit welchen ressourcen ist eine rehabilitation mit dem ziel , selbststndigkeit im bereich der aktivitten des tglichen lebens zu erlangen , durchzufhren ? erfasst werden im einzelnen : geriatrisches screening nach lachs [ 23 ] , selbsthilfefhigkeit durch den barthel - index [ 25 ] , kognition durch den mini - mental - status - test ( mmst ) mobilitt durch den timed up&go - test [ 32 ] , ernhrungsstatus durch das mini nutritional assess [ 15 ] , ment [ 29 ] , strahlenther onkol 2010 fels f , et al . 
werden 12 punkte erreicht ( normaler ernhrungszustand ) , kann die befragung beendet werden , liegt das ergebnis der voranamnese bei < 12 punkten , wird die anamnese fortgesetzt maximal sind 30 punkte zu erreichen 1723 , 5 punkte : risikobereich fr unterernhrung < 17 punkte : schlechter ernhrungszustand einfache durchfhrung , delegierbar keine relativ umfnglicher erfassungsbogen zur sozialen situation , erfassung wesentlicher personenund umfeldbezogener kontextfaktoren : angaben zu sozialen kontakten und untersttzung , aktivitten , wirtschaftlichen verhltnissen und zur wohnsituation fragen in offener form stellen ; nur wenn antworten den vorgegebenen kategorien nicht eindeutig zugeordnet werden knnen , sollte eine festlegung auf die angegebenen antwortmglichkeiten erfolgen maximal sind 25 punkte zu erreichen ab 17 punkten besteht dringender anlass , die soziale gesamtsituation zu klren , z . 
durch einschaltung des sozialdienstes einfache durchfhrung , delegierbar das instrument geht einerseits mit relativ hohem erhebungsaufwand sehr ins detail , ist dennoch in der regel fr die lsung konkreter patientenbezogener probleme nicht ausreichend , so dass hierfr meist noch eine weitergehende spezifische anamnese ( beispielweise durch den sozialdienst ) erforderlich ist festlegung eines summenscorebezogenen cut - off - werts erscheint im hinblick auf die heterogenitt der erhebungsbereiche zweifelhaft depression ber die geriatric depression scale [ 43 ] , soziale situation des patienten ber den sozialfragebogen nach nikolaus [ 30 ]  . ziel des geriatrischen basisassessments ist es , risikopatienten und risikokonstellationen frhzeitig zu erkennen , um anschlieend zu einer gezielten reha - planung sowie zu einem zielgerichteten einsatz des therapeutisch - rehabilitativen teams unter dem aspekt einer objektivierbaren verlaufskontrolle zu kommen . 
eine bersicht ber die einzelnen assessmentinstrumente gibt tabelle 3 . fallstricke des geriatrischen basisassessments um assessmentergebnisse angemessen bewerten zu knnen , ist es wichtig , sich einige einschrnkungen und fallstricke klarzumachen [ 22 ]  . 
als beispiel sei ein mit einem unterzuckerungsbedingten schock ins krankenhaus eingelieferter bewusstloser diabetiker genannt , der zum aufnahmezeitpunkt einen barthel - index von 0 , 2 h spter nach ausgleich seines zuckerstoffwechsels aber wieder einen barthel - index von 100 punkten haben kann . 
 charlson - komorbidittsindex kurzbeschreibung durchfhrung interpretation vorzge einschrnkungen karnofsky - index kurzbeschreibung durchfhrung interpretation vorzge einschrnkungen feststellung der begleiterkrankungen bei tumorpatienten checklistenartige erfassung von komorbiditten anhand einer liste von 19 begleiterkrankungen , die mit 16 punkten ( je nach schweregrad ) bewertet sind die gelisteten begleiterkrankungen erhhen die 1 - jahres - mortalitt um den faktor 1 , 2 keine patientenbefragung notwendig , ermittlung der begleiterkrankungen nur mit hilfe der krankenakte , schnelle erhebung nicht alle relevanten begleiterkrankungen gelistet beurteilung der einschrnkung von aktivitt und fhigkeit zur selbstversorgung bei tumorpatienten insgesamt sind 0100% erreichbar einstufung nach beurteilung der aktivitt und selbstversorgung abstufung in 10% - schritten von 100% = keinerlei einschrnkungen bis 0% = tod validierter index zur prognoseeinschtzung im hinblick auf die berlebenszeit nur orientierende bersicht ber die fhigkeit zur selbstversorgung ; keine genauere definition der erforderlichen hilfe der onkologie etablierten skalen zur ermittlung des funktionellen status mit denen aus der geriatrie , die informationen sind aber nicht identisch . 
die geriatrischen skalen sind sensitiver fr altersabhngige vernderungen [ 42 ]  . geriatrisches assessment in der onkologie in der onkologie flieen die charakteristika der krebserkrankung , des patienten und der therapie in die therapieentscheidung ewedding et al . 
70 jahren das konventionelle onkologische vorgehen um ein systematisches geriatrisches assessment erweitert werden sollte , da ab diesem alter die prvalenz relevanter funktioneller einschrnkungen deutlich zunehme [ 42 ]  . 
der funktionelle status des patienten orientiert sich hierbei am barthel - index zur beurteilung der aktivitten des tglichen lebens ( adl ) , am iadl zur beurteilung der erweiterten aktivitten des tglichen lebens und am charlson - index zur beurteilung der komorbiditten . gruppe 1 besteht aus patienten ohne deutliche einschrnkung des funktionellen status und ohne schwerwiegende komorbiditten ; hier ist eine intensive chemotherapie mit dem ziel der heilung bzw . 
jeder der patienten ( alter > 70 und vorliegen einer tumorerkrankung oder malignen hmatologischen erkrankung ) wurde dabei nach abschluss des geriatrischen assessments nach den einteilungskriterien von balducci & extermann einer der drei definierten gruppen ( fit , eingeschrnkt therapiefhig , gebrechlich ) zugeordnet . 
es konnte gezeigt werden , dass die verwendung eines geriatrischen assessments bei alten patienten mit krebserkrankungen zur erkennung von vernderungen fhrt , die ohne dieses vorgehen nicht erkannt worden wren [ 13 ] , diese vernderungen zu einer nderung der therapieentscheidung fhren knnen und sie prognostisch fr die endpunkte schwere toxizitt und berleben [ 16 ] relevant sind . von grter wichtigkeit ist jedoch , dass durch ein geriatrisches assessment und eine daran anschlieende zielgerichtete intervention die prognose des patienten verbessert strahlenther onkol 2010 fels f , et al . 
zeigen sich durch die kombination von assessment und zielgerichteter behandlung eine deutliche senkung der mortalitt ( reduktion der 6 - monats - mortalitt um 37% bei stationren patienten einer geriatrie ) sowie eine zunahme der selbststndigkeit des patienten im alltag [ 36 ]  . 
konnten ebenfalls nachweisen , dass diejenigen patienten , die ein assessment und im anschluss daran ein interventionsprogramm durchlaufen hatten , zum zeitpunkt der entlassung weniger fremde hilfe beanspruchen mussten als diejenigen patienten , welche eine standardversorgung ohne assessment und interventionen erhalten hatten [ 35 ]  . 
grabenbauer diacura coburg strahlentherapie und radioonkologie klinikum coburg ketschendorfer strae 33 96450 coburg telefon ( + 49 / 9562 ) 2491 - 0 , fax - 50 e - mail : gg@diacura.de strahlenther onkol 2010 strahlentherapie und onkologie case study aplastic anemia as a cause of death in a patient with glioblastoma multiforme treated with temozolomide jindrich kopeck1 , peter priester1 , ladislav slovcek1 , jir petera1 , otakar kopeck2 , zuzana macingova1 background : standard treatment of glioblastoma multiforme consists of postoperative radiochemotherapy with temozolomide , followed by a 6 - month chemotherapy . 
serious hematologic complications are rarely reported . case report and results : the authors present the case of a 61 - year - old female patient with glioblastoma multiforme treated with external - beam radiation therapy and concomitant temozolomide . 
after completion of treatment , the patient developed symptoms of serious aplastic anemia that eventually led to death due to prolonged neutroand thrombocytopenia followed by infectious complications . conclusion : lethal complications following temozolomide are , per se , extremely rare , however , a total of four other cases of aplastic anemia have been reported in the literature so far . key words : glioblastoma multiforme temozolomide aplastic anemia strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2132 - 3 aplastische anmia als todesursache bei einer patientin mit glioblastoma multiforme nach temozolomidbehandlung hintergrund : die standardbehandlung des glioblastoma multiforme ist die postoperative radiochemotherapie mit temozolomid , gefolgt von einer 6 - monatigen erhaltungschemotherapie . 
schwerwiegende hmatologische toxizitten werden selten berichtet . fallbericht und ergebnisse : die autoren prsentieren den fall einer 61 - jhrigen patientin mit glioblastoma multiforme , die mit externer strahlentherapie und begleitender temozolomidchemotherapie in standarddosierung behandelt wurde . 
nach abschluss der behandlung zeigte die patientin symptome einer schweren aplastischen anmie , die infolge prolongierter neutround thrombopenie durch infektise komplikationen zum tode fhrte . schlussfolgerung : letale komplikationen einer temozolomidchemotherapie sind selten , bislang wurden insgesamt vier flle einer aplastischen anmie in der literatur berichtet . schlsselwrter : glioblastoma multiforme temozolomid aplastische anmie introduction glioblastoma multiforme is the most malignant and the most common primary brain tumor in adults . 
symptoms , which are caused by glioblastoma multiforme , can be divided into general and specific ones due to each tumor type or due to the tumor location and size [ 7 ]  . 
the basic life functions are at risk , if the primary tumor location is in the brain steswallowing disorders and dysarthria are caused , if the tumor interferes with cranial nerves . 
unilateral blindness and misunderstanding 1department of clinical oncology and radiotherapy , charles university hospital and faculty of medicine in hradec kralove , czech republic , 2clinical oncology , regional hospital nchod , czech republic . received : february 10 , 2010 ; accepted : march 26 , 2010 published online : july 29 , 2010 strahlenther onkol 2010 urban & vogel temozolomide was subsequently stopped and treatment was continued with external - beam radiotherapy . 
 the length of patients survival with glioblastoma multiforme is dependent on many independent factors age , neurological status , cognitive functions , the type of tumor , its size and location [ 2 , 3 , 8 , 13 ]  . the treatment of glioblastoma multiforme is multimodal , i.e. , neurosurgical resection , external - beam radiotherapy , systemic chemotherapy , or their combination . 
this team should then determine the way of cancer therapy in order to ensure the highest possible quality of care and life for the patient . case report a 61 - year - old female patient with a history of arterial hypertension and open - angle glaucoma in the right eye was referred from the department of neurosurgery to the comprehensive cancer center on october 16 , 2009 . 
the patient was in a good performance status ( ecog 1 ) with reduced psychomotor tempo and without neurological deficit . after 2 weeks from the stereotactic biopsy , the patient was admitted to the comprehensive cancer center to begin a radical external - beam radiotherapy with a 25 - mm margin at a dose of 50 gy in 25 fractions and a boost to the tumor with a 15 - mm margin at a dose of 10 gy in five fractions . 
during the first days of radiotherapy , it was decided with regard to the patients good performance status ( ecog 1 ) to start a concomitant chemotherapy with temozolomide at a dose of 75 mg / m2 / day with prophylactic administration of cotrimoxazole . 
manifestationen einer hmorrhagischen diathese bei einem rckgang der thrombozytenzahl auf 4 109 / l ( aphthse ulzeration mit blutung an der unterlippe ; foto : autoren )  . strahlenther onkol 2010 kopeck j , et al . 
aplastic anemia and temozolomide on december 7 , 2009 , the full blood count control demonstrated a significant thrombocytopenia ( 11 109 / l ) with hemorrhagic diathesis signs of multiple petechiae on the legs and trunk and leukopenia ( 2.2 109 / l ) , with the absolute count of granulocytes > 500 . 
on december 11 , 2009 , severe leukopenia was revealed ( blood count 0.34 109 / l , absolute number of granulocytes < 500 ) , platelet count was > 20 109 / l , and there were no signs of fresh hemorrhagic diathesis , the patient remained afebrile . 
during the whole hospitalization , a short febrile peak without proof of any microbial agent occurred only once.high - resolution pulmonary ct demonstrated homogeneous infiltrates in the upper and lower lobes of the right lung with a pneumonic character . 
a stepwise change in antibiotic medication was made from ciprofloxacin over cefotaxime and then to meropenem , vancomycin and amikac she was put on cotrimoxazole ( pneumocystis jiroveci prophylaxis ) and acyclovir . 
the values and dynamics of white blood cells , red blood cells and platelets during hospitalization are shown in figures 3 to 5 . due to the prolonged depression of hematopoiesis after chemotherapy with temozolomide and insufficient 3 - week leukopoiesis stimulation , the patient underwent sternal puncture and subsequent trepanobiopsy of bone marrow from the iliac crest . 
immunophenotyping flow cytometry of peripheral blood was also performed , which showed an increase in lymphoid cell number , an abnormally increased population of b lymphocytes , and depletion of natural killer cells . 
by request of the patient and her family , she was discharged from hospital on january 4 , 2010 , and followed up by palliative ambulatory care of the comprehensive cancer center . 
the current standard in the adjuvant treatment for glioblastoma multiforme is external - beam radiotherapy with 60 gy in 30 fractions with concurrent chemotherapy with temozolomide at a dose of 75 mg / m2 / day orally [ 6 , 9 , 12 ]  . 
according to the fda ( food and drug administration ) , temozolomide is used to treat ( 1 ) adult patients with a newly diagnosed glioblastoma multiforme concurrently with radiotherapy and then as a maintenance treatment , ( 2 ) adolescents and adult patients with refractory anaplastic astrocytoma . 
concomitant administration of temozolomide enhances the effect of external - beam radiotherapy [ 14 ] , and the administration of temozolomide at the dose of 75 mg / m2 is considered to be safe . 
however , temozolomide is also known to have side effects , the most common being nausea , vomiting , constipation , anorexia , alopecia , headache , fatigue , seizures , rash , neutropenia , lymphopenia , and thrombocytopenia . 
 neutropenia is seen in 8% of patients , and the incidence of leukopenia in patients treated with temozolomide has been described to be up to 11% [ 5 , 10 , 12 ]  . 
despite maximum intensive supportive therapy ( 3 - week stimulation of leukopoiesis ) of aplastic anemia , deterioration of hematopoiesis was irreversible , which also resulted in death from sepsis . 
often , there are several factors such as concomitant prophylactic administration of cotrimoxazole , anticonvulsants or h2 blockers , which can cause thrombocytopenia . conclusion our case report points to the need for regular monitoring of full blood count in patients with glioblastoma multiforme treated with temozolomide in order to adequately react to the possible danger of fatal hematologic toxicity . 
cancer chemother pharmacol 2009 ; 64 : 64755 . strahlentherapie und onkologie original article radiobiological comparison of hypofractionated accelerated partial - breast irradiation ( apbi ) and single - dose intraoperative radiotherapy ( iort ) with 50 - kv x - rays carsten herskind , frederik wenz1 background and purpose : intraoperative radiotherapy ( iort ) of the tumor bed in early breast cancer is presently performed with a single dose of 50 - kv x - rays from a miniaturized x - ray machine using spherical applicators . 
the purpose was to model the biological effect of hypofractionated accelerated partial - breast irradiation ( apbi ) with ten fractions . material and methods : the relative biologic effectiveness ( rbe ) was estimated from the linear - quadratic ( l - q ) formalism including repair of sublethal damage or assuming a constant rbe = 1.21.5. 
in accordance with clinical convention , the dose for apbi was prescribed at 1 cm depth in the tumor bed , whereas for iort it was prescribed at the applicator surface . results : the fraction size was fitted to give the same risk of late normal - tissue reaction ( fibrosis ) as single - dose iort with a maximum dose of 20 gy . 
the sphere of equivalence within which the risk for local recurrence is the same for whole - breast radiotherapy was predicted to extend to 1115 mm distance from the applicator for / = 10 gy and 913 mm for / = 4 gy for hypofractionated apbi , representing an increase of the sphere of equivalence by 2.56 mm relative to single - dose iort . conclusion : an increase of the therapeutic window with hypofractionated apbi relative to single - dose iort should be feasible . key words : breast radiotherapy fractionation apbi modeling strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2147 - 9 strahlenbiologischer vergleich hypofraktionierter , akzelerierter teilbrustbestrahlung ( apbi ) und einzeitiger intraoperativer radiotherapie ( iort ) mit 50 - kv - rntgenstrahlen hintergrund und ziel : die intraoperative radiotherapie ( iort ) des tumorbetts bei frhen mammatumoren mit 50 - kv - rntgenstrahlen von einem miniaturisierten rntgengert wird derzeit als einzeitbestrahlung mit sphrischen applikatoren durchgefhrt . 
 das ziel war , die biologische wirkung einer hypofraktionierten , akzelerierten teilbrustbestrahlung ( apbi ) mit zehn fraktionen zu modellieren . material und methodik : die relative biologische wirksamkeit ( rbe ) wurde mit dem linear - quadratischen formalismus einschlielich reparatur subletaler schden veranschlagt , alternativ wurde ein konstanter wert von rbe = 1 , 21 , 5 angenommen . 
die dosis fr apbi wurde anhand der klinischen verschreibungskonventionen in 1 cm tiefe des tumorbetts festgelegt , whrend die dosis fr iort an der oberflche verschrieben wurde . ergebnisse : die fraktionsgre wurde angepasst , bis das gleiche risiko spter normalgewebsreaktion ( fibrose ) wie nach einzeit - iort mit einer maximalen dosis von 20 gy erreicht wurde ( abbildung 2 )  . 
die isoeffektive fraktionsgre in 1 cm tiefe war 1 , 01 gy , wenn rbe mit dem linear - quadratischen modell bestimmt wurde , und 1 , 64 gy fr konstante rbe ( tabelle 1 )  . 
die quivalenzkugel , innerhalb welcher das rezidivrisiko gleich gro wie bei ganzbrustbestrahlung ist , erstreckte sich bis 1115 mm abstand von der applikatoroberflche fr / = 10 gy und bis 913 mm fr / = 4 gy ( abbildung 4 )  . 
dies entspricht einer vergrerung um 2 , 56 mm im vergleich zur einzeit - iort . 1department of radiation oncology , university medical center mannheim , germany . received : march 18 , 2010 ; accepted : march 18 , 2010 published online : july 29 , 2010 strahlenther onkol 2010 urban & vogel herskind c , wenz f . 
hypofractionated apbi with 50 - kv x - rays schlussfolgerung : eine vergrerung des therapeutischen fensters durch hypofraktionierte apbi gegenber einzeit - iort sollte mglich se schlsselwrter : teilbrustbestrahlung strahlentherapie fraktionierung modellierung introduction interest in accelerated partial breast radiotherapy ( apbi ) is rising rapidly worldwide [ 18 , 20 , 22 , 24 , 27 , 33 , 34 , 38 ]  . 
although the rationale varies between different studies [ 16 ] , it is generally assumed that recurrences after breast - conserving surgery occur near the site of a tumor and that part of the patients may not need adjuvant radiotherapy to the whole breast [ 6 , 15 ]  . apbi may be applied by interstitial brachytherapy , brachytherapy applicators , and intensity - modulated external - beam radiotherapy [ 19 , 21 , 25 , 32 , 36 ]  . 
furthermore , intraoperative radiotherapy ( iort ) with high - energy electrons or low - energy x - rays is used either as a boost in combination with postoperative wbrt [ 13 , 23 , 28 , 35 ] or as sole treatment [ 11 , 13 , 17 , 27 , 29 , 31 ]  . isotropic 50 - kv x - rays from the intrabeam machine are presently applied as single - dose iort to the tumor bed . 
the rbe is influenced by the radiation quality , the dose per fraction , and the effect of sublethal damage ( sld ) repair during irradiation . an international , multicentric phase iii trial , targit ( targeted intraoperative radiotherapy ) , is testing a risk - adapted approach to iort with intrabeam in highly selected patients [ 29 ]  . 
previous modeling of the risk of late normal - tissue reaction estimated radiation - induced fibrosis to be limited to a few millimeters distance from the applicator [ 8 ]  . 
 modeling the risk of local recurrence suggested the existence of a sphere of equivalence within which the integrated risk after iort would be identical to that after whole - breast radiotherapy ( wbrt ) [ 7 ]  . 
quantitative calculation indicated that the sphere of equivalence may be close to 1 cm of tumor bed tissue targeted by iort . fractionation can increase the therapeutic window between local tumor control and late normal - tissue reaction . 
 the purpose of the present study was to model the risk of recurrence for hypofractionated apbi and single - dose iort at isoeffective doses for late reaction . material and methods radiation source and dose distribution doses of 50 - kv x - rays from the intrabeam prs400 miniaturized x - ray machine ( carl zeiss surgical gmbh , oberkochen , germany ) with spherical applicators for tumor bed irradiation were determined as function of distance from the source [ 8 ]  . modeling of rbe the rbe was estimated by the linear - quadratic ( l - q ) formalism including the effect of continuous induction and decay of sld during protracted irradiation [ 4 , 8 ]  . 
for late reaction of normal tissue , the ratio of the linear and quadratic coefficients ( and , respectively ) was assumed to be / = 3 gy , whereas for local tumor control , values of 10 gy and 4 gy were applied as indicated . 
the ratio of the linear coefficients , ref for reference radiation ( high - energy x - rays ) , was assumed to be 50kv / ref = 3 , and the repair half - time of sld t1 / 2 = 15 min as previously described [ 7 , 8 ]  . 
the total dose , 10 dref , was converted to the isoeffective total dose , dref , for the appropriate fractionation scheme using the l - q model for fractionation [ 12 ]  . dose - response relationships the biological effect ( risk of late reaction or local recurrence ) was estimated from clinical dose - response data . 
conversion to other fractionation schemes was done using / = 3 gy for late reaction [ 14 ] , which was within the confidence interval of a detailed analysis including 22 fractions [ 3 ]  . 
hypofractionated apbi with 50 - kv x - rays pression that ed50 may be slightly lower in humans than in the pig model [ 8 , 9 ]  . the risk of pneumonitis was determined by converting the total dose to the isoeffective single dose and using dose - response relationship for single - dose irradiation of human patients ( ed50 = 9.3 gy ) [ 8 , 30 ]  . a dose - response relationship for control of local recurrence was previously derived from clinical radiotherapy with daily fractions of 2 gy given five times per week with a modification to account for the effect of absent repopulation of tumor cells between surgery and iort [ 7 ]  . results previous modeling for single - dose iort [ 8 ] estimated 50% risk of fibrosis at a distance of approximately 2.8 mm from the surface of a 4.5 - cm applicator when rbe was calculated by the l - q formalism including sld repair , and at approximately 6.2 mm for constant rbe = 1.5. 
isoeffective fraction size , d , at 1.0 cm distance from the applicator surface for accelerated partial - breast irradiation ( apbi ) with ten fractions of 50 - kv x - rays from intrabeathe fraction size was determined by radiobiological modeling to be isoeffective with single dose intraoperative radiotherapy ( 20 gy at the applicator surface ) for radial extent of fibrosis . 
isoeffektive fraktionsgre , d , in 1 , 0 cm abstand von der applikatoroberflche fr akzelerierte teilbrustbestrahlung ( apbi ) mit zehn fraktionen intrabeam - 50 - kv - rntgenstrahlen . 
die fraktionsgre wurde durch strahlenbiologische modellierung so bestimmt , dass fibrose nach apbi das gleiche radiale ausma wie nach einzeitiort ( intraoperative radiotherapie ) mit 20 gy an der applikatoroberflche haben sollte . 
the dose was varied until the distance from the applicator at which 50% risk is reached fitted the curve for single - dose iort . table 1 shows the isoeffective dose per fraction , d50kv , for each applicator . 
the isoeffective dose was 711% lower for a 4.0 - cm applicator diameter and 37% higher for 5.0 cm compared with 4.5 cthus the isoeffective dose per fraction is determined mainly by the assumptions regarding rbe , whereas the effect of applicator size on the radial extent of fibrosis will be small . 
the radial distribution of fibrosis was calculated for all three applicator sizes ( 4.05.0 cm diameter ) using the fraction sizes determined for the intermediate diameter , 4.5 cm ( figures 2a and 2b )  . 
the distribution of risk of pneumonitis for the two dose fractions ( figures 2c and 2d ) estimated ed50 to be limited to 911 mm distance from the applicator . strahlenther onkol 2010 herskind c , wenz f . 
pneumonitis ( c , d ) nach zehn fraktionen der fraktionsgre d50kv in 1 , 0 cm abstand der oberflche von applikatoren mit 4 , 05 , 0 cm diameter . 
1 , 5 ( b , d )  . doses at the applicator surface can vary in the range of 3.05.7 gy / fraction , depending on d50kv and applicator size ( figures 3a and 3b )  . 
owing to the dose - squared law for isotropic radiation sources , the slope of the normalized dose versus distance from the applicator surface decreases with increasing radius of the applicator [ 8 ]  . 
for dose prescription with apbi at 1 cm distance , the physical dose of 50 - kv x - rays will increase with decreasing applicator size at distances closer to the applicator ( figures 3a and 3b )  . 
since the applicator size is predicted to have little influence on rbe for apbi ( figure 3c ) , the equivalent fraction size of reference radiation , dref = rbe d50kv , should increase with decreasing applicator size . 
therefore , the radial extent of fibrosis was predicted to increase with decreasing applicator diameter , while the radial extent of pneumonitis ( close to the prescription point at 1 cm ) will be essentially independent of the applicator size . 
 dose prescription at the applicator surface in the targit protocol for single - dose iort implies that the dose at a given distance from the applicator increases with increasing applicator diameter ( figure 3d )  . 
however , since rbe modeled by the l - q formalism including sld repair decreases with increasing applicator diameter ( figure 3c ) , the two opposing effects essentially cancel each other rendering the extent of fibrosis nearly independent of the applicator diameter . 
 for constant rbe , on the other hand , the equivalent dose of reference radiation will be proportional to physical dose and thus the radial extent of fibrosis should increase with applicator size [ 8 ]  . strahlenther onkol 2010 herskind c , wenz f . 
rbe for normal tissue reaction ( / = 3 gy ) was modeled by the l - q formalism including repair increases with increasing distance ( decreasing dose per fraction ) and shorter irradiation times ( smaller applicator diameter )  . 
the effect of applicator size was negligible for hypofractionated apbi ( short irradiation time ) , but not for single - dose iort with longer irradiation times ( c )  . 
die dosisverschreibung in 1 cm abstand von der applikatoroberflche fr apbi bedeutet eine zunahme der physikalischen dosis von 50 - kv - rntgenstrahlen mit abnehmender applikatorgre bei abstnden < 1 cd50kv = 1 , 01 gy fr rbe berechnet mit dem linear quadratischen formalismus einschlielich reparatur ( a ) ; d50kv = 1 , 64 gy fr konstante rbe = 1 , 21 , 5 ( b )  . 
bei modellierung mit dem linear - quadratischen formalismus einschlielich reparatur nimmt rbe fr normalgewebsreaktion ( / = 3 gy ) mit zunehmenden abstand ( kleinere dosen ) und krzeren bestrahlungszeiten ( kleineren applikatorgren ) zu . 
die dosisverschreibung an der applikatoroberflche bei einzeit - iort ( dmax = 20 gy ) fhrt zu einer zunahme der dosis mit zunehmender applikatorgre ( d )  . the distribution of risk of recurrence was compared for hypofractionated apbi and single - dose iort at isoeffective doses for late reactions ( figures 4a to 4f )  . 
the size of the sphere of equivalence was influenced by the rbe model and by the / value for local control , but fractionation was predicted to increase its size in all cases . 
hypofractionated apbi with 50 - kv x - rays discussion the present model calculations support that hypofractionated apbi with 50 - kv x - rays from intrabeam might increase local control in the tumor bed without increasing the risk of late fibrotic reaction , thus potentially increasing the therapeutic window . 50kv / radiobiological modeling involves a number of assumptions and estimates of model parameters . 
in the l - q formalref for d 0 and thus the assumption reism , rbe garding the numeric value of this ratio becomes increasingly important , as the dose per fraction is reduced . 
furthermore , the time to deliver each dose fraction is shorter than for iort , so the effect of sld repair during protracted irradiation is considerably smaller than for single - dose irradiation . 
both factors contribute to increasing the estimated rbe demonstrated by values in the range of 1.52 for small dose fractions compared with 0.91.3 for single - dose iort within the first 10 mm distance from the applicator surface . 
this follows from the fact that the physical dose yielding a given equivalent dose of reference radiation ( e.g. , resulting in 50% risk ) is inversely proportional to rbe ( because dref = rbe d50kv )  . 
however , the isoeffective dose per fraction was the same for the two values , because rbe influenced the spatial extent of fibrosis after single - dose iort similarly . because of the different reference points for dose prescription , the dependence of the extent of fibrosis on applicator size was reversed for apbi compared with iort . 
 however , the difference in isoeffective dose for different applicator sizes was modest and caused only a small variation of the extent of fibrosis , which did not justify using different prescribed doses for different applicator sizes . 
thus the thickness of the chest wall should shield the lung tissue against the risk of pneumonitis after hypofractionated irradiation as already found for single - dose iort . as expected , the size of tumor bed volume within the sphere of equivalence for recurrence was increased by fractionation compared with single - dose iort by a factor of 1.32.5. 
usually , a value of / = 10 gy is assumed for most tumor cells in vivo and in vitro [ 12 , 26 , 37 ] , but recent hypofractionation trials yielding / = 4.6 gy ( confidence interval 1.18.1 ) adjusted for known prognostic factors [ 1 ] , strongly suggested that values of / may be lower than 10 gy . delays between surgery and the start of radiotherapy significantly influence local control , implicating that proliferation of residual tumor cells in this time interval plays an important role [ 5 , 10 ]  . 
therefore , an important prerequisite for transferring the present model calculations into the clinical situation is that the time interval between surgery and apbi is kept short . conclusion hypofractionated apbi with intrabeam should be able to increase the therapeutic window between tumor control and late normal - tissue reaction . 
because of the increased dose per fraction at the applicator surface , the isoeffective dose per fraction in the range of 1.01.6 gy should be used only as a first estimate for a phase i / ii study to determine safe doses . 
close long - term monitoring of late reaction and local control is mandatory . acknowledgment carl zeiss surgical gmbh , oberkochen , germany , supports radiobiological research at the university medical center mannheim . strahlentherapie und onkologie originalarbeit der stellenwert der strahlentherapie bei symptomatischen wirbelkrperhmangiomen ( swkh ) * reinhard heyd1 , m . 
eich5 , frank bruns6 , georg gosheger7 , normann willich8 , oliver micke9 , fr die german cooperative group on radiotherapy for benign diseases ( gcg - bd ) ziel : analyse der effektivitt der radiotherapie ( rt ) zur behandlung symptomatischer wirbelkrperhmangiome ( swkh )  . material und methodik : basierend auf dem register fr seltene gutartige erkrankungen der german cooperative group on radiation therapy for benign diseases ( gcg - bd ) wurden die klinischen angaben , behandlungstechniken und ergebnisse aus sieben zentren retrospektiv analysiert . ergebnisse : ber eine zeitspanne von 39 jahren ( 19692008 ) wurden 84 patienten mit insgesamt 96 symptomatischen lsionen bestrahlt . 
nach einem medianen nachbeobachtungszeitraum von 68 monaten ( 6422 monate ) hatten 61 , 9% eine komplette ( cr ) , 28 , 6% eine partielle ( pr ) und 9 , 5% keine symptomregression ( nr )  . 
nach median 70 monaten ( 8124 monate ) entwickelten acht patienten ( 9 , 5% ) ein rezidiv der klinischen beschwerden , so dass die langfristige kontrollrate 80 , 9% betrug . 
 nebenwirkungen > rtog / eortc - grad 2 traten bei keinem der behandelten flle auf . schlussfolgerung : die strahlentherapie ist eine nebenwirkungsarme und effektive therapieoption fr die behandlung von swkh . 
 gesamtdosen von mindestens 34 gy sind erforderlich , um ein optimales ansprechen zu erzielen . schlsselwrter : hmangiome wirbelkrperhmangiome strahlentherapie gutartige erkrankungen strahlenther onkol 2010 doi 10.1007 / s00066 - 010 - 2140 - 3 the significance of radiation therapy for symptomatic vertebral hemangiomas ( svh ) purpose : to evaluate the efficacy of radiation therapy ( rt ) for symptomatic vertebral hemangioma ( svh )  . material and methods : based on the registry for rare benign disorders ( rrbd ) of the german cooperative group on radiation therapy for benign diseases ( gcg - bd ) , the clinical information , treatment plans and outcome data from seven cooperating german rt institutions were analyzed retrospectively . results : over a period of 39 years ( 19692008 ) , a total of 84 patients with 96 symptomatic lesions underwent rt . 
after a median follow - up of 68 months ( 6422 months ) , complete symptom relief ( cr ) occurred in 61.9% of patients , 28.6% had partial relief , and 9.5% had no relief ( nr )  . 
total doses of at least 34 gy are recommended to achieve optimal treatment response . key words : hemangiomas vertebral hemangiomas radiotherapy benign disease einleitung hmangiome sind benigne neubildungen , die sich von den gefauskleidenden endothelien ableiten und ubiquitr im krper auftreten knnen [ 6 , 9 ]  . 
der histologische aspekt ist dominiert von dnnwandigen , ektatischen gefen mit einer rarefizierung elastischer fasern , die thrombotisches material sowie hmosiderin enthalten und in kompensatorisch hypertrophierte knochenblkchen und fettgewebe eingebettet sind [ 9 , 22 , 30 ]  . 
dies fhrt zu einem charakteristischen rntgenmorphologischen erscheinungsbild ( abbildung 1 )  . bevorzugte lokalisationen der knochenhmangiome sind die schdelkalotte , der krperstamm und die metaphysen der langen rhrenknochen , wobei etwa 28% auf das achsenskelett entfallen . 
wirbelkrperhmangiome ( wkh ) sind zumeist in der brustund oberen lendenwirbelsule lokalisiert , das befallsmuster ist berwiegend singulr und auf den wirbelkrper begrenzt [ 12 , 21 , 28 ]  . 
autoptische und radiologische reihenuntersuchungen wiesen eine inzidenz von 1012% nach [ 1 , 15 , 22 , 30 ] , jedoch entwickeln nur etwa 0 , 91 , 2% der patienten behandlungspflichtige symptome [ 15 , 19 , 28 ]  . 
mgliche morphologische ursachen dafr sind eine epiund intraspinale expansion , seltener pathologische frakturen , extradurale blutungen oder ischmie des myelons [ 1 , 12 , 16 , 26 ] ( abbildung 2 )  . die konservativen therapieoptionen , die zur behandlung symptomatischer wirbelkrperhmangiome ( swkh ) eingesetzt werden , schlieen abgesehen von der radiotherapie ( rt ) [ 3 , 6 , 14 , 20 , 21 , 29 , 32 ] perkutane vertebroplastien [ 1 , 7 , 15 ] , transarterielle embolisationen [ 1 , 16 ] oder intralsionale alkoholinjektionen [ 8 ] ein , die allein oder in verschiedenen kombinationen angewendet werden . 
durch einfache laminektomien oder vertebrektomien mit wirbelkrper ersatz , angezeigt , denen zur minimierung des intraoperativen blutungsrisikos eine embolisation vorgeschaltet wird [ 1 , 12 , 16 , 19 , 28 ]  . die vorliegende untersuchung fasst die behandlungsergebnisse aus sieben zentren zusammen , die in das 2002 initiierte register fr seltene gutartige erkrankungen ( registry for rare benign diseases [ rrbd ] ) der german cooperative group on radiotherapy for benign diseases ( gcg - bd ) eingebracht wurden . ziel der untersuchung ist es , anhand eines aussage fhigen patientenkollektivs daten zur effektivitt der strahlentherapie und optimierung der dosisregime zu erarbeiten . material und methodik basierend auf dem rrbd wurden retrospektiv systematisch die einzeldaten aller patienten aus dem zeitraum von 1969 bis 2008 einbezogen . 
dabei wurden neben den stammdaten der patienten die informationen ber anzahl und art der vorbehandlungen , die bestrahlungstechnik und gewhlten zielvolumina , die dosisregime der bestrahlung sowie die behandlungsergebnisse erfasst . 
eine bersicht ber die kooperierenden zentren und eingebrachten flle gibt tabelle 1 . primrer endpunkt der untersuchung war die schmerzrckbildung , die anhand eines standardisierten schemas der gcg - bd evaluiert wurde : cr = komplette schmerzrckbildung , pr = partielle schmerzrckbildung , nr = keine schmerzremission . 
sekundre endpunkte der untersuchung umfassten die remission neurologischer defizite und die remineralisation der bestrahlten lsionen . zur evaluierung mglicher prognoseparameter wurde eine multivariate regressionsanalyse durchgefhrt , das signifikanzniveau lag bei p < 0 , 05 . 
review of the cooperating centers . zentrum universittsklinikum dresden universittsklinikum mnster universittsklinikum hamburg - eppendorf medizinische hochschule hannover alfried - krupp - krankenhaus essen universittsklinikum kln klinikum offenbach patienten ( n ) ergebnisse nach einem medianen nachbeobachtungszeitraum von 68 monaten ( spannbreite : 6422 monate ) waren insgesamt 96 lsionen bei 84 patienten auswertbar , deren medianes alter bei 48 jahren lag ( spannbreite : 1279 jahre )  . 
57 patienten ( 67 , 9% ) waren weiblichen , 27 ( 32 , 1% ) mnnlichen geschlechts , die ratio frauen / mnner betrug somit 2 , 2 : 1 . die diagnosesicherung erfolgte neben dem klinischen untersuchungsbefund anhand von computertomographien ( ct ) oder magnetresonanztomographien ( mrt ) , bei 18 patienten ( 21 , 4% ) war eine biopsie zur histologischen absicherung durchgefhrt worden . 
fhrendes klinisches symptom waren lokale schmerzen ( 82 patienten , 97 , 6% ) ; 24 patienten ( 28 , 6% ) hatten bei einengung des spinalkanals oder der neuroforamina neurologische defizite . 
vor einleitung der bestrahlung waren 20 patienten ( 23 , 8% ) einer operativen intervention unterzogen worden , sechs patienten ( 7 , 1% ) waren mit einer embolisation und fnf ( 5 , 9% ) mit einer vertebroplastie vorbehandelt . die bestrahlung war bei 42 patienten ( 50 , 0% ) an einem linearbeschleuniger , bei 34 patienten ( 40 , 5% ) an einem telecobaltgert und bei acht patienten ( 9 , 5% ) an einem orthovoltgert durchgefhrt worden . 
die mediane gesamtdosis lag bei 34 gy ( 4 , 545 gy ) , die mediane einzeldosis bei 2 , 0 gy ( 0 , 53 , 0 gy )  . zum zeitpunkt der nachuntersuchungen hatten 52 patienten ( 61 , 9% ) eine komplette ( cr ) , 24 ( 28 , 6% ) eine partielle ( pr ) und acht patienten ( 9 , 5% ) keine schmerzremission ( nr )  . 
in der gruppe der patienten mit einer operativen vorbehandlung wurde bei zwlf patienten ( 60 , 0% ) eine komplette ( cr ) , bei sechs patienten ( 30 , 0% ) eine partielle ( pr ) und bei zwei patienten ( 10 , 0% ) keine schmerzremission ( nr ) erzielt . 
im vergleich wurde in dem teilkollektiv mit primrer rt ( n = 53 ) bei 33 patienten ( 62 , 3% ) eine komplette , bei 18 ( 33 , 9% ) eine partielle und bei zwei patienten ( 3 , 8% ) keine remission erreicht . 
der vergleich der gruppen mit einer vorbehandlung ( n = 31 ) und mit primrer rt ( n = 53 ) mittels des 2 - tests zeigte hinsichtlich der symptomregression keinen signifikanten unterschied . radiologische zeichen einer remineralisation fanden sich bei 22 patienten ( 26 , 2% )  . 
eine komplette rckbildung neurologischer defizite stellte sich bei 19 von 24 patienten ( 79 , 2% ) ein , fnf patienten ( 20 , 8% ) hatten eine partielle rckbildung . 
 im rahmen der langfristigen nachbeobachtung trat nach median 70 monaten ( spannbreite : 8124 monate ) bei acht patienten ( 9 , 5% ) eine symptomprogression auf , so dass langfristig bei 68 patienten ( 80 , 9% ) eine symptomkontrolle erreicht wurde . 
clinical staging system for vertebral hemangiomas . gruppe kriterien keine symptome lokale symptome ohne beteiligung des spinalkanals lokale symptome mit beteiligung des spinalkanals ohne querschnittssyndrom beteiligung des spinalkanals mit querschnittssyndrom fr gesamtdosen 34 gy eine signifikant bessere schmerzremission und geringere rezidivrate . nebenwirkungen > rtog / eortc - grad 2 wurden nicht beobachtet . 
hinsichtlich der sptreaktionen traten bei zwei patienten ( 2 , 4% ) knochennekrosen auf , drei patienten ( 3 , 6% ) zeigten eine geringe fibrose der haut oder des subkutanen bindegewebes im bereich der strahleneintrittsfelder . diskussion hmangiome sind hamartome , deren grenzunahme definitionsgem nicht durch eine mitotische aktivitt , sondern durch eine expansion bedingt ist . 
demzufolge wird als vorrangiger mechanismus der rt eine obliteration abnormaler , zufhrender gefe diskutiert , wobei die endothelzellen dieser gefe als zielstruktur angesehen werden [ 6 , 14 , 19 ]  . 
wenngleich die genauen mechanismen der rt nach wie vor nicht geklrt sind , knnen hmangiome dennoch durch eine strahlentherapie hnlich erfolgreich behandelt werden wie zahlreiche andere entitten nichtmaligner erkrankungen [ 2 , 4 , 10 , 17 , 18 , 23 , 27 , 31 ] , was seit dem ersten bericht von bailey & bucy 1929 [ 3 ] im schrifttum belegt ist . eine literaturbersicht ber 64 publikationen aus der zeitspanne von 1929 bis 2007 unter einschluss von 347 fllen zeigte , dass durch den einsatz der rt bei 57 , 6% eine komplette und bei 27 , 7% eine partielle symptomregression erzielt wurde , whrend 14 , 7% der flle keinen behandlungsvorteil aufwiesen ( ansprechrate 85 , 3% ) [ 20 ]  . 
diese ergebnisse konnten in der vorliegenden untersuchung mit einer ansprechrate von 80 , 9% ( cr = 61 , 9% , pr = 28 , 6% , nr = 9 , 5% ) besttigt werden . uneinigkeit besteht auch in bezug auf das optimale dosiskonzept der rt , was die spannbreite der eingesetzten gesamtdosen in der vorliegenden untersuchung ( 4 , 545 gy ) besttigt . 
der stellenwert der radiochirurgie ist aufgrund zu geringer fallzahlen gegenwrtig noch unklar [ 13 ]  . fr die therapieentscheidung bei swkh hat sich eine klinische stadieneinteilung bewhrt ( tabelle 3 ) [ 19 , 21 ]  . 
so zeigte eine analyse der franzsischen gesellschaft fr neurochirurgie , dass nach alleiniger operation in bis zu 30% der flle mit einem nachbeobachtungszeitraum 3 jahre nach durchschnittlich 1 , 5 jahren , und davon etwa bei 90% binnen der ersten 2 jahre , ein lokalrezidiv auftrat [ 24 ]  . 
 [ 1 ] empfiehlt eine restriktivere indikationsstellung der rt ( abbildung 3 ) und sieht diese bei umschriebenen befunden , die isoliert vordere oder hintere anteile des wirbelkrpers betreffen , nur bei auftreten rezidivierender schmerzen oder bei nichtresektablem restgewebe konturberschreitender lsionen . 
die systematische erfassung des nebenwirkungsspektrums in der vorliegenden untersuchung zeigte , dass die akuttoxizitt vernachlssigbar war und < 5% der patienten hatten relevante sptreaktionen rtog / eortc - grad 2 hatten . zweitmalignome nach bestrahlung von knochenhmangiomen sind bislang nur fr repetitive telecobaltbestrahlungen beschrieben , wobei in zwei bestrahlungsserien kumulative gesamtdosen von 5580 gy appliziert wurden [ 11 , 25 ]  . 
untersuchten anhand von phantommessungen mittels thermolumineszenzdetektoren ( tld100 ) das risiko einer tumorinduktion und fanden einen relativen risikofaktor von 0 , 6 fr eine einzelfeldbestrahlung und von 0 , 9 fr die bestrahlung mittels zweier schrger felder [ 5 ]  . 
nach einem medianen nachbeobachtungszeitraum von 14 , 3 jahren ( spannbreite : 626 jahre ) sahen sie in einem kollektiv von 29 patienten keine radiogene zweitneoplasie , was in einklang mit den ergebnissen der eigenen untersuchung steht . somit sind die aktuellen dosisempfehlungen zwar mit dem potentiellen risiko einer tumorinduktion behaftet , jedoch ist fr diese gegenwrtig kein fall in der literatur beschrieben . schlussfolgerung die rt ist eine effektive therapieoption mit gnstigem nebenwirkungsprofil fr die behandlung von swkh . 
strahlenther onkol 1996 ; 172 : 6814 . korrespondenzanschrift reinhard heyd strahlenklinik klinikum offenbach starkenburgring 66 63069 offenbach am main telefon ( + 49 / 69 ) 8405 - 3335 , fax - 3334 e - mail : reiniheyd@aol.com strahlenther onkol 2010 strahlentherapie und onkologie original article total body irradiation ( tbi ) in pediatric patients a single - center experience after 30 years of low - dose rate irradiation claudia linsenmeier1 , daniel thoennessen1 , laura negretti1 , jean - pierre bourquin2 , tino streller1 , urs martin ltolf1 , susanne oertel1 , 3 purpose : to retrospectively analyze patient characteristics , treatment , and treatment outcome of pediatric patients with hematologic diseases treated with total body irradiation ( tbi ) between 1978 and 2006 . patients and methods : 32 pediatric patients were referred to the department of radiation - oncology at the university of zurich for tbi . 
a total of 18 patients suffered from acute lymphoblastic leukemia ( all ) , 5 from acute and 2 from chronic myelogenous leukemia , 1 from non - hodgkin lymphoma , and 2 from anaplastic anemia . 
late effects ( rtog 3 ) were pneumonitis in 1 patient , chronic bronchitis in 1 patient , cardiomyopathy in 2 patients , severe cataractogenesis in 1 patient ( 48 months after tbi with 10 gy in a single dose ) and secondary malignancies in 2 patients ( 36 and 190 months after tbi )  . 
in 2 patients with identical twins treated at ages 2 and 7 , a loss of 8% in final height of the treated twin was observed . conclusion : as severe late sequelae after tbi , we observed 2 secondary malignancies in 11 patients who survived in excess of 36 months . 
conditioning for bone marrow transplantation without radiation is an attractive option , but is not sufficiently effective to completely replace tbi for the most common pediatric indications . key words : total body irradiation  . 
low - dose rate irradiation strahlenther onkol 2010 ; 186 : 61420 doi 10.1007 / s00066 - 010 - 2089 - 2 ganzkrperbestrahlung ( tbi ) in der pdiatrie 30 jahre erfahrungen mit niedrig - dosisraten - bestrahlung ziel : retrospektive analyse von patientencharakteristika , behandlung und ergebnis bei kindern mit hmatologischen erkrankungen , die zwischen 1978 und 2006 mit ganzkrperbestrahlung behandelt wurden . patienten und methodik : 32 kinder wurden unserer klinik zur tbi zugewiesen , 28 krankengeschichten waren zugnglich ( n = 28 )  . 
 18 patienten litten unter akuter lymphoblastischer leukmie ( all ) , 5 unter akuter ( aml ) und 2 unter chronisch myeloischer leukmie ( cml ) , einer unter non - hodgkin - lymphom und zwei unter aplastischer anmie . 
acht patienten sind an einem rezidiv verstorben , einer an einer graft - versus - host erkrankung , zwei an sepsis und zwei an sekundrtumoren . resultate : das 5 - jahres gesamtberleben lag bei 60% . 
das gesamtberleben war signifikant ( p = 0.004 ) niedriger bei patienten , die nach einem rezidiv behandelt wurden ( 24% ) , als bei solchen die bei erstdiagnose behandelt wurden ( 74% )  . 
spttoxizitt rtog >= 3 waren eine pneumonitis bei 1 patienten , eine chronische bronchitis bei einem patienten , kardiomyopathie bei 2 patienten , eine katarakt bei einem patienten ( 48 monate nach tbi mit 10gy einzeldosis ) und sekundrtumore bei 2 patienten . 
 1department of radiation - oncology university hospital zurich , switzerland , 2university childrens hospital zurich , department of hemato - oncology , 3department of radiation oncology university of heidelberg , germany . received : january 13 , 2010 ; accepted : july 5 , 2010 published online : november 8 , 2010 strahlenther onkol 2010 no . 
bei zwei eineiigen zwillingen zeigt sich ein verlust von 8% an krpergrsse im vergleich zum zwilling . schlussfolgerung : wie erwartet zeigen sich schwere spttoxizitten nach ganzkrperbestrahlung mit zwei sekundrtumoren bei 11 patienten , die lnger als 36 monate berlebt haben . 
since the first successful bone marrow transplantations in the 1950s , total body irradiation ( tbi ) remained the mainstay of conditioning regimens until the late 1980s in both pediatric and adult patients [ 14 , 22 ]  . 
in the 1980s , dose rates were reduced resulting in a further decrease in late effects , especially cataractogenesis , renal toxicity , and interstitial pneumonitis [ 1 , 7 , 16 ]  . 
nevertheless , severe long - term sequelae , especially the induction of secondary malignancy , hormonal dysregulation , reproductive insufficiency , as well as growth retardation and the development of osteochondromas in pediatric patients remained an issue [ 15 , 21 , 23 , 29 ]  . in the 1990s , a couple of prospective randomized studies were initiated in which tbi was compared to chemotherapyonly regimens , usually based on busulfan and cyclophosphamide . 
 therefore , total body irradiation has remained the cornerstone of conditioning regimens in pediatric hematologic diseases [ 30 ] despite the risk of possible late consequences . the tbi technique differs dramatically between institutions . 
the applied tbi technique and its dosimetry , however , significantly affect the success of bone marrow transplantation ( bmt ) and the rate of complications [ 18 , 22 ]  . we reviewed the records of our pediatric patients treated with tbi at the university hospital of zurich from 19782006 in order to analyze treatment outcome and late sequelae . patients and methods since 1978 , 32 pediatric patients ( referred from the university childrens hospital zurich ) were treated with tbi at our institution . 
at the time of last fu , 15 patients were alive , while 8 had died of a recurrence , 1 of a gvhr , 2 of sepsis , and 2 patients died of secondary malignancy . 
at the time of last fu , 11 patients had survived tbi for more than 36 months . of the patients , 18 suffered from acute lymphoblastic leukemia ( all ) , 5 from acute and 2 from chronic myelogenous leukemia , 1 from non - hodgkin lymphoma , and 2 from anaplastic anemia . 
the other two patients ( n = 2 ) had been treated in the late 1970s and received 10 gy in a single fraction at dose rates of 0.15 gy / min and 0.035 gy / min , respectively , resulting in an overall treatment time of more than 4 hours in the latter patient . the lungs were shielded with individualized partial transmission lung blocks in order to reduce lung doses to < 10 gy . 
five children with all received an additional boost to the testes of 3x2 gy or 11x1.2 gy , 3 of them also received a boost to the brain ( 3x2 gy )  . 
three children had received irradiation to the brain before tbi was indicated . follow - up examinations after tbi were routinely performed in the department of pediatric oncology and included clinical assessment with measurement of height and weight , blood counts ( including differential blood , kidney , and liver parameters ) , hormonal status at least once yearly , chest x - ray , electrocardiogram , and an ophthalmological control in case of strahlenther onkol 2010 no . 
total body irradiation ( tbi ) in pediatric patients age at time of tbi transplantation single dose total dose secondary malignoma recurrence death follow - up ( months ) late effects table 1 . 
 ( fortsetzung ) gender diagnosis relapsed leukemia at time of tbi allogeneic hematopoietic stem cell allogeneic hematopoietic stem cell allogeneic bone marrow ( not related ) allogeneic bone marrow ( not related ) allogeneic hematopoietic stem cell allogeneic bone marrow ( not related ) allogeneic bone marrow allogeneic hematopoietic stem cell allogeneic bone marrow subjective clinical impairment . 
in addition , surviving patients and the parents of 6 patients who had been lost to follow - up were contacted and questioned . the end point selected for the retrospective analysis was overall survival ( os )  . 
differences between groups were assessed by log rank test ( 2 groups ) and x2 test ( more than two groups )  . results the 5 - year os was 60% ( figure 1 ) ; however , overall survival was significantly inferior in patients treated after relapse compared to those treated for newly diagnosed leukemia ( 24% versus 74% p = 0.004 ; figure 2 )  . 
interestingly , survival was better in those patients who had received a matched unrelated bone marrow transplant , compared to those who were administered bone marrow or peripheral stem cells of related donors , with 5 - year os of 88% versus 57% and 33% , respectively . 
this difference ( recurrence ) ( recurrence ) ( sepsis ) 33 34 28 10 19 11 cumulative survival glomerular nephritis cardiomyopathy hypothyreosis elevated liver enzymes optic nerve edema complete censored time ( months ) figure 1 . 
total body irradiation ( tbi ) in pediatric patients cumulative survival overall survival + + + + + + p = 0.004 recurrence censored first - diagnosis complete time ( months ) figure 2 . 
the cumulative incidence of chronic gvhr reached 25% after 5 years . subacute effects observed were a nonfatal pneumonitis in one of the 2 patients treated with a single dose tbi and 2 cases of severe acute parotitis requiring pain medication . 
one patient developed edema of the optic nerves within 2 months after tbi which lead to impaired sight in one eye . late effects ( rtog > 3 ) observed were chronic bronchitis in 1 patient , cardiomyopathy in 2 patients , and severe cataractogenesis requiring surgery in 1 patient ( 48 months after tbi with 10 gy in a single dose )  . 
elevated liver enzymes could be observed in 2 patients with gvhr . two children required hormones for hypothyroidis all girls treated before the onset of puberty demonstrated elevated fsh levels and 1 required hormones to induce puberty . 
there are four prospective randomized studies comparing tbi with chemotherapy - only conditioning regimens : blaise [ 5 ] reported os rates of 75% after cyclophosphamide ( cy ) / tbi conditioning versus 51% after chemotherapy - only ( busulfan ( bu ) / cy ) conditioning in 101 patients treated for aml in first remission . 
ringden [ 24 ] reported for the nordic bone marrow transplantation group a 3 - year survival rate of 76% after conditioning with tbi / cy compared to 62% after conditioning with bu / cy in 167 patients with leukemia ( ~40% aml , 35% cml , 25% all )  . 
seattle [ 10 ] and the french society of bone marrow transplantation [ 13 ] found no difference or clear advantages for either regimen ( cy / tbi versus cy / bu ) in patients with cml and reported a 3 - year os rate of 80% and a 5 - year os rate of about 60% . 
total body irradiation ( tbi ) in pediatric patients a retrospective analysis of 156 patients with all transplanted after either tbi - based or chemotherapy - only conditioning and found a statistically significant improved 6 - year eventfree survival of 43% versus 22% favoring the tbi regimen . 
 despite the well - known late sequelae , tbi - based regimens continue to be widely accepted , especially in all ( above the age of 2 years ) and remain the mainstay in conditioning treatment . side effects and complications of tbi have been extensively studied and yet remain difficult to distinguish from side effects of high - dose chemotherapy . 
in pediatric patients , especially high rates of late sequelae following tbi have been observed in studies with long median follow - up times of over 3 years [ 23 , 29 ]  . 
however , in leukemia patients cataract incidence is also influenced by cortisone medication and was observed in 12% of aml patients treated without tbi [ 28 ]  . interestingly , we detected no clinically or radiologically relevant interstitial pneumonitis ( ip ) in low - dose tbi and only one case of chronic bronchiolitis . 
busulfan is also known to impair lung function and resulted in lower mean vital capacities than fractionated tbi in a retrospective analysis of 80 children after a median follow - up of 4 years [ 9 ]  . 
compared to these data , the incidence of late side effects in our 11 long - term survivors treated with low - dose rate tbi remains low , with only one cataract and two clinically manifest cases of hypothyroidis the cases of cardiomyopathy , interstitial bronchiolitis , and decreased glomerular filtration rates are also possibly attributable to chemotherapy . with respect to organ dysfunction , long - term morbidity and mortality , the bone marrow transplant survivor study [ 3 ] demonstrated a protective effect provided by tbi compared to the chemotherapy - only regimen in over 850 patients who had survived autologous hematopoietic stem cell transplantation for more than 2 years . 
 [ 25 ] found that tbi , compared to chemotherapy - only conditioning , was mainly associated with cataracts , endocrine dysfunction , secondary cancers , and late severe bacterial infection , whereas pulmonary and cardiac problems seemed to be associated with chemotherapy and gvhr . 
there were no cases of late severe bacterial infections in our small cohort of long - term survivors , but 2 patients died secondary to sepsis during the time of aplasia . 
 [ 19 ] actually reported an inverse correlation between renal function and the prescribed tbi dose , and attributed this to the use of nephrotoxic contrast agents at the time of treatment planning with the aim of improving kidney shielding . 
hypothyroidism is a common late sequela of conditioning with and without tbi and has been observed in over 70% of patients 5 years after tbi ; supplementation was necessary in 10% of those affected [ 2 ] , which is consistent with our findings . two of our patients died as a result of secondary malignancies one hematological disease which occurred earlier and one solid tumor which occurred more than 10 years after transplantation . 
 [ 4 ] observed a cumulative incidence of 10% for solid cancer 10 years after conditioning with and without tbi , with a higher risk for younger patients and a higher risk for certain cancers , e.g. , thyroid , oral cavity , liver cancer , in patients receiving radiation therapy . 
our patients definitely remain at a life - long high risk for secondary cancers and should attend careful screening . conclusion low - dose rate tbi using conventional fractionation results in acceptable early and late toxicity with a demonstrated low risk for cataracts , interstitial pneumonitis , and veno - occlusive disease . 
therefore , despite its late sequelae , tbi remains warranted in certain pediatric patients ( over 2 years of age ) undergoing transplantation , given that chemotherapy - only conditioning regimens have not proven to be equally effective in the current literature . 
obviously , conditioning with tbi or chemotherapy for bone marrow transplantation in pediatric patients should be exclusively performed within studies and at specialized centers . strahlentherapie und onkologie original article intensity - modulated radiotherapy for prostate cancer implementing molecular imaging with 18f - choline pet - ct to define a simultaneous integrated boost michael pinkawa1 , richard holy1 , marc d . 
eble1 purpose : to report the own experience with 66 patients who received 18f - choline pet - ct ( positron emission tomography - computed tomography ) for treatment planning . patients and methods : image acquisition followed 1 h after injection of 178355 mbq 18f - choline . 
a dose of 76 gy was prescribed to the prostate in 2 - gy fractions , with a simultaneous integrated boost up to 80 gy . results : a boost volume could not be defined for a single patient . 
gtvpet and suv levels were found to be dependent on prognostic risk factors , particularly gleason score . key words : prostate cancer intensity - modulated radiotherapy simultaneous integrated boost dose escalation choline pet strahlenther onkol 2010 ; 186 : 6006 doi 10.1007 / s00066 - 010 - 2122 - 5 intensittsmodulierte radiotherapie des prostatakarzinoms mit simultanem integrierten boost nach molekularer bildgebung mit 18f - cholin - pet - ct ziel : erfahrungsbericht mit 66 patienten nach 18f - cholin - pet - ct ( positronenemissionstompgraphie - computertomographie ) zur bestrahlungsplanung . patienten und methodik : die bildakquisition erfolgte 1 h nach injektion von 178355 mbq 18f - cholein intraprostatischer herd ( gtvpet [ makroskopisches tumorvolumen ] ) wurde ab einem tumor - zu - hintergrund - suv - ( standard uptake value - ) quotienten > 2 definiert . 
die verschreibungsdosis fr die prostata betrug 76 gy in 2 - gy - einzeldosen mit simultanem integrierten boost bis 80 gy . ergebnisse : ein boostvolumen konnte bei einem patienten nicht definiert werden . 
in multivariater analyse resultierte ein gleason - score > 7 als ein unabhngiger faktor fr gtvpet > 8 cm3 ( relatives risiko 5 , 5 ; p = 0 , 02 ) und suvmax > 5 ( relatives risiko 4 , 4 ; p = 0 , 04 )  . 
eine neoadjuvante hormontherapie ( nht ) war ohne einfluss 1department of radiotherapy , rwth aachen , germany , 2department of nuclear medicine , rwth aachen , germany , 3philips research , molecular imaging systems , aachen , germany . received : january 11 , 2010 ; accepted : april 30 , 2010 published online : september 30 , 2010 strahlenther onkol 2010 no . 
die mittleren euds ( equivalent uniform doses ) fr rektum und blase ( 55 , 9 gy und 54 , 8 gy ) waren vergleichbar zu patienten ( n = 18 ) , die in der gleichen periode ohne boost bestrahlt wurden ( 54 , 3 gy und 55 , 6 gy )  . schlussfolgerung : die bestrahlungsplanung nach 18f - cholin - pet - ct ermglicht die definition eines integrierten boostvolumens bei nahezu allen patienten mit prostatakarzinom einschlielich patienten nach nht ohne einen relevanten einfluss auf die euds fr die risikoorgane . 
gtvpetund suv - werte zeigten eine abhngigkeit von prognostischen risikofaktoren , insbesondere dem gleason - score . schlsselwrter : prostatakarzinom intensittsmodulierte radiotherapie simultaner integrierter boost dosiseskalation cholin - pet introduction dose escalation in the treatment for prostate cancer has been shown to improve biochemical control rates , associated with the problem of increased rectal toxicity [ 1 , 16 , 19 , 44 ]  . 
found the origin of all local recurrences within the initial tumor volume , supporting the rationale of a selective dose escalation only to the intraprostatic lesion [ 6 ]  . 
magnetic resonance imaging ( mri ) , magnetic resonance spectroscopy ( mrs ) and positron emission tomography ( pet ) with acetate or choline are suitable noninvasive methods to localize intraprostatic lesions with an adequate sensitivity and specificity [ 13 , 20 , 21 , 23 , 25 , 30 , 42 ]  . 
in contrast to 18f - fluorodeoxyglucose ( fdg ) , a marker of the glucose metabolism with a poor performance in prostate cancer [ 11 ] , 11cor 18f - choline and 11c - acetate reflect increased lipid metabolism [ 29 ]  . the simultaneous integrated boost ( sib ) concept , using 18f - choline pet - ct ( computed tomography ) for treatment planning , has been implemented in our department . 
as demonstrated in a meta - regression analysis of randomized dose - escalation trials , the 5 - year biochemical control rate after a dose escalation from 76 to 80 gy can be expected to increase from about 70% to 80% [ 38 ]  . 
considering a low / ratio for prostate cancer , an additional benefit might result from higher doses per fraction [ 4 ]  . the purpose of this study was to correlate imaging data with prostate biopsy results and already established prognostic factors . 
treatment plans for these patients were compared to the plans of patients who were treated with the same dose to the prostate , but without an sib . patients and methods pet - ct ( philips gemini tf 16 ) with 18f - choline was performed in 66 consecutive prostate cancer patients for treatment planning . 
 gtvpet ( gross tumor volume ; intraprostatic lesion ) was defined by a tumor - to - background choline uptake ratio > 2 , based on the results of studies correlating choline pet results with histopathologic examinations [ 13 , 20 , 21 , 30 ]  . 
we have identified an area of about 1 cm2 within the prostate with the lowest activity and defined the threshold for gtvpet after multiplying the suvmax ( maximum standard uptake value ) in this area by for the planning target volume ( ptv ) , an 8 - mm lateral and anterior , 5 - mm superior and inferior and 4 - mm posterior margin was added . 
a uniform margin of 4 mm was added to the gtvpet to account for intrafraction target motion , with the exception of the posterior direction ( 3 mm )  . 
intrafraction prostate displacements have been evaluated in our department recently the required margins were calculated to be 4 mm in all directions , with 85% of displacements within a margin of 3 mm [ 27 ]  . an inverse planning with a five - field step - and - shoot imrt technique and 15 - mev photons was used . 
the direct machine parameter optimization ( dmpo ) algorithm was applied for inverse planning with a 2 - cm2 minimum segment area , 5 minimum segment monitor units and a maximum number of 70 segments . the dose to the ptv was prescribed to a reference point ( outside the volume of gtvpet ) , as suggested by the icru for conformal radiotherapy [ 17 ]  . 
the general relationship between icru reference and ptv mean doses in imrt has been found to be similar to that in three - dimensional dose distributions [ 43 ]  . 
 ct : computertomographie ; pet : positronenemissionstomographie . single lesion n ( % ) 11 ( 17 ) 6 ( 9 ) 19 ( 29 ) two lesions n ( % ) three or more lesions n ( % ) 22 ( 33 ) 7 ( 11 ) single lobe two lobes central central + both lobes multiple locations pare suv levels , volumes or dose values in independent patient groups . 
ctv : klinisches zielvolumen ; gtv : makroskopisches tumorvolumen ; pet : positronenemissionstomographie ; ptv : planungszielvolumen . region of interest gtvpet + margins gtvpet + margins ptv ( gtvpet + margins ) rectum rectum rectum bladder bladder type uniform dose = prescription dose to gtvpet dose homogeneity minimum dose minimum dose uniform dose = prescription dose to ptv maximum dose maximum dose to 20% volume maximum dose to 50% volume maximum dose to 30% volume maximum dose to 50% volume objective 80 gy 5% 76 gy 72 gy ( 95% of prescription dose ) 76 gy 76 gy ( constraint ) 70 gy 50 gy 70 gy 55 gy treatment plans for patients who were treated with sib were compared with patients treated without sib in the same period ( boost volume not defined or 18f - choline pet - ct not performed ) , but otherwise the same objectives . 
radiotherapy concepts including pelvic lymph nodes have not been considered for this comparison , so that the plans of 60 patients with sib were compared to 18 plans without sib . 
we have focused on the eud ( equivalent uniform dose ) [ 10 ] for the ptv , rectum and bladder , and the ntcp ( normal - tissue complication probability ) for the rectum and bladder . n = voxel number ; di = dose in the ith voxel ; a = tumor or normal - tissue - specific parameter that describes the dose - volume effect [ 41 ] ; with a = 10 for prostate cancer and a = 6 for bladder and rectum in this study [ 11 , 41 ]  . ntcp for grade 3 or worse rectum and bladder toxicity was computed applying the lyman - kutcher - burman model with emami parameters ( rectum : n = 0.12 , m = 0.15 , median toxicity dose = 80 gy ; bladder : n = 0.5 , m = 0.11 ; median toxicity dose = 80 gy ) [ 5 , 12 ]  . statistical analysis was performed using the spss 17.0 ( spss , chicago , il , usa ) software . 
imrt with 18f - choline pet - ct dose - volume histogram bladder rectum 1000 2000 3000 4000 5000 6000 7000 8000 9000 dose ( cgy ) gtv + margins were found for 36 ( 55% ) , 22 ( 33% ) and seven patients ( 11% ; table 3 ; figures 1 and 2 )  . 
if a boost was defined , the lobe ( s ) with a positive biopsy correlated with a gtvpet in the same lobe in 63 cases ( 97% ) 41 patients with one - sided and 22 patients with both - sided positive biopsies . 
additionally , a gtvpet was defined in 33 prostate lobes with only negative biopsies ( 80% ) , so that only eight patients remained with a unilaterally negative biopsy and negative pet in the same lobe . gtvpet , suvmean and suvmax were found to be dependent on well - known prognostic risk factors ( table 4 ) , particularly t - stage , as defined before pet - ct , and gleason score . 
a significant correlation was found between suvmax and gtvpet ( figure 3 ) larger lesions 1000 2000 3000 4000 5000 6000 7000 8000 9000 dose ( cgy ) figures 2a and 2b . 
one , two and three or more lesions within the prostate were more likely to have a higher choline uptake . no relevant differences for the eud and ntcp for grade 3 or worse toxicity resulted in the comparison of patients who were treated with sib and patients who were treated with the same prescription dose to the prostate , but without sib , for the bladder and rectum ( table 5 )  . 
dose escalation in the area of the primary macroscopic tumor is also applied in several other regions , probably most frequently for breast can cer the clinical benefit on local control has been demonstrated [ 2 , 31 ]  . 
 whole - prostate radiotherapy has always to be included in the prostate cancer treatment concept , as prostate cancer is known to be a multifocal disease , and diagnosis of microscopic cancer is not possible with presently available imaging modalities [ 7 ]  . gtv / cm3 figure 3 . 
korrelation von suvmax mit gtvpet ( spearmans rho = 0 , 53 ; p < 0 , 001 )  . with 54% , the majority of gtvpet were localized within a distance of 3 mm to the rectal wall , while only 22% were localized within a distance of 5 mm to the bladder wall . 
the sib con * p < 0.01 focal therapy without considering the whole gland has been proposed for selected low - risk patients to bridge the gap between radical treatment and active surveillance [ 35 , 36 ] this is not the concept of this study . 
 in contrast to surgical methods , cryotherapy or high - intensity focused ultrasound ( hifu ) , imrt offers the potential to treat different parts of the gland with different recurrence risk - dependent intensities . in contrast to biopsy results with predominantly unilateral tumors , pet - ct showed bilateral areas of high choline uptake in the majority of patients . 
in a study of 261 men with low - risk prostate cancer and only one or two positive cores on at least sextant biopsy , only 35% had unilateral disease following examination of radical prostatectomy specimen [ 32 ]  . the experience with sib for the primary imrt of prostate cancer is increasing . 
imrt with 18f - choline pet - ct an mri / mrs - detected lesion did not found an increase in severity or incidence of acute toxicity [ 14 ]  . 
 [ 14 ] could identify an intraprostatic lesion in only 118 of 230 prostate cancer patients after mri / mrs in contrast to the identification of a lesion in 65 of 66 patients in our study . 
 [ 42 ] reported a choline pet sensitivity of 100% for primary lesions , in comparison to only 60% for mri and 65% for mrs in a group of 20 patients . nht is known to decrease choline uptake in prostate cancer [ 15 , 34 ]  . 
the ratio between tumor and normal tissue is the key to identifying aggressive disease [ 25 ]  . two imrt planning studies have been published recently , using 18f - choline pet - ct [ 26 ] and 11c - acetate pet - ct [ 33 ] for sib definition . 
as in the present evaluation , the results of these studies demonstrate the feasibility of a dose escalation to the intraprostatic lesion without a relevant increase of eud and ntcp to the organs at risk . 
the dose to the whole prostate determines predominantly the dose to the organs at risk [ 26 ]  . the association of gtvpet and suv levels with well - known prognostic risk factors is crucial for an improved individualized imrt approach . 
larger volumes within the prostate can thus be treated with higher doses in high - risk patients , while high - dose areas can be restricted in patients with prognostically more favorable tumors . 
in our data , a separate analysis of gleason score 4 + 3 versus 3 + 4 patients was not possible , as all biopsy gleason scores 7 corresponded to 3 + 4 patterns . conclusion treatment planning with 18f - choline pet - ct allows the definition of an integrated boost in nearly all prostate cancer patients including patients after nht without considerably increasing eud and ntcp for the organs at risk . gtvpet and suv levels were found to depend on prognostic risk factors , particularly a gleason score > 7 . 
the opportunity for more individualized treatment concepts results : in contrast to a uniform concept for all prostate cancer patients in many radiotherapy departments , dose escalation in larger volumes can be limited particularly for more aggressive primary tumors . acknowledgment the implementation of the pet - ct was supported by philips research . strahlentherapie und onkologie original article variability in bladder volumes of full bladders in definitive radiotherapy for cases of localized prostate cancer naoki nakamura1 , naoto shikama1 , osamu takahashi2 , makiko ito3 , masatoshi hashimoto3 , masahiro uematsu3 , yukihiro hama3 , kenji sekiguchi1 , keiichi nakagawa4 background and purpose : to evaluate variation in bladder volume of full bladders in definitive radiotherapy for localized prostate cancer and to investigate potential predictors of increased bladder volume variations . patients and methods : in 40 patients , the bladder volume was measured with megavoltage computed tomography ( mvct ) imaging performed just before irradiation during the administration of the 1st fraction ( #1 ) , the 10th fraction ( #10 ) , the 20th fraction ( #20 ) , and the 30th fraction ( #30 )  . 
patients were also encouraged to drink an unspecified volume of liquid that would result in a clear but tolerable urge to urinate . results : the population - mean bladder volume ( 1sd ) was 219 ml ( 83 ml ) at the planning ct scan ( pln - ct ) , 186 ml ( 96 ml ) at #1 , 149 ml ( 73 ml ) at #10 , 137 ml ( 59 ml ) at #20 , and 136 ml ( 60 ml ) at #30 . 
the bladder volume at the pln - ct was correlated with the intrapatient variance in bladder volume with a correlation coefficient of 0.54 and p < 0.001. conclusion : we observed a significant decline in bladder volumes during the course of radiotherapy . 
the bladder volume at the pln - ct was a significant predictor of increased bladder volume variations . key words : radiotherapy prostate cancer imrt bladder volume full bladder mvct strahlenther onkol 2010 ; 186 : 63742 doi 10.1007 / s00066 - 010 - 2105 - 6 schwankungen des volumens gefllter blasen in der definitiven radiotherapie bei lokalisiertem prostatakarzinom hintergrund und zweck : die evaluierung der schwankungen des blasenvolumens gefllter blasen in der definitiven radiotherapie bei lokalisiertem prostatakrebs sowie die untersuchung potenzieller prdiktoren fr erhhte schwankungen des blasenvolumens . patienten und methoden : das blasenvolumen von vierzig patienten wurde mittels megavoltage - computertomographie ( mvct ) bestimmt , die bei der verabreichung der 1 . 
die patienten wurden zudem ermuntert , eine nicht nher bestimmte menge an flssigkeit zu sich zu nehmen , um einen deutlichen aber tolerierbaren harndrang herbeizufhren . ergebnisse : der mittelwert der grundgesamtheit des blasenvolumens ( 1sa ) lag beim planungs - ct - scan ( pln - ct ) bei 219 ml ( 83 ml ) , 186 ml ( 96 ml ) bei #1 , 149 ml ( 73 ml ) bei #10 , 137 ml ( 59 ml ) bei #20 und 136 ml ( 60 ml ) bei #30 . 
der mittelwert der schwankung des blasenvolumens innerhalb eines patienten ( 1sa bezogen auf den mittelwert des blasenvolumens des einzelnen patienten ) lag bei 38 % ( spannweite : 1084 % )  . 
das blasenvolumen zum zeitpunkt des pln - ct wurde mit der streuung des blasenvolumens innerhalb eines patienten korreliert , woraus sich ein korrelationskoeffizient von 0 , 54 mit p < 0 , 001 ergab . fazit : im laufe der radiotherapie konnte eine deutliche verringerung der blasenvolumen festgestellt werden . 
das blasenvolumen zum zeitpunkt des pln - ct - scans erwies sich als signifikanter prdiktor erhhter schwankungen im blasenvolumen . schlsselwrter : radiotherapie prostatakarzinom imrt blasenvolumen gefllte harnblase mvct 1department of radiation oncology , st . 
lukes international hospital , tokyo , japan 3department of radiology , edogawa hospital , tokyo , japan 4department of radiology , tokyo university school of medicine , tokyo , japan received : january 18 , 2010 ; accepted : august 3 , 2010 published online : november 8 , 2010 strahlenther onkol 2010 no . 
ct - stadium : klinisches tumorstadium ; psa : prostataspezifisches antigen ; ipss : international prostate symptom score ( internationaler prostata - symptomscore )  . nakamura n , et al . 
changes in the bladder volumes affect both bladder dose volume and the position of adjacent organs ( the prostate , seminal vesicles , small intestine , sigmoid colon , and rectum )  . 
furthermore , significant variations in bladder volume can confound the planned dose distributions for three - dimensional conformal radiotherapy ( 3d - crt ) and intensitymodulated radiotherapy ( imrt ) [ 8 , 9 , 14 , 20 , 23 ]  . 
therefore , bladder volume must be kept consistent throughout planning and treatment to reduce positional uncertainties related to the prostate and the risk of increased toxicity in the normal surrounding tissue . there is no current consensus regarding optimal bladder volumes . 
one possible advantage of maintaining a full bladder is that part of the bladder is moved away from the target volume , thus , reducing bladder toxicity [ 6 , 11 , 12 ]  . 
moreover , a full bladder moves the small intestine and the sigmoid colon out of the irradiation field , also reducing toxicity in these organs [ 3 , 5 , 10 , 13 ]  . 
time trends have been observed during the course of radiotherapy course [ 11 , 16 , 18 ]  . the aim of this study was to quantify the variations and trends in full bladder volume during the course of radiotherapy in patients being treated for prostate cancer . 
the second aim was to investigate the potential predictors of increased bladder volume variations . ct stage ( tnm 6th ed . ) gleason score initial psa damicos risk group intermediate ipss 12a 2c3 810 010 1020 high 9 - 1 - 9 2030 no . 
 ( % ) 19 ( 48 ) 4 ( 10 ) 17 ( 43 ) 15 ( 38 ) 9 ( 23 ) 16 ( 40 ) 25 ( 63 ) 10 ( 25 ) 5 ( 13 ) 10 ( 25 ) 8 ( 20 ) 22 ( 55 ) 22 ( 55 ) 13 ( 33 ) 5 ( 13 ) 21 ( 53 ) 19 ( 48 ) 71 ( 5383 ) methods and materials patient characteristics between december 2007 and march 2008 , 40 patients with localized prostate cancer ( ct1 - 3n0m0 ) were enrolled into this study ( table 1 )  . age mean ( range ) neoadjuvant hormone therapy radiotherapy all patients received definitive radiotherapy with helical tomotherapy using the hi - art system ( tomotherapy , inc . , madison , wi , usa ) at edogawa hospital ( tokyo , japan )  . 
the clinical target volume ( ctv ) was defined as prostate only for low - risk patients , and prostate with a 5 mm margin and a 2 cm wide section of the proximal seminal vesicle for the intermediate - risk and high - risk patients . 
the planning target volume ( ptv ) was defined as the ctv plus a 5 mm margthe prescribed dose , which was defined as 95% of the ptv receiving 100% of the prescribed dose ( d95 ) , was 72 gy in 36 fractions for the low - risk patients and 76 gy in 38 fractions for the intermediate - risk and high - risk patients . 
 treatment planning optimization was performed to satisfy the dose constraints defined by the in - house protocols for both the ptv and the organs at risk ( oar )  . 
the dose constraints for the ptv are a mean dose < 79.8 gy ( 105% of the prescribed dose ) and a maximum dose < 83.6 gy ( 110% of the prescribed dose )  . 
bladder volume variance with full bladders patient preparations the patients were instructed to refrain from urinating for 6090 minutes before the planning ct scan ( pln - ct ) and before daily irradiation . 
the patients were instructed to take laxatives before the pln - ct , although no specific instructions regarding bowel movements before daily irradiation were issued . bladder volume measurement bladder volume at the pln - ct was measured by kilovoltage ct ( kvct ) imaging with a thickness of 2.5 mbladder volume was also measured by mvct imaging with a thickness of 4 mm four times during the course of radiotherapy : at the 1st fraction ( #1 ) , at the 10th fraction ( #10 ) , at the 20th fraction ( #20 ) , and at the 30th fraction ( #30 )  . 
as a measure of variation in intrapatient bladder volumes , the sd of vmean ( denoted as bl ) is used , whereas , bl - rel was defined asbl relative to vmean . potential predictors we also assessed the correlations between intrapatient bladder volume variations ( bl - rel ) and potential univariate predictors . 
the following potential predictors were evaluated : age ( continuous ) , t stage ( t1t2a , t2b , t2ct3 ) , gleason score ( 26 , 7 , 810 ) , pretreatment prostate - specific antigen ( psa ) ( continuous ) , risk group ( low , intermediate , high ) , international prostate symptom score ( ipss ) [ 2 ] ( continuous ) , hormone therapy ( with or without ) , bladder volume at the plnct ( continuous ) , prostate volume ( continuous ) , ptv volume ( continuous ) , and acute cystitis ( grade 01 , grade 2 , grade 35 ) statistical analysis we used prism version 5 ( graphpad software inc . , la jolla , ca , usa ) for statistical analysis . 
the incidence of acute cystitis was described according to the common terminology criteria for adverse events ( ctcae ) v3.0. results all patients completed radiotherapy free of unscheduled interruptions exceeding 2 days . 
auf diesem korrelationsdiagramm ist die beziehung zwischen den blasenvolumen zum zeitpunkt des planungs - computertomographie - scans ( pln - ct ) und den schwankungen des blasenvolumens innerhalb eines patienten abgebildet ( bl - rel )  . 
we observed a statistically significant correlation between intrapatient variation in bladder volume ( bl - rel ) and bladder volume at the pln - ct ( pearson r = 0.54 , p < 0.001 ) ( figure 3 )  . 
 [ 16 ] report that a fixed drinking protocol did not eliminate all variations in the bladder volume , in part due to significant individual variations in velocity of bladder filling . 
they [ 16 ] also reported that patients are able to accurately judge their bladder filling state and suggested that subjective patient assessments should be taken into account during efforts to control bladder volume . 
table 2 summarizes the findings of previous reports on variations in intrapatient bladder volume , suggesting that no protocol can ensure consistent bladder volumes when the goal is to maintain a full bladder . our study showed a decline in bladder volumes during the treatment course . 
 [ 19 ] uterine cervical this study prostate cancer not fixed gave patients drinking advice according to their daily bladder volume ( feedback group ) 500 ml ( 1 hour before ) daily daily 255 ml 348 ml 367 ml twice weekly 378 ml 219 ml 89 ml ( 33% ) 149 ml ( 47% ) 156 ml ( 40% ) 168 ml 62 ml ( 38% ) * intrapatient one standard deviation ( one standard deviation relative to mean bladder volume )  . nificant correlation between intrapatient variations in bladder volume and the incidence of acute cystitis , and the mechanism underlying the decline in bladder volume can not be explained by cystitis alone , since our study and previous reports [ 1 , 11 , 16 , 18 ] showed that reductions in bladder volume occurred immediately after treatment had been initiated . 
bladder volume reductions during a treatment course may result in inadequate bladder dosevolume histograms ( dvh ) and may move the small intestine and sigmoid colon into the high dose irradiated field , increasing the potential toxicity for these organs . 
based on the clear trend toward a decline in bladder volume during the course of radiotherapy , a more effective approach may be to perform planning ct scans in the middle of the fractionated radiotherapy course and perform replanning when large bladder volume variations are found . in our study , larger bladder volumes at planning ct scans correlated with larger bladder volume variations , and previous studies reported similar findings [ 11 , 16 , 18 , 21 ]  . 
on the other hand , excessively small bladder volumes make it difficult to satisfy the planning dose constraints for adjacent organs ( the bladder , small intestine , and sigmoid colon )  . 
a half - full bladder appears to represent a reasonable target , offering the potential to improve bladder volume consistency in order to satisfy the dose constraints of the adjacent organs . we used two different modalities to measure bladder volume : kvct and mvct . 
we also found significant population - mean bladder volume reductions from #1 to #30 , which were both measured by mvct imaging . conclusions a significant decline in bladder volumes during the course of radiotherapy was observed . 
it may be possible to harness this trend to reduce bladder volume variance in order to avoid over - full bladders . funding this work was supported by health and labor sciences research grants ( h19 - 001 ) ; grants - in - aid for cancer research ( 20s - 5 ) , and a grant - in - aid for scientific research : third term comprehensive control research for cancer ( h16 - 039 , h19 - 038 ) from the ministry of health , labor , and welfare of japan . strahlentherapie und onkologie current discussion combination of ionising irradiation and hyperthermia activates programmed apoptotic and necrotic cell death pathways in human colorectal carcinoma cells frederick mantel1 , * , benjamin frey1 , * , stefan haslinger1 , petra schildkopf1 , renate sieber1 , oliver j . 
since hyperthermia ( ht ) is a very potent radiosensitizer , the influence of ht ( 41.5 c for 1 hour ) alone and in combination with ionising irradiation ( x - ray ; 5 gy or 10 gy ) on the form of cell death as well as on the expression of proteins known to be major components in tumor cells apoptotic and necrotic pathways were examined in colorectal tumor cells . material and methods : the expression of proteins was analysed by western blot and the relative activity of caspases - 3 / 7 by fluorescence - based assay . 
colony formation was analysed using the clonogenic assay and cell death was determined with annexin v - fitc / propidium iodide staining . results : combining x - ray with ht led to similar activation of caspase - 3 / 7 and p53 expression in comparison to irradiation only while the amount of the pro - apoptotic proteins puma and bax was increased in hct15 and sw480 cells . 
combining 5 gy irradiation with ht compared to irradiation resulted in a significantly increased number of necrotic tumor cells and in decreased colony formation . conclusion : the combined treatment of colorectal tumor cells with x - ray and ht activates distinct tumor cell pathways and fosters the early appearance of a necrotic tumor cell phenotype . key words : hyperthermia irradiation apoptosis necrosis colorectal cancer strahlenther onkol 2010 ; 186 : 58799 doi 10.1007 / s00066 - 010 - 2154 - x kombination von ionisierender strahlung und hyperthermie aktiviert programmierte apoptotische und nekrotische zelltodessignalwege in humanen kolorektalen tumorzellen hintergrund : die malignitt von tumorzellen kann durch eingriffe in zelltodeswege abgemindert werden . 
da hyperthermie ( ht ) strahlensensibilisierend wirkt haben wir in kolorektalen tumorzelllinien den einfluss von ht ( 41.5 c fr 1 stunde ) alleine oder in kombination mit ionisierender strahlung ( x - ray , 5 oder 10 gy ) auf tumorzelltodesformen und auf die expression von proteinen , welche hauptbestandteile von apoptotischen und nekrotischen tumorzellsignalwegen sind , untersucht . material und methodik : die expression der proteine wurde mit western - blot - technik und die relative aktivitt von caspasen 3 / 7 mit fluoreszenz basierendem ansatz bestimmt . 
die koloniebildungskapazitt wurde mit klonogenem assay und zelltod mittels annexinvfitc / propidiumjodid frbung ermittelt . ergebnisse : kombinationen von x - ray mit ht fhrten zu vergleichbaren aktivierung von caspase 3 / 7 und p53 - expression im vergleich zur alleinigen bestrahlung , wohingegen die menge der pro - apoptotischen proteine puma und bax in hct15und sw480 - zellen zunah alleinige ht behandlung oder kombinationen mit x - ray resultierten in einem vorbergehend erhhten level an anti - apoptotischem protein bcl - 2 . 
frey contributed equally to this work received : march 31 , 2010 ; accepted : july 5 , 2010 published online : november 8 , 2010 strahlenther onkol 2010 no . 
cell death pathways induced by x - ray and heat introduction hyperthermia ( ht ) has been established in the treatment of malignant diseases as an adjuvant of already existing therapies such as chemotherapy ( ct ) or radiotherapy ( rt )  . 
the combination of ionising radiation ( x - ray ) and ht leads to significantly improved tumor control in several malignomas , as recent randomized clinical studies have demonstrated ( summarised in [ 14 ] )  . 
caveolin - 1 , are capable of modulating radiationinduced cell death [ 4 ] and that specific activation of the immune system contributes to cancer therapy success [ 3 ]  . 
we recently demonstrated that ht given in addition to x - ray fosters the release of the immune activating danger signal hmgb1 by colorectal tumor cells [ 29 , 30 ]  . 
like hmgb1 , released heat shock proteins induced by ht treatment have been shown to stimulate professional antigen - presenting cells finally leading to specific immune activation [ 31 ]  . apoptosis is defined as a programmed cell death mechanism and was first described by kerr et al . 
to investigate whether ht has an influence on this newly described pathway we analyzed in addition to proand anti - apoptotic proteins the expression of rip - 1 in colorectal sw480 and hct15 cancer cells treated with x - ray and / or ht . 
the disruption of the tumor cell membrane leads to the release of danger signals and consecutively to immune activation [ 22 ]  . in the present study we examined the form of tumor cell death induction by x - ray plus ht and focussed not only on the influence of ht alone but also in combination with x - ray on the expression of proteins known to be major components in the apoptotic and necrotic pathways of cells . 
knowledge of the molecular mechanisms of radiation - induced cell death is essential to adapt multimodal tumor therapies for each tumor entity [ 5 ]  . the induction of apoptosis is accompanied with the activation of caspases . 
in this study we examined the effect of ht plus x - ray on the activation of caspase - 3 and - 7 , as two executioner caspases of either intrinsic or extrinsic apoptosis , as well as on anti - apoptotic proteins like bcl - 2 . 
two days after treatment of colorectal tumor cells with ionising irradiation ( 5 gy or 10 gy ) , ht ( 41.5 c for 1 h ) , or a combination of both , the cells were stained with axv - fitc / pi , and cell death was analysed by flow cytometry . 
 zwei tage nach behandlung von kolorektalen tumorzellen mit ionisierender bestrahlung ( 5 gy oder 10 gy ) , ht ( 41.5 c fr 1 stunde ) , oder einer kombination aus beiden wurden die zellen mit axv - fitc / pi gefrbt und der zelltod mittels durchflusszytometrischer analyse bestimmt . 
puma belongs to the bh3 - only proteins of the bcl - 2 protein family as it shows homology to the bh3 ( bcl - 2 homology region ) domait is a highly conserved protein among different species and has been shown to be very effective in the induction of apoptosis [ 37 ]  . the balance between proand anti - apoptotic proteins decides over the cells determination for apoptosis or survival [ 7 , 8 ]  . 
we determined the expression of the effector protein bax as a pro - apoptotic bcl - 2 family member and the expression of the anti - apoptotic bcl - 2 . 
in addition , whether treatment with irradiation alone or with a combination of x - ray and ht leads to differences in rip - 1 ( see above ) or irf - 5 expression levels was also studied . 
signalling through irf - 5 sensitizes p53deficient tumors to cell death [ 17 ] and displays a promising target for colorectal cancer therapeutics [ 15 ]  . materials and methods cell culture human colorectal adenocarcinoma sw480 cells and human colorectal adenocarcinoma hct15 cells were grown in dulbeccos modified eagles medium ( dmem ; pan - biotech gmbh , aidenbach , germany ) supplemented with 10% fetal strahlenther onkol 2010 mantel f , et al . 
the activation of caspase - 3 and - 7 in sw480 ( a ) or hct15 ( b ) colorectal tumor cells 0 , 8 , 24 , 32 , 48 and 72 hours after single or combined treatment were analysed using a fluorescence - based caspase activity assay . 
the relative caspase activity was calculated by the quotient of the activity value of the treated samples and the activity value of the negative control ( untreated cells )  . 
die aktivierung von caspase - 3 und - 7 in sw480 ( a ) und hct15 ( b ) kolorektalen tumorzellen 0 , 8 , 24 , 32 , 48 und 72 stunden nach einzeloder kombinationsbehandlung wurde mit fluoreszenz basierendem caspase aktivittstest analysiert . 
gy : gray ; ht : hyperthermie ( 41.5 c fr 1 stunde ) ; w / o : unbehandelte kontrolle . bovine serum ( fbs ; biochrom ag , berlin , germany ) , 1% sodium pyruvate , 2 mm glutamine , 100 u / ml penicillin , and 100 g / ml streptomycin at 37 c in 5% co2 and 90% humidity . 
the cells were stored at 37 c during this time interval . determination of colony formation the clonogenic assay was performed on single - cell suspension of exponentially growing sw480 or hct15 colorectal tumor cells . 
colonies greater than 50 cells were counted using an automatic colony analyzing machine . induction and detection of cell death flow cytometry was used to detect death of colorectal tumor cells after x - ray and / or ht treatment . 
to distinguish apoptotic from primary and secondary necrotic cells , the exposure of phosphatidylserine ( ps ) by apoptotic and necrotic cells was analyzed by binding of fitc - labelled annexin v ( axvfitc ) , and necrosis was differed from apoptosis by co - staining with propidium iodide ( pi ) as described previously [ 19 ]  . 
the levels of the protein p53 in sw480 and hct15 colorectal tumor cells 24 ( a , c ) or 48 hours ( b , d ) after treatment with x - ray and / or ht were analysed by western blot . 
die menge an p53 protein in sw480 und hct15 kolorektalen tumorzellen 24 stunden ( a , c ) oder 48 stunden ( b , d ) nach behandlung mit x - ray und / oder ht wurden mit western blot - technik analysiert . 
gy : gray ; ht : hyperthermie ( 41.5 c fr 1 stunde ) ; w / o : unbehandelte kontrolle . page and blotted to pvdf membranes ( millipore , billerica , ma , usa )  . 
the following primary antibodies were used : anti - p53 ( dilution 1 : 2 , 000 , cell signaling ) , anti - puma ( dilution 1 : 1 , 000 , cell signaling ) , anti - bcl - 2 ( dilution 1 : 200 , santa cruz biotechnology ) , anti - bax ( 1 : 200 , santa cruz biotechnology ) , anti - irf - 5 ( dilution 1 : 1 , 000 , cell signaling ) and anti - rip - 1 ( dilution 1 : 200 , santa cruz biotechnology )  . 
after washing three times with tbst for 10 minutes , the membranes were incubated with horse peroxidase - conjugated rabbit anti - mouse ( 1 : 10 , 000 dilution ) , goat anti - rabbit ( 1 : 20 , 000 dilution ) or donkey anti - goat ( 1 : 7 , 500 dilution ) secondary antibody , respectively , soluted in 5% milk in tbst for 1 hour . 
after washing , the membranes were incubated with ecl for 1 minute and then visualised using amersham hyperfilm ecl ( ge healthcare limited , uk )  . the densitometric values of the protein expressions obtained by western blot analyses are displayed in the figures 49 and have been corrected with the actin - control expression . 
the levels of the protein puma in sw480 and hct15 colorectal tumor cells 24 ( a , c ) or 48 hours ( b , d ) after treatment with x - ray and / or ht were analysed by western blot . 
die menge an puma protein in sw480 und hct15 kolorektalen tumorzellen 24 stunden ( a , c ) oder 48 stunden ( b , d ) nach behandlung mit x - ray und / oder ht wurden mit western blot - technik analysiert . 
the basal expression level in untreated was set to 1 . analysis of caspase - 3 and - 7 activities the activities of caspase - 3 and - 7 were analyzed 0 , 8 , 24 , 32 , 48 and 72 hours after the treatments using a fluorescence - based caspase activity assay ( apo - one homogeneous caspase3 / 7 assay , promega , madison , wi , usa )  . 
briefly , an equal amount of cells were given into a 96 - well plate in duplicate , and the assay reagent was added in a ratio of 1 : 1 . 
 the fluorescence emission was measured using a fluorescence plate reader ( hts 7000 bio assay reader , perkin elmer ) with an excitation filter of 485 nm and an emission filter of 535 nnot only blanks containing assay reagent but also culture medium without cells were used to measure the background fluorescence . 
the levels of the protein bax in sw480 and hct15 colorectal tumor cells 24 ( a , c ) or 48 hours ( b , d ) after treatment with x - ray and / or ht were analysed by western blot . 
die menge an bax - protein in sw480 und hct15 kolorektalen tumorzellen 24 stunden ( a , c ) oder 48 stunden ( b , d ) nach behandlung mit x - ray und / oder ht wurden mit western blot - technik analysiert . 
gy : gray ; ht : hyperthermie ( 41.5 c fr 1 stunde ) ; w / o : unbehandelte kontrolle . statistical analyses representative western blot data of three independent experiments are displayed . 
a p value < 0.05 was considered as significant ( * ) and a p value < 0.01 as highly significant ( * * )  . results x - ray ( 5 gy ) combined with hyperthermia reduces colony formation of colorectal tumor cells in both sw480 and hct15 colorectal tumor cells ht highly significantly enhanced radiosensitivity after 5 gy irradiation ( figure 1a and b )  . 
the levels of the protein bcl2 in sw480 and hct15 colorectal tumor cells 24 ( a , c ) or 48 hours ( b , d ) after treatment with x - ray and / or ht were analysed by western blot . 
die menge an bcl - 2 protein in sw480 und hct15 kolorektalen tumorzellen 24 stunden ( a , c ) oder 48 stunden ( b , d ) nach behandlung mit x - ray und / oder ht wurden mit western blot - technik analysiert . 
gy : gray ; ht : hyperthermie ( 41.5 c fr 1 stunde ) ; w / o : unbehandelte kontrolle . x - ray combined with hyperthermia induces predominantly necrosis in colorectal tumor cells colorectal sw480 and hct 15 tumor cells behaved similar in regards to cell death induction ( figure 2 )  . 
in comparison to untreated cells or cells treated with ht only , x - ray alone led to a highly significant increase of necrotic cells after 48 hours , which could be further significantly increased when combing 5 gy irradiation with ht . 
the levels of the protein irf - 5 in sw480 and hct15 colorectal tumor cells 24 ( a , c ) or 48 hours ( b , d ) after treatment with x - ray and / or ht were analysed by western blot . 
die menge an irf - 5 protein in sw480 und hct15 kolorektalen tumorzellen 24 stunden ( a , c ) oder 48 stunden ( b , d ) nach behandlung mit x - ray und / oder ht wurden mit western blot - technik analysiert . 
gy : gray ; ht : hyperthermie ( 41.5 c fr 1 stunde ) ; w / o : unbehandelte kontrolle . x - ray combined with ht leads to similar activation of caspase - 3 and - 7 compared to irradiation only to determine the activation of caspase - 3 and - 7 in colorectal sw480 and hct15 carcinoma cells treated with irradiation and / or ht a fluorescence - based caspase activity assay 0 , 8 , 24 , 32 , 48 and 72 hours after the respective treatments was performed ( figure 3a and b )  . 
 in the case of irradiation with 10 gy , the activity for caspase3 / 7 was further increased compared to 5 gy irradiation and similar in tumor cells treated with 10 gy or 10 gy plus ht . 
in the case of hct15 cells , the caspase - 3 / 7 activity further increased , especially with the 10 gy dose and reached a maximum after 72 hours . 
the levels of the protein rip - 1 in sw480 and hct15 colorectal tumor cells 24 ( a , c ) or 48 h ( b , d ) after treatment with x - ray and / or ht were analysed by western blot . 
die menge an rip - 1 protein in sw480 und hct15 kolorektalen tumorzellen 24 stunden ( a , c ) oder 48 stunden ( b , d ) nach behandlung mit x - ray und / oder ht wurden mit western blot - technik analysiert . 
gy : gray ; ht : hyperthermie ( 41.5 c fr 1 stunde ) ; w / o : unbehandelte kontrolle . 72 hours after treatment compared to irradiated only cells . 
ht only led to no detectable caspase - 3 / 7 activity at all time points investigated . x - ray alone or combined with ht increases p53 expression in colorectal tumor cells expressed more p53 than untreated cells or cells treated with ht only 48 hours after the applications . 
ht only led to a slight increase in p53 expression compared to untreated cells ( figure 4b and d )  . the expression levels of p53 in sw480 or hct15 cells 24 hours ( figure 4a and c ) and 48 hours ( figure 4b and d ) after treatment are displayed . 
colorectal tumor cells treated with irradiation only or treated with a combination of irradiation and ht hyperthermia and combinations with x - ray increases expression of puma all treatments did not result in significant higher levels of puma in the sw480 and hct15 tumor cells 24 hours after applistrahlenther onkol 2010 no . 
48 hours after treatment , a higher level of puma was observed when ht was given alone or in combinations with x - ray in both sw480 and hct15 tumor cells ( figure 5b and d )  . hyperthermia and combinations with x - ray increase the expression of the pro - apoptotic protein bax combinatory treatments of sw480 or hct15 tumor cells with irradiation and hyperthermia or ht alone caused a higher expression of the pro - apoptotic protein bax as early as 48 hours after treatment ( figure 6 )  . 
however , a similar tendency was observed for hct15 cells ( figure 6d )  . hyperthermia and combinations with x - ray modulate the expression of the anti - apoptotic protein bcl - 2 one day after treatment of sw480 colorectal tumor cells , bcl2 was up - regulated in cells that had been treated with irradiation plus ht or ht only compared to irradiated and untreated cells ( figure 7a )  . 
however , waiting for another 24 hours , the expression of bcl - 2 returned to basal levels in sw480 and hct15 cells ( figure 7b and d )  . irradiation plus hyperthermia leads to up - regulation of irf - 5 irf - 5 sensitizes tumor cells for apoptosis . 
after 48 hours , the combination of x - ray and ht resulted in a slightly higher level of irf - 5 in sw480 cells in comparison to single treatments ( figure 8b )  . 
the total amount of irf - 5 decreased in hct15 cells ; however , all treatments led to an increased expression of irf - 5 in comparison to untreated cells ( figure 8d )  . hyperthermia , x - ray , and combinations of both increase expression of rip - 1 in colorectal tumor cells to analyse whether treatment with x - ray and / or ht causes the activation of the necroptotic pathway , the expression of rip1 in colorectal sw480 and hct15 tumor cells was examined . 
however , after 48 hours the levels of rip - 1 increased in colorectal tumor cells which were treated with ht and / or x - ray ( figure 9b and d )  . 
 a combination of irradiation and hyperthermia led to similar expression of rip - 1 in comparison to irradiation or ht alone . discussion preoperative chemoradiotherapy , as compared with postoperative chemoradiotherapy , improves local control of colorectal cancer [ 28 ]  . 
ht given in addition to rt significantly improved the number of complete responses and significant regressions in patients with locally advanced carcinoma of the rectum and significantly improved the 5 - year survival rates [ 6 ]  . 
we showed that ht given in addition to x - ray ( 5 gy ) significantly reduces the colony formation of sw480 and hct15 cells , respectively ( figure 1 )  . 
however , it cannot give information about the viability of the irradiated tumor cells or the type of cell death occurring since the cells could also be senescent [ 20 ]  . 
it was shown here that 48 hours after treatment with x - ray plus ht , colorectal tumor cells display higher necrotic rates compared to apoptotic rates ( figure 2 )  . 
one could speculate that this may be a basis for the higher efficacy of ht when applied together with a lower total dose of rt in for example already pre - irradiated areas [ 33 ]  . we conclude that the dying colorectal sw480 and hct15 cells have proceeded rather quickly into secondary necrosis instead of continuing their apoptotic prograthe latter was present , since prominent apoptotic proteins displayed an increased expression ( fig 46 )  . 
we showed here that ht in combination with x - ray fosters immune activating necrotic cell death forms and leads to activation of apoptotic and necrotic programs in tumor cells . 
treatment with irradiation or combinations of x - ray with ht lead to a higher level of p53 and high activation levels of caspase - 3 / 7 in colorectal carcinoma cells . puma and bax contribute to the activation of caspase3 / 7 . 
it was shown in this study that 48 hours after application , ht given in combination with irradiation leads to a higher expression level of puma in comparison to irradiation alone . 
 [ 36 ] demonstrated with gene knockout ( ko ) experiments the necessity of puma for apoptosis induced by p53 , hypoxia and dna - damaging agents in human colorectal cancer cells . 
cell death pathways induced by x - ray and heat x - ray plus ht via mitochondrial permeability transition rip - 1 irf - 5 puma activation activation caspase3 / 7 p53# down - regulation bcl - 2 blocking taken together , we have shown that the pro - apoptotic bcl - 2 family members bax and puma are up - regulated within cells treated with a combination of irradiation and ht , and the anti - apoptotic bcl - 2 is , after an initial up - regulation , finally down - regulated . 
the cells tend towards cell death as the pro - apoptotic proteins outbalance bcl - 2 [ 8 ]  . irf - 5 is a transcription factor known to be critical in the induction of apoptosis after dna damage . 
in hct15 cells , the amount of irf - 5 was significantly increased when applying ht , x - ray or combinations of both while sw480 show increased amounts of irf - 5 after x - ray plus ht treatment ( figure 8b )  . tumor cell death figure 10 . 
a schematic overview and possible interactions of proteins that are involved in the apoptotic and necrotic cell death program of colorectal tumor cells after treatment with x - ray and / or ht is given . 
bcl - 2 , after an initial up - regulation , is finally down - regulated when the activity of caspases - 3 / 7 increases ( 48 hours after treatment )  . 
ein schematischer berblick und mgliche interaktionen von proteinen , welche an apoptotischen und nekrotischen zelltodesprogrammen in kolorektalen tumorzellen nach behandlung mit ionisierender bestrahlung und / oder hyperthermie beteiligt sind , sind dargestellt . 
irf - 5 kann indirekt durch caspasen3 / 7 aktiviert werden wohingegen rip - 1 zum zelltod fhrt indem die ausbildung der mitochondrialen permeabilitts - transitions - pore gefrdert wird . 
this means that puma binds anti - apoptotic bcl - 2 proteins that sequester direct activator bh3 - only proteins , like bid , leading to the release of bid from bcl - 2 . 
the amount of the anti - apoptotic bcl - 2 was primarily increased after 24 hours in cells treated with the combination of x - ray plus ht ( figure 7 )  . 
however , after 48 hours , the combinatory treatments resulted in slightly lower bcl - 2 expression levels in sw480 and hct15 cells in comparison to irradiation only ( figure 7b and d )  . 
a novel aranorosin derivative , k050 , could be a potent therapeutic agent against bcl - 2 - overexpressing human malignancies [ 25 ]  . in contrast to apoptosis , necrosis is been known to be a non - physiological event . 
this study illustrates for the first time that in colorectal tumor cells the expression levels of rip - 1 are increased after application of x - ray alone , ht alone or in combination of both . 
figure 10 gives a schematic overview of some of the apoptosisand necrosis - regulating proteins examined in our study that are upor down - regulated in colorectal tumor cells after treatment with x - ray plus ht . taken together , both apoptotic and necrotic cell death programs were activated in colorectal tumor cells treated with x - ray plus ht . 
because a major death form of colorectal tumor cells 48 hours after a combinatory treatment with irradiation and ht was necrosis , we assume that treated tumor cells undergo secondary necrosis shortly after starting the apoptotic prografostering distinct tumor cell pathways and the release of immune - activating danger signals , e.g. 
cell death pathways induced by x - ray and heat lular heat - shock proteins [ 24 ] and hmgb1 [ 29 ] , contribute to the development of specific anti - tumor immunity . 
science acknowledgements this work was supported by the elan fond ( st - 08.06.30.1 ) of the friedrich - alexander university of erlangen - nuremberg , by the european commissions ( note ( tpa4 fp6 ) ) , and by the german research foundation ( graduate school of the sfb 643 )  . strahlentherapie und onkologie original article fibrotic changes after postmastectomy radiotherapy and reconstructive surgery in breast cancer a retrospective analysis in 109 patients johannes claen1 , 2 , sibille nitzsche2 , diethelm wallwiener3 , peter kristen4 , rainer souchon1 , michael bamberg1 , sara brucker3 purpose : the purpose of this study was to analyze the probability and time course of fibrotic changes in breast reconstruction before or after postmastectomy radiotherapy ( pmrt )  . 
 materials and methods : between 1995 and 2004 , 109 patients were treated with pmrt at tbingen university and underwent heterologous ( hl ) or autologous ( al ) breast reconstruction prior or subsequent to radiation therapy . 
fibrosis of the reconstructed breast after radiotherapy was assessed using the baker score for hl reconstructions and the common terminology criteria for adverse events ( ctcae ) for all patients . 
 key words : postmastectomy radiotherapy fibrotic changes breast reconstruction breast cancer treatment strahlenther onkol 2010 ; 186 : 6306 doi 10.1007 / s00066 - 010 - 2158 - 6 fibrose nach thoraxwandbestrahlung und brustrekonstruktion : eine retrospektive analyse bei 109 patientinnen zielsetzung : ziel der arbeit war es , die frequenz und den zeitlichen verlauf fibrotischer vernderungen nach thoraxwandbestrahlung und plastischer rekonstruktion der mamma zu analysieren . 
vincentius - kliniken , karlsruhe 3 department of gynecology , tbingen university , tbingen 4 department of gynecology , kreiskliniken reutlingen , reutlingen received : april 13 , 2010 ; accepted : august 3 , 2010 published online : november 8 , 2010 strahlenther onkol 2010 no . 
wir konnten keine risikofaktoren fr die entwicklung hhergradiger fibrosen identifizieren . schlsselwrter : radiotherapie nach mastektomie fibrotische vernderungen brustrekonstruktion brustkrebs behandlung introduction breast cancer is the most frequent malignancy in women in western countries with approximately 60 , 000 new cases in germany every year [ 12 ]  . 
however , mastectomy is still considered an acceptable approach particularly in locally advanced or multicentric disease [ 12 ]  . radiotherapy has been used as adjuvant local treatment for decades after mastectomy particularly in patients with locally advanced disease considered at high risk of local relapse . 
 according to current guidelines , chest wall irradiation is indicated in patients with t3 or t4 tumors , node - positive disease , or in patients with marginal or incomplete resection [ 12 , 20 ]  . 
it has , thus , been demonstrated that adjuvant radiotherapy reduces the risk of local relapse by approximately two - thirds ultimately improving long - term survival of the patients [ 7 , 19 , 23 , 2 ]  . 
however , there is an abundance of literature indicating that clinical results of reconstructive surgery are impaired in those patients who undergo adjuvant radiotherapy before or after breast reconstruction as compared to patients without adjuvant radiotherapy [ 4 , 13 , 17 , 28 ]  . 
yet , in patients requiring adjuvant radiotherapy a more detailed analysis of potential factors associated with fibrotic changes and clinical outcome of breast reconstruction , including timing and technique of reconstructive surgery or parameters of radiotherapy , is warranted . 
patients who were submitted to mastectomy after initial breast - conserving surgery and radiotherapy to the residual breast or patients with breast reconstruction after partial mastectomy were not eligible for analysis . 
patients were identified by searching the electronically stored treatment reports of the patients at the department of radiation oncology , by searching the database of tbingen cancer center , and by screening the operating logs of the two main referral centers of gynecological oncology ( tbingen university and reutlingen hospital )  . 
in 13 cases , no questionnaire was mailed because the patients had already died , or complete follow - up information was available from the hospital charts . the primary end - point of the analysis presented here is the rate of chronic fibrosis assessed by common terminoltable 1 . 
adl : activity of daily life . grade 1 grade 2 grade 3 grade 4 grade 5 grade 1 grade 3 grade 4 increased density , spongy feeling increased density with firmness or tethering increased density with fixation of tissue ; operative intervention indicated ; interfering with adl life - threatening ; disabling ; loss of limb ; interfering with vital organ function death breast with implant as soft as contralateral unaffected breast grade 2 minimal breast with implant with reduced softness , implant palpable but not visible moderate breast with implant harder than contralateral breast , implant palpable and visible severe breast with implant hard , tensious , painful , distortion is frequent strahlenther onkol 2010 no . 
fibrotic changes after treatment of breast cancer breast cancer ablation of the breast x - rt n = 109 autologous n = 20 ( 18.3 % ) heterologous n = 82 ( 75.2 % ) combined ( 6.4 % ) x - rt before x - rt before reconstruction ( 7.3 % ) x - rt after reconstruction n = 101 ( 92.7 % ) autologous ( 25 % ) heterologous ( 75 % ) autologous n = 18 ( 16.5 % ) heterologous n = 76 ( 75.2 % ) figure 1 . 
grnde fr initial nicht geplante operationen nach brustrekonstruktion . patients affected ( n ) reason for surgery flap loss loss of volume after radiotherapy dog ear resection organized hematoma unsatisfying cosmetic results protrusion of implant chronic infection complication with expander dislocation of expander distension of suture correction of the scar unplanned removal of expander or implant change of reconstruction technique nipple reconstruction new implant / expander capsular fibrosis ogy criteria for adverse events v3.0 ( ctcae ) ( table 1a )  . 
the primary gynecological referral center where breast reconstruction was performed was tbingen university in 54 patients , reutlingen hospital in 29 patients , and 9 additional departments in the remaining 26 patients . 
 systemic treatment systemic treatment was applied in 101 patients ( 92.7% ) with either endocrine treatment ( n = 19 ) , chemotherapy ( n = 18 ) , or chemotherapy followed by endocrine treatment ( n = 64 )  . 
the preferred regimen for chemotherapy and endocrine treatment were anthracyclines with ( n = 21 ) or without ( n = 45 ) taxanes , and tamoxifen with ( n = 10 ) or without ( n = 57 ) lh - rh agonists . 
 due to the small number of patients with plastic surgery subsequent to radiotherapy , the timing of breast reconstruction and radiotherapy was not considered further in our analyses . complete breast reconstruction was achieved in 95 patients ( 87.2% ) ; in 4 patients with implantation of expanders information was missing as to whether these were later rebaker i baker ii baker iii baker iv figure 2 . 
 fibrosis according to the baker classification information on capsular fibrosis in patients reconstructed with the use of expander / implants was available in 86 patients including 2 cases of primary breast reconstruction with autologous material and secondary implantation of permanent implants ( figure 2 )  . 
 fibrosis according to the ctcae classification data on fibrosis according to the ctcae classification were available in 103 patients ( figure 4 ) ; 18 patients developed fibrosis > grade iii . 
the technique of breast reconstruction had no significant influence on the incidence of fibrosis according to the ctcae classification ( log - rank ; p = 0.46 ) ( figure 5 )  . when considering fibrosis at the last follow - up visit , 5 patients suffered from > grade iii fibrosis corresponding to a months after radiotherapy figure 3 . 
 comparison of the reported clinical outcomes is hampered by the complex matter of available surgical techniques of breast reconstruction , aspects of timing between radiotherapy and plastic surgery , inconsistent definition of endoints reported , and a small sample size in the majority of studies . 
 fibrotic changes of the reconstructed breast induced by surgery and radiotherapy represent a frequent and consistently reported clinical challenge forming the basis for many secondary events ultimately summarized as complication in numerous reports [ 3 , 5 , 21 ]  . 
 when assessing the maximum degree of fibrosis observed during the follow - up period , a considerable rate of severe ( > grade iii ) fibrosis with 20% and 43% at 3 years accordmonths after radiotherapy figure 5 . 
kaplan - meier - schtzung fr die wahrscheinlichkeit , keine nebenwirkung > grad iii als maximale ausprgung whrend der nachbeobachtungszeit zu entwickeln . ing to the ctcae and baker classification , respectively , was found . 
it is of note , however , that those patients evaluated by the baker classification , which is only valid for heterologous reconstructions , represent a subset of our entire population which was assessed with the ctcae score . 
this view is supported by the observation that heterologous reconstruction was complicated with an increased rate of fibrosis in patients assessed by the ctcae scale as compared to patients with autologous reconstruction even though the difference was statistically not significant ( figure 5 )  . 
our data are , thus , in line with recommendations of a recent literature review [ 13 ] emphasizing the role of delayed autologous reconstruction in patients after mastectomy and adjuvant radiotherapy . 
in addition , this report outlines the fact that heterologous reconstruction bears a considerable risk of fibrosis even without radiotherapy : a 40% rate of capsular contraction was reported after heterologous reconstruction alone . 
considering the timeline of fibrosis subsequent to radiotherapy as well as the rate of fibrotic events after heterologous reconstruction , it remains speculative as to whether a delay of breast reconstruction by 23 years after radiotherapy might reduce the substantial rate of unplanned secondary surgical events observed in our patient cohort . 
however , volume loss and fibrotic shrinkage of the reconstructed breast after adjuvant radiotherapy can be expected with a high frequency [ 22 ] , thus , subsequently requiring adoption of the contralateral breast . 
we , therefore , assume that the actuarial rates of fibrosis calculated for our patients represent in fact a fair estimate of the true fibrosis rate for the treatment received . in addition to the maximum degree of fibrosis observed in an individual patient , the status at last follow - up visit was evaluated . 
in fact , with a 3 - year rate of 18% and 2% for > grade iii fibrosis according to baker and ctcae scores , respectively , a substantial decline in the fibrosis rate as compared to the maximum scoring method was observed . 
this finding is surprising at first glance , since the rate of radiation - induced fibrosis can be expected to increase rather than decrease with time [ 18 , 28 ]  . 
yet , it is important to note that approximately 36% of our patients underwent initially unplanned surgical corrections of the reconstructed breast , and resection of capsular fibrosis or removal / replacement of expanders / implants were the most frequent reasons for doing so ( table 2 )  . 
this rate is comparable to findings reported by other investigators [ 13 ] and indicates that fibrosis may to some extent successfully be surgically corrected resulting in an ultimately comparatively low rate of high grade fibrosis . 
this factor has repeatedly been attributed a major role with different effects in heterologous and autologous reconstructions [ 5 , 13 , 22 ] , while others did not observe any effect [ 4 , 21 ]  . 
 it should , however , be noted that tamoxifen has been associated with an increased rate of fibrosis of the lung and subcutaneous and breast tissue in conjunction with radiotherapy [ 1 , 2 , 9 , 10 ]  . 
we , therefore , can not rule out that our analysis did not have sufficient power to detect a possible influence of surgical techniques on the incidence of fibrosis . our study is limited by its retrospective nature with an inherent inaccuracy of evaluating and classifying endpoints of the analysis . 
furthermore , we did not assess cosmetic outcome or quality - of - life issues which play an important role when restoration of the physical appearance is one of the primary goals of treatment in order to cope with the trauma of cancer - related loss of the breast . conclusion this study has demonstrated that postmastectomy radiotherapy and cosmetic surgery of the breast is complicated with a considerable rate of high grade fibrosis of the reconstructed breast . 
treatment - related factors that significantly correlated with fibrosis of the reconstructed breast in association with adjuvant radiotherapy could not be identified . strahlentherapie und onkologie original article objective assessment of dermatitis following post - operative radiotherapy in patients with breast cancer treated with breast - conserving treatment ken yoshida1 , hideya yamazaki2 , tadashi takenaka1 , eiichi tanaka1 , tadayuki kotsuma3 , yuka fujita4 , norikazu masuda5 , keiko kuriyama1 , mineo yoshida1 , tsunehiko nishimura2 purpose : to evaluate radiation dermatitis objectively in patients with breast cancer who had undergone post - operative radiotherapy after breast - conserving surgery . 
 patients and methods : skin color ( l * , a * , and b * values ) and moisture analyses were performed for both breasts ( before , after , 1 month , 6 months , and 1 year after radiotherapy ) to examine irradiated and non - irradiated skin divided into four quadrants in 118 patients . 
these patients underwent breast conservative surgery followed by 50 gy / 25 fractions ( median ) of radiotherapy with or without boost irradiation ( 10 gy / 5 fractions )  . 
boost radiotherapy intensified reddish and darker color changes at the completion of radiotherapy , while chemotherapy did not intensify the skin reaction caused by radiotherapy . conclusion : moisture impairment as a result of irradiation lasts longer than color alterations . 
objective assessments are useful for analyzing radiation dermatitis . key words : breast cancer radiation dermatitis breast conservative treatment corneometer spectrophotometer strahlenther onkol 2010 ; 186 : 6219 doi 10.1007 / s00066 - 010 - 2134 - 1 objektive bewertung von dermatitis nach postoperativer strahlentherapie von brustkrebspatienten , die brusterhaltend operiert wurden hintergrund und ziel : objektive bewertung von strahlendermatitis bei brustkrebspatienten , die nach einer brusterhaltenden operation mit strahlentherapie behandelt wurden . patienten und methode : wir analysierten die hautfarbe ( l * a * b * - werte ) und feuchtigkeit an beiden brsten ( vor und nach der strahlentherapie sowie einen monat , sechs monate und ein jahr danach ) , um bei 118 patienten die bestrahlte und die nichtbestrahlte haut nach einteilung in vier quadranten zu untersuchen . 
diese patienten unterzogen sich einer brusterhaltenden operation , gefolgt von strahlentherapie mit 50 gy in 25 fraktionen ( medianwert ) mit oder ohne boost - bestrahlung ( 10 gy in 5 fraktionen )  . ergebnisse : die werte fr l * , a * und feuchtigkeit wurden durch bestrahlung verndert und beim abschluss oder einen monat nach der strahlentherapie maximiert . 
bei den allgemeinen toxizittskriterien ( ctc version 3 ) ergab sich eine gute korrelation mit den a * und l * - werten beim abschluss und einen monat nach der strahlenbehand1 department of radiology , national hospital organization osaka national hospital , osaka , japan , 2 department of radiology , kyoto prefectural university of medicine , kyoto , japan , 3 department of radiation oncology , osaka university graduate school of medicine , osaka , japan . 
 4 department of diagnostic and interventional radiology , osaka university graduate school of medicine , osaka , japan , 5 department of surgery , national hospital organization osaka national hospital , osaka , japan . 
boost - strahlentherapie verstrkte rtliche und dunklere farbvernderungen beim abschluss der strahlentherapie , wogegen chemotherapie die von strahlentherapie verursachten hautreaktionen nicht verstrkte . schlussfolgerung : beeintrchtigung der feuchtigkeit in folge der bestrahlung hlt lnger an als farbvernderungen der haut . 
 objektive bewertungen sind fr die analyse von strahlendermatitis hilfreich . schlsselwrter : brustkrebs strahlendermatitis brusterhaltende behandlung corneometer spektrophotometer introduction breast cancer is one of the most frequent cancers among women in several western countries , and most of these patients are treated post - operatively with radiotherapy [ 6 , 20 , 23 , 24 ]  . 
some studies have suggested that most patients treated with post - operative external radiotherapy for breast cancer will experience some type of skin reaction , such as skin dermatitis [ 13 ]  . 
some attempts to establish objective measurements have been reported in the literature [ 4 , 11 , 12 , 14 , 21 , 22 ] , i.e. , visual reflectance spectroscopy and determination of a high - frequency dielectric constant [ 15 ]  . 
these results have prompted the present study , which is concerned with the development of an objective assessment method for skin reaction that can be used by multiple observers , especially when a multi - institute trial is involved . 
 in addition , because several objective assessments tools were used to determine the reliability and reproducibility of these methods for dermatology and industrial , large - scale usage [ 2 , 3 , 8 ] , we used some of these tools ( corneometer and spectrophotometer ) to objectively examine radiation dermatitis . 
 in addition , the time course for skin reaction , its correlation with chemotherapy and boost radiotherapy , the influence of surface geometry as well as subjective criteria such as common toxicity criteria version 3 ( ctc v3 ) grading were also studied . 
 patients and methods breast irradiation after breast - conserving surgery ( bcs ) was administered to 118 breast cancer patients at the national hospital organization osaka national hospital between may 2000 and june 2005 . 
another 28 patients were examined for 2 years or more ( median follow - up : 5 years ; range : 29 years ) as a reference group ( group b )  . 
of the patients who underwent bcs , the residual breast was conventionally treated ( 1.82.2 gy / day , 5 fractions / week ) with a tangential field 4 - mv photon beam for a total dosage of 48.450 gy / 2225 fractions at the reference point ( median 50 gy / 25 fractions )  . 
additional fractionated boost irradiation of 10 gy / 5 fractions using 412 mev electron beams was administered to patients with a positive surgical margin of 5 mm or less ( table 1 )  . 
 all measurements were performed at room temperature and under room light using the color reader cr - 13 ( konicaminolta , tokyo , japan ) and corneometer cm 825 for skin hydration ( courage + khazaka gmbh , cologne , germany )  . 
 we measured four quadrants , a ( upper inner ) , b ( lower inner ) , c ( upper outer ) , and d ( lower outer ) , separately in irradiated and non - irradiated breasts to determine anatomical differences and recorded the worst score . 
 results baseline skin color and moisture : influence of surgery skin color was examined in terms of mean l * a * b * values in unexposed and surgically treated breasts , which were strahlenther onkol 2010 no . 
before radiotherapy , surgically treated quadrants showed a significantly different color compared to the other quadrants on the treated side and the contralateral intact quadrant ( figure 1 , l * darker , a * reddish , and b * yellow , all p < 0.001 ) ; however , no difference was found in the moisture analyses . 
changes in l * , a * , and b * values were readily visible not only in the quadrant where the tumor was located , but also in the other three quadrants , that is , surgery had a significant effect on the entire breast . 
objective analysis of radiation dermatitis after bcs green white black yellow blue * p < 0.01 * p < 0.01 tumor non - tumor tumor non - tumor treated side contralateral side treated side contralateral side * p < 0.01 tumor non - tumor tumor non - tumor treated side contralateral side treated side contralateral side figure 1 . 
 comparison of ctc v3 and color and moisture analysis we also investigated whether ctc v3 for radiotherapy skin reactions correlates with objective measurements of the skin ( figure 3 )  . 
patients with grade 2 reactions showed higher a * ( reddish ) and lower l * values ( darker ) than the grade 1 group at completion and 1 month after radiotherapy . 
time course for color alteration over time in the treated quadrant and identified contralateral intact quadrant : a l * value , b a * value , c b * value , d moisture . 
gruppe b : bezugsgruppe fr langzeitwirkungen , die eine strahlentherapie vor zwei oder mehr jahren erhalten hatten , pre : vor strahlentherapie , post : nach strahlentherapie , 1m : ein monat nach strahlentherapie , 6m : sechs monate nach strahlentherapie , 12m : zwlf monate nach strahlentherapie . 
each data point was adjusted by dividing it by its corresponding contralateral value and the value before radiotherapy ( adjusted value = raw data / previous value / untreated contralateral corresponding quadrant value )  . 
at completion of radiotherapy , patients with boost radiotherapy showed lower l * values ( darker , 55.56.9 ) compared to the group without boost radiotherapy ( 58.84.8 , p = 0.02 ) as well as differences in strahlenther onkol 2010 no . 
during the early periods of radiotherapy , radiation dermatitis also played an important role in estimating radiation influence in an objective fashion , i.e. , erythema dose in the 1910s was estimated to be about 56 gy and was also used for a unit of a radiation dose . 
although nearly a century has passed , we still do not have an objective and quantitative method to assess skin reactions , partly because the introduction of high energy linacs have resulted in weakened skin reactions . 
however , with innovation of several modalities , increasing number of multi - institute clinical trials , and altered schedules ( apbi , imrt , etc . ) [ 1 , 5 , 9 , 16 , 18 , 19 , 26 ] , an objective method to compare skin reactions by avoiding inter - observer and even intra - observer variations is needed . 
reported that the skin color ( especially red , the a * value ) depended on the radiation dose applied to the skin and that the objective spectrophotometric measurements correlated well with the subjective ctc scores [ 14 ]  . 
however , in several research fields , an objective analysis could provide useful data especially in comparing the differences between humans ( e.g. , different skin colors ) or between different radiaiton techniques ( i.e. , apbi and conventional extenal radiotherapy )  . 
on the other hand , a * already appeared to have returned to its previous value 1 month after treatment , which implies that darkening of the skin lasted longer than reddening after radiotherapy . 
for example , the b * value was changed by the addition of radiotherapy to yellowish in a statistically significant manner in momms study [ 4 ] , but was not significant according to our data , partly because of pre - existing ethnic color variations ( table 2 )  . 
other published data regarding skin color in terms of l * , a * , and b * values for caucasian and asian subjects are also shown in table 2 . 
 to the best of our knowledge , this is the first reported study to analyze the influence of radiotherapy with the aid of a corneometer and to describe the influence of surgery and geometric factors on the basis of objective analysis . 
according to these types , boost irradiation in our study produced very dry skin just after irradiation in 59% ( 10 / 17 ) of patients , while 50 gy of irradiation caused 39% ( 39 / 101 , p = 0.18 ) very dry skin at the end of radiotherapy ( figure 2 )  . 
 [ 21 ] used thermography to assess skin temperature and reported that abnormal skin temperature and sweating capacity of irradiated skin persist longer than readily visible morphological changes and last 2 years or more , which agrees with our findings . 
 conclusion surgery resulted in assessable changes in skin color even before radiotherapy and that radiotherapy caused transitional changes in color and long - lasting changes in moisture in irradiated sk as radiation dermatitis could be pronounced in intertriginous areas ( grazing area : i.e. , lower mammary fold , axillary part of breast ) , we examined each quadrant separately and found that the lateral upper side ( quadrant c ) showed greater changes in l * values ( became darker ) than did the other quadrants at the end of radiotherapy . 
 acknowledgment we would like to thank noriko takayama , kokoro momozono , itsuko kuroda , miyuki sakemi , kazunobu nakamura , minoru harada , and toshiaki tarui for their assistance in preparing this manuscript . strahlentherapie und onkologie original article multidisciplinary approach in the treatment of t1 glottic cancer the role of patient preference in a homogenous patient population nicola dinapoli1 , claudio parrilla2 , jacopo galli2 , rosa autorino1 , francesco miccich1 , francesco bussu2 , mario balducci1 , lucia dalatri2 , raffaella marchese2 , mario rigante2 , giuseppe di lella3 , luca liberati2 , giovanni almadori2 , gaetano paludetti2 , vincenzo valentini1 background and purpose : to compare oncological outcome and voice quality among a uniform and well - defined subset of patients with t1 glottic carcinoma . patients and methods : patients , affected by laryngeal glottic carcinoma , treated by laser co2 surgery or radiotherapy , have been analyzed . 
in order to verify differences in functional outcomes and voice quality , all patients were interviewed during their last follow - up visit during 2009 using the vhi ( voice handicap index ) questionnaire . 
no statistically significant differences were found between the two groups in terms of overall survival and disease - free survival ; dividing patients into stages t1a and t1b also made no difference . 
furthermore , the role of patient preference in the treatment modality choice and the value of a multidisciplinary approach for a detailed and multi - oriented discussion with the patient are outlined . key words : voice quality glottic carcinoma co2 surgery radiotherapy vhi questionnaire strahlenther onkol 2010 ; 60713 doi 10.1007 / s00066 - 010 - 2142 - 1 multidisziplinre herangehensweise an die behandlung von t1 glottiskarzinomen : die rolle der patientenbevorzugung in einer homogenen patientenpopulation hintergrund und zielsetzung : es sollen das onkologische ergebnis und die sprachqualitt in einer homogenen und gut definierten gruppe von patienten mit t1 - stimmbandkarzinomen verglichen werden . patienten und methoden : patienten mit einem glottiskarzinom , die sich einer co2 - laser - operation oder einer radiotherapie unterzogen hatten , wurden analysiert . 
um unterschiede im funktionellen ergebnis und bezglich der sprachqualitt zu quantifizieren , wurden alle patienten whrend der letzten nachsorge im jahre 2009 dazu angehalten den vhi - ( voice handicap index - ) fragebogen auszufllen . 
es konnte kein statistisch signifikanter unterschied zwischen den zwei gruppen bezglich der gesamtberlebenszeit und der krankheitsfreien zeit festgestellt werden ; dies gelang auch nicht , wenn die gruppen in stadium t1a und t1b getrennt betrachtet wurden . 
es lie sich zeigen , dass in jeder kategorie des vhi - fragebogens die patienten , die strahlentherapiert wurden , bessere ergebnisse erzielten als jene , die operiert wurden ( physikalisch : p = 0 , 0023 ; funktionell : p < 0 , 0001 )  . 
der durchschnittliche vhi - score fr strahlentherapierte patienten ist 4 , im gegensatz zu 18 fr operierte patienten ( p < 0 , 0001 )  . 1department of radiation oncology , catholic university of the sacred heart , rome , italy 2department of otorhinolaryngoiatry , catholic university of the sacred heart , rome , italy 3department of radiology , catholic university of the sacred heart , rome , italy received : march 11 , 2010 ; accepted : august 25 , 2010 published online : november 8 , 2010 strahlenther onkol 2010 no . 
weiterhin wird die bedeutung des patientenwunsches im hinblick auf die therapieoptionen und die bedeutung eines multidiszplinren therapieansatzes belegt . schlsselwrter : sprachqualitt glottiskarzinom co2 - laser radiotherapie vhi - fragebogen dinapoli n , et al . 
some authors suggest that the surgical subgroup of these studies were biased by the selection of the patients , e.g. , lesions invading the anterior commissure or the contralateral vocal cord ( t1b glottis tumors ) were excluded [ 30 , 37 ]  . 
in fact , in some studies that included t1b lesions for laser surgical treatment , the mean 5 - year local control rate was slightly lower ( 88% ; range between 81 and 93% ) [ 2 , 13 , 24 , 35 , 41 ]  . 
both modalities have high local control , larynx preservation and high disease specific survival rates , and all retrospective data available in the literature show that these two treatment modalities are comparable for t1a glottic cancer . 
however , no randomized trial has been performed and the choice of the treatment is often based on the local expertise and / or patient preference [ 8 , 14 , 23 , 39 , 40 , 42 , 46 , 54 ]  . over the last decade , functional outcome and voice quality seem to play a key role in the treatment strategies . 
in fact , radiotherapy is often preferred because it seems to be associated with reduced impairment of voice quality , but qualitative studies about vocal function in post - irradiated patients have been inconclusive and not uniform [ 12 , 16 , 17 , 18 , 20 , 28 , 31 , 48 , 50 ]  . 
the main problem of the comparative studies available about voice quality is bias in the selection criteria , due to the accurate preoperative and intraoperative diagnostic work - up available today . 
in fact , there is a distinct preference to treat patients with superficial t1a tumors with co2 laser and to reserve radiotherapy for the treatment of deeper infiltrating tumors [ 4 , 28 , 44 , 51 ]  . 
a further issue concerns the differences in the follow - up periods because of the retrospective design of these studies . radiotherapy surgery total male the aim of this retrospective analysis was to compare oncological outcome and voice quality among a uniform and welldefined subset of patients with t1 glottic carcinoma . 
this is not the first comparative retrospective study about oncological and functional results after t1 glottic carcinoma , but , to our knowledge , this is the first study with no bias regarding tumor extension ( t1a or t1b ) in the treatment strategies . 
in particular , the treatment strategy was based on patient preference , and all patients were suitable for both radiotherapy and laser surgery , excluding patients directed to only one treatment modality ( surgery or radiotherapy ) because of comorbidity , insufficient laryngeal exposition , or previous headneck radiotherapy . 
nevertheless , the same tumor boarding team ( radiotherapists , head and neck surgeons , and speech pathologists ) stratified , treated , and followed the patients with uniform criteria . materials and methods in order to analyze the differences between co2 laser surgery and radiotherapy for the treatment of laryngeal glottic carcinoma , a series of patients , treated since 1994 for surgery and 2001 for radiotherapy , have been analyzed . 
in order to obtain good overlapping results between surgery and radiotherapy data , the survival plots and calculations were performed only up to 5 years although the median surgical follow - up was longer than 5 years . 
in order to verify the differences in functional outcomes and voice quality , all patients were interviewed using the voice handicap index ( vhi ) questionnaire during their last follow - up visits during 2009 . 
the data of the vhi were analyzed question by question and by summarizing the results divided into three categories of vhi : physical ( p ) , functional ( f ) , and environmental ( e ) table 1 . 
all patients were treated by using a standard conformal technique with opposing latero - lateral 6 mv photon beams , by fitting the fields shape to the whole larynx clinical target volume . 
comparing the results between the two therapeutic approaches and dividing patients into stage t1a and t1b ( 126 patients , for the remaining 17 no staging information is available ) again showed no significant differences . in order to evaluate the differences in outcomes for surgery and radiotherapy , patients were interviewed using the vhi . 
 the answers were analyzed by comparing the single questions and by summing the results for each subset of questions , physical ( p ) , functional ( f ) and environmental ( e ) , so as to enhance and categorize possible differences : 33 surgical patients ( 45% ) and 49 radiotherapy patients ( 70% ) replied to the interview . 
 in table 3 , the individual answers to the questions are summarized ; the answers , where the difference between answers given by surgical and radiotherapy patients were statistically significant , are shown in bold . 
fnf - jahres - gesamtberleben , log rank test : p = 0 , 7983 , hazard ratio : 1 , 1093 , 95% - konfidenzintervall : 0 , 39933 , 2976 . 
fnf - jahres - raten krankheitsfreien berlebens , log rank test : p = 0 , 8979 , hazard ratio : 0 , 9309 , 95% - konfidenzintervall : 0 , 29902 , 8836 . 
durchgezogene linie : strahlentherapie ; gestrichelte linie : chirurgie . the scores , the overall number of low score responses is higher for radiotherapy patients , thus , indicating better outcomes . 
in order to analyze the overall results , the sum of each category of the vhi , physical ( p ) , functional ( f ) and environmental ( e ) , and the global vhi score in each patient for surgery and radiotherapy , have been analyzed using the mannwhitney test : strahlenther onkol 2010 no . 
the median vhi score for radiotherapy patients was 4 , while the median value of the vhi score for surgical patients was 18 ( mann whitney test p < 0.0001 , figure 4 )  . discussion the results of surgery and radiotherapy in the early stage of laryngeal cancer treatment are known to have good outcome in the literature , regardless of the treatment performed . 
although the total number of patients analyzed in this study was not very high and recruitment timing was different during the last decade ( in the first period , the patients generally underwent surgery and in the second period the patients underwent radiotherapy ) , there does not seem to be a significant difference in overall and disease - free survival . independent from the t stage ( t1a or t1b ) , the choice of treatment can be addressed by considering the survival and local control to both surgery and radiotherapy ; indeed , no statistical difference was found by the log rank test . 
 on the other hand , the debate in the literature about functional outcome is still open , and depending on the group that publish the data ( surgeons or radiation oncologists ) , it seems that each technique could be superior to the other or , at least , do not show any significant functional difference . 
thus , it seems that the therapeutical approach should depend only on the cost / benefit evaluations , or on the overall treatment time required for the therapy ( i.e , the surgical technique ensures the fastest results and , thus , the better global outcome )  . 
sulendiagrammdarstellung der summe der antworten aller patienten auf die voice handicap index - ( vhi - ) fragen . treatment choice due to factors different from the patients decision has been removed from our series . no significant differences were found when the age at diagnosis and staging were evaluated . 
therefore , the validate basic protocol envisages : ( 1 ) acoustic ( jitter , shimmer , fundamental frequency range , and softest intensity ) ; ( 2 ) aerodynamics ( phonation quotient ) ; ( 3 ) perceptual analysis ( grade , roughness , and breathiness ) ; ( 4 ) videostroboscopy ( closure , regularity of vibration , mucosal valve , and symmetry ) ; and ( 5 ) subjective scores ( vhi )  . 
however , some authors consider the analysis of the speech signal of sustained vowels inadequate , because the speech in laryngeal cancer patients can be aperiodic and variable , with a large percentage of speech samples being excluded from the analysis [ 11 , 15 ]  . due to the retrospective design , most of the studies lack multidimensional or objective assessment . 
a recent interesting study suggests the use of the electroglottography as an objective voice assessment in irradiated patients to overcome the limits of the self - assessment methods ( vhi )  . 
this study demonstrated improvement of many key parameters over a 12 - month period in 25 patients with t1 / t2 glottic cancer who underwent radical radiotherapy [ 44 ] ; further studies to validate this technique and its cost / effectiveness ratio should be provided . in our study , only a subset of the whole patient series agreed to answer the questions ( administered by phone calls or during follow - up clinical visits )  . 
thus , despite this , the results in terms of functional outcomes are dramatically in favor of radiotherapy , starting from the analysis of the individual questions ( that clinicians can address to consider the value of single symptoms for clinical evaluation ) and above all for the overall physical , functional , and environmental components of the test . in conclusion , this study confirms the well - known issue about equivalent oncologic results of radiotherapy and surgery in early glottic cancer treatment . 
furthermore , it enhances the role of a patients preference in the treatment modality choice and the value of a multidisciplinary approach , through the tumor board , to a detailed and multi - oriented discussion with the patient , while taking into account the better results obtained in terms of quality of voice when using the radiotherapic approach . strahlentherapie und onkologie original article radiotherapy in early - stage dupuytrens contracture long - term results after 13 years nicolas betz1 , oliver j . 
ott1 , boris adamietz2 , rolf sauer1 , rainer fietkau1 , ludwig keilholz1 , 3 background and purpose : in early - stage dupuytrens contracture , radiotherapy is applied to prevent disease progression . 
 long - term outcome and late toxicity of the treatment were evaluated in a retrospective analysis . patients and methods : between 12 / 1982 and 02 / 2006 , 135 patients ( 208 hands ) were irradiated with orthovoltage ( 120 kv ; 20 ma ; 4 - mm al filter ) , in two courses with five daily fractions of 3.0 gy to a total dose of 30 gy ; separated by a 6to 8 - week interval . 
long - term outcome was analyzed at last follow - up between 02 / 2008 and 05 / 2008 with a median follow - up of 13 years ( range , 225 years )  . 
late treatment toxicity and objective reduction of symptoms as change in stage and numbers of nodules and cords were evaluated and used as evidence to assess treatment response . results : according to the individual stages , 123 cases ( 59% ) remained stable , 20 ( 10% ) improved , and 65 ( 31% ) progressed . 
radiotherapy did not increase the complication rate after surgery in case of disease progression and only minor late toxicity ( skin atrophy , dry desquamation ) could be observed in 32% of the patients . 
 there was no evidence for a second malignancy induced by radiotherapy . conclusion : after a mean follow - up of 13 years radiotherapy is effective in prevention of disease progression and improves patients symptoms in early - stage dupuytrens contracture ( stage n , n / i )  . 
in case of disease progression after radiotherapy , a salvage operation is still feasible . key words : dupuytrens contracture benign diseases radiotherapy long - term results strahlenther onkol 2010 ; 186 : 8290 doi 10.1007 / s00066 - 010 - 2063 - z radiotherapie in den frhstadien des morbus dupuytren . 
in einer aktuellen retrospektiven analyse wurden der langzeiterfolg sowie die nebenwirkungen untersucht . patienten und methodik : im zeitraum von 12 / 1982 bis 02 / 2006 wurden 135 patienten mit 208 erkrankten hnden am orthovoltgert ( 120 kv ; 20 ma ; 4 - mm - al - filter ) in zwei serien ( 68 wochen pause ) mit je 5 3 , 0 gy bis zu einer gesamtdosis von 30 gy bestrahlt . 
 die sptnebenwirkungen und das therapieansprechen hinsichtlich der vernderungen des erkrankungsstadiums sowie der anzahl der knoten und strnge wurden erfasst . ergebnisse : unter bercksichtigung des ausgangsstadiums zeigte sich bei 123 hnden ( 59% ) eine befundstabilitt , 20 hnde ( 10% ) verbesserten sich , whrend 65 hnde ( 31% ) eine verschlechterung im stadium erlitten . 
die radiotherapie fhrte nicht zu einer erhhten komplikationsrate nach einer bei progression durchgefhrten operation ; es zeigten sich nur geringgradige sptnebenwirkungen ( hautatrophie oder trockenheit mit schuppung ) bei 32% der patienten . 1department of radiation oncology , university hospital erlangen , germany , 2radiologic institute , university hospital erlangen , germany , 3department of radiotherapy , klinikum bayreuth gmbh , germany . received : july 20 , 2009 ; accepted : october 26 , 2009 published online : january 28 , 2010 strahlenther onkol 2010 no . 
radiotherapy in dupuytrens contracture schlussfolgerung : auch nach einer medianen nachbeobachtungszeit von 13 jahren erweist sich die radiotherapie als effektive manahme zur verhinderung einer weiteren progression in den frhstadien der erkrankung ( stadium n und n / i )  . 
im fall einer progression ist eine salvage - operation ohne erhhte nebenwirkungen mglich . schlsselwrter : morbus dupuytren gutartige erkrankungen radiotherapie langzeitresultate introduction dupuytrens contracture is an inherited proliferative connective tissue disorder which involves the palmar fascia of the hand . 
in early stage of the disease subcutaneous nodules appear followed by tough cords , both with possible fixation to the overlying skfurther disease progression is characterized by retraction of the palmar fascia and contracture of the medial phalangeal ( mp ) and proximal interphalangeal ( pip ) finger joints preferably involving the fourth and fifth fingers . 
at present , typical interventions are a transection of cords ( fasciotomy ) or an excision of diseased fascial bands ( fasciectomy ) with or without excision of the overlying skin [ 32 ]  . 
the aims of surgery are to reverse digital contractures and to restore hand function [ 3 ]  . in early stage of dupuytrens contracture a wait - and - see strategy is preferred , no conservative treatment has been firmly established . 
in one study an average of 3.2 local injections of glucocorticoids lead to a significant disease regression [ 13 ] but also to severe complications like atrophy at the injection site or rupture of the flexor tendon and have no long - term impact on disease progression . 
without any therapy , progression is observed in about 50% of patients after a follow - up of 6 years [ 19 ]  . radiotherapy has been reported to be effective for prevention of disease progression in early stages with only mild acute or late side effects ( rtog grade 1 / 2 ) [ 1 , 11 , 12 ]  . 
 the progression of dupuytrens contracture may be slowly , some cases show stabilization or even spontaneous regression ; therefore , a possible therapeutic effect of any treatment should be assessed in long - term follow - up . 
as hand surgeons still critically discuss the results and side effects of prophylactic radiotherapy , it was necessary to reevaluate the long - term efficacy and late effects of radiotherapy with a median follow - up of 13 years . patients and methods patient characteristics from 12 / 1982 to 02 / 2006 , 230 patients with clinically evident and progressive early - stage dupuytrens contracture were treated at our institute . 
after clinical examination and counseling with informed consent [ 28 ] , 178 patients received the prescribed irradiation and were contacted for a follow - up examination ; 135 patients completed all examinations , 31 were dead , and twelve refused last follow - up for personal reasons . 
last follow - up was performed between 02 / 2008 and 05 / 2008 . pretherapeutic disease symptoms were found in 87 / 135 patients ( 64% ) , eight patients with dysesthesia , 34 with burning / itching , and 45 with pressure / tension . predisposition a structured questionnaire ( appendix i ) and clinical consultation were used for identifying predisposing factors : a positive family history in 38% of cases ( 78 / 208 ) with 37% males ( 47 / 127 ) and 38% females ( 31 / 81 ) , morbus ledderhose in 11.5% of cases ( 24 / 208 ) , peyronies disease in 8.7% of male patients ( 11 / 127 ) and knuckle pads in 2.4% of cases ( 5 / 208 ) , diabetes mellitus in 17% of the cases ( 35 / 208 ) , and alcoholism in 4% . the time period from first recognition of typical symptoms until onset of radiotherapy was 112 , 1324 , 2536 , 3748 , and > 48 months in 28% , 19% , 15% , 14% , and 23% of patients , respectively . pretreatment 9 / 135 patients ( 6.7% ) had received a treatment before irradation : eight patients were sent to radiotherapy with a recurrence of dupuytrens contracture after surgery and one patient with progressive disease after local corticoid therapy . clinical evaluation the stage of disease , the number and consistency of pal pable nodules and cords were carefully analyzed using a standardized procedure and documentation form ( appendix ii ) to assess the long - term response to radiotherapy at actual follow - up . 
functional changes and the total flexion deformity of fingers were measured using a protractor ; degrees of flexion deformity of mp , pip and dip ( distal interphalangeal ) joints strahlenther onkol 2010 no . 
due to stage of disease , treatment outcome was defined as regression , stable or progression and was differentiated into in - field or out - field progression or both . 
verteilung der knoten und strnge vor beginn der radiotherapie ( rt )  . radiotherapy stage pre - rt numbers of nodules / cords 311 n / i 100 152 iii radiotherapy was carried out with 120 - kv photons , 20 ma , and a 2 - mm aluminum filter ( stabilipan ; siemens co . , erlangen , germany )  . 
a 6 8 cm cone with a focus - skin distance of 40 cm was used , and the whole afflicted area with all palpable nodules and cords were included into the irradiation field . 
uninvolved areas of the palm were shielded by placing 3 - mm lead rubber plates with a margin to the palpable nodules and cords of 12 cm distally / proximally and 1 cm laterally . 
 all recommended radiation protection measures were applied especially to minimize cancer risk from radiotherapy [ 26 , 33 ]  . 3% 3% regression status idem progression 112 months > 48 months 1324 months 2536 months 3748 months figure 1 . 
einfluss der anamnesedauer auf den langzeiteffekt der radiotherapie . radiotherapy was prescribed in two separate courses of five daily fractions of 3.0 gy each to a total dose of 30 gy . 
the interval between the two courses was 6 weeks and radiotherapy dose was individually prescribed with the skin surface as the reference dose level . results long - term results with regard to stage a total of 143 / 208 afflicted hands ( 69% ) had no progression of stage according to the classification system after a median follow - up of 13 years . 
in 65 cases ( 31% ) a progression was demonstrated with 14% , 3% , and 14% of cases in - field only , out - field only , and inand out - field , respectively . 
radiotherapy in dupuytrens contracture the initial stage of the disease the changes in stage are summarized in table 3 . the time period from first recognition of typical symptoms until onset of radiotherapy significantly influenced long - term effects of radiotherapy : patients with progressive disease irradiated within the 1st year of diagnosis showed significant better long - term results compared to those treated after 48 months ( p < 0.001 ; figure 1 )  . long - term results with regard to number of nodules and cords a total of 88 / 208 hands ( 42% ) progressed in terms of the number of nodules and cords , the new nodules or cords were localized in - field only in 16% , out - field only in 10% , and inand out - field in 16% of cases . 
2 patients complaints and symptoms patients complaints and symptoms were relatively minor , such that 58 / 87 patients ( 66% ) experienced a partial or complete relief of symptoms ( table 5 )  . treatment toxicity late effects within the irradiated area only minor long - term radiogenic skin and subcutaneous changes were found in 66 / 208 cases ( 32% ) ; 47 cases ( 23% ) had dry skin and increased desquamation ( grade 1 / 2 ) , 14 cases ( 7% ) skin atrophy with occasional telangiectasia ( grade 2 ) and five cases ( 2% ) with an erythema up to 1 year . 
no induction of cancer could be detected at last follow - up . due to progression of disease 39 / 65 patients ( 42 cases ) experienced a surgical procedure ; in two cases ( 5% ) a delayed wound healing was observed . 
20 cases demonstrated a stable disease postoperatively , 22 cases were progressive with increasing flexion deformity . discussion dupuytrens contracture is characterized by the appearance of nodules of hyperproliferative cells , i.e. , fibroblasts and myofibroblasts , within the palmar fascia . 
 during the course of the disease large bands of contracted and collagen - rich fibrotic tissue arise with an increasing flexion deformity of the affected fingers , if left untreated . fibroblasts are believed to play an important role in the genesis of dupuytrens contracture , and the proliferation process of fibroblasts is one of the hallmarks of the disorder [ 4 , 20 ]  . 
they found a downregulation of three genes , encoding for components of the extracellular matrix ( proteoglycan 4 , fibulin - i transcript variant d , and collagen i type xv )  . 
these candidate genes were analyzed in order to find molecular targets for alternative therapies in the future . the treatment of choice in symptomatic stage is surgery , but no specific surgical approach has proven to be consistently more effective than others . 
recurrence due to the trauma associated with surgery is common in up to 60% of the cases with a progressive scar contracture and , additionally , a complication rate of about 19% in the early postoperative period [ 32 ]  . 
hence there is a rationale for radiotherapy in early stage to prevent disease progression and a functional deficit in later times even after surgery . radiotherapy is a well - accepted therapy option in different hyperproliferative [ 8 , 16 , 22 , 29 ] or inflammatory [ 2 , 7 , 9 , 31 ] benign diseases , but the underlying radiobiological mechanism cannot easily be explained . 
proliferating fibroblasts / myofibroblasts are radiosensitive cells and the induction of free radicals by radiotherapy impairs their proliferative activity and thereby reduces the cell density [ 21 ]  . the potential of radiotherapy to stabilize progression of disease was shown in several studies [ 5 , 6 , 14 , 18 , 35 ] , but most of them had a follow - up of only a few years . 
this is important because surgeons are discussing radiotherapy very critically for different reasons , i.e. , long - term inefficacy [ 17 , 36 ] or possible complicated surgery after radiotherapy [ 5 ]  . after 13 - year follow - up , 69% of the cases showed no progression of stage and demonstrate the long - term efficacy of radiotherapy compared to the expected 50% progression rate for untreated patients or patients operated for advanced stages ( table 6 )  . 
nevertheless , the follow - up was only 12 months and long - term follow - up is warranted to demonstrate long - term stability for the low - dose group . in our study , we could show that patients with progressive disease irradiated within the 1st year of diagnosis showed significantly better long - term results ; nonetheless , radiotherapy should be performed only in case of progressive disease over a follow - up period of at least 6 months and when the extent of the disease can be estimated more reliably for target volume definition . conclusion radiotherapy for early - stage dupuytrens contracture is effective in long - term follow - up with acceptable late toxicity . 
schild3 , dirk rades1 background and purpose : whole - brain radiotherapy ( wbrt ) alone is the most common treatment for brain metastases from colorectal cancer , as most patients are not candidates for more aggressive therapies such as resection or radiosurgery . 
this study investigated whether an escalation of the wbrt dose improves these results . patients and methods : data from 53 patients receiving wbrt alone for brain metastases from colorectal cancer were retrospectively analyzed . 
 diese studie untersucht , ob eine dosiseskalation zu einer verbesserung der ergebnisse fhrt . patienten und methodik : daten von 53 patienten , die eine alleinige wbrt bei metastasen eines kolorektalen karzinoms erhalten hatten , wurden retrospektiv ausgewertet ( tabelle 1 )  . 
zustzlich wurden folgende mgliche prognosefaktoren untersucht : alter , geschlecht , allgemeinzustand , anzahl der hirnmetastasen sowie vorliegen extrazerebraler metastasen . ergebnisse : die raten fr das os nach 6 monaten betrugen 17% nach 10 3 gy und 50% nach 20 2 gy / 15 3 gy ( p = 0 , 014 ; tabelle 2 , abbildung 1 )  . 
in der multivarianzanalyse war ein besseres os signifikant mit hherer dosis ( p = 0 , 047 ) , besserem allgemeinzustand ( p = 0 , 034 ) , vorliegen von weniger als vier hirnmetastasen ( p = 0 , 036 ) und nichtvorliegen extrazerebraler metastasen ( p = 0 , 010 ) assoziiert . 
ein trend zeigte sich fr einen besseren allgemeinzustand ( p = 0 , 08 ) und weniger als vier hirnmetastasen ( p = 0 , 06 )  . schlussfolgerung : patienten mit hirnmetastasen eines kolorektalen karzinoms , die eine alleinige wbrt erhalten , scheinen von einer dosiseskalation ber 10 3 gy hinaus zu profitieren . schlsselwrter : kolorektales karzinom hirnmetastasen dosiseskalation gesamtberleben lokale kontrolle 1department of radiation oncology , university hospital schleswig - holstein , lubeck , germany , 2department of radiation oncology , university hospital hamburg - eppendorf , hamburg , germany , 3department of radiation oncology , mayo clinic , scottsdale , az , usa . received : july 16 , 2009 ; accepted : november 9 , 2009 published online : january 26 , 2010 strahlenther onkol 2010 no . 
however , due to improved systemic treatment of colorectal cancer , more of these patients are likely to live long enough to experience brain metastases in the near future [ 3 , 25 , 26 ]  . 
thus , it is likely that brain metastases from colorectal cancer will emerge from an almost anecdotal event to a relevant clinical problem [ 3 ]  . the prognosis of most of these patients is extraordinarily poor with median survival times ranging from a few weeks to 4 months after whole - brain radiotherapy ( wbrt ) alone [ 1 , 2 , 7 , 8 , 17 , 18 , 23 , 29 ]  . 
longer survival times can be achieved in carefully selected patients with more aggressive treatment approaches including resection or radiosurgery [ 1 , 79 , 13 , 1921 , 24 , 28 ]  . 
 however , the majority of patients with brain metastases from colorectal cancer are not candidates for such aggressive therapies due to inappropriate tumor location or too many lesions , a poor performance status , or uncontrolled extracerebral disease . 
however , the results achieved with 10 3 gy are generally poor with median overall survival ( os ) times of only a few months and need to be improved [ 1 , 2 , 7 , 8 , 29 ]  . brain metastases from colorectal cancer have been reported to be relatively radioresistant [ 5 ]  . 
thus , one may speculate as to whether an escalation of the wbrt dose beyond 10 3 gy will improve the outcome of patients with brain metastases from colorectal cancer . 
the present study compared 10 3 gy to higher doses such as 40 gy in 20 fractions ( 20 2 gy given in 4 weeks ) or 45 gy in 15 fractions ( 15 3 gy given in 3 weeks ) with respect to os and local ( intracerebral ) control ( lc )  . 
 prognostic factors may aid clinicians in choosing the most appropriate treatment regimen for an individual patient and are important for proper stratification of patients in future studies . patients and methods a total of 53 patients who received wbrt alone for brain metastases from colorectal cancer ( 34 colon cancer and 19 rectal cancer patients ) at two university hospitals between 1989 and 2008 were evaluated in this retrospective study . 
the criteria for inclusion were as follows : brain metastases from colorectal cancer treated with wbrt alone ( 6to 10 - mv photons ) , no prior radiotherapy to the brain , confirmation by computed tomography or magnetic resonance imaging , and administration table 1 . 
the 35 patients who received 30 gy in ten fractions ( 10 3 gy , overall treatment time 2 weeks ) were compared to 18 patients who received higher doses such as 40 gy in 20 fractions ( 20 2 gy , 4 weeks , n = 10 ) or 45 gy in 15 fractions ( 15 3 gy , 3 weeks , n = 8 ) for os and freedom from recurrent brain metastasis ( lc )  . 
all the patients treated at the university hospital of lbeck , germany , received 10 3 gy , whereas at the university hospital of hamburg , germany , the radiation schedule was based on the discretion of the treating physician . 
vergleich von ( 10 3 gy ) versus ( 20 2 gy / 15 3 gy ) fr das gesamtberleben . results the median duration of os was 3 months after 10 3 gy and 5 months after higher doses . 
the os rates at 6 months were 17% and 50% , respectively ( p = 0.014 ; figure 1 ) , and the os rates at 12 months were 17% and 31% , respectively . 
in addition to a higher wbrt dose , improved os was significantly associated with kps 70 ( p < 0.001 ) , presence of less than four brain metastases ( p = 0.003 ) , and lack of extracerebral metastases ( p = 0.001 ) in the univariate analysis . 
in addition to a higher wbrt dose , improved lc was significantly associated with kps 70 ( p = 0.002 ) , presence of less than four brain metastases ( p = 0.007 ) , and lack of extracerebral metastases ( p = 0.018 ) in the univariate analysis . 
presence / absence of extracerebral metastases ( rr : 2.05 : 95% ci : 0.835.89 ; p = 0.12 ) was not significant in the multivariate analysis . acute toxicity grade 2 according to the common toxicity criteria 2.0 [ 27 ] occurred in 6 / 35 patients ( 17% ) who table 2 . 
vergleich von ( 10 3 gy ) versus ( 20 2 gy / 15 3 gy ) fr die lokale kontrolle . received 30 gy in ten fractions compared with 3 / 18 patients ( 17% ) who received greater doses . 
neurocognitive deficits most likely related to wbrt were observed in 2 / 35 patients ( 6% ) who received 30 gy in ten fractions and 1 / 18 patients ( 6% ) who received greater doses . discussion the prognosis of patients with brain metastases from colorectal cancer is quite poor even when compared to patients with strahlenther onkol 2010 no . 
since brain metastases from colorectal cancer have been reported to be considered radioresistant [ 5 ] , more aggressive treatment regimens than wbrt alone such as surgery or radiosurgery have been used for selected patients in order to improve their outcomes [ 79 , 13 , 22 , 28 ]  . 
in the retrospective review of farnell et al . , 39 patients received surgery plus wbrt , eleven patients surgery alone , 79 patients wbrt alone , and 17 patients supportive care alone [ 7 ]  . 
wronski & arbit reported a 1 - year survival rate of 32% following craniotomy in 73 patients treated with resection alone or surgery with up - front or subsequent wbrt [ 28 ]  . 
unfortunately , most patients with brain metastases from colorectal cancer have to be treated with wbrt alone , because they are no candidates for aggressive approaches such as surgery or radiosurgery due to a relatively large number of cerebral lesions , a poor performance status , or uncontrolled extracerebral disease . 
however , to be more certain that these wbrt regimens reflect an escalation of the effective wbrt dose , both the total dose and the dose per fraction must be considered , as the biological effectiveness of irradiation depends on both parameters . 
different radiation schedules can be compared with the equivalent dose in 2 - gy fractions ( eqd2 ) , which takes both the total dose and the dose per fraction into account [ 11 ]  . 
the eqd2 is calculated with the equation eqd2 = d [ ( d + / ) / ( 2 gy + / ) ] , as derived from the linear - quadratic model ; d = total dose , d = dose per fraction , = linear ( first - order dose - dependent ) component of cell killing , = quadratic ( second - order dose - dependent ) component of cell killing , / ratio = the dose at which both components of cell killing are equal . 
thus , the regimens 20 2 gy and 15 3 gy reflect greater effective tumor cell killing power than 10 3 gy . given the limitations of a retrospective study , our results suggest an improvement of both os and lc with an escalation of the wbrt dose . 
the benefit of an escalation of the wbrt dose observed in this study is contradictory to the findings of our preceding study of 416 patients who received wbrt for multiple brain metastases [ 19 ]  . 
in patients with a more favorable survival prognosis , the dose per fraction should be < 3 gy , because doses per fraction of 3 gy have been reported to be associated with an increased risk of neurocognitive deficits [ 6 ]  . alternatively to an escalation of the wbrt dose , the results of wbrt may be improved with the addition of systemic therapies such as gemcitabine , temozolomide or bevacizumab [ 4 , 14 , 16 ]  . 
studies investigating the potential benefit of such combined approaches are needed . in addition to the wbrt regimen , five further potential prognostic factors for os and lc have been investigated including age , gender , performance status , number of brain metastases , and the presence of extracerebral metastases at the time of wbrt . 
patients with a relatively favorable survival prognosis appear better treated with more aggressive treatment approaches including resection or radiosurgery or , if these therapies cannot be administered , with an escalated total wbrt dose including a dose per fraction of < 3 gy [ 6 ]  . conclusion the present study suggests that patients with brain metastases from colorectal cancer who are no candidates for brain surgery or radiosurgery and have to be treated with wbrt alone may benefit from an escalation of the radiation dose beyond standard 10 3 gy . 
these results should be confirmed in a properly designed randomized trial stratifying for the significant prognostic factors such as performance status , number of brain metastases , and extracerebral metastases . strahlentherapie und onkologie original article radiation protection of persons living close to patients with radioactive implants theodor w . 
kaulich1 , michael bamberg2 background : permanent interstitial brachytherapy is in certain cases a very successful therapeutic option , but application of radioactive implants always results in only gradually diminishing radiation exposure of persons in the patients immediate surroundings . material and methods : using patients with clinically localized prostate cancer treated with iodine - 125 ( 125i ) or palladium - 103 ( 103pd ) as an example , it is shown how a patient , if necessary or wished by him , can , by wearing commercially available x - ray protection shorts , reduce radiation exposure of family members in such a way that at a distance r from the patient a given dose per year is not exceeded . results : the computational procedures necessary for the determination of the individual periods of wearing x - ray protection clothing are provided in the form of formulae and graphics . 
all considerations and calculations can also be applied to other radiotherapeutic interventions involving the use of 125i , 103pd or other - sources . conclusion : if necessary , a patient with permanent radioactive implants can reduce radiation exposure of family members by wearing special x - ray protection clothing for a limited period of time . 
this kind of radiation protection is very efficient and considerably simpler to accomplish than a reduction of exposure time or an increase of the distance between the patient and family members . key words : brachytherapy permanent seed implants 125i 103pd radiation protection strahlenther onkol 2010 ; 186 : 10712 doi 10.1007 / s00066 - 010 - 2073 - x strahlenschutz von personen , die mit patienten mit radioaktiven implantaten zusammenleben hintergrund : die permanente interstitielle brachytherapie ist eine sehr erfolgreiche therapeutische option , die aber immer auch mit einer strahlenexposition von personen in unmittelbarer umgebung des patienten verbunden ist . material and methodik : am beispiel von patienten mit prostatakarzinom , die mit jod - 125 ( 125i ) oder palladium - 103 ( 103pd ) behandelt wurden , wird gezeigt , wie der patient durch individuell begrenzte tragedauer kommerziell erhltlicher strahlenschutzhosen die strahlenexposition seiner familienmitglieder , falls erforderlich oder von ihm gewnscht , so limitieren kann , dass im abstand r vom patienten eine vorgegebene dosis pro jahr nicht berschritten wird . ergebnisse : die bentigten berechnungsgrundlagen werden als formeln und grafiken zur bestimmung der individuellen tragedauer der strahlenschutzhosen prsentiert . 
alle berlegungen und berechnungen lassen sich auch auf andere strahlentherapeutische manahmen mit 125i , 103pd oder auch andere - strahler anwenden . schlussfolgerung : ein patient mit radioaktivem permanentimplantat kann durch das zeitlich begrenzte tragen von strahlenschutzhosen die strahlenexposition von familienmitgliedern stark reduzieren . 
diese strahlenschutzmanahme ist sehr wirkungsvoll und wesentlich einfacher anzuwenden als eine reduktion der aufenthaltsdauer oder eine vergrerung des abstands zu familienmitgliedern . schlsselwrter : brachytherapie seedimplantation 125i 103pd strahlenschutz 1medical physics , university hospital of radiooncology , tbingen , germany , 2university hospital of radiooncology , tbingen , germany . received : august 20 , 2009 ; accepted : october 5 , 2009 published online : january 28 , 2010 strahlenther onkol 2010 no . 
radiation protection of persons living close to patients with radioactive implants introduction the use of radioactive implants ( iodine - 125 [ 125i ] or palladium - 103 [ 103pd ] seeds ) has been increasing rapidly all over the world for the last 15 years . 
it is estimated that more than 50 , 000 patients with clinically localized prostate cancer are treated with 125i or 103pd seeds every year worldwide and this number is anticipated to increase in the near future [ 1 , 4 , 6 , 9 , 11 , 1417 , 21 ]  . 
temporary episcleral 125i eye plaque radiotherapy of uveal melanoma is also an established therapy for medium - sized choroidal melanomas which allows control of the tumor , sparing of vision , and preservation of the globe in most cases [ 12 ]  . 
a permanent breast seed implant technique ( pbsi ) using 125i or 103pd seeds has also been developed as a new form of adjuvant partial radiation therapy for early - stage breast cancer [ 7 , 13 ]  . permanent interstitial brachytherapy is in certain cases a very successful therapeutic option , but application of radioactive implants always results in only gradually diminishing radiation exposure in the patients immediate surroundings . the patient has three ways to minimize the radiation hazards / reduce the radiation exposure of family members or carers : he can reduce the exposure time , increase the distance , or use temporary shielding between himself and other people . 
the last method of using temporary shielding is presented below . material and methods in the eu council directive 96 / 29 / euratom ( basic safety standards ) , the essential contents of the icrp 60 [ 5 ] recommendation had been adopted . 
in special circumstances , however , a higher effective dose may be authorized in a single year , provided that the average over 5 consecutive years does not exceed 1 msv / a . 
germany did not make use of the possibility allowed by the euratom directive to authorize a higher effective dose in a single year provided that the average over 5 years does not exceed 1 msv ; 1 msv is a strict dose limit which has to be kept every single year . 
following the german guideline for radiation protection in medicine the hospital is authorized to discharge patients treated with radionuclides if at a distance of 2 m from the patient the dose per year does not exceed 1 msv . now some publications are available which provide interesting and important data on radiation protection for 125i and 103pd permanent implants . 
these data [ 2 , 3 , 6 , 8 , 10 , 18 ] support the conclusion that patients treated with these implants do not represent a radiation risk to members of the public . 
as regards family members and close friends or carers , it must be taken into account , however , that for these persons there may result dose rate values due to smaller distances and considerably longer periods of contact that lead to radiation exposures exceeding , e.g. , 1 msv per calendar year [ 2 , 7 , 8 ]  . 
especially the rare case where the patients partner is pregnant or the patient has to take care of grandchildren after the time of implantation may need specific precautions . the largest group of patients with radioactive implants are patients with clinically localized prostate cancer who are treated with 125i . 
using this group of patients as an example , it is shown how , by wearing commercially available x - ray protection shorts for an individually determined period , radiation exposure of family members and close friends or carers can be limited . 
this delayed radiation protection measure may result , e.g. , from the fact that for technical reasons the x - ray protection shorts are not available immediately . the effective dose or the individual body dose of the family members is always assessed with the help of the measured area dose . for the calculation of the wearing span of x - ray protection shorts , the following parameters are used : t1 / 2 half - life of the used radionuclide , = ln , decay constant , hvl half - value layer ( mm pb ) of the used radionuclide , lev lead - equivalent value ( mm pb ) of the x - ray protection clothing ,  . 
with transmission factor of the x - ray protection clothing , r distance between patient and any person , t time , t = 1 year , strahlenther onkol 2010 no . 
immediately after seed implantation , then , during the time span t0 the patient is not wearing x - ray protection shorts , thereafter , during the time span t0 until t1 , he is wearing x - ray protection shorts , and finally , during the time span t1 until t he is again not wearing x - ray protection shorts . 
with 200 patients the mean dose rate at 50 cm from the posterior skin case 1 : without x - ray protection shorts and with f = 1 or f = 8 h / 24 h after 1 year the area dose at 50 cm results in 13 msv ( equation 1 ) and 4.3 msv , respectively ( figure 1 : example case 1 )  . case 2 : if the x - ray protection shorts with lev = 0 , 17 mm are worn immediately after seed implantation , there can be calculated according to equation ( 5 ) the wearing span which is necessary in order not to exceed the value of 1 msv / a . 
the x - ray protection shorts have to be worn according to equation ( 9 ) ( 22315 ) days = 208 days in order not to exceed the value of 1 msv / a . 
 in the above example ( 6.4 sv / h at 50 cm and f = 8 h / 24 h ) , without the wearing of x - ray protection shorts 1 msv / a is reached already 22 days after seed implantation . example case 1 example case 2 example case 3 for case 2 , the curves in figure 2 for 125i implants and in figure 3 for 103pd implants were computed from equation ( 5 )  . 
these graphs show the number of days x - ray protection shorts with lev = 0.17 mm have to be worn in order to limit the accumulated dose after 1 year at the distance r to 0.5 , 1 , 2 , 5 , or 10 msv / a given an area dose rate a of up to 10 sv / h immediately after seed application . 
in the majority of cases , an occupancy factor f has to be taken into account , as described above . the following example from the literature is to demonstrate the simple use of the graphic representation strahlenther onkol 2010 no . 
diagramm fr ein beispiel aus der literatur [ 2 ] , das die drei diskutierten mglichkeiten fr f = 8 h / 24 h zeigt . 125i 103pd kaulich tw , bamberg m . 
diagram for 125i for the determination of the period of application of x - ray protection shorts ( lev = 0.17 mm ) dependent on area dose a at a distance r ( case 2 )  . 
diagramm fr 125i zur ermittlung der tragezeit von strahlenschutzhosen ( lev = 0 , 17 mm ) in abhngigkeit von der limitierenden dosis a im abstand r ( fall 2 )  . 
the maximum measured dose to a spouse was 5.1 msv / a at 1 this area dose is produced by about 8.5 sv / h at 1 from figure 3 there results that x - ray protection clothing has to be worn for 40 days so that the area dose be 1 msv / a at 1 for f = 8 h / 24 h and 2.8 sv / h at 1 m from figure 2 there results a wearing span of only 13 days in order to obtain an area dose of 1 msv / a at 1m . brachytherapy with radioactive permanent implants is in certain cases a suitable therapeutic option for a patient . 
 [ 7 ] rejected , for instance , the possibility of using special x - ray clothing in the case of pbsi and proposed / recommended the exclusive use of 103pd , 103pd seeming to be safe because the patients partners effective dose is consistently < 5 msv . 
as our computations have shown , it is equally possible in the case of pbsi to use 125i if there is worn special x - ray protection clothing for a limited period of time . the radiation protection measure presented above is very efficient and considerably simpler to implement than a reduction of the exposure time or an increase of the distance between the patient and other people . strahlentherapie und onkologie current discussion degro practical guidelines for palliative radiotherapy of breast cancer patients : brain metastases and leptomeningeal carcinomatosis petra feyer1 , marie - luise sautter - bihl2 , wilfried budach3 , jrgen dunst4 , wulf haase5 , wolfgang harms6 , felix sedlmayer7 , rainer souchon8 , frederik wenz9 , rolf sauer10 purpose : to provide recommendations for palliative treatment of brain metastases ( bm ) and leptomeningeal carcinomatosis ( lc ) in breast cancer patients with specific emphasis on radiooncologic aspects . methods : the breast cancer expert panel of the german society of radiation oncology ( degro ) performed a comprehensive survey of the literature comprising national and international guidelines , lately published randomized trials , and relevant retrospective analyses . 
 recommendations were devised according to the panels interpretation of the evidence referring to the criteria of ebm . results : aim of any treatment of bm and lc is to alleviate symptoms and improve neurologic deficits . 
close interdisciplinary cooperation facilitates rapid diagnosis and onset of therapy , tailored to the individual and clinical situation . treatment decisions for bm should be based on the allocation to three prognostic groups defined by recursive partitioning analysis ( rpa )  . 
together with the extent of the disease , kps determines whether excision or radiosurgery / stereotactic radiotherapy is feasible and if exclusive or additional whole - brain radiotherapy ( wbrt ) is indicated . 
with adequate therapy , survival may be up to 3 years . for lc , treatment is mostly indicated for patients with positive cytology or in case of strongly indicative signs and symptoms . 
radiotherapy ( wbrt and involved - field irradiation of bulky spinal lesions ) and chemotherapy ( systemically or intrathecally applied methotrexate , thiotepa and cytarabine ) are both effective and may prolong survival from several weeks to 46 months . conclusion : radiotherapy is an effective tool for palliative treatment of bm and lc . key words : palliative treatment breast cancer brain metastases leptomeningeal carcinomatosis radiotherapy strahlenther onkol 2010 ; 186 : 639 doi 10.1007 / s00066 - 010 - 2100 - y degro - handlungsleitlinie zur strahlentherapie von hirnmetastasen und der leptomeningealen karzinomatose bei mammakarzinompatientinnen ziel : erstellung einer klinischen leitlinie zur palliativen therapie von hirnmetastasen und leptomeningeosis carcinomatosa beim mammakarzinom unter spezieller bercksichtigung radioonkologischer aspekte . 
diese soll eine vereinheitlichung des vorgehens und somit eine verbesserung der behandlungsqualitt ermglichen . methodik : die expertengruppe mammakarzinom der deutschen gesellschaft fr radioonkologie ( degro ) fhrte eine umfassende literaturrecherche durch , die nationale und internationale leitlinien , randomisierte studien und relevante retrospektive analysen im publikationszeitraum von 1995 bis 2008 bercksichtigte ( pubmed , guidelines international network [ g - i - n ] )  . 
die empfehlungen wurden entsprechend den jeweils vorliegenden evidenzen nach ebm - kriterien gewichtet . 1klinikum neuklln , berlin , germany , 2municipal hospital , karlsruhe , germany , 3university hospital dsseldorf , germany , 4university hospital schleswig - holstein , germany , 5formerly st . 
clara hospital , basel , switzerland , 7 university hospital , landeskrankenhaus salzburg , austria , 8university hospital tbingen , germany , 9department of radiation oncology , university medical center mannheim , germany , 10university hospital erlangen , germany . 
guidelines for the treatment of bm and lc in breast cancer ergebnisse : ziele jeglicher behandlung von hirnmetastasen und leptomeningeosis carcinomatosa sind die linderung entsprechender symptome und verminderung neurologischer defizite . 
eine enge interdisziplinre zusammenarbeit ermglicht eine rasche diagnose und den umgehenden beginn einer therapie , die individuell auf die persnliche und klinische situation zugeschnitten sein sollte . bei hirnmetastasen orientiert sich die therapieentscheidung an der zuordnung zu drei prognostischen gruppen , die mit dem verfahren der recursive partitioning analysis ( rpa ) der rtog definiert wurden . 
hier ist der karnofsky - performance - status wichtigster prognostischer parameter , der zusammen mit der tumorausdehnung zur entscheidung beitrgt , ob eine exzision , eine radiochirurgische / stereotaktische strahlentherapie oder eine alleinige bzw . 
mit adquater behandlung kann ein berleben bis zu 3 jahren erzielt werden . die behandlung der meningeosis carcinomatosa ist zumeist bei positiver liquorzytologie oder im fall einer eindeutigen klinischen symptomatik indiziert . 
eine ganzhirnbestrahlung und eine umschriebene strahlentherapie befallener spinaler manifestationen sowie eine entweder systemisch oder intrathekal applizierte chemotherapie ( methotrexat , thiotepa , cytarabin [ depocyte ] ) sind wirksamit einer effektiven behandlung kann das berleben von wenigen wochen auf 46 monate verlngert werden . schlussfolgerung : die strahlentherapie stellt eine effektive palliativmanahme in der therapie von hirnmetastasen und meningeosis carcinomatosa dar . 
 schlsselwrter : palliative behandlung brustkrebs hirnmetastasen leptomeningeale karzinomatose radiotherapie introduction breast cancer is the second most common cause for brain metastases ( bm ) occurring with increasing incidence to be 1040% of patients who develop distant disease , parenchymal metastases are found at autopsy in 3040% , and leptomeningeal central nervous system ( cns ) metastases in 516% [ 5 , 59 ]  . 
 standard therapy has not been established and there is a large spectrum of treatment regimens but only a small number of practice guidelines [ 4 , 39 , 42 , 62 , 65 ] which refer to all primary tumor entities . 
in order to specify these guidelines for breast cancer treatment , the respective expert panel of the german society of radiation oncology ( degro ) conducted a comprehensive survey of the literature comprising the above guidelines , lately published randomized trials , and relevant retrospective studies . 
aim of the present paper is to provide recommendations for the palliative treatment of bm and lc in breast cancer patients with specific emphasis on radiooncologic aspects , complementing the previous recommendations for adjuvant as well as palliative radiotherapy of breast cancer [ 57 , 58 , 63 ]  . clinical presentation and prognosis according to the anatomic site of the lesions , neurologic symptoms of both bm and lc are headache , signs of intracranial pressure , motor weakness , seizures , cognitive deficits , and mental dysfunction . 
untreated patients with lc have a median survival of only 46 weeks , however , adeqate therapy may prolong survival to > 6 months and achieve a 1 - year survival rate of up to 25% [ 8 , 13 ]  . 
performance status is the most important prognostic factor [ 14 ]  . for bm , the rtog defined three prognostic subgroups on the basis of data from 1 , 200 patients using the recursive partitioning analysis ( rpa )  . 
 [ 51 ] established a new scoring system to predict survival after whole - brain radiotherapy ( wbrt ) on the basis of a multivariate analysis of 1 , 085 patients . 
guidelines for the treatment of bm and lc in breast cancer diagnostic evaluation for bm , the diagnostic procedure is focused on clinical symptoms ; most commonly , computed tomography ( ct ) and magnetic resonance imaging ( mri ) are used . 
if specific local treatment such as surgery or stereotactic radiotherapy is an option , mri is superior to ct for delineation of metastases and detection of multiple lesions . differential diagnosis of lc may be difficult [ 3 , 4 ] , as cerebrospinal fluid ( csf ) cytology may be false - negative in up to 20% of the patients [ 13 , 39 ]  . 
mri of the complete craniospinal axis with gadolinium enhancement is the imaging technique of choice and should be performed prior to lumbar puncture , as this procedure may induce contrast medium enhancement and thus may compromise imaging accuracy [ 39 ]  . treatment goals aim of the treatment is to improve or stabilize the neurologic status , maintain or regain quality of life , and , optimally , prolong survival . 
any treatment decision should be based on the predominant symptoms and the probability of extra - cns tumor control . corticosteroids have a limited value in lc - related neurologic symptoms but can be useful to treat vasogenic edema associated with intraparenchymal or epidural metastases [ 13 ]  . prophylactic administration of anticonvulsant drugs is not recommended ; when necessary , interactions with other drugs such as chemotherapeutic agents or steroids have to be taken into consideration and dose monitoring is mandatory . 
 regarding metabolic interactions , valproinate seems to be superior to other drugs when combined with chemotherapy [ 24 ]  . in patients with low performance status ( kps < 50% ) for whom specific tumor treatment is not indicated and steroids are not effective , pain medication and sedative treatment should be administered as supportive care . solitary brain metastasis there are no randomized studies or data permitting a definite conclusion whether surgery and stereotactic radiotherapy are equally effective . 
 therefore , treatment decision should be made individually regarding anatomic localization and size of the lesion , amenability to surgery , acute clinical risk , and patients preference . treatment options factors in favor of primary surgery : treatment choice for bm is based on clinical symptoms and verification in diagnostic imaging . 
in asymptomatic patients , the decision depends on the individual situation : for patients in rpa class i , specific treatment is mandatory , whereas in patients with rpa class iii , symptomatic therapy may be preferable . 
in case of a long recurrence - free interval and lack of extracerebral tumor spread , histological verification should be considered prior to treatment [ 66 ]  . in contrast to bm , lc is substantially less common , thus , literature is sparse and only a small number of studies mostly nonrandomized have been published . 
treatment of lc is preferentially multidisciplinary and mostly indicated when the diagnosis is unequivocal or symptoms are strongly suggestive in case of negative cytology ( see above )  . symptomatic treatment histological verification after a long recurrence - free interval ; need for immediate decompression in case of rapidly developing clinical deterioration or life - threatening symptoms ; tumor size > 3.5 cm and surgically favorable location ; surgery + wbrt + stereotactic radiosurgery boost [ 53 ]  . factors in favor of primary radiotherapy : rpa class ii ; no need for rapid decompression ; short recurrence - free interval ; no need for histological verification due to unambiguous medical history ( e.g. , additional metastatic spread ) ; high risk of surgery ; tumor location poorly amenable to surgery . systemic application of corticosteroids is the standard treatment for brain edema . 
 doses of 4 , 8 , or 16 mg showed equivalent effectiveness after 1 week of medication ; however , side effects after 4 weeks were more pronounced with 16 mg . 
as symptoms may recur in case of rapid reduction , the dose should be reduced stepwise over a period of 4 weeks . wbrt following surgery [ 41 ] , stereotactic radiotherapy or radiosurgery [ 56 ] may improve outcome of patients with a single bm who have favorable prognostic factors and a kps of at least 70% without extracranial tumor spread ( rpa class i ) or patients with rpa class ii and metastases limited to the skeletal system ( figure 1 )  . 
after the onset of bm in her2 - positive breast cancer patients , additional trastuzumab therapy is associated with a significant survival benefit compared with patients who never received or completed trastuzumab before the bm diagnosis [ 48 ]  . + extensive extracerebral metastases wbrt 10 3 gy or 5 4 gy figure 1 . 
 two or three brain metastases resection or stereotactic radiotherapy may be considered [ 1 ( loe 2b ) , 35 ( loe 1b ) ] , additional wbrt further improves local tumor control [ 52 ] ( figure 1 )  . 
the neurologic symptoms , kps , extracranial tumor control , and the patients desire are relevant criteria for the treatment decision [ 72 ( loe 4 ) ]  . whole - brain radiotherapy of more than three brain metastases radiotherapy and chemotherapy in leptomeningeal carcinomatosis wbrt is the standard treatment ( figure 1 )  . 
several rtog studies investigated different fractionation schedules [ 10 ( loe 1b ) , 11 ( loe 1b ) , 23 ( loe 1b ) , 37 ( loe 1b ) , 43 ] and found a median survival time of 36 months irrespective of fractionation . 
a boost up to 54.4 gy did not yield better results [ 43 ( loe 1b ) ] , neither did additional excision or radiosurgery . according to the sparse data , both treatment modalities are effective in lc . 
a subgroup analysis of one of these studies , comprising breast cancer patients only , yielded a median survival of 88 days and a 1 - year survival rate of 19% . 
 intrathecal chemotherapy is effective for diffuse meningeal spread , however , may be ineffective in bulky disease , as drug permeation does not exceed 23 mm [ 12 ]  . 
effectiveness of intrathecal versus systemic treatment was analyzed and no advantage was found for the more invasive method , leading to the conclusion that systemic chemotherapy and irradiation should be preferred because of their lower toxicity [ 9 ]  . 
case studies reported remissions of lc after oral chemotherapy with capecitabine [ 55 ] and endocrine treatment [ 7 ]  . radiotherapy technique and dose for wbrt , the clinical target volume encompasses the cerebrum plus cerebellum and brain ste in case of leptomeningeal manifestation and infratentorial metastases , the treatment volume should include the spinal cord down to the caudal margin of the second vertebral body . 
in patients with a predicted survival exceeding 12 months , reduction of the single fraction to 2 gy may be preferable ( 20 2 gy ) [ 62 ] in order to reduce brain toxicity [ 19 ]  . 
 these recommendations apply to both , bm and lc . lc with spinal manifestations : the clinical target volume encompasses the gross tumor volume with a safety margin which is matched to the individual clinical requirements . 
dose recommendations are as described above . stereotactic radiosurgery : for stereotactic irradiation , the gross tumor volume in mri is regarded as clinical target volume , an additional safety margin of 12 mm for the planning target volume is recommended , depending on reproducibility and immobilization technique . 
dose prescription refers to the 8090% isodoses . fractionated stereotactic radiotherapy is feasible for tumors > 2 cm and lesions in critical anatomic sites such as the cerebellum with increased risk of incarceration . 
dose specification refers to icru report 50 [ 32 ]  . strahlentherapie und onkologie original article overexpression of caveolin - 1 in lymphoblastoid tk6 cells enhances proliferation after irradiation with clinically relevant doses david barzan1 , patrick maier1 , w . 
jens zeller2 , frederik wenz1 , carsten herskind1 background and purpose : the transmembrane protein caveolin - 1 ( cav1 ) is an essential component of caveolae , small membrane invaginations involved in vesicle formation . 
the aim of this work was to test the effect of cav1 overexpression after irradiation in human cells lacking endogenous cav1 expression . material and methods : human cav1 was overexpressed in lymphoblastoid tk6 cells ( tk6 - wt ) using a eukaryotic expression plasmid , pci - cav1 , or a lentiviral sin ( self - inactivating ) vector , hrsin - cav1 . 
this radioprotective effect was supported by a reduction of radiation - induced apoptosis . conclusion : a model system for expression of exogenous cav1 by stable lentiviral transduction of tk6 cells was established . 
 functional assays demonstrated enhanced early proliferation by cav1 expression in tk6 cells after irradiation with clinically relevant doses supporting the role of cav1 as a prosurvival factor . key words : caveolin - 1 radiation lentivirus proliferation lymphoblasts strahlenther onkol 2010 ; 186 : 99106 doi 10.1007 / s00066 - 010 - 2029 - 1 berexpression von caveolin - 1 in lymphoblastoiden tk6 - zellen erhht die proliferation nach bestrahlung mit klinisch relevanten dosen hintergrund und ziel : das transmembranprotein caveolin - 1 ( cav1 ) ist eine essentielle komponente der caveolae , kleiner membraninvaginationen , die an der vesikelbildung beteiligt sind . 
ziel dieser arbeit war es , die effekte der cav1 - berexpression nach bestrahlung in humanen zellen ohne endogene cav1 - expression zu bestimmen . material und methodik : berexpression von humanem cav1 in lymphoblastiden tk6 - zellen ( tk6 - wt ) wurde durch transfektion mit einem eukaryotischen expressionsplasmid ( pci - cav1 ) oder transduktion mit einem lentiviralen sin - ( self - inactivating - ) vektor ( hrsin - cav1 ) vermittelt . 
die lentiviral vermittelte transduktion mit hrsin - cav1 ( tk6 - cav1 ) verursachte eine deutlich strkere cav1 - expression im vergleich zu pci - cav1 - transfizierten tk6 - zellen . 
cav1 verstrkte die frhe 1department of radiation oncology , university medical center mannheim , university of heidelberg , mannheim , germany , 2pharmacology of cancer treatment , german cancer research center , heidelberg , germany . received : april 6 , 2009 ; accepted : october 15 , 2009 published online : january 28 , 2010 strahlenther onkol 2010 no . 
diese radioprotektive wirkung wurde durch eine abnahme strahleninduzierter apoptose untersttzt . schlussfolgerung : ein modellsystem fr die expression von exogenem cav1 durch stabile lentivirale transduktion von tk6 - zellen wurde etabliert . 
funktionelle untersuchungen zeigten eine verstrkte frhe proliferation durch die cav1 - expression nach bestrahlung von tk6 - zellen mit klinisch relevanten dosen , wodurch die rolle von cav1 als berlebensfaktor untersttzt wird . schlsselwrter : caveolin - 1 bestrahlung lentivirus proliferation lymphoblasten introduction caveolae are 50100 nm small invaginations of the plasma membrane involved in vesicle formation , endoand exocytosis [ 17 ]  . 
the main component of caveolae is caveolin - 1 ( cav1 ) , which functions as a scaffold for the accumulation of components of various signaling cascades like endothelial nitric oxide synthase ( enos ) , protein kinase a ( pka ) or transforming growth factor - ( tgf - ) type i and ii receptor [ 20 , 27 , 28 ]  . 
cav1 acts as a modifier of various signaling cascades but the role of cav1 in initiation and progression of cancer is still up to debate [ 7 , 14 , 40 ]  . 
however , other cancer cell lines show a high expression level of cav1 protein [ 34 ] and clinical studies have reported that upregulation of cav1 was correlated with reduced patient survival [ 2 , 30 , 37 , 43 ]  . 
thus current models consider cav1 as a stageand tissue - specific tumor modulator which acts as a tumor suppressor in nonneoplastic tissue , is downregulated upon transformation , and is reexpressed upon progression in metastatic and multidrug - resistant tumors [ 6 ]  . 
interestingly , various studies showed a relation between cav1 and the acquisition of multidrug resistance via the mdr1 protein [ 3 , 4 , 42 ]  . a dose of 8 gy ionizing radiation increased the expression of cav1 in rat spinal cord [ 1 ]  . 
the latter cells were significantly sensitized to ionizing radiation after knockdown of cav1 expression with sirna . in the studies above , effects of cav1 were inferred from experimental downregulation in cells expressing endogenous cav1 . 
to this end , we used two different vector systems ( a eukaryotic expression plasmid and a lentiviral expression vector ) to overexpress cav1 in the human lymphoblastoid tk6 cell line which does not express detectable endogenous cav1 prote a functional assay showed that overexpression of cav1 conferred enhanced proliferation after a clinically relevant dose of 2 gy and protection against cell loss after 4 gy . material and methods cell culture tk6 cells were cultured in suspension in rpmi 1640 medium with 10% heat - inactivated horse serum ( invitrogen , karlsruhe , germany ) at 37 c under 5% co2 . 
stably transfected tk6 - pcav1 and tk6 - pneo cells , and transduced tk6 - cav1 cells were maintained under the same conditions without antibiotics unless explicitly stated . cloning of human cav1 cdna the coding sequence of human cav1 was cloned from mrna isolated from huvec ( human umbilical vein endothelial cells ) with rneasy mini kit ( qiagen , hilden , germany )  . 
cdna was synthesized using amv first - strand cdna synthesis kit for rt - pcr ( roche , mannheim , germany ) and oligo p ( dt ) 15 primer according to the manufacturers protocol . 
cav1 cdna was amplified with specific primers containing restriction sites ( in italics ) at the 5 ends : forward 5 - ggaattcggatccgccagcatgtctgggggc - 3 and reverse 5 - ctctagattatatttctttctgcaagttgatgc - 3 . expression vectors and viral vector production cav1 cdna was cloned into the eukaryotic expression plasmid pci - neo ( promega , madison , wi , usa ) or into a lentiviral sin ( self - inactivating ) vector phrsin - iresegfp [ 23 ] based on phrsincppt - sew [ 10 ]  . 
2 days later , transduction efficiency was verified by determining the percentage of egfp - ( enhanced green fluorescent protein - ) positive cells by flow cytometry . electroporation and lentiviral transduction electroporation was performed with the amaxa nucleofector system ( amaxa , cologne , germany )  . 
effect of cav1 overexpression after irradation in human cells quantitative real - time pcr apoptosis assay the average number of virus integrations per cell was determined by real - time pcr ( polymerase chain reaction ) using a stratagene mx3005p light cycler ( stratagene , la jolla , ca , usa )  . 
detection was performed by chemoluminescence using hrp - conjugated secondary antibodies , sc - 2004 or sc - 2005 ( santa cruz biotechnology )  . intracellular facs staining 106 tk6 cells were washed in pbs and fixed with 3.7% formal for intracellular cav1 staining , cells were incubated with an antibody against cav1 ( sc - 894 , santa cruz biotechnology ) followed by incubation with an fitclabeled antibody ( ap307f , chemicon , temecula , ca , usa )  . 
immediately after staining , cells were analyzed in a flow cytometer ( facscalibur , bd biosciences )  . ecor i microscopic scoring of apoptotic cells was done by staining with hoechst 33342 dye ( sigma - aldrich , seelze , germany )  . 
 200 cells per condition were counted with a fluorescence microscope using an excitation wavelength of 350 ncells showing irregular chromatin dna condensation were scored as apoptotic and their fraction of the total number of cells was calculated . results construction and dna transfer efficiency of pci - cav1 and lentiviral cav1 vector hrsin - cav1 two different vector systems for transfer of the cav1 gene were used . 
initially , the eukaryotic expression plasmid pci - cav1 was constructed by cloning cav1 cdna via the ecor i / xba i sites into the eukaryotic expression vector pci - neo ( figure 1a )  . 
to avoid the high rate of lethality ( up to 70% ) associated with transfection of cells , a lentiviral sin vector was subsequently used , which is characterized by high levels of gene transfer efficiency and stable gene expression [ 10 ]  . 
to obtain phrsin - cav1 ( figure 1b ) , the cav1 cdna was cloned via the bamh i / xba i sites into the lentiviral sin vector as first cistron in a bicistronic expression cassette in front of a floxed ires - egfp . 
ires - ( internal ribosome entry site - ) mediated translation of egfp permits easy measurement of transduction efficiency by facs ( fluorescence - activated cell sorting ) analysis as both cav1 and egfp are expressed in infected tk6 cells . 
the ires - egfp cassette is flanked by two loxp sites thus allowing excision of the marker , egfp , after transfection with cre recombinase . cav1 sv40 prom xba i loxp pci - cav1 proliferation assay proliferation of each cell line was measured by fluorescence staining in 96 - well microtiter plates using the vital dye alamar blue ( biosource , solingen , germany )  . 
at different time points after irradiation , 20 l alamar blue were added and fluorescence intensity was measured directly and 24 h later using a fluoroskan ascent fluorometer ( thermo fisher scientific , bonn , germany )  . 
effect of cav1 overexpression after irradation in human cells transduction of tk6 cells with hrsin - cav1 at an moi ( multiplicity of infection ) of 0.5 , 4 , or 10 resulted in 9% , 26% , and 36% egfp - positive cells , respectively . 
tk6 - cav1 - zellen zeigten eine starke cav1 - expression , die mit dem cav1 - signal von huvec vergleichbar war , von denen zehnfach weniger gesamtzelllysat verwendet wurde . 
western blot analysis showed no detectable expression of endogenous cav1 protein in tk6 - wt cells or tk6 - pneo ( figures 2a and 2b ) but clear cav1 expression in tk6 - pcav1 ( figure 2a )  . 
cav1 expression at the single - cell level was tested by facs analysis and showed that 90% of tk6 - cav1 cells expressed cav1 compared to tk6 - wt cells ( figure 2c )  . 
thus transduction of tk6 cells with hrsin - cav1 followed by excision of the marker egfp with cre recombinase resulted in a pure population of tk6 cells expressing the cav1 transgene at a high level . cav1 enhances proliferation after irradiation the effect of cav1 overexpression on proliferation after irradiation was tested in a mass culture colorimetric proliferation assay with fluorescent vital staining . 
growth rates for unirradiated tk6 cells electroporated with pci - neo or pci - cav1 showed no difference between tk6 - pcav1 and tk6 - pneo , reaching eightto twelvefold increase on days 56 ( results not shown )  . 
irradiation with 4 gy resulted in constant fluorescence intensity in tk6 - pcav1 cells but decreasing intensity in tk6 - pneo cells , indicating loss of cells from which the culture did not recover ( results not shown )  . since lentiviral transduction was less toxic and yielded superior expression of cav1 , further experiments were performed with tk6 - cav1 . 
unirradiated tk6 - wt cells showed a 17to 18 - fold increase in relative fluorescence after 56 days of incubation with no significant difference between tk6 - cav1 and tk6 - wt ( p = 0.2 ; n = 4 ; figure 3a )  . 
at this time , fluorescence reached a maximum owing to the combined effects of the fluorescent signal being saturated and cell cultures entering plateau phase ( data not shown )  . 
by contrast , tk6 - cav1 cells exhibited a delayed proliferation up to day 3 but strong proliferation from day 4 , reaching elevenfold increase on day 6 ( p = 0.01 ; n = 4 ; figure 3b )  . 
this difference did not reach statistical significance for day 6 alone ( p = 0.057 ; n = 4 ) but was marginally significant , when days 5 and 6 were analyzed together ( p = 0.045 ; n = 8 )  . 
the protective effect of cav1 was corroborated by a reduction in the fraction of apoptotic cells observed after irradiation with 2 gy ( figure 3d )  . discussion the present work describes the effect of eukaryotic expression plasmid and lentivirally mediated cav1 overexpression on the growth rate of tk6 cells following exposure to ionizing radiation . 
therefore , lentiviral transduction and facs selection were both more efficient and more gentle to the cells . the human immature b - cell lymphoblastoid cell line tk6 [ 36 ] is characterized by a stable karyotype and wild - type p53 status [ 19 , 41 ]  . 
in contrast to previous approaches which used endogenous cav1 - expressing cells to assess radioprotection [ 9 , 18 ] , tk6 - wt show no detectable endogenous cav1 expression . 
nevertheless , the detection of cav1 in human t - cell leukemia cell lines , murine macrophages and b lymphocytes and bovine dendritic cells [ 15 , 25 ] supports a functional role for cav1 in lymphocytes . 
 cav1 expression was confirmed by immunoblot and reached a level approximately an order of magnitude lower than huvec with high endogenous cav1 expression . comparison of the proliferation rate of transduced tk6 - cav1 cells to tk6 - wt cells showed no difference between tk6 - cav1 cells and tk6 - wt cells without irradiation . 
applying a dose of 4 gy decreased the cell number of both tk6 - wt and tk6 - cav1 cells within 5 days after irradiation , indicative of cell death . 
however , the number of tk6 - cav1 cells was higher than that of tk - wt cells at all times and suggested beginning proliferation on day 6 after irradiation . 
furthermore , the reduction of radiation - induced apoptosis in lentivirally transduced cells supported an influence of cav1 on the cellular radiosensitivity . the molecular mechanism of radioprotection by cav1 is not fully understood . 
cav1 knockout mice showed increased susceptibility to - radiation [ 18 ] and sirna - mediated knockdown of cav1 was sufficient to sensitize human pancreatic tumor cells to ionizing radiation [ 9 ] , therefore increasing treatment options in radiotherapy of pancreatic cancer [ 16 ]  . 
tk6 - cav1 showed a reduced fraction of apoptotic cells relative to tk6 - wt ( n = 2 , normalized to the mean value for tk6 - wt , 24 h ; error bars signify ranges )  . 
effect of cav1 overexpression after irradation in human cells tumor response in some cancers and thus represents a therapeutic target for inhibition with small molecules or antibodies [ 5 , 8 , 24 , 26 , 33 , 35 ]  . the exact mechanism leading to enhanced early proliferation in cav1 - expressing tk6 cells is not clarified but conceivably , increased dna repair might influence clonogenic cell survival or apoptosis after irradiation . 
further studies to test these hypotheses are in progress . conclusion we have developed an in vitro model system in which effects of cav1 expression can be studied and compared with wild - type cells showing no endogenous cav1 expression . 
further preclinical studies on the relationship between cav1 and cell homeostasis after irradiation are important to explore if therapies targeting cav1 may improve outcome of radiation treatment of cancer . acknowledgments the technical assistance of anne - kathrin kirchner , nicole roth , bernhard berkus and sigrid heil is gratefully acknowledged . 
this work was supported in part by a grant from deutsche krebshilfe / mildred - scheel - stiftung ( 10 - 2089 - fi 1 ) strahlentherapie und onkologie original article gene expression signatures in the peripheral blood after radiosurgery of human cerebral arteriovenous malformations angelika zabel - du bois1 , 2 , mechthild wagner - ecker1 , stefanie milker - zabel2 , christian schwager1 , ute wirkner1 , jrgen debus2 , amir abdollahi1 , 2 , 3 , peter e . 
huber1 purpose : to unravel biological mechanisms potentially resulting in the obliteration process after radiosurgery ( rs ) of human cerebral arteriovenous malformations ( avms ) by investigating molecular signatures on the transcriptomic level in peripheral blood of patients . patients and methods : venous blood samples were obtained at definite points of time before and after rs . 
the corresponding expression profiles were correlated with clinical data and obliteration signs in radiologic imaging . results : the proof of principle that rs outcome can be successfully correlated with transcriptomics of cellular blood components as disease parameter was demonstrated . 
 they also found that low pretreatment blood mrna levels of tlr4 ( toll - like receptor 4 ) and stat3 ( signal transducer and activator of transcription 3 ) correlated with fast obliteration of avms . conclusion : the authors report on a novel technique for molecular biological analysis of blood from patients with cerebral avm treated with rs . 
differential regulation of genes in peripheral blood was successfully correlated with rs and time to obliteration of avthe identified genes indicate a potential new methodology to monitor rs , which may result in an individualized therapy and optimized follow - up . key words : arteriovenous malformation radiosurgery gene expression angiogenesis molecular markers strahlenther onkol 2010 ; 186 : 918 doi 10.1007 / s00066 - 010 - 2034 - 4 genexpressionsmuster zerebraler arteriovenser malformationen aus peripherem patientenblut nach radiochirurgie ziel : untersucht wurden die molekularen mechanismen der wirkung ionisierender strahlung auf das pathologische gefkonvolut bei zerebralen arteriovensen malformationen ( avm ) im peripheren blut von patienten nach radiochirurgie ( rs )  . patienten und methodik : bei patienten mit zerebraler avm wurde zu definierten zeitpunkten vor und nach rs eine vense blutprobe gewonnen und mittels cdnaund oligo - microarray - technologie auf strahleninduzierte vernderungen hinsichtlich biologischer marker ( mrna ) getestet . 
die entsprechenden expressionsprofile wurden mit dem obliterationsverlauf in der radiologischen bildgebung verglichen . ergebnisse : erstmals konnte gezeigt werden , dass eine korrelation zwischen klinischen parametern nach rs zerebraler avm und genaktivitt von peripheren blutbestandteilen mglich ist . 
beispielsweise zeigte sich eine signifikant verminderte expression von neuropilin - 2 ( nrp - 2 ) , protein - c - inhibitor ( pci ) und cyclin - dependent kinase 6 ( cdk6 )  . 
darber hinaus konnten eine positive korrelation zwischen niedrigen prtherapeutischen mrna - werten von tlr4 ( toll - like receptor 4 ) und stat3 ( signal transducer and activator of transcription 3 ) im blut der patienten und schneller obliteration der avm nachgewiesen werden . 1department of radiation oncology , german cancer research center , heidelberg , germany , 2department of radiooncology , university of heidelberg , heidelberg , germany , 3center of cancer systems biology , nasa specialized center of research , caritas st . 
elizabeths medical center , tufts university school of medicine , boston , ma , usa . received : april 21 , 2009 ; accepted : november 9 , 2009 published online : january 28 , 2010 strahlenther onkol 2010 no . 
molecular blood signatures in cerebral avm schlussfolgerung : durch genomweite untersuchungen an blutproben von patienten mit zerebraler avm vor und nach rs konnten erstmals molekulare signaturen im peripheren blut identifiziert werden . 
weiterfhrende untersuchungen der identifizierten gene und proteine sollen in zukunft eine optimierte verlaufskontrolle nach radiotherapie und eine individuell optimierte behandlung ermglichen . schlsselwrter : arteriovense malformation radiochirurgie genexpressionsmuster angiogenese molekulare marker introduction stereotactic radiosurgery ( rs ) is an accepted treatment modality in patients with cerebral arteriovenous malformations ( avms ) , especially in case of inoperability or after prior partial embolization [ 21 , 29 , 33 , 34 ]  . 
the heterogeneous therapeutic effects of irradiation resulting in complete obliteration ( co ) of the nidus are not seen until months or several years after rs [ 29 , 33 ] , and do not allow an individual prediction of successful treatment or individually optimized radiation dose yet . 
however , the molecular effects of ionizing radiation on the pathologic vessels leading ultimately to co are not much looked into . this study was performed to explore genomic information in patients with cerebral avm treated with rs in order to get a better understanding of the mechanisms of radiotherapy and to evaluate the possibility of an individual prediction of successful obliteration and / or an individually optimized radiation treatment . 
genome - wide expression profiling of blood samples from patients treated for cerebral avm with rs was employed to decipher the transcriptional signature of rs and to correlate gene expression with early treatment response of pathologic vessels to irradiation . patients and methods patient characteristics between january and february 2007 , 17 patients ( eight male , nine female ) with cerebral avm treated with linac - based rs at our institution were included in this study . 
written informed consent was provided from all patients . avm classification according to spetzler & martin [ 28 ] was five patients grade i , eight patients grade ii , three patients grade iii , and one patient grade iv . 
the quality of rna was ensured by lab - on chip technology according to the manufacturers instructions ( 2100 bio - analyzer in combination with the rna 6000 lab chip kit , agilent technologies , bblingen , germany )  . mrna expression analysis in patient blood using microarray technology to detect rs - induced differential regulation of genes in peripheral blood , genome - wide expression profiling was performed using human unigene iii cdna microarrays in five avm patients before and 6 weeks after rs . 
briefly , mrna was amplified and labeled using messageamp ii arna amplifikation kit ( ambion #1751 ) and atlas glass fluorescent labeling kit ( bd biosciences #k1037 - 1 )  . 
linear amplification from 500 ng total rna and spike - in - controls ( agilent #5188 - 5282 ) was performed using the agilent low rna input linear amplification kit plus , one color ( #5188 - 5339 )  . 
after rs all of these patients showed a status ideno new onset of ophthalmologic symptoms was seen so far . no significant adverse effects ctc ( common toxicity criteria ) grade 2 after rs were seen during follow - up , especially no focal necrosis or radiation - induced malignancy . messenger rna from peripheral blood could be quantified after preparation of the blood samples using the above - described cdna and oligo - microarray technology . 
especially , the downregulation of neuropilin - 2 ( nrp - 2 ) could be an indication that nrp - 2 is functionally relevant for the radiation - induced obliteration process . 
thus , the radiation - induced downregulation of nrp - 2 may be a molecular mechanism for the antiangiogenetic radiation effect in avm . while nrp - 2 plays a greater role in the venous system , nrp - 1 is more important in the arterial systeinterestingly , nrp - 1 was none of the significantly regulated genes in our strict statistical analysis , whereas sema4b was upregulated significantly after rs . 
the class 4 semas are integral membrane proteins that are widely expressed throughout the nervous systethey act as cofactors for nrp , thus having influence on the vascular system [ 18 , 30 ]  . further on , serpina5 alias pai - 3 ( plasminogen activator inhibitor ) alias pci ( protein c inhibitor ) was found to be downregulated by radiation . 
thus , the radiation - induced downregulation of pci indicates a procoagulant effect . next , we attempted to correlate the interindividual heterogeneity between additional 17 avm patients with time strahlenther onkol 2010 no . 
in particular , we found that downregulation of toll - like receptor 4 ( tlr4 ) and janus kinase 2 / signal transducer and activator of transcription 3 ( jak2 / stat3 ) signaling correlated with fast obliteration of avm ( figure 2 )  . 
therefore , the measurement of biological parameters in the patient blood seems to be an attractive way to gain information about the relevant processes induced by rs of cerebral avm . 
 in the present study , we demonstrate the proof of principle that radiotherapy treatment outcomes can be successfully correlated with transcriptomics of cellular blood components as disease parameter for patients suffering from cerebral avm . 
 however , surgical tissue after rs of cerebral avm is difficult and often impossible to obta therefore , it would be extremely helpful , if meaningful transcriptomic molecular signastrahlenther onkol 2010 no . 
here , we have successfully established a chain of processes to assure the blood sampling in avm patients before and after rs in a way that the subsequent mrna biochemistry produced biostatistically robust and biomedically interpretable data . on the basis of the variable clinical appearance of cerebral avms , especially in terms of spontaneous intracranial hemorrhage , as well as recurrence , growth and spontaneous regression , a structural instability of the avm vessels is anticipated [ 13 ]  . 
there is evidence that nrps are early genes in embryonic vessel development and both nrp - 1 and nrp - 2 are necessary for this purpose [ 31 ]  . 
basically , it is assumed that the rs induced downregulation of the activity of nrp , which seems to play a role in early vessel development of cerebral avm , also plays a role in avm obliteration . a study on hormonal regulation of nrp - 1 and nrp - 2 within the endometrium has shown that nrp - 2 was expressed only by the endothelium of the veins in the secretory phase [ 10 ] , whereas nrp - 2 was very low in the proliferative phase . 
on the other hand , one third of our patients developed a focal edema after rs despite a significant downregulation of nrp - 2 . after rs we also observed a significant downregulation of pai - 3 , which interacts with several steps of the coagulation cascade and has anticoagulant effects . 
the exact mechanism of the anticoagulant effect is not known yet , but we speculate that pai - 3 inhibits procoagulant factors ( thrombin , factor xa , factor xia ) , as well as anticoagulant factors ( activated protein c , thrombinthrombomodulin , urokinase )  . 
since pai - 3 is not only elevated in patients with venous thrombosis but also in those with arterial thrombosis [ 32 ] , it is also conceivable that components of the protein c pathway might be useful molecular biological markers in the treatment of avm . interestingly , we observed that downregulation of tlr4 and jak2 / stat3 signaling correlated with faster obliteration of avseki et al . 
they concluded that tlr4 - dependent modulation of transforming growth factorsignaling provides a link between pro - inflammatory and profibrogenic signals . cdk6 plays an important role within the cell cycle and was downregulated after rs in our study . 
due to an inhibition of the cell cycle a positive effect on the course after radiotherapy of cerebral avm may be anticipated . conclusion we report on a novel technique for molecular biological analysis of peripheral blood from patients treated with rs for cerebral avm . 
considering the intricate pattern of intracellular gene regulatory networks [ 1 ] it is conceivable that pharmacological targeting of endothelial cell - associated genes might enhance radiation effects [ 5 , 9 , 17 , 19 , 2225 ] , thus improving the obliteration rate and therapy of cerebral avm in general . acknowledgments we thank barbara schwager and claudia rittmller for their excellent technical work . 
karstens , michael bremer1 purpose : efficacy and safety of the own single - center experience with moderately dosed radiosurgery ( srs ) for limited ( one to four ) brain metastases were analyzed and correlated with patientand treatment - related variables . patients and methods : between 05 / 1998 and 10 / 2006 , 93 patients received srs for a total of 142 brain metastases . 
46 patients ( 49% ) received initial srs alone , 13 patients ( 14% ) srs with up - front whole - brain radiotherapy ( wbrt ) , and 34 patients ( 37% ) srs for recurrent metastases after wbrt . 
the actuarial 6and 12 - month data for os were 60% and 35% , for local brain control ( lbc ) 87% and 79% , and for distant brain control ( dbc ) 48% and 37% , respectively . 
 in uniand multivariate analysis , only time interval between diagnosis of primary and brain metastases ( p = 0.031 ) and volume of treated metastasis ( p = 0.02 ) were significant predictors of os . 
neither up - front wbrt nor dose had a significant influence on lbc . conclusion : moderately dosed srs of limited brain metastases was found to be both effective and safe . 
initial srs only may be offered to informed patients complying with mri - based follow - up . key words : radiosurgery brain metastases moderate dose outcome data strahlenther onkol 2010 ; 186 : 7681 doi 10.1007 / s00066 - 010 - 2036 - 2 ergebnisse der stereotaktischen einzeitbestrahlung mit moderater dosis bei limitierter hirnmetastasierung . 
 ein monozentrischer erfahrungsbericht ziel : wirksamkeit und vertrglichkeit der moderat dosierten stereotaktischen einzeitbestrahlung ( srs ) bei limitierten ( ein bis vier ) hirnmetastasen sollte am eigenen patientenkollektiv untersucht und mit patientenund behandlungsbezogenen parametern verglichen werden . patienten und methodik : von 05 / 1998 bis 10 / 2006 erhielten 93 patienten eine srs von 142 hirnmetastasen . 
bei 46 patienten ( 49% ) erfolgte die srs als alleinige primrtherapie , bei 13 patienten ( 14% ) mit frher ganzhirnbestrahlung ( wbrt ) und bei 34 patienten ( 37% ) wegen einer rezidivmetastase nach wbrt . 
12 monaten betrugen das gesamtberleben ( os ) aktuarisch 60% und 35% , die lokale kontrolle ( lbc ) 87% und 79% sowie die distale zerebrale kontrolle ( dbc ) 48% und 37% . 
in der uniund multivariaten analyse hatten nur das zeitintervall zwischen diagnose von primrtumor und hirnmetastase ( p = 0 , 031 ) und das volumen der bestrahlten metastase ( p = 0 , 02 ) signifikanten einfluss auf das berleben . 
weder der frhe einsatz der wbrt noch die dosis beeinflussten die lbc signifikant . 1department of radiation oncology , medical school hannover , germany . received : april 15 , 2009 ; accepted : october 26 , 2009 published online : january 26 , 2010 strahlenther onkol 2010 no . 
die alleinige primre srs eignet sich fr informierte patienten , die zu mrt - basierten verlaufskontrollen bereit sind . schlsselwrter : stereotaktische einzeitbestrahlung hirnmetastasen moderate dosis behandlungsergebnisse introduction brain metastases occur in about 25% of cancer patients [ 7 , 15 ] with untreated patients surviving only a few weeks [ 23 ]  . 
patients showing limited brain metastases with controlled or absent extracranial disease and a karnofsky performance score ( kps ) 70 carry a comparably better prognosis [ 5 , 10 , 19 ]  . stereotactic radiosurgery ( srs ) offers a minimally invasive high - precision single - dose radiotherapy of intracranial metastases achieving high rates of local control and even prolonged survival in patients with single brain metastasis when compared to whole - brain radiotherapy ( wbrt ) alone [ 1 , 3 , 9 , 16 ]  . 
while some studies concluded that srs combined with up - front wbrt yields higher local ( lbc ) and distant brain control ( dbc ) compared to srs alone [ 3 ] , others suggest that omission of up - front wbrt does not compromise intracranial control while sparing patients a bothersome large - volume treatment without evidence of a survival benefit [ 8 , 20 , 21 ]  . in srs , a dose - response relationship has been found for local control along with a dose - dependent increase of side effects resulting in volume - dependent dosing recommendations [ 18 , 22 ]  . 
the aim of this retrospective analysis was to report our single - center experience regarding efficacy and safety of srs for limited ( one to four ) brain metastases using moderate radiation doses and omitting up - front wbrt in the majority of patients . patients and methods patient characteristics 93 patients received srs for a total of 142 brain metastases between 05 / 1998 and 10 / 2006 . 
 in 59 patients ( 63% ) , brain metastases were newly diagnosed ; 46 of them ( 49% ) received srs alone as initial therapy ( group 1 ) , while 13 patients ( 14% ) had srs combined with up - front wbrt of 15 2.5 gy ( group 2 )  . 
the median time interval between diagnosis of the primary and the manifestation of brain metastases was 20 months ( range , 0274 months ) with 19 patients ( 20% ) having their brain metastases diagnosed simultaneously with the primary . 
the diagnosis and number of brain metastases were based on a pretreatment gadolinium - enhanced magnetic resonance imaging ( mri ) brain scan in all patients . treatment planning and delivery a stereotactic head frame ( stryker - leibinger ) was fixed to the skull through four screws under local anesthesia . 
treatment was delivered with 6 - mv linac photons using a six - arc rotational technique with isocentric couch movement of 30 between each arc and cylindrical collimators of appropriate diameter ( 521 mm )  . 
five patients ( 13% ) in group 1 ( srs alone ) were treated with doses < 16 gy ( range , 1213 gy ) , three of them received srs for a brain stem metastasis . 
in group 2 ( srs with up - front wbrt ) and group 3 ( srs for recurrence after wbrt ) , doses < 16 gy ( range , 1215 gy ) were given to six ( 46% ) and seven patients ( 21% ) , respectively . the median number of isocenters per treated metastasis was one ( range , one to four )  . 
a p - value < 0.05 was considered to be statistically significant . group 1 ( n = 46 ) ( srs alone ) group 2 ( n = 13 ) ( srs + up - front wbrt ) group 3 ( n = 34 ) ( srs for recurrence ) treatment group results treatment response median os was 7.5 months with 60% and 35% of patients surviving after 6 and 12 months , respectively . 
local brain failure ( lbf ) was observed in 15 metastases ( 14 patients , 15% ) after median 4.6 months ( range , 0.935.1 months ) ; of these , nine patients were in treatment group 1 . 
 there was no statistically significant difference ( p = 0.071 ) in os for rpa class 13 , but only five patients were classified as rpa class 3 due to pretreatment patient selection . 
dbc : distale hirnmetastasenkontrolle ; lbc : lokale hirnmetastasenkontrolle ; os : gesamtberleben ; srs : radiochirurgie ; wbrt : ganzhirnbestrahlung . at 6 months lbc ( % ) dbc ( % ) os ( % ) at 12 months lbc ( % ) dbc ( % ) os ( % ) strahlenther onkol 2010 no . 
ten patients ( 11% ) suffered from seizures within 3 months after srs ; in six of them , progressive brain tumor was diagnosed in follow - up mri . enlargement of contrast - enhancing volume occurred in 19 treated metastases ( 13% ) after median 4.4 months ; twelve of these lesions ( 63% ) were verified as tumor progression on follow - up mri . 
11c methionine positron emission tomography scan of the brain was performed in five patients for differentiation between local progression and radionecrosis , revealing radionecrosis in two and progressive disease in three patients . 
none of the patients with radionecrosis required surgery . salvage therapy only 19 of 44 patients ( 43% ) with progressive brain disease after srs received some kind of salvage therapy : 14 in group 1 , one in group 2 , and four in group 3 . 
ten of 46 patients ( 22% ) in group 1 ( srs alone ) ultimately received salvage wbrt : one of them due to lbf , seven due to dbf , and two due to combined relapse . 
moderately dosed radiosurgery in brain metastases discussion our treatment policy was to use relatively moderate srs margin doses of median 16 gy to limit the risk of radiation - related toxicity in the palliative setting of metastatic brain disease . 
our actuarial 12 - month lbc of 75% for patients with srs alone was equally effective to srs series reported in the literature using radiation doses of median 1525 gy [ 3 , 13 , 20 , 22 ]  . in our analysis , we could not find a statistically significant influence of srs dose on lbc , most probably due to the comparatively low dose range applied . 
 [ 22 ] found a dose - response relationship for srs in brain metastases : lbc at 1 year was 85% after treatment with 24 gy compared to 4549% after 1518 gy . 
 [ 17 ] with maximum tolerable srs dose in preirradiated patients being 24 gy , 18 gy , and 15 gy for metastases 20 mm , 2130 mm , and 3140 mm in diameter . 
 [ 18 ] found 20 gy to be the optimal srs dose for brain metastases 2 csrs doses 20 gy resulted in improved lbc , but at the expense of a higher level of complications . especially for patients with longer life expectancy , neurotoxicity is of major concern [ 11 , 12 ]  . 
to reduce the risk of late radiation effects like inattention , memory loss or emotional dysfunction , wbrt is increasingly being omitted in the initial treatment of limited brain metastases [ 2 , 4 , 15 , 21 ]  . 
other authors [ 8 , 20 , 21 ] could not find omission of up - front wbrt to compromise survival as well as intracranial tumor control , which is in accordance with our results . 
even if salvage brain treatment is required more frequently without up - front wbrt , a relevant number of patients may be spared wbrt during their remaining lifespan . quality of life is of key importance in the treatment of brain metastases , although reliable clinical data are still scarce [ 11 , 14 ]  . 
 [ 3 ] prospectively analyzed quality of life with patients receiving srs and found no difference in neurocognitive function between srs alone and srs plus up - front wbrt , although a more detailed analysis on quality of life was not performed . 
however , when up - front wbrt is omitted , mri - based follow - up visits at regular intervals are advisable to detect new metastases timely before neurologic deterioration may occur . an emerging treatment alternative in high - precision radiotherapy of brain metastases is the use of hypofractionated stereotactic radiotherapy ( hfsrt ) using a relocatable fixation mask . 
fractionation schedule like 5 67 gy , 7 5 gy , or 10 4 gy have been clinically investigated [ 6 ] with an equal or even better therapeutic ratio than srs and easier integration into clinical routine [ 2 , 6 ]  . 
we use our outcome data of srs reported here as an internal reference for evaluation of efficacy and safety of hfsrt . conclusion our data suggests that srs using a relatively moderate dose of 16 gy is both safe and effective with lbc rates being comparable to published data . 
we continue to prefer an individualized treatment strategy withholding up - front wbrt in informed patients complying with repeated mri - based follow - up brain imaging . strahlentherapie strahlentherapie und onkologie und onkologie letter to the editor letter to the editor partial - breast irradiation or whole - breast radiotherapy for early breast cancer : a meta - analysis of randomized trials csaba polgr1 , vratislav strnad2 , gyrgy kovcs3 over the last 4 decades , breast - conserving surgery ( bcs ) followed by whole - breast irradiation ( wbi ) consisting of 57 weeks of daily external beam radiotherapy ( rt ) with or without additional irradiation to the tumor bed has become the standard of care for the treatment of early - stage breast carcinoma . 
however , the necessity of giving wbi to all patients after bcs has been questioned , and several centers have evaluated the feasibility and efficacy of partial - breast irradiation ( pbi ) [ 1 , 2 , 4 , 5 , 7 , 911 , 14 ]  . 
parallel with the growing evidence obtained from phase iii studies supporting the use of pbi for selected early stage breast cancer patients , three early phase iii trials comparing different techniques of pbi to conventional wbi have been conducted in the early 1980s and 1990s [ 3 , 6 , 8 , 12 ]  . 
however , pbi was significantly associated with an increased risk of both local ( relative risk [ rr ] : 2.15 ; p = 0.001 ) and regional recurrences ( rr : 3.43 ; p < 0.0001 ) compared with wbi . 
in this commentary we would like to focus on the pitfalls and limitations of the presented meta - analysis . its main limitation is the mixture of the results of two unsuccessful old british pbi trials ( the christie hospital and cookridge hospital trials ) using inadequate patient selection criteria with a third successful pbi trial using stringent patient selection [ 3 , 6 , 8 , 12 ]  . 
 in the christie hospital series , patients with tumor size up to 4 cm ( 76% t2 ) were enrolled on the study , and axillary staging was omitted ( 100% pnx )  . 
specimen margins were not evaluated microscopically , and 10% of patients had positive margins even on gross examination . in the cookridge hospital study , patients with tumor size up to 4.5 cm and positive axillary lymph nodes ( 41% node - positive ) were eligible . 
therefore , the results of these early clinical trials cannot be used to disparage the concept of pbi , if performed with stringent patient selection ( as used in the hungarian pbi trial )  . there were major limitations in the rt technique used in the pbi arms of the first two studies [ 3 , 6 , 12 ]  . 
the average field size used in the pbi arm was 6 8 cm , and no attempt was made to localize the excision cavity by means of surgical clips or computed tomography based treatment planning . 
the authors themselves concluded that with improved patient selection and refinement of technique , rt restricted to the tumor bed may be an adequate local treatment [ 12 ]  . the cookridge hospital trial was conducted again > 20 years ago ( between 1986 and 1990 ) [ 3 ]  . 
for those women randomized to receive pbi , a variety of out - of - date rt techniques were used , including a direct cobalt ( n = 34 ; 41% ) or cesium ( n = 6 ; 7% ) beam , electrons ( n = 13 ; 15% ) or megavoltage tangential photon ( n = 24 ; 29% ) beams . 
 ( seven patients [ 8% ] in the pbi arm received unintended wbi . ) strahlenther onkol 2010 ; 186 : 1134 doi 10.1007 / s00066 - 010 - 3001 - 9 published online : january 26 , 2010 1department of radiotherapy , national institute of oncology , budapest , hungary , 2department of radiation oncology , university hospital erlangen , germany , 3interdisciplinary brachytherapy unit , university clinic schleswig - holstein , campus lbeck , germany . 
the ptv was defined as the excision cavity ( delineated by the surgical clips ) plus a margin of 12 cthe dose planning was based on a three - dimensional reconstruction of the locations of catheters , surgical clips , and skin points using two postimplant isocentric radiographs . 
in addition to the strict patient selection criteria ( e.g. , patient age > 40 years , maximum tumor size of 20 mm , pn01mi axillary status , pathologic margin status clear by at least 2 mm , excluding patients with invasive lobular carcinoma and eic positive tumors ) , the improved quality assurance ( qa ) program used in budapest was the key to the success of this study . in conclusion , in contrast to the so - called meta - analysis of valachis et al . 
 [ 15 ] , the results of contemporary clinical trials suggest that pbi with proper patient selection and qa yields similar results to those achieved with standard wbi [ 1 , 2 , 4 , 5 , 711 , 14 ]  . 
parallel with the growing evidence obtained from phase iii studies supporting the use of accelerated partial breast irradiation ( apbi ) for selected early - stage breast cancer patients , at least seven phase iii trials comparing different techniques of apbi to conventional wbi have been initiated in the last decade in europe , canada , and the usa [ 9 ]  . 
although both american and european experts encouraged the use of pbi in the context of prospective phase iii trials , during the past few years the concept of pbi has been widely accepted by patients and treating physicians and more than 30 , 000 patients have been treated outside clinical trials worldwide [ 9 , 13 ]  . 
therefore , the american society for therapeutic radiology and oncology ( astro ) recently published their consensus statements on the use of pbi in the daily routine practice [ 13 ]  . 
 please note the corrected strahlentherapie und onkologie original article radiation therapy for early stages of morbus ledderhose reinhard heyd1 , anne pia dorn2 , markus herkstrter3 , claus rdel4 , marcus mller - schimpfle2 , ingeborg fraunholz4 purpose : to evaluate the efficacy of radiation therapy ( rt ) in the treatment of early stages of benign plantar fibromatosis ( morbus ledderhose [ ml ] )  . patients and methods : from 2003 to 2008 , 24 patients ( 33 sites ) with a mean age of 52 years received rt for symptomatic ml . 
the rt protocol consisted of five weekly fractions of 3.0 gy ( 15 gy ) , repeated after 6 weeks to a total dose of 30 gy in 20 patients ( 28 sites )  . 
secondary endpoints were pain relief , improvement of gait , and patients subjective satisfaction measured with a linear analog scale ( las )  . results : after a median follow - up of 22.5 months , none of the patients experienced a progression of number and size of the lesions or the clinical symptoms . 
 long - term follow - up studies including a larger number of patients are required to define the role of rt in the management of this disorder . key words : radiotherapy plantar fibromatosis morbus ledderhose morbus dupuytren benign disease strahlenther onkol 2010 ; 186 : 249 doi 10.1007 / s00066 - 009 - 2049 - x strahlentherapie bei frhen stadien des morbus ledderhose ziel : prfung der effektivitt der radiotherapie ( rt ) bei der behandlung der frhen stadien der benignen plantaren fibromatose ( morbus ledderhose [ ml ] )  . patienten und methodik : zwischen 2003 und 2008 wurden 24 patienten ( 33 lokalisationen ) mit einem durchschnittsalter von 52 jahren aufgrund eines symptomatischen ml behandelt . 
20 patienten wurden mit einem intervall von 6 wochen zwei serien von 5 3 , 0 gy verabreicht ( gesamtdosis 30 gy ) ; vier patienten ( fnf lokalisationen ) erhielten an zwei konsekutiven tagen jeweils eine einzeldosis von 4 , 0 gy . 
die schmerzrckbildung , die verbesserung der gangstrungen und die subjektive zufriedenheit mit dem funktionellen status waren sekundre endpunkte . ergebnisse : nach einer medianen nachbeobachtungszeit von 22 , 5 monaten trat bei keinem patienten eine grenprogression oder zunahme der klinischen symptome auf . 
eine komplette remission der knoten oder strnge wurde bei elf lokalisationen ( 33 , 3% ) erreicht , eine verkleinerung oder zahlenmige reduktion bei 18 ( 54 , 5% ) ; vier lokalisationen ( 12 , 1% ) waren unverndert . 
eine schmerzrckbildung wurde bei 13 / 19 patienten ( 68 , 4% ) erzielt , eine verbesserung von gehstrungen bei 11 / 15 1department of radiotherapy , klinikum offenbach , germany , 2central institute of radiology , municipal hospitals , frankfurt / main - hchst , germany , 3radiotherapeutic practice at the municipal hospitals , frankfurt / main - hchst , germany , 4department of radiotherapy and oncology , university hospital frankfurt / main , germany . received : may 3 , 2009 ; accepted : october 15 , 2009 published online : december 28 , 2009 strahlenther onkol 2010 no . 
an haut und weichteilen traten keine nebenwirkungen rtog - grad > 2 auf . schlussfolgerung : die rt ist bei der behandlung der frhen stadien des ml effektiv und kann die notwendigkeit einer operativen intervention verhindern . 
zur definitiven bewertung des stellenwerts der rt sind langzeitstudien mit greren patientenzahlen erforderlich . schlsselwrter : strahlentherapie plantare fibromatose morbus ledderhose morbus dupuytren gutartige erkrankungen introduction plantar fibromatosis or morbus ledderhose ( ml ) , named after the german surgeon georg ledderhose [ 21 ] , is a rare hyperproliferative disease of the plantar aponeurosis of unknown cause . 
concomitant morbus dupuytren ( md ) is noted in 925% of patients [ 2 , 4 ] , a coincidence with knuckle pads or peyronies disease is observed in 4% of patients [ 2 ]  . 
males are found to be affected twice as often as females [ 2 ]  . the etiology of ml is unclear , and a large number of possible etiologic factors have been discussed [ 31 ]  . 
the onset of symptoms is usually in the 3rd4th decade [ 8 , 31 ] , but children and adolescents may be affected as well [ 12 , 26 ]  . 
most commonly , ml appears unilaterally , bilateral disease is observed in approximately 25% of cases [ 8 ]  . the predominant complaints are tension and a burning of the sole causing a discomfort of gait [ 31 , 32 ]  . 
in the majority of cases , the single or multiple nodules are localized on the central and medial bands of the plantar fascia , occupying the anterior third of the sole along the anterior margin of the arch of the foot [ 4 , 6 , 7 ]  . 
typically , the nodules appear rapidly over a few months , but once established , they often remain stationary for years having a slow tendency of growth [ 8 ]  . 
the overlying skin and the plantar musculature are usually not involved [ 18 , 31 ] , and the fibroblastic hyperplasia is embedded in the tissue of the plantar fascia [ 19 ]  . 
thus , in contrast to md , a contracture of the toes is observed less often [ 6 ]  . similar to md , the formal pathogenesis of ml can be divided into three phases : ( 1 ) the initial phase is characterized by an increased evidence of fibroblasts , and the formation of nodules and cords ; ( 2 ) in the involutional phase , differentiation into myofibroblasts begins ; and ( 3 ) the residual phase is histologically dominated by collagen fibers [ 31 , 32 ]  . due to the unknown cause and the low incidence of ml , a standardized treatment strategy is not defined . 
usually , the primary treatment approach is surgery including different operative techniques such as local or wide excision with a safety margin of 23 cm , and subtotal or radical fasciectomy with or without skin grafting . 
conservative treatment options include the prescription of orthotic devices , physical therapy , local steroid injections , and weight reduction [ 6 , 24 ]  . recently , the value of radiation therapy ( rt ) for primary treatment of ml has only been investigated in one study [ 32 ]  . 
this retrospective multicenter analysis was conducted to obtain more clinical information concerning the efficacy of rt . patients and methods study design the outcome data from three cooperative institutions were documented by means of a standardized documentation sheet . 
secondary endpoints were the influence of rt on functional and morphological signs of the disorder such as pain ( no , slight , moderate , severe ) , gait ( no limitations , > 1 km , < 1 km , complete limitation ) , or size and number of the nodules and cords . 
in addition , the patients subjective satisfaction with the functional status before rt and at follow - up was quantified using a linear analog scale ( las )  . patients from 2003 to 2008 , 24 patients ( twelve males and twelve females ) with a mean age of 52 years were entered into the study . 
lokale kontrolle zum zeitpunkt der nachbeobachtung . radiotherapy technique the target volume included all palpable lesions plus a safety margin of 12 cthe surrounding soft tissue was protected by individual lead shielding ( figure 1 )  . 
21 patients ( 28 sites ) were irradiated using an orthovoltage x - ray unit ( technical details : 70100 kv , 10 ma , 0.75 - mm al filter ; figure 2 )  . 
all of the patients treated by orthovoltage technique received lead shielding of the gonads , the thyroid gland , and the eye lenses . two different dose fractionation schedules were used . 
radiotherapy for morbus ledderhose slight moderate severe before rt at follow - up complete no limitation before rt at follow - up before rt at follow - up ( n = 15 ) figures 4a and 4b . 
a general patterns - of - care study executed in german rt departments revealed that annually more than 20 , 000 patients undergo rt for benign disorders of whom approximately 1 , 000 are treated for hyperproliferative disorders [ 33 ]  . since the first report by beatty in 1938 [ 5 ] the value of rt for the primary management of the early stages of md has been investigated in several studies [ 1 , 14 , 31 , 34 ]  . 
a current literature review showed that after follow - up periods ranging from 1 to 19 years , the rate of local control varied from 60% to 100% [ 31 ]  . 
despite these favorable results for md , the value of rt for the treatment of ml was , as by now , investigated in only one study [ 32 ]  . 
overall , 28 / 36 feet responded with a symptom regression , and in 8 / 36 feet the symptoms were stable . the results of seegenschmiedt & attassi [ 32 ] concerning local control , pain relief , and improvement of gait were confirmed in our study . 
subjektive zufriedenheit der patienten mit dem funktionellen status vor und nach der rt . results after a median follow - up of 22.5 months ( range : 676 months ) , none of the patients experienced a progression of size and number of the lesions or the clinical symptoms , and therefore , a surgical intervention was avoided in all patients . 
radiotherapy for morbus ledderhose in contrast to surgical procedures , which are only indicated in advanced stages of ml or cases refractory to conservative treatment , rt permits an effective prevention of symptom progression in early stages of the disease . 
furthermore , it is unclear whether rt may reduce the recurrence rates after surgical resection analogous to the treatment of plantar desmoids tumors [ 22 ]  . the radiobiological mechanism of rt in ml is suggested to be based predominantly on an inhibition of the fibroblast and myofibroblast proliferation known to be responsible for the symptoms and progression of the disease . 
in addition , md specimens show an increase of growth factors produced by macrophages and platelets , including the fibroblast growth factor , transforming growth factor - , epidermal growth factor , platelet - derived growth factor , and also connective tissue growth factor ( ctgf ) , which play key roles in the pathogenesis of ml and md [ 31 ]  . 
the impact of low rt doses on cytokine expression has been demonstrated for analgetic rt of degenerative disorders [ 2729 ] , but as by now , it remains unclear whether it also plays a role for rt of proliferative disorders . 
 nevertheless , the radiation doses used for treatment of ml or md are associated with the theoretical risk for the induction of soft tissue sarcoma or skin cancer in the radiation portals estimated to be in the range of 12% after latency periods of 830 years [ 31 ]  . 
therefore , a critical indication after an individual risk and benefit assessment , and also a careful radiation technique are recommended . by contrast , surgical treatment of ml is associated with a higher risk for the development of severe persistent side effects including hematoma , painful scars , neuroma formation , infections , and a numbness of parts of the sole [ 13 , 20 , 36 ]  . 
in addition , a delayed wound healing has been reported in up to 5285% of cases [ 10 , 30 ]  . conclusion rt is an effective treatment for early stages of ml which permits the avoidance of surgical treatment in a large number of patients . 
in terms of future perspectives , additional studies with long - term follow - up are needed to investigate the value of rt in a larger number of patients , to evaluate the duration of the treatment effect , and to define the optimal time for rt initiation . 
furthermore , a national patterns - of - care study by the german cooperative group of radiotherapy for benign diseases ( gcg - bd ) is planned to investigate the current role and rt standards for treatment of md and ml in german rt departments . strahlentherapie und onkologie originalarbeit strahlentherapie bei schmerzhafter kniegelenkarthrose ( gonarthrose ) ergebnisse einer deutschen patterns - of - care - studie * ralph mcke1 , m . 
heinrich seegenschmiedt2 , reinhard heyd3 , ulrich schfer1 , franz - josef prott4 , michael glatzel5 , oliver micke6 , german cooperative group on radiotherapy for benign diseases ( gcg - bd ) hintergrund und ziel : nach einer patterns - of - care - studie ( pcs ) der ag strahlentherapie gutartiger erkrankungen der deutschen gesellschaft fr radioonkologie ( degro ) 2003 / 2004 ist eine vielzahl von einzelnen pcs zu unterschiedlichen gutartigen erkrankungen durchgefhrt worden . 
hier wird nun die pcs betreffend radiotherapie ( rt ) bei schmerzhafter gonarthrose ( gna ) vorgestellt . material und methodik : von 2006 bis 2008 wurden alle deutschen strahlentherapeutischen institutionen mit hilfe eines standardisierten fragebogens hinsichtlich patientenzuweisung und - anzahl , anamnese , vorbehandlungen , bestrahlungsindikationen und - techniken , zielvolumenkonzepten usw . 
die rt wurde in 25% der flle mit einem orthovoltgert , in 79 , 6% mit einem linearbeschleuniger und in 8 , 3% mit einem cobalt - 60 - gert durchgefhrt . 
eine mediane schmerzreduktion von mindestens 3 monaten konnte in 60% ( 5100% ) , eine mediane schmerzreduktion von mindestens 12 monaten in 40% ( 10100% ) und eine mediane dauerhafte schmerzreduktion in 27 , 8% ( 1085% ) der bestrahlten patienten erreicht werden . 
es wurden keine radiogenen akutund sptreaktionen angegeben . schlussfolgerung : die vorliegende pcs besttigt mit der bisher weltweit grten fallzahl die traditionell weite verbreitung der rt bei der schmerzhaften gna in deutschland sowie die damit verbundenen sehr guten resultate . 
die rt bei schmerzhafter gna kann als effektive und nebenwirkungsfreie option vor operativen eingriffen durchgefhrt werden . schlsselwrter : strahlentherapie schmerzhafte gonarthrose pcs strahlenther onkol 2010 ; 186 : 717 doi 10.1007 / s00066 - 009 - 1995 - 7 radiotherapy in painful gonarthrosis . 
results of a national patterns - of - care study backgroud and purpose : after a patterns - of - care study ( pcs ) in 2003 / 2004 addressing benign disorders in general , the german cooperative group on radiotherapy for benign diseases ( gcg - bd ) conducted several multicenter cohort studies including the use of radiotherapy ( rt ) in painful gonarthrosis ( gna )  . * die vorstellung der daten erfolgte whrend der 14 . 
pcs zur radiotherapie bei schmerzhafter gonarthrose material and methods : from 2006 to 2008 , a pcs for gna was conducted in all german rt institutions using a standardized structured questionnaire . 
in addition , the long - term functional and subjective outcomes were evaluated . results : 238 / 248 institutions ( 95.9% ) returned the questionnaire : 50 ( 21% ) reported no clinical experience with rt in gna , while 188 ( 79% ) institutions treated 4 , 544 patients annually ( median 15 ; range one to 846 cases per institution )  . 
median pain reduction for at least 3 months was reported in 60% ( 5100% ) , median pain reduction for at least 12 months in 40% ( 10100% ) , and median persistent pain reduction in 27.8% ( 1085% ) of the treated patients . 
despite variations in daily rt practice , high response and low toxicity for this treatment in a very large number of painful and refractory gna cases renders low - dose rt an effective conservative therapy which can be applied prior to surgical procedures . key words : radiotherapy painful gonarthrosis pcs einleitung die bestrahlung benigner erkrankungen einschlielich degenerativer gelenkerkrankungen ( osteoarthrosis deformans ) und damit auch der gonarthrose ( gna ) hat in der radiotherapie ( rt ) eine lange tradition [ 1 , 3 , 710 , 1216 , 18 , 2022 , 24 , 2733 , 3547 ]  . 
etwa 24 , 6% ( 9 219 / 37 410 patienten ) der jhrlichen bestrahlungen von gutartigen erkrankungen in deutschland betreffen patienten mit therapierefraktren schmerzhaften ereignissen im bereich groer und kleiner gelenke , am hufigsten im bereich von schulter - , knieund hftgelenk sowie seltener bei fingergelenkund rhizarthrosen [ 40 , 41 ]  . 
aufgrund der demographischen entwicklung wird die zahl der patienten mit behandlungspflichtigen degenerativen gelenkerkrankungen eher zunehmen [ 36 ]  . unter dem begriff gonarthrose sind alle degenerativen erkrankungen des kniegelenkes ( femorotibial und femoropatellar ) zu verstehen , die durch eine progressive zerstrung des gelenkknorpels unter mitbeteiligung der gelenkstrukturen wie knochen , synovialer und fibrser gelenkkapsel sowie periartikulrer muskulatur gekennzeichnet sind . 
daher hat sie eine hohe sozialmedizinische bedeutung [ 36 ]  . im rntgenbefund zeigen sich typische verdichtungen der gelenklinien , subchondrale sklerosierungen , verschmlerungen des gelenkspalts , entrundungen an den gelenkkanten sowie im endstadium dann gerllzysten und grobe deformierungen . 
klinisch gut zu objektivierende zeichen sind gelenkerguss und schmerzhafte weichteilschwellung [ 14 , 36 ]  . die rt bei schmerzhafter gna , die brigens in der awmf - leitlinie ( arbeitsgemeinschaft der wissenschaftlichen medizinischen fachgesellschaften ) nicht genannt ist , wird meist als letzte mglichkeit ( ultima ratio ) vor einer operation genutzt . 
eine kausale therapie ist mit der rt nicht mglich , durch zahlreiche studien ist jedoch der schmerzlindernde und bewegungsverbessernde effekt belegt [ 3 , 7 , 8 , 10 , 12 , 13 , 16 , 18 , 27 , 32 , 33 , 36 , 37 , 39 , 43 , 4547 ]  . patterns - of - care - studien ( pcs ) sind , trotz gewisser methodischer einschrnkungen , eines der wichtigsten instrumente fr das qualittsmanagement und die erstellung klinischer leitlinien [ 2 , 46 , 11 , 24 , 40 , 41 ]  . 
das outcome stellt dabei den endpunkt dar , auf den sich der standard of care ausrichtet , der diesbezglich nach entsprechend definierten kriterien evaluiert wird [ 2 , 46 , 11 ]  . 
die ag strahlentherapie gutartiger erkrankungen der deutschen gesellschaft fr radioonkologie ( degro ) fhrte daher im gefolge einer allgemeinen pcs zur strahlentherapie gutartiger erkrankungen [ 40 , 41 ] eine pcs zur rt der schmerzhaften gna durch . material und methodik von 2006 bis 2008 erfolgte eine pcs an allen deutschen strahlentherapeutischen institutionen ( n = 248 ) mit hilfe eines standardisierten fragebogens , der postalisch versendet wurde . 
erfragt wurden die zuweiser , die patientenzahl , die anzahl und art der vortherapien , die schmerzanamnese , die speziellen behandlungsindikationen sowie bestrahlungsund zielvolumenkonzepte , wie sie in den einzelnen insitutionen blich sind . 
number of referring doctors and distribution to the attending institutions . 188 / 238 ( 79% ) der strahlentherapeutischen einrichtungen fhren eine rt der schmerzhaften gna durch , dieses 85 - mal ( 45 , 2% ) in versorgungskrankenhusern , 32 - mal ( 17% ) in universittskliniken und 71 - mal ( 37 , 8% ) in praxen und medizinischen versorgungszentren ( mvz )  . es wurden 4 544 patienten pro jahr aus 97 einrichtungen angegeben . 
im median wurden somit 15 patienten ( ein bis 846 ) pro institution im jahr behandelt . zuweiser zur bestrahlung 104 institutionen beantworteten die frage nach der zuweisung zur rt , die hier bei der mglichkeit von mehrfachnennungen 99 - mal ( 95 , 2% ) von orthopden , 88 - mal ( 84 , 6% ) von allgemeinrzten , 30 - mal ( 28 , 8% ) von chirurgen und 29 - mal ( 27 , 9% ) von sonstigen rzten erfolgte . 
dabei wurden pro jahr im median sechs patienten ( ein bis 170 ) von orthopden , fnf ( ein bis 132 ) von allgemeinrzten , vier ( ein bis 40 ) von chirurgen und vier ( ein bis 20 ) von sonstigen rzten zugewiesen . 
bei 688 patienten / jahr war eine gelenkschwellung zu verzeichnen . anzahl und art der vorbehandlungen tiologie und symptomatik der gonarthrose hinsichtlich der tiologie der gna handelte es sich mit 1 937 patienten / jahr am hufigsten um primre arthrosen , bei 583 patienten / jahr um zustnde nach menikusoperationen , bei 326 patienten / jahr um achsenfehler sowie bei 236 patienten / jahr um zustnde nach traumata . 
hinsichtlich der symptomatik gaben 2 449 patienten / jahr bewegungsschmerz , 1 363 patienten / jahr ein bewegungsdefizit sowie 1 292 patienten / in 95 institutionen wurde die anzahl der vortherapien dokumentiert . 
in der mehrzahl der flle ( 65 , 3% ) waren zwei bis drei vortherapien durchgefhrt worden ( abbildung 2 )  . 102 institutionen gaben die art der vorbehandlung an ; am hufigsten kamen dabei die orale medikation mit nichtsteroidalen antirheumatika ( nsar ) , lokale injektionen , operationen sowie physiotherapie zum einsatz ( abbildung 3 )  . 
die rt erfolgte in 79 , 6% am linearbeschleuniger , in 25% am othovoltgert und in 8 , 3% am cobalt - 60 - gert . prozessdaten indikationen zur radiotherapie 106 institutionen gaben die indikation an . 
am hufigsten wurden chronische schmerzen ( 95 , 3% ) , therapierefraktre schmerzen ( 81 , 1% ) nach zumindest zwei vergeblichen vorbehandlungen sowie akute schmerzen ( 18 , 9% ) ber einen zeitraum von 68 wochen genannt . 
der rest applizierte eine , vier oder fnf fraktionen . die einstellung der felder erfolgte in 60 , 6% nach vorheriger simulation , in 35 , 8% klinisch ohne vorherige simulation . 
in drei einrichtungen wurde die virtuelle simulation und in einer einrichtung die simulation jeweils nach computertomographischer planung genutzt . die rt wurde ber ventrodorsale gegenfelder ( 69 , 7% ) , seitlich opponierende gegenfelder ( 26 , 6% ) , ber ein ventrales oder dorsales stehfeld ( 16 , 5% ) oder ein laterales oder mediales stehfeld ( 2 , 8% ) appliziert . 
 eine schmerzlinderung fr wenigstens 3 monate wurde im median bei 60% ( 5100% ) , eine schmerzlinderung fr wenigstens 12 monate bei im median 40% ( 10100% ) der patienten berichtet . 
eine andauernde schmerzabnahme trat im median bei 27 , 8% ( 1085% ) der patienten e keine besserung fand sich im median bei 20 , 5% ( 570% ) der patienten . 
folgen der behandlung wurden in 56 einrichtungen verneint , aus vier einrichtungen wurde hier eine schmerzzunahme am ende der rt angegeben . diskussion die vorliegende pcs umfasst mit n = 5 069 die bisher grte anzahl von patienten , die wegen einer schmerzhaften gna bestrahlt , ausgewertet und publiziert worden sind . 
bezglich bestrahlungstechnik , zielvolumendefinition und bestrahlungsdosis zeigen sich die erwarteten angaben , die nur in einzelfllen abweichungen aufweisen ( einzeldosis von 3 gy bis zu einer gesamtdosis von 12 gy , nutzung von dreidimensionaler planung und virtueller simulation )  . im rahmen der klinischen auswertung der pcs konnte eine sehr gute wirksamkeit der rt gezeigt werden . 
in den bisher publizierten , berwiegend retrospektiven auswertungen fanden sich hnliche ergebnisse ( tabelle 1 )  . meist kommen bei der beurteilung der ergebnisqualitt subjektive schmerzscores zur anwendung , die in der regel an die einteilung von von pannewitz [ 30 , 31 ] angelehnt sind . 
 autoren patienten ( n ) radiotherapie ansprechrate cr ( % ) pr ( % ) nc ( % ) fried 1934 [ 7 ] toschke 1941 [ 43 ] cocchi 1943 [ 3 ] pape & glles 1954 [ 33 ] hess & bonmann 1955 [ 16 ] wieland & kuttig 1965 [ 46 ] wieland 1966 [ 45 ] mitrov & harbrov 1967 [ 27 ] grasshoff 1970 [ 10 ] von pannewitz 1970 [ 32 ] zschache 1972 [ 47 ] hartweg et al . 
 [ 17 ] , hss - score ( hospital special surgery ) nach ranawat & shine [ 34 ] sowie der lequesne - score [ 19 ]  . hinsichtlich nebenwirkungen und risiken wurde aus vier institutionen eine schmerzverstrkung am bestrahlungsende angegeben , weitere nebenwirkungen und auch spezielle folgen wurden verneint . 
hinsichtlich des bekannten sehr geringen tumorrisikos der niedrigdosierten rt knnen wir keine patientenzahlen angeben , da unserer meinung nach eine solche pcs den anspruch , zeitnah auf diesbezgliche ergebnisse zurckgreifen zu knnen , nicht erfllen kann . 
insgesamt kann jedoch konstatiert werden , dass die rt der schmerzhaften gna weitestgehend nebenwirkungsfrei ist . pcs sind ein wichtiges instrument fr die erstellung klinischer leitlinien , geben sie doch den allgemein blichen standard der therapie in einer gewissen region wieder [ 2 , 46 , 11 , 24 , 40 , 41 ]  . 
man bentigt eine gengend groe stichprobe , um statistisch verlssliche aussagen zu treffen , und daher ist man auf die compliance und den guten willen der teilnehmenden institutionen angewiesen , um zahlreiche und qualitativ verwertbare aussagen zu erhalten [ 4 ]  . 
stellt man einen vergleich mit anderen hnlich gelagerten pcs - studien den postalischen datenrcklauf betreffend an ( fersenbeinsporn mit 101 und desmoidtumoren mit 146 beantworteten fragebgen ) , so ordnet sich die hier vorliegende pcs - studie mit 126 beantworteten fragebgen in das bekannte niveau ein [ 25 , 26 ]  . 
auf der andere seite sind pcs in bereichen , in denen nur wenige studien mit hheren evidenzgraden vorliegen , das beste mittel , hhere fallzahlen zu erhalten , um entsprechende empfehlungen geben zu knnen [ 2 , 4 , 11 , 24 ]  . basierend auf den guten daten der pcs kann die rt bei schmerzhafter gna als effektive und nebenwirkungsfreie konservative option noch vor einem operativen eingriff empfohlen werden . 
pcs zur radiotherapie bei schmerzhafter gonarthrose schlussfolgerung die vorliegende studie besttigt mit der bisher weltweit grten fallzahl die traditionell weite verbreitung der rt bei der schmerzhaften gna in deutschland sowie die damit verbundenen sehr guten resultate . 
 questionnaire ( 4 pages )  . german cooperative group on radiotherapy for benign diseases ( gcg - bd ) strahlentherapie bei schmerzhafter kniegelenkarthrose allgemeine daten zur institution : [ .. 
 ( anzahl ) vorbehandlungen [ ] sonstige indikationen : ................................................................ welche indikations kriterien gelten in ihrer institution ? ( bitte ankreuzen ! ) [ ] nein radiologisches korrelat erforderlich : [ ] nein mittlere symptomdauer mind . 
pcs zur radiotherapie bei schmerzhafter gonarthrose angaben zur strahlentherapie : zielvolumenkonzept ( bitte einzeichnen ) : [ ] von ventral oder dorsal [ ] von lateral oder medial [ ] ventrodorsal opponierend [ ] seitlich opponierend planungskonzept : [ ] simulatorplanung [ ] klinische einstellung am gert rt - konzept : gesamtdosis : ............ 
 ( jahr ) anwendung von schmerzscore ? funktionsscore ? erzieltes resultat bei ( n ) patienten ? [ ] nein [ ] nein [ ] ja [ ] ja wenn ja , welcher score ? .......................................... wenn ja , welcher score ? .......................................... [ ] schmerz fr mind . 
1 strahlentherapie und onkologie original article partial - volume segmentation for dose optimization in whole - breast radiotherapy a comparative dosimetric and clinical analysis elisabeth tromm , andreas meyer , jrg frhauf , michael bremer1 purpose : to analyze the dosimetric and clinical benefit of a forward planned technique to optimize dose distribution in whole - breast irradation ( wbi ) using additional partial - volume segments ( pvseg )  . patients and methods : in two separate treatment periods , 265 breast cancer patients received tangential - field wbi and were retrospectively analyzed . 
between 02 / 2004 and 03 / 2006 , 96 patients were treated with one to two additional low - weighted pvseg to reduce dose peaks within the target volume . 
the planning target volume ( ptv ) receiving at least 95% , 105% and 110% of the reference dose ( v95110% ) and frequency of moist skin desquamation during radiotherapy were compared uniand multivariately with patientand treatment - related variables . results : the mean ptv was 1 , 144 ml ( range , 2352 , 365 ml )  . 
v95% was strongly correlated to the risk of developing moist skin desquamations . key words : breast cancer whole - breast radiotherapy partial - volume segmentation dose optimization moist skin desquamation strahlenther onkol 2010 ; 186 : 405 doi 10.1007 / s00066 - 009 - 2031 - 7 partialvolumensegmentierung zur optimierung der dosisverteilung bei ganzbrustbestrahlung . 
eine vergleichende dosimetrische und klinische analyse ziel : untersuchung des nutzens einer einfachen vorwrts geplanten bestrahlungstechnik mit partialvolumensegmenten ( pvseg ) bei der ganzbrustbestrahlung . patienten und methodik : es wurden 265 brustkrebspatientinnen aus zwei behandlungszeitrumen analysiert , die nach brusterhaltender therapie eine ganzbrustbestrahlung mit tangentialen feldern erhielten . 
das planungszielvolumen ( ptv ) , welches mindestens 95% , 105% und 110% der referenzdosis ( v95110% ) erhielt , und die hufigkeit feuchter epitheliolysen whrend der bestrahlung wurden mittels uniund multivariater analyse mit patientenund behandlungsparametern verglichen . ergebnisse : das mittlere ptv betrug 1 144 ml ( streubreite : 2352 365 ml )  . 
in der univariaten analyse beeinflussten folgende faktoren die entwicklung feuchter epitheliolysen signifikant : v95 ( p < 0 , 0001 ) , v105% ( p < 0 , 001 ) , v110% ( p = 0 , 012 ) , eine adjuvante chemotherapie ( p = 0 , 02 ) und die hhe der einzeldosis ( p = 0 , 009 )  . 
in der multivariaten analyse blieb nur v95% ( p = 0 , 002 ) signifikant . 1department of radiotherapy and special oncology , hannover medical school , germany . received : april 14 , 2009 ; accepted : july 24 , 2009 published online : december 28 , 2009 strahlenther onkol 2010 no . 
partial - volume segmentation in breast radiotherapy schlussfolgerung : die vorgestellte pvseg - technik reduzierte dosisspitzen im ptv , wobei patientinnen mit brustvolumina > 1 100 ml am meisten profitierten . 
es konnte eine starke korrelation zwischen v95% und dem auftreten feuchter epitheliolysen gefunden werden . schlsselwrter : brustkrebs ganzbrustbestrahlung partialvolumensegmentierung dosisoptimierung feuchte epitheliolysen introduction breast - conservative surgery ( bcs ) consisting of lumpectomy followed by whole - breast irradiation ( wbi ) is the standard of care for women with early - stage breast cancer [ 7 , 23 ]  . 
at least some degree of acute skin reactions occur in the majority of patients undergoing wbi [ 1 , 11 ] with moist desquamation being reported in 3148% even in modern radiotherapy series [ 21 ]  . 
beyond homogeneity of dose distribution several confounding factors exist , e.g. , neoadjuvant or adjuvant systemic therapy including antihormonal therapy , and variations in intrinsic radiosensitivity [ 25 ]  . 
 both , quality of life and psychological distress are related to patients ratings of cosmetic outcome [ 9 , 22 , 24 ]  . the most important determinant of dose distribution in wbi is breast size [ 19 ] with moist desquamations being more frequent in full - breasted women [ 20 ]  . 
an inhomogeneous dose distribution in wedged tangential fields predominantly occurs at the most cranial and caudal parts of the breast resulting in hot spots with increased risk of adverse effects and inferior cosmetic outcome [ 26 ]  . treatment technique is another important factor influencing frequency and extent of acute skin reactions due to differences in achieving a homogeneous dose distribution . 
for larger breast sizes the difference may be even more relevant , with the incidence of moist desquamation up to 48% with imrt compared to 79% in patients treated conventionally [ 12 ]  . however , the workload for planning and delivering imrt is significant with an increase in rad - on time leading to higher bone marrow exposure to scattered doses [ 15 ]  . the aim of this study was to comparatively analyze the impact of an easy treatment technique to improve dose distribution in wbi and its possible translation into reduced acute skin toxicity . 
this technique consisted of one to two forward planned partial - volume segments ( pvseg ) added to the conventional tangential fields in order to reduce dose peaks within the target volume . patients and methods treatment groups this retrospective analysis included 265 women receiving wbi after bcs at our department . 
treatment group 2 served as a control ( non - pvseg group ) and consisted of 169 patients treated between 01 / 2000 and 12 / 2001 with conventional wedged tangents before implementation of the pvseg technique . treatment planning and delivery all patients were treated with two tangential fields in supine position using a commercially available breast board . 
in treatment group 1 ( pvseg group ) , improvement of dose homogeneity was obtained using one or two additional pvseg with asymmetrically reduced field apertures in the lateral tangent ( figures 1 and 2 )  . 
pvseg were designed by a stepwise forward planned field reduction predominantly in the caudal and / or cranial part of the target volume according to the site of dose peaks as visualized by the isodose lines . radiation was delivered using 6 - mv linac photons . 
for quantitative dose - volume analysis , the planning target volume ( ptv ) was delineated retrospectively slice by slice within the treatment portals as identified by radiopaque skin markers . 
the following categorical variables were tested for significance between both treatment groups using the 2 - test : adjuvant chemotherapy and ptv dichotomized with a cutoff at the median ( 1 , 100 ml )  . 
quantitative dose - volume analyses were performed of the ptv receiving at least 95% , 105% , and 110% of the reference dose ( v95100% ) , respectively . acute skin toxicity occurring during radiotherapy was classified retrospectively according to the radiation oncologists records applying the ctcae 3.0 scoring system [ 5 ]  . 
 moist skin desquamation ( grade 2 toxicity ) was chosen as main criterion of radiation - related toxicity , because this side effect was reported most consistently and therefore seemed appropriate for the purpose of this retrospective analysis . 
relevant portions of the irradiated breast may receive doses exceeding 105% or even 110% of the reference dose ( v105% and v110% ) , which may negatively impact acute side effects and long - term cosmetic outcome [ 4 , 8 , 11 , 20 , 21 ]  . 
dose inhomogeneity occurs particularly at the level of the inframammary fold and other areas of the breast where substantial deviation from the tangential geometry such as scarce , retraction and dose build - up effect is found [ 2 , 17 ]  . 100% ptv 1 , 100 ml ptv 1 , 100 ml ptv > 1 , 100 ml non - pvseg pvseg pvseg ptv > 1 , 100 ml non - pvseg grade 2 grade 1 grade 0 figure 3 . 
details are shown in table 2 . with the easy and time - saving pvseg technique presented here , we were able to reduce relevant dose peaks and optimize dose distribution within the target volume in wbi . 
 quantitative dose - volume analysis in the pvseg group revealed a significant reduction of v105% and v110% compared to a previous group of patients before implementation of this technique ( non - pvseg group )  . 
thus , v95% should rather be regarded as a patient - related parameter indicating breast size ( target volume ) than as a dosimetric parameter . only a limited number of studies investigated whether improvements in dose distribution achievable by modern treatment techniques like imrt actually translate into clinical improvements in terms of reduced side effects . 
found changes in breast appearance in 40% with imrt compared to 58% after conventional tangents only [ 10 ]  . the frequency of moist desquamations found in our analysis ( 1729% ) compared favorably with that reported on imrt - based wbi [ 12 , 16 , 21 ]  . 
beyond treatment technique and dose distribution additional factors may have influenced our comparatively low rate of moist desquamations , e.g. , the exclusive sequential application of adjuvant chemotherapy and radiotherapy . 
from prospective studies it is known , that moist desquamations peak between the 5th and the 6th week of radiotherapy and may occur even 23 weeks after completion of radiotherapy [ 21 ]  . 
found that imrt could minimize breast edema in women with large breast volumes ( 1 , 600 ml ) to a level of 0% compared to 36% of patients treated with a standard technique [ 16 ]  . for an objective estimate of the real clinical benefit imrt has to be compared with the best alternative achievable with three - dimensional conformal treatment planning . 
 potential advantage of additional pvseg in tangential - field wbi is the ability to achieve dose homogeneity while at least in part replacing hard wedges and thereby reducing beam - on times [ 1 , 15 , 18 ]  . conclusion the use of pvseg represents an easy and time - saving technique for optimizing dose distribution in wbi reducing dose peaks within the ptv . 
patients with larger breast sizes ( > 1 , 100 ml , corresponding to a field length of > 17 cm ) might benefit most in terms of reduction of acute skin reactions . 
a strong correlation between v95% and the development of moist skin desquamation could be demonstrated . strahlentherapie und onkologie review article nuclear egfr as novel therapeutic target insights into nuclear translocation and function klaus dittmann , claus mayer , h . 
peter rodemann1 emerging evidence suggests the existence of a new mode of epidermal growth factor receptor ( egfr ) signaling in which activated egfr undergoes nuclear translocation following treatment with ionizing radiation . 
egfr - inhibitory antibodies , i.e. , cetuximab ( erbitux ) , can block nuclear translocation by egfr immobilization within the cytosol in responder cell lines , whereas tyrosine kinase inhibitors rather target nuclear kinase activity of egfr linked with cytosolic or nuclear functions . 
however , both strategies can inhibit dna repair following irradiation . key words : egfr nuclear translocation dna repair cetuximab tyrosine kinase inhibitor strahlenther onkol 2010 ; 186 : 16 doi 10.1007 / s00066 - 009 - 2026 - 4 der nuklere egfr als neues therapeutisches ziel . 
der kerntransport des egfr wird vor allem nach stressexposition der zelle beobachtet und ist mit einer src - kinase - abhngigen internalisierung des egfr in das endosomale kompartment der caveolae assoziiert . 
der nuklere egfr agiert zum einen als transkriptionsfaktor und induziert die transkription von zellzyklusund proliferationsrelevanten proteinen , zum anderen hat er physikalischen kontakt zu fr die dna - reparatur essentiellen proteinen . 
egfr protein can be activated through phosphorylation at specific amino acid residues in response to ligand binding ( egf , tumor necrosis factor - [ tgf - ] and amphiregulin ) [ 18 , 65 ] as well as after exposure to a variety of unspecific stimuli like ionizing radiation [ 52 ] , uv radiation [ 29 ] , hypoxia [ 45 ] , hyperthermia [ 17 ] , oxidative stress [ 28 ] , and transactivation by g - protein - coupled receptors [ 6 ]  . 
both ligand - dependent as well as ligand - independent 1division of radiobiology and molecular environmental research , department of radiooncology , university of tbingen , germany . recieved : march 18 , 2009 ; accepted : september 25 , 2009 published online : december 28 , 2009 strahlenther onkol 2010 no . 
nuclear egfr as therapeutic target phosphorylations of egfr result in receptor internalization [ 60 ] and intracellular signaling [ 13 , 50 , 51 , 57 , 59 ]  . 
cell exposure to oxidative stress can lead to internalization of egfr into caveolae , however , this process is associated with perinuclear accumulation of egfr and persistent kinase activity , as reported by khan et al . 
variations in subcellular localization are associated with a plethora of ascribed functions for this protethese observations suggest a general function of caveolae as an intracellular signaling platform . in agreement with that , compartmentation into caveolae prevents egfr degradation and simultaneously enables intracellular egfr kinase - linked signaling [ 28 ]  . 
these findings suggest a new function of egfr depending on its intracellular localization , which supplements its functions described so far and defines a new therapeutic target . ionizing radiation results in fast src kinase stabilization , activation and subsequent src - mediated caveolin - 1 y14 and egfr y845 phosphorylations . 
both phosphorylations are stress - specific and cannot be observed after treatment with egf [ 14 ] , which suggests caveolae sorting of egfr as a stress - associated event . 
treatment with the egfr - inhibitory antibody cetuximab results in some tumor cells in a strong accumulation of caveolin / egfr complexes within cytoplas radiation - induced caveolin - 1 and egfr phosphorylations are associated with nuclear egfr transport [ 14 , 32 ]  . 
as shown by the src - specific inhibitor pp2 , blockage of src activity inhibits caveolin - 1 phosphorylation and decreases nuclear transport of egfr [ 14 ]  . translocation of egfr from caveolae into endoplasmic reticulum nuclear localization of the egfr requires endocytosis and association of the receptor with the karyopherin carrier nuclear import system [ 32 ]  . 
as cells do have protein complexes that translocate proteins into and out of lipid bilayers [ 63 ] , liao & carpenter [ 32 ] explored the possibility , that the sec61 translocon could mediate nuclear transport of the egfr . 
egfr located within the membrane of late endosomes is transferred to the membranes of golgi apparatus by membrane fusion and at least locates in the endoplasmic reticulum ( er ) membrane . 
for nuclear transport egfr has to be set free from er membrane to become a cytosolic protein and to admit access of the karyopherin system to the intrinsic nuclear localization site ( nls ) of the egfr . 
the sec61 translocon is located exclusively in the er and er / golgi transitional region [ 20 ] and functions to insert secretory and transmembrane proteins into the er during protein synthesis [ 26 ]  . 
this translocon is bidirectional and also retrotranslocates proteins from er membrane to the cytosol . egfr transport into nucleus passage through the nuclear pore complex needs binding to nuclear transport receptors . 
monopartite nlss have a single cluster of four to five basic residues , whereas bipartite nlss are characterized by a second basic cluster located about ten to twelve residues downstream of the first cluster [ 16 ]  . 
existence of nuclear export sequences within egfr sequence , however , has not been demonstratfunction of nuclear egfr nuclear egfr detection was first reported in hepatocytes that underwent regeneration and in primary adrenocortical carcinomas [ 38 ]  . 
nuclear egfr as therapeutic target nuclei of many tumors , including those of adrenocorticord , breast , bladder , skin , thyroid , and oral cavity [ 35 , 36 , 38 , 49 ]  . 
indeed , transactivation domains within egfr and its family members her - 2 and her - 4 were identified and found to be functional [ 25 , 34 ]  . 
nuclear egfr and her - 2 were shown to associate with specific dna sequences designated at - rich sequence and her - 2 - associated sequence , respectively [ 25 , 34 ]  . 
given the notion that erbb receptors lack a putative dna - binding domain , it is suspected that these receptors first associate with dna - binding transcription factors and then enhance target gene transcription via their intrinsic transactivational activity . 
furthermore , cooperation of nuclear egfr with the transcription factor e2f1 activates expression of b - myb , a positive regulator of g1 / s cell - cycle progression [ 21 ]  . the observation that nuclear egfr is phosphorylated at autophosphorylation sites indicates that kinase activity of egfr is present within nucleus and suggests that this kinase activity may be relevant for the function of nuclear egfr . 
 [ 61 ] could demonstrate , that proliferating cell nuclear antigen ( pcna ) is subject to tyrosine phosphorylation at a specific site in an egfr - dependent manner and that this phosphorylation enhances pcna stability on chromatthus , these data link tyrosine kinase activity of nuclear egfr with cell proliferation and dna repair by regulating pcna function . in addition , bandyopadhyay et al . 
furthermore , they demonstrated that blocking egfr signaling by cetuximab , an anti - egfr monoclonal antibody , resulted in reduction of nuclear dna - pk protein and kinase activity , implicating a role of egfr in regulation of dna repair . 
 indeed , it could be shown that nuclear egfr is associated with phosphorylation of dna - pk at residue t2609 , which indicates dna - pk activity during nonhomologous end - joining dna repair [ 13 ]  . 
blockage of nuclear egfr transport by cetuximab decreased dna - pk activity and consequently increased residual dna damage and reduced survival after radiation treatment in a549 cells [ 15 ]  . 
these observations suggest a crucial role of nuclear egfr for regulation of dna repair following treatment with genotoxic substances . nuclear egfr transport : a therapeutic target ? as already mentioned above , increased nuclear localization of the egfr is associated with treatment resistance and poor prognosis of tumors [ 23 , 36 , 49 ]  . 
for combination treatment regimens with radiotherapy , preclinical and first clinical data report improved survival [ 8 ] and increased tumor control [ 7 , 30 , 39 , 41 , 42 ]  . 
for use of tyrosine kinase inhibitors in combination with radiation or additional genotoxic treatments , no solid clinical trials exist so far and further clinical evaluation of this approach is necessary [ 9 , 37 , 46 ]  . 
interestingly , in vitro data clearly show , that in some cells cetuximab binding results in accumulation of egfr within cytoplasm , which is associated with blockage of nuclear egfr transport following irradiation [ 15 ]  . 
these contradicting data have to be resolved in additional preclinical experiments and may help to interpret heterogeneous responses of tumors upon cetuximab treatment . in any case , the egfr is removed from cell surface and further ligand - induced signaling is hampered [ 47 ]  . 
the molecular explanation for the increased success of combination treatment with radiation , may be reasoned in the ligand - independent activation of egfr by ionizing radiation [ 14 ]  . 
this activation is not associated with a proliferative cell response , but seems to be more related to regulation of cell survival and dna damage repair [ 14 ] as indicated by means of clonogenic survival assays in vitro . 
both , regulation of cell survival [ 10 ] and dna repair [ 55 ] during treatment regimens with chemo - / radiotherapy were identified as attractive molecular targets during the last years . 
in such a scenario it is noteworthy , that treatment with tyrosine kinase inhibitors or antibodies in combination with radiation results in inhibition of egfr - dependent akt phosphorylation , which is linked with regulation of cell survival [ 40 ]  . 
nuclear egfr either interacts with dna - pk and is involved in activation of kinase activity essential for nonhomologous end - joining dna repair , or acts as a transcription factor regulating expression of essential genes . 
offensichtlich ist vor allem fr die effekte auf die dna - reparatur die kinaseaktivitt des egfr im zellkern essentiell , da sich durch den einsatz von tyrosinkinaseinhibitoren ( tki ) die dna - reparaturkapazitt reduzieren lsst . ment with cetuximab can block nuclear egfr transport in certain tumor cells , which is linked with inhibition of dna repair [ 15 ]  . 
furthermore , it is difficult to dissect the role of nuclear egfr from classic membrane - associated egfr signaling following irradiation of the cell , since both cytosolic and nuclear signaling overlay . 
following these studies , three patients with tumors proximal to the optic nerve underwent noncoplanar pbt . results : noncoplanar pbt offered advantage in dose reduction to the optic nerve when compared to coplanar therapy . 
none experienced radiation injury to the optic nerve during a short follow - up time of 712 months . conclusion : noncoplanar pbt appears to reduce doses to organs at risk . key words : proton - beam therapy irradiation noncoplanar coplanar technical consideration strahlenther onkol 2010 ; 186 : 369 doi 10.1007 / s00066 - 009 - 2019 - 3 technische aspekte der nichtkoplanaren protonenstrahlentherapie bei patienten mit proximal des sehnervs gelegenen tumoren ziel : untersuchung der technischen mglichkeiten der nichtkoplanaren protonenstrahlentherapie ( pst ) im hinblick auf die reduktion der dosisbelastung von kritischen organen . material und methodik : evaluiert wurden der grad der mechanischen przision , die rotationsbeschrnkungen der gantry und des behandlungstischs , und es wurden dosis - volumen - histogramme fr die nichtkoplanare und koplanare pst verglichen . 
im anschluss daran wurden drei patienten mit proximal des sehnervs gelegenen tumoren einer nichtkoplanaren pst unterzogen . ergebnisse : die nichtkoplanare pst war im hinblick auf die reduktion der dosisbelastung des sehnervs im vergleich zur koplanaren therapie von vorteil . 
bei keinem der patienten traten whrend eines kurzen nachuntersuchungszeitraums von 712 monaten strahlenschden am sehnerv auf . schlussfolgerung : die nichtkoplanare pst scheint die dosisbelastung fr risikoorgane zu reduzieren . schlsselwrter : protonenstrahlentherapie bestrahlung nichtkoplanar koplanar technische aspekte introduction proton - beam therapy ( pbt ) has been proven to offer the best physical dose distributions when compared to other therapeutic techniques such as three - dimensional conformal , stereotactic , or intensity - modulated radiotherapy [ 1 , 2 , 47 , 11 , 12 , 1517 , 2125 , 2730 ]  . 
differences in noncoplanar and coplanar pbt lie in the beam direction , that is , in the former the beam enters the target through any spherical angles , whereas in the latter the beam plane is perpendicular to the corporal axis . 
in this communication , attempts were made to reduce the dose to the optic nerve by selecting beam directions on noncoplanar basis . 1proton medical research center , university of tsukuba , ibaraki , japan , 2alpert medical school of brown university , providence , ri , usa , 3department of radiology , tokyo medical university , japan . received : march 16 , 2009 ; accepted : july 24 , 2009 published online : december 28 , 2009 strahlenther onkol 2010 no . 
technical consideration of noncoplanar pbt material and methods the pbt system used consists of an isocentrically rotational gantry equipped with an x - ray imager , a rotational treatment couch , a treatment - planning system , a treatment - planning computed tomography ( ct ) scanner , and an x - ray simulator without any modification of the system [ 26 ]  . 
proton beams ranging from 155 to 250 mev , generated through a linear accelerator and synchrotron ( probeat , hitachi , tokyo , japan ) , were spread out and shaped with a ridge filter , double - scattering sheets , multileaf collimators , and a custom - made bolus , to confirm the beams to the treatment - planning data . 
since the beam enters the target through unconventional routes in noncoplanar therapy , system precision studies were carried out to ensure that there was no deviation of the isocenter while rotating the gantry and the treatment couch loaded with a 60 - kg phantothis treatment - planning system was used for noncoplanar pbt planning after feeding treatment - planning ct data taken at 2 - mm intervals to the systeduring each treatment session , the position was precisely adjusted through anterior and lateral orthogonal fluoroscopy unit attached to the treatment unit . to validate dose distributions obtained by the treatment planning for noncoplanar therapy , ct images of a 10 - cm spherical phantom were taken at 2 - mm and 5 - mm intervals after matching the center of the phantom with that of the treatment - planning ct at various treatment couch angles , including 45 and 90 . 
range differences were found in noncoplanar beams according to the treatment couch angles and ct image intervals , and maximal difference was within half of ct slice thickness . following these phantom studies , dose - volume histograms ( dvhs ) were obtained for three patients whose tumors were located adjacent to the optic nerve . 
the maximal depth was measured to adjust the treatment planning . following these preliminary studies , three patients with tumors close to the optic nerve and chiasm underwent noncoplanar therapy : case 1 was a 52 - year - old woman with olfactory groove meningioma [ 8 , 19 ]  . 
she underwent noncoplanar therapy receiving 55.4 gye in 28 fractions over 45 days to the tumor with an attempt to reduce the optic nerve dose ( figure 1a )  . 
she underwent pbt because surgery failed to control the tumor [ 9 , 18 ] , receiving 45.5 gye in 23 fractions to the entire right orbit by coplanar therapy followed by noncoplanar therapy delivering 21.8 gye in eleven fractions ( figure 1c )  . these patients were followed for 712 months ( median 10 months )  . 
the relative biological effectiveness ( rbe ) of the pbt was assumed to be 1.1 in this study [ 13 ]  . results the isocenter position remained within a 1 - mm range when the treatment couch was moved and rotated with a phantom loading . 
the gantry rotation was not restricted in the coplanar setup , but restricted in the noncoplanar setup : from 270 to 30 when the treatment couch rotated counterclockwise , and from 330 to 90 when the treatment couch rotated clockwise . dose distributions and distribution lines for a spherical phantom were the same for both noncoplanar and coplanar setup . 
range differences in noncoplanar beams were from 1 to 2.5 mm , which were nearly half of the ct slice thickness , when the ranges of coplanar beams were controlled . 
in case 1 , dose distributions expressed as percent volume versus percent dose revealed that noncoplanar plans appeared desirable ( figure 2a , p1 - 1 ) when compared to coplanar plans ( figure 2a , p1 - 2 )  . 
in case 2 , dvhs remained unchanged for noncoplanar plans ( figure 2b , p2 - 1 ) even if there was a 1 - cm reduction in tumor size during therapy ( figure 2b , p2 - 3 )  . 
solid lines of p1 - 1 , p2 - 1 and p3 - 1 represent dvhs of noncoplanar planning ; dotted lines of p1 - 2 , p2 - 2 and p3 - 2 represent dvhs of coplanar planning . 
when the proton beams reach 1 cm downstream due to tumor shrinkage , the dvhs ( p1 - 3 , p2 - 3 and p3 - 3 for noncoplanar planning , and p1 - 4 , p2 - 4 and p3 - 4 for coplanar planning ) suggest superiority of noncoplanar plans in these selected patients . 
durchgehende linien von p1 - 1 , p2 - 1 und p3 - 1 stellen dvhs der nichtkoplanaren planung dar ; gepunktete linien von p1 - 2 , p2 - 2 und p3 - 2 stellen dvhs der koplanaren planung dar . 
wenn die protonenstrahlen aufgrund einer tumorschrumpfung 1 cm hinter den tumor reichen , deuten die dvhs ( p1 - 3 , p2 - 3 und p3 - 3 fr die nichtkoplanare planung und p1 - 4 , p2 - 4 und p3 - 4 fr die koplanare planung ) bei drei der ausgewhlten patienten auf eine berlegenheit nichtkoplanarer plne hin . the dvhs for coplanar plans ( figure 2b , p2 - 2 ) were the same when the tumor reduction during treatment was taken into account ( figure 2b , p2 - 4 ) , suggesting a higher dose to the optic nerve . 
these results suggest that noncoplanar plans offered a considerable advantage in dose reduction to the optic nerve in all three cases , and that this effect was more significant if reduction in tumor size occurred on the beam direction . these patients completed noncoplanar therapy without interruptions . 
in case 1 , the patient suffered from grade 1 acute dermatitis during therapy , but 1 year after pbt , the primary tumor was under control with no late adverse event . 
in case 3 , the patient experienced grade 2 acute dermatitis but no late toxicity 10 months after pbt . discussion since the dose distribution depends on the proton stopping power that is influenced by a ct hounsfield value , there is uncertainty in dose distribution within nonhomogeneous tissue . 
therefore , minimizing the radiation dose to the organs at risk should be made by cutting the beam with a collimator , or selecting a proper port rather than by means of manipulating the proton stopping power . 
in the three cases treated via noncoplanar ports , the use of a collimator made it possible to avoid the optic nerve , apparently a better approach when compared to coplanar ports . 
therefore , considerable caution is needed for selecting treatment planning when proton beams directly go to optic nerve . range uncertainty occurs in each setup , and in addition , the tumor may be reduced in size as therapy proceeds requiring in - range changes . 
when the range was lengthened by 1 cm in terms of dose distributions , dose distributions were much better for noncoplanar than those of coplanar ports ( figure 2a )  . currently , the isocenter position was confirmed with an x - ray fluoroscopy system before each therapy and by daily confirmation of its position three - dimensionally , noncoplanar therapy was given after relocating the patient to a specified position , omitting final adjustments . 
however , mechanical errors incurred during these procedures were found to be of < 1 mcurrently , treatment - planning ct for noncoplanar therapy is taken at 2 - mm intervals , resulting in an error of 1 m these two errors , possible isocentric error after rotating table and range uncertainty by ct slice interval , were in addition to those incurred by coplanar pbt . 
in our series , only three patients underwent noncoplanar pbt out of 190 patients with head or head - and - neck tumors . conclusion for selected cases , noncoplanar pbt may reduce doses to critical organs even when the tumor shrinks during treatment . 
further improvements in pbt system are necessary to broaden the application of this modality . acknowledgments the study was supported in part by a grant - in - aid for cancer research ( 15 - 9 ) from the ministry of health , labor , and welfare of the japanese government . strahlentherapie und onkologie original article high - grade acute organ toxicity during preoperative radiochemotherapy as positive predictor for complete histopathologic tumor regression in multimodal treatment of locally advanced rectal cancer * hendrik andreas wolff1 * * , jochen gaedcke2 * * , klaus jung3 , robert michael hermann1 , 4 , hilka rothe5 , markus schirmer6 , torsten liersch2 , markus karl alfred herrmann1 , steffen hennies1 , margret rave - frnk1 , clemens friedrich hess1 , hans christiansen1 purpose : to test for a possible correlation between high - grade acute organ toxicity during preoperative radiochemotherapy and complete tumor regression after total mesorectal excision in multimodal treatment of locally advanced rectal cancer . patients and methods : from 2001 to 2008 , 120 patients were treated . 
preoperative treatment consisted of normofractionated radiotherapy at a total dose of 50.4 gy , and either two cycles of 5 - fluorouracil ( 5 - fu ) or two cycles of 5 - fu and oxaliplat toxicity during treatment was monitored weekly , and any toxicity ctc ( common toxicity criteria ) grade 2 of enteritis , proctitis or cystitis was assessed as high - grade organ toxicity for later analysis . 
complete histopathologic tumor regression ( trg4 ) was defined as the absence of any viable tumor cells . results : a significant coherency between high - grade acute organ toxicity and complete histopathologic tumor regression was found , which was independent of other factors like the preoperative chemotherapy schedule . 
its possible impact on local control and survival is under further prospective evaluation by the authors working group . key words : rectal cancer side effects tumor regression preoperative radiochemotherapy strahlenther onkol 2010 ; 186 : 305 doi 10.1007 / s00066 - 009 - 2037 - 1 hhergradige akute organtoxizitt whrend properativer radiochemotherapie als positiver prdiktor fr komplette histopathologische regression in der multimodalen behandlung von lokal fortgeschrittenen rektumkarzinomen ziel : berprfung einer mglichen korrelation zwischen hhergradiger akuter organtoxizitt whrend properativer radiochemotherapie und kompletter tumorregression nach totaler mesorektaler exzision in der multimodalen behandlung von lokal fortgeschrittenen rektumkarzinomen . patienten und methodik : im zeitraum von 2001 bis 2008 wurden 120 patienten behandelt . 
die properative behandlung bestand aus einer normofraktionierten radiotherapie mit einer gesamtdosis von 50 , 4 gy und entweder zwei zyklen 5 - fluorouracil ( 5 - fu ) oder zwei zyklen 5 - fu und oxaliplatdie toxizitt whrend der behandlung wurde wchentlich untersucht . 
jede toxizitt grad 2 nach ctc ( common toxicity criteria ) in form von enteritis , proktitis oder zystitis wurde dabei als hhergradige * the study results were presented in oral form at the 2009 degro ( german society of radiooncology ) annual meeting in bremen , germany . * * both authors contributed equally to the study . 1department of radiotherapy and radiooncology , university medicine gttingen , germany , 2department of surgery , university medicine gttingen , germany , 3department of medical statistics , university medicine gttingen , germany , 4department of radiotherapy and radiooncology , rztehaus am diako , bremen , germany , 5department of pathology , university medicine gttingen , germany , 6department of clinical pharmacology , university medicine gttingen , germany . recieved : april 15 , 2009 ; accepted : september 30 , 2009 published online : december 28 , 2009 strahlenther onkol 2010 no . 
bei vollstndigem histopathologischen tumoransprechen ( trg4 ) konnten im operationsprparat nach neoadjuvanter therapie keine vitalen tumorzellen mehr identifiziert werden . ergebnisse : es fand sich eine signifikante korrelation zwischen hhergradiger akuter organtoxizitt und kompletter tumorregression , und zwar in multivariater analyse unabhngig von anderen faktoren wie z.b. 
 die wahrscheinlichkeit fr die patienten mit hhergradigen nebenwirkungen , eine histopathologische komplettremission zu entwickeln , war mehr als dreimal hher als fr patienten ohne toxizitt ( odds - ratio : 3 , 29 , 95% - konfidenzintervall : [ 1 , 01 , 10 , 96 ] )  . schlussfolgerung : hhergradige akute organtoxizitt whrend properativer radiochemotherapie bei patienten mit multimodaler therapie lokal fortgeschrittener rektumkarzinome knnte einen frhen prdiktor fr das ansprechen auf die therapie in bezug auf die histopathologische remission darstellen . 
ob dieser parameter auch fr die lokale kontrolle sowie das gesamtberleben prdiktiv sein kann , wird in weiteren prospektiven untersuchungen durch die arbeitsgruppe der autoren untersucht . schlsselwrter : rektumkarzinom nebenwirkungen tumorregression properative radiochemotherapie introduction rectal cancer is a common disease in western civilization [ 11 ]  . 
however , reliable predictors of patients treatment response are still lacking , despite encouraging developments like fdg - pet ( fluorodeoxyglucose positron emission tomography ) [ 30 ]  . besides their variation in treatment response , patients differ widely in normal - tissue radiosensitivity , which is thought to arise from the variation in individual cellular radiosensitivity . 
until now , only few reports analyzed treatment - related toxicity with respect to treatment outcome [ 2 , 3 , 7 , 28 ]  . in this context , the aim of the present study was to test for a possible correlation between high - grade acute organ toxicity ( ctc [ common toxicity criteria ] grade 2 ) during preoperative rct and complete tumor regression after total mesorectal excision in rectal cancer . patients and methods between march 2001 and april 2008 , 120 patients with locally advanced rectal cancer were treated multimodally . 
all procedures were followed in accordance with the ethical standards of the responsible committee on human experimentation and with the helsinki declaration of 1975 , as revised in 2000 . before treatment , locoregional tumor stages were classified via endoscopic ultrasound ; the distribution of tumor stages is shown in table 1 . 
the prevalence of comorbidities possibly influencing radiosensitivity ( diabetes mellitus ) was 11% . initial staging examinations included medical history , clinical examination with biopsies in potential mucosal primary sites during a whole colonoscopy , complete blood counts , biochemical analysis , electrocardiogram , chest x - rays , abdominal ultrasound , and mri ( magnetic resonance imaging ) scans of the pelvis with contrast mediu1 day before the start of rct , the hemoglobin level was determined in each patient . 
pretreatment characteristics of patients are summarized in table 1 . radiochemotherapy radiotherapy was delivered with a varian clinac 600 c / d accelerator ( varian , palo alto , ca , usa )  . 
as described previously [ 31 ] , target volume definition was performed according to the guidelines of the german rectal cancer study group . concomitant chemotherapy was given as follows : 73 patients received 5 - fluorouracil ( 5 - fu ) at a dose of 1 , 000 mg / m2 tbsa / d ( total body surface area ) by a continuous infusion for 120 h during the 1st and 5th week of irradiation according to the publication of sauer et al . 
4 weeks after surgery , 100 mg / m2 tbsa oxaliplatin by a 2 - h infusion and 5 - fu 2 , 400 mg / m2 tbsa by a 46 - h continuous infusion were administered on days 1 and 15 ( overall eight cycles in 16 weeks )  . toxicity was monitored weekly during rct and every 2nd week until disappearance of acute side effects of the preoperative therapy . 
side effects were classified according to the ctc score [ 29 ] , and any toxicity grade 2 in any form of enteritis , proctitis or cystitis was assessed as high - grade organ toxicity for later analysis . 
acute organ toxicity grade 2 was chosen as cutoff value , as in patients with toxicity grade 2 quality of life is significantly impaired . surgery and histopathologic examination 46 weeks after completion of preoperative rct , total mesorectal excision was performed according to a standardized technique . 
 if adjacent organs were involved intraoperatively , surgery was extended to partial or total resection of adjacent pelvic organs . the extent of residual tumor in the resected specimen was classified according to the tnm staging system of the uicc . 
 residual tumor mass , rct - induced fibrotic changes , and irradiation vasculopathy were semiquantitatively evaluated according to a 5 - point rectal cancer regression grading , a modification of the tumor regression grading ( trg ) as described by gavioli et al . 
briefly , tumor samples without any fibrosis / regression were considered trg0 , whereas complete regression ( trg4 ) was defined as the absence of viable tumor cells in the primary tumor and the lymph nodes ( ypt0 n0 )  . 
a regression within 5080% was classified as tgr2 , and if regression exceeded 80% , the samples were classified as trg3 . postoperative staging of resected specimens showed 17 ypt0 , 16 ypt1 , 28 ypt2 , 51 ypt3 , and eight ypt4 cases . 
high - grade acute organ toxicity as predictor of complete tumor regression in rectal cancer complete tumor regression no yes statistical analysis quantitative parameters were compared between patients with complete and those without complete tumor regression by either fishers exact test or by the 2 - test . 
because of acute side effects , radiotherapy had to be stopped in the other four patients at least at a minimum dose of 41.4 gy ( two patients ) up to 45 gy ( two patients )  . 
chemotherapy regimen had to be reduced to one cycle in eight patients ( three enteritis grade 2 , one coronary spasm , one exanthema , one hand - foot syndrome , one blood pressure decrease , and one interleukin - 6 - releasing syndrome )  . hematologic toxicity during preoperative rct appeared as follows : anemia grade 1 occurred in twelve patients , grade 2 in 15 , and grade 3 in one . 
as some patients suffered from more than one item , 35 patients had high - grade ( ctc grade 2 ) acute organ toxicity ( minimum one item or more of cystitis , proctitis , or enteritis ) in total . 
 there was no difference in the distribution of tumor localization ( lower versus middle third ) or comorbidities between the groups with high - grade acute organ toxicity versus the group without . histopathologic tumor regression was analyzed after rct and surgery in every patient . 
trg4 was recognized in 17 patients ( 14% ) , trg3 in 53 patients ( 44% ) , trg2 in 37 patients ( 31% ) , and trg1 in 13 patients ( 11% )  . in the group of patients with high - grade acute organ toxicity , 26% achieved complete tumor response ( trg4 )  . 
die prozentualen anteile unterschieden sich signifikant ( p = 0 , 04 )  . proportion was significantly different ( p = 0.04 in uniand multivariate analysis ; figure 1 , table 1 ) and independent of all other factors like type of preoperative chemotherapy schedule . 
 there was also a significant difference in the distribution of the t - stage before therapy between complete and incomplete responders ( p = 0.02 in univariate and p = 0.03 in multivariate analysis ) , where complete responders had lower t - stages . 
high - grade acute organ toxicity as predictor of complete tumor regression in rectal cancer eight patients died from tumor and three from intercurrent disease ( heart failure in two and respiratory insufficiency in one )  . 
 [ 2 ] showed that in patients with locally advanced head - and - neck cancer treated with radiotherapy and cetuximab , acute toxicity ( rash and skin toxicity ) could also predict tumor response : patients were divided by a cutoff value of toxicity grade 2 into a nontoxic ( skin toxicity grade 01 ) and toxic ( skin toxicity 24 ) group according to their acute toxicity during radiotherapy with cetuximab . 
 [ 7 ] , women with hormone receptor - positive breast cancer and vasomotor or joint symptoms at first follow - up visit during either adjuvant tamoxifen or anastrozole treatment were compared with women without these symptoms . 
furthermore , these patients had less recurrences and better disease - specific survival rates than patients without high - grade acute side effects . one possible cytogenetic approach to explain a correlation between normal - tissue and tumor - tissue radiosensitivity might be a difference in the ability to repair double - strand breaks after damage in different individuals . 
 [ 28 ] analyzing in vitro radiosensitivity of lymphoblastoid cell lines , fibroblasts and white blood cells from healthy donors and cancer patients with or without late effects ( grade 34 according to the rtog [ radiation therapy oncology group ] score ) as well as donors with known radiosensitivity syndromes like heterozygous or homozygous genotype for ataxia - telangiectasia and nijmegen breakage syndrome . 
 [ 3 ] found that individual radiosensitivity as determined with lymphocytes using a chromosomal assay after in vitro irradiation can be used to predict the risk of acute side effects during radiotherapy . 
in this context , several other studies have already shown that the pretherapeutic hemoglobin level in patients treated with concomitant rct is a prognostic factor for overall survival and outcome in several tumor entities , e.g. , head - and - neck [ 5 , 9 , 12 , 14 , 17 , 22 ] or non - small cell lung cancer [ 21 ] , and cervix carcinoma [ 10 , 18 ]  . furthermore , it is known that complete tumor regression after rct is a prognostic factor for locoregional control and overall survival [ 1 , 13 ]  . 
thus , based on our data showing a correlation between high - grade acute organ toxicity during rct and tumor regression grade , one could speculate that strahlenther onkol 2010 no . 
however , our data could not detect such a correlation , probably due to the small sample size , short time of observation after treatment , or the retrospective character of the analysis . 
to clarify these influences and possible cytogenetic factors , further prospective investigations will be done in the context of the cao / aro / aio - 04 trial of the the german rectal cancer study group in our clinical research unit 179 ( klinische forschergruppe 179 [ klifo179 ] , biological basis of individual tumor response in patients with rectal cancer ) funded by the german research foundation ( deutsche forschungsgemeinschaft ) at the university medicine gttingen . acknowledgment this work was supported by the german research foundation ( dfg , kfo 179 )  . strahlentherapie und onkologie original article calcifying tendonitis of the shoulder joint predictive value of pretreatment sonography for the response to low - dose radiotherapy boris adamietz1 , rdiger schulz - wendtland1 , sedat alibek1 , michael uder1 , rolf sauer2 , oliver ott2 , ludwig keilholz2 , 3 background and purpose : calcifying tendonitis is a degenerative inflammatory joint disorder . 
the authors tried to get predictive objectives for the response to radiotherapy on the basis of different morphological patterns of calcifications evaluated by x - ray and ultrasound . patients and methods : between august 1999 and september 2002 , a total of 102 patients with 115 painful shoulder joints underwent low - dose radiotherapy . 
29 joints with calcifying tendonitis could be further divided using the sonographic and radiographic classification according to farin and grtner , respectively . results : pain relief was achieved in 94 / 115 joints ( 82% ) at a follow - up of 18 months ( median )  . 
a different response to radiotherapy was found using the sonographic classification of farin : calcifying tendonitis type iii ( n = 18 ) responded well in contrast to a significantly worse result in type i ( n = 11 )  . 
especially patients with farin type iii calcification will benefit from low - dose radiotherapy . key words : calcifying tendonitis low - dose radiotherapy sonographic classification strahlenther onkol 2010 ; 186 : 1823 doi 10.1007 / s00066 - 009 - 2025 - 5 tendinosis calcarea des schultergelenks . 
prdiktive aussage einer prtherapeutischen sonographie fr das ansprechen nach niedrigdosierter strahlentherapie hintergrund und ziel : die tendinosis calcarea ist eine degenerativ - entzndliche gelenkerkrankung , bei der zur schmerzlinderung auch die niedrigdosierte strahlentherapie erfolgreich eingesetzt wird . 
deshalb versuchten die autoren , aufgrund der unterschiedlichen morphologischen verkalkungsmuster im ultraschall und rntgenbild eine prdiktive aussage zum therapieansprechen zu treffen . patienten und methodik : von august 1999 bis september 2002 wurden insgesamt 102 patienten mit 115 symptomatischen schultergelenken behandelt ( tabelle 1 )  . 
bei 29 schultergelenken mit tendinosis calcarea erfolgte die subtypisierung hinsichtlich des verkalkungstyps sonographisch nach farin sowie rntgenologisch nach grtner ( tabelle 4 )  . ergebnisse : insgesamt trat bei 94 / 115 schultergelenken ( 82% ) nach 18 - monatiger verlaufskontrolle eine beschwerdebesserung ebei der sonographischen klassifizierung fand sich ein unterschiedliches therapieansprechen : die tendinosis calcarea typ farin iii ( n = 18 ) sprach sehr gut auf die therapie an ( abbildung 1 ) , typ farin i ( n = 11 ) zeigte ein signifikant schlechteres therapieansprechen ( abbildung 2 )  . 
mit der rntgenologischen subklassifizierung konnte keine prdiktive aussage getroffen werden ( tabelle 3 )  . 1radiologic institute , university hospital erlangen , germany , 2department of radiology , university hospital erlangen , germany , 3department of radiotherapy , klinikum bayreuth gmbh , germany . received : march 30 , 2009 ; accepted : july 31 , 2009 published online : december 28 , 2009 strahlenther onkol 2010 no . 
treatment options encompass oral antiphlogistics , local injections of steroids , ultrasound , shock - wave , magnetic - field therapy and , finally , low - dose radiotherapy ( ld - rt ) [ 1 , 10 , 11 , 15 , 25 ]  . 
depalma implemented the term of secondary impingement in 1952 , which contains the calcifying tendonitis , bursitis subdeltoidea , and partial and total rupture of rotator cuff [ 4 ]  . 
ultrasound also provides a differentiation of calcific deposits in three types [ 5 ]  . up to now , there is no clinical consensus of which classification has the most predictive value for the response to ld - rt . 
we aimed to classify the calcific deposits according to the findings by radiograph and ultrasound and to correlate the results with the clinical response to radiotherapy graduated by an accepted orthopedic score [ 3 ]  . patients and methods after counseling with informed consent [ 27 ] , a total of 102 patients with 115 painful shoulder joints underwent ld - rt from august 1999 to september 2002 ( male : female 42 : 60 , age 57 , range 4079 years )  . 
every treated shoulder was carefully examined clinically and with ultrasound at the beginning of therapy , during therapy , as well as 6 and 18 months after the end of radiotherapy . 
the sonographic examination included the assessment of the rotator cuff , detection and classification of calcific deposits ( farin type iiii ) and , finally , the tissue focusing bursitis and tendovaginitis . 
 29 shoulder joints affected with calcifying tendonitis were opposed to 86 shoulders with different degenerative disorders as shown in table 1 . radiotherapy was applied with an orthovolt machine ( stabilipan , siemens ) 250 kv , 15 mas , 1 - mm cu filter , tubus size 10 15 cm , focus - skin distance 40 cm with two opposed fields . 
diagnosen der schultergelenkerkrankungen einschlielich der tendinosis calcarea . disease calcifying tendonitis bursitis subdeltoidea tendovaginitis of the long head of the biceps tendon partial tear of rotator cuff complete tear of rotator cuff capsulitis adhaesiva omarthrosis labral tear acromion type ii / iii arthrosis of acromioclavicular joint subacromial spur total cases ( n ) 29 16 7 14 2 3 13 4 0 19 8 115 26 14 6 12 2 3 11 3 0 16 7 table 2 . 
the level of significance was p 0.05. results a total of 82% of all shoulders ( 94 / 115 ) responded to radiotherapy with pain relief after a follow - up of 18 months . focused on the calcifying tendonitis , we found a different clinical response according to the constant score . 
all patients with farin type iii calcifying tendonitis ( n = 18 ) experienced complete pain relief with an increasing mobility in the shoulder joint after completion of therapy ( table 3 , figure 1 )  . in type i calcifying tendonitis , an excellent result could be achieved in five of eleven cases ( table 3 , figure 2 )  . 
 three patients had a good response , further three patients did not respond to therapy . the excellent results in farin type iii calcifying tendonitis were stable during the observation period after 6 weeks and 18 months . 
table 4 outlines the frequency of different types of calcifications including the classification of grtner [ 7 ] and farin [ 5 ]  . radiographic classification of the calcific deposits according to grtner did not provide a significant difference in the response to therapy . 
ansprechen ( schmerzlinderung ) auf die radiotherapie ( rt ) in abhngigkeit vom sonographischen typ nach far signifikanter unterschied zwischen farin - typ i und iii ( p = 0 , 01 )  . response to rt complete pain relief ( n ) partial pain relief ( n ) no response farin type i ( n = 11 ) farin type iii ( n = 18 ) 5 table 4 . 
both terms summarize different disorders but lack further differentiation of the etiopathologic cause of the disorder and do not provide a prediction of response to therapy . a more recent publication of our study group demonstrated an etiologic assignment of different diseases to the primary , secondary and non - impingement , based on the exact diagnosis of shoulder pain [ 1 ]  . 
to find out types of calcification predictive for a success of treatment , different scoring systems of calcification had to be proven in terms of a predictive value . there was no significant correlation between the radiologic classification of the calcification according to grtner and treatment outcome . 
we primarily differentiated all calcifications into three types , but significant differences were found between type i / ii and iii only . calcifying tendonitis affects the tendon of supraspinatus in 80% of all cases , followed by the tendon of infraspinatus ( 15% ) , and tendon of subscapularis ( 5% )  . 
most patients are aged between 30 and 50 years [ 25 ]  . the course of calcifying tendonitis can be divided pathologically into three different stages : precalcification , calcification , and postcalcification [ 29 ]  . 
those calcifications could correlate with type iii according to farin with an absorption quote of 100% after ld - rt . the anti - inflammatory effect of ld - rt on calcifying tendonitis is accompanied by a good pain relief but has no simple explanation on a cellular or molecular level . 
 [ 2 ] reported about effects of ld - rt in an animal model of systemic inflammation with a significantly attenuated adhesion of leukocytes in murine intestinal venules , which was correlated with increased levels of circulating transforming growth factor - ( tgf - ) 1 partially restored the adhesion induced by lipopolysaccharides . 
as htnf - tg mouse represents a model which is very close to the chronic autoimmune situation in humans , these in vivo data confirm anti - inflammatory effects of ld - rt even under conditions of a permanent tnfoverexpression . in vitro assays supported in vivo experimental research evaluating the different steps of the inflammatory cascade . 
 ld - rt reduced the adhesion of peripheral blood mononuclear cells ( pbmc ) to human or murine endothelial cells demonstrating a biphasic kinetics of adhesion [ 13 , 23 , 24 ]  . 
anti - tgf1 antibody treatment restored adhesion of pbmc to irradiated endothelial cells and , furthermore , a biphasic course of tgf1 secretion functionally coincided with the biphasic kinetics of adhesion . 
the profile of secreted cytokines revealed a reduction of tnfand an increase of interleukin - 10 expression [ 22 ] and may suggest a similar anti - inflammatory mechanism as described by voll et al . 
 in the last few years , an increasing number of in vitro experiments were performed to look for molecular mechanisms underlying the anti - inflammatory efficacy of ld - rt . 
various transcription factors such as nuclear factor ( nf ) b , c - fos and c - jun that collectively form homoor heterodimeric activator protein - ( ap - ) 1 transcription factor complex are of crucial importance for the expression of various immune system effector molecules like cytokines or adhesion molecules . 
radiotherapy in patients with acute tendonitis achieved good results : 33% of all patients experienced pain relief after 1 month , 35% had a significant improvement , 21% a slight improvement , and 12% no improvement . 
patients with acute inflammatory disorders ( bursitis subdeltoidea , tendinosis of the long tendon of biceps ) and calcification type iii according to farin achieved a good response to therapy . 
patients with calcifying tendonitis type i have a more chronic inflammatory process and demonstrate a worse response to ld - rt . conclusion the subclassification of calcifying tendonitis according to the sonographic pattern described by farin provides a significant prediction of response to ld - rt . 
therefore , sonographic classification of calcifying tendonitis is an appreciable tool to indicate radiotherapy carefully : especially patients with farin type iii calcification will benefit from ld - rt . strahlentherapie und onkologie original article longitudinal analysis of quality of life in patients receiving conformal radiation therapy for prostate cancer hans geinitz1 , reinhard thamm1 , christian scholz1 , christine heinrich1 , nina prause1 , simone kerndl1 , monika keller2 , raymonde busch3 , michael molls1 , frank b . 
zimmermann1 purpose : to prospectively assess quality of life ( qol ) in patients receiving conformal radiation therapy ( crt ) for prostate cancer . patients and methods : 78 men with definitive crt for prostate cancer were entered into the study . 
changes in mean qol scores with time of 10 points were considered clinically relevant . results : global qol did not change statistically significant during crt and was slightly above baseline levels during follow - up . 
a high number of concomitant diseases and having no children were negative pretreatment predictors for long - term global qol . conclusion : definitive crt for prostate cancer does not compromise global qol during therapy and up to 2 years after treatment . 
 it has a limited negative effect on role functioning , urinary symptoms and , to a lesser extent , on fatigue with restitution within 2 months to 1 year after treatment . key words : prostate cancer conformal radiation therapy quality of life fatigue strahlenther onkol 2010 ; 186 : 4652 doi 10.1007 / s00066 - 009 - 2023 - 7 longitudinale untersuchung der lebensqualitt bei patienten mit konformaler strahlentherapie des prostatakarzinoms ziel : prospektive untersuchung der gesundheitsassoziierten lebensqualitt bei patienten mit konformaler strahlentherapie des prostatakarzinoms . patienten und methodik : 78 patienten mit definitiver konformaler strahlentherapie eines prostatakarzinoms wurden vor , whrend ( 40 gy , 60 gy ) sowie 2 , 12 und 24 monate nach therapie untersucht . 
vernderungen 10 scorepunkte wurden als klinisch signifikant eingestuft . ergebnisse : die globale lebensqualitt nderte sich whrend der strahlentherapie nicht statistisch signifikant und lag im beobachtungszeitraum nach behandlung etwas oberhalb der ausgangswerte . 
bei 60 gy lag die rollenfunktion um > 10 punkte unterhalb des ausgangswerts , und bei 40 und 60 gy stieg der score fr urologische symptome um > 10 punkte ber den ausgangswert an . 
 eine hhere anzahl an begleiterkrankungen und kinderlosigkeit waren negative prtherapeutische prdiktoren fr die globale lebensqualitt nach 2 jahren . 1department of radiotherapy and radiooncology , technische universitt mnchen , germany , 2psychooncology section , department of psychosomatic and general clinical medicine , university hospital , heidelberg , germany , 3institute of medical statistics and epidemiology , technische universitt mnchen , germany . received : march 30 , 2009 ; accepted : september 30 , 2009 published online : december 28 , 2009 strahlenther onkol 2010 no.1 urban & vogel geinitz h , et al . 
quality of life in prostate cancer schlussfolgerung : eine definitive konformale strahlentherapie des prostatakarzinoms wirkt sich nicht negativ auf die globale lebensqualitt whrend und bis zu 2 jahren nach behandlung aus . 
sie hat einen zeitlich limitierten negativen effekt auf die rollenfunktion und die urologischen symptome und in einem geringeren ausma auf die fatigue . schlsselwrter : prostatakarzinom konformale strahlentherapie lebensqualitt fatigue introduction since prostate cancer is often a slowly growing disease causing little or no symptoms , treatment toxicity and quality of life ( qol ) are of major concern [ 5 , 7 , 8 , 10 , 13 , 23 , 24 ]  . 
 to describe the time course of qol in patients with conformal radiation therapy ( crt ) for prostate cancer , we undertook a prospective longitudinal study where patients were assessed at different time points before , during , and after crt . one of the major disadvantages of longitudinal studies in cancer patients is the fact that it is almost impossible to acquire true baseline values . 
with the moment of getting notified the cancer diagnosis the reference frame of the patients shifts , thus qol evaluation does no longer reflect the patients normal state of well - being . 
the aim of the present study was , therefore , to assess the net effect of crt on qol as compared to baseline values acquired within 2 weeks prior to treatment . patients and methods eligibility criteria this study was carried out in a single center , all patients received radiation treatment at the department of radiation oncology of the technische universitt in munich , germany . 
low - risk patients ( t1 / t2a and g1 or g2 [ gleason scores 26 ] and pretreatment prostate - specific antigen [ psa ] 10 ng / ml ) were treated with 70 gy to the prostate . 
intermediate - risk patients ( t1 / t2 and g3 [ gleason scores 710 ] and / or pretreatment psa > 10 ng / ml and 20 ng / ml ) were treated with 70 gy to the prostate and the base of the seminal vesicles . 
high - risk patients ( t3 / t4 or pretreatment psa > 20 ng / ml and < 50 ng / ml ) were treated with 74 gy to the prostate and base of the seminal vesicles . 
the safety margins for the ptv were 1 cm in all directions except for patients who received 74 gy , where the safety margins in the dorsal direction were 0.5 cm for the first 8 gy . of the entire patient population , 73 ( 94% ) received neoadjuvant hormonal therapy for a median duration of 3 months before the onset of radiotherapy ( table 1 )  . 
treatment was discontinued either at the end of radiotherapy ( n = 41 ) or it was continued adjuvantly for a median of another 2 months ( n = 32 )  . 
the majority of the patients ( n = 65 , 84% ) were treated with a gonadotropin - releasing hormone ( gnrh ) agonist and 32 ( 43% ) received a peripheral antiandrogen either in addition to the gnrh agonist ( n = 24 ) or as the sole hormonal treatment ( n = 8 )  . patient assessment and instruments patients were evaluated within 2 weeks before the onset of crt , at the end of treatment weeks 4 and 6 , and 2 , 12 and 24 months after the end of crt . 
at the first evaluation the patients were instructed on how to fill out the questionnaires , during the further time points they usually filled in the questionnaires on their own . 
quality of life in prostate cancer consists of five functional scales , three symptom scales , a global health status / quality of life scale , and six single items . 
for the current evaluation , only the functional scales , the global qol and the fatigue scale were considered , data on the remainder of the qlq - c30 scales will be reported elsewhere . 
since determining a clinically relevant change in qol scores is a matter of debate [ 21 , 26 ] , all statistically significant changes are displayed in addition . prostate cancer module qlq - pr25 the prostate cancer module was developed as a supplementary questionnaire to be employed in conjunction with the qlq - c30 for the assessment of prostate cancer - related symptoms and disease - affected additional qol domains . 
it consists of 25 items in four subscales assessing urinary symptoms ( nine items ) , bowel symptoms ( four items ) , treatment - related symptoms ( six items ) , and sexual functioning ( six items )  . 
since most patients were not sexually active during the study period , sexual functioning was not analyzed for the current evaluation ( the score could only be created for patients who were sexually active )  . concomitant disease all patients were interviewed for the occurrence of concomitant disease before the onset of radiation therapy and 12 and 24 months after therapy . psa values and biochemical recurrence a biochemical recurrence was defined according to the rtog - astro phoenix definition [ 25 ] as an increase of > 2 ng / ml above the nadir psa . 
furthermore , the start of hormonal therapy after radiotherapy was regarded as a biochemical failure . statistical analysis the friedman test was employed to detect changes in qol and fatigue over time . 
of those , 85 ( 81% ) agreed to take part in the study : twelve ( 12% ) denied participation , six ( 6% ) had insufficient command of the german language , and two ( 2% ) were unable to respond to questionnaires because of psychiatric disorders . 
quality of life in prostate cancer pre - crt 40 gy 60 gy 2 months 1 year 2 years pre - crt 40 gy 60 gy 2 months 1 year 2 years figure 1 . 
 five patients experienced a biochemical recurrence according to the phoenix criteria , and in two patients , hormonal therapy was ( re ) initiated due to rising psa values . quality of life global qol did not decrease statistically significant during therapy , after treatment levels were slightly above pretreatment values , reaching statistical significance at 2 years after crt ( wilcoxon test : p = 0.019 ; figure 1 , table 2 )  . 
role functioning deteriorated significantly during crt , but recovered as soon as 8 weeks after treatment and stayed within baseline levels throughout further follow - up ( friedman test : p = 0.001 ; figure 2 , table 2 )  . 
physical functioning and cognitive functioning were not affected by crt and did not change significantly during or after crt . pr25 urinary symptoms significantly increased during crt but reached baseline levels within 8 weeks after therapy ( friedman test : p < 0.001 ; figure 3 , table 2 )  . 
pr25 treatment symptoms did not change significantly during treatment but were below baseline values 2 years after crt ( wilcoxon test : p < 0.001 ; table 2 )  . 
clinically significant changes in score values of > 10 points were recorded only for role functioning and urinary symptoms : the mean score for role functioning decreased by 11.0 points at 60 gy and the mean score for urinary symptoms increased by 12.5 points at 40 gy and 14.0 points by 60 gy . 
clinically relevant changes defined as changes in mean scores of > 10 points were observed only for role functioning and urinary symptoms . longitudinal studies on qol in patients with crt for prostate cancer are rare [ 2 , 14 , 16 , 18 , 19 , 27 , 30 ] , and mostly have a follow - up of 1 year [ 2 , 14 , 16 , 18 , 27 , 30 ]  . 
in concordance with our results , these studies demonstrate that qol is not profoundly impaired by crt and that there is only a temporary deterioration of a limited number of qol domains during or shortly after therapy [ 14 , 18 , 27 ]  . 
analyzed qol ( medical outcomes study group short form health survey [ sf - 36 ] and qlq - c30 ) in 43 men receiving crt for prostate cancer [ 14 ]  . 
men in the imrt group ( 76 gy ) demonstrated a better qol as compared to the crt patients in terms of change in health 1 and 6 months after therapy . 
a recent publication of this study group disclosed a significant improvement of emotional role restriction and functioning , change in health , mental health , and insomnia 3 years after imrt with 76 gy for 95 patients as compared with baseline levels before treatment [ 19 ]  . 
quality of life in prostate cancer it is widely accepted as a threshold for clinically relevant qol changes amongst clinicians and researchers and it is comparable to other studies on qol in prostate cancer [ 19 ]  . one of the most prominent acute side effects of radiotherapy is fatigue [ 6 , 9 ]  . 
this time course is in concordance with other studies evaluating radiation - induced fatigue during and shortly after external - beam radiotherapy [ 4 , 6 , 12 , 32 , 33 ]  . 
during further follow - up ( 1 and 2 years after crt ) , fatigue stayed within pretreatment values , indicating that radiation - induced fatigue in patients with crt for prostate cancer is primarily an acute toxicity without evidence of a second chronic fatigue peak . pr25 urinary symptoms increased clinically significant in our patients during crt and reached baseline levels within 1 year after crt . 
on the other hand , pr25 bowel symptoms did not increase significantly during crt and were not elevated during follow - up which is not in accordance with clinical evidence and published reports on acute and chronic intestinal toxicity [ 3 , 8 , 10 , 11 , 13 , 17 , 20 , 22 , 31 ]  . 
a reason for this discrepancy could lie in the four questions of the pr25 addressing bowel symptoms ( have your daily activities been limited by bowel problems ? , have you had any unintentional release ( leakage ) of stools ? , have you had blood in your stools ? , did you have a bloated feeling in your abdomen ? ) , that might not be sensitive and / or specific enough to reflect alterations in bowel habits during or after crt for prostate cancer . 
in particular , questions addressing increased stool frequency , stool urge , defecation pain or mucus in stool are completely lacking , although these are rather frequent ( acute ) side effects of pelvic radiation therapy . one limitation of our study is the fact that we did not asses qol before the onset of neoadjuvant hormonal therapy , due to the fact , that most of the patients already were on antiandrogen treatment when visiting our department . 
the short - term effects on qol during crt are therefore most likely not influenced by hormonal therapy ( since its prevalence did not change during that time span )  . 
 therefore , one cannot rule out that qol at 1 and 2 years after radiotherapy might appear better in relation to pre - crt values due to the fact that a lower number of patients received hormonal therapy at these times as compared to prior to radiotherapy . 
on the other hand , neither the duration of neoadjuvant / adjuvant hormonal therapy nor the prevalence of hormonal therapy at 1 and 2 years correlated with global qol , functional qol scores , fatigue , or pr25 urinary and bowel symptoms . 
in addition , other published studies did not disclose a major effect of neoadjuvant hormonal therapy on qol except for sexual functioning [ 15 , 24 , 28 ]  . in summary , our study discloses that crt with doses of 7074 gy has only a small and limited negative impact on qol in patients with prostate cancer . 
the data might serve to guide future radiooncologic treatment strategies applying higher doses with recent techniques like imrt , igrt ( imageguided radiotherapy ) , or tomotherapy . conclusion the effects of prostate cancer crt on qol are limited and mostly temporary . 
owing to its small detrimental impact on qol definitive crt for prostate cancer seems to be an excellent treatment choice for this generally slowly growing disease with a small burden of symptoms . acknowledgments we like to thank christine bayer for reading the manuscript . 
a recent study showed no survival benefit with the addition of surgery or wbrt to srs [ 31 ]  . because of its malignant nature , an aggressive therapeu tic approach to rcc brain metastases would seem reasonable . 
in addition , we evaluated six important clinical parameters for outcome in order to identify potential clinical factors for the selection of the appropriate therapy . wbrt + srs n = 17 n ( % ) introduction brain metastases from renal cell carcinoma ( rcc ) account for 510% of the 170 , 000 new cases diagnosed each year [ 32 ]  . 
pre vious studies have reported a median survival of 27 months , and for a long time , wholebrain radiotherapy ( wbrt ) has been the standard palliative treatment [ 8 , 9 , 38 ]  . stereotactic radiosurgery ( srs ) offers an improved lo cal control ( lc ) as well as prolonged overall survival ( os ) in rcc patients with brain metastases [ 1 , 4 , 13 , 17 , 18 , 22 , 23 , 25 , 33 , 34 ]  . 
surgery has failed to improve survival , even though mixed findings have been reported [ 14 , 31 ]  . the best available treatment of rcc patients with brain lesions still remains unclear and conflicting data have been reported regarding the precise role and optimum sequence of table 1 . 
further inclusion criteria were : confirmation of metastases by computed tomography ( ct ) and / or magnetic resonance imag ing ( mri ) , no prior therapy to the brain , and administration of dexamethasone . failure in rcc patients with brain metastases is usually due to the develop strahlenther onkol 2010 no . 
subgroup analysis comparing the different treatments for os and ic in our study were performed separately for rpa class i and iiiii patients . radiotherapy planning and treatment srs was performed for patients with one to three brain le sions , with a single fraction using a linacbased system as pre viously described [ 15 , 16 ]  . 
lesions measuring > 4 cm in dimension were not treated with srs . wbrt was performed with a linear accelerator and 6mv photon beams using opposed lateral fields according to the patients karnofsky performance scale ( kps ) , using either 10 3 gy over 2 weeks ( kps < 70 ) or 20 2 gy over 4 weeks ( kps 70 )  . patients received their first followup 3 months after ra diotherapy and thereafter based on their clinical symptom atology to exclude recurrence and radiation side effects . 
the toxicity of the different treatment regimens was evaluated using the common toxicity criteria 2.0 ( national cancer institute , bethesda , md , usa ) for early toxicity [ 36 ] , and the rtog criteria for late toxicity [ 7 ]  . statistical analysis os , ic , and lc were calculated using the kaplanmeier meth od and compared by the coxmantel longrank test ( univariate analysis )  . 
the prognostic factors found to be signifi cant ( p < 0.05 ) in the univariate analysis were included in the multivariate analysis , performed with the cox proportional strahlenther onkol 2010 no . 
the 1year , 2year , and 3year survival rates from the onset of brain metastases were 30% , 29% , and 23% , respectively . the impact of potential prognostic factors on survival is shown in table 2 ( univariate analysis )  . 
treatment with srs and srs + wbrt had a better os ( both p < 0.001 ) , as compared with wbrt alone , probably due to the different number of metastases between the groups . 
however , srs + wbrt for the treatment of one to three brain metas tases did not increase os , as compared with srs alone ( p = 0.703 ; figure 1 )  . 
no significant association between lc and any of the potential prognostic factors was noted . results of univariate subgroup analyses performed separately for rpa class i and iiii patients are shown in table 4 . 
 comparison of srs and srs + wbrt with wbrt alone revealed a significant difference for both rpa classes ( both p < 0.001 ) , again probably due to the dif ferent number of metastases ( more than three in the wbrt group )  . 
addition of wbrt to srs ( p = 0.043 ) significantly improved ic in rpa class i and showed a trend ( p = 0.061 ) toward better ic in rpa class iiiii patients . 
 on univariate analysis , improved ic was associated with srs ( p < 0.001 ) and srs + wbrt ( p = 0.0127 ) , as compared with wbrt alone ( table 3 )  . 
lack of extracerebral metastases , rpa class i , and age significantly affected ic ( p < 0.001 , p < 0.001 , and p = 0.023 , respectively ) on univariate , but not on multivariate analysis . 
of this group , six ( 7% of total ) required a second radiosurgery and eleven ( 13% of total ) received grade 3 acute toxicities ( nausea , vomiting , headache ) occur red in 2% of patients treated with srs , in 3% treated with srs + wbrt , and in 3% treated with wbrt . 
grade 3 late toxicities ( headache , neurocognitive deficits , visual / hearing impairment ) occurred in 4% of patients treated with srs , in 5% treated with srs + wbrt , and in 4% treated with wbrt . discussion brain metastases represent an important sequel of rcc . 
indeed , patients with multiple me tastases receiving only wbrt have a survival of 47 months [ 9 , 38 ] , and in our study only one of the 20 patients that were treated with wbrt alone were alive 18 months after irradia tion . 
in the present work , the median os for the entire cohort was 11 months and the 1year , 2year , and 3year survival rates from the onset of brain metastases were 30% , 29% , and 23% , respectively . 
subgroup analyses of the different rpa ( recursive partitioning analysis ) classes for sur vival and intracerebral control of treated metastase ( s ) in regard to the impact of the therapeu tic regimen . 
in addition , os was associated with age , lack of extra cranial metastases , and rpa class i , in accordance with previ ous data [ 12 , 22 ]  . the exact role and combination of wbrt and srs in the treatment of brain metastases from rcc remain unclear . 
one must distinguish between the number of brain metastases treated and the different prognostic fac tors analyzed [ 24 ]  . we compared srs to srs + wbrt for rcc patients with one to three brain metastases , separately . 
this is an important finding be cause in rcc patients with brain metastases , failure is strongly correlated to the development of new metastatic lesions rather than local recurrence [ 21 , 31 ]  . 
showed that omission of wbrt in patients treated with radio surgery for up to four brain metastases did not compromise os or ic [ 35 ]  . we also compared srs and srs + wbrt to wbrt alone and showed a significant improvement of os and ic for srsbased treatment . 
to our knowledge , this is the first time that a subgroup analysis of the different rpa classes is performed in rcc patients with brain metastases . salvage op did not improve os , ic and lc in our study , which is in line with an important recent study [ 31 ]  . 
srs , therefore , represents a valuable alternative choice character ized by a high response rate , low morbidity and acceptable sideeffect profile , as in our present work [ 1 , 13 , 17 , 22 , 23 , 25 , 31 , 33 ]  . acute and late toxicity were between 3% and 4% in our study , in line with other reports [ 3 , 13 , 19 , 25 ]  . 
however , the beneficial role of wbrt in improving ic and the evidence that recurrent brain lesions have an adverse effect on quality of life ( qol ) and neurocognitive function have reevaluated its position and reinforced its significance [ 24 , 37 ] , justifying strahlenther onkol 2010 no . 
although some studies showed that cer tain parameters of qol deteriorate after wbrt , other stud ies revealed that qol is improved after wbrt , probably due to the different assessment criteria used [ 5 , 37 ]  . we acknowledge that different factors could potentially influence the present analysis and bias cannot be excluded . 
 this was a retrospective study , which must be taken into ac count when interpreting these results . conclusion srs is a valuable , effective tool for the treatment of rcc pa tients who develop brain metastases , and no difference in os was noted in comparison to srs + wbrt . 
nach 3 jahren betrug die geschtzte kumulative inzidenz gastrointestinaler 1oncologycenter , multiscan&pardubiceregionalhospital , pardubice , czechrepublic , 2departmentofoncology , hospitalnchod , czechrepublic , 3departmentofoncologyandradiotherapy , universityhospitalhradeckrlove , czechrepublic , 4departmentofurology , universityhospitalhradeckrlove , czechrepublic , 5departmentofurology , universityhospitalolomouc , czechrepublic . received : july 1 , 2009 ; accepted : december 22 , 2009 published online : march 26 , 2010 strahlenther onkol 2010 no . 
recently , four randomized controlled trials have confirmed improved biochemical control outcomes with higher radiation dose levels compared with lower doses [ 1 , 4 , 16 , 17 , 26 , 34 ]  . 
increas ing use of dose escalation with 3dcrt techniques leads to higher morbidity , especially longterm rectal toxicity . technological progress enables the implementation of new technologies such as intensitymodulated radiation ther apy ( imrt ) and imageguided radiotherapy ( igrt ) [ 5 , 7 , 9 , 1214 , 21 , 25 , 28 , 29 , 32 ]  . 
this treatment strat egy , termed simultaneous integrated boost ( sib ) , has been introduced for several anatomic sites [ 6 , 8 , 15 , 22 , 23 ]  . 
the use of sib may reduce the dose to the rectal wall and diminish normaltissue complications . patients and methods between december 1997 and june 2007 , a total of 682 patients with localized prostate cancer underwent curative radiation therapy at the department of oncology and radiotherapy , charles university hospital , hradec krlove , czech repub lic . 3dcrt was used in 458 / 682 patients ( 67% ) and imrt in 224 / 682 ( 33% )  . 
94 highrisk patients received 3dcrt to a dose of 74 gy , and 138 pre dominantly intermediate and highrisk patients were treated to a dose of 78 gy using imrt ( imrt 78 )  . 
in 52 patients with intermediate and high risk , excluding stage ct3b , we used sib to deliver 82 gy to prostate and 73.8 gy to seminal vesicles ( imrt / sib 82 )  . irradiation technique treatment planning and irradiation were performend with the patients in supine position , and they were advised to have a comfortably full bladder . 
treatment verification was performed using the electronic portal imaging device ( por talvision 3.8 varian ) once a week . in the 3dcrt group , ctv included the entire prostate and the base of seminal vesicles with the exception of cases with seminal vesicle invasion , where prostate and whole semi nal vesicles were covered . 
maximum rectal dose was to be 97% of the prescribed dose . in the imrt group , slice thickness of the planning ct scans was 3 min patients , in whom the conventional imrt approach ( imrt 78 ) was used , ctv comprised the entire prostate and the base of seminal vesicles ; in patients with sem inal vesicle invasion , prostate and complete seminal vesicles were covered . 
patients were treated with five coplanar fields ( 45 , 100 , 180 , 260 , 315 ) , the intensitymodu lated beams were delivered with a dynamic mlc , using the slidingwindow technique [ 24 ]  . followup all patients were continuously followed during and after ra diotherapy . 
gi : gastrointestinal ; gu : urogenital . gitoxicity grade 1 diarrhea / increasedfrequency / te nesmusnotrequiringmedication ; rectalbleedingnomorethanonce aweek gutoxicity nocturiatwicebaseline ; dysuria notrequiringmedication ; hematu rianomorethanonceaweek grade 2 diarrhearequiringmedicationmore thantwiceweekly ; rectalbleeding atleasttwiceaweekorrequiring onetotwocoagulations ; inter mittentuseofincontinencepads ; regularanalgesicsforpain nocturiamorethantwicebase line ; hematuriaatleasttwice aweekorrequiringonetotwo coagulations ; intermittentuseof incontinencepads ; regularanal gesicsforpain grade 3 diarrhearequiringmedicationmore thantwicedaily ; rectalbleeding requiringtransfusionormorethan twocoagulations ; persistentuseof incontinencepads ; regularnarcotic forpain nocturiamorethanonceevery hour ; hematuriarequiringtrans fusionormorethantwocoagula tions ; urethralstricturerequiring dilatationorendoscopicsurgery ; persistentuseofincontinence pads ; regularnarcoticforpain grade 4 dysfunctionrequiring surgery ( necrosis , per foration , obstruction ) severehemorrhagic cystitis , bladderne crosis , ulceration , or contracturerequiring urinarydiversionand / orcystectomy table 2 . 
3dcrt : dreidimensionale konformale strahlentherapie ; gs : gleason score ; imrt : intensittsmodulierte radiotherapie ; psa : prostataspezifisches antigen ; sib : simultaner integrierter boost ; trus : transrektaler ultraschall ; turp : transurethrale resek tion der prostata ; tvpe : transvesikale prostatektomie . cation of the radiation therapy oncol ogy group ( rtog ) and late effects normal tissue ( lent ) task force tox icity criteria ( table 1 )  . 
the 3dcrt group comprised 94 patients with a me dian followup was 68.4 months ( range , 12124 months ) , the imrt 78 group consisted of 138 patients with a median followup of 37.2 months ( range , 666 months ) , and the imrt / sib 82 group included 52 patients with a median followup of 36 months ( range , 2046 months )  . 
dose escalation in prostate radiotherapy hormonal treatment was administered to 95% ( 3dcrt ) , 55% ( imrt 78 ) , and 79% ( imrt / sib 82 ) of patients . 
symptoms of acute gu toxicity ( grade 1 ) persisted > 1 month in 26.6% ( 3dcrt ) , 36.2% ( imrt 78 ) , and 34.6% ( imrt / sib 82 ) of patient . 
symptoms were present > 12 weeks after treatment in 8.5% ( 3dcrt ) , 14.5% ( imrt 78 ) , and 11.5% ( imrt / sib 82 ) of patients . overall , no fatal toxicity or grade 34 acute gi toxicity was observed . 
symptoms of acute gi toxicity ( grade 1 ) per sisted > 4 weeks in 29.8% ( 3dcrt ) , 26.8% ( imrt 78 ) , and 17.3% ( imrt / sib 82 ) of patients . 
3dcrt : dreidimensio nale konformale strahlentherapie ; imrt : intensittsmodulierte radio therapie ; sib : simultaner integrierter boost . grade 3dcrt 74 gy imrt 78 gy imrt ( sib ) 82 gy table 4 . 
the median time to the development of grade 3 gu toxicity was 2.9 years ( 3dcrt ) , 1.0 year ( imrt 78 ) , and 0.8 years ( imrt / sib 82 )  . 
 among patients with grade 3 gu toxicity , only 50% were symptomatic at the last followup visit . the 3year risk of grade 3 gi toxicity was 14% ( 3dcrt ) , 5% ( imrt 78 ) , and 2% ( imrt / sib 82 )  . 
androgen deprivation therapy had no influence on the development of gi or gu toxicity . time ( years ) 3d - crt 74 gy imrt 78 gy imrt / sib 82 gy figure 1 . 
 ( nach 3 jahren liegt die geschtzte kumulative inzidenz der gastrointestinalen spttoxizitt grad 3 bei 14% fr 3dcrt [ rote linie ] , 5% fr imrt 78 [ grne linie ] und 2% fr imrt / sib 82 [ blaue linie ]  . ) strahlenther onkol 2010 no . 
to our knowlege , no direct comparison of toxicity 3dcrt , imrt and sib in the treatment of localized prostate cancer has been published so far . in the present study , escalating the dose using sib up to the level of 82 gy did not result in an increase of severe toxic ity . 
on the contrary , utilization of this advanced radiotherapy technique though increasing the dose by about 11% led to a significant reduction of grade 3 late gi toxicity in com parison with 3dcrt up to 74 gy . 
the risk of 3year grade 3 gi toxicity was only 5% in the imrt 78 group and 2% in the imrt / sib 82 goup , whereas it amounted to 14% in patients treated with 3dcrt . 
dose escalation resulted in a higher incidence of acute gu toxicity grade 4 ( 4.3% imrt 78 , 3.8% imrt / sib 82 ) which was al ways due to urethral obstruction requiring application of uri nary catheter . 
 3 months after radiotherapy , the urinary catheter had been removed in all patients and their symptoms disappeared . in our series , we observed somewhat higher rates of grade 2 gi toxicity in comparison with recently published data concerning highdose imrt [ 32 ]  . 
this might be explained by prospective toxicity evaluation using the rtog / fclent morbidity scale in our patients , nonuse of image guidance , a different safety margin , and different plan acceptability criteria . 
 a group from the memorial sloankettering cancer center ( mskcc ) , new york , ny , usa , used a smaller posterior safe ty margin around prostate ( 57 mm ) than we did in our patients ( 10 mm )  . 
in their analysis of 2 , 252 positional adjust ment data , setup errors exceeding 5 mm were found in 2473% of fractions according to setup imaging strategies . there are large discrepancies between some morbidity scales and quality of life in a number of patients treated with radical radiotherapy . 
although we employed this relatively strict tool to determine late toxicity , we ob served a considerably low risk of grade 34 late gi / gu toxic ity at 3 years . the rate of observed late toxicity can also influence the length of followup time . 
a group from the fox chase cancer center , philadelphia , pa , usa , reported a median time to late rectal toxicity of 18 months [ 30 ]  . 
our minimum followup for living patients was 24 months , median followup for patients treated with imrt was 37 months ( imrt 78 ) and 36 months ( imrt / sib 82 )  . 
in spite of dose escalation , results of late gu toxic ity are very promising but still premature . conclusion sib may reduce the dose to the rectal wall and diminish nor maltissue complications . 
auch ist nach den hier vorliegenden ergebnissen nicht davon auszugehen , dassesalsfolgedieserbehandlungsformzueinemvermehrtenauftretenvontraumatischemstressodergareiner posttraumaticstressdisorder ( ptsd ) kommt.insgesamtbeeinflussterwartungsgemeherdieartdergrunderkrankung ( ma ligne / benigne ) dasausmaderpsychischenbelastungderpatientennachstrahlentherapie . schlsselwrter : emotionales befinden subjektives krankheitserleben angst depressivitt posttraumatische belastungsstrung stereotaktische bestrahlung introduction confrontation with a lifethreatening illness and its treat ment can trigger reactions of extreme anxiety and depression in those affected . 
in the case of radiotherapy in the head area , for example , this is done using a rigid face mask fixed to the radiotherapy table [ 17 ]  . 
these new forms of treatment may involve greater psychosocial stress for the patients . unlike the clinical impact , there have so far only been a small number of studies on how people deal psychologically with radiotherapy [ 31 ]  . 
in one comparative study , prevalence rates for anxiety and depression in tumor patients were estimated at 10% and 21% , respectively , at 1022% / 1750% in patients in general internal medicine , and at 7% / 5% in the general popu lation [ 14 ]  . 
in more recent studies , 20% of 517 cancer patients displayed pathologic levels of anxiety in a questionnaire [ 12 ] , while 32.6% of 227 breast cancer patients showed this level of depression [ 10 ]  . 
 in each study , there were a large number of patients who either reacted with increasing depression as the therapy continued , accompanied by a deterioration in quality of life [ 18 , 20 ] , or who remained troubled by symptoms of anxiety after the com pletion of radiotherapy [ 27 ]  . 
patients who experienced high levels of psychosocial stress at the start of radiotherapy also displayed the same high level of stress during and after therapy , and required constant psychosocial support to improve their quality of life [ 32 ]  . 
with ear , nose and throat tumor patients , who already had high depression values before the start of ther apy , these values rose clearly significantly during treatment and remained high thereafter [ 5 ]  . 
 [ 30 ] were able to prove that psychopathologic comorbidity has a considerably negative impact on radiotherapy patients quality of life , an impact which remains stable as the illness progresses in the longer term [ 26 ]  . 
one factor which strongly affects patients psychological state is the quality of communi cation between doctor and patient [ 24 ]  . according to icd10 , posttraumatic stress disorder ( ptsd ) is the development of characteristic symptoms ( intru sive memories , avoidance , vegetative hyperarousal ) triggered by traumatic events which would be likely to cause pervasive distress in almost anyone ( e.g. , natural disasters , torture , being a victim of sexual attacks or incest , serious accidents or terror ism )  . 
in the 4th edition of the american psychiatric associa tions ( apa ) diagnostic manual ( dsmiv ) [ 1 ] , the criteria for trauma were revised , enabling serious physical illness to be included as a potentially traumatic event . 
trauma is defined by the apa using two criteria : a1 describes the trigger event ( experiencing or witnessing situations involving death , injury , or a threat to physical in tegrity ) , and a2 covers the subjective experience of the person affected , which must include feelings of intense fear , helplessness or horror . in studies , the lifetime prevalence of ptsd for the general pop ulation is taken as between 1% and 11% [ 6 , 19 ]  . 
 for the group most studied in terms of ptsd , breast cancer patients , prevalences are mentioned ranging between 4% [ 28 ] and 16.2% [ 33 ] or even 40% [ 8 ]  . 
however , prevalences differ greatly depending on the survey methods , with results tend ing to be lower in structured interviews ( 2.42.7% ) and higher in selfassessment questionnaires ( 16.323.4% ) [ 21 , 22 , 25 ]  . 
patients emotional state and subjective experience of illness in radiotherapy specifically , the intention was to answer the following questions : ( 1 ) what specific stress situations and support factors do pa tients experience during radiotherapy ? ( 2 ) how strongly are anxiety , depression and symptoms of ptsd expressed in patients after radiotherapy ? ( 3 ) what impact do the type of radiotherapy and the under lying disorder have on this stress ? patients and methods the present work is based on a descriptive , retrospective and correlative crosssectional study . 
the survey was written ; the questionnaires were sent to all patients along with an informa tion sheet about the aims of the study , data protection and the fact that participation was voluntary . 
in the first , there were questions on sociodemographic facts , and aspects of patients subjective experiences during radiotherapy were also record ed using specially developed questions , both openended and multiple choice . 
the reason for the 100 missing questionnaires was , in 45 cases , the death of the patient between treatment and the start of the study and , in 22 cases , patients entering the prefinal stage . 
27.1% of all patients indicated that they were part of a religious community ; 7.5% were actively in volved in religious life in their community . at the time of the survey , an operation had previously been carried out on 137 of the 287 patients to treat their dis order ; 75 had been treated with chemotherapy . 
9.1% of patients underwent radiotherapy in just one session , 29.3% over a short period ( 12 weeks ) , and 61.7% over a longer period ( > 2 weeks )  . 
bedrfnisse der patienten hinsichtlich der gewnschten aufklrung ( freie angaben , n = 57 ) und in bezug auf den umgang mit dem behandelnden arzt ( n = 287 ; mehrfach nennungen mglich )  . needs regarding the patient briefing interestinfactsaboutproceduresandhowthetreatmentworks wishformoreinformationaboutthedisorderandtreatments needforempatheticattention most important aspect in patientdoctor relationship doctortoemanatetrustandreliability doctortohavetechnologicalandprofessionalknowledge doctortoemanatefriendlinessandempathy itisimportanttohaveregularcontactwiththesameperson table 3 . 
only a small number of patients with a benign under lying disorder ( 1.5% ) described themselves as suffering from anxiety , whereas in the two other groups roughly the same number of patients was anxious ( 15% )  . 
for the group with a benign underlying disorder it was the pain ( 45.6% ) , and for the group of patients undergoing stereotactic treatment it was the treatment situation ( 40% )  . 
table 4 provides an overview of the percentage of pa tients with high values suggesting an incidence of anxiety , de pression or ptsd . for anxiety , the share of pathologic values in the overall sample was 9.6%. 
unlike the figures for anxiety , depression showed a mild ( 0.153 ) but statistically ( p = 0.01 ) correlation to age , with older patients suffering more . a pathologic tendency toward stressrelated symp toms and ptsd could be seen in radiotherapy patients , at 22.1% overall , putting them in the expected range for patients following traumatic medical procedures such as heartlung transplants or stem cell transplants ( 1040% )  . 
 [ 16 ] , which showed an increased occurrence of pathologic anxiety and depression in general in this patient group , as well as with results obtained by rolke et al . 
 [ 3 ] , the screening using a questionnaire was well accepted by the patients and revealed considerable need for psychosocial support in this patient group . 22% of patients were above the cutoff point in ptss10 indicated by stoll et al . 
 while that study found individual ptsd symptoms in a large number of patients , only 3% of the sample studied fulfilled the diagnostic criteria for the existence of a ptsd according to dsmiiir . 
patients emotional state and subjective experience of illness in radiotherapy disease , so the higher prevalence of ptsd symptoms in the sample we studied could be due to the severity of their ill ness . 
this idea is supported by the fact that amir & ra mati [ 2 ] , who did not exclude breast cancer patients with a worse prognosis in their study , reported a higher incidence of ptsd , but it is also possible that the ptss10 overesti mates the frequency of posttraumatic stress compared with a structured interview in accordance with dsm or icd cri teria [ 21 , 22 ]  . 
even if not all ptsd symptoms are present , stressrelated symptoms such as intrusive cognitions seem to be factors which keep anxiety at a high level and prevent patients from dealing with their illness as well [ 36 ]  . 
how ever , it may also be necessary for critical reconsideration of the whole concept of applying the trauma model to un derstand the experiences and subjective feelings of cancer patients before and during therapy [ 25 , 28 ]  . patients who had undergone stereotactic radiotherapy did not demonstrate higher values for anxiety , depres sion or pts symptoms than patients treated with conven tional radiotherapy . 
all in all , as expected , it is instead the type of underlying disorder ( malignant or benign ) which affects the extent of psycho logical stress experienced by patients . conclusion we have established that , after radiotherapy , a considerable proportion of patients suffer to a clinically significant degree from anxiety , depression and symptoms of ptsd , causing a significant decrease in their quality of life . 
stage i ( defined as involvement of a single lymph node region ) and stage ii ( defined as involvement of two separate regions confined to one side of the diaphragm ) presentation of fl accounts for ~ 2025% of all cases . 
morphologically , fls , as defined by the world health organization ( who ) classification [ 18 ] , are characterized by a follicular growth pat tern including centrocytes and centroblasts , and are graded from i to iii according to the amount of centroblasts present . 
the present review focuses on the role of radiotherapy ( rt ) in nodal fl grade iiiia and aims to ad dress the issue of the extent of radiation volumes , the issue of adequate doses , and the issue of combinedmodality treat ment approaches . the issue of radiation volumes varying radiation strategies have been used in patients with stage i and ii fl . 
involvedfield irradiation ( ifi : irradiation of all involved sites , i.e. , all lymph node regions of proven clinical involvement ) , extendedfield irradiation ( efi : ifi + adjacent regions of clinically noninvolved lymph nodes , e.g. , supradiaphragmatic mantle field ) , total nodal irradiation ( tni : supradiaphragmatic mantle field + infradiaphragmatic inverted y including the spleen ) , total central lymphoid irra diation ( tcli : tni + abdomen waldeyers ring ) , and total lymphoid irradiation ( tli : tni + whole abdomen + waldeyer ring ) have been applied with curative intent . 
the different irradiation protocols produce excellent local disease control ( ~ 95% ) resulting in progressionfree survival ( pfs ) rates of 3794% , 3782% , and 4075% and overall survival ( os ) rates of 7393% , 4679% , and 4062% at 5 , 10 , and 15 years , respectively . 
interestingly , the longterm results of the small subgroup of patients with stage iii treated with rt alone [ 10 , 17 , 21 , 32 , 39 ] are similar to those with stages i and ii ( table 2 ) but this concept is no longer per sued . to date , there is no consensus concerning the optimal tar get volume in patients with localized fl , since data are mainly collected from retrospective analyses and remain continuing sources of controversy [ 55 ]  . 
moreover , comparability between studies remains difficult due to exertion of different histologi cal classification systems ( real classification , kiel classifica tion , working formulation classification , rappaport classifi cation ) before the introduction of the international consensus in the who classification [ 18 ]  . the main cause for recurrent disease after ifi are re lapses at distant sites out of ifi volumes within 25 years af ter treatment [ 4 , 22 , 34 , 40 , 41 , 59 ] with declining incidence and only few relapses beyond 20 years [ 4 , 28 , 41 , 59 ] , indi cating a proportion of patients ( ~ 4050% ) being cured . 
for example , in the princess margaret series the probabilities of relapse were 11% ( 510 years ) , 6% ( 1015 years ) , and 2% ( > 15 years ) after ifi , respectively [ 41 ]  . 
in retrospective analyses it has been observed that increased target volumes result in a re duction of relapse , but there was no significant influence on os [ 8 , 38 ]  . 
the stanford experience showed that treatment of both sides of the diaphragm was associated with a lower relapse rate ( 23% and 33% ) compared with treatment to one side only ( 52% and 64% ) at 5 and 10 years . 
in this regard , there are concerns that larger irradiation volumes enhance the risk of acute toxic side ef fects ( e.g. , hematotoxicity , gastrointestinal toxicity ) , and late sequelae ( organ toxicity , higher mortality rate , and incidence of secondary malignancies , e.g. , leukemia , solid tumors ) [ 28 ]  . 
interestingly , a large proportion of relapses ( 38 / 41 ; 93% ) involved the side of the diaphragm opposite the original site of the disease and 59% exclusively affected the opposite side of the diaphragm [ 59 ]  . 
patients with more peripherally located fl were treated with efi , whereas patients with involvement of the trunk ( e.g. , mediastinal , mesenteric , paraaortic involvement ) received tcli . 
at 7 years , the risk of distant failure after efi was ~ 20% for patients with stage i / ii disease and was signifi cantly lower in the adjuvantly irradiated lymph node regions compared to nonirradiated sites supporting the effectiveness of enlarged radiation volumes . 
however , quantitative pcr demonstrated the feasibility of clearing pb and bm bcl2 + cells after ifi of the primary site of disease : as a consequence of the elimination of the primary focus , characteristic tumor cell contaminations of pb / bm were absent after treatment in the majority of patients [ 43 ]  . randomized trials comparing ifi with efi / tni / tcli / tli techniques are missing and the longterm results of the german multicenter phase iii trial ( closed in 2007 ) compar ing efi with tli are not yet available . 
to date , there is no evidence for a prognostic superiority of larger irradiation vol umes as compared to irradiation of involved regions only . the issue of radiation dose different radiation doses have been applied in patients with localized fl ( see table 1 )  . 
therefore , the authors recommend a total dose of 30 gy to lymph nodes with suspected subclinical disease and a total dose of 3644 gy to macroscopically involved lymph nodes [ 51 ]  . 
by contrast , other retrospective analy ses could not identify an additional benefit for rt doses > 25 gy to increase local control [ 22 , 48 , 52 ]  . so far , there are no systematic prospective trials available evaluating the effect of radiation dose on local control in fl . 
 the international experience suggests that radiation doses of 2530 gy to subclinical disease and 3640 gy to involved sites are appropriate to control fl disease . the issue of combined radiotherapy / chemotherapy randomized trials with small patient numbers in the 1970s / 1980s and recently published data from nonrandomized trials did not confer a definitive os advantage with additional / adjuvant chemotherapy in patients with earlystage fl [ 3 , 14 , 24 , 26 , 31 , 34 , 60 ]  . 
anderson cancer center provided evidence for a poten tial advantage of a combinedmodality ( cmt ) approach com pared to rt alone with increased freedom from relapse rates at 5 , 10 , and 15 years and no further relapses after 7.5 years [ 2 ]  . 
so far , cmt has not been con vincingly shown to improve treatment results as compared to rt alone . conclusion and perpectives for firstline treatment in earlystage fl , definitive rt in duces complete remissions in the majority of patients ( ~ 95% ) leading to relapsefree survival rates of ~ 4060% at 10 years . 
as in hodgkins disease [ 6 , 7 ] , the international literature for fl [ 53 , 54 ] and updated guidelines of the national comprehensive cancer network recommend ifi , while efi is regarded as optional therapy . 
although the longterm results of the german multicenter phase iii trial comparing efi with tli are pending , it remains questionable whether large irradiation volumes will still be applied in the future . the issue of the doseeffect relationship is not settled by systematic prospective evaluation . 
in summary , radiation dos es ranging between 2530 gy to subclinical disease and 3640 gy to involved sites have been broadly used and proven to be highly effective . in order to improve the established prognostic potential of rt , new treatment approaches for earlystage fl are investi gated . 
the eortc initiated a randomized phase iii trial with lowdose totalbody irradiation ( tbi , 1 , 5 gy ) and ifi ( 2640 gy ) versus ifi ( 2640 gy ) alone based on promising phase ii data [ 44 ]  . 
as a consequence of the success of rituximabcontaining regimens in advanced fl [ 19 , 20 , 29 , 46 ] , the german lowgrade lymphoma study group currently investigates whether the additional application of rituximab may improve the results of ifi alone in earlystage fl ( mir study )  . 
stage i - ii follicular lymphoma : the role of radiotherapy sensitive sites with enhanced risk of acute / late sequelae like the head and neck region / the abdomen , the use of intensitymodu lated therapy [ 45 , 50 ] or tomotherapy [ 49 , 57 ] to minimize sali vary gland tissue and mucosa exposure might be beneficial . strahlentherapie und onkologie original article a new modification of combining vacuum therapy and brachytherapy in large subfascial soft - tissue sarcomas of the extremities maximilian rudert1 , 2 , cornelia winkler3 , boris michael holzapfel1 , 2 , hans rechl2 , peter kneschaurek3 , reiner gradinger2 , michael molls3 , barbara rper3 purpose : to present a modification of a technique combining the advantages of brachytherapy for local radiation treatment and vacuum therapy for wound conditioning after resection of subfascial soft - tissue sarcomas ( sts ) of the extremities . patients and methods : between january and may 2008 , four patients with large ( > 10 cm ) subfascial sts of the thigh underwent marginal tumor excision followed by early postoperative hdr ( high - dose - rate ) brachytherapy ( iridium - 192 ) and vacuum therapy as part of their interdisciplinary treatment . 
the sponge of the vacuum system was used to stabilize brachytherapy applicators in parallel positions and to allow for a maximal wound contraction in the early postoperative phase , thus preventing seroma and deterioration of local dose distribution as optimized in computed tomography - ( ct - ) based three - dimensional conformal treatment planning . 
acute wound complications and late effects according to lent - soma after 48 months of follow - up were recorded . results : the combination of vacuum and brachytherapy was applicable in all patients . 
1518 gy in fractions of 3 gy bid prescribed to 5 mm tissue depth were applied over the next days with removal of the sponge and applicators on days 58 . 
the mean enneking score for functional outcome was 63% ( perfect function = 100% )  . conclusion : the combination of vacuum and brachytherapy is applicable and safe in the treatment of large subfascial sts . key words : soft - tissue sarcoma surgery brachytherapy vacuum therapy brachyvac therapy strahlenther onkol 2010 ; 186 : 2248 doi 10.1007 / s00066 - 010 - 2046 - 0 eine neue modifikation der kombinationsbehandlung aus vakuumund brachytherapie bei groen , tief gelegenen weichteilsarkomen der extremitten ziel : vorstellung einer modifikation der technik der brachytherapie nach resektion subfaszialer weichteilsarkome , die eine lokale strahlentherapie und gleichzeitig eine vakuumtherapie zur wundversorgung ermglicht . patienten und methodik : zwischen januar und mai 2008 wurde bei vier patienten mit einem weichteilsarkom der unteren extremitt ( > 10 cm ) eine marginale tumorresektion durchgefhrt . 
adjuvant erfolgten eine frhe postoperative hdr - ( high - do se - rate - ) brachytherapie ( iridium - 192 ) und eine vakuumtherapie der wunde im rahmen der interdisziplinren tumortherapie . 
entsprechend den lent - soma - kriterien wurden frhe und spte strahlenschden nach 48 monaten erfasst . ergebnisse : die kombination von vakuumund strahlentherapie konnte bei allen vier patienten komplikationslos durchgefhrt werden . 
 1department of orthopedics , university of wrzburg , germany , 2department of orthopedics and traumatology , klinikum mnchen rechts der isar , technical university of munich , germany , 3department of radiation oncology , technical university of munich , germany . received : april 23 , 2009 ; accepted : november 9 , 2009 published online : march 26 , 2010 strahlenther onkol 2010 no . 
modified brachyvac therapy for large extremity sts schlussfolgerung : die kombination von vakuumund brachytherapie stellt ein geeignetes und komplikationsarmes verfahren in der behandlung von groen , subfaszial gelegenen weichteilsarkomen dar . schlsselwrter : weichteilsarkom chirurgie brachytherapie vakuumtherapie brachyvac - therapie introduction large soft - tissue sarcomas ( sts ) are at high risk of local recurrence . 
radiation treatment is a well - established means to improve local control in these cases [ 7 , 18 , 19 , 26 , 28 , 31 , 33 ]  . 
 brachytherapy ( bt ) and intraoperative radiotherapy ( iort ) offer some advantages over external - beam radiotherapy ( ebrt ) alone like minimizing the risk of geographic miss due to interstitial fixation and maximizing normal tissue sparing as steep dose gradients can be achieved [ 32 , 34 ]  . 
except for bone tumors and children the role of chemotherapy is marginal [ 6 , 8 , 40 ]  . in bt , distension of the distance between applicators and tissue at high risk of recurrence might significantly deteriorate the intended dose distribution [ 2 , 9 , 21 ]  . 
to prevent the development of a seroma and to induce wound healing , application of a vacuum system has proven to be successful [ 3 , 16 , 17 , 23 ]  . 
delayed primary wound closure or plastic reconstructive methods can be electively scheduled after assurance of clear resection margins on the pathology report [ 4 , 5 , 11 , 16 , 20 , 25 , 29 ]  . 
vacuum therapy is shown to increase local blood flow , decrease bacterial growth , and promote delivery of oxygen and the growth of granulation tissue [ 14 , 30 , 41 ]  . 
altogether , temporary vacuum therapy in combination with bt , followed by delayed wound closure , increases efficacy of oncologic and reconstructive procedures and improves safety [ 24 , 25 , 35 , 36 ]  . therefore , we pursued a refined approach of combining bt and vacuum therapy ( brachyvac ) , inserting the required number of bt applicators into the polyurethane sponge of a vacuum system ( figure 1 )  . 
here we report on our experience with four consecutive patients undergoing brachyvac therapy after resection of large sts . patients and methods from january to may 2008 , four patients with histologically confirmed large sts of the thigh were assigned to bt and vacuum therapy as part of their individual cancer treatment . 
the brachyvac system was adjusted to the defect extension and placed into the tumor bed ( figure 2 ) with the bt applicators following the long axis of the excised tumor . 
finally , a subatmospheric pressure of 75125 mmhg was applied . the following day , a planning computed tomography ( ct ) was performed , generating a three - dimensional image dataset of the region with a slice thickness of 5 mm ( somatom sensation 16 , siemens )  . 
using the software brachyvision ( varian ) , the bt catheters were identified , contoured , and a treatment plan generated for a dose prescription to 5 mm tissue depth . 
after three - dimensional treatment planning on the 1st postoperative day , hdr - bt was applied in five to six fractions of 3 gy over the next 3 days . 
der grne drainageschlauch wird an die vakuumpumpe angeschlossen . high - dose - rate brachytherapy ( hdr - bt ) with iridium - 192 ( gammamed plus , varian ) was delivered in fractions of 3 gy bid to a total dose of 1518 gy ( minimal interfractional interval 6 h )  . 
the brachyvac system was removed in a second surgical intervention shortly after the last fraction . patient demographics , tumor characteristics , treatment factors , and course of disease were evaluated . 
for quantification of possible late toxicity , the lent - soma classification was applied ( 0 = no toxicity , 4 = severest complication ) [ 12 , 27 ]  . extremity function was analyzed using the enneking score , assigning 05 points ( 5 = best result , no functional limitation ) to each of six categories : pain , functional and emotional acceptance , supports , walking , and gait . 
the sum of the points divided by the maximal number gives an overall functional value ( i.e. , 100% = perfect function ) [ 13 ]  . results patient and tumor characteristics are given in table 1 . 
nevertheless , local control of the primary tumor site was still felt to be an important aim . tumor resection and brachyvac therapy macroscopically , all tumors were excised completely , but as expected resection margins were close ( 1 mm ) or positive in three patients , additive ebrt was started with a median time interval of 50 days after the last bt fraction . 
the other patient ( h.p. ) developed a septic enterocolitis on prophylactic antibiotics with evidence of clostridium difficile , with delay of ebrt due to reduced general condition , but healing of the tumor resection site was uneventful . 
three patients were actually able to participate in prolonged activities , such as taking a longer walk or swimming . discussion in sarcomas , several techniques have been employed in order to improve outcome , including intensity - modulated radiotherapy , tomotherapy , neutrons , protons , bt and iort [ 1 , 10 , 37 , 38 , 39 , 42 ]  . 
although the results are appealing , for iort a dedicated operating room for radiotherapy procedures is required , which is rarely the case [ 15 ]  . it also has some drawbacks concerning handling , target volume coverage and the theoretical disadvantage of a missing fractionation effect . 
after marginal resection of the tumor , the bt catheters per se or within a flap were placed directly on the deep resection plane with the vacuum sponge on top for wound coverage [ 25 , 35 ]  . 
we therefore introduced a new combined technique with insertion of bt catheters in longitudinal axis within the vacuum sponge which was cut to size appropriate for filling the cavity of the tumor resection . 
ideally , this system allows for irradiation not only of the deep plane but of all initial contact planes of the tumor , providing a homogeneous dose distribution , built up from within the vacuum foathus , the risk of overdosages to critical structures like nerves should be minimized . 
the vacuum system is known to support tissue granulation in wounds , the hydrophobic open pore structure ( 400600 ) helps facilitate exudate removal and provides a uniform distribution of subatmospheric pressure at the wound site . 
thus , the expectedly close or positive resection margins are held in place right next to the bt catheters , improving the efficacy of radiotherapy and facilitating the appropriate oncologic therapy . in our pilot study , the method seems to be feasible and safe . 
to further reduce the risk of wound infection , subsequently , the skin entry points of bt catheters are planned to be at distance rather than integrated into the surgical incision . 
modified brachyvac therapy for large extremity sts the bt catheters will be situated within the sponge may be varied according to individual necessities given by tumor site and proneness to critical structures . 
long - term results regarding the oncologic outcome have to be awaited . strahlentherapie und onkologie original article radiotherapy for oligometastatic disease in patients with spinal cord compression ( mscc ) from relatively radioresistant tumors katja freundt1 , thekla meyners1 , amira bajrovic2 , hiba basic3 , johann h . 
 since cancer patients with oligometastatic disease have a bet ter survival prognosis than those with more widespread meta static disease , these patients are candidates for longercourse radiotherapy [ 18 ]  . another important aspect that needs to be considered to select the optimal treatment regimen is the radiosensitivity of the primary tumor type . 
our previous studies of patients with mscc from renal cell carcinoma or colorectal cancer sug gested that shortcourse radiotherapy was similarly effective as longercourse radiotherapy with respect to posttreatment motor function [ 11 , 17 ]  . 
a re cent study presented data regarding decompressive surgery for mscc from renal cell carcinoma ( n = 21 ) , gastrointestinal tumors ( n = 13 ; colon cancer ) , and malignant melanoma ( n = 7 ) [ 2 ]  . 
furthermore , decompressive surgery is indicated only in 1015% of mscc patients [ 9 ]  . highprecision radiotherapy techniques such as stereo tactic body radiotherapy have been mostly used for pain re lief , not for relief of motor deficits due to mscc [ 3 , 4 , 8 ]  . 
thus , highprecision radiotherapy may also not be optimal for mscc from relatively radioresistant tumors , possibly due to the small safety margins that may not include the entire microscopic tumor . 
 oligometastatic disease has been defined as an involvement of only one to three vertebrae and absence of further bone or visceral metastases . patients and methods of a total of 206 patients who received radiotherapy alone for mscc from renal cell carcinoma , colorectal cancer , or malignant melanoma , 51 had oligometastatic disease . 
the 21 patients who were treated with 30 gy in ten fractions were ret rospectively compared to those patients who received higher doses such as 37.5 gy in 15 fractions or 40 gy in 20 fractions ( n = 30 )  . 
further crite ria for inclusion were mscc of the thoracic or lumbar spine , no prior surgery or radiotherapy to the involved sites of the spine , confirmation of mscc by computed tomography ( ct ) or magnetic resonance imaging ( mri ) , and administration of dexamethasone ( 1232 mg / day ) during radiotherapy . 
the radia tion schedule varied based on the discretion of the treating physician . radiotherapy was performed with linear accelerators and delivered through a single posterior field or parallel opposed fields depending on the depth of the spinal cord . 
motor function was evaluated before and up to 6 months after radiotherapy with a fivepoint scale [ 22 ] : grade 0 : normal strength ; grade 1 : ambu latory without aid ; grade 2 : ambulatory with aid ; grade 3 : not ambulatory ; grade 4 : paraplegia . 
regarding functional outcome , both uni and multi variate analysis were performed with the orderedlogit model , as the data for functional outcome are ordinal ( 1 = deteriora tion , 0 = no change , 1 = improvement )  . 
the prognostic factors found to be significant ( p < 0.05 ) in the univariate analysis were included in a multivariate analysis , which was performed with the cox proportional hazards model . 
the patients were followed until death or for median 12 months ( range : 638 months ) in those patients being alive at their last followup . results after radiotherapy , motor function improved in 23 patients ( 45% )  . 
on univariate analysis , improved motor function was associated with a longer interval from tumor diagnosis to radiotherapy of mscc ( p = 0.010 ) and a slower ( > 14 days ) development of motor deficits before radiotherapy ( p = 0.025 ; table 2 )  . 
on univariate analysis , none of the investigated potential prognostic factors includ ing the radiation regimen ( p = 0.75 , figure 2 ) was significantly associated with local control ( table 3 )  . 
ecog : eastern cooperative oncology group . improvement n ( % ) no change n ( % ) deteriora tion n ( % ) pvalue 30 gy / 10 fractions higher doses 18 ( 49 ) 5 ( 36 ) 17 ( 46 ) 6 ( 43 ) 2 ( 5 ) 3 ( 21 ) 0.19 improvement no change deterioration 30 gy / 10 fractions higher doses figure 1 . 
vergleich von 30 gy in zehn fraktionen und hheren dosen hinsichtlich der lokalen kontrolle . val from tumor diagnosis to radiotherapy of mscc ( p = 0.032 ) , pretreatment ambulatory status ( p = 0.025 ) , and a slower de velopment ( > 14 days ) of motor deficits before radiotherapy ( p = 0.037 ; table 4 )  . 
on multivariate analysis of survival , performance status ( risk ratio [ rr ] : 3.40 ; 95% ci : 1.209.74 ; p = 0.022 ) and interval from tumor diagnosis to ra diotherapy ( rr : 1.65 ; 95% ci : 1.032.67 ; p = 0.039 ) were sig nificantly associated with survival . 
 it may be speculated whether an escalation of the radiation dose of conventional radiotherapy can improve the outcomes of patients with mscc from relatively radioresistant tumors . mscc patients with oligometastatic disease have a rela tively favorable prognosis [ 16 ]  . 
vergleich von 30 gy in zehn fraktionen und hheren dosen hinsichtlich des berlebens . with oligometastatic disease , improvement of motor function was observed only in 29% and 14% of patients , respective ly [ 11 , 17 ]  . 
rt for oligometastatic mscc from relatively radioresistant tumors at risk of including hidden biases , despite the fact that the distribution of the other potential prognostic factors was not significantly different in both dose groups . only very little data are available with respect to an es calation of the radiation dose for metastases from relatively radioresistant tumors . 
in a retrospective study of 78 patients with metastases at different sites from renal cell carcinoma , a higher biologically effective dose was not a predictor of re sponse to radiotherapy [ 24 ]  . 
improved posttreatment motor function was associated with a longer interval from tumor diagnosis to radiotherapy on both uni and multivariate analysis , and with a slower development of motor deficits on univariate analy sis . 
most of these prognostic factors have been previously described [ 13 , 15 ]  . conclusion escalation of the radiation dose beyond 30 gy in ten fractions did not improve motor function , local control , and survival in mscc patients with oligometastatic disease from relatively radioresistant tumors . 
further studies including different treatment modalities are required to define the optimal ther apy for these patients . strahlentherapie und onkologie original article treatment results of radiation therapy for muscle invasive bladder cancer tanja langsenlehner1 , carmen dller1 , franz quehenberger2 , heidi stranzllawatsch1 , uwe langsenlehner3 , karl pummer4 , karin s . 
weiters zeigte sich eine signifikante assoziation zwischen hydronephrose , lymphgefinvasionunddemauftreteneineslokalrezidivs.dasaktuarischeprogressionsfreie3jahresber lebenundgesamtberlebenbetrugen40 , 1%und56 , 9% . 1universityclinicoftherapeuticradiologyandoncology , medicaluniversityofgraz , austria , 2instituteformedicalinformatics , statisticsanddocumentation , medicaluniversityofgraz , austria , 3internaloutpatientdepartment , steiermaerkischegkk , graz , austria , 4departmentofurology , medicaluniversityofgraz , austria . received : may 25 , 2009 ; accepted : november 26 , 2009 published online : march 26 , 2010 strahlenther onkol 2010 no . 
radiotherapy of muscleinvasive bladder cancer schlussfolgerung : dieprimreperkutanebestrahlungstellteineeffektivebehandlungsoptioninbezugaufdielokalekontrolle unddasberlebenbeipatientenauchfortgeschrittenenaltersmitlokalfortgeschrittenemblasenkarzinomdar , diefreineradi kalezystektomienichtgeeignetsind . schlsselwrter : blasenkarzinom primre perkutane strahlentherapie lokale kontrolle organerhalt introduction in europe and in the usa , bladder cancer is the fourth most common cancer in men and the eighth most common malig nancy in women [ 22 ]  . 
at the time of diagnosis , 20% of patients present with muscleinvasive tumors , and without treatment > 85% of patients with invasive disease succumb to their dis ease within 2 years after diagnosis [ 49 ]  . 
the standard therapy for patients with muscleinvasive cancer in most institutions is still radical cystectomy and pelvic lymphadenectomy provid ing 5year overall survival rates of 60% [ 47 , 49 ]  . new surgical techniques emerged rapidly during the last years with the development of continent orthotopic urinary diversion and nervesparing techniques to improve both func tional results and quality of life [ 3 , 4 , 18 ] , but even the con struction of a neobladder cannot substitute for the original urinary bladder . bladderpreserving strategies such as radiotherapy and radiochemotherapy combined with a transurethral resection of the bladder tumor ( turbt ) have been shown to offer an attractive alternative to radical cystectomy providing complete response rates of 6085% , 5year survival rates of 5060% , and survival rates with an intact bladder of 4045% [ 24 , 25 , 34 , 35 , 40 , 51 ]  . 
although there are no randomized trials com paring radical cystectomy with bladderpreserving therapy , longterm data show that overall and diseasespecific survival rates in radical cystectomy series of patients with t2t4a tu mors are comparable to those achieved by bladderpreserving strategies [ 7 , 14 , 27 , 28 ]  . radiotherapy is often limited to patients who are medi cally unfit and / or who are considered unresectable represent ing a negatively selected subgroup . 
although the treatment results are inferior to better selected patients , radiotherapy has been shown to offer longterm tumor control and survival even in this highrisk population [ 13 , 35 ]  . the aim of the present investigation was to retrospective ly analyze the treatment results of radiotherapy for locally ad vanced bladder cancer in patients not suitable for cystectomy and to evaluate prognostic factors . patients and methods the cohort was comprised of 75 patients ( female , n = 17 ; male , n = 58 ) with histologically confirmed , muscleinvasive transitional cell carcinoma of the bladder who received exter nalbeam irradiation at the university clinic of therapeutic radiology and oncology , medical university of graz , aus tria , between 1997 and 2007 . the included patients had inoperable t4b tumors or were medically unfit for radical surgery due to age and reduced performance status and / or comorbidities . 
details on tumor characteristics are given in table 1 . radiation treatment externalbeam radiation with 18 mv photons was used to encompass the tumor and the pelvic lymph nodes in a fourfieldbox technique to 5050.4 gy , then a conedown was applied to boost the bladder to 7070.4 gy with an an terior and two lateral fields . 
indi vidually manufactured , focused cerrobend blocks were used to shield the surrounding tissues and were replaced in 1998 by threedimensional conformal treatment planning and the use of multileaf collimators . 
none of the included patients re ceived simultaneous chemotherapy . acute and late genitourinary and gastrointestinal toxicity was graded according to standard radiation therapy oncol ogy group ( rtog ) criteria . statistical analysis all timedependent event rates and median time to event were estimated by the kaplanmeier method . 
rt : radiotherapie ; tis : carcinoma in situ . clinicallymphnodeinvolvement transurethralresectionspriortort characteristics tumorstage histologicalgrade t2 t3 t4 g2 g3 g4 n0 n1 n2 r1 r2 yes no yes no yes no yes no one two morethantwo marginstatus multifocality associatedtis lymphvesselinvasion hydronephrosis patients n ( % ) 34 ( 45 ) 32 ( 43 ) 9 ( 12 ) 8 ( 11 ) 60 ( 80 ) 7 ( 9 ) 62 ( 83 ) 6 ( 8 ) 7 ( 9 ) 29 ( 39 ) 31 ( 41 ) 15 ( 20 ) 13 ( 17 ) 62 ( 83 ) 6 ( 8 ) 69 ( 92 ) 6 ( 8 ) 69 ( 92 ) 20 ( 27 ) 55 ( 73 ) 24 ( 32 ) 51 ( 68 ) time intervals were calculated from the end of radiotherapy . 
 local control was defined as the absence of local bladder failure , local recurrencefree survival as the time interval from the end of radiation treatment to bladder recurrence , local progressionfree survival as the time interval from the end of radiation treatment to bladder recurrence or bladder tumor progression , progressionfree survival as the time in terval from the end of radiation treatment to locoregional and / or distant failure , and distant metastasesfree survival as the interval from the end of radiotherapy to distant disease progression . the influence of prognostic factors on event rates was as sessed by a univariate cox model , using the score criterion for testing . 
a returb to distinguish between complete responders and noncomplete responders was not demanded in the present series , as the included patients were not considered to be suitable for further treatment options such as sal vage cystectomy . 
20% of patients ( 4 / 20 ) with lymph vessel inva sion , 25% of patients ( 6 / 24 ) with hydronephrosis and 42% of patients ( 26 / 62 ) with r2 resection had no evidence of disease progression ( local and / or distant )  . 
none of the investigated parameters was a significant predictor of overall survival or distant metastases . all patients were assessed for acute radiationinduced toxicity , 50 patients were assessed for late toxicity after 1 year and 19 patients after 3 years . 
acute gastrointestinal ( n = 15 ) and / or genitourinary toxicity ( n = 21 ) grade 2 was found in 33% of patients ( 25 / 75 )  . 
 in 37% of patients , late radiationinduced bladder toxici ty rtog 1 was observed , and 17% of patients ( 13 / 75 ) expe rienced late genitourinary side effects grade 2 . 
in 15% of pa tients ( 11 / 75 ) , late radiationinduced gastrointestinal toxicity rtog 1 was found , and 7% of patients ( 5 / 75 ) experienced late gastrointestinal side effects grade 2 ( table 4 )  . 
eleven patients were followed for > 5 years and three of them ( 27% ) had developed radiationinduced late toxicity grade 3 . three patients developed a stenosis of the sigmoid colon re quiring surgical intervention . 
in 19% of patients ( 14 / 75 ) , place ment of a nephrostoma was necessary ; in two patients for hydro nephrosis due to fibrosis , and in twelve patients because of local recurrence . 
currently , data from randomized trials comparing cystectomy with bladderconserving therapy are not available , but in a cochrane analysis by shelley et al . , an overall survival benefit has been demonstrated with radical surgery , however , it has to be considered that only three trials were included for analysis [ 44 ]  . by advances in perioperative management , cystectomy has been shown to be suitable and to result in acceptable out come in terms of qualitiy of life and survival even in elderly patients [ 23 , 46 ] despite a higher risk of perioperative mortal strahlenther onkol 2010 no . 
how ever , a subset of patients present with inoperable tumors or are unfit for radical surgery due to serious comorbidity or ad vanced age associated with reduced preformance status and high operative risk . 
these patients are commonly referred to local radiotherapy , and even in this negatively selected group externalbeam radiotherapy has been shown to be feasible and effective providing local control rates ranging from 50% to 65% and overall survival rates ranging from 36% to 69% at 3 years [ 13 , 17 , 27 , 30 , 35 , 36 ]  . currently , efforts are ongoing to optimize irradiation techniques and fractionation regimens to further improve tu mor control and survival [ 11 , 12 , 37 , 45 , 54 ]  . 
more recently , however , it has been hypothesized that the differences in the outcome between different radiation schedules might be more related to the total dose than to the fractionation regimen [ 40 ]  . 
in the pres ent series , conventionally fractionated radiotherapy provided complete local tumor remission in 65% of patients leading to a 3year local control rate of 53% and has been found to be feasible even in elderly patients . 
who reported a 3year local control rate of 56% in patients using an acceler ated regimen [ 35 ]  . in several phase ii studies and one phase iii study , con comitant radiochemotherapy has been reported to increase the rate of complete responders as compared to radiotherapy alone leading to a significantly improved overall survival [ 31 , 34 , 4042 ]  . 
the only prospective , randomized comparison of radiotherapy alone versus concomitant chemoradiation in bladder cancer demonstrated an improved local control rate when cisplatin was given in combination with radiotherapy [ 9 ]  . 
cisplatinbased chemotherapy was not administered in the patients who were included in the present analysis because of contraindications such as renal dysfunction , peripheral neu ropathy , cerebrovascular or cardiovascular disease , hearing disorder , hematologic disease , or infections . it has to be taken into account that most studies on chemoradiation included patients who were able to receive a platinumbased chemotherapy and to undergo surgery in case of persistent disease after initial chemoradiation making the comparison with the negatively selected patient group in the present study difficult . 
combinations of radiotherapy with these novel radiosen sitizing agents might provide future improvements in tumor control and survival , especially for patients with medical co morbidities which preclude chemotherapy . findings of previous studies indicated that hydronephro sis and incomplete turbt might be inversely associated with tumor control [ 2 , 7 , 43 ]  . 
similar results have been obtained in the present series , however , associations between tumor stage , grade , associated tis , and local tumor control could not been found . 
currently , the prediction of radiation response is limited to the use of tradi tional factors such as tumor stage , completeness of turbt , absence of hydronephrosis , and pelvic lymph node involve ment . 
recently , the index of apoptotic tumor cells and the ex pression of regulators of apoptosis and proliferation markers have been reported to be associated with local tumor control [ 6 , 39 , 52 , 53 ] , and it might be helpful to have additional mo lecular markers to aid in predicting clinical response and to identify patients who will benefit most from radiotherapy or combined radiochemotherapy . definitive radiotherapy for bladder cancer has its merits but can be associated with several side effects . 
patients with a history of multiple transurethral resections prior to radiotherapy have been sug gested to be predisposed to develop acute radiation cystitis , and are also at higher risk to suffer from bladder shrinkage thereafter [ 38 ]  . 
the high frequency of late side effects has to be related to the relatively high dose of 70 gy delivered to the entire bladder that makes it essential to reduce the total dose to the bladder . 
to avoid an impairment of tumor control , combina tions with radiosensitzing agents will be helpful . furthermore , it could be considered to reduce the bladder treatment volume by selectively boosting the tumorcarrying bladder tissue . 
previous results indicated that in patients with solitary bladder tumors , reduction of the high dose volume to the bladder tumor area does not impair treatment efficacy [ 5 , 19 , 50 ]  . 
interesting new approaches being explored include the use of partialbladder radiotherapy , brachytherapy , and proton therapy [ 5 , 10 , 19 , 21 , 37 , 50 ]  . 
radiotherapy of muscleinvasive bladder cancer conclusion the current data show that external radiotherapy is effective in achieving tumor control in patients with locally advanced bladder cancer not suitable for radical cystectomy and it was found to be feasible even in elderly patients . 
to minimize radiation toxicity , it will be necessary to reduce the total dose to the bladder and / or to reduce the high dose volume to the bladder tumor area . 
further future efforts should be directed to identifying molecular markers predictive of radiation re sponse to enable a selection of patients with a high risk of recurrence . strahlentherapie und onkologie original article is grading of breast fibrosis with mammography feasible ? ulrike hoeller1 , barbara grzyska2 , joern lorenzen2 , antje kuhlmey1 , winfried alberti1 , gerhard adam2 purpose : to establish a grading system for mammographic fibrosis and correlate it with clinical fibrosis . 
 patients and methods : analogous to the lent / soma scale a four - tiered scoring scale of breast fibrosis in mammography ( g0 = absent , g1 = barely increased density , g2 = definitely increased density to g3 = very marked density ) was established by two observers in a group of 16 patients . 
independently and blinded to clinical results , three observers scored the fibrosis in mammograms of further 31 patients examined by one radiation oncologist in a cross - sectional follow - up study . 
the correlation of mammography with clinical grading should be further evaluated with more objective clinical reference tools . key words : mammography fibrosis breast cancer lent / soma strahlenther onkol 2005 ; 181 : 30712 doi 10.1007 / s00066 - 005 - 1312 - z kann die radiogene fibrose nach brusterhaltender therapie mit mammographie klassifiziert werden ? ziel : es wurde untersucht , ob die radiogene fibrose der mamma nach brusterhaltender therapie anhand von mammographien klassifiziert werden kann . patienten und methodik : analog lent / soma formulierten untersucher 1 und 2 bei 16 patientinnen eine vierteilige klassifikation der fibrose der gesamten mamma ( g0 = keine , g1 = kaum , g2 = deutlich bis g3 = stark sichtbare retikulre zeichnungsvermehrung ) und whlten referenzmammographien aus . 
drei untersucher werteten unabhngig voneinander und in unkenntnis des klinischen befunds die untersuchungen von 31 patientinnen vor operation und median 8 jahre ( spanne 415 jahre ) nach strahlentherapie aus . 
die interobserver - variabilit und die korrelation von mammographischem und klinischem befund wurden mit cohens gewichtetem kappa ( ck ) bestimmt . alle patientinnen hatten eine tumorektomie mit axilladissektion bei mammakarzinom t12n01 . 
das alter betrug im median 55 jahre , die nachbeobachtungszeit 8 jahre ( 415 jahre )  . ergebnisse : 14 von 31 patientinnen hatten eine palpable fibrose , zwlf g1 und zwei g2 . 
eine mammographische fibrose g1 bestand bei 12 / 12 / 18 patientinnen ( fr untersucher 1 / 2 / 3 ) und g2 bei 9 / 10 / 2 patientinnen . 
die interobserver - korrelation von 1 department of radiotherapy and radiooncology , center of radiology , university hospital eppendorf , hamburg , germany , 2 department of diagnostic and interventional radiology , center of radiology , university hospital eppendorf , hamburg , germany . received : may 3 , 2004 ; accepted : february 2 , 2005 strahlenther onkol 2005 no . 
mammographic grading of fibrosis untersucher 1 und 2 , die den score entwickelt hatten , war gut ( ck 0 , 64 , 95% - konfidenzintervall 0 , 40 , 88 )  . 
the late effects of normal tissue / subjective objective management analysis ( lent / soma ) scoring system includes mammography in the analysis category but does not specify the assessment of skin density and fibrosis other than yes / no [ 16 ]  . 
the median age at the time of follow - up was 55 years ( range 4584 years ) , the median time between radiotherapy and follow - up examination by the radiation oncologist 8 years ( range 415 years )  . fibrosis of the entire breast as opposed to circumscript fibrosis was scored according to the lent / soma classification : g1 = barely palpable increased density , g2 = definitely increased intensity and firmness , g3 = very marked density , retraction and fixation [ 16 ]  . 
 photons beam quality cobalt 2.5 gy dose per fraction 1.82 gy reference dose maximum dose ( central plane ) tamoxifen adjuvant therapy chemotherapy 34 patients 13 patients 45 patients 2 patients median 55 gy ( range 5060 gy ) median 57.7 gy ( range 5269.8 gy ) 14 patients 2 patients observers agreed on mutual interpretation of the scores by examining and discussing 40 patients jointly . 
the mammograms before surgery and at the time of the follow - up examination by the two radiation oncologists are the study group . fibrosis was defined as sharply defined , increased trabecular thickening [ 21 ]  . 
the mammograms of all 16 patients who were examined by one radiation oncologist were discussed by an experienced radiologist and one radiologist with basic knowledge of mammography ( observers 1 and 2 ) to establish a subjective score of fibrosis , analogous to the lent / soma score ranging from g0 = absent , g1 = barely increased density , g2 = definitely increased density to g3 = very marked density . 
mammographic grading of fibrosis fibrosis g1 , low parenchyma density fibrosis g1 , high parenchyma density fibrosis g2 , low parenchyma density fibrosis g2 , high parenchyma density grade 03 were selected for a patient with dense and nondense breast parenchyma each . 
fibrosis fully developed by a median of 6 years after radiotherapy ( range 314 years ) in 24 ( 23 ) patients ( observers 1 and 2 ) , and partly regressed in 1 / 24 patients ( observer 1 ) and 4 / 23 patients ( observer 2 ) , respectively . 
mammographic grading of fibrosis interobserver variation interobserver correlation of grading of fibrosis was fair for observers 1 and 2 who had agreed upon a consensus ( cohens weighted kappa 0.64 ; table 3 )  . 
basic interobserver correlation was estimated with pretreatment breast density classification ( acr ) independently of grading fibrosis and proved very good ( cohens weighted kappa 0.730.8 ; table 3 )  . 
though the location of circumscript fibrosis was recorded , a correlation with the dose distribution was not possible , because dose was calculated in the central plane only . the patients were selected from a larger study group ( 287 patients ) , because complete mammography follow - up studies were available . 
in short , the crude rate of late effects ( lent / soma ) was as follows : fibrosis of the entire breast g1 28% , g2 9% , g3 1% , telangiectasia 20% , pigmentation 22% , and atrophy / retraction g1 57% , g2 16% , g3 4% , breast edema 4% . 
in multivariate analysis , only dose per fraction was a significant risk factor ( not beam quality , patients age at therapy , chemo - / hormone therapy )  . 
results were updated in a follow - up study [ 5 ]  . correlation of mammography and clinical findings the correlation of clinical and mammography scoring was weak and for all observers alike ( cohens weighted kappa 0.320.42 ; table 5 )  . discussion the changes in mammographic pattern after breast - conserving surgery and radiotherapy have been studied extensively [ 14 , 10 , 12 , 14 , 17 ]  . 
our study group had yearly mammograms and a long median follow - up of 8 years ( range 415 years ) , so that resolution of edema and development of fibrosis were readily distinguished . 
 observer 1 fibrosis ( patients ) observer 2 sum observer 3 sum observer 2 sum 4 7 2 3 9 2 9 7 3 7 1 1 2 observer 3 fibrosis ( patients ) tween radiotherapy and complete development of fibrosis was longer than previously described [ 24 , 20 ]  . 
previous reports have graded parenchymal density either according to the intensity ( slight , moderate and pronounced ) [ 1 ] or according to its extent ( fraction of projected area of the breast occupied by water density tissue ) [ 12 ]  . 
in order to provide a well - defined and reproducible description of grading , reference mammograms were selected . interobserver correlation was fair for the observers who had agreed upon a consensus . 
further evaluation of the proposed grading by other groups could clarify this issue . the aim of the study was to explore whether classification of fibrosis by palpation can be objectified with mammography . 
though care was taken to minimize this effect by reducing the number of examiners , the evaluation of fibrosis with more objective tools such as a tissue compliance meter might render different results [ 13 ]  . 
 acr 12 observer 1 fibrosis ( patients ) acr 34 observer 1 fibrosis ( patients ) 1 3 1 5 4 4 1 3 6 acr 12 observer 3 fibrosis ( patients ) acr 34 observer 3 fibrosis ( patients ) table 5 . 
interobserver correlation of scoring fibrosis ( g03 ) with mammography and clinical criteria according to the lent / soma classification ( g03 ) in 31 patients , estimated with cohens weighted kappa . 
 strahlentherapie und onkologie originalarbeit prognosefaktoren beim operierten und adjuvant bestrahlten zervixkarzinom eine retrospektive analyse von 298 operierten und nachbestrahlten patientinnen gabriele hnsgen , konstanze richter , reinhard gerlach , thomas kuhnt , jrgen dunst1 ziel : analyse von risikofaktoren , die bei patientinnen mit operierten und nachbestrahlten zervixkarzinomen einen einfluss auf die lokale kontrollrate und das gesamtberleben hatten . patienten und methodik : retrospektiv wurden die verlufe von patientinnen ausgewertet , die zwischen 1980 und 1993 in der klinik fr strahlentherapie der universitt halle - wittenberg behandelt worden waren . 
die lymphknotenmetastasierung war in der mehrfaktoriellen analyse ( cox - regression ) mit einem relativen risiko von 3 , 06 ein unabhngiger prognosefaktor ( p < 0 , 01 ) ; fr das grading g1 / g2 versus g3 / g4 ergab sich ein relatives risiko von 1 , 7 ( p = 0 , 087 ) und fr die tumorgre pt1 vs . 
der lymphonodektomie kommt eine grere diagnostische und wahrscheinlich weniger therapeutische bedeutung zu . schlsselwrter : zervixkarzinom adjuvante strahlentherapie lymphknotenmetastasierung strahlenther onkol 2005 ; 181 : 28592 doi 10.1007 / s00066 - 005 - 1281 - 2 prognostic factors after surgery and adjuvant radiotherapy in cervical cancers . 
a retrospective analysis of 298 patients after surgery and adjuvant radiotherapy purpose : to determine prognostic factors in patients with cervical cancer treated with surgery followed by radiotherapy . patients and methods : in a retrospective analysis , patients treated at the department of radiotherapy , university of halle wittenberg , germany , from 1980 through 1993 were evaluated for local control , survival and treatment sequelae with special emphasis on prognostic factors . 
a value of lymphadenectomy for survival in this group of irradiated patients could not be established . key words : cervical carcinoma surgery and irradiation lymph node metastasis einleitung das zervixkarzinom ist nach dem mammaund endometriumkarzinom das dritthufigste karzinom der frau [ 1 ]  . 
 neben den klassischen therapieoptionen der operation und der strahlentherapie hat sich in den letzten 5 jahren die chemotherapie etabliert , wobei die kombination einer strahlentherapie mit einer platinhaltigen chemotherapie sowohl in der definitiven als auch in der adjuvanten situation die besten resultate zu haben scheint [ 4 , 13 , 14 , 16 , 19 , 31 , 33 ]  . 
 [ 28 ] wird die lokalrezidivquote durch die radiatio gesenkt , ohne einen einfluss auf das gesamtberleben zu haben . ziel der vorliegenden retrospektiven analyse war die evaluation von prognosefaktoren bei patientinnen , die nach operation eines zervixkarzinoms einer adjuvanten strahlentherapie unterzogen wurden . 
es sollten insbesondere postoperative histologische kriterien fr eine patientinnengruppe mit hohem risiko definiert werden , die als potentielle risikogruppe zustzlich zur strahlentherapie fr eine chemotherapie in frage kme . die stadieneinteilung erfolgt zum gegenwrtigen zeitpunkt einzig beim zervixkarzinom entsprechend den kriterien der figo klinisch - diagnostisch [ 37 ]  . 
fast die hlfte aller patientinnen ( 46 , 3% ) konnte 5 jahre beobachtet werden . das mittlere alter der patientinnen betrug 46 jahre ( 2381 jahre ) , mit einem hufigkeitsgipfel zwischen dem 30 . 
 histologie die histologische untersuchung der operationsprparate ergab in 241 fllen ( 80 , 9% ) ein plattenepithelkarzinom und bei 37 patientinnen ( 12 , 4% ) ein adenokarzinoin 20 fllen ( 6 , 7% ) zeigten sich seltene karzinomformen wie dimorphe ( n = 10 ) , mukoepidermoide ( n = 6 ) und undifferenzierte ( n = 4 ) karzinome ( tabelle 1 )  . 
gut differenzierte karzinome bestanden bei 13 ( 4 , 4% ) , mig differenzierte bei 73 ( 24 , 5% ) , schlecht differenzierte bei 82 ( 27 , 5% ) und undifferenzierte bei 36 ( 12 , 1% ) der patientinnen . 
 alter : 46 jahre ( 2381 jahre ) < 35 jahre > 60 jahre histologie plattenepithelkarzinome adenokarzinome sonstige karzinome differenzierungsgrad g1 / g2 g3 / g4 keine angaben stadienverteilung pt1a + b pt2a + b pt3 + 4 fehlwerte lymphknotenbefall n ( + ) n ( ) keine angaben lokalisation der lymphknotenmetastasen einseitig beidseitig keine angaben anzahl der lymphknotenmetastasen 1 2 34 keine angaben 25 56 241 37 20 86 118 94 174 116 6 2 79 162 9 35 24 20 24 12 5 38 8 , 4 18 , 8 80 , 9 12 , 4 6 , 7 28 , 9 39 , 6 31 , 5 58 , 4 38 , 9 2 , 0 0 , 7 31 , 6 64 , 8 3 , 6 14 , 0 9 , 6 8 , 0 9 , 6 4 , 8 2 , 0 15 , 2 ben . 
eine bersicht ber die anzahl und verteilung der lymphknotenmetastasen ist tabelle 1 zu entnehmen . die untersuchung zeigte eine korrelation zwischen der anzahl der entfernten lymphknoten und deren metastatischem befall : wurden bis zu 20 lymphknoten ( n = 15 ) entfernt , fanden sich nur bei drei patientinnen metastasen ( 20% ) ; wurden bis zu 30 lymphknoten operiert ( n = 36 ) , zeigte sich bei 13 ( 36% ) , bei bis 40 entfernten lymphknoten ( n = 66 ) bei 29 patientinnen ( 44% ) eine lymphknotenbeteiligung . strahlentherapie die indikation zur adjuvanten bestrahlung wurde auf der basis des histologischen operationsbefunds gestellt . 
r2 - resektion und bei zweizeitigen operationsverlufen . die hochvolttherapie erfolgte in einer serie , bei 24 patientinnen noch als biaxiale telekobaltpendelung , bei den restlichen 274 patientinnen mittels opponierender 15 - mev photonenstehfelder in 1 , 82 , 0 gy einzeldosis bis zu einer gesamtdosis von 5054 gy an der beckenwand . 
bei 58 patientinnen wurde zustzlich die scheidenabschlussnarbe mit high - dose - rate - ( hdr - ) afterloading in zwei bis vier fraktionen mit einer einzeldosis von 5 gy bezogen auf 0 , 5 cm gewebetiefe bestrahlt . 
eine signifikante abhngigkeit der berlebenswahrscheinlichkeit vom alter der patientinnen konnte nicht nachgewiesen werden ( p = 0 , 13 ) ; allerdings war die prognose fr die > 65 - jhrigen patientinnen mit 45% deutlich schlechter als fr jngere frauen . 
schlecht differenzierte und undifferenzierte karzinome hatten zwar mit einer 5 - jahres - berlebensrate von 69 , 4% gegenber 80% fr mig und gut differenzierte karzinome eine ungnstigere prognose , der unterschied war mit p = 0 , 074 aber nur als trend zu werten . interessant ist der einfluss der radikalitt der operation in den frhen tumorstadien : fr die 130 patientinnen im stadium pt1 , die nach wertheim radikal und mit einer lymphonodektomie operiert und nachbestrahlt waren , ergab sich eine 5 - jahres - berlebensrate von 75% gegenber 79% fr die 39 patientinnen , die nur hysterektomiert und nachbestrahlt waren ( in diesen fllen war das karzinom meist ein zufallsbefund )  . obwohl in den universittskliniken mehr lymphknoten entfernt wurden als in den zuweisenden kreiskrankenhusern , waren die 5 - jahre - berlebensraten nach kaplan - meier mit 66% bzw . 
in der cox - regression unter einschluss des lymphknotenstatus als kovariate ergab sich fr die patientinnen , die an kreiskrankenhusern operiert waren , eine schlechtere 5 - jahres - berlebensrate ; dies ist jedoch mit p = 0 , 084 nur als trend zu deuten . der einfluss der tumorgre ( tabelle 2 ) war signifikant : fr die patientinnen im stadium pt2 war die 5 - jahres - berlebensrate mit 60 , 8% gegenber 75 , 8% im stadium pt1 schlechter ( p < 0 , 01 )  . deutlich ungnstig wirkte sich der lymphknotenbefall auf die prognose aus : verschlechterte sich die prognose bei strahlenther onkol 2005 no . 
 radikaloperation mit lymphonodektomie n ( ) t - kategorie patienten5 - jahres berleben ( % ) zahl ( n ) n ( + ) patienten5 - jahresberleben zahl ( n ) pt1a pt1b pt2a pt2b pt1 pt2 grading g1 / g2 g3 / g4 8 87 , 5 75 , 1 70 , 7 64 , 9 76 , 2 68 , 2 84 , 0 79 , 6 2 9 62 , 8 44 , 4 40 , 4 65 , 8 41 , 4 64 , 8 39 , 9 nodal negativen patientinnen vom stadium pt1b mit 75% zum stadium pt2b mit 65% nur um 10% 5 - jahres - berleben , betrug die differenz bei nodal positiven patientinnen mit 63% bei pt1b versus 40% im stadium pt2b fast 25% ! analyse des lymphknotenstatus aufgrund der bedeutung als prognoseparameter wurde der lymphknotenstatus differenzierter betrachtet . 
weitgehend ohne bedeutung fr die lymphknotenmetastasierung war der differenzierungsgrad : bei g1 / g2 - tumoren waren 31% , bei g2 / g3 - tumoren 33 , 6% der lymphknoten befallen . 
auch ein doppelseitiger lymphknotenbefall verschlechterte das 5 - jahres - ergebnis von 45% im vergleich zum einseitigen befund mit 60% berleben . fr die nodal negativen patientinnen hatte der differenzierungsgrad keinen einfluss auf die prognose ; dagegen war ein groer unterschied im berleben fr die n + g1 / g2 - karzinome mit 65% gegenber 40% fr n + g3 / g4 - tumoren festzustellen ( tabelle 2 )  . 
 rezidivanalyse ein zusammenhang zwischen hmangiosis und lymphknotenbefall war ebenfalls zu sehen : bei den prparaten mit einer hmangiosis wiesen 29 / 68 ( 45% ) lymphknotenmetaim beobachtungszeitraum wurde bei 75 patientinnen ( 25% ) ein rezidiv nach einem mindestens 6 - monatigen tumorfreien intervall festgestellt , wobei das auftreten des rezidivs strahlenther onkol 2005 no . 
5 - year survival according to lymphangiosis and hemangiosis . patientenzahl ( n ) 5 - jahres berlebensrate lymphgefeinbrche nachgewiesen nicht nachgewiesen hmangiosis nachgewiesen nicht nachgewiesen 40 244 65 219 63 , 8 69 , 6 55 , 4 72 , 7 0 , 38 < 0 , 01 unabhngig vom erkrankungsalter war . 
bei 68 patientinnen konnte der zeitraum zwischen primrerkrankung und rezidiventstehung genau eruiert werden : bei einem durchschnittlichen zeitintervall von 26 monaten ( 7170 monate ) wurde bei 45 / 68 patientinnen ( 66% ) das tumorrezidiv innerhalb der ersten 2 jahre nach erkrankungsbeginn festgestellt . 
mit dem nachweis von lymphknotenmetastasen erhhte sich die rezidivquote ebenfalls dramatisch : im stadium pt1n0 betrug sie 15 , 6% , bei pt1n + 35 , 3% und im stadium pt2n0 26% gegenber 50% bei pt2n + ( tabelle 5 )  . 
bei 50 gy gesamtdosis traten in 12% ( 24 / 196 patientinnen ) lokalrezidive und bei 54 gy gesamtdosis in 13% ( 13 / 102 patientinnen ) lokalrezidive auf . die durchschnittliche berlebenszeit zwischen rezidivdiagnose und tod konnte bei 56 verstorbenen ermittelt werden und betrug im durchschnitt 12 , 7 monate ( 273 monate ) ; die meisten patientinnen ( n = 34 ) starben innerhalb des 1 . 
jahres. eine analyse der todesursachen zeigte , dass nach 5 jahren von den 79 nodal positiven patientinnen 34 ( 43% ) am tumor verstorben waren , von den 162 nodal negativen dagegen nur 35 ( 21% )  . 
 kategorie gesamtpatientenzahl ( n ) rezidivrate patientenzahl ( n ) pt1n0m0 pt1n1m0 keine angaben pt2n0m0 pt2n1m0 keine angaben 5 4 15 , 6 35 , 3 26 , 2 50 , 0 25 , 0 0 1 als sptkomplikationen fanden sich bei 9% der patientinnen unterhautfibrosen , bei elf patientinnen ( 3 , 7% ) ein sekundres lymphdeeine chronische blasenund darmirritation grad 3 wurde nur bei vier patientinnen dokumentiert . diskussion die radikale hysterektomie mit lymphonodektomie ist beim invasiven zervixkarzinom in den stadien ia bis iia , in gnstigen fllen in deutschland auch bis iib nach figo die bliche therapie , wenn keine grnde gegen ein operatives vorgehen sprechen [ 23 ]  . 
die vorliegende retrospektive analyse sollte nicht die indikation zur postoperativen bestrahlung bei operierten zervixkarzinomen berprfen , sondern die patientinnen herausfiltern , bei denen die erkrankung trotz operation und strahlentherapie einen fatalen verlauf nahm , um damit eine begrndung fr den einsatz einer kombinierten radiochemotherapie [ 31 ] zu haben . 
 [ 13 ] verbessert eine platinhaltige chemotherapie sowohl das ereignisfreie als auch das gesamtberleben hochsignifikant , der preis fr das bessere ergebnis besteht aber in einer bis zu achtfach erhhten akuten gastroenterologischen und hmatologischen toxizitt . 
es muss die risikogruppe definiert werden . das zervixkarzinom ist das einzige karzinom , bei dem die stadieneinteilung bis jetzt noch entsprechend der figo klinisch - diagnostisch erfolgt , ohne dass computertomographie , magnetresonanztomographie und operatives staging fr die stadieneinteilung zugelassen sind . 
aus diesem grund ist es schwierig , die ergebnisse der vorliegenden untersuchung mit den literaturdaten [ 10 , 21 , 26 , 30 ] zu vergleichen , zumal es sich nicht um das krankengut einer frauenklinik handelt , sondern um patientinnen , die aus den verschiedensten krankenhusern zur nachbestrahlung berwiesen worden waren . 
 die absiedlung von metastasen in die lokoregionren lymphknoten ist der wichtigste prognosefaktor [ 2 , 5 , 11 , 17 , 27 , 30 , 32 , 36 ]  . 
die tumorgre , reprsentiert durch die pt - klassifikation , ging dagegen in die cox - regression nur mit dem faktor 1 , 3 ein ein hinweis darauf , dass die lymphknotenmetastasierung wichtiger ist als die lokale grenausdehnung . 
diese resultate stehen in einklang mit einer reihe entsprechender untersuchungen [ 6 , 7 , 10 , 18 , 21 , 26 , 27 , 29 ]  . bei unseren patientinnen hatte eine lymphangiosis keinen einfluss als prognoseparameter , wohl aber der nachweis einer hmangiosis . 
wir konnten keinen signifikanten unterschied in der prognose zwischen adenound plattenepithelkarzinomen beobachten und stehen damit im gegensatz zu anderen autoren [ 9 , 11 , 22 ]  . die feststellung , dass im stadium pt1 die patientinnen , die nur hysterektomiert und nachbestrahlt worden waren , eine geringgradig bessere prognose im vergleich zu den lymphonodektomierten und bestrahlten patientinnen hatten , sollte zumindest die schlussfolgerung zulassen , dass bei zufallsbefunden keine aufwendigen zweitoperationen erforderlich sind , sondern eine nachbestrahlung angezeigt ist . bei unseren patientinnen konnte kein unterschied im berleben in abhngigkeit von der anzahl der entfernten lymphknoten festgestellt werden . 
diese aussage weist auf eine andere frage hin : hat die lymphknotenentfernung einen therapeutischen oder nicht eher einen diagnostischen wert ? sicher ist die wahrscheinlichkeit des nachweises von metastasen grer , je mehr lymphknoten entfernt werden ; fr die prognose ist aber allein die tatsache der lymphknotenmetastasierung entscheidend . 
damit stellt sich konsequenterweise die forderung nach der zulassung bildgebender verfahren und eines operativen stagings mit einer definierten mindestanzahl von entfernten lymphknoten zur stadieneinteilung als basis fr eine individuelle , befundadaptierte multimodale therapie . 
 gesichert erscheint fr die adjuvante behandlung , wenn auch nur in einer studie , der vorteil durch eine simultane platinhaltige radiochemotherapie in der hochrisikosituation im vergleich zu einer alleinigen radiotherapie . 
 [ 25 ] mit einer 4 - jahres - berlebensrate von 80% bei radiochemotherapierten patientinnen gegenber 63% bei allein nachbestrahlten patientinnen weisen auf den therapeutischen gewinn durch eine platinhaltige postoperative radiochemotherapie h in einer eigenen retrospektiven analyse von 34 operierten patientinnen in der hochrisikosituation , die adjuvant eine simultane radiochemotherapie mit cisplatin / 5 - fluorouracil erhalten hatten , verstarben nur vier patientinnen innerhalb der ersten 6 monate am tumor , unabhngig von der anzahl der entfernten lymphknoten . 
keiner weiteren nachbehandlung bedrfen patientinnen mit einem kleinen , adquat operierten zervixkarzinom ohne risikofaktoren ( bis pt1b1n0 ) , durch eine postoperative strahlentherapie kann die rate an lokalrezidiven sehr wohl gesenkt werden [ 4 , 20 , 28 , 35 ]  . 
aus unserer sicht ist deshalb die nachbestrahlung bei inadquater lymphonodektomie ( < 15 entfernte lymphknoten ) und einem groen tumor mit tiefer stromainvasion im zervixbereich ( stadium pt1b2n0 ) immer noch indiziert . 
beim vorliegen folgender risikofaktoren besteht eine hochrisikosituation , die eine kombinierte radiochemotherapie begrndet : histologisch verifizierte lymphknotenmetastasen , r1und r2 - resezierte karzinome und eine nachgewiesene hman giosis , wobei jeder dieser faktoren eine kombinierte nachbehandlung rechtfertigt . 
ob auch eine lymphangiosis an sich als risikofaktor zu werten ist , lsst sich von uns nicht beweisen und ist auch in der literatur nicht gesichert [ 25 , 27 ]  . 
preoperative prognostic variables and the impact of postoperative adjuvant therapy on the outcomes of stage ib or ii cervical carcinoma patients with or without pelvic lymph node metastases : an analysis of 891 cases . 
a randomized trial of pelvic radiation therapy versus no further therapy in selected patients with stage ib carcinoma of the cervix after radical hysterectomy and pelvic lymphadenectomy : a gynecologic oncology group study . 
5 urban & vogel strahlentherapie und onkologie original article does the imaging method have an influence on the measured tumor height in ruthenium plaque therapy of uveal melanoma ? patrick schueller1 , adnan dogan1 , joan e . 
the purpose of this analysis is to examine systematic differences between ultrasound ( us ) , computed tomography ( ct ) , and magnetic resonance imaging ( mri ) measurements of tumor height in uveal melanoma . 
separate comparisons were carried out for tumor size and localization and between two - dimensional ( 2 - d ) and three - dimensional ( 3 - d ) measurements in reconstructed planes . 
 conclusion : differences between the measurements from all three modalities were generally acceptable , except for small tumors ( 4 mm ; limited spatial resolution of ct / mri ) and temporal or peripheral lesions ( angular distortion in us )  . 
ziel dieser arbeit ist deshalb die untersuchung systematischer unterschiede zwischen den messungen der tumorprominenz mittels ultraschall ( us ) , computertomographie ( ct ) und magnetresonanztomographie ( mrt )  . material und methodik : von 1993 bis 2000 wurden 208 patienten mit aderhautmelanomen mit rutheniumplaques behandelt . 
des weiteren wurde nach tumorgre und - lage differenziert , und zweidimensionale ( 2 - d ) messungen wurden mit dreidimensionalen ( 3 - d ) in rekonstruierten ebenen korreliert . ergebnisse : im direkten vergleich waren die im ct gemessenen werte ( median : 4 , 5 mm ; bereich : 1 , 610 , 5 mm ) nahezu identisch mit den mrt - messungen ( median : 4 , 5 mm ; bereich : 2 , 011 , 4 mm ) , whrend der us die hchsten werte lieferte ( median : 5 , 2 mm ; bereich : 2 , 513 , 4 mm )  . 
die lineare regression ergab folgende werte : ct versus us ( r2 = 0 , 88 , korrelationskoeffizient = 1 , 04 ) , mrt versus us ( r2 = 0 , 79 , korrelationskoeffizient = 0 , 92 ) , mrt versus ct ( r2 = 0 , 84 , korrelationskoeffizient = 0 , 90 ) und 2 - dversus rekonstruierte 3 - d - messungen ( r2 = 0 , 93 , korrelationskoeffizient = 0 , 98 )  . schlussfolgerung : die abweichungen zwischen den messungen aller drei verfahren waren insgesamt akzeptabel , auer bei kleinen tumoren ( 4 mm ; begrenzte auflsung von ct / mrt ) und temporalen oder peripheren lsionen ( winkelverzerrung im us )  . 
other eye - conserving radiotherapy techniques , like stereotactic irradiation [ 12 ] , proton [ 5 ] and heavy - particle irradiation , have been developed and successfully applied in the clinical setting . 
the accuracy of measurements of tumor size is as important for ruthenium plaque therapy as an exact patient positioning is for external - beam therapy [ 3 , 18 ] and stereotactic irradiation [ 12 ]  . 
the standard imaging method for measuring tumor height and diameter in uveal melanoma is ultrasound ( us ) , which is routinely used in the initial diagnostic work - up [ 4 ]  . 
a further alternative for patients with contraindications against mri ( heart pacemakers , metal implants , etc . ) is computed tomography ( ct )  . in our institution , us , mri and ct scans are routinely performed for all patients receiving ocular brachytherapy . 
assuming a mathematically exact cone shape , the maximum error resulting from measurement in one plane can be as high as cos 45 , which amounts to about 1.41 times the true size . 
these were performed by reconstructing a virtual ct or mri plane from the dataset perpendicular to the eye bulb ct / mri slice measured height ( h ) true height ( h ) figure 1 . 
das problem : die gemessene prominenz h kann bis zu 1 , 41 - mal so gro wie die tatschliche hhe h se material and methods from 1993 to 2000 , a total of 208 patients with uveal melanoma were treated with ruthenium plaque brachytherapy at our institution . 
the solution : the true height h can be determined by reconstructing a slice orthogonal to the sclera and using this reconstruction for measurement ( 3 - d measurement )  . 
die lsung : die wahre prominenz h kann bestimmt werden , indem eine orthogonal zur sklera verlaufende schicht rekonstruiert und in dieser schicht gemessen wird ( 3 - d messung )  . 
the tumor height was then measured in the resulting reconstructed image ( figures 3a and 3b )  . measurements were compared by computing the median absolute differences and by linear regression . 
 the median absolute differences between the measurements amounted to 0.6 mm ( ct / us ) , 0.9 mm ( us / mri ) , and 0.6 mm ( ct / mri )  . 
the median relative differences between the measurements amounted to 13.8% ( ct / us ) , 13.8% ( us / mri ) , and 9.5% ( ct / mri )  . 
linear regression between ct and us data yielded a good correlation with an r2 of 0.88 , a constant of 0.57 ( us values tending to be higher ) , and a correlation coefficient of 1.04. 
linear regression between mri and ct yielded an r2 of 0.84 , a constant of 0.59 ( ct values tending to be higher ) and a correlation coefficient of 0.90 ( figure 5c )  . 
two values exceeded the 95% ci . further comparisons between subgroups were performed using the ct and us measurements because the intersection between ct and us patients yielded the largest data pool ( n = 138 )  . 
tumor localizations were compared in us and ct measurements , the theory being that temporal and peripheral tumors should be more difficult to measure with us than nasal and central tumors . 
 ( four values outside 95% ci ) , for nasal / central tumors , to 0.82 ( five values outside 95% ci ) , meaning a slightly better fit for nasal / central lesions . 
for central tumors , r2 amounted to 0.86 ( two values outside 95% ci ) , and for peripheral tumors , to 0.77 ( seven values outside 95% ci )  . 
when we compared small tumors ( 4 mm ) with large tumors ( > 4 mm ) , we encountered large differences between ct and us measurements for small tumors , resulting in an r2 of only 0.08 ( three values outside 95% ci )  . 
 discussion in general , the differences between the tumor size measurements from all three modalities were moderate ( median : 0.60.9 mm or < 15% ) with us values tending to be a little larger than those by ct or mri . 
the interobserver variability of us has been described as 0.6 mm ( 2 sd [ standard deviations ] ) [ 4 ]  . the maximum possible dose - rate error resulting from the differences mentioned above can be calculated from the depth - dose curves and amounts to 19% ( steep portion of curve for ccb plaque , bebig , berlin , germany )  . 
this seems tolerable considering the fact that the dose rate of the currently used ruthenium applicators can only be measured to an accuracy of 25% ( 95% ci ) [ 6 ]  . in special anatomic situations we observed larger differences . 
this can be explained by an angular distortion of the us measurements when scanning cannot be done orthogonally to the sclera , which is not discussed by haritoglou et al . 
 when the tumor is located at the upper or lower edge of the eye bulb , axial 2 - d measurements ( ct , mri ) can theoretically result in distortions up to 1.41 times the original tumor height . 
when the tumor is located at the upper or lower edge of the eye bulb , 3 - d measurements can yield more precise values . strahlentherapie und onkologie current discussion hypoxic versus normoxic external - beam irradiation of cervical carcinoma combined with californium - 252 neutron brachytherapy comparative treatment results of a 5 - year randomized study taco tacev1 , antonn vacek2 , blanka ptckov1 , vratislav strnad3 purpose : the article focuses on the treatment and protective effects of hypoxyradiotherapy during external - beam irradiation of cervical carcinoma , including paraaortic lymph nodes , combining radiotherapy with californium - 252 ( 252cf ) neutron brachytherapy . 
an analysis of treatment results , early and late side effects and complications is presented . patients and methods : from january 1989 to may 1997 , 307 women with stage iib and iiib cervical carcinoma , treated with 252cf neutron brachytherapy , were randomly divided into two groups and treated with external - beam irradiation to the paraaortic lymph nodes as follows : 155 patients ( 59 with stage iib , 96 with stage iiib ) were treated by external - beam irradiation administered as a 60 - gy dose applied under conditions of acute hypoxia ; 77 patients ( 30 with stage iib and 47 with stage iiib ) received extended - field irradiation up to l4 and 78 patients ( 29 with stage iib and 49 with stage iiib ) up to t12 . 152 patients ( 58 with stage iib , 94 with stage iiib ) were treated by external - beam irradiation administered as a 40 - gy dose applied under normal oxygenation conditions . 
73 patients ( 29 with stage iib and 44 with stage iiib ) received extended - field irradiaton up to l4 and 79 patients ( 29 with stage iib and 50 with stage iiib ) up to t12 . the same 56 gy - equivalent ( eq ) doses at point a and 19 gy - eq doses at point b were applied intracavitarily in both groups . 
the total radiation doses at points a and b were 99 and 79 gy - eq , respectively , for patients treated with external - beam irradiation to 60 gy under conditions of acute hypoxia . 
during the period of 612 years after treatment there were no changes in the frequencies of occurrences of late effects and complications . conclusion : the importance of the protective effects of hypoxyradiotherapy for dose escalation in external - beam irradiation of cervical carcinoma , including paraaortic lymph nodes , with regard to an improvement of the cure rates of metastases in paraaortic lymph nodes has been confirmed . key words : cervical carcinoma hypoxyradiotherapy californium - 252 treatment results side effects and complications strahlenther onkol 2005 ; 181 : 27384 doi 10.1007 / s00066 - 005 - 1303 - 0 perkutane hypoxieversus normoxieradiotherapie des zervixkarzinoms kombiniert mit californium - 252 - neutronenbrachytherapie . 
vergleich der behandlungsergebnisse einer randomisierten studie ber fnf jahre ziel : untersuchung der protektiven wirkung der hypoxieradiotherapie im rahmen der perkutanen bestrahlung des zervixkarzinoms einschlielich der paraaortalen lymphknoten , wobei die perkutane strahlentherapie mit californium - 252 - ( 252 - cf - ) neutro1 masaryk memorial cancer institute , brno , czech republic , 2 institute of biophysics , academy of sciences of the czech republic , brno , czech republic , 3 department of radiation oncology , friedrich alexander university erlangen - nuremberg , erlangen , germany . received : march 24 , 2004 ; accepted : february 17 , 2005 strahlenther onkol 2005 no . 
 patienten und methodik : zwischen januar 1985 und mai 1997 wurden insgesamt 307 patientinnen mit zervixkarzinom stadium iib und iiib , die sich einer 252cf - neutronenbrachytherapie unterzogen , wie folgt randomisiert und behandelt : 155 patientinnen ( 59 im stadium iib , 96 stadium iii ) erhielten eine perkutane bestrahlung bis 60 gy unter bedingungen der akuten hypoxie . 
bei 77 patientinnen ( 30 im stadium ii und 47 im stadium iiib ) wurden die paraaortalen lymphknoten bis auf hhe l4 bestrahlt , bei 78 patientinnen ( 29 im stadium iib und 49 im stadium iiib ) bis auf hhe th12 . 152 patientinnen ( 58 im stadium iib und 94 in stadium iiib ) erhielten eine perkutane bestrahlung bis zu einer gesamtreferenzdosis von 40 gy unter normoxischen bedingungen . 
bei 73 patientinnen ( 29 im stadium iib und 44 im stadium iiib ) wurden die paraaortalen lymphknoten bis auf hhe l4 bestrahlt , bei 79 patientinnen ( 29 im stadium iib und 50 im stadium iiib ) bis auf hhe th12 . in beiden gruppen wurden die gleichen 56 gy - quivalent - ( q ) - dosen in punkt a und 19 gy - q in punkt b intrakavitr verabreicht . 
jahr nach behandlung ergaben sich keine unterschiede zwischen den beiden gruppen bezglich der inzidenz von spten nebenwirkungen und komplikationen . schussfolgerung : die bedeutung der protektiven wirkung einer hypoxieradiotherapie fr die verbesserung der heilungsraten bei zervixkarzinom im rahmen der dosiseskalation wurde besttigt . schlsselwrter : zervixkarzinom hypoxieradiotherapie californium - 252 therapieergebnisse nebenwirkungen introduction the therapeutic results of conventional photon radiotherapy of tumors , including cervical carcinoma , have not improved as expected , despite great progress in the technical process of irradiation . 
photon irradiation does not induce the changes needed for a decrease of influences by the factors produced by a zonal heterogeneity of microarrangement , as hypoxia and intrinsic genetic heterogeneity in the tumor stem cell population influence the repair of posttreatment changes following exposure to ionizing radiation [ 50 ]  . 
it seems clear that inactivation of the tumor cells resistant to photon therapy requires a new approach in the radiotherapy of malignant tumors . there are prospects to overcome the stagnation of conventional radiation treatment results by the use of unconventional sources of radiation , neutrons , and to modify the radiation effects of photon therapy . using unconventional radiation sources in medical practice is not easy . 
the discovery of the californium - 252 nuclide ( 252cf ) , a source of gamma / neutron radiation , established good conditions for using neutrons in tumor brachytherapy [ 4 , 44 ]  . 
in addition to the use of radiation with a high linear energy transfer ( let ) , i.e. , neutrons , an alternative method of increasing the biological effect of external photon radiotherapy with application of grays discovery of the radiosensitizing effect of oxygen may also be beneficial in a clinical setting [ 6 ]  . previous experimental efforts utilizing this effect were devoted to reoxygenation of tumor tissue by different fractionation schemes of radiotherapy [ 12 , 48 ] , irradiation under hyperbaric conditions [ 10 ] , and the use of radiosensitizing agents [ 2 , 22 ]  . 
currently , more attention is being focused on the reduction of radiosensitivity of normal tissues in order to extend the therapeutic range for higher doses of radiation . the results of studies in radiotherapy of tumors indicate that , independent of chemotherapeutic treatment [ 20 , 24 ] , there is strong radiobiological evidence that the duration of radioprotection in normal tissue during respiratory hypoxia strahlenther onkol 2005 no . 
 since tumor tissue is usually chronically hypoxic , the induction of acute hypoxia during radiotherapy causes a selective radioprotective effect only in noncancerous , normoxic tissues , especially in hemopoietic and intestinal tissues [ 46 ]  . 
 theoretical assumptions of differential radioprotection by acute hypoxia to tumor and normal tissues have been verified experimentally [ 21 , 29 , 45 , 52 ] , as well as clinically [ 1 , 28 , 30 , 37 , 40 , 42 , 43 ]  . 
one objective was a clinical experimental study aimed at the improvement of treatment procedure by determining optimum levels of the neutron component [ 32 , 36 , 39 , 41 ] and optimum o2 percentages in the hypoxic gas mixture ( hgm ) inhaled during irradiation [ 49 ]  . 
our second objective consisted of two randomized clinical studies as follows : ( cid : 127 ) comparison of the curative effects of 252cf intracavitary therapy versus gamma - only radiation intracavitary therapy of cervical carcinoma ; ( cid : 127 ) comparison of the treatment results of hypoxic versus normoxic external irradiation combined with 252cf neutron brachytherapy of cervical carcinoma . the treatment results were examined by comparing the 5 - year survival rates of patients with cervical carcinoma treated intracavitarily by 252cf plus gamma radiation versus gamma - only radiation . 
this comparison strongly supported the role of neutron irradiation for significant improvement in the results of treatment [ 34 ]  . the subject of the presented paper is the comparison of the treatment results , using 5 - year survival rates , of patients with cervical carcinoma treated intracavitarily by 252cf plus external - beam irradiation under hypoxic conditions , versus external - beam irradiation under normoxic conditions . patients and methods in a randomized study between january 1989 and may 1997 , 307 women with advanced cervical carcinoma , treated with 252cf neutron brachytherapy , were divided into two groups based on the method of external - beam irradiation : ( cid : 127 ) 155 patients ( 59 with stage iib , 96 with stage iiib ) were treated by external irradiation administered as a 60 - gy dose applied under conditions of acute hypoxia ; ( cid : 127 ) 152 patients ( 58 with stage iib , 94 with stage iiib ) were treated by external - beam irradiation administered as a 40 - gy dose applied under normal oxygenation conditions . the stage of disease was determined according to the figo classification on the basis of the following examinations : inspection , palpation , biopsy , cystoscopy , intravenous pyelography ( ivp ) , renography , bone scintigraphy , liver sonography , chest x - ray , and hematologic / biochemical examination of blood . 
all patients had normal cardiac and respiratory function , and were free of any disease representing a contraindication to acute hypoxic condition ( chronic bronchitis , bronchial asthma , ischemic heart disease and others )  . 
 external - beam irradiation for both groups , the external - beam radiation was produced by standard x - ray beams from a mevatron linear accelerator with an energy level of 20 mev . 
the field in the small pelvis was 18 cm wide with its upper edge at the level of the l4l5 or t12l1 boundaries in accordance with the metastatic involvement of the lymph nodes . 
the width of the central shield of the split field was 4 cm and consequently , the dose at point a of the split field was 50% lower than that applied at point b . 
hypoxyradiotherapy in cervical carcinoma was extended to the paraaortic nodes using an asymmetric y2 jaw ; the width of the extended field was 9 c for both groups the extent of metastatic disease in lymph nodes was assessed by a lymphogram together with a retroperitoneal and pelvic ct scan , notwithstanding our awareness that interpretation of lymphatic observations is problematic . 
 the extent of external irradiation fields for patients in both groups was determined using the following criteria : ( cid : 127 ) in patients without metastases of the lymph nodes , and in patients with positive lymphography of the regional lymph table 1 . 
verteilung der patienten nach gre des bestrahlungsfelds . lower margin l - 4 vertebra external beam irradiation in normooxic condition lower margin th - 12 vertebra stage iib stage iiib stage iib stage iiib external beam irradiation in hypoxic condition nodes in the small pelvis , the field was extended to the level of the l4l5 boundary ; ( cid : 127 ) in patients with positive lymphography of the common iliac and paraaortic lymph nodes , the field was extended to the level of the t12l1 boundary . 
the applied dose of 40 gy , f - 2 gy / day , was administered with two opposite fields as divided doses of 20 gy in full and split fields to the small pelvis . 
the applied dose of 60 gy , f - 2 gy / day , was administered with two opposite fields as divided doses of 26 gy in full field and 34 gy in split field to the small pelvis . 
 the rbe of the 252cf neutron component had a value of 6 [ 3 , 15 ]  . the dose at point a ( 56 gy - eq ) for all patients was divided into two parts . 
the intracavitary 252cf neutron component was applied to each patient in one uterovaginal application , using six tubes of 2.8 108 bq ( 10 g ) per tube , per patient . 
the supplementary intracavitary gamma radiation was delivered to each patient by means of conventional brachytherapy in one uterovaginal application , using radium - 226 ( 226ra ) or cesium - 137 ( 137cs ) as the radiation source . 
252cf and 226ra were applied using a manual afterloading system ; 137cs was applied using the selectron ldr / mdr afterloading systethe dose distribution for all sources was determined individually by means of a planning syste the overall dose applied to patients treated with neutron brachytherapy plus external - beam irradiation under hypoxic conditions was 99 gy - eq at point a and 79 gy - eq at point b . the overall dose applied to patients treated with neutron brachytherapy plus external - beam radiation under normal oxygenation conditions was 85 gy - eq at point a and 59 gy - eq at point b . there was no change of therapy for any patient due to intolerance of treatment or any other reason during the course of treatment . follow - up after completion of treatment , patients in both groups received long - term follow - up monitoring according to the following scheme : once per month follow - up was done in the first 6 months following treatment ; once per 3 months follow - up was done for the time period of 7 months following treatment to the end of the 3rd year ; and once per 6 months from the end of the 3rd year on . 
the patients who died for reasons other than cervical carcinoma had no evidence of disease at the last checkup and have been included in the overall survival rates . statistics a statistical comparison of the treatment results of the procedures was calculated according to log - rank test and kaplanmeier analysis for comparison of survival rates . 
early reactions after irradiation were evaluated according to the ctc - nci ( 1988 ) , as modified by the european organisation for research and treatment of cancer ( eortc , 1992 )  . results overall survival rate the comparison of overall survival rates for all patients ( stages iib and iiib ) is shown in figure 2 . 
hypoxyradiotherapy in cervical carcinoma cervical carcinoma stage iiib cervical carcinoma stages iib hypoxia normoxia p < 0.10 normoxia hypoxia p < 0 , 50 time ( months ) figure 3 . 
hypoxyradiotherapy in cervical carcinoma cervical carcinoma stages iib + iiib cervical carcinoma stages iib + iiib normoxia hypoxia p < 0.50 hypoxia normoxia p < 0.11 time ( months ) figure 5 . 
the 5 - year metastases - free survival rate for patients in normoxic condition was 85.40% for patients with the field extending to t12l1 , and 77.3% for patients whose field extended to l4l5 . 
comparison of metastases - free survival for stage iiib patients in hypoxic condition according to the extent of external irradiation field : periaortic region up to t12 versus pelvic field alone ( including l4 )  . 
it appears that within 612 years after the end of treatment there were no significant changes in the occurrence of late reactions and complications of treatment even when the applied radiation dose in patients treated under hypoxic conditions was significantly higher than the radiation tolerance of healthy tissues . 
 discussion the radiotherapy of cervical carcinoma in our study is a standard combined procedure of two distinct irradiation processes : prolonged intracavitary irradiation and external - beam fractionated irradiation with the use of two qualitatively new treatment modalities . 
with the use of 252cf for intracavitary therapy , this combined procedure is influenced by the qualitatively different natures and effects of these two radiation types high let ( intracavitary 252cf radiation ) and low let ( gamma radiation , both external - beam and brachytherapy ) and is further influenced , during external - beam irradiation , by hypoxic conditions . 
the complexity of this new combined procedure was demonstrated for the first time in a clinical setting by maruyama [ 1618 ] and our clinical - experimental trial [ 32 , 33 , 36 , 40 , 41 ]  . our choice of intracavitary 252cf therapy as the procedure to be used in this study was based on maruyamas empirical finding that improvement of curative results was produced only by early application of the neutron source of radiation during therapy , in combination with external gamma radiation applied subsequently [ 15 ]  . in our clinical - experimental trial , we monitored and analyzed the relationship between the processes of reoxygenation and tumor regression after irradiation of tumors with various doses of neutrons . 
spte nebenwirkungen in bezug zur behandlungsmethode . grade iii grade ii grade i external irradiation in normoxic condition gastrointestinal chronic rectal proctitis ulcer rectovaginal smal bowel fistula toxicity 20 , 4% 31 / 152 11 , 2% 17 / 152 35 , 5% 54 / 152 gastrointestinal nausea vomiting diarrhea urologic hemorrhage and hemorrhagic cystitis 15 / 152 25 , 6% dysuria 39 / 152 9 , 8% 18 , 1% 28 / 155 7 , 1% 11 / 155 30 , 3% 47 / 155 gastrointestinal nausea vomiting diarrhea urologic hemorrhage and 5 , 1% hemorrhagic cystitis 3 / 155 21 , 3% dysuria 33 / 155 4 , 0% 6 / 152 6 , 6% 10 / 152 11 , 8% 18 / 152 3 , 3% 5 / 152 1 , 9% 3 / 155 5 , 1% 8 / 155 3 , 9% 6 / 155 gastrointestinal external irradiation in hypoxic condition became the basis of our procedure in treating cervical carcinoma with brachytherapy using a combination of 252cf radiation with gamma radiation [ 32 , 35 , 36 , 41 ]  . comparative treatment results of our 5 - year , randomized study show that the application of 252cf neutron radiation , with gamma radiation , in uterovaginal intracavitary therapy creates promising prospects for improvement in the cure rates of cervical carcinoma as a consequence of eradication of the part of the tumor cell population that is resistant to conventional photon radiation . 
this is supported by the observed result that one of the improved aspects of therapy outcomes was the significant decrease of local tumor recurrences in the small pelvis , in the near locality where 252cf neutrons interact with the primary tumor cells [ 34 ]  . 
 our treatment data supports the hypothesis that significant improvement of the results after treatment of cervical carcinoma , evidenced by the decrease of local recurrences in the small pelvis after brachytherapy by 252cf neutrons , is evoked by the role of irradiation of paraaortic lymph nodes [ 32 ]  . 
on the other hand , irradiation of juxtaregional lymph nodes may have a curative result only under conditions in which the tumor process in the small pelvis can be treated successfully [ 26 ]  . 
 0 , 6% ( 1 ) 1 , 3% ( 2 ) 0 , 6% 2 , 6% external irradiation in normoxic condition ( n = 152 ) external irradiation in hypoxic condition ( n = 155 ) 2 , 6% ( 4 ) 5 , 8% ( 9 ) external irradiation in normoxic condition ( n = 152 ) external irradiation in hypoxic condition ( n = 155 ) 8 , 5% ( 13 ) 7 , 1% ( 11 ) 0 , 6% ( 1 ) 2 , 0% 1 , 9% ( 3 ) 2 , 6% urologic chronic urocystic cystovaginal cystitis ulcer fistula this treatment modality was considered in the 1970s , but the application of a therapeutic dose of 60 gy to the sensitive tissues of the abdomen resulted in a high number of early and late side effects and treatment complications [ 47 ]  . the value of paraaortic prophylactic irradiation with 45 gy was studied in two large randomized trials : the rtog 79 - 20 trial [ 25 ] , and the eortc trial [ 7 ]  . 
 in the eortc trial , patients with cervical carcinoma ( stages iiiib without clinically or surgically involved paraaortic nodes ) were randomized to pelvic irradiation or pelvic plus paraaortic prophylactic irradiation . 
 the statistically significant improvement of metastasesfree survival in stage iiib after irradiation of paraaortic nodes with a dose of 60 gy in acute hypoxia is a genuine manifestation of the increased effect of the tumor photon irradiation . 
 the presented results confirm our hypothesis that the treatment effect after external - beam irradiation with a dose of 60 gy in acute hypoxia , combined with 252cf neutron brachystrahlenther onkol 2005 no . 
hypoxyradiotherapy in cervical carcinoma therapy , is only significant in the extended part of the irradiation field , namely in the form of improved cure rates of metastases in paraaortic lymph nodes . 
in comparison with conventional brachytherapy , neutron brachytherapy using 252cf significantly enhances radiocurability of a primary tumor in the small pelvis which is a consequence of eradication of that part of the tumor cell population resistant to conventional photon radiation [ 34 ]  . 
 the presented treatment results document that acute hypoxia , induced during external - beam irradiation by ventilation of an hgm containing 8.2% oxygen , significantly decreases the radiosensitivity of healthy tissues in the abdominal region . 
the early acute manifestation of postirradiation syndrome of the gastrointestinal tract was paradoxically less acute in patients receiving hypoxyradiotherapy , even when the applied dose was > 50% higher than that used in normoxic conditions . thus , our results , correlated with those of a study in hypoxyradiotherapy of pelvic tumors ( including cervical carcinoma ) , showed a dose modification factor ( dmf ) of 1.5 compared to conventional radiotherapy [ 30 ] and our preliminary treatment results [ 43 ]  . similarly , in our study of preoperative accelerated hypoxyradiotherapy for colorectal carcinoma , in which a dose to the pelvic area involving the primary tumor and regional lymph nodes exceeded the radiation tolerance of healthy tissues , we observed a very good tolerance by healthy tissues as a result of the hypoxia - induced radioprotection . 
the significance of hypoxyradiotherapy in decreasing the side effects and complications of irradiation is supported by the results of other investigations as well [ 13 ]  . in the past 30 years , radiotherapy of cervical carcinoma has undergone considerable technical improvement . 
the utilization of the remote afterloading system in brachytherapy of tumors with the high - dose - rate iridium - 192 ( 192ir ) nuclide solved the problem of radioprotection of medical personnel and improved the comfort of patients during treatment . 
 the results of our clinical research using 252cf in tumor brachytherapy and external - beam irradiation under hypoxic conditions show that it is a qualitatively new , highly effective method of treatment that is able to eliminate tumor cells resistant to conventional gamma radiation . the eradication of tumor cell populations in photon therapy is caused by specific interactions of photons with tumor cells , which is determined by numerous factors and phenomena . 
the most important of these are the state of oxygenation of the tumor population , cell kinetic factors , including the cells ability to repair radiation damage , and other inherent factors , resulting in differences in the radiosensitivity of distinct tumor populations during irradiation [ 27 ]  . using high - let radiation - based treatment can decrease tumor resistance to photon bombardment . 
biological effects of high - let radiation include lower oxygen enhancement rate ( oer ) [ 9 ] , suppression of the repair processes of sublethal and potentially lethal cell damages [ 8 ] , and minimal dependency of radiation sensitivity on the cell cycle [ 5 ]  . this clinical data supports the results obtained in experimental studies demonstrating the radioprotective effect of 10% respiratory hypoxia on hemopoiesis , as well as on intestinal epithelium of rats ( v18 ) and intestinal crypt stem cells in hypoxic mice ( v11 , 26 ) [ 46 ]  . enhanced radioprotection on hemopoiesis was conferred by respiratory hypoxia plus administration of the immunomodulator dextran sulphate ( v22 ) , cytokine ( rmgm - csf ) [ 46 ]  . 
 the presented results of our treatment study are the first clinical findings in support of the hypothesis regarding overcoming the current stagnation in the therapy of cervical carcinoma by the use of the neutron component of 252cf in brachytherapy and hypoxyradiotherapy during external - beam irradiation . 
if neutron brachytherapy using 252cf , in comparison with conventional therapy , significantly enhances radiocurability of a primary tumor and improves medical treatment results , then the enhancement of the dose of external irradiation to the regional and juxtaregional lymph nodes further improves the medical results by decreasing the frequency of remote metastases . the desirable radiobiological , physical and clinical - experimental qualifications for the introduction of neutron brachytherapy and hypoxyradiotherapy in clinical practice have been attained [ 49 ]  . 
the main problems are the protection and safety of the technical personnel working with the neutron source of irradiation and the shortening of the time of patient irradiation . the present progress in the technology of production of the miniaturized , highly active source of the 252cf nuclide [ 14 , 23 ] as well as the progress in the design concept of the remote afterloading system applied to these sources satisfy the preconditions for introducing neutron brachytherapy in clinical practice [ 31 ]  . strahlentherapie und onkologie kommentar kommentar zum beitrag von o . 
 whrend jedoch von anderen arbeitsgruppen eine dosisabhngige , diskontinuierliche modulation der stickstoffmonoxid - ( no - ) produktion mit signifikanter inhibition durch niedrige strahlendosen ( 1 , 25 gy ) und rckkehr zu kontrollwerten oder hheren konzentrationen nach dosen 5 gy beobachtet wurde [ 2 , 3 ] , scheinen die ergebnisse der vorliegenden arbeit das gegenteil zu belegen , nmlich dass die no - freisetzung durch niedrige strahlendosen ( 2 , 0 gy ) erhht und durch hhere strahlendosen ( 3 , 54 , 0 gy ) supprimiert wird . 
 die autoren konstatieren , dass allgemein angenommen wird , je hher die strahlendosis und der effekt auf die granulozytenfunktion , umso niedriger sei die no - freisetzung , und zitieren als beleg die arbeit von de vries et al . 
 zudem darf nicht bersehen werden , dass die freisetzung toxischer sauerstoffradikale wie im bersichtsartikel von weiss [ 4 ] ausfhrlich dargelegt wird nur einer von zahlreichen mechanismen ist , die die phagozytische aktivitt neutrophiler granulozyten bestimmen . 
darber hinaus sind natrlich viele weitere mechanismen mageblich an entzndungsreaktionen beteiligt , so dass man mit schlussfolgerungen , die auf untersuchungen nur eines mglichen mechanismus basieren , sehr zurckhaltend sein sollte . 
5 urban & vogel strahlentherapie und onkologie original article irradiation causes biphasic neutrophilic granulocyte phagocytic function * oliver micke1 , alfred haidenberger2 , thomas auer2 , sabine egger2 , m . 
the current study examines the influence of low radiation doses on neutrophilic granulocyte function , which could be helpful in finding the optimal dose for either stimulation or suppression of anti - inflammatory activity . material and methods : lymphoprep density gradient - purified neutrophilic granulocytes of three voluntary , healthy donors were used for all experiments . 
 these results may provide a further explanation for the local anti - inflammatory effect of low - dose ionizing irradiation . key words : neutrophilic granulocytes phagocytic function reactive oxygen species low - dose irradiation strahlenther onkol 2005 ; 181 : 3138 doi 10.1007 / s00066 - 005 - 1346 - 2 biphasischer verlauf der phagozytischen aktivitt neutrophiler granulozyten nach bestrahlung hintergrund und ziel : der antiinflammatorische effekt niedrigdosierter strahlentherapie ist klinischerseits bereits gut beschrieben . 
ihre funktion wurde anhand der granulozytren freisetzung von reaktiven sauerstoffradikalen ( ros [ reactive oxygen species ] ) mittels luminolverstrkter chemilumineszenz nach stimulation mit phorbol - myristat - acetat ( pma ) gemessen . ergebnisse : die relativen nderungen der ros - freisetzung ( ros - freisetzung vor stimulation wurde gleich 100% gesetzt ) nach stimulation mit pma betrugen ( mittelwert standardabweichung [ sd ] ) : 0 gy : 147 , 6% 60% ; 0 , 5 gy : 153 , 6% 70% ; 1 gy : 164 , 9% 63% ; 1 , 5 gy : 177 , 8% 66% ; 2 gy : 162 , 5% 57% ; 2 , 5 gy : 156 , 2% 60% ; 3 gy : 159 , 2% 60% ; 3 , 5 gy : 126 , 9% 55% ; 4 gy : 137 , 9% 71% ; 6 gy : 148 , 3% 65% ; 12 gy : 156 , 1% 52% . 
die relative ros - freisetzung zeigte einen signifikanten an * presented in part at the rsna 2002 , 88th scientific assembly and annual meeting , december 16 , 2002 , chicago , il , usa . 
 1 department of radiotherapy , mnster university hospital , mnster , germany , 2 department of radiotherapy , innsbruck university medical hospital , innsbruck , austria , 3 department of radiotherapy , alfried krupp hospital , essen , germany , 4 department of general and transplant surgery , daniel swarovski research laboratory , innsbruck university medical hospital , innsbruck , austria . received : july 20 , 2004 ; accepted : november 29 , 2004 strahlenther onkol 2005 no . 
irradiation and granulocyte function stieg bei 1 , 5 gy ( p < 0 , 001 ) nach pma - stimulation , allerdings einen deutlich signifikanten abfall der ros - freisetzung bei 3 , 5 gy ( p < 0 , 005 ) und etwas weniger deutlich bei 4 gy ( p < 0 , 05 )  . 
6 und 12 gy zeigten wieder einen signifikanten anstieg . schlussfolgerung : diese ex - vivo - in - vitro - untersuchung an nativen humanen neutrophilen granulozyten zeigte einen anstieg der granulozytenfunktion bei 1 , 5 gy sowie einen signifikanten abfall bei 3 , 5 und 4 , 0 gy , wie er schon fr verschiedene phnomene niedrigdosierter strahlentherapie beschrieben worden ist . 
die ergebnisse knnen einen weiteren erklrungsansatz fr den lokalen entzndungshemmenden effekt niedrigdosierter strahlentherapie bieten . schlsselwrter : neutrophile granulozyten phagozytische funktion reaktive sauerstoffradikale niedrigdosierte bestrahlung introduction since the introduction of radiotherapy ( rt ) in clinical medicine in 1896 and during the first decades of the 20th century , the treatment of benign inflammatory disorders with rt was a main domain of radiotherapists [ 23 , 25 , 35 ]  . 
however , after publications on potential induction of malignancies [ 3 ] this option was discredited and consequently restricted to few indications , particularly in the anglo - american countries [ 5 , 17 ]  . 
recently , on the background of excellent anti - inflammatory and analgesic effect , in particular in benign inflammatory and painful disorders of the skeleton , the low toxicity and cost level of low - dose rt as well as the limited effectiveness of conventional treatment alternatives , rt has again become an emerging focus in clinical routine and radiobiological research on benign disorders [ 20 , 27 , 29 ]  . 
a presumed therapeutic effect of ionizing irradiation seems to be related to the local anti - inflammatory activity [ 38 ] , and preclinical studies have demonstrated such an anti - inflammatory effect of rt [ 13 , 14 , 18 , 28 , 37 ]  . neutrophilic granulocytes are critical effector cells in innate immunity and play a vital role in phagocytosis and bacterial killing [ 39 ]  . 
however , until now the influence of irradiation on cellular function has only been poorly illuminated [ 38 ] , particularly at doses in the low dose range used in benign diseases [ 24 ]  . a function of neutrophilic granulocytes is the production and release of reactive oxygen species ( ros ) [ 36 ] , a process known as oxidative or respiratory burst [ 6 ]  . 
 thus , the phagocytic function of granulocytes can be elegantly detected and quantified using cl [ 1 ]  . it was the aim of the current study to investigate the influence of various irradiation doses in the low and medium dose range on the release of ros by cl and thus indirectly obtain information about granulocyte functions . 
this should make it possible to determine the optimal irradiation dose for either stimulation or suppression of anti - inflammatory activity . material and methods cells fresh blood from three healthy volunteer donors was used as leukocyte source after separating plasma and red blood cells . 
 buffy coat ( 35 ml ) was layered on 15 ml lymphoprep ( nycomed pharma , oslo , norway ) in a conical 50 - ml tube ( falcon , becton dickinson labware , franklin lakes , nj , usa ) and centrifuged at 1 , 000 g for 20 mthe band containing mononuclear cells was removed . 
remaining erythrocytes were lysed by adding nh4cl 0.84% for 20 min at 37 c and then centrifuged aga after washing , cell count was adjusted to 1 106 / ml in rpmi 1640 without fetal calf serum ( fcs )  . 
for the initial measurements 50 l of luminol ( sigma , deisenhofen , germany ) , 1 : 1 , 000 dilution of 1.77 mg dissolved in 1 ml dimethylsulfoxide ( sigma ) at a final concentration of 44.5 m , was added and the measurement started . 
measurements on cells not stimulated by pma were excluded from analysis . statistical analysis statistical analyses were performed using the program package spss 11.01 ( spss , chicago , il , usa )  . 
in order to investigate the relevant changes in ros release after pma stimulation and minimize the influence of the absolute cell count and day - by - day variations , relative changes were calculated with the starting point before stimulation set at 100% . 
differences between relative changes and radiation were evaluated using the nonparametric mann - whitney u - test at a significance level of p < 0.05. this research study was performed under the approval of the institutional review board and in accordance with the helsinki declaration of 1975 , as revised in 1983 , 1989 , 1996 , 2000 , and 2002 . 
informed consent was obtained by all donors prior to inclusion in the study . results pma stimulation caused an immediate ros release within seconds , reaching the maximum at 10 min and decreasing during a 60 - min observation period . 
interestingly , higher doses of 6 and 12 gy were not able to completely destroy the functional capacity ; by contrast , ros release increased ( table 1 )  . 
granulocytes are involved in acute and chronic inflammatory reactions [ 31 , 32 ] , and knowledge about function and optimal dose could be helpful in finding the optimal radiation dose for either stimulation or suppression of anti - inflammatory activity , which can explain the pain relief by low - dose rt . 
 therefore , the aim of this study was to investigate the effect of irradiation at various doses on phagocytic function . it is generally assumed that the higher the radiation dose and the effect on granulocyte function , the lower the ros release should be [ 7 , 11 ]  . 
on the other hand , it was recently shown that irradiation given in single doses of up to 32 gy did not significantly diminish ros release of granulocytes [ 7 ]  . 
at 12 gy the activity remained at the same level and , as previously shown , did not significantly compromise granulocyte function [ 7 ]  . biphasic phenomena have also been reported with other biological effects after low - dose ionizing irradiation . 
an explanation for these findings could be the involvement of differential induction of transcription and translation , as shown for cellular repair mechanisms at various radiation doses [ 4 , 15 , 26 ]  . in benign inflammatory and painful disorders , the granulocyte population at the inflammatory site is generally treated with total doses in the range between 1 and 5 gy [ 23 ]  . 
admittedly , this neoplastic mouse leukemic monocyte - macrophage cell line is far from the physiological function of native human granulocytes , and some authors could not detect any oxidative burst formation in this cell line [ 8 ]  . in addition , animal experiments support our findings . 
increased phagocytic activity was found at 1 gy , followed by a marked decrease in the left hind leg of rabbits treated at a dose range between 0.5 and 10 gy [ 10 ]  . the sequence of ros release is very much similar in all individuals , but the amount of ros release varies greatly between individuals [ 12 ]  . 
 [ 11 ] reported higher amounts of ros release , which can be easily explained by these interindividual variations , underlining the importance to compare relative values in this setting . 
the variations in our study cause a high standard deviation as well as a large 95% confidence interval , but do not influence statistical analysis , which revealed a clear dose - dependent relationship using the nonparametric mann - whitney u - test , because a normal distribution was not assumed . 
although the ( cid : 1 ) - failure of second type is higher and the selectivity is somewhat lower than in parametric tests , a sinusoidal curve was statistically confirmed [ 11 , 12 ]  . 
in future , a more detailed analysis at the molecular level has to be added . it is known , that phagocytosis with release of ros can also provoke tissue damage , if it proceeds uncontrolled . 
clearly , the inflammatory reaction represents a complex , well - balanced system of oxidative and antioxidative valences [ 6 , 31 , 36 , 39 ] , where low - dose rt may have immunomodulatory effect [ 7 , 10 , 11 ]  . 
 so far , the optimal dose of rt for acute or chronic inflammatory disorders has not been established , as recent patterns - of - care studies show [ 21 , 33 ]  . 
 even though ros release in phagocytic activity is not the only mechanism involved in local inflammation [ 31 , 39 ] but definitely playing a key role [ 6 , 31 , 36 , 39 ] , our findings provide a further possible explanation for the differentiated beneficial effect of irradiation at selected dose levels in inflammatory disorders . 
 strahlentherapie und onkologie original article dose - response relations for anal sphincter regarding fecal leakage and blood or phlegm in stools after radiotherapy for prostate cancer radiobiological study of 65 consecutive patients panayiotis mavroidis1 , 2 , massoud al - abany3 , sgeir r . 
lind1 , gunnar steineck3 , anders brahme1 background : the estimation of the parameters that describe the dose - response relations of anal sphincter regarding the clinical endpoints of fecal leakage and blood or phlegm in stools is important in the optimization of prostate cancer radiotherapy . 
also , the validity of the relative seriality model for this clinical case needs to be examined by associating the clinical follow - up results with the predicted complication rates . patients and methods : in this study , 65 patients who received radiation therapy for clinically localized prostate adenocarcinoma are analyzed . 
the clinical utilization of the calculated parameters in predicting anal sphincter complication probabilities was illustrated by applying the best estimate of the parameters to a subset of the patient population . results : the estimated values of the parameters for the two clinical endpoints are d50 = 70.2 gy , = 1.22 , s = 0.35 for fecal leakage and d50 = 74.0 gy , = 0.75 , s 0 for blood or phlegm in stools . 
diminishing the biologically effective uniform dose to anal sphincter < 4045 gy may significantly reduce the risk of fecal leakage or blood or phlegm in stools for patients irradiated for prostate cancer . key words : radiobiological parameters prostate cancer fecal leakage blood or phlegm in stools ntcp relative seriality strahlenther onkol 2005 ; 181 : 293306 doi 10.1007 / s00066 - 005 - 1313 - y dosis - wirkungs - beziehungen fr die analsphinkterfunktion hinsichtlich stuhlinkontinenz , blutoder schleimabgang nach strahlentherapie des prostatakarzinoms . 
eine radiobiologische studie an 65 patienten hintergrund : um die strahlenbehandlung des prostatakarzinoms optimieren zu knnen , ist ein modell der dosis - wirkungs - beziehung fr die analsphinkterfunktion notwendig , dessen parameter verlsslich geschtzt werden knnen . 
das klinische ergebnis und die dosisverteilung im analsphinkter waren 1 department of medical radiation physics , karolinska institutet and stockholm university , sweden , 2 department of medical physics , larissa university hospital , greece 3 departments of clinical cancer epidemiology and oncology - pathology , karolinska institutet , stockholm , sweden , 4 stockholm center for public health , sweden , 5 department of medical hospital radiation physics , sder hospital , sweden , 6 department of oncology , radiumhemmet , karolinska hospital , stockholm , sweden , 7 department of radiology , karolinska hospital , stockholm , sweden . received : may 3 , 2004 ; accepted : february 2 , 2005 strahlenther onkol 2005 no . 
 ergebnisse : die schtzwerte der parameter der zwei klinischen endpunkte sind d50 = 70 , 2 gy , = 1 , 22 , s = 0 , 35 fr stuhlinkontinenz und d50 = 74 , 0 gy , = 0 , 75 , s 0 fr blut oder schleim im stuhl . 
eine reduktion der biologisch effektiven , uniformen dosis des analsphinkters unter 4045 gy knnte die risiken der stuhlinkontinenz und von blut oder schleim im stuhl fr prostatakarzinom - patienten signifikant senken . 
 schlsselwrter : radiobiologische parameter prostatakarzinom stuhlinkontinenz blut oder schleim im stuhl risiko von normalgewebereaktionen relative seriality introduction in cancer radiotherapy the prescribed dose needed to eradicate the involved tumors is limited by the risk of frequent and severe unwanted effects . 
late side effects associated with radiotherapy of prostate cancer can permanently deteriorate the patients quality of life [ 5 , 8 , 13 , 21 , 30 , 42 ]  . 
the incidence of radiation - induced rectal injury depends on many factors and the knowledge on normal - tissue radiosensitivity is weak [ 2 , 17 , 29 , 39 ]  . 
in prostate cancer radiotherapy , the main organs at risk are the urinary bladder , the anal sphincter , the rectum , and the nerves and vessels involved in erectile function [ 46 , 8 , 44 ]  . 
this is supported by randomized studies where fewer patients developed radiation - induced proctitis and bleeding , when a dose distribution of high conformity was applied in comparison with simpler techniques [ 13 , 38 ]  . 
it has been reported that dose - volume histograms ( dvhs ) delivering 6075 gy to 7030% of the anterior rectal wall , respectively , were associated with higher risk of rectal bleeding than lower respective values [ 23 ]  . 
 [ 4 , 6 , 7 ]  . to quantify the clinical improvements in dose distributions delivered by conformal instead of conventional radiotherapy , radiobiological parameters and models are useful . 
newer and more accurate clinical data about dose - response relations of tumors and normal tissues are reported by many investigators at an increasing rate [ 2 , 17 , 18 , 25 , 31 , 37 ]  . 
for this reason , analysis of large patient datasets should be conducted before introducing information about normal - tissue radiation reactions in the clinical routine [ 25 , 28 , 35 ]  . 
a number of different radiobiological models have been developed to calculate normal - tissue complication probability ( ntcp ) , which is very important in the evaluation and comparison of treatment plans [ 9 , 11 , 26 , 27 ]  . 
in the case of prostate cancer radiotherapy , radiobiologically optimized treatment planning can be performed using relevant dose - response parameters , which can be estimated from well - organized studies of previously treated patients . 
however , the clinical utilization of such parameters and means by which the readers may examine whether certain parameters are applicable to their local organ delineation methods and treatment techniques have been illustrated by only a few studies [ 28 , 37 ]  . the aim of the present study is to relate long - lasting fecal leakage and blood or phlegm in stools after radiation therapy with the dose delivered to patients with clinically localized prostate cancer . 
for a certain dose range , where a statistically valid number of patients exist , the probabilities of fecal leakage and blood or phlegm in stools following radiation therapy are calculated . 
 patients and methods patient selection the patient group consisted of 65 consecutive patients with clinically localized prostate adenocarcinoma treated by external radiotherapy at radiumhemmet , karolinska hospital , stockhol the study population included all patients that were alive in november of 1998 and had been treated between 1995 and 1996 . 
a questionnaire including modules assessing bowel symptoms , sexual function and urinary symptoms was sent to the patients 24 years after treatment [ 4 , 10 , 44 ]  . the treatment modality was decided by a team of radiation oncologists and medical physicists prior to therapy . 
accurate delineation of anal sphincter during treatment planning and accurate dose delivery to the examined tissue according to the treatment plans are the basis of the analysis in this work . 
 treatment techniques and dose planning information on the external - beam radiation therapy including dose , treatment protocol , collimation technique , treatment period , and disease stage as well as grade was retrieved from the hospital records . 
the planning was based on contiguously acquired ct slices with thickness of 1.0 cm inferior to the level of the ischial tuberosities to the apex of an empty bladder or the bottom of the sacroiliac joint . 
during treatment planning , corrections for tissue inhomogeneities were also performed . the gross target volume ( gtv ) was the entire prostate gland and the seminal vesicles as visualized on the planning ct scan . 
the planning target volume ( ptv ) was derived from the ctv by adding a 2 - cm margin around it apart from the apex , where the margin was 2.5 cm to allow positioning and mobility uncertainties concerning the microscopic spread outside the ctv [ 1 , 15 , 43 ]  . 
 a three - field technique ( one anterior and two oblique posterior fields ) was delivered to 36 patients as shown in the upper graph of figure 1 , while 29 patients were treated with a four - field box technique ( two opposing anteroposterior - posteroanterior [ ap - pa ] fields and two opposing lateral fields ; figure 2 , upper graph )  . 
dose - response relations for anal sphincter from prostate cancer radiotherapy ( cid : 1 ) , has been provided by heterogeneous dose distribution , d many authors [ 3 , 26 , 27 , 33 ]  . 
in this model the fundamental radiobiological parameters are the following : d50 is the dose corresponding to the 50% complication rate and is the maximum normalized gradient of the dose - response curve . 
vi = vi / vref is the fractional subvolume of the irradiated organ compared to the reference volume for which the values of d50 95 85 anal sphincter once a week , twice or three times a week , four to six times a week , and seven times a week or more . 
first , the effects at any frequency of symptoms were assessed and second , the frequency of more prevalent symptoms ( e.g. , twice a week or more )  . 
 the relative seriality model and the biologically effective uniform dose , d the inactivation of functional subunits ( fsus ) in normal tissues is directly related to the complications observed after the therapeutic use of radiation . 
the dependence of normal - tissue injury on the organization of the fsus and internal structure of the irradiated organ makes the calculation of its response probability a very complicated task . 
the mathematical expression of the response prob ( cid : 1 ) ability , pi ( d ) ( i denotes injury ) , for a normal tissue being irradiated with a strahlenther onkol 2005 no . 
the linear - quadratic model was used to correct each dose distribution in the anal sphincter to 2 gy per fraction [ 19 ] and the / ( cid : 2 ) ratio assumed was 3 gy . 
the uniform dose that is ( cid : 1 ) , delivered biologically as effective as the dose distribution , d to each patient is determined using this concept , which was introduced by mavroidis et al . 
the two sets of the relative seriality models radiobiological parameters estimated by the maximum likelihood method are used to calculate the effectiveness of the individual dose distributions applied to each patient . 
 fitting response models to clinical data using the maximum likelihood method the best estimates of the radiobiological parameters of the relative seriality model were determined together with their cis by fitting the theoretical predictions for complications to the clinical follow - up results . 
the maximum likelihood method was used , which determines the best estimates of the parameters by maximizing the likelihood to reproduce the given pattern of observations [ 20 , 25 ]  . 
the fitting of the likelihood function and the estimation of the cis were performed by using the minos minimization package and locally developed code [ 41 ]  . to determine the cis of the estimated parameters in pathologic likelihood functions , which are usually non - normal , the values of the parameters should be searched numerically to find multidimensional confidence regions . 
this is achieved by finding the hyper - volume lnl , which is produced by calculating the values of the log - likelihood function for dif ( cid : 1 ) ferent values of d50 , and s . 
the region [ x max ] , which is treated as a confidence region of probability content a is defined by the intersection of the above hyper - volume with the volume lnl = lnlmax 1 / 2 ( cid : 2 ) 2 a ( k ) , where k is the number of dimensions . 
in this study , the 68% cis of the radiobiological parameters d50 , and s were calculated from their 3 - d 68% joint confidence region . ( cid : 1 ) min , x goodness of fit of the dose - response parameters three independent statistical methods were used to estimate the goodness of fit . 
in this method , assuming that the log - likelihood function follows a gaussian distribution and comparing the expected mean and maximum values of the lnl considering the magnitude of the variance , the goodness of fit can be determined . 
the fit can be considered optimal for large probabilities ( close to 1 ) , which would mean that a very good agreement between the two distributions ( predictions , clinical results ) has been reached . 
the numerator of the ( cid : 2 ) 2 - formula is a measure of the spread of the observations , whereas the denominator is a good measure of the expected spread . 
if the probability is small , either the data sample is not representative of the parent distribution or the predicted distribution is not a good estimate of the parent distribution . 
 in the analysis using receiver operating characteristic ( roc ) curves [ 22 , 45 ] the true positive ratio ( tpr ) , which is the ratio of observed positive incidences above a series of cutoff levels , pcut , to the total number of positive incidences , and the false positive ratio ( fpr ) , which is the ratio of observed incidence - free patients above pcut to the total number of incidence - free patients , are determined . 
dose - response relations for anal sphincter from prostate cancer radiotherapy v / v0 v / v0 of the predictive model to correctly classify those patients with and without the clinical endpoint is measured by the area under the roc curve . 
an area under the curve equal to 1 indicates a perfect discrimination of the complication and complication - free patient subgroups , which implies a perfect classification of the observed against the predicted complication results . 
similarly , for the clinical endpoint of blood or phlegm in stools the positive association with dose was significant at the cutoff of 40 gy with or = 8.68 and 95% ci of 1.0373.22. fecal leakag e complications 100% complication ( cid : 1 ) free anal sphincter 140 d / gy 70d / gy blood or phlegm in stools complications 100% complication ( cid : 1 ) free anal sphincter 70d / gy 140 d / gy figure 3 . 
in the left diagrams , the mean cumulative dose - volume histograms of the whole study population , divided into the complication - free group and the group of patients with radiation - induced fecal leakage and blood or phlegm in stools at least twice a week , are shown . 
the volume dependence of anal sphincter for the two clinical endpoints is demonstrated by assuming that : ( a ) the whole organ ( 100% ) receives a uniform dose ; ( b ) two thirds ( 66% ) of the organ receive a certain uniform dose and the remaining part receives 5% of this dose ; and ( c ) one third ( 33% ) of the organ receives a uniform dose and the rest 5% of this dose . 
die diagramme links zeigen die mittleren kumulativen dosis - volumen - histogramme aller in dieser studie erfassten patienten , unterteilt in die komplikationsfreie gruppe und die patientengruppe mit mindestens zweimal wchentlich auftretend strahlungsinduzierter stuhlinkontinenz und blut oder schleim im stuhl . 
die volumenabhngigkeit des analsphinkter wird fr die zwei klinischen endpunkte dargestellt unter folgenden annahmen : ( a ) das gesamte organ ( 100% ) erhlt eine einheitliche strahlendosis , ( b ) zwei drittel ( 66% ) des organs erhalten eine bestimmte einheitliche dosis und der brige teil erhlt 5% dieser dosis , und ( c ) ein drittel ( 33% ) des organs erhlt eine einheitliche dosis und der rest 5% dieser dosis . 
of the patients that manifested blood or phlegm in stools at least twice a week , four ( 11.1% ) had the three - field as the treatment technique and six ( 20.7% ) were treated with the four - field box technique , respectively . 
dose - response relations for anal sphincter from prostate cancer radiotherapy and the fractionation protocols of the two applied techniques are given . in order to assess the differences between the dvhs of the patients with and without fecal leakage and blood or phlegm in stools and to find the dose and volume threshold where patient groups reported more or fewer symptoms , the distributions of dose over the volumes of anal sphincter and rectum were calculated for each patient . 
the results of the analysis did not show any relation between the mean dose to the rectum or rectal wall and blood or phlegm in stools and fecal leakage symptoms . 
there was no difference between the mean dvh for rectal wall of the patients with and without blood or phlegm in stools at any frequency or at least twice a week . the best estimates of the model parameters for the two complication endpoints used in the study are given in table 2 together with their 68% cis . 
the best estimates of the model parameters obtained were d50 = 70.2 gy , = 1.22 , s = 0.35 for the clinical endpoint of fecal leakage and d50 = 74.0 gy , = 0.75 , s 0 for blood or phlegm in stools . 
the spread among the dose - response curves corresponding to whole and partial anal sphincter irradiation indicates that the induction of fecal leakage and blood or phlegm in stools varies substantially with the irradiated volume . 
this is indicated in this study by the observation that in the three - field technique , which spares anal sphincter a little better , fewer patients showed complications compared to the four - field box technique . 
from the viewpoint of functional organization , anal sphincter shows a parallel - like architecture for the two endpoints examined ( especially for blood or phlegm in stools ) , which is expressed in the relative seriality model by the low s values . 
 by calculating the hyper - volumes of lnl above the threshold of lnlmax 1 / 2 ( cid : 2 ) 2 68% ( 3 ) , the 68% joint confidence region of the parameters d50 , and s was obtained ( figure 4 , upper diagram )  . 
the cis of the dose - response curves for fecal leakage and blood or phlegm in stools can be obtained by using d50 and values from their individual confidence regions . 
 these diagrams practically illustrate the uncertainties from the interpatient radiosensitivities and discrepancies between the calculated and the delivered dose , which are involved in the estimation of the dose - response curves . 
the approach that any combination of the parameter values from their joint confidence region can be possible for an individual patient was followed to determine the corresponding cis of the dose - response relations . 
to estimate the impact of the volume effect of anal sphincter to the response probability , diagrams of d and mean dose against pi were produced for fecal leakage and blood or phlegm in stools , respectively , as shown in figure 5 . 
the values of reduced ( cid : 2 ) 2 that were calculated were 0.085 for fecal leakage and 0.247 for blood or phlegm in stools ( table 3 )  . 
these values indicate that the relative seriality model and the estimated parameters reproduce very well the pattern of the clinically recorded complications , especially for the endpoint of fecal leakage . 
the area under the roc curve , which measures the ability of the model to classify the patients with and without complications , is a measure of the predictive power of the applied radiobiological model . 
these values indicate that the model distinguishes quite well the groups of patients with and without complications based on their treatment characteristics ( figure 6 , left diagrams )  . 
the dose - response curves for the two clinical endpoints of anal sphincter are calculated for a range of uniform doses using the relative seriality model and the estimated radiobiological parameters ( figure 6 , right diagrams )  . 
the hyper - surface shown in the upper graph illustrates the fall - off of the maximum likelihood function in the region around the best estimates of the radiobiological parameters . 
to examine whether the theoretical curve reproduces the observed complication rates , the patients confined in the dose ranges 4448 , 4853 , and 5358 gy are selected in the case of fecal leakage . 
in these diagrams , the associations of the mean dose , dmean , and biologically effective , as a function of the response probability , pi , are presented for the two clinical uniform dose , d endpoints . 
in the first case , the fsus are organized serially along the circumference of anal sphincter causing complications even if a small part of anal sphincter is located inside the high dose region . 
in the parallel organization , the fsus are arranged in the longitudinal direction , which means that the whole circumference of anal sphincter has to be irradiated to a high dose to cause complications . 
im ersten fall sind die fsus seriell entlang der umfangslinie des analsphinkters angeordnet , was zu komplikationen selbst dann fhrt , wenn ein kleiner teil des analsphinkters innerhalb der hochdosisregion liegt . 
in der parallelen organisation sind die fsus longitudinal angeordnet , was bedeutet , dass zum auslsen von komplikationen der gesamte umfang des analsphinkters von einer hohen strahlendosis erfasst werden muss . 
the goodness of fit was determined for the patient population by three different methods ( normal error distribution , 2 - test , receiver operating characteristic [ roc ] analysis )  . 
in this diagram , statistically valid comparisons between average predicted and true follow - up rates can be made only for dose ranges comprising a considerable number of patients with and without complications . 
nevertheless , this method can be suitably used to examine , if a set of parameters is compatible with a certain treatment technique given that the same endpoint definition is used . 
 discussion of the patients that participated in this study and were analyzed for anal sphincter complications , 12.3% had radiation - induced fecal leakage and 15.4% showed blood or phlegm in stools . 
according to these studies and the present one , fecal leakage may be due to damage to the blood vessels that provide blood to the anal sphincter muscles . diminishing the dose given to anal sphincter may be more important than diminishing the dose given to rectum wall , if one wants to reduce the risk of long - term blood or phlegm in stools or fecal leakage . 
a correlation was found between the risk for these symptoms and mean dose and dvhs for anal sphincter , but no certain associations were found between these symptoms and dose given to rectu possibly , there is a threshold in the vicinity of a mean dose of 4045 gy given to the anal sphincter below which there may be little or no risk of long - term fecal leakage . 
it was found that among patients receiving a mean dose of < 44 gy to the anal sphincter , one only patient reported fecal leakage at least twice a week . 
the comparison of data from different sources is vulnerable to different factors like endpoint definition , follow - up recording , adequate dosimetric data , and the different radiobiological models used . 
 one of the very interesting points of this study is that of the low relative seriality , s values that are derived , especially for the endpoint of blood or phlegm in stools [ 4 , 8 ]  . 
in the right diagrams , the dose - response curves of anal sphincter , which were produced using the relative seriality model and the estimated radiobiological parameters ( solid line ) , are presented . 
the biologically effective , is used in the dose axis , because this dose unit allows every patient of the uniform dose , d study population to be found on the theoretical response curve . 
in den diagrammen rechts werden die dosis - wirkungs - kurven der analsphinkterfunktion wiedergegeben , die mit hilfe des relative - seriality - modells und der geschtzten radiobiologischen parameter ( durchgezogene linie ) erstellt worden sind . 
this is because the response probabilities of the individual fsus would be identical , since all of them would receive the same dose , which prevents the identification of their structural association . 
for similar reasons , the volume of the whole organ should be used as the reference volume , although selecting a large part of the organ can also be done in certain cases . 
in this way , sparing part of the organ shows , if this is adequate for retaining its function , which will lead to the estimation of the tissue volume effect . 
for a tissue that shows a parallel pattern and dmean appear to regarding a certain clinical endpoint , d becomes higher than the coincide , whereas in serial patterns d mean dose . 
this is because the mean dose is usually the result of averaging over hot and cold regions and in the case of serial tissues a hot spot cannot be counteracted by a corresponding cold spot . 
in this case , the increased relative seriality of anal sphincter regarding fecal values against dmean , while these leakage results in higher d quantities are very similar for blood or phlegm in stools , which is characterized by a very low relative seriality . 
consequently , the increase of biologically effective uniform dose with decreasing partial volume of the normal tissue being irradiated is an expression of its volume effect for the certain endpoint . 
in the left diagram , the fsus are arranged in such a way that even irradiating a small volume of anal sphincter circumference to a high dose is associated with a high risk for fecal leakage at least twice a week . 
in the right diagram , the fsus are organized longitudinally , which is better related to a more parallel behavior of anal sphincter for blood or phlegm in stools at least twice a week . 
consequently , the final result of the fitting process is a dose - response curve within an interval , which is a quantitative evaluation of the effect of including parameter uncertainties in the radiobiological model analysis . 
 the statistics shown in table 3 indicate that for both of the clinical endpoints the radiobiological model used and its estimated parameters predict complication rates , which closely agree with the observed complication incidences for the study population . 
however , apart from the purpose of verifying the estimated parameters , the presented statistical methods also serve as recommended means for checking if another patient population associated with another irradiation technique or treatment methodology is compatible with the derived model parameters . 
before using parameters from the literature or other sources in the clinic , such a verification of their validity should always be done with the aim that locally derived data will support and update the initially used parameters . in the present work , the complete dosimetric information was used in the form of anal sphincter dvhs , which were calculated from the 3 - d dose distributions . 
to simplify the calculations in the quantification of normal - tissue response , a scalar quantity such as the mean dose could be used but at the cost of losing important information in the data structure . 
in the light of these observations , a further analysis of the patient population studied using a radiobiological model , which would take the location of the different partial volumes irradiated into account , would be useful . 
the dose - response curves of anal sphincter for radiation - induced complications are described by the parameters d50 = 70.2 gy , = 1.22 , s = 0.35 for fecal leakage at least twice a week and d50 = 74.0 gy , = 0.75 , s 0 for blood or phlegm in stools at least twice a week , respectively . 
 acknowledgments this research was supported by grants from the cancer society in stockholm , the king gustaf v jubilee fund , stockholm , and within the center of excellence by the swedish national board for industrial and technical development . 
 strahlentherapie strahlentherapie und onkologie und onkologie original article individual radiosensitivity does not correlate with radiation - induced apoptosis in lymphoblastoid cell lines or cd3 + lymphocytes anja wistop1 , ulrike keller1 , carl n . 
distel1 background and purpose : spontaneous and radiation - induced apoptosis of lymphoblastoid cell lines ( lcls ) derived from healthy donors , cancer patients and donors with radiosensitivity syndromes as well as cd3 + lymphocytes from patients with grade 3 late toxicity were investigated as a possible marker for the detection of individual radiosensitivity . 
these investigations are based on the hypothesis that hypersensitive patients have reduced levels of apoptosis after in vitro irradiation as a result of a defect in the signaling pathway . material and methods : epstein - barr virus - ( ebv - ) transformed lcls derived from five healthy donors , seven patients with heterozygous or homozygous genotype for ataxia - telangiectasia or nijmegen breakage syndrome and five patients with grade 3 late toxicity ( rtog ) were investigated . 
apoptotic rates were measured by the tunel assay followed by customized image analysis . results : four out of seven radiosensitivity syndrome patients were identified to have an increased cellular radiosensitivity as determined by reduced apoptotic rates after irradiation of their respective lcls . 
spontaneous apoptotic rates were very homogeneous among all 39 samples from controls and patients , while lymphocytes of all cancer patients showed significantly lower radiation - induced rates . conclusion : only a subgroup of hypersensitive patients may be identified by reduction of radiation - induced apoptotic rate . 
 the authors suggest that this assay can be used in combination with additional tests evaluating dna double - strand break repair , cell - cycle control and chromosomal aberrations for the evaluation for individual hypersensitivity . key words : radiation - induced apoptosis individual radiosensitivity hypersensitivity lcls lymphocytes strahlenther onkol 2005 ; 181 : 32635 doi 10.1007 / s00066 - 005 - 1372 - 0 individuelle radiosensibilitt korreliert nicht mit strahleninduzierter apoptose in lymphoblastoiden zelllinien oder cd3 + - lymphozyten hintergrund und ziel : spontane und strahleninduzierte apoptose in lymphoblastoiden zelllinien ( lcl ) von gesunden , krebspatienten und spendern mit strahlenempfindlichkeitssyndromen sowie in cd3 + - lymphozyten von patienten mit spttoxizitt grad 3 wurden mit dem ziel untersucht , apoptose als einen marker zur detektion von strahlenempfindlichkeit zu verwenden . 
dies basiert auf der hypothese , dass erhht strahlenempfindliche zellen auf in - vitro - bestrahlung mit erniedrigten apoptoseraten reagieren , was durch eine strung in der signaltransduktion bedingt ist . 
 material und methodik : epstein - barr - virus - ( ebv - ) transformierte lcl von fnf gesunden spendern , sieben patienten mit heterozygotem oder homozygotem genotyp fr ataxia teleangiectatica oder nijmegen - breakage - syndrom und fnf patienten mit spttoxizitt grad 3 ( rtog ) wurden untersucht . 
die apoptoseraten wurden mit dem tunel - assay und einem selbst entwickelten bildanalysesystem gemessen . ergebnisse : nur vier der sieben patienten mit strahlenempfindlichkeitssyndromen wiesen eine durch erniedrigte apoptoseraten belegte zellulre strahlenempfindlichkeit auf . 
die spontanen apoptoseraten der lymphozyten aller 39 patienten 1 department of radiation oncology , friedrich alexander university erlangen - nuremberg , erlangen , germany 2 division of research , peter maccallum cancer centre , east melbourne , victoria , australia . received : september 28 , 2004 ; accepted : february 2 , 2005 strahlenther onkol 2005 no . 
apoptosis and individual radiosensitivity und kontrollen waren in sich sehr hnlich , whrend die lymphozyten der krebspatienten erniedrigte strahleninduzierte apoptoseraten aufwiesen . schlussfolgerung : nur eine untergruppe der erhht strahlenempfindlichen patienten kann durch erniedrigte apoptoseraten identifiziert werden . 
fr die detektion von erhhter strahlenempfindlichkeit wre eine kombination mit anderen tests , die die dna - doppelstrangbruch - reparatur , zellzykluskontrolle und chromosomale aberrationen untersuchen , zu empfehlen . schlsselwrter : strahleninduzierte apoptose individuelle strahlenempfindlichkeit berempfindlichkeit lymphoblastoide zelllinien lymphozyten introduction to identify the relatively small proportion of patients with an elevated risk for major acute and late radiation toxicity would be an attractive accomplishment for the practice of radiation oncology . 
by adapting single dose , total dose and fractionation of a given radiation treatment schedule to fit individual radiosensitivity , one would expect to have reduced numbers of individuals with severe late effects in a given patient population without compromising the intended tumoricidal effect of radiotherapy [ 29 ]  . 
concurrently , in those individuals who are found to be rather insensitive , dose escalation trials with the aim to increase total dose may be considered , leading to higher tumor cure rates . while the known radiosensitivity syndromes are relatively rare diseases , around 14% of patients will experience late complications due to their increased intrinsic radiosensitivity . 
 patients with radiosensitivity syndromes , like ataxia - telangiectasia ( at ) [ 32 ] , nijmegen breakage syndrome ( nbs ) [ 34 ] , bloom syndrome and mutations in hmre11 [ 33 ] and ligase iv [ 25 ] , have a markedly increased cellular radiosensitivity . 
common features of patients with these genomic instability syndromes or dna repair disorders are short stature , immunodeficiency , predisposition to cancer , elevated radiosensitivity , and a chromosomal instability . 
if such patients need radiotherapy , dose has to be reduced by a factor of 23 [ 14 ] ; otherwise radiation treatment with a conventional total dose may result in severe toxicity and death [ 12 ]  . however , in addition to these hypersensitivity syndromes , a proportion of patients exist who also suffer from severe treatment - related complications . 
 cells from patients with radiosensitivity syndromes can be identified by a twoto threefold increase in chromosomal aberrations as detected by fluorescence in situ hybridization ( fish ) or cell inactivation by the clonogenic assay or other functional assays [ 18 , 19 , 24 ]  . 
it should be noted , that cell inactivation and subsequent removal of cells by apoptosis protect the individual against genomic alterations in daughter cells and no late complications can result from these cells . 
the most commonly used method is to determine the dna subpeak in flow cytometry , which is reported to be in good agreement with the tunel assay [ 1 , 6 ]  . 
the tunel assay is considered to be highly specific for apoptosis . our investigations provide data on spontaneous and radiation - induced apoptosis in epstein - barr virus - ( ebv - ) transformed lymphoblasts and cd3 + lymphocytes . 
a total of 17 lymphoblastoid cell lines ( lcls ) were used , derived from healthy donors as well as from individuals with heterozygous and homozygous genotype for at and nbs . 
in addition , five patients with a clinically well - documented hypersensitivity against radiation were included , for whom cellular hypersensitivity was documented in advance by fish analysis of radiation - induced chromosomal aberrations [ 18 ]  . 
apoptosis and individual radiosensitivity apoptosis , where five patients had a clinical hypersensitivity as well as a proven cellular hypersensitivity to radiation . material and methods lymphoblastoid cells lymphocytes were obtained from five healthy donors and transformed into lymphoblastoid cells by ebv [ 23 ]  . 
three ebv - transformed cell lines from at patients with homozygous and one at patient with heterozygous genotypes were provided by the institute for human genetics , university of erlangen - nuremberg , germany . 
the cancer patients ( twelve female and six male ) suffered from different primary tumors and seven of these showed a significant clinical radiosensitivity of at least grade 3 according to the rtog late toxicity scale within 1 year after treatment . 
heparinized ( 200 l liquemin 2 , 500 iu , roche , basel , switzerland ) blood ( 10 ml ) was drawn from healthy donors and patients after a written informed consent had been obtained . 
ficoll separation solution was coated with the blood ( 17.5 ml ficoll , biochrom ag , germany ) and centrifuged about 20 min ( 300 rcf / decel 0 )  . 
 after centrifugation blood cells were resuspended in 400 l phosphate - buffered saline ( pbs ) and 20 l magnetically labeled antibodies ( macs cd3 microbeads , miltenyi biotec , bergisch gladbach , germany ) and incubated 15 min at 10 c . 
the cells were centrifuged and distributed into cell culture flasks containing 4 ml mediuradiation exposure using 120 - kv x - rays at room temperature under air with 2 and 5 gy at a dose rate of 2.2 gy / min ( isovolt , seifert , germany ) was followed by incubation at 37 c in 5% co2 . 
cell suspension was partially dropped into a ring formed by a liquid blocker on the slides and after the evaporation of fix solution slides were preserved in 70% ethanol solution at 20 c . 
 for the tunel - tdt ( terminal transferase nick - end labeling ) assay ( apoptag fluorescein , oncor , gaithersburg , md , usa ) , the slides were coated first by equilibration buffer ( 75 l ) for 10 s followed by 110 l tdt reaction buffer and incubated at 37 c . 
the cells were incubated for 30 min at room temperature in darkness in 65 l anti - digoxigenin conjugate and after an additional four washes in pbs , the dry slides were coated with 40 l propidium iodide for 5 min and mounted on vectashield ( vector laboratories , orton southgate , uk )  . 
biomas software ( biomas , msab , erlangen , germany ) was used to capture and analyze images acquired by a hitachi three - chip ccd camera ( vh - cc20a , hitachi denshi , rodgau , germany )  . 
then , the rate of apoptosis was determined by a semiautomatic analysis systeafter acquisition of the first of a series of images , thresholds for background reduction and identification of red and green cells had to be identified once . 
counts of total cells and positive green cells were transferred to an excel sheet ( microsoft excel 2000 , microsoft corporation , redmond , wa , usa ) and the fraction of apoptotic cells was calculated . 
 spontaneously occurring apoptosis ( a ) and apoptosis 48 h after irradiation with a dose of 2 gy x - rays ( b ) were detected by the tunel assay , where red cells ( propidium iodide ) are nonapoptotic cells and yellow and green cells are apoptotic cells . 
a cutoff was computed by the software and indicated by a line , and all cells with a higher fluorescence than seven grey values for the spontaneous ( e ) and seven grey values for the x - ray - induced apoptosis by a dose of 2 gy ( f ) were counted as positive . 
fr die analyse der spontanen apoptose wurden 1 249 zellen ( c ) und fr die durch 2 gy nach 48 h induzierte apoptose 1 279 zellen gezhlt ( d )  . 
ein grenzwert wurde mittels der software generiert , und alle zellen mit einer hheren fluoreszenz als sieben graustufen , sowohl fr spontane ( e ) als auch strahleninduzierte ( f ) apoptose , wurden positiv gewertet . 
in diesem fall waren 5 , 6% und 18 , 1% der zellen apoptosepositiv . statistical methods one - way analysis of variance ( anova ) was used for evaluating the repeated measurements on the controls and cancer patients and for evaluating intraand interindividual differences . 
 results identification of apoptotic cells by image analysis apoptotic cells were identified by the tunel assay , where apoptosis - positive cells were green and cells having no apoptosis were red . 
results of automatic counting with user correction of scored cells were compared to direct counting on the microscope and counting cells on the screen by marking cells with the mouse cursor and direct data transfer to an excel sheet by the count feature of biostrahlenther onkol 2005 no . 
at : ataxia - telangiectasia ; cv : coefficient of variation ; f : f - distribution ; mv : mean value ; n : number of individuals ; nbs : nijmegen breakage syndrome ; p : significance probability ; sd : standard deviation . 
at : ataxia teleangiectatica ; cv : variationskoeffizient ; f : f - verteilung ; mv : mittelwert ; n : anzahl der individuen ; nbs : nijmegen - breakage - syndrom ; p : signifikanzniveau ; sd : standardabweichung . 
at : ataxia - telangiectasia ; cv : coefficient of variation ; f : f - distribution ; mv : mean value ; n : number of individuals ; nbs : nijmegen breakage syndrome ; p : significance probability ; sd : standard deviation . 
at : ataxia teleangiectatica ; cv : variationskoeffizient ; f : f - verteilung ; mv : mittelwert ; n : anzahl der individuen ; nbs : nijmegen - breakage - syndrom ; p : signifikanzniveau ; sd : standardabweichung . 
apoptosis and individual radiosensitivity comparison between spontaneous and radiationinduced apoptosis in ebv - transformed lymphoblasts derived from controls and from patients with radiosensitivity syndromes five lcls derived from healthy donors were used as controls ( figure 2a )  . 
apoptotic rates observed 48 h after irradiation with 2 and 5 gy were corrected by subtraction of spontaneous apoptotic rates , giving levels increasing with dose and similar cvs for both spontaneous apoptosis ( cv 38.6% ) and irradiation with 2 gy ( cv 46.0% ) and 5 gy ( cv 33.4% ; table 2 )  . 
 cd3 + lymphocytes of healthy controls and cancer patients cd3 + lymphocytes from 21 healthy donors were tested as a matched - pair analysis together with 18 patients consisting of five , four and one patient with head and neck , breast and rectal cancer , respectively . 
however , age of control individuals showed a decreasing radiation - induced apoptosis rate by 0.16% year1 at 2 gy and 0.15% year1 at 5 gy ( figure 3 )  . 
mutations in these at individuals were q1425x ( het ) , 1561delag ( het ; terminal exon 44 ) and ivs16 - 1 g - c ( het ; unknown )  . 
the spontaneous rates of heteroand homozygous nbs cell lines differed only slightly from controls ( p = 0.61 ) , however , the 5 - gy values showed a trend to an increase ( p = 0.38 ) of the apoptotic rate for the homozygous cell line ( figure 2c )  . 
 comparison between spontaneous and radiation - induced apoptosis in controls and cancer patients five lcls from cancer patients with severe late toxicity ( rtog grade 3 ) after standard radiotherapy were retrospectively identified . 
apoptotic rates of lcls with at - heterozygous ( open bars ) and at - homozygous ( striped bars ) genotype in comparison to the average of five cell lines from healthy donors ( filled bars ) ( b )  . 
apoptotic rates of lcls with nbs - heterozygous ( open bar ) and nbs - homozygous ( striped bars ) genotype compared to the average of five cell lines from healthy donors ( filled bars ) ( c )  . 
apoptotic rates of five lcls ( stripped and open bars ) derived from cancer patients who have suffered from severe treatment - related grade 3 ( rtog ) toxicity compared to the average of five cell lines from healthy donors ( filled bars ) ( d )  . 
spontane und strahleninduzierte apoptoseraten von fnf lcl von gesunden ( a ) , von lcl mit at - heterozygotem ( weie balken ) und at - homozygotem ( gestrichelte balken ) genotyp im vergleich zum durchschnitt von fnf lcl von gesunden ( graue balken ) ( b ) , von lcl mit heterozygotem ( weie balken ) und homozygotem genotyp ( gestrichelte balken ) fr nbs im vergleich zu gesunden ( graue balken ) ( c )  . 
 discussion radiation - induced apoptosis of in vitro irradiated lcls and cd3 + lymphocytes from patients were studied to evaluate whether patients with radiation hypersensitivity can be identified with this analysis endpoint . 
only two of the five patients with a clinically detected severe toxicity ( rtog 3 ) and cytogenetic proof of elevated cellular radiosensitivity could be identified by lowered apoptotic rates . previous studies on radiation - induced apoptosis as a predictor of individual radiosensitivity have provided conflicting results [ 1 , 48 , 31 , 37 , 38 ]  . 
early events like the translocation of phosphatidylserine from the cytoplasmic surface of the cell membrane to the external cell surface may be detected by the annexin v protein [ 37 ]  . 
frequently , fragmentation of the dna is measured by agarose electrophoresis [ 21 ] , comet assay [ 38 ] , tunel assay [ 1 ] , or flow cytometry [ 4 , 5 , 7 , 8 ]  . 
the tunel assay is based on the action of the endogenous enzyme dnase i which is activated in response to apoptotic signals creating typical 3 ' - oh ends in the fragmented dna . 
this is a standard technique and is compared to other faster and less expensive methods like flow cytometry detecting dna content and morphology ( by light scattering ) figure 3 . 
effect of age on apoptotic rates of the cd3 + cells from controls grouped into 20 to < 40 years , 40 to < 60 years , and 6080 years . 
cells were grown 48 h after irradiation with 2 gy ( striped bars ) and 5 gy ( filled bars ) and the apoptotic rates were analyzed by the tunel assay . 
the difference of cv existed between spontaneous ( cvcontrols = 28.7% ; cvpatients = 42.6% ) as well as radiation - induced ( 5 gy ) apoptosis ( cvcontrols = 24.0% ; cvpatients = 89.9% ) , irrespective of the applied radiation doses . classification of cancer patients into groups with different radiosensitivity apoptotic levels of radiosensitive cancer patients were compared to patients without considerable early or late normal - tissue reactions ( figure 4 )  . 
five of the seven patients with grade 3 toxicity had previously been tested and identified by cytogenetic analysis ( fish ) to have an elevated radiosensitivity [ 17 , 18 ]  . 
it is well known that radiosensitivity is dependent on cell cycle and therefore restricts the utilization of fibroblasts to quantify radiosensitivity by the clonogenic assay to cells in g1 / g0 [ 10 ]  . 
the advantage of having peripheral blood mononuclear cells in g0 has to be compared to the disadvantage represented by different subpopulations like granulocytes , b - cells , natural killer ( nk ) cells , and t - cells . 
quite homogeneous spontaneous rates are found for cd4 + and cd8 + cells [ 38 ] , while cd8 + cells have higher apoptotic rates than cd4 + cells [ 30 , 38 ]  . 
our approach was twofold , first , to use lcls derived from b - cells , and second , to separate mononuclear cells by density gradient centrifugation followed by isolation of the cd3 + cells by magnetic beads . 
consequently , cd3 antibodies identify all cells detected by cd4 and cd8 antibodies . other parameters that may influence apoptosis include culture conditions and cell concentration in the medium after irradiation . 
the culturing of whole blood [ 22 ] or all mononuclear cells [ 1 ] together and using flow cytometry methods by labeling the cells may have an advantage over the cell separation and culturing relatively small numbers of cells of a homogeneous subpopulation . 
according to our experience , culturing cells in conical tubes with a high cell density and sufficient nutrients can achieve a stress - free [ 27 ] cultivation of the isolated cd3 + cells . it is important for a radiosensitivity assay to have a high level of reproducibility and validity . 
three groups of patients which suffered from grade 1 ( + ) , 2 ( ( cid : 1 ) ) and 3 ( ( cid : 2 ) ) toxicity after radiotherapy were graphed . 
another group were patients with grade 3 toxicity which were previously identified by cytogenetic analysis to have a cellular elevated sensitivity ( ( cid : 3 ) , crs )  . 
eine weitere gruppe von patienten mit grad - 3 - nebenwirkungen war zuvor durch zytogenetische untersuchung getestet und als zellulr strahlenempfindlich gewertet worden ( ( cid : 3 ) , crs )  . 
 validity of a test system is much more difficult to estimate , since it is difficult to determine whether a clinically detected severe side effect is due to factors related to the treatment itself or whether it is based on a genetic disorder leading to cellular radiation hypersensitivity . 
one important indicator for the validity of our apoptosis test system is that we found a decrease in inducible apoptosis with age which has previously been observed by other investigators [ 7 ]  . 
there was a decrease in apoptosis varying from 0.15% year1 for cd8 + and 0.3% year1 for cd4 + at 2 gy to 0.43% year1 for cd8 + and 0.65% year1 for cd4 + at 9 gy [ 8 ]  . 
we have found a decreased apoptotic rate of 0.15% year1 ( cd3 + ) , which corresponds exactly to the apoptotic rate after 2 gy in cd8 + cells reported by crompton et al . 
additionally , our apoptotic rate of 13% for cd3 + cells from 50 - year - old individuals correlated quite well with that of the cd4 + and cd8 + cells at 2 gy where apoptotic rates of 10% ( cd4 ) and 18% ( cd8 ) were reported [ 8 ]  . 
in a previous study , cellular radiosensitivity of the at cell lines used in this study was evaluated by three - color fish , a more demanding method , indicating radiosensitivity with a high sensitivity [ 18 , 23 , 24 ]  . 
both cell lines had the mutation 657del5 in exon 6 in both alleles of the nbs1 gene leading to formation of a truncated version of the protein nibrit is the typical founder mutation in nbs [ 35 ]  . 
in contrast to our findings , another study investigating cd4 + / cd8 + cells derived from an nbs - homozygous patient found a reduced apoptotic rate when compared to the average control cell rate [ 7 ]  . five cell lines from patients with severe treatment - related side effects were identified to have increased cellular radiosensitivity as determined by the fish assay , but only two of these had a distinctly lower apoptotic rate . 
nevertheless , there are sensitive cell lines , which cannot be identified by this approach . increased radiosensitivity is an event , which can be caused by mutation in different genes . 
 cellular radiosensitivity and severity of the at disease [ 32 ] are dependent on different locations and types of mutations [ 23 ] and cancer predisposition [ 32 ] may result . 
mutations in the mre11 gene leads to abrogation of mre11 - rad50 - nbs1 radiation - induced foci [ 33 ] and a mutation in ligase iv disrupts the ligase iv domain or the interaction of the ligase iv and xrcc4 [ 25 , 28 ]  . 
there are > 130 other repair proteins [ 39 ] and many more proteins in the entire dna - damage response system which include cell - cycle control and tumor suppressor proteins . 
it can be speculated , that if hypersensitivity is caused by mild mutations in the dna - damage response system , only a subgroup will have reduced apoptotic rates depending on the involvement in the apoptosis - inducing pathways . conclusion these data indicate that measurement of radiation - induced apoptosis is not suitable to detect individual radiosensitivity . 
therefore , it is necessary to combine more than one method for the detection of individual radiosensitivity including assessments of remaining dna double - strand breaks , apoptosis , cell - cycle control and measurement of chromosomal aberrations . 
 acknowledgments we thank renate sieber for excellent technical assistance , susann neubauer for providing her data on chromosomal aberrations by fish and helpful discussion , and professor helga schuessler for valuable discussions . 
apoptosis and individual radiosensitivity strahlentherapie strahlentherapie und onkologie und onkologie technical note radiosurgery of small skull - base lesions no advantage for intensity - modulated stereotactic radiosurgery versus conformal arc technique antje ernst - stecken1 , ulrike lambrecht1 , 2 , oliver ganslandt3 , reinhold mueller1 , 2 , rudolf fahlbusch3 , rolf sauer1 , gerhard grabenbauer1 background and purpose : intensity - modulated stereotactic radiotherapy ( imsrt ) has shown the ability to conform the dose to concavities and to better avoid critical organs for large tumors . 
given the availability of an electronically driven micro - multileaf collimator , both intensity - modulated stereotactic radiosurgery ( imsrs ) and dynamic conformal arc ( dca ) technique ( dca ) can be performed at the novalis shaped beam surgery center , university of erlangen - nuremberg , germany , since 12 / 2002 . 
this study evaluates both techniques in small skull - base tumors treated with radiosurgery . material and methods : between 12 / 2002 and 04 / 2004 , a total of 109 radiosurgical procedures were performed in 77 patients , equally distributed between patients with acoustic neuroma ( an ) , pituitary adenoma ( pa ) and meningeoma ( m )  . 
six index patients ( n = 2 an , n = 1 pa , n = 3 m ) routinely planned for dynamic arc stereotactic radiosurgery were replanned using the imsrs approach ( brainscan , brainlab , heimstetten , germany )  . 
the rtog radiosurgery quality assurance guidelines , isodose volumes , doses to organs at risk ( oar ) , and dose delivery criteria were compared . results : dca was superior to imsrs for homogeneity and coverage . 
imsrs could keep the high - dose - irradiated volumes ( 90% isodose volume ) lower than dca in the pa and an with very small volumes , but all other lower dose volumes were larger for imsrs . 
the integral absorbed dose to the brain was much higher in the imsrs than in the dca approach ( factor 23 )  . conclusion : rtog radiosurgery guidelines were best met by the dca rather than imsrs approach for the treatment of small skull - base lesions . 
the imsrs approach will increase the time for planning , dose delivery and integral dose to the brathus , imsrt techniques are recommended for fractionated stereotactic radiotherapy to larger volumes rather than for radiosurgery in small skull - base lesions . key words : stereotactic radiosurgery micro - multileaf collimator dynamic conformal arc technique intensity - modulated radiosurgery small skull - base tumors strahlenther onkol 2005 ; 181 : 33644 doi 10.1007 / s00066 - 005 - 1371 - 1 radiochirurgie kleiner schdelbasistumoren . 
kein vorteil der intensittsmodulierten radiochirurgie gegenber der dynamic - conformal - arc - technik hintergrund und ziel : die intensittsmodulierte stereotaktische radiotherapie ( imsrt ) kann an konkave zielvolumina angepasste dosisverteilungen kreieren . 
 material und methodik : seit 12 / 2002 wurden im novalis shaped beam surgery center der universitt erlangen 109 zielvolumina bei 77 patienten radiochirurgisch behandelt , davon gleich viele patienten mit akustikusneurinomen ( an ) , hypophysenadenomen ( pa ) und meningeomen ( m )  . 
sechs fr dca - technik geplante patienten ( n = 2 an , n = 1 pa , n = 3 m ) wurden mit imsrs neu geplant und hinsichtlich der rtog - qualittsindizes und dosisvolumina ausgewertet . 
die geschtzte 1 department of radiation therapy and novalis shaped beam surgery center , university of erlangen - nuremberg , erlangen , germany , 2 division of medical physics , department of radiation therapy , university of erlangen - nuremberg , erlangen , germany , 3 department of neurosurgery , university of erlangen - nuremberg , erlangen , germany . received : september 28 , 2004 ; accepted : february 2 , 2005 strahlenther onkol 2005 no . 
imsrs versus dca in small skull - base lesions behandlungszeit ( anzahl bestrahlungsfelder , intensittsstufen ) war fr die imsrs wesentlich lnger , mit einer weitaus greren zur dosisverabreichung erforderlichen anzahl an monitoreinheiten ( jeweils um den faktor 23 hher )  . 
die zeiten fr die planung und verabreichung der dosis sind fr dca krzer , die integrale ganzhirndosis und die bestrahlungsvolumina fr die mittleren und niedrigen dosen sind geringer als bei der imsrs . 
 schlsselwrter : stereotaktische radiochirurgie mikromultileafkollimator dynamic - conformal - arc - technik intensittsmodulierte radiochirurgie kleine schdelbasistumoren introduction in radiotherapy , the most important limiting factor is normal - tissue radiation tolerance . 
 intensity - modulated stereotactic radiotherapy ( imsrt ) has shown to have the ability to conform the dose to concavities and to better avoid critical organs , however , most studies have been performed in larger tumors [ 1 , 33 , 34 , 39 , 40 , 45 , 51 , 53 , 57 ]  . 
since 2002 , the university of erlangen has been using a dedicated linac - based system for srs , the novalis system ( brainlab ag , heimstetten , germany )  . 
 material and methods patients from 12 / 2002 to 04 / 2004 , a total of 109 radiosurgery procedures were performed in 77 patients at the novalis shaped beam surgery center of the university hospital of erlangen - nuremberg , germany . 
among these patients with acoustic neuroma ( an ) , pituitary adenoma ( pa ) and meningeoma ( m ) , six index patients with small tumors located near the base of skull were selected for replanning with the imsrs approach ( brainscan , brainlab )  . 
shortly thereafter , helical ct images of 1 mm slice thickness ( somatom vz , siemens , erlangen , germany ) were obtained with the localizer box attached to the frame and these were fused with the previously generated thin - slice ( 0.81.0 mm ) mr images ( magnetom expert , siemens ) by the automatic image fusion system software . 
 dose calculation dose calculation for dca and imsrs was done by pencil - beam algorithhere , inhomogeneities are taken into account by attenuating the primary photon fluence exponentially utilizing the average total linear attenuation coefficient of intervening tissue , by multiplying photon fluence by linear attenuation coefficient to yield the number of collisions in the scattering volume , and by scaling the path between the scattering volume element and the computation point by an effective tissue . 
the algorithm is characterized by a fast and accurate dose calculation for large and irregular fields and for intensity - modulated radiotherapy ( imrt ) , although secondary dose distribution will not be density - corrected and large cavities can still give errors [ 33 ]  . 
 quality criteria and evaluation according to the rtog guidelines , dose homogeneity within the target volume is defined by the ratio between maximum dose and prescription dose ( md / pd ratio ) [ 46 ]  . 
the conformation of the prescription dose to the target is defined by the ratio of the prescription isodose surface volume to the target volume ( piv / tv ratio )  . 
the dose gradient achieved outside the target defined as the ratio of the target volume to the volume encompassed by the 90% isodose volume ( tv / v90 ) is of further use and usually referred to as coverage . we compared dca technique and imsrs for six irregularly shaped skull - base targets for the endpoints homogeneity , conformity , coverage , dose to nontargeted brain and oar . 
 results conformity and coverage conformity was better for the pa and the an1 using intensity - modulated therapy and superior using dynamic arcs for the an2 and all skull - base meningeomas ( table 2 )  . 
for the volumes > 2 cm3 , imsrs would create equal or even better coverage . isodose volumes normal - brain sparing was better for imsrs only for the high - dose 90% volume and only for the pa and the an1 . 
 field setup , treatment time , and monitor units the number of arcs and step - and - shoot static imsrs fields were significantly different taking the number of intensity steps in imsrs into account . 
imsrs versus dca in small skull - base lesions reevaluation after improvement of imsrs coverage to achieve better coverage in the smaller volumes , the imsrs plans were again modified by different weighting of fields ( table 6 )  . 
the maximum doses , which were lower for imsrs for the pa , the same for the an1 and higher for the m1 than for dca technique before modification of coverage , increased . 
the 90% isodose volumes changed from 80% , 68% , and 113% for imsrs compared to dca technique to 182% , 177% , and 212% for the pa , an1 , and m1 , respectively . 
in the case of circular collimators , as in gamma - knife treatment , multiple isocenters and a varying collimation of the circular beams can give good conformation to irregular targets with inhomogeneous dose distribution within the target [ 38 , 57 ]  . 
overlapping shots create a high internal dose gradient resulting in a potential damage to oar within the target volume such as the cranial nerves v , vii , and viii in vestibular schwannoma treatment [ 41 ]  . 
during this progress each new planning and delivery advice was compared with the formerly best established one in terms of the rtog quality criteria that are acceptable in current radiotherapy practice . 
table 7 shows an excerpt of these studies , chronologically following this evolution toward more sophisticated approaches in performing srs : the first studies concerning field shaping in linac radiosurgery have shown static conformal fields to be superior to arc treatment with circular collimator techniques in terms of conformity [ 57 ]  . 
 for stereotactically guided conformal radiotherapy to volumes > 13 cm3 , four to six noncoplanar fixed fields are clearly superior to coplanar field arrangements , while even techniques approaching dynamic conformal radiotherapy like a 30 - field approach reveal no further sparing of normal brain irradiated [ 39 ]  . 
 tumor pituitary adenoma acoustic neuroma 1 skull - base meningeoma 1 acoustic neuroma 2 skull - base meningeoma 2 skull - base meningeoma 3 dca 2 , 925 2 , 059 2 , 178 2 , 113 2 , 287 1 , 925 monitor units imsrs imsrsi 5 , 705 4 , 655 4 , 026 4 , 931 4 , 979 6 , 425 5 , 998 5 , 323 4 , 734 arcs dca fields imsrs strahlenther onkol 2005 no . 
 variables that were associated with a significantly higher complication rate after radiosurgery are tumor dose inhomogeneity , number of isocenters and maximum normal tissue dose , with tumor dose inhomogeneity being the most importable 6 . 
the more recent publications could show an advantage for imrt over stereotactic conformal radiotherapy in terms of ptv coverage for irregular and concave targets by creating lower doses to oar at the same time [ 1 ]  . 
our results identified the advantage for dca technique over imsrs in very small targets , while imsrt seems to play the major role in the fractionated treatment of irregularly shaped and large lesions in the bra our close comparison of the dca technique with imsrs , planned within the dose constraints given by the physician , highlights that the coverage of the ptv is better for the dca technique . 
an : acoustic neuroma ; ci : conformity index ; dca : dynamic conformal arc ; hi : homogeneity index ; imsrs : intensity - modulated stereotactic radiosurgery ; imsrt : intensity - modulated stereotactic radiotherapy ; na : not available ; oar : organ at risk . 
an : akustikusneurinom ; ci : konformittsindex ; dca : dynamic - conformal - arc - technik ; hi : homogenittsindex ; imsrs : intensittsmodulierte stereotaktische radiochirurgie ; imsrt : intensittsmodulierte stereotaktische radiotherapie ; na : nicht verfgbar ; oar : risikoorgan . 
 author ( year ) evaluation of methods patients ( n ) ptv ( cm3 ) results 1 2 1 3 bourland & mccollough [ 6 ] ( 1994 ) noncoplanar circular arc hamilton et al . 
in all of our computed plans , imsrs generated much higher volumes of normal tissue irradiated with low doses , conformity was worse than with the dca approach , especially in the plans generated with higher coverage for imsrs . a large percentage of patients treated with radiosurgery presents with benign tumors or functional disorders . 
although photon therapy can be superior to neurosurgery with regard to preservation of cranial nerve function [ 15 , 16 , 55 ] , general risks resulting from anesthesia and requirement of inpatient hospital time , at the same time , some risk of cancer induction is generally accepted . 
for lower minimum target dose for imrt in all cases , by the significantly higher number of monitor units needed for imrt dose delivery , a larger integral dose to the brain will be delivered ( table 4 )  . 
this can easily be visualized by the isodose lines shown as an example for the an1 , where in contrast to the dca plan the 20% isodose is not conformal to the ptv in imsrs ( figure 3 )  . 
consequently , the dca approach seems to be safer in terms of cancer induction , although this depends on a number of assumptions and data comparing the two techniques for this question are not available [ 3 ]  . 
in our institution , for fractionated imrt , we have been using radiographic films , permitting measurements of the dose in a matrix of points [ 7 , 30 ]  . 
 the steep dose gradient is registered on a radiographic film first for the whole plan with all fields in the coronal plane of the imrt phantom and afterwards for each single field . 
the distribution of the optical density in the film has to be correlated with the calculated distribution by using the software omnipro imrt ( scanditronix medical ab , uppsala , sweden , 2003 )  . 
the whole procedure usually takes at least several hours and it is easily understood that for radiosurgery , that is planned and delivered on a single day , imrt verification using radiographic films does not seem to represent an appropriate means . 
on the other hand , conformal arc treatment has been tested by dosimetric , mechanical and geometric verification with an ionization chamber in phantom studies and radiographic films to be accurate [ 12 , 32 , 44 ]  . conclusion for very small skull - base lesions up to 2.0 cm3 , dca radiosurgery field shaping allows to fulfill the rtog quality guidelines with a better coverage for the ptv , superior homogeneity , and lower maximum doses to oar than imsrs . 
thus , we recommend imsrt techniques for fractionated stereotactic radiotherapy to larger volumes rather than for radiosurgery . strahlentherapie strahlentherapie und onkologie und onkologie original article original article esthesioneuroblastoma in childhood and adolescence better prognosis with multimodal treatment ? * * * hans theodor eich1 , rolf - peter mller1 , oliver micke2 , martin kocher1 , frank berthold3 , barbara hero3 background and purpose : only 3% of all malignant intranasal tumors are esthesioneuroblastomas ( enb ) and only 20% of these rare neuroectodermal tumors are diagnosed up to 20 years of age . 
17 patients underwent surgery , either without further therapy ( n = 4 ) , followed by radiotherapy ( n = 1 ) or as part of multimodal regimens ( n = 12 )  . 
 results : the 5 - year overall survival ( os ) for the whole group was 73% 12% and the 5 - year event - free survival ( efs ) 55% 13% . 
none of the four patients with stage b experienced tumor progression so far , whereas seven out of 15 patients with stage c did ( 5 - year efs 47% 14% ; not significant )  . 
 key words : pediatric esthesioneuroblastoma olfactory neuroblastoma radiotherapy multimodality therapy chemotherapy strahlenther onkol 2005 ; 181 : 37884 doi 10.1007 / s00066 - 005 - 1362 - 2 sthesioneuroblastom im kindesund jugendalter . 
verbesserte prognose durch multimodale behandlungsanstze ? hintergrund und ziel : das sthesioneuroblastom macht lediglich 3% aller intranasalen tumoren aus , und nur 20% dieser seltenen neuroektodermalen tumoren werden bei patienten 20 jahre diagnostiziert . 
17 patienten waren operiert worden , entweder ohne weitere therapie ( n = 4 ) , gefolgt von einer radiotherapie ( n = 1 ) oder im rahmen multimodaler therapieanstze ( n = 12 ; tabelle 3 )  . 
bei allen fnf patienten , die eine neoadjuvante chemotherapie infolge inoperabler primrtumoren erhalten hatten , konnte eine r0 - resektion erreicht werden . * oral presentation at the 10th annual meeting of the german society for therapeutic radiology and oncology ( degro ) , erfurt , june 1013 , 2004 . * * the following participating german institutions recruited patients in this retrospective study : klinikum augsburg , universittsklinikum dsseldorf , universittsklinikum erlangen , universittsklinikum frankfurt , universittsklinikum freiburg , universittsklinikum gieen , universittsklinikum hamburg , universittsklinikum mnster , klinikum hannover nordstadt , klinikum oldenburg , katharinenhospital stuttgart , olgaspital stuttgart , universittsklinikum tbingen , universittsklinikum ulm , universittsklinikum wrzburg . 1 department of radiation oncology , university of cologne , cologne , germany , 2 department of radiation oncology , university of mnster , mnster , germany , 3 department of pediatric oncology , childrens hospital , university of cologne , cologne , germany . received : september 8 , 2004 ; accepted : march 15 , 2005 strahlenther onkol 2005 no . 
esthesioneuroblastoma in children results : das 5 - jahres - gesamtberleben ( os ) aller patienten betrug 73% 12% , das ereignisfreie 5 - jahres - berleben ( efs ) 55% 13% ( abbildung 2 )  . 
keiner der vier patienten im stadium b entwickelte eine tumorprogression , wohingegen es bei sieben von 15 patienten im stadium c zu einer tumorprogression kam ( 5 - jahres - efs 47% 14% ; nicht signifikant ; abbildung 3 )  . 
 schlsselwrter : kindliches sthesioneuroblastom olfaktoriusneuroblastom radiotherapie multimodale therapie chemotherapie introduction esthesioneuroblastoma ( enb ) is a rare and uncommon neuroectodermal tumor arising from the olfactory epithelium in the upper nasal cavity and often shows an intracranial extension [ 5 ]  . 
 since the first description of enb by berger & luc [ 1 ] in 1924 , about 1 , 000 cases have been reported in the world literature [ 5 ]  . 
reported that only 20% of all enb are diagnosed up to 20 years of age [ 4 ]  . as in all intranasal tumors , initial symptoms are mostly nonspecific and include nasal obstruction , epistaxis , cephalgia , hyposmia , exophthalmos , and amaurosis in correlation to the tumor extension . since pediatric enbs are rare , the number of children and adolescents treated in individual departments is very small . 
chemotherapy has been reported mainly for recurrent or metastatic disease [ 1012 , 25 , 26 , 30 ]  . the present analysis of 19 children and adolescents with enb was performed to evaluate the efficacy of radiotherapy and chemotherapy especially in a multimodal treatment approach in this age group . 
especially the positive reaction for s - 100 protein and the presence of neuron - specific enolase ( nse ) in combination with a negative stain for epithelial and lymphoma marker suggest its classification as a neurogenic tumor [ 15 , 32 ]  . patients were staged according to the kadish system ( table 1 ) which is predominantly used in literature , although multiple modifications have been proposed [ 3 , 5 , 9 , 16 ]  . 
for reasons of comparability we have chosen the original syste radiotherapy was performed with linear accelerators mostly in three - field technique : an anterior field combined with wedged lateral fields . 
when computed tomography treatment planning was available , the target volume ( ptv ) encompassed the primary tumor site and varied upon the tumor extension including a safety margin of 12 cthe ptv had to be covtable 1 . 
 patients and methods type extension this study comprises a retrospective multicenter review of 19 children and young adolescents ( 20 years ) with enb treated from january 1979 to august 2001 . 
a questionnaire including data of the patients characteristics , initial presenting symptumor limited to the nasal cavity tumor infiltrating the nasal and paranasal cavities tumor extending beyond the nasal and paranasal cavities strahlenther onkol 2005 no . 
 statistical analysis treatment response was assessed by clinical examinations and since 1985 by computed tomography or magnetic resonance imaging and classified as complete response , partial response , stable disease , and progressive disease according to common rules . 
kaplan - meier estimates for overall survival ( os ) and event - free survival ( efs ) were calculated and compared by the log - rank test [ 17 ]  . 
12 / 15 patients with stage c tumors showed orbital infiltration , 10 / 15 patients cranial base and 5 / 15 patients brain infiltration ( figure 1 )  . 
 17 patients underwent surgery , either without further therapy ( n = 4 ) , followed by radiotherapy ( n = 1 ) or as part of multimodal regimens ( n = 12 )  . 
initiale symptome bei 19 kindern und jugendlichen mit sthesioneuroblasto symptoms patients ( n ) treatment nasal obstruction , rhinitis epistaxis exophthalmos visual dysfunction / diplopia headache , facial pain tumor mass nausea , vomiting loss of sense of smell mental change eich ht , et al . 
chemotherapeutika bei 14 kindern und jugendlichen mit sthesioneuroblasto chemotherapy patients ( n ) vincristine / vindesine ifosfamide / cyclophosphamide doxorubicin etoposide / teniposide cisplatinum / carboplatin actinomycin d dacarbazine methotrexate , intrathecal complete resection ( r0 ) was achieved in 15 out of 17 patients with surgery including all five patients with preoperative chemotherapy due to unresectable primary at diagnosis . 
 as there were no common treatment recommendations for enb during this 21 - year time span , chemotherapeutic agents were used in various combinations , mostly based on trials for childhood neuroblastoma or soft - tissue sarcoma . 
 table 4 gives an overview on the applied agents . treatment to the neck in two patients , who had palpable nodes at presentation , consisted of therapeutic lymph node dissection and postoperative radiotherapy in one patient , and neoadjuvant chemotherapy followed by therapeutic lymph node dissection and postoperative radiotherapy in the other . 
none of the four patients with stage b experienced tumor progression so far , whereas seven out of 15 patients with stage c did ( 5 - year efs 47% 14% , n.s. ) ; four of those died ( figure 3 )  . 
efs bei multimodaler therapie ( n = 10 ) 65% 17% versus keine multimodale therapie ( n = 5 ) 20% 18% , letzte berechnung ; p = 0 , 02 . 
it may be interesting that these cats did not show any other evidence of neoplasms or leukemia [ 29 ]  . the following findings emerge from this analysis : first , enb is a very rare intranasal tumor , but can also be found in childhood and adolescence . 
four patients were excluded from the presented study , since reference pathology showed a rhabdomyosarcoma ( n = 2 ) , a primitive neuroectodermal tumor ( pnet , n = 1 ) , and a malignant mesenchymal tumor ( n = 1 )  . 
third , the presented data indicate a stage - adapted therapy and especially a benefit of multimodal treatment regimens combining surgery , chemotherapy and radiotherapy for pediatric patients with enb kadish stage c . the first report about a child with enb was published in an 11 - year - old patient in 1929 and a 14 - year - old patient in 1959 in the us literature [ 31 ]  . 
approximately 90100 children and adolescents ( 20 years ) have been described with this tumor in the literature , making it an extremely rare pediatric entity [ 23 ]  . 
 the wide variety of treatment approaches in the current analysis , which is due to the multiinstitutional collection of enb patients , reflects the absence of commonly accepted therapeutic recommendations . 
a meta - analysis of the literature published between 1990 and 2000 [ 8 ] reports an os and a 5 - year disease - free survival of 45% ( standard deviation [ sd ] = 22 ) and 41% ( sd = 29 ) , respectively , in 390 patients including all ages . 
survival according to treatment modalities was as follows : 65% for surgery plus radiotherapy ; 51% for radiotherapy and chemotherapy ; 48% for surgery ; 47% for surgery , radiotherapy , and chemotherapy ; and 37% for radiotherapy alone . 
chemotherapy for enb was initially reserved for patients with relapses , metastatic or inoperable disease and occasionally used in the adjuvant setting [ 4 , 5 , 23 ]  . 
neoadjuvant chemotherapy was reported in one patient only . the agents most frequently used are cisplatin , etoposide , adriamycin , cyclophosphamide , vincristine , 5 - fluorouracil , doxorubicin , and thiotepa . 
in individual cases there are data about the successful use of neoadjuvant chemotherapy followed by surgery and / or radiotherapy in patients with stage c disease [ 11 , 13 , 23 ]  . 
 reported results in 16 adult patients with stage a or b and 24 with stage c disease treated with radiotherapy ( median dose 50 gy ) and surgery for stage a and b disease , with addition of chemotherapy ( cyclophosphamide and vincristine ) for stage c disease [ 10 ]  . 
vorschlag zur stadienadaptierten therapie von kindern und jugendlichen mit sthesioneuroblasto kadish stage treatment modalities surgery only surgery ( cid : 1 ) radiotherapy ( 5060 gy ) resectable unresectable surgery ( cid : 1 ) chemotherapy ( 2 cycles ) ( cid : 1 ) radiotherapy ( cid : 1 ) chemotherapy ( 2 cycles ) chemotherapy ( 4 cycles ) ( cid : 1 ) surgery ( cid : 1 ) radiotherapy chemotherapy plus surgery plus radiotherapy . 
although primary tumor response to chemotherapy did not result in significant survival advantage in patients treated with multimodality regimen , the disease - free interval was significantly better than in those patients who did not receive chemotherapy prior to surgery . 
for kadish stage c patients with multimodality therapy efs was significantly improved compared to the other treatment groups , although three patients developed local recurrences and two of them died . 
whether the use of new radiation treatment techniques with the option of local dose escalation and the use of intensity - modulated radiotherapy ( imrt ) can lead to an improvement of local control remains to be proven [ 7 , 35 ]  . the presented retrospective analysis and the review of the literature support a stage - adapted therapy of enb in children and adolescents ( table 5 ) : in our series no patient with kadish stage a tumor was included . 
careful radiation treatment planning is necessary to avoid extensive acute and late toxicity in the regions of nose , orbitae , and the frontal brafor kadish stage c tumors we recommend a multimodal approach : if these tumors are judged to be completely surgically resectable , initial surgery should be performed followed by two cycles of polychemotherapy , radiotherapy , and further two cycles of polychemotherapy . 
currently , we are recommending alternating chemotherapy cycles of the neuroblastoma protocol ( n5 : cisplatinum , etoposide , vindesine ; n6 : ifosfamide , doxorubicine , darcabazine , vincristine ; for details see [ 2 ] )  . 
 strahlentherapie und onkologie original article three - times - daily radiotherapy with induction chemotherapy in locally advanced non - small cell lung cancer feasibility and toxicity study gianpiero catalano1 , barbara alicija jereczek - fossa1 , tommaso de pas1 , maria elena leon3 , frederica cattani4 , lorenzo spaggiari5 , giulia veronesi5 , filippo de braud2 , roberto orecchia1 , 6 purpose : to evaluate the feasibility and toxicity of three - times - daily radiotherapy ( 3tdrt ) , preceded by induction chemotherapy ( ict ) , in stage iiiaiiib non - small cell lung cancer ( nsclc )  . patients and methods : ict consisted of three cycles of cisplatin and gemcitabine . 
toxicity was limited to rtog grade 2 ( 25 patients , 67.6% ) and grade 3 ( four patients , 10.8% ) acute esophagitis ; no grade 3 late esophagitis occurred . 
 the limited statistical power does not permit a definition of predictors for radiation - induced esophagitis incidence and severity ; additional studies are required to clarify the impact of volumetric and dosimetric parameters . 
failure patterns and survival results are warranted to confirm the efficacy of this approach in locally advanced nsclc . key words : lung cancer hyperfractionated radiotherapy three - times - daily radiotherapy induction chemotherapy acute toxicity esophagitis strahlenther onkol 2005 ; 181 : 36371 doi 10.1007 / s00066 - 005 - 1332 - 8 dreimal tgliche strahlentherapie mit induktionschemotherapie bei lokal fortgeschrittenem nichtkleinzelligen bronchialkarzinomachbarkeitsund toxizittsstudie ziel : untersuchung der durchfhrbarkeit und toxizitt einer dreimal tglichen strahlentherapie ( 3tdrt ) nach induktionschemotherapie ( ict ) bei nichtkleinzelligem bronchialkarzinom ( nsclc ) im stadium iiiaiiib . patienten und methodik : die ict umfasste drei zyklen cisplatin und gemcitabbei patienten , die auf die ict ansprachen , wurde eine operative therapie erwogen . 
64 , 6 gy in drei fraktionen pro tag verabreicht . ergebnisse : zwischen februar 1998 und oktober 2000 erhielten 37 patienten eine radikale ( n = 18 ) oder postoperative 3tdrt ( n = 19 )  . 
die toxizitt beschrnkte sich auf eine akute sophagitis rtog - grad 2 ( 25 patienten , 67 , 6% ) und 3 ( vier patienten , 10 , 8% ) ; eine spte sophagitis grad 3 wurde nicht beobachtet . 
feasibility of three - times - daily radiotherapy in lung cancer schlussfolgerung : in dieser studie zur 3tdrt nach ict erwies sich die kombinationstherapie aufgrund ihrer geringen toxizitt als geeignet . 
die eingeschrnkte statistische aussagekraft lsst keine bestimmung prdiktiver faktoren fr hufigkeit und schwere einer strahlenbedingten sophagitis zu ; weitere studien sind erforderlich , um den einfluss von volumenund dosisparametern zu klren . 
analysen von rezidivierungsverhalten und berleben knnten die wirksamkeit dieses verfahrens bei lokal fortgeschrittenem nsclc besttigen . schlsselwrter : lungenkarzinom hyperfraktionierte strahlentherapie dreimal tgliche strahlentherapie induktionschemotherapie akuttoxizitt sophagitis introduction there is no consensus on what is the most appropriate treatment of locally advanced non - small cell lung cancer ( nsclc )  . 
 actual strategies are directed toward the reduction of metastatic disease by adding chemotherapy ( ct ) to local treatments and the improvement of local control through more aggressive radiotherapy ( rt ) , since it is well known that a direct dose - survival relationship exists [ 3 , 14 ]  . 
recent studies revealed a significant survival improvement when adding a systemic treatment , such as induction chemotherapy ( ict ) , to rt [ 2 , 11 , 12 , 18 , 21 , 25 , 26 , 31 , 32 ]  . 
unconventional rt showed to be more effective than conventional treatment in improving local control and overall survival , as reported in phase iiiii studies [ 7 , 16 , 17 , 21 ] ; dose escalation trials have also been performed , confirming a dose - effect relationship for locally advanced nsclc , with a significant survival advantage in selected patients [ 8 ]  . 
 a major randomized trial investigated a more aggressive schedule of continuous hyperfractionated accelerated radiotherapy ( chart ) , given as definitive treatment by means of three daily fractions of 1.5 gy up to a total dose of 54 gy . 
 to our knowledge , few data are available in the literature on the association of ict followed by hyperfractionated accelerated rt and specifically , on the integration of ict and three - times - daily rt ( 3tdrt )  . 
during ict , complete blood cell count and renal function assessments were performed weekly . treatment cisplatin ( cddp ) 80 mg / m2 as 1 - h intravenous infusion on day 1 and gemcitabine ( gcb ) 1 , 250 mg / m2 administered as a 30 - min infusion on days 1 and 8 , repeated every 3 weeks , were planned . 
for stage iiib patients or stage iiia not suitable for surgery , definitive rt was planned 46 weeks after the completion of ict . patients were considered eligible for surgery with acceptable risk , if postoperative predictive fev1 ( forced expiratory volume in 1 s ) at spirometry was > 33% of the theoretical value ( based on weight , height , and sex )  . 
the rules used to evaluate this parameter were the following : ( cid : 127 ) for lobectomy , predictive postoperative fev1 was equal to preoperative fev1 1 ( 0.053 number of resected segments ) , where 0.053 is 1 / 19 ; strahlenther onkol 2005 no . 
feasibility of three - times - daily radiotherapy in lung cancer ( cid : 127 ) for pneumonectomy , predictive postoperative fev1 was equal to ( preoperative fev1 percentage of perfusion of the healthy lung ) / 100 . 
in both cases , total doses were delivered in three daily fractions of 1.2 gy , 1 gy and 1.2 gy , 5 days a week , with an interfraction interval of at least 4 h . 
conscious that a 4 - h interval may not be as safe as a longer one to guarantee a partial recovery from radiation sublethal damage , especially for cord tolerance , a concomitant - boost technique was used for delivery of the planned dose . 
this volume consisted of pre - ct gross tumor disease , mediastinal - ipsilateral hilar lymph nodes ( with a safety margin of 2 cm ) , plus ipsilateral supraclavicular lymph nodes in case of upper lobe tumors . 
in the second daily fraction , a boost volume , limited to gross tumor volume ( plus a 1.5 - cm margin ) , was irradiated via isocentric multiportal fields , assessed depending on volume site and extension , up to the additional dose of 16 gy . 
with this approach in the second daily fraction the irradiation was delivered off - cord , thus reducing cord irradiation by means of a longer interval ( 8 h ) between the first and third fraction in which spinal cord was irradiated . 
 lungs , spinal cord and esophagus were defined as organs at risk ( oars ) ; in particular , lungs were automatically contoured by the treatment planning software , while spinal cord and esophagus were manually drawn , starting from the upper thoracic inlet to the diaphragm . all patients were treated in a supine position , with arms above head and - cradle immobilization devices with skin marks ensuring the reproducibility of treatment . 
in vivo dosimetry and electronic portal verification were also performed , ensuring the requested quality assurance program . dose - volume histograms ( dvhs ) completed the assessment of treatment , comparing different plans . 
since the absolute dose differed in relation to the aim of treatment , dvhs were expressed in terms of percent of total dose , allowing comparison of definitive and postoperative 3tdrt . 
furthermore , since treatment technique for the first 38.4 gy was standard , ap - pa dvhs were referred to the first phase , boost dvhs were referred to the latter part of treatment , and dvh calculations were made separately . 
the percentages of either the target or oar volumes exposed to a dose 100% , 95% , 80% , and 50% of the prescribed dose were recorded for ap - pa and boost dvhs , respectively . 
 follow - up first follow - up started 4 weeks after rt with clinical and radiologic evaluation of medical conditions , toxicity and disease status every 4 months , for the first 2 years , and subsequently every 6 months . 
after treatment patients were also instructed to refer to the physician in case of any symptom , if occurring before the scheduled follow - up control . rt acute toxicity ( from the beginning up to 3 months after 3tdrt ) was evaluated according to the rtog ( radiation therapy oncology group ) scoring system ; similarly , late toxicity ( > 3 months after 3tdrt ) was scored according to the rtog / eortc ( european organization for research and treatment of cancer ) system . statistical analysis in order to identify factors possibly associated with esophagitis , patients were grouped according to two different toxicity classifications : grades 0 / 1 versus 2 / 3 , and grades 0 / 1 , 2 and 3 separately . 
mean percentage of irradiated esophageal volume , as derived from dvh calculation , was compared to the toxicity level developed for each percentage of intended dose separately , using simple linear regression . 
surgery was performed in 28 / 39 stage iiia patients , with 25 radical resections and no perioperative mortality ; in eleven iiia patients surgery was not performed because of pd ( five patients ) , extension of disease ( three patients ) , or strahlenther onkol 2005 no . 
 patients enrolled completed not completed response to ict partial stable disease progressive disease surgery ( only stage iiia ) performed not performed radical surgery 3tdrt performed not performed 3tdrt purpose definitive postoperative iiib total 5 ( toxicity 3 ; pd 1 ; unknown 1 ) ( toxicity ) iiia 6 6 2 ( pd 5 ; disease extension 3 ; respiratory condition 3 ) ( after surgery 20 ; without surgery 5 ) ( after surgery 8 ; without surgery 6 ) 6 ( pd after ict ) medical and functional respiratory limitations ( three patients )  . 
in 15 cases 3tdrt was not performed because of pd ( five patients with systemic pd after ict , two with systemic pd after surgery , two with locoregional pd after ict , one with locoregional pd at surgical exploration ) , protocol violation ( four patients ) , and postoperative complications ( one patient )  . 
 the majority of patients receiving 3tdrt were male ( 32 of 37 ) ; median age was 58 years ( range , 4075 years ) with a good performance status ( median karnofsky index of 90 )  . overall , patient compliance was satisfactory , and no 3tdrt delays due to treatment - related toxicity occurred . 
 severe esophagitis , with a weight loss > 15% or enteral / parenteral feeding ( grade 3 ) , occurred in four patients ( 10.8% ) ; in one case only 3tdrt was interrupted ( after 51 gy )  . 
even though endoscopic control was not considered a routine procedure during follow - up , it was performed in two patients , due to the long - lasting dysphagia after 3tdrt , and revealed a pattern of mucosal erythema without any sign of ulceration . 
no severe late toxicity occurred during follow - up . lung acute toxicity was confined , in the majority of irradiated patients , to mild symptoms of cough and dyspnea with minimal effort ( table 2 ) ; one episode of septic pneumonitis completely recovered after administration of antibiotics , occurred few days after the end of 3tdrt . 
feasibility of three - times - daily radiotherapy in lung cancer low - up , and 14 patients developed grade 12 lung toxicity , in the majority of cases characterized by radiologic signs of lung fibrosis without clinical symptoms . dvh calculation evidenced that the esophagus , due to its central position in the mediastinum , was heavily irradiated in the ap - pa fields , receiving a mean of > 95% of the prescribed dose to almost two thirds ( 61% ) of its volume . 
regarding lungs , preservation of the uninvolved lung was achieved ( 16% and 21% of volume irradiated to 50% of prescribed dose , in the two phases of treatment , respectively )  . 
the absolute dose to the spinal cord never exceeded 42 gy ( table 3 )  . there was no association between irradiated esophageal volume , as measured by means of dvhs , and the observed toxicity grade ( table 4 )  . 
particularly , no correlation was found between esophageal toxicity and gender , age , or performance status ; furthermore , no statistical significance emerged when considering disease - specific ( histology , lobe , number of involved mediastinal stations ) and treatment - related parameters , like ict grade 3 toxicity , ict dose reduction , 3tdrt dose , and ap - pa target volume . 
in the literature , severe esophagitis rate commonly ranges from 10% to > 40% and is mainly related to the applied radiation dose , rt fractionation , and concomitant ct administration . 
specifically , the incidence of severe acute esophageal toxicity results to be higher in case of unconventional fractionation schedules and / or concomitant chemoradiation [ 4 , 6 , 33 , 37 ]  . a retrospective analysis of 461 locally advanced nsclc patients revealed a significant increase of severe acute esophagitis rate in case of unconventional rt and concomitant ct up to 34% [ 4 ]  . 
similar conclusions have been reached in another report in which the overall grade 3 , or greater , dysphagia rate was 13% , with higher values occurring in case of chemotable 3 . 
ap - pa : anterior - posterior and posterior - anterior fields ; ict : induction chemotherapy ; ps : performance status ( karnofsky index ) ; 3tdrt : three - times - daily radiotherapy . 
ap - pa : anterior - posteriore und posterior - anteriore felder ; ict : induktionschemotherapie ; ps : performance - status ( karnofsky - index ) ; 3tdrt : dreimal tgliche strahlentherapie . 
at the same time , the possibility of radical surgery for iiia patients who experienced a response to ict was also considered , as recommended in a previous report [ 1 ]  . 
for a radical treatment , calculated biological effective dose ( bed ) for earlyand late - reacting tissues was 72 gy10 ( calculated assuming an / ratio of 10 ) and 89 gy3 ( / ratio of 3 ) , respectively , with a theoretical similar impact on tumor and acute toxicity of a conventional rt and a potential advantage in terms of late toxicity reduction . 
the inclusion of postoperative patients was performed to guarantee a better theoretical local treatment even on good - prognosis patients with subclinical disease only , even if we were conscious that such a decision could increase the heterogeneity of the population and reduce the statistical power of any conclusion . 
 concerning technical details of irradiation , a concomitant - boost approach was chosen , improving the spinal cord tolerance by means of an adequate interval between the larger treatment fields . 
 this approach is similar to another study of 3tdrt reported in the literature ( eastern cooperative oncology group , ecog 4593 ) in which 30 stage iiiab patients were treated with exclusive rt up to 57.6 gy , delivered in two daily fractions of 1.5 gy to a larger volume , and a concomitant boost of 1.8 gy in the central daily fraction . 
severe difficulty in swallowing and alimentation limited to fluids were only experienced by 19% of patients , while a soft diet was tolerated by 46% of patients and some discomfort was observed in 28% [ 28 ]  . 
nevertheless , the very low rate of severe esophagitis ( 10% grade 3 ) , the satisfactory compliance with the treatment schedule ( only one interruption of 3tdrt ) , and the absence of severe lung toxicity or late effects were surprising [ 38 ] and confirmed the feasibility of the regimen . 
 a comparison between our observation and previously reported experiences is somewhat difficult , due to differences in patient selection , study design , treatment characteristics , and the different criteria used to score toxicity . 
focusing on low - grade ( grade 12 ) toxicity levels , mild to moderate dysphagia occurred more often in our study than in the chart and ecog trials ( 86.5% , 74% , and 78% , respectively )  . 
this trend was , on the other hand , not confirmed for high - grade ( grade 3 ) toxicity where 3tdrt , compared to the other two studies , showed lower rates ( 10.8% , 19% , and 22% , respectively ) , as shown in table 6 . 
in this context , the impact of pretreatment dysphagia might be of particular importance , since this parameter is known to be predictive of severe esophagitis [ 23 ]  . 
feasibility of three - times - daily radiotherapy in lung cancer signs or symptoms of esophageal toxicity occurred before 3tdrt started ; unfortunately , except for the 40% pretreatment weight loss reported in ecog 4593 , no data concerning this point was mentioned regarding chart patients . 
 in the chart trial the population was very heterogeneous , with more than one third of patients ( 36% ) having stage iii disease ; furthermore , a strict restriction of irradiated areas was made , limiting the large - field area to 240 cm2 and the boost area to 140 cm2 . 
rt technique was , indeed , very similar overweighting the short interfraction interval , predictive of severe toxicity [ 34 ] , with a concomitant boost approach in which esophageal irradiation tended to be theoretically minimized . 
moreover , in both studies the patient population consisted of locally advanced disease cases , although in the ecog trial the aim of treatment was only curative and postoperative option was not contemplated . 
as for lung toxicity , according to common opinion a direct relationship exists and the current trend is to minimize volumes of treatment , especially in the context of dose escalation [ 20 ]  . 
 contrarily , some other analysis showed no correlation between toxicity and irradiated esophageal length , assuming that acute dysphagia is related more to the individual sensitivity [ 6 , 23 , 37 ]  . 
 in this context , a retrospective review on 207 consecutive nsclc patients rejected any correlation between esophagitis and the percentage of esophageal volume exposed to a certain dose , underlining the concept of the maximal esophageal dose as being significantly associated with a major risk of grade 3 toxicity . 
no other patientor treatment - related parameters were found to be predictive of severe esophagitis [ 35 ]  . our results apparently confirm the latter hypothesis of no correlation between irradiated esophageal volume and toxicity . 
looking at the dvh analysis , an apparent contradiction emerges : despite the evidence of important esophageal irradiation both in ap - pa and boost phase , with > 61% of the esophagus being irradiated to > 95% and 80% of the prescribed dose , respectively ( table 3 ) , there is no statistical correlation with toxicity ( table 4 )  . 
in addition , other parameters theoretically related to the disease extension ( t - class , number of positive mediastinal stations , ap - pa and boost target volume ) are not correlated with the incidence and severity of esophagitis . 
the interpretation of these findings is difficult , because these parameters seem to be related to the disease extension and , realistically , to the amount of esophagus irradiated , thus contradicting the absence of sigtable 6 . 
 [ 35 ] , our analysis was not able to calculate the maximal esophageal dose , since our treatment planning system did not allow a dvh calculation of the summed plan , so that the value of this factor was not investigated . 
although potentially obscured by the small sample size , the lack of significance observed might support a negligible role of total prescribed dose on acute esophagitis incidence . another parameter expected to be relevant in the toxicity occurrence is the addition of ct and particularly the timing with rt . 
in a recent trial of continuous hyperfractionated accelerated radiotherapy week - end - less ( chartwel ) combined with neoadjuvant ct , systemic treatment was given sequentially [ 30 ]  . 
 this approach resulted in enhancement of the incidence and the duration of acute dysphagia ; nevertheless , this increase was transient , subsequent healing occurred in all cases , and no evidence of late esophageal complications was shown . 
in particular , neither the presence of ict grade 3 toxicity nor the reduction ( due to toxicity ) of the planned ict regimen were associated with more severe toxicity . 
as already remembered , it is difficult to make comparisons between our results and others , because of the lack of statistical power due to the small number of events , and the differences in treatment schedules . 
with these uncertainties it is still possible that our findings may be a consequence of different study inclusion criteria , confirming the importance of patient selection , well known to be potentially related to radiation - induced esophagitis incidence [ 23 ]  . the toxicity profile in our series was in agreement with other reports present in the literature . 
for definitive treatments , calculated beds for early - reacting tissues were 72 gy10 ; so , compared with chart schedule ( bed10 of 62 gy10 ) and ecog schedule ( bed10 of 67 gy10 ) , a higher biological effect on early toxicity could theoretically occur . 
 as mentioned above , it was difficult to compare our toxicity results with the data obtained from the other two studies of 3tdrt because of differences in patient selections and treatment characteristics . 
furthermore , apart from the theoretical radiobiological considerations , it has to be remembered that , compared to the other trials , in our schedule the fraction dose was lower and the planned and resultant treatment time were more prolonged . 
 anyway , despite these limitations , our results seem to support a negligible role of dosimetric parameters and induction ct regimen in the genesis of radiation - induced acute esophagitis . 
our results also confirmed the clinical feasibility of and the good patient compliance with this intensive approach of 3tdrt , preceded by ict , as a definitive or postoperative local treatment in locally advanced nsclc , as already reported [ 10 ]  . 
analysis of pattern of failure and long - term survival is warranted to confirm the overall efficacy of this approach as an acceptable treatment option in well - selected locally advanced nsclc . 
5 3 gy wegen interponierter feiertage . ergebnisse : die lymphfistelsekretion variierte zu beginn der radiatio zwischen 50 und 650 ml / 24 h ( durchschnittlich 203 ml , median 175 ml ) , am ende der radiatio zwischen 0 und 350 ml ( durchschnittlich 126 ml , median 120 ml )  . 
die redon - drainage konnte bei 17 / 28 patienten ( 60 , 7% ) innerhalb von 10 tagen , bei weiteren 10 / 28 patienten ( 35 , 7% ) innerhalb von 1020 tagen nach abgeschlossener radiotherapie entfernt werden . schlussfolgerung : insgesamt erwies sich die radiatio von lymphfisteln als effektive , nebenwirkungsfreie und kostengnstige therapie , die nach durchschnittlich 10 , 5 tagen ( median 7 tage ) eine entfernung der redon - drainage ermglichte . 
damit stellt die radiatio eine effiziente alternative zu den sonst angewandten konservativen verfahren dar . schlsselwrter : lymphorrh bestrahlung von lymphfisteln radiotherapie gutartiger erkrankungen strahlenther onkol 2005 ; 181 : 396400 doi 10.1007 / s00066 - 005 - 1364 - 0 radiotherapy of inguinal lymphorrhea after vascular surgery . 
 patients and methods : from 08 / 1997 to 12 / 2000 , 28 patients with inguinal lymph fistulas were irradiated postoperatively ( 4th19th day ) with a single dose of 3 gy up to a total dose of 9 gy on 3 consecutive days using 120to 300 - kv photons . 
 results : secretion volume at the beginning of radiotherapy varied between 50 and 650 ml daily ( mean 203 ml , median 175 ml ) , at the end of radiotherapy between 0 and 350 ml ( mean 126 ml , median 120 ml )  . 
in 17 / 28 patients ( 60.7% ) the drains could be removed within 10 days , in further 10 / 28 patients ( 35.7% ) within 1020 days after the end of radiotherapy . 
 conclusion : overall , irradiation of inguinal lymph fistulas proved to be an effective and well - tolerated treatment , facilitating removal of fistula drains within 1020 days ( mean 10.5 , median 7 days ) after the completion of radiotherapy , thus appearing a good alternative to other conservative treatment modalities . 
die kutane lymphatische zirkulation nimmt ihren ursprung im subepithelialraum der dermis als oberflchlicher klappenloser kapillarplexus , der die gesamte krperoberflche kontinuierlich berzieht und ber schrge und vertikale stmme in ein system grerer lymphgefe einmndet [ 26 ]  . die oberflchlichen lymphgefe der unteren extremitt beginnen an den zehenspitzen , folgen dem stromgebiet der v . 
die tiefen lymphgefe begleiten die femoralgefe bis zu den tiefen leistenlymphknoten . das dichte oberflchliche und tiefe netz inguinaler lymphgefe birgt bei gefchirurgischen eingriffen ein hohes verletzungsund transsektionsrisiko mit konsekutiver bildung von lymphozelen , lymphorrhen oder lymphfisteln . 
lymphatische leckagen stellen eine ernsthafte komplikation dar , da eine kontamination das prothetische material gefhrden kann [ 16 ]  . eine standardtherapie von lymphfisteln ist nicht etabliert ; sowohl konservative als auch invasive manahmen werden empfohlen [ 13 , 16 , 23 ]  . 
die vorliegende arbeit prsentiert eine retrospektive analyse von 28 patienten mit lymphfisteln nach gefchirurgischen eingriffen , die zwischen 08 / 1997 und 12 / 2000 bestrahlt wurden . patienten und methodik patienten 28 patienten ( 21 mnner , sieben frauen , alter 4389 jahre , median 71 jahre , durchschnittlich 68 , 5 jahre ) wurden von 08 / 1997 bis 12 / 2000 wegen sezernierender leistenlymphfisteln zur durchfhrung einer radiatio vorgestellt . 
13 / 28 patienten hatten bereits einen gefeingriff , 4 / 28 zwei und 1 / 28 drei gefeingriffe hinter sich . nach der klassifikation der american society of anesthesiologists ( asa ) zur einschtzung des perioperativen risikos ( tabelle 1 ) entsprachen 2 / 28 patienten der risikogruppe ii , 15 / 28 der risikogruppe iii , 8 / 28 der risikogruppe iv und 1 / 28 der risikogruppe v . 
bei 11 / 28 patienten war das akute - phase - protein crp ohne klinisches korrelat whrend der radiatio erhht , bei 17 / 28 dagegen im normbereich . operationen smtliche lymphfisteln traten nach gefchirurgischen eingriffen auf : 25 / 28 nach bypassoperation mit gefrekonstruktion , 1 / 28 nach embolektomie , 1 / 28 nach patchplastik und 1 / 28 nach einer aneurysmaresektion . 
intraoperativ bentigten 1 / 28 patienten ein erythrozytenkonzentrat , 3 / 28 patienten zwei , 1 / 28 patienten drei , 3 / 28 patienten vier , 2 / 28 patienten sechs , 1 / 28 patienten acht und 1 / 28 patienten zwlf erythrozytenkonzentrate . 
als prothesenmaterial kamen in 12 / 28 fllen polytetrafluorethylen ( ptfe ) , bei 7 / 28 patienten dacron und bei 4 / 28 fallen silberimprgnierte gewebte prothesen zur anwendung ; bei 5 / 28 patienten fehlten die angaben . 
postoperativen tag ( median 7 , 5 tage )  . vor durchfhrung der bestrahlung erfolgte bei jedem patienten eine sonographische morphometrie der fistel mit exakten angaben zu lnge , breite und tiefenausdehnung . 
aufgrund eines interponierten wochenendes erhielten 1 / 28 patienten 8 gy ( 2 4 gy ) und 2 / 28 patienten 15 gy ( 5 3 gy )  . statistik die statistische auswertung erfolgte unter verwendung des programms med calc version 7.0. 
die potentiellen einflussparameter auf die sekretvolumennderung whrend der radiatio wurde mit dem spearman - rank - test ( < 0 , 05 ) untersucht . ergebnisse lymphfistelsekretion whrend der radiatio smtliche lymphfisteln waren mit einer redon - drainage versorgt ; das sekretvolumen in der redon - flasche wurde ab dem 1 . 
postoperativen tag alle 24 h bis zur entfernung der drainage nach sistieren der lymphsekretion dokumentiert . die lymphfistelsekretion variierte zu beginn der radiatio zwischen 50 und 650 ml / 24 h ( durchschnittlich 203 ml , median 175 ml ) , am ende der radiatio zwischen 0 und 350 ml ( durchschnittlich 126 ml , median 120 ml )  . 
die sekretmenge nahm im durchschnitt um 78 ml ( median 75 ml ) ab . hypertonus , diabetes , alter , bmi , hb vor radiatio , crp whrend der radiatio , strahlenenergie , - dosis bzw . 
 der gesamtstationre aufenthalt betrug durchschnittlich 32 , 85 tage ( 5118 tage , median 29 , 5 tage ) , von der operation bis zur entlassung durchschnittlich 27 , 85 tage ( 595 tage , median 22 , 5 tage )  . 
 [ 11 ] sprechen bei einem sekretaustritt von 30 ml / d klarer flssigkeit aus der operationswunde > 3 tage nach dem operativen eingriff oder > 5 tage nach der operation unabhngig von der sekretmenge von einer lymphfistel . 
die fehlende definition erklrt die unterschiedlichen angaben zu inzidenz und prvalenz der lymphfisteln in der literatur . lymphorrhen treten nach gefchirurgischen oder interventionellen eingriffen mit einer hufigkeit von 1 , 55 , 1% [ 1 , 16 , 19 , 20 ] auf und sind meist entlang der v . 
 pathophysiologisch fliet proteinreiche flssigkeit , die frei von gerinnungsfaktoren und thrombozyten ist , in den paravasalraum , ohne deckung der gefleckage durch eine gerinnselbildung [ 2 , 5 ]  . 
11 / 28 patienten in unserer eigenen klientel hatten whrend der radiatio ein erhhtes crp ohne klinisches korrelat einer infektion . infektionen stellen die schwerwiegendste komplikation einer lymphfistel dar [ 20 ] , da sie das prothetische material und damit die gesamte extremitt gefhrden . 
die angaben zur infektion variieren zwischen 1% und 25% , zur verzgerten wundheilung zwischen 1% und 6% und zur hautnekrose bis zu 5% [ 4 , 13 , 16 , 20 ]  . es besteht kein konsens ber die wirksamste therapie von lymphfisteln . 
daneben kommen invasive verfahren wie chirurgische revision und ligatur oder deckung der lymphfistel mit muskelflaps zur anwendung [ 23 , 28 ]  . eine weitere therapiemglichkeit stellt die radiatio von lymphfisteln dar , wobei der exakte wirkmodus unbekannt ist . 
diskutiert werden eine antiinflammatorische , antiproliferative wirkung [ 22 , 24 , 27 , 29 ] sowie eine radiogene beeinflussung der stickstoffmonoxid - ( no - ) synthese mit konsekutiver reduktion des mikrovaskulren filtrationsdrucks [ 12 ]  . whrend croft [ 7 ] und kutzner et al . 
 [ 17 ] eine einzeldosis von 12 gy vierbis fnfmal wchentlich bis zu einer ghd ( gesamtherddosis ) von 520 gy ; als konkretes beispiel werden 10 1 gy in 23 wochen genannt . 
zu beginn unserer bestrahlungsserie 08 / 1997 konzipierten wir das kurzzeitschema mit 3 3 gy in der absicht , den therapieassoziierten krankenhausaufentlymphsekretvolumen zu beginn der rt ( ml ) abbildung 1 . 
die aktuelle therapiestrategie befolgt die degro - leitlinie , zumal ihre therapeutische breite die fehlende dosisabhngigkeit des therapieerfolgs bercksichtigt und ein dem sekretfluss adaptiertes vorgehen ermglicht [ 17 ]  . 
 das nebenwirkungsprofil entspricht dem der radiatio paraossrer verkalkungen nach hftendoprothese [ 14 ] ; eine erhhte infektionsrate wurde nicht beobachtet , und das risiko einer radiogenen tumorinduktion ist zu vernachlssigen [ 8 , 9 ]  . 
bestrahlung von lymphfisteln schlussfolgerung insgesamt erwies sich in unserer retrospektiven analyse die radiatio von lymphfisteln mit 3 3 gy als effektive , nebenwirkungsfreie und kostengnstige therapie , die nach durchschnittlich 10 , 5 tagen ( median 7 tage ) eine entfernung der drainage ermglichte . 
 die fehlende begriffsdefinition der lymphfistel sowie die verwendung unterschiedlicher messparameter zur therapieevaluation erschweren den vergleich verschiedener , vor allem konservativer , therapiemodalitten und unterstreichen den bedarf an studien zu diesem thema . 
6 urban & vogel strahlentherapie und onkologie review article neck lymph node metastases from an unknown primary tumor retrospective study and review of literature hans christiansen1 , robert michael hermann1 , alexios martin2 , mirko nitsche1 , heinz schmidberger1 , olivier pradier1 background and purpose : up to 10% of all neck lymph node metastases present without a known primary site . 
furthermore , prognostic factors and treatment modalities are discussed . patients and methods : from 1984 to 2003 , 28 patients with squamous cell neck metastases from a cup were treated at the authors institution . 
whether limited radiotherapy might be equal to extended irradiation and can reduce side effects , must be shown in ongoing clinical trials . key words : neck lymph node metastases cup extended radiotherapy prognostic factors strahlenther onkol 2005 ; 181 : 35562 doi 10.1007 / s00066 - 005 - 1338 - 2 ergebnisse der behandlung zervikaler lymphknotenmetastasen bei unbekanntem primrtumor hintergrund und ziel : bei bis zu 10% aller patienten mit zervikalen lymphknotenmetastasen wird der primrtumor nicht gefunden . 
auerdem werden therapieoptionen und prognostische faktoren diskutiert . patienten und methodik : von 1984 bis 2003 wurden 28 patienten mit zervikalen lymphknotenmetastasen eines plattenepithelkarzinoms mit unbekanntem primrtumor in der universittsklinik gttingen behandelt . 
 die bestrahlung umfasste bei insgesamt 25 patienten die zervikalen lymphabflussgebiete beidseits sowie den gesamten rachenraum , vier patienten wurden lediglich ipsilateral zervikal bestrahlt . ergebnisse : die nachbeobachtungszeit betrug median 45 , 1 monate ( 4 , 1189 , 5 monate )  . 
die lokoregionre kontrolle war bei lymphknoten mit kapseldurchbruch signifikant schlechter als ohne kapseldurchbruch . 1 department of radiotherapy and radiooncology , university of gttingen , germany , 2 department of otorhinolaryngology , university of gttingen , germany . received : june 28 , 2004 ; accepted : january 14 , 2005 strahlenther onkol 2005 no . 
radiotherapy in neck lymph node metastases from a cup schlussfolgerung : mit radikaler operation und anschlieender adjuvanter radiotherapie knnen bei patienten mit zervikalen lymphknotenmetastasen eines unbekannten primrtumors gute berlebensund lokoregionre kontrollraten erzielt werden . 
ob durch eine weniger toxische auf das ipsilaterale zervikale lymphabflussgebiet limitierte bestrahlung dieselben ergebnisse wie durch eine ausgedehnte bestrahlung der gesamten rachenregion erreicht werden knnen , muss durch laufende klinische studien gezeigt werden . schlsselwrter : zervikale lymphknotenmetastasen unbekannter primrtumor radiotherapie prognostische faktoren patients were male and four female , patients age ranged from 38 to 86 years ( mean 58 years )  . 
nodal status was graded according to the union internationale contre le cancer / american joint committee on cancer ( uicc / ajcc ) criteria [ 34 ] : three patients ( 11% ) were n1 , five patients ( 18% ) n2 , and 20 patients ( 71% ) n3 . 
 initial examinations before the start of treatment included medical history , clinical ent ( ear - nose - throat ) examination ( magnifying laryngoscopy , bronchoscopy , esophagoscopy , endoscopy ) with multiple biopsies in potential mucosal primary sites , complete blood counts , biochemical analysis , electrocardiogram , chest x - rays , abdominal ultrasound , and ct scans of the thorax and the head and neck . in 17 patients ( 61% ) , neck dissection was performed in curative intention . 
after neck dissection , adjuvant radiotherapy was carried out with a mean of introduction according to the who definition , carcinoma of unknown primary ( cup ) is defined as histological diagnosis of metastases without diagnosis of a primary tumor . 
besides lung , liver and bone , the most frequent localizations of the metastases are neck lymph nodes : up to 10% of all neck lymph node metastases present without a known primary site [ 39 ]  . 
with physical examination of the head and neck and ct or mri scans followed by panendoscopy and biopsies , the primary tumor can be detected in > 40% of patients [ 25 ]  . 
besides , fmiso - pet ( 18f fluoromisonidazole positron emission tomography ) is also feasible to evaluate the state of oxygenation in subjacent head and neck tumors [ 13 ]  . 
others advise an extended irradiation including prophylactic therapy of all mucosal sites and both sides of the neck [ 6 , 30 ] , even though this approach causes more acute and late morbidity , especially chronic xerostomia [ 23 ]  . our retrospective analysis examined the clinical presentation , the diagnostic management and therapy of squamous cell neck lymph node metastases from an unknown primary tumor treated at the university of gttingen . patients and methods between 1984 and 2003 , 28 patients with squamous cell neck lymph node metastases of an unknown primary tumor were treated at our department . 
radiotherapy in neck lymph node metastases from a cup 56.7 gy ( range 49.663 gy ) , including an additional boost to the tumor region in nine of these patients ( mean dose 10.7 gy , range 918 gy )  . geneous in our patients owing to change of therapy concepts over the last 20 years in our department . 
 these patients received definitive radiotherapy with a mean of 66.8 gy ( range 56.774.4 gy ) , including an additional boost of 14.8 gy on average ( range 9.620 gy ) in ten patients . 
in summary , treatment modalities ( irradiation dose , boost application , fractionation , concomitant chemotherapy ) are inhomotoxicity was monitored weekly during therapy and every 2nd week following therapy until disappearance of acute side effects . 
 afterwards , all patients were examined at least yearly ; they underwent clinical ent examination , complete blood counts , biochemical analysis , chest x - rays , abdominal ultrasound , or a ct of the head and neck , if necessary . 
radiotherapy in neck lymph node metastases from a cup were taken from suspect findings to receive histological confirmation of tumor growth . follow - up data for assessment of tumor response , toxicity and overall survival and neck control were available for all patients . 
after this period of time , ten patients ( 36% ) remained alive . response and overall survival neck dissection with curative intent was possible in 17 patients ( 61% )  . 
5 - year overall survival rate was 40.1%. neck control , distant metastases and subsequent head and neck primary ( mucosal failure ) relapse in the neck occurred in six patients ( 21% ) , the mean time to neck failure was 11.2 months ( range 232 months )  . 
 similarly , extracapsular extension showed a statistically significant influence on neck control ( p = 0.04 ) : 5 - year neck control rate was 100% ( no extracapsular extension ) compared to 60% ( extracapsular extension )  . 
thereby , spearmans correlation test confirmed no dependence between surgery and extracapsular extension . by contrast , all other tested factors showed no significant influence on overall survival or neck control in our patients . 
as seen in table 3 , 5 - year overall survival rates in the literature vary from 16% to 86% , 5 - year neck control rates from 37% to 91% . 
surgery alone seems to be sufficient in nodal status n1 with no extracapsular extension [ 7 ]  . extent of radiotherapy and toxicity an important issue in neck metastases from an unknown primary is the appearance of a subsequent head and neck primary tumor . 
therefore , some authors advise an extended irradiation including prophylactic therapy of potential primary mucosal sites and both sides of the neck to minimize the risk of subsequent appearance of a primary tumor [ 2 , 6 , 15 , 24 , 30 , 35 , 38 ]  . 
acute ( skin reactions , mucositis , dysphagia , hoarseness ) and long - term ( xerostomia , trismus , osteonecrosis , lymphedema ) side effects of radiotherapy according to the rtog - eortc score . 
c : kombinierte behandlung aus operation und bestrahlung ; ext : bestrahlungsvolumen umfasste das zervikale lymphabflussgebiet und die rachenschleimhaut ; lim : bestrahlung der ipsilateralen zervikalen lymphknoten ; rt : radiotherapie ; s : operation . study patients ( n ) therapy regimen extent of rt 5 - year overall survival ( % ) 5 - year neck control ( % ) 5 - year appearance of head and neck primary ( % ) 26 coker et al . 
 [ 36 ] , who reported a risk of approximately 5% for osteoradionecrosis in head and neck cancer patients . role of chemotherapy some authors support the use of chemotherapy in neck metastases from an unknown primary tumor [ 8 , 9 , 18 ]  . 
the future role of chemotherapy in patients with neck metastases from an unknown primary tumor probably could be inferred from what is known about the value of chemotherapy in head and neck cancer : several meta - analyses indicate that the concomitant use of chemoand radiotherapy is superior to radiotherapy alone in improving survival and locoregional control in primary inoperable head and neck cancer [ 4 , 11 , 28 ]  . 
 [ 1 ] reported , in a randomized trial , that in advanced head and neck cancer concomitant radiochemotherapy with cisplatin as a radiosensitizer was superior to postoperative irradiation alone . 
by contrast , gender , histological grading , nodal status , tumor localization , and pretherapeutic hemoglobin level , which is a well - known independent prognostic factor in the radiotherapy of head and neck tumors [ 32 ] , had no significant influence on overall survival or neck control in our patients . 
still , this may be due to the small sample size . conclusion with radical surgery followed by radiotherapy good survival rates can be achieved in patients with neck metastases from an unknown primary tumor . 
 strahlentherapie und onkologie original article spectrophotometric skin measurements correlate with eortc / rtog - common toxicity criteria felix momm1 * , susanne bartelt1 * , kristine haigis1 , astrid groe - sender1 , gerlo witucki2 purpose : it was investigated whether the elementary eortc / rtog - ctc score ( common toxicity criteria ) for radiotherapy skin reactions correlates with spectrophotometric measurements of the skin color . patients , material , and methods : in 41 patients irradiated for unilateral breast cancer the regular scoring by ctc was done during radiotherapy . 
in parallel , a total of 4 , 920 spectrophotometric measurements to determine the skin color were performed at baseline , at the beginning of radiotherapy , and at 20 , 40 and 60 gy . 
the nonirradiated contralateral breast was used for control measurements . results : as expected , the skin color ( especially red ) depended on the radiation dose applied to the skthe objective spectrophotometric measurements were found to correlate well with the subjective ctc scores . conclusion : for classification of acute radiation toxicity there seems to be no need to replace the common ctc scoring by technical methods . key words : spectrophotometry radiotherapy side effects skin eortc / rtog - ctc score strahlenther onkol 2005 ; 181 : 3925 doi 10.1007 / s00066 - 005 - 1345 - 3 spektralphotometrische hautmessungen korrelieren mit dem eortc / rtog - ctc - klassifizierungssystem ziel : es wurde untersucht , ob der einfach zu handhabende eortc / rtog - ctc - score ( common toxicity criteria ) zur bestimmung der hauttoxizitt einer strahlentherapie mit spektralphotometrischen messungen der hautfarbe korreliert . patienten , material und methodik : bei 41 patientinnen , die wegen eines unilateralen mammakarzinoms bestrahlt wurden , wurde whrend der strahlentherapie regelmig der ctc - score fr die haut im strahlenfeld erhoben . 
die ergebnisse der spektralphotometrischen messungen korrelierten stark mit den subjektiven bewertungen anhand der ctc - klassifikation ( abbildung 2 )  . schlussfolgerung : bei der bewertung akuter strahlennebenwirkungen scheint es keine notwendigkeit zu geben , die bewhrte ctc - klassifikation durch technische messmethoden zu ersetzen . schlsselwrter : spektralphotometrie strahlentherapie nebenwirkungen haut eortc / rtog - ctc * f.m. 
contributed equally as first authors . 1 department of radiotherapy , university hospital freiburg , freiburg i.br. , germany , 2 radiotherapeutic department , diakonie - krankenhaus schwbisch - hall , schwbisch - hall , germany . received : july 20 , 2004 ; accepted : march 15 , 2005 strahlenther onkol 2005 no . 
as color is an important parameter in scoring skin toxicity [ 5 , 7 ] , it was expected that spectrophotometric measurements could contribute a new piece of mosaic in validating skin toxicity scoring systems . patients , material , and methods in the context of study rp 970015 , which tested the efficacy of topical rp 97 st ( perfluordecalin ) use in diminishing acute radiation skin toxicity , clinical classifications of skin reactions and spectrophotometric measurements were performed prospectively . 
we investigated the results of the ctc skin scores and compared them to the spectrophotometric measurements of the skin color to examine the correlation between subjective toxicity scores and objective measurements . 
the trial was approved by the ethics committee of the university of freiburg , germany , and written informed consent was obtained from each patient following the current revision of the helsinki declaration . 
exclusion criteria were any previous long - term dermatologic treatment , difficulties in wound healing , morphological changes of skin in the target volume , skin treatment with steroid - containing compounds in the treatment skin areas within 6 months before start of the study , insulin - dependent diabetes mellitus , alcohol or nicotine abuse , or sensitivity against components of the rp 97 st creafurther , patients with severe disease of heart , kidneys , lung or liver or with seizures or psychiatric diseases were excluded . 
considering skin color , an erythema will make skin darker and redder , thus diminishing the l * - value and increasing the + a * - value . study endpoints and question the study question was whether subjective scoring of radiation skin toxicity correlates with objective spectrophotometric measurements . 
 statistics to graphically demonstrate results , boxplots ( quartiles ) for the l * a * b * - values with different skin scores were performed ( figure 1 )  . 
as score data were in an ordinal scale , the spearman correlation between the l * - , a * and b * - values and the skin scores was calculated . results demographic data due to strict selection criteria of the study , the group of patients was very homogeneous . 
l * ( helligkeit ) , a * ( rot / grn ) und b * - werte ( gelb / blau ) der spektralphotometrischen messungen ber die strahlendosis : regressionsgeraden aus scatter - plots ( scatter nicht dargestellt : 4 920 einzelpunkte )  . 
 correlation of radiation dose with spectrophotometry to graphically demonstrate correlation between radiation dose and skin color evaluated by spectrophotometric measurements , scatterplots of l * - , a * and b * - values were performed and linear regression was calculated ( figure 1 )  . 
in irradiated skin lightness ( l * - value ) decreased markedly and the color got redder ( a * - value ) , whereas changes in the blue / yellow spectrum ( b * - value ) were less pronounced . 
comparing the results of b * - value ( blue / yellow ) measurements with ctc classification , no appreciable correlation was found ( spearman correlation coefficient 0.27 ; figure 2 )  . 
spectrophotometric skin measurements score for classification of late radiation toxicity was introduced [ 6 , 11 , 16 ] for more detailed differentiation of side effects [ 18 ]  . 
this higher accuracy led to a higher rate of registered late side effects [ 10 ]  . the ctc score was used in this study to show correlations between this very common subjective side - effect scoring system and objective measurements . 
additionally , the validity of these measurements is confirmed by correlation between spectrophotometry results and radiation dose ( figure 1 )  . a correlation between objective measurements and independent subjective toxicity scoring at the same point of time could be shown . 
 strahlentherapie und onkologie original article analysis of local control in patients with non - hodgkins lymphoma according to the who classification koh - ichi sakata1 , masaaki satoh2 , masanori someya1 , hisayasu nagakura1 , atushi oouchi1 , kensei nakata1 , katsuhisa kogawa3 , kazumitsu koito1 , masato hareyama1 , tetsuo himi4 purpose : to analyze the influence of radiotherapy doses , chemotherapy doses , and clinical parameters on in - field disease control to assess the optimal radiation doses for treatment of non - hodgkins lymphoma according to the newly proposed who classification . patients and methods : subjects consisted of 35 extranodal marginal - zone b - cell lymphomas of mucosa - associated lymphoid tissue ( malt ) type , 75 diffuse large b - cell lymphomas ( dlbcl ) , 14 follicular lymphomas , 17 extranodal natural killer ( nk ) / t - cell lymphomas , nasal type , eight unclassified peripheral t - cell lymphomas , four anaplastic large - cell lymphomas , t / null cell type , and five others . 
98 patients received chop , modified chop , or more intensive chemotherapy , and six patients were treated with other combination . results : no patients with malt lymphoma had in - field local recurrence . 
there were no recurrences in dlbcl patients who received chemotherapy in which the doses of adriamycin were > 200 mg / m2 , nor in dlbcl patients who were treated with > 45 gy . 
 the dose of adriamycin had no influence on local control of t - cell lymphoma . conclusion : t / nk - cell lymphomas were more radioresistant than b - cell lymphomas . 
the prognosis for peripheral t / nk - cell lymphomas is poor even when treated by irradiation combined with chemotherapy . key words : non - hodgkins lymphoma who classification t - cell lymphoma dose - response analysis strahlenther onkol 2005 ; 181 : 38591 doi 10.1007 / s00066 - 005 - 1330 - x analyse der lokalen kontrolle beim non - hodgkin - lymphom gem who - klassifikation ziel : untersuchung des einflusses der strahlungsdosis , chemotherapie - intensitt und klinischer parameter auf die kontrolle lokalisierter herde , um optimale parameter fr die behandlung des non - hodgkin - lymphoms gem der vor kurzem vorgeschlagenen who - klassifikation zu ermitteln . patienten und methodik : in die untersuchung einbezogen wurden 35 extranodale ( marginal - zone ) b - zell - lymphome des mukosa - assoziierten - lymphom - ( malt - ) typs , 75 diffuse grozellige b - zell - lymphome ( dlbcl ) , 14 follikulre lymphome , 17 extranodale natrliche - killer - ( nk - ) / t - zell - lymphome ( nasaltyp ) , 8 unklassifizierte periphere t - zell - lymphome , 4 anaplastische ( grozellige ) lymphome ( t / null - zell - typ ) and 5 andere . 
rezidive traten weder bei dlbcl - patienten auf , die chemotherapie mit adriamycin in dosierungen > 200 mg / m2 erhalten hatten , noch bei dlbcl - patienten , die mit > 45 gy behandelt worden waren . 
nur bei 9 von 15 t - zell - lymphom - patienten , die mit 50 gy , und bei 3 von 5 patienten die mit > 50 gy behandelt worden waren , wurde eine lokale kontrolle erreicht . 
 schlsselwrter : non - hodgkin - lymphom who - klassifikation t - zell - lymphom dosis - wirkungs - analyse 1 department of radiology , sapporo medical university , school of medicine , sapporo , japan , 2 department of clinical pathology , sapporo medical university , school of medicine , sapporo , japan , 3 department of fourth internal medicine , sapporo medical university , school of medicine , sapporo , japan , 4 department of otorhinolaryngology , sapporo medical university , school of medicine , sapporo , japan . received : june 8 , 2004 ; accepted : february 17 , 2005 strahlenther onkol 2005 no . 
dose - response analysis of nhl introduction the clinical course of non - hodgkins lymphoma ( nhl ) is highly variable , depending on the histological subtype and primary site of organ involvement [ 20 ]  . 
 with advances in combination chemotherapy regimens , patients with intermediate or more aggressive nhl are usually treated with combined chemotherapy and irradiation [ 3 , 13 , 19 ]  . however , little information is available on the optimal radiotherapy dose necessary to achieve in - field disease control and prolonged relapse - free survival in patients with nhl who receive chemotherapy . 
although no prospective randomized studies have been performed to evaluate the optimal radiotherapy dose for nhl , some retrospective data support the use of lower radiotherapy doses for low - grade lymphoma [ 17 ]  . 
besides , most of the dose - response analyses of lymphoma in the literature were performed in the era when patients received radiotherapy alone [ 4 , 12 , 28 ]  . 
 the revised european and american lymphoma ( real ) classification and the who classification were proposed and have been rapidly accepted [ 10 , 11 , 22 , 25 ]  . 
these classifications were proposed based on the cell of origin and delineate individual disease entities from the perspective of morphological features , immunophenotype and / or stage of differentiation , genotype , etiology , epidemiology , and clinical behavior . 
 we reevaluated histopathologic specimens of nhl , using the who classification , and investigated the relationship between the clinical characteristics and histopathologic classification of these specimens , in order to assess the usefulness of this new classification system in selecting treatment modalities . 
 we also analyzed the influence of radiotherapy doses as well as other treatment - related and clinical parameters on in - field disease control in order to assess the optimal radiation doses for treatment of nhl according to the who classification . 
 patients and methods patient characteristics between 1983 and 2001 , 158 patients with histologically confirmed nhl were treated at the department of radiology , sapporo medical university hospital , japan . 
 there were 35 extranodal marginal - zone b - cell lymphomas of mucosa - associated lymphoid tissue ( malt ) type ( malt lymphoma ) , 75 diffuse large b - cell lymphomas ( dlbcl ) , 14 follicular lymphomas ( five for grade 1 , six for grade 2 , and three for grade 3 ) , 17 extranodal natural killer ( nk ) / t - cell lymphomas , nasal type ( nasal nk / t - cell lymphoma ) , eight unclassified peripheral t - cell lymphomas , four anaplastic large - cell lymphomas , t / null cell type , and five others . 
 immunohistochemical studies were performed using paraffin sections , the avidin - biotin peroxidase complex technique , and a panel of monoclonal antibodies ( l2 cd3 , mt1 , uchl1 , and cd56 )  . 
 98 patients received chop ( cyclophosphamide : 750 mg / m2 or 600 mg / m2 in the elderly ; adriamycin : 50 mg / m2 or 40 mg / m2 in the elderly ; vincristine : 1.4 mg / m2 ; and prednisolone : 60 mg for 5 days ) , modified chop , or more intensive chemotherapy , and six patients were treated with other combinationor single - agent chemotherapy , mostly before irradiation . 
according to these results and others [ 21 ] , primary brain lymphomas were excluded from the following analysis , because their natural history and prognosis are very different from the other lymphomas [ 6 ]  . 
patients with malt lymphoma demonstrated higher statistical analysis in - field failure was defined as any failure with an in - field component , i.e. , any recurrence in the irradiated volume . 
 the overall and failure - free survival rates were calculated from the start of treatment by the kaplan - meier method , and differences in the survival rates were examined by the log - rank test . 
dlbcl : diffuses grozelliges b - zell - lymphom ; l / n : lymphknoten ; malt : mukosa - assoziiertes lymphoides gewebe ; nc : nasenhhle ; nk - cell : natrliche killer - zelle . 
overall survival curves ( a ) and relapse - free survival curves ( b ) for patients with stage i and ii non - hodgkins lymphoma according to histological examinations . 
dlbcl : diffuses grozelliges b - zell - lymphom ; l : lymphom ; malt : mukosa - assoziiertes lymphoides gewebe ; nasal nk / tl : nasales natrliche - killer / t - zellen - lymphom ; peripheral tl : nicht klassifizierte periphere t - zell - lymphome . 
no patients underwent in - field local recurrence even though there was a large variation in dose of radiotherapy and in the combinations of chemotherapy used in the treatment of malt lymphomas . figure 3 demonstrates the in - field local control of dlbcl according to intensity of chemotherapy and dose of radiotherapy . 
 there were no recurrences in patients who received chemotherapy in which the doses of adriamycin were > 200 mg / m2 , nor in patients who were irradiated with > 45 gy . 
however , the effect of chemotherapy in patients with a tumor size 6 cm was unclear . in 69 patients with dlbcl ( excluding brain lymphoma ) , 25 had bulky disease . 
in patients with stage i or ii , eight of 15 patients with nasal nk / t - cell lymphoma developed distant involvement , whereas none of six patients with unclassified peripheral t - cell lymphomas and only one of four with anaplastic large - cell lymphoma did so . 
 discussion it is necessary to identify the adverse prognostic factors in patients with localized aggressive nhl in order to select the patients who cannot be expected to be cured by the combined modality consisting of a short course of chop followed by radiotherapy . 
most studies on the optimal radiotherapy dose required to achieve in - field disease control and prolonged relapse - free survival in nhl , including our previous report [ 26 ] , utilized the working formulation [ 17 , 23 , 29 ]  . 
thus , there is little information on the clinical characteristics of nhl from the perspective of the who classification . in this series , about 20% of patients had tand nk - cell lymphoma . 
this is a unusual distribution in terms of pathology of nhl patients in the usa and europe [ 2 , 9 ] and it reflects a difference in prevalence of nhl between japan and western countries ; tand nk - cell lymphoma is relatively rare in the latter [ 16 ]  . 
nasal t / nk - cell lymphoma , which is characterized by progressive , unrelenting ulceration , and necrosis of the nasal cavity and midline facial tissues , is rare in the usa and europe but more common in asia . 
therefore , little information is available on the optimal radiotherapy dose to achieve in - field disease control and prolonged relapse - free survival , especially in t / nk - cell lymphoma [ 7 , 15 ]  . radiation dose ( gy ) figure 4 . 
no patients underwent in - field local recurrence even though there were large variations in doses of radiotherapy and in the combinations of chemotherapy used in the treatment for malt lymphoma ( figure 2 )  . 
 low - grade nhl of the gastrointestinal tract and other sites , such as salivary glands , the orbital regions , and thyroid , are grouped together as tumors arising in malt . 
therefore , patients with malt lymphoma are good candidates for radiation therapy alone . there were no in - field failures in patients with malt lymphoma treated with doses of at least 30 gy , suggesting that in our series the radiation doses used were adequate . 
these results concur with those obtained in other studies [ 5 , 27 ]  . there were no recurrences in dlbcl patients who received chemotherapy in which the doses of adriamycin were > 200 mg / m2 ( figure 3 )  . 
when patients treated with adriamycin 200 mg / m2 were compared with those treated with adriamycin < 200 mg / m2 , the difference in local control was not statistically significant , most likely because of the inadequate sample size . 
however , 45 gy might be required to treat patients who have received irradiation alone or chemotherapy in which the doses of adriamycin were < 100 mg / m2 . the presence of tumor bulk has been suggested to influence treatment outcome [ 17 , 23 , 29 ] , and recently , oguchi et al . 
in our series , chemotherapy was effective in preventing distant involvement in dlbcl patients whose tumor size was < 6 cm , whereas the effect of chemotherapy was unclear for patients whose tumor size was 6 cm ( table 3 )  . 
most patients in our study belonged to intermediate - grade nhl , which may explain this discrepancy of results . our study indicated that a minimum dose of 46 gy was required to obtain local control of t - cell lymphoma and some radioresistant t - cell lymphomas could not be controlled even with 60 gy ( figure 4 )  . 
 although it is unclear whether there is a difference in responses to radioand chemotherapy among subtypes of t / nk - cell lymphoma due to the small numbers of these lymphomas , our results indicate that the standard treatment strategy for nhl , i.e. , a combined modality consisting of three cycles of chop and radiotherapy , is not sufficiently effective . 
reported that in centroblastic - centrocytic nhl ( stages i / ii ) , most relapses were located outside the radiation portals , yet extended field radiotherapy was not superior to involved - field radiotherapy in terms of overall survival and relapse - free survival [ 8 ]  . 
prospective randomized trials are necessary to prove a potentially favorable effect of more extended radiotherapy portals ( tli or tni [ total nodal irradiation ] ) and to evaluate the optimal radiotherapy dose . 
to evaluate the feasibility and toxicity of irradiation and concomitant administration of 50 mg / m2 temozolomide in patients with primary malignant glioma , this phase i / ii study was conducted . patients and methods : 53 patients with histologically confirmed who grade iv malignant glioma were enrolled into the study . 
 temozolomide was administered orally each therapy day at a dose of 50 mg / m2 . results : prior to radiochemotherapy , complete resection ( n = 14 ) , subtotal resection ( n = 22 ) or a biopsy ( n = 17 ) of the tumor was performed . 
the application of 50 mg / m2 of temozolomide can be performed throughout the whole time course without interruption due to side effects and might largely contribute to the prolonged overall survival . 
further evaluation is warranted as to which dose of temozolomide is optimal with regard to tumor response and toxicity . key words : glioblastoma multiforme temozolomide radiation overall survival toxicity strahlenther onkol 2005 ; 181 : 3727 doi 10.1007 / s00066 - 005 - 1359 - x radiochemotherapie mit temozolomid zur postoperativen behandlung von patienten mit primrem glioblastoma multiforme . 
die vorliegende studie evaluiert die durchfhrbarkeit und toxizitt der strahlentherapie mit simultaner gabe von 50 mg / m2 temozolomid zur therapie von patienten mit primrem glioblastoma multiforme . patienten und methodik : 53 patienten mit histologisch gesichertem glioblastoma multiforme ( who - grad iv ) wurden in die studie eingeschlossen . 
temozolomid wurde an jedem tag der strahlentherapie in einer oralen dosierung von 50 mg / m2 appliziert . ergebnisse : vor der strahlentherapie wurde bei 14 patienten eine komplette tumorresektion , bei 22 patienten eine partielle resektion und bei 17 patienten ein biopsie durchgefhrt . 
das alter und das ausma der neurochirurgischen resektion beeinflussten das gesamtberleben signifikant . 1 department of radiation oncology , university of heidelberg , heidelberg , germany , 2 department of radiation oncology , nordwestkrankenhaus frankfurt , frankfurt / main , germany , 3 central unit biostatistics , german cancer research center ( dkfz ) , heidelberg , germany . received : august 25 , 2004 ; accepted : february 2 , 2005 strahlenther onkol 2005 no . 
in most malignancies of the brain the blood - brain barrier is an obstacle to chemotherapy , but in malignant glioma chemotherapy is discussed controversially since the blood - brain barrier is commonly disrupted . recent studies have proven different chemotherapy regimens to be effective in prolonging progression - free survival and overall survival in patients with malignant glioma [ 14 ]  . 
in the last years new drugs such as irinotecan [ 9 ] , paclitaxel ( taxol ) [ 3 ] and temozolomide [ 1 ] have been evaluated in the treatment of high - grade gliomas . 
temozolomide penetrates into all body tissues including the braone mechanism that can produce resistance against this drug is mediated through the enzyme o6 - alkylguanine transferase ( agt ) , which is expressed in very low concentrations in most brain tumors . 
the rationale for the combination of temozolomide and radiation therapy is based on preclinical data suggesting additive or perhaps synergistic activity , demonstrating additive cytotoxicity against the u373mg glioblastoma cell line [ 31 , 34 ]  . 
 the efficacy of temozolomide was evaluated in recent phase i [ 2 , 20 ] and phase ii studies [ 11 , 13 , 36 ] focusing on patients with recurrent malignant glioma . 
a large randomized prospective clinical trial conducted by the eortc could demonstrate a highly significant advantage for patients treated with irradiation and concomitant application of 75 mg / m2 temozolomide and up to six cycles of adjuvant temozolomide as compared to radiotherapy alone [ 29 ]  . 
 the present phase i / ii study of 50 mg / m2 temozolomide in combination with irradiation as a first - line treatment of malignant glioma evaluates the feasibility , safety , tolerability , and toxicity of this regimen and the effect on progression - free survival and overall survival of the enrolled patient population . patients and methods from april 1999 to october 2003 , 53 patients with glioblastoma multiforme were enrolled into the phase i / ii protocol . 
 demographics and baseline characteristics are presented in table 1 . eligibility criteria were histologically proven supratentorial disease , either glioblastoma multiforme , gliosarcoma or giant cell glioblastoma , enrollment within 45 days after surgery , age between 18 and 70 years , and karnofsky performance score ( kps ) 50 . 
laboratory values performed within 14 days prior to treatment with an absolute neutrophil count ( anc ) 1 , 500 / mm3 or white blood cells ( wbc ) 2 , 000 / mm3 , platelet count 100 , 000 / mm3 , hemoglobin 10 g / dl , urea and serum creatinine < 1.5 times upper limit of laboratory normal , sgot and sgpt 3 times upper limit of laboratory normal and alkaline phosphatase 3 times upper limit of laboratory normal were required . 
 exclusion criteria were any prior chemotherapy with dacarbazine ( dtic ) or temozolomide , prior radiation therapy to the brain , and lack of recovery from all active toxicities or prior therapies . 
frequent vomiting or a medical condition interfering with the intake of oral medication , as well as patients with previous or concurrent malignancies with the exception of surgically cured carcinoma in situ of the cervix and basal or squamous cell carstrahlenther onkol 2005 no . 
 3072 parameter patients ( n ) sex ( n ) male female age ( years ) median range karnofsky performance status 80 < 80 prior neurosurgical treatment ( n ) complete resection subtotal resection biopsy neurologic symptoms ( n ) yes headaches nausea / vomiting seizures motor deficiencies sensory deficiencies edema / increased intracranial pressure other no steroids prior to radio - / chemotherapy ( n ) yes no steroids after radio - / chemotherapy ( n ) yes no antiepileptic medication prior to radio - / chemotherapy ( n ) yes no antiepileptic medication after radio - / chemotherapy ( n ) yes no approximately the same time of the day within and during each week . 
 at the time point of tumor progression a subgroup of 17 patients received stereotactically guided fractionated radiotherapy with a median dose of 36 gy in a median fractionation of 5 2 gy per week . overall survival time was defined from the time point of primary diagnosis to the date of death , or november 1 , 2003 , depending on which occurred first . 
we recorded the time from the beginning of radio - / chemotherapy to the last visit as follow - up time ; progression - free survival was the time from treatment beginning to tumor progression diagnosed by mri scans . 
subgroup analysis was based on age , gender , kps , extent of neurosurgery performed prior to study enrollment , and neurologic symptoms . results patients cinoma of the skin , were exclusion criteria . 
all women of childbearing potential had to have a negative serum pregnancy test 24 h prior to administration of the study drug and were required to practice medically approved contraceptive precautions . 
all patients meeting the inclusion criteria who gave informed consent were included into the study . temozolomide was prescribed at a dose of 50 mg / m2 each day of radiation treatment . 
all patients underwent neurosurgical treatment prior to radiochemotherapy ; in 14 patients a complete resection of the tumor could be performed , in 22 patients residual tumor was present after neurosurgery , and in 17 patients stereotactically guided biopsies were performed . 
 kps was 80 in 42 patients and < 80 in eleven patients before treatment began , and 80 in 39 and < 80 in 14 patients after completion of treatment . 
46 patients presented with neurologic symptoms before and 45 after radiochemotherapy , including motor and sensory deficits , headache , nausea and vomiting , epilepsy and edema with increased intracranial strahlenther onkol 2005 no . 
blood values including hemoglobin ( a ) , thrombocytes ( b ) , and leukocytes ( c ) before therapy ( t0 ) and once weekly ( t1t6 ) during radiochemotherapy . 
hmoglobin ( a ) , thrombozyten ( b ) und leukozyten ( c ) zum zeitpunkt t0 zu beginn der behandlung und nachfolgend wchentlich ( t1t6 ) whrend der radiochemotherapie . 
das ausma der chirurgischen resektion ( b ; p = 0 , 00075 ) und das alter der patienten ( c ; p = 0 , 0008 ) beeinflussten das gesamtberleben signifikant . 
median follow - up time was 17 months ( range , 353 months ) , progression - free survival 8 months ( range , 240 months ; figure 3 )  . 
multivariate cox regression analysis evaluating the influence of age , extent of neurosurgical resection , gender , presence of neurologic symptoms and kps on overall survival identified only age ( p = 0.0008 ) and the extent of neurosurgical resection ( p = 0.00075 ) as significant prognosticators . discussion malignant gliomas are the most challenging of all cancers to treat successfully . 
they are characterized not only by aggressive proliferation and expansion but also inexorable tumor invasion into distant brain tissue , and occur at a rate of five cases per 100 , 000 per year . 
median overall survival times between 9 and 12 months can be achieved for patients with glioblastoma multiforme [ 7 , 8 , 19 , 24 , 26 , 29 ]  . in recent years , a noticeable reorientation is taking place in the treatment of malignant glioma . 
recent evaluation of radiochemotherapy regimens has proven a beneficial outcome for this multimodality approach [ 23 , 26 ] , resulting in a prolongation of median overall survival with chemotherapy being a part of the first - line treatment of patients with malignant glioma . 
 a combination of radiation therapy with oral and intravenous administration of pcv ( procarbazine , ccnu , vincristine ) could slightly increase overall survival [ 15 , 19 ]  . 
the downside of pcv application is the high rate of side effects including severe neuropathies . application of concomitant irradiation and bcnu can increase overall survival significantly from 8.5 months for radiotherapy alone to 11.5 months for combined radiochemotherapy [ 25 , 32 ] , independently of major prognostic factors [ 16 , 29 ]  . 
the addition of teniposide ( vm26 ) to bcnu and radiation therapy has been shown to further extend progression - free survival in a trial of the gag group , but influence on overall survival could not be observed ( gag study group )  . 
the noa - 1 trial confirmed the notion that concomitant application of acnu plus ara - c or teniposide ( vm26 ) is beneficial in the treatment of primary malignant glioma , without relevant pulmonary toxicity [ 35 ]  . 
median overall survival times of 16.5 months for patients with primary glioblastoma multiforme could be achieved , representing better median survival times than any other previous phase iii trial [ 7 , 8 , 24 ]  . temozolomide exerts its cytotoxic effect by methylating guanine in dna at the n - 7 and o - 6 positions [ 4 , 21 , 25 , 30 ]  . 
it readily crosses the blood - brain barrier and achieves effective concentrations in the central nervous system with a reported plasma - csf ( cerebrospinal fluid ) ratio of 3040% [ 28 ]  . 
 the patient population enrolled in our study profited from combined radiochemotherapy shown by a median overall survival time of 19 months , comparably high to survival times found in the literature . 
in accordance with the literature , younger patients and patients after complete and subtotal resection had a significantly better outcome , whereas no statistical significance could be demonstrated between patients receiving a total as opposed to a subtotal resection . 
concomitant radiotherapy plus temozolomide followed by adjuvant temozolomide evaluated in a phase ii study led to a median overall survival of 16 months in a clinical phase iii trial published by stupp et al . 
recently , the results of a large randomized phase iii clinical trial were presented demonstrating a highly significant increase in overall survival for patients who received radiochemotherapy with 75 mg / m2 temozolomide and up to six cycles of adjuvant temozolomide as compared to patients treated with irradiation alone . 
however , with the application of only 50 mg / m2 temozolomide as performed in the present study , toxicities can be kept low , allowing the continuous application of temozolomide without interruptions . 
temozolomide and irradiation in glioblastoma multiforme cause continuous exposure to temozolomide leads to depletion of o6 - alkylguanine dna alkyltransferase ( agt ) , which is also known as methylguanine - dna [ 10 ] , and therefore might largely contribute to the outcome , since treatment interruptions due to toxicity can be prevented . 
 conclusion our data strongly support the idea that 50 mg / m2 temozolomide in combination with irradiation is beneficial in the treatment of patients with primary glioblastoma multiforme , with very little toxicity . 
therefore , further investigation as to which dose of temozolomide should be administered is warranted . strahlentherapie und onkologie fallstudie porphyrie und radiotherapie : doch eine risikokonstellation ? walter rhomberg1 , felix albert offner2 hintergrund : ber die strahlenreaktionen bei patienten mit einer porphyrie ist wenig bekannt . 
theoretisch msste bei einer porphyrie mit verstrkten reaktionen zu rechnen sein , doch in kasuistischen darstellungen bei zwei mammakarzinomen , einem blasenkarzinom und einem malignen lymphom zeigten sich keine auffallenden vorkommnisse . fallbericht : berichtet wird ber zwei patienten mit porphyrie und glioblastoder nachweis der porphyrie und die klinischen krankheitsverlufe werden beschrieben . 
gleichzeitig zur radiatio wurden den patienten 100 mg / m2 acnu [ 1 - ( 4 - amino - 2 - methyl - 5 - pyrimidinyl ) - methyl - ( 2 - chloroethyl ) - 3 - nitrosoharnstoff ] in geplanten 6 - wchigen intervallen infundiert . ergebnisse : beide patienten zeigten zwar eine gute objektive rckbildungstendenz ihrer glioblastome , verstarben jedoch schon 7 bzw . 
der zweite patient wies schon nach 38 gy eine deutliche tumornekrose auf ; er starb noch whrend der strahlenbehandlung unter den zeichen einer kardiopulmonalen insuffizienz . schlussfolgerung : hinweise in der literatur und die hier beschriebene kasuistik legen nahe , bei der strahlenbehandlung von hirntumoren oder bei einer mitbestrahlung von nervengewebe im fall einer porphyrie vorsichtig zu seeine reihe von molekularbiologischen erkenntnissen untersttzt diese empfehlung . 
 schlsselwrter : porphyrie glioblastoma multiforme konkomitante radiochemotherapie hirnnekrose strahlenther onkol 2005 ; 181 : 4014 doi 10.1007 / s00066 - 005 - 1311 - 0 porphyria and radiotherapy : yet a constellation of risk ? background : little is known concerning the relation of porphyrias to radiation treatment for cancer . 
the patients received a concomitant radiochemotherapy with infusions of acnu [ 1 - ( 4 - amino - 2 - methyl - 5 - pyrimidinyl ) - methyl - ( 2 - chloroethyl ) - 3 - nitrosourea ] every 6 weeks . 
gleichzeitig zur bestrahlung erhielt die patientin 150 und 100 mg acnu [ 1 - ( 4 - amino - 2 - methyl - 5 - pyrimidinyl ) - methyl - ( 2 - chloroethyl ) - 3 - nitrosoharnstoff ] als kurzinfusion . 
ein rezidiv war im ct und mrt nicht nachweisbar . unklare neuritische schmerzen , septisches fieber sowie das auftreten von hautinfiltraten lsten neue diagnostische berlegungen aus und fhrten zur diagnose einer akuten hepatischen porphyrie , vermutlich durch sedativa , schmerzmittel und / oder barbiturate ausgelst . 
die diagnose wurde durch eine permanente hyponatrimie , erhhte ausscheidung von uroporphyrin im urin , eine leichte erhhung von - aminolvulinsure im urin ( 4 , 6 mg / l , normalwerte 0 , 14 , 5 mg / l ) und eine sechsfache erhhung von protoporphyrin in erythrozyten auf 5 927 nmol / l ec ( normalwert < 1 068 nmol / l ec ) gesichert . an der haut bestand seit jugendjahren eine vitiligo . 
 jetzt entwickelten sich zuerst an den streckseiten der extremitten , dann auch an stamm , handrcken und axilla entzndlich - solide hauteffloreszenzen , die nicht auf sonnenexponierte stellen beschrnkt waren . 
da neben den beinschmerzen auch intermittierende abdominale schmerzzustnde auffielen , wurde die verdachtsdiagnose einer porphyrie gestellt . laborprofil : protoporphyrin im erythrozyten : 1 560 ng / l ec ( normal < 1 068 ng / l ec ) , koproporphyrin iii / i + iii : 90% ( normal 6886% )  . 
 es ist natrlich nicht bekannt , ob bei den beiden in der literatur genannten brustkrebsfllen mit porphyrie und bestrahlungen dieses resistenzgen vorhanden war . anders scheint die situation bei tumoren des nervensystems zu seim ersten der hier beschriebenen flle eines bestrahlten glioblastoms hatte sich die akute porphyrie postoperativ entwickelt und unter der strahlentherapie verstrkt . 
 bei der autopsie war das ausma der zerebralen nekrose schon makroskopisch eindrcklich und soweit wir uns erinnern konnten ohne vergleich zu kleineren vorkommnissen dieser art unter unseren letzten 160 fllen mit strahlenbehandelten hirntumoren . 
ob photofrin ii bei unserer patientin eine solche rolle spielen konnte , muss offen bleiben , aber es ist evident , dass sich bei einer porphyrie unter einer radiatio im gehirn mehrere zytotoxische mechanismen summieren knnen . 
bei fall 2 war eine abschlieende beurteilung nicht mglich , da der patient whrend der laufenden behandlung verstarb , doch ist die histologisch gesicherte weitgehende nekrotisierung eines glioblastoms schon nach 38 gy nicht die regel . 
beide patienten hatten mit 1 , 5 und 7 monaten nach diagnosestellung eine berlebenszeit , die weit unter dem median von 13 monaten unserer patienten mit glioblastoma multiforme und gleichzeitiger radiochemotherapie mit acnu , aber auch unter den erfahrungen anderer autoren [ 3 , 10 , 11 , 16 ] liegt . 
 in diesem zusammenhang ist auch ein lterer literaturbericht von interesse , der die auslsung einer tdlichen porphyrieattacke durch die bestrahlung eines benignen zervikalsyndroms mit 1 500 cgy beschreibt [ 9 ]  . 
 ein 60 - jhriger mann [ b.l. ] wurde wegen eines multifokalen glioblastoms der rechten hemisphre mit 60 gy bestrahlt ; gleichzeitig wurde temozolomid ( temodal ) jeweils 75 mg / m2 per os an den bestrahlungstagen gegeben . 
klinisch fhrten eine hyponatrimie und atypische neurologische symptome ( ischiassyndrom ohne erkennbare ursache ) zur verdachtsdiagnose porphyrie , welche dann durch eine erhhte ausscheidung von gesamtporphyrin im urin ( 690 g / 24 h ; normalwerte 0150 g ) wahrscheinlich gemacht wurde . 
 korrespondenzanschrift walter rhomberg abteilung fr radioonkologie landeskrankenhaus feldkirch carinagasse 47 6800 feldkirch sterreich telefon ( + 43 / 5522 ) 303 - 3301 , fax - 7527 e - mail : walter.rhomberg@lkhf.at strahlenther onkol 2005 no . 
6 urban & vogel strahlentherapie und onkologie case study a microcystic adnexal carcinoma in the auditory canal 15 years after radiotherapy of a 12 - year - old boy with nasopharynx carcinoma karl t . 
we are already in a time when a higher number of patients with radiogenic secondary malignancies must be expected . case report : a 12 - year - old boy is reported who suffered from an advanced nasopharynx carcinoma and was treated with radical irradiation in 1983 . 
the secondary malignant neoplasm was resected and required another radiation treatment ( 1 gy b.i.d. ) due to involved margins . discussion and literature review : the entity of microcystic carcinoma is discussed with a review of the literature on biology , diagnosis , and treatment . key words : radiogenic malignancy pediatric nasopharynx carcinoma microcystic adnexal carcinoma reirradiation strahlenther onkol 2005 ; 181 : 40510 doi 10.1007 / s00066 - 005 - 1323 - 9 mikrozystisches adnexales karzinom des ueren gehrgangs 15 jahre nach radiotherapie eines 12 - jhrigen patienten mit nasopharynxkarzinom hintergrund : radiogene zweittumoren setzen heilung der ersterkrankung und langes berleben voraus . 
wir kommen zu oder sind bereits in einer zeit , in der mit erhhter wahrscheinlichkeit mit dem auftreten radiogener zweittumoren gerechnet werden muss . fallbericht : berichtet wird ber einen patienten , der 1983 als 12 - jhriger wegen eines lokoregionr fortgeschrittenen nasopharynxkarzinoms kurativ bestrahlt wurde und bei dem 15 jahre spter ein sehr seltenes mikrozystisches adnexales karzinom des ueren gehrgangs im volumen der zieldosis diagnostiziert wurde . 
cure from the first malignancy and long survival are the preconditions for the development of a radiogenic secondary malignant neoplas due to their longer life expectancy and their still growing organs children are particularly at risk [ 8 , 15 , 25 , 27 , 31 , 33 , 36 , 38 , 40 , 42 , 45 , 46 , 57 , 59 ]  . 
 most literature is about secondary malignant neoplasms in hodgkins disease and brain tumors . nasopharynx carcinoma ( npc ) in children is rare [ 6 , 35 , 58 ] and often develops as a painless cervical swelling of enlarged , sometimes huge cervical lymph nodes . 
 the current standard treatment of npc in children is simultaneous radiochemotherapy [ 5 , 14 , 24 , 53 , 61 ]  . we would like to report on a secondary malignancy 15 years after radical exclusive radiotherapy in a 12 - year - old boy , who suffered from an advanced npc . 
 case report nasopharynx carcinoma ( npc ) in 1983 , a 12 - year - old boy in good health and with an unremarkable personal history was sent to radiotherapy for a locoregionally advanced undifferentiated npc , then called type schmincke - regaud . 
the oral mucosa became atrophic and the patient lost his teeth as a consequence of xerostomia but did not suffer from severe side effects at first [ 17 , 22 , 23 ]  . 
 however , beginning in the 5th year after radiotherapy the then 17 - year - old boy became symptomatic from diverse severe and clinically evident late effects . as the first symptom a left phrenicus paresis appeared . 
meanwhile , the cervical spine had become heavily deformed ( figure 2 ) , the right mandible hypotrophic and all cervical soft tissues atrophic . in the 10th year after radiotherapy the meanwhile 22 - year - old patient suffered from a thrombosis of the left jugular vein and the left brachiocephalic vein , and a collateral circulation in the upper thoracic aperture had developed ( figure 2 )  . 
radiogenic malignancy in a boy with npc the radiotherapy had also caused endocrinological alterations , which were clinically not significant and were diagnosed only at the time when preparation for postoperative radiotherapy of the secondary malignant neoplasm was organized . 
basal tsh ( thyroid - stimulating hormone ) was significantly increased to 12.7 mu / l ( normal range , 0.354.5 mu / l ) with an ft3 ( free triiodothyronine ) of 4.84 pmol / l ( normal range , 3.56.5 pmol / l ) and an ft4 ( free thyroxine ) of 10.7 pmol / l , ( normal range , 9.525 pmol / l )  . 
the sex hormones showed the following baseline values : lh ( luteinizing hormone ) 10.8 u / l ( normal range , 316 u / l ) , fsh ( follicle - stimulating hormone ) 24.9 u / l ( normal range , 29 u / l ) , and testosterone 94.8 pmol / l ( normal range , 66142 pmol / l )  . 
the acth - cortisol axis and the growth hormone production were not involved . 13 years after treatment , a chronic eczema of the right external auditory canal was diagnosed for the first time , presumably the first hint at the later diagnosed secondary malignant neoplasm . microcystic adnexal carcinoma ( mac ) diagnosis . 
in december 1998 , 15 years after radiotherapy of the npc , the meanwhile 28 - year - old patient contacted his family practitioner because of increased pain in the right ear and progressive hearing loss . 
musculoskeletal changes ( atrophy of erector trunci muscles , kyphoscoliosis of the cervical spine ) , marked telangectasias in the previously irradiated regions , and extensive collateral circulation in the left thoracic aperture . 
histological specimen showing a typical microcystic adnexal skin carcinoma with extended dissociated and infiltrating growth , infiltration of perineural sheaths , focal squamous differentiation , and pseudoepitheliomatous hyperplasia , he 25 . 
saliva production was reduced ( unstimulated saliva flow 0.24 ml / min ; stimulated 0.44 ml / min ) and , as a consequence , the patient was edentulous . as our standard treatment for a second course of radical irradiation after a first full - course radiotherapy , we employed a 3 - d - based bifractionated ( 1 gy b.i.d. ) regimen and applied a total dose of 66 gy in the icru point . 
the clinical target volume ( ctv ) encompassed the former tumor region of the resected auditory canal and the first lymphatic drainage to the parotid and the level ii area . 
the last follow - up ct scan showed a complete remission , a fibrosis of the temporomandibular joint , and a streaky imbuement of the fatty tissues of the flap ( figure 5 )  . the most recent laboratory parameters included a macrocystic anemia ( hemoglobin 105 g / l ) probably as a consequence of chronic alcohol abuse . 
the substitution with levothyroxine was successful with a suppression of the basal tsh level to 0.003 and an increase in ft3 and ft4 to 6 and 24.2 pmol / l , respectively . radiotherapy was not combined with simultaneous chediscussion motherapy which does not seem effective for mac . the second radiation treatment was surprisingly well tolerated ; acute skin and mucosal reactions did never exceed grade 2 and disappeared within 6 weeks . the patient was last seen 66 months after the second radiotherapy . 
the patient reported occasional slight pain when opening his mouth which was already reduced after the first treatment , we report on a rare case of mac in the auditory canal that developed 15 years after radical radiotherapy for an npc in a then 12 - year - old boy , who was a second time successfully treated by subradical surgery and postoperative irradiation . since npc in children is a rare disease , few data on secondary tumors after radiotherapy of npc in children are found . mac was first defined in 1982 by goldstein et al . 
radiogenic malignancy in a boy with npc 49 ] , but never as a secondary malignant neoplasm after radiotherapy for npc . in a larger series of 27 patients , antley et al . 
 at clinical examination most often asymptomatic slowly growing nodules or cyst - like tumors are found , some presenting with a scar - like appearance [ 7 , 10 ]  . 
the tumor can be mistaken for other neoplasms , such as squamous cell carcinoma [ 7 , 12 , 13 , 21 ] as in the first biopsy of our patient . 
there is a relationship of mac with salivary and sweat gland tumors [ 60 ] , since they share common histological features and chromosomal aberrations . the macs are locally invasive , destructive , and often infiltrate perineural sheaths [ 7 ]  . 
surgery is recommended as the treatment of choice [ 12 , 18 ] , particularly mohs microsurgery . a gross tumor mass of mac is commonly considered to be radioresistant [ 49 ]  . 
this approach was validated in our case , in which the concept of a second radical radiotherapy 15 years after the first radical treatment was chosen instead of a further mutilating surgery followed by adjuvant radiotherapy [ 16 , 26 , 29 , 32 , 34 , 37 , 5156 ]  . 
grotz ka ; gemeinsame stellungnahme der deutschen gesellschaft fr zahn - , mundund kieferheilkunde ; deutschen gesellschaft fur radioonkologie , medizinische physik und strahlenbiologie ; abstimmung mit dem vorstand der deutschen gesellschaft fur zahnerhaltungskunde . 
microcystic adstrahlentherapie strahlentherapie und onkologie und onkologie original article original article results of three dimensional conformal radiotherapy and hormonal therapy for local recurrence after radical prostatectomy rudolf schwarz , andreas krll , silke tribius , winfried alberti1 background and purpose : analysis of treatment results of combined three - dimensional conformal radiotherapy ( 3dcrt ) and hormonal therapy in patients with locally recurrent prostate cancer after radical prostatectomy . patients and methods : between 1992 and 1998 , 24 patients presented with a rising prostate - specific antigen ( psa ) between 4 and 152 months following radical prostatectomy and a local recurrence demonstrated by imaging . 
acute and late toxicities , classified with the rtog score , were moderate . conclusion : radiotherapy and short - term adjuvant hormone therapy represent an effective and well - tolerated treatment for locally recurrent prostate cancer after radical prostatectomy resulting in good local control . 
 key words : prostate cancer prostatectomy local recurrence three - dimensional conformal radiotherapy strahlenther onkol 2005 ; 181 : 4427 doi 10.1007 / s00066 - 005 - 1363 - 1 ergebnisse der dreidimensional geplanten , konformalen radiotherapie von lokalrezidiven nach radikaler prostatektomie hintergrund und ziel : die ergebnisse der kombinierten konformalen radiotherapie und hormontherapie von lokalrezidiven nach radikaler prostatektomie werden analysiert . patienten und methodik : zwischen 1992 und 1998 wurde bei 24 patienten mit steigenden psa - werten ( prostataspezifisches antigen ) 4152 monate nach radikaler prostatektomie ein lokalrezidiv in der bildgebung nachgewiesen . 
bei 21 patienten wurde zustzlich eine bis zu 6 - monatige hormontherapie durchgefhrt . ergebnisse : bei allen patienten kam es nach der therapie zu einem absinken der psa - werte . 
die langfristige prognose in hinblick auf die biochemische rezidivfreiheit ist schlecht . schlsselwrter : prostatakarzinom prostatektomie lokalrezidiv dreidimensionale konformale radiotherapie introduction for men with clinically localized low - risk prostate cancer and at least a 10 - year life expectancy radical prostatectomy is an accepted and effective treatment modality . 
the introduction of prostate - specific antigen ( psa ) has revolutionized the postoperative management of these patients allowing detection of recurrent disease months to years before its clinical appearance . 
treatment options in patients with isolated psa failure include immediate radiotherapy for a presumed local recurrence [ 2 , 7 , 14 , 17 , 30 , 34 ] , radiotherapy for con1 department of radiation oncology , university hospital hamburg - eppendorf , hamburg , germany . received : september 9 , 2004 ; accepted : march 24 , 2005 strahlenther onkol 2005 no . 
 grade g1 g2 g3 pathologic stage pt2a pt2b pt3a pt3b pt4a pn0 pn1 results patients and methods between january 1992 and december 1998 , 24 patients were treated with three - dimensional conformal radiation therapy ( 3dcrt ) for confirmed local recurrence after radical retropubic prostatectomy for adenocarcinoma of the prostate . 
six patients were treated with neoadjuvant or adjuvant hormone therapy at the time of surgery . median age at the time of radiotherapy was 66 years ( range , 4674 years )  . 
the median dose was 64 gy ( range , 59.470 gy ) at the reference point following icru 50 [ 20 ] given in fractions of 1.8 gy five times per week . 
overall survival , disease - specific survival , biochemical control and local control were calculated using the product - limit kaplan - meier method [ 21 ]  . time ( months ) figure 1 . 
 local control initially , partial or complete remission at the site of local recurrence was documented in all patients using pelvic imaging with trus , ct and / or mri . 
local progression was defined as increase of the tumor after partial remission or local recurrence after complete remission documented by imaging for restaging at the time of second psa relapse . 
with trus , ct , or mri and bone scan the site of relapse was demonstrated in seven patients ( local progressions in four patients , one of them combined with distant metastases , and distant metastases in three patients )  . 
 author , year [ reference ] patients ( n ) verification of the recurrence radiation dose , median or range ( gy ) follow - up , median ( months ) wiegel et al . 
this is in accordance with most of the reported series ( table 2 )  . as in most of the published series , in 21 of our patients the target volume was restricted to the local recurrence including the prostatic bed [ 7 , 911 , 14 , 23 , 25 , 26 , 28 , 32 , 35 , 3941 ]  . 
considering the low toxicity of 3dcrt , a dose of 70 gy can be recommended for the treatment of local recurrence of prostate cancer diagnosed by imaging and / or biopsies . 
 [ 36 ] investigated the impact of prostatectomy on the definition of clinical target volume ( ctv ) , on the position of the bladder and rectum and the implication for 3dcrt . 
they could show a significant reduction of ctv , planning target volume ( ptv ) , and treatment volume with a consequent reduction of the portions of rectum and bladder for postprostatectomy radiotherapy in comparison to primary radiotherapy . 
on the other hand escalating the dose in postprostatectomy radiotherapy , dose - volume effects on sigmoid colon and small bowel as potentially dose - limiting organs should be taken into consideration . 
 [ 12 ] reported that in primary radiotherapy for prostate cancer parts of both organs are often in close vicinity to the ptv which results in small - volume high - dose effects . 
 [ 29 ] reported on 16 patients with biopsy - proven local recurrences treated with combined hdr brachytherapy with each two fractions of 15 gy to the local recurrence and percutaneous radiotherapy to the pelvis with 30 gy , 2 gy per fraction . 
health - related quality of life measurements for this method were reported for combined brachytherapy and percutaneous radiotherapy for primary tumors [ 16 ] , but not for salvage therapy after surgery . 
 [ 10 ] demonstrated that the predominant pattern of relapse for patients with salvage radiotherapy with clinically palpable and / or biopsy - proven local recurrence was a psa failure alone . 
however , it remains unsolved whether achieving local control in this group of patients translates into an improvement in overall and disease - free survival , including freedom from psa failure . biochemical control rates vary from 8% to 68% ( table 2 )  . 
an earlier series from our department with 20 patients treated between 1977 and 1991 showed a disease - free survival of 68% with a median follow - up of 45 months [ 41 ]  . 
also , some patients were treated in the pre - psa era . in high - risk prostate cancer patients it is well established that results obtained with primary radiotherapy can be improved , if radiation treatment is combined with hormonal therapy [ 5 , 6 , 33 , 34 ]  . 
at 5 years , biochemical control was 56% versus 27% in favor of the combined treatment . many groups have confirmed the importance of a low preradiotherapy psa as prognostic factor for biochemical control after salvage radiotherapy for a rising psa and proven local recurrence after prostatectomy [ 9 , 11 , 14 , 23 , 32 , 40 ]  . 
 other prognostic factors include the preoperative psa value [ 32 ] and psa doubling time [ 23 ] , time between surgery and radiotherapy [ 7 ] , and initial pathologic stage [ 25 , 32 ]  . 
however , long - term prognosis in terms of biochemical control with a rate of 38% at 5 years and a disease - specific survival of 67% at 5 years remains poor . 
 material and methods : the prostate and seminal vesicles of 13 patients treated with intensity - modulated radiotherapy for prostatic adenocarcinoma were retrospectively delineated by three radiation oncologists on ct only and on ct + mri in consensus reading with a radiologist . 
the volumes and margin positions were calculated and intermodality and interobserver variations were assessed for the clinical target volume ( ctv ) , seminal vesicles , prostate and three prostatic subdivisions ( apical , middle and basal third )  . 
 conclusion : addition of mri to ct in consensus reading with a radiologist results in a moderate decrease of the ctv , but an important decrease of the interobserver delineation variation , especially at the prostatic apex . 
 key words : prostate neoplasms therapeutic radiology computed tomography ( ct ) , comparative studies magnetic resonance ( mr ) , comparative studies diagnostic radiology observer performance conformal radiotherapy strahlenther onkol 2005 ; 181 : 42430 doi 10.1007 / s00066 - 005 - 1383 - x quantifizierung der interobserver - variation im ct im vergleich zur kombination ct und mrt bei intensittsmodulierter strahlentherapie ziel : quantifizierung der interobserver - variation bei der abgrenzung von prostata und samenblasen im ct im vergleich zur kombination ct und mrt nach einer konsensusbefundung mit einem radiologen . material und methodik : die prostata und die samenblasen von 13 patienten , die fr eine intensittsmodulierte strahlentherapie wegen adenokarzinoms der prostata vorgesehen waren , wurden retrospektiv im ct und mit der kombination ct und mrt durch drei strahlentherapeuten nach einer konsensusbefundung mit einem radiologen abgegrenzt . 
interobservervariationen fr das klinische zielvolumen ( ctv ) , die samenblasen , die prostata und drei prostatasegmente ( apikales , mittleres und basales drittel ) beurteilt . ergebnisse : mit der kombination von ct und mrt verringerte sich im vergleich zur alleinigen ct der mittelwert fr das ctv , prostataund samenblasenvolumen signifikant um 6 , 54% , 5 , 21% und 10 , 47% . 
die hchste variation wurde im apex der prostata festgestellt , gefolgt von der basis der prostata und den samenblasen . schlussfolgerung : die kombination von ct und mrt nach konsensus mit einem radiologen resultiert in einer bedeutenden abnahme der interobservervariation bei der anatomischen abgrenzung , insbesondere im bereich des apex der prostata , und zustzlich in einer moderaten verringerung des ctv . 
 schlsselwrter : prostataneoplasien strahlentherapie computertomographie ( ct ) , vergleichende studien kernspintomographie ( mrt ) , vergleichende studien diagnostische radiologie beobachterleistung konformale strahlen therapie 1 department of radiology , ghent university hospital , gent , belgium , 2 department of radiotherapy , ghent university hospital , gent , belgium . received : october 19 , 2004 ; accepted : april 26 , 2005 strahlenther onkol 2005 no . 
interobserver delineation variation using ct versus ct + mri introduction several authors have demonstrated that a higher radiation dose to the prostate is associated with improved local tumor control [ 12 , 20 , 25 , 27 ] , but at the price of a latent increase in normal tissue complication rate [ 14 ]  . 
with conformal or intensity - modulated radiation therapy ( imrt ) , it is possible to increase the radiation dose to the target volume while minimizing the dose to the surrounding normal tissues , by applying tightly constricted isodose lines around the target , thereby minimizing the risk of acute and late complications [ 2 , 5 , 8 , 10 , 13 , 16 , 17 , 23 ]  . 
the latter statement only holds true when these isodose lines are adequately placed around the target volume and therefore , accurate delineation of the clinical target volume ( ctv ) and surrounding tissues is crucial . 
these delineations are usually performed by radiation oncologists on ct images , in part because ct can easily produce tissue electron density values ( calculated from hounsfield units ) , which are required for dose calculations and to account for tissue inhomogeneities within the treatment volume [ 15 ]  . 
compared to ct , more anatomic information can be derived from mri due to its multiplanar imaging capability and its higher soft - tissue contrast on t2 - weighted images , resulting in detailed visualization of both the prostate and periprostatic structures [ 19 ]  . 
this advantage can be employed indirectly by using mri information to improve the delineation accuracy on ct images or by direct delineation on the mr images , using image segmentation and image registration or correlation to account for the lack of tissue electron density values on mri [ 11 , 15 ]  . 
 the aim of our study was to assess whether the additional anatomic information derived from mri in consensus reading with a radiologist could decrease the interobserver variation of prostate and seminal vesicle delineations on ct images , and in the given case , to quantify this effect with reference to prostatic anatomy . 
 material and methods between april 2000 and april 2003 , 187 patients were admitted to the radiotherapy department of ghent university hospital , belgium , to receive primary imrt for histologically proven localized adenocarcinoma of the prostate . 
observers 1 and 2 had < 5 years of experience in pelvic target delineation , whereas observer 3 had > 10 years of experience . all ct data were acquired on a helical ct scanner ( siemens somatom 4 + , siemens , erlangen , germany ) as previously described [ 5 ]  . 
the patients were instructed to drink 750 ml of dilute contrast medium ( 30 ml gastrografin [ schering , berlin , germany ] in 720 ml water ) the evening before and the morning of the ct scan procedure to increase the visibility of the small bowel and sigmoid colon . 
approximately 30 min before the ct scan procedure , all patients received a rectal laxative ( microlax , sanofi - winthrop , colomiers , france ) and were asked to drink an additional 300 ml of water . 
 this procedure ensures a comfortably filled bladder during treatment , in an attempt to keep as much small bowel loops away from the treatment field as possible [ 6 , 26 ]  . 
to further improve visualization of the bladder , 100 ml of intravenous iodinated contrast medium ( ultravist , schering ) was administered 10 min prior to the ct scan procedure [ 24 ]  . 
the ct data consisted of 10 mm thick contiguous sequential slices obtained in the supine position from the level of the umbilicus to a level 10 cm caudal to the testes . 
additional data on prostate , seminal vesicles and surrounding tissues were obtained using 2 mm ( n = 5 ) or 5 mm ( n = 8 ) thick contiguous slices from the superior border of both femoral heads to the distal border of the ischial tuberosity . 
5 - mm transverse , sagittal and coronal t2 - weighted turbo - spin echo images ( tr / te 4 , 000 / 99 ms , two signal averages , no interslice gap , 25to 40 - cm field of view [ fov ] , and matrix size of 330 512 ) of the pelvis were obtained . 
approximately 30 min before the mri scan procedure , all patients received a rectal laxative ( microlax , sanofi - winthrop ) and were asked to drink 300 ml of water , in order to attain a comfortably filled bladder . 
all patients were scanned in the same treatment position as described above , with the pelvis positioned in the isocenter of the magnet . both the ct and mr data were available on hard copy and the ct data were digitally transferred to a pinnacle3 computer workstation ( adac , philips medical systems , best , the netherlands )  . 
on every ct slice , contouring of the prostate and seminal vesicles was performed , first by a radiation oncologist without additional mri data nor the help of a radiologist . 
after an interval of at least 2 weeks , the same set of images was again delineated in a randomized order by the same radiation oncologist and with the addition of mri data in consensus reading with the radiologist , by transferring the mri information visually to the ct data set on the computer workstation , without image registration nor fusion . 
interobserver delineation variation using ct versus ct + mri radiologist were performed in a randomized order and with an interval of at least 1 month between each set of consensus readings . 
 the surface of the delineated prostate and seminal vesicles on each slice was calculated using the treatment planning system and this surface was multiplied with the interslice distance , yielding the respective volume in each slice . 
subsequently , the mean of these averages and their sds were calculated for both ctand mri - based volumes of the ctv , prostate gland , basal , middle and apical third and seminal vesicles . 
comparisons between ctand mri - derived values ( means or sd ) were represented in percentage decrease , defined as ( xctxmri ) / xct ; negative values indicated that the mri - derived value was larger than the corresponding ct - derived value . 
also , the dimensionless coefficient of variation ( % ) , defined as the ratio between the sd and the mean , was calculated to measure the relative scatter in data with respect to the mean . to quantify the modality - related delineation uncertainty of the observers , we calculated the delineation uncertainty ratio by slightly modifying a method introduced by rasch et al . 
it is defined as the ratio between the actually delineated volume on a given modality ( ct or mri ) and the ct / mri intersection volume ( the volume that was jointly delineated on both ct and mri )  . 
a large ratio means that a large amount of the actually delineated volume is discordant with the ct / mri intersection volume ( high degree of uncertainty ) , whereas a ratio of 1 means that the actually delineated volume equals the intersection volume ( low uncertainty )  . 
in two patients , however , the ct - based apical prostatic volume was very small because of discordant delineation in the lowermost aspect of the prostate , leading to an inappropriately small intersection volume and hence extremely outlying uncertainty ratios on mri . 
 besides variation in delineated volumes , variations in the position of the anterior , posterior , right , left , superior and inferior margins of the prostate were assessed and broken down into the three prostatic thirds . 
 the z - axis ( parallel to the body axis and perpendicular to the scan plane ) was defined at the intersection of a sagittal and a coronal plane through the cog . 
on each ct slice , the distance to the z - axis ( in mm ) of the anterior and posterior prostatic border in the sagittal plane and of the right and left prostatic border in the coronal plane to the z - axis was calculated . 
 furthermore , the distance between the superior and inferior border of the prostatic base and apex was determined by counting the number of delineated slices and multiplying it with the interslice distance . 
to compare ctand mri - derived differences , the mri - derived distances were subtracted from the corresponding ct - derived distances , a negative number indicating a larger mri - derived distance and vice versa . 
for the anteroposterior and mediolateral directions , the mean difference and sd of the three observer measurements per prostatic third were calculated . differences of the mean were considered in three categories : intramodality interobserver , intermodality intraobserver and intermodality all - observer variation . 
statistical significance testing of means in the first category was performed using the one - way analysis of variance for independent samples ( anova ) and students paired t - test in the other categories . 
 results the mean delineated volumes of the ctv , prostate , seminal vesicles , prostatic base , midprostate and prostatic apex per modality ( ct or mri ) and per observer are shown in figures 1 and 2 . 
we found no statistically significant intramodality interobserver differences of these mean delineated volumes both on ct or mri ( one - way anova ) , indicating that any intermodality differences could not be attributed to deviant delineations by one of the observers . 
 the addition of mri led to a significant intermodality intraobserver reduction of all delineated volumes in observer 1 , especially at the apical third ( paired students t - test )  . 
interestingly , the delineated prostate volume on ct was slightly smaller than on mri in the most experienced observer , largely because of an apparent underestimation of the middle third volume . 
 overall , we found a significant intermodality all - observer reduction of the mean delineated ctv volumes of 6.54% , consisting of a 5.21% reduction of the prostate mean volume and a 10.47% reduction of the seminal vesicle mean volume ( table 1 )  . 
when mri was used in addition to ct , we found a 63.06% reduction of the sd around the mean ctv volume , consisting of a 62.65% reduction of the sd around the mean prostate volume and a 44.83% reduction of the sd around the mean seminal vesicle volume ( table 1 )  . 
when the coefficient of variation was calculated ( sd / mean ) , a particularly high variation was found on ct at the level of the apical third ( table 1 )  . 
 the apical third of the prostate is the most problematic area for accurate delineation on ct , and a high coefficient of variation and uncertainty ratio were observed in our study . 
 the main reasons for this inaccuracy are the susceptibility of ct to partial volume averaging in the transverse plane and the inability of ct to discriminate the prostatic apex from surrounding tissues ( levator ani muscle , rectum , distal urethral sphincter and fibrous tissue in the urogenital diaphragm ) , because they all have similar attenuation coefficients . 
furthermore , the fibromuscular and glandular elements at the prostatic apex diffusely intermingle with one another , with the adjoining external urethral sphincter and surrounding fibrous tissue , further adding to the delineation uncertainty [ 3 ]  . 
it is therefore virtually impossible to ascertain which slice represents the lowermost part of the prostate , which was clearly illustrated by the high sd around its mean craniocaudal distance ( stated differently : a high interobserver variation in the number of delineated slices )  . 
because of its better soft - tissue contrast and its direct multiplanar image acquisition capability , mri can more reliably show the boundary between the high signal - intensity peripheral zone tissue and the low signal - intensity levator ani muscle , rectum , distal urethral sphincter and fibrous tissue in the urogenital diaphragcompared to the mean ct delineation , the mri delineation is somewhat narrower in the anteroposterior and mediolateral direction , but taller in the superior - inferior direction . 
more importantly : for an almost equal delineated apical third volume , we actually saw a halving of the mean sd around this mean and of the coefficient of variation and a considerable decrease of the uncertainty ratio . 
except for the anterior border , there was a significant near - halving of the mean sd around the mean position of the apical borders , all illustrating the impact of better visualization of the apical tissue on mri and corroborating previous findings at other institutions [ 1 , 4 , 7 , 9 , 18 , 21 , 22 ]  . the middle third is the least problematic . 
because of the presence of fatty tissue around the prostate , the prostatic margin may be clearly visible on ct , where low - density fat contrasts well with intermediate - density prostatic tissue . 
however , fat may not be sufficiently present in all patients , especially at the posterior boundary with the rectum and the anterior boundary with retzius space , which may be vague due to the presence of adjoining intermediate - density veins of santorinis venous plexus [ 9 ]  . 
because of a better contrast between the prostatic and surrounding tissues , the addition of mri results in a significant , although small , decrease of the mean delineated volume and , more importantly , an improvement of the delineation accuracy , as demonstrated by a decrease of the mean sd around both the mean midprostatic volume and the position of the midprostatic margins , especially the lateral borders . the basal third behaves on ct quite similar as the middle third , due to the presence of fatty tissue around the prostate . 
 however , just underneath the bladder , the anterolateral margins are more difficult to delineate because of partial volume averaging with the isodense overlying bladder wall ( which runs obliquely through the scan plane ) [ 7 ]  . 
because of a more apparent distinction between the isointense prostate and the hypointense bladder wall on the one hand and the hyperintense seminal vesicles on the other hand , the addition of mri to ct results in a significant decrease of the sd around the mean basal third volume and of the sd around the anterior and posterior mean position of the basal third borders , corroborating earlier findings by kagawa et al . 
interestingly , mri does not lead to a significant improvement of the cranial delineation accuracy , because the use of iodinated contrast material on ct already allowed excellent visibility of the prostatebladder transition and therefore rather straightforward identification of the uppermost part of the prostatic base ( unlike the situation at the prostatic apex )  . 
 although the seminal vesicles are generally surrounded by fatty tissue , their delineation on ct can be cumbersome because of the presence of the isodense deferent ducts medially and multiple plexular veins laterally . 
on mri , the seminal vesicles are usually visible as paired grape - like pouches filled with high signal - intensity fluid , as opposed to the low signal - intensity deferent ducts that traverse along their craniomedial sides [ 3 ]  . 
mri can therefore better separate the seminal vesicles from the deferent ducts and helps to more accurately delineate the most cranial portion of the ( fluid - filled ) seminal vesicles . 
the resulting effect is a significant decrease in the mean seminal vesicle volume and an improvement of the delineation accuracy , as demonstrated by a significant decrease of the mean sd and uncertainty ratio . 
 our results suggest that the main impact of the addition of mri to ct is a decrease of the delineation variation , rather than a decrease of the variation of mean margin positions or mean volumes . 
nevertheless , a moderate variation of prostate volume can be associated with only minor differences of margin position , because the volume of a spheroid object depends on the radius cubed . 
on the other hand , we believe that these differences are also a reflection of the large delineation variation on ct , more specifically a multiinstitutional variation , in which the magnitude of the difference largely depends on the ct delineation practice in a given center . 
in our hospital , we have been using mri in concordance reading with a radiologist for > 3 years and hence our observers had a prior knowledge derived from mri about the most likely boundaries of the prostate and seminal vesicles . 
this is illustrated by the fact that the prostate volume in our most experienced observer was even smaller on ct than on mri , contrary to what is commonly expected . 
 an important question that could be raised is to what extent the decrease in delineation variation might have been influenced by the cooperation of the same radiologist , who could have been able to remember previous delineations , thereby favoring a very low intraobserver variation on ct + mri . 
although we expected that this impact , if any , would have been equally true ( but in the opposite direction ) for each radiation oncologist , we chose to prevent any possible bias as much as possible , by using a randomized order of appearance of the strahlenther onkol 2005 no . 
furthermore , all ctvs were delineated by a radiation oncologist , not the radiologist : he was solicited to give advise about the mr information ( consensus reading ) , not to delineate . 
our results further plead against the hypothesis that the decreased delineation variation would be primarily influenced by the cooperation of the same radiologist rather than the additional use of mri . 
otherwise , we would have expected small and very similar sds and coefficients of variation around the means of delineated volumes ( table 1 ) and mean sds of prostatic margin positions ( table 4 ) throughout the prostate gland on ct + mri delineations . 
again , this was not the case ( table 2 ) , suggesting that differences were determined by ( mri - based ) anatomy , not by personal delineation consistency . the clinical implication of a reduced variation of organ delineation with the addition of mri in consensus with a radiologist is obvious . 
in a previous study , we showed that random prostatic movement as measured at the midprostatic level was 2.3 mm anteriorly , 3.2 mm posteriorly , 1.5 mm on the right side and 1.1 mm on the left side and 2.6 mm at the prostatic base and apex ( all values representing 1 sd ) [ 26 ]  . 
from the present study , we conclude that the delineation variabilities on ct exceed those of the random prostatic movement variabilities ( except the posterior and cranial margins ) , and that they significantly decrease when using mri in addition to ct , reaching values of only half the random variation . 
 strahlentherapie und onkologie original article radiation exposure of extracranial organs at risk during stereotactic linac radiosurgery mohammad maarouf1 , harald treuer1 , martin kocher2 , jrgen voges1 , andreas gierich1 , volker sturm1 background and purpose : stereotactic radiosurgery of intracranial tumors and vascular malformations can be performed by either a linear accelerator ( linac ) or gamma knife . 
the aim of this first study on patients was to determine the radiation exposure of organs at risk and assess the risk for late effects including secondary tumors and / or hereditary disorders after stereotactic linac radiosurgery . material and methods : thermoluminescent dosimetry ( tld ) measurements were done on 21 consecutively admitted patients with various intracranial lesions scheduled for linac radiosurgery . 
the tld chips were placed on the eyelid , thyroid , breast and the regions of the ovary or testes . results : the mean doses in organs at risk were 276 200 mgy ( eye lens ) , 155 83 mgy ( thyroid ) , 47 22 mgy ( breast ) , 20 12 mgy ( ovary ) , and 9 3 mgy ( testes )  . 
 conclusion : the absorbed doses to the extracranial organs at risk in patients undergoing linac radiosurgery were very low , ranging from 0.025% ( testes ) to 0.76% ( eye lens ) of the mean maximum target dose ( 36 gy )  . 
nevertheless , while the majority of radiosurgery patients have benign tumors or arteriovenous malformations and their life expectancy is long , all doses should be kept as low as reasonably achievable . 
this could be accomplished by the use of modern irradiation techniques including conformal beams with micro - multileaf collimator and avoiding beams directed to the trunk . key words : linac malignancy organs at risk radiation exposure radiosurgery tld strahlenther onkol 2005 ; 181 : 4637 doi 10.1007 / s00066 - 005 - 1391 - x strahlenexposition extrakranieller risikoorgane bei stereotaktischer linac - radiochirurgie hintergrund und ziel : die stereotaktische radiochirurgie zur behandlung intrakranieller tumoren und geffehlbildungen kann entweder am linearbeschleuniger ( linac ) oder am gamma - knife durchgefhrt werden . 
ziel dieser ersten studie am patienten war , die strahlendosen an extrakraniellen risikoorganen bei der stereotaktischen linac - radiochirurgie zu bestimmen und das potentielle risiko der entwicklung von strahlensptfolgen inkl . 
sekundrer tumoren und hereditrer erkrankungen nach einer stereotaktischen linac - radiochirurgie abzuschtzen . material und methodik : thermolumineszenzdosimetrische ( tld ) messungen wurden an 21 wegen unterschiedlicher hirnerkrankungen mittels linac - radiochirurgie konsekutiv behandelten patienten durchgefhrt . 
die tld - chips waren an augenlid , schilddrse , brustdrse , hodenund der eierstockregion angeklebt . ergebnisse : die mittleren gemessenen strahlendosen im bereich der risikoorgane betrugen 276 200 mgy ( augenlinse ) , 155 83 mgy ( schilddrse ) , 47 22 mgy ( brust ) , 20 12 mgy ( ovar ) und 9 3 mgy ( hoden )  . 
da die mehrheit der radiochirurgisch zu behandelnden patienten an gutartigen tumoren oder arteriovensen malformationen erkrankt ist und eine lange lebenserwartung hat , sind potentielle langzeit - strahlenfolgen durch den einsatz von mikro - multileaf - kollimatoren und vermeidung von einstrahlrichtungen entlang der krperachse zu minimieren . schlsselwrter : radiochirurgie risikoorgane sekundrtumor strahlenexposition tld 1 department of stereotactic and functional neurosurgery , university of cologne , cologne , germany , 2 department of radiation oncology , university of cologne , cologne , germany . received : november 4 , 2004 ; accepted : march 15 , 2005 strahlenther onkol 2005 no . 
linac radiosurgery : radiation exposure of organs at risk introduction so far , tens of thousands of patients all over the world have been treated with radiosurgery using a linear accelerator ( linac - ) based system or a gamma knife , and their number is steadily increasing . 
radiosurgery , a standard method for treating oncologic and vascular disorders of the brain such as brain metastases and arteriovenous malformations ( avms ) , consists of stereotactically guided , single application of highly focused percutaneous irradiation . 
precise stereotactic localization of the target point together with a steep dose gradient outside the target volume allows a high single - dose application to devitalize small , clearly bordered intracranial tumors and to occlude avms without damaging adjacent healthy tissue [ 14 ]  . 
 while many reports about the efficacy of this innovative method exist [ 5 , 8 , 11 , 13 , 1618 , 29 ] , only a small number deal with dosimetry [ 15 , 19 ] , including radiation exposure of sensitive organs during radiosurgery ( eye , thyroid , gonads , etc . ) and hence the possible induction of secondary malignancy or hereditary defects . 
the present paper gives the thermoluminescent dosimetry ( tld ) data of 21 consecutively admitted patients treated for various intracranial lesions using a linac - based radiosurgery syste material and methods measurements were done on 21 consecutively admitted patients with various intracranial lesions who were treated at our institution . 
 our radiosurgery technique involves up to ten non - coplanar rotation arcs using an adequately calibrated standard linac ( elekta sl 75 / 20 , 9 - mev beam energy , crawley , uk )  . 
 a different set of 24 supplementary circular collimators ( range 330 mm ) with a field size range of 4.545 mm ( leibinger , freiburg , germany ) was used with the linac secondary collimating jaws set to a field of 9 9 cthe technical data were published previously [ 10 , 23 ]  . 
 tld measurements ( tld 100 , harshaw chemical , cleveland , oh , usa ) were done during linac radiosurgery to estimate the energy doses absorbed by the organs at risk . 
the lithium fluoride ( lif ) tld chips were individually calibrated using a cobalt - 60 teletherapy device , then placed in individual thin - walled plastic bags and taped in pairs to the eyelid , thyroid , breast , testes and regions overlying the ovary . 
following linac radiosurgery , the tlds were preheated to 100 c and read with the automatic tld - reader ( model 5500 bicron , solon , oh , usa )  . 
absorbed dose did not differ significantly between the rightand the left - sided organs at risk except for the right eye lens due to the irradiation of more cases with tumors near the right orbital cavity . 
this can be well explained with the fact that both leakage irradiation from the linac head during arc irradiation , as well as the direct and scattered irradiation to the organs at risk decrease with a larger distance from the isocenter . 
 an analysis of other radiosurgical factors such as surface dose , maximum target dose , number of isocenters and target volume revealed no significant correlations between these and the doses in organs at risk . 
 discussion radiosurgery with a linac or gamma knife has become a standard method for treating clearly bordered intracranial tumors and avover the last 20 years > 200 , 000 patients were efficiently treated and with an extremely low rate of side effects . 
 for some indications ( e.g. , metastases and avms in critical brain areas , small vestibular schwannomas , meningeomas of the cavernous sinus ) radiosurgery is regarded as the method of choice or equivalent to surgery . 
in light of these facts , there is need to investigate if there might be a substantial risk for radiation - sensitive organs after low - dose exposure during radiosurgery . 
 the few studies dealing with this topic found out that the absorbed doses in extracranial organs at risk depend on factors such as maximum target dose , number of isocenters , target volume , number of arcs , and collimator size . 
comparing fiveand four - arc arrangements , they found that the sagittal arc contributed the greatest neck and trunk doses , with an up to fourfold increase in thyroid dose . 
a higher axis exit dose was also observed for the 40 - mm collimator , resulting in twice the mediastinal dose than that measured for the 20 - mm collimator . 
 table 2 shows that the absorbed doses in organs at risk during linac radiosurgery in our 21 patients are well comparable to the doses reported by gamma knife groups [ 2 , 21 , 31 ] and others using linac [ 24 ]  . 
the transportation dose received during gamma knife radiosurgery ( i.e. , the dose received while bringing the patient into and out of the treatment position ) is low but significantly higher than that received during radiosurgery with a linac . 
1988 [ 24 ] , linac ( phantom ) own data 2004 , linac ( 21 patients ) nevertheless , on average , the absorbed doses to the extracranial organs study 800 700 600 500 400 300 100 200 n = lens thyroid breast ovary testis organ at risk figure 1 . 
 at risk in patients undergoing linac or gamma knife radiosurgery were low , ranging from 0.055% ( ovary ) and 0.025% ( testes ) to 0.76% ( eye lens ) and 0.43% ( thyroid ) of the mean maximum target dose ( 36 gy )  . 
 eye lens thyroid breast ovary region testis 90 80 150 70 200 100 30 ( gonads ) 223 168 81 50 49 33 12 8 ( gonads ) 357 308 206 89 214 121 ( sternum ) 41 27 ( pelvis ) 100 30 10 ( gonads ) 277 200 155 84 47 23 20 12 9 3.6 strahlenther onkol 2005 no . 
 organ effects of radiation dose ( gy ) temporary sterility testes permanent sterility permanent sterility ovary radiation cataract lens of the eye excess mortality due to radiation induced cancer ( any organ ) , icrp 60 hereditary effects ( gonads ) ~ 4% / sv 0.5% / gy it is well known that ionizing radiation can cause lens cataract . 
a detailed analysis attached to the occurrence of cataract and factors associated with its development following whole - body irradiation and bone marrow transplantation was published [ 6 , 22 ]  . 
it has also been postulated that there is a threshold dose for the induction of detectable lens opacification in humans , which is about 2 gy for a single - dose exposure [ 9 , 26 , 30 ]  . the most radiation - sensitive extracranial organs which receive low doses during radiosurgery are the gonads , with spermatogenesis showing the highest susceptibility to radiation . 
however , the doses to the testes during radiosurgery are far below the above mentioned thresholds . in females , the oocyte as a resting differentiated intermitotic cell is less sensitive than the spermatogonium , but especially the mature oocytes are highly mutable [ 1 , 30 ]  . 
the doubling dose ( the gonadal dose that will double the spontaneous incidence of genetic mutations ) for a low - dose rate is 1 gy , as defined by the international commission of radiological protection ( icrp ) , and the estimated risk for radiation - induced genetic disorders in future generations is 0.5% per 1 gy parental exposure [ 28 ]  . 
 thus , the genetic consequences after linac radiosurgery should be estimated as extremely low . compared to conventional radiotherapy , radiosurgery with the combination of smaller target volumes and a steeply declining dose gradient probably leads to an incidence of secondary malignancies which is certainly significantly lower than that described following radiotherapy for pituitary adenoma [ 4 ]  . 
 the latency periods for radiation - induced tumors are different ; it takes on average 19 years for carcinomas , 13 years for sarcomas , and 8 years for leukemias [ 7 ]  . 
 nevertheless , while the majority of radiosurgery patients have benign tumors or avms and their life expectancy is long , long - term side effects are important , including those of radiation exposure of extracranial organs . 
die radikalen operationen wurden zunehmend von konservativen chirurgischen strategien verdrngt , so dass heute die brusterhaltende therapie ( bet ) mit nachfolgender homogenbestrahlung der brust ( wbrt [ whole breast radiotherapy ] ) bei karzinomen bis 3 cm gre standard ist [ 23 ]  . 
 dabei betrgt die standarddosis 4550 , 4 gy in einzeldosen von 1 , 82 , 0 gy , in definierten fllen gefolgt von einer rtlichen dosiserhhung am tumorbett , je nach rckfallrisiko , mit 1020 gy ( boost )  . 
auf die indikationen und durchfhrung einer lymphabflussbestrahlung [ 15 , 16 ] wird in unserem bericht nicht eingegangen . die abkehr von der radikalen chirurgie wurde durch die ergebnisse sorgfltig geplanter klinischer studien bewirkt , die eine quivalenz der brusterhaltenden operationen mit nachbestrahlung gegenber einer modifizierten radikalen mastektomie bezglich der lokalen kontrolle und des gesamtberlebens nachwiesen [ 2 , 79 , 30 , 41 ]  . 
die homogenbestrahlung der ganzen brust ( wbrt ) plus boost senkt dabei das risiko fr ein intramammres rezidiv auf etwa ein viertel gegenber der alleinigen brusterhaltenden operation ohne nachbestrahlung ; d.h. , die rate an intramammren rezidiven innerhalb von 810 jahren liegt nach alleiniger operation und ggf . 
whrend die sinnhaftigkeit einer chemound hormontherapie kaum je zur diskussion gestellt wird , obwohl auch hier nur ein kleiner teil der frauen profitiert , wurde die rechtfertigung der routinemigen wbrt , die heute allen patientinnen nach brusterhaltender operation angeboten wird , immer wieder hinterfragt . 
alle anstze verliefen jedoch bisher im sinne der fraschlsselwrter : experimentelle therapie multikatheter - technik externe strahlentherapie 3 - d ballonkatheter intraoperative bestrahlung intrabeam klinische studien key words : experimental treatment multicatheter technique external beam 3 - d mammosite iort / ioert intrabeam clinical studies strahlenther onkol 2005 ; 181 : 41723 doi 10.1007 / s00066 - 005 - 5701 - 0 1 universittsklinikum erlangen , 2 universittsklinikum mannheim , 3 st . 
selbst bei lteren patientinnen mit hormonrezeptorpositiven tumoren , die < 1 cm im durchmesser waren , traten trotz zustzlicher tamoxifentherapie bereits innerhalb von 8 jahren in 1516 , 5% der flle lokalrezidive auf [ 10 , 12 ]  . 
in keiner prospektiven studie und bei keiner subgruppenanalyse konnten bisher kriterien definiert werden , die einen verzicht auf eine bestrahlung nach brusterhaltender operation rechtfertigen wrden . aufgrund der beobachtung , dass die berwiegende mehrzahl der in - brust - rezidive nach bet im bereich des tumorbetts auftritt [ 3 , 9 , 18 , 35 , 41 ] und die distant hierzu sich in derselben brust entwickelnden karzinome hufig als zweittumoren ( second primaries [ 19 ] ) gedeutet werden , wurde die hypothese formuliert , dass es patientinnen geben knnte , die mit einer teilbrustbestrahlung ausreichend behandelt sind . 
dies wird derzeit in verschiedenen klinischen studien gepr dabei werden ganz unterschiedliche konzepte und techniken eingesetzt [ 1 , 13 , 2022 , 24 , 2629 , 36 , 38 , 39 , 4248 ]  . 
multikathetertechnik im ldr - , pdroder hdrverfahren [ 21 , 2729 , 36 , 44 ] , die dreidimensionale konformale perkutane strahlentherapie [ 1 , 11 , 47 ] , die ballonkathetertechnik ( proxima - katheter ) mit dem sog . 
mammosite [ 14 , 20 ] , die intraoperative radiotherapie mit elektronen ( ioert ) eines linearbeschleunigers [ 13 , 26 , 27 , 42 , 43 ] und das intrabeam , eine anlage mit 50 - kv - rntgenstrahlen [ 22 , 38 , 39 ]  . 
sowohl die rationale als auch die technik der teilbrustbestrahlung , die die wbrt ersetzen soll , beruht im wesentlichen auf den erfahrungen , die mit diesen methoden im rahmen einer boostbestrahlung gewonnen wurden , z.b. 
interstitielle multikathetertechnik bei der klassischen multikatheter - brachytherapie werden 612 wochen nach bet mehrere dnne plastikkatheter in paralleler geometrie in das tumorbett mit einem 20 mm breiten sicherheitssaum an umgebendem gesundem gewebe , dem zielvolumen entsprechend , eingefhrt . 
fr gewhnlich wird in zwei oder drei ebenen implantiert , mit einem abstand von jeweils 10 m die bestrahlung selbst erfolgt in afterloading - technik mit entweder hoher dosisleistung ( hdr , 32 gy in acht fraktionen 4 gy oder 30 , 1 gy in sieben fraktionen 4 , 3 gy , zwei fraktionen tglich ) oder als pdr - brachytherapie ( ein puls 0 , 60 , 8 gy / h , 24 h pro tag , gesamtdosis 50 gy )  . 
 ( cid : 127 ) die groe flexibilitt der methode gestattet , ein tumorbett nahezu jeder form und gre individuell konformiert mit der tumorbiologisch notwendigen dosis zu belegen und das brige brustdrsengewebe und die haut zu schonen . 
verschiedene phase - iund - ii - protokolle zeigten , dass bei einem selektionierten patientengut gleiche tumorkontrollraten beim frhen mammakarzinom erzielt werden knnen wie mit der konventionellen perkutanen wbrt [ 21 , 27 , 29 , 36 , 44 ]  . 
heute fordern wir im rahmen von studien fr die teilbrustbestrahlung mit der multikathetertechnik folgende restriktive einschlusskriterien : ( cid : 127 ) tumorgre 3 cm ( kein bilaterales oder zweitkarzinom ) ; ( cid : 127 ) unifokaler tumor ( keine multifokalitt oder multizentrizi ( cid : 127 ) tumorfreie resektionsrnder mit einem minimalen sicherheitsabstand von > 2 mm ( keine gefinvasion ) ; ( cid : 127 ) invasive duktale karzinome ( kein paget - karzinom , keine hautinfiltration , keine extensive intraduktale komponente [ eic ] ) oder ( cid : 127 ) limitiertes dcis ( van nuys prognostic index [ 34 ] : < 8 von tt ) ; 12 ) ; ( cid : 127 ) niedriges tumorgrading ( g1 und 2 ) ; ( cid : 127 ) negativer axillrer lymphknotenstatus ( pn0 oder pnmi ) ; ( cid : 127 ) keine lymphangiosis carcinomatosa ( l0 ) ; ( cid : 127 ) strogenund progesteronrezeptorpositivitt ; ( cid : 127 ) alter 40 jahre . 
 gegenwrtig prft die european brachytherapy breast cancer working group der gec - estro , ausgehend von erlangen , leipzig , rostock und wien , in einer internationalen phase - iii - studie die rechtfertigung , also effektivitt und vertrglichkeit , der alleinigen brachytherapie im vergleich mit der herkmmlichen wbrt bei einem nach den oben angegebenen einschlusskriterien selektionierten patientengut [ 27 , 29 , 36 , 49 ]  . 
 so lange , bis diese oder hnliche studien nicht abgeschlossen sind und ber eine mehrjhrige nachbeobachtungszeit verfgen , kann die interstitielle teilbrustbestrahlung nicht fr die tgliche klinische praxis empfohlen werden . 
ballonkathetertechnik ( mammosite ) mit dem ballonkatheter steht neuerdings auch eine sehr einfache , allerdings von vornherein standardisierte und nicht individualisierbare brachytherapietechnik fr die intrakavitre teilbrustbestrahlung nach brusterhaltender operation zur diskussion . 
dem stehen allerdings gewichtige probleme gegenber : ( cid : 127 ) wenn die behandlung intraoperativ begonnen wird , liegen zum zeitpunkt der katheterimplantation noch keine kenntnisse ber die tumorcharakteristika , den resektionsund axillren lymphknotenstatus vor . 
 ( cid : 127 ) das bestrahlungsvolumen und die dosimetrie sind standardisiert , also nicht den individuellen erfordernissen , die sich beispielsweise aus der weite der resektionsrnder ergeben , anzupassen . 
 ( cid : 127 ) die therapeutische reichweite ist mit 10 mm zu kurz , da auch auerhalb eines sicherheitssaums von 1020 mm noch ein substantielles rezidivrisiko von bis zu 50% je nach tumorcharakteristik besteht [ 2 , 3 , 18 , 35 ]  . 
 ( cid : 127 ) in der rigiden kugelfrmigen dosisverteilung liegt auch die gefahr fr ein ungnstiges kosmetisches ergebnis , weil es zu unbeabsichtigten berdosierungen im bereich der haut kommen kann . 
 die schon kurz nach der einfhrung des systems berichtete inzidenz von akuten und chronischen nebenwirkungen scheint hher als bei der multikathetertechnik zu sebisher untersuchte nur eine studiengruppe die durchfhrbarkeit an 43 patientinnen in einer phase - i - studie [ 20 ]  . 
es liegen also zur alleinigen teilbrustbestrahlung mit der ballonkathetertechnik weder eine randomisierte studie noch aussagekrftige daten vor , die deren einsatz auerhalb von klinischen studien oder gar im routinebetrieb rechtfertigen wrden . 
 erst im herbst 2004 initiierte die nsabp eine prospektive , randomisierte multicenterstudie , die die alleinige teilbrustbestrahlung mit hilfe der multikathetertechnik oder der ballonkathetertechnik mit der konventionellen perkutanen wbrt vergleicht . 
die intention fr diese verfahren entspringt der richtigen einschtzung , dass die strahlentherapie des tumorbetts ohne verzgerung sofort nach dem brusterhaltenden operativen eingriff erfolgen sollte und dass mit einer intraoperativen radiotherapeutischen manahme die applikation einer hohen , zielgerichteten dosis in einem begrenzten volumen ohne wesentliche belastung kritischer strukturen grundstzlich mglich ist . 
 [ 5 ] stellten 1989 die ioert mit elektronen als boost vor der homogenbestrahlung der restbrust vor ; erste langzeitresultate wurden 1997 gemeinsam mit einer franzsischen arbeitsgruppe verffentlicht [ 6 , 25 ]  . 
in mailand kam ab 1999 ein speziell fr die ioert entwickelter mobiler elektronenbeschleuniger ( novac7 ) zum einsatz , der energien von 312 mev liefert [ 13 , 26 , 42 ]  . 
 ioert als ausschlieliche teilbrustbestrahlung nach der oben erwhnten pilotphase , in der die ioert als boost eingesetzt wurde , ging man in mailand dazu ber , intraoperativ hhere einzeitdosen bis 22 , 3 gy zu applizieren und auf die perkutane homogenbestrahlung der restbrust als postoperative manahme zu verzichten . 
die gruppe fordert eine r0 - resektion und einen zustzlichen sicherheitsabstand von > 10 m nach mobilisierung des drsenkrpers vom pektoralismuskel wird vor der bestrahlung eine blei - platte zwischen brustdrsengewebe und muskel eingebracht , um rippenoder brustwandnekrosen zu vermeiden . 
 aus unserer sicht seien zu dem verfahren aber doch folgende kritische punkte angemerkt : ( cid : 127 ) zum zeitpunkt der ioert liegt keine definitive information ber die beschaffenheit der resektionsrnder , die tumorcharakteristika und den lymphknotenstatus vor , was die patientenselektion erschwert . 
 ( cid : 127 ) die prparation aller parenchymanteile , die potentiell subklinische tumoranteile tragen , und deren zentrierung in das bestrahlungsfeld erfordern besondere chirurgische und radioonkologische expertise , vor allem wenn keine weitere bestrahlung der brust geplant ist . 
 ( cid : 127 ) bei der verwendung von elektronentuben ist zu beachten , dass sich der von der referenzdosis abgedeckte bereich in der tiefe verschmlert ( einschnrung der 80% - isodose ) , d.h. , es besteht die gefahr , dass die erforderliche breite des elektronentubus in der klinischen routine in bezug auf das zielvolumen zu klein bemessen wird . 
 trotzdem sind die bisherigen erfahrungen mit der ioert im european institute of oncology in mailand als alleinige apbi [ 13 , 26 , 42 , 43 ] und in salzburg als antizipierter boost [ 31 , 33 ] ermutigend . 
 dieses system wirft , als alleinige intraoperative therapiemanahme eingesetzt , eine reihe kritischer fragen auf : ( cid : 127 ) zur zeit der intraoperativen bestrahlung kennt man die pathohistologischen risikofaktoren noch nicht : breite der resektionsrnder , tumorcharakteristika , ausma eines eventuellen carcinoma in situ , lymphknotenund rezeptorstatus . 
 ( cid : 127 ) wie die ballonkathetertechnik ermglicht auch das intrabeam lediglich eine starre , kugelfrmige bestrahlung der resektionsrnder ohne individuelle dosisanpassung an die breite der individuellen resektionsrnder bzw . 
ermutigt von diesem resultat wurde in grobritannien , australien , den usa und deutschland im jahr 2000 eine internationale randomisierte targit - studie begonnen , die die frage prft , ob bei patientinnen nach einer die brust erhaltenden operation eine einmalige intraoperative bestrahlung prognostisch gleichwertig mit einer konventionellen perkutanen postoperativen wbrt ist . 
die randomisierung erfolgt in einen iortoder den standardar ergibt die endgltige pathohistologische aufarbeitung des operationsprparats jedoch einen risikofaktor ( tumorgre > 2 cm , freier schnittrand < 1 cm , eic > 25% des tumorvolumens , eine lymphangioinvasion [ l1 ] oder eine andere histologie ) , folgt nach der iort grundstzlich eine perkutane wbrt mit 46 gy . 
erste ergebnisse knnen wohl frhestens im jahr 2007 erwartet werden . diskussion prinzipiell ist es wissenschaftlich wnschenswert , innovative therapieoptionen in randomisierten studien zu prfen , sofern sie von der rationale her ein substantielles verbesserungspotential primr hinsichtlich kuration und sekundr hinsichtlich ihres nebenwirkungsprofils erwarten lassen . 
 die idee , durch eine teilbrustbestrahlung nebenwirkungen , vor allem im sinne einer kosmetischen beeintrchtigung durch eine homogenbestrahlung der brust , zu vermeiden , wird in zeiten der dreidimensional geplanten konformalen strahlentherapie mit zunehmend vermeidbaren strahlenreaktionen und berwiegend exzellenten kosmetischen ergebnissen deutlich relativiert . 
auch das vielfach ins feld gefhrte argument , die teilbrustbestrahlung knne solchen frauen die brust retten [ 39 ] , die sich anderenfalls einer ablatio unterziehen wrden , da sie sich eine fraktionierte strahlentherapie zeitlich und finanziell nicht leisten knnten [ 32 ] , hat in unserem gesundheitssystem bislang keine gltigkeit . 
die latenz bis zum auftreten von radiogenen sptfibrosen betrgt in 90% der flle 4 , 7 jahre [ 4 ] , also eine zeitspanne , die mit der nachbeobachtungszeit der meisten studien zur teilbrustbestrahlung noch lngst nicht erreicht ist . angreifbar ist auch die argumentation eines der prominentesten frsprecher der teilbrustbestrahlung und mitinitiators der targit - studie , j.s. 
spter schloss sie aber aus der tatsache , dass 90% der rezidive klinisch im ursprnglich befallenen quadranten auftreten , dass solche distanten herde klinisch irrelevant seien und man sich deshalb in vielen fllen auf die bestrahlung der eigentlichen tumorregion beschrnken knne [ 38 ]  . 
diese berlegung ist schon deshalb unzutreffend , weil distante tumorherde deshalb klinisch nicht mehr in erscheinung treten , weil ein manifestes rezidiv im betroffenen quadranten bereits zur ablatio gefhrt hat . 
dies gilt umso mehr , als neuere strahlenbiologische vergleichsuntersuchungen zweifel daran aufkommen lassen , ob die biologisch effektive dosis einer apbi berhaupt einer konventionell fraktionierten homogenbestrahlung entspricht [ 32 ]  . 
 die definitive teilbrustbestrahlung nach brusterhaltender operation unter verzicht auf die homogenbestrahlung der brust ist derzeit als experimentelle therapie einzustufen , auch bei patientinnen mit sehr niedrigem risiko , nmlich bei lteren frauen mit gnstigen prognosefaktoren . 
bei allen diskutierten verfahren interstitielle multikathetertechnik , dreidimensionale konformale perkutane strahlentherapie , ballonkathetertechnik ( mammosite ) sowie intraoperative bestrahlungen mit elektronen ( ioert ) oder mit dem intrabeam handelt es sich um eine apbi , deren biologische effektivitt , nebenwirkungsund chronische komplikationsrate noch nicht abzuschtzen sind . 
7 urban & vogel strahlentherapie und onkologie original article the cfse distribution assay is a powerful technique for the analysis of radiation - induced cell death and survival on a single - cell level franz rdel1 * , sandra franz2 * , ahmed sheriff2 , udo gaipl2 , petra heyder2 , guido hildebrandt3 , stefan schultze - mosgau4 , reinhard e . 
voll2 , martin herrmann2 background and purpose : to analyze radiation sensitivity of cells and to monitor cellular responses to irradiation , sensitive test systems for cell death and proliferation on a single - cell level are required . 
here it is reported , that labeling of cells with 5 - ( and 6 - ) carboxyfluorescein diacetate succinimidyl ester ( cfdase ) can be used as a highly sensitive assay to determine cellular response toward irradiation on a single - cell level . 
 material and methods : the human malignant cell lines u937 ( myelomonocytic , nonadherent ) , sw48 and sw480 ( colorectal , adherent ) were labeled with cfdase , irradiated with either uvb ( 0540 mj / cm2 ) , or x - rays ( 016 gy )  . 
cell death and proliferation were monitored by cytofluorometry and compared to the clonogenic assay for adherent sw48 and sw480 cells . results : dividing nonadherent u937 cells displayed a shift in carboxyfluorescein ( cf ) fluorescence in parallel with an increased cell count indicating cell proliferation . 
calculating the number of cell divisions it was observed that the nonirradiated cells underwent approximately six cell divisions within 7 days , whereas the irradiated cells divided only once on average . 
the adherent sw480 colorectal cells showed a more pronounced cell - cycle arrest after irradiation with 240 mj / cm2 uvb as compared to cells treated with x - ray up to 16 gy . 
 conclusion : analysis of cf distribution can be employed as a powerful add - on to the clonogenic assay to simultaneously monitor cellular responses toward irradiation on a single - cell level . 
hier wird gezeigt , dass die markierung von zellen mit 5 - ( und 6 - ) carboxyfluorescein - diacetat - succinimidyl - ester ( cfdase ) eine sensitive methode fr die bestimmung der zellulren antwort nach bestrahlung auf einzelzellebene darstellt . material und methodik : die humane zelllinien u937 ( myelomonozytisch , nichtadhrent ) , sw48 und sw480 ( kolorektal , adhrent ) wurden mit dem farbstoff cfdase markiert und mit uvb ( 0540 mj / cm2 ) oder rntgenstrahlen ( 016 gy ) bestrahlt . 
die ergebnisse wurden mit einem koloniebildungstest fr adhrente sw48 und sw480 verglichen . * both authors contributed equally to this work . 1 department of radiooncology , university of erlangen - nuremberg , erlangen , germany , 2 institute of clinical immunology and rheumatology , department of internal medicine iii , university of erlangen - nuremberg , erlangen , germany , 3 department of radiotherapy and radiooncology , university of leipzig , leipzig , germany , 4 department of oral and maxillofacial surgery , university of erlangen - nuremberg , erlangen , germany . received : september 9 , 2004 ; accepted : march 24 , 2005 strahlenther onkol 2005 no . 
single - cell proliferation assay ergebnisse : sich teilende , nichtadhrente u937 - zellen zeigten eine verschiebung der carboxyfluorescein - ( cf - ) fluoreszenz und einen anstieg der messereignisse als zeichen der zellproliferation . 
to analyze radiation sensitivity of cells and to monitor cellular responses to irradiation , sensitive test systems for cell death and proliferation on a single - cell level are required . 
traditionally , cellular radiation survival and chemosensitivity are measured using the clonogenic assay as the gold standard [ 1 , 3 , 4 , 8 , 14 , 21 , 24 ]  . 
therefore , several alternative , nonclonogenic methods have been developed monitoring thymidine uptake , dye exclusion and metabolism of mtt to analyze responses to radiation [ 1 , 8 , 14 , 17 , 19 , 20 ]  . 
approximately 10% of the cf couples to intracellular macromolecules ( r - nh2 ) to form long - lived fluorescent conjugates ( cf - nhr ) that cannot escape from the cell . 
the cf labeling is therefore frequently used in studies of cell migration , cell death , and phagocytosis [ 2 , 5 , 9 , 1012 ]  . when weston & parish first used cfdase as a long - term tracking dye [ 23 ] , they did not anticipate that it could be used to monitor cell proliferation . 
however , a major advantage of cf - labeled cells is that they can be used to analyze cell division , since the dye is evenly distributed to the progenies resulting in halving of the fluorescence intensity after each division . 
here we report , that cfdase labeling and analysis of cf distribution can be used as a highly sensitive assay to determine cellular response toward both ionizing and uv irradiation on a single cell level and displays a powerful add - on to the clonogenic survival assay . 
 material and methods cells and cell culture the human malignant cell line u937 ( myelomonocytic ) was maintained in rpmi 1640 medium supplemented with 10% heat - inactivated fetal calf serum ( fcs ) , 1% glutamine , and 1% penicillin - streptomycin ( all gibcobrl , eggenstein , germany )  . 
cells were cultured in dulbeccos modified eagles medium ( dmem ) supplemented with 10% heat - inactivated fcs , 1% sodium pyruvate , 2 mm glutamine and 1% penicillin - streptomycin ( all biochrom , berlin , germany ) at 37 c , 5% co2 , and 95% humidity . 
the cultured cells were routinely checked for mycoplasma contamination . irradiation procedure sw48 , sw480 and u937 cells , plated at a density of 35 106 / culture flask were irradiated at room temperature using orthovoltage irradiation ( stabilipan , siemens , munich , germany ) at 250 kv / 15 ma 40 cm focus - surface distance at a dose rate of 1.15 gy / min with single doses ranging from 2 to 16 gy . 
in addition , cells plated at 1 106 ml1 in flat - bottom 24 - well tissue culture plates were irradiated with 3 mj cm2 s1 of uvb ( 60540 mj cm2 )  . 
 dye distribution was monitored with an epics - xl flow cytofluorometer ( coulter , hialeah , fl , usa ) equipped with a 15 - mw argon laser , tuned to 488 nm and standard sets of filters for green ( fl - 1 ) and red ( fl - 3 ) fluorescence . 
the validity of the gating was confirmed by staining with annexin v in a separate set of experiments ( not shown )  . the number of cell divisions was calculated by assuming that the dye of the mother cells is equally distributed to both daughters , resulting in a halving of the fluorescence intensity . clonogenic survival assay the clonogenic assay was performed on single - cell suspension of exponentially growing cells . 
cells were counted using a coulter counter ( casy1 , schrfe system , reutlingen germany ) , plated in growth medium into petri dishes and were irradiated 12 h after plating . 
after 1014 days cells were stained with methylene blue solution for 30 min ; colonies > 50 cells were counted using an automatic colony - analyzing machine ( acam )  . 
next , calculation of survival fractions ( sf ) was performed using the equation sf = colonies counted / cells seeded ( pe / 100 ) , taking the individual plating efficieny ( pe ) into consideration . 
 results cfdase labeling to distinguish irradiated from nonirradiated cells in a mixed cell culture labeling with cfdase of both adherent sw480 and nonadherent u937 cells was engaged to study cell - cycle arrest and division after irradiation . 
in this assay , cf fluorochrome is evenly distributed to cell progenies during mitosis , enabling tracing of cells and cell proliferation in biological composites . first , myelomonocytic u937 cells were uvb - irradiated , subsequently mixed with nonirradiated cells ( irradiated cell to nonirradiated cell ratio 20 : 1 ) and subjected to cytofluorometric analysis on day 0 , 2 , 4 , and 7 after irradiation . 
nontreated , dividing controls displayed a shift in cf fluorescence in parallel with an increased cell count indicating cell proliferation within the 7 - day observation period ( left panel )  . 
by comparison , irradiated u937 cells did not show a shift in cf fluorescence and an increase in cell count ( right panel ) indicating no proliferation due to cell - cycle arrest . 
 cf staining to discriminate dead and viable cells and analyze cell divisions in a mixed population the fsc and ssc can be used to discriminate between dying and viable cells . 
when 10 , 000 nonirradiated cells , 200 , 000 irradiated cells , or a mixture of both were cultured for 7 days in 1 ml of medium , both populations grew up to approximately 400 , 000 cells / ml . 
as shown in figure 2 , the nonirradiated cells displayed a viable morphology ( fsc / ssc ) and had lost most of the initial fluorescence ( second lane )  . 
calculating the number of cell divisions by assuming that the dye of the mother cells is equally distributed to both daughters , we observed that the nonirradiated cells underwent approximately six cell divisions within the observation period of 7 days , whereas the irradiated cells divided only once on average ( figure 3b )  . 
 determination of cell division rates following irradiation with uvb and x - rays from cf fluorescence next , dye distribution was monitored in sw480 colorectal cells following irradiation with either uvb ( 0540 mj / cm2 ) or x - ray ( 016 gy ) and cell division rates were calculated from cytofluorometry data . 
in nontreated cells , eight cell divisions were detected within the observation period of 140 h when the cells reached a plateau due to high confluence ( figure 4 )  . 
 most intriguingly , the effect on cell proliferation and cell divisions was more pronounced in sw480 colorectal cells irradiated with > 240 mj / cm2 uvb , as compared with cells treated with x - ray up to 16 gy . 
after two to three divisions in a 60 - h culture period , cells treated with > 240 mj / cm2 showed no cell division within the following 120 h , whereas x - ray - treated cells went on dividing , although at significantly reduced rates ( figure 4b )  . count count count count log cfse log cfse log cfse log cfse count count count log cfse log cfse log cfse figure 2 . 
10 , 000 cf - stained nonirradiated u937 cells and 200 , 000 uvb - irradiated ( 540 mj cm2 ) cf - stained u937 cells , or a mixture of both were cultured for 7 days and subjected to cytofluorometry ( fourth lane )  . 
pure cultures of nontreated cf - stained cells at day 0 ( first lane ) and day 7 ( second lane ) or uvb - irradiated cf - stained cells ( third lane ) served as controls . 
 10 000 unbestrahlte , cf - markierte zellen und 200 000 uvb - bestrahlte ( 540 mj cm2 ) , markierte zellen wurden in einer gemischten zellkultur fr 7 tage kultiviert und anschlieend durchflusszytometrisch analysiert ( vierte reihe )  . 
alleinige kulturen von unbestrahlten , cfmarkierten zellen an tag 0 ( erste reihe ) und tag 7 ( zweite reihe ) oder uvb - bestrahlten , markierten zellen ( dritte reihe ) dienten als kontrolle . 
a time - dependent decrease of mean cf fluorescence ( a ) and increase in cell division rates ( b ) were observed in mock - irradiated u937 cells as compared to uvb - irradiated cells or the mixed population . 
eine zeitabhngige abnahme der mittleren cf - fluoreszenz ( a ) und ein anstieg der zellteilungsrate ( b ) knnen bei nicht bestrahlten u937 - zellen im vergleich zu uvb - bestrahlten zellen oder der gemischten zellkultur beobachtet werden . 
 cfse distribution and clonogenic assay discriminate between cells of different intrinsic radiosensitivities sw48 and sw480 colorectal cells were labeled with cfdase and subjected to cytofluorometric analysis on day 0 , 1 , 3 , 6 , and 7 after irradiation or were used in parallel in a clonogenic survival assay . 
irradiation of both sw48 and sw480 resulted in a time - dependent decrease of the dividing rates as determined by the cfse staining , with a more pronounced proliferation block at day 3 after irradiation in the radiosensitive line sw48 as compared to sw480 ( figure 5b )  . 
therefore , both techniques clearly distinguished between cell lines of different intrinsic radiosensitivities and complemented each other in the determination of early ( cfse ) and late effects of ionizing radiation . 
single - cell proliferation assay ( cfdase ) and carboxyfluorescein diacetate ( cfda ) , were shown to be suitable for accumulation and staining of viable cells without compromising their functional properties [ 2 , 5 , 23 ]  . 
it is possible to follow up to ten cell divisions by flow cytometry [ 16 , 18 ]  . the classic colony - forming assay used for decades as the gold standard in radiation research provides information on cell division and clonogenic survival . 
furthermore , alternative methods like thymidine uptake , cell counting , bromo - desoxy - uridine ( brdu ) labeling , or the mtt assay can quantify overall cell division , and viability , but do not record the division history of an individual cell [ 14 , 15 , 19 , 20 ]  . here , we present the cfse dye distribution assay to our knowledge not yet introduced in the field of radiation research . 
cfdase labeling allows the discrimination of an irradiated population in mixed cellular composites and is suitable for adherent sw480 ( figure 4 ) as well as nonadherent cells as exemplified for uvb - irradiated u937 cells ( figure 1 )  . 
in addition , the method can easily be combined with surface and intracellular immune staining . ionizing radiation is known to have essentially three main effects on cellular survival : ( 1 ) reduced proliferation rate , ( 2 ) abortive divisions of inactivated cells , and ( 3 ) loss of unlimited proliferation , with the last criteria being the most essential to cancer cure by radiotherapy . 
the capability of a single cell to grow into a visible colony of > 50 cells as determined by the colony - forming assay is a convenient proof that it has retained its productive integrity . 
cell division rates as calculated from the fluorescence data of a cfse dye distribution assay at 0 , 1 , 3 , 6 , and 7 days after irradiation ( b )  . 
single - cell proliferation assay acknowledgments this work was supported in part by a grant of the staedler foundation , nuremberg , and the interdisciplinary center for clinical research ( izkf ) at the university hospital of the university of erlangen - nuremberg : project b 28 , the research training grant grk 592 from the german research society ( dfg ) to s.f. , and by the european commission : e.u. 
 ( qlk3 - ct - 2002 - 02017 apoclear )  . strahlentherapie und onkologie original article comparative treatment planning on localized prostate carcinoma conformal photonversus proton - based radiotherapy ulrike mock1 , joachim bogner1 , dietmar georg1 , thomas auberger2 , richard ptter1 purpose : to assess the potential benefit of proton - beam therapy in comparison to 3 - d conformal photon therapy and photon - based intensity - modulated radiotherapy ( imrt ) in prostate carcinoma for various stages of disease . material and methods : in five patients a 3 - d conformal proton - based ( two lateral beams ) irradiation technique was compared with 3 - d conformal photon - beam radiotherapy ( four - field box ) and imrt ( seven beams )  . 
dose - volume histograms ( dvhs ) were analyzed for the different ptvs and various organs at risk ( oars ) , i.e. , rectal wall , bladder , both femoral heads . 
in comparison to conformal 3 - d treatments imrt reduced doses to oars in the medium dose range , especially for the rectal wall . conclusion : imrt enabled dose reductions to oars in the medium dose range compared to 3 - d conformal radiotherapy . 
the advantageous dose distribution of proton - beam therapy for prostate cancer may result in reduced side effects , which needs to be confirmed in clinical studies . key words : prostate carcinoma proton therapy imrt treatment planning strahlenther onkol 2005 ; 181 : 44855 doi 10.1007 / s00066 - 005 - 1317 - 7 vergleichende bestrahlungsplanung beim lokalisierten prostatakarzinom : konformale photonenversus protonengesttzte radiotherapie ziel : im rahmen einer planungstechnischen studie wurde fr die behandlung des primren prostatakarzinoms die dosisverteilung einer konformalen protonentechnik mit intensittsmodulierten ( imrt ) und konformalen photonentechniken verglichen und analysiert . material und methodik : bei fnf patienten wurde eine konformale zwei - felder - protonentechnik mit einer konformalen photonentechnik ( vier - felder - becken - box ) und einer sieben - felder - imrt - technik verglichen . 
mittels dosis - volumen - histogramm - ( dvh - ) auswertung wurden mittlere und maximale dosiswerte im bereich der unterschiedlichen ptv sowie der risikoorgane ( rektumwand , harnblase , hftkpfe beidseits ) verglichen . 
zustzlich wurden die volumina des bestrahlten normalgewebes , der ptv und risikoorgane in unterschiedlichen dosisbereichen bewertet . 1 department of radiotherapy and radiobiology , medical university of vienna , vienna , austria , 2 department of radiotherapy , medical university of innsbruck , innsbruck , austria . received : may 10 , 2004 ; accepted : april 26 , 2005 strahlenther onkol 2005 no . 
 im vergleich zur protonentherapie ergaben sich bei den photonentechniken erhhte mittlere dosiswerte ( ~ 4080% ) fr die evaluierten risikoorgane , sowie ein anstieg ( differenz mittlere dosis 70% ) des bestrahlten normalgewebevolumens . 
beim vergleich der konformalen photonentherapie mit der imrt zeigte letztere eine geringere risikoorganbelastung im mittleren dosisbereich , im speziellen im bereich der rektumwand . schlussfolgerung : im vergleich zur 3 - d - gesttzten konformalen photonentherapie konnte mit hilfe der imrt die dosisbelastung an den risikoorganen in den mittleren dosisbereichen reduziert werden . 
 schlsselwrter : prostatakarzinom protonentherapie imrt bestrahlungsplanung introduction current options for the treatment of organ - confined prostate cancer include radical surgery , photon - based external - beam therapy , brachytherapy or special treatment options such as proton radiotherapy [ 2 , 8 , 12 , 15 , 18 , 20 , 21 , 28 , 30 , 38 ]  . 
 long - term studies have demonstrated that radiotherapy is an effective treatment for controlling localized neoplasm , whereas the management of advanced stages of disease remains suboptimal [ 28 ]  . a statistically significant relationship has been described between applied total doses and recurrence rates , but it is generally accepted that with conventional photon radiotherapy techniques an increase in total doses is associated with higher risks of long - term complications ( i.e. , rectal bleeding , hematuria , urethral stricture ) [ 9 , 23 , 34 , 35 , 37 ]  . 
published results on prostate dose escalation trials are encouraging in terms of improved tumor control rates and acceptable complication levels [ 3 , 4 , 7 , 17 , 39 ]  . intensity - modulated radiotherapy ( imrt ) is regarded as an advanced form of 3 - d conformal radiotherapy which significantly improves the conformality of dose distributions [ 1 , 39 ]  . 
based on the results of comparative treatment - planning studies this treatment option is expected to reduce doses to organs at risk ( oars ) when compared to conventional and conformal irradiation techniques . 
proton beams can be modified to deliver a homogeneous radiation dose to an irregular 3 - d volume , and depth conformation is possible due to the finite and energy - dependent proton range ( i.e. , steep distal dose fall - off ) [ 27 , 31 , 32 ]  . 
studies using protons alone or as a boost after photons have been published , which demonstrate that proton - beam therapy was well tolerated and good tumor control and treatment outcomes could be achieved [ 31 , 32 , 38 ]  . the present study was performed to assess the potential benefit of proton - beam therapy for different stages of prostate cancer . 
proton - beam therapy is compared with state - of - the - art and advanced photon - beam therapy options , i.e. , imrt and uniform - intensity conformal radiotherapy . 
 material and methods comparative treatment planning was performed in five patients receiving radiotherapy for localized prostate carcinoma in the department of radiotherapy and radiobiology , medical university of vienna , austria . 
each patient was ct - scanned in supine position with 5 - mm slice spacing using a rectal balloon ( containing approximately 40 ml of water ) to exclude the majority of the rectal lumen from the high dose area [ 36 ]  . 
 for all treatment options a total dose of 70 cge ( 2 - gy daily fractions ) was prescribed at the isocenter and the 95% isodose had to cover 99% of the ptv . 
for the conformal photon techniques ( four - field box , gantry angles 0 , 90 , 180 , 270 ) beam weights were optimized if considered necessary , otherwise each field contributed equally to the dose at the isocenter . 
similar to the photon - based treatment - planning techniques a total dose of 70 cge ( 2 - cge daily fractions ) was prescribed at the isocenter with the 95% isodose encompassing 99% of the ptvs . imrt planning was based on five or seven equally spaced isocentric beams ( e.g. , seven fields at gantry angles of 0 , 52 , 104 , 154 , 208 , 256 , and 308 )  . 
the part of the rectal wall excluding the ptv was defined as a separate 3 - d organ to facilitate inverse planning , with the following dose - volume histogram ( dvh ) constraints defined for this help structure : 105% , 90% and 70% of the dose was allowed to be delivered to 2% , 15% and 30% of the volume , respectively . 
additionally , mean doses of 70 gy were assigned to 99% of ptv iiii . evaluation criteria for all treatment options dvhs were analyzed and compared for the different targets and oars . 
additionally , d5% and d95% , defined as the dose ( in % of the prescribed dose ) where the cumulative dvhs intersected with 5% and 95% of the ptv , respectively , were determined to calculated target dose homogeneities u for the different treatment options using to the following definition : u = ( d5%d95% ) / dmean . 
finally , dose conformity was assessed by calculating ratios of ptv and volumes of the respective 95% isodose . for oars ( bladder , rectal wall and both femoral heads ) mean doses were derived from dvhs , and volumes receiving strahlenther onkol 2005 no . 
mean dvhs of all patients for the right femoral head ( a ) , the bladder ( b ) and the rectal wall ( c ) based on calculations of ptv iii . 
mittlere dvhs aller patienten fr den rechten hftkopf ( a ) , die harnblase ( b ) und die rektumwand ( c ) kalkulationen auf der basis von ptv iii . 
the same isodose levels were used to assess the dose delivered to non - target normal tissue . results figure 2c abbildung 2c low dose range medium dose range relative dose ( % ) figures 1a to 1c show typical dose distributions in transverse planes at the level of the prostate for the 3 - d conformal photon - , the imrt and the proton - beam techniques . 
mean dose ( gy ) and range values to non - target tissues and organs at risk for the different treatment - planning options according to planning target volumes ptv iiii . 
the reduction in the dose delivered to non - target structures observed for proton - beam radiotherapy was predominantly observed in the low to medium dose ranges , while almost similar dose values were determined for isodose levels > 70% . 
 imrt , when compared to 3 - d conformal irradiation techniques , resulted in reductions of non - target tissue volumes receiving low to medium doses ( see figures 2b and 2c )  . comparing the conformal treatment plans ( four - field box techniques ) performed on two different treatment - planning systems , denoted as photons i and ii in tables 1 and 2 , small dose differences in the order of 25% were observed . 
this can be explained by inaccuracies in the transfer of delineated structures ( target volumes and oars ) and in the dose calculation algorithms of the helax and optirad treatment - planning systems . 
 discussion the different irradiation techniques compared in this study were considered the treatment options of choice for externalbeam therapy of prostate cancer ; both the high - energy photon and proton beams have shown to be highly effective and are currently used to treat patients in several facilities [ 57 , 10 , 26 , 27 , 29 ]  . 
for example , it has been demonstrated that conformal radiotherapy in prostate cancer can reduce acute side effects of the rectuhowever , this beneficial effect may not reduce late toxicity . 
 [ 17 ] analyzed late morbidity rates of conventional and conformal irradiation in prostate cancer and did not find a significant difference in the incidence of rectal , anal and bladder toxicity after a follow - up period of 2 years . 
 imrt , on the other hand , is regarded as an advanced form of 3 - d conformal radiotherapy , which can significantly improve the conformality of the dose distribution relative to the ptv . 
 in the current study , for the relatively symmetrical and spherical target prostate ( seminal vesicles ) similar conformity indices were obtained for all photonand proton - based treatment - planning options . 
for imrt based on computerized treatment plan optimization results are to some extent dependent on the treatment - planning system , the imrt delivery technique and the treatment goal defined as dose constraints . 
 in the present study target coverage at a dose level of 70 gy was given highest priority and in dose escalation studies aiming at doses around 7678 gy the benefit of imrt might be strahlenther onkol 2005 no . 
 [ 39 ] reported on a dose reduction of the rectal wall and the bladder wall when using imrt . conformal proton - beam therapy is regarded as a promising radiation treatment technique [ 29 ] , and the present , as well as other studies , have shown that improvements in dose delivery to oars can be achieved with this treatment option [ 19 ]  . 
most investigations correlated acute and / or late toxicity with rectal dvh patterns especially in the high dose area [ 5 , 13 , 16 , 25 , 26 , 35 ]  . 
 [ 10 ] , the incidence of late rectal bleeding was significantly correlated with the percentage of rectal volume receiving dose levels of > 5065 gy but not in the dose region between 7075 gy . 
 [ 16 ] compared rectal wall dvhs of bleeding versus nonbleeding patients and found the largest difference in the dvh shape in the 40to 50 - gy region , while relatively small differences were found in the high dose region between 7075 gy . 
 [ 30 ] analyzed dosimetric parameters associated with late rectal toxicity > grade 2 and found the following factors to be predictive of rectum bleeding : small rectal volumes , maximum dose to the rectal wall and enclosure of the outer rectal constrahlenther onkol 2005 no . 
independent of irradiation technique the bladder base , urinary sphincter and urethra receive high doses , since these structures lie within the radiation target volume [ 7 , 25 ]  . 
the significantly lower dose to the bladder by using protons might result in a risk reduction . conclusion imrt enabled dose reductions to oars at medium dose ranges when compared to uniform - intensity 3 - d conformal photon radiotherapy . 
 acknowledgment this study was performed within the framework of the med austron project and was supported by the government of lower austria and the federal ministry for education , science and culture . 
endres2 , giuseppe sanguineti1 background and purpose : to assess and quantify the benefit of introducing intensity - modulated radiotherapy ( imrt ) over conventional approaches to cover the pelvic nodes while escalating the dose to the prostate gland . material and methods : the pelvic lymphatics were planned to receive 50 gy at 2 gy per fraction by four - field box ( 4fb ) technique and standard field blocks drawn on digitally reconstructed radiographs ( drr ) , 4fb with field blocks according to the position of pelvic nodes as contoured on serial planning ct slices , or imrt . 
by the combination of a pelvic treatment and boost , several plans were obtained for each patient , all normalized to be isoeffective with regard to prostate - planning target volume ( ptv - p ) coverage . 
plans were compared with respect to dose - volume histogram ( dvh ) of pelvic nodes / seminal vesicles - ptv ( ptv - pn / sv ) , rectum , bladder and intestinal cavity . 
reported are the results obtained in eight patients . results : pelvic imrt with a conformal boost provided superior sparing of both bladder and rectum over any of the 4fb plans with the same boost . 
finally , the effect of utilizing an imrt boost with initial pelvic imrt was greater for the bladder than for the rectum ( at v70 , about 9% and 3% for the bladder and rectum , respectively )  . conclusion : imrt to pelvic nodes with a conformal boost allows dose escalation to the prostate while respecting current dose objectives in the majority of patients and it is dosimetrically superior to 4fb . 
an imrt boost should be considered for patients who fail to meet bladder dose objectives . key words : imrt whole - pelvis radiotherapy dose escalation strahlenther onkol 2005 ; 181 : 43141 doi 10.1007 / s00066 - 005 - 1384 - 9 imrt zur eskalation der prostatadosis bei bestrahlung der beckenlymphknoten ziel : evaluation des vorteils der intensittsmodulierten radiotherapie ( imrt ) im vergleich zu konventionellen methoden , um bei bestrahlung der beckenlymphknoten die prostatadosis zu eskalieren . 
 material und methoden : fr die bestrahlung der beckenlymphknoten wurde eine gesamtdosis von 50 gy , in fraktionen von 2 gy , geplant unter einsatz einer vier - felder - box - ( 4fb - ) technik mit standard - blcken , von 4fb - technik mit blcken entsprechend der in seriellen planungs - cts festgestellten lage der lymphknoten , oder der imrt . 
die planungen wurden hinsichtlich der dosis - volumenhistogramme ( dvh ) des planungszielvolumens der beckenlymphknoten / blschendrsen ( ptv - pn / sv ) , des rektums , der blase und des bauchraumes verglichen . 
vorgestellt werden die bei acht patienten ermittelten ergebnisse . ergebnisse : die imrt des beckens mit einem konformalen boost war hinsichtlich des schutzes von blase und rektum allen 4fbplanungen mit demselben boost berlegen . 
der vorteil war jedoch bei imrt des beckens mit konformalem boost immer grer als bei 4fb1 department of radiation oncology , university of texas medical branch , galveston , tx , usa , 2 department of medical physics , university of texas medical branch , galveston , tx , usa . received : october 19 , 2004 ; accepted : april 26 , 2005 strahlenther onkol 2005 no . 
 schlussfolgerung : imrt der beckenlymphknoten mit konformalem boost erlaubt bei der mehrzahl der patienten die eskalation der prostatadosis unter bercksichtigung der zieldosis und ist dosimetrisch der 4fb - technik berlegen . 
 schlsselwrter : imrt strahlenbehandlung des beckens dosiseskalation introduction strategies to improve outcome in patients with prostate cancer undergoing definitive radiotherapy include escalation of radiotherapy total dose , the addition of androgen deprivation to radiotherapy , the coverage of pelvic nodes by the initial target volume , or any combination thereof . 
 dose escalation has been shown to improve outcome predominantly in intermediateto high - risk patients in both retrospective and prospective studies [ 16 , 22 , 2931 , 43 , 49 ]  . 
the role of adding pelvic node treatment to standard - dose radiotherapy to the prostate has been recently addressed by rtog study 9413 [ 34 ] after several retrospective and prospective studies , as summarized by roberts & roach [ 36 ] , were unable to provide a definitive answer . 
preliminary results suggest that for patients with a > 15% risk of involvement of pelvic lymph nodes , as defined by the roach formula [ 35 ] , including the pelvic nodes in the initial fields may provide some benefit [ 34 ]  . 
 interestingly , for the same patient population , both androgen deprivation [ 34 ] and dose escalation [ 18 , 23 ] seem to play an independent role from pelvic node coverage in ameliorating outcome ; in other words , combining the three strategies may provide additional benefits over each alone . 
concerns arise from the fact that long - term adjuvant androgen deprivation has been associated with an increased incidence of gastrointestinal toxicity [ 4 , 15 , 38 , 40 , 46 ]  . 
although it is not an unequivocal finding [ 1 , 3 , 21 , 41 ] , some studies have also reported increased gastrointestinal / genitourinary ( gi / gu ) toxicity when wholepelvis radiotherapy is added to standard - dose ( 70 gy ) radiotherapy to the prostate compared to prostate - only ( po ) radiotherapy [ 25 , 37 ]  . 
 recent data on rectal tolerance to radiation therapy ( xrt ) show that the volume of rectum that receives both intermediate ( 5065 gy ) and high ( 6575 gy ) doses is independently correlated to rectal bleeding [ 8 , 11 , 12 , 17 , 32 ]  . 
the inclusion of pelvic nodes in the initial clinical target volume ( ctv ) of a four - field box ( 4fb ) can potentially expose more rectum to intermediate doses and saturate rectal tolerance before the dose escalation can occur . 
in the present paper , this issue is quantified and compared in terms of changes in dosevolume histogram ( dvh ) of both bladder and rectum using different approaches to treating both the pelvic nodes and boosting the prostate , including conventional , conformal , and intensity - modulated radiotherapy ( imrt ) techniques . material and methods in the present study , different approaches to include the pelvic nodes in the initial treatment volume were considered . 
each plan was isoeffective with respect to coverage of the planning target volume of the prostate ( ptv - p ) , i.e. , 100% of ptv - p received at least 95% of the prescription dose ( v95 100 ) for all strategies . patients and volumes eight consecutive patients with biopsy - proven adenocarcinoma of the prostate referred to our department for radical radiotherapy were selected for this study . 
all patients had clinically prostate - confined disease without obvious extracapsular extension or positive pelvic nodes . for the simulation procedure , the patient was placed in the supine position with alpha cradle immobilizing the lower extremities . 
the patients were instructed to present for simulation ( and treatment ) with an empty rectum ; bladder had to be voided 0.51 h before simulation and each treatment . first , urethrography was performed . 
on the conventional simulator table , the isocenter was placed at the midpoint between l5 / s1 and the beak of the urethrogram in the craniocaudal direction , and behind the femoral heads in the anterior - posterior plane . 
typically , 5 mm slice thickness is used from the top of iliac bone to at least 5 cm below the base of the penis ; a slice thickness of 3 mm was obtained for the cross - sectional slices containing the prostate . the ct data sets were transferred to the philips pinnacle3 treatment planning system ( philips medical systems , madison , wi , usa )  . 
regions of interest ( rois ) and oars were outlined by a radiation oncologist and reviewed by another and included the prostate ( p ) , seminal vesicles ( sv ) , pelvic lymph nodes ( pn ) , bladder ( b ) , rectum ( r ) , instrahlenther onkol 2005 no . 
the pelvic lymphatics included the obturator and hypogastric , internal and external iliac ( from the bifurcation of the common iliac artery at the level of the top of the sacroiliac joints , to the point where the external iliac artery crossed the inguinal ligament ) , and the presciatic and presacral ( anterior to the first and second sacral segments ) nodes . 
on axial ct slices , its boundaries included the abdominal wall anteriorly and anterolaterally , the retroperitoneal and deep pelvic muscles posterolaterally , and the great vessels , vertebral bodies , sacrum and rectum posteriorly . 
 fields the goal was to deliver 50 gy to the pelvic nodes and seminal vesicles ( ptv - pn ) and 76 gy to the prostate ( ptv - p ) at 2 gy per fraction . 
the two phases were considered in a conventional , sequential way with a plan for the initial 50 gy covering pn + sv + p and a boost to the p only for an additional 26 gy . 
it should be noted that the posterior / lower part of the lateral block is identical in all the fields and conformal to ptv - p coverage , while the posterior / upper part differs among b1 , d1 and a1 / c1 . 
zu beachten ist , dass der posteriore / untere teil des lateralen blocks in allen feldern identisch ist und konformal der bestrahlung des planungszielvolumens der prostata ( ptv - p ) , whrend der posteriore / obere teil unterschiede zwischen b1 , d1 und a1 / c1 aufweist . 
 in general , three main approaches were investigated to cover the initial volume : conventional 4fb ( trial a ) with customized blocks drawn on digitally reconstructed radiographs ( drrs ) ; three - dimensional conformal radiotherapy ( 3dcrt ) 4fb ( b , c , d ) with blocks that conformed to ptv ( pn + sv + p ) on beams eye view except at the posterior border of lateral fields , where various degrees of rectal shielding were utilized ; and imrt ( e ) , covering the same volume as 3dcrt but with eight - field imrt . 3dcrt fields were further divided according to the degree of rectal shielding on lateral fields : ( 1 ) no shielding ( b ) , ( 2 ) mid - shielding ( c ) , or shielding the anterior half of the rectum above the prostate ptv up to s2 , and ( 3 ) mid + upper shielding ( d ) , or shielding the anterior half of the rectum superiorly to the rectosigmoid junction . 
for the conventional ( a ) approach , once the blocks had been drawn on the drr , part of rectum was shielded ( as done in technique c )  . 
the anteroposterior field was again drawn on drrs without volumes ( except for p ) for trial a and according to ptv ( pn + sv + p ) for trials bd ( figure 1 )  . it should be noted that geometric coverage of the prostate was identical for all the plans and took precedence over rectal shielding . 
 trial ptv - pn field arrangement comment ptv - p field arrangement four - field box four - field box four - field box four - field box eight - field imrt none standard blocks ; split rectum as c drawn per ptv - pn ; open on rectum drawn per ptv - pn ; split part up rectum drawn per ptv - pn ; split all up rectum 3dcrt , six - field imrt , eight - field 3dcrt , six - field imrt , eight - field 3dcrt , six - field imrt , eight - field 3dcrt , six - field imrt , eight - field 3dcrt , six - field imrt , eight - field 3dcrt , six - field 3dcrt , six - field imrt , eight - field imrt , eight - field the eight gantry angles selected for the inverse planning imrt fields were coplanar and non - opposed at angles of 220 , 260 , 300 , 340 , 20 , 60 , 100 , and 140 . 
field sizes were determined by the inverse planning system , but were initially set to allow exposure of the sum of all ptvs plus an additional margin of 1.5 c regarding the boost , two approaches were investigated : 3dcrt and imrt . 
for the imrt boost plan , the field sizes were initially set to allow exposure of the prostate + margin with an additional 1.5 cm , but were ultimately determined by the inverse planning syste plans the combination of these pelvic and boost plans resulted in the list of trials presented in table 1 . 
the method in which the two phases ( pelvis and boost ) were combined and optimized is as follows : 4fb plans ( ad ) were created independent of boost technique , i.e. , each field arrangement in table 1 has the same monitor units regardless of boost plan . 
each boost plan was adjusted slightly ( < 1% ) for each pelvic plan when matched to a particular pelvic plan in order to ensure v95 100 for ptv - p . 
however , during the optimization process the planner may have adjusted the dose objectives to achieve a superior plan with the stated goal of achieving the lowest possible rectal dvh while maintaining the ptv prescription constraints . total dose ( gy ) for the imrt pelvis plans , dose objectives for bladder and rectum were set slightly lower than those achieved by the imrt boost plan in hopes to yield the most optimal plan . 
 by convention , objectives for each plan , boost and pelvis imrt , were based on a plan delivering 76 gy in 38 fractions , even though only techniques f1 strahlenther onkol 2005 no . 
for each roi , both the mean dvh ( standard deviation [ sd ] ) and the fraction of each roi receiving a percent of a relevant prescribed dose , for the purpose of the present study , are reported . 
for ptv - pn coverage , v40 ( or 80% of prescribed dose to target ) , v47.5 ( 95% ) , v50 ( 100% ) and v60 ( 120% ) were considered . 
statistically significant difference was claimed for p - value < 0.05. results target volume coverage first , the coverages of ptv - p and ptv - pn were examined according to the various initial techniques . 
ptv - pn data are summarized in table 3 , and figures 2 and 3 illustrate the mean dvh for all eight patients considered in this study for the most significant trials . 
with respect to ptv - p coverage , per initial assumption , all techniques were set to be isoeffective with regard to ptv - p coverage , delivering at least 95% of the prescription dose to 100% of the ptv - p volume ( figure 2 )  . 
regarding ptv - pn / sv coverage ( figure 3 ) , the mean ptv - pn volume is 1 , 095 cm3 ( sd = 109 cm3 ) or about six times greater than mean ptv - p volume and therefore , small changes along the y - axis are associated with a large effect on the absolute amount of the ptv that is included in a given isodose cloud . 
comparison between e1 and b1 reveals a slightly superior coverage of the target at v47.5 ( p = 0.014 ) by b1 ( both v40 and v50 are not statistically different ) , but this comes at the cost of a significantly higher v60 ( table 3 , figure 3b ) , as a result of a more conformal dose distribution with pelvic imrt . introducing an imrt as compared to a conformal boost had a negligible effect on prostate gland coverage ( figure 4a )  . 
 however , as reflected by figure 4b , the imrt boost by increasing the conformity of dose to the ptv - p reduced v60 and v70 for ptv - pn . d ( gy ) figure 2 . 
shielding the rectum on lateral fields of 4fb translated in underdosing part of ptv - pn volume that is proportional to the extent of shielding , as shown in table 3 . 
 compared to the 4fb technique with rectal shielding ( c1 ) , imrt to the pelvic nodes ( e1 ) results in statistically improved ( p < 0.01 ) coverage of the target in the 47.550 gy interval , and a steeper gradient outside ptv - p producing a more rectum as expected , conforming fields to ptv - pn without shielding part of the rectum on the lateral fields ( b1 ) exposes a large amount of rectum to low and intermediate doses ( figure 5a )  . 
 however , even adding rectal shielding ( a1 , c1 , d1 ) does not ensure that a plan meets dose - volume objectives for the rectum ( figure 5b )  . figure 5b also shows that including the pelvic nodes in the 4fb ( a1 , c1 , d1 ) translated into an absolute increase in the percent of rectum getting 45 gy , 55 gy and 65 gy of approximately 2530% , 1015% and 56% , respectively , as compared to po radiotherapy ( f1 )  . 
at 70 gy , although the difference was smaller ( 34% ) , it was still highly statistically significant . pelvic imrt ( e1 ) spares more rectum as compared to b1 ( table 4 , figure 5a )  . 
 bladder trials with 4fb followed by 3dcrt ( a1d1 ) provided an average dose to bladder higher than that of initial imrt to the pelvis with the same 3dcrt boost ( e1 , figure 7 )  . 
 as with the rectum , the coverage of pelvic nodes with any of the 4fb techniques ( a1d1 ) translated into a significantly larger portion of the bladder being irradiated over po 3dcrt ( f1 )  . 
in particular , up to 40% more of the bladder was exposed to doses in the range of v3050 ; at 60 gy and 70 gy , the absolute difference is around 20% and 15% , respectively . 
 60 gy and 70 gy the advantage was about 7% , 11% and 9% , respectively , while , as previously stated , it was always < 5% for the rectu as shown in figure 8 , switching from a conformal to an imrt boost for 4fb plans ( ad ) allows at least 5% sparing of the bladder from v55 on . 
on average , both e1 and a2d2 plans are very close to the dosimetric constraints suggested by rtog . in terms of percent of organ spared at a given dose level , the advantage of an imrt boost after initial pelvic imrt ( e2 ) was greater for the bladder than for the rectum : at 50 gy , intestinal cavity as mentioned in the material and methods section , besides usual dose objectives , the following dose - volume objectives were utilized : v45 gy 412 cm3 , v30 gy 785 cm3 , and v15 gy 1 , 279 cm3 . 
rectal dose - volume histogra average of four - field box plans with 3dcrt ( a1d1 ) versus imrt ( a2d2 ) boost compared with imrt whole pelvis + 3dcrt ( e1 ) or imrt ( e2 ) boost . 
given the fact that the intestinal cavity volume is large ( mean : 1 , 509.3 ; sd : 391.6 cm3 ) , the small advantage in favor of e1 may become clinically relevant for late complications . 
patients with whole - pelvis radiotherapy experienced a 4 - year progression - free survival of 54.2% compared to 47% for patients treated on the prostate only [ 34 ]  . 
these data , although preliminary , suggest that inclusion of pelvic nodes in the initial fields should be seriously taken into consideration in patients at significant risk of nodal involvement [ 28 ]  . 
 interestingly , for the same group of patients , a recent retrospective study from fox chase suggests that radiation dose to the prostate is an independent predictor of biochemical control [ 17 ]  . 
bladder dose - volume histograaverage of four - field box plans with 3dcrt ( a1d1 ) versus imrt ( a2d2 ) boost compared with imrt whole pelvis + 3dcrt ( e1 ) or imrt ( e2 ) boost . 
in summary , while there is some evidence that extending initial fields may be worthwhile , other strategies may work equally as well and therefore the issue may be whether or not it is possible to combine the strategies safely in order to improve outcomes in this group of patients . 
on the other hand , while an imrt boost added to initial 4fb can provide some benefit , the best results , in terms of both ptv coverage and bladder / rectum sparing , are achieved with pelvic imrt . 
finally , an imrt boost added to an initial imrt plan can provide additional benefits , mainly in terms of bladder sparing . the results of the present paper should be viewed and interpreted under the conditions initially set . 
if the pelvic lymphatics were treated to 45 gy instead of 50 gy and therefore the boost comprised a larger percentage of the total dose , then the relative benefit of an imrt boost may be greater than in this study . 
however , in order to deliver the dose to ptv - pn and ptv - p in the same number of fractions , this would have introduced dose - fractionation issues and uncertainties in plan comparison [ 44 ]  . rectal shielding in proximity to the prostate gland as a means to improve rectal tolerance , even for only few fractions , was deliberately avoided . 
although this has been a popular way to improve rectal tolerance and allow safe dose escalation [ 19 , 48 ] , coverage of ptv - p is affected as well , hampering the planned coverage of 95% of the volume . 
however , it should also be noted that based on the observed range of improvement from switching from plans with 3dcrt boost to those with imrt boost ( figures 6 and 9 ) , a modest improvement in the conformal boost would have had a limited effect on the rectal and bladder dvh . 
others have used much lower estimates for v40 and v65 that are consistent with a full bladder and the use of daily ultrasound for prostate localization [ 47 ]  . 
 within prostate cancer radiotherapy , imrt has been explored for its ability over 3dcrt to better conform to a concave - shaped volume such as the prostate [ 7 , 10 ] and to better spare normal structures , including part of the bowel [ 14 , 24 ] and even the penile bulb [ 42 ]  . 
to our knowledge , however , the issue of dose escalation to the prostate while treating the pelvic lymphatics and the resultant bladder and rectal dvhs has not been studied in detail . 
while there is no doubt that there is a dosimetric advantage in using imrt for treating the pelvic nodes , little is known to justify whether this is clinically worthwhile and cost - effective . 
 for example , in the studies that have reported rectal constraints ( table 2 ) , most of the events are grade 2 toxicity [ 11 , 17 ] ; it has been shown that such toxicity has a modest impact on quality of life [ 20 ] and is transient [ 45 ]  . 
moreover , it has been reported that grade 2 and 3 rectal reactions may have a different radiobiological behavior with less severe reaction being linked to intermediate doses and more severe one to high dose regions along the dvh [ 33 ]  . 
however , even taking into consideration this fact , it should be noted that pelvic imrt is superior to 4fb across the entire rectal dvh , as shown in figure 5 . 
we believe that clinical testing of this approach within a prospective phase iii study is warranted and such a study has been open at utmb for patients with prostate cancer at significant risk of pelvic node involvement referred to us for definitive radiotherapy [ 39 ]  . 
an imrt boost is considered particularly if the bladder dvh falls outside dose objectives . strahlentherapie und onkologie technical note dosimetric quality assurance for intensity - modulated radiotherapy feasibility study for a filmless approach tilo wiezorek1 , nico banz2 , michael schwedas1 , marcel scheithauer1 , henning salz1 , dietmar georg3 , thomas g . 
wendt1 purpose : test and comparison of various 2 - d real - time detectors for dosimetric quality assurance ( qa ) of intensity - modulated radiotherapy ( imrt ) with the vision to replace radiographic films for 2 - d dosimetry . 
a mevatron primus ( siemens ocs ) linear accelerator which provides 6 - mv and 15 - mv highenergy photon beams was used for the delivery of segmented multileaf - modulated imrt . 
three different 2 - d detectors , each based on a different physical ( interaction ) principle , were tested for the field - related imrt verification : ( 1 ) the mapcheck diode system ( sun nuclear ) , ( 2 ) the imrt qa scintillation detector ( scanditronix / wellhfer ) , and the seven29 ionization chamber array ( ptw )  . 
 the performance of these detector arrays was evaluated against imrt dose distributions created and calculated with konrad and the results obtained were compared with film measurements performed with radiographic films ( edr2 , kodak )  . 
additionally , measurements were performed with point detectors , such as diamond , diodes ( ptw ) and ionization chambers ( ptw , scanditronics / wellhfer ) and radiochromic films ( gafchromic film md55 , isp )  . 
 results : the results obtained with all three 2 - d detector systems were in good agreement with calculations performed with the treatment - planning system and with the standard dosimetric tools , i.e. , films or various point dose detectors . 
 key words : film dosimetry quality assurance 2 - d detectors intensity - modulated radiotherapy imrt strahlenther onkol 2005 ; 181 : 46874 doi 10.1007 / s00066 - 005 - 1381 - z dosimetrische qualittssicherung fr die intensittsmodulierte strahlentherapie . 
machbarkeitsstudie eines filmlosen ansatzes ziel : verschiedene 2 - d - echtzeitdetektoren wurden hinsichtlich ihrer eignung zur dosimetrischen verifikation der intensittsmodulierten strahlentherapie ( imrt ) untersucht und getestet mit der vision , zuknftig radiographische filme abzulsen . 
als referenzdosimetrie - systeme wurden radiographische filme ( edr2 , kodak ) und radiochromatische filme ( gafchromic - film md55 , isp ) sowie ein diamantdetektor , ein halbleiterdetektor ( beide ptw ) und eine ionisationskammer ( scanditronix / wellhfer ) verwendet . 
 ergebnisse : die mit den drei 2 - d - detektoren gewonnenen ergebnisse zeigten eine gute bereinstimmung mit den rechnungen des bestrahlungsplanungssystems und mit den messwerten von herkmmlichen dosimetern wie filmen oder verschiedenen punkt1 department of radiotherapy , radiologic clinic , university hospital , jena , germany , 2 institute for biomedical technics and informatics , technical university , ilmenau , germany , 3 department of medical radiation physics , university hospital for radiotherapy and radiobiology , medical university , vienna , austria . received : october 6 , 2004 ; accepted : march 15 , 2005 strahlenther onkol 2005 no . 
die wesentlichen unterschiede zwischen den detektorsystemen lagen in der rumlichen auflsung , der maximalen feldgre und der fhigkeit zur absolutdosimetrie . schlussfolgerung : kommerziell erhltliche 2 - d - detektorsysteme haben das potential , den film als flchendetektor zu ersetzen . 
 die durch die untersuchten 2 - d - systeme in echtzeit erhltlichen informationen knnen auch die effizienz der gesamten qualittssicherungsprozedur verbessern . schlsselwrter : filmdosimetrie qualittssicherung 2 - d - detektoren intensittsmodulierte strahlentherapie imrt introduction today , the use of intensity - modulated radiotherapy ( imrt ) is a very helpful technology for the optimization of radiation therapy , e.g. , for dose enhancement , for complex - shaped targets and for dose reduction in organs at risk partially surrounded by a concavely shaped target volume [ 4 , 8 , 12 ]  . 
 at present , mainly two different approaches are applied for the dosimetric verification of imrt plans or quality assurance ( qa ) of imrt : the plan - related approach and the field - related approach [ 1 , 2 , 10 , 11 , 13 ]  . 
despite the fact that the field - related approach does not reflect the whole treatment , the main advantage is that the complete area of the modulated beams is covered . 
the main disadvantage is that a field - related approach does not add up results and it is thus difficult to derive information on the overall accuracy of a composite treatment plan . 
however , to obtain absolute and relative dosimetric information with acceptable accuracy , point dose ( e.g. , using an ionization chamber ) and the 2 - d methods need to be combined . 
however , there is potential to optimize and modernize film verification procedures , e.g. , by using electronic real - time 2 - d detector systems which became commercially available recently . 
for example , many hospitals are aiming toward a so - called digital hospital , where film - processing machines for traditional silver - halide - based films will not be available or easily accessible in the near future . 
radiochromic film , which is self - developing and an alternative to radiographic film , requires a rather high dose and hence the monitor units ( mu ) of the treatment plan need to be multiplied by a high factor to reach the sensitive range of these fil additionally , these types of film are rather expensive . although there are many published papers [ 5 , 7 , 9 , 15 ] describing the application of radiographic film for dosimetric purposes in radiotherapy including imrt , their application is not straightforward due to many factors of influence on the optical density , such as energy and spectral composition , depth , fields size , orientation , and processing conditions . 
the aim of the present work was , therefore , to test and evaluate different commercially available 2 - d detectors for the imrt verification based on a field - related approach . material and methods imrt planning and delivery all imrt treatment plans were generated with the konrad software v 2.1.3 ( siemens ocs )  . 
a mevatron primus ( siemens ocs ) linear accelerator , providing 6 - mv and 15 - mv highenergy photon beams , was used to deliver the imrt plans by a step - and - shoot approach . 
the dosimetric characteristics of the integrated mlc can be found in the literature [ 3 ]  . additionally , some experiments were made with cerrobend compensator with three different thicknesses ( 7 mm , 18 mm , 32 mm )  . 
the diodes are arranged with a 7 - mm grid spacing in an inner square field of 10 10 cm2 , and with a spacing of 14 mm in the border between the inner square and a field of 22 22 cm2 . 
 a buildup layer of acrylic ( approximately 2 cm water - equivalent thickness ) covers the diodes and a back layer of acrylic ( approximately 2.3 cm water - equivalent thickness ) provides backscatter . 
no backscatter material is possible because of the bodywork of the system . seven29 system ( ptw ) the third system is an ionization chamber array consisting of 729 air - filled chambers . 
in this way , it was decided to use all 2 - d detectors with their own evaluation software as a closed measurement syste cessing machine ( kodak )  . 
 for point dose verification and profile measurements a small - volume ionization chamber ic04 ( scanditronix / wellhfer ) connected to a dose 1 electrometer ( scanditronix / wellhfer ) , a diamond detector type 60003 - 013 ( ptw ) and a conventional - sized chamber type 31002 ( ptw ) connected to a unidos electrometer ( ptw ) were used . 
all point dose measurements were performed in a water phantom at a depth of 10 c dosimetric comparison the 2 - d detector systems signal behavior was analyzed as a function of applied dose and with respect to signal delay . 
in order to check this detector characteristic , output factors were measured with different 2 - d dosimetric systems and with the diamond detector and the ionization chamber , respectively . 
however , it was impossible to guarantee the same backscatter conditions for all detectors . finally , imrt plans were verified with a field - related apreference dosimetric systems proach applying the different detector systems . the reference detector for relative 2 - d dosimetry was radiographic and radiochromic filas radiographic film an edr2 type film ( kodak ) was used , while as radiochromic reference detector the film type md55 ( nuclear associates ) was chosen . 
the radiographic film was processed with a curix260 proresults figure 1 illustrates the relative signal response of the various 2 - d detectors as a function of delivered mu , for a square field of 10 cm length at 15 mv . 
output factors determined with radiographic film edr2 and with radiochromic film gafchromic md55 in comparison to values taken with an ionization chamber type 31002 in dependence on square field sizes from 5 5 cm2 to 27 27 cm2 ( 6 mv , depth 5 cm )  . 
outputfaktoren , gemessen mit radiographischem film edr2 und mit radiochromatischem film gafchromic md55 , im vergleich zu werten , ermittelt mit einer ionisationskammer typ 31002 in abhngigkeit von der quadratischen feldgre von 5 5 cm2 bis 27 27 cm2 ( 6 mv , tiefe 5 cm )  . 
 tector relative to the increase of low - energy scatter for larger field sizes . for comparison , output factors were measured additionally with radiochromic and radiographic films for 6 - mv photon beams ( figure 4 )  . 
outputfaktoren fr 15 mv , gemessen mit verschiedenen detektoren fr quadratische feldgren von 2 2 cm2 bis 20 20 cm2 . tions were considered , which are most relevant for imrt . 
 the results concerning field size dependence of the detector are shown in figure 2 for 6 - mv and in figure 3 for 15mv high - energy photon beams , respectively . 
 while there was a good agreement between output factors determined with the diode array , the ionization chamber array , the diamond detector and the ionization chamber , there was a larger discrepancy for results obtained with the scintillation - based detector . 
relative comparison of the measured ( blue ) versus the calculated ( green ) dose profils normalized to high - dose area ; taken with the edr2 and processed with the lumiscan and the software veridos v 2.11. 
relativer vergleich der gemessenen ( blau ) zu den berechneten ( grn ) isodosen , normalisiert auf die hochdosisregion ; erzeugt mit dem edr2 und verarbeitet mit dem lumiscan und der software veridos v 2.11. 
for this specific test an imrt plan with different fluence levels in a 3 3 cm2 matrix and different matrix elements with a size of 3 3 cm2 was created . 
this fluence matrix should represent an imrt field with a wide range of and sharp borders between different intensity levels similar to the intensity shapes suggested for commissioning by ezzell et al . 
the calculation of the dose matrices were done in 10 cm water - equivalent depth ; the measurements of the dose matrices were realized in the same depth behind layers of pmma . 
 all measurements were compared with respect to the calculated dose matrices exported from the planning systethe different irregular multileaf - collimator - ( mlc - ) shaped segments to create the intensity distribution are shown in figure 5 . 
 as described above , the comparisons of the measured and the calculated profiles and dose matrices were carried out with the specific software tool coming with the respective 2 - d strahlenther onkol 2005 no . 
dosimetric quality assurance for imrt detector systebasically , all systems with different analysis programs have different evaluation modes , e.g. , gamma criteria , distance - to - agreement ( dta ) or composite analyses . 
figures 6a to 6d show dose profiles calculated with the treatment - planning system konrad and measured with the mapcheck ( figure 6a ) , the imrt ( figure 6b ) , the seven29 system ( figure 6c ) , and the edr2 film ( figure 6d )  . 
these deviations can be explained by the well - known overresponse of radiographic films to low - energy photons [ 14 ] due to a higher mass energy absorption coefficient for energies up to 150 kev . 
figure 7 illustrates the mass energy absorption coefficients as a function of photon - beam energy for different materials used in the various detectors investigated in the framework of the present study . the results of the experiments with different cerrobend filters show a strong influence on the relative detector sensitivity . 
an error of 5% is generated by a 32 - mm cerrobend filter which corresponds to a transmission of about 25% for 15 mv while using the edr2 film for dose measurements of compensator generated imrt fields ( figure 8 )  . 
an error of 2% was detected by 32 - mm cerrobend which corresponds to a transmission of about 20% for 6 mv nominal photon energy ( not shown )  . compensators are a source of contamination particles which can have an influence on the detector response and hence on the signal . 
 conclusion all three 2 - d detector systems investigated in the present study , each having its specific software for dosimetric analysis , are an alternative to ( radiographic ) film for imrt verification with a field - related approach . 
 in addition , it has to be pointed out that this stimulation of granulocytes by phorbol myristate acid ( pma ) is a chemical one which causes complete and almost irreversible release of all phagocytic substances and thus allows for characterization of total and relative function of these cells prior to and after radiotherapy . 
 strahlentherapie und onkologie original article prediction of axillary lymph node status of breast cancer patients by tumorbiological factors of the primary tumor tanja fehm1 , holger maul2 , sigrun gebauer3 , alexander scharf4 , peter baier2 , christof sohn2 , wolfram jger5 , gerhard gebauer2 background and purpose : the increasing use of systemic adjuvant therapy even in lymph node - negative breast cancer patients and breast cancer screening programs detecting smaller tumors with less probability of metastatic lymph nodes questions the need for routine axillary lymph node dissection . 
since morbidity of breast cancer surgery is predominantly related to axillary lymph node dissection , predictive models for lymph node involvement may provide a way to avoid lymph node surgery and its side effects in subgroups of patients . 
 patients and methods : using a multivariate logistic regression model , tumorbiological parameters such as expression of estrogen and progesterone receptors , ki - 67 , p53 , cathepsin d , her2 , s - phase fraction , and ploidy were analyzed regarding their ability to predict axillary lymph node involvement in 655 breast cancer patients . 
 key words : breast cancer axillary lymph node status tumorbiological factors ki - 67 progesterone receptor her2 strahlenther onkol 2005 ; 181 : 5806 doi 10.1007 / s00066 - 005 - 1374 - y prdiktion des axillren lymphknotenstatus mittels tumorbiologischer parameter des primrtumors beim mammakarzinom hintergrund und ziel : die zunehmende anwendung adjuvanter therapien auch bei nodal negativen mammakarzinompatientinnen sowie die im rahmen von screeningprogrammen immer frhzeitigere entdeckung kleiner mammakarzinome mit geringer wahrscheinlichkeit einer axillren lymphknotenmetastasierung stellen den nutzen der axillren lymphonodektomie zunehmend in frage . 
da die axillre lymphonodektomie mageblich fr die morbiditt der mammakarzinomoperation verantwortlich ist , stellt sich die frage , ob das risiko eines axillren lymphknotenbefalls fr subgruppen von mammakarzinompatientinnen properativ vorhergesagt werden kann . 
 patienten und methodik : mit hilfe einer multivariaten logistischen regression wurden tumorbiologische parameter ( expression von strogenund progesteronrezeptoren , ki - 67 , p53 , cathepsin d , her2 , s - phasen - anteil , ploidie ) in bezug auf ihre vorhersagekraft fr den axillren lymphknotenstatus bei 655 patientinnen mit primrer mammakarzinomerkrankung untersucht . 
 1 department of obstetrics and gynecology , university of tuebingen , germany , 2 department of obstetrics and gynecology , university of heidelberg , germany , 3 heidelberg , germany , 4 department of obstetrics and gynecology , hanover medical school , hanover , germany , 5 department of obstetrics and gynecology duesseldorf gerresheim , duesseldorf , germany . 
durch erweiterung auf zustzliche faktoren liee sich so ein modell entwickeln , auf dessen grundlage bei frauen mit geringem risiko fr eine axillre metastasierung auf die axillre lymphonodektomie verzichtet werden knnte . 
 schlsselwrter : mammakarzinom axillrer lymphknotenstatus tumorbiologische faktoren ki - 67 progesteronrezeptor her2 introduction the majority of breast cancer patients presents to date at an early stage with tumors histologically and radiologically restricted to the breast and without evidence of a systemic metastatic disease . 
however , standard therapy of breast cancer still consists of breast - conserving surgery in combination with axillary lymph node dissection and radiotherapy of the breast and lymphatics [ 18 , 2830 ]  . 
although surgical procedures of axillary lymph node dissection have changed over the last decade by introduction of less radical procedures limiting axillary surgery to level 1 and 2 lymph nodes or sentinel lymph node biopsy [ 17 , 26 ] , a considerable number of patients still suffers from side effects of surgery . 
however , the preoperative clinical and ultrasonographic examination of the axilla is a poor predictor of axillary lymph node involvement [ 24 , 25 ] and is therefore not suitable for selecting patients in whom axillary lymph node dissection might be avoided . 
 the use of breast cancer screening programs will most likely further reduce the average tumor size at primary diagnosis and , consecutively , the number of lymph node - positive patients . 
finally , axillary lymph node status today is less relevant to selecting patients for systemic therapy , since adjuvant chemoor endocrine therapy is recommended for increasing proportions of lymph node - negative patients [ 10 , 11 ]  . 
 model systems , allowing the prediction of axillary lymph node status without histopathologic analysis of the lymph node tissue itself may very well help to specifically select patients at high risk for axillary lymph node metastases and hence reduce the number of patients requiring axillary lymph node dissection . 
recent evidence suggests , that lymph node involvement indicates a more aggressive phenotype of the primary tumor rather than just a later time point of the diagnosis during the natural course of the disease [ 4 , 23 , 27 ]  . 
a strategy to assess the risk of axillary lymph node involvement based on tumorbiological parameters of a core biopsy prior to surgery complemented by new technologies to reveal a subclinical tumor cell spread [ 7 , 8 , 14 , 15 ] may provide all information needed for a decision whether or not axillary lymph node dissection should be performed . 
this may result in a better selection of patients to be referred to axillary lymph node dissection in order to avoid overtreatment , although it needs to be demonstrated that patients not predicted correctly by such a model system do not have worse outcome . 
 patients and methods patients breast cancer patients with operable tumor stage pt1pt3 m0 treated at the department of obstetrics and gynecology of the university of erlangen - nuremberg , erlangen , germany , met the eligibility criteria for this study . 
all patients were treated with either breast - conserving surgery ( n = 354 ) or modified radical mastectomy ( n = 301 ) including axillary lymph node dissection ( at least ten nodes resected )  . 
expression of estrogen ( er ) and progesterone receptors ( pr ) , ki - 67 , p53 , cathepsin d , her2 , s - phase fraction , and ploidy were determined in the primary tumor by immunohistochemistry . 
prediction criterion was a dichotomous variable indicating the pathologic result of the axillary lymph node dissection revealing either no lymph node metastases or at least one metastatic axillary lymph node in multilevel h&e analysis . 
the model was then validated by ( cid : 1 ) 2 - test comparing the prediction of axillary lymph node status by the model to the histopathologic result , again assuming statistical significance at p < 0.05. 
in 436 patients complete datasets of tumorbiological factors ( expression of er and pr , ki - 67 , p53 , cathepsin d , her2 , s - phase fraction , ploidy ) were available . only these patients were included into the logistic regression to identify independent predictors for lymph node involvement ( training set )  . 
prediction of axillary lymph node status prediction of axillary lymph node status based on the expression of pr , ki - 67 , and her2 was then applied to 654 patients . 
defining a high - risk group of patients with negative pr status , ki - 67 expression > 18% of the cells , and her2 overexpression , 118 of 124 ( 95.2% ) patients were correctly predicted to be lymph node - negative ( table 5 )  . 
there was also a highly significant correlation of risk prediction of axillary lymph node status by tumorbiological factors and survival ( p < 0.0001 for os , p < 0.0003 for dsf ; figure 1 )  . 
comparing the group defined by tumorbiological factors as extremely high risk ( er negative , ki - 67 18 , her2 positive ) versus extremely low risk ( er positive , ki - 67 18 , her2 negative ) , a mean survival time of 60 months versus 137 months for dsf and 70 months versus 139 months for os was recorded , which was also highly significant ( table 6 )  . 
 analyzing the survival of the four patient groups correctly predicted positive , false positive , correctly predicted negative , and false negative , there was no difference in dfs as well as in os between patients in whom prediction was either false positive or negative ( figure 2 )  . 
taking this into consideration , surgical procedures already changed over the last decade limiting axillary lymph node dissection to level 1 and 2 lymph nodes or just sentinel lymph node biopsy prior to a decision for more advanced surgery [ 3 , 17 , 21 , 26 ]  . 
 ln negative ln positive predicted ln - negative predicted ln - positive 263 87 350 189 115 304 452 ( 100% ) 202 ( 100% ) 654 ( 100% ) table 5 . 
 due to recent advances in detection of early breast cancer the number of lymph node - negative patients is increasing and , simultaneously , a decrease in mean tumor size at the time of diagnosis is observed [ 34 ]  . 
nevertheless , in the majority ( 53.4% ) of our patients treated for breast cancer , axillary surgery was unnecessary in order to achieve complete resection , since these patients were lymph node - negative . 
therefore , parameters predicting negative axillary lymph node status and providing information about prognosis comparable to the prognostic value of the axillary lymph node status are urgently needed [ 19 , 20 , 32 , 33 ]  . 
the tissue obtained by this procedure can easily be analyzed for tumorbiological parameters such as steroid receptor status , ki - 67 expression , her2 , and various other parameters . 
interestingly , patients predicted to be lymph node - negative but being node - positive in histopathologic analysis had significantly less lymph nodes involved than patients correctly predicted to be positive . 
survival according to prediction of axillary lymph node status by tumorbiological parameters : patients predicted correctly ( left ) , patients predicted false positive / false negative ( right )  . 
 the approach used in our study may be further improved by including additional parameters into the prediction strategy [ 5 , 6 , 19 , 20 , 22 ]  . 
considering the unnecessary side effects of axillary surgery in the majority of breast cancer patients today , surgical strategies have to be reconsidered based on risk prediction in order to avoid overtreatment . 
 strahlentherapie und onkologie original article radiation induced lung reactions in breast cancer therapy modulating factors and consequential effects wolfgang drr1 , 2 , simone bertmann1 , thomas herrmann1 background and purpose : radiologic reactions in lung , usually subclinical , are a frequent side effect of radiotherapy for breast cancer . 
 patients and methods : retrospectively , 451 patients irradiated postoperatively between 1992 and 1995 at the department of radiotherapy of carl - thiem - klinikum ( cottbus , germany ) were analyzed . 
in patients with reversible observations in standard chest radiography from 15 weeks to 1 year , ct or high - resolution ( hr - ) ct scans were analyzed after 47 years . 
 key words : radiotherapy lung pneumonitis fibrosis breast cancer tamoxifen age strahlenther onkol 2005 ; 181 : 56773 doi 10.1007 / s00066 - 005 - 1457 - 9 strahlenreaktionen der lunge bei der therapie von mammakarzinomen . 
 patienten und methodik : in die retrospektive analyse wurden 451 patientinnen einbezogen , die zwischen 1992 und 1995 in der klinik fr strahlentherapie des carl - thiem - klinikums cottbus eine postoperative strahlentherapie erhalten hatten . 
bei patientinnen mit reversiblen vernderungen in der standard - thoraxaufnahme zwischen 15 wochen und 1 jahr wurden ct oder hochauflsende ( hr - ) ct - untersuchungen zwischen 4 und 7 jahren ausgewertet . 
alter ( > 58 jahre ; p = 0 , 0127 ) und tamoxifen ( p = 0 , 0001 ) stellten sich als signifikante einflussfaktoren fr die frhe pneumopathie dar . 
spte radiologische vernderungen zeigten sich bei 94 / 425 patientinnen ( 22 , 1% ) , die alle auch frhe vernderungen aufgewiesen hatten ( p = 0 , 001 )  . 
 1 department of radiotherapy and radiooncology , medical faculty carl gustav carus , university of technology , dresden , germany , 2 experimental center , medical faculty carl gustav carus , university of technology , dresden , germany . 
analysis of lung reactions in this patient population can serve two purposes : first , it can be used as a model for radiobiological studies of normal lung tissue , not compromised by tumor burden and tumor response to treatment , in contrast e.g. , to patients with bronchial carcinoma . 
radiologic endpoints , from examinations with conventional thorax radiography , computed tomography ( ct ) or high - resolution ( hr - ) ct , are the dominant parameter ; less frequently , clinical parameters are assessed . 
a total of 451 patients , treated postoperatively between 1992 and 1995 at the department of radiotherapy of carl - thiem - klinikum in cottbus , germany , were analyzed . 
 patients and methods patients characteristics files of patients receiving postoperative radiotherapy for breast cancer at the department for radiotherapy of carlthiem - klinikum in cottbus , germany , from 1992 to 1995 were reviewed . 
chemotherapy was defined as an exclusion criterion because it might add in an unknown manner to the pulmonary toxicity of the treatment , and the present study was focused on radiation effects proper . 
the median age at the onset of radiotherapy was 61 years ( range 2683 years ) in the me group , and 57 years ( range 2079 years ) in the bct group . 
tamoxifen ( usually 30 mg / d ) was administered to a total of 221 patients , 171 / 296 ( 57.7% ) in the me group , and 50 / 155 ( 32.2% ) in the bct group . 
in the me group , irradiation of the axillary , supraclavicular and parasternal lymphatics was included as well as of the thoracic wall according to the strategy of the department in the time period under investigation . 
a four - field technique was applied , with oblique anterior posterior fields ( fields 1 and 2 ) to the axilla and supraclavicular region , a parasternal field ( field 3 ) , and an electron field ( field 4 ) adjusted to the size of the scar region at the thoracic wall . 
radiation induced lung reactions in breast cancer therapy fields 1 and 2 resulted in a homogeneous exposure of apical and lateral parts of the lung with 25 2.0 gy , with the volume exposed depending on the patients anatomy . 
 in patients with bct and pnx and pn12 ( group bct1 ) , the breast and ipsilateral axilla were included in the treatment volume ( n = 131 )  . 
the patients received 30 2.0 gy normalized to the center of the mamma , resulting in an 80% isodose of 30 1.6 gy to breast and axilla ( and the lung volume exposed )  . 
for this follow - up time point , a total of 346 radiographs were available , which were reexamined by specialists for radiotherapy or radiology at carl - thiemklinikum in cottbus . 
these were recalled for further follow - up in 1999 ( 47 year after radiotherapy ) , when seven of the patients had deceased , and three did not comply . 
 classification of radiation pneumopathy clinical symptoms of radiation pneumopathy were defined as dry cough , cough with sputum , increased body temperature , dyspnea and respiration - related thoracic pa these symptoms reflect the grading according to rtog / eortc [ 28 , 29 ]  . radiologic signs of pneumopathy were defined in more detail than in the rtog / eortc or lent / soma classification . 
multivariate analyses of variance were done with the general linear models ( glm ) procedure of sas [ 24 ] , for the influence of age and tamoxifen treatment on pneumonitis ( at 15 weeks ) and the influence of age , tamoxifen and pneuresults the incidence of clinical symptoms and radiologic changes at 15 weeks and 1 year after radiotherapy is illustrated in figure 1 . 
 in all patients , first clinical symptoms of pneumonitis developed before the first follow - up examination at 15 weeks , i.e. , at 6 weeks in one case and at 78 weeks after the end of radiotherapy in all other patients . 
the patients received postoperative radiotherapy after mastectomy ( me , n = 296 ) , or breast - conserving therapy ( bct ) , in the latter group locoregional ( bct1 , n = 131 ) or local radiotherapy ( bct2 , n = 24 )  . 
die patientinnen erhielten eine postoperative strahlentherapie nach mastektomie ( me , n = 296 ) oder nach brusterhaltender therapie ( bct ) eine lokoregionre ( bct1 , n = 131 ) oder lokale bestrahlung ( bct2 , n = 24 )  . 
incidence of early pneumopathy , at 15 weeks after the end of radiotherapy , in patients with ( left panel , n = 221 ) or without ( right panel , n = 230 ) administration of tamoxifen . 
inzidenz der frhen pneumopathie , 15 wochen nach ende der strahlentherapie , bei patientinnen mit ( linke abbildung , n = 221 ) oder ohne ( rechte abbildung , n = 230 ) tamoxifengabe . 
 451 ( 296 / 131 / 24 ) yes in patients with tamoxifen treatment ( n = 221 ) , 86 developed pneumopathy ( 38.9% ) , with 30.2% in patients 58 years , and 44.4% in older patients ( figure 2 ) , in contrast to 48 / 230 ( 20.9% ; punivar = 0.0065 ) in the group without tamoxifen , with 16.4% in patients 58 years , and 27.8% in older patients ( figure 2 )  . 
in patients with a reversion of the response from 15 weeks to 1 year ( shaded group ) , a ct or hr - ct analysis was added between 47 years after radiotherapy . 
bei patientinnen mit positiven reaktionen nach 15 wochen , bei denen nach 1 jahr keine vernderungen festgestellt wurden ( schattiert ) , wurde nach 47 jahren eine weitere ct oder hr - ct ausgewertet . 
of the 317 patients without early pneumopathy , 17 were not available for follow - up , and 300 had no pneumopathy at 1 year ( figure 4 )  . 
 multivariate analysis revealed a significant effect of pneumopathy at 15 weeks ( p < 0.0001 ) , while age ( p = 0.1245 ) and tamoxifen treatment ( p = 0.2242 ) were not identified as significant sources . 
 patients with pneumopathy at 15 weeks with no radiologic ( x - ray ) changes at 1 year were subjected to analyses of ct or hr - ct scans at 47 years after radiotherapy . 
radiation induced lung reactions in breast cancer therapy external ct scans had revealed fibrotic changes , and similar changes were found in five hr - cts of the remaining patients . 
another instance , where lung reactions are frequently seen , although in only a small fraction of the total lung volume , and hence usually asymptomatic , is in patients treated for breast tumors . 
therefore , the present , retrospective study was initiated in 451 patients to address the question of dependence of radiation pneumopathy on age and hormonal treatment at the time of radiotherapy . 
all patients received homogeneous radiation exposure of the lung with 2.0 gy per fraction to total doses of 5060 gy in strictly conventional , daily fractionated protocols , thus excluding effects of varying dose per fraction . 
the highest incidence of clinical pneumonitis was observed in the me group and no reactions in the group with exclusive irradiation of the breast , despite higher doses in the bct groups , particularly the group with inclusion of the axilla in the treatment volume ( bct1 )  . 
it is well known from preclinical [ 11 ] and clinical studies [ 17 , 30 , 32 ] that in contrast to radiologic changes clinical symptoms of pneumopathy are highly dependent on the lung volume exposed , and hence this difference can be attributed to the smaller irradiated volume in the bct groups . 
corresponding data from the literature range between 0% and 34% [ 5 , 16 , 22 , 25 ] , with higher incidences associated with a higher number of fields , again indicating the volume effect for symptomatic radiation reactions . 
 [ 30 ] , maximum radiologic changes reflecting pneumonitis occur between 1420 weeks after the onset of radiotherapy , and hence the endpoint in the present study reflects pneumonitis progressing into p < 0.0001 no pneumonitis pneumonitis figure 4 . 
frequency of radiographic changes in irradiated lung tissue at 1 year or later , reflecting fibrosis , in patients without or with positive radiographic changes ( standard chest radiography ) at 15 weeks after radiotherapy . 
the latter , particularly close to the pleura , may have prevented detection of a fraction of pneumonitic / fibrotic changes , particularly in very small volumes , in the present study . 
as volumes in the bct groups were significantly smaller than in the me group , this may explain the lower incidence of radiologic changes in the bct groups , which were observed despite higher doses compared to the me group . 
 in contrast , more recent studies in breast cancer patients [ 3 , 9 , 14 , 22 ] and lung cancer patients [ 5 , 18 , 26 ] did not confirm the age dependence . 
 [ 15 ] report an increase in pulmonary changes in ct scans by tamoxifen in a total of 422 breast cancer patients , which , however , did not reach statistical significance . 
 basis for the effect of tamoxifen may be an induction of transforming growth factor ( tgf - ) ( cid : 2 ) [ 1 , 3 ] , which is a key molecule in the early signaling cascade eventually resulting in fibrosis [ 4 , 7 , 10 , 13 , 21 , 23 ]  . 
interestingly , the factors affecting early pneumopathy , i.e. , treatment group , age and tamoxifen administration , all were without an independent effect on changes after 1 year , when early pneumopathy was included as a source parameter in the multivariate analysis . 
 recent radiobiological studies , summarized in drr & herrmann [ 7 ] demonstrated , that the development of radiation pneumopathy is a complex dynamic process , which is initiated immediately after the exposure to radiation , and which progresses over long time periods , although in some phases at a subclinical level without morphological or functional changes , i.e. , during the latent time of the radiation effect . 
 the influence of the diagnostic procedure on the results is demonstrated in the present study , when patients with radiographically negative responses at 1 year , which were positive at 15 weeks , were reexamined with ct or hr - ct . 
the authors are grateful to the staff of the department of radiotherapy and the department for radiologic diagnostics of carl - thiem - klinikum cottbus , where the patients had been treated , for their assistance . 
 strahlentherapie und onkologie original article comparative analysis of the effects of belly board and bladder distension in postoperative radiotherapy of rectal cancer patients tae hyun kim , dae yong kim , kwan ho cho , young hoon kim , kyung hae jung , joong - bae ahn , hee jin chang , joo - young kim , hyo seong choi , seok - byung lim , dae kyung sohn , seung - yong jeong1 purpose : to compare the effect of reducing the irradiated small - bowel volume with the use of belly board , bladder distension or both methods combined , in patients with rectal cancer undergoing postoperative pelvic radiotherapy . 
all patients underwent four sets of ct scans under four different methods as follows : group i : empty bladder without the use of a belly board ; group ii : empty bladder with the use of a belly board ; group iii : bladder distension without the use of a belly board ; group iv : bladder distension with the use of a belly board . 
the conventional three - field treatment plan was made using a three - dimensional treatment planning systethe irradiated small - bowel volume was calculated at 10% intervals from 10% to 100% of the prescribed dose . 
 key words : rectal cancer belly board bladder distension small bowel postoperative radiotherapy strahlenther onkol 2005 ; 181 : 6015 doi 10.1007 / s00066 - 005 - 1398 - 3 vergleichende analyse der wirkungen eines bauchbretts und einer blasendehnung bei der postoperativen strahlentherapie von patienten mit rektumkarzinom ziel : vergleich der wirkung einer reduktion des bestrahlten dnndarmvolumens mittels bauchbrett , blasenfllung bzw . 
von allen patienten wurden vier ct - bilddatenstze angefertigt , wobei folgende vier methoden zum einsatz kamen : gruppe i : leere blase ohne verwendung eines bauchbretts ; gruppe ii : leere blase mit verwendung eines bauchbretts ; gruppe iii : blasenfllung ohne verwendung eines bauchbretts ; gruppe iv : blasenfllung mit verwendung eines bauchbretts . 
 ergebnisse : das volumen des bestrahlten dnndarms verringerte sich von gruppe i ber gruppen ii und iii bis gruppe iv in allen dosisbereichen stetig ( p < 0 , 001 )  . 
 schlussfolgerung : die blasenfllung erwies sich im vergleich zum bauchbrett als effektivere methode zur reduktion des bestrahlten dnndarmvolumens bei der postoperativen beckenbestrahlung von patienten mit rektumkarzinodie kombination von bauchbrett und blasenfllung zeigte eine zustzliche wirkung und verringerte das bestrahlte dnndarmvolumen am deutlichsten . 
 schlsselwrter : rektumkarzinom bauchbrett blasenfllung dnndarm postoperative strahlentherapie 1 research institute and hospital , national cancer center , goyang , gyeonggi , korea . received : december 2 , 2004 ; accepted : june 23 , 2005 strahlenther onkol 2005 no . 
comparative analysis of belly board and bladder distension introduction radiotherapy ( rt ) combined with chemotherapy plays an important role in the treatment of rectal cancers that invade through the rectal wall or involve lymph nodes [ 4 , 7 , 10 , 15 ]  . 
the main factors predisposing to small - bowel complication are the irradiated small - bowel volume , radiation dose , chemotherapy , sequence of surgery and chemoradiotherapy , and previous abdominal surgery [ 5 , 11 , 13 ]  . 
 to minimize the complication , radiation oncologists have mainly focused on reducing irradiated small - bowel volume [ 1 , 3 , 5 , 6 , 8 , 9 ]  . 
among the various methods for a reduction of the irradiated volume , belly board ( bb ) and bladder distension ( bd ) are the most commonly used methods to achieve maximal smallbowel protection during rt with or without prone positioning . 
most of these studies were limited to two - dimensional ( 2 - d ) analysis of the small - bowel volume using orthogonal planar radiographs that do not provide dose - volume information . 
however , thorough quantitative analysis of reducing the irradiated small - bowel volume by use of the above methods is needed , e.g. , comparison of respective effects , which of the techniques is superior , or the combined effect of these methods . 
 in rectal cancer patients treated with postoperative pelvic rt using a 3 - d planning system , the present study was carried out by dose - volume analysis to compare the effect of using bb alone , bd alone and the two methods combined , on the reduction of irradiated small - bowel volume . 
 patients and methods patients between december 2003 and june 2004 , 20 consecutive patients ( ten male and ten female ) with rectal adenocarcinoma scheduled to receive postoperative pelvic rt were prospectively evaluated . 
according to rectal examinations , the median size and distance from anal verge of the primary tumor were 5.5 cm ( range : 17 cm ) and 8 cm ( range : 112 cm ) , respectively . 
two sets of transverse images were taken at 1 cm thick intervals from the upper portion of the diaphragm to 5 cm inferior to the perineum in the prone position , first without , the with the bb . 
thus , all patients underwent four sets of ct scans under four different methods as follows : group i : empty bladder without the use of a bb ; group ii : empty bladder with the use of a bb ; group iii : bd without the use of a bb ; group iv : bd with the use of a bb . 
 the bb used was a polyurethane foam board ( 180 cm 50 cm 8 cm ) with a rectangular aperture ( 25 cm 25 cm ) , located 100 cm from the caudal end of the board , for the belly region . 
the bb used for the simulator had a lead wire attached to the caudal edge of the aperture for clear identification on simulation films and pilot images of ct simulation . 
 radiation treatment planning all patients had their targets defined in accordance with the international commission on radiation units and measurements report ( icru 50 ) as follows : clinical target volume ( ctv ) included the primary tumor bed and regional lymphatics [ 12 ]  . 
since the lymphatics follow vascular structures , the distal common and internal iliac vessels were included , plus a 5 - mm margplanning target volume ( ptv ) included ctv plus a 15 - mm margthe superior border was placed at the l5 / s1 and the inferior border at > 3 cm caudal to the primary tumor bed . 
a conventional three - field treatment plan , composed of a 6 - mv photon posterior - anterior field and 15 - mv photon opposed lateral fields with wedges of 45 , was made using the treatment planning syste beam weights of the three - field plan were equal . 
comparative analysis of belly board and bladder distension volume of the small bowel within the radiation field was calculated at 10% dose intervals between 10% and 100% of the prescribed dose . 
for each dose level , the effect of the bb and bd on the irradiated small - bowel volume was analyzed using kruskal - wallis , wilcoxon signed rank , and wilcoxon rank sum tests . 
definitions : group i : empty bladder without the use of belly board ; group ii : empty bladder with the use of belly board ; group iii : distended bladder without the use of belly board ; group iv : distended bladder with the use of belly board . 
definitionen : gruppe i leere blase ohne verwendung eines bauchbretts ; gruppe ii leere blase mit verwendung eines bauchbretts ; gruppe iii blasenfllung ohne verwendung eines bauchbretts ; gruppe iv blasenfllung mit verwendung eines bauchbretts . 
for groups ii and iii , the group i group ii group iii group iv results a wilcoxon rank sum test the median volume of the total small bowel was 964.5 cm3 ( mean : 991.7 cm3 , standard deviation : 185.4 cm3 ) in group i , 965.5 cm3 ( mean : 992.6 cm3 , standard deviation : 187.3 cm3 ) in group ii , 962.8 cm3 ( mean : 991.9 cm3 , standard deviation : 185.0 cm3 ) in group iii , and 969.0 cm3 ( mean : 992.8 cm3 , standard deviation : 187.4 cm3 ) in group iv . 
 the total small - bowel volume and the mean volume of irradiated small bowel ( mean standard deviation , cm3 ) at the 50% dose level according to age and gender are summarized in table 1 . 
the irradiated smallbowel volume ( mean standard deviation , cm3 ) for the four groups at 10% intervals from 10% to 100% of the prescribed dose is summarized in normalized dose ( % ) figure 1 . 
compared with group i , the absolute reductions of irradiated small - bowel volume in groups ii , iii , and iv were more prominent at lower dose levels ( 10% to 20% dose ) and the relative reductions were more prominent between 30% and 100% dose levels . 
 discussion the effectiveness of bb and bd on reducing the irradiated small - bowel volume has been demonstrated in previous studies [ 3 , 5 , 9 , 14 ] , but direct comparison between these two methods is difficult due to the following reasons . 
before we started this study , we assumed the impact of bd might be equivalent to , or more effective than bb , so uniformity of bladder status was necessary . 
 initially , we thought gender could influence the reduction of the irradiated small - bowel volume because of the difference of pelvic anatomy , e.g. , the shape and size of bony pelvis or the presence of a uterus . 
thus , the present study was carried out on the basis that inconsistencies in previous studies left many questions unanswered regarding the comparison of effects from bb and bd alone or in combination , on irradiated small - bowel volume . 
 our study demonstrated that using either the bb or bd reduced the irradiated small - bowel volume better than prone position alone , with the bd being more effective than the bb . 
some studies reported that a region of small bowel receiving 15 gy correlated with acute small - bowel toxicity and a region of small bowel receiving 45 gy correlated with late gastrointestinal toxicity [ 2 , 5 ]  . 
in pilot studies , we used relatively large aperture sizes of 35 cm 35 cm or 30 cm 30 cm , but this caused hyperlordosis of the lumbar spine and rolling of the pelvis , which induced poor setup accuracy without reduction of irradiated smallbowel volume . 
we have used bb for patients with permanent or temporary stoma to avoid discomfort and body distortion caused by stoma , but we sometimes adopted the combined method of bb and bd for the high - risk patients such as patients who have had extensive pelvic surgery and previous abdominal or pelvic rt history to minimize the irradiated small - bowel volume . 
 strahlentherapie und onkologie current discussion the development of quality assurance programs for radiotherapy within the german hodgkin study group ( ghsg ) introduction , continuing work , and results of the radiotherapy reference panel * rolf - peter mller , hans theodor eich1 background and purpose : the german hodgkin study group ( ghsg ) , including more than 500 participating centers , established a central radiotherapy ( rt ) reference center to improve quality of treatment , starting with the first study generation in 1978 . 
 material and methods : a panel of expert radiation oncologists ( second study generation hd46 , 19881994 , and third study generation hd79 , 19931998 ) retrospectively evaluated the adequacy of treatment fields , applied radiation doses , treatment time , and technical parameters . 
new rt qaps were initiated according to the demands of the new trials and former programs were enhanced : ( 1 ) central prospective radiation oncologic review of cross - sectional imaging ( hd10 , hd11 ) to create the individual radiation treatment plan ; ( 2 ) retrospective analysis of the adequacy of the performed involved - field ( if ) rt ( hd10 , hd11 ) ; ( 3 ) the multidisciplinary hd12 panel ( radiation oncologists , medical oncologists , diagnostic radiologists ) ; ( 4 ) initiation and integration of a teleradiotherapy network into the ghsg trials . 
 results : a strong achievement of these activities in the era of extended - field rt was to show that major deviations of radiation treatment portals and radiation dose from prospective treatment prescriptions revealed to be unfavorable prognostic factors for patients with early - stage hl ( hd4 )  . 
the central prospective radiation oncological review of all diagnostic imaging ( hd10 , hd11 ) showed that corrections of disease involvement in 49% of patients ( 593 / 1 , 214 ) with early stages ( hd10 ) and in 67% of patients ( 936 / 1 , 397 ) with intermediate stages ( hd11 ) were necessary . 
in the hd12 trial ( advanced stages ) , a multidisciplinary panel of radiation oncologists , radiologists and medical oncologists reviewed all the diagnostic imaging from diagnosis throughout the treatment in comparison to the documentation forms . 
after chemotherapy , 599 patients ( 56% ) showed residual disease ( > 1.5 cm ) , and in 145 / 1 , 080 patients ( 13.5% ) the panel recommended additional rt independent of the randomization arthe introduction of electronic image transfer optimized and simplified the workflow of the qaps . 
for early favorable and unfavorable hl a central prospective review of all diagnostic imaging is performed by expert radiation oncologists to control the disease extension and to define the if treatment volume . 
participants are trained on the definition of if - rt by strahlenther onkol 2005 ; 181 : 55766 doi 10.1007 / s00066 - 005 - 1437 - 0 on the occasion of his 80th birthday . 
the introduction of teleradiotherapy into the ghsg trials improves the dialogue between the central rt reference center and study participants and thus contributes to high rt quality for study patients . 
die vorliegende arbeit soll die erfahrungen dieser bemhungen und die ergebnisse der durchgefhrten und derzeit praktizierten qsp aufzeigen . material und methodik : von einem expertengremium ( zweite studiengeneration hd46 , 19881994 , und dritte generation hd79 , 19931998 ) wurde nach erfolgter rt eine retrospektive qualitative bewertung aller patienten hinsichtlich angewandter bestrahlungstechniken , bestrahlter volumina und des verhltnisses von bestrahlungszeit zu verabreichter strahlendosis vorgenommen . 
 ergebnisse : auswertungen dieser systematischen analysen konnten fr die alleinige extended - field - rt nachweisen , dass abweichungen von den prospektiv erstellten bestrahlungsplnen einen ungnstigen prognosefaktor fr patienten mit hl in frhen stadien darstellen ( abbildung 1 )  . 
bei 49% der patienten ( 593 / 1 214 ) in frhen stadien ( hd10 ) und in 67% der patienten ( 936 / 1 397 ) in intermediren stadien ( hd11 ) waren korrekturen der befallenen regionen notwendig . 
diese korrekturen hatten einen signifikanten einfluss auf das korrekte krankheitsstadium , die zuordnung zur adquaten behandlungsgruppe und auf die ausdehnung des if - rt - volumens ( tabelle 2 )  . 
599 patienten ( 56% ) zeigten nach der chemotherapie einen resttumor ( > 1 , 5 cm ) , fr 145 / 1 080 patienten ( 13 , 5% ) empfahl das panel eine additive rt unabhngig vom randomisationsardie einfhrung eines elektronischen bildtransfers konnte die arbeitsablufe dieser qsp weiter optimieren . 
relevante bilddaten des patienten knnen vor rt - beginn dem referenzzentrum nicht nur zur prospektiven erstellung eines rt - plans , sondern auch zur berprfung der bestrahlungsvolumina zur verfgung gestellt werden . 
basierend auf den ergebnissen der prospektiven rt - planung und der retrospektiven beurteilung der if - rt werden die studienteilnehmer auf den jhrlich stattfindenden studiengruppentreffen sowie auf dem deutschen kongress fr radioonkologie ( degro ) ber die korrekte dokumentation des hl und ber die adquate durchfhrung der if - rt informiert . 
in five consecutive generations of studies , therapy switched from extendedfield radiotherapy ( ef - rt ) only to a balanced application of polychemotherapy and reduced radiation volumes and doses , resulting in cure rates of 8090% , independent of anatomic stage and histological subtype ( table 1 )  . 
five generations of randomized clinical trials ( hd1 / hd3 , hd4hd6 , hd7hd9 , hd10hd12 , hd13hd15 ) in the treatment of primary early favorable , intermediate ( early unfavorable ) , and advanced stage hodgkins lymphoma . 
fnf generationen randomisierter klinischer studien ( hd1 / hd3 , hd4hd6 , hd7hd9 , hd10hd12 , hd13hd15 ) zur behandlung frher , intermedirer und fortgeschrittener stadien des hodgkin - lymphoms . 
one important achievement of these activities in the era of ef - rt was to show that deviations of radiation treatment portals and radiation doses from prospective treatment prescriptions proved to be unfavorable prognostic factors for patients with early stage hl ( figure 1 ) [ 4 , 5 ]  . 
here , new rt - qaps were initiated according to the demands of the new trials and former programs were enhanced : ( 1 ) central prospective radiation oncologic review of crosssectional imaging in hd10 and hd11 to have a complete information for creating the radiation treatment plan ; ( 2 ) retrospective analysis of the adequacy of the performed if - rt in hd10 and hd11 ; ( 3 ) the multidisciplinary hd12 panel of the ghsg ( radiation oncologists , medical oncologists , diagnostic radiologists ) ; ( 4 ) initiation and integration of teleradiotherapy into the ghsg trials . 
 central prospective radiation oncologic review of cross - sectional imaging in hd10 and hd11 since radiation treatment fields and volumes as well as radiation doses changed dramatically in the past 2 decades and combined - modality management ( chemotherapy plus if - rt ) has proven to be the treatment of choice for early and intermediate stages of hl , the exact documentation and evaluation of patients individual spread and stage of disease , based on clinical data and diagnostic imaging , become more and more important in multicenter trials [ 19 , 21 ]  . 
an individual rt prescription was provided for every study patient . procedure of the central prospective radiation oncologic review all participating study centers ( both the responsible radiation oncologist and the medical oncologist ) were requested to score disease involvement at a total of 34 possible anatomic sites on crf ( figure 2 ) and to determine the stage of disease accordfigure 1 . 
relapse - free survival ( rfs ) to presence ( n = 127 ) or absence ( n = 242 ) of a relevant radiotherapy protocol violation ( pv )  . 
 the study group successfully evaluated different dose effect relationships and could also prove the efficacy of involved - field radiotherapy ( if - rt ) in early and intermediate stages in combination with effective chemotherapy [ 68 , 14 ]  . 
at present , a radiation dose of 30 gy to the involved lymph node areas after a not too aggressive chemotherapy ( two cycles abvd ) should be the standard for early and favorable stages of hodgkins lymphoma ( hl )  . 
 preliminary results of the own and other groups may show , that additive rt after intensive chemotherapy might be useful for elective subgroups of patients , e.g. , after no complete remission [ 8 , 23 ]  . 
in the ghsg trials , the tracheal bifurcation reflected the anatomic border between the upper and lower mediastinulymph node involvement exclusively above the tracheal bifurcation was differentiated from involvement below the bifurcation . 
in case of a superior mediastinal involvement only , the lower field border was one vertebral body below the tracheal bifurcation . 1 waldeyers ring upper cervical cervical 7a supraclavicular infraclavicular axillary lung hilum 17a liver hilum 17b celiac 18 mesenterial iliac inguinal lung right liver 26 skeleton 27 bone marrow 2 waldeyers ring upper cervical cervical 8a supraclavicular infraclavicular 10 axillary lung hilum 19 spleen 20 splenic hilum 21 paraaortal iliac inguinal lung left 28 pleura 29 pericardium 30 other organ involvement 11a upper mediastinum 11b lower mediastinum the crf as well as all diagnostic images ( ct , mri and x - rays ) were sent to the rt reference center in cologne , germany . 
 criteria for reevaluation were any abnormalities on chest radiographs and ct / mri scans suspicious of disease , in particular taking the size and form of lymph nodes ( > 1.5 cm ) and any extra lymphatic disease based on widely accepted standards in radiology into account . 
site , extent and spread of disease were marked in a schematic figure , as was the resulting individual treatment field for the if - rt ( figure 3 )  . 
 results of the central prospective radiation oncologic review complete sets of documentation ( crf as well as ct , mri and x - rays images ) of 1 , 214 / 1 , 371 patients ( 89% ) in hd10 and 1 , 397 / 1 , 570 patients ( 89% ) in hd11 were submitted to the reference center . 
 comparison of the documented disease by the study centers and the experts statement the evaluation of the qap showed that a considerable proportion of involved sites were not recorded or incorrectly recorded on the corresponding crf by the participating center . 
 for patients with early - stage hl ( hd10 ) there was a correction of disease involvement in 49% ( 593 / 1 , 214 patients ) , for patients with intermediate stages ( hd11 ) in 67% ( 936 / 1 , 397 patients ) ( table 2 )  . 
total number of reviewed patients in the hd10 and hd11 trials and impact of the quality assurance program on the correctness of stage definition , allocation to treatment groups , and extension of the involved - field radiotherapy ( if - rt ) volume . 
anzahl der beurteilten patienten in der hd10und hd11studie ; einfluss des qualittssicherungsprogramms auf das korrekte lymphomstadium , die korrekte zuordnung zur behandlungsgruppe und die ausdehnung des involved - field - radiotherapie - ( if - rt - ) volumens . 
 considering disease stage as revised and the guidelines of the protocol , 93 of the 1 , 529 patients ( 6% ) had to be treated in a different protocol ( table 2 ) : in the hd10 trial 36 patients were qualified for the hd11 trial ( intermediate stages )  . 
in the hd11 trial 27 patients were qualified for the hd10 trial and 30 patients for the hd12 trial ( advanced stages ) due to changes of stage and risk factors . 
in 13 / 93 patients changes of the risk factor extranodal involvement and in 17 / 93 patients changes of the risk factor bulky mediastinal mass led to a shift into a different treatment protocol . 
 influence on the radiation treatment volume due to the incorrect lymph node documentation of the participating study centers the radiation treatment volume had to be enlarged in 891 / 2 , 611 ( 34% ) patients and reduced in 82 / 2 , 611 ( 3% ) patients . 
according to the most frequently corrected lymph node sites , the changes of the if - rt volume particularly affected the lower mediastinum , pulmonary hilar and neck lymph nodes . 
typical individualized treatment prescription for the involvedfield radiotherapy after centralized data review : patient with stage iia hodgkins disease , with one side of the neck and superior mediastinal involvement only . 
most discrepancies were seen in the lower mediastinum ( 23% ) , infraclavicular ( 17% ) , upper cervical ( 16% ) , supraclavicular ( 13% ) and pulmonary hilar region ( 13% ) ( figure 4 )  . 
 revision of stage and influence on treatment protocol the comparison of the documented disease by the participating study centers and the experts statement resulted in a change of disease stage in 41 of those 1 , 529 patients ( 2.7% ) , whose documented disease involvement had to be corrected . 
in 7 / 14 patients the reference center negated extranodal involvement : there were no findings of contiguous bone involvement with regard to conventional x - ray and mri in three patients and no ct findings of lung involvement in three further patients . 
 such a review process has to be distinguished from other qaps for rt as described by the eortc [ 2 , 1518 , 28 ] , the rtog [ 20 ] , and the qarc for pediatric trials [ 24 ]  . 
these groups analyzed clinical and technical rt parameters such as radiation dose ( dosimetry ) and treated volume ( control of simulation and verification films ) after diagnosis and treatment decision for rt . 
in contrast to these programs , the current reported qap had been performed prospectively at the start of therapy , comparable to a centralized pathology review process , which is also integrated into the ghsg trials . 
 in the current analysis the most common site of disagreement was the mediastinuthis is possibly due to the study protocol definition of the tracheal bifurcation being the anatomic border between the upper and lower mediastinuinconsistent ct interpretation of hilar lymphadenopathy has been recognized previously and was apparent here [ 13 ]  . 
since radiation oncologists in germany must receive at least 1 year of training in diagnostic radiology during their education , they should be familiar with the interpretation of cross - sectional imaging . 
in the routine use of if - rt in combined - modality treatment protocols for hl , it is mandatory that the treating radiation oncologist looks at the ct scans personally in order to plan the rt fields . 
apparently , the external medical and radiation oncologists sometimes documented the disease involvement on the basis of the radiologic report , but the primary radiologists were not always familiar with the scoring systems in hl or might have had no sufficient information . 
proportion of disagreements of involved anatomic regions between the experts statement and the documentation forthis is shown anatomic site based ( n = 2 , 724 [ 100% ] changes of the involved anatomic sites )  . 
the reviewing radiologists and radiation oncologists performed daily systematic analyses of all images for a large number of patients , focusing on involvement according to the individual spread and its potential impact on staging and if - rt volume . 
though this review process in hodgkin study protocols occupies time and personnel , it is justified for the use of if - rt where the individual extent of disease determines the extent of irradiation . 
 retrospective analysis of the adequacy of the performed involved field radiotherapy in hd10 and hd11 apparently , some of the differences between the documented disease involvement of the study centers and the based on the simulation films , verification films and radiation treatment protocols of the patients in the hd10 and hd11 strahlenther onkol 2005 no . 
the reference panel study centers got a precise rt prescription , most difficulties occurred in the adequate coverage of the if [ 22 ] as defined in the study protocol followed by faults in the rt technique ( figure 5 )  . 
 as a consequence , radiation oncologists are trained on the definition of if - rt on the ghsg meetings and on the annual meetings of the german society of therapeutic radiation oncology ( degro ) by members of the rt reference center of cologne . 
however , since combined modality therapy has been introduced into the management of early favorable and unfavorable stages , no significant influence of the quality of the performed rt on freedom of treatment failure could be shown [ 25 , 26 ]  . the multidisciplinary hd12 panel of the ghsg the hd12 protocol is a multicenter prospective randomized trial of the ghsg for advanced stages of hl . 
the indication and effectiveness of additional rt ( 30 gy ) in the area of initial bulky disease and of residual disease following intensive chemotherapy , using the beacopp schema , had to be investigated . 
the introduction of a multidisciplinary panel reviewing all patients imaging as a tool to secure or improve quality assurance of patients in a multicenter study has not been described yet [ 11 ]  . 
 procedure of the hd12 panel in the hd12 protocol for advanced stages of hl , all study participants were asked to send all diagnostic imaging and crf ( initial status , after four and eight cycles of chemotherapy ) to the rt reference center in cologne . 
 after chemotherapy 599 patients ( 56% ) showed residual disease ( > 1.5 cm ) , and for 145 / 1 , 080 patients ( 13.5% ) the panel recommended additional rt independent of randomization ar according to the quality of ct a total of 2 , 607 ct scans of 371 patients have been evaluated . 
conventional ct scanning consisted of sequential acquisition with a median thick section of 5 mm for the neck region , 10 mm for the thorax and 10 mm for the abdomen . 
the helical ct protocol included a median slice collimation , table feed and reconstruction interval for the neck of 5 mm / 7 mm / 5 mm , for the thorax of 8 mm / 12 mm / 8 mm , and for the abdomen of 8 mm / 12 mm / 8 m cts of the thorax were all adequately reconstructed at lung ( median : width , 1 , 600 hu ; center , 600 hu ) and mediastinal ( median : width , 350 hu ; center , 50 hu ) window settings . 
 initiation and integration of teleradiotherapy into the ghsg trials before initiation of the project teleradiotherapy which is part of the competence network malignant lymphoma , the qaps described above were performed via conventional mailing , which was moneyand time - consuming . 
 since the introduction of a teleradiotherapeutic workstation in the rt reference center in cologne in january 2001 , the images of 10% ( 856 patients ) of all reviewed cases of the ongoing hd1015 trials were delivered digitally . 
another possibility to get digital imaging was the introduction of a patients own cd - rom on which all relevant imaging , before and after the end of therapy , could be stored and offered to the rt reference centers . 
 our experiences with teleradiotherapy reveal that electronic imaging transfer between rt reference centers and study centers for the purposes of interpretation of radiologic images and planning individual rt based on standardized prescriptions is feasible . 
rapid online consultation and realtime teleconferences regarding disease involvement , patient management and communication of the treatment plan and of simulation as well as portal verification images between the remote hospitals are possible and helpful . 
 in the future , communication between the connected rt centers and further centers that are able to send diagnostic imaging digitally on mobile data carriers or via an isdn pointto - point connection will expand . 
the long - term aim is to build up a network of all those hospitals , institutions and private facilities taking part in the lymphoma studies to achieve an integrated system of cooperation . 
in comparison with conventional mailing procedures of radiologic / radiotherapeutic imaging , there are obvious possibilities for cost reduction , but additional research has to be performed in this field . 
for early favorable and unfavorable hl a central prospective review of all diagnostic imaging is performed by expert radiation oncologists to control the disease extension and to define the if treatment volume . 
the introduction of teleradiotherapy [ 9 ] into the ghsg trials improves the dialogue between the rt reference center and study centers and thus contributes to high rt quality for study patients . 
 patienten und methodik : 74 patienten , die zwischen 01 / 1995 und 12 / 2003 aufgrund einer mbrk bestrahlt wurden , erhielten eine re - rt bei erneuter mbrk in der vorbestrahlten region ( in - field - rezidiv )  . 
nach der multivarianzanalyse hatten die art des primrtumors ( p = 0 , 013 ) und die entwicklungszeit motorischer defizite vor re - rt ( p = 0 , 037 ) einen signifikanten einfluss auf die motorische funktion nach re - rt , nicht hingegen das fraktionierungsschema ( p = 0 , 560 ) , die kumulative eqd2 ( p = 0 , 795 ) , die gehfhigkeit vor re - rt ( p = 0 , 471 ) und das intervall zwischen primrer rt und re - rt ( p = 0 , 420 )  . 
 schlsselwrter : metastatisch bedingte rckenmarkkompression re - bestrahlung wirksamkeit myelopathie strahlenther onkol 2005 ; 181 : 595600 doi 10.1007 / s00066 - 005 - 1406 - 7 effectiveness and toxicity of reirradiation ( re - rt ) for metastatic spinal cord compression ( mscc ) background and purpose : radiation myelopathy is a serious late toxicity after radiotherapy ( rt ) of metastatic spinal cord compression ( mscc )  . 
 patients and methods : 74 patients , irradiated between 01 / 1995 and 12 / 2003 for mscc , were reirradiated for in - field recurrence of mscc ( table 1 )  . 
on multivariate analysis , outcome was significantly influenced by type of primary tumor ( p = 0.013 ) and by the time of developing motor deficits before 1 klinik und poliklinik fr strahlentherapie und radioonkologie , universittsklinikum hamburg eppendorf , 2 department of radiotherapy , academic medical center , amsterdam , niederlande , 3 department of radiotherapy , bernard verbeeten institute , tilburg , niederlande , 4 klinik fr strahlentherapie und nuklearmedizin , medizinische universitt lbeck , 5 mount vernon centre for cancer treatment , northwood , grobritannien . 
re - bestrahlung bei metastatisch bedingter rckenmarkkompression re - rt ( p = 0.037 ) , but not by radiation schedule ( p = 0.560 ) , by ambulatory status before re - rt ( p = 0.471 ) , by cumulative eqd2 ( p = 0.795 ) , nor by the interval between primary rt and re - rt ( p = 0.420 ; table 2 )  . 
 key words : metastatic spinal cord compression reirradiation effectiveness myelopathy einleitung verschiedene onkologische krankheitsbilder wie hirntumoren , hirnmetastasen oder die metastatisch bedingte rckenmarkkompression ( mbrk ) knnen zu motorischen defiziten fhren [ 4 , 7 , 1017 ]  . 
im fall einer erneuten rt ( re - bestrahlung [ re - rt ] ) kann es zu einer vergleichsweise hohen kumulativen eqd2 ( eqd2 der primren rt plus eqd2 der re - rt ) im rckenmark kommen [ 11 , 18 ]  . 
 patienten und methodik 74 patienten , die zwischen januar 1995 und dezember 2003 aufgrund einer mbrk bestrahlt wurden , erhielten eine re - rt bei erneuter mbrk in der vorbestrahlten region ( in - fieldrezidiv )  . 
wie bei der primren rt wurde die dosis mit 6bis 10 - mv - photonen ber ein dorsales stehfeld unter einschluss von ein bis zwei wirbelkrpern oberund unterhalb der lsionen appliziert . 
 die re - rt fhrte insgesamt bei 29 / 74 patienten ( 39% ) zu einer verbesserung der motorischen funktion , bei 34 / 74 patienten ( 46% ) zu einem status idem und bei 11 / 74 patienten ( 15% ) zu einer verschlechterung . 
darin zeigte sich ein signifikanter einfluss auf die motorische funktion nach re - rt fr die art des primrtumors und fr die entwicklungszeit motorischer defizite vor re - rt , nicht hingegen fr die anderen vier untersuchten variablen . 
whrend der re - rt kam es bei den patienten , die im bereich der brustwirbelsule bestrahlt wurden , in 19 / 52 fllen ( 37% ) zu einer belkeit grad 1 und in 12 / 52 fllen ( 23% ) zu einer dysphagie / sophagitis grad 1 . 
 [ 21 ] ; grad 0 : normale kraft ; grad 1 : gehfhig ohne hilfe ; grad 2 : gehfhig mit hilfe ; grad 3 : nicht gehfhig , paraparese ; grad 4 : komplette paraplegie . 
 der univariate vergleich der bei der re - rt verwendeten fraktionierungsschemata im hinblick auf die motorische funktion nach re - rt erfolgte mit dem ( cid : 3 ) 2 - test . 
der mediane beobachtungszeitraum nach re - rt betrug 9 monate ( bereich 242 monate ) bei den patienten , die eine kumulative eqd2 50 gy erhalten hatten , und 10 monate 1 monat n . 
derartige rezidive sind nach einer eigenen studie hufiger nach 1 8 gy oder nach 5 4 gy als nach 10 3 gy oder 20 2 gy zu beobachten [ 17 ]  . 
diesbezglich kann ein selektionsbias nicht sicher ausgeschlossen werden , da patienten mit einem in - field - rezidiv nach 1 8 gy vermutlich eher einem radioonkologen zur re - rt vorgestellt werden als patienten , die bereits eine gesamtdosis von 30 oder 40 gy erhalten haben . 
so waren 77% unserer patienten vor der re - rt gehfhig , und bei 46% der patienten betrug die entwicklungszeit der motorischen defizite vor re - rt > 14 tage [ 13 ]  . 
ferner lag eine prselektion vor , da nur patienten mit einem rezidiv eingeschlossen wurden , was strenggenommen eine verbesserung der motorischen funktion nach primrer rt oder mindestens einen status idem voraussetzt . 
 diese ergebnisse stehen in bereinstimmung mit vergleichenden studien zur primren rt der mbrk [ 12 , 14 , 16 , 17 ]  . eine ernstzunehmende sptfolge nach rt im bereich der wirbelsule ist die radiogene myelopathie , die zu schweren neurologischen ausfllen fhren kann . 
 untersuchte variablen art des primrtumors intervall zwischen primrer rt und re - rt entwicklungszeit motorischer defizite vor re - rt gehfhigkeit vor re - rt fraktionierungsschema bei re - rt kumulative eqd2 p - wert 0 , 013 0 , 420 0 , 037 0 , 471 0 , 560 0 , 795 ( laminektomie , dorsale stabilisierung ) ist in der regel nur bei befall von ein bis zwei rckenmarkssegmenten indiziert . 
in dieser literaturbersicht wurden neben der kumulativen biologisch effektiven dosis ( bed = 2 eqd2 fr ein / ( cid : 2 ) von 2 gy ) zwei weitere risikofaktoren beschrieben , das intervall zwischen primrer rt und re - rt sowie die hhere bed beider bestrahlungsserien . 
das risiko fr eine myelopathie war deutlich erhht , wenn das intervall zwischen beiden bestrahlungsserien < 3 monate war und / oder wenn die bed in einer bestrahlungsserie mindestens 102 gy2 ( entsprechend einer eqd2 von 51 gy ) betrug . 
 der einfluss des intervalls lsst sich durch eine signifikante langzeiterholung des rckenmarks erklren , die sowohl im tiermodell als auch fr das menschliche rckenmark beschrieben wurde [ 1 , 23 , 24 ]  . 
bei den zwlf patienten unserer serie , die eine kumulative eqd2 > 50 gy erhalten hatten , betrug das intervall zwischen primrer rt und re - rt median 10 monate ( bereich 433 monate )  . 
somit erscheint auch eine re - rt mglich , die zu einer kumulativen eqd2 von > 50 gy fhrt , wenn das intervall zwischen den bestrahlungsserien mindestens 4 monate betrgt . 
allerdings ist die anzahl der patienten mit einer kumulativen eqd2 > 50 gy sowohl in dieser analyse als auch in der literatur vergleichsweise gering , der nachuntersuchungszeitraum zumeist < 24 monate . 
dirk rades klinik und poliklinik fr strahlentherapie und radioonkologie universittsklinikum hamburg - eppendorf martinistrae 52 20246 hamburg telefon ( + 49 / 40 ) 42803 - 6139 , fax - 2846 e - mail : rades.dirk@gmx.net strahlenther onkol 2005 no . 
9 urban & vogel strahlentherapie und onkologie original article measurements of characteristics of time pattern in dose delivery in step - and - shoot imrt mattias schfer1 , marc mnter1 , florian sterzing1 , peter hring2 , bernhard rhein2 , jrgen debus3 background and purpose : although intensity - modulated radiotherapy ( imrt ) has already shown its clinical benefit , there are some issues which are not yet fully understood . 
a set of parameters was defined to describe the dose rate profiles including the effective fraction time ( eft , which is the percentage of the fraction time in which any dose is delivered to a specific point ) , and a quotient of the percentage of dose delivered in high dose pulses ( > 0.01 gy / s ) divided by the percentage of fraction time needed to deliver this dose ( dhd / thd )  . 
 key words : imrt dosimetry dose rates step - and - shoot strahlenther onkol 2005 ; 181 : 58794 doi 10.1007 / s00066 - 005 - 1289 - 7 charakterisierung der zeitlichen dosisverteilung in der step - and - shoot - imrt hintergrund und ziel : obwohl die intensittsmodulierte strahlentherapie ( imrt ) ihren klinischen nutzen bereits zeigen konnte , harren einige grundlegende fragestellungen noch immer ihrer antwort : beispielsweise konnte noch nicht zufriedenstellend gezeigt werden , ob die zeitliche dosisprotrahierung zu strahlenbiologischen konsequenzen fhrt , und wenn ja , zu welchen . 
des weiteren knnte eine solche charakterisierung zu neuen hinweisen bezglich der technischen optimierung der imrt fhren . material und methodik : es wurde ein neues phantom entwickelt , das die przise messung von bis zu neun punkten gleichzeitig mittels pin - point - ionisationskammern ermglicht . 
der quotient aus dem anteil der fraktionsdosis , der in hochdosispulsen appliziert wird ( > 0 , 01 gy / s ) , und dem anteil der dafr notwendigen fraktionszeit ( dhd / thd )  . 
bei beiden parametern wurden groe unterschiede sowohl innerhalb eines plans als auch zwischen den verschiedenen plnen beobachtet : beispielsweise variierten eft zwischen 11 , 6% und 37 , 3% und der anteil der fraktionszeit , in dem hochdosispulse ( und damit der hauptteil der dosis ) appliziert wurden , zwischen 3 , 6% und 10 , 1% der gesamten fraktionszeit . 
 1 clinical cooperation unit radiotherapy , german cancer research center ( dkfz ) , heidelberg , germany , 2 department of medical physics in radiotherapy , german cancer research center ( dkfz ) , heidelberg , germany , 3 department of radiology , university hospital heidelberg , germany . received : february 27 , 2004 ; accepted : june 10 , 2005 strahlenther onkol 2005 no . 
 schlsselwrter : imrt dosimetrie dosisrateneffekte step - and - shoot introduction in recent years intensity - modulated radiotherapy ( imrt ) has become an encouraging new technology in radiation oncology . 
current indications include complex - shaped tumors or tumors at problematic localizations [ 21 ] , especially tumors of the head and neck [ 9 , 13 , 20 , 22 , 26 ] or the prostate [ 7 , 32 , 33 ]  . 
it is the aim of this work to establish parameters which describe and quantify this pattern and the resulting inhomogeneities of dose delivery . approach , or static mlc - delivered imrt , which is one of the most common imrt techniques : the fraction dose is delivered in up to 100 small pulses between which the beam is switched off to let the gantry or the multileaf collimators move to their next position [ 4 ]  . 
 to avoid simplifications which might limit the value of our results , we decided to use real clinical patient plans both for dosimetric investigations and for the following cell culture experiments . 
 material and methods to fulfill the requests of our study , it was necessary to measure the dose delivered to any point of interest ( preferably more than one simultaneously ) at very short intervals during the irradiation . 
 phantom a new phantom had to be developed to be able to perform both measurements with ionization chambers ( preferably more than one at a time ) and forthcoming cell experiments in the same experimental setting . 
a new phantom of cylindrical shape made of pmma ( polymethylmethacrylate ) ; the revolving and shiftable inner core allows movement of the nine channels suited for ionization chambers as well as cryotubes for cell experiments . 
ein neues phantom von zylindrischer struktur aus pmma ( polymethylmethacrylat ) ; der drehbare und seitlich verschiebbare innere kern erlaubt die dreidimensionale positionierung sowohl von ionisationskammern als auch von cryotubes . 
by varying this arrangement , nearly every point of a target volume can be examined both for physical and biological matters after transferring imrt plans to the phanto software since no commercial software was able to read doses in such small intervals as required , a new software tool called grayhound was developed . 
 patient affection beams subsegments energy ( mv ) mean fraction time 7 sphenoid meningeoma nasopharyngeal carcinoma 7 carcinoma of the maxillary sinus 7 carcinoma of the breast 6 6 6 14 min 23 s 16 min 16 s 14 min 56 s 20 min 57 s figure 2 . 
furthermore , we defined points of high dose gradient as points where in at least one of the main axes ( x , y , z ) there is a dose difference of > 10% within 10 mm around the point according to the calculated dose of the phantom plan . 
 effective fraction time figure 7b shows that the time of gantry and collimator movement ( when the beam is switched off ) limits the effective fraction time ( eft ) to a certain percentage of total fraction time . 
 no significant difference could be seen between high dose points in low dose gradients and in high dose gradients ( as defined above ; figures 3b and 3c to 6b and 6c )  . 
 patient d showed the vastest differences ( figures 6a and 6b )  . high dose rates and corresponding time significant differences between high dose points in low - dose gradient areas and those in high - dose - gradient areas could not be stated for any patient . it is remarkable that nearly always > 70% of the fraction dose is delivered in < 10% of the fraction time . we therefore created a parameter called dhd / thd which is defined as the percentage of dose delivered during these high - dose - rate pulses divided by the percentage of fraction time in which they occur . 
for instance , the value of eft in simple plans with two orthogonal fields should be far > 50% whereas complicated ( non - imrt ) techniques may even almost equal the range of eft for imrt . the comparison with other kinds of imrt should be helpful as well , since our investigations only deal with the step - and - shoot approach . 
even within static imrt systems , different planning systems and linacs should generate different results . in dynamic imrt less dose rate inhomogeneities should be seen : eft should be higher and dhd / thd should be t [ s ] mogeneities of dose rate delivery . 
our results suggest that a 15 - mv plan as well as a higher number of segments will lead to higher values of dhd / thd ( see table 3 and figure 8 )  . 
dose in percent of fraction dose which is delivered in high dose pulses ( > 0.01 gy / s ; = dhd ) and the time needed to deliver that dose ( = thd ) in percent of fraction time . 
anteil der fraktionsdosis ( in % ) , der in hochdosispulsen ( > 0 , 01 gy / s ; = dhd ) appliziert wird , sowie die zeit , die bentigt wird , um diese dosis zu applizieren ( in % der fraktionszeit ; = thd )  . 
nevertheless , problems similar to the ones presented in this work should occur in all kinds of radiotherapy with protracted dose delivery . furthermore , our investigations show the influence of the number of beams and subsegments , respectively , and of the dose rate ( patient c )  . 
to quantify the amount of reduction , more investigations are needed in slightly different plans . thus , eft and dhd / thd might be practical to become parameters in the evaluation of radiotherapy regarding time efficiency and necessary radiobiological experiments provided biological significance . since our experiments were performed on one linac , it is necessary to emphasize that the parameters cannot be used to compare different plans on different linac without further research . patient c patient d figures 8a to 8d . 
according to our results the number of beams ( and subsegments ) should be as low as possible . the algorithms of the inverse planning program for creating the intensity maps as well as the algorithms for translation of the intensity maps into leaf sequences have already been an aim of enhancement . 
the parameters presented in this paper could be useful for this purpose [ 27 ]  . our results and the requirements of a high - quality imrt plan ( target conformity , sparing of organs at risk ) may not be easily connected . 
 with the given level of time ( in ) efficiency one could say the goal in designing ( step - and - shoot ) imrt plans should be as much intensity modulation as needed but at the same time as little intensity modulation as possible . 
 strahlentherapie und onkologie original article sites of failure in breast cancer patients with extracapsular invasion of axillary lymph node metastases no need for axillary irradiation ? ! gnther gruber1 , samuel menzi1 , andrea forster1 , gilles berclaz2 , hans - jrg altermatt3 , richard h . 
 patients and methods : after a retrospective review of pathology reports , the information about ecs was available in 254 lymph node - positive patients : ecs was absent in 34% ( ecs - negative ; n = 87 ) and present in 66% ( ecs - positive ; n = 167 )  . 
the 5 - year axillary relapse - free survival was 100% in ecs - negative and 90% in ecs - positive patients ( p = 0.01 ) , whereas corresponding values for periclavicular relapse - free survival ( with ecs : 91% 4% ; without ecs : 94% 3% ; p = 0.77 ) and local relapse - free survival ( with ecs : 86% 4% ; without ecs : 91% 3% ; p = 0.69 ) were not significantly different . 
2 - tests revealed a high correlation of ecs with t - stage , number of positive lymph nodes and progesterone receptor status , comparisons with estrogen receptor , grade , or age were not significant . 
 key words : extranodal pattern of failure axillary failure strahlenther onkol 2005 ; 181 : 5749 doi 10.1007 / s00066 - 005 - 1367 - x rckfallmuster beim nodal positiven mammakarzinom mit extrakapsulrer ausdehnung . 
 patienten und methodik : es wurden nur jene 254 nodal positiven patientinnen ausgewertet , bei denen gem histologischem bericht zum vorliegen oder fehlen von ecs klar stellung genommen wurde : in 66% ( ecs - positiv ; n = 167 ) wurde ecs beschrieben , und in 34% fehlte es ( ecs - negativ ; n = 87 )  . 
die korrespondierenden werte fr das periklavikulre rezidivfreie berleben ( mit ecs : 91% 4% ; ohne ecs : 94% 3% ; p = 0 , 77 ) und das lokalrezidivfreie berleben ( mit ecs : 86% 4% ; ohne ecs : 91% 3% ; p = 0 , 69 ) waren nicht signifikant unterschiedlich . 
ecs ( ja / nein ) korrelierte signifikant mit dem t - stadium , der anzahl positiver lymphknoten und dem progesteronrezeptorstatus , dagegen nicht mit dem strogenrezeptor , dem tumorgrad oder dem alter . 
multivariat war die anzahl positiver lymphknoten der einzige signifikante parameter fr das regionale 1 department of radiation oncology , inselspital , university of berne , switzerland , 2 department of gynecology , inselspital , university of berne , switzerland , 3 institute of pathology , berne , switzerland . 
nach der stratifikation der patientinnen in solche mit ein bis drei und solche mit vier oder mehr positiven lymphknoten lie sich keine signifikanz von ecs fr die axillre rezidivhufigkeit mehr finden . schlussfolgerung : in der univariaten analyse war das vorliegen von ecs mit einer erhhten axillren rezidivhufigkeit vergesellschaftet . 
 schlsselwrter : extranodal rezidivmuster axillres versagen multivariat introduction the presence of extracapsular spread ( ecs ) of axillary lymph node metastasis / metastases is often correlated with locoregional failure [ 11 ]  . 
it is unclear , if the risk of axillary recurrence justifies the enhanced risk of toxicity ( e.g. , lymphedema , impaired shoulder movement ) caused by irradiation to this site . 
 statistical methods cross tabulations between ecs - positive and ecs - negative patients in regard to clinicopathologic parameters were calpatients and methods as the information of ecs is not always prospectively recorded in the pathology report , only lymph node - positive patients with a clear definition of the presence or absence of ecs were eligible for this retrospective review . 
ecs was defined as any breech of the capsule of one or more metastatic lymph node / s . between 08 / 1988 and 12 / 2001 , 254 node - positive breast cancer patients with a median age of 56 years ( range : 2687 years ) could be identified , 167 ( 66% ) of them with ecs . 
all patients had segmental mastectomy with axillary node dissection ( level i , ii , iii ; n = 144 ) or modified radical mastectomy ( n = 110 )  . 
the median number of resected lymph nodes was 17 ( range : one to 68 ) , of which a median of three ( range : one to 49 ) were positive . 
no patient had evidence of distant metastasis after staging which included routine chest x - rays , blood tests , liver ultrasounds , bone scans , and , in several cases , computed tomographies of the thorax . 
the kaplan - meier method was used for the estimation of survival times , and the log - rank test for univariate analyses of various parameters as to local relapse - free survival ( lrfs ) , axillary relapse - free survival ( arfs ) , periclavicular relapse - free survival ( prfs ) , and distant metastasis - free survival ( dmfs )  . 
 regional failure ( = axillary + periclavicular failure ) was of special interest , and all factors were also evaluated in multivariate analysis for this endpoint using the cox regression proportional hazard model . 
axillres rezidivfreies berleben bei 254 nodal positiven patientinnen in abhngigkeit vom extrakapsulren wachstu sites of first failure ( table 2 ) after a mean follow - up of 46 months , 26 patients relapsed locally . 
 the next step to evaluate the role of ecs for axillary and periclavicular failure was to divide the patients into two subgroups according to the number of positive lymph nodes . 
 we could not detect a significant difference in patients with or without ecs in both subgroups ; however ; the p - value for axillary failure was 0.07 in patients with one to three positive nodes ( figure 4 )  . 
 this positive correlation was highly significant and goes in line with a previous examination [ 7 ] and other data in the literature [ 1 , 3 , 9 , 13 ]  . 
 first reports which found a correlation of ecs with decreased survival were published nearly 30 years ago [ 5 , 13 ] and have been confirmed by almost every study afterwards [ 1 , 3 , 10 , 12 , 14 , 18 , 20 ]  . 
 if we assume that all node - positive breast cancer patients should receive postoperative radiotherapy after breast - conserving surgery [ 15 , 26 ] and mastectomy [ 16 , 17 , 19 , 27 ] , the question remains about the necessity of regional irradiation , especially if ecs is present . 
the number of positive lymph nodes might be much more important than ecs in the consideration of axillary irradiation . interestingly , all but one regional relapses were accompanied by distant failure . 
axillres rezidivfreies berleben bei 131 patientinnen mit ein bis drei positiven lymphknoten in abhngigkeit vom extrakapsulren wachstu due to the retrospective design and a relatively small patient cohort firm conclusions cannot be made , but based gruber g , et al . 
pattern of relapse in breast cancer patients with extracapsular invasion on our findings and data from the literature we do not support axillary irradiation regardless if ecs is present or not . 
the inclusion of the axillary apex and subclavian area is appropriate for selected node - positive cases , particularly those with four or more positive nodes [ 8 ]  . 
 despite the frequency of ecs in node - positive breast cancer data about the prognostic role of ecs are rare , and the current evaluation represents one of the largest in the literature . 
their arguments for this new terminology may have some merit , however , it should be kept in mind that the terms planned or scheduled and unplanned or unscheduled gaps have been widely used in the scientific literature after their introduction in the report of a working party of the royal college of radiology in 1996 [ 1 , 2 , 5 ]  . 
 [ 6 ] share our opinion that the negative influence of treatment gaps on the outcome of radiotherapy , and the compensation of such a gap by modification of the remaining part of the treatment to adjust for the interruption , can , for ethical reasons , not be tested in a randomized clinical trial . 
this is correct , however , in situations where it not feasible to perform a randomized clinical trial , we have to rely on laboratory data , on nonrandomized clinical evidence , and on evidence coming from randomized clinical trials on the time factor of fractionated radiotherapy , all indicating that overall treatment time of radiotherapy , i.e. , the time between first and last fraction , has significant impact on local tumor control , most notably in squamous cell carcinoma . 
 [ 6 ] ask the important question whether also for patients who receive radiochemotherapy , treatment interruptions should be compensated and whether chemotherapy may be used to compensate treatment gaps instead of radiotherapy . 
these questions are less well investigated than the time factor of radiotherapy alone , however , a time factor has , e.g. , been demonstrated in the randomized trial by turrisi et al . 
 [ 6 ] recommend a comprehensive approach for compensation of treatment gaps which considers radiobiological and clinical data , but also other aspects such as distributive justice with an open debate about rationing . 
 strahlentherapie und onkologie original article effect of pentoxifylline and tocopherol on radiation proctitis / enteritis andrea hille1 , hans christiansen1 , olivier pradier1 , robert michael hermann1 , birgit siekmeyer1 , elisabeth weiss1 , reinhard hilgers2 , clemens f . 
hess1 , heinz schmidberger1 background and purpose : chronic radiation proctitis / enteritis is a relevant complication of pelvic irradiation , which is still mainly treated by supportive measures only . 
 patients and methods : of 30 patients with radiation - induced proctitis / enteritis grade iii according to the rtog / eortc toxicity criteria , 21 were treated with pentoxifylline and tocopherol . 
 key words : radiotherapy late toxicity enteritis proctitis pentoxifylline tocopherol strahlenther onkol 2005 ; 181 : 60614 doi 10.1007 / s00066 - 005 - 1390 - y effekt einer kombinationstherapie aus pentoxifyllin und tocopherol auf die strahleninduzierte proktitis / enteritis hintergrund und ziel : die strahleninduzierte chronische proktitis / enteritis ist eine relevante komplikation nach beckenbestrahlungen , die hauptschlich symptomatisch therapiert wird . 
in einer retrospektiven analyse wurde der klinische nutzen dieser kombinationstherapie bei strahleninduzierter proktitis / enteritis ausgewertet und mit alleiniger symptomatischer behandlung verglichen . patienten und methodik : von 30 patienten mit einer strahleninduzierten proktitis / enteritis grad iii nach den kriterien der rtog / eortc wurden 21 mit pentoxifyllin und tocopherol behandelt . 
in abhngigkeit von der rztlichen entscheidung wurden neun patienten nur symptomatisch behandelt ( tabelle 1 )  . ergebnisse : 15 / 21 patienten ( 71% ) unter therapie mit pentoxifyllin und tocopherol erlebten eine verbesserung ihrer symptome ( tabelle 3 , abbildung 1 )  . 
 schlsselwrter : radiotherapie spttoxizitt enteritis proktitis pentoxifyllin tocopherol 1 department of radiotherapy and radiation oncology , university of goettingen , germany , 2 department for medical statistics , university of goettingen , germany . 
radiation proctitis results in bleeding , pain , abdominal cramping , mucoid discharge , and fecal urgency ; the incidence has been estimated between 5% and 30% after radiotherapy for prostate cancer [ 29 ]  . 
radiation - induced chronic disease emerges with a latent period of 90 days to several years with the highest frequency within the first 3 years [ 7 ] and a median time to occurrence of 1416 months [ 17 , 38 ]  . 
several drugs have been used to reduce the inflammatory reaction associated with fibrosis : corticosteroids , nonsteroidal anti - inflammatory agents [ 37 , 42 ] , sucralfate [ 39 , 47 ] and short - chain fatty acids [ 40 ]  . 
 the pathogenesis of radiation enteritis / proctitis is characterized by inflammatory disease , endarteritis of arterioles , epithelial atrophy , vascular thrombi , ischemia , necrosis , and excessive fibrosis . 
several studies on the treatment of radiation - induced late injury to other tissues indicated that a treatment with pentoxifylline and tocopherol might be promising [ 46 , 28 ]  . 
pentoxifylline produces hemorheologic effects and , additionally , is an immunomodulator with activities on downregulation of several cytokines , that are known to be mediators of inflammatory and fibrogenic reactions after irradiation . 
radiation damage is mediated through reactive oxygen metabolites and , therefore , tocopherol , which has antioxidant properties [ 31 ] , may also be beneficial in the treatment of inflammatory and fibrotic processes . 
thus , we evaluated the therapeutic effect of pentoxifylline and tocopherol in patients with radiation - induced chronic proctitis / enteritis in a retrospective study , and compared the relief of symptoms in these patients with the relief of symptoms in a group of patients who did not receive this treatment . 
 patients and methods between june 1998 and december 2003 , 30 patients suffering from chronic radiation - induced proctitis and enteritis could be identified at the university hospital in goettingen , germany . 
six patients who were treated with pentoxifylline and tocopherol received additional symptomatic therapy with smectite ( n = 1 ) , laxatives ( n = 1 ) , short - chain fatty acids ( n = 3 ) , or misoprostol ( n = 1 )  . 
 each patient in our study suffered from chronic symptoms , with an interval from the date of their last radiation treatment , of 348 months ( median 12 months )  . 
most patient information was available from the medical file , part of the information either from mail or telephone with the referring physician or with patients . in 13 patients , chronic proctitis / enteritis occurred after curative external - beam irradiation for prostate cancer , in one patient for anal cancer . 
in 16 patients with chronic disease , irradiation had been given as postoperative treatment for prostate cancer ( n = 3 ) , cervical cancer ( n = 4 ) , vulvar cancer ( n = 1 ) , endometrial cancer ( n = 4 ) , and rectal cancer ( n = 4 )  . 
brachytherapy was given using a high - dose - rate ( hdr ) remote afterloading machine with an iridium - 192 source ( varian ) in a linear source arrangement . 
 patients with prostate cancer received stage - adapted irradiation to the pelvis to a total dose of 45 gy ( 1.8 gy per fraction ) and to the prostate region to a total dose of 6571 gy ( 2 gy per fraction ) , or to the prostate region to a total dose strahlenther onkol 2005 no . 
 optimized irradiation technique with the use of multiple radiation fields , individual blocks and the prone position with a belly board had been used , if possible , to reduce the small - bowel volume within the planning target volume . 
the patient with vulvar cancer received concomitant cisplatin and 5 - fluorouracil ( 5 - fu ) chemotherapy , and the patient with anal cancer was given simultaneous 5 - fu and mitomycin c chemotherapy . 
 drug duration of intake effect ( months ) 3 rectal said systemic nsaid and rectal application of short - chain 69 fatty acids rectal said systemic nsaid systemic nsaid systemic nsaid systemic nsaid , loperamide systemic nsaid loperamide loperamide systemic nsaid loperamide and rectal said 2 3 3 3 4 2 3 1 no change no change increase in symptoms no change no change no change no change partly decrease in symptoms partly decrease in symptoms no change no change no change statistical analysis the pearson 2 - test was performed to compare the efficacy of both treatments . 
 the difference between the toxicity in each treatment group at the onset of treatment and at the time the patient was evaluated and toxicity scored last , was calculated using the sign test . 
 of the seven patients with chronic radiation enteritis , three had undergone treatment for cervical cancer ( grade ii ) , one for endometrial cancer ( grade ii ) , and three for rectal cancer ( grade i )  . 
of the patients with chronic radiation - induced proctitis , five had been treated for prostate cancer ( grade i ) , and two for endometrial cancer ( grade i and ii )  . 
of the two patients with chronic radiation enteritis , one each had undergone treatment for anal cancer ( grade i ) and for endometrial cancer ( grade ii )  . 
 efficacy of pentoxifylline and tocopherol a reduction from grade i to grade 0 toxicity was observed in four , from grade ii to grade 0 toxicity in three , and from grade ii to grade i toxicity in eight patients . 
two of these nonresponders took the drugs for 23 weeks and one patient for 4 months only . one patient with radiation - induced enteritis after treatment for cervical cancer suffered from 1015 , another from 2030 daily bowel movements . 
a statistically significant lower frequency and severity of symptoms were seen at the time of the last control compared to the time at onset of treatment beginning with pentoxifylline and tocopherol ( pearsons ( cid : 1 ) 2 - test , p = 0.0003 ; figure 1 )  . 
 efficacy of pentoxifylline and tocopherol compared to symptomatic treatment only amelioration of symptoms was significantly better in patients treated with pentoxifylline and tocopherol compared to patients with symptomatic treatment only ( sign test , p = 0.014 ; figure 2 )  . 
 treatment toxicity treatment treatment toxicity drug and treatment treatment treatment grade after drug and time ( months ) grade after drug and treatment treatment time ( months ) treatment toxicity drug and grade after drug and treatment treatment treatment treatment toxicity grade after treatment time ( months ) time ( months ) patient toxicity grade at onset of treatment time ( time after ( months ) end of radiation treatment in months ) rectal application of said ( 13 ) rectal application of said and loper amide ( 3 ) no change loperamide and smectite ( no further follow - up ) i ( 48 ) ii ( 12 ) i ( 11 ) i ( 11 ) i ( 3 ) i ( 12 ) i ( 12 ) i ( 5 ) ii ( 13 ) rectal application of nsaid ( 9 ) and systemic application of nsaid ( no further follow - up ) systemic application of nsaid ( 4 ) no further follow - up loperamide ii ( 6 ) loperamide no change loperamide ( 54 ) rectal application of said ( 4 ) rectal application of said and systemic application of nsaid ( 4 ) no treat ment ( 3 ) rectal application application of nsaid ( 5 ) of said ( 1 ) systemic rectal and rectal application application of nsaid of nsaid ( 7 ) ( 18 ) no change rectal no treat application ment ( 13 ) of nsaid ( 13 ) rectal no change smectite and application of nsaid and toco pherol ( 11 ) no change no treat ment ( 4 ) no change systemic rectal application of said ( no further follow - up ) enteritis 1 proctitis 3 no further follow - up rectal application of short - chain fatty acids no change no further follow - up no further follow - up ii systemic and rectal application of nsaid ( 5 ) no treatment 0 ( 15 ) rectal application of shortchain fatty acids ( 5 ) strahlenther onkol 2005 no . 
9 urban & vogel p = 0.014 pentoxifylline and tocopherol treatment ( n = 21 ) pentoxifylline and tocopherol treatment ( n = 9 ) ( cid : 127 ) changed + not changed hille a , et al . 
pentoxifylline and tocopherol in radiation proctitis / enteritis p = 0.0003 symptoms at onset of treatment symptoms at the time of the last control grade 0 grade i grade ii worsening no change amelioration symptoms treatment effects figure 1 . 
 course of toxicity in patients without pentoxifylline and tocopherol treatment depending on the physicians decision , nine of 30 patients with chronic disease did not undergo a treatment with pentoxifylline and tocopherol . 
patients were treated with various course of toxicity after taking off pentoxifylline and tocopherol treatment ten of 21 patients stopped taking pentoxifylline for the following reasons : three patients refused taking both drugs because of nausea and an increase in weight , and four patients stopped taking pentoxifylline and tocopherol because of an amelioration of their symptoms . 
only one patient who had taken the drugs for 30 months with a complete relief of the symptoms experienced no deterioration 20 28 100 120 140 time ( weeks ) figure 3 . 
all of these drugs are only useful when administered early in the fibrotic process , but are ineffective in reversing the fibrotic process . pentoxifylline alone had a therapeutic effect in radiation - induced trismus [ 2 ] , and soft - tissue injury [ 14 ]  . 
however , a randomized study in cutaneous fibrosis found no significant effect of pentoxifylline or tocopherol as single treatment drugs [ 6 ]  . we decided to give pentoxifylline and tocopherol as a combination treatment , based on the observations of several investigators [ 46 , 11 , 28 ]  . 
 histopathology of radiation effect on intestine radiation enteritis and proctitis are characterized histologically by progressive vasculitis leading to thrombosis of small arteries and arterioles resulting in wall ischemia [ 8 ]  . 
the ischemia and vascular alterations including teleangiectatic vessels predispose to bleeding and mucosa ulceration and necrosis as well as obstruction , submucosal fibrosis , and fistula development [ 18 , 19 ]  . 
 molecular biology of radiation effects on intestine ionizing irradiation produces hydroxyl radicals that stimulate the production of transforming growth factor - ( tgf - ) ( cid : 2 ) 1 . 
overexpression of tgf - ( cid : 2 ) was found in experimental models of pneumonitis [ 12 ] , and cutaneous [ 34 ] , bladder [ 26 ] , kidney [ 45 ] and bowel fibrosis [ 20 ]  . 
several inflammatory cytokines , like tumor necrosis factor - ( tnf - ) have been shown to be mediators in intestinal inflammation and in inflammatory bowel diseases [ 1 , 35 ]  . 
 potential mediators in inflammatory bowel disease and radiation - induced fibrosis antagonists of tgf - ( cid : 2 ) and tnfmay play a role in the therapeutic intervention of radiation - induced inflammatory disease and fibrosis . 
in vitro studies and animal models showed an effect of pentoxifylline on tnflevels in inflamed intestinal mucosa cultures from patients with crohns disease and mouse colitis [ 30 ]  . 
modulation of cytokine transcription in humans with inflammatory bowel disease by tnfantibody treatment and pentoxifylline could be shown with clinical response in the treatment of crohns disease [ 41 ]  . 
 the phosphodiesterase inhibitor pentoxifylline and the antioxidant tocopherol the phosphodiesterase inhibitor pentoxifylline results in an increased elasticity of erythrocytes , vasodilatation , decreasing blood viscosity , and inhibition of inflammatory reactions . 
additionally , pentoxifylline is an immunomodulator with activities on downregulation of several cytokines , like tgf - ( cid : 2 ) and tnf - , that are known to be mediators of inflammatory and fibrogenic reactions after irradiation . 
radiation damage , as mentioned above , is mediated through reactive oxygen metabolites and , therefore , tocopherol may also be beneficial in the treatment of inflammatory and fibrotic processes . 
the combination of pentoxifylline and tocopherol has synergistic effects on cell regeneration and extracellular matrix and could induce significant reduction of subcutaneous radiation - induced fibrosis in pigs [ 27 ]  . 
several randomized and nonrandomized trials in humans have shown the efficacy of pentoxifylline and tocopherol on radiation - induced late injury as well , e.g. , cutaneous fibrosis [ 4 , 6 , 10 , 11 , 16 ] , osteoradionecrosis [ 5 ] , and fibroatrophic lesions of the uterus [ 28 ]  . 
 the hemorheologic effect of pentoxifylline , the potential to inhibit tgf - ( cid : 2 ) and tnf - , and the additional antioxidant effect of tocopherol may lead to an effective synergistic action on radiation - induced damage of intestine and colorectal mucosa . 
further studies are needed to understand the cellular mechanism underlying radiation fibrosis and to open the opportunity of selective etiology - based intervention to improve chronic radiation - induced disease . 
pentoxifylline and tocopherol in radiation proctitis / enteritis efficacy of pentoxifylline and tocopherol compared to symptomatic treatment only our retrospective analysis of 30 patients with radiation - induced chronic proctitis and enteritis grade iii showed a difference between patients treated and those only observed . 
different retrospective studies with rectal bleeding not requiring blood transfusions showed spontaneous cessation of bleeding within 2 years in many patients , whereas no patient suffering from rectal bleeding requiring blood transfusions had a spontaneous remission [ 15 ]  . 
in our own study , no patient with continued pentoxifylline and tocopherol treatment experienced a deterioration of symptoms compared to three of nine patients with symptomatic treatment and six of ten patients who stopped taking pentoxifylline . 
six of 21 patients with pentoxifylline and tocopherol treatment suffered from symptoms without a relief compared to five of nine patients with symptomatic treatment and six of ten patients who stopped taking pentoxifylline . 
 importance of treatment time with pentoxifylline and tocopherol in a randomized study , which showed a reduction of radiation - induced subcutaneous fibrosis , better results were obtained with a treatment period of 6 months , compared to 3 months [ 6 ]  . 
we are aware that our study is a retrospective analysis with few patients , but nevertheless , it indicates , that the combination of pentoxifylline and tocopherol might alleviate the symptoms of chronic radiation enteritis and proctitis . 
holidays are forseeable gaps , which must be discussed initially with the patient , especially how and whether to compensate for theunforseeable gaps such as acute side effects and machine breakdown must be discussed at the moment they occur . 
 strahlenther onkol 2005 ; 181 : 6156 doi 10.1007 / s00066 - 005 - 9331 - 3 after reviewing the clinical and radiobiological literature , the authors set out their premises . 
in the following , two central premises ( a shorter treatment time is advantageous , shortening of treatment time results in better local control for head and neck tumors and bronchial cancers ) and one conclusion ( palliative radiotherapy needs no compensation of unplanned gaps ) are presented . 
another very important question would be , whether patients receiving radiochemotherapy need compensation to the same extent as those who have radiotherapy alone , and whether chemotherapy can be used to compensate treatment gaps instead of radiotherapy [ 13 , 8 ]  . 
dearnaley3 , klaus - rdiger trott4 purpose : to investigate the dose distribution in active bone marrow of patients undergoing intensity - modulated radiotherapy ( imrt ) for prostate cancer and compare it to the distribution in the same patients , if they had been treated using conformal plans , in order to develop criteria for optimization to minimize the estimated risk of secondary leukemia . 
 the mean bone marrow dose is therefore not a useful criterion to judge plan quality , since scattered low doses to distant sites may be more critical than the high dose volumes receiving > 10 gy . 
 key words : prostate cancer dose - volume histogram bone marrow doses strahlenther onkol 2005 ; 181 : 1728 doi 10.1007 / s00066 - 005 - 1360 - 4 die strahlenbelastung des knochenmarks bei der intensittsmodulierten strahlentherapie des prostatakarzinoms ziel : die dosisverteilung im roten knochenmark von patienten , die wegen eines prostatakarzinoms mit einer intensittsmodulierten strahlentherapie ( imrt ) behandelt werden , sollte mit derjenigen verglichen werden , die sie bei einer dreidimensionalen ( 3 - d ) konformalen strahlentherapie erhalten wrden , um optimierungskriterien fr die beurteilung von bestrahlungsplnen zu entwickeln und so das mgliche risiko einer strahlentherapieinduzierten leukmie zu minimieren . patienten und methodik : bei zehn patienten , die eine imrt des ganzen beckens erhielten , wurde die dosisverteilung im roten knochenmark berechnet und mit der dosisverteilung verglichen , die sie bei einer 3 - d - konformalen strahlentherapie des gleichen zielvolumens erhalten htten . 
die dosis auerhalb des beckens wurde fr alle bestrahlungsplne im sternum eines rando - phantoms mit thermolumineszenzdioden - ( tld - ) dosimetern gemessen . ergebnisse : sowohl bei bestrahlung des ganzen beckens als auch der prostata allein ergab die imrt - technik eine verkleinerung des hochdosisvolumens im rektum , in der blase und im dnndarm bei akzeptabler dosisverteilung im planungszielvolumen ( ptv )  . 
 die imrt - technik reduzierte bei bestrahlung des beckens das mit hoher dosis belastete knochenmarkvolumen , vergrerte aber das mit mittlerer dosis von 1020 gy belastete volumen , whrend kein unterschied im mit < 5 gy belasteten volumen gemessen wurde . 
die leckagedosis war bei der imrt - technik um den faktor 2 erhht . 1 department of radiotherapy , cancer center , north - estonian regional hospital , tallinn , estonia , 2 joint department of physics , the royal marsden nhs trust , london , uk , 3 academic department of clinical oncology , institute of cancer research and the royal marsden nhs trust , sutton , surrey , uk , 4 st . 
bartholomews and the royal school of medicine and dentistry , queen mary college , university of london , and gray cancer institute , northwood , uk . received : august 25 , 2004 ; accepted : january 14 , 2005 strahlenther onkol 2005 no . 
bone marrow doses in prostate cancer schlussfolgerung : die dosis - volumen - histogramme im roten knochenmark unterscheiden sich signifikant bei der imrt im vergleich zur 3 - d - konformalen strahlentherapie des prostatakarzinoms . 
die zahl der monitoreinheiten hat einen groen einfluss auf die leckagedosis bei der imrt ; es wre zu berlegen , ob dieser parameter in die optimierungskriterien der imrt einbezogen werden sollte . schlsselwrter : prostatakarzinom dosis - volumen - histogramm knochenmarkdosis introduction cancer of the prostate is the second most common malignancy in males . 
it has been estimated [ 14 ] that the intensity - modulated radiotherapy ( imrt ) could almost double the incidence of second malignancies compared with conventional radiotherapy . both large - scale epidemiologic studies on long - term survivors of curative radiotherapy of cervix cancer and of prostate cancer demonstrated an increased risk of developing second cancers [ 1 , 2 , 19 ]  . 
the results of the seer study demonstrated a two - fold increase in the risk of leukemia in the irradiated group of patients within 10 years after treatment which was significant [ 11 ]  . 
the increased risk of secondary early bladder cancer and of rectal cancer is probably related to severe chronic tissue injury caused by the high radiation doses in the bladder and rectum which are well - established precancerous lesions . 
this interpretation is supported by the fact that radiation - induced rectal cancer has only been found in those studies where organ doses were very high causing a high frequency of chronic inflammation , severe atrophy and necrosis ( 60 gy ) [ 26 ]  . 
improved conformality of treatment will reduce the severity of chronic rectal damage which we expect to reduce also the risk of consequential secondary cancer in the rectum and the bladder . 
 five patients were scanned from 1 cm below the ischial tuberosities to the level of l5s1 and five to the level of l3 with 5 mm slice thickness and separation . 
the ct slices were transferred to cadplan 6.3.5 ( varian medical systems ) treatment planning system . the clinical target volumes ( ctvs ) , bladder , rectum , bowel and femora were outlined on each ct image . 
ctv2 included the seminal vesicles and the following lymph node groups : internal and external iliac nodes , presciatic and presacral ( anterior to the first , second and third sacral segments ) , and the obturator - hypogastric complex [ 20 ]  . 
it has been shown [ 20 ] that for prostate and pelvic node irradiation reducing the number of beams from nine to five had no adverse effect on the ptv coverage obtainable . 
gantry angles of 180 ( posterior ) , 270 ( right lateral ) , 325 ( right anterior oblique ) , 35 ( left anterior oblique ) , and 100 ( left posterior oblique ) have been chosen after evaluation of five different patients treatment plans . 
the pelvic bones and the pelvic bone marrow were not intentionally avoided in the planning process , although the selection of the beam angles could have an impact on dose distribution within the pelvic bone marrow . 
treatment plans were created for 6 - mv photons from a varian 2100 c / d ( palo alto , ca , usa ) linear accelerator for delivery with a dynamic 120 - leaf mlc technique . 
the treatment is designed to give 35 fractions and to deliver 70 gy to ptv1 and 50 gy to ptv2 ( this corresponds to 44 gy delivered in 2 - gy fractions and using / = 3 )  . 
afterwards , the priorities were increased on the rectum , the bladder and the bowel and the dose - volume points were moved to lower - dose constraints to maximize tissue sparing whilst ensuring that ptv coverage was not lost . 
due to limitations arising from our inability to differentiate between two types of bone marrow on ct , the whole non - bony space inside the pelvic bones was outlined on every ct slice . 
the pelvic bone marrow was divided into seven parts ( left femur head and neck , right femur head and neck , os coxae left side , os coxae right side , symphysis pubis , sacrum , and lumbar vertebrae )  . 
three tld 100 ( lif ) chips manufactured by harshaw were placed in the middle of the sternum region inside the rando phantothe sternum was chosen because it lies in the middle of the extrapelvic bone marrow sites ( skull , ribs , cervical and thoracic vertebrae , sternum , etc . ) and the dose delivered is predominantly from the leakage radiation which gives roughly the same dose to all critical organs . 
the volumes of the os coxae irradiated to 5 gy , 10 gy , 15 gy , 20 gy and to > 20 gy were recorded for each technique , and compared using a two - tailed paired students t - test . 
mean bone marrow doses and mean volumes of the os coxae irradiated to 5 gy , 10 gy , 15 gy , 20 gy and to > 20 gy for both treatments are shown in strahlenther onkol 2005 no . 
however , for both treatments the number of monitor units needed to deliver each imrt plan was increased by a factor of 3 ( table 2 ) and the dose to extrapelvic sites was increased by a factor of 2 . 
 long - term studies on large numbers of patients are unlikely to produce definitive answers , since radiotherapy modalities and dose distributions associated with them vary widely and evolve continuously further . 
the significant differences of the findings of the seer study in the usa [ 2 ] and the canadian study reported by pickles & phillips [ 21 ] were interpreted by the authors as being related to differences in the treatment techniques in the different periods covered by the studies . 
the bone marrow was chosen because dvhs vary most widely and leukemia is more closely related to radiation exposure than the other organs reported as showing an increased incidence after radiotherapy of prostate cancer . 
in imrt of other cancers , even greater problems may arise from the low doses imparted on other radiosensitive organs , in particular lung and stomach , which need to be studied in more strahlenther onkol 2005 no . 
moreover , genetic factors may also interact with radiotherapy in other cancer types , although these seem to be of minor importance in prostate cancer . in most epidemiologic studies , leukemia has been found to be the first radiation - induced malignancy to be observed . 
a significant increase in the incidence of leukemia within the first 10 years after exposure has been found in the japanese atom bomb survivors [ 22 ] and after radiotherapy of benign diseases such as ankylosing spondylitis [ 5 ] or uterine bleeding [ 17 ]  . in hiroshima and nagasaki , a total of 261 leukemia cases were observed among 93 , 696 members of the life span study ( lss )  . 
 in the first 10 years after irradiation there were 26 excess leukemia cases , which could be attributed to the effect of radiation , which would be a risk of approximately 0.2%. 
in irradiated prostate cancer patients from the seer study [ 19 ] , during the first 8 years after treatment 25 leukemias were observed , which was significantly higher than the 13 cases seen in patients treated surgically . 
 the risk values derived from lss data are higher than those from the radiotherapy data which demonstrates that as the distribution of radiation doses in the bone marrow becomes less homogeneous , the risk of radiation - induced leukemia decreases . 
 mean bone marrow dose might be a useful criterion to optimize the treatment plan in reducing the risk of leukopenia particularly in those patients who are scheduled to receive concomitant chemotherapy . 
however , the mean bone marrow dose may not be adequate for optimizing the distribution of radiation doses in the red bone marrow , if the aim is to reduce the risk of secondary leukemia . 
the bone marrow is a dynamic tissue with stem cells migrating between different bone marrow sites during the course of radiotherapy ; it is likely that individual stem cells may only be in the irradiated volume for one or a few dose fractions and will survive . 
moreover , bone marrow stem cells are also abundant in the peripheral blood and their concentration increases during a course of radiotherapy as radiation damage to bone marrow sites within the irradiated volume increases . 
on the other hand , it is unlikely that bone marrow stem cells resident in the high dose volumes for more than a few dose fractions survive and are thus unlikely to become the origin of a leukemic transformation . 
the risk of leukemia decreases with increasing dose inhomogeneity with comparable mean bone marrow doses by a factor of > 10 , and this suggests that bone marrow sites which receive doses < 5 gy may be more critical than those which contribute most to the mean bone marrow dose such as the os coxae and sacruthis was also concluded from a study on the kinetics of induction of dicentric chromosome aberrations in the lymphocytes of patients during radiotherapy for prostate cancer [ 10 ]  . 
 a greater number of monitor units required to deliver the prescribed dose increases the radiation dose to extrapelvic bone marrow sites by the leakage and scattering of x - rays through the collimation and treatment head assemblies of the linear accelerator . 
we therefore believe that the number of monitor units needed to deliver a plan should be incorporated into the evaluation of plan quality and some attempt be made to introduce it into the optimization algorithm , if the aim is to limit the risk of secondary leukemia . 
mean bone marrow doses for common radiotherapy schedules are several grays and similar to or higher than those from the treatment of ankylosing spondylitis , one of the main sources of information on radiationinduced leukemia . 
these can be reduced by limiting the variability of the fluence profile and by imposing delivery constraints during the interpretation phase ; delivery technique segmental or dynamic multileaf collimation and machine parameters may also impact . 
 strahlentherapie und onkologie original article efficacy and toxicity of postoperative temozolomide radiochemotherapy in malignant glioma martin kocher , sabine kunze , hans - theodor eich , robert semrau , rolf - peter mller1 purpose : to evaluate the feasibility , safety and efficacy of daily temozolomide concurrent with postoperative radiotherapy in malignant glioma . 
 patients and methods : from 11 / 1999 to 03 / 2003 , n = 81 patients aged 1572 years ( median 52 years , karnofsky score 80100% in 83% ) suffering from primary glioblastoma ( n = 47 ) , anaplastic astrocytoma ( n = 6 ) , anaplastic oligodendroglioma ( n = 16 ) , and recurrent glioma ( n = 12 ) were treated . 
effort should be taken to minimize corticosteroid doses , since both steroids and temozolomide lead to immunosuppression . key words : malignant glioma oligodendroglioma radiochemotherapy temozolomide strahlenther onkol 2005 ; 181 : 15763 doi 10.1007 / s00066 - 005 - 1314 - x postoperative radiochemotherapie mit temozolomid beim malignen gliom ziel : bestimmung der durchfhrbarkeit , toxizitt und effektivitt einer kombinierten postoperativen radiochemotherapie mit tglicher oraler applikation von temozolomid beim malignen gliom . patienten und methodik : von 11 / 1999 bis 03 / 2003 wurden n = 81 patienten ( alter 1572 jahre , median 52 jahre , karnofsky - index 80100% in 83% ) mit primrem glioblastom ( n = 47 ) , anaplastischem astrozytom ( n = 6 ) , anaplastischem oligodendrogliom ( n = 16 ) oder rezidivgliom ( n = 12 ) behandelt . 
patienten mit primren gliomen erhielten simultan zur postoperativen bestrahlung mit 60 gy ( 1 , 8bis 2 , 0 - gy - fraktionen ) an allen bestrahlungstagen temozolomid oral in einer dosierung von 75 mg / m2 ( 3033 dosen ) , rezidive wurden mit 4560 gy und temozolomid behandelt . 
die mediane berlebenszeit betrug fr glioblastome 15 monate , die 4 - jahres - berlebensrate fr oligodendrogliome 78% . schlussfolgerung : fr patienten mit malignen gliomen ist die simultane postoperative radiochemotherapie mit temozolomid ein sicheres und wenig belastendes verfahren . 
bei den chemosensiblen oligodendroglialen tumoren ist die radiochemotherapie effektiv ; bei den glioblastomen scheint eine prognoseverbesserung mglich . schlsselwrter : maligne gliome oligodendrogliom radiochemotherapie temozolomid 1 department of radiation oncology , university of cologne , germany . received : may 5 , 2004 ; accepted : january 14 , 2005 strahlenther onkol 2005 no . 
temozolomide in malignant glioma introduction despite long - lasting efforts to optimize the treatment for malignant glioma , the prognosis after standard therapy , comprising macroscopic resection and postoperative local radiotherapy , remains poor because almost all patients will die from local recurrences [ 2 , 26 ]  . 
nitrosoureas , cytarabine ( ara - c ) [ 1 , 8 , 15 , 25 ] , platinum plus etoposide or teniposide [ 4 , 24 , 29 ] have been used for intravenous or intraarterial [ 10 , 14 , 25 , 32 ] infusion during the period of irradiation , but so far , none of these regimens has led to a significant increase in survival . a new step was possible by the introduction of temozolomide which was shown to penetrate the blood - brain barrier to a significant amount and to sensitize glioma cells against irradiation [ 43 ]  . 
this led to the development of a therapeutic scheme where temozolomide was used in a manner that aimed at maximal radiosensitization by daily chemotherapy application during fractionated radiotherapy [ 38 ]  . 
patients with a karnofsky performance score 50% and no contraindications against the use of temozolomide ( no severe liver or renal dysfunction , normal blood cell counts , no known hypersensitivity against temozolomide or darcarbazine , no local or systemic infection , no pregnancy ) were offered temozolomide and irradiation as an individual treatment . 
they comprised 39% ( 47 / 121 ) of all glioblastoma , 45% ( 22 / 45 ) of all anaplastic glioma and 67% ( 12 / 18 ) of all recurrent glioma patients referred for local irradiation to the radiotherapy department . 
planning target volumes included the contrast - enhancing regions in the postoperative ct and / or the resection cavity with a margin of 1.52.5 ctemozolomide was applied as a single daily oral dose of 75 mg / m2 12 h before each radiotherapy fraction ( median 30 doses )  . 
the same schedule ( radiation doses of 4560 gy ) was used in twelve patients with recurrent or progressive malignant glioma after previous resection ( 12 / 12 ) and postoperative irradiation ( 10 / 12 )  . 
 supportive therapy most of the patients received ambulatory treatment only ( 39% ) while some were hospitalized for a short ( 12 weeks , 42% ) or a longer ( 37 weeks , 19% ) period for general supportive care . 
in total , 25% of the patients did not need any steroids at all , while 43% had low - dose ( 210 mg / d ) or high - dose ( 1232 mg / d ) dexamethasone for some time during their therapy . 
blood cell counts and serum chemistry were performed weekly in hospitalized patients and also in the majority of ambulatory patients ( see table 2 )  . statistical analysis patients were followed up by clinical examination and ct / mri scans every 36 months after therapy until deterioration . 
a database was set up that registered date and type of resection , details of radiotherapy and temozolomide application , hemotologic and nonhematologic toxicity , time to progression , adjuvant chemotherapy , procedures for treatment of recurrences , and overall survival time . 
progression - free survival was calculated from the time difference between date of surgery and date of progression , or date of death in cases where patients died without progression or where the date of progression was not known . 
toxicity was the dominant reason in six patients who experienced the following events : nausea for 1 day leading to refusal of therapy ( n = 1 ) , myelosuppression causing grade 2 / grade 4 thrombopenia / leukopenia ( n = 2 ) , encephalitis caused by herpes simplex virus ( n = 2 ) , skin infection by herpes zoster ( n = 1 )  . 
reasons probably unrelated to therapy ( five patients ) were : pneumonia by aspergillus following an epileptic seizure ( n = 1 ) , sudden cardiac death due to unknown cause ( n = 1 ) , asthenia ( n = 1 ) , intracerebral hemorrhage at site of stereotactic biopsy ( n = 1 ) , tooth extraction ( n = 1 )  . 
while leukopenia and thrombopenia were rare events ( 1% grade 34 ) , severe lymphopenia was observed in almost half of the patients ( grade 3 : 38% , grade 4 : 8% )  . 
serum enzymes expressing the secretory function ( ggt ) and integrity ( gpt ) of the liver cells showed abnormalities in a minority of patients ( grade 34 : 36% ) , but some of these events might have been caused by the simultaneous use of anticonvulsive drugs . 
in the first patient , only one dose of temozolomide of 75 mg / m2 had been applied 1 day before the patient became symptomatic , which almost excludes a causal relationship between the applied chemotherapy and the infection . 
temozolomide in malignant glioma adjuvant and salvage therapy progression - free and overall survival as shown in table 5 , adjuvant chemotherapy was used infrequently ( 12 / 81 patients , 15% )  . 
aa : anaplastisches astrozytom ; gbm : glioblastom ; od : anaplastisches oligodendro - / oligoastrozyto gbm ( n = 47 ) ( n = 6 ) ( n = 16 ) ( n = 12 ) recurrent glioma adjuvant chemotherapy temozolomide pcv other total chemotherapy for recurrence temozolomide pcv other total surgery / irradiation for recurrence resection 1 brachytherapy 1 surgery + brachytherapy reirradiation + brachytherapy 1 total 6 0 1 7 ( 15% ) 1 ( 17% ) 3 ( 19% ) 1 ( 8% ) 9 1 2 12 ( 26% ) 3 ( 50% ) 2 ( 13% ) 6 ( 50% ) 15 ( 32% ) 1 ( 17% ) 3 ( 19% ) 4 ( 33% ) progression - free survival was highest in the oligodendroglial tumors ( figure 1a ) with a median progression - free survival time of 34 months . 
 discussion besides altered fractionation radiotherapy schemes , adjuvant and simultaneous chemotherapy has been one of the most extensively followed directions in order to increase local control and survival in malignant glioma patients . 
 in glioblastoma patients , a meta - analysis found a total increase in the 2 - year survival rate of 4% [ 37 ] for any kind of adjuvant chemotherapy . 
oligo g3 : anaplastic oligodendroglial tumors ( n = 16 ) , astro g3 : anaplastic astrocytomas ( n = 6 ) , gbm : glioblastoma multiforme ( n = 47 )  . 
oligo g3 : anaplastische oligodendrogliale tumoren ( n = 16 ) , astro g3 : anaplastische astrozytome ( n = 6 ) , gbm : glioblastoma multiforme ( n = 47 )  . 
 the neuro - oncology working group of the german cancer society carried out a study ( noa 01 ) where malignant glioma patients with a karnofsky performance score 70% were treated with postoperative radiotherapy and adjuvant acnu / vm26 or acnu / ara - c . 
although these patients were selected according to one of the major prognostic factors , these results were superior to those from the rtog trials when patients were grouped into rpa classes [ 44 ] ( table 6 )  . 
in the present investigation , however , comparable survival times ( 15 months ) were achieved by simultaneous radiochemotherapy alone , which suggests that adjuvant chemotherapy is of minor importance in this disease . 
in addition , comparison of survival in the rpa classes seems to demonstrate that short - term concomitant radiochemotherapy with temozolomide is at least as effective as long - term adjuvant chemotherapy as applied in the noa 01 trial [ 44 ]  . 
at present , it is difficult to estimate the efficacy of simultaneous radiochemotherapy in anaplastic astrocytoma , since most reports do not separate these tumors from glioblastoma when reporting survival . 
the present data concerning combined radiochemotherapy using temozolomide does not add much information to this question , since only six patients were treated . for patients with anaplastic oligodendroglioma or mixed anaplastic astrocytoma / oligodendroglioma , the role of chemotherapy is far better defined . 
the standard therapy , comprising resection , postoperative radiotherapy and adjuvant pcv , leads to 3 - year survival times of 7085% [ 23 , 27 , 40 ]  . 
so far , temozolomide was mainly used as first - line [ 7 , 22 , 42 ] and second - line [ 41 ] salvage chemotherapy in recurrent oligodendroglial tumors . 
the results achieved in the present investigation for primary and recurrent oligodendroglial tumors compare well with these figures and suggest that radiotherapy combined with short - term simultaneous temozolomide is at least as effective as radiotherapy plus long - term adjuvant pcv in the primary setting . the relative effectiveness of sequential radiotherapy temozolomide compared to the sequential temozolomide radiotherapy is now being tested in a randomized trial of the neuro - oncology working group of the german cancer society [ 3 ]  . 
although it is , at present , uncertain whether results can be improved by simultaneous radiochemotherapy , the latter should be offered to patients with an oligodendroglial tumor outside clinical trials . 
it has , however , to be considered that these tumors present a heterogeneous group within itself , since cytogenetic analyses have shown a strong dependence of prognosis on specific chromosomal aberrations . 
patients with a combined 1p / 19q loss have a 10 - year survival rate of 80% , while all others have median survival times between 1.5 and 5 years [ 21 ]  . the protracted , daily application of temozolomide with doses of 75 mg / m2 was found to be safe in a dose - finding phase i study in 1998 [ 5 ]  . 
the most unexpected toxicity was the occurrence of herpes simplex encephalitis which , however , at least in one patient was not caused by temozolomide , since that patient had only received one dose of 75 mg / m2 the day before . 
therefore , care should be taken to reduce corticosteroids as much as possible during daily chemotherapy with temozolomide . combined and adjuvant radiochemotherapy with temozolomide has now been tested in a randomized , multicenter , multinational trial for glioblastoma by the eortc and was found to increase 2 - year survival from 10% to 26% [ 39 ]  . 
although glioblastoma is the most frequent type of malignant gliomas in adults , it would probably be more interesting to set up a randomized trial comparing postoperative radiotherapy to radiochemotherapy in oligodendroglial tumors and perhaps in anaplastic astrocytoma . 
in addition , the role of adjuvant temozolomide in glioblastoma still remains unclear . strahlentherapie und onkologie original article selective radioprotection of normal tissues by bowman - birk proteinase inhibitor ( bbi ) in mice klaus dittmann1 , mahmoud toulany1 , johannes classen2 , vanessa heinrich2 , luka milas3 , h . 
the purpose of the present study was to explore the in vivo normal - tissue radioprotective potential of bowman - birk proteinase inhibitor ( bbi ) , which acts as a normal - cell - specific radioprotector in vitro . 
treatment of mice with 100 mg / kg bbi before irradiation reduced leg contracture by > 4 mm , by about 50% ( p < 0.05 , t - test )  . 
by contrast , bbi did not induce radioprotection of either tp53 - mutated fsa or tp53 - normal fsaii tumor xenografts in mice , which argues for normal - tissue - specific effect . 
 conclusion : bbi acts as a potent selective normal - tissue radioprotector in vitro and in vivo , apparently without protecting tumors , and thus has the potential to improve clinical radiotherapy . 
 key words : normal - tissue radioprotector leg contracture tumor growth delay tp53 strahlenther onkol 2005 ; 181 : 1916 doi 10.1007 / s00066 - 005 - 1358 - y selektive radioprotektion von normalgeweben durch den bowman - birk - proteinase - inhibitor bei musen hintergrund und ziel : der erfolg einer radioonkologischen therapie wird hufig durch die reaktion des normalgewebes im bestrahlungsfeld limitiert . 
 ergebnisse : die strahleninduzierte beinverkrzung bei musen erreichte 150 tage nach der bestrahlung ein maximum von 8 m eine behandlung der muse mit einer bbi - dosis von 100 mg / kg vor der bestrahlung reduzierte die beinverkrzung um > 4 mm ( 50% ; p < 0 , 05 , t - test )  . 
dieser befund spricht fr eine normalgewebespezifitt . schlussfolgerung : bbi wirkt in vitro und in vivo als potenter normalgewebespezifischer radioprotektor , offensichtlich ohne tumoren zu schtzen , und hat so das potential , den erfolg der radiotherapie weiter zu verbessern . schlsselwrter : normalgewebespezifischer radioprotektor beinverkrzungsassay tumorwachstumsverzgerungsassay tp53 1 division of radiobiology and environmental research , department of radiation oncology , university of tuebingen , germany , 2 department of radiation oncology , university of tuebingen , germany , 3 department of experimental radiation oncology , the university of texas , m.d. 
although the use of precise radiation field sizes and accurate dose planning minimize the unwanted side effects of radiotherapy [ 11 ] , the side effects still occur in a percentage of patients and may be so severe as to compromise optimal radiation dose delivery or to significantly reduce the quality of life of treated patients . 
the pathogenesis of radiation - induced normal - tissue injury involves many mechanisms ranging from early molecular signaling in cells exposed to radiation to tissue remodeling ; however , the unrepaired radiation - induced dna damage in affected cells constitutes the primary molecular basis for this injury . 
normal cells possess various signaling pathways ( cascades ) to ensure cell elimination when their genomic integrity is lost , but which pathway or mechanism is activated depends on a number of factors including cell type . 
for example , complex dna damage , as that caused by ionizing radiation , induces cellular differentiation in fibroblasts [ 26 ] and apoptotic cell death in endothelial cells [ 19 ]  . 
there are two principal biological ways to protect normal tissue from radiation injury , one to reduce or eliminate radiation - induced free radicals responsible for dna damage , and the other to stimulate existing cellular repair mechanisms . 
 the free - radical elimination approach is largely exemplified by amifostine ( ethyol ) , recently approved for clinical use as a radioprotector in radiotherapy of head and neck cancer . 
despite many reports indicating a radioprotective effect for various normal tissues [ 3 , 4 , 15 , 20 , 30 , 31 ] the selectivity of amifostine for normal tissues remains controversial , and a possibility of tumor radioprotection has hindered widespread clinical use of this drug [ 22 ]  . 
we showed that the bowman - birk protease inhibitor ( bbi ) stimulates dna repair after irradiation of fibroblasts [ 10 ] , and have begun studies to elucidate molecular mechanisms involved in this radioprotection . 
to perform clinical trials , a crude extract from soybeans was developed ( bbi concentrate [ bbic ] ) [ 18 ] and in 1992 approved by the fda for investigational new drug status . 
it was well tolerated by the patients , and no clinical or laboratory evidence of toxicity or drug allergy was observed other than infrequent reporting of nausea , diarrhea , or epigastric discomfort , which do not seem related to drug ingestion [ 1 ]  . 
 our in vitro studies on radiation - induced fibroblast differentiation , a cellular process leading to radiation - induced fibrosis [ 12 , 25 ] , showed that pretreatment of fibroblasts with bbi prevented the radiation - induced differentiation and increased clonogenic survival up to 30% [ 7 ]  . 
 the bbi treatment significantly reduced radiation - induced dicentric chromosomes [ 8 ] , implying that bbi improved the fidelity of the nhej process . on the basis of these in vitro data we started to test the radioprotective potential of bbi in vivo . 
 material and methods reduction in leg contracture experiments were performed using female c3h / hencrl mice ( charles river , sultzfeld , germany ) with a mean weight of 25 g . 
 at day 0 the right legs of mice were irradiated with a single dose of 55 gy using a linac ( mevatron60 / siemens , erlangen , germany ) and a dose rate of 2 gy / mradiation - induced leg contracture was measured at 20to 30 - day intervals , starting at strahlenther onkol 2005 no . 
 results effects of bbi upon the radiation - induced normal - tissue response in c3h / hencrl mice , a single dose of 55 gy induced a distinct leg contracture after irradiation ( figure 1 )  . 
 effect of bbi upon the radiation - induced growth delay of fibrosarcoma xenografts in mice the sarcoma fsa is a rapidly growing tumor that , when untreated , reaches a diameter of about 15 mm within 5 days from the time when its diameter was 8 mm ( figure 3 )  . 
however , this effect was only significant for the time points 4 and 6 days after irradiation , but not at the last measured endpoint at day 8 ( figure 4 )  . 
 discussion radiation - induced fibrosis is a major component of many late sequelae in radiotherapy and may become dose - limiting in many organs and tissues such as the lung , kidney , heart , and vascular system [ 13 ]  . 
to test whether bbi which we identified as normal - cell - specific radioprotector in vitro [ 7 ] acts as an inhibitor of radiation - induced fibrosis in vivo , we chose the radiation - induced leg contracture assay as a model syste this assay was originally developed by stone [ 28 ] and is based on the radiation - induced fibrotic reorganization of connective tissue of the leg . 
with respect to the life expectancy of c3h mice , this fibrotic process is clearly a late sequela of radiation and comparable to fibrosis in humans developing years after radiation treatment . 
the first phase is characterized by a radiation - induced acute inflammatory response which is followed by a second phase of chronic inflammation resulting in the molecular changes [ 25 ] , possibly responsible for the fibrotic tissue reorganization . 
as shown earlier , bbi improved dna repair of initial damage [ 8 ] , which increased genomic integrity and was associated with prevention of radiation - induced terminal differentiation of fibroblasts . 
tp53 [ 9 ] , we performed this growth delay assay with sarcoma fsa , presenting mutated tp53 , and the sarcoma fsaii , presenting a wild - type tp53 [ 27 ]  . 
this in vivo result is clearly in contrast to previous published in vitro experiments , which demonstrated a radioprotective effect of bbi for tumor cells characterized by a wild - type tp53 [ 9 ]  . 
since the use of tumor xenografts combined with single - dose treatment clearly owes several restrictions when the value of a substance for clinical use should be estimated , additional animal studies need to be performed . 
nevertheless , the clear and selective radioprotective effect of bbi on normal - tissue responses , i.e. , radiation - induced leg contracture , observed here is of special interest in radiation oncology . 
 strahlentherapie und onkologie review article cognitive effects of chemotherapy and / or cranial irradiation in adults grit welzel1 , sarah steinvorth2 , frederik wenz1 background : cognitive effects after cranial radiotherapy are widely discussed , but there is growing evidence that chemotherapy may also induce changes in neuropsychological functioning . 
this review summarizes the published literature regarding cognitive functioning after cancer therapy in adult patients . material and methods : 63 reports from january 1980 to july 2003 assessing objective cognitive effects of irradiation and / or chemotherapy by neuropsychologic evaluation were analyzed . 
no clinically relevant differences are found for cognitive deficits , cognitive impairment rate , and single cognitive domains , when chemotherapy , cranial irradiation and combined radioand chemotherapy were compared . 
furthermore , cognitive functioning below average before chemoor radiotherapy is found in subgroups of cancer patients . conclusion : there is evidence of cognitive impairment in adult tumor patients after chemotherapy similar to effects after cranial irradiation . 
more prospective studies with a long - term follow - up using standardized neuropsychometric testing , assessment of premorbid intelligence , and suited control groups are needed . key words : chemotherapy radiotherapy neuropsychology cognitive functions strahlenther onkol 2005 ; 181 : 14156 doi 10.1007 / s00066 - 005 - 1351 - 5 kognitive leistungsfhigkeit von erwachsenen nach chemound / oder kranieller strahlentherapie hintergrund : kognitive nebenwirkungen wurden bisher vor allem nach kranieller strahlentherapie beobachtet und untersucht ; in der literatur finden sich jedoch zunehmend hinweise darauf , dass neuropsychologische vernderungen auch nach chemotherapie auftreten knnen . 
diese bersichtsarbeit fasst die literatur zur kognitiven funktionsfhigkeit nach tumortherapie bei erwachsenen zusammen . material und methodik : es wurden 63 verffentlichungen zwischen januar 1980 und juli 2003 , die objektive kognitive nebenwirkungen nach chemound / oder kranieller strahlentherapie mit neuropsychologischen testverfahren berprfen , analysiert . 
die rate posttherapeutischer kognitiver funktionsstrungen wird lediglich in 28 studien angegeben und liegt in der chemotherapiegruppe bei 44 , 1% ( 1875% ; 451 patienten ) , in der radiotherapiegruppe bei 44 , 0% ( 2983% ; 320 patienten ) und in der radiochemotherapiegruppe bei 64 , 5% ( 30100% ; 229 patienten )  . 
cognitive effects of chemotherapy and cranial irradiation introduction cognitive deficits in adult tumor patients come increasingly into the focus of interest because of their influence on quality of life in patients who are cured of their primary tumor [ 1 , 11 , 18 , 32 , 51 ]  . 
starting from studies with children at the beginning of the 1980s , cognitive deficits were demonstrated in adults over the past years , which were mostly attributed to cranial radiotherapy . 
indeed , there is little data regarding effects of chemotherapy on cognitive functioning , but recent findings show that cognitive impairment can occur after systemic chemotherapy as well [ 12 ]  . 
the incidence and clinical picture of combined neurotoxicity may vary greatly depending upon the schedule of chemotherapy administration , e.g. , before , during or after radiotherapy , the selection and combination of single agents , the precise doses of each modality , the administration route , i.e. , intravenous or intrathecal , and patient factors [ 29 ]  . 
the medline search identified 63 articles by 35 different investigator groups studying objective cognitive deficits after irradiation , chemotherapy , or combined radiochemotherapy by neuropsychological evaluation and analyzing a random sample size with a minimum of ten patients . 
 six trials were excluded from the analyses for one or more of the following reasons : the trial was published again with an extended sample size and the same results , the tested cognitive domains were not specified , or no objective cognitive assessment was used . 
 statistical methods ( cid : 1 ) 2 - testing or exact ( cid : 1 ) 2 - testing was performed for all proportions , and the mann - whitney u - test was used for all by sample size - weighted means . 
 we found no significant differences for cognitive deficits at all , cognitive impairment rate , and single cognitive domains , if specified , when chemotherapy , irradiation and combined radioand chemotherapy were compared . 
only 28 trials with 1 , 000 patients reported percentages on patients with deficits after differentiated cognitive testing > 15.8% as expected from a normally distributed population ( 15.8% aberrant results are expected in a normally distributed population )  . 
the weighted mean rate of patients with cognitive impairment was 44.1% in the chemotherapy group ( range 1875% ; 451 patients ) , 44.0% in the radiotherapy group ( range 2983% ; 320 patients ) , and 64.5% in the combined irradiation and chemotherapy group ( range 30100% ; 229 patients )  . 
the characteristics of these trials , including author , publication year , patient number , tumor entity , therapy regimen , tested cognitive domains , and main results are shown in appendix a . 
one trial demonstrated differences to healthy controls [ 12 ] , and one trial demonstrated differences to a mixed control group consisting of healthy controls and patients without chemotherapy [ 57 ]  . 
in one trial deterioration during follow - up was reported [ 44 ] , and three trials identified cognitive impairment already before chemotherapy [ 28 , 41 , 44 ]  . 
 in most published studies reporting individual test data , deficits in memory functions ( 80% of ten studies ) , attention functions ( 70% of ten studies ) , visuospatial functions ( 60% of five studies ) , and motor functions ( 50% of six studies ) during or after chemotherapy were found . 
no clear findings were reported for intellectual ( 20% of five studies ) , executive ( 33% of three studies ) , and language functioning ( 25% of four studies )  . 
 out of ten eligible trials reporting quantitative data on patients with cognitive dysfunction after chemotherapy , seven retrospective and two prospective trials with 451 patients performed differentiated cognitive testing [ 1 , 16 , 28 , 40 , 44 , 53 , 54 , 65 , 73 ]  . 
 four trials were excluded from the analyses for one or more of the following reasons : the trial was published again with an extended sample size and the same results , the tested cognitive domains were not specified , or no objective cognitive assessment was used [ 4 , 38 , 69 , 72 ]  . 
 seven different patient groups were examined , including patients with low - grade brain tumor , glioma , not specified glioma and other brain tumors , nasopharyngeal carcinoma , pituitary tumor , skull base tumor , and arteriovenous malformation . overall , in 18 trials ( 90% ) out of the 20 studies summarized in appendix b cognitive dysfunction was noted . 
zeitliches auftreten kognitiver nebenwirkungen nach chemound / oder radiotherapie : anzahl an untersuchungen mit nachweis von nebenwirkungen ( untersuchte patientenzahl ) und gesamtzahl an untersuchungen ( untersuchte patientenzahl )  . 
 chemotherapy impaired / total number irradiation impaired / total number radiochemotherapy impaired / total number overall , cognitive impairment occurred in all four patient groups at different time points ( tables 1 and 2 )  . 
in one trial differences to published test norms [ 59 ] , and in another trial differences to healthy controls at baseline without further deterioration during follow - up were reported [ 37 ]  . 
in six trials ( 67% ) deteriorations during follow - up were found : transient worsening at 1 day or 6 months after treatment [ 7 , 9 , 58 , 68 ] , and deficits at 2 years up to 6 years after treatment [ 8 , 9 , 20 ]  . in most published studies reporting individual test data , deficits in memory functions ( 50% of 20 studies ) , motor functions ( 50% of eight studies ) , and executive functions ( 40% of ten studies ) during or after radiotherapy were found . 
deficits in attention functions were observed in 35% of 17 studies , deficits in language domains in 33% of nine studies , deficits in intellectual functioning in 29% of 14 studies , and deficits in visuospatial functions in 18% of eleven studies . 
patientengruppen mit kognitiven nebenwirkungen nach chemound / oder radiotherapie : anzahl an untersuchungen mit nachweis von nebenwirkungen ( untersuchte patientenzahl ) und gesamtzahl an untersuchungen ( untersuchte patientenzahl )  . 
 [ 53 ] out of nine eligible trials reporting quantitative data on cancer patients with cognitive dysfunction after cranial irradiation , eight trials with 320 patients performed differentiated cognitive testing [ 8 , 9 , 20 , 22 , 30 , 42 , 59 , 68 ]  . 
 in three trials data to the number of glioma patients with cognitive dysfunction before radiotherapy or without irradiation were reported , indicating cognitive impairment in 48% , 44% , and 29% of patients [ 8 , 30 , 59 ]  . 
in most studies the cognitive deficits were not related to mood disturbances , and we found no significant differences between cognitive deficits after irradiation compared to cognitive deficits after chemotherapy ( p > 0.05 for cognitive deficits at all , cognitive impairment rate , and single cognitive domains , if specified )  . 
there was evidence of pronounced cognitive impairment after whole - brain irradiation compared to focal irradiation [ 22 ] , after single doses > 2 gy [ 39 ] , and in patients with tumor progression [ 62 ]  . 
however , transient deficits in verbal memory functioning 1 day and 3 months after therapy [ 7 , 9 , 58 ] or in attention functioning 6 months after therapy [ 68 ] were reported . 
by contrast , improvements were observed for intelligence , memory , or attention functioning after radiosurgery in patients with arteriovenous malformations and after focal irradiation in patients with low - grade brain tumors or meningiomas [ 9 , 37 , 58 , 59 ]  . 
overall , seven different patient groups were examined , including patients with glioma , mixed tumors , hematologic malignancies and breast cancer , small - cell lung cancer , brain tumors , and nasopharyngeal carcinoma . 
eight retrospective trials showed differences to published test norms [ 5 , 15 , 24 , 25 , 34 , 48 , 49 , 63 ] , but no differences to patients without irradiation and radiochemotherapy , respectively [ 48 , 49 ]  . 
in three retrospective trials differences to healthy controls were found [ 6 , 33 , 67 ] , but no differences to patients with chemotherapy alone [ 67 ]  . 
a total of four trials showed differences to published test norms at baseline [ 10 , 21 , 31 , 48 ] , but no differences to patients without irradiation [ 10 , 21 ]  . 
one trial reported differences to patients without prophylactic cranial irradiation shortly after irradiation and deterioration during further follow - up [ 64 ] , and in another trial memory deficits to test norms at baseline and during further follow - up were found [ 48 ]  . 
furthermore , five trials reported improvement in intelligence , memory , or attention functioning at shortand long - term follow - up [ 11 , 33 , 48 , 49 , 71 ]  . 
the two trials reporting data for partial - brain radiotherapy showed poorer memory performances in patients with nasopharyngeal carcinoma [ 33 ] , and no general deterioration in intelligence screening in high - grade glioma patients [ 61 ]  . 
 in most published studies reporting individual test data , deficits in memory ( 62.5% of 16 studies ) , executive ( 60% of five studies ) , attention ( 56% of 18 studies ) , language ( 40% of five studies ) , motor ( 33% of six studies ) , and intellectual functioning ( 25% of 16 studies ) during or after combined radioand chemotherapy were found . 
 out of nine eligible trials reporting numerical data about patients with cognitive dysfunction after combined radioand chemotherapy , seven retrospective trials with 229 patients performed detailed cognitive testing [ 5 , 6 , 15 , 24 , 25 , 34 , 49 ]  . 
 overall , we found no significant differences between cognitive deficits after combined radiochemotherapy compared to cognitive deficits after chemotherapy or cranial irradiation ( p > 0.05 for cognitive deficits at all , cognitive impairment rate , and single cognitive domains , if specified )  . 
 however , deficits in memory functioning immediately after therapy , attention functioning and logical thinking 1 month after therapy , attention functioning 4 months after therapy , and cognitive functioning 6 months after therapy are reported [ 2 , 21 , 47 , 64 ]  . 
there was evidence of pronounced cognitive impairment in elderly brain tumor patients with earlier tumor progression and shorter survival [ 61 ] , after high - dose irradiation [ 45 ] , and before cranial radiotherapy or radiochemotherapy in patients with small - cell lung cancer or mixed tumors [ 10 , 31 , 47 , 48 , 66 ]  . 
data also suggest that some individuals might be more vulnerable than others , however , the risk factors are currently unknown due to the lack of understanding of the underlying mechanisms . 
no significant differences were found for cognitive deficits at all , cognitive impairment rate , and single cognitive domains , if specified , when chemotherapy , irradiation and radiochemotherapy were compared ( although knowing that a direct statistical comparison as done for the purpose of this review is not absolutely valid due to extremely different criteria for cognitive impairment )  . 
there is evidence of pronounced cognitive impairment for memory and motor functioning after chemotherapy , for memory , motor , executive , attention , and visuospatial functioning after irradiation , and for memory , executive , and attention functioning after combined irradiation and chemotherapy . 
cognitive impairment is found in different patient groups at different time points , supporting the hypothesis of chemotherapyinduced cognitive deficits contrary to an influence of hormonal factors as it is discussed for women with breast cancer [ 29 ]  . 
in the radiotherapy group 70% of all prospective trials indicate reversible or irreversible cognitive impairment immediately and up to 6 years after irradiation [ 79 , 20 , 52 , 58 , 68 ]  . 
report subtle cognitive impairment in patients with chordomas and chondrosarcomas [ 20 ] , and three trials observed transient deteriorations in verbal memory or attention functioning [ 7 , 58 , 68 ]  . 
similar to cognitive impairment before chemotherapy , cognitive deficits before irradiation are reported as well for patients with brain tumors ( visual memory , sentence recall ) , astrocytomas and oligodendrogliomas ( memory , attention , visuospatial functioning ) , and arteriovenous malformations ( intellectual , memory , attention functioning ) [ 9 , 37 , 59 ]  . 
widespread cognitive impairment was found in 42% of prospective trials during , immediately and up to 3 years after therapy in the combined chemotherapy and irradiation group [ 3 , 11 , 48 , 61 , 64 ]  . 
cognitive impairment before combined radioand chemotherapy was predominantly observed in patients with small - cell lung cancer [ 10 , 21 , 31 , 66 ] , supporting the hypothesis of paraneoplastic effects in these patients . 
found improved attention functioning immediately after chemotherapy indicating a practice effect followed by deterioration in memory immediately after prophylactic cranial irradiation in patients with small - cell lung cancer [ 2 ]  . 
reported improvement in attention functioning immediately after the first radiation fraction attributed to a practice effect and improvement in memory and attention functioning at further follow - up [ 70 , 71 ]  . 
observed a tendency to improvement in intellectual and attention functioning in patients with different tumor types after therapeutic cranial irradiation [ 48 ]  . overall , there is evidence of pronounced cognitive impairment in elderly brain tumor patients with earlier tumor progression and shorter survival , after high - dose irradiation , and before any cancer treatment in patients with small - cell lung cancer . 
in most studies reporting percentages to the number of impaired patients , the criterion was at least one , one and a half or two standard deviations below the mean of normative data for age - standardized scores , with impairment in at least one cognitive doma from this classic neuropsychological standpoint , most of the patients have subtle cognitive impairment when compared to normative data for age - standardized scores . 
it cannot be excluded that therapy - related subtle cognitive dysfunction may have serious and persisting implications for the adequacy of the patients daily quality of life or professional life . 
 strahlentherapie und onkologie original article can intensity - modulated radiation therapy of the paraaortic region overcome the problems of critical organ tolerance ? johanne hermesse , magali devillers , jean - marie deneufbourg , philippe nickers1 background and purpose : the recent rtog guidelines for future clinical developments in gynecologic malignancies included the investigation of dose escalation in the paraaortic ( po ) region which is , however , very difficult to target due to the presence of critical organs such as kidneys , liver , spinal cord , and digestive structures . 
the aim of this study was to investigate intensity - modulated radiotherapys ( imrt ) possibilites of either increasing , in a safe way , the dose to 5060 gy in case of macroscopic disease or decreasing the dose to organs at risk ( or ) when treatment is given in an adjuvant setting . 
 material and methods : the dosimetric charts of 14 patients irradiated to the po region at the department of radiation oncology , university hospital of lige , belgium , in 2000 were analyzed in order to compare six - field conformal external - beam radiotherapy ( cebr ) and five - beam imrt approaches . 
students t - test was used to compare the paired dvh data issued from cebr and imrt planning . results : the imrt approach allowed to cover the ptv at a higher level as compared to cebr . 
doses to the liver remained low regardless of the method used . conclusion : at 60 gy , imrt is largely sparing the spinal cord and kidneys as compared to cebr and represents an interesting approach not only for dose escalation up to 5060 gy ( probably facilitating the radiochemotherapy approaches ) but also in an adjuvant setting at lower doses . 
the dosimetric data of this study are in the same range as those published recently with a dynamic arc conformal approach . key words : paraaortic intensity - modulated radiotherapy strahlenther onkol 2005 ; 181 : 18590 doi 10.1007 / s00066 - 005 - 1324 - 8 kann intensittsmodulierte radiotherapie der paraaortalen region probleme der strahlentoleranz gefhrdeter organe berwinden ? hintergrund und ziel : die erstellung der aktuellen rtog - leitlinien fr klinische entwicklungen in der gynkologischen onkologie erforderten auch untersuchungen zur strahlendosiseskalation in der paraaortalen ( po - ) region , die wegen der nhe gefhrdeter organe wie niere , leber , rckenmark und gastrointestinaltrakt ein sehr problematisches zielgebiet ist . 
zweck dieser studie war zu untersuchen , welche mglichkeiten die intensittsmodulierte radiotherapie ( imrt ) bietet , entweder auf sichere weise die strahlendosis auf 5060 gy im fall ausgedehnter malignome zu steigern oder die strahlendosis gefhrdeter risikoorgane in der adjuvanten situation zu vermindern . 
 material und methoden : die dosimetriekarten von 14 patientinnen , bei denen im jahr 2000 in der abteilung fr radioonkologie am universittsklinikum lige , belgien , eine radiotherapie der po - region durchgefhrt worden war , wurden analysiert , um die konformale sechs - felder - radiotherapie ( krt ) mit fnf - felder - imrt - konzepten zu vergleichen . 
irradiation of the paraaortic region schlussfolgerung : bei einer dosis von 60 gy schont die imrt rckenmark und nieren im vergleich zur krt weitgehend und bietet ein interessantes konzept nicht nur fr die dosiseskalation bis zu 5060 gy ( was radiochemotherapie - planungen entgegenkommen drfte ) , sondern auch fr die niedriger dosierte adjuvante strahlentherapie . 
 schlsselwrter : paraaortal intensittsmoduliert radiotherapie introduction in 1988 , the eortc radiotherapy group investigated the place of prophylactic paraaortic ( po ) lymph node irradiation in the treatment of patients with locally advanced cervical cancer [ 7 ]  . 
 the randomized rtog 79 - 20 study included 367 ib or iia cervical cancers , 4 cm in diameter , and stages iib subjected to radiotherapy [ 12 ]  . 
a prophylactic irradiation of the po lymph nodes significantly improved 10 - year overall survival from 44% to 55% ( p = 0.02 ) in comparison with pelvic irradiation only . 
remained any place for po irradiation in an adjuvant approach ? the rtog 92 - 10 study tried to add chemotherapy to extended - field radiotherapy for cervical cancer with biopsyproven positive po nodes but was stopped prematurely for 24% of late grade 3 and 4 toxicity [ 6 ]  . 
disease - free survival ( dfs ) of at least 20% at 5 years has been reported without any prohibitive late toxicity resulting from small or large bowel side effects [ 1 , 13 , 14 ]  . 
one of these studies investigated , on 29 patients , the role of dynamic arc conformal radiotherapy to increase the total dose up to 5560 gy with no late grade 3 side effect [ 1 ]  . 
 until now , no study reported , in detail , the dose volume histograms ( dvhs ) for the clinical target volume ( ctv ) , planning target volume ( ptv ) , and organs at risk ( or ) , neither for an imrt approach nor with an inverse planning philosophy [ 1 , 11 ]  . 
from ct scan data of patients irradiated to the po region , this study is investigating imrts possibilities of increasing the dose to 60 gy in comparison with conformal external - beam radiotherapy ( cebr )  . 
after simulation they underwent a ct scan in supine position , covering the area ( slices 1 cm apart ) from the tenth thoracic vertebra ( t10 ) to the lower border of the bony pelvis . 
spinal cord is a tissue with a high relative seriality implying that a dose above the tolerance limit , even to a small volume , can totally impair the function of the organ ( myelitis )  . 
irradiation of the paraaortic region parallelity , implying that the main parameter for impairing hepatic function is the proportion of the organ that receives a dose above the tolerance level . 
so it was regarded as a whole - unit structure due to a uniform biological function throughout the organ , which can tolerate hot spots focally without significantly impairing the whole function . 
at first , the internal margin , that is defined so as to take variations in size , shape , and position of the ctv in relation to the anatomic reference point into account , was considered nonexistent . 
the setup margins that are added to take uncertainties in patient - beam positioning into account were fixed to 3 mm for ap , 3 mm for left - right , and 5 mm for craniocaudal directions . 
 limit dose ( gy ) volume minimal below ( % ) dose ( gy ) maximal dose ( gy ) ctv spinal cord liver left kidney right kidney digestive structures 5 5 5 66 42 60 40 35 cording to the icru 50 and 62 recommendations , the 95% isodose of the prescribed dose had to circumvent the ptv [ 8 , 9 ]  . 
this approach , however , remains very difficult to achieve due to the presence of or in close vicinity to the ctv like spinal cord , kidneys , and digestive structures . 
so , only techniques largely sparing the or at the highest level offer a chance of safely achieving the minimum level of 5460 gy necessary to sterilize a macroscopic lesion . 
moreover , at lower dose levels required in an adjuvant setting or for lymphomas , seminomas or other malignancies , the higher ballistic selectivity of a radiation treatment is always appreciated in a multidisciplinary treatment approach . 
 recently , published pilot studies suggested that po metastatic lymph nodes are better controlled when doses from 45 to 60 gy are used even with concomitant chemotherapy , while dfs rates of 20% at 5 years have been published [ 13 , 14 ]  . 
on the other hand , when the ptv is analyzed , the heterogeneity of irradiation is higher with cebr , mainly due to the presence of larger volumes irradiated at lower doses . 
for both cebr and imrt , doses to liver and digestive structures remain low with < 25% of the organs receiving < 14 gy and < 35 gy , respectively . 
 whether or not these new technologies will provide a benefit to the patients in terms of survival has to be further investigated in clinical trials , but they will probably make concomitant chemoradiotherapy approaches to the po region safer . 
 strahlentherapie und onkologie original article testicular dose in prostate cancer radiotherapy impact on impairment of fertility and hormonal function dirk boehmer1 , harun badakhshi1 , wolf kuschke2 , joerg bohsung2 , volker budach1 purpose : to determine the dose received by the unshielded testicles during a course of 20 - mv conventional external - beam radiotherapy for patients with localized prostate cancer . 
a flexible tube , containing three calibrated thermoluminescence dosimeters ( tlds ) was placed on top or underneath the testicle closest to the perineal region with a day - to - day alternation . 
 results : the mean total dose ( standard deviation ) measured in a series of 10 subsequent treatment days in all patients was 49 cgy ( 36 cgy )  . 
 conclusion : the dose received by the unshielded testes can be assessed as a risk for permanent infertility and impairment of hormonal function in prostate cancer patients treated with external - beam radiotherapy . 
 key words : prostate cancer radiotherapy testicles fertility strahlenther onkol 2005 ; 181 : 17984 doi 10.1007 / s00066 - 005 - 1282 - 1 hodendosis in der strahlentherapie des prostatakarzinoms . 
auswirkung auf die beeintrchtigung der zeugungsfhigkeit und der hormonellen funktion ziel : bestimmung der strahlendosis an ungeschtzten hoden whrend einer serie mit 20 - mv - photonen und konventioneller externer strahlentherapie bei patienten mit lokalisiertem prostatakarzinokritische evaluation des potentiellen einflusses auf fertilitt und hormonale strungen dieser patienten anhand der literatur . patienten und methodik : die absolute hodendosis von 20 zufllig ausgewhlten patienten , die sich einer strahlentherapie bei prostatakarzinom unterzogen , wurde mittels thermolumineszenzdosimetrie gemessen . 
die individuellen tld wurden ausgewertet und die absorbierte gesamtdosis berechnet . ergebnisse : die mittlere gesamtdosis ( standardabweichung ) , welche whrend der serie von 10 aufeinander folgenden behandlungstagen gemessen wurde , betrug 49 cgy ( 36 cgy )  . 
die ergebnisse werden unter einschluss der verfgbaren literatur bewertet . schlussfolgerung : die whrend einer bestrahlungsserie bei prostatakarzinompatienten von den hoden absorbierte strahlendosis kann als ursache eines erhhten risikos fr eine bleibende infertilitt und hormonale strung angesehen werden . schlsselwrter : prostatakarzinom strahlentherapie hoden fertilitt 1 department of radiation oncology , charit university clinic campus mitte , berlin , germany , 2 department of medical physics , charit university clinic campus mitte , berlin , germany . received : february 11 , 2004 ; accepted : december 9 , 2004 strahlenther onkol 2005 no . 
since prostate - specific antigen ( psa ) measurements have been introduced in 1979 as a screening method for prostate cancer , the rate of detecting earlier tumor stages as well as the number of younger men being detected with prostate cancer have increased . 
in terms of increasing contributions of disease - related information via the internet and the explicit information in the consent discussion , there are now more patients < 60 years of age asking about the impact of treatment on their quality of life . 
regarding the testicular tissue , the spermatogonial stem cells represent the main target concerning fertility , as these cells are known to be among the most radiosensitive cells in the human body . 
found that there is a relative increased radiosensitivity ( even after 11 cgy irradiation ) in early differentiating spermatogonia , compared to spermatogonial stem cells and late differentiating spermatogonia [ 24 ]  . 
for rhesus monkeys undergoing total - body irradiation ( 48.5 gy ) at the age of 24 years , it was demonstrated after a 3to 8 - year follow - up , that testes were devoid of germ cells after having received a dose > 8 gy and cross sections of all monkeys showed indications for extensive germ cell killing [ 9 ]  . 
there is also evidence that radiation - induced damage to germ cells is dependent on the dose rate , with more damage induced at an ldr compared to an hdr [ 28 ]  . 
on the other hand , there is evidence that external - beam radiotherapy of prostate cancer patients results in a significant and persistent change in hormone levels even after a follow - up of 38 years , which significantly increased the rate of hypogonadism and testicular atrophy [ 7 , 8 ]  . 
doses < 20 cgy had no influence on follicle - stimulating hormone ( fsh ) secretion , whereas higher doses led to a transient fsh increase [ 31 ]  . 
the clinical target volume ( ctv ) comprised the prostate alone in low - risk patients and the prostate plus a 5 - mm margin in all directions for patients with intermediate risk . 
 tld dosimetry tld dosimetry was performed using lithium - fluorine rods with a diameter of 1 mm and a length of 6 mfirst of all , a set of tlds for patient dosimetry had to be selected as follows : 100 tlds were irradiated ten times with a dose of approximately 0.5 gy cobalt - 60 ( 60co ) - ray , each time followed by an annealing cycle . 
for calibration three tld rods at a time were placed within a plastic tube of approximately 4 cm length and 1.8 mm inner diameter , which was sealed at both ends . 
 after the tlds had been irradiated ten times during the patients treatment , they were analyzed in the tld reader and the resulting doses were calculated , using the tld - specific calibration factors . 
 the specific doses to the testicles of each patient were calculated from the mean dose of the three tlds and extrapolated according to formula 1 , thus representing the testicular dose for a treatment course of 40 fractions . dtot = dtld fplan dtot = dtld firr dtot = dtld formula 1 . 
in order to achieve comparable results , we assumed that all patients would have received 40 treatment fractions and recalculated the tld readouts . all given results represent the dose of a treatment course of 40 fractions . 
two out of five patients showed no toxicity at all , two had mild toxicity ( maximum grade 1 ) , and one patient experienced grade 3 genitourinary and grade 2 gastrointestinal toxicity . 
because of lacking data on testicular dose measurements in prostate cancer patients , the presented literature focuses on data of low radiation doses to the testes from patients being treated with radioiodine or radiotherapy for thyroid cancer , hodgkins disease or testicular cancer . 
noted no impairment of fertility in all patients who wished to have children , despite a transient increase of fsh which returned to normal values within 9 months [ 20 ]  . 
concluded from low sperm counts of patients with seminoma and radiotherapy , that oligospermia is likely to be the result of highly impaired preradiotherapy sperm cell production and not the expression of radiotherapy damage [ 10 ]  . 
after a follow - up of 38 years they found a significant decrease in testosterone levels , and an increase in lh and fsh levels for the irradiated group , indicating that prostate bed irradiation leads to a prominent and permanent testicular damage [ 7 , 8 ]  . 
older studies investigating the effect of prostate external - beam radiotherapy found similar results concerning fsh and lh serum levels , but on the other hand , the measured low testosterone levels returned to normal values within 2 years of follow - up [ 14 , 32 ]  . 
higher doses , in the range of 1420 gy , as applied for patients with carcinoma in situ of the testis , induce a long - term negative impact on hormonal function . 
retrospektive studien , welche den einfluss der testikulren dosis auf die fertilitt untersucht haben . author patients ( n ) irradiation of testicular dose ( cgy ) impairment of fertility hyer et al . 
 [ 17 ] 122 8 27 8 17 14 5.421.2 thyroid cancer 158 seminoma 120480 seminoma 7178 seminoma hodgkins disease 670 seminoma 32178 + ( 5 / 8 patients ) + ( 7 / 8 patients ) + ( 2 / 8 patients ) + ( 10 / 14 patients ) strahlenther onkol 2005 no . 
 the main factor influencing the overall scattered dose ( including the dose due to backscatter ) to the testicles was found to be the distance of the testes to the lower field border and the occasion of a port fila portal image increased the total testicular dose by 2.5 cgy per fraction , which in a study by amies et al . 
with respect to the potential increase of germ cell and hormonal impairment , this policy has to be appraised critically . a simple method of testicular protection is the use of a sufficient gonadal shield , most commonly made of lead . 
in 1982 , kubo & shipley described a reduction of testicular dose to negligible levels when a 10 cm thick lead scrotal block above the scrotum immediately outside the field was added to a standard clam - shell shielding [ 23 ]  . 
the same conclusion and recommendation were given in an evaluation of 207 men in the southwest oncology group study of orchidectomy and irradiation of patients with seminoma ( swog - 8711 ) [ 13 ]  . 
 conclusion summarizing our results and data from the literature , there is strong evidence that doses received by unshielded testicles during a course of radiotherapy for localized prostate cancer result in an impairment of the reproductive function of testicular tissue . 
although there are contradictory data about the question whether this is a transient or permanent impairment , we recommend that patients who have not completed their family planning , must be informed about the possible deteriorating effect of irradiation on their reproductive function . 
as erectile function mainly depends on normal testosterone levels , the effect of testicular scattered irradiation may contribute substantially to the known rates of erectile dysfunction after prostate cancer radiotherapy . 
although prostate cancer patients usually have completed family planning , it seems reasonable to offer testicular shielding in the rare case of those men who are still planning to have children . 
gross1 , alison kraus2 , kamal nashwan1 , hans - dieter mennel2 , rita engenhart - cabillic1 , juergen schlegel3 background and purpose : primary glioblastomas ( gbms ) are highly radioresistant , and in contrast to secondary gbms , they bear wild - type ( wt ) p53 protein , which is stabilized in a proportion of these tumors . 
additionally , the authors tried to identify , in vitro , subgroups of primary gbm with different susceptibilities to irradiation , on the basis of their p53 and p21 responses to ionizing radiation . material and methods : tumor tissue samples from 31 patients suffering from primary gbm undergoing a combined radiochemotherapy with topotecan were investigated . 
p53 protein expression was measured by western analysis and p21 mrna expression by reverse transcription - polymerase chain reaction ( rt - pcr )  . results : the percentage of p53 - positive cells within the tumor specimens obtained from the 31 patients ranged from 0% to 28% , the median value being 4.3%. 
despite these responses , g1 arrest was not detectable in any of the gbm cultures . conclusion : p53 protein expression in vivo does not correlate with the outcome of patients with primary gbm . 
 the failure of g1 arrest seems to be due to a functional defect in the p53 pathway , either because p21 was not induced or because of an unidentified defect downstream from p21 . key words : glioblastoma p53 p21 prognostic factors p53und p21 - expression in primren glioblastomen hintergrund und ziel : in primren glioblastomen ( gbm ) liegt die wildtyp - ( wt - ) form des tp53 - gens mit stabilisierung des proteins in einem teil der tumoren vor . 
kann die p53 - expression in vivo aussagen ber das ansprechen auf eine radiochemotherapie liefern , und lassen sich auf dem boden der p53und p21 - antwort auf bestrahlung prognostisch differente subgruppen primrer gbm in vitro identifizieren ? material und methodik : tumorgewebe von 31 gbm - patienten , die mit topotecan kombiniert radiochemotherapiert wurden , wurde immunhistochemisch auf p53 - protein ausgewertet . 
basale p21 - expression bestand in strahlenther onkol 2005 ; 181 : 16471 doi 10.1007 / s00066 - 005 - 1304 - z 1 department of radiotherapy and radiooncology , philipps university of marburg , germany , 2 department of neuropathology , philipps university of marburg , germany , 3 division of neuropathology , technical university , muenchen , germany . received : march 24 , 2004 ; accepted : november 30 , 2004 strahlenther onkol 2005 no . 
trotz der reagibilitt von p53 und p21 kam es bei keiner zelllinie zu einem g1 - arrest . schlussfolgerung : in vivo korreliert der p53 - protein - gehalt der gbm nicht mit den therapieergebnissen , so dass der p53 - nachweis keine prognostische relevanz aufweist . 
adjuvant radiotherapy , however , provides an improvement in the prognosis , increasing the median survival time to about 1 year [ 13 , 14 , 24 , 28 , 30 , 39 ]  . 
the search for novel therapeutic strategies in gbm requires clearer insight into the mechanisms involved in the cellular response to ionizing radiation . a distinction between different gbms on clinical grounds has long been recognized . 
approximately 7580% of gbms arise de novo , without history of progression from a grade ii or iii glial tumor , and are referred to as primary gbthese tumors are genetically characterized by a loss of chromosome 10 and epidermal growth factor receptor ( egfr ) gene amplification occurring predominantly in older patients and exclusively in gbms , being demonstrable in neither grade ii nor grade iii astrocytomas [ 25 , 38 ]  . 
by contrast , approximately 2025% of gbms show progression from astrocytoma or anaplastic astrocytoma and are clinically referred to as secondary gbthis second genetic subgroup of gbm displays mutations in the tumor suppressor gene tp53 [ 31 ]  . 
histologically , primary and secondary gbms cannot be distinguished from each another , as both exhibit tumor necrosis , vascular endothelial proliferation , and cellular atypia . the mutant tp53 present in secondary gbms readily explains their radioresistance . 
although the functional significance of this stabilized p53 protein is not understood , it raises the possibility that p53 functions abnormally in at least some primary gbms , despite the presence of an intact tp53 gene . 
thus , a functional defect in p53 or its pathway might account for the genetic instability and radioresistance of primary gbms [ 32 ]  . the tumor suppressor gene tp53 has been shown to play a pivotal role in bringing about an arrest at the g1 / s transition [ 5 , 41 ]  . 
activation of p53 by dna damage leads to the transcriptional activation of p21 , an inhibitor of the cyclin - dependent kinases regarded as the engine of the cell cycle , responsible for driving the cell through the various phases of the cycle when bound to its respective cyclin [ 6 ]  . 
since g1 arrest can be induced by the overexpression of p21 and , furthermore , is abrogated in irradiated p21 - deficient cells [ 3 , 40 ] , p21 seems to be the key effector of the g1 arrest in response to dna damage . 
while some groups showed that p21 is solely dependent on p53 for its induction , for example in human peripheral neuroepithelial tumor cell lines [ 15 ] , other groups maintain that p21 can be induced independently of p53 [ 18 ]  . therefore , the aim of this project was to determine the impact of p53 status on intracellular pathways in primary gbm cells , and g1 arrest in vitro . 
additionally , we investigated the value of p53 expression on survival rates in vivo in primary gbm treated with simultaneous radiochemotherapy . material and methods patients and methods a total of 31 patients with histologically confirmed supratentorial primary gbm without a known history of low - grade tumor were enrolled in the study . 
a total dose of 60 gy in daily fractions of 2.0 gy with simultaneous chemotherapy with 0.5 mg topotecan ( hycamtin ) intravenously administered 1 h prior to each irradiation was given as described previously [ 10 ]  . 
histological paraffin sections of these 31 samples were immunohistochemically stained , using a monoclonal mouse antibody ( ncl - tp53 - do7 , novocastra ltd , newcastle , uk ) specific to human wt and mutant p53 prote for the detection of bound antibodies , a rabbit anti - mouse antibody and an abc peroxidase kit were used . 
diaminobenzidine was used as the chromogen , and slides were counterstained with hematoxylin and eos the percentage of p53 - immunopositive tumor cells was calculated for five consecutive microscopic fields per sample using a 400 - fold magnification resulting in 250300 cells evaluable in each microscopic field . 
 all primary cell cultures were maintained as monolayers in rpmi , supplemented with 10% fcs , 2 mm l - glutamine , penicillin ( 100 u / ml ) and streptomycin ( 100 g / ml )  . 
at and above a dose of 6 gy , ln 229 cells showed a modest arrest in g1 with the effect plateauing at a maximum between 7 and 12 gy . 
at 24 h after irradiation , irradiated and nonirradiated control cells were fixed in 70% methanol for flow cytometric analysis of the cell cycle status and were subjected to a cytotoxicity test . 
cell material was lysed under highly denaturing conditions to inactivate rnases and diluted in a high - salt buffer syste the sample was applied to a spin column containing a silica gel - based membrane , which bound total rna during the subsequent washes . 
 protein extraction according to standard protocol [ 36 ] , after two washes in cold pbs the proliferating cells were incubated for 10 min on ice in triton x - 100 lysis buffer ( 50 mm tris - cl , 5mm edta , 1% triton x - 100 , 150 mm nacl , 1 mm pmsf , 80 ng / ml apoprotein , 50 ng / ml leupeptin , 4 ng / ml pepstatin )  . 
the membrane was incubated for 1 h at room temperature with an hrp - conjugated anti - rabbit igg antibody , before incubation with lumiglo reagent ( 20 concentrate )  . 
expression of p53 and p21 flow cytometry at 24 h after treatment , asynchronous irradiated cells and nonirradiated control cells were fixed in ice - cold 70% methanol , then incubated with 5 g rnase , and subsequently stained with 0.05 mg / ml propidium iodide . 
at the time of diagnosis , mean age was 59 7.5 ( mean standard deviation [ sd ] ) years and median age was 58.8 years ( range , 4373 years )  . 
there was a slight tendency toward a better outcome with elevated p53 level , but our data showed no statistical significance . median time to tumor progression was 206 days ( 7 months )  . 
 irradiation effects in vitro the biological effect of irradiation was measured in terms of the percentage of cells present in g1 phase of the cell cycle at 24 h after irradiation compared to nonirradiated control cells at the same time point , as shown in table 2 . 
in the cell line ln 229 ( gbm cell line with one mutant tp53 allele , but functional p53 protein ) , no significant response to irradiation was observed until a dose of 6 gy was table 1 . 
expression of p53 and p21 survival ( days ) progression - free survival f ( x ) = 285 x + 224 r = 0.1070 overall survival f ( x ) = 198 x + 450 r = 0.0448 frequency survival disease - free survival censored 2000 1500 1000 500 1000 1500 2000 p53 - positive - cells ( % ) time after diagnosis ( days ) figure 2 . 
at and above this dose of 6 gy , the ln 229 cells showed a modest arrest in g1 with the effect plateauing at a maximum between 7 and 12 gy . 
 in those primary gbm cultures with no detectable basal p53 protein expression , the level of p53 protein either remained undetectable ( two out of four cases ) or showed a modest increment ( two cases ) after irradiation . 
 a pronounced reduction in p53 protein was observed after irradiation in six of the seven glial tumor primary cultures which exhibited increased basal p53 protein expression , as shown in table 2 . 
in four out of the six gbms exhibiting basal p21 overexpression , irradiation caused a reduction in the p21 expression , and in one case p21 expression showed an additional increase ( g145 )  . 
 discussion for radioresistant tumors such as gbms , a deeper understanding of the mechanisms involved in the response to ionizing radiation is crucial in order to permit the development of improved therapeutic strategies . 
secondary gbms bear a mutation in the tumor suppressor gene tp53 , while primary gbms are characterized by amplification of the egfr gene and deletion of chromosome 10 [ 20 ]  . 
the equally pronounced genetic instability and radioresistance seen in primary gbms , however , cannot be accounted for by their characteristic genetic alterations , which bear no reported signaling connection to apoptotic pathways . 
 instead , the radioresistance of primary gbms indicates that , despite the presence of wt tp53 , the p53 pathway is functionally defective in these gbms [ 32 ]  . in the primary gbms that we investigated in vivo , the percentage of p53 protein - positive cells did not correlate with disease - free survival or overall survival . 
while this study needs to be expanded to improve validity of the results , this is in agreement with the findings of other groups [ 1 , 2 , 26 ]  . disease - free survival and overall survival in our collective were comparable to reported data in the literature [ 39 ] , although our collective shows a favorable rate of long - time survivors . 
this may be due to our administration of chemotherapy , which is known to improve prognosis [ 9 ] or intensive salvage treatment , which involves further surgery or radio and chemotherapy . 
nevertheless , genetic alterations within the p53 - p21 pathway in vitro do correlate with reduced radiosensitivity in some cases , as shown in this study and other reports [ 1 , 8 , 40 ] , but the mechanisms causing radioresistance still remain unclear . 
in about half of our series of primary gbm cultures , p21 overexpression has been cell cycle change after irradiation ( % ) g1 - phase s - phase g2 / m - phase figure 4 . 
despite adequate induction of p21 in the remaining gbms after irradiation , g1 arrest was not achieved , indicative of a defect in the p53 pathway downstream from p21 in these cases . 
a significant correlation between the level of irradiation - induced g1 arrest and degree of radiosensitivity has been demonstrated in a series of tumor cell lines of varying radiosensitivities [ 27 ]  . 
this is in agreement with the concept that normal p53 function is required for sensitivity of tumor cells to dna - damaging insults such as irradiation [ 7 ]  . 
the traditional model of p53 activity proposes that activation of p53 by dna damage causes g1 arrest , permitting repair before dna synthesis in s - phase , unless the damage is beyond repair , in which case p53 eliminates the cell by apoptosis . 
 the intricate relationship between control of the g1 checkpoint and susceptibility to irradiation - induced apoptosis has particular bearing to the overexpression of p21 , which has been detected in a subgroup of this series of primary gbm cultures . 
irradiation of cultures with basal p21 overexpression failed to achieve p21 induction in most cases and no g1 checkpoint halt was achieved , indicating a functional defect in overexpressed p21 . 
this implies that a defect downstream from p21 occurs in this subgroup of primary gba possible candidate is the rb gene , which is deleted in approximately 30% of gbms [ 4 ]  . 
 wild - type p53 is not normally detected by western blot analysis because the half - life of wt p53 protein is very short , while mutant p53 protein , which has a longer half - life , is frequently detectable . 
the finding of detectable wt p53 protein is indicative of an abnormally prolonged half - life and consequent stabilization of wt p53 in these primary gb in all except one gbm primary cultures with increased basal p53 protein expression , irradiation led to a marked reduction in the protein level . 
this suggests that irradiation stimulated degradation of the stabilized p53 prote in a little more than half of these cases the defect appears to lie at or above the level of p53 , since induction of p21 after irradiation fails . 
further in vitro and in vivo studies on the radioand chemosensitivity of individual tumor cell cultures and correlation with other genetic alterations are relevant for the prediction of patient outcomes and the establishment of individualized therapy . acknowledgments we are most grateful to f . 
 strahlentherapie und onkologie original article radiosensitivity of tumor cell lines after pretreatment with the egfr tyrosine kinase inhibitor zd1839 ( iressa ) susanne burdak - rothkamm1 , 2 , claudia e . 
rbe1 , tan phu nguyen1 , daniela ludwig1 , klaus feldmann3 , thomas wiegel4 , christian rbe1 background and purpose : the epidermal growth factor receptor ( egfr ) tyrosine kinase inhibitor zd1839 ( iressa ) reduces survival and augments radiation response of certain tumor cells . 
clonogenic cell survival was determined by colony assays , egfr and transforming growth factor - ( tgf - ) expression by quantitative real - time reverse transcription - polymerase chain reaction ( rt - pcr ) , cell cycle distribution and apoptosis by flow cytometry . 
fadu cells expressed relatively high amounts of egfr and tgftranscripts and showed marked inhibition of clonogenic growth , reduction of s - phase cells , and induction of apoptosis after treatment with 1 m zd1839 and combined treatment . 
 key words : egfr tyrosine kinase inhibitor zd1839 ( iressa ) radiosensitization non - small - cell lung cancer head and neck squamous cell carcinoma tgf strahlenther onkol 2005 ; 181 : 197204 doi 10.1007 / s00066 - 005 - 1319 - 5 strahlenempfindlichkeit von tumorzelllinien nach vorbehandlung mit dem egfr - tyrosinkinase inhibitor zd1839 ( iressa ) hintergrund und ziel : der epidermal growth factor receptor - ( egfr - ) tyrosinkinase - inhibitor zd1839 ( iressa ) reduziert das zellberleben und verstrkt die strahlenwirkung auf verschiedene tumorzelllinien . 
ziel dieser studie war es zu untersuchen , mit welchen anderen zellulren ereignissen die modulation der strahlenempfindlichkeit durch zd1839 assoziiert ist . material und methodik : die drei tumorzelllinien a549 , h596 und fadu wurden mit ionisierender strahlung und zd1839 allein sowie in kombination behandelt . 
zellberleben wurde im koloniebildungstest bestimmt , egfrund transforming growth factor - ( tgf - ) - expression durch quantitative real - time - rt - pcr ( reverse - transkription - polymerase - kettenreaktion ) , zellzyklusverteilung und apoptose in der durchflusszytometrie . ergebnisse : in a549und h596 - zellen war der effekt von zd1839 auf die koloniebildung gering , jedoch zeigten die berlebenskurven einen radiosensibilisierenden effekt von 5 m zd1839 auf a549 - zellen . 
fadu - zellen exprimierten eine vergleichsweise hohe anzahl an egfr und tgf - - transkripten und wiesen eine deutliche inhibition der koloniebildung , eine reduktion von s - phase - zellen und eine induktion der apoptose nach behandlung mit 1 m zd1839 und kombination mit bestrahlung auf . 
behandlung mit zd1839 fhrte zu einer abnahme der egfr - mrna - expression in a549 - zellen , keiner vernderung in h596 - zellen und sogar einem anstieg in fadu - zellen . 1 department of radiotherapy , saarland university hospital , homburg / saar , germany , 2 gray cancer institute , northwood , middlesex ha6 2jr , uk , 3 astrazeneca gmbh , wedel , germany , 4 department of radiotherapy , university hospital benjamin franklin , berlin , germany . received : may 14 , 2004 ; accepted : january 14 , 2005 strahlenther onkol 2005 no . 
zd1839 and radiation in tumor cell lines schlussfolgerung : in den untersuchten zelllinien korrelierte die empfindlichkeit gegenber behandlung mit zd1839 mit der menge an egfr - transkript , der inhibition der zellproliferation und der apoptoseinduktion . 
 schlsselwrter : egfr - tyrosinkinase - inhibitor zd1839 ( iressa ) ionisierende strahlung nichtkleinzelliges bronchialkarzinom kopf - hals - tumoren tgf introduction recent advances in the elucidation of cell signaling networks and the development of novel agents targeting molecular pathways that affect tumor growth have led to new perspectives in cancer therapy [ 5 , 7 , 8 , 17 , 38 ]  . 
erbb receptor signaling can be induced by binding of several ligands including epidermal growth factor ( egf ) and transforming growth factor ( tgf - ) as well as by ionizing radiation through the release of tgf [ 12 ] and activation of the egfr tyrosine kinase [ 41 ]  . 
several intracellular pathways such as ras / raf / mitogen activated protein kinase ( mapk ) pathway , phosphatidylinositol 3 kinase ( pi3k ) and akt , jun n terminal kinase cascade ( pak - jnkk - jnk ) , and the signal transducers and activators of transcription ( stats ) are involved in egfr signaling [ 3 , 32 , 46 ]  . 
proproliferative signals of the egfr are predominantly mediated through mapk but also through pi3k , whereas signaling toward pi3k and akt results in anti - apoptotic signals [ 40 ]  . 
 the egfr and one of its ligands , tgf - , are overexpressed in a variety of solid tumors including non small cell lung cancer ( nsclc ) [ 37 , 44 ] and squamous cell carcinoma of the head and neck ( scchn ) [ 14 ] thus establishing an autocrine pathway in coexpressing tumor cells . 
an elevated egfr expression level was found as a strong prognostic indicator in head and neck cancers associated with reduced recurrence free survival or overall survival , whereas it poorly correlates with patients outcome in nsclc [ 31 ]  . 
egfr expression is inversely correlated with radiocurability in a mouse tumor model [ 1 ]  . as the blockage of the egfr / tgfautocrine pathway has been proposed as a potential therapeutic modality , several inhibitors of egfr signaling have been developed [ 23 , 24 , 26 , 34 ] : antibodies which block the egfr ectodomain , several small molecule egfr tyrosine kinase inhibitors , and an antisense egfr construct for genetic therapy usage . 
 the orally active egfr tyrosine kinase inhibitor zd1839 ( iressa ) is a potent inhibitor of proliferation in egfr overexpressing cells and egfr positive cells that overexpress erbb2 [ 2 ]  . 
first clinical trials have proven zd1839 to be well tolerated and effective in patients with solid malignant tumors , and further clinical studies on zd1839 monotherapy and combination with chemotherapeutic drugs , hormone therapy and radiotherapy are being conducted [ 22 , 35 , 36 , 39 ]  . 
recent results from the monotherapy trial ideal 1 and 2 in lung carcinoma patients ( nsclc ) revealed a response rate of 1020% with mean survival of 68 months , but in the intact study on combination of chemotherapy with zd1839 in nsclc treatment no increase in survival rates could be detected [ 20 , 22 ]  . 
 surprisingly , no correlation was found between egfr expression level in tumor samples of nsclc patients from the ideal 1 and 2 trial prior to treatment and response to zd1839 monotherapy [ 4 ]  . 
in vitro experiments and animal studies have proven an enhancement of antitumor activity of single dose or fractionated irradiation [ 6 , 16 , 27 , 29 , 42 , 45 ] by egfr blockage in certain tumor types . 
 [ 40 ] : inhibition of tumor cell proliferation , tumor angiogenesis and radiation - induced damage repair , induction of cell cycle arrest , promotion of radiation - induced apoptosis , and probably effects on invasion and metastasis . 
 in this study , clonogenic cell survival , cell cycle distribution , proliferation , apoptosis as well as egfr and tgfexpression were examined in order to determine which of these parameters might explain or predict the effects of zd1839 treatment on radiosensitivity of tumor cell lines . material and methods culture of tumor cell lines two human nsclc tumor cell lines , a549 and h596 ( adenosquamous carcinoma ) , were obtained from atcc and one human scchn cell line , fadu , was a kind gift from m . 
a549 cells were cultured in f12k medium containing 1.5 g / l sodium bicarbonate , 10% fetal bovine serum ( fbs ) , and 1% penicillin / streptomych596 cells were cultured in rpmi 1640 medium with 2 mm l - glutamine containing 1.5 g / l sodium bicarbonate , 10 mm hepes , 1 mm sodium pyruvate , 10% fbs , and 1% penicillin / streptomyc fadu cells were cultured in dmem with stabilized glutamine containing 1 mm sodium pyruvate , 10% fbs , and 1% penicillin / streptomyc all cell culture reagents were purchased from biochrom seromed and sigma aldrich , plastic ware was obtained from nunc and greiner . 
zd1839 and radiation in tumor cell lines survival fraction cells were grown to confluence and treated with 0 , 1 , and 5 m zd1839 for 16 h before irradiation using a 6 - mev linear accelerator with doses from 1 to 6 gy . 
after an incubation time of 1014 days ( depending on different doubling times of the cell lines ) at 37 c , 5% co2 culture dishes were stained with 0.1% crystal violet in 70% ethanol and counted for colony formation . 
cells were fixed in 70% ethanol for at least 30 min on ice , stained with propidium iodide ( pi ) / triton x - 100 staining solution with rnase a and analyzed by flow cytometry ( facscan / cell quest software , becton dickinson ) for dna content . 
 detection of apoptosis apoptosis was detected and quantified as a sub - g1 fraction in flow - cytometric analyses of pi / triton x - 100 / rnase a - stained cells . 
for confirmation of these results , annexin v / 7 - amino - actinomycin d ( 7 - aad ) staining ( annexin v - pe apoptosis detection kit i , bd pharmingen ) was performed in parallel for selected samples . 
cells positive only for annexin v were quantified as early apoptotic cells , whereas cells with positive staining for both annexin v and 7 - aad were classified as late apoptotic or necrotic cells . 
supernatant and trypsinized cells were combined before staining , because apoptotic cells detach early from the surface of culture flasks [ 11 ]  . egfr and tgfexpression level in a real - time two - step rt - pcr cells were harvested and rna extraction was performed with the rneasy mini kit ( qiagen )  . 
egfr , tgfand porphobilinogen desaminase ( pbgd ) expression was measured by real - time two - step reverse transcription - polymerase chain reaction ( rt - pcr ) with the lightcycler instrument ( roche ) using the quantitect sybr green pcr kit ( qiagen ) and sequence - specific oligonucleotides ( roth , operon , invitrogen ) as primers : egfr - 1 forward 5gccgacagctatgagatgg - 3 , egfr - 3 reverse 5 cccctaaatgccaccggc - 3 ( modified from [ 33 ] ) , tgf forward 5 - gctctgggtattgtgttgg - 3 , tgf reverse 5 - cagaatggcagacacatgc - 3 , pbgd - 1 forward 5 - ggagccatgtctggtaacg - 3 , pbgd - 2 reverse 5 - gaatcttgtcccctgtggt - 3 . 
the following protocol was used for the pcr : activation of the polymerase at 95 c for 900 s and 45 cycles of amplification at 95 c for 15 s ( denaturation ) , 58 c for 30 s ( annealing ) , 72 c for 10 s ( elongation ) with acquisition of fluorescence at the end of each elongation step . 
a melting curve was generated by heating to 95 c for 0 s , cooling to 65 c for 15 s , and heating at 0.1 c / s to 95 c under continuous acquisition of fluorescence . 
for a549 and h596 cells radiosensitivity was found to be in a similar range , whereas fadu cells were more radiosensitive than the other two cell lines ( figure 1a )  . 
 the effect of 1 m or 5 m zd1839 on the plating efficiency of these cell lines is shown in figure 1b : whereas in a549 and h596 cells the plating efficiency was not drastically altered after treatment with zd1839 , the plating efficiency of fadu cells treated with 1 m zd1839 was reduced by a factor of 30 compared to controls and even lower values were obtained for fadu cells treated with 5 m zd1839 . 
in a549 cells survival was slightly lower after irradiation in combination with 1 m zd1839 compared to irradiation only , but only at a higher concentration of 5 m a significant radiosensitizing effect was seen . 
 fadu cells treated with zd1839 and radiation revealed even a drug dose - dependent decrease of radiosensitivity , implying that the few percent of cells surviving zd1839 treatment were even more radioresistant . 
compared to the results in the other two cell lines zd1839 and irradiation were still most effective in fadu cells , albeit with a less than additive effect of these treatment modalities . cell cycle distribution after treatment with zd1839 and irradiation to determine the underlying mechanisms of the different effects of zd1839 on clonogenic survival in a549 , h596 , and fadu tumor cell lines , the impact of irradiation at three different doses ( 2 , 4 , and 8 gy ) , treatment with 1 m zd1839 and combined treatment of 1 m zd1839 and irradiation with 2 , 4 , and 8 gy was studied on cell cycle distribution at 24 h , 48 h , and 72 h after irradiation in all three cell lines . 
 induction of apoptosis whereas no significant increase in cells containing a lower amount of dna than g1 cells ( sub - g1 fraction ) occurred in a549 and h596 cells upon treatment with zd1839 and irradiation , in fadu cells there was a considerable increase in this subpopulation 48 h after irradiation in combination with 1 m zd1839 with a further increase 72 h after irradiation ( figure 2 )  . 
in order to confirm that apoptosis contributes to the occurrence of this subpopulation of cells , fadu cells treated with 1 m zd1839 and irradiation of 4 gy were stained with annexin v / 7 - aad 48 h and 72 h after irradiation and analyzed by flow cytometry ( figure 3 )  . 
48 h after irradiation only a small increase of 4.4% in early apoptotic cells ( annexin v - positive / 7 - aad - negative ) and 1.2% in late apoptotic / necrotic cells ( annexin v - positive / 7 - aad - positive ) was detected compared to untreated cells . 
the total amount of early apoptotic and late apoptotic / necrotic fadu cells detected with this approach ( 18.8% after 48 h and 43.9% after 72 h ) was similar to the level of sub - g1 cells determined by pi staining ( figure 2 )  . 
 in the squamous cell carcinoma cell line fadu , the percentage of sub - g1 cells increased dramatically between 24 h and 72 h following combined treatment and to a lesser extent after single treatment with zd1839 or radiation ( figure 2 )  . 
 the presence of a considerable fraction of s - phase cells at all time points after irradiation alone indicates that no radiation - induced g1 arrest occurs in this cell line . 
 the only significant finding in a549 and h596 cells was an early cell cycle arrest at the g2 / m - checkpoint following irraegfr and tgfmrna expression the expression of egfr mrna and tgfmrna was determined by real - time rt - pcr in untreated cells as well as 1 h , 6 h , and 24 h after irradiation with 4 gy in the three cell lines fadu , a549 , and h596 ( figure 4 )  . 
egfr mrna expression was also determined 16 h after treatment with zd1839 in these cell lines , as at this time point cells were exposed to radiation in the colony assays and the cell cycle distribution / apoptosis experiments described earlier in this study . in untreated fadu cells the expression of egfr mrna exceeded the expression level of the housekeeping gene pbgd about 8.5 - fold , whereas in a549 and h596 cells the expression of egfr was in the same range as pbgd mrna expression in untreated samples . 
while egfr mrna expression was downregulated in a549 cells after 16 h exposure to zd1839 , a moderate upregulation was observed in h596 and fadu cells strahlenther onkol 2005 no . 
24 h after irradiation egfr mrna expression was restored to the level of untreated samples in a549 cells , whereas it was still suppressed in fadu cells and exceeded the level of untreated samples in h596 cells . 
in a549 and fadu cells , tgfmrna was upregulated 6 h after irradiation with 4 gy and had returned to basal expression levels after 24 h , whereas no radiation - induced changes occurred in h596 cells ( figure 4c )  . 
several biological characteristics investigated in the three tumor cell lines ( a549 , h596 , fadu ) seem to be related to the response to treatment with the egfr tyrosine kinase inhibitor zd1839 ( iressa ) and combination with irradiation . 
although the initial expression levels of egfr and tgfseem to be crucial to the outcome of zd1839 treatment , this is questioned at least in the case of nsclc cells by results of recent studies [ 4 , 43 ]  . 
remarkably , this g1 arrest has to be mediated through mechanisms independent of tp53 and could accordingly not be detected after irradiation of fadu cells , as tp53 is mutated in fadu cells [ 21 , 28 , 30 ]  . 
recently , a role for p27 and p21 as well as cyclin dependent kinase 2 ( cdk2 ) , cdk4 , cdk6 , cyclin d1 , cyclin d3 , and rb2 / p130 in the zd1839 - induced g1 arrest has been suggested figure 2 . 
cell cycle distribution of fadu cells after treatment with 1 m zd1839 , irradiation with 2 , 4 , and 8 gy , and combination of irradiation and treatment with zd1839 in comparison to untreated control cells ( c )  . 
zellzyklusverteilung von fadu - zellen nach behandlung mit 1 m zd1839 , bestrahlung mit 2 , 4 und 8 gy sowie kombination von bestrahlung und zd1839 verglichen mit unbehandelten kontrollen ( c )  . 
 for the combination of zd1839 and radiation , we have not only to consider egfr / tgfexpression levels in untreated tumor cells but the effects of irradiation and treatment with zd1839 on the expression levels of egfr and tgf -  . 
a considerable downregulation of egfr mrna expression in a549 cells was found after 16 h of treatment with zd1839 which should contribute to a radiosensitizing effect [ 6 ] that was also demonstrated in this study . 
cells negative for both annexin v and 7 - aad were alive ( lower left quadrant ) , cells positive only for annexin v were early apoptotic cells ( upper left quadrant ) , and cells positive for both annexin v and 7 - aad were late apoptotic / necrotic cells ( upper right quadrant )  . 
lebende zellen sind annexin - vund 7 - aad - negativ ( unterer linker quadrant ) , annexin - v - positive / 7 - aad - negative zellen sind frhapoptotisch ( oberer linker quadrant ) , und zellen , die sowohl fr annexin v als auch fr 7 - aad positiv anfrben , sind sptapoptotisch / nekrotisch ( oberer rechter quadrant )  . 
after 24 h the expression level of untreated cells was restored in a549 cells and was exceeded in h596 cells , whereas mrna levels in fadu cells were still lower than prior to irradiation . 
this study was supported by a grant from astrazeneca , wedel , germany . cancer 2003 ; 41 : 238 . levels were extremely low in a549 and h596 cells , this effect presumably has only biological relevance for fadu cells , where an early upregulation of tgfmrna expression may counteract to some extent the effect of downregulation of egfr expression upon irradiation . it has already been shown by dent et al . 
that ionizing radiation can induce activation of the egfr / ras / raf / mapk pathway through the release of tgf and activation of the egfr tyrosine kinase [ 12 , 41 ]  . 
thus , it must be assumed that modulation of the total cellular amount of egfr and tgfby irradiation or drug treatment influences the extent of these effects and plays a role in modulation of radiosensitivity . 
 strahlentherapie und onkologie original article neutron activation of patients following boron neutron capture therapy of brain tumors at the high flux reactor ( hfr ) petten ( eortc trials 11961 and 11011 ) andrea wittig1 , raymond l . 
moss2 , finn stecher - rasmussen3 , 4 , klaas appelman4 , jrgen rassow1 , antoanetta roca2 , wolfgang sauerwein1 background and purpose : at the high flux reactor ( hfr ) , petten , the netherlands , eortc clinical trials of boron neutron capture therapy ( bnct ) have been in progress since 1997 . 
the importance of this induced activity with respect to the absorbed dose in the patient as well as to the radiation exposure of the staff has been investigated . material and methods : as a standard radiation protection procedure , the ambient dose equivalent rate was measured on all patients following bnct using a dose ratemeter . 
furthermore , some of the patients underwent measurements using a - ray spectrometer to identify which elements and confirm which isotopes are activated . results : peak levels , i.e. , at contact and directly after irradiation , are of the order of 4060 sv / h , falling to < 10 sv / h 3050 min after treatment . 
the ambient dose equivalent rate in 2 m distance from the patients head at the earliest time of leaving the reactor center ( 20 min after the end of treatment ) is far less than 1 sv / h . 
the initial activity is predominantly due to 49ca , whilst the remaining activity is predominantly due to 24na . conclusion : the absorbed dose resulting from the activated isotopes in the irradiated volume is in the order of < 1% of the prescribed dose and therefore does not add a significant contribution to the absorbed dose in the target volume . 
the levels of radiation received by staff members and non - radiation workers ( i.e. , accompanying persons ) are well below the recommended limits . key words : boron neutron capture therapy ( bnct ) activation radiation protection - ray spectrometry strahlenther onkol 2005 ; 181 : 77482 doi 10.1007 / s00066 - 005 - 1433 - 4 gewebeaktivierung bei patienten nach bor - neutroneneinfangtherapie von hirntumoren am hochflussreaktor ( hfr ) in petten im rahmen der eortc - studien 11961 und 11011 hintergrund und ziel : am hochflussreaktor ( hfr ) der europischen kommission in petten , niederlande , werden seit 1997 klinische studien zur bor - neutroneneinfangtherapie ( bnct ) durchgefhrt . 
den strahlenschutz der umgebung zu erfassen . material und methodik : im rahmen von standardprozeduren wurde bei allen patienten nach der bestrahlung die ortsdosisleistung im kontakt und in 30 cm abstand gemessen . 
zustzlich wurde bei einigen patienten mit einem - spektrometer untersucht , welche isotope aktiviert wurden . 1 strahlenklinik , university hospital essen , germany , 2 institute for energy , joint research center , petten , the netherlands , 3 nct physics , alkmaar , the netherlands , 4 nuclear research and consultancy group ( nrg ) , petten , the netherlands . 
 schlsselwrter : bor - neutroneneinfangtherapie aktivierung strahlenschutz - spektrometrie introduction eortc clinical trials on boron neutron capture therapy ( bnct ) are being performed under the medical responsibility of the university hospital essen , germany , at the high flux reactor ( hfr ) of the european commission at petten , the netherlands [ 19 ]  . 
 the beam itself contains neutrons of several energies up to a few mev , but in most cases predominantly epithermal neutrons , i.e. , in the energy range 1 ev to 10 kev [ 12 ]  . 
the principle of bnct relies on the underlying requirement that with a higher concentration of 10b atoms in the tumor , in comparison to healthy tissue , neutron capture in the 10b atoms gives an effective lethal radiation dose to the tumor cells , whilst sparing the cells of the healthy tissue [ 18 ]  . treatment with bnct , as also with fast neutron radiotherapy [ 1 ] , results in neutron capture in some of the isotopes of elements that are naturally present in tissues . 
consequently , following bnct ( and fast neutron treatment ) , the patient is radioactive and as such , dedicated radiation protection measures need to be taken [ 13 ]  . 
this aspect can normally be neglected after conventional irradiation involving treatment with photons or electrons . the first european clinical trial on bnct , a phase i trial ( eortc protocol 11961 ) for patients suffering from glioblastoma multiforme , started at petten in october 1997 [ 6 , 7 , 20 ]  . 
a second trial , a phase ii trial ( eortc protocol 11011 ) for patients with melanoma metastases , was started more recently in july 2004 [ 21 ]  . 
the treatment of a patient and the potential exposure of personnel to ionizing radiation require by the dutch nuclear energy law ( besluit stralingsbescherming , 2002 ) that the joint research centre of the european commission ( jrc ) ( as licence holder of the hfr ) must ensure that radiologic protection and monitoring of all personnel , including external staff , but also the patient are provided and that the correct radiation protection measures are taken and followed . 
 due to the organizational structure of these european trials , where the treatment takes place at a facility in the netherlands under the responsibility of clinicians from germany , some radiation protection aspects have to satisfy both german and dutch radiation protection laws . 
 a contractual agreement had to be signed between the german institute ( university of essen ) and jrc petten to guarantee that procedures to be followed comply with german radiation protection regulations ( 15 strahlenschutzverordnung , 2001 ) , as well as regulations under the dutch nuclear energy law ( article 66 in the besluit stralingsbescherming , 2002 )  . 
in fact , the radiation measurements of the patient and subsequent reporting , for example to the local radiation protection committee , form part of the overall quality assurance system related to bnct [ 14 ] , which includes : thoroughly and regularly characterizing the beam , using dosimetry techniques in addition to those of conventional radiotherapy ; modeling the complex dose distribution in the patient using treatment planning codes based on programs developed for nuclear applications [ 16 ] , and developing in vivo boron distribution measurement techniques using on - line prompt - ray spectroscopy [ 24 ]  . a summary of all measurements taken on the patients for radiation protection purposes after the treatment is presented here , in order to evaluate the impact of the patients activation on the absorbed dose in the patient and on the radiation exposure of the personnel . 
lagerung eines patienten zur bnct am hfr . to return to the hospital in amsterdam ( between 30 min and 2 h post - bnct ) , where the patient is hospitalized during the week of treatment . 
in eortc trial 11961 ( bnct treatment of glioblastoma multiforme , with bsh ) [ 6 , 7 , 20 ] , each patient received four fractions ( apart from the very first patient in whom , due to complications , the treatment had to be completed on the 3rd day giving an increased dose at the third fraction )  . 
in addition , mainly driven from a scientific perspective , the spectrum of the emitted radiation has been investigated by - ray spectroscopy in order to identify the isotopes activated during treatment . 
the first measurement is taken 12 min directly following each beam of radiation , the second when the patient leaves the reactor building ( 510 min post - bnct ) , and the third just prior to the patient leaving the reactor site in petten figure 3 . 
all dose rate values are given in sv / h , numbers 1 , 2 , and 3 refer to the measurements taken immediately after irradiation , on leaving the controlled area and on leaving the reactor site , respectively . 
die zahlen 1 , 2 und 3 im tabellenkopf verweisen auf den zeitpunkt und ort der messung : direkt im anschluss an die bestrahlung im bestrahlungsraum , beim verlassen des kontrollbereichs und beim verlassen des reaktors . 
activation of patients following bnct activation measurements using a portable - ray analyzer the use of the dose ratemeter to measure the overall radioactivity of the patients head , is adequate for radiation protecfigure 4 . 
gemessene umgebungsquivalentdosisleistung an der oberflche des patienten in einer der eintrittsfeldpforten in abhngigkeit von der zeit . tion purposes , as well as with respect to the patient and to the environment . 
hence , from the scientific perspective , it is of interest to determine and observe which radioisotopes are present and which give the most significant contribution to the total absorbed dose to the patient over time . measurements were performed on five patients using a portable - ray spectrometer . 
 results radiation protection measurements measurements of the ambient dose equivalent rate in contact with the irradiated head at the beam entrance side of the last beam of each fraction are collated in table 1 . 
 this can be easily explained by an equilibrium of production and decay of the isotopes with very short half - life , which give the major contribution to the activity present immediately after the irradiation . 
the measurements taken at the end of the observation period at the reactor site , however , seem to be slightly higher in this group of patients as compared to the patients treated in trial 11961 , even if in individual patients similar values are observed . 
 discussion the absorbed dose given to the patient during bnct , not only depends on the dose due to the 10b reaction ( which produces a helium and lithium ion ) , but also due to the presence of h ( hydrogen ) and n ( nitrogen ) in tissue , which cause additional doses due to the neutron capture reactions 1h ( n , ) 2h and 14n ( n , p ) 14c [ 17 ] , the neutron absorbed dose due to recoil protons and the - radiation present in the incident bea however , in the tissue itself , other elements such as cl ( chlorine ) , ca ( calcium ) and na ( sodium ) , also undergo neutron capture producing radioactive isotopes that due to decay continue to be radioactive and thus give a continued absorbed dose to the patient , as well as the personnel ( medical staff , accompanying persons ) involved . 
 the main contribution to the total dose is assumed to be due to the more common radioactive isotopes 38cl , 49ca , and 24na [ 1 , 2 ]  . 
to some extent 18o and other minor isotopes contribute to the overall activity , though due to their relatively small abundance in tissue and their short half - lives , their contribution very soon after bnct is negligible . 
typisches - spektrum bei einem patienten nach bnct . channel number the exponential fit to the measured data , as shown in figure 6 , has the form : y = aebt where from regression analysis , a = 44.44 sv / h and b = 3.6 h1 ( if t , as in this case , is in hours )  . 
for simplicity , if this is compared with the decay term for a single radioisotope , then the exponential constant b is the disintegration constant , and equivalent to ln2 / t1 / 2 , which gives t1 / 2 = 11.55 m of the table 2 . 
data of radionuclides identified in the spectrum shown in figure 6 ( - ray lines [ 3 ] , energies of ( cid : 2 ) - particles [ 22 ] )  . 
radionuklide , die in dem in abbildung 6 dargestellten spektrum identifiziert wurden ( werte der - linien und energie der ( cid : 2 ) - teilchen sind zitiert nach [ 3 ] und [ 22 ] )  . 
this would therefore indicate that the initial activity is predominantly due to 49ca , which is due to the activation of calcium ( 17.6% mass ) in the cranium [ 9 ]  . 
 furthermore , the relatively longer half - life of 24na and the shorter half - life of 49ca would suggest that after about 1 h ( approximately six half - lives of 49ca ) , the activity is dominated by 38cl , with a low background stable contribution from 24na , which after a number of hours , as observed on the measurements taken on the next day , remains as the main radioactive isotope . 
under such circumstances , a nurse could do this 400 times per year prior to reach the threshold of 1 msv , which would make her a radiation worker of category b . 
the observed ambient dose equivalent rate in 2 m from our patients at the earliest time , when patients leave the reactor center ( 20 min after treatment end [ table 1 ] ) is far less than 1 sv / h . 
we can conclude that the accumulated doses due to patients activation are , for staff members , well within permissible levels with respect to radiation protection and well outside levels for a controlled area as long as only a few patients are treated by this method at one place . 
 with respect to the absorbed dose in patients , due to the induced activity of 24na , 38cl and 49ca in the target region , an estimation can be performed on the basis of the presented measured data by two methods , which are shown in detail in the appendix to this article . 
 the resulting value , 170 msv , for the maximum dose equivalent contribution by ( cid : 2 ) - particles is a very rough estimation of the upper limit for h ( cid : 1 ) max and overestimates it by a factor of up to 10 . 
the value corresponds approximately to 1% of the maximum total absorbed dose in the target volume of the patient and is within the uncertainty of the calculated patient - absorbed dose . 
in other parts of the patients body , where only some scattered neutrons are acting , the dose equivalent by induced activity is magnitudes smaller , this is in the same order of < 0.1% as was found by frost & michel [ 4 ] for ultrahard x - rays of the bbc 35 mv betatron . 
whilst radiation protection measurements involving patients are less restrictive than , for example , when handling radioactive material in the nuclear industry , it is nevertheless prudent to take cautious measures that protect the staff involved . 
one concerns radiation protection measures , which , as described above , involve a strict measurement campaign to systematically be aware of the levels of radiation that the patient emits . 
after about 30 min , levels decayed to half these values , which at 30 cm distance from the patient , being the equivalent distance at which staff are present , are < 10 sv / h . 
when comparing both trials , where in the second trial ( 11011 ) , the irradiation times are twice as long , the measured levels of radioactivity are the same . 
 from the results of the portable - ray spectrometry campaign , it could be concluded that initially , the activity is predominantly due to 49ca ( half - life = 8.72 min ) , coming from the activation of calcium in the cranium , whilst after approximately 1 h , the total activity is due to a combination of 38cl and 24na , and after a number of hours , the remaining activity is due to 24na only . the - ray spectrometry measurements were also able to detect such idiosyncrasies as the isotopes 198au and 116min , which are assumed to be due to the activation in some of the elements ( isotopes ) that make up the patients fillings . 
 finally , to reiterate , and with respect to radiation protection , the levels of radiation received by personnel and non - radiation workers ( spouse , drivers ) are well below the recommended limits [ 10 ]  . 
144 patients had sole ibt ( median dref = 56 gy ) , in 92 patients ibt procedures ( median dref = 24 gy ) were performed in combination with external irradiation . 
the analysis of tumor control , survival and treatment - related toxicity was performed after a median follow - up of 26 months ( 675 months )  . results : at the time of analysis permanent local tumor control was registered in 208 of 236 patients ( 88% )  . 
at 5 years overall survival and local recurrence - free survival of the entire group were 8273% and 9383% for t1 / 2 , and 56% and 83% for t3 / 4 , respectively . 
144 patienten erhielten eine alleinige ibt ( median dref = 56 gy ) , bei 92% wurde die brachytherapie ( median dref = 24 gy ) mit perkutaner strahlentherapie kombiniert . 
die analyse der tumorkontrolle , des berlebens und der nebenwirkungen wurde nach einem medianen beobachtungszeitraum von 26 monaten ( 675 monate ) durchgefhrt . ergebnisse : zur zeit der analyse wurde bei 208 von 236 patienten ( 88% ) eine dauerhafte lokale tumorkontrolle registriert . 
es wurden keine weiteren schwerwiegenden nebenwirkungen registriert . schlussfolgerung : die pdr - ibt mit 0 , 40 , 7 gy / h und einem intervall zwischen den pulsen von 1 h ist eine sichere und effektive behandlung . 
diese ergebnisse besttigen , dass die pdr - ibt bei hno - tumoren der low - dose - rate - ( ldr - ) brachytherapie vergleichbar ist gleich effektiv und weniger toxisch . schlsselwrter : pdr - brachytherapie hno - tumoren 1 department of radiation oncology , university erlangen - nuremberg , erlangen , germany , 2 department of otorhinolaryngology , head and neck surgery , university erlangen - nuremberg , erlangen , germany . received : february 8 , 2005 ; accepted : august 22 , 2005 strahlenther onkol 2005 no . 
pdr brachytherapy in head - and - neck cancer introduction interstitial brachytherapy ( ibt ) alone or as boost combined with external - beam therapy as definitive treatment modality or as postoperative therapy is indicated in the treatment of both primary and recurrent head - and - neck cancer . 
the results of low - dose - rate ( ldr ) brachytherapy with iridium - 192 ( 192ir ) wires using the rules of the paris system are considered , up to now , the gold standard in the therapy of preferably small head - and - neck tumors , particularly in comparison with high - dose - rate ( hdr ) brachytherapy results [ 20 , 21 , 25 , 27 , 28 , 41 ]  . 
pulsed - dose - rate ( pdr ) brachytherapy as a substitute for ldr brachytherapy is considered a useful option in the treatment of head - and - neck tumors , because here , the biological advantages of ldr brachytherapy meet with the technological advantages of the hdr afterloading method [ 21 , 26 , 35 , 39 ]  . 
 patient characteristics and distribution in regard to tumor sites and tumor stage ( table 1 ) show that the majority of the patients had tumors of the oral cavity ( 72% ) and that only a minority of our patients was treated with small tumors ( t1 = 38% )  . 
in addition , some unfavorable prognostic parameters were presented by a relevant number of our patients : tumor grade g3 in 20% ( 47 / 236 patients ) , lymph vessel invasion present ( l1 ) in 20% ( 47 / 236 patients ) and close or positive resection margins microscopic ( r1 ) or macroscopic ( r2 ) residual tumors were found in 11% ( 26 / 236 patients ) and 17% ( 41 / 236 patients ) , respectively , before we started ibt . 
as inclusion criteria for ibt after surgery we defined any tumor with a size between 2 and 45 cm without significant bone infiltration and all tumors sized < 2 cm ( t1 ) with infiltration depth of > 5 mm or with lymphangiosis ( l1 ) or grading 3 . 
 for dose specification and prescription the rules were used similar to the paris systethus , the dp of 0.40.7 gy corresponded to our reference dose ( dref ) , which was prescribed at 85% of the mean central dose . 
external - beam irradiation was performed up to a median reference dose of 51 gy ( range : 472 gy ) using a linear accelerator with 6 - mv photons . 
 tumor site type of surgery ( number of patients ) tumor biopsy resection only ( no only surgery ) lip floor of mouth oral tongue base of tongue tonsil soft palate others total 5 6 9 3 0 1 0 9 6 1 2 4 1 39 63 9 15 3 3 133 tumor resection and neck dissection tumor resection and lymph node sampling tumor resection with plastic reconstruction tumor resection with plastic reconstruction and neck dissection total tumor debulking only 0 9 6 1 0 1 1 7 67 25 19 6 9 236 table 2b . 
r0 : clear resection margins ; r1 : microscopically positive resection margins ; r2 : macroscopically positive resection margins ( no surgery ) ; rx : resection margins not known . 
 tumor site r - state total lip floor of mouth oral tongue base of tongue tonsil soft palate others total 2 54 75 11 12 6 6 166 1 6 9 4 4 0 2 3 6 9 3 0 1 7 67 25 19 6 9 tumor site and comprehensive regional lymph nodes , generally using opposed lateral field matched to an anteroposterior supraclavicular field . 
most local recurrences developed in the first 18 months after therapy with a plateau apparent after 20 months ( figure 1b ) , the mean time to local recurrence was 9.2 months ( median 9.5 months , 234 months )  . the 5 - year overall survival rates of the entire group according to tumor size and lymph node metastases were : 90.8% for t1 n0 , 81.5% for t1 n + , 72.7% for t2 n0 , 44.1% for t2 n + , 62.8% for t3 / 4 n0 , and 56.3% for t3 / 4 n +  . 
the differences in patients with oropharynx cancer without or with lymph node metastases were also without any statistical significance and , in our opinion , were only due to the small number of patients in these subgroups . 
in the detailed analysis of subsets of each tumor localization we observed that in oropharynx cancer , the best results were achieved by tonsil cancer and the worst by base of tongue cancer patients ( figure 3 ) , again without significant differences . 
 serious late side effects ( table 4 ) such as soft - tissue necrosis and bone necrosis were observed in 23 / 236 ( 9.7% ) strahlenther onkol 2005 no . 
 discussion radiobiological studies showed , that pdr brachytherapy is probably equivalent to ldr brachytherapy models [ 1 , 5 , 7 , 10 , 12 , 13 , 17 , 19 , 24 , 29 , 32 , 42 ]  . 
 unfortunately , for head - and - neck cancer only limited experiences with pdr brachytherapy have been presented up to now mostly only feasibility studies with limited patient numbers [ 6 , 11 , 18 , 21 , 26 , 43 ]  . 
the french experiences with pdr brachytherapy in 30 head - and - neck cancer patients [ 26 ] only showed , that pdr brachytherapy is feasible and that 14 / 28 patients had short or definitive breakdown of therapy due to different problems . 
 [ 18 ] treated 38 patients with head - and - neck cancer with pdr brachytherapy ( dp = 2 gy , four to eight times / day ) alone or in combination with external irradiation . 
local control rates are , depending on tumor size , between 78% and 92% for t1 / 2 tumors and 57% for t3 / 4 tumors in the largest study so far [ 16 ] and between 93% and 70% in studies with smaller patient numbers [ 2 , 4 ]  . 
our results suggest , that pdr brachytherapy is most probably safer and equally effective compared to ldr brachytherapy . strahlentherapie und onkologie original article dose delivery accuracy of therapeutic photon and electron beams at low monitor unit settings manickam ravikumar , mohammed a . 
knowledge of this study is required for few dosimetric applications and to know the dose delivered to the patient when the treatment is delivered with few monitor units ( mu )  . 
 material and methods : dose measurements were carried out for photon and electron beams with 0.6 cm3 ptw ion chamber in white polystyrene phantom at dmax with a field size of 10 10 cm2 at 100 cm fsd . 
 results : significant deviation ( + 20% to + 25% ) in dose delivery was noticed for photon and electron beams ( + 39% to + 45% ) at lmu settings . 
 key words : low monitor units output factors dose delivery imrt strahlenther onkol 2005 ; 181 : 7969 doi 10.1007 / s00066 - 005 - 1412 - 9 genauigkeit der dosierung therapeutischer photonenund elektronenstrahlung bei niederen monitoreinheiten ziel : fr photonenund elektronenstrahlung wurde die abhngigkeit der output - faktoren von den monitoreinheiten gemessen . 
 relevant sind die ergebnisse dieser untersuchung fr einige dosimetrische anwendungen und zur ermittlung der referenzdosis , wenn mit wenigen monitorwerten ( mu ) bestrahlt wird . material und methode : die output - faktoren wurden mit einer 0 , 6 - cm3 - ionisationskammer , ptw , jeweils in maximumstiefe mit einem weien polystyrol - phantom ermittelt ( feldgre 10 10 cm2 , fokus - oberflchen - abstand 100 cm )  . 
 schlsselwrter : niedere monitorwerte output - faktoren applizierte dosis imrt introduction dose estimation uncertainty of 2% is necessary to deliver a uniform target dose within 5% for better tumor control [ 6 , 7 , 10 , 12 , 21 , 26 , 27 , 30 ]  . 
dosimetric studies involving tld phosphors for radiation protection , film dosimetry at low level of radiation dose , nuclear medicine dosimetry , estimation of low ( cid : 1 ) - doses and few other research applications related to environmental dosimetry require few monitor unit ( mu ) settings of photon and electron beams in a linear accelerator . 
the conformal therapy makes use of multiple multileaf collimated ( mlc ) beams of varying 1 oncology center , king abdul aziz hospital and oncology center , jeddah , saudi arabia . 
 sometimes the number of mu per field might vary as low as 10 mu depending on the location of the target and the neighboring normal structures [ 1 , 8 , 17 , 18 , 25 ]  . 
with intensity - modulated radiotherapy ( imrt ) technique , each individual field is divided into small beamlets and the weight of each beamlet can be adjusted by varying the number of mu delivered [ 2 , 11 , 20 , 28 , 29 ]  . 
 also , possibility of the treatment machine internal interlock terminating the treatment is common after delivering few mu when the dose rate does not build up to the specified set level . 
 these situations require the knowledge of accuracy in dose delivery at low monitor unit ( lmu ) settings for photon and electron beams in order to estimate the delivered dose . 
 material and methods the delivered dose per mu at different mu settings was evaluated from the charge measured using a 0.6 cm3 farmer type ion chamber ( ptw , type 30001 ) connected to a ptw unidos e digital electrometer . 
the chamber was positioned with its effective point of measurement , which is the center of the chamber for photon beams and 0.5r upstream from the center toward the source for electron beams , at the depth of maximum in a 30 30 30 cm3 water - equivalent rw3 slab phantom ( ptw t29672 )  . 
the depth of maximum dose was determined in a water phantom using wp 600 wellhofer radiation field analyzer ( rfa ) system and 0.14 cm3 ( wellhofer ) sensitive volume ionization chamber . 
the linearity of the 0.6 cm3 chamber and an electrometer system to measure the low level of charge was checked using a strontium - 90 check source ( ptw type 23261 - 935 ) of 25 - mbq activity . 
the consistency in the measured charge / s over a range of measuring time ( 1150 s ) indicates that the measuring system is sensitive and linear for the measurement of low charge levels . 
 the absorbed dose to the medium was estimated using technical report series 398 [ 10 ] of iaea ( trs - 398 ) and is given by d / mu = ( mq / mu ) nd , w , qo kq , qo ( 1 ) , where d / mu is the dose to the medium per mu at the beam quality q , mq is the corrected charge per mu for influencing quantities , nd , w , qo is the calibration factor in terms of absorbed dose to water for the dosimeter at the reference quality qo , and kq , qo is a chamber - specific factor which corrects for the difference between the reference beam quality qo and the actual beam quality of measurement q . 
 the relative dose ( rd ) is defined as the ratio of dose delivered per mu at the testing condition to that of the dose delivered per mu at the normal calibration condition , usually with 200 - mu setting . 
 since the ionization chamber and the beam quality are same in the above measurement conditions , nd , w , qo and kq , qo are constant in equation ( 2 )  . 
as the variation in energy for the scattering foil - produced electron beam is within + 2% [ 3 ] , same values of kq , qo were considered for the testing and calibrating mu . 
 hence equation ( 2 ) can be written as rd = ( mr / mu ) test / ( mr / mu ) cal ( 3 ) , where ( mr / mu ) test and ( mr / mu ) cal are the dosimeter readings per mu for photon and electron beams under testing and calibrating conditions . 
 results the rd / mu for different mu settings for 6and 18 - mv photons from mevatron 6700 and mevatron kds for the dose rate of 300 mu / min is shown in figure 1 . 
variation of relative dose ( rd ) for a 10 10 cm2 field at 100 cm fsd for 6 ( mevatron 6700 ) and 18 - mv ( mevatron kds ) photons at different monitor unit settings with a dose rate of 300 mu / m abbildung 1 . 
vernderung der relativen dosis ( rd ) in einem 10 10 cm2 feld bei 100 cm fokus - oberflchen - abstand fr 6 - ( mevatron 6700 ) und 18 - mv - ( mevatron kds ) - photonen bei verschiedenen monitoreinheiten mit 300 mu / min dosisrate . 
vernderung der relativen dosis ( rd ) in einem 10 10 cm2 kegel bei 100 cm fokus - oberflchen - abstand fr 6 - , 8 - , 10 - , 12 - , 15und 18 - mev - elektronenstrahlen bei verschiedenen monitoreinheiten mit 300 mu / min dosisrate . 
variation of relative dose ( rd ) for 10 10 cm2 cone at 100 cm fsd for 10 - mev electrons beam with cylindrical chamber and parallel plate chambers at different monitor unit settings with a dose rate of 300 mu / m abbildung 4 . 
vernderung der relativen dosis ( rd ) in einem 10 10 cm2 kegel bei 100 cm fokus - oberflchen - abstand fr 10 - mev - elektronenstrahlen mit zylindrischer kammer und parallelplatten - kammern bei verschiedenen monitoreinheiten mit 300 mu / min dosisrate . 
 rd is significantly high ( + 25% for 6 mv and + 20% for 18 mv ) at the lowest possible mu setting ( 1 mu ) for both energies . 
at 300 mu / min dose rate ( mevatron 6700 ) the inaccuracy is + 25% as compared to + 17% for 200 mu / min ( mevatron kds ) at the lowest possible mu setting ( figure 2 )  . 
it can be noticed that the dose delivery inaccuracy is maximum for all the electron energies at the lowest possible mu setting ( 1 mu ) and the inaccuracy is present up to about 30 - mu setting . 
the variation in rd at different mu settings with 0.6 cm3 cylindrical ionization chamber for 10 - mev electrons was found to be consistent with the measurements carried out using parallel plate ionization chamber ( figure 4 ) , confirming the presence of inaccuracy in dose delivery at lmu settings . 
dose delivery accuracy at lmu settings discussion and conclusion usually , the absolute dose estimation is carried out with high mu ( about 200 mu ) set in the accelerator both for photon and electron beams . 
the discrepancy in dose delivery is found to be slightly higher for low - energy photons ( 6 mv ) compared to high - energy photons ( 18 mv ) at 300 - mu / min settings as against the higher deviation reported for 18 - mv photons compared to 6 - mv photons [ 23 ]  . 
the reasons for the difference in variation in dose delivery noticed are mainly due to the change in design and the difference in start - up behavior of the linacs . 
though it was reported that the variation in dose delivery is energy - dependent [ 3 ] , no definite conclusion of such variation is observed in our study for electron beams . 
 strahlentherapie und onkologie current discussion restricted - expressed proliferation - associated protein ( repp86 ) expression in squamous cell carcinoma of the oral cavity matthias fenner1 , falk wehrhan1 , 2 , marc jehle1 , kerstin amann3 , martin radespiel - trger4 , gerhard grabenbauer5 , johannes zenk6 , emeka nkenke1 , martin schinhammer1 , stefan schultze - mosgau1 , 2 purpose : to determine the expression of repp86 ( restricted - expressed protein of 86 kda theoretical molecular mass ) , a proliferation - associated protein expressed in s - , g2and m - phases of the cell cycle , in samples of normal mucosa as well as squamous cell carcinoma of the oral cavity ( oscc )  . patients and methods : the repp86 labeling index ( li ) was determined imunohistochemically in ten samples of normal oral mucosa and 59 samples of oscc . 
repp86 li was correlated with tumor stage , histopathologic grading , and the expression of ki - 67 and topoisomerase ii . results : repp86 was detectable in all tissues analyzed . 
 key words : oral squamous cell carcinoma repp86 proliferation strahlenther onkol 2005 ; 181 : 75561 doi 10.1007 / s00066 - 005 - 1430 - 7 repp86 - expression beim plattenepithelkarzinom der mundhhle ziel : erfassung der expression von repp86 ( restricted - expressed proliferation - associated protein ) , eines in den zyklusphasen s , g2 und m exprimierten , proliferationsassoziierten proteins , bei normalschleimhaut und plattenepithelkarzinomen der mundhhpatienten und methodik : im rahmen dieser retrospektiven untersuchung wurde formalinfixiertes histopathologisches routinematerial von 59 patienten mit plattenepithelkarzinomen der mundhhle sowie zehn proben unvernderter normaler mundschleimhaut untersucht . 
 schlsselwrter : plattenepithelkarzinom der mundhhle repp86 proliferation 1 department of oral and maxillofacial surgery , university of erlangen - nuremberg , erlangen , germany , 2 department of maxillofacial surgery / plastic surgery , university of jena , germany , 3 department of pathology , university of erlangen - nuremberg , erlangen , germany , 4 population - based cancer registry bavaria , registration office , university of erlangen - nuremberg , erlangen , germany , 5 department of radiation oncology , university of erlangen - nuremberg , erlangen , germany , 6 department of otolaryngology / head and neck surgery , university of erlangen - nuremberg , erlangen , germany . received : february 22 , 2005 ; accepted : august 1 , 2005 strahlenther onkol 2005 no . 
repp expression in oral squamous cell carcinoma introduction squamous cell carcinomas of the oral cavity ( oscc ) constitute a major proportion of head - and - neck cancers with 10 , 846 new cases diagnosed in the federal republic of germany in 1998 [ 9 , 17 , 21 ]  . 
the most common immunohistochemical marker used to study cell proliferation is the ki - 67 antigen , which describes the global growth fraction , defined as the cell population in g1 - , s - , g2 - , and m - phases of the cell cycle [ 6 ]  . 
the inevitable inclusion of g1 - phase cells with uncertain destinies might account for the limited utility of proliferation markers such as ki - 67 and topoisomerase ii [ 14 , 15 , 19 , 31 ]  . 
the g1 - phase cells may resume cycling but may remain in g1 for an indeterminate period of time , or they may definitely leave the cell cycle to become quiescent or succumb by apoptosis . 
however , once cells have crossed the restriction point and become engaged in dna replication , they are determined to complete a division cycle because cell cycle progression depends on an intrinsic program that is largely refractory to external influences [ 13 , 19 ]  . in 1997 , heidebrecht et al . 
reported a hitherto unknown proliferation - associated protein , which later was defined as repp86 ( i.e. , restrictedly expressed proliferation - associated protein ) [ 13 ]  . in mammals , repp86 expression was shown to be cell cycle - regulated , with a diffuse nuclear distribution becoming apparent at the onset of s - phase , persisting through g2 - phase , relocating to the mitotic spindle in m - phase , and vanishing with the completion of cytokinesis [ 19 ]  . 
in immunohistochemical analyses of normal tissues and different tumor entities , the labeling index ( li ) was only about 40% of the ki - 67 - positive cell fraction . 
as repp86 is expressed exclusively in cell cycle phases s , g2 , and m , it reflects the biologically relevant fraction of proliferating cells more accurately [ 17 , 19 , 22 , 24 ]  . in this study , we evaluate the expression of repp86 in normal oral mucosa as well as in samples of oscc . 
the expression is analyzed quantitatively in relation to tumor stage , histopathologic grading as well as to the expression of ki - 67 and topoisomerase ii . patients and methods tissue samples after approval by the ethics committee of friedrich alexander university erlangen - nuremberg , germany ( ethics approval 2430 ) , tissue samples were obtained from ten healthy subjects during routine elective surgical procedures . 
the specimens were fixed in 10% buffered formalin and embedded in paraffall subjects had signed informed consent a minimum 24 h before surgery . paraffin - embedded tumor samples of patients with oscc were retrieved from the department of pathology of friedrich alexander university erlangen - nuremberg . 
for statistical analysis , age , sex , tumor size , regional lymph node metastasis , and histopathologic grading according to uicc criteria were documented by the cancer center of friedrich alexander university erlangen - nuremberg . patient selection was performed according to an in - / exclusion protocol . 
the inclusion criteria were : primary oscc diagnosed between january 1 , 1996 and december 31 , 1999 , therapy with a curative intent , tumor resection ( r0 ) , and pre or postoperative radiotherapy / radiochemotherapy . 
according to the tnm classification , three tumors ( 5% ) were characterized as t1 , 24 tumors ( 41% ) were t2 , three tumors ( 5% ) t3 , 27 tumors t4 ( 46% ) , and information was missing for two tumors ( 3% )  . 
in 20 patients ( 34% ) a lymph node invasion could not be detected , 13 patients ( 22% ) were diagnosed n1 , and 22 patients were diagnosed n2 ( 37% )  . 
information on lymph node invasion was missing in four patients ( 7% )  . immunohistochemical analyses expression of the mitotic spindle - associated protein repp86 was analyzed immunohistochemically with the monoclonal antibody ki - s2 . 
briefly , 35 m thick sections were cut from formalin - fixed , paraffin - embedded tumor specimens , mounted on sialanized slides , and dried overnight at 37 c . 
immunoreactivity was restored by incubation of the slides with target retrieval solution at 100 c in a water bath for 30 min ( s1700 , dako , glostrup , denmark )  . 
to prevent nonspecific binding of the secondary antibody and the abcomplex with the tissue section , the slides were subsequently incubated with avidin and biotin solutions for 15 min each ( x0590 , dako ) as well as with rabbit serum for 30 min ( x0902 , dako )  . for qualitative and quantitative analysis of repp86 expression , the avidin - biotin peroxidase complex ( abc - pox ) method was used . 
the secondary antibody consisted of a polyclonal , biotinylated rabbitanti - mouse antibody ( e0464 , dako , dilution 1 : 50 in tbs , 30 min , room temperature )  . 
to provide subsequent chromogenic assay , incubation was carried out with avidin - biotin / horseraddish - peroxidase complex for 30 min ( streptabcomplex / hrp , k0377 , dako )  . 
for ki - 67 immunostaining , we used the antibody ki - s5 , a monoclonal mouse igg ( dilution 1 : 100 in tbs , department of pathology and hematopathology , university of kiel , germany )  . 
repp expression in oral squamous cell carcinoma qualitative and quantitative analysis slides were examined qualitatively under a bright - field microscope ( axioskop , zeiss , oberkochen , germany ) with 100 400 magnification for changes in the extent and localization of repp86 expression . 
counting was carried out per cm2 using a grid template , evaluating 300 50 cells median per visual field so that the overall number of evaluated cells with three visual fields per section was 900 150 cells [ 28 , 32 ]  . 
 staining of the extracellular matrix was not evaluated [ 13 , 22 ]  . statistical analysis descriptive analysis of li data was performed using the arithmetic mean and standard deviation ( sd )  . 
all calculations were made using spss 12.0 for windows ( spss inc , chicago , il , usa )  . results immunohistochemical analyses a total of ten samples of normal oral mucosa and 59 samples of oscc of all stages were analyzed in a blind - trial fashion by immunostaining repp86 using the monoclonal antibody ki - s2 . 
topoisomerase ii immunostaining is demonstrated by figures 3a and 3b . correlation of labeling indices with clinical and histopathologic parameters repp86 li in relation to different groups defined by clinical and histopathologic characteristics is surveyed in table 1 . 
while topoisomerase iia expression was significantly correlated with tumor size ( p < 0.05 ) , a correlation with lymph node invasion , or histopathologic grading could not be observed . 
 notwithstanding the statistical significance found for some of these correlations , a broad range of lis were encountered in all of the above - defined categories and the ranges were not strikingly different . 
 recent progress in analyzing the function and structure of cell cycle - associated proteins has considerably promoted our understanding of the mechanisms controlling cellular proliferation [ 19 , 26 ]  . 
the ability to identify antigens that are reliably associated with cellular proliferation in normal and neoplastic tissue , such as ki - 67 antigen and topoisomerase ii , has proven valuable in diagnostic histopathology table 2 . 
consequently , the assessment of proliferative activity has not been incorporated into broad clinical routine and decision processes in treatment of oscc [ 4 , 16 , 18 , 30 ]  . 
as cells in g1 make up the largest fraction of the cycling subpopulation , g1 is a major source of uncertainty in assessment of tumor proliferation [ 19 ]  . in our investigation , the anti - repp86 antibody labeled only two thirds ( 66.7% ) of the ki - 67and less than one half ( 44.1% ) of the topoisomerase ii - expressing cell population . 
although the size of the growth fraction is estimated correctly by ki - 67 and topoisomerase ii immunostaining , the repp86 li may reflect the biologically relevant fraction of proliferating cells more accurately . to be of relevance , any proliferation marker has to show a correlation with clinical outcome . 
the critical question is whether an exclusion of g1 - phase cells yields any advantages in terms of assessment of prognosis compared to an evaluation of the entire growth fraction . 
reported repp86 li to be the most statistically significant predictor of overall survival , disease - specific survival , and disease - free survival in multivariate analysis ( all two - sided p < 0.0001 ) [ 22 ]  . 
found repp86 li of > 10% to significantly predict a shortened disease - free interval and an increased tumor mortality ( both p < 0.0001 ) [ 17 ]  . 
repp expression in oral squamous cell carcinoma conclusion the results of our study show that the expression of repp86 is significantly elevated in oscc , when compared to normal oral mucosa . 
on the basis of our findings , a further evaluation of repp86 expression in a larger series of cases with respect to prognosis is necessary . acknowledgments we would like to thank parwaresch , department of pathology and hematopathology , university of kiel , germany , for the generous provision of ki - s2 and ki - s5 antibodies . 
 strahlentherapie und onkologie original article a prospective three - dimensional analysis about the impact of differences in the clinical target volume in prostate cancer irradiation on normal - tissue exposure a potential for increasing the benefit / risk ratio andrea hille , nadja tws , heinz schmidberger , clemens f . 
 results : the exposure of rectum and bladder volume was significantly lower in case of irradiation of the prostate only compared to inclusion of the proximal or entire seminal vesicles into the ctv . 
 conclusion : reduction of the ctv to the prostate only , or to the prostate + proximal seminal vesicles led to significant rectal and bladder dose sparing compared to irradiation of the prostate + entire seminal vesicles . 
in case of a need for irradiation of the entire seminal vesicles , patients should be informed about a higher risk for chronic rectal toxicity and , possibly , for bladder complications . 
 key words : radiotherapy prostate cancer clinical target volume normal - tissue complication strahlenther onkol 2005 ; 181 : 78995 doi 10.1007 / s00066 - 005 - 1452 - 1 eine prospektive dreidimensionale analyse ber den einfluss verschiedener klinischer zielvolumina bei der radiotherapie des prostatakarzinoms auf die normalgewebsbelastung . 
 ergebnisse : die belastung des darms ( tabelle 1 und abbildung 1 ) und der blase ( tabelle 2 ) war bei alleiniger bestrahlung der prostata im vergleich zum einschluss der proximalen oder ganzen samenblasen in das ctv signifikant niedriger . 
 schlsselwrter : radiotherapie prostatakarzinom klinisches zielvolumen normalgewebsbelastung 1 department of radiotherapy , university of goettingen , germany . received : april 12 , 2005 ; accepted : august 1 , 2005 strahlenther onkol 2005 no . 
the impact of differences in the ctv in prostate cancer irradiation on normal - tissue exposure introduction of fundamental importance in radiation treatment planning is the definition of the target volume . 
in prostate cancer treatment planning an uncertainty in clinical target volume ( ctv ) definition [ 7 , 24 , 37 ] and between different physicians [ 11 , 39 , 44 ] has been recognized in the recent years . 
newer technologies like magnetic resonance imaging ( mri ) have improved the delineation of the prostate and seminal vesicles [ 4 , 26 , 34 , 36 ] , but not the identification of patients with seminal vesicle involvement [ 15 , 35 ]  . 
 the assessment if the seminal vesicles may have tumor infiltration and should be included in the ctv must still rely on clinical and biological features [ 7 , 9 , 24 , 25 , 31 ]  . 
authors suggested a risk calculation for seminal vesicle involvement based on prostate - specific antigen ( psa ) and gleason score ( gs ) [ 7 , 25 , 36 ] , assigning patients in highand low - risk groups for seminal vesicle involvement , respectively . 
furthermore , even for high - risk patients the inclusion of the seminal vesicles in the treatment volume is still controversial [ 9 , 20 , 24 , 41 ]  . 
it is known that the normal tissues , including rectum and bladder , receive significantly higher radiation doses when the seminal vesicles are included in the ctv [ 7 , 24 ]  . 
suggested a risk - adapted ctv with the exclusion of seminal vesicles in low - risk patients , and the inclusion of only the proximal 22.5 cm ( approximately 60% ) of the seminal vesicles in high - risk patients [ 25 ]  . 
therefore , we performed a prospective analysis of prostate cancer irradiation with different ctvs , including prostate only , prostate + proximal seminal vesicles , and prostate + entire seminal vesicles , on rectal and bladder dose sparing . 
the prostate ( p ) , the prostate + entire seminal vesicles ( pesv ) , or the prostate + 60% in longitudinal direction ( 22.5 cm ) of the seminal vesicles ( ppsv ) were taken as ctv . 
though patients were asked to empty the rectum before ct scan was performed , and it is described that the dvhs of the rectal wall and of the whole rectum including filling are strongly correlated when the rectum is mostly empty [ 13 ] , we decided to contour both the rectal wall and the whole rectuthe difference between the inner and outer walls of the rectum was the rectal wall . 
the craniocaudal rectal extension was defined as the first ct slice above the anal verge ( caudal border ) , and the cranial limit was defined as the first slice below the sigmoid flexure . 
 one planning ct scan ( 5 - mm continuing , 5 - mm slice ) with patients in supine position was done with comfortably filled bladder and three plans were produced for each of the 14 patients . 
 to determine the amount of the rectum and the rectal wall exposed to radiation , the percentages of the volumes irradiated to 40 gy , 50 gy , 60 gy , and 70 gy were calculated by the treatment planning systeto determine the amount of the bladder exposed to radiation , the percentages of the bladder irradiated to 50 gy , 60 gy , 65 gy , and 70 gy were calculated by the treatment planning syste statistical analysis analysis was performed using the program statistica 6.1 ( stat soft , palo alto , ca , usa )  . 
 results rectum patients and methods 14 consecutive patients with localized prostate cancer undergoing external - beam radiotherapy with curative intent to volume of the whole rectuthe median volume of the whole rectum was 84 cm3 ( mean value 90 cm3 , standard deviation 31 cm3 )  . 
mean , median values , standard deviations ( sd ) , and p - values for the whole rectum exposed to 4070 gy in different clinical target volumes ( ctvs )  . 
vergleich der mittelwerte , standardfehler , standardabweichungen ( sd ) und p - werte des volumens des ganzen darms , der mit 4070 gy bei verschiedenen klinischen zielvolumina ( ctvs ) bestrahlt wurde . 
the mean exposure of the whole rectum in case of irradiation of the p only was 39% , 26% , 19% , and 9% to 40 gy , 50 gy , 60 gy , and 70 gy , respectively . 
for irradiation of the ppsv the mean exposure of the rectum was 64% , 49% , 39% , and 23% to 40 gy , 50 gy , 60 gy , and 70 gy , respectively . 
 in case of irradiation of the pesv the mean exposure of the rectum was 74% , 57% , 46% , and 27% to 40 gy , 50 gy , 60 gy , and 70 gy , respectively . 
the mean values for the whole rectum exposed to 40 gy , 50 gy , 60 gy , and 70 gy for the different ctvs are demonstrated graphically in figure 1 . 
 40 gy mean 50 gy mean 60 gy mean 70 gy mean median 35 median 25 6 median 19 5 9 9 3 median the mean values for the rectal wall volume exposed to 40 gy , 50 gy , 60 gy , and 70 gy for the different ctvs were comparable to the values for the whole rectu the differences between both the rectum and the rectal wall volume receiving 4070 gy were significant between p compared to ppsv / pesv , and between ppsv compared to pesv . 
for irradiation of the ppsv the mean exposure of the bladder volume was 57% , 44% , 36% , 30% , and 22% to 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy , respectively . 
 the differences between the bladder volume receiving 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy , were significant between p compared to ppsv / pesv , and between ppsv compared to pesv . 
 1 2 3 1 = prostate 2 = prostate + proximal seminal vesicles 3 = prostate + entire seminal vesicles 1 2 3 1 2 3 1 2 3 40 gy 50 gy 60 gy 70 gy mean value mean value standard error mean value standard diviation figure 1 . 
 in conclusion , the reduction of the ctv to the p only , or to the ppsv led to significant rectal dose sparing with a significantly reduced estimated risk for late rectal toxicity compared to irradiation of the pesv . 
our data are indicating that the suggestion of a risk - adapted ctv with the exclusion of seminal vesicle in low - risk patients and inclusion of only the proximal 22.5 cm ( approximately 60% ) of the seminal vesicles in patients with a higher risk for seminal vesicle involvement [ 25 ] should be followed wherever possible , to reduce the dose to the rectuhowever , due to the scarce data available quantifying the extent of seminal vesicle involvement [ 15 , 35 , 40 , 43 ] , irradiation of the entire seminal vesicles may be warranted in specific cases and patients should be informed about a higher risk for chronic rectal toxicity . 
 rectum several investigations indicate a relationship between the irradiated volume and the development of chronic rectal toxicity [ 1 , 3 , 10 , 12 , 19 , 22 , 28 , 42 , 45 , 47 ]  . 
 to relate the rectal dvhs in our study to an estimated risk for chronic rectal toxicity , the results were compared with studies analyzing relationships between dose - volume and rectal toxicity . 
it is known that there is a high variability of volume fractions of rectal dvhs depending on how the rectal borders are defined , and it is difficult to compare the results of different studies concerning rectal dvhs [ 14 , 16 ]  . 
 though the definitions of the rectum differ in some of these studies from our definition , and though the cutoff levels and the resulting risks for chronic rectal toxicity grade 2 are different in these studies , we can draw cautious conclusions from our results regarding an estimated risk for chronic rectal toxicity . for irradiation of the p only the dose constraint recommendations can easily be met . 
the estimated risk for chronic rectal toxicity ( > grade 2 ) in all plans irradiating the p only was < 5% , compared to 1520% for irradiation of the pesv . 
however , a study investigating different three - dimensional techniques ( two different four - field techniques and a three - field technique ) found that the differences in ctvs were comparable to the differences shown with the four - field technique described in our study [ 21 ]  . 
 new technologies like intensity - modulated radiation therapy ( imrt ) [ 2 , 5 , 17 , 30 ] are awaited to increase local control by increasing the dose in part of the prostate with lower normal - tissue toxicity . 
until such new technologies are not introduced as a widespread clinical routine treatment [ 6 ] , three - dimensional conformal radiation therapy should be used as standard treatment [ 1 , 18 , 27 , 38 , 46 ] in the awareness that the definition of the ctv has a great impact on normal - tissue exposure . 
 bladder to estimate the risk for chronic bladder toxicity , we tried to compare our data with the clinical relationship between dvhs and the development of chronic bladder toxicity , as reported in the literature . 
it is not known whether the differences in radiation exposure between the different ctvs would be comparable to the differences shown in our study in case of an empty or filled bladder . 
 authors definition of the rectum rectal volume ( % ) rectal dose ( gy ) toxicity risk for chronic rectal grade toxicity ( % ) used toxicity score median follow - up whole rectum cozzarini et al . 
 [ 10 ] 52 < 63 flexure ( patients with large air / 39 fecal content in the rectum < 39 were excluded from analysis ) > 65 anal verge to the sigmoid flexure < 65 > 30 < 30 > 25 < 25 anal verge to the sigmoid flexure 50 ( patients with large air / fecal content in 50 the rectum were excluded from analysis ) 60 50 anal verge to the sigmoid flexure ( patients with large air / fecal content in 50 the rectum were excluded from analysis ) 60 60 70 70 > 42 < 42 11 cm in length starting at 2 cm below > 26 the inferiormost aspect of the ischial < 26 tuberositas from the lower to the upper border of the fields rectum was identified with rectal contrast rectal wall 70 inferior border of the sacroiliac joints 70 to the anal region sigmoid colon to 15 mm caudal to the > 30 < 30 apex of the prostate fiorino et al . 
late complications like bladder contracture and volume loss are described in 510% at doses of 40 gy delivered to the majority of the bladder , at doses of 5065 gy delivered to about 30% of the bladder volume , and at doses of 6575 gy applied to < 20% of the bladder volume [ 32 ]  . 
 the risk for bladder toxicity in our study can be estimated to be < 510% in case of irradiation of the p only , and > 10% in case of irradiation of the ppsv / pesv . 
though the reduction of the ctv to the p / pssv led to a significantly lower exposed bladder volume compared to pesv , the estimation of the clinical value of a reduced irradiated bladder volume is difficult . 
 strahlentherapie und onkologie original article proton or stereotactic photon irradiation for posterior uveal melanoma ? a planning intercomparison stefan hcht1 , roland stark2 , frank seiler1 , jens heufelder2 , nikolaos e . 
foerster3 , wolfgang hinkelbein1 background and purpose : proton and stereotactic radiotherapy with photons ( srt ) are both used to treat choroidal melanomas in proximity to optic disk and fovea centralis , a situation where plaque therapy is prone to complications . 
a comparative treatment - planning study was done to assess the capability of both modalities to preserve vision . patients and methods : in ten patients treated with 68 - mev protons , srt with 6 - mv photons was planned . 
 results : proton - beam therapy was superior in eight of ten situations , and this result did not differ significantly by changes in the weighting of the different parameters analyzed . 
 conclusion : when dose deposition to those structures most important for the preservation of vision is taken into account , under the conditions examined proton therapy offers an advantage in the majority of the patients evaluated . 
 key words : proton therapy stereotactic radiotherapy comparative planning study uveal melanoma strahlenther onkol 2005 ; 181 : 7838 doi 10.1007 / s00066 - 005 - 1395 - 6 protonenoder stereotaktische photonenbestrahlung fr posteriore aderhautmelanome ? ein planungsvergleich hintergrund und ziel : fr aderhautmelanome am hinteren augenpol , die nicht mit plaques behandelt werden knnen , stehen protonentherapie und stereotaktische bestrahlung mit photonen ( srt ) zur verfgung . 
 schlussfolgerung : wenn die dosisbelastung der fr den erhalt des sehvermgens bedeutsamsten strukturen als entscheidend betrachtet wird , ist die protonentherapie unter den fr die untersuchung gewhlten bedingungen in der mehrzahl der flle berlegen . 
 schlsselwrter : protonentherapie stereotaktische bestrahlung vergleichende planungsstudie aderhautmelanom 1 department of radiooncology and radiotherapy , charit university medicine berlin , campus benjamin franklin , berlin , germany , 2 ophthalmic tumor therapy at the ion - beam laboratory , hahn - meitner institute berlin , germany , 3 ophthalmologic clinic , charit university medicine berlin , campus benjamin franklin , berlin , germany . received : november 17 , 2004 ; accepted : august 11 , 2005 strahlenther onkol 2005 no . 
stereotactic photon irradiation for uveal melanoma introduction uveal melanoma is a very rare malignant tumor with an estimated incidence of only 0.60.8 per 100 , 000 per annum in western europe [ 5 ]  . 
tumors of the posterior aspect of the globe are difficult to treat because of the proximity to those structures most relevant for preservation of visual acuity [ 1 ]  . 
 the general perception is , that tumors located within 2 mm of the optic disk or fovea centralis should not be treated with radioactive plaques due to the high doses at areas in close proximity to the surface of the plaque applicator and hence an inevitable risk of radiation damage to these structures [ 2 , 7 ]  . 
 proton - beam therapy not only in this situation offers many advantages by the very sharp distal fall - off , enabling homogeneous treatment of the tumor without excessive risks of damage to organs or structures nearby [ 10 , 14 , 17 , 22 , 24 ]  . 
 excellent local control rates of approximately 95% at 5 years have been reported from most of the centers , but proton therapy centers are rare with only some ten centers in europe and russia , a population of about 0.5 billion inhabitants , and due to the enormous costs in building and maintenance and the manpower necessary to run them , therapy is expensive [ 6 , 11 , 15 ]  . 
other forms of high - precision conformal radiotherapy have developed over the years and nowadays gamma knife as well as linear accelerator - based stereotactic radiotherapy or radiosurgery are broadly available . 
 comparison of the published series is a difficult matter , as there are many interdependent risk factors for not achieving tumor control as well as for developing sequelae and there are merely no prospective studies . 
high - resolution computed tomography of the involved eye in each case was done ( somatom volume zoom , siemens ag medical solutions , erlangen , germany ; slice thickness and collimation 1.0 mm , 120 kv , 100 ma , reconstruction increments of 1.0 mm ; kernel h 50 )  . 
 for proton therapy a safety margin of 1.5 mm surrounding the tumor outline was applied and adjusted manually , as the eyeplan program does not support modern icru - based volume definitions . 
planning cts for this study were performed in a modified headrest of a stereotactic treatment system ( brainlab ag , heimstetten , germany ) which had been supplemented for these purposes by an adjustable led light for eye fixation as shown in figure 1 . 
to make all the information which form the basis of treatment plan generation in proton therapy available for srt planning , based on the program image pro plus 4.0 ( media cybernetics , silver spring , md , usa ) a tool was developed to export the information used for proton therapy treatment planning into the planning cts on a slice - by - slice basis as shown in figure 2 . 
 srt was planned with a straightforward view without globe rotation , and therefore a reduction of the safety margin in ptv ( planning target volume ) delineation to 1.0 mm was made , taking into account that the direction on which the globe is rotated for proton therapy ( in general approximately 30 ) sometimes leads to inconsistencies and rapid correctional movements that cannot be compensated otherwise , thus giving need for a somewhat larger safety marg to be comparable with the restricted possibilities of the eyeplan program , only the first 10 mm of the optic nerve were contoured without surrounding fibrovascular or connective tissue for srt . 
srt planning was done with the program brainscan 4.03 ( brainlab ag ) for a 6 - mv photon linear accelerator ( clinac 600 cd , varian medical systems , palo alto , ca , usa )  . 
minimum allowed distance between ptv contour and beam aperture was set to 2.0 m to achieve a dose homogeneity comparable to proton treatment , constraints were set as follows : at least 97% of the ptv should be encompassed with at least 90% and at most 110% of the reference dose ( for reasons see discussion )  . 
due to the tiny size of fovea and optic disk no dvhs could be generated for them with the srt program , instead point doses were measured with the program tool available for these purposes . 
for the optic nerve a 15% difference in minimum or maximum dose or a significant difference in the integrated dose was chosen as cutoff point for evaluating differences , whereas the criteria applied to dose deposition to the lens were no versus any dose deposition or a significant reduction in the maximum dose . comparison of the doses to the optic nerve was complicated twofold , first by the fact that the program eyeplan on the one hand uses a simplification showing only 10 mm of its length and on the other hand it does not show the anatomy as seen in ct or mri examinations , as only the central parts are shown and not the surrounding tissues . 
 results in detail , the results of dose deposition to the structures fovea centralis , optic disk , optic nerve , and lens are shown in table 2 , and a summary of the results achieved is given in table 3 . 
 the doses to fovea centralis for patients #1 , 3 , 5 , 6 , 9 , and 10 were equal for both modalities , protons were superior in patients #4 , 7 , and 8 , whereas srt was superior in patient #2 . 
in the analysis of dose deposition to optic disk results for patients #1 , 6 , 7 , 8 , and 9 were without relevant differences , in patients #2 , 3 , 4 , and 5 protons were better , in patient #10 srt fared figure 1 . 
 in patients #2 , 3 , 4 , and 5 there was no dose delivery ; in patients #1 and 9 , although comparable in their minima and maxima , the integrated dose over volume was by far lower for protons ( making them advantageous )  . 
proton therapy has been in clinical use in this indication for approximately 30 years and many thousands of patients have been treated that way , the majority either at massachusetts general hospital harvard cylotron in boston , ma , usa , or and at the paul scherrer institute in switzerland . 
extensive documentations on long - term follow - up do exist , and the results could more or less be reproduced by other institutions [ 6 , 11 , 15 , 16 ]  . 
still all of these publications are retrospective in nature and direct comparisons to the second existing radiotherapeutic modality stereotactic radiotherapy or radiosurgery do not exist although many aspects of these modalities have been described [ 9 , 18 , 20 , 23 ]  . 
 many different factors have potential influence on the results achievable in the treatment of uveal melanomas and some of them are even interrelated , making direct comparisons of the reports on stereotactic radiotherapy and hadron therapy a very difficult topic [ 6 , 8 , 12 ]  . 
as this problem will most probably not dissolve over the next years , there is a substantial need for alternative modes to compare these modalities , although one has to keep in mind , that long - term clinical results are the main objective measure of treatment quality . 
fovea centralis and even the optic disk , which may be positioned eccentric to the optic nerve , are not visible on ct and mri , and thus they cannot routinely be taken into account in srt planning , leaving dose deposition to them unaddressed although they are the factors most critical in preserving vision [ 2 , 5 , 13 , 21 ]  . 
by the methods employed , we were able to use these anatomic areas and tailor srt to reduce the probability of side effects to the analysis of treatment plans on the basis of dvhs could not be done by the srt planning program for fovea and optic disk due to the small size of these structures and point doses had to be used for comparison , which has to be regarded as a drawback of the present study , as more sophisticated tools for comparisons are desirable [ 19 ]  . 
 reduction of the safety margin to 1.0 mm for the ptv in srt planning in this study is down to the level of the resolution of the imaging modalities used , and without technical means to control for setup accuracy as they are used for proton therapy , this would be a very risky strategy , given the known deviations in ocular srt , where in general safety margins of 1.52.5 mm are applied [ 3 , 9 , 13 , 18 , 20 , 21 ]  . 
as srt will not have the necessity to utilize far out view directions as in proton therapy , a smaller safety margin in srt than in proton therapy helps to compare both modalities under conditions which at least are not putting srt at a disadvantage . 
 we could not evaluate dose distribution to the ciliary body , which is not easily viewable in planning cts and the representation in eyeplan is not precise enough to transfer this information to srt planning . 
as a surrogate dose deposition to the lens may be a suitable parameter and there were no major differences in both modalities making it unlikely that analysis of the ciliary body would have much influence on the results . 
given the well - documented dose dependency of radiation maculopathy and papillopathy , allowing higher maximum doses in srt plans might bear severe risks for the preservation of vision [ 12 ]  . 
combs1 , 2 , sybille gutwein2 , christoph thilmann1 , 2 , jrgen debus1 , 2 , daniela schulz - ertner1 , 2 purpose : to assess the effect of reirradiation in recurrent who grade iii astrocytomas . patients and methods : from january 1995 to july 2003 , 40 patients with grade iii gliomas were treated with fractionated stereotactic reirradiation at the time point of recurrence . 
a median target total dose of 36 gy ( range 2057.6 gy ) was applied using a median fractionation of 5 2 gy / week with a 6 - mev linear accelerator . results : radiotherapy was well tolerated by all patients . 
no prognosticators for survival or progression - free survival after reirradiation could be identified . conclusion : fractionated stereotactic radiotherapy is well tolerated and effective in patients with recurrent grade iii astrocytomas . key words : recurrent grade iii astrocytoma oligodendroglioma oligoastrocytoma radiation therapy strahlenther onkol 2005 ; 181 : 76873 doi 10.1007 / s00066 - 005 - 1415 - 6 rebestrahlung von grad - iii - astrozytomen mit fraktionierter stereotaktischer radiotherapie ( fsrt ) ziel : evaluation des effekts einer rebestrahlung bei patienten mit who - grad - iii - astrozytomen . patienten und methodik : von januar 1995 bis juli 2003 wurden 40 patienten mit who - grad - iii - gliomen zum zeitpunkt der tumorprogression mit stereotaktischer fraktionierter rebestrahlung behandelt . 
appliziert wurde eine mediane dosis von 36 gy ( spannbreite 2057 , 6 gy ) auf das zielvolumen in einer medianen fraktionierung von 5 2 gy / woche mit einem 6 - mev - linearbeschleuniger . ergebnisse : die therapie wurde von allen patienten gut vertragen . 
es konnten keine signifikanten einflussfaktoren auf berleben und progressionsfreies berleben nach rebestrahlung identifiziert werden . schlussfolgerung : die fraktionierte stereotaktische radiotherapie wird von den patienten sehr gut toleriert und ist eine effektive therapieform fr patienten mit rezidivierten who - grad - iii - gliomen nach vorbestrahlung . schlsselwrter : progrediente grad - iii - astrozytome oligodendrogliome oligoastrozytome strahlentherapie 1 department of radiation oncology german cancer research center ( dkfz ) , inf 280 , heidelberg , germany , 2 department of radiation oncology , inf 400 , university of heidelberg , germany . received : january 18 , 2005 ; accepted : june 10 , 2005 strahlenther onkol 2005 no . 
in spite of improvement of neurosurgical and radiotherapeutic techniques and of the implementation of chemotherapy in the primary treatment , all gliomas eventually recur locally after initial treatment [ 34 , 44 ]  . 
the inability to achieve local tumor control leads to progressive neurologic deficits resulting in a devastating medical condition and subsequent death in most patients with recurrent gliomas [ 7 ]  . 
a benefit of neurosurgical intervention might be that subsequent treatments can become more effective since treatment - resistant hypoxic cells are removed , and the size of the lesion can be reduced [ 42 ]  . 
however , complete reresection is often very difficult due to the infiltrative nature of the disease , if substantial morbidity is to be avoided [ 11 , 18 ]  . systemic chemotherapy offers a modest benefit for recurrent gliomas [ 3 , 4 , 37 ]  . 
in meta - analyses , a minor survival benefit has been recognized , if chemotherapy was added to standard surgical and radiation therapy ( rt ) of primary gliomas [ 13 , 41 ]  . 
however , there is little evidence that patients benefit from chemotherapy at the time point of progression [ 20 ]  . rt may be applied in selected cases of tumor progression or recurrence , even though radiation was a component of initial therapy . 
stereotactic radiosurgery ( srs ) is appealing due to its ability to deliver a high dose of radiation in a single fraction to the target in a very precise manner [ 7 , 8 , 21 , 25 , 43 ]  . 
in the present study we evaluated benefits and side effects of reirradiation with fsrt in patients with recurrent anaplastic gliomas ( who grade iii )  . patients and methods from january 1995 to july 2003 , we treated 40 patients with primary who grade iii gliomas with stereotactically performed reirradiation at the time point of recurrence . 
pathology reviews at the time point of primary diagnosis confirmed primary grade iii astrocytoma in 22 patients ; in ten patients a grade iii oligodendroglioma and in eight patients a grade iii oligoastrocytoma could be diagnosed . 
in one patient , iodine - 125 ( 125i ) seeds were implanted as the primary irradiation modality . median age at recurrence was 42 years ( range 2475 years )  . 
surgery was performed for recurrent tumors in ten patients ( subtotal resection n = 9 , biopsy n = 1 )  . karnofsky performance score was 80 in 38 and < 80 in two patients upon initiation and also at the end of reirradiation . 
the median time interval between primary diagnosis and reirradiation for recurrence was 34.5 months ( range 4139 months ) , the median interval between the first rt and the initiation of reirradiation was 31.5 months ( range 3126 months )  . as described previously , contrast - enhanced ct and mri scans were performed in an individual scotch cast mask fixation for three - dimensional treatment planning with an overall geometric accuracy of 12 mm [ 8 , 22 , 33 ]  . 
the median size of the planning target volume ( ptv ) for reirradiation was 56.2 ml ( range 25.1296.2 ml ) , consisting of the area of contrast entable 1 . 
 n = 40 female male histology who grade iii glioma age at primary diagnosis ( years ) < 50 50 age at reirradiation ( years ) < 50 50 karnofsky performance score 80 < 80 neurologic symptoms yes no strahlenther onkol 2005 no . 
fsrt for recurrent grade iii astrocytoma none of the patients received concomitant chemotherapy . patients were seen for follow - up visits 6 weeks after completion of rt , then in regular 3to 6 - month intervals depending on the patients clinical condition . 
 additional mri scans and clinical assessment were performed , if new symptoms developed or deterioration was observed . overall survival was calculated from the time point of primary diagnosis of who grade iii glioma ; survival after reirradiation was calculated from initiation of reirradiation for recurrence . 
progression - free survival after reirradiation was calculated from the first day of reirradiation treatment until tumor progression or death ( by any cause ) , whichever happened first , using the kaplan - meier method . 
statistical analyses were perfomed using the software program statistica 6.0 ( statsoft , hamburg , germany )  . 100 time ( months ) 20 40 60 80 100 120 140 160 180 200 time ( months ) figures 1a and 1b . 
das ausma der neurochirurgischen resektion hatte einen signifikanten einfluss auf das gesamtberleben ( b ; p = 0 , 009 )  . hancement in t1 - weighted sequences , adding a 0.5to 1 - cm safety margin to include microscopic spread of tumor cells . 
we applied a median total dose of 36 gy ( range 2057.6 gy ) , depending on size and localization of the recurrence with respect to the dose which had been applied in this area by the first course of irradiation , using a median fractionation of 5 2 gy / week with a 6 - mev linear accelerator ( primus , siemens , erlangen , germany )  . 
three to four irregular non - coplanar fields were implemented and shaped with a multileaf collimator . results complete resection subtotal resection biopsy in all patients overall toleration of stereotactically guided reirradiation was very good . 
the median follow - up time after reirradiation was 13 months ( range 198 months )  . median overall survival calculated from primary diagnosis was 48 months ( range 7180 months ; figure 1a )  . 
no prognosticators for survival and progression - free survival from reirradiation could be identified . discussion tumors of the central nervous system ( cns ) represent a heterogeneous population of neoplasms . the who definition of gliomas emphasizes degrees of cellularity , nuclear and cellular pleomorphism , mitosis , endothelial proliferation , and necrosis , dividing gliomas into four categories [ 24 ]  . 
glioblastoma multiforme , the most malignant neuroepithelial brain tumor , is a highly cellular tumor with nuclear and cellular pleomorphism , endothelial proliferation , mitotic figures , and , often , necrosis . 
commonly , overall survival from the time point of primary diagnosis ranks between 2 and 3 years , with 5 - year survival rates of 18% [ 2 , 19 , 23 , 35 ]  . 
one study reports a median survival of 81 and 54 weeks , respectively , in patients with anaplastic astrocytoma and glioblastoma treated with high - activity 125i interstitial implants [ 29 ]  . 
generally , srs has demonstrated efficacy in selected patients suffering from recurrent glioblastoma with median overall survival times for patients with glioblastoma multiforme of up to 18 months , calculated from the time of primary diagnosis [ 43 ]  . 
could only achieve a median survival of 8 months in patients with recurrent malignant glioma treated with srs [ 16 ]  . however , srs is limited to small lesions . 
reirradiation using conventional external beam was associated with only modest palliative and survival benefits , and the toxicity associated with retreatment with conventional external beam is likely to outweigh its benefits [ 1 ]  . 
however , to allow precision rt , patients must be fixed in an individual mask fixation system ; thus only patients with an overall tolerable performance status to allow for daily positioning were chosen for reirradiation , weighing potential side effects against a potential therapeutic effect . 
 in the present study of patients with recurrent aa , toleration of fsrt was very good in all patients , and the median overall survival time of 48 months is well above the data found in the literature . 
 in the literature , the majority of studies investigating the effectiveness of fsrt apply a relatively large dose per fraction , commonly 5 gy in a hypofractionated regimen , with only a single study applying doses in the range of 1.83 gy [ 7 , 15 , 28 ]  . 
the late complication rate is relatively high with a range from 8% up to 36% , however , a fair comparison is difficult because of variation in target definition , treatment technique , total dose and fractionation scheme , and preexisting patient characteristics . 
a major factor that could lead to an increased risk for toxicity is the concurrent administration of chemotherapy [ 15 , 28 ]  . histological features of gliomas are considered prognostic factors determining the outcome . 
our patient collective did not show statistical differences in overall survival and progression - free survival in regard to their histological classification , in accordance with a study published by winger et al . 
however , extent of neurosurgical resection after primary diagnosis significantly influenced overall survival , with patients who received a complete resection demonstrating a clear benefit compared to patients whose tumors could only be biopsied . 
this direct influence of neurosurgical resection has been shown to be one of the strongest prognosticators of overall survival [ 45 ]  . karnofsky performance score has been reported to be a strong predictor of survival in patients with gliomas [ 5 , 14 , 26 , 36 ]  . 
 this might be due to the small number of patient with a performance score < 80 , since the rigid mask fixation system commonly requires a relatively good performance status . median survival calculated from the time point of reirradiation amounted to 16 months in our trial . 
in the literature , survival times of 14.7 months for grade iii astrocytomas treated with srs or fsrt at the time point of recurrence were reported by cho et al . 
however , this was a nonrandomized study and results might be influenced by confounding factors affecting the outcome . further evaluation of fsrt in a larger patient collective is warranted in a randomized , controlled setting . 
additionally , since radiochemotherapy regimens revealed to be safe , feasible and effective with regard to overall and progression - free survival , combined treatment of recurrent aa with radiotherapy and concomitant chemotherapy such as temozolomide might be considered . conclusion our data underline previous results from our institution and other groups investigating fsrt in cases of recurrent aa . 
both materials allow a sufficient dose distribution , but with mcp96 the coverage of the planning target volume and the dose sparing of the left parotid gland can be improved . 
12 urban & vogel strahlentherapie und onkologie originalarbeit prognostische wertigkeit der zeitparameter in der adjuvanten radiotherapie von hno - tumoren eine retrospektive untersuchung an 138 patienten barbara dietl , christof schfer , oliver klbl1 ziel : untersuchung der frage , welchen einfluss die radiotherapie - assoziierten zeitfaktoren wartezeit , bestrahlungszeit und gesamtbehandlungszeit ( ott [ overall treatment time ] ) auf die endpunkte gesamtberleben , ereignissowie lokalrezidivfreies berleben ( os , efs , lrfs ) bei patienten mit fortgeschrittenen hno - tumoren und adjuvanter radiatio ausben . 
 patienten und methodik : retrospektiv wurden bei n = 138 patienten geschlecht , tumor - , nodalund resektionskantenstatus , differenzierungsgrad , tumorlokalisation , operationstechnik , wartezeit auf eine radiatio , ott , bestrahlungszeit sowie der postoperative hmoglobinwert univariat ( log - rank - test nach kaplan - meier ) bezglich des os , lrfs und efs untersucht . 
 ergebnisse : in der univariaten analyse beeinflusste neben einem postoperativen hmoglobinwert < 12 g / dl eine ott 105 tage smtliche endpunkte signifikant negativ , ebenso eine bestrahlungszeit 60 tage . 
in der multivariaten analyse nach cox verblieben als unabhngige negative prognostische parameter fr smtliche endpunkte eine ott 105 tage sowie ein postoperativer hmoglobinwert < 12 g / dl . schlussfolgerung : die wartezeit sollte nach dem asara - prinzip as short as reasonably achievable gehandhabt , die bestrahlungszeit nicht protrahiert werden , um einen grenzwert der ott < 105 tage einzuhalten . 
prinzipiell sind die zeitparameter in die onkologische standarddokumentation einzubinden , um knftig eine weitere evaluation und differenzierung dieser prognostisch relevanten faktoren im kontext einer tumorerkrankung zu ermglichen . schlsselwrter : zeitparameter wartezeit bestrahlungszeit gesamtbehandlungszeit hno - tumoren prognostische faktoren strahlenther onkol 2005 ; 181 : 8007 doi 10.1007 / s00066 - 005 - 1449 - 9 the prognostic value of time parameters in adjuvant radiotherapy of head and neck cancer . 
a retrospective analysis of 138 patients purpose : to answer the question , how the parameters waiting time , radiation treatment time and overall treatment time ( ott ) influenced the endpoints overall ( os ) , event - free ( efs ) and local recurrence - free survival ( lrfs ) in patients with locally advanced head - and - neck cancer , who had received postoperative radiotherapy . 
besides the time parameters waiting time , radiation treatment time and ott , tumorand therapy - related parameters ( t - , n - , r - status , grading , tumor site , surgical technique , and postoperative hemoglobin < 12 g / dl ) with potential impact on the endpoints were investigated in the univariate analysis ( kaplan - meier log - rank test )  . 
 results : besides a postoperative hemoglobin value < 12 g / dl , in the univariate analysis an ott 105 days negatively influenced all endpoints , as well as a radiation treatment time 60 days . 
 conclusion : the waiting time should be managed according to the asara ( as short as reasonably achievable ) recommendation , radiation treatment should not be protracted exceeding an overall treatment of 105 days . 
die durch fraktionierte strahlentherapie erreichbare lokale kontrolle von tumorerkrankungen wird nicht nur durch die gesamtdosis , dosis pro fraktion und strahlentherapeutische parameter beeinflusst , sondern auch durch den zeitraum , der zwischen einer eventuellen operation und dem bestrahlungsbeginn vergeht , sowie aus strahlenbiologischen grnden durch die gesamtbehandlungszeit einer fraktionierten strahlenbehandlung . 
daher fordern herrmann & baumann in einer bersichtsarbeit , neben den strahlenbiologischen parametern einzelund gesamtdosis auch die gesamtbehandlungszeit ( ott [ overall treatment time ] ) zu bercksichtigen [ 15 ]  . 
 diese setzt sich im fall einer postoperativen bestrahlung aus der wartezeit , dem zeitraum von der operation bis zum ersten bestrahlungstag , sowie der dauer einer strahlentherapeutischen behandlung vom ersten bis zum letzten bestrahlungstag zusammen . 
 die wartezeit auf eine radiotherapie hngt neben einer qualifizierten interdisziplinren kooperation vor allem von der verfgbarkeit strahlentherapeutischer einrichtungen ab , die in europa sehr unterschiedlich ist [ 7 ]  . 
 eine aktuelle statistik aus dem thames cancer registry bei 57 426 mnnern und 71 018 frauen ergab , dass in sdostengland die mediane wartezeit auf eine radiotherapie zwischen 42 und 65 tagen variiert und seit 1999 deutlich ansteigt [ 26 ]  . 
die aus der wartezeit resultierenden konsequenzen bezglich des ereignisfreien berlebens ( efs ) und gesamtberlebens ( os ) wurden in diesen studien nicht weiter analysiert . ziel dieser arbeit war es , bei einem monozentrischen kollektiv postoperativ bestrahlter patienten mit meist fortgeschrittenen hno - tumoren retrospektiv die parameter wartezeit , bestrahlungszeit und ott im kontext der tumorerkrankung und ihrer therapie in einer deskriptiven statistik zu erfassen und ihre prognostische wertigkeit bezglich des os , lrfs ( rezidivfreies berleben ) und efs zu untersuchen . 
 patienten und methodik patienten in die retrospektive analyse wurde 138 patienten eingeschlossen ( 115 mnner , 23 frauen , medianes alter 56 jahre ) , die von 10 / 1993 bis 05 / 2000 nach operativer entfernung eines hno - tumors bestrahlt wurden und anschlieend im rahmen der tumornachsorge im tumorzentrum regensburg registriert waren . 
smtliche patienten waren zum zeitpunkt der erstdiagnose metastasenfrei ; 121 patienten litten an einem lokal fortgeschrittenen befund ( 87 , 7% stadium iii und iv nach ajcc [ american joint committee on cancer ] ) ; der body - mass - index ( bmi ) betrug im median 23 , 3 . 
einfluss radiotherapie - assoziierter zeitfaktoren auf das berleben 70 60 50 40 30 20 10 0 ( r0 ) , bei 27 lag ein mikroskopischer tumorrest vor ( r1 ) , bei neun patienten ein makroskopischer ( r2 ) ( tabelle 2 )  . 
bei smtlichen stadien iii und iv wurde in einer gemeinsamen interdisziplinren besprechung die indikation zur radiatio gestellt , bei vier patienten mit stadium ii wurde aufgrund der r1 - situation , bei 13 patienten im stadium ii aufgrund knapper resektionskanten individuell eine postoperative radiatio indiziert . 
 postoperative radiotherapie die radiotherapie erfolgte nach individueller maskenanpassung , computer - , simulatorund rechnergesttzter planung dreidimensional konformal in einzeldosen von 1 , 8 gy ( n = 9 ) bzw . 
die radiatio wurde ber seitliche gegenfelder unter einschluss des primrtumors und der regionren lymphabflsse in isozentrischer technik bis zu einer gesamtherddosis ( ghd ) von 56 gy bei n0 bzw . 
 therapie chirurgie chirurgie des primrtumors tumorexzision laser - tumorexzision neck - dissektion ( nd ) keine nd unilaterale nd bilaterale nd resektionskantenstatus r0 r1 r2 intraoperative transfusionen ja nein strahlentherapie wartezeit ( tage ) median spannweite bestrahlungstage ( rt ) median spannweite gesamtbehandlungszeit ( ott , tage ) median spannweite einzeldosis 1 , 8 gy 2 , 0 gy 2 , 5 gy gesamtherddosis ( gy ) median spannweite 78 , 3 21 , 7 5 , 8 40 , 6 53 , 6 73 , 9 19 , 6 6 , 5 94 , 2 5 , 8 6 , 5 80 , 4 patienten ( n ) 108 30 8 56 74 102 27 9 130 8 35 15127 48 3295 86 56176 9 111 18 65 5672 56 58 60 62 64 66 68 70 72 74 gesamtherddosis ( gy ) abbildung 1 . 
 zeitintervalle das zeitintervall vom operationstag bis zur ersten bestrahlung wurde als wartezeit definiert , der zeitraum von der ersten bis zur letzten bestrahlung als bestrahlungszeit , die summe beider intervalle als ott bzw . 
 fr die statistische auswertung wurden die hb - werte bei erstdiagnose ( hb pr op ) , postoperativ ( hb post op ) , vor beginn der radiatio ( hb pr rt ) und im nadir ( hb min rt ) geschlechtsunabhngig bei 12 g / dl dichotomiert ( 0 12 , 1 g / dl ; 1 < 12 g / dl ) , da dieser wert entsprechend den ascoempfehlungen im rahmen einer erythropoetin - basierten anmiekorrektur angestrebt werden soll [ 25 ]  . 
einfluss radiotherapie - assoziierter zeitfaktoren auf das berleben nachbeobachtung in den ersten 5 jahren stellten sich die patienten entsprechend den nachsorgeempfehlungen der degro regelmig , mindestens einmal jhrlich , in unserer strahlentherapeutischen ambulanz vor . 
 die mediane nachbeobachtungszeit betrug 56 , 5 monate . statistik zur evaluation von einflussgren auf das os , efs und lrfs erfolgte eine univariate analyse potentieller einflussfaktoren mit dem log - rank - test nach kaplan - meier . 
 einzelparameter mit einem signifikanten einfluss ( signifikanzniveau 5% ; p = 0 , 05 ) auf os , efs und lrfs im logrank - test wurden in einer multivariaten regressionsanalyse nach cox weiter in einem stepwise - backward - verfahren untersucht , das bei jedem schritt die am wenigsten signifikante variable eliminierte . 
 ergebnisse hmoglobinwerte und hmoglobinverlauf properativ betrug der hb - wert im median 13 , 8 g / dl , postoperativ 12 g / dl , vor der radiatio 12 , 4 g / dl , und im nadir whrend der radiatio median 11 , 3 g / dl ( tabelle 3 )  . 
 die bestrahlungszeit variierte zwischen 32 und 95 tagen , im median betrug sie 48 tage , im durchschnitt 50 tage ; bei 75% der patienten dauerte die radiotherapie < 54 tage ( figure 2b )  . 
 im log - rank - test bten von den untersuchten parametern mnnliches geschlecht , ein positiver n - status , eine positive resektionskantensituation und ein postoperatives hb < 12 g / dl einen signifikant negativen einfluss auf das os aus . 
 in der multivariaten analyse nach cox verblieben als unabhngige negative prognostische parameter auf das os mnnliches geschlecht , ein postoperatives hb < 12 g / dl , ein positiver n - status , ein positiver resektionskantenstatus sowie eine ott 105 tage ( tabelle 5 )  . 
 patienten mit einem postoperativen hb 12 g / dl ( n = 71 ) hatten ein medianes os von 83 monaten , mit einem hb < 12 g / dl ( n = 67 ) ein medianes os von 29 monaten . 
 ereignisfreies berleben ( efs ) das mediane efs betrug 44 , 5 monate , das 2 - jahres - efs 58% , das 5 - jahres - efs 45% ( abbildung 3b )  . 
 zum zeitpunkt der auswertung ( 05.03.2004 ) waren 54 patienten am leben und 84 verstorben ; 16 patienten hatten ein lokalrezidiv , 14 einen kombinierten systemischen und lokalen progress und zehn einen alleinigen systemischen progress . 
 properatives hmoglobin ( g / dl ) median spannweite postoperatives hmoglobin ( g / dl ) median spannweite hmoglobin vor radiatio ( g / dl ) median spannweite nadir hmoglobin whrend radiatio ( g / dl ) median spannweite 13 , 8 817 , 3 715 , 7 12 , 4 8 , 115 , 7 11 , 3 715 , 7 strahlenther onkol 2005 no . 
einfluss radiotherapie - assoziierter zeitfaktoren auf das berleben 10 20 30 40 50 60 70 80 90 100 110 120 130 140 wartezeit ( tage ) 30 35 40 45 50 55 60 65 70 75 80 85 90 95 100 bestrahlungszeit ( tage ) abbildung 2a figure 2a abbildung 2b figure 2b 45 40 35 30 25 20 15 10 5 0 80 70 60 50 40 30 20 10 0 20 40 60 80 100 120 140 160 180 200 gesamtbehandlungszeit ( tage ) abbildung 2c figure 2c im log - rank - test beeinflussten mnnliches geschlecht , positiver resektionskantenstatus und ein postoperatives hb < 12 g / dl das efs signifikant negativ . 
in die coxanalyse ging als bergeordneter unabhngiger zeitparameter nur noch die ott e in der multivariaten analyse nach cox verblieben als unabhngige negative prognostische parameter fr das efs mnnliches geschlecht , ein postoperatives hb < 12 g / dl , positive resektionsrnder und eine ott 105 tage ( tabelle 5 )  . 
 so hatten patienten mit einem postoperativen hb 12 g / dl ( n = 71 ) ein medianes efs von 69 monaten versus 20 , 3 monaten bei patienten mit einem postoperativen hb < 12 g / dl ( n = 67 )  . 
wartezeit , entsprechend dem intervall von der operation bis zum ersten bestrahlungstag ( a ) , bestrahlungszeit , entsprechend dem zeitraum vom ersten bis zum letzten bestrahlungstag ( b ) , und gesamtbehandlungszeit ( c ) , in tagen . 
univariate analyse potentieller einflussfaktoren auf gesamtberleben ( os ) , ereignisfreies berleben ( efs ) und lokalrezidivfreies berleben ( lrfs ) , log - rank - test nach kaplan - meier . 
univariate analysis of potential influence factors on overall survival ( os ) , event - free survival ( efs ) , and local recurrence - free survival ( lrfs ) , kaplan - meier log - rank test . 
ci : konfidenzintervall ; efs : ereignisfreies berleben ; hb : hmoglobin ; hr : hazard - ratio ; lrfs : lokalrezidivfreies berleben ; os : gesamtberleben ; ott : gesamtbehandlungszeit . 
ci : confidence interval ; efs : event - free survival ; hb : hemoglobin ; hr : hazard ratio ; lrfs : local recurrence free survival ; os : overall survival ; ott : overall treatment time . 
 im log - rank - test bten von den untersuchten parametern ein postoperatives hb < 12 g / dl , eine bestrahlungszeit 60 tage sowie eine ott 100 tage einen signifikant negativen einfluss auf das lrfs aus ( tabelle 4 )  . 
 in der multivariaten analyse nach cox verblieben als unabhngige negative prognostische parameter fr das lfrs ein postoperatives hb < 12 g / dl sowie eine ott 100 tage ( tabelle 5 )  . 
 die hazard - ratio - werte und die zugehrigen konfidenzintervalle demonstrieren das relative risiko bezglich des eintretens der endpunkte exitus , ereignisse und lokalrezidiv in den unterschiedlichen kategorien der untersuchten variablen ( tabelle 5 )  . 
 so versteht man in der angelschsischen literatur unter wartezeit den zeitraum von der tumordiagnosestellung bis zum beginn der radiotherapie [ 26 ] , eine definition , die fr die primre radiotherapie zutrifft , whrend die wartezeit auf eine adjuvante radiotherapie blicherweise das postoperative intervall bis zum beginn der radiotherapie beschreibt . richtlinien zu den grenzwerten der einzelnen zeitintervalle existieren nicht , obwohl die klinische bedeutung der zeitfaktoren bekannt ist . 
 [ 16 ] zeigten in der metaanalyse eines gepoolten kollektivs von 851 patienten aus sieben studien [ 2 , 6 , 9 , 18 , 29 , 32 , 33 ] ein erhhtes lokalrezidivrisiko bei einem aufschub der postoperativen radiatio von > 6 wochen ; in zwei studien wurde das signifikanzniveau erreicht [ 9 , 32 ]  . 
 nach den standards for waiting times des jcco ( joint collegiate council for oncology ) soll mit einer postoperativen radiotherapie , zumindest bei brustkrebs , nicht lnger als 4 wochen post operationem gewartet werden . 
in anlehnung an das alara - prinzip ( as low as reasonably achievable ) der strahlenschutzgesellschaft forderten sie daher das asara - prinzip ( as short as reasonably achievable ) [ 21 ]  . 
an 868 adjuvant bestrahlten patienten mit hno - tumoren , dass bei einer therapiezeit von 45 tagen behandlungspausen von < 6 tagen fr die lokale kontrolle bedeutungslos sind , eine verlngerung der therapiedauer darber hinaus die 5 - jahres - lokalkontrollrate um jeweils 12% pro zustzlichen therapietag reduziert und auerdem das os beeintrchtigt . 
die wartezeit hatte in derselben studie eine geringere prognostische bedeutung mit einer tendenziell signifikanten reduktion der lokalen kontrolle bei einem postoperativen intervall von > 56 tagen [ 30 , 31 ]  . 
letztlich basiert die rationale hyperfraktionierter therapieprotokolle in der klinischen praxis auf der radiobiologischen bedeutung dieses zeitintervalls [ 3 , 4 , 11 , 17 , 19 , 20 , 28 ]  . 
 in der angloamerikanischen literatur als treatment package time bezeichnet , impliziert der begriff bereits den holistischen charakter dieses zeitraums und relativiert eine trennung in wartezeit und behandlungszeit in der adjuvanten situation . 
dies erklrt mglicherweise die kontroverse diskussion um die wartezeit und somit unsere eigene beobachtung , wonach die treatment package time der entscheidende parameter war : eine treatment package time 105 tage erwies sich als unabhngiger negativer prognosefaktor fr smtliche endpunkte . 
 [ 27 ] beeinflusste eine ott > 100 tage in einer retrospektiven untersuchung an 208 postoperativ bestrahlten patienten mit hno - tumoren das os sowie die lokale kontrolle signifikant negativ . 
daher , entsprechend dem asara - prinzip unntige verzgerungen zwischen operation und dem beginn der radiatio zu vermeiden , ebenso eine protraktion der radiotherapie [ 27 ]  . schlussfolgerung zusammenfassend muss daher aufgrund der eigenen daten und der diskutierten literatur nochmals die eingangs zitierte forderung von herrmann & baumann [ 15 ] unterstrichen werden , neben den strahlenbiologischen parametern einzelund gesamtdosis auch die zeitparameter zu bercksichtigen . 
strahlenund chemotherapie mssen die vorhandene tumorzellzahl mit ihren behandlungsverfahren so lange verdnnen , bis im idealfall die letzte klonogene tumorzelle vernichtet und damit dem tumor die rezidivmglichkeit genommen sowie heilung erreicht ist . 
 die toleranz des gesunden gewebes bei der lokoregionren strahlentherapie in unmittelbarer umgebung des tumors , bei der systemischen therapie der gesamtkrper limitiert hufig diese verdnnungsreihen klonogener zellen , so dass berlebende tumorklone wieder heranwachsen knnen . 
 den autoren dietl , schfer und klbl ist dafr zu danken , dass sie in einer analyse im eigenen krankengut nachweisen , dass bei hno - patienten nach der operation nicht nur verbliebene tumorzellen ( positive resektionsrnder und lymphknotenbefall ) , sondern neben bisher noch nicht erklrbaren parametern ( hmoglobinwert ! ) auch die zeit bis zum beginn einer postoperativen strahlentherapie einen signifikanten einfluss auf das gesamtberleben sowie die lokalrezidivbzw . 
 [ 4 , 5 ] in anlehnung an prinzipien des strahlenschutzes postuliert gilt , gehen die meinungen ber den weg zu dem allgemein anerkannten ziel , dass eine notwendige strahlenbehandlung baldmglichst beginnen muss , auseinander . 
dieses verfahren hat darber hinaus gegenber der schaffung weiterer kleiner strahlentherapieabteilungen den vorteil , dass es mit einer hheren zahl behandelter patienten in zentren mit zunehmender kompetenz und erfahrung einhergeht . 
 vielleicht hat sich seit dieser befragung , die annehmbar im jahre 2003 durchgefhrt wurde , und auch angesichts der heutigen wirtschaftlichen lage in deutschland der blickwinkel der deutschen radioonkologen geweitet , und der ruf nach dem staat , der neue technik bereitstellen soll , ist leiser geworden . 
12 urban & vogel kommentar tensivere ausnutzung der vorhandenen bestrahlungstechnik zu lsen ! sicher sind zur umsetzung dieser berlegungen in die praxis gemeinsame anstrengungen notwendig , um politik , personalabteilungen und personalrte von der notwendigkeit einer intensiven gertenutzung zum wohle der den radioonkologen anvertrauten patienten zu berzeugen . 
 [ 8 ] geforderte national call for ethical discourse on waiting lists in radiotherapy sollte von den deutschen radioonkologen jedenfalls am besten dadurch beantwortet werden , dass sie gemeinsam mit ihren mitarbeitern und den krankenhausverwaltungen darber nachdenken , wie zu verhindern ist , dass wartelisten fr eine strahlentherapie berhaupt erst entstehen knnen . 
eine voraussetzung fr einen mehrschichtbetrieb wird also immer sein , dass nicht vllig veraltete gerte zur verfgung stehen , sondern dass eine angemessene erneuerung der bestrahlungstechnik durch die krankenhaustrger oder privatinvestoren sichergestellt ist . 
the swedish council on technology assessment in health care ( sbu ) systematic overview of radiotherapy for cancer including a prospective survey of radiotherapy practice in sweden 2001 summary and conclusions . 
12 urban & vogel strahlentherapie und onkologie original article significant negative impact of adjuvant chemotherapy on health - related quality of life ( hr - qol ) in women with breast cancer treated by conserving surgery and postoperative 3 - d radiotherapy a prospective measurement razvan m . 
galalae1 , jan michel1 , jens ullrich siebmann2 , thomas kchler2 , kirsten eilf2 , bernard kimmig1 purpose : to prospectively assess health - related quality of life ( hr - qol ) in women after conserving surgery for breast cancer during / after postoperative 3 - d radiotherapy . patients and methods : 109 consecutively treated patients were analyzed . 
hr - qol was assessed at initiation ( t1 ) , end ( t2 ) , and 6 weeks after radiotherapy ( t3 ) using the eortc modules qlq - c30 / br23 . 
group i comprised 41 patients ( radiotherapy and adjuvant chemotherapy ) , group ii 45 patients ( radiotherapy and adjuvant hormonal therapy ) , and group iii 23 patients ( radiotherapy alone )  . 
 key words : breast cancer conformal 3 - d radiotherapy health - related quality of life hormonal therapy chemotherapy strahlenther onkol 2005 ; 181 : 64551 doi 10.1007 / s00066 - 005 - 1403 - x signifikanter negativer einfluss der adjuvanten chemotherapie auf die gesundheitsbezogene lebensqualitt ( lq ) bei brustkrebspatientinnen nach brusterhaltender operation und postoperativer 3 - d - radiotherapie . 
eine prospektive messung ziel : die gesundheitsbezogene lebensqualitt ( lq ) bei patientinnen mit einem mammakarzinom nach brusterhaltender operation sollte prospektiv whrend / nach postoperativer 3 - d - radiotherapie erfasst werden . 
die gesundheitsbezogene lq wurde mit hilfe der eortc - instrumente qlq - c30 und br23 bei beginn ( t1 ) , abschluss ( t2 ) und 6 wochen nach radiotherapie ( t3 ) gemessen . 
 die studienpopulation wurde in drei therapiegruppen stratifiziert : gruppe i mit 41 patientinnen ( radiotherapie und adjuvante chemotherapie ) , gruppe ii mit 45 patientinnen ( radiotherapie und adjuvante hormontherapie ) und gruppe iii mit 23 patientinnen ( alleinige radiotherapie )  . 
 1 clinic for radiation therapy ( radiooncology ) , university hospital schleswig - holstein , campus kiel , germany 2 department of general and thoracic surgery / reference center on quality of life in oncology , university hospital schleswig - holstein , campus kiel , germany . received : december 14 , 2004 ; accepted : august 1 , 2005 strahlenther onkol 2005 no . 
impact of adjuvant systemic therapy on quality of life in patients with breast cancer schlussfolgerung : die messung der gesundheitsbezogenen lq mit den eortc - instrumenten whrend / nach radiotherapie ist reliabel . 
 schlsselwrter : mammakarzinom konformale 3 - d - radiotherapie gesundheitsbezogene lebensqualitt hormontherapie chemotherapie introduction despite advances in medicine and beneficial lifestyle changes , breast cancer remains the most common malignancy in women worldwide . 
breast cancer accounts for about one in ten cancers and is the one most frequently affecting women in industrialized countries as well as in the developing world [ 25 ]  . 
however , disease - free survival drops in stage iii and is low in stage iv . breast - conserving therapy ( bct ) consisting of conservative surgery ( cs ) and postoperative radiotherapy ( rt ) has become the standard of care in early - stage breast cancer for more than a decade . 
a number of prospective randomized trials have reported no significant differences between bct and mastectomy for early - stage breast cancer in terms of locoregional control , distant metastases , and long - term survival [ 9 , 17 , 30 ]  . 
endocrine adjuvant treatment for primary breast cancer was also shown to be beneficial in terms of prolonged disease - free survival ( dfs ) and overall survival ( os ) especially in older women [ 5 ]  . 
however , the definitive role and type of adjuvant therapy are still a matter of debate not only for the older , but the entire breast cancer population . despite abundant information on survival and locoregional or distant recurrence rates in relation to the specific type of adjuvant treatment for early - stage breast cancer , knowledge concerning quality of life ( qol ) , cosmesis or late sequelae outcomes is very limited [ 1 , 23 , 26 ]  . 
 [ 2 ] examined several aspects of sexuality in different types of adjuvant treatment : goserelin alone , tamoxifen alone , goserelin ( zoladex ) and tamoxifen in combination versus no adjuvant endocrine therapy among premenopausal breast cancer patients with / without chemotherapy in a controlled clinical trial . 
patients undergoing chemotherapy had a higher level of sexual dysfunction than patients who received no systemic treatment . furthermore , there is evidence that cognitive dysfunction , fatigue , and menopausal symptoms may occur in women receiving adjuvant chemotherapy for breast cancer [ 29 ]  . the present study prospectively measured qol during the acute rt phase ( day 090 ) after cs for early breast cancer giving special attention to the impact of applied adjuvant systemic treatment . 
it refers to patients appraisals of their current level of functioning and satisfaction compared to what they perceive to be ideal [ 15 ]  . patients and methods patient population , tumor characteristics , and treatment 109 women with breast carcinoma , consecutively treated since 1997 , were analyzed . 
mean minimal resection margin was 0.5 cin the 105 invasive tumors , a complete axillary clearance ( level i / ii ) was performed ( in 22 cases using sentinel lymph node method )  . 
median dose in the breast was 50 gy , and in supraclavicular / axillary region 46 gy . definition of adjuvant therapy groups in order to achieve a more homogeneous patient cohort , the four dcis patients and the two patients who underwent a mastectomy were excluded from this analysis . 
group i included 39 patients ( 37.9% ; rt and adjuvant chemotherapy ) , group ii 45 patients ( 43.6% ; rt and adjuvant hormonal therapy with tamoxifen ) , and group iii 19 patients ( 18.5% ; rt alone )  . 
adjuvant systemic treatment was given in patients with one or more poor prognostic factors ( high t - stage , lymph node involvement , high grading , negative er and / or pr status ) , and started after surgery . 
 statistics the reliability ( internal consistency ) of both eortc qol instruments used was assessed for multi - item scales by calculating cronbachs coefficients , a statistic measure which represents the degree to which items within a single scale are associated with one another [ 4 ]  . 
 univariate analyses of variance ( anova ) and age - adjusted multivariate analyses of covariance ( mancova ) [ 3 ] were used to test the impact of adjuvant treatment on hr - qol . 
the mean design and instruments used for hr - qol assessment the eortc study group on quality of life has adopted a modular approach to qol assessment in cancer clinical trials . 
 we used the eortcs core instrument ( qlq - c30 ) , that has been designed to cover a range of qol issues relevant to a broad spectrum of cancer patients . 
the qlq - c30 version 2.0 [ 20 ] was supplemented by the more specific qlq - br23 to assess qol aspects of particular importance of breast cancer patients . the qlq - c30 core questionnaire contains five functional scales , a global health quality of life scale , and nine symptom scales . 
in the dimensions fatigue , pain , and breast symptoms an intermediate qol level was measured with a small increase of hr - qol impairments from t1 to t2 and a subsequent decrease to t3 . 
 perspective future functioning p hysical functioning r ole functioning e m otional functioning c ognitive functioning s ocial of life q uality im age b ody functioning s exual figure 1 . 
 however , the mean differences between patient groups ii ( rt and adjuvant hormonal therapy ) and iii were not statistically significant ( figure 1 and table 3 )  . 
in addition , chemotherapy was also associated with impaired hr - qol in the functional scales of qlq - c30 at t2 ( p = 0.051 ) and t3 ( p = 0.051 ) with marginal statistical significance . 
in the current study , the mean calculated cronbachs values ranged between 0.73 ( olq - c30 at t2 ) and 0.82 ( qlq - br23 at t2 )  . 
 group ii , t1 group ii , t2 group ii , t2 the functional scale means in dimensions role functioning , emotional functioning , cognitive functioning , social functioning , and global health status were impaired to a statistically significant degree in patient group i versus ii . 
in group iii patients , the scales appetite loss ( p < 0.01 ) , body image ( p < 0.01 ) , and sexual functioning ( p < 0.01 ) showed statistically significant improvements of qol from t1 to t3 as well . 
impact of adjuvant systemic therapy on quality of life in patients with breast cancer the mainstay of care for patients with early - stage breast cancer has become local therapy , consisting of cs and rt [ 6 , 16 , 31 ] , along with adjuvant systemic therapy , which can include chemotherapy , hormonal therapy , or a combination of these treatments . 
anova analyses revealed statistically impaired hr - qol in five functional scales from nine and in five symptom dimensions out of twelve in chemotherapy patients ( group i ) versus hormonal therapy ( group ii )  . 
in addition , chemotherapy was associated with the lowest qol scores in all functional domains versus hormonal therapy or rt alone , and chemotherapy patients did not recover from t1 to t3 ( longitudinal analysis )  . 
by contrast , patients receiving hormonal therapy had higher qol scores with no statistically significant differences versus those measured in patients undergoing rt alone , and they recovered in eight qol dimensions from t1 to t3 . 
in the multivariate analysis of covariance ( mancova ) , chemotherapy was a statistically significant predictor of low hr - qol in the symptom scales and the breast module functional scales . 
studying in detail the pattern of hr - qol impairments caused by chemotherapy , it is remarkable , that the dimensions role functioning ( mean score 45.73 ) , emotional functioning ( mean score 49.50 ) , sexual functioning ( mean score 33.33 ) , future perspective ( mean score 32.36 ) , fatigue ( mean score 59.12 ) , and insomnia ( mean score 53.42 ) showed marked qol deprivations . 
 [ 7 ] reported results of a prospective field study with 988 breast cancer patients also suffering from significantly worse emotional functioning , fatigue , pain and sleeplessness in comparison with 327 female rectal cancer patients . 
patients receiving a combination of hormonal and rt or rt only recovered in the initially impaired hr - qol domains from treatment initiation ( t1 ) to the end of acute treatment phase ( 3 months later , at t3 )  . 
 strahlentherapie und onkologie original article organ - sparing treatment in muscle - invasive bladder cancer jrgen dunst1 , andrea diestelhorst1 , reinhard khn2 , arndt - christian mller1 , hans - jrg scholz3 , paolo fornara4 background and purpose : organ - sparing treatment of bladder cancer by a trimodality approach is feasible and effective . 
 patients and methods : in the period from june 1995 through december 2003 , 68 patients ( 64 males , four females ) with urothelial bladder cancer were treated with curative intent . 
34 patients received concurrent cisplatin - based chemotherapy ( 25 mg / m2 on days 15 and 2933 ) , and patients with impaired renal function were either treated with irradiation alone ( n = 7 ) or received paclitaxel as alternative to cisplatin in a phase ii protocol or on an individual decision ( n = 27 )  . 
cr rates were not significantly correlated to t - category ( cr : 24 / 32 t2 , 9 / 19 t3 , and 9 / 16 t4 tumors ) or clinical nodal status . 
patients with non - radical resection and macroscopic residual tumor ( r2 resection ) achieved a cr in only 39% ( 12 / 31 ) ; this figure was significantly lower as compared to patients with radical r0 tur - bt ( cr : 15 / 16 , 94% , p = 0.013 ) furthermore , age and preexisting anemia had no impact on response . 
 key words : bladder cancer radiotherapy chemotherapy strahlenther onkol 2005 ; 181 : 6327 doi 10.1007 / s00066 - 005 - 1416 - 5 organerhaltende behandlung des muskelinvasiven harnblasenkarzinoms hintergrund und ziel : die organerhaltende behandlung des lokal fortgeschrittenen harnblasenkarzinoms hat sich in prospektiven studien als effektive manahme erwiesen . 
in dieser studie werden retrospektive daten der eigenen klinik an einem ungnstig selektionierten kollektiv primr nicht zystektomiefhiger patienten vorgestellt . patienten und methodik : von juni 1995 bis dezember 2003 wurden an der eigenen klinik 68 patienten ( 64 mnner , vier frauen ) mit urothelkarzinomen der harnblase in kurativer intention mit einer radiotherapie oder radiochemotherapie behandelt . 
die radiotherapie erfolgte in konventioneller fraktionierung ( fnfmal wchentlich 1 , 8 gy ) bis zu einer gesamtdosis von 50 , 4 gy an blase und lymphknoten ; die ganze blase wurde bis 54 gy ( r0 - tur ) bzw . 
34 patienten erhielten eine simultane chemotherapie mit cisplatin ( 25 mg / m2 an den tagen 15 und 2933 ) , und patienten mit eingeschrnkter nierenfunktion erhielten entweder eine alleinige strahlentherapie ( n = 7 ) oder wurden im rahmen eines phase - ii - protokolls mit paclitaxel als ersatz fr cisplatin behandelt ( n = 27 )  . 
die mediane nachbeobachtungszeit betrug 34 monate ( spanne 2104 monate )  . 1 department of radiotherapy , martin luther university halle - wittenberg , germany , 2 department of urology , martha maria hospital halle , germany , 3 department of urology , asklepios hospital weienfels , germany , 4 department of urology , martin luther university halle - wittenberg , germany . 
die klinischen cr - raten waren unabhngig von der initialen t - kategorie ( cr : 24 / 32 t2 - , 9 / 19 t3und 9 / 16 t4 - tumoren ) und dem klinischen nodalstatus . 
patienten mit nicht - radikaler tur und makroskopischem resttumor ( r2 - tur ) erreichten in 39% eine cr ( signifikant verschieden von patienten mit r0 - tur )  . 
die berlebensrate aller patienten lag bei 45% nach 5 jahren , und die berlebensraten in abhngigkeit von der t - kategorie betrugen 62% fr t2 , 43% fr t3 und 19% fr t4 ( p = 0 , 015 )  . 
 schlsselwrter : blasenkarzinom radiotherapie chemotherapie introduction organ preservation is feasible and effective in patients with muscle - invasive bladder cancer and offers an attractive alternative to radical cystectomy which has been considered the standard of care for this disease . 
optimal results in terms of organ preservation are achieved , if radiotherapy is embedded in a multimodal approach including transurethral resection ( tur ) , irradiation plus concurrent cisplatin chemotherapy and salvage cystectomy for nonresponding or recurrent tumors [ 4 , 8 , 9 , 1618 , 21 , 22 , 24 ]  . 
 a subset of patients with advanced bladder cancer is not suitable for radical cystectomy due to patient ( age , comorbidity ) or tumor - related factors ( local non - resectability )  . 
on the other hand , the prognosis of locally advanced bladder cancer not only depends on tumor - related parameters , but also on patient - related factors such as performance status , age , and pretreatment hemoglobin level or sedimentation reaction ( bsr ) [ 4 ]  . 
however , this subgroup of patients , according to data in the literature , can be cured by radiotherapy or radiochemotherapy with acceptable long - term survival figures [ 18 , 19 ]  . 
 patients and methods patient population in the period from june 1995 through december 2003 , 68 patients ( 64 males , four females ) with muscle - invasive urothelial bladder cancer were treated in our department with curative intent . 
24 patients treated in the same period who had non - urothelial histology ( n = 4 ) , metastatic disease ( n = 8 ) or received low - dose palliative irradiation for symptoms ( n = 12 ) were excluded . 
thus , the majority of patients in this analysis are patients with either contraindications to major surgery ( due to advanced age or comorbidity ) or locally advanced tumors which were considered non radically resectable . 
after establishing the histological diagnosis of invasive or recurrent urothelial cancer , further staging procedures included a computed tomography ( ct ) or magnetic resonance imaging ( mri ) of the pelvis and abdomen to detect extravesical spread and / or enlarged regional or paraaortic lymph nodes , ct or ultrasound examination of the liver to exclude liver metastases , a chest x - ray or thoracic ct to exclude lung metastases , and laboratory work - up . 
in case of superficial or t2 tumors , a second tur - bt was routinely performed to achieve a complete resection , if the first tur - bt was non - radical . 
organ preservation in bladder cancer radiotherapy all patients underwent ct - based treatment planning ( mainly three - dimensional planning ) plus treatment simulation at a simulator with instillation of contrast medium in bladder and rectu radiotherapy was administered with 10to 15 - mv photons via four individually shaped fields in conventional fractionation ( five fractions of 1.8 gy per week , doses refer to the icru reference point )  . 
the regional lymphatics were included up to 50.4 gy in the majority of patients up to the aortic bifurcation ; however , the upper field border was chosen lower in patients with advanced age in case of clinically uninvolved nodes ( cn0 ) on an individual decision to improve treatment table 1 . 
the whole bladder received a boost up to 54 gy in case of r0 resection or 59.4 gy in case of non - radical tur - bt ( r12 )  . chemotherapy concurrent cisplatin - based chemotherapy was routinely used in all patients except in case of contraindications . 
the standard regimen was cisplatin 25 mg / m2 per day on 5 consecutive days in the 1st and 5th week of radiotherapy ( days 15 and 2933 ) as published recently [ 17 ] , and 34 patients ( 50% ) were treated according to this regimen . 
patients with impaired renal function were either treated with irradiation alone ( n = 7 ) or received paclitaxel as alternative to cisplatin in a phase ii protocol or on an individual decision ( n = 27 ) ; the results of this study have been presented recently [ 3 ]  . 
in this analysis , only 46 patients underwent restaging tur - bt , because the others were considered inoperable due to medical reasons and a consequence of the restaging tur in terms of decision - making for further procedures was not expected ( n = 19 ) or patients progressed clinically immediately after radiochemotherapy ( n = 3 )  . 
survival curves were compared with the log - rank test . results completeness of tur - bt and t - category 16 patients ( 23% ) had a microscopically complete tur , and further twelve patients ( 18% ) had an r1 resection . 
significant association ( p = 0.002 , pearsons 2 - test ) between clinical t - category and radicality of transurethral resection in muscle - invasive tumors ( t 2 )  . 
signifikanter zusammenhang ( p = 0 , 002 , 2 - test nach pearson ) zwischen klinischer t - kategorie und radikalitt der transurethralen resektion bei muskelinvasiven tumoren ( t 2 )  . 
a histologically confirmed complete remission ( cr ) on restaging tur - bt was observed in 40 patients ( 59% of all patients , 87% of patients who underwent restaging tur - bt )  . 
for muscle - invasive cancers , a marked difference between tumors with invasion limited to the muscle wall ( ct2 ) and extravesical spread ( ct34 ) was noted ( figure 1 )  . 
so far , the following long - term sequelae have been observed : reduced bladder capacity ( 5 / 47 evaluable patients ) , grade 12 chronic cystitis ( 4 / 64 patients ) , grade 12 mild enteritis ( 3 / 64 patients ) , one hydronephrosis due to fibrosis , one urethral stricture , and mild renal insufficiency after cisplatin chemotherapy in two ct34 local and systemic control in eleven patients , disease progression or relapse was observed . 
systemic metastases ( local recurrence ) occurred in nine patients ( lung n = 1 , bone n = 1 , brain n = 2 , multiple sites n = 5 )  . 
 conclusion discussion the efficacy of an organ - sparing approach including transurethral surgery , irradiation and simultaneous chemotherapy for locally advanced bladder cancer has been demonstrated in a variety of large prospective studies and populationbased analyses [ 1 , 2 , 4 , 5 , 79 , 11 , 1419 , 21 , 22 , 24 ]  . 
although randomized trials are missing , the synopsis of the currently available data suggest that this multimodal approach does not compromise survival as compared to radical cystectomy and yields preservation of a functioning bladder in the vast majority of patients . 
the survival figures reported in these series are at least comparable , if not better than survival figures of the best contemporary european and us cystectomy series [ 14 , 20 ]  . 
 our data , in general , support those in the literature and further emphasize the high potential of radiochemotherapy for locally advanced bladder cancer , although the analysis in this paper has some limitations . 
the most striking difference as compared to other series with an organ - sparing approach is the fact that none of our patients received a salvage cystectomy , although salvage surgery was part of the treatment concept . 
retrospective analyses suggest that molecular markers such as apoptotic index or proliferation markers may help to identify patients who may benefit most from an organ - sparing approach [ 23 ]  . 
tur plus simultaneous radiochemotherapy plus selected salvage cystectomy is probably the optimal treatment for these patients , and the overall survival figures which have been reported in this and other investigations are robust and at least equal to current cystectomy series . 
 strahlentherapie und onkologie original article imrt with compensators for head - and - neck cancers treatment technique , dosimetric accuracy , and practical experiences henning salz , tilo wiezorek , marcel scheithauer , michael schwedas , jochen beck , thomas georg wendt1 background and purpose : with three - dimensional conformal intensity - modulated radiotherapy ( 3d - c - imrt ) a heterogeneous dose distribution can be achieved in both planning treatment volume and in adjacent normal tissues and organs to be spared . 
 patients and methods : from january 2002 to april 2004 , 24 patients with head - and - neck cancers were treated with 3d - c - imrt using tin - wax compensators . 
high - dose volume was irradiated with 6070 gy ( median 66 gy ) , low - dose volume with 4854 gy ( median 52 gy ) administered by a standardized seven - portal coplanar beam arrangement . 
 conclusion : the described method offers facilities for a good dose coverage of irregular target volumes with different prescribed doses and a considerable dose reduction in adjacent organs at risk . 
 key words : intensity - modulated radiotherapy compensators dose coverage quality assurance treatment delivery time strahlenther onkol 2005 ; 181 : 66572 doi 10.1007 / s00066 - 005 - 1402 - y imrt mit kompensatoren fr kopf - hals - tumoren . 
bestrahlungstechnik , dosimetrische genauigkeit und praktische erfahrungen hintergrund und ziel : mit der dreidimensionalen konformalen intensittsmodulierten strahlentherapie ( 3d - c - imrt ) kann eine heterogene dosisverteilung sowohl im planungszielvolumen als auch in benachbartem normalgewebe und zu schonenden organen erreicht werden . 
 patienten und methodik : von januar 2002 bis april 2004 wurden 24 patienten mit einem hno - tumor mit der 3d - c - imrt - technik mit zinn - wachs - kompensatoren behandelt . 
die dosisverordnung schloss einen gleichzeitigen integrierten boost edas hochdosisvolumen wurde mit 6070 gy ( median 66 gy ) , das niedrigdosisvolumen mit 4854 gy ( median 52 gy ) mit einer koplanaren standardisierten sieben - felder - technik behandelt . 
 ergebnisse : fr 21 von 24 patienten reduzierte die 3d - c - imrt mit zinn - wachs - kompensatoren die mediandosis fr eine glandula parotidea auf < 30 gy . 
die dosis des patienten auerhalb des bestrahlten volumens war gegenber offenen 1 department of radiotherapy , radiologic clinic , university hospital jena , germany . received : december 14 , 2004 ; accepted : july 13 , 2005 strahlenther onkol 2005 no . 
 schlsselwrter : intensittsmodulierte strahlentherapie kompensatoren dosiserfassung qualittssicherung bestrahlungszeit introduction since their introduction , modulators have been mostly used to generate a uniform dose distribution on a specified plane inside of the patient . 
by contrast , for three - dimensional conformal intensity - modulated radiotherapy ( 3d - cimrt ) a compensator is used as a beam intensity modifier to achieve the photon fluence distribution generated by the inverse planning procedure [ 6 , 15 , 20 ]  . 
 patients and methods treatment planning for the treatment planning procedure and dose calculation the three - dimensional treatment planning system helax - tms ( nucletron b.v. , veenendaal , the netherlands ) , a modulation - matrix software tool modifix ( bebig isotopenund medizintechnik , berlin , germany ) and , since 2004 , the imrt application konrad ( siemens ocs , heidelberg , germany ) were used . 
the following total dose prescriptions were made : high - dose planning target volume ( ptv ) : 6070 gy ( median 66 gy ) , low - dose ptv : 4854 gy ( median 52 gy ) , median dose at one parotid gland : 26 gy . 
the maximum thickness of a compensator amounts to 40 m pretreatment quality assurance the pretreatment quality assurance encompassed the planning system , the accuracy of the compensator manufacturing strahlenther onkol 2005 no . 
imrt with compensators for head - and - neck cancers the checks of the milling process were carried out manually and included accuracy of the depth , position of the central axis , and the divergence . 
 for dosimetric quality assurance , line doses in water ( ionization chambers , ptw freiburg , germany ) and two - dimensional dose distributions ( film kodak x - omat and edr2 , kodak and array seven29 , ptw freiburg ) are measured [ 28 ]  . 
the analysis of two - dimensional distributions was realized with an in - house developed software [ 31 ]  . the checks of the planning system were performed with even and extremely shaped compensators . 
finally , for an anthropomorphic phantom a complete treatment plan was calculated and dose distribution achieved was compared with that measured with ionization chambers and thermoluminescent rods calibrated specifically for compensators . 
these measurements had been replaced by at least two point dose measurements per field with ionization chambers in a flat phantothe implementation of the software verisoft@ ( ptw freiburg ) allowed for analysis of film measurements and dosimetric quality assurance with high spatial resolution . 
 after getting confidence in the accuracy and reproducibility of different steps described above , for routine use of compensators the quality assurance program comprises : ( 1 ) manual check of depth and position during manufacturing a compensator ; ( 2 ) an x - ray picture ( 6 mv ) with film , later with a phosphorizing plate to assure that a compensator is not erroneously used with a wrong field ; ( 3 ) one point dose measurement in the high - dose region on a three - dimensional phantom after recalculation . 
die verschriebene dosis betrgt 66 gy ( = 100% , hochdosis - planungszielvolumen ) und 52 , 8 gy ( niedrigdosis - planungszielvolumen ) die 95% - isodosislinie umschreibt das planungszielvolumen ; die maximaldosis des rckenmarks betrgt ca . 
imrt with compensators for head - and - neck cancers the treatment delivery time is the time elapsed from the beginning of the first field irradiation to the end of the last field irradiation . 
we analyzed the mean value of fraction 6 , 12 , and 18 of every patient irradiated in the lantis treatment record & verify system ( siemens medical systems )  . patient accrual in a pilot phase selected patients with advanced squamous cell cancer of the head and neck ( bilateral ptv , curative intention , ptv extension to the base of scull ) were irradiated using the 3d - c - imrt performed with compensators . 
 compensator ( tin granules + wax ) ( mcp96 ) compensator im range ( photons 6 mv ) inverse planning manual changes of fluence profile after inverse planning yes coverage high - dose ptv ( d95 , d90 ) coverage low - dose ptv ( d95 , d90 ) dose contralateral parotid gland monitor units per 2 gy ( separate fields for lower neck not included ) additional block shielding 45100% helax - tms median 87% / 96% median 88% / 96% median 26.3 gy 263314 yes ( recommended ) 16100% konrad median 93% / 99% median 89% / 96% median 23.8 gy 343436 results treatment planning table 1 shows details and the results of the treatment planning procedure for 24 patients treated with tin - wax compensators . 
 the checks of the milling process reveal that the shape of the compensators profile can be manufactured with an accuracy of depth of 0.5 min any case , strahlenther onkol 2005 no . 
both materials allow a sufficient dose distribution , but with mcp96 the coverage of the planning target volume and the dose sparing of the left parotid gland can be improved . 
 finally , we carried out a final check with an anthropomorphic phantothis included treatment planning , compensator manufacturing , quality assurance , and irradiation of the phantoinside of the phantom thermoluminescent rods had been placed and analyzed . 
 the dosimetric quality assurance in clinical routine was carried out with line dose measurements , later with radiographic films in a flat phantoit can be summarized , that deviations amount to 3% in the high - dose region , except for dose gradients . 
for small target volumes it is possible that one compensator contains the fluence profiles of two asymmetric fields , so the treatment room must be entered after two consecutive portals have been irradiated . 
 the additional dosage corresponds to the monitor units : with tin - wax compensators we calculated between 263 and 326 mu per 2 gy ; with compensators consisting of mcp96 between 343 and 436 mu are needed ( see table 2 )  . 
 discussion according to other methods of 3d - c - imrt ( overview [ 28 ] , clinical and biological examples [ 8 , 11 , 26 ] ) , with compensators a prescribed dose distribution can be achieved in both irregular ptvs and in adjacent normal tissues and organs to be spared . 
a more detailed comparison between 3d - c - imrt with compensators and with segmental multileaf collimator imrt technologies is presented in [ 4 ] and [ 5 ]  . 
a detailed analysis showed that underdosage of high - dose volumes mainly occurs in the built - up region underneath the skin and to a lesser extent at their borders to the surrounding low - dose volume . 
 using the inverse treatment tool of helax - tms including manual improvements of the fluence profiles , the procedure was very time - consuming , but the obtained dose distribution resulted both in a better dose coverage of the target volumes and better dose sparing of one parotid gland in comparison with non - imrt treatment plans . 
since the implementation of a tool especially for inverse treatment planning in 2004 ( konrad ) , high - quality dose distributions have been achieved without manual changes of the fluence profiles . 
abweichungen zwischen gemessenen und berechneten punktdosiswerten an 21 punkten in der hochdosisregion eines kopf - hals - bestrahlungsplans , bestrahlt an einem phantodie dosismessungen wurden mit thermolumineszenzdetektoren ( 95% - vertrauensintervall : 1 , 0% ) durchgefhrt . 
both materials can be recommended for compensator fabrication , the spatial resolutions of 7 mm ( tin - wax , source - compensator - distance = 41.3 cm ) and 5 mm ( mcp96 , source - compensator - distance = 56.5 cm ) are sufficient for imrt . 
we expect this time will diminish with further experience . for 24 patients with head - and - neck cancer treated with compensators consisting of tin granulate embedded in wax , 90% of the ptvs were encompassed by the 95% isodose . 
 at present , the compensator technology is not only used for imrt in the head - and - neck region , but also for cancers of salz h , et al . 
 conclusion quality assurance in routine because of the static nature of compensators , the quality assurance program with compensators is easy to realize , for instance with x - ray pictures with only few monitor units , measurements of line dose in water and the analysis of the depth profile during compensator manufacturing . 
so for extreme cases is was measured , that the deviation of film x - omat and edr2 is approximately 5% between small ( 34 mm ) and large ( 3035 mm ) compensator thicknesses of mcp96 . 
because of a fast but safe quality assurance management system , it is recommended to prefer methods based on more energy - independent detectors ( ionization chambers , special two - dimensional arrays , film gafchromic ebt [ isp ] ) or to take nonlinear fluence dependence of detectors into account [ 18 , 30 ]  . 
 the irradiated monitor units amount to approximately 300 mu ( 263326 mu , see table 1 ) for tin - wax compensators and about 400 mu ( 343436 mu , see table 2 ) for mcp96 compensators . 
 compared with open fields the dose outside the target volume is increased and comparable with a physical wedge of 1530 ( see figure 6 ) , which seems acceptable for patient treatments . 
open field ( open squares ) , physical wedge 30 ( open triangles up ) , physical wedge 45 ( open triangles down ) , clinically used tin compensator ( filled circles ) , and mcp96 compensator with maximum depth of 4 cm ( filled squares ) are compared . 
verglichen werden offenes feld ( offene quadrate ) , fester 30 - keil ( offene dreiecke , spitze nach oben ) , fester 45 - keil ( offene dreiecke , spitze nach unten ) , klinisch eingesetzter zinnkompensator ( gefllte kreise ) und mcp96 - kompensator mit der maximaltiefe von 4 cm ( gefllte quadrate )  . 
 strahlentherapie und onkologie current discussion late effects and cosmetic results of conventional versus hypofractionated irradiation in breastconserving therapy fabian fehlauer , silke tribius , winfried alberti , dirk rades1 background and purpose : breast irradiation after lumpectomy is an integral component of breast - conserving therapy ( bct )  . 
 patients and methods : 129 breast cancer patients ( pt12 pn01 cm0 ) were irradiated between 09 / 1992 and 08 / 1994 with either a 22 - day fractionation schedule ( 2.5 gy to 55 gy , 4 / week , n = 65 ) or with a conventional fractionation schedule ( 28 days , 2.0 gy to 55 gy , 5 / week , n = 64 ) , both without additional boost . 
late toxicity , assessed according to the lent - soma criteria , and cosmetic outcome , graded on a 5 - point scale , were evaluated after a median of 86 months ( range 7294 months ) in tumor - free breast cancer patients . 
 key words : breast cancer radiotherapy hypofractionation late toxicity lent - soma cosmesis strahlenther onkol 2005 ; 181 : 62531 doi 10.1007 / s00066 - 005 - 1404 - 9 sptnebenwirkungen und kosmetik nach konventioneller versus hypofraktionierter bestrahlung im rahmen der brusterhaltenden therapie des mammakarzinoms hintergrund und ziel : die adjuvante bestrahlung der brust nach operation ist ein integraler bestandteil der brusterhaltenden therapie ( bet )  . 
die vorliegende untersuchung vergleicht zwei unterschiedliche fraktionierungsschemata in bezug auf diese endpunkte . patienten und methodik : 129 patientinnen mit brustkrebs ( pt12 pn01 cm0 ) wurden zwischen 09 / 1992 und 08 / 1994 entweder mit einem 22 - tage - fraktionierungsschema ( 2 , 5 gy bis 55 gy , 4 / woche , n = 65 ) oder mit einem 28 - tage - fraktionierungsschema ( 2 , 0 gy bis 55 gy , 5 / woche , n = 64 ) , jeweils ohne boost , behandelt . 
late effects after hypofractionated rt in bct introduction with the good prognosis of breast - conserving therapy ( bct ) , an acceptable rate of long - term radiation sequelae with satisfactory cosmesis has become an important issue of successful therapy . 
for external - beam radiotherapy , it has been sufficiently proven that the probability of late side effects depends on , among other factors , the fractionation , interfraction interval , total dose , and the volume irradiated , as well as individual patient factors [ 2 , 4 , 5 , 31 ]  . 
 clinical experience and previous studies have revealed a heterogeneous spectrum of late toxicity following bct such as breast pain , breast edema , fibrosis , atrophy , skin ulcerations , lung fibrosis , rib fractures , and others [ 15 , 16 , 21 , 32 ]  . 
 between 1988 to 1993 at the university of hamburg , all patients treated with bct received a 22 - day fractionation schedule , 2.5 gy per fraction to a total dose of 55 gy , four fractions per week . 
the evidence that fraction size of > 2 gy is associated with more late toxicity , led to a change to a 28 - day fractionation schedule ( 2.0 gy to 55 gy , five fractions per week ) in august 1993 . 
 the aim of this study was to evaluate the long - term toxicity according to the lent - soma criteria and long - term cosmetic results from the radiation oncologists perspective in 129 cured women who underwent bct treated with 6 - mev photons to a total dose of 55 gy , either hypofractionated or conventionally fractionated . 
 patients and methods patients between 1988 and 1995 , 2 , 365 women with early - stage breast cancer were irradiated after breast - conserving surgery ( lumpectomy ) at the university hospital hamburg - eppendorf , germany . 
 women received bct if they fulfilled the following criteria : ( a ) pathologic stage i ( pt1 pn0 m0 ) or stage ii ( pt2 pn0 m0 , pt1 pn1 m0 , pt2 pn0 cm0 ) , ( b ) compatibility between tumor size and remaining breast allowing an acceptable cosmetic result . 1 , 668 patients ( 71% ) were eligible for follow - up examination ( alive and known address )  . 
 all known long - term survivors were invited at least twice by mail for a follow - up visit focusing on late toxicity , 545 women ( 33% ) accepted . 
 to record the incidence of normal - tissue effects following radiotherapy , a standardized treatment planning and delivery for a homogeneous dose distribution , and close observation interval are required . 
to obtain patient populations with comparable follow - up , we chose to evaluate those patients who were treated close to the period , where the treatment regimen was changed . 
 therefore , only patients with comparable follow - up interval ( treated between september 1992 and august 1994 , irradiated with 6 - mev photons , no recurrence ) were defined as the definitive study group ( inclusion criteria )  . 
 two different fractionation schedules were applied over the years : ( a ) 19881993 , 2.5 gy 4 / week to 55 gy : 1 , 598 patients were treated predominantly with 6 - mv photons to a dose of 55 gy ( fractionation : 2.5 gy , 4 days / week )  . 
 ( b ) 19941995 , 2.0 gy 5 / week to 55 gy : 767 patients were treated using megavoltage to a total dose of 54 or 55 gy , in fractions of 2.0 gy 5 days / week . 
 a direct comparison of the results of the two treatment groups ( a ; b ) is not appropriate because of different follow - up intervals , beam energy , and patient numbers . 
out of 169 patients , 129 ( 75% ) met the inclusion criteria and two study groups were defined ( table 1 )  . follow - up and assessment a first baseline mammogram was obtained 68 weeks following radiotherapy . 
 patients were routinely monitored up to 5 years following radiotherapy : our follow - up policy consisted of a clinical examination and a mammogram every 612 months for the first 5 years followed by yearly mammograms . 
 between february 2000 and october 2001 patients underwent a physical examination : many of them were assessed by two physician staff members to synchronize the objective grading to optimize the interobserver reliability . 
cosmesis was determined by the examining physician according to a 5 - point scale ( table 2 ) based on the degree of multiple findings [ 22 , 23 ]  . 
 arm edema was quantified by measuring the difference in circumference of the ipsilateral and contralateral arm using standard anatomic criteria ( 15 cm above and 10 cm below the olecranon )  . 
 grade 1 grade 2 grade 3 grade 4 subjective objective management analytic occasional and minimal , hypersensation , pruritus asymptomatic barely palpable increased density < 1 cm2 24 cm increased circumference pain edema fibrosis telangiectasia lymphedema , arm atrophy / retraction 1025% ulcer pain edema lymphedema , arm atrophy ulcer photographs tape measure mammogram ct / mri epidermal only , 1cm2 occasional nonnarcotic intermittent and persistent and intense tolerable symptomatic secondary dysfunction definitely increased very marked density , density and firmness retraction and fixation 14 cm2 > 4 cm2 > 46 cm increased > 6 cm increased circumference circumference > 2540% > 4075% dermal , > 1 cm2 subcutaneous regular nonnarcotic regular narcotic medical intervention elevate arm , elastic compression wrapping , stocking intensive physiotherapy medical intervention surgical intervention , wound debridement assessment of skin changes assessment of breast size and arm diameter assessment of skin thickness and density assessment of size , fat atrophy , fibrosis refractory and excruciating useless arm whole breast bone exposed , necrosis surgical intervention surgical intervention / mastectomy surgical intervention / amputation surgical intervention / mastectomy surgical intervention / mastectomy y / n date : y / n date : y / n date : y / n date : for statistical analysis . 
 lent - soma group a : 2.5 gy ( n = 65 ) group b : 2.0 gy ( n = 64 ) pain breast edema fibrosis telangiectasia arm edema atrophy ulcer 0 1 3 5 7 1 2 1 4 3 1 3 2 5 0 1 1 4 4 ethics results all patients received verbal and written information regarding the study . 
 65 patients irradiated 4 / week with 2.5 gy per fraction ( group a ) , and 64 patients irradiated 5 / week with 2.0 gy per fraction ( group b ) , both to a total dose of 55 gy , met the criteria and could be analyzed ( table 4 )  . 
 severe breast pain , as the only subjective lent - soma criterion , and breast edema , fibrosis , telangiectasia , and atrophy , as objective criteria , were rare late sequelae ( table 4 )  . 
late effects after hypofractionated rt in bct observed late reaction in group a : half of the women presented with a definitely increased density or very marked density of the irradiated breast ( grade 2 : 56% , 37 / 65 patients ) , whereas in group b ( 2.0 gy ) grade 2 fibrosis occurred in only 16% of women ( 10 / 64 )  . 
 the majority of women treated with 2.0 gy did not develop arm edema ( 94% , 60 / 64 ) , whereas in 15% of women ( 10 / 65 ) the circumference of the arm differed by > 2 cm ( grade 2 ) following 2.5 - gy single dose . 
 only fraction size , not tumor size , additional chemotherapy nor endocrine therapy , was a significant factor on univariate analysis for the development of fibrosis grade 2 / 3 , atrophy grade 2 / 3 , and poorer cosmesis . 
 discussion radiotherapy , with curative and palliative intention , is known to be a highly effective and well - tolerated approach in the management of breast cancer [ 1 , 6 , 8 , 9 , 13 , 14 , 2428 ]  . 
according to the eqd2 , the hypofractionation schedule causes a biological effect of eqd2 = 62 gy ( for / = 2 gy ) to the irradiated breast [ 18 ]  . 
 most of the studies on late toxicity after bct are based on follow - up periods not exceeding 5 years , due to the fact that it is assumed by radiation oncologists that all late effects will have occurred . 
 even if a high proportion of patients would be affected by treatment - related late morbidity , they may actually have lived for a number of years without or with mild symptoms from toxicity . 
 [ 17 ] followed breast cancer patients up to 30 years after aggressive post - mastectomy radiotherapy and found that the incidence of late morbidity was still increasing over time . 
furthermore , an increase of the dose per fraction was reported to be much more relevant for the development of fibrosis than an increase in the total dose [ 11 ]  . 
 a recently published randomized study with 1 , 234 women from canada compared 42.5 gy in 16 fractions over 22 days to 50 gy in 25 fractions and found no differences in cosmesis or survival at 5 years . 
it was strongly suggested that cosmetic results using a fraction size of 2.5 gy are as good as with 1.82.0 gy per fraction , when modern radiotherapy techniques are employed and the total dose to the breast is limited to 4050 gy [ 33 ]  . 
 in our series , the cosmetic outcome in patients using a higher dose per fraction ( 2.5 gy ) can be directly compared to the standard fractionation group ( 2.0 gy ) due to the equivalent follow - up periods and technical aspects ( beam quality , treatment volume )  . 
the major limitation of that study is the fact , that the follow - up period is far too short and the variation of the follow - up is much too high ( range 7121 months ) to allow final conclusions . 
 the extraordinarily good prognosis of patients who underwent bct and limited therapeutic approaches in the management of symptomatic late sequelae implicate that the risk of severe late morbidity must be kept at a very low level . 
 in our study population , the total proportion of grade 3 complications , either of objective or of subjective lent parameters , was 6% ( 2.0 gy ) versus 43% ( 2.5 gy ) , which presents a sevenfold increase of toxicity . 
 however , given the history of long - term high morbidity of hypofractionation applied in the past with curative intent , it would seem premature to reintroduce this technique without randomized trial involving many patients . 
mcbride3 , heidi stranzl1 , ulrike prettenhofer1 , johannes fruhwirth4 , johann poschauko1 background : lymphatic drainage from the surgical wound is an uncommon but challenging complication of surgical intervention . 
 patients and methods : 17 patients ( 19 fistulas ) with lymphorrhea following vena saphena harvesting ( n = 7 ) , femoropopliteal bypass ( n = 3 ) , varicose vein surgery ( n = 2 ) , hip arthroplasty ( n = 3 ; five fistulas ) , shunt surgery ( n = 1 ) , and piercing ( n = 1 ) were referred for external radiotherapy . 
 conclusion : radiotherapy represents an efficacious and economical treatment option in cases of persistent lymphorrhea and is able to reduce the risk of secondary infection , to decrease the duration of hospitalization , and to reduce overall costs for the individual patient . 
 key words : radiotherapy lymphatic fistulas lymphorrhea surgery complications radiobiology strahlenther onkol 2005 ; 181 : 6604 doi 10.1007 / s00066 - 005 - 1393 - 8 lymphfisteln : verschluss durch niedrigdosierte strahlentherapie hintergrund : persistierende sezernierende lymphfisteln stellen eine seltene , aber fr den patienten belastende komplikation chirurgischer eingriffe dar . 
auslsende ursachen fr die fistelbildung waren : entnahme der vena saphena magna ( n = 7 ) , anlegen eines femoropoplitealen bypass ( n = 3 ) , erneuter wechsel einer totalendoprothese ( tep ) der hfte ( n = 3 ; fnf fisteln ) , varizenoperation ( n = 2 ) , anlegen eines dialyseshunts ( n = 1 ) bzw . 
je nach tiefenausdehnung der fistel wurden die patienten mit orthovolttherapie ( n = 12 ) , elektronen ( 411 mev ; n = 2 ) oder photonen ( 8 mv ; n = 3 ) bestrahlt . 
es fiel auf , dass bei neun von zehn patienten , die mit sehr niedrigen einzeldosen ( 0 , 30 , 5 gy ) und gesamtdosen von 3 gy bestrahlt wurden , eine komplette obliteration der lymphfistel beobachtet werden konnte . 
 1 department of radiation oncology , medical university of graz , austria , 2 department of radiation oncology , section radiobiology , vu university medical center , amsterdam , the netherlands , 3 roy e . 
coats research laboratories , department of radiation oncology , david geffen school of medicine at ucla , los angeles , ca , usa , 4 department of vascular surgery , department of surgery , medical university of graz , austria . received : november 9 , 2004 ; accepted : may 13 , 2005 strahlenther onkol 2005 no . 
in german - speaking countries and in central and eastern europe , there are different indications for radiotherapy of nonmalignant disorders but they include : radiotherapy of chronic painful degenerative disease such as hyperproliferative soft - tissue disorders , e.g. , early - stage dupuytrens / peyronies disease or postoperative keloid prophylaxis ; functional disease such as graves orbitopathy ; prophylaxis of heterotopic ossification or neointimal hyperplasia and lymphatic complications ( persistent lymphoceles or lymphocutaneous fistulas ) [ 3 , 8 , 1113 , 1719 , 21 , 24 , 3033 ]  . 
 the subject of this paper is a retrospective analysis of the role of external radiotherapy in the treatment of persistent lymphocutaneous fistulas and discussion of hypotheses as to its possible radiobiological mechanis patients and methods between 1987 and 2002 , 17 patients with a total of 19 persistent lymphocutaneous fistulas were referred to the department of radiation oncology , graz , austria , for external radiotherapy . 
lymph fistulas were obtained after vena saphena harvesting ( n = 7 ) , femoropopliteal bypass ( n = 3 ) , surgery for varicose veins ( n = 2 ) , hip arthroplasty ( n = 3 patients ; five fistulas ) , shunt surgery ( n = 1 ) , and piercing ( n = 1 )  . 
in twelve patients , radiotherapy was administered with an orthovoltage unit ( 100 kv , 20 ma , 3 mm aluminum ) and a source - skin distance of 40 cfive patients were treated with a linear accelerator using electrons ( 411 mev ) in two cases , while a further three patients , who presented with lymphatic complications after hip arthroplasty ( five fistulas ) , were irradiated with photon beams ( 8 mv )  . 
the treated area included the scar with a surrounding margin of 23 c fraction size ranged from 0.3 gy to 2 gy and the mean treatment duration was 7 days ( range , 216 days )  . 
the results in the four nonresponders were as follows : in one patients with hip arthroplasty only two out of three fistulas disappeared after 12 gy ; the second patient developed a recurrent lymphatic fistula 14 days after radiotherapy and received a second series of irradiation up to 10.5 gy , without success . 
no treatment - related early or late side effects were observed . discussion lymphatic drainage from a surgical wound is an uncommon but challenging complication of surgical intervention , particularly after vascular and cardiac surgery . 
the most frequent location of persistent lymphatic fistulas is the groin where the incidence is 0.56% [ 1 , 2 , 5 , 2628 , 36 , 39 ]  . 
observed the highest incidence of groin lymphatic complications in patients having an aortobifemoral bypass for aneurysmal disease or an isolated femoral procedure in a previously operated groin [ 39 ]  . 
held that lymphatic fistulas were more likely to develop in older patients and in patients who underwent aortobifemoral bypass for limb salvage rather than for claudication [ 20 ]  . 
diabetes , infection of the operated leg or foot , use of a prosthetic graft , as well as reoperation were associated with statistically insignificant increases in risk [ 36 ]  . 
 lymphatic fistulas also have been reported as a complication of vena saphena magna harvesting [ 25 ] , of central venous line placement [ 29 ] , or in chronic ulcers [ 4 , 15 ]  . 
a variety of treatment attempts have been described including leg elevation , continuous local pressure [ 35 ] , subatmospheric pressure dressing therapy [ 6 ] , surgical ligation of the leaking vessel alone [ 14 ] or with the assistance of blue - dye staining of lymphatic anatomy [ 31 , 37 ] , or radiotherapy [ 3 , 12 , 21 ]  . 
 [ 33 ] published the results of a german patterns - of - care study ( pcs ) of radiotherapy for benign disease including 134 of 152 german institutions ( 88% )  . 
reported efficacy of low - dose external radiotherapy ( 1 gy per fraction ) in 29 patients ( 25 with lymphatic fistulas , four with lymphoceles ) [ 21 ]  . 
since the doses used are small , the mechanism of action of radiation on benign pathologic processes must be very different from that of radiation therapy on malign and benign tumors , which is ascribed to cell killing [ 41 ]  . 
the analgesic , anti - inflammatory , and immunosuppressive effects of low - dose irradiation are well known and therapeutically exploited , but the molecular mechanism of the phenomenon is largely unknown . 
inhibition of cell proliferation might explain the effectiveness of radiotherapy in preventing heterotopic ossification , while radiation - induced terminal cell differentiation might result in a therapeutic effect in keloid radiotherapy , the differences being due to the nature of the cellular target . 
 with regard to the radiation - induced healing of lymphatic fistulas , the biological explanation might be found in the effect of irradiation on the vascular endotheliuover the last decade , most radiobiological studies on the effects of radiation on the vasculature were concentrated on the role of endothelial cells in the development of irreversible late normal - tissue injury following therapeutic irradiation for cancer . 
 hence , despite continuous subclinical progression of the injury , the time for endothelium - based normal - tissue side effects to manifest is thought to range from months to years after exposure . 
 [ 9 ] performed experiments to investigate whether radiation doses commonly used in anti - inflammatory radiotherapy modulate the expression of cell adhesion molecules such as e - selectin by tumor necrosis factor - ( tnf - ) - activated endothelial cells . 
a radiation dose - dependent decrease in e - selectin expression was found , which might be a mechanism that decreases leukocyte adhesion after lowdose irradiation [ 9 ]  . 
the 26s proteasome controls degradation and the kinetics of most key molecules involved in signal transduction , inflammatory / immune responses , and cell cycle progression and therefore profoundly influences cell function [ 16 ]  . 
 based on these literature data , which demonstrate low dose radiation - induced changes in endothelial cell adhesion properties , cell motility and cell function , it is likely that the explanation for the therapeutic effect of irradiation in the treatment of lymphatic fistulae could be found at the level of cell function and metabolism rather than cell killing . 
both the fact that small doses are effective and the healing time is relatively short indicates a fast process and excludes proliferative cell death as a reason for the therapeutic effect . 
 leakage of lymph through the vascular endothelial cell lining is a result of the pressure of interstitial fluid and requires motility of the endothelial cells in opening and closing the intercellular spaces . 
 the pathologically increased lymph secretion observed in patients with lymphatic fistulas might be due to endothelial cell disorganization , and radiation could serve as the trigger to allow them to recover from their pathologic dysfunction . 
 strahlentherapie und onkologie original article toxicity and survival results of a phase ii study investigating the role of postoperative chemo radioimmunotherapy for gastric adenocarcinoma nuran s enel bes e1 , evin byknal2 , mustafa zgrog lu2 , gkhan demir2 , ays e yldrm1 , nil molinas mandel2 , fuat demirelli2 , sheyla serdengeti2 , ahmet ber1 background and purpose : to investigate the role of postoperative concomitant chemoradioimmunotherapy in gastric adenocarcinoma patients . 
 patients and methods : 59 patients , who underwent total or subtotal gastrectomy , with lymph node involvement , positive microscopic surgical margins or serosal involvement were included in the study . 
bolus of 450 mg / m2 / day 5 - fluorouracil ( 5 - fu ) was administered concomitantly during the first 3 days and at the 20th day of irradiation . 
however , due to high toxicity , radiotherapy must be delivered with the most proper techniques along with adequate nutrition and supportive care . key words : gastric adenocancer chemoradiotherapy immunotherapy strahlenther onkol 2005 ; 181 : 6529 doi 10.1007 / s00066 - 005 - 1399 - 2 ergebnisse einer phase - ii - studie ber nebenwirkungen und berlebenszeit der radiochemoimmuntherapie bei patienten mit adenokarzinom des magens hintergrund und ziel : untersuchung der rolle der postoperativen radiochemotherapie bei patienten mit adenokarzinom des magens . 
 patienten und methodik : 59 total oder subtotal operierte patienten mit adenokarzinom des magens , die eine invasion der serosaoberflche , einen befall der regionren lymphknoten oder positive resektionsrnder aufwiesen , wurden in die studie eingeschlossen . 
die bestrahlung wurde in extended - field - technik ber zwei felder ( anterior - posterior und posterior - anterior ) mit einer gesamtdosis von 45 gy in 25 fraktionen zu 1 , 8 gy appliziert . 
die adjuvante chemotherapie mit einem 450 - mg / m2 - bolus 5 - fluorouracil ( 5 - fu ) wurde an den ersten 3 tagen verabreicht und am 20 . 
die lokoregionale kontroll1 department of radiation oncology , istanbul university , cerrahpas a medical school , istanbul , turkey , 2 department of internal medicine , medical oncology section , istanbul university , cerrahpas a medical school , istanbul , turkey . 
sechs patienten konnten die behandlung aufgrund von nebenwirkungen nicht beenden . schlussfolgerung : obwohl 48% der patienten in dieser studie einen mikroskopisch nachweisbaren resttumor aufwiesen , war die beobachtete berlebenszeit verhltnismig gut . 
however , even after complete resection with negative margins , many patients experience recurrence and have poor survival results unless the tumor is strictly confined to the gastric mucosa [ 19 ]  . 
local and regional relapse in gastric bed , regional nodes , or at anastomosis site occurs in 5060% of node positive patients with extension of tumor through serosa , after gastric resection with a curative intent [ 15 , 23 ]  . 
therefore , adjuvant chemoradiotherapy might be a treatment option to achieve better locoregional control and overall survival in gastric cancer patients after curative resection [ 17 , 31 ]  . 
previously , immunotherapy with levamisole was shown to have additive effects on survival both in early disease as well as locally advanced disease of various gastrointestinal cancers [ 16 , 26 28 , 33 ]  . 
according to these results , a phase ii study to determine the efficacy of chemoradioimmunotherapy in gastric cancer patients after macroscopic complete resection was started in 1993 at istanbul university , cerrahpas a medical faculty , turkey . 
the eligibility criteria included histologically confirmed gastric or gastroesophageal adenocarcinoma , complete resection of the tumor with total or partial gastrectomy without any macroscopic residual disease , without gross peritoneal seeding and distant metastasis . 
a concomitant chemotherapy with 450 mg / m2 / day 5 - fluorouracil ( 5 - fu ) , intravenous ( i.v. ) bolus , during the first 3 days of radiotherapy ( d13 ) and at the 20th day of irradiation ( d1 ) was planned . 
the radiation fields included the tumor bed and major nodal chains : lesser and greater curvature ; celiac axis including pancreoduodenal , splenic , suprapancreatic lymph nodes and porta hepatis ; paraaortic to the level of mid - l3 or mid - l4 . 
patients were treated in the supine position and parallel opposed anterior - posterior / posterior - anterior ( ap / pa ) fields were used ; the dose was calculated at mid - plane . 
for tumors originating in the cardia or proximal gastric lesions , the field extended up into the esophagus ; a major portion of the left hemidiaphragm was included , the heart was shielded and the lower border of the field extended to mid - l3 . 
for distal gastric lesions , the lower border of the field extended to mid - l4 , and 50% of the right kidney was usually in the field , so that 75% of left kidney was tried to be spared to maintain renal function . 
 staging and pathologic characteristics patients ( n ) proportion ( % ) 3 9 2 1 7 5 9 2 2 1 3 2 9 3 3 2 staging system tnm stage ii t3 n0 m0 t2 n1 m0 stage iiia t2 n2 m0 t3 n1 m0 t4 n0 m0 stage iiib t3 n2 m0 t4 n1 m0 t4 n2 m0 location of primary tumor cardia corpus and antrum pylorus linitis plastica gastric remnant billroth serosal involvement without serosal involvement serosal involvement microscopic surgical margin positive negative using additional fractions . 
 patient evaluation patients were followed regularly at 3to 4 - month intervals for 2 years after the completion of maintenance chemotherapy , at 6 - month intervals for the next 3 years , and yearly thereafter . 
 locoregional recurrence was defined as disease documented by biopsy or cytology reports or abnormal images on radiographic studies in the irradiation field and distant failure as recurrence elsewhere including the peritoneum and liver parenchyma . 
disease - free survival ( dfs ) was the duration from the date of completion of treatment until the date of last follow - up visit or death without locoregional or distant metastases . 
only four patients ( 7% ) showed no lymph node involvement , and the median number of involved lymph nodes was four in the remaining 55 patients ( range , one to 34 lymph nodes )  . 
in 28 patients ( 48% ) with microscopically positive proximal or distal surgical margins , a 10 - gy boost dose was given to the anastomosis site after reduction of the initial treatment volumes . 
 patients ( n ) proportion ( % ) organ tissue upper gastrointestinal system grade 1 grade 2 grade 3 grade 4 no toxicity lower gastrointestinal system grade 1 grade 3 no toxicity hematologic wbcs grade 1 grade 2 grade 3 grade 4 no toxicity hemoglobin grade 1 grade 2 no toxicity platelets grade 3 no toxicity 6 5 2 4 1 4 3 5 1 1 58 was stopped at a total dose of 39 gy . 
except for two patients who experienced grade 4 leukopenia during maintenance chemotherapy , all grade 3 and grade 4 ugis , lower gastrointestinal system ( lgis ) and hematologic toxicities occurred during concomitant chemoradiotherapy . 
one patient died at 22 months due to small cell lung carcinoma , and another patient died of high grade malignant mixed brain tumor ( oligodendroglioma and anaplastic astrocytoma ) at 61 months , while both of them did not have any recurrence owing to gastric carcinoma . 
the 3and 5year lc rates were 59% and 55% , respectively ( figure 3 )  . the 3and 5 - year os rates for 31 patients with negative surgical margins were 39% and 21% , respectively , and the os survival rates were 29% and 9% for the same periods in 28 patients with positive surgical margins . 
the crude locoregional failure was 10 / 31 ( 32% ) for patients with no residual disease and 10 / 28 ( 36% ) for those with microscopic residual disease ( figure 5 )  . 
 discussion a reduction in recurrence and prolongation of survival with postoperative irradiation plus chemotherapy has been shown in other gastrointestinal system tumors such as rectal [ 32 ] and p = 0.2932 negative positive 0 12 24 36 48 60 72 84 96 108 120 months figure 4 . 
in their study , the 3 - year survival rates were 50% in the chemoradiotherapy group and 41% in the surgery - only group ( p = 0.005 ) , and the median survival amounted to 36 months in the chemoradiotherapy arm while it was 27 months in the surgery - alone group . 
 the major criticism attributed to the int - 0116 study was that most of the patients had d0d1 dissection which might be substantially associated with an increased risk of residual positive lymph nodes . 
in two large randomized western studies [ 4 , 8 ] comparing d1 with d2 dissection , a substantial increase in morbidity was found without improvement in survival of the patients with d2 . 
 [ 29 ] where all 290 patients underwent d2 dissection followed by a concomitant chemoradiotherapy protocol which was almost identical with the int0116 protocol , the 3 - year os and relapse - free survival rates were 68% and 62% , respectively . 
other than os , 34% of the patients experienced locoregional recurrences and it was also higher than the locoregional recurrence rates of the patients who received adjuvant therapy in the int - 0116 [ 25 ] and korean study [ 29 ]  . 
although the survival rates of patients with positive and negative margins were different in this study , the difference did not reach a statistically significant level , which might be attributed to the small number of patients in the whole population , the increased radiation dose in patients with microscopic residual disease or the extremely poor prognostic factors such as extension beyond gastric wall and involved lymph nodes of the patients without microscopic residual disease . 
the median survival duration of 22 months seen in our study group with microscopic residual disease was higher than that of the corresponding patients in the mayo clinic study [ 18 ]  . 
 the median survival of patients with negative surgical margins amounted to 19.3 in the mayo clinic study which was also lower than the median survival of patients with the same characteristic in the current study which was found to be 25 months . 
in the mayo clinic series concomitant 5 - fu - based chemotherapy was given during irradiation in 79% of the patients , and only 22% of the patients received any maintenance chemotherapy , usually of a limited duration . 
the median survival values of the current study were similar to the massachusetts general hospital series [ 14 ] in which median survival times were both 24 months for patients without or with microscopic residual disease . 
the irradiation factors were basically the same as in our study , and 93% of the patients in the massachusetts general hospital series received concomitant 5 - fu - based chemotherapy with irradiation and 83% were given five cycles of maintenance chemotherapy with two different 5 - fu - based regimens . 
 [ 13 ] , 25 patients receiving postoperative irradiation to a total dose of 50 gy with a 2 - week split and concomitant 5 - fu were followed weekly for 1 year or until disease progression after completion of chemoradiotherapy . 
although differences in prognostic factors make it difficult to draw definitive conclusions , in the series , including ours , with microscopic residual disease and more intensive adjuvant chemotherapy , the median survival times were higher [ 13 , 14 ] , as compared with the series in which less intensive chemotherapy regimens with a short duration were applied [ 18 , 30 ]  . 
although the prognostic factors were not balanced over the treatment groups , the median survival was longer for patients who received long - term 5 - fu every 2 weeks for 18 months or until progression as compared to patients not administered long - term 5 - fu [ 2 ]  . 
the crude locoregional failure rate of patients with microscopic residual disease in the current study was almost similar to that of patients in the mayo clinic study with the same characteristics [ 18 ]  . 
a significant improvement in lc of patients treated with > 50 gy compared to those treated with 50 gy has also been noted by the mayo clinic group [ 18 ] , though in our study higher doses were applied to patients with positive margins in order to increase local control for residual disease . 
in a prospective study by the national cancer institute of rome [ 1 ] , the total dose of 55 gy , a hyperfractionated radiation dose of two 1.1 - gy fractions per day , was given with protracted venous infusion of 5 - fu to 40 gastric cancer patients with negative margins . 
in - field local recurrence was observed in one case ( 2.5% ) , and both in - field and distant relapse in two cases ( 5% ) ; the 3 - year survival rate was 52% . 
 although , in the current study , the rates of early grade 3 and 4 toxicity were comparable with the chemoirradiation arm of the int - 0116 [ 25 ] and korean study [ 29 ] , we must consider that four patients ( 7% ) died on account of early toxic effects and six ( 10% ) could not complete treatment . 
 [ 29 ] year 1983 1986 1992 2000 2001 2002 2003 design patients ( n ) margins radiation dose ( gy ) median survival ( months ) retrospective retrospective retrospective retrospective randomized prospective prospective 46 25 20 63 281 40 290 positive / negative / gross positive / negative positive / negative positive / negative / gross negative negative negative 4552 50b 5560 39.659.4 55c 24 / 24 / 15 16.7 a number of patients who received chemoradiotherapy ; b radiotherapy was given with a 2 week split ; c hyperfractionated irradiation was applied . chemotherapy was 5 fu - based in all studies . 
intensity - modulated radiotherapy ( imrt ) may reduce toxicity by significantly reducing maximum and median doses to organs at risk while still applying sufficient dose to the target volume [ 3 , 9 ]  . 
in that study , 1 , 296 patients with stage b2 and stage c were randomly assigned to observation or to 1 - year treatment with levamisole combined with 5 - fu . 
on the other hand , in some studies it has been reported that adding levamisole to combination chemotherapy offered no improvement or even had a negative effect on treatment outcome [ 5 , 6 , 20 ]  . 
 conclusion the results of the int - 0116 trial [ 25 ] have definitely established the role of combined irradiation and chemotherapy as standard adjuvant treatment in completely resected gastric cancer . 
however , especially for the patients with microscopic residual disease , the optimal treatment is still to be defined in terms of radiation dose , fractionation , and technique , as well as chemotherapy drugs , intensity and timing in a randomized trial . 
beckmann4 , rolf sauer1 , vratislav strnad1 purpose : to investigate the incidence of fat necrosis , breast tissue fibrosis and breast pain after conserving surgery and accelerated partial - breast irradiation ( apbi , group a ) , whole - breast external - beam irradiation ( ebrt , group b ) , or ebrt combined with an interstitial boost ( ebib , group c ) in women with breast cancer . 
this analysis did not support the hypothesis that apbi with multicatheter implants leads to higher rates of fat necrosis , fibrosis , or pa key words : breast cancer fat necrosis radiotherapy partial - breast irradiation breast - conserving therapy strahlenther onkol 2005 ; 181 : 63844 doi 10.1007 / s00066 - 005 - 1439 - y fettnekrosen nach brusterhaltender operation und interstitieller brachytherapie und / oder externer radiotherapie bei frauen mit mammakarzinom ziel : untersuchung und vergleich der inzidenz und des schweregrades des auftretens von fettnekrosen , fibrosierung und brustschmerz nach brusterhaltender operation und akzelerierter teilbrustbestrahlung ( gruppe a ) , externer ganzbrustbestrahlung ( gruppe b ) sowie externer ganzbrustbestrahlung mit interstitiellem brachytherapie - boost ( gruppe c ) bei frauen mit einem mammakarzino patienten und methodik : die auswertung umfasst 85 patientinnen , die zwischen 02 / 2000 und 03 / 2002 brusterhaltend therapiert wurden . 
 ergebnisse : bei 15 , 3% aller patientinnen wurden fettnekrosen gefunden , in den gruppen a , b und c bei 15 , 2% , 20 , 0% and 9 , 0% der flle . 
 schlsselwrter : mammakarzinom fettnekrose strahlentherapie teilbrustbestrahlung brusterhaltende therapie 1 department of radiation oncology , university hospital erlangen , germany , 2 department of diagnostic radiology , university hospital erlangen , germany , 3 department of medical informatics , biometry and epidemiology , university of erlangen , germany , 4 department of obstetrics and gynecology , university hospital erlangen , germany . 
fat necrosis after breast - conserving surgery and radiotherapy introduction compared to external - beam radiotherapy ( ebrt ) , brachytherapy alone has been suspected to lead to higher side effects in the treatment volume because of a higher dose inhomogeneity . 
aim of this analysis was to evaluate if fat necrosis is more likely to develop after partial - breast irradiation compared to ebrt in women irradiated because of breast cancer . 
the most common causes of fat necrosis are cyst aspiration , biopsy , lumpectomy , reduction mammoplasty , implant removal , breast reconstruction with a transverse rectus abdominis myocutaneous flap , radiation therapy , and trauma [ 9 , 13 ]  . 
 while it is well known that radiation therapy may cause or promote fat necrosis , there is no clear evidence whether accelerated partial - breast irradiation ( apbi ) of the tumor bed with multicatheter brachytherapy implants leads to higher rates of clinically evident fat necrosis , especially in fractionated high - dose - rate ( hdr ) brachytherapy regimens [ 27 , 28 ]  . 
mammographically , there is a wide spectrum of appearances ranging from well - defined superficial oil cysts which may show rim calcification , through a spiculate mass resembling carcinoma , to malignant - appearing microcalcification . 
 in this retrospective study we compared three groups of patients who had received either multicatheter brachytherapy apbi , ebrt , or combined external - beam and interstitialboost irradiation ( ebib ) , regarding a possible impact of radifigures 1a to 1c . 
 patients and methods patient characteristics 85 patients who received breast - conserving surgery and postoperative irradiation between 02 / 2000 and 03 / 2002 were selected for this retrospective analysis . 
33 patients received apbi ( group a ) of the tumor bed with multicatheter brachytherapy , 30 patients received ebrt ( group b ) of the whole breast with or without external - beam small - volume electron - boost irradiation , and 22 patients received ebrt of the whole breast with an interstitial multicatheter implant for boost irradiation ( ebib , group c )  . 
the mean number of invasive procedures ( including biopsies , breastconserving surgery , and interstitial brachytherapy ) per patient was higher in the brachytherapy - containing apbi and combined treatment group ( ebib )  . 
18 patients ( 60% ) received an additional small - volume electron boost to the tumor bed with a median total dose of 12 gy ( range , 1012 gy ) with 2 - gy fractions daily . 
 the median number of flexible afterloading tubes was 13 ( range , seven to 17 ) ; 16 patients ( 72.7% ) had two - plane implants and six ( 27.3% ) three - plane implants . 
for the statistical testing of heterogeneity , i.e. , differences between the three subgroups , either the kruskal - wallis or / and the wilcoxon test was used for continuous data , as appropriate , and fishers exact test for categorical data . 
the time to event with regard to mammographically evident fat necrosis was graphically displayed with a kaplan - meier curve ( figure 2 ) and statistically analyzed by log - rank tests . 
detailed information about the results in respect of the endpoints , mammographically evident signs of fat necrosis , clinically evident breast tissue fibrosis , and subjective breast pain is presented in table 2 . 
 the 3 - year fat necrosis - free survival probability ( kaplanmeier analysis ) for groups a , b , and c ranged between 80% and 90% , the differences not being significant ( table 2 )  . 
 using pairwise comparison , its incidence was significantly 5 10 15 20 25 30 35 40 45 50 55 60 time ( month ) radiotherapy intersitial percutaneous interstitial and percutaneous figure 2 . 
 higher in the two subgroups with ebrt ( b and c ) , compared with apbi alone ( p < 0.001 and p = 0.006 , respectively ) , while the difference between groups b and c was not significant . the endpoint subjective breast pain was found in 9.1% ( 95% ci : 1.924.3 ) of the patients who received brachytherapy only ( group a )  . 
it is noteworthy that the highest pain incidence was not found in the subgroups with interstitial treatment , but in the ebrt subgroup , with a significant difference between groups a and b only ( p = 0.028 ) in pairwise comparisons of the subgroups . 
although no significant differences were found between the three groups , it is of interest that the patients who received ebrt exclusively had the highest incidence of signs indicative of fat necrosis in their mammograms . 
other authors described comparable rates for asymptomatic fat necrosis of 1025% after ebrt [ 8 , 18 ] and 621% after apbi [ 4 , 14 , 15 , 18 ]  . 
in summary , our results confirm the hypothesis of other working groups [ 4 , 5 , 7 , 8 , 10 , 14 , 15 , 18 , 20 , 2628 ] that fat necrosis is a common side effect of breast - conserving therapy and is neither restricted to , nor a specific problem of interstitial radiotherapy techniques . 
 [ 27 ] described an alarming rate of symptomatic fat necroses after apbi with hdr multicatheter implants : 32 patients with 33 breast cancers received a total dose of 34 gy in ten bi - daily fractions to each lesion . 
 fibrosis yes fibrosis pain pain yes yes fat necrosis yes 4 6 8 fat necrosis yes 0 3 3 5 statistical testing results second - order association between all three endpoints : association between fibrosis and fat necrosis : association between fibrosis and pain : association between pain and fat necrosis : not significant not significant not significant not significant in all cases , pain resolution was complete at a median follow - up duration of 8 weeks . 
the fact , that , in contrast to the experience of other working groups [ 5 , 14 , 18 , 19 ] , no patient of this series needed surgical intervention may indicate a somewhat biased grading . 
 impact of systemic chemotherapy on the endpoints fat necrosis and fibrosis some authors described a significant negative impact of systemic anthracycline - based chemotherapy on cosmetic outcome after partial - breast irradiation [ 22 , 27 ]  . 
although they failed to show a significant difference for the endpoints fat necrosis ( p = 0.10 ) and subcutaneous toxicity grade 2 ( p = 0.62 ) between the chemotherapy and the no - chemotherapy group , they postulated a trend toward a greater risk of fat necrosis in those patients who received anthracycline - based chemotherapy [ 27 ]  . 
but this would mean that the factors trauma ( = invasive procedures per patient ) and total radiotherapy dose may be not as important as chemotherapy for the development of clinically evident breast tissue fibrosis . 
 analysis of the association between the endpoints fat necrosis , fibrosis and pain table 3 shows that there is no association between fibrosis and breast pain and mammographic evidence of fat necrosis . 
in cases when there is no histopathologic confirmation , and if the standardized mammographic diagnosis is not taken into account , the terms fat necrosis and symptomatic fat necrosis are not defined clearly , which may cause confusion [ 1 ]  . 
our analysis did not support the hypothesis that apbi with multicatheter implants leads to higher rates of clinically evident fat necrosis , breast tissue fibrosis , or breast pa therefore our results do not reveal a clear ( dis ) advantage of interstitial versus percutaneous radiotherapy in respect of these sequelae . 
 strahlentherapie und onkologie original article conpas : a 3 - d conformal parotid gland - sparing irradiation technique for bilateral neck treatment as an alternative to imrt ruud wiggenraad1 , mirjam mast1 , jan van santvoort2 , marc hoogendoorn3 , henk struikmans1 background and purpose : intensity - modulated radiotherapy ( imrt ) is used in most reported techniques for bilateral neck irradiation that aim at parotid gland sparing . 
the purpose of this paper is to demonstrate , in patients with larynx or hypopharynx carcinoma , that conpas enables adequate coverage of the primary tumor and the bilateral neck nodes , while keeping the mean parotid dose ( mpd ) < 26 gy . 
 patients and methods : treatment plans using conpas and the conventional technique ( using one anteroposterior supraclavicular and two lateral beams ) were computed for ten consecutive patients with t14 n01 larynx or hypopharynx carcinoma ( not t1 glottic )  . 
a dose of 46 gy was prescribed to the primary tumor and the bilateral neck nodes , planned either with the conventional technique or conpas , followed by a boost up to 70 gy with a simple two - field technique . 
the target coverage of both techniques was compared using the v95 , the percentage of the planning target volume ( ptv ) of the primary tumor and nodal regions receiving at least 95% of the prescribed elective dose . 
 key words : head - and - neck cancer parotid gland conformal radiotherapy strahlenther onkol 2005 ; 181 : 67382 doi 10.1007 / s00066 - 005 - 1413 - 8 conpas : eine dreidimensionale , die parotis aussparende bestrahlungstechnik fr bilaterale halsbestrahlung als alternative zur imrt hintergrund und ziel : die intensittsmodulierte strahlentherapie ( imrt ) ist die am hufigsten beschriebene technik fr bilaterale halsbestrahlung mit schonung der parotis . 
ziel dieser studie ist zu zeigen , dass bei patienten mit larynxoder hypopharynxkarzinom mit conpas eine adquate dosisabdeckung des primrtumors und der bilateralen lymphknoten erreicht werden kann , wobei die gemittelte dosis in der parotis ( mdp ) < 26 gy liegt . 
 patienten und methodik : fr zehn konsekutive patienten mit larynxund hypopharynxkarzinom ( t14 n01 ) wurde sowohl ein bestrahlungsplan mit der conpas - technik als auch mit der konventionellen technik ( zwei seitliche felder und ein anteroposteriores supraklavikulres feld ) erstellt . 
die zielvolumenabdeckungen der beiden techniken wurden mit hilfe des v95 ( prozentsatz des planungszielvolumens [ ptv ] des primrtumors und der lymphknotenregionen , der mindestens 95% der vorgeschriebenen elektiven dosis erreicht ) miteinander verglichen . 
 1 department of radiotherapy , the hague medical center , the hague , the netherlands , 2 department of clinical physics , the hague medical center , the hague , the netherlands , 3 arnhems radiotherapeutisch instituut , arnhem , the netherlands . received : january 18 , 2005 ; accepted : may 13 , 2005 strahlenther onkol 2005 no . 
die dosimetrische verifikation zeigt eine gute bereinstimmung zwischen dosisberechnung und messungen . schlussfolgerung : conpas ermglicht eine adquate zielvolumenabdeckung und eine klinisch relevante parotisaussparung bei bilateraler halsbestrahlung ohne intensittsmodulation . schlsselwrter : kopf - hals - karzinome ohrspeicheldrse konformale strahlentherapie introduction xerostomia may severely impair quality of life of patients with head - and - neck cancer , who have been irradiated [ 20 , 34 ]  . 
a mean dose to the parotid gland ( mpd ) of < 26 gy should be applied to reach substantial sparing of the gland function [ 14 ]  . the conventional radiotherapy technique for patients with head - and - neck cancer , in whom the ctv includes both sides of the neck , usually is based upon two parallel opposed lateral fields and an anteroposterior ( ap ) supraclavicular field . 
in recent years more and more attention is given to intensity - modulated radiotherapy ( imrt ) for head - and - neck cancer , using either forward or inverse planning [ 2 , 4 , 6 , 7 , 11 , 13 , 16 , 23 , 24 ]  . 
 patient tumor location stage larynx hypopharynx larynx larynx larynx hypopharynx larynx larynx larynx larynx t2 n0 m0 t4 n0 m0 t1 n0 m0 t2 n0 m0 t4 n0 m0 t3 n1 m0 t2 n0 m0 t3 n0 m0 t3 n1 m0 t4 n0 m0 1 2 3 4 5 6 7 8 9 rotid glands is possible with adequate coverage of the primary tumor and the neck nodes . 
the purpose of this study is to demonstrate that conpas can keep the mpd < 26 gy , whereas it is equal to the conventional technique with respect to target coverage . 
 patients and methods patients for the purposes of our study we used the planning ct scans of ten consecutive patients who had been treated in our department and fulfilled the following criteria : glottic larynx carcinoma t24 n01 m0 ( t2 only with impaired vocal cord mobility ) , or ( cid : 127 ) supraglottic larynx carcinoma t14 n01 m0 , or ( cid : 127 ) hypopharynx carcinoma t14 n01 m0 . 
the two hypopharynx carcinomas were mainly located in the piriform sinus . patient positioning and ct scanning the patients had been immobilized in supine position , with a thermoplastic mask attached at five points to a carbon - fiber plate support . 
the basis of this sixto seven - field isocentric technique is formed by two pairs of full - length parallel opposed oblique half - beams and a large ap beam with a separate supraclavicular segment . 
 the planning procedure is as follows : to begin with , the isocenter is placed in the anterior part of the vertebral body halfway between the upper and lower limits of the ptvac . 
 then , both oblique posterior beams are set up and turned into half - beams by closing the collimators on the side of the spinal cord ( figure 1 )  . 
in the beams eye view mode the angles may be modified slightly , so that maximal blocking of the parotid glands is possible , while preserving adequate coverage of the ptvac . 
 then , the two oblique anterior beams are set up and turned into half - beams by closing the collimators that are off the side wiggenraad r , et al . 
conformal parotid - sparing technique treatment planning all contouring and planning was done on helax - tms , version 6.1 , a three - dimensional ( 3 - d ) treatment planning system ( nucletron , the netherlands )  . 
 target volume and regions of interest three separate elective ctvs ( ctva ) were drawn for the locoregional treatment : one for the primary tumor and one for the right and left neck , respectively . 
the ctva for both sides of the neck included neck node levels ii , iii , and iv in n0 patients and levels ii , iii , iv , and v in n1 patients . 
the ptvs were created by adding 3 - d margins of 5 mm to the ctvs in the mediolateral and ap directions and 4 mm in the craniocaudal direction . three separate elective ptvs ( ptva ) combined ( ptvac ) formed the target that had to be covered by the 95% isodose . 
in the slices at or below the bottom edge of c1 where the parotid gland was recognizable , the lateral border of the ctva was drawn at the medial edge of the parotid . 
 dose prescription in all plans 46 gy was prescribed to ptvac and 24 gy to ptvb with the conventional fractionation scheme of 2 gy per fraction , five fractions per week . 
furthermore , all 20 plans were remade with 5 mm bolus material on the skthis was done to examine to what extent incomplete coverage of a ptv was caused by the build - up effect . 
in the conventional plan two parallel opposed lateral fields are designed covering the cranial part of the ptvac and an ap supraclavicular field covering the caudal part of the ptvac . 
beam weights and wedge fractions are optimized in each individual beatable 2 shows the usual characteristics of the different beams of conpas , and figure 5 gives a schematic overview of the complete setup with six beams . 
 evaluation and comparison of dose plans at first , plans were assessed by visual inspection of the dose distributions and by reviewing the dose - volume histograms ( dvhs ) of the ptvs and the regions of interest . 
 for all plans the maximum dose in the spinal cord ( mscd ) , the mean dose in the left and right parotid glands ( mpd left and mpd right ) and the oral cavity ( mocd ) were calculated . 
furthermore , we calculated the v95 ( percentage of the ptvac receiving at least 95% of the prescribed dose ) and the v107 ( percentage of the ptvac receiving at least 107% of the prescribed dose ) for all plans . 
the same ct slice as in figure 1 with an example of a left anterior oblique beathe shaded area represents the half - beam , that is actually used in the plan . 
note 1 : in any plan either an anteroposterior beam ( total number of beams becomes six ) or the two lateral beams ( total number of beams becomes seven ) will be given . 
 anmerkung 1 : in jedem plan werden entweder ein antero - posterior strahlenbndel ( die totale anzahl der strahlenbndel wird sechs ) oder die zwei lateralen strahlenbndel ( die totale anzahl der strahlenbndel wird sieben ) gegeben . 
 beam angle ( ) weight parotida right oblique anterior left oblique anterior right oblique posterior left oblique posterior anteroposterior supraclavicular segment left lateral right lateral 320 40 220 140 0 0 90 270 50 50 100 100 40 40 40 40 inside inside blockedb blockedb blockedb outside inside inside a the relation of the parotid gland to the beam b in this beam the parotid gland is blocked as much as possible c the relation of the spinal cord to the beam spinal cordc inside inside outside outside inside inside inside inside the patients are well fixated in a mask , we consider a 2 - mm shift to be a high estimate of what is realistic . 
conformal parotid - sparing technique sk as it was obvious that sparing of the submandibular glands was not possible in either technique , we did not calculate ( mean ) doses in the submandibular glands . 
these parameters are the td50 ( the 50% tolerance dose for uniform irradiation of the partial volume v ) , the n representing the volume effect , and the m representing the steepness of the dose - complication curve for a fixed partial volume . 
as the boost plans of both techniques were the same , differences found in the parameters could be ascribed to the differences in the way the conventional technique and conpas treat the ptvac . 
 dosimetric validation there are some potential causes for inaccuracies in the delivered dose distribution : ( 1 ) not all treatment planning systems can predict the dose distribution of highly asymmetric wedged fields with sufficient accuracy ; ( 2 ) the isocentric accuracy and calibration of jaws or leaves is critical when abutting half - fields ; and ( 3 ) small movements of the patient between fields will disturb the dose distribution . 
 to investigate the influence of intrafraction variations of the patient position on the dose distribution , also two films ( 40 mm caudal and 50 mm cranial ) were irradiated while the phantom was moved 2 mm between the left oblique fields and the right oblique fields . 
in c ( conventional plan ) the 95% isodose line almost entirely covers the parotid glands , but only a small part of the oral cavity , whereas in f ( conpas ) the parotid glands are spared at the expense of a higher dose in the oral cavity . 
vergleich der dosisverteilung bei einen herkmmlichen plan und conpas in drei ct - schnitten bei einem patienten mit hypoparynxkarzinodie weipunktierten linien stellen das ptv dar , die durchgezogenen schwarzen linien die 95% - isodose linien dar . 
in c ( herkmmlicher plan ) bedeckt die 95% - isodose - linie fast die gesamten ohrspeicheldrsen , aber nur einen kleinen teil der mundhhle , whrend in f ( conpas ) die ohrspeicheldrsen ausgespart werden . 
 figure 7 , showing the mean dvhs of all 20 parotid glands and ten ptvacs , illustrates that the target coverages with the conventional technique or conpas are equivalent , whereas the doses in the parotid glands are significantly lower with conpas . 
 dosimetric validation the absolute dose measurement showed a discrepancy of 0.16% compared to the value calculated by treatment planning system ( tps )  . a typical result of the dose comparison is depicted in figure 8 . 
as can be seen , there are slight differences between the measured and calculated isodoses , but at steep dose gradients the distance between the two is small ( < 3 mm ) and at shallow dose gradients the dose difference between the two is small ( < 4% )  . 
 figure 9 shows a comparison of dose profiles from the measurement without shift and the measurement with a 2 - mm shias can be seen , there is a slight underdosage near x = 85 mm of approximately 4% without the intentional shiwhen the shift is applied , the underdosage occurs at x = 125 mm and is approximately 8% . 
 discussion in this study we demonstrate that the use of our conformal parotid - sparing technique conpas leads to a significant decrease of the mean dose in both parotid glands , when elective radiotherapy up to 46 gy is given to the neck nodes . 
we included in our study patients with primary tumors located in either larynx or hypopharynx , because the boost to the primary would not include large parts of the parotids in these cases . 
in this way we could study the merits of our technique in the most favorable situation , without the confounding influence of large primary tumors in other sites ( such as oropharynx ) or nodes , that may generate elective ptvs or even boost ptvs covering larger parts of the parotids . 
when our results are compared to the ones reported in the literature , it should be kept in mind that some planning studies deal with patient categories different from ours [ 11 , 16 , 28 ]  . 
conformal parotid - sparing technique the critical structures cannot be optimally blocked by the multileaf collimator ( mlc ) in some wedged fields , as the use of a wedge determines the angle of the collimator . 
 as the criterion for target coverage we used the percentage of the ptvac receiving at least 95% of the prescribed dose ( v95 ) , which did not differ significantly between both techniques . 
the questions , whether the first 5 mm of tissue below the skin surface really should be considered part of the ptv , and if so , what doses should be aimed at , remain to be answered . 
v95 : percentage of the ptvac receiving at least 95% of the prescribed dose ; v107 : percentage of the ptvac receiving at least 107% of the prescribed dose ; mpd right : mean dose in the right parotid gland ( in gy ) ; mpd left : mean dose in the left parotid gland ( in gy ) ; mocd : mean dose in the oral cavity ( in gy ) ; mscd : maximum dose in the spinal cord ( in gy )  . 
 v95 : prozentsatz von ptvac , wobei zumindest 95% der vorgeschriebenen dosierung aufgenommen wird ; v107 : prozentsatz von ptvac , wobei zumindest 107% der vorgeschriebenen dosis aufgenommen wird ; mpd rechts : mittlere dosis in der rechten ohrspeicheldrse ( in gy ) ; mpd links : mittlere dosis in der linken ohrspeicheldrse ( in gy ) ; mocd : mittlere dosis in der mundhhle ( in gy ) ; mscd : maximale dosis im rckenmark ( in gy )  . 
although forward - planned imrt can generate plans with adequate target coverage and normal - tissue sparing , there is evidence that inverse - planned imrt yields superior plans [ 4 , 23 ]  . 
however , the introduction of inverse - planned imrt will take at least some years for many radiotherapy departments , due to its requirements on many aspects of the planning and treatment process . 
there have also been reports about possible disadvantages of imrt , such as an increased risk of radiation - induced malignancies due to a higher whole - body equivalent dose [ 33 ] and increased cell survival rates in vitro due to the protracted dose delivery with imrt [ 32 ]  . 
in one imrt series of eight patients with oropharynx cancers the contralateral parotid glands could at best be spared to a mean dose of 32.6 gy ( elective dose 54 gy , ctv - ptv margin 5 mm ) [ 2 ]  . 
in another imrt series of seven oropharynx and three larynx cancers , for all but three parotid glands a mean dose of 24 gy was reported ( elective dose 46 gy , ctv - ptv margin not mentioned ) [ 4 ]  . 
in a series of 67 patients with nasopharynx carcinoma treated with imrt , planned with four different planning systems , dvh statistics , but no mpds were reported , showing a considerable range in strahlenther onkol 2005 no . 
mean dvhs of the parotid glands ( n = 20 ) and the ptvac ( n = 10 ) of all patients using either the conventional technique or conpas for the treatment of the primary tumor and the bilateral neck up to 46 gy . 
mittlere dvhs in ohrspeicheldrsen ( n = 20 ) und ptvac ( n = 10 ) von allen patienten , bei denen entweder die herkmmliche technik oder conpas fr die behandlung des primren tumors und des halses bilateral bis zu 46 gy zum einsatz ka table 4 . 
inverse - planned imrt is used for almost all head - and - neck sites , whereas we describe conpas only for larynx and hypopharynx tumors [ 2 , 8 , 10 , 24 , 29 ]  . 
other factors that may explain the variation of reported mpds are the chosen ctv - ptv margin [ 1 ] , prescribed elective dose , cranial border of the ctv [ 3 ] , and perhaps the planning system [ 17 ]  . 
in some imrt series , sparing of the parotid glands is not aimed at , with the consequence of mpds far > 26 gy [ 10 , 21 ]  . 
the variability in reported mpds and lack of data on oral cavity dose with inverse - planned imrt makes it hard to define the place of conpas relative to imrt , with respect to parotid sparing and xerostomia prevention . 
 use , at least in a number of their patients , an irradiation technique that spares the parotids like in conpas , namely by avoiding the lateral part of the parotids , and not the cranial part , as in the conventional technique . 
however , the mocds in the henson study appear to be slightly lower than those used with conpas , the influence of which on subjective xerostomia is uncerta chao et al . 
but since it is unlikely that a movement will take place in the same direction during each fraction , these effects will most likely cancel out to a very large extent . 
vergleich der berechneten und gemessenen dosisverteilung in der axialen ebene , 6 mm kranial zum isozentrum . 45 cgy 70 cgy 95 cgy 120 cgy 140 cgy 165 cgy 190 cgy 210 cgy without shift with 2 mm shift wiggenraad r , et al . 
we expect comparable results with respect to maintenance of saliva production and prevention of xerostomia with conpas , first , because conpas may keep the mean dose in many cases in both ( and not only one , as in the maes study ) parotids < 26 gy and second , because the mean doses in the oral cavity and submandibular glands in the maes study are , based on the dose distributions shown in the article , probably not much different from those with conpas . 
are not in accordance with the other ones mentioned , because they report that their parotid - sparing technique did not prevent xerostomia in most patients who had an mpd < 26 gy [ 6 ]  . 
especially if one considers that there will be some smearing out of the possible dose peaks or gaps because of interfraction patient movement , hardly any effect will rema the measurement of the worst - case scenario regarding intrafraction movement , being a 2 - mm shift between the left and right oblique fields , revealed 100 150 200 figure 9 . 
conformal parotid - sparing technique conclusion this 3 - d conformal technique ( conpas ) enables clinically relevant parotid sparing in bilateral elective neck irradiation with non - modulated beams , without compromising target coverage . 
conpas is relatively easy to implement in departments that have not yet started an imrt progra acknowledgment the authors would like to thank jaap van egmond , bsc , for his help in the preparation of the figures . 
 strahlentherapie und onkologie originalarbeit der einfluss ionisierender strahlen auf die entwicklung der sekundrkatarakt in vitro barbara dietl1 , sascha hunner2 , wolfgang herrmann2 , jrg marienhagen3 , michael mller2 , chris lohmann2 , veit - peter gabel2 hintergrund und ziel : histologisch entspricht die sekundrkatarakt ( posterior capsule opacification [ pco ] ) regenerativem gewebe aus transformierten linsenepithelzellen ( lens epithelial cells [ lec ] ) und extrazellulrmatrix . 
der versuch galt als beendet , wenn die linsenkapsel durch konfluierende zellproliferate vollstndig getrbt war . ergebnisse : eine radiatio mit elektronen verzgert signifikant die entwicklung einer pco im dosisbereich von 812 gy in vitro . 
 schlsselwrter : inhibition der sekundrkatarakt proliferationsinhibition von linsenepithelzellen bestrahlung gutartiger erkrankungen radiobiologische modelle strahlenther onkol 2005 ; 181 : 5159 doi 10.1007 / s00066 - 005 - 1365 - z the influence of ionizing radiation on the development of posterior capsule opacification in vitro background and purpose : histologically , the posterior capsule opacification ( pco ) corresponds to regenerative tissue of transformed lens epithelial cells ( lecs ) with extracellular matrix production . 
 material and methods : each four and 14 pork lenses , respectively , were irradiated with 6 mev electrons with single doses of 8 , 10 , 12 , and 20 gy . 
 results : single dose irradiation with electrons in a dose range from 8 to 12 gy significantly protracted the development of pco with complete inhibition of pco after application of 20 gy . 
nach entfernung der getrbten linse proliferieren residuelle linsenepithelzellen ( lens epithelial cells [ lec ] ) , wandern auf den hinteren kapselsack aus und produzieren extrazellulre matrix mit konsekutiver trbung der optischen achse und klinik der pco [ 1 , 21 , 22 ]  . 
 ballonkatheterinduzierten vaskulren restenosen warfen die frage auf , ob ionisierende strahlen auch die entstehung der pco reduzieren oder inhibieren knnen [ 13 , 20 , 30 , 31 ]  . 
unter sterilen bedingungen im zellkulturlabor wurde durch einen schnitt im bereich der pars plana der bulbus kreisrund erffnet , und die linse wurde mit einer feinen schere unter dem operationsmikroskop bei zwlffacher vergrerung von den zonulafasern abgelst . 
 im anschluss an die radiatio wurden die linsen mit histoacrylkleber ( histoacryl , braun melsungen ) in einem linsenhalter aus va - stahl ( eigenherstellung der werkstatt der universitt , durchmesser der ffnung 9 mm ) fixiert . 
die im linsenhalter fixierten linsenkapseln wurden dann in einer kulturschale mit dulbeccos modified eagle medium unter zugabe von penicillin , streptomycin 10 000 u / ml und klberserum bei 48 - stndigem mediumwechsel kultiviert . 
siemens ( primus ) mit elektronen der energie 6 mev und einer dosisleistung von 300 cgy / mzur dosishomogenisierung wurde ein gewebequivalenter flap von 1 cm dicke auf die geschlossenen kulturschalen gelegt . der versuchsaufbau entsprach einer properativen radiatio ; das intervall zwischen radiatio und linsenextraktion betrug ca . 
der progress der proliferationsbedingten trbung wurde alle 2448 h durch ein makroskop ( leica ) bei zwlffacher vergrerung beobachtet und auf diafilm ( kodak epy 64 ) unter definierten bedingungen photodokumentiert . 
 diese daten wurden gegen die zeitachse ( tag 1 : beginn der proliferation letzter untersuchungstag , tag x : vollstndige konfluenz ) aufgetragen , um die proliferationsaktivitt der lec graphisch darzustellen . 
7 tagen eine vollstndige konfluenz erkennbar war ( mittlere konfluenzzeit 6 , 5 tage , standardabweichung 0 , 57 ) , induzierten 8 gy nach durchschnittlich 12 , 75 tagen ( standardabweichung 2 , 21 ) , 10 gy nach durchschnittlich 17 tagen ( standardabweichung 1 , 41 ) eine vollstndige konfluenz . 
nach 20 gy proliferierten ber einen beobachtungszeitraum von 30 tagen lediglich zwei der 14 proben sprlich , ohne erreichen des konfluenzstadiums ; die brigen zwlf proben wiesen kein makroskopisch sichtbares wachstum auf . 
inhibition der sekundrkatarakt durch ionisierende strahlen statistische auswertung die daten wurden mit dem exakten jonckheere - terpstratest4 ( 0 , 05 ) ausgewertet ( statxact 6.01 , cytel software )  . die wachstumsverzgerung in den bestrahlungsserien war gegenber der kontrollserie ohne radiatio nach applikation von 8 und 12 gy statistisch hochsignifikant ( p = 0 , 0000 ) , ebenso zwischen den einzelnen serien ( p = 0 , 0000 )  . 
nach entfernung der katarakt proliferieren residuelle lec ausgehend von der quatorregion [ 21 , 22 ] und transformieren unter expression von - sma ( smooth muscle actin ) zu myofibroblasten [ 15 ] , wodurch sie mobil werden und auf das hintere kapselblatt wandern . 
 an der genese der pco sind vorwiegend zwei zytokine beteiligt : bfgf ( basic fibroblast growth factor ) stimuliert die mitosen der lec , whrend tgf - ( cid : 3 ) ( transforming growth factor ) die proliferation epithelialer zellen inhibiert sowie die fibromuskulre transformation der lec und die bildung extrazellulren kollagens aktiviert [ 26 ]  . unmittelbar postoperativ sinkt tgf - ( cid : 3 ) auf ein minimum , so dass whrend dieser periode der effekt von bfgf dominiert und die zellen proliferieren [ 16 , 29 , 34 ]  . 
23 wochen postoperativ normalisieren sich die bfgf - spiegel wieder ; unter dem zunehmenden einfluss von tgf - ( cid : 3 ) transformieren die lec unter expression von - sma [ 15 ] zu myofibroblasten - artigen zellen [ 5 ] , produzieren extrazellulre matrix und haften an der hinteren kapsel an [ 16 ] , wo sie epitheliale perlen bilden [ 12 ]  . 
 simultan wandern im rahmen der wundheilung lymphozyten und makrophagen unter sekretion proinflammatorischer zytokine ein , wodurch die proliferation der lec und die produktion extrazellulrer matrix weiter stimuliert werden [ 18 , 19 , 35 , 36 ]  . 
das von monozyten , epithelialen zellen und fibroblasten gebildete interleukin 6 wurde 3 tage nach einer kataraktoperation in 4 000fach erhhten spiegeln in der kammerflssigkeit operierter patienten nachgewiesen [ 10 , 14 ]  . 
 neben einer optimalen operationstechnik wren zur inhibition der pco eine annhernd 100%ige entfernung residueller lec zum zeitpunkt der kataraktextraktion sowie eine maximale suppression inflammatorischer prozesse erforderlich [ 7 ]  . 
durchschnittliche zeitintervalle ( in tagen ) bis zur vollstndigen trbung der hinteren linsentasche durch proliferierende linsenepithelzellen in abhngigkeit von der bestrahlungsdosis ( n = 4 / serie , durchschnittswerte als balkendiagramm )  . 
mean time ( in days ) to complete opacification of the posterior capsule by proliferating lec in dependence on radiation dose ( n = 4 / trial , mean values as bars )  . 
 ionisierende strahlen wirken antiproliferativ und antiinflammatorisch [ 28 ] , mglicherweise aufgrund der hohen radiosensibilitt von lymphozyten , die bereits nach 2 gy in der interphase zugrunde gehen [ 27 ]  . 
 [ 11 ] zeigten erstmals , dass 5 gy einzeldosis mit photonen ( 6 mv ) bei kaninchen - lec in vitro eine wachstumsverzgerung induzierten , 30 gy einzeldosis nach 9 tagen eine avitalisierung der zellen zur folge hatten . 
 die gleiche arbeitsgruppe implantierte in vivo einen mit 32p ( halbwertszeit : 14 , 3 tage ) beschichteten kapselspannungsring in die linsentasche von kaninchen , um die in der regenerativen quatorialzone lokalisierten zellen gezielt zu bestrahlen . 
im gegensatz zur in - vitro - situation kam eine ldr - ( low - dose - rate - ) radiatio zur anwendung mit einer dosis von 15 gy nach fnf halbwertszeiten . 
die wirkung ionisierender strahlen auf benigne zellen wurde in vorklinischen experimenten in vitro untersucht und ergab vergleichbare resultate bei glatten muskelzellen und endothelzellen : dosen < 10 gy verzgerten die proliferation der smc ( smooth muscle cells ) und endothelzellen , erst dosen > 15 gy bewirkten eine proliferationsinhibition [ 4 ]  . mglicherweise induzieren ionisierende strahlen eine prmature seneszenz der bestrahlten , zu myofibroblasten transformierten lec [ 9 , 24 ] und damit eine dosisabhngige verzgerung bzw . 
 wegen der radiogenen gefhrdung der unmittelbar in der nachbarschaft lokalisierten risikostrukturen cornea , corpus ciliare und retina gibt es keinerlei klinische erfahrungen bezglich der wirkung derartig hoher einzeldosen am auge . 
dennoch existieren indirekt klinische beobachtungen ber eine potentielle wirkung ionisierender strahlen zur prvention der pco bei patienten nach ganzkrperradiatio ( total body irradiation [ tbi ] ) im rahmen einer knochenmarktransplantation . 
bei einem kollektiv von 494 patienten eine geschtzte 5 - jahres - kataraktinzidenz nach tbi von 23% ( 42 / 494 patienten ) an ; 38 patienten wurden einer bilateralen kataraktentfernung unterzogen und erhielten eine kunstlinse [ 2 ]  . 
nach einer medianen nachbeobachtungsperiode von 39 monaten entwickelten lediglich 10% der tbipatienten eine pco , im gegensatz zu einer pco - inzidenz von 50% bei der normalbevlkerung in einem vergleichbaren zeitrau neben einer kombinierten wirkung ist mglicherweise die chemobzw . 
wir konnten prinzipiell zeigen , dass ionisierende strahlen ( elektronen der energie 6 mev , dosisleistung 300 cgy / min ) in vitro im dosisbereich allerdings waren in unserer versuchsanordnung smtliche radiosensiblen strukturen der augenvorderkammer in das bestrahlungsvolumen inkludiert . 
8 urban & vogel strahlentherapie und onkologie original article 12 years experience with intraoperative radiotherapy ( iort ) of malignant gliomas patrick schueller1 , oliver micke1 , stefan palkovic2 , johannes schroeder2 , christos moustakis1 , frank bruns1 , andreas schuck1 , hansdetlef wassmann2 , normann willich1 background : even after surgery and radiotherapy , malignant gliomas still have a poor prognosis . 
the authors report on their experience with iort in 71 patients . patients and methods : from may 1992 to february 2004 , 71 patients with malignant gliomas were treated with iort . 
total versus subtotal resection had no significant influence on survival ( p = 0.0741 ) , nor had age , sex , tumor site , performance status , size , primary versus recurrence , and radiation dose . 
3 months after treatment , initial symptoms had improved in 59% ( hemiparesis ) , 50% ( aphasia ) , 50% ( hemianopsia ) , and 60% ( convulsions )  . 
 key words : iort intraoperative radiotherapy brain gliomas strahlenther onkol 2005 ; 181 : 5006 doi 10.1007 / s00066 - 005 - 1354 - 2 12 - jahres - erfahrungen mit der intraoperativen strahlentherapie ( iort ) bei malignen gliomen hintergrund : auch nach resektion und strahlentherapie haben maligne gliome nach wie vor eine schlechte prognose . 
die autoren berichten ber ihre erfahrungen mit der iort bei 71 patienten . patienten und methodik : von mai 1992 bis februar 2004 wurden 71 patienten mit malignen gliomen mit iort behandelt . 
52 / 71 patienten wurden primr mit 20 gy iort + 60 gy postoperativer radiotherapie behandelt , 19 / 71 patienten mit rezidiven erhielten nur eine iort ( 2025 gy )  . ergebnisse : die komplikationsraten betrugen 1 , 4% fr wundinfektionen und 5 , 6% fr blutungen . 
der resektionsstatus hatte keinen signifikanten einfluss ( p = 0 , 0741 ) , ebenso wenig alter , geschlecht , lokalisation , allgemeinzustand , gre , primrtumor versus rezidiv und bestrahlungsdosis . 
3 monate nach therapie hatten sich die initialen symptome in 59% ( hemiparese ) , 50% ( aphasie ) , 50% ( hemianopsie ) und 60% ( krampfanflle ) gebessert . 
 schlsselwrter : iort intraoperative radiotherapie gehirn gliome 1 department of radiotherapy and radiation oncology , university hospital muenster , germany , 2 department of neurosurgery , university hospital muenster , germany , received : august 6 , 2004 ; accepted : may 13 , 2005 strahlenther onkol 2005 no . 
after radical surgery and subsequent external - beam irradiation , median survival times for patients with glioblastoma multiforme ( gbm ) range from 9 to 12 months [ 11 , 15 , 37 ]  . 
the median life expectancy of patients with grade iii gliomas is higher ( depending on the exact histology ) and amounts to about 2030 months after surgery and postoperative radiotherapy ; retrospective results of > 40 months have been scarcely reported [ 11 , 15 ]  . 
published a case - control study comparing postoperative external - beam irradiation alone versus iort followed by external - beam irradiation that did not show any significant improvement for the iort patients . 
the results are presented here together with historical data from other patients who received standard postoperative external - beam irradiation during a similar time period ( thus serving as control )  . 
the female : male ratio amounted to 23 : 48 , the median age to 56 years ( 3182 years )  . the 52 patients treated with iort as a first - line therapy were compared with 65 control patients treated between 1990 and 1996 who only received surgery and postoperative external - beam irradiation . 
 treatment first - line therapy consisted in surgery , 20 gy electron - beam iort , and 60 gy postoperative external - beam irradiation in conventional fractionation ( 5 2 gy / week )  . 
to enable complete irradiation of the resection cavity , the craniotomy had to surround the tumor region by a margin of at least 2 cthe operation was usually done using a stereotactically guided neuronavigation syste after complete resectable 1 . 
 histological examination yielded grade iii glioma in 26 / 71 cases ( 21 anaplastic astrocytomas [ aas ] , four oligodendrogliomas , and one ependymoma ) and gbm in 45 / 71 cases . 
from 2003 on , iort dose was reconstructed by a trigonometric calculation of virtual gantry and table angles ( relative to the postoperative ct data ) from the irradiation angles measured by the neuronavigation system , which enabled us to use a standard treatment planning software ( cadplan , varian medical systems , palo alto , ca , usa ) for retrospective electron - beam calculation and quality control . 
iort of malignant gliomas tion , the resection cavity was measured in all three dimensions by the radiotherapist and filled up with wet , i.e. , tissue - equivalent , cotton strips . 
 in the more recently treated patients , the neuronavigation system was also used to determine the intended beam direction by means of a specially constructed device called the bdi ( beam direction indicator )  . 
in the operating room , the neuronavigation pointer was adjusted to the optimal direction of the electron beam by the radiation oncologist and the neurosurgeon using three - dimensional data from the preoperative ct scan . 
the gantry angle of the linear accelerator and the position of the mobile operating table were then adjusted to the intended beam direction by the following method : a laser was mounted on the tray in such a way that the laser indicated the central beam axis . 
the operating table mounted on a special transporter so that its height could be individually adjusted was then turned until the angle of the bdi device could be matched by turning the gantry only . 
the table position , height and gantry angle were then adjusted until the central beam laser matched the pointer at the end of the bdi device ( figure 2 )  . 
 the electron cone in some cases modified with individual lead absorbers was selected according to the diameter of the resection cavity including a safety margin of at least 1 cthe electron energy was chosen according to the depth of the resection cavity including a margin of at least 1 cafter the application patients were brought back to the operating room to close the craniotomy wound . 
the angle and position of the beam are correct if the laser beam shines through the hole in the center of the gray cylinder ( red light at the bottom of the white cylinder )  . 
einstellung des operationstischs und gantrywinkels mit hilfe des bdi und eines lasers , der entlang dem zentralstrahl verlu winkel und zentrierung des strahls sind korrekt , wenn der laser durch die bohrung im zentrum des grauen zylinders scheint ( rotes licht am unteren ende des weien zylinders )  . 
iort of malignant gliomas follow - up follow - up examinations in 3 - month intervals consisted of ct and / or mri scans , scintigraphic controls with imt - spect and neurologic examination . 
median follow - up for all patients amounted to 15.2 months ( iort ) and 19.7 months ( control )  . statistics primary endpoints were overall survival and disease - specific survival , and freedom from progression ( ffp )  . 
overall survival showed similar figures : glioma iii : median survival 14.9 months , 2 - year survival 26.9% , 5 - year survival 11.5% ; gbm : median survival 12.2 months , 2 - year survival 5.8% , 5 - year survival 0.0%. 
age , sex , extent of resection , tumor site , karnofsky performance index , primary or recurrence , tumor size , iort dose , iort electron energy , and postoperative dose had no significant influence . in a cox multivariate analysis for disease - specific survival with the backward conditional model and the variables age , sex , tumor grade , tumor site , karnofsky performance index , extent of resection , primary or recurrence , tumor size , iort dose , iort electron energy , and postoperative dose , none of the variables reached significance . the 71 iort patients were compared to a historical control group of 65 conventionally treated patients ( see table 1 )  . 
 complications perioperative complications were not increased compared to complications after surgery alone ( one infection , four hemorrhages , one massive brain edema , three femoral vein thromboses , two pulmonary embolisms )  . 
iort of malignant gliomas symptoms discussion the majority of patients could benefit from a remission of their neurologic symptoms ( measured at the first follow - up exam 3 months after treatment ) after the combined treatment of surgery , iort and external - beam radiation ( figure 5 )  . 
the median karnofsky status before therapy for all patients was 70% ; 6 months after therapy it increased to 80% . dose reconstruction starting in august 2003 , six patients have been treated using the described improved method of neuronavigation treatment planning . 
however , the depth of the tumor bed + a margin of > 1 cm was not sufficiently covered by the 90% isodose in 4 / 5 cases , indicating that the electron energy had initially been chosen too low . 
only in 2 / 4 cases this had been done on purpose because of the immediate proximity of the brain stealso in two cases , rather small electron cones had been chosen so that the peripheral aspects of the tumor bed ( including a safety margin of > 1 cm ) were not sufficiently covered by the 90% isodose . 
treated 30 gbm patients with a combination of iort ( 18.3 gy mean dose ) and external - beam radiotherapy ( 58.5 gy mean dose ) , resulting in a median survival of 30 months and a 2 - year survival of 61% [ 20 ]  . 
 they reported an improved median survival of iort patients ( 14 months ) compared to those treated with external - beam irradiation alone ( 10 months ) [ 7 ]  . 
the few available data include those from ortiz de urbina et al . , who reported on the results of 1020 gy iort in 17 malignant glioma patients and found overall 1 - year survival rates of 67% for aa patients and 56% for gbm patients [ 25 ]  . 
why the concept of increasing the total dose by an intraoperative boost did not yield significantly better results than conventional treatment could by explained by several hypotheses : ( 1 ) no further benefit beyond 60 gy . 
these include the use of neutrons [ 9 , 14 ] , heavy particles [ 6 ] , boron neutron capture therapy [ 2 ] , radiosensitizers [ 21 , 26 ] , hyperthermia [ 33 ] , modified fractionation schemes [ 23 ] , conformal radiation therapy [ 16 ] , high - dose - rate interstitial brachytherapy [ 29 ] , iodine - 125 seeds [ 13 , 32 ] , stereotactic radiosurgery [ 4 , 8 ] , and last but not least iort [ 7 , 20 , 25 ]  . 
the vast majority of these studies showed an increased rate of radiation necrosis without an improvement in overall survival . ( 2 ) tumor regrowth at the edge or outside high - dose area . ( 3 ) selection bias . 
this is improbable because the key parameters between the iort patients and control group were similar . ( 4 ) insufficient coverage of the target volume ( angle error , low electron energy , small electron cone )  . 
because of the special situation encountered in electron - beam iort on a mobile operating table , the usual treatment planning process ( ct ( cid : 1 ) dose calculation ( cid : 1 ) beam setup ) with its high precision [ 10 , 31 , 38 ] cannot be performed . 
due to several possible errors , this can lead to an insufficient target volume coverage ( beam angle , beam position , cone size , electron energy ) and to high radiation doses in normal brain tissue [ 5 ] with subsequent radiation necrosis [ 1 ]  . 
posttreatment quality control was performed by a coordinate transformation from the neuronavigation to the postoperative planning ct , making it possible to calculate the dose distribution of the electron beam relative to the resection area . 
 the analysis of the five cases treated so far by this method showed that in general , there are two dangers : ( 1 ) a large risk of choosing too low an electron energy and ( 2 ) a small risk of choosing too small a cone . 
a current meta - analysis including > 3 , 000 patients from twelve randomized trials could show a 2 - month increase in median survival duration for patients treated with additional chemotherapy [ 34 ]  . 
 could show a significant improvement in progression - free and overall survival for patients treated with irradiation and temozolomide versus irradiation alone [ 36 ]  . finally , it is interesting to note that we did not find any significant difference in outcome between primary tumors and recurrences . 
this means that for patients with recurrent malignant gliomas , iort was able to achieve the same median survival again ( calculated from the time of recurrence ) as at the time of primary treatment ( calculated from the time of initial diagnosis )  . 
possible indications for iort might be relatively small ( < 56 cm ) recurrent gliomas iii or primary or recurrent gbm , located at the periphery of the brain , with no risk structures in the immediate neighborhood , when alternative techniques ( radiosurgery , brachytherapy ) cannot be used . 
brmswig2 , stefan knemann1 , claudia rbe3 , stefan hesselmann1 , dorothea riesenbeck1 , ekkehard horst4 , tobias blling1 , michael paulussen5 , heribert jrgens5 , normann willich1 purpose : to analyze the effect of pelvic radiotherapy on ovarian function in prepubertal and pubertal girls and young adult women . 
 key words : ovarian function pelvic irradiation strahlenther onkol 2005 ; 181 : 5349 doi 10.1007 / s00066 - 005 - 9500 - 4 ovarialfunktion nach beckenbestrahlung bei mdchen und jungen frauen ziel : analyse des einflusses einer beckenbestrahlung auf die ovarialfunktion bei mdchen und jungen frauen . 
 patienten und methodik : in einer retrospektiven monoinstitutionalen analyse wurden patientinnen evaluiert , die in den jahren 19791998 in der klinik fr strahlentherapie des universittsklinikums mnster bestrahlt worden waren und bei therapie < 30 jahre waren . 
 schlsselwrter : ovarialfunktion beckenbestrahlung 1 department of radiotherapy , university hospital muenster , germany , 2 department of pediatrics , university hospital muenster , germany , 3 department of radiotherapy , university of homburg / saar , germany , 4 department of radiotherapy , university hospital essen , germany , 5 department of pediatric oncology , university hospital muenster , germany . 
radiotherapy to the abdomen and pelvis has frequently been applied to girls and young women with hodgkins disease , ewings sarcoma and nephroblastoma [ 11 , 13 , 24 ]  . 
this surgical procedure takes the ovary out of the high dose area of irradiation and may therefore reduce radiation - associated side effects to the reproductive organs [ 5 , 6 , 8 , 19 ]  . 
apart from radiotherapy , ovarian function can be impaired by ovariopexy itself and also by various chemotherapeutic agents [ 7 , 11 , 15 , 17 , 23 , 29 ]  . 
 in a retrospective monoinstitutional analysis we have evaluated the effect of pelvic irradiation on ovarian function in prepubertal and pubertal girls and young adult women with different malignancies needing pelvic irradiation as part of their treatment protocol . 
 patients and methods study design in a retrospective analysis , ovarian function was evaluated in female patients who had received radiotherapy to the pelvis at the radiotherapy department of the university hospital in muenster , germany , between january 1979 and december 1998 and were between 1 and 30 years of age at the time of irradiation . 
 patients were classified into three groups : ( cid : 127 ) group 1 included patients with irradiation of both ovaries or patients with unilateral ovariectomy and irradiation of the remaining ovary ; ( cid : 127 ) group 2 included patients in whom the ovarian function was possibly affected by radiotherapy , e.g. , patients with potential direct irradiation to both ovaries , definite irradiation to one and potential irradiation to the other ovary or patients who following unilateral ovariectomy had potential irradiation to the remaining ovary ; ( cid : 127 ) group 3 included patients in whom one or both ovaries were definitely not included in the radiation field . 
 diagnosis patients ( n ) hodgkins disease ewings sarcoma nephroblastoma rhabdomyosarcoma osteosarcoma neuroblastoma t cell lymphoma teratoma adenocarcinoma ( gartners duct ) synovial sarcoma pheochromocytoma dysgerminoma keloid heterotopic ossification unspecified sarcoma total group 1 hormonal evaluation was possible in ten of 16 patients . 
two of them were still prepubertal at the time of evaluation ; one had turners syndrome with gonadal dysgenesis , and it could not be distinguished whether hormonal levels were unnormal due to the treatment or due to the syndrome . 
the diagnoses of patients treated with hormonal failure were hodgkins disease ( four patients ) , ewings sarcoma ( four patients ) , and t - cell lymphoma ( one patient )  . 
the diagnoses of patients treated without signs of hormonal failure were hodgkins disease ( four patients ) , nephroblastoma ( three patients ) , neuroblastoma ( one patient ) , rhabdomyosarcoma ( one patient ) , and keloid formation ( one patient )  . 
in patients without hormone failure in group 3 , the median age at chemotherapy was 6 years ( range : 9 months to 18 years , one patient without chemotherapy )  . 
the median dose of radiotherapy in patients showing ovarian failure was 40 gy ( range : 2054 gy ) and 24 gy ( range : 1232 gy ) in the group of patients without signs of ovarian failure . 
furthermore , in patients with ewings sarcoma of the pelvis , with nephroblastoma and with rhabdomyosarcoma of the genitourinary tract [ 13 , 24 ] , pelvic irradiation may be necessary . 
a number of drugs carry a particularly high risk of inducing ovarian failure , i.e. , cyclophosphamide , ifosfamide , cisplatinum , vinblastine , busulfan , bcnu , and ccnu [ 7 , 11 , 17 , 23 , 29 ]  . 
in patients mostly > 40 years , ovarian doses of 510.5 gy in one to three fractions for hemorrhagic metropathy resulted in ovarian failure in 97% [ 3 ]  . 
there is no indication so far that the offspring of patients who received cancer treatment before conception are at a conceivably higher risk of teratogenic effects or of developing malignancies [ 10 ]  . 
 there is a statistically significant difference in the incidence of ovarian failure amongst the three groups even when the patients with unknown hormonal status are included in the analysis ( table 4 )  . 
the high incidence of ovarian failure is very likely due to the fact that in this group , the ovaries still received a considerable radiation dose and additional chemotherapy was given . 
it was 40 gy ( range : 2054 gy ) in the group of patients that developed hormone deficits and 25 gy ( range : 1232 gy ) in the patients who did not develop ovarian failure . 
the median age at the onset of chemotherapy was 18.5 years ( range : 1321 years , one patient without chemotherapy ) in patients who had ovarian failure and 6 years ( range : 9 months to 18 years , one patient without chemotherapy ) in patients without hormone failure . 
ovarian transposition resulted in ovarian preservation in nearly all patients treated with surgery alone and in about half of the patients treated with external - beam pelvic radiotherapy [ 5 , 19 ]  . 
 conclusion radiation to the pelvis in childhood and adolescence is associated with a considerable risk of ovarian failure , particularly when one or both ovaries are included in the radiation field . 
the following points are discussed for each tumor entity : biological background for the pet investigation , sensitivity and specificity of pet ( with different tracers ) in comparison to computed tomography ( ct ) and magnetic resonance imaging ( mri ) and impact of pet on target volume definition . 
 results : the results of clinical studies on the integration of pet in target volume definition for lung , head - and - neck , genitourinary and brain tumors were analyzed . 
fluorodeoxyglucose - ( fdg - ) pet has a significant impact on gtv ( gross tumor volume ) and ptv ( planning target volume ) delineation in lung cancer and can detect lymph node involvement and differentiate malignant tissue from atelectasis . 
for example , fdg - pet could be superior to ct and mri in the detection of lymph node metastases and unknown primary cancer and in the differentiation of viable tumor tissue after treatment . 
choline pet and acetate pet are promising tracers in the diagnosis of prostate cancer , but their validity in local tumor demarcation , lymph node diagnosis and detection of recurrence has to be defined in future clinical trials . 
the imaging of hypoxia , cell proliferation , angiogenesis , apoptosis and gene expression leads to the identification of different areas of a biologically heterogeneous tumor mass that can individually be targeted using intensity modulated radiotherapy ( imrt )  . 
 key words : pet biological imaging biological target volume radiation treatment planning strahlenther onkol 2005 ; 181 : 48399 doi 10.1007 / s00066 - 005 - 1422 - 7 positronenemissionstomographie in der strahlentherapieplanung ziel : untersuchung der wertigkeit der positronenemissionstomographie ( pet ) fr die strahlentherapieplanung . 
 material und methodik : die arbeit fasst die daten aus der literatur zur integration der pet in die zielvolumendefinition fr die entitten lungen - , kopf - hals , beckenund hirntumoren zusammen . 
fr jede tumorentitt werden folgende punkte diskutiert : der biologische hintergrund der pet - untersuchung , die sensitivitt und spezifitt ( mit verschiedenen tracern ) im vergleich zur computertomographie ( ct ) und magnetresonanztomographie ( mrt ) und der einfluss auf die zielvolumendefinition . 
 ergebnisse : die fluorodesoxyglucose - ( fdg - ) pet hat einen signifikanten einfluss auf die zielvolumendefinition bei lungentumoren , insbesondere in der diagnose pathologischer lymphknoten und in der abgrenzung des tumors von einer atelektase . 
bei 1 department of radiation oncology , klinikum rechts der isar , technical university munich , germany , 2 department of nuclear medicine , klinikum rechts der isar , technical university munich , germany , 3 department of nuclear medicine , scientific institute h . 
pet for radiation treatment planning kopf - hals - tumoren ist der stellenwert der pet noch offen : die fdg - pet knnte der ct und mrt in der diagnose von lymphknotenmetastasen , der suche des primrtumors bei cup und der differentialdiagnostischen abgrenzung des primroder rezidivtumors von einer nekrose nach therapie berlegen sehierdurch knnten die definition des zielvolumens und die schonung des normalgewebes mageblich beeinflusst werden . 
new software and hardware systems , such as stereotactic radiotherapy , radiosurgery , intensity - modulated radiotherapy ( imrt ) and three - dimensional planning of brachytherapy , enable the delivery of radiation treatment with high geometric precision . 
techniques such as positron emission tomography ( pet ) , single - photon emission computed tomography ( spect ) and magnetic resonance spectroscopy ( mrs ) permit the visualization of biological pathways of tumors , giving additional information about metabolism , physiology and molecular biology of tumor tissue . 
 the goal of this review is to present published data on the correlation of radiologic investigation with biological imaging ( pet ) in radiation treatment planning and to discuss which tools of molecular imaging used in experimental models could be useful for radiation treatment planning in the near future . this review examines and summarizes the available literature about the effectiveness of using biological imaging ( pet ) for target volume definition in radiation treatment planning . 
we were not able to find convincing published evidence supporting the integration of pet in the target volume definition of other tumor entities such as lymphoma , breast cancer , gastrointestinal cancer , seminoma , melanoma , sarcoma , etc . 
however , the experience accumulated in the trials presented in this review could be useful for the integration of biological imaging in the radiation treatment planning of other tumor entities . 
 the following points are discussed in this study for each tumor entity : ( 1 ) the biological background for pet investigation with different tracers used in tumor diagnosis ; ( 2 ) the sensitivity and specificity of pet ( with different tracers ) in the detection of tumor tissue , in comparison to traditional radiological investigations , ct and mri ; strahlenther onkol 2005 no . 
they determined whether or not investigation results are conditionally dependent and found that the sensitivity and specificity of fdgpet depend on the presence or absence of enlarged mediastinal lymph nodes on ct . 
the authors concluded that fdg - pet is more accurate than ct for mediastinal staging and more sensitive but less specific when ct shows enlarged mediastinal lymph nodes [ 30 ]  . 
additionally , the plus multicentric randomized trial showed that the addition of pet to conventional work - up prevented unnecessary surgery in one out of five patients with suspected nsclc [ 129 ]  . 
 lung cancer fdg - pet in lung cancer the observation that malignant tumor cells are characterized by increased glycolysis [ 136 ] resulted in the development of whole - body imaging using pet and the fluorine - 18 - ( 18f - ) labeled glucose analog fluorodeoxyglucose ( fdg )  . 
to date , numerous oncologic pet studies have been published and recently summarized according to sensitivity , specificity and accuracy from > 26 , 000 patients [ 27 ]  . 
following phosphorylation by the hexokinase , fdg gets trapped in cells and leads to an uptake into tissue in proportion to the overall glucose metabolisnevertheless , fdg uptake is not tumor - specific , since glucose metabolism is also generally increased in inflammatory processes . recently , weber et al . 
reviewed all clinical trials published between 1995 and 2002 for the use of fdg - pet for preoperative staging of patients with non - small cell lung cancer ( nsclc ) according to the criteria of evidence - based medicine [ 139 ]  . 
the value of fdg - pet in the diagnosis of lymph node metastases in patients with nsclc was investigated in 16 studies including 1 , 355 patients and corresponded to the criteria of the agency for health care policy and research . 
in the studies comparing fdg - pet and ct , the mean sensitivity and specificity of ct alone remained at 66% ( 5873% ) and 71% ( 6576% ) , respectively . 
five analyses of cost effectiveness from the usa , japan and germany demonstrated that fdg - pet improved the outcome of treatment and reduced or only minimally increased the overall cost [ 139 ]  . 
patient with lung cancer investigated on integrated pet / ct ; upper left : fdg - pet , upper right : ct , lower left : fusion imaging pet / ct , lower right : ct ( lung windowing )  . 
patient mit bronchialkarzinom untersucht mit pet - ct ; oben links : fdg - pet , oben rechts : ct , unten links : pet / ct - fusion , unten rechts : ct ( lungenfenster )  . 
 fdg - pet in target volume definition of lung cancer eleven published clinical trials including 415 patients are currently available to assess the impact of fdg - pet on radiation treatment planning ( table 1 )  . 
in the remaining 23 / 35 cases ( 66% ) , the pet target volume was equal to or smaller than the ct target , although these cases were not analyzed . 
nine of the twelve patients with changes in radiation field size presented atelectasis , suggesting that fdg - pet plays an important role in radiation treatment planning , particularly in patients with tumor - associated atelectasis , causing a substantial reduction in irradiation field size [ 96 , 122 ]  . 
 of the 73 patients with histologically proven metastatic lymph nodes , 65 ( 89% ) tested positive by pet and ct , while ct alone detected lymph nodes in 55 patients ( 75% )  . 
a virtual radiotherapy planning based on ct / pet - fused images and on ct alone was performed and a comparison of the gtv and the ptv , defined by the two different approaches , was analyzed . 
 fdg - pet modified the gtv definition in 5 / 12 patients due to a more accurate lymph node , tumor tissue and distant metastasis detection [ 28 ]  . 
prospectively compared gtv and ptv based on ct alone versus combined ct and fdg - pet imaging in 30 patients ( stage iaiiib ) whose tumors were poorly defined by ct . 
in five ( 22% ) of the remaining 23 patients , positive lymph nodes located within 5 cm of the primary tumor were detected in pet images and included in the gtv definition . 
an important result of the study was the fact that the interobserver variability of gtv and ptv definition may be significantly reduced using the additional information of fdg - pet [ 80 ]  . 
 in 4 / 11 patients , the ptv decreased ( average 18% , range 248% ) , and in 7 / 11 patients , the ptv increased ( average 19% , range 546% )  . 
importantly , the interobserver variability in gtv delineation by two different radiation oncologists was significantly reduced , when pet / ct was used in comparison to ct alone [ 15 ]  . 
in three cases pet helped to distinguish tumor from atelectasis , in ten patients it detected unsuspected nodal disease , and in one patient a second tumor was found in the same lobe of the lung . 
 fdg - pet in lung cancer : discussion and conclusion the role of fdg - pet in the radiation treatment planning of lung cancer has been investigated thoroughly in a total of 415 patients and eleven trials . 
the percentage of cases presenting significant changes in tumor volume after the integration of fdg - pet investigation in the radiation treatment planning ranged from 21% [ 78 ] to 100% [ 22 ]  . 
in addition , the improvement of delineating malignant tissue from atelectasis using fdg - pet instead of ct has been demonstrated [ 9 , 15 , 22 , 28 , 78 , 96 , 122 ]  . 
on the other hand , the enhanced fdg uptake in inflammatory diseases might limit the use of fdg - pet in radiation treatment planning [ 58 , 62 ]  . 
 however , as gtv delineation is a fundamental step in radiation treatment planning , the use of combined ct / pet imaging for all dose escalation studies with either conformal radiotherapy or imrt has been recommended by the rtog as a standard method in lung cancer [ 13 ]  . 
 head - and - neck cancer fdg - pet in head - and - neck cancer sensitivity and specificity of fdg - pet , ct and mri in the detection of lymph node matastases in patients with head - andneck cancer were evaluated in 7 studies including 452 patients [ 1 , 6 , 42 , 57 , 82 , 98 , 126 ]  . 
in comparison to fdg - pet , the sensitivity and specificity of ct and mri were in many studies lower , ranging from 64% [ 126 ] to 95% [ 6 ] and from 41% [ 57 ] to 97% [ 6 ] , respectively . 
false - positive fdg - pet findings occurred in inflammatory lymph nodes and in some structures such as tonsils and salivary glands , where fdg uptake may have been increased . 
 the role of fdg - pet in detecting unknown primary tumors in the head - and - neck area in patients with cervical lymph node metastases was investigated in ten studies including 278 patients [ 3 , 8 , 32 , 41 , 51 , 53 , 61 , 65 , 71 , 112 ]  . 
 fdg - pet plays an important role in differentiating between residual / recurrent tumor and unspecific posttherapeutic changes [ 24 , 54 , 66 , 75 , 76 ]  . 
studied 34 patients with histologically confirmed squamous cell carcinoma of the head and neck by performing fdg - pet prior to treatment planning in addition to conventional staging procedures , including ct , mri and ultrasound . 
 the integration of fdg - pet in radiation treatment planning led to significant changes in the radiation field and dose in 9 / 22 patients ( 44% ) with a primary tumor and in 7 / 12 patients ( 58% ) with tumor recurrence . 
the authors concluded that the image fusion between fdg - pet and mri / ct was useful in gtv , ctv and ptv determination , both for encompassing the whole tumor area in the irradiation field and for sparing of normal tissue [ 97 ]  . 
 therefore , noninvasive measurement of the hypoxic fraction in individual tumors using radioactive tracers is an appealing concept , which ultimately might lead to the individualization of specific hypoxia - adapted treatment regimens and enhance local tumor control after radiotherapy . 
the most important factors are the specificity of the retention mechanism , the amount of tracer delivery in a perfusion - limited microenvironment , and the amount of unspecific metabolites . 
these parameters ultimately influence the target - tobackground ratio which determines the ability to detect tissue hypoxia ( sensitivity ) and the range of oxygen concentration that defines the radiobiological oxygen effect , in other words the prediction of tumor response to therapy ( specificity )  . 
 it is unfortunate for imaging purposes that tissue hypoxia often occurs only after a significant decrease in tissue perfusion , since the reduction in blood flow to < 10% of normal values critically reduces tracer delivery [ 77 , 99 ]  . 
most importantly , an oxygen - specific retention mechanism should determine the amount of tracer that is temporarily or permanently trapped in hypoxic tissues in order to detect viable cells that are indeed hypoxic . 
 several bioreductive substances have been evaluated as hypoxia tracers , mainly nitroimidazole compounds ( i.e. , [ 123i ] iodoazomycin arabinoside , [ 123i ] iaza ; [ 18f ] fluoromisonidazole , [ 18f ] fmiso ; [ 18f ] azomycin arabinoside , [ 18f ] faza ) , where the bioreductive molecule accepts a single electron , leading to free radical metabolites that are further reduced and bound to cell constituents under hypoxic conditions . 
 these experiments also demonstrated that [ 18f ] fmiso retention occurred at tissue po2 levels that are ( radio ) biologically relevant , thus between approximately 2 and 10 mmhg . 
the superior spatial resolution of pet compared to spect and the possibility to determine truly quantitative measurements favors [ 18f ] - labeled compounds such as [ 18f ] fmiso , which is currently being used in several cancer centers worldwide . 
 more recently , [ 18f ] faza was synthesized for pet imaging taking advantage of a faster blood clearance of azomycin arabinoside compounds yielding more favorable tumor - to - background ratios in various murine tumors . 
in addition , an inverse relationship of the [ 18f ] faza retention under high and low oxygenation was demonstrated in hypoxic murine tumors using repeated small - animal pet studies [ 109 ]  . 
 besides nitroimidazole compounds , metal complexes such as [ 99mtc ] - labeled dioximes ( [ 99mtc ] hl91 ) and [ 60cu ] - labeled methylthiosemicarbazone ( [ 60cu ] atsm ) , being bioreductive molecules themselves , have been proposed for tumor hypoxia imaging . 
showed visible [ 99mtc ] hl91 tumor uptake in a variety of different tumors , some of them also being able to be identified with [ 18f ] fdgpet [ 17 ]  . 
this mechanism is due to the irreversible reduction of cu ( ii ) to cu ( i ) in a disturbed electron flow ( in viable mitochondria ) caused by the depletion of the final electron acceptor oxygen [ 72 ]  . 
using tissue po2 measurements with needle electrode systems , animal studies have demonstrated that this agent is a promising , selective diagnostic marker for hypoxia imaging [ 26 , 8588 ]  . 
the generation of highresolution maps of hypoxic tumor microenvironment remains the goal of hypoxia imaging and offers the prospect of guiding the application of higher radiation doses to resistant tumor sites . 
the imrt plan delivered 80 gy in 35 fractions to the atsm - avid tumor subvolume ( hgtv ) and the gtv simultaneously received 70 gy in 35 fractions , keeping the radiation dose to the parotid glands < 30 gy . 
used [ 18f ] misonidazole scans to detect hypoxia in patients with t3 / 4 , n2 / 3 head - and - neck tumors treated with tirapazamine , cisplatin and radiation therapy . 
14 of 15 patients were hypoxia - positive at the beginning of the treatment , but only one patient had detectable hypoxia at the end of radiochemotherapy [ 118 ]  . 
 fdg - pet and hypoxia - pet in head - and - neck cancer : discussion and conclusion the value of fdg - pet for radiation treatment planning in head - and - neck cancer is still under investigation . 
questions that remain open regarding the best hypoxia imaging strategy are : the relationship to current gold - standard methods to measure tissue hypoxia in vivo and the dynamic changes in tumor hypoxia . 
however , if future studies demonstrate that hypoxic areas can accurately be visualized using pet , this could have a significant impact on radiation treatment and monitoring , not only in head - and - neck cancer but also in other malignancies . 
considering the high frequency of this tumor , the dose related curative chance of radiation treatment and the high importance of rectum sparing , precise visualization of the primary tumor and lymph node metastases as well as of the recurrences after treatment are of eminent importance for the planning of the radiation therapy . 
 fdg - pet in prostate cancer the low glucose uptake , the significant overlap of tracer uptake in tumor and in the benign prostate hyperplasia and the renal excretion of fdg into the bladder limit the diagnosis of prostate cancer using fdg - pet [ 21 , 49 , 124 ]  . 
found a sensitivity of 67% in the detection of primary disease in prostate cancer patients with localized disease and of 92% in patients with advanced stage disease [ 103 ]  . 
however , the results of fdg - pet in early stages of prostate cancer are not satisfactory for tumor detection , and other tracers have been intensively evaluated in the recent past . 
the magnitude of choline uptake in tumor cells is generally dependent on two main metabolic steps : the ( nonspecific ) transport from the blood to the tumor cell and the specific phosphorylation of choline catalyzed by the enzyme choline kinase , which is upregulated in cells with a higher rate of proliferation . 
in a feasibility study , they were able to correctly localize known bone and lymph node metastases with the exception of one false - negative lymph node that was < 1 cm in size [ 63 ]  . 
of the 15 patients with histologically proven lymph node metastases , twelve were correctly diagnosed by c11 - choline pet ( true - positive ) , while three were incorrectly staged because of a micrometastasis and bowel activity interfering with lymph node evaluation . 
in summary , in the diagnosis of lymph node metastases of prostate cancer by c11 - choline pet , a sensitivity of 80% , a specificity of 96% and an accuracy of 93% have been reported . 
 in a large group of 100 patients , c11 - choline pet was shown to be a useful technique to restage prostatectomized patients with increasing serum psa ( prostate - specific antigen ) levels . 
it is superior to [ 18f ] fdg - pet and complementary to conventional imaging techniques , although it has the advantage of being able to stage the disease in one single step [ 106 ]  . 
 acetate pet in the diagnosis of prostate cancer besides carbon - 11or fluorine - 18 - labeled choline , carbon - 11labeled acetate ( c11 - acetate ) is also attracting attention as a promising pet tracer . 
the uptake mechanism of c11 - acetate is not completely understood , however , experimental data suggest that c11 - acetate incorporation is higher in tumor tissue with low oxidative metabolism and high lipid synthesis . 
although all six investigated patients with prostate cancer showed a higher tumor uptake compared to normal tissue , a high overlap between malignant and benign prostate tissue ( benign prostatic hyperplasia ) was found [ 56 ]  . 
high c11 - acetate uptake in the prostate was detected in all 22 patients ( sensitivity 100% ) and in three additional patients with unknown metastases in lymph nodes and bone . 
evaluated the effectiveness of c11 - acetate pet in detecting local or systemic recurrent disease by rising psa after prostatectomy ( 30 patients ) or radiation therapy ( 16 patients )  . 
27 / 46 patients ( 59% ) showed abnormalities in c11 - acetate pet , but the analysis was limited only to 14 patients with findings confirmed by ct , bone scintigraphy , or biopsy . 
of the 22 patients with psa levels > 3 ng / ml , 13 ( 59% ) showed positive results on c11 - acetate pet , whereas only one of the 24 patients ( 4% ) with psa < 3 ng / ml showed abnormalities on pet . 
unfortunately , sensitivity and specificity of c11 - acetate pet in the detection of local or systemic recurrences could not be defined , since the positive c11acetate pet findings were not confirmed by biopsy or other objective reference standards [ 105 ]  . 
in both trials , fdg - pet was compared to c11 - acetate pet , demonstrating the advantage of c11 - acetate pet in the detection of local or systemic prostate cancer . 
c11 acetate showed an almost complete absence of urinary elimination , and c11 - choline had the advantage of a better - defined uptake mechanis [ 18f ] fdg - pet , c11 - choline pet and c11 - acetate pet in prostate cancer : discussion and conclusion c11 - acetate pet and c11 - choline pet are two promising tracers in prostate cancer . 
however , their validity in local tumor demarcation , lymph node diagnosis , and the detection of recurrences and distant metastases needs to be clearly defined in future clinical trials . 
clinical trials analyzing cancer location and extent within the prostate , extracapsular spread and cancer aggressiveness in pre - prostatectomy patients have indicated that the metabolic information provided by mrs combined with the anatomic information provided by mri can significantly improve the diagnosis [ 16 , 84 , 92 , 144 , 148 ]  . 
to date , only preliminary data ( two case reports ) are available on the use of fdg - pet in the management of recurrent disease , suggesting that fdg - pet might be useful to differentiate between viable tumor tissue and fibrosis after surgery or radiotherapy [ 83 , 131 ]  . 
 fdg - pet in target volume definition of cervical cancer fdg - pet was integrated in the radiation treatment planning of four patients with cervical cancer [ 95 ]  . 
a smaller and a larger gtv was seen in two out of eight patients , each approximately 25% , and the changes in ptv were about 20% [ 15 ]  . 
the first fdg - pet for tumor volume definition was followed by a second pet , where the fdg tracer was placed inside the tandem and ovoid applicators to visualize the treatment source positions for threedimensional treatment planning . 
the authors concluded that this technique has the potential to improve tumor coverage in patients with cervical cancer , sparing critical structures at the same time [ 81 , 94 ]  . 
 brain tumors gliomas amino acid pet and spect in the diagnosis of brain gliomas the most important radiolabeled amino acids used in the diagnosis of gliomas are carbon - 11 - labeled methionine ( met ) , iodine - 123 - labeled - methyl - tyrosine ( imt ) and fluorine - 18labeled o - ( 2 ) fluoroethyl - l - tyrosine ( fet )  . 
the uptake in tumor cells is mediated by specific l and a amino acid transporters at the level of the blood brain barrier ( bbb ) , independent of the bbb disturbance [ 46 , 116 , 121 ]  . 
the advantage of the amino acid analog fet is that it can be radio labeled with fluorine - 18 , an isotope with a physical half - life ( about 110 min ) longer than that of c11 , so that it can be distributed to pet centers without an on - site cyclotron . 
 although pet offers superior spatial resolution ( 34 mm ) compared to spect ( 78 mm ) , met - pet and imt - spect are comparable in the ability to identify tumor tissue [ 68 , 69 , 138 , 142 , 143 ]  . 
a number of studies provided controversial findings regarding the impact of amino acid tracers on determination of the tumor grade in various brain tumors [ 121 , 137 ]  . 
 amino acid pet and spect in target volume definition of brain gliomas to date , only limited data is available in the literature concerning the value of amino acid tracers in radiation treatment planning of gliomas . 
in 67% of the cases , the spatial extent of increased tracer uptake in gliomas was larger than that of the contrast enhancement on ct / mri images , while in the remaining 33% of the cases , the extent of tumor tissue was diagnosed with comparable accuracy . 
introduced spect ( the tracer used was not mentioned in the study ) and met - pet in radiation treatment planning for interstitial irradiation of brain tumors with stereotactically implanted 125i seeds [ 52 ]  . 
they described their experience in 13 patients and concluded that ct / mri / pet or spect image fusion helped improve accuracy and minimized the perifocal morbidity of interstitial irradiation . 
in comparison with mri , metpet was helpful in outlining the gtv in 3 / 11 cases ( 27% ) , whereas it was complementary to mri in 46% of the cases and less distinctive in 27% [ 100 ]  . we investigated the value of imt - spect in gtv , ptv and the bv definition for radiation treatment planning of brain gliomas . 
based on the mri / spect fusion images , the gtv defined on spect was compared with the volume of hyperintensity regions on t2 - weighted mri and with the volume of gadolinium ( gd ) enhancement on t1 - weighted mri . 
in most cases , the hyperintensity area on t2 - mri included the area with imt - increased uptake in spect , confirming that t2 - changes incorporate both tumor tissue and perifocal edema . 
however , the most striking finding of the study was the observation that the tumor uptake of imt extended up to 2 cm outside t2 - changes in mri in 23% of patients ( 7 / 30 in all cases high - grade gliomas )  . 
comparing the imt uptake to the gd enhancement areas on the t1 - mri / spect fusion images , we observed that the imt tumor uptake incorporated contrast enhancement regions in all cases , even extending outside of the gd - enhancing regions . 
 consequently , we analyzed the impact of imt - spect on gtv , ptv and bv delineation in 66 patients with lowand high - grade gliomas after surgical resection [ 35 ]  . 
since imt - spect can visualize tumor tissue with a higher specificity and sensitivity than anatomic imaging modalities , these findings could significantly modify target volumes for radiation treatment planning . 
in 7 / 39 patients ( 18% ) did met uptake correspond exactly to gd enhancement , whereas in 31 / 39 cases ( 79% ) , the region of met uptake was larger than that of gd enhancement , while in 29 / 39 patients ( 74% ) the gd enhancement area extended beyond the met enhancement . 
met uptake did not correspond exactly to hyperintensity areas on t2 in any patient : in 9 / 18 cases ( 50% ) , met uptake was extended beyond the hyperintensity on t2 , while in 18 / 18 patients ( 100% ) at least some hyperintensity on t2 was located outside of the met enhancement area . 
 a recent analysis of an amino acid spector pet - planned group of patients with recurrent gliomas reirradiated using stereotactic fractionated radiotherapy ( 6 5 gy ) suggests that the integration of amino acid pet or spect in target volume definition might contribute to an improved outcome [ 39 ]  . 
 fdg - pet in brain gliomas the accumulation of fdg in the brain is closely related to glucose metabolis unlike other tissues , the brain utilizes glucose almost exclusively to meet its energy demands . 
additional information from fdg - pet was derived from only a few patients for radiation treatment planning , due to the low contrast between viable tumor and normal brain tissue . 
dose painting based on met - pet / ct image fusion and imrs ( intensity - modulated stereotactic radiotherapy brainlab system ) in a patient with glioblastoma , 2 weeks after surgery ; upper left : metpet , upper right : ct with contrast , lower left : dose distribution on metpet , lower right : dose distribution on ct . 
the met - pet data are co - registered with the ct data and integrated in the imrs planning syste in the same session , the region with high met uptake ( outlined in red ) is treated with 3 gy / fraction ( green area [ total dose 90 gy ] ) ; the region with microscopic tumor infiltration ( outlined in pink ) with 2 gy / fraction ( orange area [ total dose 60 gy ] )  . 
dose painting basiert auf met - pet / ct - bildfusion und imrs ( intensittsmodulierte stereotaktische strahlentherapie brainlab system ) bei einem patienten mit glioblastom , untersucht 2 wochen nach der operation ; oben links : met - pet , oben rechts : ct mit kontrastmittel , unten links : darstellung der dosisverteilung im metpet , unten rechts : darstellung der dosisverteilung im ct . 
die areale mit hoher met - aufnahme ( rot markiert ) werden behandelt mit 3 gy / fraktion ( grnes areal [ gesamtdosis 90 gy ] ) ; die region mit mikroskopischer tumorinfiltration ( pink markiert ) wird behandelt mit 2 gy / fraktion ( oranges areal [ gesamtdosis 60 gy ] )  . 
 met - pet in target volume definition of meningiomas in meningiomas , the gtv is routinely delineated by considering the contrast enhancement areas in ct and mri and bone windowing on ct . 
recently , it was demonstrated that by using met - pet / ct fused images , meningioma borders can be more accurately defined with respect to critical normal organs [ 36 , 128 ]  . 
 amino acid pet and spect and [ 18f ] fdg - pet in gliomas and meningiomas : discussion and conclusion although only preliminary data is available , the presented literature indicates that amino acid pet and spect , in addition to conventional morphological imaging , are superior to the exclusive use of either mri or ct in the visualization of vital tumor extension in gliomas . 
showed that the outcome of patients with tumor infiltration in mrs outside the changes in conventional mri was significantly worse than that of patients without additional information in mrs regarding tumor extension [ 31 ]  . 
 in conclusion , our recent studies showed that pet and spect can be helpful in outlining the residual tumor after surgery and the recurrences after surgery and radiation therastrahlenther onkol 2005 no . 
the role of amino acid pet in gtv definition for meningiomas seems to be helpful in defining the tumor extension in the dura region and has to be systematically analyzed in future studies . 
fdg - pet has only a limited impact on radiation treatment planning of brain tumors , since the high glucose uptake in normal brain tissue complicates the identification of target volumes . 
gene imaging using the established pet reporter gene / reporter probe imaging approach and the herpes simplex type 1 virus thymidine kinase ( hsv1 - tk ) gene would permit the monitoring of the expression of the therapeutic gene ( egr - 1 ) and allow the definition of a target volume , that is likely to respond to such an approach [ 130 ]  . 
the future biological target volume definition might be based on tracers that image different tumor - specific metabolic pathways such as hypoxia ( see above ) , tumor cell proliferation , apoptosis , angiogenesis , and specific gene expression patterns . 
 a possible candidate is the fluorine - 18 - labeled thymidine analog 3 ' - deoxy - 3 ' - [ 18f ] fluorothymidine ( flt ) , which has been shown to correlate with tumor cell proliferation as assessed by the ki - 67 labeling index [ 135 ]  . 
first imaging results using a small - animal pet suggest that this compound is suitable for the noninvasive determination of v ( cid : 3 ) 3 integrin expression [ 44 ]  . 
fdurd was demonstrated to increase 100 - fold in cell cultures irradiated under the prodrug pet may be helpful in obtaining a clearer answer to three important questions : ( 1 ) where is the tumor located and where are the ( macroscopic ) tumor margins ? the co - registration of pet with morphological imaging techniques seems to improve the delineation of viable tumor tissue compared to ct or mri alone . 
therefore , pet allows the definition of a target volume based on a biological paradigm ( btv ) and increases , in some cases , our ability to differentiate between tumor and normal tissue as compared to ct and mri alone . 
however , there are also other tumor entities , in which pet has a high impact on staging , treatment management , and monitoring such as lymphomas , melanomas , breast cancer and gastrointestinal tumors . 
therefore , the concept of btv should be named after the respective tracer ( i.e. , btv ( fdg - pet ) , btv ( faza - pet ) )  . 
 this novel treatment approach will generate a new set of problems and questions such as : what are the dynamics of the visualized biological processes ? how many biological investigations are necessary during treatment and at which points in strahlenther onkol 2005 no . 
although evaluating the response after radiochemotherapy is often difficult due to treatment - induced inflammatory tissue changes , preliminary data in lung [ 14 , 79 ] esophageal [ 11 , 25 ] , and cervical cancer [ 33 ] suggest that the decrease in fdg uptake after treatment correlates with histological tumor remission and longer survival . 
however , the time points at which pet imaging should be performed still need to be defined , as well as the tracer which should be used and the criteria which could be used for the definition of the tumor response in pet . 
therefore , future clinical studies based on integrated pet / ct or on pet / ct / mri image fusion , which compare the outcome of biologically directed treatment with conventional treatment regimes , still need to be conducted for each individual tumor entity before the btv definition can generally be recommended . 
 strahlentherapie und onkologie original article the influence of heterotopic ossification on functional status of hip joint following total hip arthroplasty fabian pohl1 , julia seufert1 , annette tauscher2 , harald lehmann3 , hans - werner springorum2 , michael flentje1 , oliver koelbl1 purpose : the functional failure induced by heterotopic ossification ( ho ) following total hip arthroplasty ( tha ) was analyzed and correlated to the radiologic failure . 
 patients and methods : from july 1997 to july 2001 , 315 patients ( 345 hips ) received tha indicated by a hypertrophic osteoarthritis of higher degree ( kellgren grade iii , iv )  . 
comparing the preand postoperative rom , all patients with brooker grade 0 , i and ii showed a significant improvement of flexion , internal and external rotation , abduction and adduction movement . 
ho of lower degree ( brooker i , ii ) does not influence the clinical outcome , whereas ho of higher degree ( brooker iii , iv ) reduces the function of hip arthroplasty . 
 key words : hip arthroplasty prophylactic radiotherapy heterotopic ossification hip function strahlenther onkol 2005 ; 181 : 52933 doi 10.1007 / s00066 - 005 - 1352 - 4 der einfluss heterotoper ossifikationen nach totalendoprothese des hftgelenks auf die gelenkbeweglichkeit ziel : der einfluss heterotoper ossifikationen ( ho ) nach totalendoprothese des hftgelenks ( tep ) auf die gelenkbeweglichkeit wird untersucht . 
die erhobenen rom unterschieden sich signifikant bei den patienten , die keine oder niedriggradige ho ( brooker i , ii ) entwickelt hatten , und denen , die hhergradige ho ( brooker iii , iv ) aufwiesen . 
die patienten mit ho brooker 0 , i und ii zeigten im gegensatz zu den patienten mit ho brooker iii und iv postoperativ eine signifikante verbesserung der werte fr flexion , innenund auenrotation , abund adduktion . 
daher muss eine prophylaktische therapie insbesondere darauf abzielen , die inzidenz hhergradiger ho zu reduzieren . schlsselwrter : hftendoprothese prophylaktische bestrahlung heterotope ossifikation hftgelenkbeweglichkeit 1 department of radiotherapy , university of wuerzburg , germany , 2 orthopedic clinic , caritas krankenhaus bad mergentheim , germany , 3 institute for radiology , caritas krankenhaus bad mergentheim , germany . 
factors associated with the development of ho after tha include previous ho , sex and age , idiopathic skeletal hyperostosis , ankylosing spondylitis , and hypertrophic osteoarthritis [ 1 , 2 , 6 , 8 , 18 , 37 ]  . 
in the last 3 decades both , prophylactic radiotherapy and the prophylactic use of nonsteroidal anti - inflammatory drugs ( nsaids ) were shown to be effective for prevention of ho by numerous prospective and retrospective studies [ 16 , 2123 , 29 , 3234 ]  . 
a systematic analysis of the functional failure defined as the range of motion ( rom ) of the hip joint is rare in literature . therefore , the purpose of this study was to assess the physical function of the hip joint following tha and prophylactic preoperative radiotherapy and to correlate the physical results with those of radiography . 
 the central pivot of the goniometer was placed over the greater trochanter , the stationary arm of the goniometer was aligned with the body and the medioaxillary line taken as 0 , and the moving arm of the goniometer was placed parallel to the longitudinal axis of the femur on the lateral surface of the thigh , pointing toward the lateral condyle . 
the stationary arm of the goniometer was placed perpendicular to a reference line anteriorly between the iliac crest , the central pivot was placed over the anterior superior iliac spine , and the movtable 2 . 
 definite osteophytes beginning joint space narrowing presence of two of the following : joint space narrowing , osteophytosis , subchondral sclerosis , cyst formation presence of three of the following : joint space narrowing , osteophytosis , subchondral sclerosis , cyst formation table 3 . 
analysis of radiographs was performed by a panel of four experts ( two radiotherapists , one orthopedist , one radiologist ) according the brooker score ( table 3 ) [ 5 ]  . 
in the starting position , the center of the goniometer was placed over the tuberosity of the tibia , and both arms of the goniometer were placed vertically parallel to the longitudinal axis of the tibia on its anterior surface . 
then , the moving arm was moved to overlie the anterior surface of the tibia after it had been swung laterally or medially , whereas the stationary arm remained in the starting position before hip rotation . 
 discussion radiotherapy plays an important role in the treatment of benign diseases , especially in the prevention of ho [ 4 , 14 , 26 , 30 , 35 , 36 ]  . 
in the past , clinical studies showed that the incidence of ho following hip arthroplasty was reduced by either prophylactic radiotherapy or the use of nsaids [ 17 , 19 , 20 , 27 , 31 ]  . 
influence of heterotopic ossification on hip function on radiologic signs and does not consider whether ho influences the clinical function of the hip or not . in our study all patients were irradiated preoperatively with a 7 - gy single - dose fraction . 
the reported overall incidence and the results published in other studies using preoperative radiotherapy for prevention of ho are higher than those of studies using postoperative radiotherapy [ 11 , 22 , 23 , 32 , 33 ]  . 
showed that only 4% of the participating departments of radiotherapy were able to specify the functional results following tha and prophylactic irradiation for prevention of ho [ 33 ]  . 
even though several authors suggest that only ho of higher degree ( brooker iii , iv ) results in a reduced postoperative functional outcome , an analysis of hip function and a correlation between the extent of ho and the functional situation of the hip is rare in literature [ 10 , 25 , 28 ]  . 
 brooker himself originally concluded that ho grade i , ii and iii did not significantly alter the functional results after tha and that only ho grade iv was significant [ 5 ]  . 
reported that ho brooker i and ii did not deteriorate the harris hip score , whereas patients with ho brooker iii and iv had a lower harris score following tha [ 31 , 33 ]  . 
the harris hip score is a grading system to assess both , the functional status of the hip joint and the quality of life basing on information about pain , functional capacity , deformity , and rom [ 12 ]  . 
several studies demonstrated that the harris score for brooker grades 0ii did not differ significantly from that for grades iii and iv [ 3 , 9 , 17 ]  . 
reported no correlation between harris score and the extent of ho in patients with revision of arthroplasty , they found a negative correlation between broker grades and range of flexion , an important finding , because range of flexion is the most important motion for walking [ 9 ]  . 
in our study of 345 hips with severe coxarthrosis , we demonstrated that the rom of the hip , especially the range of flexion , was not reduced in patients with ho grade i and ii compared to those without ho . 
from this point of view the increased incidence of ho of lower degree ( brooker i and ii ) after preoperative compared to postoperative prophylactic radiotherapy seems to be of no importance for the clinical outcome following tha . 
hence , for comparison of the results of previous radiologic studies the incidence of ho of higher degree ( brooker iii and iv ) should be given more consideration than the overall incidence . 
to be able to compare the clinical results , a standardized system , e.g. , the harris hip score , which considers subjective and objective functional hip parameters , should be used to classify hip function . 
 strahlentherapie und onkologie originalarbeit quantitative und qualitative speicheldrsenfunktionsuntersuchungen in abhngigkeit von dosis und volumen einer radiotherapie zur verringerung der xerostomie bei kopf - hals - tumoren thomas kuhnt1 , nicole jirsak2 , arndt christian mller1 , tanja pelz1 , christian gernhardt2 , hans - gnter schaller2 , martin janich1 , reinhard gerlach1 , jrgen dunst1 hintergrund und ziel : die strahlentherapie bei kopf - hals - tumoren fhrt in aller regel zu einer schdigung der speicheldrsen und somit auch zu einer dauerhaften mundtrockenheit . 
ziel dieser untersuchung war es , eine moderne dreidimensionale konformationsbestrahlungstechnik ( three - dimensional conformal radiotherapy [ 3d - crt ] ) fr kopf - hals - tumoren zu etablieren , um im vergleich zur konventionellen bestrahlungstechnik ( k - rt ) mit photonen und elektronen xerostomien zu vermeiden . patienten und methodik : zwischen april 2002 und september 2003 wurden in einer prospektiven , nicht randomisierten studie 32 patienten ( 25 mnner , sieben frauen , mittleres alter : 58 jahre ) mit malignen tumoren im kopf - hals - bereich nach operation oder bei inoperabilitt mit einer kurativen radiotherapie bzw . 
10 / 32 patienten ( 31% ) erhielten die bliche k - rt , die brigen 22 / 32 patienten ( 69% ) wurden mittels 3d - crt ( sechs bis acht photonenstehfelder ) behandelt . 
als ma fr die strahlenbelastung der parotiden wurde die mediane parotisdosis in gray ( dmean - wert ) als mittelwert der dmean - dosen beider parotiden aus den dosis - volumen - histogrammen ( dvh ) anhand der ct - schnitte bei der dreidimensionalen planung bestimmt . 
die mit k - rt behandelten patienten hatten im mittel signifikant hhere gemittelte dmean - werte als die mit 3d - crt bestrahlten patienten ( p < 0 , 012 )  . 
patienten , die mit 3d - crt wegen eines larynx - / hypopharynxkarzinoms behandelt wurden , hatten im mittel signifikant niedrigere dmean - werte als patienten , die wegen eines mundhhlen - / oropharynxkarzinoms mit 3d - crt oder gleich welchen tumorsitzes mit k - rt bestrahlt wurden ( p < 0 , 003 )  . 
die nach nlsf - methode berechnete 50% - komplikationsrate der speicheldrsen ( td50 ) lag bei 36 , 9 gy ( 30 , 943 , 5 gy ; 95% - vorhersageintervall )  . 
der anstieg k im punkt td50 wurde mit 7 , 7 ( 4 , 815 , 8 ; 95% - vorhersageintervall ) bestimmt . schlussfolgerung : die 3d - crt eignet sich als standard grundstzlich fr patienten mit karzinomen im mundhhlen - , oround hypopharynxbereich . 
vor allem bei patienten mit larynxund hypopharynxkarzinomen knnen mittlere dmean - werte ( ipsilaterale plus kontralaterale glandula parotidea ) erreicht werden , die nachweislich den speichelfluss erhalten . schlsselwrter : strahlentherapie kopf - hals - tumoren xerostomie sptfolgen strahlenther onkol 2005 ; 181 : 5208 doi 10.1007 / s00066 - 005 - 1366 - y quantitative and qualitative investigations of salivary gland function in dependence on irradiation dose and volume for reduction of xerostomia in patients with head - and - neck cancer background and purpose : radiation treatment of head - and - neck tumors mostly leads to a damage to the salivary glands and a consequential permanent loss of saliva . 
10 / 32 patients ( 31% ) received k - rt with photons and electrons , and 22 / 32 patients ( 69% ) 3d - crt ( six to eight photon portals )  . 
the quantity of saliva was measured as stimulated saliva flow rate ( ml / 5 min ) prior to treatment , at the end , and 1 , 6 , and 12 months after termination of treatment . 
to find out the resulting mean dose of both parotid glands for every patient in gray ( dmean doses ) , the dmean doses of the ipsilateral and the contralateral parotid gland , determined by dose - volume histograms ( dvhs ) , were averaged over . 
patients , who were irradiated with 3d - crt for tumors of the larynx or hypopharynx , showed , on average , significantly lower dmean values than patients , who were treated with 3d - drt because of oral cavity or oropharynx carcinomas or with k - rt irrespective of the primary tumor site ( p < 0 , 003 )  . 
especially in patients with tumors located in the larynx and hypopharynx , averaged dmean doses of both parotids during irradiation can be reached , to conserve salivary flow rates , which are similar to baseline flow rates . 
 key words : irradiation head - and - neck tumors xerostomia chronic side effects einleitung die strahlentherapie ist neben der operation die wichtigste option in der behandlung von kopf - hals - tumoren . 
 die rate an zahnextraktionen und infektionen der zhne mit schwerwiegenden folgen ( infizierte osteoradionekrose ) kann durch senkung der radiogenen karies zweifelsfrei verringert werden [ 13 , 14 , 18 , 36 ]  . ein derzeit wichtiges forschungsgebiet der radioonkologie ist die vermeidung oder verringerung der xerostomie durch schonung der speicheldrsen whrend der radiotherapie von kopf - hals - tumoren . 
die hauptbemhungen zur speicheldrsenschonung konzentrieren sich auf die glandula parotidea , die ( von ausnahmen abgesehen ) nicht teil des zielvolumens ist und aufgrund ihrer anatomischen lagebeziehungen zu den lymphknotenstationen meist an dessen rand liegt . 
 ziel unserer untersuchung war es deshalb , eine dreidimensionale konformationsbestrahlung ( three - dimensional conformal radiotherapy [ 3d - crt ] ) bei kopf - hals - tumoren gegenber der lteren konventionellen bestrahlungstechnik ( k - rt ) so zu optimieren , dass durch schonung der parotiden bei einem groen teil der patienten xerostomien vermieden werden knnen . 
 patienten und methodik patienten die studien zur quantitt und qualitt des speichels wurden in zusammenarbeit mit der universittsklinik fr parodontologie und zahnerhaltungskunde der martin - luther - universitt halle - wittenberg prospektiv unter der fragestellung begonnen , die bis dato relevanten parameter der speicheltestung an unseren patienten zu untersuchen . 
im zeitraum von april 2002 bis september 2003 wurden in dieser studie 32 patienten ( 25 mnner , sieben frauen , mittleres alter : 58 jahre ) mit malignen tumoren im kopf - hals - bereich behandelt . 
danach erhielten 17 / 32 patienten ( 53% ) eine adjuvante radiotherapie , 11 / 32 patienten ( 34% ) eine adjuvante radiochemotherapie ( im rahmen der aro - studie 95 - 3 ) , 1 / 32 patienten ( 3% ) eine alleinige definitive radiotherapie und 3 / 32 patienten ( 10% ) wegen primrer inoperabilitt eine definitive radiochemotherapie . 
 k - rt ( n = 10 ) 3d - crt ( n = 22 ) radiotherapietechniken alter ( jahre ) spanne median geschlecht frauen mnner primrtumorsitz mundhhle oropharynx larynx hypopharynx speicheldrse cup 4174 59 , 7 2 8 3 5 2 0 0 0 4468 55 , 5 k - rt . 
10 / 32 patienten ( 31% ) erhielten die konventionelle therapie , die zunchst ber zwei seitlich opponierende photonenstehfelder unter einschluss der primrtumorregion und der beidseitigen zervikalen lymphabstromgebiete ohne schonung der rckenmarkes ( offen ) bis zu einer dosis von 36 gy erfolgte . 
im anschluss wurden das rckenmark aus den photonenfeldern ausgeblendet und die dorsalen halsabschnitte mit angesetzten elektronenfeldern individuell , je nach lymphknotenbefall , bis 50 , 60 oder 64 gy aufgesttigt . 
die primrtumorregion wurde dann , je nach tumorsitz , weiter mit zwei seitlichen oder zwei bis drei gewinkelten photonenfeldern bis zur verordneten gesamtdosis von 64 oder 70 gy bestrahlt ( zielvolumen und dosisverteilung der 95% - isodose in gy in abbildung 1 )  . 
 bestimmung der speichelflierate ( quantitativ ) bei allen patienten erfolgten untersuchungen der speichelflieraten vor beginn der bestrahlung , nach 3 und 6 wochen whrend der behandlung sowie 10 , 26 und 52 wostrahlenther onkol 2005 no . 
 statistik nach untersuchung der ersten zehn patienten wurde die alte technik , die im wesentlichen auf den prinzipien der zweidimensionalen technik beruhte , verlassen und die 3d - crt , da im theoretischen planungsbeispiel hinsichtlich der parotisschonung berlegen , eingefhrt . 
unterschiede zwischen den kollektiven wurden mittels statistischer testverfahren auf signifikanz gepr ergebnisse speichelflieraten die mittlere prtherapeutische speichelflierate aller patienten lag mit 3 , 8 2 , 2 ml / 5 min etwas unter dem wert fr normale probanden ( 5 ml / 5 min ) [ 8 ]  . 
die bestimmung der parameter erfolgte durch die nichtlineare approximation der beobachteten schadenshufigkeit in abhngigkeit von den gemittelten dmean - werten beider parotiden nach der methode der kleinsten abweichungsquadrate ( nlsf )  . 
fr alle patienten wurde die mittlere parotisdosis ( dmean - wert ) aus den dosis - volumen - histogrammen ( dvh ) beider parotiden ermittelt , die die mittlere dosis der organe bei inhomogener dosisverteilung kennzeichnet . 
im trend war der speichelfluss in der gruppe mit 3d - crt zum ende der bestrahlung ( 6 - wochen - wert ) und 4 wochen nach der strahlenbehandlung ( 10 - wochen - wert ) etwas hher ( 10 - wochen - wert , p < 0 , 1 ) als in der k - rt - gruppe ( abbildung 3 )  . 
 volumeneffekte die therapierten volumina lagen im ptv im mittel bei 1 133 391 cm3 ( spanne : 2911 872 cm3 ) und im boost im mittel bei 413 209 cm3 ( spanne : 134925 cm3 )  . 
 die patienten , die mit 3d - crt wegen eines larynx - / hypopharynxkarzinoms behandelt wurden , wiesen im mittel signifikant niedrigere dmean - werte auf als die patienten , die wegen eines mundhhlen - / oropharynxkarzinoms mit 3d - crt oder gleich welchen tumorsitzes mit k - rt bestrahlt wurden ( p < 0 , 003 ; abbildung 4 )  . 
 mit zunehmenden dmean - werten beider parotiden fllt die speichelflierate ab ( regressionskoeffizient r = 0 , 61 , ratiowert f = 1 , 71 gemittelter dmean - wert + 102 , 8 )  . 
besonders patienten , die mit der neuen 3d - crt wegen eines larynx - / hypopharynxkarzinoms behandelt wurden , wiesen eine hohe ratio von postzu prtherapeutischem speichelfluss auf ( abbildung 5 )  . 
 in den verschiedenen dosisintervallen wurden zunehmend schden ( nach who - klassifikation verminderung der speichelflierate auf 25% des ausgangswerts ) der glandulae parotideae mit anstieg des gemittelten dmeanwerts beider parotiden beobachtet . 
 die td50 nach nlsf - schtzung lag bei unseren patienten bei 36 , 9 gy ( 30 , 943 , 5 gy , 95% - vorhersageintervall ; abbildung 6 )  . 
in den letzten jahren hat in der operativen behandlung von kopf - hals - tumoren ein sehr differenziertes konzept zur behandlung der regionren lymphknoten an bedeutung gewonnen [ 31 ]  . 
dieses lsst sich auch auf die bestrahlung der regionren lymphknoten bertragen und wird deshalb in der radioonkologischen literatur ebenfalls zunehmend propagiert und in studien umgesetzt [ 2 , 16 ]  . 
 die kleinen speicheldrsen in der mundund pharynxschleimhaut lassen sich vor allem bei der bestrahlung von 3d - crt larynx / hypopharynx 3d - crt mundhhle / oropharynx k - rt larynx / hypopharynx k - rt mundhhle / oropharynx gemittelter d mean - wert parotiden ( gy ) abbildung 5 . 
die waagrechte linie markiert die schadensgrenze 25% vom ausgangswert ; die gestrichelte linie stellt die regressionsgerade mit dem regressionskoeffizienten r = 0 , 61 , f = 1 , 71 gemittelter dmean - wert + 102 , 8 dar . 
the horizontal line characterizes the complication probability at 25% of the pretreatment levels ; the broken line showes the regression line with the regression coefficient r = 0.61 , f = 1.71 averaged dmean value + 102.8. 
in den verschiedenen dosisintervallen beobachtete schden ( verminderung der speichelflierate auf 25% des ausgangswerts ) an den glandulae parotideae unter angabe der gemittelten der dmean - werte beider parotiden nach der methode der kleinsten abweichungsquadrate ( nlsf )  . 
observed complications of the parotid glands ( reduction of the salivatory flow rate to 25% of the pretreatment level ) in the different dose intervals under specification of the averaged dmean values of both parotid glands according to the method of the smallest discrepancy squares ( nlsf )  . 
 dosisintervall ( gy ) anzahl der patienten gemittelter dmean - wert beider mit schaden ( i ) / parotiden ( gy ) gesamter patientenzahl ( n ) im dosisintervall ( i / n ) 010 1020 2030 3040 4050 5060 6070 16 , 7 27 , 5 33 , 6 43 , 4 53 , 9 61 , 9 strahlenther onkol 2005 no . 
die hauptbemhungen zur speicheldrsenschonung konzentrieren sich deshalb auf die glandula parotidea , die , von ausnahmen abgesehen , nicht teil des zielvolumens ist und aufgrund ihrer anatomischen lagebeziehungen zu den lymphknotenstationen meist an dessen rand liegt . 
ziel unserer untersuchung war es , eine 3d - crt bei kopf - halstumoren gegenber der lteren bestrahlungstechnik so zu optimieren , dass durch die reduktion der dosisbelastung an den parotiden xerostomien vermieden werden knnen . 
 als methoden zur quantifizierung der speicheldrsenfunktion werden in der literatur die speicheldrsenszintigraphie und / oder klinische methoden wie messung von ruheund reizspeichelmenge eingesetzt [ 10 , 12 , 27 , 29 ]  . 
aus der literatur ist bekannt , dass nach entfernung der glandula submandibularis bei einer modifiziert radikalen neck - dissection schon eine deutliche verringerung der speichelflierate resultieren kann [ 25 ]  . 
im trend war die speichelflierate der patienten , die mit der 3d - crt behandelt wurden , ber den gesamten beobachtungszeitraum hher als bei patienten , die mit der k - rt therapiert wurden . 
patienten der 3d - crt - gruppe mit tumorsitz im hypopharynx / larynx wiesen signifikant niedrigere gemittelte dmean - werte beider parotiden auf als patienten der k - rt - gruppe mit diesem tumorsitz . 
die niedrigeren gemittelten dmean - werte beider parotiden mit 3d - crt und hypopharynx / larynxkarzinomen gegenber patienten mit mundhhlen - / oropharynxkarzinomen resultieren aus der tatsache , dass das boostvolumen sich anatomisch unterhalb der region der ohrspeicheldrsen befindet und somit nur ein geringer teil der boostdosis zur gesamten parotisdosis beitrgt . 
nach radfar & sirois [ 30 ] werden als typische radiogene sptvernderungen die fibrosierung der drse , die atrophie der azini , ausfhrungsgangsvernderungen mit gangproliferationen , gangerweiterungen und verlust an parenchym gesehen . 
somit wird prinzipiell ein fibrotischer umbau der drse zu erwarten seerste klinische daten zeigen , dass nur durch die reduktion der medianen dosis auf < 30 gy an der glandula parotidea auch eine relevante verringerung der xerostomie erreicht werden kann [ 27 ]  . 
in unserer untersuchung zeigten alle patienten , die eine gemittelte dmean - dosis der parotiden < 30 gy aufwiesen , keinen funktionellen schaden nach who - klassifikation , was die klinischen daten von mnter et al . 
unsere nach nlsf - methode berechnete td50 lag bei 36 , 9 gy ( 30 , 943 , 5 gy , 95% - vorhersageintervall ) und war somit ebenfalls den werten der literatur vergleichbar [ 27 , 32 ]  . 
dies korrelierte auch mit der verminderung der speichelflierate auf 25% ihres ausgangswerts , so dass zum zeitpunkt 4 wochen nach strahlentherapie diese patienten offensichtlich nicht von der 3d - crt profitierten . 
unsere ergebnisse zeigen jedoch auch , dass die methode der schadensermittlung mittels stimulierter speichelmessung durchaus geeignet ist , um dosis - wirkungs - beziehungen der wirkungswahrscheinlichkeit an den glandulae aufzustellen . 
vor allem bei patienten mit larynxund hypopharynxkarzinomen knnen gemittelte dmean - werte beider parotiden erreicht werden , die nachweislich quantitativ und auch qualitativ den speichel und speichelfluss so erhalten , dass die patienten in ihrer lebensqualitt nur wenig beeintrchtigt werden . 
des weiteren wird es notwendig sein , moderne zielvolumenkonzepte zu entwickeln , um dann selektiv nach risikoprofil lymphknotenlevel zu bestrahlen oder auszusparen und so die schonung zumindest einer drse zu erreichen . 
grtz ka ; gemeinsame stellungnahme der deutschen gesellschaft fr zahn - , mundund kieferheilkunde ; deutschen gesellschaft fr radioonkologie , medicinische physik und strahlenbiologie ; abstimmung mit dem vorstand der deutschen gesellschaft fr zahnerhaltungskunde . 
8 urban & vogel strahlentherapie und onkologie original article optimizing cancer radiotherapy with 2 - deoxyd - glucose dose escalation studies in patients with glioblastoma multiforme dinesh singh1 , ajit k . 
lazar mathew3 , turuga ravindranath3 , viney jain4 background and purpose : higher rates of glucose utilization and glycolysis generally correlate with poor prognosis in several types of malignant tumors . 
own earlier studies on model systems demonstrated that the nonmetabolizable glucose analog 2 - deoxy - d - glucose ( 2 - dg ) could enhance the efficacy of radiotherapy in a dose - dependent manner by selectively sensitizing cancer cells while protecting normal cells . 
phase i / ii clinical trials indicated that the combination of 2 - dg , at an oral dose of 200 mg / kg body weight ( bw ) , with large fractions of - radiation was well tolerated in cerebral glioma patients . 
since higher 2 - dg doses are expected to improve the therapeutic gain , present studies were undertaken to examine the tolerance and safety of escalating 2 - dg dose during combined treatment ( 2 - dg + radiotherapy ) in glioblastoma multiforme patients . 
seven weekly fractions of 60co - rays ( 5 gy / fraction ) were delivered to the tumor volume ( presurgical ct / mri evaluation ) plus 3 cm margescalating 2 - dg doses ( 200250300 mg / kg bw ) were administered orally 30 min before irradiation after overnight fasting . 
however , at the higher dose of 300 mg / kg bw , two out of six patients were very restless and could not complete treatment , though significant changes in the vital parameters were not observed even at this dose . 
no significant damage to the normal brain tissue was observed during follow - up in seven out of ten patients who received complete treatment and survived between 11 and 46 months after treatment . 
 conclusion : oral administration of 2 - dg combined with large fractions of radiation ( 5 gy / fraction / week ) is safe and could be tolerated in glioblastoma patients without any acute toxicity and late radiation damage to the normal brafurther clinical studies to evaluate the efficacy of the combined treatment are warranted . 
 key words : 2 - deoxy - d - glucose glioblastoma multiforme radiotherapy dose escalation safety and tolerance strahlenther onkol 2005 ; 181 : 50714 doi 10.1007 / s00066 - 005 - 1320 - z optimierte krebsbestrahlung mit 2 - deoxy - d - glukose . 
eigene untersuchungen an modellsystemen zeigten , dass die nichtmetabolisierbare glukoseverbindung 2 - deoxy - d - glukose ( 2 - dg ) die wirksamkeit der strahlentherapie dosisabhngig verstrken kann , indem sie selektiv krebszellen sensibilisiert , dagegen auf normale zellen protektiv wirkt . 
klinische phase - i / ii - studien sprechen dafr , dass die kombination von 2 - dg ( in einer oralen dosis von 200 mg / kg krpergewicht ) mit groen fraktionen einer - strahlung von patienten mit hirntumoren gut vertragen wird . 
da man erwartet , dass hhere 2 - dg - dosierungen das therapeutische ansprechen verbessern , wurden die hier vorgestellten untersuchungen unternommen , um an glioblastoma - multiforme - patienten vertrglichkeit und sicherheit der dosiseskalation von 2 - dg in der kombinationsbehandlung ( 2 - dg + radiotherapie ) zu prfen . 
das tumorvolumen ( gem properativer ct / mrt - auswertung ) plus ein 3 - cm - sicherheitssaum wurden wchentlich mit sieben fraktionen einer 60co - - strahlung ( 5 gy / fraktion ) behandelt . 
in ansteigender dosierung 1 dharmshila cancer hospital , new delhi , india , 2 vidyasagar institute of mental health and neurosciences , new delhi , india , 3 institute of nuclear medicine and allied sciences , delhi , india , 4 department of emergency medicine and department of nuclear medicine , kettering medical center , wright state university , dayton , oh , usa . received : may 25 , 2004 ; accepted : may 13 , 2005 strahlenther onkol 2005 no . 
vertrglichkeit und patienten - compliance der kombinationsbehandlung waren bis zu einer 2 - dg - dosis von 250 mg / kg kg sehr gut ; bei der hheren dosis von 300 mg / kg kg entwickelten zwei von sechs patienten jedoch starke unruhe und konnten die behandlung nicht abschlieen , obwohl auch unter dieser dosis keine signifikanten vernderungen der vitalparameter festgestellt wurden . 
im follow - up war keine signifikante schdigung des normalen hirngewebes bei sieben von zehn patienten zu beobachten , die die komplette behandlung erhalten und zwischen 11 und 46 monate nach der behandlung berlebt hatten . 
 schlussfolgerung : die orale gabe von 2 - dg kombiniert mit hohen einzelfraktionen ( 5 gy / fraktion / woche ) ist sicher und wurde von gliom - patienten ohne akuttoxizitt und ohne strahlungssptschden im hirngewebe vertragen . 
um die wirksamkeit der kombinationstherapie zu prfen , sind weitere klinische studien erforderlich . schlsselwrter : 2 - deoxy - d - glukose glioblastoma multiforme strahlentherapie dosiseskalation sicherheit und vertrglichkeit introduction poorly differentiated and rapidly growing malignant tumors are generally characterized by higher rates of glucose usage and glycolysis as compared to corresponding normal tissues [ 1 , 54 , 55 ]  . 
a higher glucose flux in transformed cells may be mediated by increased activities of glucose transporters [ 3 , 59 ] and glycolytic enzymes [ 45 , 53 , 55 ] induced by growth factors [ 16 , 39 ] that are often overexpressed in malignant tumors . these fundamental differences in the glucose metabolism of transformed and normal cells form the basis of noninvasive detection and grading of tumors by positron emission tomography ( pet ) using [ 18 - f ] - 2 - fluoro - deoxyglucose ( fdg ) , a nonmetabolizable analog of glucose . 
measurements of glucose uptake in human tumors by fdg - pet suggest that glucose uptake may directly correlate with the degree of malignancy and treatment resistance / poor prognosis [ 5 , 42 ]  . 
irrespective of the mechanisms involved , a strong correlation between glucose uptake , glycolysis , hypoxia and treatment resistance in tumors has important implications in the management of cancer patients . 
several approaches to differentially modulate glucose flux and energy supply in cancer cells and to develop hypoxic cell sensitizers are , therefore , being investigated to improve tumor therapy . the glucose antimetabolite , 2 - deoxy - d - glucose ( 2 - dg ) , a competitive inhibitor of glucose transport and glucose phosphorylation by hexokinase , is known to inhibit glycolytic energy ( adenosine triphosphate [ atp ] ) production [ 7 , 9 , 38 , 57 ]  . 
initial attempts in the late 1950s to treat cancer patients with 2 - dg as an anticancer agent proved unsuccessful and were abandoned [ 32 ] , since continuous administration of 2 - dg for long time could be toxic . 
in pharmacological doses , 2 - dg is known to produce symptoms of hypoglycemia due to reduction in the utilization of glucose also in normal tissues , especially in the brain , since brain tissues strongly depend on glucose for energy supply [ 17 , 33 ]  . we have studied the use of glucose analog to differentially modulate the energy - linked damage responses induced by genotoxic agents including ionizing radiation to improve cancer therapy . 
it was subsequently shown that 2 - dg could inhibit repair of dna lesions and potentially lethal damage differentially in cells with high rates of glycolysis , e.g. , in respiratory - deficient mutants of yeast [ 13 , 19 , 22 ]  . 
 most importantly , these studies have strongly indicated that modifications of radiation responses by 2 - dg depend on the cell type , pattern of energy metabolism ( especially the rates of glucose usage and glycolysis ) , and the ratio of molar concentrations of 2 - dg to glucose . 
for example , at high 2 - dg concentrations ( 2 - dg / glucose 1 ) , radiosensitization in hela and malignant glioma cells was observed [ 7 , 8 , 12 , 21 ] , the radiosensitization being significantly higher in the absence of respiratory metabolism [ 6 , 7 , 25 ]  . 
on the other hand , in normal cells such as human peripheral blood leukocytes , a reduction in radiation - induced cytogenetic damage [ 20 , 26 ] has been observed under similar conditions . experiments with in vivo animal models have confirmed the results on cell cultures described above . 
for example , in murine tumors ( ehrlich ascites and sarcoma 180 ) increased tumor cell loss , tumor regression and enhanced animal survival have been reported when 2 - dg 1g / kg body weight ( bw ) was administered just before or immediately after irradiation [ 11 , 23 , 34 , 43 ]  . 
2 - dg escalation in glioblastoma multiforme patients the precise molecular mechanisms underlying the differential effects induced by 2 - dg in tumors and normal tissues remain , however , yet to be completely understood . 
nevertheless , the ability of 2 - dg to differentially radiosensitize tumors and at the same time protect normal tissues against radiotoxicity makes it a strong candidate as an adjuvant for improving therapy of radioresistant tumors . 
we have , therefore , undertaken clinical trials on malignant glioma patients to evaluate the feasibility and efficacy of combining 2 - dg with radiotherapy . the prognosis of patients suffering from malignant cerebral gliomas has remained dismal despite many advances in surgery , radiation therapy and chemotherapy [ 15 , 30 , 31 , 41 ]  . 
 during the last several decades a large number of clinical trials have been undertaken [ 2 , 36 ] , however , the median survival of glioblastoma patients treated with multimodality therapy has remained unchanged at < 12 months with a 2 - year survival of < 10% and a 5 - year survival of around 2% [ 36 , 50 ]  . 
the failure of radiotherapy in cerebral gliomas is primarily due to the diffusely infiltrating nature of the tumor and the presence of hypoxic , repair - proficient and intrinsically radioresistant subpopulation of cells [ 29 , 49 , 58 ]  . 
an analysis of the pattern of responses to conventional therapy comprising surgery , radiotherapy , and chemotherapy shows that local regrowth of the tumor is mainly responsible for the failure indicating that the conventional treatment ( 1.82.0 gy / fraction ; 3035 fractions ; five fractions / week ; total absorbed dose 6070 gy ) is inadequate in local control of the tumor [ 1 ]  . 
on the other hand , delivery of high radiation doses is limited due to damage to surrounding normal brain tissue [ 44 ]  . strategies directed toward differentially enhancing radiation damage in tumor cells and reducing the damage to normal tissues could significantly improve the treatment efficacy of radiotherapy leading to better local control . 
enhanced glucose usage in vitro [ 53 ] as well an in vivo , correlating with the degree of malignancy and poor prognosis , has been demonstrated in glioma tumors [ 5 , 42 ]  . 
in vitro studies in established glioma cell lines showed that the presence of 2 - dg for a few hours after irradiation could increase radiation damage significantly and the radiosensitization was higher under conditions of reduced respiratory metabolism [ 6 , 9 , 12 ]  . 
human patients with malignant cerebral gliomas , were , therefore , selected to evaluate the possibility of improving the efficacy of the combined therapy ( radiotherapy + 2 - dg )  . 
initial phase i / ii clinical trials in malignant glioma patients [ 40 ] were designed to combine 2 - dg with relatively large radiation doses in order to minimize the frequency and potential toxicity of 2 - dg administration . 
the therapy protocol consisted of 4 5 gy / fraction / week delivered to the whole brain 30 min after oral administration of 2 - dg ( 200 mg / kg bw ) , followed 2 weeks later by supplemental focal irradiation ( 7 2 gy ) to the tumor site . 
investigations in 20 patients yielded encouraging results showing that the combination of large doses of radiation ( 5 gy / fraction / week ) with 2 - dg administered orally 30 min before irradiation was well tolerated , without any serious acute toxicity and late radiation damage to the brain . while in vitro and in vivo studies have clearly shown a concentration / dose - dependent radiosensitization by 2 - dg [ 810 , 12 , 21 ] , transient disturbances induced by 2 - dg combined with relatively high radiation dose fractions are an important concern for the patients safety . 
therefore , the present studies were undertaken to determine the tolerance and safety of administering the combined treatment ( 2 - dg + radiotherapy ) with escalating doses of 2 - dg > 200 mg / kg bw in glioblastoma multiforme patients . 
preliminary results of these studies have been presented [ 46 ]  . patients and methods eligible patients previously untreated patients with histologically proven glioblastoma multiforme ( according to who criteria ) were included in the study . 
additional criteria for selection were : ( 1 ) morphologically well - defined tumor mass on ct / mri ; ( 2 ) age < 75 years ; ( 3 ) karnofsky performance status of at least 70% ; ( 4 ) no associated diabetes mellitus , hepatic , renal , psychiatric or cardiac disorders ; and ( 5 ) informed consent from the patient and family members . authorization the present studies were conducted after obtaining clearance from the ethics committees of dharmshila cancer hospital and vidyasagar institute of mental health and neurosciences , new delhi , india . 
approval for the administration of 2 - dg in the prescribed doses was also obtained from the drug controller general of india , and indian council of medical research . study design the study design used for the dose escalation of 2 - dg in combination with 5 - gy weekly fractions was essentially according to storer [ 48 ]  . 
escalation to the next dose level occurred when no toxicity was observed in all three patients ; otherwise , an additional three patients were treated at the same dose level . 
histological evaluation of the tumor was carried out according to the who criteria [ 60 ] , and patients with histologically confirmed glioblastoma multiforme were recruited strahlenther onkol 2005 no . 
all patients were administered dexamethasone ( 8 mg ) postoperatively for 12 weeks which was stopped before starting radiotherapy . administration of 2 - dg after overnight fasting , blood glucose levels were determined . 
 if the blood glucose was > 60 mg / ml , 2 - dg ( sigma , usa ) dissolved in 100 ml water was administered orally , 30 min before irradiation . radiotherapy a cobalt - 60 ( 60co ) - teletherapy unit ( phenix , theratron ) was used for irradiation . 
seven weekly fractions of 60co - rays ( 5 gy ) were delivered to the treatment volume , which included the preoperative tumor volume ( ct / mri evaluation ) plus a 3 cm margthe bed was 2 gy compared to the conventional protocol of five fractions / week at 2 gy per fraction with / - values of 3 for normal brain and 10 for the tumor . 
 irradiation was carried out according to the ct plan over multiple and also non - coplanar fields , using the computerized treatment planning system ( multidata , usa )  . 
no other medications except antiepileptic drugs ( whenever required ) were administered either during or after treatment . evaluation of safety and tolerance patients were closely monitored for changes in vital parameters like blood pressure , pulse rate and body temperature , besides other symptoms like vomiting , headache , drowsiness , sweating , thirst and giddiness for 24 h after treatment . 
if neurologic symptoms of category 3 or more ( according to the who scale ) appeared or when patients had excess vomiting and nausea , an additional 8 mg dexamethasone was administered in physiological saline ( with 20% glucose ) to maintain a blood glucose level of 200 mg / ml . 
 total leukocyte and platelet counts as well as hemoglobin levels were obtained weekly . estimation of toxicity and tumor response a cranial ct / mri was carried out 2845 days after completion of radiation therapy . 
during follow - up , patients were evaluated every 3 months during the first year and every 6 months thereafter with clinical assessment for disease - related symptoms and neurologic status , and radiologically with ct scan / mri . 
the effects of combined treatment on the normal brain and the tumor were assessed according to the who criteria , and the degree of toxicity was analyzed according to lent - soma criteria [ 35 ]  . 
 orally administered 2 - dg at doses of 200250300 mg / kg bw did not induce life - threatening changes in any of the vital parameters including peripheral pulse rate , blood pressure , body temperature , either on the day of treatment or on subsequent days in all seven fractions . 
a marginal fall in body temperature in the range of 0.21.2 c indicating hypothermia was noted in some patients in the first hour following 2 - dg administration , which reversed completely by 23 h without any supportive medication . 
significant alterations in pulse rate requiring close ecg monitoring were also not encountered during any of the treatment fractions in these patients . in most of the patients , a transient increase in blood pressure was noted , which returned to the basal values by 23 h following administration of 2 - dg . 
the maximum and minimum values of blood pressure changes observed from the seven fractions are given in table 1 . general weakness and lethargy were observed in all patients on the day of administering the combined ( 2 - dg + irrradiation ) treatment . 
excess sweating , transient disorientation lasting for 2 h and fall in blood pressure were observed in the first fraction of one patient ( k.b.k ) at 200 mg / kg bw ( table 1 )  . 
none of the three patients treated at a dose of 250 mg / kg bw had any discomfort or disturbances on the day of treatment or subsequent days in all the seven fractions . 
treatment was discontinued after two ( r.c.s. ) and three ( d.s. ) fractions in these patients , as they were not stable during irradiation due to restlessness , although no significant changes were observed in the vital parameters . in the next group of three patients ( at 300 mg / kg bw ) , one ( k.k. ) had severe thirst , giddiness and mild restlessness accompanied by nausea and excess vomiting , besides headache in first and two subsequent fractions , while no changes in the vital parameters could be noticed . 
patient profile , tumor site , safety and tolerance observed in gbm patients following the administration of the combined treatment ( 2 - deoxy - d - glucose [ 2 - dg ] + radiotherapy ) with escalating 2 - dg doses . 
patientencharakteristika , tumorlokalisation , sicherheit und vertrglichkeit der kombinationstherapie ( 2 - deoxy - d - glukose [ 2 - dg ] + strahlentherapie ) mit eskalation der 2 - dg - dosierung bei glioblastoma - multiforme - ( gbm - ) patienten . 
very restless in fraction 7 increase in bp to 200 / 90 mmhg in fraction 1 and 170 / 90 mmhg in fractions 27 in the first and the last ( seventh ) fraction , although all vital parameters were nearly normal . since two out of the six patients showed poor tolerance , escalation of the 2 - dg dose > 300 mg / kg bw was not continued , as per the design of the study . 
detailed analysis of the toxicity according to lent - soma tables [ 35 ] using various subjective and objective criteria including normal brain damage ( as observed by mri ) , general condition ( karnofsky performance status ) and patient survival ( time after diagnosis ) are given in table 2 . 
the data clearly shows that the toxicity levels ( evaluated with both subjective and objective criteria ) were rather low and did not show any significant increase with increasing 2 - dg doses . 
laminar necrosis and ipsilateral ventricular dilation were noticed in one patient at 200 mg / kg bw during 1 month and 8 months of follow - up ; significant damage was not observed in the other two patients at this dose . 
further , two of the three patients at 250 mg / kg bw did not show any late radiation damage during the follow - up period of 411 months , while one patient with occipital lobe lesion had indications of mild cortical atrophy in the parietal lobes . 
 two out of four patients ( # 2 and # 3 ) , who completed treatment at 300 mg / kg bw , are alive for > 31 months with improved quality of life ( karnofsky score > 85 ) compared to their status prior to therapy ( karnofsky score about 75 )  . 
one patient ( # 4 ) who died 22 months after treatment had a karnofsky score of 80 at the last follow - up time ( table 2 ) , which was 20 months . 
2 - dg escalation in glioblastoma multiforme patients discussion present studies indicate that oral administration of 2 - dg in the dose range of 200300 mg / kg bw in combination with high - dose radiation fractions is well tolerated by most glioblastoma multiforme patients , so that the treatment can be administered on an outpatient basis . 
at the highest dose of 2 - dg administered ( 300 mg / kg bw ) in the present study , two patients were very restless and unstable on the treatment couch , so that precise delivery of radiation to the target volume could not be carried out . 
such disturbances were not seen in the other four patients , permitting completion of radiation treatment without any difficulty , although transient alterations in blood pressure were noted in two of the patients . 
these self - limiting physiological perturbations arise due to metabolic stress caused by cellular glucopenia , particularly in the neuroendocrine systein the peripheral blood , hyperglycemia is observed due to the increased secretion of noradrenaline from the hypothalamus leading to the release of glucagon from the pancreas , mobilization of fatty acid , breakdown of liver glycogen and gluconeogenesis [ 33 ]  . 
dose - dependent increases ( twoto threefold ) in the blood glucose levels observable between 14 h after the administration of 2 - dg have been reported [ 28 , 40 ]  . 
 increase in blood glucose is a regulatory process , which compensates for the 2 - dg - induced decrease in bioavailability of glucose and may limit the acute side effects . 
 since brain is a classic example of late - responding tissue to radiation , one of the major concerns in the treatment with high dose per fraction is the late radiation damage to the normal brain tissue . 
total radiation dose , dose fraction and time interval between fractions are among the important factors , besides repair and repopulation kinetics of the cells that contribute to the treatment response of the tumor and development of necrosis and myelitis . 
in this study , the total dose was 35 gy in 7 5 gy / week fractions , which is biologically equivalent to a dose of 62 gy ( bed ) in the conventional fractionation ( / - values of 3 for normal brain and 10 for the tumor )  . 
however , the irradiated volume consisted of a well - defined tumor boundary ( obtained by x - ray ct ) plus a 3 cm margin and not the whole brapresent results are in agreement with previous observations showing no significant enhancement in acute toxicity with large radiation dose per fraction ( 36 gy ) administered over different periods of time [ 36 ]  . 
recent studies have indicated slight benefit in functional status and patient convenience with hypofractionation treatment schedules in comparison with the conventional radiotherapy regimens in glioblastoma multiforme patients with poor prognosis [ 14 , 18 , 37 ]  . 
 our present results suggest that the combination of large fractions of radiation dose with increasing doses of 2 - dg may not lead to any apparent increase in the late radiation damage to the brain , similar to our earlier observations at a 2 - dg dose of 200 mg / kg bw [ 40 ]  . 
mri of the brain carried out at 31 months in one of the patients at 200 mg / kg bw alive till 46 months ( # 3 , a.s.c. ) and at 28 months in a patient treated with a dose of 300 mg / kg bw ( # 5 , d.b.m. ) did not reveal any significant damage to the normal bra furthermore , present observations support the suggestion that administration of 2 - dg may reduce radiation damage to the normal brain partly due to the protection of glial cells of the cranium and endothelial cells of the vasculature . 
experimental studies in vitro and in vivo have indeed shown a reduction in the radiation damage to the normal cells like bone marrow , peripheral blood leukocytes and thymocytes / splenocytes in the presence of 2 - dg [ 20 , 26 , 47 , 51 ]  . although investigations of the safety and tolerance of the combination of radiotherapy with 2 - dg at escalating doses were the main focus of the present studies , it is interesting to note that four out of ten patients who completed treatment with 2 - dg dose in the range of 200300 mg / kg bw survived > 2 years ( 3146 months ) , with a trend toward better survival at 300 mg / kg bw ( table 2 )  . 
this survival is significantly higher than the average survival of glioblastoma multiforme patients treated with conventional irradiation , where the 2 - year survival is < 10% [ 36 , 50 ]  . 
the number of patients in the present study are too small to permit any conclusions regarding treatment responses ; however , we have demonstrated that the treatment protocol as proposed here is feasible , safe , convenient and cost - effective . 
therefore , multicenter phase ii clinical trials to systematically evaluate the efficacy of combining 2 - dg ( 250 mg / kg bw ) with hypofractionated radiotherapy regimens in the management of glioblastoma have been undertaken . 
since the acute side effects ( table 1 ) , late reactions and particularly the therapeutic responses ( table 2 ) show considerable variations among patients , the individualization of the therapy based on predictive assays would be beneficial in the management of these tumors . 
in view of the large interand intratumoral heterogeneity of glioblastomas , noninvasive imaging of glucose and oxygen usage with pet combined with molecular characterization of the tumors by genomic and proteomic profiles in surgical specimens could be useful in identifying the subset of patients most likely to benefit from the combination of 2 - dg plus radiotherapy . 
 strahlentherapie und onkologie original article ultrafractionation does not improve the results of radiotherapy in radioresistant murine ddl1 lymphoma mechthild krause1 , jenny prager1 , jana wohlfarth1 , 2 , franziska hessel1 , daniela dorner1 , michael haase3 , michael c . 
joiner4 , michael baumann1 , 2 background and purpose : low - dose hyperradiosensitivity ( hrs ) , i.e. , a relatively higher efficacy of doses 0.5 gy compared to doses > 1 gy , has been shown in a number of tumor cell lines in vitro . 
 material and methods : uf was performed with 0.4 gy per fraction , three fractions per day at 7 days per week , and conventional fractionation ( cf ) with 1.68 gy per fraction , one fraction per day at 5 days per week . 
taken together with previous experiments on human a7 glioblastoma , which showed a negative effect of uf on local tumor control , the preclinical data obtained in this laboratory so far do not support the use of ultrafractionated schedules in radiotherapy . 
 key words : ultrafractionation low - dose hyperradiosensitivity lymphoma murine tumor tumor growth delay strahlenther onkol 2005 ; 181 : 54044 doi 10.1007 / s00066 - 005 - 1396 - 5 ultrafraktionierung fhrt nicht zur verbesserung des ergebnisses der strahlentherapie von radioresistenten murinen ddl1 - lymphomen hintergrund und ziel : low - dose hyperradiosensitivity ( hrs ) , d.h. 
 material und methodik : die bestrahlungen im uf - arm wurden mit 0 , 4 gy pro fraktion , drei fraktionen pro tag an 7 tagen pro woche , und im konventionell fraktionierten ( cf ) arm mit 1 , 68 gy pro fraktion , einer fraktion pro tag an 5 tagen pro woche , durchgefhrt . 
die zusammenfassende analyse der medianen relativen gdv5 fr alle tumoren dieser untersuchung ergab werte von 1 , 00 [ 95% - vertrauensbereich 0 , 99 ; 1 , 08 ] im cfund 0 , 99 [ 0 , 92 ; 1 , 01 ] im uf - arm ( p = 0 , 24 )  . 
unter bercksichtigung frherer experimente am humanen glioblastom a7 , die einen negativen effekt der uf - bestrahlung auf die lokale tumorkontrolle ergaben , sprechen die bisher im eigenen labor erzielten resultate gegen den einsatz ultrafraktionierter bestrahlungsschemata in der klinik . 
 schlsselwrter : ultrafraktionierung low - dose hyperradiosensitivity lymphom muriner tumor tumorwachstumsverzgerung 1 clinic for radiotherapy and radiation oncology , medical faculty carl gustav carus , university of technology , dresden , germany , 2experimental center , medical faculty carl gustav carus , university of technology , dresden , germany , 3 institute of pathology , medical faculty carl gustav carus , university of technology , dresden , germany , 4 department of radiation oncology , karmanos cancer institute , wayne state university , detroit , mi , usa . 
ultrafractionation in murine lymphoma low - dose hyperradiosensitivity ( hrs ) , i.e. , a higher effect per unit dose of radiation doses 0.5 gy compared to doses > 1 gy , has been demonstrated in a variety of tumor cell lines in vitro after single - dose ( reviewed in [ 4 , 15 ] ) and after fractionated irradiation [ 16 ] as well as in some normal tissues ( reviewed in [ 4 ] )  . 
irr is possibly caused by onset of repair processes after doses of 1 gy , whereas the lack of such repair responses at lower doses may explain hrs [ 3 ]  . 
a relationship to the so - called bystander effect has been suggested [ 9 ] , however , so far experimental data do not support this hypothesis [ 8 ]  . 
separate analysis of radioresistant tumor nodules ( sarcoma and melanoma ) showed longer times to regrowth after uf , suggesting a possible advantage of uf in radioresistant tumors [ 1 ]  . 
however , because of the small number of patients and the different tumor entities this study does not answer the question whether ultrafractionated irradiation results in an improvement of the outcome of radiotherapy . 
 in an ongoing cooperation project with the gray cancer institute london , uk , and wayne state university , detroit , mi , usa , the efficacy of uf is currently investigated in different tumor models in vivo . 
 material and methods animals the experiments were performed using 7to 14 - week - old female and male nmri ( nu / nu ) mice from the specific pathogen - free breeding facility of the experimental center of the medical faculty carl gustav carus , university of dresden , germany . 
for further immunosuppression total - body irradiation ( tbi ) with 4 gy x - rays ( 200 kv , 0.5 mm cu , 1.2 gy / min ) was performed 2 days before tumor transplantation . 
the murine origin of the tumor was not immediately recognized and the tumor was mistaken for being t98g and therefore used accidentally as a source for the tumors transplanted for the experiments reported here . 
for the experiments , pieces of 12 mm from a tumor with median volume doubling were transplanted subcutaneously into the right hind leg of the animals [ 5 , 13 ]  . 
 to exclude major immunogenicity of the tumor model , groups of tumors were irradiated with graded single doses under clamp hypoxic conditions with and without tbi before with tbi without tbi figure 1 . 
relative time to recurrence of ddl1 tumors after single - dose irradiation under clamp hypoxic conditions with doses of 16 , 24 , 32 , 40 , 48 , and 56 gy with ( ) or without tbi ( ( cid : 1 ) ) before tumor transplantation . 
relative zeit bis zum auftreten von rezidiven von ddl1 tumoren nach einzeldosisbestrahlung unter abgeklemmten blutflussbedingungen mit dosen von 16 , 24 , 32 , 40 , 48 und 56 gy mit ( ) und ohne ganzkrperbestrahlung ( ( cid : 1 ) ) vor der tumortransplantation . 
time course of the relative volume of ddl1 tumors after start of ultrafractionated ( ( cid : 2 ) ) or conventional irradiation ( ( cid : 3 ) ) over 2 ( a ) , 4 ( b ) , or 6 weeks ( c ) without top - up doses . 
comparison of the relative times to recurrence ( definition see determination of time to recurrence and tumor growth delay ) between the two groups yielded a p value of 0.52 , indicating no or little residual immune response reaction of the host against this tumor ( figure 1 )  . 
tumor growth delay ( gdv5 ) of ddl1 tumors after start of ultrafractionated ( ( cid : 2 ) ) or conventional irradiation ( ( cid : 3 ) ) over 2 , 4 , and 6 weeks . 
tumorwachstumsverzgerung ( gdv5 ) fr ddl1 - tumoren nach beginn einer 2 - , 4und 6 - wchigen fraktionierten bestrahlung nach dem uf ( ( cid : 2 ) ) oder cf - schema ( ( cid : 3 ) )  . 
to minimize dose uncertainties for the low - dose fractions given during uf , the dose rate for the fractionated irradiations in both arms was reduced to 0.3 gy / mfractionated irradiations were performed under normal blood flow and top up irradiations under clamp hypoxic conditions as described previously [ 5 ]  . 
uf was performed with 126 fractions in 6 weeks ( 0.4 gy per fraction , three fractions per day , 21 fractions per week , interfraction interval 6 h )  . 
tumors in the cf arm were irradiated with 30 fractions in 6 weeks ( 1.68 gy per fraction , one fraction per day , five fractions per week )  . 
we also attempted to obtain dose - response curves for local tumor control by application of graded top - up irradiations after 6 weeks of fractionated irradiation , however , this could not be achieved because of the high radioresistance of ddl1 . 
in total , the present study includes data obtained from 219 irradiated tumors , of which 90 tumors were included in the single - dose irradiation arms and 129 tumors in the comparison of uf and cf over 2 , 4 and 6 weeks ( 92 over 6 weeks , 37 over 2 and 4 weeks )  . 
ultrafractionation in murine lymphoma follow - up and determination of tumor volumes the animals were observed until the mean diameter of the recurrent tumor was 1015 mm or until death . 
tumor volumes were determined by the formula of the rotational ellipsoid / 6 * a * b2 , where a is the longest and b the perpendicular shorter tumor axis . 
in the 92 tumors irradiated over 6 weeks in the present study , 95% of the 63 recurrences occurred until day 58 , the last recurrence was scored at day 104 . 
 determination of time to recurrence and tumor growth delay comparison of the groups treated with single dose irradiation with and without previous tbi were performed as follows : for each irradiation dose group , a median time to recurrence of all tumors ( with and without tbi ) was calculated . 
for each individual tumor , the relative time to recurrence was calculated as the ratio of the absolute time to recurrence to the median time to recurrence for this dose group . 
 growth delay was evaluated from tumor growth curves of the individual animals as the time needed after start of treatment to reach five times the starting volume ( gdv5 )  . 
for calculation of the relative growth delay , the individual growth delay values were divided by the median growth delay value of all tumors irradiated with the same dose ( uf and cf )  . 
animals censored without failure after a follow - up time longer than the median growth delay in the dose group were included in the analysis with their follow - up time . 
 results figure 2 compares the tumor growth curves for irradiation of ddl1 over 2 , 4 and 6 weeks without top - up irradiation , figure 3 shows the corresponding tumor growth top - up dose ( gy ) figure 4a abbildung 4a figure 4b abbildung 4b figure 4a and 4b . 
ultrafractionation in murine lymphoma in a previous experiment reported from our laboratory using a7 , a human glioblastoma with a clear - cut hrs effect in vitro , a significantly negative effect of ultrafractionated irradiation on tumor growth delay and on local tumor control was observed [ 5 ]  . 
whereas overall , no significant advantage of uf could be demonstrated , subgroup analysis of the melanoma and sarcoma metastases showed a significant prolongation of the time to recurrence after ultrafractionated irradiation , suggesting that uf possibly improves the outcome of radiotherapy in radioresistant but not in radiosensitive tumors like lymphomas . 
our data on ddl1 and a7 [ 5 ] are in contrast to this hypothesis , because both of these tumors are radioresistant but do not show higher efficacy of uf compared with cf . 
 however , also in a7 tumors which show hrs in vitro , uf was not more efficient than cf in vivo , in fact , the results after uf were significantly inferior to cf . 
this might be explained by fading of the hrs effect after application of multiple fractions , possibly as a consequence of triggered repair mechanisms [ 5 , 7 ]  . 
alternatively , as hrs is most pronounced in g2 , different cell - cycle distributions between in vitro and in vivo conditions and between different tumor models may have influenced the results [ 5 , 11 , 14 ]  . 
taken together with previous experiments on human a7 glioblastoma , which showed a negative effect of uf on tumor growth delay and on local tumor control , the preclinical data obtained in this laboratory so far do not support the use of ultrafractionated schedules in radiotherapy . acknowledgments the authors wish to thank dorothee pfitzmann for excellent technical assistance and the team of the experimental center of the medical faculty for breeding and maintenance of high - quality nude mice . 
 key words : recurrent cervical carcinoma radiochemotherapy strahlenther onkol 2005 ; 181 : 54550 doi 10.1007 / s00066 - 005 - 1340 - 8 radiochemotherapie bei zervixkarzinomrezidiven ziel : ermittlung der wirksamkeit und toxizitt einer radiochemotherapie bei patientinnen mit zervixkarzinomrezidiven . 
eine monotherapie mit cisplatin ( 25 mg / m2 / d15 ) oder carboplatin ( 800 mg / m2 / d15 ) erhielten 5 / 24 patientinnen ( 21% ) bzw . 
 this retrospective study analyzed the effectiveness and the side effects of simultaneous chemotherapy and radiation therapy and the influence of selected prognostic factors in patients with recurrences of cervical carcinoma . 
 patients and methods patient characteristics between 1987 and 2001 , 24 patients with recurrent cervical carcinoma were treated with radiation therapy and simultaneous chemotherapy at our institution ( table 1 )  . 
as prior therapy , 6158 months earlier ( median : 24 months earlier ) , 22 patients underwent radical hysterectomy , sometimes followed by radiation therapy ( n = 8 ) or chemotherapy ( n = 1 )  . 
 patients ( n ) median age ( years ) location of recurrence pelvic sidewall recurrence ( n ) central pelvic recurrence ( n ) isolated paraaortic lymph node recurrence ( n ) tumor volume < 97 ml ( n ) > 97 ml ( n ) > 1 / 3 necrosis in the tumor mass ( n ) 5 7 48 ( range : 2677 ) 25 gy were used in two patients . 
1 / 24 patients ( 4% ) received two courses of chemotherapy with 5 - fu ( 1 , 000 mg / m2 / d15 , 2933 ) and mitomycin c ( 10 mg / m2 / d2 , 30 ) , and the patient who underwent brachytherapy alone received 20 mg / m2 of cisplatin on days 15 . 
the median dose given by external - beam to the pelvis and / or the paraaortic and iliac lymph nodes was 47 gy ( 3650 gy ) , the median dose administered to the recurrent tumor site amounted to 59.4 gy ( 5461 gy )  . 
 radical hysterectomy radical hysterectomy + chemotherapy radical hysterectomy + external - beam therapy radical hysterectomy + external - beam therapy + brachytherapy radical hysterectomy + brachytherapy external - beam therapy alone external - beam therapy + brachytherapy table 3 . 
 debulking operation external - beam radiation therapy + chemotherapy external - beam radiation therapy + brachytherapy brachytherapy + chemotherapy patients ( n ) 13 / 24 1 / 24 2 / 24 2 / 24 4 / 24 1 / 24 1 / 24 patients ( n ) 9 / 24 20 / 24 3 / 24 1 / 24 strahlenther onkol 2005 no . 
 the main endpoints evaluated included overall survival , local recurrence - free survival , and disease - free survival according to the kaplan - meier method , and the differences were determined by using the log - rank test . 
the location of recurrence was classified as pelvic sidewall recurrence , if pelvic sidewall fixation was observed in ct scan , or as central pelvic recurrence , if the tumor mass involved pelvic structures without sidewall fixation . 
 results therapy efficacy at the time of evaluation 7 / 24 patients ( 29% ) were alive without evidence of disease after a mean follow - up of 38 months ( 4137 months )  . 
the local recurrence - free , disease - free and overall survival rates at 10 years were 37% , 25% and 17% , respectively ( figures 1 to 3 )  . 
 a complete response 6 weeks after the end of therapy was achieved in 6 / 24 patients ( 25% ) , and in 8 / 24 ( 33% ) a partial response was seen . 
there was a statistically significant difference between the 5 - year survival rates of patients with large tumor volume ( > 97 cm3 ) and patients with smaller tumor volume : 8% versus 26% for overall survival ( p = 0.05 ; figure 6 ) , 8% versus 42% for disease - free survival ( p = 0.02 ; figure 7 )  . 
also , an analysis of the influence of other important treatmentor tumor - related factors such as use of radiation therapy modality and dose , tumor grading , lymphangiosis , histology , and site of recurrence , on the treatment results did not show statistically significant differences . 
cr : vollremission ; pr : teilremission ; nc : keine vernderung . diarrhea ( 38% ) , leukopenia ( 33% ) , and nausea with or without vomiting ( 21% )  . 
frequent physical examinations , ct scan , mri techniques , cytologic screening and liberal use of biopsy are effective methods [ 5 , 6 , 11 , 20 ]  . 
 if a recurrence is diagnosed , different curative treatment approaches exist : pelvic exenteration , cort ( combined operative and radiotherapeutic treatment ) , iort ( intraoperative radiation therapy ) , or irradiation with simultaneous chemotherapy [ 10 , 16 , 21 ]  . an important role to improve survival of patients subjected to nonoperative treatment modalities falls to a combined treatment with pelvic irradiation and systemic chemotherapy [ 24 ]  . 
the efficacy of radiotherapy or chemotherapy alone is limited [ 4 , 6 , 7 , 19 , 25 , 27 ]  . in our series we could show that the addition of simultaneous chemotherapy to irradiation results in a respectable survival and local control rate not only for patients with central pelvic recurrences but also for patients with pelvic sidewall recurrences and distant recurrences . 
 overall , central pelvic recurrences with small tumor sizes have a better outcome than recurrences infiltrating the pelvic wall or relapses located beyond the pelvis [ 1 , 8 , 9 , 1214 , 18 , 26 ] , for two reasons : first , recurrences limited to the vagina are more easily detected with clinical pelvic examination than are pelvic wall recurrences ; and an earlier diagnosis generally allows for detection of cervical relapses with small tumor sizes . 
the current series confirms the findings by others with a 5 - year overall survival of 39% for patients with central recurrence of cervical cancer [ 9 , 12 , 14 , 23 , 26 ]  . 
the fact that the tumor volume determines the treatment results justifies frequent follow - ups to detect locoregional recurrent cervical carcinoma , in particular pelvic sidewall recurrences , in leukopenia anemia thrombocytopenia creatinine diarrhea / nausea / vomiting erythema strahlenther onkol 2005 no . 
radiochemotherapy for recurrent cervical carcinoma ing chemotherapy to irradiation in the treatment of recurrent cervical carcinoma has been shown in other series [ 4 , 25 , 27 ]  . 
 [ 6 ] have shown that only patients with isolated paraaortic lymph node recurrence who received irradiation and concurrent cisplatin - based chemotherapy enjoyed long - term , disease - free survival . 
however , a direct comparison of delineated sections with the corresponding histomorphological sections is difficult to perform for several reasons : ( 1 ) the shape of the prostate in the human body does not only depend on its own structure , but also on surrounding tissues ; after resection , the latter are absent , so the prostate shape might be different ; ( 2 ) the prostate shrinks ( possibly asymmetrically ) during fixation ; ( 3 ) the angulation and thickness of the cut slices through the removed prostate are very difficult to accurately match with the corresponding ct or mr slices . 
therefore , in the absence of an absolute standard , we have chosen a surrogate standard , i.e. , the assessment of interobserver variability of each modality , assuming that a low interobserver variability is indicative of high precision and vice versa . 
 we have introduced mri as an adjunct to ct in radiotherapy planning for prostate cancer since 1999 and we have developed a protocol that aims at accurate and reproducible delineation of the target organs ; we hence observed a 50% decrease of the interobserver delineation variability [ 6 ]  . 
 meanwhile , we also introduced image fusion since 2004 and agree with weiss and hess that this has been beneficial to achieve accurate target definitions , although in our experience this benefit has been mainly a time gain , not a further improvement of delineation accuracy ( unpublished data )  . 
although this theoretically might have biased the results of our work , we do not agree with weiss and hess that this effect might have been dominant , as we pointed out in the last section of our article [ 6 ]  . 
in our opinion , interobserver delineation errors strahlenther onkol 2005 ; 181 : 7456 doi 10.1007 / s00066 - 005 - 8383 - 8 should be regarded as a variant of setup errors ; they are not inherent to the target volume , but the result of external influence . 
since this volume is generally overestimated on ct ( from 6.5% in our study to up to 34% in other reports [ 14 , 6 ] ) , the impact of addition of mri is a decrease of the ctv and , consequently , a decrease of the ptv . 
in the conventional radiotherapy era , the position of the target structures ( i.e. , prostate and seminal vesicles ) was usually estimated using clinical guidance and / or anteroposterior and lateral radiographs . 
but with the introduction of ct , the exciting ability to acquire a 3 - d image set of the pelvic anatomy could be exploited to directly depict the target position and boundaries , and a new era of target delineation was entered . 
in spite of the initial enthusiasm about ct - based target delineations , which was obviously much better than in the conventional radiology era , several authors perceived wide variations in target volume definition [ 14 ]  . 
possible explanations might be ( 1 ) that mri , in contrast to ct , is unable to produce tissue electron density values ( normally calculated from ct hounsfield units ) , ( 2 ) that earlier generation mri scanners might produce image distortions , ( 3 ) that the availability of mr facilities is much less than ct , or ( 4 ) that it is onerous to organize consensus readings between radiotherapists and radiologists . 
 strahlentherapie und onkologie original article the impact of varying volumes in rectal balloons on rectal dose sparing in conformal radiation therapy of prostate cancer a prospective three - dimensional analysis andrea hille , heinz schmidberger , nadja tws , elisabeth weiss , hilke vorwerk , clemens f . 
the purpose of this analysis was to quantitatively assess the optimal volume in rectal balloons concerning rectal dose sparing in different clinical target volumes ( ctvs ) in prostate cancer irradiation . 
treatment plans without a rectal balloon and with a rectal balloon inflated with 40 ml ( six patients ) or 60 ml air ( eight patients ) were generated for each ctv and compared concerning rectal dose volume histograms . 
the use of a rectal balloon filled with 60 ml air resulted in a significant decrease of the exposed rectal wall volume in all ctvs with a reduced estimated risk for chronic toxicity in case of inclusion of the proximal or entire seminal vesicles into the ctv . conclusion : the use of a rectal balloon filled with 60 ml air led to a significantly decreased proportion of the irradiated rectal wall for all ctvs . 
in case of irradiation of the prostate without the seminal vesicles , the use of a rectal balloon should be considered carefully concerning the patients imaginable discomfort using a rectal balloon and a questionable advantage concerning the estimated risk for chronic toxicity . 
 key words : radiotherapy rectal balloon prostate cancer clinical target volume strahlenther onkol 2005 ; 181 : 70916 doi 10.1007 / s00066 - 005 - 1443 - 2 prospektive dreidimensionale analyse des einflusses verschiedener volumina in rektalen ballons auf die darmschonung bei der konformalen radiotherapie des prostatakarzinoms hintergrund und ziel : der einsatz eines rektal applizierten ballons fhrt zu einem schutz der rektumhinterwand bei der bestrahlung des prostatakarzinoms . 
das ziel der vorliegenden analyse war , das optimale volumen in rektalen ballons bezglich darmschonung bei verschiedenen klinischen zielvolumina ( ctvs ) bei bestrahlung von patienten mit prostatakarzinom quantitativ zu erfassen . 
plne mit und ohne ballon , gefllt mit 40 ml ( sechs patienten ) oder 60 ml luft ( acht patienten ) , wurden fr jedes ctv erstellt und die dosis - volumen - histogramme des darms miteinander verglichen . 
im fall einer bestrahlung nur der prostata sollte der einsatz eines rektalen ballons sorgfltig geprft werden , da er den patienten unbehagen verursachen kann und der nutzen bezglich einer geschtzten reduktion der spttoxizitt fraglich ist . 
 schlsselwrter : radiotherapie prostatakarzinom strahlentherapietechnik klinisches zielvolumen 1 department of radiotherapy , university of goettingen , germany . received : march 18 , 2005 ; accepted : july 13 , 2005 strahlenther onkol 2005 no . 
rectal dose sparing in prostate cancer irradiation with rectal balloons introduction rectal toxicity following external beam irradiation of prostate cancer correlates with radiation dose , exposed rectal wall volume , in particular with the percentage of rectal volume included in the intermediate and high dose volume [ 1 , 16 , 20 , 27 , 28 ]  . 
 efforts in optimizing external beam radiation to the prostate are aiming to increase the total dose applied to the prostate while minimizing the delivered dose to the organs at risk , e.g. , the rectum [ 5 , 6 , 13 , 25 ]  . 
several reports have indicated that the use of a rectal balloon reduces prostate movement during treatment course which will allow reduced margins around the clinical target volume ( ctv ) with , consecutively , rectal dose sparing [ 24 , 22 , 23 , 26 ]  . 
additionally , the distance between prostate and the rectal posterior wall can be increased with the use of a rectal balloon , which leads , in some cases , to a protection of the posterior rectal wall [ 2 , 15 , 24 , 26 ]  . 
three studies compared dose volume histograms ( dvhs ) of the rectal wall with and without the use of a rectal balloon [ 2 , 24 , 26 ]  . 
two studies showed a significant reduction in partial posterior rectal volumes included in the high dose region as long as the seminal vesicles were not entirely included in the ctv [ 2 , 26 ]  . 
 recently , the impact of inclusion of the seminal vesicles in the ctv on rectal dose has been recognized and a risk - adapted ctv with exclusion of seminal vesicles or inclusion of the proximal 22.5 cm of the seminal vesicles [ 7 , 8 , 18 , 19 ] was suggested to reduce the risk for rectal toxicity . 
therefore , we performed a prospective analysis of prostate cancer irradiation with different ctvs to quantitatively assess the influence of the inflated volumes in rectal balloons on rectal dose sparing . 
a catheter with a rectal balloon ( rectal catheter , cat no 209000 , size 6 mm , rsch ag , kernen , germany ) was inserted into the rectum with the patient lying in lateral position on the ct couch . 
all patients had two ct scans ( 5 mm continuing , 5 mm slice ) , one with and the other without a rectal balloon the standard in our department . 
the ct scans were done directly one after the other within approximately 5 min . three - dimensional conformal computer - based planning was performed on the cadplan treatment planning system ( varian , palo alto , ca , usa )  . 
the prostate ( p ) , the prostate + entire seminal vesicles ( pesv ) , or the prostate + 60% in longitudinal direction ( 22.5 cm ) of the seminal vesicles ( ppsv ) were taken as ctv . 
since the volume of the rectum increased to a great extent with a rectal balloon in place , compared to the volume of the rectum with no rectal balloon , the rectal wall volume was outlined . 
the inner and outer walls of the rectum were both contoured with the volume of the difference being the rectal wall , as described by others [ 2 , 26 ]  . 
the craniocaudal rectal extension was defined as the first ct slice above the anal verge ( caudal border ) and the cranial limit was defined as the first slice below the sigmoid flexure . 
dose was specified according to the icru 50 report [ 17 ] : at least 95% of the ptv was covered by 95% of the prescribed dose as minimu field size was adjusted to reach this dose homogeneity criterion . 
 to determine the amount of rectal wall exposed to ionizing radiation in the presence of a 40 ml or 60 ml air - filled balloon or in the absence of a balloon , the percentages of the irradiated rectum volumes receiving 40 gy , 60 gy , 65 gy , and 70 gy were calculated three - dimensionally by the treatment planning syste if the rectal balloon gave maximum rectal protection , it was chosen for the application during radiotherapy . 
mean , median values , and standard deviations ( sd ) for the volumes of the rectal wall irradiated with a rectal balloon inflated with 40 ml air and without a rectal balloon . 
axial ct scans at the center of the prostate with and without a rectal balloon filled with 40 ml air demonstrating only a small increased distance between prostate ( ptv ) and posterior rectal wall . 
axiale ct - schichten im bereich des prostatazentrums mit einem mit 40 ml luft gefllten und ohne rektalen ballon zeigen nur eine geringe zunahme der distanz zwischen prostata ( ptv ) und hinterer rektumwand . 
the presence of a rectal balloon inflated with 40 ml compared to no rectal balloon did not significantly decrease the volume of the rectal wall receiving 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy , respectively ( table 1 )  . 
in few patients a small advantage could be shown concerning rectal dose sparing , due to a small increased distance between prostate ( ptv ) and posterior rectal wall ( figure 1 )  . 
axial ct scans with and without a rectal balloon filled with 40 ml air showing a decreased distance between seminal vesicles ( ptv ) and posterior rectal wall with the rectal balloon . 
axiale ct - schichten mit einem mit 40 ml luft gefllten und ohne rektalen ballon zeigen eine abnahme der distanz zwischen samenblasen ( ptv ) und hinterer rektumwand mit dem rektalen ballon . 
mean , median values , and standard deviations ( sd ) for the volumes of the rectal wall irradiated with a rectal balloon inflated with 60 ml air and without a rectal balloon . 
the presence of a rectal balloon inflated with 60 ml compared to no rectal balloon resulted in a significant decrease of the rectal wall receiving 40 gy and 50 gy . 
the mean values of the exposed rectal wall volume to 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy for irradiation of the prostate are demonstrated graphically in figure 4 . 
the presence of a rectal balloon inflated with 60 ml compared to no rectal balloon resulted in a significant decrease of the rectal wall receiving 40 gy , 50 gy , and 60 gy ( table 2 )  . 
 the mean values of 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy for the rectal wall in case of irradiation of the ppsv and pesv are demonstrated graphically in figures 5 and 6 . 
axial ct scans of one patient with and without a rectal balloon filled with 60 ml air demonstrating a decreased distance not only between prostate ( ptv ) and posterior rectal wall but also between seminal vesicles ( ptv ) and posterior rectal wall . 
axiale ct - schichten eines patienten mit einem mit 60 ml luft gefllten und ohne rektalen ballon zeigen nicht nur eine grere distanz zwischen prostata ( ptv ) und hinterer rektumwand , sondern auch zwischen samenblasen ( ptv ) und hinterer rektumwand . 
rectal dose sparing in prostate cancer irradiation with rectal balloons ( % ) ( % ) ( % ) no 60 ml no = no balloon 60 ml = balloon filled with 60 ml air no 60 ml no = no balloon 60 ml = balloon filled with 60 ml air no 60 ml no 60 ml no 60 ml no 60 ml no 60 ml no 60 ml no 60 ml no 60 ml 40 gy 50 gy 60 gy 65 gy 70 gy 40 gy 50 gy 60 gy 65 gy 70 gy mean value mean value standard error mean value standard deviation mean value mean value standard error mean value standard deviation figure 4 . 
mean values , standard error , and standard deviations ( sd ) for the rectum exposed to 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy with and without a rectal balloon filled with 60 ml air in case of irradiation of the prostate only . 
mean values , standard error , and standard deviations ( sd ) for the rectum exposed to 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy with and without a rectal balloon filled with 60 ml air in case of irradiation of the prostate + proximal seminal vesicles . 
vergleich der mittelwerte , standardfehler und standardabweichungen ( sd ) der mit 40 gy , 50 gy , 60 gy , 65 gy und 70 gy belasteten darmvolumina mit einem mit 60 ml luft gefllten und ohne rektalen ballon bei bestrahlung der prostata . 
vergleich der mittelwerte , standardfehler und standardabweichungen ( sd ) der mit 40 gy , 50 gy , 60 gy , 65 gy und 70 gy belasteten darmvolumina mit einem mit 60 ml luft gefllten und ohne rektalen ballon bei bestrahlung der prostata + proximalen samenblasen . 
 ing effect of rectal balloons on the rectal exposure during radiotherapy for prostate cancer has been defined differently in different studies , we asked the question whether this dose sparing effect might be depending on the volume of the inserted balloons or the definition of the ctv for prostate cancer irradiation [ 2 , 24 , 26 ]  . 
 rectal balloons several studies have reported a reduction of the percentage of rectal wall included in the intermediate and high dose volume with a rectal balloon [ 2 , 24 , 26 ]  . 
 similarly , the volumes of the rectal wall receiving intermediate and high doses could not be significantly decreased with 40 ml air filled in a rectal balloon in our study , neither in irradiation of the p , ppsv , nor pesv . 
in irradiation of the prostate + seminal vesicles with a rectal balloon filled with 60 ml air no 60 ml no = no balloon 60 ml = balloon filled with 60 ml air no 60 ml no 60 ml no 60 ml no 60 ml 40 gy 50 gy 60 gy 65 gy 70 gy mean value mean value standard error mean value standard deviation figure 6 . 
mean values , standard error , and standard deviations ( sd ) for the rectum exposed to 40 gy , 50 gy , 60 gy , 65 gy , and 70 gy with and without a rectal balloon filled with 60 ml air in case of irradiation of the prostate + entire seminal vesicles . 
vergleich der mittelwerte , standardfehler und standardabweichungen ( sd ) der mit 40 gy , 50 gy , 60 gy , 65 gy und 70 gy belasteten darmvolumina mit einem mit 60 ml luft gefllten und ohne rektalen ballon bei bestrahlung der prostata + ganzen samenblasen . 
 authors used rectum definition ( outlined structure craniocaudal borders ) rectal volume ( % ) risk for chronic rectal toxicity ( % ) toxicity grade used toxicity score median follow up koper et al . 
 [ 3 ] whole rectum anal verge to the sigmoid flexure ( patients with large air / fecal content in the rectum were excluded from analysis ) greco et al . 
 [ 9 ] whole rectum anal verge to the sigmoid flexure whole rectum anal verge to the sigmoid flexure ( patients with large air / fecal content in the rectum ) fiorino et al . 
 in irradiation of the prostate only with a rectal balloon filled with 60 ml air the volumes of the rectal wall receiving 60 gy , 65 gy , and 70 gy were 18% , 14% , and 10% , compared to 35% , 30% , and 25% without a rectal balloon . 
in our study the rectal wall volume receiving 60 gy , 65 gy , and 70 gy without a rectal balloon was much smaller , compared to the study of patel et al . 
the use of a rectal balloon filled with 60 ml air in our study did lead to a significant reduction of the rectal wall volume receiving 40 gy and 50 gy , but not to a significantly reduced rectal wall volume receiving 6070 gy ( table 2 )  . 
were as follows : 30% , 25% , and 20% with a rectal balloon , compared to 60% , 55% , and 50% without a rectal balloon [ 24 ]  . 
 estimated risk for chronic rectal toxicity several investigations indicate a relationship between dvhs and the development of chronic rectal toxicity [ 1 , 3 , 9 , 11 , 16 , 20 , 28 ]  . 
to associate the rectal dvhs in our study with an estimated risk for chronic rectal toxicity , the results were compared with studies analyzing relationships between dose volume and rectal toxicity . 
it is known that there is a high variability of volume fractions of rectal dvhs depending on how the rectal borders are defined , and it is difficult to compare the results of different studies concerning rectal dvhs [ 12 , 14 ]  . 
we decided to contour the rectal wall in our study , because the volume of the rectum increased to a great extent with a rectal balloon in place compared to the volume of the rectum with no rectal balloon . 
 studies analyzing either dose volume relationships of the rectal wall with or without the craniocaudal definition which we have used in our study , or studies using an identical or similar craniocaudal definition of the whole rectum are summarized in table 3 . 
found that the most significant volume effect with respect to moderate / severe late rectal bleeding at 3 years was 60 gy for the rectal wall [ 20 ]  . 
when 70% of the rectal volume received < 60 gy , rectal bleeding occurred in 20% , compared to 52% , when 70% of the rectal wall received > 60 gy . 
 [ 1 ] found a 9% risk for grade 2 late rectal toxicity when > 30% of the rectal wall was exposed to 70 gy compared to no grade 2 late rectal toxicity when < 30% of the rectal wall was exposed to 70 gy . 
others found a higher risk for late rectal toxicity when > 50% of the rectal volume was exposed to 50 gy , or when > 40% of the rectal volume was exposed to 60 gy [ 3 ]  . 
 [ 9 ] supposed to keep the volume of the rectum exposed to 50 gy < 6065% and the volume of the rectum exposed to 60 gy < 5055% to keep the risk of developing late rectal toxicity grade 2 < 510% . 
recommended to keep the volume of the rectum exposed to 50 gy < 6065% , the volume of the rectum exposed to 60 gy < 4555% , and the volume of the rectum exposed to 70 gy < 2530% to keep the rate of moderate / severe rectal bleeding < 510% [ 11 ]  . 
found no rectal bleeding when the rectal volume exposed to 60 gy was < 42% compared to 7.7% rectal bleeding when > 60 gy were exposed to > 42% of the rectal volume [ 28 ]  . 
 though the definitions of the rectum differ in some of these studies from our definition , and though the cutoff levels and the resulting risks for chronic rectal toxicity grade 2 are different in these studies , we can draw cautious conclusions from our results regarding an estimated risk for chronic rectal toxicity . 
 [ 28 ] can easily be met in our study without using a rectal balloon in case of irradiation of the prostate only ( tables 1 and 2 )  . 
we can conclude from our data that the risk for chronic rectal toxicity grade 2 in all patients in our study who were treated with irradiation of the prostate only was < 5% with or without the use of a rectal balloon . 
therefore , the use of a rectal balloon in case of irradiation of the prostate only should be considered carefully concerning the patients imaginable discomfort with the use of a rectal balloon and a questionable advantage concerning the estimated risk for chronic toxicity . 
 ppsv and pesv for irradiation of the ppsv and pesv the recommendations can only be met with using a rectal balloon filled with 60 ml air ( table 2 )  . 
in case of irradiation of the ppsv , the achievable values resulted in a 515% risk for chronic rectal toxicity grade 2 without the use of a rectal balloon and in a risk < 10% with the use of a rectal balloon filled with 60 ml air . 
in case of irradiation of the pesv , the values for rectal wall exposure resulted in a 1520% risk for chronic rectal toxicity grade 2 without the use of a rectal balloon and with the use of a 60 ml air - filled rectal balloon in a risk below that for chronic rectal bleeding . 
in case of irradiation of the prostate without the seminal vesicles , the use of a rectal balloon should be considered carefully concerning the patients imaginable discomfort using a rectal balloon and a questionable advantage concerning the estimated risk for chronic toxicity . 
 strahlentherapie und onkologie original article feasibility and early results of interstitial intensity modulated hdr / pdr brachytherapy ( imbt ) with / without complementary external - beam radiotherapy and extended surgery in recurrent pelvic colorectal cancer juergen tepel1 , peter niehoff2 , frank bokelmann1 , fred faendrich1 , bernd kremer1 , andreas schmid3 , gyoergy kovcs2 , 4 background : a new multimodality treatment concept consisting of extended resection and postoperative fractionated intensity - modulated interstitial brachytherapy ( imbt ) was introduced for pelvic recurrence of colorectal carcinoma . 
patients were treated either with high - dose - rate brachytherapy ( hdr ; n = 23 ) or with pulsed - dose - rate brachytherapy ( pdr ; n = 23 )  . 
 key words : brachytherapy pelvic recurrence colorectal cancer extended surgery intensity modulation strahlenther onkol 2005 ; 181 : 696703 doi 10.1007 / s00066 - 005 - 1401 - z durchfhrbarkeit und erste ergebnisse der interstitiellen intensittsmodulierten hdr / pdr - brachytherapie ( imbt ) mit / ohne perkutane bestrahlung und erweiterter chirurgischer resektion bei pelvinen kolorektalen karzinomrezidiven hintergrund : zur behandlung von beckenrezidiven bei kolorektalen karzinomen wurde die erweiterte chirurgische resektion mit anschlieender postoperativer fraktionierter intensittsmodulierter interstitieller brachytherapie ( imbt ) als neuartige interdisziplinre behandlungsform entwickelt und in einer nicht randomisierten beobachtungsstudie untersucht . patienten und methodik : 46 patienten erhielten eine erweiterte chirurgische resektion im kleinen becken mit direkter aufnhung von brachytherapieapplikatoren auf das clipmarkierte tumorbett . 
die patienten wurden entweder mit high - dose - rate ( hdr - ) brachytherapie ( n = 23 ) oder mit pulsed - dose - rate - ( pdr - ) brachytherapie ( n = 23 ) behandelt . 
bei 25 patienten wurde eine zustzliche perkutane bestrahlung des beckens bis 45 gy durchgefhrt . ergebnisse : der mediane nachbeobachtungszeitraum betrug 20 , 6 monate ( 7107 monate ) und das mittlere berleben 25 , 7 25 , 8 monate ( median 17 , bereich 1107 monate )  . 
es zeigte sich ein trend zugunsten der pdr - brachytherapie im vergleich zur hdr - brachytherapie ; dieser trend war statistisch signifikant fr patienten , die keine zustzliche perkutane strahlentherapie erhielten . 
hierbei scheint in diesem kleinen und sehr inhomogenen patientengut die pdr - therapie effektiver als die hdr - therapie zu sein , insbesondere wenn keine zustzliche perkutane radiatio mglich ist . 
 schlsselwrter : brachytherapie intensittsmodulation kolorektale karzinome rezidive im becken erweiterte resektion introduction although the rate of local recurrence following surgical treatment of rectal cancer has been reduced by total mesorectal excision [ 5 , 10 , 19 ] and , in addition , by preand postoperative radiochemotherapy [ 6 , 22 , 30 ] , it still varies in different series from 3% to 19% [ 2 , 3 , 21 ]  . 
 some authors report a 5 - year survival rate of about 30% after extended sacral resection alone , at the cost of a high perioperative mortality and severe morbidity [ 31 ]  . 
multimodality treatment is likely to provide a better therapeutic option [ 4 , 9 , 24 ] , but is often limited by the fact that many patients have undergone previous radiotherapy . 
 we have introduced a treatment concept for recurrent pelvic colorectal cancer , which combines extended surgical resection and postoperative fractionated intensity - modulated interstitial brachytherapy ( imbt ) with or without complementary external - beam irradiation ( ebrt )  . 
 stage and treatment of primary tumors primary tumor stage was reported as follows : stage i in 22.2% , stage ii in 32.6% , stage iii in 39.1% , and stage iv in 6.7%. 
 pelvic recurrence in 35 patients local recurrence had occurred for the first time , eleven patients had been treated for local recurrence before ( one patient ebrt alone , seven patients ebrt + chemotherapy , two patients resection of local recurrence + chemotherapy , one patient resection + ebrt + chemotherapy )  . 
 ing of all patients included abdominal and thoracic ct scan , endorectal ultrasound whenever possible , colonoscopy , biopsy for histology ( either by endoscopy or sonographically guided needle aspiration ) and measurement of tumor markers ( carcinoembryonic antigen [ cea ] , cancer antigen [ ca ] 19 - 9 )  . 
plastic tubes were inserted through the perineum or lower abdominal wall by the surgeon in cooperation with the radiotherapist , and fixed onto the tumor site by single sutures placed in multiple locations ( figure 1 )  . 
the geometry of the single plain tubes predefined an optimal dose distribution with intertube distances of 812 m whenever possible , an omental pedicle flap was used to displace dose - limiting anatomic structures ( small bowel , large vessels , nerves , ureter , etc . ) away from the region of brachytherapy . 
in lack of guidelines for imbt dose prescription in the literature , we allowed maximum 10 mm distance between the lateral tubes and a maximum of four times prescription dose on the surface of the plastic tubes . 
subsequently , brachytherapy with 535 gy ( mean 24.5 gy ) was administered using hdr ( 370 gbq iridium - 192 [ 192ir ] source ) or pdr ( 37 gbq 192ir source ) using a remote afterloading machine . 
 results surgical therapy 21 patients ( 45.7% ) received resection of pelvic tumor ( abdominoperineal resection or low anterior resection ) , twelve patients ( 26.1% ) had an anterior or posterior pelvic exenteration , and 13 patients ( 28.3% ; seven in the pdr and six in the hdr group ) were treated by combined intraand extrapelvic multivisceral resection ( e.g. , resection of liver or pulmonary metastases or segmental resection of small intestine )  . 
in 23 patients ( 50% ) the surgeon assessed the resectional state as r2 when no clear resection margin could be achieved due to tumor growth close to the sacral of pelvic bone with possible infiltration . 
 hdr ( n = 23 ) pdr ( n = 23 ) surgery abdominoperineal rectum resection pelvic tumor resection low anterior rectal resection hartmanns procedure resection of liver metastases resectional state r0 r1 r2 additional ebrt yes additional chemotherapy yes ebrt + chemotherapy 9 3 1 4 5 5 6 strahlenther onkol 2005 no . 
 toxicity of radiation therapy there were no cases of severe early toxicity ( grade 3 and 4 rtog / eortc scale ) with regard to skin , bladder and small or large intestine . 
six patients developed perineal necrosis , in some patients extending up to the presacral plane with severely impaired wound healing , which required long - term treatment including surgical debridement and vacuum wound closure . 
 there was a trend toward a better survival of patients who had received r0 resection ( 46% ) compared to those with incomplete tumor resection ( r1 , r2 ; 14% )  . 
local control had a clear impact on survival , as no patient suffering from local recurrence ( n = 25 ) survived > 3 years , whereas > 40% of patients being free of local recurrence ( n = 21 ) were alive after 4 years . 
 disease - free survival in 34 patients tumor relapse was diagnosed during follow - up ( local in 24 , distant in 19 , and both in nine patients ) leading to a disease - free survival rate of 20% after 5 years ( figure 4b )  . 
again , there was a trend toward better diseasefree survival for the pdr protocol ( 30% ) compared to the hdr protocol ( 14% ; p = 0.47 ) in the whole group ( n = 46 )  . 
the fact that local control was achievable in these cases is most likely to be explained by a virtual minimal margin of remaining tumor , mostly at the osseous sacral plane , which does not necessarily reflect actual bone infiltration . 
patients receiving tumor resection only had significantly better local control rate than those who required resection of extrapelvic metastases ( p = 0.0233 ) ; other differences did not reach statistical significance ( data not shown )  . 
this effect reached statistical significance ( p = 0.026 ) in the subgroup of patients who exclusively received irradiation by imbt without additional ebrt ( n = 21 ; table 3 )  . 
it still occurs , although significant progress has been made especially in the treatment of primary rectal cancer by the introduction of total mesorectal excision and perioperative radiochemotherapy for advanced tumor stages . 
it is generally accepted that the best approach for long - term survival in local recurrence is extensive surgical resection whenever possible [ 23 , 27 ] , for which 5 - year survival rates of 1930% have been reported [ 11 , 23 , 28 ]  . 
 nevertheless , in many patients this is hardly possible and might require sacral resection , which is associated with a high complication rate and poor wound healing [ 29 , 30 ]  . 
our approach of a postoperative brachytherapy via intraoperatively inserted and individually sutured plastic tubes offers the very individual possibility to carefully calculate volume and dose distribution , which can thereafter be applied in multiple carefully planned fractions . 
 additionally , introducing imbt ( in other words : individually volume - optimized dose distribution according to target and critical structure volumes similar to the step - and - shoot technique in intensity - modulated external beam therapy ) higher and more conformal dose delivery becomes possible including an excellent intraoperative target definition and the radiobiological advantage of fractionated irradiation [ 16 ]  . 
 a 5 - year overall survival rate of 23% , a disease - free survival rate of 20% and a local control rate of 33% in our retrospective analysis correspond to multimodality treatment series of other investigators [ 1 , 29 ]  . 
however , this was reached with a high number of late side effects resulting in limited quality of life , and no data with local control were published [ 20 ]  . 
a reported disease - free survival rate of 47% [ 9 ] after 2 years , which is superior to that observed in our patients ( 25% ) , is very likely to be explained by a more unfavorable patient selection in our study : 28.2% received simultaneous resection of distant metastases and microscopically proven complete resection was documented in 24% only . the resectional state , being a highly significant parameter with regard to overall survival , disease - free survival and local control as observed in our patients , has been shown likewise by several other groups [ 1 , 8 ]  . 
this corresponds to the finding that local control is a positive predictor of overall survival , although it failed to reach statistical significance in this analysis . no patient requiring resection of distant metastases ( hepatic or pulmonary ) did survive > 2 years . 
we would only exclude patients from combined operative therapy when irresectable extrapelvic disease or circumferential pelvic tumor with bilateral ureteric obstruction is present or advanced tumor pelvic bone lesions are present or those in whom general condition does not allow extensive surgery . in all analyses , for pdr , the results were , according to tendency , better than for hdr . 
in patients who had undergone previous ebrt and therefore exclusively received imbt for the treatment of pelvic recurrence , this superiority of pdr did reach statistical significance with regard to local tumor control . 
as local control is a significant parameter for survival , one might speculate that the effect of pdr will be more pronounced also in terms of overall and disease - free survival with an increase in patient numbers and statistical power . 
 strahlentherapie und onkologie original article no effect of the hemoglobin solution hboc - 201 on the response of the rat r1h tumor to fractionated irradiation annette raabe1 * , andr gottschalk2 * , matthias hommel2 , hans - hermann dubben3 , thomas strandl4 background and purpose : tumor hypoxia is regarded as one important underlying feature of radioresistance . 
the authors report on an experimental approach to improve tumor response to radiation by combining fractionated irradiation with hboc - 201 , an ultrapurified polymerized hemoglobin solution , which is currently used in clinical phase ii / iii trials as alternative oxygen carrier and proved to be highly effective in tissue oxygenation ( tpo2 )  . 
 material and methods : subcutaneously growing rhabdomyosarcoma r1h tumors of the rat were treated with either 40 gy ( 2 gy / fraction , 20 fractions in 2 weeks , ambient ) followed by graded top - up doses ( clamped ) alone , or in combination with hboc - 201 , or with hboc - 201 plus carbogen ( 95% o2 + 5% co2 )  . 
in addition , the effect of hboc - 201 alone or in combination with carbogen on the tpo2 of tumor and muscle was determined using a flexible stationary probe ( licox , gms )  . 
 results : tcd50% values of 119 gy ( 95% confidence interval 103 ; 135 ) , 111 gy ( 84 ; 138 ) , and 102 gy ( 83 ; 120 ) were determined for tumors irradiated alone , in combination with hboc - 201 , and with hboc - 201 plus carbogen , respectively . 
although the dose - response curves showed a slight shift to lower doses when hboc - 201 or hboc - 201 plus carbogen was added , the differences in tcd50% were not statistically significant . 
 key words : tumor oxygenation hemoglobin solution rhabdomyosarcoma r1h of the rat irradiation fractionation strahlenther onkol 2005 ; 181 : 7307 doi 10.1007 / s00066 - 005 - 1418 - 3 kein einfluss der hmoglobinlsung hboc - 201 auf die wirksamkeit einer fraktionierten bestrahlung des r1h - tumors der ratte hintergrund und ziel : strategien zur berwindung der hypoxievermittelten radioresistenz von tumoren sind gegenwrtig von groem klinischen und wissenschaftlichen interesse . 
es wurden gesamtdosen von 40 gy fraktioniert verabreicht ( 2 gy / fraktion , 20 fraktionen in 2 wochen ) und mit top - up - dosen auf gesamtdosen aufgesttigt , die eine bestimmung der lokalen tumorkontrolle ermglichten . 
 1 department of radiotherapy and radiation oncology , university hospital hamburg - eppendorf , hamburg , germany , 2 department of anesthesiology , university hospital hamburg - eppendorf , hamburg , germany , 3 department of primary medical care , university hospital hamburg - eppendorf , hamburg , germany , 4 department of anesthesia and critical care medicine , solingen , germany . received : january 26 , 2005 ; accepted : may 13 , 2005 strahlenther onkol 2005 no . 
es wurde eine nur geringfgige verringerung der tcd50% - werte von 119 gy ( 95% - konfidenzintervall : 103 ; 135 ) auf 111 gy ( 84 ; 138 ) bzw . 
die oxygenierung von tumorund muskelgewebe konnte durch carbogenatmung , nicht aber durch hboc - 201 verbessert werden . schlussfolgerung : die wirksamkeit einer fraktionierten tumorbestrahlung wird durch niedrigdosierte hmoglobinlsung hboc - 201 nicht verbessert . 
 schlsselwrter : tumoroxygenierung hmoglobin rhabdomyosarkom der ratte fraktionierte bestrahlung introduction tumor hypoxia is a generally accepted marker for tumor malignancy , since hypoxic tumors show a poorer treatment outcome in terms of local tumor control and overall survival [ 9 , 12 ]  . 
 tumors are characterized by their chaotic vascular network and large temporal fluctuations in blood flow ; consequently , they exhibit a varying proportion of hypoxic cells [ 8 , 37 39 ]  . 
tumor hypoxia is determined in a number of clinical and experimental settings [ 1 , 17 , 22 , 40 ] and correction for hypoxia is an important issue in the clinic [ 2 , 7 ]  . 
a number of therapeutic strategies have been established to determine and to overcome tumor hypoxia by improving oxygen supply either by oxygen or carbogen breathing or by increasing the hemoglobin level and oxygen delivery [ 6 , 16 , 30 ]  . 
an enhancement of tissue oxygenation ( tpo2 ) in experimental tumors associated with an increased tumor growth delay was reported for hemoglobin solutions combined with single - dose irradiation [ 32 , 35 ] as well as with chemotherapeutic agents [ 33 , 36 ]  . 
 hboc - 201 ( biopure , cambridge , ma , usa ) is a cellfree ultrapurified polymerized bovine hemoglobin solution without significant side effects on liver , kidney and coagulation [ 1820 ]  . 
low oxygen affinity ( p50 = 34 mmhg ) , which is regulated by chloride ions rather than by 2 , 3 - diphosphoglycerate ( 2 , 3 - dpg ) , and a pronounced bohr effect are the main advantages of bovine over human hemoglobin [ 10 , 15 ]  . 
the higher oxygen extraction ratio from hboc results in a relative tissue oxygenation potential that is threeto fourfold higher than that of stored autologous red cells [ 27 ]  . 
the favorable oxygen binding curve of hboc - 201 with a low oxygen affinity results in facilitated oxygen release to oxygen - deprived tissue , e.g. , in poststenotic areas [ 13 ]  . 
hboc - 201 was additionally combined with carbogen ( 95% o2 + 5% co2 ) , which has been shown to be an effective and nontoxic radiosensitizer , both in clinical and experimental settings [ 11 , 16 , 26 ]  . 
since free hemoglobin is known to act as a nitric oxide ( no ) scavenger and thus might lead to vasoconstriction , the addition of carbogen to the treatment seemed reasonable to overcome hboc - 201induced vasoconstriction by co2 - induced vasodilation . 
 material and methods tumor model the study was approved by the ethics committee of the hamburg ministry of health , and supervised according to the german law for animal protection from 1987 . 
 local tumor irradiation and experimental design local irradiation was given using 200 kvp x - rays ( 0.5 mm additional cu filtering ; dose rate 1.0 gy / min )  . 
the animals were shielded by a rotable lead cylinder ( 1 mm ) , that allowed to adjust the tumor precisely into the radiation beathe correct positioning of the tumor during irradiation was monitored using a tv camera . 
the problem of dose inhomogeneity was partly overcome by alternating irradiation of the tumors from opposite sides , leaving a dose difference between tumor center and periphery of < 10% . 
however , the dose difference between tumor center and periphery for most of the tumors was < 5% , which , with regard to other sources of error , seems to be tolerable . for studying the effect of hboc - 201 , a daily intravenous ( i.v. ) application of the hemoglobin solution throughout the treatment time had to be assured . 
to minimize the risk of rupture or breakdown of the catheter system , the treatment time was reduced to 2 weeks in which a fractionated dose of 40 gy was administered under ambient conditions using 200 kvp x - rays ( 0.5 cu filter , dose rate 2 gy / min ) applying two fractions of 2 gy per day with no irradiation during the weekend . 
since 40 gy are far beyond the threshold dose for local tumor control , graded top - up doses ranging from 0 to 70 gy were given on the clamped tumor 12 h after the last fraction . 
this method of applying top - up doses is generally used in the experimental setup of tumor irradiation on animals when an appropriate fractionation of the total dose high enough to achieve tumor control cannot be administered . 
top - up doses have to be applied under clamped conditions , since a clamped tumor is 100% hypoxic and no individual variations of hypoxia can occur [ 15 ]  . 
originally , top - up doses of 1050 gy were planned , but since no local control could be achieved in the lower dose groups , these were modified to up to 110 gy accumulative dose . 
volume was calculated after correction for skin thickness using the formula v = / 6 ( a2d ) ( b2d ) 2 , where a is the longest and b the perpendicular tumor axis and d the measure of the skgrowth delay was strahlenther onkol 2005 no . 
 figure 1 shows the observed local tumor control rates and the calculated tumor control probabilities for r1h tumors treated with fractionated irradiation alone or in combination with hboc - 201 , and hboc - 201 plus carbogen , respectively . 
combination of radiation treatment with hboc - 201 or with hboc - 201 plus carbogen resulted in a slight shift of the dose - response curves toward lower doses ; this was more pronounced for the combination of hboc - 201 with carbogen , but no statistically significant reduction of the tcd50% could be demonstrated in either group . 
 statistical analysis using maximum likelihood techniques , dose - modifying factors ( dmfs ) and their 95% confidence intervals ( cis ) were calculated from p = e vin0eddmfcadmfhboc eq . 
after induction of anesthesia ( 0.5 mg / 100 g xylazine and 4.5 mg / 100 g ketamine hydrochloride i.m. ) , a tracheotomy was performed and animals were ventilated via a 16 - g cannula with an fio2 of 0.21 ( tidal volume 7 ml kg1 , respiratory frequency 80 min1 )  . 
a central venous catheter was placed in the left or right jugular vein , an arterial line for withdrawal of blood and blood pressure measurement was placed in the left or right carotid artery . 
lokale tumorkontrollraten nach alleiniger fraktionierter bestrahlung ( ( cid : 1 ) ) , sowie nach bestrahlung in kombination mit hboc - 201 ( ( cid : 2 ) ) bzw . 
tcd50% values ( 95% confidence interval [ ci ] ) obtained for r1h tumors irradiated alone or in combination with hboc - 201 , or with hboc - 201 plus carbogen . 
 irradiation + hboc - 201 + hboc - 201 + carbogen tcd50% ( gy ) 95% ci 119 103 ; 135 111 84 ; 138 83 ; 120 hboc - 201 , and hboc - 201 plus carbogen , respectively . 
the results are depicted in figure 2 , which shows the median growth delay per gy for the n = 35 n = 30 n = 28 three different treatment arms . 
 influence of hboc - 201 , carbogen , or a combination of both on the tpo2 within tumors and skeletal muscle animals of all groups were comparable with respect to body weight and tumor volume . 
the effect of hboc - 201 , carbogen , or the combination of both on arterial po2 , mean arterial pressure , paco2 and plasma hemoglobin concentrations are summarized in table 2 . 
 no significant changes of arterial po2 were observed neither 15 nor 60 min after application of hboc - 201 , whereas carbogen breathing alone or in combination with hboc - 201 resulted in a significant increase in arterial po2 at each time of measurement . 
an increase was also seen 60 min after treatment with hboc - 201 plus carbogen , but no change of tpo2 could be detected after application of hboc - 201 alone ( figure 3a )  . 
a significant increase in oxygen tensions 15 and 60 min after carbogen breathing alone or in combination with hboc - 201 was also seen in the skeletal muscle on the opposite leg ( figure 3b ) , whereas hboc - 201 alone had no effect . 
growth delay ( gd ) per gy of recurrent r1h tumors treated with irradiation alone or in combination with hboc - 201 , or with hboc - 201 plus carbogen . 
 for socioeconomic reasons the development of safe and effective synthetic oxygen carriers as an alternative to allogenic red blood cells was an important issue in clinical medicine during the last 2 decades . 
mean arterial blod pressure ( map ) and oxygenation parameters of animals treated with 0.3 g / kg hboc - 201 , carbogen alone , and a combination of hboc - 201 with carbogen . 
since bovine hemoglobin solutions proved very effective in tissue oxygenation [ 21 ] with no significant side effects on liver , kidney and coagulation [ 19 , 20 ] , their application for sensitizing tumors in radiation therapy was nearby . 
 a clinical phase i / ii study on the effect of polyethylenegycol - conjugated hemoglobin ( enzon corp . , usa ) for radiosensitization of tumors has been performed , but results are not published until now . 
in contrast to the application of erythropoietin , which results in an increase in red blood cells , plasmatic hemoglobin is able to transport oxygen into tissue areas which red blood cells are unable to reach because of their greater diameter . 
 plasmatic transport of hemoglobin after application of hemoglobin solutions and the diffusive oxygen delivery , which is facilitated by the lack of 2 , 3 - dpg dependency in comparison to red blood cells , should be able to improve tissue oxygenation in a hypoxic tumor . 10 years ago , an improvement of tumor response to radiation treatment as well as to chemotherapy by hemoglobin solutions was shown . 
these studies on different mouse tumors [ 31 , 32 , 33 , 35 ] demonstrated an effect on growth delay and cell survival in the in vivo - in vitro excision assay after single - dose irradiation or fractionated treatment applying five fractions . 
 the present study was performed in order to determine the effect of the bovine hemoglobin solution hboc - 201 alone or in combination with carbogen on the tumor response to fractionated irradiation , since this is a clinically more relevant setting . 
it can be speculated that the lacking effect of the hemoglobin solution can be explained by an insufficient proportion of the hypoxic fraction of this tumor , but this seems not reasonable , since carbogen breathing alone seemed to reduce the tcd50% ( figure 2 and table 1 )  . 
 the ability of hboc - 201 to provide adequate tissue oxygenation independent of the number of perfused blood vessels ( convective oxygen supply ) and / or erythrocytes was shown in an experiment on dogs [ 27 ]  . 
since no effect of low - dose hboc - 201 on radiation therapy was seen in our study , one has to draw the conclusion that hboc - 201 did not increase the oxygen supply in tumors as aimed for . 
 our results are in conflict with the literature [ 21 , 32 , 34 ] , where an improvement of radiation response of experimental murine tumors after treatment with hemoglobin solutions is reported . 
with the dosage of 0.3 g / kg hboc - 201 we were able to achieve a plasmatic hemoglobin concentration of 0.50.8 g / dl , which we considered to be high enough for improvement of tissue oxygenation according to previous studies [ 2729 ]  . 
we conclude that hboc - 201 has the potential to improve tissue oxygenation when hemoglobin concentration is extremely reduced , comparable to the clinical situation of highly anemic patients , but obviously this is not the case for a normal hemoglobin status . 
 conclusion in summary , low - dose hboc - 201 does not affect the radiobiologically relevant hypoxic fraction of the r1h tumor and possibly of tumors in general , and its application proved not beneficial in terms of tumor response . 
 strahlentherapie und onkologie current discussion effects of insulin - like growth factor - 1 ( igf - 1 ) and amifostine in spinal cord reirradiation carsten nieder1 , roger e . 
kian ang3 purpose : to test whether insulin - like growth factor - 1 ( igf - 1 ) and amifostine modulate the reirradiation tolerance of rat cervical spinal cord . 
initial experiments by the authors group suggested that administration of each agent alone significantly increased the median latent time to radiation myelopathy ( rm ) in previously unirradiated animals but did not change the dose - response relationship . 
 material and methods : the cervical spinal cord of 51 adult fisher f - 344 rats received a single fraction of 16 gy , which corresponds to approximately 75% of the median paresis dose ( ed50 ) , followed 5 months later by a second radiation dose , which ranged from 17 to 21 gy . 
the study animals received a single intrathecal injection of 0.3 mg amifostine into the cisterna magna 3060 min before reirradiation plus three subcutaneous doses of igf - 1 ( 700 g ) starting from 24 h before to 24 h after reirradiation . 
rm occurred in controls versus treated rats after a mean latency of 218 versus 314 days ( 19 gy ; p = 0.11 ) and 104 versus 186 days ( 21 gy ; p = 0.002 ) from second dose ( figure 1 )  . 
 key words : radiation myelopathy spinal cord radiotherapy reirradiation growth factors insulin - like growth factor - 1 amifostine strahlenther onkol 2005 ; 181 : 6915 doi 10.1007 / s00066 - 005 - 1464 - x wirkung von insulin - like growth factor - 1 ( igf - 1 ) und amifostin bei der zweitbestrahlung des rckenmarks ziel : untersuchung der fhigkeit von insulin - like growth factor - 1 ( igf - 1 ) und amifostin , die zweitbestrahlungstoleranz des rckenmarks von ratten zu beeinflussen . 
erste eigene experimente ergaben , dass die applikation jeder einzelsubstanz bei noch nicht vorbestrahlten tieren die mediane latenzzeit bis zum auftreten einer strahlenmyelopathie signifikant verlngerte , ohne jedoch die dosis - wirkungs - beziehung zu verndern . 
da die substanzen unterschiedliche wirkmechanismen aufweisen , wurde die kombination der beiden behandlungen in einem folgeexperiment getestet . material und methodik : das zervikale rckenmark von 51 erwachsenen fisher - f - 344 - ratten erhielt eine einzeitdosis von 16 gy , die ca . 
 schlsselwrter : strahlenmyelopathie rckenmarksbestrahlung zweitbestrahlung wachstumsfaktoren insulin - like growth factor - 1 amifostin introduction radiobiological advances and technical developments have contributed significantly to reduce the risk of radiation - induced spinal cord damage . 
in some instances , reduced doses per fraction and methods to decrease the irradiated volume may even allow for administration of an increased dose to the target volume without exceeding the usually accepted tolerance limits of the cord . 
briefly , radiation myelopathy ( rm ) is thought to result from complex dynamic interactions between parenchymal and endothelial cells , their progenitors and the microenvironment within the spinal cord [ 7 , 13 , 23 ]  . 
 among initial reactions , radiation - induced cell killing by apoptosis has been demonstrated [ 4 , 8 , 9 , 18 ] , e.g. , in endothelial cells of the central nervous system ( cns ) of mice as well as in oligodendrocytes . 
further in vitro data suggest that doses leading to apoptosis of oligodendrocytes will also decrease the clonogenic capacity of their o - 2a progenitor cells [ 25 , 27 ]  . 
 even if the cascade of events leading to neurotoxicity is not completely deciphered yet , the end stage is characterized by cell loss , blood vessel hyperpermeability , perivascular edema , demyelination , and necrosis [ 7 , 13 , 23 ]  . 
 insulin - like growth factor - 1 ( igf - 1 ) is an important survival factor for o - 2a progenitor cells and oligodendrocytes in vitro [ 28 ]  . 
 regarding the anti - apoptotic effect of igf - 1 , other possible downstream events include inhibition of caspase - 3 activity via activation of bcl - 2 , inhibition of bax , and the mitogen - activated protein kinase ( mapk / erk ) pathway [ 17 ]  . 
it has been described that igf - 1 crosses the blood - brain barrier ( bbb ) , entering the cns by a saturable transport system , and that a single subcutaneous injection provides sufficient plasma levels for 24 h [ 16 , 22 ]  . 
initial experiments by our group suggested that either of two strategies , i.e. , subcutaneous administration of igf - 1 and intrathecal amifostine treatment , significantly increased the median latent time to rm in previously unirradiated animals but did not change the dose - response relationship [ 12 , 14 ]  . 
 material and methods adult female fisher f - 344 rats ( age 12 weeks , weight 160190 g ) were purchased from sasco inc . , wilmington , ma , usa . 
these facilities are accredited by the american association for accreditation of laboratory animal care and are operated in accordance with standards and laws of the united states department of agriculture , the department of health and human services , and the national institutes of health . 
a single anterior field was treated by use of a cobalt - 60 device ( atomic energy of canada , dose rate approximately 0.5 gy / min , source - skin distance 70 cm )  . 
dose was prescribed to a depth of 1.3 c the experiment started with treating the spinal cord segment with a single dose of 16 gy which does not lead to overt damage ( corresponding to 75% of ed50 in this model )  . 
a control group of 22 rats received an intrathecal saline injection 3060 min before reirradiation , whereas a treatment group of 29 rats received a single intrathecal injection of 0.3 mg amifostine at that time . 
we used a surgical technique for intrathecal injection of amifostine or saline , where a cannula was inserted into the cisterna magna , as described in [ 1 ]  . 
2 days after development of definitive front leg paresis , rats were sacrificed in a co2 chamber and prepared ( formalin fixation , decalcification ) for histopathologic examination of hematoxylin - eosin - stained slides of the complete cns . 
 discussion as shown in our previous experiments , administration of single - agent igf - 1 during radiotherapy significantly delayed the development of rm , alike treatment with amifostine [ 12 , 14 ]  . 
 we decided to test for the first time the combined treatment in a setting of reirradiation , a clinically difficult situation that occurs not infrequently , for example in head - and - neck tumors . 
 to our knowledge , experimental modification of the radiation response of previously irradiated spinal cord by pharmacological agents has not been reported so far [ 19 , 29 , 31 ]  . 
as shown graphically in figures 1a to 1c , igf - 1 and amifostine reduced rm rates ( statistically significant in the 21 - gy group ) , resulting in a slightly increased ed50 . 
igf - 1 and amifostine in spinal cord reirradiation control p = 0.10 igf1 plus amifostine control p = 0.11 igf - 1 plus amifostine 100 90 80 70 60 50 40 30 20 10 90 180 270 360 450 time from reirradiation with 17 gy ( days ) 180 90 time from reirradiation with 19 gy ( days ) 270 360 450 figure 1a abbildung 1a figure 1b abbildung 1b 90 time from reirradiation with 21 gy ( days ) 180 270 360 450 figure 1c abbildung 1c 16 18 20 22 retreatment dose ( gy ) figure 2 . 
actuarial estimates of the risk of radiation myelopathy in pretreated f - 344 rats ( 16 gy , interval 5 months ) treated with a single intrathecal injection of amifostine and subcutaneous injections of igf - 1 or saline together with the second radiation treatment . 
aktuarische darstellung des risikos einer strahlenmyelopathie in vorbehandelten f - 344 - ratten ( 16 gy , intervall 5 monate ) , die mit einer intrathekalen einzeitgabe von amifostin und subkutanen injektionen von igf - 1 oder kochsalzgaben zu einer zweitbestrahlung behandelt wurden . 
however , we think that further experiments should be performed with platelet - derived growth factor ( pdgf ) rather than igf - 1 , because we have now shown that pdgf alone already was able to shift the dose - response curve significantly [ 1 ]  . 
our data , although with limited statistical power , do not support the hypothesis that igf - 1 increases the rate or the growth of radiation - induced tumors , which certainly could have been induced already by the first fraction of radiation and thus were microscopically present when exposed to igf - 1 5 months later . 
igf - 1 and amifostine in spinal cord reirradiation tageous to established tumors that are simultaneously being exposed to radiation needs to be addressed in further studies in order to clarify if an improvement of the therapeutic ratio would be obtained when attempting to protect healthy spinal cord with this strategy . 
fraunholz , anja gerstenhauer , heinz - dietrich bttcher1 background and purpose : as treatment of keloids is mainly a cosmetic indication , the authors investigated , beyond the recurrence rate , the patients satisfaction with the result and its correlation with objective medical findings . 
 patients and methods : 83 keloids of 66 patients had been irradiated after excision by a uniform protocol with 4 5 gy ( strontium - 90 [ 90sr ] surface applicator )  . 
the relief from former keloid - caused symptoms ( therapeutic outcome : p = 0.0005 ; cosmetic outcome : p = 0.0011 ) , the ear as keloid localization ( p = 0.0008 and p = 0.0197 ) , and male gender ( therapeutic outcome : p = 0.0423 ) were significantly associated with higher satisfaction . 
 key words : keloids radiotherapy strontium - 90 subjective assessment side effects strahlenther onkol 2005 ; 181 : 7249 doi 10.1007 / s00066 - 005 - 1411 - x ergebnisse der postoperativen 90sr - radiotherapie bei keloiden im hinblick auf die subjektive bewertung der patienten hintergrund und ziel : da die behandlung von keloiden berwiegend aus kosmetischen grnden erfolgt , wurden ber die rezidivrate hinaus die zufriedenheit der patienten mit dem therapieergebnis und deren korrelation mit objektiven medizinischen befunden untersucht . 
 patienten und methodik : 83 keloide waren bei 66 patienten nach exzision mit einem einheitlichen protokoll bestrahlt worden ( 4 5 gy , strontium - 90 - [ 90sr - ] oberflchenapplikator )  . 
 schlsselwrter : keloide radiotherapie strontium - 90 subjektive bewertung nebenwirkungen 1 department of radiation oncology , johann wolfgang goethe university , frankfurt / main , germany . received : january 5 , 2005 ; accepted : june 23 , 2005 strahlenther onkol 2005 no . 
the intralesional steroid injection for instance with or without cryotherapy and / or compression is quite established but a high patient compliance is required , as the injections can be very painful and have to be given over a long period of time [ 24 , 38 ]  . 
new strategies which have to be further evaluated include the topical use of cyclosporine [ 8 ] , intralesional verapamil [ 25 ] or - interferon [ 14 ] , and 5 - fluorouracil [ 12 , 16 ] or bleomycin [ 11 ] injections . 
the radiation protocols used in the clinical setting include x - ray therapy [ 22 , 35 ] , afterloading brachytherapy with iridium - 192 ( 192ir ) wires [ 10 , 15 ] , electrons from linear accelerator [ 27 , 32 ] , and strontium - 90 - yttrium - 90 ( 90sr - 90y ) contact brachytherapy [ 37 , 41 ]  . 
 although treatment of keloids is mainly a cosmetic indication , the recurrence rate represents the only outcome measurement , and little is known about the subjective assessment of the results by the patients and the factors by which it is influenced . 
based on our experience with a postoperative 90sr contact therapy protocol , we therefore investigated , beyond the recurrence rate , the patients satisfaction and its correlation with objective findings which were ascertained during a special follow - up examination . 
 patients and methods from october 1990 to may 1999 , 66 patients with 83 keloids had been treated by a uniform protocol with 90sr contact brachytherapy at the university hospital in frankfurt / main , germany . 
follow - up data were actualized and specified by generating a questionnaire which was sent to all treated patients and by inviting them to a special follow - up examination . 
15 women ( 63% ) and nine men ( 37% ) with a median age of 30 years ( range 1056 years ) additionally participated in the follow - up examination . 
90sr decays into the therapeutically used 90y which almost exclusively emits - radiation with a minimal invasion depth : the dose at 2 mm tissue depth is , dependent on the area of the source , 2030% of the surface dose and it decreases to 13% in 5 mm tissue depth . 
 questionnaire a 20 - item questionnaire had been developed containing the following categories : case history ( familial disposition , skin type , triggering trauma ) , discomforts and their improvement by therapy , results ( recurrence , skin alterations ) , and satisfaction with therapy and with cosmetic outcome ( subdivided by four gradations )  . 
 keloids recurrences n ( % ) characteristics sex male female localization ear neck sternum trunk extremeties trauma operation injury inflammation spontaneous 7 2 9 4 6 5 ( 25 ) 14 ( 42 ) 4 ( 33 ) 4 ( 40 ) 6 ( 86 ) 4 ( 18 ) 1 ( 50 ) 13 ( 38 ) 1 ( 11 ) 1 ( 25 ) 4 ( 67 ) follow - up examination the local findings were documented focusing on recurrences ( extent , relation to scar ) and radiation side effects . 
they were recorded following the objective criteria of the lent - soma scale for skin ( depigmentation , hyperpigmentation , telangiectasias , redness ) [ 1 ] by using four gradations ( none , mild , middle , severe )  . 
 results recurrences according to the questionnaires 19 of the 53 treated keloids ( 36% ) had relapsed in 18 of the 41 patients ( 44% ; table 2 )  . 
the parameters gender , age , familial disposition , skin type , triggering trauma , and length of keloid had no significant influence on the recurrence rate . discomforts the keloid - associated symptoms had completely resolved after treatment in eleven patients ( 32% ) and had improved in 16 patients ( 47% )  . 
 the skin alterations were slight in 17% , moderate in 33% , and severe in 37% of the patients ( in relapsed keloids the radiation - caused side effects could not be distinguished from recurrence - associated alterations [ 34 ] )  . 
grade 3 toxicity according to the lent - soma gradation ( gross telangiectasias ) was found in six sites : in three of the 19 relapse - free scars ( 16% ) and in three recurrences ( 25% )  . 
among the relapse - free scars the side effects were distributed as follows : hypopigmentation in 63% ( mild : 26% , middle : 26% , severe : 11% ) , telangiectasias in 48% ( 16% for each gradation ) , hyperpigmentation in 42% ( mild : 26% , middle : 11% , severe : 5% ) , and mild redness in 21% . 
 satisfaction with therapy and with cosmetic outcome 29% of the patients were extremely satisfied with the therapeutic outcome , 32% were mainly , and approximately 20% each were little or not at all satisfied . 
this assessment did not correspond with the recurrence status : more patients with recurrence ( 67% ) were very or mainly satisfied with the cosmetic result than patients without relapse ( 39% ; figure 2a )  . 
the high satisfaction with both , therapy ( 91% ; p = 0.0008 ) and cosmetic outcome ( 92% ; p = 0.0197 ) , of patients with keloids localized on the ear was significant ( figure 2b )  . 
among the 24 patients who participated in the examination we could not observe a significant correlation between the satisfaction with therapeutic or cosmetic outcome and the extent of dermal side effects . 
possibly , patients who are disappointed with the treatment outcome ( because of recurrence , increased side effects or unidentified factors ) are exceptionally motivated to express their dissatisfaction by participating in the extra follow - up examination or filling out the questionnaire . 
 ( this for instance happened in one patient who wrongly diagnosed telangiectasias as relapse . ) in addition the recurrence rates reported in the literature are not very meaningful for comparison as has already been criticized : mostly , the term recurrence is not clearly defined , nonstandardized examinations are used , and most studies are based on retrospective evaluation , so that with the sparse follow - up in benign diseases relapses can be unidentified [ 23 , 31 , 34 ]  . 
these critical objections have been confirmed by our data : the retrospective analysis alone would have found a recurrence rate of 13% for our collective , only about one third of the rate which is revealed by the current evaluation . 
as 5% of the recurrences occurred during the 2nd year after treatment , the demand for a follow - up period of at least 2 years can be supported [ 23 ]  . 
 ( in our trial 75% of the patients with a follow - up period of < 2 years had already relapsed , so that they were not excluded from this study . ) in accordance with other studies which described the anterior thorax , a site of high dermal tension , as localization with increased relapses [ 9 , 41 ] , we found an extensive recurrence rate of 86% for keloids localized on the sternuother unfavorable factors which were identified in previous studies , like high middle low not at all satisfied high middle low not at all satisfied figures 1a and 1b . 
they are mentioned mostly without any specification only in a few , mainly retrospective studies : for the different treatment schedules the reported rates range between 0% and 45.6% [ 10 , 15 , 22 , 23 , 28 , 32 , 35 ]  . 
the application of high single doses [ 39 , 40 ] ( 5 gy in our trial ) as well as the use of strontium contact therapy which delivers the multiple dosis on the superficial layers of the dermis ( e.g. , stratum papillare , where telangiectasias develop ) are determinants for causing late side effects of the skin fact , in our evaluation after a median follow - up of approximately 3 years extensive rates of hypopigmentation ( 63% ) , telangiectasias ( 48% ) , and hyperpigmentation ( 42% ) were found in the examined 19 relapse - free scars . 
 patients without recurrence tended to be more satisfied with therapy , but regarding the cosmetic result an adverse effect emerged : more patients with recurrence were extremely or mainly satisfied than patients without relapse . 
instead , the relief from former keloid - caused symptoms as well as the localization of the keloid were significant factors which influenced the satisfaction with both , therapy and cosmetic outcome . 
 ( interestingly , this difference was significant regarding the therapeutic and not the cosmetic outcome . ) in the literature only a few studies investigated the subjective assessment of the results by the patients : in the analysis by maarouf et al . , 83% of the 36 treated patients were satisfied or very satisfied with the cosmetic outcome ; all patients who were dissatisfied with the cosmetic outcome had a recurrence [ 28 ]  . 
reported a high accordance between objective and subjective assessment : they described successful treatment in 83% of 126 treated keloids and also 80% of the patients rated the result as excellent or good [ 20 ]  . 
found that the cosmetic aspect was assessed controversially : women were more interested in a good cosmetic result than the examiner [ 10 ]  . in our evaluation in which the patients satisfaction was investigated in detail , only 61% of the patients were extremely or mainly satisfied with the therapeutic outcome and 51% were extremely or mainly satisfied with the cosmetic outcome . 
 with the reservation of possible negative selection mentioned above , this assessment might be influenced , in addition to the evaluated medical parameters , by individual psychological factors which have not been investigated in this trial ( e.g. , half of the patients had a strong feeling of cosmetic disfigurement by the keloid before treatment )  . 
as we have changed our radiation protocol in the last years by increasingly using after single dose reduction electrons ( four daily fractions of 4 gy ) , it will be interesting to compare the different results in a further evaluation . 
the reporting of the results should therefore not only focus on the recurrence rate : the extent of the radiation side effects and the patients satisfaction with the treatment result have to be considered as well . 
veen1 purpose : to review the recurrence rates of keloids after surgical excision followed by radiotherapy , and to answer the question whether after normalization of the dose , a dose - effect relationship could be derived . 
 key words : keloid recurrence rate radiotherapy brachytherapy linear - quadratic model biologically effective dose overall treatment time strahlenther onkol 2005 ; 181 : 71723 doi 10.1007 / s00066 - 005 - 1407 - 6 biologisch effektive dosierung postoperativer strahlentherapie zur prvention von keloiden : dosis - wirkungs - beziehung ziel : auswertung der rckfallraten von keloiden nach chirurgischer entferung und bestrahlung und die frage , ob sich aus den normalisierten werten der strahlendosis eine dosis - wirkungs - beziehung ableiten lsst . 
ein bed - wert von 30 gy kann beispielsweise mit einer einzelakutdosis von 13 gy , 2 fraktionen von 8 gy oder 3 fraktionen von 6 gy , oder mit einer einzeldosis von 27 gy mit geringer dosisrate erzielt werden . 
 schlsselwrter : keloid rckfallrate strahlentherapie brachytherapie linear - quadratisches modell biologisch effektive dosis gesamtbehandlungszeit 1 department of radiotherapy , university medical center utrecht , the netherlands received : january 5 , 2005 ; accepted : june 10 , 2005 strahlenther onkol 2005 no . 
the scar does not improve with time and , besides its unattractive visual effect , it may cause tingling , burning and itching ( e.g. , [ 3 , 8 , 10 , 20 ] )  . 
keloids belong to the class of hyperproliferative diseases , just as pterygium of the eye , dupuytrens disease , scleredema adultorum buschke and peyronies disease [ 27 , 37 , 47 ]  . 
radiation therapy is applied with superficial kilovolt x - rays , electron beams , telecobalt , and interstitial radiation therapy either at low or high dose rate ; also different overall treatment times ( otts ) are applied . 
a relationship may be found when the doses applied are normalized to the biologically effective dose ( bed ) using the linear - quadratic concept [ 1 , 51 ]  . 
 material and mthods literature search a literature search was conducted in pubmed to identify studies published in 19702004 reporting on treatment of keloids after surgery , using the search terms keloids , surgery , radiation therapy , radiotherapy . 
studies were excluded when the recurrence rate of keloids after surgery and radiation treatment could not be related to a specific radiation dose , the number of cases per dose group was smaller than ten , earlier results were included in a next study , or results were reported to be strongly related to localization of the keloids , but no doses and recurrences were provided per localization . 
 linear - quadratic and biologically effective dose ( lq - bed ) concept the occurrence of a biological effect e depends on the dose in a linear and quadratic fashion : e = n ( d + ( cid : 2 ) d2 ) ( 1 )  . 
 the strength of the lq - bed concept is that for highand low - dose - rate treatments , fractionated or not , the bed values resulting in a specific isoeffect are equal . the value of / ( cid : 2 ) is about 10 gy for acute - reacting tissues , and 14 gy for late - reacting tissues . 
for keloids as an acute - reacting tissue we assumed / ( cid : 2 ) = 10 gy and = 1 h1 . relative biological effectiveness keloids are treated with a diversity of radiation modalities : kilovolt x - rays , strontium 90 ( 90sr ) ( cid : 2 ) - rays , iridium 192 ( 192ir ) - rays , and megavolt electrons . 
x - rays in the kilovoltage range have a larger biological effect per unit dose than cobalt - 60 ( 60co ) - rays or electrons in the megavolt range . 
the relative biological effectiveness ( rbe ) values of x - rays relative to 60co - rays were derived from various reports [ 7 , 41 , 48 , 53 ]  . 
 overall treatment time in most of the studies the ott , i.e. , time period between surgery and last radiation dose , was < 1 week and for these studies a correction for ott in the bed is hardly interesting . 
we will only show the results for accelerated proliferation starting on day 7 after surgery . data handling curve fitting was applied using spss 10.1 for windows with the models for curve estimation . 
 results a number of 31 articles were identified of which 13 were excluded , because no link could be found between recurrence rate and dose given [ 8 , 17 , 19 , 20 , 23 , 24 , 26 , 28 , 34 , 44 ] , the number of cases per dose group was smaller than ten [ 46 ] , earlier results were included in a next study [ 42 ] , or results were reported to be strongly related to localization of the keloids , but no doses and recurrences were provided per localization [ 52 ]  . 
 in table 1 , the references of the articles , the number of keloids treated , recurrence rate of keloids after radiation therapy , the radiation regimen , the ott and the calculated bed values are shown . 
 in several reports [ 35 , 39 , 52 ] it was stated that the recurrence rate of keloids depended on the anatomic site ; less recurrences were found on the face , and more recurrences for keloids on the trunk . 
we therefore selected reports with results of keloids on earlobes , face and neck region ( favorable sites , keloids in no stretch tension areas ) [ 10 , 13 , 22 , 33 , 35 , 36 , 39 , 40 , 43 ] and reports with results of keloids mainly located in stretch tension areas as limbs and trunk ( nonfavorable sites ) [ 9 , 12 , 3840 , 43 , 49 ]  . 
other methods of treatment include intralesial 5 - fluorouracil , pulsed dye laser , compression with silicone sheeting , and radiotherapy [ 3 ]  . with surgery and radiation therapy recurrence rates of 2.861% were reported ( table 1 )  . 
 strahlentherapie und onkologie original article renal dysfunction after total - body irradiation significance of selective renal shielding blocks hiroshi igaki1 , 2 , 3 , katsuyuki karasawa1 , hisashi sakamaki4 , hiroshi saito5 , keiichi nakagawa3 , kuni ohtomo3 , yoshiaki tanaka6 purpose : a retrospective analysis was conducted on the outcome of total - body irradiation ( tbi ) followed by bone marrow transplantation ( bmt ) on leukemia patients . 
 key words : total - body irradiation renal dysfunction leukemia bone marrow transplantation strahlenther onkol 2005 ; 181 : 7048 doi 10.1007 / s00066 - 005 - 1405 - 8 eingeschrnkte nierenfunktion nach ganzkrperbestrahlung : bedeutung selektiver abschirmung der nieren ziel : retrospektive analyse des outcome der ganzkrperbestrahlung ( total body irradiation : tbi ) vor knochenmarktransplantation ( kmt ) bei leukmiepatienten . 
 schlsselwrter : ganzkrperbestrahlung nierenfunktionsstrung leukmie knochenmarktransplantation 1 department of radiation oncology , tokyo metropolitan komagome hospital , tokyo , japan , 2 proton medical research center , university of tsukuba , ibaraki , japan , 3 department of radiology , graduate school of medicine , university of tokyo , tokyo , japan , 4 department of hematology , tokyo metropolitan komagome hospital , tokyo , japan , 5 department of nephrology , tokyo metropolitan komagome hospital , tokyo , japan , 6 department of radiology , nihon university school of medicine , tokyo , japan . received : december 14 , 2004 ; may 13 , 2005 strahlenther onkol 2005 no . 
selective renal shielding for tbi introduction total - body irradiation ( tbi ) is extensively used as a component of the conditioning regimen of bone marrow transplantation ( bmt ) for hematologic malignancies and other malignant or benign diseases [ 8 ]  . 
in those longterm survivors after tbi / bmt , various complications such as cataract , pulmonary fibrosis , veno - occlusive disease , graftversus - host disease ( gvhd ) , and renal dysfunction have been observed . 
it is known that tbi is the principal risk factor for post - bmt renal dysfunction [ 4 , 9 , 21 ] , and renal dysfunction is mainly attributable to radiation nephropathy , which is characterized by the clinical signs of hypertension , edema , anemia , and hematuria , with elevated serum creatinine concentration and decreased glomerular filtration rate [ 2 ]  . 
some institutions have attempted to prevent these complications by reducing the dose to the kidney with customized blocks , but the optimal dose has not been established [ 6 , 10 ]  . 
in this study , we retrospectively analyzed the outcomes of tbi / bmt at our institution , and evaluated the risk of renal dysfunction after tbi with or without the use of selective renal shielding blocks . 
 patients and methods between june 1987 and october 2001 , 109 leukemia patients received tbi at tokyo metropolitan komagome hospital , japan , as a component of the conditioning regimen prior to their bmt . 
in all patients , eyes and lungs were shielded at the time of irradiation only from the anteroposterior portal , so that the absorbed dose was diminished to 7 gy and 8 gy , respectively . 
the follow - up period ranged from 1.9180.1 months with a median of 28.5 months for patients without renal shielding blocks , and 0.336.9 months with a median of 10.7 months for those with shielding blocks . 
among the 53 patients who were dead , 32 were by relapse or disease progression , seven by gvhd , twelve by other treatment - related morbidities , one by late graft rejection , and one by intercurrent disease ( table 3 )  . 
all : acute lymphocytic leukemia ; anll : acute non - lymphocytic leukemia ; bu : busulfan ; ca : cytosine arabinoside ; cml : chronic myelocytic leukemia ; cy : cyclophosphamide ; cya : cyclosporine a ; nhl : non - hodgkins lymphoma . 
 all group renal block renal block ( ) relapse or disease progression gvhd treatment - related morbidity graft rejection intercurrent disease total 7 1 1 4 8 1 1 1999 . 
in our institution tbi was started in 1987 with pulmonary and lens shielding , and renal shielding blocks have been used since march of 100 months after tbi figure 2 . 
selective renal shielding for tbi renal shielding ( + ) renal shielding ( ) renal shielding ( + ) 1 0 renal shielding ( ) p = 0.53 100 0 20 40 60 80 90 100 months after tbi months after tbi figure 3 . 
however , the rate and degree of renal dysfunction were reported to be modified by the use of drugs such as renotoxic antibiotics , chemotherapeutic agents , radioimmunotherapy or cyclosporine a , and the presence of gvhd in clinical settings [ 2 , 5 , 10 , 13 , 21 ]  . 
the dose - fractionation schedules and conditions of other bmt - related treatments in such animal experiments are obviously different from those used in tbi / bmt in clinical practice . 
in our patients who received 12 gy of tbi in six fractions over 3 days , the renal dysfunction - free rates at 2 years were 100% and 78.5% for the patients whose renal doses were 10 gy and 12 gy , respectively . 
morever , when more sensitive indicators were used for the definition of renal dysfunction , i.e. , [ 51cr ] edta clearance , renal plasma flow , or glomerular filtration rate , most patients and animals presented some signs of radiation - induced renal damage [ 1 , 15 , 16 ]  . 
 for the majority of the patients , however , elevations of serum creatinine and / or urea nitrogen levels were observed within 11.5 years after treatment [ 2 , 5 , 16 ] , and the latent periods did not appear to be different among the different renal dose groups under the clinical setting [ 6 , 10 ]  . 
 serum creatinine concentration patients ( n ) > 1.10 mg / dl , 2.00 mg / dl > 2.00 mg / dl , 3.00 mg / dl > 3.00 mg / dl , 5.00 mg / dl > 5.00 mg / dl , 10.0 mg / dl the severity of renal dysfunction was generally mild in the majority of the patients when the endpoint was determined total strahlenther onkol 2005 no . 
as for the lung , the dose exceeding 7.58 gy is associated with an increased in cidence of lethal interstitial pneumonia [ 12 , 14 , 17 , 19 , 22 ]  . 
these results shed a new light on the tbi procedure , and the benefits of using renal shielding blocks are worthy of further exploration with respect both to the quality of life and to the overall survival . 
in addition , further data need to be compiled with respect to the optimal doses to the whole body and to each organ during tbi , not only for treatment - related toxicities but also for overall survival . 
reports that using mri for conformal treatment planning of prostate cancer reduces the delineated clinical target volumes and improves the consistency of target volume definition between different physicians [ 1 , 2 , 68 , 15 ]  . 
studies comparing ctversus mri - derived volumes found that in general , prostate volumes delineated on ct were approximately 1.3 times larger than mri - derived volumes [ 12 ]  . 
 variations in ctv delineation due to different imaging modalities always bring forward one question : which type of imaging depicts the true organ or tumor volume best ? the fact that mri makes the identification of the prostatic edges easier , does not necessarily imply that mri is more correct in representing the actual prostate size . 
presently , modern mri techniques are used for prostate tumor staging and localization . what has repeatedly been shown in other reports and what was also observed in the present article is the fact that prostate delineation based on ct images is particularly difficult at the superior aspect of the prostate and the base of the seminal vesicles . 
perhaps even more important is the inability strahlenther onkol 2005 ; 181 : 7434 doi 10.1007 / s00066 - 005 - 9383 - 4 to correctly define the prostatic apex on ct which is virtually undistinguishable from the structures of the urogenital diaphragsince the apex is reported to be infiltrated by tumor in 7585% , a geometric miss could result in a substantial deterioration of cure rates [ 8 ]  . 
correct identification particularly of the caudal parts of the prostate using mri further leads to improved sparing of the penile bulb with a potentially lower likelihood for persisting impotence [ 12 ]  . 
is the improved discrimination of the anterior rectal wall from the posterior parts of the prostate resulting in a better rectal sparing and potentially reduced toxicities with the use of mri [ 12 ]  . 
concerning prostate tumors , image fusion software appears to be of outstanding value for tumor localization due to the limited soft - tissue contrast in the small pelvis [ 5 ]  . 
the decreased standard deviations of ctvs using mri might have been essentially determined by the fact that all ctv definitions based on the combined use of ct and mri were influenced by the interpretations of the same radiologist . 
of course , the major results of this study have already been reported in similar studies without additional hearings of radiologists , implying that in fact mri plays an important role for accurate and consistent target volume definition [ 7 , 8 ]  . 
 concerning clinical implications , the additional use of mri ( and a radiologist ) in this study leads to a systematic decrease of contoured prostate volumes of 6.54% compared to ct alone . 
there is no general rule how variations from ctv definition contribute to the safety margto estimate their impact on the overall geometric precision in radiotherapy of the prostate is certainly not trivial . 
it should be assumed from the data cited above and the detailed analysis by villeirs et al . , however , that mri is more reliable concerning the visualization of prostate and tumor expansion . 
 [ 3 ] konnte nachgewiesen werden , dass bei patienten mit einer d90post > 140 gy das psa - freie berleben signifikant hher ist als bei patienten , bei denen dieser wert nicht erzielt wurde . 
inzwischen gelang es in unserer arbeitsgruppe , die abdeckung v100post auf > 95% anzuheben bei leicht fallender v150post auf 61% ( unpublizierte daten ) , dies jedoch nach jahrelanger erfahrung mit hunderten von patienten . 
so wurde auch in unserer neuesten datenanalyse besttigt ( nicht publizierte daten ) , dass eine hohe v200post mit der strke der dysurie im langzeitverlauf assoziiert ist ( bei subtiler auswertung der langzeittoxizitt , die in der hier besprochenen arbeit nicht erfolgte )  . 
so zeigen unsere daten eine statistisch signifikante assoziation der rektalen spttoxizitt mit der dosis , die in 1 ml des rektums berschritten wird ( median bei uns 153 gy )  . 
lernkurve mit genderten segmentierungsgewohnheiten zusammenhngt , vor allem wenn man den zeitlichen verlauf von zu groen ct - volumina ( gruppen 1 + 2 ) zu dem schon mal zu kleinen ct - volumen ( in gruppe 3 ) in rechnung stellt . 
 abschlieend mchten wir die in dieser arbeit dargestellte vorgehensweise nicht zur nachahmung empfehlen und unsere kritikpunkte in folgender weise zusammenfassen : ( cid : 127 ) die lernkurve fr die implantationstechnik ( und die postimplantationsanalyse ) ist sicher noch nicht abgeschlossen . 
gegenstand der arbeit war die analyse der prund posttherapeutischen dosimetrischen qualittsindikatoren in der frhphase der anwendung in unserem zentrum und nicht die onkologischen langzeitergebnisse und auch nicht die kurzoder mittelfristigen nebenwirkungen . 
als universitres zentrum sehen wir uns verpflichtet , die probleme whrend der lernphase zu analysieren , weil es einerseits notwendig ist , bei der etablierung einer neuen methode kritisch gegenber den eigenen ergebnissen zu sein und es andererseits auch sinnvoll ist , anderen anwendern , die mit dieser methode beginnen , solche informationen zugnglich zu machen . 
 die autoren kahmann et al . , welche seit 1999 in einer monotherapeutischen einrichtung die permanente interstitielle brachytherapie an einer greren fallzahl angewandt haben , kritisieren zahlreiche aspekte unserer arbeit unter verweis auf eine publizierte analyse der nebenwirkungen in ihrer patientengruppe , die sie mit einem nicht validierten fragebogen erhoben haben [ 7 ] sowie unter mehrfachen hinweisen auf sehr gute eigene , aber unpublizierte daten . 
bei der betrachtung unserer lernkurve ist zu bercksichtigen , dass wir wie angegeben im rahmen der etablierung der methode unsere vorgehensweise mehrfach aufgrund der fortlaufenden analyse der zwischenergebnisse verndert haben . 
zu bercksichtigen ist weiter , dass es strahlenther onkol 2005 ; 181 : 7402 doi 10.1007 / s00066 - 005 - 8337 - 1 sich bei unserer serie , im gegensatz zu vielen anderen , um eine reine monotherapie ohne adjuvante behandlung handelt . 
 bei der bewertung der ergebnisse in den gruppen 1 und 2 unserer serie muss die tatsache bercksichtigt werden , dass bei verwendung von pd - 103 ( patienten 127 unserer serie ) die empfohlene prostataumschlieende dosis bei nur 124 gy liegt . 
kritisieren die in unserer serie nach ihrer ansicht zu niedrige v100post ( 82% fr alle patienten , 88% fr die patienten der gruppe 3 ) und fordern als untergrenze einen wert von 90% . 
 die abbildung 3 unserer verffentlichung demonsriert , dass die konturierung der prostata in der computertomographischen bildgebung nur mit unsicherheit mglich war und in der frhen lernphase wahrscheinlich zu grozgig eingezeichnet wurde . 
die kritik , dass die verbesserten d90 - werte in gruppe 3 durch unzulssig klein konturierte prostatavolumina zu erklren seien dies wird mit dem verhltnis vct / vtrus < 1 begrndet ist nicht stichhaltig . 
 [ 7 ] beschreiben selbst im mittel 10% kleinere volumina im postplan ( vpost ) im vergleich zum ultraschall ( vrealtime ) in ihrer serie , in der nur bei 114 von 174 patienten berhaupt ein postimplantations - ct durchgefhrt wurde . 
v100post zurckzufhren , ist daher spekulativ und bersieht , dass wie in unserer arbeit angegeben insgesamt 12 patienten behandelt wurden , die bezglich prostatagre , tumorstadium oder psa die von der degro und dgu gemeinsam empfohlenen stringenten eingangskriterien [ 6 ] verfehlten . 
dazu kommt zweitens , dass unser zentrum alle kurativen behandlungsmethoden zur therapie des lokalisierten prostatakarzinoms anbietet und durchfhrt , wie es im sinne einer optimalen und unabhngigen patientenberatung auch erforderlich ist . 
drittens sind wir der berzeugung , dass eine zwar nebenwirkungsarme behandlung , wie die permanente interstitielle brachytherapie des prostatakarzinoms sie darstellt , bei der etablierung dennoch sehr kritisch analysiert werden muss , bevor die behandlungszahlen gesteigert werden . 
 unsere darstellung der eigenen lernkurve , die sich mit den publizierten lernkurven anderer arbeitsgruppen vergleichen lsst , stellt in keinster weise eine diskreditierung der behandlungsmethode der permanenten interstitiellen brachytherapie dar . 
11 urban & vogel strahlentherapie und onkologie original article evaluation of hdr interstitial breast implants planned by conventional and optimized ct - based dosimetry systems with respect to dose homogeneity and conformality tibor major , jnos fodor , zoltn takcsi - nagy , pter goston , csaba polgr1 background and purpose : recently , the use of brachytherapy for partial breast irradiation has increased significantly . 
the aim of this study was to make dosimetric comparisons between conventional ( conv ) and ct - based optimized dosimetry systems applied to breast implants . patients and methods : 17 patients treated with high - dose - rate ( hdr ) interstitial brachytherapy were selected for the study . 
to quantify the dose distributions , volume ( v90 , v100 , v150 , v200 ) and dose ( d90 , dmin , mean central dose [ mcd ] ) parameters , along with the dose nonuniformity ratio ( dnr ) , dose homogeneity index ( dhi ) , external volume index ( ei ) and conformal index ( coin ) were used . 
for each implant , three more virtual treatment plans were created using the paris dosimetry system ( pds ) , geometrically optimized system ( gos ) and conformal system ( conf )  . 
to improve the quality of brachytherapy implants , the image - based three - dimensional information should be used not only for dose plan evaluation , but also previously , for planning the geometry of the catheter positions and performing the insertions . key words : breast implants ct - based brachytherapy planning dose homogeneity and conformality strahlenther onkol 2005 ; 181 : 8996 doi 10.1007 / s00066 - 005 - 1350 - 6 dosishomogenitt und dosiskonformitt bei ct - geplanten hdr - implantaten der brust hintergrund und ziel : der einsatz der brachytherapie bei der bestrahlung der brust hat in den letzten jahren deutlich zugenommen . 
ziel dieser studie ist ein vergleich zwischen konventionellen ( conv ) und ct - gesttzten , optimierten dosimetriesystemen . patienten und methodik : fr die studie wurden 17 mit interstitieller high - dose - rate - ( hdr - ) brachytherapie behandelte patientinnen ausgewhlt . 
nach der implantation wurden von allen patientinnen ct - bilder angefertigt , und das zielvolumen ( resektionshhle mit einem sicherheitsabstand von 1 cm ) wurde auf den axialen schichten eingezeichnet . 
zur quantifizierung der dosisverteilungen wurden volumetrische parameter ( v90 , v100 , v150 , v200 ) , dosisparameter ( d90 , dmin , mittlere basale dosis [ mcd ] ) sowie dnr ( dose nonuniformity ratio ) , dhi ( dose homogeneity index ) , ei ( external volume index ) und coin ( conformal index ) ermittelt . 
fr jedes implantat wurden drei weitere virtuelle bestrahlungsplne unter verwendung des pariser dosimetriesystems ( pds ) , des geometrisch optimierten systems ( gos ) und des konformalen systems ( conf ) erstellt . 
dosisund volumenparameter wurden ermittelt und verglichen . 1 radiotherapy department , national institute of oncology , budapest , hungary . received : august 3 , 2004 ; accepted : november 29 , 2004 strahlenther onkol 2005 no . 
dosimetric evaluation of hdr breast implants ergebnisse : die mediane katheterzahl lag bei zehn ( 6 bis 13 ) , die durchschnittliche gre des planungszielvolumens bei 63 , 4 cm3 ( 17 , 7122 cm3 )  . 
um die qualitt brachytherapeutischer implantate zu verbessern , sollten die bildgesttzten dreidimensionalen informationen nicht nur zur dosisspezifikation , sondern auch fr die geometrische planung der katheteranordnung und die implantation verwendet werden . 
 schlsselwrter : brustimplantate ct - gesttzte bestrahlungsplanung dosishomogenitt und dosiskonformitt introduction the use of brachytherapy for partial breast irradiation has increased significantly over the past several years [ 26 , 31 , 34 ]  . 
in selected subgroups of patients with early - stage breast cancer , partial breast irradiation is an alternative to radiotherapy of the whole breast [ 2 , 32 , 45 ]  . advances in technology of brachytherapy equipments and computerized treatment planning systems allow to adapt the reference isodose surface to the shape of the three - dimensional ( 3 - d ) imaging - defined target volume , while reducing exposure to adjacent normal tissues . 
a good implant will be characterized by a good dose coverage of the target volume , a high dose homogeneity inside and a steep dose fall - off outside the target volume . 
to date , there is no consensus about the clinical importance of dose coverage and homogeneity . the most common classic interstitial dosimetry system in europe is the paris dosimetry system ( pds ) [ 6 , 29 ]  . 
originally , the pds was based on low - dose - rate ( ldr ) wire sources , but later its application was extended to the high - dose - rate ( hdr ) technique , where the linear source was simulated by a stepping source with uniform dwell times [ 18 , 39 ]  . 
the technological developments and progress in the planning software have led many clinicians to depart from the classic dosimetry systems , emphasizing that the dosimetry must be conform to the target volume and not to the implant . 
 [ 16 ] , an in - house developed cross - sectional imaging - based planning system is described , which was successfully used for freehand interstitial brachytherapy at different tumor localizations in 42 patients . 
despite the everyday use of the ct - based brachytherapy treatment planning , the rules and concepts of this new planning modality have not been established yet . this paper presents a comparative analysis between the conventional and image - based dosimetry systems applied to planning of hdr breast implants . 
following ct - based 3 - d target volume definition and different dwell time optimizations , dose and volumetric parameters were used to quantify the dose distributions , and comparisons between the various dosimetry systems were made . patients and methods patients and dosimetry systems between may 2003 and june 2004 17 consecutive patients treated with hdr interstitial brachytherapy were selected for the study . 
 for each implant , three other virtual plans were created using the pds , geometrically optimized system ( gos ) and conformal dosimetry system ( conf ) [ 6 , 7 , 25 , 29 , 41 ]  . 
for the gos , the active lengths in the catheters were equal to the target length , while for the conf , the active source positions were kept inside the target volume . 
the dose points were created on the target contour in each slice , and the separation between the points was 5 m dose prescription and plan evaluation at the pds and gos the dose distribution was normalized to the mean central dose ( mcd ) , and the dose was prescribed to 85% , while at the conf and conv the normalization was made to the mean dose in the reference points , and the prescription was made to the 100% isodose line . 
to quantify the dose distributions , volume ( v90 , v100 , v150 , v200 ) and dose ( d90 , dmin , mcd ) parameters , along with the dose nonuniformity ratio ( dnr ) , dose homogeneity index ( dhi ) , external volume index ( ei ) , coverage index ( ci ) and conformal index ( coin ) were used [ 3 , 25 , 36 , 37 , 49 ]  . 
the volume parameters indicate the fraction of the target volume that receives at least the corresponding percentage of the prescribed dose , e.g. , the v100 is the fraction of the ptv receiving 100% of the reference dose or more . 
the dnr is the ratio of volume receiving 1.5 times the reference dose or more , to the volume receiving at least the reference dose [ 36 , 37 ]  . 
 the icru report 58 recommends using the spread between the local minimum doses in the central plane and the ratio of minimum target dose to the mcd as parameters of the dose uniformity for interstitial implants [ 12 ]  . 
the maximal percentage deviations of the individual minimum doses from the mcd ( mcd + / mcd ) and ratio of minimum target dose to the mcd were also calculated . 
however , the v200 was very high for the conf ; almost one third of the target volume received at least the double of the reference dose , and > 50% of the target volume was irradiated by 1.5 times the reference dose , on average . 
in the central plane the most uniform dose distributions developed at the pds and gos , because the spread between the local minimum dose values is lowest for these dosimetry systems . 
the dose distributions were the most inhomogeneous in the central region at the conf , where the maximal positive and negative mean deviations of the local minimum doses from the mcd were 31% and 23% , respectively . 
the coin was highest for the conf ( 0.74 ) and lowest for the pds ( 0.34 ) , indicating that the conformal dose planning results in the most superior dose distributions with respect to conformality . the statistical analysis showed a significant difference ( p < 0.05 ) between conv , pds , gos , and conf for any of the v100 , dnr , dhi , and coin parameters . 
 discussion although 3 - d treatment planning provides radiation oncologists with the tools necessary to improve local control and possibly also the cure rates , the most common planning method in brachytherapy is still based on radiography . 
in traditional interstitial brachytherapy the use of a two - film localization technique allows to reconstruct the catheters / needles ( with the sources ) in three dimensions , but the definition of actual extensions of the target volume is impossible . 
integrating ct imaging into stereotactic interstitial radiotherapy of brain tumors has been successfully applied since the 1980s , and the image - based brachytherapy has regularly been used in the treatment of prostate cancer for many years [ 9 , 24 ]  . 
 [ 28 ] used ct films to determine the volume of the lumpectomy site , the number of implant planes necessary , and the orientation of the implant planes , but treatment planning was still based on orthogonal radiographs . 
 they used the preimplant images to define the positions of the needles , and following the implantation a second set of ct images were taken for comparison of the actual target volume coverage with the virtual implant generated preoperatively . 
in the postimplant ct images the lumpectomy cavity and target volume ( lumpectomy cavity + 1 cm margin ) were outlined , and following the geometric optimization different volumetric and dose parameters were calculated . 
 [ 13 ] performed a retrospective ct - based 3 - d dose - volume analysis of hdr breast implants to evaluate the dose coverage of lumpectomy cavity and target volume . 
they used standard geometric optimization , and in the actual implants of eleven patients the median proportion of the lumpectomy cavity and target volume ( cavity with 1 cm margin ) receiving at least the prescription dose was 85% and 68% , respectively . 
however , in their study only the clip doses and the mean dose on the target surface were used as measures of conformality , and evaluation of anatomic dvhs was not applied . 
van der laarse [ 39 ] recommends that the outer active source positions should be inside the target volume at 0.5 cm from the target surface in the stepping source dosimetry systeperera et al . 
 [ 1 ] used shorter active lengths in geometrically optimized biplane implants than in the nonoptimized implants , but the average active length was still 9% longer than the treatment length . 
when the catheters were placed at 1.5 cm from each other and dose point optimization was used , the optimal active length appeared to be 0.5 cm shorter than the length of the ptv , but at geometric optimization the best conformality occurred when the active length was equal to the target length . 
based on these results , in this study the active source positions were kept inside the target volume at dose point optimization , and the active lengths were equal to the longitudinal dimension of the ptv when geometric optimization was applied . although the quantitative dosimetric measures of implants are used in many publications , their correlation to clinical outcome is still unclarified . 
in another study from the same department , no clear statistical correlation between dose homogeneity and complication risk was found in the dosimetric analysis of the sole hdr brachytherapy treatment for early - stage breast cancer [ 48 ]  . 
in our study , the implants planned with the pds and gos had more homogeneous distributions with a mean dnr of 0.25 , while the use of conv and conf resulted in worse homogeneity . one of the aims of a good interstitial implant is the high dose coverage . 
the reason for the relatively low value is that the needles were placed at the border of the ptv and dwell positions were allowed to extend beyond the target volume . 
in addition to the low dose coverage , the large amount of normal tissue outside the ptv irradiated by the reference dose also contributed to these low values at the conv and pds . 
on average , related to the target volume > 50% normal tissue volume received the reference dose . in this study , most of the patients were treated with a three - plane implant , but in spite of this , the target volume coverage by the catheters was generally insufficient in regions superficial and sometimes deep to the implant . 
at the conf , where the optimization is performed on reference dose points placed on the surface of the ptv , the geographic miss can be compensated , but the dose homogeneity worsens . 
in order to improve both the coverage and homogeneity , more catheters have to be implanted , and their positions must conform better to the shape of the target volume . 
for this , preimplant 3 - d imaging is necessary on the lumpectomy cavity and patient anatomy , and the implant has to be performed according to this 3 - d information . 
to obtain better brachytherapy implants , the image - based 3 - d information should be used not only for postimplant dose plan evaluation , but also for planning the geometry of the catheter positions and performing the insertions . 
dudley werner1 , gerd schmitt2 , 3 , clare stannard1 , 3 , anne gudgeon1 , jennifer wilson3 , shaheeda fredericks1 , 3 , elene mcevoy1 , elizabeth nel1 , alistair hunter1 , jacobus p . 
slabbert3 , gerald langman4 background and purpose : by virtue of their high linear energy transfer ( let ) characteristics the biologic effectiveness of neutrons is less dependent on tissue oxygenation tension and cell cycle phase as compared to that with photons . 
since a short course of radiotherapy is required for clinical reasons , it prompted the authors to initiate a randomly controlled trial on locally advanced breast cancer . patients and methods : between 1996 and 1999 , 27 patients with locally advanced breast cancer were irradiated with photons ( 60 gy , 30 fractions ; 8 mv , 60co ) or neutrons ( 18 gy , twelve fractions ; 66 mevp ( cid : 1 ) be )  . 
the mean tumor diameters were 699 399 ml for the photon group and 1 , 097 831 ml in the neutron group . results : after a mean follow - up period of 21.5 months tumor involution was evaluated in 22 patients . 
with regard to tumor control and late radiation morbidity no differences between the two treatment arms were observed . conclusion : the underlying data indicate that no benefit is to be expected from neutron therapy in breast cancer . key words : breast cancer neutron therapy strahlenther onkol 2005 ; 181 : 7781 doi 10.1007 / s00066 - 005 - 1298 - 6 neutronenversus photonentherapie zur lokalen kontrolle inoperabler mammakarzinome hintergrund und ziel : die biologische wirkung von neutronen beruht im wesentlichen auf der geringeren abhngigkeit von der sauerstoffkonzentration und der zellzyklusphase im vergleich zu dnn ionisierender strahlung . 
dies veranlasste die autoren , eine kontrollierte , randomisierte studie bei lokal fortgeschrittenen mammakarzinomen durchzufhren . patienten und methodik : zwischen 1996 und 1999 wurden 27 patientinnen mit lokal fortgeschrittenen mammakarzinomen mit photonen ( 60 gy , 30 fraktionen ; 8 mv , 60co ) oder neutronen ( 18 gy , zwlf fraktionen ; 66 mevp ( cid : 1 ) be ) bestrahlt . 
die mittleren tumorvolumina betrugen 699 399 ml in der photonengruppe und 1 097 831 ml in der neutronengruppe . ergebnisse : nach einer mittleren nachbeobachtungszeit von 21 , 5 monaten waren die ergebnisse von 22 patientinnen auswertbar . 
 schlsselwrter : mammakarzinom neutronentherapie 1 radiation oncology department , groote schuur hospital and university of cape town , cape town , south africa , 2 department of radiation oncology , university of duesseldorf , germany , 3 nac / ithemba labs , faure , south africa , 4 department of anatomical pathology , university of cape town , cape town , south africa . received : march 11 , 2004 ; resubmitted : april 8 , 2004 ; accepted : july 28 , 2004 strahlenther onkol 2005 no . 
neutron therapy in breast cancer introduction despite remarkable progress in systemic treatment of breast cancer , no optimal treatment for patients with locally advanced tumor that is either inoperable after systemic treatment or is seen in a patient unsuitable for systemic treatment has been reported . 
in countries with limited resources , such as south africa , breast cancer is often diagnosed late [ 9 , 21 ] ; so the treatment of inoperable , advanced local disease is of particular relevance . 
promising results have previously been reported in the treatment of this condition with neutron therapy [ 57 , 26 ] , although the value remains controversial [ 13 ]  . 
 while cells in mitosis and g2 - phase are considerably more sensitive to photons than those in late s - phase [ 30 ] , there is less variation in sensitivity to neutrons for cells in different phases of the cell cycle [ 34 ]  . 
also , as neutron irradiation has an oxygen enhancement ratio ( oer ) of about 1.6 and is less dependent on oxygen than photon irradiation , hypoxic tumor cells may be less radioresistant to neutrons [ 29 ]  . 
since these factors are less important for neutrons and neutrons exhibit less sublethal [ 12 ] and potentially lethal damage repair [ 11 , 23 ] , neutron fractionation is apparently more flexible . 
typically , rbes ( relative biological effectiveness ) for neutrons are between 2 and 5 , varying with factors such as dose , endpoint and neutron energy [ 33 ]  . 
using human cancer cells with different radiosensitivities the neutron beam used in the clinical trial reported here has indeed shown to have the potential for therapeutic gain [ 24 ] although it may be somewhat less than that of older - generation lower - energy neutron sources [ 25 ]  . 
since almost half of all locally advanced breast tumors are thought to contain hypoxic cells [ 32 ] , a sizable proportion of these tumors will have a substantable 1 . 
neutron therapy in breast cancer tially higher rbe than that of normal aerated tissue and thus may benefit from neutron therapy , especially those that are well differentiated and slowly growing . a potential further advantage of neutron therapy in rapidly dividing tumors is that treatment may be able to be delivered over a shorter period and thus counteract repopulation [ 16 , 31 ]  . 
 we had first performed a dose - finding study for neutrons [ 27 ] and then set out to compare the efficacy of 18 gy neutrons and 60 gy photons in locally advanced breast cancer with or without metastases . 
 photon therapy was prescribed to a total dose of 60 gy in 30 fractions given five times per week , using either 8 - mv photons or 60co - rays . 
neutrons with a mean energy of ~27 mev were generated with 66 - mev protons on berylliuthe prescribed dose was 18 ngy in twelve fractions given three times per week . 
doses of 6580 gy have been found to be necessary in stage iii disease [ 20 ] , and control rates of 1364% have been reported [ 10 ]  . 
although a dose - response relationship has been shown in the irradiation of breast cancer [ 1 , 14 ] , tumor size has been reported as an independent factor for local control [ 2 , 8 , 10 ]  . 
as the tumors treated in this study eligible for assessment had a mean volume of 692 cm3 and a mean diameter of 12.8 cm , there was a relatively high risk of complications . 
 much better response rates than that of 6 / 12 ( cr [ complete remission ] + pr [ partial remission ] ) in this study have been reported for neutron therapy of breast cancer [ 13 , 17 ]  . 
in our neutron group the mean tumor volume was 1 , 097 cm3 and mean diameter 12.8 c both beam quality and doses have varied in these studies , making comparisons difficult . 
 the effect of local tumor control must be weighed up against the complications from high doses , particularly in patients with metastases or huge ulcerating and fungating inoperable tumors where irradiation is aimed at palliation , not cure . 
the study was also stopped early due to the difficulty of accruing , treating and following up patients from poor socioeconomic circumstances who cannot afford to visit treatment centers regularly . 
jansen10 , luciano ditri11 , peter sminia12 , the european intergovernmental framework cost ( european co - operation in the field of science and technology research ) , cost b14 working group oncology background : hyperbaric oxygen ( hbo ) therapy is the inhalation of 100% oxygen at a pressure of at least 1.5 atmospheres absolute ( 150 kpa )  . 
it uses oxygen as a drug by dissolving it in the plasma and delivering it to the tissues independent of hemoglob for a variety of organ systems , hbo is known to promote new vessel growth into areas with reduced oxygen tension due to poor vascularity , and therewith promotes wound healing and recovery of radiation - injured tissue . 
furthermore , tumors may be sensitized to irradiation by raising intratumoral oxygen tensions . methods : a network of hyperbaric facilities exists in europe , and a number of clinical studies are ongoing . 
andererseits kann sauerstoff unter hyperbaren bedingungen whrend oder kurz vor der strahlentherapie verabreicht durch erhhung der intratumoralen sauerstoffspannung als radiosensitizer eingesetzt werden . methodik : in europa existiert ein netzwerk von druckkammern , an denen klinische studien laufen . 
 1 department of radiation oncology , medical university of graz , austria , 2 hyperbaric unit , whipps cross hospital , leytonstone , london , united kingdom , 3 department of surgery , academic medical center , amsterdam , the netherlands , 4 foundation for hyperbaric medicine , basel , switzerland , 5 department of otolaryngology , head and neck surgery , sahlgrenska university hospital , gteborg , sweden , 6 institute of maritime and tropical medicine , national center of hyperbaric medicine , gdynia , poland , 7 hyperbaric & diving medical center , elisha / rambam hospitals , haifa , israel , 8 klinik fr strahlentherapie , radioonkologie und nuklearmedizin , rotenburg / wmme , germany , 9 department of radiation oncology , marien - hospital , duesseldorf , germany , 10 antesi - og operationsklinikken , hovedortocentret , rigshospitalet , copenhagen , denmark , 11 hyperbaric centre oti mediacale vicenza , torri di quartesolo , vicenza , italy , 12 division of radiobiology , department of radiation oncology , vu university medical center , amsterdam , the netherlands . 
schlsselwrter : hyperbare sauerstofftherapie radiogene sptfolgen strahlensensibilisierung strahlentherapie klinische protokolle introduction hyperbaric oxygen therapy hyperbaric oxygen ( hbo ) therapy is the inhalation of 100% oxygen at elevated pressure > 1.5 atmospheres absolute ( ata ; 150 kpa ) , typically 23 ata ( 200300 kpa )  . 
the hyperbaric chamber is the medical tool that provides those conditions to apply very high doses of oxygen in amounts that cannot be reached by any other means . during hbo , oxygen is dissolved physically in the blood plasma . 
at an ambient pressure of 2.8 ata , the amount of plasma - dissolved oxygen is approximately 6 vol.% , equivalent to basic oxygen metabolic needs , and the pao2 in the arteries can reach 2 , 000 mmhg . 
the physiological effects of hbo include short - term effects like vasoconstriction and enhanced oxygen delivery , reduction of edema , and phagocytosis activation , and it has an anti - inflammatory effect [ 25 , 71 ]  . 
for irradiation sensitization it is aimed for euoxic conditions , which may persist for some time after leaving the pressure chamber , even if the high level oxygenation has been exhaled . hbo in radiation oncology was discussed at the estro ( european society for therapeutic radiology and oncology ) echm ( european committee for hyperbaric medicine ) consensus meeting in lisbon 2001 [ 46 ]  . 
the aim of the present project is to obtain clinical data that meet this evidence . the hyperbaric treatment each patient is examined by the hyperbaric physician regarding their suitability for the treatment . 
before hbo treatment patients may have spirometry and a chest x - ray , to exclude severe lung disease , and an investigation by the ear - nose - throat ( ent ) specialist confirming their ability to equalize pressures in the middle ear . 
 absolute contraindications untreated pneumothorax simultaneous administration of doxorubicin bleomycin disulfiram cisplatinum mafenide acetate previous administration of bleomycin relative contraindications claustrophobia seizure disorders pyrexia ( severe ) upper respiratory tract infections chronic sinusitis chronic lung disease with co2 retention history of spontaneous pneumothorax history of thoracic surgery asymptomatic pulmonary lesions on chest x - ray history of surgery for otosclerosis history of optic neuritis viral infections congenital spherocytosis pregnancy strahlenther onkol 2005 no . 
die atmosphre in der kammer besteht aus lu sauerstoffaufnahme erfolgt ber ein maskensyste trained staff members , taking care that the chamber is pressurized or depressurized within the safety limits . 
it is estimated that about 500 patients a year are treated in european hyperbaric facilities for radiation - induced injuries , the majority with disease in the head and neck . 
although hbo treatment is limited to dedicated centers , its use might contribute to cost reduction in the care of long - term survivors of malignancy . hyperbaric oxygen and tumor induction and recurrence feldmeier et al . 
a large number of studies ( mostly controlled ) including > 3 , 000 patients enrolled in trials designed to investigate hbo as a radiosensitizer demonstrated either a neutral or cancer - inhibitory effect . hyperbaric oxygen and radiotherapy regarding the combination of hbo and radiotherapy , we are faced with two applications in clinical practice : ( 1 ) hbo as radiosensitizer : hyperbaric oxygen is then applied simultaneously with or prior to irradiation with the aim of sensitizing hypoxic tumor cells and thereby increasing tumor cure probability ; ( 2 ) hbo as therapeutic agent : once late radiation - induced normal tissue side effects have become manifest , hbo is used to dissolve or reduce the severity of symptoms [ 1 , 3 , 4 , 6 , 812 , 15 , 1724 , 2629 , 33 , 42 , 4649 , 51 , 52 , 5459 , 6266 , 72 , 73 , 75 , 7779 , 82 , 83 ]  . hyperbaric oxygen as radiosensitizer most tumors contain nutrientand oxygen - deprived compartments . 
hbo therapy is an effective approach to cope with the phenomenon of hypoxia by increasing the oxygen load of the tumor [ 2 , 5 , 34 , 41 ] , and therewith to enhance the response to irradiation [ 7 , 34 , 60 ]  . 
however , in the radiation and hbo treatment arm of the study , doses per fraction up to 7 gy were used in pelvic irradiation whereas the control radiation treatment arm consisted of standard fractionation . 
a second mrc trial of hbo and radiotherapy for bladder carcinoma showed hbo not to be better than misonidazole additional to radiotherapy , while carbogen inhalation resulted in a significantly increased bladder tumor local control and overall survival [ 36 ]  . 
a meta - analysis of randomized clinical trials of radiotherapy with any hypoxic cell modifier including hbo [ 61 ] demonstrated that , in particular in carcinoma of the head and neck , significant improvement of overall survival and local tumor control could be obtained . 
with regard to brain tumor treatment , recent japanese data showed the feasibility of a treatment setup with hbo applied prior to radiotherapy [ 4 , 43 , 60 ] ( table 3 )  . 
the two radiosensitization treatment protocols presented here allow a time interval between hbo and subsequent irradiation of 1020 min . hyperbaric oxygen as therapeutic modality for radiation sequelae the goal of radiation treatment is to eradicate tumors with minimal , if any , adverse effects on normal tissue [ 69 , 80 ]  . 
in a number of tissues , an early wave of damage ( weeks or months after exposure ) may be followed by a later wave of injury ( months or years after exposure )  . 
 late effects are often considered irreversible and may lead to severe , even life - threatening , complications after therapeutic use of irradiation [ 39 , 44 , 70 , 81 ]  . 
hbo seems to be able to overcome progressive loss of the microvasculature resulting in chronic tissue hypoxia present in radiation - induced changes ; repetitive hbo sessions gradually induce regrowth of connective tissue , and thereby of capillaries and epithelium [ 37 , 38 , 40 ]  . 
the following organ - specific summary gives a short overview on experiences with hbo in the management of radiation - induced normal tissue side effects . radionecrosis of the mandible and improvement of osseointegration in previously irradiated tissues . 
hbo therapy for radiation - damaged tissues was introduced in 1973 by two principal studies [ 29 , 49 ] and since then , numerous studies have attested to the value of hbo for the treatment of osteoradionecrosis of different bone tissues [ 2629 , 51 ]  . 
a randomized , prospective clinical trial using hbo and penicillin in previously irradiated jaws demonstrated that hbo significantly reduced the development of osteoradionecrosis after tooth removal [ 54 ]  . 
the authors also discussed that hbo may prevent from development of osteoradionecrosis by pressure from tissue - borne appliances , periodontal surgery , endodontic instrumentation , mucosal grafts , skin grafts and secondary excisional biopsies . 
 the value of hbo has also been demonstrated in the management of radiation - induced injury of the nose , floor of the mouth and temporal bone [ 15 , 45 ]  . hbo therapy produces sufficient oxygen partial pressures in poorly perfused tissues to allow fibroblastic activity and collagen production , creating a matrix for capillary budding and neovascularization . 
the daily elevation of oxygen tension in hypoxic bone and soft tissues results in the ingrowth of capillaries [ 38 ] , fibroblastic proliferation and collagen synthesis [ 37 ] and capillary angiogenesis [ 40 ]  . 
 [ 54 ] it was shown that hbo - induced angiogenesis became measurable after eight hbo sessions , rapidly progressed to a plateau at 8085% of nonirradiated tissue vascularity by 20 sessions and remained at that level without further improvement with additional hbo . 
 [ 21 ] reported , that signs and symptoms of radionecrosis were dramatically ameliorated in seven of eight patients , while one patient , despite subjective improvement , eventually required strahlenther onkol 2005 no . 
five patients failed to have a good response , however ; one of them presented with local recurrence , three had significant concurrent medical problems , and one patient had received an insufficient number of hbo sessions . radiation - induced pelvic late effects and radiation - induced proctitis [ 3 , 9 , 20 , 24 , 42 , 56 , 73 , 75 , 79 , 82 , 83 ]  . 
 [ 79 ] obtained healing of vaginal necrosis in 13 out of 14 patients as well as feldmeier & hampson [ 17 ] , who reported encouraging results , particularly in patients who had received a sufficient number of hbo sessions . 
the reason might be the induction of neovascularization prior to the formation of firm connective tissue and reepithelization . radiation - induced cystitis [ 6 , 11 , 12 , 47 , 5557 , 59 , 62 , 65 , 72 , 77 ]  . 
as observed , hbo should not be delayed too long , as in case of extensive bladder shrinkage significant improvement of symptoms seems hard to achieve [ 56 ]  . late radiation sequelae to the breast [ 8 , 19 , 23 , 33 , 64 , 69 ]  . 
 table 6 shows five papers dealing with late sequelae of breast cancer radiotherapy encompassing late effects like breast and arm lymphedema , brachial plexopathy as well as soft - tissue and bone necrosis of the chest wall . 
a statistically significant reduction of lymphedema was also reported by two other trials , one prospective observation and one retrospective analysis published recently [ 8 , 23 ]  . see schmutz [ 66 ] and feldmeier & hampson [ 17 ] for a comprehensive review of the literature . 
the main goal of the working group is preparation as well as actual implementation and follow - up of european clinical randomized studies in the field of hbo and radiation oncology . 
the activities of the working group include : ( 1 ) elaboration , adoption and approval of protocols ; ( 2 ) implementation and follow - up of protocols ; ( 3 ) advisory board for studies on hbo in oncology ; ( 4 ) actively providing information on hbo to radiation oncologists ; ( 5 ) bibliography . 
 clinical protocols with hyperbaric oxygen as radiosensitizer reirradiation of recurrent squamous cell carcinoma of the head and neck after hbo sensitization the objective of the study is to evaluate whether hbo enhances tumor radiosensitivity in patients with previously irradiated histologically proven recurrent head and neck cancers , using a conventionally fractionated treatment schedule . 
 endpoints of the study include : tumor recurrence rate and disease - free survival , overall survival , early and late normal tissue morbidity . role of hbo in enhancing radiosensitivity on glioblastoma multiforme : a clinical study the objective of the study is to evaluate the efficacy of hbo on median survival when applied in combination with conventionally fractionated radiotherapy . 
this treatment setup is based on the japanese studies listed in table 3 . clinical protocols for hyperbaric oxygen therapy of radiation sequelae two protocols , implemented and supported by the working group , are focused on the effectiveness of hbo as therapeutic modality in previously irradiated patients . according to the osseointegration principle , implants of titanium can be installed in the skeleton and used to anchor fixed dental bridges or prostheses intraor extraorally . 
the survival of the implants is depending on several factors including type and design of the implant , the surgical technique , the host bone , pharmacological and physiological affects . 
the objectives of the study are to establish whether ( 1 ) osseointegrated implant failure rates are higher in previously irradiated tissues , and ( 2 ) hbo can be used to reduce implant failure rates in irradiated tissues . 
all centers working with rehabilitation of former cancer patients using the osseointegration concept are cordially invited to participate in this multicenter study . the role of hbo in the treatment of late irradiation sequelae in the pelvic region this is a prospective randomized controlled clinical cross - over multicenter study . 
the objective of this study is to evaluate the extent to which hbo plays a role in the treatment of symptoms due to late radiation injuries induced by curative pelvic radiotherapy for malignancies . 
at the onset of the hbo treatment and during follow - up , organ - related parameters are to be assessed using the eortc grading system , as well as other parameters ( applying to all patients ) such as health - related quality of life as scored in the sf - 36 questionnaire . conclusion randomized clinical studies on hbo and radiation oncology are initiated and supported by the working group oncology of the cost b14 action hyperbaric oxygen therapy . 
the final outcome of the clinical studies will provide data on the efficacy of hbo therapy of late radiation injuries and on the therapeutic efficacy of hbo used as radiosensitizer . 
hbo and radiotherapy strahlentherapie und onkologie aktuelles forum die verlngerung der wartezeit oder der gesamtbehandlungszeit durch ungeplante bestrahlungspausen klinische bedeutung der kompensation thomas herrmann , michael baumann1 hintergrund und ziel : die durch fraktionierte strahlentherapie erreichbare lokale kontrolle von tumorerkrankungen wird nicht nur durch gesamtdosis , dosis pro fraktion und strahlenphysikalische parameter beeinflusst , sondern auch durch den zeitraum , der zwischen einer eventuellen operation und bestrahlungsbeginn vergeht , sowie aus strahlenbiologischen grnden durch die gesamtbehandlungszeit einer fraktionierten strahlenbehandlung . 
 schlsselwrter : strahlentherapie wartezeit gesamtbehandlungszeit lokale kontrolle pausenausgleich strahlenther onkol 2005 ; 181 : 6576 doi 10.1007 / s00066 - 005 - 1331 - 9 protraction of waiting time or overall treatment time by unplanned gaps . 
clinical importance of compensation background and purpose : local tumor control after radiotherapy does not only depend on total dose , dose per fraction and physical parameters but also on the time interval between surgery and begin of radiotherapy and on overall time of fractionated irradiation . 
this study summarizes the evidence for an impact of delay and overall time of radiotherapy on locoregional tumor control . methods : published reports of the last 30 years were reviewed for evidence of a time factor , i.e. , for an influence of overall treatment time on local tumor control . 
overall , 33 nonrandomized studies and twelve randomized trials addressing this question were identified . results : prolongation of waiting time between surgery and radiotherapy , dependent on tumor type and residual burden , decreases local control . 
almost all nonrandomized and randomized trials indicate that prolongation of overall time of fractionated irradiation decreases local tumor control , particularly of squamous cell carcinoma of the head and neck and cervix , but also of non - small cell and small cell lung cancer . 
klinische bedeutung der kompensation ungeplanter bestrahlungspausen conclusion : prescription of radiotherapy may not be limited to total dose and dose per fraction , but needs to include the parameter overall treatment time . 
unscheduled treatment interruptions such as holidays , machine breakdown or patient - related factors , leading to protraction of the overall treatment time , decrease the chance of cure for the patient . 
therefore , unplanned gaps need to be compensated by appropriate measures such as additional fractions at weekends or by applications of a second fraction per day . key words : radiotherapy waiting time overall treatment time local tumor control compensation of unscheduled gaps einleitung seit etwa 25 jahren ist bekannt , dass die gesamtdauer einer strahlenbehandlung die lokale kontrolle eines bestrahlten tumors beeinflusst . 
hatte bis mitte der 70er jahre des letzten jahrhunderts vor allem die verbesserung der technischen mglichkeiten der strahlenbehandlung mit dem bergang von kobaltgerten auf linearbeschleuniger die radioonkologen beschftigt , so begann um 1980 das interesse an fraktionierungsrhythmen einer strahlenbehandlung generell und damit auch an der gesamtbehandlungszeit unter den strahlentherapeuten zuzunehmen . 
 [ 75 ] fanden 1980 bei 468 zwischen 1964 und 1976 behandelten kopf - hals - tumoren mit einer geplanten behandlungspause ( 214 patienten ) von 1416 tagen eine schlechtere lokale kontrolle sowohl im primrtumorals auch im halslymphknotenbereich . 
gleiches lsst sich auch an kleinen klinischen serien ( von rottkay [ 83 ] am sophaguskarzinom und vikram [ 97 ] ) nachweisen , in denen aufgefallen war , dass eine verlngerung der gesamtbehandlungszeit zu einem bemerkenswerten anstieg der rezidivhufigkeit fhrte . 
dabei wurden sechs fraktionen von 1 , 71 , 8 gy pro woche verabfolgt und in der split - course - gruppe eine 2bis 3 - wchige pause zur kompensation der akutreaktionen etwa in der mitte der serie eingelegt . 
aus diesen studien wurde die logische konsequenz gezogen , dass eine krzere behandlungszeit bessere lokale erfolge erwarten lsst , was dann letztendlich auch im mount - vernon - hospital , grobritannien , zur entwicklung eines ultrakurzen protokolls ( chart [ 85 ] ) fhrte . 
 [ 78 ] formulierten 1988 vorsichtig , dass ein kontinuierliches behandlungsregime sofern der patient es toleriert hinsichtlich des therapeutischen erfolgs sicherer als eine split - course - therapie mit gleicher dosis oder dauer ist . 
 [ 100 ] aus dem jahre 1988 zum thema repopulation wurde dann ein dosisinkrement von 0 , 6 gy / tag als ausgleich fr eine behandlungsverlngerung postuliert [ 44 ] , und fowler & lindstrom [ 36 ] fassten 1992 den kenntnisstand von immerhin schon zwlf untersuchungen bei kopf - hals - tumoren zusammen , in denen ausnahmslos ein verlust an lokaler kontrolle bei der behandlungszeitverlngerung zu beobachten war , der im mittel 14% bei verlngerung um 1 woche und 26% bei verlngerung um 2 wochen betrug . 
dennoch bleibt festzustellen , dass es sptestens seit 1990 deutliche anhaltspunkte dafr gibt , dass bei bestimmten tumormanifestationen und - histologien die gesamtbehandlungszeit einen wesentlichen einfluss auf die lokale tumorkontrollwahrscheinlichkeit hat . 
somit stellt nicht nur die fraktionsund gesamtdosis , sondern auch die gesamtbehandlungszeit eine vom strahlentherapeuten zu verordnende und dann auch einzuhaltende gre dar , deren nichtbercksichtigung fr den patienten schwere nachteile nach sich ziehen kann . 
 diese arbeit soll den aktuellen kenntnisstand ber den zeiteinfluss bei bestimmten tumorentitten zusammenfassen , auf die zwei wichtigen , vom radioonkologen beeinflussbaren zeitabschnitte wartezeit und gesamtbehandlungszeit eingehen und mglichkeiten zur kompensation von bestrahlungspausen aufzeigen . 
aufgrund der differierenden tumorbiologie liegt es nahe anzunehmen , dass dieser einfluss sich sehr unterschiedlich auswirkt , je nachdem ob es sich um schnell wachsende , langsam wachsende , schnell fernmetastasen bildende oder zuerst lokoregional metastasierende tumoren handelt . 
 [ 1 ] bei 195 patienten , dass bei einer wartezeit auf die strahlentherapie von > 6 wochen die lokale kontrolle sich grenzwertig ( p = 0 , 06 ) verschlechtert und im krankheitsspezifischen berleben eine signifikante reduktion durch diese verzgerung eintritt . 
 [ 2 ] fanden bei patienten mit plattenepithelkarzinomen der kopf - hals - region , die mit einer konventionell fraktionierten postoperativen strahlentherapie behandelt wurden , eine signifikante verschlechterung der lokalen tumorkontrolle und des berlebens mit zunehmender wartezeit vor der strahlentherapie . 
 [ 34 ] untersuchten frhe kopf - hals - tumoren ( 623 patienten mit stadien t1t2 n0n1 ) und bildeten drei gruppen unterschiedlicher behandlungszeitverzgerung ( < 30 tage , 3040 tage , > 40 tage )  . 
 orourke & edwards [ 72 ] beurteilten im jahr 2000 bei 29 unbehandelten nichtkleinzelligen lungenkarzinomen die durch eine mittlere therapieverzgerung von 54 tagen ( zeitpunkt zwischen diagnostischem und planungs - ct ) ausgelsten konsequenzen . 
die autoren , die die wartezeiten zwischen 18 und 161 tagen bei ihren patienten der nicht ausreichenden bereitstellung von bestrahlungstechnik in grobritannien anlasten , schlussfolgern zusammen mit ash [ 3 ] , dass diese fr das bronchialkarzinom gemachte feststellung auch fr kopf - halsund fr gynkologische tumoren gelten drfte . 
dische [ 23 ] postulierte in seinem editorial zu diesem artikel , dass eine frhere strahlentherapie beim bronchialkarzinom die ergebnisse um 510% verbessern drfte , eine zwar nur geringe prognoseverbesserung , aber im verhltnis zum sonstigen therapeutischen aufwand bei diesem tumor doch relativ leicht zu realisierende manahme , um eine signifikante steigerung von heilungsergebnissen in der krebstherapie von lungentumoren zu erreichen . 
das joint council for clinical oncology [ 52 ] hat 1993 in einem dokument ( reducing delays in cancer treatment ) im sinne einer good practice maximal 4 wochen wartezeit bis zum bestrahlungsbeginn empfohlen . 
allerdings musste fr england nach einem national audit im jahre 1998 die realisierung dieser forderung nochmals unterstrichen werden offensichtlich weil sie bei ungengender gertebereitstellung mit linearbeschleunigern nicht erreicht werden konnte . ein erneutes nationales audit 2002 [ 21 ] zeigte erstaunliche ergebnisse beim zervixkarzinom an 62 radioonkologischen zentren in england . 
whrend offensichtlich aufgrund der gewachsenen kenntnis ber die bedeutung der behandlungszeit bei diesem tumor die gesamtbehandlungszeit von 49 tagen ( 1996 ) signifikant auf 39 tage ( 2001 ) zurckging und 94% aller patientinnen ohne pausen in ihrer behandlungsserie bestrahlt wurden ( 1996 nur 22% ! ) , kam es zu einem anstieg der wartezeit von 14 tagen im jahr 1996 auf 35 tage im jahr 2001 . 
 [ 5 ] demonstrieren , dass nicht nur die gesamtbehandlungszeit ( s.u. ) , sondern auch die zeit zwischen operation und strahlentherapieende ( grenze 10 wochen ) in einer multivariaten analyse signifikante bedeutung fr die lokoregionale tumorkontrolle und das berleben hat , dass also der abstand zwischen operation und bestrahlungsbestrahlenther onkol 2005 no . 
eine untersuchung aus jngster zeit bei 482 patienten mit kleinen mammakarzinomen zeigte in einer multivariaten analyse einen geringen ( 1% zunahme von lokalrezidiven pro monat behandlungsverzgerung ) , aber nachweisbaren effekt [ 12 ]  . hnliche ergebnisse sind auch aus verschiedenen weiteren nachuntersuchungen beim mammakarzinom nach brusterhaltender operation bekannt . 
es muss allerdings bercksichtigt werden , dass einerseits die verbliebene resttumormenge ( r1 , r2 [ 89 ] ) , andererseits aber auch die tumorspezifische neigung zur fernmetastasierung fr die beurteilung eines einflusses des intervalls zwischen operation und bestrahlung auf die heilungsergebnisse bercksichtigt werden muss . 
unabhngig davon , ob dieses ergebnis durch tumorspezifische faktoren wie fernmetastasierungsrate , tumorwachstumsgeschwindigkeit und sonstige populationskinetische parameter beeinflusst wird , gilt fr den radioonkologen die grundregel , dass da er diese faktoren im einzelfall nicht kennt und auch in absehbarer zeit nicht kennen wird ein frher behandlungsbeginn grundstzlich anzustreben ist , sofern nicht sonstige faktoren ( reparative prozesse nach einer operation [ 101 ] ) oder andere den patienten betreffende faktoren dem entgegenstehen . 
 eine verzgerung des behandlungsbeginns , sei es aus organisatorischen grnden oder aufgrund ungengender personeller oder materieller ressourcen , ist im sinne der tumorheilung in jedem fall negativ einzustufen und fhrt zu einer verschlechterung der ergebnisse der strahlentherapie . der einfluss einer verlngerung der gesamtbehandlungszeit alle wichtigen arbeiten , die sich um die erforschung und quantifizierung dieses verlusts in relation zur vernderung der gesamtbehandlungszeit bemhen , sind in den tabellen 1 bis 5 fr verschiedene tumorentitten zusammengestellt . 
aus diesen tabellen lassen sich folgende allgemeine schlussfolgerungen ziehen : ( cid : 127 ) in keiner publikation kann nachgewiesen werden , dass eine verlngerung der gesamtbehandlungszeit zu einer verbesserung der behandlungsergebnisse fhren wrde . 
 ( cid : 127 ) eine verkrzung der gesamtbehandlungszeit fhrt in der mehrzahl der randomisierten studien bei kopf - hals - tumoren , nichtkleinzelligen bronchialkarzinomen und kleinzelligen bronchialkarzinomen zu einer verbesserung der lokalen tumorkontrolle . 
 ( cid : 127 ) eine verlngerung der gesamtbehandlungszeit , sei es durch einlegen einer pause [ 31 ] oder aus anderen grnden ( gertedefekte , feiertage , interkurrente erkrankungen des patienten ) , fhrt in unterschiedlichem mae zu einem verlust an lokaler kontrolle , der sich u.u. 
 > 50 tage 63 , > 63 tage besonders groe tumoren ( stadium iii / iv ) , nicht stadium i + ii auch negativer einfluss der verlngerung verlust an lokaler kontrolle in den intervallen 5% , 11% , auf das berleben , nicht stadium i + ii 15% , 20% 1 , 1% / tag verlngerung 0 , 85% / tag verlngerung 0 , 7% / tag verlngerung keine signifikanten unterschiede multivariate analyse : berleben ( p = 0 , 003 ) und lokale kontrolle ( p = 0 , 003 ) < 50 tage besser 0 , 67% / tag verlngerung fr berleben sind zeit und transfusionen wichtigste faktoren alle stadien ibiii ( ausnahme ib > 3 cm ) verlust an lokaler kontrolle erst oberhalb 55 tagen nachweisbar partielle hyperfraktionierung in der 3 . 
woche , strkere rektale blutungen bei krzerer behandlungszeit gesamtbehandlungszeit , teleund brachytherapie zustzlich signifikant je kleiner tumor , umso geringer zeiteinfluss ( 0 , 45% / tag ibiia , 0 , 57% / tag iib , 0 , 73% / tag iii ) negativ im letzten drittel eines behandlungsregimes wirkt , wie dies beispielsweise von skladowski et al . 
die radioonkologie wird noch ber jahre hinweg mit ungelsten fragen auf diesem gebiet zu leben haben , und der strahlentherapeut muss deshalb ganz pragmatisch entscheiden , dass es bei der gegenwrtigen datenlage das oberste behandlungsziel sein muss , eine verordnete gesamtbehandlungszeit ( die sicher abhngig von den institutsspezifischen verordnungspraxen ist [ 25 ] ) einzuhalten . 
 klinische konsequenzen und ausgleich von bestrahlungspausen die vorliegenden arbeiten besttigen sowohl in retrospektiven auswertungen ( tabellen 1 bis 3 ) als auch in randomisierten studien ( tabellen 4 und 5 ) , dass sich eine verlngerte gesamtbehandlungszeit bei den untersuchten patientenund tumorgruppen negativ auswirkt . 
die in dieser arbeit dafr errechneten standardabweichungen bei einbeziehung verschiedener datenstze sind erheblich ; trotzdem bedeutet 1 woche behandlungszeitverlngerung einen verlust an lokaler kontrolle zwischen 0 , 4% ( t1 - tumor ) und 16% ( groer tumor )  . 
the influence of overall treatment time on head and neck tumors . autor lokalisation patientenzahl behandlungszeitraum variationen verlust an lokaler kontrolle ergebnisse bemerkungen hno 468 larynx t1 , t2 t3 / t4 - tumoren 310 nasopharynx 107 t2 / t3 larynx 496 larynx 997 parsons et al . 
 1996 [ 27 ] 864 tonsille 676 ( multizentrisch ) glottis t1 217 larynx 383 alle patienten von split - course haben schlechtere ergebnisse ( lokale kontrolle ) berechnung von isoeffektivitt ( anstieg 0 , 33 0 , 06 ) korrelation zwischen lokaler kontrolle und zeitverlngerung verlngerungen von 4 tagen mssen mit einer zustzlichen fraktion von 2 gy kompensiert werden unterbrechung von > 3 wochen schlechter als ohne unterbrechung 941 tage 0 , 50 , 6 gy / d , um isoeffektivitt zu erreichen lokale kontrollrate 2 , 1 ( 1 , 43 , 1 ) hher bei kontinuierlicher kontinuierlich ( 214 ) vs . 
 split - course ( 352 ) lokale kontrolle ( in field ) lokale kontrolle 26 / 28 2 tage ( 29 / 30 ; 31 / 32 ; 33 tage ) stadium zustzlich von bedeutung ausgleich 0 , 50 , 7 gy / d in t2 zeitverlngerung negativ und in bei greren tumoren effekt nicht gesamtgruppe ( multivariate analyse ) , mehr nachweisbar , tund nin weiteren subgruppen nicht 1% / tag ( cid : 1 ) in tumorkontroll wahrscheinlichkeit 4442 tage : 88% 4346 tage : 78% hhere rezidivrate ( anstieg von 27% nur plattenepithelkarzinome auf 39% ) bei behandlungszeit > 31 tage gesamtbehandlungszeit kein prognostischer faktor fr t1 - glottiskarzinome kontinuierlich : 10% hhere 5 - jahresberlebensrate 5 - jahres - berlebensrate identisch nsd - konzept genutzt besonders zwischen 4 . 
split ( in hheren stadien ) eindeutig , nicht jedoch innerhalb der untersuchungszeitrume 20 fraktionen mit 2 , 63 gy ( 4 - mal hhere raten an karzinombedingten todes fllen , wenn > 30 tage ; effekt nicht bei t1n0 - tumoren ) bereits die unterbrechung der bestrahlungsserien um 1 woche ( feiertage ) reduziert bei t1 - tumoren lokale kontrolle von 89% auf 74% ( p < 0 , 05 ) multizentrische analyse ( edinburg , glasgow , manchester , toronto ) differente zeiten und dosen gleiche ergebnisse auch fr lokoregionale kontrolle und berleben nishimura et al . 
 1996 [ 70 ] larynx 96 t1n0 , 32 t2n0 4249 tage / > 49 tage in multivariater analyse ist nur die zeit signifikant ( p = 0 , 0008 ) ( nicht t , n , fraktionsgre , f / tag ) robertson et al . 
 44 tage ( 4052 ) t1 : 62 gy in 6 , 5 wochen t2 : 65 gy in 4 , 5 wochen larynx ( t1t4 ) > 2 700 patienten zungengrund 217 hno 419 stimmband 519 larynx t12n0m0 137 hno postoperativ 60 gy in 6 wochen ( 39 ) vs . 
 2003 [ 39 ] larynx t1 200 52 gy ( ed 3 , 3 gy ! ) in 21 tagen 96% 5 - jahres - kontrolle kein anstieg kurzes regime bietet weitere vorteile der toxizitt fr patienten und klinik strahlenther onkol 2005 no . 
 2003 [ 40 ] mammakarzinom 398 ( perkutan und interstitiell ) sophagus 353 lunge ( nsclc ) 153 lunge ( nsclc ) 256 analkarzinom 103 lokale kontrolle ( 3 jahre ) 3540 , 4150 , 5160 tage intervall zwischen perkutan und interstitiell durchschnittlich 5 , 9 wochen variabel 3555 tage lokale kontrolle krankheitsfreies berleben < 36 , 3650 , > 50 tage vergleich hyperfraktioniert ( hart [ 3049 tage ] ) vs . 
kontinuierliche fraktionierung ( 38 ) daten werden angezweifelt von marks 1992 [ 65 ] und kleineidam & dubben 1992 [ 56 ] multivariate analyse : zunahme des rezidivrisikos um faktor 1 , 23 ( 1 , 071 , 48 ) / woche , intervall so kurz wie mglich ! 1 woche verlngerung fordert 1 , 8 gy mehr , um identisches berleben zu erreichen ab 40 . 
tag 0 , 60 , 7 gy / tag lymphknoten schlechter , wenn intervall lnger kontinuierlich besser als split - course , 0 , 24 gy / tag bei t2 - tumoren fr lokale kontrolle nach 1 jahr lokale kontrolle nach 2 jahren 0 , 2 gy / tag fr n0 - patienten 0 , 45 gy / tag fr alle patienten multivariate analyse , signifikante weitere faktoren tumorgre , reduktion ( p = 0 , 02 ) zwischen hart , hyperfraktioniert und konventioneller fraktionierung in lokaler kontrolle lokale kontrolle nach 5 jahren 41 tage 58% vs . 
 < 41 tage 79% ( p = 0 , 04 ) kein einfluss der pause , nur der gesamtbehandlungszeit stadium , dosen > 66 gy in allen drei gruppen ( cid : 127 ) eine krzere behandlungszeit ist gnstig auch der abstand zu einer vorherigen operation sollte so kurz wie aus der klinischen situation heraus akzeptabel gewhlt werden [ 5 ]  . 
 ( cid : 127 ) bei kleineren tumoren im larynxbereich sind auch verkrzte behandlungsregime mit greren einzeldosen vertretbar , ohne dass dadurch schwerere akute nebenwirkungen eingetreten wren [ 39 ]  . 
 ( cid : 127 ) behandlungsprotokolle , die eine verkrzung der behandlungsserie durch akzeleration whrend der ganzen serie oder whrend eines teils der behandlungsserie vorsehen , sind hinsichtlich der akuten nebenwirkungen akzeptabel und erhhen die lokale kontrolle [ 29 , 102 ]  . ( cid : 127 ) die bestrahlung mit sechs fraktionen pro woche , die zu einer verkrzung der behandlungszeit von kopf - halstumoren auf 5 wochen fhrt , ist signifikant besser als eine 6 - wchige serie und in dnemark inzwischen standard [ 73 ]  . 
damit sind als feste endpunkte einer kurativ intendierten strahlentherapie primr eine gesamtdosis und eine gesamtbehandlungszeit zu verschreiben die einzeldosis und die anzahl der fraktionen / tag sind so zu whlen , dass die primr verordneten dosen und zeiten eingehalten werden knnen . 
es lassen sich folgende praktische schlussfolgerungen ableiten : ( cid : 127 ) wenn kein kuratives ziel angestrebt wird , ist eine kompensation von bestrahlungspausen in der regel nicht notwendig . 
 ( cid : 127 ) die gegenwrtige studienlage bei einigen , meist langsam wachsenden tumorentitten ( tabelle 6 ) liefert nicht gengend belastbare daten , dass eine verlngerung der behandlung um einige wenige tage zu verschlechterter lokaler kontrolle fhrt und damit unbedingt ausgeglichen werden muss . 
20% identische lokale kontrolle bei 12 gy niedrigerer dosis ( = 0 , 36 gy dosisverlust / tag ) schwere frhund sptnebenwirkungen fraktionsintervall 4 , 5 h ! gesamtbehandlungszeit von 7 auf 5 wochen verkrzt concomitant boost kein signifikanter unterschied , allerdings 10 gy weniger dosis ! keine signifikanz , 66 gy in beiden armen krankheitsspezifisches berleben steigt von 66% auf 70% an , nicht gesamtberleben bessere ergebnisse ( 42% ) bei radiochemotherapie tabelle 5 . 
48% ( p = 0 , 06 ) ( cid : 127 ) es gibt tumorerkrankungen mit spezieller histologie ( plattenepithelkarzinome ) , bei denen in einer flle von studien meist im kopf - hals - bereich nachgewiesen werden konnte , dass eine behandlungsverlngerung vermieden bzw . 
analogschlsse auf plattenepithelkarzinome in allen auch den noch nicht durch studien untersuchten krperregionen sind erlaubt , so dass speziell bei plattenepithelkarzinomen eine mglichst kurze behandlungszeit zu verordnen ist , die streng eingehalten werden muss . 
hierfr stehen in der praxis verschiedene mglichkeiten zur verfgung [ 9 , 13 ] ( tabelle 7 ) : die beste kompensation einer eingetretenen bestrahlungspause ist die zustzliche gabe von fraktionen gleicher fraktionsdosis an den ansonsten bestrahlungsfreien strahlenther onkol 2005 no . 
 dringend erforderlich notwendig nicht notwendig plattenepithelkarzinome der kopf - hals - region plattenepithelkarzinome der lunge zervixkarzinome plattenepithelkarzinome der haut und sonstige manifestationen medulloblastome alle kurativen therapieanstze bei verschiedenen histologien palliative bestrahlungen bestrahlung gutartiger erkrankungen hodgkinund non - hodgkin - lymphomea prostatakarzinomeb a bisher liegen keine evidenzbasierten daten zu diesen bestrahlungsindikationen vor , was jedoch nicht heit , dass die gesamtbehandlungszeit keine bedeutung htte [ 69 ] ; b diese aussage ist nicht evidenzbasiert ; allerdings ist anzunehmen , dass auch bei diesen bestrahlungsindikationen die einhaltung der verordneten gesamtbehandlungszeit sinnvoll ist wochenenden . 
 kompensationsmglichkeiten zu beachten feiertage gerteausfall patientenbezogene grnde ( radiogene nebenwirkungen , interkurrente erkrankungen ) bestrahlung am wochenende bestrahlung mehr als 1 / tag bestrahlung mit hherer einzeldosis abstand > 6 , besser 8 ha grere hufigkeit von spteffektenb grundlage : die verschriebene gesamtbehandlungszeit muss eingehalten werden ! a u.u. 
3 / tag wie in chart - protokoll , allerdings nur mit strenger einhaltung der abstnde zwischen den fraktionen und nicht , sofern rckenmark im zielvolumen bis an die toleranzgrenze ( bei 1 tglicher bestrahlung ) belastet werden soll ; b die restlichen fraktionsdosen und die neue gesamtdosis sind mit dem lq - modell ( / = 3 ! ) abzuschtzen ! grnde alternativ kann die gabe zustzlicher fraktionen an bestrahlungstagen im abstand von mindestens 6 h ( sofern das rckenmark im bestrahlungsvolumen liegt und hoch belastet wird , besser 8 h ) eingesetzt werden . 
 beide methoden haben den vorteil , dass sie sehr einfach sind und keinerlei strahlenbiologische berechnungen brauchen : die verschriebene gesamtdosis , die verschriebene dosis pro fraktion , die anzahl der fraktionen und die gesamtbehandlungszeit bleiben vllig unverndert . 
angesichts der guten erfahrungen hinsichtlich der vertrglichkeit von drei fraktionen im abstand von 6 h im rahmen der chart - programme kommt dieser kompensationsform neben der bestrahlung an den wochenenden besondere bedeutung zu . 
 seit der publikation der guidelines for the management of the unscheduled interruption or prolongation of a radical course of radiotherapy des royal college of radiology london im jahre 1986 , die 1998 von baumann & herrmann [ 9 ] referiert wurden , hat sich zweifelsohne die datenlage zu strahlenther onkol 2005 no . 
klinische bedeutung der kompensation ungeplanter bestrahlungspausen diesen fragen so stabilisiert , dass die damals ausgesprochene empfehlung , an den einzelnen radioonkologischen behandlungszentren handlungsanweisungen zu entwickeln und eine verlngerung einer kurativen bestrahlungsserie zu kompensieren , heute , 6 jahre nach dieser publikation , nicht mehr als empfehlung , sondern als forderung formuliert werden muss . 
 angesichts der bei bestimmten tumoren nachgewiesenen verschlechterung an heilungswahrscheinlichkeit durch eine behandlungszeitverlngerung hat der patient in der radioonkologie nicht nur ein recht auf einen qualittskontrollierten hohen physikalischen standard seiner therapie , sondern auch auf die einhaltung strahlenbiologischer parameter , zu denen neben der einzelund gesamtdosis die gesamtbehandlungszeit zu zhlen ist . 
failure - specific prognostic factors after continuous hyperfractionated accelerated radiotherapy ( chart ) or conventional radiotherapy in locally advanced non - small - cell lung cancer : a competition risks analysis . 
a randomised phase iii study of accelerated or standard fraction radiotherapy with or without concurrent carboplatin in inoperable non - small - cell lung cancer : final report of an australian multi - centre trial . 
a radiation therapy oncology group ( rtog ) phase iii randomized study to compare hyperfractionation and radiotherapy for head and neck squamous cell carcinomas : first report of rtog 9003 . 
accelerated fractionation ( af ) compared to conventional fractionation ( cf ) improves loco - regional control in the radiotherapy of advanced head and neck cancers : results of the eortc 22851 randomized trial . 
2 urban & vogel strahlentherapie und onkologie original article radiotherapy of prostate cancer with multileaf collimators ( mlcs ) optimization of the undulating dose distribution at the mlc edge oliver koelbl , franz schwab , klaus bratengeier , dirk vordermark , michael flentje1 background and purpose : a technical modification for radiotherapy of prostate cancer is presented to smooth the scalloped dose pattern that occurs at treatment field edge , when a multileaf collimator ( mlc ) has been used . material and methods : ten patients with prostate cancer receiving postoperative , adjuvant irradiation were studied prospectively . 
by a three - dimensional planning system ( tms , helax 6.1b ) the irradiation was planned for an 18 - mv linear accelerator ( primus 1 , siemens )  . 
the volumes of interest ( voi ) were the planning target volume ( ptv ; the region of the prostate including the seminal vesicles ) , the volume of rectum ( vrectum ) and urinary bladder ( vbladder )  . 
film dosimetry was used to show the dose pattern at the field edge produced by the two techniques . results : dose to ptv did not differ between technique a and b . 
especially for irradiation to escalated dose levels , this modification may reduce the dose to the rectum and thus the rectal side effects in comparison to the conventional mlc fields . key words : prostate cancer irradiation technique multileaf collimator strahlenther onkol 2005 ; 181 : 10812 doi 10.1007 / s00066 - 005 - 1341 - 7 radiotherapie des prostatakarzinoms unter verwendung des multileaf - kollimators ( mlc )  . 
optimierung der stufenartigen dosisverteilung am mlc - rand hintergrund und ziel : eine modifikation der bestrahlungstechnik beim prostatakarzinom wird vorgestellt , die den mehrstufigen dosisverlauf am feldrand ausgleicht , wie er bei verwendung eines multileaf - kollimators ( mlc ) entsteht . material und methodik : zehn patienten wurden in die analyse einbezogen . 
bei technik a wurde der mlc in jedem feld bei einem kollimatorwinkel von 0 an das ptv angepasst , bei technik b wurde der kollimatorwinkel der seitlichen felder so optimiert , dass sich die in den seitlichen feldern entstehenden stufen gegenseitig ausglichen . 
die mediane dosis in vbladder unterschied sich bei beiden techniken nicht ( p > 0 , 05 )  . 1 department of radiotherapy , university of wuerzburg , germany . received : july 20 , 2004 ; accepted : november 29 , 2004 strahlenther onkol 2005 no . 
field edge smoothing by optimized multileaf collimation schlussfolgerung : die vorgestellte modifikation ist eine einfache und effektive methode zum ausgleich der stufigen feldrnder und dosisverlufe , wie sie bei der verwendung von mlc entstehen . 
 ( cid : 127 ) for technique b the collimator angle of the 90 - field was individually chosen to optimize the adaptation of leaves to the dorsal border of ptv . 
the collimator angle of the 270 - field worked in opposite direction to compensate the cascade dorsal field border of the 90 - field . figures 1 and 2 schematically show the principle of technique a and b . 
film exposures were carried out using a laser scanner , and film densities were converted to dose ( iba omni pro - accept 6.0a , kodak x - omatv , perspex phantom with 10 cm depth , 18 - mv photon )  . 
 stepped field edge congruent multileaf position of the 90and 270 - field introduction multileaf collimators ( mlcs ) allow the radiation beam to be irregularly shaped to conform to tumor volumes without the use of individually shaped alloy blocks , whose production , daily handling and storage are labor - intensive and resource - consuming [ 11 ]  . 
 the present study aims to optimize the mlc leaf fitting of a four - field irradiation technique for prostate cancer and thereby to reduce the dose to the rectu material and methods ten consecutive patients receiving postoperative radiotherapy because of prostate cancer were studied . 
 treatment planning was performed using a three - dimensional ( 3 - d ) planning system ( helax , tms 6.1b ) for 18 - mv photons to be delivered by a primus 1 ( siemens ) linear accelerator . 
die individuell angepasste kollimatorposition der gegenfelder fhrt zu einem ausgleich des stufenfrmigen feldrandes . isodose lines is smoothed and the effective penumbra width , defined as the area between ptv and isodose lines , is reduced ( figure 3 )  . 
technique a irradiates a larger vrectum than technique b , being significant for all tested isodose levels tested ( 90% / 80% / 60% / 40% isodose ; table 2 )  . contrary to this , neither median dose to the bladder nor irradiated vbladder at any dose level differed for technique a and b . 
 helyer & heisig reported a time reduction of 1948% for parallel opposed beams and 644% for conformal isocentric beams by the change from alloy blocks to mlcs [ 11 ]  . 
additionally , losasso & kutcher described a higher accuracy of mlcs , because lead alloy blocking contains lower precision with positioning errors due to block misalignment [ 12 ]  . 
since the mlc leaf width is commonly 10 mm at isocenter , the treatment fields do not exactly follow the beams eye view of the ptv , but instead provide a stepped approximation to the ptv shape [ 1 ]  . 
when the border of the ptv falls in close proximity to a critical structure also having a relatively smooth edge , the undulating dose pattern can be a disadvantage . some authors suggest that the importance of this effect is reduced by the daily setup variations and the organ mobility [ 2 , 6 ]  . 
although the mlc fitting is closer to the ptv by this technical modification , the width of the dose pattern steps is still 1 cm because of the 1 - cm width of the leaves . 
they divided the treatment field into a number of subfields in which the mlc is shifted by a fraction of leaf width and adjusted to redefine the field edge in relation to the new position of the treatment volume border . 
as a result of this , the steps of the mlc field edges of both fields are shifted and the effective leaf width is reduced , both resulting in a blurred dose pattern . 
in our clinical study we could significantly reduce the vrectum within the high - dose ( 90% isodose ) and the low - dose ( 40% isodose ) regions for a four - field - technique . 
since it is an isocenter technique and treatment time is not extended compared to the conventional mlc technique , this technique is practicable for daily routine irradiation of patients with prostate cancer . 
especially for irradiation of the prostate to escalated dose levels , the presented mlc field modification may reduce the dose to the rectum and thus the rectal side effects in comparison to conventional mlc fields . strahlentherapie und onkologie original article feasibility of combined operation and perioperative intensity - modulated brachytherapy of advanced / recurrent malignancies involving the skull base rainer j . 
maximilian mehdorn1 purpose : to assess the technical feasibility and toxicity of combined operation and perioperative intensity - modulated fractionated interstitial brachytherapy ( imbt ) in advanced - stage malignancies involving the skull base with the goal of preserving the patients senses of sight . patients and methods : this series consisted of 18 consecutive cases : ten patients with paranasal sinus carcinomas , five with sarcomas , two with primitive neuroectodermal tumors ( pnets ) , and one with parotid gland carcinoma . 
after , in most cases , subtotal surgical resection ( r1r2 : carried out so that the patients senses of sight were preserved ) , two to twelve ( mean five ) afterloading plastic tubes were placed into the tumor bed . 
the total imbt dose , ranging from 10 to 30 gy , was administered in a fractionated manner ( 35 gy / day , 5 days / week )  . results : perioperative fractionated imbt was performed in 15 out of 18 patients and was well tolerated . 
complications that partially prevented or delayed imbt in some cases included cerebrospinal fluid leakage ( twice ) , meningitis ( twice ) , frontal brain syndrome ( twice ) , afterloading tube displacement ( twice ) , seizure ( once ) , and general morbidity ( once )  . 
median survival times were 33 months after diagnosis and 16 months after combined operation and imbt . conclusion : perioperative fractionated imbt after extensive but vision - preserving tumor resection seems to be a safe and well - tolerated treatment of advanced / recurrent malignancies involving the skull base . 
these preliminary data suggest that combined operation and perioperative fractionated imbt is a palliative therapeutic option in the management of fatal malignancies involving the base of the skull , a strategy which leaves the patients visual acuity intact . key words : iridium - 192 afterloading palliation paranasal sinus carcinomas perioperative hdr / pdr brachytherapy recurrent skull base tumors sarcomas visual acuity strahlenther onkol 2005 ; 181 : 97107 doi 10.1007 / s00066 - 005 - 1274 - 1 durchfhrbarkeit einer kombinationsbehandlung aus operation und perioperativer intensittsmodulierter brachytherapie bei malignomen mit schdelbasisbefall ziel : prfung der technischen durchfhrbarkeit und toxizitt einer kombinationsbehandlung aus operation und perioperativer intensittsmodulierter fraktionierter interstitieller brachytherapie ( imbt ) bei malignomen fortgeschrittener stadien mit schdelbasisbefall mit dem ziel , die sehfunktion zu erhalten . 
 patienten und methodik : diese serie bestand aus 18 konsekutiven fllen : zehn patienten mit nasennebenhhlenkarzinomen , fnf mit sarkomen , zwei mit primitiven neuroektodermalen tumoren ( pnets ) und ein patient mit speicheldrsenkarzinonach zumeist subtotaler chirurgischer resektion ( r1r2 : ausgefhrt unter erhalt der sehfunktion ) wurden zwei bis zwlf ( durchschnittlich fnf ) afterloading - applikatoren im tumorbett platziert . 
die imbt wurde mit einer wandernden iridium - 192 - strahlungsquelle im pulsed - dose - rate / high - dose - rate - ( pdr / hdr - ) afterloading - verfahren durchgefhrt . 
die imbt - gesamtdosis von 1030 gy wurde fraktioniert mit 35 gy tglich fr 5 tage / woche appliziert . ergebnisse : die perioperative fraktionierte imbt wurde bei 15 von 18 patienten durchgefhrt und gut vertragen . 
komplikationen , welche die imbt teilweise verhinderten oder verzgerten , umfassten : liquorleck ( zweimal ) , meningitis ( zweimal ) , frontalhirnsyndrom ( zweimal ) , dislokation der afterloading - applikatoren ( zweimal ) , krampfanfall ( einmal ) und allgemeine morbiditt ( einmal )  . 
 1 department of neurosurgery , university hospital schleswig - holstein campus kiel , germany , 2 interdisciplinary brachytherapy center , department of radiotherapy / radiation oncology , university hospital schleswig - holstein campus kiel , germany , 3 department of otolaryngology , university hospital schleswig - holstein campus kiel , germany , 4 department of ophthalmology , university hospital schleswig - holstein campus kiel , germany . 
die mittleren berlebenszeiten betrugen 33 monate nach diagnosestellung und 16 monate nach kombinierter operation und imbt . schlussfolgerung : die perioperative fraktionierte imbt nach ausgedehnter , die sehfunktion jedoch erhaltender tumorresektion scheint eine sichere und gut vertrgliche behandlungsmethode fr fortgeschrittene malignome mit schdelbasisbefall zu se diese vorlufigen daten lassen den schluss zu , dass die kombination aus operation und perioperativer fraktionierter imbt eine palliative therapeutische option bei patienten mit ansonsten verhngnisvollen malignomen mit schdelbasisbefall darstellt , eine strategie , welche die sehschrfe des patienten intakt lsst . schlsselwrter : iridium - 192 - nachladeverfahren nasennebenhhlenkarzinome palliation perioperative hdr / pdr brachytherapie rezidivierende schdelbasistumoren sarkome sehschrfe introduction advanced malignancies involving the base of the skull are particularly difficult to treat because of their proximity to vital structures such as the brain , the optic nerves , the eyes , and the internal carotid arteries . 
despite significant advances in cranial base surgery [ 9 , 12 ] and radiation therapy [ 1 , 5 , 6 , 11 , 27 , 29 , 3537 ] , complete tumor eradication of advanced skull base tumors is still often impossible . 
adjuvant radiotherapy in conjunction with debulking surgery has proven to increase the life span of patients [ 15 , 25 , 30 ] , but such treatment also increases the risk of toxic damage due to the limited radiation tolerance of important surrounding structures . 
by exploiting intraoperative and histopathologic information , however , the effectiveness of such combined treatment modalities can be increased over that attainable on the basis of imaging - based target definition alone . 
 intensity - modulated fractionated brachytherapy ( imbt ) enables the local control of microscopic residual disease by employing high focal radiation which is relatively innocuous to normal tissue surrounding the lesion . 
compared with various external - beam radiation therapy ( ebrt ) techniques , intraoperative placement of plastic tubes for postoperative irradiation offers better target definition based on intraoperatively derived information and supported by neuronavigation . most tumors located on the skull base which have , up to now , been treated by brachytherapy were intracranial gliomas [ 40 ] or meningiomas , adenomas , and chordomas [ 6 , 21 ]  . 
in the past , brachytherapy was mainly applied to such tumors by stereotactic seed implantation [ 21 , 33 ]  . in this study , we report our preliminary experience with a novel multimodal , interdisciplinary therapy which involves salvage tumor surgery and perioperative imbt and allows for the preservation of visual function while yielding effective treatment to advanced malignancies involving the skull base . 
 the motivation for developing this therapeutic approach was the desire to elaborate an interdisciplinary method which is effective in gaining local tumor control but one which , at the same time , allows for the preservation of visual acuity also in patients who have undergone previous therapeutic irradiation . 
the aim of this retrospective analysis was to assess the technical feasibility and toxicity involved in this method and to evaluate the outcomes of patients who have received such treatments with a particular emphasis on the posttreatment intactness of their visual systems . patients and methods patient selection 18 consecutive patients were selected at the university hospital schleswig - holstein campus kiel , germany , between december 1992 and june 2002 . 
the criteria of patient selection were as follows : either complete tumor resection seemed to be impossible and / or the tumor was in the proximity of vital structures and / or ebrt had already been performed or imbt enabled ebrt to be performed either at lower doses or to be omitted entirely . 
the decision to include a patient was made after interdisciplinary consultation among surgeons of several specialties and radiation oncologists / brachytherapy experts who work together in the interdisciplinary brachytherapy center of the faculty . 
 patient characteristics ten patients had paranasal sinus carcinomas including one esthesioneuroblastoma , five had sarcomas , two had primitive neuroectodermal tumors ( pnets ) , and one had a parotid gland tumor ( table 1 )  . 
perioperative imbt in recurrent skull base tumors the bra15 patients had recurrent ( n = 11 ) , progressive ( n = 2 ) or persistent ( n = 2 ) tumor after prior treatment . 
these were initially treated by either surgery alone ( twice ) , chemotherapy alone ( twice ) , surgery and chemotherapy ( three times ) , surgery and radiotherapy ( twice ) , chemotherapy and radiotherapy ( twice ) , or combined surgery , radiotherapy and chemotherapy ( four times )  . 
the total imbt dose ranged from 10 to 30 gy ( median 20 gy ) and was administered using a fractionated regimen ( 35 gy / day ) in afterloading technique a few days after the operations . 
the brachytherapy was a planned boost before complementary ebrt in nine patients and after prior ebrt in eight . limitations of the procedure as seen in our series it can be the case that patients who were primarily planned for perioperative imbt had to be excluded postoperatively from this form of perioperative imbt due to various reasons . 
because of a lack of commercial systems at the time period of our series , we used a homemade software system for ct / mri - based three - dimensional treatment planning in interstitial brachytherapy [ 14 ] which allowed for neither the generation of volume values such as table 1 . 
ac : adenocarcinoma ; acc : adenoid - cystic carcinoma ; awd : alive with disease ; c : chemotherapy ; dod : dead of disease ; enb : esthesioneuroblastoma ; imbt : intensity - modulated fractionated interstitial brachytherapy ; ldc : low differentiated carcinoma ; lms : leiomyosarcoma ; ned : no evidence of disease ; ns : neurogenous sarcoma ; pnet : primitive neuroectodermal tumor ; r : radiotherapy ( = external - beam radiation therapy [ ebrt ] ) ; rms : rhabdomyosarcoma ; s : surgery ; scc : squamous cell carcinoma ; tcc : transitional cell carcinoma . 
 [ 16 ] ; c tumor metastasis originating from parotid gland carcinoma ; d ebrt + second imbt with 20 gy ( 2 2.5 gy / d ) ; e preor postprocedural ebrt strahlenther onkol 2005 no . 
acquisition of data such as anatomic site of locally recurrent tumor growth is difficult because the chosen imbt radiation dose may be reduced for the purpose of palliation ( rather than eradication ) , i.e. , eye preservation , so that there is still resid - ual / microscopic tumor in the clinical target volume ( ctv = primary tumor volume [ ptv ] ) immediately after imbt . 
 the decision for the surgical approach was made under interdisciplinary consultation with special reference to optimal anatomic access and maximal tumor resection with preservation of critical functions , as well as optimal placement of plastic tubes for fractionated imbt . 
the tumor was resected by an interdisciplinary surgical team including the brachytherapy expert and with the aid of an image - guided navigation system which was able to confirm the degree of tumor removal and to define the positive margins ( figure 1a )  . 
after maximal resection of the tumor , i.e. , r1r2 resection , bearing in mind the preservation of function and vital structures , an appropriate number of flexible , nonradioactive plastic tube imbt applicators were intraoperatively placed in the resected tumor bed near the positive margins ( figure 1b )  . 
the placement was performed in the presence of the radiation oncologist , using a manual technique with a geometry for an optimized radiation dose distribution : distances between plastic tubes were enlarged in regions , where higher doses were needed , and the tubes were implanted closer to each other for lower radiation doses if sensitive areas were surrounding . 
the imbt applicator tubes were fixed by using artificially created semistereotactic channels through bone structures , whenever possible , and also aided by the image - guided navigation systethese channels were prepared to have the same outer diameter as the plastic tubes . 
at the end of operation , the ends of the tubes jutted out from the patients body at locations which resulted in the optimal position for uncomplicated postoperative care without kinking the applicators ( figure 1c )  . 
for this purpose , using cross - section imaging data , applicator positions had to be correctly digitized on each image manually , but several contours could have been found by an automatic algorith regions or structures of interest such as the eye with the optic nerve and bony structures were contoured in a manual , semiautomatic , or automatic mode . the volume - optimized target dose was calculated for use with , preferentially , the pulsed - dose - rate ( pdr ) or , if the machine was occupied , the high - dose - rate ( hdr ) remote afterloading unit with an individual reference fraction dose of 1 and 2.5 gy , respectively , at a distance of 10 mm lateral to the applicator surface . 
the accepted maximal applicator surface dose was defined to be four times the reference isodose value , because there was no preexistent prescription data in the literature concerning such kind of application . 
the inhomogeneity of the dose distribution within the target volume was adapted to the anatomic situation : critical structures were close to cold spots , and residual / potentially residual tumor areas were covered with hot spots . 
in the majority of cases , the dose was given as fractionated 2 - h pulses , five times a day with a dose per pulse of 1 gy on the surface of the individual target volume , using the pdr unit , or 2 2.5 gy daily with an interval of 6 h using the hdr unit . 
due to the combination of imbt with its steep dose fall - off and ebrt , the total dose to critical structures could be kept below the tolerance level . clinical outcome evaluation all patients were regularly examined preand postprocedurally by the treating surgeons and the ophthalmologists at our university hospital . 
follow - up data were obtained for all patients either by examinations or by phone calls with the patient or his / her relatives , his / her ophthalmologist , or general practitioner . 
neurologic - clinical examinations were performed at our neurosurgical department at 3 - month or longer intervals depending upon the clinical course and the compliance of the patient . illustrative cases the total bt radiation dose varied in the range of 1030 gy depending on the site of the tumor and the aim of patient #3 . 
at the end of surgery , a lumbar cerebrospinal fluid ( csf ) drainage was inserted for several days . postoperative ct scan showed the proper position of applicator tubes , and clinical aspects were unremarkable . 
after three - dimensional imbt simulation planning ( figure 1d ) , a total fractionated radiation dose of 15 gy was given in 3 - gy daily single fractions . in the course of imbt , replanning of irradiation became necessary due to a slight displacement of two tubes . 
the irradiation was tolerated well , and he developed only temporary local erythema and mucositis . 5 months later , a cervical metastasis was diagnosed and removed by neck dissection followed by ebrt . 
a 33 - year - old woman , with a history of acute lymphatic leukemia treated by chemotherapy and ebrt of the whole brain 26 years earlier , presented with current olfactory dysfunction and reduced visual acuity on the right side . 
an mri scan showed infiltration of the skull base and the right orbit ( figure 3a )  . the patient underwent tumor excision with incomplete tumor removal from a combined transfacial and subfrontal approach . 
postoperatively , she received two cycles of polychemotherapy consisting of vincristine , ifosfamide , actinomycin d , mesna ( uromitexan ) , and adriamycwhile the orbital tumor showed partial remission , the tumor in the sphenoidal sinus revealed progression , so that another eye - preserving operation for maximal tumor resection through a paranasal route was indicated and fractionated perioperative imbt was included . five imbt applicator tubes were placed with their tips into the sphenoidal sinus and the right orbit . 
mri scans at 3 - month intervals showed local tumor control for the complete ongoing clinical course ( figure 3b )  . her score on the karnofsky performance scale was 100% , when a single spine metastasis was diagnosed at the t5 level 19 months later and subsequently operated on . 
 results feasibility maximally extensive and function - preserving tumor resection as well as intraoperative imbt tube applicator implantation were feasible in all patients and were aided by image - guided neuronavigation . 
they were as follows : i nerve palsy ( eight times ) , v nerve palsy ( twice ) , viii nerve palsy ( three times ) , ix nerve palsy ( once ) , x nerve palsy ( twice ) , xii nerve palsy ( four times ) , and ataxia by polyneuropathy after chemotherapy ( once )  . 
 table 3 shows preand postprocedural tumor - related pathologic findings in the visual system . in patient #6 who did not undergo imbt because of his frontal brain syndrome and seizures , deterioration of visual acuity was caused by bilateral tumor invasion into the orbit 7 months after the operation . 
perioperative imbt in recurrent skull base tumors at the last follow - up , 14 patients were dead of disease ( dod ) , three alive with no evidence of disease ( ned ) , and one alive with disease ( awd )  . 
it was 15 months ( mean 15.6 ; range 726 months ) for patients with paranasal sinus carcinomas / sarcomas and 33 ( mean 34.9 ; range 1598 months ) and 27 months ( mean 28.1 ; range 1838 months ) , respectively , after first diagnosis . 
 the median progression - free survival time after imbt was 7 months ( range 117 months ) for the whole group and 7 months ( range 112 months ) for patients with paranasal sinus carcinomas / sarcomas in particular . 
kaplan - meier analysis confirmed by log - rank test yielded a strong but nonsignificant trend ( p = 0.08 ) toward shorter survival in patients with dura infiltration versus those without ( figure 4 )  . procedure complications postprocedural complications to various extents occurred in ten of 18 patients ( table 2 )  . 
apart from patient #14 in whom the tumor - infiltrated vertebral artery was injured and had to be surgically remodeled in the same operation without any sequelae , there were no intraoperative complications . 
directly or indirectly operation - related postoperative complications of importance were csf leakage ( twice ) , meningitis ( twice ) , and frontal brain syndrome resulting in artificial tube displacement ( twice )  . 
after repair of the csf leakage , remission of the frontal brain syndrome , replacement of dislocated tubes , and resolution of meningitis , imbt was performed in patients #4 , #5 , and #18 . in patient #6 with prolonged frontal brain syndrome and additional seizures , as well as patient #15 with a serious csf leakage ( and without clear pathomorphological proof of tumor in the resected tissue ) , imbt was not performed . 
in a third patient ( #8 ) disease - related progress of general morbidity prevented imbt and was followed by tumor explosion on ct scans and death 2 months later . 
the bacterial skull osteomyelitis in patient #9 was diagnosed and treated 6 months after uneventful operation / imbt . apart from patient #1 developing a superficial skin defect in the operated and irradiated frontal area which had to be successfully revised by local operation , serious imbt - related side effects were not observed . 
another patient ( #12 ) , who received 25 gy interstitial irradiation by imbt and 76 gy complementary ebrt , developed a circumscribed superficial skin defect of about 10 mm and a small fistula channel to the table 3 . 
preand postprocedural pathologic findings of the visual systeawd : alive with disease ; b : both sides ; dod : dead of disease ; imbt : intensity - modulated fractionated interstitial brachytherapy ; l : left ; ned : no evidence of disease ; r : right ; vision ( cid : 1 ) : visual impairment . 
awd : mit krankheitszeichen am leben ; b : beidseits ; dod : an krankheit verstorben ; imbt : intensittsmodulierte fraktionierte interstitielle brachytherapie ; l : linksseitig ; ned : ohne krankheitszeichen ; r : rechtsseitig ; vision ( cid : 1 ) : visusabnahme . 
 discussion in this study , we examined the feasibility and benefits of a novel multimodal therapy approach consisting of combined tumor resection and fractionated perioperative interstitial imbt with special reference to the preservation of critical structures with relevance to the patients quality of life . 
the patients included in this study had advanced , mostly pretreated and recurrent malignancies with mainly intradural tumor extension whose prognosis would have been clearly fatal without any further treatment . 
apart from one case with vertebral artery injury and subsequent surgical remodeling without any sequelae , there were no major intraoperative complications and no operative deterioration of preexistent neurologic deficits . 
 [ 12 ] observed postoperative complications in 62 out of 143 cases of their large , multiinstitutional study on surgical results of skull base surgery for the treatment of head and neck malignancies involving the base of the skull . 
in their study , local infection was the most frequent complication ( 29 / 62 ) ; meningitis was diagnosed in ten cases , and liquorrhea occurred in 18 / 62 cases . 
 [ 28 ] reported occurrence of serious infections such as meningitis resulting from csf leakage in ten out of 14 patients undergoing neurosurgery for paranasal sinus carcinoma invading the skull base . 
it deserves to be noted that operation - related complications of our series occurred nearly exclusively in cases with extensive intradural tumor extension and subsequent surgical reconstruction of the dura . 
three patients agreed to be excluded from the procedure due to the following causes : disease - related progressive morbidity , csf leakage ( in combination with absence of tumor in the resected tissue ) , and ongoing frontal brain syndrome leading to artificial tube removal plus seizures . 
 while the methods benefit to the eye was quite obvious , any meaningful survival statistics for comparison with other series or other means of treatment were hampered not only by the small sample size , the palliative character of the study , and the lack of a control group , but even more severely by the diversity of histological diagnoses , tumor stage , site of origin , extent of tumor invasion , prior therapy , surgical approach , and individually adapted radiation . 
perioperative imbt in recurrent skull base tumors tion and radiotherapy [ 13 , 15 , 25 ] the prognosis for advanced / recurrent tumors , however , is generally considered to be rather poor . 
 [ 15 ] examined 73 patients with paranasal sinus carcinomas including 59% t4 tumors according to uicc / tnm 1997 , 50 of which had been treated by debulking surgery and ebrt . 
the median survival time after combined operation and bt ( as the main time point of recurrence ) of the large and advanced paranasal sinus carcinomas in our series was also 15 months with special respect to preservation of critical structures . 
 moreover , besides tumor stage , origin [ 8 ] and histology [ 9 ] , involvement of the dura mater [ 7 , 9 ] or the orbit [ 7 ] were identified as statistically significant prognostic indicators . 
in this context , tumor involvement of the orbit and intradural tumor extension each in ten of 14 dod patients in our series probably contributed to the relatively short survival time . 
 however , in strong concordance with the patients desire , we favored an enhancement in their quality of life instead of surgical mutilation , if complete surgical tumor eradication appeared to be improbable . 
there is , however , a large body of evidence for the efficiency of brachytherapy in skull base tumors in general [ 6 , 21 ] , so that a positive effect can at least be postulated . 
 compared to implantation of radioactive seeds [ 21 , 33 , 37 , 38 , 40 ] or intraoperative irradiation [ 11 , 26 , 31 ] , perioperative fractionated imbt with remote - controlled afterloading machine appears to be more user - friendly in terms of adequate definition of the target and critical structures . 
the targeted tumors , however , are usually < 3 cm in maximum dimension ( the selection being due to side effects and limited efficiency with increasing tumor size [ 22 ] ) ; this is in contrast to the larger tumors of 38 cm diameter in our series . 
 although there are excellent literature data concerning rare application forms of radiotherapy on the base of skull , the application of high linear energy transfer ( let ) irradiation is still not a common method and will seldom be used for palliative purposes [ 35 , 36 ]  . 
 conclusion these preliminary data suggest that perioperative imbt after extensive but function - preserving tumor resection of advanced skull base malignancies is a technically feasible salvage treatment modality with acceptable risks and the potential of preserving quality of life . 
the novel procedure described here may not improve the survival rate at advanced stages , but offers positive palliative potential by its functional and cosmetic advantages compared with radical surgical resection with or without ebrt . 
 strahlentherapie strahlentherapie und onkologie und onkologie original article automatic generation of a plan optimization volume for tangential field breast cancer radiation therapy koen van vaerenbergh , werner de gersem , luc vakaet , marc coghe , tom boterberg , marlies bakker , christina derie , wouter willaert , patricia seij , wim duthoy , carlos de wagter , wilfried de neve1 background and purpose : dose homogeneity is one of the objectives during computer planning of postoperative radiotherapy of the conserved breast . 
the purpose of this study was to develop a computer - generated delineation of a plan optimization volume ( pov ) and an irradiated volume ( iv ) and to automate their use in a fast dose homogeneity optimization engine . 
 patients and methods : simulation was performed according to our standard procedure which involves the positioning of a lead collar around the palpable breast to facilitate the definition of gantry angle , collimator angle and field aperture for tangential wedged photon beams . 
images from a serial ct scan were acquired in treatment position , and the geometric data of the three simulated beams were used by a computer program to generate the pov and iv . 
for each patient , weights of wedged and unwedged beams were optimized by either human heuristics using only the central slice ( 2 - d ) , the whole set of ct slices ( 3 - d ) , or by a computer algorithm using the pov , iv and lung volume with constrained matrix inversion ( cmi ) as optimization method . 
 results : the total planning procedure took , on average , 44 min of which < 7 min were needed for human interactions , compared to about 52 min for the standard planning at ghent university hospital , belgiuthe simulation time is increased by 23 m the method provides 3 - d information of the dose distribution . 
 conclusion : this automated planning method is capable of replacing the contouring of the clinical target volume as well as the trial - and - error procedure of assigning weights of wedged and unwedged beams by an experienced planner . 
 key words : breast cancer automated generation plan optimization strahlenther onkol 2005 ; 181 : 828 doi 10.1007 / s00066 - 005 - 1310 - 1 automatisierte erstellung eines optimierten planungszielvolumens fr ein tangentiales bestrahlungsfeld bei brustkrebs hintergrund und ziel : dosishomogenititt ist eines der ziele bei der planung fr die strahlentherapie nach brusterhaltender operation . 
ziel dieser studie war , eine computergesteuerte erstellung des optimierten planungszielvolumens ( pov ) und des bestrahlten volumens ( iv ) zu entwickeln und ihren einsatz in einem schnellen rechner zur optimierung der dosishomogenitt zu automatisieren . 
 patienten und methoden : die simulation wurde nach unserem standardverfahren durchgefhrt , bei dem eine bleikette um die tastbare brust gelegt wird , um die festlegung von gantry - winkel , kollimatorwinkel und feldgren fr tangentiale keilfilterfelder zu erleichtern . 
in einer abwandlung des standardverfahrens wurde ein anterolaterales rntgenbild aufgenommen , dessen achse orthogonal zur zentralebene der beiden tangentialen strahlen verluserielle ct - schnitte wurden in behandlungsposition aufgenommen , und mit den geometrischen daten der drei simulierten felder erstellte ein computerprogramm pov und iv . 
fr jede patientin wurde die wichtung fr die strahlenfelder mit und ohne keilfilter optimiert , indem manuell nach menschlichem ermessen nur die zentrale schicht ( 2 - d ) bzw . 
 ergebnisse : das gesamte planungsverfahren dauerte durchschnittlich 44 min , von denen < 7 min fr menschliche interaktion bentigt wurden , im vergleich zu rund 52 minuten beim standardverfahren der universittsklinik gent / belgien . 
 schlsselwrter : mammakarzinom automatisierte erstellung planoptimierung introduction the clinical target volume ( ctv ) for patients treated with breast - conserving surgery and requiring adjuvant external tangential field irradiation is the total palpable breast volume [ 23 ]  . 
however , the icru recommendations [ 13 ] are frequently violated , if the full three - dimensional ( 3 - d ) dose distribution is analyzed [ 1 ]  . 
computer optimization ( at ghent university hospital [ guh ] , belgium , this is done using in - house developed tools [ 5 , 7 ] ) of the 3 - d dose homogeneity is possible but requires the delineation of a volume on all slices that can be used for optimization of the dose distribution . 
contouring such a volume manually is a time - consuming task , and since radiation therapy of breast cancer represents a large part of the workload in our centers , we were interested in having an automated contouring procedure . 
 according to icru , dose prescription and dose reporting is done to the planning target volume ( ptv ) , which is created by adding a margin for setup and motion uncertainty to the ctv [ 13 ]  . 
by adding a margin , the ptv expands across the skin and contains a volume of air besides tissues of the patient , which complicates the dose prescription and the dose computation . 
in addition , such a ptv , containing a volume of air outside the patients surface , is unsuitable for computer optimization of the dose distribution , a problem well known in the field of intensity - modulated radiotherapy ( imrt ) [ 3 , 6 ]  . 
for 3 - d optimization of the dose distribution , we propose the concept of a plan optimization volume ( pov ) which is the ptv minus its regions that are located in air or close to the patients body surface , in the initial part of the buildup region of the photon beams . 
 the aims of this study were to ( 1 ) write the computer tool for automatic pov delineation , ( 2 ) incorporate this tool into the simulation and planning procedures for optimization of the weights of wedged and unwedged parts of the tangential beams , and ( 3 ) evaluate the performance of the pov tool on the planning ct scans of 43 consecutive patients . 
 simulation and image data acquisition the patients are placed on a simulator in supine position with the ipsilateral arm elevated 90 and with the palm of the hand in the dorsal neck and the head turned toward the opposite direction , as described previously [ 4 ]  . 
the precision of placement of the lead collar varies between patients and is dependent on the resistance to breast tissue on palpation and on the presence of folds between breast and thoracic wall . 
next , the collar beam data is added and its aperture is drawn according to the beams eye view ( bev ) projection of the lead collar on the radiograph using a graphic tablet . 
 der in cranial as well as in caudal direction was covered , using a slice thickness and spacing of 1.0 cthe scanned volume contains the entire volume of the lungs . 
in order to accomplish this , the pov is shrunk to a specified distance from the skin , to prevent problems when optimizing in dose buildup zones ; a distance to the beam borders , to avoid penumbra ; and a distance to the lung , to prevent the optimizing process to generate high doses too close to this organ at risk ( oar )  . 
they maintain a distance of 1.0 cm away from the edge of the tangential beams to avoid influence of beam penumbra on the pov edges and the lungs , and a distance of 0.5 cm to the skat a depth of 0.5 cm in water , the dose is > 80% of the dose maximum for 6 - mv photon beams of 10 10 cm or 20 20 cm field size on our accelerators [ 21 ]  . 
 the pov and irradiated volume ( iv ) are generated by a single algorithm which takes as input the transverse contours of skin and lung , the edges of the tangential beams and the position of the collar beam as projected in the radiograph . 
 the part of this zone that is not in the pov ( i.e. , the part outside the collar beam ) will form a penalty zone in the planning optimization , to prevent hot spots outside the pov . 
point a is the most lateral point of the expanded lung ; point b is the point on the anterior region of the expanded lung that is the most distant from the interior shrunken beam line . 
2 urban & vogel step of the procedure was timed and rounded up to 1 min except for the automatic weight assignment by cmi , which took significantly less ( 5 s )  . 
 the evaluation of the three plans was done using indices for dose homogeneity , defined as dmax dmin , dmedian inside the pov and for overdosage anywhere inside the iv . 
in guh , this algorithm is implemented on a dec alpha 433 - mhz single processor system , running the plunc planning system ( planunc , university of north carolina , chapel hill , nc , usa )  . 
one entire pov generation of 30 slices takes about 60 s of the central processing unit ( cpu ) time , the time being a function of the number of points each contour contains and the number of slices . 
 planning study design 43 breast cancer patients were referred to the radiotherapy department after tumorectomy for breast cancer tangential fields only , to make the additional simulator radiograph of the collar beam and to use the imaging material ( simulator radiographs and ct scan ) for study purposes . 
at the planning platform the previously described planning operations were performed , including generation of pov and iv , and the heart was contoured ( manually ) in order to compute dose - volume histogram ( dvh ) statistics . 
dose computation was performed with 6 - mv photons , using the convolution - superposition algorithm of the adac pinnacle system ( philips medical systems , the netherlands ) , based on the hounsfield units obtained from ct scanning . 
the weights of the wedged and unwedged segments ( coming from the tangential beams ) were assigned in three different ways : ( cid : 127 ) by a procedure of human trial and error using overlays of the dose distribution on the central slice only ( 2 - d user optimization , resulting in a 2 - d plan )  . 
 ( cid : 127 ) by a standard clinical procedure involving human trial and error using overlays of the isodose lines on the ct slices with the aim to obtain the most acceptable dose distribution . 
multiple slices were evaluated ( 3 - d user optimization , resulting in the 3 - d plan )  . ( cid : 127 ) using the computer - based algorithm cmi [ 7 ] , resulting in the pov plan . 
step 3 : the thin lines represent skin and lung , thick lines represent expansion of lung and shrinkage of skthe dark shaded area is the result of consecutive steps in the creation of the pov . 
step 4 : the hatched area is the organ region to be spared ; this is an expanded region ( margin : dlung ) including the lungs and the heart . 
 various planning steps various planning methods 2 - d planning 3 - d planning pov planning simulation virtual simulator target volume delineation dose calculation on pinnacle optimization total time adding two unwedged tangential and two wedged tangential beams adding two unwedged tangential and two wedged tangential beams and one collar beam freehand ctv drawing pov and iv generation user optimization automated optimization using cmi 20 3 min 4 1 min n / a 10 2 min n / a 15 2 min 3 1 min n / a 52 9 min 20 3 min 4 1 min n / a 10 2 min n / a 15 2 min 3 1 min n / a 52 9 min 22 3 min n / a 6 1 min 1 1 min 15 2 min 3 2 s 44 7 min processes have increased in time due to the additional simulation of the collar beam , but the steps downstream can be accelerated due to the reduction of human interaction . 
 4 / 43 4 / 43 the aim of this study was to automate the generation and use of the total breast volume both as clinical target volume ( ctv ) and for optimization of dose homogeneity by cmi [ 7 ]  . 
automated 3 - d optimization for breast cancer therapy not surprising that a large interand intraobserver variation was found in a ct scan - based delineation study of the breast [ 12 ]  . 
to avoid unwanted effects of dose in buildup regions , a separate pov volume was used , defined as the ctv minus the volume that was located < 0.5 cm to the skin surface . 
 the geometric accuracy of the procedure is critically dependent on the placement of the lead collar beawith the 3 - d procedure , the risk of geographic miss is lower than with a 2 - d procedure , since in the latter only a few slices were inspected at plan evaluation , while with the 3 - d procedure all slices are inspected . 
no significant difference was found when comparing the results of the automated procedure to the 2 - d and 3 - d planning procedures ; the resulting dose distributions were at least as good as those obtained by an experienced planner . 
 when looking critically at the three planning methods the reader can conclude that there is no dosimetric gain of the pov method over the ( user interactive ) 2 - d / 3 - d planning methods executed by experienced planners . 
dose homogeneity is limited by the physical properties of the photon beams and with only four parameters to optimize ( weights of wedged and unwedged beams ) , a close to optimal solution can be found by human heuristics in a short time . 
 in order to use the pov for imrt planning , a method has to be applied that ensures adequate doses in the buildup region in the presence of setup error . 
 conclusion it can be stated that this automated planning method is capable of replacing the contouring of the ctv as well as the trial - and - error procedure of assigning weights of wedged and unwedged beams , with results matching the manual procedure executed by an experienced planner . 
 strahlentherapie und onkologie case study vacuum application increases therapeutic safety and allows intensified local radiation treatment of malignant soft - tissue tumors jrgen kopp1 , vratislav strnad2 , alexander d . 
horch1 purpose : in order to simplify and improve outcome of radiation therapy and final defect coverage in patients suffering from invasive soft - tissue tumors , brachytherapy and application of v.a.c.uum - assisted closure ( v.a.c. ) were combined with delaying flap incision . patients and methods : two patients were excised as radically as possible and brachytherapy tubes were implanted directly on the tumor bed . 
brachytherapy and external - beam irradiation were performed directly on the vacuum sponge followed by subsequent defect coverage with the preconditioned flaps . results : excision significantly reduced tumor masses in both patients ; in one case sensible and motor function of the involved extremity was clearly improved . 
exact placement of tubes on the tumor bed without subsequent tissue coverage is conserving preconditioned flap tissues , which are transposed for final defect coverage at the end of radiotherapy . 
however , by circumventing radiation exposure of these tissues , a possible later irradiation sequence can be performed without endangering defect - covering flaps . key words : brachytherapy vacuum - assisted closure tissue preconditioning flap surgery strahlenther onkol 2005 ; 181 : 12430 doi 10.1007 / s00066 - 005 - 1291 - 0 vakuumapplikation erhht die therapeutische sicherheit und erlaubt die intensivierte lokale bestrahlungsbehandlung maligner weichteiltumoren ziel : zur vereinfachung und verbesserung radiotherapeutischer strategien bei der behandlung invasiv wachsender weichgewebetumoren wurde die gemeinsame anwendung von brachytherapie und vakuumversiegelung ( v.a.c. ) mit der technik der chirurgischen lappenprkonditionierung kombiniert . patienten und methodik : bei zwei patienten wurde so radikal wie mglich reseziert . 
anschlieend erfolgte die defektdeckung mit den prkonditionierten weichgewebelappen . ergebnisse : die exzisionen reduzierten die jeweilige tumormasse erheblich und resultierten in einem fall in einer deutlichen verbesserung von motorik und sensibilitt an der betroffenen extremitt . 
die wiederholte radiatio hatte keinen effekt auf die benachbarten , prkonditionierten lappengewebe , welche nach einschwenken in den jeweiligen defekt ohne strung einheilten . schlussfolgerung : die kombination von vakuumund brachytherapie kann die umstndliche und aufwendige anwendung einer intraoperativen bestrahlung ( iort ) effektiv ersetzen . 
die exakte platzierung der bestrahlungsrhren ohne nachfolgende defekt1 department of plastic and hand surgery , university medical center erlangen - nuremberg , erlangen , germany , 2 department of radiation therapy , university medical center erlangen - nuremberg , erlangen , germany . received : march 1 , 2004 ; accepted : july 23 , 2004 strahlenther onkol 2005 no . 
da eine strahlenexposition dieser gewebe umgangen wird , kann eine spter erforderliche bestrahlung durchgefhrt werden , ohne die lappengewebe dabei zu gefhrden . schlsselwrter : brachytherapie vakuumtherapie gewebeprkonditionierung lappenchirurgie fractions and in patient 2 with a dose of 9 gy in three fractions as boost . 
in this second patient radiation therapy was continued with simultaneous chemoradiation ( external - beam therapy with a total dose of 63 gy [ 1.5 - gy fraction , 2 / day ] and ifosfamide 1.5 g / m2 days 15 and 2933 and adriamycin 50 mg / m2 days 2 and 30 )  . results case report 1 a 36 - year - old patient presented herself with the second relapse of an aggressive dt situated in the left gluteal region . 
therefore , in a introduction optimizing the management of patients suffering from malignant and aggressive semimalignant soft - tissue tumors with high risk of recurrence continues to be a challenge . 
 additionally , we propose an algorithm of therapy concluded from our preliminary experiences . patients and methods two patients ( both female , 36 and 69 years , respectively ) suffering from fibrous soft - tissue tumors were excised as radically as possible . 
following excision , the plastic afterloading tubes were sutured in the region of close or positive resection margins , as far as possible parallel and equidistant to each other , either in freehand technique or , if necessary , using a flab for fixation of tubes . 
the dose specification was chosen for the desmoid tumor ( dt ) patient using a flab on the resection surface flab surface ( figure 2a ) and for the patient with malignant fibrous histiocytoma ( mfh ) on the 85% isodose . 
afterwards , transposed high - dose - rate ( hdr ) brachytherapy was done in patient 1 as brachytherapy alone with a total dose of 36 gy in nine tissue figure 1 . 
im nchsten schritt wird ein v.a.c. - schwamm in den defekt eingelegt ( b ) , anschlieend mit einer durchsichtigen folie bedeckt und an die v.a.c. - pumpe angeschlossen ( c )  . 
2 tage nach der flab - implantation ist die patientin vollstndig mobilisiert . fixed on the resection surface using a flab and covered with a polyurethane sponge subjected to 125 mmhg negative - pressure v.a.c. 
additionally , a tensor fasciae latae ( tfl ) flap [ 10 , 11 ] was elevated on the lateral border of the defect to precondition the flap tissues for final future defect closure . 
during the following 5 days a total dose of 36 gy was applied by using hdr brachytherapy directly onto the surface of the tumor resection area ( figure 2a ; for more details see patients and methods ) , which was covered with the v.a.c. 
the postoperative course was uneventful , and the patient was discharged from our department 7 days later with properly healing wounds , that have remained stable for > 6 months now . case report 2 in order to achieve a maximal local radiation protection of surrounding healthy tissues during both brachytherapy and external - beam therapy , twelve afterloading tubes were a 69 - year - old patient presented with an mfh of her right hip and minor pelvis , inguinal region and right anterior thigh . 
several attempts to surgically excise the tumor had been without any success , and the oncologic surgeons had declared that due to the intensive local invasion of vital structures the tumor was not resectable . 
it was decided with the patients approval to palliatively reduce the tumor mass by surgery followed by subsequent brachytherapy , conventional high - dose irradiation and chemotherapy to improve quality of life . 
a myocutaneous vertical rectus abdominis ( vram ) flap , pedicled at the right inferior epigastric artery , was circumcised and laid back into the harvesting defect for preconditioning ( figure 8 )  . 
this operation resulted in a markedly improved motor and sensible condition of the right upper leg , allowing the patient to ambulate aga during the following week hdr brachytherapy with 9 gy was applied subsequently pursued by 6 figure 5 . 
additionally , the patient was subjected to simultaneous chemotherapy with ifosfamide and adriamycin in the 1st and 5th week of therapy ( for more details see patients and methods ) while v.a.c. 
 there is strong evidence that adjuvant radiotherapy is indicated in patients with negative , marginal or minimal microscopically positive surgical margins , as demonstrated in case report 2 [ 24 ]  . 
 iort , which has become an effective tool in the treatment of various malignancies [ 25 , 7 , 8 , 12 , 15 , 16 , 19 , 20 , 22 , 23 , 25 , 26 ] , has also proven to be valuable in patients suffering from mfh . 
although highly effective , its application implicates considerable disadvantages like additional architectural measures , high purchase and maintenance costs , the need for specialized staff ; its limiting stationary operation results in circumstantial operating procedures and therapy management . 
additionally , problems with rigid electron applicators and tube misalignment are well known as further drawbacks , thus restricting iort installations to certain centers [ 13 , 14 ]  . 
 since brachytherapy has been introduced to treat invasive soft - tissue tumors , minimally invasive and exact - to - the - point application of therapeutic irradiation may prevent surrounding tissues and organs from impairment by implanting guide gutters and prefabricated plastic templates to ensure parallelism and equidistance of sources . 
 thereby , brachytherapy is circumventing iort drawbacks and hence favorable to iort in the selection of radiotherapeutic methods when required . following our newly introduced concept a definite wound closure can be achieved more safely in a two - stage operation . 
thus , in a secondary procedure , definitive harvesting of the flap and subsequent definitive wound closure are achieved with a nonirradiated soft tissue and with increased safety of tissue oxygenation through the previous delay . application of negative pressure in impaired wounds has been demonstrated valuable to improve healing conditions . 
whereas in traumatic and chronic wounds these procedures represent the state of the art in plastic surgical approaches to cover extensive soft - tissue defects , irradiated sites are much more difficult to handle since irradiation of the tumor bed and accompanying chemotherapy result in severely impaired wound - healing conditions [ 9 ]  . taking advantage of the combination of both techniques in order to improve the therapeutic outcome in patients with semimalignant and malignant soft - tissue tumors seems at hand . 
coverage the patient is mobile immediately and can easily be transferred to the radiation department , thereby avoiding the costly installation of an iort facility , allowing high - dose local radiotherapy . 
 strahlentherapie strahlentherapie und onkologie und onkologie original article original article phase i / ii trial of simultaneous whole - brain irradiation and dose - escalating topotecan for brain metastases martin kocher , hans - theodor eich , robert semrau , semi aykut gner , rolf - peter mller1 background and purpose : topotecan penetrates the blood - brain barrier and sensitizes tumor cells against radiation . 
topotecan application simultaneously with whole - brain irradiation ( wbrt ) was conducted to estimate toxicity , maximum tolerated dose and survival in patients with inoperable brain metastases . patients and methods : in 47 patients suffering from previously untreated brain metastases , topotecan was applied on a daily i.v. 
response evaluation was possible in 26 / 47 patients , overall response rate was 58% ( cr [ complete remission ] 5 / 26 , pr [ partial remission ] 10 / 26 , nc [ no change ] 8 / 26 )  . 
in 15 / 42 patients ( 36% ) , brain metastases were the dominant cause of death . conclusion : for a daily topotecan schedule simultaneous to wbrt , the maximum tolerated dose is 12 0.5 mg / m2 in chemonaive patients . 
a phase iii trial has now been started to find out whether wbrt + topotecan increases survival compared to wbrt alone . key words : brain metastases whole - brain radiotherapy combined radiochemotherapy topoisomerase i inhibitor topotecan strahlenther onkol 2005 ; 181 : 205 doi 10.1007 / s00066 - 005 - 1242 - 9 phase - i / ii - studie zur simultanen ganzhirnbestrahlung mit dosiseskaliertem topotecan bei hirnmetastasen hintergrund und ziel : topotecan , ein topoisomeraseinhibitor , gehrt zu den wenigen substanzen , die die blut - hirn - schranke durchdringen und tumorzellen gegenber ionisierender strahlung sensibilisieren . 
untersucht wurden toxizitt , maximal tolerable dosis , ansprechen der hirnmetastasen und berlebenszeit . patienten und methodik : bei 47 patienten mit unvorbehandelten hirnmetastasen wurde eine palliative ganzhirnbestrahlung mit 36 gy / 3 gy mit einer tglichen kurzinfusion von topotecan 12 h vor der bestrahlung kombiniert . 
die topotecandosis wurde wie folgt eskaliert : 5 0 , 5 mg / m2 , 8 0 , 5 mg / m2 , 12 0 , 5 mg / m2 , 12 0 , 6 mg / m2 . ergebnisse : insgesamt konnte bei 38 / 47 patienten ( 81% ) die therapie wie vorgesehen durchgefhrt werden . 
eine hmatotoxizitt grad 3 / 4 trat bei 5 / 32 chemotherapeutisch unvorbehandelten patienten ( 16% ) und bei 7 / 15 patienten ( 47% ) auf , die bereits zuvor eine chemotherapie erhalten hatten . 
bei 26 / 47 patienten konnte das ansprechen beurteilt werden ; die ansprechrate lag bei 58% ( cr [ komplette remission ] 5 / 26 , pr [ partielle remission ] 10 / 26 , nc [ stabile erkrankung ] 8 / 26 )  . 
 schlsselwrter : hirnmetastasen ganzhirnbestrahlung kombinierte radiochemotherapie topoisomerase - i - hemmer topotecan 1 department of radiation oncology , university hospital , university of cologne , cologne , germany . received : october 2 , 2003 ; accepted : july 23 , 2004 strahlenther onkol 2005 no . 
while surgery [ 31 ] and radiosurgery [ 10 , 13 ] are efficient only in selected subgroups , most patients can only be treated by palliative whole - brain irradition ( wbrt ) with overall response rates of about 5060% and median survival times of 34 months [ 3 , 5 , 6 ]  . 
due to the limited tolerance of the normal brain tissue to radiation and a shallow radiation dose - response curve [ 24 ] , increased doses of radiation have failed to improve outcome . 
therefore , we evaluated the use of topotecan , a topoisomerase i inhibitor , which has been shown to penetrate the intact blood - brain barrier [ 2 , 35 ] and to sensitize tumor cells against radiation [ 12 , 17 , 33 ]  . 
toxicity and effectiveness were examined in a dose - escalating phase ii trial where topotecan was infused daily before the radiation fractions in order to allow for a maximum of interaction between the damage - repair processes induced by radiation and the topoisomerase i inhibition . 
preliminary results of this study have been published earlier [ 14 ]  . patients and methods dose - finding pilot study from 1996 to 2002 , 47 patients with newly diagnosed brain metastases of various primary cancers were treated with wbrt and simultaneous topotecan . 
patients who fulfilled the institutions standard criteria for receiving wbrt ( irresectable brain metastases unsuitable for radiosurgery , histological proof of malignant disease , no prior irradiation to the brain , karnofsky performance score of 50 ) and who had sufficient bone marrow function ( leukocytes 4 , 000 / l , thrombocytes 100 , 000 / l , hemoglobin 9 g / dl ) and normal renal function ( serum creatine levels ) were included , irrespective of prior chemotherapy . 
wbrt was applied according to the usual irradiation technique and fractionation scheme in the institution , 36 gy in twelve fractions of 3 gy referred to the midplane using opposing fields . 
 phase ii dose - escalating study resembled those for the dose - finding study ( irresectable brain metastases unsuitable for radiosurgery , histological proof of malignant disease , no prior irradiation to the brain , leukocytes 4 , 000 / l , thrombocytes 100 , 000 / l , hemoglobin 9 g / dl and normal renal function , prior chemotherapy allowed ) , but only patients with a performance score ( karnofsky ) 70% were included . 
in general , wbrt was applied using 36 gy in twelve daily fractions of 3 gy , but as in the dose - finding protocol , patients with a pronounced brain edema were given 4050 gy in 2025 fractions of 2 gy . 
 the protocol prescribed a dose increase in steps of 0.1 mg / m2 , starting at a dose level of 12 0.5 mg / m2 which was found to be safe in the dose - finding study . 
in case that one of the three patients experienced a grade 4 toxicity , up to another three patients had to be treated at this dose level until another grade 4 toxicity was observed . 
partial remission ( pr ) was supposed , if the estimated total volume of the metastases ( estimated from two perpendicular diameters ) or the total number of metastases was reduced by at least 50% . 
response , survival time , cause of death and toxicities were recorded and evaluated using the spss 11.0 ( statistical package for the social sciences , chicago , il , usa ) software package . 
 consecutively , a phase ii dose - escalating protocol was started that aimed to evaluate the maximum tolerated dose ( mtd ) of topotecan when given in twelve daily doses . 
 results dose - finding pilot study during the pilot phase ( n = 14 ) with topotecan doses of 5 0.5 mg / m2 ( n = 5 ) , 8 0.5 mg / m2 ( n = 5 ) , and 12 0.5 mg / m2 ( n = 4 ) , one patient who received 8 0.5 mg / m2 developed a grade 4 thrombopenia synchronously to a disseminated intravascular coagulation syndrome . 
 phase ii dose - escalating study the phase ii study was started with 12 0.5 mg / m2 in three patients without grade 4 toxicity and continued with 12 0.6 mg / m2 in three patients , one of whom developed grade 4 leukopenia and thrombopenia . 
the first of the scheduled next three patients also experienced grade 4 leukopenia / thrombopenia ; thus , a total of two out of four patients were affected , and one of the two patients with leukopenia died from poststenotic pneumonia within 3 weeks . 
in consequence , another 18 patients ( instead of the planned 20 ) were treated in the phase ii protocol at this dose level until the closing date of the protocol . 
the reasons for not completing the scheduled therapy in nine patients were : leukopenia / fever / infection ( n = 4 ) , tumor progression ( n = 2 ) , myocardial infarction ( n = 1 ) , non - compliance ( n = 1 ) , administrative failure ( n = 1 )  . 
there was no indication of neurologic toxicity caused by topotecan [ 26 ]  . outcome median survival of all patients was 5.1 months ; five patients are still alive at a median follow - up of 11 months ( figure 2 )  . 
 survival data were compared to both a historical collective of the same institution ( n = 207 , 19771991 ) and to the patients treated in the rtog recursive partitioning analysis ( rpa )  . 
it has , however , been questioned whether the rpa keeps its prognostic power in patients with more than three metastases [ 23 ] , to which group 66% of the present patients belong . 
the main dose - limiting toxicity was leukopenia , and the mtd in chemonaive patients was 12 0.5 mg / m2 , resulting in 16% grade 3 / 4 hematotoxicity . 
for patients with prior chemotherapy , the dose should be reduced , because 6 / 12 ( 50% ) had a grade 3 / 4 leukopenia / thrombopenia at this dose level . 
although no clear recommendation can be made , a reduction to daily doses of 0.4 mg / m2 ( dose intensity reduction by 20% ) should allow to detect severe hemototoxicities and stop topotecan infusion early enough in the radiochemotherapy course . 
oral mucositis grade 12 ( n = 3 ) was possibly caused by topotecan , while oral thrush ( n = 4 ) seems to relate to the use of high - dose dexamethasone . 
 the finding that topotecan given as a single drug has some activity in brain metastases of small cell lung cancer [ 15 ] and breast cancer [ 25 ] , and the observation that it penetrates the chemonaive prior chemotherapy 6 / 12 3 / 21 5 0.5 mg / m2 8 0.5 mg / m2 12 0.5 mg / m2 12 0.6 mg / m2 topotecan figure 1 . 
frequency of any grade 3 / 4 hematologic toxicity ( number of affected patients / total number of patients in each dose group ) in patients without and with prior chemotherapy during daily infusion of topotecan simultaneously with whole - brain irradiation . 
 blood - brain barrier [ 2 , 35 ] and sensitizes tumor cells against radiation [ 12 , 17 ] has stimulated several phase i / ii trials which evaluated the use of combined radiochemotherapy with topotecan for brain metastases . 
 grade 1 / 2 3 symptoms of increased intracranial pressure asthenia , depression , general weekness oral thrush oral mucositis cushing fever / pneumonia deep vein thrombosis emesis coagulation ( disseminated intravascular coagulation ) 0 0 0 0 0 1 0 0 strahlenther onkol 2005 no . 
again , the mtd was 0.4 mg / m2 / d , the overall response rate amounted to 57% , and a median survival time of 5 months was achieved . 
 [ 20 ] treated seven patients with primarily diagnosed or recurrent brain metastases with twelve to 18 daily doses of 0.5 mg / m2 and observed two grade 3 hematotoxicities and 4 / 6 prs . 
 while some effort has been undertaken to evaluate the effectiveness of chemotherapy alone in patients with brain metastases [ 4 , 11 , 22 , 28 , 32 ] , approaches that investigated concurrent radiochemotherapy have been rare [ 6 , 9 , 16 , 21 ]  . 
in the latter scheme that also used high radiation doses ( 54 gy ) , objective response rates of 56% and median survival times of 8 months were found , but chemotherapy produced unacceptable hematotoxicity . 
survival analysis ( median survival time ) for patients treated with whole - brain irradiation ( wbrt ) and topotecan , compared to the rtog group and to a historical group of the institution , both treated with wbrt alone . 
berlebensanalyse ( mediane berlebenszeit ) der patienten , die mit einer ganzhirnbestrahlung ( wbrt ) in kombination mit topotecan behandelt wurden , im vergleich zu den patienten aus der rtog - analyse ( alleinige wbrt ) und zu einer gruppe von patienten , die in kln ebenfalls eine alleinige wbrt erhalten hatten . 
 [ 1 ] treated patients with multiple brain metastases with wbrt and applied concurrent and adjuvant temozolomide in the investigational arresponse rate was increased from 67% to 96% , and a marked neurologic improvement was observed . 
 besides overall survival , the duration of functional independence , e.g. , the survival time with acceptable quality of life , and the freedom from cerebral death should be evaluated . 
 a phase iii trial supported by the german cancer society ( deutsche krebsgesellschaft ) comparing wbrt with daily topotecan to wbrt alone in lung cancer patients has now been started . 
the authors compared the efficacy of two regimens in 210 stage iiaiiib cervical cancer patients : sequential radiation therapy ( srt ) with 4 8 gy high - dose - rate brachytherapy ( hdr - bt ) to point a followed by external - beam radiotherapy ( ebrt ) , and continuous irradiation ( crt ) in which 5 6 gy hdr - bt to point a administered weekly was integrated with ebrt ( ebrt was omitted on the day of bt )  . 
moreover , prolonged ott is considered a factor attributed to the outcome of the only negative randomized trial of weekly cisplatin in addition to rt [ 3 , 5 ]  . in the study by mayer et al . 
additionally , administering bt in srt before ebrt might also have influenced the outcome , particularly in stage iiib tumors [ 4 ]  . the authors stated that the ott in the crt group was the shortest possible ( 35 days ) which could be found in the literature , which is incorrect . 
in our study , only eleven of the 28 strahlenther onkol 2005 ; 181 : 54 doi 10.1007 / s00066 - 005 - 9122 - x evaluable patients ( 39% ) completed treatment within the prescribed ott ( 45% and 35% for groups a and b , respectively ) , and 17 had unplanned treatment breaks , almost in all cases due to treatment toxicity . 
 [ 1 ] reported a retrospective series of cervical cancer patients irradiated up to 7 weeks ( including weekend ldr - bt insertions ) to a total point a dose of 60 gy . 
they found a significantly increased incidence of serious late morbidity in the shortest treatment group ( 23% at 5 years grade 4 morbidity in patients treated within 2932 days with only 4 radiotherapy - free days )  . 
importantly , also in this series no significant effect of ott on the cause - specific survival was found . thus , shortening the ott to < 35 days has been attempted in cervical cancer , yet without impressive results . 
 strahlentherapie und onkologie original article regional hyperthermia in conjunction with definitive radiotherapy against recurrent or locally advanced prostate cancer t3 pn0 m0 wolfgang tilly1 , johanna gellermann1 , reinhold graf1 , bert hildebrandt2 , lothar weibach3 , volker budach4 , roland felix1 , peter wust1 background and purpose : since long - term results of the standard treatment of locally advanced or recurrent prostatic carcinoma are unsatisfactory , the role for additional regional hyperthermia was evaluated in a phase i / ii study . patients and methods : from 08 / 1996 to 03 / 2000 , 22 patients were treated by a standard irradiation regimen ( 68.4 gy ) in combination with regional hyperthermia ( weekly , five to six times ) , and five of 22 patients received short - term ( neoadjuvant ) hormonal treatment . 
feasibility of hyperthermia , and acute / late toxicity as well as long - term follow - up ( prostate - specific antigen [ psa ] control , overall survival ) were analyzed . 
severe acute toxicity of grade 3 occurred at the rectum in three , at the urethra in four , at the intestine in one , and a burn induced by hyperthermia in one of 22 patients . 
 key words : regional hyperthermia prostate carcinoma psa control strahlenther onkol 2005 ; 181 : 3541 doi 10.1007 / s00066 - 005 - 1296 - 8 definitive externe radiotherapie mit regionaler hyperthermie beim lokal fortgeschrittenen oder rezidivierten prostatakarzinom stadium t3pn0m0 hintergrund und ziel : die langzeitergebnisse der standardtherapie beim lokal fortgeschrittenen oder rezidivierten prostatakarzinom sind unbefriedigend . 
daher wurde eine zustzliche regionale hyperthermie in einer phase - i / ii - studie evaluiert . patienten und methodik : von 08 / 1996 bis 03 / 2000 wurden 22 patienten mit einer standardradiotherapie von 68 , 4 gy in kombination mit regionaler hyperthermie ( wchentlich , fnf bis sechs sitzungen ) behandelt . 
die klinischen endpunkte wurden mit thermischen parametern korreliert . ergebnisse : es konnten mittlere maximaltemperaturen entlang der urethra von 41 , 4 c ( 41 , 0 c fr die rezidive ) sowie mittlere t90 von 40 , 7 c erreicht werden . 
schwere akute nebenwirkungen vom grad 3 traten am rektum bei drei , an der urethra bei vier , am dnndarm bei einem sowie durch hyperthermie bedingt ( verbrennung ) bei einem von 22 patienten auf . 
thermischen dosen und der langfristigen psa - kontrolle . 1 department of radiation medicine , charit medical school , berlin , germany , 2 department of internal medicine hematology and oncology , charit medical school , berlin , germany , 3 department of urology , urban hospital , berlin , germany , 4 department of radiation oncology , charit medical school , berlin , germany . received : march 11 , 2004 ; accepted : july 2 , 2004 strahlenther onkol 2005 no . 
hier ist eine weitere evaluation sinnvoll , insbesondere auch unter anwendung verbesserter hyperthermietechnologien . schlsselwrter : regionale hyperthermie prostatakarzinom psa - kontrolle introduction for locally advanced prostate cancer ct3 / 4 with cn0 or pn0 , external - beam radiotherapy ( ebrt ) is accepted as standard treatment . 
reports with large numbers of t3 carcinomas describe a 5 - year prostate - specific antigen ( psa ) relapse - free survival of only 3040% paralleled by considerable rates of local recurrences in the range of 20% [ 12 , 24 ]  . 
therefore , taking the peri - / postoperative morbidity into account , ebrt is widely favored . however , in t3 / t4 tumors definitive radiotherapy alone with standard doses of about 72 gy is also inadequate . 
innovative strategies include dose escalation by intensity modulation , additive interstitial radiotherapy , and / or cytoreduction by hormonal manipulation , either neoadjuvant and / or adjuvant , for several years . 
nonetheless , these approaches could not improve the outcome , but imply some late normal tissue reactions . dose escalation with three - dimensional conformal irradiation led to an increased late rectal toxicity grade 2 , and in fact , investigators found a higher rate of proctitis grade 2 [ 19 , 22 ]  . 
long - term hormonal treatment causes specific side effects of the medication , impotency , and increased late reactions [ 8 ]  . there is currently no standard of care for locally advanced prostatic carcinoma . 
 external radiotherapy was performed with a linear accelerator ( siemens mevatron kd , 18 mv ) using fractions of 5 1.8 gy up to 68.4 gy at the reference point ( icru )  . 
a conformal four - field box technique was used . regional hyperthermia was carried out about 30 min before or after a single fraction once a week five to six times during the radiotherapy course as described elsewhere [ 29 ]  . 
 we used the sigma - 60 applicator of the bsd 2000 syste the midplane ( feed points of the antennas , central plane of the applicator ) was positioned a few centimeters cranial to the symphysis defining the longitudinal position [ 21 ]  . 
for the temperature - time curves in between , we left the point probe at the maximu we assume that these reference points for the temperature - time curves characterize the central part and the periphery of the prostate . 
using the temperature - time curves at the beginning ( power - on ) and at the end ( power - off ) of heat treatment , we could derive specific absorption rates ( sars ) in w / kg at the reference points . 
hyperthermia and definitive radiotherapy in prostate cancer in the measurement points ( attempting to achieve > 41.5 c ) , we increased or reduced the total power and , in particular , the weights at the dorsal or ventral channel or modified the phase delay . 
for the heat treatments we defined a toxicity score as follows : 0 no complaints or some discomfort by bolus pressure , thermal stress or positioning ; 1 power - dependent discomfort , which resolves completely at the end of heat treatment ; 2 hot spot sensation , which persists or occurs after the end of heat exposure and resolves in days or ( rarely ) weeks ; 3 burn or thermal lesion . 
local progression was defined according to who as macroscopic tumor growth of > 25% . all statistical analyses were conducted with spss software version 10 ( spss inc , chicago , il , usa )  . 
 69 years ( 5675 years ) age stage primary ct3a pno ct3b pn0 hormonal manipulation primary none neoadjuvant 6 grading primary recurrent rtx cno recurrent none recurrent psa primary < 10 ng / ml 10 20 ng / ml 4 > 20 ng / ml mean = 16.7 ng / ml recurrent < 10 ng / ml 10 20 ng / ml mean = 10.8 ng / ml table 2 . 
die spttoxizitt ( unten ) wurde nach dem lent - score klassifiziert ( sptwirkungen auf das normalgewebe ) [ 18 ]  . acute grade 0 grade 1 grade 2 grade 3 grade 4 rectum bladder / urethra intestine skin heat 2 3 5 1 3 5 8 4 2 late grade 1 grade 2 grade 3 / 4 gastroinestinal urogenital 2 / 20 ( 10% ) 1 / 20 ( 5% ) 2 / 20 ( 10% ) 1 / 20 ( 5% ) patient was comparable for both tumor entities . 
nevertheless , the temperatures achieved for recurrences are similar or even higher , which is probably based on a reduced perfusion and perfusion regulation capacity . table 2 illustrates that primary prostatic carcinomas are easier to heat than primary rectal carcinomas with higher relative sar and t90 ( for lower total power ) [ 21 , 23 ]  . 
only 14% grade 3 reactions at the rectum , 18% at the urethra ( dysuria ) , < 5% at the small intestine and hyperthermia - related ( burn ) , respectively , were observed . 
grade 2 reactions at the urethra or caused by heat ( persistent hot spot sensations ) are frequent ( 55% ) , but moderate urinary toxicity is common during radiotherapy . 
persistent hot spots ( muscle - skeletal pain syndrome ) heal within a few days or , at most , several weeks without any late morbidity . no correlation was observed between thermal parameters ( tmax , t90 ) and acute toxicity . 
however , this might be explained by an increased tolerance for more aggressive heating in cases of less radio - induced toxicity . late reactions ( see table 3 below ) were moderate . 
of these , only 5% had rectal toxicity grade 3 ( with permanent loss of mucus and urgency ) and 10% ( n = 2 / 20 ) suffered from long - term urinary reactions grade 2 ( intermittent urgency and dysuria )  . 
our analysis showed no correlation between thermal parameters and chronic toxicity . follow - up a subdivision of the clinical events according to death , psa failure , local progression , and distant metastases is shown in table 4 . 
berleben unter psa - kontrolle ( astro - konsensus , < 1 ng / ml ) bei primren karzinomen ( 15 patienten ) und rezidiven ( sieben patienten )  . 
in the group with psa control ( n = 8 ) significantly higher temperatures and thermal doses were achieved ( p - values of 0.010.02 ) in spite of the small number of patients . 
in fact , tmax was the only relevant predictive factor for psa control with five local psa failures for patients with tmax < 41.2 c and only one psa failure for tmax 41.2 c ( p = 0.037 , mann - whitney test )  . 
 even though the ( pretherapeutic ) psa value is well established as prognostic factor ( see , e.g. , [ 14 ] ) , the correlation between the initial psa and the psa control was not as high in this small group according to table 5 . 
the widespread therapeutic option was radiotherapy alone with radiation doses of 6670 gy resulting in a long - term psa control of only 30% for observation times > 5 years [ 31 ]  . 
psa control in a similar range is achieved for high - risk tumors ( e.g. , t3 / 4 ) by other groups applying standard radiotherapy , e.g. , a 5 - year psa control of 35% [ 28 ] or a 3 - year psa control of 60% [ 6 ]  . 
 alive psa progression progression metastases distant local primary n = 15 recurrent n = 7 4 monal treatment in patients with either lymphatic involvement ( pn + ) or clinical stage t3 ( palpable tumor infiltration beyond the capsula )  . 
rtog trial 92 - 02 , dealing with a patient group similar to ours ( t2ct4 tumors ) , found a biochemical control of 21% after 5 years in the reference arm with radiotherapy and neoadjuvant androgen suppression ( 2 months ) , while additional long - term androgen deprivation improved psa control to 46% [ 8 ]  . 
 an eortc trial [ 4 ] investigated a patient group of 415 men with locally advanced prostate cancer treated with either ebrt or radiotherapy and long - term androgen deprivation . 
univariate analysis of thermal parameters correlates the effectiveness of the heat treatments with the major clinical endpoint psa control ( for primary prostatic carcinoma , 14 patients alive )  . 
the one patient with metastatic disease was excluded from the thermal analysis ( n = 6 ) , which can only characterize local psa control , whereas the whole patient group is described by the initial psa value ( n = 7 )  . 
der patient mit metastasierender erkrankung wurde aus der thermischen analyse genommen ( n = 6 ) , da diese nur die lokale psa - kontrolle betrifft , whrend die gesamte patientengruppe ( n = 7 ) durch den initialen psa - wert beschrieben wurde . 
however , a summary of studies showed that the long - term biochemical control of the surgical approach is not superior to conservative treatments , achieving a psa control of < 40% [ 19 ] and even with postoperative radiotherapy of only 57% . 
 from these data we may conclude , that a combined and / or more aggressive treatment strategy can improve the 5 - year biochemical control of radiotherapy alone from 2040% up to slightly > 50% . 
 therefore , a careful evaluation of all treatment combinations with respect to toxicity is required . in our small series we gained a long - term psa control ( > 5 years ) of 50% , and an excellent overall survival of > 90% for primary locally advanced prostatic carcinoma t3 pn0 . 
they found after a shorter observation time a 3 - year biochemical control of 70% , which is fairly in agreement with our data ( see figure 1 )  . 
 conclusion regional hyperthermia is a very feasible and well - tolerated procedure , which might increase the local effectiveness of radiotherapy or any combination therapy against locally advanced prostate cancer . 
for example , standard radiotherapy plus regional hyperthermia might be as effective as standard radiotherapy plus long - term androgen suppression or a dose - escalated schedule , but less burdensome ( or less expensive )  . 
 acknowledgment this work has been supported by the lieselotte - beutel - stiftung , berl strahlentherapie und onkologie original article multimodality treatment including postoperative radiation and concurrent chemotherapy with weekly docetaxel is feasible and effective in patients with oral and oropharyngeal cancer adorjn f . 
bttcher2 , klaus bitter1 background : to examine the feasibility and efficacy of weekly docetaxel with concurrent radiation as postoperative treatment in a multimodality approach to oral and oropharyngeal cancer . 
 patients and methods : 94 patients ( table 1 ) with primary resectable squamous cell carcinoma of the oral cavity and oropharynx ( uicc stage i 14% , ii 15% , iii 18% , iv 53% ; table 2 ) were treated with a multimodality therapy program consisting of neoadjuvant intra - arterial high - dose chemotherapy ( cisplatin 150 mg / m2 with parallel systemic sodium thiosulfate 9 g / m2 for neutralization ) , followed by surgery of the primary and neck , and postoperative concurrent radiation and chemotherapy with weekly docetaxel ( 2030 mg / m2 ; table 3 )  . 
 results : at a median follow - up of 4 years , the 5 - year survival rate for all 94 patients was 80% , and disease - free survival was 73% ( figures 1 and 2 )  . 
 conclusions : concurrent radiation and chemotherapy with weekly docetaxel is a feasible postoperative treatment in a multimodality approach to oral and oropharyngeal cancer , resulting in high overall and disease - free survival . 
 key words : head and neck cancer docetaxel multimodal treatment adjuvant radiation strahlenther onkol 2005 ; 181 : 2634 doi 10.1007 / s00066 - 005 - 1272 - 3 multimodale therapie einschlielich postoperativer bestrahlung und konkomitanter wchentlicher chemotherapie mit docetaxel ist bei patienten mit mundhhlenund oropharynxkarzinomen durchfhrbar und effektiv hintergrund : untersuchung der durchfhrbarkeit und effektivitt einer wchentlichen docetaxelapplikation bei konkomitanter bestrahlung in einem multimodalen behandlungskonzept von mundhhlenund oropharynxkarzinomen . patienten und methoden : 94 patienten ( tabelle 1 ) mit primren resektablen plattenepithelkarzinomen der mundhhle und des oropharynx ( uicc - stadium i 14% , ii 15% , iii 18% , iv 53% ; tabelle 2 ) wurden mit einem multimodalen therapiekonzept behandelt , das aus einer neoadjuvanten intraarteriellen hochdosischemotherapie ( 150 mg / m2 cisplatin mit paralleler systemischer neutralisierung durch 9 g / m2 natriumthiosulfat ) , einer radikaloperation des primarius und des halses sowie einer postoperativen konkomitanten bestrahlung und chemotherapie mit wchentlicher docetaxelgabe ( 2030 mg / m2 ) bestand ( tabelle 3 )  . 
 ergebnisse : nach einem medianen follow - up von 4 jahren lag die 5 - jahres - berlebensrate aller 94 patienten bei 80% und das krankheitsfreie berleben bei 73% ( abbildungen 1 und 2 )  . 
 schlussfolgerungen : die konkomitante bestrahlung und chemotherapie mit wchentlicher docetaxelgabe ist eine durchfhrbare postoperative behandlung in einem multimodalen therapiekonzept fr mundhhlenund oropharynxkarzinome , die in einem hohen gesamtund krankheitsfreien berleben resultiert . 
 schlsselwrter : kopf - hals - karzinome docetaxel multimodale therapie adjuvante bestrahlung 1 department of maxillofacial plastic surgery , and 2 department of radiation therapy , johann wolfgang goethe university frankfurt am main medical school , frankfurt am main , germany . 
a potential advantage of preoperative radiation is that it is directed at tissues not altered by scarring , but there are also clear drawbacks : wound healing may be impaired , and neoadjuvant radiation is given with a uniform dose irrespective of particular unfavourable factors becoming evident at the surgical specimen due to exact pathologic staging . 
docetaxel is a potent radiosensitizer in vitro [ 14 , 30 , 39 ] and has proven very effective in the treatment of non - small - cell lung cancer ( nsclc )  . 
in several studies , docetaxel was used at weekly doses between 15 mg / m2 and 30 mg / m2 with concomitant radiation up to 70 gy [ 16 , 21 , 40 ] ; these trials included patients with advanced inoperable tumors . 
in three phase ii studies , docetaxel - based regimens given as induction therapy to patients with locally advanced squamous - cell carcinoma ( scc ) of the head and neck yielded overall response rates from 93% to 100% , with complete response rates of 40% to 63% [ 29 ]  . 
 the present report describes the results of a phase ii study of docetaxel given as part of a novel postoperative chemoradiation protocol for the curative treatment of head and neck cancer . 
patients with the following were excluded from the study : age > 80 years , known hypersensitivity to cisplatin or docetaxel , severely impaired renal or hepatic function ( serum creatinine > 5 mg / dl as sign for a beginning renal insufficiency , serum bilirubin > 1.3 mg / dl and / or transaminases > 3.5 times the upper limit of normal ) , distant metastases or synchronous malignancies . 
 treatment treatment consisted of three parts : ( 1 ) neoadjuvant superselective intra - arterial chemotherapy with cisplatin given to the primary , with concomitant systemic sodium thiosulfate for neutralization , followed by ( 2 ) surgery and ( 3 ) adjuvant chemoradiation with weekly doses of docetaxel . 
treatment was initiated with one cycle of preoperative intra - arterial highdose cisplatin at 150 mg / m2 given on an inpatient basis ( hospital admission for 46 days due to health care system guidelines )  . 
if a near to complete partial response was achieved , as determined by clinical examination and ct scan , one or two additional cycles of intra - arterial cisplatin were given 3 weeks apart . 
 ( the maximum number of cycles was restricted to three . ) on day 1 of each neoadjuvant chemotherapy cycle , patients received hyperhydration and other supportive measures as described elsewhere [ 22 ]  . 
using a transfemoral approach , a 4 - french catheter containing a coaxial micro - catheter for superselective visualization of the tumor - feeding vessel by means of fluoroscopy and contrast medium was inserted , and cisplatin ( medac gmbh , wedel , germany ) at a dose of 150 mg / m2 ( maximum absolute dose , 300 mg ) and diluted in 500 ml of 0.9% saline solution was infused at controlled pressure ( 2 ml / s )  . 
10 s after initiation of the cisplatin infusion , a concomitant intravenous infusion of 9 g / m of sodium thiosulfate was started and continued for the duration of intra - arterial cisplatin administration . 
adjuvant chemoradiation in head and neck cancer routine laboratory studies were performed on alternate days after the start of neoadjuvant treatment , and toxicity was graded using who criteria [ 27 ]  . 
since significant downstaging of the tumor was not considered a realistic aim of induction chemotherapy , all resections were intended to include tumor - free margins based on the tumor extension prior to therapy ( which was also recorded on photographs )  . 
surgical treatment was carried out according to the guidelines of the german - austrian - swiss cooperative group on tumors of the maxillofacial region ( dsak ) [ 5 ] , with two important modifications . 
first , patients with n0 disease after baseline staging including pet underwent only ipsilateral suprahyoid neck dissection ( a selective neck dissection including levels i and ii ) , irrespective of the localization and size of the primary tumor . 
second , a radical neck dissection was carried out only in cases of fixed lymph nodes ; in all other cases of lymph node involvement at baseline , and independent of the side , a type iii modified radical neck dissection was performed . 
if the histological examination of the dissection material revealed a positive finding despite baseline n0 staging , a lower neck dissection that included levels iii to v was performed as soon as possible to eventually result in a modified radical neck dissection . 
the classification of neck levels and types of operations followed the proposal of the committee for neck dissection classification of the american head and neck society [ 31 ]  . 
the last treatment step involved weekly irradiation of the primary and lymphatic drainage area and concurrent systemic administration of docetaxel ( aventis pharma s.a. , antony cedex , france )  . 
if microscopic local tumor residues were detected at the surgical margin at primary surgery , an additional boost of 10 gy was delivered ; in case of infiltration of a surgical margin at the additional resection , a boost of 20 gy ( 5 / week , 2.0 gy / day ) was delivered to these selected local areas , respectively . 
the target volume was defined as the pretreatment tumor site and the bilateral regional lymph node areas including the submental , submandibular , pharyngeal and retropharyngeal lymph nodes as well as the lower cervical and supraclavicular regions , depending on tumor localization and stage . 
since the optimal dose was unknown at the beginning of the study , three different dose levels of docetaxel ( 20 , 25 , and 30 mg / m2 ) were considered , depending on tolerability . 
the first 15 patients were planned to start with 30 mg / m2 of docetaxel for three cycles , with the dose being adjusted if accumulating toxicities occurred ( de - escalation strategy )  . 
to prevent edema and hypersensitivity reactions , the patients received oral dexamethasone 4 mg bid and oral cimetidine 300 mg daily for 3 days , starting the day before each administration of docetaxel . 
 endpoints these were stage - related and overall survival ( primary endpoint ) , relapse history , feasibility and early plus long - term late toxicity of concurrent radiation and chemotherapy with weekly docetaxel ( secondary endpoints )  . 
 the diagnosis included lung cancer ( 3 patients ) , prostate cancer ( 2 patients ) , scc of the floor of the mouth , scc of the palate , scc of the hypopharynx , scc of the esophagus , and breast cancer ( 1 patient each )  . 
intra - arterial chemotherapy with cisplatin resulted in a clinical overall response rate ( cr + pr ) of 56% , with 14 cr , 39 pr , 40 sd , and 1 pd . 
 local pathologic staging demonstrated a pcr rate of 10% ( 9 patients ) ; the remaining patients had the following t stages : pt1 ( 25 patients ) , pt2 ( 28 patients ) , pt3 ( 3 patients ) , and pt4 table 1 . 
 15 patients ( 16% ) had narrow or positive surgical margins that required additional local resection . all patients routinely received a percutaneous endoscopic gastrostomy ( peg ) tube before the starting of radiation to ensure sufficient nutrition during therapy . the first dose level of docetaxel given with concomitant radiation was 30 mg / m2 . 
however , this dose had to be reduced after the first 13 consecutive patients because 2 patients developed grade iv mucositis , and one patient each had grade 1 thrombocytopenia , and hyperuricemia with gout . 
these doses were better and equally well tolerated ; thus , the maximum tolerated dose ( mtd ) of docetaxel with concomitant radiation was defined as 25 mg / m2 in the adjuvant setting . 
patients ( % ) 94 ( 100 ) intra - arterial chemotherapy 85 ( 90 ) 1 cycle 7 ( 7 ) 2 cycles 2 ( 3 ) 3 cycles 94 ( 100 ) local operation 22 ( 23 ) with mandibular continuity resection 72 ( 77 ) with soft tissue and / or rim resections 92 ( 98 ) neck dissection 9 ( 10 ) bilateral mrnd ipsilateral mrnd 21 ( 22 ) ipsilateral mrnd + contralateral selective nd ( i - ii ) 17 ( 18 ) 21 ( 22 ) bilateral selective nd ( i - ii ) 10 ( 11 ) ipsilateral selective nd ( i - ii ) 8 ( 9 ) unilateral sentinel node biopsy 6 ( 6 ) bilateral sentinel node biopsy 2 ( 2 ) no neck dissection radiation 51.3 gy to tumor + lymph nodes + boost 10 gy + boost 20 gy concomitant chemotherapy docetaxel 30 mg / m2 ( 3 scheduled cycles ) docetaxel 25 mg / m2 ( 5 scheduled cycles ) docetaxel 20 mg / m2 ( 5 scheduled cycles ) all scheduled cycles administered mean no . 
 acute and late toxicities acute toxicities of chemoradiation at the 25 and 20 mg / m2 dose levels that prompted withdrawal of docetaxel included grade iii or iv mucositis ( 22 patients ) , hypersensitivity reactions with flush syndrome ( 2 patients ) , grade iv dermatitis ( 2 patients ) , fluid retention ( facial edema ) ( 1 patient ) , and grade iii transaminase elevation ( 1 patient )  . 
 in 6 of 22 patients , the metal plate bridging the mandibular defect had to be removed because of extreme shrinking of the skin with consecutive exposure of the implant . 
 treatment outcome to date , 18 patients have developed recurrent disease ( local relapse in 9 patients , lymph node metastases in 3 patients , distant metastases in 5 patients , and both locoregional recurrence and distant metastasis in 1 patient )  . 
23 patients have died , but 6 deaths were not related to the malignant disease ( 3 heart failures , 1 trauma , 1 stroke , 1 treatment - related renal failure )  . 
at a median follow - up of 4 years ( range , 1877 months ) , the actuarial 5 - year overall survival rate was 80% , and disease - free survival , defined as survival without local or locoregional relapse or distant metastatic disease , was 73% ( figures 1 and 2 )  . 
among patients with advanced disease ( stage iv ) , survival was 59% for all patients ( figure 4 ) and 56% for those receiving 25 mg / m2 of docetaxel . 
 published data demonstrated that in the non - surgical setting , the combination of high - dose radiotherapy ( up to 70 gy ) and chemotherapy using conventional agents like cisplatin and fluorouracil resulted in significantly improved survival rates compared with radiation alone [ 1 , 6 , 7 ]  . 
 therefore , new antineoplastic agents have been evaluated , and the use of the taxanes for the treatment of patients with head and neck cancer is under intensive investigation since several years . 
in phase ii studies of chemotherapy for recurrent and incurable head and neck cancer , overall response rates of up to 42% were achieved with 100 mg / m2 of docetaxel given every 3 weeks [ 10 , 12 ]  . 
adjuvant chemoradiation in head and neck cancer effects were acute and of short duration , including leukopenia ( up to 61% ) , alopecia ( up to 90% ) , hypersensitivity reactions ( up to 23% ) , skin toxicities ( 54% ) , and peripheral edema ( 31% )  . 
in 42 patients with bladder cancer who received postoperative chemoradiation ( 6874 gy in daily fractions of 2 gy with weekly doses of 30 mg / m2 of cisplatin ) , the addition of docetaxel at weekly doses of 40 mg / m2 was not tolerated , and the dose had to be reduced to 20 mg / m2 [ 43 ]  . 
this latter dose seemed to be well tolerated in combination with 60 gy for the treatment of non - small - cell lung cancer and esophageal cancer [ 26 ]  . 
in several studies of advanced inoperable head and neck cancer , the administration of weekly doses of 1530 mg / m of docetaxel was found to be feasible with concomitant radiation at doses of up to 70 gy [ 16 , 21 , 40 ]  . 
published data suggest that intra - arterial high - dose chemotherapy is associated with a very low incidence of acute systemic side effects [ 2224 ] ; this is particularly important for the treatment of patients with a high comorbidity . 
in a recent report of a regimen consisting of weekly cycles of docetaxel with concurrent radiation ( 6872 gy ) following induction therapy for locally advanced head and neck cancer , the 25 mg / m2 dose level of docetaxel also proved to be tolerable even though all patients developed grade iii mucositis and pain [ 40 ]  . 
 actuarial 3 - year - survival was 48% , and the incidence of local recurrence seemed to be reduced compared with a historical control group treated with postoperative irradiation alone . 
radiation had to be discontinued in 10% of the patients , and 39% received less than three cycles of chemotherapy . compared with these studies , outcome was superior in our trial of postoperative radiotherapy and concurrent docetaxel , with a 5 - year - survival of 83% in stage iii and 59% in stage iv patients . 
the survival of patients with early stage disease ( 8592% ) has to be judged as an improvement in the light of the data of the german - austrian - swiss tumor registry where these patients have a survival below 70% [ 17 ]  . 
grade iii or iv toxicities occurred in 41% of patients in the chemoradiation ar 18% of the patients received less than two thirds of the scheduled chemotherapy due to significant nausea and vomiting [ 3 ]  . 
in the rtog - trial 88 - 24 [ 2 ] , 51 patients received radiotherapy and concurrent moreover , compliance to therapy was acceptable when compared to published study data , and the incidence of acute toxicities following chemoradiation with docetaxel appear similar to those observed with concurrent cisplat therefore it appears that docetaxel has the potential to replace platinum agents in combined chemoradiation protocols . 
 at present , a final conclusion as to the efficacy of our treatment program with regard to local recurrence rate and long - term survival is not yet possible because of the still limited follow - up . 
in that study which combined conventional radiotherapy at 70 gy with weekly docetaxel 20 mg / m2 , the actuarial 3 - year survival rate was 47% and the local control rate 64% at a median follow - up of 37 months . 
instead of a comparison of side effects of neoadjuvant radiochemotherapy and postoperative radiotherapy [ 45 ] , which might not be appropriate , the present report offers the possibility to judge postoperative radiochemotherapy more adequately . 
how important the issue of life quality may be , however , long - term survival must remain the main goal of cancer treatment . acknowledgment this work was supported in part by aventis pharma deutschland , bad soden , germany . 
mnter1 , mattias schfer1 , peter haering2 , bernhard rhein2 , christoph thilmann1 , jrgen debus1 background and purpose : intensity - modulated radiation therapy ( imrt ) has proven extraordinary capability in physical terms such as target conformity , dose escalation in the target volume , and sparing of neighboring organs at risk . 
the radiobiological consequences of the protracted dose delivery for cell survival and cell cycle progression are still unclear and shall be examined in this study . material and methods : human lymphoblasts ( tk6 ) and human melanoma cells ( mewo ) were irradiated with protocols of increasing dose protraction . 
 results : in a first series of experiments , melanoma cells showed a highly significant increase of survival of 6.0% after protracted dose delivery of 2 gy compared to conventional fast application with the same dose . 
in comparison to irradiation with application of the same dose in a classic four - field box , a significantly increased survival of 5.1% ( mean value ) was determined . conclusion : even at fraction times of 1530 min the protracted dose delivery increases the survival rates in cell culture . 
doch die strahlenbiologischen konsequenzen fr zellberleben und zellzyklusprogression , die sich aus der protrahierten dosisapplikation ergeben knnten , sind noch unklar und sollen in dieser arbeit untersucht werden . material und methodik : humane lymphoblasten ( tk6 ) und humane melanomzellen ( mewo ) wurden mit protokollen ansteigender dosisprotrahierung bestrahlt . 
klonogenes zellberleben sowie zellzyklusprogression nach verschiedenen bestrahlungsexperimenten wurden untersucht . ergebnisse : in einer ersten versuchsreihe zeigten die melanomzellen ein signifikant um 6 , 0% erhhtes zellberleben , wenn 2 gy stark protrahiert appliziert wurden , verglichen mit schneller herkmmlicher bestrahlung . 
im vergleich zur bestrahlung mit der gleichen dosis in einer konventionellen vierfelderbox war das berleben nach imrt durchschnittlich um 5 , 1% erhht . schlussfolgerung : selbst bei fraktionszeiten von 1530 min fhrt die protrahierte dosisapplikation zu einem erhhten zellberleben in zellkultur . 
radiobiological investigations of dose - rate effects in imrt introduction after 1 decade of clinical intensity - modulated radiation therapy ( imrt ) , a lot is known about its capabilities in physical terms such as target conformity , dose escalation in the target volume , and sparing of neighboring organs at risk [ 6 , 10 , 1619 , 23 , 28 ]  . 
these qualities permit the irradiation of patients with complex - shaped tumors at problematic locations such as the skull base , which could not be treated successfully with conventional irradiation methods due to tolerance doses of surrounding structures . 
complex imrt plans result in a pulsed dose delivery consisting of > 100 subsegments with a fraction time of up to 30 mthe radiobiological consequences of this decreased dose rate and pulsed dose application are still unclear [ 8 , 18 ]  . 
figure 1 shows a hypothetical survival curve of cells displaying cumulative hypersensitivity to low - dose pulses . yet , the lowered dose rate might as well allow split - dose recovery during the prolonged time of one fraction and thus diminish the probability of strand break interactions resulting in a higher cell survival [ 8 , 25 ]  . 
these dose rates are similar 30 m in addition , enzymes involved in dna repair could be induced by early hits of radiation and radioresistance would be altered during the radiation fraction [ 11 ]  . 
 cell cycle progression during a fraction should be low due to the comparatively long generation times of the cells , but a low percentage of cells might become arrested in resistant cycle phases after early radiation hits and therefore radiation sensitivity might change during the time of a fraction . 
 mycoplasm - free human lymphoblastoid cells ( tk6 ) were maintained in suspension in rpmi 1640 ( pan ) supplemented with 10% heat - inactivated horse serum ( sigma ) without addition of antibiotics . 
hypothetical survival curve for added hypersensitivity effects : the black line shows a classic survival curve , the dotted line hypersensitivity after low - dose irradiation , and the gray line the initial part of the dotted curve iterated for several 0.2 - gy pulses resulting in a hypothetical survival curve with decreased survival after 2 gy . 
hypothetische berlebenskurve fr eine folge von hypersensitivittseffekten : schwarz dargestellt ist die klassische berlebenskurve , gepunktet die hypersensitivitt im niedrigdosisbereich und grau die addition des anfangsabschnitts der gepunkteten linie fr mehrere 0 , 2 - gy - pulse , was hypothetisch zu einem erniedrigten berleben nach 2 gy fhrt . 
after an incubation time of 30 min with the alcohol cells were washed twice with pbs and 10 g rnase ( sigma ) and 900 l propidiumiodide ( sigma ) at a concentration of 20 g / ml were added . 
by this arrangement every point of a target volume can be examined in stereotactic coordinates for physical or biological studies after transferring imrt plans to the phanto irradiations all irradiations were performed at the clinical cooperation unit radiotherapy of the german cancer research center ( dkfz ) in heidelberg , germany , using a siemens linear accelerator primus at energies of 6 or 15 mev . 
 in the preliminary experiments cells were irradiated in 25 - cm2 culture flasks and 96 multiwell plates under rw3 plates 3 cm thick ( ptw , freiburg , germany )  . 
six different irradiation schedules incorporating a successive decrease of dose rate and a pulsed dose delivery , thus simulating the situation in imrt , were used ( figure 2 )  . 
in each protocol a total dose of 2 gy was applied , at first in one single pulse , then in two pulses with intervals of 5 , 15 , and 30 min the last two protocols the dose was delivered in six and 21 pulses , respectively , each in an overall time of 30 mthe clonogenic survival of the melanoma cells ( mewo ) and the lymphoblasts ( tk6 ) was determined as described above . 
 in the experiments using patient plans , cells were irradiated in cryotubes in the phanto after trypsinization they were transferred to the cryotubes at suitable concentration and centrifuged to concentrate the cells at the half - ball - shaped bottom of the cryotube . 
 four clinical imrt plans were transferred to the phantom reproducing one case of a sphenoidal meningioma , a nasopharyngeal carcinoma , a carcinoma in the maxillary sinus , and a carcinoma of the breast . 
 the points were localized at the center of the target volume , at the center of an organ at risk or even very close to such structures to get points with heterogeneous temporal dose distributions . 
 software results preliminary experiments figure 4 shows the average survival data after twelve repeats of the experiments with corresponding standard deviations for both cell lines and the six different irradiation protocols . 
melanoma cells showed a highly significant increase of survival of 7.03% ( p = 0.0002 , t - test ) and lymphoblasts an increase of survival of 2.24% ( p = 0.022 , t - test )  . 
 tributions before , immediately after , and 0.5 , 1 , 2 , 4 , 6 , 8 , 16 , 24 , 48 , 72 , 96 h after irradiation were analyzed and were almost the same for the two protocols and two cell lines . 
 discussion there are several reports about the excellent therapeutic effectiveness of imrt in the treatment of prostatic carcinoma and head and neck tumors [ 7 , 26 , 27 ]  . 
although there is an enormous amount of articles about imrt , its advantages and new qualities , there are hardly any investigations and considerations regarding biological consequences of the new temporal dose characteristics . 
the consequences of protracted dose application have been investigated by morgan et al . , who found increased cell survival after several fractions of protracted dose delivery [ 14 ]  . 
radiobiological investigations of dose - rate effects in imrt could these results be a consequence of a systemic error in the experimental setup and methods ? in both series of experiments the samples of the different protocols , plans and controls were treated absolutely the same way , beginning from trypsinization , preparation in culture flasks , time out of the incubator up to the counting of colonies , which was performed blindly to prevent any bias influences . 
 although the principle of the colonyforming assay remains the same , the experimental setup has to be viewed as a different testing systeabsolute values of survival rates between the preliminary experiments and the imrt experiments can only carefully be compared . 
the laser positioning system of the linear accelerator and a millimeter scaling of the filling cylinders allowed an accuracy of 1 mbefore irradiation cells were centrifuged to concentrate the cells in an aggregate at the bottom of the half - ball - shaped cryotube . 
the cells remained in this position even after horizontal placement , so the accuracy here should also be around 1 m the overall positioning error should be at most 2 mcould this positioning error have influence on the measured survival rates ? in a plan with inhomogeneous dose distribution as typically present in imrt , the cells could get into areas of the plan with different doses than expected or previously measured . 
berlebenskurve der mewo - melanomzellen nach bestrahlung mit den vier verschiedenen imrt - plnen ( gepunktet und rautensymbole ) und nach bestrahlung in der vierfelderbox ( schwarz und kreissymbole ) ; mittelwerte und standardabweichungen nach zehn wiederholungen . value of total dose was used for further analyzation of the survival data . 
 so what does this increased cell survival mean for the effectiveness of imrt ? does imrt kill less tumor cells than conventional therapy does ? does the protracted dose delivery diminish advantages such as dose escalation ? could this be a disadvantage of imrt technologies with a long fraction time like the step - and - shoot technology and should faster technologies be preferred ? in that case methods that improve the efficiency of segmentation algorithms or segment delivery would gain importance [ 1 , 35 , 13 , 24 ]  . 
depending on the fraction time and a parameter of radioresistance and dna repair capacity of different cells , the needed iso - effect treatment dose could be adjusted to the protraction effects . 
can these results be transferred to the real situation of cells in a tumor with all special parameters such as intercellular interactions or inhomogeneities in blood or oxygen supply ? to perform the experiments described in this paper , we had to make a lot of compromises in cell handling and testing procedures . 
this was necessary to be able to work in the phantom , to use patient imrt plans , to have the best positioning accuracy , and to be the closest to imrt reality as possible . 
 strahlentherapie und onkologie original article regional hyperthermia in conjunction with definitive radiotherapy against recurrent or locally advanced prostate cancer t3 pn0 m0 wolfgang tilly1 , johanna gellermann1 , reinhold graf1 , bert hildebrandt2 , lothar weibach3 , volker budach4 , roland felix1 , peter wust1 background and purpose : since long - term results of the standard treatment of locally advanced or recurrent prostatic carcinoma are unsatisfactory , the role for additional regional hyperthermia was evaluated in a phase i / ii study . patients and methods : from 08 / 1996 to 03 / 2000 , 22 patients were treated by a standard irradiation regimen ( 68.4 gy ) in combination with regional hyperthermia ( weekly , five to six times ) , and five of 22 patients received short - term ( neoadjuvant ) hormonal treatment . 
feasibility of hyperthermia , and acute / late toxicity as well as long - term follow - up ( prostate - specific antigen [ psa ] control , overall survival ) were analyzed . 
severe acute toxicity of grade 3 occurred at the rectum in three , at the urethra in four , at the intestine in one , and a burn induced by hyperthermia in one of 22 patients . 
 key words : regional hyperthermia prostate carcinoma psa control strahlenther onkol 2005 ; 181 : 3541 doi 10.1007 / s00066 - 005 - 1296 - 8 definitive externe radiotherapie mit regionaler hyperthermie beim lokal fortgeschrittenen oder rezidivierten prostatakarzinom stadium t3pn0m0 hintergrund und ziel : die langzeitergebnisse der standardtherapie beim lokal fortgeschrittenen oder rezidivierten prostatakarzinom sind unbefriedigend . 
daher wurde eine zustzliche regionale hyperthermie in einer phase - i / ii - studie evaluiert . patienten und methodik : von 08 / 1996 bis 03 / 2000 wurden 22 patienten mit einer standardradiotherapie von 68 , 4 gy in kombination mit regionaler hyperthermie ( wchentlich , fnf bis sechs sitzungen ) behandelt . 
die klinischen endpunkte wurden mit thermischen parametern korreliert . ergebnisse : es konnten mittlere maximaltemperaturen entlang der urethra von 41 , 4 c ( 41 , 0 c fr die rezidive ) sowie mittlere t90 von 40 , 7 c erreicht werden . 
schwere akute nebenwirkungen vom grad 3 traten am rektum bei drei , an der urethra bei vier , am dnndarm bei einem sowie durch hyperthermie bedingt ( verbrennung ) bei einem von 22 patienten auf . 
thermischen dosen und der langfristigen psa - kontrolle . 1 department of radiation medicine , charit medical school , berlin , germany , 2 department of internal medicine hematology and oncology , charit medical school , berlin , germany , 3 department of urology , urban hospital , berlin , germany , 4 department of radiation oncology , charit medical school , berlin , germany . received : march 11 , 2004 ; accepted : july 2 , 2004 strahlenther onkol 2005 no . 
hier ist eine weitere evaluation sinnvoll , insbesondere auch unter anwendung verbesserter hyperthermietechnologien . schlsselwrter : regionale hyperthermie prostatakarzinom psa - kontrolle introduction for locally advanced prostate cancer ct3 / 4 with cn0 or pn0 , external - beam radiotherapy ( ebrt ) is accepted as standard treatment . 
reports with large numbers of t3 carcinomas describe a 5 - year prostate - specific antigen ( psa ) relapse - free survival of only 3040% paralleled by considerable rates of local recurrences in the range of 20% [ 12 , 24 ]  . 
therefore , taking the peri - / postoperative morbidity into account , ebrt is widely favored . however , in t3 / t4 tumors definitive radiotherapy alone with standard doses of about 72 gy is also inadequate . 
innovative strategies include dose escalation by intensity modulation , additive interstitial radiotherapy , and / or cytoreduction by hormonal manipulation , either neoadjuvant and / or adjuvant , for several years . 
nonetheless , these approaches could not improve the outcome , but imply some late normal tissue reactions . dose escalation with three - dimensional conformal irradiation led to an increased late rectal toxicity grade 2 , and in fact , investigators found a higher rate of proctitis grade 2 [ 19 , 22 ]  . 
long - term hormonal treatment causes specific side effects of the medication , impotency , and increased late reactions [ 8 ]  . there is currently no standard of care for locally advanced prostatic carcinoma . 
 external radiotherapy was performed with a linear accelerator ( siemens mevatron kd , 18 mv ) using fractions of 5 1.8 gy up to 68.4 gy at the reference point ( icru )  . 
a conformal four - field box technique was used . regional hyperthermia was carried out about 30 min before or after a single fraction once a week five to six times during the radiotherapy course as described elsewhere [ 29 ]  . 
 we used the sigma - 60 applicator of the bsd 2000 syste the midplane ( feed points of the antennas , central plane of the applicator ) was positioned a few centimeters cranial to the symphysis defining the longitudinal position [ 21 ]  . 
for the temperature - time curves in between , we left the point probe at the maximu we assume that these reference points for the temperature - time curves characterize the central part and the periphery of the prostate . 
using the temperature - time curves at the beginning ( power - on ) and at the end ( power - off ) of heat treatment , we could derive specific absorption rates ( sars ) in w / kg at the reference points . 
hyperthermia and definitive radiotherapy in prostate cancer in the measurement points ( attempting to achieve > 41.5 c ) , we increased or reduced the total power and , in particular , the weights at the dorsal or ventral channel or modified the phase delay . 
for the heat treatments we defined a toxicity score as follows : 0 no complaints or some discomfort by bolus pressure , thermal stress or positioning ; 1 power - dependent discomfort , which resolves completely at the end of heat treatment ; 2 hot spot sensation , which persists or occurs after the end of heat exposure and resolves in days or ( rarely ) weeks ; 3 burn or thermal lesion . 
local progression was defined according to who as macroscopic tumor growth of > 25% . all statistical analyses were conducted with spss software version 10 ( spss inc , chicago , il , usa )  . 
 69 years ( 5675 years ) age stage primary ct3a pno ct3b pn0 hormonal manipulation primary none neoadjuvant 6 grading primary recurrent rtx cno recurrent none recurrent psa primary < 10 ng / ml 10 20 ng / ml 4 > 20 ng / ml mean = 16.7 ng / ml recurrent < 10 ng / ml 10 20 ng / ml mean = 10.8 ng / ml table 2 . 
die spttoxizitt ( unten ) wurde nach dem lent - score klassifiziert ( sptwirkungen auf das normalgewebe ) [ 18 ]  . acute grade 0 grade 1 grade 2 grade 3 grade 4 rectum bladder / urethra intestine skin heat 2 3 5 1 3 5 8 4 2 late grade 1 grade 2 grade 3 / 4 gastroinestinal urogenital 2 / 20 ( 10% ) 1 / 20 ( 5% ) 2 / 20 ( 10% ) 1 / 20 ( 5% ) patient was comparable for both tumor entities . 
nevertheless , the temperatures achieved for recurrences are similar or even higher , which is probably based on a reduced perfusion and perfusion regulation capacity . table 2 illustrates that primary prostatic carcinomas are easier to heat than primary rectal carcinomas with higher relative sar and t90 ( for lower total power ) [ 21 , 23 ]  . 
only 14% grade 3 reactions at the rectum , 18% at the urethra ( dysuria ) , < 5% at the small intestine and hyperthermia - related ( burn ) , respectively , were observed . 
grade 2 reactions at the urethra or caused by heat ( persistent hot spot sensations ) are frequent ( 55% ) , but moderate urinary toxicity is common during radiotherapy . 
persistent hot spots ( muscle - skeletal pain syndrome ) heal within a few days or , at most , several weeks without any late morbidity . no correlation was observed between thermal parameters ( tmax , t90 ) and acute toxicity . 
however , this might be explained by an increased tolerance for more aggressive heating in cases of less radio - induced toxicity . late reactions ( see table 3 below ) were moderate . 
of these , only 5% had rectal toxicity grade 3 ( with permanent loss of mucus and urgency ) and 10% ( n = 2 / 20 ) suffered from long - term urinary reactions grade 2 ( intermittent urgency and dysuria )  . 
our analysis showed no correlation between thermal parameters and chronic toxicity . follow - up a subdivision of the clinical events according to death , psa failure , local progression , and distant metastases is shown in table 4 . 
berleben unter psa - kontrolle ( astro - konsensus , < 1 ng / ml ) bei primren karzinomen ( 15 patienten ) und rezidiven ( sieben patienten )  . 
in the group with psa control ( n = 8 ) significantly higher temperatures and thermal doses were achieved ( p - values of 0.010.02 ) in spite of the small number of patients . 
in fact , tmax was the only relevant predictive factor for psa control with five local psa failures for patients with tmax < 41.2 c and only one psa failure for tmax 41.2 c ( p = 0.037 , mann - whitney test )  . 
 even though the ( pretherapeutic ) psa value is well established as prognostic factor ( see , e.g. , [ 14 ] ) , the correlation between the initial psa and the psa control was not as high in this small group according to table 5 . 
the widespread therapeutic option was radiotherapy alone with radiation doses of 6670 gy resulting in a long - term psa control of only 30% for observation times > 5 years [ 31 ]  . 
psa control in a similar range is achieved for high - risk tumors ( e.g. , t3 / 4 ) by other groups applying standard radiotherapy , e.g. , a 5 - year psa control of 35% [ 28 ] or a 3 - year psa control of 60% [ 6 ]  . 
 alive psa progression progression metastases distant local primary n = 15 recurrent n = 7 4 monal treatment in patients with either lymphatic involvement ( pn + ) or clinical stage t3 ( palpable tumor infiltration beyond the capsula )  . 
rtog trial 92 - 02 , dealing with a patient group similar to ours ( t2ct4 tumors ) , found a biochemical control of 21% after 5 years in the reference arm with radiotherapy and neoadjuvant androgen suppression ( 2 months ) , while additional long - term androgen deprivation improved psa control to 46% [ 8 ]  . 
 an eortc trial [ 4 ] investigated a patient group of 415 men with locally advanced prostate cancer treated with either ebrt or radiotherapy and long - term androgen deprivation . 
univariate analysis of thermal parameters correlates the effectiveness of the heat treatments with the major clinical endpoint psa control ( for primary prostatic carcinoma , 14 patients alive )  . 
the one patient with metastatic disease was excluded from the thermal analysis ( n = 6 ) , which can only characterize local psa control , whereas the whole patient group is described by the initial psa value ( n = 7 )  . 
der patient mit metastasierender erkrankung wurde aus der thermischen analyse genommen ( n = 6 ) , da diese nur die lokale psa - kontrolle betrifft , whrend die gesamte patientengruppe ( n = 7 ) durch den initialen psa - wert beschrieben wurde . 
however , a summary of studies showed that the long - term biochemical control of the surgical approach is not superior to conservative treatments , achieving a psa control of < 40% [ 19 ] and even with postoperative radiotherapy of only 57% . 
 from these data we may conclude , that a combined and / or more aggressive treatment strategy can improve the 5 - year biochemical control of radiotherapy alone from 2040% up to slightly > 50% . 
 therefore , a careful evaluation of all treatment combinations with respect to toxicity is required . in our small series we gained a long - term psa control ( > 5 years ) of 50% , and an excellent overall survival of > 90% for primary locally advanced prostatic carcinoma t3 pn0 . 
they found after a shorter observation time a 3 - year biochemical control of 70% , which is fairly in agreement with our data ( see figure 1 )  . 
 conclusion regional hyperthermia is a very feasible and well - tolerated procedure , which might increase the local effectiveness of radiotherapy or any combination therapy against locally advanced prostate cancer . 
for example , standard radiotherapy plus regional hyperthermia might be as effective as standard radiotherapy plus long - term androgen suppression or a dose - escalated schedule , but less burdensome ( or less expensive )  . 
 acknowledgment this work has been supported by the lieselotte - beutel - stiftung , berl strahlentherapie strahlentherapie und onkologie und onkologie original article original article phase i / ii trial of simultaneous whole - brain irradiation and dose - escalating topotecan for brain metastases martin kocher , hans - theodor eich , robert semrau , semi aykut gner , rolf - peter mller1 background and purpose : topotecan penetrates the blood - brain barrier and sensitizes tumor cells against radiation . 
topotecan application simultaneously with whole - brain irradiation ( wbrt ) was conducted to estimate toxicity , maximum tolerated dose and survival in patients with inoperable brain metastases . patients and methods : in 47 patients suffering from previously untreated brain metastases , topotecan was applied on a daily i.v. 
response evaluation was possible in 26 / 47 patients , overall response rate was 58% ( cr [ complete remission ] 5 / 26 , pr [ partial remission ] 10 / 26 , nc [ no change ] 8 / 26 )  . 
in 15 / 42 patients ( 36% ) , brain metastases were the dominant cause of death . conclusion : for a daily topotecan schedule simultaneous to wbrt , the maximum tolerated dose is 12 0.5 mg / m2 in chemonaive patients . 
a phase iii trial has now been started to find out whether wbrt + topotecan increases survival compared to wbrt alone . key words : brain metastases whole - brain radiotherapy combined radiochemotherapy topoisomerase i inhibitor topotecan strahlenther onkol 2005 ; 181 : 205 doi 10.1007 / s00066 - 005 - 1242 - 9 phase - i / ii - studie zur simultanen ganzhirnbestrahlung mit dosiseskaliertem topotecan bei hirnmetastasen hintergrund und ziel : topotecan , ein topoisomeraseinhibitor , gehrt zu den wenigen substanzen , die die blut - hirn - schranke durchdringen und tumorzellen gegenber ionisierender strahlung sensibilisieren . 
untersucht wurden toxizitt , maximal tolerable dosis , ansprechen der hirnmetastasen und berlebenszeit . patienten und methodik : bei 47 patienten mit unvorbehandelten hirnmetastasen wurde eine palliative ganzhirnbestrahlung mit 36 gy / 3 gy mit einer tglichen kurzinfusion von topotecan 12 h vor der bestrahlung kombiniert . 
die topotecandosis wurde wie folgt eskaliert : 5 0 , 5 mg / m2 , 8 0 , 5 mg / m2 , 12 0 , 5 mg / m2 , 12 0 , 6 mg / m2 . ergebnisse : insgesamt konnte bei 38 / 47 patienten ( 81% ) die therapie wie vorgesehen durchgefhrt werden . 
eine hmatotoxizitt grad 3 / 4 trat bei 5 / 32 chemotherapeutisch unvorbehandelten patienten ( 16% ) und bei 7 / 15 patienten ( 47% ) auf , die bereits zuvor eine chemotherapie erhalten hatten . 
bei 26 / 47 patienten konnte das ansprechen beurteilt werden ; die ansprechrate lag bei 58% ( cr [ komplette remission ] 5 / 26 , pr [ partielle remission ] 10 / 26 , nc [ stabile erkrankung ] 8 / 26 )  . 
 schlsselwrter : hirnmetastasen ganzhirnbestrahlung kombinierte radiochemotherapie topoisomerase - i - hemmer topotecan 1 department of radiation oncology , university hospital , university of cologne , cologne , germany . received : october 2 , 2003 ; accepted : july 23 , 2004 strahlenther onkol 2005 no . 
while surgery [ 31 ] and radiosurgery [ 10 , 13 ] are efficient only in selected subgroups , most patients can only be treated by palliative whole - brain irradition ( wbrt ) with overall response rates of about 5060% and median survival times of 34 months [ 3 , 5 , 6 ]  . 
due to the limited tolerance of the normal brain tissue to radiation and a shallow radiation dose - response curve [ 24 ] , increased doses of radiation have failed to improve outcome . 
therefore , we evaluated the use of topotecan , a topoisomerase i inhibitor , which has been shown to penetrate the intact blood - brain barrier [ 2 , 35 ] and to sensitize tumor cells against radiation [ 12 , 17 , 33 ]  . 
toxicity and effectiveness were examined in a dose - escalating phase ii trial where topotecan was infused daily before the radiation fractions in order to allow for a maximum of interaction between the damage - repair processes induced by radiation and the topoisomerase i inhibition . 
preliminary results of this study have been published earlier [ 14 ]  . patients and methods dose - finding pilot study from 1996 to 2002 , 47 patients with newly diagnosed brain metastases of various primary cancers were treated with wbrt and simultaneous topotecan . 
patients who fulfilled the institutions standard criteria for receiving wbrt ( irresectable brain metastases unsuitable for radiosurgery , histological proof of malignant disease , no prior irradiation to the brain , karnofsky performance score of 50 ) and who had sufficient bone marrow function ( leukocytes 4 , 000 / l , thrombocytes 100 , 000 / l , hemoglobin 9 g / dl ) and normal renal function ( serum creatine levels ) were included , irrespective of prior chemotherapy . 
wbrt was applied according to the usual irradiation technique and fractionation scheme in the institution , 36 gy in twelve fractions of 3 gy referred to the midplane using opposing fields . 
 phase ii dose - escalating study resembled those for the dose - finding study ( irresectable brain metastases unsuitable for radiosurgery , histological proof of malignant disease , no prior irradiation to the brain , leukocytes 4 , 000 / l , thrombocytes 100 , 000 / l , hemoglobin 9 g / dl and normal renal function , prior chemotherapy allowed ) , but only patients with a performance score ( karnofsky ) 70% were included . 
in general , wbrt was applied using 36 gy in twelve daily fractions of 3 gy , but as in the dose - finding protocol , patients with a pronounced brain edema were given 4050 gy in 2025 fractions of 2 gy . 
 the protocol prescribed a dose increase in steps of 0.1 mg / m2 , starting at a dose level of 12 0.5 mg / m2 which was found to be safe in the dose - finding study . 
in case that one of the three patients experienced a grade 4 toxicity , up to another three patients had to be treated at this dose level until another grade 4 toxicity was observed . 
partial remission ( pr ) was supposed , if the estimated total volume of the metastases ( estimated from two perpendicular diameters ) or the total number of metastases was reduced by at least 50% . 
response , survival time , cause of death and toxicities were recorded and evaluated using the spss 11.0 ( statistical package for the social sciences , chicago , il , usa ) software package . 
 consecutively , a phase ii dose - escalating protocol was started that aimed to evaluate the maximum tolerated dose ( mtd ) of topotecan when given in twelve daily doses . 
 results dose - finding pilot study during the pilot phase ( n = 14 ) with topotecan doses of 5 0.5 mg / m2 ( n = 5 ) , 8 0.5 mg / m2 ( n = 5 ) , and 12 0.5 mg / m2 ( n = 4 ) , one patient who received 8 0.5 mg / m2 developed a grade 4 thrombopenia synchronously to a disseminated intravascular coagulation syndrome . 
 phase ii dose - escalating study the phase ii study was started with 12 0.5 mg / m2 in three patients without grade 4 toxicity and continued with 12 0.6 mg / m2 in three patients , one of whom developed grade 4 leukopenia and thrombopenia . 
the first of the scheduled next three patients also experienced grade 4 leukopenia / thrombopenia ; thus , a total of two out of four patients were affected , and one of the two patients with leukopenia died from poststenotic pneumonia within 3 weeks . 
in consequence , another 18 patients ( instead of the planned 20 ) were treated in the phase ii protocol at this dose level until the closing date of the protocol . 
the reasons for not completing the scheduled therapy in nine patients were : leukopenia / fever / infection ( n = 4 ) , tumor progression ( n = 2 ) , myocardial infarction ( n = 1 ) , non - compliance ( n = 1 ) , administrative failure ( n = 1 )  . 
there was no indication of neurologic toxicity caused by topotecan [ 26 ]  . outcome median survival of all patients was 5.1 months ; five patients are still alive at a median follow - up of 11 months ( figure 2 )  . 
 survival data were compared to both a historical collective of the same institution ( n = 207 , 19771991 ) and to the patients treated in the rtog recursive partitioning analysis ( rpa )  . 
it has , however , been questioned whether the rpa keeps its prognostic power in patients with more than three metastases [ 23 ] , to which group 66% of the present patients belong . 
the main dose - limiting toxicity was leukopenia , and the mtd in chemonaive patients was 12 0.5 mg / m2 , resulting in 16% grade 3 / 4 hematotoxicity . 
for patients with prior chemotherapy , the dose should be reduced , because 6 / 12 ( 50% ) had a grade 3 / 4 leukopenia / thrombopenia at this dose level . 
although no clear recommendation can be made , a reduction to daily doses of 0.4 mg / m2 ( dose intensity reduction by 20% ) should allow to detect severe hemototoxicities and stop topotecan infusion early enough in the radiochemotherapy course . 
oral mucositis grade 12 ( n = 3 ) was possibly caused by topotecan , while oral thrush ( n = 4 ) seems to relate to the use of high - dose dexamethasone . 
 the finding that topotecan given as a single drug has some activity in brain metastases of small cell lung cancer [ 15 ] and breast cancer [ 25 ] , and the observation that it penetrates the chemonaive prior chemotherapy 6 / 12 3 / 21 5 0.5 mg / m2 8 0.5 mg / m2 12 0.5 mg / m2 12 0.6 mg / m2 topotecan figure 1 . 
frequency of any grade 3 / 4 hematologic toxicity ( number of affected patients / total number of patients in each dose group ) in patients without and with prior chemotherapy during daily infusion of topotecan simultaneously with whole - brain irradiation . 
 blood - brain barrier [ 2 , 35 ] and sensitizes tumor cells against radiation [ 12 , 17 ] has stimulated several phase i / ii trials which evaluated the use of combined radiochemotherapy with topotecan for brain metastases . 
 grade 1 / 2 3 symptoms of increased intracranial pressure asthenia , depression , general weekness oral thrush oral mucositis cushing fever / pneumonia deep vein thrombosis emesis coagulation ( disseminated intravascular coagulation ) 0 0 0 0 0 1 0 0 strahlenther onkol 2005 no . 
again , the mtd was 0.4 mg / m2 / d , the overall response rate amounted to 57% , and a median survival time of 5 months was achieved . 
 [ 20 ] treated seven patients with primarily diagnosed or recurrent brain metastases with twelve to 18 daily doses of 0.5 mg / m2 and observed two grade 3 hematotoxicities and 4 / 6 prs . 
 while some effort has been undertaken to evaluate the effectiveness of chemotherapy alone in patients with brain metastases [ 4 , 11 , 22 , 28 , 32 ] , approaches that investigated concurrent radiochemotherapy have been rare [ 6 , 9 , 16 , 21 ]  . 
in the latter scheme that also used high radiation doses ( 54 gy ) , objective response rates of 56% and median survival times of 8 months were found , but chemotherapy produced unacceptable hematotoxicity . 
survival analysis ( median survival time ) for patients treated with whole - brain irradiation ( wbrt ) and topotecan , compared to the rtog group and to a historical group of the institution , both treated with wbrt alone . 
berlebensanalyse ( mediane berlebenszeit ) der patienten , die mit einer ganzhirnbestrahlung ( wbrt ) in kombination mit topotecan behandelt wurden , im vergleich zu den patienten aus der rtog - analyse ( alleinige wbrt ) und zu einer gruppe von patienten , die in kln ebenfalls eine alleinige wbrt erhalten hatten . 
 [ 1 ] treated patients with multiple brain metastases with wbrt and applied concurrent and adjuvant temozolomide in the investigational arresponse rate was increased from 67% to 96% , and a marked neurologic improvement was observed . 
 besides overall survival , the duration of functional independence , e.g. , the survival time with acceptable quality of life , and the freedom from cerebral death should be evaluated . 
 a phase iii trial supported by the german cancer society ( deutsche krebsgesellschaft ) comparing wbrt with daily topotecan to wbrt alone in lung cancer patients has now been started . 
the authors compared the efficacy of two regimens in 210 stage iiaiiib cervical cancer patients : sequential radiation therapy ( srt ) with 4 8 gy high - dose - rate brachytherapy ( hdr - bt ) to point a followed by external - beam radiotherapy ( ebrt ) , and continuous irradiation ( crt ) in which 5 6 gy hdr - bt to point a administered weekly was integrated with ebrt ( ebrt was omitted on the day of bt )  . 
moreover , prolonged ott is considered a factor attributed to the outcome of the only negative randomized trial of weekly cisplatin in addition to rt [ 3 , 5 ]  . in the study by mayer et al . 
additionally , administering bt in srt before ebrt might also have influenced the outcome , particularly in stage iiib tumors [ 4 ]  . the authors stated that the ott in the crt group was the shortest possible ( 35 days ) which could be found in the literature , which is incorrect . 
in our study , only eleven of the 28 strahlenther onkol 2005 ; 181 : 54 doi 10.1007 / s00066 - 005 - 9122 - x evaluable patients ( 39% ) completed treatment within the prescribed ott ( 45% and 35% for groups a and b , respectively ) , and 17 had unplanned treatment breaks , almost in all cases due to treatment toxicity . 
 [ 1 ] reported a retrospective series of cervical cancer patients irradiated up to 7 weeks ( including weekend ldr - bt insertions ) to a total point a dose of 60 gy . 
they found a significantly increased incidence of serious late morbidity in the shortest treatment group ( 23% at 5 years grade 4 morbidity in patients treated within 2932 days with only 4 radiotherapy - free days )  . 
importantly , also in this series no significant effect of ott on the cause - specific survival was found . thus , shortening the ott to < 35 days has been attempted in cervical cancer , yet without impressive results . 
 strahlentherapie und onkologie original article amifostine is a potent radioprotector of salivary glands in radioiodine therapy structural and ultrastructural findings * hannes kutta1 , 2 , uwe kampen3 , christoph sagowski2 , winfried brenner3 , 4 , karl - heinz bohuslavizki5 , friedrich paulsen1 , 6 background and purpose : salivary gland impairment following high - dose radioiodine treatment is well recognized . 
this study investigates the radioprotective effects of amifostine in salivary glands of rabbits receiving high - dose radioiodine therapy so as to obtain deeper insight in changes on the cellular and ultrastructural level . material and methods : a total of 20 rabbits were investigated . 
subsequently , salivary glands ( submandibular and parotid glands , respectively ) of all animals were examined by light and transmission electron microscopy . results : parenchymal damage of both parotid and submandibular glands , specially acinar structures comprising cell organelles and nuclei , of animals pretreated with amifostine was much less pronounced than in animals without amifostine pretreatment . conclusion : the results indicate that parenchymal damage in salivary glands induced by high - dose radioiodine therapy can significantly be reduced by amifostine . 
 key words : salivary glands high - dose radioiodine therapy radioprotection amifostine thyroid cancer strahlenther onkol 2005 ; 181 : 23745 doi 10.1007 / s00066 - 005 - 1353 - 3 wirksame protektion von speicheldrsen unter radiojodtherapie durch amifoststrukturelle und ultrastrukturelle analyse hintergrund und ziel : die schdigung von speicheldrsengewebe durch radiojodtherapie ist bereits beschrieben . 
in dieser studie werden die radioprotektiven auswirkungen nach gabe von amifostin auf speicheldrsen von kaninchen nach hochdosis - radiojodtherapie untersucht , um genauere kenntnis ber vernderungen auf dem zellulren und ultrastrukturellen sektor zu erlangen . material und methodik : 20 kaninchen wurden untersucht . 
 ergebnisse : die schdigung des parenchyms , insbesondere von zellorganellen und zellkernen der azini , der glandulae parotidea und submandibularis von kaninchen , die mit amifostin vorbehandelt waren , war bedeutend geringer ausgeprgt als bei den tieren ohne amifostingabe . 
 * the animal experiments were done at the clinic of nuclear medicine , kiel university hospital , and the light and electron microscopic investigations were done at the department of anatomy , christian albrecht university of kiel . 
radioprotection of salivary glands by amifostine schlussfolgerung : die ergebnisse verdeutlichen , dass der durch eine hochdosis - radiojodtherapie hervorgerufene schaden in den speicheldrsen durch die gabe von amifostin signifikant reduziert werden kann . 
 schlsselwrter : speicheldrsen hochdosis - radiojodtherapie radioprotektion amifostin schilddrsenkarzinom introduction today , benchmark in therapy of head and neck cancer comprises percutaneous radiotherapy used alone or in conjunction with surgery . 
impairment of normal tissues in the radiation port usually results from radiation therapy , mainly affecting the salivary glands and oral mucosa [ 33 ] leading to unpleasant side effects for the patient such as xerostomia , oral mucositis , dysphagia , increase in dental caries , gustatory dysfunction , candidiasis , and neoplasia . 
 the point of reference in differentiated thyroid cancer treatment is based on total thyroidectomy and high - dose radioiodine therapy with the intention of a complete ablation of thyroid remnants . 
interestingly , it is accumulated actively by an adenosine triphosphate - ( atp - ) dependent na + / k + / 2 cl cotransport due to its similar atomic diameter and comparable electric charge [ 4 , 24 ]  . 
due to these problems , radioiodine therapy is carried out under salivary gland stimulation so as to reduce impairment of salivary gland function [ 5 , 15 , 43 , 42 , 54 ]  . 
 in view of the very good prognosis for differentiated thyroid cancer it is crucial to patient quality of life that long - term side effects of high - dose radioiodine therapy be reduced to a minimu the organic thiophosphate amifostine , also known as s - 2 - ( 3 - aminopropylamino ) - ethylphosphorothioic acid or wr1065 , represents the first of a new class of drugs that have been categorized as cytoprotective agents for about 25 years now [ 28 , 29 , 34 ]  . 
 furthermore , it is not only the first but also the only admitted ( since 1996 ) radioprotective substance for prevention of radiation - induced xerostomia following fractionated irradiation of the head and neck area . 
short - term and long - term protection by amifostine against radiation - induced damage were shown in preclinical studies using a rat parotid gland model [ 38 , 5153 ] in view of the fact that amifostine accumulates markedly in salivary glands . 
as a result of these findings , amifostine was applied in patients with head and neck cancer and salivary gland protection was proven in early clinical trials with amifostine [ 12 , 31 , 35 , 55 ]  . 
 [ 8 ] evaluated the radioprotective effect of the radical scavenger amifostine in a rabbit model and showed that amifostine appears to have comparable radioprotective characteristics on salivary gland function following high - dose radioiodine therapy , since both external radiotherapy and 131i radioiodine therapy cause their therapeutic effect by generating free radicals . 
in further investigations , the protective properties of amifostine were demonstrated by functional scintigraphy of the salivary glands following high - dose radioiodine therapy [ 7 , 10 , 11 ]  . 
 to obtain further insight into the protective effect of amifostine on salivary glands at the histological and ultrastructural level , we undertook the present animal study using conventional histology and transmission electron microscopy on parotid and submandibular gland specimens from 20 rabbits with and without amifostine pretreatment . 
two of them received neither radioiodine therapy nor amifostine injection , the other two rabbits received only amifostine intravenously without prior radioiodine therapy in order to evaluate a possible effect of amifostine on the morphology of healthy salivary gland cells ( table 1 )  . 
 the other 16 rabbits received radioiodine ( 131i ) which was given intravenously in a quantity of 1 gbq in order to ablate the thyroid and as a side effect to act on salivary gland parenchyma ( groups 3 and 4 , table 1 )  . 
prior to application of 131i all 16 animals received 4 mg dexamethasone ( fortecortin , merck , darmstadt , germany ) and 0.5 mg tropisetron ( navoban , sandoz , nrnberg , germany ) as an antiemetic strahlenther onkol 2005 no . 
eight of the 16 rabbits received 200 mg / m2 body surface amifostine ( ethyol , essex , munich , germany ) intravenously ( group 3 , table 1 ) , the other eight animals received physiological saline solution prior to high - dose radioiodine therapy ( group 4 , table 1 )  . 
 3 months after 131i application , half of the animals of each group were sacrificed and the parotid and submandibular glands were removed for light and transmission electron microscopic examination . 
 light microscopy for light microscopy , all right parotid and submandibular glands were fixed in 4% formalin , dehydrated in graded concentrations of ethanol and embedded in paraff sections ( 7 m ) were stained with toluidine blue ( ph 8.5 ) , azan , resorcin - fuchsin - thiazin picric acid , alcian blue ( ph 1 ) and using the goldner method according to romeis [ 44 ]  . 
parts of each left parotid and submandibular gland were fixed in 3.5% glutaraldehyde ( in 0.1 m srensen phosphate buffer solution at ph 7.4 ) at 4 c for 1 week . 
 parotid and submandibular glands of rabbits ( group 2 ; table 1 ) treated exclusively with amifostine showed a comparable regular structure without pathologic changes after 3 months and after 6 months . 
submandibular glands of animals that received amifostine prior to 131i showed a normal structure of the acini with correct lobular structure 3 months after irradiation ( figure 1a )  . 
 histological and electron microscopic analysis of nonirradiated parotid and submandibular gland specimens ( group 1 ; table 1 ) revealed the well - known lobular structure with densely packed acini and a well - developed excretory duct systethis was the case for the 3 - month animal as also for the 6 - month animal . 
histopathologic examination of submandibular gland of rabbits only irradiated with 131i showed cytoplasmic vacuolization with a moderate degree of pleomorphism among acinar cells , intracellular edema , signs of apoptosis of some acinar cells and nuclear pleomorphism 3 months after irradiation ( figure 1c )  . 
6 months after irradiation combined with amifostine , the submandibular gland of rabbits irradiated with 131i showed regular acinar nuclei with an entirely intact duct syste only slight edema was observed between acinar cells ( figure 1e )  . 
we carried out the present animal study using normal rabbits to elucidate morphological effects of amifostine on salivary glands following treatment with high - dose radioiodine therapy at the cellular and ultrastructural level . 
 [ 55 ] studied 67ga uptake as an indicator of radiation - induced damage in salivary glands of patients with head and neck cancer and showed that pretreatment with amifostine resulted in a significantly increased number of 67ga - negative salivary glands following irradiation . 
studies undertaken to date on head and neck tumors have yielded very promising results concerning reduction of radiation - induced salivary gland damage [ 3 , 12 , 31 , 35 ]  . 
g : sekretgranula ; balken : 3 , 75 investigation of cytoprotective properties of amifostine has a long history that can be summarized as follows : therapeutic thiol compounds have been recognized as radioprotectant substances against radiation damage to normal tissues for > 40 years [ 37 ]  . 
 preferential rapid uptake of amifostine into normal tissues such as salivary glands , liver , kidney , heart , and bone marrow occurs with up to 100 times the retention levels seen in tumor tissues [ 13 , 3941 , 66 ]  . 
this different uptake is due to higher ph and alkaline phosphatase activity in normal tissue compared to tumor tissue that causes the conversion of amifostine into active , protective thiol , wr - 1065 [ 36 ] , which in turn acts as a scavenger of oxygen free radicals inside the cell [ 1 ]  . 
interestingly , the highest tissue levels of amifostine and its metabolites are found in salivary glands [ 3941 , 5759 ] , but accumulation in thyroid tissue was found to be negligible [ 39 , 63 ]  . 
radioprotection of salivary glands by amifostine submandibular gland tissue is postulated to be relatively resistant to ionizing irradiation in the same dosage range [ 1 , 19 , 47 ]  . 
histologically , irradiated parotid and submandibular glands revealed nonspecific manifestation of severe cellular injury combined with a massive acinar loss with disorganization and some cases of enlargement of glandular ducts [ 7 , 9 , 11 , 14 , 20 , 23 , 45 , 46 , 49 , 65 ]  . 
our present animal trial with rabbits showed the following results : 3 and 6 months after irradiation with 131i , submandibular glands , and to an even greater extent parotid glands , revealed disturbed arrangement of acini with the morphological signs of apoptosis . 
serous and mucous acinar cells showed degranulation and vacuolization . submandibular and parotid glands of rabbits pretreated with amifostine prior to 131i revealed an incorrect structure of acini with intercellular edema 3 and 6 months after irradiation . 
in most cases preserved cellular organelles were found ; only some nuclei of acinar cells were pyknotic . taken together , the histopathologic and electron microscopic examination showed significantly less parenchymal damage in salivary glands of rabbits pretreated with amifostine after 3 and 6 months than in those not treated with amifostine . 
 although the morphology of the submandibular and parotid glands is very similar in rabbits and primates , the protective effects of amifostine , as shown in the present study , cannot be directly extrapolated to humans . 
it is well known that rabbits can manage for long periods without drinking water [ 16 , 56 ] , suggesting potential differences in the se - cretion efficiency of their salivary glands and throwing a different light on our results , the upshot being that it is unknown whether this animal trial can be applied to humans in the same way . 
 conclusion parenchymal damage in salivary glands following high - dose radioiodine treatment can effectively be reduced by amifostine , thus preventing negative side effects like xerostomia and enhancing the quality of life . 
treatment of the varied complications including gland massage , sialogic agents , duct probing , antibiotics , mouthwashes , good oral hygiene , and adequate hydration could become more effective due to more effective preservation of salivary gland function . however , optimum dosage and dose potency , especially in combined radiotherapy , are still under discussion [ 3 , 60 , 61 ] and it is doubtful whether the high price of amifostine will justify administration to patients . 
 strahlentherapie und onkologie original article induction chemotherapy with cisplatin , epirubicin , and paclitaxel ( cep ) , followed by concomitant radiotherapy and weekly paclitaxel for the management of locally advanced nasopharyngeal carcinoma a hellenic cooperative oncology group phase ii study * george fountzilas1 , christos tolis2 , anna kalogera - fountzila1 , charisios karanikiotis1 , maria bai2 , despina misailidou3 , epaminodas samantas4 , eleni athanassiou4 , demetris papamichael5 , periklis tsekeris2 , nikos catodritis5 , angelos nicolaou1 , george plataniotis1 , thomas makatsoris6 , pavlos papakostas7 , nikolaos zamboglou8 , john daniilidis1 background : clinical research on the treatment of nasopharyngeal cancer ( npc ) has been focused primarily on the reduction of incidence of the development of distant metastases as well as the improvement of locoregional control . 
 patients and methods : untreated patients with stage iibivb nonmetastatic npc were treated with three cycles of induction chemotherapy ( ic ) consisting of epirubicin 75 mg / m2 followed by paclitaxel 175 mg / m2 as 3 - h infusion on day 1 and cisplatin 75 mg / m2 on day 2 every 3 weeks , followed by concomitant radiation therapy ( 70 gy ) , and chemotherapy ( ccrt ) with weekly paclitaxel 60 mg / m2 . 
the most frequent side effect from ic was myelotoxicity ( 55% ) , whereas stomatitis and xerostomia were the most pronounced ( grade 3 , 4 ) toxicities during ccrt . 
the presence of epstein - barr virus ( ebv ) was detected either by in situ hybridization in tumor tissue sections or by polymerase chain reaction in the peripheral blood in 37 out of 46 patients tested ( 80% )  . 
 key words : nasopharyngeal cancer radiation therapy chemotherapy paclitaxel epirubicin epstein - barr virus strahlenther onkol 2005 ; 181 : 22330 doi 10.1007 / s00066 - 005 - 1355 - 1 induktionschemotherapie mit cisplatin , epirubicin und paclitaxel ( cep ) , gefolgt von simultaner radiochemotherapie mit wchentlichem paclitaxel , bei lokal fortgeschrittenem nasopharynxkarzinom hintergrund : die klinische forschung in der behandlung des nasopharynxkarzinoms ( npc ) fokussiert vorrangig auf die reduktion von fernmetastasen und die verbesserung der lokoregionren kontrolle . patienten und methodik : unbehandelte patienten mit nicht metastasiertem npc wurden mit drei zyklen induktionschemotherapie ( ic ) , bestehend aus epirubicin 75 mg / m2 und paclitaxel 175 mg / m2 als 3 - stndige infusion an tag 1 sowie cisplatin 75 mg / m2 an tag 2 alle 3 wochen , gefolgt von simultaner radiochemotherapie ( rct ) mit 70 gy und 60 mg / m2 paclitaxel wchentlich , behandelt . 
 * part of this work has been presented at the 15th international congress on anti - cancer treatment , february 912 , 2004 , paris , france . 1 ahepa hospital , aristotle university of thessaloniki , thessaloniki , greece , 2 university of ioannina medical school , ioannina , greece , 3 papageorgiou hospital , thessaloniki , greece , 4 agii anargiri cancer hospital , athens , greece , 5 bank of cyprus oncology center , nicosia , cyprus , 6 rio hospital , university of patras medical school , rio , patras , greece , 7 ippokration hospital , athens , greece , 8 department of radiotherapy , klinikum offenbach , offenbach , germany . received : august 17 , 2004 ; accepted : january 14 , 2005 strahlenther onkol 2005 no . 
eine epstein - barr - virus ( ebv - ) positivitt wurde durch in - situ - hybridisierung in tumorgewebe oder polymerase - kettenreaktion im peripheren blut in 37 von 46 fllen ( 80% ) nachgewiesen . 
 schlsselwrter : nasopharynxkarzinom radiotherapie chemotherapie paclitaxel epirubicin epstein - barr - virus introduction nasopharyngeal cancer ( npc ) is a tumor of epidermoid origin with biological behavior entirely different from that of other epidermoid carcinomas of the head and neck region . 
its incidence varies among different ethnic groups with the highest incidence reported in southeast asia , north africa , alaska , and mediterranean basin [ 28 , 32 ]  . 
the undifferentiated type , strictly associated with the epstein - barr virus ( ebv ) infection , predominates in asian and african areas , while the differentiated and the nonkeratinizing squamous cell variants are accounting for 5075% of npcs in the usa [ 34 ]  . 
 radiation therapy ( rt ) is considered the standard treatment for newly diagnosed nonmetastatic npc in most countries , providing complete locoregional control in > 70% of cases and a 5 - year survival rate of approximately 50% [ 22 ]  . however , 1550% of patients develop local recurrence at 5 years , while distant metastases occur in 2040% of cases at 5 years , particularly in those patients with extensive nodal involvement [ 9 , 14 ]  . 
therefore , the main goals of clinical research in the treatment of npc remain the reduction of incidence of the development of distant metastases as well as the improvement of locoregional control . 
in a randomized study [ 1 ] , led by the radiation therapy oncology group ( rtog ) , patients with locally advanced npc were randomized to concomitant chemoradiotherapy ( ccrt ) with cisplatin ( ddp ) followed by adjuvant chemotherapy or to rt monotherapy . 
the study had to be terminated prematurely , since a significant survival benefit was evident for the combined - modality group at the time of the first preplanned interim analysis . 
in general , the experience obtained from phase ii studies in advanced npc and from randomized studies suggests that npc is a chemosensitive tumor with ddp and epirubicin ( epi ) being two of the most active drugs [ 8 ]  . 
we also tried to increase the activity of the induction regimen by adding a third drug , paclitaxel , an active drug in npc [ 10 ] , into the combination of ddp and epi . 
the dosages of the three drugs and especially that of paclitaxel were based on our previous experience with a similar regimen , in which epi was substituted by doxorubicin , in patients with ovarian cancer and also , with the combination of paclitaxel , ddp and continuous infusion of 5 - fluorouracil in patients with nonnasopharyngeal head and neck cancer [ 18 ]  . 
 patients and methods eligibility criteria in order to be eligible for the study , all patients should have histologically confirmed locally advanced ( stage iibivb ) npc , performance status ( ps ) of 2 according to the eastern cooperative oncology group ( ecog ) , age 15 years , normal bone marrow , hepatic and renal function , and no history of previous or synchronous cancer except for nonmelanoma skin cancer or curatively resected in situ cervical cancer . 
 all patients were initially examined by an ent surgeon , a medical oncologist , a radiotherapist and a radiologist and staged according to the american joint committee on cancer ( ajcc ) classification [ 2 ]  . 
initial work - up included completed blood count ( cbc ) , biochemistry , ct scan or mri of the nasopharynx , base of the skull and cervical nodes , ecg , chest x - ray , liver ultrasound , or ct scan and bone scan . 
each cycle consisted of epi 75 mg / m2 over 20 min followed by paclitaxel 175 mg / m2 given as a 3 - h infusion , preceded by standard premedication , on day 1 and ddp 75 mg / m2 as a 2 - h infusion with standard prehydration on day 2 ( cep regimen )  . 
when a dose reduction was required , no dose reescalation was performed subsequently . chemotherapy was given on schedule , provided that absolute neutrophil count ( anc ) was 1.5 109 / l and platelet count 100 109 / l . 
if the hemoglobin value was < 9 g / dl , chemotherapy was administered on time , along with red blood cell ( rbc ) transfusions or erythropoietin administration as recommended by the treating physician . 
although no dose reduction was recommended for grade 12 neutropenia and / or thrombocytopenia , a 25% and 40% dose reduction of all drugs was required in case of grade 34 neutropenia and / or thrombocytopenia in all subsequent cycles . 
in case of grade 3 or 4 neutropenia and / or thrombocytopenia , treatment was interrupted and a dose reduction of 25% and 40% was required in all subsequent cycles . 
if creatinine clearance was calculated to be < 30 mg / min , then treatment was interrupted for a maximum of 2 weeks to recovery , otherwise the patient was taken off study . in case of grade 2 mucositis during ic , treatment was postponed until recovery and then chemotherapy was reinstituted with prophylactic administration of g - csf and a 25% reduction of the dose of paclitaxel and epi . 
rt was discontinued until complete recovery only in case of grade > 2 mucositis or febrile neutropenia . chemotherapy was discontinued permanently in case of grade 2 neurologic toxicity or other grade 4 nonhematologic toxicity except for alopecia . 
 radiotherapy rt was given by conventional fractionation ; 6570 gy ( in 6.57 weeks ) were delivered to the primary tumor , 65 gy to clinically involved nodes , and 50 gy to uninvolved cervical and supraclavicular areas . 
the anterior border encompassed the posterior 2 cm of the nasal cavity and maxillary antrum ; in case of anterior extension the border was moved forward 2 cm to cover ethmoids and maxillary sinuses with adequate margthe posterior border was set behind the spinal apophysis . 
 the lower margin was usually placed at the thyroid notch , but it was modified depending on the lower extent of the parapharyngeal tumor or the location of enlarged cervical lymph nodes , to avoid field abutment in the middle of tumor extension or a lymph node . 
 the lower neck and supraclavicular fossa were electively treated with a single anterior field to 4550 gy at 3 c follow - up of patients and quality assurance 1012 weeks after the completion of ccrt all patients underwent a work - up including endoscopic examination , chest x - ray and ct scan or mri of the head and neck region . 
the extracted dna was used as a template in polymerase chain reaction ( pcr ) with specific primers to amplify the region of ebna - 1 gene ( 5 - cttgggtcgccggtgtgt - 3 and 5ccttcatctccgtcatctcc - 3 )  . 
 statistical analysis according to simons two - stage optimal design , assuming that the expected overall response rate was at least 50% and the minimum acceptable response rate 30% , a sample of 15 patients were required in the first step . 
 time to treatment failure ( ttf ) was estimated from the initiation of treatment until the date progression of the disease was first diagnosed , and overall survival ( os ) from the initiation of treatment until the date of last contact or death from whatever cause , using the kaplan - meier method . 
the median relative dose intensity ( rdi ) was 0.98 for each of the three drugs . rt was initiated in 45 patients , since one patient died from sepsis during ic and one refused to start ccrt . 
even though the administration of amifostine was allowed by the protocol and particularly to those patients with xerostomia , the drug was eventually prescribed only to a few of them probably because of its high cost . 
four patients were not evaluable for response post ccrt ; two patients never started ccrt , as mentioned above , one patient died after the fifth weekly cycle of paclitaxel from heart attack without having been evaluated , and one patient refused evaluation . 
ccrt : concomitant chemoradiotherapy ; ci : confidence interval ; cr : complete response ; ic : induction chemotherapy ; ne : nonevaluable ; orr : overall response rate ; pd : progressive disease ; pr : partial response ; sd : stable disease . 
ccrt : simultane radiochemotherapie ; ci : konfidenzintervall ; cr : komplettremission ; ic : induktionschemotherapy ; ne : nicht evaluierbar ; orr : gesamtansprechrate ; pd : tumorprogression ; pr : teilremission ; sd : stable disease . 
the association of the presence of ebv with npc by in situ hybridization or by pcr was higher ( although not significant ) in patients with who type 3 ( 19 out of 20 patients , 95% ) than in patients with who type 2 ( eight out of 13 patients , 61.5% ) or with who type 1 ( eleven out of 13 patients , 85% )  . 
two large randomized trials in patients with locally advanced npc [ 13 , 25 ] have shown an improvement on relapse - free survival ( rfs ) with the incorporation of ic into rt compared to rt monotherapy . 
chemotherapeutic agents used in the aforementioned studies consisted of ddp , epi , and continuous infusion of fluorouracil or bleomyc the cr rate of 15% observed in the present study by the cep regimen appeared to be similar to that reported by others in single - institution trials [ 5 , 9 , 17 ] or in neoadjuvant randomized trials [ 4 , 15 , 25 ] , but it was inferior to the 47% achieved by the international nasopharyngeal carcinoma study group with the combination of ddp , epi , and continuous infusion of bleomycin ( bep ) [ 13 ]  . 
additionally , 14 treatment - related deaths were recorded among 171 patients ( 8.2% ) assigned to ic plus rt ar furthermore , the cr rate of 66% achieved post ccrt in our patients was in the range reported in other studies using combined - modality programs . 
at any rate , we have to keep in mind that the assessment of response is often complicated by the presence of residual mucosal nasopharyngeal thickening or following rt from post - radiation fibrosis and results may often be overor underestimated . 
it has been suggested that a uniform treatment schedule should be applied to npc patients with different histological subtypes to better delineate the role of combined - modality treatment in different entities of npc [ 3 ]  . 
 the cep regimen as used in the present study was well tolerated , since most of the patients received adequate ic , while rdi of the three drugs was 0.98. 
the survival benefit with the administration of chemotherapy concomitantly with rt over rt in npc patients has been shown in single - institution series [ 11 ] and in three randomized trials [ 1 , 6 , 38 ] , although the superiority of ccrt could not be demonstrated in another randomized trial [ 21 ]  . 
in addition to single trials , the beneficial effect of chemotherapy combined with rt over rt monotherapy was clearly demonstrated in a number of meta - analyses [ 12 , 20 ]  . 
in our study , 2 - year survival and 2 - year locoregional control rates were in accordance with those reported in other studies with similar design [ 16 , 30 ]  . 
furthermore , paclitaxel was shown to be a potent rt sensitizer in a variety of human cell lines including those derived from squamous cell head and neck cancer [ 23 , 26 ]  . 
it was postulated that important mechanisms for its radiosensitization are a cell - cycle blockade at the g2 / m - transition [ 31 , 36 ] and enhanced tissue oxygenation [ 26 ]  . 
paclitaxel as single agent or in combination with other agents has been tested in phase iii studies [ 17 , 35 ] on patients with locally advanced head and neck tumors of various primary sites . 
induction chemotherapy and ccrt in nasopharyngeal cancer paclitaxel administered as a 120 - h continuous infusion every 3 weeks during the course of rt in a cohort of 33 such patients . in the present study , ccrt was well tolerated . 
in the rtog study [ 1 ] , in which ddp was used at a dose of 100 mg / m2 on days 1 , 22 and 42 , the incidence of severe stomatitis , nausea and vomiting was 29% , 14% and 11% , respectively . 
 [ 6 ] , despite the fact that ddp was administered weekly and at a lower dose ( 40 mg / m2 ) , severe nausea / vomiting was reported in 12% of patients . 
of note , in the same study 63% of patients suffered from grade 3 weight loss ( 1020% of their initial body weight ) and 11% from grade 4 ( > 20% )  . 
however , it has to be mentioned that half of our patients who received paclitaxel concomitantly with rt discontinued chemotherapy , especially during the last 23 weeks , mainly because of myelotoxicity . 
therefore , an interesting part of our study was the attempt to detect the presence of ebv in the tumor tissue and / or in the peripheral blood of our patients . 
among our patients , eber expression was not observed exclusively in those with nonkeratinizing tumors , since two out of seven who type 1 tumors were also eber - positive . 
it has been demonstrated that who type 1 tumors are frequently associated with ebv in endemic areas , whereas this does not hold true in nonendemic areas where smoking and alcohol intake are considered the primary causative factors for carcinogenesis [ 29 , 37 ]  . 
it is noteworthy , that no significant differences were found , among our patients with eber - positive or eber - negative tumors in terms of cr rate or median ttf . 
notably , ebna - 1 in peripheral blood was detected in eight out of eleven patients with who type 1 and in 20 out of 25 ( 80% ) with nonkeratinizing tumors . 
these results are in accordance with those found in a similar study conducted in asian population [ 24 ] in which ebna - 1 dna - positive rates in peripheral blood of the who type 2 and type 3 npc patients were 71% . 
nevertheless , there are important issues , such as the optimal drug or schedule of administration concomitantly with rt , the optimal type of rt etc . , which have to be clarified through prospective randomized studies . 
this regimen was selected because it is less toxic than other active regimens , such as bep , and is accompanied by reduced hospitalization time compared to wayne state regimen ( ddp and 5 - day continuous infusion of fluorouracil )  . 
taking our increasing experience with the use of weekly ddp in ccrt of patients with nonnasopharyngeal head and neck cancer and the low cost accompanied with its use into account , we substituted paclitaxel by weekly ddp . 
 acknowledgments the authors would like to thank dimitrios karanikolas , md , and ioannis tsifountoudis , md , department of radiology , aristotle university of thessaloniki , thessaloniki , for reviewing all imaging material , evita fragou for monitoring the study , maria moschoni for coordinating data management , and stella dallidou for secretarial assistance . 
 strahlentherapie und onkologie originalarbeit volumetrische vernderungen der mamma whrend der radiotherapie ist vor boostbestrahlung mit elektronen eine nachplanung erforderlich ? daniela trog1 , stephan garbe1 , gtz lutterbey1 , christiana ltter1 , peter barwig1 , ilse boldt1 , anja stolz2 , oliver richter3 , hans heinrich schild1 , heinrich schller1 hintergrund und ziel : eine radiotherapie der mamma induziert eine gewebereaktion mit daraus resultierendem dedieses dem fhrt zu einer volumenzunahme der mamma . 
 patienten und methodik : bei 140 patientinnen mit mammakarzinom nach brusterhaltender therapie erfolgte vor , whrend und / oder nach der bestrahlung eine ct - planung , um die volumenvernderungen whrend der bestrahlung zu evaluieren . 
gemessen am ausgangsvolumen wurden die patientinnen in drei subgruppen unterteilt : gruppe 1 ( n = 47 ) : 670 cm3 , gruppe 2 ( n = 46 ) : 671999 cm3 und gruppe 3 ( n = 47 ) : 1 000 cm3 brustvolumen . 
bezogen auf die drei subgruppen ergaben sich folgende mittlere volumenzunahmen : gruppe 1 : 53 cm3 ( 3120 cm3 ) , gruppe 2 : 85 cm3 ( 20200 cm3 ) und gruppe 3 : 105 cm3 ( 5340 cm3 )  . 
je nach volumenzunahme der brust resultierte eine nderung der herdtiefe um bis zu 1 , 0 c schlussfolgerung : aufgrund der interkurrenten volumennderungen unter bestrahlung erscheint eine zweite ct - untersuchung zur nachplanung vor boostbestrahlung sinnvoll . 
 schlsselwrter : mammakarzinom ct - planung elektronenboost radiogen induziertes dem strahlenther onkol 2005 ; 181 : 2559 doi 10.1007 / s00066 - 005 - 1316 - 8 volumetric changes of the breast during radiotherapy . 
the aim of the present study was to quantify this increase and analyze its effect on the electron boost technique . patients and methods : 140 patients with breast cancer treated with breast - conserving surgery underwent ct planning before , during and / or after radiotherapy in order to evaluate breast volume changes due to radiotherapy . 
determination of the breast volume was achieved using an interpolation algoriththree subgroups were analyzed : group 1 ( n = 47 ) : 670 cm3 , group 2 ( n = 46 ) : 671999 cm3 , and group 3 ( n = 47 ) : 1000 cm3 breast volume . 
corresponding to the volume increase , depth of the boost target volume changed up to 1.0 c conclusion : as radiotherapy may lead to a significant increase in breast volume , it seems appropriate to perform a second planning ct after about 40 gy in order to optimize dose distribution for boost irradiation . 
 alter bei diagnose anzahl der entfernten lk zeitraum zwischen op und rt - beginn ( monate ) tumorgre ( cm ) mittelwert spannweite median 3 , 14 2079 042 16 16 3 , 0 patientinnen chemotherapie vor rt anihormonelle therapie whrend rt hormonstatus 50 positiv 111 nein negativ zielle fixierungen . 
zur planung der bestrahlung wurde eine spiral - ct durchgefhrt , wobei die mamma an drei punkten , nmlich im bereich der feldmitte , der mamille und der narbe , mit drhten markiert wurde . 
die schichtdicke der spiral - ct betrug 1 c die erste ct - planung erfolgte vor beginn der radiotherapie , eine weitere im allgemeinen nach 40 gy ( median : 49 gy , spannweite : 3255 gy )  . 
obwohl keine generellen richtlinien ber die indikation zur boostbestrahlung vorliegen , erhalten im allgemeinen patientinnen mit risikofaktoren eine kleinrumige aufsttigung der primrtumorregion mit einer dosis von 1016 gy [ 1 , 2 , 10 , 20 ]  . 
 patienten und methodik bei insgesamt 140 patientinnen im alter zwischen 20 und 79 jahren ( median : 58 jahre ) erfolgte nach brusterhaltender tumorektomie eine perkutane radiotherapie der restbrust ( gesamtdosis 50 gy ) mit anschlieender kleinrumiger aufsttigung der primrtumorregion , wobei auf eine antidematse therapie verzichtet wurde . 
weitere details zum patientengut ( alter bei diagnose , tumorgre , anzahl entfernter lymphknoten , zeitraum zwischen operation und bestrahlungsbeginn , durchfhrung einer chemotherapie , hormonstatus , antihormonelle therapie whrend der bestrahlung ) sind in tabelle 1 aufgelistet . 
 die bestrahlung erfolgte an zwei linearbeschleunigern ( siemens mevatron md2 und kd ) mit photonenstrahlung und den energien 6 mv ( n = 134 ) und 10 mv ( n = 6 )  . 
die homogene dosisverteilung gem icru 50 wurde durch die bestrahlungstechnik mittels opponierender tangentialfelder mit und ohne divergenzausgleich bei unterschiedlicher gewichtung und einem fokus - isozentrum - abstand von 100 cm unter verwendung statischer keilfilter erreicht . 
 fr unsere auswertungen teilten wir die patientinnen in drei gruppen ein : ( cid : 127 ) gruppe 1 : patientinnen mit initialen volumina von 670 cm3 ( n = 47 ) , ( n = 47 )  . ( cid : 127 ) gruppe 2 : patientinnen mit brustvolumina zwischen 671 und 999 cm3 ( n = 46 ) , ( cid : 127 ) gruppe 3 : patientinnen mit brustvolumina von 1 000 cm3 dabei ergaben sich fr die gruppen unterschiedliche altersverteilungen : in gruppe 1 lag das mittlere alter bei 51 jahren ( 2070 jahre ) , in gruppe 2 bei 59 jahren ( 3579 jahre ) und in gruppe 3 bei 63 jahren ( 4278 jahre )  . mittels des statistikprogramms spss 12.0 fr windows wurden die korrelationskoeffizienten zwischen der volumenzunahme und der tumorgre , dem tumorsitz , der anzahl der entfernten lymphknoten , dem zeitraum zwischen beginn der radiotherapie und operation , dem hormonstatus , einer antihormonellen therapie whrend der bestrahlung , einer vorangegangenen chemotherapie sowie dem alter der patientinnen bei diagnose ermittelt . 
die durchschnittliche zunahme variierte zwischen den gruppen : ( cid : 127 ) in gruppe 1 ergab sich eine durchschnittliche zunahme um 53 cm3 ( 12 , 3% ; spannweite 3120 cm3 ; standardabweichung 8 , 8 )  . 
 ( cid : 127 ) in gruppe 2 fand sich eine durchschnittliche volumenzunahme um 85 cm3 ( 10 , 5% ; spannweite 20200 cm3 ; standardabweichung 5 , 8 )  . 
der unterschied zwischen den gruppen 1 und 2 ( p = 0 , 287 ) war nicht bedeutsa insgesamt wiesen 27 / 140 patientinnen eine volumenzunahme von > 15% , 15 patientinnen von > 20% , acht von > 30% und fnf von > 35% auf . 
 korrelationskoeffizient : absoluter anstieg ( % ) anzahl der entfernten lk chemotherapie hormonstatus antihormonelle therapie zeitraum zwischen op und rt - beginn tumorgre tumorsitz alter bei diagnose 0 , 443 0 , 240 0 , 912 0 , 216 0 , 472 0 , 280 0 , 771 0 , 013a a die korrelation ist auf dem niveau von 0 , 05 ( zweiseitig ) signifikant strahlenther onkol 2005 no . 
 diskussion eine postoperative radiotherapie impliziert eine dreidimensionale bestrahlungsplanung mit einem ct - gesttzten planungssystem , um die homogene verteilung der dosis in der behandelten brust zu gewhrleisten [ 11 ]  . 
diese ct wird vor beginn der radiotherapie angefertigt . whrend einer bestrahlung der brust entwickelt sich ein radiogenes dedas ausma dieser akuttoxizitt der haut und des gewebes ist laut literatur von verschiedenen faktoren wie u.a. 
der brustgre und dem gewicht , der bestrahlungstechnik , dem alter der patientin , der tumorgre , nikotinabusus , dem bestrahlungsvolumen und / oder der bestrahlungsdosis abhngig [ 6 , 15 , 19 ]  . hauptursache fr dieses dem sind inflammatorische reaktionen des gewebes , die zu permeabilittsstrungen mit vermehrter exsudation von flssigkeit in das intramammre gewebe fhren . 
anhand von mrt - untersuchungen der brust unter bestrahlung lsst sich in der t2 - wichtung , neben der deutlichen verdickung der kutis , ein verstrktes enhancement des intramammren gewebes durch den erhhten wassergehalt nachweisen . 
 die gebruchlichste technik der boostbestrahlung ist die eines elektronenstehfeldes , weitere mgliche techniken umfassen die bestrahlung ber tangentiale modifizierte felder mit photonen , mittels interstitieller brachytherapie oder durch einen intraoperativen elektronenboost [ 9 , 13 , 14 ]  . 
untersuchungen hinsichtlich der lokalisation eines rezidivs in bezug auf den primrtumor weisen aber darauf hin , dass sich > 50% aller rezidive innerhalb des ehemaligen operationsgebiets , aber auerhalb des boostvolumens befinden [ 1 , 3 , 5 , 10 , 21 , 22 , 24 ]  . 
unter der magabe , dass mit der boostbestrahlung ein wichtiges instrument zur lokalen tumorkontrolle gegeben ist , erscheint es umso wichtiger , dass der ehemalige tumorsitz optimal erfasst und bestrahlt wird . 
als hinweis fr eine exakte lokalisation des tumorbetts zeigten die studien zur intraoperativen boostbestrahlung sowohl hinsichtlich der lokalrezidivrate als auch des krankheitsspezifischen berlebens deutlich bessere ergebnisse als nach konventioneller applikation des elektronenboosts [ 7 , 18 ]  . 
bei erheblichen volumenzunahmen muss davon ausgegangen werden , dass ohne erneute ct - untersuchung , ab einer einstrahldosis von mindestens 40 gy , die gefahr einer fehlerhaften lokalisation und unterdosierung des boosts besteht . 
im extremfall haben wir volumenzunahmen von > 30% ( n = 8 / 140 ) beobachtet , wobei sich die herdtiefe um maximal 1 , 0 cm vernderte und bei allen acht patientinnen die elektronenenergien angepasst werden mussten . 
can the addition of regional radiotherapy counterbalance important risk factors in breast cancer patients with extracapsular invasion of axillary lymph node metastases ? strahlenther onkol 2003 ; 179 : 6616 . 
can patient - , treatmentand pathology - related characteristics explain the high local recurrence rate following breast - conserving therapy in young patients ? eur j cancer 2003 ; 39 : 93244 . 
4 urban & vogel strahlentherapie und onkologie current discussion combined - modality treatment and organ preservation in bladder cancer do molecular markers predict outcome ? christian weiss1 , franz rdel1 , ina wolf1 , thomas papadopoulos2 , dirk g . 
schrott3 , rolf sauer1 , claus rdel1 purpose : in invasive bladder cancer , several groups have reported the value of organ preservation by a combined - treatment approach , including transurethral resection ( tur - bt ) and radiochemotherapy ( rct )  . 
clinical factors are limited in their potential to identify patients most likely to respond to rct , thus , additional molecular markers for predicting treatment response of individual lesions are sorely needed . 
 patients and methods : the apoptotic index ( ai ) and ki - 67 index were evaluated by immunohistochemistry on pretreatment biopsies of 134 patients treated for bladder cancer by tur - bt and rct . 
expression of each marker as well as clinicopathologic factors were then correlated with initial response , local control and cancer - specific survival with preserved bladder in univariate and multivariate analysis . 
 key words : bladder cancer radiochemotherapy response prediction apoptosis proliferation strahlenther onkol 2005 ; 181 : 21322 doi 10.1007 / s00066 - 005 - 1417 - 4 multimodale organerhaltende therapie des blasenkarzinoms . 
knnen molekulare marker den therapieerfolg vorhersagen ? hintergrund : mehrere arbeitsgruppen konnten zeigen , dass eine multimodale organerhaltende behandlung des invasiven blasenkarzinoms unter einsatz der transurethralen resektion ( tur - bt ) und anschlieender radiochemotherapie ( rct ) zu therapieergebnissen fhrt , die denen der primren zystektomie gleichwertig sind . 
prdiktive molekulare marker sind hier dringend notwendig . patienten und methodik : der apoptoseindex ( ai ) und der ki - 67 - index wurden an prtherapeutischen biopsien von 134 patienten , die mittels tur - bt und rct behandelt wurden , immunhistochemisch bestimmt . 
die expression beider marker sowie klinische faktoren wurden anschlieend mit der initialen ansprechrate , der lokalen kontrolle und dem krankheitsspezifischen berleben mit intakter blase univariat und multivariat korreliert . ergebnisse : der median des ai aller patienten betrug 1 , 5% ( spanne : 0 , 27 , 4% )  . 
prdiktive faktoren fr das komplette ansprechen waren die t - kategorie ( p < 0 , 0001 ) , der re1 department of radiation oncology , university of erlangen , germany , 2 department of pathology , university of erlangen , germany , 3 department of urology , university of erlangen , germany . 
molecular markers for predicting treatment response in bladder cancer sektionsstatus ( p = 0 , 02 ) , die lymphgefinvasion ( p = 0 , 01 ) und der ki - 67 - index ( p = 0 , 02 )  . 
die t - kategorie war der strkste unabhngige prognostische faktor fr alle drei endpunkte in der multivariaten analyse . schlussfolgerung : die indizes fr die prtherapeutische apoptose und ki - 67 prdizieren einen gnstigen verlauf nach tur - bt und rct . 
molekulare marker knnen bei der selektion von patienten fr ein organerhaltendes therapieverfahren hilfreich se schlsselwrter : blasenkarzinom radiochemotherapie prdiktion apoptose proliferation introduction bladder cancer is the second most common malignancy of the genitourinary tract with > 15 , 000 newly diagnosed cases each year in germany [ 2 ]  . 
in the last years , sophisticated techniques for urinary diversion have been developed to improve quality of life , but even the construction of an orthotopic neobladder with continent urinary diversion cannot substitute for the patients original bladder . 
 therefore , organ - sparing approaches for bladder cancer , as already established in the treatment of other malignancies , such as breast , anal or laryngeal cancer [ 9 , 10 , 14 , 16 , 31 , 34 , 44 , 46 , 68 , 69 , 73 ] , have been initiated by several groups in the last 20 years . 
after conservative surgery using transurethral resection of the bladder tumor ( tur - bt ) and concomitant radiochemotherapy ( rct ) , 5 - year survival rates in the range of 5060% have been published in these series , and about three quarters of the surviving patients maintained their own bladder [ 51 ]  . 
in the large erlangen series , patients with nonresponding tumors showed a 5 - year disease - specific survival rate of only 21% , even when salvage cystectomy could be performed , and > 40% developed distant metastases within the first 2 years [ 52 ]  . 
 several markers have been linked to radioand chemosensitivity of bladder cancer cells , including p53 , prb , cyclin d1 , p21 and bcl - 2 as key protein regulators of the cell cycle and the apoptotic pathway as well as markers of tumor cell proliferation . 
a former study of our group , performed in a selected and small group of 70 patients with residual tumor after initial tur - bt , assessed the molecular markers p53 , bcl - 2 , ki - 67 and apoptosis for their predictive and prognostic significance in combined - modality treatment for bladder cancer [ 53 ]  . 
since only pretreatment levels of apoptosis and ki - 67 index were significantly related to response and local control in our earlier series , this consecutive study on 134 unselected patients with long - term follow - up focused on these markers . 
of these , 106 patients had muscle - invasive bladder cancer and 26 patients high - risk t1 tumors ( i.e. , grade 3 , multifocal or multiple recurrent tumors )  . 
having been compiled for research purposes , this group represents patients , who received rct patients treated with radiotherapy alone have been excluded , and for whom pretreatment archival paraffin - embedded tissue blocks and a complete clinical follow - up were available . 
 the aim of our study was to investigate the role of biological markers as possible predictors for initial response , local control with preserved bladder , and cause - specific survival . 
the unique features of this group are , that ( a ) treatment was homogeneous , ( b ) patients were treated at a single institution so that staging and patient selection were consistent , and ( c ) response to rct could be assessed 6 weeks after completion of therapy by a restaging tur - bt . 
the t - category , grading , resection status , lymphovascular invasion , and the presence or absence of associated tis and multifocality were derived from pathologic evaluation of the initial tur - bt ( table 1 )  . 
radiotherapy was initiated 46 weeks after initial tur - bt , using at least 6 - mv photons and a four - field box technique with individually shaped portals and daily fractions of 1.82.0 gy on 5 consecutive days per week . 
 following complete resection ( r0 ) , the total dose prescribed to the bladder tumor was 55.80 gy , after incomplete resection ( r1 = microscopic , r2 = macroscopic residual tumor ) table 1 . 
in case of histologically proven complete response ( pcr ) , patients were followed up at 3 - month intervals , including cystoscopy , biopsies of all suspected areas , and urine cytology . 
in case of a residual tumor ( no response or only partial response ) at restaging tur - bt , or the occurrence of an invasive local failure during follow - up , a salvage cystectomy was recommended . 
molecular markers for predicting treatment response in bladder cancer triphosphate ( dutp ) nick - end - labeling ( tunel ) technique ( in situ cell death detection kit , boehringer mannheim gmbh , mannheim , germany )  . 
briefly , paraffin - embedded tissue in 5 - mm sections was mounted on silane - coated slides , dewaxed , rehydrated in graded alcohols , and washed with phosphate - buffered saline ( pbs )  . 
the samples were denatured by 15 - min exposure to proteinase k ( 20 mg / ml ) at room temperature and then incubated with tunel - reaction mixture in a humidified chamber for 60 min at 37 c in the dark according to the manufacturers recommendation , followed by biotinylated mouse anti - fluorescein antibody ( dako , hamburg , germany , dilution 1 : 50 , incubated for 1 h at room temperature )  . 
after incubation with an avidin / biotinylated alkaline phosphatase solution ( dako ) for 30 min the samples were exposed to fast - red solution for 10 min and subsequently counterstained with hematoxylin ( 37% )  . 
a minimum of 1 , 000 tumor cells were counted in ten random regions using an image system ( optimas 6.2 , stemmer pc systeme , puchheim , germany )  . 
to undo the masking effect of formalin fixation , all sections were overlain with 10 mm citrate buffer ( ph 6.0 ) and heated for 15 min in a microwave oven at 750 w . 
when the slides and buffer were at room temperature , the slides were rinsed in pbs , and nonspecific binding sites were blocked with 5% bovine serum albumin in pbs . 
 after washing in pbs , the following primary antibody was applied and incubated for 2 h at room temperature : mib - 1 , monoclonal mouse antibody , that reacts to a nuclear antigen ( ki - 67 ) present in all phases of the cell cycle with exception of g0 / g1 and early s - phase ( dianova , hamburg , germany , dilution 1 : 30 )  . 
the samples were next incubated with biotinylated rabbit anti - mouse secondary antibody ( dianova , dilution 1 : 50 , incubated for 1 h at room temperature ) followed by an avidin / biotinylated alkaline phosphatase and fast - red solution as described before . 
ki - 67 labeling index , defined as the percentage of positive carcinoma cells , was determined after evaluation of at least 1 , 000 carcinoma cells for ki - 67 immunoreactivity using the previously described image syste statistical analysis continuous variables were compared between the groups using the t - test for independent samples and , in case of more than two groups , the one - way anova . 
101 patients ( 76% ) showed a complete response , six patients ( 5% ) had superficial and 25 patients ( 19% ) muscleinvasive residual tumors ( figure 1 )  . 
5 - year local control with preserved bladder , cause - specific survival , cause - specific survival with preserved bladder , and overall survival for the entire cohort of 134 patients were 45% , 59% , 52% , and 53% , respectively . 
 predictive factors for initial response to radiochemotherapy and local control with respect to the endpoint complete response at restaging tur - bt , the t - category ( p < 0.0001 ) , r - status ( p = 0.02 ) , lymphovascular invasion ( p = 0.01 ) , and ki - 67 index ( p = 0.02 ) significantly predicted response ( table 2 )  . 
the corresponding figures for the ki - 67 index were 57% for highly proliferating tumors , compared with only 35% local control rate for tumors with a low proliferation index ( p = 0.05 , figure 3 )  . 
in univariate analysis t - category ( p < 0.0001 ) , r - status ( p = 0.002 ) , and lymphovascular invasion ( p = 0.004 ) were significantly related to cause - specific survival . 
using the clinically meaningful endpoint of the percentage of patients who survived 5 years with their bladder preserved , t - category ( p < 0.0001 ) , r - status ( p = 0.02 ) , lymphovascular invasion ( p = 0.02 ) , and the ki - 67 index ( p = 0.04 ) had a significant prognostic value ( table 4 )  . 
if overall survival ( 53% at 5 years , not shown ) was chosen as endpoint and data were compared using the log - rank test , t - category ( p < 0.0001 ) , r - status ( p = 0.009 ) , and lymphostrahlenther onkol 2005 no . 
 multivariate analysis in multivariate analysis for treatment response , local control and cause - specific survival with preserved bladder , only t - category remained an independent prognostic factor ( table 5 )  . 
 the ki - 67 index was the second most important factor and showed borderline significance for the first two endpoints al > median 60% al > median 39% at risk : months figure 2 . 
association of clinical factors and markers with cause - specific survival and cause - specific survival with preserved bladder following tur - bt and rct in 134 patients with bladder cancer . 
zusammenhang klinischer und biologischer faktoren mit dem krankheitsspezifischen berleben nach 5 jahren und dem krankheitsspezifischen berleben mit erhaltener blase nach tur - bt und rct bei 134 patienten mit harnblasenkarzinoabkrzungen s . 
multivariate analyse prdiktiver faktoren in bezug auf das initiale therapieansprechen , die lokoregionre kontrolle und das krankheitsspezifische berleben mit blasenerhalt von 134 patienten mit harnblasenkarzino p - value reference value for odds ratio odds ratio 95% confidence interval for odds ratio discussion variable treatment response t - category ki - 67 local control t - category ki - 67 cause - specific survival with preserved bladder t - category ki - 67 with more experience acquired regarding organ - sparing treatment in bladder cancer , future clinical and basic research will focus on two main topics : ( a ) the optimization of the treatment modalities , including incorporation of new cytotoxic agents , and ( b ) the proper selection of patients who will most probably benefit from the respective treatment alternatives . 
as shown in our current analysis , clinical criteria helpful in determining patients for bladder preservation include such variables as an early tumor stage , a visibly and microscopically complete tur - bt ( r0 , r1 ) , and absence of lymphovascular invasion . 
we could thus confirm our earlier results that were based on a much smaller and more selected cohort of patients [ 53 ]  . numerous other studies have addressed the predictive and prognostic significance of genetic alterations associated with the apoptotic susceptibility , cell - cycle alterations , and proliferation in bladder cancer patients . 
table 6 summarizes the available data on molecular markers that have been investigated for their potential role in predicting favorable or unfavorable outcome after rt / rct or cystectomy , respectively . 
overall , these findings do not yet confirm that abnormal expression of any of these proteins unequivocally predicts tumor response to rt / rct with possibly one exception : higher rates of spontaneous apoptosis were significantly related to better initial response and better local control with bladder preservation in all but one study . 
in vitro studies suggest that radiation - induced apoptosis closely correlates with radiosensitivity , and that the spontaneous apoptotic rate of untreated tumor cell lines may also correlate with the induced apoptotic rate and radiosensitivity [ 38 , 62 ]  . 
 a more recent study from moonen et al . , that used radiotherapy as definitive treatment , also demonstrated that an apoptosis level above the median was significantly associated with better local control [ 39 ]  . 
it is now becoming increasingly clear , that the inability to undergo apoptosis due to overexpression of bcl - 2 or other inhibitors of apoptosis , such as survivin , may predict local failure after irradiation and chemotherapy . 
this is in accordance with other series in bladder cancer , that demonstrated a significant association of ai with dna aneuploidy , higher t - category , higher grade , and proliferation [ 6 , 22 , 37 ]  . 
it is our conclusion from all these findings that the biological profile of bladder tumors with a high spontaneous ai is that of a more aggressive phenotype and a worse outcome if treated by surgery only , yet with enhanced radiation and chemotherapy response . 
ai : apoptotic index ; mi : mitotic index ; pcna : proliferating cell nuclear antigen ; rct : radiochemotherapy ; rt : radiotherapy ; x : results of the present study . 
given all these results , it is interesting that our group is the only one that found a high proliferative index to be associated with a favorable outcome in univariate and multivariate analysis . 
 this is consistent with the clinical experience , whereby rapidly proliferating tumors are more sensitive to irradiation and chemotherapy than those growing slowly , yet may also be associated with rapid tumor repopulation . 
it is our hypothesis , that concomitant chemotherapy may have inhibited rapid tumor repopulation during the course of fractionated radiotherapy , while this phenomenon might have reduced the probability of tumor control in the radiotherapy - alone series . 
molecular markers for predicting treatment response in bladder cancer sparing approach using tur - bt and rct are those with early - stage tumors and a high ai and ki - 67 index . 
 strahlentherapie und onkologie original article is a diagnostic ct of the brain indicated in patients with choroidal metastases before radiotherapy ? dirk bottke1 , thomas wiegel1 , klaus - martin kreusel2 , stefan hcht1 , wolfgang hinkelbein1 background and purpose : there is no evidence in the literature about the incidence of synchronous brain metastases in patients with choroidal metastases . 
this is of major importance , because the radiation fields of choroidal metastases and , later on , brain metastases , if treated consecutively , are partly overlapping , thus potentially increasing the rate of late side effects such as brain necrosis . 
 patients and methods : 50 patients with choroidal metastases were enrolled into a study of the arbeitsgemeinschaft radiologische onkologie of the german cancer society ( aro 95 - 08 ) with standardized 40 gy radiotherapy , 2 gy single dose . 
no patient showed clinical signs of brain metastases . results : 13 out of 50 patients ( 26% ) had brain metastases in the cct leading to radiotherapy of the brain and choroidal metastases in one volume . 
the incidence is about 25% , and the diagnosis of brain metastases results in a different target volume : the whole brain including the posterior parts of the eyes compared to the posterior parts of the eyes alone . 
 key words : choroidal metastases brain metastases cranial computed tomography strahlenther onkol 2005 ; 181 : 2514 doi 10.1007 / s00066 - 005 - 1336 - 4 ist eine diagnostische ct des schdels bei patienten mit aderhautmetastasen vor radiotherapie indiziert ? hintergrund und ziel : bislang gibt es in der literatur keine angaben zur inzidenz synchroner hirnmetastasen bei patienten mit aderhautmetastasen . 
 patienten und methodik : 50 patienten mit aderhautmetastasen wurden in eine studie der arbeitsgemeinschaft radiologische onkologie der deutschen krebsgesellschaft ( aro 95 - 08 ) zur standardisierten strahlentherapie mit 40 gy , einzeldosis 2 gy , eingeschlossen . 
 schlsselwrter : aderhautmetastasen hirnmetastasen kraniale computertomographie 1 department of radiation oncology and radiotherapy , charit campus benjamin franklin , berlin , germany , 2 eye clinic berlin - marzahn , berlin , germany . 
the median survival time of these patients is about 612 months , but 10% of the patients with breast cancer survive > 5 years [ 21 , 22 ] , and therefore , long - term palliative treatment is important for the patients quality of life . 
percutanous irradiation is the treatment of choice resulting in high remission rates and significant improvement of visual acuity [ 18 , 21 , 26 ]  . there is no evidence in the literature about the incidence of synchronous brain metastases in patients with choroidal metastases . 
this is of major importance , because the standard radiation fields for the treatment of choroidal metastases and , later on , brain metastases are partly overlapping , thus potentially increasing the rate of late side effects such as brain necrosis . 
 in 1994 , we initiated a prospective , nonrandomized monocentric study together with the arbeitsgemeinschaft radiologische onkologie ( aro ) of the german cancer society to evaluate the efficacy and safety of a standardized treatment with 40 gy , since there was a lack of prospective data in the literature for uniformly treated patients . 
one patient refused rt after 4 gy , four patients died due to metastatic disease before finishing rt , and in one patient the diagnosis was changed to malignant uveal melanoma . 
the majority of patients had primary breast cancer ( 31 / 50 [ 62% ] ) or lung cancer ( 13 / 50 [ 26% ] ) , while the remainder had primary prostatic ( 2% ) , cervical ( 2% ) or ovarian carcinoma ( 2% ) , lymphoma ( 2% ) , or an unknown primary tumor ( 4% )  . 
 in nine patients ( 18% ) choroidal metastasis was the first clinical manifestation of their malignant disease ; all of these could be shown to suffer from metastatic lung cancer . 
 no patient showed clinical signs of brain metastases . treatment in patients without brain metastases in cct , rt was performed with 6 - mev photons using a lens - sparing technique . 
in case of unilateral involvement a unilateral field without sparing of the contralateral choroid was employed , thus delivering 5070% of the prescribed dose to the posterior contralateral choroid ( figure 1a )  . 
diagnostic cct in patients with choroidal metastases results 13 out of 50 patients ( 26% ) had brain metastases in the cct leading to rt of the brain and the choroidal metastases in one target volume . 
in detail , 7 / 31 ( 23% ) patients with breast cancer , 4 / 13 patients ( 31% ) with lung cancer , and 2 / 6 patients ( 33% ) with other tumors had evidence of brain metastases in the cct ( table 2 )  . 
different target volumes : the posterior parts of the eyes alone ( a ) compared to the whole brain including the posterior parts of the eyes ( b )  . 
 discussion the aim of our prospective study ( aro 95 - 08 ) was to characterize the therapeutic outcome and the side effects of standardized 40 gy rt for choroidal metastases , and the goal of this part of evaluation was to determine the frequency of synchronous brain metastases in patients with choroidal metastasis . 
to date , there is no evidence in the literature about this incidence , although this is of major importance , because the radiation fields of the treatment of choroidal metastases and , later on , treated brain metastases are partly overlapping , thus increasing the rate of late side effects . 
 ct of the brain has a well - documented accuracy in detecting metastatic tumors and has been described as being of value in the staging of patients who were free of neurologic symptoms [ 11 , 20 , 24 ]  . 
recently , magnetic resonance imaging ( mri ) has also started to be used for diagnosing brain tumors , and contrast - enhanced mri has been demonstrated to be very sensitive to small lesions and documented to have a higher sensitivity than ct [ 19 , 23 ]  . 
on the other hand , ct is less expensive , with a sufficient sensitivity . palliative radiotherapy of the whole brain ( wbrt ) with or without stereotactic rt is the standard treatment for patients with symptomatic and asymptomatic brain metastases [ 3 , 4 , 10 , 16 ]  . 
the incidence is about 25% , and the diagnosis of brain metastases results in a different target volume : the whole brain including the posterior parts of the eyes compared to the posterior parts of the eyes alone . 
 strahlentherapie und onkologie original article postoperative irradiation of incompletely excised gemistocytic astrocytomas clinical outcome and prognostic factors jadwiga nowak - sadzikowska , bogdan gli nski , teresa szpytma , elzbieta pluta1 background and purpose : although gemistocytic astrocytomas are considered slow - growing tumors , they often behave aggressively and carry the least favorable prognosis among low - grade astrocytomas . 
the aim of this study is to evaluate the outcomes and prognostic factors of patients with incompletely excised gemistocytic astrocytomas irradiated postoperatively . patients and methods : records of 48 patients with incompletely excised gemistocytic astrocytoma , irradiated between 1976 and 1998 at the department of radiation oncology , maria skodowska - curie memorial cancer center , cracow , poland , were reviewed . 
 the total dose ranged from 50 to 60 gy ( mean : 59.35 , median : 60 gy ) delivered in daily fractions of 2 gy , 5 days a week . 
 key words : gemistocytic astrocytoma low - grade astrocytoma radiotherapy strahlenther onkol 2005 ; 181 : 24650 doi 10.1007 / s00066 - 005 - 1305 - y adjuvante bestrahlung gemistozytischer astrozytome nach nicht radikaler tumorexzision . 
klinischer verlauf und prognostische faktoren hintergrund und ziel : gemistozytische astrozytome gehren zur gruppe der langsam wachsenden tumoren , sind jedoch sehr aggressiv und besitzen die schlechteste prognose unter den hochdifferenzierten astrozytomen . 
 patienten und methodik : eine gruppe von 48 patienten mit gemistozytischen astrozytomen , die in den jahren 19761998 nach nicht radikaler tumorexzision im onkologiezentrum krakau , polen , adjuvant bestrahlt worden waren , wurde analysiert . 
die gesamtdosis lag zwischen 50 und 60 gy ( mittelwert : 59 , 35 , median : 60 gy ) in tglichen fraktionen von 2 gy an 5 tagen pro woche . 
hohes alter ist der wichtigste ungnstige prognostische faktor bei patienten mit gemistozytischen astrozytomen . schlsselwrter : gemistozytisches astrozytom hochdifferenzierte astrozytome strahlentherapie 1 department of radiation oncology , the maria skodowska - curie memorial cancer center and institute of oncology , cracow , poland . received : march 24 , 2004 ; accepted : december 9 , 2004 strahlenther onkol 2005 no . 
although gemistocytic astrocytomas are considered slow - growing tumors , they often behave aggressively and carry the least favorable prognosis among low - grade astrocytomas ( who grade ii ) [ 18 , 24 , 26 ] the majority of gemistocytic astrocytomas rapidly progress to anaplastic astrocytoma or glioblastoma [ 16 , 32 ]  . 
 patients and methods the records of 48 patients with incompletely excised gemistocytic astrocytoma , irradiated between 1976 and 1998 at the department of radiation oncology , maria skodowska - curie memorial cancer center , cracow , poland , were retrospectively reviewed . 
the parameters monitored to determine clinical response to therapy included neurologic function and performance status ( according to eortc / mrc scale and karnofsky scale ) [ 13 , 15 ]  . patient characteristics are shown in table 1 . 
in 14 patients ( 29% ) angiography , in 32 ( 67% ) computed tomography ( ct ) , and in one ( 2% ) magnetic resonance imaging ( mri ) were performed . 
the total dose ranged from 50 to 60 gy ( mean : 59.35 , median : 60 gy ) delivered in daily fractions of 2 gy , 5 days a week . 
the treatment volume covered the residual tumor with a margin of 12 c after radiotherapy , ten patients ( 20% ) showed an improvement in neurologic function , in 38 ( 80% ) neurologic function was assessed as being stable . 
the kaplan - meier method and log - rank test were used for univariate analysis , and the cox regression model for multivariate analysis [ 4 , 27 ]  . 
 results acute toxicity of treatment the tolerance to treatment was assessed as being very good ( treatment without complications ) in 40 patients ( 83% ) , and good ( periodic symptoms of increased intracranial pressure controlled pharmacologically with no breaks in irradiation ) in eight ( 17% )  . 
 characteristics number of patients ( % ) 36 ( range 1760 ) median age ( years ) gender female male symptoms seizures others localization occipital frontal temporal stage one lobe more than one lobe surgery subtotal resection partial resection biopsy neurologic function very good good moderate poor karnofsky status 80% 7060% < 60% 22 ( 46 ) 26 ( 54 ) 30 ( 63 ) 18 ( 37 ) 9 ( 19 ) 26 ( 54 ) 13 ( 27 ) 29 ( 60 ) 19 ( 40 ) 35 ( 73 ) 12 ( 25 ) 1 ( 2 ) 10 ( 21 ) 25 ( 52 ) 11 ( 23 ) 2 ( 4 ) 11 ( 23 ) 35 ( 73 ) 2 ( 4 ) strahlenther onkol 2005 no . 
postoperative radiotherapy in gemistocytic astrocytomas the presence of gemistocytes in low - grade astrocytomas is regarded as a sign of poor prognosis because of the high incidence of dedifferentiation and malignant transformation [ 16 , 26 , 32 ]  . 
showed that malignant progression took significantly less time in patients with tumors containing > 5% gemistocytes ( 35 months ) than in those with lesions containing < 5% gemistocytes ( 64 months ; p = 0.038 ) [ 32 ]  . 
 numerous prognostic factors have been reported for gemistocytic astrocytoma , such as age , performance status , neurologic function , length and nature of symptoms , localization , stage , percent of gemistocytes among others tumor cells , p53 mutation , proliferative potential of tumor , extent of surgery , and postoperative radiotherapy , but no consensus has been obtained [ 16 , 17 , 22 , 25 , 26 , 28 , 30 , 32 ]  . our results indicate that age is the principal variable determining the survival times of patients with gemistocytic astrocytoma . 
this is also consistent with many others reports , which showed that gemistocytic astrocytoma has been associated with poorer prognosis among low - grade astrocytomas ( who grade ii ) [ 18 , 24 , 26 , 28 ]  . 
observed , in multivariate analysis , that patients with gemistocytic astrocytoma fared significantly worse than others ( p = 0.015 ) [ 29 ]  . age > 35 age 35 male female months months figure 2 . 
a review of the literature has provided no information about gender influence on the prognosis of patients with gemistocytic astrocytoma , but there are some works assessing the impact of sex in patients with low - grade astrocytoma ( who grade ii )  . 
the results of these studies are inconsistent ; some authors observed improved survival times in females , some in males , while others have failed to find any significant influence [ 2 , 19 , 23 , 24 , 28 ]  . the karnofsky performance status and parameters of neurologic function did not significantly affect survival in the present material . 
 besides , a comparison of own results with others is difficult due to differences in the criteria used for assessment of neurologic status ; the same problem applies to performance status . 
in many series , neurologic functional grade and / or karnofsky score were important variables which have an impact on the survival time of patients [ 14 , 19 , 23 , 24 , 31 ]  . 
 the neurologic status appears to be more precise than the performance status , which is assessed second to neurologic function . in the present series , seizures had no influence on prognosis . 
 small tumors may cause epilepsy years before any other symptoms , and patients diagnosed with smaller tumors may be expected to live longer . there were no differences between survival times in patients with tumors limited to one lobe and patients with tumors extending beyond one lobe . 
showed that patients with involvement of two or more lobes fared significantly worse than patients with involvement of only one lobe ( p = 0.016 ) [ 23 ]  . 
in a randomized trial on dose response in radiation therapy of low - grade cerebral glioma , it was found that the t of the tnm classification appears to be one of the most important prognostic factors ( p < 0.00001 ) on multivariate analysis [ 14 ]  . 
some authors do not find advantages in removing them , whereas others do , and emphasize a relationship between the survival time and the extent of resection [ 3 , 19 , 23 , 24 , 26 , 28 , 29 , 31 ]  . 
showed that recurrences after gross total resection or progression after subtotal resection , occurred more often in gemistocytic astrocytomas ( 40% and 100% , respectively ) than in other subtypes [ 26 ]  . 
the 5and 10 - year overall survivals of our group of 48 patients with gemistocytic astrocytomas are worse , compared to survival in other subtypes of low - grade astrocytomas [ 5 , 17 , 18 , 24 , 29 ]  . 
a low 5and 10 - year probability of survival ( 30% and 17% , respectively ) , short time to recurrence , and progression to high - grade astrocytoma in all reoperated tumors indicate a very aggressive behavior of gemistocytic astrocytomas and the need for more effective therapy . 
although gemistocytic astrocytoma is included in low - grade astrocytomas who grade ii , we might consider whether it should be classified , from the clinical point of view , as anaplastic astrocytoma , and treated accordingly [ 6 , 7 , 17 ]  . 
 strahlentherapie und onkologie original article different saliva substitutes for treatment of xerostomia following radiotherapy a prospective crossover study felix momm1 , natalja jurievna volegova - neher1 , jrgen schulte - mnting2 , roland guttenberger1 background and purpose : xerostomia is an important chronic side effect of radiotherapy in the head and neck area . 
the authors investigated the efficacy of different artificial saliva compounds in patients with postirradiation xerostomia . patients and methods : in 120 patients with xerostomia after radiotherapy for head and neck cancer , four different saliva substitute compounds ( gel , carmellose spray , oil , mucin spray ) were tested in a prospective crossover design . 
this will help to find the individually best way to cope with the dry mouth . key words : xerostomia saliva substitutes radiotherapy supportive care head and neck cancer strahlenther onkol 2005 ; 181 : 2316 doi 10.1007 / s00066 - 005 - 1333 - 7 unterschiedliche speichelersatzprparate zur behandlung der xerostomie nach strahlentherapie im kopf - hals - bereich . 
die vorliegende studie untersucht unterschiedliche speichelersatzprodukte bezglich ihrer effektivitt auf diese mundtrockenheit . patienten und methodik : an 120 patienten mit einer xerostomie nach bestrahlung im kopf - hals - bereich wurden vier unterschiedliche speichelersatzprodukte ( gel , carmellose - spray , l , mucin - spray ) in einem prospektiven cross - over - design getestet . 
 die xerostomie vor beginn der studie und whrend der behandlung mit den einzelnen prparaten wurde mit einem fragebogen ermittelt , der in einer pilotstudie entwickelt worden war . ergebnisse : alle prparate verbesserten im vergleich mit der situation vor der studie die xerostomie signifikant ( p < 0 , 0001 )  . 
dies trgt dazu bei , die individuell beste mglichkeit der xerostomiebehandlung herauszufinden . schlsselwrter : xerostomie speichelersatzprparate strahlentherapie supportive therapie kopf - hals - tumoren 1 department of radiotherapy , university clinic freiburg , freiburg , germany , 2 department of medical biometry and statistics , university of freiburg , freiburg , germany . received : june 16 , 2004 ; accepted : september 30 , 2004 strahlenther onkol 2005 no . 
water - binding molecules such as sodium carboxymethylcellulose or mucin [ 1 , 18 , 20 ] are approved as well as oily liquids or gels [ 7 , 30 , 34 , 35 ]  . 
inclusion criteria were time after radiotherapy > 4 weeks , karnofsky index > 70 , tumor in complete remission , age > 18 years , written informed consent , and subjective xerostomia after radiotherapy in the head and neck region ( question have you got problems with a dryness in your mouth ? answered with yes ; all patients in our follow - up outpatient department were asked )  . 
 tested compounds four different compounds were tested as saliva substitutes : ( 1 ) aldiamed gel ( biomedica , rodgau , germany ) , containing aloe vera ( gel ) ; ( 2 ) glandosane spray ( cell pharm , hannover , germany ) , containing sodium carboxymethylcellulose ( carmellose ) ; ( 3 ) rape oil ( oil pressed by brndle , germany , and filled in pump spray bottles at freiburg university clinic , germany ; oil ) ; ( 4 ) saliva medac spray ( medac , wedel , germany ) , containing mucin extracted from pig stomach ( mucin )  . 
 total number of patients ( evaluable ) age ( range ) gender male : female mean radiation total dose ( range ) mean time from radiotherapy ( range ) patients with additional chemotherapy treatment of xerostomia before study drinking much water / tea chewing gum mouth washes candies oil / fat saliva substitute ( spray ) tumor site oropharynx hypopharynx oral cavity / tongue larynx nose salivary glands thyroidea cervical lymphatic nodes unknown primary histology squamous cell carcinoma adenocarcinoma lymphoma other staging staging lymphoma ( ann arbor ) iii 114 12 13 18 6 13 37 14 25 16 3 2 4 13 6 100 5 14 1 2 5 17 37 24 21 19 24 55 5 3 104 2 5 7 0 2 study process the patients were numbered in order of inclusion in the study . 
all questions about xerostomia had to be answered using the german school mark scale ( 16 , 1 = very good ; 6 = poor ) well known to our patients . 
 ethics the trial was approved by the ethics committee of the university of freiburg , germany , and informed consent was obtained for each patient following the current revision of the helsinki declaration . 
fragebogen. questions 18 : baseline and after each week please estimate your xerostomia in resting state ( without eating , 1 = not dry 6 = very dry chewing , any saliva substitute ) 1 = no difficulties please estimate your difficulties with speaking 6 = big difficulties 1 = no difficulties please estimate your difficulties with eating , swallowing and 6 = big difficulties chewing 1 = no liquid needed please estimate how often you need liquid to facilitate eating 6 = liquid for every bite 1 = never or 1 / day please estimate how often you need a product against dryness 2 = 5 / day or less of the mouth ( saliva substitute , water , chewing gum , etc . ) 3 = 10 / day or less when not eating 4 = 15 / day or less 5 = 20 / day or less 6 = more than 20 / day 1 = no difficulties please estimate your difficulties with sleeping caused by 6 = big difficulties dryness of the mouth 1 = no difficulties please estimate your difficulties with taste 6 = big difficulties 1 = liquid how viscous is your saliva ? 6 = highly viscous additional questions after each test week how do you mark the tested compound as saliva substitute ? a : in general , b : in taste would you like to go on using the tested compound ? 1 = very good 6 = poor yes / no additional question after all 4 test weeks after testing all four compounds : which compound would you prefer for further use ? statistics the main tool for comparing the four ( compounds ) and five ( including baseline ) paired measurements , respectively , was the friedman test , followed by pairwise wilcoxon tests . 
no - adjustment was applied , since the significance level of all differences to baseline would not be affected , and for the no difference statements between the compounds such a correction would not be appropriate . however , for a more detailed look on possible predictive factors , use of repeated measures anova was necessary . 
 for this purpose , data were transformed by the function log10 ( 64 ) log10 ( 64x ) for the summary score and log10 ( 8 ) log10 ( 8x ) for single items , thus achieving a better fit to the requirements of the linear model . 
 when asked about the general effect of each compound , the patients marked the gel best with 3.5 and the oil worst with 4.0 on average ( table 4 )  . 
 by cell death and fibrotic conversion of the tissue , function is affected irreversibly in the sense of a consequential late effect : saliva can be produced only in a small quantity [ 5 ]  . 
 thus , many patients complain about severe xerostomia after radiation therapy : salivary gland tissue has a tolerated dose td 100 / 5 of 50 gy when the whole organ is irradiated . 
 the td 100 / 5 is the smallest radiation dose which will cause a clinically relevant and well - defined consequence of radiation with a probability of 100% in 5 years [ 5 , 11 ]  . 
other patients prefer compounds with an effect lasting overnight and resulting in better sleep . in the main questionnaire ( questions 18 ) , the carmellose spray received the worst marks , whereas most patients wanted to go on using it when asked after the test week . 
as we were told in additional free text parts of the questionnaire ( data not shown ) , many patients had considerable problems with the application of the compounds and especially with handling the gel . 
as depicted in figure 1 , the oil was as good as the other compounds in the main questionnaire , and by one patient it was even marked with the best result of all questionnaires . 
 high standard deviations in marks given for the oil ( table 4 ) also show , that patients had very different opinions about its effect and taste : best treatment of xerostomia seems to be very individual . considering sex , age [ 19 ] and radiation dose , it was not possible to identify groups of patients preferring one single product . 
thus , the easiest way to improve xerostomia treatment seems to offer several compounds to test and to choose frothis way , patients can find their favorites and can even choose combinations , for example a spray at work and a gel at night . 
improved xerostomia treatment will positively influence quality of life and may also promote dental health and prevent infections in the head and neck region . recently , great efforts were made to develop radioprotective medications to decrease side effects of radiotherapy . 
the application of pilocarpine / carbacholine [ 4 , 16 , 17 , 26 ] , coumarin / troxerutine [ 10 ] and adrenergic substances [ 22 ] had some success as well . further , first studies exist about possibilities to relocate the salivary glands out of the radiation field by operation [ 8 ]  . 
 dose reduction at the glands by modern treatment techniques such as three - dimensional treatment planning or intensitymodulated radiotherapy has a protective effect as well [ 6 , 12 , 21 , 37 ]  . 
 in spite of great efforts in the field of radioprotection of salivary glands , chronic xerostomia is still a considerable problem for quality of life and oral health in patients after radiotherapy for head and neck cancer [ 1 , 13 , 15 , 2325 ]  . 
on the basis of the present study we suggest that every patient should be encouraged to test different artificial saliva compounds to find the individually best way to cope with xerostomia . acknowledgments we thank the firms biomedica ( rodgau , germany ) , gaba ( muenchenstein , switzerland ) and medac ( wedel , germany ) for sponsoring the study in equal shares . 
 key words : brain tumor sellar tumor radiotherapy chemotherapy myoepithelioma strahlenther onkol 2005 ; 181 : 2603 doi 10.1007 / s00066 - 005 - 1356 - 0 strahlentherapie und chemotherapie eines myoepithelioms der sellaregion hintergrund : myoepitheliome knnen in der kopf - hals - region entstehen , insbesondere in den speicheldrsen . 
 fallbericht : beschrieben wird eine 34 - jhrige afrikanische patientin mit proliferierendem myoepitheliom in der sellaregion , das trotz teilresektion und postoperativer strahlentherapie mit einer gesamtdosis von 54 gy ein aggressives lokales wachstum zeigte ( abbildungen 1 und 2 )  . 
 schlsselwrter : hirntumoren sellatumoren strahlentherapie chemotherapie myoepitheliom introduction introduction myoepithelioma is a rare disease which might occur in the myoepithelioma is a rare disease which might occur in the extremities , the head and neck region , particularly within the extremities , the head and neck region , particularly within the salivary glands , the breast , and the lung [ 1 , 5 , 12 , 13 ]  . 
however , primary intracranial myoepithelioma is very rare and , according to our literature search , epithelioma is very rare and , according to our literature search , might not have been reported at all so far . 
interestingly , salivary gland rests occur in the posterior lobe of the pituitary vary gland rests occur in the posterior lobe of the pituitary gland near rathkes cleft [ 2 ]  . 
the most common types of intracranial tumors are glioma , meningioma , and brain metastatracranial tumors are glioma , meningioma , and brain metastases [ 4 , 8 , 10 , 14 ]  . 
 case report case report in june 2002 , a 34 - year - old female african patient presented in june 2002 , a 34 - year - old female african patient presented with bitemporal hemianopsia and visual impairment . 
computed tomography ( ct ) and magnetic resonance imaging ( mri ) ed tomography ( ct ) and magnetic resonance imaging ( mri ) demonstrated an intracranial mass in the sellar region , most demonstrated an intracranial mass in the sellar region , most likely craniopharyngioma . 
diagnostic work - up also showed 1 department of radiation oncology , klinikum rechts der isar , technical university of munich , germany , 2 department of hematology and oncology , klinikum rechts der isar , technical university of munich , germany . received : august 16 , 2004 ; accepted : january 14 , 2005 strahlenther onkol 2005 no . 
 complete insufficiency of the anterior lobe of the pituitary complete insufficiency of the anterior lobe of the pituitary gland and partial insufficiency of the posterior lobe , resulting gland and partial insufficiency of the posterior lobe , resulting for example in diabetes insipidus , amenorrhea and hypothyfor example in diabetes insipidus , amenorrhea and hypothyroidis only incomplete surgical resection was performed roidis only incomplete surgical resection was performed because the tumor extended to the hypothalamus and adhered because the tumor extended to the hypothalamus and adhered to the optic chiasm and right optic nerve . 
instead , a malignant tumor of mesenchymal origin with ki - 67 staining in 3040% of the tumor cells mal origin with ki - 67 staining in 3040% of the tumor cells was found . 
 between august and october 2002 , three - dimensional conbetween august and october 2002 , three - dimensional conformal radiotherapy was performed with single daily fractions formal radiotherapy was performed with single daily fractions of 1.8 gy to a total dose of 54 gy ( figure 1 )  . 
in june 2003 , cranial imaging showed local tumor progression with comcranial imaging showed local tumor progression with compression of the optic chiasm and a metastasis in the right paripression of the optic chiasm and a metastasis in the right parietal lobe ( figure 2 )  . 
histology of both specimens was very similar to the original tumor , except for a biphasic structure which lar to the original tumor , except for a biphasic structure which appeared typical of synovial sarcoma . 
however , molecular pathology at the reference center did not show the typical x ; 18 thology at the reference center did not show the typical x ; 18 translocation . 
staging including ct of the chest and abdomen did not show further metastases nor was chest and abdomen did not show further metastases nor was there any indication for a primary sarcoma elsewhere in the there any indication for a primary sarcoma elsewhere in the body . 
the latter was initiated in october 2003 , when mri demonstrated latter was initiated in october 2003 , when mri demonstrated enlargement of the residual sellar tumor with visual impairenlargement of the residual sellar tumor with visual impairment as well as distant progression in the mesencephalon close ment as well as distant progression in the mesencephalon close to the pons . 
 due to the development of complete blindness and the lack of due to the development of complete blindness and the lack of other therapeutic options , a different chemotherapy schedule other therapeutic options , a different chemotherapy schedule was started in december ( bcnu 200 mg / m22 )  . 
therefore , the patient and her husband decided to discontinue further treatment and to prohusband decided to discontinue further treatment and to proceed with best supportive care in a dedicated palliative mediceed with best supportive care in a dedicated palliative medicine department . 
 discussion discussion recent review articles summarized the current knowledge recent review articles summarized the current knowledge about myoepithelioma , a rare disease which is diagnosed about myoepithelioma , a rare disease which is diagnosed mainly in younger patients ( mean age 38 years [ 5 ] )  . 
magnetic resonance imaging ( contrast - enhanced t1 - weighted ) 3 months after incomplete resection and radiotherapy ( a ) and at diagnosis of local progression ( c , d ) and metastasis ( b )  . 
 magnetresonanztomographie ( kontrastverstrkte t1 - gewichtung ) 3 monate nach subtotaler resektion und strahlentherapie ( a ) sowie bei diagnose der lokalen progression ( c , d ) und der metastase ( b )  . 
 figure 2c abbildung 2c figure 2d abbildung 2d logically malignant forms , risk of local recurrence and metaslogically malignant forms , risk of local recurrence and metastases is > 30% each [ 5 ]  . 
the patient described here had typical clinical symptoms of sellar and suprasellar tumors , such as craclinical symptoms of sellar and suprasellar tumors , such as craniopharyngioma , which was the most likely initial diagnosis niopharyngioma , which was the most likely initial diagnosis [ 15 ]  . 
in the present case , repeat specimens were available and sent to the naent case , repeat specimens were available and sent to the national reference center for soft - tissue tumors in jena , gertional reference center for soft - tissue tumors in jena , germany . 
regardless of the histological subtype of the tumor , it appears likely that the sellar lesion was the true primary rather pears likely that the sellar lesion was the true primary rather than a metastasis because during follow - up , no putative other than a metastasis because during follow - up , no putative other primary tumor or extracranial metastases were detected . 
 manifestation of lesions outside the brain would have been manifestation of lesions outside the brain would have been expected in case of a typical sarcoma eventually spreading to expected in case of a typical sarcoma eventually spreading to the brain during the course of the disease . 
 the course of the disease was very unfavorable , because comthe course of the disease was very unfavorable , because complete resection could not be achieved and the dose to this plete resection could not be achieved and the dose to this critical region of the brain was limited to 54 gy . 
with stereotactic radiotherapy , such doses can be administered if there is at least a small marsuch doses can be administered if there is at least a small margin between the tumor and the organs at risk . 
 after < 1 year , local progression of the residual tumor was after < 1 year , local progression of the residual tumor was diagnosed , with simultaneous metastasis in the parietal lobe . 
it should be noted that established chemotherapy regimens for this disease do not exist , lished chemotherapy regimens for this disease do not exist , but occasional shrinkage of such tumors has been observed but occasional shrinkage of such tumors has been observed [ 7 ]  . 
nevertheless , a certain percentage of patients will fail , because the risk of micrometastatic spread is high and unfail , because the risk of micrometastatic spread is high and undetectable distant disease might already be present at primary detectable distant disease might already be present at primary diagnosis . 
59.000 patienten , die ihre diagnose im zeitraum 1998 bis 2012 erhalten hatten und mit einer kombinationschemotherapie behandelt wurden . mediastinale grozellige b - zell - lymphome ( lbcl ) wurden nicht eingeschlossen . 
der verzicht auf eine konsolidierende rt hat negative konsequenzen fr die berlebenswahrscheinlichkeit . originalpublikation vargo ja , gill bs , balasubramani gk , baeilrw s ( 2015 ) treatment selection and survival outcomes in early - stage diffuse large b - cell lymphoma : do we still need consolidative radiotherapy ? j clin oncol 33 : 37103717 med . 
of oncology and palliative medicine , nordland hospitaltrust 8092 bod , norwegen e - mail : cnied@hotmail.com kommentar die autoren bemhten sich , die typischen fallgruben einer retrospektiven analyse zu umschiffen und unausgewogenheiten wie selection bias und immortal time bias durch statistische methoden abzuschwchen . 
zum beispiel wurden patienten , die in den ersten monaten nach der diagnose verstarben , nicht inkludiert ( immortal time bias : eine strahlenther onkol ( 2016 ) 192 : 354355 weitere therapielinie kann nur gegeben werden , wenn die patienten die frhphase berleben )  . 
allerdings ist nicht bekannt , warum berhaupt diese frhen todesflle auftraten ( refraktre erkrankung , therapieassoziiert , komorbiditt ? )  . auch wenn die groe zahl an patienten grundstzlich von vorteil ist , lsst sich eine prospektiv randomisierte studie nach dem intention - to - treat - prinzip und die stratizierung fr bestimmte prognosefaktoren wie alter oder stadium dennoch nicht perfekt simulieren . 
diese soziokonomischen einussfaktoren sind im us - amerikanischen gesundheitswesen nach wie vor bedeutsam . es ist auch typisch fr die analyse derartiger datenbanken , dass im dunkeln bleibt , wie viele patienten nun r - chop 21 erhalten haben , welche anderen regime zum einsatz kamen , ob die geplante dosisintensitt erreicht wurde , wie die zielvolumina deniert wurden , ob und wann eine pet - ct erfolgte , ob in abhngigkeit von der baseline - ausbreitung oder einer response bestrahlt wurde , wie mit extranodalen lokalisationen verfahren wurde usw . 
wie knnen wir patienten , die nach chemotherapie bereits geheilt sind , identizieren und wann ist eine deintensivierung mglich ? seine diskussion der literatur kommt zu der schlussfolgerung , dass nicht alle patienten konsolidierend bestrahlt werden sollten . 
liegt dagegen eine partielle remission nach systemischer behandlung vor oder eine ausgedehnte initiale manifestation ( bulky disease , wofr jedoch unterschiedliche denitionen in den bisherigen studien galten ) , knnte ein gewinn zu erzielen seer fordert uns auf , prospektiv - randomisierte studien zu starten , die ausschlielich auf subgruppen fokussieren , bei denen mglicherweise die strahlentherapie das berleben verbessern kann . 
vielleicht wre es auch interessant , patienten zu inkludieren , deren ereignisfreies berleben mit systemischer behandlung nicht zufriedenstellend ist und die insbesondere an ursprnglich bereits befallenen lokalisationen rezidivieren [ 3 , 4 ]  . voraussetzung dafr ist ein partnerschaftlicher dialog , da von hmatoonkologischer seite vermehrt das verstndliche interesse an fragestellungen wie der verbesserten klassikation und einer zielgerichteten oder immunmodulierenden behandlung besteht ( germinal center b - cell like dlbcl , activated b - cell like dlbcl ; [ 57 ] )  . 
beispielsweise sollen bei lteren patienten ( 6180 jahre ) mit ungnstiger prognose in der aktuellen optimal - studie der deutschen studiengruppe fr hochmaligne non - hodgkinlymphome ( dshnhl ) mehrere fragestellungen beantwortet werden . 
vargo ja , gill bs , balasubramani gk , beriwal s ( 2015 ) treatment selection and survival outcomes in early - stage diffuse large b - cell lymphoma : do we still need consolidative radiotherapy ? j clin oncol 33 : 37103717 2 . 
maurer mj , jais jp , ghesquires h et al ( 2015 ) personalized risk prediction for event - free survival at 24 months in patients with diffuse large b - cell lymphoma . 
ghesquieres h , slager sl , jardin f et al ( 2015 ) genome - wide association study of event - free survival in diffuse large b - cell lymphoma treated with immunochemotherapy . 
semin hematol 52 : 107118 strahlenther onkol ( 2016 ) 192 : 305311 doi 10.1007 / s00066 - 016 - 0961 - 4 seed loss in prostate brachytherapy operator dependency and impact on dosimetry nancy el - bared1 natanel sebbag1 dominic bliveau - nadeau1 yannick hervieux1 rene larouche1 daniel taussky1 guila delouya1 received : 17 october 2015 / accepted : 10 february 2016 / published online : 29 february 2016 springer - verlag berlin heidelberg 2016 abstract introduction the aim of our study was to review seed loss and its impact on dosimetry as well as the influence of the treating physician on seed loss and dosimetry in patients treated with prostate brachytherapy using permanent loose 125i implant . patients and methods we analyzed 1087 consecutive patients treated by two physicians between july 2005 and april 2015 at a single institution . 
when at least one seed was lost , a decrease of 4.2 gy ( p < 0.001 ) in the d90 and a decrease of 3.5 % ( p = 0.002 ) in the v150 was observed . conclusion we found a significant decrease in v150 and d90 with the occurrence of seed loss . 
e. , h2l 4m1 montreal , qc , canada found a difference in seed migration among the physicians demonstrating that seed loss is operator dependant . keywords radiation dose implant radiotherapy seed migration to thorax learning curve complications seed - verlust nach prostata - brachytherapy einfluss von operateur und dosimetrie zusammenfassung zielsetzung wir analysierten den prozentsatz des seedverlusts sowie den einfluss von arzterfahrung und seedabgang auf die dosimetrie bei patienten , die mit einer prostata - brachytherapie mit permanent beweglichen 125iimplantaten behandelt wurden . patienten und methode eingeschlossen in diese studie wurden alle zwischen juli 2005 und april 2015 an unserem krankenhaus von zwei rzten konsekutiv behandelten 1087 patienten . 
 bei unvollstndiger seed - anzahl wurde ein thorax - rntgenbild angefertigt . ergebnisse in 19% der patienten ging mindestens ein seed verloren : 20% der implantate beim erfahrenen arzt und 17 , 2 % beim weniger erfahrenen arzt ( p = 0 , 4 )  . 
die durchschnittliche seed - verlustrate war 0 , 57% [ standardabweichung ( sd ) 1 , 39 ] und der prozentsatz an abgegangenen seeds pro implantierten seeds 0 , 14% ( sd 0 , 65 )  . 
beim verlust von mindestens einem seed wurde eine reduktion der d90 um 4 , 2 gy ( p < 0 , 001 ) und der v150 um 3 , 5% ( p = 0 , 002 ) festgestellt . schlussfolgerung ein seed - abgang senkt v150 und d90 signifikant . 
ob ein seed - abgang nachgewiesen werden kann , hngt vom behandelnden arzt ab . schlsselwrter strahlendosis implant - radiotherapie seed - migration zum thorax lernkurve komplikationen therapy at our institution . 
low - dose rate ( ldr ) brachytherapy was used as monotherapy in 1026 patients and used as a boost in combination with external beam radiation therapy ( ebrt ) in 73 patients . the prescribed dose was 144 gy as monotherapy and 110 gy as a boost . 
seeds seen in the pelvis but outside of the introduction seed loss is a known complication of transperineal permanent seed prostate brachytherapy ( pb ) used in prostate cancer treatment , with the primary site of migration being the lungs [ 1 ]  . 
seeds may be lost through the urinary tract , possibly due to urethral mucosal puncture or migrate to remote organs after having gained access to the peripheral venous system through periprostatic veins [ 2 ]  . 
however , serious adverse effects such as acute myocardial infarction [ 3 ] or small cell lung cancer [ 4 ] have been reported to occur at the site of migration . one can speculate that dosimetry would be influenced by seed loss . 
in our previous publications [ 11 , 12 ] , the impact of seed loss on dosimetry was not significant . we have previously reported the existence of a learning curve and , that with gained experience , the number of seed migration decreases [ 12 ]  . 
with the arrival of a second physician performing pb in our center , we examined whether seed migration could also be physician dependent . the aim of our study was to update the results of the largest reported cohort on seed loss and migration rates in patients treated with an automated delivery system of loose seeds for prostate cancer . 
1 posterioranterior and lateral lung x - rays in patient with four seeds in thorax strahlenther onkol ( 2016 ) 192 : 3053111 3 307 prostate were not classified as lost seeds . 
such seeds in the pelvis were a very rare occurrence and not recorded separately . for the purpose of this retrospective study , radiologists reports of the chest x - rays were used . 
seeds not found on chest x - ray were assumed to have been lost in the urine . the patients also underwent a pelvic computed tomography and , since january 2014 , an additional mri for dosimetric assessment . 
dosimetry was evaluated for the v100 , v150 ( percent of prostate receiving 100 and 150 % respectively of the prescribed dose ) , and d90 ( minimum dose covering 90 % ) of the prostate volume . 1087 patients for statistical analysis . 
patient characteristics are detailed in table 1 and treatment characteristics in table 2 . of the 1087 patients analysed , 19 % had lost at least one seed and only 6 % had at least one seed in the thorax . 
in the 20 patients with at least 4 seeds lost , only one patient had a previous transurethral resection of the prostate ( turp ) and none of the patients that had lost 5 seeds had previous brachytherapy technique prostate brachytherapy ( pb ) is performed at our center by either one of two physicians . 
this system does not allow for stranded seed implants . for all patients , loose 125i seeds with a median activity of 0.44 mci ( range 0.310.68 mci ) were used . 
and if seeds were placed outside the prostate , this was done at the apex and usually close to the prostate capsule . statistical analysis the seed loss rate was calculated as the mean total seed loss rate ( number of seeds lost / number seeds implanted ) as a percentage . 
six of the 20 patients having lost 4 seeds were amongst the first 100 patients treated at our center . two of the 11 patients who had a previous turp lost seeds : one patient three , the other four seeds . 
the most experienced physician has proceeded to 862 implants while the less experienced physician , 236 . at least one seed was lost in 20.0 % of implants done by the most experienced physician and in 17.2 % of the implants of the less experienced physician ( p = 0.4 , c2 test )  . 
 the difference in seed loss rate was borderline significant between both physicians ( p = 0.056 ) with a mean seed loss rate of 0.61 % ( sd 1.44 ) for the most experienced physician and mean 0.43 % ( sd 1.16 ) for physician 2 . 
the rate of seeds in the thorax was significantly different between both physicians ( p < 0.001 ) with a mean of 0.17 % ( sd 0.72 ) for the most experienced physician and a mean of 0.04 % ( sd 0.26 ) for physician 2 . figure 2 illustrates the learning curve of the entire team and each individual physician : it is possible that some of the differences between both physicians are statistical artefacts due to the relatively small number of patients with seed loss per physician . 
when compared with absence of seed loss , a difference of 4.2 gy ( p < 0.001 ) was observed in the d90 and of 3.5 % ( p = 0.002 ) in the v150 . 
furthermore , we have reported seed loss in 19 % of our patients ; this represents a number below that reported in the literature as described in a publication by ishiyama et al . 
 [ 14 ] with loose seeds loss occurring in 3076 % of patients . in our previous publication on the first 495 patients treated at our center by the most experienced physician , we have shown the existence of a learning curve for seed loss [ 12 ]  . 
surprisingly , the less experienced physician had a borderline significantly lower ( p = 0.056 ) seed loss rate and a significantly ( p < 0.001 ) lower migration rate to the thorax . 
however , since 2011 , the year when the less experienced physician began practice , there has been no difference between both physicians as to whether at least one seed was lost ( p 0.20 ) or at least one seed had migrated to the thorax ( p 0.24 , detailed data not shown )  . 
we believe that this paper points towards the physician as the main cause of seed loss , but we are unable to pinpoint on how exactly to avoid seed loss . 
the same team of physicists have been rotating for many years in the operating roothey are essential for operative planning and have to approve each needle positioning before the delivery of the seeds . 
thus , the less experienced physician may have benefited from the skills of a more experienced teait has also been hypothesized that the learning curve for less experienced physician was steeper because of intensive training with the most experienced physician . 
on the other hand , the most experienced physician did a fellowship before starting the prograwe did not want to further fragment our analysis with excluding the first cases of each physician to adjust for a possible learning curve . 
thus along with technique , the rigours verifications and quality control developed and perfected over the years by the pb team has further helped the less experienced physician attain very low seed loss rates . 
however , as the rate of patients with 2 seed loss is 8.4 % , we doubt that a randomized study would be able to show an advantage of one technique over the other . we have found that , among the 11 patients who had a previous turp , two experienced seed loss : one patient lost three seeds and the other patient lost four seeds . 
careful preoperative evaluastrahlenther onkol ( 2016 ) 192 : 3053111 3 310 tion is necessary to assess whether a seed implant is feasible in a patient with previous turp to avoid large seed loss . this paper is an update from our previous paper published in 2012 with 592 additional patients . 
 [ 5 ] , they found a reduction of the d90 proportional to the percentage of seed loss , but this did not result in a significant decrease in tumor control probability . 
 [ 17 ] , it was demonstrated that higher d90 were correlated with better biochemical disease - free survival , with doses of 160180 gy or greater offering a better control . 
thus the significant decrease in day 30 mean d90 from 159.8 gy ( no seed loss ) to 159.6 gy ( one seed loss ) to 150 gy ( 2 seed loss ) might affect biochemical - free survival . 
 [ 19 ] , the nuclear regulatory commission defines a medical event ( me ) as the total dose delivered differs from the prescribed dose by 20 percent or more . an astro working group recommended , for permanent prostate brachytherapy , that a me be defined as > 20 % of source strength prescribed in the post - procedure written directive being implanted outside the planning target volume [ 19 ]  . 
therefore not even cases with such a large seed loss of 45 seeds would qualify as a me because this amounts to only 57 % of the total number of seeds outside of the prostate . conclusion we have found that seed loss is operator dependent as well as subject to a learning curve . 
we are unable to give further recommendations on how to reduce seed loss other than paying attention to positioning of the needle tip . acknowledgments we thank david roberge , md for his helpful suggestions in preparing this article . compliance with ethical standards conflicts of interest n . 
we did not receive any direct financial support to conduct this research . this study was approved by the institutional ethics committee , therefore the study has been performed in accordance with the ethical standards laid down in the 1964 . strahlenther onkol ( 2016 ) 192 : 288296 doi 10.1007 / s00066 - 016 - 0957 - 0 radioablation of liver malignancies with interstitial high - dose - rate brachytherapy complications and risk factors konrad mohnike1steffenwolf1 robert damm1 max seidensticker1 ricarda seidensticker1 frank fischbach1 nils peters2 peter hass2 gnther gademann2 maciej pech1 jens ricke1 received : 5 october 2015 / accepted : 3 february 2016 / published online : 29 february 2016 springer - verlag berlin heidelberg 2016 abstract background to evaluate complications and identify risk factors for adverse events in patients undergoing high - doserate interstitial brachytherapy ( ibt )  . material and methods data from 192 patients treated in 343 ctor mri - guided interventions from 20062009 at our institution were analyzed . 
in 41 % , the largest tumor treated was 5 cm , 6 % of the patients had tumors 10 c prior to ibt , 60 % of the patients had chemotherapy , 22 % liver resection , 19 % thermoablation or transarterial chemoembolization ( tace )  . 
median overall survival after the first liver treatment was 20.1 months for all patients and the local recurrence - free surviving proportion was 89 % after 12 months . conclusions image - guided ibt yields a low rate of major complications and is effective . keywords liver neoplasms treatment efficacy local ablation hepatocellular carcinoma adverse events radioablation von lebermalignomen mit interstitieller high - dose - rate - brachytherapie komplikationen und risikofaktoren zusammenfassung hintergrund evaluierung der komplikationsrate und identifizierung von risikofaktoren fr komplikationen und nebenwirkungen bei patienten mit lebermalignomen , die mit der hochdosierten interstitiellen brachytherapie ( ibt ) behandelt wurden . material und methoden von 2006 bis 2009 wurden 192 patienten in 343 ctoder mrt - gefhrten interventionen behandelt und deren daten ausgewertet . 
der grte behandelte tumor war in 41% der flle 5 cm , 6% der patienten hatten tumoren 10 c vor behandlungsbeginn hatten 60% der patienten eine chemotherapie , 22% eine leberesektion und 19% eine thermoablation oder transarterielle chemoembolisation ( tace )  . 
das mediane gesamtberleben nach der ersten leberbehandlung betrug 20 , 1 monate , die lokalrezidivfreiheit nach 12 monaten lag bei 89% . schlussfolgerung die bildgefhrte ibt hat eine niedrige komplikationsrate und ist effektiv . significantly [ 16 , 17 ]  . 
to our knowledge , this is the largest study which thoroughly evaluates complications and risk factors for adverse events in patients with liver neoplasms treated with ibt . schlsselwrter leberneoplasien behandlungswirksamkeit lokale ablation hepatozellulres karzinom nebenwirkungen materials and methods study design introduction the diagnosis and treatment of primary and secondary liver malignancies have recently improved [ 1 , 2 ]  . 
liver transplantation and surgical resection in patients with hepatocellular carcinoma ( hcc ) can potentially lead to cure in the minority of patients for whom these options are feasible [ 3 ]  . 
however , fewer than 25 % of patients with crlm are candidates for a potential curative treatment [ 6 ]  . thermoablative techniques have evolved for more than a decade ; particularly , radiofrequency ablation ( rfa ) yields promising rates of tumor control and survival in small tumors [ 79 ]  . 
however , rfa is of limited value in tumor lesions exceeding 3 cm in diameter , located close to the hepatic hilum or close to large vessels [ 10 ]  . precise radiotherapeutic techniques like stereotactic body radiotherapy ( sbrt ) has proven excellent local control , also after single - dose irradiation of liver tumors [ 11 ]  . there is also experience with proton beam therapy , especially from japan [ 12 , 13 ]  . 
nonetheless , sbrt has demonstrated limitations in previous studies , such as a limited number of reasonably treatable metastases or a safe lesion diameter up to 45 cm [ 14 , 15 ]  . 
beyond that size threshold , local tumor control rates after sbrt tend to decrease patients treated at our institution with ibt from march 2006 to december 2007 were included in this study ( group a , n = 144 )  . 
to address somatic discomfort more specifically , a second cohort of patients was recruited from december 2008 to march 2009 ( group b , n = 48 ) based on the same inclusion criteria , more closely monitored especially during the hospital stay with structured interviews to cover minor and more subjective side effects like mild pain and nausea more precisely . prior interventional therapies ( e.g. , rfa ) were to have been completed at least 4 weeks before ibt ; prior ibt had to be completed 3 months and yttrium90 radioembolization 6 months before ibt . 
ascites was not an exclusion criterion if controlled or minimal . in general , we set a limit of liver involvement in a single session of not more than 5 gy in two - thirds of the liver volume . 
 in patient cohort a , this documentation was supplemented by thorough chart reviews , external documents , and telephone interviews ( if events in the follow - up required such ) , whereas patient cohort b was additionally more closely monitored especially during the hospital stay with structured interviews to cover side effects regarding somatic discomfort such as pain and nausea more precisely . intervention and irradiation technique irradiation by the ibt technique , using an afterloading 10ci iridium192 source system ( nucletron , the netherlands ) was performed . 
the prescribed dose at the tumor margin depended on the primary tumor based on findings from previous trials ( e.g. , hepatocellular carcinoma 15 gy , and colorectal carcinoma 20 gy ) [ 20 , 21 ]  . 
2 ibt planning based on interventional contrast - enhanced strahlenther onkol ( 2016 ) 192 : 2882961 3 292 analysis and statistical methods adverse events were graded according to the 3rd version of the national cancer institutes common terminology criteria for adverse events [ 27 ]  . 
time to progression ( ttp ) and overall survival ( os ) were estimated by the kaplanmeier method and compared by employing the log - rank , breslow , and taroneware tests . 
calculations were performed with spss software , version 15 ( spss inc . , chicago , il , usa )  . results patients and procedures a total of 192 patients with primary and secondary malignancies of the liver were treated in 343 interventions , in which 1275 brachytherapy catheters were placed [ patients with colorectal liver metastases ( lm ) , n = 84 ; hepatocellular carcinoma , n = 50 ; cholangiocellular carcinoma , n = 16 ; breast cancer lm , n = 13 ; lung cancer lm , n = 8 ; and 21 patients with lm of other origin ]  . 
of the 192 patients , 111 received more than one ibt . complications overall , the proportion of patients with major complications was below 5 % ( 15 / 343 )  . 
that patient with a relapsed hepatocellular carcinoma 22 months after resection of the left liver lobe and hepatitis c with steatohepatitis and preprocedural preserved liver function ( child a ) developed ascites and an icteric elevation of liver enzymes with a 5fold elevation of bilirubin , a > 5fold elevation of alkaline phosphatase , and a 3fold elevation of transaminases 7 weeks after the last of four brachytherapy sessions . 
 the patient died 27 months after the last brachytherapy . postinterventional infection overall , ten postprocedural infections ( 10 / 343 , 2.92 % ) , including four liver abscesses , were diagnosed . 
serum levels of postinterventional c - reactive protein ( crp ) positively correlated with the clinical target volume ( ctv ; r = 0.473 ; p < 0.001 ; n = 312 / 343 )  . 
median time to progression was 5.5 months , ranging from 11.7 months in patients with hepatocellular carcinoma to 2.2 months in patients with lung cancer . local recurrences ( lr ) were defined as any tumor growth , at any time point after ibt , adjacent to the field of administered radiation . 
forty - four lesions ( 14.9 % ) of 296 treated developed a local recurrence ( lr ) with a 12 - month local control rate ( lcr ) of 89 % for all lesions ( ranging from 97 % in hcc lesions to 84 % in colorectal liver metastases )  . 
 a multivariate cox regression including tumor diameter , strahlenther onkol ( 2016 ) 192 : 2882961 3 clinical target volume ( ctv ) and dose covering 100 % of the ctv ( d100 ) revealed the significant influence of d100 upon lr - free survival only in colorectal liver metastases ( p = 0.03 ) , while this was not the case for lesions of other orig neither tumor diameter nor ctv had a significant effect on lr - free survival . discussion data from this study suggest that the safety of ibt compares to that of other minimally invasive ablation methods such as rfa . 
the interventional major complication rate of 4.1 % in ibt is equivalent to that reported for rfa ( 4.1 % ) and below the surgical complication rate [ 29 , 30 ]  . the greater complication rate in cirrhotic than in noncirrhotic patients was also found in an earlier trial of ibt in hcc [ 19 , 20 ]  . 
 [ 31 ] showed in a small patient group that a dose exposure of the upper gi mucosa of 15.5 gy ( d1cc ) was predictive of gastric ulceration after a single ibt . 
 therefore , we now routinely start patients on ppi , when the dose exceeds 5 gy to the highest exposed mucosal area . the frequency of severe to irreversible liver toxicity is very low irrespective of single doses of up to 25 gy , and of repetitive high - dose radiotherapies , as supported by findings of ruehl et al . 
 [ 34 ] , 11 of 60 patients ( 18 , 3 % ) with hcc treated with pbt developed a radiation - induced liver disease ( rild , or proton - induced hepatic insufficiency , phi ) , of whom 7 patients ( 11 % ) died of phi . 
has proven the effectiveness in ibt [ 39 , 40 ]  . a postinterventional ( 2nd day after ibt ) crp of 165 mg / l and / or leukocyte count 12.7 gpt / l was considered to be a reliable threshold for distinguishing reactive elevations from inflammatory complications . in this trial , 41 % of the lesions treated exceeded 5 cm in diameter but the 12 months local control rate ranged from 97 % in hepatocellular carcinoma to 84 % in colorectal liver metastases despite the fact that patients with limited disease were included , receiving a more or less curative intended high dose as well as patients with an advanced stage of disease with palliative treatment and lower doses . overall , our results indicate that ibt is a safe and effective procedure in heavily pretreated patients . financial support this work was funded exclusively by the university of magdeburg . compliance with ethical standards conflict of interest k . 
ricke state that there are no conflicts of interest . the study was conducted in accordance with the protocol , the ethical principles that have their origin in the declaration of helsinki and ich - gcp . 
bohndorf betreute diese anlage bis zur flucht der familie 1960 . nach einer station in hanau , in der er oberarzt in der diagnostik war , kam er 1961 an die hno - klinik der universitt wrzburg , die von wullstein geleitet wurde . dort unterstanden ihm die bestrahlung an der co - anlage und die diagnostik fr die hautklinik . 
1967 bernahm er die leitung der hartstrahlenabteilung der hno - klinik . diese abteilung zog 1970 in die neue kopfklinik uzu ihr gehrten nun co - anlage , cs - anlage , weichstrahlgert rt50 , simulator - eigenbau und anlagen zur rntgendiagnostik . 
letztere waren bohndorf sehr wichtig , denn er vertrat stets die meinung , jeder strahlentherapeut muss auch in der diagnostik gut ausgebildet se1971 erfolgte die ernennung zum professor.1974 bernahm bohndorf die leitung der nun selbststndigen abteilung fr therapeutische radiologie.1977 erhielt er den ruf auf den neuen lehrstuhl fr strahlentherapie , dem ersten radiologischen lehrstuhl an der universitt wrzburg . 
obwohl die baulichen manahmen noch mehrere jahre zurckgewerner bohndorf werner bohndorf , der frhere lehrstuhlinhaber und direktor der klinik und poliklinik fr strahlentherapie der universitt wrzburg , feierte am 24 . 
dort besuchte er auch das gymnasium , konnte es aber nicht beenden , denn er wurde 1943 mit notabitur zum militr eingezogen , kam zur marine und diente 2 jahre im eismeer zwischen hammerfest und spitzbergen . 
dadurch setzten in verstrktem mae die entwicklung neuer bestrahlungstechniken und die validierung bisher eingesetzter techniken ean der klinik hatte der einsatz der bewegungsbestrahlung eine lange tradition , die sich bei der entwicklung neuer techniken fortsetzte . 
mit der einfhrung der computertomographie konnte der nachteil der halbindividuellen krperquerschnitte beseitigt werden . bohndorf erkannte frhzeitig die groe bedeutung der ct nicht nur fr die tumordiagnostik , sondern auch fr die bestrahlungsplanung . 
als jahre spter an anderer stelle ein symposium stattfand , bei dem die beziehung zwischen ct und simulator untersucht wurde , konnte die wrzburger klinik bereits feststellen , dass die ct auch fr die bestrahlungsplanung unverzichtbar ist . 
dieses beispiel demonstriert eine fr die auendarstellung der klinik nachteilige eigenschaft , ergebnisse und erkenntnisse zurckhaltend oder gar nicht zu publizieren . der ausbau der klinik zog sich in die lnge , so dass erst jahre spter die klinik und poliklinik fr strahlentherapie feierlich erffnet werden konnte . 
das von bohndorf an der klinik praktizierte vorgehen , zielvolumenorientiert zu handeln , konnte in der brachytherapie , besonders bei der intraoperativen bestrahlung nicht durchgngig realisiert werden , denn die damaligen bestrahlungsplanungssysteme fr die brachytherapie arbeiteten nur applikatororientiert und nicht zielvolumenorientiert , d . 
nach seinen ideen wurde eine spter kommerziell vertriebene mundhalterung entwickelt , mit der bei kooperativen patienten eine reproduzierbare lagerung mit einer geringen unsicherheit erreicht werden konnte , die derjenigen beim einsatz von masken entsprach . an den mikroprozessorgesteuerten beschleunigern konnte mit der entwicklung dynamischer techniken der bewegungsbestrahlung begonnen werden . 
dennoch wurde die entwicklung soweit fortgefhrt , dass unter bestimmten bedingungen dynamische techniken analog zu vmat oder dynamic arc zur verfgung standen , etwa 10 jahre vor der kommerziellen einfhrung . 
b. , dass er abendliche forschungsttigkeit am beschleuniger zulie , auch mit dem risiko eines defekts , was eine patientenbestrahlung am nchsten morgen eingeschrnkt htte . da bohndorf sich nun schon ber 20 jahre im ruhestand bendet , kennen ihn viele der jngeren kollegen nicht . 
der ltere sohn , ehemals chef der radiologie in augsburg , ist inzwischen auch schon im ruhestand , und der jngere sohn betreibt in dsseldorf erfolgreich eine hno - praxis . die ehemaligen mitarbeiter und freunde wnschen dem ehepaar bohndorf fr die nchsten jahre einen erhalt der geistigen und krperlichen frische . jrgen richter , wrzburg hier steht eine anzeige . strahlenther onkol ( 2016 ) 192 : 333341 doi 10.1007 / s00066 - 016 - 0960 - 5 treatment of breast cancer with simultaneous integrated boost in hybrid plan technique influence of flattening filter - free beams marzieh bahrainy1 matthias kretschmer1 vincent jst1 astrid kasch1 florian wrschmidt1 jrg dahle1 jrn lorenzen1 received : 16 november 2015 / accepted : 10 february 2016 / published online : 14 march 2016 springer - verlag berlin heidelberg 2016 abstract objective the present study compares in silico treatment plans using hybrid plan technique during hypofractionated radiation of mammary carcinoma with simultaneous integrated boost ( sib )  . 
the influence of 6 mv photon radiation in flattening filter free ( fff ) mode against the clinical standard flattening filter ( ff ) mode is to be examined . patients and methods rt planning took place with ff and fff radiation plans for 10 left - sided breast cancer patients . 
fff - based rt plans reduced the average treatment time by 17 s / fraction . in comparison to the ff - based hybrid plan conclusion technique the fff mode allows further reduction of the average lad dose for comparable target volume coverage without adverse low - dose exposure of contralateral structures . 
the increased dose rate allows a substantial reduction of treatment time and thus beneficial application of the deep inspiration breath hold technique . keywords breast cancer intensity - modulated radiotherapy volumetric - modulated arc therapy heart dose dose hypofractionation behandlung von brustkrebs mit simultan integriertem boost in hybridplan - technik einfluss des flattening - filter - free - modus zusammenfassung zielsetzung vergleich der in - silico - bestrahlungsplne der klinisch etablierten hybridplan - technik bei hypofraktionierter bestrahlung des mammakarzinoms mit simultan integriertem boost ( sib )  . 
untersucht wird der einfluss von 6mv - photonenstrahlung im flattening - filteroriginal article 334 free - modus ( fff ) gegen den klinischen standard im flattening - filter - modus ( ff ) patienten und methoden die rt - planung erfolgte jeweils mit ffund fff - bestrahlungsplne fr 10 patientinnen mit linksseitigem mammakarzino hybridplne wurden mit zwei tangentialen imrt - feldern und einem vmat - feld umgesetzt . 
 ber das gesamte patientenkollektiv ergaben sich mittelwerte der lad - dosis ( left anterior descending artery ) von 8 , 24 3 , 9 gy in der fffund 9 , 05 3 , 7 gy in der ffgruppe ( p < 0 , 05 )  . 
mit fff - basierten rt - plnen sank die mittlere behandlungszeit um 17 s / fraktion . schlussfolgerung im vergleich zur ff - basierten hybridplan - technik ermglicht der fff - modus eine weitere senkung der mittleren lad - belastung bei vergleichbarer zielvolumenerfassung und ohne nachteilige niedrigdosisbelastung kontralateral gelegener strukturen . 
die erhhte dosisleistung verkrzt die behandlungszeit deutlich und begnstigt die anwendung der deep - inspiration - breath - hold - technik . schlsselwrter brustkrebs intensittsmodulierte strahlentherapie volumenmodulierte arc - therapie herzdosis dosishypofraktionierung introduction three - dimensional conformal radiation therapy ( 3d - crt ) with tangential beam setup is the clinically established gold standard for percutaneous radiotherapy of breast cancer using a linear accelerator . 
the sequential dose saturation of the former tumour region with an electron field is increasingly being displaced by a multiple - field technique with photons in a simultaneous integrated concept ( simultaneously integrated boost , sib ) to further reduce the overall treatment time . 
a recent study [ 1 ] compares hypofractionated radiotherapy of the breast with simultaneous integrated boost with a greatly reduced treatment time ( approximately 3 weeks ) with normofractionated radiotherapy as part of a noninferiority study . 
investigations by the english start trial with 4451 included patients studied the normal 5 - week therapy against shorter therapy schemes with a 10 - year follow - up [ 2 ]  . 
they can increase conformity in dose distribution for complex shaped planning target volumes ( ptv ) in comparison to 3d - crt with improved protection of organs at risk ( oar ) [ 4 ]  . despite initial positive results in vmat - based studies sole use of vmat is now viewed critically for the treatment of breast cancer because of the comparatively high low - dose exposure of healthy tissue [ 57 ]  . 
our study group was able to demonstrate the benefit of a new type of hybrid plan technique while retaining the tangential setup by using sliding window imrt for covering the ptv breast and one additional vmat segment exclusively for the sib region [ 10 ]  . 
only 6 mv flattened photon beams were used in this planning study . if the flattening filter ( ff ) is removed from the beam path , this results in inhomogeneous fluence distribution with a high - dose rate enabling further reduction of outof - field radiation exposure [ 11 , 12 ]  . 
it has already been possible to demonstrate the clinical use of flattening filter free ( fff ) - based radiation plans for the treatment of breast cancer [ 1618 ]  . in the present study the influence of 6 mv photon beams in fff mode compared to the clinical standard in ff mode has been evaluated . 
patients with ptv expansions of 22 cm or more in craniocaudal direction were excluded as they thus exceeded the field size limitations of the linear accelerator truebeam stx ( varian medical systems , palo alto , ca , usa ) that was used . 
the ipsilateral and contralateral lung as well as the contralateral breast were contoured taking into account the requirements of the aro2010 - 01 study and the heart in accordance with feng et al . 
the contouring of the left anterior descending artery ( lad ) , branch of the left coronary artery ( lca ) and the right coronary artery ( rca ) was carried out by a diagnostic radiologist ( jl )  . 
in accordance with the aro - 201001 study 16fractions of2.5 gy to a total dose of 40 gy were prescribed to the breast ptv and 16 fractions of 3.0 gy to a total dose of 48 gy to the ptv sib . 
the calculation of the homogeneity index ( hi ) for both ptv was carried out using the following formula : the following dose parameters were selected for the oar : d2 % , dmean , dmedian . 
the v5gy value was assessed to evaluate the low - dose exposure for the normal tissue ( nt )  . plan verifications were carried out for ff and fff plans with the octavius 4d in combination with the 2d - array octavius 1500 ( ptw , freiburg , germany )  . 
the area of reducing half - shade from the tangent at the level of the isocenter is of particular interest here , starting from 1 cm away from the average field edge at a defined distance of 1050 m related to anatomy the oar lung , heart and lad are located here . 
a visualised example of the measurestrahlenther onkol ( 2016 ) 192 : 3333411 3 336 ment structure using anatomic data for the spatial allocation of the named measurement points is shown in fig . 
significant differences were assumed between tested value pairs for p - values less than 0.05. results if no deviation is indicated , all values are presented as mean appropriate standard deviation . 
the figure shows a diagram of one single ct slice with the isocenter c of the field limit of the tangents ( shown here as solid line a )  . 
the fff group was characterised by lower dose exposure for the heart and coronary vessels . with regard to the average ipsilateral lung dose there were significant differences in dmean , d2 % , v5gy and v10gy ( p < 0.02 ) for ff and fff . 
 for ff the maximum deviation of dcalc to dmeas was 34 and 35 % for fff at 10 mas the distance of the measurement points to the tangential field limit ( high - dose area ) increases the deviation of ff to fff decreases . 
 the comparison of the box plots illustrates the difference in tt with a maximum possible dose rate of 600 mu / min for ff and a dose rate of 1400 mu / min for fff . 
the diagram shows the measured ( solid ) and calculated dose values ( dashed ) , determined at the level of the isocenter starting from 1 cm from the medial field edge at the defined distance of 1050 mm in a horizontal direction . 
 [ 10 ] were able to show the benefit of a new kind of hybrid technique while retaining the tangential setup in sliding window imrt for the coverage of the breast ptv with an additional vmat segment on only the sib region in comparison to the gold standard of the 3d - crt . 
 there was no correlation found between the breast size and the amount of monitor units needed for the two groups ( ff and fff )  . it was possible to keep to the prescribed oar dose limitations in accordance with rtog and the aro - 2010 - 01 study in both planning groups . 
significantly improved results could be proven in the fff group in some dvh parameters for the ipsilateral and contralateral lung lobes , contralateral breast and normal tissue ( nt )  . 
late side effects have been observed in these risk groups even 20 years later and thus represent a substantial risk , particularly in young patients with long life expectancy and pre - existing cardiac disease [ 23 ]  . 
they assume , in contrast to the conclusion of darby , that additional parameters beside the average heart dose should be considered with regard to long - term cardiac effects with imrt . 
 the linac enables dose rates of up to 1400 mu / min in fff mode , thus leading to a significantly reduced average treatment time in the fff group by 22 % . 
the time advantage of the fff plans also allows this technique to be carried out on patients with lower compliance . the time - saving effect is only realised by the imrt tangents , which contribute 80 % ( 2.5 gy ) of the prescribed total dose . 
a forced increase of the dose rate is only possible by reducing the size of the vmat segment at the cost of a substantially increased oar dose ( ipsilateral lung lobe and heart )  . 
it was possible to securely achieve the required clinical prescription of < 1 for 95 % ( dd 3 % and dta 3 mm ) of the examined volume in the high - dose area in both groups . 
the - correspondence percentages were 99 % for fff and 96 % for ff and demonstrate the reproducibility of the combinations of imrt and vmat fields on the linear accelerator . in the local area to 20 mm beyond the field edge there were underestimates of the calculated dose in comparison to the measured dose amounting to an average of 18 % ( 0.07 gy for a single fraction ) for both radiation modes . 
 the measured 2d - array datasets will be corrected by output factor and percentage depth dose in order to recalculate a 3d dose distribution . conclusion the objective of this study was to investigate the combination of the hybrid plan technique with the requirements of the hypofractionated scheme of the aro - 2010 - 01 study ( hyposib )  . 
jst have received speaker honoraria from varian . strahlenther onkol ( 2016 ) 192 : 279287 doi 10.1007 / s00066 - 016 - 0948 - 1 adenosine can thwart antitumor immune responses elicited by radiotherapy therapeutic strategies alleviating protumor ado activities peter vaupel1gabrielemulthoff1 , 2 received : 23 october 2015 / accepted : 25 january 2016 / published online : 9 march 2016 springer - verlag berlin heidelberg 2016 abstract background by studying the bioenergetic status we could show that the development of tumor hypoxia is accompanied , apart from myriad other biologically relevant effects , by a substantial accumulation of adenosine ( ado )  . 
ado has been shown to act as a strong immunosuppressive agent in tumors by modulating the innate and adaptive immune systein contrast to ado , standard radiotherapy ( rt ) can either stimulate or abrogate antitumor immune responses . 
 herein , we present ado - mediated mechanisms that may thwart antitumor immune responses elicited by rt . materials and methods an overview of the generation , accumulation , and ado - related multifaceted inhibition of immune functions , contrasted with the antitumor immune effects of rt , is provided . results upon hypoxic stress , cancer cells release atp into the extracellular space where nucleotides are converted into ado by hypoxia - sensitive , membrane - bound ectoenzymes ( cd39 / cd73 )  . 
mechanisms include ( 1 ) impaired activity of cd4 + t and cd8 + t , nk cells and dendritic cells ( dc ) , decreased production of immunostimulatory lymphokines , and ( 2 ) activation of treg cells , expansion of mdscs , promotion of m2 macrophages , and increased activity of major immunosuppressive cytokines . 
therapeutic strategies alleviating tumor - promoting activities of ado include respiratory hyperoxia or mild hyperthermia , inhibition of cd39 / cd73 ectoenzymes or blockade of a2a receptors , and inhibition of atp - release channels or ado transporters . keywords immunosuppression adenosine tumor hypoxia tumor progression radiotherapy immunostimulation adenosine kann strahlentherapie - vermittelte immunantworten gegen tumore konterkarieren zusammenfassung hintergrund untersuchungen des bioenergetischen status ergaben , dass tumorhypoxie neben vielen anderen bedeutsamen biologischen effekten zu einem starken adenosinanstieg ( ado ) im tumorgewebe fhrt . 
diese hat starke immunsuppressive wirkung sowohl ( 1 ) durch hemmung von tumorinfiltrierenden cd4 + und cd8 + t - , nkund dendritischen zellen sowie immunstimulierender lymphokinsekretion , als auch ( 2 ) durch aktivierung von tregund myeloischen vorluferzellen ( mdscs ) , m2 - polarisation von makrophagen und sekretionssteigerung immunsuppressiver zytokine . 
 abzuschwchen , stehen derzeit folgende therapieoptionen zur verfgung : atmung sauerstoffreicher gasgemische und / oder milde hyperthermie , hemmung der cd39 / cd73ektoenzyme und a2a - rezeptorblockade , hemmung des atp - kanals bzw . 
at standard therapeutic doses ( fractionated doses of 1.82 gy / day up to a cumulative dose of 4570 gy ) , rt also modifies the phenotype of surviving strahlenther onkol ( 2016 ) 192 : 2792871 3 malignant cells and their microenvironment , thus , inducing an effective antitumor immune response leading to immunogenic tumor cell death , tumor shrinkage , and eventually complete tumor eradication [ 15 ]  . 
the immunogenic death of tumor cells is initiated by translocation of calreticulin from the endoplasmic reticulum to the cell surface and release of damps such as ( uncleaved ) atp , hsps ( including hsp70 ) , hmgb1 , s100 proteins , and monosodium urate [ 6 ]  . 
together with pro - inflammatory cytokines such as il - 1b , tnf - a , ifn - a / b , and ifn - g , these proteins can initiate protective antitumor immune responses via m1 - macrophages , monocytes , and dcs that prime cd4 + helper and cd8 + cytotoxic t cells [ 1 , 79 ]  . 
in addition , rt can promote the release of chemokines ( cxcl9 , cxcl10 ; cxcl16 ) by tumor cells , which result in further recruitment of effector t cells . 
an irradiation - elicited increase in the expression of death receptors ( e.g. , fas ligand ) , classical and nonclassical ( mica / micb ) mhc class i / ii molecules , adhesion ( e.g. , icam - 1 ) and co - stimulatory molecules ( e.g. , b7 - 1 ) , toll - like receptors - 4 , - 7 , and potentially 9 ( tlr - 4 , tlr - 7 , tlr - 9 ) that can activate nuclear factor kappa b ( nf - kb ) [ 1113 ] , and other stressinduced ligands including hsp70 [ 14 ] on tumor cells can further enhance their recognition and killing by cytotoxic t and nk cells [ 7 ]  . 
 [ 15 ] suggested that this radiation - induced antitumor immune stimulation can be activated by dual immune checkpoint blockade using the combination anti - ctla - 4 and anti - pd - l1 . apart from these immunostimulatory effects , rt also activates immunosuppressive factors [ 2 , 3 , 7 , 1618 ] leading to a stimulation of inhibitory immune cells such as tregs , mdscs , and protumorigenic m2 - macrophages that suppress t and nk cell - mediated immune responses , thus , promoting tumor cell growth . 
moreover , rt can activate immunosuppressive factors such as tgfand radiationinduced vascular damage which is induced by hypofractionated radiation at doses > 10 gy / fraction have been found to induce hypoxia by critically reduced blood perfusion [ 19 , 20 ] and , thus , might also cause immune suppression . 
these opposing effects of rt on the innate and adaptive immune system can suppress protective antitumor immunity which is also induced by rt [ 16 ]  . at present a majority of publications suggest that rt induces pro - immunogenic rather than immunosuppressive negative effects . 
information is accumulating that high ado levels which are generally found in the hypoxic tumor microenvironment may boost negative effects that significantly dampen the pro - immunogenic processes and thus avoid tumor rejection [ 19 , 2126 ]  . 
the multifaceted mechanisms by which hypoxia - driven adenosinergic ( i.e. , ado - receptor mediated ) pathways act on immune cells , cancer cells , and tumor angiogenesis , facilitate the escape of tumor cells from control by the innate and adaptive immune system and possibly promoting tumor growth , are reviewed in this article . hypoxia - driven adenosine accumulation in tumors two decades ago [ 27 ] , we studied the bioenergetic status of experimental tumors as a function of tumor size and oxygenation status . 
in order to analyze the levels of different metabolites of atp hydrolysis ( purinolysis , yielding nucleotides , nucleosides , purine bases and the final product uric acid , besides the formation of superoxide radical anions and h + ions ) , ado was assessed in snap - frozen tissue samples using gradient ion - pair , reversed phase hplc . key results of these investigations were high ado concentrations in the range of 50100 mm . 
these ectoenzymes are broadly expressed in many tumor cell lines and cells of the tumor microenvironment including the tumor stroma ( e.g. , ecs , foxp3 + treg cells , cd8 + t cells )  . 
intracellular ado formation from amp by a hypoxia - driven catabolic pathway ( partially through hif1a stabilization ) with subsequent ado export into the extracellular space through a nucleoside transporter ( ent1 ) seems to play a subordinate role [ 30 ]  . 
1 schematic diagram showing the individual steps of hypoxia - / hif - 1a - mediated adenosine ( ado ) generation in the intracellular and extracellular space of tumor ( tc ) or stromal cells [ e.g. , immune cells ( ic ) and endothelial cells ( ec ) of tumor microvessels ]  . 
upon hypoxic stress , atp ( atp4 ) is released into the positively charged extracellular space through pannexin - 1 - channels ( panx - 1 ) or via exocytosis . 
following the release of atp into the extracellular space , the hypoxia - / hif - 1a - dependent tandem - enzymes cd39 and cd73 , the major nucleotide catabolizing enzymes , convert atp into amp and thereafter to ado . 
upon accumulation in the extracellular space , ado acts in an autocrine and paracrine fashion in a way that ( a ) tumor - mediated immunesuppression occurs and ( b ) stimulating effects on endothelial ( ec ) and tumor cells ( tc ) are exerted through activation of different ado receptors ( ar )  . 
hif - 1a sensitive membrane proteins are indicated ( a2a and a2b receptors included ) adenosine receptors and signaling pathways in tumor and immune cells ado is not a mere metabolite of atp hydrolysis in cancer cells as generally thought in the past . 
adoreceptor subtypes a1 , a2a , a2b , and a3 were found to be upregulated in various tumor cell lines , but also in ecs of the tumor microvessels and in a range of immune cells ( particularly in immunosuppressive treg cells ) [ 3234 ]  . observations concerning the modulation of tumor growth upon activation of a1 receptors are still conflicting since both antiand protumorigenic effects have been described [ 35 ]  . 
a2a , a2b , and a3 receptors are implicated in tumor angiogenesis via secretion of pro - angiogenic vegf , bfgf , angiopoietin - 2 , and il - 8 [ 32 , 35 ]  . 
as nonredundant part of a negative feedback loop , a2a receptors are expressed on a variety of immune cells preferentially involved in the inhibition of antitumor immune functions ( table 1 )  . all receptor subtypes are g - protein coupled that either stimulate ( hif - 1a - sensitive gs - coupled a2a a2b ) or inhibit ( a1 , a3 ) adenylate cyclase ( adenylyl cyclase ) activity with concordant changes of intracellular camp levels . 
 all ado receptors also couple to mitogen - activated protein kinase ( mapk ) pathways with activation of erk1 and erk2 [ 19 ]  . adenosinergic tumor immune evasion by inhibition of immune cells functions the seminal observations of hoskin et al . 
 [ 25 , 28 ] have established a role for ado in the immune escape from immune control through blocking antitumor immune responses ( mounting an immunogenic barrier )  . 
at present , there is strong evidence that adenosinergic signaling , preferentially via a2a receptors , in hypoxic , ado - rich tumor microenvironments can lead to a broad spectrum of strong immunosuppressive properties that facilitate tumor escape from immune control ( and immunotherapies )  . 
adenosinergic effects on immune cellsa ado receptors involved a2a , a2b a2a , a2b impaired activity of dendritic cellsb enhanced proliferation of treg cellsb leading to suppression of tumor - associated antigen presentation and weakening cytotoxic t cell functions expansion of mdscb functions promoting tumor tolerance ( tumor evasion ) through inhibition of dcs , nk cells , t cells , and promotion of m2 proliferation inhibition of tumor - suppressive m1 macrophages ( m2 polarization ) activation of immunosuppressive macrophages a2a , a2b decrease in antitumor activities of nk cellsb ( e.g. , downregulation of effector molecule expression , e.g. , perforin ) weakening of tumor - directed cd4 + cellsb , reduced th1 - type lymphokine production ( e.g. , inf - g , tnf - b , il - 2 ) decreased proliferation and reduced cytotoxicity of cd8 + t cellsb increased activity of immunosuppressive proteins ( e.g. , tgf - b , il - 10 , galectin - 1 ) , immune checkpoint receptors ( ctla - 4 , pd - 1 ) , and transcription factors ( e.g. , foxp3 ) promotion of chronic inflammation fostering a2a a1 tumor growth increased production of metalloproteases by neutrophils promoting metastasis b . 
adenosinergic effects on cancer cells stimulation of cell cycle and proliferationc a1 , a2a stimulation of glycolytic flux increase in hif - 1a expression increase in production of pro - angiogenic factors a3 stimulation of cell migration and invasion facilitation of metastatic spread c . 
adenosinergic effects on angiogenesis stimulation of proliferation and migration of a2a , a2b increase in vegf expression in ecs increase in bfgf expression in ecs stimulation of il - 8 secretion from stromal and a2a , a2b , a3 tumor cells increase in angiopoietin expression see list of abbreviations . abroad spectrum of immunosuppressive properties facilitates tumor escape from immune control mainly via stimulation of a2a receptors . bimmune cells involved in antitumor immunity elicited by rt . ccontrasting proand antitumor effects have been described upon a1 receptor activation . therapeutic strategies alleviating protumor ado activities in the light of the data presented , the following therapeutic strategies may help to mitigate ( or even eliminate ) the tumor promoting activities of ado . 
however , even inspiration of 100 % oxygen most probably is not able to completely eradicate severe tumor hypoxia in all malignancies , especially human malignancies and considering the multicausal pathogenesis of this condition [ 30 , 3842 ]  . 
upon respiratory hyperoxia , a switch from glycolytic breakdown to a more oxidative metabolism of glucose resulting in a reduced production of lactic acid and protons can significantly attenuate tumor tissue acidosis [ 43 ]  . 
2 immunosuppressive adenosine ( ado ) actions and immunostimulatory radiotherapy ( rt ) - elicited processes in solid tumors ( with detailed effects of ado - rich tumor microenvironments on key cells and cytokines involved in the antitumor immune responses )  . 
as a result , a reduction in tumor hypoxia has been described in the preclinical ( and occasionally in the clinical ) setting and , thus , reversal of the hypoxiainduced antitumor immune suppression has to be expected . 
in addition , mild thermal therapy has the ability to enhance the function of some immune effector activities that are inhibited by hypoxia . the aspects summarized in ( a ) and ( g ) refer to modulations of the tumor microenvironment , ( b ) , ( d ) , and ( e ) refer to ado transporters and ado receptors , respectively , and ( c ) and ( f ) discuss the inhibition of ectoenzymes and interference with atp transport , respectively . 
other therapeutic strategies currently tested to dampen ado - mediated immunosuppression exploit small molecule inhibition of hifactivity [ 57 ] , downregulate a2a and a2b receptor density on antitumor t cells [ 58 ] , and enhance ado degradation to inosine by ado - ( ecto - ) deaminase [ 53 ]  . conclusion hypoxia - triggered accumulation of ado is a crucial microenvironmental factor ( pathophysiological hallmark ) in a wide range of solid tumors . 
ado acts in an autocrine and paracrine fashion on cells involved in the innate and adaptive immune response , on cancer cells and on ecs , thus , strahlenther onkol ( 2016 ) 192 : 2792871 3 hier steht eine anzeige . 286 critically suppressing antitumor immune responses , stimulating tumor cell proliferation , migration and metastatic dissemination , and promoting tumor angiogenesis . 
ado - mediated dampening of the antitumor immune response is based on inhibition of cytotoxic t cells , nk cells , dcs , and th1 - type immunostimulatory cytokine production by cd4 + t cells , and on activation of treg cells , mdscs , m2 polarization , and various immunosuppressive cytokines . 
immunosuppressive ado actions can thwart the antitumor immune response elicited by standard rt and may counteract immunotherapies of solid tumors , since immune cells involved are common for both immunosuppressive ado actions and immunostimulatory rt processes . 
currently tested approaches to alleviate / abrogate adenosinergic tumor immune escape include respiratory hyperoxia ( reduction of tumor hypoxia ) , mild hyperthermia ( reduction of tumor hypoxia , enhanced function of some immune effector activities inhibited by hypoxia ) , inhibition of atp release and ado export , antagonizing of ado receptors ( especially a2a receptors ) , targeting cd39 / cd73 with specific mabs , and inhibiting immune checkpoints ctla - 4 and pd - 1 ( combined with a2aor cd73 - blockade )  . acknowledgments the authors would like to thank anett lange for her valuable help during preparation of this article . this work was supported by eu - celleurope ( 315963 ) ; bmbf ( strahlenkompetenz , 02nuk038a ; innovative therapies , 01gu0823 ; nsclc , 16gw0030 and the dfg cluster of excellence : munich centre for advanced photonics )  . 
sfb 824 / 2 ; inst 95 / 980 - 1 fugg ; inst 411 / 37 - 1 fugg irradiation devices and the helmholtz zentrum mnchen ( hmgu ) , ccginnate immunity in tumor biology . compliance with ethical standards conflictofinterest p . 
multhoff state that there are no conflicts of interest . the manuscript does not include studies on humans or animals . strahlenther onkol ( 2016 ) 192 : 322332 doi 10.1007 / s00066 - 016 - 0949 - 0 4d - listmode - pet - ct and 4d - ct for optimizing ptv margins in gastric lymphoma determination of intraand interfractional gastric motion gabriele reinartz1 uwe haverkamp1 ramona wullenkord1 philipp lehrich1 jan kriz1 florian bther2 klaus schfers2 , 4 michael schfers2 , 3 , 4 hans theodor eich1 received : 20 june 2015 / accepted : 26 january 2016 / published online : 22 february 2016 springer - verlag berlin heidelberg 2016 abstract purpose new imaging protocols for radiotherapy in localized gastric lymphoma were evaluated to optimize planning target volume ( ptv ) margin and determine intra - / interfractional variation of the stomach . methods imaging of 6 patients was explored prospectively . 
 intensity - modulated radiotherapy ( imrt ) planning was based on 4d / 3d imaging of computed tomography ( ct ) and positron - emission tomography ( pet ) - ct . 
static and motion gross tumor volume ( sgtv and mgtv , respectively ) were distinguished by defining gtv ( empty stomach ) , clinical target volume ( ctv = gtv + 5 mm margin ) , ptv ( gtv + 10 / 15 / 20 / 25 mm margins ) plus paraaortic lymph nodes and proximal duodenu overlap of 4d - listmodepet - based mctv with 3d - ct - based ptv ( increasing margins ) and v95 / d95 of mctv were evaluated . 
die planung der intensittsmodulierten strahlentherapie ( imrt ) basierte auf 4d - / 3d - bildgebung von comoriginal article1 3 putertomographie ( ct ) und positronenemissionstomographie - ct ( pet - ct )  . 
wir differenzierten zwischen static und motion gesamttumorvolumen ( sgtv , mgtv ) unter definition von gtv ( leerer magen ) , klinischem zielvolumen ( ctv = gtv + 5 mm sicherheitsabstand ) , ptv ( gtv + 10 / 15 / 20 / 25 mm sicherheitsabstand ) plus paraaortalen lymphknoten ( lk ) und proximalem duodenudie berschneidung des 4d - listmode - pet - basierten mctv mit dem 3d - ct - basierten ptv ( steigender sicherheitssaum ) und die v95 / d95 des mctv wurden evaluiert . 
die konventionelle 3d - ct - planung mit schrittweise zunehmenden ptv - sicherheitsabstnden von 10 / 15 / 20 / 25 mm resultierte in steigender dosisversorgung des mctv ( 4d - listmode - pet - summation - ct ) und steigender d95 und v95 des mctv . 
bei 3 von 6 patienten war ein ptv - sicherheitsabstand von 15 mm ausreichend , bei 4 von 6 patienten 20 mm und bei 5 von 6 patienten 25 mm . schlussfolgerung die imrt - planung auf basis von 4dpet - ct / 4d - ct mit der online - conebeam - ct kann die ptv - sicherheitsabstnde individualisieren und die zielvolumenerfassung bei magenlymphomen optimieren . schlsselwrter intensittsmodulierte strahlentherapie positronenemissionstomographie magenlymphome 4 - d - computertomographie sicherheitssaum planungszielvolumen conebeam - computertomographie introduction radiation is an established ( multimodal ) treatment with excellent long - term results in localized gastric lymphoma [ 15 ]  . 
we used 4d - ct , 4d - positron - emission tomography ( pet ) - ct , cone - beam ct imaging techniques and newly developed 4d - ct reconstructions on the basis of 4d - listmode - pet . 
rt planning based on 4d - imaging was compared with conventional 3d - ct based planning with regard to target miss and normal tissue doses . patients and methods imaging of 6 patients treated with imrt using a varian truebeam linear accelerator for gastric lymphoma from october 2011 until march 2013 at the university hospital of muenster , was evaluated prospectively for this study . 
 the patient and tumor characteristics : 3 women / 3 men , median age 53.5 years ( range : 4361 years ) , 3 diffuse large b - cell lymphoma ( dlbcl ) / 3 indolent gastric lymphomas , 5 stage ii1 / 1 stage ii2 disease . 
for detection of gastric motion , the 4d - listmode - pet data were processed by in - house reconstruction algorithms developed at the european institute for molecular imaging ( eimi ) , using accurate high coincidence gating methods with real organ displacement [ 7 ]  . 
the 4d - listmode - pet data provided a basis for creation of 3d - ct reconstructions named sum - ct ( summation - ct , based on 10 respiratory gates ) and add - ct ( addition - ct , based on breath - hold cts at end - inhalation / exhalation ) , in which the contours of the stomach and the normal tissue were clearer [ 7 ]  . 
for generation of the sum - ct images , listmode - pet data were reconstructed into 10 respiratory - gated images ( gates ) and motion between a reference gate ( usually the end - expiration phase ) and all remaining gates was calculated . 
using the calculated motion vector fields , the acquired single ct data ( same respiratory phase as the reference pet ) were transformed into nine ct images , resulting in ten ct datasets for ten respiratory phases . 
similar to the generation of the sum - ct data , both the end - inhalation / exhalation ct datasets were averaged to form a new virtual 3d - ct dataset named add - ct . 4d - / 3d - ct and listmode - pet - ct together with sumct , add - ct and evaluation cone - beam ct [ 8 ] were taken for imaging fusion of all series . 
 ( b ) 4d - ct with transferred dose from 3d - ct plan , 4d - ctv incompletely covered by 95 % isodose ( black ) ; white = mgtv in sum - ct ach structure in the add - ct better reflects the inhalation / exhalation , whereas the reconstructed sum - ct represents an averaging of the respiratory phases . 
the organs at risk ( oar ) including the kidneys , liver , and myelon were contoured in the conventional 3d - ct exclusively . we evaluated the stomachs center of gravity in inhalation / exhalation and determined the maximal length of displacement between in - / exhalation in all directions [ 9 ]  . 
the treatment plans were created for the truebeam for 15 mv photon beams as arrangement of seven fields at predetermined gantry positions ( 0 / 51 / 102 / 153 / 204 / 255 / 306 ) in the sliding - window imrt technique . 
in addition , the setup variation was calculated on base of the gastric shifts in the online cone - beam ct , using the margin recipe by van herk et al . 
we also measured the v95 / d95 of the online ctv in the cone - beam ct ( cb - ctv ) using the 4d - ct based plan in comparison to the sum - ct based plan . 
we calculated the percentage volume of the liver and both kidneys receiving 28 gy ( v28 30 % ) or 20 gy ( v20 30 % ) , respectively , comparing the 3d - ct with the 4d - ct and 4d - listmodepet - based plans . the comparison of the resulting oar doses between the different treatment plans was carried out applying the nonparametric wilcoxon significance test for paired samples . 
statistical significance as p value < 0.05. intra - / interfractional stomach variation the intrafractional stomach displacement caused by breathing was complex with movement in all three dimensions [ 11 , 12 ]  . 
the respiratory excursions in add - ct at end - inhalation versus exhalation showed intrafractional motion of the center of gravity of the stomach with great interindividual variability in stomach shifts , especially along the vertical axis ( table 1 )  . 
the four rt plans for each patient , based on the four different imaging methods , showed a great variability of gastric volume mgtv in contrast to conventional 3d - ct . 
 the enlargement of mgtv in 4d imaging methods showed interindividual variability and varied in size depending on the different 4d imaging methods with the largest increase of gastric volume mgtv in add - ct . the coverage of the ctvs in the dvh of the four treatment plans based on different imaging modalities was evaluated by different methods : the results using the d95 / v95 of ctv listed in table 2 show inhomogeneous results in the 6 patients . 
in contrast , the 4d - listmode - pet - based ptvs showed marginal or sufficient coverage of the 3d - ct - ctv in 3 of 6 patients ( patients 2 , 3 , 6 ; table 2 )  . 
calculation of the median ctv coverage for all patients , referring to the d95 / v95 of ctv , the treatment plans based on 3d - ct and 4d - ct showed an insufficient coverage of the ctvsumct and ctvaddct . 
 the results for the right / left kidney showed interindividual variability of the v20 with a tendency towards higher mean right / left kidney doses and towards higher maximum myelon doses in treatment plans based on sum - ct and add - ct . the wilcoxon signed - rank test showed statistical significance for comparison of oar doses between the rt plans based on the following cts : median v28liver ( p = 0.043 ) in sum - ct versus add - ct , mean right kidney dose ( p = 0.027 ) in 3d - ct versus sum - ct , median v20left kidney ( p = 0.028 ) and mean left kidney dose ( p = 0.046 ) in 3d - ct versus strahlenther onkol ( 2016 ) 192 : 3223321 3 327 table 3 dose coverage of clinical target volume ( ctv ) by planning target volume ( ptv ) in radiotherapy ( rt ) plans based on 3d - ct / 4d - ct / 4d - listmodepet - based ct reconstructions ( sum - ct , add - ct )  . 
pet positron - emission tomography , ct computed tomography table 4 dose coverage of clinical target volume ( ctv ) by planning target volume ( ptv ) in radiotherapy ( rt ) plans based on 3d - ct / 4d - ct / 4d - listmodepet - based ct reconstructions ( sum - ct , add - ct )  . 
apart from isolated p - values , the overall results for the oar doses showed no conspicuous differences between the treatment plans based on different imaging methods . impact of increasing ptv margin on ctv coverage in 3d - ct the coverage of the ctvs of rt plans based on different imaging methods by 3d - ct based ptv with increasing margin was established by evaluation of d95 / v95 of ctv ( table 5 )  . referring to the ctv coverage in sum - ct by means of d95 / v95 of ctv a ptv margin of 25 mm was sufficient in 5 of 6 patients , a ptv margin of 20 mm was marginal or sufficient in 5 of 6 patients , a ptv margin of 15 mm was sufficient in 3 of 6 patients , a ptv margin of 10 mm was at least marginal in 1 of 6 patient , respectively ( table 6 )  . referring to the ctv coverage by means of d95 / v95 of ctv , a ptv margin of 10 mm was required for sufficient coverage of ctv - 4d - ct , whereas a ptv margin of 15 mm was required for at least marginal coverage of ctv - sumct and ctv - add - ct , and a ptv margin of 20 mm was required for sufficient coverage of ctv - sum - ct and ctvadd - ct , respectively ( table 7 )  . on ctv coverage in cone - beam ct measuring the percentage overlap volume of the five conebeam ct ctvs ( patient no.6 ) with increased ptv documented sufficient ctv coverage in 2 of 5 cone - beam cts ( numbers 2 , 3 , 5 ) as required ptv margin 15 mm , whereas in 2 of 5 cone - beam cts ( numbers 1 , 4 ) it was 20 mm , respectively . strahlenther onkol ( 2016 ) 192 : 3223321 3 328 fig . 
2 clinical target volume ( ctv ) of the five cone - beam ( cb ) - cts in one patient seems sufficiently covered in listmode - pet - based treatment plan : median dose coverage of cb - ct - ctv in rt plans based on 3d - ct / 4d - ct / 4d - listmodepet - based ct reconstructions ( sum - ct , add - ct )  . 
rt radiation treatment on oar doses in 3d - ct all of the 6 patients showed an almost linear and significant gain of the mean liver dose and of v28liver in the course of increasing ptv margins [ fig . 
our findings revealed insufficiency of the conventional 3d - ct - based rt planning in gastric lymphoma . stomach position and displacement interfractional changing of gastric volume showed great interindividual variation , taken as a basis for studying the interfractional modification of gastric volume , instead of using vector shifts as described in watanabe et al . 
the simultaneous increase of gastric volume and air content in the stomach during the course of radiation series possibly reflects a radiogenic effect on the stomach ( mucosa ) [ 17 ]  . 
3 specific organs - at - risk ( oar ) doses at median for all patients in radiotherapy ( rt ) plans ( a ) based on 3d - ct / 4d - ct / 4dlistmode - pet - based computed tomography ( ct ) reconstructions ( sum - ct , add - ct ) , ( b ) among different ptv margins . 
rt right , lt left tion on more patients is required for ascertained conclusions on this topic . the intrafractional gastric shifts are mainly caused by breathing movements ( [ 18 ] , abstract at the annual meeting of the american society of radiation oncology ) , measured by 4d - listmode - pet based add - ct . 
examined the intrafractional movement of the stomach based on conventional 3d - ct in inhalation / exhalation among 6 patients [ 15 ] along the anteriorposterior ( ap ) , rightleft ( rl ) and superiorinferior ( si ) axis . 
the maximum movement was detected in strahlenther onkol ( 2016 ) 192 : 3223321 3 330 table 5 dose coverage of clinical target volume ( ctv ) by 3d planning target volume ( ptv ) with increasing ptv marg d95 / v95 of ctv superiorinferior direction , the minimum movement was detected in rightleft direction , respectively . 
in our study the intrafractional mean gastric movement was smaller , potentially because of the averaged data being calculated during the long lasting 4d - listmode - pet measurement . target definition based on different imaging methods the investigation of intrafractional gastric movement based on 4d - listmode - pet measurement and following ct reconstruction provided a superior reproducibility of the inner organs , eliminated respiratory outliers , and delivered a better description of the stomach boundary in contrast to 4d - ct , even without radiation exposure . the comparison of stomach volumes between different imaging methods confirmed that 3d - ct shows smaller volumes than 4d - listmode - pet based reconstruction - ct . 
 4d - listmode - pet at end - inhalation / exhalation ( addct ) showed the greatest stomach volumes , whereas the 4d - listmode - pet - based sum - ct showed slightly smaller strahlenther onkol ( 2016 ) 192 : 3223321 3 table 6 dose coverage of clinical target volume ( ctv ) by 3d planning target volume ( ptv ) with increasing ptv margrecommendation for ptv margin on base of 4d - listmode - pet sum - ct ( d95 / v95 ) is individual table 7 dose coverage of clinical target volume ( ctv ) by 3d planning target volume ( ptv ) with increasing ptv margmedian coverage of ctv by d95 / v95 for all patients volumes , emphasizing the statistical probability of gastric localization . 
 [ 19 ] also proved an increase of stomach volume of 51.8 % at mean in 4d - ct compared with 3d - ct . in comparison to add - ct , the target definition on the base of sum - ct should be preferred for sparing radiation volume . 
 [ 13 ] , no general difference for 4d imaging - based target definition was evident among oar doses , besides isolated noticeable p - values ( 5 out of 48 )  . 
the geometric relationship between the oar and the target is also relevant for oar doses [ 20 ]  . we aimed at optimizing target definition for target coverage and oar protection simultaneously and therefore determined the overlap of all ctvs with the ptvs as well as the d95 / v95 of all ctvs . 
the results of both measurements varied slightly showing a tendency to a better ctv coverage by determination of the d95 / v95 in contrast to the ptv / ctv overlap . the ptv definition with 10 mm margin around the staticgtv showed inadequate coverage of intra - / interfractional stomach displacement . 
according to other authors and their presentations at the annual meeting of the astro , the required margins are relatively large [ 21 , 22 ] and the common recommendation for ptv margin around gtv is 20 mm , especially along the vertical axis , in case of 3d - ctbased rt planning [ 23 , 24 ]  . 
oar doses increase with growing ptv margins as well , documenting the need for critical evaluation before expanding the margin . the interfractional movement of gastric volume can be quantified for target definition with repeated acquisition of ct data [ 15 , 22 ]  . 
online cone - beam ct ensures daily covering of gastric movement as an alternative evaluation method . conclusion in our investigation into the value of 4d - ct and 4d - petct on the target definition in gastric lymphoma , it was found that imrt planning based on 4d techniques helps to define ptv margins in gastric lymphoma for each patient to optimize individual target coverage . 
in addition , individual inter - / intrafractional gastric movement should be checked regularly using cone - beam ct . acknowledgments this study was partly supported by the deutsche forschungsgemeinschaft ( dfg ) , collaborative research centre 656 ( sfb 656 ) , muenster , germany ( projects b02 and b03 )  . strahlenther onkol ( 2016 ) 192 : 3223321 3 332 compliance with ethical standards conflict of interest g . 
prior to clinical implementation , positioning accuracy was evaluated and compared to clinically established imaging techniques . methods and materials an inhomogeneous thorax phantom with four tumor - mimicking inlays was imaged in 10 predefined positions and registered to a planning ct . 
manual registration , automatic registration provided by the manufacturer and an additional inhouse developed manufacturer - independent framework based on the matlab registration toolkit were applied . results systematic setup error was reduced to 0.05 mm by high - precision phantom positioning with optical tracking . 
im hinblick auf die klinische implementierung wurde die positionierungsgenauigkeit untersucht und mit klinischetablierten bildgebungstechniken verglichen . methoden und material ein inhomogenes thoraxphantom mit 4 tumorhnlichen inlays wurde in 10 vordefinierten positionen aufgenommen und auf ein planungs - ct registriert . 
however , high fractional doses in combination with breathing - induced motion require meticulous motion management . common image guidance techniques for pretreatment target localizations are megavoltage cone - beam computed tomography ( mv - cbct ) [ 6 , 7 ] or perpendicularly mounted kilovoltage ( kv ) cbct [ 8 , 9 ]  . 
to compensate for breathing motion in lung sabr , gating [ 1012 ] , tracking [ 13 , 14 ] , formation of an internal target volume based on a 4d cbct [ 1517 ] , or breath - hold strategies such as deep inspiration breath - hold ( dibh ) are usually applied . 
the dibh strategy has several dosimetric and methodical advantages [ 1822 ]  . the combination of cbct image - guided patient positioning , hypofractionated treatment , and computer - assisted breath - hold gating resulted in excellent treatment outcomes [ 20 , 23 ]  . 
initially , continuous cbct image acquisition was performed in repeated breath - hold , generating a volume reconstructed from 65 % breath - hold phases and acceptable image quality with small motion artifacts . 
finally , the kv - mv volume replaced the initial kv volume in the xvi registration tool for further routine processing [ 27 , 29 , 30 ]  . mv180 cbct the development of the kv - mv synchronization hardware also allowed creating an mv180 cbct preset , using the same low - dose mv beam characteristics ( 8 mu equally distributed over a 180 arc plus 10 cone angle )  . 
due to the triggered linac pulse and the inability of the mv panel to constantly read out , the projections could only be acquired every 5 , resulting in a dataset of 36 mv projections . 
the gantry speed was 1 rpm and the image acquisition time for breath - hold treatment with one necessary breathing phase was 30 + 10 s . the planning ct ( brilliance big bore oncology , philips , hamburg , germany ) was used as reference for registration . phantom setup four different custom - made tumor - mimicking inlays were placed in the inhomogeneous thorax phantom ( model 002lfc , cirs , norfolk , va , usa )  . 
the tumor shapes represented a ball , a cylinder with spikes , and two star - shaped objects with large and small body ( diameter = 615 mm )  . 
each tumor shape was marked at isocenter in the planning ct and set as reference in the xvi software registration tool . in total , 10 different shifts were preselected randomly based on a gaussian distribution around the isocenter position ( positive on right hand side ) and applied in rightleft ( rl ) , anteriorposterior ( ap ) , and craniocaudal ( cc ) directions . 
the standard deviation of the gaussian was chosen to be 1 cm ( table 2 )  . imaging speed number of projections imaging time rpm 2 min 1 rpm 30 s to compare with a clinically used preset routinely used for lung / liver sabr , conventional kv - chest360 cbct was applied . 
clinical image acquisition time is 2 min ( standard imaging gantry speed rpm ) with continuous acquisition and 34 min for imaging in dibh due to necessary freebreathing interruptions [ 25 , 26 ]  . kv180 cbct for correct reconstruction , filtered backprojection methods require a minimum scan angle of 180 ( plus 10 cone angle in our case ) with centered detector panel [ 31 , 32 ]  . 
gantry speed was accelerated to 1 rpm , resulting in 15 s imaging time.our automated workflow software used a communication port to adjust the linac parameters for a low mv dose output ( 4 mu distributed over 90 )  . 
our hardware triggered the linac pulses and synchronized kv - mv image acquisition by using every fifth kv pulse to trigger the mv panel readout , such that no interfering linac pulse occurred during mv readout , i.e. , mv radiation was off when mv detector was read out [ 27 , 29 ]  . 
the order of the volumes was mixed when presented to the clinicians such that objectiveness was assured . ( cid : 404 ) automatic registration in xvi software automatic registration provided in xvi software is based on a voxel greyscale intensity value algorithm [ 34 ]  . 
the correction reference point was the isocenter position of the planning ct . ( cid : 404 ) automatic registration with in - house developed software to guarantee manufacturer - independent evaluation , a framework was developed for automatic registration with the rigid intensity - based registration toolkit provided in matlab , using a mutual information algorithm [ 35 ]  . all datasets were cropped to separate regions of interests ( tumor inlays ) similar to the alignment box in xvi . 
 thus , 4 times 30 datasets were collected . to provide comparison with a clinically used preset , the panel position and the gantry speed were changed to kvchest360 setup and the procedure was repeated for all tumormimicking inlays ( 4 times 10 shifts )  . evaluation methods the detection error was the difference between registration result and original couch shia total of 36 datasets were generated , separated by imaging technique , registration method , and translational shift direction . 
furthermore , the same test was results the cbct scans of the small star - shaped tumor inlay for different imaging techniques in a representative axial slice are shown in figure 2 . 
in row 1 , the full phantom reconstruction is shown and in row 2 , the full phantom cbct is overlaid with the planning ct after successful registration of shift 1 . 
the two automatic registration results validated the objective performance of manual registration by the clinical experts . the corresponding mean detection errors ( standard deviation ) and the maximum / minimum values are provided in table 3 . 
row 1 : manual registration , row 2 : automatic registration ( xvi ) , row 3 : automatic registration ( in - house ) ( xvi ) method , maximum cc error with automatic registration ( in - house )  . 
the detection error rather attributed to the interplay of degraded image quality , as well as error - prone software interpolation for challenging star - shaped tumor inlay of diameter 10 mm ; in planning ct the slice - to - slice variation was large due to a slice thickness of 1 mas a matter of fact , the marginal volume sizes of all four tumor - mimicking inlays induced challenging test paradigms for registration accuracy . 
outliers in kv - chest360 cbct for manual registration in cc direcstrahlenther onkol ( 2016 ) 192 : 3123211 3 318 tion attributed to erroneous matching by the same physician . 
for kv - chest360 cbct , the pixel size and the slice thickness were 1 mm , and 0.5 mm for kv180 , mv180 , and kv - mv cbct . 
thus , the registration offset of only one pixel could potentially result in an offset of 0.5 m since the currently achievable precision in clinical routine is 1 mm , systematic and stochastic errors in this study are within the given limit . paired difference test showed significant advantage of manual vs . 
all three methods resulted in mean strahlenther onkol ( 2016 ) 192 : 3123211 3 displacement errors of 0.00.8 mm , which is the currently achievable precision with volume imaging in clinical routine . 
the absolute maximum error in all matching attempts was 1.6 mm for manual matching , thus , without exception fulfilling the clinical requirements . estimation of measurement setup error similar registration accuracy studies to assess different clinically used imaging modalities were performed by yan et al . 
the initial isocenter position was calibrated and each couch shift relative to this zero position could be defined as reference for latter detection error calculation . optical tracking lead to negligible couch movement tolerances . 
fundstrahlenther onkol ( 2016 ) 192 : 3123211 3 320 ing was received by an elekta research grant and by grant numbers bo3192 / 1 - 1 , we5294 / 1 - 1 , and lo713 / 3 - 1 of the german research council ( dfg )  . compliance with ethical guidelines conflicts of interest a . 
at the time of this analysis , information on potency 1 year after treatment was available for 62 of 91 patients ( 42 treated with hypofractionation : 2.352.65 gy / fr , 7074.2 gy ; 20 with conventional fractionation : 7478 gy )  . 
prospectively collected individual information and dmax / dmean to the penile bulb were available ; the corresponding 2 gy - equivalent values ( eqd2_max / eqd2_mean ) were also considered . 
fiorino 1 radiotherapy , san raffaele scientic institute milano , italy prostate cancer program , fondazione irccs istituto nazionale dei tumori milan , italy 3 medical physics , san raffaele scientic institute 4 radiation oncology 1 , fondazione irccs istituto nazionale milan , italy dei tumori milan , italy 5 radiotherapy , ospedale bellaria bologna , italy 6 radiotherapy , ospedale asl9 ivrea , italy 7 radiotherapy , cliniche gavazzeni - humanitas bergamo , italy variable backward logistic regression : the best cut - off values discriminating between potent and impotent patients were assessed by roc analyses . 
the discriminative power of the models and goodness - of - t were measured by auc analysis and the hosmerlemeshow ( h&l ) test . results at 1 - year follow - up , 26 of 62 patients ( 42 % ) became impotent . 
zum zeitpunkt dieser analyse waren informationen ber die potenz von 62 / 91 patienten ein jahr nach der behandlung verfgbar ( 42 hypofraktioniert behandelt : 2 , 352 , 65 gy / fr ; 7074 , 2 gy ; 20 konventionell : 7478 gy )  . 
prospektiv erhobene individuelle informationen und dmax / dmean am bulbus penis waren verfgbar , ebenfalls bercksichtigt wurden die entsprechenden 2 gyquivalent werte ( eqd2_max / eqd2_mean )  . prdiktoren der 1 - jahres - impotenz wurden durch uniund multivariable rckwrtsgerichtete logistische regression beurteilt , die besten cut - off - werte zur potent - impotentunterscheidung durch roc - analysen . 
die diskriminative power der modelle und die anpassungsgte wurden mithilfe der auc und dem hosmerlemeshow - test bestimmt . ergebnisse bei der kontrolle nach einem jahr waren 26 / 62 patienten ( 42 % ) impotent . 
die einzigen vorhersagevariablen waren baseline iief1 - 5 ( bester cut - off iief1 - 5 19 ) , dmax 68 , 5 gy und eqd2_max 74 , 2 gy . 
das impotenzrisiko ein jahr nach hochdosierter radiotherapie hngt ab von eqd2_max im bulbus penis und vom baseline iief1 - 5 . schlussfolgerung eine signikante risikoreduktion ist v.a. zu erwarten bei schonung des bulbus bei potenz bzw . 
nur schwacher impotenz zu behandlungsbeginn ( iief1 - 5 > 17 )  . schlsselwrter prostatakrebs radiotherapie erektile dysfunktion vohersagemodelle dosiseffekte potency preservation after radiotherapy for prostate cancer is an issue of growing interest [ 1 , 2 ]  . 
the increasing number of younger , potent and sexually active patients treated with radiotherapy ( rt ) is leading radiation oncologists to consider the avoidance of severe erectile dysfunction ( ed ) as a major goal . a higher baseline potency score has been reported to be associated with better potency preservation in patients who are potent before starting rt [ 14 ] ; ageing [ 5 ] , vascular co - morbidities and psychological issues have also been reported to be correlated with potency loss [ 3 , 4 , 6 ]  . radiation - induced effects on potency mostly occur within the rst 2 years of rt [ 7 ] , although similar ed rates at 1 and 2 years after treatment have recently been reported [ 4 , 8 , 9 ]  . several studies suggested that the risk of ed after rt is correlated with the dose received by structures related to erection , rstly the penile bulb ( pb ) [ 2 , 10 ]  . 
however , there is a clear lack of prospective studies focused on potent patients including dosimetry data referring to the pb and prospective information regarding potential clinical risk factors [ 2 ]  . 
a multi - centric prospective study aimed at identifying reliable predictors of patient - reported urinary toxicity and ed ( termed due01 [ 11 , 12 ] ) was started in 2010 : the current report concerns the ad interim results regarding 1 - year patient - reported potency on hormone - nave patients who were potent before rt . patients and methods the due01 study and patient characteristics the due01 study started in 2010 , after the approval of the ethics committees of the eight participating centres , and patient enrolment was completed at the end of 2014 . 
the aim of this study is to develop predictive models of urinary toxicity and ed after rt for prostate cancer delivered with conventional fractionation to 70 gy or with moderate hypofractionation to 65 gy ( 2.32.7 gy / fraction )  . 
ed was prospectively evaluated by means of the international index of erectile function ( iief ) [ 13 ] , to be completed by patients before rt , at the end of rt , as well as 3 and 6 months after rt completion , and subsequently every 6 months up to 5 years . 
these ve questions are focused on the ability / difculty to have an erection and to have ( satisfactory ) sexual intercourse ; for each of the ve items , a score from 0 to 5 ( from bad to optimal ) has to be scored by the patient , generating an overall score ranging between 0 and 25 . 
the impotence status is assessed according to the following scale : severe = 07 ; moderate = 811 ; mild to moderate = 1216 ; mild = 1721 ; none = 2225 [ 13 ]  . ad interim analyses for late urinary toxicity were planned when the data of at least 161 patients with an 18 - month follow - up were available [ 12 ]  . 
at the time of the ad interim analysis for late urinary toxicity ( february 2015 ) , data regarding ed were also collected and considered , with an update being additionally performed in january 2016 . in total , 337 patients lled in the iief questionnaire before rt : 157 of 337 had a baseline iief1 - 5 score of > 11 and were considered to be potent before rt . among them , 91 patients received no hormonal therapy ; at the time of this ad interim analysis , 62 of 91 patients that lled in the 1 - year iief were considered . 
the caudal strahlenther onkol ( 2016 ) 192 : 297304 margin for ptv expansion varied in the range of 510 mm in 32 of 62 patients some overlap among the centres : between ptv and pb was evident . 
image guidance procedures also varied between centres : 30 , 22 and 10 patients in four , three and two institutes underwent daily megavoltage computed tomography ( mvct ) , daily cone - beam ct , and at least twice weekly electronic portal imaging device ( epid ) image guidance , respectively . 
at the time of this ad interim analysis , the mean ( dmean ) and maximum dose ( dmax , expressed as the dose received by 1 % of pb ) were available . contouring the penile bulb the referring radiation oncologist at each participating centre contoured the pb following written study guidelines [ 11 ]  . 
in short , well - known anatomic boundaries were considered ( the paired crura laterally , the corpus spongiosum anteriorly and the levator ani muscle posteriorly [ 14 ] ) ; moreover , because of the low contrast on ct images in the pelvic area , the anterior border of the pb was arbitrarily dened as the projection of the anterior border of the most caudal slice , where this border is more visible . 
an atlas was prepared and distributed to the participating centres that took part in a dummy run exercise [ 11 , 15 ]  . in the case of poor concordance , bad observers were instructed to correct their contouring procedure to better adhere to the guidelines [ 15 ]  . 
the results of the dummy run clearly showed that the impact of contouring uncertainty on pb dosevolume parameters is signicant but much lower than inter - patient variability , conrming the feasibility of multi - institute investigations [ 11 , 15 ]  . 
on the other hand , we clearly know that magnetic resonance imaging ( mri ) would be highly preferable for contouring the pb as well as other structures potentially involved in erections , such as the neurovascular bundles and internal pudendal arteries [ 7 , 10 , 14 , 16 , 17 ] : however , at the time of the activation of the study , the possibility to have a planning mri for all patients in all participating centres was not considered feasible and this is a limitation of the study . assessing predictors of 1 - year impotence the end - point of the current analysis was the prevalence of moderate / severe impotence dened as iief1 - 5 11 1 year after radiotherapy [ 13 ]  . prospectively collected individual data were available for all patients and included : baseline iief1 - 5 ( iief1 - 5_pre ) ; age ; body mass index ( bmi ) ; diabetes ; use of anti - hypertensive , anti - coagulants , anti - aggregants , anti - impotence drugs ; use of nasteride / dutasteride ; previous abdominal surgery ; smoking ( yes / no ) ; alcohol ( yes / no ) ; t stage ( t1 vs t2 ) , prostate - specic antigen ( psa ) score ; gleason score ( gps ) ; and pelvic node irradiation . 
as different fractionation schemes were allowed , the dmean and dmax to the pb were also corrected into 2 - gy equivalent doses using the linear - quadratic model and an / value of 3 gy and termed eqd2_mean / eqd2_max , respectively . 
variables with a p value of < 0.20 at uni - variate analysis were included in a backward logistic multi - variable model , retaining in the model variables with a p value of 0.05. 
roc curves were used to assess best cut - off values for iief1 - 5_pre , dmean / eqd2_mean and dmax / eqd2_max [ 18 ]  . the odds ratio ( or ) was reported to express the strength of association between each variable and 1 - year impotence . the discriminative power of the models was measured by the area under the roc curve ( auc )  . 
moderate hypofractionation was used in 42 of 62 patients ( 2.352.65 gy / fraction , 7074.2 gy ) while the remaining received 2 gy / fraction ( 7478 gy )  . 
all patients were treated with imrt with static or rotational techniques . at the 1 - year follow - up , 26 patients ( 42 % ) reported moderate / severe impotence , with similar rates for patients treated with hypoor conventional fractionation ( 40 % vs 45 % )  . 
of note , only six patients reported at baseline the use of anti - impotence drugs with iief1 - 5_pre ranging between 12 and 25 : three out of six had a 1 - year iief1 - 5 score of 11 . the results of the uni - variate analysis are shown in including the best cut - off values for tables 2 and 3 , dmax / eqd2_max and iief1 - 5_pre discriminating between potent and impotent patients . 
1 : in the same gure , the curve referring to the overall population ( regardless of eqd2_max ) is shown together with the true rates , grouping the patients according to the quartile values of iief1 - 5_pre . 
unfortunately , the unavailability of mri for all patients did not permit us to take these structures into account in the current study . on the other hand , a few studies reported some correlation between the dose received by the pb and 12 - year impotence [ 1923 ] , although other investigations did not conrm these results [ 2427 ]  . 
1 including baseline iief1 - 5 and eqd2_max ( vs < 74.2 gy ) predicting the 1 - year risk of impotence ( expressed as the predicted fraction of impotent patients )  . 
 [ 22 ] showed the dose received by at least 90 % of the pb ( d90 % ) to be correlated with the 2 - year risk of severe impotence in a cohort of 51 patients treated with 3dcrt at 6474 gy . 
unfortunately , multi - variable analysis including the baseline situation was not performed . our study , considering only the mean and maximum doses , clearly showed a strong correlation only for the maximum dose , suggesting the existence of a threshold effect . this result may be partly due to a doseeffect , which has also been reported in two large prospective trials [ 4 , 29 ] ; on the other hand , it also reasonably suggests that potency is much better preserved in those patients with no overlap between the pb and the ptv . this hypothesis found indirect conrmation from the very high rates of potency preservation reported by hoppe et al . 
the potential sparing of the pb by using mri to dene the prostatic apex has clearly been reported and quantied [ 30 ] and is likely to explain the ndings by hoppe and colleagues as compared with the worse rates of the other studies , including the current one , that used ct only to dene the prostate . very importantly , our study was the rst to assess the combined effect of the potency status before rt and of the maximum dose to the pb in predicting 1 - year moderate / severe impotence . on the other hand , this analysis has some limitations such as the relatively low number of patients and the current unavailability of the full dvh information . 
with respect to the rst point , it is worth noting that the number of patients in the current study is among the largest when considering prospective studies with patient - reported impotence assessment . 
we expect to have our nal 23 - year results from all 91 patients not before 12 years of commencing the study , when it should be possible to also analyse patients undergoing short - term androgen deprivation and therefore candidates for having total / partial recovery of erectile function . 
owing to the ndings of the ad interim analysis , we were encouraged to nalize a publication so as to avoid postponing this important result for the radiation oncology community . regarding the dvh information , recovering of dvh parameters together with dosesurface maps of the pb will be accomplished when the whole subpopulation of potent hormone - nave patients reaches the 1 - year follow - up . on the other hand , given the small dimension of the bulb , maximum and mean doses are quite robust dosimetry surrogates synthetically describing the dose received by this organ . another important issue concerns the fact that , although extremely accurate and informative , the patient - reported scoring of impotence does not capture all the functional and psychological aspects of radiation - induced ed , which may benet from other quantitative methods / measurements such as the stamp test or several diagnostic tests for physiological erectile capability including somatosensory evoked potentials , reex latency , electromyography , doppler ultrasound among others [ 31 , 32 ]  . 
in addition , the clear effect of baseline iief1 - 5 also indirectly reects the limits of the denition of a threshold for moderate / severe impotence using current patient - reported scores . conclusion in conclusion , our results clearly support the idea that sparing the pb may lead to a signicant increase of potency preservation rates after rt , especially in patients with no / mild impotency before irradiation . 
on the other hand , the impact of bulb sparing in patients with iief1 - 5 scores below 1517 seems to be questionable . the growing fraction of young patients and the possible reduction of the use of androgen deprivation consequent to the delivery of higher doses [ 33 ] may translate in the future into a signicant increase of fully potent patients who could benet greatly from the sparing of the pb . 
a full sparing of the pb may be expected when using mri to dene the prostate apex , as previously demonstrated [ 30 ] : our ndings provide further motivation for the implementation of mri - based planning for potent patients . acknowledgements the study was supported by the associazione italiana ricerca sul cancro ( airc - ig13090 )  . 
fiorino state that there are no conicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
eine betrchtliche heterogenitt der behandlungsprotokolle mit ihren unterschiedlichen endpunkten vorausgesetzt , verringerte die kst das risiko fr isolierte zns - rezidive in der gruppe von kindern , die schon bei diagnosestellung einen zns - befall aufwiesen . 
es wird darauf verwiesen , dass diese gruppe unabhngig davon , ob sie eine kst erhalten hatte , eine hhere rate an ereignissen whrend der gesamttherapie aufwies . originalpublikation vora a , adreano a , oui ch , hunger sp et al ( 2016 ) inuence of cranial radiotherapy on outcome in children with acute lymphoblastic leukemia treated with contemporary therapy . 
die autoren folgern , dass die kst das rezidivrisiko bei kindern mit all nicht reduziert , sofern eine behandlung mit modernen therapieprotokollen erfolgt ist . kommentar bei ungefhr 5 % aller kinder mit neu diagnostizierter all wird ein zns - befall diagnostiziert . 
die subgruppe mit einer t - zell - all trgt ein hheres risiko ( 1530 % ) fr einen zns - befall und kann im fall eines rezidivs unabhngig vom ursprnglichen vorliegen eines zns - befalls kaum noch geheilt werden [ 1 ]  . langzeitergebnisse der all - bfm - 90 - studie zeigen bei patienten 16 jahre nach therapieende eine kumulative inzidenz fr hirntumoren von 3 , 4 1 , 6 % , wenn diese eine prophylaktische kst von 12 gy erhalten hatten [ 2 ]  . 
eine prophylaktische schdelbestrahlung ist dort nur noch fr die kleine gruppe von kinder vorgesehen , die lter als 2 jahre ist , eine t - all hat und bei diagnose mehr als 100.000 leukozyten / l aufweist . 
eine therapeutische bestrahlung ist fr patienten mit offener zns - beteiligung ( cns 3 ) weiterhin vorgesehen . strahlenther onkol ( 2016 ) 192 : 352353 fazit literatur die vorliegende metaanalyse beleuchtet eindrcklich ein dilemma , ohne es wirklich aufzulsen . 
neuere randomisierte studien , welche die bedeutung der kst als bestandteil moderner therapieprotokolle prospektiv evaluieren knnten , werden aufgrund der kleinen verbleibenden fallzahlen und ethischer bedenken nicht mehr durchfhrbar sein [ 6 ]  . 
burger b , zimmermann m , mann g , kuhl j , loning l , riehm h et al ( 2003 ) diagnostic cerebrospinal uid examination in children with acute lymphoblastic leukemia : signicance of low leukocyte counts with blasts or traumatic lumbar puncture . 
schrappe m , moricke a , reiter a , henze g , welte k , gadner h et al ( 2013 ) key treatment questions in childhood acute lymphoblastic leukemia : results in 5 consecutive trials performed by the all - bfm study group from 1981 to 2000 . 
schmiegelow k , levinsen mf , attarbaschi a , baruchel a , devidas m , escherich g et al ( 2013 ) second malignant neoplasms after treatment of childhood acute lymphoblastic leukemia . 
moricke a , reiter a , zimmermann m , gadner h , stanulla m , dordelmann m et al ( 2008 ) risk - adjusted therapy of acute lymphoblastic leukemia can decrease treatment burden and improve survival : treatment results of 2169 unselected pediatric and adolescent patients enrolled in the trial all - bfm 95 . 
kelly mj , trikalinos ta , dahabreh ij , gianferante m , parsons sk ( 2014 ) cranial radiation for pediatric t - lineage acute lymphoblastic leukemia : a systematic review and meta - analysis . 
kelly mj , pauker sg , parsons sk ( 2015 ) using nonrandomized studies to inform complex clinical decisions : the thorny issue of cranial radiation therapy for t - cell acute lymphoblastic leukemia . pediatr blood cancer 62 ( 5 ) : 790797 strahlenther onkol ( 2016 ) 192 : 342348 doi 10.1007 / s00066 - 016 - 0950 - 7 radiation recall dermatitis induced by sorafenib a case study and review of the literature sonja stieb1 , 2 oliver riesterer1 cornelia brssow1 bernhard pestalozzi3 matthias guckenberger1 stefan weiler4 received : 29 october 2015 / accepted : 28 january 2016 / published online : 23 february 2016 springer - verlag berlin heidelberg 2016 abstract background radiation recall dermatitis ( rrd ) is an acute inflammatory reaction confined to previously irradiated skin , mainly subsequent to the administration of certain chemotherapeutics . 
here we present a rare case of rrd induced by the oral multikinase inhibitor sorafenib . case report a 77 - year - old male with hepatocellular carcinoma was irradiated at ten different sites for bone metastases with 2036 gray in 512 fractions from january to march 2015 . 
sorafenib was readministered after 3 weeks , which did not lead to recurrence of rrd but did cause fluctuating fever . discussion only four other such cases have been reported in the literature and who pharmacovigilance database on individual case safety reports . 
the current report is the first to show a potential relationship between the severity of sorafenib - induced rrd and radiation dose , histopathological features , and simultaneous acute radiation dermatitis and mucositis . conclusion rrd induced by sorafenib is a rare phenomenon , but should be considered in patients showing erythematous skin lesions 12 weeks after initiation of the drug , predominantly in areas where skin has been irradiated with an equivalent dose 30 gy . 
discontinuation of sorafenib with possible readministration should be evaluated with respect to the clinical situation and severity of reaction . keywords hepatocellular carcinoma radiotherapy chemotherapy toxicity erythema 1 department of radiation oncology , university hospital zurich , rmistrasse 100 , 8091 zurich , switzerland recall - strahlendermatitis durch sorafenib 2 center for proton therapy , paul scherrer institute , villigen psi , 5232 villigen , switzerland 3 department of oncology , university hospital zurich , rmistrasse 100 , 8091 zurich , switzerland 4 department of clinical pharmacology and toxicology , university hospital and university of zurich , rmistrasse 100 , 8091 zurich , switzerland eine fallstudie und literaturbersicht zusammenfassung hintergrund recall - strahlendermatitis ist eine akute entzndungsreaktion der haut in zuvor bestrahlten arealen , welche meist nach einnahme bestimmter chemo ( rrd ) case study1 3 therapeutika auftritt . 
nachfolgend prsentieren wir einen seltenen fall von rrd unter therapie mit dem multikinaseinhibitor sorafenib . fallbeschreibung ein 77 - jhriger , mnnlicher patient mit ossr metastasiertem hepatozellulrem karzinom wurde zwischen januar und mrz 2015 an insgesamt 10 verschiedenen lokalisationen mit 2036 gy in 512 fraktionen bestrahlt . 
eine erneute gabe von sorafenib nach insgesamt 3 - wchiger pause fhrte zu keiner neuerlichen hautreaktion , lste jedoch fluktuierendes fieber aus . diskussion weltweit wurden bislang nur vier weitere flle von rrd unter sorafenib berichtet . 
im vorliegenden fall werden erstmals ein potentieller zusammenhang des schweregrads der rrd unter sorafenib mit der bestrahlungsdosis der haut , die histopathologischen vernderungen sowie eine gleichzeitig vorliegende akute strahlendermatitis und mukositis dargestellt . schlussfolgerung durch sorafenib hervorgerufene rrd ist ein seltenes phnomen , das in den bestrahlten hautarealen , vornehmlich nach einer quivalentdosis von 30 gy , als erythematse hautreaktion 12 wochen nach therapiebeginn mit der substanz auftritt . 
eine therapiepause mit mglichem wiederbeginn von sorafenib sollte abhngig von der klinischen situation und dem schweregrad der reaktion evaluiert werden . schlsselwrter hepatozellulres karzinom strahlentherapie chemotherapie toxizitt erythem radiation recall dermatitis ( rrd ) is defined as an acute inflammatory reaction confined to previously irradiated skin after the administration of certain drugs , mostly classical chemotherapeutics , usually occurring months or even years after radiotherapy [ 1 ]  . sorafenib is an oral multikinase inhibitor and targeted anticancer substance . 
sorafenib is indicated for treatment of unresectable hepatocellular carcinoma ( hcc ) , advanced 133i - refractory thyroid carcinoma , or advanced pretreated renal cell carcinoma [ 2 ]  . 
the most common adverse effects of sorafenib are gastrointestinal , with abdominal pain , diarrhea , and nausea ; hepatic , with elevated levels of liver enzymes ; and dermatologic , with palmar - plantar erythrodysesthesia ( hand - foot reaction ) , alopecia , and rash [ 35 ]  . 
 a systematic review of published cases in the scientific literature and the who pharmacovigilance database was conducted to identify risk factors , signs , and course of this reaction , as well as outcome . case study a 77 - year - old male caucasian ( weight 67 kg ; height 160 cm ; body mass index , bmi 26 kg / m2 ) with hepatitis c - associated hcc ( diagnosed april 2014 ) received radiation to several metastatic bone sites between january and march 2015 . 
long - term comedication included amlodipine , metoprolol , hydrochlorothiazide for hypertension , tamsulosin for prostatic hyperplasia , oxycodone for pain , and esomeprazole for gastric ulcer prophylaxis . one week after initiation of sorafenib the patient presented with fever ( 38.2 c ) , rising c - reactive protein ( crp ; 23 mg / l ) , and a painless erythematous lesion at the right elbow where he had undergone surgery for pathologic fracture and received postoperative irradiation with 12 fractions of3 gy . 
blood pressure , heart rate , and oxygen saturation were unchanged compared to baseline values ( blood pressure 150 / 80 mmhg ; pulse rate 91 / min ; oxygen saturation , spo2 92 % )  . 
as per schedule , the dose of sorafenib was escalated to 400 mg twice daily and the erythema spread proximally into a distinct rectangular shape equivalent to the previous irradiation field during the following days . 
the severity of dermatitis showed a potential relationship with the administered radiation dose , because grade 2 skin toxicity predominantly occurred when the maximal skin dose was above 30 gy ( table 1 )  . 
 the skin reaction did not worsen , but the patient developed fluctuating fever , so sorafenib was eventually discontinued after another week . systematic review and discussion we present a case of increased skin toxicity and severe mucositis shortly after initiation of sorafenib , with worsening ard in areas currently under treatment ( acetabulum , sij , l1 , mandible ) , and rrd in previously irradiated areas ( scapula , humerus , t3 , t6 , t10 , 8th rib ; see table 1 )  . the radiosensitizing effect of sorafenib in combination with radiotherapy has been shown in different cell lines [ 7 11 ]  . 
reported on a patient receiving sorafenib and irradiation for lumbar metastasis of a renal cell carcinoma who died of severe bowel complications after radiotherapy [ 12 ]  . in contrast to other cutaneous complications of molecularly targeted therapies , such as hand - foot skin reaction , rrd induced by sorafenib is a rare phenomenon . 
similarly , no known reactions have been reported after treatment of gliomas [ 15 , 16 ] , pancreatic cancer [ 17 , 18 ] , or sarcoma [ 1921 ]  . we performed a systematic search for rrd induced by sorafenib in medline ( radiation recall dermatitis sorafenib ; recall sorafenib ) and the who global database vigibase on pharmacovigilance [ 22 ]  . 
described rrd in a patient with hcc after intensity - modulated radiotherapy ( imrt ) of the liver with 48 gy and start of sorafenib 300 mg twice daily 10 days after sbrt . 
a well - defined skin lesion on the right upper abdomen appeared 1 week after the start of sorafenib and resolved 10 days after stopping the drug and local therapy with clobetasol propionate [ 23 ]  . 
1 correlation of radiation recall dermatitis ( right humerus , left scapula , t10 ) and acute radiation dermatitis ( l1 ) with radiation fields database , only one other case of recall phenomenon and sorafenib was identified . 
other reported symptoms included vesicular rash , swelling , tenderness , and pa all reported patients with sorafenib - associated rrd were male , with a median age of 51 years and an average daily sorafenib dose of 575 mg ( range 300800 mg )  . 
symptoms started early after initiation of sorafenib , within 12 weeks . the leading symptoms in the reported cases include erythematous skin lesions localized to areas of previous radiation exposure , marked by disseminated exanthematous rash , pruritus , and parrd caused by other chemotherapeutics frequently occurred with an interval between radiotherapy and chemotherapy of less than 2 months [ 26 ]  . 
 in particular , lesions near to the body surface and those irradiated with 3d - conformal radiotherapy are associated with high skin doses and are therefore more prone to rrd . 
interestingly , the first occurrence of rrd in our patient was on the right upper arm , where he had received postoperative radiotherapy after osteosynthesis of a pathological humerus fracture . 
other authors have hypothesized that potential triggers might be impaired epithelial function induced by the radiation effect on epithelial stem cells , changes in vascularization , or dna repair [ 29 ]  . sorafenib is an inhibitor of multiple intracellular and cell surface kinases . 
generally , the pathogenetic process of rrd is controversialranging from an idiosyncratic hypersensitivity reaction , to a defect in dna repair and a direct toxic effect of the respective agent [ 31 ]  . 
our patient displayed enhanced mucosal toxicity in the oral cavity ( maximum biologically effective dose , bed 30 gy ; / = 8 ) and the urethra / bladder neck ( maximum bed 9 gy ; / = 8 ) with urinary retention in response to radiotherapy of the mandible and the pelvic region , which might be related to the radiosensitizing effect of sorafenib described above . including rrd is more commonly reported with conventional chemotherapeutic agents , the anthracycline doxorubicin , the taxanes docetaxel and paclitaxel , and the antimetabolites gemcitabine and capecitabine [ 1 ]  . 
however , rrd has also been described with other targeted cancer therapies in case reports or case series , such as for the braf inhibitor vemurafenib [ 33 , 34 ] , the egfr inhibitor erlotinib [ 35 ] , and the multitargeting tyrosine kinase inhibitor sunitinib [ 25 ]  . 
the bed ranged from 20 to 57 gy , the interval between irradiation and targeted therapy from 1 to 1584 weeks , and the time to onset of rrd after targeted therapy start from 1 day to 87 weeks [ 36 ]  . 
a clear correlation between the severity of rrd caused by sorafenib and the time interval between irradiation and the onset of symptoms ( range 3759 days ) could not be demonstrated on the basis of our data ( table 1 )  . 
the histopathological finding revealed a vacuolization of the dermoepidermal junction and apoptotic keratinocytes with sparse perivascular lymphocytic infiltrate and few eosinophils present case might be plausible , with fluctuating fever as a systemic reaction after rechallenge with sorafenib . 
however , fever as an unspecific symptom is reported with an incidence of about 10 % in patients treated with sorafenib . radiation recall reactions followed by sorafenib might not only be confined to skin reactions : cardiotoxicitiy has also been described [ 32 ]  . 
not available , rcc renal cell carcinoma , rrd radiation recall dermatitis , sbrt stereotactic radiotherapy strahlenther onkol ( 2016 ) 192 : 3423481 3 conclusion rrd induced by sorafenib is a rare phenomenon . 
diese prospektive , zweiarmige ecog - acrin - e5194 - kohortenstudie schloss von 1997 bis 2002 patientinnen ein mit alleinigem dcis nach brusterhaltender operation und freien absetzungsrndern von mindestens 3 mm bzw . 
in kohorte 1 konnten patientinnen mit gut oder mig differenzierten tumoren 2 , 5 cm eingebracht werden ( 561 frauen in der aktuellen auswertung ) , fr kohorte 2 war ein geringgradig differenziertes dcis mit einer tumorgre von bis zu 1 cm vorausgesetzt ( 104 frauen )  . 
die autoren empfehlen eine individuelle risikoabwgung fr den verzicht auf eine postoperative bestrahlungsbehandlung bei brusterhaltend operiertem dcis auf der basis der um diese studie erweiterten datengrundlage . originalpublikation solin lj , gray r , hughes ll et al ( 2015 ) surgical excision without radiation for ductal carcinoma in situ of the breast : 12 - year results from the ecog - acrin e5194 study . 
souchon berlin , deutschland die prospektive e5194 - kohortenstudie der cancer research group der eastern cooperative oncology group ( ecog ) und des american college of radiology imaging network ( acrin ) zielte auf patientinnen mit unter klinischen und pathomorphologischen aspekten vermeintlich gnstigem dcis unterschiedlicher differenzierungsgrade [ 1 ]  . 
magebliche grundlage fr die empfehlung zur rt sind die daten der metaanalyse der early breast cancer trialists collaborative trial group ( ebctcg ) : dort senkte die rt das lokalrezidivrisiko relativ um 54 % , absolut nach 10 jahren um 15 , 2 % [ 2 ]  . 
ein einuss der rt auf die brustkrebsspezische letalitt oder die berlebenswahrscheinlichkeit bestand nicht . durch die einfhrung des mammographie - screenings ist die diagnosestellung eines dcis angestiegen : es werden mehr tumoren in einem frhen stadium , d . 
da die brustkrebsspezische letalitt nach diagnose eines dcis aufgrund der biologischen und denitionsgemen nichtinvasivitt des dcis gering ist und die adjuvante rt und / oder auch eine tamoxifen - prophylaxe das berleben der betroffenen frauen nicht beeinusst , wird eine therapiedeeskalation beim dcis als mgliche weitere option diskutiert [ 3 ]  . beachtenswerterweise haben die 10 - jahres - lokalrezidivraten im zeitlichen verlauf abgenommen , laut einer publikation vom memorial sloan kettering - cancer center in new york von etwa 20 % im zeitraum 19781998 auf etwa 14 % im zeitraum 19992010 [ 4 ]  . 
allerdings beschrnkte sich diese reduktion nur auf die allein operierten patientinnen und betraf nicht diejenigen , die eine adjuvante rt erhalten hatten und unverndert weiterhin ein signikant geringeres lokalrezidivrisiko haben . 
wahrscheinlicher ist allerdings , dass eine zunehmende patientenselektion zugunsten einer alleinigen tumorexzision unter brusterhalt erfolgte und die rt die negativen prognosefaktoren kompensiert [ 5 ]  . ebenso wie in der e5194 - studie wurde auch von anderen forschungsgruppen versucht , dcis - patientinnen zu identizieren , die ein so geringes lokalrezidivrisiko haben , dass sie faktisch nicht von einer rt protieren . 
so hat beispielsweise die rtog9804 - studie nachgewiesen , dass klinische und histopathologische selektionskriterien zu unspezisch fr eine zuverlssige abschtzung sind , ob auch patientinnen mit vermeintlich gnstiger prognose von einer rt protieren . die rtog - 9804 - studie ist bislang die einzige studie , die randomisiert die effektivitt einer rt in einem denierten und entsprechend selektionierten niedrigrisikokollektiv untersucht hat . 
eindrucksvoll konnte gezeigt werden , dass auch hier ein deutlicher benet durch eine rt besteht : die lokalrezidivrate nach 7 jahren wurde durch von 6 , 7 % auf 0 , 9 % gesenkt [ 7 ]  . 
an dieser stelle sei auf zwei literaturkommentare in dieser zeitschrift verwiesen , welche die ergebnisse dieser studie ausfhrlich diskutieren [ 8 , 9 ]  . die e5194 - studie belegt nun , dass das rezidivrisiko sowohl fr ein dcis als auch fr ein invasives karzinom kontinuierlich ber einen zeitraum von 12 jahren in beiden kohorten ansteigt , ohne dass ein plateau erreicht wird . 
der auch in dieser studie dokumentierte fehlende nachweis einer plateauphase fr das auftreten von rezidiven kann die diskussion beleben , ob es sich bei den im langzeitverlauf beobachteten lokalrezidiven um echte rezidive handelt oder um zweitkarzinome [ 7 ]  . fazit der erkenntnisgewinn durch die 12 - jahres - daten der e5194 - studie ist gering . 
die studie besttigt im wesentlichen daten anderer prospektiver studien und die bisherigen therapieempfehlungen . auch fr vermeintliche niedrigrisikokollektive ist ein verzicht auf die adjuvante radiotherapie mit einem kontinuierlichen anstieg der lokalrezidive ohne erreichen eines plateaus verbunden . aktuell besteht fr das dcis weiterhin keine allgemein akzeptierte risikoklassikation , die einen verzicht auf die adjuvante radiotherapie erlauben wrde . 
im einzelfall muss mit der patientin weiterhin das postoperative vorgehen unter errterung ihres individuellen risikos eingehend besprochen werden . david krug , heidelberg und rainer souchon , berlin strahlenther onkol ( 2016 ) 192 : 349351 interessenkonikt d . 
solin lj , gray r , hughes ll et al ( 2015 ) surgical excision without radiation for ductal carcinoma in situ of the breast : 12 - year results from the ecog - acrin e5194 study . 
subhedar p , olcese c , patil s et al ( 2015 ) decreasing recurrence rates for ductal carcinoma in situ : analysis of 2996 women treated with breast - conserving surgery over 30 years . 
solin lj , gray r , baehner fl et al ( 2013 ) a multigene expression assay to predict local recurrence risk for ductal carcinoma in situ of the breast . 
mccormick b , winter k , hudis c et al ( 2015 ) rtog 9804 : a prospective randomized trial for good - risk ductal carcinoma in situ comparing radiotherapy with observation . 
for hsrt , the median prescribed dose was 35 gy in 5 fractions . results the 1 - year lc rate was 83.6 % in hsrt ; on multivariate analysis , a planning target volume ( ptv ) of < 4 cm3 , biologically effective dose ( bed10 ) of 51 gy , and adenocarcinoma were signicantly associated with better lc . 
furthermore , in bms 4 cm3 , a dose of bed 51 gy should be considered . keywords stereotactic radiotherapy , linac - based hypofractionated metastasis , brain lung cancer control , local prognosis hypofraktionierte stereotaktische strahlentherapie bei hirnmetastasen eines lungenkarzinoms evaluierung von indikationen und prdiktoren der lokalen kontrolle zusammenfassung ziel beurteilung von wirksamkeit und toxizitt einer hypofraktionierten stereotaktischen strahlentherapie ( hsrt ) zur behandlung von hirnmetastasen ( hm ) eines lungenkarzinoms und erforschung von mit der lokalen kontrolle ( lk ) und der indikation assoziierten prognosefaktoren . patienten und methoden analysiert wurden daten von patienten ( n = 53 ) , die sich einer linearbeschleuniger - basierten hsrt unterzogen ( mit hsrt behandelte lsionen n = 76 ; median der verordneten dosis : 35 gy in 5 fraktionen )  . analysiert wurden ferner bei den gleichen patienten im gleichen zeitraum mit stereotaktischer strahlenchirurgie ( srs ) behandelte lsionen ( n = 138 )  . 
die ergebnisse wurden in bezug auf lk oder toxizitt verglichen . strahlenther onkol ( 2016 ) 192 : 386393 ergebnisse nach einem jahr betrug die lk nach hsrt 83 , 6 % ; bei der multivariaten analyse zeigte sich , dass ein planning target volume ( ptv ) < 4 cm3 , eine biologisch effektive dosis ( bed10 ) 51 gy und ein adenokarzinom signikant mit einer besseren lk assoziiert waren . 
darber hinaus wurde bei einem ptv 4 cm3 ein signikanter unterschied in der lk zwischen bed10 < 51 gy und 51 gy beobachtet ( p = 0 , 024 )  . 
andererseits wurde bei einem ptv < 4 cm3 sowohl mit der hsrt als auch mit der srs eine gute lk erreicht , der unterschied war nicht signikant ( p = 0 , 195 )  . 
bei 5 der 76 ( 6 , 6 % ) mit hrst behandelten lsionen und bei 21 der 138 ( 15 , 2 % ) mit srs behandelten lsionen traten strahlennekrosen auf ( p = 0 , 064 )  . schlussfolgerung die linearbeschleuniger - basierte hsrt war eine sichere und effektive behandlung von hm eines lungenkarzinoms . 
signikante prognosefaktoren waren ptv , bed 10 und der histopathologische typ . bei hm mit einer ausdehnung 4 cm3 sollte eine bed 51 gy erwogen werden . schlsselwrter stereotaktische radiotherapie , linearbeschleuniger - basierte , hypofraktionierte intrazerebrale metastasen lungenkarzinom lokale kontrolle prognose introduction lung cancer often metastasizes to the brain ; approximately 50 % of brain metastases ( bms ) are reported to originate from lung cancers [ 1 ]  . 
reported that wbrt + srs for bms was superior to wbrt alone in terms of median survival time ( mst ) and local control ( lc ) [ 2 ]  . on the other hand , not all bms are recommended for srs . 
hsrt appears to be a safe and efcient option for lesions not amenable to srs ; it has comparable overall survival and progression - free survival with low treatment - related toxicity [ 4 , 5 ]  . 
although some reports have described the treatment results of hsrt , there has been no consensus on the recommended indication ( such as size and location ) , dose , or number of fractions [ 612 ]  . the purpose of this analysis was to evaluate the efcacy and toxicity of linear accelerator ( linac ) - based hsrt for bms from lung cancer , as well as to explore prognostic factors associated with lc and indication , in comparison with linac - based srs performed in the same patients during the same periods . patients and methods patients between may 2007 and may 2013 , 197 patients were treated with hsrt and / or srs at our institution . 
the inclusion criteria were : ( 1 ) patients with ve or fewer bms from lung cancer , and ( 2 ) patients who were administered hsrt or srs for bms as primary or salvage treatment for new lesions . 
the exclusion criteria were : ( 1 ) patients with resection before hsrt or srs , and ( 2 ) patients with a combination of wbrt and hsrt / srs as initial therapy for bm . 
the lesions treated with srs in the same patients and during the same period were analysed and compared with hsrt in terms of lc and toxicity ( mainly radiation necrosis [ rn ] )  . 
patients without these factors were generally treated with srs . the m3 micro - multileaf collimator ( mmlc ; brainlab ag , feldkirchen , germany ) and novalis - tx ( brainlab ag ) systems can both perform hsrt and srs on a caseby - case basis . 
of patients primary tumour lung cancer male / female 70 / < 70 status of primary tumour active / inactive extracranial metastasis yes / no pathology adenocarcinoma squamous cell carcinoma others chemotherapy ( post radiation ) yes / no target therapy ( before or after radiation ) yes / no rpa class i / ii / iii no . 
of lesions at the time of initial hsrt or srs 1 / 23 / 4 prior resection of brain lesion yes / no prior whole - brain irradiation to hsrt / srs 0 / 4 / 49 wbrt / pci / none 21 / 18 / 14 13 / 22 / 18 42 / 11 11 / 42 0 / 53 kps karnofsky performance status scale , rpa recursive partitioning analysis , hsrt hypofractionated stereotactic radiotherapy , srs stereotactic radiosurgery , wbrt whole - brain radiotherapy , pci prophylactic cranial irradiation radiotherapy hsrt and srs methods may 2007april 2010 the mmlc system was used as an add - on device on a non - dedicated linac ( clinac 21ex ; varian medical system , palo alto , calif . ) with 4 mv of photon energy . 
a purpose - built mask for m3 was prepared for hsrt and a brownrobertswells stereotactic base ring ( radionics , burlington , mass . ) was applied for srs . next , stereotactic contrast - enhanced computed tomography ( ct ) was performed with contiguous 1.25 - mm slices by plain radiography . 
t1 - weighted post - contrast magnetic resonance ( mr ) images were also acquired with 2.5 - mm slices and merged with the ct images to aid in determining the clinical target volume ( ctv )  . 
the ctv was expanded to the planning target volume ( ptv ) with a 12 - mm autoisotropic three - dimensional margin for hsrt and a 1 - mm tab . 
2 lesion and treatment characteristics characteristics hsrt ( n ) srs ( n ) median 0.7 cm3 ( range , 0.18.3 cm3 ) 134 / 4 0 / 138 median 6.2 cm3 ( range , 0.129.5 cm3 ) 27 / 49 18 / 58 total no . 
all hsrt was prescribed to the area covering the ptv - marginal area by the 8090 % dose line , and all srs was prescribed to cover the ptv - marginal area by the 80 % dose line . may 2010may 2013 the novalis - tx system was used with 6 - mv photon energy . 
the ctv was expanded to a ptv with a 1 - mm auto - isotropic three - dimensional margin , and the leaf - to - ptv margin was strahlenther onkol ( 2016 ) 192 : 386393 11c methionine positron emission tomography ct was performed when required . 
adverse events were scored using the national cancer institute common toxicity criteria version 4.0. statistical analysis the survival time and overall survival ( os ) were dened as the time from the beginning of initial hsrt or srs to the date of death or last follow - up visit . 
pearsons 2 test was used to compare the incidences of rn between hsrt and srs . results local tumour control of the 76 lesions treated with hsrt , 10 had local recurrence . 
srs was administered to the other lesion at 25 gy in 1 fraction at the isocentre because the tumour was small 11.4 mfive dynamic conformal arcs were used in all treatment plans . 
all hsrt was prescribed in such a way as to reach a goal of covering the ptv - marginal area by the 8090 % dose line , and all srs was performed under the same conditions as used with m3 . treatment follow - up the characteristics of the lesions and the corresponding hsrt / srs parameters are shown in tab . 
the prescribed dose was recalculated using the biologically effective dose ( bed ) , depending on the tumour location , since the dose was administered in 3 , 5 , or 13 fractions ( bed : / = 10 , with dose covering 95 % of ptv [ ptv d95 ] )  . all patients were evaluated with mr imaging in the rst month after the treatment , and every 2 months thereafter . rn was assessed using mr imaging or conrmed pathologically after surgical resection . 
the following criteria were considered for rn : ( 1 ) increased t1 - contrast enhancement observed in the irradiated area with central hypo - intensity and increased peripheral oedema ; ( 2 ) substantial regression or stability ( for at least 3 months ) of enhancing areas on serial follow - up mr imaging scan without additional treatment ; ( 3 ) a clear absence of perfusion within the contrastenhancing lesion on dynamic susceptibility contrast perfusion mr imaging . strahlenther onkol ( 2016 ) 192 : 386393 fig . 
b the local control rate of lesions treated with hypofractionated stereotactic radiotherapy ( hsrt ; n = 27 ) and stereotactic radiosurgery ( srs ; n = 134 ) in ptvs < 4 cm3 the mst of each class was : class i , 17 months ; class ii , 10.5 months ; and class iii , 4 months . 
reported a 1 - year lc rate of 68 % for 52 bms from various cancers in 27 patients treated with linac - based hsrt ( median 25 gy in 5 fractions ) [ 6 ]  . 
analysed 38 large bms from various cancers in 37 patients treated with hsrt ( median 35 gy in 35 fractions ) using cyberknife ( ck ) , and found the 1 - year lc rate to be 87 % [ 7 ]  . 
analysed 56 bms from various cancers in 44 patients treated with linac - based hsrt ( 24 to 30 gy in 3 to 5 fractions ) ; the 1 - year lc rate was 79.4 % [ 8 ]  . on the other hand , fewer studies investigated bms from lung cancer . 
in the report of matsuyama et al . , the lc was good because their prescribed dose ( median peripheral bed10 = 83.2 gy ) was higher than ours ( median ptv d95 bed10 = 53.6 gy ) , and their targeted tumour volume ( median 1.4 cm3 ) was smaller than ours was ( median 6.4 cm3 ) [ 10 ]  . second , it is important to identify prognostic factors associated with lc in hsrt . 
in this analysis , it was revealed that a ptv of < 4 cm3 , bed10 51 gy , and adenocarcinoma were statistically signicant factors that improved lc on multivariate analysis . 
thus , for ptvs 4 cm3 , higher doses might be required . recently , a good response has been reported in nonsmall - cell lung cancer patients with bms treated with tyrosine kinase inhibitors ( tkis ) [ 15 , 16 ]  . 
tki therapy was not a signicant prognostic factor in our analysis , although this may be due to inadequate statistical power . third , it is very important that hsrt is safer than srs because lesions for which hsrt is indicated are larger or strahlenther onkol ( 2016 ) 192 : 386393 tab . 
reported that the incidences of rn were not different between single - fraction gamma knife ( gk ) for small bms and fractionated ck for large bms [ 17 ]  . 
proposed that an eloquent area component such as the brainstem has a lower tolerance for irradiation , and late toxicities can be more problematic than in non - eloquent areas [ 18 ]  . 
not available , bed biological effective dose , fr fraction , gtv gross tumour volume , gy gray , hsrt hypofractionated stereotactic radiotherapy , ptv planning target volume , wbrt whole brain radiotherapy aon multivariate analysis gk or ck . 
reported that the irradiation plan for ck was superior to that of linac - srs in terms of coverage , minimal dose within target volume , conformity index , and volume of normal brain receiving 10 gy [ 27 ]  . 
since the majority of treatments in this analysis involved 35 gy in 5 fractions , we believe that this regimen produces good results if proper coverage of the target is achieved with correct dose distribution . 
however , prospective studies are required in a larger numbers of patients to better evaluate the efcacy , toxicity , proper prescribed dose , application range , and other factors . fr radioonkologie ( degro ) working group found that , although focal cerebral rn occurred in 210 % of cases , neuro - radiological changes such as progressive contrast enhancement on follow - up serial mr imaging could occur in up to 45 % of cases , with most occurring 1015 months after srs [ 19 ]  . 
although controversial , linac - based hsrt was safe in our analysis , and might therefore be particularly useful in or near an eloquent area . in cases using higher doses per faction , it is debatable whether the linear - quadratic ( lq ) model and bed can be dealt with in the same manner as conventional fractionation . fowler reported in 2009 that , if certain conditions were met , the lq model and bed were clinically applicable with hypofractionation [ 20 ]  . 
reported a systematic review of hsrt in bms using a modied lq - cubic model , which adjusted the lq model to account for a more linear response at higher doses by adding an additional term proportional to the cube of the dose [ 24 ]  . 
showed that the current lq model underestimates the cell toxicity in cases where the dose was 13 gy per fraction [ 25 ]  . there were some limitations in this analysis . 
first , it focused on bms treated with linac - based hsrt or srs . thus , our results are unlikely to be reproduced when using strahlenther onkol ( 2016 ) 192 : 386393 conclusion despite some limitations , this retrospective analysis showed that linac - based hsrt was effective and safe for treatment of bms from lung cancer . 
sasaki state that there are no conicts of interest . ethical standards the accompanying manuscript does not include studies on humans or animals . strahlenther onkol ( 2016 ) 192 : 368376 doi 10.1007 / s00066 - 016 - 0955 - 2 hfsrt of the resection cavity in patients with brain metastases hanno m . 
combs1 , 4 , 5 received : 4 august 2015 / accepted : 3 february 2016 / published online : 10 march 2016 springer - verlag berlin heidelberg 2016 abstract purpose aim of this single center , retrospective study was to assess the efficacy and safety of linear accelerator - based hypofractionated stereotactic radiotherapy ( hfsrt ) to the resection cavity of brain metastases after surgical resection . 
 local control ( lc ) , locoregional control ( lrc = new brain metastases outside of the treatment volume ) , overall survival ( os ) as well as acute and late toxicity were evaluated . patients and methods 46 patients with large ( > 3 cm ) or symptomatic brain metastases were treated with hfsrt . 
lc and lrc were assessed by follow - up magnetic resonance imaging . results the 1 - year lc rate was 88 % and lrc was 48 % ; 57% of all patients showed cranial progression after hfsrt ( 4% local , 44% locoregional , 9% local and locoregional )  . 
hfsrt was tolerated well without any severe acute side effects > grade 2 according to ctcae criteria . conclusion hfsrt after surgical resection of brain metastases was tolerated well without any severe acute side effects and led to excellent lc and a favorable os . 
 neben der lokalen kontrolle ( lc ) , der lokoregionren kontrolle ( lrc = neue hirnmetastasen auerhalb des behandlungsvolumens ) und dem gesamtberleben ( os ) wurden die akute und spte toxizitt analysiert . patienten und methoden 46 patienten wurden nach chirurgischer resektion von groen ( > 3 cm ) oder symptomatischen hirnmetastasen mit hfsrt behandelt . 
das mediane volumen der resektionshhle betrug 14 , 16 cm3 ( spanne original article1 3 1 , 4438 , 68 cm3 ) , das mediane planungszielvolumen ( ptv ) 26 , 19 cm3 ( spanne 3 , 4563 , 97 cm3 )  . 
 lc und lrc wurden mit hilfe von magnetresonanztomographie bewertet . ergebnisse nach einem jahr betrug die lc 88% und die lrc 48% ; 57% aller patienten entwickelten eine intrakranielle tumorprogression nach hfsrt ( 4% lokal , 44% lokoregionr , 9% lokal und lokoregionr )  . 
es traten keine hhergradigen akuten nebenwirkungen ( > grad 2 gem der ctcae - kriterien ) auf . schlussfolgerung hfsrt nach chirurgischer resektion von hirnmetastasen fhrt zu einer exzellenten lc und positivem os ohne hhergradige akute nebenwirkungen . 
 prospektive evaluationen im rahmen von klinischen studien werden derzeit durchgefhrt . schlsselwrter neoplasie , metastasierung radiochirurgie berleben hypofraktionierte stereotaktische strahlentherapie lebensqualitt introduction about 25 % of all patients with solid malignancies develop brain metastases during the course of their disease [ 1 ]  . 
the incidence of brain metastases is on the rise due to enhanced systemic therapies leading to longer overall survival ( os ) , and due to the growing use of mr imaging , which enables early detection of very small lesions . 
 only 10 % of the patients survive more than 1 year [ 3 ]  . surgery is a well - accepted treatment method for symptomatic singular or solitary brain metastases [ 4 ]  . 
it is also feasible for selected patients with two or three brain metastases , especially in cases when removal is possible within only one surgical session [ 5 ]  . 
only recently the eortc 2295226001 study [ 6 ] demonstrated a local recurrence rate of 60 % after 2 years with more than half of the patients suffering from tumor recurrence within the first year . whole brain radiotherapy ( wbrt ) can still be considered the standard treatment for brain metastases . 
in most current studies , wbrt following surgical resection or radiosurgery significantly increased the local control rate ( lc ) , referring to the rate of recurrence at the initial site as well as the locoregional control rate ( lrc ) , referring to new brain metastases distant from the initial site . 
in the eortc 2295226001 study mentioned above , the addition of wbrt reduced the local recurrence rate to 29 % after 2 years , while os was almost equal in both study arms ( 10.9 months with wbrt ; 10.7 months without wbrt )  . patients quality of life ( qol ) decreases mainly due to cognitive impairment caused by the irradiation of healthy brain tissue [ 12 ] , while local irradiation of the tumor bed might be a promising treatment alternative leading to significantly less neurocognitive impairment [ 8 ]  . 
also , for tumor entities , which are known to be radioresistant , higher single doses are more effective and therefore conventional wbrt does not lead to a favorable outcome [ 13 ]  . with increased treatment volume , the risk of late side effects such as radionecrosis also increases and the efficacy in terms of lc decreases . 
to date , only retrospective data is available , supporting the feasibility and efficacy of hfsrt [ 15 ]  . the present analysis reports on our data of hfsrt for patients with brain metastases evaluating treatment efficacy in terms of lc . 
furthermore , the feasibility and the outcome is assessed by evaluating lrc , os , and treatment - related acute and late toxicity . patients and methods between 2008 and 2014 , 46 patients with brain metastases were treated with hfsrt after surgical resection and were included into this analysis . 
surgical resection of the brain metastasis was performed due to the size ( > 3 cm ) or due to neurologic symptoms such as seizures , neurological motor deficits , gait or limb ataxia , or headache caused by intracranial pressure . patients characteristics are shown in table 1 . 
median age was 56 years ( range 1984 years ) and patients showed a good performance status ( median karnofsky index = 90 % , range 70100 % )  . 
63 % showed a complete resection on mri with no evidence of residual tumor tissue , while in 37 % of all patients remaining gadolinium ( gd ) enhancement in the contrast - enhanced t1 - weighted mri sequence was present suspicious of residual tumor . 
the median time interval between the planning mri and the first day of radiation was 4 days ( range 125 days )  . treatment planning was based on preand postsurgery ctas well as mr - imaging with and without contrast enhancement . 
we defined the clinical target volume ( ctv ) as the resection cavity and residual macroscopic tumor defined by postop contrast - enhanced mri ( t1 + gd ) plus a safety margin of 2 mm accounting for potential microscopic spread . 
a total dose of 35 gy was applied in 7 fractions ( 5 gy per fraction ) using a stereotactic treatment setup with a thermoplastic mask system ( brainlab , germany ) and daily image - guided radiotherapy ( igrt ) by robotic exactrac positioning ( brainlab , germany )  . the dose was prescribed to the 95100 % isodose line . 
if lesions were close to critical organs such as the brain stem or the optic nerve , imrt planning was performed using eclipse software ( varian , usa )  . six patients had an additional , asymptomatic brain metastasis at the time of treatment planning , which was not resected and thus required additional local treatment . 
these lesions were irradiated with stereotactic radiosurgery ( srs ) at a single dose of 20 gy ( prescribed to the 80 or 100 % isodose line ) using the identical stereotactic treatment setup . all patients were included in a strict follow - up regime and clinical data were collected prospectively within the in - house documentation database . 
2 example of a hfsrt treatment plan for a large resection cavity : cavity volume : 37.6cm3 , ptv : 44.6cm3 , dosing : 7x5gy ( 95% ) , 9 treatment beams ( 6 mev photons , non - coplanar )  . had regular follow - up visits including a thorough neurologic exam and mr imaging initially 6 weeks after treatment , every 3 months in the first 2 years , and thereafter once a year or as clinically needed . 
 besides lc and lrc , the systemic status of the disease as well as the overall performance score and treatment - related side effects were documented . the primary endpoint of the present analysis was lc . 
for the evaluation of lc and lrc , the time interval was calculated from the first day of radiation to the date of tumor recurrence in the follow - up imaging . 
for the evaluation of os , the time interval was calculated from the first day of radiation to the last time of contact ( during regular patient follow - up or by phone , if patients refused to show up for a regular visit )  . treatment - related toxicity was closely monitored during treatment and during regular follow - up . 
 if there was a progressive , contrast enhancing lesion and symptoms led to an impaired qol , surgical resection was performed after a consent statement has been obtained in an interdisciplinary tumor board . 
 all patients gave their written informed consent and agreed that their scientific data could be used for analyses . results median follow - up for all patients was 18 months ( range 280 months )  . 
3 kaplan - meier estimation of overall survival according to ( a ) recursive partitioning analysis ( rpa ) , ( b ) graded prognostic assessment ( gpa ) and ( c ) main tumor histologies ( breast cancer , non - smallcell lung cancer ( nsclc ) , gastrointestinal cancer ( gi - tract ) and malignant melanoma )  . strahlenther onkol ( 2016 ) 192 : 3683761 3 fig . 
4 kaplan - meier estimation of ( a ) local control according to resection cavity volume , ( b ) locoregional control according to the main tumor histologies ( breast cancer , non - small - cell lung cancer ( nsclc ) , gastrointestinal cancer ( gi - tract ) and malignant melanoma ) and ( c ) locoregional control according to resection cavity volume . eight patients ( 18 % ) were treated for further tumor recurrences after they had already received one salvage treatment as mentioned above . 
since most patients ( 65 % ) had already received wbrt , the treatment of choice was now mostly srs ( 75 % , 20 gy to the 80100 % surrounding isodose line ) and local hfsrt ( 25 % , 3035 in 56 fractions to the 95 % surrounding isodose line )  . three patients suffered from a further intracranial tumor recurrence and two patients received a third set of radiotherapy . 
an overview of recurrence patterns and time intervals to initial hfsrt and to last radiation treatment is provided in table 2 . a total of five patients underwent another surgical resection due to a progressive lesion in the initial treatment region . 
 the most common acute side effects were local alopecia ( 9 % ) and skin erythema ( 4 % )  . discussion there is an increasing desire to develop personalized approaches for the management of patients with brain metastases . 
but this can come at the price of neurocognitive impairment , especially when large doses per fraction , certain systemic treatments have been applied or when comorbidities are present [ 4 ]  . 
hfsrt to the resection cavity following surgical resection of brain metastases seems to be an effective approached based on an lc rate after 1 year of 88 % as shown in this analysis . 
 the applied dose of 35 gy in 7 fractions seems to be sufficient based on the good lc and based on the fact that no significant difference between small or large resection cavities and between complete resection and residual macroscopic tumor in the postoperative mri could be found . 
 [ 41 ] , where large resection cavities showed poorer lc with a rate of 54.5 % of local recurrence if the metastases were larger than 3 cm in diameter and deep seated . 
there certainly is an influence of further radiation or systemic treatment administered to the patients during the course of their disease , which might support the good local control rate shown by hfsrt . postoperative srs as a substitute for wbrt has been explored in several retrospective series , with 1 - year actuarial local control rates varying from 7886 % [ 9 , 1922 ]  . 
there is strong evidence in the literature that the target volume should not only compromise the resection cavity , but also a margin of at least 2 msoltys et al . 
but with increased volume of irradiated healthy brain tissue , the risk of unwanted side effects such as symptomatic necrosis increases [ 23 ]  . an important approach to optimize treatment and reduce the risk of brain necrosis is the use of a dedicated mri for treatment planning . 
still , often after resection of large metastases , the target volumes are too large for a one - shot approach ; hence , hfsrt can be considered as the safer treatment option compared to srs , as it was suggested by eaton et al . 
 strahlenther onkol ( 2016 ) 192 : 3683761 3 table 3 summarizes the experience gained with postoperative srs and hfsrt for brain metastases . an increasing number of patients with brain metastases will suffer from local progression after radiation treatment due to improved systemic therapies [ 27 ]  . 
 therefore , a risk of about 10 % for the occurrence of a radionecrosis was predicted based on the literature [ 28 ] and patients signed the informed consent willing to take that risk . 
the time interval between initial hfsrt and the development of radionecrosis was between 13 and 38 months , the time interval from radiation retreatment until the development of radionecrosis was within the expected range with 1126 months . depending on the underlying malignancy , the clinical course of the individual patient will differ quite considerably . 
while most patients with malignant melanoma suffered from new brain metastases at the time of first follow - up , the median time to tumor recurrence for lung cancer patients was more than 2 years . 
noteworthy , even though the median time to cerebral recurrence was shorter for breast cancer patients compared to lung cancer patients , their os was considerably longer which is probably due to more effective systemic therapies . to date , brain metastases are treated as a single tumor entity . 
however , there are some patients who develop only one or two metastases in the course of their disease that can be effectively treated by local therapy and then this leads to long timespans of brain metatstases - free survival . 
the size of the brain metastasis does not seem to be a prognostic factor , since lrc rates between patients with large or small metastases were similar . patients with brain metastases have limited survival ; hence , treatment options that offer minimal morbidity and maximal qol are essential . 
 since 57 % of all patients showed intracranial progression after local irradiation of the resection cavity during followup , regular patient follow - up must be warranted in order to initiate effective salvage treatments . 
neurocognitive impairment should be monitored in this trial , since it might be the major benefit of local hfsrt compared to wbrt . compliance with ethical standards conflict of interest h.m. 
combs state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
ldrt was well tolerated with only mild acute and late complications . conclusion primary radiotherapy of indolent orbital lymphomas is an effective treatment with high response rates and excellent local control in crt and ldrt . 
die ldrt wurde sehr gut vertragen und verursachte nur milde nebenwirkungen . schlussfolgerung eine primre und alleinige radiatio bei indolenten orbitalymphomen erwies sich als effektive therapiemethode mit hohen ansprechraten und ausgezeichneten lokalen kontrollraten , sowohl nach bestrahlung mit einer konventionellen dosis als auch nach einer radiotherapie mit 4 gy . 
da bei unzureichendem ansprechen nach ldrt eine re - bestrahlung sogar in voller konventioneller dosierung mglich ist , kann eine niedrigdosisbestrahlung mit 4 gy unter engmaschiger , bildmorphologischer nachsorge bei indolenten orbitalymphomen in erwgung gezogen werden . schlsselwrter niedrigdosisbestrahlung indolentes non - hodgkin lymphom orbitalymphom behandlungsergebnis lokal progressionsfreies berleben introduction lymprimary lymphoma of the ocular adnexa ( orbital phoma ) is a very rare tumor entity that accounts for less than 1 % of all non - hodgkin lymphomas ( nhl ) and 8 % of all extranodal nhl [ 1 , 2 ]  . 
with a proportion of 55 % of all orbital tumors , they are the most frequent malignant tumor of the eye and ocular adnexae [ 3 ]  . most common histology subtypes are low - grade ( indolent ) lymphoma entities like marginal zone or mucosa - associated lymphoid tissue ( malt ) lymphoma , follicular lymphoma ( fl ) , or lymphoplasmacytic lymphoma ( immunocytoma )  . 
g. , diffuse large b - cell lymphoma ( dlbcl ) or mantlecell lymphoma ( mcl ) , may also occur [ 4 , 5 ]  . these types of cancer typically originate from supercial tissues like conjunctiva , eyelids , or the lacrimal gland . patients with early conjunctival affection characteristically present with a localized plaque , which is described in the literature as salmon - pink . 
 [ 79 ] veried that bacterial eradication with antibiotic therapy was often followed by lymphoma regression . in contrast , primary intraocular lymphoma ( pol ) is a subset of primary central nervous system lymphoma with mainly high - grade histology subtypes like dlcbl [ 10 , 11 ] , associated with immune deciency , e . 
because of the different clinical features and prognosis , therapeutic management is fundamentally different . radiotherapy alone is the curative option in patients with indolent lymphoma revealing high response rates and manageable toxicity [ 13 , 14 ]  . 
radiation - related side effects were tolerable but with increasing severe complications ( grade 34 ) when more than 36 gy is administered [ 1719 ]  . the aim of this retrospective study was to review the response rates , toxicity , and relapse rates of conventional radiation doses in the treatment of patients with indolent orbital lymphomas in our institution . 
in addition , the efcacy and toxicity of a low - dose radiation treatment applied to patients with indolent orbital lymphomas were analyzed . patients and methods patient characteristics patient records of 70 patients ( 87 lesions ) with orbital lymphoma who were treated with radiotherapy from 19872014 at the department of radiation oncology at heidelberg university hospital were reviewed . 
inclusion criteria for this analysis were histologically proven low - grade ( indolent ) orbital lymphomas treated with radiotherapy alone ; high - grade lymphomas or intraocular localization were excluded for reasons explained above . a total of 52 patients with 60 lesions ( 3 synchronous bilateral , 2 metachronous bilateral , 3 relapses ) of indolent orbital nhl were treated with radiotherapy between 1987 and 2014 ( 35 left side , 25 right side )  . 
1 patient characteristics strahlenther onkol ( 2016 ) 192 : 414421 45 / 52 64 ( 2484 ) ldrt 75 ( 5979 ) 36 gy ( 2646 gy ) 4 gy total n ( % ) 52 / 60 19 ( 36.5 % ) 33 ( 63.5 % ) 27 ( 51.9 % ) 7 ( 13.5 % ) 5 ( 9.6 % ) 13 ( 25.0 % ) 43 ( 82.7 % ) 4 ( 7.7 % ) 2 ( 3.8 % ) 1 ( 1.9 % ) 2 ( 3.8 % ) 56 lesions , n ( % ) 6 ( 10.7 ) 5 ( 12.5 ) 2 ( 3.6 ) 19 ( 33.9 ) 15 ( 26.8 ) 4 ( 26.7 ) 4 ( 7.1 ) 5 ( 8.9 ) 9 ( 16.1 ) patients / lesions age : median ( range ) gender histological subtype stage ( ann arbor ) dose : median ( range ) male female malt immunocytoma indolent nhl , not further classied not classied initial symptoms1 diplopia conjunctivitis epiphora swelling exophthalmos foreign body sensation visual reduction pain ptosis 1multiple symptoms possible malt mucosa - associated lymphoid tissue , fl follicular lymphoma , nhl non - hodgkin lymphoma , crt conventional radiotherapy , ldrt low - dose radiotherapy tab . 
treatment was done using a linear accelerator : 24 lesions were treated with photons ( 6 mv ) , 25 lesions with electrons ( 720 mev ) , 2 lesions with combined electronphoton beams and one with cobalt . 
lesions treated in the earlier years were usually planned with an anterior photon or electron eld with a hanging block for lens shielding , whereas a ct - planned 3d conformal technique was applied in the latter years . in addition , we reviewed 7 patients with 8 lesions of orbital lymphomas who underwent low - dose radiotherapy ( ldrt )  . 
ct - based 3d conformal technique was applied in 2 lesions , while the other 6 lesions were treated with intensity - modulated helical tomotherapy . strahlenther onkol ( 2016 ) 192 : 414421 tab . 
3 response rates response not classied n ( % ) 35 / 46 ( 76.1 % ) 10 / 46 ( 21.7 % ) 1 / 46 ( 2.2 % ) ldrt n ( % ) after 2 months : 3 ( 37.5 % ) after 6 months : 8 ( 100 % ) after 2 months : 5 ( 62.5 % ) after 6 months : 0 crt conventional radiotherapy , ldrt low - dose radiotherapy , n number of lesions , cr complete response , pr partial response , sd stable disease , pd progressive disease ; out of 52 lesions receiving crt , 46 lesions had a documented response , 6 lesions were without documented response and therefore excluded in the analysis statistical analysis and follow - up patient records , planning documents and imaging scans , if present , were reviewed . 
local and distant progression - free survivals ( lpfs and dpfs , respectively ) were calculated in months from the beginning of radiotherapy until the diagnosis of recurrent disease of the orbit or elsewhere . os and dpfs were calculated for all patients ( 45 patients with crt and 8 patients with ldrt ) , whereas lpfs refers to the treated lesions ( 52 lesions after crt and 8 lesions after ldrt )  . 
only for one lesion ( 2.2 % ) was progressive disease ( pd ) after radiotherapy documented . one patient with initially bilateral manifestation was treated with radiotherapy of both eyes and had bilateral recurrence 38 months after crt , which was again treated with crt . 
low - dose radiotherapy was well tolerated with only mild acute and late complications such as xerophthalmia and quick symptom relief after irradiation . no grade 34 acute toxicity occurred . primary radiation therapy with conventional doses ( 2436 gy ) is the standard therapy for early stage indolent lymphomas of the orbit resulting in high response rates and discussion outstanding local control [ 15 , 16 , 2022 ]  . 
they showed high response rates of 96 % with a 2 - year freedom from local relapse of 100 % , comparable to our data that revealed a similar high response rate of 100 % and 2 - year lpfs of 100 % and no local relapse at the time of manuscript preparation ( longest follow - up : 41 months )  . 
however , both patients with a systemic relapse after ldrt suffered from higher stages of nhl , which may explain the difference . patients receiving ldrt should be closely followed and in the setting of modern and broadly available imaging techniques like mri scans ; another benet of ldrt also in a curative setting is the fact that further radiotherapy is still possible . however , the study has its limitations owing to the retrospective analysis and the limited follow - up data and low patient quantity on ldrt . 
moreover , a lack of documentation of response and the heterogeneity of radiation treatment techniques in earlier years of crt are negative aspects of this analysis . nevertheless , our data conrm that crt is a well - established technique with excellent response and control rates in the treatment of orbital lymphomas . 
in addition , we demonstrate that ldrt is effective andin combination with close follow - up examsan attractive option also in the curative settings with the possibility of re - irradiation . by inducing anti - inammatory effects like activating nf - b or tgfpathway [ 32 ] , as well as inuencing granulocyte / endothelial cell adhesion [ 33 , 34 ] , low - dose radiation is well integrated into the routine treatment of benign diseases . similar to anti - inammatory mechanisms , effectiveness in cancer - related diseases is only partly understood : local effects like overexpression of p53 - associated genes , induction of extrinsic and intrinsic apoptosis pathways , and up - regulation of immune reactions via macrophage activation - related genes are induced by ldrt [ 35 ]  . 
besides chemokine induction , activation of dendritic cells and th1 - related genes have been connected to ldrt , suggesting possible systemic ( abscopal ) effects [ 35 ]  . 
axial and coronal contrast - enhanced t1 - weighted mri scans a before radiotherapy and b 6 months after radiotherapy show complete response of a left - sided retrobulbar mucosa - associated lymphoid tissue ( malt ) lymphoma difcult to prove . 
furthermore , the evolution of radiation techniques ( 3d conformal radiotherapy and intensity - modulated radiotherapy ) has optimized current treatment and enables homogenous dose delivery and simultaneously precise sparing of organs at risk . since indolent lymphomas are highly radiosensitive , low - dose radiation has become increasingly used with promising results regarding local control rates with minimal toxicity . 
in the rst series , published by ganem et al . [ 25 ] , 27 patients with 57 sites of lymphoma affection were treated with 2 fractions of 2.0 gy in a palliative setting with a surprisingly high response rate of 89 % . 
several other publications showed comparable results in ldrt even in patients with early stage disease [ 2628 ]  . a randomized non - inferiority trial ( fort ) compared a conventional radiation scheme ( 24 gy ) to ldrt ( 4 gy ) in patients with fl [ 29 ]  . 
no differentiation in terms of size of affected regions or gradings of fl ( study included grade 3b ) and inconsistencies concerning the analysis itself are only some pitfalls the study reveals [ 30 ]  . 
4 radiotherapy - related acute and late side effects acute toxicity1 grade 12 grade 34 grade 12 late toxicity1 grade 34 conjunctivitis xerophthalmia photophobia periorbital edema dermatitis / hyperpigmentation epiphora other symptoms keratitis conjunctivitis xerophthalmia photophobia periorbital edema dermatitis / hyperpigmentation epiphora other symptoms corneal ulcer cataract strahlenther onkol ( 2016 ) 192 : 414421 n ( % ) 28 ( 59.6 % ) 14 ( 29.8 % ) 13 ( 27.7 % ) 13 ( 27.7 % ) 24 ( 78.7 % ) 10 ( 21.3 % ) 15 ( 31.9 % ) 1 ( 2.3 % ) 6 ( 14.0 % ) 17 ( 39.5 % ) 11 ( 25.6 % ) 1 ( 2.3 % ) 1 ( 2.3 % ) 9 ( 20.3 % ) 17 ( 39.5 % ) 1 ( 2.3 % ) 11 ( 25.6 % ) ldrt n ( % ) 2 ( 25.0 % ) 1 ( 12.5 % ) 1 ( 12.5 % ) n number of lesions of total 47 respectively 43 lesions ( acute toxicity respectively late toxicity ) in crt and 8 lesions in ldrt with documented side effects , crt conventional radiotherapy , ldrt low - dose radiotherapy , 1multiple symptoms possible conclusion our retrospective analysis shows that primary radiotherapy of indolent orbital lymphomas is a well - established treatment with high response rates and excellent local control in crt and ldrt . 
in combination with close follow - up and modern imaging techniques like mri , insufcient response or disease progression after ldrt can be detected in a timely manner and re - irradiation after ldrt even with full conventional doses is still feasible . 
ferry ja , fung cy , zukerberg l , lucarelli mj , hasserjian rp , preffer fi , harris nl ( 2007 ) lymphoma of the ocular adnexa : a study of 353 cases . 
fung cy , tarbell nj , lucarelli mj , goldberg si , linggood rm , harris nl , ferry ja ( 2003 ) ocular adnexal lymphoma : clinical behavior of distinct world health organization classication subtypes . 
ferreri aj , ponzoni m , guidoboni m , de conciliis c , resti ag , mazzi b , lettini aa , demeter j , delloro s , doglioni c , villa e , boiocchi m , dolcetti r ( 2005 ) regression of ocular adnexal lymphoma after chlamydia psittaci - eradicating antibiotic therapy . j clin oncol 23 ( 22 ) : 50675073 . 
ferreri aj , guidoboni m , ponzoni m , de conciliis c , delloro s , fleischhauer k , caggiari l , lettini aa , dal cin e , ieri r , freschi m , villa e , boiocchi m , dolcetti r ( 2004 ) evidence for an association between chlamydia psittaci and ocular adnexal lymphomas . j natl cancer inst 96 ( 8 ) : 586594 10 . 
cassoux n , merle - beral h , leblond v , bodaghi b , milea d , gerber s , fardeau c , reux i , xuan kh , chan cc , lehoang p ( 2000 ) ocular and central nervous system lymphoma : clinical features and diagnosis . 
curr opin oncol 13 ( 3 ) : 137142 strahlenther onkol ( 2016 ) 192 : 359367 doi 10.1007 / s00066 - 016 - 0956 - 1 symptomatic radiation - induced cardiac disease in long - term survivors of esophageal cancer ichiro ogino1 shigenobu watanabe1 noriaki iwahashi2 masami kosuge2 kentaro sakamaki3 chikara kunisaki4 kazuo kimura2 received : 31 august 2015 / accepted : 3 february 2016 / published online : 16 february 2016 springer - verlag berlin heidelberg 2016 abstract purpose to evaluate clinical and dosimetric factors retrospectively affecting the risk of symptomatic cardiac disease ( scd ) in esophageal cancer patients treated with radiotherapy . patients and methods a total of 343 patients with newly diagnosed esophageal cancer were managed with concurrent chemoradiotherapy or radiotherapy alone . 
the heart diseases included three pericardial effusions , one pericardial effusion with valvular disease and paroxysmal atrial tachycardia , three atrial fibrillations , one sinus tachycardia , one coronary artery disease , one chest pain with strongly suspected coronary artery disease , and one congestive heart failure . 
for v45 , v50 , and v55 , the lowest significant cutoff values were 15 , 10 , and 5 % , respectively . conclusion high - dose and large - volume irradiation of the heart increased the risk of scd in long - term survivors . 
using modern radiotherapy techniques , it is important to minimize the heart dosevolume parameters without reducing the tumor dose . keywords toxicity chemoradiotherapy hodgkins disease radiotherapy risk factors symptomatische strahleninduzierte herzerkrankung bei langzeitberlebenden nach sophaguskarzinom zusammenfassung ziel beurteilung von klinischen und dosimetrischen faktoren , die mit risiken eines retrospektiven auftretens von symptomatischen herzerkrankungen ( scd ) bei patienten zusammenhngen , die aufgrund eines sophaguskarzinoms strahlentherapeutisch behandelt wurden . patienten und methoden insgesamt 343 patienten mit neu diagnostiziertem sophaguskarzinom wurden mit kombinierter chemound strahlentherapie oder nur strahlentherapeutisch behandelt . 
uniund multivariate analysen mit den stetigen variablen ergaben , dass das risiko fr eine scd vom volumen des herzens abhngt , das dosen von mehr als 45 gy ( v45 ) , v50 und v55 erhielt . 
bei v45 , v50 und v55 betrug der niedrigste signifikante toleranzwert jeweils 15 , 10 und 5% . schlussfolgerung hochdosierte , grovolumige bestrahlungen des herzens wirkten sich auf das scd - risiko bei langzeitberlebenden aus . 
dosis - volumen - parameter fr das herz mssen mit modernen strahlentherapiemethoden verringert werden , ohne die tumordosis zu reduzieren . schlsselwrter toxizitt strahlenchemotherapie hodgkin - erkrankung strahlentherapie risikofaktoren the effect of radiation therapy on the heart has been well discussed for breast cancer and hodgkins disease . 
radiation dosage [ 13 ] , volume of the heart involved in the radiation field [ 46 ] , and fraction size [ 7 ] were identified as risk factors for cardiac toxicities . 
long - term survivors of hodgkins lymphoma have increased risks for cardiac mortality after delivered total tumor doses of 3040 gy , where large volumes of the heart were included in the field . 
breast doses are generally 4050 gy , but only a small part of the heart is included in the treatment fields , and mean heart doses rarely exceed 1015 gy . 
the relative risks of cardiac mortality are consequently lower than for hodgkins lymphoma survivors [ 8 ]  . for patients with distal esophageal cancer , the dose delivered to the heart is 50 gy or more [ 9 ]  . 
the irradiated volume of the heart in esophageal cancer patients is larger than for breast cancer . the eastern cooperative oncology group study compared a radiation therapy alone arm to those in an arm who received concurrent chemoradiotherapy ( ccrt ) , with 2and 5 - year survival rates of 12 and 7 % in the radiation alone arm and 27 and 9 % in the ccrt arm , respectively [ 10 ]  . 
there are few reports available and late complications of the heart are not well understood in long - term survivors with esophageal cancer treated by radiotherapy . we retrospectively analyzed long - term survivors with esophageal cancer who were followed at our hospital for 4 years , in order to investigate the risk factors for radiation - induced symptomatic cardiac disease ( scd )  . methods patients between january 2000 and june 2011 , 343 patients with newly diagnosed esophageal cancer were managed with ccrt or radiation alone without surgery . 
the study was carried out with the approval of the institutional review board , in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
this resulted in a median clinical follow - up for the remaining 58 patients of 79 months ( range 48127 months ) , with an interquartile range of 6096 months . 
the boost ptv2 was defined as the ctv2 ( gtv with 2 - cm superiorinferior and 0.5 - cm radial margins ) plus 01 c involved nodes with 0.5 - cm margins were also included in ctv2 . 
an additional dose was delivered to ptv2 using oblique off - cord beams . combined cisplatin and 5 - flourouracil ( 5 - fu ) was the most common regimen for patients with ccrt ( continuous infusion of 500 mg / m2 / day 5 - fu and 5 mg / m2 / day cisplatin administered on days 15 , 812 , 1519 , and 2226 ) [ 12 ]  . 
any evidence of cardiac symptoms after radiotherapy , history of heart disease , and risk factors for the development of cardiac disease , such as diabetes mellitus , total cholesterol , hypertension , and smoking habits , was recorded for each patient [ 13 ]  . cardiologists evaluated all patients with cardiac symptoms . 
the cardiac status of symptomatic patients was reviewed using electrocardiography by a single cardiologist ( mk ) and echocardiography by a single cardiologist ( ni ) with comparison of the data before and after radiotherapy . 
 the time of onset of cardiac toxicity was defined as the interval between radiotherapy and the clinical presentation with cardiac symptoms . dosimetric analysis a planning computed tomography ( ct ) scan was obtained using a ct scanner with 5 - mm slice thickness before june 2009 and 2.5 - mm slice thickness after june 2009 . 
forty - one ( 71 % ) patients were heavy smokers , with their brinkman index ( cigarettes per day multiplied by years of smoking ) before radiotherapy ranging from 48 to 2220 . 
there were 53 ( 91 % ) patients with squamous cell carcinoma , 3 ( 5 % ) with adenocarcinoma , and 2 ( 3 % ) with small cell carcinoma . 
the median total dose delivered to the central tumor was 60 gy ( range 4068 gy )  . symptomatic patients the clinical data and results for the 11 patients with scd ( grade 2 or more ) are shown in table 3 . 
scd included thress pericardial effusions , one pericardial effusion with valvular disease and paroxysmal atrial tachycardia , three atrial fibrillations , one sinus tachycardia , one coronary artery disease , one cardiac chest pain with strongly suspected coronary artery disease , and one congestive heart failure . 
risk factors for the development of cardiac disease were not associated with the incidence of scd . as the dosimetric parameters were highly correlated with each other , multivariate analysis included the dosimetric factors significant in univariate analysis analyzed separately . 
in multivariate analysis , v45 , v50 , and v55 significantly affected the incidence of scd compared with gender ( table 4 )  . recursive partition analysis recursive partition analysis was used to derive hypotheses for the dose and volume parameters strongly affecting the incidence of scd . 
a dose range of 3065 gy in increments of 5 gy , and the percent volume from heart dvhs were analyzed in the range of 585 % in increments of 5 % . 
these different clinical manifestations have different latency periods which range from months to decades . acute pericarditis during radiotherapy is uncommon and pericarditis and pericardial effusion were reported to occur 142 months after radiotherapy [ 6 , 1618 ]  . 
 the incidence of symptomatic radiation - induced pericarditis was 6.9 % in our study , which is similar to the results of the latter study . coronary artery diseases were reported to occur 28179 months after radiation therapy [ 1 , 16 , 17 ]  . 
these authors found actual incidences of coronary artery disease of 3 % at 5 years , 6 % at 10 years , and 10 % at 20 years [ 4 ]  . 
reported that standardized mortality ratios decreased sharply with an older age at the initial treatment of hodgkins disease , but absolute excess risks of death strahlenther onkol ( 2016 ) 192 : 3593671 3 364 fig . 
1 cumulative incidence of symptomatic cardiac disease for a all patents , b v45 cutoff values of 15 % , c v50 cutoff values of 10 % , and d v50 cutoff values of 5 % . 
found actual incidences of clinically important valvular dysfunction of 1 % at 10 years , 4 % at 15 years , and 6 % at 20 years in 415 patients with hodgkins disease . 
4.0 g2 60 ( 1.82 ) scd symptomatic cardiac disease , ctcae v.4.0 common terminology criteria for adverse events version 4.0 , rtog / eortc radiation therapy oncology group / european organization for research and treatment of cancer , nci - ctc v.2.0 national cancer institute - common toxicity criteria version 2.0 , rt radiotherapy , pe pericardial effusion , op operation , g grade 18 ( 12.9 % ) not available 79 ( 48127 ) 62 ( 3875 ) 68 ( 4886 ) 53 ( 1486 ) 37 ( 770 ) there are a few reports regarding atrial fibrillation occurring after radiation therapy to the mediastinugayed et al . 
in the present study , 3 ( 5.2 % ) patients suffered atrial fibrillation 3170 months after radiotherapy . congestive heart failure - related death was reported by hancock et al . 
congestive heart failure death was the second most common cause of cardiac disease death , arising in 24 ( 1.1 % ) of 2232 patients , after 55 ( 2.4 % ) cases of acute myocardial infarction [ 3 ]  . 
 reported on radiotherapy using photon beams to either side of the internal mammary chain for breast cancer , which was associated with increased congestive heart failure compared with no radiotherapy . 
these authors stated that many cardiac events may be missed by restricting the study outcome to coronary artery disease only and not considering congestive heart failure [ 22 ]  . 
although our follow - up was 4 years or more , and this follow - up period may be too short to analyze the morbidity or mortality due to coronary artery disease and valvular disease ; other radiation - induced cardiac diseases increased with a longer follow - up . there are a few articles reporting on the correlation between the dosevolume parameters of the heart and scd . 
a total of 76 of the latter patients ( 74.5 % ) underwent esophagectomy 46 weeks after completion of ccrt [ 5 ]  . intensity - modulated radiotherapy ( imrt ) plans reduced unnecessary radiation to the heart compared with threedimensional conformal radiotherapy ( 3dcrt ) plans in esophageal cancer . 
 although they found that the rate of cardiac - related deaths was significantly lower after imrt than after 3dcrt , and that there were no differences in the cumulative incidence of cancer - specific deaths , the authors did not propose a dose volume parameter for the heart [ 26 ]  . 
despite the known associations of radiation with long - term cardiac toxicities , there is neither a consensus statement nor are there specific recommendations on a dosevolume parameter for the heart . in int 0123 , a higher radiation dose ( 64.8 gy ) did not increase survival or local / regional control , and it was concluded that the standard radiation dose for patients treated with concurrent 5 - fu and cisplatin chemotherapy is 50.4 gy [ 9 ]  . 
a significantly higher strahlenther onkol ( 2016 ) 192 : 3593671 3 366 incidence of scd was seen in association with an increasing percentage of the volume in v45 , v50 , and v55 . 
the implications of these results on dose reduction to the heart and identifying whether a tumor dose above 50.4 gy can improve survival of patients treated with ccrt for esophageal cancer will require future long - term studies . conclusion we generated hypotheses for future testing of v45 , v50 , and v55 of the heart being below 15 , 10 , and 5 % to reduce scd . 
all multiple beams have recently been applied simultaneously during each treatment fraction , whereas most of our patients were treated with initial anteriorposterior beams followed by oblique off - cord beams . 
it is necessary to minimize the dosevolume parameter of the heart without reducing the tumor dose using modern radiotherapy techniques for esophageal cancer patients . compliance with ethical standards conflict of interest i . 
kimura state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 403413 doi 10.1007 / s00066 - 016 - 0958 - z iterative metal artifact reduction improves dose calculation accuracy phantom study with dental implants manuel maerz1 pia mittermair1 andreas krauss2 oliver koelbl1 barbara dobler1 received : 17 july 2015 / accepted : 3 february 2016 / published online : 11 march 2016 springer - verlag berlin heidelberg 2016 abstract purpose metallic dental implants cause severe streaking artifacts in computed tomography ( ct ) data , which affect the accuracy of dose calculations in radiation therapy . 
the aim of this study was to investigate the benefit of the metal artifact reduction algorithm iterative metal artifact reduction ( imar ) in terms of correct representation of hounsfield units ( hu ) and dose calculation accuracy . materials and methods heterogeneous phantoms consisting of different types of tissue equivalent material surrounding metallic dental implants were designed . 
intensity - modulated radiation therapy ( imrt ) and volumetric modulated arc therapy ( vmat ) plans were calculated in oncentra v4.3 on corrected and uncorrected ct data and compared to gafchromic ebt3 films to assess accuracy of dose calculation . results the use of imar increased the accuracy of hu reproduction . 
in dieser studie soll der nutzen des iterativen metall - artefakt - reduktions - algorithmus imar hinsichtlich der wiedergabetreue von hounsfield - werten ( hu ) und der genauigkeit von dosisberechnungen untersucht werden . material und methoden es wurden heterogene phantome aus verschiedenen arten gewebequivalenten materials mit zahnimplantaten entworfen . 
die mittlere akzeptanzrate der gammaevaluation mit 3 % dosistoleranz und 3 mm ortstoleranz steigt von 90 , 6 auf 96 , 2% , wenn artefakte mittels imar korrigiert werden . schlussfolgerung mit hilfe von imar konnten die artefakte zu groen teilen entfernt werden , was zu einer signifikanten erhhung der dosisberechnungsgenauigkeit fhrt . schlsselwrter metallartefaktreduktion metallartefakte mar zahnimplantate dosisberechnung gafchromic strahlentherapie introduction modern treatment planning is based on computed tomography ( ct ) data . 
the electron density information contained in the hounsfield units ( hu ) of the ct data is required for accurate dose calculation ; however , metallic dental implants lead to streaking artifacts on ct data which impede the delineation of tumors and organs at risk . 
in addition , due to a limited value range of standard ct , the density values of metallic implants are not represented correctly in ct data [ 1 ]  . several studies have investigated the use of metal artifact reduction algorithms to improve dose calculation in radiation therapy [ 19 ]  . 
if dose measurements are performed for the verification of calculations , the measurements are based on simple beam geometries only instead of realistic plans [ 2 , 5 ] or evaluated for small regions only [ 4 , 5 ]  . 
 [ 1 ] investigated the influence of metal artifacts on dose calculation accuracy of intensitymodulated radiotherapy ( imrt ) and volumetric modulated arc therapy ( vmat ) plans by 2d film measurements in homogeneous phantoms with realistic dental implants . 
it could be shown that metal artifacts lead to a significant reduction in dose calculation accuracy and that vmat leads to more accurate results than imrt . the study presented here follows on from the publication of maerz et al [ 1 ] , investigating the benefit of the iterative metal artifact reduction algorithm ( imar ; siemens healthcare gmbh , forchheim , germany ) on dose calculation accuracy . 
the result of the dose calculations was compared to two - dimensional ( 2d ) dosimetry using gafchromic ebt3 ( ashland inc . , covington , ky , usa ) films to assess the accuracy of the calculations and thus the benefit of the artifact reduction . 
the effect of metal itself and artifacts were evaluated separately . materials and methods phantoms the study is conducted on a cylindrical phantom with a diameter of 18 cm consisting of water equivalent material ( high density polyethylene , hdpe ) and a set of cylindrical inserts that can be placed in the phantothe phantom includes a holding brace of polyether ether ketone with 30 % = 1 4 . 
the geometric arrangement of the implants is intended to repstrahlenther onkol ( 2016 ) 192 : 4034131 3 resent teeth implants generating many artifacts and fewer artifacts , respectively . the phantom in its different configurations can be equipped with radiochromic films for dose measurements which serve as reference dose distributions . 
1 in the configuration with eight teeth implants and muscle equivalent material in the center . ct scans were acquired for all phantoms using a somatom sensation open ct scanner ( siemens healthcare gmbh , forchheim , germany ) using the rt head preset and a slice thickness of 1.5 martifact - containing ct scans were corrected using the imar algorithm ( siemens healthcare gmbh , forchheim , germany )  . 
the synthetic ct data were generated in matlabtm r2013b ( the mathworks inc . , natick , ma , usa ) using the knowledge of the geometric setup of the phantothe used hounsfield units were acquired by ct scans of the materials using the same presets . 
1 phantom for dose measurements and calculations in the configuration with eight symmetric implants and muscle equivalent insert in the center of the phantom : a phantom in preparation without and b with radiochromic film ; c complete phantom mar algorithm the imar algorithm combines two previously introduced mar algorithms , normalized metal artifact reduction ( nmar [ 14 ] ) and frequency - split metal artifact reduction ( fsmar [ 15 ] )  . 
the aim of fsmar is to preserve both the natural image impression and the valid edge information of the uncorrected image , which is often affected by pure sinogram inpainting methods , especially in the vicinity of the metal implants . 
 this effectively reduces the remaining artifacts of the prior image and consequently improves the quality of nmar in each iteration [ 10 , 11 ]  . treatment planning and dose calculation a planning target volume and organs at risk were delineated on the ct scan of each phantom as they are typical for hypopharyngeal carcinoma including parotid glands , brain stem , spinal canal , and spinal cord . 
for each phantom three treatment plans were optimized in oncentra external beam v4.3 ( nucletron , an elekta company , veenendaal , the netherlands ) as described in [ 1618 ] : imrt with 5 equispaced beams , imrt with 9 equispaced beams , and a dual arc vmat . 
all calculations were compared to measurements using gafchromic ebt3 films for validation . for dose calculation oncentra external beam assigns hounsfield units to material properties of standard tissues as defined in icrp23 [ 19 ] and icru 44 [ 20 ]  . 
the implemented pencil beam algorithm calculates dose to water whereas the collapsed cone algorithm calculates dose to media . to exclude the influence of transmission and scattering by metal implants on dose calculation , the plans were recalculated on ct datasets in which regions with metal inserts were set to the mass density of water , but the artifacts were retained . 
dose calculations were compared to dose measurements in phantoms without metal implants . as a reference on accuracy of calculations in heterogeneous phantoms without artifacts , plans were also recalculated on reference ct data and compared to the corresponding film measurements . 
for calculations without an influence of metal , ct scans of the phantoms without dental implants were used . dose measurements the phantoms were positioned with a spatial uncertainty of less than 1 mm , equipped with radiochromic films gafchromic ebt3 and irradiated with the corresponding plans . 
film measurements were accomplished as previously described [ 1 ]  . as the calibration is performed in water equivalent material and the films are approximately water equivalent [ 21 ] , dose distributions are measured as dose to water and subsequently converted to dose to medium for comparison to collapsed cone calculations . 
since no reference values are available for the tissue equivalent material used in the phantoms , empirical factors were determined by comparing measured and calculated dose profiles of single open fields in tissue equivalent material . 
 [ 22 ] was used . evaluation to assess the ct images with respect to accuracy of hounsfield units , corrected and uncorrected ct data were registered with synthetic ct data . 
therefore , the fraction of pixels differing less than 60 hu , between 60 hu and 500 hu and more than 500 hu of the synthetic ct data was evaluated as an additional measure . 
accuracy of hounsfield unit reproduction was evaluated separately for tissue regions excluding dental implants and dental implants with a 3 mm margin . dose calculation accuracy was determined in the software omnipro imrt ( iba dosimetry , schwarzenbruck , germany ) by comparing dose calculations and film measurements using the gamma method [ 23 ]  . 
the measured dose distributions were aligned to the corresponding calculations on uncorrected ct data and compared to the corresponding calculations on uncorrected , corrected , and reference ct datasets without being repositioned . 
gamma parameters were chosen according to aapm tg119 [ 24 ] to be delta dose d = 3 % and distance to agreement dta = 3 m passing rates of gafchromic ebt3 film measurements of imrt plans in homogenous phantoms found by other investigators are 97.2 % [ 25 ] and 99 % [ 26 ]  . 
in addition , difference values were determined between calculations on uncorrected and corrected ct data , respectively , and calculations on reference ct data and evaluated on cold and hot areas within the planning target volume . results reproduction of hounsfield units figure 2 shows uncorrected and corrected ct data of the phantoms with muscle insert . 
 in the corrected data , the artifacts are removed to a large extent and the circular shape of the insert can be detected . the evaluation of correct hounsfield unit representation is illustrated in fig . 
for phantoms including dental implants a substantial improvement in hounsfield unit reproduction could be observed due to imar correction of the data . dose calculation accuracy figure 4 shows the gamma evaluation of the dual arc vmat plan on the phantom including the insert of muscle equivalent material and eight metal implants . 
in the top images , the influence of both the metal and the artifacts are considered , while in the bottom images metal was removed from the ct data and replaced by the hu of water for dose calculation . 
2 uncorrected ( left ) and imar - corrected ( right ) ct data of the phantom with muscle equivalent insert and five and eight implants , respectively ; the streaking artifacts are removed to a great extent in the corrected data on the right hand side ; the structure of the central insert can be identified after correction table 1 evaluation of reproduction of hounsfield units ( hu ) for uncorrected and imar - corrected ct data no metal metal region tissue tissue metal mean difference [ hu ] hu 60 60 < hu 500 hu > 500 uncorrected corrected uncorrected corrected 1006 95 % 27 % 92 % 20 % 55 % 54 % 20 % 27 % 19 % 60 % 18 % phantoms without metal implants ( first row ) as reference ; for phantoms including metal implants the evaluation is separated for tissue areas and regions of metal implants including a 3 mm margin for uncorrected and corrected ct data ; for evaluation the mean absolute difference between ct data and reference data is calculated and the fraction of pixels differing less than 60 hu , between 60 hu and 500 hu and more than 500 hu of the reference ct data is determined for all collapsed cone and pencil beam calculations on uncorrected , corrected , and reference ct data . 
a detailed evaluation of improvement in accuracy depending on treatment techniques , tissue inserts , geometry of the implants , and dose calculation algorithms is displayed in table 2 . for all insert materials a significant increase of the passing rates can be detected if artifact reduction is applied . 
3 evaluation of correct hounsfield unit reproduction of uncorrected and imar - corrected ct data of the phantom with five implants and muscle equivalent insert : a evaluation of tissue regions , b evaluation of metal regions including a margin of 3 mm surrounding the metal ; in both images on top : spectral representation of absolute difference with reference images , bottom : corresponding histograms ; the red bars highlight the limit of 60 hu difference the passing rates of all calculations on reference ct data to all calculations on corrected ct data showed no relevant differences . 
only in one case , i.e. , the phantom with air insert , are calculations on synthetic ct data substantially more accurate than on corrected ct data ( p = 1.8 % , p = 0.040 , no metal ; p = 2.1 % , p = 0.027 , including metal )  . for asymmetric and symmetric implants a significant increase in passing rates can be observed that is higher for symmetric implants . 
no significant difference in passing rates could be detected between pencil beam calculations on corrected and reference ct data . comparing the passing rates of pencil beam and collapsed cone calculations on uncorrected ct data shows a higher agreement for pencil beam calculations . 
in calculations on uncorrected ct data , some cold and hot regions compared to calculations on reference ct data can be observed . in table 3 , the amount of voxels with dose differences within certain ranges in the planning target volume , constrained to ct slices containing artifacts , is evaluated for all calculations compared to the corresponding calculations on reference ct data . 
negative numbers mean that calculated dose on uncorrected / corrected ct data is lower than calculations on reference ct data strahlenther onkol ( 2016 ) 192 : 4034131 3 % discussion 98.5 % of the voxels differ less than 3 % if calculations on corrected ct data are compared to calculations on reference ct data . 
if calculations on corrected ct data are compared to calculations on reference ct data , this amount is reduced to 10.2 % several studies have previously shown an influence of metal artifacts and metal artifact reduction techniques on dose calculations . 
this study demonstrates a substantial reduction of the artifacts by the imar algorith in tissue regions of corrected ct data , deviations from synthetic ct data tend to be close to the value of the phantoms without metal . 
we found that if metal is taken into account , the accuracy of calculations on corrected data of the phantom with 8 symmetric implants is higher than of the phantom with 5 asymmetric implants . 
therefore , it will be of interest for future research if this effect can be reduced using a more accurate handling of the metal properties in other treatment planning systems . the comparison of pencil beam and collapsed cone calculations showed that especially collapsed cone calculations benefit from the use of an artifact reduction . 
the collapsed cone algorithm is known to account for tissue heterogeneities in dose calculations more precisely than pencil beam ; therefore , collapsed cone considers artificial structures more than pencil bea moreover , collapsed cone in oncentra strahlenther onkol ( 2016 ) 192 : 4034131 3 412 calculates dose as dose to mediuartifacts of low and high hounsfield units are converted to structures of low and high density . 
therefore , dose is calculated as if it was deposited in high or low density material , but is in reality deposited in materials of density close to water . dose difference calculations using the reference ct data show that cold and hot areas exist in calculations on uncorrected ct data with differences between 20 % and 10 % compared to calculations on reference ct data . 
this results in hot regions within the planning target volume compared to plans optimized on reference ct data . conclusion metal artifacts in ct scans of the phantoms were largely corrected by the imar algoriththis led to a significant increase in dose calculation accuracy . 
therefore , the use of imar is highly recommended for artifact - containing ct data . metal implants were found to impact negatively on dose calculation accuracy even when artifacts were removed . 
if no artifact reduction is available , the use of pencil beam instead of collapsed cone should be considered based on the better agreement between dose measurements and pencil beam calculations on uncorrected ct data , provided that there are no other reasons like huge amounts of lung or bone and only small artifact regions to the contrary . acknowledgments the work was supported by the wilhelm sander foundation . 
this study compared concurrent chemoradiotherapy plus ac ( ccrt / ac ) with ccrt . methods pair - matched analysis based on eight clinicopathological features of 244 patients treated with platinumbased ccrt / ac or ccrt alone was performed . 
in dieser studie wurde die simultane radiochemotherapie ( concurrent chemoradiotherapy , ccrt ) plus adjuvante chemotherapie ( ac ) mit einer alleinigen ccrt verglichen . patienten und methoden die matched - pair - analyse basiert auf acht klinisch - pathologischen merkmalen von 244 pastrahlenther onkol ( 2016 ) 192 : 394402 tienten , die mit platinbasierter ccrt / ac oder alleiniger ccrt behandelt wurden . 
toxische reaktionen und ansprechraten wurden mit dem exakten fisher - test verglichen . ergebnisse das vier - jahres - gesamtberleben , das progressionsfreie berleben , das fernmetastasenfreie berleben ohne therapieversagen und das lokoregionale berleben ohne therapieversagen betrugen jeweils 72 % , 61 % , 71 % bzw . 
die hugsten unerwnschten ereignisse vom grad 34 im ccrt / ac - arm waren erbrechen ( 27 % ) , belkeit ( 43 % ) , leukopenie / neutropenie ( 23 % ) , thrombozytopenie ( 8 , 8 % ) und anmie ( 6 , 2 % )  . schlussfolgerung eine zustzliche ac zur ccrt erhhte die toxischen reaktionen , fhrte jedoch zu keiner verbesserung des berlebens bei lokal fortgeschrittenem npc . schlsselwrter berleben nebenwirkungen toxizitt strahlenonkologie china approximately 70 % of patients with newly diagnosed nasopharyngeal carcinoma ( npc ) present with locoregionally advanced stage - iii or ivab disease , which have higher rates of local recurrence and distant metastasis , and signicantly poorer overall survival than early - stage disease [ 1 , 2 ]  . 
reduction of local recurrence and distant metastasis in locoregionally advanced npc is an active research topic [ 3 ]  . as an important approach that aims to reduce recurrence and metastasis , adjuvant chemotherapy ( ac ) has been widely used in an attempt to improve outcomes in a range of tumor types , including colon and breast cancer [ 4 , 5 ]  . 
combined analysis of the npc - 9901 and npc - 9902 trials by the hong kong nasopharyngeal cancer study group [ 7 ] suggested additional ac containing uorouracil ( fu ) improved distant control . 
for instance , in the randomized controlled trial by ma et al . , concurrent chemoradiotherapy ( ccrt ) plus ac ( ccrt / ac ) resulted in a similar outcome to ccrt [ 8 ]  . 
kwong and colleagues evaluated the efcacy of ac for npc using a factorial study , and found that addition of ac to ccrt did not improve overall survival , failure - free survival , or distant failure - free survival [ 9 ]  . 
furthermore , the use of ac in npc varies greatly between different countries and institutions . in order to reassess the therapeutic effects of ac for locoregionally advanced npc in regions of china where npc is endemic , a matched - pair analysis was performed , following strict matching criteria to compare the outcomes of platinum - based ccrt / ac with those of ccrt alone . patients and methods patient eligibility eligible patients treated between january 2008 and december 2010 at four radiation oncology institutions in guangxi , china , were included . 
inclusion criteria were : eastern cooperative oncology group ( ecog ) performance status of 0 or 1 ; normal renal function ( serum creatinine 1.5 mg / dl , creatinine clearance 60 ml / min ) ; normal hepatic function ( serum total bilirubin 1.6 mg / dl , serum transaminase < 2.5times higher than upper limit ) ; normal complete blood count ( hemoglobin > 10 g / dl , white blood cells 4000 / l , platelets 100 , 000 / l ) ; absence of severe cardiac disease , such as coronary artery disease or congestive heart failure ; and no previous radiotherapy and / or chemotherapy . the study protocol was approved by the institutional ethics committees of the four participating institutions . 
overall survival ( os ) , progression - free survival ( pfs ) , distant failure396 strahlenther onkol ( 2016 ) 192 : 394402 free survival ( dffs ) , and locoregional failure - free survival ( lrffs ) were compared between the two arms . baseline assessments patients in both arms provided full medical histories and underwent initial assessments including a physical examination , chest computed tomography ( ct ) , liver ultrasound , electrocardiogram , and a dental examination . 
all patients underwent nasopharyngeal ber optic endoscopy and biopsy , as well as magnetic resonance imaging ( mri ) or intensive ct of the nasopharynx and neck at baseline ; metastatic workup included chest and abdominal ct scans , and bone emission ct scans in patients with bone pain . treatment radiotherapy all patients underwent 2drt or 3dcrt delivered by a linear accelerator with 6 - megavolt ( mv ) photon energy . 
all doses were given at 2 gy per fraction ( ve fractions per week )  . concurrent chemotherapy all patients received platinum - based doublet chemotherapy . during radiotherapy , 27 mg / m2 / d of cisplatin was administered concomitantly on days 13 plus 800 mg / m2 / d fu on days 15 or 135 mg / m2 paclitaxel on day 1 every 4 weeks , for three cycles [ 11 ]  . 
antiemetic drugs were administered as required . adjuvant chemotherapy one month after the completion of ccrt , the ccrt / ac arm received 27 mg / m2 / d cisplatin on day 13 plus 800 mg / m2 / d fu on days 15 or 135 mg / m2 paclitaxel on days 1 every three weeks , for three cycles . response and toxicity evaluation during treatment , full blood counts , biochemistry , and toxicity assessments were performed weekly , and acute chemotherapy - related toxicities were assessed using the national cancer institute common terminology criteria for adverse events ( ctcae ) version 3.0. 
acute and late radiotherapy - related toxicities were graded using the radiation morbidity scoring criteria of the radiation therapy oncology group . after ccrt , mri or ct scans of the nasopharynx and neck were performed and treatment response was assessed using the response evaluation criteria in solid tumors ( recist ) [ 12 ]  . 
acute toxicities were dened as occurring from the initiation of treatment to 90 days after completion ; late toxicities occurred or persisted beyond 90 days from commencement of radiotherapy . follow - up after discharge from hospital , patients were assessed every 3 months for 2 years , and every 6 months in years 3 and 4 . all local recurrences were diagnosed by endoscopic biopsy or mri / intensive ct of the nasopharynx and skull base . regional neck recurrences were diagnosed by clinical examination and mri / ct ; unclear cases were conrmed by ne - needle aspiration . 
os was calculated from initiation of treatment to death due to any cause or last follow - up ; pfs to rst observation of disease progression ( local recurrence and / or distant metastasis ) or death from any cause ; distant metastasis to the date distant metastasis was rst detected ; and local control to locoregional progression . 
response rates ( including complete response , partial response , stable disease , and progressive disease ) were assessed at the third month after completion of treatment . to determine the appropriate study sample size , a 10 % difference in pfs between the two arms of the study was considered clinical efcacy [ 8 ]  . 
the median follow - up was the length of follow - up for the middle patient in the patient list sorted by follow - up duration ( or average of the middle two ) [ 13 ]  . 
independent prognostic factors were determined using multivariate cox regression analysis with the backward stepwise method . cox proportional hazards models stratied by gender , age , who pathological type , t category , n category , and treatment arm were used to estimate hazard ratios ( hrs )  . 
at the end of the matching process , a total of 244 patients who received platinum - based ccrt as controls were pairmatched with 244 patients who received platinum - based ccrt / ac . 
in total , 437 / 488 patients ( 90 % ) had undifferentiated non - keratinizing npc and 51 / 488 ( 10 % ) had differentiated non - keratinizing npc . 
overall , 191 / 244 patients ( 78 % ) in the ccrt arm and 186 / 244 ( 76 % ) in the ccrt / ac arm had a treatment delay related to toxic effects . in the ccrt / ac arm , ac was initiated 1 month after the completion of radiotherapy ; a median of 2 cycles were administered ( range 14 )  . 
overall , 201 / 244 patients ( 82 % ) suffered treatment delays due to ac - related adverse events . response and survival outcomes responses after completion of treatment were assessed at the third month after completion of treatment for all 488 patients . 
1 kaplanmeier survival curves for patients with locoregionally advanced nasopharyngeal carcinoma in the ccrt / ac and ccrt arms . a overall survival ; b progression - free survival ; c distant failure - free survival ; d locoregional failure - free survival . 
ccrt concurrent chemoradiotherapy , ac adjuvant chemotherapy , hr hazard ratio , ci condence interval cisplatin - based ac to ccrt in terms of 4 - year os , pfs , dffs , or lrffs in patients with locoregionally advanced npc from the endemic area of china . in agreement , ma et al . [ 8 ] reported that ccrt plus cisplatin - based ac did not signicantly improve os , pfs , dffs , and lrffs in stage - iii or iv ( except t34n0 ) npc compared to ccrt alone in chinese patients . 
 [ 18 ] demonstrated that radiotherapy plus ac increased toxicities but had no effect on os , pfs , drfs , or lrfs in patients with locoregionally advanced npc from hong kong . 
variables were selected using the backward stepwise approach ccrt concurrent chemoradiotherapy , ac adjuvant chemotherapy , ci condence interval , hr hazard ratio , tnm tumor - node - metastasis * indicates a statistically signicant p - value lowed by ac ( cisplatin and 5 - fu ) failed to improve os or relapse - free survival in patients with advanced npc from taiwan . 
demonstrated that six cycles of ac did not show any survival benet compared to patients with locoregionally advanced npc who did not receive any ac [ 20 ]  . in the present study , subgroup analysis did not show signicant survival benets for adjuvant schedules based on cisplatin and 5 - fu or paclitaxel in n2n3 disease . 
these negative results are also in concordance with a bayesian network meta - analysis of eight studies involving 2144 patients , which indicated no signicant improvements in os , lrffs , or dffs following ccrt / ac compared with ccrt alone [ 21 ]  . 
recently , interesting observations have been reported by the updated meta - analysis of chemotherapy in nasopharynx carcinoma ( mac - npc ) meta - analysis ; addition of ac to radiotherapy did not signicantly improve os ( hr 0.87 , 95 % ci 0.681.12 ) or pfs ( hr 0.80 , 95 % ci 0.641.00 ) , and the specic benets of ac after ccrt needed further investigation [ 22 ]  . local recurrence and distant metastasis after radiotherapy are the main causes of death in locoregionally advanced npc . 
in theory , patients with advanced - stage npc should receive a relatively large benet from ac after ccrt comit is reasonable to hypothpared to early - stage patients . esize that adjuvant therapy would improve the control of micrometastatic disease , which is more likely in advancedstage npc , while chemoradiotherapy provides local control . 
our ndings are in line with other studies [ 8 , 1822 ] that failed to demonstrate any signicant value for ac in locoregionally advanced npc ; however , the reasons why ac provides no survival advantage have not yet been well strahlenther onkol ( 2016 ) 192 : 394402 tab . 
despite the fact that the patient population was relatively t , with a median age of only 47 years , 70 % of patients in this study experienced grade 3 or 4 toxicities , which is similar to the studies by ma et al . 
furthermore , patient tolerance to chemotherapy after radiotherapy was usually very poor ; compliance was 47 % for three or more cycles , 39 % for two cycles , and 14 % for one cycle of ac ; these rates are lower than in other studies ( 5563 % ) [ 6 , 8 , 17 ]  . 
however , existing data appear to indicate that over half of patients who receive ccrt cannot complete an adjuvant schedule due to the high frequency of toxicities , which makes radiologists in the endemic region reluctant to employ ac in clinical practice . 
most patients received 2drt , which not only showed poorer quality - of - life ( qol ) outcomes , such as a high level of xerostomia [ 28 ] or hearing impairment [ 29 ] , but also presented a lower local control rate and shorter os and dfs compared with intensity - modulated radiotherapy ( imrt ) [ 30 ] despite these limitations , we were able to demonstrate that ac does not provide a signicant survival benet in locoregionally advanced npc . conclusion in summary , the addition of ac to ccrt increases toxicity but does not signicantly improve survival in patients with locoregionally advanced npc from the endemic area . therefore , we do not recommend the use of ac in this setting . 
jiang state that there are no conicts of interest . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 377385 doi 10.1007 / s00066 - 016 - 0959 - y imrt vs . 
2d - radiotherapy or 3d - conformal radiotherapy of nasopharyngeal carcinoma survival outcome in a korean multi - institutional retrospective study ( krog 11 - 06 ) sung ho moon1 kwan ho cho1 chang - geol lee2 ki chang keum2 yeon - sil kim3 hong - gyun wu4 jin ho kim4 yong chan ahn5 dongryul oh5 jong hoon lee6 received : 1 november 2015 / accepted : 10 february 2016 / published online : 14 march 2016 springer - verlag berlin heidelberg 2016 abstract objective we compared treatment outcomes of two - dimensional radiotherapy ( 2d - rt ) , three - dimensional conformal radiotherapy ( 3d - crt ) , and intensity - modulated radiotherapy ( imrt ) in patients with nasopharyngeal carcinoma ( npc )  . patients and methods in total , 1237 patients with ct14n0 - 3m0 npc were retrospectively analyzed . 
in multivariate analyses of all patients , imrt was a predictive factor for os when compared with 2d - rt or 3d - crt , as was 3d - crt when compared with 2d - rt . conclusion our study showed that 3d - crt and imrt were associated with a better local progression - free survival and os than was 2d - rt in npc . 
in multivariater analyse von allen patienten war die imrt ein prdiktiver faktor fr das os im vergleich mit 2d - rt oder 3d - crt , hingegen 3d - crt verglichen mit 2d - rt . schlussfolgerung unsere studie zeigte , dass 3d - crt und imrt mit dem lokalen progressionsfreien berleben und os besser verbunden sind als 2d - rt in npc . 
imrt war erheblich berlegen in bezug auf das os fr fortgeschrittene primre tumoren ( t34 )  . schlsselwrter nasopharyngeale neoplasien strahlentherapie intensittsmodulierte strahlentherapie patients and methods study population this was a multi - institutional retrospective analysis of the korean radiation oncology group ( krog ) 11 - 06 study . 
the inclusion criteria were histologically confirmed npc , ct1 - 4n0 - 3m0 disease according to the uicc / ajcc staging classification , and no history of malignancy for 5 years except basal cell or squamous cell carcinoma of the skpatients who underwent incomplete rt of < 90 % of the planned schedule and had inadequate information regarding recurrence and patients who died during rt were excluded . 
 the study was performed in accordance with the guidelines of the institutional review board of each participating hospital . introduction rt techniques nasopharyngeal carcinoma ( npc ) is a disease with high radiosensitivity , but administration of radiation to patients with npc is challenging due to the proximity of the primary tumor to critical organs and structures related with quality of life and function . 
concurrent chemotherapy combined with radiotherapy ( rt ) , especially in locoregionally advanced disease , has dramatically improved clinical outcomes of npc [ 18 ] , with a 6.3absolute benefit of 5 - year overall survival ( os ) in a recently updated meta - analysis [ 9 ]  . meanwhile , the application of intensity - modulated rt ( imrt ) has resulted in the current improvements in treatment outcomes of npc . 
the advantages of imrt in terms of treatment efficacy and its ability to spare the parotid gland have been repeatedly demonstrated [ 1012 ] , and its use in npc has prevailed over conventional two - dimensional rt ( 2d - rt ) or three - dimensional conformal rt ( 3dcrt )  . 
however , results showing the benefits of imrt over 2d - rt or 3d - crt in terms of treatment efficacy are still limited , and most results have come from areas where npc is endemic [ 1316 ]  . as the incidence rate of npc in korea is < 1.5 / 105 [ 17 ] , which is relatively lower than that of southern china where it is endemic with an incidence rate of 20 to 50 / 105 [ 18 ] , a nationwide multi - institutional retrospective study was conducted to compare the treatment outcomes of 2d - rt , 3d - crt , and imrt . all patients were treated with a megavoltage beam linear accelerator . 
in this study , the 2d - rt technique comprised planning with the use of a conventional technique on a simulator and treatment with a 24 initial field with the appropriate beam energy and field shaping . 
for 3d - crt , computed tomography ( ct ) - based planning was performed using a treatment - planning system . the clinical target volume ( ctv ) was defined by the primary tumor and lymph nodes suspected to be malignant either clinically or radiologically , the entire nasopharynx and nearby anatomical structures such as the parapharyngeal space or retropharyngeal spaces , and the bilateral neck lymphatics of internal jugular chain and spinal accessory cha high - risk ctv ( ctv1 ) , intermediate - risk ctv ( ctv2 ) , and low - risk ctv ( ctv3 ) were defined as the gross tumor volume plus an appropriate margin , subclinical disease , and elective nodal area , respectively . 
the field arrangement for 2d - rt or 3d - crt could adopt a conventional rt technique of initial opposed lateral fields to encompass the primary tumor and upper cervical lymph nodes with an adequate margin , matched to low neck field ( s )  . 
next , the organs at risk , including the brain stem , spinal cord , parotid glands , eyeballs , optic nerves , optic chiasm , and inner ear , were contoured in the planning stage for 3d - crt . 
regarding dose specification for 2d - rt , a daily dose was prescribed to the mid - depth point along the central axis for parallel - opposed fields whether initial or final cone down . 
for low neck field ( s ) , the same daily dose as in parallel - opposed fields was usually prescribed to a reference point selected on the central axis . 
for 3d - crt , planning target volume ( ptv ) should be covered by at least 95 % isodose line of prescribed dose ( pd ) and the maximum dose within the ptv was maintained less than 110 % of pd as possible . for 3d - crt and imrt , the planning target volume was defined as the ctv plus a 3to 10 - mm ( median , 5 - mm ) margin after contouring the gross tumor volume and ctv . 
the periods during which each rt technique was used were 19882009 ( mid : 1998 ) for 2d - rt , 19942009 ( mid : 2005 ) for 3d - crt , and 2002 2011 ( mid : 2008 ) for imrt . combined chemotherapy a total of 29 % of patients received neoadjuvant chemotherapy . 
concurrent chemotherapy was used in 64 % of patients and the regimen most commonly used were as follows : ( 1 ) 3040 mg / m2 of cisplatin , weekly , for a maximum of eight cycles , beginning on the first day of radiotherapy ; ( 2 ) 100 mg / m2 of cisplatin , every 3 weeks , for 3 cycles , on days 1 , 22 , and 43 in concurrence with radiotherapy ; and ( 3 ) 80 mg / m2 of cisplatin plus 400 mg / m2 of fluorouracil ( 96 - h continuous infusion ) , monthly , for 2 cycles , on days 1 and 29 in concurrence with radiotherapy . 
three cycles of adjuvant chemotherapy consisting of cisplatin ( 80 mg / m2 / day ) and fluorouracil ( 1000 mg / m2 / day by 96 - h infusion ) followed in 28 % of patients . endpoints and statistical analyses the endpoints of this study were overall survival ( os ) , progression - free survival ( pfs ) , local pfs ( lpfs ) , regional pfs ( rpfs ) , and distant metastasis - free survival ( dmfs )  . 
 these endpoints were defined as the time from the start of rt to the time of death from any cause ( os ) , first failure at any site ( pfs ) , persistence or recurrence in the nasopharynx ( lpfs ) , persistence or recurrence in the neck ( rpfs ) , and new lesion development outside the head and neck region ( dmfs )  . 
the cox proportional hazards model by backward wald elimination method , where only variables whose p value of < 0.10 entered into the next step analysis repeating until a model where all the remaining variables had p < 0.05 , was used for multivariate analyses . results although the who histological type was unknown in some patients , approximately 70 % of all patients had either type ii or iii nonkeratinizing carcinoma . 
in the staging of npc , magnetic resonance imaging ( mri ) was used more frequently in the imrt group than in the 2d - rt or 3d - crt groups . 
table 4 summarized acute and late toxicities of 2d - rt , 3d - crt , and imrt groups . discussion in the pre - imrt era , 3d - crt was successfully used to treat npc as an alternative technique to 2d - rt , as well as a boost [ 20 , 21 ]  . 
soon after the clinical application of imrt in the treatment of npc , the short - term results of imrt suggested improved survival outcomes and quality of life [ 22 ]  . 
recent comparative clinical studies , both prospective and nonprospective , have compared the advantages of imrt with those of 2d - rt or 3d - crt [ 10 , 1316 , 20 ]  . although an improved dosage coverage of advanced primary t34 tumors by 3d - crt and imrt led to better local control than 2d - rt in recent clinical settings , there were some discrepancies in the results . 
83.8 % , respectively ( p = 0.046 ) ; however , the local control benefit of imrt over 2d - rt was statistically significant only in patients with stage t4 cancer . contrary to the above results [ 16 , 20 ] , another retrospective comparative analysis by lai et al . 
in our study , 3d - crt was associated with significantly improved lpfs for patients with t12 cancer , but the lpfs gain between imrt and 2d - rt was evident for both patients with t12 and those with t34 cancer , supporting the findings suggested by lee et al . 
 [ 13 ] suggested that the advantage of imrt over 3d - crt in patients with npc might be apparent in terms of quality of life , but without differences in tumor control . 
the lpfs results of the clinical comparative studies of 2d - rt , 3d - crt , and imrt according to t - category are summarized in table 5 . strahlenther onkol ( 2016 ) 192 : 3773851 3 383 table 4 acute and late toxicities of 2 - dimensional radiotherapy ( 2d - rt ) , 3 - dimensional conformal radiotherapy ( 3d - crt ) , and the intensitymodulated radiotherapy ( imrt ) groups scored by rtog / eortc toxicity criteria number ( % ) total ( n = 1237 ) 2d - rt ( n = 350 ) 3d - crt ( n = 390 ) imrt ( n = 497 ) 2d - rt vs . 
imrt was associated with a better os than was 2d - rt only in patients with stage iii to iv cancer , while 3d - crt was associated with a worse os strahlenther onkol ( 2016 ) 192 : 3773851 3 384 fig . 
furthermore , the finding that the proportion of use of concurrent chemotherapy among 2d - rt , 3d - crt , and imrt groups were different , and the factors such as stage migration or improved supportive care should also be evaluated in terms of their association with survival outcomes , especially os ; however , the evaluation of these factors was not included in the scope of this study . 
nonetheless , the importance of optimal control of the primary tumor must be emphasized , considering that a successful outcome was achieved in only a quarter of patients with isolated local recurrence . while differences in this study were compared among patients within southern asian countries , multivariate analyses showed that patients with cancers of who histology type i had poorer 5 - year os than did those with cancers of who types ii and iii , indicating that the prognosis according to the who histology type was consistent [ 13 , 23 , 24 ]  . 
 some sequencing patterns of combination chemotherapy were significantly associated with lpfs or os in the multivariate analyses , but the effects of neoadjuvant , concurrent , or adjuvant chemotherapy on the survival outcome could not be fully evaluated because the patients included in this study had stage i to iv cancer . an important drawback in the interpretation of our results is that the study was a multi - institutional retrospective analysis , in which a dose - fractionation scheme and the details of techniques within the 2d - rt , 3d - crt , and imrt groups were somewhat heterogeneous . 
because of the evaluation of toxicities was limited and just dependent on medical records , the association between the survival outcome of each rt technique and the treatment toxicity profile was also not fully evaluated . 
however , the overall results showed the survival outcomes of various rt techniques , and these were comparable with those from other large scale studies . conclusion our study showed that 3d - crt and imrt were associated with a better lpfs and os than was 2d - rt in npc . 
imrt was significantly superior in terms of os for advanced primary tumors ( t34 )  . strahlenther onkol ( 2016 ) 192 : 3773851 3 acknowledgments the authors would like to thank jihye cha , m.d. , jae myoung noh , m.d. , won taek kim , m.d. , young taek oh , m.d. , min kyu kang , m.d. , jin hee kim , m.d. , ji - yoon kim , m.d. , and sung whan kim , m.d. 
das gesamtpatientenkollektiv hatte ein medianes follow - up von 91 monaten ( cmt : 95 monate ; ef - rt : 110 monate ; if - rt : 87 monate ; rituximab : 49 monate )  . 
nach 8 jahren betrug das originalpublikation eichenauer da , pltschow a , fuchs m et al ( 2015 ) long - term course of patients with stage ia nodular lymphocyte - predominant hodgkin lymphoma : a report from the german hodgkin study group . 
aus diesem grund sollte die if - rt , welche das geringste risiko fr unerwnschte nebenwirkungen birgt , als goldstandard fr die therapie von patienten mit einem nlphl im stadium ia gelten . 
die alleinige therapie mit rituximab ist mit einem hheren rezidivrisiko in diesem patientenkollektiv belastet . kommentar das lymphozytenprdominante hodgkin - lymphom ( lphl ) unterscheidet sich hinsichtlich der histopathologie und dem klinischen verlauf grundstzlich vom klassischen hodgkinlymphom [ 1 , 2 ]  . 
ber alle tumorstadien hinweg kann durch die therapie bei durchschnittlich 95 % der patienten eine komplette remission erreicht werden ; in fortgeschrittenen stadien und frhen stadien mit risikofaktoren sind die berlebenschancen und die rezidivfreiheit deutlich schlechter [ 1 , 4 , 5 ]  . 
daher sollten fortgeschrittene stadien nach den klasstrahlenther onkol ( 2016 ) 192 : 428430 sischen hodgkin - lymphom - protokollen behandelt werden [ 1 , 4 ]  . die patienten mit einem lphl im frhen stadium ohne risikofaktoren haben eine exzellente langzeitprognose [ 1 ]  . die therapie war lange nicht klar deniert und beinhaltete eine alleinige rt , multimodale therapien aus rt und cht ( chemotherapie ) sowie monoklonale antikrper ( rituximab ; [ 68 ] )  . 
die if - rt mit reduzierter feldgre gilt laut der leitlinie der european society for medical oncology ( esmo ) und dem national comprehensive cancer network als goldstandard [ 8 , 10 , 11 ]  . das nlphl ist mit 5 % aller hodgkin - lymphome eine extrem seltene erkrankung , an der deutschlandweit lediglich 100 patienten im jahr erkranken [ 1 ]  . 
bezglich des os und pfs zeigte sich kein signikanter unterschied , ob nun mit einer cmt , if - rt oder ef - rt behandelt worden war [ 13 ]  . 
dies stimmt mit frheren kleineren retrospektiven untersuchungen berein [ 8 , 14 ]  . die rekrutierung der 256 patienten fr die vorliegende analyse erstreckte sich ber 21 jahre , in denen unterschiedliche therapieschemata angewandt wurden , insbesondere bei der radiochemotherapie ( rct )  . 
im median betrug die zeit der lokalen kontrolle nach cmt 55 monate , nach ef - rt 74 monate , nach if - rt 42 monate und nach alleiniger rituximab - therapie 10 monate . 
dies lsst vermuten , dass die alleinige rituximabtherapie keine komplette und dauerhafte lokale remission erreichen kann . neben den daten fr os und pfs wurde in der vorliegenden auswertung besonderer wert auf das ausma therapieassoziierter sptfolgen gelegt . 
in vorausgegangen publikationen wurde bereits gezeigt , dass diese sptfolgen hauptverantwortlich fr die letalitt von patienten mit nlphl im stadium ia sind , insbesondere kardiale toxizitten und sekundrmalignome [ 15 ]  . 
sie stimmt mit beobachtungen der kanadischen studiengruppe berein , die eine deutliche risikoreduktion beim bergang von efauf if - rt in kombination mit cht beobachtet hat [ 16 , 17 ]  . die vorliegende langzeitbeobachtung der deutschen hodgkin - studiengruppe zeigt , dass die alleinige if - rt ( 30 gy ) , verglichen mit cmt oder ef - rt , hnlich effektiv bei allerdings geringerer toxizitt ist . 
diehl v , sextro m , franklin j et al ( 1999 ) clinical presentation , course , and prognostic factors in lymphocyte - predominant hodgkins disease and lymphocyte - rich classical hodgkins disease : report from the european task force on lymphoma project on lymphocyte - predominant hodgkins disease . 
anagnostopoulos i , hansmann ml , franssila k et al ( 2000 ) european task force on lymphoma project on lymphocyte predominance hodgkin disease : histologic and immunohistologic analysis of submitted cases reveals 2 types of hodgkin disease with a nodular growth pattern and abundant lymphocytes . 
nogov l , reineke t , brillant c et al ( 2008 ) lymphocyte - predominant and classical hodgkins lymphoma : a comprehensive analysis from the german hodgkin study group . 
rehwald u , schulz h , reiser m et al ( 2003 ) treatment of relapsed cd20 + hodgkin lymphoma with the monoclonal antibody rituxi430 strahlenther onkol ( 2016 ) 192 : 428430 mab is effective and well tolerated : results of a phase 2 trial of the german hodgkin lymphoma study group . 
nogov l , reineke t , eich ht et al ( 2005 ) extended eld radiotherapy , combined modality treatment or involved eld radiotherapy for patients with stage ia lymphocyte - predominant hodgkins lymphoma : a retrospective analysis from the german hodgkin study group ( ghsg )  . 
wilder rb , schlembach pj , jones d et al ( 2002 ) european organization for research and treatment of cancer and groupe detude des lymphomes de ladulte very favorable and favorable , lymphocytepredominant hodgkin disease . 
wirth a , yuen k , barton m et al ( 2005 ) long - term outcome after radiotherapy alone for lymphocyte - predominant hodgkin lymphoma : a retrospective multicenter study of the australasian radiation oncology lymphoma group . 
eichenauer da , pltschow a , fuchs m et al ( 2015 ) long - term course of patients with stage ia nodular lymphocyte - predominant hodgkin lymphoma : a report from the german hodgkin study group . 
koh e - s , tran th , heydarian m et al ( 2007 ) a comparison of mantle versus involved - eld radiotherapy for hodgkins lymphoma : reduction in normal tissue dose and second cancer risk . 
fr die weitere analyse wurden nur patienten bercksichtigt , fr die komplette datenstze inklusive informationen ber komorbiditten vorlagen , bei denen eine rt dokumentiert und innerhalb von 6 monaten nach diagnose mit mindestens 25 fraktionen auch erfolgt war . 
die zahl der patienten pro arzt lag ber den gesamten zeitraum zwischen 1 und 70 patienten . bei solchen , die mit 3d - konformaler rt behandelt worden waren , spielte die jhrlich vom strahlentherapeuten behandelte patientenzahl keine rolle . 
bei imrt - patienten hingegen fand sich in der multivariaten analyse ein signikanter einuss des patientenvolumens : fr jeweils 5 patienten , die pro jahr mehr ( also ber dem durchschnittswert ) behandelt wurden , sank das todesrisiko um 21 % . 
die rt - qualitt spielt eine rolle bei den behandlungsergebnissen . originalpublikation boero ij , paravati aj , xu b et al ( 2016 ) importance of radiation oncologist experience among patients with head - and - neck cancer treated with intensity - modulated radiation therapy . 
soll also ein strahlentherapeut , der nur wenige patienten behandelt , lieber auf nummer sicher gehen und eine robuste 3d - crt anwenden statt eine difziele imrt , vereinfacht ausgedrckt : lieber geheilt mit xerostomie als ein marginales rezidiv ? die zahl der patienten pro behandelndem arzt war insgesamt sehr niedrig , nmlich ber einen zeitraum von 10 jahren durchschnittlich weniger als ein patient pro jahr und arzt . 
natrlich muss man davon ausgehen , dass wesentlich mehr patienten in den betreffenden einrichtungen behandelt worden waren und dass die geringe anzahl durch die selektionskriterien bedingt ist ( seer - daten von medicare - patienten , also dem staatlichen krankenversicherungsprogramm , das etwa 15 % der us - bevlkerung einschliet )  . 
allerdings bleibt die jhrliche patientenzahl auch dann niedrig , wenn man die zahlen fr die gesamtbevlkerung hochrechnet . der anteil von patienten , der eine simultane chemotherapie mit cisplatin oder cetuximab erhielt , war vergleichsweise gering , nmlich weniger als 40 % . 
vermutlich hatten also einige rzte noch wenig erfahrung mit ihr und andere bereits viel mehr . wenn man eine lernphase annimmt , kann das bedeuten , dass einige rzte diese phase vielleicht bereits abgeschlossen hatten und andere sich noch in ihr befanden . es knnte sein , dass die untersuchung heute anders ausfallen wrde , wenn alle ihre lernphase abgeschlossen haben . innerhalb der einrichtungen ist eine interne selektion nicht auszuschlieen . 
es knnte sein , dass erfahrenere rzte sich eher um die prognostisch gnstigen flle kmmerten und diejenigen mit ungnstiger prognose und fraglich kurativer intention von weniger erfahrenen rzten behandelt wurden . 
ein bias dieser art wird trotz multivariater analyse die ergebnisse verzerren . die autoren fragen in der diskussion schon selbst , ob es wirklich die erfahrung mit der imrt ist , welche die guten ergebnisse bewirkt , oder ob nicht die imrt ein indikator fr die qualitt einer komplexen interdisziplinren behandlungskette ist . noch komplizierter ist eine ganz andere frage zu beurteilen , die auch im kommentar zu der arbeit bereits aufgeworfen wird [ 4 ] : imrt kann die nebenwirkungen zwar sicher gegenber einer 3d - crt vermindern , ein effekt auf die lokoregionale kontrolle besteht aber doch fazit die hier mitgeteilten daten lassen sich nicht einfach interpretieren . 
bei der bestimmung der tumorausbreitung , der normalgewebeschonung oder der planevaluierung , und bieten daher eine hervorragende chance , die ohnehin relativ zu anderen verfahren hohe qualitt der strahlentherapie weiter zu verbessern . 
boero ij , paravati aj , xu b et al ( 2016 ) importance of radiation oncologist experience among patients with head - and - neck cancer treated with intensity - modulated radiation therapy . 
eisbruch a , harris j , garden as et al ( 2010 ) multiinstitutional trial of accelerated hypofractionatedintensity - modulated radiation therapy for early - stage oropharyngeal cancer ( rtog 00 - 22 )  . 
kam mk , leung sf , zee b et al ( 2007 ) prospective randomized study of intensity - modulated radiotherapyon salivary gland function in early - stage nasopharyngeal carcinoma patients . 
nutting cm , morden jp , harrington kj et al ( 2011 ) parsport trial management group : parotidsparingintensity modulated versus conventional radiotherapy in head and neck cancer ( parsport ) : aphase 3 multicentrerandomised controlled trial . 
peters lj , osullivan b , giralt j et al ( 2010 ) critical impact of radiotherapy protocol compliance andquality in the treatment of ad424 strahlenther onkol ( 2016 ) 192 : 422424 vanced head and neck cancer : results from trog 02.02. 
die nach der bindung des egf ( epidermal growth factor ) an den egfrezeptor ( egfr ) ausgelsten signalkaskaden spielen bei vielen tumorentitten sowohl bei der entwicklung und dem fortschreiten eines tumors als auch bei der bildung von metastasen eine groe rolle . 
kombinationen aus radio ( chemo ) therapie mit blockierung des egfr durch antikrper oder tyrosinkinaseinhibitoren ( tkis ) erscheinen somit klinisch sinnvoll , um sowohl die lokale tumorkontrolle zu verbessern , als auch systemische antitumorreaktionen auszulsen und das gesamtberleben zu verbessern . 
die vorliegende prklinische arbeit untersucht nun erstmals , wie eine hemmung des egfr auf originalpublikation kriegs m , gurtner k , brammer i et al ( 2016 ) radiosensitization of nsclc cells by egfr inhibition is the result of an enhanced p53 - dependent g1 arrest . 
die abhngigkeit vom p53 - status wurde an weiteren zelllinien besttigt . des weiteren war p21 , ein inhibitor zyklinabhngiger kinasen , welcher wesentlich fr die kontrolle des zellzyklus ist , fr den rtund tki - induzierten g1 - arrest notwendig . 
ein wesentlicher unterschied von rtim vergleich zu tki - induziertem g1 - arrest ist allerdings , dass nur der durch rt induzierte permanent ist und durch eine vorherige egfrhemmung verstrkt werden kann . 
bei der frage , ob der induzierte g1 - arrest auswirkungen auf die koloniebildung 426 strahlenther onkol ( 2016 ) 192 : 425427 des egfr zur strahlensensibilisierung infolge der induktion eines permanenten g1 - zellzyklusarrests beitrgt , ist in vivo kein signikanter effekt dieser kombination auf das wachstum von xenogenen tumoren festzustellen . 
eine hemmung des egfr lst tatschlich auch immunologische effektormechanismen aus [ 7 ]  . die autoren zeigten weiter mechanistisch , dass bei nsclc - zellen keine apoptose durch einzeloder kombinationsbehandlung ausgelst wird , zumindest noch nicht am ersten tag nach der behandlung . 
somit gilt es , in zuknftigen studien herauszunden , welche formen des zelltodes durch kombinationen aus egfr - hemmung und rt induzierbar sind , einschlielich seneszenz , autophagie und nekrose [ 9 ]  . auch werfen die versuche die wichtige frage auf , warum gerade erlotinib bei dem gewhlten modellsystem sowohl in vitro als auch in vivo am effektivsten ist . 
dies zeigt einmal mehr , dass mehrere prklinische modellsysteme mit detaillierten mechanistischen untersuchungen notwendig sind , um die fr die klinik basalen fragen zu beantworten . fazit es werden dringend weitere prklinische arbeiten wie die hier vorliegende bentigt , um die multimodalen konzepte zur therapie des nsclc weiter zu verbessern . 
in vivo scheint allerdings eine restimulation der tumorzellen und eine damit einhergehende ausung des zellzyklusarrests der grund zu sein , dass durch egfr - hemmung keine radiosensitivierung stattfand , zumindest nicht im gewhlten immundezienten mausmodell . kommentar dass vor allem multimodale tumortherapiekonzepte zur optimierung der therapieergebnisse fhren , ist in den letzten jahren immer deutlicher geworden . 
allerdings bedarf es dafr sorgfltiger prklinischer analysen , um die besten kombinationen aus rt , chemotherapie , immunotherapie und zielgerichteter therapie sowie deren zeitliche abfolge herauszunden [ 4 ]  . 
pd - l1 ist der ligand fr den immuncheckpoint - rezeptor pd - 1 ( programmed death 1 ; [ 5 ] )  . die vorliegende sorgfltige prklinische arbeit zeigt berzeugend , dass interagierende effekte einer egfrhemmung mit ionisierender strahlung vielschichtig sind und auf mehreren ebenen stattnden . 
bonner ja , harari pm , giralt j , cohen rb , jones cu , sur rk , raben d , baselga j , spencer sa , zhu j , youssouan h , rowinsky ek , ang kk ( 2010 ) radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
giralt j , trigo j , nuyts s , ozsahin m , skladowski k , hatoum g , daisne jf , yunes ancona ac , cmelak a , mesia r , zhang a , oliner ks , vanderwalde a ( 2015 ) panitumumab plus radiotherapy versus chemoradiotherapy in patients with unresected , locally advanced squamous - cell carcinoma of the head and neck ( concert - 2 ) : a randomised , controlled , open - label phase 2 trial . 
hotta k , sasaki j , saeki s , takigawa n , katsui k , takayama k , nogami n , shioyama y , bessho a , kishimoto j , tanimoto m , kiura k , ichinose y ( 2015 ) getinib combined with standard chemoradiotherapy in egfr - mutant locally advanced non - small - cell lung cancer : the logik0902 / olcsg0905 intergroup study protocol . 
troiani t , zappavigna s , martinelli e , addeo sr , stiuso p , ciardiello f , caraglia m ( 2013 ) optimizing treatment of metastatic colorectal cancer patients with anti - egfr antibodies : overcoming the mechanisms of cancer cell resistance . 
jones kr , elmore lw , jackson - cook c , demasters g , povirk lf , holt se , gewirtz da ( 2005 ) p53 - dependent accelerated senescence induced by ionizing radiation in breast tumour cells . 
lauber k , ernst a , orth m , herrmann m , belka c ( 2012 ) dying cell clearance and its impact on the outcome of tumor radiotherapy . front oncol 2 : 116 . 
patienten mit einem dlbcl im stadium i und ii , die mit einer polychemotherapie oder chemotherapie plus konsolidierender rt behandelt worden waren , wurden in der amerikanischen ncdb - datenbank ( national cancer data base , 19982012 ) identiziert . 
die wahl der behandlung wurde signikant durch folgende faktoren beeinusst : rasse , komorbiditt , versicherungstyp , bildung , art der behandlungseinrichtung , alter , stadium , b - symptome , entfernung vom behandlungsort und diagnosejahr . die mediane nachbeobachtungszeit betrug 60 monate ( iqr , 33 bis 93 )  . 
insgesamt ist in den usa der einsatz einer konsolidierenden rt nach erfolgter polychemotherapie rcklug , doch wirkt sich der verzicht auf eine konsolidierende rt nach erfolgter chemotherapie , also die alleinige chemotherapie , negativ auf das berleben der patienten aus . originalpublikation vargo ja , gill bs , balasubramani gk et al ( 2015 ) treatment selection and survival outcomes in early - stage diffuse large b - cell lymphoma : do we still need consolidative radiotherapy ? j clin oncol 10 ( 33 ) : 37107 ( cid : 2 ) med . 
nach einfhrung der rituximab - kombination mit einer polychemotherapie ist die rolle einer konsolidierenden rt nach der systemischen therapie nicht klar festgelegt , obwohl mehrere retrospektive analysen auf den gnstigen einuss der konsolidierenden rt hingewiesen strahlenther onkol ( 2016 ) 192 : 502504 hatten [ 29 ]  . 
in einer zwischenanalyse der randomisierten studie unfolder der deutschen studiengruppe hochmaligne nhl ( dshnhl ) wurde ein vorteil der additiven rt auch in der rituximab - ra bei patienten mit dlbcl nachgewiesen ( nct00278408 ) [ 10 ]  . die vorliegende studie , in der 59.255 patienten aus der ncdb ausgewertet wurden , ist die grte analyse zu dieser fragestellung . 
dass im zusammenhang mit modernen chemotherapieprotokollen und ihrer optimistischen erwartungen zunehmend auf die rt verzichtet wird , beruht auf bertriebenen befrchtungen von erhhter toxizitt und einem gesteigerten risiko fr sekundrmalignome . 
leider wird immer noch zu wenig wahrgenommen , dass die neuen mglichkeiten der modernen rt ( differenzierter einsatz der imrt und der bildgefhrten rt [ igrt ] , auch die rt in tiefer inspiration bei mediastinalem befall sowie verkleinerte bestrahlungsvolumina ) die therapeutische ratio fr rt erweitern und mgliche radiogene toxizitten verringern knnen [ 1214 ]  . fazit die kombination aus chemotherapie und rt zeigt bei patienten mit dlbcl auch in der rituximab - ra einen signikanten berlebensvorteil gegenber einer alleinigen chemotherapie . 
vargo ja , gill bs , balasubramani gk et al ( 2015 ) treatment selection and survival outcomes in early - stage diffuse large b - cell lymphoma : do we still need consolidative radiotherapy ? j clin oncol 33 ( 32 ) : 37103717 . 
phan j , mazloom a , medeiros lj et al ( 2010 ) benet of consolidative radiation therapy in patients with diffuse large b - cell lymphoma treated with r - chop chemotherapy . 
dabaja bs , vanderplas am , crosby - thompson al et al ( 2015 ) radiation for diffuse large b - cell lymphoma in the rituximab era : analysis of the national comprehensive cancer network lymphoma outcomes project . 
pfreundschuh m , ho ad , cavallin - stahl e et al ( 2008 ) prognostic signicance of maximum tumour ( bulk ) diameter in young patients with good - prognosis diffuse large - b - cell lymphoma treated with chop - like chemotherapy with or without rituximab . 
held g , zeynalova s , murawski n et al ( 2013 ) impact of rituximab and radiotherapy on outcome of patients with aggressive b - cell lymphoma and skeletal involvement . 
ballonoff a , rusthoven ke , schwer a et al ( 2008 ) outcomes and effect of radiotherapy in patients with stage i or ii diffuse large b - cell lymphoma : a surveillance , epidemiology , and end 504 strahlenther onkol ( 2016 ) 192 : 502504 results analysis . 
hu c , deng c , zou w et al ( 2015 ) the role of consolidative radiotherapy after a complete response to chemotherapy in the treatment of diffuse large b - cell lymphoma in the rituximab era : results from a systematic review with a meta - analysis . 
eich ht , heimann m , sttzer h et al ( 2009 ) long - term outcome and prognostic factors in early - stage nodal low - grade non - hodgkins lymphomas treated with radiation therapy . 
pugh tj , ballonoff a , rusthoven ke et al ( 2010 ) cardiac mortality in patients with stage i and ii diffuse large b - cell lymphoma treated with and without radiation : a surveillance , epidemiology , and end - results analysis . 
lowry l , smith p , qian w et al ( 2011 ) reduced dose radiotherapy for local control in non - hodgkin lymphoma : a randomised phase iii trial . 
illidge t , specht l , yahalom j et al ( 2014 ) modern radiation therapy for nodal non - hodgkin lymphoma - target denition and dose guidelines from the international lymphoma radiation oncology group . 
yahalom j , illidge t , specht l et al ( 2015 ) modern radiation therapy for extranodal lymphomas : field and dose guidelines from the international lymphoma radiation oncology group . 
huber1 , 2 , 3 katja lindel1 received : 10 february 2016 / accepted : 8 april 2016 / published online : 31 may 2016 springer - verlag berlin heidelberg 2016 abstract purpose the aim of this work was to evaluate outcomes and toxicities of high dose - rate ( hdr ) endoluminal brachytherapy in a cohort of esophageal cancer patients . patients and methods we analyzed the records of 36 patients treated with hdr brachytherapy for histologically conrmed esophageal cancer . 
locoregional recurrence was observed in 24 patients after a median time of 3 months ; 1and 2 - year recurrence - free survival rates were 51 and 51 % for the patients treated for primary tumors and 11 and 6 % for patients treated for tumor recurrence , respectively . 
median overall survival was 18 months ; estimated overall survival rates at 1 , 2 , and 3 years were 63 , 50 , and 30 % after primary brachytherapy , and 60 , 25 , and 6 % after recurrence therapy . 
mild dysphagia was the most common side effect in 17 patients ; 8 patients suffered from locoregional grade 3 toxicities , and no grade 4 or 5 toxicities were observed . conclusions endoluminal brachytherapy during the course of esophageal cancer treatment can be safely applied and results in good functional outcomes regarding dysphagia with low rates of severe toxicities . keywords adverse effects dysphagia neoplasm recurrence , local survival outcome toxicity endoluminale high dose - rate - brachytherapie bei primrem und rezidivierendem sophaguskarzinom ergebnisse der kohorte eines groen einzelzentrums zusammenfassung zielsetzung analyse von berleben und toxizitten nach endoluminaler high dose - rate ( hdr ) - brachytherapie in einer kohorte von patienten mit sophaguskarzinom . strahlenther onkol ( 2016 ) 192 : 458466 patienten und methoden ausgewertet wurden die krankenakten von 36 patienten , die aufgrund eines histologisch besttigten sophaguskarzinoms mit hdr - brachytherapie behandelt wurden . 
ein lokalrezidiv wurde bei 24 patienten im mittel nach 3 monaten diagnostiziert ; die raten fr das rezidivfreie berleben nach 1 und 2 jahren betrugen jeweils 51 % fr die patienten nach primrtherapie und 11 bzw . 
das mittlere gesamtberleben betrug 18 monate ; die berlebenszeiten nach 1 , 2 und 3 jahren lagen bei 63 , 50 und 30 % nach primrer brachytherapie , und 60 , 25 und 6 % nach rezidivbehandlung . der histologische befund eines adenokarzinoms , fehlende komplettremission nach behandlung und rezidivtherapie waren mit signikant schlechteren prognosen assoziiert . eine geringgradige dysphagie wurde bei 17 % der patienten beobachtet und war damit die hugste nebenwirkung ; 8 patienten litten an lokoregionren grad - 3 - toxizitten ; es wurden keine grad - 4oder - 5 - toxizitten beobachtet . schlussfolgerung die endoluminale brachytherapie zur behandlung von sophaguskarzinomen kann sicher durchgefhrt werden und resultiert in guten ergebnissen mit moderater lokaler toxizitt und geringen raten schwerwiegender nebenwirkungen . schlsselwrter nebenwirkungen dysphagie lokales tumorrezidiv berlebensbezogenes ergebnis toxizitt introduction esophageal cancer is the sixth most common cause for cancer - related deaths worldwide [ 13 ]  . 
while the majority of esophageal cancers are squamous cell carcinomas with a high incidence in the middle east and southern asia , the incidence of esophageal adenocarcinomas has measurably increased in western europe and the united states in recent years [ 1 , 4 , 5 ]  . 
surgical tumor resection has been established as the treatment of choice for locally limited cancer stages and may be combined with a neo - adjuvant course of chemoradiotherapy in locally advanced stages , resulting in better overall survival and local control [ 6 , 7 ]  . 
in cases of inoperable disease , denitive chemoradiotherapy is the treatment of choice ; to date , no study has demonstrated superior survival of patients treated with neo - adjuvant chemoradiotherapy followed by surgery as compared to denitive chemoradiotherapy alone [ 8 ]  . 
radiation dose concepts for denitive chemoradiotherapy are largely based on the rtog 94 - 05 trial , while the observed high levels of persistent or recurrent disease warrant optimization of the radiotherapy , e . 
g. , by highly conformal application of increased radiation doses [ 9 , 10 ]  . irrespective of therapeutic advances over the last 20 years , the prognosis for this disease is still dismal with 5 - year overall survival of less than 20 % [ 3 , 11 ]  . 
endoluminal brachytherapy has also demonstrated benecial effects for the treatment of recurrent esophageal cancer [ 16 ]  . high dose - rate ( hdr ) brachytherapy delivers highly conformal radiotherapy treatments using high dose - rate radiation , commonly exceeding 12 gy / h . 
for endoluminal brachytherapy treatments of the esophagus , temporary catheters are placed in the organs lumen adjacent the tumor , using endoscopic or uoroscopic guidance . radioactive isotopes such as 192ir are then administered through the catheters and radiotherapy is delivered based on calculated dwell locations and dwell times [ 17 ]  . 
due to the highly conformal nature of this radiotherapy treatment , esophageal endoluminal brachytherapy can deliver high local doses while largely sparing the surrounding organs at risk , especially the lung and spinal cord . 
however , the rtog 92 - 07 trial reported high rates of severe local toxicities associated with endoluminal hdr brachytherapy . brachytherapy may be a valuable treatment option for patients having undergone prior percutaneous radiotherapy . based on the high levels of severe brachytherapy - associated toxicities reported in the rtog 92 - 07 phase i / ii trial , caution is warranted regarding the wide - spread application of endoluminal brachytherapy for the boost treatment of esophageal cancer [ 18 ]  . 
nevertheless , certain subgroups of esophageal cancer patients may benet from this treatment that need to be further identied . this retrospective study analyzed the efcacy and side effects of endoluminal hdr brachytherapy for the treatment of esophageal cancer in a large single - center patient cohort . strahlenther onkol ( 2016 ) 192 : 458466 63.5 brachytherapy initial tumor recurrent tumor brachytherapy regimes 2 4 gy 3 4 gy 4 4 gy 2 5 gy 3 5 gy 4 5 gy 2 6 gy other treatment planning ct - based processor - based concurrent ebrt mean ebrt total dose ( gy ) concurrent chemotherapy cisplatin / 5 - uorouracil cisplatin none tab . 
1 patient characteristics patient characteristics age ( years ) median minimum maximum gender male female histology squamous cell carcinoma adenocarcinoma other location upper thoracic central thoracic lower thoracic prior malignancy previous radiotherapy for esophageal cancer for secondary malignancy no previous radiotherapy patients and methods patient characteristics ebrt external beam radiotherapy , ct computed tomography a total of 36 patients treated with endoluminal hdr brachytherapy for esophageal cancer at heidelberg university hospital between 2005 and 2015 were included in this analysis . 
thereby , 56 % of patients ( 20 patients ) were treated with brachytherapy to target recurrent disease in order to achieve palliation for stenosing tumors or to treat dysphagia or bleeding . 
six patients ( 17 % ) had been treated with radiotherapy for a prior secondary malignancy : 5 patients ( 14 % ) had been treated for head - and - neck cancers , and 1 patient had received mediastinal radiotherapy for non - small cell lung cancer . 
after local analgesia with lidocaine spray and sedation using midazolam , a catheter with a diameter of 9 mm ( mallinckrodt medical , petten , the netherlands ) was inserted into the esophageal lumen by the radiation oncologist and xed to the mouth . 
endoluminal radiation was delivered to the endoscopically visible tumor area including 2 cm margins at the proximal and distal end , and dose was prescribed to 10 mm from the radiation source . 
total dose and fractionation regimes were chosen depending on the length of tumor inltration and radiation doses applied during potential previous treatments . follow - up examinations the initial follow - up examination was scheduled at 68 weeks after endoluminal brachytherapy , and further followup examinations were carried out at 3 - month intervals . 
depending on the performance status of the patients , followup examinations consisted of esophageal endoscopy including biopsy assessment and thoracic / abdominal ct scans . the endoscopic response at the rst follow - up appointment was assessed as complete response ( cr ) with no histologic sign of vital tumor tissue , as stable disease ( sd ) with incomplete regression and positive biopsy ndings , or as progressive disease ( pd ) with tumor progression > 25 % . systemic progression was measured by thoracic / abdominal ct scans at 3 - month intervals . 
univariate analyses were carried out by log - rank test . results response to hdr brachytherapy median follow - up time was 9 months ( range 193 months ) for the entire cohort and 19 months for the surviving patients . 
complete endoscopic response at the rst followup examination was observed in 11 of 16 patients ( 69 % ) treated for the primary presentation of their cancer and in 462 primary recurrence strahlenther onkol ( 2016 ) 192 : 458466 primary recurrence time ( months ) time ( months ) fig . 
locoregional recurrence after esophageal brachytherapy was observed in 5 patients receiving an initial brachytherapy boost ( 31 % ) and in 17 patients treated for recurrent disease ( 85 % ) after a median time of 15 and 3 months , respectively . 
one patient in the primary brachytherapy cohort developed pulmonary metastases ; 4 patients treated for recurrence suffered from distant spread : 2 of them exhibited pulmonary metastases , 1 patient developed both pulmonary and hepatic spread , and 1 patient suffered from bone metastases . 
adenocarcinoma histology and treatment for recurrent tumors were associated with signicantly reduced prognoses . in addition , patients with a noncomplete response after endoluminal brachytherapy only had 3 months to rfs as opposed to 15 months observed in patients with a complete response . 
a total of 35 patients ( 97 % ) received the complete endoluminal treatment as planned : one patient scheduled for brachytherapy for a recurrent cancer received only one hdr fraction due to a persistent tightness of the laryngeal anatomy and was subsequently rescheduled for external beam re - irradiation . 
the most commonly observed adverse effect was dysphagia : 10 patients ( 28 % ) complained about mild dysphagia ( ctcae grade 1 ) and 7 patients ( 19 % ) about grade 2 dysphagia . 
one patient ( 3 % ) treated for the primary presentation of his cancer developed a brachytherapy - associated tracheo - esophageal stula after 2 years , requiring tracheal stenting . 
no patient reported neurological or pulmonary side effects . discussion here , we report encouraging outcome and toxicity data of esophageal cancer patients treated with high dose - rate endoluminal brachytherapy compared to previously published patient cohorts . in this dataset , the 16 patients receiving treatment for the primary presentation of their esophageal cancer revealed a median overall survival of 18 months . 
 [ 20 ] reported a median overall survival of 15 months in patients treated with combination radiotherapy , while vuong et al . [ 21 ] found a median overall survival of 26 months in their patient cohort , when high total doses up to 70 gy were applied to the tumor . 
dose prescription for the chemoradiation treatment of esophageal cancer has been subject to some discussion and has largely been based on the rtog 94 - 05 trial that compared an established course of 50.4 gy with a high - dose regime using in this 64.8 gy using 2d radiotherapy planning [ 9 , 22 ]  . trial , high - dose irradiation did not improve locoregional control or patient survival , but strongly increased the rate of treatment - related mortality . 
however , a meta - analysis [ 23 ] based on 26 trials provided evidence by geh et al . for a dose - response relationship between increased doses of radiotherapy and levels of pathological complete remission , suggesting benecial effects of dose escalation in esophageal cancer . 
since then , several studies using conformal radiotherapy techniques have demonstrated ways of applying higher tumor doses without increasing radiation in our cohort doses to the surrounding normal tissues . of patients receiving radiation treatment for the primary presentation of esophageal cancer , patients received external beam radiotherapy to a median dose of 45 gy and endoluminal boost radiation to an additional median dose of 15 gy . 
in line with our ndings , total radiation doses up to 60 gy have been shown to be safely applied in several patient cohorts with promising results regarding tumor response and survival [ 10 , 2426 ]  . in contrast to patients treated for the primary presentation of esophageal cancer , patients suffering from recurrent disease have often been pre - irradiated and therefore tolerate only reduced doses for re - irradiation . 
while improvements in chemotherapeutic treatment have increased response rates for systemic spread , efcient local therapies are needed to target locoregional recurrence , as it often strongly affects the patients quality of life . 
in our dataset , patients undergoing brachytherapy for tumor recurrence only had a 14 - month median overall survival . these survival data compare favorably with other cohorts of patients treated with endoluminal brachytherapy for recurrent esophageal cancer . 
cancer [ 16 ] showed a median overall survival of 10 months in a cohort of 30 patients treated with hdr 464 strahlenther onkol ( 2016 ) 192 : 458466 brachytherapy for recurrent esophageal ; similarly , harms et al . 
a different patient cohort treated with 12 gy endoluminal brachytherapy exhibited an overall survival of 6 months [ 28 ]  . various different dose regimes have been used to apply esophageal endoluminal brachytherapy ; and single doses between 4 and 6 gy have been most commonly reported . although it has been suggested that higher single doses in increased treatment - associated toxicities , may result a prospective trial by sur et al . [ 29 ] compared a total dose of 16 gy using 2 sessions of 8 gy with 18 gy in 3 fractions of 6 gy demonstrated comparable survival rates with a median overall survival of 8 months and equal toxicities regarding strictures and stulas . 
due to the highly conformal nature of endoluminal brachytherapy , radiation - related toxicities are mostly conned to the esophageal tissue and rarely affect adjacent organs at risk ; apart from dysphagia , esophageal strictures and tracheo - esophageal stulas are the most common severe side effects from endoluminal treatment [ 16 , 30 , 31 ]  . in the rtog 92 - 07 trial , 12 % of patients treated with 3 brachytherapy fractions of 5 gy were found to develop esophageal stulas [ 18 , 32 ]  . in our patient cohort , mostly mild - to - moderate toxicities to the esophagus were observed ; only 1 patient ( 3 % ) was found to develop a brachytherapy - induced tracheo - esophageal stula . 
 [ 16 ] reported 4 patients ( 15 % ) suffering from persistent stulas and an additional 2 patients ( 7 % ) with severe stenosis after brachytherapy , and harms et al . [ 27 ] reported 2 of 16 patients ( 13 % ) developing stulas and 1 patient with fatal arterial bleeding . 
several risk factors for the development of severe brachytherapy - associated toxicities have been discussed , and it has been suggested that the risk increases with the use of smaller applicators , total doses delivered to the mucosal surface exceeding 12 gy and the application of concomitant chemotherapy [ 33 ]  . 
however , as those parameters derive from a summary of relatively small retrospective cohorts , further analyses are needed to more clearly identify potential parameters inuencing esophageal toxicities after brachytherapy . 
based on the ndings reported from the rtog 92 - 07 trial , the american brachytherapy society [ 35 ] has published guidelines outlining which patients may benet from receiving endoluminal brachytherapy boost treatment as a part of curative chemoradiotherapy regimes . 
the outlined criteria include unifocal cancers located within the thoracic part , a tumor length of less than 10 cm , the absence of distant metastases and no tracheo - esophageal stula or tracheal involvement . 
the potential usage of endoluminal esophageal brachytherapy in the palliative setting has been investigated in several randomized trials [ 3639 ] , and potential treatment indications have been outlined by the american brachytherapy society [ 35 ]  . 
these include stenoses , dysphagia , or esophageal hemorrhage and seem to be a viable alternative to esophageal stent placement [ 40 ]  . beyond the use of endoluminal brachytherapy to target primary or recurrent esophageal cancers , usage of highly conformal external beam radiation techniques has been investigated as a means of applying high radiation doses while sparing surrounding organs at risk . 
several planning studies have been published on that topic ; it has been demonstrated that compared to 2d treatment plans applying 50.4 gy , intensity - modulated radiotherapy ( imrt ) plans using 64.8 gy were able to signicantly reduce normal tissue doses despite increasing tumor doses by 14 gy [ 41 ]  . another imrt - based planning study showed no signicant increase in radiation doses to normal tissues by escalating esophageal tumor doses from 45 to 54 gy [ 24 ]  . 
in addition , it has been suggested that the use of rotational imrt techniques may help in further decreasing the doses applied to mediastinal organs at risk [ 25 , 42 ]  . 
analyses of esophageal cancer patients receiving imrt as a primary treatment with integrated tumor boost doses reaching or exceeding 60 gy have demonstrated reasonably good results [ 10 , 43 ]  . 
however , several publications demonstrated high levels of severe toxicity when recurrent esophageal cancers were re - irradiated using external beam approaches , with high rates of tracheo - esophageal stulas and toxicities to the surrounding tissues [ 4446 ]  . 
while photon imrt may be associated with increased severe side effects compared to endoluminal brachytherapy , the advent of particle treatments , especially proton radiotherapy , may open up a possibility for external beam re - treatment of esophageal cancer patients . 
a recent prospective study investigating proton re - radiotherapy in 14 esophageal cancer patients demonstrated the feasibility of this method and encouraging rates of symptom control , albeit with 14 % grade 5 toxicities [ 47 ]  . conclusion similar to most other analyses in the eld , our study has limitations such as the relatively small number of patients and the heterogeneity of the cohort . 
nevertheless , endoluminal brachytherapy was showed to be a safe and feastrahlenther onkol ( 2016 ) 192 : 458466 sible treatment option both as a highly conformal boost for denitive radiation and chemoradiation approaches and as a salvage treatment for recurrent esophageal cancer for a selective subgroup of patients . 
while bearing in mind increased levels of treatment - associated toxicities , further prospective studies are warranted investigating endoluminal brachytherapy approaches in larger cohorts of esophageal cancer patients in order to further identify subgroups of patients who may especially benet from this treatment . acknowledgements this work was supported by a heidelberg university young investigator grant to n.h. 
15 , 81377 munich , germany 2 department of urology , ludwig - maximilians - university , munich , germany 3 department of pathology , university hospital rwth aachen , aachen , germany in subgroup 2 , and 9 patients in subgroup 3 had ongoing androgen deprivation therapy . conclusion the present study of 94 pt3a n0 r1 prostate cancer patients provides insight into medical care of this patient cohort and underlines the need for additive rt for the majority of patients to achieve long - term biochemical control . 
although immediate adjuvant rt was applied with restraint ( 20 % ) , during the observation period 60 of 94 patients ( 63.8 % ) received rt highlighting the need of postoperative treatment . keywords prostate cancer postoperative radiotherapy salvage radiotherapy biochemical relapse radical prostatectomy risiko fr ein biochemisches rezidiv und zeitpunkt der strahlentherapie bei pt3a n0 prostatakarzinom mit positivem schnittrand eine monozentrische analyse zusammenfassung hintergrund trotz der nachweislich verbesserten biochemischen kontrolle besteht uneinigkeit hinsichtlich notwendigkeit und zeitpunkt einer adjuvanten radiotherapie ( rt ) bei lokal fortgeschrittenem prostatakarzinom . patienten und methoden vierundneunzig prostatakarzinompatienten ( pt3a n0 r1 ) , die zwischen 2005 und 2009 radikal operiert worden waren , wurden retrospektiv ausgewertet . 
postoperativ waren 71 patienten psa ( prostataspezisches antigen ) - negativ ( < 0.07 ng / ml ) ; von diesen strahlenther onkol ( 2016 ) 192 : 440448 blieben whrend des gesamten follow - up 36 psa - negativ ( gruppe 1 ) , 14 von ihnen erhielten eine adjuvante rt . bei 35 der postoperativ psa - negativen patienten trat ein biochemisches rezidiv auf , von diesen erhielten 28 eine salvage - bestrahlung ( gruppe 2 )  . 
ein patient in gruppe 1 , 5 patienten in gruppe 2 und 9 in gruppe 3 standen bis zum letzten follow - up unter antiandrogener therapie . schlussfolgerung das vorgestellte kollektiv zeigt reprsentativ die versorgungsrealitt und die notwendigkeit einer postoperativen behandlung fr die mehrheit der patienten , um eine langfristige biochemische kontrolle zu erreichen . bei unmittelbar postoperativ eher zurckhaltendem einsatz einer adjuvanten rt ( 20 % ) wurden im verlauf letztlich 60 von 94 patienten ( 63 , 8 % ) einer rt zugefhrt . schlsselwrter prostatakarzinom postoperative radiotherapie salvage - radiotherapie biochemisches rezidiv radikale prostatektomie introduction despite mature results from three randomized trials ( eortc 22911 , swog 8794 , aro 96 - 02 ; [ 17 ] ) on adjuvant radiotherapy ( rt ) in locally advanced prostate cancer with signicantly improved biochemical recurrence - free survival ( bfs ) , the need for adjuvant rt is still under debate . although the risk of recurrence in locally advanced stages reach up to 3060 % [ 8 , 9 ] , many patients are not referred to rt . 
the main reason inuencing clinical decision - making may be the lack of improved overall survival ( os ) seen only in the swog 8794 [ 6 ] or the assumed noninferiority of early salvage rt [ 1014 ]  . 
in order to investigate medical care of pt3a r1 disease after radical prostatectomy ( rpe ) and the use of adjuvant or salvage rt in daily practice , a retrospective analysis of 94 patients was performed . methods patients a total of 94 patients with pt3a n0 stage and microscopic positive resection margin ( r1 ) who had consecutively undergone rpe between 2005 and 2009 at the department of urology , ludwig - maximilians - university , munich , were identied . 
patients with a prostate - specic antigen ( psa ) value of > 10 ng / ml , gleason score ( gs ) 8 , stage ct3 / 4 had a bone scintigraphy . 
cox proportional hazard models were used to estimate hazard ratios ( hr ) with corresponding 95 % condence intervals ( ci )  . results in total , 94 pt3a n0 r1 patients were identied . 
based on the damico risk group classication [ 17 , 18 ] for estimating the preoperative risk of biochemical relapse , 24 patients ( 26 % ) had a low , 51 patients ( 54 % ) an intermediate , and 19 patients ( 20 % ) a high risk stage . 
more than two - thirds of the initially thought low / intermediate risk patients turned out to be high risk after 442 strahlenther onkol ( 2016 ) 192 : 440448 tab . 
after rpe 71 of 94 patients ( 76 % ) had an undetectable psa level ( < 0.07 ng / ml ) , while 23 of 94 patients ( 24 % ) showed elevated psa levels immediately after surgery ( > 0.07 ng / ml , subgroup 3 )  . 
fourteen of 36 patients with undetectable psa levels received immediate postoperative rt , while 28 of 35 patients with biochemical relapse received salvage rt , and 18 of 23 patients with persisting psa levels after surgery received additive rt . 
after rt , 4 patients had distant metastases only , 3 patients nodal and distant metastases , 1 patient pelvic lymph node involvement only , and 1 patient had locoregional and distant recurrence . no other therapies apart from rpe , postoperative rt , and adt were applied . strahlenther onkol ( 2016 ) 192 : 440448 fig . 
b time from surgery until androgen deprivation therapy ( months ) stratied to subgroups 2 ( red lines ) and 3 ( blue lines ) and the use of radiotherapy . 
d time from surgery until biochemical recurrence ( months ) stratied to preoperative psa . psa prostate - specic antigen , gs gleason score , rt + radiotherapy applied , rt radiotherapy not applied psa - negative patients after surgery without biochemical relapse ( subgroup 1 ) psa - negative patients after surgery with biochemical relapse ( subgroup 2 ) fourteen of 36 patients in subgroup 1 received adjuvant rt within the rst 15 months after rpe . 
two patients of the rt group had adt starting before / concomitantly with rt ( median duration 43 months ; range 482 months ) and 1 patient had it permanently . 
grey boxes / stars / lines = number / treatment / outcome of no rt patients ; rpe radical prostatectomy , psa prostate - specic antigen , rt radiotherapy , adt androgen deprivation therapy at last contact follow - up 19 of the 28 rt patients remained psa negative , whereas 9 patients had detectable psa . 
six of the rt patients underwent adt : 5 of them received it as long - term treatment beginning in 4 patients before , and in 1 patient after rt . 
all 7 patients who had not received salvage rt were psa positive at last contact with a median psa of 0.79 ng / ml ( range 0.131.73 ng / ml )  . 
while 3 of the 6 patients who were permanently psa negative following rt had never received adt , 2 of them underwent adt for a short period and 1 patient received long - term adt . 
thus , 5 of the initially psa - positive patients returned to undetectable psa levels after rt without being inuenced by adt 446 strahlenther onkol ( 2016 ) 192 : 440448 tab . 
only 14 of 71 psa - negative patients in our cohort ( 20042009 ) received immediate rt similar to aro 96 - 02 [ 3 , 4 ] requiring an undetectable psa prior to rt . 
in clinical practice , salvage rt is frequently thought to be noninferior to immediate adjuvant rt , when conducted as soon as serum psa is detectable [ 1013 , 2327 ]  . 
in the absence of randomized evidence comparing adjuvant with salvage rt , the results of three ongoing randomized trials ( trog 08.03 raves , getug - 17 , and radicals ) are eagerly awaited [ 2830 ]  . as mentioned above , two of the three randomized trials on adjuvant rt ( swog 8794 , eortc 22911 ) included patients with detectable psa levels , thus , representing a subgroup of patients who received rather an early salvage than adjuvant rt . 
a subgroup analysis of aro 96 - 02 patients with persisting psa assessed the impact of psa persistence on efcacy of rt , clinical progression , and os : this subgroup ( 74 patients ) received rt with 66 gy to the prostate bed . 
results showed a signicantly decreased metastasisfree and os compared to postoperative psa - negative patients within this trial [ 31 ]  . in accordance , a detectable psa following rpe in our study was correlated to a diminished cancer - specic survival and higher rate of distant metastases : in this group there were 3 patients with cancer - specic death and distinguishably more patients with distant metastases regardless of whether they received rt ( 5 patients ) or not ( 3 patients )  . 
univariate cox regression analysis strahlenther onkol ( 2016 ) 192 : 440448 conrmed that gs is a signicant predictor for biochemical recurrence and despite excellent efcacy of rt on local control , os is compromised by the concomitant risk of metastatic disease . 
lacking prospective data , gs and presurgery psa levels can help clinicians to decide whether one should opt for adjuvant rt or favor a wait - and - see approach . 
however , in contrast to other studies and risk classications [ 10 , 17 , 34 ] , the present results did not conrm a signicant correlation between preoperative psa levels and risk of biochemical recurrence . 
although rpe was exclusively performed by the same department of urology , further treatment decisions , in particular timing / use of rt and / or adt , were made by different urologists and radiation oncologists in a multireferral systethus , the use of adt and rt was inconsistent , and indeed , many individual treatment decisions remained unclear in retrospective analysis . 
however , in contrast to many other published data the present study contains a central and standardized histopathological workup regarding focality , gleason , and extent of positive margins [ 16 ]  . 
we tried to clarify whether pathological features of r1 may distinguish patients who would most likely prot from adjuvant rt from those who would rather be harmed . in our cohort we did not see any signicant association between pathological features of r1 and the risk of biochemical recurrence . 
again , our results may be hampered by small sample sizes and the high percentage of high - risk patients in our cohort . taken together , the present observational study shows clinical practice of medical care in pt3a n0 r1 patients , particularly the use of rt and adt in a multireferral system between 2005 and 2009 and it provides an insight into prognostic / predictive factors . 
however , up to now clinical decision making about t3 r1 patients who should be opted for immediate adjuvant rt or in whom adjuvant rt could safely be omitted remains difcult . 
bearing in mind that only 20 % of t3 r1 patients received immediate adjuvant rt , but nearly the half of the early psa - negative group suffered from psa relapse resulting in a salvage rt rate of 80 % in this patient subgroup , such patients at a high risk of biochemical or local relapse should be offered adjuvant rt more frequently . conclusion presented data of 94 pt3a n0 r1 prostate cancer patients give insight into clinical practice and underline the need of additive rt for the majority of such patients in order to achieve long - term biochemical control . 
ganswindt state that there are no conicts of interest . this retrospective study was exempt from requiring ethics approval . the bavarian hospital law ( bayerisches krankenhausgesetz ) , 27 data protection ( datenschutz ) , allows the retrospective use of patient data for research , provided that any persons related data remain anonymously . 
whrend die mosaic - studie durch folfox4 auch eine signikante verbesserung des gesamtberlebens zeigen konnte , wurde dieser wichtige sekundre endpunkt durch das 5 - fu - bolusproin kombination mit oxaliplatin in der nsabp tokoll c - 07 - studie nicht erzielt . 
auch die erste auswertung der no16968 - studie zeigte eine wichtige verbesserung des krankheitsfreien berlebens ( dfs ) ( hr 0 , 80 ; p = 0 , 0045 ) im stadium iii des kolonkarzinoms durch eine therapie mit dem oralen fluoropyrimidine capecitabine in kombination mit oxaliplatin ( xelox ) im vergleich zur adjuvanten bolus - 5fu - therapien wie das mayooder roswellpark - protokoll [ 3 ]  . 
die jetzt vororiginalpublikation schmoll hj , tabernero j , maroun j et al ( 2015 ) capecitabine plus oxaliplatin compared with fluorouracil / folinic acid as adjuvant therapy for stage iii colon cancer : final results of the no16968 randomized controlled phase iii trial . 
berichtet ber die langzeitergebnisse der no16968 - studie nach einer medianen beobachtungszeit von 7 jahren , um den stellenwert der adjuvanten xelox - therapie im stadium iii aufzuzeigen [ 4 ]  . 
die intention - to - treat - population der no16968 - studie bestand aus 1886 patienten , die in die beiden arme xelox ( n = 944 ) oder fu / fs ( mayo oder roswell - park , n = 942 ) randomisiert wurden . 
nach einer langen medianen nachbeobachtungszeit von 7 jahren verbessert eine adjuvante chemotherapie mit xelox im vergleich zu fu / fs bei patienten mit kolonkarzinomen im stadium iii sowohl das dfs als auch das os signikant . 
publizierte no16968 - studie belegt eine signikante verbesserung des dfs und os durch die 6 - monatige adjuvante xelox - therapie im vergleich zu fu / fs im stadium iii des kolonkarzinoms . 
obwohl die nebenwirkungsraten der no16986 - studie bereits in zwei publikationen prsentiert wurden [ 3 , 5 ] , htte man sich in der jetzigen publikation mehr daten zu den sptfolgen der durch oxaliplatin induzierten peripheren neuropathie ( pnp ) gewnscht . 
vorgestellten ergebnisse des translationalen begleitprogramms . die niedrige mrna - expression von dihydropyrimidinedehydrogenase in den tumoren ist ein vielversprechender prdiktiver biomarker fr die effektivitt einer adjuvanten xelox - therapie und sollte in weiteren studien retrospektiv und prospektiv untersucht werden . 
dieser biomarker knnte auch fr gruppen von kolonkarzinomen interessant sein , bei welchen eine kombinationschemotherapie bisher nicht indiziert ist ( stadium ii ) oder im einzelfall kritisch gerprft werden sollte , z . 
whrend im uicc - stadium ii des mikrosatelliten - stabilen kolonkarzinoms den patienten eine adjuvante fu / fsoder capecitabin - therapie aufgrund der belegten geringen verbesserungen des dfs individuell empfohlen werden kann , gibt es daher aktuell keine empfehlung fr die oxaliplatin - basierte kombinationschemotherapie im stadium ii . 
obwohl aktuelle metaanalysen mit einschluss von adjuvanten kombinationschemotherapien ( ohne die 5fu - bolus - protokolle ) auch fr ltere patienten > 70 lebenjahre einen prot durch oxaliplatinbasierte kombinationschemotherapie zeigen [ 6 ] , knnen im einzelfall schwerwiegende komorbiditten ein grund dafr sein , die therapie mit hher toxischen adjuvanten protokollen zu berdenken . 
andr t , boni c , navarro m , tabernero j , hickish t , topham c , bonetti a , clingan p , bridgewater j , rivera f , gramont a de ( 2009 ) improved overall survival with oxaliplatin , uorouracil , and leucovorin as adjuvant treatment in stage ii or iii colon cancer in the mosaic trial . 
haller dg , tabernero j , maroun j , braud f de , price t , van cutsem e , hill m , gilberg f , rittweger k , schmoll hj ( 2011 ) compared with uorouracil oxaliplatin plus capecitabine and folinic acid as adjuvant stage iii colon therapy for cancer . 
schmoll hj , tabernero j , maroun j , braud f de , price t , van cutsem e , hill m , hoersch s , rittweger k , haller dg ( 2015 ) capecitabine fluorouracil / folinic acid as adjuvant therapy for stage iii colon cancer : nal results of the no16968 randomized controlled phase iii trial . 
schmoll hj , cartwright t , tabernero j , nowacki mp , figer a , maroun j , price t , lim r , van cutsem e , park ys , mckendrick j , topham c , soler - gonzalez g , braud f de , hill m , sirzn f , haller dg ( 2007 ) phase iii trial of capecitabine plus oxaliplatin as adjuvant therapy for stage iii colon cancer : a planned safety analysis in 1 , 864 patients . 
haller dg , oconnell mj , cartwright th , twelves cj , mckenna ef , sun w , saif mw , lee s , yothers g , schmoll hj ( 2015 ) impact of age and medical comorbidity on adjuvant treatment outcomes for stage iii colon cancer : a pooled analysis of individual patient data from four randomized , controlled trials . 
schller1 received : 27 december 2015 / accepted : 20 april 2016 / published online : 3 june 2016 springer - verlag berlin heidelberg 2016 abstract aim to evaluate the role of magnetic resonance imaging ( mri ) as a predictor for the clinical course in patients with glioblastoma . patients and methods in 64 patients with glioblastoma undergoing ( chemo ) radiotherapy mri studies were obtained before radiation , after 30 gray ( gy ) , after 60 gy and during follow - up . 
in the 64 patients , 5 of the 60 gy mris showed dp / qp after being classied as no change at the 30 gy mri , 2 of the 30 gy mris showed qp , while the 60 gy mri showed tumour regression and 3 fullled the criteria for pseudoprogression during ongoing radiotherapy . 
based on these ndings , early discussion of treatment modication is possible . keywords chemoradiotherapy magnetic resonance imaging radiotherapy prognosis survival analysis magnetresonanztomographien whrend einer glioblastom - strahlentherapie lsst sich die prognose anhand der mrt abschtzen ? zusammenfassung ziel evaluation von mrt ( magnetresonanztomographie ) verlaufskontrollen als prognoseindikator fr patienten mit glioblastom unter laufender strahlentherapie . patienten und methoden mrt - verlaufskontrollen zu verschiedenen zeitpunkten vor beginn der radiotherapie , nach erreichen der hlfte der radiotherapiedosis ( 30 gy ) , bei abschluss ( 60 gy ) und in der nachsorge erhielten 64 zur radio ( chemo ) therapie vorgestellte patienten mit histologisch nachgewiesenem glioblastoma multiforme . 
anschlieend wurden die mrt - befunde ( 3 kategorien : ohne vernderungen , verdacht auf progress [ vap ] , sicherer progress [ sp ] ) mit dem weiteren klinischen und bildgebenden verlauf korreliert . ergebnisse nach 30 gy zeigten 23 von 64 untersuchungen ( 36 % ) ein sp oder der vap ; 41 / 64 ( 64 % ) waren ohne vernderungen im vergleich zum befund vor bestrahlung . nach abschluss der bestrahlung ergab sich bei 26 von 64 ( 41 % ) patienten ein sp ( n = 18 ) oder der vap ( n = 8 )  . 
in 2 der flle mit vap ergab sich im folge - mrt bei 60 gy ein sp ; 5 / 64 60 gy - mrt - kontrollen zeigten sp / vap , nachdem das 30 gy - mrt keine vernderungen ergeben hatte . 
1 table of patient characteristics patients age ( years ) gender histology by treatment radiochemotherapy follow - up ( months ) median range female male total tumour resection partial tumour resection biopsy tomotherapy unit conventional linear accelerator temozolomide other cytostatic drugs median range 2484 290 ten die kriterien fr eine pseudoprogression whrend der laufenden strahlentherapie . 
die 30 - gy - mrt - untersuchungen ermglichen eine prognoseabschtzung : sp / vap haben ein mittleres berleben von 10 , 5 im vergleich zu 20 monaten bei patienten mit befunden ohne vernderung . schlussfolgerung mrt - verlaufskontrollen nach 30 gy whrend der radio ( chemo ) therapie erlauben eine abschtzung der weiteren prognose . 
an eine mgliche pseudoprogression ist zu denken , auch wenn sie im vorgestellten kollektiv selten vorkaauf dieser grundlage kann eine anpassung der therapie diskutiert werden . schlsselwrter glioblastom mrt strahlentherapie pseudoprogress berleben therapy introduction glioblastoma is the most common primary brain tumour in adults [ 1 , 2 ]  . 
a number of prognostic factors are known today , like general patient condition , age ( > / < 65 years ) [ 12 , 13 ] or extent of resection [ 14 ]  . 
also , a correlation between chemotherapeutic effectiveness and o6 - methylguanine - dna - methyltransferase ( mgmt ) status has been demonstrated [ 1518 ]  . the ( postoperative ) radiotherapy uses magnetic resonance imaging ( mri ) to dene the target volumes . 
radiotherapy nowadays is done standardized using 3 d conformal strahlenther onkol ( 2016 ) 192 : 481488 planning with 3 or more beams or also intensity - modulated radiotherapy ( imrt )  . 
for elderly patients or patients in poor performance status hypofractionation is possible . besides playing an essential role for tumour diagnosis and being an indispensable planning tool , mri is also used for posttherapeutic assessment and follow - up . 
with regards to the imaging data , this meant a baseline mr study before radiation treatment , a study after 30 gy and after 60 gy ( as it is the usual imaging practice in our department )  . 
the denition of the gross tumour volume ( gtv ) was based on axial t1 preand postcontrast sequences dening the ( residual ) enhancing tumour or the tumour resection cavity . the gtv was expanded by 2 cm to obtain the clinical target volume ( ctv ) considering anatomic barriers . 
the dose was prescribed according to the international commission on the radiation units and measurements ( icru ) reports 50 , 62 and 83 recommendations . thirty - one patients were treated at a tomotherapy unit ( tomotherapy hi - art ii ) using imrt as radiation technique . 
the other 33 patients received 3d conformal treatment with a conventional linear accelerator ( siemens mevatron md 2 )  . strahlenther onkol ( 2016 ) 192 : 481488 fifty - two patients ( 81 % ) received simultaneous chemotherapy with temozolomide , and 46 continued with this treatment after radiotherapy . 
in 5 patients receiving radiotherapy in 2005 no cytostatic drugs were given . mri studies imaging was performed with a 3.0 tesla system ( intera 3t by philips health care ) using a 8 - channel head coil , a slice thickness of 6 mm and a weight - adapted dose ( 0.1 mmol / kg ) of gadobutrol ( gadovist , bayer ) as contrast mediustudies included transverse sequences ( diffusionweighted echo - planar imaging [ epi ] , uid - attenuated inversion recovery [ flair ] , t2 turbo spin echo [ tse ] , t1weighted spin echo [ se ] [ iv contrast medium ] ) , coronal sequences ( uid - attenuated inversion recovery [ flair ] , t1 - weighted [ + iv contrast medium ] ) and sagittal sequences ( t1 - weighted [ + iv contrast medium ] )  . baseline studies were performed after biopsy or tumour resection ; the median time between this baseline study and the start of radiation treatment was 12 days ( range 040 days )  . 
the mris were independently analyzed by two experienced board - certied radiologists unaware of the clinical outcome . mr ndings of the 30 and 60 gy studies were compared to the baseline study before radiation therapy and assigned to one of three categories : denite progression , questionable progression or no change . 
the criteria to evaluate the mri follow - up after radiotherapy were chosen on the basis of rano criteria [ 19 ] despite the fact that these have been exclusively used for posttherapeutic imaging and not in patients still undergoing therapy . unequivocal tumour growth on mri was classied as denite progression , regardless of the bloodbrain barrier status , this means a tumour with increasing contrast enhancement of more than 25 % , with clear progression of nonmeasurable disease or also new tumour lesions . 
for 13 of those patients ( 62 % ) the status was methylated . in patients with total resection , ( questionable or denite ) disease progression was diagnosed in 10 of 44 patients ( 23 % )  . 
in the group of biopsied patients 6 of 8 ( 75 % ) showed ( questionable or denite ) progression at 30 gy . two of 5 patients ( 40 % ) receiving radiotherapy without chemotherapy were placed in the progression group . comparing follow - up mris with the baseline study revealed the following for the 60 gy study group : in 26 of 64 patients ( 41 % ) disease progression was diagnosed , which was considered denite in 18 patients and questionable in 8 cases . of 64 patients ( 59 % ) 38 were in the no change group . in the progression group the mgmt status of 12 patients was known , with a methylated status in 6 . in the no change group , mgmt promoter methylation status was known for 22 of 38 patients ( 58 % ) , with a methylated status in 13 ( 59 % )  . in 11 of 44 patients ( 25 % ) with total resection , disease progression ( questionable or denite ) was diagnosed in the 60 gy study . 
3 follow - up : mri 3 months after radiotherapy showing denite progression with increasing oedema up was obtained 6 weeks after the end of the radiotherapy and during the further course depending on clinical circumstances and imaging procedures . mgmt promoter methylation mgmt promoter methylation status was known for 34 of 66 patients ( 52 % ) : in 19 of 34 patients ( 56 % ) the tumours showed mgmt promoter methylation , all of these patients were receiving chemotherapy with temozolomide . statistical analysis descriptive statistics were used to describe the baseline characteristics of the patients . 
the starting point was the end of the radiotherapy . comparison between subgroups was done with the logrank test as a nonparametric test to compare the survival distributions of two samples . 
statistical analyses were performed with the excel program . survival curves were calculated using win stat . strahlenther onkol ( 2016 ) 192 : 481488 30 gy 23 progression 15 definite 8 questionable 60 gy 26 progression 18 definite 8 questionable n = 2 n = 1 n = 4 regardless of the time of progression , we found in cases of ( questionable or denite ) progression that the location of progression mostly in - eld of the radiotherapy . 
4 comparing follow - up 30and 60 - gy mri survival analysis median survival overall median survival was 19 months ( range 258 months )  . with methylated mgmt promoter status median survival was 24 months ( range 328 months ) , while in the nonmethylated mgmt promoter status group median survival was 18 months ( range 243 months )  . 
the biopsied patients had a median survival of 7 months ( range 335 months ) , those with subtotal resection a median survival of 10 months ( range 218 months ) and after total resection median survival was 19 months ( range 258 months )  . patients without chemotherapy survived a median of in 13 patients at no 12 months ( range 428 months )  . change was observed until the end of follow - up ( end of study or individual death without proven [ mri ] tumour progression )  . 
6 kaplanmeier analysis of survival of patients with ( questionable ) progression and patients with status idem dened by mri after 60 gy of radiotherapy comparison of 30 and 60 gy mri follow - up revealed the following : in 55 patients ( 86 % ) the ndings at 30 and 60 gy were concordant and categorized in the same group . 
2 survival of the patients with pseudoprogression date of pseudoprogression date of denite progression ( months after completion of radiotherapy ) 30 gy mri 30 gy mri 60 gy mri pseudoprogression survival ( months after completion of radiotherapy ) alive ( follow - up 18 months ) a total of 3 patients fullled the criteria for pseudoprogression at some point during the 30 / 60 gy studies proven by the respective follow - up : two patients showed additional contrast enhancement in the 30 gy mri , and one on the 60 gy study , all of which resolved in the next mri . the mgmt promoter methylation of 2 of these 3 patients was known : 1 patient showed methylated mgmt promoter status , the 1 patient did not . the survival of these patients is shown in tab . 
in the group of patients having no change in the 30 and 60 gy mri , more patients were still alive at the end of the study and this group encompasses more patients with a survival > 15 months , irrespective of the mgmt promoter methylation . 
for the group of methylated mgmt promoter status , we found a signicant lower life expectancy ( p < 0.03 ) for patients with progressive mri compared to those with no change at 30 gy . discussion despite improvements in therapy [ 8 , 2022 ] patients with glioblastoma still have a dismal prognosis [ 23 ]  . 
we analyzed whether it is possible to use the ndings in mris during ( chemo ) radiotherapy as a predictor for the clinical course and for early prognostic stratication of patients . 
if an early mr study would allow such stratication , patients might be identied , in whom therapy might be adjusted / modied early in the course [ 32 ]  . until now the incidence of progress during ongoing radiotherapy based on mri ndings is unclear . 
with 20 months median survival in the 30 gy unchanged group , and 8 months survival in the 30 gy denite progression group , this difference was quite pronounced . a signicant difference is also seen between the unchanged 20 months median survival and the questionable progression group , which had a median survival of about 11 months . 
while this is also signicant , it has to be realized that this group also encompasses patients with pseudoprogression , in whom a change in therapy would be undesirable . median survival in the questionable progress groups ( excluding pseudoprogression patients ) at 30 gy vs 60 gy were 10 months and 18 months respectively . 
this could be explained by the small sample size of only 8 patients in this subgroup showing a substantial change in categorization from 30 to 60 gy . it is important to be aware of pseudoprogression and radionecrosis , which may mimic real progression , and therefore potentially might cause overor undertreatment [ 3436 ]  . in our 30 / 60 gy patients pseudoprogression was only seen in the group with questionable progress . 
thus , a mr study showing denite progress at 30 gy allows for risk stratication . a follow - up mri is needed in case of questionable progress to exclude pseudoprogression before modications of therapy can be discussed . 
if other mr techniques or nuclear medicine procedures can help with this distinction and obviate the need for a follow - up mri cannot be decided at this time . our data is limited by number and heterogeneity of the patients . 
in biopsied patients the percentage of patients with progression during radiotherapy was particularly high . there were also differences among patients in chemotherstrahlenther onkol ( 2016 ) 192 : 481488 apy regime and mgmt promoter methylation status which was only known for nearly half of the patients . 
this may justify modications in therapy if these data are conrmed on a larger prospective scale . the decision about therapy modication must be made individually and in cases of substantial changes this should be subject of controlled clinical studies . 
adaption / optimization of the eld size to reach all tumour regions and intensication of therapy by adapting the radiation dose to progressive areas are further options . conclusion it is possible after 3 weeks of ( chemo ) radiotherapy to make a preliminary estimation of the individual prognosis for patients with glioblastoma on the basis of a mri criteria . those patients with a progressing tumour at this point in time have a signicantly shorter life expectancy . in patients with questionable progression a follow - up mri is required to differentiate progress from pseudoprogression . therefore , in these cases therapeutic modications may be implemented only after a follow - up mri . compliance with ethical guidelines conict of interest c . 
merseburger5 jens vogel - claussen6 hans christiansen1 thorsten derlin3 received : 1 march 2016 / accepted : 20 april 2016 / published online : 7 june 2016 springer - verlag berlin heidelberg 2016 abstract purpose the goal of this work was to evaluate the early efcacy of 68ga - psma ligand pet / ct imaging for radiotherapy of locally recurrent and / or oligometastatic prostate cancer . patients and methods a total of 29 patients with biochemical recurrence received a 68ga - psma ligand pet / ct for restaging of disease , followed by 3d conformal radiotherapy of metastases or intensity - modulated radiation therapy of the prostate bed . 
prostate - specic antigen ( psa ) levels and imaging procedures served as the reference standard to assess the treatment efcacy . results pet / ct was positive in 96.6% of patients and revealed that 13.8% of patients had locally recurrent disease , 58.6% had isolated lymph node metastases , 20.7% had isolated bone metastases , and 3.4% showed lymph node metastases and a vertebral metastasis . 
3 , 85748 garching , germany 5 department of urology , university hospital schleswig - holstein , campus lbeck , ratzeburger allee 160 , 23538 lbeck , germany 6 department of radiology , hannover medical school , carl - neuberg - str . 
1 , 30625 hannover , germany 432 strahlenther onkol ( 2016 ) 192 : 431439 conclusion preliminary results in the presented cohort suggest that radiotherapy based on 68ga - psma ligand pet / ct yields effective local control and signicant treatment response in terms of psa levels in the absence of clinically important side effects . 
psa - werte und bildgebungsresultate dienten als referenzstandard zur beurteilung der frhen effektivitt . ergebnisse das psma - pet / ct zeigte bei 96 , 6% der patienten eine pathologische tracer - bindung , 13 , 8% der patienten hatten ein lokalrezidiv der prostataloge , 58 , 6% isolierte lymphknotenmetastasen , 20 , 7% isolierte knochenmetastasen und 3 , 4% pelvine lymphknotenmetastasen sowie eine singulre wirbelkrpermetastase . 
darber hinaus trat bei keinem patienten eine verschlechterung der harnoder stuhlkontinenz auf . schlussfolgerung nach 68ga - psma - liganden - pet / ct - basierter strahlentherapie zeigten sich eine effektive lokale kontrolle und ein signikantes psa - ansprechen , klinisch in the context of biochemical recurrence after primary therapy for prostate cancer , e . 
g. locally recurrent and oligometastastic prostate cancer , the diagnostic accuracy of conventional imaging modalities such as transrectal ultrasound , computed tomography ( ct ) and magnetic resonance ( mr ) imaging is still considered suboptimal in the management of these patients [ 1 ]  . 
clinical molecular imaging by positron emission tomography ( pet ) using choline - based radiotracers for radiation treatment planning , which has a pooled sensitivity and a specicity > 85% for diagnosis of bone metastases [ 2 , 3 ] but only a sensitivity of approximately 62% for lymph node metastases from prostate cancer , has shown unsatisfactory accuracy for detection of small metastases [ 4 , 5 ]  . a substantial number of patients relapse within 10 years after primary therapy , and precise information about the site of recurrence is crucial to distinguish between local recurrence , oligometastatic and extensive disease [ 6 ]  . 
patients with local recurrence [ 7 ] and patients with a limited number of metastases , so - called oligometastatic patients , have a much better prognosis than patients with extensive metastatic disease , as the oligometastatic cancer state is considered to be an intermediate state of tumour spread with limited metastatic capacity and less aggressive behaviour [ 8 ]  . 
in analogy with other solid tumours , eradication of these tumour manifestations by means of metastases directed therapy ( mdt ) with radiotherapy is an emerging way to delay disease progression and postpone systemic treatment without major treatment toxicity [ 9 ]  . 
the identication of these patients is challenging due to the lack of sufciently sensitive imaging for detection of low - volume , locally recurrent and metastatic disease at low psa levels [ 8 ]  . the potential roles of pet / ct in radio - oncology are patient selection for treatment and target volume denition [ 1 , 6 ]  . 
prostate - specic membrane antigen ( psma ) ligands for pet / ct have recently gained increased interest as a novel diagnostic approach to improve the detection of metastases and selection of prostate cancer patients [ 10 ]  . 
68ga - psma ligand pet / ct has been reported to have substantially higher senstrahlenther onkol ( 2016 ) 192 : 431439 sitivity for the detection of metastatic lesions in recurrent prostate cancer than choline - based pet / ct , particularly in the case of lymph node metastases [ 10 , 12 ]  . 
however , data on the effectiveness of psma ligand pet / ct - based radiation treatment are very limited . here , we report on the early efcacy of 68ga - labelled psma ligand pet / ct - guided 3d conformal radiotherapy or intensity - modulated radiation therapy ( imrt ) in prostate cancer patients with locally recurrent or oligometastatic disease . patients and methods study population between august 2014 and june 2015 , 29 patients with a history of prostate cancer and continuously increasing psa levels after primary curative therapy received a 68gapsma ligand pet / ct and were subsequently treated with radiotherapy . 
the psa threshold to perform a 68ga - psma ligand pet / ct was 0.3 ng / ml and all scans were performed for clinical indications according to 13.2b of the german pharmaceutical act . 
all cases were discussed and approved for radiotherapy by the local multidisciplinary uro - oncologic teaa total of 26 ( 89.8% ) patients had high - risk cancer , 1 ( 3.4% ) had intermediate and 2 ( 6.8% ) presented with low - risk cancer . 
this retrospective study complied with the regulations of the local institutional review board and the principles of the declaration of helsinki . staging staging included physical examination with digital rectal palpation , complete laboratory tests , 68ga - psma ligand pet / ct and mri of the pelvis in the case of local pelvic recurrence . psma - targeting ligand synthesis and pet / ct imaging 68ga - psma i&t [ 13 ] was synthesised by a fully automated , well - manufactured practice - compliant procedure using a grp module ( scintomics gmbh , frstenfeldbruck , germany ) connected to a 68ge / 68ga generator ( 30 mci obninsk generator , eckert & ziegler eurotope gmbh , berlin , germany ) and equipped with a disposable single - use cassette kit ( abx , radeberg , germany ) [ 14 ]  . 
before application , the radiopharmaceuticals were analysed according to the monographs 2462 ( gallium chloride ) and 2482 ( gallium edotreotide ) of the european pharmacopoeia , including analytic high - performance liquid chromatography . 
radioanalytic high - performance liquid chromatography was performed on a varian prostar high - pressure gradient system equipped with a uv / vis detector ( varian prostar 335 ) and a radiodetector ( berthold lb 3800 - 20 with lb 6657 probe ) using an rp - 18 column ( gemini c18 5 110 a , 250 x ; phenomenex , torrance , ca , usa )  . 
imaging started with a low - dose nonenhanced helical ct ( 120 kv , ma modulated , pitch 1.2 , reconstructed axial slice thickness 5.0 mm ) performed for attenuation correction of pet acquisitions . 
whole - body pet images were then acquired in all patients using continuous bed motion ( cbm ) at a speed of 0.9 mm / s for chest and abdomen and 2.1 mm / s for legs at 60 min p . 
visual assessment of focally increased tracer uptake higher than the surrounding background was used as criterion for malignancy . high focal uptake in the prostate region was considered to be recurrent disease . 
peak standardised uptake values ( suvpeaks ) were used for semiquantitative assessment of tracer uptake within malignant lesions . radiotherapy treatment planning was conducted with masterplan ( nucletron , the netherlands )  . image fusion was performed using the masterplans mutual information algorithpa434 strahlenther onkol ( 2016 ) 192 : 431439 tients were treated ve times weekly with 2.0 gray ( gy ) up to a dose of 66.0 gy using imrt in the case of local recurrence in the prostate bed . 
the pathological ndings in the planning ct , the low - dose ct of the 68ga - psma ligand pet / ct and the mri in cases of pelvic irradiation were dened as the gross target volume ( gtv ) , whereas the area with the pathological tracer uptake was dened as the clinical target volume ( ctv )  . 
the planning target volume ( ptv ) included the ctv plus a 10 mm safety margin in all directions to account for setup errors . in cases of pelvic lymph node irradiation , only the lymph node area with the increased tracer uptake without the whole ipsilateral lymphatic drainage was irradiated . cases of a 68ga - psma ligand pet / ct proven local relapse in the prostatic bed , the ctv only included the focal pathological tracer uptake . image guidance was conducted twice a week with a megavoltage cone beam ct ( cbct )  . 
late side effects were dened as persisting after more than 90 days following treatment and were assessed using the lent - soma scale [ 16 ]  . periodical urological follow - up , which included prostate - specic antigen ( psa ) measurement , was performed every 3 months . 
increased psa levels above baseline warranted a bone scan , as well as new 68ga - psma ligand pet / ct for staging purposes . if there was no increase in psa , no imaging was conducted . 
in cases of new metastases , a systemic therapy of the urologists choice or local therapy was initiated . statistical analysis outcomes were dened from the last day of irradiation . kaplanmeier curves were used to estimate the biochemical relapse - free survival ( brfs ) and distant disease - free survival ( ddfs )  . 
both gleason grading ( rs = 0.44 , p = 0.002 ) and psa levels at the time of pet / ct imaging ( rs = 0.40 , p = 0.0009 ) demonstrated a signicant correlation with maximum suvpeak . 
they declined androgen deprivation therapy ( adt ) and instead chose para - aortic lymph node irradiation . strahlenther onkol ( 2016 ) 192 : 431439 table 1 patient and tumour characteristics ( years ) stage gleason ipsa pet / ct dt . 
left iliac and right pubic bone stage initial tumour stage , ipsa initial psa value ( ng / ml ) , psa nadir minimal psa value after primary therapy ( ng / ml ) , dt . 
3. no grade iii acute toxicity according to ctcae or late toxicity grade ii according to lent - soma was observed . in patients with bone metastases , neither early nor late tox436 strahlenther onkol ( 2016 ) 192 : 431439 oration of urinary or faecal continence was not observed in any patient . discussion in locally recurrent and oligometastatic prostate cancer , the diagnostic accuracy of imaging for disease location has been dramatically improved by the introduction of psma ligands for pet / ct , which have recently been introduced 68ga - psma ligand pet / ct outinto clinical routine . performs all other imaging modalities , including cholinelow psa levels in previously published based pet at it is crucial in patients with increasing series [ 10 , 12 ]  . psa levels after primary therapy for prostate cancer to obtain precise information about the site of recurrence to distinguish between local recurrence , oligometastatic , and extensive disease [ 6 ]  . 
patients with local recurrence [ 7 ] and oligometastatic patients are characterised by a much better prognosis than patients with extensive metastatic disease , as the oligometastatic cancer state is considered to be an intermediate state of tumour spread with limited metastatic capacity and less aggressive behaviour [ 8 ]  . 
furthermore , patients with a single lesion have a 5 - year prostate cancer - specic survival rate of 90% , compared to only 32% in patients with two or more metastases in analogy with other solid tumours , eradication of these tumour manifestations by means of mdt with radiotherapy is an emerging way to delay disease progression and postpone systemic treatment without major treatment - associated toxicity [ 8 ]  . 
2 solitary bone metastasis in the left iliac bone ( arrow ) of a 66 - year - old man with biochemical recurrence from prostate cancer ( a axial ct image ; b fused pet / ct image )  . 
the 9 - month brfs and ddfs were 100% and the estimated 12 - month survival was 75% that emphasises the high importance of exact imaging and staging to tailor the individual treatment . 
although exact data on sensitivity and specicity of psma ligand pet are still lacking , psma ligand pet showed a high correlation with histopathological ndings [ 18 ] and is more sensitive than ct - based 3d volumetric lymph node assessment in patients with recurrent prostate cancer [ 19 ]  . 
 [ 21 ] recently showed that a psa of 0.83 ng / ml and a psa doubling time of 6.5 months were optimal cut - off values for psma ligand pet / ct staging in recurrent prostate cancer . 
therefore , we assume that staging by psma ligand pet / ct was reliable , which is also supported by the signicant treatment response , as evidenced by the decrease in psa levels . furthermore , in our study of 29 patients , we showed that 68ga - psma ligand pet / ct guided radiotherapy represents a promising treatment option in patients with rising psa levels and local recurrent or oligometastatic prostate cancer . in patients with bone metastases ( 8 of 29 patients ; 27.6% ) adt was continued after denitive therapy of prostate cancer during and after radiotherapy as adt is the backbone of metastatic and nonmetastatic castration - resistant prostate cancer ( crpc ) therapy and should be maintained when crpc develops , although no prospective trial has shown a survival benet in metastatic prostate cancer [ 22 ]  . 
none of the 8 patients showed biochemically progressive disease until their last follow - up visit ; thus , adt was continued and no chemotherapy or treatment with abiraterone has so far been necessary . 
in addition , we showed a favourable riskbenet ratio as no grade iii acute toxicity according to ctcae or late toxicity grade ii according to lent - soma was observed . 
only two patients ( 6.8% ) reported on persistent grade i diarrhoea according to the lent - soma criteria 3 months after radiotherapy , whereas patients who received radiotherapy of bone metastases reported neither on any acute nor late toxicities . 
in addition , deterioration of urinary or faecal continence was not observed in any patient . although external beam radiotherapy ( ebrt ) is a wellestablished salvage therapy in biochemical recurrent prostate cancer after prostatectomy , the exact localisation of biochemical recurrence remains difcult and salvage ebrt provides better response if initiated below psa levels of 1 ng / ml [ 23 ]  . 
unfortunately , this therapy fails particularly among patients with a high - risk constellation , and their overall death rate is signicantly higher than in patients 438 strahlenther onkol ( 2016 ) 192 : 431439 where therapy did not fail [ 24 ]  . 
this suggests that psma ligand pet / ct , with its excellent detection rate of prostate cancer lesions in psa levels less than 1 ng / ml [ 21 ] , can overcome the problem of staging uncertainties and might result in a lower failure rate in salvage radiotherapy after prostatectomy , thus improving the clinical outcome . with regard to the biochemical response , we observed a statistically signicant decrease ( p < 0.001 ) of the psa levels prior to radiotherapy compared with psa levels at the last follow - up visit . 
this fact also implies that reduction in tumour burden , as widely accepted for several cancer entities , improves the clinical outcome and inuences the pathway of systemic therapy [ 25 , 26 ]  . in cases of isolated lymph node metastases , there is also the option to perform a salvage lymph node dissection of the pelvis with [ 27 , 28 ] or without [ 29 ] adjuvant radiotherapy . complications of this surgical metastasis directed approach are bleeding , infection , ileus , hydronephrosis and drainage requiring lymphocele [ 30 ]  . 
to the authors best knowledge , no prospective studies comparing lymph node dissection with radiotherapy have been published . several studies reported good local control rates in oligometastatic prostate cancer [ 4 , 6 , 3135 ]  . 
 [ 33 ] in a series of patients with bone lesions treated with image - guided robotic radiosurgery . there are several reports of inhomogeneous study populations with lymph node metastases and / or simultaneous or metachronous bone metastases in which some of the lesions were irradiated twice if there was a local recurrence within the irradiated volume [ 4 , 3134 ] , whereas there are few studies reporting on radiotherapy of isolated lymph node metastases [ 31 , 35 ]  . 
they reported a 3 - year local control rate of 90% , which seems to conrm our therapeutic approach of pelvic lymph node irradiation without lymph node dissection prior to radiotherapy . there are uncertainties concerning the biologically optimal radiation dose due to the absence of a reliable radiobiological dose model for lymph node metastases in prostate cancer . 
the authors conclusions were cautious about achieving clinically important increases in local tumour control rates with this mathematical approach . some limitations of this analysis should be mentioned . first , due to the retrospective nature of the study , a selection bias cannot be ruled out . 
third , we presented a cohort with a high percentage ( 89.8% ) of high - risk constellations , which represents a selected cohort with high risk of recurrent disease . 
however , the observed early efcacy of psma ligand pet - guided radiotherapy is promising , and efcacy data have not been previously reported in the context of 68ga - psma ligand pet - based radiation treatment . conclusion in this retrospective study , we showed that 68ga - psma ligand pet / ct - guided radiotherapy in locally recurrent and oligometastatic prostate cancer delayed clinical progression , thus delaying the start of systemic treatment . 
hswbrt plans of coplanar vmat for each ct set were generated with a prescribed dose of 30 gy in 10 fractions . maximum dose to the hippocampi was limited to 16 gy ; to the optic nerve , optic chiasm , and eyeballs this was conned to less than 37.5 gy ; for the lenses to 8 gy . 
die hs474 strahlenther onkol ( 2016 ) 192 : 473480 wbrt - plne mit koplanarer vmat enthielten fr jeden ct - datensatz eine vorgeschriebene dosis von 30 gy in 10 fraktionen . 
die maximale dosierung des hippokampus war auf 17 gy , fr sehnerv , sehnervenkreuzung und augapfel war die dosierung auf 37 , 5 gy und fr linsen auf 8 gy begrenzt . 
11 geneigtem kopf fhrt im vergleich zum gerade positionierten kopf zu einer besseren ptv - dosisverteilung und reduziert die dosisbelastung in hippokampus und optischen sehorganen . schlsselwrter intensittsmodulierte strahlentherapie risikoorgane berleben kognitive funktionen metastasen neural stem cells of the hippocampus play an important role in memory function . 
during radiation therapy ( rt ) to the brain , the dose of radiation to the hippocampal area is known to be associated with reduced cognitive and memory function [ 13 ]  . 
recently reported outcomes of the radiation therapy oncology group ( rtog ) 0933 trial , a phase 2 trial including 113 patients with brain metastases treated with hippocampal - sparing whole brain radiotherapy ( hswbrt ) , showed promising results in preserving memory function as compared to historical data [ 4 ]  . 
several rt techniques have been used in hs - wbrt , including linear accelerator - based intensity - modulated radiotherapy ( imrt ) and helical tomotherapy [ 2 , 5 , 6 ]  . 
volumetric modulated arc therapy ( vmat ) uses a dynamically - modulated gantry arc rotation of up to 360 degrees to deliver a conformal threedimensional ( 3d ) dose distribution within a short period of time [ 7 , 8 ]  . 
reported that a head position inclined to 30 degrees could optimize coplanar whole brain imrt treatment , thereby obviating the need for timeconsuming non - coplanar imrt plans [ 10 ]  . 
the ct scans were acquired using a brilliance ct big boretm ct simulator ( philips , cleveland , oh , usa ) with a slide thickness of 2 mm . target contouring all ct image sets were incorporated to the eclipsetm ( varian medical systems , palo alto , ca , usa ) version 10.1 treatment planning systeall patient ct images were fused with the most recent magnetic resonance ( mr ) images . 
the planning target volume ( ptv ) was dened as the whole brain volume excluding the hippocampal avoidance region , which was obtained by expanding the hippocampus by 5 mthe lenses , eyeballs , optic nerves , and optic chiasm were also delineated . strahlenther onkol ( 2016 ) 192 : 473480 fig . 
axial , coronal , and sagittal images were displaced from top to bottothe hippocampi were contoured with a blue line for comparison of dose distribution between inclined head position and non - inclined head position hs - wbrt plans , non - inclined head images were generated by articially rotating the ct images of the 8 patients using customized matlabtm ( mathworks , inc . , natick , ma , usa ) programming . 
this procedure has already been used in a previous study by lee et al . [ 12 ] , who compared the dosimetric parameters of the lung stereotactic ablative rt plan of an articially rotated ( roll radiation 13 ) image using the same method . 
regarding the mathematical procedure , because the pixel sizes in the three directions were not identical , three - shear operation was used to rotate the image [ 13 ]  . 
the dose received by 98 % of the ptv ( d98% ) was set to at least 25 gy , and the dose received by the most irradiated 2 % ( d2% ) was limited tab . 
1 planning targets parameter hippocampus lenses optic apparatus ( optic nerves , optic chiasm , eyeballs ) planning goal v30 gy 90 % d2 % < 40 gy d98 % 25 gy maximum dose < 16 gy maximum dose < 8 gy maximum dose < 37.5 gy ptv planning target volume , v30gy volume of the ptv receiving 100 % of the prescribed dose , d2% dose received by the most irradiated 2 % of the ptv , d98% dose received by 98 % of the ptv 476 strahlenther onkol ( 2016 ) 192 : 473480 to 40 gy . 
the gantry rotation speed and monitor units ( mu ) per gantry angle degree were optimized for a variable dose rate plan with a maximum dose rate of 600 mu / mthe progressive resolution optimizer 3 ( pro3 , ver.10 , varian medical systems ) was used for optimization . 
for dose calculation , the anisotropic analytic algorithm ( aaa , ver.10 , varian medical systems ) was used with a dose calculation grid of 1 mall 16 plans were normalized to cover 90 % of the target volume with 100 % of prescription dose ( v30gy = 90 % )  . mum dose delivered to 2 % of the target volume ( d2% ) minus the dose delivered to 98 % of the target volume ( d98 % ) divided by the median dose of the target volume ( d50 % ) : hi = ( d2% - d98% ) / d50% . 
conformity index ( ci ) was dened as ci = vri / tv , where tv is the target volume and vri is the target volume covered by the reference isodose [ 15 , 16 ]  . the dose difference between these two positions was evaluated as a percent change of inclined position compared to the non - inclined position ( [ dose of inclined position dose of non - inclined position ] / dose of non - inclined position )  . 
dose homogeneity was quantied in terms of homogeneity ( hi ) , as recommended by the international commission on radiation units and measurements [ 14 ] and as used by hsu et al . 
the hi was dened as the maxito assess the setup accuracy of the inclined head position , the weekly setup shifts of 8 patients with an inclined head position were compared to those of another randomly chosen 6 patients with a non - inclined head position . 
the population systemic error was dened as the standard deviation of the individual systemic error , and the population random error was dened as the standard deviation of the individual random error [ 17 ]  . results inclined head angle the median age of the patients was 53 years ( range 2676 years ) and 4 patients ( 50 % ) were male . 
each image was rotated 0 , which was the head angle of the non - inclined head position , to generate an image for use in comparison . whole brain ptv coverage detailed dosimetric parameters are listed in tab . 
the non - coplanar imrt technique can provide an acceptable plan for hs - wbrt ; however , conventional nineeld non - coplanar imrt treatment increases not only the treatment time , but also the possibility of delivery errors because of multiple couch movements . 
arc therapy , such as helical tomotherapy or vmat , is advantageous because of its short treatment delivery time , which may be particularly important for the treatment of patients who are physiologically compromised ( such as those with brain metastases )  . 
by analogy to the procedure proposed by siglin et al . , we hypothesized that an inclined head position might also be benecial for coplanar vmat . in the coplanar vmat planning of hs - wbrt , constraint of the dose to the optic apparatus was sometimes considered to be a difcult goal [ 79 , 1821 ]  . 
for better dose distribution , vmat plan techniques other than coplanar vmat plans were recently reported to use multiple non - coplanar arcs or partial - eld arc techniques [ 19 , 21 ]  . 
however , these studies reported high hippocampi dmax values of around 20 gy , or higher dose constraints for the lenses . if the eyeball lies within the coplane of the ptv in the brain parenchyma , a substantial dose of rt to the lenses cannot be avoided when using coplanar arc therapy . 
moreover , when the head is not inclined , the eyeballs and the hippocampi were collated on the same plane , which is an obstacle when optimizing the vmat plan . 
in the current study , the volume of ptv positioned within the same plane as the eyeball could be reduced by inclining the head , resulting in a low dose to the hippocampi and optic apparatus . moreover , the inclined position could generate a more homogeneous radiation dose in the ptv , which guarantees a more uniform dose distribution with an eventually decreased complication rate [ 22 ]  . unlike the study by siglin et al . , in which inclined head positions were articially generated by ct images , the current study took ct simulation images with an inclined head position and then generated non - inclined head position images by articially rotating the images . 
although siglins group reported that a 30 - degree head angle produced an optimal dose distribution in hs - wbrt with coplanar imrt , inclining the head during treatment could cause several problems . 
for rt of primary brain tumor , inclining the head position in the coplanar vmat planning could be more benecial : according to the location of the lesion , clinical targets may be better separated from critical structures by inclining the head than they would be in hs - wbrt , where the clinical target volume is the whole brain our institution , hippocampal sparing with an inclined head position using coplanar vmat has been a routine procedure during rt to the primary brain tumor since january 2014 . 
however , considering the nature of the intracranial structures , rotating and registering the structure with the same angle and not recontouring on additionally taken ct images could facilitate exact comparison between the two positions . conclusion an inclined head position of around 11 produced a better dose homogeneity in the ptv and lower doses to the hippocampi and optic apparatus than with a non - inclined head position during hs - wbrt using coplanar vmat . 
clinical usability and functional outcome of this strategy should be further investigated . acknowledgements this work was supported by the grant ( #0820010 ) for cancer control program from korean ministry of health & welfare to in ah kim . compliance with ethical guidelines conict of interest k.s. 
kim state that there are no conicts of interest . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
all patients were treated using interstitial pdr brachytherapy with dose specications according to the paris systefor data collection of erectile dysfunction , the international index of erectile function questionnaire was used , supplemented by the follow - up data . results the median follow - up was 54.0 months ( range , 13155 months )  . 
at the time of analysis , nine of 13 men were alive ; two of 13 men died of distant metastases from the tumor and two for other reasons with no sign of cancer disease . 
eight of 11 men ( 72.7 % ) never or only sometimes had erectile dysfunction . conclusion in selected patients , interstitial pdr brachytherapy of penile cancer is effective as an organ - sparing treatment . 
it yields satisfactory results for the conservation of sexual function . keywords penile cancer brachytherapy erectile dysfunction surgery , conservative survival organschonende behandlung beim peniskarzinom mittels interstitieller pulsed - dose - ratebrachytherapie zusammenfassung ziel analyse der ergebnisse von 13 patienten mit plattenepithelkarzinom des penis , die mittels protokollbasierter interstitieller pulsed - dose - rate - ( pdr ) - brachytherapie behandelt wurden . patienten und methoden von august 2002 bis februar 2014 wurden 13 mnner mit peniskarzinom mittels brachytherapie behandelt . 
es verstarben 2 / 13 mnner am tumor durch fernmetastasen und 2 krankheitsfrei aus anderen grnden . ernsthafte spte nebenwirkungen wie weichteilnekrosen traten in 4 / 13 fllen ( 30 , 8 % ) auf und wurden alle erfolgreich medikaments behandelt . 
insgesamt 8 / 13 mnnern ( 61 , 5 % ) hatten niemals oder nur manchmal eine erektile dysfunktion . schlussfolgerung bei ausgewhlten patienten ist die interstitielle pdr - brachytherapie bei peniskarzinom eine effektive , organschonende behandlung . 
sie kann zufriedenstellende resultate in der erhaltung der sexualfunktion erzielen . schlsselwrter peniskarzinom brachytherapie erektile dysfunktion konservative chirurgie berleben virus ( hpv ) , of which hpv - 16 has the biggest share [ 13 , 19 ]  . 
most commonly , the glans is affected [ 17 ]  . surgical therapy in the form of total or partial penectomy is most often chosen as the method of treatment [ 2 , 6 ]  . 
as a consequence , for the majority of patients , radical surgery has a major and disastrous impact on their sexuality and on patient satisfaction , leading to a dramatically reduced quality of life . 
it is reported that the risk of suffering from depression or anxiety disorders is increased for these patients [ 10 ]  . brachytherapy is a proven and very effective treatment modality in different tumor entities [ 16 , 18 , 25 ]  . 
hence , interstitial brachytherapy as an organand function - sparing therapy is an excellent alternative treatment modality in early stages of penile cancer , as is also specied in european guidelines [ 11 ]  . 
the incidence in europe and north america is less than 1 : 100 , 000 with an increased risk starting from the sixth decade of life and a peak at 68 years of age [ 1 , 3 , 20 ]  . 
it has been reported that 3040 % of cases are associated with the human papilloma patients and methods we reviewed the clinical records of 13 patients with penile cancer treated from august 2002 to february 2014 in our hospital exclusively with interstitial pulsed - dose - rate ( pdr ) brachytherapy . 
for the majority of patients , magnetic resonance imaging ( mri ) was performed before brachytherapy to verify precisely the size of the tumor and particularly the depth of invasion . consequently , gross tumor volume ( gtv ) was identied using inspection , palpation , and mri . 
two patients being treated for recurrence received 22 and 24 pulses and a total dose of 10 and 12 gy as boost on the glans penis in addition to external beam radiation therapy ( ebrt )  . 
we sent this questionnaire to all patients still alive or asked them to ll it out in the context of a follow - up appointment . statistical analysis the kaplanmeier method was used for cumulative local recurrence rate , disease - free survival rate , cancer - specic survival rate , and overall survival rate . 
of these two , one patient with lymph node involvement had recurrence after 35 months . it was the only local failure in this study . in the other patient , metastases developed 4 months after brachytherapy . 470 strahlenther onkol ( 2016 ) 192 : 467472 tab . 
this corresponds to grade 2 radiation dermatitis . late side effects in four of 13 patients ( 31 % ) , soft tissue necrosis occurred during the follow - up , but conservative treatment with medication ( pentoxifylline , ciprooxacin , and prednisolone ) was successful in all cases . 
thus , mutilating salvage surgery was not necessary in any of the cases ( 0 / 13 , 0 % )  . in two patients ( 2 / 15 , 15 % ) , a urethral stenosis was diagnosed and dysuria occurred in four cases ( 4 / 13 , 31 % )  . during follow - up care , scarring and various other sequelae occurred . 
in addition , a number of other changes were detected : two patients got scar stretching ; three patients ( 23.1 % ) , telangiectasia ; one patient , hyperpigmentation ; and one patient , superinfected scars . the results of the questionnaire with parts of the iief were combined with the data from the current follow - ups . 
four patients indicated that they had no problems with erectile function , while 2 patients reported a limited capability to get an erection and one patient reported using viagra as an aid . 
four of 13 patients ( 30.7 % ) reported having severe erection problems and thus suffered from erectile dysfunction . discussion it is obvious that our study with only 13 cases , one of the smaller studies , can provide only limited statements . 
unsurprisingly , our study conrms the published recent trends in the therapy of penile carcinomas . regarding brachytherapy of penile cancer , four studies with a median follow - up of more than 4 years were carried out within the past 6 years [ 4 , 7 , 14 , 21 ]  . 
in the [ 4 ] , studies of de crevoisier et al . the 5 - year local control rate was 80 and 88 % , respectively . kamsu - kom et al . 
thus , a comparison of these studies is difcult and only tendencies can be sketched . in this context , our study conrms that patients with stage t1 or t2 disease without lymph node involvement have a very good prognosis and the results of sole interstistrahlenther onkol ( 2016 ) 192 : 467472 tial pdr brachytherapy are excellent . 
kamsu - kom et al . reported that the treated volume signicantly correlated to the risk of clinically relevant delayed toxicity [ 14 ]  . in our study , the number of implanted needles for the patients with necrosis was the same as the average of all patients . 
it is reported that the risk of urethral stenosis increases signicantly and is associated with the irradiation volume and the number of implanted needles [ 5 ]  . in most cases , there are reports about long - term changes in the skoften brosis is caused in the places of the implanted needles . 
in the studies of kilite et al . [ 21 ] , the proportion of cases of telangiectasia was eight of 25 and 14 of 25 , respectively . [ 15 ] and pimenta et al . although functional integrity is one of the main intentions of brachytherapy , there are few studies on the effect of brachytherapy on sexual function . 
of 17 patients who were sexually active before brachytherapy , there were 10 still active postoperatively . in our study , seven of 11 patients were capable of erection at the time of the last follow - up or when sending the iief questionnaire . 
of the four patients with severe erectile dysfunction , this was appropriate for age in one patient . our results are limited not only because of the small number of patients . 
further limitations are that the surveys refer solely to the postoperative condition , that four patients had already died at the time of analysis , and that not all patients returned the questionnaires . 
conducted a meta - analysis and a review of the literature [ 12 ]  . overall , 1 , 505 patients were treated with penectomy and 673 patients with brachytherapy in 19 studies . 
and the 5 - year local control rate was 84 % for penectomy and 79 % for brachytherapy . especially in early tumors as t1 , and t2 without nodal involvement , there was no signicant difference between the treatment results in early tumor stages . 
compared with surgical methods , brachytherapy provides a maximum of organ preservation and functional integrity . acknowledgments the present publication was performed in fulllment of the requirements for obtaining the degree med . 
this study aimed to investigate the toxicity of hypofractionated stereotactic radiotherapy ( sbrt ) and qol after treatment in localized prostate cancer patients . materials and methods a prospective single - center clinical study was performed in lowand intermediate - risk prostate cancer patients . 
neoadjuvant androgen deprivation therapy was given to 52 patients ( 76.5 % ) , and stopped in 31 patients ( 45.5 % ) after 6 months ; in 21 patients ( 31 % ) after 23 years . 
average and median follow - up was 24 months ( cid : 2 ) monika rucinska m_rucinska@poczta.onet.pl 1 department of oncology , university of warmia and mazury in olsztyn , olsztyn , poland 2 department of radiation oncology , independent public health care facility of the ministry of the interior with warmia and mazury oncology centre in olsztyn , wojska polskiego 37 , 10 - 228 olsztyn , poland polish association of cognitive and behavioural therapy , minds of hope , warsaw , poland 4 department of oncology and radiotherapy , medical university of silesia , katowice , poland ( 1845 )  . 
global health status / qol was good and improved during the observational period . conclusion sbrt for prostate cancer patients is a welltolerated treatment in terms of toxicity and qol , has no negative impact on functioning and everyday life , with the important benet of a short treatment period . 
however , long - term follow - up data are needed . keywords hypofractionated stereotactic radiotherapy quality of life rectum bladder organs of risk hypofraktionierte stereotaktische radiotherapie sharp ist eine gut tolerierte behandlung beim prostatakarzinom beurteilung der toxizitt und lebensqualitt zusammenfassung hintergrund die lebensqualitt ( qol ) ist zu einem der wichtigsten schwerpunkte bei der wahl der prostatakarzinombehandlung geworden . 
das thema dieser studie war die untersuchung der toxizitt der hypofraktionierten stereotaktischen radiotherapie ( sbrt ) und der qol nach behandlung des lokal begrenzten prostatakarzinoms . 450 strahlenther onkol ( 2016 ) 192 : 449457 materialien und methoden die prospektive , monozentrische , klinische studie wurde bei prostatakarzinompatienten mit niedrigem bis mittlerem risiko durchgefhrt . 
die patienten fllten das eortc - qlq - c30und das prostatakarzinomspezische qlq - pr25 - formular aus . ergebnisse die analyse umfasste 68 prostatakarzinompatienten ( medianes alter 73 , spanne 5583 jahre ) im klinischen staging t1ct2cn0m0 , mit einem medianen gleason - score von 6 ( spanne 38 ) und einem medianen psawert ( prostataspezisches antigen ) von 10 ng / ml ( spanne 420 ng / ml )  . 
eine neoadjuvante androgendeprivationstherapie erhielten 52 patienten ( 76 , 5 % ) ; die hormontherapie beendet 31 patienten ( 45 , 5 % ) nach 6 monaten und 21 patienten ( 31 % ) nach 23 jahren . 
das durchschnittliche und mediane follow - up dauerte 24 monate ( spanne 1845 )  . der mediane psa - nadir betrug 0 , 03 ng / ml fr alle patienten und 0 , 6 ng / ml fr patienten ohne hormontherapie . psa - versagen und akute grad - iv - toxizitten traten nicht auf . 
ein patient ( 1 , 5 % ) hatte eine grad - iiiund 24 patienten ( 35 , 3 % ) eine grad - ii - harnblasentoxizitt , kein patient eine grad - iiiund 7 patienten ( 10 , 3 % ) eine akute gradii - rektumtoxizitt . 
globaler gesundheitsstatus / qol war gut und besserte sich in der untersuchten zeit . schlussfolgerung sbrt ist beim prostatakarzinom eine gut tolerierte behandlung hinsichtlich toxizitt und qol , ohne negativen einuss auf das alltagsleben und dem wichtigen vorteil einer kurzen behandlungszeit . 
langfristige followup - untersuchungen mssen noch folgen . schlsselwrter hypofraktionierte stereotaktische radiotherapie lebensqualitt rektum harnblase risikoorgane prostate cancer is the second most common solid tumor in men worldwide [ 1 ]  . 
the disease - specic survival rate is 98 % for patients after radical prostatectomy and 97 % for patients after external beam radiotherapy ( p = 0.543 ) [ 2 ]  . 
in the case of clinically localized , very lowand low - risk prostate cancer , active surveillance ( wait and see ) is also an option . the goal of radiotherapy is to deliver an adequate dose of radiation to the target , in this case the prostate , with an appropriate margin and while minimizing the dose to normal tissues ( in the rectum , bladder , bulb of penis , and femoral heads )  . 
three - dimensional conformal radiation therapy ( 3d - crt ) has replaced the old two - dimensional technique and has been the standard treatment for prostate cancer patients for years . 
for intermediate - risk patients , androgen deprivation therapy is recommended , and should start 6 months before external beam radiotherapy [ 14 ]  . the prognosis for most prostate cancer patients , particularly those in an early stage and independent of treatment options , is very good . 
for prostate cancer survivors , quality of life ( qol ) is a very important factor and it has become one of the most signicant issues in prostate cancer treatment decisions . the objective of this study was to investigate the effectiveness and safety of hypofractionated sbrt for localized prostate cancer , as well as patients qol after treatment . materials and methods a prospective single - center clinical study was performed in lowand intermediate - risk localized prostate cancer patients ( according to the national comprehensive cancer network , nccn )  . 
all patients underwent thoracic x - ray , abdominal ultrasonography , pelvic magnetic resonance ( mr ) , and bone scintigraphy . treatment planning patients were treated according to the special protocol prepared for this study . 
patients were placed on a diet designed to minimize gas production , without milk products , fresh fruits , and vegetables , 14 days before planning and during the entire treatment period . 
the radiation dose of 33.5 gy in 5 fractions was equivalent to the conventional dose of 78 gy in 39 fractions of 2 gy each ; the / ratio for prostate cancer was estimated to be around 1.41.5 gy [ 9 , 20 , 21 ]  . 
the / ratio for late complications in the rectum is 3 gy [ 22 ]  . taking this into account , the late rectal reactions dose was equivalent to the dose of 65 gy in 2 - gy fraction regimens . follow - up prostate - specic antigen ( psa ) levels were obtained before treatment and every 3 months . 
all patients submitted a signed consent form . we used demographic frequencies and descriptive statistics in the analysis , as well as a students t - test and a general linear model to measure the mean differences between time assessments . results patients were considered eligible for inclusion in this study if they had previously untreated , histologically conrmed adenocarcinoma of the prostate . the analysis included 68 men ( age 5583 years , mean 72.5 years , median 73 years ) treated between august 2011 and september 2013 at the department of radiation oncology of the independent public health care facility of the ministry of the interior with warmia and mazury oncology centre in olsztyn , poland . 
the clinical stage of prostate cancer was t1c - t2cn0m0 , the combined gleason score was 38 ( mean and median 6 ) , psa level was 420 ng / ml ( mean 10.9 ng / ml , median 10 ng / ml )  . 
the follow - up was stopped after 9 months for one patient and after 12 months for another because of other illnesses ; all other patients had a follow - up visit at least 18 months after the end of treatment . 
the median 3 - month posttreatment psa levels were 0.08 ng / ml for all patients and 2.8 ng / ml for those who did not receive androgen deprivation therapy . 
twelve months after the end of radiotherapy , the median psa levels were 0.06 ng / ml for all patients , 1.6 ng / ml for those who did not receive androgen deprivation therapy , and 0.04 ng / ml for patients who underwent 6 months of hormone therapy . 
twenty - four months after the end of radiotherapy , the median psa levels were 0.1 ng / ml for all patients , 0.4 ng / ml for those who did not receive androgen deprivation therapy , and 0.1 ng / ml for patients who underwent 6 months of hormone therapy . 
1 acute and late gastrointestinal ( a ) and genitourinary ( b ) toxicities according to radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc ) score strahlenther onkol ( 2016 ) 192 : 449457 fig . 
2 mean results of quality of life functional scales ( a ) and assessment of symptoms ( b ) in three measuring points of observation ( in median 9 , 21 and 30 months after end of radiotherapy )  . 
a scale i ( left site ) presents subscales of qol : physical functioning , emotional functioning , cognitive functioning , role functioning and social functioning ; scale ii ( right site ) presents summary results for all functional scales . 
b scale i ( left site ) presents subscales of each symptoms : fatigue , nausea and vomiting , pain , dyspnea , insomnia , loss of appetite , constipation , diarrhea , nancial difculties ; scale ii ( right site ) presents summary results for all symptoms . 
after 6 months of androgen deprivation , the psa level of two patients increased by over 1 ng / ml from the nadir during the observation period . more than two thirds of the patients ( 75 % ) showed stable or decreased levels of psa . patients tolerance of the treatment was good . 
most of the patients ( 67.6 % ) developed mild and moderate ( grade i or ii ) acute genitourinary and / or gastrointestinal toxicities : 24 patients ( 35.3 % ) developed grade ii acute bladder toxicity and 7 patients ( 10.3 % ) grade ii acute rectum toxicity . 
preliminary data have shown that this approach leads to successful tumor control without increasing complications [ 2527 ]  . acute urinary and rectal toxicities during and after sbrt are not higher than those for 3d - crt and imrt . 
king [ 26 ] , on behalf of the multi - institutional consoret al . tium of prospective trials , presented an analysis of 864 patients from phase ii clinical trials of sbrt ( median dose of 36.25 gy in 45 fractions ) for localized prostate cancer ( median follow - up of 3 years ; 194 patients remained evaluable at 5 years )  . 
some problems with the bladder and rectum were observed within the rst 3 months after sbrt , but the conditions returned to baseline status or better within 6 months . in the current study , 42 % of patients showed no treatment - related reaction during the radiotherapy schedules . there were no grade iii or iv toxicities in the rectum , and only one patient ( 1.5 % ) developed grade iii toxicity in the bladder . 
furthermore , in the sharp trial , 61 % of the patients had no acute ( during and 1 month after the end of treatment ) gastrointestinal toxicity , whereas this value was 63.5 % in our study . 
series [ 29 ] , with a median follow - up of 2.7 years , reported no grade iii or higher rectal toxicity and no grade iv urinary toxicity ; only 3.5 % of the patients developed grade iii urinary toxicity ( 36.25 gy in 5 fractions )  . yarbro and ferrans [ 30 ] demonstrated that radiotherapy has little impact on deterioration of qol . 
we observed that the ghs / qol of the patients was good 9 months after the end of treatment and signicantly improved during the following months . functional aspects , such as physical , emotional , cognitive , social , and general functioning , also improved . the american society for therapeutic radiation and oncology ( astro ) denition of biochemical psa failure as a surrogate endpoint for recurrence is three consecutive increases in the psa level after the posttreatment psa nadir dated at the midpoint between the nadir and the rst increase [ 31 ]  . 
as a potential surrogate endpoint in clinical trials , the phoenix denition of psa failure is a strong correlate of mortality and a predictor of metastatic disease ; it is superior to the astro denition [ 32 ]  . 
for 2 patients , the psa level increased by over 1 ng / ml from the nadir ; for 15 patients , the increase was 0.21.0 ng / ml from the nadir ( 25 % of all patients )  . 
 [ 36 ] observed an increase in psa level of > 0.2 ng / ml in 16 % of patients at a median 36 - month follow - up . there is more information about the cyberknife ( accuray , sunnyvale , ca , usa ) than linear accelerator ( linac ) use for sbrt of prostate cancer patients . 
our study used a linac , and all our results ( acute and late toxicities , qol , and psa increase and failure ) are similar to those obtained with the cyberknife series . one of the potential benets of sbrt is a short treatment period and probably lower costs compared with other advanced techniques . 
 [ 37 ] showed that sbrt is a more cost - effective ( in terms of radiotherapy , treatment of acute and late toxicities , and quality - adjusted life year ) external beam modality than imrt . our data are preliminary , as the number of treated patients is relatively small and follow - up should be longer . 
in the intermediate risk - group patients treated with hormonal therapy , the potential curative effect of radiotherapy cannot be assessed reliably during hormonal treatment ; therefore the efcacy of sbrt in our patients could not be estimated precisely and further follow - up is necessary . 
follow - up is planned for 10 years and will be presented in the future . one of the potential shortcomings was lack of the pre - study qol assessment ; however we believe that qol measured thrice after treatment is informative . conclusions hypofractionated stereotactic radiotherapy for lowand intermediate - risk prostate cancer patients is a safe and convenient treatment in terms of its duration , psa response , toxicity and patients qol assessment in the short term . however , a longer follow - up is needed . compliance with ethical guidelines conict of interest m . 
nawrocki state that there are no conicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
mai 2016 springer - verlag berlin heidelberg 2016 hintergrund und ziel die non - hodgkin - lymphome ( nhl ) stellen eine heterogene gruppe maligner erkrankungen des lymphatischen systems dar . 
standardbehandlung aggressiver diffus grozelliger b - zell - nhl ( dlbcl ) ist die immunchemotherapie bestrahlung als involvedeld - ( ifrt ) oder involved site ( isrt ) - radiation therapy , d . 
die bestrahlung von bulk - lsionen ( 7 , 5 cm ) fhrte dagegen zu einer signikanten verbesserung der langzeitergebnisse [ 6 ]  . die vorliegende studie von li et al . 
untersuchte retrospektiv den effekt einer konsolidierenden strahlentherapie bei patienten mit primren extranodalen , diffus grozelligen b - zell - lymphom des magens in den stadium ieiie ohne bulkbefall . originalpublikation li q , li w , wang l , wang w , niu s , bi x , et al ( 2015 ) consolidation radiotherapy in stage ieiie , non - bulky primary gastric diffuse large b - cell lymphoma with post - chemotherapy complete remission . 
74 , 01307 dresden , deutschland 2 oncoray national center for radiation research in oncology , dresden , deutschland patienten und methoden eine kohorte von 71 konsekutiven patienten wurde retrospektiv analysiert . 
die anzahl der events fr lrf , os und dmfs waren fr eine multivariate analyse zu gering . ergebnisse die patientencharakteristika alter , geschlecht , pathologischer typ , ldh , allgemeinzustand , b - symptomatik , ip - index und die anzahl der chemotherapie - zyklen unterschieden sich in beiden gruppen nicht . die mediane strahlentherapiedosis betrug 36 gy ( spannweite 24 , 440 gy )  . 
das gesamtpatientenkollektiv hatte ein medianes follow - up von 52 monaten ( spannweite : 7140 ) , 50 monate ( spannweite 7140 ) in der bestrahlten gruppe und 53 monate ( spannweite 8265 ) in der gruppe ohne bestrahlung . in der bestrahlten gruppe entwickelten 2 patienten ( 7 , 1 % ) ein lokalrezidiv , ohne bestrahlung 9 patienten ( 20 , 9 % )  . 
nach 10 jahren betrug fr die patienten mit oder ohne konsolidierender strahlentherapie das lokalrezidivfreie berleben 100 und 81 , 4 % ( p = 0 , 028 ) , das krankheitsfreie berleben 91 , 7 und 77 , 1 % ( p = 0 , 14 ) , das gesamtberleben 91 , 7 und 77 , 8 % ( p = 0 , 67 ) und das fernmetastasenfreie berleben 91 , 7 und 78 , 0 % ( p = 0 , 42 )  . schlussfolgerung der autoren die konsolidierende strahlentherapie fhrt zu einer verbesserten lokoregiostrahlenther onkol ( 2016 ) 192 : 500501 nalen kontrolle bei patienten mit frhem stadium eines primren dlbcl des magens mit klinisch kompletter remission nach mindestens vier zyklen einer ( immun - ) chemotherapie literatur kommentar nach den empfehlungen on der leitlinie der dgho erfolgt die erstlinientherapie beim dlbcl mit 6 - 8 zyklen des chop - protokolls und 8 gaben rituximab ( r - chop - protokoll ) [ 7 , 8 ]  . 
dagegen wird international zur therapie extranodaler nhl [ 13 ] fr die dlbcl des magens nach r - chop - therapie eine konsolidierende radiotherapie empfohlen . trotz der einschrnkungen , dass es sich in der hier vorliegenden publikation um eine retrospektive auswertung handelt , konnte erstmalig eine evidenz vom level iii erreicht werden , dass eine konsolidierende radiotherapie des dlbcl des magens nach 4 - 6 zyklen chemotherapie rituximab mit einer verbesserung der lokoregionren kontrolle assoziiert ist . 
ob dieser effekt auch nach einer erstlinientherapie mit 6 - 8 zyklen des chop - protokolls und 8 gaben rituximab einstellt , ist spekulativ und muss in weiteren studien untersucht werden . fazit fr patienten mit dlbcl des magens im stadium ieiie nach r - chop - therapie wird eine konsolidierende radiotherapie empfohlen . 
bonnet c et al ( 2007 ) chop alone compared with chop plus radiotherapy for localized aggressive lymphoma in elderly patients : a study by the groupe detude des lymphomes de ladulte . 
cunningham d et al ( 2013 ) rituximab plus cyclophosphamide , doxorubicin , vincristine , and prednisolone in patients with newly diagnosed diffuse large b - cell non - hodgkin lymphoma : a phase 3 comparison of dose intensication with 14 - day versus 21 - day cycles . 
delarue r et al ( 2013 ) dose - dense rituximab - chop compared with standard rituximab - chop in elderly patients with diffuse large b - cell lymphoma ( the lnh03 - 6b study ) : a randomised phase 3 trial . 
coifer b et al ( 2010 ) long - term outcome of patients in the lnh - 98.5 trial , the rst randomized study comparing rituximabchop to standard chop chemotherapy in dlbcl patients : a study by the groupe detudes des lymphomes de ladulte . 
pfreundschuh m et al ( 2008 ) six versus eight cycles of bi - weekly chop - 14 with or without rituximab in elderly patients with aggressive cd20 + b - cell lymphomas : a randomised controlled trial ( ricover - 60 )  . 
pfreundschuh m et al ( 2006 ) chop - like chemotherapy plus rituximab versus chop - like chemotherapy alone in young patients with good - prognosis diffuse large - b - cell lymphoma : a randomised controlled trial by the mabthera international trial ( mint ) group . lancet oncol 7 ( 5 ) : 379391 13 . 
fietkau1 received : 24 february 2016 / accepted : 21 april 2016 / published online : 31 may 2016 springer - verlag berlin heidelberg 2016 abstract introduction for both patients with high - grade gliomas and multiple cerebral metastases , radio ( chemo ) therapy is the standard therapy . 
neurological decline during treatment is rarely attributed to infections of the brain but to tumor progression or side effects of radiotherapy . case reports we present 4 cases of cytomegalovirus ( cmv ) viremia associated with neurological deterioration , which occurred during or shortly after radiotherapy and / or chemotherapy of the brain ( brain metastases 2 , high - grade glioma 1 , carcinoma inltrating brain 1 )  . 
general infections were either excluded or receding before the neurological symptoms occurred . all patients presented with decreasing levels of thrombocytes . in all cases , cmv ( re ) activation could be proven using blood test for cmv - dna . 
the anti - cmv - igg status suggested reactivation rather than a primary infection . one patient died within 72 h of onset of the symptoms ( results of cmv tests were received postmortem )  . 
diagnosis of 3 patients allowed successful administration of antiviral treatment , which greatly improved the general and neurological conditions of the patients within 48 h . discussion neurological deterioration during rt is hardly ever attributed to viral infections . 
these cases suggest that cmv reactivation and subsequent infection might actually be causative and has to be considered and treated . conclusion further prospective studies verifying and investigating this observation in terms of frequency and clinical relevance seem indicated . keywords encephalitis encephalopathy opportunistic infections ganciclovir neurological manifestations the present work was performed in ( partial ) fulllment of the requirements for obtaining the degree med . 
nach bestrahlung / chemotherapie des gehirns korrelation mit neurologischer verschlechterung und besserung unter antiviraler therapie zusammenfassung einleitung sowohl fr patienten mit hirnmetastasen als auch fr patienten mit hochgradigen gliomen ist eine radio ( chemo ) therapie die therapie der wahl . 
neurologische verschlechterungen whrend der behandlung werden meist einem tumorprogress oder nebenwirkungen der strahlentherapie attribuiert . falldarstellungen prsentiert werden 4 flle von mit einer cmv - virmie assoziierten neurologischer verschlechte490 strahlenther onkol ( 2016 ) 192 : 489497 rung , die whrend bzw . 
kurz nach bestrahlung und / oder chemotherapie des gehirns auftrat ( hirnmetastasen 2 , hochgradiges gliom 1 , zerebral inltrierendes karzinom 1 ) : in allen fllen war die neurologische verschlechterung unerwartet , und ursachen wie erhhter intrakranieller druck oder tumorprogress wurden radiologisch ausgeschlossen . dexamethason und mannitol hatte keinen dauerhaften effekt . 
bei allen patienten zeigten sich abnehmende thrombozytenzahlen , bei allen lie sich eine cmv - infektion serologisch nachweisen ( anti - cmv - igm und / oder cmv - dna )  . 
der anti - cmv - igg - status wies dabei jeweils auf eine cmv - reaktivierung hwhrend 2 patienten innerhalb von 72 h nach beginn der neurologischen symptome verstarben ( die cmv - testresultate lagen erst post mortem vor ) , konnten 3 patienten antiviral behandelt werden . 
ihr zustand besserte sich innerhalb von 48 h deutlich . diskussion an neurotrope infektionen wird bei neurologischer verschlechterung von am hirn bestrahlten / chemotherapierten patienten normalerweise nicht gedacht . die vorgestellten ergebnisse deuten aber darauf hin , dass eine cmv - reaktivierung / - infektion in betracht gezogen und gegebenenfalls behandelt werden sollte . ausblick weitere prospektive studien zur besttigung und zur untersuchung dieser beobachtung bezglich frequenz und klinische relevanz scheinen angebracht . schlsselwrter enzephalitis enzephalopathie opportunistische infektionen ganciclovir neurologische manifestationen introduction for both patients with high - grade gliomas and multiple cerebral metastases , radio ( chemo ) therapy ( r [ c ] t ) is the standard therapy [ 32 , 34 ]  . 
neurological decline during treatment ( e.g. , speech impairment , severe fatigue , disorientation , decreasing cognitive function ) is usually attributed to microscopic tumor progression , side effects of rt , or chemo - brain if magnet resonance images ( mri ) do not show edema , disease progression , or signs of increased intracranial pressure . 
treatment of these symptoms usually includes increasing doses of dexamethasone in an attempt to decrease intracranial pressure and ameliorate symptoms . success , however , is often limited and patients rarely reach their pretherapeutic neurological status . one as of yet underestimated reason for neurological decline may be opportunistic infections . 
it is known that cancer patients , as a collective of patients with unspecically compromised immune system , seem to be susceptible to cmv ( cytomegalovirus ) reactivation and disease . 
unfortunately , symptoms and treatment were not specied . patients with high - grade gliomas who are treated with temozolomide , the standard chemotherapy for this type of cancer , have been shown to suffer opportunistic infections to a surprisingly high degree , the most common being mucocutaneous candidiasis ( 28.2 % ) , pneumocystis jirovecii pneumonia ( 7.6 % ) and cmv reactivation ( 12.8 % ) [ 2 , 8 ]  . evaluating the sparse literature shows that cmv activation during treatment with temozolomide is mostly known to cause cmv colitis or cmv pneumonia [ 31 ]  . while cmv reactivation and subsequent disease is known to sometimes occur during chemotherapy , a connection between rt , especially of the brain , is as of yet unknown . 
up to now , cmv infections causing symptoms like encephalitis / encephalopathy are hardly ever diagnosed in patients with brain cancer . in this article , we present the cases of 4 patients ( brain metastases [ 2 / 4 ] , high - grade glioma [ 1 / 4 ] , or carcinoma inltrating the brain [ 1 / 4 ] ) with sudden onset neurological decline , who actually suffered from systemic cmv infection . cmv infections are usually not considered as a diagnosis when confronted with neurological decline ; thus , we present these case reports so that treating physicians are aware of this possible differential diagnosis . case 1 patient history a 63 - year - old woman with cerebrally metastasized lung cancer ( sclc , ct1b cn1 cm1 ) and beginning hydrocephalus occlusus was treated rst with implantation of a ventriculoperitoneal shunt . 
whole - brain radiotherapy ( wbrt ) started 16 days after shunt implantation and proceeded without problems for 5 days up to a dose of 15 gray ( gy ) ( 30 gy planned dose ; 3 gy single dose )  . at this point , her general condition worsened and she was treated for febrile neutropenia . 
her general condition and serum parameters improved with antibiotic treatment within 2 days and rt could be continued . strahlenther onkol ( 2016 ) 192 : 489497 neurological decline caused by systemic cmv infection her neurological condition suddenly and unexpectedly worsened 26 days after shunt implantation ( rt dose 24 gy )  . within a period of hours she was disorientated but opened her eyes and was able to move her extremities upon request . she had no hemiplegic symptoms , signs of meningeal affection , or increased intracranial pressure . 
e. , lumbar puncture to gain csf ( cerebrospinal uid ) , were performed . treatment and prognosis after consultation with her relatives and following the patients will , further diagnostics and treatments were not performed , apart from continuing antibiotics and uids . 
tests for acute infection with herpes simplex virus and varizella zoster virus were negative . treatment and prognosis the patient was treated with ganciclovir 5 mg / kg body weight twice daily for 14 days . 
the patient could be discharged in much improved general condition . case 3 patient history a 72 - year - old woman with triple negative breast cancer had been treated with neoadjuvant chemotherapy , surgery , and adjuvant rt in 2013 . 
it is supposed to say wbrt , which i have introduced in case 1 . six days after the start of rt ( rt dose 6 gy of planned 40 gy wbrt and 20 gy boost ; 2 gy single dose ) , the patient suffered from double vision and bilateral facial paralysis . 
double vision disappeared under treatment with dexamethasone , but facial paralysis remained . neurological decline caused by systemic cmv infection the patient became somnolent over a period of a few hours 36 days after the start of rt ( nal dose 52 gy )  . 
a lumbar puncture was not performed in accordance with the sisters decision . strahlenther onkol ( 2016 ) 192 : 489497 strahlenther onkol ( 2016 ) 192 : 489497 494 strahlenther onkol ( 2016 ) 192 : 489497 treatment and prognosis facts all cases have in common she was treated with ganciclovir i . 
5 mg / kg body weight for 14 days until the virus dna was no longer detectable . her condition improved within 48 h and she could be discharged after completion of rt . 
she was discharged in stable condition to a rehabilitation facility . neurological decline caused by systemic cmv infection the patient was hospitalized 28 days after completion of radiochemotherapy with severe ataxia and speech impairment . 
anticmv - igg was positive but anti - cmv - igm was negative . she tested negative for varizella zoster virus and jc virus . a lumbar puncture was not performed due to the assumed risk of subfalcine herniation . treatment and prognosis treatment consisted of ganciclovir i . 
she could be discharged in much improved condition . in all four cases , neurological decline was sudden , unexpected , and occurred over a period of 72 h at the most . in most cases ( 3 / 4 ) , the symptoms developed during or within 10 weeks after rt of the bracauses such as increased intracranial pressure or tumor progression could be excluded using mri or ct . 
for all patients , active infection with cmv could be proven via quantitative pcr . treatment with dexamethasone and mannitol had no or only very short - lived effects on the general condition of the patients . 
from these rst cases , we learned to test for cmv ( re ) activation early on . discussion radiotherapy is often considered to be the reason for neurological decline and cognitive dysfunction during but also after r ( c ) t [ 33 ]  . 
we believe it to be of great importance to know that the possibility of this infection exists and that it can be treated successfully . radiation has been shown to activate viruses in vitro [ 26 ]  . 
one could hypothesize that rt of tumor masses known to contain at least particles of the virus ( 8099 % for high - grade gliomas [ 6 , 27 ] and 92100 % for brain metastases [ 9 ] ) can lead to local infection - encephalitis / encephalopathyand systemic viremia . 
moreover viral encephalitis is known to mimic the radiological appearance of glioblastoma and vice versa [ 13 ]  . glioblastoma patients as a very specic group of cancer patients are suspected to have higher prevalence of positivity for anti - cmv - igg ( 5099 % ) [ 3 , 4 ] compared to the healthy population ( 3060 % ) [ 5 , 6 ]  . strahlenther onkol ( 2016 ) 192 : 489497 corticosteroids are known risk factors for the occurrence of cmv infection in aids patients [ 19 ] but also otherwise healthy individuals [ 20 ]  . 
additional effects on reactivation of the virus are possible and need to be investigated further . usually , cmv reactivations subsequent to secondary infections are most well - known to occur in severely immunosuppressed patients . 
a direct link between the amount of corticosteroids administered and the probability of cmv reactivation has been demonstrated [ 1 ]  . a second susceptible group are aids patients with inherent immunosuppression [ 17 ] , who also suffer from cmv reactivation to a much higher degree than the healthy population . known factors to provoke reactivation are immunosuppression and inammation [ 10 ] , with natural killer ( nk ) cells seemingly playing a major role in in controlling the virus . 
sepsis - associated nk cell dysfunction has been shown to contribute to cmv reactivation [ 11 , 23 ]  . while the role of cmv viremia during infection remains controversial , results from murine models suggest that pulmonary cmv reactivation that was caused by sepsis causes a stronger onset and prolonged infection [ 24 ]  . for both cerebral metastases and high - grade gliomas , it has been shown that up to 30 % of the patients die of unknown causes , 4 months and 1 month after diagnosis , respectively , partially even with denite exclusion of the tumor being the cause of death [ 15 , 16 ]  . 
 [ 29 ] , who presented a collection of 16 / 18 patients who had blood drawn for quantitative pcr before treatment , found only 1 patient showing detectable viral load during follow - up . however , holdhoff et al . 
 [ 29 ] concluded that their results proved an absence of cmv in those tested patients , it is possible that the method needs to be improved , the sample size was too small or the mean age was too low , as the risk of seropositivity increases with age . as far as we know , no one has ever considered an association between the unexplained clinical neurological deterioration of glioblastoma patients or patients with brain metastases with a reactivation of a viral infection , i . 
it was only after treating the rst patient that we learned to look for the symptoms especially if initial dexamethasone fails to improve the patients condition . we are aware that we cannot prove cmv encephalopathy / encephalitis , as lumbar punctures were only performed in one case , and even in this case , we did not think to test for cmv . 
according to the guidelines of the german society of neurology , however , cmv encephalitis should be proven in csf by either detecting the specic antibody or the virus itself , though searching for the virus in peripheral blood is possible . 
therefore , cmv encephalopathy or encelphalitis was not proven . but there are some facts that make it rather probable that cmv encephalopathy or encephalitis may be responsible for the neurological deterioration of the patients : the blood - brain - barrier being impaired [ 35 , 36 ] due to the underlying disease , allowing virus particles to become detectable in peripheral blood in combination with distinct symptoms typical for encephalitis / encephalopathy allowed us to make the diagnosis rather probable . 
this seems especially true for case 3 , as cmv is known to often affect central nerves or cause ( meningo - ) encephalitis rather than meningitis [ 37 ]  . 
furthermore , the patients signicantly improved within hours after antiviral treatment was initiated , partly even from somnolence to complete clarity , whereas they had not responded to anti - edematous treatment , and inltration of the meninges was excluded using mri . certainly , the death of the rst patient might have also been caused by other factors such as nonconvulsive epileptic seizure . 
as she was able to perform basic tasks such as 496 strahlenther onkol ( 2016 ) 192 : 489497 opening her eyes or moving distinct parts of her body upon request , we do not consider a seizure to be the most likely cause . when patients with brain metastases or high - grade glioma , especially patients over the age of 60 , present with declining neurocognitive function , severe fatigue , etc . , even if the onset is sudden and decline progresses within hours or days , progressive disease is usually proclaimed to be the cause , even if mris are unchanged or show minimal progress at most . 
palliative care is often recommended in such cases , and the patients die within days or weeks . it is not our intention to claim that all patients with neurological decline suffer from cmv reactivation and subsequent central nervous infection and can be saved with antiviral treatment . 
the patients quality of life could improve considerably , and the patient may reach a state that makes standard therapy worth reconsidering . we initiated the prospective glio - cmv - 01 study in order to determine the frequency of cmv ( re ) activation and the frequency these ( re ) activations become clinically relevant and require treatment . 
in this setting we will also try to determine further risk factors for the occurrence of these infections ( e.g. , radiotherapy , chemotherapy , or exposure to corticosteroids )  . 
this is especially necessary as cmv reactivation and subsequent disease during r ( c ) t of the brain for high - grade glioma or brain metastases are as of yet unknown . rapid neurological decline during or after radiotherapy / chemotherapy of the brain in the absence of radiological explanation should make every treating physician remember this possibility and lead to subsequent testing for cmv and systematic treatment , if applicable . acknowledgements we wish to thank the editor and the reviewers for their detailed analysis of our manuscript and their helpful suggestions . compliance with ethical guidelines conict of interest n . 
lewis rm , johnson pc , golden d , van buren ct , kerman rh , kahan bd ( 1988 ) the adverse impact of cytomegalovirus infection on clinical outcome in cyclosporine - prednisone treated renal allograft recipients . 
juni 2016 springer - verlag berlin heidelberg 2016 hintergrund aufgrund der physikalischen eigenschaften der protonentherapie ( prt ) kommt es im vergleich zur photonentherapie zu einer reduktion der strahlendosis am gesunden gewebe . 
in der vorliegenden studie wurde die klinische relevanz dieser hypothese mit den endpunkten akutund sptfolgen sowie berleben bei kindern mit einem medulloblastom untersucht . methode in eine nicht - randomisierten phase ii - studie wurden 59 patienten ( 321 jahre alt ) mit medulloblastom eingeschlossen . 
bestrahlt wurde die kraniospinale achse mit einer dosis von 1836 gy rbe , in einzeldosen von 1 , 8 gy rbe , anschlieend erfolgte eine dosisaufsttigung ( boost ) auf das tumorbett bis zu einer medianen gesamtdosis von 54 gy rbe . 
der primre endpunkt der studie war die inzidenz von ototoxizitt ( kumulative ototoxizitt nach 3 jahren ) , sekundre endpunkte waren neuroendokrine sowie neurokognitive nebenwirkungen . originalpublikation yock ti , yeap by , ebb dv et al ( 2016 ) long - term toxic effects of proton radiotherapy for paediatric medulloblastoma : a phase 2 single - arm study . 
das progressionsfreie berleben nach 3 jahren betrug 80 % , das gesamtberleben 83 % . schlussfolgerung der autoren eine protonentherapie fhrt bei akzeptablen nebenwirkungsraten zu hnlichen behandlungserfolgen wie die photonentherapie und kann als alternative behandlungsmethode eingesetzt werden . kommentar bliche kritikpunkte bei publikationen aus dem bereich der protonentherapie sind einerseits immer die unzureichende datenlage aus prospektiven klinischen studien sowie der fehlende ergebnisvergleich mit der modernen photonentherapie . 
trotzdem kann das angewendete studienprotokoll die notwendigen fragen und bedenken gegenber einer neuen therapieform nicht vollends beantworten . schade ist vor allem das fehlen eines kontrollarms in form einer modernen photonentherapie , z . 
da aber die potentiellen vorteile der protonentherapie bei der reduktion von akustrahlenther onkol ( 2016 ) 192 : 498499 ten und chronischen nebenwirkungen gesehen werden , insbesondere von neurokognitiven deziten , und dieser vorteil insbesondere fr pdiatrische patienten postuliert wird , ist wohl eine randomisierung zwischen beiden verfahren wegen groer widerstnde und sicherlich auch mit dem argument einer unethischen behandlung im standardarm schwer durchsetzbar . was knnen wir nun aus den vorliegenden daten fr den klinischen alltag lernen ? sicherlich besttigen die daten , dass eine protonentherapie , die an einem zentrum mit hoher expertise durchgefhrt wird , eine sichere und auch effektive , aber zugleich schonende therapieform ist [ 1 , 2 ]  . die daten zeigen aber ebenfalls , dass die protonentherapie nicht nebenwirkungsfrei ist . 
da fr die behandlung von patienten mit medulloblastomen nicht nur die strahlentherapie allein ein wichtiger prognostischer faktor ist , sondern auch das zeitintervall zwischen diagnose , operation und dem beginn der bestrahlung [ 3 , 4 ] , sollte die zeitnahe verfgbarkeit der strahlenbehandlung im vordergrund stehen . 
letztlich ist die bestrahlung der neuroachse , wie es bei patienten mit medulloblastomen notwendig ist , eine hochkomplexe therapieform , die einer ausreichenden expertise in der onkologie und strahlenphysik bedarf und deshalb nur an spezialisierten zentren angeboten werden sollte . fazit da weiterhin auch mit der vorliegenden studie offen bleibt , inwiefern sich durch die protonentherapie ein wirklicher benet ergibt , reiht sie sich , wenn auch prospektiv aufleider nahtlos in die literaturmitteilungen ein , gesetzt , wonach die protonentherapie lediglich als eine mgliche alternative zur modernen photonentherapie bewertet wird . aufgrund der vorhandenen datenlage sollte jedoch insbesondere bei pdiatrischen patienten die mglichkeit einer protonentherapie immer geprft werden . 
allen am , pawlicki t , dong l , fourkal e , buyyounouski m , cengel k , plastaras j , bucci mk , yock ti , bonilla l , price r , harris ee , konski aa ( 2012 ) an evidence based review of proton beam therapy : the report of astros emerging technology committee . radiother oncol 103 ( 1 ) : 811 2 . 
combs se , kessel ka , herfarth k , jensen a , oertel s , blattmann c , ecker s , hoess a , martin e , witt o , jkel o , kulozik ae , debus j ( 2012 ) treatment of pediatric patients and young adults with particle therapy at the heidelberg ion therapy center ( hit ) : establishment of workow and initial clinical data . 
rieken s , mohr a , habermehl d , welzel t , lindel k , witt o , kulozik ae , wick w , debus j , combs se ( 2011 ) outcome and prognostic factors of radiation therapy for medulloblastoma . 
chan aw , tarbell nj , black pm , louis dn , frosch mp , ancukiewicz m , chapman p , loefer js ( 2000 ) adult medulloblastoma : prognostic factors and patterns of relapse . 
juli 2016 springer - verlag berlin heidelberg 2016 hintergrund in einem vor kurzem in strahlentherapie und onkologie bereits von panje und guckenberger verffentlichten literaturkommentar [ 1 ] wurde eine studie von golden und kollegen [ 2 ] vorgestellt , die sich mit dem abskopalen effekt der strahlentherapie , d . 
die autoren vermuteten einen vorteil durch die gabe von gm - csf , jedoch knne dies aufgrund fehlender kontrollarme ohne diese behandlung nicht sicher geschlussfolgert werden . patienten und methoden in einer zweistugen phasei / ii - studie wurden patienten mit metastasierten stabilen oder progredienten tumoren mit strahlentherapie und granulozyten - / makrophagenkoloniestimulierendem faktor ( gm - csf ) behandelt . 
golden eb , chhabra a , chachoua a et al ( 2015 ) local radiotherapy and granulocyte macrophage colony - stimulating factor to generate abscopal responses in patients with metastatic solid tumours : a proof - of - principle trial . 
pdl1 - inhibitoren , gm - csf oder imiquimod erhofft man sich eine synergistische antineoplastische wirkung , die durch den immunologischen wirkmechanismus nicht auf das bestrahlungsfeld beschrnkt ist . panje und guckenberger [ 1 ] haben diese studie bereits kommentiert und auf wichtige limitationen im hinblick auf ihre klinische bedeutung hingewiesen . 
insbesondere stellten sie die nicht eindeutig zu klrende rolle der strahlentherapie bei fortfhrung der systemischen therapie whrend der behandlung und die mglichkeit einer prognostisch gnstigeren tumorbiologie bei patienten mit abskopalen effekten heraus . 
uns erscheinen noch weitere aspekte der vorgestellten arbeit diskussionswrdig . trotz des sehr innovativen konzepts ist angesichts der tumorerkrankungen , bei denen in der studie abskopale effekte konstatiert wurden , nmlich skepsis angebracht : mammakarzinome gehren vermutlich zu den stark im676 strahlenther onkol ( 2016 ) 192 : 675676 munologisch beeinussbaren tumoren [ 5 ] , bei denen in der vergangenheit auch ohne systemische adjuvanz ausgeprgte abskopale effekte beschrieben wurden [ 6 ]  . 
das gute ansprechen bei patienten mit nicht - kleinzelligen bronchialkarzinomen lsst die frage aufkommen , wie viele dieser patienten bereits eine neuartige immuntherapie erhalten hatten und ob in diesem fall die vom studienprotokoll geforderte vierwchige behandlungspause zwischen immuntherapie und studienbeginn ausreicht . 
die studie wurde zwar noch vor der etablierung der immuntherapie bei metastasierten nicht - kleinzelligen bronchialkarzinomen durchgefhrt , in new york waren jedoch bereits zuvor patienten mit immuncheckpoint - inhibitoren unter studienbedingungen behandelt worden . 
hier wren zumindest detaillierte angaben zur vortherapie der patienten wnschenswert gewesen . die lange rekrutierungsdauer von 10 jahren und die tatsache , dass 88 % der patienten lediglich 36 messbare lsionen aufwiesen , deuten darauf hin , dass es sich um ein stark selektiertes patientengut handelte , bei dem eine prognostisch gnstige oligometastasierung vorlag . 
die autoren teilten jedoch patienten , die noch vor der bildgebung systemisch progredient waren , dem non - responder - arm zu , unabhngig davon , ob sie einen abskopalen effekt an einer lsion zeigten oder nicht . 
diese art der auswertung verschlechtert natrlich die berlebensrate des non - responder - arms erheblich . fazit trotz der genannten schwchen handelt es sich auch aus unserer sicht um eine wichtige publikation , da sie den stellenwert der strahlenbehandlung in einer knftig strker immunologisch ausgerichteten onkologischen therapie ins blickfeld der prklinischen und klinischen forschung rckt . in der klinischen praxis sind abskopale effekte aufgrund des multidisziplinren behandlungsansatzes nicht sicher einer bestimmten behandlungsmodalitt , z . 
jedoch gibt es anhalte , dass m - csf im gegensatz zu gm - csf ein eher tumorpermissives mikromilieu frdert [ 8 , 9 ]  . sebastian zschaeck und michael baumann , dresden interessenkonikt s . 
golden eb , chhabra a , chachoua a et al ( 2015 ) local radiotherapy and granulocyte - macrophage colony - stimulating factor to generate abscopal responses in patients with metastatic solid tumours : a proof - of - principle trial . 
klug f , prakash h , huber pe et al ( 2013 ) low - dose irradiation programs macrophage differentiation to an inos + / m1 phenotype that orchestrates effective t cell immunotherapy . 
frey b , rubner y , kulzer l et al ( 2014 ) antitumor immune responses induced by ionizing irradiation and further immune stimulation . cancer immunol immunother 63 : 2936 5 . 
kitoh y , saio m , gotoh n et al ( 2011 ) combined gm - csf treatment and m - csf inhibition of tumor - associated macrophages induces dendritic cell - like signaling in vitro . 
zhang m , he y , sun x et al ( 2014 ) a high m1 / m2 ratio of tumor - associated macrophages is associated with extended survival in ovarian cancer patients . 
however , in free - breathing plans commonly measured dose constraints do not allow precise estimation of the dose to the coronary arteries . keywords adverse effects myocardial ischemia adjuvant radiotherapy cardiac toxicity breastconserving therapy spiegelt die mittlere herzdosis im rahmen der radiotherapie beim linksseitigen mammakarzinom die dosisbelastung der koronararterien ausreichend wider ? einuss der atemtriggerung zusammenfassung hintergrund das risiko kardialer sptfolgen nach bestrahlung ( rt ) eines mammakarzinoms spielt insbesondere auch aufgrund der zunehmenden systemischen begleittherapien eine wichtige rolle . 
der einuss der atemtriggerung und der daraus resultierenden geometrischen lagevariabilitt der risikoorgane auf die dosisverteilung am herzen / koronarien sollte geprft werden , um zu klren , inwieweit die mittlere herzdosis ein ausreichender surrogatparameter fr die dosisbelastung der koronarien ist . patienten und methoden ausgewertet wurden 130 patientinnen mit mammakarzinom , die mit einer adjuvanten rt ( 50 , 4 gy + boost 916 gy ) bestrahlt wurden . 
des weiteren wurde strahlenther onkol ( 2016 ) 192 : 624631 die kardiale / koronare dosisbelastung mit und ohne atemtriggerung verglichen . ergebnisse die mittlere herdosis ( dmean herz ) wurde durch atemtriggerung von 2 , 7 gy ( spanne 0 , 85 , 2 gy ) auf 2 , 4 gy ( spanne 1 , 14 , 6 gy ) reduziert . 
die dosisparameter dmean herz dmean lad , v25 herz dmean lad und dmax herz dmax lad waren nur fr atemgetriggerte flle signikant korrelierbar ( p < 0 , 01 ) , mit einem durchschnittlichen anstieg der mittleren lad - dosis von 3 , 6 gy pro 1 gy mittlere herzdosis . 
bei einer nicht - atemgetriggerten rt lagen die mittleren lad - dosen zwischen 1 , 3 und 28 , 6 gy trotz v25 ( cid : 2 ) 5 % . schlussfolgerung unter einsatz einer atemgetriggerten bestrahlungstechnik lassen sich sowohl die mittlere herzals auch die lad - dosis senken und die kardialen dosisparameter miteinander korrelieren . 
fr die rt ohne atemtriggerung lsst sich die lad - belastung jedoch nicht sicher abschtzen . schlsselwrter nebenwirkungen myokardiale ischmie adjuvante radiotherapie kardiale toxizitt brusterhaltende therapie introduction breast - conserving therapy has been proven as the appropriate treatment for most women with early breast cancer [ 1 ]  . 
a meta - analysis demonstrated that adjuvant irradiation reduces the 5 - year local recurrence and 15 - year overall mortality in breast cancer patients [ 1 , 2 ]  . 
with the extensive use of concurrent systemic treatment , the issue of cardiac mortality after breast cancer radiation is still important today [ 4 , 5 ] , which is most frequently reported as decreased myocardial function or coronary artery disease . 
many studies only addressed the entire heart volume when evaluating cardiac toxicity [ 5 , 6 ] and the mean heart dose was used as the only common reference dose without considering exposure to the coronary arteries . 
however , trials [ 8 ] suggest that the coronary arteries are particularly radiosensitive and are responsible for long - term radiation - induced ischemic disease . the implementation of improved techniques as respiratory gating has demonstrated reduction of heart doses and is recommended in left - sided breast cancer radiotherapy [ 9 ]  . 
to exclude any selection bias we have chosen a period in 2004 and in 2014 for our study , during which we evaluated all left - sided breast cancer patients . in all , 84 % ( 109 / 130 ) of patients underwent breast - conserving surgery , the remaining mastectomy . 
an additional boost of 916 gy was applied to the primary site of tumor depending on age ( total dose of 66.6 gy for patients < 50 years )  . 
contouring was performed according to the rtog contouring atlas using a validated physician - contouring protocol [ 10 ] developed for ct 626 strahlenther onkol ( 2016 ) 192 : 624631 images without intravenous contrast , too . 
these contouring recommendations have been shown to improve accuracy of cardiac contours in a tested group of radiation oncologists [ 10 , 11 ]  . the upper border of the heart included both atria without the pulmonary trunk , ascending aorta , and superior vena cava . 
the left anterior descending artery ( lad ) originated from the left coronary artery . its location was identied using the course of the anterior interventricular groove between the right and left ventricle . 
the lad was contoured from its origin down to the last segment at the cardiac apex . raising the level to 50 and lowering the window to 150 is recommended [ 10 ]  . 
a radial margin of 5 mm was added to each coronary artery contour to allow for uncertainty in identication of artery positions and cardiac beating movements . the 3d conformal rt was applied using the eclipse treatment planning system ( varian medical systems ) and dosevolume histograms ( dvhs ) were generated for the planning target volume ( ptv ) and all organs at risk . 
the heart dose constraints were v25 < 10 % and dmean < 5 gy [ 7 , 12 ]  . dosimetric comparisons were made between patients treated with gated and nongated rt . 
antihormonal therapy was applied in 75 % ( nongated ) and 71 % ( gated ) of patients ; adjuvant chemotherapy was applied in 38 % ( nongated ) vs 51 % ( gated ) of cases . 
with the introduction of 3d - ct - based rt the dose to the heart can be precisely estimated , and since then constraints on mean heart dose have been introduced into guidelines [ 7 , 13 , 14 ]  . 
however , it still remains unclear which dosevolume constraint of the lad may be a surrogate of later risk of heart disease . respiratory motion management systems have been shown to potentially reduce heart doses [ 15 , 16 ]  . 
baseline characteristics of our gated and non - gated treatment cohort were typical for breast cancer patients with a majority of the women with low - risk disease and good prognosis factors [ 2 ]  . 
as reported in a swedish series [ 20 ] , the extent of dose reduction depends on radiation technique and may be more relevant when internal mammary lymph nodes are included . 
3 relationship between dmax heart ( gy ) and dmax left anterior descending artery ( lad , in gy ) for a gated ( n = 59 ) and b non - gated radiotherapy ( n = 71 ) of 7 studies with a cohort size of up to 30 patients reported a decrease in lad doses and smaller variability of dose ranges for gated rt [ 17 ]  . 
comparable to this , lad doses of our patients ranged from 2.219.9 gy for gated rt and 1.328.6 for non - gated rt . anteriorly placed coronary arteries are more often affected by rt compared to the lcx or atria [ 14 ]  . 
nevertheless , to date there are no data available to precisely dene the impact of gated rt in breast cancer patients on late cardiac mortality due to the limited number of published gating studies and the long latency until cardiac toxicities may gain clinical signicance [ 16 , 17 ]  . 
up to now , the clinical benet of gating rt has only been determined by dosimetric studies . the danish and swedish study group [ 18 ] found an increased risk of heart disease of 4 % for each 1 gy increase in dmean heart . 
the recently published populationbased casecontrol study of major coronary events in 2 , 168 women calculated that rates of major coronary events increased linearly with dmean heart by 7.4 % / gy [ 7 ]  . 
the cardiac events encompassed myocardial and coronary morbidity equally , thus , also supporting the impact of lad dosimetry for breast cancer patients as well [ 14 , 15 , 18 ]  . the mean dose to lad was a predictor of the rate of major coronary events ( p = 0.001 ) , but without statistical significance in multivariate analysis . 
however , in this analysis ct - based information on treatment plans were unavailable and the effect of valvular diseases on the rate of myocardial deaths was not specied [ 7 ]  . as published by taylor et al . 
analysis of myocardial and vascular perfusion changes of the left ventricle and the correlation with coronary artery distribution demonstrated that the majority of left - sided abnormalities were identied to be mainly located in the lad territory in patients undergoing left - sided breast cancer rt [ 23 ]  . 
contradictory to this , a large variability of mean heart and lad doses using breathing - adapted rt was reported [ 27 ] for node - positive breast cancer patients who were treated by 2 630 strahlenther onkol ( 2016 ) 192 : 624631 tangential and 1 supraclavicular eld . 
our analysis demonstrated a signicant association between maximum heart and lad exposure for patients with gated rt ( p < 0.01 ) but a large variability of lad doses up to 52.6 gy using free - breathing rt despite mean heart doses well below dose constraints . investigations of radiation - induced coronary changes found persistent changes in regions receiving more than 45 gy and supported the necessity to avoid high lad doses [ 23 , 25 , 26 ]  . 
according to guidelines , the validated atlas to study cardiac exposure to radiation [ 10 ] was used for contouring procedures ; nevertheless , anatomical variations may occur , which cause differences in lad volumes and lengths [ 10 , 13 , 22 , 30 ]  . 
our results of dose values depending on respiratory gating may not be translated to nontangential 3d or intensity - modulated radiotherapy ( imrt ) elds . conclusion with the background of our data generated in a large , uniformly treated cohort of left - sided breast cancer patients , we can show a signicant reduction and association of heart and coronary artery ( lad ) doses for adjuvant radiotherapy using inspiratory gating . 
in free - breathing plans , commonly measured heart dose constraints do not allow precise estimation of the dose exposure to coronary arteries . the absolute risk of radiation - associated cardiac disease with modern rt techniques remains uncertathus , mean heart dose remains the reference measure for cardiotoxicity , which is more reproducible from one physician to another . nevertheless , coronary artery exposure should be as low as possible . 
eble1 received : 15 september 2015 / accepted : 13 april 2016 / published online : 10 june 2016 springer - verlag berlin heidelberg 2016 abstract background despite modern techniques , in some patients receiving whole breast radiotherapy ( wbi ) parts of the heart and the lung might receive doses which are nowadays considered relevant for the development of late morbidity . 
our aim was to analyze the usefulness of a thermoplastic breast brassiere to reduce lung and heart doses . patients and methods a total of 29 patients with left - sided and 16 patients with right - sided breast cancer treated with breast conserving surgery and wbi between 2012 and 2013 were included in a prospective study analyzing the effectiveness of a thermoplastic breast bra . 
no acute skin toxicities > grade 2 were observed . conclusion by using a thermoplastic breast bra , radiation doses to the heart and especially parts of the heart apex and ipsilateral lung can be signicantly lowered without additional skin toxicity . ( cid : 2 ) pd med . 
40 , 42283 wuppertal , germany keywords breast - conserving surgery cardiotoxicity mortality cardiac apex left anterior descending artery nutzen eines thermoplastischen bstenhalters bei radiotherapie eines mammakarzinoms eine prospektive analyse zusammenfassung hintergrund trotz moderner techniken knnen bei manchen patientinnen bei der ganzbrustbestrahlung areale des herzens und der lunge dosen erhalten , die heute als relevant fr spttoxizitten gelten . 
ziel war es , den nutzen eines thermoplastischen bstenhalters hinsichtlich der reduktion von lungenund herzdosen zu ermitteln . methoden prospektiv wurde bei 29 patientinnen mit linksseitigem und 16 mit rechtsseitigem brustkrebs , bei denen 610 strahlenther onkol ( 2016 ) 192 : 609616 die zwischen 2012 und 2013 eine brusterhaltende op und ganzbrustbestrahlung ( whole breast irradiation , wbi ) erfolgte , die effektivitt eines thermoplastischen bstenhalters ( bh ) untersucht . 
interventricularis anterior ( riva ) und eine denierte apikale region , das apical myocardial territory ( amt ) , deniert . ergebnisse die ipsilaterale lungendosis wurde durchschnittlich um 30 , 6 % ( karzinom linksseitig ) bzw . 
es traten keine akuten hauttoxizitten > grad 2 auf . schlussfolgerung der thermoplastische bh ermglicht die signikante reduzierung der strahlenbelastung am herzen , insbesondere im herzspitzenbereich sowie der ipsilateralen lunge , ohne die hauttoxizitt zu erhhen . schlsselwrter brusterhaltende chirurgie kardiotoxizitt mortalitt herzspitze linke anterior absteigende koronararterie introduction after breast - conserving surgery ( bcs ) , whole breast irradiation ( wbi ) with a total dose of 50 gy reduces the local recurrence rate by 7088 % [ 1 , 2 ]  . 
in early trials , an increase of cardiac deaths was seen [ 3 ] and cardiac mortality was higher in left - sided breast cancer patients than in right - sided [ 4 , 6 , 7 ]  . 
due to the general use of 3 - dimensional ( 3d ) radiation treatment planning , cardiac morbidity has been reduced to an extent that it is generally no longer a relevant issue of concern in longer - term analyses [ 712 ]  . however , in some patients , i . 
e. , with adverse thorax geometry or close distance between heart and ribs , standard 3d tangential treatment planning results in heart and also lung dose ranges which are nowadays regarded as possibly being associated with the development of severe late reactions . 
 [ 13 ] showed an odds ratio of 7.22 for high - grade stenoses of the mid and distal lad including the distal diagonal branch . the aim of this analysis was to analyze the usefulness of a breast brassiere ( breast bra ) with one - sided thermoplastic cup for breast cancer radiotherapy to reduce exit doses to both heart and lung . patients and methods from 20122013 , a total of 45 breast cancer patients ( stage i / ii , 29 women with left - sided and 16 women with right - sided breast cancer ) treated with bcs followed by wbi were included in the prospective analysis . 
median age was 67 years ( range 3784 years )  . adjuvant wbi started 46 weeks after surgery and was delivered with 6 - mv photon beams using wedged tangential elds at 1.8 gy daily fractional doses up to a total dose of 50.4 gy ( icru )  . 
 [ 14 , 15 ] covering the outer 10 mm of the cardiac wall or myocardium , respectively . the lad was identied and delineated in the anterior interventricular groove down to the apex of the heart [ 16 , 17 ]  . looking for selection criteria identifying patients particularly proting from using the bra several parameters were analyzed . 
regarding this , we analyzed correlation coefcients between the patient related parameters clinical target volume ( ctv ) , reecting the breast size and body mass instrahlenther onkol ( 2016 ) 192 : 609616 fig . 
the thickness of the plastic material is 0.50.63 mm dependent on the cup size , with several sizes available to account for individual breast volumes . all patients gave written informed consent prior to participation in the study . statistics for evaluation of dose differences the paired t - test was used . correlation analyses were performed with pearson correlation coefcient . 
for left - sided cancer , all parameters comparatively analyzed are shown in detail in table 1 , corresponding dose distributions and dosevolume histograms ( dvh ) calculated without vs . 
six weeks after nishing radiotherapy , 9 patients presented with grade 1 erythema , while all others were scored grade 0 . no selection criteria could be found to identify patients particularly suitable for using the bra . 
however , sometimes even small heart doses are suspected to increase sd standard deviation , ctv clinical target volume , ptv planning target volume lung left mean strahlenther onkol ( 2016 ) 192 : 609616 fig . 
2 dose - wash images from the 3d treatment plans in transversal , sagittal , and coronary planes without bra ( a ) and with bra ( b ) fig . 
however , it has to be considered that despite low mean heart doses , relevant areas of the heart could be exposed to doses between 40 and 50 gy [ 24 ]  . 
the mean heart dose , as only parameter reported in earlier studies , does not really reect the cardiac risk in many cases . the question , which parts of the heart are of highest relevance considering late effects , thus , implying their optimal protection is not denitely answered , but there is increasstrahlenther onkol ( 2016 ) 192 : 609616 ing evidence , e . 
 [ 13 ] found an increase of clinically signicant coronary artery stenoses in predened hotspot areas for radiation inpatients who underwent left - sided wbi compared to patients receiving no radiotherapy to these predened areas . in this swedish cohort analysis , a 4to 7 - fold risk increase of signicant stenoses was shown for the mid and distal left anterior descending artery ( lad ) in rt hotspot areas . 
 [ 25 ] demonstrated perfusion defects in the cardial apex already 624 months after radiotherapy after exposing these areas to > 50 % of the prescribed dose . an analysis by magee et al . 
 [ 26 ] revealed that in 9 % of patients treated with tangential beams the cardial apex was within the radiation eld . considering the different heart dosevolume aspects , it seems to be reasonable to dene several parts of the heart , especially the anterior part , as organs at risk . 
 [ 14 , 15 ] demonstrated that using the anterior myocardial territory ( amt ) as an organ at risk in left - sided breast imrts , the radiation dose to the heart could be reduced . several technical options are presently being investigated to optimize heart and also lung doses in breast cancer radiotherapy without compromising the target dose and volume . such techniques are , i . 
consecutively , a signicant reduction of the heart and especially apical subvolumes like the left anterior descending artery ( lad ) could be demonstrated by several authors [ 16 , 27 , 28 ]  . 
although subvolumes of the heart like the left ventricle , amt , or lad were not analyzed separately , the dose reduction may affect mainly the heart apex due to the treatment technique using nondivergent tangential beams . likewise , stranzl et al . 
also , the ( multi - angle ) imrt has pros and cons . in general , long - term side effects of low doses exposed to larger volumes of healthy tissue and also the increase in strahlenther onkol ( 2016 ) 192 : 609616 scatter dose to the body is not fully claried [ 31 ]  . 
 [ 29 ] or hepp et al . [ 27 ] , both using the dihb technique . considering the thermoplastic material on the breast skin we were cautious about potential skin reactions , which were found to be in the normal range , and no skin toxicities > grade 2 were observed . 
no significant correlations were found between the ctv , reecting the breast size , and oar values such as dmax for amt , dmax for lad or v10 for left lung using the bra . 
in addition , the body mass index or the denition of a cut - off value concerning the breast size could not be identied to select the patient needing the bra . of note , no cut - off in breast size was identied where patients would not have proted from the bra application in term to doses of oars , albeit in different dimension , and rather triggered by the mobility of the tissue : patients with a small but pendulous breast with low consistency may also benet from the raising effect caused by the bra . 
from a practical point of view , the benet may be strong if the breast is dropping and if the bra is able to raise the breast forward . conclusion by using a thermoplastic breast bra , radiation doses to the heart and especially parts of the heart apex and ipsilateral lung can be signicantly lowered , without additional skin toxicity . 
eble state that there are no conicts of interest . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
juli 2016 der / die autor ( en ) 2016 hintergrund und ziel die autoren berprfen mittels prospektiver dokumentation die mittelfristigen ergebnisse der wait - and - see - strategie ihrer patienten mit karzinomen in den unteren 6 cm des rektums nach kompletter remission infolge einer hochdosierten radiochemotherapie ( rct )  . patienten und methode einschlusskriterien fr die studie waren patienten mit primr durch tiefe anteriore resektion oder exstirpation resektable karzinome t2 / 3 n01 . erosionen und oberchliche ulzerationen waren ebenfalls zulssig . 
die properativ intendierte rct bestand aus 60 gy in 30 fraktionen und einem endorektalen brachytherapie - boost von 5 gy auf den tumor und 50 gy in 30 fraktionen auf die elektiven regionalen lymphknoten ( lk )  . 
patienten , die nach 6 wochen eine klinisch komplette tumorremission und tumorfreie biopsien sowie in der computertomographie ( ct ) und in der magnetresonanztomographie ( mrt ) keine regionalen oder distanten metastasen aufwiesen , wurden der beobachtungsgruppe ( watchful waiting ) zugewiesen und im median 23 , 9 monate mit endoskopien und biopsien aus suspekten bereichen nachbeobachtet . 
alle anderen patienten originalpublikation appelt al , plaen j , harling h et al ( 2015 ) high - dose chemoradiotherapy and watchful waiting for distal rectal cancer : a prospective observational study . 
die studie war ofziell registriert ( clinicaltrials.gov , number nct00952926 ) und die patientenallokation ist abgeschlossen . ergebnisse zwischen oktober 2009 und dezember 2013 wurden an drei behandlungszentren in dnemark 55 patienten erfasst . 
lokalrezidive traten nach 1 jahr in 15 , 5 % auf ( 95 % - kondenzintervall [ 95% - ki ] 3 , 326 , 3 ) , die mediane zeit bis zum rezidiv betrug 10 , 4 monate . 
die sphinkterfunktion war exzellent mit 72 % nach 1 jahr und 69 % nach 2 jahren ( jorge - wexner - score 0 [ iqr 00 ] zu allen zeitpunkten )  . 
rektale blutungen vom grad 3 als sptreaktion wurden nach 1 jahr mit 7 % ( 2 / 30 ) und nach 2 jahren mit 6 % ( 1 / 17 ) angegeben . schlussfolgerung der autoren watchful waiting ist mglicherweise eine sichere alternative zur rektumexstirpation , wenn es nach neoadjuvant intendierter radiochemotherapie zu einer kompletten tumorremission gekommen ist . kommentar die diskussion dieser studie muss sich ausschlielich auf das risiko eines lokalrezidivs in einem durchaus greren kollektiv und mit der hier angewandten form der radiochemotherapie mit nachfolgender kompletter remission beschrnken . 
dabei entspricht die indikation zur rct grundstzlich der gngigen auswahl in bezug auf die t - kategorie , die hier wohl das ausschlieliche selektionskriteri678 strahlenther onkol ( 2016 ) 192 : 677678 um war . 
damit bleibt die gesamtzahl der berhaupt behandelten patienten und die rate der klinisch kompletten remissionen unklar . man darf auch nicht auer betracht lassen , dass ein nicht unerheblicher teil von patienten mit klinisch kompletter remission nach rct trotzdem radikal operiert wird , weil eben keine komplette remission unter wertung von inspektion , palpation und bildgebung bewiesen ist . 
all dies knnte in der diskussion besser herausgearbeitet werden , zumal manche untersucher inzwischen im ersten jahr von regrowth und erst spter von rezidiv reden , womit das gesamtergebnis geschnt wird . 
dennoch sollte tatschlich im falle einer kompletten oder klinisch sehr guten remission mit der ansonsten erforderlichen exstirpation oder sehr tiefen anterioren resektion zunchst erstmal zugewartet werden . allerdings ist der verzicht auf eine standardgeme tumoroperation nur zu vertreten , wenn die entsprechenden patienten auer einer narbe und eventuellen teleangiektasien keine sichtbare weitere lsion mehr aufweisen , palpatorisch keinerlei tumor zu tasten und auch in der bildgebung ( mrt und endosonographie ) nicht zu erkennen ist . 
die pet ist zustzlich nur in sehr erfahrenen hnden hilfreich , schlielich erfordert die bewertung solcher flle nach eigener erfahrung die lngste lernkurve . fr gewhnlich ist sie nmlich zur bewertung entbehrlich , so dass alleine hieraus die unschrfe der daten um ein weiteres zunimmt . werner hohenberger und rolf sauer , erlangen interessenkonikt w . 
a total dose of 5072 cge ( cobalt gray equivalent ) in 512 fractions was delivered . results the median follow - up duration was 29 months ( range 495 months )  . 
one grade 5 treatment - related adverse event occurred in a patient with symptomatic idiopathic pulmonary brosis . conclusions ablative dose hypofractionated pbt was safe and promising for stage i and recurrent nsclc . keywords non - small - cell lung carcinoma proton beam therapy ablativ dosierte protonentherapie bei stadium - iund rekurrierenden nichtkleinzelligen lungenkarzinomen ablativ dosierte protonentherapie fr nsclc zusammenfassung zweck beurteilung von wirksamkeit und sicherheit hypofraktionierter protonentherapie ( pbt ) mit ablativen dosen fr nichtkleinzellige lungenkarzinome ( nsclc ) im stadium i und rekurrierende nsclc . methode und materialien retrospektiv wurden insgesamt 55 nsclc - patienten ( stadium i : n = 42 ; rekurrierender tumor : n = 13 ) , analysiert . 
sie waren mit einer gesamtdosis von 5072 cge ( cobalt gray equivalent ) in 512 fraktionen behandelt worden . ergebnisse der median der follow - up - dauer lag bei 29 monaten ( 495 )  . 
die 3 - jahrekaplan - meier - gesamtberlebensrate ( os ) war 54 , 9% , der 650 strahlenther onkol ( 2016 ) 192 : 649657 median lag bei 48 , 6 monaten ( 495 )  . 
therapiebedingte grad - 3oder - 4 - toxizitten traten nicht auf , bei einem patienten mit symptomatischer idiopathischer lungenbrose kam es zu einer unerwnschten therapiewirkung grad 5 . schlussfolgerung die hypofraktionierte pbt mit ablativen dosen hat sich als sicheres und erfolgversprechendes therapieverfahren fr nsclc im stadium i und fr rekurrierenden nsclc erwiesen . schlsselwrter nicht - kleinzellige lungenkarzinome protonen - strahl - therapie introduction non - small cell lung carcinoma ( nsclc ) is the leading cause of cancer death worldwide [ 1 ]  . 
although surgical resection is the standard of care for early - stage nsclc , with 5 - year survival rates of 5080% [ 2 ] , a considerable number of patients are deemed inoperable because of their underlying medical conditions . 
radiotherapy ( rt ) using conventional fractionation for those patients had been disappointing , with local progression of about 40% and overall survival ( os ) rates of 631% [ 3 ]  . stereotactic ablative radiotherapy ( sabr ) is characterized by a higher dose per fraction compared to conventional fractionation , a highly conformal dose distribution , and measures that ensure precise radiation dose delivery . treatment of early stage nsclc with sabr yields a notable local control rate ( lcr ) reaching 90% or above with minimal toxicity [ 46 ]  . 
there has been constant interest in the use of proton beam therapy ( pbt ) for early - stage lung cancer as well as locally advanced disease [ 8 ]  . 
recently , some investigators have reported a favorable local control rate with acceptable toxicities after ablative dose pbt comparable to those of sabr in early - stage nsclc patients [ 915 ]  . however , most pbt studies still have more protracted treatment courses compared with those of sabr standards , so the evidence concerning pbt with hypofractionation for early - stage nsclc is still limited [ 915 ]  . thus , the objective of our study is to evaluate clinical outcomes of ablative dose hypofractionated pbt for patients with stage i and recurrent nsclc . patients and methods patients between september 2007 and december 2013 , 55 patients with stage i and recurrent nsclc treated with ablative dose hypofractionated pbt were included in the current study . 
the required clinical stage was t1 - 2n0m0 according to the american joint committee on cancer staging , 6th edition ( n = 42 ) or isolated parenchymal lung recurrence of nsclc ( n = 13 )  . 
recurrent cases were diagnosed with isolated parenchymal lung recurrence after initial treatment using either surgical resection ( n = 9 ) or thoracic rt to the other lobe ( n = 4 )  . 
for inclusion of recurrent cases , isolated parenchymal recurrence should have at least a 2 - year disease - free interval from initial treatment , and it should be staged as recurrent t1 - 2n0m0 ( tumor diameter < 5 cm ) with the following diagnostic evaluation . except 1 patient with recurrence whose tumor was inaccessible by guided biopsy procedure , all patients underwent pretreatment work - up , including a complete blood count ( cbc ) , a biochemical prole , chest radiographs , pulmonary function tests ( pfts ) , computed tomography ( ct ) of the chest and 18f - uorodeoxyglucose positron emission tomography ( [ 18f ] fdg - pet ) scan . 
when any hilar or mediastinal lymph nodes were suspicious on imaging workups , a guided biopsy using either endobronchial ultrasound ( ebus ) or endoscopic esophageal ultrasound ( eus ) was performed . 
before undergoing ct simulation , tumor or lung motion was checked by uoroscopy to choose between pbt with respiratorygated and four - dimensional ( 4d ) ct planning alone . the range of tumor motion or the involved lung motion were more than 1 cm , respiratory gating treatment was selected and planned . 
respiratory - correlated 4d - ct datasets were generated using the planning ct ( lightspeed rt ; ge medical systems , waukesha , wi , usa ) and the real - time position managementtm ( rpm ) system from varian medical systems ( palo alto , ca , usa )  . 
datasets of the average ct images and maximum intensity projection were reconstructed using the images of 10 time - binned breathstrahlenther onkol ( 2016 ) 192 : 649657 ing phases ( phase 0 , 10 , 20 , 30 , 40 , 50 , 60 , 70 , 80 , and 90% )  . 
next , the datasets of ct images were transferred to a treatment planning system ( eclipsetm , version 8.0 ; varian medical systems ) , and target volumes and organs at risk were contoured . the gross tumor volume ( gtv ) is comprised of radiological lesion in lung parenchyma under the lung window setting . 
hence , all treatment planning processes for respiratory - gated treatment , including contouring , beam arrangement , and dose calculation , were restricted only in the respiratory phase at 40 , 50 , and 60% . 
for the expansion of ptv from itv , set - up error ( 35 mm ) and range uncertainty of proximal and distal sobp ( 35 mm ) had been considered . 
a relatively larger safety margin of 1 cm in dening ptv in the early period of applying hypofractionated pbt was used at our institution , but it has been reduced gradually to 68 mm with the accumulation of experience . 
all target volumes were compared with all ct images of each phase or targeted phase , including maximum - intensity projection ct images before being copied to the average ct images for a proton beam treatment planning . 
pbt plans were optimized so that 100% of the prescribed dose would cover at least 95% of the ptv and that 99% of the ptv receives a minimum of 90% of the prescribed dose . 
we adapted organs - atrisk ( oar ) dose constraints from rtog protocols [ 16 ] , and the following oars were considered : lungs , heart , spinal cord , esophagus , ipsilateral brachial plexus , skin , trachea , and ipsilateral bronchus . 
patients were treated daily , ve times per week , with one of the following ablative dose fractionation schemes : 60 cge / 5 fractions , 50 cge / 5 fractions , 60 cge / 10 fractions , or 72 cge / 12 fractions . 
all centrally located tumors were delivered 60 cge over 10 fractions . for treating tumors at a peripheral location , the dose fractionation scheme was chosen considering tumor size and underlying lung function and the ambiguity of location between central and peripheral . 
the treatment set - up of each patient was veried by geometric repositioning using the digital imaging position system ( dips ) to match bony landmarks to digitally reconstructed radiographs from the planning ct . 
the passive double scattering mode ( proteus 235 ; ion beam application , s.a. , louvain - la - neuve , belgium ) was used at an energy of 230 mev . follow - up evaluation and statistical analysis patients were assessed weekly during pbt , 1 month after completion of pbt , every 3 months for the rst 2 years , and every 6 months thereafter . 
local progression refers to primary tumor failure meeting one of the following criteria : ( 1 ) at least a 20% increase in the longest diameter of the target lesion , and the measurable tumor should be avid on pet imaging with similar uptake intensity as the pretreatment pet , ( 2 ) the presence of 3 high - risk features suggested by the well - established huang criteria [ 19 ] on serial ct images , ( 3 ) be biopsied to conrm a viable carcinoma . outeld recurrence in the ipsilateral involved lobe was considered as local progression . 
regional recurrence refers to the appearance after pbt of a measurable tumor within the lymph node along the natural lymphatic drainage typical for the location of the treated primary disease only with a dimension of at least 1.0 cm on imaging studies within the lung , bronchial hilum , or mediastinum [ 20 ]  . 
a total of 29 patients ( 53% ) were treated with respiratory - gated pbt . the median total dose was 60 cge ( range 5072 cge ) , and the median fraction size was 10 cge ( range 512 cge ) corresponding to a bed10 of the median 115 cge ( range 90132 cge )  . 
a grade 5 toxicity of sudden exacerbation of symptomatic idiopathic pulmonary brosis ( ipf ) was observed in a patient 3 months after pbt , and he expired due to respiratory failure . 
1 kaplanmeier curves illustrating local control rate ( lcr ) , lymph node metastasis - free survival ( lnmfs ) , distant metastasis - free survival ( dmfs ) , and overall survival ( os ) rates over time described in table 1 . 
the contralateral lung in all cases received no dose due to the lack of exit dose of protons . treatment outcomes therefore , the median follow - up duration was 29 months ( range 495 months )  . 
majority of the local progression cases ( n = 5 ; 71% ) occurred in lower lobe area , and among them , three of lower lobe located tumor were very close to diaphragm . all but one case ( n = 6 ; 86% ) were treated with respiratory - gated treatment due to wide tumor motion range . 
we intended to deliver higher bed to peripherally located tumors and those delivered more than 100 gy of bed were all peripherally located . to reduce the concern of normal tissue toxicities , we usually used 34 portals to patients who needed more than a bed of 100 gy in our study . 
although we did not observe a doseresponse relationship of pbt in the present study , several sabr and hypofractionated pbt studies conrmed the doseresponse relationship in early - stage nsclc , particularly in stage ib tumors [ 15 , 24 , 25 ]  . 
some investigators reported that motion of small lesions located in the lower half of the lung was considerable during the respiration cycle and greatest near the diaphragm [ 2729 ]  . 
also the uncontrollable motion of abdominal organs such as stomach or large bowel can result in variations in tissue density on beam path and , therefore , interrupt adequate dose delivery to the target [ 30 , 31 ]  . 
as proton beam is highly sensitive to depth variation and tissue density changes on the beam path , adequate control of intrafractional tumor and organ motion is a key component of pbt application [ 32 ]  . 
in the present study , we usually employed 4 - dimensional ct or respiratory - gated system for motion control during the early period of pbt for lung cancer without abdominal compression . 
recently , both respiratory - gating and bellows - type abdominal compression have been used for treating lower lobe tumors . standardized uptake value ( suv ) is a semiquantitative index that characterizes [ 18f ] fdg uptake approximating the glucose metabolic rate . 
 [ 35 ] found that pre - sabr suvmax on [ 18f ] fdg - pet scan has strong correlation to distant failure in medically inoperable early - stage nsclc patients . 
before the introduction of pbt to clinical practices at our institution , we usually deliver photon sabr to nsclc patients on a daily basis , as described in the report of japanese experience [ 38 ]  . 
we assumed that daily pbt schedule would be tolerable and sufcient for normal tissue recovery between treatment fractions , as pbt is better able to expose a tumor to a higher radiation dose without increasing normal tissue toxicity than photon sabr . 
in previous pbt studies , severe pulmonary toxicity rates were reported to be only 07% [ 915 , 23 ] and the explanation might be that pbt can reduce low - dose contamination by a lower integral dose and little exit dose [ 39 ]  . 
several investi656 strahlenther onkol ( 2016 ) 192 : 649657 gators have reported that acute exacerbation of ipf could occur after conventional radiotherapy or sabr for nsclc at a rate of approximately 25% [ 40 ]  . 
despite the expectation that pbt would have lower normal tissue complication probability with lower mean lung dose and v20 , pulmonary toxicity prole of our study was not largely different from those after photon sabr . 
on the other hand , it might be inspiring that there were no other grade 35 toxicities except 1 patient with aggravating ipf , although 24% of tumors included in our study were centrally located , which differs from the nding of rtog 0618 [ 17 ]  . 
there was a relatively large percentage of patients suffering from rib fractures ( n = 3 ; 5% ) and chest pain ( n = 16 , 29% ) , possibly because we did not strictly apply the chest wall dose constraint in the early period of hypofractionated pbt . 
nevertheless , the results of this study are meaningful because of the rarity of pbt clinical data for early - stage nsclc , and the dose schemes used were almost similar to those of photon sabr . 
a total of 15 patients were treated with proton sabr with a median of 45 cge ( range 4250 cge ) in 35 fractions and showed no local progression within the radiation eld and minimal toxicity rates . 
the databases used for computation of the present gap and additional requirements are ( a ) global cancer incidence , mortality and prevalence ( globocan ) for cancer incidence ( b ) the directory of radiotherapy centres ( dirac ) of the iaea for existing trt units ( c ) human resources from the recent estro health economics in radiation oncology ( hero ) survey and ( d ) radiotherapy utilization ( rtu ) rates for each tumour site , published by the ingham institute for applied medical research ( iiamr )  . results in 2015 , 30 , 999 of 45 , 903 cancer patients would have required radiotherapy . 
by 2020 , this will have inpresented at the 19th annual meeting of the scientic association of swiss radiation oncology ( sasro ) , basel , 1113 june 2015 . ( cid : 2 ) med . 
the present study should assist the stakeholders and health planners in designing an appropriate strategy for meeting future radiotherapy needs for switzerland . keywords cancer population radiation oncology staff intensity - modulated radiotherapy infrastruktur und personalausstattung der strahlentherapie in der schweiz derzeitiger stand und vorausberechnungen bis 2020 zusammenfassung ziel ziel dieser studie war es , den aktuellen stand der infrastruktur und personalausstattung der strahlentherapie in der schweiz zu bewerten und prognosen fr das jahr 2020 zu erstellen . material die estro - quartsund iaea - richtlinien wurden angewandt , um den bedarf fr teletherapie ( trt - ) einheiten , radioonkologen ( ro ) , medizinphysiker ( mp ) und medizinisch - technische radiologieassistenten ( rtt ) abzuschtzen . 
dieses modell knnte auf die individuellen bedrfnisse eines beliebigen bestrahlungszentrums angepasst werden . schlussfolgerung der bedarf an bestrahlungstherapie fr krebspatienten wird in den nchsten 5 jahren um 9 , 8 % steigen . 
diese studie soll stakeholder und gesundheitsplaner dabei untersttzen , eine entsprechende strategie zu entwickeln , um knftigen anforderungen in der strahlentherapie in der schweiz gerecht zu werden . fazit der bedarf an bestrahlungstherapie fr krebspatienten wird in den nchsten 5 - jahren um 9 , 8 % steigen . diese studie soll stakeholder und gesundheitsplaner dabei untersttzen , eine entsprechende strategie zu entwickeln , um knftigen anforderungen in der strahlentherapie in der schweiz gerecht zu werden . schlsselwrter krebs population radioonkologie personal intensittsmodulierte strahlentherapie the european health report 2012 indicates that around 20 % of all deaths in europe could be attributed to cancer [ 1 ]  . 
there is also a gradual change in rt treatment techniques from conventional two - / three - dimensional conformal rt ( 2d / 3d crt ) to intensity - modulated radiation therapy ( imrt ) and stereotactic radiosurgery / stereotactic radiotherapy ( srs / srt )  . 
as these are gradually being embraced by most clinics in the country , this aspect needs to be accounted for future human resource computations . thus , the present paper evaluates the rt needs in switzerland using country - specic parameters based on cancer incidence and the proportion of patients of each site who would need rt . 
both the rt infrastructure , in terms of teleradiotherapy ( trt ) units , and human resources , namely radiation oncologists ( ro ) , medical physicists ( mp ) and radiotherapy technologists ( rtt ) have been considered . the present status and the projections for 2020 of switzerland are based on these considerations and the changing rt practices , to help identify the existing gaps and design future long - term strategies to optimize rt services in the country . methods databases used the population details of switzerland and its distribution over the 26 cantons were obtained from the fdha , switzerland [ 2 ]  . 
the details of the rt units were mined from the directory of radiotherapy centres ( dirac ) of the international atomic energy agency ( iaea ) [ 7 ]  . 
radiation oncology stafng in terms of full - time equivalent ( fte ) of ro , mp and rtt have been taken from the recently published data in the health economics in radiation oncology survey by the european society of therapeutic radiation oncology ( estro - hero ) [ 8 ]  . 
the other categories pertaining to medical dosimetrists , radiotherapy nurses and radiation biologists have not been considered , as there are no specic guidelines pertaining to these groups in the estro quantication of radiation therapy infrastructure and stafng recommendations ( estro - quarts ) or in those of the iaea [ 4 , 9 ]  . 
all calculations are based on the information posted at the above databases in the public domain as of 12 dec 2015 . strahlenther onkol ( 2016 ) 192 : 599608 fig . 
c trend in the number of cancer cases reported per year during the periods 20052009 and 20152019 . for both genders , a steep rise is projected : 30 % in males and 20 % in females [ 3 ] computation of the radiotherapy requirements for each tumour site guidelines for radiotherapy infrastructure and human resources the rt needs for different tumour sites have been ascertained based on the rt utilization ( rtu ) rates derived for 27 major clinical sites by barton et al . 
since around 2025 % of cancer patients are estimated to need retreatment with irradiation , an rtu of 0.25 for reirradiation was considered [ 4 ]  . calculations for various components of rt capacity have been based on estro - quarts and iaea guidelines [ 4 , 9 ]  . 
thus , the requirements have been considered to conform to the higher end of these standard guidelines . consequently , the benchmarks adapted in the present calcu602 strahlenther onkol ( 2016 ) 192 : 599608 table 1 computation for total annual person - hours using a weighted manpower to meet the requirements for adopting a combination of conventional ( 2d / 3d crt ) and state - of - the - art radiotherapy techniques ( imrt / srs / srt )  . 
with the widespread availability of dynamic imrt techniques , the treatment time on the machines for imrt has been reduced considerably compared to the static step - and - shoot imrt methods [ 1417 ]  . 
however , the time required for contouring tumour and organs of interest is higher compared to conventional 2d / 3d crt , as has been the experience at the authors department and which is in line with observations from the quality and innovation assurance in radiation oncology ( quiro ) project surveys conducted by the german society of radiation oncology ( degro ) [ 1823 ]  . 
to some extent , this could be reduced using automated atlas - based segmentation , although the available tools from various vendors are presently still far from ideal [ 24 , 25 ]  . 
the total person - hours per yearassuming 52 weeks , 5 working days / week , 8 hours working / day , and 30 staff and public holidayswould be 1840 person - hours / year for each category of staff , computed as ( 52 5 8 ) ( 30 8 )  . 
this would be based on the number of patients a department proposes to treat with 2d / 3d crt , imrt and srs / srt , as detailed in table 1 . results present status and projections for 2020 at present , the annual cancer incidence in switzerland is estimated to be 45 , 903 , and this is expected to reach 50 , 427 by 2020 . 
however , a total of 78 trt units results in 10.5 trt units / million population , which is well above the median of 5.3 trt units / million population for the entirety of europe ( table 2 )  . strahlenther onkol ( 2016 ) 192 : 599608 table 2 distribution of teleradiotherapy and brachytherapy units in various cantons of switzerland populationa ( in millions ) centres with rt facilitiesb teleradiotherapy unitsb brachytherapy unitsb teleradiotherapy units / million canton aargau appenzell ausserrhoden appenzell innerrhoden basel - land basel - stadt bern fribourg geneva glarus graubnden jura luzern neuchtel nidwalden obwalden schaffhausen schwyz solothurn st . 
the proton therapy facility at the centre of proton therapy , paul scherrer institute , villigen is not included in this table . using the rtu values for each cancer site , 30 , 999 patients required rt in 2015 . 
an additional seven trt units will be required by 2020 . fte of 98 , 75 and 274 ros , mps and rtts , respectively , are reported to be available in switzerland as per the 2014 estro - hero survey [ 8 ]  . 
the fte presently required are 155 , 89 and 310 ros , mps and rtts , respectively , resulting in a corresponding gap of 57 , 14 and 36 in each of these categories , respectively . 
3. discussion the incidence of cancer in switzerland is predicted to substantially increase between 2005 and 2019 both for males ( at 30 % ) and females ( at 20 % ) [ 3 ]  . 
this is similar to that observed in other industrialized countries like the usa , where the projected rise is estimated to be 26 % and 18 % for men and women , respectively , during the period 2010 to 2020 [ 27 ]  . the swiss health system offers universal coverage with high levels of access to services and is high - performing with a particularly strong backup of hospital care . 
this subsequently translates into high cancer survival rates [ 28 ]  . thus , for switzerland , effective cancer control programmes need to be directed not only at the cancer incidence for newly diagnosed cancer cases , but also to address the need for supportive treatment ( including reirradiation ) for cancer survivors . 
the national institute for cancer epidemiology and registration ( nicer ) estimates that in 2015 , 316 , 000 patients will be living with a history of cancer ( 146 , 500 men and 169 , 500 women ) , and this is expected to strahlenther onkol ( 2016 ) 192 : 599608 fig . 
2 radiotherapy infrastructure and human resources in switzerland , as existing in 2015 and the additional needs by 2020 , are shown for a teleradiotherapy units b radiation oncologists c medical physicists and d radiation therapy technologists . 
for each rt technique 2d / 3d imrt table 4 an illustrative example to show the human resource requirements for ro , mp and rtt due to the gradual change in adapting from 2d / 3d crt to imrt / srs / srt over 5 - years ( y15 )  . 
it is therefore mandatory that the projected rt needsin terms of both infrastructure and human resourcestake into account all these elements . until now , the estro - quarts and iaea have been used as the benchmarks for quantifying the requirements of trt units and rt staff . 
although , the basic impression still stands valid in the present calculations , subtle differences in the actual numbers are due to ( a ) previous data being for the status as of april 2014 , while the present study pertains to december 2015 ( b ) earlier gures for all 39 european countries being computed based on an overall assumption that 62.5 % strahlenther onkol ( 2016 ) 192 : 599608 fig . 
3 a changes in the anticipated treatment techniques from only two - / three - dimensional conventional radiotherapy ( 2d / 3d crt ) to intensity - modulated radiotherapy ( imrt ) and stereotactic radiosurgery / radiotherapy ( srs / srt ) over 5 years . 
b changes in the fte for radiation oncologists , medical physicists and radiation therapy technologists over the 5 - years corresponding to the change in treatment techniques . the numbers have been calculated keeping the total number of patients treated annually at 1000 . 
 ( details of computation described in the text and table 4 ) of all cancer patients would require rt [ 29 , 30 ] , while the present data takes into consideration the individual rtus for each specic cancer site based on the actual number of different cancer types prevalent in switzerland and ( c ) earlier estimates being made for all european countries using the benchmark values for required trt units , ro , mp and rtt of 1 / 450 patients , 1 / 250 patients , 1 / 450 patients and 1 / 150 patients , respectively . 
however , to conform to the current swiss rt practices , the yardsticks have been made stiffer and now correspond to 1 / 400 patients , 1 / 200 patients , 1 / 350 patients and 1 / 100 patients for trt units , ro , mp and rtt , respectively . 
thus , the present estimates of an additional requirement of 7 trt units , 72 ros , 22 mps and 66 rtts by 2020 should be more realistic , as they are specic for switzerland . consideration has also been paid to the changing scenario in most centres adapting to state - of - the - art rt treatments . 
as staff members become familiar with the entire treatment process of state - of - the - art rt techniques and move ahead along the learning curve , the entire process for the practice of these techniques would be reduced . 
thus , these factors need to be taken into account by individual departments when working out their staff requirements in a longitudinal manner . in addition , the process innovations could help to improve the efciency of the treatment . 
this has been aptly demonstrated for various treatment sites and specialized techniques like imrt in the quiro project surveys of degro [ 1823 ]  . individualization of rt stafng has also to be carried out by centres having specialized treatment facilities . 
their requirements need to be ascertained at the level of individual departments . a closer look at the distribution of rt facilities across the swiss cantons shows that 10 out of the 26 cantons dont have an rt facility . 
however , in future , some of these cantons ( depending on their respective population ) could have satellite rt centres linked via telenetworking to the existing rt centres of the adjacent cantons . 
these could be run with limited rt staff from the main centre ; thereby also ensuring quality - assured rt care [ 31 , 32 ]  . the rt stafng details described here are limited to ros , mps and rtts , as the recommendations for these categories are listed in estro - quarts and the iaea guidelines . however , other staff members , such medical dosimetrists and rt nurses , are also an integral part of the rt departstrahlenther onkol ( 2016 ) 192 : 599608 ments . 
furthermore , with the widespread use of networking in the present - day rt departments , there is a growing need for dedicated information technology personnel in rt departments to assist in the day - to - day working . 
although no specic guidelines are available , individual departments would have to decide their own norms to ensure a seamless workow and optimal rt care . the present estimates are based on the available data from the public domains of the databases used . 
future efforts may therefore be needed in this direction . conclusion switzerland , with a very efcient and high standard of health care , could well adapt to the challenges of an estimated 9.8 % increase in rt requirements as expected over the next 5 years . 
taking into account the changing rt practices , the present paper provides the necessary insight that could assist all major stakeholders and health planners to design appropriate strategies for meeting future rt needs . this could provide effective and sustainable rt services on a long - term basis , tailor - made to the countrys requirements . compliance with ethical guidelines conict of interest n.r. 
simeonova - chergou1 carsten herskind1 frederik wenz1 frank lohr1 received : 20 december 2015 / accepted : 15 june 2016 / published online : 8 july 2016 springer - verlag berlin heidelberg 2016 abstract aim ct morphologic and histopathologic alterations have been reported after sbrt . 
we analyzed the correlation of mri morphologic alterations with radiation doses to assess the potential for mri - based doseeffect correlation in healthy liver tissue . patients and methods mri data of 24 patients with liver metastases 73 weeks after image - guided sbrt in deepinspiration breath - hold were retrospectively analyzed . 
beam path doses of 3842 gy ( eqd2 , / = 23 ) induce characteristic mri morphologic alterations . keywords stereotactic body radiation therapy liver metastases deep inspiration breath - hold magnetic resonance imaging normal tissue reactions mr - morphologische vernderungen nach lebersbrt direkte dosiskorrelation mit intermodalen matching zusammenfassung ziel ct - morphologische vernderungen nach sbrt sind beschrieben und korrelieren mit histopathologischen vernderungen . 
ziel war es , mrt - morphologische vernderungen mit den bestrahlungsdosen direkt zu korrelieren und aussagen zur dosis - wirkungs - korrelation im gesunden lebergewebe zu treffen . patienten und methoden bildgebungsdaten von 24 patienten mit lebermetastasen 7 3 wochen nach bildgefhrter sbrt in computergesttztem atemanhalt wurden retrospektiv analysiert . 
die absolutdosen wurden unter annahme eines / - werts von 2 und 3 fr 642 strahlenther onkol ( 2016 ) 192 : 641648 toxicity , which is typically very minor , as a consequence of strict dosevolume constraints established early in most institutional protocols [ 1 , 10 , 11 ]  . 
usually only minimal changes in liver laboratory values in the acute phase are observed which mostly normalize in the chronic phase after treatment [ 1 , 11 , 12 ]  . few studies describe radiological alterations after liver radiotherapy . 
ct morphologic alterations after sbrt have been reported and they can be correlated to histopathologic alterations [ 1316 ] with vod ( veno - occlusive disease ) being the main nding [ 14 ]  . 
 [ 15 ] characterized sharply dened changes in the healthy liver tissue in contrast - enhanced multiphasic ct beginning at a median of 3 months post - sbrt and disappearing 9 months later . 
increasing radiation dose was linearly correlated with lower post - sbrt normal liver tissue density based on hounseld unit change [ 17 ]  . a threshold dose for signicant density change ( 7 ( cid : 2 ) hu ) was observed in the range of 3035 gy nominal dose . 
eine randstndige kontrastmittelaufnahme wurde ab den isodosenlinien von nominell 46 , 9 15 , 3 gy , eqd2gy / / = 10 90 , 5 28 , 3 gy beobachtet . 
auerhalb des hochdosisbereichs traten im bereich des strahleintritts scharf begrenzte vernderungen auf , die direkt mit den isodosenlinien korrelierten : t1 - intensittsnderung bei den isodosenlinien von nominell 21 , 9 6 , 7 gy ( eqd2 , / = 2 42 , 5 8 , 7 gy , eqd2 , / = 3 38 , 5 7 , 6 gy und eqd2 , / = 8 30 , 2 6 , 3 gy ) ; t2 - hyper - / hypointensitt ab isodosen von nominell 22 , 4 6 , 6 gy ( eqd2 , / = 2 42 , 7 8 , 1 gy , eqd2 , / = 3 38 , 7 7 gy und eqd2 , / = 8 30 , 5 5 , 9 gy )  . schlussfolgerung charakteristische mrt - morphologische vernderungen zeigen die ersten post - sbrt - mrts . 
diese daten erlauben erstmalig eine direkte , durch deformierbares matching genau ortsund dosisaufgelste quantizierung von nebenwirkungen durch bildgebende vernderungen nach teilorganbelastung bei sbrt . schlsselwrter stereotaktische krperbestrahlungstherapie lebermetastasen tiefer atemanhalt magnetresonanzbildgebung normalgewebereaktionen introduction stereotactic body radiotherapy ( sbrt ) for liver metastases and hepatocellular carcinoma ( hcc ) results in excellent local control rates [ 13 ]  . 
novel radiotherapy techniques such as fast ig - imrt ( image - guided intensity - modulated radiotherapy ) with fff ( attening - lter - free ) delivery have made this modality a fast and well - tolerated therapy option [ 4 ]  . radiation tolerance of healthy liver tissue and the biliary system for the whole organ and normofractionated treatment has been studied and reported [ 57 ] with td5 / 5 and td50 / 5 for rild ( radiation - induced liver disease ) being 2832 gy and 4043 gy [ 8 ] , respectively , though no systematic imaging data are available . 
most published sbrt studies only report clinical strahlenther onkol ( 2016 ) 192 : 641648 methods and materials patients a total of 24 patients with liver metastases of various primaries ( 11 colorectal cancer , 5 breast cancer , 2 melanoma , 1 gastrointestinal stromal tumor , 2 prostate , 1 gastric cancer , 1 renal cell carcinoma , 1 pancreas ) were treated with imageguided sbrt [ 1 ] ( in computer - controlled deep inspiration breath hold [ dibh ] )  . 
planning and delivery of ig - sbrt was performed as published previously [ 1 ] : planning ct scans were acquired with a spiral - ct ( somatom volume zoom ; siemens , germany ) with i . 
contrast , in the portal - venous phase after an initial training session in dibh with the active breathing coordinator ( abc , elekta ab , sweden ) [ 30 ]  . 
patients were treated on a linac with 6 mv photons ( synergy , elekta )  . daily image - guidance was performed with cbct ( elekta xvi ) and stereotactic ultrasound ( bat , nomos , usa ) at setup and stereotactic ultrasound at least once intrafractionally , with all image acquisitions performed in ( repeated ) breath - hold [ 30 , 32 ]  . 
prescription dose ( median dose to the ptv ) was adjusted during the reported period and varied between single - fraction doses of 2628 gy initially ( depending on tumor and liver volume ) and hypofractionated regimens with the current , nal protocol prescribing 5 fractions of 12 gy every other day ( 13 patients )  . 
all patients received mri 23 months after sbrt as rst follow - up . mri images before and 7.7 3 weeks after sbrt were retrospectively analyzed . if available , further follow - up mris and additional ct / pet data were also analyzed . 
retrospective evaluation for all mri images was approved by the local ethical committee . mr hardware in - house examinations were performed on a whole - body 3.0 tesla mr scanner ( skyra , siemens healthcare , germany )  . 
if no in - house mris were available , external mri data were received as dicom data and were evaluated by two experienced liver radiologists on osirix dicom viewer ( osirix 64 - bit version 3.7.1 , the osirix foundation , geneva , switzerland )  . 
gd - dota ( dotarem , guerbet , 22 patients ) and gadoxetic acid ( primovist , bayer schering pharma , 2 patients ) were used for contrast enhancement [ 33 , 34 ]  . 
precontrast , arterial , portalvenous and venous - phase images were acquired in transversal orientation , followed by a coronal venous phase vibe . when gadoxetic acid was used ( 2 patients ) , late hepatobiliary phase coronal and axial vibes were acquired 10 and 20 min after contrast injection , respectively . 
in the external mri examinations , similar parameters were used , 3d gre t1 - weighted and t2 - weigthed ultrafast tse sequences with slice thickness not more than 5 mm were available in all scans . 
the comparison between rt dose and mri alterations has been done by two independent radiologists and two radiation oncologists . the linear - quadratic model was used to convert absolute doses to eqd2 , / = x ( equivalent dose in 2 gy single doses for a given / , ( eqd2 , / = x = dx ( d + / ) / ( 2 gy + / ) ) [ 36 , 37 ] ) for each patient . 
postcontrast , t1 - weighted intensity changes were observed for the same patients for the same isodose lines ; however , 14 patients showed postcontrast hypointesity and 8 hyperintensity . the hyperor hypointensity could not be correlated to the administered contrast media , primary tumor , dose level or fractionation pattern . 
t2 - hypointensity was observed in 4 patients , hyperintensity in 18 patients . chronic radiological alterations long - term follow - up mr images ( 6 months3 years ) were only available for 10 patients . 
in 5 cases , the observed alterations persisted but had shrunk in diameter and retraction of the lesion borders ( most likely due to brotic reaction ) made the rendered matching less unequivocal ( missing tissue )  . 
the underlying pathology might have been strictures of bile ducts in the high - isodose areas . in 3 patients , alterations stayed identical or several distant liver metastases appeared . results patient characteristics , eqd2 , / = x for tumor and matching results all patients received chemotherapy ( various regimens according to primary disease , predominantly 5 - uorouracil [ 5 - fu ] - based ) at various time points before sbrt . 
1 patient example : a t1 - weighted coronal mri image , b t1 - weighted transversal mri , c t2 - weighted transversal mri , all 6 weeks - post rt with deformably registered dose distribution from the planning ct . 
correlations between imaging changes and dose are largely qualitative with few attempts at precise quantication that until recently have been hampered by methodical difculties . very few studies report mri - based radiological alterations after partial liver radiotherapy , especially after sbrt with also no systematic mri data being available data after whole - liver radiotherapy . 
mri morphologic and functional alterations based on t1 - weighted gre enhanced by hepatocyte - targeted gd - eob - dtpa were described 6 weeks after ct - guided interstitial brachytherapy [ 1921 ] at mean liver threshold doses of 1419 gy depending on use of experimental liver - protective drugs in a prospective trial . postbrachytherapy t1 - weighted hypointensity ( loss of hepatocyte function ) and t2 - weighed hyperintensity ( edema ) was observed at an isosurface area of 9.4 gy [ 1921 ]  . 
however , due to steep dose gradients and almost no dose load to healthy liver tissue in brachytherapy , a direct doseresponse correlation in the low dose regions is not possible . after cyberknife - sbrt , normal tissue adc values in diffusion weighted mri have not shown signicant changes between preand postinterventional mri [ 22 ]  . 
hypointense areas in gd - eob - dtpa - enhanced mri were observed with the largest extension 3 months post - sbrt at median threshold doses of 28 gy [ 3 ]  . 
quantication is likely more precise than in other series as a consequence of the methodology ( dibh treatment planning , treatment and breath - hold follow - up mri ; deformable registration then reliably allows direct spatial correlation of dose and imaging changes )  . 
this is supported by the morphological appearance of the sharply dened pattern of radiological changes indicating a precise dose application . up to now , no eqd2 data for doses causing radiological alterations in healthy liver tissue have been reported . 
given that we cannot rule out that livers in the patients treated had previous damage though less likely in a predominantly metastatic setting than in primary hepatocellular carcinoma , we calculated both tolerance doses of 3842 gy eqd2 , / = 23 for healthy liver ( / = 2 gy and 3 gy ) and 30 gy eqd2 , / = 8 for presumably predamaged liver ( / = 8 gy ) to model the reaction of predamaged tissue . however , in the cohort reported here , no patients with previous liver disease like hepatitis or cirrhosis were present . these data can provide a basis for individual liver dose constraint estimation . the shown imaging changes show probably functionally compromised regions of the liver , which can be volumetrically measured . 
based on these data , the amount of functionally healthy residual liver tissue can be approximated and threshold doses ( this manuscript as a rst attempt ) can be determined to fully exploit the potential of novel delivery techniques [ 45 ]  . t1 - hypointensity in postcontrast venous phase imaging might be related to both parenchymal edema and reduced perfusion in the irradiated liver parenchyma , where vod was found to be a major underlying pathology responsible for reduced contrast enhancement in ct studies [ 14 ]  . 
this strahlenther onkol ( 2016 ) 192 : 641648 lower nominal dose can be due to several factors : given the different prescription / fractionation regimens in different series , nominal dose may be different but eqd2 , / = x may be more similar . 
beyond this issue , mri with liver - specic contrast media is probably more sensitive to detect liver cell damage than noncontrast imaging [ 46 ] or even contrast - enhanced ct . finally the breath - hold application results in a nonblurred interface region between damaged and nondamaged liver tissue ( particularly vertically ) which can be more precisely matched by deformable matching . conclusions characteristic radiogenic changes occur in the rst postsbrt mri . 
based on deformable matching , these data allow a direct spatial and dosimetric correlation and quantication of sbrt - induced changes in healthy liver tissue . these data may aid in the choice of individual treatment planning constraints ( table 1 )  . acknowledgements parts of these studies were supported by a rejbh was supported by the search grant from elekta ab , sweden . ministerium fr bildung und forschung , baden - wrttemberg and the esf ( european social funds ) during the study . 
ziel dieser studie ist die systematische bewertung der beziehung zwischen den ausgangswerten im blutbild und dem therapieerfolg bei patienten mit rektumkarzinom , die properativ mit radiochemotherapie behandelt wurden . patienten und methoden zwischen den jahren 2009 und 2015 wurden die daten von insgesamt 173 patienten mit lokal fortgeschrittenem rektumkarzinom retrospektiv analysiert . 
in contrast , tumor growth may affect systemic immune processes throughout the whole organiscancer - related inammation inuences cell proliferation , survival , migration , invasion , and metastasis [ 2 ]  . 
as sir is associated with outcome in a variety of malignancies , understanding these processes and the recognition of the current state of the inammatory response prior to cancer treatment may be an important prognostic and predictive factor for clinical outcome [ 3 ]  . 
active ongoing inammation affects blood counts rst , so this parameter can be easily used to monitor acute and chronic inammatory responses [ 4 ]  . one widely accepted inammation - based prognostic score system in oncological diseases is the glasgow score system ( gps ) , which is based on an increased concentration of circulating c - reactive protein and hypoalbuminemia . gps was found to be a useful , independent prognostic factor in cancer patients [ 5 , 6 ]  . 
the disadvantage of this system is the fact thatunlike with a full blood count or differential leukocyte countthese two blood parameters are not routinely measured prior to treatment [ 7 ]  . the most important hematological parameters , with regard to having an impact on preoperative treatment in locally advanced rectal carcinoma , are hemoglobin levels [ 8 ]  . 
similarly , the ratio between circulating neutrophils and leukocytes ( nlr ) is also important [ 9 ]  . in contrast , thrombocytosis is considered a negative predictive parameter [ 10 ]  . the role of neutrophils in sir is understood as protumorigenic . 
1 patient and tumor characteristics and their impact on survival ( log - rank test / cox univariate regression analysis ) n = 173 characteristics gender age ( years ) diabetes mellitus cvs disease clinical t stage clinical n stage tumor grade tumor location circular vs . 
only a simple blood test is required . in the present study , we focused on patients with locally advanced rectal carcinoma who underwent neoadjuvant chemoradiotherapy followed by surgical resection . the principal objective was to assess the relationship between response and pretreatment blood values representative of the state of sir . 
the main points of interest were the neutrophil - to - lymphocyte ratio ( nlr ) , platelet - to - lymphocyte ratio ( plr ) , and initial hemoglobin ( hb ) and platelet levels . 
these parameters have been investigated individually in various malignancies [ 14 , 15 ] and their impact on long - term outcomes after curative intent has been also demonstrated [ 16 ]  . patients and methods between january 2009 and january 2015 , 173 patients ( 120 men and 53 women ) with local advanced , histologically veried rectal adenocarcinoma were treated with neoadjuvant chemoradiotherapy . 
clinical tumor staging ( ct stage and cn stage ) was based on physical examination , endoscopy and endosonography , pelvic mri ( magnetic resonance imaging ) , abdominal ct ( computed tomography ) , and lung x - rays . detailed patient and tumor characteristics and their impact on survival are summarized in tab . 
the baseline blood count and leukocyte differential count were analyzed in all patients one week before the start of chemoradiation . treatment preoperative chemoradiation consisted of external beam radiation at a dose of 45 gy in 25 fractions ( single fraction of 1.8 gy ) over a 5 - week period ( mondaysfridays ) with a further external beam boost to the tumor ( 5.4 gy in 3 fractions )  . 
all patients received pelvic radiotherapy with either the four - eld box technique ( anterior to posterior , posterior to anterior and two laterals ) , the three - eld technique ( posterior to anterior and two laterals ) or imrt ( intensity - modulated radiotherapy ) with megavoltage photon beams ( 6 or 18 mv ) from a linear accelerator ( varian medical systems , palo alto , ca , usa )  . 
2 shows treatment response characteristics with corresponding impact on os ( overall survival ) and dfs ( diseasefree survival )  . postoperative chemotherapy was applied in 141 ( 83.4 % ) patients , while 24 ( 14.8 % ) patients had no adjuvant chemotherapy ; in the remaining 3 patients , palliative treatment began shortly after surgery . statistical analyses basic descriptive statistics were used for the analysis : median , mean , range , standard deviation , and 95 % condence interval ( 95 % ci ) for continuous data , and absolute and relative frequencies for categorical data . 
all statistical analyses were performed using ncss 8 statistical software program ( ncss , keysville , ut , usa )  . within a median follow - up of 35.0 months ( range 5.676.9 months ) , 22 ( 12.7 % ) patients died and in 34 ( 19.7 % ) disease had progressed . 
the rate of pcr was not signicantly dependent on the baseline nlr in our patients . eosinophils , basophils , and monocytes counts were not signicant for survival ( os nor dfs ) or for treatment response prediction . only the baseline rbc count ( p = 0.0001 ) , hemoglobin ( p = 0.0130 ) , and neutrophils ( p = 0.0465 ) remained signicant for os in the multivariate cox regression analysis , which incorporated clinical and pathological t staging and n staging , t and n downstaging , pathological tumor characteristics , and baseline hematological characteristics inuencing os in univariate analyses . 
the results were based on a prein our opinion , vious clinical trial at our institute [ 17 ]  . pretreatment blood counts correlate well with the actual state of sir and can , therefore , be used as a predictive and prognostic parameter of overall response . undoubtedly , the most important hematological parameter , as expected , was the pretreatment levels of hemoglobin and absolute erythrocyte count . it appears that overall survival is signicantly negatively affected by the presence of anemia before and during treatment ( hemoglobin level was correlated by gender )  . 
relatively higher levels of hemoglobin and erythrocytes are signicant predictors of pathological response after neoadjuvant chemoradiotherapy . the greatest benet of normal hemoglobin levels has been demonstrated for squamous cell cancers treated with radiation therapy . 
in addition , anemia was identied as an important predictive factor inuencing tumor response , os , and risk of local recurrence in rectal cancer [ 8 , 20 ]  . 
although some authors recommend using blood transfusions [ 23 ] , recent studies suggest that the clinical effect of interventions with transfusion and erythropoietin stimulating agents is not an efcient way to improve outcome [ 24 ]  . we have identied initial pretreatment thrombocytosis as a negative independent prognostic factor for os and dfs . analogous to changes in leukocytes and erythrocytes levels is thrombocytosis , a manifestation of abnormal immune system activation and a sign of ongoing sir due to the tumorhost interactions . 
the secretory platelet function is very extensive , including adhesive , coagulation , mitogenic , angiogenic , and brinolytic factors , and participates not only in hemostasis but also in the whole inammatory response [ 25 ]  . 
other mediators facilitate intravascular tumor invasion and metastasis processes by protect circulating tumor cells against destruction by the host immunity [ 26 ]  . recent studies demonstrate that preoperative thrombocytosis in colorectal cancer signicantly correlates with the tumor size , depth of invasion , and poor prognosis [ 27 ] , as well as with the venous invasion , response rate and grade of pathological response to preoperative chemoradiotherapy [ 10 ]  . 
in accordance with previous published literature , we believe that these very complex changes in physiological processes signicantly affect os and dfs , as indeed has been demonstrated in our study . 
such conditions result in the formation of antitumor microenvironment and activate the immune system to inhibit tumor growth . it also manifests as normal or reduced platelet levels in the peripheral blood count . strahlenther onkol ( 2016 ) 192 : 632640 the interrelationship of neutrophils and lymphocytes reects the current setting of the immunity and its ability to defend itself against the ongoing cancer growth . 
lymphopenia is , thus , a hallmark of impaired cell - mediated immunity and , in combination with an absolute decit of leukocytes , leads to weakening of antitumor immunity and facilitation of tumor progression . 
neutrophilia may further potentiate vegf production and consequently accelerate tumor progress [ 28 ]  . the level of tumor inltrating lymphocytes ( til ) , specifically cd3 + , cd8 + , and cd45ro + cells , is an important prognostic value in various cancers [ 13 ]  . 
similarly , blood level of neutrophils represents an occurrence of tumor inltrating neutrophils ( cd10 + cells )  . these immune phenomena have also been investigated in lung cancer [ 30 ] or esophageal cancer [ 31 ]  . 
further studies with large patient cohorts are required to conrm our hypothesis about a link between til and nlr , especially in colorectal cancer . many studies have demonstrated the impact of elevated nlr on the prognosis of colorectal cancer regardless of the primary treatment modality . 
 [ 34 ] has described the positive effect of an increased level of circulating lymphocytes on complete tumor eradication . the cause may be the retrospective analysis of our cohort ; in a prospective study there would be exclusion of some patients with serious comorbidities and the elimination of the possible impact of these diseases on the overall response and also on pcr . conclusion the knowledge of pretreatment hematological parameters appears to be an important prognostic factor in patients with rectal carcinoma . 
perhaps in the future it could be used to determine the course of optimal treatment . acknowledgements this work was supported by charles university faculty of medicine in hradec krlov grant prvouk [ prvoukp 37 / 06 ]  . compliance with ethical guidelines conict of interest m . 
fietkau1 received : 1 february 2016 / accepted : 8 june 2016 / published online : 5 july 2016 springer - verlag berlin heidelberg 2016 abstract aim following mastectomy and adjuvant external beam radiation therapy in patients with breast cancer , the incidence of local or locoregional recurrence is approximately 9 % ( 220 % )  . 
in the present work , a retrospective analysis of salvage brachytherapy combined with supercial hyperthermia for chest wall recurrences is presented . patients and methods between 2004 and 2011 , 18 patients with a total of 23 target volumes resulting from chest wall recurrences after previously mastectomy and external beam radiation therapy ( median 56 gy , range 5068 gy ) were treated with supercial brachytherapy as salvage treatment : 8 patients ( 44 % ) had macroscopic tumor , 3 ( 17 % ) had microscopic tumor ( r1 ) , and 7 ( 39 % ) had undergone r0 resection and were treated due to risk factors . 
in all , 5 of 23 patients ( 22 % ) received additional concurrent chemotherapy , and in 20 of 23 ( 87 % ) target volumes additional supercial hyperthermia was carried out twice weekly . results the 5 - year local recurrence - free survival was 56 % , the disease - free survival was 28 % , and a 5 - year overall sur ( cid : 2 ) v . 
27 , 91054 erlangen , germany 2 department of radiation oncology , hospital fuerth , fuerth , germany 3 department of gynecology and obstetrics , university hospital erlangen , erlangen , germany vival was 22 % . 
late side effects common toxicity criteria ( ctc ) grade 3 were reported in 17 % of the patients : 2 of 18 ( 11 % ) had ctc grade 3 brosis , and 1 of 18 ( 6 % ) had a chronic wound healing disorder . conclusion re - irradiation as salvage brachytherapy with supercial hyperthermia for chest wall recurrences is a feasible and safe treatment with good local control results and acceptable late side effects . keywords radiotherapy quality of life hyperthermia , induced neoplasm recurrence , local mastectomy re - bestrahlung der brustwand bei lokalen brustkrebsrezidiven ergebnisse der salvage - brachytherapie mit hyperthermie zusammenfassung ziel nach einer mastektomie und adjuvanter strahlentherapie bei patientinnen mit mammakarzinom kommt es bei 9 % ( 220 % ) zum lokalen bzw . 
im folgenden wird eine retrospektive analyse der ergebnisse der re - bestrahlung als salvage - brachytherapie beim brustwandrezidiv vorgestellt . patienten und methode in den jahren 2004 bis 2011 wurden 18 patientinnen mit insgesamt 23 zielvolumina aufgrund eines thoraxwandrezidivs nach bereits frher erfolgter mastektomie und perkutaner strahlentherapie . ( median 56 gy , spanne 5068 gy ) mit einer salvageoberchen - brachytherapie behandelt 44 % patientinnen mit makroskopischem tumor , 17 % in einer r1 - situation und 39 % nach einer r0 - resektion aufgrund von risikofaktoren . 
die applizierte dosis betrug 50 gy ( high - dose rate 618 strahlenther onkol ( 2016 ) 192 : 617623 table 1 patient characteristics ( n = 18 ) age ( median , range ) dose of primary ebrt ( median , range ) time interval between primary ebrt and salvage brachytherapy ( median , range ) histology invasive ductal invasive lobular tumor burden at the time of salvage brachytherapy previous chemotherapy previous antihormone therapy number of recurrences prior to salvage brachytherapy distant metastasis at time of re - irradiation simultaneous chemotherapy with salvage brachytherapy used drugs for simultaneous chemotherapy and salvage brachytherapy ebrt external beam radiation therapy , gy gray , 5 - fu 5 - uorouracil [ hdr ] und pulsed - dose rate [ pdr ] )  . 
in 5 / 23 ( 22 % ) fllen wurde eine simultane chemotherapie durchgefhrt , bei 20 / 23 ( 87 % ) zielvolumina auerdem 2 - mal wchentlich eine oberchenhyperthermie . ergebnisse das lokalrezidivfreie 5 - jahres - berleben betrug 56 % , das krankheitsfreie 5 - jahres - berleben 28 % und das 5 - jahres - gesamtberleben 22 % . 
bei 17 % der patientinnen wurden chronische nebenwirkungen nach den common toxicity criteria ( ctc ) vom grad 3 beobachtet , darunter 2 / 18 patientinnen ( 11 % ) mit einer fibrose ctc grad 3 und eine patientin ( 1 / 18 , 6 % ) mit einer chronischen wundheilungsstrung . schlussfolgerung die salvage - brachytherapie beim thoraxwandrezidiv als re - bestrahlung in verbindung mit oberchenhyperthermie stellt eine durchfhrbare und sichere behandlung mit guter lokaler kontrolle und akzeptablem nebenwirkungsprol dar . schlsselwrter strahlentherapie lebensqualitt induzierte hyperthermie lokaler neoplasierckfall mastektomie in patients with breast cancer after mastectomy , adjuvant external beam radiation therapy and systemic treatment , the incidence of local or locoregional recurrence is approximately 9 % ( 220 % ) [ 1 , 2 ]  . 
approximately one third of these patients already have distant metastases by the time of local recurrence , approximately one third develop metachronous distant metastases , and one third have an isolated , local / locoregional tumor recurrence [ 35 ]  . in patients with isolated local recurrence , surgery is usually performed . 
with surgical options being limited , the most effective local treatment is external beam radiation therapy , especially in isolated local recurrences where treatment is performed with curative intent [ 1 , 6 ]  . 
regardless of whether the therapeutic intent for local breast cancer recurrence is curative or palliative , one of the most important aims of salvage brachytherapy is to improve quality of life . 
hence , efforts should also be made to control the symptoms locally in the palliative setting . thus , a retrospective analysis of the results from protocol - based re - irradiationsalvage brachytherapy combined with supercial hyperthermiain breast cancer patients with local chest wall recurrences is presented . strahlenther onkol ( 2016 ) 192 : 617623 fig . 
1 typical arrangement of moulage and corresponding dose distribution of supercial pulsed - dose rate ( pdr ) brachytherapy in patient with chest wall recurrence patients and methods between 2004 and 2011 , a total of 18 patients were treated with salvage brachytherapy for chest wall recurrence ( table 1 )  . 
the total prescribed dose in all patients was 50 gy . the total dose was administered in 21 of 23 patients ( 91 % ) treated target volumes using a split course of pdr brachytherapy with 2 treatment sessions ( 2 25 gy , singlepulse dose dp = 0.40.6 gy / h / 24 h ) ; in 2 patients with large affected skin area using a split course of pdr brachytherapy with 3 sessions ( 3 1617 gy , dp = 0.3 gy / h ) ; 1 patient ( 1 of 23 , 4 % ) or hdr brachytherapy with a single dose of 2 gy . 
the rationale for leaving a treatment - free interval was to minimize the risk of potential late side effects to allow recovery of the surrounding healthy skthe median area of skin treated was 215 cm ( range 98346 cm )  . 
in 5 of 23 target volumes ( 22 % ) , concurrent chemotherapy was performed in patients with a macroscopic tumor , good compliance , and ecog score of 01 . 
in 20 of 23 target volumes ( 87 % ) all patients with good compliance supercial hyperthermia was additionally performed twice weekly with a target temperature of 43 c covering the whole tumor , if possible , for 70 ma dedicated supercial heating system ( bsd 500 supercial hyperthermia system , bsd medical corp . , salt lake city , ut , usa ) was used . 
2 typical clinical arrangement of supercial brachytherapy of the thoracic wall strahlenther onkol ( 2016 ) 192 : 617623 the hyperthermia system and the skbolus temperature usually was 40 c . statistics the kaplanmeier method was used to calculate the probability of local control and survival , and a log - rank test was used to compare the subsets . 
adverse effects were documented in accordance with version 3 of the common toxicity criteria ( ctc ) [ 11 ]  . results the median interval between primary external beam radiation therapy and re - irradiation using supercial salvage brachytherapy was 64.5 months ( range 10234 months )  . the median follow - up for surviving patients is 5.7 years ( minmax : 24108 months ) , for all patients 2.2 years ( minmax : 4108 months )  . the indication for re - irradiation in 8 of the 18 patients ( 44 % ) was a recurrent , inoperable macroscopic tumor . 
salvage brachytherapy was then indicated in 3 patients ( 3 of 18 , 17 % ) because a r1 resection and in 7 patients ( 7 of 18 , 39 % ) after r0 resection due to risk factors ( close resection margins , extensive recurrence , multiple recurrence )  . 
of the 18 patients , 5 ( 28 % ) received treatment after the rst recurrence , 8 of 18 ( 44 % ) after the second recurrence , and 5 of 18 ( 28 % ) after 3 or more recurrences . 
at the time of treatment , 13 of 18 patients ( 72 % ) had an isolated local recurrence , and 5 of 18 ( 28 % ) were found to already have distant metastases . 
in the remaining patients without distant metastases no immediate adjuvant systemic treatment was performed after salvage brachytherapy with hyperthermia . at the time of treatment , a macroscopic tumor was identiable in 12 of 23 target volumes ( 52 % )  . 
 [ 13 ] demonstrated that re - irradiation using supercial brachytherapy resulted in good local control with 1 , 2 , and 3 years of local relapse - free survival of 89 , 81 , and 75 % in case of microscopic and 96 , 85 , and 71 % with macroscopic tumor burden , respectively . 
e. , patients with macroscopic and microscopic tumor burden , as well as the risk factors described above ( close resection margins , extensive recurrence , and multiple recurrences )  . 
in our analysis , 17 % of patients developed late side effects of ctc grade 3 : 2 patients developed brosis ( 11 % ) and 1 patient developed a wound healing disorder ( 6 % )  . 
thus , it seems that the results of both analyses are comparable with respect to efcacy and in terms of the toxicity prole , but the total number of patients of both groups is too low for any valid statistical analysis with sufcient statistical power . additional hyperthermia in combination with irradiation is without a doubt the second important treatment modality improving the chances of local control especially in previously irradiated patients with locally recurrent breast cancer [ 1418 ]  . 
all these data are supported by a meta - analysis of ve randomized trials [ 21 ]  . an important treatment option for strictly local chest wall recurrence is salvage surgery generally considered to be the rst - line local salvage treatment . 
the preferred surgical method is radical chest wall resection ( full - thickness chest wall resection ) [ 22 , 23 ] or simple tumor resection ( wide soft - tissue resection ) [ 24 ]  . 
late ctc grade 3 effects were documented in 3 of 18 patients ( 17 % ) : 2 ( 11 % ) had ctc grade 3 brosis , and the other ( 1 of 18 , 5.5 % ) a chronic wound healing disorder . discussion analysis of the results of salvage radiation therapy in isolated local recurrences after mastectomy shows that initial nodal involvement is a risk factor for local recurrence . furthermore age < 50 years and salvage therapy without chemotherapy were found to be relevant risk factors for distant recurrence [ 12 ]  . 
during last 15 years , a number of retrospective analyses of surgical treatment for chest wall recurrence have been published which , as expected , are also been based on small case numbers . 
salvage brachytherapy offers those patients results comparable to salvage surgery . for patients in the palliative setting , salvage brachytherapy is a therapeutic option that effectively alleviates the prevailing symptoms with good local control without exposing patients to potential serious risks during and after salvage therapy . compliance with ethical guidelines conict of interest a . 
juli 2016 springer - verlag berlin heidelberg 2016 hintergrund gliome vom who - grad ii treten in der regel bei jungen erwachsenen auf und sind zumeist mit progredienten neurologischen deziten sowie einer eingeschrnkten lebenserwartung assoziiert . 
in der vorliegenden arbeit werden die langzeitergebnisse berichtet . patienten und methode eingeschlossen wurden patienten mit astrozytomen , oligoastozytomen sowie oligodendrogliomen vom who - grad ii , < 40 jahre alt nach biopsie originalpublikation buckner jc , shaw eg , pugh sl et al ( 2016 ) radiation plus procarbazine , ccnu , and vincristine in low - grade glioma . 
patienten , die mit bestrahlung und chemotherapie behandelt worden waren , berlebten signikant lnger als nach alleiniger strahlentherapie ( 11 , 3 vs . 7 , 8 jahre ; p = 0 , 003 )  . 
als gnstige prognostische faktoren in der cox - analyse zeigte sich die kombination von bestrahlung und chemotherapie und das vorliegen eines oligodendroglioms , und zwar sowohl fr das progressionsfreie als auch fr das gesamtberleben . schlussfolgerung der autoren patienten < 40 jahre , die biopsiert oder teilreseziert sind und patienten 40 jahre , unabhngig vom resektionsstatus , berleben nach einer kombinationsbehandlung aus strahlentherapie und pcvchemotherapie im vergleich mit einer alleinigen strahlentherapie signikant lnger ( progressionsfrei und auch insgesamt )  . strahlenther onkol ( 2016 ) 192 : 672674 kommentar ber viele jahre wurden patienten mit niedriggradigen gliomen postoperativ abhngig von etablierten risikofaktoren behandelt . 
whrend mit letzterer studie die hypothese widerlegt wurde , dass die orale chemotherapie der strahlentherapie berlegen sei und somit formal negativ verlief , konnte fr die gruppe der who - grad - iii - gliome eine therapieintensivierung als vorteilhaft identiziert werden : langzeitergebnisse zweier rtogund eortc - studien zeigten bereits einen vorteil durch bestrahlung mit sequentieller applikation von pcv hinsichtlich des gesamtberlebens bei grad - iii - gliomen mit 1p / 19q - deletion [ 2 , 4 , 5 ]  . mit der vorliegenden arbeit knnen , in zusammenschau der studienergebnisse fr who - grad - iii - gliome , drei hypothesen fr niedriggradige gliome als widerlegt betrachtet werden , und nachfolgende sachverhalte erarbeitet werden : 1 . 
die frhzeitige behandlung von patienten mit whograd - ii - gliomen verbessert und verlngert das progressionsfreie berleben nicht , wie viele jahre postuliert . langfristig geht die behandlung aber mit einer verlngerung des gesamtberlebens einher , was im falle einer tumorprogression durch eine erneute , noch so effektive therapie nicht ausgeglichen werden kann [ 1 , 3 ]  . wie sollte nun eine mageschneiderte therapie fr patienten mit who - grad - ii - gliomen im tglichen alltag aussehen ? viel diskussion gibt es zur notwendigkeit von pcv , das als kombinationstherapie auch mit nebenwirkungen einhergehen kann wie insbesondere myelosuppression und allergische reaktionen . 
die verfgbarkeit des oralen medikaments temozolomide ( tmz ) , das bei initiierung der vorliegenden studie noch nicht gegeben war , hat sich als teil der kombinierten radiochemotherapie als mgliche alternative zu pcv etabliert . 
interessante ergebnisse , die aus einer randomisierten studie zu who - grad - iii - gliomen gewonnen wurden , zeigen eine differentielle effektivitt von tmz und pcv in abhngigkeit von molekularen faktoren , insbesondere vom 1p / 19q - status , was auf eine differenzierte wirkung der beiden chemotherapieregime hinweist [ 6 , 7 ]  . 
daher knnte beispielsweise bei patienten mit who - grad - ii - gliomen mit 1p / 19q - kodeletion eine kombination von pcv und strahlentherapie favorisiert werden , whrend bei abwesenheit einer 1p / 19q - kodeletion tmz und bestrahlung ebenso effektiv zu sein scheint . 
obgleich in der vorliegenden rtog - studie der 1p / 19q - status bisher nicht mitgeteilt wurde , ist ein solches analoges vorgehen aufgrund der vorhandenen datenlage sicherlich vertretbar . fazit die diagnose eines who - grad - ii - glioms sollte unabhngig vom histologischen subtyp , alter und resektionsstatus als indikation fr eine frhe behandlung gesehen werden , nach mglichkeit bestehend aus einer strahlentherapie und chemotherapie . 
bent mj van den et al ( 2013 ) adjuvant procarbazine , lomustine , and vincristine chemotherapy in newly diagnosed anaplastic oligo674 strahlenther onkol ( 2016 ) 192 : 672674 dendroglioma : long - term follow - up of eortc brain tumor group study 26951 . 
bent mj van den et al ( 2005 ) long - term efcacy of early versus delayed radiotherapy for low - grade astrocytoma and oligodendroglioma in adults : the eortc 22845 randomised trial . 
prabhu rs et al ( 2014 ) effect of the addition of chemotherapy to radiotherapy on cognitive function in patients with low - grade glioma : secondary analysis of rtog 98 - 02 . 
we also examined a new dvh parameter , because the unresected lung should be more spared than the later resected lung . patients and methods data from 43 non - small cell lung cancer patients were retrospectively analyzed . 
the dvh parameters of the lung were calculated from the total bilateral lung volume minus ( 1 ) the gross tumor volume ( dvhg ) or ( 2 ) the later resected lung volume ( dvhr )  . 
zudem wurde ein neuer dvhparameter untersucht , da das nichtresezierte lungengewebe mehr geschont werden sollte als reseziertes gewebe . patienten und methoden daten von 43 patienten mit nichtkleinzelligem bronchialkarzinom wurden retrospektiv analysiert . 
die dvh - parameter der lunge wurden aus dem gesamten beidseitigen lungenvolumen minus ( 1 ) das makroskopische tumorvolumen ( dvhg ) oder ( 2 ) das resezierte lungenvolumen ( dvhr ) ermittelt . 
strahlenpneumonitis ( rp ) und fisteln , einschlielich bronchopleuraler und pulmonaler fisteln , wurden als pulmonale komplikationen nach graden abgestuauerdem erfolgte eine analyse der faktoren , welche die inzidenz einer rp von grad 2 oder hher ( g2 rp ) und von fisteln beeinussen . ergebnisse bei 16 patienten ( 37 % ) wurde eine rp g2 festgestellt , wobei der v20 - wert des gesamtlungenvolumens minus dem spter resezierten lungenvolumen ( v20r ) 12 % ein signikanter einussfaktor bezglich der inzidenz einer rp g2 war ( p = 0 , 032 )  . 
prolonged air leakage , pneumonia , atelectasis , and bronchopleural stula were reported as the common postoperative pulmonary complications of nacrt [ 2 ]  . bronchopleural stula in particular is a life - threatening complication , and its prevention by identifying risk factors associated with the incidence of stula is critical [ 3 , 4 ]  . 
of the factors that could potentially affect the relationship between radiotherapy ( rt ) and the incidence of postoperative pulmonary complications , only the total dose of rt has been reported as a risk factor [ 5 , 6 ]  . 
there are no published studies investigating the relationship between pulmonary complications and dosevolume histogram ( dvh ) parameters . radiation pneumonitis ( rp ) is another major pulmonary complication after thoracic rt . 
in patients treated with denitive rt , tolerance radiation doses of the lung were assessed using dvh parameters by the quantitative analyses of normal tissue effects in the clinic review [ 7 ]  . 
however , the tolerance dose in patients treated with nacrt is still unclear . at the authors institution , nacrt is performed for patients with resectable cn2 / 3 non - small cell lung cancer based on the promising results of an in - house prospective trial [ 8 ]  . 
furthermore , a new dvh parameter was also evaluated , because the unresected lung after surgery should be spared more than the later resected lung . patients who received nacrt at the authors institution between august 2008 and november 2013 were retrospectively analyzed . 
the eligibility criteria of this study were as follows : histologically conrmed nonsmall cell lung cancer ; rt performed with a dose of 50 gy in 25 fractions ; administration of concurrent chemotherapy with rt ; and the surgery performed after completion of nacrt . 
written informed consent was obtained from each patient before treatment . the institutional review board approved this retrospective study . treatment the planning computed tomography ( ct ) scan was obtained under free breathing with a scan time of 3 s per section . 
gross tumor volume ( gtv ) was dened as the primary tumor volume plus the volumes of metastatic lymph nodes that were clinically diagnosed by a ct or uorodeoxyglucose positron - emission tomography scan . 
the planning target volume included the ctv plus 810 mall patients received three - dimensional conformal rt planned by pinnacle3 version 8.0 m ( philips healthcare , andover , ma , usa )  . 
the prescribed dose at the isocenter was 50 gy with 2 gy per fraction once daily , using a 6 - mv photon beam delivered by a linear accelerator . chemotherapy was concurrently administered with rt based on the results of in - house prospective trials [ 8 , 9 ]  . the regimens were selected mainly according to the status of biomarkers . 
a summary of the selection criteria is as follows : ( i ) patients with a tubulin - negative carcinoma received platinum and docetaxel ; ( ii ) patients with a thymidylate synthase - negative and tubulin - positive non - squamous carcinoma received platinum and pemetrexed ; ( iii ) patients with a thymidylate synthase - negative and tubulin - positive squamous carcinoma received platinum and s - 1 ; ( iv ) when all biomarkers were positive or when the patient was allergic to the assigned drug , the alternative selection was docetaxel or the second - best drug . 660 strahlenther onkol ( 2016 ) 192 : 658667 fig . 
an open thoracotomy was performed . bronchial stumps were covered with the pedicle fat pad or intercostal muscle ap in principle . evaluation rp and stula , including bronchopleural and pulmonary stula , were graded according to the common toxicity criteria for adverse events ( ctcae ) version 4.0. 
the incidences of rp and stulas were related to the total lung dvh either under consideration of the gross tumor only ( g - sufx ) , or by considering the later resected parts of the lung ( r - sufx )  . 
the mean lung dose ( mld ) and the percentage of the lung volume that received more than 550 gy in increments of 5 gy ( v5v50 ) were analyzed as dvh parameters . statistics the relationship between dvh parameters and the incidences of grade 2 or higher rp ( g2 rp ) and stula were analyzed for all patients using the wilcoxon signed - rank test . 
the wilcoxon signed - rank test was also performed to compare the incidence of pulmonary stula between patients treated with bilobectomy or lobectomy , because the pulmonary stula occurred in the unresected lung of the operated side . we evaluated the factors affecting g2 rp and stula in univariate analysis using fishers exact test and in multivariate analysis using multiple logistic regression . 
the software program jmp 11 ( sas institute , cary , nc , usa ) was used for all statistical analyses . results patient characteristics and dosevolume histogram parameters in total , 43 patients were included in this study . 
clinical stage according to the 7th edition of the union for international cancer control tnm classication was iia in 3 patients , iib in 3 , iiia in 32 , iiib in 4 , and iv in 1 patient . 
2 comparison of a v5gv50g and b v5rv50r values by wilcoxon signed - rank test for the patients with or without grade 2 or higher radiation pneumonitis ( g2 rp )  . 
v5gv50g percentage of total lung volume minus gross tumor receiving more than 550 gy , v5rv50r percentage of total lung volume minus later resected parts receiving more than 550 gy radiation pneumonitis fistula of the 43 patients , 16 ( 37 % ) experienced g2 rp : 13 had grade 2 , 2 had grade 3 , and 1 patient had grade 5 . 
v5gv50g percentage of total lung volume minus gross tumor receiving more than 550 gy , v5rv50r percentage of total lung volume minus later resected parts receiving more than 550 gy results of the comparisons of v5gv50g and v5rv50r values in patients with or without a pulmonary stula ( treated with either bilobectomy or lobectomy ) are shown in fig . 
the average v40g and v5rv50r values were signicantly higher in patients with pulmonary stulas . discussion to the best of the authors knowledge , this is the rst study to investigate the relationship between pulmonary complications and dvh parameters in patients with non - small cell lung cancer treated with nacrt . 
the incidences of rp and stulas were related to the total lung dvh either under consideration of the gross tumor only ( g - sufx ) or the later resected parts of the lung ( r - sufx )  . 
the authors developed the dvhr because the unresected lung after surgery 666 strahlenther onkol ( 2016 ) 192 : 658667 should be spared more than the later resected lung following nacrt and surgery . 
the current comparison of patients with or without g2 rp by the wilcoxon signed - rank test revealed signicant differences in dvhr but not in dvhg . the authors suggest that this is because postoperative rp occurs in the unresected lung , and the dvhg may thus be insufciently sensitive for rp prediction . 
therefore , the authors think that the dvhr can be mostly estimated at the time of rt planning using the planned resected lung . lobectomy was a signicant factor affecting g2 rp in the present univariate analysis , possibly because patients treated with lobectomy have larger unresected lung volumes and are thus more likely to experience rp postoperatively . 
however , the previous dvh data were not reported in the setting of nacrt , and thus the results of the present study cannot be compared with those of previous investigations . 
in a literaturebased meta - analysis [ 11 ] , age and tumor location were reported as clinical risk factors for rp , but these factors were not signicant in our study . although they are separated in the ctcae , both bronchopleural and pulmonary stula are major life - threatening postoperative pulmonary complications . 
performance status [ 2 ] and tumor location [ 3 , 4 ] were also reported as risk factors for stula , and indeed both an ecog - ps of 1 and tumor location in the lower lobe were signicant factors affecting stula incidence in univariate analysis in the present study . 
of the 6 patients who exhibited a stula in the present study , 5 had the tumor located in the right lung , and 4 patients underwent pneumonectomy or bilobectomy , although no signicant differences were observed . considering the dvh parameters examined , a v35 value of the total lung minus the gross tumor ( v35g ) 19 % and v40g 16 % were signicant factors affecting stula incidence in univariate analysis . 
as for the relationship between the bronchial stump and nacrt , yamamoto et al . [ 12 ] reported that the preoperative bronchial mucosal blood ow was signicantly lower in patients treated with nacrt than in patients without preoperative therapy , and that healing of the bronchial stump was also poor in patients treated with nacrt . 
therefore , stula may have occurred in our patients because of poor stump healing . regarding the relationship between radiation dose and healing of the bronchial stump , inui et al . [ 13 ] reported the results of preoperative irradiation followed by bronchial anastomosis . 
although their report was of a non - human study using a single fraction , the results suggest that > 35 gy of the conventional fractionation may increase the incidence of stula through dehiscence of the stump . 
the dose of approximately 3540 gy may be related to the incidence of stula . it was observed in the present that the pulmonary stula occurred in the unresected lung of the operated side . patients treated with a bilobectomy or lobectomy had the unresected lung of the operated side . 
the dvhr may be useful for the prediction of pulmonary stulas ; however , a pulmonary stula occurred in only 2 of the patients in the present series , and conrmation thus is required . this study had a number of limitations . 
shibata state that there are no conicts of interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
jacobs1 gerhard bogner1 alfons staudach1 horst koch1 pia wolfrum - ristau1 christiane schausberger1 thorsten fischer1 felix sedlmayer2 received : 5 april 2016 / accepted : 18 may 2016 / published online : 27 june 2016 the author ( s ) 2016 . 
this article is available at springerlink with open access abstract background mesonephric adenocarcinoma of the vagina is an extremely rare tumor of the female genital tract , with only a few cases reported so far worldwide . 
following surgical excision , histologic analysis determined mesonephric adenocarcinoma of the vagina , stage pt2 r1 . in order to avoid the mutilating extended surgery which would be required to reach r0 and considerable impairment of quality of life , adjuvant radiochemotherapy was administered with external radiation and brachytherapy , including 5 cycles of cisplatin ( 40 mg / m ) for radiosensitization . 
after 4 years of continuous oncologic follow - up , the patient is alive and clinically free of disease . conclusion in this case it was shown that adjuvant radiochemotherapy with radiation and brachytherapy was effective to manage the surgical r1 situation and maintain ( cid : 2 ) iris mueller i.haberlehner@salk.at 1 department of obstetrics and gynecology ( ob / gyn ) , paracelsus medical university ( pmu ) , mllner hauptstr . 
48 , 5020 salzburg , austria 2 department of radiology and radiation oncology , paracelsus medical university ( pmu ) , mllner hauptstrasse 48 , 5020 salzburg , austria the patients life quality . 
more published cases reports are needed to gradually substantiate optimal treatment strategies . keywords quality of life diethylstilbestrol brachytherapy radiochemotherapy radiotherapy das mesonephrische adenokarzinom der vagina diagnostik und multimodale behandlung eines seltenen tumors und analyse der weltweiten erfahrung zusammenfassung hintergrund das mesonephrische adenokarzinom der vagina ist ein uerst seltener tumor des weiblichen genitaltrakts . 
das biologische verhaltensmuster dieses tumors und dessen prognose sind weitgehend unbekannt . methoden in diesem bericht wird ein neuer fall einer 54jhrigen frau mit einem mesonephrischen adenokarzinom der vagina vorgestellt und unter bercksichtigung aller bisher publizierten flle analysiert . ergebnisse bei dem 2 , 5 1 , 8 cm groen tumor der vaginalwand zeigte sich in der magnetresonanztomographie eine inltration der urethra und harnblase . 
um diese massive einschrnkung der lebensqualitt zu vermeiden , wurde eine adjuvante radiochemotherapie mit externer bestrahlung und brachytherapie mit 5 zyklen cisplatin ( 40 mg / m ) zur strahlensensibilisierung durchgefhrt . 
die strahlenther onkol ( 2016 ) 192 : 668671 im 4 - jahres - follow - up beschwerdefrei und patientin ist ohne rezidivgeschehen . schlussfolgerung in diesem fall ist die adjuvante radiochemotherapie mit brachytherapie die bestmgliche strategie , um auf die chirurgische r1 - situation einzugehen und dabei die lebensqualitt der patientin zu erhalten . 
weitere fallberichte sind ntigt , um optimale behandlungsstrategien zu etablieren . schlsselwrter lebensqualitt diethylstilbestrol brachytherapie radiochemotherapie strahlentherapie background mesonephric adenocarcinoma ( ma ) of the vagina is a rare tumor of the female genital tract , with only six cases listed in medline as of march 2016 ( table 1 )  . 
a few more reports on ma occurring in the cervix , uterus , and urinary bladder , including pediatric patients , have been published [ 13 , 6 , 7 , 14 , 16 ]  . the rst link between adenocarcinoma of the vagina and intrauterine exposure to diethylstilbestrol ( des ) was described in 1971 [ 11 ]  . 
des is an orally administered active synthetic estrogen which was routinely given to selected pregnant woman from about the 1940s to the 1960s , in the mistaken belief it would reduce the risk of pregnancy complications and losses . 
follow - up studies demonstrated that exposure to des in utero causes a spectrum of congenital anomalies in females , cervical and vaginal adenosis being those most commonly found [ 13 ]  . 
mas exhibit a variety of morphologic patterns and may therefore be confused with immunomixed mllerian tumors and other neoplasms . histochemical ndings may help to distinguish mas from their mllerian counterparts [ 2 ]  . 
many of the reported cases were previously categorized as mesonephric carcinoma and are now reclassied as clear - cell carcinoma of mllerian type . we present the case report of a 54 - year - old woman with ma of the vaginal wall invading urethra and bladder and describe the course of treatment . gynecologic case presentation a 54 - year - old caucasian woman ( 1g 1p 1 gravida , 0 para ) was referred to the obstetrics / gynecology department because of vaginal bleeding after cohabitation . 
in pelvic mri , invasion of the urethra and the urinary bladder by the tumor was described , without any evidence of suspect lymph nodes . a cystoscopy showed no pathologic ndings . 
microscopically , the tumor showed a tubulocystic and papillary pattern , with scanty pale to eosinophilic cytoplasm with low nuclear atypia . the immunohistochemical prole of the tumor cells was positive for pancytokeratin and ck7 , but for calretinin and vimentin only focal positive . 
furthermore estrogen and progesterone receptor were negative and cd 10 was slightly positive . the nal diagnosis was ma of the vagina , stage pt2 r1 . achievement of an r0 resection would only have been possible by extended , mutilating surgery resulting in a severely impaired quality of life . 
hence , in the interdisciplinary tumor board the consecutive decision was made to treat in a conservative approach by adjuvant radiotherapy including sensitization with cisplatin in analogy to treatment strategies for gynecological adenocarcinoma [ 8 ]  . radiotherapy the planning target volume comprised the vulva , vagina , and the whole uterus , as well as bilateral inguinal , external , and internal iliac lymph nodes up to the pelvic inlet as the cranial eld border . 
the entire length of the vaginal mucosa including the whole introitus was treated with an additional overall surface dose of 22 gy in two treatment courses in weekly distance , each of them comprising three fractions of 3.5 gy ( bid ) or 4 gy ( once daily ) on two consecutive days . 
radiosensitization was performed with concomitant chemotherapy consisting of ve cycles of cisplatin ( 40 mg / m ) once per week throughout the ebrt course , up to an overall dose of 329 mg at an individual body surface area of 1.67 m , according to common schedules for adjuvant treatment regimens in cervical carcinoma and following the suggestions of a previous case report [ 7 ]  . 
the patient is alive and clinically free of disease at 4 years of follow - up . 670 strahlenther onkol ( 2016 ) 192 : 668671 table 1 clinical characteristics of patients with mesonephric adenocarcinoma of the vagina reported in the literature . 
not known adjuvant treatment follow - up ned 4.5 years discussion mesonephric adenocarcinoma of the vagina is a rare entity and any knowledge about is it therefore very limited . prognosis , biologic behavior , and treatment strategies are controversially discussed and due to the rareness of the disease , there is no established standard therapy . 
therefore , many cases previously categorized as ma have been reclassied as clear - cell carcinomas or malignant mixed mllerian tumors , and vice versa [ 17 ]  . the mllerian and wolfan ducts originate from mesodermal tissue . 
in females the mllerian ducts develop to form the fallopian tubes , uterus , cervix , and upper two - thirds of the vagina ; whereas in males they regress . 
mas may arise out of these remnants [ 15 ]  . compared to the malignant mixed mllerian tumor , it seems that mas located in the female genital tract have a better prognosis [ 2 ]  . however , the optimal management strategy for ma remains uncertatreatment recommendations can evolve only gradually , based on episodic reports and , in principle , derived in analogy to allegedly comparable oncologic constellations . 
radical surgery is suggested as a potentially curative option , particularly when malignant lesions appear well capsulated [ 3 ]  . in this patient , ro resection would have only been possible by extended surgery with subsequent functional losses . 
g. , vaginal cancer [ 4 ]  . conclusion despite a limited current follow - up time of 4 years , this favorable disease course supports the hypothesis that these rare tumors are sensitive to adjuvant chemoradiation . 
adjuvant treatment should be considered in cases with a higher probability of microscopic remnants , thus potentially also avoiding mutilation without compromising oncologic outcome . open access funding provided by paracelsus medical university compliance with ethical guidelines conict of interest i . 
sedlmayer state that there are no conicts of interest . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki decstrahlenther onkol ( 2016 ) 192 : 668671 laration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . open access this article is distributed under the terms of the creative commons attribution 4.0 international license ( creativecommons.org / licenses / by / 4.0 / ) , which permits unrestricted use , distribution , and reproduction in any medium , provided you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons license , and indicate if changes were made . strahlenther onkol ( 2016 ) 192 : 157165 doi 10.1007 / s00066 - 015 - 0910 - 7 stereotactic intracavitary brachytherapy with p - 32 for cystic craniopharyngiomas in children mohammad maarouf faycal el majdoub manuel fuetsch mauritius hoevels ralph lehrke frank berthold jrgen voges volker sturm received : 23 june 2015 / accepted : 23 september 2015 / published online : 5 november 2015 springer - verlag berlin heidelberg 2015 abstract purpose although microsurgery remains the first - line treatment , gross total resection of cystic craniopharyngeomas ( cp ) is associated with significant morbidity and mortality and the addition of external irradiation to subtotal resection proves to achieve similar tumor control . 
with this retrospective analysis , the authors emphasize intracavitary brachytherapy using phosphorus - 32 ( p - 32 ) as a treatment option for children with cystic cp . patients and methods between 1992 and 2009 , 17 children ( median age 15.4 years ; range 718 years ) with cystic cp underwent intracavitary brachytherapy using p - 32 . 
three patients showed progression of the treated cystic formation ( in - field progression ) after a median time of 8.3 months ( range 5.310.3 months ) , which led to subsequent interventions . 
the overall progression - free survival was 75 , 63 , and 52 % after 1 , 3 , and 5 years , respectively . conclusion intracavitary brachytherapy using p - 32 represents a safe and effective treatment option for children harboring cystic cp , even as primary treatment . 
however , p - 32 does not clearly affect growth of solid tumor parts or the development of new cystic formations . keywords pediatrics intracavitary brachytherapy phosphorus - 32 survival treatment outcome progressionsfreie berleben betrug 75 , 63 und 52 % nach 1 , 3 und 5 jahren . schlussfolgerung die intrakavitre brachytherapie mit p - 32 stellt eine sichere und effektive behandlungsoption fr kinder mit zystischen kraniopharyngeomen , sogar als primrtherapie , dar . 
jedoch zeigt sich kein eindeutiger effekt auf solide tumoranteile , sowie auf die entwicklung neuer tumorzysten . schlsselwrter kinderheilkunde intrakavitre brachytherapie 32phosphor berleben behandlungserfolg stereotaktische , intrakavitre brachytherapie mit p - 32 zur behandlung zystischer kraniopharyngeome bei kindern zusammenfassung zielsetzung obwohl die mikrochirurgie die methode der wahl darstellt , ist die komplette resektion zystischer kraniopharyngeome hufig mit einer signifikanten morbiditt und mortalitt assoziiert . 
mit dieser retrospektiven studie wollen die autoren die intrakavitre brachytherapie mit radioaktivem phosphor - 32 ( p - 32 ) als eine behandlungsoption bei kindern mit zystischen kraniopharyngeomen hervorheben . patienten und methoden zwischen 1992 und 2009 wurden 17 kinder ( medianes alter 15 , 4 jahre ; spanne 718 jahre ) mit zystischen kraniopharyngeomen durch eine intrakavitre brachytherapie mit p - 32 behandelt . 
mrt - aufnahmen zeigten solitre zysten bei 7 patienten , whrend 10 patienten gemischt solide - zystische lsionen aufwiesen ( medianes tumorvolumen 11 , 1 ml ; spanne 0 , 578 , 9 ml )  . 
die mediane nachbeobachtungszeit betrug 61 , 9 monate ( spanne 16 , 9 196 , 6 monate )  . ergebnisse eine lokale kontrolle der tumorzyste konnte bei 14 patienten erreicht werden ( 82 % )  . 
bei 3 patienten zeigte sich ein progress der behandelten zysten ( in - field progression ) nach einer medianen nachbeobachtungszeit von 8 , 3 monaten ( spanne 5 , 310 , 3 monaten ) , was nachfolgende interventionen notwendig machte . 
das craniopharyngiomas ( cps ) are benign , epithelial tumors arising either from embryogenic remnants of the craniopharyngeal duct ( adamantinomatous type ) or as a neoplasia of adenohypophyseal tissue ( squamous papillary type ) [ 1 , 2 ]  . 
however , due to their bimodal age distribution ( one peak during childhood , the other at the age of 5074 years ) , they represent the most common nonglial pediatric brain tumor , accounting for 5.615 % of central nervous system ( cns ) tumors in children [ 3 , 4 ]  . 
 cps embrace a cystic component in approximately 90 % of cases , [ 5 , 6 ] dividing the pathologies in radiological subtypes solitary cysts , solid tumors , and mixed solid and cystic tumors , as described in the previously published data [ 7 ]  . although cps are histologically benign , their aggressive , recurrent behavior and proximity to critical structures such as the hypothalamus , pituitary stalk , and parts of the optic pathway lead to a high impact on the patients quality of life with regard to endocrine and visual dysfunction as well as to symptoms of increased intracranial pressure [ 8 , 9 ]  . several reports have shown that intracavitary irradiation with colloidal , - emitting sources such as phosphorus - 32 ( p - 32 ) or yttrium - 90 ( y - 90 ) seem to be successful in the treatment of cystic cp while minimizing procedure - related morbidities [ 6 , 7 , 10 ]  . based on previously published reports p - 32 emerged as a favorable - emitting source due to its short range of tissue penetrance and steep dosage decline [ 7 , 1015 ]  . this retrospective study shows the long - term efficacy of intracavitary brachytherapy using p - 32 achieving a high local tumor control and an improved clinical outcome in pediatric patients with cystic cp . 
 mri revealed solitary cysts in 7 patients ( 41 % ) , while the remaining patients ( 59 % ) suffered from mixed solidcystic tumors inducing clinical status deterioration through an increment of their cystic portion . the most common initial symptoms leading to subsequent diagnosis were headache ( n = 8 ) , visual acuity or field deterioration ( n = 7 ) , followed by nausea / vomiting ( n = 3 ) , growth retardation ( n = 3 ) , amenorrhea and hemiparesis of the left upper limb in one patient each , respectively . 
similar to the approach reported in our previous study , diagnosis was either established by histological examination in patients who underwent prior surgical resection or microscopic examination of the aspirated fluid of the tumor cyst in the group treated primarily [ 7 ]  . 
further patient characteristics , including pretreatment clinical conditions and type of interventions prior to intracavitary brachytherapy , are summarized in table 1 . surgical procedure intracavitary brachytherapy was performed a median of 1.7 months ( range 05.3 months ) after initial diagnosis in the group treated primarily and 7.6 months ( range 4.8128.6 months ) after the last surgical procedure in the salvage treatment group . under general anesthesia , the patients head was fixed in a modified riechertmundinger stereotactic frame . 
in order to establish the optimal surgical approach and to determine the cysts volume , image fusion of an intraoperative , contrast - enhanced cranial ct ( slice thickness 1.25 mm ) and a preoperatively conducted axial contrast - enhanced t1and t2 - weighted mri ( slice thickness 1.5 mm ) was performed by anatomical landmark correlation using stp 3.5 software ( howmedica / leibinger gmbh , freiburg , germany ) [ 7 , 12 , 13 , 16 , 17 ]  . 
1 shows a representative treatment plan . after blunt penetration of the cyst wall using a thin cannula ( 0.9 mm in diameter ) , additional volumetry was performed by the application of technetium - 99m ( tc - 99m )  . 
with a0 representing the required radiation activity ( mci ) , this formula not only shows the obvious dependence of the activity of the lesion volume ( v ) , but also reports a variation of the factor f in the treatment of different lesion sizes , with f = 0.455 being exclusively reliable for cyst volumes of 7.5 ml [ 15 ]  . 
in all 17 patients undergoing intracavitary irradiation , the cyst volume was reduced by a median of 24.8 % compared to the initial size ( range 040 % ; table 2 )  . due to the small volumes of the required phosphate for the delivered activity of 5 mci / ml , we prepared a solution of phosphate / glucose 30 % in order to ease administration , similar to previously published reports [ 6 , 7 , 12 ]  . 
following the final instillation of p - 32 , we conducted scintigraphic imaging through a - camera investigation in two sections ( coronal , sagittal ) immediately after the procedure and repeatedly during the first postoperative days in order to exclude dispersal of the - emitting source outside the cp cyst [ 7 ]  . follow - up our follow - up schedule consists of mr imaging 3 months after intracavitary brachytherapy and every 612 months thereafter . 
an observation time of greater than 10 years could be obtained in 4 patients ( table 3 )  . statistical analysis statistical analysis was performed using pasw statistics 20 ( spss inc . , chicago , il , usa )  . 
the difference was considered significant , when p < 0.05. results results are summarized in table 3 . radiological response the stereotactic application of a - emitting radioactive source represents a local treatment that does not affect growth of solid tumor parts or the development of new cystic formations of cp [ 5 , 6 , 18 ]  . 
2 preoperative neuroimaging ( left ) of a 14 - year old female who presented with headache , left - sided hemianopsia , and panhypopituitaristhe sagittal t1 - weighted mr images revealed a cystic craniopharyngioma extending to the suprasellar region . 
three patients showed a progression of the treated lesion following intracavitary brachytherapy after a median time of 8.3 months ( range 510 months ) , leading to visual field deterioration and , thus , subsequent additional interventions . due to the fact that all progressions occurred during the first year after treatment , in - field progression - free survival rate was 81 % at 1 , 3 , and 5 years after treatment . 
while one of these patients underwent microsurgical resection , the remaining two were treated with stereotactical cyst aspiration and one of them additionally received a rickham catheter connected with a subcutaneously placed reservoir . 
 none of these patients underwent further interventions and their final clinical outcome , compared to prior intracavitary brachytherapy , improved in all cases . out - of - field response four patients suffered from the development of new outof - field cystic formations and one patient died in the early years of therapy due to the progression of solid tumor parts . 
in 3 of the 4 patients suffering from new out - of - field cysts , the progression leads to transient neurological deficits ( visual decline in all cases ) necessitating further treatments ( microsurgery , cyst aspiration and a secondary intracavitary brachytherapy in one case each )  . 
 none of these patients suffered from permanent neurological worsening . overall response overall progression - free survival rates ( including both in and out - of - field progression ) at 1 , 3 , and 5 years were 75 , 63 , and 52 % , respectively . neurological outcome at the time of the last clinical follow - up ( median 61.9 months ; range 16.9196.6 months ) , the neurological outcome improved in 6 and remained unchanged in 10 patients . 
 only 1 patient who already presented with severe left - sided hemiparesis and cognitive decline prior to treatment , suffered from symptom deterioration and died due to progression of solid tumor parts after 14 months . ophthalmological outcome prior to treatment , 11 patients presented either visual acuity or a visual field decline . 
the development of new endocrine dysfunctions was not associated with disease progression and involved worsening of anterior pituitary function in 3 and induction of diabetes insipidus in 1 patient . surgery - related complications there was neither surgery - related permanent morbidity nor mortality in this study . 
mild - emission outside of the circumscribed cp cyst could be detected through postoperative scintigraphic imaging in 1 patient resolving during the first postoperative days without clinical consequences . correlation statistical analysis of patient characteristics and clinical / radiological outcome did not show any correlation , except for progression - free survival in patients treated primarily with intracavitary brachytherapy compared to those in the salvage treatment group . 
patients who already underwent interventions prior to intracavitary brachytherapy proved to have a significantly lower risk ( p = 0.04 ) to develop in - field progression ( increment of the treated cyst )  . discussion in our study a control rate of the treated pediatric cp cyst of 81 % and an overall pfs of 75 , 63 , and 52 % at 1 , 3 , and 5 years were achieved . 
there was neither surgery - related permanent morbidity nor mortality . however , the optimal treatment for patientsespecially for childrensuffering from primarily cystic cp has yet to be established [ 19 , 20 ]  . 
but for all treatment procedures the main aim should be preservation of visual , hypothalamic , and pituitary function . surgery / irradiation traditionally , gross - total resection ( gtr ) has become established as a first - line treatment of cp due to its curative potential [ 21 ]  . 
however , because of extension to the suprasellar region the majority of these tumors must be removed via a transcranial approach leading to a high risk of surgery - induced deficits , mainly hypothalamic , even in experienced hands [ 2228 ]  . 
moreover , gtr does not guarantee local tumor control showing recurrent rates of 1330 % [ 23 , 26 , 29 ]  . irradiation ( ebi ) to str proved to achieve similar local control rates compared to gtr ( 21 % progression rate at 5 years for str + ebi ) alone [ 27 , 30 ] while lowering the procedure - related morbidity [ 21 , 31 , 32 ]  . 
however , especially in children , there remains concern about long - term morbidity associated with ebi , including endocrinological , cognitive , and functional outcomes as well as the development of secondary malignancies and vascular syndromes [ 31 , 33 37 ]  . 
 [ 33 ] reported that children lost 9.8 points in the full scale intelligence quotient after the first complete resection and 13.1 points after the second surgical intervention for relapse compared to a 1.25 point loss after limited resection followed by ebi . 
this led us to propose that radical and / or repeat surgeries have a negative influence on neurocognition compared to limited surgery plus adjuvant , immediate ebi . cp are less infiltrating tumors compared to gliomas with sharp borders on mr imaging . 
 [ 6 ] included 15 children of at least 16 years of age in a large patient series in 2004 , but they did not differentiate in their results between adult and pediatric patient population . subtotal resection ( str ) alone runs an even higher risk for progression of residual tumor parts ( 7190 % ) [ 21 , 27 ]  . 
 brachytherapy with p - 32 led to shrinkage of the treated stereotactic intracavitary brachytherapy with p - 32 for cystic craniopharyngiomas in children1 3 164 cysts in 10 of 12 cases . 
their follow - up period of 62 months and approach to differentiate between the response of the treated cysts and the development of new , defined cystic formations or progression of solid tumor parts is similar to ours . 
their reported cyst control rate was 67 % and the complete tumor control rate was 42 % with an overall 1 - , 3 - , and 5 - year pfs of 68 , 49 , and 31 % , respectively . conclusion with a tumor cyst control rate of 81 % and an overall pfs of 75 , 63 , and 52 % at 1 , 3 , and 5 years , respectively , we can confirm that intracavitary brachytherapy with p - 32 is a safe and effective option for the treatment of primarily pediatric cystic cp . 
since we did not experience any procedure - related morbidities in our population , we emphasize the stereotactic application of p - 32 without the additional placement of a rickham system , as this would be associated with a significantly higher risk of infections and - emitting agent leakage . acknowledgments the authors fe , vs , and mm were at the department of stereotaxy and functional neurosurgery , university hospital of cologne during conceptualization , collection , and evaluation of the study data and moved to different institutions thereafter . compliance with ethical guidelines conflict of interest m . 
sturm state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . strahlenther onkol ( 2016 ) 192 : 146155 doi 10.1007 / s00066 - 015 - 0926 - z primary glioblastoma multiforme tumors and recurrence comparative analysis of the danger signals hmgb1 , hsp70 , and calreticulin carolin muth yvonne rubner sabine semrau paul - friedrich rhle benjamin frey annedore strnad rolf buslei rainer fietkau udo s . 
gaipl received : 2 september 2015 / accepted : 11 november 2015 / published online : 8 december 2015 springer - verlag berlin heidelberg 2015 abstract purpose glioblastoma multiforme ( gbm ) is the most common and aggressive brain tumor . 
danger signals such as high - mobility group box protein 1 ( hmgb1 ) , heat shock protein 70 ( hsp70 ) , and calreticulin ( crt ) are biomarker candidates , due to their association with tumor progression versus induction of antitumor immune responses . 
a direct comparison of their expression in the primary tumor versus the corresponding relapse is still lacking for most tumor entities . patients and methods we therefore performed an expression analysis by immunohistochemistry of the danger signals hmgb1 , hsp70 , and crt in primary tumors and the corresponding relapses of 9 patients with de novo gbm . results hmgb1 was highly expressed in primary tumors with a significant reduction in the respective relapse . 
crt was generally highly expressed in the primary tumor , with a slight increase in the relapse . conclusion the combination of a decreased expression of hmgb1 , an increased expression of extracellular hsp70 , and an increased expression of crt in the relapse seems to be beneficial for patient survival . 
gefahrensignale wie high - mobility - groupprotein b1 ( hmgb1 ) , hitzeschockprotein 70 ( hsp70 ) und calreticulin ( crt ) sind einerseits aufgrund ihrer assoziation mit der tumorprogression und andererseits aufgrund der induktion von antitumor - immunantworten original article1 3 biomarkerkandidaten . 
ein direkter vergleich der gefahrensignale in primrtumoren und deren korrespondierender rezidive fehlt bisher fr die meisten tumorentitten . patienten und methoden wir fhrten daher eine expressionsanalyse der gefahrensignale hmgb1 , hsp70 und crt mittels immunhistochemie in primrtumoren und deren korrespondierender rezidive bei 9 patienten mit de novo gbm durch . ergebnisse hmgb1 war hoch exprimiert in primrtumoren und zeigte eine signifikante reduktion in den korrespondierenden rezidiven . 
crt war generell hoch exprimiert in den primrtumoren mit einem leichten anstieg in den rezidiven . schlussfolgerung die kombination einer verminderten hmbg1 - expression mit einer erhhten expression von extrazellulrem hsp70 und einer gesteigerten expression von crt im rezidiv scheint positiv fr das patientenberleben zu se hmgb1 , extrazellulres hsp70 und crt knnten gemeinsam als potentielle biomarker fr die prognose von patienten mit gbm in betracht gezogen werden . schlsselwrter hirnneoplasien hmgb1 - protein calreticulin hsp70 - hitzeschockproteine rezidiv glioblastoma multiforme ( gbm ) is the most common and aggressive malignant primary brain tumor . 
despite improved multimodal therapies comprising surgery and radiotherapy ( rt ) with concomitant and adjuvant chemotherapy ( ct ) with temozolomide ( tmz ) , the 5 - year survival rate of those patients is only 9.8 % [ 1 ]  . 
incomplete tumor resection caused by diffuse invasion of malignant cells and inherent resistance to rt and ct leads to recurrence of nearly all gbm [ 2 ]  . although the prognosis remains poor , survival is heterogeneous between individual patients . 
furthermore , the o ( 6 ) methylguanine - dna - methyltransferase ( mgmt ) promotor methylation status and isocitrate dehydrogenase 1 ( idh1 ) mutation are associated with extended survival . 
due to the heterogeneity of the treatment outcome , the immune system is most likely involved in anti - gbm responses [ 3 ]  . since gbm is a highly variable and infiltrative tumor , a personalized and systemic immune cell - based treatment approach is promising . 
promising clinical data are currently being collected with dc - based therapies of malignant gliomas [ 6 , 7 ]  . dc activation and maturation can be promoted by apoptotic and necrotic tumor cells and the release or surface exposure of danger signals [ 8 , 9 ]  . 
the induction of immunogenic cell death forms is characterized by the release or exposure of danger signals such as high - mobility group box protein 1 ( hmgb1 ) , heat shock protein 70 ( hsp70 ) , or calreticulin ( crt )  . hmgb1 is a ubiquitous and highly conserved chromatin - associated nuclear protein with a pleiotropic character . 
extracellular hmgb1 acts as a classical danger signal or damage - associated molecular pattern ( damp ) with a high affinity to the receptor for advanced glycation end products ( rage ) and toll - like receptors ( tlr ) - 2 , tlr - 4 , and tlr - 9 . 
hmgb1 is passively released by necrotic / damaged cells after rt and / or ct or actively secreted by phagocytic / inflammatory cells such as monocytes , macrophages , or natural killer ( nk ) cells . 
the hmgb1 - mediated dc maturation and activation finally lead to the elimination of tumor cells through the stimulation of tumor - specific cd4 + helper and cd8 + cytotoxic t lymphocytes , the latter through crosspresentation [ 12 ]  . 
besides the induction of a specific antitumor and t cell - mediated response , hmgb1 also acts as a pro - angiogenic cytokine , which results in a faster and larger growth of the tumor . 
thus , overexpression of hmgb1 reflects a poor prognosis , e.g. , for hepatocellular carcinoma [ 14 ] , melanoma [ 15 ] or bladder cancer [ 16 ]  . 
in contrast , preclinical data give hints that released hmgb1 is beneficial for the therapy outcome in gbm [ 17 ]  . heat shock proteins are a highly conserved , ubiquitously expressed family of molecular chaperones maintaining cellular homeostasis . 
analysis of several tumor entities together with their equivalent healthy tissue could show that surface expression of hsp70 on the plasma membrane is only found in the tumor area [ 18 ]  . 
instead , a negative correlation between hsp70 surface expression primary glioblastoma multiforme tumors and recurrence1 3 148 and os was found in patients with non - small cell lung cancer and lower rectal carcinoma [ 19 ]  . 
hsp70 in complex with tumor - derived antigens is recognized and engulfed by dcs , which can lead to cross - presentation of tumor peptides to cytotoxic cd8 + t cells [ 20 ]  . crt , a ca2 + - binding chaperone , is one of the most abundant proteins in the endoplasmic reticulum ( er ) that prevents the export of misfolded proteins . 
in contrast , colon cancer patients with a stronger crt expression show a tumor infiltration of t cells and a higher os [ 23 ]  . the overall poor prognosis for patients with gbm demands new therapeutic concepts . 
here , we examined for the first time the expression of the danger signals hmgb1 , hsp70 , and crt in biopsies of de novo gbm at initial manifestation and in corresponding in - field relapses . 
biopsy specimens from all 9 patients ( 5 men , 4 women , age 4372 years , averaged age 59.2 years ) were classified as gbm according to the world health organization ( who ) guidelines using hematoxylin and eosin staining . 
1. immunohistochemistry all biopsy samples were fixed overnight in 4 % formaldehyde and embedded into liquid paraffthen , 3 m sections were stretched in hot water , mounted onto positively charged slides ( superfrost ) , and air - dried overnight at 37 c . 
all slides were counterstained with hematoxyl positive and negative controls were used for validation . evaluation of immunohistochemical stainings immunohistochemical staining patterns of hmgb1 , hsp70 , and crt were analyzed in the tumor area . 
a quotient for every marker was calculated , setting 0 = 0 , + = 1 , + + = 2 , and + + + = 3 , divided by the number of samples . a statistical comparison was performed between the staining patterns of the primary tumor ( pt ) versus the relapse ( r ) for each marker . 
statistical analysis was performed with the mannwhitney test ( graphpad ) and statistical significance determined to p values less than 0.05. results hmgb1 expression due to immune - activating properties of hmgb1 versus its role in cancer progression , we compared hmgb1 expression in tissue sections of the primary tumor ( pt ) and the corresponding relapse ( r )  . 
two representative cases of immunohistochemical staining pattern of the pt and the corresponding r using an antibody directed against hmgb1 are shown as well as that of normal brain tissue as control fig . 
a the expression of hmgb1 in the pt compared to the r for all 9 patients and b the correlation between hmgb1 expression and time to relapse or death , respectively , are shown . 
two representative cases of immunohistochemical staining pattern of the pt and the corresponding r using an antibody directed against hsp70 are shown as well as that of normal brain tissue as control . 
biomarkers related to immunogenic tumor cell death are of great interest [ 10 ]  . surface - exposed crt , hsp70 , released hmgb1 , and various other danger signals such as atp stimulate antitumor immune responses by fostering communication between immune cells such as macrophages , neutrophils , nk cells , dcs , and t cells [ 27 ]  . 
knowledge of the expression of hmgb1 , hsp70 , and crt in the central nervous system , which was once considered as a strictly immune privileged area , is rare . 
not significant ( p = 0.9694 ) ; * p < 0.05 is significantly increased after treatment of glioblastoma cell lines with fractionated irradiation with single doses of 2 gy [ 11 ]  . 
the patient numbers in studies of patients with gbm focusing on immune therapies and immune biomarkers for gbm is in particular low due to restricted availability of corresponding biomaterial and the novelty of the approach in this special tumor entity [ 29 , 30 ]  . in the present study , we analyzed for the first time the expression pattern of the danger signals hmgb1 , hsp70 , and crt in de novo glioblastoma . 
in particular , the comparison of primary tumor biopsies and their corresponding relapses offers valuable insights into how the immunogenic potential of gbm can be modified by primary therapies ( irradiation and chemotherapy ) and how relapses differ in their immunogenic potential from primary tumors . 
furthermore , the impact of those changes on patient survival and time to relapse was assessed . our analyses revealed a high expression of hmgb1 in the pt , with a significant decrease in the r . 
for certain types of cancer , it is reported that the overexpression of hmgb1 reflects a poor prognosis , while in others a prolonged cancer - free survival was observed . 
 increased expression of crt is also observed in other tumors such as breast [ 36 ] and prostate cancer [ 37 ]  . soluble crt has been already proposed as a potential diagnostic marker for bladder [ 38 ] and lung cancer [ 39 ]  . 
in neuroblastoma , positive crt expression predicts better survival in patients with advanced - stage disease [ 40 ]  . it is well known that radiationand / or chemotherapyinduced surface exposure of crt enhances the phagocytosis of dying tumor cells by dcs and thereby fosters antitumor immune reactions [ 21 ]  . 
two representative cases of immunohistochemical staining pattern of the pt and the corresponding r using an antibody directed against crt are shown as well as that of normal brain tissue as control fig . 
not significant ( p = 0.0588 ) most accessible for dc - based immune therapies , which aim to specifically target invasive tumor cells and are capable to overcome intrinsic mechanisms of immune evasion that are observed in gbm [ 41 ]  . 
therefore , detailed knowledge of the immunogenic potential of the primary tumor and especially of recurrent tumors is crucial for the definition of the most beneficial time - point for immune therapy integration into radiochemotherapy schemes [ 42 ]  . similar to released hmgb1 and / or exposed crt , released hsp70 is capable of fostering the induction of antitumor immune responses . 
we detected a significant increase of extracellular hsp70 in the r compared to the pt , while the intraprimary glioblastoma multiforme tumors and recurrence1 3 154 cellular hsp70 showed a similar expression . 
this suggests that a beneficial microenvironment for additional dc - based immune therapies is created , since consecutively released hsp70 from the cytoplasm into the extracellular space is capable of activating dcs [ 43 ]  . conclusion our data demonstrate that hmgb1 , hsp70 , and crt are expressed in the pt and in the r of de novo gbm . 
beneficial for patient survival seems to be the combination of a decreased expression of hmgb1 , an increased expression of extracellular hsp70 , and an increased expression of crt in the r . 
in future studies , focus should be set on comparison of the local expression of the immune - modulating danger signals with the systemic presence of these danger signals in the peripheral blood . 
this has become possible because of novel elisas such as the liphsp70 elisa [ 45 ]  . in the present study , we had the unique opportunity to analyze biopsies of patients with de novo gbm at the initial manifestation as well as in the in - field relapse situation . 
gaipl state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . strahlenther onkol ( 2016 ) 192 : 182189 doi 10.1007 / s00066 - 015 - 0928 - x erectile function following brachytherapy , external beam radiotherapy , or radical prostatectomy in prostate cancer patients p . 
plasswilm received : 29 april 2015 / accepted : 20 november 2015 / published online : 28 december 2015 springer - verlag berlin heidelberg 2015 abstract background and purpose for localized prostate cancer , treatment options include external beam radiotherapy ( ebrt ) , radical prostatectomy ( rp ) , and brachytherapy ( bt )  . 
 our aim was to evaluate penile erectile function ( ef ) before and after bt , ebrt , or rp using a validated self - administered quality - of - life survey from a prospective registry . material and methods analysis included 478 patients undergoing rp ( n = 252 ) , ebrt ( n = 91 ) , and bt ( n = 135 ) with at least 1 year of follow - up and ef documented using iief5 scores at baseline , 6 weeks , 6 months , 1 year , and annually thereafter . results differences among treatments were most pronounced among patients with no or mild initial ed ( iief5 17 )  . 
overall , corrected for baseline ef and age , bt was associated with higher iief - 5 scores than rp ( + 7.8 iief - 5 score ) or ebrt ( + 3.1 iief - 5 score )  . 
considered overall , bt provided the best ef preservation in comparison to ebrt or rp . keywords quality of life erectile dysfunction brachytherapy prostatectomy radiotherapy erektile funktion nach brachytherapie , externer radiotherapie oder radikaler prostatektomie bei prostatakrebs - patienten zusammenfassung hintergrund und ziel die externe radiotherapie ( ebrt ) , die radikale prostatektomie ( rp ) sowie die brachytherapie ( bt ) stellen behandlungsoptionen fr das lokalisierte prostatakarzinom dar . 
unser ziel war es , die penile erektile funktion ( ef ) vor und nach bt , ebrt und rp mit hilfe eines validierten , vom patienten einer lebensqualittsfragebogens ausgefllten prospektiven datenbank zu beurteilen . material und methoden mit einer minimalen nachbeobachtungszeit von einem jahr wurden 478 patienten analysiert , die eine rp ( n = 252 ) , ebrt ( n = 91 ) oder bt ( n = 135 ) erhalten hatten und deren ef mit dem iief - 5score vor therapie sowie nach 6 wochen , 6 monaten , nach einem jahr und danach jhrlich ermittelt worden sind . therapiebedingten unterschiede ergebnis die grten wurden bei patienten ohne oder nur mit milder initialer ed beobachtet ( iief - 5 17 )  . 
 insgesamt hatte ein hheres alter einen negativen einfluss auf die erhaltung der ef ( korrigiert fr ausgangs - ef )  . schlussfolgerung in unserer serie verschlechterte sich die ef durch alle therapieformen . 
insgesamt bot die bt die beste ef - erhaltung verglichen mit der ebrt oder rp . schlsselwrter lebensqualitt erektile dysfunktion brachytherapie prostatektomie radiotherapie prostate cancer remains the most common nondermatologic cancer affecting men in the western world [ 1 ]  . 
because of a lack of definitive evidence demonstrating superiority in cure rates of one local treatment over another [ 2 , 3 ] , quality - of - life ( qol ) parameters are even more important [ 46 ]  . 
although local treatments focus on cure , there is a need to include ed and possible recovery of potency in their assessment [ 7 , 12 ] , especially since patients decisions are driven by many factors other than cancer cure [ 13 ]  . our aim was to perform an intention - to - treat analysis from prospectively collected data from a single institution on the functional results associated with three different treatment modalities for localized prostate cancer . 
in our study , we evaluated penile erectile function ( ef ) at baseline , and after treatment with a minimum follow - up of 12 months using a validated selfadministered patient quality - of - life survey ; we subsequently determined the impact of clinical and treatment parameters . 
 the five - item version ( iief - 5 ) of the 15 - item international index of erectile function ( iief ; [ 14 ] ) was used to quantify ed [ 15 ]  . bt with a prescribed dose of 145 gy , ebrt with a median dose of 72 gy ( 7078 gy ; the target of treatment being the prostate and the base of the seminal vesicles ) in 3d conventional four - field technique or rp between 2005 and 2013 for mostly lowintermediate risk prostate cancer based on eligibility to these treatments and treatment decision was based on patient preference . 
an age of 65 years , the median of our cohort , was used to differentiate younger from older patients . statistical analysis multinomial regression was used to explore the relationship between age , ef , and the choice of treatment . 
adjusted confidence intervals for differences between the treatments were computed from the regre ssion models , and adjusted using the holm correction [ 17 ]  . all analyses were performed in the r programming language ( version 3.0.2 ; [ 18 ] )  . 
the package lme4 [ 19 ] was used to estimate the mixed models , while the multcomp package [ 20 ] was used to compute the p - values and confidence intervals . 
however , when analyzed separately for patients with no or mild ed at baseline ( iief - 5 17 ) or worse , age was a significant predictor only for patients with worse ed ( iief - 5 < 17 ; table 2 )  . for patients with mild to no ed ( iief - 5 17 ) at baseline , differences in ef according to treatment modality persisted . 
 patients who received bt had iief - 5 scores that were on average 9.1 points higher than those treated with rp , while patients treated with ebrt had iief - 5 scores that were on average 6.9 points higher than those who received rp . 
we also observed a small , slightly nonsignificant difference between the bt and ebrt patients favoring the bt patients ( table 2 )  . differences between treatments were smaller but nonetheless significant among patients with worse ed ( iief - 5 < 17 ) at baseline . 
patients treated with ebrt had an iief - 5 that was on average 1.8 higher than that in patients treated with rp ( table 2 )  . nerve sparing ( ns ) was used in 45 % of radical prostatectomies . 
among patients treated with rp , there were no statistically significant differences in iief - 5 between those receiving unilateral or no ns , even after adjusting for iief - 5 at baseline and age ( table 2 )  . 
for patients with mild to no ed at baseline , we observed a 0.7 point higher iief - 5 among those receiving unilateral vs no ns , and a 4.4 point higher iief - 5 comparing patients receiving a bilateral and no ns . 
at the 3 - year follow - up ebrt and rp with bilateral ns were associated with worse ef than bt , but this difference was not statistically significant ( table 3 )  . discussion our study results revealed that in a large proportion of men who undergo therapy with curative intent for localized prostate cancer , ed will occur as an adverse effect . 
besides active surveillance for low - risk prostate cancers , ebrt , bt , and rp are all associated with good long - term cancer control in early stage disease [ 21 ]  . 
unfortunately , similar to cancer outcomes , little information exists in terms of randomized trial data for the evaluation of sexual qol measures following rp , bt , or ebrt . rp is known to cause immediate ed , after which recovery of potency typically occurs slowly or not at all [ 23 , 24 ]  . 
 [ 25 ] who reported an incidence of 81.1 % ed after nerve sparing surgery relative to 44.1 % in the observational ar in a recent paper , montorsi et al . 
summarizing these trials , it can be assumed that about 8095 % of patients may suffer from ed immediately after rp . ed is also a common sequelae of rt for prostate cancer , affecting approximately 3555 % of patients after ebrt [ 2729 ] and 2550 % after bt [ 3033 ]  . 
potent patients were statistically younger , had a higher pre - implant iief , were less likely to be diabetic , and were more likely to report nocturnal erections [ 34 ]  . 
a matched - pair study compared erectile dysfunction between patients undergoing dose - escalated image - guided radiotherapy ( imrt ) and high dose - rate interstitial brachytherapy ( hdr ) revealed no overall difference in erectile function with a 2 - year median follow - up [ 35 ]  . few prospective series , comparing different treatment modalities , have been reported using validated qol instruments and incorporating pretreatment functional data . 
however , beyond 8 months after treatment the proportion of men reporting severe sexual bother did not differ significantly among treatment groups , largely due to an improvement in the sexual bother score among rp patients over time . 
in 2013 , the prostate cancer outcomes study [ 8 ] reported on data from a cohort comprising 1655 men in whom localized prostate cancer had been diagnosed in 1994 or 1995 , between the ages of 55 and 74 years , and who had undergone either surgery ( 1164 men ) or ebrt ( 491 men )  . 
patients undergoing rp were more likely to have ed at 2 years ( or 3.46 ) and 5 years ( or 1.96 ) , but no significant between - group difference was noted at 15 years . 
at the 1 - year follow - up , the treatment - related difference in occurrence of ed was most pronounced in patients with good baseline ef , favoring bt and ebrt relative to rp . there were a number of limitations associated with the current study . 
second , the sample size of this prospective , single - center study was limited as compared with the sample sizes evaluated in other series , especially those with single arms . 
 bilateral , ns nerve sparing in addition , prospective data collection did not include other risk factors that may be associated with erectile function , such as smoking history , concomitant medication , diabetes mellitus , or other comorbidities [ 4245 ]  . 
 currently many centers are implementing imrt in prostate cancer [ 47 ] which has been shown to be associated with better long - term erectile function [ 48 ]  . 
considering all these shortcomings , a risk for bias cannot be excluded ; unknown factors may have influenced treatment decision , baseline ed as well the effect of individual treatments on ef . our current study also had a number of notable strengths . 
 in comparison to many other series we were able to include erectile function following brachytherapy , external beam radiotherapy , or radical1 3 188 three treatment modalities ( bt , ebrt , and rp )  . 
according to the literature the follow - up should be about 24 months , after which time the development of ed tends to stabilize , at least for the following few years [ 8 , 27 , 29 , 49 ]  . 
both surgical and radiotherapy patients were evaluated during the same time period with the same standardized questionnaire at the same institution . conclusion in our series , relative to baseline , ef was adversely affected by each treatment modality . 
the treatment - related differences in occurrence of ed was most pronounced in younger patients ( < 65 years of age ) with a good baseline ef favoring bt over other modalities . 
although not conclusive , these data enhance our existing understanding of treatment - induced ed , which is essential when counselling patients on their treatment options . compliance with ethical guidelines conflict of interest p.m. 
passwilm state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . strahlenther onkol ( 2016 ) 192 : 139145 doi 10.1007 / s00066 - 015 - 0917 - 0 radiotherapy of spinal cord gliomas a retrospective mono - institutional analysis stefanie corradini indrawati hadi vinzent hankel lorenz ertl ute ganswindt claus belka maximilian niyazi received : 24 june 2015 / accepted : 7 october 2015 / published online : 30 october 2015 springer - verlag berlin heidelberg 2015 abstract background due to the rarity of spinal cord gliomas , no consensus has been reached regarding the optimal treatment strategy . 
the aim of the present retrospective study was to identify patient and tumor characteristics and to evaluate the effectiveness of radiotherapy within this setting . patients and methods patients diagnosed with spinal cord gliomas between 2003 and 2013 and treated at the department of radiation oncology , university of munich , were retrospectively analyzed . 
simultaneous chemotherapy did not influence survival outcome . conclusion despite the aggressive treatment in the present study , the prognosis for spinal cord gliomas was still poor , with a median overall survival of 6 months . 
a combined chemoradiation treatment seems feasible and can be considered as a new treatment option in the management of spinal cord gliomas . keywords spinal cord glioma radiotherapy chemoradiation temozolomide outcome strahlentherapie bei spinalen gliomen eine retrospektive monoinstitutionelle analyse zusammenfassung hintergrund das spinale gliom stellt eine uerst seltene entitt dar . 
ziel dieser retrospektiven studie war es , die patientensowie tumorbezogenen charakteristika auszuwerten und den einsatz sowie die original article 140 rolle der strahlentherapie ( rt ) bei der behandlung von spinalen gliomen zu untersuchen . patienten und methoden es wurden retrospektiv die daten von allen patienten mit spinalen gliomen untersucht , welche von 2003 bis 2013 an der klinik fr strahlentherapie der lmu mnchen behandelt wurden . 
 bezglich der rt zeigte sich eine dosis - wirkungs - beziehung ab einer dosis von 45 gy , welche mit einem verbesserten os im vergleich zu einer bestrahlungsdosis von < 45 gy korrelierte ( p < 0 , 001 )  . 
die simultane chemotherapie hatte keinen einfluss auf das os . schlussfolgerung trotz der fortschritte im bereich der multimodalen therapie ist die prognose spinaler gliome mit einem medianen os von nur 6 monaten immer noch schlecht . 
eine kombinierte radiochemotherapie scheint machbar und kann als neue behandlungsoption bei spinalen gliomen in erwgung gezogen werden . schlsselwrter spinale gliome strahlentherapie radiochemotherapie temozolomid gesamtberleben spinal cord gliomas are rare and represent only 22 % of all spinal cord tumors [ 1 ]  . 
 the aim of the present retrospective study was to identify the patient and tumor characteristics of this rare disease and to evaluate the effectiveness of rt within this setting . patients and methods patient selection the patient database was retrospectively searched for patients diagnosed with spinal cord gliomas between 2003 and 2013 . 
clinical data , including the patients demographics , primary tumor site , extent of disease , histology , treatment modalities , and follow - up , were retrieved from the patients medical records . 
 magnetic resonance imaging ( mri ) was fused with the treatment planning ct , and a gross tumor volume ( gtv ) was delineated based on the contrast - enhancing lesion in the t1 - weighted sequence with gadolinium in cases of high - grade gliomas . 
ptv included a 2 - cm cranio / caudal margin from the gtv , including the tumor extent or edema in the t2 - weighted sequence and encompassing at least a onevertebral body margin above and below the tumor . 
the median total radiation dose was 45.0 gy ( range : 30.054.0 gy ) and the median dose per fraction was 1.8 gy ( range : 1.83.0 gy ) , on five consecutive days per treatment week . 
median age at diagnosis of the spinal cord glioma was 42 years ( range : 872 years ) ; 75 % of the patients were 50 years of age and there were three pediatric cases ( range : 817 years )  . 
isocitrate dehydrogenase 1 ( idh1 ) mutation analysis revealed four tumors with lacking idh1 mutation and one case with a mutation of the idh1 gene . treatment characteristics all patients received rt of the spinal cord glioma . 
for the remaining two patients , failure was adjacent to the irradiated volume , and the treatment comprised 35.0 gy in 14 fractions and 27.0 gy in 9 fractions . of the subgroup of patients with prior diagnosis of a cerebral glioma , four had glioblastoma multiforme and five had a low - grade or intermediate - grade glioma of the central nervous systemedian age at diagnosis of the cerebral tumor was 47.5 years ( range : 272 years )  . 
another factor associated with improved os was the diagnosis of a primary spinal cord glioma , presenting with a mean os of 79.4 months ( 95% ci : 49.9109.0 , median os has not yet been reached )  . 
2 kaplanmeier estimates of overall survival for patients with spinal cord glioma following surgery and radiotherapy ( n = 9 ) or radiotherapy alone ( n = 7 )  . 
patients receiving a total radiation dose of 45 gy had a mean os of 64.0 months ( 95% ci : 15.234.2.3 , median os has not yet been reached )  . 
3 kaplanmeier estimates of overall survival for patients with primary spinal glioma ( n = 7 ) compared with patients presenting with a metastatic deposit from a cerebral glioma ( n = 9 ) fig . 
4 kaplanmeier estimates of overall survival for patients receiving radiotherapy with a median radiation dose of 45 gy ( n = 9 ) compared with a radiation dose of < 45 gy ( n = 7 ) discussion astrocytomas and ependymomas account for the majority of spinal cord gliomas . 
because of the infiltrative nature of spinal cord astrocytomas , these lesions commonly have poorly characterized boundaries between the tumor and the adjacent normal spinal cord tissue , resulting in significant limitations for resectability [ 2 , 19 ]  . 
owing to the long natural history and the superior outcome of ependymomas , these tumors were excluded from the present study . to avoid neurological morbidity , surgical management in astrocytomas typically consists of initial biopsy with an attempt of maximal safe surgical resection . 
with recent advances in surgical techniques and improved imaging techniques , the ability to achieve partial and gross total resections has grown continually [ 4 ] and microsurgical techniques have resulted in fewer neurological impairments [ 1 ]  . 
 [ 22 ] found that os was improved by the extent of surgery in spinal cord gliomas . the optimal extent of surgical resection and the need for postoperative rt are still under debate [ 7 , 19 ]  . 
the effectiveness of postoperative rt has been proved by a number of case reports and small series [ 2 , 4 , 5 , 7 , 19 , 2325 ] , reporting significantly better survival outcome for patients undergoing rt . 
the traditional radiation dose given to spinal cord gliomas ranges between 45 and 50 gy delivered in a conventional dose per fraction of 1.82.0 gy , and is generally limited by the normal tissue tolerance dose of the spinal cord [ 3 , 26 , 27 ]  . 
the estimated risk of late radiation myelopathy is dose related , ranging from 0.2 % at 50 gy to 6 % at 60 gy , with conventional fractionation of 2.0 gy per day including the full cord cross - section [ 2628 ]  . 
recently , advances in modern rt techniques , such as intensity - modulated radiotherapy ( imrt ) , enable the physicians to maximize radiation dose to the tumor , while minimizing the dose to the surrounding normal tissue [ 7 ]  . a review of the literature showed very heterogeneous fractionation schemes and total doses delivered to spinal cord gliomas , making it difficult to draw a final conclusion regarding the optimal rt regimen [ 5 , 7 , 23 , 25 , 29 ]  . 
in contrast to some previously reported studies [ 5 , 7 ] , evaluaradiotherapy of spinal cord gliomas1 3 144 tion of the impact of radiation dose on survival in the present series revealed a statistically significant difference . 
our observation is consistent with those of several other studies , but might be influenced by a potential selection bias due to two hypofractionated rt schedules ( 10 3 gy ) used in the present cohort . 
 [ 25 ] found that a radiation dose of > 40 gy was a significant factor when correlated with local control and survival in a retrospective analysis of 37 patients . 
standard target volume definitions vary between a local treatment approach encompassing a oneto two - vertebral - body margin to the tumor [ 7 , 8 , 23 ] to more extended treatment volumes , including craniospinal rt in pediatric patients [ 31 , 32 ]  . while chemotherapy is a cornerstone in the treatment of intracranial gliomas [ 9 , 33 ] , in cases of spinal cord gliomas chemotherapy is usually reserved for patients that fail standard treatment with surgery and / or rt . 
there is an extremely limited number of retrospective series and single case reports , suggesting that regimens used in the treatment of cerebral gliomas may be beneficial in spinal cord gliomas [ 3438 ]  . 
this might , on the one hand , be influenced by the small number of patients , and on the other hand , be affected by the various rt regimens utilized in the present series . as known from other studies [ 2 , 3 , 20 , 23 ] , prognostic factors predicting clinical behavior and outcome in patients with spinal cord glioma include tumor histology , histological grade , age at diagnosis , functional status at time of presentation , and duration of symptoms . 
by contrast , the diagnosis of a primary spinal cord glioma was a highly significant factor associated with improved os as compared with patients presenting with a metastatic deposit from a cerebral glioma . 
on reviewing the other aforementioned prognostic factors , we were unable to find any statistically significant influence on os on univariate analysis . the unavoidable limitations of this retrospective study include the small sample size and the subsequently inherent potential for selection bias . 
moreover , detailed information concerning clinical presentation , pain , neurological dysfunction , or local control was lacking in the present study , thereby not allowing the desired analysis of local outcome and changes in neurologic function . 
nonetheless , the present observational study is a good source of information on patient and tumor characteristics of gliomas of the spinal cord and is very useful in providing a window into prognostic factors that predict outcome . 
furthermore , it contributes to the small amount of existing evidence on the effectiveness of rt and chemoradiation within this setting . conclusion despite the aggressive treatment of spinal cord glioma in the present study , including surgery , rt , or chemoradiation , the prognosis is poor with a short median os of 6 months . 
niyazi state that there are no conflicts of interest . strahlenther onkol ( 2016 ) 192 : 174181 doi 10.1007 / s00066 - 015 - 0916 - 1 temporal changes in tumor oxygenation and perfusion upon normoand hyperbaric inspiratory hyperoxia oliver thews peter vaupel received : 9 august 2015 / accepted : 7 october 2015 / published online : 26 october 2015 springer - verlag berlin heidelberg 2015 abstract background inspiratory hyperoxia under hyperbaric conditions has been shown to effectively reduce tumor hypoxia and to improve radiosensitivity . 
however , applying irradiation ( rt ) under hyperbaric conditions is technically difficult in the clinical setting since rt after decompression may be effective only if tumor po2 remains elevated for a certain period of time . 
the aim of the present study was to analyze the time course of tumor oxygenation and perfusion during and after hyperbaric hyperoxia . materials and methods tumor oxygenation , red blood cell ( rbc ) flux for perfusion monitoring , and vascular resistance were assessed continuously in experimental rat dssarcomas by polarographic catheter electrodes and laser doppler flowmetry at 1 and 2 atm ( bar ) of environmental pressure during breathing of pure o2 or carbogen ( 95 % o2 + 5 % co2 )  . results during room air breathing , the tumor po2 followed very rapidly within a few minutes the change of the ambient pressure during compression or decompression . 
with o2 breathing under hyperbaric conditions , the tumor po2 increased more than expected based on the rise of the environmental pressure , although the time course was comparably rapid . 
vaupel department of radiooncology and radiotherapy , tumor pathophysiology section , university medical center mainz , 55131 mainz , germany ter decompression the baseline values were reached aga rbc flux increased during carbogen breathing but remained almost constant with pure o2 , indicating a vasodilation ( decrease in vascular resistance ) with carbogen but a vasoconstriction ( increase in vascular resistance ) with o2 during hyperbaric conditions . conclusion since the tumor po2 directly followed the environmental pressure , teletherapy after hyperbaric conditions does not seem to be promising as the po2 reaches baseline values again within 510 min after decompression . keywords hyperbaric hyperoxia normobaric hyperoxia temporal changes tumor oxygenation tumor perfusion zeitliche vernderungen der tumoroxygenierung und - durchblutung whrend normound hyperbarer inspiratorischer hyperoxie zusammenfassung hintergrund inspiratorische hyperoxie unter hyperbaren bedingungen reduziert sehr effektiv die tumorhypoxie und erhht die strahlensensitivitt . 
jedoch lsst sich eine strahlentherapie ( rt ) bei berdruckbedingungen technisch nur schwer realisieren , da die bestrahlung nach der dekompression nur sinnvoll ist , wenn der tumor - po2 fr eine gewisse zeit erhht bleibt . 
in der untersuchung sollte daher der zeitverlauf der tumoroxygenierung und - durchblutung whrend und nach hyperbarer hyperoxie analysiert werden . material und methoden tumoroxygenierung , erythrozytenfluss ( als perfusionsparameter ) und gefwiderstand wurden in experimentellen ds - sarkomen der ratte mit polarographischen katheterelektroden und mittels laserdoppler - flussmessungen bei einem umgebungsdruck von original article1 3 1 und 2 atm ( bar ) whrend atmung von reinem sauerstoff oder carbogen ( 95 % o2 + 5 % co2 ) kontinuierlich erfasst . ergebnisse whrend raumluftatmung folgte der tumorpo2 sehr schnell innerhalb weniger minuten der nderung des umgebungsdrucks sowohl whrend kompression als auch dekompression . 
der po2 erreichte innerhalb von 510 min nach der dekompression wieder ausgangswerte . schlsselwrter hyperbare hyperoxie normobare hyperoxie zeitliche nderungen tumoroxygenierung tumordurchblutung tumor hypoxia is known to limit the efficacy of sparsely ionizing radiation [ 1 , 2 ] leading to a poor prognosis of patients after radiotherapy [ 3 , 4 ]  . 
furthermore , several studies have indicated that the addition of small amounts of co2 to the inspiratory gas ( carbogen containing 95 % o2 + 5 % co2 ) could improve tumor perfusion , and thereby increase the oxygen supply to the tumor [ 69 ]  . 
these results have led to combined treatment regimens ( inspiratory hyperoxia using carbogen + radiation ) , which have been tested in clinical phase 3 studies [ 1012 ]  . in most tumor entities , normobaric hyperoxia is not sufficient to eradicate tumor hypoxia completely [ 5 ] requiring the use of hyperbaric conditions in which tumor oxygenation is markedly increased [ 5 , 13 , 14 ]  . 
for technical reasons , clinical studies are much more difficult and thus have been performed in only a few institutions where irradiation in a large - dimension hyperbaric chamber was possible [ 19 , 20 ]  . 
this concept was supported by magnetic resonance ( mr ) measurements assessing the tumor oxygenation after hbo [ 28 ]  . since the concept of irradiation after hbo would offer new opportunities for improving the tumor oxygen status , the question arises of whether the po2 in the tumor remains elevated long enough after the end of the hyperbaric conditions to perform tumor irradiation . 
therefore the aim of the present study was to analyze the temporal chances in tumor oxygenation following the switch to inspiratory hyperoxia ( either by 100 % o2 or by carbogen breathing ) under normobaric conditions , followed by an increase of the ambient pressure to 2 atafter an hbo period of 30 min the atmospheric pressure was reduced to normobaric conditions and inspiratory hyperoxia was terminated . 
tumor oxygenation was followed by continuous polarographic measurements and assessment of tumor perfusion and resistance to flow by laser doppler flowmetry . materials and methods animals and tumors experiments were performed using ds - sarcoma cells implanted in male spraguedawley rats ( body weight 180 250 g ) housed in the animal care facility of the university of mainz . 
all experiments had previously been approved by the regional animal ethics committee and were conducted in accordance with the german law for animal protection and the ukcccr guidelines [ 29 ]  . 
volumes were determined by measuring the three orthogonal diameters ( d ) of the tumors and using an ellipsoid approximation with the formula : v = d1 d2 d3 / 6 . 
714 days after tumor cell inoculation . surgical procedure when tumors reached the desired volume , rats were anesthetized with sodium pentobarbital ( 40 mg / kg i.p. , nartemporal changes in tumor oxygenation and perfusion upon normoand hyperbaric inspiratory1 3 176 coren , merial , hallbergmoos , germany )  . 
a tube was inserted into the trachea through which the animals could continuously breathe one of the gas mixtures ( see next section )  . hyperbaric conditions and inspiratory hyperoxia hyperbaric experiments were performed in a six - person pressure chamber ( sauter ag , sulgen , switzerland ) that enables an ambient pressure of up to 2.1 atm during continuous operation . 
the complete equipment for animal handling , inspiratory hyperoxia , as well as po2 and red blood cell flux ( rbc ) measurements ( see below ) was located in this chamber . for assessing the dynamic changes of the parameters , the animal breathedafter an initial stabilization period either room air , 100 % o2 , or carbogen for 10 mtherefore , gases were flushed around the tracheal tube at a flow rate of approx . 
2 l / mafter 10 min , the ambient pressure was increased to 2 atm ( hyperbaric ) within 10 m the barometric pressure remained elevated for 30 min followed by a 10 - min decompression back to normobaric conditions . 
animals breathed the respective gas mixture ( room air , 100 % o2 , carbogen ) continuously from 10 min prior to hyperbaric compression until 10 min after decompression . measurement of tissue oxygenation for assessment of the temporal changes of the tumor oxygenation , mean tumor po2 was measured continuously using polarographic catheter electrodes of the clark type ( licox , gms , kiel , germany )  . 
350 in all tumors a stable pre - treatment po2 was reached within 15 mmeasured po2 values were averaged over a period of 1 m to measure the course of the arterial po2 , the licox catheter electrode was placed in the carotid artery after withdrawal of the blood pressure catheter . measurements of red blood cell flux rbc flux ( used as a perfusion parameter ) was measured using the laser doppler technique ( semiconductor laser diode , wavelength 780 nm , output power 12.5 mw , cutoff frequency 15 khz ; oxford array , oxford optronics , oxford , uk )  . 
in each tumor , rbc fluxes were obtained from three different central and peripheral locations in the tissue using steel - shafted needle probes ( outer diameter 0.5 mm ) that were inserted to a depth of 25 mm into the tissue . 
at the end of each experiment , the probes were left in place and the animal was sacrificed by an overdose of the narcotic to obtain the biological zero laser doppler signal . 
as a measure of resistance to flow , the relative tumor vascular resistance ( tvr ) was calculated from the ratio of the mean arterial blood pressure to the rbc flux ( mabp / rbc - flux )  . statistical analysis all results are presented as mean values sem . 
upon raising the ambient pressure to 2 atm , the arterial po2 followed immediately and linearly to the environmental po2 reaching po2 values of 1179 6 mmhg and 1135 8 mmhg , respectively . 
1 time course of the arterial po2 during change in the inspiratory gas ( oxygen or carbogen ) and the ambient pressure ( indicated by gray bars ) ; n = 3 for each gas . 
vaupel1 3 177 tumor oxygenation using the licox catheter electrode , which provides an averaged po2 within a relative large tissue area ( 5 mm length ) , the tumor po2 during normobaric room air breathing was 18 4 mmhg . 
with increasing atmospheric pressure the tumor oxygenation increased further but in this case more than expected from doubling the barometric pressure , resulting in a mean po2 of 319 43 mmhg . 
3 correlation of the initial po2 values at 1 atm prior to hyperbaric inspiratory hyperoxia with the increase in tumor po2 values upon change to hyperbaric conditions ( po2 from 1 to 2 atm ) ; n = 9 fig . 
6 time course of ( a ) erythrocyte flux ( n = 1011 ) , ( b ) mean arterial blood pressure ( mabp ; n = 56 ) , and ( c ) vascular resistance to flow ( n = 1011 ) upon change in the inspiratory gas ( oxygen or carbogen ) and the ambient pressure ( indicated by gray bars )  . 
after the end of hbo , the resistance stayed 1015 % above the initial control value for at least 30 min , which was , however , not statistically significant . 
 however , during the course of elevated pressure , the arterial po2 slightly decreased with o2 breathing , whereas with carbogen it further increased , finally reaching comparable values with both gases . 
these slight changes could be the result of an adaptation of the ventilatory driving force : with very high arterial po2 the o2 - dependent ventilatory stimulus decreases , while the high co2 content of carbogen will stimulate ventilation markedly . the tumor po2 increased significantly with inspiratory hyperoxia ( either with o2 or carbogen )  . 
in these studies using higher ambient pressures ( 35 atm ) than in the present experiments ( 2 atm ) , the authors described a worsening of the oxygenation in some tumors , a result not seen in the present experiments . 
the authors attributed the worsening to a compression of vessels within the outer tumor layers by the barometric pressure , which was lower in the present study . concerning the time course of oxygenation changes , our data clearly indicate that during 100 % o2 breathing the tumor po2 directly and rapidly followed the change of the gas mixture or the ambient pressure . 
since this technique assesses only the intravascular oxygenation that depends on the vascular po2 and the hemoglobin content , the latter results might be attributed to an increase in intravascular blood volume . 
since in the present carbogen experiments the inspiratory co2 level was elevated over a period of more than 1 h , large amounts of co2 were accumulated in the body . 
from henrys law and the hendersonhasselbalch equation [ 35 ] it can be calculated that even during normobaric carbogen breathing ( resulting in an arterial pco2 of about 5560 mmhg [ 9 ] ) roughly 10 l co2 are stored in the human body ( 95 % of it as bicarbonate that is in an equilibrium with co2 )  . 
this long - lasting effect has been described for normobaric conditions as well as for periods in which the vascular resistance was reduced during and after inspiratory hyperoxia depending on the co2 fraction of the respiratory gas mixture [ 9 ]  . 
with both hyperoxic gases , the vascular resistance was continuously increasing during the hyperbaric period ( but from a different initial value for 100 % o2 and carbogen )  . 
these results indicate that a teletherapy after hyperbaric conditions does not seem to be promising in the clinical setting , since the tumor po2 reaches baseline values within 510 min after decompression . 
especially in low - dose rate brachytherapy ( e.g. , for prostate carcinoma ) the radioactive implants stay in the tissue for a longer period of time [ 38 ]  . 
furtemporal changes in tumor oxygenation and perfusion upon normoand hyperbaric inspiratory1 3 180 ther studies should address whether hbo is able to augment the cytotoxic efficacy of brachytherapy . acknowledgments this study was supported by the med . 
vaupel state that there are no conflicts of interest . all national guidelines on the care and use of laboratory animals have been followed and the necessary approval was obtained from the relevant authorities . strahlenther onkol ( 2016 ) 192 : 166173 doi 10.1007 / s00066 - 015 - 0934 - z automatically gated image - guided breath - hold imrt is a fast , precise , and dosimetrically robust treatment for lung cancer patients anna simeonova - chergou1 anika jahnke1 kerstin siebenlist1 florian stieler1 sabine mai1 judit boda - heggemann1 frederik wenz1 frank lohr1 lennart jahnke1 received : 20 march 2015 / accepted : 12 december 2015 / published online : 15 january 2016 springer - verlag berlin heidelberg 2016 abstract background high - dose radiotherapy of lung cancer is challenging . 
tumor displacement increases with treatment time , which consequentially increases the treatment uncertainty . objective this study analyzed whether automatically gated cone - beam - ct ( cbct ) - controlled intensity modulated fast deep inspiration breath hold ( dibh ) stereotactic body radiation therapy ( sbrt ) in flattening filter free ( fff ) technique and normofractionated lung dibh intensity - modulated radiotherapy ( imrt ) / volumetric - modulated arc therapy ( vmat ) treatments delivered with a flattening filter can be applied with sufficient accuracy within a clinically acceptable timeslot . materials and methods plans of 34 patients with lung tumors were analyzed . 
in clinical routine , these approaches combine optimally reduced lung tissue irradiation with maximal delivery precision for patients with small and larger lung tumors . keywords imaging linear accelerators breathing cone - beam computed tomography quality assurance automatisch gesteuerte , bildgesttzte imrt im atemanhalt als schnelle , przise und dosimetrisch stabile therapie fr patienten mit bronchialkarzinom zusammenfassung hintergrund die hochdosisstrahlentherapie des bronchialkarzinoms ist eine herausforderung . 
die tumorverschiebung nimmt mit der behandlungsdauer zu , was also die behandlungsunsicherheit vermehrt . original article1 3 der vorliegenden studie wurde ( volumetric - modulated arc ziel in untersucht , ob die automatisch gesteuerte , cone - beamcomputertomographie ( cbct ) - kontrollierte , intensittsmodulierte stereotaktische strahlentherapie ( stereotactic body radiation therapy , sbrt ) im atemanhalt nach schneller tiefer inspiration ( deep inspiration breath hold , dibh ) ohne ausgleichskrper ( flattening filter free , fff ) und die mit einem ausgleichskrper applizierte normal fraktionierte intensittsmodulierte dibh - strahlentherapie / volumenmodulierte strahlentherapie mit rotation des bestrahlungsarms therapy , vmat ) der lunge mit ausreichender genauigkeit innerhalb eines klinisch akzeptablen zeitfensters angewendet werden knnen . material und methoden die bestrahlungsplne von 34 patienten mit bronchialkarzinomen wurden ausgewertet . 
 von diesen patienten erhielten 17 eine computergesteuerte sbrt mit schneller dibh und einer dosis von 60 gy ( 5 fraktionen 12 gy oder 12 fraktionen 5 gy ) in fffvmat - technik ( fff - sbrt ) jeden 2 . 
alle therapiemodalitten konnten genau appliziert werden trotz mehrerer beam - on - / - off - zyklen und waren bei mehrfachen unterbrechungen stabil . schlussfolgerung automatisch cbctkontrollierte sbrt mit schneller dibh in vmat - ffftechnik und normal fraktionierte dibh - lungen - vmat knnen mit wenigen malen luftanhalten in einem kurzen zeitfenster mit ausgezeichneter dosimetrischer genauigkeit appliziert werden . 
im klinischen alltag wird bei diesen anstzen die optimal reduzierte bestrahlung des lungengewebes mit maximaler bestrahlungsprzision fr patienten mit kleinen und greren bronchialkarzinomen kombiniert . gesteuerte schlsselwrter bildgebung linearbeschleuniger atmung cone - beam - computertomographie qualittssicherung atemanhalt lungenkarzinom stereotactic body radiation therapy ( sbrt ) has become the standard of care for patients with medically inoperable early lung cancer [ 1 , 2 ] , resulting in excellent tumor control rates of more than 90 % at 3 years with a benign toxicity profile [ 35 ]  . 
the recent randomized trial rtog 0617 reported reduced survival with dose escalation , but the fact that the local relapse rate was paradoxically higher in the high - dose arm indicates an issue with target definition which is currently being analyzed [ 8 ]  . 
dose escalation with sbrt in early lung cancer therefore has a sound basis and a benefit of dose escalation in advanced tumors cannot yet be ruled out . radiotherapy of lung tumors at high doses is , however , challenging . 
the standard remedy to compensate for target motion is appropriate setting of planning target volume ( ptv ) margins , individually chosen based on four - dimensional computed tomography ( 4d - ct )  . 
realtime target tracking or continuous patient position adjustment with a fully robotic patient positioning system with six degrees of freedom can reduce ptv margins [ 10 , 11 ]  . 
onboard imaging devices with integrated linear accelerators ( linacs ) represent a valuable tool for obtaining details of patient anatomy during radiation treatment delivery , with reduced imaging dose [ 12 ]  . 
 compared target coverage and lung tissue sparing between inspiration and expiration breath - hold intensity - modulated radiotherapy ( imrt ) plans for patients with non - small cell lung cancer ( nsclc )  . 
conversely , a mean difference of only 1.1 % ( p = 0.044 ) in the percentage of the ptv receiving 90 % of the prescription dose ( ptv90 ) was demonstrated in favor of expiration [ 13 ]  . 
these authors concluded that when using imrt , inspiration breath - hold can reduce the dose to normal lung tissue , while expiration breath - hold can improve the target coverage , although the improved lung sparing at inspiration may outweigh the modest improvements in target coverage at expiration [ 13 ]  . 
limiting treatment to deep inspiration ( deep inspiration breath hold , dibh ) thus reduces lung exposure and a treatment chain based on volume imaging and treatment under dibh also reduces treatment uncertainty [ 1618 ] and , as automatically gated image - guided breath - hold imrt1 3 168 a consequence , treatment margins , again reducing normal tissue exposure . introduced only recently as a new treatment modality for conventional linacs , flattening filter free ( fff ) delivery can dramatically accelerate low - modulation sbrt treatments . 
this renders dibh - gated treatments easier than ever , while maintaining a similar plan quality as compared to plans with a flattening filter [ 19 , 20 ]  . 
for patients undergoing sbrt , planning ct was performed after an initial training session in inspiratory breath - hold at approximately 70 % of vital capacity with the abc system ( active breathing coordinator , elekta ab , stockholm , sweden )  . 
treatment planning ct for conv - vmat was performed without dibh for the actually performed treatment , but was considered a breath - hold treatment for the purpose of this study . plan optimization was performed based on monte carlo dose calculation ( 1 % variance per plan ) with the inverse treatment planning system monaco ( elekta ab )  . 
dose prescription was performed at the median dose in the ptv with the 90 % isodose line covering the ptv and the 95 % isodose line covering the clinical target volume ( ctv )  . all plans were delivered on an linac with photon energy of 6 mev or 10 mev . 
automatic gating was performed with the abc system through the response gating interface ( elekta ab ) , with a delay between gating signal and beam activation of approximately 1 s . 
the gating setup through the abc system and the response gating interface allow running actual gating from outside the treatment roothe abc system is mobile and a connection to the gating interface can be established with a regular network cable in the control roothe gating studies were then performed with a volunteer actually triggering the system in the same way a patient would ( volunteer inhales in supine position through the abc system , passing the gating threshold )  . 
the system measures the quantity of air that the patient breathes and a balloon valve blocks the airway when a predefined threshold is reached , to prevent airflow through the spirometer when a breath - hold starts . 
the response gating interface triggers the linac upon the receipt of the signal from the abc system [ 16 , 24 ]  . fluence measurements were performed with a twodimensional ( 2d ) array detector attached directly to the gantry ( matrixx , iba dosimetry gmbh , schwarzenbruck , germany )  . 
the number of breath - hold cycles and the total delivery time with breath - hold phases of 15 or 20 s and recovery phases of 25 s were recorded during quality assurance ( qa ) procedures . the measurements were evaluated using the omnipro imrt software ( iba dosimetry gmbh ) by comparing them to the treatment plan . 
the accuracy of the delivered fluence of plans delivered under gating conditions was assessed using a global gamma index with 3 and 2 % dose differences , 3 mm dta ( distance to agreement ) , and 5 % threshold . to demonstrate the robustness against multiple interruptions at high frequency , a 3.8 - s gating window and 30 interruptions were chosen for one case . 
total slot time was approximately 13.0 min for fff - sbrt and 14.0 min for conv - vmat ( with 60 s required for the patient entering and leaving the treatment room , 240 s for patient positioning , 120 s for cbct , 90 s for matching , and finally the treatment times of 268 s for fff - sbrt and 330 s for conv - vmat plans reported above )  . 
studies have shown that patient setup based on bony anatomy may lead to underdosing of the tumor and only a soft tissue - based setup can reliably deliver the intended dose to the target [ 27 , 28 ]  . 
with the use of controlled breath - hold approaches such as dibh , the effect of breathing motion can be reduced , treatment margins can be decreased , normal lung can be spared , and dose to the tumor can be escalated [ 2931 ]  . 
this approach is an excellent option for patients receiving stereotactic treatments , where high doses are delivered . a prerequisite for establishing gated radiotherapy is dosimetric stability of fluence delivery under gating conditions . 
the beam - on times computed from the matrixx data were almost identical in all cases , and they matched the time between beam - on and beam - off signals of the real - time position management ( rpm ) gating systethe gated step - and - shoot imrt delivery demonstrated an mu delivery accuracy that was equivalent to ungated imrt and the delivered mus with a gating signal agreed with the planned mus within 0.5 mu , regardless of dose rate and duty cycle [ 32 ]  . 
beam flatness exceeded 5 % and monitor linearity deviated more than 3 % for the gated operation with a 2.5 - s breathing cycle and 20 % duty cycle with segment sizes less than 10 mu . 
these authors compared plans delivered with continuously variable dose rate ( cvdr ) to plans delivered with non - cvdr , and showed that treatment times for the former were reduced on average by 28 and 16 % with gated deliveries for gating windows 77 and 66 % , respectively . 
high dosimetric accuracy was demonstrated for as many as 214 beam interruptions during a single 360 - degree arc delivery with gamma index passing rates not lower than 99.0 % for all tests [ 34 ]  . 
the dose measurements results of these authors confirmed that application of gating to rapidarc delivery does not affect the quality of dose delivery : with criteria of delta d = 3 % , dta = 3 mm , the gamma test was passed in a range of 99 to 100 % of the measured points for most of the cases ( with maximum number of interruptions of about 20 per arc ) , and from 97 to 98 % for the extreme case of 15 gy and 8 s gate - open signal ( corresponding to almost 50 interruptions per arc ; [ 35 ] )  . 
investigated the interplay effect for different target residual errors during gated rapidarc delivery using a one - dimensional moving phantom capable of producing stable sinusoidal movement , and evaluated the dosimetric influence using this moving phantothey concluded that the interplay effect has a limited impact on gated rapidarc therapy when evaluated with a linear phanto these results expand on more general work regarding interplay effects in modulated arc therapy [ 36 ]  . 
variations in patient breathing patterns are , however , of much greater clinical significance and caution must be taken when evaluating patients respiratory efforts for gated arc therapy [ 37 ]  . less data are available for accelerated treatments with high dose rates and fast delivery modulated paradigms such as vmat in fff mode . 
while several groups have characterized the general stability of fff photon beams [ 3840 ] , to our knowledge there is just one publication in the literature which reported the dosimetric accuracy of gated treatments with fff beams , though no modulated beams were studied [ 41 ]  . 
specifically , the gated output verification in a phaseor amplitude - gating mode was measured in a solid water phantoa fixed number of mus were delivered to the solid water phantom using both gated and nongated radiation delivery , and the measurements showed less than 0.05 % discrepancy [ 41 ]  . the accuracy of the delivered dose for vmat delivered with and without flattening filter as gated therapy has not yet been reported . 
dosimetric verification of both plan paradigms analyzed in our study ( high - dose / low - modulation / fff and low - dose / high - modulation / normal dose rate ) resulted in excellent mean qa pass rates of > 95 % under all conditions . 
this is within the same range as that normally obtained for ungated vmat with a flattened bea the pattern that emerges from all published data therefore suggests that fff treatments and nonmodulated gated treatments per se are dosimetrically robust on todays delivery equipment , and that gated modulated treatments are robust if gating phases are not too short . 
as a consequence of the long beam - on phases with dibh gating , our data synoptically show that the treatment paradigms analyzed for this manuscript are dosimetrically accurate across a wide range of treatment situations with flattened and fff beams , and , as a consequence of dibh delivery , also robust in terms of actual dose delivery in tissue . 
these approaches have therefore been introduced into clinical routine to optimally reduce the amount of irradiated lung tissue with maximal delivery precision for patients with small and larger lung tumors . compliance with ethical guidelines conflicts of interest a . 
lohr state that there are no conflicts of interest . automatically gated image - guided breath - hold imrt1 3 all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 156 doi 10.1007 / s00066 - 016 - 0942 - 7 erratum to : primary glioblastoma multiforme tumors and recurrence : comparative analysis of the danger signals hmgb1 , hsp70 , and calreticulin carolin muth1 yvonne rubner1 sabine semrau1 paul - friedrich rhle1 benjamin frey1 annedore strnad1 rolf buslei2 rainer fietkau1 udo s . 
gaipl1 erratum to : strahlenther onkol we further thank verena kollera for her excellent technidoi 10.1007 / s00066 - 015 - 0926 - z cal assistance . the present work was performed by the first author muth in fulfillment of the requirements for obtaining the degree med . we apologize for any inconveniences caused . published online : 26 january 2016 springer - verlag berlin heidelberg 2016 unfortunately , the authors acknowledgments were omitted in the final version of the article primary glioblastoma multiforme tumors and recurrence : comparative analysis of the danger signals hmgb1 , hsp70 , and calreticulin the acknowledgments read as follows : we thank francesca pasi from the department of biology and biotechnology lazzaro spallanzani , university of pavia , for her initial help in establishing staining protocols . the online version of the original article can be found at doi : 10.1007 / s00066 - 015 - 0926 - z udo s . 
die hier kommentierte arbeit vergleicht zwei verschiedene behandlungskonzepte von zwei bisher verffentlichten phase - ii - studien . patienten und methoden die daten von 183 patienten [ 123 in der einmalig implantierten gruppe i , ( medianes follow - up 73 monate ) versus 60 patienten in der gruppe ii mit hdr - boost in 2 fraktionen ( medianes follow - up 99 monate ) ] wurden prospektiv bezglich des klinischen und biochemischen outcomes analysiert . 
die implantation wurde originalpublikation helou j , dalimonte l , loblaw a et al ( 2015 ) high dose - rate brachytherapy boost for intermediate risk prostate cancer : long term outcomes of two different treatment schedules and early biochemical predictors success . 
es wurde angestrebt , jeweils v100 > 95% , v150 < 40% und v200 < 14% zu halten sowie an der urethra eine dmax < 118% und an blase und rektum eine dmax < 80% zu erreichen . 
bei allen patienten wurde der initiale psa - wert gemessen und im ersten jahr alle 3 monate , in den darauffolgenden 4 jahren alle 6 monate und danach einmal jhrlich kontrolliert . 
die statistical analysis software 9.3 ermglichte bewhrte statistische methoden wie rocund aucanalysen , kaplan - meier - auswertung und log - rank - test fr das berleben , das cox proportional hazard model , hazard ratio und 95% - konfidenzintervall . ergebnisse der mediane npsa ( nadirpsa ) betrug in der gruppe i mit der einmaligen hdr - fraktion 0 , 08 ng / ml und 0 , 05 ng / ml in der gruppe ii mit zweimaliger hdrbrachytherapie , whrend der psa3y ( psa nach 3 jahren ) 0 , 24 ng / ml in der gruppe i und 0 , 18 ng / ml in der gruppe ii literatur kommentiert1 3 langzeitergebnisse zweier verschiedener behandlungskonzepte mit hdr - brachytherapie - boost mit zweimaligen fraktionen ergab . 
biochemische rezidive wurden bei 12 patienten beobachtet : 8 / 123 patienten in der gruppe i mit einmaliger hdr - brachytherapie und 4 / 60 patienten in der gruppe ii mit 2 fraktionen hdrbrachytherapie . 
das biochemische , rezidivfreie berleben nach 5 jahren zeigte keinen signifikanten unterschied ( p = 0 , 995 ) zwischen den beiden gruppen , auch nicht beim psa - verlauf . 
 niedriges alter sowie ein hoher initialer psa - wert waren in den univariaten analysen signifikante prdiktive faktoren fr einen hheren psa3y ; in den multivariaten analysen blieb jedoch nur das alter signifikant ( p = 0 , 0321 )  . hier vorgestellten arbeit hatten vergleichbare bed - werte ( 90 gy mit eimaligem hdr - boost + hypofraktionierter perkutaner bestrahlung versus 86 , 7 gy mit zweimaligem hdr - boost + konventionell fraktionierter perkutaner bestrahlung )  . 
auch wenn die bed - werte nicht berechnet und die unterschiede der bed nicht diskutiert wurden , liefert die arbeit einen wichtigen beitrag zur diskussion ber die verschiedenen methoden der strahlentherapie beim lokal begrenzten prostatakarzinom . nina seibold und gyrgy kovcs , lbeck schlussfolgerung der autoren die ergebnisse in beiden behandlungsgruppen waren gleich . 
der npsa < 0 , 4 ng / ml ist ein starker prdiktiver faktor fr ein niedriges biochemisches rezidivrisiko ( p = 0 , 0001 )  . literatur kommentar obwohl ein hdr - brachytherapie - boost zur ebrt das outcome bei patienten mit einem lokal begrenzten prostatakarzinom wegen der lokalen dosiseskalation verbessert [ 13 ] , gibt es auch jetzt noch keine zuverlssigen daten bezglich der optimalen dosis und fraktionierung der brachytherapie [ 46 ]  . im vergleich deutsch et al . 
zeigten einen berlebensvorteil zugunsten des hdr - brachytherapie - boosts zur alleinigen sehr hoch dosierten perkutanen bestrahlung mit imrt - technik ( 86 , 4 gy ; [ 7 ] )  . 
es stehen auch keine zuverlssigen biologisch quivalenten berechnungen fr die hdr - brachytherapie zur verfgung , obwohl immer wieder berechnungsmethoden fr die bed bei der seedbrachytherapie empfohlen werden [ 8 ] , die die kontinuierlich hhere dosis im nahbereich der nadeln sowie den steilen dosisabfall der strahler bercksichtigen . des weiteren zeigte sich bei der analyse der literaturdaten , dass die fraktionierung bei der behandlung von prostatakarzinomen nicht das entscheidende ist . 
hoskin pj , colombo a , henry a et al ( 2013 ) gec / estro recommendations on high dose rate afterloading brachytherapy for localized prostate cancer : an update . 
pieters br , van de kamer jb , van herten yrj et al ( 2008 ) comparison of biologicaly equivalent dose - volume parameters for the treatment of prostate cancer with concomitant boost imrt versus imrt combined with brachytherapy . 
hoskin pj , rojas am , bownes pj et al ( 2012 ) randomized trial of external beam radiotherapy alone or combined with high - doserate brachytherapy boost for localized prostate cancer . 
morton g , loblaw a , cheung p et al ( 2011 ) is single fraction 15 gy the preferred high dose - rate brachytherapy boost dose for prostate cancer ? radiother oncol 100 : 463467 6 . 
morton gg , loblaw a , sankreacha r et al ( 2010 ) single - fraction high dose - rate brachytherapy and hypofractionated external beam radiotherapy for men with intermediate - risk prostate cancer : analysis of shortand medium - term toxicity and quality of life . 
deutsch i , zelefsky mj , zhiang z et al ( 2010 ) comparison of psa relapse - free survival in patients treated with ultra - high - dose imrt versus combination of hdr brachytherapy and imrt . 
pritz j , forster km , saini as et al ( 2012 ) providing a fast conversion of total dose to biological effective dose ( bed ) for hybrid seed brachytherapy . 
int j radiat oncol biol phys 43 : 10951101 1 3 hier steht eine anzeige . 1 springer strahlenther onkol ( 2016 ) 192 : 190192 doi 10.1007 / s00066 - 015 - 0936 - x reduziertes rezidivrisiko im bestrahlungsareal durch adjuvante strahlentherapie bei lymphogen metastasierten malignen melanomen mit hohem regionrem rezidivrisiko ralf gutzmer1 hans christiansen2 published online : 21 january 2016 springer - verlag berlin heidelberg 2016 hintergrund das maligne melanom ( mm ) metastasiert hufig initial in die regionren lymphknoten ( lk )  . 
die studie der trans - tasman radiation oncology group ( trog ) untersuchte den stellenwert einer postoperativen adjuvanten radiatio der betreffenden regionren lk - station . patienten und methode in die studie wurden patienten nach kompletter regionrer lk - dissektion aufgrund von melanommetastasen mit hohem rezidivrisiko eingeschlossen . 
darber hinaus wurden rezidive in der in - transit - region und in entfernten regionen , nebenwirkungen der radiotherapie sowie die lebensqualitt erfasst und ausgewertet . ergebnisse prsentiert wurden in der jetzt vorgelegten arbeit die daten der langzeitnachbeobachtung mit einer medianen nachbeobachtung von 73 monaten . 
patienten der beobachtungsgruppe hatten in der regionren lk - station sowohl signifikant mehr erstrezidive als auch rezidive im gesamten beobachtungszeitraum [ erstrezidive : hazard ratio ( hr ) 0 , 52 ; 95% - konfidenzintervall ( ki ) 0 , 390 , 88 ; p = 0 , 023 ; gesamtrezidive : hr 0 , 54 ; 95 % - ki 0 , 330 , 89 ; p = 0 , 021 ]  . 
 die kumulative inzidenz nach 5 jahren fr die regionre lkstation als erstem rezidivort war 18% in der bestrahlungsgruppe und 33% in der beobachtungsgruppe ( p = 0 , 011 )  . 
 betrachtet man nur isolierte rezidive in der regionren lkstation , dann war der unterschied mit 8 , 3% versus 23% noch deutlicher ( p = 0 , 0015 )  . 
in bezug auf nebenwirkungen fanden sich im strahlentherapiearm hufiger ( geringgradig ausgeprgte ) subkutane fibrosen ( hr 2 , 25 ; 95 % - ki 1 , 473 , 46 ; p = 0 , 00022 ) sowie eine strkere umfangsvermehrung der unteren extremitt literatur kommentiert1 3 nach behandlung im leistenbereich ( 15 , 0% im strahlentherapiearm versus 7 , 7% im beobachtungsarm ; p = 0 , 014 )  . 
 die patienten im beobachtungsarm bewerteten die lebensqualitt fr die parameter physisches wohlbefinden zum 3 - monats - zeitpunkt und regionre symptome zu den 3 - , 6und 12 - monats - zeitpunkten signifikant besser . schlussfolgerung der autoren die adjuvante strahlentherapie reduziert nach lymphadenektomie das rezidivrisiko im bestrahlungsareal signifikant , verndert aber nicht das gesamtberleben . 
daher sollte eine adjuvante strahlentherapie bei mm - patienten mit hohem rezidivrisiko in betracht gezogen werden . kommentar es handelt sich hier um eine hochwertige , prospektive , randomisierte phase - iii - studie zum stellenwert der adjuvanten strahlentherapie nach resektion von regionren lk - filiae beim malignen melano dabei geht es um eine relevante fragestellung , da rezidive des mm initial hufig in der regionren lk - station auftreten . 
die 2012 publizierten daten der vorherigen auswertung der trog - 02.01 - studie mit einer nachbeobachtungszeit von 40 monaten [ 1 ] wurde bereits in der s3 - leitlinie des malignen melanoms der deutschen krebsgesellschaft und der awmf bercksichtigt , welche im januar 2013 publiziert wurde [ 2 ]  . 
hier heit es in der schlsselempfehlung 3.4.3a mit einem empfehlungsgrad b und einem evidenzlevel 1b : zur verbesserung der tumorkontrolle im bereich der lymphknotenstation sollte eine postoperative adjuvante radiotherapie bei vorliegen mindestens eines der folgenden kriterien durchgefhrt werden : 3 befallene lymphknoten , kapseldurchbruch , lymphknotenmetastase > 3 cweiterhin heit es in schlsselempfehlung 3.4.3c ( empfehlungsgrad a , evidenzlevel 2b ) : falls die indikation zur bestrahlung des lymphabflussgebietes gestellt wird , soll die strahlentherapie mit 5060 gy in konventioneller fraktionierung ( 5 1 , 82 , 5 gy / woche ) erfolgen . das feld der melanomtherapie unterliegt allerdings momentan einem dramatischen wandel . 
studien zum adjuvanten einsatz von vemurafenib [ 4 ] und dabrafenib plus trametinib [ 5 ] bei patienten mit braf - mutation haben vollstndig rekrutiert und befinden sich in der behandlungsbzw . 
kriterien zum teil erlaubt , allerdings auch nicht obligater bestandteil der therapie . aus radioonkologischer sicht knnen in diesem bereich weitere spannende subgruppenanalysen erwartet werden , welche hoffentlich zustzlich klarheit ber den stellenwert der strahlentherapie unter verfgbarkeit und anwendung moderner systemtherapien bringen . 
erfahrungen aus den bereichen anderer tumorentitten lassen erwarten , dass durchaus damit gerechnet werden kann , dass eine effektivere systemtherapie den vorteil einer adjuvanten strahlentherapie insbesondere auf die lokoregionre tumorkontrolle nicht kompensieren kann . fazit aufgrund der ergebnisse der kommentierten studie sollte patienten / innen mit malignem melanom und einem hohen regionren rezidivrisiko derzeit auf jeden fall eine adjuvante strahlentherapie entsprechend der aktuellen leitlinie der dkg und awmf angeboten werden auerhalb von studien sowieso und auch innerhalb von studien , sofern die studienprotokolle eine strahlentherapie nicht ausdrcklich ausschlieen . es bleibt mit spannung abzuwarten , wie sich das feld der adjuvanten melanomtherapie in den kommenden jahren aufgrund laufender studien mit zielgerichteten und immunologischen therapie entwickeln wird und ob dabei der durch eine lokoregionre strahlentherapie erreichbare gewinn relativiert werden kann . ralf gutzmer und hans christiansen , hannover literatur 1 . 
burmeister bh , henderson ma , ainslie j et al ( 2012 ) adjuvant radiotherapy versus observation alone for patients at risk of lymph - node field relapse after therapeutic lymphadenectomy for melanoma : a randomised trial . 
eggermont am , chiarion - sileni v , grob jj et al ( 2015 ) adjuvant ipilimumab versus placebo after complete resection of high - risk stage iii melanoma ( eortc 18071 ) : a randomised , double - blind , phase 3 trial . 
a study of the braf inhibitor dabrafenib in combination with the mek inhibitor trametinib in the adjuvant treatment of high - risk braf v600 mutation - positive melanoma after surgical resection . 
study of pembrolizumab ( mk - 3475 ) versus placebo after complete resection of high - risk stage iii melanoma ( mk3475 - 054 / keynote - 054 )  . 
efficacy study of nivolumab compared to ipilimumab in prevention of recurrence of melanoma after complete resection of stage iiib / c or stage iv melanoma ( checkmate 238 )  . 
christiansen1 3 strahlenther onkol ( 2016 ) 192 : 193195 doi 10.1007 / s00066 - 015 - 0938 - 8 kardiale toxizitt von trastuzumab in der adjuvanten therapie von mammakarzinompatientinnen ergebnisse der ncctg - n9831 - studie david krug1 published online : 21 january 2016 springer - verlag berlin heidelberg 2016 hintergrund der monoklonale antikrper trastuzumab , der gegen den wachstumsfaktorrezeptor her2 / neu gerichtet ist , wurde 2006 zur adjuvanten therapie des her2 - positiven mammakarzinoms in europa zugelassen . 
die hier kommentierte ncctg - n9831 - studie sollte eine nutzen - risiko - abwgung der kardiotoxischen effekte gegenber den positiven effekten ermglichen . patienten und methoden die phase - iii - studie verglich randomisiert drei verschiedene schemata in der adjuvanten systemtherapie des her2 positiven mammakarzinoms . 
anschlieend bekamen sie entweder 12 zyklen paclitaxel ( arm a ) oder sequentiell paclitaxel und trastuzumab ( arm b ) oder simultan paclitaxel und trastuzumab , gefolgt von einer monotherapie mit trastuzumab ( arm c )  . 
die wchentliche originalpublikation advani pp , ballman kv , dockter tj et al ( 2015 ) long - term cardiac safety analysis of ncctg n9831 ( alliance ) adjuvant trastuzumab trial . 
an 1944 patientinnen wurden jhrlich die kardialen ereignisse , definiert als herzinsuffizienz nyha grad iii / iv oder belegte kardiale todesflle nach myokardinfarkt , herzinsuffizienz oder arrhythmie und ungeklrte todesflle mit mglichem kardialem hintergrund analysiert . 
nach 6 jahren erfolgte eine abschlieende echokardiographie . ergebnisse die kumulative inzidenz kardialer ereignisse nach 6 jahren betrug 0 , 6% in arm a , 2 , 8% in arm b und 3 , 4% in arm c . 
die nutzen - risiko - abwgung fllt weiterhin gnstig aus . literatur kommentiert 194 kommentar die hier vorgestellten daten zur kardiotoxizitt von trastuzumab aus der n9831 - studie decken sich prinzipiell mit den berichten aus anderen prospektiven studien und einer groen metaanalyse von 2011 [ 1 ]  . 
denn als ausschlusskriterien fr die studie werden nmlich aktive kardiale begleiterkrankungen sowie eine anamnese mit herzinsuffizienz , arrhythmie , erkrankungen der herzklappen , myokardinfarkt , unkontrollierte arterielle hypertonie , perikarderguss und andere nicht nher definierte kardiovaskulre erkrankungen genannt . 
tatschlich legen einige registerstudien nahe , dass im klinischen alltag die inzidenz kardialer ereignisse unter trastuzumab - therapie hher sein knnte , insbesondere bei lteren frauen und bei kardialen vorerkrankungen [ 2 , 3 ]  . zudem stellt die verwendete definition fr kardiale ereignisse wohl sinnbildlich nur die spitze des eisbergs dar . 
in der initialpublikation der n9831 - studie , die 2005 gemeinsam mit der nsabp - b - 31 - studie im new england journal of medicine erfolgte [ 4 ] , ist vermerkt , dass 31 , 4% der frauen in beiden studien die trastuzumab - therapie vorzeitig abbrachen . 
auch wenn sich die lvef bei den patientinnen mit kardialen ereignissen in der mehrzahl der flle wieder erholt hatte , so ist aus der nsabp - b - 31 - studie bekannt , dass in ber der hlfte der flle auch dann noch eine behandlung der herzinsuffizienz erfolgte . 
auch bei patientinnen mit asymptomatischem lvef - abfall war dies in einem viertel der flle ntig ; zudem verblieb die lvef bei 20% dieser patientinnen unter 50% [ 6 ]  . 
eine langfristige subklinische kardiale schdigung , die sich erst spter manifestieren knnte , konnte also insbesondere vor dem hintergrund des vergleichsweise niedrigen durchschnittsalters der patientinnen nicht ausgeschlossen werden [ 7 ]  . ein zusammenhang zwischen den kardialen ereignissen und einer radiotherapie lie sich nicht feststellen . 
bearbeiteten diese fragestellung prospektiv an 106 patientinnen , von denen nach einer mittleren nachbeobachtungszeit von 28 monaten 6 eine reversible linksventrikulre systolische dysfunktion vom grad iiiii entwickelten , darunter eine im rahmen eines myokardinfarkts [ 9 ]  . fazit hhergradige kardiale toxizitten , insbesondere kardiale todesflle , sind nach adjuvantem trastuzumab selten und ihre hufigkeit scheint nach etwa 2 jahren ein plateau zu erreichen . 
eine radiotherapie der mammaria - interna - lymphabflusswege sollte unter laufender trastuzumab - gabe nur nach kritischer berprfung der indikation und unter bestmglicher herzschonung erfolgen . david krug , heidelberg literatur 1 . 
bowles eja , wellman r , feigelson hs et al ( 2012 ) risk of heart failure in breast cancer patients after anthracycline and trastuzumab treatment : a retrospective cohort study . 
halyard my , pisansky tm , dueck ac et al ( 2009 ) radiotherapy and adjuvant trastuzumab in operable breast cancer : tolerability and adverse event data from the ncctg phase iii trial n9831 . 
caussa l , kirova ym , gault n et al ( 2011 ) the acute skin and heart toxicity of a concurrent association of trastuzumab and locoregional breast radiotherapy including internal mammary chain : a single - institution study . 
nach einer ersten randomisierung erhielten 223 patienten 1000 mg / m krperoberche gemzitabin wchentlich und 219 patienten zustzlich 100 mg / tag erlotinib fr 4 monate als induktionstherapie . nach einer zweiten randomisierung wurden die patienten ohne tumorprogress fr weitere 2 monate entweder mit derselben chemotherapie weiterbehandelt ( 136 patienten ) oder einer rct mit capecitabin bis 54 gy unterzogen . primrer endpunkt war die gesamtberlebenszeit , ausgehend vom datum der ersten randomisierung . 
sekundre endpunkte waren der einuss der qualittssicherung der originalpublikation hammel p , huguet f , van laethem jl et al ( 2016 ) effect of chemoradiotherapy vs chemotherapy on survival in patients with locally advanced pancreatic cancer controlled after 4 months of gemcitabine with or without erlotinib : the lap07 randomized clinical trial . 
eine interimsanalyse nach dem tod von 221 patienten ( 109 in der rct - gruppe und 112 in der chemotherapiegruppe ) erzwang den frhen studienabbruch , weil die h1 - hypothese einer verlngerung des gesamtberlebens durch die radiochemotherapie nicht mehr erreichbar war . 
nach einer medianen nachbeobachtungszeit von 36 , 7 monaten war die mediane gesamtberlebenszeit , vom ersten tag der randomisierung angerechnet , nicht signikant unterschiedlich zwischen nur chemotherapie und rct mit 16 , 5 monaten ( 95% - ki 14 , 518 , 5 m ) bzw . 
15 , 2 monaten ( 95%ki 13 , 917 , 3 m ; hr 1 , 03 ; 95% - ki 0 , 791 , 34 ; p = 0 , 83 )  . die mediane gesamtberlebenszeit von protokollgerecht bestrahlten patienten bzw . 
geringfgigen protokollversten lag bei 17 , 0 monaten gegenber 13 , 4 monaten nach schwerwiegenden protokollversten ( hr 1 , 34 ; 0 , 862 , 36 ; p = 0 , 17 )  . 
nach 4 monaten induktionschemotherapie gibt es keinen signikanten unterschied im gesamtberleben nach rct im vergleich zur chemotherapie alleauch verbesserte erlotinib im vergleich mit gemzitabin allein das gesamtberleben nicht . kommentar das interesse an der wirkung einer lokalen therapie beim rasch systemisch metastasierenden pankreaskarzinom wurde vor einiger zeit geweckt , als aus einer autopsieserie berichtet wurde , dass knapp 40 % aller patienten mit pankreaskarzinom an den lokalen folgen des tumors und nicht an einer fernmetastasierung versterben [ 1 ]  . 
daher wurde die volltextpublikation der lap07 - studie lange erwartet , um die ergebnisse dieser modernen vergleichsstudie zwischen chemotherapie und radiochemotherapie ( rct ) bei lokal fortgeschrittenen pankreaskarzinomen ( lapc ) in ihrer gesamtheit bewerten zu knnen [ 2 ]  . 
in der studie gab es zwei randomisierungsschritte , zunchst bei der induktionschemotherapie zwischen gemzitabin allein und der kombination aus gemzitabin und erlotinib , und spter anschlieend zwischen der fortfhrung der chemotherapie und einem wechsel zur rct mit capecitabuns erscheint es wichtig , dass der stellenwert des egfr - inhibitors erlotinib erneut geprft wurde , und zwar prospektiv randomisiert in einer phase - iii - studie . 
in der erhaltungstherapie mit erlotinib , also bei patienten , die das medikament mehr als 4 monate lang erhalten hatten , verschlechterte sich das berleben sogar , und zwar statistisch signikant . 
krzlich war nmlich behauptet worden , dass patienten mit egfr - mutationen bei der kombination von gemzitabin und erlotinib einen vorteil im progressionsfreien berleben ( pfs ) haben knnten [ 3 ]  . mit mehr spannung wurde allerdings die antwort auf die frage erwartet , ob nach einer induktionschemotherapie eine anschlieende rct das berleben von patienten mit lapc verlngern kann . 
erfreulicherweise betrug in der lap07 - studie die gesamtberlebenszeit nach rct wiederum 15 , 2 monate und lag gesamthaft mit 16 , 5 monaten klar oberhalb des seinerzeitigen historischen vergleichs beider therapiearme , ohne dass hierfr ein spezischer grund erkennbar wre . 
bei der studienplanung war man davon ausgegangen , dass die mediane gesamtberlebenszeit nach chemotherapie bei 9 und nach radiochemotherapie bei 12 monaten liegen msste , um statistische signikanz zu erreichen . es ist wichtig zu betonen , dass in der lap07 - studie die qualitt der radiotherapie gegenber vorausgegangenen studien deutlich verbessert war und darber hinaus auch eine spezische qualittsanalyse der radiotherapie durchgefhrt wurde . 
es darf davon ausgegangen werden , dass zum einen der verzicht auf die bestrahlung elektiver lymphabussgebiete , aber auch die kombination mit capecitabin dazu beigetragen haben , dass die rct nicht schlechter als die fortgefhrte chemotherapie vertragen wurde . auf den ersten blick mag man meinen , dass die berechnung des berlebens vom zeitpunkt der ersten randomisierung die unterschiede zwischen dem rct - arm und dem chemotherapie - arm verschleiert haben knnte , da die unterschiedlichen therapiemodalitten erst 5 monate nach beginn der induktionschemotherapie begannen . 
ebenso war die lnge der therapiepause nach abgeschlossener rct mit 6 , 1 monaten deutlich lnger als nach chemotherapie mit 3 , 7 monaten ( p = 0 , 02 )  . 
da die lebensqualitt der patienten whrend des studienablaufs leider nicht mitgeteilt wurde , knnen wir die bedeutung dieses effekts nicht erklren . die praxisrelevanz der studie heute wird sicher dadurch eingeschrnkt , dass gemzitabin mittlerweile nicht mehr der aktuelle behandlungsstandard beim lapc ist , sondern von den kombinationen gemzitabin / nab - paclitaxel und folfirinox weitgehend abgelst wurde . 
darauf lsst die uerst niedrige resektionsrate von nur 4 % insofern schlieen , dass die meisten eingeschlossenen patienten 958 strahlenther onkol ( 2016 ) 192 : 956958 irresektable tumoren hatten . 
die frage der bedeutung einer rct bei brpc und mit folfirinox wird in deutschland zurzeit mit der randomisierten phase - iii - conko - 007 - studie untersucht ( eudract 2009 - 014476 - 21 )  . wrde man die lap07 - studie heute erneut planen , wrde man fordern , vor der zweiten randomisierung in den rct - arm eine fdg - pet / ct durchzufhren . 
man knnte damit erstens patienten mit fernmetastasen ausschlieen , zweitens die zielvolumina des primrtumors besser denieren und drittens positive lymphknoten leichter aufnden . fr alle drei genannten punkte sind sensibilitt und spezitt der fdg - pet / ct der ct berlegen . 
auch wrde man die denition des bestrahlungsvolumens nicht in direkter expansion des makroskopischen volumens zum planungszielvolumen durchfhren , sondern die atembeweglichkeit ber eine 4 - d - bildgebung in die planung mit einbeziehen . 
all diese faktoren und der umstand , dass nur ein drittel der patienten eine radiotherapie in der vom protokoll geforderten qualitt erhalten hat , knnten grnde dafr sein , dass feldrandrezidive durch inadquate erfassung des zielvolumens u . 
man wrde sich auch darum bemhen , nach abschluss der induktionschemotherapie nicht 46 wochen therapiepause bis zum beginn der rct vorzugeben , sondern nur maximal 23 wochen . in der zukunft wird darber hinaus geklrt werden mssen , ob nicht eine stereotaktische radiotherapie ( sbrt ) , welche die systemtherapie nur kurz unterbricht , geeigneter als die konventionelle rct ist , in der phase der bestrahlung auf verstreute zellen einen hohen therapiedruck auszuben [ 5 ]  . 
sie wre wegen der erreichbaren hheren effektiven bestrahlungsdosis dem bestrahlungskonzept der lap07 - studie onkologisch berlegen . fazit ohne zweifel sehen wir in der lap07 - studie die derzeit beste und aussagekrftigste studie zum vergleich zwischen rct und chemotherapie . 
der schluss jedoch , dass aufgrund der daten der lap07 - studie die rct bei patienten mit einem lapc keine bedeutung mehr habe , ist voreilig , schlecht begrndet und anfechtbar . thomas brunner , freiburg , und emmanouil fokas , frankfurt / main interessenkonikt t . 
iacobuzio - donahue ca , fu b , yachida s , luo m , abe h , henderson cm et al ( 2009 ) dpc4 gene status of the primary carcinoma correlates with patterns of failure in patients with pancreatic cancer . j clin oncol 27 ( 11 ) : 18061813 . 
hammel p , huguet f , van laethem jl , goldstein d , glimelius b , artru p et al ( 2016 ) effect of chemoradiotherapy vs chemotherapy on survival in patients with locally advanced pancreatic cancer controlled after 4 months of gemcitabine with or without erlotinib : the lap07 randomized clinical trial . 
wang jp , wu cy , yeh yc , shyr ym , wu yy , kuo cy et al ( 2015 ) erlotinib is effective in pancreatic cancer with epidermal growth factor receptor mutations : a randomized , open - label , prospective trial . 
huguet f , andre t , hammel p , artru p , balosso j , selle f et al ( 2007 ) impact of chemoradiotherapy after disease control with chemotherapy in locally advanced pancreatic adenocarcinoma in gercor phase ii and iii studies . 
mahadevan a , miksad r , goldstein m , sullivan r , bullock a , buchbinder e et al ( 2011 ) induction gemcitabine and stereotactic body radiotherapy for locally advanced nonmetastatic pancreas cancer . 
the incidence of brain metastases , brain metastases - free survival ( bmfs ) , and adverse effects were also evaluated . results survival data of the 204 patients were analyzed statistically . 
45 patienten ( 22 , 1 % ) wurden anschlieend mit pci behandelt , die brigen ( 77 , 9 % ) erhielten keine behandlung ( kontroll906 strahlenther onkol ( 2016 ) 192 : 905912 gruppe )  . 
der primre endpunkt der studie war das os . ebenfalls beurteilt wurden das auftreten von hirnmetastasen , das hirnmetastasenfreie berleben ( bmfs ) und nebenwirkungen . ergebnisse die daten zum berleben der 204 patienten wurden statistisch ausgewertet . 
in 2011 , these results were considered category - 1 evidence by the national comprehensive cancer network ( nccn ) clinical practice guideline , recommending pci for esclc patients showing a response to initial chemotherapy . 
however , the eorct trial was questioned for not performing brain imaging on patients without symptoms of brain metastases before randomization [ 20 ] ; hence , some asymptomatic patients who should have received irradiation with 3034 gy in 1517 fractions were underdosed . 
the dose fractionation of the eorct study was also challenged ( mostly 20 gy in 5 fractions ) , which was not a common prescription for pci in north america . in contrast , the latest preliminary data of a phase iii randomized trial from japan [ 21 ] indicated that pci had a detrimental effect on os in esclc patients . 
therefore , the revised nccn guideline degraded the evidence level from 1 to 2a in 2016 , awaiting more upcoming data to strengthen or deny such a recommendation . by including the patients without the aforementioned this retrospective study aims to investigate limitations , whether pci could improve os in esclc patients . patients and methods schlsselwrter strahlentherapie chemotherapie zerebrale bildgebung metastasen dosisfraktionierung patients a study on esclc patients was initiated with valid approval from the hospital ethics committee . 
a total of 204 patients were reviewed , all of whom were pathologically diagnosed with esclc and had a complete ( cr ) or partial response ( pr ) to initial chemotherapy between april 2005 and may 2014 . 
the remaining 17 patients were conrmed with cranial ct instead , due to mri contraindications such as articial implants , cardiac pacemakers , dental prostheses , contraceptive ring , etc . 
most of these patients die from such brain metastases [ 13 ]  . previous studies [ 1417 ] and meta - analyses [ 18 , 19 ] irradiation have demonstrated that prophylactic cranial ( pci ) can reduce the incidence of brain metastases and improve overall survival ( os ) in patients with limited small cell lung cancer ( lsclc )  . 
in 2007 , a randomized trial [ 20 ] from the european organization for research and treatment of cancer ( eortc ) reported that pci could lower the risk of brain metastases and improve os of esclc patients with a response to initial strahlenther onkol ( 2016 ) 192 : 905912 performance status , diagnosis , and staging denition of endpoints as mentioned above , performance status was assessed according to the ecog - ps scale . 
esclc referred to the lesion beyond the ipsilateral hemithorax , including contralateral supraclavicular nodes , malignant pericardial or pleural effusion , and distant hematogenous metastases , and also included patients with extensive local disease that was not covered by a reasonable radiation portal . 
stage determination was also assisted by other available initial examinations including ct , mri , abdominal ultrasonography , bone scan , and positron - emission tomography ( pet ) / ct . the primary endpoint of this study was os , dened as the interval from the date of diagnosis to the date of death or patient censored at the last follow - up . 
bmfs was dened as the interval from the date of diagnosis to the date of development of brain metastases or death or patient censored at the last follow - up . 
to evaluate late adverse effects , the internationally accepted lent - soma scoring system ( late effects normal tissue task force - subjective , objective , management , analytic ) was used . treatment and treatment response statistical analysis all involved patients had received four to six cycles of initial chemotherapy and showed positive responses , including cr and pr . 
any pathological lymph nodes ( whether target or non - target ) must show a reduction in the short axis to < 10 mpr : at least a 30 - % decrease in the sum of diameters of target lesions , taking as reference the baseline summed diameters . pci was delivered using a three - dimensional conformal radiation therapy ( 3dcrt ) technique comprising two opposing lateral elds . 
all the 204 patients involved were eligible and may potentially benet from pci according to nccn criteria ( attaining cr or pr ; good ps of 02 ; acute toxicities of initial therapy have resolved ; no impaired neurocognitive function )  . 
univariate and multivariate analyses of os and bmfs were performed with the cox proportional hazard regression model ; univariate and multivariate analyses of the incidence of brain metastases were performed by logistic regression analysis . 
1 overall survival in correlated to prophylactic cranial irradiation ( pci ) ing pci developed brain metastases , 22.2 % of whom were treated with whole - brain radiation therapy ( wbrt ) after brain metastases . 
of the 159 cases in the control group , 91 patients developed brain metastases , 43.2 % of whom were treated with wbrt . during the follow - up period , 29 out of 45 patients in the pci group died , as did 83 out of 159 patients in the control group . 
1 , patients receiving pci had overall survival strahlenther onkol ( 2016 ) 192 : 905912 skin reactions , which were graded according to the ctcae version 4.0 scoring scale ( table 3 )  . 
late adverse effects mainly included headache and somnolence , both of which were below grade 2 according to the lent - soma scale for brain ( table 4 )  . discussion up until now , no consensus has been reached regarding the impact of pci on os in esclc , due to inconsistent results from previous randomized trials [ 20 , 21 ]  . 
patients in both the current study and the eorct trial [ 20 ] received four to six cycles of initial chemotherapy and had a response to the treatment . although a benecial impact on os was observed in both the eortc and the present study , the current work has overcome several deciencies of the eortc trial . 
secondly , the pci fractionalization for the majority of patients in the present study ( 93.3 % ) was closer to the clinical routine of north america ( 25 gy / 10 fractions ) than in the eorct trial ( mostly 20 gy / 5 fractions )  . 
the solid line suggests that the cumulative incidence of brain metastases for the patients receiving prophylactic cranial irradiation ( pci ) increases with time . the dotted line shows that the cumulative incidence of brain metastases for patients not receiving pci also increases with time . 
 [ 21 ] have questioned the wide variations of total dose from 20 to 39 gy in the eorct study , whereas this range was much smaller in the current study ( 22.5 to 30 gy )  . 
 [ 21 ] pointed out that the initial chemotherapy did not include platinum in the eorct trial , whereas a platinum - based chemotherapy regimen was administered in 97.8 % of patients in the pci group and 95.6 % of patients in the control group of the current study . based on comparable patient baseline conditions but avoiding some limitations , this retrospective study echoed the eortc trial ndings that pci could signicantly improve os in esclc patients . the inconsistent conclusions of the three studies may suggest that not all patients with a response to chemotherapy would benet from pci in terms of os . 
 [ 21 ] reported that pci signicantly reduced the incidence of brain metastases compared to the control group ( p < 0.001 ) in esclc , where the 1 - year incidence of brain metastases was 32.4 % in the pci group vs . 
further multivariate analysis indicated that pci was a positive prognostic factor for bmfs . the primary acute and late adverse effects observed in this work are in line with previous studies [ 20 ] and generally well tolerated . in addition to pci , a study [ 26 , 27 ] on prophylactic thoracic irradiation ( pti ) was presented at the 2014 asco annual meeting , reporting that pti improved progressionfree and 2 - year survival , although pti did not inuence the risk of death in the rst year ; therefore recommending pti for all esclc patients with a response to chemotherapy . considering the limited existing data , more studies on pti might be needed in the future . as to limitations , this retrospective single - center study involved a limited sample size . 
these studies shall include and analyze more patient risk factors to establish appropriate indications for pci aimed at a maximum patient benet . 912 conclusion this study indicated that pci , for patients with any response to the initial chemotherapy , signicantly improved os , reduced the incidence of brain metastases , and delayed development of brain metastases in esclc patients . should be noted that these results are only representative of the analyzed patient population , as this was a single - center retrospective analysis . acknowledgements this work was jointly supported by the national natural science foundation of china ( 11505012 ) and the beijing municipal administration of hospitals youth programme ( qml20151004 )  . compliance with ethical guidelines conict of interest y . 
jiao declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
brunner1 , 2 ursula nestle1 , 2 sonja adebahr1 , 2 eleni gkika1 , 2 rolf wiehle1 , 2 dimos baltas1 , 2 anca - ligia grosu1 , 2 received : 10 may 2016 / accepted : 21 september 2016 / published online : 18 october 2016 the author ( s ) 2016 . 
a novel intensity - modulated radiotherapy ( imrt ) prescription concept termed simultaneous integrated protection ( sip ) for quantiable and comparable dose prescription to targets very close to oar is described . materials and methods an intersection volume of a planning risk volume ( prv ) with the total planning target volume ( ptv ) dened the protection volume ( ptvsip )  . the remainder of the ptv represented the dominant ptv ( ptvdom )  . 
dose to ptvsip was required to be as high as possible within the constraints to avoid local relapse . results sip was applied in 6 patients with oar being large airways ( n = 2 ) or bowel ( n = 4 ) in 3 , 5 , 8 , and thomas b . 
brunner and ursula nestle contributed equally to the manuscript . electronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 016 - 1057 - x ) contains supplementary material , which is available to authorized users . ( cid : 2 ) thomas b . 
all patients had local control at a median 9 month follow - up and toxicity was low . conclusion sip results in a median dose of 100 % to ptv , to achieve high local control and low toxicity . 
longer follow - up is required to verify results and a prospective clinical trial is currently testing this new approach in chest and abdomen stereotactic body radiotherapy . keywords stereotactic body radiation therapy intensitymodulated radiotherapy efcacy toxicity organs at risk simultan integrierte protektion ein neues konzept fr die hochprzisionsbestrahlung zusammenfassung zielsetzung die stereotaktische radiotherapie nahe serieller risikoorgane ( oar ) erfordert besondere vorsicht . 
wir beschreiben ein neues konzept fr die intensittsmodulierte strahlentherapie ( imrt ) , genannt simultan integrierte protektion ( sip ) , das die dosisverschreibung auf zielvolumina in unmittelbarer nhe von oar quantiziert . material und methoden das berschneidungsvolumen eines planungsrisikovolumens ( prv ) mit dem gesamten planungszielvolumen ( ptv ) denierte das protektionsvolumen ( ptvsip )  . 
die ptvsip - dosis sollte so hoch wie mglich sein , aber innerhalb der constraints , um lokalrezidive zu vermeiden . ergebnisse die sip - technik wurde bei 6 patienten mit den oars groe atemwege ( n = 2 ) und darm ( n = 4 ) in 3 , 5 , 8 und 12 fraktionen bei jeweils 1 , 3 , 1 und 1 patienten angewendet . 
die vertrglichkeit der plne wurde durch die analyse der absoluten dosisvolumenhistogramme ( dosis auf ml ) berprdie steilheit des dosisabfalls wurde durch den vergleich der dosis - constraints mit der dosis auf die prvs gegenber der dosis auf die oars abgelesen ( wilcoxon - test p = 0 , 001 )  . 
alle patienten zeigten eine lokalkontrolle bei einem medianen 9 - monatigen nachbeobachtungszeitraum und niedrige toxizitt . schlussfolgerung sip ermglichte eine mediane dosis von 100 % auf das ptv und ergab eine hervorragende lokalkontrolle bei niedriger toxizitt . 
eine prospektive klinische studie testet derzeit diesen neuen ansatz fr die thorakale und abdominelle krperstereotaxie . schlsselwrter stereotaktische krperbestrahlung intensittsmodulierte strahlentherapie efzienz toxizitt risikoorgane introduction over the past two decades stereotactic radiotherapy ( srt ) has evolved to a powerful tool to control lesions especially in the brain , lungs , and liver [ 11 , 12 , 19 , 21 , 23 ]  . 
however , reports of high - grade toxicities after stereotactic body radiotherapy ( sbrt ) of central lung tumors and of lesions near the bowel or stomach on the other hand demonstrated the difculties to safely administer sbrt in these situations despite multimodal imaging , accurate motion management , intensity - modulated radiotherapy ( imrt ) , and image - guided radiotherapy ( igrt ) [ 9 , 22 , 26 ]  . the concept of srt relies on avoiding organs at risk ( oars ) through high spatial precision . 
inherently , limitations of srt and sbrt were encountered when the target lesions were too close to oars and this is the clinical problem stipulating the development of the currently described novel concept of simultaneous integrated protection ( sip )  . for example , perforation of central airways , bronchial hemorrhage , perforations of the esophagus , stomach , or small bowel were observed [ 7 , 14 , 26 ]  . 
another strategy is to increase the number of fractions to exploit the differential radiosensitivity of tumor and oars as dened by their / ratios [ 1 , 3 ]  . 
while this will help to overcome some of the limitations in more critical locations , there are still a signicant number of cases where neither reduction of the total dose nor increasing the number of fractions within the limits of signicant hypofractionation enables the application of an adequate radiation dose . 
the tradition of prescribing sbrt not according to icru but to individually chosen isodoses ( typically 6080 % ) aggravates the problem due to steep dose gradients which make even small setup errors highly risky . 
in summary , there is no standard approach to overcome such obstacles of the safe application of sbrt at this time . when change of dose or fractionation is not sufcient , this problem is often addressed by individual dose reductions at the interface of target lesions with a critical organ at risk ( oar ) at the discretion of the treating physician . however , in addition to the lack of data in the literature , such compromises derived from the fear of normal tissue complications may lead to the application of insufcient tumor doses and impair local control [ 20 ]  . 
furthermore , the lack of interobserver and interinstitutional comparability is a cardinal factor of inconsistencies , and it is a problem for prospective trials . our aim was therefore to develop a prescription method maximizing consistency of sbrt hypofractionation plans for targets near oars [ 5 ] which deliberately and in a calculated way lowers the dose to a part of the ptv that is close to critical oars . 
it is based on the denition of a subvolume being the intersection of the ptv and the prv of a critical oar to which the highest possible dose respecting the dose constraints for this oar is planned and delivered . materials and methods the stepwise procedure to dene the sip approach is summarized in table 1 , while a owchart is shown in supplemental fig . 
the sip concept was required for sbrt 888 strahlenther onkol ( 2016 ) 192 : 886894 table 1 standardized denition of the simultaneous integrated protection ( sip ) concept in the treatment planning algorithm 1 . 
indication : the use of the technique is indicated when first , the standard indications for stereotactic radiotherapy are given ( not further specied in the framework of this manuscript ) and 2 . 
prescription : second , there is overlap of the planning target volume ( ptv ) with a critical organ at risk ( oar ) or with the planning risk volume ( prv ) of this oar for the tumor : standard volumes gtv , ctv , itv , and ptv are used ( icru 50 , 62 ) for the oar : gross risk volume ( oar ) , planning risk volume ( prv ) is used ; for oars with signicant motion an internal risk volume ( irv ) may be used to dene the prv nomenclature of volumes ( expressed in set theory notation ) : total ptv : ptv simultaneous protection volume : ptvsip = ptv \ prv dominant ptv : ptvdom = ptv \ ptvsip by denition the sip concept is an application of imrt dose is prescribed according to icru ( report 83 ) to ptvdom reporting dmedian , d98 , and d02 dmedian in ptvdom should have a table mount - like dose prole as typical for stereotactic radiotherapy within ptvdom a classical simultaneous integrated boost volume ( sib ) may be planned after denition of a respective sib volume for ptvsip , the transition volume from ptvdom to oar , the planning instructions are twofold : ( 1 ) stay within the boundaries of the given dose constraints for the oar ( 2 ) within ( 1 ) , make use of the maximum possible dose to the oar to minimise dose inhomogeneity for ptv report dmedian , d98 , and d02 4 . 
igrt : cutting edge patient positioning and igrt is mandatory for the use of the sip concept treatment planning in case where there was an unacceptable high dose to an oar , i . 
e. , if there was overlap of the ptv with either the oar or its expansions ( irv , prv )  . this represented the key inclusion criterion for this report . patients with an indication for sbrt where the sip concept did not achieve adequate protection of the oar at the highest planned fraction number , i . 
the term dominant was chosen to imply that the sip approach is only valid for small volumes of ptvsip . third , we dened the prescription of dose to the above volumes . 
the concept inherently requires an imrt apstrahlenther onkol ( 2016 ) 192 : 886894 the dose constraints were violated at a chosen number of fractions , planning iterations with a higher number of fractions up to a specied maximum of 12 fractions were performed . 
prescribed doses and dose constraints were recalculated to the eqd2 using the respective / ratios of tumor and oar , and aiming to deliver iso - effective doses to the tumor with lower toxicity by protracted dose delivery . 
if the normal tissue constraints could not be fullled by increasing the number of fractions to the maximum number , sbrt was not given but conventionally fractionated treatment performed instead . 
seventh , we required high - precision patient positioning , motion management , and igrt for the use of the sip concept . for the analysis descriptive statistics were used and the wilcoxon test for paired differences was used for the comparison of dose to the prvs with dose to the respective oars to evaluate the plans for given dose constraints . 
safety of the plans was analyzed from the absolute volume dvhs as summarized in supplemental table 1 showing the comparison of the dose constraints with the doses in the plans to the oars of the oars and to the prvs . 
scheme of a critical organ at risk ( oar ; blue , left side ) with its planning risk volume ( prv ) overlapping with the planning target volume ( ptv , pink )  . 
the dominant ptv ( ptvdom = ptv\prv ; orange ) is the prescribed dose in the conventional way , whereas the ptvsip ( = ptv \ prv ; purple ) is prescribed a lower dose to stay within the dose constraints for the oar proach for simultaneous administration of different doses to ptvdom and to ptvsip . 
dose was prescribed according to icru report 83 to ptvdom indicating dmedian , d98 , and d02 . as typical for sbrt , we were asking for a table mountlike dose prole in ptvdom and a d02 being up to 120 % of the prescribed dose [ 25 ]  . 
e. , the volume that contains the dose gradient from ptvdom to the oar ( s ) , the planning instructions were twofold : to stay within the boundaries of the given dose constraints for the oar itself , and to make use of the maximum possible dose to ptvsip to minimize dose inhomogeneity for ptv . in order to ensure this , the dose gradient between the dose to the oar and the dose prescribed to the ptvdom typically localizes to the prv volume around the oar . 
we also reported dmedian , d98 , and d02 for ptvsip to quantify the dose sacrice that was made for the ptv of a distinct lesion . fourth , we carefully chose available dose constraints for the oars following the recommendations published by quantec and other published recommendations commonly used for sbrt [ 1 , 5 , 12 , 16 , 27 , 28 ]  . 
to quantify this , a comparison of the given dose constraints with the actual doses to the oar volumes and the prv volumes was performed by analyzing the difference of the ratio d ( oar ) / d ( constraint ) with d ( prv ) / d ( constraint ) for the 19 dose constraint values shown in supplemental table 1 ( p = 0.001 , wilcoxon test )  . 
none of these patients showed severe toxicity within a median follow - up of 8.6 months ( range 3.126.2 months ) with favorable local control ( 100 % )  . strahlenther onkol ( 2016 ) 192 : 886894 fig . 
for each patient from left to right the relative prescription doses to the dominant non - protection ptv , ptv , and ptvsip are shown with minimal ( min ) , maximal ( max ) , and mean ( lled diamonds ) relative doses . 
comparing dmean , ptv with dmean , ptvdom , the difference was just about signicant at p = 0.043 whereas the difference was more signicant between dmean , ptv with dmean , ptvsip at p = 0.028 ( wilcoxon test )  . 
mean and median relative doses to 95 % ( d95 vol.% ) of the volumes ptvdom , ptv , and ptvsip were 122 , 105 , and 90 % , as well as 120 , 107 , and 93 % , respectively . this reects that the dose sacrice to ptvsip was kept to a minimumaximum bed ( / 10 ) doses in the ptv for the 6 patients were 124 , 135 , 93 , 92 , 114 , and 154 gy , respectively . 
4 and supplemental table 2 show further examples of applications of the sip concept for conventionally fractionated imrt for cerebral and extracerebral target volumes . 892 strahlenther onkol ( 2016 ) 192 : 886894 fig . 
tumor shrinkage after two courses of induction chemotherapy with paclitaxel / cisplatin , then chemoradiotherapy with sip - imrt to 54 gy during phase 1 followed by an adaptive sequential boost ( not shown ) during phase 2 . 
h delineation of the right ( sky blue ) and left ( blue - green ) hippocampus with the respective prvs ( yellow ) that are generated by a 7 mm isotropic margin to the hippocampi . 
i a total dose of 35 gy in 14 fractions was prescribed to the ptvdonote the 28.0 gy ( green ) and the 17.5 gy ( cornower blue ) isodoses at the two sip volumes . 
prv planning risk volume , ptv planning target volume discussion the described technique of the sip concept proposes a fully quantied method to protect oars and to avoid toxicity in a deliberate and reproducible way , while keeping the dose to the remaining ptv at effective levels . 
the main advantage of this approach is the high level of transparency which makes it a suitable tool for multicenter trials in sbrt minimizing interinstitutional technical differences as a source of error . 
in contrast to the sib method where a small subvolume inside a ptv is prescribed to receive an escalated dose to enhance local control , the sip concept prescribes a lower dose to a subvolume of a ptv with a high risk of severe toxicity . the sip concept is proposed for serial oars according to the model of functional subunits ( fsu ) [ 29 ]  . 
g. , spinal cord , esophagus , and bowel , the defect of a few fsus has a high likelihood for toxicity compared to parallel oars such as the lung or the liver . using the sip concept , the protection of an oar is achieved by a protective outer shell around an oar as a volume for the steep dose gradient between the tumor strahlenther onkol ( 2016 ) 192 : 886894 and the oar . 
summarizing , igrt is key to verify whether employed margins of oars are correct and clinical trials will have to verify whether the concept is useful and whether the dose constraints were correct . 
adaptive radiotherapy strategies can also be combined with the sip concept and we are currently analyzing this approach in prostate cancer imrt for the rectuhowever , we felt that this would be too complex in the framework of this article and therefore we plan to describe this in a subsequent publication . excessive contact volumes between the tumor and the oar are not thought to be a good indication for sip . 
at this time it is not fully clear yet which dose parameters are most important for local tumor control , ptv encompassing dose , or maximum dose [ 15 ]  . in a recent analysis of more than 1500 sbrt treatments of primary and secondary tumors of the lung with a broad range of primaries , a plateau of the doseresponse curve with 90 % local tumor control probability was reached at 160 gy bed when using the ptv maximum dose [ 13 ]  . 
their report supports the view to aim to a give a high dose to large parts of the ptv with a maximum dose at the center of the ptv where the likelihood of tumor location of a moving target is highest . 
if this concept is correct , then it might be possible to use the sip concept with a lower dose in a peripheral subvolume of the ptv with lower likelihood of tumor cells being present without compromising local control . 
in this context it is also intriguing that in parotid sparing head and neck imrt locoregional recurrences were not observed to occur predominantly in the spared areas but within the highdose regions [ 1 , 25 ]  . 
the safety of sip critically depends on the reliability of the chosen dose constraints which also need to be validated in prospective trials . from the point of view of radiation biology , it should be stressed that the tumor front might harbor especially radioresistant subvolumes of the tumor . 
epithelial mesenchymal transition ( emt ) was described to be more prevalent in residual tumor subvolumes at the invasion front [ 4 ] which in turn was described to be enriched for cancer stem cells [ 2 ]  . 
another important factor of resistance to radiotherapy is hypoxia which is not restricted to the tumor core but also is found in subvolumes of the invasive front again warning from low doses at the edge of the tumor [ 6 ]  . 
with the eqd2 formula , isoeffective and isotoxic fractionations should be calculated . the prescription technique for sbrt described here allows accurate quantication of the dose delivered to dose limiting oars based on the sip approach . 
this system has two advantages : the dose sacrice to the ptv due to the proximity to a dose - limiting oar is fully quantied and can be used for local control analysis . 
this method can be used for sbrt with all sbrt equipment and is suitable for multicenter trials . conclusion we present a concept for sbrt and imrt close to highrisk oars that is expected to be safe and effective and at the same time suitable for multicenter clinical testing . 
we currently test this approach in a single center phase i trial in patients with thoracic and abdominal lesions and we are condent to thereby further increase the safety of sbrt . compliance with ethical guidelines conict of interest t.b. 
oktober 2016 springer - verlag berlin heidelberg 2016 fragestellung und hintergrund . in der vielzitierten imcl - 9815 - studie erfolgte eine randomisation zwischen strahlentherapie plus wchentlicher gabe von cetuximab oder alleiniger strahlentherapie , wobei unterschiedliche fraktionierungskonzepte mglich waren [ 1 ]  . 
nach strahlentherapie plus cetuximab waren vergleichbare unterschiede zu sehen ( hr 0 , 120 , 18 )  . originalpublikation rosenthal di , harari pm , giralt j et al ( 2016 ) association of human papillomavirus and p16 status with outcomes in the imcl - 9815 phase iii registration trial for patients with locoregionally advanced oropharyngeal squamous cell carcinoma of the head and neck treated with radiotherapy with or without cetuximab . 
obgleich ein deutlicher effekt nur in der p16 - positiven subgruppe vorlag , fand sich keine statistisch signikante interaktion zwischen dem behandlungsarm und dem p16 - status ( p = 0 , 085 )  . 
die zustzliche gabe von cetuximab zur strahlentherapie verbesserte sowohl bei p16 - positiven als auch p16 - negativen patienten die ergebnisse . kommentar inzwischen sind die frhen publikationen ber die bedeutung einer hpv - infektion fr das rezidivrisiko und das berleben nach alleiniger bzw . 
artscan , hatten patienten mit p16 - positiven tumoren ( n = 153 ; die p16 - expression gilt als surrogatmarker einer hpv - infektion ) eine bessere prognose [ 4 ]  . 
als folge der deutlich hheren rate an langzeitberlebenden wird groes augenmerk auf die nebenwirkungen der therapie und die lebensqualitt gelegt . die im ursprnglichen imcl - 9815 - studiendesign nicht geplante und jetzt retrospektiv durchgefhrte analyse des p16 - status bei patienten mit oropharynxkarzinomen kommt im vergleich zu den anderen studien relativ spt und kann , wie alle retrospektiven studien , keinen denitiven beweis fr die berlegenheit einer bestimmten therapie erbringen . 
zwar fand sich keine statistisch signikante interaktion zwischen dem behandlungsarm und dem p16 - status , aber der p - wert von 0 , 085 gibt raum fr spekulationen , inwieweit die fallzahl ausreichend war , um einen signikanten zusammenhang nachzuweisen . 
klar ist , dass die lokoregionale kontrollrate nach 3 jahren von 32 % und die berlebensrate von 42 % in der p16 - negativen cetuximab - gruppe weiter verbessert werden mssen . 
in diesem zusammenhang ist zu erwhnen , dass studien zur radiochemotherapie bei p16negativen patienten teilweise von 3 - jahres - berlebensraten von mehr als 70 % berichteten [ 6 ]  . fazit die im ursprnglichen imcl - 9815 - studiendesign nicht vorgesehene und jetzt retrospektiv durchgefhrte analyse des p16 - status bei patienten mit oropharynxkarzinomen trgt relevante erkenntnisse bei . 
bonner ja , harari pm , giralt j et al ( 2010 ) radiotherapy plus cetuximab for locoregionally advanced head and neck cancer : 5 - year survival data from a phase 3 randomised trial , and relation between cetuximab - induced rash and survival . 
rosenthal di , harari pm , giralt j et al ( 2016 ) association of human papillomavirus and p16 status with outcomes in the imcl - 9815 phase iii registration trial for patients with locoregionally advanced oropharyngeal squamous cell carcinoma of the head and neck treated with radiotherapy with or without cetuximab . 
mellin h , friesland s , lewensohn r et al ( 2000 ) human papillomavirus ( hpv ) dna in tonsillar cancer : clinical correlates , risk of relapse , and survival . 
zackrisson b , kjelln e , sderstrm k et al ( 2015 ) mature results from a swedish comparison study of conventional versus accelerated radiotherapy in head and neck squamous cell carcinoma the artscan trial . 
masterson l , moualed d , liu zw et al ( 2014 ) de - escalation treatment protocols for human papillomavirus - associated oropharyngeal squamous cell carcinoma : a systematic review and meta - analysis of current clinical trials . 
lorch jh , hanna gj , posner mr et al ( 2016 ) human papillomavirus and induction chemotherapy versus concurrent chemoradiotherapy in locally advanced oropharyngeal cancer : the dana farber experience . 
merlotti7 received : 12 april 2016 / accepted : 19 september 2016 / published online : 19 october 2016 springer - verlag berlin heidelberg 2016 abstract purpose to evaluate the outcomes with respect to longterm survival and toxicity in patients with nasopharyngeal carcinoma ( npc ) treated in a european country with low incidence . materials and methods a prospective observational study carried out by the airo head and neck group in 12 italian institutions included 136 consecutive patients treated with radiotherapy ( rt ) chemotherapy ( cht ) for npc ( without distant metastasis ) between january 1 , 2008 and december 31 , 2010 . results the disease - specic survival ( dss ) , overall survival ( os ) , and disease - free survival ( dfs ) at 5 years were 92 ( 2 ) , 91 ( 3 ) , and 69 % ( 5 % ) , respectively . 
an adequate minimum dose coverage to ptv ( t ) is a predictive variable well related to outcome . conclusion our data do not substantially differ in terms of survival and toxicity outcomes from those reported in contribution author ( s ) study concept : sandro tonoli study design : sandro tonoli data acquisition : s . 
spedali civili di brescia , piazzale spedali civili , 1 , 25123 brescia , italy 2 milan - european institute of oncology , milan , italy 3 roma - isola tiberina hospital , rome , italy irccs a.o.u. 
san martino ist genoa , genoa , italy 5 bologna - s.orsola hospital , bologna , italy 6 roma - s.camillo hospital , rome , italy 7 busto arsizio hospital , busto arsizio , italy 8 milan university monza s . 
gerardo hospital , milan , italy turin university , turin , italy 10 treviglio hospital , treviglio , italy 11 prato hospital , prato , italy 932 strahlenther onkol ( 2016 ) 192 : 931943 entwickelte imrt - technologien zur dosisverabreichung mittels bildgesttzter strahlentherapie knnten zu besserer ptv ( t ) - minimaldosis mit erhhter dfs fhren ; fernmetastasen nach der behandlung bleiben ein ungelstes problem . schlsselwrter berleben strahlentherapie chemotherapie toxizitt prognose introduction nasopharyngeal cancer ( npc ) is an uncommon cancer in europe and in italy [ 1 ]  . 
after the publication of the results of the intergroup 0099 study [ 2 ] , the addition of concurrent adjuvant platinum - based chemotherapy has become the standard practice for the treatment of locally advanced disease ( stage iii and iv )  . 
several randomized trials [ 3 , 4 ] comparing concomitant radio - chemotherapy ( ccht / rt ) and radiation alone conrmed that the addition of concomitant chemotherapy ( c - cht ) was more effective in terms of survival , but it was associated with higher acute toxicity rates . 
on the contrary , data on late toxicity were found to be similar in the two treatment arms , even if the c - cht / rt arm had a slightly higher rate of noncancer - related deaths . induction chemotherapy ( n - cht ) followed by c - cht / rt has been also investigated as a feasible treatment modality in locally advanced npc , but it is not considered a standard therapy [ 5 ]  . moreover , the pooled analysis by lee et al . [ 6 ] comparing conventional and accelerated radiotherapy , with or without chemotherapy ( concurrent and adjuvant ) , showed that radiation dose , fractionation , number of chemotherapy cycles ( both concurrent and adjuvant ) are all variables that exert a signicant effect both on survival and toxicity . while many articles have been published by eastern groups on this topic , fewer studies have been published by european investigators due to the rarity of npc in europe . 
the head and neck study group of the italian society of radiation oncology ( airo ) launched a multicenter prospective observational analysis in 2007 in order to nd conrmations or discrepancies with the data reported in eastern published series in terms of correlations of dosimetric data with clinical outcome and toxicity . larger series of patients treated in countries with higher incidences of npc . 
sophisticated technologies of dose delivery ( imrt ) with image - guided radiotherapy could help to obtain better minimum ptv ( t ) coverage dose with increased dfs ; distant metastasis after treatment still remains an unresolved issue . keywords survival radiotherapy chemotherapy toxicity prognosis nasopharynxkarzinom in einem europischen gebiet mit geringer inzidenz eine prospektive beobachtungsanalyse der kopfund halsstudiengruppe der italienischen gesellschaft fr radioonkologie ( airo ) zusammenfassung ziel bewertung von langfristigem berleben und toxizitt bei patienten mit nasopharynxkarzinom ( npc ) , die in einem europischen land mit geringer inzidenz behandelt wurden . materialien und methoden die prospektive beobachtungsanalyse , durchgefhrt von der airo kopfund hals - gruppe an 12 italienischen zentren , beinhaltete 136 folgepatienten , die zwischen 1 . 
dezember 2010 wegen npc ( ohne fernmetastasen ) mit strahlentherapie ( rt ) chemotherapie ( cht ) behandelt wurden . ergebnisse die krankheitsspezische berlebensrate ( dss ) , das gesamtberleben ( os ) und krankheitsfreie berleben ( dfs ) nach 5 jahren waren jeweils 92 % ( 2 % ) , 91 % ( 3 % ) und 69 % ( 5 % )  . 
die kontrollwahrscheinlichkeit liegt lokal , regional und lokoregional nach 5 jahren bei 89 % ( 3 % ) , 93 % ( 3 % ) und 84 % ( 4 % )  . 
die inzidenz der akuten und spten toxizitt und korrelationen mit verschiedenen klinisch / technischen variablen wurden analysiert . neoadjuvante cht verlngert die zeit der gesamtbehandlung und reduziert die therapiecompliance whrend der zusammen durchgefhrten radiochemotherapie . 
eine angemessene minimaldosis von ptv ( t ) ist eine prdiktive variable , die gut mit der berlebensquote korreliert . schlussfolgerung unsere daten zeigen keinen groen unterschied bezglich der berlebensquote und toxizitt im vergleich zu denen aus lndern mit hherer npc - inzidenz . 
weiterstrahlenther onkol ( 2016 ) 192 : 931943 table 1 karnofsky performance status scale , histology , grading and stage of disease , t and n classes according to tnm 6th edition . 
the gross ( gtv ) , clinical ( ctv ) , and planning target volumes ( ptv ) were dened according to icru 62 and 83 specications [ 15 ]  . 
all the relevant organs at risk ( oar ) were contoured . doses to parotid glands according to nodal status were also analytically collected and summarized . doses were expressed in gy or as 2 gy / fraction equivalent doses ( eqd2 ) , considering a / value of 10 gy for npc . since different fractionation schemes and total doses were delivered , a dichotomous variable to dene compliance to the planned treatment time has been dened , considering two classes : the rst includes overall radiotherapy treatment times ( ott ) no more than 5 days longer than planned , the second ott 6 days or more longer than planned . 
two cases were judged unt to tolerate prophylactic treatment to clinically negative neck nodal regions . most patients ( 123 / 136 ) were treated using intensitymodulated radiotherapy ( imrt ) with simultaneous integrated boost ( sib ) ( 19 of them were treated with helical tomotherapy ) ; in 6 patients imrt included a sequential boost instead of sib ; 7 cases were treated with three - dimensional conformal radiotherapy ( 3dcrt )  . 
the ctv was dened according to the policy of the single center ( with a margin from the gtv not inferior to 5 mm , corrected by anatomical barriers )  . 
the ptv was obtained by adding a margin in all the directions , usually between 3 and 5 mm . exclusive radiotherapy was given to only 12 patients : 3 stage i , 6 stage ii , 1 stage iii , and 2 stage iv . n - cht was given in 69 cases ( 51 % )  . 
changes in these schedules were adopted in 18 patients : in 7 patients tpf was given with paclitaxel instead of docetaxel , in 7 patients cisplatin ( cddp ) and epirubicine ( epi ) were given [ 18 ] ; other drug combinations were chosen in the remaining 3 cases . planned cycles number varied sometimes from the original schema , but 2 or 3 cycles were usually given ( 25 and 37 cases , respectively ) ; more cycles ( 46 ) were given in 5 cases . 
three stage iv cases were not given c - cht , one because of gastrointestinal g3 toxicity observed during the induction phase , two because were judged unt for c - cht . cddp was used alone ( 40 mg / m2 weekly in 69 cases , 100 mg / m2 every 3 weeks in 45 cases ) or associated with 5 - fu ( 7 cases )  . 
cutaneous toxicity was related only to ptv ( t ) ( d1 % and d5 % ) and dysgeusia with ptv ( t ) ( d1 % )  . the statistically signicant factors found at univariate analysis were evaluated with a logistic multivariate regression ( backward stepwise method wald )  . 
similar results were found for functional mucositis and dysphagia , while for pain and dysgeusia only d1 % to ptv was statistically signicant ( data not shown )  . long - term results the median time of follow - up was 42 months ( range 277 months )  . 
cum survival cumulative survival without disease , 22 alive with disease , 12 dead ( 10 due to the tumor , 2 for other causes not related to treatment )  . 
local , regional , and locoregional control probability at 5 years were 89 ( 3 ) , 93 ( 3 ) , and 84 % ( 4 % )  . ten , 5 , and 21 patients had a local relapse , locoregional relapse , and distant failure ( 15 with locoregional control ) , respectively . 
one patient with local recurrence underwent surgery obtaining complete remission ( ned after 3 years ) ; another patient was treated with re - irradiation , but he died after a few months from disease progression ; a third patient , treated with chemotherapy , had no evidence of disease ( ned ) after 15 months . 
one of the patients relapsed with m1 ( bone ) was treated with chemo + rt obtaining again a cr ( ned 4 years after treatment for relapse )  . 
the results of the univariate analysis are reported in table 5 . the signicant variables at univariate analysis have been evaluated with multivariate analysis by cox proportional hazards model : t class was identied as independent prognostic predictor of dss and os . 
treatment technique ( imrt with tomotherapy was better than imrt with other techniques , both better than the few cases of 3dcrt ) resulted an independent prognostic predictor of dfs and eqd2 ptv ( t ) d95 % of local control ( better results with doses > 60 gy )  . the incidence of late sequelae at 1 and 3 years are listed in table 6 . 
g1 brain damage totaled 1.4 % at 3 years . no cases of myelitis or cataract were observed after 3 years . strahlenther onkol ( 2016 ) 192 : 931943 discussion this prospective study describes the management of npc in 12 italian centers and it represents the real clinical behavior of practicing radiation oncologists , outside randomized clinical trials . clinical results of the present series are accordant to the ones previously reported in the literature [ 27 ]  . 
the main prognostic factor for survival were identied to be t class , whereas n classication was not a good predictor for regional and distant failure and survival , which is in contrast with data found in the literature . 
in the present series , stage has a good progressive correlation with dss , os , lc , and lrfs , but not with dmfs and dfs . neo - adjuvant chemotherapy is widely used , as reported also in countries with a higher incidence of npc [ 27 ] , even if the evidence of its superiority over concomitant radio - chemotherapy is missing [ 19 ]  . 
our cases treated with n - cht obtained lower rates of survival outcomes ( but not statistically signicant ) , even if they do not seem to be unfavorably selected ( data not shown )  . 
this suggests that delays in starting radiation treatment or the reduction in gtv induced by n - cht are not a sufcient reason to support this choice outside clinical trials . 
in our series , neo - adjuvant tpf , as compared to pf , was not related to a better outcome . the use of n - cht does not signicantly worsen compliance ( dened in terms of cycles given / planned ) to c - cht / rt . 
however , this observation should be considered cautiously , because 3 patients treated with neo - adjuvant chemotherapy manifested toxicities not allowing the association of radiotherapy with concomitant chemotherapy . moreover , patients with excessively long radiotherapy ott were treated signicantly more often with neo - adjuvant chemotherapy . 
the increase in radiotherapy ott could counteract the overall survival benet of adding chemotherapy , even if this association did not reach statistical signicance in the present dataset . in a recently published study , a signicantly better overall survival was observed when more than 5 cycles of 40 mg / m2 weekly in our study the given mean cisplatin were given [ 21 ]  . dose of cddp was lower than that ( 150 mg / m2 ) in patients treated without n - cht and even more in those previously treated with n - cht . 
however , in the patients who received less than 200 mg / m2 of cddp ( the equivalent of 5 cycles of weekly cddp 40 mg / m ) concomitant to radiotherapy in our analysis the outcome was worse than in patients who received more than 200 mg / m2 of cddp , but the difference did not reach statistical signicance . 
the poor compliance to concomitant chemotherapy was particularly evident in patients treated with a 2.3 gy fractional dose , a subsequently abandoned fractionation . technical level of radiation treatment was high in the imrt was used in about 90 % of the recruiting centers . cases , the remaining ones having been treated with 3dcrt . better homogeneity of dose distribution to the target was shown in the cases treated with tomotherapy , but the lower doses prescribed do not allow correlations with toxicity . the wide diffusion of imrt has led to the use of sib along with different fractionations , in an attempt to tailor the treatment , considering previous chemotherapy , volume to be treated , and patient tolerance . 
the sib technique permits reduction of the volume receiving high dose outside ptv ( t ) and ptv ( n ) ( high dose ptvs ) , so it has been adopted by most centers regardless of the evidence of large competitive clinical trials for nasopharyngeal carcinoma . in a recently published meta - analysis [ 23 ] , 13 / 411 studies with 2920 npc cases staged with mri between 1990 and 2006 were considered . 
these results conrm the difculties of obtaining good parotid sparing , while retaining adequate target coverage , even with imrt or tomotherapy or using small ctvptv margins ( 35 mm ) [ 26 ]  . 
the increase in the minimal dose to ptv ( t ) ( eqd2gy d95 % ) 942 strahlenther onkol ( 2016 ) 192 : 931943 is more strictly related to a progressively better dss / os . the reported late toxicities were not greatly different from those reported by larger series [ 27 ] , but we did not nd cases of g2 or higher grade radiation - induced brain damage at 3 years . our analysis has some limitations due to the small number of cases . 
every patient gave informed consent for the treatment and the permission to use their data for this prospective observational analysis . ethical standards the treatments given to the patients have been performed in accordance with the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . conclusions nasopharyngeal carcinoma is quite rare in italy , but , in terms of clinical outcome , we did not nd great differences from the much larger eastern series , with the exception of a different incidence of nodal metastasis in levels i and iv . the staging of the disease ( tnm 2002 uicc ) had a progressive correlation with the outcome . 
therefore , the use of sophisticated technologies of dose delivery ( imrt ) with image - guided radiotherapy ( igrt ) could help in this objective , even if the incidence of distant metastasis after treatment remains an unresolved issue . 
even if survival and toxicity results in this series appear good , some therapeutic options may have a negative impact on treatment compliance and toxicity ( the use of n - cht or that of high fractional doses )  . 
therefore , the airo head and neck study group will continue to support efforts for multicenter prospective controlled studies , data collection , and updated guideline validation . acknowledgements the authors thank the 136 patients who consented to release their data for the analysis . 
a particular acknowledgement to filippo bertoni for his help with statistical analyses and to gundi steinhilber for the german translation of the abstract . compliance with ethical guidelines conict of interest s . 
in behandlungsanstzen mit selinexor und / oder einzelnen bestrahlungen mit 5 gy wurden mit hilfe von mtt - assay , caspase - 3 / 7 - aktivitt , annexinvfitc / pi - assay und klonogenem assay die apoptoserate bzw . 
caspase - 3 / 7 - assays und western - blot - analysen zeigten , dass die zellen mit steigender selinexordosis huger in apoptose bergehen und dass parp strker gespalten wird . 
selinexor steigert sowohl in vitro als auch in vivo in mausmodellen die apoptose und die strahlenwirkung an tumoren . originalpublikation ferreiro - neira i et al ( 2016 ) xpo1 inhibition enhances radiation response in preclinical models of rectal cancer . 
bei vielen tumoren ist xpo1 strker exprimiert , was einen verstrkten export von tumorsuppressoren , wie beispielsweise survivin und fbw7 , aus dem zellkern zur folge hat [ 3 , 5 ]  . auf die rolle von survivin fr die strahlentherapie wurde in dieser zeitschrift bereits hingewiesen [ 6 ]  . 
in letzteren ist diese kaskade hug unkontrolliert aktiv und frdert so das krebswachstufbw7 ist teil einer ubiquitinligase , welche in gesunden zellen die degradation der intrazellulren notch - domne ( nicd ) bewirkt . 
auerdem konnte vor einigen jahren in mausmodellen gezeigt werden , dass heterozygote fbw7 - knockout - muse nach einer einmaligen bestrahlung mit 4 gy binnen 65 wochen tumoren bildeten , was bei den wildtyp - musen nicht der fall war . 
roedel c , graeven u , fietkau r et al ( 2015 ) oxaliplatin added to uorouracilbased preoperative chemoradiotherapy and postoperative chemotherapy of locally advanced rectal cancer ( the german cao / aro / aio04 study ) : nal results of the multicentre , openlabel , randomised , phase 3 trial . 
abdul razak ar , mausoerensen m , gagrail my et al ( 2016 ) firstin - class , rst - in - human phase i study of selinexor , a selective inhibtor of nuclear export , in patients with advanced solid tumors . 
gao j , azmi as , aboukameel a et al ( 2014 ) nuclear retention of fbw7 by specic inhibitors of nuclear export leads to notch1 degradation in pancreatic cancer . 
brunner2 maximilian niyazi3 matthias guckenberger1 received : 19 may 2016 / accepted : 19 september 2016 / published online : 24 october 2016 springer - verlag berlin heidelberg 2016 abstract purpose this report of the working group on stereotactic radiotherapy of the german society of radiation oncology ( degro ) aims to provide a literature review and practice recommendations for stereotactic body radiotherapy ( sbrt ) of primary renal cell cancer and primary pancreatic cancer . methods a literature search on sbrt for both renal cancer and pancreatic cancer was performed with focus on prospective trials and technical aspects for clinical implementation . results data on renal and pancreatic sbrt are limited , but show promising rates of local control for both treatment sites . 
motion - compensation strategies and image guidance are paramount for safe sbrt delivery in both tumor entities . conclusion sbrt for renal cancer and pancreatic cancer have been successfully evaluated in phase i and phase ii trials . 
fr beide tumorentitten sind strategien zur bewegungskompensation und bildgefhrte strahlentherapie fr die sichere durchfhrung der behandlung zwingend notwendig . schlussfolgerung die sbrt zur behandlung des pankreaskarzinoms und des nierenzellkarzinoms ist erfolg876 strahlenther onkol ( 2016 ) 192 : 875885 reich in phase - i / ii - studien durchgefhrt worden . pankreas - sbrt sollte aktuell nur in prospektiven studienprotokollen praktiziert werden , da ein potentielles risiko fr schwerwiegende gastrointestinale nebenwirkungen besteht . 
fr das nierenzellkarzinom stellt die sbrt eine behandlungsoption fr inoperable patienten dar , wobei insbesondere die optimale patientenselektion und technische aspekte in zuknftigen studien untersucht werden sollten . schlsselwrter krperstereotaxie pankreaskarzinom nierenzellkarzinom pankreas - sbrt nieren - sbrt introduction stereotactic body radiotherapy ( sbrt ) has become a guideline - recommended treatment and standard of care in modern radiation oncology [ 1 ] : it is characterized by delivery of high doses of irradiation in one or few fractions to extracranial tumors using techniques for highly conformal and accurate target localization such as an external coordinate system and advanced image guidance [ 2 ]  . 
the concept has shown impressive rates of local control both in primary tumors such as stage i non - small cell lung cancer ( nsclc ) [ 2 ] and in the treatment of metastases at various sites [ 3 , 4 ]  . 
additionally , stereotactic radiotherapy has shown high rates of local control in intracranial and extracranial metastases of tumor histologies that are generally considered resistant to conventionally fractionated radiotherapy , which gives promise for its translation to other primary tumor sites [ 5 ]  . 
we focus on prospective studies and give practice recommendations for clinical application outside of clinical trials . study selection we performed a comprehensive literature search of papers and abstracts published in english until june 2016 on sbrt for pancreatic cancer and renal cell cancer using the pubmed database . 
the resultant papers were independently reviewed for relevance by two radiation oncologists ( cp and na )  . both retrospective and prospective studies were included in the reviewing process , although the main focus of the review is on prospective trials . 
for ongoing studies , a search on clinicaltrials.gov was performed using the abovementioned keywords and a representative selection was included in this article . sbrt for renal cell cancer rationale for sbrt renal cell cancer ( rcc ) is the seventh most common cancer in men , the ninth most common cancer in women , and accounts for 2 %3 % of all adult malignancies [ 6 , 7 ]  . 
standard therapy for primary rcc is the complete resection of the tumor by radical or partial nephrectomy , which is even recommended in metastasized rcc [ 8 ]  . historically , radiotherapy has played a very limited role in the treatment of primary rcc based on negative prospective studies on perioperative radiotherapy [ 9 ] , although retrospective analyses suggest improved local control for adjuvant radiotherapy in tumors with perinephric invasion and positive margins [ 10 , 11 ]  . radiotherapy for rcc has therefore been restricted to the palliative treatment of metastatic sites [ 12 , 13 ]  . 
rcc has been traditionally considered less radiosensitive using conventionally fractionated radiotherapy [ 14 ] , but stereotactic radiotherapy using high fraction and total doses achieved local control rates above 90 % in metastatic rcc at intracranial and extracranial target sites such as lung and spine metastases [ 5 , 15 , 16 ]  . 
based on the promising experiences in the treatment of metastatic rcc , sbrt has consequently been investigated as denitive therapy for primary renal cell cancer [ 17 , 18 ] : this is in patients refusing surgery or being medically inoperable , as well as in patients with bilateral tumors or a contralateral recurrence after nephrectomy who are at risk of chronic hemodialysis after radical resection . clinical results of renal sbrt to date , several prospective trials on sbrt for primary rcc have been published which are summarized in table 1 . 
 [ 23 ] phase ii , 19992004 13.7 months reached ; 3 - year os 72 % stable disease at 6 months in all evaluable patients 98 % for all lesions 32 months for all patients 52 months for patients alive , 22 for deceased patients staehler et al . 
 [ 17 ] phase ii , 20072011 28 months 98 % at 9 months not yet reached rcc renal cell carcinoma , os overall survival , 3dcrt three - dimensional conformal radiotherapy , itv internal target volume , pts . 
patients , ptv planning target volume a single fraction of 25 gy for smaller tumors , both prescribed to the planning target volume ( ptv ) - surrounding isodose ( generally 7585 % )  . 
using a 3d - conformal technique , the authors reported grade 12 acute toxicity in 60 % of the patients which was mainly restricted to nausea , chest wall pain , and fatigue . 
however , the authors reported only on patient follow - up up to 6 months , which was too short for the evaluation of late toxicity and local tumor control [ 20 ]  . 
a separate analysis of renal dysfunction one year after treatment showed a moderate , clinically acceptable deterioration of the glomerular ltration rate as well as a dose - dependent regional function loss in the irradiated kidney by spect / ct [ 21 ]  . 
 [ 22 ] performed a phase i dose escalation study with 19 medically inoperable patients with renal cancer by delivering 4 fractions of 612 gy prescribed to the 6575 % isodose using robotic radiosurgery . 
the maximum planned dose of 48 gy in 4 fractions was safely administered with tolerable toxicity ( including one case of grade 4 duodenal ulcer possibly related to therapy )  . 
with a median follow - up of 13.7 months , all evaluable patients showed radiologically stable disease ( 80 % ) or partial remission ( 20 % ) , while biopsies at the median of 9 months posttreatment remained positive in the majority of cases ( 64 % ) [ 22 ]  . 
the investigators used various treatment schedules with 35 fractions of 515 gy prescribed to the ptv margexcellent local tumor control of crude 98 % and mild side effects with 54 % acute grade 12 toxicity were reported [ 23 ]  . 
 [ 17 ] 878 strahlenther onkol ( 2016 ) 192 : 875885 reported on the largest prospective series of 40 patients with primary renal tumors , including 11 patients with transitional cell cancer of the renal pelvis , who underwent robotic radiosurgery with a single dose of 25 gy prescribed to the 70 % isodose . 
no signicant deterioration of renal function nor any grade 3 or greater side effects have been observed in any patient . prospective data on sbrt for primary rcc is complemented by several retrospective patient series , which demonstrate local control rates from 86100 % with a median follow - up of 1749 months [ 2428 ]  . 
the authors consistently report very low toxicity rates without any grade 3 or higher event , but the results have to be judged carefully due to the small patient numbers which were mainly below ten per trial . clinical practice the majority of published series on renal sbrt included patients with histology - proven renal cancer and initial diagnosis on abdominal computed tomography ( ct )  . 
magnetic resonance imaging ( mri ) and positron emission imaging ( pet ) play currently only a minor role in diagnostic imaging of renal tumors [ 29 ] , although additional mri imaging is frequently used for treatment planning [ 30 ]  . 
all study patients were medically inoperable or refused the risks of surgery . important aspects of sbrt in the abdomen are strict patient immobilization and control of internal respiratory motion , which are accounted for by various techniques [ 31 ]  . patient immobilization was achieved by most investigators using vacuum stabilization systems and , in some series , with additional abdominal pressure devices to reduce respiratory motion [ 25 , 27 ]  . 
the mean breathing - induced displacement of the kidney on 4d - ct was found to be about 0.75 cm for both sides in a series of 62 patients , but may be up to a maximum of 2 cm [ 32 ]  . 
the correlation between kidney motion and surrogate parameter such as diaphragmatic motion or abdominal wall motion was reported to be relatively poor [ 32 ] ; additionally , breathing patterns may vary between the planning ct and during radiotherapy [ 33 ]  . 
daily image guidance is considered as mandatory using either conebeam ct or planar stereoscopic x - ray imaging combined with implanted markers ; each igrt strategy needs to take breathing - induced target motion fully into account . 
in most studies , the clinical target volume ( ctv ) was identical to the gross tumor volume ( gtv ) , meaning no safety margins to compensate for potential microscopic disease were used . minimum ptv margins were 510 mm , mostly depending on the immobilization technique and motion compensation strategies [ 20 , 23 ]  . 
technetium ( 99 m ) mag - 3 renal scintigraphy prior to sbrt may help to estimate the relative contribution of right and left kidneys and of regional inhomogeneities of excretion . treatment was applied using linac - based 3d - conformal radiotherapy with 58 coplanar and non - coplanar beams in the majority of studies [ 20 , 23 ] , or , alternatively , with cyberknife robotic radiosurgery [ 17 , 19 , 22 ]  . there are currently no reports on volumetric modulated arc therapy ( vmat ) for renal sbrt , although it has shown dosimetric advantages for sbrt in other tumor entities and might therefore be used in future trials [ 34 ]  . published studies on renal sbrt used a wide variety of radiation dose and fractionation , which differed considerably even within single institution series [ 25 , 27 ]  . 
to date , most centers experienced in renal sbrt use 3 - fraction schedules with 3645 gy total dose or 5 - fraction schedules with 4050 gy total dose [ 30 ]  . 
future studies also need to address the limited knowledge about the doseeffect relationship of functional renal tissue and radiation tolerance of the stomach and other critical gastrointestinal organs and structures . in conclusion , sbrt appears a viable option for primary rcc but future research needs to better dene patient selection criteria and the detailed practice of sbrt . 
additionally , renal sbrt could potentially provide a less - invasive alternative to cytoreductive surgery in patients with limited metastatic disease , although there is currently no evidence for this approach . 
with the advent of new immunotherapies such as the anti - pd - 1 checkpoint inhibitor nivolumab for metastatic rcc [ 37 ] , sbrt of rcc may in the future also have a role as immunostimulatory agent by increasing intratumoral antigen presentation and the t - cell receptor repertoire as shown in preclinical studies [ 38 ]  . rationale for pancreatic sbrt pancreatic ductal adenocarcinoma ( pca ) is the 10th most common solid tumor in europe and the usa and the 4th leading cause of cancer death due to its poor prognosis with a 5 - year overall survival of 7 % for all stages combined [ 39 , 40 ]  . 
surgery is currently the only treatment modality performed with curative intent , but only 20 % of pca patients present with resectable disease , while each 40 % present with unresectable , locally advanced disease , and metastatic disease , respectively [ 41 ]  . 
although early metastatic spread is common in pca , local control remains an important aim in the treatment of pca in order to prevent pain and obstructive symptoms and to improve the patients quality of it was found that up to 30 % of pca patients life [ 42 ]  . died of local progression with little metastatic tumor burden which highlights the need for an effective local therapy [ 43 ]  . conventionally fractionated chemoradiation ( crt ) has traditionally been used in inoperable patients after induction chemotherapy as consolidation therapy with doses up to 60 gy and concurrent 5 - uorouracil - based chemotherapy or gemcitabine [ 44 ]  . 
technological advances such as imrt , igrt , and breathing motion compensation have shown to facilitate dose - escalated chemoradiotherapy with reduced doses to organs - at - risk and tolerable toxicity [ 45 ]  . 
however , even combined chemoradiation shows local control rates of less than 40 % after two years with local failure as signicant predictor of overall survival ( os ) [ 46 ]  . 
 [ 52 ] phase ii 16 lapc gemcitabine before and after sbrt ( median 4 cycles , range 19 cycles ) 11.4 months 81 % ( 1 - year lc : 100 % ) schellenberg et al . 
the advantages of sbrt include the possibility to deliver higher biological effective doses than in conventional radiotherapy as well as patient comfort and better integration into multidisciplinary treatment concepts due to signicantly shorter treatment courses , shorter interruption of full - dose chemotherapy , and signicantly less bone marrow toxicity [ 49 ]  . clinical results of pancreatic sbrt most prospective studies and retrospective patient series of sbrt for pancreatic cancer have been performed in locally advanced disease ( table 3 ) , but this experience has been strahlenther onkol ( 2016 ) 192 : 875885 recently complemented by rst data on sbrt in borderline resectable tumors as well as in the adjuvant setting and for re - irradiation [ 48 ]  . prospective data on sbrt in locally advanced pancreatic cancer ( lapc ) has rst been generated by the stanford group in four phase iii trials starting more than a decade ago . 
toxicity was substantially higher in a subsequent trial when single - dose sbrt of 25 gy was performed after a 5 - week course of 5 - fu - based chemoradiotherapy of 45 gy : 69 % of patients experienced acute grade 12 toxicity and 13 % acute grade 3 toxicity [ 51 ]  . 
with a median os of less than 8 months , local control was 94 % , but 13 % of patients developed duodenal ulcers as late toxicity [ 51 ]  . 
consequently , the role of cyberknife - based single - dose sbrt for lapc was investigated in combination with systemic therapy with gemcitabine before and after irradiation in a phase ii trial with 16 patients [ 52 ]  . 
while acute toxicity was tolerable , 31 % of patients developed gastric and duodenal ulcers and two patients ( 13 % ) showed late grade 4 toxicity including one case of intestinal obstruction and duodenal perforation each 2046 weeks after treatment [ 52 ]  . 
a second phase ii trial combining singledose sbrt of 25 gy ( prescribed to the icru reference point ) with preceding and subsequent gemcitabine - based chemotherapy demonstrated in 20 patients equivalent local control and comparable toxicity using a linear acceleratorbased ( linac ) treatment instead of the cyberknife system [ 53 ]  . 
in summary of these trials , single - fraction sbrt with doses of 25 gy was not feasible due to substantial gastrointestinal ( gi ) toxicity while os remained disappointing . subsequently , hypofractionated sbrt treatment regimens were investigated as alternative to single - dose treatment in order to reduce normal tissue toxicity while maintaining equivalent local control . an early danish study performed linac - based fractionated sbrt with a 1 - week schedule of 3 fractions of 15 gy prescribed to the icru reference point in 22 patients with lapc [ 54 ]  . 
a high rate of 79 % of patients progressed to grade 2 or higher acute toxicity after treatment and 2 patients ( 9 % ) showed late grade 2 toxicity ( mucosal ulcers ) and 1 patient ( 5 % ) late grade 4 toxicity ( gastric perforation ) , most likely due to relatively large treatment volumes and the lack of dose constraints for organs at risk ( oars ) [ 54 ]  . more recently , a multi - institutional phase ii study of 49 patients with lapc applied a linac - based hypofractionated sbrt regimen of ve consecutive fractions of 6.6 gy prescribed at the ptv - surrounding isodose ( 77 % ) during a treatment break of gemcitabine - based chemotherapy [ 55 ]  . 
using modern image - guidance and motion compensation strategies as well as fdg - pet - ct - based planning and strict oar dose constraints , acute and late gastrointestinal grade 2 or higher toxicities were reduced to 2 % and 11 % , respectively . 
 [ 56 ] published a phase ii trial of 45 patients with inoperable node - negative lapc using a similar regimen of 6 fractions of 7.5 gy prescribed to the mean ctv dose . 
toxicity was mild with no greater than grade 2 acute and late toxicity . the available prospective data of sbrt in lapc is complemented by several retrospective patient series using single - fraction [ 57 , 58 ] and hypofractionated sbrt [ 59 , 60 ] in locally pancreatic cancer demonstrating equivalent high rates of local control which compare favorably to conventionally fractionated ebrt regimens . 
however , a series including 57 patients with brpc treated with gemcitabine - based chemotherapy and fractionated sbrt showed that 56 % of the patients underwent surgery with an impressive r0 resection rate of 97 % and a median os of 19.3 months in these patients [ 62 ]  . 
sbrt was applied in ve fractions with a median total dose of 25 gy to the tumor and 35 gy as simultaneous integrated boost to the region of vessel involvement [ 62 ]  . 
likewise a smaller series of 12 patients with brpc treated with neoadjuvant chemotherapy and fractionated sbrt demonstrated a r0 resection rate of 92 % and a complete or extensive pathologic response in 42 % [ 63 ]  . due to the high postoperative local recurrence rate in patients undergoing surgery , sbrt may also play a role as adjuvant therapy in pancreatic cancer . 
a series of 24 resected 882 strahlenther onkol ( 2016 ) 192 : 875885 table 4 dose constraints for sbrt for pancreatic cancer in ve fractions derived from a recent multicenter phase ii study [ 55 ] organ at risk dose constraint duodenum , stomach , small bowel liver combined kidneys spinal cord d9cc < 15 gy , d3cc < 20 gy , d1cc < 33 gy d50 % < 12 gy d75 % < 12 gy d1cc < 8 gy patients with close or positive margins received a postoperative sbrt treatment with a median single dose of 24 gy resulting in a favorable freedom from local progression of 66 % at 1 year and a median os of 26.7 months with no observed late grade 3 toxicity [ 64 ]  . 
additionally , a retrospective series of 18 patients reports on re - irradiation of local recurrences after chemoradiotherapy using sbrt with a median dose of 25 gy in ve fractions without severe side effects [ 65 ]  . clinical practice although initial studies on sbrt for pancreatic cancer have demonstrated excellent local control with single - dose radiotherapy , these regimens have been abandoned due to excessive gastrointestinal toxicity [ 61 ]  . 
the most recent patient series published from experienced centers in pancreatic sbrt use fractionated regimens , mainly with 5 to 6 fractions of 57.5 gy either on consecutive days or every other day [ 55 , 56 , 60 , 62 , 66 ]  . 
moderately dosed sbrt for pancreatic cancer is also supported by a comprehensive review showing no signicantly improved local control rates and no os benet beyond biological effective doses ( bed ) of 75 gy [ 67 ]  . 
these ndings might be explained by insufcient systemic therapy employed in sbrt series with high bed as well as by toxicity related to radiation dose to normal tissue [ 67 ]  . current strategies to reduce radiation exposure of organs at risk imply accurate imaging as well as motion compensation techniques [ 55 , 56 , 61 ]  . 
with regard to imaging , contrast - enhanced ct is often complemented by pet - ct to improve tumor delineation in contrast to the surrounding edema [ 54 , 55 ]  . 
additionally , most contemporary series use 4 - dimensional planning ct scans to assess breathing motion [ 55 , 61 ] although it has been shown that 4d - ct alone is not sufcient to determine the extent of intrafraction movement [ 68 , 69 ]  . 
mri can provide information on organ motion on cine sequences [ 70 ] and has been investigated for target volume delineation resulting in reduced gtv volumes [ 71 ] , but there is the risk that mri may underestimate tumor extension compared to the pathological specimen [ 72 ]  . 
interand intrafraction organ movement can be further reduced by vacuum stabilization systems and , particularly if excessive respiratory motion is observed on 4d - ct , by abdominal pressure devices and / or respiratory gating [ 55 , 73 ]  . both linac - based and cyberknife - based sbrt series frequently employ endoscopic ultrasound - guided implantation of gold ducial markers before planning ct to improve daily patient positioning [ 55 , 61 , 73 ]  . the gtv is generally delineated as macroscopic tumor dened by all available imaging study with an additional internal target volume ( itv ) margin to compensate for organ motion . 
most series do not include elective lymph nodes [ 61 ] , although suspicious peripancreatic nodes have been included in the ptv by some authors if dose constraints were met [ 55 ]  . 
some authors crop the ptv at intestinal luminal structures to avoid excessive exposure of organs at risk [ 55 , 60 ] , although this is not in line with icru standards . regarding dose constraints for organ at risks with sbrt in ve fractions , most authors constrain the maximal dose to the duodenum , stomach , and bowel to 33 gy ( dose to 12 cc ) [ 55 , 61 , 73 ] with different lower - dose constraints ranging from d3cc < 20 gy [ 55 ] to a mean dose of 20 gy [ 73 ]  . 
similar dosevolume constraints including a d1cc < 36 gy for the duodenum have been implied by comito et al . [ 56 ] for a sbrt schedule of six consecutive fractions . future directions and conclusion the main advantages of sbrt for pancreatic cancer are that high rates of local control can be achieved with a short treatment course which facilitates combination with fulldose chemotherapy . 
consequently , ongoing trials are testing sbrt in combination with escalated chemotherapy regimens such as folfirinox ( nct02128100 ; nct02292745 ; nct01926197 ) which has already shown to improve os compared to gemcitabine - based chemotherapy in metastatic pancreatic cancer [ 75 ]  . 
additionally , sbrt is currently investigated as neoadjuvant treatment in order to increase operability and r0 resection ( nct01918644 ; nct02208024 ; nct01754623 )  . although rst reported experiences of sbrt for pancreatic cancer are promising , this treatment is still experimental and should not be practiced outside of prospective trials . this is particularly important as tolerance doses of sensitive organs at risk such as the duodenum and stomach in strahlenther onkol ( 2016 ) 192 : 875885 immediate vicinity of the target volume are still not clearly dened or validated . compliance with ethical guidelines conict of interest cdric panje , n . 
guckenberger declare that they have no competing interests . this article does not contain any studies with human participants or animals performed by any of the authors . strahlenther onkol ( 2016 ) 192 : 963964 doi 10.1007 / s00066 - 016 - 1078 - 5 acknowledgement to reviewers thank you to all reviewers of strahlentherapie und onkologie 2016 rainer fietkau1 frederik wenz2 online publiziert : 17 november 2016 springer - verlag berlin heidelberg 2016 we would like to deeply thank all of those who make the success of strahlentherapie und onkologie possible by supporting the editors - in - chief with their reviews to articles submitted . 
we are grateful for your dedication to provide the authors with helpful and precise reviews and for keeping the review times as low as possible . this list includes reviewers registered to the online submission system editorial manager , but we would like to also thank all reviewers who supported us by personal communication and may not be on this list . 
patients also received high - dose - rate mri - guided brachytherapy of 5 gy in 6 fractions . results we analyzed 128 patients with international federation of gynecology and obstetrics stage ibivb cervical cancer who underwent mri - guided brachytherapy . 
negative pelvic lymphadenopathy , gross tumor volume ( gtv ) dose covering 90 % of the target ( gtv d90 ) of > 110 gy , and treatment duration ( cid : 2 ) 56 days were associated with better overall survival in univariate analyses . 
gtv d90 of > 110 gy and treatment duration ( cid : 2 ) 56 days were potentially associated with overall survival . keywords conformal radiotherapy helical tomotherapy gynecology lymph nodes chemotherapy electronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 016 - 1049 - x ) contains supplementary material , which is available to authorized users . magnetresonanztomographisch gesteuerte brachytherapie bei gebrmutterhalskrebs prognostische faktoren fr das berleben ( cid : 2 ) joo - young kim , md , phd jooyoungcasa@ncc.re.kr proton therapy center , national cancer center , 323 ilsan - ro , ilsandong - gu , goyang - si , gyeonggi - do , 410769 goyang , republic of korea 2 center for uterine cancer , national cancer center , 323 ilsan - ro , ilsandong - gu , goyang - si , gyeonggi - do , 410769 goyang , republic of korea 3 department of radiation oncology , asan medical center , university of ulsan college of medicine , seoul , republic of korea 4 research center , dongnam inst . 
of radiology and medical sciences , busan , republic of korea zusammenfassung hintergrund ziel der arbeit war es , prognostische faktoren nach magnetresonanztomographisch ( mrt - ) gesteuerter brachytherapie in verbindung mit externer strahlentherapie fr gebrmutterhalskrebs zu identizieren . material und methoden externe strahlentherapie von 4550 , 4 gy erfolgte entweder mittels dreidimensionaler konformaler strahlentherapie oder helikaler tomotherapie . 
die patientinnen erhielten auch eine mrt - gesteuerte hochdosisbrachytherapie von 5 gy in 6 fraktionen . ergebnisse es wurden die flle von 128 patientinnen mit gebrmutterhalskrebs im stadium ibivb gem der strahlenther onkol ( 2016 ) 192 : 922930 internationalen fderation fr gynkologie und geburtshilfe ( figo ) ausgewertet , bei denen eine mrt - gesteuerte brachytherapie durchgefhrt wurde . 
negative beckenlymphknoten , eine dosis von > 110 gy fr die makroskopisch sichtbare tumormasse ( gtv ) , die 90 % der zielstruktur erreicht ( gtv d90 ) , und eine behandlungsdauer ( cid : 2 ) 56 tage gingen in univariaten analysen mit besserem gesamtberleben einher . 
die multivariable analyse zeigte , dass eine gtv d90 von > 110 gy und eine behandlungsdauer ( cid : 2 ) 56 tage mit beinahe signikanten p - werten von 0 , 062 bzw . 0 , 073 mglicherweise mit dem gesamtberleben assoziiert waren . schlussfolgerungen die ergebnisse der mrt - gesteuerten brachytherapie in kombination mit externer strahlentherapie bei patientinnen mit gebrmutterhalskrebs waren hervorragend . 
eine gtv d90 von > 110 gy und eine behandlungsdauer ( cid : 2 ) 56 tage waren potenziell mit dem gesamtberleben assoziiert . schlsselwrter konformale strahlentherapie helikale tomotherapie gynkologie lymphknoten chemotherapie introduction it was previously demonstrated that magnetic resonance image ( mri ) - guided brachytherapy achieved better local control and was better tolerated than conventional brachytherapy [ 1 ]  . 
 [ 10 ] showed that the delivered dose was associated with signicant differences in local control , the prognostic factors for survival after mri - guided brachytherapy for cervical cancer have not been fully evaluated . 
therefore , the present study was designed to evaluate the impact of traditional prognostic factors in addition to dosevolume histogram ( dvh ) parameters on survival after mri - guided brachytherapy in patients with cervical cancer . methods and materials patients and treatment between february 2008 and july 2013 , 161 consecutive patients received high - dose - rate mri - guided brachytherapy with curative intent . 
all of the patients underwent a comprehensive workup , which included their medical history , physical examination , complete blood count , liver and renal function tests , cervical biopsy , human papillomavirus typing and titer , gynecologic mri , and positron emission tomography ( pet ) - computed tomography ( ct )  . 
patients with advanced stage cervical cancer , dened as international federation of gynecology and obstetrics ( figo ) stage exceeding iib , also underwent cystoscopy and sigmoidoscopy . of the 161 patients , 33 were excluded from the present analyses for the following reasons : 14 had distant metastasis at diagnosis or during treatment , 13 had simultaneous double primary lesions , 3 were followed up for less than 3 months , the dvh was not sufcient for analysis in 2 , and 1 received salvage brachytherapy after the planned treatment owing to residual tumor . 
thirty - eight patients with a tumor of > 4 cm in diameter or pelvic ln ( ln ) involvement without denitive pan metastasis had been enrolled in a phase ii trial at our institution and received prophylactic extended eld rt . 
most patients ( 96 % , 123 / 128 ) received 27 cycles ( median 5 cycles ) of concomitant chemotherapy during radiotherapy : 114 received weekly cisplatin , 6 received weekly carboplatin , 2 received cisplatin and etoposide , and 1 received cisplatin and 5 - uorouracil . 
outpatient - based high - dose - rate mriguided brachytherapy with median physical dose of 30 gy ( range , 2040 gy ) in 6 fractions ( range , 48 fractions ) was delivered twice a week using a 192ir remote afterloading system ( microselectron , nucletron , veenendaal , the netherlands )  . 
brachytherapy was started after 39.645.0 gy of ebrt and the remain924 strahlenther onkol ( 2016 ) 192 : 922930 ing ebrt dose was administered on the rest day without overlapping with brachytherapy . mri - guided brachytherapy we could not repeat planning mri at every treatment session because of limited time and resources . 
the position of the applicators was checked by orthogonal uoroscopy at every treatment session . the mri - guided brachytherapy procedures are described in more detail elsewhere [ 11 ]  . 
during the simulation and at each treatment session , the patients were asked to keep a full bladder before brachytherapy to move the intestine from the uterus , and to empty their bowels in the morning of treatment to reduce the rectal dose . 
t2 - weighted axial mris were transferred to the treatment planning system ( plato , version 14.3.5 , nucletron ) and a 3d image set was prepared . delineation of the target structures and organs at risk ( oars ) was performed according to the recommendations of the gynecologic groupe european de curietherapie , european society for therapeutic radiology and oncology working group [ 1215 ]  . 
the gross tumor volume ( gtv ) , high - risk clinical target volume ( hr - ctv ) , intermediaterisk clinical target volume ( ir - ctv ) , and oars ( rectum , sigmoid , and bladder ) were delineated on reconstructed images . 
the irctv also included a safety margin of 510 mm , which was added to the hr - ctv . the ebrt and brachytherapy doses were converted into radiobiologically weighted dose equivalents of 2 gy per fraction ( eqd2 ) and were combined . 
then , patients were followed up every 3 months for the rst 2 years , every 4 months in the next year , and then every 6 months for up to 5 years . 
if the patient had complete remission ( cr ) of the primary tumor and there was no evidence of recurrence at this visit , mri or ct scans were done at 12 months and then annually thereafter . 
if the patient had equivocal mri ndings , mri was performed again 3 month later to conrm the tumor response . cr of the primary tumor was dened as no evidence of residual disease on the clinical or cytologic examinations , and the absence of residual abnormal signals on mri at 3 or 6 months after treatment . 
cancer - specic survival ( css ) and overall survival ( os ) were dened as times from the date of starting rt to the dates of cervical - cancer - related death or any death , respectively . treatment - related rectal toxicity was recorded using the modied radiation therapy oncology group ( rtog ) / european organization for research and treatment of cancer ( eortc ) scoring system [ 17 ] ( supplement 1 , table 5 )  . statistics all statistical analyses were performed using spss software version 20.0 ( spss , chicago , il , usa )  . 
variables that were statistically signicant in the univariate analyses were included in the multivariable model . strahlenther onkol ( 2016 ) 192 : 922930 results patient and treatment characteristics the median follow - up time was 44 months ( range , 6 78 months )  . 
the median gtv and hr - ctv at the time of brachytherapy were 7 cc ( range , 057 cc ) and 27 cc ( range , 796 cc ) , respectively . 
the primary tumor cr rate was also better in patients with sqcc ( 95 % , 100 / 105 ) than in patients with non - sqcc ( 70 % , 16 / 23 ) ( p = 0.014 , 2 test )  . the rrfs , dmfs , dfs , and os rates were signicantly worse in patients with pelvic ln metastases than in patients without these metastases . 
our actuarial 3 - year lrfs , ccs , and os rates were 94 , 90 , and 87 % , which were similar to the rates at these leading centers , even though our study included a large number of patients with advanced disease ; 67 % ( 86 / 128 ) of patients were classied as figo stage iib and 62 % ( 79 / 128 ) had pelvic ln involvement . 
the higher rate of concurrent chemotherapy in our study ( 96 % ) compared with that at medical university of vienna ( 73 % ) and the high - dose ln boost with tomotherapy could explain the better outcomes in our study . 
of 7 patients who had lr , 4 underwent salvage treatment , which comprised re - irradiation in 2 patients and hysterectomy and total pelvic exentration in 1 patient each . 
1 a five year local recur - free survival ( lrfs ) , cancer specic survival ( ccs ) , overall survival ( os ) rates were 94 , 89 , 85 % , respectively . b five year regional recur - free survival ( rrfs ) , distant metastasis - free survival ( dmfs ) , disease - free survival ( dfs ) rates were 92 , 74 , 73 % , respectively strahlenther onkol ( 2016 ) 192 : 922930 ( cid : 2 ) ( cid : 2 ) ( cid : 2 ) ( cid : 2 ) ( cid : 2 ) 928 strahlenther onkol ( 2016 ) 192 : 922930 fig . 
2 patients with a negative pelvic lymph node ( ln ) , b gross tumor volume ( gtv ) dose covering 90 % ( d90 ) of the target ( gtv d90 ) of > 110 gy , and c treatment duration ( cid : 2 ) 56 days showed better overall survival ( os ) 3 patients , 2 were disease - free at the last follow - up and 1 patient experienced distant metastasis at 38 months after the rate of severe rectal toxicities ( grade 3 ) in our study ( 2 % , 3 / 128 ) was similar to the rate reported by the medical university of vienna ( 3 % , 5 / 156 ) [ 1 ]  . 
similar to the medical university of vienna , the rectal toxicity rate was about one - third lower in our study compared with our institutions historical data ( [ 17 ] ; table 4 )  . although it has been almost 20 years since mri - guided brachytherapy was introduced in 1998 at the medical university of vienna , the prognostic factors for survival after this procedure have not extensively evaluated . 
in this study , we found that ln metastasis , large tumor size , lower gtv d90 , and long treatment duration were associated with worse treatment outcomes . consistent with a previous study [ 5 ] , patients with nonsqcc had a lower primary tumor cr rate and worse dfs than patients with sqcc . 
although we could not nd evidence for a doseresponse relationship in the non - sqcc group , dose escalation might be necessary in patients with non - sqcc to improve the primary tumor response . 
these results indicate that it is not simply the bulkiness of the tumor at diagnosis that determines the response to irradiation but that biological factors may underlie the different tumor responses to rt . 
even in patients receiving high - dose mri - guided brachytherapy , we should try to make the treatment duration as short as possible to achieve a better treatment outcome . our mri - guided brachytherapy protocol had several limitations . 
although we tried to deliver the highest possible dose to the target and the lowest possible dose to the oar , we could not apply dose constraints to the target and oars in all cases . 
oelschlager8 smith apisarnthanarax2 jing zeng2 received : 30 march 2016 / accepted : 30 july 2016 / published online : 5 september 2016 springer - verlag berlin heidelberg 2016 abstract purpose the aim of this study is to present the dosimetry , feasibility , and preliminary clinical results of a novel pencil beam scanning ( pbs ) posterior beam technique of proton treatment for esophageal cancer in the setting of trimodality therapy . methods from february 2014 to june 2015 , 13 patients with locally advanced esophageal cancer ( t3 - 4n0 - 2m0 ; 11 adenocarcinoma , 2 squamous cell carcinoma ) were treated with trimodality therapy ( neoadjuvant chemoradiation followed by esophagectomy )  . 
eight patients were treated with uniform scanning ( us ) and 5 patients were treated with a single posterioranterior ( pa ) beam pbs technique with volumetric rescanning for motion mitigation . 
comparison planning with pbs was performed using three plans : ap / pa beam arrangement ; pa plus left posterior oblique ( lpo ) beams , and a single pa beapatient outcomes , including pathologic response and toxicity , were evaluated . results all 13 patients completed chemoradiation to 50.4 gy ( relative biological effectiveness , rbe ) and 12 paelectronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 016 - 1034 - 4 ) contains a supplemental table which is available to authorized users . ( cid : 2 ) jing zeng , md jzeng13@uw.edu 1 department of medical oncology , cancer center , shengjing hospital of china medical university , 39 huaxiang road , 110022 shenyang , china 2 department of radiation oncology , university of washington medical center , 1959 ne pacic street seattle , wa 98195 , usa seattle cancer care alliance proton therapy center , 1570 n 115th st . 
insgesamt 8 patienten wurden mit dem uniform scanning ( us ) sowie 5 patienten mit einer posterior - anterior ( pa ) - pbs - methode mit einzelnem strahl und volumetrischem rescanning zur bewegungsminderung behandelt . 
vergleichsplanung mit pbs wurde unter nutzung dreier plne durchgefhrt : ap / pa - strahlenanordnung , pa plus left - posterior - oblique - ( lpo - ) strahlen und ein einzelner pa - strahl . 
patientenergebnisse , einschlielich pathologischer reaktionen und toxizitt wurden evaluiert . ergebnisse alle 13 patienten schlossen die radiochemotherapie mit 50 , 4 gy ( relative biological effectiveness , rbe ) ab ; 12 patienten unterzogen sich einer operation . alle 12 operierten patienten hatten eine r0 - resektion und 25 % davon eine pathologische komplettremission . 
squamous cell cancers constitute about 95 % of the pathologies seen in developing countries , while adenocarcinomas are becoming more common in the western world , including the usa [ 2 ]  . 
for locally advanced esophageal cancers ( > t1 - 2n0m0 ) , neoadjuvant chemoradiation prior to surgery has been shown to improve survival and is considered a standard of care [ 3 , 4 ]  . 
chemotherapy plus radiation therapy ( rt ) is also a standard treatment approach for localized but unresectable disease [ 5 ]  . proton beam therapy ( pbt ) , with the lack of an exit dose as seen with photon therapy , can decrease the irradiated volumes of heart and lungs compared to photon techniques [ 6 , 7 ]  . 
the delivery of pbt in published studies has employed either a two - eld anteroposterior and posteroanterior ( ap / pa ) beam arrangement , or 23 - eld posterior oblique beams plus or minus a lateral beam [ 8 , 9 ]  . 
however , with the increasing availability of pencil beam scanning ( pbs ) , it may be possible to treat the esophageal tumor to full dose with a single posterior beam approach , while still respecting the dose constraints of surrounding tissues , namely keeping the spinal cord maximum dose to < 45 gy . 
the clinical and pathologic outcome of patients , a dosimetric comparison with other published proton techniques , and the feasibility of this technique are presented . patients and methods patients all patients in this study were enrolled in a prospective registry trial approved by the institutional review board of the authors institution , with written informed consent . 
thirteen patients with carcinoma of the esophagus were treated at the university of washington and seattle cancer care alliance proton therapy center from february 2014 through june 2015 and met the following study eligibility criteria : histologically conrmed diagnosis of adenocarcinoma or squamous cell carcinoma of the esophagus or gastroesophageal junction ( gej ) ; plan for trimodality therapy with neoadjuvant chemoradiation followed by esophagectomy , performance status ( ps ) of 02 ; clinical stage > t2n0m0 according to endoscopic ultrasound ( eus ) for evaluation of tumor ( t ) category , and positron - emission tomography / computed tomography ( pet / ct ) scan for evaluation of nodal and distant disease spread ; an absence of other uncontrolled malignant disease and lack of medical comorbidities that would preclude trimodality therapy . 
the ptv was the target for all treatment plans , as it includes the motion envelope dened by the itv in addition to a generous margthis ptv received 45 gy , with an additional 5.4 - gy boost delivered to the gtv plus 1 - cm margall margins are stated in geometric millimeters . 
the robustness of target and organs at risk ( oar ) doses was evaluated by computing the plan with 3 - % range uncertainty , as well as simulating setup errors by 3 - mm isocenter deviations in the anterior / posterior , superior / inferior , and lateral directions . 
all patients had daily orthogonal x - rays for image guidance prior to treatment . proton therapy was delivered using the proteus plus system ( ion beam applications , louvain - la - neuve , belgium ) with a mix of uniform scanning ( us ) and pbs , as the centers technology evolved over the study period . 
after the center started transitioning to pbs in march 2015 , 5 patients were treated with a single pa beam . in us beam delivery , patient - specic brass apertures were created based on ptv structures with a 0.81.2 - cm margin to account for penumbra . 
wax range compensators were designed with an additional range uncertainty of 2.5 % + 2 mm added to the distal and proximal ranges , as well as 12 - cm smearing margins . 
these were designed using commercially available xio treatment planning software ( impac medical systems , maryland heights , mo , usa )  . dose was veried with an ion chamber measurement performed in water and eld shape was veried by comparing the physical shape of the apertures and compensators with the treatment planning system . for pbs delivery , treatment plans were created using the raystation treatment planning software ( raysearch laboratories ab , stockholm , sweden )  . 
dose and uence were measured pretreatment using the matrixxpt ion chamber array device ( iba dosimetry gmbh , schwarzenbruck , germany ) , which consists of 1020 vented parallel chambers with sensitive volumes of 0.028 cm3 arranged on a 32 32 grid . 
the standard for verication was a gamma pass rate of > 90 % using acceptance criteria of 3 % / 3 mdose distributions delivered using pbs are susceptible to deviations in the event of organ motion ( interplay effects )  . 
toxicity of chemoradiotherapy was monitored using the national cancer institute common terminology criteria for adverse events ( ctcae ) version 4.0. surgery patients underwent repeat pet / ct 24 weeks after completion of chemoradiation for restaging and then esophagectomy 68 weeks after completion of chemoradiotherapy if there was no systemic progression of disease . 
a sample axial images from three comparison plans on the same patient , using three beam arrangements left to right : posterioranterior beams ; an anteriorposterior / posterioranterior beams ; posterioranterior / left posterior oblique beams . 
b sample axial images from original planning ct simulation scan ( top left ) , and 15 gy on - treatment quality assurance resimulation ct scan ( bottom left ) , to ensure consistent target coverage and normal tissue sparing throughout the treatment course , as shown in the dosevolume histogram ( right ) had progressive systemic disease on post - chemoradiation pet / ct . 
for tumors involving the gej , a transhiatal resection was preferred . pathologic response pathologic complete response ( pcr ) was dened as absence of viable carcinoma in the surgical specimen . 
other normal tissue doses were also slightly lower in the pa plan ( including heart , stomach , kidneys , and liver ) , although the differences were not statistically signicant ( table 2 )  . 
maximum cord dose was higher in the pa plan but still within tolerance levels . compared to the pa / lpo plan , the ap / pa plan reduced the lung dose , whereas the heart and liver doses were higher with the ap / pa plan ( table 2 )  . 
cord dose was similar between these two plans . dosimetric comparisons for mid - esophageal tumors for the 2 patients with mid - esophageal tumors , the sample size was too small for statistical comparison ; however , similar differences between the three planning techniques were seen ( supplementary table 1 )  . verication of plan delivery all patients underwent a quality assurance repeat ct simulation scan at 15 and 30 gy , to ensure that target coverage was still adequate and normal tissue constraints were still met . 
r0 resection was achieved gej gastroesophageal junction , ecog eastern cooperative oncology group ap / pa plan versus pa / lpo plan endpoints and statistical analysis the clinical outcome , including pathologic response of tumor , toxicity , r0 resection rate , and disease recurrence is reported . 
dividing patients into two groups based on whether they were treated with us ( 8 patients ) or pbs with a pa beam ( 4 patients ) , the same pcr rate was seen in both groups ( 25 % ) , as well as similar rates of tumor and nodal downstaging . treatment - related toxicities chemoradiation therapy . 
dividing patients into two groups , those treated with us ( 8 patients ) and those treated with a single posterior pencil beam ( 5 patients ) , there were no signicant differences in toxicity between the two groups , as shown in table 5 . 
of patients ( % ) toxicity neutropenia thrombopenia anemia nausea vomiting diarrhea anorexia fatigue alopecia radiation dermatitis radiation pneumonitis esophagitis 1 ( 7.7 ) 4 ( 30.8 ) 3 ( 23.1 ) 1 ( 7.7 ) 1 ( 7.7 ) 3 ( 23.1 ) 5 ( 38.5 ) 3 ( 23.1 ) 1 ( 7.7 ) 1 ( 7.7 ) 1 ( 7.7 ) not been reached . 
at the time of the analyses , 3 patients had recurrent disease ( all distant metastases ) , and one postoperative death had been observed , as detailed above . discussion pbt can increase sparing of normal tissues in the radiation treatment of esophageal cancer compared with photon radiation [ 13 ]  . 
comparison planning between proton and photon therapy shows that when using ap / pa or pa / lpo proton beam arrangements , proton treatment plans deliver less radiation dose to the lungs and heart than photon therapy [ 14 ]  . in the present study , the authors report their experience with pbt in patients with esophageal cancer intended for trimodality therapy , with pathologic response and toxicity data that are comparable to published clinical series [ 4 , 15 , 16 ]  . 
this report also details the rst clinical experience in the treatment of operable esophageal cancers using a single pbs approach ( with volumetric rescanning for motion mitigation ) combined with concurrent chemotherapy , which further decreases radiation dose to the lungs and heart compared to published proton therapy planning methods . 
the pcr rate ( 25 % ) of this study was similar to prior studies [ 4 , 15 , 16 ]  . in the current study , treatment planning was compared between pa ( 1 eld ) , ap / pa ( 2 elds ) , and pa / lpo ( 23 elds ) proton beams for 13 patients using the same image sets . 
the pa technique also delivered a lower dose to the other normal organs compared to the pa / lpo technique ( including heart , stomach , kidneys , and liver ) , although the differences were not statistically signicant . higher radiation dose to the lungs is associated with increased risk of radiation pneumonitis , as shown in both lung and esophageal cancer [ 17 , 18 ]  . 
dosimetric parameters such as mean lung dose ( mld ) and percentage volume of lung receiving 20 gy ( v20 ) are often used to evaluate radiation treatment plans and the risk for pneumonitis . 
in the current study , mld and v20 were lowest with pa plans , although the difference between the pa and ap / pa lung doses were not statistically signicant . 
besides lung dose , clinical studies have indicated that minimizing the heart volume receiving radiation can signicantly reduce the risk of potentially life - threatening complications [ 19 ]  . 
consequently , with pbs technology , a single pa beam may produce radiation treatment plans that have the lowest risk for toxicity in patients . with pbs there is potential concern regarding treating intrathoracic and upper abdominal cancers , such as lung and distal esophageal tumors , which have targets that may move with respiration . 
of patients ( % ) complications pulmonary complicationsa cardiac complicationsb anastomotic leakage chylothorax conduit necrosis in - hospital mortalityc 4 ( 33.3 ) 2 ( 16.7 ) 1 ( 8.3 ) 1 ( 8.3 ) apulmonary complications were 4 cases of pneumonia . bcardiac complications were 2 cases of arrhythmia requiring treatment . cthe patient was > 75 years old , with a history of diabetes , hypertension , hyperlipidemia , prostate cancer , and > 40 pack - year smoking history . 
the current results to do not show a difference in pcr or downstaging with pbs compared to other published photon series , which suggests the pbs radiation treatment is on target and similar in antitumor efcacy as photon radiation . 
1 , the single pa beam plan was robust and target doses were not compromised using one posterior pencil beam , as veried by multiple quality assurance ct scans during treatment ( at 15 and 30 gy )  . this study did not perform a dosimetric comparison between proton and photon therapy . 
other published dosimetry studies on photon therapy have typically described a mean heart dose of around 22 gy ( compared to 14 gy in this study ) , an mld of around 15 gy ( 4.96 gy in this study ) , and a v20 of around 30 % ( 10 % in this study ) [ 22 ]  . most patients in the current study had distal esophageal adenocarcinoma , which is consistent with the patient population expected in the usa . 
for other countries with different patient demographics , such as a higher rate of upper / mid - thoracic squamous cell carcinomas , the pa technique might not be as feasible , particularly when treatment of supraclavicular nodes is required . 
this limits the statistical power of comparisons , and it is possible that there are clinical differences between the different beam arrangements and technologies that are not detectable with this sample size . 
zeng state that there are no conicts of interest . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
this study aimed to investigate such factors and assess the role of the vaginal dilator ( vd )  . methods qol was assessed in 112 ec patients 6 years ( median ) after rt . 
vaginal brachytherapy only and intensity - modulated rt ( imrt ) were associated with better global health status and reduced chronic gastrointestinal ( gi ) symptoms . higher acute gi toxicity was associated with increased chronic gi symptoms , particularly diarrhea , and reduced role functioning . 
higher acute urinary toxicity was associated with increased chronic urological symptoms , muscular / pelvic pain , and chronic gi symptoms , as well as with reduced emotional / social functioning and reduced global health status . 
subjective vaginal shortening / tightness was not reduced in vd users . conclusion rt technique and acute toxicities are prognostic for the extent of chronic symptoms and long - term qol . sexuality is important even at a higher age . 
few patients use the vd and a reduction of subjective vaginal shortening / tightness was not achieved . keywords toxicity diarrhea dyspareunia sexual dysfunction sexual intercourse prognostische faktoren fr die langfristige lebensqualitt nach adjuvanter radiotherapie von frauen mit endometriumkarzinom zusammenfassung hintergrund eine adjuvante radiotherapie ( rt ) kann die lebensqualitt von patientinnen mit endometriumkarzinom ( ec ) beeinussen . 
ziel war es , diese faktoren und die rolle des vaginaldilators ( vd ) zu untersuchen . methoden zur qol wurden 112 ec - patientinnen 6 jahre ( median ) nach rt befragt . 
wenige patientinnen nutzen den vd und die subjektiv empfundene vaginale verkrzung / enge nahm nicht schlsselwrter toxizitt diarrhoe dyspareunie sexuelle dysfunktion geschlechtsverkehr endometrial cancer ( ec ) is the most frequent gynecologic malignancy and radiotherapy ( rt ) remains an important treatment pillar by ensuring excellent local control . 
in recent years , efforts have been made to tailor adjuvant rt to patients individual risk constellation [ 14 ] , because pelvic rt may cause substantial gastrointestinal ( gi ) and genitourinary ( gu ) morbidity [ 5 , 6 ]  . 
sexual symptoms have been described to be more frequent after rt than in the normal population [ 9 ] and sexual dysfunction may be greater than 80 % after treatment for ec [ 10 ] ; however , it has also been shown that sexual dysfunction is similar in patients who only underwent surgery and those who received adjuvant rt [ 8 , 11 ]  . 
whether vaginal dilation exercises are capable of preventing vaginal stenosis is currently unclear [ 12 , 13 ]  . therefore , this study was designed to compare long - term qol in patients treated at the authors institution to published normative data and to analyze possible prognostic factors for long - term qol . 
furthermore , the study aimed to assess which patients used the vaginal dilator ( vd ) and whether its use had any inuence on subjectively perceived vaginal stenosis . methods between 2004 and 2012 , 293 women were treated with adjuvant rt for ec at the authors department . 
no reference values were available from a german population for the sexual items in the qlq - en24 questionnaire , thus the results were compared with reported scores from a dutch reference population [ 15 ]  . 
it was then analyzed whether the different scores from the qlq - c30 strahlenther onkol ( 2016 ) 192 : 895904 and qlq - en24 questionnaires were inuenced by age , initial tumor stage , histology , lymphadenectomy , modality of rt , and observed acute toxicities . 
all statistical analyses were performed with sas version 9 ( sas institute , cary , nc , usa )  . results a median of 6 years had passed between adjuvant rt for ec and the current survey . 
women with a higher degree of acute gi and / or urinary toxicities during and ( cid : 2 ) 6 weeks after rt reported more chronic symptoms and a reduced qol ( table 4 )  . 
patients with higher sexual activity ( p < 0.001 ) and sexual interest ( p < 0.001 ) were more likely to use the vd for more than 1 year ( table 4 )  . 
acute vaginal toxicity ( p = 0.030 ) as well as persistent pain in the back and pelvis ( p = 0.005 ) or muscular pain ( p = 0.013 ) were associated with not using the vd ( table 4 )  . 
relevant vaginal shortening or tightness ( quite a bit and very much ) was subjectively experienced by 64.7 % ( n = 22 ) of the patients who answered this question ( n = 34 ; 30.4 % ) and there was no statistically signicant difference in perceived vaginal shortening or tightness between vd users and non - users ( table 4 )  . discussion this study was conducted to compare long - term qol in ec patients treated with adjuvant rt to normative data , as well as to analyze possible prognostic factors for long - term qol . 
furthermore , it was assessed which patients used the vd and whether vd use had any inuence on subjectively perceived vaginal stenosis . patients were surveyed at a median of 6 years after rt . only the postoperative radiation therapy in endometrial carcinoma ( portec ) trials can report longer follow - up periods [ 7 , 8 ]  . 
age is a known factor inuencing qol [ 16 ] and elderly patients reported reduced physical functioning ( p < 0.001 ) , more dyspnea ( p = 0.007 ) , and a poorer body image ( p = 0.005 ) in the present study . 
the authors believe this to have partially compensated for the absence of multivariate analyses in their study , which were not possible due to the small sample size . values of functioning and symptoms items were generally found to be worse in the present patients when compared to an age - matched normal population , whereas patients from the portec - 2 study reported functioning scores similar to normative data 5 years after treatment [ 9 ]  . 
a large population - based study from the united states found health - related qol in survivors of cervical cancer to be worse than in the normal population [ 17 ]  . 
particularly urinary urgency , urinary incontinence , diarrhea , and fecal leakage were the prevailing symptoms negatively effectivb was substantially better for ing patients qol [ 8 ]  . patients qol and associated with signicantly less bowel and urinary symptoms in long - term follow - up [ 7 ]  . 
another randomized trial comparing ebrt / ivb to sole ivb in intermediate - risk ec found a lower global health status at the end of rt in women who underwent combined treatment , but the difference disappeared 612 months after rt [ 18 ]  . in the current analysis , women treated with ivb alone had a better global health status ( p = 0.049 ) compared to those treated with combined ebrt / ivb . 
this may be explained by the fact that the authors of the current study mostly conducted combined rt in patients with more advanced disease , while sole ivb was reserved for women tting the portec - 2 criteria . in agreement with previous investigators , gi symptoms , particularly diarrhea , were found to persist for years after rt [ 8 , 9 ]  . importantly , the current study found that the observed acute toxicities were relevant for patients longterm qol . 
apart from the dosevolume relationship , which is found for both acute and late effects , chronic gi toxicities have been described to be consequential to acute damage , and amelioration of the acute response to irradiation may be a useful approach to minimizing late side effects [ 20 ]  . 
correspondingly , patients who received imrt reported fewer chronic gi symptoms ( p = 0.028 ) and had a better global health status ( p = 0.017 ) in the present study . imrt has been shown to produce less acute [ 21 ] and chronic gi toxicities [ 22 ]  . 
a recent retrospective series published reported urinary bladder v40 ( volume of by pisani et al . bladder receiving 40 gy ) and mean dose to the vagina to be signicantly associated with global health status , urinary urgency , urinary incontinence , and dyspareunia [ 23 ]  . 
in the current study , patients with higher acute urinary toxicity also reported more chronic urological symptoms ( p = 0.011 ) as well as more chronic gi symptoms ( p < 0.001 ) with diarrhea ( p = 0.003 ) ; furthermore , they complained more 902 strahlenther onkol ( 2016 ) 192 : 895904 higher degree of acute vaginal toxicity ( p = 0.030 ) , persistent pain in the back and pelvis ( p = 0.005 ) , or muscular pain ( p = 0.013 ) were identied as factors preventing patients from using the prescribed vd , irrespective of age , in the current cohort . it was not possible to detect any statistically signicant difference in subjectively perceived vaginal shortening or tightness between patients using the vd and those who did not , although the relatively small number of patients answering this question has to be acknowledged . 
these results are questionable because the investigators compared vd sizes 4 weeks after rt , when patients still exhibit acute vaginal mucositis , with vd sizes 12 months after rt . 
another prospective study from the same institution in patients with rectal and anal cancer [ 30 ] suggested that a greater adherence to vd use was associated with reduced stenosis , but only 10 patients actually presented with vaginal stenosis 12 months after rt , making it very difcult to assess the inuence of compliance with vd use on the development of vaginal stenosis . these authors also demonstrated a decrease in mean vd size 4 weeks after rt , with a continuous increase to prert size after 12 months . in the authors opinion , acute vaginal toxicity at 4 weeks after rt is more likely to be the reason for the decrease in vd size than actual brosis of the vagina . 
dosimetric parameters for the development of vaginal stenosis have been suggested in ec patients [ 13 ] as well as in patients with rectal or anal cancer [ 30 ] , and the authors believe that this also deserves further investigation . 
on the contrary , it was found that acute urinary toxicity is a major issue for various aspects of long - term qol . despite vaginal dryness ( p < 0.0001 ) , pain during intercourse ( p < 0.0001 ) , and reduced sexual enjoyment ( p < 0.0001 ) , patients in this study reported increased sexual activity ( p < 0.0001 ) and sexual interest ( p < 0.0001 ) compared to the reference population . 
these results have to be interpreted with caution , since only one third of the patients who answered the questions on sexual activity and sexual interest also reported on sexual enjoyment , vaginal dryness , and dyspareunia . 
vaginal dryness and reduced sexual enjoyment are known complications of rt and occur after ivb as well as after ebrt [ 9 , 25 ] , although increased sexual interest and activity have not been reported in survivors of ec so far . 
although the current authors do not believe the results to be biased , since almost all patients answered these questions , it must be stated that the study is limited by the fact that only 40 % of the survivors ( 112 out of 280 ) were eligible for inclusion . 
on the one hand , sexual functioning has been reported to be lower after rt [ 9 , 10 , 23 ] and sexual activity decreases in survivors of gynecologic malignancies [ 26 , 27 ] ; on the other hand , sexual functioning did not differ between patients who had only undergone surgery and those who were treated with adjuvant rt in various clinical trials [ 28 ]  . 
nevertheless , the current results underline the importance of sexuality and sexual functioning for elderly patients , and the authors believe that these qualities should be evaluated in future randomized clinical trials . mainly younger patients used the vd and only women with increased sexual activity ( p = 0.013 ) or interest ( p = 0.002 ) used the vd for longer than 1 year . 
furthermore , a strahlenther onkol ( 2016 ) 192 : 895904 conclusion rt technique and acute toxicities are prognostic for the extent of chronic symptoms and long - term qol . 
lindel state that they have no competing interests . this study was approved by the heidelberg ethics committee ( # s481 / 2014 ) and was conducted in accordance with the helsinki declaration of 1975 in its most recently amended version . 
zu dieser frage erschien originalpublikation stish bj , pisansky tm , harmsen ws et al ( 2016 ) improved metastasis - free and survival outcomes with early salvage radiotherapy in men with detectable prostate - specic antigen after prostatectomy for prostate cancer . 
es handelt sich um eine retrospektive aufarbeitung der daten von 1106 patienten der mayo clinic , die in den jahren 1987 bis 2013 eine salvagert der prostataloge wegen eines psa - rezidivs nach prostatektomie ( pe ) erhalten hatten . 
es ist nicht sinnvoll , weiter abzuwarten . strahlenther onkol ( 2016 ) 192 : 954955 kommentar fazit die indikation zur strahlentherapie der prostataloge bei vorliegen eines psa - rezidivs nach pe ist unstrittig . 
also bleibt nur der psa - wert bei beginn der salvage - rt als relevanter faktor , der vom arzt und patienten in dieser situation beeinusst werden kann . in metaanalysen ndet sich eine klare beziehung zwischen dem prradiotherapeutischem psa - wert und dem ansprechen auf die rt ab einem psa - wert von 0 , 5 ng / ml . fr niedrigere psa - werte ist dieser zusammenhang nicht belegt , vor allem wegen der sehr kleinen patientenzahlen in solchen gruppen [ 4 ]  . 
fr uns stellt sich somit die frage , ob der in leitlinien angegebene grenzwert von 0 , 5 ng / ml fr die indikation zur rt weiterhin gehalten werden darf . 
erste hinweise , dass auch bei psa - werten unter 0 , 5 ng / ml eine korrelation zum ansprechen besteht , gibt es seit kurzer zeit ; sie beziehen sich aber lediglich auf den endpunkt biochemische rezidivfreiheit . die jetzt publizierte arbeit ist die grte monozentrische analyse , die den vorteil einer sehr frhen salvage - rt hinsichtlich der biochemischen rezidivfreiheit , fernmetastasenfreiheit , des krankheitsspezischen berlebens und in der multivariaten analyse auch hinsichtlich des gesamtberlebens zeigt . 
sie enthlt viele patienten mit niedrigen psa - werten und zeichnet sich durch eine lange nachbeobachtungszeit aus . ergnzend muss man betonen , dass neuerdings mit dem psma - pet - ct zustzlich ein sehr sensitives verfahren fr die frhe rezidivdiagnostik zur verfgung steht [ 9 ]  . 
nach unserer einschtzung sollte man diese untersuchung bei psa - werten oberhalb von 0 , 5 ng / ml durchfhren , um die indikationsstellung und das bestrahlungsvolumen przisieren zu knnen . gerade die sehr frhe salvage - rt scheint besonders wirksam zu sein ; sie sollte also mglichst frh nach der diagnose eines psa - rezidivs ( nach phoenix - denition zweimaliger psa - anstieg ber nadir ) beginnen . 
ab einem psawert von 0 , 5 ng / ml empfehlen wir das psma - pet , um den lokalbefund besser beurteilen zu knnen . ren baumann und jrgen dunst , kiel interessenkonikt r . 
cotter se , chen mh , moul jw et al ( 2011 ) salvage radiation in men after prostate - specic antigen failure and the risk of death . cancer 117 : 39253932 3 . 
fossati n , karnes rj , cozzarini c et al ( 2016 ) assessing the optimal timing for early salvage radiation therapy in patients with prostate - specic antigen rise after radical prostatectomy . 
ohri n , dicker ap , trabulsi ej et al ( 2012 ) can early implementation of salvage radiotherapy for prostate cancer improve the therapeutic ratio ? a systematic review and regression meta - analysis with radiobiological modelling . 
leitlinienprogramm onkologie ( deutsche krebsgesellschaft , deutsche krebshilfe , awmf ) : interdisziplinre leitlinie der qualitt s3 zur frherkennung , diagnose und therapie der verschiedenen stadien des prostatakarzinoms , langversion 3.1 , 2014 awmf registernummer : 034 / 022ol . 
sterzing f , kratochwils c , fiedler h et al ( 2016 ) 68 ga - psma11 pet / ct : a new technique with high potential for the radiotherapeutic management of prostate cancer patients . 
stish bj , pisansky tm , harmsen ws et al ( 2016 ) improved metastasis - free and survival outcomes with early salvage radiotherapy in men with detectable prostate - specic antigen after prostatectomy for prostate cancer . 
trock bj , han m , freedland sj et al ( 2008 ) prostate cancer - specic survival following salvage radiotherapy vs observation in men with biochemical recurrence after radical prostatectomy . 
because of its challenging anatomical position , surgery alone hardly results in complete resection of the localized amyloidosis . therefore , an interdisciplinary planning board to design optimal treatment is of particular importance . patient and methods a 39 - year - old man presented with a several - week history of nasal obstruction and epistaxis . computed tomography ( ct ) and magnetic resonance imaging ( mri ) revealed the presence of a retro - odontoid nonenhancing soft tissue mass . results the endoscopic biopsy demonstrated that the mass was amyloid in nature . 
the patient was treated with a combination of surgery and radiotherapy , showing no evidence of recurrence or progression at his 1 - year followming luo and gang peng contributed equally to this work and should be considered co - rst authors ( cid : 2 ) jing cheng , m.d. 
to the best of our knowledge , this is the rst report of a nasopharyngeal amyloidosis case treated with excision and radiation leading to complete remission . because of the difculty for surgeons to achieve radical resection with such lesions , radiotherapy proved to be an excellent adjuvant treatment in this case . keywords cytoreduction surgical procedures primary amyloidosis nasopharynx surgery diagnostic imaging intensittsmodulierte strahlentherapie bei lokalisierter nasopharyngealer amyloidose kasuistik und review der literatur zusammenfassung hintergrund die primre lokalisierte amyloidose ist durch die ablagerung von amyloidproteinen gekennzeichnet , die sich auf ein organ beschrnkt , also nicht systemisch ist . eine primre amyloidose im nasen - rachen - raum ist auerordentlich selten , bisher gibt es keine standardtherapie . ihre anatomische position bedeutet eine herausforderung , nur selten resultiert eine chirurgische intervention in einer vollstndigen resektion der lokalisierten amyloidose . daher ist die beteiligung mehrerer disziplinen fr eine optimale behandlung von besonderer bedeutung . patient und methoden bei einem 39 - jhrigen patienten mit seit einigen wochen bestehenden symptomen nasaler obstruktion und nasenbluten zeigten computer ( ct ) und magnetresonanztomographie ( mrt ) einen hinter dem dens liegenden weichteiltumor ohne enhancement . ergebnisse die endoskopisch gewonnene biopsie zeigte , dass es sich bei dem tumor um eine amyloidose handelte . 
eine umfassende diagnostik ergab keine entzndlistrahlenther onkol ( 2016 ) 192 : 944950 and vigilant to this rare disease development , and favor the joint involvement of multiple departments for treatments . here , we describe a rare case of nasopharyngeal amyloidosis treated with partial excision and intensity - modulated radiotherapy ( imrt ) , resulting in good patient tolerance and satisfactory therapeutic effects . case report a 39 - year - old man with no signicant past medical history or evidence of immunosuppression presented with a complaint of right side nasal obstruction and epistaxis over several weeks . 
magnetic resonance imaging ( mri ) revealed a 40 25 18 mm t1 - weighted hypointense to mildly hyperintense contrast - enhancing mass involving the right nasopharynx and obstructing the eustachian tube opening . 
a biopsy of the mass was taken , and pathological evaluation demonstrated the presence of abnormal deposits that were positively stained by congo red , thereby conrming the nasopharyngeal amyloidosis diagnosis . 
no m protein was detected in the serum and urine by protein electrophoresis . the human immunodeciency virus status was negative . no intraor extra - osseous lesions were identied on full skeletal x - ray examination or mri scans . 
a bone marrow biopsy showed a normocellular marrow with trilineage hematopoiesis and no increase in the number of plasma cells . results the decision was made to proceed with an operative intervention to debulk the pharyngeal tumor and obtain tissue for pathological examination and diagnosis . 
1 congo red - stained section of the amyloid mass showing the presence of amyloidosis aggregates partly surrounding small cells ( original magnication : 400 ) chen prozesse , keine systematische amyloidose und keine plasmazell - dyskrasie . 
wegen der schwierig zu erreichenden radikalen resektion bei lsionen in diesem bereich hat sich die strahlentherapie fr den vorgestellten patienten als ausgezeichnete adjuvante behandlungsoption erwiesen . schlsselwrter zytoreduktive chirurgische verfahren primre amyloidose nasopharynx chirurgie diagnostische bildgebung amyloidosis is a heterogeneous group of diseases , characterized by the deposition of insoluble proteins in the extracellular space . 
amyloidosis can arise in many organs , such as bone , skin , larynx , lymph nodes , tongue , eyes , and the gastrointestinal tract [ 3 ]  . 
the histopathological detection of the typical apple - green birefringence of the amyloid deposits on congo red - stained histological samples is still the gold standard for the diagnosis of amyloidosis . in addition , specic laboratory tests and systemic workup should be routinely performed to rule out any systemic involvement . 
2 mri images showing the evolution of the well - demarcated mass in the right nasopharynx a before and b after radiotherapy , c 3 months after radiotherapy , and d the disappearance of the mass 9 months after radiotherapy strahlenther onkol ( 2016 ) 192 : 944950 results , a diagnosis of primary nasopharyngeal amyloidosis was established . postoperative imrt was performed to further control the residual disease . 
the gtv covered the gross residual disease in the pharyngeal recess and the ctv - 60 covered the gtv with an additional 510 mm margin ( where possible )  . 
considering the restricted local aggressiveness and the benign characteristics of this mass , we did not cover the same high - risk local structures and lymphatic regions as for nasopharyngeal carcinoma treatment . 
a 3 - mm margin was added to each of the target volumes to produce three planning target volumes ( ptvs )  . the gtv was subjected to 70 gy in 25 fractions spread over a 5 - week period , using a photon beam energy of 6 mv with 7 isocentric gantry angles . 
familial amyloidosis , accounting for less than 2 % of the cases , can be caused by the accumulation of abnormal proteins bearing an inherited detrimental mutation , most of which are found in transthyretin ( ttr ; most common form ) , apolipoprotein ai , brinogen , cystatin , or gelsolin [ 6 ]  . 
the gastrointestinal system is another common site of amyloid deposition in patients with al ( 70 % ) and aa ( 50 % ) [ 8 ]  . however , the only single organ or localized form of amyloidosis occurring without systemic involvement is comparatively rare , and mostly found in the head and neck region . 
among the preferred localized amyloidosis sites , the larynx is the most frequently affected ( 61 % ) , followed by the oropharynx ( 23 % ) , trachea ( 9 % ) , and orbit ( 4 % )  . only 3 % of the cases occur in the nasopharyngeal region [ 911 ]  . 
once amyloidosis is diagnosed , a proper medical work - up is required to rule out any systemic involvement . 948 strahlenther onkol ( 2016 ) 192 : 944950 unfortunately , no standard therapeutic plan currently exists for amyloidosis because of the limited number of cases . chemotherapy using a melphalan plus prednisone combination is commonly used in systemic amyloidosis but has an efcacy level of 4060 % [ 13 ]  . 
unlike systemic amyloidosis , a primary solitary amyloidosis diagnosis usually implicates a better prognosis , although long - term follow - up data are unavailable for the majority of the cases reported in the literature . 
recurrence in up to 22 % was reported for patients undergoing monotherapy with either radiation or surgery , while the combination of both provided a superior local control of the disease over either modality administered alone [ 14 ]  . 
lesserson and finn [ 16 ] reported that their attempt at removing a nasopharyngeal amyloid tumor surgically resulted in a bilateral amyloid recurrence on the palate , and particularly on the palate pressure areas . 
however , follow - up details were omitted in many instances [ 1722 ] , while other reports described ill patients dying soon after surgery [ 19 , 2325 ]  . after partial resection , the mass regrew much faster than before , showing a more aggressive appearance and symptoms , which potentially indicated the onset of a malignant transformation process after the surgery . in addition , radiotherapy has been used effectively either as an adjuvant or primary treatment modality . 
indeed , thibault and vallires [ 28 ] reported treatment failure in the case of a patient with amyloidosis of the tongue who received a low dose of 20 gy in 10 fractions , attributing the failure to the insufcient dose . 
in their review of 185 cases of extramedullary plasmacytoma treated with radiation therapy , the doses < 40 gy resulted in a local failure rate of 37 % compared to only 11 % with doses 40 gy . 
in choosing a radiation dose , it is important to consider numerous factors , including the potential evolution to systemic amyloidosis , the previous treatments received , the presence of comorbidities , and the patients preferences and overall physical status . 
it is also essential to analyze the available doseresponse relationships regarding both efcacy and safety . in our case , the recurrent amyloidosis was growing faster than before the surgery , suggesting a potential risk of ongoing malignant transformation . 
in addition , should this patient have needed an additional surgery or supplementary radiotherapy in the near future , the high risk of hemorrhage would have represented another serious complication threatening the patient . in addition , considering the age and strong survival desire of this patient , we chose to administer a high dose of radiation by imrt . 
because imrt has better dose - distribution properties , it is possible to increase the dose toward a dened target volume while reducing the dose delivered to the surrounding healthy organs , preserving their function and subsequently improving quality of life [ 33 ]  . based on our experience with approximately four hundred nasopharyngeal cancer patients , the irradiated eld covers a larger region than the sole amyloid mass . 
nevertheless , the extent of early and long - term complications remained lower than in the control group receiving the same radiotherapy using the traditional method [ 34 ]  . 
longer follow - up and more studies strahlenther onkol ( 2016 ) 192 : 944950 may be helpful in determining the ideal dosing , identifying the best way of monitoring the response , and determining for how long the observed benets are to be sustained . in this case , the amyloidosis regressed gradually , eventually disappearing completely 9 months after the radiotherapy . 
indeed , low radiation doses , such as those typically used in anti - inammatory radiotherapy , resulted in a signicant inhibition of the no pathway in macrophages , while an overstimulation was observed at higher radiation doses . 
however , in stimulated macrophages , the metabolic activity , proliferation , and reproductive integrity were not affected by radiation doses up to 10 gy because activated macrophages were shown to be irreversibly post - mitotic [ 35 ]  . 
in another study , the authors found that the number of adherent leukocytes was signicantly reduced at 5 , 24 , and 48 h , but not at 72 h , after irradiation in lps - challenged mice . 
the evidence - based anti - inammatory effect of radiotherapy on benign diseases appears to be due to the specic modulation of different inammatory response pathways , such as the no pathway in stimulated macrophages [ 36 ]  . 
another proposed theory is that the radiotherapy affects plasma cells locally , which has been shown in patients with multiple myeloma and plasmacytomas [ 3739 ]  . it was postulated that amyloidosis results from light - chain immunoglobulin deposition by local plasma cells . 
nevertheless , it is strongly suggested that radiotherapy maybe a unique and an effective treatment . conclusion we report an extremely rare case of localized nasopharyngeal amyloidosis in a 39 - year - old man . 
because relatively few nasopharyngeal amyloidosis patients exist and because of the multitude of factors to consider , it would be difcult to perform a randomized controlled trial in this setting . 
oktober 2016 springer - verlag berlin heidelberg 2016 originalarbeit bujko k , wyrwicz l , rutkowski a et al ( 2016 ) long - course oxaliplatin - based preoperative chemoradiation versus 5 5 gy and consolidation chemotherapy for ct4 or xed ct3 rectal cancer : results of a randomized phase iii study . 
die prospektive , randomisierte phase - iii - studie rekrutierte von 2008 bis 2014 an 39 polnischen zentren 515 patienten mit ct4oder palpatorisch xiertem ct3 - rektumkarzinom , who - performance status 12 . 
die patienten wurden randomisiert in arm a ( scrt mit 5 5 gy , gefolgt von 3 zyklen folfox4 , beginnend eine woche nach abschluss der radiotherapie ) oder arm b ( lcrct mit 50 , 4 gy in 28 fraktionen )  . 
primrer endpunkt der intention - to - treat - analyse war die r0 - resektionsrate mit der annahme , dass diese im experimentellen arm a von 75 % auf 85 % verbessert werden knnte . 
ber die hlfte der tumoren lag im unteren rektumdrittel , ber 60 % zeigten ein t4 - stadiudie akuttoxizitt war in arm a signikant geringer ( p = 0 , 001 ) , dies betraf jedoch vor allem niedriggradige nebenwirkungen . 
im arm a entwickelten immerhin 17 % der patienten nach abschluss der scrt eine grad - 3 / 4 - diarrhoe . der primre endpunkt wurde nicht erreicht : die r0 - resektionsrate betrug 77 % vs . 
65 % im experimentellen arm a signikant besser ( p = 0 , 047 ; hazard ratio 0 , 73 )  . 952 strahlenther onkol ( 2016 ) 192 : 951953 schlussfolgerung der autoren . 
die scrt mit nachfolgender folfox - chemotherapie ist eine effektive behandlungsoption fr patienten mit lokal fortgeschrittenem rektumkarzinom , insbesondere in lndern mit begrenzten ressourcen und eingeschrnkten strahlentherapeutischen behandlungskapazitten . kommentar es existieren zwei abgeschlossene phase - iii - studien , die die scrt und die normofraktionierte lcrct im neoadjuvanten setting randomisiert vergleichen [ 1 , 2 ]  . 
in der deutschen s3 - leitlinie wird daher , wenn ein downsizing angestrebt wird ( bei tiefsitzenden tumoren oder bildmorphologisch positivem zirkumferentiellem resektionsrand ) , der lcrct der vorzug gegeben . unter anderem aus der stockholm - iii - studie ist aber durchaus bekannt , dass auch scrt eine pcr - rate von 11 , 8 % verglichen mit 1 , 7 % erzielen kann , wenn anschlieend an die scrt nicht sofort operiert , sondern das intervall auf 48 wochen bis zur operation verlngert wird [ 3 ]  . die rolle der systemtherapie beim rektumkarzinom wird hug diskutiert . 
aufgrund der verbesserten lokalen kontrolle durch den konsequenten einsatz der neoadjuvanten radio ( chemo ) therapie und der tme - chirurgie ( totale mesorektale exzision ) ist das systemische rezidivrisiko zunehmend in den vordergrund gerckt . 
die datenlage zur adjuvanten chemotherapie ist jedoch bedeutend schwcher als beim kolonkarzinoeine metaanalyse der randomisierten studien mit fluorouracil - basierter chemotherapie konnten keine signikante verbesserung der onkologischen endpunkte erreichen [ 4 ]  . 
auch eine intensivierung der lcrct durch die hinzunahme von oxaliplatin konnte allein in der cao / aro / aio - 04 - studie die pcr - rate und das krankheitsfreie berleben verbessern [ 5 ]  . 
die pcr - rate betrug 25 % , das krankheitsfreie und gesamtberleben nach 4 jahren jeweils 92 % . in der chinesischen forwarc - phase - iii - studie lag die pcr - rate nach 46 zyklen folfox bei 6 , 6 % verglichen mit 14 % nach einer 5 - fu - basierten lcrct und 27 , 5 % nach einer lcrct mit folfox [ 7 ]  . 
garcia - aguilar et al . wiederum ergnzten eine lcrct um eine properative erhaltungschemotherapie nach dem folfox6 - regime [ 8 ]  . in dieser nichtrandomisierten , 4 - armigen phase - ii - studie stieg die pcr - rate nach 2 , 4 , bzw . 
nachgeschaltete neoadjuvante chemotherapie nach dem folfox - regime ergnzt . folgende kritikpunkte an der hier kommentierten polnischen studie sollten erwhnt werden : der wchentliche zustzliche einsatz von oxaliplatin in der gewhlten dosierung im lcrct - arm hat in den drei o . 
allein die cao / aro / aio - 04 - studie ergab eine verbesserung der pcr - rate und des krankheitsfreien berlebens , mglicherweise wegen der hohen qualitt der patientenbegleitung whrend der therapiephase und in der nachsorge oder weil die chemotherapie - compliance durch die oxaliplatin - pause in woche 3 deutlich besser als in den anderen studien war . 
darber hinaus erhielten mehr patienten in arm a oxaliplatin . die studie schloss gegenber einem nichtselektionierten patientengut eine ungewhnlich hohe zahl an patienten mit t4 - tumoren edas spiegelt sich in der nicht zu akzeptierbaren hohen rate an r1 / r2 - resektionen bzw . 
wurden die 16 patienten , die mit lokal rezidivierten tumoren in die studie rekrutiert worden waren , von der analyse ausgeschlosstrahlenther onkol ( 2016 ) 192 : 951953 sen , so verschwand die signikanz des unterschieds im gesamtberleben ( p = 0 , 078 )  . fazit die scrt , gefolgt von einer folfox - chemotherapie ist kein standardschema . 
bei patienten mit oligometastasierter tumorerkrankung interessant sein , wenn in einem kurativ intendierten behandlungskonzept eine frhzeitige intensive systemtherapie vor der operation angestrebt wird [ 9 ]  . david krug und matthias f . 
bujko k , nowacki mp , nasierowska - guttmejer a et al ( 2006 ) long - term results of a randomized trial comparing preoperative short - course radiotherapy with preoperative conventionally fractionated chemoradiation for rectal cancer . 
ngan sy , burmeister b , fisher rj et al ( 2012 ) randomized trial of short - course radiotherapy versus long - course chemoradiation comparing rates of local recurrence in patients with t3 rectal cancer : trans - tasman radiation oncology group trial 01.04. 
breugom aj , swets m , bosset j - f et al ( 2015 ) adjuvant chemotherapy after preoperative ( chemo ) radiotherapy and surgery for patients with rectal cancer : a systematic review and meta - analysis of individual patient data . 
rdel c , graeven u , fietkau r et al ( 2015 ) oxaliplatin added to uorouracil - based preoperative chemoradiotherapy and postoperative chemotherapy of locally advanced rectal cancer ( the german cao / aro / aio - 04 study ) : nal results of the multicentre , openlabel , randomised , phase 3 trial . 
schrag d , weiser mr , goodman ka et al ( 2014 ) neoadjuvant chemotherapy without routine use of radiation therapy for patients with locally advanced rectal cancer : a pilot trial . 
deng y , chi p , lan p et al ( 2016 ) modied folfox6 with or without radiation versus uorouracil and leucovorin with radiation in neoadjuvant treatment of locally advanced rectal cancer : initial results of the chinese fowarc multicenter , open - label , randomized three - arm phase iii trial . 
garca - aguilar j , chow os , smith dd et al ( 2015 ) effect of adding mfolfox6 after neoadjuvant chemoradiation in locally advanced rectal cancer : a multicentre , phase 2 trial . 
nach dem medizinischen und zahnrztlichen staatsexamen erfolgte zunchst die weiterbildung zum facharzt fr mund - , kieferund gesichtschirurgie und anschlieend die radiologische ausbildung mit dem schwerpunkt strahlentherapie in mnster . er habilitierte sich auf dem gebiet des einusses der strahlentherapie auf knochenwachstum und reparatur . besondere bekanntheit hat wannenmacher durch die einfhrung der grofeldbestrahlung bei malignen lymphomen erlangt . seit 1977 hatte er den lehrstuhl fr strahlentherapie in freiburg inne und 1988 wechselte auf den lehrstuhl fr strahlentherapie in heidelberg , den er bis 2003 leitete . die wissenschaftlichen arbeiten von michael wannenmacher waren wesentlich geprgt durch die entwicklung von verfahren der przisionsstrahlentherapie , wie z . 
diese forderung nach einer fachbergreifenden behandlung von krebskranken menschen erfllte er wie kaum ein anderer mediziner mit leben : als prsident der deutschen krebsgesellschaft gestaltete er nachhaltig die onkologischen strukturen in deutschland . er gab dem deutschen krebskongress 1994 als prsident mit einer starken interdisziplinren betonung ein neues format . seine patienten schtzten sein freundliches wesen und die vertrauensvolle art . 
kollegen und mitarbeitern begegnete er als ruhiger , bestimmter und zielgerichteter mensch . seine zahlreichen schler verehren ihn als groartigen lehrer und vorbild . die verdienste von wannenmacher um die onkologie wurden durch zahlreiche ehrungen und preise ausgezeichnet , darunter das bundesverdienstkreuz 1 . 
immink3 , 6 andreas marinelli4 jos merkus5 anna petoukhova1 gabrielle speijer2 peter koper1 received : 23 march 2016 / accepted : 21 july 2016 / published online : 18 august 2016 springer - verlag berlin heidelberg 2016 abstract background scarce data are available about the cosmetic result of single dose intraoperative electron radiotherapy ( ioert ) in breast - conserving radiotherapy . methods and materials we included 71 breast cancer patients . 
we compared the subjectively and the objectively derived cosmetic scores with each other . results for four asymmetry features we noted signicantly smaller differences for patients treated with ioert when compared to those treated with wbi : relative breast contour difference , relative breast area difference and relative breast overlap difference . 
after correcting for excision volume a signicant difference was noticed also for relative lower ( cid : 2 ) henk struikmans h.struikmans@mchaaglanden.nl 1 radiotherapy centre west , medical centre haaglanden , lijnbaan 32 , 2501 ck the hague , the netherlands 2 department of radiotherapy , haga medical centre , leyweg 275 , 2545 ch the hague , the netherlands 3 department of radiotherapy , reinier de graaf medical centre , reinier de graafweg 3 / 11 , 2625 ad delft , the netherlands 4 department of surgery , medical centre haaglanden , lijnbaan 32 , 2501 ck the hague , the netherlands 5 department of surgery , haga medical centre , leyweg 275 , 2545 ch the hague , the netherlands 6 department of radiotherapy , leiden university medical centre , albinusdreef 2 , 2300 rc leiden , the netherlands breast contour . 
when the overall cosmetic scores for patients treated with ioert and wbi were compared to those of the objectively derived scores , there was a fair level of agreement . conclusion for patients treated with ioert we noted less asymmetry and high rates of good or excellent subjectively derived cosmetic scores . 
due to the small sample size and the design of the study no denitive conclusions can be drawn . keywords radiotherapy accelerated partial breast irradiation intraoperative electron radiotherapy asymmetry lumpectomy alleinige ioert versus ganzbrustbestrahlung kosmetische ergebnisse bei der brusterhaltenden therapie zusammenfassung hintergrund es sind nur wenige daten zum kosmetischen ergebnis nach alleiniger intraoperativer radiotherapie mittels elektronen ( ioert ) in der brusterhaltenden behandlung verfgbar . methoden und materialien in einer komparativen kohortenanalyse wurden 71 brustkrebspatientinnen eingeschlossen . 
im anschluss erhielten 26 patientinnen zustzlich eine ioert und 45 patientinnen eine postoperative ganzbrustbestrahlung ( wbi )  . wir verglichen die unterschiede von 7 dimensionslosen asymmetriemerkmalen zwischen beiden gruppen sowie subjektiv und objektiv ermittelte kosmetische werte . 706 strahlenther onkol ( 2016 ) 192 : 705713 ergebnisse die folgenden vier dimensionslosen asymmetriemerkmale waren in der ioert - gruppe im vergleich zur wbi - kohorte signikant besser : relative brustkonturlngendifferenz , differenz der relativen brustche und relativer brustberlappungsunterschied . 
die kosmetischen gesamt - scores der ioertund wbi - gruppe zeigten eine begrenzte bereinstimmung mit den objektiv bestimmten kosmetischen scores . schlussfolgerung fr die ioert - gruppe wurden geringere asymmetrieraten festgestellt sowie hohe raten von subjektiven bewertungen mit ausgezeichnet oder gut . 
aufgrund der kleinen anzahl von patientinnen und des studiendesigns knnen keine endgltigen schlussfolgerungen gezogen werden . schlsselwrter strahlentherapie akzelerierte teilbrustbestrahlung intraoperative elektronenbestrahlung asymmetrie lumpektomie introduction accelerated partial breast irradiation ( abpi ) focuses on irradiating only the lumpectomy cavity [ 13 ]  . 
in a subgroup they noted signicantly less skin side effects in the ioert group . we concluded that ioert could safely be administered in breast cancer patients with a low risk of developing an ibtr . 
for these patients 5 - year ibtr rates of 1.51.9 % have been reported [ 2 , 3 ]  . breast - conserving therapy also aims at an optimal cosmetic result . 
moreover , a fair or poor cosmetic outcome has also been associated with worse psychological recovery , a decrease in quality of life and a negative body image [ 69 ]  . 
the aim of our study is to compare the ( objectively assessed ) degree of asymmetry features and the ( subjectively and objectively derived ) cosmetic results after ioert with those after wbi . methods and materials patients we included patients irradiated with ioert and wbi 3 years after breast - conserving surgery . 
the following inclusion criteria were used for both groups : breast cancer or ductal carcinoma in situ ( dcis ) in female patients aged 60 years or older , tumour size less than 3 cm , tumour - free resection margins of at least 2 mm and absence of axillary lymph node metastases . 
comorbidity was scored as yes or no , since only few patients suffered from each specic type ( or combinations ) of comorbidity . we determined the median interval time between surgery and the date of the follow - up . 
written informed consent was obtained in all cases . strahlenther onkol ( 2016 ) 192 : 705713 radiotherapy cosmetic evaluation ioert was administered directly after the lumpectomy and the sentinel procedure . 
during the surgical procedure the presence of a tumour - free resection margin of at least 2 mm was checked by visual inspection of the lumpectomy specimen by the pathologist in case of a palpable lesion or was determined by specimen radiology in case of a nonpalpable lesion . 
re - excision was done if the tumour - free resection margin was < 2 ma total dose of 23.3 gy ( prescribed at the 100 % isodose ) was administered and directed to the lumpectomy cavity with a margin of 2 chigh - energy electron ( 612 mev ) beam radiotherapy was used . 
thirty - eight patients received a breast dose of 42.56 gy , while 7 patients received a breast dose of 50 gy ; a boost dose was given in 19 and 2 patients , respectively . full colour digital photographs , using a 3 - megapixel camera , were taken . 
2 examples of the overall cosmetic result : excellent , good , fair and poor table 1 the denitions of the seven dimensionless asymmetry features for breast brosis statistical analyses pbra plbc punr pbce pbcd pbad pbod the relative breast retraction assessment . 
this quanties the non - overlapping area of the two breasts after ipping one of them along a vertical line and making coincident both points of junction with thorax the software prograadding a boost leads to a more pronounced asymmetry rate [ 4 ]  . 
in the wbi group we , therefore , compared the rate of asymmetry between patients with and those without a boost . due to the relatively small numbers , the tumour locations were divided in 2 groups : the mediocentral location and the lateral location . 
the overall cosmetic scores for 26 ioert patients and 45 wbi patients , as measured by the software program , are summarized in table 3 . ioert patients judged the cosmetic result as excellent or good in 88 % of the cases ( table 4 ) , whereas this rating by the physician was 96 % ( table 5 )  . 
the ratings , as applied by each wbi patient and the single physician , of patients treated with wbi were 81 and 73 % , respectively . the levels of agreement for all 71 patients between the cosmetic scores derived from the software program , the patients and the physicians evaluation are given in table 6 and 7 . 
noted an overall better cosmetic outcome for patients treated with the targit type iort compared to those treated with wbi throughout the whole follow - up period of ve years . 
although not scored in this study , it is well known that radiation - induced changes in colour of the skin and shape of the breast depend on the skin dose , the irradiated volume [ 47 ]  . 
it is likely that the observed high scores of good or excellent of the cosmetic results in the ioert group are related to the fact that only the lumpectomy cavity is irradiated , while the skin did not receive any radiation . 
the observed disagreement between the results of the subjectively and the objectively derived cosmetic scores may partly be explained by the characteristics of the software of the program because this program seldom scores the category excellent . 
the reason for the latter is the basic assumption of the program , being that excellent cosmetic result can only be scored if there is a perfect symmetry of both breasts . differences of dimensionless asymmetry features for four of seven asymmetry features the results of the software program for the ioert group , when compared with those treated with wbi signicant , better results were noted . 
although different values were found , the scores for the seven dimensionless features of asymmetry in the wbi group in our series were in line with the scores reported by immink et al . 
we want to stress that the volume of the lumpectomy specimen ( being a major surgical variable determining cosmetic result ) did not differ between the ioert and the wbi groups . 
two fractionation schemes were given in the wbi group , but from this no major bias can be anticipated [ 22 , 23 ]  . analysis of the patient characteristics showed a signicant difference in age between the two groups . 
with respect to the latter , munshi et al . [ 5 ] showed that menopausal status and not age is an important factor inuencing the cosmetic result of the breast after breast conserving therapy . 
the higher proportion of adjuvant tamoxifen use in the iort group , though , may potentially have caused an increase , but not a decrease , of the rate of brosis [ 24 ]  . 
such a phenomenon is not known for aromatase inhibitors [ 25 ]  . hence , the higher rate of tamoxifen medication in the ioert group may ( if any ) have caused a worsening of the cosmetic outcome in these cases . 
in former studies it was noted that bmi and scar visibility as well as breast size and smoking might also inuence the cosmetic result [ 26 , 27 ]  . these characteristics were not available in this study . 
low recurrence rates were reported , but few data are available that compare the cosmetic results between ioert and wbi . 712 conclusion in this comparative non - randomised study we noted , after 3 years of follow - up , less asymmetry for patients treated with ioert . 
koper state that they have no competing interest . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the ear was calculated for the contralateral breast and the lungs from dosevolume histograms ( dvh ) based on the linear - exponential , the plateau , and the full mechanistic doseresponse model . 
peripheral lowdose measurements were performed to compare the ear in more distant regions as the thyroids and the uterus . results fff reduces the ear signicantly in the contralateral and peripheral organs for tvmat and in the peripheral organs for vmat . 
no reduction was found for imrt . the lowest ear for the contralateral breast and lung was achieved with tvmat fff , reducing the ear by 25 % and 29 % as compared to tvmat ff , and by 44 % to 58 % as compared to vmat and imrt in both irradiation modes . tvmat fff showed also the lowest peripheral dose corresponding to the lowest ear in the thyroids and the uterus . ( cid : 2 ) barbara dobler barbara.dobler@ukr.de 1 department of radiotherapy , regensburg university medical center , 93042 regensburg , germany faculty of computer science and mathematics , ostbayerische technische hochschule regensburg , regensburg , germany conclusion the use of fff mode allows reducing the ear signicantly when tvmat is used as the treatment technique . 
when second cancer risk is a major concern , tvmat fff is considered the preferred treatment option in sib irradiation of right - sided breast cancer . keywords breast cancer radiotherapy second cancer risk flattening filter free peripheral dose sekundrmalignom - risiko nach simultan integrierter boost - bestrahlung des rechtsseitigen mamma - karzinoms mit und ohne ausgleichskrper zusammenfassung zielsetzung ziel der studie war es zu untersuchen , ob der ausgleichskrperfreie modus ( fff ) bei der simultan integrierten boost - ( sib - ) bestrahlung des rechtsseitigen mammakarzinoms eine reduktion des strahleninduzierten sekundrmalignomrisikos ( excess absolute risk , ear ) im vergleich zur bestrahlung mit ausgleichskrper ( ff ) erlaubt . patienten und methoden auf ct - daten von 10 patienten wurden jeweils 6 plne zur behandlung der gesamten brust mit einer verschreibungsdosis von 50 , 4 gy und eines sib mit 63 gy generiert : eine intensittsmodulierte strahlentherapie ( imrt ) , eine volumenmodulierte rotationstherapie ( vmat ) und eine tangentiale vmat ( tvmat ) , jeweils mit und ohne ausgleichskrper . 
das ear wurde fr die kontralaterale brust und die lungen anhand des linear - exponentiellen modells , des plateauund des mechanistischen modells fr die dosisreaktion aus den dosis - volumen - histogrammen ( dvh ) der organe berechnet . 
zustzlich wur688 strahlenther onkol ( 2016 ) 192 : 687695 den periphere dosismessungen durchgefhrt , um das ear in schilddrse und uterus zu vergleichen . ergebnisse fff reduziert das ear in den kontralateralen und peripheren risikoorganen bei tvmat und in den peripheren organen bei vmat . 
das niedrigste ear in schilddrse und uterus wurde ebenfalls mit tvmat fff erreicht . schlussfolgerung der ausgleichskrperfreie modus eines linearbeschleunigers erlaubt eine signikante reduktion des ear , wenn zugleich tvmat als bestrahlungstechnik gewhlt wird . 
daher wird tvmat fff als bevorzugte bestrahlungsoption betrachtet , wenn das sekundrmalignomrisiko von groer bedeutung ist . and hodgkin patients treated with radiation therapy [ 37 ]  . the ear after whole breast radiation therapy has been previously investigated by abo - madyan et al . [ 8 ] who found an increased ear in the contralateral breast and the lungs for imrt and vmat as compared to tangential eld techniques . the latest development in the technology of linear accelerators is the opportunity to irradiate patients without a attening lter in the beam path to increase dose rate and reduce beam - on time [ 9 ]  . 
since the attening lter is a source of scatter radiation , its removal has the positive side effect of lowering out - of - eld doses [ 10 ]  . 
the purpose of the study presented here was to investigate if the use of the attening lter free mode ( fff ) allows decreasing the ear after simultaneous integrated boost ( sib ) radiation therapy of right - sided breast cancer as compared to the at beam mode ( ff )  . schlsselwrter mamma - karzinom radiotherapie strahleninduziertes sekundrmalignomrisiko ausgleichskrperfreie bestrahlung periphere dosis methods patients dosevolume histogram excess absolute risk attening lter attening lter free intensity - modulated radiation therapy linear model abbreviations 3d - crt three - dimensional conformal radiation therapy imrt lin_exp linearexponential model mech plateau plateau model vmat volumetric modulated arc therapy tvmat tangential volumetric modulated arc therapy full mechanistic model organ at risk organ equivalent dose planning target volume simultaneous integrated boost background adjuvant radiation therapy following breast - conserving surgery allows improving local control and overall survival in early stage breast cancer patients [ 1 ]  . 
it has been shown , however , that the risk of developing a second cancer is increased after radiation therapy for women under the age of 40 [ 2 ]  . 
the excess absolute risk of developing a second cancer after exposure to radiation ( ear ) can be estimated from dosevolume histograms ( dvh ) based on biological models which are tted to data of atomic bomb survivors computed tomography ( ct ) data of 10 patients with rightsided breast cancer were randomly selected from our database for a retrospective planning study . 
the treatment goals were an average dose of 50.4 gy in 28 fractions of 1.8 gy to the planning target volume ( ptv ) and 63 gy in 28 fractions of 2.25 gy in the sib according to [ 12 ]  . 
doses to the contralateral breast and lungs and the normal tissue , dened as the patient outline excluding the targets , should be kept as low as possible to minimize the risk of second cancer induction [ 13 ]  . treatment planning treatment planning was performed with monaco 5.0 ( elekta ab , stockholm , sweden ) with x - ray voxel monte carlo dose algorithm for a synergy linear accelerator ( linac ) with agility head ( elekta ab , stockholm , sweden )  . 
in total six treatment plans were created for each patient , using the three different treatment techniques imrt , vmat , and tangential arc vmat ( tvmat ) each with 6 mv photons with and without attening lter . 
a so - called surface margin of 3 mm was used to prevent the optimizer from adding dose to the strahlenther onkol ( 2016 ) 192 : 687695 surface region to compensate for the buildup effect . 
to ensure coverage of the breast a so - called auto ash margin of 2 cm was used , which automatically extends the beam 2 cm beyond the patient outline . 
 [ 18 ] were calculated with a dose tolerance of 3 % of the maximum dose and 3 mm distance to agreement . pixels with a dose below 10 % of the maximum dose are excluded from the gamma evaluation . 
for verication of the dose calculation in the low - dose region of the contralateral breast , a second setup with matrixx evolutiontm was used : the isocenter was placed such that the high - dose area of the ptv was inside the phantom to maintain phantom scatter and the dose region corresponding to the medial part of the contralateral breast was located in the active area of the matrixx evolutiontm . 
dose differences between measured and calculated doses were calculated for all pixels in the roi to assess the accuracy of dose calculation in the lowdose region . excess absolute risk of second cancer development the excess absolute risk ( ear ) to develop a solid cancer after exposure to radiation has been estimated from data [ 19 ] for of the atomic bomb survivors by preston et al . different kinds of solid cancer . 
the ear describes the absolute difference in cancer rates of persons exposed to a dose d and those not exposed to a dose beyond the natural dose exposition per 10 , 000 personyears per gy and can be described as ear .d ; e ; s ; a / d g .e ; s ; a / ( cid : 2 ) f .d / with a function g of age at exposure e , sex s and attained age a and a doseresponse function f ( d )  . 
in this study , ear values are calculated for women at an age at exposure of 30 years and an attained age of 70 years and reported per 10 , 000 personyears per gy . a linear doseresponse has been observed for doses up to 2 gy leading to ear .d ; e ; s ; a / d ear0 .e ; s ; a / ( cid : 2 ) d with the excess absolute risk per 10 , 000 personyears per gy at low doses ear0 . 
for higher doses and inhomogeneous dose distributions , however , the doseresponse is no longer linear [ 3 , 13 ] and other doseresponse functions are required . for this purpose schneider et al . 
for the linear model oedlin , it is assumed that the doseresponse is linear to the dose exposition , and the oedlin for an organ can be calculated as oedlin d 1 vi di where vi is the volume of the organ that is exposed to dose di and v is the total volume of the organ . 
the linear exponential model oedlin_exp takes into account that the probability for cell killing increases exponentially with dose which leads to a decrease of the risk of cancer induction due to the killing of mutated cells : oedlin _ exp d 1 vi di e ( cid : 2 ) ( cid : 2 ) di the parameter = 0.044 gy1 has been derived from a combined t to the data of atomic bomb survivors and data of hodgkin patients treated with doses up to 40 gy [ 4 ]  . 
the plateau model oedplateau assumes that the doseresponse reaches a plateau after rising linearly up to a certain dose due to a balance in cell killing and recovery effects in a fractionated scheme : oedplateau d 1 vi .1 ( cid : 3 ) e ( cid : 2 ) di / = the parameter = 0.139 gy1 has been derived from a combined t to the data of atomic bomb survivors and 690 strahlenther onkol ( 2016 ) 192 : 687695 fig . 
the full mechanistic model leads to the linearexponential model in the limit of no repopulation and repair r ! 0 with a dose dependent = 0 and to the plateau model in the limit of full repopulation and repair r ! 1 with a dose dependent = 0 . in the full mechanistic model , the difference between the baseline risks of developing cancer without exposition to radiation for japanese and western population has been accounted for , leading to values of ear0 ( 30 , f , 70 ) = 8.2 for female breast and ear0 ( 30 , s , 70 ) = 8.0 for lung ( sex averaged )  . no separate value is listed for female lungs [ 6 ]  . 
the organ specic parameters = 0.044 gy1 and r = 0.15 for female breast and = 0.042 gy1 and r = 0.83 for lung have been derived from a combined t to the data of atomic bomb survivors and data of hodgkin patients treated with single doses of 2 up to 40 gy assuming an / value of 3 gy [ 6 ]  . it has been shown that especially for doses above 4 gy and inhomogeneous dose distributions the linearexponential , the plateau and the full mechanistic model improved the description of the doseresponse relationship as compared to the linear model [ 4 , 6 ]  . 
therefore the linear model was not included in the estimation of ear of breast and lung in this study . peripheral low - dose assessment planning ct data do not include cranial and caudal organs at risk ( oar ) at larger distances for reasons of radiation protection . 
analysis was performed comparing rst the two irradiation modes ff and fff and second the treatment techniques imrt , vmat , and tvmat . since the main subject of the study was the comparison of the two irradiation modes ff and fff , statistical signicance between the irradiation modes is marked in the tables using bold characters . 
the orange isoband shows 95 % of the prescription dose to the sib , the turquoise the 76 % corresponding to 95 % of the prescription dose to the planning target volume . 
isodoses are shown for the range of 76110 % of the prescription dose of 63 gy for illustration of target coverage , and for the range of 14 % to illustrate the differences in the low - dose region . 
bold - italic values indicate signicantly lowest ear values in the comparison over all planning techniques and irradiation modes imrt intensity - modulated radiotherapy , vmat volumetric modulated arc therapy , tvmat tangential volumetric modulated arc therapy , ff attening lter , fff attening lter free nique . 
comparison of the three treatment planning techniques showed a signicant reduction in ear of the contralateral breast and lung for tvmat as compared to imrt and vmat in both irradiation modes for all doseresponse models . 
in fff mode , the reduction was even more pronounced ranging from 4447 % for the contralateral breast and from 5658 % for the contralateral lung depending on the doseresponse model . 
fff reduced out - of - eld doses significantly as compared to ff when vmat or tvmat were used , with a dose reduction of 21 % for vmat and of 22 % for tvmat . 
the dose reduction was not signicant when in comparison imrt was used as treatment technique . of the treatment techniques tvmat showed signicantly lower out - of - eld doses than vmat and imrt with a reduction of 6 % as compared to vmat in both irradiation modes and of 20 % and 31 % as compared to imrt in ff and fff mode , respectively . 
lowest out - of - eld dose over all treatment techniques and irradiation modes was found for tvmat fff followed by vmat fff . discussion the aim of this study was to investigate if the use of attening lter free beams allows decreasing radiation induced second cancer risk in sib radiation therapy of breast cancer . 
the bold - italic value indicates the signicantly lowest dose value in the comparison over all planning techniques and irradiation modes imrt intensity - modulated radiotherapy , vmat volumetric modulated arc therapy , tvmat tangential volumetric modulated arc therapy , ff attening lter , fff attening lter free to predict the excess absolute risk of second cancer after radiation therapy based on dosevolume histograms of the treatment plans . 
to assure that the dvh calculated by monaco 5.0 in this study can be used as a proper base for the calculation of the second cancer risk , the dose calculation has been veried by 2d measurements for all 60 plans . the results of the study show that fff reduces the ear in the contralateral oar signicantly , when tvmat is used as treatment technique . 
when vmat was used as treatment technique , the risk was kept comparable for the contralateral breast and the lungs . in case of imrt treatments , the linear exponential doseresponse model predicted even a signicant increase of the ear in the contralateral lung when fff was used as irradiation mode , and no improvement could be observed in any of the oar . 
comparison of the three treatment planning techniques showed a signicant reduction in ear of the contralateral breast and lung for tvmat as compared to imrt and vmat in both irradiation modes . 
the signicantly lowest ear for the contralateral breast and lung was achieved in all doseresponse models with tvmat fff as compared to all other techniques and irradiation modes , with a reduction by about 50 % as compared to imrt and vmat and about 25 % as compared to tvmat ff . 
since planning ct data do not include cranial and caudal oar at larger distances for reasons of radiation protection , no calculations of the second cancer risk based on dvh are possible for these organs . 
therefore peripheral dose measurements at a distance of 31 cm in cranial direction were compared , which can be associated with the location of the thyroids in cranial and the uterus and the bladder in caudal direction due to the symmetry of the breast in craniocaudal direction . 
mean values per 10 , 000 personyears per gy averaged over all 10 patients are shown 694 strahlenther onkol ( 2016 ) 192 : 687695 mgy for tvmat and from ( 121 20 ) mgy to ( 95 20 ) mgy for vmat when fff was used as irradiation mode . this is associated with a signicant reduction of the ear of 22 % and 21 % in these regions due to the linearity of the doseresponse below 2 gy [ 19 ]  . 
the signicantly lowest peripheral dose in the comparison of all treatment techniques and irradiation modes was achieved with tvmat fff followed by vmat fff . planning studies including the prediction of radiationinduced cancer risk are still sparse . 
one group published two studies comparing the excess relative risk after three dimensional conformal radiation therapy ( 3d - crt ) , imrt , and vmat with varian devices for breast cancer [ 22 ] and for hodgkin lymphoma [ 23 ] using a linear and a non - linear model : weber et al . 
 [ 23 ] found an increased risk for radiation - induced cancer in breast and lung in involved eld radiation therapy of hodgkin lymphoma when imrt and vmat were used as treatment techniques as compared to 3d - crt . 
 [ 22 ] found no statistically signicant differences between the different treatment techniques when comparing the risk for radiation - induced cancer in the contralateral breast for breast cancer radiation therapy . two studies have been published previously assessing the second cancer risk after 3d - crt , imrt , and vmat for breast cancer using elekta devices [ 8 , 24 ]  . 
 [ 8 ] compared tangential 3d - crt , tangential imrt , imrt , and vmat , the two latter with a gantry angle range of about 200 , for a whole breast treatment of left - sided breast cancer with a total prescription dose of 50 gy . 
they estimated an increased ear in the contralateral breast and lung for imrt and vmat as compared to 3d - crt and tangential imrt using the linear , the linearexponential , and the plateau doseresponse model . 
 [ 24 ] performed measurements in an anthropomorphic phantom to compare dose exposition of the thyroid , contralateral breast , and ipsilateral lung in whole breast radiation therapy and concluded also an increased second cancer risk for imrt and vmat as compared to 3d - crt . combining the results of these studies with the results of our study the following can be concluded : imrt and vmat are associated with a higher second cancer risk when exploiting a larger gantry angle range of around 200 as compared to techniques with a limitation of the beam orientation to the tangents or short arcs around the tangents for whole breast and sib treatment . 
the study presented here also showed that the use of fff allows further decreasing the second cancer risk for the contralateral breast and lung as well as for more distant organs as the thyroid , uterus , and bladder if tvmat is used as treatment technique . 
if vmat is used , a reduction of ear was only achieved in the peripheral oar , whereas for imrt no reduction in ear could be found in any of the organs and even signicant increase was predicted for the contralateral lung in one of the three doseresponse models . conclusion the results of the study show that fff reduces the ear in the contralateral and peripheral oar signicantly , when tvmat is used as treatment technique . 
when the risk of radiation induced second cancer is a major concern , as it is for young women , tvmat fff is therefore the preferred treatment option for sib treatment of right - sided breast cancer . 
when fff is not available , tvmat ff should be used for this kind of treatment . funding this study was funded by the bavarian state ministry of the environment and consumer protection . compliance with ethical guidelines conict of interest the department has research cooperation with elekta gmbh hamburg . 
despite various hypotheses , the pathomechanism of rrd appears complex and is still not fully understood . in addition , no clinical guidelines exist concerning whether drug treatment should be continued upon manifestation of an associated radiation recall phenomenon . 
we present the case of a patient with docetaxel - induced rrd , which was successfully treated with topical steroids and systemic antihistamines ; re - challenge to docetaxel did result in very mild remanifestation of skin reactions . keywords antihistaminics irradiation antiinammatory agents , non - steroidal corticosteriods radiation , sensitizing agents docetaxel - induzierte strahlen - recall - dermatitis eine kasuistik und review der literatur zusammenfassung die strahlen - recall - dermatitis ( rrd ) ist eine akute entzndliche reaktion der haut in einem zuvor bestrahlten areal als reaktion auf die systemische applikation eines triggernden agens . 
ferner gibt es keine klinischen leitlinien dazu , ob bei einem assoziierten rrd - phnomen die medikamentse behand ( cid : 2 ) iosif strouthos jstrouthos@gmail.com strahlenklinik , sana klinikum offenbach , starkenburgring 66 , 63069 offenbach , germany lung fortgesetzt werden sollte oder nicht . 
eine erneute docetaxel - exposition des patienten ging mit einer sehr milden remanifestation der kutanen eforeszenzen einher . schlsselwrter antihistaminika bestrahlung nichtsteroidale antiinammatorische agenzien kortikosteroide strahlensensibilisierende substanzen introduction radiation recall dermatitis ( rrd ) refers to an acute inammatory skin reaction appearing on a previously irradiated skin area in response to the systemic administration of a triggering agent . 
chemotherapeutic compounds are common instigators , but the appearance of rrd has also been described to arise from antibiotics , monoclonal antibodies , or biological response modiers [ 1 ]  . in 1959 , dangio et al . [ 2 ] originally described the phenomenon of rrd in association with the systemic administration of actinomycin d . 
consequently , no high - evidence guidelines exist for the clinical management of rrd and especially the further administration or discontinuation of triggering agents from an oncological point of view . despite systematic research efforts , the pathomechanism of rrd remains unknown . 
a number of hypotheses have been introduced with vascular damage , epithelial stem cell strahlenther onkol ( 2016 ) 192 : 730736 depletion / inadequacy , epithelial stem cell sensitivity , and idiosyncratic drug hypersensitivity constituting the most promising research approaches [ 3 ]  . 
at this point , however , it is crucial to differentiate between direct sensitizing effects of systemically administered agents causing acute radiation - induced dermatitis ( radiosensitization ) and the , socalled , real recall phenomenon . 
the time boundary distinguishing the two entities has been set at 7 days past the end of radiotherapy ( rt ) [ 3 ]  . independent of the exact etiopathology , several substances have been implemented for symptomatic treatment including corticosteroids , nonsteroidal anti - inammatory drugs ( nsaids ) , and antihistaminics [ 4 ]  . case report a 71 - year old caucasian male was diagnosed in may 2014 with metastatic non - small cell lung cancer . 
the case was reviewed once again at the pneumo - oncological tumor conference , resulting in a switch of the cht protocol to docetaxel 35 mg / m2 weekly and rt of the symptomatic osseous metastases at the level of twelfth thoracic and the third lumbar vertebrae . 
of note , the skin reactions manifested only on the posterior side of the body with no clinical signs anteriorly . interestingly , the previously irradiated areas of the skull and right iliac crest did not show any erythematous lesions . 
the re - challenge again induced pruritus and erythema , however less vivid as initially seen . oral antihistaminics were additionally prescribed contributing to the complete resolution of the skin reactions 3 weeks later . discussion radiation recall dermatitis describes a rare inammatory skin reaction which develops on a previously irradiated area in response to systemic administration of various agents [ 1 ]  . 
in the absence of systematic studies , rrd is depicted predominantly through case reports with cytostatic compounds , antibiotics , monoclonal antibodies , and biological response modiers being identied to trigger reactive dermatitis weeks , months , or even years after rt [ 612 ]  . 
 [ 2 ] described rrd upon systemic administration of actinomycin d already in 1959 , no guidelines exist regarding its clinical management or the further handling of instigator administration until present . the incidence of rrd has been reported to be 510 % with no gender preference [ 13 , 14 ]  . it is mainly a clinical diagnosis based on the patients treatment history in association with typical symptoms of cutaneous inammation including erythema , maculopapular or vesicular lesions accompanied by pruritus and localized hyperesthesia followed by xerodermia with or without localized paskin biopsies are not routinely performed as part of the diagnostic work - up since histopathological changes in patients presenting with clinically diagnosed rrd are not specic [ 15 ]  . 
c clinical status 9 days after initiation of topical corticosteroids showing a gradual relief of signs and symptoms of rrd from other dermatologic disease entities following the administration of radiosensitizing drugs should be based on a time boundary . 
the period for manifestation of rrd has been set to be more than 7 days after completion of rt . our study involves a case of docetaxel - induced rrd , a very rare recall phenomenon with few data reported in the literature ( [ 1627 ] ; table 1 )  . 
the most comprehensive source represents a systematic analysis by mizumoto et al . [ 27 ] reporting the incidence of docetaxel - induced rrd in a series of 171 consecutively treated patients . 
popular approaches focus on vascular damage [ 7 , 9 , 29 ] , epithelial stem cells inadequacy / depletion [ 30 ] , epithelial stem cell sensitivity [ 31 , 32 ] , and idiosyncratic drug hypersensitivity with the latter one proposed by camidge and price [ 3 ] seeming to be the most promising . 
through this hypothesis , the unpredictable event of agent rechallenge can be explained including the benet seen from steroid prophylaxis in preventing the recurrence of the phenomenon . several adjuvant concerning the treatment and management of rrd , there are no standard interventions relieving symptoms or enhancing recuperation . 
although discontinuing the triggering agent is advised by many reports , rechallenge does not always result in re - occurrence of the cutaneous treatments have been dereactions . scribed including systemic administration of corticosteroids , nsaids , or antihistaminics depending on the clinical severity [ 4 ]  . 
local treatment with hydrocortisone , silver sulfadiazine , sodium hyaluronate , or antioxidants has also been successfully implemented [ 20 ]  . in our study , topical steroids ( hydrocortisone 0.25 % cream ) and consecutively oral antihistaminics ( cetirizine 10 mg tablet ) were used resulting in a total recovery within 3 weeks . conclusion radiation recall phenomenon was rst described in 1959 and since then multiple chemotherapeutic and nonchemotherapeutic drugs have been found to elicit the reaction . 
d50 for body 1 is 25.0 gy , which is nearly twice the dose of 13.1 gy to body 2 though some etiological explanations have been postulated , the pathophysiology of rrd remains unknown . 
steroids ( topical and systemic ) , nsaids , antihistamines , and antioxidants have been implemented in the treatment of rrd . given the lack of high - quality evidence , it seems prudent to establish a universal recording system in order to improve the understanding of rrd and to optimize its treatment . acknowledgements the authors would like to thank sokratis papaioannou msc for his help in the preparation of the manuscript . compliance with ethical guidelines conict of interest i . 
zamboglou state that there are no conicts of interest . all procedures followed were in accordance with the ethical standards of the responsible committee on human experimentation ( institutional and national ) and with the helsinki declaration of 1975 ( in its most recently amended version )  . 
grosu5 received : 6 april 2016 / accepted : 15 july 2016 / published online : 17 august 2016 springer - verlag berlin heidelberg 2016 abstract background reirradiation is a potentially useful option for many patients with recurrent cancer . 
the purpose of this study was to review all recently published randomized trials in order to identify methodological strengths and weaknesses , comment on the results , clinical implications and open questions , and give advice for the planning of future trials . materials and methods systematic review of trials published between 2000 and 2015 ( databases searched were pubmed , scopus and web of science )  . results we reviewed 9 trials , most of which addressed reirradiation of head and neck tumours . 
the trials with relatively long median follow - up conrm that serious toxicity remains a concern after high cumulative total doses . conclusion multi - institutional collaboration is encouraged to complete sufciently large trials . 
despite a paucity of ( cid : 2 ) carsten nieder , md carsten.nieder@nlsh.no 1 department of oncology and palliative medicine , nordland hospital , 8092 bod , norway 2 department of clinical medicine , faculty of health sciences , university of troms , 9038 troms , norway 3 department of radiation oncology , university medical centre groningen , 9713 groningen , the netherlands 4 department of radiation oncology , university hospital zrich , 8091 zrich , switzerland 5 department of radiation oncology , university hospital freiburg , 79106 freiburg , germany large randomized studies , reirradiation has been adopted in different clinical scenarios by many institutions . 
typically , the patients have been assessed by multidisciplinary tumour boards and advanced technologies are used to create highly conformal dose distributions . keywords radiotherapy radiation oncology radiation retreatment research design randomized controlled trial prospektiv randomisierte studien ber rebestrahlung gewonnene erkenntnisse zusammenfassung hintergrund eine rebestrahlung kann fr viele patienten mit rezidivierenden malignomen eine ntzliche option bieten . 
der zweck dieser studie bestand darin , alle in der jngeren vergangenheit publizierten randomisierten studien zu beurteilen , da deren methodische strken und schwchen , ergebnisse und resultierende implikationen bzw . 
offene fragen die planung knftiger studien wesentlich beeinussen knnen . material und methoden systematische bersicht aller zwischen 2000 und 2015 verffentlichten studien ( literatursuche ber pubmed , scopus und web of science )  . ergebnisse ausgewertet wurden 9 studien , in die vor allem patienten mit kopf - hals - tumoren eingeschlossen waren . 
die studien mit lngerer nachbeobachtungszeit besttigen , dass 680 strahlenther onkol ( 2016 ) 192 : 679686 ernste nebenwirkungen nach hohen kumulativen totaldosen ein problem darstellen . schlussfolgerung um studien mit ausreichender fallzahl abschlieen zu knnen , sind multizentrische kollaborationen erforderlich . 
geeignete patienten werden meist in interdisziplinren tumorboards vorgestellt und mittels fortschrittlicher techniken hochkonformal und mglichst schonend bestrahlt . schlsselwrter strahlentherapie radioonkologie erneute strahlenbehandlung forschungsdesign randomisierte kontrollierte studien introduction as a consequence of the relentless dynamics of many human malignancies , local disease recurrence is a common clinical probleradiation oncologists have long been interested in administering a repeat course of radiotherapy to a previously irradiated volume ( reirradiation ) because such treatment might provide worthwhile clinical benet in terms of symptom palliation or sometimes even cure after diagnosis of local or regional relapse or second primary tumours in a pretreated region [ 14 ]  . 
in the era of evidence - based medicine practice - changing research advances are typically generated in large randomized clinical trials . the purpose of our study was to review all recently published randomized trials in order to identify methodological strengths and weaknesses , comment on the results , clinical implications and open questions , and give advice for the planning of future trials . methods all authors contributed to the textbook reirradiation : new frontiers and are thus aware of the historical data on this subject [ 5 ]  . 
trials were identied through systematic searches of the databases pubmed , scopus and web of science by use of the key words reirradiation , re - irradiation , repeat radiotherapy , radiation retreatment and recurrent and radiotherapy in february 2016 . 
combs1 , 4 daniel habermehl1 received : 18 december 2015 / accepted : 24 june 2016 / published online : 14 july 2016 springer - verlag berlin heidelberg 2016 abstract purpose volumetric - modulated arc therapy ( vmat ) achieves high conformity to the planned target volume ( ptv ) and good sparing of organs at risk ( oar )  . 
this study compares dosimetric parameters and toxicity in esophageal cancer ( ec ) patients treated with vmat and 3d conformal radiotherapy ( 3d - crt )  . materials and methods between 2007 and 2014 , 17 sc patients received neoadjuvant chemoradiation ( crt ) with vmat . 
of 20 patients treated with 3d - crt , 13 ( 65 % ) also received crt with cisplatin and 5 - fu , whereas 6 patients ( 30 % ) received crt with weekly oxaliplatin and cetuximab , and a continuous infusion of 5 - fu ( oe - 7 )  . results there were no differences in baseline characteristics between the treatment groups . 
verglichen wurden dosimetrische parameter und toxizitt zwischen vmat und 3d - konformaler strahlentherapie ( 3d - crt ) bei patienten mit sophaguskarzinom . material und methoden zwischen 2007 und 2014 erhielten 17 patienten whrend der neoadjuvanten radiochemotherapie eine vmat . 
in der 3d - crt - gruppe bekamen 13 patienten ( 65% ) ebenfalls eine chemotherapie mit cisplatin und 5 - fu , 6 patienten ( 30% ) eine wchentliche chemotherapie mit oxaliplatin und cetuximab , sowie eine kontinuierliche chemotherapie mit 5 - fu ( oe - 7 )  . ergebnisse hinsichtlich der basischarakteristika zeigte sich kein unterschied zwischen den gruppen . 
hugste postoperative komplikation war die anastomoseninsufzienz bei einem vmat ( 6 , 7 % ) und 5 3d - crt - patienten ( 27 , 8 % ; p = 0 , 180 )  . 
ein lokalrezidiv wurde bei 6 3d - crt ( 30 % ) und bei einem vmat - patienten ( 6 % ) beobachtet ( p = 0 , 097 )  . schlussfolgerung dosimetrische unterschiede der dosisverteilung in herz und lungen waren klinisch nicht relevant . 
verglichen mit 3d - crt reduziert vmat v30 fr lunge und herz und somit mglicherweise die toxizitt . schlsselwrter risikoorgane chemotherapie herz lungen berleben with more than 450 , 000 cases per year , esophageal cancer ( ec ) is the eighth most common cancer in the world . 
since many studies have demonstrated the advantage of neoadjuvant chemoradiation ( ncrt ) compared to surgery alone , multimodal therapy has become the standard treatment for patients with locally advanced ec who are suitable for surgery [ 3 , 4 , 5 ]  . for a long time , three - dimensional conformal radiotherapy ( 3d - crt ) was the standard planning method for radiotherapy ( rt ) of ec . 
by using different beam angles and varying intensities , this technique allows application of a highly conformal dose to the target with the possibility of reducing the dose to the organs at risk ( oar ) [ 6 , 7 , 8 , 9 ]  . in the case of ec , great attention should be payed to rt techniques and dose distribution , because with the heart , lungs , and spinal cord , there are at least three critical organs in close proximity to the target volume . 
it is well known that for the lungs , the volume receiving more than 20 gy ( v20 ) , that receiving more than 30 gy ( v30 ) , and the mean lung dose correlate with the risk of developing acute or chronic pneumonitis [ 10 , 11 ]  . 
however , a recent study examining biomarkers for myocardial or lung damage in patients undergoing mediastinal rt failed to identify useful parameters , although prospective studies are ongoing [ 14 , 15 , 16 ]  . a special variant of imrt is volumetric - modulated arc therapy ( vmat )  . 
by rotation of the irradiation beam during therapy , this technique uses all possible directions to achieve high conformity and dose sparing of the oar [ 6 ]  . the dosimetric superiority of vmat over 3d - crt and even xed - beam imrt has already been demonstrated for cervical cancer and prostate carcinoma [ 17 , 18 ]  . 
com724 strahlenther onkol ( 2016 ) 192 : 722729 pared to 3d - crt , imrt plans revealed better conformity and homogeneity indices , as well as a lower v20 for the left kidney and a lower v30 for the liver [ 19 , 20 ]  . 
also demonstrated that , compared to 45 gy with 3d - crt , an increased radiation dose of 50.4 gy is not associated with in a planning higher toxicities when using imrt [ 21 ]  . study by fakhrian et al . 
 [ 22 ] , modern radiation techniques like imrt and vmat also allowed an increase of the radiation dose to the planning target volume ( ptv ) without higher doses to oar when using simultaneous integrated boost ( sib ) concepts . however , results are heterogeneous when different techniques are used , particularly concerning the evaluation of lung doses . 
found an elevated risk for acute radiation pneumonitis in postoperative ec patients irradiated with vmat ( higher values for mean lung dose , v20 , and v30 ) compared to xed - eld imrt ( ffimrt ) [ 23 ]  . 
calculated lower v5 and v10 values for ffimrt compared to vmat plans , but higher v20 in patients with mid - thoracic ec in the context of an in silico treatment planning comparison [ 24 ]  . since there is no comparison concerning the clinical relevance of dosimetric differences between vmat and 3dcrt for ec in the literature , the purpose of this study is to compare dosimetric parameters and acute toxicity of 3d - crt and vmat in a real - life and homogeneous patient group with squamous cell carcinoma of the esophagus ( scc ) undergoing ncrt . patients and methods patient and treatment characteristics at the authors institution 17 patients with ec were treated with vmat and a daily dose of 1.8 gy up to an overall dose of 45 gy . 
patients with a tumor in the upper third of the esophagus were excluded . there was no signicant difference in baseline characteristics including gender , age , t category , positive lymph nodes , tumor localization , and craniocaudal tumor extension . 
3d - crt was performed with a median of six ( interquartile range , iqr , 57 ) coplanar beams , whereas all vmat plans used two arcs to deliver the planned dose . 
in patients who were treated with vmat , image - guided rt was conducted according to internal guidelines . all 17 patients who were treated with vmat received chemotherapy with cisplatin and 5 - uorouracil ( 5 - fu )  . 
of 20 patients treated with 3d - crt , 13 patients also received chemotherapy with cisplatin and 5 - fu , whereas chemotherapy with oxaliplatin , 5 - fu , and cetuximab was used in 6 patients analogous to the oe - 7 - protocol . 
after a median follow - up of 33.9 months , all surviving patients were contacted and asked for long - term effects . dose coverage of the ptv , compared by dmean and dmedian , was comparable in both groups ( table 3 )  . statistics progression - free survival ( pfs ) was dened as the time interval from the rst day of rt until tumor progression , local or distant failure , or death from any cause . statistical analyses comprised comparison of baseline parameters , side effects , and different dose parameters using the wilcoxonmannwhitney u test or fishers exact test . 
overall survival and pfs where compared using the log - rank test . the study was performed in accordance with the ethics standards at the technical university of munich ( tum )  . results dosimetric comparison regarding dose distribution to the lungs , patients who were treated with vmat had a higher v5 ( p = 0.013 ) and v10 ( p = 0.014 ) than patients treated with 3d - crt . 
no difference was observed for v20 ( p = 0.478 ) , mean , median , or maximum dose to the lungs ( table 2 )  . comparing dose distribution to the heart , vmat plans showed a higher dmax ( p = 0.003 ) , v5 ( p = 0.043 ) , and v10 ( p = 0.047 ) than 3d - rt plans . in contrast , dmedian ( p = 0.026 ) and v30 ( p = 0.015 ) were higher in 3d - crt plans . no signicant difference was observed for dmean , v15 , v20 , or v40 . clinical data chemoradiation was followed by surgery in 16 / 17 patients of the vmat group and 19 / 20 patients of the 3d - crt group . 
2 progression - free survival ( pfs ) in esophageal cancer patients treated with volumetric - modulated arc therapy ( vmat ) and three - dimensional conformal radiotherapy ( 3d - crt ; p = 0.421 ) in this study , one of the most common ncrt - related side effects was dysphagia . 
a total of 12 patients ( 70.6 % ) treated with vmat reported some kind of dysphagia during treatment : 7 patients ( 41.2 % ) had grade i dysphagia , 3 patients ( 17.6 % ) had grade ii dysphagia , and 2 patients ( 11.8 % ) reported grade iii dysphagia . 
no higher grades of dysphagia were reported by surviving patients . discussion aims of our study were the evaluation of dosimetric differences in real - life patient cohorts undergoing ncrt with vmat or 3d - crt , and a possible correlation of dosimetric parameters with distinct toxicities . as to be expected , for both the lungs and the heart , the volume receiving a low dose ( v5 , v10 ) is enlarged in patients treated with vmat plans compared to those treated with 3d - crt plans . in contrast , vmat can reduce the median volume receiving more than 30 gy by almost 65 % for the heart and by 40 % for the lungs . 
despite the lack of statistical signicance , the authors point out the large absolute difference of more than 27.5 % for the median v20 . the current study was not able to reveal signicant clinical differences in the analyzed groups , despite clear dosimetric differences . 
its superiority over conventional 3d - crt regarding target dose conformity and reduction of higher doses to the oar could already be demonstrated for different cancer subtypes [ 18 , 19 , 20 , 26 , 27 ]  . 
for ec , the critical oar are the lungs and the heart . as previously mentioned , mean lung dose , v20 , and v30 seem to be the most important risk factors for pneumonitis [ 11 , 23 ]  . 
regarding vmat , the mean dose to the lungs , v5 , and v20 were slightly lower in this planning study , although treatment plans were calculated with a sib dose of 54 gy . v30 and dmean relate to cardiac complications such as pericardial effusion . 
these parameters are also part of the quantitative analyses of normal tissue effects in the clinic ( quantec ) recommendations [ 30 ]  . particularly v30 could be signicantly reduced with vmat and a median v30 of 17.7 % is signicantly below the previously published threshold of 46 % . 
the median v30 in the 3d - crt plans exceeded this threshold . for both dmean and v20 , there is a clear absolute , but nonsignicant difference between the two groups . 
therefore , the authors can conclude that the number of patients with a dmean of more than 26 gy can be more than halved using vmat plans compared to 3dcrt . comparisons between vmat and imrt or 3d - rt and imrt revealed no signicant difference in dose distribution to the heart in ec patients [ 8 , 24 , 31 ]  . 
the current study , however , could demonstrate a signicant reduction of more than 64 % for v30 when comparing vmat and 3dcrt , and a clear albeit nonsignicant reduction in v20 and dmean . 
further studies should be performed in order to assess which of these three parameters is most important for cardiac toxicities . unlike the lungs , the heart covers only the lower half of the esophagus and its craniocaudal overlap with the radiation eld borders thus strongly depends on tumor localization and length . 
further studies aimed at investigating the relationship between rt technique and dose distribution should keep this fact in mind when selecting patients . in contrast to a study by boda - heggemann et al . 
 [ 32 ] , who demonstrated improved overall and disease - free survival in gastric cancer patients treated with imrt , this study revealed no signicant differences for 3 - year overall survival and 3 - year pfs between patients treated with 3d - crt and patients treated with vmat , which might be explained by the small number of patients . the most common non - hematological side effect was dysphagia . 
because of the low number of patients this result is not statistically signicant and evidence of whether further studies can reproduce this result in larger patient groups is awaited . in contrast to other planning studies , this study uses a real - life cohort and cannot only compare different dose parameters , but also clinical aspects . 
obviously , this is an advantage over planning studies that compare different radiation techniques in the same collective . one limitation of the present study is its retrospective nature with all the inherent problems concerning followup data . 
for every patient , a ct scan of the thorax was performed within the rst 3 months after therapy , but clinical symptoms such as fever , dyspnea , or cough could not be queried retrospectively . 
nonetheless , we wanted to ensure a consistent daily and total dose for the whole group . conclusion although clear dosimetric differences in lung and heart exposure were observed , no acute changes in toxicity proles were detectable . 
for the heart , however , longer follow - up times are required for full development of cardiac toxicity . for side effects such as dysphagia , no clinical benet of the vmat plan could be seen . 
despite these short - term clinical results , vmat provides the opportunity of reducing v30 of the lungs and the heart with comparable dose coverage of the ptv as compared to 3d - crt in a real - life patient cohort . 
the signicant dosimetric benet of vmat and possible benets regarding long - term toxicity therefore clearly justify its clinical use in this setting . compliance with ethical guidelines conict of interest s . 
habermehl declare that they have no competing interests . all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
we analyzed interobserver variability in gross tumor volume ( gtv ) delineation for hcc . patients and methods twelve radiation oncologists specializing in liver malignancy participated in a multi - institutional contouring dummy - run study of nine hcc cases and independently delineated gtv on the same set of provided computed tomography images . 
wir analysierten die interobservervariabilitt in abgrenzung zum makroskopischen tumorvolumen ( gtv ) beim hcc . patienten und methoden in einer institutsbergreifenden konturierenden teststudie mit 9 hcc - fllen beschrieben 12 strahlentherapeuten das gtv anhand des gleichen satzes von zur verfgung gestellten computertomogrammen . die quantitative analyse wurde unter verwendung eines expectation - maximization - algorithmus fr die simultaneous truth and performance level estimation ( staple ) in verbindung mit einer zwischen den rzten vereinbarten berechnung von kappa - statistiken durchgefhrt . 
um die interobservervariabilitt der gtv - abgrenzung zu bestimmen , wurden das verhltnis des tatschlich abgegrenzten volumens zum geschtzten konsensvolumen ( staple ) , das verhltnis des gemeinsamen volumens zum umfassenden volumen sowie der variationskoefzient berechnet . ergebnisse das mediane kappa - agreement - level betrug 0 , 71 ( spanne 0 , 280 , 86 )  . 
der variationskoefzient fr die gtv - abgrenzung lag im bereich von 857 % ( mittelwert 26 % )  . schlussfolgerung die interobservervariabilitt in der zielabgrenzung des hcc - gtv ist in dieser studie bemerkenswert . 
institutsbergreifende studien fr eine hcc - strahlentherapie erfordern geeignete qualittssicherungsprogramme fr die zielabgrenzung . schlsselwrter risikoorgane strahlentherapie chemoembolisation radiofrequenzablation qualittssicherung there has been increasing use of external beam radiotherapy ( ebrt ) for localized treatment of hepatocellular carcinoma ( hcc ) with both palliative and curative intent [ 1 ]  . ebrt has also been used in combination with transarterial chemoembolization ( tace ) and radiofrequency ablation ( rfa ) [ 2 ]  . 
quality control of target delineation in primary hcc is essential to deliver adequate doses of radiation to the primary tumor , while preserving adjacent healthy organs [ 2 ]  . 
it still remains to be veried whether contouring agreement would still hold when a variety of clinical cases are presented . the purpose of this multi - institution dummy - run study was to quantify the interobserver variability in gtv delineation for nine hcc cases presenting with various tumor characteristics . patients and methods in november 2012 , the korean radiation oncology group ( krog ) established a multicenter study to analyze the interobserver variability in gtv delineation for primary hcc in ebrt ( krog 1207 )  . 
all datasets were fully anonymized before being delivered to the participating centers . this study protocol conformed to the ethical guidelines outlined in the 1975 declaration of helsinki and was approved by the institutional review boards of participating institutions . case histories clinical information of nine selected patients is presented in supplementary table 1 . 
an inltrative and illdened tumor margin was present in patients 4 , 5 , 6 , and 9 . 716 strahlenther onkol ( 2016 ) 192 : 714721 diagnostic multiphasic ct images were provided in four cases , whereas mri images were provided for all patients . image acquisition the planning ct scan was obtained using a standard acquisition protocol ( arterial phase contrast - enhanced , supine position , both arms above the head , free breathing , and slice thickness of 5 mm ) using a somatom sensation open ( siemens medical , erlangen , germany ) ct scanner [ 4 ]  . 
the slice thickness was 3 mm in patients 1 and 2 . two - dimensional ( 2d ) uoroscopy was acquired in every hcc patient to evaluate respiratory movement of the diaphragfour - dimensional ( 4d ) ct simulation using respiratory gating system 3.0 ( anzai medical , tokyo , japan ) was acquired in the case of hypofractionated radiotherapy or respiratory movement of the diaphragm on 2d uoroscopy over 11.5 can abdominal compression device was used in the case of hypofractionated radiotherapy or respiratory movement of the diaphragm on 2d uoroscopy over 11.5 cif there was no improvement of respiratory movement of the diaphragm on 2d uoroscopy with an abdominal compression device , an abdominal compression device was not applied in that case . 
diagnostic liver mri ( magnetom tim trio , siemens healthcare ; achieva , philips healthcare , eindhoven , netherlands ) in gadoliniumenhanced t1 - weighted volumetric interpolated breath - hold examination ( vibe ) at arterial phase ( 2035 s ) and t1weighted vibe at hepatobiliary delayed phase ( 20 min ) were provided for all nine patients . target delineation patient histories and the ofcial radiographic interpretation of mri were provided to the panelists to aid decision making in identication of gtv . 
the dimensionless coefcient of variation ( % ) , dened as the ratio between the standard deviation and the mean , was calculated to measure the relative data scatter with respect to the mean [ 9 ]  . 
due to the small volume , small inaccuracies in outlining the tumor had an amplied impact on the ultimately delineated gtv . in patient 2 , residual tumor after incomplete tace did not show clear enhancement on the contrast - enhanced arterial phase planning ct scan . 
coregistered mri images did not align well with planning ct images due to differences in patient positioning during image acquisition , resulting in noteworthy liver deformation ( supplementary gure 2 )  . in patient 4 , ill - dened and inltrative perivascular mass formation ( in the right upper anterior pvt ) likely contributed to the variability . 
1 box - and - whisker plots of the ratio of true contoured gross tumor volume ( gtv ) to the 95 % condence level ( s95 ) for each of nine patients . 
the box spans the rst to the third quartile ; the line inside each box shows the median values and the upper and lower whiskers indicate the range ing ct - mri fusion for gtv delineation was the positional difference of the liver between ct and mri images . 
the tumor had a relatively well - demarcated margdiagnostic multiphasic ct images were provided ( supplementary gure 5 )  . observers 3 , 5 , 7 , and 9 contoured the gtv 20 % smaller than the s95 in six , four , six , and four cases , respectively . observer 3 contoured the gtv 10 % smaller than the s95 in all nine cases . 
observers 1 , 3 , 7 , 8 , and 9 had experience with more than 100 cases of hcc irradiation in their lifetime . discussion all institutions that participated in the current study are located in hcc - endemic areas , and the radiation oncologists had abundant clinical experience in treating hcc . 
nonetheless , our results indicate substantial variation in gtv delineation among radiation oncologists from different institutions , especially in four cases . factors that may have been associated with the largest variation include absence of diagnostic multiphasic ct , tumor location adjacent to the previous treatment with tace or rfa , pvt , and small tumor size . ill - dened inltrative tumor margin , extensive diagnostic multiphasic ct images were provided for patients 2 , 5 , 7 , and 9 . 
lipiodol deposit after transarterial chemoembolization ( tace ) presented with high - density nodule stitution study and consensus meeting discussion may help in improving frequent errors and disagreements [ 12 ]  . of target delineation related to the respiratory motion and mri acquisition position . another issue is utilization of imaging studies in target delineation . 
coregistration of mri improved the accuracy of gtv delineation greatly in radiotherapy for many tumors , including prostate cancer [ 13 ] , head and neck cancer [ 14 ] , and brain tumors [ 15 ]  . 
several motion management strategies are employed in order to compensate for the respiratory - dependent motion of the liver , including abdominal compression to reduce the breathing motion , treating during repeated breath holds , gating radiotherapy , and real - time tumor tracking [ 17 ]  . in designing a radiotherapy protocol for a multi - institution study , it is important to minimize technical requirements , while maintaining quality control of the treatment protocol . 
investigators need to be aware of the technologies available at participating institutions . recent studies have shown that the mri deformable registration technique for liver can improve the accuracy of tumor delineation [ 18 ]  . 
further investigations of liver mri deformable registration may help in improving the accuracy consultation with a diagnostic hepatobiliary radiologist is encouraged to improve the accuracy of target delineation [ 3 ]  . 
in particular , discussion with a diagnostic radiologist may help in targeting recurrent tumor adjacent to the previous tace and rfa treatment area , as well as tumor with extensive pvt . introduction of 4d - ct has improved respiratory management of tumors in the abdomen and thorax [ 19 , 20 ]  . however , acquiring 4d - ct images with intravenous ( iv ) contrast is not practical , since 4d - ct may take up to 1 min or more and administration of multiple doses of iv contrast may be necessary . 
4dct scanning was performed only in the region containing the liver in cine mode for at least one complete breathing cycle , while the iv contrast was synchronized with the 3d image acquisition [ 21 ]  . 
the impact of multiphasic ct images may have been more pronounced for tumors with less clear margins 720 strahlenther onkol ( 2016 ) 192 : 714721 and may have further reduced interobserver variability . 
to reduce interobserver variability for future prospective studies , a protocol for acquiring high - quality planning ct images in addition to implementing the breath - hold technique and reduced slice thickness , is required . 
consensus meeting is encouraged to discuss guidelines for contouring gtv , ctv , and ptv prior to developing multi - institutional study protocols involving radiotherapy for hcc . conclusion in the current study , the interobserver variability in the target delineation of gtv for primary hcc was noteworthy . to reduce this variability , the authors plan to evaluate the variability further and come up with a consensus guideline as an extension to this study in the near future . 
in designing a multi - institution study of radiotherapy for primary hcc , clear guidelines and appropriate quality assurance of target delineation are necessary . acknowledgements this work was supported by a grant ( 0620390 ) from the national r&d program for cancer control , ministry of health and welfare , republic of korea . compliance with ethical guidelines conict of interest y.s. 
seong declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
struikmans1 , 6 received : 24 march 2016 / accepted : 15 july 2016 / published online : 17 august 2016 springer - verlag berlin heidelberg 2016 abstract purpose the aim of this prospective longitudinal study was to compare coronary artery calcium ( cac ) scores determined before the start of whole breast irradiation with those determined 3 years afterwards . patients and methods changes in cac scores were analysed in 99 breast cancer patients . 
therefore , breath - hold probably prevents the development of radiation - induced coronary artery disease . however , the sample size of this study is limited and the follow - up period relatively short . keywords breast cancer coronary artery disease coronary arteries cardiovascular disease atherosclerotic plaque geringe zunahme ct - basierter kalziumwerte der koronararterien wirkung drei jahre nach brusterhaltender radiotherapie unter atemanhalt zusammenfassung ziel das ziel dieser prospektiven langzeitstudie war der vergleich der coronary - artery - calcium - ( cac - ) werte vor beginn der brustbestrahlung mit den werten nach 3 jahren . patienten und methoden nderungen der cac - werte wurden bei 99 brustkrebspatienten analysiert . 
drei gruppen wurden untersucht : patienten nach linksund rechtsseitiger strahlentherapie sowie mit bestrahlung unter atemanhalt . wir analysierten die gesamt - cac - werte sowie die cacwerte der vorderen linken absteigenden ( left anterior descending , lad ) und der rechten koronararterie ( right coronary artery , rca )  . 
zwischen den drei gruppen wurden auch die vernderungen der cac - werte der lad mistrahlenther onkol ( 2016 ) 192 : 696704 nus der rca - werte fr jeden einzelnen patienten verglichen . ergebnisse drei jahre nach brustbestrahlung mit atemanhalt wurde eine gering ausgeprgte erhhung der cacwerte zur kenntnis genommen . 
patienten mit linksseitigem brustkrebs , die ohne atemanhalt behandelt wurden , hatten einen hheren lad - minus - rca - wert als patienten mit rechtsseitigem brustkrebs und als jene mit linksseitigem brustkrebs mit atemanhalt . schlussfolgerung atemanhalt zusammen mit einer brusterhaltenden radiotherapie fhrt zu einem geringen anstieg der ct - basierten cac - werte . 
allerdings ist die stichprobengre dieser studie begrenzt und die follow - up - periode relativ kurz . schlsselwrter brustkrebs koronare herzerkrankung koronararterien herz - kreislauf - erkrankungen artherosklerotische plaque introduction radiotherapy for left - sided breast cancer has been associated with an increased risk of coronary artery disease ( cad ) [ 1 , 2 ]  . 
 [ 4 ] found a higher amount of calcium deposits in the left anterior descending ( lad ) coronary artery after radiotherapy for left - sided compared to radiotherapy for right - sided breast cancer . 
in another study cac scores , when compared with 11 other newer coronary heart disease risk markers , appeared to be the best predictors of the occurrence of cardiovascular disease in persons who were initially without cad [ 8 ]  . to the best of our knowledge , no studies have been performed comparing the amount of cac before and after radiotherapy in breast cancer patients . 
the aim was to identify possible differences in cac scores between patients irradiated for right - sided and patients irradiated for left - sided breast cancer ( with and without using a breath - hold technique )  . methods and materials patients patients with either ductal carcinoma in situ ( dcis ; < 4 cm ) or breast cancer ( < 5 cm ) and treated with breast - conserving surgery and whole breast radiotherapy were considered eligible . 
every eligible patient referred to our department was asked to participate in this study and ultimately 70% agreed to participate . from 20082011 , 109 consecutive patients were included in this prospective study . 
from january 2010 onwards , the active breathing control ( abc ) breath - hold method [ 9 , 10 ] was used in all left - sided breast cancer patients . this population consisted of three groups : 21 patients treated with left - sided radiotherapy ( group l - bh ) before january 2010 ; 23 patients treated with right - sided radiotherapy ( group r ) ; 65 patients treated with left - sided radiotherapy using a breath - hold technique ( group l + bh )  . subsequently , from october 2010 hypofractionation schemes were routinely administered [ 11 , 12 ]  . 
cac was measured using noncontrast , low - dose nongated cardiac ct studies on a ge 64 - slice mdct scanner ( lightspeed vct , general electric medical system , milwaukee , wi ; usa )  . 
we compared the distribution of these three risk groups over time between each of the three patients groups : r , l - bh , and l + bh . radiotherapy radiotherapy details were described previously [ 10 ]  . 
total doses were 50 gy in 25 fractions for the conventionally fractionated cases and 42.56 gy in 16 fractions for the cases irradiated with a hypofractionation scheme . if indicated according to the national guidelines , a boost dose , using a photon based 3d - crt technique , was added to the tumor bed . 
this boost was given after completion of the whole breast irradiation ( table 1 )  . risk factors the following variables were obtained before starting radiotherapy : age , height , body mass index ( bmi ) , postmenopausal status , smoking habits . 
this , within patient evaluation , prevents a patient - related risk factor bias , by representing the differences in each individual patient . the rca is the coronary artery that receives the lowest dose when administering whole breast radiotherapy , since the rca is furthest away from the radiation treatment elds , both in left - sided as well as right - sided breast cancer radiotherapy . 
therefore , this artery was used as a reference . statistical analysis a descriptive analysis of the change in time of the cac scores was carried out , reporting the following values : mean , median , and the standard error ( se )  . 
p - values ( cid : 2 ) 0.05 ( two - sided ) were considered statistically signicant . strahlenther onkol ( 2016 ) 192 : 696704 results general patient characteristics and risk factors for all 109 women , a baseline absolute cac score was calculated . 
hence , after 3 years of follow - up , in 99 women both a baseline and a follow - up absolute cac score were available ( see table 3 for the range when the follow - up calcium ct scan had taken place )  . the mean age of the patients was 56 years ( range 2874 years )  . 
patient , treatment characteristics , and risk factors per group are summarized in table 1 and 2 . the mean bmi in the rcwest cohort was 26 ( range 1839 ) , corresponding with overweight on the bmi scale [ 15 ]  . 
in addition 17% in our cohort had a bmi higher or equal to 30 , corresponding with obesity on the bmi scale [ 15 ]  . one patient had experienced a cardiac arrest in the past and two reported that they had experienced signs of angina pectoris in the past . 
after 3 years , only a small nonsignicant shift was found in the cac risk distribution ( p > 0.1 ; table 3 )  . the mean overall absolute cac score at baseline was 52 with a range of 0825 . 
therefore , these ndings are reassuring that the statistical analyses are sufciently reliable . cac scores : lad minus rca at baseline we found a mean lad minus rca absolute cac score of 3 ( sd 48 ) , 37 ( sd 100 ) and 8 ( sd 60 ) for the r , l - bh , and l + bh groups , respectively . 
three years after radiotherapy we found a mean lad minus rca absolute cac score of 11 ( sd 97 ) , 47 ( sd 157 ) , and 5 ( sd 74 ) for the r , l - bh , and l + bh groups , respectively . smaller differences were observed in patients treated for left - sided breast cancer with breath - hold ( l + bh ) compared to left - sided breast cancer patients treated without a breathhold technique ( l - bh )  . 
3 shows the mean differences in lad minus rca scores between baseline and 3 years after radiotherapy . discussion in this prospective longitudinal study , we found a less pronounced increase in cac scores in patients with left - sided radiotherapy when using a breath - hold technique compared to those with left - sided radiotherapy without breath - hold . 
2 plotted data ( regression lines ) of the three treatment groups : left - sided radiotherapy ( l - bh , blue line ) , right - sided radiotherapy ( r , red line ) and left - sided radiotherapy with breath - hold technique ( l + bh , green line )  . 
the increased cac scores 3 years after radiotherapy , administered without a breath - hold technique , are indicative for a more pronounced development of ( radiation - induced ) atherosclerosis . 
therefore , age was not added to the model and does not appear to be a confounder . finally , as we found in 2012 that 98 % of all 192 patients completed the full course of this breath - hold based radiotherapy technique without experiencing any problem or delay [ 22 ] , in our opinion the radiotherapy compliance , with and without breath - hold , was not biased by age . 
this nding was conrmed in other studies as well [ 9 ]  . drawbacks were the limited sample size of our cohort and the relatively short follow - up period of 3 years . 
however , in order to avoid missing relevant information after a short follow - up as well , we wanted to assess the radiation - induced coronary artery effects at an earlier ( presymptomatic ) stage . 
no such studies have been published before . specically since the individual differences were evaluated in several patient groups , the results of our study might give insight in the inuence of radiation therapy which was performed according to the latest dutch standards . 
in this study , no baseline cac scores were determined ; and the control group consisted of nonirradiated patients who were referred for ct angiography of the precranial arteries due to the suspicion of a recent stroke or transient ischemic attack [ 5 ]  . 
did not nd increased calcium scores in left - sided breast cancer patients . the latter was probably due to the fact that most of them had a calcium score of zero ; also in this study , no baseline cac values were available . another drawback of our study is that we did not investigate the relation between the amount of cac and the dose levels delivered to the heart and the lad for each individual patient . 
moreover , the three cohorts represented daily practice . a strong point of our study is that the ct - based cac score is known for its highly predictive value of developing [ 29 ] reported the cardiac vascular events . 
the biological effective breast doses were identical [ 1921 ]  . with respect to the design of our study we chose to prospectively compare the changes of the cac scores in time for the three groups of patients : r , l - bh , and l + bh . this design is debatable , since we did not randomize between using a breath - hold radiotherapy technique or not . for this we had two reasons : rst , our aim was to compare the results of the l - bh and l + bh group with those of right - sided breast cancer patients , being irradiated without breath hold ; second , the consecutive inclusion of study patients treated without breath - hold ( group r and l - bh ) started in 2009 . 
after in 2010 routinely was started to treat patients with a breath - hold technique it seemed unethical to randomize them and thus refrain half of the patients from a breath - hold technique . 
we also felt that a phase iii setting would have resulted in a low accrual rate because patients probably would have preferred the breath - hold based treatment . concerning the observed statistically signicant differences of mean ages between the l - bh and l + bh group ( table 1 ) , in may 2010 we also started to use a single fraction , intraoperative radiotherapy ( iort ) , treatment while recruiting patients for our cac study . 
they found that a low cac value was associated with higher survival rates in all ages . in a systematic review , it was stated that the absence of an increased cac score was associated with a low risk of future cardiovascular events [ 30 ]  . a potential drawback is the differences of the cac scores zero between the three groups . 
the latter prevented a patient - related risk factor bias , as the value represents the differences in cac scores in the individual patient . conclusion breath - hold in breast - conserving radiotherapy results in less increase over time of ct - based cac scores . 
however , the sample size of this study is limited and the follow - up period is relatively short . acknowledgements we thank the patients for participating in this study ; the radiation oncologists : j . 
wiggenraad for including patients in this study ; the medical receptionists for arranging the appointments for the calcium ct scans ; colleagues of the radiology department in mch antoniushove for arranging and performing the calcium ct scans ; i . 
struikmans state that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
august 2016 springer - verlag berlin heidelberg 2016 hintergrund und fragestellung die einzige kurative therapie fr patienten mit einem psa - rezidiv ( prostataspezisches antigen ) nach radikaler prostatektomie besteht in der sog . 
allerdings erleiden bis zu 75 % der patienten nach rt einen erneuten biochemischen oder klinischen rckfall innerhalb von 5 jahren . risikofaktoren fr ein therapieversagen sind ein frher wiederanstieg der psa - werte , eine kurze psa - verdoppelungszeit , ein hoher psa - wert bei der einleitung der rt , ein gleason - score > 7 und pt3b . 
die vorliegende getug - afu 16 ist die erste studie , die prospektiv den stellenwert der kombination der salvage - rt mit einer kurzzeit - aht beim biochemischen rezidiv prft . studienziel und - design ziel der prospektiv randomisierten studie war der nachweis , dass eine kurzzeit - aht das biochemische oder klinische progressionsfreie berleben originalpublikation carrie c , hasbini a , de laroche g et al ( 2016 ) salvage radiotherapy with or without short - term hormone therapy for rising prostate - specic antigen concentration after radical prostatectomy ( getug - afu 16 ) : a randomised , multicentre , open - label phase 3 trial . 
einschlusskriterien waren patienten nach prostatektomie bei einem adenokarzinom pt24a ( blasenhalsinltration ) und pn0 / cn0 , deren psa - wert nach der operation fr mindestens 6 monate auf < 0 , 1 ng / ml abgefallen und anschlieend in 2 konsekutiven messungen wieder auf werte zwischen 0 , 22 ng / ml angestiegen war . 
die pelvinen lymphabsse wurden in 16 % bis 46 gy bestrahlt , und zwar bei patienten , die primr bei der prostatektomie nicht pelvin lymphadenektomiert wurden und ein befallsrisiko > 15 % nach partin hatten . 
als biochemisches rezidiv galten ein psa - anstieg ber den nadir + 0 , 5 ng / ml , der nach 2 monaten durch eine weitere mes742 strahlenther onkol ( 2016 ) 192 : 741744 sung besttigt wurde , oder ein klinisch fassbarer rckfall . die behandlung eines weiteren rezidivs nach salvage - rt war nicht bestandteil des studienprotokolls . 
primrer studienendpunkt war das ( biochemische und klinische ) progressionsfreie berleben , sekundre endpunkte waren das gesamtberleben , die zeit zwischen randomisation und psa - nadir , akute und spte toxizitt ( nach common toxicity criteria , ctc ) sowie vernderungen der lebensqualitt . ergebnisse zwischen oktober 2006 und mrz 2010 wurden 743 patienten in 43 franzsischen zentren eingeschlossen : 373 in den kontrollarm und 369 in den kombinationsarm mit aht . 
dieser unterschied hatte sich aber noch nicht auf das gesamtberleben ausgewirkt : das mediane berleben betrug in beiden gruppen 58 monate , die 5 - jahres - berlebensrate 95 % vs . 
prdiktiv fr einen progress waren in der multivariaten analyse der psa - wert bei einleitung der rt ( > 0 , 5 ng / ml verdoppelte das risiko in beiden gruppen ) , ein r1 - status , die psa - verdoppelungszeit und ein samenblasenbefall . 
interessanterweise erhhte die aht in der subgruppenanalyse die progressionsfreiheit sowohl bei patienten mit low - risk - erkrankung ( von 75 % in der kontrolle auf 87 % ) als auch bei jenen mit high - risk - erkrankung ( von 58 % auf 77 % )  . 
erwartungsgem litten die patienten akut whrend der aht unter hitzewallungen ( grad 1 / 2 : 45 % , grad 3 : 1 % ) und schwitzen ( grad 1 / 2 : 13 % )  . 
sexuell aktiv waren bei einschluss in die studie in der kontrollgruppe im vergleich zur aht 51 % ( 46 % ) , nach 1 jahr noch 48 % ( 30 % ) und nach 5 jahren 52 % ( 46 % )  . 
statistische unterschiede ergaben sich dabei nicht , doch muss insbesondere bei der lngeren nachbeobachtung eine niedrige antwortrate teilweise nur von 25 % der kollektive bercksichtigt werden . schlussfolgerungen der autoren die kombination von salvage - rt mit kurzzeit - aht verbessert das progressionsfreie berleben signikant und verzgert damit die einleitung einer aggressiveren therapie . 
in zusammenschau mit den zwischenergebnissen der rtog - studie 9601 ist die kombinationstherapie beim psa - rezidiv eine sinnvolle option . kommentar da das progressionsfreie berleben nach 5 jahren durch die kombination von rt mit einer kurzzeit - aht tatschlich um ber 15 % gesteigert wurde , knnen die ergebnisse als statistisch abgesichert eingestuft werden . 
dieses ergebnis passt in das bild der erhhung der effektivitt der rt durch die aht in der konservativen therapie des prostatakarzinoms , welche in vielen randomisierten studien eindrucksvoll nachgewiesen werden konnte [ 1 ]  . 
letztlich wre auch nicht verstndlich , warum sich tumorzellen , die nach einer operation im krper des patienten verblieben sind , biologisch anders verhalten sollten als tumorzellen bei patienten , die zuvor keiner prostatektomie unterzogen wurden . 
allerdings ist der molekularbiologische mechanismus dieser klinisch eindeutigen radiosensibilisierung noch weitgehend unverstanden [ 2 ]  . in der bislang nur als abstracts publizierten rtog 9601 wurde ebenfalls die effektivitt einer kombination von rt ( 64 , 8 gy ) mit aht in der salvage - situation geprft [ 3 ]  . allerdings wurde in dieser studie eine langzeit - aht ber 2 jahre mit bicalutamid 150 mg whrend und nach der rt eingesetzt . 
das patientenkollektiv unterschied sich von der getug - afu 16 insofern , als dass in der rtog - studie auch patienten mit inadquatem psa - abfall nach prostatektomie eingeschlossen wurden ; ein postoperatives erreichen eines nullwerts war also nicht zwingend . 
allerdings entwickelten 70 % der patienten innerhalb der 2 jahre 150 mg bicalutamid eine gynkomastie . andere randomisierte studien prften den stellenwert einer aht in vergleichbaren klinischen situationen , haben aber entweder noch keine ergebnisse publiziert oder rekrutieren noch : die eortc 22043 - 30041 war zwar initial nur fr die adjuvanz bei pt2r1 oder pt3r0 / 1 mit einem psa - abfall nach operation ( cid : 2 ) 0 , 2 ng / ml ausgelegt [ 4 ]  . 
bei schlechter rekrutierung wurde sie jedoch auch fr earlysalvage - patienten ( psa 0 , 4 ng / ml ) geffnet und konnte dann ihr rekrutierungsziel erreichen [ 5 ]  . 
ergebnisse liegen aber noch nicht vor . mit fast 1800 patienten anfang 2015 hat auch die rtog 0534 spport ihr rekrutierungsziel erreicht [ 6 ]  . eingeschlossen wurden hier patienten mit pt2 / 3 pn0 / x cm0 , gleason ( cid : 2 ) 9 sowie einem psa 0 , 1 ng / ml und < 2 ng / ml 6 wochen postoperativ . 
randomisiert wurde in 3 gruppen : im kontrollarm wurde nur das prostatabett normofraktioniert zwischen 64 , 8 bis 70 , 2 gy bestrahlt ; in arm b wurde eine aht 2 monate vorher begonnen und insgesamt ber 46 monate gegeben ; in arm c wurden zustzlich die pelvinen lymphabsse bis 45 gy bestrahlt . die grte studie , die zur beantwortung der frage nach der optimalen dauer der aht bei der salvage - rt wird beitragen knnen , ist die aktuell in uk , kanada und dnemark rekrutierende mrc - studie radicals ( radiotherapy and androgen deprivation in combination after local surgery , [ 7 ] )  . 
die studie besteht aus zwei substudien : radicals - rt randomisiert die adjuvante rt gegen eine early - salvage - rt ( 2 konsekutive anstiege auf > 0 , 1 ng / ml oder 3 konsekutive anstiege ) , whrend radicals - hd diese patienten randomisiert zwischen 0 vs . 
deshalb sind bereits jetzt metaanalysen mit den anderen studien zu dieser fragestellung im protokoll vorgesehen . in der zusammenschau der aktuell verfgbaren evidenz ist eine steigerung der effektivitt der salvage - rt durch eine aht beim biochemischen rezidiv des initial nodal - negativen prostatakarzinoms sehr wahrscheinlich . 
die nachbeobachtungszeit ist noch zu kurz , um effekte quo ad vitam analysieren zu knnen . subgruppenanalysen der rtog 9601 mit den endpunkten gesamtberleben und metastasierung sind zwar vorgesehen , liegen aber noch nicht vor . 
in der sakk 09 / 10 der schweizerischen arbeitsgemeinschaft fr klinische krebsforschung wurden 350 patienten mit einer bestrahlung des prostatabetts zwischen 64 und 70 gy randomisiert [ 8 ]  . 
ergebnisse hinsichtlich der onkologischen effektivitt wurden bislang noch nicht publiziert . 744 strahlenther onkol ( 2016 ) 192 : 741744 jedoch liegt in analogie zur primrsituation eine dosis - wirkungs - beziehung auch bei der salvage - rt nahe . inwieweit diese mglichen effekte durch die hinzunahme der aht weiter verstrkt werden , ist aktuell nicht absehbar . 
studien ( rtog 0534 spport , eortc 22043 - 30041 ) hinweise auf diese frage geben knnen . die zeitnahe beantwortung einiger dieser fragen ist vermutlich erst mglich , wenn die besagten studien weitere ergebnisse verffentlicht haben . 
basierend auf den ergebnissen der getug - afu 16 und der rtog 9601 sollte patienten mit einer lebenserwartung von ber 10 jahren , ohne relevante komorbiditt und mit einer high - risk - konstellation die kombinationstherapie im rahmen individueller konzepte angeboten werden , allerdings nach aufklrung ber die aktuell noch limitierte datenlage . fazit die kommentierte getug - afu - 16 - studie zeigt eine signikante verbesserung des progressionsfreien berlebens , wenn die salvage - rt mit 66 gy bei biochemischem rezidiv mit einer kurzzeit - aht ( 6 monate ) kombiniert wurde . 
davon protierten alle analysierten subgruppen ( sowohl mit low - riskals auch mit high - risk - erkrankung , unabhngig vom alter und der psa - verdoppelungszeit )  . fr die beurteilung des effekts auf das gesamtberleben reichte die nachbeobachtung noch nicht aus . rtog 9601 berichtete fr ein hnliches kollektiv sogar eine verbesserung des gesamtberlebens , wenn die rt mit 2 jahren aht ( bicalutamid ) kombiniert wurde . 
in dieser studie litten allerdings viele patienten unter gynkomastie . derzeit kann die kombinationstherapie aufgrund der vorliegenden daten noch nicht generell empfohlen werden , da die nachbeobachtungszeit noch zu kurz ist und die ergebnisse weiterer laufender studien zu dieser frage abgewartet werden mssen . 
weiterhin ist der effekt der dosiseskalation > 66 gy noch nicht absehbar . allerdings sollte zumindest patienten mit noch langer lebenserwartung und einer high - risk - konstellation ( gleason score 8 , samenblasenbefall , psa - verdoppelungszeit < 6 monate ) die kombinationstherapie als individuelles konzept angeboten werden . robert michael hermann , westerstede , und hans christiansen , hannover interessenkonikt r . 
hermann rm , schwarten d , fister s et al ( 2007 ) no supra - additive effects of goserelin and radiotherapy on clonogenic survival of prostate carcinoma cells in vitro . 
shipley wu , pugh sl , lukka hr et al ( 2016 ) rtog 9601 , a phase iii trial in prostate cancer patients : anti - androgen therapy ( aat ) with bicalutamide during and after salvage radiation therapy ( rt ) following radical prostatectomy ( rp ) and an elevated psa . 
ghadjar p , hayoz s , bernhard j et al ( 2015 ) acute toxicity and quality of life after dose - intensied salvage radiation therapy for biochemically recurrent prostate cancer after prostatectomy : rst results of the randomized trial sakk 09 / 10 . 
august 2016 springer - verlag berlin heidelberg 2016 hintergrund sehr junges alter ( nach allgemeiner denition 3540 jahre ) ist wohl infolge besonders aggressiver tumoren ( rezeptornegativ , her - 2neu - positiv , triple - negativ , g3 ; [ 6 ] ) mit einer schlechteren prognose assoziiert . 
in retrospektiven analysen und auch in prospektiven studien wurde vor allem ein hohes risiko fr lokoregionale rezidive nach brusterhaltender therapie ( bet ) gefunden [ 3 , 4 ]  . 
beispielsweise war in den studien der european organisation for research and treatment of cancer ( eortc ) das risiko fr intramammre rezidive nach bet um den faktor 2 , 8 gegenber postmenopausalen patientinnen erhht [ 2 , 8 ]  . 
dennoch whlen viele sehr junge patientinnen primr eine mastektomie , um das psychologische trauma eines rezidivs zu vermeiden [ 9 ]  . patienten die analyse basiert auf daten des niederlndischen krebsregisters und beinhaltet 1000 patientinnen mit unilateralem mammakarzinom ( mc ) , die jnger als 35 jahre und von 20032008 behandelt wurden [ 1 ]  . 
das betraf sowohl lokale rezidive , deren frequenz bei behandlung in den jahren 20032004 noch 4 , 2 % betrug und auf 2 , 2 % in den behandlungsjahren 20072008 sank . 
die lokalrezidivrate betrug 3 , 2 % nach bet und 3 , 8 % nach mastektomie . schlussfolgerung der autoren die lokalrezidivraten sind insgesamt niedrig , aber vom subtyp abhngig . kommentar originalpublikation aalders kc , postma el , strobbe lj et al ( 2016 ) contemporary locoregional recurrence rates in young patients with early - stage breast cancer . 
man kann also auch sehr jungen patientinnen guten gewissens eine brusterhaltende therapie empfehlen . fazit in derselben ausgabe des journal of clinical oncology publizierten die herausgeber einen kommentar zu der hier besprochenen arbeit unter dem titel a rosier picture for young women with breast cancer [ 9 ]  . 
der titel bringt es auf den punkt : man darf nicht zu optimistisch sein , aber junges alter ist per se auch kein grund fr bertriebenen pessimismus . ren baumann und jrgen dunst , kiel interessenkonikt r . 
de bock gh , van der hage ja , putter h et al ( 2006 ) isolated locoregional recurrence of breast cancer is more common in young patients and following breast conserving therapy : long - term results of european organisation for research and treatment of cancer studies . 
elkhuizen ph , van de vijver hermans mjj et al ( 1998 ) local recurrence after breast - conserving therapy for invasive breast cancer : high incidence in young patients and association with poor survival . 
gnerlich jl , deshpande ad , jeffe db et al ( 2009 ) elevated breast cancer mortality in women younger than age 40 years compared with older women is attributed to poorer survival in early - stage disease . 
mahmood u , morris c , neuner g et al ( 2012 ) similar survival with breast conservation therapy or mastectomy in the management of young women with early - stage breast cancer . 
nixon aj , neuberg d , hayes df et al ( 1994 ) relationship of patient age to pathologic features of the tumor and prognosis for patients with stage i or ii breast cancer . 
voogd ac , nielsen m , peterse jl et al ( 2001 ) differences in risk factors for local and distant recurrence after breast - conserving therapy or mastectomy for stage i and ii breast cancer : pooled results of two large european randomized trials . 
in der studie soll geklrt werden , ob es auch die prognose von brustkrebspatientinnen verschlechtert . methode die autoren untersuchten die assoziation von nikotinabusus , vor und nach einer brustkrebsdiagnose , mit der letalitt in der collaborative breast cancer and womens longevity study , einer populationsbasierten prospektiven beobachtungsstudie , die in wisconsin , new hampshire und massachusetts durchgefhrt wurde . 
hierbei wurden relative risiken ( hr ) mit 95 %kondenzintervallen ( 95 % ki ) und auch der rauchstatus fr tod durch brustkrebs , durch krebs der atemwege ( lunge , kopf - hals - tumoren ) und durch andere tumorerkrankungen ermittelt . 
auch die hr fr atemwegsund kardiovaskulre erkrankungen wurde ausndig gemacht . ergebnisse whrend einer medianen beobachtungszeit von 12 jahren starben in dem untersuchten kollektiv insgesamt 6778 frauen , 2894 hiervon an brustkrebs . 
patientinnen , die 1 jahr vor der brustkrebsdiagnose rauchten , hatten , im vergleich zu patientinnen ohne nikotinanamnese , eine hhere wahrscheinlichkeit an ihrem karzinom zu sterben ( hr 1 , 25 ; 95 % ki : 1 , 131 , 37 ) , sowie fr den tod durch atemwegstumoren ( hr 14 , 48 ; 95 % ki : 9 , 8921 , 21 ) und auch fr andere atemwegs ( hr 6 , 02 ; 95 % ki : 4 , 557 , 97 ) und kardiovaskulren erkrankungen ( hr 2 , 08 ; 95 % ki : 1 , 802 , 41 )  . 
die10 % der frauen , die auch nach brustkrebsdiagnose weiterhin rauchten , starben mit hherer wahrscheinlichkeit an brustkrebs als patientinnen , die niemals geraucht haben ( hr 1 , 72 ; 95% ki : 1 , 132 , 60 )  . 
im vergleich zu patientinnen , die nach der brustkrebsdiagnose weiterhin rauchten , sank nach rauchstopp die letalitt durch brustkrebs ( hr 0 , 67 ; 95 % ki : 0 , 381 , 19 ) und atemwegstumoren deutlich ( hr 0 , 39 ; 95 % ki : 0 , 160 , 95 )  . schlussfolgerung der autoren fortgesetztes rauchen nach diagnose eines mammakarzinoms erhht die letalitt fr brustkrebs und andere tumorarten . originalpublikation passarelli mn , newcomb pa , hampton jm , trentham - dietz a , titus lj , egan km , baron ja , willett wc ( 2016 ) cigarette smoking before and after breast cancer diagnosis : mortality from breast cancer and smoking - related diseases . 
fortgesetztes rauchen hat , auch nach einer tumordiagnose , einen negativen einuss auf die prognose dieser tumorerkrankungen ( diskutiert in [ 1 ] )  . in der vorliegenden groen , prospektiven langzeitbeobachtungsstudie wird diese aussage fr patientinnen mit brustkrebs konkretisiert . 
fanden bei patientinnen , die vor der brustkrebsdiagnose rauchten , ein um 25 % hheres relatives risiko daran zu versterben , im vergleich 740 strahlenther onkol ( 2016 ) 192 : 739740 zu nichtraucherinnen . 
hier eingeschlossen war eine 33 %ige reduktion des relativen risikos fr tod durch brustkrebs ( grenzwertig , nicht signikant ) , eine 60 %ige reduktion bei karzinomen der atemwege und eine 20 %ige reduktion bei kardiovaskulren ereignissen . 
das risiko fr ischmische herzerkrankungen ist , vor allem nach linksseitiger bestrahlung aufgrund eines mammakarzinoms , bekannt [ 24 ]  . es erhht sich bei nikotinabusus [ 2 ]  . 
auch hier gilt die kombination aus nikotinabusus und strahlentherapie als besonders risikobehaftet [ 5 , 7 ]  . fazit insgesamt knnen patientinnen mit brustkrebs durch nderung ihres lebensstils ihr sterblichkeitsrisiko fr verschiedene krebsund kardiorespiratorische erkrankungen senken . die diagnose von brustkrebs rechtfertigt also keinesfalls eine vernachlssigung der prvention . auch den radioonkologen muss die unter umstnden deletre interaktion von nikotinabusus und strahlenfolgen jederzeit bewusst sein . clemens seidel und rolf - dieter kortmann , leipzig interessenkonikt c . 
correa cr , litt hi , hwang w - t , ferrari va , solin lj , harris ee ( 2007 ) coronary artery ndings after left - sided compared with right - sided radiation treatment for early - stage breast cancer . 
darby sc , ewertz m , mcgale p , bennet am , blom - goldman u , brnnum d et al ( 2013 ) risk of ischemic heart disease in women after radiotherapy for breast cancer . 
nilsson g , holmberg l , garmo h , duvernoy o , sjgren i , lagerqvist b et al ( 2012 ) distribution of coronary artery stenosis after radiation for breast cancer . 
berrington de gonzalez a , curtis re , gilbert e , berg cd , smith sa , stovall m et al ( 2010 ) second solid cancers after radiotherapy for breast cancer in seer cancer registries . 
morton lm , gilbert es , hall p , andersson m , joensuu h , vaalavirta l et al ( 2012 ) risk of treatment related esophageal cancer among breast cancer survivors . 
stovall m , smith sa , langholz bm , boice jd jr , shore re , andersson m et al ( 2008 ) womens environmental , cancer , and radiation epidemiology study collaborative group . 
eingeschlossen wurden patienten mit histologisch gesichertem nsclc im stadium iiia ( n2 ) sowie ausgewhlte patienten mit einem nsclc im stadium iiib ( tnm - klassikation von 1997 ; [ 1 ] ) , die als medizinisch und funktionell operabel eingestuft wurden und einen sehr guten allgemeinzustand ( ecog 01 ) aufwiesen . 
die induktionstherapie bestand aus 3 kursen chemotherapie ( cht ) mit cisplatin ( 50 mg / m2 an den tagen 1 und 8 ) und paclitaxel ( 175 mg / m2 an tag 1 alle 3 wochen )  . im anschluss erfolgte eine radiochemotherapie ( rct ) mit 45 gy ( 2 - mal 1 , 5 gy pro tag ) und simultaner gabe von cisplatin ( 50 mg / m2 an den tagen 2 und 9 ) und vinorelbin ( 20 mg / m2 an den tagen 2 und 9 )  . 
patienten in arm a erhielten eine boost - bestrahlung von 2026 gy ( 5 - mal 2 , 0 gy pro woche ) , patienten in arm b wurden operiert . 
primrer originalpublikation eberhardt we , pttgen c , gauler tc et al ( 2015 ) phase iii study of surgery versus denitive concurrent chemoradiotherapy boost in patients with resectable stage iiia ( n2 ) and selected iiib non - small - cell lung cancer after induction chemotherapy and concurrent chemoradiotherapy ( espatue )  . 
die 161 patienten ( 65 % ) , bei denen der tumor nach der induktionstherapie als resektabel eingestuft wurde , wurden randomisiert ( statt 300 geplanter patienten )  . stratiziert wurde nach tn - kategorie ( t13n2 ; t4n01 ; t13n3 ; t4n2 ) , geplanter prophylaktischer ganzhirnbestrahlung ( ja / nein ) und dem land des behandelnden zentrums ( deutschland ; andere lnder )  . 
somit sind sowohl die denitive rct als auch die induktionstherapie gefolgt von einer operation als therapieoption fr patienten mit einem resektablen nsclc im stadium iii akzeptabel . kommentar die espatue - studie widmet sich einer wichtigen fragestellung , dem stellenwert der operation nach induktionstherapie beim resektablen nsclc im stadium iii [ 2 ]  . 
nach ihren ergebnissen bringt die operation gegenber einer denitiven rct fr das os und das pfs keinen vorteil . strahlenther onkol ( 2016 ) 192 : 592594 zu hnlichen ergebnissen kommt die 2007 publizierte randomisierte eortc - 0841 - studie ( nsclc im stadium iiia - n2 ; [ 3 ] )  . 
die 5 - jahres - berlebensraten waren 16 % ohne operation und 14 % mit operation ( p = 0 , 60 )  . die 5 - jahres - raten fr das pfs waren identisch und betrugen etwa 12 % ( abgeschtzt anhand der kaplan - meierkurven ; p = 0 , 61 )  . 
allerdings sind beide studien aufgrund ihrer unterschiedlichen designs nur bedingt vergleichbar . in der eortc - studie bestand die induktionstherapie bei allen patienten ( n = 579 ) aus drei kursen einer alleinigen platinhaltigen kombinationschemotherapie [ 3 ]  . 
hier stellt sich die frage nach dem waruschlielich hatten ja studien bei nichtresektablem nsclc gezeigt , dass eine zustzliche vorgeschaltete cht gegenber der alleinigen rct keinen berlebensvorteil bringt [ 4 , 5 ]  . ferner erfolgte in der espatue - studie die strahlentherapie im rahmen der simultanen rct hyperfraktioniert , obwohl deren stellenwert nicht hinreichend geklrt ist . 
obwohl die autoren der espatue - studie ihr sehr intensives induktionsregime zuvor in einer phase - ii - studie untersucht hatten , hatte es einen experimentellen charakter [ 7 ]  . 
fr dieses regime sprechen die in der espatue - studie im vergleich zu anderen studien deutlich besseren 5 - jahres - berlebensund pathologischen komplettremissionsraten ( pcr , [ 3 , 8 ] )  . 
diese unterschiede knnen aber zum teil auch in der unterschiedlichen patientenauswahl begrndet sein . insgesamt stellt sich die frage , ob ein experimentelles regime wie das der espatue - studie geeignet ist , den stellenwert der operation beim resektablen nsclc im stadium iii in adquater weise zu untersuchen . 
nach der aktuellen datenlage scheint die denitive rct einer operation mit vorgeschalteter induktionstherapie nicht unterlegen zu sedieser aspekt muss mit den betroffenen patienten unter bercksichtigung der bestehenden unsicherheiten besprochen werden , um gemeinsam das ihren individuellen bedrfnissen und wnschen am ehesten entsprechende therapieregime festzulegen . fazit die espatue - studie untersuchte eine wichtige fragestellung , nmlich den stellenwert der operation nach induktionstherapie bei der behandlung des resektablen nsclc im stadium iii . 
eberhardt we , pttgen c , gauler tc et al ( 2015 ) phase iii study of surgery versus denitive concurrent chemoradiotherapy boost in patients with resectable stage iiia ( n2 ) and selected iiib nonsmall - cell lung cancer after induction chemotherapy and concurrent chemoradiotherapy ( espatue )  . 
meerbeeck jp van , kramer gw , van schil pe et al ( 2007 ) randomized controlled trial of resection versus radiotherapy after induction chemotherapy in stage iiia - n2 non - small - cell lung cancer . 
vokes ee , herndon j 2nd , kelley mj et al ( 2007 ) induction chemotherapy followed by chemoradiotherapy compared with chemoradiotherapy alone for regionally advanced unresectable stage iii non - small - cell lung cancer : cancer and leukemia group b . 
el - sharouni sy , kal hb , battermann jj , schramel fm ( 2006 ) sequential versus concurrent chemo - radiotherapy in inoperable stage iii non - small cell lung cancer . 
eberhardt we , gauler tc , lepechoux c et al ( 2013 ) 10 - year longterm survival ( lts ) of induction chemotherapy with three cycles cisplatin / paclitaxel followed by concurrent chemoradiation cisplatin / etoposide / 45 gy ( 1.5 gy bid ) plus surgery in locally advanced non - small - cell lung cancer ( nsclc ) - a multicenter phase - ii trial ( cistaxol )  . 
albain ks , swann rs , rusch vr et al ( 2009 ) radiotherapy plus chemotherapy with or without surgical resection for stage iii nonsmall - cell lung cancer : a phase iii randomised controlled trial . 
ren z , zhou s , liu z , xu s ( 2015 ) randomized controlled trials of induction treatment and surgery versus combined chemotherapy and radiotherapy in stages iiia - n2 nsclc : a systematic review and meta - analysis . 
eni ( ipsilateral level ii , ib and iii or bilateral ) needs to be proposed in selected patients , especially when snd has not been performed . keywords radiotherapy intensity - modulated radiotherapy chemotherapy treatment outcomes neck dissection sinunasales plattenepithelkarzinom ohne klinische lymphknotenbeteiligung welches halsmanagement ist das beste ? zusammenfassung zielsetzung ziel der arbeit war es , den klinischen verlauf von patienten mit einem sinunasalen plattenepithelkarzinom ( snscc ) retrospektiv zu untersuchen und die therapieergebnisse von elektiver halsbestrahlung ( eni , elective neck irradiation ) , selektiver operation ( snd , selective neck dissection ) und initialer chemotherapie bei klinischen lymphknotennegativen ( n0 ) patienten zu diskutieren . methoden die daten von 104 patienten mit metastasenfreiem snscc , die mit kurativer absicht behandelt worden waren , wurden retrospektiv analysiert . 
uniund multivariante analysen wurden verwendet , um prognostische faktoren fr das gesamtberleben ( os ) und fr die lokale tumorprogression ( lrc ) zu erheben . 538 strahlenther onkol ( 2016 ) 192 : 537544 ergebnisse die mediane nachbeobachtungszeit betrug 4 , 5 jahre . 
in diesem kollektiv hatten patienten mit snd eine signikant hhere lrc ( 94 % vs . 47 % ; p = 0 , 002 ) , nicht jedoch mit eni . schlussfolgerung snd bietet die mglichkeit , okkulte zervikale metastatische lymphknoten zu entdecken und eine elektive , postoperative rt zu ermglichen . 
eine eni ( ipsilaterale stationen ii , ib und iii oder bilateral ) sollte ausgewhlten patienten angeboten werden , vor allem wenn keine snd durchgefhrt wurde . schlsselwrter strahlentherapie intensittsmodulierte strahlentherapie chemotherapie behandlungsergebnis halsdissektion introduction sinonasal cancers are rare but aggressive tumours [ 1 , 2 ]  . they represent less than 5 % of all head - and - neck cancers and 0.5 % of all cancers . 
because of their location , tumours could easily spread to critical adjacent structures before becoming symptomatic , posing a therapeutic challenge as a result of advanced stage at the time of diagnosis [ 4 ]  . 
treatment modalities include a combination of surgical resection , when feasible , and / or external beam radiation therapy ( ebrt ) , while induction chemotherapy ( ict ) has been increasingly used for bulky disease [ 5 ]  . management of the neck in a disease without lymph node ( ln ) invasion ( n0 ) remains controversial due to the poor outcome of this population , with a relatively high incidence of neck relapse ( 4.320 % ) [ 6 , 7 ]  . 
selective neck dissection ( snd ) is usually considered for n0 neck when surgery is feasible for the primary disease , even though it is not considered as a gold standard [ 8 ]  . 
the role of prophylactic elective neck irradiation ( eni ) in n0 patients still remains unclear and controversial due to the difculty to select a subpopulation with sinonasal scc ( snscc ) with a higher risk of regional relapse ( rr ) [ 810 ]  . 
furthermore , the radiation volume is debated , including the ipsilateral or bilateral neck , level ii , ib and sometimes also iii [ 11 , 12 ]  . the aim of our study was to assess outcomes of a series of patients with nonmetastatic snscc and to discuss the impact of eni and snd in clinically n0 patients . patients and methods patients from january 1998 to december 2012 , 139 patients with histologically proven nonmetastatic snscc were recorded and treated with curative intent in gustave - roussy ( villejuif , france )  . 
exclusion criteria were previous treatment of the head - and - neck area ( radiotherapy : n = 3 , surgery : n = 1 ) , exclusive brachytherapy ( n = 2 ) , palliative care ( n = 6 ) , and non - scc histology ( n = 23 )  . 
the 2010 american joint committee on cancer ( ajcc ) tnm classication [ 13 ] was retrospectively used for staging . treatments and follow - up all patients have been referred to a multidisciplinary head and neck tumour board prior to treatment . 
ict was delivered for bulky primary disease with the objective of tumour downstaging to allow surgery or prior to concomitant chemoradiotherapy ( crt ) if surgery was contra - indicated . standard ict was administered in a median number of 3 cycles ( every 3 weeks : d1d21 ) and contained the association of ( tpf ) cisplatin ( 75 mg / m2 / day , intravenous , day 1 ) , 5 - uorouracil ( 5fu : 750 mg / m2 / day intravenous continuous infusion , days 14 ) and docetaxel ( 75 mg / m2 / day , day 1 ) [ 14 ]  . 
other associations were ( pf ) cisplatin5fu ( cisplatin 100 mg / m2 / day , intravenous , day 1 and 5fu 1000 mg / m2 / day intravenous continuous infusion , days 14 , respectively , d1d21 ) , or carboplatin5fu ( carboplatin 300 mg / m2 , intravenous , day 1 and 5fu 1000 mg / m2 / day , intravenous continuous infusion , days 14 , respectively , d1d28 ) [ 15 ]  . when feasible ( with the objective of ablative resection , without contra - indication of surgery or excessive surgical morbidity ) , patients underwent radical resection of the primary tumour with synchronous neck dissection , when ln were clinically positive . 
moreover , exclusive surgery of the primary tumour without ebrt could be performed in n0 patients , with or without snd . postoperative ebrt , with or without chemotherapy , was performed in most patients and exclusive ebrt was done when surgery was contra - indicated or unreasonable with high risk of morbidity . 
3d - conformal or intensity - modulated radiotherapy ( imrt ) were used . crt consisted in 3 cycles of cisplatin ( 100 mg / m2 / day , intravenous days 1 , 22 and 43 )  . 
other options were used in case of severe comorbidities ( carboplatin : auc 2 weekly , or cetuximab : 400 mg / m2 day 7 , followed by weekly intravenous 250 mg / m2 during ebrt )  . the tumour response was evaluated on ct , or mri when possible , after 2 cycles of ict ( recist 1.1 criteria ) and on histological ndings when surgery was performed [ 16 ]  . patients were rst assessed 3 months after the completion of the treatment by physical examination and head - andneck ct / mri imaging ; then by physical examination every 3 months for 2 years ( ct / mri imaging every 6 months ) , every 6 months until 5 years , and yearly thereafter . 
overall survival ( os ) , progression - free survival ( pfs ) , locoregional control ( lrc ) and distant control ( dc ) rates were estimated with kaplanmeier method . 
events were death from any cause for os , death or tumour progression for pfs , and death from the treated cancer or occurring after a relapse for disease - specic survival ( dss )  . 
variables associated with pfs or os with a p - value < 0.20 were included in the mva . in the cox model , continuous variables ( ps , t , n and age ) were dichotomized . 
standard ict , as previously described , was performed in 28 patients , with a median number of 3 cycles , and other associations were also performed including pf ( cisplatin or carboplatin5fu ; n = 20 ) , or other ( n = 11 )  . seventy - ve patients underwent surgery ( 72 % ) with radical resection of the primary tumour , and 37 / 75 ( 49.3 % ) underwent simultaneous neck dissection , of which 10 / 37 ( 27 % ) had clinically palpable neck nodes . 
exclusive surgical treatment without ebrt was performed in 14 patients ; all of them were n0 ( 5 t1 , 3 t2 , 2 t3 and 4 t4 , respectively ) , and 2 of them had snd . postoperative and exclusive ebrt , with or without chemotherapy , was performed on 60 ( 57.7 % ) and 30 patients ( 28.8 % ) , respectively . 
ebrt was delivered at a median dose of 64 gy ( range 2470 gy ) after surgery to the surgical bed and 70 gy ( range 2070 gy ) in case of exclusive treatment , to gross tumour volume and positive ln . 
1 overall survival ( os ) and progression - free survival ( pfs ) in the entire population were used ( n = 15 / 90 , 17 % )  . 
crt was delivered in 46 patients ( 44 % ) : 3 cycles ( range 13 ) of cisplatin , or other in case of severe comorbidities ( carboplatin : 14 or cetuximab : 7 )  . 
among them , 13 had postoperative combined modality treatment with prior ict . survival and relapse in the overall population at a median follow - up of 4.5 years , 57 patients ( 55 % ) had died . 
there was no signicant factor for dc ( including ict ) in the univariate analysis ( 14 events )  . cervical metastasis status at baseline and relapse of 104 patients , 17 ( 16 % ) had initial clinically positive ln ( n13 )  . 
of them , 2 , 3 and 12 patients had t12 , t3 and t4 classication at diagnosis , respectively ; 12 ( 70.6 % ) had cancer of maxillary sinus . 
the most common sites of rr were level ii ( n = 12 , 70.6 % ) , level iii ( n = 5 , 29.4 % , only 1 patient without positive ln in level ii ) , level ib ( n = 4 , 23.5 % ) , level v ( n = 3 , 17.6 % , all with positive ln in level ii or iii as well ) and retropharyngeal ln ( n = 1 , 5.9 % , level iii as well )  . total no relapse relapse lr + d total 104 ( 100 ) 57 ( 55 ) 47 ( 45 ) 33 ( 32 ) 4 ( 4 ) 10 ( 9.6 ) 87 ( 100 ) 48 ( 55 ) 39 ( 45 ) 27 ( 31 ) 4 ( 4.6 ) 8 ( 9 ) cn 13 17 ( 100 ) 9 ( 53 ) 8 ( 47 ) 6 ( 35 ) 0 ( 0 ) 2 ( 12 ) lr locoregional , d distant , cn clinical n classication at baseline table 6 number of clinically n0 patients with neck relapse according to neck radiation ipsilateral contralateral patients treated no eni ipsilateral bilateral eni total rt radiotherapy , eni elective neck irradiation , nr neck relapse clinically n0 population outcomes among the 87 ( 84 % ) clinically n0 patients , 57 patients were initially classied t4 . 
among 27 patients who had a snd , only 3 / 27 ( 11 % ) had pathologically positive ln ( table 2 )  . regarding the management of the neck : 28 / 87 ( 32 % ) had eni alone ( 21 bilateral and 7 ipsilateral ) , 10 ( 11.5 % ) had snd alone ( 3 bilateral and 7 ipsilateral ) , 17 ( 20 % ) had both snd ( 2 bilateral , 15 ipsilateral ) and eni ( 9 bilateral , 8 ipsilateral ) , and 32 ( 37 % ) had no neck treatment . among the 39 relapses , 27 / 39 ( 69 % ) were exclusively locoregional and 8 were associated with distant relapses ( dr ; table 5 )  . 
relapses were in the ipsilateral neck for 4 patients , bilateral for 3 and 1 contralateral alone ( table 6 )  . according to the management of the neck , no difference of os was found , but there was a signicant difference in lrc . 
only one patient who was initially treated with snd ( pathologically positive neck pn + ) followed by bilateral neck ebrt relapsed in the neck and none of the 24 patients who were treated with snd and with pathologically negative neck ( pn ) progressed in the neck . 
bilateral neck irradiation was delivered . there were 3 / 15 rr ( all local relapses ) out of the patients who had ipsilateral neck irradiation , 2 / 30 rr ( with local relapse as well ) in the patients who had bilateral neck radiotherapy and 3 / 42 rr ( 1 with local relapse and 2 neck alone ) for the patients without neck irradiation . 
there was no signicant difference of rr among these 3 groups . toxicity grade 3 + radiomucositis , radiodermatitis and dysphagia occurred in 22 , 10 and 21 % of patients , respectively ( table 7 )  . there was no difference in radiotherapy - related toxicities and the use of ipsilateral or bilateral irradiation . 
however , such a nding may be biased , as most patients without surgical treatment have the most extensive tumours . unfortunately , we did not retrieve other prognostic factors that could allow us to propose tailored therapeutic strategies . 
the exact impact of ict ( 52.9 % ) in our series also remains unclear . other authors [ 18 , 19 ] have found that maxillary sinus tumours , intracranial invasion and n > 0 classication at initial diagnosis were associated with increased local failure and decreased survival . 
 [ 21 ] reported , in 73 patients with maxillary sinus cancers ( 36 scc ) who underwent postoperative ebrt , 11 / 50 without any prophylactic neck treatment developed rr . 
modern imaging modalities , ct scan and pet / ct , allow a better evaluation of nodal status before treatment leading to less neck failure during the follow - up . considering possible related toxicities and potential surgical salvage treatments , the exact role of eni remains to be dened [ 24 ]  . 
on the other hand , recent systematic review reporting 139 patients with n0 maxillary scc showed that eni reduced signicantly the risk of rr compared to observation , while its impact on os remained uncertain [ 12 ]  . 
some authors then proposed eni in larger t3t4 tumours [ 7 ]  . the necessity of eni should be determined according whether there was an initial snd and the result of snd . snd is generally considered for large tumours . in our study , only one pn + patient after snd presented a rr . none of the 24 patients with negative snd progressed in the neck , and 7 / 60 without snd had a rr . 
 [ 24 ] observed 5 / 133 isolated rr in patients with n0 sinonasal carcinoma ( 3 / 51 with scc ) ; 3 of which were salvaged by further treatment . volumes of ebrt , unilateral vs . 
bilateral neck irradiation would largely increase the radiation volume in normal tissues when levels iiii or more need to be treated , but could potentially reduce the contralateral and low neck ( level iiiv ) recurrences . in our series there was no locoregional relapse or toxicity difference according to ipsilateral or bilateral eni in the n0 population . 
 [ 21 ] reported in 11 patients who developed rr , 4 were in level ib ( 3 ipsilateral , 1 bilateral ) , 7 in ipsilateral iia level and no contralateral rr alone . 
the level of nodal involvement depends on the primary tumour extension ( skin , hard palate or nasopharynx ) , whereas contralateral rr could probably occur in tumours that inltrated the midline [ 6 , 20 , 25 ]  . 
 [ 26 ] showed that ipsilateral eni of 50 gy in clinically n0 maxillary scc could decrease the 5 - year actuarial risk of rr from 20 % to 0 % in t3t4 patients . 
bristol ij , ahamad a , garden as , morrison wh , hanna ey , papadimitrakopoulou va et al ( 2007 ) postoperative radiotherapy for maxillary sinus cancer : long - term outcomes and toxicities of treatment . 
abu - ghanem s , horowitz g , abergel a , yehuda m , gutfeld o , carmel n - n et al ( 2014 ) elective neck irradiation versus observation in squamous cell carcinoma of the maxillary sinus with n0 neck : a meta - analysis and review of the literature . 
posner mr , hershock dm , blajman cr , mickiewicz e , winquist e , gorbounova v et al ( 2007 ) cisplatin and uorouracil alone or with docetaxel in head and neck cancer . 
forastiere aa , metch b , schuller de , ensley jf , hutchins lf , triozzi p et al ( 1992 ) randomized comparison of cisplatin plus uorouracil and carboplatin plus uorouracil versus methotrexate in advanced squamous - cell carcinoma of the head and neck : a southwest oncology group study . 
llorente jl , lpez f , surez c , hermsen ma ( 2014 ) sinonasal carcinoma : clinical , pathological , genetic and therapeutic advances . nat rev clin oncol 11 ( 8 ) : 460472 18 . 
mirghani h , mortuaire g , armas gl , hartl d , auprin a , el bedoui s et al ( 2014 ) sinonasal cancer : analysis of oncological failures in 156 consecutive cases . 
duprez f , madani i , morbe l , bonte k , deron p , domjn v et al ( 2012 ) imrt for sinonasal tumors minimizes severe late ocular toxicity and preserves disease control and survival . 
homma a , hayashi r , matsuura k , kato k , kawabata k , monden n et al ( 2014 ) lymph node metastasis in t4 maxillary sinus squamous cell carcinoma : incidence and treatment outcome . 
jiang gl , ang kk , peters lj , wendt cd , oswald mj , goepfert h ( 1991 ) maxillary sinus carcinomas : natural history and results of postoperative radiotherapy . 
jiang gl , morrison wh , garden as , geara f , callender d , goepfert h et al ( 1998 ) ethmoid sinus carcinomas : natural history and treatment results . 
paulino ac , fisher sg , marks je ( 1997 ) is prophylactic neck irradiation indicated in patients with squamous cell carcinoma of the maxillary sinus ? int j radiat oncol biol phys 39 ( 2 ) : 283289 24 . 
mirghani h , hartl d , mortuaire g , armas gl , auprin a , chevalier d et al ( 2013 ) nodal recurrence of sinonasal cancer : does the risk of cervical relapse justify a prophylactic neck treatment ? oral oncol 49 ( 4 ) : 374380 25 . 
guan x , wang x , liu y , hu c , zhu g ( 2013 ) lymph node metastasis in sinonasal squamous cell carcinoma treated with imrt / 3dcrt . 
jeremic b , shibamoto y , milicic b , nikolic n , dagovic a , aleksandrovic j et al ( 2000 ) elective ipsilateral neck irradiation of patients with locally advanced maxillary sinus carcinoma . 
eni ( ipsilateral level ii , ib and iii or bilateral neck according to the primary tumour extension ) needs to be proposed in selected patients , especially when snd has not been performed . compliance with ethical guidelines conict of interest p . 
bhide1 , 2 , 3 , 4 received : 25 september 2015 / accepted : 12 april 2016 / published online : 13 june 2016 springer - verlag berlin heidelberg 2016 abstract aim the aim of this study was to investigate potential advantages and disadvantages of three - dimensional conformal radiotherapy ( 3dcrt ) , multiple xed - eld intensity - modulated radiotherapy ( imrt ) and volumetric - modulated arc therapy ( vmat ) in terms of dose to the planning target volume ( ptv ) , organs at risk ( oars ) and normal tissue complication probability ( ntcp ) for delivering ipsilateral radiotherapy . materials and methods 3dcrt , imrt and vmat were compared in patients with well - lateralised primary tonsillar cancers who underwent primary radical ipsilateral radiotherapy . 
the following parameters were compared : conformity index ( ci ) ; homogeneity index ( hi ) ; dosevolume histograms ( dvhs ) of ptvs and oars ; ntcp , risk of radiation - induced cancer and dose accumulation during treatment . results imrt and vmat were superior to 3dcrt in terms of ci , hi and dose to the target volumes , as well as mandible and dose accumulation robustness . 
the techniques were equivalent in terms of dose and ntcp for the contralateral oral cavity , contralateral submandibular gland and mandible , when specic dose constraint objectives were used on the oral cavity volume . 
dosimetry and ntcp calculations show that these techniques are equivalent to 3dcrt with regard to the risk of acute mucositis when specic dose constraint objectives were used on the contralateral oral cavity oar . keywords volumetric - modulated arc therapy intensitymodulated radiotherapy conformal radiotherapy organs at risk radiation induced cancer ipsilateral oropharynx radiotherapy untersuchung von strahlentherapieverfahren zur radikalen bestrahlung von unilateralen oropharynxtumoren dosimetrie und komplikationswahrscheinlichkeit in normalgeweben zusammenfassung ziel das ziel dieser studie war die untersuchung potenzieller vorund nachteile der dreidimensionalen , konformalen strahlentherapie ( 3dcrt ) , der intensittsmodulierten strahlentherapie ( imrt ) in step - and - shoot - technik und der intensittsmodulierten rotationstherapie ( volumetricmodulated arc therapy , vmat ) fr die ipsilaterale bestrahlung von oropharynxtumoren hinsichtlich der dosisverteilung im planungszielvolumen ( ptv ) , den risikoorstrahlenther onkol ( 2016 ) 192 : 516525 ganen ( oar ) und der komplikationswahrscheinlichkeit in normalgeweben ( ntcp )  . materialien und methoden fr die radikale primrtherapie unterschiedlicher flle von streng unilateralen primren tonsillenkarzinomen wurden dosisverteilungen von 3dcrt , imrt und vmat verglichen . 
hierfr wurden konformittsindex ( ci ) , homogenittsindex ( hi ) , dosisvolumen - histogramme ( dvh ) des ptv und der oar , ntcp , risiko von strahleninduzierten zweittumoren und die aufsummierte applizierte gesamtdosis untersucht . ergebnisse die bestrahlungsplne von imrt und vmat waren in bezug auf ci , hi , dosisverteilung im zielvolumen und im unterkiefer sowie der tatschlich applizierten dosis der 3dcrt berlegen . 
obwohl das niedrigdosisvolumen bei imrt und vmat signikant hher war als bei 3dcrt , war das erwartete risiko strahleninduzierter zweittumoren abhngig vom verwendeten mathematischen modell . schlussfolgerung die untersuchten imrt - / vmat - techniken sind der 3dcrt bei der bestrahlung streng unilateraler oropharyngealer tumoren in bezug auf die dosishomogenitt , konformitt und konsistente bestrahlung des ptv whrend der gesamten behandlungsdauer berlegen . 
dosimetrie und ntcp - berechnungen zeigen , dass diese techniken in bezug auf das risiko einer akuten mukositis bei anwendung einer spezischen dosisbeschrnkung auf die kontralaterale mundhhle quivalent zu 3dcrt sind . schlsselwrter intensittsmodulierte rotationstherapie intensittsmodulierte radiotherapie konformale strahlentherapie risikoorgane strahleninduzierte karzinome ipsilaterale strahlentherapie des oropharynx evaluation of radiotherapy techniques for lateralised oropharyngeal radiotherapy to the ipsilateral oropharynx and neck is a well - established treatment technique for patients with well - lateralised tonsillar squamous cell carcinomas ( scc ) [ 16 ]  . 
an acceptable rate ( 28 % ) of contralateral nodal recurrence in a carefully selected population is supported by published evidence in the form of single - centre retrospective case series [ 16 ]  . 
the rationale behind using an ipsilateral technique is to achieve sparing of contralateral normal structures , the parotid salivary gland in particular , to reduce the rates of long - term xerostomia and associated morbidities . 
this improves quality of life in survivors [ 5 ]  . in addition , it is presumed that the lower dose delivered to the contralateral oral cavity and mandible reduces the rates of acute oral mucositis and mandibular osteoradionecrosis ( orn ) [ 1 , 2 , 4 ]  . two or three ipsilateral wedged elds with three - dimensional conformal radiotherapy ( 3dcrt ) or inverse planning techniques for intensity - modulated radiotherapy ( imrt ) and volumetric - modulated arc therapy ( vmat ) can be used to deliver ipsilateral radiotherapy . in published studies of ipsilateral radiotherapy , some centres have used 3dcrt [ 1 , 4 , 6 ] , some centres have used imrt / vmat [ 2 ] and some centres historically used 3dcrt and converted to imrt / vmat [ 3 ]  . 
when treating non - lateralised tumours of the oropharynx , the advantages of imrt techniques ( multiple - eld and arc therapy ) for sparing the parotid gland and constrictor muscles are well proven [ 7 , 8 ]  . 
such techniques represent the standard of care in the majority of radiotherapy departments . in contrast , there is a lack of evidence to support the use of imrt / vmat techniques in preference to 3dcrt when treating welllateralised oropharyngeal tumours . these techniques use two to three times more monitor units , which results in an increased total body dose due to increased radiation leakage . 
quantication of predicted normal tissue complication probability ( ntcp ) for 3dcrt and imrt / vmat will aid the choice of optimal treatment technique in the setting of ipsilateral irradiation . the specic aim of this study was to demonstrate the potential dosimetric advantages ( or at least equivalence ) of the imrt techniques ( using precise well - dened optimisation ) compared to 3dcrt in terms of dose to the planning target volume ( ptv ) , organs at risk ( oars ) , and ntcp ( including the risk of secondary malignancy ) for treatment of well - lateralised oropharyngeal scc before implementation in clinical practice . 
the secondary aim was to study the dosimetric effect of volumetric changes during treatment for each of these three techniques . materials and methods this was a non - interventional retrospective planning study in 10 patients with well - lateralised primary tonsillar cancers who underwent primary radical ipsilateral radiotherapy at our institute . 
1 isodose distributions for three - dimentsional radiotherapy ( 3dcrt ) , intensity - modulated radiotherapy ( imrt ) and volumetric - modulated arc therapy ( vmat ) , and the dose - difference maps of 3dcrt vs . 
contours : primary planning target volume ( pink ) , contralateral oral cavity ( green ) , contralateral parotid ( orange ) contralateral mandible ( red ) and spinal cord ( white ) fig . 
2 dose volume histograms for the treatment plans of all patients without ( a ) and with ( b ) reoptimisation of the treatment plan using 36 gy as an additional constraint for the contralateral oral cavity . 
3dcrt three - dimentsional radiotherapy , imrt intensity - modulated radiotherapy , vmat volumetricmodulated arc therapy , oc oral cavity tasis or involvement of ipsilateral cervical lymph nodes and therefore required ipsilateral neck irradiation . 
all patients underwent a diagnostic tonsillectomy prior to radiotherapy , which is standard practice across the majority of centres . of the patients , 5 were treated with 3dcrt and the remaining cases received vmat . 
doses to the elective target ( ptv2 ) were 54 gy in 30 fractions ( 1.8 gy / fraction ) over 6 weeks for vmat and 50 gy in 25 fractions ( 2 gy / fraction ) over 5 weeks for 3dcrt . 
patients with node - positive disease and those under the age of 71 years received platin - based concomitant chemoradiotherapy . target volume delineation all patients were treated in a standard thermoplastic shell . planning ct scans were obtained at 2 - mm intervals . 
clinical target volume ( ctv ) 1 included gross tumour volume ( gtv ) plus a 1 - cm isotropic margin plus ipsilateral level ib , iia and any involved lymph nodes . 
uninvolved barriers to tumour spread , such as bone and fasciae , were excluded . strahlenther onkol ( 2016 ) 192 : 516525 table 1 clinical dose objectives for intensity - modulated radiotherapy and volumetric - modulated arc therapy treatment plans optimal required structure ptv1 ptv1 ptv1 ptv1 ptv2 ptv2 ptv2 bilateral parotids supercial parotids spinal cord spinal cord prv ( + 3 mm ) brain stem brain stem prv ( + 3 mm ) optic chiasm bilateral optic nerves bilateral lens dose statistic dose to 99 % dose to 95 % dose to 50 % dose to 2 % dose to 99 % dose to 95 % dose to 50 % mean dose mean dose maximum point dose maximum point dose maximum point dose maximum point dose maximum point dose maximum point dose mean dose ptv planning target volume , prv planning organ at risk volume the elective nodal volume ( ctv2 ) included uninvolved levels iiiv and supraclavicular fossa ( scf ) nodes ipsilaterally . 
in addition , contralateral and ipsilateral mandible , contralateral oral cavity , contralateral submandibular gland ( smg ) and posterior fossa were delineated on the ct by an experienced clinical oncologist ( sb )  . 
the sections of the mandible ipsilateral and contralateral to the side of the tumour , with the midline as the medial border , were delineated as ipsilateral and contralateral mandible , respectively . 
the surfaces of the inner table of mandible , tongue , oor of mouth and hard palate , with the medial border at midline at a distance of 1 cm from the ptv , were outlined as the contralateral oral cavity . 
hippocampal structures were delineated using atlas - based methods [ 13 ]  . treatment planning methods radiotherapy plans were generated using the philips pinnacle3 v 9.6 ( philips , fitchburg , wi , usa ) treatment planning system ( tps )  . 
imrt and vmat plans were retrospectively generated for cases that were initially treated using 3dcrt , and imrt and 3dcrt plans were produced for patients treated using vmat . 3dcrt was planned using a single isocentre anterioroblique and posterior - oblique wedged pair to encompass the ctv1 . 
vmat plans consisted of partial arcs varying from 90 to 105 control points with 2 - degree control point spacing , optimised using pinnacles smartarc algoriththe xed - eld imrt plans consisted of ve coplanar beams with a maximum of 50 control points in total . 
ptv ring structures and other optimisation regions of interest ( rois ; in otherwise noncontoured tissue ) were used in vmat and imrt inverse planning in order to generate conformal plans with reduced rvr integral dose . 
vmat and imrt plans were further optimised with a constraint of maximum mean dose of 36 gy ( based on average mean dose from the 3dcrt plans , table 2 ) to the contralateral oral cavity volume . treatment plan evaluation coverage of ptvs was evaluated using the volume receiving 95 % of the prescribed dose ( v95 ) and dose distribution to ptv1 was further evaluated using the paddick conformity index ( ci ) and the homogeneity index ( hi )  . 
mean results with corresponding standard deviations ( sds ) are shown with p - values to test for statistical signicance between the planning techniques ptv planning target volume , v95 volume receiving 95 % of the prescribed dose , ci conformity index , hi homogeneity index , d2 maximum dose ( gy ) received by 2 % of the ptv , d98 minimum dose ( gy ) received by 98 % of the ptv , d50 dose ( gy ) received by 50 % of volume conformal plans have ci = 1 , whilst smaller ci values correspond to less conformal dose distributions . 
doses to oars were evaluated using the following dosimetric criteria : clinical dose objectives ( table 1 ) ; mean and maximum dose ( d2 - dose to 2 % volume ) to the ipsilateral and contralateral mandible ; mean dose to the contralateral oral cavity , contralateral smg and posterior fossa . 
dose cubes were exported from pinnacle to the raystation tps ( raysearch laboratories , stockholm , sweden ) in order to generate dose difference maps . ntcp calculations the doses to the bilateral hippocampi and contralateral oral cavity were converted to the equivalent dose in 2 - gy fractions ( eqd2 ) using the withers formula and / = 2 [ 15 ] and 10 , respectively [ 16 ]  . 
 [ 15 ] , where the probability of a decline in short - term memory function , as measured by the wechsler memory scale - iii word lists as delayed recall at 18 months post - rt , is related to the bilateral hipstrahlenther onkol ( 2016 ) 192 : 516525 pocampal eqd2 d40 . 
to capture the range of possible estimates of secondary cancer risk , the probability was assessed using a model with reducing risk for higher doses , where the risk is assumed to fall off for increasing dose with d0 = 10 , and also using a dose plateau model , where the risk of radiation - induced cancer is postulated to plateau beyond a threshold dose of 4 gy [ 9 ]  . 
 ( d0 ( gy ) is the reciprocal of the slope ; i.e. , the dose required to reduce cell survival to 37% on the linear portion of the survival curve . ) dose accumulation cone beam ct ( cbct ) images , acquired on days 13 and at weekly intervals thereafter , were used to calculate dose accumulation for each of the plans . 
cbct images lack sufcient quality for use in dose calculation so the images were post - processed to remove scatter , using data from the in addition , to correct for patients planning cts [ 11 ]  . when the patients shoulders and top of head were outside the cbct eld of view ( fov ) , the fov was increased and these structures were mapped to the cbct from the planning ct and the hounseld units were set to values for soft tissue . 
furthermore , the patients shoulders and top of head , which were outside the imaged fov on treatment , were outlined on the planning ct and mapped across to the on - treatment images with density overrides applied to the body tissue outside of the cbct fov . 
the deformations were then applied to the dose cube calculated on the cbct to enable dose summation , thereby allowing us to calculate an estimate of the delivered accumulated dose . 
estimates for the changes in the dose to target volumes and oars from planning to treatment were then quantied . data analysis a statistically signicant ( for p - values see table 2 ) , higher percentage volume of ptv 1 and 2 , respectively , received 95 % of the prescribed dose ( v95 ) when using imrt ( 97 and 98 % ) and vmat ( 97 and 97 % ) as compared to 3dcrt ( 92 and 89 % ; table 2 )  . 
there was no statistical difference in v95 , hi or ci between imrt and vmat plans ( pvalues table 2 )  . maximum doses to the spinal cord and brainstem were signicantly higher with imrt ( 43 gy , p = 0.008 and 46 gy , p = 0.002 , respectively ) and vmat ( 42 gy , p = 0.004 and 44 gy , p = 0.002 , respectively ) compared to 3dcrt ( 36 and 35 gy , respectively ; table 2 )  . 
however , these were within published tolerance values [ 19 , 20 ]  . the mean dose to the ipsilateral mandible and percentage volume receiving 60 gy ( v60 ) were signicantly lower with imrt and vmat versus 3dcrt ( table 2 for pvalues )  . 
wilcoxon signed - rank tests were used to compare differences between 3dcrt , ntcp calculations 522 strahlenther onkol ( 2016 ) 192 : 516525 based on ntcp calculations ( table 3 )  . 
when a specic oral cavity constraint was used , the apparent advantage of 3dcrt disappeared . however , the imrt technique maintained its signicant advantage over vmat . radiation - induced cancers the predicted probabilities of radiation - induced cancers depend on the applied model and are always higher for imrt and vmat than 3dcrt ; always resulting in higher risk values than those for 3dcrt . 
however , differences between the planning techniques were not statistically signicant ( table 3 )  . dose accumulation data on estimates of change in dose from planning to treatment were available for 8 out of 10 patients . 
statistically signicant reduction in the d95 for ctv1 was observed for all 3dcrt ( 3.5 gy ) , imrt ( 1.9 gy ) and vmat ( 1.9 gy ) plans , with the largest reduction observed for 3dcrt ( table 4 )  . 
a statistically signicant increase of approximately 1 gy in both the brain stem ( d0.1cm3 ) and posterior fossa ( mean dose ) , was measured for imrt and vmat as compared to the original treatment plan . 
additionally , 3dcrt resulted in a signicant ( p = 0.014 ) reduction in elective target ( ctv2 ) coverage . discussion this study demonstrates that imrt and vmat resulted in improved dose conformity ( ci ) and homogeneity to both primary and elective targets . 
however , this was at the expense of a higher dose to the contralateral oral cavity , when using standard optimisation rois for inverse planning . imrt and vmat were equivalent to 3dcrt for contralateral oral cavity sparing when optimised using a specic dose constraint of < 36 gy to the contralateral oral cavity , without affecting the ptv . 
this is reected in the ntcp calculations with equivalent probabilities of acute mucositis for the reoptimised plans . the mean dose and v60 to the ipsilateral mandible were signicantly lower for imrt and vmat , table 2 . 
a study of 30 patients with orn ( out of total of 402 patients with oropharyngeal cancer ) demonstrated v50 and v60 to be signicant factors for development of orn [ 21 ]  . 
the mean dose with all three techniques was lower than the 26 gy threshold for table 3 predicted normal tissue complication probabilities ( ntcps ) for 3d conformal radiotherapy ( 3dcrt ) , intensity - modulated radiotherapy ( imrt ) and volumetric - modulated arc therapy ( vmat ) plans for all 10 patients ntcp model dose statistic ncf impairment [ 12 ] grade 3 dysphagia [ 13 ] eqd2 d40 bilateral hippocampi md2 gy oral cavity vmat mean ( sd ) p - values , wilcoxon signed - rank test 3dcrt vs . 
using a larger patient dataset ( including the one used in the eisbruch study ) , the predicted risk of late grade 2 xerostomia is less than 5 % with 3dcrt and vmat in addition , there was no signicant difference in the dose to the contralateral smg when imrt / vmat plans were reoptimised using specic dose constraints . 
therefore , 3dcrt and imrt / vmat are likely to be equivalent in terms of the late patient - reported xerostomia scores . imrt techniques resulted in a statistically signicant increase in the volume of normal tissue receiving low - dose radiation ( table 2 )  . 
the rst two of these are probably lower with imrt due to the reduced high - dose eld sizes and reduced intensity of the individual beahead leakage is responsible only for scatter radiation > 1530 cm from the treatment area [ 27 ]  . 
the radiation dose to distant tissues from head leakage is very low and data from clinical and experimental studies suggest that the risk from doses < 0.15 gy is negligible [ 28 ]  . 
head leakage is hardwareand softwaredependent , with variation among treatment centres [ 29 ]  . the probability of developing a secondary malignancy as a result of low - dose irradiation to a greater volume in the proximity of treatment elds depends on the model applied . 
also modelled the risk using measurements of dose in phantom to tissues within the proposed target volumes for various possible treatment sites including tonsillar and nasopharyngeal cancer and failed to demonstrate increased risk with either of these models [ 29 ]  . given the uncertainties in the model of secondary cancer risk , more research in this area is required prior to drawing denite conclusions [ 28 ]  . dose accumulation calculations demonstrate that mean d95 to ctv1 throughout the 6 weeks of treatment was , on average , 1.6 gy lower for 3dcrt plans compared to both imrt and vmat . 
it should be noted , however , that in spite of the absence of statistically signicant differences between treatment techniques , the 524 strahlenther onkol ( 2016 ) 192 : 516525 difference for an individual patient might still be clinically signicant . conclusion this study demonstrates that vmat , which is highly optimised to minimise dose deposition in areas outside the ptv , is the best technique in terms of dose homogeneity , conformity , risk of orn and consistent dose delivery to the ptv throughout the course of treatment for patients with lateralised oropharyngeal cancers . 
dosimetric and ntcp calculations show that vmat is equivalent to 3dcrt in terms of the risk of acute mucositis and late xerostomia with specic dose constraints on a contralateral oral cavity oar . 
a higher volume of normal tissue outside the ptv is exposed to a low radiation dose with these techniques , which may translate into a higher a risk of radiation - induced malignancies , depending on the applied radiobiological model . acknowledgements this work was undertaken in the royal marsden nhs foundation trust which received a proportion of its funding from the nhs executive ; the views expressed in this publication are those of the authors and not necessarily those of the nhs executive . 
the authors also acknowledge the support of the national institute for health research royal marsden and institute of cancer research biomedical research centre . compliance with ethical guidelines conict of interest d . 
juni 2016 springer - verlag berlin heidelberg 2016 hintergrund die standardbehandlung von patienten in frhen stadien eines hodgkin - lymphoms ( hl ) besteht gegenwrtig aus einer polychemotherapie , gefolgt von einer konsolidierenden involved - field - radiotherapie ( ifrt )  . 
ein hnliches studiendesign wird auch in den aktuell rekrutierenden studien der deutschen hodgkin - lymphom - studiengruppe ( ghsg ) und der eortc verfolgt . patienten und methode zwischen oktober 2003 und august 2010 wurden in england insgesamt 602 patienten aus 94 teilnehmenden zentren rekrutiert . 
patienten mit pet - positivem befund erhielten einen weiteren zyklus abvd und anschlieend eine konsolidierende ifrt mit 30 gy . ergebnisse von den 602 eingeschlossenen patienten erhielten 571 patienten eine pet - untersuchung ; 426 von ihnen ( 74 , 6 % ) hatten ein pet - negatives ergebnis . 
nach einem medianen follow - up von 60 monaten erlitten 22 patienten in dem therapiearm ohne if - rt eine krankheitsprogression , wovon 2 patienten verstarben , keiner jedoch am hl . zwei weitere patienten verstarben ohne vorherige krankheitsprogression . 
das progressionsfreie 3 - jahresberleben ( pfs ) im therapiearm mit if - rt betrug 94 , 6 % und 90 , 8 % im therapiearm ohne konsolidierende rt . schlussfolgerung der autoren die ergebnisse der studie konnten die nichtunterlegenheit des rt - freien experimentellen arms nicht belegen . 
jedoch hatten patienten in frhen stadien eines hl mit einem pet - negativen ergebnis nach 3 zyklen abvd auch ohne if - rt noch eine sehr gute prognose . originalpublikation radford j , illidge t , counsell n , counsell n et al ( 2015 ) results of a trial of pet - directed therapy for early - stage hodgkins lymphoma . 
folgende berlegungen sind anzumerken : der stellenwert der pet zur therapiekontrolle und - stratizierung ist gegenstand mehrerer randomisierter 596 strahlenther onkol ( 2016 ) 192 : 595596 therapieprotokolle , u . 
die daten der endauswertung der deutschen hd15 - studie ( fortgeschrittene stadien ) belegen , dass patienten , die nach abschluss der chemotherapie noch einen positiven pet - restbefund 2 , 5 cm aufweisen , eine additive lokale bestrahlung bentigen [ 1 ]  . da patienten mit hl langzeitberlebende geworden sind und eine exzellente prognose haben , sollten therapieassoziierte spttoxizitten minimiert werden . 
hier ist eine therapie , die aus lediglich 2 zyklen abvd gefolgt von einer if - rt mit 20 gy besteht , ausreichend [ 2 ]  . aktuell wird sowohl von der eortc als auch der ghsg der stellenwert des pet zur therapiestratizierung fr patienten in frhen stadien weiter geprft . in der hd16 - studie ( frhe gnstige stadien ) und der hd17 - studie ( frhe ungnstige stadien ) der ghsg wird die konsolidierende radiotherapie pet - basiert eingesetzt . die daten der zwischensowie der endauswertung mssen hier jedoch noch abgewartet werden . 
die ersten daten der eortc , die in ihrer h10 - studie ebenfalls die rt petbasiert einsetzt , zeigen jedoch vermehrt krankheitsereignisse , wenn die patienten keine konsolidierende bestrahlung erhielten [ 3 ]  . die auswertung der hier kommentierten studie konnte die nichtunterlegenheit des experimentellen , rt - freien studienarms wegen dessen schlechterer tumorkontrolle nicht nachweisen . 
in den publizierten daten der intention - to - treat - analyse ( itt ) hinsichtlich des 3 - jahrespfs zeigt sich ein unterschied von bis zu 8 , 8 % , in der per - protocol - analyse von bis zu 11 % . 
diese ergebnisse sollten bei therapieplanungen kritisch bercksichtigt werden . mit modernen zielvolumenkonzepten wie der involvednode - radiotherapie ( in - rt ) [ 4 ] oder auch der krzlich von der international lymphoma radiation oncology group denierten involved - site - radiotherapie ( is - rt ) werden die bestrahlungsvolumina knftig konsekutiv reduziert werden . 
hierdurch ist auch zu erwarten , dass weniger therapieassoziierte nebenwirkungen eintreten [ 5 ]  . die bestrahlung stellt somit eine nebenwirkungsarme therapiekomponente dar . fazit insgesamt ist die schlussfolgerung der autoren kritisch zu beleuchten . 
eine pet - basierte radiatio sollte weiterhin als experimentell betrachtet werden und kann daher regelhaft nur im rahmen groer randomisierter klinischer studien anwendung nden . jan kriz und hans theodor eich , mnster literatur 1 . 
engert a , haverkamp h , kobe c , markova j , renner c , ho a et al ( 2012 ) reduced intensity of chemotherapy and pet - giuded radiotherapy in patients with advanced stage hodgkin lymphoma : an open - label , randomised phase 3 trial . 
engert a , plutschow a , eich ht , lohri a , dorken b , borchmann p et al ( 2010 ) reduced treatment intensity in patients with earlystage hodgkins lymphoma . 
raemaekers jm , andr mp , federico m et al ( 2014 ) omitting radiotherapy in early positron emission tomography - negative stage i / ii hodgkin lymphoma is associated with an increased risk of early relapse : clinical results of the preplanned interim analysis of the randomized eortc / lysa / fil h10 trial . 
specht l , yahalom j , illidge t et al ( 2014 ) modern radiotherapy for hodgkin lymphoma field and dose guidelines from the international lymphoma radiation oncology group ( ilrog )  . 
the epithelial radiation response is accompanied by changes in the inammatory signaling cascades mediated by the transcription factor nuclear factor - kappa b ( nf - b )  . the present study was initiated to determine the effect of the nf - b inhibitor thalidomide on the clinical manifestation of oral mucositis in the established mouse tongue model . materials and methods treatment protocols comprised single dose irradiation and daily fractionated irradiation ( 5 fractions of 3 gy / week ) over 1 ( days 04 ) or 2 weeks ( days 04 , 711 ) , alone or in combination with daily thalidomide application ( 100 mg / kg intraperitoneally ) over varying time intervals . 
similar results were observed during two weeks of fractionated irradiation in all but one experiment . conclusion thalidomide treatment demonstrated a significant mucositis - ameliorating effect during fractionated irradiation , which is likely to result from nf - b inhibition . however , further mechanistic studies are required to dene the underlying mechanisms of the observed mucoprotective effect . keywords radiotherapy oral mucositis thalidomide nf - b mouse model modulation der strahleninduzierten oralen mukositis durch thalidomid prklinische studien zusammenfassung hintergrund die orale mukositis ist eine huge , dosislimitierende frhe nebenwirkung der radio ( chemo ) therapie von kopf - hals - tumoren . 
die vorliegende studie soll den effekt von thalidomid , einem nf - b - inhibitor , auf die klinische ausprgung der oralen mukositis am etablierten modell der musezunge klren . material und methoden die behandlungsprotokolle beinhalteten eine einzeitbestrahlung und eine tglich fraktionierte bestrahlung ( 5 3 gy / woche ) ber eine ( tage 04 ) 562 strahlenther onkol ( 2016 ) 192 : 561568 oder 2 wochen ( tage 04 , 711 ) , allein oder in kombination mit tglicher thalidomid - gabe ( 100 mg / kg intraperitoneal ) ber verschiedene zeitintervalle . 
whrend der 2 - wchigen fraktionierten bestrahlung konnte , mit ausnahme eines experiments , ebenfalls ein signikanter effekt festgestellt werden . schlussfolgerung die thalidomid - behandlung unter tglicher fraktionierter bestrahlung zeigte eine signikante verminderung der oralen mukositis , mglicherweise als folge der nf - b - inhibition . 
weitere mechanistische studien sind jedoch notwendig , um die zugrundeliegenden mechanismen dieses mukoprotektiven effekts zu klren . for prevention and / or mitigation of radiation - induced oral mucositis [ 1517 ]  . thalidomide , a - n - phthalmidoglutarimide , inhibits nfb activation [ 18 ] and has anti - inammatory , anti - neoplastic , and anti - angiogenic properties [ 19 ]  . 
preclinical studies in a hamster model demonstrated a mucositis - ameliorating effect of this drug after chemotherapy [ 20 ]  . the aim of the present study was to investigate the oral mucositis - ameliorating potential of thalidomide in the established mouse tongue model . 
mucosal ulceration , corresponding to mucositis grade 3 of the classication of the radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc ) , was analyzed as the clinically relevant endpoint . 
the time course parameters latency and duration of ulcerative lesions were analyzed as secondary endpoints . materials and methods schlsselwrter radiotherapie orale mukositis thalidomid nf - b mausmodell animals introduction oral mucositis is the most frequent and often dose - limiting early side effect of radio ( chemo ) therapy for advanced head - and - neck malignancies , eventually resulting in ulcerative lesions in the oral cavity . 
severe pain , swallowing difculties , also associated with weight loss , often lead to unplanned treatment breaks , which result in a signicant decrease in tumor control probability [ 35 ]  . various prophylactic and therapeutic approaches to reduce the severity of oral mucositis have been tested preclinically and also in initial clinical studies [ 610 ]  . 
e. , improvement of oral hygiene , mucosal coating agents , mouth washes , and administration of antibiotics and analgesics [ 11 ]  . the pathobiology of oral mucositis includes activation of transcriptions factors , such as nf - b , which leads to the up - regulation of pro - inammatory signaling cascades [ 1214 ]  . 
nf - b inhibition represents a promising strategy eight to 12 weeks old mice of the inbred c3h / neu strain from the breeding facility of the department for biomedical research of the medical university of vienna were used for all experiments . 
animals were housed under specic pathogen - free conditions with controlled humidity ( 55 10 % ) , temperature ( 22 2 c ) , and a 12 / 12 - h lightdark rhythfree access to standard mouse diet ( ssniff spezialditen gmbh , soest , germany ) and fresh water from standard drinking bottles was provided ad libitum . a maximum of 5 animals were kept in makrolon cages ( techniplast gmbh , hohenpeienberg , germany ) on aspen wood bedding ( abedd - lab & vet service gmbh , vienna , austria )  . 
the beam was applied vertically . percutaneous irradiation of the entire snout was performed without anesthesia as described previously [ 21 , 22 ]  . in brief , animals were guided into perspex tubes ( inner diameter 25 mm )  . 
the graded local top - up doses are listed in the rightmost column . front end of the tubes served for positioning of the snouts . the back ends of the tubes were closed with a polystyrene plug to prevent withdrawal of the animals . 
the dose rate at the focus - to - surface distance 45.5 cm was approximately 1 gy / ma 12 - mm thick collimator plate , consisting of lead equivalent mcp - 96 , shielded the bodies of the animals caudally from a plane from the eyes to the throat , thus , including the entire tongue . 
briey , mice were immobilized by pentobarbital sodium , 60 mg / kg intraperitoneally ( release , wdt , garbsen , germany ) , and placed in a supine position in the central bore ( diameter 25 mm ) of an aluminum block . 
the tongue was pulled gently through a hole ( diameter 3 mm ) in the roof of the block and the upper surface was xed to the block with adhesive tape . 
in animals that did not develop ulceration , thalidomide treatment was stopped when the ulcerations of the responders had healed ( table 1 )  . fractionation ( experiment f 1 , f 2 ) comprised daily 3 gy fractions over one ( days 04 , f 1.0 ) or two weeks ( days 04 , 711 , f 2.0 ) , followed by graded local top - up doses on day 7 or day 14 , respectively ( table 1 )  . 
e. , in fractionation protocols relative to the day of top - up irradiation ealternative test ( see statistical analysis ) sd standard deviation ulceration was analyzed as the primary endpoint . 
latency ( time between irradiation and rst ulcer diagnosis ) and ulcer duration ( from rst diagnosis to macroscopic healing ) served as secondary endpoints . ance or behavior of the animals , other than the mucosal radiation response were observed . thalidomide and single dose irradiation statistical analysis the statistical analysis system , sas , version 9.3 ( sas institute inc . , cary , nc , usa ) was used for all statistical procedures . 
ed50 values and their standard deviation ( error bars ) were calculated by logit analyses . thalidomide was applied daily from day 3 until the day of rst diagnosis of ulcerations ( sd 1 ) or until the day of healing of ulcerations ( sd 2 )  . 
thalidomide administration over the above mentioned time intervals did not signicantly or systematically inuence these time course parameters . discussion oral mucositis is a frequent and dose - limiting side effect of radio ( chemo ) therapy of head and neck cancer . 
when thalidomide was given only in the rst week , the increase of the ed50 value did not reach signicance . the biological mechanisms underlying the mucoprotective effect of thalidomide are still unclear . in the initial phase of mucositis , dna damage and reactive oxygen species result in activation of nf - b and up - regulation of pro - inammatory cytokines , such as tumor necrosis factor , interleukin - 6 , and interleukin - 1 in the epitheliuseveral preclinical and clinical studies revealed that increased levels of these cytokines correlate with the development and also the severity of oral mucositis [ 13 , 25 ]  . 
the mucoprotective potential of thalidomide may hence be based on the direct inhibition of nf - b and down - stream inammatory signaling cascades in the crucial phase of mucositis development . 
however , once the ulcerative phase is initiated , thalidomide does not accelerate healing of the oral mucosal epithelium . irradiation also stimulates the expression of the pro - inammatory enzyme cyclooxygenase - 2 ( cox - 2 ) in endothelial cells and broblasts in the submucosa . 
 * * p < 0.0001 receiving radiation therapy for head - and - neck cancer also failed to prove a benecial effect on the severity and / or the morbidity of mucositis [ 26 ]  . 
in response to inammatory stimuli , icam - 1 expression is increased on multiple cell types , for example , human epithelial and endothelial cells and facilitates transendothelial migration of leukocytes [ 2931 ]  . 
 * * p < 0.0001 sponse , and therefore cox - 2 activation may not initiate but rather modulate already existing mucosal reactions [ 12 ]  . in line with these considerations , selective inhibition of cox - 2 did not affect the incidence of mouse tongue ulcers [ 8 ]  . 
moreover , a randomized double - blind placebocontrolled trial of celecoxib for oral mucositis in patients strahlenther onkol ( 2016 ) 192 : 561568 nf - b binding to the icam - 1 promoter . 
the anti - inammatory effect of thalidomide could hence also be ( partly ) due to the indirect inhibition of this adhesion molecule . in oral mucosa regenerative processes in response to fractionated irradiation ( repopulation ) start at the end of the rst treatment week , and subsequently are responsible for the increase in radiation tolerance with increasing overall treatment time . 
the highly complex process consists of three major mechanisms : acceleration of stem cell proliferation , asymmetry loss of stem cell divisions , and abortive divisions of sterilized cells [ 3335 ]  . 
thalidomide application during the rst week of fractionated irradiation may lead to an earlier onset of the compensatory regenerative response , thus , resulting in a decreased incidence of ulcerations . 
furthermore , the interrelation with inhibition of nf - b and the inammatory signaling cascade may additionally stimulate , indirectly , one or more of the underlying mechanisms of repopulation . conclusion in this study , a mucoprotective potential of thalidomide in radiation - induced oral mucositis during fractionated radiotherapy was demonstrated , presumably by inhibiting nf - b and supporting epithelial repopulation . 
however , further mechanistic studies are needed to clarify the biological mechanisms underlying the mucoprotective efcacy of this drug . acknowledgements the nancial support by the federal ministry of science , research and economy and the national foundation for research , technology and development is gratefully acknowledged . compliance with ethical guidelines conict of interest k . 
juli 2016 springer - verlag berlin heidelberg 2016 burg zum facharzt fr radiologie ( 1983 ) und zum facharzt fr strahlentherapie ( 1984 ) absolvierte er in den abteilungen fr strahlentherapie , rntgendiagnostik und gynkologische radiologie . 
von 1984 bis 1995 war er zunchst unter wannenmacher , nach dessen wechsel nach heidelberg unter frommhold als oberarzt der abteilung fr strahlentherapie an der freiburger universittsklinik ttig . nach seiner habilitation im jahre 1989 ber experimentelle untersuchungen an menschlichen tumoren auf der thymusdysplastischen nacktmaus erhielt er die venia legendi fr das fach strahlentherapie . 
einen ruf an die abteilung fr strahlentherapie am universittsklinikum marburg lehnte er ab und erhielt 1993 den ruf auf den lehrstuhl fr strahlentherapie im fachbereich humanmedizin der freien universitt berldamit verbunden war die leitung der klinik fr radioonkologie und strahlentherapie am universittsklinikum benjamin franklin der freien universitt berlin ( ukbf ) , die er am 1 . 
besonders am herzen lag ihm die protonentherapie am auge und die interdisziplinre therapie des prostatakarzinoms . gemeinsam mit michael frster und norbert bornfeld ( augenklinik ukbf ) implementierte er die protonentherapie am auge am hahn - leitner - institut ( spter helmholtzinstitut ) in berlinnerhalb dieser , auch international bedeutsamen kooperation wurden seit 1998 bis 2015 mehr als 2000 patienten mit tumoren des auges durch protonenstrahlen behandelt , lange bevor die ersten protonentherapiezentren in deutschland ihre klinische und wissenschaftliche arbeit aufnahmen . in der interdisziplinren multimodalen therapie des prostatakarzinoms beschftigte er sich insbesondere mit der postoperativen strahlentherapie und hatte als mitglied der leitkommission der deutschen s3 - leitlinie des prostatakarzinoms , die erstmals 2007 publiziert wurde , mageblichen anteil an dem erfolg dieser leitlinie . das ergebnis seiner vielfltigen arbeiten waren mehr als 200 verffentlichungen in wissenschaftlichen zeitschriften oder als buchbeitrge . 
konsequenterweise wurden wolfgang hinkelbein zahlreiche wichtige wissenschaftliche auszeichnungen verliehen , von denen hier nur auf den wilhelm - conrad - rntgen - preis der deutschen rntgengesellschaft und an die medaille der medizinischen fakultt der freien universitt berlin hingewiesen werden soll . neben diesen beeindruckenden zeichen seines erfolgs als arzt und wissenschaftler gab es auch weitere seiten der persnlichkeit von wolfgang hinkelbein , die ihm auch auerhalb seines privaten umfelds vielfltige freundschaften von kolleginnen und kollegen sicherte , die ihn oder er sie als kollege , chef , mentor und freund begleiteten . 
er hatte die seltene gabe , konzentriert und aufmerksam anliegen zuzuhren und neutral bewerten zu knnen , ohne vorab inhaltlich festgelegt zu sehatte er sich einmal zu einem vorgehen entschlossen , wurde es vorbehaltlos mit aller intensitt und konsequenz untersttzt und umgesetzt . 
dabei kam auch sein ausgeprgter sinn fr humor nicht zu kurz . kurzum , es ging weniger um das , was er machte , sondern darum , wie er es machte . 
es war wohl diese mischung aus witz und charme , pragmatismus , gelassenheit , autoritt und souvernitt und seine art auf die menschen zuzugehen , die ihm die wertschtzung so vieler einbrachte . bei alledem menschlich am beeindruckendsten war der umgang mit der schweren erkrankung , der lungenbrose , die sich erstmals 2008 abzeichnete . 
nach der geglckten ersten lungentransplantation im november 2008 war es jedoch nicht nur die beschriebene persnlichkeit wolfgang hinkelbeins , sondern auch die vollkommen uneingeschrnkte untersttzung seines groen umfeldes , aber insbesondere auch seiner frau margit , selbst strahlentherapeutin an der charit , die seinen erfolgreichen kampf gegen diese erkrankung erst ermglichte . 
nur wenige hatten damit gerechnet , dass er zu seiner regulren ttigkeit als rztlicher direktor der klinik fr radioonkologie am cbf wrde zurckkehren knnen , aber genau so geschah es . 
er konnte tatschlich bis zu seiner emeritierung im jahre 2013 weiterhin wissenschaftlich und klinisch sehr erfolgreich wirken , wobei die umfassende untersttzung seiner mitarbeiterinnen und mitarbeiter in seiner klinik fr ihn menschlich beraus wichtig war . 
nach seiner emeritierung kam es zu zunehmenden komplikationen als folge der lungentransplantation , die eine erneute transplantation erforderlich machten und fr deren umsetzung er noch einmal unerschrocken mit aller untersttzung seiner ehefrau ins feld zog . 
we aimed to assess the current situation of young radiation oncologists , medical physicists and radiation biologists . methods an online survey that included 52 questions or statements was designed to evaluate topics related to training , clinical duties and research opportunities . 
there was a strong interest in research among the participants ; however a clear separation between research , teaching and routine clinical duties was rarely present for radiation oncologists and medical physicists . 
for radiation biologists , a lack of training in clinical and translational research was stated . conclusion this survey details the current state of education and research opportunities in young radiation oncologists , medical physicists and radiation biologists . 
these results will form the basis for the future working program of the ydegro . keywords ydegro residency education research survey situation junger mediziner , physiker und biologen in der radioonkologie im deutschsprachigen raum ergebnisse einer webbasierten umfrage der arbeitsgruppe junge degro zusammenfassung hintergrund die arbeitsgruppe junge degro ( ydegro ) wurde 2014 innerhalb der deutschen gesellschaft fr radioonkologie ( degro ) gegrndet . 
ziel dieser arbeit ist die statuserhebung der aktuellen situation von jun508 strahlenther onkol ( 2016 ) 192 : 507515 gen rzten , physikern und biologen in der radioonkologie in deutschland . methoden es wurde eine onlineumfrage mit 52 fragen zu den themen ausund weiterbildung , klinische ttigkeit und forschung entwickelt . 
mithilfe der elektronischen degro - mitgliedskartei und kontaktpersonen an den deutschen universittskliniken sowie an 4 kliniken in sterreich und der schweiz wurde die einladung zur teilnahme an dieser umfrage per e - mail an junge mediziner , physiker und biologen in der strahlentherapie verschickt . ergebnisse insgesamt wurden 260 antworten ausgewertet ; 69 % der teilnehmer waren mediziner , 23 % physiker und 9 % biologen . 
im bereich der biologie zeichnete sich ein bedarf in der ausund weiterbildung bezglich klinischer und translationaler forschung schlussfolgerung diese umfrage gibt detaillierte einblicke in die aktuelle situation junger rzte , physiker , und biologen bezglich ausund weiterbildung , klinischer routine und forschung in der deutschen radioonkologie . 
die ergebnisse dieser umfrage bilden die grundlage fr das zuknftige arbeitsprogramm der ydegro . schlsselwrter ydegro facharztausbildung ausbildung forschung befragung background and purpose radiation oncology a cornerstone in the treatment of malignant diseases . 
the majority of cancer patients receive radiotherapy during their course of disease , either as a part of a unior multimodal curative concept [ 1 , 2 ] or as a palliative measure to reduce the symptomatic burden of advanced disease [ 3 ]  . 
using guidelines for infrastructure and human resources published by the european society for radiotherapy and oncology ( estro ) and the international atomic energy agency ( iaea ) , datta et al . 
 [ 4 ] showed that there is a current decit of 26 , 18 , 23 and 11 % regarding teletherapy units , radiation oncologists , medical physicists and radiotherapy technologists in 39 european countries , respectively . 
they estimated the increase of cancer incidence and calculated that by 2020 , an additional 1698 teletherapy units , 2429 radiation oncologists , 1563 medical physicists and 2956 radiotherapy technicians would be needed in these countries to meet the increasing patient number [ 4 ]  . treatment would increase by 22 % between 2010 and 2020 for the united states population , creating a considerable demand for qualied radiation oncologists , medical physicists , radiotherapy technicians and radiation biologists . the german society of radiation oncology ( degro ) was founded in 1995 and originated from a section within the german rntgen society . in 2014 , the degro had 2 , 167 members . 
the largest member group were physicians ( 73 % ) , followed by technicians / dosimetrists ( 14 % ) , medical physicists ( 8 % ) and biologists ( 2 % )  . 
of the society members , 111 ( 5 % ) were aged 2029 years and 359 ( 17 % ) were 3039 years old [ personal communication from heide mller , degro ofce ]  . the degro has performed two prior surveys regarding the situation of radiation oncology residents in germany in 2006 and 2008 , respectively [ 6 , 7 ]  . 
while the rst mainly dealt with recruitment challenges and radiation oncology training in general [ 6 ] , the second survey focused on residency itself as well as important advantages and drawbacks [ 7 ]  . 
while most residents were satised with their residency , the majority of respondents stated that training in special techniques , such as stereotactic radiotherapy or intensity - modulated radiotherapy at that time were underrepresented in the curriculum and that the organization of the curriculum was suboptimal [ 7 ]  . 
only 41 % felt that they were provided with adequate support and time for academic research [ 7 ]  . in february 2014 , the degro working group young degro ( ydegro ) was established within the degro . the goal was to establish a representation of the young physicians , physicists and biologists in the eld of radiation oncology . 
as a rst step , a survey was generated to gather opinions on the current state of education and training among young radiation oncologists , medical physicists and radiation biologists in germany . methods an online survey was developed regarding ( 1 ) the future projects of the ydegro , ( 2 ) participation in activities of the ydegro and the degro and ( 3 ) the current status of education / training , clinical duties , teaching and research activities for radiation oncologists , medical physicists and radiation biologists . 
of those questions and statements , 22 were general , whereas the rest were specic to the professional background of the participants ( 13 for medicine , 7 for medical physics and 10 for radiation biology )  . 
 [ 5 ] projected that the absolute number of cancer patients receiving radiotherapy during their initial an open source software ( limesurvey gmbh , hamburg , germany ) was used to generate an online survey . 
these contact persons were instructed to invite all young professionals of their respective departments as well as those from other hospitals and private practices to participate in the survey . despite younger professionals being the primary target audience , there was no age limit for participation . 
to enhance the clarity of the data , we grouped the positive answers strongly agree and agree unless otherwise stated . results baseline characteristics there were a total of 387 responses to the survey . 
median age was 33 years . scope of ydegro activities of the respondents 89 % voted that the ydegro should be the lobby for the young professionals inside the degro . promoting the participation of young members in committees and panels of the degro was approved by 82 % of respondents . 
building a platform for professional communication and exchange , improvement of working conditions for scientists as well as clinicians and enhancement of continuing education was advocated by 80 , 79 and 89 % , respectively . in all , 44 % stated that they were very interested or mostly interested in joining the activities of ydegro . 
2 , only 4 % of respondents strongly agreed that there was a complete separation between clinical duties and research or teaching activities , while 22 % strongly disagreed with this statement ( 25 % of physicians and 14 % of medical physicists )  . 
only 23 % agreed that conducting research was possible during normal working hours on a regular basis ( 9 % for physicians and 22 % for medical physicists )  . 
1 question 12 are you interested in clinical research ? ; are you interested in preclinical / experimental research ? ; and are you interested in physical / technical research ? for physicians and medical physicists 100% strahlenther onkol ( 2016 ) 192 : 507515 fig . 
the mean number of night or weekend shifts per month was 2.3 ( range 08 ) with 123 responses ( 32 % ) and 56 % of respondents being satised with the number of night / weekend shifts . 
regular team meetings or individual feedback discussions were held in 68 % of cases and 52 % stated that their ideas for improvement were mostly taken up for discussion . strahlenther onkol ( 2016 ) 192 : 507515 fig . 
3 question / statement 25 it is possible to handle the clinical responsibilities during the regular working hours shown separately for physicians at university hospitals and at other hospitals or private practices fig . 
while 71 % of participants stated an interest in this area , only 19 % rated their respective education as good and only 33 % were mostly satised with the cooperation between scientists and clinicians . 
with 33 % of positive ratings , the score for education in basic research was better than in the translational / clinical eld . in addition , 30 % of participants saw their interests in translational rather than in basic research and in free text questions the majority of answers stated that the cooperation between clinicians and scientists needed to be improved at the institutions and that the degro conferdiscussion the increasing incidence and prevalence of malignant diseases due to the growing life expectancy in the developed world creates a demand for qualied experts in all oncologic disciplines including radiation oncology [ 4 , 5 ]  . 
however , there is evidence from both europe and the united states that suggests that the supply of radiation oncologists might not keep pace with these trends [ 4 , 5 ]  . 
5 questions / statements 3840 i have a basic interest in translational / clinical training ; the education and training in the translational / clinical eld is satisfactory and the education and training in basic research is satisfactory for radiation biologists strahlenther onkol ( 2016 ) 192 : 507515 interest in transla ( cid : 2 ) onal / clinical educa ( cid : 2 ) on transla ( cid : 2 ) onal / clinical educa ( cid : 2 ) on basic research educa ( cid : 2 ) on strongly agree agree partly disagree strongly disagree not relevant not answered there is a lack of data projecting the need for medical physicists in radiation oncology . 
a survey performed by the astro in 2007 raised concerns in terms of education in radiation biology because there was a signicant decline in teaching experts in radiation biology educators who had received graduate training in radiation biology themselves . furthermore , the mean age of experts in charge of radiation biology education for residents in radiation biology was 52 years [ 8 ]  . previous surveys from germany and other countries have demonstrated that the satisfaction with the residency and the profession itself is high among radiation oncologists [ 6 , 7 , 9 ]  . 
however , allocation of working time to research and teaching activities was suboptimal . the results of our survey conrm that there is a high interest in research activities among the respondents . 
the residents rst choice of an academic career varied from 14 to 33 % between 2000 and 2002 , while 38 to 54 % stated that they wish to join a private practice [ 11 ]  . 
our survey also shows that the nancial support for attending professional education events or conferences is suboptimal as 43.4 % reported minimal or lack of compensation for registration fees or travel costs . 
this is in line with the ndings of a survey conducted among the young members of the italian association of radiation oncology ( airo ) [ 12 ]  . regarding the contents of the residency and training in medical physics , national and international guidelines have been published [ 1315 ]  . 
in one of the previous degro surveys , 71 % of participants stated that there was no designated person in charge of the residency curriculum at their institution [ 7 ]  . 
as shown in our survey , there is room for improvement regarding the professional development of physicians , physicists and radiation biologists including regular individual progress meetings , nancial support for professional education and conferences , facilitation of clinical rotations and implementation of educational and teaching programs for physicists . to our knowledge , there are no specic guidelines for the training of future radiation biologists . 
it needs to be mentioned , however , that the total number of participating radiobiologists was comparably low and there may also be a selection bias towards biologists with stronger interest in translational research taking part in our survey . 
in the airo survey , knowledge of radiation biology was described as moderate or poor by 72.1 % of participating physicians [ 12 ]  . there are some limitations to this survey . 
the distribution of the invitation through the degro mailing list and contacts at university hospitals has likely lead to an underrepresentation of young professionals employed at nonacademic hospitals and private practices . 
this was , however , a deliberate decision of the ydegro to allow maximum inclusion of subjects willing to contribute to the program of the ydegro . in summary , our survey provides important insight into the current situation of training and education in radiation strahlenther onkol ( 2016 ) 192 : 507515 oncology , medical physics and radiation biology . 
these ndings should be employed to further improve the training and research perspectives of young radiation oncologists , physicists and radiation biologists and will form the basis for the future working program of the ydegro . conclusion based on the results of this survey , the ydegro has proposed a list of activities for the upcoming years . 
this includes improving access to technical information and professional education regarding the residency as well as education for medical physicists and radiation biologists , enhancing the interdisciplinary knowledge exchange between physicians , medical physicists and radiation biologists through clinical and research mobility grants , establishing a research network ( ytrialists ) providing the infrastructure to perform clinical and translational studies in conjunction with the arbeitsgemeinschaft radiologische onkologie and facilitating active participation of young physicians , physicists and biologists in committees , working groups , conferences and other relevant activities of the degro . the feasibility and success of these measures will be determined by performing follow - up surveys on the subject matter . acknowledgements we would like to thank the degro board for providing nancial support for several group meetings as well as for the great general support and trust in the ydegro . 
niyazi declare that they have no competing interests . ethical standards the accompanying manuscript does not include any studies on humans or animals performed by any of the authors . strahlenther onkol ( 2016 ) 192 : 507515 male , female university hospital , tertiary hospital , community hospital , private practice medicine , medical physics , biology degro , estro , other ( free text ) 012 months , 1324 months , 2536 months , 3760 months strongly agree agree partly disagree strongly disagree not relevant strongly agree agree partly disagree strongly disagree not relevant strongly agree agree partly disagree strongly disagree not relevant appendix table a 1 survey questions / statements general questions 1 . 
what would you like to change in your hospital and how ? ( free text ) strahlenther onkol ( 2016 ) 192 : 507515 table a 1 survey questions / statements ( continued ) physics profession ( physicists only ) 30 . 
aebersold12 volker budach1 received : 7 march 2016 / accepted : 10 may 2016 / published online : 20 june 2016 springer - verlag berlin heidelberg 2016 abstract background to determine the inuence of baseline laboratory values on treatment outcome in patients with locally advanced head and neck cancer ( hnscc )  . methods data of the randomized trials aro 95 - 06 ( n = 384 ) and sakk 10 / 94 ( n = 224 ) were pooled for a total sample size of 608 patients . 
gallen , switzerland 10 department for head and neck surgery , charit universitaetsmedizin berlin , berlin , germany 11 clinique de genolier , genolier , switzerland inselspital , bern university hospital , and university of bern , bern , switzerland strahlenther onkol ( 2016 ) 192 : 552560 with locoregional recurrence - free survival ( lrrfs ) , distant metastasis - free survival ( dmfs ) , cancer - specic survival ( css ) , and overall survival ( os ) was analyzed using univariable and multivariable cox regression models . results a total of 580 and 564 patients were available with baseline hb and cr values in the pooled analysis . univariable analyses revealed that lower baseline hb values were signicantly associated with decreased lrrfs , dmfs , css and os . 
increased baseline cr remained signicantly associated with improved os in patients who underwent crt ( hr 0.79 , 95 % ci 0.690.92 , p = 0.002 ) but not in those patients who underwent rt alone . conclusions an association between lower baseline hb and inferior treatment outcome was conrmed . 
baseline cr was introduced as a prognosticator of outcome after crt for locally advanced hnscc . keywords carcinoma , squamous cell of head and neck radiation therapy chemotherapy hemoglobin creatinine ergebnisse insgesamt waren 580 und 564 patienten mit hbund kreatininwerten in der gepoolten analyse verfgbar . 
ein erhhter baseline - kreatininwert blieb signikant assoziiert mit einem verbesserten os bei patienten mit simultaner rct ( hr 0 , 79 , 95 % - ki 0 , 690 , 92 , p = 0 , 002 ) , aber nicht im rahmen der alleinigen bestrahlung . schlussfolgerung es besttigte sich ein zusammenhang zwischen niedrigen baseline - hmoglobinwerten und unterlegenem outcome . 
der baseline - kreatininwert wurde als neuer prognostischer faktor fr die behandlungsergebnisse der kombinierten rct bei fortgeschrittenen kopf - halstumoren eingefhrt . schlsselwrter kopf - hals - plattenepithelkarzinome radiotherapie chemotherapie hmoglobin kreatinin background hmoglobinund kreatininwerte als prognostische outcome - faktoren nach simultaner radiochemotherapie lokal fortgeschrittener kopfhals - tumoren sekundre ergebnisse von 2 randomisierten europischen phase - iii - studien ( aro95 - 06 , sakk 10 / 94 ) zusammenfassung hintergrund untersucht werden sollte der einuss von baseline - laborwerten auf das outcome der behandlung von patienten mit fortgeschrittenen kopf - hals - tumoren . methoden daten der randomisierten studien aro 95 - 06 ( n = 384 ) und sakk 10 / 94 ( n = 224 ) wurden gepoolt , die gesamtzahl von 608 patienten wurde untersucht . 
der einuss der prtherapeutischen hmoglobin ( hb ) und kreatininwerte auf das lokoregionre rezidivfreien berleben ( lrrfs ) , das fernmetastasenfreie berleben ( dmfs ) , das krebsspezische berleben ( css ) und das gesamtberleben ( os ) wurde unter verwendung uniund multivariabler cox - regressionsmodelle untersucht . denitive radiation therapy ( rt ) usually administered with concurrent platinum - based chemotherapy is one recommended type of treatment for patients with locoregionally advanced squamous cell head and neck cancer ( hnscc ) who desire organ preservation , and for those who have surgically unresectable disease [ 1 , 2 ]  . altered - fractionation rt schedules , including accelerated rt and hyperfractionation , have been investigated to overcome accelerated repopulation and to safely escalate the dose , respectively . 
accelerated fractionation improves locoregional recurrencefree survival ( lrrfs ) , but its effect on os is less clear [ 3 , concomitant chemotherapy has been described to improve os as compared to rt alone [ 2 , 5 , 6 ]  . 
however , despite combined treatment , prognosis for patients who present with locally advanced ( stage iii or iv ) disease is 554 strahlenther onkol ( 2016 ) 192 : 552560 poor . 
the surveillance , epidemiology and end results ( seer ) cancer statistics review for the years 19752007 reports a 5 - year relative survival for locally advanced oral cavity and oropharyngeal cancer of 55 % , in contrast to 83 %for early stage disease [ 7 ]  . for patients with oropharyngeal hnscc , favourable prognosis is associated with the proof of hpv positivity , both for primary as well as for post - op radiochemotherapy [ 8 ]  . 
for patients with locoregionally advanced oropharyngeal cancer , hpv is associated with long - term local control rates of approximately 80 % in the primary situation [ 9 ] and of almost 100 % in the post - op situation . combined chemoradiation has been described to be associated with increased toxicity , which may have a more adverse effect on survival , function and quality of life than has been previously recognized [ 10 ]  . 
thus , every effort should be made to identify predictors for treatment outcomes to be able to escalate or de - escalate treatment intensity for certain subgroups of patients to improve cancer control and to decrease late toxicity . methods and patients the data of the two randomized trials aro 95 / 06 and sakk 10 / 94 were pooled . aro 95 / 06 in a multicentric , prospective randomized trial on 384 patients with locally advanced hnscc who were randomized to hyperfractionated accelerated rt with 77.6 gy ( hart ) or hart with 70.6 gy combined with 5 - uorouracil ( 5fu ) 600 mg / m as continuous infusion during days 15 and mitomycin c ( mmc ) 10 mg / m as a single intravenous bolus injection on days 5 and 36 , respectively ( c - hart )  . the primary endpoint was locoregional control ( lrc )  . 
secondary endpoints were os , cancer - specic survival ( css ) , late treatment - related toxicity , and quality of life . a creatinine of > 1.5 mg / dl or a creatinine clearance 80 ml / min was an exclusion criterion for this trial . 
the trial was registered at the national institutes of health ( identiﬁer number : nct00002654 )  . both trials were approved by the local ethics committees of all participating centers and have therefore been conducted in accordance with the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . the pooled total sample size was 608 patients . 
baseline laboratory values available for analysis in both trials were haemoglobin ( continuous variable , n = 580 ) and creatinine ( continuous variable , n = 564 )  . 
the inuence of the baseline laboratory values on the time - to - event endpoints was assessed in the pooled data set using univariable cox regression models with trial as random effect as well as by trial and by treatment arm separately using univariable cox regression models . 
statistical analyses were performed using sas version 9.2 ( sas institute inc . , cary , nc , usa )  . patient characteristics for the trials were summarized in table 1 . a total of 580 patients were available with baseline haemoglobin values in the pooled analysis . 
univariable analyses revealed that lower baseline haemoglobin values were signicantly associated with decreased lrrfs ( hazard ratio [ hr ] 0.85 , 95 % condence interval [ ci ] 0.740.96 , p = 0.01 ) , decreased dmfs ( hr 0.82 , 95 % ci 0.700.96 , p = 0.01 ) , decreased css ( hr 0.74 , 95 % ci 0.640.86 , p < 0.001 ) and decreased os ( hr 0.76 , 95 % ci 0.680.86 , p < 0.001 ; table 2 )  . 
this effect remained signicant for os when the treatment arms ( rt alone vs . chemoradiation ) were analyzed separately ( data not shown )  . a total of 564 patients were available with baseline creatinine values . 
for none of the endpoints a significant association with baseline creatinine clearance could be shown , neither in the pooled analysis nor by treatment or by trial ( supplementary tables 1 , 2 , 3 and 4 )  . in the multivariable cox regression model lower baseline haemoglobin remained associated with decreased os both in the patients who received chemoradiation ( hr 0.79 , 95 % ci 0.660.94 , p = 0.009 ; table 5 ) and in those patients who underwent rt alone ( hr 0.67 , 95 % ci 0.580.78 , p < 0.001 ; table 6 )  . 
the impact of anaemia on treatment outcome in patients with squamous cell carcinoma of the larynx and pharynx was conrmed in the dahanca 585 study where the use of the radiosensitizer nimorazole in association with rt was shown to signicantly improve lrc and css [ 13 ] and multivariable analysis in the study of denis et al . 
the nding however that anaemia correlates with inferior lrc among patients treated with surgery alone suggests that anaemia may inuence outcome in head and neck cancer patients also independent of its inuence on hypoxic radioresistance [ 15 ]  . attempts were made to overcome the negative effect of low baseline haemoglobin the dahanca 5 and 7 protocols including a total of almost 1200 head and neck cancer patients , low haemoglobin patients were subrandomized to red blood cell transfusion or no transfusion . 
these studies showed that transfusions to patients with haemoglobin level below 13 g / dl in females and 14.5 g / dl in males , raised the haemoglobin levels and brought these patients into the high haemoglobin group . 
moreover , the role of erythropoiesis - stimulating agents ( esas ) have been investigated in several trials and a 2012 cochrane review of 91 trials with 20 , 102 participants came to the conclusion that esas increase mortality during active therapy ( on - study mortality , hr 1.17 , 95 % ci 1.061.29 ) , and modest evidence that they increase overall mortality ( hr 1.05 , 95 % ci 1.001.11 ) [ 16 ]  . little is known regarding the prognostic effect of baseline creatinine in patients undergoing chemoradiation . 
cn0 - 1 haemoglobin at baseline creatinine at baseline crt chemoradiation therapy , rt radiation therapy , os overall survival , css cancer - specic survival , lrffs locoregional recurrence - free survival , dmfs distant metastasis - free survival , hr hazard ratio , ci condence interval aiqr normalized for easier interpretation ous to rt into the context of kidney function . 
interestingly our data suggest that impaired kidney function , although in the range of values allowing application of chemotherapy in these trials , is associated with better prognosis in those patients receiving chemoradiation but not in the patients receiving rt alone . 
the reason for the identied association between baseline creatinine values and outcome parameters remains thus to be elucidated . besides the results for the mentioned laboratory values our analysis revealed that gender , age , performance status , tumour site , tumour classication and nodal classication were signicantly associated with outcome after chemoradiation or rt alone , however , most of these associations have been described before [ 5 , 6 ]  . a limitation of our analysis is , however , that there are several other factors with known inuence on kidney function as other diseases , co - medication , uid restriction etc . , which were not available for analysis in the two analyzed trials [ 17 , 18 ]  . 
another limitation is that baseline lab values were not available for analysis in several of the patients . strahlenther onkol ( 2016 ) 192 : 552560 also it has to be acknowledged that this was an unplanned retrospective analysis of the two trials and the data is therefore of exploratory nature . it remains currently unclear which interventions might be based in clinical practice on haemoglobin and creatinine assessment . 
as red blood cell transfusions or esas do not improve the prognosis of patients with low baseline haemoglobin , low baseline haemoglobin at present remains a prognostic factor for poor outcome in patients with locally advanced hnscc . 
regarding baseline creatinine it is necessary to conrm this parameter as a prognostic parameter in currently ongoing prospective trials for patients undergoing chemoradiation , and if conrmed , to characterize this association in more detail . conclusion our data from a secondary joint analysis of two randomized trials conrm published knowledge regarding baseline haemoglobin as a prognostic parameter and introduce baseline creatinine as a novel predictor of outcome after chemoradiation for locally advanced hnscc . availability of data and materials the databases for the trials are managed by the sakk coordinating center ( sakk 10 / 94 ) or the department of radiation oncology , charit universittsmedizin berlin ( aro 95 - 06 ) and are not publicly available . trial registration aro 95 - 06 was registered with the german cancer society and sakk 10 / 94 was registered at the national institutes of health ( identier number : nct00002654 ) acknowledgements for the aro 95 - 06 trial the following contributors enrolled patients into the trial without meeting the criteria for authorship : w . 
v. the sakk 10 / 94 trial was supported by the swiss state secretariat for education , research and innovation ( seri )  . compliance with ethical guidelines conict of interest p ghadjar , c . 
in this study the accuracy of dir for registration of planning ct ( pct ) and recurrence ct ( rct ) images of head and neck squamous cell carcinoma ( hnscc ) patients was evaluated . patients and materials twenty patients treated with denitive imrt for hnscc in 20102012 were included . 
one observer manually contoured eight anatomical regions - of - interest ( roi ) twice on pct and once on rct . methods pct and rct images were deformably registered using the open source software elastix . 
die studie evaluiert die treffsicherheit der dir bei der registrierung von planungs - ct - bildern ( pct ) und ct - scans des rezidivs ( rct ) bei patienten mit plattenepithelkarzinomen im kopf - hals - bereich ( hnscc )  . patienten und methoden mithilfe der dir wurden planungs - ct und rezidiv - scans von 20 hnscc - patienten analysiert ; alle waren zwischen 2010 und 2012 mit intensittsmodulierter strahlentherapie behandelt worden . 
zur beurteilung der gte der registrierung wurden msd ( mean surface distance ) und der dice - koefzient ( dsc ) zwischen den konturen bestimmt . um etwaige unsicherheiten bei der konturierung abschtzen zu knnen , wurde der msd der roi im pct als auch in der wiedereinzeichnung verglichen . 
dir und manuelle konturierungsunsicherheiten wurden mit gewebsvolumen und - rigiditt korreliert . ergebnisse der msd liegt zwischen 13 mm fr verschiedene roi in der dir und zwischen 1 und 1 , 5 mm fr wiederholt eingezeichnete rois auf dem pct . 
der dsc bei dir variierte zwischen 0 , 58 und 0 , 79 fr weichteilgewebe und war 0 , 79 fr kncherne strukturen , er korrelierte mit den volumina der roi ( r = 0 , 5 , p < 0 , 001 ) und mit der gewebsrigiditt ( r = 0 , 54 , p = 0 , 001 )  . schlussfolgerung die deformierbare bildregistrierung hnscc - patienten ist an pct und rct durchfhrbar . 
die methodenunsicherheit liegt in der grenordnung der voxelgre des planungs - ct . schlsselwrter computertomographie validierung elastix kopf - hals - bereich introduction optimal image registration is crucial for radiotherapy planning , delivery and outcome evaluation . 
however , anatomy and posture changes are usually nonrigid and therefore require a different approach . image registration in the head and neck region is challenging , especially if the patient is positioned with different degrees of exion , extension and rotation between scans . thus , use of rigid image registration is often not sufcient to link the images to each other with an acceptable accuracy . deformable image registration ( dir ) or nonrigid registration can account for complex nonlinear transformations of patient anatomy . 
therefore , validation of various dir algorithms is mandatory for each application and anatomical site to assess the precision and accuracy of the method . developed and validated by klein et al . [ 7 ] elastix is a freeware toolbox [ 6 ]  . it is a collection of parametric intensity - based registration methods , enabling deformable registration by constructing the algorithm , tailored to a specic application . 
the advantage of using this method is the free availability and the ability of different institutions to reproduce the results by applying the same parameter les . this study aims to validate dir using elastix between ct recurrence scans and original treatment planning scans in the head and neck region . materials and methods twenty patients with radiological conrmed recurrence of head and neck squamous cell carcinoma ( hnscc ) were randomly selected from a larger cohort of patients with locally advanced hnscc treated with imrt between 2010 and 2012 . 
recurrence scans were obtained after clinical suspicion of locoregional failure during a followup period of up to 2 years . the planning ct ( pct ) was obtained during the clinical ct simulation based on a standard local protocol : patients were scanned from the supraorbital margin to 4 cm below the clavicles , obtaining images with slice thickness of 3 mm using a source potential of 120 kv . 
different structures were selected to reect possible differences in dir validation . the second contour on pct performed 2 weeks after the rst delineation was used to disentangle the uncertainty of delineation from the uncertainty of the dir method . 
since the re - delineation was performed on the original image , no deform registration was needed for the comparison and the observed uncertainty would be a measure of re - delineation precision . 
if the two types of uncertainty ( dir and delineation ) were independent , an estimated value of the uncertainty of dir could be calculated using the equation : msd2 total = msd2 dir + msd2 del in the second comparison metric was based on the dice similarity coefcient ( dsc )  . 
more precisely , the dsc value was calculated as : dsc = 2 ( vroiaroib ) vroia + vroib where the v values are the volume of the intersection of the original and deformed roi , the volume of the original roi , and the volume of the deformed roi , respectively . correlation values between dsc and roi volumes and the rois likelihood of structural change over time ( spinal cord , mandible and vertebrae c35 vs . thyroid gland , right / left parotid and submandibular glands ) were calculated . results the deformable registrations were successful for all image sets for the 20 patients . 
except for an increased uncertainty in the cranialcaudal direction ( which is the direction where the image voxel is longest ; in this case 3 mm ) , no apparent spatial specic variations were common for all the patients . table 1 shows variations of volume , msd values and averaged dsc values across the different organs . 
the combined delineation and deformation uncertainty was approximately twice the uncertainty related to the manual delineation . when delineation uncertainty was excluded from the calculation , no correlation was found between the uncertainties fig . 
the warped roi ( roi - b ) were subsequently compared with the roi delineated on the pct scans ( roi - a ) image registrations of pct and rct were performed for all 20 patients using the open source software elastix , [ 7 ] and applied in our instituadapted from klein et al . tion as described by brink et al . 
neither were there any correlations within a specic organ over the included patients ( spearman correlation between sd of surface maps for dir and delin for the individual patients )  . the highest dsc was found for the two bony structures and the spinal cord , whereas the submandibular glands and the thyroid gland had the lowest dsc ( table 1 )  . 
signicant differences were seen between dsc and volumes of the rois ( spearman correlation coefcient 0.6 , p < 0.001 ) and between dsc in soft tissues versus bony structures and spinal cord ( p < 0.001 , using wilcoxon signed rank test )  . discussion the current study has demonstrated that the open software elastix can be used for reliable deformable registration of planning and recurrence ct in the head and neck area . dir is frequently incorporated in different parts of the radiotherapy chavalidation of dir algorithms are therefore important and may for some clinical or research applications be crucial for the interpretation of the results . only few studies have described dir for planning ct and recurrence ct registration [ 5 , 13 ] , and these studies did not optimally report the results of validation method . 
this study was initiated to validate if dir is sufciently robust to account for the advanced deformations in anatomy , such as locoregional failures in the head and neck region , and over a longer period . 
using planning and diagnostic ct scans from 20 patients , we found that dir using elastix in the head and neck area is valid . validation of dir is a challenging task because there are no standardized means of evaluating the results of a dir method . 
validation can be performed using a mathematical or a physical phantom [ 14 , 15 ] , or by propagation of rois or identied points between registered images [ 14 ]  . 
with patient images , the commonly used approach requires experts to dene rois ( landmarks ) in all registered images and to compare positions dened by experts to positions obtained with dir . in this study we performed validation using patient images and evaluated the method by measuring the mean surface distance ( msd ) between the surfaces of rois , and dsc , a spatial overlap between rois . the results showed msd of 23 mm in all directions for the majority of rois , indicating registration accuracy at or near the voxel length ( 3 mm ) of the planning ct images . only cervical vertebrae had msd above 3 mthis could be explained by the anatomical inhomogeneity of these upper cervical structures , imaging using 3 mm slices , as well as small differences in neck exion that would dene the vertebrae differently on pct and rct which is difcult to correct by dir . in this study , one observer was chosen to delineate rois once on pct and twice on rct to estimate interobserver delineation uncertainty . 
msd values of 23 mm are thus as low as can be expected for the current situation . most validation studies used dsc to express the spatial overlap between two structures relative to their volumes . our ndings were generally in accordance with studies that used intensity - based algorithms , with slight variations for the submandibular and parotid glands [ 10 , 14 , 20 ]  . 
the thyroid gland has often more pronounced anatomical changes between the planning and recurrence scans caused by the shrinkage or dislocation of the organ . in contrast , more xed and voluminous bony structures had the highest values . 
the relation between volume and dsc showed that dsc values obtained for different organs were difcult to compare and no specic dsc value could be dened to correspond to a high degree of overlap . for intensity - based algorithms , such as elastix , image similarity metrics , for instance target registration error [ 16 , 21 ] , distance - to - agreement [ 17 ] , hausdorff distances [ 10 , 20 ] , average surface distance [ 20 ] or correlation coefcient [ 18 ] may also be used to describe the accuracy in matching anatomical landmarks between two images . 
this approach represents the typical distance deviation that is useful in many evaluations of overall accuracy and precision of a given method . conclusion this validation study showed that dir using an open source system in head and neck region on planning ct and recurrence ct images is feasible and reliable with an internal accuracy close to the voxel length of the planning ct images . acknowledgements this project was supported by the region of southern denmark , the danish cancer research foundation , and the department of oncology , odense university hospital . strahlenther onkol ( 2016 ) 192 : 545551 compliance with ethical guidelines conict of interest r . 
brown1 christoph glanzmann1 gerhard huber2 marius bredell3 tamara rordorf4 gabriela studer1 received : 11 january 2016 / accepted : 21 april 2016 / published online : 15 june 2016 the author ( s ) 2016 . 
our aim was to investigate the outcome of patients aged 80 + years undergoing curative intent intensityor volume - modulated radiation therapy ( imrt / vmat )  . methods we retrospectively reviewed our hnt patients aged 80 + treated with curative imrt / vmat from december 2003 to november 2015 . 
outcome results were compared with that of a younger hnt patient cohort from our hospital . results a total of 140 consecutive patients were included ( 65 postoperative , 75 denitive )  . 
of the 140 patients , 80 were alive with no evidence of disease when last seen , 28 had died due to ( cid : 2 ) prof gabriela studer gabriela.studer@luks.ch 1 department of radiation oncology , head neck cancer center , university hospital zurich , raemistrasse 100 , 8091 zurich , switzerland 2 department of otorhinolaryngology , head neck cancer center , head and neck surgery , university hospital zurich , zurich , switzerland 3 department of craniomaxillofacial and oral surgery , head neck cancer center , university hospital zurich , zurich , switzerland 4 department of medical oncology , head neck cancer center , university hospital zurich , zurich , switzerland the cancer , 12 remained alive with disease , the remaining 20 died intercurrently . 
hospitalization and feeding tube rates were 26 % and 11 % , respectively . the 2 - / 3 - year lc , dfs , and os rates for the entire cohort were 81 / 80 % , 69 / 63 % , and 68 / 66 % , respectively . 
squamous cell carcinoma ( scc ) patients showed an inferior 3year os rate as compared to non - scc patients ( 62 % vs 77 % , p = 0.0002 ) , while lc and dfs did not differ . 
corresponding rates for > 1400 hnt patients < 80 years treated during the same time interval were 81 / 80 % , 69 / 67 % , and 77 / 72 % , respectively . conclusions treatment tolerance in our patients aged 80 + was high . 
these results suggest that elderly hnt patients should not be denied potentially curative treatment strategies . keywords elderly treatment outcome radiotherapy of elderly patients survival analysis radiation tolerance imrt / vmat zur behandlung von malignomen im kopf - hals - bereich outcome bei ber 80 - jhrigen patienten zusammenfassung ziele das therapeutische vorgehen bei betagten patienten mit kopf - hals - tumoren ( kht ) ist anspruchsvoll . 
ziel war es , therapieerfolg und strahlenther onkol ( 2016 ) 192 : 526536 - toleranz unserer kurativ intensittsoder volumenmoduliert radiotherapierten ( imrt / vmat ) patienten im alter von > 80 jahren zu evaluieren . methoden zwischen dezember 2003 und november 2015 an unserer klinik kurativ imrt / vmat - behandelte khtpatienten im alter von > 80 jahren wurden retrospektiv analysiert . 
das mittlere / mediane alter bei behandlungsbeginn betrug 84 , 8 / 84 , 1 jahre ( 8096 ) , die mittlere / mediane verlaufsbeobachtungszeit 25 / 16 monate ( 292 )  . bei letztkontakt waren von den 140 patienten 80 patienten krankheitsfrei am leben , 28 verstarben am tumorleiden , 12 lebten mit krankheitsmanifestationen , 20 verstarben interkurrent . 
die korrespondierenden raten fr unsere > 1400 imrt / vmatkht - patienten < 80 jahren betrugen 81 / 80 % , 69 / 67 % und 77 / 72 % . fazit die behandlungstoleranz unserer patienten im alter > 80 war hoch . 
dieses ergebnis spricht dafr , betagten patienten ein potenziell kuratives vorgehen nicht vorzuenthalten . schlsselwrter betagte behandlungserfolg radiotherapie im alter berlebenszeitanalyse strahlentoleranz introduction elderly patients with malignant head - and - neck tumors ( hnt ) pose a therapeutic challenge . 
they are often ineligible for systemic therapy and participation in clinical trials due to their advanced age and may have signicant comorbidities that inuence their ability to tolerate tumorspecic therapies . 
chemotherapy may be combined with radiation in cases of locally advanced disease with no contraindications to systemic treatment ; however , the role of chemotherapy in elderly patients remains controversial as the meta - analysis of chemotherapy in head and neck cancer ( mach - nc ) demonstrated a diminishing effect on survival with increasing age [ 1 ]  . hnt is typically a cancer of the elderly population and u.s. 
dening elderly remains problematic and is often based on chronological age alone . the national institute on aging and national institutes of health have dened 3 categories : young old ( 6574 years ) , older old ( 7585 years ) and oldest old ( > 85 years ) [ 4 ]  . 
it is prudent to consider and improve upon methods by which elderly patients will be assessed for curative therapies [ 5 ] and to determine the outcomes for treatment in order to provide adequate and accurate information to patients . the optimal radiotherapeutic management of elderly hnt patients cannot be easily dened at present , due to the paucity of randomized data , particularly of very elderly patients . 
two multimorbid patients selected for curative radiation were excluded from this analysis : in one patient , imrt was prematurely interrupted ( 3 fractions of 2 gy ) due to a sacrum fracture following a fall ; a second patient developed cardiopulmonary decompensation following surgery prior to the start of radiation and did not sufciently recover to commence curative radiation ( 2 of 142 patients with intention to treat )  . patterns of care , including treatment modalities received ( surgery , radiotherapy , chemotherapy , immunotherapy ) and ambulant or inpatient treatment were evaluated . 
further patient , tumor and treatment characteristics were collected , including age , ecog performance status ( ps ) at the time of initial radiation oncology consultation , radiotherapy dose , and fractionation . 
approval from the local ethics committee was obtained for data evaluation of our imrt / vmat cohort . patients were immobilized in the supine position from the vertex to shoulders with commercially available thermoplastic masks . 
no specic modications of our planning target volume ( ptv ) concepts were performed , except in a few patients with very large gross tumor volume ( gtv ) , whereby the gtv was individually dened as ptv70 gy , with a margin of approximately 0.5 to 1 cm dened as ptv68 gy . 
an extended eld simultaneous integrated boost ( sib ) - imrt technique , whereby the primary tumor and regional lymph nodes are covered in a single phase by a 6 - mv dynamic mlc system ( varian medical systems , palo alto , ca , usa ) using a sliding window technique , or alternatively a vmat technique , was used [ 7 ]  . 
adjuvant chemotherapy consisted of carboplatin auc 5 and 5 - uorouracil ( 5 - fu ) 1000 mg / m2 ( 6 cycles ) and was given to one patient . 
no cisplatin - based systemic therapy was given in this elderly patient subgroup . follow - up patients were seen weekly during the course of radiotherapy , or more frequently as required . 
worst grade of late toxicity was scored according to the radiation therapy oncology group ( rtog ) / european organization for research and treatment of cancer ( eortc ) radiation morbidity criteria . detailed treatment toxicity data were not analyzed for the younger imrt cohort in the statistical analysis ; therefore , no comparison was performed with the elderly cohort . kaplanmeier survival curves were performed using the statview ( version 4.5 ) statistics prograp values < 0.05 were considered statistically signicant . statistics results patient and tumor characteristics a total of 140 patients aged 80 + years out of 1606 ( 9 % ) consecutively curatively treated patients with mucosal ( 98 / 140 ) and nonmucosal hnt were identied from our database and included in this analysis ( table 2 )  . 
mean / median follow - up time was 25 / 16 months ( range 292 months )  . more than 60 % of all patients presented with advanced t3 / 4 , and / or n2c / n3 , or recurrent disease after previous surgery alone . data from our younger imrt cohort aged < 80 years was evaluated and compared with the elderly group . 
both the > 80 and < 80 year subgroups showed approximately 50 % t3 / 4 primary stage tumors , while the advanced nodal status ( n2c / n3 ) was 20 % for younger patients and 11 % for the older cohort . 
imrt was postoperatively delivered in 46 and 41 % of patients aged > 80 and < 80 years , respectively . 530 strahlenther onkol ( 2016 ) 192 : 526536 treatment tolerance of 140 patients , 36 ( 26 % ) required part or all of their treatment as an inpatient ( table 1 )  . 
the need for a feeding tube was inversely related to the age intervals : no tube was required in 19 patients > 90 years , 7 tubes in 36 patients aged 8590 years , 8 tubes in 85 patients aged 8085 years . all patients were able to complete treatment . 
total treatment times were maintained according to the initial schedule in 136 of 140 patients ( 74 % ) ; 4 patients had a treatment delay between 5 and 11 days . 
as this subgroup accounts for approximately 10 % of all patients referred for curative or postoperative imrt or vmat to our center , knowledge regarding tumor control and side effects is crucial . 
we chose an arbitrary age of 80 + years , as this was an age whereby treatment decisions were often challenging for our interdisciplinary team . this is , to our knowledge , the largest published group of older and oldest old hnt patients treated with modern radiation techniques ( table 3 ; [ 815 ] )  . 
treatment decisions made at our weekly interdisciplinary head and neck cancer center tumor board represent a selection process in favor of tter patients , as patients considered too ill or noncompliant to undergo treatment with potentially substantial side effects were not selected for curative radiation . 
we acknowledge that treatment tolerance may be different in this group as less mucosa may have been included in the radiation eld ; however , the radiation dose applied was very similar . 
patients with spinocellular carcinoma underwent extensive lymphatic pathway irradiation and were not at substantially lower risk for side effects than patients with , for example , early stage laryngeal carcinoma . 
we included 7 patients with nasal tumors ( including nasal mucosa only ) as a dose of 70 gy to the nose is not easy to tolerate at any age , which was our rationale for including these patients in our elderly cohort . 
as the aim of this analysis was to evaluate whether irradiating elderly hnt patients with curative intent is benecial compared to its potential risk , we included all patients irrespective of mucosal or nonmucosal tumor origin . we also included postoperatively irradiated patients , as the question of the benetrisk ratio of postoperative radiation therapy is often difcult to decide in elderly patients . although these patients are exposed to a somewhat lower radiation dose , they underwent and survived a surgical procedure ; conversely , patients not t enough for surgery receive a higher radiation dose and are , thus , exposed to other potential risks . 
the risk level of the two approaches are difcult to compare and may be dependent on the individual patient , their comorbidities , their treatment wishes , or the potential treatment bias of the treating physicians . the study was also limited by the retrospective nature of the analysis . 
the limited follow - up of our patients can also be attributed to their age and other comorbid or social problems , which prevented their attendance for ongoing followthe total number of patients with theoretically curable malignant hnt who were not selected for curative treatment is not available to us , however is estimated to be low ( < 5 patients / year )  . 
in addition , having a diagnosis of cancer at an advanced age and being an older individual who is well enough to attend for a specialist consultation , may already represent a substantial positive preselection for curative treatment . consistent with our own cohort , many of the published series conrm a high rate of treatment completion in the elderly population ( approximately 90100 % ) suggesting that patients either tolerate treatment well and / or were well selected to receive curative therapy . 
some of the published series show 5 - year os rates of 2030 % , reecting the inuence of reduced life expectancy in this group and the competing risk from comorbid conditions . 
we found only three further reports assessing patients 80 + ( zachariah et al . , n = 35 [ 11 ] , mitsuhashi et al . , n = 11 [ 12 ] , schoeld et al . , n = 98 [ 14 ] ) , therefore , limiting data comparison ( table 3 )  . there have been an increasing number of publications assessing the tolerance and outcome of radiochemotherapy regimens in elderly patients ( table 4 ; [ 1623 ] )  . 
when combined with the subgroup analysis nding of decreasing effect of chemotherapy with age in the mach - nc meta - analysis of chemoradiation trials , one needs to proceed with caution when offering combined modality therapy to elderly patients [ 1 ]  . 
 [ 24 ] study demonstrated on subgroup analysis that cetuximab had no benet in patients aged 65 years or older ; however , this analysis was underpowered due to small patient numbers aged greater than 65 years and age was not a study endpoint . 
 [ 25 ] reported on a phase ii study in elderly patients utilizing cetuximab in combination with imrt - sib , which conrmed rates of toxicity consistent with the bonner data [ 24 ]  . a randomized controlled trial is currently assessing the impact of comprehensive geriatric assessment ( cga ) on survival , function , and nutritional status in elderly hnc patients receiving standard care [ 26 ]  . 
the international society of geriatric oncology is addressing these issues and has undertaken a review of current best practice and priorities for research in radiation oncology for elderly patients [ 27 ]  . conclusions treatment tolerance in our patient cohort aged 80 + was high . 
juni 2016 springer - verlag berlin heidelberg 2016 hintergrund und fragestellung bislang war bei patienten mit lokoregionr fortgeschrittenen plattenepithelkarzinomen im hno - bereich ( hnscc ) , die unter kurativer zielsetzung mit einer radiochemotherapie ( rct ) behandelt wurden , der stellenwert einer geplanten halslymphknotenausrumung ( neck - dissektion , nd ) oder einer nachsorge nach vollstndigem ansprechen im pet - ct ungeklrt . 
bei bis zu 40 % der patienten werden in der nach rct durchgefhrten nd histopathologisch noch tumorresiduen gefunden , whrend andererseits patienten mit einer klinisch / radiologischen vollremission nur selten regionr rezidivieren . 
alle anderen wurden der nd zugefhrt . studienziel und - design die non - inferioritt der mit der pet - ct gefhrten indikationsstellung fr eine nd nach rct gegenber einer planmig in kurativer intention durchgefhrten nd sollte geprft werden . 
einschlusskriterien waren histologisch gesicherte plattenepithelkarzinome originalpublikation mehanna h , wong wl , mcconkey cc et al ( 2016 ) pet - ct surveillance versus neck dissection in advanced head and neck cancer . 
1 , 30625 hannover , deutschland des oropharynx , hypopharynx , larynx , der mundhhle oder zervikale cup , die klinisch oder radiologisch ( ct oder mrt ) einen n2oder n3 - nodalstatus ohne fernmetastasen aufwiesen . 
sie wurden randomisiert zwischen einer geplanten nd ( als kontrollgruppe ; entweder 4 wochen vor oder 48 wochen nach der rct ) oder einem pet - ct 12 wochen nach abschluss der rct . 
um eine gleichmige aufteilung der risikofaktoren zwischen den studienarmen zu gewhrleisten , wurde nach zentrum , zeitpunkt der nd , chemotherapieprotokoll , tumorlokalisation und tumor - / nodalstadium stratiziert . wenn nach abschluss der rct aber klinisch progrediente zervikale metastasen aufelen , wurden die patienten unmittelbar zur salvage - nd vorgestellt . 
als sekundre endpunkte waren das krankheitsspezische berleben , rckfallraten , lebensqualitt , komplikationsraten und gesundheitskonomische analysen ( quality adjusted life years , qaly ) deniert . ergebnisse zwischen 2007 und 2012 wurden 564 patienten in grobritannien randomisiert . 
fast 60 % erhielten eine simultane chemotherapie ( cht ) mit cisplatin , 30 % eine induktionstherapie mit taxanen und platcetuximab war zwar mglich , spielte aber nur eine untergeordnete rolle . 
in der subgruppenanalyse gab es abhngig vom hpv - status keine signikanten unterschiede zwischen beiden behandlungsarmen , wobei die hpv - negativen patienten erwartungsgem generell eine deutlich schlechtere prognose aufwiesen . die lebensqualitt war in beiden gruppen nicht wesentlich unterschiedlich . 
nur 6 monate nach der randomisation zeigte sich im c30 - status ein geringer vorteil fr die petct - gruppe , der sich aber nach 12 monaten nivellierte und nach 24 monaten vollstndig verschwunden war . 
die auf dem petct basierte beurteilung des therapieansprechens reduziert die indikation zur nd deutlich und spart damit insgesamt kosten ein . kommentar die vorliegende publikation ist eine schlsselstudie , welche die kombination von primrer rct beim lokoregionr metastasierten hnscc mit einer nd auf der basis eines mit der pet - ct gesttzten restagings prospektiv onkologisch absichert . 
damit wird eine lange whrende kontroverse hinsichtlich des fr dieses patientenkollektiv optimalen vorgehens beendet [ 1 ]  . die bisher einzige weitere randomisierte studie zu dieser fragestellung stammt aus dem jahr 2001 [ 2 ]  . 
viele prospektive und retrospektive fallsammlungen zeigten divergierende ergebnisse ( bersicht in [ 1 ] )  . letztlich setzte sich aus pragmatischen grnden die praxis durch , patienten mit einer nach denitiver rct vollstndigen tumorremission in der bildgebung eine elektive nd zu ersparen . 
zum anderen ist aus groen serien zum hnscc [ 3 ] und zum nasopharynxkarzinom [ 4 ] bekannt , dass mit zunehmender beobachtung die rate an histopathologisch vollstndigen tumorregressionen nach rct zunimmt . 
im hnostrahlenther onkol ( 2016 ) 192 : 589591 bereich werden erst 12 wochen nach der rct residuen denitiv als tumorpersistenz eingestuft [ 3 ]  . die sensitivitt einer alleinigen pet - untersuchung zum restaging nach rct nodal metastasierter hnscc wurde in einer groen metaanalyse aus 27 studien zusammengefasst [ 7 ]  . 
dabei war die spezitt signikant hher , wenn die untersuchung > 10 wochen nach abschluss der rct durchgefhrt wurde . hnliche ergebnisse , allerdings mit kleineren patientenzahlen , konnten auch fr die koregistrierung von pet und ct als pet - ct gewonnen werden , mit einem negativen vorhersagewert von 97 % [ 8 ]  . in der jetzt vorgelegten studie kann denitiv besttigt werden , dass die moderne pet - ct - bildgebung so sensitiv ist , dass ein verzicht auf eine nd bei patienten mit radiologisch vollstndiger tumorremission verantwortet werden kann . 
die dadurch eintretende verzgerung einer notwendigen nd auf 12 wochen fr patienten , die nicht vollstndig auf die rct ansprechen , verschlechtert die prognose nicht im vergleich zu patienten , die bereits vor diesem zeitpunkt eine elektive nd erhalten haben . allerdings muss aus methodischen grnden darauf hingewiesen werden , dass patienten mit einem n3 - status in der studie unterreprsentiert waren , so dass fr diese subgruppe keine gesicherten aussagen gemacht werden knnen . erstaunlich bei diesem vorgehen ist der geringe effekt auf die lebensqualitt , die durch den verzicht auf die geplante nd ( also auf eine zustzliche operation bei allen patienten ) nur temporr geringfgig messbar ist . fazit die hier besprochene studie beantwortet eine wesentliche onkologische fragestellung , und kann deshalb als practice changing eingestuft werden . 
eine positive nutzenbewertung durch den gemeinsamen bundesausschuss sollte auch fr unsere kassenpatienten die regulre anwendung der pet - ct in dieser onkologischen situation ermglichen , um ber die weitere therapie ( nd oder nachsorge ) zuverlssig entscheiden zu knnen . robert michael hermann , westerstede , und hans christiansen , hannover literatur 1 . 
hermann rm , christiansen h , rdel rm ( 2013 ) lymph node positive head and neck carcinoma after curative radiochemotherapy : a long lasting debate on elective post - therapeutic neck dissections comes to a conclusion . 
francois y , nemoz cj , baulieux j et al ( 1999 ) inuence of the interval between preoperative radiation therapy and surgery on downstaging and on the rate of sphincter - sparing surgery for rectal cancer : the lyon r90 - 01 randomized trial . 
isles mg , mcconkey c , mehanna hm ( 2008 ) a systematic review and meta - analysis of the role of positron emission tomography in the follow up of head and neck squamous cell carcinoma following radiotherapy or chemoradiotherapy . 
nayak jv , walvekar rr , andrade rs et al ( 2007 ) deferring planned neck dissection following chemoradiation for stage iv head and neck cancer : the utility of pet - ct . 
the median interval between surgery and rt was 5 months ( range 211 months )  . results two months after completion of rt , 4 patients had achieved complete radiologic remission . 
the other 3 patients ( cases 2 , 4 , and 5 ) remain alive with no evidence of disease 59 , 46 and 90 months after therapy , respectively . conclusion overall , the 5 patients survived for a median of 48 months ( range 2590 months ) from the time of initial diagnosis and they tolerated the rt well , without severe acute or late onset toxicities . 
the results imply a potential survival gain after irradiation at acceptable toxicity level . keywords central nervous system toxicity children tomotherapy intensity - modulated radiotherapy atrt langzeitberleben nach additiver radiotherapie bei patienten mit atypischem teratoiden rhabdoidtumoren zusammenfassung hintergrund atypische teratoide rhabdoidtumore ( atrt ) sind eine hoch aggressive erkrankung embryonalen ursprungs und reprsentieren < 5% aller pdiatrischen tumore des zentralen nervensystems ( zns )  . patienten und methoden wir beschreiben eine fallserie von 5 patienten mit atrt des zns . 
eine dreidimensionale ( 3d ) konformale rt oder intensittmodulierte rt ( imrt ) wurde mit einer mittleren dosis von 54 gy ( spanne 50 , 459 , 0 gy ) in einer tglichen fraktionierung von 1 , 8 gy durchgefhrt . 
das mediane intervall zwischen operation und rt betrug 5 monate ( spanne 211 monate )  . 570 strahlenther onkol ( 2016 ) 192 : 569581 ergebnisse zwei monate nach abschluss der rt zeigten 4 patienten eine komplette radiologische remission . die mediane ereignisfreie berlebenszeit betrug 46 monate ( spanne 1090 monate )  . 
die anderen 3 patienten ( fall 2 , 4 und 5 ) sind bisher 59 , 46 und 90 monate nach der behandlung tumorfrei . zusammenfassung die mediane gesamtberlebenszeit seit erstdiagnose betrgt 48 monate ( spanne 2590 monate )  . die rt wurde insgesamt ohne schwere akute oder spte toxizitten vertragen . 
die ergebnisse implizieren einen mglichen berlebensgewinn nach der bestrahlung mit einem akzeptablen toxizittsniveau . schlsselwrter zentrales nervensystem toxizitt kinder tomotherapie intensittsmodulierte strahlentherapie atrt collectively , brain tumors are the second most common type of malignancy in the pediatric population , following leukemia [ 1 ]  . 
atypical teratoid rhabdoid tumor ( atrt ) is a highly aggressive malignancy of embryonic origin , and it comprises approximately 3 to 5% of all pediatric central nervous system ( cns ) tumors [ 1 ]  . 
atrt most often affects infants and children that are younger than 3 years of age , and these patients represent approximately 80 % of all atrt cases [ 2 , 3 ]  . 
atrt can also occur in older children , young adults , and the elderly [ 13 ] ; although , only a few cases of atrt have involved individuals older than 65 years [ 2 , 4 ]  . 
over the past few years , atrt has been increasingly recognized as an important tumor in infants and children [ 2 ]  . pathologically , atrt is diagnosed based on distinctive light microscopy ndings in combination with immunohistochemical and molecular genetic analysis . 
cytogenetics represents a powerful tool for atrt diagnosis , with most cases demonstrating monosomy 22 or deletions of chromosomal band 22q11 , in addition to hsnf5 / ini1 gene alterations [ 6 , 7 ]  . 
recently , studies of the molecular mechanisms of atrt , including the involvement of micrornas ( mirnas ) in mediating tumorigenicity , have become a major focus in the search for novel therapies for atrt [ 811 ]  . in particular , the elucidated roles of mirnas in atrt have improved our understanding of the biological characteristics of this tumor [ 811 ]  . clinically , patients with atrt typically present with headaches , vomiting , seizures , and irritability , due to increased intracranial pressure . 
furthermore , patients presenting with metastases have a reported median survival of 3 months versus 13 months for those without metastases [ 2 ]  . current therapeutic options for patients with atrt include maximal surgical debulking , radiotherapy ( rt ) , and anthracycline - based chemotherapy ( ctx )  . 
additive rt as part of an intensive multimodal therapy has also been shown to improve progression - free ( pfs ) and overall survival ( os ) [ 1 , 3 , 1220 ]  . 
these patients underwent additive radiation at our institution between 2006 and 2012 , and their medical records were analyzed to evaluate treatment response , disease control , and toxicity prole . patients and methods six courses of radiation were administered to 5 patients whose pathologic diagnosis of atrt was conrmed in immunohistochemical examinations . 
the median treatment time was 43 d ( range 3763 d ) and the median interval time between surgery and rt was 5 months ( range 211 months )  . 
the planning target volume consisted of the gross tumor volume or clinical target volume ( based on t1or t2 - weighted mri images ) plus a 11.5 - cm safety margthe radiation dose applied to the surrounding normal structures was limited . 
after completing the entire course of treatment , no disease progression was observed for 13 months . however , tumor progression did eventually occur and the patient succumbed to the disease 17 months after salvage rt . 
therefore , the os of this patient was 37 months from her initial diagnosis . case 2 a 21 - month - old girl with a large mass ( 5.5 5 4 cm3 ) in the fourth ventricle presented with hydrocephalus . 
to date , the patient has remained recurrence - free for 59 months with os of 60 months since the diagnosis . this patient suffers from mild late skin and subcutaneous tissue toxicity in the form of skin dryness and induration . concerning neurotoxicity , this patient still has a postoperative mild motoric decit and mild ataxia following treatment . 
1 t1 - weighted , contrast - enhanced postsurgical mri of the left frontal lobe recurrence ( a axial , b coronal , c sagittal ) and radiotherapy treatment plan ( d axial , e coronal , f sagittal ) for patient 1 . 
the patient received additive three - dimensional ( 3d ) conformal rt in a nearby hospital 4 months after surgery , with a total dose of 54 gy applied in 30 fractions . 
during the second rt course , the patient exhibited grade 1 dermatitis with temporary nausea a 12 - month - old boy presented with hydrocephalus and mri detected a large heterogeneously enhanced cerebral mass within the lateral ventricle ( 4 5 6 cm3 )  . 
approximately 3 weeks after surgery , the patient started a ctx regimen according to the intergroup rhabdomyosarcoma study group trial iii . this regimen was maintained for 8 months , and partial radiologic remission of the lesion was observed ( 3 2 2 cm3 )  . after an efs period of 10 months , the lesion progressed ( 4 3 3 cm2 )  . 
therefore , the os from initial diagnosis for this patient was 25 months . a 66 - year - old male presented with diplopia and a headache . mri detected a 22 16 14 cm3 pituitary lesion . 
3 t1 - weighted , contrast - enhanced presurgical mri ( a axial , b coronal , c sagittal ) and radiotherapy treatment plan ( d axial , e coronal , f sagittal ) for patient 2 . 
no clinical signs of chronic neurotoxicity have been observed after rt . results case 5 a 8 - year - old boy presented clinically with diplopia , headache , and right - sided hemiparalysis . 
during rt , the patient experienced mild skin erythema , focal alopecia , and fatigue . the patient has remained recurrence free for 90 months . the last follow - up examination , only focal alopecia could be detected . 
this patient suffers from a postoperative neurological decit in the form of hemiparesis without impairment of his daily and cognitive activities . two months after completion of rt , complete radiologic remission was achieved in patients 1 , 2 , 4 , and 5 . 
however , the rst patient later developed an out - of - eld recurrence in their left frontal lobe 19 months after resection , while patient 3 developed local progression 11 months after salvage rt . 
on the other hand , at the time of publication , patients 2 , 4 , and 5 showed no evidence of disease 59 , 46 and 90 months after resection , respectively . 
the median survival from the time of initial diagnosis was 48 months ( range 2590 months ) and the efs period was 46 months ( range 1090 months )  . long - term radiation sequelae included mild skin and subcutaneous tissue toxicity ( case 2 , 5 ) and hormone deciency ( case 4 )  . 
4 radiotherapy treatment plan for patient 3 based on t1 - weighted , contrast - enhanced mri and ct postsurgical images ( a axial , b coronal , c sagittal )  . 
5 t1 - weighted , contrast - enhanced postsurgical mri ( a axial , b coronal , c sagittal ) and radiotherapy treatment plan ( d axial , e coronal , f sagittal ) for patient 4 . 
6 radiotherapy treatment plan for patient 5 based on t1 - weighted , contrast - enhanced mri postsurgical images ( a axial , b coronal , c sagittal )  . clinical target volume and isodose lines are provided discussion to date , standard treatment guidelines for atrt have not been established . 
in the present study , 4 patients received postoperative radiochemotherapy , while advanced age precluded ctx use in the fth patient . in previous studies , focal radiation doses ranging from 3060 gy have been found to improve local control for atrt ( table 1 )  . 
moreover , a german study [ 25 ] suggests that characteristics associated with favorable results include : patient age at presentation , complete surgical resection , tumor size , and tumor location . in contrast , an infratentorial tumor site and incomplete tumor remission following ctx have a negative impact on patient survival [ 25 ]  . 
for this cohort , metastatic disease and rt were the only independent prognostic factors identied , and patients < 3 years of age derived greater benet from initial rt compared to the older children . 
 [ 13 ] demonstrated that a signicant improvement in pfs and os were achieved for patients that underwent surgery , ctx , and rt compared with those who did not receive these treatments . 
other studies have also reported that patient age is a predictive factor for patient survival [ 25 ]  . an optimal ctx regimen for atrt has not yet been determined , and data supporting the use of any particular ctx agent are lacking [ 12 ]  . 
ctx regimens have been effective in treating patients with atrt , yet are also associated with substantial toxicity . [ 26 ] of 15 patients who received multimodal ctx , the 2 - year os and pfs rates were 94 and 72% , respectively . in a study by peters et al . due to the poor overall prognosis of atrt patients , high - dose myeloablative ctx with autologous stem cell rescue has been considered [ 12 , 24 ]  . 
based on their outcomes , the authors concluded that early administration of rt prior to tandem highdose ctx ( hdct ) with autologous sct improved patient outcome , even in the patients who were very young [ 27 ]  . in a more recent study , schrey et al . 
 [ 30 ] found that systemic and it administration of mafosfamide followed by conformal radiation was well tolerated , yet it did not impact on patient outcome compared with it mafosfamide alone . 
furthermore , the 1 - year pfs rate for 12 patients with m0 atrt was 27 13% and the 5 - year pfs was 0% [ 30 ]  . stereotactic rt or gamma knife rt can be used to treat small atrt lesions and may provide a radiobiologic advantage [ 13 , 20 , 31 ]  . 
nowadays , proton therapy offers improved sparing of normal tissue with good radiation tolerability [ 33 ]  . regarding relapse pattern , 3 patients in our analysis who received additive rt following primary diagnosis ( cases 2 , 4 , and 5 ) have no progression to date with a median efs of 59 months ( range 4690 months )  . 
 [ 13 ] and per [ 34 ] reported that nearly one - third of atrt reault et al . patients develop tumor recurrence within 2 years postdiagnosis ( half relapse locally and other half develop metastasis or leptomeningeal relapse )  . 
in patients who relapse , survival is reported to be less than 1 year . ongoing studies of the biology of atrt are revealing novel diagnostic and therapeutic insights into this disease . for example , when lee et al . 
 [ 8 ] isolated cd133 + cancer stem - like cells from atrt patient specimens and compared their mirna expression proles with non - stem - like atrt cells , mirna142 - 3p was found to promote tumor - initiating and radioresistant phenotypes in atrt . 
 [ 10 ] targeted disruption of enhancer of zeste 2 ( ezh2 ) by rnai or pharmacologic inhibition of the protein and this strongly impaired cell growth , suppressed self - renewal , and induced radiation sensitivity in [ 9 ] reported atrt cells . 
similarly , venkataraman et al . that targeted inhibition of aurora kinase a enhanced the radiation sensitivity of atrt cells , while knipstein et al . [ 11 ] reported that inhibition of histone deacetylase in atrt cells in vitro resulted in a decrease in cell proliferation and a potentiation of the effect of radiation . 
regarding radiation toxicities , low incidence of sever acute ( approximately 1% ) and chronic ( approximately 10% ) adverse events might be observed in patients receiving local brain rt [ 35 ]  . 
longterm survivors may suffer from mental impairments , which are reected in poor academic achievement and impaired memory , attention , and processing speed [ 36 , 37 ]  . 
however , no moderate or severe mental impairments were observed in our patients . in summary , accumulating evidence is demonstrating that a combination of surgical resection , ctx , and rt provides longer survival rates for patients with atrt . 
while the small sample size of the present study is a consideration , the reported data are relevant to treating clinicians given the paucity of publications regarding this rare entity . conclusion postoperative local rt with 54 gy in 1.8 - gy daily fractions to the tumor bed with 1 - cm safety margins is a feasible and tolerable treatment for patients with cns atrt . 
at the end of therapy , about 70 % of patients reported a response ( partial remission or complete remission ) , 3 months later about 60 % , and 1 year after treatment 70 % . in univariate regression analysis , higher patient age and eld size greater than 6 4 cm were associated with response to treatment , while initial increase of pain under treatment was predictive for treatment failure . duration of rt series ( more than 18 days ) , gender , time of symptoms before rt , stress pain or rest pain , or prior ortheses use , injections , or surgery of the joint were not associated with treatment efcacy . 
in multivariate regression analysis , only eld size and initial pain increase were ( cid : 2 ) pd robert michael hermann hermann@strahlentherapie - westerstede.com 1 department of hand , trauma and orthopedic surgery , federal armed forces hospital westerstede , westerstede , germany 2 core facility quality management and health technology assessment in transplantation , integrated research and treatment center transplantation ( ifb - tx ) , hannover medical school , hannover , germany 3 center for radiotherapy and radiooncology bremen and westerstede , mozartstr . 
30 , 26655 westerstede , germany 4 department of radiotherapy , karl - lennert cancer center , university of schleswig holstein , campus kiel , kiel , germany 5 department of radiotherapy and special oncology , hannover medical school , hannover , germany highly correlated with treatment outcome . 
in contrast to other benign indications , a larger eld size ( > 6 4 cm ) seems to be more effective than smaller elds and should be evaluated in further prospective studies . keywords rhizarthrosis carpometacarpal joints treatment outcome pain hand relevanz der feldgre in der reizbestrahlung bei rhizarthrose relevanz der feldgre zusammenfassung wir analysierten den berichteten therapieeffekt einer protrahiert fraktionierten schmerzbestrahlung bei 84 patienten ( n = 101 gelenke , kontrolluntersuchungen nach 3 monaten bei n = 65 , nach 12 monaten bei n = 27 )  . 
lnge der therapieserie , geschlecht , dauer der symptome vor einleitung der bestrahlung , schmerzen unter belastung oder in ruhe oder vorherige orthesenversorgung , injektionen oder operationen des gelenks waren hingegen nicht mit dem therapieerfolg korreliert . 
in der multivariaten regression waren nur die feldgre und die initiale schmerzverstrkung prdiktiv fr das therapieerstrahlenther onkol ( 2016 ) 192 : 582588 table 1 patient and treatment characteristics of the investigated cohort gebnis . 
diverse effects of rt on inammatory processes were reported in in vitro studies [ 69 ] , such as lymphocyte apoptosis [ 6 ] , down - regulation of pro - inammatory and up - regulation of anti - inammatory cytokines in macrophages [ 7 , 8 ]  . 
it was furthermore reported that leukocyte adherence to the endothelium is notably reduced due to alteration of e - selectine presentation [ 8 ]  . especially on rt for painful plantar fasciitis , promising data were published in recent years . 
one prospectively randomized trial reported the efcacy of low - dose radiotherapy [ 10 ] , two others with 130 and 457 patients showed comparable efcacy of 6 fractions of 1 gy vs . 
the included patients were referred to the radiotherapy centers from their general practitioner or orthopedic clinics for treatment . inclusion and exclusion criteria included were all consecutively treated patients in the dened study period . 
exclusion criteria were age < 18 years ( n = 0 ) , infectious arthritis ( n = 1 ) , or generalized polyarthritis ( n = 3 )  . study endpoints the primary study endpoint was the patients reported subjective response to treatment , and classied according to complete symptom remission of pain and / or stiffness ( complete remission , cr ) , some remission ( partial remission , pr ) , and no remission ( no change , nc )  . 
however , at 3 months post - rt 36 joints ( 35.6 % ) were lost to follow - up and did not respond to the invitation for a follow - up visit at the treating rt center . 
the nowadays widely adopted 6 fractions of 0.5 gy fractionation ( to a total dose of 3 gy ) after the publication of two randomized trials on calcaneodynia [ 11 , 12 ] has been increasingly used in our group shortly after the end of the recruiting time for our study in april 2013 . treatments were administered as 6mvx photons with a linear accelerator ( siemens , erlangen , germany )  . 
in one center treatment policy was based on standard eld sizes , while in the other center the treating physicians measured the x and y extension of the painful joint ( + 1 cm additional margin in each direction ) to ensure an individual eld denition . all patients stood beside the treatment table and positioned their affected arm on this table . 
one stationary eld insuring a sourceskin distance of 100 cm was applied . statistical methods pre - rt data on patient demographics as well as the underlying disease and rt - specic data were prospectively collected and retrospectively complemented in a study database . 
normally distributed data is presented as mean and standard deviation and was analyzed with the independent students t - test , whereas nonparametric data is presented as median and range and was analyzed with the mannwhitney u test . 
pearsons 2 tests were applied were appropriate . possible relevant risk factors for impaired outcome of rt were identied by univariate binary logistic regression analyses applying an - level of 0.20. 
there was no statistically signicant difference in duration of rt , gender distribution , the time of symptoms before rt and whether surgery had been performed before rt ( see table 2 )  . 
all variables with an - level below 0.2 were included in multivariate , risk - adjusted modeling , hence patient age , duration of rt in days , presence of rest pain prior to rt , as well as initial increase of pain under rt and eld size greater than 6 4 cm versus smaller eld size were considered in multivariate , risk - adjusted binary regression analysis . 
2 shown is the distribution of joints treated with rt and complete or partial remission at the end of rt , at 3 months and at 12 months after therapy 5 months after the rst series . 
four joints had been treated with elds 6 4 cm ( 18 % of the small eld collective ) , 7 with larger elds ( 9 % of the large eld collective ) during the rst course . 
the world health organization anticipated that increases in life expectancy , and aging populations are expected to make osteoarthritis the fourth leading cause of disability by the year 2020 [ 18 ]  . 
there are no vectors pointing into the same direction ; therefore , all investigated variables in the multivariate binary regression analysis are independent from each other and from the endpoint onset of remission after rt . 
thus , if a patient was treated with a large eld size the chance for remission was more than ve times higher to experience a symptom remission than with smaller eld sizes . 
at 3 months post rt 36 joints ( 35.6 % ) were lost to follow - up and did not respond on the invitation to follow - up visit at the treating rt center . 
a remission was observed in 19 ( 70.3 % ) investigated joints : 7 ( 25.9 % ) with complete and 12 ( 44.4 % ) with partial remission . due to unsatisfactory treatment response 9 patients ( 11 joints ) received a second rt series ( re - rt ) , at mean second rt series strahlenther onkol ( 2016 ) 192 : 582588 fig . 
in rt of plantar fasciitis , our group demonstrated the same treatment efcacy of rt with individualized , small elds in comparison to larger standard elds covering the entire calcaneus . 
this group used 120 - kv irradiation ( stabilipan , siemens , erlangen , germany ) with a eld size of 6 8 cm and a focus skin distance of 40 cover 50 % of the patients reported subjective improvements , even in longer follow - up ( mean 4 years )  . 
therefore , a detailed comparison is not possible . the main limitation of this study is its retrospective design and the relatively high numbers of patients lost to follow - up in the long terthus , the presented results should be validated in a larger , prospective trial . 
moreover , some population bias cannot be excluded , as the eld sizes were not prospectively randomized . an important aspect in the context of rt for nonmalignant disorders is the risk of radiation - induced cancer ( ric ) , which needs to be discussed with the patient . 
nevertheless , the median patient age of 62 years in this study as well as the fact that relatively low doses are applied to a very peripheral area of the body should be kept in mind . 
 [ 26 ] showed that out of 1 , 528 cases with local steroid injections and alleged treatment errors about 40 % were falsely applied leading to serious septic and aseptic complications . the presented data show good efcacy especially in elderly patients . 
alternative ist dann die organerhaltende therapie , bestehend aus einer transurethralen tumorresektion mit dem ziel der r0 - resektion ( tur - b ) und einer sich dann anschlieenden simultanen radiochemotherapie ( rct )  . 
daher unternahmen es die autoren , in einer matched pair analyse die prognose der patienten nach alter und behandlungsjahr vergleichend auszuwerten [ 2 ]  . plus 20 gy boost und 40 mg / m2 cisplatin wchentlich , bei ber 75 - jhrigen nur 25 mg / m2 . ergebnisse von 1998 bis 2008 wurden 33 patienten organerhaltend behandelt . 
63 und 54 , 3 % ( p = 0 , 89 )  . patienten und methode alle in die analyse eingeschlossenen patienten hatten ein histologisch gesichertes invasives harnblasenkarzinom und die blichen staginguntersuchungen inklusive computertomographie ( ct ) des thorax , des abdomens und des kleinen beckens . 
die organerhaltende therapie bestand aus einer kurativ intendierten tur - b und anschlieend einer rct mit 45 gy originalpublikation gofrit on , nof r , meirovitz a et al ( 2015 ) radical cystectomy vs . 
dies ist auf jeden fall eine beachtliche leistung unserer vertreter in der leitlinienkommission , aber auch nicht ganz unerwartet , denn sowohl die esmo - leitlinie [ 1 ] als auch die nice - leitlinie von 2015 sehen die organerhaltende therapie aus tur - b 824 strahlenther onkol ( 2016 ) 192 : 823824 muskelinvasiven harnblasenkarzinom ? literatur und rct als kurativen , gleichwertigen therapieansatz zur zystektomie an und empfehlen , dass der patient umfassend ber beide therapieoptionen aufgeklrt werden sollte . es bleibt also zu hoffen , dass uns die patienten in den tumorboards tatschlich auch vorgestellt werden . 
auerdem sollten wir entsprechende ffentlichkeitsarbeit leisten , um potenzielle patienten mit harnblasenkarzinom bereits im vorfeld ber die mglichkeit des organerhalts zu informieren . welche argumente gibt es fr den organerhalt beim vergleichbare berlebenschancen nach operation und intaktes blasenorgan in bis zu 80 % der flle nach 5 jahnach tur - b + rct ren [ 3 , 4 ] 5 - jahres - berleben mit intakter blase von etwa 70 % [ 6 ] die rct im organerhaltenden konzept ist i . 
die erlanger daten [ 3 , 6 , 7 ] zeigen , dass die rate an kompletten remissionen bei der ersten kontroll - tur - b hher ist , wenn die rct mit 5 - fu und cisplatin durchgefhrt wurde . 
 [ 5 ] randomisierte 5 - fu / cis ( n = 47 ) gegen pac / cis ( n = 46 ) und beobachtete eine steigerung der kompletten remissionen von 62 % auf 72 % . 
auch der einsatz der tiefenhyperthermie kann die ansprechrate auf die rct weiter verbessern [ 7 ]  . es spricht also sehr viel dafr , das von rolf sauer in erlangen entwickelte und bewhrte onkologische konzept des organerhalts mit hilfe der rct auch auf das harnblasenkarzinom zu bertragen . 
krause fs , walter b , ott oj , hberle l et al ( 2011 ) 15 year survival rates after transurethral resection and radiochemotherapy or radiation in bladder cancer treatment . 
mak rh , hunt d , shipley wu et al ( 2014 ) long - term outcomes in patients with muscle - invasive bladder cancer after selective bladder - preserving combined - modality therapy : a pooled analysis of radiation therapy oncology group protocols 8802 , 8903 , 9506 , 9706 , 9906 , and 0233 . 
mitin t , hunt d , shipley wu et al ( 2013 ) transurethral surgery and twice - daily radiation plus paclitaxel - cisplatin or uorouracil - cisplatin with selective bladder preservation and adjuvant chemotherapy for patients with muscleinvasive bladder cancer ( rtog 0233 ) : a randomised multicentre phase 2 trial . 
wittlinger w , rdel cm , weiss c et al ( 2009 ) quadrimodal treatment of high - risk t1 and t2 bladder cancer : transurethral tumor resection followed by concurrent radiochemotherapy and regional deep hyperthermia . 
rieken1 , 2 , 3 received : 22 march 2016 / accepted : 20 may 2016 / published online : 22 june 2016 springer - verlag berlin heidelberg 2016 abstract purpose the prognosis for high - grade glioma ( hgg ) patients is poor ; thus , treatment - related side effects need to be minimized to conserve quality of life and functionality . 
advanced techniques such as proton radiation therapy ( prt ) and volumetric - modulated arc therapy ( vmat ) may potentially further reduce the frequency and severity of radiogenic impairment . materials and methods we retrospectively assessed 12 hgg patients who had undergone postoperative intensitymodulated proton therapy ( impt )  . 
these ndings were supported by preliminary clinical results conrming the safety and feasibility of prt in hgg . keywords brain tumors toxicity neurogenesis quality of life organs at risk intensittsmodulierte protonentherapie , volumenmodulierte arc - therapie und dreidimensionale konformale radiotherapie beim anaplastischen astrozytom und glioblastom ein dosimetrischer vergleich zusammenfassung zielsetzung die prognose bei high - grade - gliomen infaust . 
moderne radiotherapietechniken , wie die protonenradiotherapie ( prt ) und die volumenmodulierte arc - therapie ( vmat ) , haben das potential , die dosisbelastung von risikoorganen weiter zu reduzieren . material und methoden 12 hgg - patienten , die eine postoperative intensittsmodulierten protonentherapie ( impt ) erhalten hatten , wurden retrospketiv bewertet . 
anhand von dosisstatistiken wurden die integraldosis ( id ) , der homogenittsindex ( hi ) und der inhomogenittskoefzient ( ic ) berechnet und die therapieassoziierte toxizitt bestimmt . ergebnisse fr alle drei techniken war die zielvolumenabdeckung vergleichbar gut . 
die hugsten akuten nebenwirkungen waren fatigue ( 91 , 7 % ) , radiogene dermatitis ( 75 , 0 % ) , fokale alopezie ( 100 , 0 % ) , nausea ( 41 , 7 % ) , cephalgien ( 58 , 3 % ) und vorbergehende zerebrale deme ( 16 , 7 % )  . schlussfolgerung durch die prt konnte bei aufrechterhaltung der zielvolumenabdeckung eine signikante dosisreduktion insbesondere in kontralateralen kritischen neuronalen strukturen sowie in essentiellen arealen fr die neurokognitiven funktionen und neurogenese beobachtet werden . 
die vorlugen klinischen ergebnisse besttigen die sichere durchfhrbarkeit und praktikabilitt der prt bei hgg . schlsselwrter hirntumore toxizitt neurogenese lebensqualitt risikoorgane high - grade gliomas ( hggs ) are considered the most devastating of primary brain tumors . 
at present , delayed radiation - induced toxicity is underestimated because of the limited life expectancy and symptoms induced by disease progression , but its consideration is becoming increasingly essential . 
the current target volume concepts are not only prone to missing or underdosage of an essential proportion of the disease [ 2 ] , but are also associated with unnecessary dose exposure of non - target normal tissues [ 3 ]  . in this context , the most widely discussed and feared late effects following cranial radiation therapy would include impaired neurocognitive functions [ 4 , 5 ] , neurologic decits , neuroendocrine dysfunctions , and reduced quality of life ( qol )  . 
in particular , the intermodal treatment of young patients with hgg still has plenty of scope for vast improvement . technical advances , such as new imaging technologies , image guidance , and improved radiation modalities are now part of daily routine and have resulted in signicant advances in terms of conformity . 
intensity - modulated radiotherapy ( imrt ) has been conrmed as a valid treatment alternative for 3dcrt [ 8 ] and might potentially minimize treatment - related side effects in long - term survivors [ 9 ]  . furthermore , international availability and experience with prt is increasing [ 10 ]  . 
proton radiation therapy ( prt ) is a highly conformal therapy approach that offers a favorable low - dose distribution in the beam entrance path , a reduced integral dose ( id ) , and a steep dose gradient outside the target volume . 
this provides a further reduction in the dose to organs at risk ( oars ) , as well as escalation of the radiation dose without a need for compromise due to nearby oarsa feature that is not practicable with 3d - crt . the present study aimed to compare treatment planning for three frequently used radiation therapy modalities used with hgg . 
we combined our dosimetric comparison with the evaluation of early treatment toxicity numbers . materials and methods patient selection we retrospectively selected 12 consecutive patients who had undergone postoperative prt for histologically proven anaplastic astrocytoma , anaplastic oligodendroglioma or glioblastoma at the department of radiation oncology , university hospital heidelberg between 2012 and 2015 . all patients underwent maximum reasonable microsurgical resection . 
one experienced radiation therapist performed the replanning on the oncentra masterplan , version 4.5 ( elekta , stockholm , sweden ) planning system for photon plans using a collapsed cone algorithm and the syngo pt planning , version 13 ( siemens ) for proton plans to minimize interobserver variability . in 3d - crt , beam directions were individually selected and consisted of four to ve coplanar and non - coplanar elds , and subelds if necessary , using a eld - in - eld ( fif ) technique . 
all volumetric - modulated arc ( vmat ) plans were calculated as dual - arc vmat . ion beams were applied in two to three coplanar or noncoplanar beams using a horizontal beam or the gantry . 
the lateral full - width - at - half - maximum ( fwhm ) for the pencil beam was 10 mtreatment planning aimed for coverage of the ctv with the 95 % isodose . 
additional oars were monitored but not considered as an avoidance structure in 3d - crt , imrt , and prt . numbers in brackets represent percentages and refer to the absolute values in front tmz temozolomide , gy ( rbe ) gray equivalent , mgmt o6 - methylguanine methyltransferase , who world health organization dose analysis the gross tumor volume ( gtv ) was dened as the contrastenhancing lesion visible with t1 - weighted mr - imaging and t2 - flair hyperintense areas . 
custom - tted workows were used to analyze dose data across all patients automatically . comparative evaluation of treatment plans dose parameters and target volume coverage were evaluated for all three radiation modalities . 
progression - related symptoms were not evaluated as treatment - related side effects . represents the homogeneity of the target dose and should be as close to 0 as possible ; optimal if d5 equals d95 ( see below for denitions ) [ 22 ]  . 
dmean , dmax , and dmin represent the average , maximum , and minimum target doses , respectively . integral dose ( id ) = dmeanvi the id has been dened as the sum of mean dose multiplied by the volume ( vi ) receiving that dose , as determined from dose data [ 24 ]  . 
the id allows for evaluation of a lower dose spread than is possible with conventional measurements . ethics the study was approved by the local ethics committee , university of department of radiation oncology , university hospital heidelberg . ctv coverage was comparable in all three treatment modalities . 
no difference was observed regarding v90 % and v95 % ( percentage of ctv receiving a minimum of 90 and 95 % of the prescribed dose , respectively )  . 
a reasonable 3d - crt plan could not be generated for one patient due to proximity to the optical system and brainstem , and this plan was excluded from the analysis . 
here , sparing of the contralateral svz and contralateral hippocampus was significant for dmean ( vmat : 66.7 % and 3d - crt : 62.7 % ; vmat : 98.7 % and 3d - crt 98.9 % , respectively ) and id ( vmat : 67.0 % and 3d - crt : 66.6 % ; vmat : 92.8 % and 3d - crt 92.3 % , respectively ) using prt . 
xeropthalmia during radiation therapy was reported by 1 patient ( 8.3 % ) , and 2 patients ( 16.7 % ) experienced cerebral edema accompanied with progredient neurologic symptoms ; these patients were treated with high - dose corticosteroids . 
a significant reduction was achieved , particularly for the contralateral dmean , dmax , and id , when compared to 3d - crt and vmat . the current results complement other series that performed treatment planning comparisons in different entities . the benets of prt over other treatment modalities can be twofold . 
first , maintenance of dose coverage in difcult treatment volumes or dose escalation might be benecial in some individuals or cancer types , and can be best realized with prt . 
second , prt achieves a superior reduction in radiation exposure to non - target normal tissues and might therefore decrease the risk of treatment - associated side effects , which is why patients were selected for prt . 
fuss and colleagues performed a dosimetric comparison for optic pathway glioma and were able to reduce dmax to the contralateral on by almost 50 % , while the chiasm and pituitary gland doses were also reduced signicantly using prt [ 25 ]  . 
pituitary dysfunction and secondary hypopituitarism are well - known late effects of cranial irradiation [ 26 , 27 ] , and these become more relevant and prevalent in long - term survivors . 
sparing of the on becomes particularly relevant in hgg in proximity to the optic system ( n = 6 ) , which could be a reason the dose reduction for the on did not reach statistical signicance . 
another reason for this circumstance might be that the radiation therapist tended to spare important oars in vmat and 3d - crt planning if they were in proximity to the target volume at the expense of target volume coverage , as depicted by the higher ctv dmin using prt . in centrally localized craniopharyngioma , prt was superior to imrt when comparing radiation dose exposures to the contralateral svz and hippocampus [ 28 ]  . 
when discussing the preservation of neuronal function after radiation therapy , the dosimetric advantages of prt for the whole brain , hippocampus , temporal lobes , and sensory organs are particularly overwhelming . 
karunamuni and colleagues observed a dose - dependent thinning of the cerebral cortex of 0.0033 mm / gy , with a pronounced effect in the temporal lobes and limbic cortex [ 29 ]  . 
long - term follow - up of highand low - grade glioma patients after radiation therapy indicates a frequent occurrence of dementia [ 30 , 31 ]  . this context , the degree of radiation - related neurocognitive dysfunction is likely associated with the volume exposed to treatment and the dose to the critical organs . 
previous series have shown a signicant dose reduction when treating young patients with cerebral tumors with prt , thereby conrming the potential to reduce neurocognitive deciencies [ 32 ]  . 
the advantages become even more relevant in children , where declines in iq , processing speed , and ne motor skills have been reported after crt [ 3335 ]  . 
the hippocampus and the bilateral svz are known to harbor npcs [ 36 , 37 ] , which are assumed to contribute to neurogenesis and injury repair with their self - renewing capacities [ 38 , 39 ] , and could thereby play a major role in the initiation of neurocognitive impairment . 
the prevention of secondary malignancies is of minor importance in hgg , due to the still limited life expectancy of these patients compared to those with other types of intracranial tumors [ 41 , 42 ]  . all these series support the current ndings indicating the advantages of prt with respect to conformity and target volume coverage when comparing proton plans with photon plans . 
our dosimetric results for vmat planning also showed a trend toward dose reduction when compared to 3d - crt in contralateral oar and the infratentorial brahowever , for future multiplearc treatments , non - coplanar vmat [ 43 , 44 ] might be an excellent study objective to provide further improvements in oar sparing in hgg . in the era of improved systemic therapies and treatment options for disease relapse in hgg , the number of longterm survivors is increasing , thereby escalating the demand for optimized techniques like vmat and prt to improve qol and neurocognitive outcomes . 
however , a comprehensive provision of prt in europe and worldwide remains wishful thinking , which is why a greater effort is needed to identify appropriate patient populations for prt . 
young patients in particular , as well as highly functioning adults with favorable molecular biologic and clinical tumor constellations , represent a beneting patient group in which the maintenance of qol and neurocognitive function should take priority . 
furthermore , patients with unresectable tumors with complex - shaped target volumes might prot from prt in terms of dose escalation in the proximity of oars . in summary , the current data underscore the capability of prt in hgg , but several facts must be considered . a comparison of these results with other studies remains challenging because the tumors were located in all cerebral lobes and various fractionation schemes were chosen to account for individual anatomic demands . 
the oars and treatment plans were contoured and performed by one experienced radiation oncologist to minimize interobserver variability , which can be considered as a substantial strength of this study . 
therefore , in vmat and prt , the full potential for sparing critical oars has not yet been exhausted . this study also showed that vmat , with some limitations , represents an alternative to prt in terms of oar sparing . the authors are aware of the limited access to proton therapy facilities . 
furthermore , these results can be used to support the interdisciplinary argument for the feasibility and opportunity of using prt in specic cases . conclusion prt can serve as a valuable alternative to photon therapy for hgg , as it seems to reduce dose exposure to the surrounding non - target tissue while maintaining target coverage . 
this can potentially reduce the doseand volume778 strahlenther onkol ( 2016 ) 192 : 770779 related side effects of treatment , such as neurocognitive impairment , in long - term survivors . 
in these patients with limited life expectancies , the qol and neuronal functionality might be major endpoints and major treatment goals . acknowledgements we thank eric tonndorf - martini and thomas mielke for excellent technical assistance . 
scheithauer1 received : 21 april 2016 / accepted : 12 august 2016 / published online : 8 september 2016 springer - verlag berlin heidelberg 2016 abstract background and purpose the radiation dose received by the heart during adjuvant left - sided breast irradiation plays a crucial role in development of late toxicity . 
this study evaluated the inuence of different amplitudes of inspiration breath hold ( ibh ) during simulated left - sided breast irradiation on cardiac doses compared to free breathing ( fb )  . patients and methods ct data of 11 lung cancer patients were retrospectively used as left - sided pseudo - breast cancer cases . 
1 , 80336 munich , germany lad mean dose and the mean thoracic diameter and volume change , as well as with the absolute change in thoracic diameter were seen . 
im fokus dieser studie stand der einuss verschiedener individueller inspirationstiefen bei einer simulierten linksseitigen brustbestrahlung auf die kardiale strahlenbelastung im vergleich zur freien atmung . patienten und methoden computertomographiedaten von 11 lungenkrebspatienten wurden retrospektiv als linksseitige pseudobrustkrebsflle verwendet . 
for estimation of the clinical relevance of inspiration breath hold in comparison to free breathing , the normal tissue complication probability was calculated using the relative seriality model with parameters for late cardiac mortality according to [ 21 ] aus dosis - volumen - histogrammen konnten relevante parameter von herz , lunge und vorderer linker koronararterie ( left anterior descending artery [ lad ] ) abgeleitet werden . 
zustzlich wurde auf basis des relative seriality model die normalgewebekomplikationsrate ( ntcp ) fr kardiale sterblichkeit berechnet , die inspirationstiefe mithilfe des thoraxvolumens und - durchmessers quantiziert und anschlieend diese mit einer mglichen herzgewebsschonung korreliert . ergebnisse die mittlere herzdosisreduktion bei inspiration im vergleich zu freier atmung betrug 40 % ( 1 , 65 gy auf 0 , 99 gy ; p = 0 , 007 )  . 
die ntcp fr kardiale sterblichkeit konnte relativ um 78 % ( p = 0 , 017 ) reduziert werden . schlussfolgerung durch eine tangentiale bestrahlung der linken brust in tiefer inspiration kann bei patienten mit linksseitigem brustkrebs die herzdosis signikant reduziert werden . schlsselwrter kardiotoxizitt strahlentherapie brusterhaltende operation risikoorgane ntcp breast cancer is the most common cancer among women worldwide [ 1 ]  . 
according to guidelines , in particular after breast - conserving surgery ( bcs ) , it is obligatory to treat the breast with homogenous external radiotherapy [ 2 , 3 ]  . 
after mastectomy of a t3 or t4 tumor , after r1or r2 - resection , or in case of more than three positive lymph nodes , patients should receive rt [ 58 ]  . 
in addition to mostly mild and / or rare side effects , including erythema , oedema , inammation , brosis of the lung , and pericarditis , late cardiac effects in left - sided breast cancer patients have received increased attention [ 1012 ]  . numerous studies have clearly documented that it is important to spare the heart [ 13 ]  . 
furthermore , automatically gated image - guided breath - hold irradiation is nowadays feasible to combine optimally reduced tissue irradiation with maximal delivery precision [ 16 ]  . one possibility to estimate the risk for adverse events is provided by doseresponse curves , with the assumption of a uniform dose within a specied volume . 
the two best - known models are the lyman kutcher burman ( lkb ) [ 18 ] and the relative seriality ( rs ) [ 19 ] model . besides rt , anthracyclines or the antibody trastuzumab are important parts of adjuvant treatment . 
particularly for young women with early breast cancer who are treated with multimodal concepts including anthracyclines and / or trastuzumab , it should be a matter of concern for radiation oncologists to spare as much heart tissue as possible , in order to reduce late cardiac effects . 
the latter can impair patients up to 20 years and more after irradiation . it is still uncertain which regions of the heart are most relevant for rt - induced toxicities . 
many studies dene the entire heart [ 21 ] ; other studies just the left ventricle [ 22 , 23 ] , the pericardium [ 23 ] , or the anterior descending artery ( lad ) , which is the most important coronary artery affected by radiation exposures in tangential breast irradiation [ 2426 ]  . during recent years , some strategies have been developed to decrease heart and lung doses [ 27 ]  . 
this development includes respiratory - gated and breath - hold rt techniques , such as deep inspiration breath hold ( dibh ) [ 25 , 2831 ] , and technologies like forwardand inverse - planned intensity - modulated rt ( imrt ; including tangential imrt ) as well as helical tomotherapy [ 3236 ]  . 
in particular for dibh , it was shown that irradiation during deep inspiration leads to signicant dose reduction of heart and lung tissue [ 37 , 38 ]  . the intention of the present study was to analyze the inuence of inspiration breath hold ( ibh ) during simulated left - sided breast irradiation on cardiac doses compared to free breathing ( fb )  . 
for this purpose , data from stereotactic lung irradiation patients were taken , specically thoracic ct scans in different breathing circles , and thereby leftsided pseudo - breast cancer patients were created . materials and methods ct data of 11 lung cancer patients , 7 male and 4 female , were retrospectively used as pseudo - breast cancer cases . mean patient age was 71 years ( 3986 years )  . 
due to the currently limited availability of complete datasets and cts with good inspiration depths , male as well as female patients were included . regions of interest for the planning target volumes ( ptvs ) , the fossa jugularis was set as the upper limit for women and men . 
for the lower limit , the lowest visible breast tissue ( women ) or the mammary gland was used as an anatomical marker , plus approximately 8 cm distal ( men )  . 
cardiac delineation referred to feng and colleagues [ 39 ]  . in difcult cases , two coronary thin - layer ct scans with contrast agent were used as a model to estimate the location of the lad . 
right and left lung were regarded as separate regions of interest ( rois )  . due to different ct lengths in the analysis , only lung tissue that had been imaged in both cts was analysed . 
the ptv was copied and adapted to the second ct scan of each patient to secure comparability . nal parameters were the mean doses to the left and right lung , but with the special aspect of different length of the ct scans . 
all plans were veried by the same physicist and physician , and checked for radiation conformity and dose homogeneity . calculation specications and dvhs the calculation algorithm used was collapsed cone convolution with a calculation grid of 1 1 maccording to the dvhs , the following parameters were derived : mean and maximum dose to the heart , relative volumes of the heart receiving at least 35 gy ( v35 ) and 45 gy ( v45 ) , and relative volume of the heart receiving 50 % of the dose ( vrel50 % )  . 
further , the mean dose to the lad and lad d2 % , namely the dose to 2 % of the lad volume , was chosen as a robust estimator for maximum dose . 
these parameters were derived from two studies including patients treated between 1964 and 1976 , with a follow - up of up to 20 years . chest diameter versus dose to heart prior to ct acquisition , patients were instructed to breathe in and hold their breath , which led to different individual inspiration levels . 
consequently , just the volume increase due to centrifugal expansion was considered , while craniocaudal expansion was excluded . results in the fb plans of 3 out of 11 patients , the heart was outside the treatment eld ; in 8 out of 11 patients , the heart was inside the treatment eld . 
5 correlation between the relative ( rel . ) mean dose reduction to the left anterior descending artery ( lad ) and the absolute ( abs . ) change in thoracic diameter . 
during ibh , a heart maximum dose reduction to 25.4 gy ( range 5.946.9 gy ; ibh ) and a dose reduction to the lad to 15.6 gy ( range 3.241.6 gy ; ibh ) was achieved . 
no signicant difference in the mean heart dose reduction with dibh between volumetric - modulated arc rt and tangential imrt have been observed [ 44 ] , and current data support that all methods of dibh delivery reduce radiation dose to the heart ( summarized in [ 45 ] )  . 
the rationales and technical implementations of dibh gating for hypofractionated and normofractionated rt of intrathoracic and upper abdominal tumors in rt with different radiation qualities has just recently been extensively summarized by boda - heggemann and colleagues [ 46 ]  . 
of note is that less reduction of cardiac exposure is observed in patients after bsc [ 48 ] and that patients receiving regional nodal irradiation seem to benet most from dibh treatment [ 49 ]  . comparing mean and maximum ( d2 % ) doses to the lad , the presented data are also in line with former studies . 
furthermore , the quality of the planning ct images was limited due to the slice thickness of mostly 5 mfor more precise vessel delineation it would be recommendable for future studies to use ct scans with contrast agent . nevertheless , a considerable advantage of the study is the fig . 
to the best of the authors knowledge , this report is the rst comparing a whole range of inspiration levels to a potential heart dose reduction . to obtain a clinical assessment , the ntcps were calculated for each patient . 
nevertheless , it is important to mention that this patient had the second smallest inspiration level and the second smallest ntcp , even in fb with 1.3e6 ( cid : 2 ) vs . 
a summary of cardiotoxicity of breast cancer rt with special emphasis on the use of imrt was nicely provided by lohr and colleagues [ 52 ]  . conclusion this planning study demonstrates that for left - sided breast cancer patients the cardiac doses can be decreased signicantly with tangential irradiation and ibh . compliance with ethical guidelines conict of interest s . 
diese von unserem us - kollegen ralph weichselbaum vor fast 20 jahren erstmals formulierte hypothese ist zwar noch nicht wissenschaftlich einwandfrei durch prospektive studien besttigt , wird aber dennoch zunehmend auch im klinischen alltag akzeptiert . 
eine aktuelle analyse der national cancer data base der usa kommt zum selben ergebnis und deutet auf einen positiven effekt der strahlentherapie hin [ 6 ]  . in die retrospektive analyse wurden mnner mit neu diagnostiziertem metastasiertem prostatakarzinom eingeschlossen , die eine antihormonelle therapie ( androgendeprivation therapy , adt ) erhalten hatten und bei denen daten zur lokalen therapie ( keine oder radiotherapie bzw . operation ) und daten ber krankheit ( gleason - score , psa ) und komorbiditt vorhanden waren . 
der berlebensvorteil blieb auch signikant , wenn man nur die langzeitberlebenden betrachtete ( also diejenigen patienten mit tod in den ersten 3 oder 5 jahren nach diagnose von der analyse ausschloss )  . 
ihre berlebensrate war signikant besser als die der 163 mnner mit niedrig dosierter rt ( hr fr tod : 0 , 43 ; p < 0 , 001 multivariat )  . 
es bestand kein unterschied im berleben zwischen hoch dosierter rt und prostatektomie . schlussfolgerung patienten mit primr metastasiertem prostatakarzinom lebten in dieser retrospektiven analyse lnger , wenn sie eine kurative radiotherapie der prostata erhalten hatten . originalpublikation rusthoven cg , jones bl , flaig tw et al ( 2016 ) improved survival with prostate radiation in addition to androgen deprivation therapy for men with newly diagnosed metastatic prostate cancer . 
21 , 24105 kiel , deutschland in den letzten jahren gab es mehrere retrospektive arbeiten , die einen berlebensvorteil durch eine zustzliche lokale therapie der prostata bei patienten mit primr metastasier826 strahlenther onkol ( 2016 ) 192 : 825826 tem prostatakarzinom andeuteten . 
in deutschland wurde daher 2015 eine randomisierte studie gestartet , die den effekt der prostatektomie in diesem kollektiv untersucht ; die studie wird von der martini - klinik in hamburg geleitet und ist in der studiendatenbank clinicaltrials.gov die einzige phase - iii - studie zu dieser frage . 
allerdings gibt es auch radiotherapie - studien , die sich dann aber mit der therapie der metastasen beschftigen . die in den letzten jahren ( 2014 und 2015 ) publizierten seer - daten [ 24 , 7 ] und die jetzt publizierte analyse der national cancer data base [ 6 ] sind in den grundaussagen konsistent : patienten , die zustzlich zur antiandrogenen therapie eine kurative therapie der prostata erhalten , leben lnger . 
eine 2015 publizierte analyse , in der imrt und prostatektomie bei primr metastasierten karzinomen verglichen wurden , schnitt die imrt besonders gut ab [ 7 ]  . die homogene datenlage suggeriert , dass die hypothese benet durch lokale therapie bei m1 richtig sein knnte . 
die zu dieser frage durchgefhrte ( bisher einzige ) randomisierte studie konnte dies aber nicht besttigen [ 1 ]  . fazit die hier vorgestellten , fr die radiotherapie sehr eindrucksvollen daten reichen unseres erachtens bisher noch nicht aus , um eine allgemeine behandlungsempfehlung zu formulieren . 
badwe r , hawaldar r , nair n et al ( 2015 ) locoregional treatment versus no treatment of the primary tumour in metastatic breas tcancer : an open - label randomised controlled trial . 
rusthoven cg , jones bl , flaig tw et al ( 2016 ) improved survival with prostate radiation in addition to androgen deprivation therapy for men with newly diagnosed metastatic prostate cancer . 
neben dem gesamtberleben wurden erkrankungskomplikationen , toxizitt und therapiedurchfhrbarkeit im detail analysiert und zwischen verheirateten und unverheirateten patienten verglichen . 798 strahlenther onkol ( 2016 ) 192 : 797805 ergebnisse das gesamtberleben war bei verheirateten patienten signikant hher als bei unverheirateten . 
der familienstand knnte ein wichtiger prdiktiver faktor bei lteren glioblastompatienten sein und sollte weiter untersucht werden . schlsselwrter glioblastom ltere patienten familienstand radiotherapie temozolomid introduction glioblastoma multiforme is the most frequent primary brain tumor and continues to carry a dismal prognosis despite aggressive multimodal treatment regimens [ 1 ]  . 
the current standard of care for patients younger than 70 years with newly diagnosed glioblastoma includes maximal safe resection followed by adjuvant chemoradiation with temozolomide as was dened by the landmark stupp trial in 2005 [ 2 ]  . 
in the present work , we therefore sought to investigate the impact of marital status on survival , treatment delivery , and complications in a retrospective series of elderly patients with glioblastoma ( > 70 years )  . methods patients and procedures this study was conducted as a retrospective chart review . we identied 57 glioblastoma patients who were at least 70 years old at the time of diagnosis during the period 20042013 ( table 1 )  . 
adjuvant chemotherapy with temozolomide at 150 mg / m d15 q 28d was recommended for all patients without contraindications . for radiotherapy planning , all patients underwent computed tomography imaging with contrast medium and pretreatment magnetic resonance imaging . 
three - dimensional conformal radiation was delivered with 6 - mv photons . intensity - modulated radiation therapy was used whenever necessary for normal tissue sparing [ 22 ]  . in general , target volumes were delineated following the radiation therapy oncology group ( rtog ) guidelines [ 23 ]  . 
most patients were treated with conventional fractionation ( n = 49 , 86.0 % ) , whereas eight patients were treated with hypofractionated regimens with a single dose of 3.0 gy ( n = 4 ) and 3.5 gy ( n = 4 ) ( table 1 )  . 
parameters with univariate values of p < 0.100 were included in the multivariate model . differences in toxicity and treatment delivery between married and unmarried patients were evaluated using the student t test or chi - square test , as indicated . 
the statistics were calculated using spss ( ibm ) version 22 . impact of marital status on overall survival after a median follow - up of 26.4 months , 54 patients ( 94.7 % ) had died . 
importantly , marital status retained its prognostic signicance in multivariate cox regression analysis among established prognostic factors . our ndings of improved survival in married patients with glioblastoma are generally in line with multiple large population - based studies [ 1217 ]  . these trials in part investigated variable treatment years or geographic regions and focused on different age groups as well as on glioma subtypes but are essentially all based strahlenther onkol ( 2016 ) 192 : 797805 on analyses of the seer database . 
furthermore , unmarried patients had a higher risk of death in multivariate analysis ( hr = 1.10 ; p = 0.003 ) adjusting for age , gender , tumor location , histology , and year of diagnosis as well as race and poverty level . 
as in other studies with similar ndings , this survival difference remains unexplained [ 14 ]  . in the present work , we conducted a detailed analysis of disease complications , toxicity , and treatment feasibility that was not possible in the aforementioned populationbased studies . we did not nd signicant differences in treatment according to marital status , although married patients tended to be treated more aggressively . 
however , we did nd striking differences in treatment feasibility as well as toxicity and disease complications . concerning treatment delivery , married patients could receive much higher daily doses of temozolomide and needed to be hospitalized less frequently during rt . 
married patients had higher chances to be treated with maintenance temozolomide and tended to receive rt more completely as well as treatment for recurrence more often . interestingly , depression could be one potential mediator of worse treatment delivery in unmarried patients that could be targeted therapeutically . 
found that unmarried male patients with cancer have a higher prevalence of depression , lower levels of ghting spirit , and higher levels of helplessness [ 24 ] , which could subsequently lead to reduced treatment adherence [ 25 ]  . 
found that being unmarried or not with a partner was associated with nonadherence to oral chemotherapy in patients with cancer [ 26 ]  . aside from hematologic complications , hepatic toxicity is a well - described side effect of temozolomide treatment [ 2 , 2426 ]  . 
interestingly , higher serum glucose levels may have a detrimental effect on survival in patients with gliomas [ 27 , 28 ]  . in further detailed analyses , we evaluated potential differences in nonlaboratory disease complications and treatment toxicity between married and unmarried patients . we mostly found infectious and neurologic complications , which may represent disease - associated complications rather than treatment - related toxicity ( table 5 )  . 
of particular concern , however , is a striking increase in the high - grade complications ( including grade v ) we observed in the unmarried subgroup . reduced disease complications and treatment - associated toxicity in married patients could be well explained by better support and surveillance during chemoradiation . 
interestingly , marital status continued to have a signicant effect on self - reported health after adjusting for living arrangements including living in a stable partnership [ 33 ]  . unmarried patients with glioblastoma living in a stable partnership may benet to the same degree as married patients . 
future studies are clearly warranted to clarify the prognostic impact of stable partnership and other important social factors in patients with malignant gliomas . given the available evidence concerning marital status as a relevant prognostic factor and a potential modier of toxicity , the impact of marital status on treatment outcomes in prospective clinical trials should be addressed . 
furthermore , it would be reasonable for future clinical trials to include marital status as a potential confounder for treatment outcomes and toxicity . limitations of the current work are its retrospective nature and the limited patient number . 
however , to the best of our knowledge , this study is the rst to show that the as - yet unexplained survival advantage for married patients with glioblastoma may be mediated by improved treatment delivery , less severe toxicity , and fewer high - grade disease complications . our ndings have important implications for clinical practice and future research as they suggest that marital status is an important predictor for treatment delivery and toxicity in elderly patients with glioblastoma that could aid in clinical decision - making . 
furthermore , the inferior outcome of unmarried patients may be ameliorated by social support systems . conclusion we found the well - described but as - yet unexplained survival disadvantage of unmarried glioblastoma patients to be mediated by poorer treatment delivery as well as by an unexpected severe increase in toxicity and disease complications . 
marital status may be an important predictive factor that may aid in clinical decision - making in elderly patients with glioblastoma and warrants to be addressed in larger and prospective trials . 
fietkau state that there are no conicts of interest . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
september 2016 springer - verlag berlin heidelberg 2016 ziel prospektive nichtrandomisierte studie zur prfung , ob die exzellenten ergebnisse bei kindern und jugendlichen mit nodulrem lymphozyten - prdominanten hodgkin - lymphom ( nlphl ) niedriger stadien nach einer therapiereduktion erhalten bleiben . patienten und methoden patienten mit stadium ia eines nlphl und singulrem , komplett reseziertem lymphknotenbefall wurden ohne weitere therapie beobachtet . 
patienten ohne komplettes ansprechen auf chemotherapie wurden mit 21 gy bestrahlt ( involved eld radiotherapy , if - rt )  . ergebnisse von den 183 in die studie aufgenommenen patienten konnten 178 evaluiert werden . 
insgesamt 135 patienten erhielten av - pc ; 126 wurden bei diagnose und 9 nach rezidiv und initialer resektion und observaoriginalpublikation appel be , chen l , buxton ab et al ( 2016 ) minimal treatment of low - risk , pediatric lymphocyte - predominant hodgkin lymphoma : a report from the childrens oncology group . 
das 5 - jahres - efs der gesamten kohorte belief sich auf 85 , 5 % ( 95 % ci 79 , 290 , 1 )  . das gesamtberleben betrug 100 % . schlussfolgerung der autoren bei etwa 75 % von hochselektionierten patienten mit komplett reseziertem nlphl kann eine chemotherapie unterbleiben . 
bei den wenigen rezidiven war die weitere behandlung mit einer berlebensrate von 100 % erfolgreich . kommentar die entitt des lymphozyten - prdominanten hodgkinlymphoms ( lphl ) ist histopathologisch , immunhistochemisch und klinisch vom klassischen morbus hodgkin ( mh ) gut abgrenzbar [ 2 ]  . 
in 6 pdiatrischen serien mit insgesamt 258 patienten unterschiedlicher stadien und therapien eines lphl lag die gesamtberlebensrate bei 100 % , das ereignisfreie oder progressionsfreie berleben je nach stadium und gewhlter erstbehandlung zwischen 40 und 100 % . 
in retrospektiven analysen konnte die mglichkeit des primren verzichts auf weitere behandlungen 828 strahlenther onkol ( 2016 ) 192 : 827829 nach kompletter resektion einer lokalisierten erkrankung dargestellt werden [ 35 ]  . vor dem hintergrund einer hohen heilungsrate lag bei pdiatrischen mh - erkrankungen seit langem der schwerpunkt auf der registrierung und vermeidung von unerwnschten effekten . 
stand zu beginn die wachstumsstrung im relativ hoch dosierten strahlenfeld bei nichtausgewachsenen kindern und jugendlichen im vordergrund , so waren durch alkylanzien - induzierte sekundre leukmien , anthrazyklin - induzierte kardiovaskulre folgen , bleomycin - induzierte lungenbrosen , sekundrmalignome im strahlenfeld und schlielich procarbazin - induzierte fertilittsminderungen im fokus . 
therapieadaptionen der konsekutiven , ber die letzten jahrzehnte durchgefhrten studienprotokolle fr die behandlung von hodgkin - erkrankungen im kindesund jugendalter der deutsch - sterreichischen gesellschaft fr pdiatrische onkologie und hmatologie spiegeln die anstze zur vermeidung von gesundheitlichen sptfolgen der behandlung wider [ 68 ]  . 
der verzicht auf staging - laparotomie , splenektomie und die indikationsstellung zur radiotherapie in abhngigkeit vom mittels fdg - pet gemessenen ansprechen sind errungenschaften der modernen bildgebenden verfahren . die von der us - amerikanischen childrens oncology group ( cog ) von 2006 bis 2010 durchgefhrte prospektive nichtrandomisierte studie rekrutierte insgesamt 183 patienten im alter von < 22 jahren und einem lphl der stadien ia und iia , die in zwei arme gegliedert wurden : den observationsarm fr patienten mit einem singulren und komplett resezierten lymphknoten und in einen therapiearm fr patienten mit stadium ia und befall von mehr als einem lymphknoten , fr patienten im stadium iia und patienten des beobachtungsarms mit rckfall . 
aus den retrospektiven analysen kleinerer serien ging hervor , dass bei patienten , die nach kompletter resektion nur beobachtet wurden , ein rckfall meist lokal und als stadium ia oder iia auftrat und dann noch erfolgreich behandelt werden konnte . 
ein wiederauftreten der erkrankung ereignete sich bei lediglich 13 patienten , und zwar 12 - mal im ursprnglichen gebiet als stadium ia und 1 - mal als iia auch an der kontralateralen halsseite ( efs 77 , 1 % )  . die fr den therapiearm gewhlte chemotherapeutische behandlung , bestehend aus klassischen chop - zyklen , die hier als av - pc bezeichnet werden , war bei 124 von 135 patienten ( 92 % ) erfolgreich im sinne einer kompletten remission nach 3 zyklen ; auch hier sind die aus retrospektiven serien stammenden ergebnisse besttigt worden . 
offen bleibt die frage , ob es sich bei den nhl um rezidive der variante eines lphl mit aspekten eines t - zell - reichen histiozytenreichen grozelligen b - lymphoms handelte . 
in der revision der who - klassikation lymphoider neoplasien von 2016 wird auf eine in etwa 15 % der flle auftretende variante mit aspekten eines t - zell - reichen histiozytenreichen grozelligen b - lymphoms eingegangen [ 2 ]  . 
insgesamt blieben von der gesamten kohorte 152 von 178 patienten ohne erstes ereignis und einer 5 - jahres - efs - rate von 85 , 5 % ( 95 % ci 79 , 290 )  . 
chirurgischen , chemooder radiotherapeutischen behandlungsrisikos im vordergrund . hier wren prospektive randomisierte studien wnschenswert , sind aber sicher wegen der seltenheit der erkrankung mit etwa 15 neudiagnosen pro jahr in deutschland schwer realisierbar . 
die verwendung weiter reduzierter chemotherapiezyklen ohne anthrazykline wird in einer laufenden prospektiven europischen studie geprft . die in der pdiatrie zu erwartenden langen erlebenszeiten haben wegen eines potenziell kumulierenden risikos radiotherapiebedingter zweitmalignome zu einer reservierung der bestrahlung fr patienten mit inkomplettem ansprechen auf chemotherapie gefhrt . 
je nach lokalisation und technik wird die abwgung des chemotherapeutischen gegen das radiotherapeutische behandlungsrisiko zunchst eine herausforderung bleiben , wobei die protonentherapie besonders in der pdiatrie vorteile zeigen knnte . auch alternative medikamentse therapieformen wren wnschenswert . 
vorluge ergebnisse lassen allerdings , wie hier korrekt zitiert , den monotherapeutischen ansatz wenig attraktiv erscheinen [ 12 ]  . strahlenther onkol ( 2016 ) 192 : 827829 fazit mit der hier kommentierten prospektiven studie der childrens oncology group liegt erstmals eine sehr sorgfltige und umfassende beschreibung zur therapiereduktion bei pdiatrischen lymphozyten - prdominanten hodgkinlymphomen vor , die ein hervorragendes ergebnis zur rcknahme der behandlungsintensitt prsentiert und dazu anregt , im internationalen vergleich weitere modikationen zu untersuchen . georg mann und wolfgang holter , wien interessenkonikt g . 
appel be , chen l , buxton ab et al ( 2016 ) minimal treatment of low - risk , pediatric lymphocyte - predominant hodgkin lymphoma : a report from the childrens oncology group . 
mauz - krholz c , gorde - grosjean s , hasenclever d et al ( 2007 ) resection alone in 58 children with limited stage , lymphocyte - predominant hodgkin lymphoma - experience from the european network group on pediatric hodgkin lymphoma . 
shankar a , hall gw , gorde - grosjean s et al ( 2012 ) treatment outcome after low intensity chemotherapy [ cvp ] in children and adolescents with early stage nodularlymphocyte predominant hodgkinslymphoma an anglo - french collaborative report . 
shankar ag , kirkwood aa , depani s et al ( 2016 ) relapsed or poorly responsive nodular lymphocyte predominant hodgkin lymphoma in children and adolescents a report from the united kingdoms childrens cancer and leukaemia study group . 
boudov l , torlakovic e , delabie j et al ( 2003 ) nodular lymphocyte - predominant hodgkin lymphoma with nodules resembling t - cell / histiocyte - rich b - cell lymphoma : differential diagnosis between nodular lymphocyte predominant hodgkin lymphoma and t - cell / histiocyte - rich b - cell lymphoma . 
hartmann s , eichenauer da , pltschow a et al ( 2013 ) the prognostic impact of variant histology in nodular lymphocyte - predominant hodgkin lymphoma : a report fromthe german hodgkin study group ( ghsg )  . 
schellong g , ptter r , brmswig j et al ( 1999 ) high cure rates and reduced long - term toxicity in pediatric hodgkins disease : the german - austrian multicenter trial dal - hd - 90 . 
drffel w , rhl u , lders h et al ( 2013 ) treatment of children and adolescents with hodgkin lymphoma without radiotherapy for patients in complete remission after chemotherapy : nal results of the multinational trial gpoh - hd95 . 
mauz - krholz c , hasenclever d , drffel w et al ( 2010 ) procarbazine - free oepa - copdac chemotherapy in boys and standard oppa - copp in girls have comparable effectiveness in pediatric hodgkins lymphoma : the gpoh - hd - 2002 study . 
advani rh , horning sj , hoppe rt et al ( 2014 ) mature results of a phase ii study of rituximab therapy for nodular lymphocyte - predominant hodgkin lymphoma . 
j clin oncol 32 : 912918 strahlenther onkol ( 2016 ) 192 : 831874 doi 10.1007 / s00066 - 016 - 1051 - 3 abstra cts 2nd joint meeting sasro / sgsmp congress presidents : rachid boucenna , sgsmp ; guenther gruber , sasro campus sursee , 25.8.27.8.2016 scientific committees for medical physics for sgsmp : raphael moeckli , lausanne stefano presilla , bellinzona gtz kohler , basel peter manser , berne for sasro : giovanna dipasquale , geneva manfred sassowsky , inselspital , berne for medical radiation oncology damien weber , villigen daniel zwahlen , chur gianfranco pesce , bellinzona paul martin putora , st . 
gallen for nurses marianne scharfenberger , winterthur for sgsmp : goetz kohler , basel stefano presilla , bellinzona manfred sassowsky , berne for sasro : oscar matzinger , vevey karl beer , biel award committees best poster and best presentation awards svmtra award ulrike dechantsreiter , lucerne arthur sterchele , st . 
gallen published online : 12 october 2016 springer - verlag berlin heidelberg 2016 abstracts strahlenther onkol ( 2016 ) 192 : 831874 conclusions : in lacc , htrt demonstrates a therapeutic advantage over rt without significant acute or late morbidities . 
on nma , htctrt appears promising but needs further confirmation through prospective randomized trials . hyperthermia and radiotherapy with or without chemotherapy in locally advanced cervical cancer : a systematic review with conventional and network meta - analyses n . 
the outcomes evaluated were complete response ( cr ) , long - term loco - regional control ( lrc ) , overall survival ( os ) , acute and late grade iii / iv toxicities . 
the risk differences for achieving cr and lrc were greater by 22 % ( p < 0.001 ) and 23 % ( p < 0.001 ) respectively with htrt compared to rt . 
bayesian nma , incorporating 13 studies ( n = 1000 patients ) for cr and 12 studies for os ( n = 807 patients ) , comparing htctrt , htrt , ctrt and rt alone was also conducted . 
 a treatment planning study simulating stereotactic body radiation therapy ( sbrt ) for pancreatic tumors was performed to compare dosimetrically the internal target volume ( itv ) to the tumor tracking concept . 
white shade areas show lower dose values for tracking , white gray shaded areas show lower values for itv concept strahlenther onkol ( 2016 ) 192 : 831874 dosimetry of flah irradiation for studies on the biological effect induced in normal brain and gbm k . 
 1 institute of radiation physics ( ira ) , 2 department of radiation oncology , 3 radio - oncology laboratory , lausanne university hospital , lausanne , switzerland * equal contribution to the work no abstract calculation of the effective dose delivered by igrt in h&n and breast treatments mireille conrad1 , 2 , grgory bolard3 , marie nowak1 , berardino de bari1 , wendy jeanneret1 , jean - franois germond1 , franois bochud1 , raphal moeckli1 1institute of radiation physics , lausanne university hospital , lausanne , switzerland 2universit de genve , genve , switzerland 3clinique de genolier , genolier , switzerland aims : to create a model , implementable in a tps , able to calculate the dose distributions delivered by igrt for h&n and breast patients and use these distributions to calculate the effective dose . methods : the obi ( varian , usa ) thorax and the xvi ( elekta , uk ) h&n , thorax and 4d cone beam ct ( cbct ) acquisition modalities were studied . 
the mean dose received by each organ was calculated with the models and the effective dose was calculated using the icrp 103 recommendations ( effective dose is in quotes because it is a similar calculation than the effective dose , but for each individual patients , which is not the rigorous definition of effective dose )  . 
 the most important organs for effective dose calculations are the one close to the isocenter and the one with a high tissue weighting factor . conclusion : the model created allows to calculate dose distributions due to igrt in patients and to determine the corresponding effective dose the model is robust in terms of uncertainty . 
 impact of the radiation dose on hepatic perfusion evaluated using liver scintigraphy mebrofenin . berardino de bari1 , thomas breuneval1 , michelezeverino2 , sarah godin1 , john prior3 , jean bourhis1 , raphal moeckli2 , mahmut ozsahin1 , 1radiotherapy department , centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland 2medical physics , centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland 3service de mdecine nuclaire , centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland introduction : aim of this study is to evaluate the impact of the radiation dose on hepatic perfusion by integrating mebrofenin liver scintigraphy ( hbs ) before and after radiotherapy ( rt ) in patients treated with stereotactic body radiotherapy ( sbrt ) on liver . 
 methods : between april and september 2015 , six patients with primary ( three patients ) or secondary liver cancers ( three patients ) were treated with sbrt ( 315 gy : 4 pts , 58 gy : 1 pt or 65 gy 1 pt )  . 
for each patient , the biological equivalent dose of 2 gy per fraction ( eqd2 ) was calculated with an alpha / beta = 10 gy , to assess the acute toxicity . 
then , we calculated the activity ( mbq ) in these volumes before and after treatment . results : linear regression analysis showed a significant reduction in liver function at three months . 
this analysis shows a functional decrease , which is proportional to the delivered dose , thus predicting the resulting acute toxicity . impact of the radiation dose on the pulmonary perfusion assessed using lung scintigraphy berardino de bari1 , sarah godin1 , michele zeverino2 , thomasbreuneval1 , john prior3 , jean bourhis1 , raphal moeckli2 , mahmut ozsahin1 1radiotherapy department , centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland 2medical physics , centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland 3service de mdecine nuclaire , centre hospitalier universitaire vaudois ( chuv ) , lausanne , switzerland aim : we evaluated the impact of the radiation dose on the lung perfusion ( lp ) using lung scintigraphy ( ls ) performed before and after the treatment in patients ( pts ) treated for primary or secondary lung cancers . 
all patients received a ls to evaluate the lp before and three months after radiotherapy , which was co - registered with the planning phase of the simulation ct - scan . 
for pts treated with hypo - fractionated regimens , the biological equivalent dose at 2 gy / fraction ( eqd2 ) was calculated ( alpha / beta = 10 gy for acute toxicity )  . 
allal1. 1service de radio - oncologie , hfrhpital fribourgeois 2service doncologie , hfrhpital fribourgeois 3service de chirurgie , hfrhpital fribourgeois aims : to evaluate the acute and late toxicities and patients outcome ( progression free and overall survival ) in a single center retrospective analysis of patients ( pts ) treated with high dose rt with concomitant chemotherapy ( gemcitabine ) for non - resected or r1 resected pancreatic adenocarcinoma . 
 parients & methods : between march 2009 and august 2015 , 24 patients , with non - resected locally advanced ( 18 pts ) or r1 resected ( 6 pts ) pancreatic adenocarcinoma , have been treated with concomitant radio - chemotherapy . 
 except one patient who received 56 gy , all patients received > = 59 gy ( median dose 60.0 gy ) in standard fractionation , using mainly imrt technique ( 58 % )  . 
the acute and late toxicities were evaluated according to ctcae v3.0 criteria during and after the treatment . results : the median follow - up was 8.0 months ( range , 1 42 months )  . 
late toxicities consisted mainly of g1 digestive toxicities . conclusion : the present study confirms the feasibility of high dose rt combined with gemcitabine - based chemotherapy in patients with locally advanced pancreatic adenocarcinoma . 
aebersold1 , roland giger2 , olgun elicin1 1department of radiation oncology , inselspital , bern university hospital , bern , switzerland 2department of otorhinolaryngology - head and neck surgery , inselspital , bern university hospital , bern , switzerland 3radiation - oncology - centre , biel seeland berner jura , biel , switzerland purpose : to evaluate the long - term outcome of ct1 - 2 cn0 cm0 glottic squamous cell carcinoma ( scc ) cases managed with radiotherapy ( rt ) or surgical treatment ( st )  . patients and methods : retrospective , single institution analysis of early stage glottic scc patients , treated with either normo - fractionated rt or st between 1990 and 2013 . 
the primary endpoint was relapse - free survival ( rfs )  . results : the median age of patients ( n = 244 ) was 65 ( range : 3692 ) years , with the majority ( 92 % ) being male and 81.6 % presenting a ct1 stage . 
without any significant differences ( p > 0.1 ) among treatment groups , the 5 - year overall and disease - specific survival rates of the whole cohort were 92 % and 96 % , respectively . 
this study aims to evaluate the impact of the metastatic site on the outcome of pca pts treated with curative radiotherapy . methods : the analysis from the iosi database included 531 cases of localized pca diagnosed between 2000 and 2014 . 
six pts had visceral metastasis only ( 9.7 % ; liver , lung , brain ) and 12 ( 19.3 % ) multiple metastases with median pcass of 15.1 mo ( 95 %ci 6 - nr )  . 
if the first metastatic sites are lymph nodes , local treatments including stereotactic radiotherapy to the metastatic nodes may significantly slow the rate of progression of the disease . risk factors for peg - dependency and unplanned hospitalizations in patients with head and neck cancer who underwent gastrostomy tube installment binaya k . 
aebersold1 , kathrin zaugg1 1department of radiation oncology , head and neck surgery , inselspital , bern university hospital , bern , switzerland 2department of visceral surgery and medicine , division of gastroenterology , head and neck surgery , inselspital , bern university hospital , bern , switzerland 3department of otorhinolaryngology , head and neck surgery , inselspital , bern university hospital , bern , switzerland purpose : to identify any risk factors for percutaneous endoscopic gastrostomy ( peg ) - dependency and unplanned hospitalizations in patients with head and neck squamous cell carcinoma ( hnscc )  . methods : all uicc stage iii - ivb non - nasopharyngeal / - paranasal / - nasal hnscc patients ( n = 218 ) treated from 2007 to 2012 with postoperative or definitive radio ( chemo ) therapy in a curative intent were included . 
patients with these factors may require careful monitoring and proactive measures . keywords : head and neck cancer , percutaneous endoscopic gastrostomy , morbidity , hospitalization dose - escalated salvage radiotherapy for histologically proven macroscopic recurrence after radical prostatectomy : clinical outcomes and toxicity results mohamed shelan , seline odermatt * , beat bojaxhiu , olgun elicin , daniel m . 
aebersold , alan dal pra department of radiation oncology , inselspital , bern university hospital , bern , switzerland aims : salvage radiotherapy ( srt ) is a potentially curative treatment for local recurrences after radical prostatectomy ( rp )  . 
this work aims to retrospectively assess clinical outcomes and toxicity data of patients treated with dose - escalated srt to histologically proven macroscopic local recurrence . methods : we report on a cohort of 28 patients with histologically proven macroscopic local recurrence on mri and / or ct treated with srt between 2008 and 2015 . 
a dose of 6466 gy ( 2 gy / fr ) was delivered to the prostatic bed followed by a dose escalation to 7274 gy ( 2 gy / fr ) to the site of macroscopic disease using image - guided imrt . 
baseline , acute and late urinary and gastrointestinal ( gi ) toxicity rates were reported using ctcae v4 . results : median follow - up was 38 months ( 8 66 )  . 
this study aims to evaluate the safety and efficacy of srs in a population of patients with tn . methods : between 2011 and 2015 , 8 patients presenting with tn were treated using srs . 
the frequency and severity of pain , as well strahlenther onkol ( 2016 ) 192 : 831874 as trigeminal nerve function , according to barrow neurological institute ( bni ) scale , were evaluated before srs and regularly thereafter . 
 after immobilization with a leksell b stereotactic frame under local anesthesia , srs was planned on iplan ( brainlab ) with the help of computed tomography ( ct ) and magnetic resonance ( mr ) images for targeting and delivered with a novalis txtm linac using circular cones . 
moeckli institute of radiation physics , lausanne university hospital , lausanne , switzerland aim : stereotactic radiotherapy treatments have increased during the past years , arising the needs for specific quality assurance programs and dedicated detectors with higher resolution . in this study we analyze the feasibility of using the two - dimensional liquid filled ionization chamber array octavius 1000srs ( ptw - freiburg , germany ) for patient specific qa for cyberknife treatment plans . methods : twenty treatment plans for several anatomical sites have been considered and recalculated in the octavius phantoadditionally six static beams with different incidence angles have been measured in order to assess the response of the detector for simple irradiation . 
the doses measured by the central chamber of the 2d array 1000srs were compared with the a1sl chamber measurements and with the tps dose calculations . results : the measures performed with the a1sl are in good agreement with the tps calculations . 
weber1 , tony lomax1 1center for proton therapy , paul scherrer institut , 5232 villigen psi , switzerland 2department of radiation oncology , massachusetts general hospital and harvard medical school , boston , ma aims : to model the psi proton scanning gantry ( gantry 2 ) using a monte carlo ( mc ) tool in order to explore new delivery techniques , such as the use of apertures . 
particular attention has been concentrated on reproducing the measured angular and spatial distribution of pencil beams in air . methods : beams have been simulated using topas 2.0.p3 , which is built around the mc toolkit geant4.10.1.p02. 
mc dose calculations in water and on patient ct data have been dose and energy measurements in radio therapy by a combination of tld100 and tld100h pascal hauri1 , 2 , uwe schneider1 , 2 1faculty of science , university of zurich , zurich , switzerland 2radiotherapy hirslanden , hirslanden medical center , aarau , switzerland purpose : due to the small size and the tissue equivalent composition tlds are well suitable for out - of - field dose measurements . 
we present a method to automatically correct for energy variation of the measured photons by combining lif : mg , ti and lif : mg , cu , p chips . methods : the energy response of tld100 and tld100h compared to 60co was taken from the literature . 
with the ratio between the tld100 and tld100h dose the mean energy was deterfig.1 relative dose calculated using the tps ( a ) , topas ( b ) and dose difference topastps ( c ) mined . 
the inand out - of - field dose accuracy of the double tld method for nominal beam energy of 6mev was determined by an end - to - end measurement . 
 finally , the photon energy distribution in an alderson phantom was measured for different treatment technics applied with a linear accelerator and a cobalt machine combined with a mri . results : the presented method to determine the dose showed an accuracy of 0 + / 3 % double standard deviation of the mean compared to the ionization chamber . 
for mean energies lower than 0.6mev , the method systematically overestimated the energy by 0.1mev. conclusion : the method is suitable for accurate inand out - of - field dose measurements down to a photon energy of 150 kev . comparison of two automated treatment planning solutions for complex head and neck cancer m . 
guckenberger1 1 university hospital zurich , department of radiation and oncology , zurich , switzerland 2 philips radiation oncology systems , fitchburg , wisconsin , usa purpose : volumetric modulated arc treatment ( vmat ) optimization is a time consuming process which involves several iteration cycles before an acceptable plan is achieved . 
 material and methods : a vmat model was created with a knowledge based , auto - planning v9.10 ( ap ) ( pinnacle , philips radiation oncology systems , fitchburg , wi ) and a model based , rapidplan v13.5 ( rp ) ( eclipse , varian medical system , palo alto , ca ) , optimization systems . 
moeckli institute of radiation physics lausanne university hospital , lausanne , switzerland aims : deformable image registration ( dir ) is becoming an essential tool in radiotherapy for processes like multimodal segmentation , dose accumulation , adaptive therapy , etc . 
 methods : the tools proposed for dir qa can be split into four categories : visual ( image fusion , deformation vector maps , voxels tracking ) , localized ( target registration error , critical points , jacobian ) , contours and volumes ( dice similarity coefficient , hausdorff distance , mdt ) and test objects ( physical , virtual phantoms )  . 
we have evaluated the suitability of the different qa tools in terms of their usefulness , time consumption , accuracy and ease of realization . results : we found that 30 % of the tools allow to quantify errors of keys points but at the expense of extra time . 
finally the appropriate choice of tools also depends on the subsequent use of the deformed images . conclusion : our analysis shows that there are multiple ways of implementing dir qa in the clinics and that they should be clearly defined . 
rouzaud radiation therapy department , geneva university hospital , geneva , switzerland introduction : the multimodality image fusion , widely used in radiotherapy to precisely contour the target volumes , opened the field to deformable registration , as significant anatomical and positional modifications may occur between acquisitions . 
 in this work , a heat deformable 3d phantom , with two rigid well defined lesions , was conceived to quantify the performances of velocity and smart adapt in their ability to segment structures on deformed images . 
 material and methods : the phantoms deformable body ( body ) is made from wax ( deformable at 40 c ) and includes two rigid elements of aquaplast ( deformable at 60 c ) in its extremities . 
the initial distance between the centers of ptv1 and ptv2 was 10.6 cat first , it was scanned on its initial form ( ctinitial ) , then undergone two deformations , having one ct imaging for each deformation ( ct - 1deform , ct - 2deform )  . 
endpoints were local failure , regional / distant failure , and disease - free survival ( dfs )  . results : among pre / perimenopausal patients there were no significant differences in disease - related outcomes . 
richetti1 1radiation oncology , oncology institute of southern switzerland , bellinzona - lugano , switzerland 2eoc , medical physics unit , bellinzona , ticino , switzerland aims : stereotactic body radiotherapy ( sbrt ) is a curative treatment for patients ( pts ) with early - stage non - small cell lung cancer who are not healthy enough to undergo surgery and for pts with oligometastatic disease . 
the aim of the study was to report clinical results of sbrt in lung cancer . methods : 41 pts and 46 lesions were consecutively treated from september 2011 to december 2015 with vmat / rapidarc and exactrac ( brainlab ) technique to a biologically effective dose ( bed10 ) 90 gye . 
30 pts had histologically proven cancer ( 21 adenocarcinoma , 9 squamous cell carcinoma ) while 11 pts were irradiated without a proven histology but based on highly suspicious pet / ct scans . 
larger errors were related to larger physical deformations of the phantoclinical performances will be tested when effects like tissue / air modifications , low contrast and , large shifts are present . timing of radiotherapy and chemotherapy after breast - conserving surgery for node - positive breast cancer : long term results from ibcsg trials vi and vii per karlsson1 ; bernard f cole2 ; karen n price3 , bs ; richard d gelber4 ; alan s coates5 ; aron goldhirsch6 ; monica castiglione7 ; marco colleoni8 ; gnther gruber9 * 1department of oncology , institute of clinical sciences , sahlgrenska academy , university of gothenburg , sahlgrenska university hospital , gothenburg , sweden 2department of mathematics and statistics , university of vermont , burlington , vt , usa 3ibcsg statistical center , frontier science and technology research foundation , boston , ma 4ibcsg statistical center , department of biostatistics and computational biology , dana - farber cancer institute , frontier science and technology research foundation , harvard tf chan school of public health , boston , ma 5ibcsg and university of sydney , sydney , australia 6program for breast health ( senology ) , european institute of oncology and ibcsg , milan , italy 7ibcsg ( retired ) , bern , switzerland 8division of medical senology , european institute of oncology and ibcsg , milan , italy 9institute of radiotherapy , klinik hirslanden , zrich , switzerland purpose : the aims of the present study were to update the previous report from two randomized clinical trials , now with median follow - up of 16 years , to analyze the effect of radiotherapy timing on local failure and disease - free survival . methods and materials : from july 1986 to april 1993 the international breast cancer study group ( ibcsg ) trial vi randomly assigned 1475 pre / perimenopausal women with node - positive breast cancer to receive 3 or 6 cycles of initial chemotherapy ( ct )  . 
ibcsg trial vii randomly assigned 1212 postmenopausal women with node - positive breast cancer to receive tamoxifen for 5 years , or tamoxifen for 5 years with three early cycles of initial ct . 
for patients who received breast - conserving surgery ( bcs ) , radiotherapy ( rt ) was delayed until initial ct was completed ; 4 or 7 months after bcs for trial vi and 2 or 4 months for trial vii . 
we compared rt - timing groups among 433 patients on trial vi and 285 patients on trial vii who received bcs 840 prognostic factors in breast cancer ( bc ) associated with brain metastases ( bm ) o . 
ozsahin6 1radiation oncology , hopital neuchatelois , la chaux - de - fonds , switzerland 2medical oncology , centre hospitalier du valais romand ( chvr ) , sion , switzerland 3radiation oncology , centre hospitalier du valais romand ( chvr ) , sion , switzerland 4radiation oncology , clinica luganese moncucco , lugano , switzerland 5pathology , centre hospitalier du valais romand ( chvr ) , sion , switzerland 6radiation oncology , centre hospitalier universitaire vaudois chuv , lausanne , switzerland background : bc is the 2nd commonest cause of bm . 
this study aims to define prognostic factors of brain dissemination in patients with limited bc . methods : we retrospectively analyzed 726 pts with non - metastatic bc , treated between 2008 and 2013 . 
dfs and os were also significantly influenced by primary tumor > t1 , cl and her2 + or triple - negative bs and hormonal receptor percentage expression . conclusions : the risk of bm in early - stage bc remains low , but our study found a substantial variation in risk by bs , tumour size and hormonal receptor positivity . 
zilli radiation oncology , geneva university hospital , geneva , switzerland no abstract miss the target in old age breast cancer patients : the experience of the ticino breast unit s . 
the median age was 77 years ( range 7096 ) and pts were divided in 3 subgroups according to age : 70 to 79 years , 80 to 89 years and 90 years and older . 
we are analysing data to look for a likely correlation between age , comorbidities , patient preference and rt omission . comparison of mlc and couch tracking for sbrt prostate cancer s . 
guckenberger1 , 3 , s.tanadini - lang1 , 3 1university hospital zurich , department of radiation oncology , zrich , switzerland 2eth zrich , department of physics , zurich , switzerland 3university of zurich , faculty of science , zurich , switzerland aims : relaxation of the patient and bowel motion contribute to the uncertainty in dose delivery to prostate cancer patients . 
dosimetric measurements were performed in order to characterize and compare the performance of couch and mlc tracking . methods : for ten prostate patients , vmat sbrt treatment plans were prepared . 
to simulate a moving target , the delta4 phantom ( scandidos ) was mounted on the motion platform hexamotion ( sandidos ) and operated with five different prostate motion patterns . 
 intraindividual comparison of 11c - acetate and 18f - fluorocholine pet / ct and pet / mri studies for early recurrent prostate cancer after primary treatment giorgio lamanna1 , 2 . 
valentina garibotto3 , 4 , claire tabouret - viaud3 , olivier rager3 , sandra jorcano5 , hans - joerg vees1 , yannseimbille3 , habib zaidi3 , 4 , osman ratib3 , 4 , franz buchegger3 , 4 , raymondmiralbell1 , 4 , 5 , thomas zilli1 , 4 1radiation - oncology , university hospital of geneva , geneva , switzerland 2radiation - oncology , irccs san martino ist national cancer research institute , genoa , italy 3nuclear medicine , university hospital of geneva , geneva , switzerland 4faculty of medicine , geneva university , geneva , switzerland 5radiation oncology , teknon oncologic institute , barcelona , spain aims : to assess the intra - individual performance of 18f - fluorocholine ( fch ) and 11c - acetate ( ace ) pet studies for restaging of recurrent prostate cancer ( pca ) , to correlate pet findings with long term clinical and imaging follow - up ( fu ) and to evaluate the impact of pet results on patient management . methods : thirty - three pca patients ( pts ) relapsing after radical prostatectomy ( rp ) ( n = 9 ) ( psa 3 ng / ml ) , primary radiotherapy ( rt ) ( n = 8 ) ( psa 5 ng / ml ) , or rp + salvage rt ( n = 15 ) underwent ace and fch pet - ct ( n = 29 ) or pet - mr ( n = 4 ) studies in a randomized sequence 0 to 21 days apart . 
based on pet results , treatment approach was changed in 13 pts ( 41 % ) : 11 pts were treated with a curative intent for oligometastatic progression ( n = 8 ) or local recurrence ( n = 3 ) after rt and / or rp + salvage rt , while in 2 relapsing rp pts the rt plan was modified to include pelvic nodes or to boost a local relapse . 
 conclusions : in pts with early recurrent pca , ace and fch showed minor discrepancies , limited to nodal staging and mainly in the retroperitoneal area , with true positivity of pet findings confirmed in half of the cases during fu . 
treatment approach turned out to be influenced by ace or fch pet - ct studies in more than one third of the pts . prospective study on the clinical impact of 18f - fluorocholine ( fch ) pet / ct on treatment management in biochemical recurrent prostate cancer : hit the right target for the right patient b . 
richetti radiation oncology , oncology institute of southern switzerland , bellinzona - lugano , switzerland aims : after curative treatment for prostate cancer , biochemical recurrence occurs in 20 to 50 % of patients . 
in 40 / 59 ( 68 % ) cases , fch pet / ct was positive ( 8 had prostatic recurrence , 14 had pelvic nodal relapse , 12 had bone metastases with / without lymph nodal recurrence , 5 had both prostatic and nodal relapse and one a suspicious lung lesion )  . 
c.weber2 , 4 , 5 no abstract 1department of physics and astronomy , university of bologna , italy , 2center for proton therapy , paul scherrer institute , villigen , switzerland , 3department of radiology , cantonal hospital baden , baden , switzerland , 4radiation oncology inselspital , bern , switzerland , 5radiation oncology , university hospital of zurich , switzerland metal implants introduce substantial uncertainties in proton dose calculation . 
we investigated the potential of imar in an experimental scenario . we simulated a cervical spine chordoma ptv in an anthropomorphic head phantom , which embeds a titanium rod implanted in a cervical vertebra . 
 in addition , we measured under - dosage of approximately 0.8 gy for all the deliveries in this plane , possibly due to residual positioning errors combined with dose calculation inaccuracies at bone / air interfaces . 
considering the other two sagittal planes , the differences between calculated and measured dose distributions are comparable . based on this preliminary analysis , imar shows potential to be used as an easy and fast alternative to manual artifact delineation for proton therapy in presence of metal artifacts . no abstract das krebstelefon ist da mit wissen und frsorge a zahno , leiterin krebstelefon , krebsliga schweiz no abstract natrlich essen whrend der strahlentherapie vortrag mit kostproben e . 
fischer , autorin von kochbchern und essensratgebern , wien , sterreich mepitel film vs standard treatments for the prevention and cure of skin toxicity in postoperative treatment of breast cancer : a phase iii study giovanni presta1 , andrea puliatti1 , dario valcarenghi2 , simona cima1 , antonella richetti1 , roberto guggiari3 , mariacarla valli1 1radiation oncology unit oncology institute of southern switzerland ( iosi ) 2office of development and nursing research iosi ; 3nursing office iosi aims : verify the clinical efficacy , the patients satisfaction and the costs of a dressing ( mepitel film ) in prevent or reducing the radiation - induced skin reaction ( acute and chronic ) in breast cancer patients . methods : we defined a randomized controlled trial ( phase iii ) to compare two different type of dressing : group 1 : use of acqueous creams as defined in sasro guidelines ; group 2 : use of mepitel film from the first session of radiotherapy to at least 1 week after the end of treatment . clinical incidence of moist desquamation ( g2 ) in the two groups . primary endpoint : secondary endpoints : humanistic patient satisfaction scores collected during and after the end of treatment by visual analogue score ( vas ) for pain and final questionnaire . economic average total cost of the two treatments ( in swiss francs )  . according to the study of herst et al . 
 ( 2014 ) , we expect a proportion of moist desquamation in nearly 20 % of patients in the control group vs nearly 5 % in the treatment group ( mepitel film )  . 
 conclusions : this project , shared by nurses and doctors , is an example of evidence - based practice and use of research for improving the quality of life for patients . 
currently , no conclusion can be drawn because the trial is still ongoing . prone breast automatic segmentation of organs at risk including heart and coronary vessels : similarity indexes , contouring times and dose volume parameters xinzhuo wang12 , giovanna dipasquale1 , vanessachatelain - fontanella1 , odile fargier - bochaton1 , raymondmiralbell1 1department of radiation oncology , geneva university hospital , geneva , switzerland 2department of radiation oncology , tianjin union medical center , tianjin , china objective : to investigate the effects of different parameters on atlas sampling for automatic - segmentation ( as ) in prone breast cancer planning . methods : two sets of contours of organs at risk ( oar ) and ctv were generated using as on 27 patients ( pts ) with selected atlas cases to match test pts sampled either stratifying by breast volume ( as1 ) or by breast cup size and body mass index ( bmi ) , ( as2 )  . 
for the left anterior descending artery ( lada ) , lada + 1 cm margin , the right coronary artery ( rca ) and , rca + 1 cm margin , even as2 structures presented a low dice . 
when comparing the dose distribution of as structures versus manual , as2 decreased the mean dose difference for d10 and dmean of heart ( p < 0.05 ) as compared to as1 and was also able to reduce the standard deviation of lada , lada + 1 cm and , rca . 
with the exception of heart for mean doses , structures editing was necessary to obtain dose distributions similar to ms for most oar . conclusions : breast cup - size and bmi are more reliable parameters than breast volume to sample the atlas for as . 
the as2 heart may be used unedited to estimate mean doses , while wire - form structures , lada and rca , need a larger atlas population to improve dice values . estimation of late effects for mert and photon plans in radiotherapy of the breast and chest wall a . 
fix division of medical radiation physics and department of radiation oncology , inselspital , bern university hospital and university of bern , switzerland no abstract fig.1 tumor control rate as a function of blood flow entropy , curves are different at the significance level of 0.1 strahlenther onkol ( 2016 ) 192 : 831874 pet / ct - guided sib - imrt combined with concurrent 5 - fu / mmc for the treatment of anal cancer : a single institution experience j . 
oehler department of radiation oncology , kantonsspital graubnden , chur , switzerland aims : to evaluate local control , survival and toxicity in anal cancer patients treated with pet / ct - guided intensity - modulated radiation therapy ( imrt ) and concurrent chemotherapy at a single institution . methods : from august 2010 to may 2015 , 26 consecutive patients with localized squamous cell carcinoma of the anal canal ( sccac ) were treated with imrt and concurrent 5fluorouracil / mitomycin - c ( 5 - fu / mmc ) , and retrospectively evaluated . 
endpoints were local control ( lc ) , overall survival ( os ) , disease free survival ( dfs ) , colostomy free survival ( cfs ) and toxicity . results : median age was 61 years , 85 % were female , and 50 % had advanced ( stage iii ) disease . 
pet / ct was the most accurate imaging modality for nodal staging , having an impact on nodal boost volume delineation and / or rt dose definition in 9 / 23 patients ( 39 % )  . 
 conclusion : pet / ct leads to significant changes in both target volume delineation and final treatment dose in 39 % of cases , and should be included as standard staging and planning procedure for any sccac patient . 
sib - imrt with 5 - fu / mmc is feasible and results in excellent lc and survival outcomes , if all efforts are being made to minimize rt interruptions . 
it was compared with a tumor volume - based model . results : ten parameters were found to be stable in both hnc and lung cancer after the correction for inter - parameter correlation . 
in the multivariate backward selection of the variables , blood flow entropy showed a significant impact on tumor control ( p = 0.03 ) with concordance index ( ci ) of 0.76. 
this model was found to be superior to a volume - based model . 1department of radiation oncology , university hospital zurich , university of zurich , switzerland 2department of nuclear medicine , university hospital zurich , university of zurich , switzerland 3department of diagnostic and interventional radiology , university hospital zurich , university of zurich , switzerland 4department of nuclear medicine , university hospital bonn , germany aim : this study aimed to test the tumor control predictive value of radiomics features computed on pretreatment ct perfusion maps after a preselection of features in a robustness study regarding perfusion calculation factors . methods : 11 patients with head and neck cancer ( hnc ) and 11 patients with lung cancer were included in the robustness study to preselect stable radiomics features . 
 results : the most suitable roi was found to be the irradiated breast itself , excluding the shoulder and clavicular region , but including a 2 cm margin of chest wall surrounding the breast . 
in the future we plan to use the osms system for deep inspiration breath hold techniques and the set - up of extremities . stability in positioning for lung radiosurgery ( sbrt ) patients s . 
rabe radio - onkologie - zentrum ksa - ksb , kantonsspital aarau , switzerland aim : a large number of departments position their lung sbrt patients using some kind of fixation . 
to be certain that using a frameless positioning in combination with a free - breathing ( fb ) technique is stable enough to treat lung sbrt patients an intrafraction stability study has been done . method : 10 patients were positioned on a wingboard ( unger ) , in combination with a thin mattress and head cushion . 
 an itv match was used to define the shifts and the table was then fig.1 number of fractions against the deviation in cm , in vertical ( a ) , longitudinal ( b ) and lateral ( c ) direction strahlenther onkol ( 2016 ) 192 : 831874 shifted in the right position for treatment . 
 the range of motion is the biggest in vertical direction with a standard deviation of 1.4 mm , this is the direction of the breathing motion , this could explain the bigger deviation in this direction and it cant be overcome with a fb technique . 
another explanation could be that the patients get more relaxed during the treatment because we can see that almost all of them move in the dorsal direction . validation of patient preparation and setup verification in sbrt for liver tumors case report d . 
richetti2 1ente ospedaliero cantonale , medical physics unit , bellinzona , switzerland 2oncology institute of southern switzerland , radiation oncology unit , bellinzona - lugano , switzerland aims : to report our initial experience on patient preparation and setup verification for sbrt liver - confined disease . methods : we present our patient preparation and set - up verification procedure performed for hepatocellular carcinoma treatment . 
for the patient immobilization we used a vacuum pillow and an abdominal compression belt , aimed at decreasing the respiratory motion related to diaphragct images were acquired with tailored 4d - ct protocol and with intravenous contrast medium enhancement . 
during a dry run before the treatment planning , the patient positioning was verified using co - registration between radiographic oblique kv imaging and digitally reconstructed radiography from the planning ct to determine the actual position of the liver volume : we performed a marker - based verification using previous chemoembolization implants as fiducial surrogates . 
after making a radiographic - based shift an additional kv cone beam ct was done , to confirm the proper position of the organs at risk with respect to the liver on the basis of soft tissue localization . 
imaging analysis showed proper choice of planning target volume margin to account for the residual motion . conclusions : the adopted protocol is appropriate and can be implemented in clinical practice for the majority of such patients . 
literature analysis of liver sbrt protocols showed that ours approach has the potential for ensuring the effective and patient - friendly delivery . multi radiotherapy modalities treatment for multi targets in malignant pheochromocytoma setting case report j . 
bourhis1 1department of radiation oncology , chuv and university of lausanne , lausanne , switzerland 2institute of radiation physics , chuv and university of lausanne , lausanne , switzerland purpose / objective : this case report regards a 46 - year - old male patient , known for malignant pheochromocytoma of the left adrenal gland , initially treated by nephrectomy in 2011 . 
for thoracic and abdominal lesions , the ptvs were defined based on an itv ( internal target volume ) strategy , where we performed an expirium , inspirium and free breathing ct scan . 
because the itv volume was too large for the thoracic lesions , we decided to perform a ct scan with the abc system ( active breathing coordinator , elekta )  . 
 one lung lesion was located in left inferior lobe near the stomach and esophagus which had both received radiation in 2014 and we decided to treat it by cyberknife ( accuray ) with fiducial tracking . 
tomotherapy plans were created using tomotherapy treatment planning system ( volo , accuray ) , to treat the lesions located at left chest wall , right gluteus ( 57 gy ) , vertebra ( 55 / 7 gy ) , psoas and para - aortic nodes ( 56 gy )  . 
to estimate the composite dose and analyze the oar ( organ at risk ) tolerance doses , we used velocity ai software . results : the oar tolerance doses were checked using an in - house dose tolerance protocol , inputted into velocity ai software . 
 key - words : re - irradiation , composite plan , precision , pheochromocytoma hypofractionated stereotactic radiotherapy feedback for the treatment of liver tumors using backup gating and auto beam hold a . 
the threshold of tolerance depends on the amplitude of the breathing curve . results : this results in 50 % decrease in average duration positioning and treatment between the 1st , 2nd and 3rd session ( 58 , 28 and 27min respectively )  . 
sometimes the algorithm of the abh does not detect visicoils although they appear to be in the correct position . conclusion : we reached our objective , which was to treat a moving target in optimal conditions . 
we still need to work on the technique we use to record the breathing curve so that it is as accurate as possible . implementation of a complete time - effective dosimetric verification system for the commissioning and routine verification of multiple metastases element ( brainlab ) s . 
bodis radioonkologiezentrum , ksa - ksb , kantonsspital aarau , aarau , switzerland aim : the multiple metastases element by brainlab ( mme ) is a stereotactic planning system that uses multiple inversely optimised single isocenter dynamic conformal arcs ( sidca ) , to treat up to 10 brain metastases . 
the traditional verification system of film dosimetry and small volume detectors ( ionization chamber , diamond detectors , etc ) , is not only cumbersome and very time consuming , but also becomes technically impractical when the number of lesions to be verified increases ( > 3 )  . 
the physics verification and machine qa time has dropped by a factor greater than 2 , from around 180225 min with ebtfilm / diamond chamber system to some 80115 min with pd_mob , for a single lesion , with a rapidly increasing favourable trend towards the pd_mob system when the number of lesions increase . conclusion : an alternative to the traditional ebt_dc verification system that allows complete verification of a multiple stereotactic brain metastasis plan with up to 10 lesions has been successfully implemented with a significant reduction in the physics and machine time . benchmarking an automated planning tool for multiple brain metastases against an established multiple isocentre dynamic conformal arc technique n . 
bodis radio - onkologie - zentrum ksa - ksb , kantonsspital aarau , switzerland aim : a new commercial planning tool ( multiple metastases elements , mme , brainlab ) dedicated to automatically producing plans for multiple brain metastases , using a single isocentre and multiple inversely optimised dynamic conformal arcs , is compared with the multiple isocentre dynamic conformal arc ( midca ) technique used until now ( iplan , brainlab )  . method : 8 patients treated with a number of lesions varying from 2 9 were planned using both the midca method and the new single isocentre mme tool . 
the total monitor units delivered is significantly lower for mme plans ( 2.5 to 4 times lower )  . conclusion : both planning tools achieved conformal plans with steep dose fall - off , however the mme plans were more efficient both in terms of the time taken to plan and also the time needed to deliver the treatment . 
when combined with an efficient plan verification method , this tool should make radiosurgery of multiple metastases a viable treatment approach . high dose - per - pulse electron beam dosimetry a saturation model for the advanced markus ionization chamber kristoffer petersson1 , maud jaccard1 , jean - franois germond1 , thierry buchillier1 , franois bochud1 , jean bourhis2 , 3 , marie - catherine vozenin2 , 3 , and claude bailat1 1institute of radiation physics ( ira ) , do / chuv , lausanne university hospital , lausanne , switzerland 2department of radiation oncology , do / chuv , lausanne university hospital , lausanne , switzerland 3radio - oncology laboratory , do / chuv , lausanne university hospital , lausanne , switzerland strahlenther onkol ( 2016 ) 192 : 831874 fig . 
1 the ion collection efficiency ( 1 / ks ) as a function of the the dose - per - pulse according two measurement methods ( 1 open , 2filled symbols ) , and the logistic function ( lines ) fitted to the data points , for a polarizing voltage ( u ) of 50 ( crosses ) , 150 ( circles ) , and 300 v ( squares ) aims : similar to other ionization chambers , the advanced markus saturates during measurements in high dose - per - pulse ( dp ) beams . 
an empirical model of the saturation was found by fitting a logistic function to the data ( figure )  . conclusions : the advanced markus ionization chamber saturates but remains functional for dose measurements in beams with high dp values , if the saturation is taken into account . 
the model depends on the dp and the polarizing chamber voltage . in ebt3 dosimetry as well as the energy and dose - rate dependence of their response . uncertainty sources in ebt3 dosimetry were analyzed using irradiations at a clinical radiotherapy linac . 
this was bed at the prototype , for first performed by studying the correlation between doses measured by films and the charge of electrons measured at the exit of the machine by an induction torus . 
films were also compared to independently calibrated thermo - luminescent dosimeters ( tld ) that have been reported as being independent . we showed that uncertainty below 4 % ( k = 2 ) can be achieved for doses between 3 and 17 gy . 
excellent consistency between films and tld was obtained over the entire range attainable at the prototype linac confirming the absence of any dose - rate dependence within the investigated range . 
the measurements are associated with an uncertainty below 4 % and are dose - rate and energy independent . electron dosimetry with gafchromic ebt3 films : energy and dose - rate dependence m . 
bailat1 1institute of radiation physics ( ira ) do / chuv lausanne university hospital , lausanne , switzerland 2department of radiation oncology do / chuv lausanne university hospital , lausanne , switzerland 3radio - oncology laboratory , do / chuv lausanne university hospital , lausanne , switzerland the aim of this study was to assess the suitability of gafchromic ebt3 films for absolute dosimetry in the beam of a prototype high doseper - pulse linac able to deliver electron beams with dose - rate ( ) up to 8106 gy / s . 
manser1 1division of medical radiation physics and department of radiation oncology , inselspital , bern university hospital , and university of bern , switzerland 2institute for biomedical engineering , eth zrich and psi , villigen , switzerland aims : for the collimation of electron beams , the photon multileaf collimator ( pmlc ) is an alternative to patient specific molded cut - outs to optimize clinical workflow . 
dose distributions of single electron field plans were compared for six clinical breast cases using the varian emc 13.6 and an in - house monte carlo algorithm for dose calculation of cut - out and pmlc collimated electron beams , respectively . results : dose differences and distances to agreement in the relative depth dose curves are within 3 % / 3 mm for all beam setups . 
for all the investigated clinical cases , a comparable dose homogeneity and a slightly worse dose conformity is achieved with pmlc collimation and an ssd of 70 cm compared to cut - out collimation . conclusion : the results suggest that pmlc collimation of electron beams with an ssd of 70 cm is appropriate for standard electron treatments . 
moreover , we aim to investigate met addiction further , as oncogene addiction constitutes the rationale behind newly developed anticancer therapies and little is known of the molecular mechanisms responsible for this phenomenon . methods : we performed a targeted proteomics approach based on selected reaction monitoring ( srm ) in order to monitor phosphorylation changes of 120 candidate proteins in nine met - positive cellular models upon met inhibition ( meti ) , alone or in combination with ionizing radiation ( ir )  . 
remarkably , not only crucial regulators of ddr - related processes , but also key nodes of a plethora of other cellular processes seem to be regulated in met - addicted cellular models upon meti . 
not met - addicted cellular models , are descriptive for their phenotypic response to meti , alone or in combination with ir , and have the potential to shed light on the molecular mechanisms of the phenomenon of oncogene addiction . 
aebersold1 , 2 , yitzhak zimmer1 , 2 1department of radiation oncology , inselspital , university of bern , bern , switzerland 2department of clinical research , radiation oncology , university of bern , bern , switzerland aims : poor oxygenation is a common biologic feature involved in aggressive manifestations of solid tumors . 
as both met and hypoxia are determinants that affect cellular responses to dna damaging agents , we aimed to elucidate the effect of met inhibition on met - overexpressing tumor cell lines under hypoxic conditions . methods : met - overexpressing cancer cell lines were exposed to a hypoxic environment ( 1.5 % o2 ) and met was inhibited by a highly specific pharmacological inhibitor . 
a 3d ex vivo model consisting of organotypic xenograft tissues was used to confirm the in vitro observations . results : met inhibition reduces the protein levels of the key hypoxic regulator hif - 1 and its targets . 
this phenomenon can be observed not only in 2d cell line cultures , but also in a 3d ex vivo model . conclusion : we have identified a link between met and hif - 1 signaling which is likely to be important in tumor progression . 
rna and protein expression was measured by quantitative pcr and western blotting , respectively . results : cpt1c expression was upregulated in a time dependent manner under severe hypoxia ( 0.2 % oxygen ) , a condition in which both pathways , hif1 alpha and p53 , were activated . 
e. , either mild hypoxic condition ( 1.5 % oxygen ) or treatment using hypoxia - mimicking reagents . conclusion : our results suggest both hif1 alpha and p53 are required for the proper activation of cpt1c under hypoxia . 
 results : to optimize the 3d cell culture model for our purpose we tested 3 different systems : nunclon sphera surface coating - low attachment flasks , agarose - coated microtiter plates and the freiburg matrix . 
 hct116 cells did grow as spheroids in all methods but only using agarose - coated plates we are able to generate spheroids with a stable morphology and of equal size . 
zwahlen1 1department of radiation oncology , kantonsspital graubnden , chur , switzerland 2clinresearch ltd , aesch , switzerland 3novelpharm ag , schlieren , switzerland purpose : to evaluate the effectiveness of noviphenone for the prevention of acute dermatitis ( ad ) during adjuvant radiotherapy ( rt ) for breast cancer ( bc )  . methods : between november 2014 and january 2015 , 20 patients who had been operated on for bc and receiving adjuvant rt were enrolled in this open - label , prospective mono - centric study . 
patients were allocated to application of noviphenone gel 2.5 % 7 days prior to rt , 1 hour before each rt session and noviphenone 0.4 % lotion on the irradiated fields after each session twice daily as well as 4 8 weeks thereafter or longer if needed . 
but tumor motion can be mitigated with other motion management techniques , namely with mid - ventilation ( midv ) , gating or tracking concepts , raising the question : what to use when ? methods : a planning study with 20 lung cancer patients ( tumor motion : 5 28 mm ) was performed . 
tumor volumes were contoured on the 4dct phases and target volumes ( tv ) were delineated : for the itv concept , the tumor volumes of all respiratory phases were combined , for gating 3 / 10 phases at end of inhale , for tracking and midv 1 / 10 at the mid - position . 
correlations of dose benefit with tumor motion were found for gating and tracking , while the midv concept showed correlation to tumor volume . conclusion : regarding 4d dose calculations , gating gives the most reliable tumor coverage , while tracking shows the highest benefit in lung dose , which is more pronounced for higher motion amplitudes , and allows for shorter treatment times than gating . 852 strahlenther onkol ( 2016 ) 192 : 831874 fig1 left : 3d and 4d dose parameters of target volumes for the different techniques . 
guckenberger1 1university hospital zrich , department of radiotherapy , switzerland , 2university hospital freiburg , department of radiotherapy , germany aims : stereotactic radiotherapy ( srt ) is increasingly used in the metastatic tumor situation . 
 methods : a survey was handed out at the german degro stereotactic meeting in december 2015 and was sent to all swiss clinics performing srt at the beginning of 2016 . 
the survey obtained information about the experience of performing srt in the metastatic situation , how targeted therapies were combined with srt , if there were any contraindications to a combinational therapy and if the srt or targeted therapy dose was reduced . 
the targeted therapy asked for were new immunotherapies and tyrosine - kinase inhibitors . results : 27 clinics took part in the survey , of which the majority ( n = 16 ) were university hospitals . 
vemurafenib ( 33 % ) , bevacizumab ( 26 % ) , erlotinib ( 11 % ) , sorafenib ( 7 % ) and ipilimumab ( 4 % ) were considered a contraindication for combinational therapy . 
hejira clinique de genolier , genolier , switzerland purpose : to quantify the effect of mr - only treatment planning on dose distributions for prostate cancer for the clinical validation of mr - only workflow . methods : for pre - clinical validation of the mr workflow , where five - value stratified synthetic ct ( magnetic resonance for calculating attenuation ( mrcat ) algorithm , philips ingenia 3.0t ) , are used for dose calculation instead of ct , we ( 1 ) converted conventional 12bit ct scans to five - value stratified ct and ( 2 ) applied the measured geometric distortions ( deformation vector field measured with a dedicated phantom ) from the mr scanner to the ct scans of 10 patients to quantify the effect on dose to target and organs - at - risk ( oar ) for imat prostate plans . 
for the clinical validation , we calculated the gamma index of the 3d dose distribution for mr - only and conventional ct dose calculations for the same patient . results : five - value perturbed ct and conventional ct dose distributions were equivalent . 
dvh - parameters were generally higher for five - density ct / ct dose calculations ; ptv mean dose was 100.5 % compared to 100 % for ct - based plans . 
 mr - only compared to ct 3d dose distribution 3d gamma analysis ( 1 mm / 2 % ) pass rates were > 95 % , except for one patient ( 92 % ) in the 50 % and 90 % isodose volumes . conclusion : synthetic ct dose distributions are equivalent to ct for oars and slightly overestimate the dose to the target . 
3d gamma analysis ( 1 mm / 2 % ) pass rates for mr - only dose distributions compared to ct are > 95 % for comparable organ filling at both scans . strahlenther onkol ( 2016 ) 192 : 831874 11.5 radiotherapy infrastructure and human resources in switzerland present status and its projected computations for 2020 n . 
bodis1 , 3 1radioonkologiezentrum , ksa - ksb , kantonsspital aarau , aarau , switzerland 2department of radiotherapy , kantonsspital graubnden , chur , switzerland 3department of radiation oncology , university hospital zurich , zurich , switzerland aims : the study evaluates the present status of radiotherapy ( rt ) infrastructure and human resources in switzerland . 
projections for 2020 were computed taking into consideration the changes in the future rt practices , with a gradual emphasis on the practices of state - of - the - art rt techniques . methods : the guidelines of estro - quarts and iaea were adapted to estimate the requirements for teleradiotherapy ( trt ) units , radiation oncologists ( ro ) , medical physicists ( mp ) and radiotherapy technologists ( rtt )  . 
the databases used for computation of the present gap and additional requirements are ( a ) globocan for the cancer incidence and its types ( b ) directory of radiotherapy centres ( dirac ) , iaea for existing trt units ( c ) human resources from the recent estro - hero survey and ( d ) radiotherapy utilization ( rtu ) rates for each cancer sites , published by ingham institute for applied medical research ( iiamr )  . 
with a gradual transition from 2d and 3d conformal rt techniques to imrt , igrt and srs / srt , an increased time factor of person - hr / patient for ro ( 3 times ) , mp ( 2 2.5 times ) and rtt ( 1.5 2 times ) were considered for contouring , plan evaluation , treatment execution , supervision and monitoring . 
this could be tailor - made and individualized for any rt centre . conclusions : by 2020 , the increase in cancer incidence would reflect in a 9.8 % increase in patients requiring rt . 
dal pra2 1division of medical radiation physics and department of radiation oncology , inselspital , bern university hospital , and university of bern , switzerland 2department of radiation oncology , inselspital , bern university hospital , and university of bern , switzerland no abstract fatal hemorrhage due to an aortoesophageal fistula after neoadjuvant chemoradiation in locally advanced esophageal cancer a case report b . 
meier1 1department of radiation oncology , kantonsspital winterthur , winterthur , switzerland aim : chemoradiation ( crt ) is an established treatment for locally advanced esophageal cancer ( ec ) [ 1 ]  . 
however , locally advanced disease with malignant esophageal stricture or tumors invading neighboring structures ( t4 ) are associated with poor outcome and the risk of development of esophageal fistula during treatment [ 2 ]  . 
we present a case of fatal bleeding due to a newly developed aortoesophageal fistula after neoadjuvant crt in ec . methods : a 54 - year - old female patient with newly diagnosed squamous cell carcinoma of the middle esophagus ct3 cn3 m1 ( solitary renal metastasis ) g2 was referred to our clinic for neoadjuvant crt . 
the patient underwent neoadjuvant crt according to the cross protocol [ 3 ] : rt : 41.4 gy in 23 fractions , concomitant chemotherapy : paclitaxel and carboplatin weekly . results : neoadjuvant crt was completed according to the planned protocol . 
autopsy revealed an aortoesophageal fistula within the necrotic tumor as cause for the fatal hemorrhage . conclusion : invasion of thoracic structures such as the aorta , trachea and bronchi is commonly observed in locally advanced ec [ 4 ]  . 
while treatment - related arterioesophageal fistula are found in 1518 % of t4 tumors , aortoesophageal fistula are rare ( 8 % ) , but often result in fatal bleeding [ 2 , 6 ]  . 
the report by kodama in the early 1990s of a signicant dose - related increase in deaths from heart diseases among japanese a - bomb survivors observed in the life span study , which was compatible with a linear non - threshold doserisk relationship [ 3 ] , stimulated a large number of epidemiological and clinical research activities , e . 
only few studies attempted to determine ( cid : 2 ) klaus rdiger trott klaustrott@yahoo.it 1 ucl cancer institute , university college london , london , uk partial heart doses in relation to specic radiation - induced heart diseases [ 1619 ]  . the results of these studies were often considered by workshops , committees and institutions with a special interest in the potential implications they would have for the current system of radiation protection . 
they concluded that there was convincing evidence for a signicant risk of cardiovascular mortality after moderate and low radiation doses , and that policy and regulatory implication should be further discussed and research in this eld stimulated . 
the anatomical site of the manifestation of the pathology is different for each of these heart diseases , and thus the location of the target within the organ is also likely to be different . 
worldwide , the european atomic energy community ( euratom ) has been at the forefront of developing and supporting research on the biological mechanisms underlying the development of pathological changes in the heart after low and intermediate radiation exposure . 
it goes without saying that any new research project into the biology , the mechanisms and the biological modelling of radiation - induced heart diseases and dose specication for epidemiological studies has to be based on the results of these eufunded projects . 
whereas cancer incidence or mortality rates increase with increasing dose , for cardiovascular diseases it is the severity of the disease and the rate of severity progression which depends on dose [ 23 ]  . this problem is not easy to overcome but is usually washed away by using severity scoring systems which have been developed for completely different purposes and are more or less useless for research of the role of radiation in the development and progression of highly specic and multifactorial diseases such as radiation - induced heart disease . 
the aim would be to study the localization of pathological and pathophysiological changes in relation to the anatomical dose distribution and the progression of these changes over the years ( follow - up at least 10 years )  . 
in vitro studies on established endothelial cell lines or primary cells which are irradiated and followed in vitro are of limited value for investigation of the pathogenic pathways leading to microvascular insufciency and radiation - induced heart diseases . 
the experimental design developed by the cardiorisk project overcomes many of the problems by giving high - precision local radiation exposure to the heart and keeping the animals until their natural end of life up to 12 months later . this way , cardiac pathology develops under physiological conditions , and additional stress factors or protective modulation can be added to study their effect in vivo . 
therefore , methods have been developed in the cardiorisk project to study changesfrom organ physiology to tissue pathology and molecular biology of different cell typesdeveloping in a physiological tissue environment many months after exposure . 
in order to develop a sound understanding of the dose dependence of radiation - induced cardiovascular diseases , prospective epidemiological studies with precise dosimetry concentrating on local dose distribution are required . 
the most signicant animal studies performed in recent years on the problem of the pathophysiology of radiation - induced heart disease are those conducted in groningen on the functional interaction between radiation injury in the heart and the radiation injury of the lung [ 27 ]  . 
they demonstrate that radiation - induced pneustrahlenther onkol ( 2016 ) 192 : 747749 monitis or lung brosis may cause a potentially lethal increase in pulmonary hypertension , which may cause severe stress on the right heart function causing potentially lethal right heart backward failure . 
any study on potentially useful predictive markers should be aware of the fact that most of the currently used heart irradiation techniques expose a larger volume of lung than heart . 
however , this heart / lung interaction is not only a major complicating factor of radiobiological experiments on the heart , it can also be used to investigate the complex pathophysiological development of radiationinduced heart diseases by modulating the interaction of partial organ exposure of heart and lung , e . 
rieken1 , 2 received : 4 march 2016 / accepted : 8 june 2016 / published online : 4 july 2016 springer - verlag berlin heidelberg 2016 abstract background radiosurgical treatment of brain metastases is well established in daily clinical routine . 
utilization of attening - lter - free beams ( fff ) may allow for more rapid delivery of treatment doses and improve clinical comfort . hence , we compared plan quality and efciency of radiosurgery in fff mode to ff techniques . materials and methods between november 2014 and june 2015 , 21 consecutive patients with 25 brain metastases were treated with stereotactic radiosurgery ( srs ) in fff mode . brain metastases received dose - fractionation schedules of 1 20 gy or 1 18 gy , delivered to the conformally enclosing 80 % isodose . 
fff plans were compared to those using the ff method , and early clinical outcome and toxicity were assessed . results fff mode resulted in signicant reductions in beam - on time ( p < 0.001 ) and mean brain dose ( p = 0.001 ) relative to ff - mode comparison plans . 
die zustzliche anwendung von ausgleichslterfreien bestrahlungstechniken ( fff ) kann die bestrahlungszeit verkrzen und den patientenkomfort erhhen . daher fhrten wir einen planund efzienzvergleich zwischen der radiochirurgie in fff - technik und ff - technik durch . 790 strahlenther onkol ( 2016 ) 192 : 789796 material und methode zwischen november 2014 und juni 2015 wurden 21 patienten mit 25 hirnmetastasen mit srs in fff - technik behandelt . 
des weiteren wurden berleben und toxizitt analysiert . ergebnisse sowohl die bestrahlungszeit sank signikant um 57 , 9 % ( p ( cid : 2 ) 0 , 001 ) fr die srs in fff - technik im vergleich zur ff - technik . 
des weiteren wurden signikant verbesserte dosisgradienten und folglich ein steilerer dosisabfall fr die srs in fff - technik ( 1 , 1 % , 29 , 6 % ; p ( cid : 2 ) 0 , 003 ) festgestellt . 
bei den behandelten 25 hirnmetastasen ( 96 % ) waren 24 ohne lokalen progress . schlussfolgerung srs in fff - technik ist zeitefzient und ermglicht gleiche planqualitt sowie eine leicht reduzierte dosisbelastung des gesunden hirngewebes im vergleich zur srs in ff - technik . 
entsprechend vielversprechend sind die ersten klinischen ergebnisse bei moderater toxizitt . schlsselwrter radiochirurgie stereotaktische bestrahlung ausgleichslterfrei hirnmetastasen planvergleich introduction stereotactic radiosurgery ( srs ) has since the 1980s , evolved into a precise and effective treatment option with minimal morbidity for patients with oligometastatic cranial disease [ 15 ]  . 
srs is particularly useful for the treatment of single brain metastases less than 3 cm in diameter in patients with a life expectancy of more than 3 months [ 6 , 7 ]  . 
for patients with 24 brain metastases , srs is preferred over whole - brain radiotherapy ( wbrt ) given srs minimizes neurocognitive side effects and yields improved quality of life [ 8 ]  . 
furthermore , adjuvant wbrt following srs has not been shown to improve survival when compared to srs with salvage wbrt [ 6 , 9 ]  . srs is a noninvasive , highly conformal technique that allows for high single doses of radiation to be delivered in an effort to effectively ablate metastatic disease [ 10 ]  . 
however , long duration of radiotherapy fractions with single doses up to 20 gy has been a worry for many patients who are commonly positioned within rigid and uncomfortable masks . 
in an effort to reduce treatment time , the attening lter ( ff ) of a linac can be removed leading to a higher doserate delivery and thereby substantially shortening beam - on time . by utilizing these steep dose gradients surrounding normal tissue is spared to a greater extent than could be achieved with conventional radiotherapy [ 11 ]  . 
in addition , these attening - lter - free ( fff ) techniques have certain dosimetric advantages with lower out - of - eld dose due to reduced head scatter , leaf transmission , and lower dose outside the eld edge [ 12 , 13 ]  . in our institution , this method has been clinically available for over a year . 
here we report the dosimetric and clinical outcomes of 21 patients with 25 brain metastases treated with srs in fff mode relative to standard ff mode . materials and methods patients and brain metastases patient characteristics are summarized in table 1 . 
for treatment planning , the gross tumor volume ( gtv ) of each brain metastasis was delineated on both contrast - enhanced computer tomography ( ct ) and magnetic resonance imaging ( mri )  . 
as the geometric accuracy due to intrafractional movement was expected to be in the range of 23 mm , a safety margin of 3 mm was expanded from gtv to create the planning target volume ( ptv )  . 
prior to irradiation , image guidance was performed by means of kv cone beam ct ( cbct )  . concordant plans in ff mode were created for each treated lesions . 
delivery techniques comprised strahlenther onkol ( 2016 ) 192 : 789796 table 1 patient characteristics of 21 patients with 25 brain metastases plan evaluation and comparison for comparative plan evaluation , 6 mv attening lter plans were calculated . 
not dened , nsclc non - small cell lung cancer 3 - dimensional ( 3d ) conventional ( n = 21 ) , step - and - shoot intensity - modulated radiotherapy ( step - and - shoot imrt ; n = 3 ) and volumetric modulated arc therapy ( vmat ; n = 1 ) radiotherapy in fff and ff mode , respectively . 
stepand - shoot imrt and vmat plans were applied whenever dose coverage was inadequate with 3d conventional plans . a collapsed cone ( cc ) algorithm was used for dose calculation . 
all patients were treated with 6 mv attening lter - free plans using the elekta versa hd with a maximum dose rate of 1400 mu / mthe multileaf collimator ( mlc ) agility with 5 mm leafs at the isocenter was used for radiation delivery . where vptv , pi is the partial volume of the ptv covered by the prescribed isodose , vptv is the planning target volume , and vpi is the body volume of the patient covered by the prescribed isodose [ 15 ]  . 
hence , a score of 1.0 indicates perfect conformity , while a score of less than 1 shows inferior conformity . in addition , two gradient indices as described by paddick et al . 
the other three fractionated plans were normalized such that the prescription dose was the median dose to the ptv . no detailed analysis of organs at risk ( oar ) as chiasma or optical nerves was conducted as their distance from the ptv was too long to result in clinically meaningful dose exposure . 
furthermore , beam - on and total treatment times were also calculated for ff plans for comparison . outcome evaluation all patients were seen for follow - up visits at the university hospital and underwent a clinical examination . 
1 overall survival ( a ) and local progression - free survival . ( b ) after radiosurgery in fff mode strahlenther onkol ( 2016 ) 192 : 789796 follow - up ( months ) follow - up ( months ) signed - rank test . 
outcome was calculated using the kaplanmeier method and treatment - related toxicity was classied according to ctcae v4.0. results planning procedure and technical administration in total , 21 patients with up to 3 brain metastases were treated using srs in fff mode . 
patient characteristics are shown in table 1 . to show comparability between fff and ff techniques , we generated both fff and ff plans for all lesions with the respective technique . 
one patient developed asymptomatic intracerebral * value considered signicant gilow gihigh beam - on time ( min ) treatment time ( min ) monitor units ( mu ) strahlenther onkol ( 2016 ) 192 : 789796 planning mri planning mri 1 . 
b after 6 months the initially treated left temporal brain metastasis delineates complete treatment response , however a further temporopolar brain metastasis is newly diagnosed and also treated with radiosurgery . 
furthermore , we performed plan comparisons and time efciency analysis of srs with fff technique to treatment in ff mode for all patients . in recent years , srs has been increasingly utilized for treatment of brain metastases as it is known to be safe and highly efcient [ 7 , 9 ]  . 
a current report of the degro working group on stereotactic radiotherapy recommends considering srs as treatment for patients with 14 brain metastases ( < 2.5 cm ) and a life expectancy of more than 3 months [ 6 ]  . 
according to the graded prognostic assessment scores dened by sperduto et al . [ 14 ] , all patients in this study showed a life expectancy of more than 3 months ( median life expectancy 9.4 months [ range 3.115.1 months ] ) and hence were candidates for srs . however , a recent meta - analysis compared three prospective trials investigating srs with or without wbrt for patients with 14 brain metastases and showed that patients > 55 years of age had a signicantly increased risk of intracranial failure following srs alone [ 19 ]  . 
however , the above mentioned meta - analysis failed to show that srs had a statistically signicant negative impact on survival in this cohort [ 19 ]  . in line with these results , the eortc 22952 - 26001 study reported that wbrt after srs or surgery did not improve the duration of functional independence and os [ 20 ]  . 
hence , the degro guideline recommends to withhold wbrt for as long as possible for patients with 14 small ( < 2.5 cm ) brain metastases , as wbrt carries the risk of causing neurocognitive decline [ 20 ]  . two recent trials even questioned whether primary treatment with srs could also be extended to patients with larger numbers of brain metastases [ 21 , 22 ]  . 
 [ 22 ] reported that srs alone as initial treatment for patients with ve to ten brain metastases demonstrated noninferior survival compared to patients with two to four brain metastases . however , radiotherapy with srs using conventional linacs is known to last up to 4560 mhence , treatment of multiple brain metastases would force patients to spend hours in rigid and uncomfortable scotch cast masks . 
hence , radiosurgery using high doses per fraction is an ideal treatment for utilization of the fff technique . one further advantage of fff beams is believed to be their different physical characteristics when compared to conventional unattened photon beams . 
removing the attening lter leads to a reduction of out - of - eld dose due to reduced head scatter , leaf transmission , and lower dose outside the eld edge [ 11 , 12 , 24 ]  . 
in summary , we detected a slight reduction in strahlenther onkol ( 2016 ) 192 : 789796 mean brain dose which may be of only minor clinical relevance . we also showed improved dose gradients and sharper dose falloff for srs in fff mode compared to srs in ff mode . 
in general , using highly variable treatment techniques ( 3d conformal radiotherapy , volumetric modulated arc therapy [ vmat ] and step - and - shoot intensitymodulated radiotherapy [ step - and - shoot imrt ] ) and analyzing radiotherapy for different tumor locations and sizes , several previous studies described similar plan quality and oar sparing for radiotherapy in fff mode compared to ff technique [ 2632 ]  . regarding other radiosurgery devices , there is evidence that plan quality is probably improved when performing srs with cyberor gammaknife compared to srs with classical linacs [ 33 , 34 ]  . 
the further usage of fff mode with vmat techniques might provide optimal plan quality for metastases at critical locations combined with faster treatment time compared to cyberor gammaknife irradiation . although fff beams have been increasingly applied in patient treatment , only few clinical data regarding their safety and clinical efcacy have been reported . 
clinical data with respect to toxicity and outcome for fff treatment have mainly been reported by an italian group from irccs instituto clinico humanitas in milan [ 26 , 3739 ]  . analyzing 25 oligometastatic patients with isolated abdominal or pelvic lymph nodes treated with vmat using fff beams , they detected no local progression or toxicity ctcae 3 after 6 months [ 38 ]  . 
furthermore , they recently showed preliminary results of a phase ii study investigating the clinical potential of hypofractionated radiotherapy strahlenther onkol ( 2016 ) 192 : 789796 in prostate cancer and reported only minimal acute toxic [ 40 ] reported ity [ 37 ]  . 
a previous study by stieb et al . minimal toxicity and excellent 1 - year local control using sbrt in fff technique for various tumors of 84 patients . similar results were also shown by prendergast and wang investigating feasibility of sbrt for patients with et al . lung malignancies and hepatocellular carcinoma , respectively [ 41 , 42 ]  . 
furthermore , our study is one of the few studies which did not only perform comparative plan and time efciency analysis but also provided preliminary clinical data for the analyzed patients . one limitation to the study was the relatively short follow - up time which was caused by the fact that radiosurgery treatment in fff mode has only been available for 18 months at our institution . 
in addition , all clinical analyses were performed retrospectively on the basis of medical records which may have led to an underestimation of side effects . conclusion patient treatment with srs in fff mode was time efcient and safe . 
in general , plan quality was comparable between srs in ff mode and fff technique ; however srs in fff technique provided slightly reduced dose spillage to normal brain parenchyma . acknowledgements this work was supported by the medical faculty providing a research grant for jr . compliance with ethical guidelines conict of interest j . 
rieken declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
this study compared riskbenet proles of upfront and salvage iodine - 125 brachytherapy ( sbt ) for small brain metastases . as the applied sbt treatment algorithm required histologic proof of metastatic brain disease in all patients , we additionally aimed to elucidate the value of biopsy before sbt . patients and methods patients with small untreated ( n = 20 ) or pre - irradiated ( n = 28 ) suspected metastases intended for upfront or salvage sbt , respectively , were consecutively included . 
temporary iodine - 125 implants were used ( median reference dose : 50 gy , median dose rate : 15 cgy / h )  . cumulative biologically effective doses ( bed ) were calculated and used for risk assessment . 
treatment toxicity was classied according to radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc ) criteria . results upfront sbt was initiated in 20 patients and salvage sbt in 23 . 
histologic reevaluation should be reconsidered after previous radiotherapy to avoid underor overtreatment . keywords radiotherapy toxicity biopsy neoplasms , radiation - induced molecular imaging jod - 125 - brachytherapie als primrund rezidivtherapie von intrakraniellen metastasen eine vergleichsstudie zusammenfassung hintergrund daten zu risiko und efzienz ablativer stereotaktischer rebestrahlungsstrategien zerebraler metastasen sind kaum publiziert worden . 
dieses einheitliche vorgehen erlaubte , zustzlich den stellenwert bioptischer verfahren zu analysieren . patienten und methoden patienten mit kleinen unbehandelten ( n = 20 ) oder vorbestrahlen ( n = 28 ) metastasensustrahlenther onkol ( 2016 ) 192 : 780788 fig . 
while the implanted left cerebellar lesion ( a ) showed complete response 8 months after iodine - 125 brachytherapy ( b ) , two new distant intracranial metastases were seen in the same mri scan ( c , d ) and were than treated with stereotactic radiosurgery spekten lsionen wurden konsekutiv eingeschlossen . 
implantiert wurden temporre jod - 125 - seeds ( mediane referenzdosis : 50 gy , mediane energiedosisleistung : 15 cgy / h )  . fr risikoanalysen berechneten wir die kumulative biologische effektive dosis ( bed )  . 
die klassikation der neurotoxizitt erfolgte entsprechend den kriterien der rtog / eortc ( radiation therapy oncology group / european organization for research and treatment of cancer )  . ergebnisse sbt als initialtherapie wurde bei 20 patienten und als rezidivtherapie bei 23 patienten durchgefhrt . 
eine toxizitt vom grad i / ii fand sich bei 2 patienten ( kumulative bed : 192 , 1 gy3 und 249 , 6 gy3 )  . schlussfolgerung sbt verbindet diagnostische genauigkeit mit effektiver behandlung . 
die indikation zur histologischen reevaluation sollte nach vorausgegangener bestrahlung immer erwogen werden , um unteroder berbehandlungen zu vermeiden . schlsselwrter strahlentherapie toxizitt biopsie neoplasien , strahleninduzierte molekulare bildgebung ablative stereotactic high - dose radiation strategies are increasingly used for small brain metastases of limited number [ 14 ]  . 
these strategies are effective , well tolerated , and can be applied in any location in the brain [ 5 , 6 ]  . in contrast , the outcome and toxicity proles of salvage high - dose radiotherapy of recurrent , previously irradiated brain metastases are poorly dened [ 79 ]  . 
whereas in the de novo situation histologic proof of disease is strongly recommended for selected patients with an unknown primary tumor or those exhibiting long latency periods between the occurrence of primary tumor and that of brain disease , no widely accepted diagnostic recommendations exist for patients with suspected progressive brain disease after previous radiotherapy . 
it remains unknown whether all patients with suspected tumor recurrence after previous irradiation need histologic verication of recurrence before initiation of salvage radiotherapy / radiosurgery [ 6 , 11 , 12 ]  . conventional mri lacks the sensitivity and specicity to discriminate between tumor recurrence and radiation - induced neoplasms [ 13 ]  . 
the green line represents the trajectory for stereotactic implantation low - activity sbt , it was expected that salvage sbt would not rate worse on toxicity scales as compared to upfront treatment . 
it was further hypothesized that biopsy before salvage radiotherapy / radiosurgery is necessary in case of suspected progressive pre - irradiated brain metastases . racy after high - dose radiation has not been systematically analyzed . in the current study , the outcome and toxicity proles of upfront and salvage iodine - 125 brachytherapy ( sbt ) was analyzed and compared in selected patients with either small untreated metastases or suspected progressive disease . 
patients with a karnofsky performance score ( kps ) 70 and an estimated survival prognosis of at least 3 months undergoing biopsy plus sbt were considered eligible for this study . in the de novo group , biopsy was indicated because of unknown primary cancer or long latency period ( > 3 years ) between the primary cancer diagnosis and the appearance of cerebral disease . 
in the salvage group , histologic proof of recurrence was always considered to be necessary by the interdisciplinary tumor board . minimal invasive surgery with biopsy plus sbt was preferred over conventional tumor resection strategies ( by the interdisciplinary tumor board ) in resectable small tumors of unknown / uncertain histology with no / moderate spaceoccupying effects and / or those with unfavorable risk proles . 
briey , three - dimensional ( 3d ) treatment planning was based on preoperative computerized tomography ( ct ) and magnetic resonance imaging ( mri ) sequences , including an axial t2 - weighted sequence , an isovoxel ( 3d ) contrast - enhanced t1 - weighted gradient - echo sequence , and a contrast - enhanced mr - angiography , which were fused to the preoperative localized ct scan . 
the tissue diagnosis was made intraoperatively by the attending neuropathologist . the contrast - enhancing tumor parts , including necrotic areas if present , were considered the treatment volume and outlined in each slice of the axial gadolinium - enhanced mri . 
exclusively temporary low - activity ( 21 mci ) i - 125 seeds ( model : oncoseedtm imc6711 ; oncura ltd . , austin , tx , usa ) were used . 
the seed catheters were subsequently stereotactically placed , each of them through a 2 - mm burr hole , and secured directly above the calvaria with a hemoclip and an overlying tight cutaneous suture . 
overall hospitalization time for sbt was 4 days . seed removal was carried out under local anesthesia . follow - up evaluation and radiologic assessment clinical parameters were determined using patients electronic medical records and paper charts . 
neurologic status and kps were assessed preoperatively , at discharge , at seed removal , and routinely every 3 months thereafter in combination with mri scans . in - eld and distant brain failure was determined according to the macdonald criteria [ 18 ]  . 
in the case of a local recurrence , re - biopsy was always considered necessary before initiation of further treatment . 784 strahlenther onkol ( 2016 ) 192 : 780788 ered as neurologic deaths ; otherwise , systemic death was assumed . 
the distribution of continuously scaled ( categorical ) variables was analyzed with the wilcoxon test ( chi - square statistics )  . prognostic factors were obtained from univariate and multivariate proportional hazards models . 
all analyses were performed on an intent - to - treat basis . results study population a total of 48 consecutively treated patients ( de novo group : n = 20 ; salvage group : n = 28 ) were included . 
in the salvage group , median follow - up of the survivors after initial diagnosis and after sbt was 31.9 months ( range 1273 months ) and 19.7 months ( range 949 months ) , respectively . 
median follow - up times after sbt did not signicantly differ between the treatment groups . stereotactic biopsy indicated metastatic disease in 43 patients ; however , in 5 patients of the salvage group , reactive gliotic lesions were found and sbt was withheld accordingly . 
in the salvage group ( n = 23 ) , more than one pretreated metastasis was seen in 11 cases ( 2 in 7 patients , 3 in 2 patients , 4 in 2 patients )  . 
the overall median tumor volume was 3.4 ml ( range 0.29.9 ml ; diameter 1.9 cm , range 0.72.7 cm ) ; median treatment time was 400 h ( range 120936 h )  . 
wbrt whole brain radiation therapy recurrent assessment of the biologically effective dose and treatment toxicity the cumulative biologically effective dose ( bed ) after treatment was calculated for the tumor undergoing sbt ( bed gy10 ) and in the direct vicinity outside the tumor for late - responding tissue ( bed gy3 )  . 
this approach allows comparison of the bed values of the de novo group with those of the recurrent group and , in contrast to other models , takes into account the tumor repopulation as a time factor k ( k = 0.6 gy day1 [ 20 ] )  . 
treatment toxicity was assessed using the radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc ) criteria [ 21 ]  . statistical analysis reference points of the study were the date of sbt and the date of initial diagnosis of the brain metastasis . 
the median overall cumulative bed of late - reacting tissue was 57.2 gy3 in the de novo group and 180.7 gy3 in the salvage group ( p = 0.002 ; table 2 )  . 
3 ; 6 patients were retreated with iodine - 125 seeds because of distant tumor recurrences . outcome at the time of last follow - up , 29 patients had died . 
none of the analyzed patient - , tumor - , and treatment - related factors had a prognostic impact on tumor control rates or os in univariate or multivariate models ( data not shown )  . treatment toxicity there was no perioperative morbidity or mortality . 
overall , 2 patients in the salvage group had received a cumulative bed between 185 and 195 gy3 , and another 9 patients a cumulative bed > 200 gy3 ( median 232 gy3 )  . 
edema resolved after steroid application 1 month later in 1 patient ; edema development in the other patient was overshadowed by progressive tumor growth . discussion salvage treatment concepts for brain metastases are poorly dened [ 9 , 23 ]  . 
to the best of the authors knowledge , this is the rst analysis comparing the outcome and toxicity proles of salvage sbt for recurrent tumors with that of upfront sbt for de novo lesions . 
a overall survival after rst diagnosis of a cerebral metastasis ; b survival after iodine - 125 brachytherapy ; c local tumor control rates ; d distant tumor control rate sbt was safe and similarly effective in both the de novo and the salvage groups . the presented results underscore the importance of stereotactic biopsy in cases of previously performed radiotherapy . 
whereas the suspicion of metastatic disease was conrmed in all patients of the de novo group , 5 out of 28 patients of the salvage group did not exhibit tumor progression even though imaging had strongly pointed in that direction : biopsy - proven radiation - induced reactive lesions resolved over time in all of these patients as demonstrated by mri follow - up . 
in this study , high sensitivity , specicity , and accuracy values ( 95 % , 91 % , and 93 % , respectively ) could be assessed combining static and dynamic pet parameters [ 14 ]  . 
moreover , the risk prole seems not to be inuenced by tumor location : no functional deterioration was observed , even in cases of highly eloquent tumor location . this by no means indicates that the cumulative dose does not matter in the framework of sbt treatment : the 2 patients suffering from grade i / ii treatment toxicity exhibited extremely high cumulative bed3 values . because of the low number of adverse events , we could not identify a threshold for bed values predictive for radiogenic complications . 
transient symptomatic edema occurred in 2 patents receiving a cumulative bed > 190 gy3 . however , most patients of this series treated with a cumulative bed > 200 gy3 did not exhibit any signs of acute or delayed toxicity , potentially highlighting favorable radiobiologic characteristics of continuous low - dose rate irradiation . 
a recently published meta - analysis of reirradiation studies in malignant gliomas has found radiation - induced normal brain tissue necrosis to occur at cumulative bed2 values > 200 gy2 [ 25 ]  . 
it remains a matter of speculation whether this threshold could be increased by use of sbt strahlenther onkol ( 2016 ) 192 : 780788 without increasing the risk of severe toxicity in selected small pre - irradiated metastases . 
so far , careful balancing of the possibility of local control versus toxicity under consideration of alternative treatment concepts ( such as surgery ) is mandatory for these patients . the results of this comparative analysis support ndings of previously published reports dealing either with sbt of de novo tumors or sbt of recurrent lesions , and underscore the role of sbt as a safe and effective treatment option with tumor control rates in the range of those reported for srs [ 6 , 26 , 27 ]  . 
the presented data might provide a basis upon which other treatment modalities dealing with similar tumors can be compared . this analysis has limitations : the tumor volume in the salvage group was smaller than that in the de novo group . even though the difference did not reach statistical signicance , a selection bias in favor of the salvage group cannot be excluded . 
a larger sample size is necessary to dene both bed and tumor volume thresholds for a riskadjusted use of salvage sbt , as well as to identify prognostic factors for outcome measurements . 
given the increasing number of patients with recurrent brain metastases , the elucidation of outcome and toxicity proles of the respective salvage treatment options is a prerequisite for personalized treatment concepts . conclusion it is highly likely that the number of patients needing salvage treatment for recurrent brain metastases will increase during the coming years . 
the favorable biologic characteristics of sbt and the possibility of histologic diagnosis render this treatment modality particularly suitable for recurrences of small metastases after previously performed wbrt and / or srs . compliance with ethical guidelines conict of interest a . 
nachbichler report no conict of interest concerning the materials or methods used in this study or the ndings specied in this paper . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
adeberg1 , 2 , 3 , 4 received : 6 january 2016 / accepted : 20 may 2016 / published online : 30 june 2016 the author ( s ) 2016 . 
this article is available at springerlink with open access . abstract background and purpose low - grade glioma ( lgg ) is a very common brain tumor in pediatric patients typically associated with a very good prognosis . 
this prognosis makes it imperative that the risk of long - term treatment - related side effects be kept at an absolute minimuproton therapy ( prt ) provides a radiation technique that has the potential to further reduce the genesis of radiogenic impairment . materials and methods we retrospectively assessed 74 patients with lgg who underwent prt . 
of radiation oncology , university hospital heidelberg , im neuenheimer feld 400 , 69120 heidelberg , germany 4 clinical cooperation unit radiation oncology , german cancer research center ( dkfz ) , im neuenheimer feld 280 , 69120 heidelberg , germany 5 department of medical physics in radiation oncology , german cancer research center ( dkfz ) , im neuenheimer feld 280 , 69120 heidelberg , germany 6 department of radiation sciences ( drs ) , institute of innovative radiotherapy ( irt ) , helmholtz zentrum mnchen , ingolstdter landstrae 1 , 85764 oberschleiheim , germany partner site munich , deutsches konsortium fr translationale krebsforschung ( dktk ) , munich , germany homogeneity index ( hi ) and inhomogeneity coefcient ( ic )  . 
overall , we could show an essential reduction in maximal , mean , and integral doses in critical neurologic structures , areas of neurogenesis , and structures of neurocognitive function . 
the study indicated specically how contralaterally located structures could be spared with prt . conclusion prt is a highly conformal radiation technique offering superior dosimetric advantages over conventional radiotherapy by allowing signicant dose reduction for organs at risk ( oar ) that are essential for neurologic function , neurocognition , and quality of life , thus demonstrating the potential of this technique for minimizing long - term sequelae . keywords brain tumors children neurogenesis quality of life organs at risk dosimetrische vorteile der protonentherapie gegenber der konventionellen strahlentherapie mit photonen bei jungen patienten und erwachsenen mit niedriggradigem gliom zusammenfassung hintergrund und ziel niedriggradige gliome ( lgg ) zhlen zu den hugsten hirntumoren im kindesalter und sind blicherweise mit einer sehr guten prognose vergesellschaftet . 
mit der protonenbestrahlung steht eine bestrahlungsmodalitt zur verfgung , mit der das auftreten radiogener sptfolgen im vergleich 760 strahlenther onkol ( 2016 ) 192 : 759769 zu konventionellen bestrahlungstechniken weiter minimiert werden knnte . material und methoden fr diese studie wurden 74 konsekutive patienten retrospektiv ausgewertet , die aufgrund eines lgg einer protonenbestrahlung unterzogen wurden . ergnzend wurden zunchst auf der planungscomputertomographie die fr neurokognitive funktionen relevanten zentren sowie strukturen der neurogenese identiziert und konturiert ; anschlieend wurden korrelierende konventionelle photonenplne berechnet . 
die zielvolumenabdeckung wurde mithilfe des homogenittsindex ( hi ) und des inhomogenittskoefzienten ( ic ) beurteilt und die ergebnisse mit dem wilcoxon - vorzeichen - rang - test verglichen , wobei ein p - wert < 0 , 05 als statistisch signikant gewertet wurde . ergebnisse die zielvolumenabdeckung war sowohl fr photonenals auch fr protonenplne vergleichbar . 
dies gilt in besonderem mae fr die dem tumor kontralateral gelegene hemisphre . schlussfolgerung die protonenbestrahlung zeigt eine der konventionellen radiotherapie mit photonen in hinblick auf risikoorganschonung bei weitem berlegene dosimetrische verteilung , mit dem groen potential , radiogene sptfolgen wie die beeintrchtigung neurologischer und neurokognitiver funktionen und der lebensqualitt zu minimieren . schlsselwrter hirntumor kinder neurogenese lebensqualitt risikoorgane low - grade gliomas ( lgg ) are the most common type of brain tumor in children . 
today , the prognosis is very good and pediatric patients are expected to become long - term it is , therefore , essential to reduce the risk of survivors . long - term side effects as much as possible . surgery is generally accepted as the rst - line treatment if a complete resection can be achieved without major neurologic impairment . 
however , in many cases , only a partial resection or biopsy can be performed due to an unfavorable localization in proximity to vital structures such as the brainstem , optic system , pituitary , hypothalamus , or other areas of the brain with critical functions . 
since the risk for disease progression is signicantly higher in cases of subtotal compared to complete resection [ 1 ] , radiotherapy plays an important role in the treatment of pediatric lgg . 
the recommended lower age limit for initiation of radiotherapy differs among international protocols : european trials set the threshold at 8 years of age [ 4 ] , while north american studies advise waiting until the age of 10 [ 5 ]  . 
however , adult patients also show a tendency to develop dementia more frequently after cranial irradiation [ 6 ] , which is known to be related to a signicant impairment of the patients quality of life . over time , many technical advances , such as three - dimensional ( 3d ) treatment planning , image guidance , intensity modulation , and particle therapy , have been adopted in daily routine , leading to incremental improvements in terms of conformity . 
a multitude of data is available for 3d - crt , but long - term studies of prt are still scarce . along with the commissioning of new proton facilities , the use of prt is rapidly increasing [ 10 ]  . 
due to its distinct biophysical properties with typically low doses in the beam entrance area and a nearly complete dose deposition in the so - called bragg - peak , prt is a highly conformal technique that allows steep dose gradients . 
as a result , excellent target coverage can be maintained without compromises due to nearby critical oar because their tolerances are not exceeded . in view of the dosimetric superiority of prt compared to 3d - crt , this study was conducted to present in detail the inuence on structures that are essential for neurocognitive function , in addition to specic oar that are responsible for neurologic side effects or impairment of quality of life . 
however , there are several risk factors for the development of neurocognitive dysfunction : in addition to radiotherapy , tumor localization , the extent of resection , and concomitant chemotherapy are recognized risk factors [ 13 ]  . 
the authors set out to determine and quantify the superiority of prt in terms of dose distribution for the abovementioned oar and , thereby , evaluate the potential benet with regard to long - term radiogenic sequelae . materials and methods patient selection a total of 74 patients with histologically proven lgg originally treated at the authors institution between 2012 and 2014 were retrospectively selected for this comparative study . 
all patients underwent 3d - prt or intensity - modulated proton therapy ( impt ) with a median dose of 54 gy ( range 50.460 gy ) in 1.8 gy per fraction ( range 1.82.0 gy ) , with a horizontal beamline using the raster scanning technique [ 14 ]  . 
in the authors study group , at the time of initial treatment planning and delivery , the additional oar were not explicitly contoured , monitored , or used as avoidance structures for either treatment technique . 
contouring of the initial and additional oar and the treatment volume denition for photon and particle therapy planning was performed using the siemens dosimetrist and oncologist software ( siemens , erlangen , germany )  . 
ipsilateral ( il ) and contralateral ( cl ) subventricular zones ( svz ) were contoured as a 5 - mm margin lateral to the lateral ventricles as previously described [ 15 , 16 ]  . the hippocampus and amygdala were contoured according to previously published guidelines [ 17 ]  . 
treatment planning was performed by a single experienced radiation therapist using the oncentra masterplan ( nucletron , columbia , sc , usa ) planning system , version 4.5 , with a collapsed cone algorithm for 3d photon treatment planning . 
in 3d - crt , beam directions were carefully selected and consisted of four to ve coplanar and non - coplanar elds in the majority of cases and , if necessary , subelds , using a eld - in - eld ( fif ) technique . for all patients , 6 - mv photons were used . 
the pencil beams chosen for the prt typically had a lateral full width at half maximum ( fwhm ) of 10 mthe treatment table position was restricted to between 10 and 170 degrees to avoid collisions of the horizontal beam nozzle with the table . 
planning target volume ( ptv ) coverage of 95 % of the prescribed dose was required and in all patients , at the time of treatment planning and delivery , the additional oar were monitored but not considered an avoidance structure in either radiotherapy modality . treatment plan evaluation qualitative and quantitative dose evaluations were conducted for both radiotherapy modalities . 
dosevolume histograms ( dvhs ) were constructed for all volumes , and 762 strahlenther onkol ( 2016 ) 192 : 759769 dose parameters were extracted to check for proper target volume coverage and to assure compliance with the oar dose constraints . 
conrmation of ptv dose distribution was evaluated by calculating hi and ic . homogene it y index ( hi ) = d5 d95 x 100 inhomogeneit y coe f f icient ( ic ) = dmax dmin dmean d5 and d95 are the minimum doses in 5 % and 95 % of the ptv , respectively , and dp is the prescribed dose in the ptv . 
the ideal hi value is zero , where d5 equals d95 [ 26 ]  . the ic assesses the distribution variance of the ptv dose , where higher values indicate greater variability [ 27 ]  . 
dmax and dmin represent the maximum and minimum doses in the ptv , respectively , and dmean equals the average ptv dose . data management and automatic dosevolume analysis all prt data and additional treatment information were available in the central research database of the authors department , which functioned as the central data source project - specic oar like previously described [ 29 ]  . re - contouring and 3d - crt data were additionally imported into the central research database after re - planning . dosevolume analysis was performed automatically on a central analysis platform directly connected to the central research database like previously described [ 30 ]  . 
all results were written into the central storage of the analysis platforfinally , results for all patients were summarized in a single result le for further statistical analysis . inte gral dose ( id ) = dmeanvi ethics the integral dose ( id ) is dened as the sum of the mean dose multiplied by the volume if the voxels are assumed to be the same size and the organ is hypothesized to have a uniform density . 
no statistically signicant difference could be detected regarding v90 % and v95 % ( percentage of ptv receiving a minimum of 90 and 95 % of the prescribed dose , respectively )  . 
1 cumulative dosevolume histogram dvh ( n = 74 ) comparing planning target coverage for both proton beam therapy ( prt ) and three - dimensional conventional radiotherapy ( 3d - crt ) table 3 dose comparison of organs at risk 3d - crt ( relative dose in % sd ) ( relative dose in % sd ) 3d - crt vs . 
svz subventricular zone critical organs of neurogenesis it has been shown that neuronal stem cellsinitiating cells for neurogenesis even in adult individualsare extremely sensitive [ 31 ] and show diverse recovery behaviors after exposure to ionizing radiation [ 32 ]  . 
3 cumulative dosevolume histograms for unifocal organs at risk showing a signicant dose reduction for proton beam therapy compared to three - dimensional conventional radiotherapy discussion these data present an overwhelming dosimetric advantage of prt over 3d - crt in terms of sparing not only stem cell niches , but also nearly any other oar . 
particular attention must be paid to structures that are considered essential for neurocognitive functions , such as the hippocampus or the svz . there are several reports of treatment planning comparisons for various entities . 
their study showed a reduction of the id received by the hippocampus of up to 51 % and up to 57 % for the svz [ 33 ] , whereby intensity modulated prt had the largest potential for relative dose reduction . 
a decrease in id was also noted for the chiasm ( 11 % ) and the pituitary ( 13 % )  . likewise , dosimetric superiority for the whole brain , temporal lobes , chiasm , and cochlea could be demonstrated in both supratentorial and infratentorial locations [ 10 , 35 , 36 ]  . the id represents a valuable option for considering oar volumes in the dosimetric assessment . 
here the id should offer objective values , which allow for improved evaluation of lower dose spreads compared to dmean or median dose . however , even the id is not able to predict normal toxicity complication probability ( ntcp ) without correlation of clinical long - term toxicity data . 
especially in children , a decrease in intelligence quotient ( iq ) , processing speed , and ne motor skills has been reported [ 3739 ]  . our particular focus was on the exposure of structures constrahlenther onkol ( 2016 ) 192 : 759769 diation - induced neurocognitive impairment is most likely multifactorial [ 13 , 39 ] ; however , there is growing evidence that supports the idea that neural progenitor cells ( npcs ) in stem cell niches play an important role . 
the hippocampus and the svz are known areas of origin for npcs [ 11 , 12 ]  . although their role has not yet been fully elucidated , it is hypothesized that their capability for self - renewal and injury repair is of central importance to the genesis of longterm neurocognitive effects [ 41 , 42 ]  . 
one of the reasons is attributed to its potential to contribute to tumor propagation [ 44 ]  . as the current ndings show , inter alia , prt is an excellent treatment option that does not compromise target coverage . 
here , prt allows for improved sparing of centrally localized neuronal structures like the hippocampus , optic chiasm , brainstem , and pituitary gland . preliminary results from the prospective radiation therapy oncology group ( rtog 0933 ) described the effect of hippocampal sparing during whole brain irradiation and concluded that decreased short - term memory impairment compared to historical controls is attributed to sparing of stem cell niches [ 45 ]  . 
whether , and how , these preliminary results will be reected in a clinically relevant decrease of treatment - related long - term toxicity remains to be seen and , of course , substantiated by long - term results . although the present ndings provide strong evidence in favor of prt , their limitations should be considered . 
first , following the recommendation of the german society of radiation oncology ( degro ) , prt should be used subject to disease , localization and availability of patients with lgg , as they are particularly appropriate candidates . 
lgg is the most common diagnosis of central nervous system malignancy in pediatric patients and the use of radiotherapy must inevitably be considered , especially in patients presenting with an unfavorable or irresectable tumor location . 
equally interesting would be the possibility of taking the sensitive oar into consideration for treatment planning initially and also consideration of whether there is an additional potential for sparing oar with protons , as is well - known from earlier fig . 
in contrast to a general assessment of dose distribution ( whole brain , supratentorial , infratentorial , temporal lobe ) , a more detailed analysis substantiated by clinical parameters could lead to a better understanding and risk assessment for the occurrence of neurocognitive impairment . 
the authors collected dosimetric information for 40 patients with different types of childhood brain tumors and calculated the estimated decline in their full scale iqs using dosedependent cognitive effect models [ 40 ]  . 
the reason for ra768 strahlenther onkol ( 2016 ) 192 : 759769 planning studies with photons based on the motto that seeing is saving . the strength of this study is its large number of patients with proven lgg . 
to our knowledge , this is the largest case series of lgg patients , providing valuable dosimetric information because of its homogenous distribution to all lobes of the brato minimize interobserver variability , all oar and all treatment plans were contoured / performed by the same experienced radiation oncologist . 
the information obtained by the presented analysis is not only helpful for identifying patients who would potentially benet from prt , but also provides important arguments in interdisciplinary discussions about why the effort should be made to expand access to prt . however , as previously stated , the availability of proton centers remains limited . 
this is why the authors goal is to acquire new data and correlate dosimetric information with functional outcomes , potentially providing further selection criteria for patients who would benet signicantly from prt . conclusion the dose distribution of prt is signicantly superior when compared to conventional radiotherapy , particularly with regard to oar that are considered essential for neurologic function and neurocognition , or which play an important role in terms of quality of life . 
eine aktuelle , sehr groe kohortenanalyse belegt aber den hohen stellenwert der strahlentherapie und zeigt auch einen signikanten berlebensvorteil [ 9 ]  . patienten und methoden die autoren fhrten eine propensity score - matched fall - kontroll - studie anhand der daten der national cancer data base der usa durch . eingeschlossen wurden erwachsene patienten mit retroperitonealen sarkomen und behandlung in den jahren 2003 bis 2011 . 
eingeschlossen waren alle histologien sowie auch patienten mit positiven resektionsrndern . originalpublikation nussbaum dp , rushing cn , lane wo et al ( 2016 ) preoperative or postoperative radiotherapy versus surgery alone for retroperitoneal sarcoma : a case - control , propensity score - matched analysis of a nationwide clinical oncology database . 
21 , 24105 kiel , deutschland ergebnis die daten von 9068 patienten wurden in die analyse eingeschlossen , davon 563 mit properativer radiotherapie , 2215 mit postoperativer radiotherapie und 6290 ohne radiotherapie . 
die 5 - jahres - berlebensrate wurde durch properative rt signikant verbessert von 54 % auf 62 % ( hr = 0 , 67 ; p < 0 , 0001 )  . 
die 5 - jahres - berlebensrate wurde durch die postoperative rt signikant verbessert von 52 % auf 60 % ( hr = 0 , 77 ; p < 0 , 0001 )  . 
die hazard - ratio ( hr ) fr berlebensverbesserung ( also die effektivitt der rt ) war an akademischen einrichtungen signikant niedriger ( besser ) als an nichtakademischen einrichtungen . schlussfolgerungen der autoren dies sei die grte analyse zur frage der strahlentherapie bei retroperitonealen sarkomen . 
diese daten wren wegweisend bis zum vorliegen der ergebnisse der eortc - studie . strahlenther onkol ( 2016 ) 192 : 820822 kommentar der positive effekt der radiotherapie im hinblick auf die lokale kontrolle ist bei weichteilsarkomen der extremitten seit mehr als 20 jahren unstrittig . 
man streitet lediglich ber die frage eines berlebensvorteils , der fr einen groen teil der patienten nicht erwartet werden kann wegen effektiver salvage - therapien , und ber die frage , welche nebenwirkungen fr die verbesserte lokale kontrolle in kauf genommen werden knnen . 
randomisierte studien gibt es bisher zwar nicht ( eine studie der eortc luft ) , aber die aktuellen retrospektiven daten und kohortenanalysen zeigen bereinstimmend eine verbesserte lokale kontrolle , zum teil mit einem berlebensvorteil [ 57 , 10 , 11 ]  . 
einen berlebensvorteil nachzuweisen , ist brigens auch wegen der heterogenitt der erkrankungen uerst schwierig . deutsche leitlinien der awmf gibt es nicht ; es existiert nur eine leitlinie fr pdiatrische weichteilsarkome , die aber seit jahren nicht aktualisiert wurde . 
die esmo guideline von 2012 stellt fr retroperitoneale sarkome fest , dass es keine ausreichenden daten fr eine properative therapie gibt ; mgliche optionen seien radiooder chemotherapie oder hyperthermie [ 4 ]  . 
empfohlen werden postoperative strahlendosen von 50 gy mit boostdosen von 1016 gy bei r0 , 1618 gy bei r1 und 2026 gy bei r2 . allerdings wird betont , dass die radiotherapie nur mit modernen techniken wie imrt , tomotherapie oder protonen durchgefhrt werden soll . 
die 2015 von der astro publizierten empfehlungen konkretisieren diese bewertungen speziell fr die properative radiotherapie [ 2 , 3 ]  . die hier referierte analyse liegt also im trend und unterstreicht die bedeutung der radiotherapie . 
zum vergleich : der unterschied zwischen radikaler resektion und r1 - resektion war in dieser untersuchung mit einem erhhten mortalittsrisiko assoziiert , das in etwa so hoch war wie der verzicht auf die strahlentherapie . 
in einer tumorkonferenz wird vermutlich immer eine r1 - resektion als ein extremes risiko betrachtet . der generelle verzicht auf rt birgt jedoch ( fr alle patienten ) ein ebenso groes risiko . 
das sollten wir deutlich machen . die arbeit wurde im selben heft , lancet oncology , durch frau baldini , einer radioonkologischen kollegin vom dana farber cancer institute in boston , kommentiert [ 1 ]  . 
sie sieht die eindeutige verbesserung der lokalen tumorkontrolle allein schon als ein argument fr die radiotherapie , selbst wenn ein berlebensgewinn in der summe der studien aus ihrer sicht aktuell noch fraglich ist . 
darber hinaus empehlt sie , solche patienten an ein high - volume - center zu berweisen . nach meiner einschtzung sind ihre in diesem kommentar ausgesprochenen empfehlungen eher zurckhaltend , vermutlich um die erst krzlich publizierten astro - empfehlungen ( baldini war erstautorin bei beiden publikationen ) nicht zu unterlaufen . fazit diese kohortenanalyse hat natrlich einschrnkungen , aber es ist die grte analyse und die beste aktuell verfgbare evidenz . 
und dass man die radiotherapie noch viel zu selten bercksichtigt , wird auch an den zahlen der national cancer data base deutlich : im auswertungszeitraum hatten nur 30 % der patienten eine radiotherapie erhalten . fr diejenigen , die sich mit derartigen fllen beschftigen , wird die lektre der astro - empfehlungen zur konturierung und technik empfohlen [ 2 , 3 ]  . jrgen dunst , kiel 822 literatur 1 . 
baldini eh , wang d , haas rl et al ( 2015 ) treatment guidelines for preoperative radiation therapy for retroperitoneal sarcoma : preliminary consensus of an international expert panel . 
gronchi a , lo vullo s , fiore m et al ( 2009 ) aggressive surgical policies in a retrospectively reviewed single - institution case series of retroperitoneal soft tissue sarcoma patients . 
gronchi a , miceli r , colombo c et al ( 2012 ) frontline extended surgery is associated with improved survival in retroperitoneal lowto intermediate - grade soft tissue sarcomas . 
nussbaum dp , rushing cn , lane wo et al ( 2016 ) preoperative or postoperative radiotherapy versus surgery alone for retroperitoneal sarcoma : a case - control , propensity score - matched analysis of a nationwide clinical oncology database . 
sampath s , hitchcock yj , shrieve dc , randall rl , schultheiss te , wong jy ( 2010 ) radiotherapy and extent of surgical resection in retroperitoneal soft - tissue sarcoma : multi - institutional analysis of 261 patients . 
frey1 received : 29 march 2016 / accepted : 15 june 2016 / published online : 11 july 2016 springer - verlag berlin heidelberg 2016 abstract background and purpose small animal irradiation systems were developed for preclinical evaluation of tumor therapy closely resembling the clinical situation . 
this study denes a protocol for conformal brain tumor irradiations in mice . materials and methods ct and mri images were used to demarcate the target volume and organs at risk . 
the in - house developed applicator was suitable for individual positioning at submillimeter accuracy of anesthetized mice during irradiation , altogether performed in less than 10 mall mice tolerated the treatment well . 
measured dose values perfectly matched the nominal values from treatment planning . cellular response was restricted to the target volume . conclusion clinical linac - based irradiations of mice offer the potential to treat orthotopic tumors conformably . 
especially with respect to lateral penumbra , dedicated small animal irradiation systems exceed the clinical linac solution . keywords mouse irradiation small eld dosimetry craniopharyngioma orthotopic xenograft neuartige bestrahlungsmethode fr stereotaktische hochprzisionsbestrahlung von maushirnen zusammenfassung hintergrund und zielsetzung kleintierbestrahlungsanlagen wurden entwickelt um prklinische studien in der tumortherapie unter mglichst klinischen bedingungen durchzufhren . 
die berechneten werte aus dem planungssystem stimmten mit den gemessenen dosiswerten berein und zeigten auf das zielvolumen begrenzte zellulre effekte . schlussfolgerung mittels klinischer linacs knnen orthotopische tumore von musen konform bestrahlt werden . 
as a consequence of these technical prerequisites and the broad availability of clinical linacs at most centers working with preclinical tumor models , all research questions not requiring the utmost precision achievable in dedicated small animal irradiation systems can be addressed with clinical linacs . 
however , reproducible treatment settings and positioning capabilities need to be prepared and optimized for small animals . therefore , the aim of this study is to dene a clinical standard protocol for sapbi to irradiate orthotopic brain tumors in mice while sparing of healthy tissue using a clinical linac . schlsselwrter mausbestrahlung kleinfelddosimetrie kraniopharyngiom orthotop xenograft mice materials and methods introduction small animal partial body irradiation ( sapbi ) advances in recent years more and more to the fore [ 13 ]  . 
the need for such treatment options is growing since orthotopic tumor models resembling the clinical situation for testing innovative radiation schemes , consecutive dna damage , systemic responses , and side effects are urgently needed , especially in times of multimodal therapies and are essential for preclinical research [ 46 ]  . 
special small animal irradiation systems , as the x - rad smart ( precision x - ray , north branford , connecticut , usa ) [ 7 ] , the small animal radiation research platform ( xstrahl , camberley , uk ) [ 8 ] , or the saigrt system [ 9 ] were developed and allow high - precision sapbi of very small target volumes . 
therefore , simpler irradiation settings and devices are still applied in most studies [ 10 , 11 ] , since most centers focusing on preclinical animal research do not have a sapbi installation available . 
in addition , small animal irradiation was mostly performed with industrial kv x - ray tubes [ 7 , 8 , 11 , 13 , 14 ] instead of clinical linear accelerators ( linac ) to minimize dose buildup rethe clinical standard protocol for sapbi was developed within the scope of a study based on the treatment of craniopharyngioma xenograft nmri - nu rj : nmri - foxn1nu / foxn1nu mice . 
this applicator was designed to position the mice consistently and to be compatible with the arccheck ( sun nuclear , melbourne , florida , usa ) for real - time dose verication measurements . 
d a 3d volume rendering of the located mouse inside the applicator , while e depicts an acquired mri slice with the segmented gross tumor volume ( gtv ) highlighted in green ing and irradiation . 
two oars were considered for treatment plan optimization : the muzzle should be blocked out completely and should receive only scattered radiation in order to avoid side effects on the skthe constraint of the eyes was done to avoid radiation - induced cataracts , inducing enhanced stress to the animals and falsifying future experiments . positioning and irradiation a therapeutic linac , novalis tx ( brainlab ag , feldkirchen , germany ) , was used for positioning and irradiation . 
this linac features a hd120 mlc ( varian , palo alto , california , usa ) with a leaf thickness of 0.25 cm in the central beam region and an exactrac v6.0.5 positioning system ( brainlab ag , feldkirchen , germany ) [ 18 ]  . 
after placing the anesthetized mouse without any xation in the applicator , the animal was prepositioned to the linac by the in - room laser systerened positioning based on stereoscopic kv x - ray images and matching of the head region to digitally reconstructed radiographs ( drr ) from the planning ct followed . 
irradiation followed immediately afterwards , while the mice were positioned under deep inhalation anesthesia , avoiding any further stress . treatment eld verication by radiation - induced dna damage targeted area was visualized based on immediate cellular radiation response . 
therefore , mice were sacriced 1 hour after receiving two fractions ( 3.6 gy , n = 1 ) , three fractions ( 5.4 gy , n = 2 ) , or nonfraction ( control mouse ; n = 1 ) and processed as described elsewhere [ 17 ]  . 
ultrathin sections of the parafn embedded murine brain were used for immunohistochemical staining utilizing the anti - h2a.x - phosphorylated ( s139 ) antibody ( 1 : 100 , clone 2f3 ; biolegend , san diego , california , usa ) indicating early radiation - induced dna damage and repair [ 19 ]  . 
staining was performed as described elsewhere [ 20 ] on coronal brain sections inside and outside the ptv . dosimetry to assess the dosimetric accuracy of the developed treatment approach , a number of measurements were performed in addition to the mouse irradiation . 
first , a pin point ionization chamber ( type : 23332 , ptw , freiburg , germany ) was used and positioned in place of the mouse inside the applicator . 
the mean dose within the ptv was used as reference dose of the tps . in addition , gafchromic ebt lms ( international specialty products , wayne , new jersey , usa ) were irradiated with the three treatment elds and with nine ( 4 cm ) elds of varying dose levels for a lm calibration . 
films were digitized using the lm scanner vxr - 16 dosimetrypro ( vidar systems corp . , herndon , virginia , usa ) and calibrated to dose [ 21 ]  . 
planar dose distributions ( pdds ) at the position of the three elds in 1.5 cm depth were determined with pinnacle3 for the lm evaluation . results treatment planning the dose distribution in fig . 
3 representative example of mouse positioning before irradiation : the left column shows an overlay of the x - ray image ( gray ) and the corresponding drr ( red ) after manual positioning using the in - room laser systethe column in the middle demonstrates an overlay of x - ray image ( gray ) and drr ( green ) after automatic positioning using the exactrac systethe right column shows the differences between the two drrs for manual and automatic positioning . 
the yellow arrow indicates an occurring mismatch after laser positioning and the corresponding correction with the exactrac system positioning an overlay of the stereoscopic x - ray images to the drrs after manual positioning of the mouse using the in - room laser system and after exactrac positioning are shown in fig . 
3. in addition , the accuracy and the reproducibility were signicantly enhanced with the exactrac - based positioning . overall , positioning and irradiation of a single mouse was practicable in less than 10 minutes . treatment eld verication by radiation - induced dna damage the proof of principle of the targeted irradiation of the murine brain tumor was veried by analyses of radiationinduced dna damage . 
the two sampled two - sided paired t - test was performed to evaluate the change in weight of the irradiated strahlenther onkol ( 2016 ) 192 : 806814 fig . 
4 immunohistochemical analysis of irradiation - induced early dna damage by detection of phosphorylated h2a.x ( s139 ) in coronal brain section : a negative staining control performed of the 3.6 gy irradiated mouse without using primary antibody , b xenograft craniopharyngioma within the planning target volume ( ptv ) of a nonirradiated reference mouse , c xenograft craniopharyngioma within the ptv of a mouse receiving two fractions of 1.8 gy and d cerebellum which is located outside the ptv of the same irradiated mouse . 
the qa0 eld , having also the smallest eld size , shows the smallest deviation between mean dose of the irradiated lm ( 48 cgy ) and the corresponding pdd ( 49 gy )  . 
the outcomes of the qa270 eld are 91 cgy for the irradiated lm and 86 cgy for the pdd , respectively . thus , the lm dose distributions , the calculated pdd , the dose values measured with the ionization chamber , and the mean dose values calculated with the tps are comparable and similar to each other . 
taking the uncertainties into account , the resulting values are even identical . discussion preclinical research on tumor therapy by radiochemotherapy , and in particular in combination with immunotherapy , is currently developing from ectopic to orthotopic xenograft and syngeneic models resembling closely a situation in tumor patients . 
even if the linac used in this study is meant for stereotactic treatments , the introduced protocol was designed to be applicable for each recent clinical linac with mlc thickness of less than 0.5 cone requirement of this protocol is an in - room imaging system for a precise positioning , which is a clinical standard for modern therapeutic machines . 
nevertheless , a major disadvantage of this approach is the nonconformal irradiation and missing of precise individual positioning , which has been solved by a dedicated applicator in this study . 
they used an industrial micro - ct and developed extensions with low effort and inexpensive in order to apply high - precision small animal treatment . imaging and irradiation were both performed by the x - ray tube . 
similar as in the presented study , they evaluated the resulting treatment elds with an ionization chamber and radiochromic lms in combination with solid water slabs , yielding comparable results . the use of kv photons for small animal irradiation was also supported by verhaegen et al . 
typical calculation models are unsuitable for treatment eld sizes smaller than 3 chowever , since the linac and the tps used in our study has been commissioned for patients treatments for minimum eld sizes of 1 cm side length , these small elds are predictable exactly and were applicable with a subsequent dosimetric verication . 
the conformity of the evaluated ionization chamber doses and the lm dose distributions to the calculated doses from the tps validated the feasibility of clinical tps application in the presented protocol . 
furthermore , planned dose distributions of the three individual elds were validated by lm measurements with uncertainties of less than 10 % , which is acceptable for lm dosimetry [ 24 ]  . 
thus , the design of the applicator was chosen to perform 3d online dosimetry with the arccheck but is currently not available for living small animals due to missing mouse monitoring during irradiation . treatment using the dened standard protocol was applicable for all mice , even if the treatment plan was based on one single mouse . 
the constant mouse weight and behavior is one indicator that the physiological condition was not degraded . a tumor conformal dose could be delivered as indicated in the immunohistochemically analyzed slices . 
further , only one medical physicist and one biologist are required to perform treatment planning , irradiation , and anesthesia . conclusion the in - house applicator was suitable for individual positioning and irradiation of mice . 
the big advantage of the presented methodology is the feasibility of a precise irradiation of preclinical mouse models at nearly all centers using stereotactic clinical linacs . acknowledgements the presented work was performed in partial fulllment of the requirements for obtaining the degree rer . 
the funders had no role in study design , data collection and analysis , decision to publish , or preparation of the manuscript . compliance with ethical guidelines conict of interest j . 
mai1 received : 25 january 2016 / accepted : 27 may 2016 / published online : 5 july 2016 springer - verlag berlin heidelberg 2016 abstract objective the gamma knife icon ( elekta ab , stockholm , sweden ) allows frameless stereotactic treatment using a combination of cone beam computer tomography ( cbct ) , a thermoplastic mask system , and an infrared - based highdenition motion management ( hdmm ) camera system for patient tracking during treatment . 
we report on the rst patient with meningioma at the left petrous bone treated with adaptive fractionated stereotactic radiotherapy ( a - gkfsrt )  . methods the rst patient treated with gamma knife icon at our institute received mr imaging for preplanning before treatment . 
furthermore , the icon system introduces a new online patient tracking system to the clinical routine . the interfractional accuracy of patient positioning was controlled with a thermoplastic mask and cbct . keywords radiosurgery adaptive fractionated stereotactic radiotherapy benign meningioma gamma knife patient tracking adaptierte fraktionierte stereotaktische strahlentherapie mit dem gamma knife bei meningeom mit cone - beam - ct und adaptiver replanung ( a - gkfsrt ) zusammenfassung einleitung das gamma knife icon ( elekta ab , stockholm , schweden ) ermglicht die stereotaktische behandlung von patienten mittels cone - beam - computertomographie ( cbct ) , thermoplastischer maske und infrarotbasierendem kamerasystem ( high denition motion managment , hdmm ) zur patientenberwachung whrend der bestrahlung . 
wir berichten ber die behandlung mit der adaptiven fraktionierten stereotaktischer radiotherapie ( a - gkfsrt ) bei einem ersten patienten mit einem meningeom im bereich des linken fersenbeines . methodik der erste patient , der mit dem gamma knife icon in unserem institut behandelt wurde , erhielt vor behandlung eine magnetresonanz ( mr - ) bildgebung zur vorplanung . 
das system adaptierte automatisch die geplanten positionen 816 strahlenther onkol ( 2016 ) 192 : 815819 der shots an die aktuelle situation und fhrte eine erneute dosisberechnung durch ( adaptive replanung in echtzeit )  . whrend der behandlung berwachte das hdmm - system die intrafraktionelle patientenbewegung . 
die bentigten zeiten wurden erfasst , um die klinische behandlungsdauer zu ermitteln . ergebnisse die komplette behandlungszeit betrug im mittel 20 mdabei dauerte die patientenpositionierung 0 , 8 min , cbct 1 , 65 min , verarbeitung der bilddaten und adaptive replanung 2 , 66 min und behandlung 15 , 6 min . die mittelwerte und standardabweichungen fr die 5 tglichen cbcts im vergleich zu den referenzdaten lagen bei 0 , 59 0 , 49 / 0 , 18 0 , 20 / 0 , 05 0 , 36 fr die rotation und 0 , 94 0 , 52 mm / 0 , 08 0 , 08 mm / 1 , 13 0 , 89 mm fr die translation . 
die ergebnisse des hdmm - systems fr alle fraktionen zeigten eine mittlere intrafraktionelle bewegung von 0 , 13 0 , 04 mm . schlussfolgerung das gamma knife icon kombiniert die stereotaktische genauigkeit des gamma - knife - systems mit der flexibilitt der fraktionierten behandlung mit maskensystem und cbct . 
die interfraktionelle genauigkeit der patientenposition wird durch thermoplastische masken und cbct ermglicht . schlsselwrter strahlenchirurgie adaptive fraktionierte stereotaktische radiotherapie gutartige meningiome gamma knife patientennachverfolgung meningiomas are tumors originating from arachnoid cells . most meningiomas are of benign nature ( who grade i ) and show slow progression without causing ( neurological ) symptoms . 
standard treatment is surgical resection or primary radiotherapy , with local control rates of up to 90 % after 5 years . in case of incomplete resection , recurrent , or a priori nonresectable tumors , radiotherapy is the treatment of choice . 
however , a treatment period of roughly 6 weeks for a benign tumor disease may pose a challenge for many patients . to date , only a few reports with small numbers of patients exist concerning hypofractionated radiotherapy of benign meningioma [ 46 ] , wherein single doses of 37 gy in 315 fractions have been reported . 
using these novel options , the gamma knife icon provides the possibility of adaptive fractionated stereotactic radiotherapy ( a - gkfsrt )  . the authors here report the rst case of a patient treated for petrous meningioma with this setup . case presentation patient details the current article reports on a 76 - year - old female patient who presented in the department with a meningioma who grade i located at the left petrous bone . 
the isodose lines represent the following doses ( outer to inner lines ) : 5 gy , 12 gy , 25 gy , and 50 gy treatment planning the patient rst underwent mri in 1 - mm resolution with an individual cushion but without mask for preplanning with the treatment planning system ( tps ) gammaplan 11.0.1 ( elekta ab ) 7 days before treatment . 
on the day of treatment , the patient received a planning ct scan ( brilliance big bore ; philips , amsterdam , netherlands ) with a gamma knifespecic thermoplastic mask to verify the actual situation and position of the tumor . both image datasets where coregistered and the preplanned treatment plan was adapted to the actual situation after head xation . 
before nishing the treatment planning process , a standalone cbct in high quality ( ct dose index , cdti : 6.3 mgy ) was acquired on the gamma knife icon to dene the stereotactic reference for the fractionated treatment . prior to each fraction , daily cbcts in low quality ( cdti : 2.5 mgy ) were performed to verify the actual skull position . 
the daily difference between the adapted and initial plan was analyzed and approved by a physician and a medical physicist . plan quality dose calculation was performed with the tmr10 algoriththe plan quality values for conformity , selectivity , gradient , and dose for target and brainstem are shown in table 1 . 
the largest translational deviation of 2.58 mm was seen in the longitudinal direction . the hdmm system continuously monitors , via exposure of infrared light to reecting markers on the patients nose , the movement of the nose tip and thus the intrafractional patient motion . 
g. , coverage , selectivity , and gradient for the delivered dose identical to the initial values of table 1 . outcome the total treatment time for fractions 25 was around 20 mthe positioning of the patient required 0.8 min , overall , the treatment was tolerated well . 
after the rst treatment session , the patient complained of a slight headache , which was treated with a short course of dextreatment strahlenther onkol ( 2016 ) 192 : 815819 fig . 
on days 2 and 3 , no intrafractional movement was detected day 1 day 2 day 3 day 4 day 5 00 : 00 05 : 00 15 : 00 20 : 00 10 : 00 minutes amethasone and resolved within 1 day . 
mai state that there are no conicts of interest . ethical standards all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . conclusion strahlenther onkol ( 2016 ) 192 : 102108 doi 10.1007 / s00066 - 015 - 0901 - 8 tomotherapy pet - guided dose escalation a dosimetric feasibility study for patients with malignant pleural mesothelioma angelo maggio claudia cutaia amalia di dia sara bresciani anna miranti matteo poli elena del mastro elisabetta garibaldi pietro gabriele michele stasi received : 4 may 2015 / accepted : 15 september 2015 / published online : 9 october 2015 springer - verlag berlin heidelberg 2015 abstract aim the aim of this study was to investigate whether a safe escalation of the dose to the pleural cavity and pet / ct - positive areas in patients with unresectable malignant pleural mesothelioma ( mpm ) is possible using helical tomotherapy ( ht )  . material and methods we selected 12 patients with mpm . 
in the first strategy ( standard treatment ) , treated comprised a prescribed median dose to the planning target volume ( ptv ) boost ( ptv1 ) of 64.5 gy ( range : 56 gy / 28 fractions to 66 gy / 30 fractions ) and 51 gy ( range : 50.4 gy / 28 fractions to 54 gy / 30 fractions ) to the pleura ptv ( ptv2 )  . 
dosevolume histogram ( dvh ) constraints and normal tissue complication probability ( ntcp ) calculations were used to evaluate the differences between the plans . results for all plans , the 95 % ptvs received at least 95 % of the prescribed dose . 
bei der ersten strategie ( standardbehandlung ) wurden die patienten im einem ptv - boost ( ptv1 , planungszielvolumen ) mit einer medianen dosis von 64 , 5 gy ( dosisbereich von 56 gy / 28 fraktionen bis 66 gy / 30 fraktionen ) und 51 gy im pleura - ptv ( ptv2 ) behandelt . 
danach wurden fr jeden patienten zwei dosiseskalationsplne mit der veroriginal article1 3 schreibung von 62 , 5 und 70 gy ( jeweils 2 , 5 und 2 , 8 gy / fraktion ) im ptv1 und 56 gy ( 2 , 24 gy / fraktion ) im ptv2 in 25 fraktionen generiert . 
dosis - volumen - histogramme und die wahrscheinlichkeit fr komplikationen am normalgewebe ( ntcp ) wurden verwendet , um unterschiede zwischen den plnen zu bewerten . ergebnisse alle plne der 95 % - ptv erzielten zumindest 95 % der verschriebenen dosis . 
bei allen patienten war es mglich , die dosiseskalation durchzufhren , ohne die toleranzdosisgrenzen fr risikoorgane ( oars ) nach quantec ( quantitative analysis of normal tissue effects in the clinic ) zu verletzen . 
bei allen plnen war das lungenvolumen stark mit den v20 - , v30 - , v40 - dosis - volumenhistogrammen ( dvh ; p < 0 , 0003 ) der lunge und mit der mittleren lungendosis ( p < 0 , 0001 ) korreliert . schlussfolgerungen die ergebnisse dieser studie zeigen , dass unter verwendung der ht die dosiseskalation bis mindestens 62 , 5 gy auf pet - positive flchen gefahrlos mglich ist , whrend die pleurahhle mit bis zu 56 gy in 25 fraktionen behandelt werden kann , ohne die dosis auf die umgebenden normalen organe bedeutsam zu erhhen . schlsselwrter helikale tomotherapie maligne pleuramesotheliome pet - bildgebung dosiseskalation berleben malignant pleural mesothelioma ( mpm ) is a rare and aggressive malignancy of the pleura related to asbestos exposure . 
the world health organization ( who ) has recognized asbestos as one of the most important occupational carcinogenic agents and in 2010 it upgraded its global estimate of asbestos - related diseases to 107 , 000 annual deaths [ 1 ]  . 
this disease has become an important health issue over recent years , especially in some parts of italy such as piedmont , which has one of the highest reported incidence rates in the world [ 2 ]  . 
although asbestos production in italy has been banned since 1992 , a peak of mpm - related deaths ( about 800 annual deaths ) is expected in the next few years owing to the latency period of the disease [ 2 ]  . the median survival is extremely poor ( less than 2 years ) [ 3 ] and there is no clear consensus on the optimal treatment ( surgery , chemotherapy , and / or radiotherapy ) of mpm . 
surgery alone [ 46 ] , aggressive combined approaches utilizing adjuvant chemotherapy , extrapleural pneumonectomy and radiation therapy ( trimodality therapy ) have been attempted [ 7 , 8 ]  . the role of radiotherapy ( rt ) and the optimal dose and timing of rt have not yet been established . 
the use of rt alone with curative intent for unresected disease is not recommended with traditional techniques , since target volumes typically exceed normal tissue tolerance limits ; a therapeutic dose of 60 gy to the pleura , delivered with a standard three - dimensional conformal rt ( 3dcrt ) technique , would expose more than 50 % of the ipsilateral lung volume to doses of > 20 gy [ 9 ]  . 
the radiosensitivity of human mesothelioma [ 13 ] would make it a good candidate for a positive response to radiation treatment but the limitation of doses to the adjacent organs at risk ( oar ) such as the heart , ipsilateral kidney , liver , lungs , oesophagus and / or spinal cord and the size and shape of the volume to be treated represent the main obstacle in delivering effective rt doses . 
therefore , intensity - modulated radiation therapy ( imrt ) combined with an image - guided system could be a valid instrument for achieving a better therapeutic ratio thanks to the possibility of escalating the tumour dose and tailoring the dose distribution around the target without increasing the risk of normal tissue toxicity to an unacceptable level . 
the aim of this study was to explore the possibility of using helical tomotherapy ( ht ) to safely escalate the dose to the pleural cavity and pet / ct - positive areas and to evaluate the possibility of obtaining lung dosevolume histogram ( dvh ) values from volumetric ct information for patients with unresectable pleural mesothelioma . because the size and the shape of the volumes to be treated and the close relationship with oars represent the main limitation to tumour dose escalation , normal tissue complication probability ( ntcp ) calculations were performed using the most recently available models so as to investigate whether substantial dose escalation is feasible without significantly increasing the risk of complications . material and methods between february 2012 and march 2014 , 12 consecutive patients with histologically confirmed mpm , who had been treated with ht ( hd , madison , wisc . ) in our department , were selected for this study . 
the group consisted of three tomotherapy pet - guided dose escalation1 3 104 female and nine male patients ; eight patients presented rightsided mpm and four patients left - sided mpm . 
all of the patients had not been previously irradiated and had presented after surgery and / or chemotherapy treatment with 18fdg - pet / ct - positive disease persistence / progression / relapse . 
all patients were immobilized in a supine position with their arms overhead on an arm shuttletm device ( q - fix , avondale , pa . ) during positron emission scan simulation performed with a philips gemini time of flight pet / ct unit ( the netherlands )  . 
the biological target volume ( btv ) , which included the uptake areas , was contoured based on the cooperation between the nuclear medicine physicians and the radiation oncologists without the application of a fixed threshold level . 
an isotropic margin of 5 mm was added to the ctv to obtain the ptv corresponding to the btv ( ptv1 ) and to the pleura ( ptv2 )  . 
moreover , in order to take into account the limited information provided by quantec [ 14 ] on this pathology for fatal pulmonary toxicity , the constraints for the v5 gy ( % ) , v10 gy ( % ) , and v20 gy ( % ) of the contralateral lung proposed by rice et al . 
in the first step ( standard treatment ) the 12 mpm patients were treated with a prescribed median dose of 64.5 gy ( range : 56 gy / 28 fractions to 66 gy / 30 fractions ) to ptv1 and 51 gy ( range : 50.4 gy / 28 fractions to 54 gy / 30 fractions ) to ptv2according to our internal protocols . 
thereafter , for each patient two dose escalation plans were generated prescribing 62.5 and 70 gy ( 2.5 / fraction and 2.8 gy / fraction , respectively ) to the ptv1 and simultaneously 56 gy ( 2.24 gy / fraction ) to the ptv2 , in 25 fractions . 
figure 1 shows the dose distributions and the dvhs of a patient with left - sided mpm for the standard treatment and for the dose escalation strategies . table 1 summarizes the ntcp and relevant dosimetric data for the oars considered , in 2 - gy equivalent doses . as shown in table 1 , the dose escalation to 18fdg - petpositive areas and the pleural cavity produced a significant increase of the dose to oars compared with the standard treatment . 
for all plans , the mean v5 gy ( % ) , v10 gy ( % ) and v20 gy ( % ) of the contralateral lung were below the dosimetric parameters for patients without fatal pulmonary toxicity [ 1517 ] ; only the mean v5 gy ( % ) for strategy ii and iii was slightly higher than the constraint proposed by patel et al . 
no correlation was observed between the lung sum volume and v20 , v30 and v40 ( r < 0.2 , p > 0.1 ) , discussion the surveillance of mesothelioma patients is still an important issue despite the ban on industrial asbestos use . 
2 correlation between ipsilateral / contralateral lung volume and lung a v20 gy ( % ) , b v30 gy ( % ) and c v40 gy ( % ) for all patients and strategies . 
the corresponding spearmans correlation ( r ) and p values are indicated ing into account the peak of mpm - related deaths expected in the next few years [ 2 ] and the extremely poor survival of mpm patients [ 19 ] , there is great interest in identifying treatment options capable of improving prognosis . 
the difference in clinical outcomes between patients randomly assigned to undergo extrapleural pneumonectomy ( epp ) or no epp was recently investigated in the mesothelioma and radical surgery ( mars ) multicentre randomized controlled trial [ 20 ]  . 
several studies evaluated the potential role of adjuvant rt in mpm [ 4 , 6 , 19 ] ; however , to date there has been limited reported experience in the feasibility of dose escalation with imrt for unresectable mpm [ 21 , 22 ]  . 
in our study , for the first time , we demonstrated from a dosimetric / radiobiological point of view the potential of ht to selectively increase the dose to high - risk areas detected by 18fdg - pet from 62.5 to 70 gy using an accelerated hypofractionated regimen in 25 fractions ; with a simultaneous integrated boost ( sib ) to the pleural cavity of 56 gy without significantly increasing the toxicity risk in the surrounding normal organs . 
 [ 24 ] showed that there was no improvement in local disease control when a low rt dose was delivered ( 30.6 gy to the ipsilateral hemithorax and mediastinum followed by a boost for a total of 50 gy )  . 
 [ 25 ] , in the sakk 17 / 04 study of 151 mesothelioma patients , reported that for the patients who received rt ( 46 gy to the hemithorax and mediastinal nodes and a 10 - gy boost for a total dose of 56 gy ) , the contribution of radiation did not improve time to recurrence of the disease . 
nccn guidelines reported that a dose of > 60 gy should be delivered to macroscopic residual tumours if it is possible to respect the tolerance doses to adjacent normal structures [ 26 ]  . 
the authors reported local recurrence in six ( 46 % ) patients , while nine ( 69 % ) patients were still alive at a median 9.5 months after completion of imrt [ 28 ]  . recently , fodor et al . 
 [ 22 ] highlighted the advantages of dose escalation in pet - positive volumes in an sib approach with ht comparing a group of 12 mpm patients treated with 56 gy / 25 fractions to the whole pleura with a second group of 12 patients treated with the same dose to the pleura plus a simultaneous boost of 62.5 gy to 18fdgpet / ct - positive areas . 
they observed a statistically significant difference in the median time to local relapse and the 1 - year local relapse - free rate and , even if not statistically significant , an improved overall survival and cancer - specific survival in favour of the dose escalation group . 
with conformational techniques , the main limitation to the dose escalation approach was the obvious negative impact of doses delivered to oars owing to the extent of the irradiated volume . 
it is important to highlight that in our study , using ht , it was always possible to maintain the average dose to the contralateral lung , which is the main limitation in dose escalation strategies , below 8 gy in 2 - gy equivalent doses . 
moreover , the analysis of the contralateral lung v5 gy ( % ) , v10 gy ( % ) and v20 gy ( % ) showed that it was possible to obtain dvh values below the dosimetric parameter for patients without fatal pulmonary toxicity as proposed in the literature [ 1517 ] , except for the mean v5 gy ( % ) for strategies ii and iii that was slightly higher than the constraint proposed by patel et al . 
recently , the ability to reduce the average contralateral dose below 8 gy using ht has been reported [ 22 , 29 ] , and no fatal rt - induced pneumonitis has been found as a result [ 22 ]  . 
moreover , although a statistically significant difference was found between some dosimetric parameters of standard treatment and dose escalation strategies , the quantec constraints for all oars were always satisfied . 
concerning the lung dose , an important challenge of this dose escalation approach could be the lack of knowledge of the side effects of the ipsilateral lung ( a part of it is included in the target volume ) , especially when high doses are delivered to pet / ct - positive areas . 
however , as reported in other works [ 4 , 20 ] , the lung toxicity was acceptable , although an increase in the sib group was observed , with three patients experiencing grade - 3 pneumonitis [ 22 ]  . 
interestingly , in our study we found a strong correlation between the lung v20 , v30 and v40 dvh values , the mean lung dose and the lung volume ratio ( ipsilateral / contralateral lung ) , derived from ct simulations . 
obtaining lung dvh values from patient - specific treatment simulation ct data may be a valid approach for better understanding , before planning preparation , the adequate patient - specific planning strategies associated with an acceptable lung dose . 
 however , owing to the limited number of patients treated , no correlation analysis between the dosimetric parameters and lung clinical toxicity was performed . conclusion the results of this study suggest that by using ht it is possible to perform a safe dose escalation delivering at least 62.5 gy to pet - positive areas using an accelerated hypofractionated regimen while applying an sib of 56 gy in 25 fractions to the pleural cavity without significantly increasing the toxicity risk in the surrounding normal organs . 
the results of our study point to the advantage of using rt techniques such as ht to minimize doses to oars while increasing the dose conformity to the tumour volume . 
when used in combination with an integrated image - guided technique that is able to correct for the geometrical uncertainties due to daily set - up variations , this approach may lead to new treatment options for patients with unresectable mpm . 
the results of this pre - clinical study support the initiation of a phase iii clinical trial including dose painting to ptv1of up to 70 gy in 25 fractions . acknowledgements this work was supported by tomo 25 mille 2009 ministero della salutefprc onlus . compliance with ethical guidelines conflict of interest a . 
stasi state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 8391 doi 10.1007 / s00066 - 015 - 0927 - y cone - beam ct - guided radiotherapy in the management of lung cancer diagnostic and therapeutic value khaled elsayad jan kriz gabriele reinartz sergiu scobioala iris ernst uwe haverkamp hans theodor eich received : 31 august 2015 / accepted : 18 november 2015 / published online : 2 december 2015 springer - verlag berlin heidelberg 2015 abstract background recent studies have demonstrated an increase in the necessity of adaptive planning over the course of lung cancer radiation therapy ( rt ) treatment . 
in this study , we evaluated intrathoracic changes detected by cone - beam ct ( cbct ) in lung cancer patients during rt . methods and materials a total of 71 lung cancer patients treated with fractionated cbct - guided rt were evaluated . 
in this study , the monitoring allowed for plan adaptations due to tumor volume changes and to other anatomical changes . keywords lung neoplasms intensity - modulated radiation therapy radiotherapy planning , computer - assisted radiotherapy , image - guided chemoradiotherapy cone - beam - ct - basierte strahlentherapie bei lungenkrebs diagnostischer und therapeutischer wert zusammenfassung hintergrund neuere studien haben eine zunehmende notwendigkeit der adaptiven bestrahlungsplanung im verlauf der bestrahlungsserie bei patienten mit lungenkrebs nachgewiesen . 
in der vorliegenden studie haben wir intrathorakale nderungen mittels cone - beam - ct ( cbct ) bei lungenkrebspatienten whrend der radiotherapie ( rt ) analysiert . methoden und materialien analysiert wurden 71 patienten , die eine fraktionierte cbct - basierte rt bei lungenkrebs erhalten haben . 
intrathorakale vernderungen und prioritt - scores fr die adaptive plananpassung ( ap ) wurden original article 84 zwischen kleinzelligem ( sclc : 13 patienten ) und nichtkleinzelligem bronchialkarzinom ( nsclc : 58 patienten ) verglichen . ergebnisse die mediane kumulative strahlendosis betrug 54 gy ( spanne 3072 gy ) , die mediane einzeldosis 1 , 8 gy ( spanne 1 , 83 , 0 gy )  . 
wir beobachteten intrathorakale nderungen in 83% der patienten im verlauf der rt [ 58 % ( 41 / 71 ) regression , 17 % ( 12 / 71 ) progression , 20 % ( 14 / 71 ) atelektase , 25 % ( 18 / 71 ) pleuraerguss , 13 % ( 9 / 71 ) infiltrative vernderungen und 10 % ( 7 / 71 ) anatomische verschiebung des tumors ]  . 
die visuelle volumenreduktion korrelierte mit der anzahl der erworbenen cbct - scans ( r = 0 , 313 ; p = 0 , 046 ) als auch mit dem zeitpunkt der verabreichung der chemotherapie ( r = 0 , 385 ; p = 0 , 013 )  . schlussfolgerung das wchentliche cbct - monitoring bietet einen adaptationsvorteil bei patienten mit lungenkrebs . 
in dieser studie hat das monitoring die adaptiven plananpassungen auf basis der tumorvolumenvernderungen intrathorakalen anatomischen versowie der anderen nderungen ermglicht . schlsselwrter lungenneoplasien intensittsmodulierte strahlentherapie computerassistierte strahlentherapieplanung bildgesttzte strahlentherapie radiochemotherapie lung cancer causes more deaths worldwide than any other form of cancer and is the second most common type of cancer in both males and females [ 1 , 2 ]  . 
non - small cell lung cancer ( nsclc ) is the most common subtype of lung cancer , accounting for 84 % of all lung cancers [ 1 ]  . 
according to the recent guidelines , inoperable patients should be treated with concurrent chemoradiation therapy ( crt ) if possible to maximize survival , local control , and response rate [ 3 ]  . 
for patients who cannot tolerate crt , radiation therapy ( rt ) alone or sequential rt - chemotherapy can also provide a survival benefit [ 3 , 4 ]  . 
novel treatment approaches , such as adaptive radiotherapy ( art ) , respiratory motion management , image guidance , intensity - modulated radiation technique ( imrt ) simultaneous integrated boost , and incorporation of pet data in the treatment planning process , have emerged in recent years [ 711 ]  . modern technological developments , such as intrafraction imaging acquisition with cone - beam ct ( cbct ) , enable more accurate delivery ( prevention of set - up errors ) and verification of radiation doses [ 1214 ]  . 
in addition , adaptive planning may help optimize rt courses given that tumor volume shrinkage is highly variable over the radiation period and across patients [ 12 , 13 , 1526 ]  . 
other soft tissue changes that can occur following rt , such as atelectasis , pleural effusion , and pneumonia / pneumonitis , should also being monitored in adaptive planning protocols [ 13 , 18 , 20 , 27 ]  . in this study , we conducted a retrospective review of cases in which cbct was used to determine the volumetric changes and we evaluated the importance of image guidance in detecting intrathoracic anatomical changes in lung cancer patients over the rt period . materials and methods patient selection we reviewed the medical records of 117 lung cancer patients treated with rt in a varian truebeam linear accelerator at our institution between july 2013 and january 2015 . 
 the remaining 46 patients had been treated with stereotactic rt and were excluded from further analysis due to minimal volumetric changes and an absence of necessity for adaptation [ 27 ]  . 
the patients clinical characteristics and rt course details , including total radiation dose , daily fraction , and use of daily on - board imaging , were obtained from their medical records , electronic charts , and planning software ( varian medical systems , the eclipse treatment planning system , version 10 )  . 
the planning target volumes ( ptvs ) , gross target volumes ( gtvs ) , and intrafraction anatomic changes in each cbct scan were evaluated retrospectively and scored . treatment planning cts ( pcts ) were performed with intravenous contrast approximately 7 days ( range 136 days ) before starting rt . 
additional 4d - ct ( n = 2 ) or 4d - pet - ct ( n = 23 ) scans were performed on 25 patients for tumor delineation and to quantify respiratory motion . 
gtvs were delineated in the midventilation phase and expanded to a ptv with a safety margin of 510 mall 71 patients received imrt ; 53 patients ( 75 % ) also received chemotherapy ( 39 % concurrent , 30 % sequential , and 6 % both regimens )  . 
ptv , cm sclc small cell lung cancer , nsclc non - small cell lung cancer , scc squamous cell carcinoma , rul right upper lobe , rll right lower lobe , lul left upper lobe , lll left lower lobe , med . 
median , pct planning ct , rt radiotherapy , gtv gross target volume , ptv planning target volume only 6 / 71 patients ( 8.5 % ) were irradiated postoperatively ( table 1 )  . 
an ap score of 1 ( very high ) indicated the urgent administration of a new pct before rt delivery due to possible effects on dosimetric distribution ( due to gtv dislocation outside ptv or due to tumor progression )  . 
a priority score 2 ( high priority ) was interpreted as meaning that although a radiation dose could be delivered and gtv is still inside ptv , a new pct needed to be performed within 1 week ( due to marked volumetric or intrathoracic soft tissue changes )  . 
a priority score of 3 ( intermediate priority ) indicated that rt could be delivered and that there was ample time to adapt the radiation plan ( a new pct for boost rt planning is usually required after delivery of 40 gy , if marked gtv changes are observed )  . 
a priority score of 4 ( low priority ) indicated that radiation could be delivered and that no actions were required until rt was completed , if no gtv or soft tissue changes are observed in radiation fields . 
in case boost planning was performed , the dose distribution of the primary treatment was matched with the current computed tomography and total dose distribution ( primary and boost ) was calculated . in total , 2 , 038 fractions were delivered to the 71 patients in this study cohort ( median , 30 fractions / patient ; range 540 fractions / patient ) and 535 kilovoltage - cbct scans were performed ( median 6 scans / patient , range 125 scans / patient )  . statistical analysis mean changes are reported with standard deviations ( sds )  . 
 the a initial planning ct ( pct ) and b first cbct , 9 days after the pct , showed atelectasis that resulted in a tumor shift outside of the planning target volume ( ptv ) , resulting in an ap score of 1 . 
d cbct 3 days later showing resolution of the atelectatic changes , which required second adaptive plan ( ap score 2 ) toured in pcts in 43 / 71 cases ( 60.6 % ) ; in the remainder of the cases ( 28 / 71 ; 39.4 % ) , the gtvs could not be differentiated from the mediastinum , chest wall , or soft tissue changes in pcts or cbcts . 
b cbct in week 4 of rt showing development of atelectasis ( outside the radiation field ) without a tumor shic cbct in week 5 of rt showing resolution of atelectasis . 
of the 37 nsclc patients who required plan changes , 24 ( 64.8 % ) had only one adaptation , 10 ( 27 % ) had two adaptations , 2 ( 5 % ) had three adaptations , and 1 ( 3 % ) had four adaptations . 
in addition , ptv modifications were indicated due to marked anatomical changes in 30 / 71 cases ( 42.3 % ) , including 13 / 71 cases ( 18 % ) with pleural effusion , 11 cases ( 15 % ) with atelectasis , and 6 cases ( 8 % ) with infiltrative changes . treatment response treatment response was analyzed in the 42 patients for whom gtvs could be followed with delineation in cbcts . 
in addition , 15 / 42 patients ( 35.7 % ) maintained a stable gross volume ( 035 % gtv reduction ) and 5 / 42 patients ( 11.9 % ) experienced marginal progression ( range 322 % )  . examination of the histological records revealed that the patients in the sclc group experienced a marked gtv reduction , ranging from 23 to 83 % ( mean 46 % ; median 36 % )  . 
the number of volumetric changes observed differed significantly between patients at different cancer stages ( p = 0.047 ) , with more changes occurring in patients with stages iii and iv disease than in early stage patients . more advanced tumor progression showed a very - near significant trend toward correlating with a higher ap score ( r = 0.231 , p = 0.052 ) , as well as a trend toward correlating k . 
these changes were seen most frequently in weeks 4 ( n = 2 ) and 5 ( n = 2 )  . discussion the present work extends the limited literature of retrospective investigations of cancer treatment adaptation necessity due to intrathoracic anatomical [ 13 , 18 , 20 ] or volumetric changes [ 13 , 14 , 17 , 1921 , 2325 ]  . 
 [ 26 ] concluded that adaptive planning ( in week 3 week 5 ) significantly reduces the mean lung dose ( 58 % ) and allows for dose escalation , which may improve the therapeutic ratio and tumor control probability [ 11 , 28 ]  . 
 other researchers have observed tumor volume regression in 3035 % of treated lung cancer patients and progression in 1230 % of treated patients , usually in the first week of treatment [ 13 , 14 , 17 , 24 ]  . 
the higher regression rate in our study ( 58 % ) could be due to the longer treatment periods of our patients ( median , 30 fractions ) relative to those described by kwint et al . 
 ( 82 % received < 24 fractions , [ 13 ] )  . we observed median gtv reductions of 31 and 51 % after 3 and 5 weeks of rt , respectively . 
marked regression during rt for nonadenocarcinoma tumors has been associated with a higher probability of recurrence and a trend toward poorer survival [ 21 , 30 ] , suggesting that such patients should receive dose escalation . 
 [ 31 ] recommended a novel treatment planning technique , which incorporates a tumor regression model that allows dose escalation without increasing toxicity . regarding other anatomical changes , moller et al . 
 [ 18 ] concluded that only 23 % of patients receiving rt show lung density changes , with only 12 % requiring plan adaptations due to geometric shifts and / or dosimetric changes . 
 unlike some prior studies [ 13 , 18 ] , the most common reason for adaptation in our study was pleural effusion ( 18 % ) , followed by atelectasis ( 15 % ) and infiltrative pulmonary changes ( 8 % )  . 
 our findings of most intrathoracic changes ( 74 % ) occurring within the first 3 weeks of rt and of 45 % of patients showing one anatomical change , 22.5 % showing two , and 15.5 % showing three or more changes are consistent with data in literature [ 13 ]  . this study bears the limitation of being relatively small , although the findings are consistent with other publications [ 13 , 18 ]  . 
in addition , it should be noted that the accuracy of cbct monitoring may be diminished for lesions that are associated with lung atelectasis or located in the mediastinum [ 14 ]  . 
more clinical and biological data are needed to identify patients who may require plan modification during radiotherapy . conclusion a large majority of lung cancer patients in this study ( 83 % ; 68 % having tumor volume changes and 41 % having other intrathoracic changes ) exhibited soft tissue changes over the course of rt . 
moreover , in 25 % of the patients , the radiation oncologist needed to perform a new pct for adaptation with urgency . compliance with ethical guidelines conflict of interest k . 
eich state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . cone - beam ct - guided radiotherapy in the management of lung cancer1 3 90 strahlenther onkol ( 2016 ) 192 : 127129 doi 10.1007 / s00066 - 015 - 0932 - 1 akzelerierte teilbrustbestrahlung mit interstitieller multikatheter - brachytherapie eine valide therapieoption fr mammakarzinompatientinnen mit niedrigem risikoprofil ? david krug online publiziert : 5 . 
zum einsatz kam sie bisher vor allem zur boost - applikation im rahmen der brusterhaltenden therapie ( bet ) des mammakarzinoms oder fr rebestrahlungen bei in - brust - rezidiven . 
in der hier kommentierten studie ging esumdiefrage , obeineteilbrustbestrahlung ( pbrt ) mit hilfe der mk - brt bei patientinnen mit einem mammakarzinomniedrigenrisikoprofilsdieganzbrustbestrahlung ( wbrt ) ersetzenkann . material und methode in der randomisierten phase - iiistudiedergec - estro - gruppe wurden von 2004 bis 2009 1184 patientinnen mit einem mammakarzinom niedrigen risikoprofilsodereinemdcisnachbrusterhaltenderoperationentwedereinerteilbrustbestrahlungmitmk - brtoder einerperkutanenwbrtderoperiertenbrustmitanschlieendem boost des tumorbetts zugefhrt . 
einschlusskriteoriginalpublikation strnad v , ott oj , hildebrandt g et al ( 2015 ) 5 - yearresultsofacceleratedpartialbreastirradiation usingsoleinterstitialmulticatheterbrachytherapyversuswholebreastirradiationwithboostafterbreast - conservingsurgeryfor low - riskinvasiveandin - situcarcinomaofthefemalebreast : a randomised , phase3 , non - inferioritytrial.lancet [ epubaheadof print ] med . 
es handelte sich um eine nichtunterlegenheitsstudie ; die schwelle wurde hier bei einerdifferenzvon3%inbezugaufdielokalrezidivrate , diegleichzeitigdenprimrenendpunktdarstellte , angelegt . diedatenwurdennachdertatschlicherhaltenentherapie ( perprotocoloderastreated ) ausgewertetundprsentiert.dasmedianefollow - uplagbei6 , 6jahren . ergebnisse insgesamt handelte es sich bei den patientinnen um ein niedrig - risiko - kollektiv . 
mglicherweise lassen sich hier aber mit hilfe der imrt bessere kosmetischeergebnisseerzielen ; erstedatenzureffektivittundtoxizittwurdenkrzlichausitalienpubliziert [ 5 ]  . etwasinvergessenheitgeratenwarwhrenddessen , dass mit der mk - brt eine seit langem bewhrte und vielseitige technik zur verfgung steht , fr die im vergleich zu denanderengenanntenverfahrenderteilbrustbestrahlung die grte kumulative erfahrung vorliegt . 
vor allem die ungarischerandomisiertephase - iii - studiezeigtemiteinem follow - upvon10jahrenvergleichbareergebnissederteilbrustbestrahlungmithilfedermk - brt ( nureineminderheit der frauen hatte eine perkutane teilbrustbestrahlung mit elektronen ) und der perkutanen wbrt mit 56% lokalrezidiven und gleichzeitig besserem kosmetischem outcomeimbrachytherapie - arm [ 6 ] .dieerfahrungenmit derteilbrustbestrahlungbeidcissindhingegenunabhngig von der eingesetztentechnik gering und beschrnken sichaktuellaufmonozentrische , retrospektiveserien [ 7 ]  . anlass zur kritik an der gec - estro - arbeit gibt es kaudie studie wurde kritisch und verantwortungsvoll geplant und sorgfltig durchgefhrt . 
insbesondere werden auch die statistischen hintergrnde in der appendix ausfhrlichdargestellt.nichtsdestotrotzsollteandieserstelle aufdielimitationenundbesonderheitenvonnichtunterlegenheitsstudienverwiesenwerden [ 8 , 9 ] .wegendeswechselsaufgrundindividuellerpatientenwnschezwischenden beiden behandlungsarmen werden die daten als per - protocol - analyseprsentiert.imanhangfindetsichallerdings auch eine intention - to - treat - auswertung , die ebenfalls die nichtunterlegenheitbelegt.aufgrunddergeringenanzahl an rezidiven ist eine detaillierte multivariate subgruppenauswertungaktuellnichtmglich . fazit die mk - brt ist bei entsprechender patientenselektion und sorgfltiger planung und durchfhrung eine ernstzunehmende therapiealternative fr patientinnen mit mammakarzinomenniedrigenrisikoprofils.einneuerstandard wird durch die hier vorgestellte gec - estro allerdings wohlnichtdefiniert.beachtetwerdensolltenaberauchhier dasweiterefollow - upsowiedieangekndigtenauswertungen zu kosmetik , lebensqualitt und toxizitt . 
brigens belegendieindergec - estro - studieprsentiertenrezidivraten nach adjuvanter ganzbrustbestrahlung mit boost [ 10 ] gemeinsam mit den ergebnissen aus den standardarmen anderer prospektiv randomisierter studien der letzten jahre eindrucksvoll , dass sich die 5 - jahres - lokalrezidivrate heutzutage bei entsprechender patientenselektion im bereichvon < 2%bewegtunddamitdiemesslattefrjede nderungderklinischenpraxishochliegt . david krug , heidelberg d . 
veronesi u , orecchia r , maisonneuve p et al ( 2013 ) intraoperative radiotherapy versus external radiotherapy for early breast cancer ( eliot ) : arandomisedcontrolledequivalencetrial.lancet oncol14 : 12691277 4 . 
elective nodal irradiation ( eni )  . methods treatment planning was performed for 41 patients with la - nsclc , using four different planning approaches ( 3d - crt - if , 3d - crt - eni , imrt - if , imrt - eni )  . 
rbe , md , phd department of radiotherapy and radiation oncology , saarland university medical school , 66421 homburg / saar , germany e - mail : jochen.fleckenstein@uks.eu conclusion the imrt technique and if target volume delineation allow a significant dose escalation and an increase in tcp . 
imrt results in an improved sparing of oars as compared with 3d - crt at equivalent dose levels . keywords non - small cell lung carcinoma intensitymodulated radiation therapy conformal radiotherapy positron emission tomography organs at risk imrt und 3 - d - konformale radiotherapie mit oder ohne elektive nodalbestrahlung bei lokal fortgeschrittenem nichtkleinzelligem bronchialkarzinom direkter vergleich der pet - basierten therapieplanung zusammenfassung zielsetzung das potenzial der intensittsmodulierten strahlentherapie ( imrt ) soll im rahmen der fdg - pet basierten bestrahlungsplanung des lokal fortgeschrittenen nichtkleinzelligen bronchialkarzinoms ( la - nsclc ) fr 2 zielvolumenanstze ( involved - field - bestrahlung , if ) sowie elektive nodalbestrahlung ( eni ) geprft und mit der 3 - d - konformalen strahlentherapie ( 3 - d - crt ) als referenz verglichen werden . material und methoden die bestrahlungsplanung erfolgte an ct - datenstzen von 41 patienten mit la - nsclc in 4 anstzen ( 3 - d - crt - if , 3 - d - crt - eni , imrt - if , imrteni ) jeweils mit 2 gy einzeldosis . 
die imrt ermglicht auerdem eine signifikant geringere normalgewebsbelastung im vergleich zur 3 - d - crt bei quivalenten gesamtdosen . schlsselwrter nichtkleinzelliges bronchialkarzinom intensittsmodulierte strahlentherapie konformale radiotherapie positronenemissionstomographie risikoorgane three more or less parallel developments changed the therapeutic scenario in locally advanced non - small cell lung cancer ( la - nsclc ) during the past 15 years : the advent of intensity - modulated radiotherapy ( imrt ) , the integration of fluorodeoxyglucose positron emission tomography ( fdgpet ) into treatment planning , and the shift to involved - field radiotherapy ( if - rt )  . induced by the ongoing technical evolution of linear accelerators , imrt became a standard treatment technique in various indications such as prostate cancer , head and neck cancer , and primary brain tumors . 
treating moving targets with imrtas is the case with radiotherapy of nsclcwas initially considered with caution mainly because of the dosimetric relevance of the interplay effect [ 3 ]  . 
in the meantime , reassuring dosimetric and clinical data have been published , demonstrating the safe and effective use of imrt in patients with la - nsclc [ 4 , 5 ]  . the concept of if - rt evolved at the same time as fdgpet - based treatment planning became a standard for lansclc . 
if - rt can be safely applied in combination with fdg - pet - based target volume definition [ 610 ]  . the aim of the present planning study was to validate the assumed superiority of imrt in direct comparison with 3d - crt with respect to both the achievable total dose for each technique [ and the potential of dose escalation in terms of calculated tumor control probability ( tcp ) ] and the sparing of organs at risk ( oar ) regarded at equal maximum prescription doses ( pd )  . 
also , by using a two - by - two planning approach , imrt and 3d - crt plans were established for two alternative concepts of target volume delineation , i.e. , the addition of elective nodal irradiation ( eni ) vs . 
the detailed inclusion criteria and conditions for the acquisition of computed tomography ( ct ) and fdg - pet images ( with identical patient positioning ) are provided in a previous publication [ 10 ]  . 
for lymph nodes , all mediastinal and / or hilar lymph node stations as classified by the american joint committee on cancer were delineated according to the guidelines published by chapet et al . 
ctvs of elective nodal stations had to be fdg - pet negative and contained the ipsilateral hilum , the infracarinal lymph node station , all lymph node stations adjacent to any fdg - pet - positive station , and all ct - positive lymph node stations ( in case of lymph nodes of > 1.5 cm in the short axis )  . 
identical prerequisites were defined for 3d - crt and imrt plans based on prespecified dose constraintswhole lung : v20 35 % ; mean lung dose < 20 gy ; heart : v45 < 67 % ; v60 < 33 % ; spinal cord : 45 gy as maximum ; esophagus : v50 < 50 % and / or v60 < 33 % and / or mean esophageal dose < 34 gy ; 70 gy as maximum ( mandatory )  . 
in the eni arm the pd was 50 gy for the ptv including elective nodal stations followed by a boost , which was escalated until oar dose limits were reached . 
in the same way , pd was escalated in the if - rt arfor both volumes , total pd was capped at 110 gy if oar constraints were not reached beforehand ; all plans were calculated with single doses of 2 gy and escalated or deescalated by 2 - gy increments . for 3d - crt planning , at least three beams had to be used and the number and arrangement of beams and their weights , the use of wedges , as well as the photon energy ( 6 and 18 mv ) were optimized by an experienced medical physicist . imrt step - and shoot plans ( photon energy : 6 mv ) were calculated using direct machine parameter optimization . 
 inverse planning was started with a default pd of 70 gy , and standardized objectives for the coverage of the ptv as provided by icru report 83 were applied [ 16 ]  . 
to allow for potential dose escalation , predefined lower oar constraints were used as default values for the initial 70 - gy planwhole lung : v20 < 28 % ; heart : v40 < 20 % ; spinal cord : maximum dose of 40 gy ; esophagus : v50 < 50 % and maximum dose of 70 gy . 
therefore , imrt plans were additionally normalized to the same maximum dose level ( defined as total reference dose , dref ) as it was reached with 3d - crt plans in the corresponding study arm ( adapted doses are labeled as imrtnorm )  . based on the relative seriality model as described by kllman et al . 
 [ 19 ] and implemented in pinnacle3 , normal tissue complication probability ( ntcp ) values were calculated for the whole lung ( endpoint : pneumonitis grade 1 ; d50 : 26 gy ; / = 3 ) , the esophagus ( endpoint : stricture ; d50 : 68 gy ; / = 3 ) , the heart ( endpoint : pericarditis ; d50 : 49 gy / = 3 ) , and the spinal cord ( endpoint : myelitis ; d50 : 68 , 6 gy ; / = 3 )  . 
as the dose constraints used for the presented study imply a low risk of normal tissue toxicity , 3d - crt dose levels were normalized to the ( higher ) dref of the imrt plans ( indicated as 3d - crtnorm ) to enable a meaningful ntcp comparison . statistical analysis in the case of normal distribution , a paired sample t test was used to test for statistical differences between data sets , otherwise the wilcoxon signed rank test was applied . 
a if - rt planning with treatment volume : fdg - pet - based gtv of the primary tumor ( orange line on ct ) and ptv with inclusion of station 5 ( red , colorwash ) .with imrt planning ( second row ) administration of a total dose of 78 gy would be possible vs . 
this holds true for the majority of the analyzed parameters in the if - rt and the eni arimrt was superior to 3d - crt in sparing the spinal cord ( dmax ) and limiting the high - dose exposure of the esophagus ( v60 )  . 
a significant reduction of the mld and v20 of the lung by using imrt could only be demonstrated in the eni approach , whereas the impact seemed to vanish with the lower treatment volumes in if - rt . 
when 3d - crt plans were normalized ( 3d - crtnorm , as presented in table 4 ) to the dref that was reached with imrt , i.e. , escalated in most cases , the effect on ntcp values was detrimental as compared with imrt and the difference in ntcp of the lung and esophagus was largest in the eni arm . discussion can be ascribed to the superior dose conformality of imrt resulting in improved sparing of oar . 
the advantages of imrt were more pronounced with eni : 39 of 41 patients could be administered a dref of at least 2 gy more as compared with 3d - crt , whereas in the if - rt arm a dose escalation was feasible in 32 of 41 patients with imrt vs . 
the upper boundary of a total dose of 110 gy was reached with an if - rt / imrtplan in a single patient exhibiting a peripheral nsclc without lymph node involvement . 
in eni constraints for the whole lung ( mld , v20 ) most often prohibited a higher dref ( with imrt in 32 , and with 3d - crt in 31 of 41 patients ) , whereas in the if - rt arm the esophagus ( with imrt in 24 cases ) and the spinal cord ( with 3d - crt in 19 cases ) became more relevant . 
as shown in table 2 , tcp values increased both with the use of imrt and with if - rt . the present planning study gives strong support to two ongoing major shifts in radiotherapy of la - nsclc : first , the increasing use of imrt and second , the abandonment of irradiating elective nodal stations in the context of fdg - petbased target volume definition . 
 it may matter even more that a dose of 60 gy ( considered as curative by the standard of care ) could not be achieved in 15 of 41 analyzed patients with eni planned with 3d - crt andby contrastin 39 of these patients the administration of a dose of 66 gy or more was possible with if - rt when combined with imrt . 
our data also imply that even if imrt with if - rt planning was not exploited for the purpose of dose escalation ( in regard to the conflicting results of the rtog 0617 trial [ 20 ] ) it should lead to a significant reduction of normal tissue toxicity . 
interestingly , we found that imrt is of greater benefit in sparing the spinal cord and esophaimrt and 3d conformal radiotherapy with or without elective nodal irradiation1 3 80 table 2 3d - crt vs . 
in a dosimetric analysis by shi et al . , lung v10 and ntcp values were predictive of severe acute radiation pneumonitis whereas lung v5 was not [ 21 ]  . the role of imrt in la - nsclc has previously been investigated in three similar planning studies , which also favored the use of imrt over 3d - crt [ 2224 ]  . 
clinical evidence for the use of if - rt is derived from one randomized clinical trial [ 26 ] and several single - arm trials [ 7 , 8 , 10 , 27 ]  . 
regarding imrt in la - nsclc , the evidence for its role is weaker in comparison with that of if - rt because of limited clinical data [ 28 ]  . 
reported clinical results for the safe and effective use of imrt in combination with image - guided radiotherapy ( igrt ) in a retrospective analysis , which was superior to 3d - crt with respect to overall survival and toxicity [ 5 ]  . 
yet , it remains to be seen if the higher conformality of imrt plans may have a detrimental effect to the control of microscopic disease in out - of - field lymph node stations an issue which should be monitored in future trials . it remains speculative if the results of the present study , which were generated with a step - and - shoot imrt approach , would also apply for volumetric - modulated arc therapy ( vmat )  . 
two studies comparing imrt and vmat for la - nsclc did not reveal relevant differences between the two techniques with respect to dose coverage of the ptv or lung exposure [ 31 , 32 ]  . in practice , a significant proportion of patients with lansclc should benefit from the use of imrt . 
especially patients who could otherwise not be treated with a curative dose should not be withheld the option of imrt . conclusion if combined , fdg - pet - based if - rt and imrt allow for a significant dose escalation as compared with eni in combination with 3d - crt . 
rbe state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 118126 doi 10.1007 / s00066 - 015 - 0925 - 0 scanned ion beam therapy for prostate carcinoma comparison of single plan treatment and daily plan - adapted treatment sebastian hild christian graeff antoni rucinski klemens zink gregor habl marco durante klaus herfarth christoph bert received : 20 august 2015 / accepted : 11 november 2015 / published online : 27 november 2015 springer - verlag berlin heidelberg 2015 abstract background and purpose intensity - modulated particle therapy ( impt ) for tumors showing interfraction motion is a topic of current research . 
the purpose of this work is to compare three treatment strategies for impt to determine potential advantages and disadvantages of ion prostate cancer therapy . materials and methods simulations for three treatment strategies , conventional one - plan radiotherapy ( convrt ) , image - guided radiotherapy ( igrt ) , and online adaptive radiotherapy ( art ) were performed employing a dataset of 10 prostate cancer patients with six ct scans taken at one week intervals . 
d. faculty of physics , technische universitt darmstadt , darmstadt , germany original article1 3 conclusion impt of prostate cancer demands consideration of rectal sparing and adaptive treatment replanning for patients exhibiting large prostate motion . keywords intensity - modulated radiotherapy radiotherapy planning , computer - assisted prostatic neoplasm organs at risk image - guided radiotherapy gescannte ionenstrahltherapie beim prostatakarzinom vergleich konventioneller und tagesaktueller bestrahlungsplanung zusammenfassung hintergrund und ziel adaptive therapieanstze fr sich interfraktionell bewegende zielvolumina in der intensittsmodulierten partikeltherapie ( impt ) befinden sich zurzeit in der entwicklung . 
in dieser arbeit werden drei behandlungsstrategien auf mgliche vorund nachteile in der impt des prostatakarzinoms hin untersucht . material und methoden auf basis eines anonymisierten datensatzes aus 10 patienten mit prostatakarzinom wurden die drei bestrahlungsstrategien , konventionelle ein - planstrahlentherapie ( convrt ) , bilduntersttzte strahlentherapie ( igrt ) und tagesaktuelle strahlentherapie ( adaptive radiotherapy , art ) , simuliert . 
 die ergebnisse der planungsstudie , die geometrische und patientenspezifische definitionen der zielvolumina in der impt vergleicht , wurden anhand der zieldosis und der dosisbelastung von rektum , hftkpfen und blase beurteilt . ergebnisse fr patienten mit kleiner prostatabewegung ( mittelwert < 4 mm ) fhrten alle untersuchten behandlungsstrategien zu einer klinisch akzeptablen dosis im zielvolumen ; igrt und art konnten die rektumdosis signifikant senken . 
bei 20% der patienten berstieg die prostatabewegung 4 m dies fhrte zu unzureichender dosisabdeckung des zielvolumens fr convrt ( v95mean = 0 , 86 ; spanne 0 , 630 , 99 ) und igrt ( v95mean = 0 , 91 ; spanne 1 , 000 , 68 ) , whrend art die volle zieldosis erreichte . schlussfolgerung schonung des rektums ist eine der wichtigsten gesichtspunkte in der impt des prostatakarzinoms . 
fr patienten mit groer prostatabewegung sollten zustzlich wirksame adaptive strahlentherapieanstze , wie beispielsweise eine tgliche neuplanung , gewhlt werden , um die abdeckung des zielvolumens zu gewhrleisten . schlsselwrter intensittsmodulierte strahlentherapie computerassisitierte strahlentherapieplanung prostataneoplasie risikoorgane bildgesttzte strahlentherapie in clinical practice , radiation therapy is often planned only once based on the planning computed tomography ( ct ) scan acquired days before the actual treatment delivery . 
daily setup uncertainties and internal organ motions are generally compensated by safety margins which , especially in the case of prostate cancer , partially overlap with surrounding critical structures [ 1 ]  . 
an increasing complication rate in critical organs , in particular the anterior rectal wall and the base of the bladder , limits the maximum target dose [ 4 , 5 ]  . 
for the bladder as well as the rectum , high volume effects have been reported [ 6 ] ; hence , one objective of radiation therapy in the treatment of prostate cancer should be minimization of the irradiated volume of these structures . intensity - modulated particle therapy ( impt ) has been successfully used to treat prostate cancer since 1994 at the national institute of radiological science ( nirs ) in chiba , japan [ 7 ] and since 2006 at the gsi helmholzzentrum fr schwerionenforschung in germany [ 8 ]  . 
currently , a randomized phase ii study for ion prostate irradiation ( ipi ) is underway at the heidelberg ion - beam therapy center ( hit ) in germany [ 6 , 9 ]  . 
the rationale for considering pt in prostate cancer treatment is the characteristic depth dose profile of particles , which can provide a therapeutic high dose to a deep - seated target like the prostate , while reducing the integral out - of - target dose in comparison to photon treatment [ 10 ]  . 
a growing interest in hypofractionation for prostate / parameters cancer , supported by a differential in tissue ( low for the prostate , high for rectum and bladder as organs at risk ( oars ) , [ 11 ] ) , makes precise dose deposition within one fraction even more important . 
however , large daily variations in prostate position [ 1214 ] require generous margins which cause considerable volumes of the aforementioned oars to be included in the planning target volume ( ptv )  . image - guided radiotherapy ( igrt ) aims to reduce geometrical uncertainties by acquiring additional image data shortly before or during radiation delivery featuring various plan adaptation possibilities [ 1 , 8 , 1519 ]  . 
a more suitable adaptation strategy to adequately deal with changes in tumor size and shape could be online planning , based on image data in the treatment position acquired immediately before delivering each fraction using a predefined setup [ 20 ]  . 
to quantify the potential advantages of patientspecific treatment adaptation in impt for prostate cancer , we compared online adaptive radiotherapy ( art , [ 20 ] ) with igrt ( i.e. , using patient specific margins [ 16 ] ) and convenscanned ion beam therapy for prostate carcinoma1 3 120 table 1 summary of all combination possibilities for one patient ( six single ct scans ) for the three treatment approaches planning target volumes number of optimized treatment plans 20 ptvs 6 cts = 120 plans forward dose calculation planning ct only online art 20 geoptvs per ct convrt number of simulated fraction doses 120 plans 1 ct = 120 fractions all fraction cts , excluding the planning ct 120 plans 5 cts = 600 fractions igrt 56 itvs one plan per itv = 56 plans all fraction cts , excluding all cts used to create itv fractions ! ! = 156 nct ( here = 6 ) total number of patient cts , art online adaptive radiotherapy , convrt conventional one - plan radiotherapy , igrt image - guided radiotherapy , ptv planning target volume , itv internal target volume , ct computed tomography table 2 prostate volume and displacement from its mean position ( center of mass )  . 
also the mean 3d displacement vector length with sd is given patient ctv mean ( 1 sd ) [ cm3 ] 3d mean ( 1 sd ) [ mm ] approved by a radiation oncologist . 
in patients 2 and 6 , the analysis of the prostates center of mass displacement with respect to its mean position had a maximum > 4 mm ( 3d vector length ) , which will further be referred to as large motion . 
they were originally treated with photons at the german cancer research center ( dkfz ) in heidelberg , germany where the cts were acquired weekly on the in - room ct on rails scanner siemens emotions [ 21 ]  . 
in this study , three treatment strategies for impt , ( 1 ) a conventional one - plan strategy , ( 2 ) an image - guided strategy , and ( 3 ) an online planning strategy , were simulated . 
details are outlined in table 1 . dataset the clinical target volume ( ctv ) , prostate without seminal vesicles , and the critical organs ( bladder , rectum , and femoral heads ) were delineated on each ct separately and margin concepts / ptv definition the ptvs which have been employed in the simulations of convrt and online art were generated by adding a geometrical margin to the ctv . 
to account for the sensitivity of particle therapy to changes of the radiological path length in the entrance channel , we further generated water equivalent path length ( wepl - ) itvs as described by graeff et al . 
 the smallest ptv322 ( + 3 mm lr , + 2 mm si , ap ) of all cts was transferred into water equivalent geometry , where either 2 , 3 , 4 , or 5 ptvs were combined to form an internal target volume ( itv )  . 
from water equivalent geometry , they were transformed back into patient geometry ; hence , they incorporate a range margin sufficient for all datasets which were included in the construction process . 
ptvs and itvs will further be referred to by indices indicating the geometrical margins and the number of scans used to compose the itv , respectively . treatment planning assuming random prostate motion [ 14 ] , we used the individual cts without temporal correlation . 
the carbon treatment plans with a general were optimized according to the parameters used in the ipi study [ 6 , 9 ] : single fraction dose of 3.3 gy ( rbe ) ; two lateral opposing fields . 
the dose was recalculated with a pencil beam algorithm , which includes a model for multiple coulomb scattering [ 28 ] , using our in - house planning software trip4d [ 20 , 25 , 26 ]  . 
there were no optimization constraints given for critical organs . data analysis the simulations were analyzed using dosevolume histogram constraints , namely the target volume receiving at least 95 % of the desired dose ( v95 ) , as well as v63 and v60 for bladder and rectum , respectively [ 6 , 9 ]  . 
significance between convrt and the adaptive strategies was assessed by a wilcoxon signed rank test . results ptv volumes the itv shape and volume is determined by the target motion characteristic such that it naturally is a patient and field - specific target volume . 
assuming no or only minor changes in patient geometry between imaging and treatment delivery [ 12 , 20 ] , online art improved the target coverage significantly compared to all other simulations to 0.99. 
3 whisker plots showing the results of clinical target volume ( ctv ) coverage and organs at risk ( oar ) exposure in patients exhibiting small or large prostate motion . 
due to smaller margins , art ( ptv322 ) reduced the rectal v90mean by more than 50 % . discussion our simulations demonstrate the general problem of prostate irradiation with a target conformal irradiation technique also outlined by various other groups : interfraction prostate motion is random and shows large interpatient variability [ 18 , 24 ]  . 
it is a reasonable approach throughout the literature to group patients according to the extent of their internal organ motion [ 13 , 18 ]  . in the simulations for the patient subgroup showing small daily prostate shifts ( 80 % of our dataset ) , a patient - specific target volume definition with the igrt approach improves target coverage and reduces the dose to bladder and rectum significantly when including four or more datasets . 
 the absorbable gel is injected between the prostate and the anterior rectal wall [ 31 ] and establishes a stable gap of 710 mm between the two structures over the entire course of treatment [ 6 ]  . 
investigations on effects of gel applications on the prostate motion itself were beyond the scope of this work . the simulations for the patient subgroup showing large daily prostate shifts yielded insufficient target dose coverage when using geometrical or range margins . 
to meet clinical standards in target coverage and rectal exposure , these patients would have to be replanned on a daily basis as , in terms of target coverage , online art was the only strategy that ensured clinically requested v95 levels of > 0.95 for patients with large motion . 
the online art strategy using ptv755 showed rectal exposure comparable to convrt ( ptv455 ; p = 0.52 and p = 0.93 for v60 in rectum and v63 in bladder , respectively ) which could be scanned ion beam therapy for prostate carcinoma1 3 124 fig . 
 [ 12 ] reported prostate shifts to be smaller than 3 mm in the first 20 min after initial imaging for 90 % of the patients with empty rectuaccording to van herk et al . 
nevertheless due to intrafraction organ motion and target volume delineation inaccuracies , a margin around the ctv will always remain necessary [ 1 ]  . the increase of the clinical workload with daily replanning is high and the two main associated aspectstight integration of hardand software and rapid quality assurancehave not been addressed yet [ 1 ]  . 
however , recent developments in our laboratory suggest that plan optimization for carbon ion therapy can be completed from a computational standpoint in approximately 6 min [ 20 ] , which supports that online planning might be feasible in the near future . given the problem of a considerable number of patients showing large internal organ motion , a possible clinical approach keeping the additional work load at a minimum could be rectal preparation via balloons , enemas , antigas medication , laxatives , etc . , which has the potential to reduce large prostate motion [ 32 , 33 ] , followed by pretreatment imaging [ 8 , 34 ]  . 
in that case , the treatment strategy could be tailored for individual patients motion characteristic , possibly supported by automated simulation software and backed up by using more robust therapy approaches like brachytherapy [ 3537 ] or external beam radiation therapy with photons , in extreme cases . as described by georg et al . 
 [ 39 ] the results , however , are expected to improve slightly , i.e. , potential / parameters are likely to reduce the dose to changes in rectum , bladder , and femoral heads . 
the qualitative findings reported in this study are not expected to change when considering the foreseeable changes in / parameters . conclusion particle therapy for prostate tumors that show considerable interfraction motion requires additional clinical effort as it demands frequent imaging and sometimes replanning . 
 the lack of tight integration of imaging units and treatment planning units as well as the tremendous increase in workload currently makes it difficult to integrate online art into a clinical environment . acknowledgments this study was funded by the german research foundation ( dfg ) , clinical research group ( kfo ) 214 . 
bert state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . strahlenther onkol ( 2016 ) 192 : 109117 doi 10.1007 / s00066 - 015 - 0919 - y image - guided intensity - modulated radiotherapy of prostate cancer analysis of interfractional errors and acute toxicity volker rudat a . 
this article is published with open access at springerlink.com abstract purpose the aim of the study was to estimate interfractional deviations in patient and prostate position , the impact of the frequency of online verification on the treatment margins , and to assess acute radiation reactions of high - dose external beam image - guided intensity - modulated radiotherapy ( ig - imrt ) of localized prostate cancer . patients and methods ig - imrt was performed by daily online verification of implanted fiducial prostate markers using a megavoltage electronic portal imaging device ( epid )  . 
acute radiation reactions were assessed weekly during radiotherapy using the common terminology criteria for adverse events ( ctcae ) v.4.03. results a relevant combined patient set - up and prostate motion population random error of 45 mm was observed . 
no grade 3 or 4 acute radiation reactions were observed with daily ig - imrt . conclusion a high dose with surprisingly low acute toxicity can be applied with daily ig - imrt using implanted fiducial prostate markers . 
mohammed department of radiation oncology , saad specialist hospital , 31952 al khobar , saudi arabia e - mail : volker.rudat@gmail.com superior to image guidance every other fraction concerning adequate target coverage with minimal margins . keywords prostate neoplasms image - guided radiotherapy intensity - modulated radiotherapy planning target volume fiducial markers bildgesteuerte intensittsmodulierte strahlentherapie des prostatakarzinoms analyse interfraktioneller abweichungen und akutreaktionen zusammenfassung ziel ziel der studie war es , die interfraktionelle variabilitt der patientenlagerung und prostataposition , den einfluss der bildgebungsfrequenz und die akuten strahlenreaktionen bei einer hochdosierten bildgesteuerten intensittsmodulierten strahlentherapie ( ig - imrt ) des prostatakarzinoms zu untersuchen . methoden ig - imrt wurde durch tgliche verifikation von implantierten rntgendichten prostatamarkern mittels megavolt - bildgebung ( electronic portal imaging device , epid ) und anschlieender patientenrepositionierung vor strahlentherapie erreicht . 
bei der ig - imrt mit tglicher bildgebung wurden in der vorliegenden studie keine grad - 3oder grad - 4 - akutreaktionen beobachtet . schlussfolgerung bei einer ig - imrt mit tglicher verifikation von prostatamarkern kann eine hohe dosis mit berraschend geringer akuttoxizitt appliziert werden . 
im hinblick auf adquate tumorerfassung mit geringstmglichen sicherheitssumen ist die tgliche igrt einer igrt bei jeder zweiten bestrahlungsfraktion deutlich berlegen . schlsselwrter prostataneoplasien bildgesteuerte strahlentherapie intensittsmodulierte strahlentherapie planungszielvolumen rntgendichte marker several meta - analyses have shown that higher doses of radiotherapy improve the biochemical relapse - free survival of patients with organ - confined prostate cancer compared to those treated with conventional - dose radiotherapy [ 7 , 22 ]  . 
in order to keep the risk of acute and late radiation toxicity as low as possible , the radiotherapeutic high - dose region should be as small as possible . early studies revealed a relevant prostate motion variability [ 20 ] , evaluated the patient set - up variability without image guidance [ 15 ] , and estimated the treatment margins for the combined error of both factors [ 17 ]  . 
image - guided radiotherapy ( igrt ) and reverse planned intensity - modulated radiotherapy ( imrt ) are current radiation techniques commonly used to minimize the high - dose region without compromising tumor coverage for the definitive radiotherapy of localized prostate cancer . 
igrt reduces the highdose volume by minimizing the required internal margin ( im ) and set - up margin ( sm ) , thereby , downsizing the planning target volume ( ptv )  . 
imrt reduces the high - dose volume by generating a dose distribution more conformal to the ptv compared to conventional three - dimensional conformal radiotherapy ( 3dcrt )  . in this study , igrt was achieved with daily online verification of implanted fiducial prostate markers using an electronic portal imaging device ( epid )  . 
the goal of the study was to assess prostate motion variability and patient set - up variability , and to estimate the safety margin to accommodate for the combined error of both factors . 
acute radiation reactions were assessed weekly during radiotherapy to evaluate the tolerance to high radiation doses applied using daily ig - imrt . patients and methods patient data and preparation for treatment planning a total of 23 consecutive , unselected patients receiving definitive radiotherapy for localized prostate cancer between december 2013 and march 2015 were analyzed . 
 after an interval of 3 days , the patients underwent a computed tomography ( ct ) scan and magnetic resonance imaging ( mri ) in the supine position for radiotherapy planning . 
the slice thickness was 2 mfive sequences ( axial t1w , axial t2w , coronal t2 stir , axial t1fs ) were obtained before and three sequences ( axial , sagittal , and coronal t1fs ) after the application of contrast media . 
the mri and ct images were electronically fused using the autoregister method of the syngo - based coherence oncologist workspace version 2.0.52 ( siemens healthcare , erlangen , germany )  . 
mri images were used for the target volume definition in particular because the apex of the prostate can be better visualized using mri compared to ct [ 13 , 23 ]  . 
for ct simulation and radiotherapy , patients were immobilized in supine position using a headrest , kneefix , and feetfix ( civco medical solutions , coralville , ia , usa )  . 
the images were zoomed and electronically superposed with the reference images , the corresponding digitally reconstructed radiographs ( drr ) generated by the treatment planning system ( tps )  . 
online correction of deviation of the fiducial prostate markers was done by automatic adjustment of the treatment table in three dimensions prior to every radiotherapy application in all patients . inverse - planned intensity - modulated radiotherapy the target volumes were defined and the dose prescribed according to the international commission on radiation units and measurement ( icru ) reports 50 and 62 recommendations . 
the contouring of the ptv and organs at risk was done according to the rtog consensus contouring guidelines male pelvis normal tissue and other specific recommendations [ 13 , 23 ]  . 
d calculated deviation of the compared structures of images a and b image - guided intensity - modulated radiotherapy of prostate cancer1 3 112 patient with very high risk , the ctv included the prostate , the complete seminal vesicals , and the locoregional pelvic lymph nodes . 
 the number of segments of a typical plan was around 100 and the corresponding treatment time about 15 mlinear accelerators ( oncor avant garde , siemens medical , erlangen , germany ) equipped with a multileaf collimator ( 160 leaves ) and an epid ( optivue , siemens medical , erlangen germany ) were used for the treatment . assessment of acute radiation reactions acute radiation reactions were prospectively assessed by two radiation oncologists using the common terminology criteria for adverse events ( ctcae ) v.4.03. 
the acute reactions were assessed once weekly during the course of radiotherapy and 6 weeks after radiotherapy . statistical analysis individual and population based parameters of the patient set - up variability were calculated according to the report on target : ensuring geometric accuracy in radiotherapy by the royal college of radiologists [ 14 ]  . 
the patient set - up parameters were calculated for each direction ( longitudinal , vertical , and lateral )  . image - guided correction of the patient set - up and prostate motion error was performed prior to every radiotherapy fraction in all patients . 
in order to estimate the margins required for image guidance every other radiotherapy fraction or no image guidance during radiotherapy , the patient set - up and prostate motion error before correction of the corresponding radiotherapy fractions was used for the statistical analysis . 
 accordingly , the margin required to ensure 95 % minimum dose to the ptv for 90 % of the patients was given by m ptv 2 50 1 64 1 64 where s is the square root of the quadratic sum of the standard deviations of all contributing systematic errors , s the square root of the quadratic sum of the standard deviations of all contributing random errors , and p the standard deviation describing the width of the penumbra . 
the patient set - up variability , prostate motion variability , and the combined error of both factors ( referred to as combined error ) were slightly different in the three dimensions . 
 most probably due to differences in the bladder and rectum filling [ 20 , 21 ] and respiration [ 4 ] the prostate motion variability was greater in the longitudinal and vertical direction than in the lateral direction . 
the patient set - up variability , prostate motion variability , and the required safety margin to accommodate for the combined error in dependence of the frequency of the image guidance are listed in table 2 . 
in order to save cost in terms of increased dose and in - room time [ 9 ] , the question arises whether the frequency of image guidance can be reduced from daily to every other day without losing relevant benefit . our data show that the combined patient set - up and prostate motion error on average remains basically constant over the course of radiotherapy . 
the impact of the random error on the ctvptv margin can be significantly reduced by daily online verification of the prostate position with necessary corrections applied before delivery of treatment . 
according to the van herk formula , reducing the frequency of image - guided fractions to every other fraction would require an expansion of the ctvptv margin of 48 mthis additional margin would increase the ptv by approximately 3040 % in a typical prostate cancer patient . 
it is likely that an increase of the ptv of this magnitude will significantly increase the risk of toxicity at the high radiation doses prescribed . similar results have been reported by kupelian et al . 
in agreement with our study , imaged guidance every other day compared to daily image guidance would have increased the ctvptv margin by 47 mm using the van herk formula . 
the authors concluded that high - dose external beam radiotherapy for localized prostate cancer delivered with tight treatment margins requires daily image guidance . image - guided intensity - modulated radiotherapy of prostate cancer1 3 114 fig . 
 [ 19 ] reported about 141 patients with localized prostate cancer treated with igimrt to a total dose of 76 gy ( n = 13 ) and 80 gy ( n = 128 )  . 
 [ 25 ] assessed the acute radiation toxicity of patients treated to 78 gy with either igimrt ( n = 260 ) or 3d - crt ( n = 215 ) using toxicity questionnaires distributed at baseline , prior to fraction 20 and 30 , and at 90 days after treatment . 
 for grade 2 and higher acute gastrointestinal / genitourinary ( gi / gu ) toxicity , both univariate and multivariate analyses showed a statistically significant decrease in grade 2 and higher acute collective gi / gu toxicity for imrt . 
 [ 6 ] analyzed 150 prostate cancer patients treated with dose - escalated , moderately hypofractionated cone - beam ct based ig - imrt with a simultaneous integrated boost ( sib ) technique . 
the rate of gu toxicity grade 2 or higher was less than 10 % at 612 months but increased continuously to 22.4 % at 60 months ; grade 3 gu toxicity remained below 5 % during follow - up . 
mohammed state that there are no conflicts of interests . table 3 maximal acute radiation reactions [ common terminology criteria for adverse events ( ctcae ) v.4.03 ] parameter dermatitis radiation grade all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
a more sophisticated approach to minimize the ptv and to optimize the dose distribution would be adaptive radiotherapy where an adaption of the dose open access this article is distributed under the terms of the creative commons attribution license which permits any use , distribution , and reproduction in any medium , provided the original author ( s ) and the source are credited . strahlenther onkol ( 2016 ) 192 : 92101 doi 10.1007 / s00066 - 015 - 0929 - 9 lipiodol versus diaphragm in 4d - cbct - guided stereotactic radiotherapy of hepatocellular carcinomas mark k . 
tung hollis luk oliver blanck received : 1 august 2015 / accepted : 20 november 2015 / published online : 3 december 2015 springer - verlag berlin heidelberg 2015 abstract purpose the purpose of this work was to investigate the potential of lipiodol as a direct tumor surrogate alternative to the diaphragm surrogate on four - dimensional cone - beam computed tomography ( 4d - cbct ) image guidance for stereotactic radiotherapy of hepatocellular carcinomas . methods a total of 29 hepatocellular carcinomas ( hcc ) patients treated by stereotactic radiotherapy following transarterial chemoembolization ( tace ) with homogeneous or partial defective lipiodol retention were included . 
resulting lipiodol / diaphragm motion ranges and position errors relative to the reconstructed midventilation images were analyzed to obtain the motion variations , and group mean ( m ) , systematic ( ) , and random ( ) errors of the treatment setup . results of the lipiodolized tumors , 55 % qualified for direct localization on the 4d - cbct . 
m and obtained with lipiodol and diaphragm were similar , agreed to within 0.5 mm in the lr and ap , and 0.3 mm in the cc directions , and differed by 1.4 ( lr ) , 1.1 ( cc ) , and 0.6 ( ap ) mvariations of diaphragm motion range > 5 mm were not observed with lipiodol and in one patient with diaphragthe margin required for the tumor prediction error using the diaphragm surrogate was 6.7 ( lr ) , 11.7 ( cc ) , and 4.1 ( ap ) mm . conclusion image - guidance combining lipiodol with 4dcbct enabled accurate localization of hcc and thus margin reduction . 
a major limitation was the degraded lipiodol contrast on 4d - cbct . keywords image - guided radiotherapy 4d cone beam ct stereotactic body radiotherapy contrast media planning techniques lipiodol versus zwerchfell in 4d - cbct - gefhrter stereotaktischer strahlentherapie bei hepatozellulren karzinomen zusammenfassung hintergrund ziel dieser studie war es , das potential von lipiodol als direktes tumorsurrogat alternativ zum zwerchfellsurrogat fr die vierdimensionale cone - beamcomputertomographie ( 4d - cbct ) in der stereotaktischen strahlentherapie von hepatozellulren karzinomen ( hcc ) zu analysieren . methoden eingeschlossen wurden 29 hcc - patienten , die mittels stereotaktischer strahlentherapie nach transarterieller chemoembolisation ( tace ) mit homogener oder teilweise defekter lipiodolspeicherung behandelt wurden . 
zwerchfellbewegungen und positionsfehler relativ zu den rekonstruierten midpbildern ( midv , midventilation images ) wurden analysiert , um vernderungen in den bewegungen , gruppen ( m ) , systematische ( ) und zufllige ( ) fehler in der patientenlagerung sowie notwendige sicherheitssume ( m ) beurteilen zu knnen . ergebnisse fr die direkte lokalisierung auf den 4dcbct waren 55 % der tumoren mit lipiodol geeignet . 
der notwendige sicherheitssaum , um den tumorvorhersagefehler fr das alleinige zwerchfellsurrogat auszugleichen , betrug 6 , 7 mm ( lr ) , 11 , 1 mm ( cc ) und 4 , 1 mm ( ap )  . schlussfolgerung bildregistrierungsprotokolle mit lipiodol in kombination mit 4d - cbct ermglichen die genaue lokalisierung von hcc und somit die signifikante reduktion von sicherheitssumen . 
haupteinschrnkungen dieser technik sind bereits abgebaute lipiodolanreicherungen auf dem 4d - cbct . schlsselwrter bildgefhrte strahlentherapie 4d - cone - beam - computertomographie stereotaktische krperbestrahlung kontrastmittel planungstechnik at our institute , the image - guidance solution is based on linac - integrated four - dimensional ( 4d ) - cbct , which technically is similar to the 4d - ct in the way that the cbct images are reconstructed at different positions along the respiratory cycle [ 5 ]  . 
the advantage of targeting the tumor at its time time - weighted average position has been discussed extensively in the literature [ 5 , 6 ] , being able to minimize the systematic errors from tumor motion . 
the major application of 4d - cbct so far has been focusing on treatments of lung tumors [ 7 , 8 ] , and experience in applying it to hcc are relatively limited [ 9 , 10 ] notably owing to the poor tumor contrast . 
because of the lobe dependence of tumor motion in the liver [ 11 , 12 ] , population statistics about the interand intrafractional liver motion and position provided by case et al . 
 [ 9 , 10 ] were of limited applicability in terms of formulating the safety margin . in this study , we aimed to ( 1 ) investigate the potential of lipiodol for direct target localization on 4d - cbct , ( 2 ) assess the uncertainties of interfractional treatment setup , interfractional tumor baseline , and motion amplitude estimated by the lipiodol and the diaphragm using 4d - cbct , and ( 3 ) provide an assessment of the margin required for diaphragm / lipiodol - guided treatment setup . methods and materials patients and treatment image - guidance ( ig ) is impeccable for hypofractionated / stereotactic body radiotherapy ( sbrt ) of hepatocellular carcinomas ( hcc ) to achieve safety margin reduction and hence minimization of radiation to normal tissues . 
because the tumor contrast with surrounding tissue is often too low for direct target localization during treatment , surrogates such as implanted metal markers or diaphragm / liver contour are used , in some situations demanding considerable margin to account for the uncertainty in the correlation between the surrogate and the tumor [ 1 ]  . for patients who had prior transcatheter arterial chemoembolization with lipiodol ( tace ) in combined treatment therapy , the retention of intense tumor stain due to selective uptake of lipiodol by tumor cells that generally remains for several weeks [ 2 ] can serve as a natural contrast medium for direct image - guided tumor targeting [ 3 , 4 ]  . a total of 29 patients with single primary nonresectable hcc were enrolled in this retrospective analysis approved by the institutional review board . 
the prescription dose was individualized to either 4 gy for 610 fractions or 69 gy for 6 fractions at 7787 % prescription isodose lines relative to the maximum dose by a risk - adaptive approach . lipiodol versus diaphragm in 4d - cbct - guided stereotactic radiotherapy of hepatocellular carcinomas1 3 94 immobilization , 4d - ct simulation , and treatment planning immobilization of the patients was achieved by a vaclok cushion ( medtec , orange city , ia , usa )  . 
for each patient , 3 mm slice thickness 4d - ct images were acquired in helical mode on a philips brilliance big bore 16 - slice ct scanner ( philips medical systems , cleveland , oh , usa ) and phase - sorted into ten bins of equal time share of the respiratory cycle . 
 based on the lipiodol contrast on the 4d ct scan , the tumor trajectory and motion range was estimated for the three cardinal directions : x , y and z corresponding to the leftright ( lr ) , craniocaudal ( cc ) , and anteroposterior ( ap ) directions , respectively . 
next , the time - weighted mean tumor position ( midp ) and its corresponding time - percentage were calculated as described in our previous study [ 13 ] , and 1 of the initial 10 4d - ct phases that was closest to this midventilation ( midv ) time percentage was selected for tumor delineation , treatment planning , and as the reference images for image guidance . 
we assumed that tumor delineation and 4d - ct / cbct registration each contributed to error of 1 mfurthermore , the statistics about intrafractional baseline drift was adapted from case et al . 
the xvi software implemented a feature - based algorithm to extract the respiratory trace for sorting the projections into ten bins according to the respiratory phase , thus , removing the need of external respiratory monitoring . 
after the cbct acquisition , a bone registration was first performed by a user - defined 3d region - of - interest ( roi ) placed around the vertebrae in the midv reference ct , yielding three rotational and three translational errors . 
 next , a 3d roi so - called mask expanded from the planning contour of either the gtv ( lipiodol - based ) or the liver ( diaphragm - based ) was automatically registered to each phase of a 4d - cbct scan by local rigid registrations . 
this step resulted in an estimated target trajectory relative to the reference ct and a displacement of the time - weighted mean position ( midp ) that was used for couch correction . 
at this point , the registration was visually inspected , and the necessary adjustment was made by a single expert oncologist to avoid interobserver variability . all patients were treated by the strategy described above as planning and treating the tumor at midp , which has been shown to facilitate margin reduction compared to the use of internal target volume ( itv ; [ 6 ] )  . 
prior to each delivery , we further ensured that the motion range in each direction estimated with the lipiodol / diaphragm mask on the 4d - cbct was no larger than that estimated on the planning 4d - ct by 3 mm , which required roughly an additional 2 mm margin for motion range of 110 mm [ 7 , 15 ]  . quantitative assessment of the lipiodol / diaphragm position on 4d - cbct data only lipiodol retention that was classified as homogeneous accumulation and partial defect [ 16 ] in both the simulation 4d - ct and treatment verification 4d - cbct scans was considered as an acceptable surrogate for inclusion in the analysis . 
the interfractional changes of absolute tumor position ( i.e. , treatment setup ) were analyzed separately for ig correction protocols using the centroid positions of the lipiodol and liver contours at midp . 
 the interfractional change of absolute lipiodol / diaphragm position was obtained from the result of 4d registration of each scan as the difference of lipiodol / diaphragm at midp on the 4d - cbct compared with the lipiodol at midv on the m . 
statistical significance was considered with p - value < 0.05. impact of lipiodol for target localization and motion estimation results lipiodol was hypothesized to provide the reference treatment setup in our online correction protocol . 
because the motion of liver tumors is lobe dependent , we measured the distance from the tumor to the diaphragm ( d ) to understand its relationship with ex y z  . 
the norm of the mean tumor prediction error ex y z 1 / 3 / 5 mm was evaluated for the whole patient group to understand the spectrum of variability and the percentage of cases that would have required a margin of approximately 1 / 5 / 10 mm if the diaphragm had been otherwise used for target localization . quantitative assessment of the lipiodol / diaphragm motion range on 4d - cbct the motion range in each direction obtained from the planning 4d - ct was compared with that of the treatment 4d - cbct for the lipiodol and diaphragthe motion difference between the 4d - ct and the 4d - cbct with the lipiodol / diaphragm that was 3 / 5 mm was evaluated over all scans of each patient . statistical analysis the patient mean ( ) and standard deviation ( sd ) of the interfractional changes of absolute lipiodol / diaphragm position were calculated over all 4d - cbct scans , and from averaging the individual patient means , the group means ( m ) were calculated . 
population statistics were also obtained for the tumor prediction error e for estimating the margin with the diaphragm - based correction protocol . for statistical tests for correlations , one sample t - test for the difference of group mean from zero , and the two sample paired t - test for difference of motion range based on the diaphragm and lipiodol , matlab statistical toolbox quantitative assessment of the lipiodol / diaphragm position of 29 ( 55 % ) lipiodolized tumors , 16 showed contrast that qualified for the purpose of target localization on the 4d - cbct and were entered in the subsequent analysis that included 87 4d - cbct scans . 
 the group means did not significantly differ between the absolute lipiodol and diaphragm positions for all directions , and insignificantly differ from 0 except for the cc direction where both lipiodol and diaphragm positioning showed an average offset of the estimated position towards the caudal direction with respect to the planning midv position . the absolute tumor prediction errors ex y z were summarized for all selected fractions across all individuals and over each individual in fig . 
when registration was made according to the diaphragm , noticeable target misalignment was observed , compared with the lipiodol reference . quantitative assessment of the lipiodol / diaphragm motion range variations of the motion range obtained from 4d registrations by the lipiodol and diaphragm averaged over all selected fractions are demonstrated for individual patients in fig . 
mean variations in the motion range on the 4d - cbct 5 mm relative to the reference 4d - ct for individuals were not infrequent , occurring for diaphragm - based registrations in 31 % of the patients in the cc direction , lipiodol versus diaphragm in 4d - cbct - guided stereotactic radiotherapy of hepatocellular carcinomas1 3 96 fig . 
solid lines are the linear fits with corresponding r2 while variations > 3 mm were observed in 19 and 6 % of the patients in the cc and ap directions for lipiodol - based registrations with 100 % being increases of motion range , and 50 and 19 % for diaphragm - based registration , of which 38 and 67 % were increases . 
concerning those fractions that showed increases of motion range , the 95th percentiles were 2.4 ( lr ) , 6.7 ( cc ) , and 4.0 ( ap ) mm for lipiodol , and 2.4 ( lr ) , 9.1 ( cc ) , and 5.3 ( ap ) mm for the diaphrag the lr and cc motion ranges estimated with the diaphragm were significantly larger ( p < 0.05 ) compared with the reference lipiodol . margin assessment combining the observed variations for lipiodol / diaphragm position , delineation , 4d registration and intrafractional baseline , into the van herks margin formula ( see methods and materials section ) , yields , without any image - guidance correction , the margins as shown in fig . 
when the variability of the diaphragmatic position was entered into the margin recipe , the resulting margins were either underestimated by 3.0 mm ( lr ) and 1.1 mm ( ap ) , or overestimated by 2.1 mm ( cc ) with respect to those calculated with the lipiodol for the motion range from 0 to 20 mm . the tumor prediction error alone contributed 5.6 ( lr ) , 10.0 ( cc ) , and 2.9 ( ap ) mm to the ptv margin even employing online 4d - cbct due to the important systematic and random variations between the lipiodol and the diaphragm ( table 1 )  . 
the possible gain in margin reduction from the online 4d - cbct correction decreased from 5.3 ( lr ) , 7.8 ( cc ) , and 1.9 ( ap ) mm using the lipiodol - guided setup to 2.0 ( lr ) , 2.0 ( cc ) , and 0.7 ( ap ) mm with the diaphragm - guided setup with respect to those without any image - guided correction . 
 in addition , the whole ptv should be shifted 3.0 mm in the caudal direction to correct for the group mean of the lipiodol and the diaphragm motion . discussion linac - integrated cbct is a common ig tool for treatment verification in hypofractionated / stereotactic body radiotherapy of intrahepatic tumors . 
nonetheless , the low soft - tissue contrast in cbct makes visualization of the tumor almost impossible , and therefore anatomical or fiducial marker surrogates are often necessary to guide treatment verification . 
4 planning contour of the gross tumor volume ( gtv ) overlaid on the time - weighted average 4d - cbct images after registration using lipiodol ( top row ) and the diaphragm ( bottom row )  . 
 misalignment of the gtv was observed when target localization was made using the diaphragm as a surrogate , as indicated by the arrows the effect of iv contrast was found to be seriously degraded on cbct , and the signal - to - noise ratio of the iv contrast was very sensitive to the acquisition timing of cbct [ 17 ]  . 
 lipiodol during transarterial chemoembolization ( tace ) was investigated as a direct surrogate for tumor localization previously [ 3 , 18 ] , but this study was the first to assess the potential of combining prior lipiodol contrast with online time - resolved 4d - cbct . 
our preliminary clinical outcomes for primary hcc using this treatment method have demonstrating response rate of 67 % ( with a median follow - up of 12 months ) , and 2 - year overall survival rate of 54 % . for patients without lipiodol contrast , diaphragm / liver contour is the most popular tumor surrogate . 
their benchmark results against the iv contrast - enhanced ct scans that were acquired with a mobile in - room ct found < 3 mm difference in the lr and ap directions but up to 10 mm difference in the cc direction . 
the present work , which included the 4d information in the planning phase and treatment phase with 4d - ct simulation and 4d - cbct verification , also found individual mean tumor prediction error up to 9.5 mm in the cc direction , suggesting that the differential motions between the diaphragm and tumor did play an important role . for our cohort of 16 patients , the systematic tumor prediction error was found to be most important in the cc direction while the random contribution was roughly of the same order magnitude in the three directions and was comparable to those reported by seppenwoolde et al . 
on the other hand , the 3 - mm shift in the caudal direction indicated by the group mean was likely due to the finite axial resolution ( 3 mm ) of the 4d planning ct in comparison to the 4d - cbct with 1 mm axial resolution . 
the shift may also come from the treatment room laser setup which at our institution was intended to offset by 0.5 mm from the radiation isocenter towards the cranial direction to align visually better with the mechanical crosshair at zero gantry degree for daily quality assurance purpose . even with dynamic iv - enhanced or lipiodol contrast , patient breath hold is still important for conventional 3d cbct image acquisition to avoid significant motion artifacts caused by respiratory motion to obtain reasonable image quality . 
although this strategy was useful to minimize respiratory motion , artifacts were still observed in their studies , possibly due to inconsistent anatomy between cbct data acquisitions from different breath holds and / or residual motions such as heart beat and peristalsis . 
5 differences of the leftright , craniocaudal , and anteriorposterior motion ranges between 4d - ct and 4d - cbct obtained by 4d registrations using the lipiodol and diaphragm masks for our patients , it would have been extremely difficult for them to complete the cbct scan in a single breath hold or even in multiple breath holds that usually had to last for > 20 s . 
 such approach of planning and treating at the time - weighted average tumor position was not only suitable for all patients and also allowed a safety margin that is slightly larger than that for the breath hold approach because the systematic contribution due to tumor motion can be reduced to nearly zero , leaving a small random error ( estimated using the sd of the tumor motion , or approximately one third of the tumor amplitude )  . 
another advantage of 4d - cbct over standard 3d - cbct in free breathing treatment condition is the possibility of assessing the variation of motion range , which allowed us to halt the treatments if the increasing motion amplitude was well beyond the set tolerance ( 3 mm in our case )  . 
variations of motion range with the lipiodol over all fractions for individuals were generally small , being less than 3 mm in the lr and 5 mm in the cc and ap directions for all patients . 
their results found that the change of gtvs com position was within 1 mm in all directions after rigid liver - to - liver registration for 16 patients under abdominal compression . 
the same group reported residual displacement of gtvs com > 3 mm in 15 % of the treatment fractions for 12 patients imaged in breath hold [ 22 ] , whereas our study found tumor prediction error > 3 mm in 33 % of the treatment fractions in the cc direction . 
the fem - based dir may be useful to predict the gtvs com position where the gtv cannot be seen without iv / lipiodol contrast , but the poor efficiency because of the necessity of manual liver contouring on multiple cbct datasets ( for a 4d - cbct scan ) on top of the computational overhead thus far restricted its clinical implementation . 
 unlike the usual practice with fiducial markers or lipiodol deposit available for visual inspections , the dir result of the deformed gtvs contour and com cannot be directly confirmed , which may also concern the clinicians or radiotherapists . 
more importantly , using the deformed liver contour to infer via a biomechanical relationship the position of the interior gtv can have vector magnitude residual error as large as 4 mm , which necessitates a considerable ptv margin and , thus , hampering its potential as compared to lipiodol as a direct tumor surrogate . in our study , almost all patients showed decreased lipiodol contrast on the 4d - cbct as compared to on the 4d - ct , and about half of the lipiodolized tumors were abandoned for clinical setup because the lipiodol contrast was too low . 
the clinical implication of changing from lipiodolguided to diaphragm - guided setup due to the absence of lipiodol contrast on 4d - cbct without adapting the ptv margin may warrant further investigation . 
according to our initial experience , the visibility of the lipiodol deposit on the 4d - cbct critically depended on its initial pattern on the planning ct , and that lipiodol deposits that showed higher housfield unit ( hu ) on the 4d - ct usually had better visualization on the 4d - cbct than those with lower hu . 
6 calculated leftright ( lr ) , craniocaudal ( cc ) , and anterior posterior ( ap ) margins inclusive of delineation , 4d - ct to cbct registration , and intrafractional baseline drift for different treatment approaches as a function of motion amplitude . 
margins for the online 4d - cbct - lipiodol were obtained assuming ideal soft - tissue tumor correction protocol with zero systematic errors , while margins for the online 4dcbctdiaphragm were obtained including the systematic and random errors due to the offset between the diaphragm and the lipiodolized tumor in chen et al . 
 [ 16 ] , lipiodol retention showing homogeneous and defective patterns was more frequent in the patient group receiving the high dose ( 2053 ml ) than that given the low dose ( 515 ml )  . 
based on the initial findings of this study and previous reports , we have started to adjust the lipiodol volume to achieve better lipiodol contrast on 4d - cbct for tumor localization . conclusion image guidance using lipiodol combined with 4d - cbct enables accurate localization of hcc , thus , permitting significant reduction of uncertainty from the diaphragm surrogate and motion artifacts . 
part of the results of this work has been presented at the estro 3rd forum . the accompanying manuscript does not include studies on humans or animals . strahlenther onkol ( 2016 ) 192 : 136138 doi 10.1007 / s00066 - 015 - 0931 - 2 prognosebestimmung mit genexpressionsanalysen konsequenzen fr die indikation zur radiotherapie ? ren baumann david krug online publiziert : 8 . 
dezember 2015 springer - verlag berlin heidelberg 2015 hintergrund die indikation zu einer adjuvanten therapie beruht immer auf einer risikoanalyse ( prognoseabschtzung ) und der kenntnis ber die generelle wirksamkeit der weiteren therapie . 
in den aktuellen originalpublikation fitzal f , filipits m , rudas m et al ( 2015 ) the genomic expression test endopredict is a prognostic tool for identifying risk of local recurrence in postmenopausal endocrine receptor - positive , her2neu - negative breast cancer patients randomised within the prospective abcsg 8 trial . 
bisher gibt es wenige daten zur frage , ob diese verfahren auch zur bewertung des lokalen rckfallrisikos geeignet sind und ob sie eine prdiktive aussagekraft bezglich des nutzens einer radiotherapie haben . 
damit haben sich jetzt fitzal und mitarbeiter auseinandergesetzt [ 4 ]  . patientinnen und methoden analysiert wurde in dieser studie eine subgruppe von 1324 patientinnen , die in der sterreichischen abcsg - 8 - studie ( rekrutierung 1996 2004 , n = 3713 ) behandelt wurden . 
die initiale fragestellung dieser prospektiven randomisierten abcsg - 8 - studie bezog sich auf die antihormonelle therapie ( tamoxifen , gefolgt von anastrozol versus tamoxifen allein ) bei postmenopausalen , hormonrezeptor - positiven brustkrebspatientinnen . 
die lokaltherapie war , wenn mglich , eine brusterhaltende operation ( bet ) : tumorektomie plus sn - biopsie , axilladissektion bei positivem sn , adjuvante radiotherapie ( rt ) der brust als standard . 
innerhalb der aktuellen subgruppenanalyse befanden sich 138 brusterhaltend operierte patientinnen , welche beim vorliegen von low - risk - tumoren ( durchmesser < 3 cm , pn0 , g12 ) gem einer weiteren randomisierung keine radiotherapie nach bet erhalten hatten . 
 die gewebeproben ( 641 der low - risk - gruppe und 683 der high - risk - gruppe ) wurden in der aktuellen studie mit dem ep - test ausgewertet . 
nach der stratifizierung in ep - risikoprofile zeigten sich bei verzicht auf eine adjuvante radiotherapie in der hochrisikogruppe 12 % rezidive im vergleich zu der niedrigrisikogruppe mit 11 , 1 % rezidiven . 
die trennschrfe des tests war aber aufgrund der insgesamt niedrigen risikokonstellation eher gering , das 5 - jahres - berleben ohne lokalrezidiv lag bei 98 , 6 % ( low risk ) bzw . 
festzuhalten blieb jedoch , dass die radiotherapie in beiden risikokollektiven hocheffektiv war : in der ep - low - risk - gruppe sank die lokalrezidivrate von 11 , 1 % auf 0 , 2 % ( p < 0 , 001 ) und im high - risk - arm von 12 , 0 % auf 2 , 5 % . schlussfolgerung der autoren mit dem genexpressionstest endopredict knnen patientinnen mit niedrigem lokalem rckfallrisiko identifiziert werden . 
insbesondere geht es um solche der low - risk - gruppe ( nodal negativ , hormonrezeptor - positiv ) , innerhalb derer durch das testergebnis eine kleine gruppe mit erhhtem metastasierungsrisiko ( und daraus abgeleiteter indikation zur chemotherapie ) identifiziert werden kann [ 13 ]  . 
betrachtet man beispielsweise den oncotype - dx - test , so lassen sich gruppen mit einem rezidivrisiko zwischen < 5 % bis hin zu 16 % nach 10 jahren identifizieren . 
das testergebnis kann damit in grenzsituationen eine gnstige prognose besttigen und die entscheidung gegen eine zustzliche chemotherapie erleichtern . genetische tests sind im allgemeinen jedoch nur fr prognostische aussagen zum metastasierungsrisiko validiert , teilweise auch nur fr 5 jahre , also ohne bewertung einer spten metastasierung . 
zunchst ist nmlich zu klren , ob diese verfahren berhaupt informationen zum lokalen rckfallrisiko geben und nicht nur zum fernmetastasierungsrisiko . dass es patientinnen mit niedrigem lokalrezidivrisiko gibt , ist unstrittig [ 6 ]  . 
mamounas und mitarbeiter haben krzlich bei patientinnen aus den nsabp - 14und - 20 - studien den oncotype - dx - test mit der analyse von 21 genen bei prund postmenopausalen brustkrebspatientinnen eingesetzt . 
bei postmenopausalen patientinnen , die mit bet und rt behandelt worden waren , konnte der test keine signifikanten unterschiede hinsichtlich des lokalrezidivrisikos in der radiotherapiegruppe identifizieren [ 6 ]  . 
dubsky p , filipits m , jakesz r et al ( 2013 ) endopredict improves the prognostic classification derived from commonclinical guidelines in er - positive , her2 - negative early breast cancer . 
filipits m , rudas m , jakesz r et al ( 2011 ) a new molecular predictor of distant recurrence in er - positive , her2 - negative breast cancer adds independent information to conventional clinical risk factors . 
fitzal f , filipits m , rudas m et al ( 2015 ) the genomic expression test endopredict is a prognostic tool for identifying risk of local recurrence in postmenopausal endocrine receptor - positive , her2neunegative breast cancer patients randomised within the prospective abcsg 8 trial . 
liu ff , shi w , done sj et al ( 2015 ) identification of a low - risk luminal a breast cancer cohort that may not benefit from breast radiotherapy . 
ontario clinical oncology group ( ocog ) a prospective cohort study evaluating risk of local recurrence following breast conserving surgery and endocrine therapy in low risk luminal a breast cancer ( lumina ) ; clinicaltrials.gov identifier : nct01791829 8 . 
perou cm , sorlie t , eisen mb , van de rijn m , jeffrey ss , rees ca , pollack jr , ross dt , johnsen h , akslen la , fluge o , pergamenschikov a , williams c , zhu sx , lonning pe , borresen - dale al , brown po , botstein d ( 2000 ) molecularportraits of human breasttumours . 
tramm t , kyndi m , myrhe s et al ( 2014 ) relationship between the prognostic and predictive value of the intrinsic subtypes and a validated gene profile predictive of loco - regional control and benefit from post - mastectomy radiotherapy in patients with high - risk breast cancer . 
acta oncol 53 : 13371346 erreicht ! die wichtigste aussage der autoren ist deshalb : endopredict ist nicht in der lage , eine patientengruppe zu identifizieren , bei der auf eine radiotherapie verzichtet werden kann . 
auch die retrospektive auswertung einer kanadischen studie zum bestrahlungsverzicht hat krzlich diese aussage mithilfe eines panels von fnf immunhistochemischen parametern besttigt [ 5 ]  . bei betrachtung der postmastektomie - radiotherapie ( pmrt ) sieht die datenlage anders aus . 
die derzeit rekrutierende , prospektive einarmige lumina - studie liefern [ 7 ] , welche patientinnen 55 jahre mit den gnstigen luminal - a - tumoren im stadium pt1n0 nach bet untersucht , die alleinig endokrin weiter behandelt werden . fazit genexpressionstests knnen die entscheidung fr oder gegen eine adjuvante chemotherapie erleichtern und geben zustzliche informationen ber die wahrscheinlichkeit von lokalrezidiven . 
insbesondere erlauben sie nicht , patientinnen zu identifizieren , die nicht von einer radiotherapie profitieren . ren baumann , kiel , und david krug , heidelberg einhaltung ethischer richtlinien interessenkonflikt r . 
krug1 3 strahlenther onkol ( 2016 ) 192 : 130132 doi 10.1007 / s00066 - 015 - 0930 - 3 verbesserte prognose fr symptomfreie ltere frauen mit einem durch mammographie detektiertem mammakarzinom ? alexander katalinic online publiziert : 7 . 
dezember 2015 springer - verlag berlin heidelberg 2015 ziel der arbeit evaluation der charakteristika und des verlaufs von mammakarzinomen bei patientinnen , 75 jahre und lter , deren karzinome mit der mammographie detektiert wurden , also einer altersgruppe , die nicht in effektivittsstudien zum mammographie - screening eingeschlossen ist . material und methoden prospektive kohortenstudie mit patientinnen im alter von 75 jahren und lter mit primrem mammakarzinom im stadium 0iv ( von 19902011 ) , identifiziert aus dem patientenregister der autoren ( n = 1162 )  . 
im untersuchungszeitraum nahmen die karzinome im stadium ii um 8 % ab , die karzinome originalpublikation malmgren ja , parikh j , alwood mk , kaplan hg ( 2014 ) improved prognosis of women aged 75 and older with mammography - detected breast cancer . 
katalinic ( ) institut fr sozialmedizin und epidemiologie , universitt zu lbeck , ratzeburger allee 160 , 23562 lbeck , deutschland e - mail : alexander.katalinic@uksh.de im stadium 0 aber um 15 % zu ( p < 0 , 001 )  . 
legen eine qualitativ hochwertige registerstudie vor , in der frauen im alter von 75 jahren und lter mit mammakarzinom anhand des detektionsmodus in zwei gruppen unterschieden und anschlieend hinsichtlich tumorcharakteristika und prognose untersucht wurden . 
zu nennen sind hier der lead time bias ( vorverlegung des diagnosezeitpunkts mit artifizieller verlngerung der berlebenszeit ohne echten lebenszeitgewinn ) und der length time bias ( entdeckung von langsam wachsenden tumoren mit einer a priori gnstigeren berlebenszeit )  . 
die eigentlich wichtige fragestellung nach der reduktion der krankheitsspezifischen mortalitt wird aber nicht thematisiert , nmlich : ist die brustkrebssterblichkeit in einer gruppe von asymptomatischen frauen 75 jahre , die sich einer mammographie unterzogen , niedriger als in einer vergleichbaren gruppe ohne mammographie ? leider werden in der arbeit auch weitere mgliche verzerrungsmglichkeiten nicht diskutiert . 
frauen , die eine frherkennungsmammographie bekamen , knnten einen hheren sozialstatus und weniger komorbiditt haben , frher an einem regulren mammographie - screening teilgenommen haben oder einen gnstigeren lebensstil und eine bessere compliance bei der therapie aufweisen . 
wird nun bei einer 80 - jhrigen ein kleiner tumor oder ein dcis entdeckt , ist die wahrscheinlichkeit zu bercksichtigen , dass dieser in der verbleibenden lebensspanne nie beschwerden verursacht htte bzw . 
 berdiagnosen sind daher bei der interpretation von ergebnissen unbedingt mit zu bercksichtigen . fazit zusammenfassend ist die frage , ob die systematische mammographie bei asymptomatischen frauen 75 jahre tatschlich die mortalitt verringert , mit dem gewhlten studiendesign der publikation nicht zu beantworten . 
die who sieht zwar eine positive evidenz fr die altersgruppe zwischen 70 und 74 jahren , doch ob diese in das ltere alterssegment bertragbar ist , bleibt unklar [ 2 ]  . dennoch scheint die empfehlung der s3 - leitlinie zur brustkrebsfrherkennung , dass sich nmlich frauen ab dem 70 . 
lebensjahr unter bercksichtigung des persnlichen risikoprofils , des gesundheitszustands und der lebenserwartung regelmigen mammographien unterziehen sollten , gerechtfertigt [ 3 ] , insbesondere wenn die betreffende frau vor dem 70 . 
lebensjahr regelmig am mammographie - screening teilnah die gefahr von berdiagnosen mit mammographie drfte dann durch das bereits erfolgte wegfischen von befunden in den vorjahren gering se bei symptomlosen frauen ab dem 75 . 
dies sollte solange gelten , bis durch hochqualitative studien ein gnstiges nutzen - schaden - verhltnis gezeigt wird . alexander katalinic , lbeck verbesserte prognose fr symptomfreie ltere frauen mit einem durch mammographie1 3 132 einhaltung ethischer richtlinien interessenkonflikt a . 
lauby - secretan b , scoccianti c , loomis d , benbrahim - tallaa l , bouvard v , bianchini f et al ( 2015 ) breast - cancer screeningviewpoint of the iarc working group . 
katalinic1 3 strahlenther onkol ( 2016 ) 192 : 133135 doi 10.1007 / s00066 - 015 - 0933 - 0 keine verbesserung des progressionsfreien berlebens von patienten mit lokal fortgeschrittenem nsclc durch konsolidierende chemotherapie nach simultaner radiochemotherapie nadja ebert michael baumann online publiziert : 23 . 
 die rct wurde mit docetaxel ( 20 mg / m2 ) und cisplatin ( 20 mg / m2 ) einmal wchentlich fr 6 wochen simultan zur strahlentherapie mit einer gesamtdosis von 66 gy in 33 fraktionen appliziert . 
nach studieneinschluss erhielten 17 patienten aufgrund einer rcknahme der einoriginalpublikation ahn js , ahn yc , kim jh et al ( 2015 ) multinational randomized phase iii trial with or without consolidation chemotherapy using docetaxel and cisplatin after concurrent chemoradiation in inoperable stage iii non - small - cell lung cancer . 
das mediane pfs betrug 8 , 1 monate im beobachtungsarm und 9 , 1 monate im konsolidierungsarm [ hazard ratio ( hr ) 0 , 91 ; 95% - vertrauensbereich ( vb ) 0 , 731 , 12 ; p = 0 , 36 ]  . 
die vorliegende , hier kommentierte , randomisierte studie , in die 437 patienten literatur kommentiert 134 aus sdkorea und der volksrepublik china eingebracht und die daten von 420 personen ausgewertet wurden , ist eine der bislang grten studien zu dieser fragestellung . 
die ergebnisse zeigen nun aber keinen vorteil durch eine konsolidierende chemotherapie nach rct [ 5 ]  . einschlusskriterien und staging - untersuchungen der studie entsprachen den internationalen standards , ebenso das in der studie applizierte strahlentherapieschema mit einer gesamtdosis von 66 gy in konventioneller fraktionierung . 
mit 20 mg / m2 liegt die cisplatin - dosis innerhalb der empfohlenen bandbreite von 6 mg / m2 tglich bis zu 100 mg / m2 im abstand mehrerer wochen [ 3 ]  . 
in einer metaanalyse von 9 randomisierten studien mit individuellen patientendaten konnte kein signifikanter unterschied zwischen diesen applikationsprotokollen und dosierungen gefunden werden [ 7 ]  . im vergleich zu den kumulativen cisplatin - dosen bei der rct von kopf - halsoder zervixkarzinomen , die durchschnittlich 200 mg / m2 betragen [ 8 , 9 ] , ist die in der studie von ahn et al . 
verwendete dosis fr die konsolidierende chemotherapie mit 35 mg / m2 erheblich geringer , allerdings in kombination mit cisplatin einer studie zur konsolidierenden chemotherapie nach primrer rct an kopf - hals - tumoren wurden dosen von 75 mg / m2 fr cisplatin und docetaxel verwendet . 
mit einem medianen berleben von 20 monaten und einer 5 - jahres - berlebensrate von etwa 20% sprechen allerdings fr eine insgesamt gute wirksamkeit und qualitt der in der studie durchgefhrten behandlung . beim design einer konsolidierenden chemotherapie besteht ebenso weitgehende uneinheitlichkeit [ 3 , 7 , 8 ]  . 
des weiteren verstarben 2 , 9% der patienten im therapiearm mit konsolidierender chemotherapie behandlungsbedingt , in der kontrollgruppe aber keiner [ 5 ]  . die tatsache , dass nur eine relativ kleine gruppe von patienten die komplette konsolidierende chemotherapie erhielt , knnte als erklrung fr das negative ergebnis der studie herangezogen werden , wenn man davon ausgeht , dass nur patienten mit der kompletten chemotherapie von einer konsolidierenden chemotherapie profitieren . 
dagegen spricht allerdings , dass auch in der vergleichbaren phaseiii - studie der housier oncology group , bei der 80% der patienten die geplanten 3 zyklen einer konsolidierenden chemotherapie mit docetaxel als monotherapie erhielten , kein vorteil gegenber einer alleinigen rct erzielt werden konnte . 
diese studie wurde brigens vorzeitig beendet , weil aufgrund einer interimsanalyse nach 147 rekrutierten patienten nicht mehr zu erwarten war , dass sich das behandlungsergebnis im experimentellen arm noch verbessern wrde , wenn man die studie weiterfhrt [ 11 ]  . 
alle bisherigen untersuchungen , einschlielich der aktuellen studie , verliefen somit bezglich der konsolidierenden systemischen chemotherapie nach rct negativ [ 5 , 11 , 14 ]  . fazit derzeit gibt es keine evidenz dafr , dass eine konsolidierende chemotherapie nach radiochemotherapie lokal fortgeschrittener nsclc die behandlungsergebnisse bezglich eines progressionsfreien berlebens bzw . 
zatloukal p , petruzelka l , zemanova m , havel l , janku f , judas l , kubik a , krepela e , fiala p , pecen l ( 2004 ) concurrent versus sequential chemoradiotherapy with cisplatin and vinorelbine in locally advanced non - small cell lung cancer : a randomized study . 
curran wj , paulus r , langer cj , komaki r , lee js , hauser s , movsas b , wasserman t , rosenthal sa , gore e , machtay m , sause w , cox jd ( 2011 ) sequential vs concurrent chemoradiation for stage iii nonsmall cell lung cancer : randomized phase iii trial rtog 9410 . 
auprin a , le pchoux c , rolland e , curran wj , furuse k , fournel p , belderbos j , clamon g , ulutin hc , paulus r , yamanaka t , bozonnat m - c , uitterhoeve a , wang x , stewart l , arriagada r , burdett s , pignon j - p ( 2010 ) meta - analysis of concomitant versus sequential radiochemotherapy in locally advanced nonsmall - cell lung cancer . 
belani cp , choy h , bonomi p , scott c , travis p , haluschak j , curran wj ( 2005 ) combined chemoradiotherapy regimens of paclitaxel and carboplatin for locally advanced nonsmall - cell lung cancer : a randomized phase ii locally advanced multi - modality protocol . 
bradley jd , paulus r , komaki r , masters g , blumenschein g , schild s , bogart j , hu c , forster k , magliocco a , kavadi v , garces yi , narayan s , iyengar p , robinson c , wynn rb , koprowski c , meng j , beitler j , gaur r , curran wj , choy h ( 2015 ) standarddose versus high - dose conformal radiotherapy with concurrent and consolidation carboplatin plus paclitaxel with or without cetuximab for patients with stage iiia or iiib non - small - cell lung cancer ( rtog 0617 ) : a randomised , two - by - two factorial phase 3 study . 
auperin a , le pechoux c , pignon jp , koning c , jeremic b , clamon g , einhorn l , ball d , trovo mg , groen hjm , bonner ja , le chevalier t , arriagada r ( 2006 ) concomitant radio - chemotherapy based on platin compounds in patients with locally advanced nonsmall cell lung cancer ( nsclc ) : a meta - analysis of individual data from 1764 patients . 
chemoradiotherapy for cervical cancer meta - analysis collaboration ( 2008 ) reducing uncertainties about the effects of chemoradiotherapy for cervical cancer : a systematic review and meta - analysis of individual patient data from 18 randomized trials . 
gandara dr , chansky k , albain ks , leigh br , gaspar le , lara pn , burris h , gumerlock p , kuebler jp , bearden jd , crowley j , livingston r ( 2003 ) consolidation docetaxel after concurrent chemoradiotherapy in stage iiib nonsmall - cell lung cancer : phase ii southwest oncology group study s9504 . 
hanna n , neubauer m , yiannoutsos c , mcgarry r , arseneau j , ansari r , reynolds c , govindan r , melnyk a , fisher w , richards d , bruetman d , anderson t , chowhan n , nattam s , mantravadi p , johnson c , breen t , white a , einhorn l ( 2008 ) phase iii study of cisplatin , etoposide , and concurrent chest radiation with or without consolidation docetaxel in patients with inoperable stage iii nonsmall - cell lung cancer : the hoosier oncology group and u.s. 
jain ak , hughes rs , sandler ab , dowlati a , schwartzberg ls , dobbs t , schlabach l , wu j , muldowney nj , choy h ( 2009 ) a phase ii study of concurrent chemoradiation with weekly docetaxel , carboplatin , and radiation therapy followed by consolidation chemotherapy with docetaxel and carboplatin for locally advanced inoperable non - small cell lung cancer ( nsclc )  . 
lee kc , lee sh , lee y , park sh , park j , cho ek , shin db , lee jh , kim dy , kim st ( 2008 ) prospective pilot study of consolidation chemotherapy with docetaxel and cisplatin after concurrent chemoradiotherapy for advanced head and neck cancer . 
tsujino k , kurata t , yamamoto s , kawaguchi t , kubo a , isa s , hasegawa y , ou sh , takada m , ando m ( 2013 ) is consolidation chemotherapy after concurrent chemo - radiotherapy beneficial for patients with locally advanced non - small - cell lung cancer ? a pooled analysis of the literature . 
nsclc meta - analyses collaborative group ( 2010 ) adjuvant chemotherapy , with or without postoperative radiotherapy , in operable non - small - cell lung cancer : two meta - analyses of individual patient data . 
lancet 375 : 12671277 keine verbesserung des progressionsfreien berlebens von patienten mit lokal1 3 strahlenther onkol ( 2016 ) 192 : 6769 doi 10.1007 / s00066 - 015 - 0924 - 1 akuttoxizitt nach hypofraktionierter versus konventionell fraktionierter strahlentherapie bei patienten mit prostatakarzinom frank lohr michael ehmann online publiziert : 6 . 
november 2015 springer - verlag berlin heidelberg 2015 hintergrund im jahre 2007 begann die randomisierte phase - iii - studie ( hypro ) , die den effekt einer hypofraktionierten im vergleich zu einer normal fraktionierten strahlentherapie bei patienten mit prostatakarzinom auf das rezidivfreie berleben untersuchen sollte . 
in der hier kommentierten arbeit geht es um die akuten gastrointestinalen und urogenitalen nebenwirkungen . methoden in die studie wurden aus sieben niederlndischen strahlentherapiezentren patienten im alter zwischen 44 und 85 jahren mit histologisch gesicherten prostatakarzinomen mit intermedirem oder hohem risiko eingeschlossen . 
es handelte sich um tumoren in den stadien t1bt4 nx0 mx0 mit einem serum - psa von < 60 ng / ml oder niedriger und einem who - performance - status von 02 . 
mit hilfe einer webbasierten applikation wurden patienten im verhltnis 1 : 1 randomisiert , entweder zu einer strahlentherapie mit standardfraktionierung ( 39 fraktionen zu je 2 gy / 8 wochen ) oder einer hypofraktionierung ( 19 fraktionen zu je 3 , 4 gy / 6 , 5 wochen , 3 fraktionen / woche )  . 
nichtunterlegenheit der hypooriginalpublikation aluwini s , pos f , schimmel e et al ( 2015 ) hypofractionated versus conventionally fractionated radiotherapy for patients with prostate cancer ( hypro ) : acute toxicity results from a randomised non - inferiority phase 3 trial . 
ehmann klinik fr strahlentherapie und radioonkologie , universittsmedizin mannheim , theodor - kutzer - ufer 13 , 68167 mannheim , deutschland e - mail : frank.lohr@umm.de fraktionierung wurde separat fr urogenitale und gastrointestinale akuttoxizitt getestet mit der nullhypothese , dass kumulative inzidenzen jedes toxizittstyps nicht mehr als 8 % hher in der hypofraktionierungsgruppe als bei standardfraktionierung sind . 
drei monate nach strahlentherapie berichteten 73 patienten ( 22 % ) in der standardfraktionierungsgruppe und 75 ( 23 % ) in der hypofraktionierungsgruppe ber urogenitale toxizitt grad 2 sowie 43 ( 13 % ) versus 42 patienten ( 13 % ) ber gastrointestinale toxizitt grad 2 . 
die kumulative inzidenz akuter gastrointestinaler toxizitt grad 2 war 120 tage nach hypofraktionierung hher ( 42 , 0 % ; 37 , 2 46 , 9 ) als nach standardfraktionierung ( 31 , 2 % ; 95 % - ki 26 , 635 , 8 ; differenz 10 , 8 % ; 90 % - ki 5 , 2516 , 43 ; or 1 , 6 ; p = 0 , 0015 ; nichtunterlegenheit nicht besttigt )  . literatur kommentiert 68 schlussfolgerung der autoren hypofraktionierung war der standardfraktionierung bezglich urogenitaler und gastrointestinaler toxizitt bei mnnern mit prostatakarzinom bei intermedirem oder hohem risiko nicht nicht - unterlegen . 
die patienten verbleiben in beobachtung hinsichtlich der effektivittsendpunkte . kommentar eine dosiseskalation bei der strahlentherapie des prostatakarzinoms hat das biochemisch rezidivfreie berleben ( brfs ) in mehreren randomisierten studien bei tolerabler toxizitt verbessern knnen [ 13 ]  . 
die bisherigen ergebnisse mit solchen schemata waren allerdings zwiespltig . whrend in der randomisierten kanadischen studie die hypofraktionierung sowohl hinsichtlich toxizitt als auch brfs schlechter als die normofraktionierung abschnitt [ 8 ] , berichteten die autoren der italienischen studie ber ein besseres brfs durch hypofraktionierung bei gleicher toxizitt [ 9 ]  . 
im fox chase cancer center [ 10 ] waren die erfahrungen mit der hypofraktionierung hinsichtlich toxizitt und brfs schlechter als bei der normofraktionierung , allerdings wegen der kleinen patientenzahlen statistisch nicht signifikant . damit besteht derzeit wegen unterschiedlicher aussagen eine unklare situation . 
daher sollten der hier besprochene hypro - trial sowie krzlich als abstract publizierte ergebnisse der britischen chhip - studie ( [ 11 ] , die vollpublikation steht noch aus ) und spter auch die rtog0415sowie die profit - studie die datenlage verbessern , insbesondere deshalb , weil sie mit modernen bestrahlungstechniken durchgefhrt wurden : anspruchsvolle 3d - crt / imrt , teilweise igrt . die aktuelle auswertung der hypro - studie befasst sich mit der akuttoxizitt der hypofraktionierung . 
in der gesamtschwere scheinen diese unterschiede akzeptabel , auch wenn hier formal ( im falle der urogenitalen nebenwirkungen durch underpowering , im fall der gastrointestinalen nebenwirkungen durch signifikante effektunterschiede ) die nicht - nichtunterlegenheit der hypofraktionierung festgestellt werden muss . im auge behalten werden sollten schlielich im hier besprochenen kontext auch die daten des ascendert - trials [ 12 ] , der eine dosiseskalation mithilfe der brachytherapie erreicht und mit der allein externen bestrahlung vergleicht . 
der vergleich des ldr - boosts mit off - protocol - hdr - daten scheint in diesem fall auf eine berlegenheit des ldr - boosts hinzuweisen , was mglicherweise a / b - berechnungen zwischen der hdrhypofraktionierung und den dosisquivalenten einer der standardfraktionierung entsprechenden ldr - brachytherapie ermglicht . 
hier muss zunchst allerdings noch die vollpublikation abgewartet werden . fazit die hochdosierte strahlentherapie des prostatakarzinoms fhrt zu immer besseren ergebnissen bezglich des brfs und mglicherweise auch des berlebens , auch wenn dieser endpunkt angesichts von immer mehr confoundern / salvagetherapien immer schwerer zu bewerten ist . 
die vorliegende arbeit liefert einen weiteren datenpunkt , der nahe legt , dass moderat hypofraktionierte bestrahlungsprotokolle nicht bezglich aller medizinischer endpunkte den normofraktionierten schemata berlegen sind , jedoch bisher beherrschbar erscheinen . 
dearnaley dp , jovic g , syndikus i et al ( 2014 ) escalated - dose versus control - dose conformal radiotherapy for prostate cancer : long - term results from the mrc rt01 randomised controlled trial . 
heemsbergen wd , al - mamgani a , slot a , dielwart mf , lebesque jv ( 2014 ) long - term results of the dutch randomized prostate cancer trial : impact of dose - escalation on local , biochemical , clinical failure , and survival . 
king c , freeman d , kaplan i et al ( 2013 ) stereotactic body radiotherapy for localized prostate cancer : pooled analysis from a multi - institutional consortium of prospective phase ii trials . 
arcangeli s , strigari l , gomellini s et al ( 2012 ) updated results and patterns of failure in a randomized hypofractionation trial for high - risk prostate cancer . 
dearnaley d , syndikus i , sumo g et al ( 2012 ) conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : preliminary safety results from the chhip randomised controlled trial . 
morris j , tyldesley s , pai h et al ( 2015 ) ascende - rt : a multicenter , randomized trial of dose - escalated external beam radiation therapy versus low - dose - rate brachytherapy for men with unfavorable - risk localized prostate cancer . 
j clin oncol 33 akuttoxizitt nach hypofraktionierter versus konventionell fraktionierter strahlentherapie1 3 strahlenther onkol ( 2016 ) 192 : 1724 doi 10.1007 / s00066 - 015 - 0913 - 4 comparative treatment planning study on sequential vs . 
both strategies provided satisfactory oar sparing . conclusion this study showed significant dosimetric differences with potential clinical relevance between two vmat boost strategies regarding coverage , conformity and dose to the ptvs . 
a clinical phase iii / iv trial endorsed by the german head and neck clinical trials group ( iag - kht ) will evaluate differences in acute / late toxicity as well as in locoregional recurrences between the two boost techniques . keywords radiotherapy volumetric modulated arc therapy chemoradiation sequential boost toxicity simultaneous integrated boost vergleichende therapieplanungsstudie zum sequentiell oder simultan integrierten boost bei patienten mit kopf - hals - tumoren unterschiede in der dosisverteilung und potentielle implikationen fr die klinische praxis zusammenfassung ziel vergleich von sequentiellem ( seqb ) und simultanintegriertem boost ( sib ) mit moderner volumetrischer arc - therapie ( vmat ) fr patienten mit plattenepithelkarzinomen der kopf - hals - region . original article 18 patienten und methoden fr 10 patienten mit plattenepithelkarzinomen der kopf - hals - region und definitiver radiochemotherapie erfolgte eine vmat - planung als seqb und sib fr die planungszielvolumina ( ptv ) 13 . 
 es wurden dosisverteilung , abdeckung , konformitt , und homogenitt der ptvs sowie die risikoorganschonung verglichen . ergebnisse das mittlere definierte volumen standardabweichung betrug 137 , 7 44 , 8 cm3 , 351 , 3 83 , 9 cm3 und 895 , 6 120 , 5 cm3 fr die ptvs13 . 
seqb erreichte jedoch signifikant bessere abdeckung des ptv1 / 3 , schlechtere konformitt fr ptv13 und eine hhere mittlerer dosis ( 111115 % ) in ptv2 / 3 , ( p 0 , 007 )  . 
beide boost - strategien fhrten zu vergleichbar guter risikoorganschonung . vergleichende bestrahlungsschlussfolgerung diese planungsstudie zeigt wichtige dosimetrische unterschiede in bezug auf ptv - abdeckung , konformitt und dosis , die mglicherweise klinisch relevant sein knnten . 
eine klinische phase - iii / iv - studie mit untersttzung der interdisziplinren arbeitsgruppe fr kopf - hals - tumoren der deutschen krebsgesellschaft ( iag - kht ) wird derzeit vorbereitet , die zur klrung der wertigkeit dieser beiden boost - techniken im hinblick auf akutund sptmorbiditt und lokoregionre rezidive beitragen kann . schlsselwrter strahlentherapie volumetrisch modulierte arc - therapie radiochemotherapie sequentieller boost toxizitt simultan integrierter boost definitive chemoradiation remains the standard of care for patients with locally advanced squamous cell carcinoma of the head and neck ( lahnscc ) [ 1 ] with locoregional relapse as the main form of failure . 
historically , radiotherapy ( rtx ) has been applied using a shrinking field or so - called sequential boost ( seqb ) strategy , starting with a large treatment volume and progressively shrinking it , corresponding to the different total doses needed for tumor control for the low ( elective lymph node levels ) , intermediateand highrisk target volumes ( tv )  . 
the simultaneous integrated boost ( sib ) technique using intensity - modulated radiotherapy ( imrt ) or volumetric modulated arc therapy ( vmat ) [ 2 ] allows risk - adapted single plan efficient planning and treatment with different dose levels and intensities appropriate for the selected tvs . 
 imrt caused significantly fewer occurrences of xerostomia without compromising tumor control as compared to threedimensional conformal rtx ( 3d - crtx ) in a phase iii trial on patients with hnscc by parotid gland ( pg ) sparing to a mean dose of < 26 gy [ 6 ]  . 
despite the fact that , besides one trial on patients with nasopharyngeal carcinoma [ 17 ] , no randomized prospective trial comparing outcome data and / or toxicity for seqb versus sib ( chemo ) rtx for lahnscc has been published , many departments around the world have adopted the sib as current practice , assuming it to be as effective as seqb . this comparative planning study compares three dose level seqb and sib derived cumulative dosevolume histograms ( dvh ) for tvs , and organs at risk ( oar ) using modern vmat technology instead of imrt for lahnscc by comprehensive evaluation of various established plan quality parameters . 
this data should underline the rationale for a phase iii / iv randomized multicenter trial . patients and methods patient selection and contouring ten patients with lahnscc were randomly selected from a list of patients previously treated with a definitive vmat ( rapidarc , varian medical systems , palo alto , ca , usa ) plan at our department . 
the final dose distribution was calculated using the aaa algorithm ( 2.5 mm grid size )  . plan evaluation quantitative comparisons used a dvh analysis , with parallel qualitative visual comparisons of the axial isodose curves . 
the mean volumes of ptv13 , the dmean , dmax ( maximal dose to the ptv ) , d2 ( dose delivered to at most 2 % of the ptv ) , d100 ( dose delivered to 100 % of the ptv ) , d98 ( dose delivered to 98 % of the ptv ) and d95 ( dose delivered to 95 % of the ptv ) for ptv13 were also evaluated . 
the salt coverage factor ( cvfsalt ; cvf = tvri / tv ; tvri : irradiated tv encompassed by the 95 % reference isodose ) was calculated for each ptv , with 1 indicating perfect coverage . 
the conformities of the dose distributions were calculated with : rtog conformity index ( cirtog ; ci = vri / tv ; vri : irradiated volume encompassed by the 95 % reference isodose )  . 
both strategies achieved excellent coverage for all ptvs ( range of cvfsalt for seqb : 0.971 , and for sib : 0.950.97 ) with a significantly better cvfsalt for ptv1 and 3 in seqb plans . 
 sib plans gave dmeans for all ptvs ( p 0.007 ) close to the prescribed doses ( range 1.11.5 % ) , while seqb plans had higher than prescribed dmeans to ptv2 and ptv3 . 
1 final dose distribution for an example patient showing the surrounding 95 % isodose to ptv3 for a seqb ( summation of plans 14 ) and b sib plans nique . 
the data demonstrates that there were no significant ( pgs , oc , nt ) or clinically relevant differences regarding classical oar ( sc , bs and larynx )  . 
 interestingly , the seqb gave a significantly lower physical mean dmax to the sc and bs , which may translate into an even larger advantage when the biological sparing ( eqd2 ) of the hart approach is taken into account . 
our data show that the appropriate definition of the tv is especially crucial with the sib approach and demands detailed knowledge of clinical findings as provided by collaboration with the surgeon together with high - resolution imaging . 
this raises the question as to what kinds of cross - sectional , multiplanar or functional imaging should be used in defining the gtv , and what is the most sensitive and specific imaging method to detect lymph node metastasis . 
 [ 25 ] showed a pooled sensitivity of 89 % and a specificity of 89.5 % for fdg - pet / ct and a corresponding pooled sensitivity and specificity of 71.6 and 78 % for standard conventional imaging methods . furthermore , a recent detailed per - neck - level meta - analysis on 13 studies ( 3460 neck levels ) demonstrated a sensitivity and specificity for fdg - pet / ct of 84 and 96 % , and for conventional imaging of 63 and 96 % , respectively , for the detection of nodal metastasis in this group of patients [ 26 ]  . 
fdg - pet / ct carries inherent limitations , including its inability to define the depth of invasion due to inflammatory changes of the tumor environment and the relation of tumors to neighboring structures [ 27 ]  . 
although fdg - pet / ct does not seem to add value over ct for the routine delineation of nodal gtvs , the implementation of an automated segmentation method to improve the reproducibility and interinstitutional comparison of nodal gtvs has been recommended if it be used [ 28 ]  . 
simultaneous integrated1 3 table 3 dosevolume histogram parameters and treatment efficiency for seqb and sib plans ( mean sd ) p - value volume ptv1 ptv1 coverage conformity homogeneity ptv2 ptv2 coverage conformity homogeneity ptv3 ptv3 coverage conformity homogeneity conformity larynx body parameter defined volume ref . 
this could imply a higher risk of acute and late effects of rtx , including dysphagia , xerostomia , edema , subcutaneous fibrosis , muscle strictures and osteoradionecrosis , possibly affecting tissues not routinely delineated and therefore not accounted for with constraints during planning . 
 however , the sib technique has been adopted for clinical studies [ 716 , 29 ] and in the daily routine as the primary approach without clear evidence of equality or noninferiority in terms of efficacy and safety . 
possible strategies to prevent excessive weight loss and changes in dose distribution could include the routine placement of a gastric feeding tube prior to chemoradiation and weekly dietary counselling [ 30 ]  . 
a clinical phase iii / iv trial endorsed by the german head and neck clinical trials group ( iag - kht ) will address differences in locoregional control and acute / late toxicities between the two techniques . compliance with ethical guidelines conflict of interest c . 
budach state that there are no conflicts of interest . this study was approved by the institutional review board of the charit universittsmedizin berlin ( ea4 / 015 / 15 )  . strahlenther onkol ( 2016 ) 192 : 5562 doi 10.1007 / s00066 - 015 - 0909 - 0 undetected human papillomavirus dna and uterine cervical carcinoma association with cancer recurrence kae okuma hideomi yamashita terufumi yokoyama keiichi nakagawa kei kawana received : 29 may 2015 / accepted : 23 september 2015 / published online : 20 october 2015 springer - verlag berlin heidelberg 2015 abstract background the time course of human papillomavirus ( hpv ) dna clearance was studied in patients with carcinoma of the cervix during follow - up after primary radical radiotherapy ( rt )  . 
this study investigated the relationship between timing of hpv clearance and rt effectiveness . patients and methods a total of 71 consecutive patients who were treated for cervical cancer with primary radical radiotherapy and high - dose rate intracavitary brachytherapy with or without chemotherapy were enrolled in the study . 
diese studie untersuchte den zusammenhang zwischen dem zeitpunkt der hpv - eliminierung und der rt - effizienz . patienten und methoden insgesamt 71 aufeinanderfolgende patienten , die mit einer primren rt behandelt wurden , nahmen an der studie teil . 
die flle , bei denen keine hpv - dna entdeckt wurde , wurden auf einen zusammenhang zu rckfallfreiem berleben analysiert . original article 56 ergebnisse bei 13 patienten ( 18 % ) konnte keine hpvdna vor der rt festgestellt werden . 
von den 58 patienten , bei denen hpv - dna vor der behandlung identifiziert wurde , wurde die hpv - dna bei 34 % nicht whrend der behandlung und bei 66 % nicht nach der behandlung entdeckt . 
patienten , bei denen vor der behandlung keine hpv - dna identifiziert werden konnte , sollten sorgfltig nachbeobachtet werden und fr zustzliche oder alternative therapien in erwgung gezogen werden . keywords strahlentherapie hpv - clearance behandlungswirksamkeit zervikale neoplasien radiochemotherapie cervical cancer is one of the most common malignancies in japan . 
it has been reported that 95100 % of patients with invasive carcinoma of the cervix are infected with hpv [ 24 ]  . in the past , radical surgery was usually adopted in japan for cases up to stage iib ( figo , international federation of gynecology and obstetrics classification )  . 
 [ 5 ] reported that persistence of hpv deoxyribonucleic acid ( dna ) in the cervix at the end of irradiation in hpv - positive cervical carcinoma was highly predictive of local disease - free survival ( ldfs ) and overall survival ( os )  . 
also of interest was whether a change from negative to positive hpv status during the follow - up period after rt could be an indicator to predict local recurrence . materials and methods patients a total of 71 consecutive patients who were treated for cervical cancer with primary radical radiotherapy with or without chemotherapy at the university of tokyo hospital between december 2008 and november 2011 were evaluated . 
 external - beam radiation therapy ( ebrt ) consisted of whole pelvic irradiation of 30.639.6 gy in 1722 fractions and whole pelvic irradiation with midline block of 10.89.8 gy in 611 fractions ( 1.8 gy per fraction from monday to friday )  . 
whole pelvic irradiation was administered using a linear accelerator with four fields of a 10 mv photon beam ( two anteriorposterior opposed fields , and two lateral opposed fields ) and whole pelvic irradiation with a 4 cm wide midline block was administered using two anterior posterior opposed fields to reduce the dose to the rectum and the bladder . 
the clinical target volume ( ctv ) included all areas of gross and potentially microscopic disease , and included the upper half of the vagina , parametria , uterus , presacral region , and regional lymph node regions ( common , internal and external iliacs , and obturator regions )  . 
in about the first 32 patients , before the third and fourth treatment of hdricbt , biopsies of the cervix were taken from all patients and checked for residual malignant cells . 
 nineteen patients were treated with rt alone ( ebrt + icbt ) for the following reasons : patients with early stages , advanced age , poor renal or heart function , or refusal of chemotherapy . 
of these 52 patients , 25 patients received weekly cisplatin ( cddp ) of 3040 mg / m2 , 25 received tri - weekly nedaplatin ( ndp ; 80100 mg / m2 ) , and two received a paclitaxel and cddp regimen . 
response to radiotherapy was evaluated by pelvic examination , conventional cervical papanicolaou smear which was done in addition to the research samples , and review of tumor markers including serum squamous cell carcinoma ( scc ) antigen value and carcinoembryonic antigen ( cea )  . 
other imaging studies , such as mri , ultrasound , bone scintigraphy and positron emission tomography ( pet ) were not routinely performed . statistical analysis statistical analyses were performed using spss version 21.0. 
swab samples from the external os of the uterus were subjected to dna extraction with a qiaamp dna blood mini kit ( qiagen , venlo , the netherlands )  . 
briefly , a standard polymerase chain reaction ( pcr ) was conducted using the pgmy 09 / 11 l1 consensus primer sets [ 7 ] and human leukocyte antigen - dq ( hla - dq ) primer sets . 
of the 20 patients who had recurrence disease , hpv status did not change from negative to positive during the follow - up period after rt . the 3 - year cumulative disease - free survival ( dfs ) rate was 71 5.4 % for all 71 patients . 
 [ 14 ] investigated hpv status and e2 gene integrity as potential prognostic parameters for clinical outcome and prediction of rt response in 40 women with locally advanced cervical cancer treated with curative rt . 
for cervical carcinoma of the uterus , hpv infection induces cancerous changes of cervical cells through alterations in microrna expression patterns during consecutive stages of cervical cancer development and their association with chromosomal instability [ 17 ]  . 
in addition , whether hpv is detectable or not before treatment may be a biomarker of rt effectiveness for cervical carcinoma . conclusion the patients in whom hpv was not detected had the worst prognosis . 
kawana state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 3239 doi 10.1007 / s00066 - 015 - 0875 - 6 risk profile for osteoradionecrosis of the mandible in the imrt era gabriela studer marius bredell stephan studer gerhard huber christoph glanzmann received : 1 may 2015 / accepted : 2 july 2015 / published online : 12 august 2015 the author ( s ) 2015 . 
this article is published with open access at springerlink.com abstract background the risk for osteoradionecrosis ( orn ) of the mandible is positively related to bone volume exposed to > ~ 60 gy . 
we hypothesized that in combined treatment , surgery may also be a risk factor . patients and methods the impact of mandibular surgery on orn in locally disease - free imrt cohorts was retrospectively analyzed . results between october 2002 and october 2013 , 531 of 715 patients with oral cavity cancer ( occ ) , mesopharyngeal cancer ( mc ) , or salivary gland tumor were treated with the mandible bone exposed to ~ > 60 gy ( mean follow - up , 38 months ; 7143 months )  . 
huber , pd department of otorhinolaryngology , head neck cancer center , head and neck surgery , university hospital zurich , zurich , switzerland conclusion marginal or periosteal bone resection of the mandible was identified as the highest orn risk factor in our imrt cohort . keywords osteoradionecrosis , orn risk factors , orn preradiation surgery surgery - related orn postoperative orn risikoprofil fr osteoradionekrosen des kiefers in der imrt - ra zusammenfassung hintergrund das risiko fr die entwicklung einer kiefernekrose nach radiotherapie ( osteoradionekrose , orn ) korreliert bekanntlich mit dem knochenvolumen , das einer dosis von ~ > 60 gy ausgesetzt wurde . 
hypothese war , dass die chirurgie bei kombinierten therapien ebenfalls einen risikofaktor darstellt . material und methode der einfluss chirurgischer interventionen am kiefer auf das risiko einer orn wurde in unserem lokal krankheitsfreien imrt - kollektiv retrospektiv analysiert . ergebnisse zwischen oktober 2002 und oktober 2013 wurden 531 / 715 patienten mit mundhhlenkarzinomen ( occ ) , mesopharynxkarzinomen ( mc ) oder speicheldrsentumoren mit dosen > 60 gy am kieferknochen behandelt ( mittlere beobachtungszeit 38 monate ; spanne 7143 monate )  . 
die orn - rate nach definitiver imrt bei mc ( 16 / 227 ) und nach postoperativer imrt bei occ ohne chirurgischen eingriff am kieferknochen ( 3 / 46 ) belief sich auf je 7 % , bei occ - patienten mit operation am kieferknochen auf 29 % ( 15 / 60 ; p = 0 , 002 )  . 
this observation motivated us to analyze the impact of previous mandibular surgery on the risk for orn . our hypothesis was that pre - imrt surgery of the mandible may also be a risk factor for orn . patients and methods we retrospectively analyzed a single - center occ / mc / salivary gland tumor imrt cohort with respect to orn . 
the maximum dose ( dmax ) is defined as the highest dose in 1 % . details of the imrt schedules used have been provided in previous reports [ 10 , 11 ]  . systemic concomitant therapy if indicated , cisplatin was concomitantly given ( 40 mg / m2 / week )  . 
since april 2006 , cetuximab has been used for patients with contraindications for cisplatin chemotherapy ( 400 mg / m2 loading dose , followed by 250 mg / m2 1 day / week )  . 
age and / or comorbidity or early - stage disease were reasons not to add systemic therapy ( 15 % )  . follow - up all patients were regularly seen in our joint clinics 36 weeks after completion of imrt , at the departments of otorhinolaryngology and head and neck surgery or the department of craniomaxillofacial and oral surgery . 
 actuarial survival data were calculated using kaplanmeier curves and log - rank tests implemented in statview ; p values of < 0.05 were considered statistically significant . multivariate analysis was performed using the statview calculation program ( mantelcox log - rank test )  . 
 19 of 249 operated patients ( 7.6% , ns ; table 2 ) , suggesting an additional risk factor impacting the risk for orn other than radiation dose only . we observed 5 % ( 36 / 715 ) orn events of grade 14 in the entire cohort , and 7 % ( 36 / 531 ) in the cohort at risk ( table 2 )  . 
all orn events occurred in mandibles exposed to > 60 gy . grade 1 , 2 , 23 , 3 , and 4 orn events were observed in 2 , 5 , 21 , 4 , and 4 patients , respectively . of 36 orn events , eight ( 22 % ) developed as a consequence of invasive manipulation on previously with > 50 gy irradiated bone areas ( postintervention orn ) : four of eight events translated into complicated grade 4 orn ( pathological fracture , osteocutaneous fistula , osteomyelitis , persisting pain ) following segmental resection or limited surgery for orn . 
1 mandible bone dosevolume histograms ( mean values , cc ) of the following subgroups , all with the mandible exposed to > 60 gy ( n total = 458 ) : - postoperative imrt in oral cavity cancer ( occ ) patients with / without osteoradionecrosis ( orn ) who underwent mandibular surgery ( + ms ) or not ( ms ) - definitive imrt in occ patients ( no ms , all in the cohort without orn ) - definitive and postoperative imrt in mesopharynx cancer ( mc ) patients orn ( none of them underwent mandibular surgery )  . 
red curves represent the two cohorts with orn ( + orn ) , dotted lines postoperative imrt groups , and continuous lines definitive imrt groups 1 3risk profile for osteoradionecrosis of the mandible in the imrt era 36 fig . 
 figure 2 shows kaplanmeier survival curves for orn events following ( 1 ) definitive imrt in mc patients and ( 2 ) postoperative imrt in occ patients : most orn events occurred early after imrt completion , during the first 20 months . 
no ms ( 227 ) mc postop no ms ( 72 ) mc postop with ms ( 2 ) ( 1 segmental , 1 periosteal ) occ postop with ms ( 60 ) periosteal or marginal ( 33 ) segmental ( 27 ) ~ 115200 cc ~ 1710410 cc ~ 2315102.50 dvh dosevolume histogram , mc mesopharyngeal carcinoma , occ oral cavity cancer , postop postoperative imrt ( prescription dose 6066 gy ) , def . 
an orn rate ( grade 23 ) of 39 % was found for postoperative imrt patients at risk with floor of the mouth carcinoma or mandible infiltrating carcinoma who underwent previous periosteal or marginal mandibular resection ( table 3 )  . 
a plausible explanation for this finding is that the mandible is more dependent on the periosteum for its blood supply than on the inferior alveolar neurovascular bundle , especially in older individuals [ 12 ]  . 
in segmental resection cases the surgery is more extensive and mostly requires a composite free vascularized graft with a well - nourished bone flap with an unharmed periosteum and adequate soft tissue coverage . table 4 summarizes the orn rates of our mc / occ cohorts based on combined surgical and imrt - related risk parameters . 
17 % in 106 patients with postoperative occ is explained by ( a ) the lower dose to the bone ( dvh ) and ( b ) only 2 of 74 cases underwent mandibular surgery in the mc subgroup . 
poor outcome following definitive irradiation of occ also in the imrt era was previously reported ; however , data on this topic are scant [ 13 ] , which may partly be explained by a negative selection of occ patients referred for definitive radiation ( elderly , comorbid patients with large / inoperable tumors )  . 
for the small subgroup ( n = 14 ) who survived 2 years , we cannot exclude an orn rate of approximately 22 % ( according to the statistical " rule of three " to estimate the probability of adverse events in small sample sizes with few events , giving the upper limit of the 95 % confidence interval of the probability : 3 / 14 = 22 % )  . 1 3risk profile for osteoradionecrosis of the mandible in the imrt era 38 the positive relationship between radiation dosevolumes and the risk for orn is known , and the reduced orn risk by using mandible - sparing imrt techniques was confirmed in several reports [ 3 , 58 ]  . 
only scant information is available on the orn risk in the postoperative setting , which is characterized by lower radiation doses to the mandible than in the definitive radiation setting . 
table 5 gives an overview of the orn events in our patients related to the treatment sequence . korean researchers reported on occ / mc patients irradiated postoperatively with conventional three - dimensional radiation techniques . 
 [ 15 ] , who assessed 221 patients divided into the following groups : ( 1 ) parotidectomy only ; ( 2 ) parotidectomy with mastoidectomy ; and ( 3 ) parotidectomy with subtotal petrosectomy . 
this low susceptibility to orn may be partially explained by the fewer surgical interventions performed in this area , the absence of teeth , and adequate soft tissue coverage by the masticatory muscles . in summary , the following conclusions can be drawn from the present results : 1 . 
half the patients with postintervention orn developed grade 4 orn ( 4 / 8 ) conclusion periosteal or marginal mandibular resection was the statistically significantly highest orn risk factor , translating into a 39 % orn rate grade of 23 , vs . 
7 % following defini tive imrt or postoperative imrt with no or segmental resection . consequently , the radiation dose to the mandible should be minimized in patients at high risk for orn . open access this article is distributed under the terms of the creative commons attribution license which permits any use , distribution , and reproduction in any medium , provided the original author ( s ) and the source are credited . compliance with ethical guidelines conflicts of interest g . 
glanzmann state that there are no conflicts of interest . strahlenther onkol ( 2016 ) 192 : 4754 doi 10.1007 / s00066 - 015 - 0892 - 5 prognostic value of cxcl12 and cxcr4 in inoperable head and neck squamous cell carcinoma margret rave - frnk narges tehrany julia kitz martin leu hanne elisabeth weber peter burfeind henning schliephake martin canis tim beissbarth holger michael reichardt hendrik andreas wolff received : 24 june 2015 / accepted : 19 august 2015 / published online : 15 september 2015 springer - verlag berlin heidelberg 2015 abstract its receptor objective the chemokine cxcl12 and cxcr4 can affect tumor growth , recurrence , and metastasis . 
we tested the hypothesis that the cxcl12 and cxcr4 expression influences the prognosis of patients with inoperable head and neck cancer treated with definite radiotherapy or chemoradiotherapy . methods formalin - fixed paraffin - embedded pretreatment tumor tissue from 233 patients with known hpv / p16ink4a status was analyzed . 
cxcl12 and cxcr4 expressions were correlated with pretreatment parameters and survival data by univariate and multivariate cox regression . results cxcl12 was expressed in 43.3 % and cxcr4 in 66.1 % of the samples and both were correlated with hpv / p16ink4a positivity . 
this may recommend cxcr4 as therapeutic target for combating head and neck cancer metastasis . keywords head and neck cancer squamous cell cancer chemokines radio ( chemo ) therapy prognosis m . 
reichardt institute for cellular and molecular immunology , university medical center gttingen , 37099 gttingen , germany original article 48 prognostischer stellenwert von cxcl12 und cxcr4 bei inoperablen kopf - hals - tumoren zusammenfassung hintergrund das chemokin cxcl12 und sein rezeptor cxcr4 beeinflussen tumorwachstum , auftreten von rezidiven und metastasierung . 
es wurde die hypothese geprft , dass ein zusammenhang der cxcl12und cxcr4 - expression mit der prognose von patienten bestehe , die wegen eines inoperablen kopf - hals - tumors eine primre radio oder radiochemotherapie erhielten . 
die cxcl12und cxcr4expression wurde mit klinischen parametern und berlebensdaten mittels uniund multivariater cox regression analysiert . ergebnisse cxcl12 wurde von 43 , 3 % , cxcr4 von 66 , 1 % der tumoren exprimiert , und beide marker korrelierten mit einer hpv / p16ink4a - expression . 
eine hohe cxcl12 - expression war mit einem verbesserten gesamtberleben ( p = 0 , 036 ) , eine hohe cxcr4 - expression mit einem reduzierten fernmetastasenfreien berleben ( p = 0 , 034 ) assoziiert . schlussfolgerung eine hohe cxcr4 - expression erscheint auch fr patienten mit inoperablen kopf - hals - tumoren als negativer prognostischer faktor , weil es metastasierungsprozesse frdert . 
eine gezielte unterdrckung der cxcl12 - / cxcr4 - signalwege kann eine mglichkeit zur reduktion der metastasierung sein . schlsselwrter kopf - hals - plattenepithelkarzinom plattenepithelkarzinome chemokin radio ( chemo ) therapie prognose despite the use of surgery , chemotherapy , and radiotherapy , the 5 - year survival rates for head and neck squamous cell carcinoma ( hnscc ) are below 50 % . 
moreover , human papilloma virus ( hpv ) - related tumors are more responsive to therapy than tumors related to the traditional risk factors smoking and alcohol consumption [ 1 ]  . 
although hnscc is often regarded as a locoregional disease , in the end distant metastases determine the patients prognosis [ 2 ]  . the tumor microenvironment plays a decisive role in cancer development and treatment outcome . 
the chemokine cxcl12 ( sdf - 1 ) and its main receptor cxcr4 have been identified as one of the key players because they affect tumor growth , tumor recurrence , metastasis , vascular formation , and therapy resistance [ 3 , 4 ]  . 
to date an interaction between cxcr4 / cxcl12 and hpv status has not been clarified . clinically , the role of the cxcl12 / cxcr4 axis in hnscc has been investigated in some smaller studies , and for the subgroup of oral squamous cell carcinoma ( oscc ) a correlation between cxcr4 expression and overall survival ( os ) [ 57 ] as well as a correlation between cxcr4 expression and lymph node or distant metastasis was described [ 5 , 710 ]  . 
the expression of cxcl12 was found to be higher in metastatic lymph nodes than in the primary tumor [ 9 ] , and the intratumor cxcl12 level correlated with the os [ 11 ]  . the present study focused on the expression and prognostic value of cxcl12 and cxcr4 in a well - defined cohort of 233 patients with inoperable hnscc treated with definite radiotherapy ( rt ) or chemoradiotherapy ( crt )  . patients and methods study cohort a search of clinical records and pathology archives identified 233 patients with primary inoperable hnscc without distant metastasis at diagnosis who were treated at a single institution . 
we included all patients with untreated , pathologically confirmed hnscc with union for international cancer control ( uicc ) stages ii , iii , or iv of the oral cavity , oropharynx , hypopharynx , or larynx . 
patients with metastatic disease or previously treated for another cancer were excluded . the patients hpv status was determined by pcr analysis and by the surrogate parameter p16ink4a [ 12 ]  . 
for 138 patients , from june 1994 to november 1999 normofractionated definite rt ( 2 gy / day , 5 times / week ) was delivered as parallel - opposed lateral portals . 
for 45 patients , from december 1999 to october 2008 , normofractionated ( 2 gy / day , 5 times / week ) 3d conformal external - beam rt was given , the total dose being 70 gy in each case [ 14 ]  . 
for 50 patients , from november 2008 to november 2011 , an integrated intensity - modulated radiotherapy ( imrt ) with single fractions of 2.2 gy to the primary tumor and involved lymph nodes up to 66 gy and single fractions of 1.8 gy to the drainage sites on both sides m . 
rt was supplemented by a concomitant chemotherapy for 171 patients , which either consisted of 5 - fluorouracil plus mitomycin c or of cisplatin only . patient follow - up after therapy , remission was evaluated by means of a clinical earnosethroat examination and contrast - enhanced computed tomography ( ct )  . 
biopsy specimens were taken from suspect findings to receive histologic confirmation of tumor ( re ) growth . immunohistochemistry immunohistochemical staining of cxcr4 and cxcl12 was performed on ffpe tissue samples from pretreatment tumor biopsies . 
a standardized immunohistochemical staining technique was performed using rabbit - anti - cxcr4 ( ab2074 ; dilution 1 : 500 ; abcam , cambridge , uk ) and human / mouse - anti - cxcl12 ( clone #79018 ; dilution 1 : 50 ; r&d systems , abingdon , uk ) antibodies on a ventana benchmark xt immunostainer ( ventana , tucson , az )  . 
the antibodies were incubated at 37 c for 32 m the staining reaction was visualized by means of horseradish peroxidase with the ultraview universal dab detection kit ( ventana medical systems ) and hematoxylin solution ( gill 3 , sigma aldrich , munich , germany ) for counterstaining . 
the individual weighted labeling score for cxcr4 and cxcl12 results from the addition of the products of the percentage of positive tumor cells multiplied by their staining intensity , thus scores from 0 ( no positive tumor cell ) to 300 ( 100 % intensely stained tumor cells ) could be found . 
the individual labeling scores served for correlation analyses with clinicopathological parameters and patient survival . statistical analysis survival times were calculated from the day of histologic diagnosis until the end of study . 
the kaplanmeier method was used to estimate os , disease - free survival ( dfs ) , locoregional control rates ( lrc ) , and distant metastasisfree survival ( dmfs )  . 
furthermore , an additional multivariate analysis ( multivariate cox regression ) was performed to test that the association between marker expression and survival was independent of other possible prognostic factors or factors that may influence treatment outcome , which may bias the univariate analysis . 
at the end of the analysis , 185 of 233 patients ( 79.4 % ) had died and collectively the 5and 10 - year os rates were 22 and 15 % , respectively . 
we further tested whether commonly used predictors for distant metastasis such as the primary tumor site , t and n status , or histological grading correlated with dmfs , but we found no significant associations ( table 2 )  . 
in the multivariate setting , a high cxcr4 score remained significantly correlated with a reduced dmfs ( p = 0.041 , table 3 ) , while os was only associated with p16ink4a positivity ( p = 0.034 , table 4 )  . 
since no expression or a very low expression with a score of 10 was detected in about one third of the patients ( n = 79 , 33.9 % ) , a trisection of the data was performed . 
in the case of cxcl12 , the pretreatment parameters tumor localization ( 84.1 % negative for oral cavity ) and n status ( > 70 % negative for n0 , n1 ) were significantly associated with an existing expression . 
moreover , we noticed a significant increase of cxcl12 positivity with increasing n status ( see table 1 )  . correlations with survival data when analyzing the patients survival we found no significant correlations between cxcr4 expression and os , dfs , or local recurrence - free survival ( lrfs )  . 
2 distant metastasis - free survival ( a ) and disease - free survival ( b ) according to low , medium , and high cxcr4 expression in pretreatment biopsies of patients with hnscc treated with radiotherapy or radiochemotherapy fig . 
4 box plots summarizing immunohistological scores for cxcr4 and cxcl12 stratified by p16ink4a positivity discussion the cxcl12 / cxcr4 axis plays multiple roles in hnscc by influencing tumor growth [ 15 ] , angiogenesis [ 16 ] , metastasis [ 6 , 11 , 17 ] , and patient survival [ 4 , 11 ]  . 
in the present study , immunohistochemistry was used to analyze the expression of cxcl12 and cxcr4 with respect to the clinicopathological characteristics and survival data of 233 hnscc patients treated with definite rt or rct . 
 [ 5 ] studied 56 patients with oscc and found that cxcr4 positivity was an independent factor for cause - specific death . the underlying mechanism of increased cxcr4 expression in hnscc and the relation to enhanced tumor metastasis and inferior patient survival are generally ascribed to diverse factors , including emt ( epithelialmesenchymal transition ) induction and activation of matrix metalloproteinases . 
reported that the cxcr4 expression in oral oscc cells was up - regulated by cxcl12 and transforming growth factor 1 in a snail - dependent manner [ 19 ] , which is also an emt promoting transcription factor . 
another important cxcr4 regulating factor is hypoxia , which is common in hnscc , and may induce the enhanced expression of cxcr4 via activation of hypoxia - inducible factor - 1 [ 20 ]  . 
clinical and experimental evidence for the relationship between cxcr4 expression and tumor cell migration or tumor metastasis already led to the assumption that cxcr4 targeting by monoclonal antibodies or small molecule inhibitors could become an efficient strategy for treating human cancer metastasis , and the first clinical trials are ongoing [ 3 , 21 ]  . to our knowledge , data on the herein described correlation between high cxcr4 expression and p16ink4a / hpv tumor positivity have not been published to date . 
however , patients with whim ( warts , hypogammaglobulinemia , infections , and myelokathexis ) syndrome , an autosomal dominant disease caused by a gain of function mutation in cxcr4 , show increased susceptibility to hpv infections [ 22 ]  . 
whim manifests as cutaneous warts , cervical dysplasia , and squamous carcinoma in women , and the incidence of hpv - related ssc of the oral cavity in two relatives with whim syndrome has been described [ 23 ]  . 
the mutations present in whim patients probably result in enhanced cxcr4 signaling and an increase of the normal adhesionpromoting function of cxcr4 , which is consistent with the increased cxcr4 expression of patients with distant metastases as described here . clinical studies addressing the association between cxcl12 and patient outcome are still scarce . 
furthermore , in a gene expression study by these authors [ 24 ] higher expression levels of genes involved in cxcl12 signaling were observed in the group with better prognosis . 
in the case of hnscc , it was suggested that high cxcl12 expression in the primary tumor or in the tumor microenvironment suppresses the cxcr4 - driven chemotactic migration of tumor cells toward distant tissues expressing cxcl12 [ 4 , 24 ]  . 
therefore , it is also conceivable that due to the strong correlation between cxcl12 and p16ink4a expression , the positive prognostic value of cxcl12 simply mirrors the well - known advantageous effect of p16ink4a expression on patient survival [ 25 ]  . prognostic value of cxcl12 and cxcr4 in inoperable head and neck squamous cell carcinoma1 3 54 conclusion in summary , we have presented clinical data underscoring the prognostic value of cxcr4 in hnscc patients treated with rt or rct . 
the association between inferior dmfs and high cxcr4 expression is not only useful in estimating the prognosis but also recommends the cxcl12 / cxcr4 axis as a novel therapeutic target for treating hnscc metastasis . compliance with ethical guidelines conflict of interest m . 
wolff state that there are no conflicts of interest . strahlenther onkol ( 2016 ) 192 : 2531 doi 10.1007 / s00066 - 015 - 0902 - 7 hedgehog pathway inhibitor in combination with radiation therapy for basal cell carcinomas of the head and neck first clinical experience with vismodegib for locally advanced disease bjrn schulze markus meissner shahram ghanaati iris burck claus rdel panagiotis balermpas received : 21 august 2015 / accepted : 15 september 2015 / published online : 8 october 2015 springer - verlag berlin heidelberg 2015 abstract background definitive radiotherapy and vismodegib , an oral inhibitor of the hedgehog pathway , are both established treatment options for locally advanced basal cell carcinomas ( bcc )  . 
both have shown good results in local tumor control ; however , the effects concerning advanced tumors are often not of a lasting nature and to date no systematic data about the combination of the two modalities are available . patients and methods we retrospectively analyzed four patients who received vismodegib and radiotherapy in combination . 
vismodegib was taken once a day ( 150 mg ) during the entire time of irradiation and beyond upon instructions of the attending dermatologist . results in three cases a persistent complete response was observed , in one case the tumor remained stable for approximately 6 months until further tumor progression was documented . 
rdel , md department of radiation oncology , university hospital johann wolfgang goethe university , theodor stern kai 7 , 60590 frankfurt , germany e - mail : panagiotis.balermpas@kgu.de inhibitor der hedgehog - signalkaskade in kombination mit bestrahlung beim basalzellkarzinom der kopfhals - region erste klinische erfahrungen mit vismodegib bei lokal fortgeschrittener erkrankung m . 
burck , md department of diagnostic and interventional radiology , university hospital johann wolfgang goethe university , frankfurt , germany zusammenfassung hintergrund sowohl definitive radiotherapie als auch vismodegib , ein oraler inhibitor der hedgehog - signalkaskade , sind etablierte behandlungsoptionen fr lokal fortgeschrittene basalzellkarzinome ( bcc )  . 
beide therapien zeigen fr sich gute ansprechraten , aber die lokale tumorkontrolle ist oft nicht dauerhaft und bis heute existieren kaum daten ber eine kombination der beiden modalitten . patienten und methoden wir analysierten retrospektiv vier patientenflle nach simultaner applikation von vismodegib und bestrahlung . 
vismodegib wurde einmal tglich ( 150 mg ) ber die gesamte radiotherapie und nach deren beendigung , je nach empfehlung des betreuenden dermatologen , eingenommen . ergebnisse in drei fllen konnte ein lnger andauerndes ansprechen beobachtet werden . 
knftige studien sollten den stellenwert dieser kombinierten therapie untersuchen . schlsselwrter basalzellkarzinom bestrahlung vismodegib hedgehog - pathway kombinationstherapie basal cell carcinomas ( bcc ) are one of the most common cancers worldwide and account for approximately 80 % of all non - melanoma skin cancers . 
the incidence rates vary between 100 per 100 , 000 in europe and 300 per 100 , 000 people in australia , indicating that exposure to ultraviolet radiation is the strongest risk factor for its development [ 1 ]  . aggressive local infiltration into neighboring structures is the main feature of these tumors , whereas distant spread is rare [ 2 ]  . 
external beam radiotherapy ( rt ) is an effective treatment option for recurrent , incompletely resected , or otherwise inoperable tumors , especially when surgical resection would lead to an unacceptable craniofacial mutilation . 
rt provides local control rates in the range of 85100 % , and is associated with a good cosmetic outcome [ 38 ]  . in 2012 and 2013 , vismodegib , a novel oral therapeutic agent for the treatment of locally advanced or metastasized bcc , was approved by the american food and drug administration ( fda ) and the european medicines agency ( ema ) for lesions not amenable to surgery and / or rt . 
the median duration of response was 9.6 months in patients with locally advanced bcc [ 9 ]  . the hedgehog pathway vismodegib is a small - molecule inhibitor of the hedgehog signaling pathway that is abnormally activated in about 90 % of all bccs . 
the most common reason for its aberrant activation is a loss of ptch1 , the hedgehog membrane receptor , which normally inhibits smo as the main signal transducer [ 12 ]  . possible interactions between rt and the hedgehog pathway are not fully explored . 
both preclinical and clinical data showed that inhibition of the hedgehog pathway radiosensitizes cancer cell lines and murine models [ 14 ] , whereas hedgehog activation correlates with poorer outcome in patients undergoing rt . 
this has been shown for a variety of human malignancies , including esophageal , cervical , and head and neck squamous cell carcinoma [ 1517 ]  . because vismodegib has not been approved for combined application with rt , clinical experience with this bimodal regimen is rare , and only three cases of combined therapy with vismodegib and rt have been published in the current literature to date [ 18 , 19 ]  . 
the combination of small - molecule inhibitors and rt has already shown enhanced efficacy in the treatment of other malignancies , i.e. , squamous cell carcinoma of the head and neck [ 20 ]  . 
however , unexpected side effects were observed in some cases [ 21 , 22 ]  . patients and methods we report four cases of patients with locally advanced inoperable bcc of the head and neck region who received vismodegib during and after definitive rt within the scope of a compassionate - use progradetailed patient and treatment characteristics are given in table 1 . 
to exclude patients with distant metastases , pretherapeutic tumor stagingincluding computer tomography ( ct ) scans of the head and neck as well as the thorax or conventional chest x - ray and abdominal ultrasound was performed . 
all patients were informed about the individual character of this treatment combination , and written informed consent was obtained from each patient before start of treatment . external electron - beam or mixed - beam rt was delivered by a linear accelerator with energies of 6 mev in each case . 
 ( m ) 66 ( 2 / fr ) gy 6 months disease control m male , f female , fr fraction , cr complete remission , pd progressive disease . afollow - up calculated from begin of radiotherapy to last patient contact . stable , then pd thermoplastic immobilization mask of the head were used to guarantee reproducible accuracy and precision of beam delivery . 
follow - up intervals were calculated from start of rt to last patient contact . results case 1 a 71 - year - old male patient with a recurrent bcc of the left facial skull was referred to our hospital . 
during rt no extraordinary acute side effects were noted . two months after completion of rt , re - staging ct scans showed stable disease with a mostly unaltered osseous 3 . 
 ( f ) 55 ( 2.75 / fr ) gy 3 months destruction and extensive tissue defects of the left nasal cavity , the nasal soft tissue , and the left maxillary sinus . 
six months after rt , putative local progression was diagnosed via ct and mri scans ; however , repeat biopsies from the left nasal cavity did not confirm bcc malignancy . 
owing to the lack of other therapeutical alternatives , continuation of vismodegib was recommended by our dermato - oncological tumor board , and currently the patient is being closely monitored by the department of facial surgery . case 2 a 57 - year - old male patient with a late relapse of a bcc of the right cheek / nasolabial fold underwent definitive rt in combination with vismodegib ( 66.0 gy in single fractions of 2.0 gy per day )  . 
at 6 moths after rt , the only notable sequela was a mild epiphora of the ipsilateral eye , which did not impair any activities of daily living . hedgehog pathway inhibitor in combination with radiation therapy for basal cell carcinomas of the head1 3 28 fig . 
a biopsy showed no evidence of residual disease case 3 an 80 - year - old male patient with a locally advanced bcc of the right temple with extension to the ipsilateral parotid region was referred to our hospital . 
reconstructive surgery with a musculocutaneous flap was highly recommended but was rejected by the patient . case 4 a 78 - year - old female patient with recurrent bcc of the facial area and the right earlobe and auditory channel underwent multiple tumor excisions within the last 3 years until rt in combination with concurrent vismodegib for a recurrent tumor of the right earlobe was started . 
in one case , clinical examination and imaging during the last follow - up visit gave no indications of a residual tumor so that there was no reason to perform another biopsy . 
in a core biopsy , however , no vital tumor tissue could be detected . side effects / adverse events radiodermatitis occurred in all four cases but only in one patient was a severe grade - 3 skin reaction observed . 
one patient , whose bcc was located next to the right eye , developed a persistent blepharitis and epiphora , which was still ongoing at the last follow - up visit . 
in all , 50 % of the patients reported muscle spasms that were always mild and needed no specific therapy except an oral substitution of magnesiu in one case , osteoradionecrosis ( orn ) of the manb . 
3 magnetic resonance images ( t1 with intravenous contrast agent ) of a 78 - year - old patient with a recurrent bcc of the right auditory channel before ( top ) and 3 months after ( bottom ) combined therapy with radiotherapy and vismodegib ( case 4 )  . 
clinical examinations provided no evidence of residual disease discussion there are hardly any published data on experiences about the feasibility and effectiveness of combining rt with the hedgehog inhibitor vismodegib for patients with bcc . 
 showed that rt doses above 102.6 gy were significantly associated with osteoradionecrosis [ 23 ] .thus , this late side effect is likely due to rt alone , and not attributable to the combination of rt and vismodegib . these toxicity results are in line with two other case reports in the literature where patients with advanced bcc were treated with vismodegib and rt [ 18 , 19 ]  . 
similarly , lasting local control could be achieved in a patient who received vismodegib as an induction therapy followed by rt [ 19 ]  . in recent years , the implementation of vismodegib , a small - molecule inhibitor of the hedgehog pathway , enhanced the therapeutic options for advanced bcc [ 24 , 25 ]  . 
2 computed tomography images with intravenous contrast agent of an 80 - year - old patient with inoperable , ulcerated bcc of the right cheek before ( top ) and 6 weeks after ( bottom ) combined therapy with radiotherapy and vismodegib ( case 3 )  . 
a detailed list of all observed side effects and adverse events is given in table 2 . hedgehog pathway inhibitor in combination with radiation therapy for basal cell carcinomas of the head1 3 30 table 2 observed side effects and adverse events during combined treatment and vismodegib maintenance therapya observed side effects and adverse events time of occurrence sequelae severity according to ctcae total 1 / 4 ( 25 % ) 1 / 4 ( 25 % ) 4 / 4 ( 100 % ) 2 / 4 ( 50 % ) 1 / 4 ( 25 % ) 2 / 4 ( 50 % ) 1 / 4 ( 25 % ) grade 1 / grade2 1 / 4 ( 25 % ) 1 / 4 ( 25 % ) 3 / 4 ( 75 % ) 2 / 4 ( 50 % ) 1 / 4 ( 25 % ) ctcae n.a. alopecia dysgeusia radiodermatitis mucositis blepharitis / epiphora muscle spasms osteoradionecrosis of the jaw prostate cancer ctcae common terminology criteria for adverse events , n.a. 
because of the small number of patients and the relatively short follow - up in the present study , no valid conclusions about tumor control rates and survival can be made . 
furthermore , three of the four patients ( 75 % ) had recurrent bcc , which is generally associated with worse prognosis compared with primary tumors . in a recently published large interim analysis of the stevie trial [ 26 ] , the response rates were similar to the already published data , but serious adverse events were recorded in 22 % ( 108 of 499 ) of the patients . 
the authors observed that the rate of these adverse events increased with prolonged exposure times to vismodegib , but , in most cases , ceased after discontinuation of the drug . 
the limited duration of response following vismodegib therapy , and the significant rate of adverse events after prolonged application , both provide a good rationale for a combined modality therapy , which could increase response rates and possibly shorten the need for drug continuation . conclusion against this background we suggest that a combination therapy consisting of rt and inhibition of the hedgehog pathway by vismodegib could lead to higher and longerlasting remissions . 
future randomized phase iii trials should then be conducted to test a possible superiority of the combined modality strategy over radiotherapy or vismodegib alone . compliance with ethical guidelines conflict of interest b . 
balermpas state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
no underage patients were included . strahlenther onkol ( 2016 ) 192 : 4046 doi 10.1007 / s00066 - 015 - 0886 - 3 hyperfractionated stereotactic reirradiation for recurrent head and neck cancer jakub cvek lukas knybel eva skacelikova jiri stransky petr matousek karol zelenik oldrich res bretislav otahal lukas molenda david feltl received : 15 april 2015 / accepted : 31 july 2015 / published online : 28 august 2015 springer - verlag berlin heidelberg 2015 abstract purpose the goal of this work was to evaluate the efficacy and toxicity of hyperfractionated stereotactic reirradiation ( re - rt ) as a treatment for inoperable , recurrent , or second primary head and neck squamous cell cancer ( hnscc ) that is not suitable for systemic treatment . patients and materials forty patients with recurrent or second primary hnscc were included in this study . 
performance status and gtv proved to be significant prognostic factors regarding local control and survival . conclusion hyperfractionated stereotactic re - rt is a reasonable treatment option for patients with recurrent / second primary hnscc who were previously exposed to high - dose irradiation and who are not candidates for systemic treatment or hypofractionation . keywords stereotactic radiotherapy squamous cell carcinoma of the head and neck reirradiation overall survival toxicity hyperfraktionierte akzelerierte stereotaktische wiederbestrahlung von rekurrierten kopf - hals - karzinomen zusammenfassung ziel ziel der studie war es , die effektivitt und toxizitt der hyperfraktionierten akzelerierten stereotaktischen wiederbestrahlung ( re - rt ) fr die behandlung von patienten mit lokalrezidiv von fortgeschrittenen kopf - hals - tumoren ( head and neck squamous cell cancer , hnscc ) , die fr eine systemische therapie nicht geeignet sind , zu untersuchen . 1 3original article patienten und methodik in die studie wurden 40 patienten mit rekurrierten oder sekundren hnscc eingeschlossen . 
die behandlung musste 95 % des planungszielvolumens ( ptv , definiert als makroskopisches tumorvolumen [ gtv ] + 3 mm zur bercksichtigung der mikroskopischen streuung , ohne zustzlichen saum ) abdecken.unbeteiligte lymphknoten wurden nicht bestrahlt . ergebnisse alle patienten absolvierten die behandlung plangem ( mediane behandlungsdauer 11 tage ; spanne 914 tage )  . 
 patientenstatus und gtv waren signifikante prognostische faktoren fr die lokale tumorkontrolle und das berleben . schlussfolgerung hyperfraktionierte akzelerierte stereotaktische re - rt ist eine interessante wahl fr patienten mit rekurrierten oder sekundren hnscc , die fr eine systemische therapie nicht geeignet sind . schlsselwrter stereotaktische strahlentherapie plattenepithelkarzinom der kopf - hals - region wiederbestrahlung gesamtberleben toxizitt despite advancements in treatment of patients with advanced head and neck squamous cell carcinoma ( hnscc ) , including altered radiation fractionation and the addition of chemotherapy regimens to radiation therapy , treatment outcomes remain poor [ 1 ]  . 
most relapses occur within the first 2 years after the primary treatment , and 96 % of these local or regional failures are located inside the 95 % isodose lines . 
salvage therapy using external beam re - irradiation ( re - rt ) has been used rather infrequently in the past due to concerns about potential toxicity [ 1 ]  . 
in 2001 , the rtog 9610 trial observed 7 % grade 5 ( fatal ) toxicity and 15 % grade 4 acute toxicity [ 5 ] ; however , with the advent of new technologies , there is now renewed interest in re - rt . stereotactic body radiotherapy ( sbrt ) may be an appropriate option for re - rt in the head and neck region , due to its ability to deliver a high dose to a limited target volume in a short amount of time [ 6 , 7 ]  . 
in patients treated with re - rt , almost all of the locoregional recurrences occur within the reirradiated recurrent gross tumor volume ( rgtv ) , despite efforts made to avoid prophylactic radiotherapy ( rt ) of tissue that is at risk of subclinical disease , which underscores the importance of minimizing the volume of reirradiated tissue [ 8 ]  . 
approaches that decrease the daily dose and increase the number of radiation treatments , while still maintaining the precision of stereotactic radiotherapy , may be desirable options to reduce late toxicity [ 9 ]  . 
brachytherapy ( bt ) has been used in treatment of recurrent head - and - neck cancer with impressive outcomes [ 10 ] , but technical and anatomical constraints limit its scope of use . the purpose of this study was to evaluate the toxicity and efficacy of hyperfractionated stereotactic re - rt as a salvage treatment for head and neck cancer in terms of overall survival ( os ) , local control , and complications . 
to the best of our knowledge , this is the first study of the use of hyperfractionated sbrt to treat head and neck cancer . materials and methods a total of 40 patients with hnscc were included in this study between november 2011 and july 2014 . 
contraindications to chemotherapy were the following : low performance status ( 13 patients , 33 % ) , low liver functions ( 11 patients , 28 % ) , low kidney functions ( 9 patients , 23 % ) , low cardiac and / or pulmonary function ( 7 patients , 18 % )  . 
the primary radiotherapy dose was higher than 60 gy , and the time gap between primary treatment and the start of re - rt was greater than 9 months for all patients . 
no adjuvant therapy was used , including chemotherapy , hyperthermia , and external - beam radiation . this study was approved by the local institutional review board ( university hospital ostrava )  . 
patients whose disease progressed after sbrt were provided best supportive care . treatment planning the target volume was defined based on simulation using ct images combined with magnetic resonance imaging ( mri )  . 
the planning target volume ( ptv ) was defined as the radiographic gross tumor volume ( gtv ) plus a 3 mm marg during treatment , repeated pairs of orthogonal x - ray images were used to provide on - line image guidance based on the skull base ( 20 % ) or cervical spine ( 80 % )  . dose prescription treatment was provided using a linear accelerator with 6 mv photons . 
the median duration of treatment was 28 min ( range 1752 min )  . evaluation of toxicity and response the analysis was performed after a median follow - up of 12 months ( range 336 months )  . 
the rtog / eortc scale was also used for scoring of late toxicity . statistical analysis dose - limiting toxicity was defined as toxicity that required interruption of the course of rt due to the intolerance . 
other parameters that were evaluated included the incidence and duration of acute toxicity , incidence of late toxicity , local progression - free survival ( l - pfs ) , metastatic progressionfree survival ( m - pfs ) , and overall survival ( os )  . initial patient characteristics were recorded at the start of re - rt . 
the incidence of mucosal grade 3 acute toxicity was 37 % ( oral cavity and / or pharynx ) , and the recovery time was 4 weeks for all of these patients . 
in 4 cases ( 21 % ) , patients were hospitalized to provide parenteral support for severe mucositis . there was 0 % incidence of grade 3 acute toxicity of sk no grade 4 or 5 toxicities were recorded . 
neither carotid blowout syndrome nor any other grade 3 or 4 late toxicity was observed . outcomes the entire treatment schedule was completed as planned for all patients ( median duration 11 days , range 914 days )  . 
the median maximal dose to the spinal cord was 9 gy ( range 021 gy )  . during follow - up , 14 patients ( 35 % ) showed disease progression , of which 4 cases ( 10 % ) involved distant metastasis . 
dose of primary radiotherapy , time to re - rt and history of surgery were found to not be significantly predictive of os . discussion the treatment of recurrent hnscc in previously irradiated patients remains a therapeutic challenge . 
several studies have demonstrated that re - irradiation ( > 60 gy ) is a feasible and effective alternative option , using a variety of techniques and fractionation schedules in carefully selected patients [ 14 ] , and subset analysis indicates that an increased total dose correlated with increased local control and survival [ 15 ]  . 
 the effectiveness of sbrt has been demonstrated , but concern exists that the high dose per fraction could cause considerable treatment - related morbidity and mortality [ 16 , 17 ]  . 
to our knowledge , this is the first study of the use of hyperfractionated sbrt for treatment of recurrent / second primary hnscc . in this study , the incidence of grade 3 acute mucositis was 37 % , and the median and maximum duration of confluent mucositis were 19 days and 4 weeks , respectively . 
 [ 18 ] , who first reported on the use of frameless sbrt for treatment of recurrent hnscc ; in this pioneering work no acute grade 4 or 5 toxicities or long - term adverse events were observed . 
 [ 19 ] observed grade 3 mucosal toxicity in only 7 of 56 patients ( 13 % ) ; however , this patient group was different with respect to tumor burden . 
although it is generally believed that large arteries are relatively resistant to radiotherapy , there are some reports of fatal hemorrhage or occlusion of large vessels resulting from treatment [ 20 ]  . 
we did not observe such complications in our study , probably because of the low dose used per fraction . in our group of heavily pretreated patients , the 1 - year and 2 - year l - pfs were both 44 % . 
in previous studies using a reirradiation dose ranging from 20 to 30 gy in 5 fractions , the 2 - year local control ( lc ) obtained was 26 % . 
n at risk number at risk in 200 - day increments of up to 3039 gy in 3 fractions , but this schedule could be considered too hot . comparison between the use of sbrt and brachytherapy favors the latter treatment method . 
there are two possible explanations for the better effectiveness observed with bt : ( 1 ) the dose inhomogeneity typical of bt produces higher equivalent uniform dose , and ( 2 ) the target volumes of typical brachytherapy patients is much smaller than those of patients treated with external beam rt . os is a better indicator of the treatment outcome in patients with recurrent hnscc cancers , because it reflects the cumulative effect of both lc and treatment toxicity . 
in the rtog 9610 phase ii trial comparing external beam radiation to 60 gy with concurrent 5 - fluorouracil and hydroxyurea chemotherapy , the median os observed was 8.2 months and the estimated 1 - year survival rate was 41.7 % [ 5 ]  . 
this is in agreement with previous reports observing that significantly improved clinical outcomes are associated with doses above 35 gy and tumor volumes below 25 ml [ 18 ]  . although our study is limited by its retrospective nature and its small patient population , it still demonstrates that re - rt can be curative in patients with good performance status who have small tumors . 
further improvement might be expected after incorporation of improved systemic therapy into the treatment regimen [ 24 ]  . 1 3hyperfractionated stereotactic reirradiation for recurrent head and neck cancer 46 conclusion hyperfractionated sbrt is a reasonable treatment option for patients with inoperable recurrent / second primary hnscc who were previously subjected to high - dose irradiation and who are not suitable candidates for systemic treatment or hypofractionation . 
longer survival could be expected in patients with good performance status who have small tumors . acknowledgment institutional supportrvo - fnos / 2012was re ceived for this work . compliance with ethical guidelines conflicts of interest j . 
feltl state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 7274 doi 10.1007 / s00066 - 015 - 0921 - 4 abskopale effekte der lokalen radiotherapie in kombination mit systemischer immuntherapie bei patienten mit metastasierten soliden tumoren cdric panje matthias guckenberger online publiziert : 6 . 
november 2015 springer - verlag berlin heidelberg 2015 hintergrund abskopale effekte im sinne eines tumoransprechens auerhalb des bestrahlungsfelds bei patienten mit metastasierten malignomen gelten als immunvermittelte reaktion , wurden jedoch bei alleiniger radiotherapie nur uerst selten beobachtet und bisher nicht systematisch untersucht . 
ging erstmalig prospektiv der hufigkeit abskopaler effekte bei fokaler radiotherapie in kombination mit systemischer applikation des granulozyten - makrophagen - kolonie - stimulierenden faktors ( gm - csf ) nach , einem aktivator der dendritischen zellen [ 1 ]  . patienten und methoden in einem zweistufigen prospektiven studiendesign wurden zwischen 2003 und 2012 insgesamt 41 patienten eingeschlossen , die bei verschiedenen metastasierten soliden tumoren unter palliativer hormonoder chemotherapie einen stabilen verlauf oder einen progress zeigten . 
die patienten erhielten zustzlich zur fortfhrung der chemotherapie eine 2 - wchige fokale radiotherapie mit 10 3 , 5 gy sequenziell an zwei verschiedenen lsionen ; diese wurde jeweils ab der zweiten bestrahlungswoche von einer tglichen subkutanen applikation von gm - csf ber 2 wochen begleitet . 
alle patienten hatten mindestens eine weitere ( dritte ) metastase , die keine fokale therapie erhielt und zur evaluation des abskopalen ansprechens genutzt wurde . ergebnisse der primre endpunkt des abskopalentumoransprechens wurde bei 26 , 7 % der patienten erreicht . 
 unter kombinierter radiotherapie , chemotherapie und gmcsf - applikation zeigten 17 von 41 patienten eine toxizitt vom grad 34 , wobei fatigue und hmatologische nebenwirkungen dominierten . schlussfolgerung der autoren die vorliegende studie demonstriert , dass die kombination von lokaler radiotherapie und systemischer immuntherapie bei patienten mit metastasierten soliden tumoren prinzipiell durchgefhrt werden kann und bei einem teil der patienten ein abskopales tumoransprechen bewirkt . kommentar originalpublikation golden eb , chhabra a , chachoua a et al ( 2015 ) local radiotherapy and granulocyte - macrophage colonystimulating factor to generate abscopal responses in patients with metastatic solid tumours : a proof - of - principle trial . 
panje klinik fr radio - onkologie , universittsspital zrich ( usz ) , rmistrasse 100 , 8091 zrich , schweiz e - mail : matthias.guckenberger@usz.ch ausma und mechanismen des abskopalen effekts abskopales tumoransprechen bei alleiniger radiotherapie stellt historisch gesehen zwar eine raritt dar , ist jedoch mit dem aufkommen neuer immuntherapeutischer strategien , insbesondere der immun - checkpoint - inhibitoren , vermehrt ins interesse der forschung gerckt [ 2 ]  . 
neben der dna - vermittelten zytotoxischen wirkung der radiotherapie deuten literatur kommentiert1 3 prklinische daten auf einen immunstimulierenden effekt der lokalen radiotherapie durch induktion proinflammatorischer zytokine und verstrkter antigenprsentation im bestrahlten tumor hin , die das immunsuppressive mikromilieu in tumoren berwinden und potentiell eine systemische antitumorale immunreaktion hervorrufen knnen [ 2 , 3 ]  . die vorliegende studie liefert erstmals prospektive daten dafr , dass unter einer kombination aus radiound immuntherapie ein abskopales ansprechen bei patienten mit metastasiertem tumorleiden auftreten kann [ 1 ]  . 
den anteil der radiotherapie am abskopalen tumoransprechen kann die studie jedoch aufgrund ihres designs nicht abschlieend definieren : einerseits wurde die palliative systemtherapie whrend der bestrahlung fortgefhrt , andererseits ist bekannt , dass zustzlich appliziertes gm - csf auch ohne radiotherapie einen effekt bei metastasierten tumorerkrankungen aufweist [ 4 ]  . 
hinzu kommt , dass die studie nur das beste abskopale ansprechen je patient angibt , jedoch keine informationen ber das ansprechen der brigen metastasen und ber das progressionsfreie berleben liefert . 
leider liefert die vorliegende studie auch keine einblicke in die potentiellen mechanismen einer durch radiotherapie stimulierten tumorspezifischen immunreaktion : abgesehen von der analyse der leukozytensubpopulationen erfolgte keinerlei immunmonitoring , wie etwa eine charakterisierung der zirkulierenden cd4 + und cd8 + - lymphozyten . da die immunstimulatorischen effekte der radiotherapie noch nicht vollstndig verstanden sind , ist eine strkere translationale komponente in zuknftigen studien dringend notwendig . 
so zeigte eine krzlich publizierte phase - i - studie zur kombination von ipilimumab und radiotherapie bei patienten mit metastasiertem malignem melanom eine ernchternd geringe ansprechrate , konnte jedoch im translationalen part eine durch den immunsuppressiven oberflchenliganden programmed death ligand 1 ( pdl1 ) vermittelte t - zell - erschpfung als resistenzmechanismus identifizieren [ 5 ]  . einfluss des abskopalen effekts auf das gesamtberleben wie aus anderen immuntherapeutischen studien bekannt , sprach in der hier kommentierten studie nur ein teil der patienten mit metastasiertem tumorleiden auf die behandlung an . 
dieses liee sich einerseits durch die abskopale wirkung auf die bestehenden makrometastasen erklren , andererseits aber auch durch die mgliche induktion einer tumorspezifischen immunantwort , die die ausbildung neuer lsionen effektiv verhindert . 
schlielich bleibt auch einzuwenden , dass der abskopale effekt nur ein surrogatparameter fr eine prognostisch gnstige tumorbiologie oder einen gnstigeren immunstatus sein knnte . ausblick aufgrund des frhen beginns dieser studie im jahr 2003 standen die aktuellen immuntherapien wie anti - ctla4 oder anti - pd1 - immun - checkpoint - inhibitoren als kombinationspartner fr die radiotherapie leider noch nicht zur verfgung . 
retrospektive analysen berichteten erst krzlich ber die sichere anwendbarkeit des anti - ctla4antikrpers ipilimumab in kombination mit einer stereotaktischen radiotherapie bei patienten mit metastasiertem malignem melanom und deuteten sogar auf eine mgliche verbesserung des gesamtberlebens hin [ 6 , 7 ]  . 
die ergebnisse prospektiver studien zur kombinierten immuntherapie und radiotherapie sind aktuell jedoch noch ausstehend [ 8 ]  . fazit zusammengefasst stimmen die ergebnisse der vorliegenden studie [ 1 ] zuversichtlich , dass die strahlentherapie das potential hat , sich als wichtiger bestandteil immuntherapeutischer behandlungsstrategien zu etablieren . 
die strahlentherapie wird hier ihren stellenwert gegenber anderen potentiellen kombinationspartnern wie vakzinen oder targeted therapies beweisen mssen [ 9 ]  . cdric panje und matthias guckenberger , zrich einhaltung ethischer richtlinien interessenkonflikt c . 
golden eb , chhabra a , chachoua a , adams s , donach m , fenton - kerimian m , friedman k , ponzo f , babb js , goldberg j , demaria s , formenti sc ( 2015 ) local radiotherapy and granulocyte - macrophage colony - stimulating factor to generate abscopal responses in patients with metastatic solid tumours : a proof - ofprinciple trial . 
gaipl us , multhoff g , scheithauer h , lauber k , hehlgans s , frey b , rdel f ( 2014 ) kill and spread the word : stimulation of antitumor immune responses in the context of radiotherapy . 
hodi fs , lee s , mcdermott df , rao un , butterfield lh , tarhini aa , leming p , puzanov i , shin d , kirkwood jm ( 2014 ) ipilimumab plus sargramostim vs ipilimumab alone for treatment of metastatic melanoma : a randomized clinical trial . 
victor ct - s , rech aj , maity a , rengan r , pauken ke , stelekati e , benci jl , xu b , dada h , odorizzi pm , herati rs , mansfield kd , patsch d , amaravadi rk , schuchter lm , ishwaran h , mick r , pryma da , xu x , feldman md , gangadhar tc , hahn sm , wherry ej , vonderheide rh , minn aj ( 2015 ) radiation and dual checkpoint blockade activate non - redundant immune mechanisms in cancer . 
knisely jps , yu jb , flanigan j , sznol m , kluger hm , chiang vls ( 2012 ) radiosurgery for melanoma brain metastases in the ipilimumab era and the possibility of longer survival . 
kiess ap , wolchok jd , barker ca , postow ma , tabar v , huse jt , chan ta , yamada y , beal k ( 2015 ) stereotactic radiosurgery for melanoma brain metastases in patients receiving ipilimumab : safety profile and efficacy of combined treatment . 
crittenden m , kohrt h , levy r , jones j , camphausen k , dicker a , demaria s , formenti s ( 2015 ) current clinical trials testing combinations of immunotherapy and radiation . 
wargo ja , reuben a , cooper za , oh ks , sullivan rj ( 2015 ) immune effects of chemotherapy , radiation , and targeted therapy and opportunities for combination with immunotherapy . 
guckenberger1 3 strahlenther onkol ( 2016 ) 192 : 6566 doi 10.1007 / s00066 - 015 - 0922 - 3 berlebensvorteil durch kombination von bevacizumab mit konventioneller radiochemotherapie bei glioblastomen vom proneuralen subtyp ? clemens seidel rolf - dieter kortmann online publiziert : 12 . 
in den beiden groen phase - iii - studien ( avaglio und rtog - 0825 ) , welche die wirksamkeit von bev in der erstlinientherapie bei glioblastomen untersuchten , wurde weder fr die gesamtpopulation noch nach unterteilung in mgmt - promotorbzw . 
dennoch entspricht es der klinischen beobachtung , dass manche patienten einen langfristigen berlebensvorteil von bev haben , wogegen viele nur kurzfristig durch antidematse effekte oder gar nicht von bev profitieren . in der vorliegenden arbeit von sandmann et al . 
entsprechend prdefinierter expressionsprofile bei der testung von 31 genen nach phillips originalpublikation sandmann t , bourgon r , garcia j et al ( 2015 ) patients with proneural glioblastoma may derive overall survival benefit from the addition of bevacizumab to first - line radiotherapy and temozolomide : retrospective analysis of the avaglio trial . 
 [ 1 ] lieen sich 349 verfgbare tumoren mithilfe von nanostring - assays retrospektiv in proneural ( 32 , 1 % ) , mesenchymal ( 39 , 8 % ) , proliferativ ( 16 , 6 % ) und nichtklassifiziert ( 11 , 5 % ) aufteilen . 
nach ausschluss von idh1mutierten tumoren zeigten patienten mit tumoren vom proneuralen subtyp ein verlngertes berleben nach bev ( n = 58 ) , verglichen mit plazebo ( n = 45 ) : 17 , 1 monate vs . 
ein effekt , der in der multivariaten analyse mit anderen faktoren ( alter , steroideinnahme , resektionsstatus , geschlecht , karnofsky - index , mgmt - status , mini - mental - test , rpaklasse ) deutlicher war ( hr 0 , 43 , p = 0 , 002 )  . 
die autoren argumentieren , dass nicht die berexpression von proangiogenen faktoren oder morphologisch starke angiogenese , sondern die empfindlichkeit fr eine vegf - blockade innerhalb der signaltransduktion das ansprechen auf bev definieren [ 710 ]  . 
 die geringere angiogenese des proneuralen subtyps knnte damit also hypothetisch insgesamt empfindlicher fr eine vegf - blockade sein . literatur kommentiert obschon sehr interessant , sollten die vorliegenden daten doch mit vorsicht bewertet werden , da es sich letztlich um eine retrospektive subgruppenanalyse handelt . 
in anbetracht der komplexen statistik bei der analyse von genexpressionsprofilen ist zudem eine externe validierung dieser avaglio - daten mit unabhngigen proben aus der rtog0825 - studie oder glarius - studie unbedingt erforderlich . fazit durch genexpressionsprofile lassen sich gbm - subtypen ( proneural , klassisch / proliferativ , mesenchymal ) definieren . 
beim proneuralen subtyp ist ein berlebensvorteil durch eine kombinationstherapie mit bev wahrscheinlich zu erwarten , auch wenn dieser sachverhalt erst noch weiter validiert werden muss . clemens seidel und rolf - dieter kortmann , leipzig einhaltung ethischer richtlinien interessenkonflikt c . 
phillips hs , kharbanda s , chen rh et al ( 2006 ) molecular subclasses of high - grade glioma predict prognosis delineate a pattern of disease progression , and resemble stages in neurogenesis . 
verhaak rg , hoadley ka , purdom e et al ( 2010 ) integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
sulman ep , won m , blumenthal dt et al ( 2013 ) molecular predictors of outcome and response to bevacizumab ( bev ) based on analysis of rtog 0825 , a phase iii trial comparing chemoradiation ( crt ) with and without bev in patients with newly diagnosed glioblastoma ( gbm )  . 
bais c , rabe c , wild n et al ( 2014 ) comprehensive re - assessment of plasma vegfa ( pvegfa ) as a candidate predictive biomarker for bevacizumab ( bv ) in thirteen pivotal trials ( seven indications )  . 
jubb am , hurwitz hi , bai w et al ( 2006 ) impact of vascular endothelial growth factor - a expression , thrombospondin - 2 expression , and microvessel density on the treatment effect of bevacizurnab in metastatic colorectal cancer . 
brauer mj , zhuang gl , schmidt m et al ( 2013 ) identification and analysis of in vivo vegf downstream markers link vegf pathway activity with efficacy of anti - vegf therapies . 
kortmann1 3 strahlenther onkol ( 2016 ) 192 : 4046 doi 10.1007 / s00066 - 015 - 0886 - 3 hyperfractionated stereotactic reirradiation for recurrent head and neck cancer jakub cvek lukas knybel eva skacelikova jiri stransky petr matousek karol zelenik oldrich res bretislav otahal lukas molenda david feltl received : 15 april 2015 / accepted : 31 july 2015 / published online : 28 august 2015 springer - verlag berlin heidelberg 2015 abstract purpose the goal of this work was to evaluate the efficacy and toxicity of hyperfractionated stereotactic reirradiation ( re - rt ) as a treatment for inoperable , recurrent , or second primary head and neck squamous cell cancer ( hnscc ) that is not suitable for systemic treatment . patients and materials forty patients with recurrent or second primary hnscc were included in this study . 
performance status and gtv proved to be significant prognostic factors regarding local control and survival . conclusion hyperfractionated stereotactic re - rt is a reasonable treatment option for patients with recurrent / second primary hnscc who were previously exposed to high - dose irradiation and who are not candidates for systemic treatment or hypofractionation . keywords stereotactic radiotherapy squamous cell carcinoma of the head and neck reirradiation overall survival toxicity hyperfraktionierte akzelerierte stereotaktische wiederbestrahlung von rekurrierten kopf - hals - karzinomen zusammenfassung ziel ziel der studie war es , die effektivitt und toxizitt der hyperfraktionierten akzelerierten stereotaktischen wiederbestrahlung ( re - rt ) fr die behandlung von patienten mit lokalrezidiv von fortgeschrittenen kopf - hals - tumoren ( head and neck squamous cell cancer , hnscc ) , die fr eine systemische therapie nicht geeignet sind , zu untersuchen . 1 3original article patienten und methodik in die studie wurden 40 patienten mit rekurrierten oder sekundren hnscc eingeschlossen . 
die behandlung musste 95 % des planungszielvolumens ( ptv , definiert als makroskopisches tumorvolumen [ gtv ] + 3 mm zur bercksichtigung der mikroskopischen streuung , ohne zustzlichen saum ) abdecken.unbeteiligte lymphknoten wurden nicht bestrahlt . ergebnisse alle patienten absolvierten die behandlung plangem ( mediane behandlungsdauer 11 tage ; spanne 914 tage )  . 
 patientenstatus und gtv waren signifikante prognostische faktoren fr die lokale tumorkontrolle und das berleben . schlussfolgerung hyperfraktionierte akzelerierte stereotaktische re - rt ist eine interessante wahl fr patienten mit rekurrierten oder sekundren hnscc , die fr eine systemische therapie nicht geeignet sind . schlsselwrter stereotaktische strahlentherapie plattenepithelkarzinom der kopf - hals - region wiederbestrahlung gesamtberleben toxizitt despite advancements in treatment of patients with advanced head and neck squamous cell carcinoma ( hnscc ) , including altered radiation fractionation and the addition of chemotherapy regimens to radiation therapy , treatment outcomes remain poor [ 1 ]  . 
most relapses occur within the first 2 years after the primary treatment , and 96 % of these local or regional failures are located inside the 95 % isodose lines . 
salvage therapy using external beam re - irradiation ( re - rt ) has been used rather infrequently in the past due to concerns about potential toxicity [ 1 ]  . 
in 2001 , the rtog 9610 trial observed 7 % grade 5 ( fatal ) toxicity and 15 % grade 4 acute toxicity [ 5 ] ; however , with the advent of new technologies , there is now renewed interest in re - rt . stereotactic body radiotherapy ( sbrt ) may be an appropriate option for re - rt in the head and neck region , due to its ability to deliver a high dose to a limited target volume in a short amount of time [ 6 , 7 ]  . 
in patients treated with re - rt , almost all of the locoregional recurrences occur within the reirradiated recurrent gross tumor volume ( rgtv ) , despite efforts made to avoid prophylactic radiotherapy ( rt ) of tissue that is at risk of subclinical disease , which underscores the importance of minimizing the volume of reirradiated tissue [ 8 ]  . 
approaches that decrease the daily dose and increase the number of radiation treatments , while still maintaining the precision of stereotactic radiotherapy , may be desirable options to reduce late toxicity [ 9 ]  . 
brachytherapy ( bt ) has been used in treatment of recurrent head - and - neck cancer with impressive outcomes [ 10 ] , but technical and anatomical constraints limit its scope of use . the purpose of this study was to evaluate the toxicity and efficacy of hyperfractionated stereotactic re - rt as a salvage treatment for head and neck cancer in terms of overall survival ( os ) , local control , and complications . 
to the best of our knowledge , this is the first study of the use of hyperfractionated sbrt to treat head and neck cancer . materials and methods a total of 40 patients with hnscc were included in this study between november 2011 and july 2014 . 
contraindications to chemotherapy were the following : low performance status ( 13 patients , 33 % ) , low liver functions ( 11 patients , 28 % ) , low kidney functions ( 9 patients , 23 % ) , low cardiac and / or pulmonary function ( 7 patients , 18 % )  . 
the primary radiotherapy dose was higher than 60 gy , and the time gap between primary treatment and the start of re - rt was greater than 9 months for all patients . 
no adjuvant therapy was used , including chemotherapy , hyperthermia , and external - beam radiation . this study was approved by the local institutional review board ( university hospital ostrava )  . 
patients whose disease progressed after sbrt were provided best supportive care . treatment planning the target volume was defined based on simulation using ct images combined with magnetic resonance imaging ( mri )  . 
the planning target volume ( ptv ) was defined as the radiographic gross tumor volume ( gtv ) plus a 3 mm marg during treatment , repeated pairs of orthogonal x - ray images were used to provide on - line image guidance based on the skull base ( 20 % ) or cervical spine ( 80 % )  . dose prescription treatment was provided using a linear accelerator with 6 mv photons . 
the median duration of treatment was 28 min ( range 1752 min )  . evaluation of toxicity and response the analysis was performed after a median follow - up of 12 months ( range 336 months )  . 
the rtog / eortc scale was also used for scoring of late toxicity . statistical analysis dose - limiting toxicity was defined as toxicity that required interruption of the course of rt due to the intolerance . 
other parameters that were evaluated included the incidence and duration of acute toxicity , incidence of late toxicity , local progression - free survival ( l - pfs ) , metastatic progressionfree survival ( m - pfs ) , and overall survival ( os )  . initial patient characteristics were recorded at the start of re - rt . 
the incidence of mucosal grade 3 acute toxicity was 37 % ( oral cavity and / or pharynx ) , and the recovery time was 4 weeks for all of these patients . 
in 4 cases ( 21 % ) , patients were hospitalized to provide parenteral support for severe mucositis . there was 0 % incidence of grade 3 acute toxicity of sk no grade 4 or 5 toxicities were recorded . 
neither carotid blowout syndrome nor any other grade 3 or 4 late toxicity was observed . outcomes the entire treatment schedule was completed as planned for all patients ( median duration 11 days , range 914 days )  . 
the median maximal dose to the spinal cord was 9 gy ( range 021 gy )  . during follow - up , 14 patients ( 35 % ) showed disease progression , of which 4 cases ( 10 % ) involved distant metastasis . 
dose of primary radiotherapy , time to re - rt and history of surgery were found to not be significantly predictive of os . discussion the treatment of recurrent hnscc in previously irradiated patients remains a therapeutic challenge . 
several studies have demonstrated that re - irradiation ( > 60 gy ) is a feasible and effective alternative option , using a variety of techniques and fractionation schedules in carefully selected patients [ 14 ] , and subset analysis indicates that an increased total dose correlated with increased local control and survival [ 15 ]  . 
 the effectiveness of sbrt has been demonstrated , but concern exists that the high dose per fraction could cause considerable treatment - related morbidity and mortality [ 16 , 17 ]  . 
to our knowledge , this is the first study of the use of hyperfractionated sbrt for treatment of recurrent / second primary hnscc . in this study , the incidence of grade 3 acute mucositis was 37 % , and the median and maximum duration of confluent mucositis were 19 days and 4 weeks , respectively . 
 [ 18 ] , who first reported on the use of frameless sbrt for treatment of recurrent hnscc ; in this pioneering work no acute grade 4 or 5 toxicities or long - term adverse events were observed . 
 [ 19 ] observed grade 3 mucosal toxicity in only 7 of 56 patients ( 13 % ) ; however , this patient group was different with respect to tumor burden . 
although it is generally believed that large arteries are relatively resistant to radiotherapy , there are some reports of fatal hemorrhage or occlusion of large vessels resulting from treatment [ 20 ]  . 
we did not observe such complications in our study , probably because of the low dose used per fraction . in our group of heavily pretreated patients , the 1 - year and 2 - year l - pfs were both 44 % . 
in previous studies using a reirradiation dose ranging from 20 to 30 gy in 5 fractions , the 2 - year local control ( lc ) obtained was 26 % . 
n at risk number at risk in 200 - day increments of up to 3039 gy in 3 fractions , but this schedule could be considered too hot . comparison between the use of sbrt and brachytherapy favors the latter treatment method . 
there are two possible explanations for the better effectiveness observed with bt : ( 1 ) the dose inhomogeneity typical of bt produces higher equivalent uniform dose , and ( 2 ) the target volumes of typical brachytherapy patients is much smaller than those of patients treated with external beam rt . os is a better indicator of the treatment outcome in patients with recurrent hnscc cancers , because it reflects the cumulative effect of both lc and treatment toxicity . 
in the rtog 9610 phase ii trial comparing external beam radiation to 60 gy with concurrent 5 - fluorouracil and hydroxyurea chemotherapy , the median os observed was 8.2 months and the estimated 1 - year survival rate was 41.7 % [ 5 ]  . 
this is in agreement with previous reports observing that significantly improved clinical outcomes are associated with doses above 35 gy and tumor volumes below 25 ml [ 18 ]  . although our study is limited by its retrospective nature and its small patient population , it still demonstrates that re - rt can be curative in patients with good performance status who have small tumors . 
further improvement might be expected after incorporation of improved systemic therapy into the treatment regimen [ 24 ]  . 1 3hyperfractionated stereotactic reirradiation for recurrent head and neck cancer 46 conclusion hyperfractionated sbrt is a reasonable treatment option for patients with inoperable recurrent / second primary hnscc who were previously subjected to high - dose irradiation and who are not suitable candidates for systemic treatment or hypofractionation . 
longer survival could be expected in patients with good performance status who have small tumors . acknowledgment institutional supportrvo - fnos / 2012was re ceived for this work . compliance with ethical guidelines conflicts of interest j . 
feltl state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 3239 doi 10.1007 / s00066 - 015 - 0875 - 6 risk profile for osteoradionecrosis of the mandible in the imrt era gabriela studer marius bredell stephan studer gerhard huber christoph glanzmann received : 1 may 2015 / accepted : 2 july 2015 / published online : 12 august 2015 the author ( s ) 2015 . 
this article is published with open access at springerlink.com abstract background the risk for osteoradionecrosis ( orn ) of the mandible is positively related to bone volume exposed to > ~ 60 gy . 
we hypothesized that in combined treatment , surgery may also be a risk factor . patients and methods the impact of mandibular surgery on orn in locally disease - free imrt cohorts was retrospectively analyzed . results between october 2002 and october 2013 , 531 of 715 patients with oral cavity cancer ( occ ) , mesopharyngeal cancer ( mc ) , or salivary gland tumor were treated with the mandible bone exposed to ~ > 60 gy ( mean follow - up , 38 months ; 7143 months )  . 
huber , pd department of otorhinolaryngology , head neck cancer center , head and neck surgery , university hospital zurich , zurich , switzerland conclusion marginal or periosteal bone resection of the mandible was identified as the highest orn risk factor in our imrt cohort . keywords osteoradionecrosis , orn risk factors , orn preradiation surgery surgery - related orn postoperative orn risikoprofil fr osteoradionekrosen des kiefers in der imrt - ra zusammenfassung hintergrund das risiko fr die entwicklung einer kiefernekrose nach radiotherapie ( osteoradionekrose , orn ) korreliert bekanntlich mit dem knochenvolumen , das einer dosis von ~ > 60 gy ausgesetzt wurde . 
hypothese war , dass die chirurgie bei kombinierten therapien ebenfalls einen risikofaktor darstellt . material und methode der einfluss chirurgischer interventionen am kiefer auf das risiko einer orn wurde in unserem lokal krankheitsfreien imrt - kollektiv retrospektiv analysiert . ergebnisse zwischen oktober 2002 und oktober 2013 wurden 531 / 715 patienten mit mundhhlenkarzinomen ( occ ) , mesopharynxkarzinomen ( mc ) oder speicheldrsentumoren mit dosen > 60 gy am kieferknochen behandelt ( mittlere beobachtungszeit 38 monate ; spanne 7143 monate )  . 
die orn - rate nach definitiver imrt bei mc ( 16 / 227 ) und nach postoperativer imrt bei occ ohne chirurgischen eingriff am kieferknochen ( 3 / 46 ) belief sich auf je 7 % , bei occ - patienten mit operation am kieferknochen auf 29 % ( 15 / 60 ; p = 0 , 002 )  . 
this observation motivated us to analyze the impact of previous mandibular surgery on the risk for orn . our hypothesis was that pre - imrt surgery of the mandible may also be a risk factor for orn . patients and methods we retrospectively analyzed a single - center occ / mc / salivary gland tumor imrt cohort with respect to orn . 
the maximum dose ( dmax ) is defined as the highest dose in 1 % . details of the imrt schedules used have been provided in previous reports [ 10 , 11 ]  . systemic concomitant therapy if indicated , cisplatin was concomitantly given ( 40 mg / m2 / week )  . 
since april 2006 , cetuximab has been used for patients with contraindications for cisplatin chemotherapy ( 400 mg / m2 loading dose , followed by 250 mg / m2 1 day / week )  . 
age and / or comorbidity or early - stage disease were reasons not to add systemic therapy ( 15 % )  . follow - up all patients were regularly seen in our joint clinics 36 weeks after completion of imrt , at the departments of otorhinolaryngology and head and neck surgery or the department of craniomaxillofacial and oral surgery . 
 actuarial survival data were calculated using kaplanmeier curves and log - rank tests implemented in statview ; p values of < 0.05 were considered statistically significant . multivariate analysis was performed using the statview calculation program ( mantelcox log - rank test )  . 
 19 of 249 operated patients ( 7.6% , ns ; table 2 ) , suggesting an additional risk factor impacting the risk for orn other than radiation dose only . we observed 5 % ( 36 / 715 ) orn events of grade 14 in the entire cohort , and 7 % ( 36 / 531 ) in the cohort at risk ( table 2 )  . 
all orn events occurred in mandibles exposed to > 60 gy . grade 1 , 2 , 23 , 3 , and 4 orn events were observed in 2 , 5 , 21 , 4 , and 4 patients , respectively . of 36 orn events , eight ( 22 % ) developed as a consequence of invasive manipulation on previously with > 50 gy irradiated bone areas ( postintervention orn ) : four of eight events translated into complicated grade 4 orn ( pathological fracture , osteocutaneous fistula , osteomyelitis , persisting pain ) following segmental resection or limited surgery for orn . 
1 mandible bone dosevolume histograms ( mean values , cc ) of the following subgroups , all with the mandible exposed to > 60 gy ( n total = 458 ) : - postoperative imrt in oral cavity cancer ( occ ) patients with / without osteoradionecrosis ( orn ) who underwent mandibular surgery ( + ms ) or not ( ms ) - definitive imrt in occ patients ( no ms , all in the cohort without orn ) - definitive and postoperative imrt in mesopharynx cancer ( mc ) patients orn ( none of them underwent mandibular surgery )  . 
red curves represent the two cohorts with orn ( + orn ) , dotted lines postoperative imrt groups , and continuous lines definitive imrt groups 1 3risk profile for osteoradionecrosis of the mandible in the imrt era 36 fig . 
 figure 2 shows kaplanmeier survival curves for orn events following ( 1 ) definitive imrt in mc patients and ( 2 ) postoperative imrt in occ patients : most orn events occurred early after imrt completion , during the first 20 months . 
no ms ( 227 ) mc postop no ms ( 72 ) mc postop with ms ( 2 ) ( 1 segmental , 1 periosteal ) occ postop with ms ( 60 ) periosteal or marginal ( 33 ) segmental ( 27 ) ~ 115200 cc ~ 1710410 cc ~ 2315102.50 dvh dosevolume histogram , mc mesopharyngeal carcinoma , occ oral cavity cancer , postop postoperative imrt ( prescription dose 6066 gy ) , def . 
an orn rate ( grade 23 ) of 39 % was found for postoperative imrt patients at risk with floor of the mouth carcinoma or mandible infiltrating carcinoma who underwent previous periosteal or marginal mandibular resection ( table 3 )  . 
a plausible explanation for this finding is that the mandible is more dependent on the periosteum for its blood supply than on the inferior alveolar neurovascular bundle , especially in older individuals [ 12 ]  . 
in segmental resection cases the surgery is more extensive and mostly requires a composite free vascularized graft with a well - nourished bone flap with an unharmed periosteum and adequate soft tissue coverage . table 4 summarizes the orn rates of our mc / occ cohorts based on combined surgical and imrt - related risk parameters . 
17 % in 106 patients with postoperative occ is explained by ( a ) the lower dose to the bone ( dvh ) and ( b ) only 2 of 74 cases underwent mandibular surgery in the mc subgroup . 
poor outcome following definitive irradiation of occ also in the imrt era was previously reported ; however , data on this topic are scant [ 13 ] , which may partly be explained by a negative selection of occ patients referred for definitive radiation ( elderly , comorbid patients with large / inoperable tumors )  . 
for the small subgroup ( n = 14 ) who survived 2 years , we cannot exclude an orn rate of approximately 22 % ( according to the statistical " rule of three " to estimate the probability of adverse events in small sample sizes with few events , giving the upper limit of the 95 % confidence interval of the probability : 3 / 14 = 22 % )  . 1 3risk profile for osteoradionecrosis of the mandible in the imrt era 38 the positive relationship between radiation dosevolumes and the risk for orn is known , and the reduced orn risk by using mandible - sparing imrt techniques was confirmed in several reports [ 3 , 58 ]  . 
only scant information is available on the orn risk in the postoperative setting , which is characterized by lower radiation doses to the mandible than in the definitive radiation setting . 
table 5 gives an overview of the orn events in our patients related to the treatment sequence . korean researchers reported on occ / mc patients irradiated postoperatively with conventional three - dimensional radiation techniques . 
 [ 15 ] , who assessed 221 patients divided into the following groups : ( 1 ) parotidectomy only ; ( 2 ) parotidectomy with mastoidectomy ; and ( 3 ) parotidectomy with subtotal petrosectomy . 
this low susceptibility to orn may be partially explained by the fewer surgical interventions performed in this area , the absence of teeth , and adequate soft tissue coverage by the masticatory muscles . in summary , the following conclusions can be drawn from the present results : 1 . 
half the patients with postintervention orn developed grade 4 orn ( 4 / 8 ) conclusion periosteal or marginal mandibular resection was the statistically significantly highest orn risk factor , translating into a 39 % orn rate grade of 23 , vs . 
7 % following defini tive imrt or postoperative imrt with no or segmental resection . consequently , the radiation dose to the mandible should be minimized in patients at high risk for orn . open access this article is distributed under the terms of the creative commons attribution license which permits any use , distribution , and reproduction in any medium , provided the original author ( s ) and the source are credited . compliance with ethical guidelines conflicts of interest g . 
glanzmann state that there are no conflicts of interest . strahlenther onkol ( 2016 ) 192 : 1724 doi 10.1007 / s00066 - 015 - 0913 - 4 comparative treatment planning study on sequential vs . 
both strategies provided satisfactory oar sparing . conclusion this study showed significant dosimetric differences with potential clinical relevance between two vmat boost strategies regarding coverage , conformity and dose to the ptvs . 
a clinical phase iii / iv trial endorsed by the german head and neck clinical trials group ( iag - kht ) will evaluate differences in acute / late toxicity as well as in locoregional recurrences between the two boost techniques . keywords radiotherapy volumetric modulated arc therapy chemoradiation sequential boost toxicity simultaneous integrated boost vergleichende therapieplanungsstudie zum sequentiell oder simultan integrierten boost bei patienten mit kopf - hals - tumoren unterschiede in der dosisverteilung und potentielle implikationen fr die klinische praxis zusammenfassung ziel vergleich von sequentiellem ( seqb ) und simultanintegriertem boost ( sib ) mit moderner volumetrischer arc - therapie ( vmat ) fr patienten mit plattenepithelkarzinomen der kopf - hals - region . original article 18 patienten und methoden fr 10 patienten mit plattenepithelkarzinomen der kopf - hals - region und definitiver radiochemotherapie erfolgte eine vmat - planung als seqb und sib fr die planungszielvolumina ( ptv ) 13 . 
 es wurden dosisverteilung , abdeckung , konformitt , und homogenitt der ptvs sowie die risikoorganschonung verglichen . ergebnisse das mittlere definierte volumen standardabweichung betrug 137 , 7 44 , 8 cm3 , 351 , 3 83 , 9 cm3 und 895 , 6 120 , 5 cm3 fr die ptvs13 . 
seqb erreichte jedoch signifikant bessere abdeckung des ptv1 / 3 , schlechtere konformitt fr ptv13 und eine hhere mittlerer dosis ( 111115 % ) in ptv2 / 3 , ( p 0 , 007 )  . 
beide boost - strategien fhrten zu vergleichbar guter risikoorganschonung . vergleichende bestrahlungsschlussfolgerung diese planungsstudie zeigt wichtige dosimetrische unterschiede in bezug auf ptv - abdeckung , konformitt und dosis , die mglicherweise klinisch relevant sein knnten . 
eine klinische phase - iii / iv - studie mit untersttzung der interdisziplinren arbeitsgruppe fr kopf - hals - tumoren der deutschen krebsgesellschaft ( iag - kht ) wird derzeit vorbereitet , die zur klrung der wertigkeit dieser beiden boost - techniken im hinblick auf akutund sptmorbiditt und lokoregionre rezidive beitragen kann . schlsselwrter strahlentherapie volumetrisch modulierte arc - therapie radiochemotherapie sequentieller boost toxizitt simultan integrierter boost definitive chemoradiation remains the standard of care for patients with locally advanced squamous cell carcinoma of the head and neck ( lahnscc ) [ 1 ] with locoregional relapse as the main form of failure . 
historically , radiotherapy ( rtx ) has been applied using a shrinking field or so - called sequential boost ( seqb ) strategy , starting with a large treatment volume and progressively shrinking it , corresponding to the different total doses needed for tumor control for the low ( elective lymph node levels ) , intermediateand highrisk target volumes ( tv )  . 
the simultaneous integrated boost ( sib ) technique using intensity - modulated radiotherapy ( imrt ) or volumetric modulated arc therapy ( vmat ) [ 2 ] allows risk - adapted single plan efficient planning and treatment with different dose levels and intensities appropriate for the selected tvs . 
 imrt caused significantly fewer occurrences of xerostomia without compromising tumor control as compared to threedimensional conformal rtx ( 3d - crtx ) in a phase iii trial on patients with hnscc by parotid gland ( pg ) sparing to a mean dose of < 26 gy [ 6 ]  . 
despite the fact that , besides one trial on patients with nasopharyngeal carcinoma [ 17 ] , no randomized prospective trial comparing outcome data and / or toxicity for seqb versus sib ( chemo ) rtx for lahnscc has been published , many departments around the world have adopted the sib as current practice , assuming it to be as effective as seqb . this comparative planning study compares three dose level seqb and sib derived cumulative dosevolume histograms ( dvh ) for tvs , and organs at risk ( oar ) using modern vmat technology instead of imrt for lahnscc by comprehensive evaluation of various established plan quality parameters . 
this data should underline the rationale for a phase iii / iv randomized multicenter trial . patients and methods patient selection and contouring ten patients with lahnscc were randomly selected from a list of patients previously treated with a definitive vmat ( rapidarc , varian medical systems , palo alto , ca , usa ) plan at our department . 
the final dose distribution was calculated using the aaa algorithm ( 2.5 mm grid size )  . plan evaluation quantitative comparisons used a dvh analysis , with parallel qualitative visual comparisons of the axial isodose curves . 
the mean volumes of ptv13 , the dmean , dmax ( maximal dose to the ptv ) , d2 ( dose delivered to at most 2 % of the ptv ) , d100 ( dose delivered to 100 % of the ptv ) , d98 ( dose delivered to 98 % of the ptv ) and d95 ( dose delivered to 95 % of the ptv ) for ptv13 were also evaluated . 
the salt coverage factor ( cvfsalt ; cvf = tvri / tv ; tvri : irradiated tv encompassed by the 95 % reference isodose ) was calculated for each ptv , with 1 indicating perfect coverage . 
the conformities of the dose distributions were calculated with : rtog conformity index ( cirtog ; ci = vri / tv ; vri : irradiated volume encompassed by the 95 % reference isodose )  . 
both strategies achieved excellent coverage for all ptvs ( range of cvfsalt for seqb : 0.971 , and for sib : 0.950.97 ) with a significantly better cvfsalt for ptv1 and 3 in seqb plans . 
 sib plans gave dmeans for all ptvs ( p 0.007 ) close to the prescribed doses ( range 1.11.5 % ) , while seqb plans had higher than prescribed dmeans to ptv2 and ptv3 . 
1 final dose distribution for an example patient showing the surrounding 95 % isodose to ptv3 for a seqb ( summation of plans 14 ) and b sib plans nique . 
the data demonstrates that there were no significant ( pgs , oc , nt ) or clinically relevant differences regarding classical oar ( sc , bs and larynx )  . 
 interestingly , the seqb gave a significantly lower physical mean dmax to the sc and bs , which may translate into an even larger advantage when the biological sparing ( eqd2 ) of the hart approach is taken into account . 
our data show that the appropriate definition of the tv is especially crucial with the sib approach and demands detailed knowledge of clinical findings as provided by collaboration with the surgeon together with high - resolution imaging . 
this raises the question as to what kinds of cross - sectional , multiplanar or functional imaging should be used in defining the gtv , and what is the most sensitive and specific imaging method to detect lymph node metastasis . 
 [ 25 ] showed a pooled sensitivity of 89 % and a specificity of 89.5 % for fdg - pet / ct and a corresponding pooled sensitivity and specificity of 71.6 and 78 % for standard conventional imaging methods . furthermore , a recent detailed per - neck - level meta - analysis on 13 studies ( 3460 neck levels ) demonstrated a sensitivity and specificity for fdg - pet / ct of 84 and 96 % , and for conventional imaging of 63 and 96 % , respectively , for the detection of nodal metastasis in this group of patients [ 26 ]  . 
fdg - pet / ct carries inherent limitations , including its inability to define the depth of invasion due to inflammatory changes of the tumor environment and the relation of tumors to neighboring structures [ 27 ]  . 
although fdg - pet / ct does not seem to add value over ct for the routine delineation of nodal gtvs , the implementation of an automated segmentation method to improve the reproducibility and interinstitutional comparison of nodal gtvs has been recommended if it be used [ 28 ]  . 
simultaneous integrated1 3 table 3 dosevolume histogram parameters and treatment efficiency for seqb and sib plans ( mean sd ) p - value volume ptv1 ptv1 coverage conformity homogeneity ptv2 ptv2 coverage conformity homogeneity ptv3 ptv3 coverage conformity homogeneity conformity larynx body parameter defined volume ref . 
this could imply a higher risk of acute and late effects of rtx , including dysphagia , xerostomia , edema , subcutaneous fibrosis , muscle strictures and osteoradionecrosis , possibly affecting tissues not routinely delineated and therefore not accounted for with constraints during planning . 
 however , the sib technique has been adopted for clinical studies [ 716 , 29 ] and in the daily routine as the primary approach without clear evidence of equality or noninferiority in terms of efficacy and safety . 
possible strategies to prevent excessive weight loss and changes in dose distribution could include the routine placement of a gastric feeding tube prior to chemoradiation and weekly dietary counselling [ 30 ]  . 
a clinical phase iii / iv trial endorsed by the german head and neck clinical trials group ( iag - kht ) will address differences in locoregional control and acute / late toxicities between the two techniques . compliance with ethical guidelines conflict of interest c . 
budach state that there are no conflicts of interest . this study was approved by the institutional review board of the charit universittsmedizin berlin ( ea4 / 015 / 15 )  . strahlenther onkol ( 2016 ) 192 : 6769 doi 10.1007 / s00066 - 015 - 0924 - 1 akuttoxizitt nach hypofraktionierter versus konventionell fraktionierter strahlentherapie bei patienten mit prostatakarzinom frank lohr michael ehmann online publiziert : 6 . 
november 2015 springer - verlag berlin heidelberg 2015 hintergrund im jahre 2007 begann die randomisierte phase - iii - studie ( hypro ) , die den effekt einer hypofraktionierten im vergleich zu einer normal fraktionierten strahlentherapie bei patienten mit prostatakarzinom auf das rezidivfreie berleben untersuchen sollte . 
in der hier kommentierten arbeit geht es um die akuten gastrointestinalen und urogenitalen nebenwirkungen . methoden in die studie wurden aus sieben niederlndischen strahlentherapiezentren patienten im alter zwischen 44 und 85 jahren mit histologisch gesicherten prostatakarzinomen mit intermedirem oder hohem risiko eingeschlossen . 
es handelte sich um tumoren in den stadien t1bt4 nx0 mx0 mit einem serum - psa von < 60 ng / ml oder niedriger und einem who - performance - status von 02 . 
mit hilfe einer webbasierten applikation wurden patienten im verhltnis 1 : 1 randomisiert , entweder zu einer strahlentherapie mit standardfraktionierung ( 39 fraktionen zu je 2 gy / 8 wochen ) oder einer hypofraktionierung ( 19 fraktionen zu je 3 , 4 gy / 6 , 5 wochen , 3 fraktionen / woche )  . 
nichtunterlegenheit der hypooriginalpublikation aluwini s , pos f , schimmel e et al ( 2015 ) hypofractionated versus conventionally fractionated radiotherapy for patients with prostate cancer ( hypro ) : acute toxicity results from a randomised non - inferiority phase 3 trial . 
ehmann klinik fr strahlentherapie und radioonkologie , universittsmedizin mannheim , theodor - kutzer - ufer 13 , 68167 mannheim , deutschland e - mail : frank.lohr@umm.de fraktionierung wurde separat fr urogenitale und gastrointestinale akuttoxizitt getestet mit der nullhypothese , dass kumulative inzidenzen jedes toxizittstyps nicht mehr als 8 % hher in der hypofraktionierungsgruppe als bei standardfraktionierung sind . 
drei monate nach strahlentherapie berichteten 73 patienten ( 22 % ) in der standardfraktionierungsgruppe und 75 ( 23 % ) in der hypofraktionierungsgruppe ber urogenitale toxizitt grad 2 sowie 43 ( 13 % ) versus 42 patienten ( 13 % ) ber gastrointestinale toxizitt grad 2 . 
die kumulative inzidenz akuter gastrointestinaler toxizitt grad 2 war 120 tage nach hypofraktionierung hher ( 42 , 0 % ; 37 , 2 46 , 9 ) als nach standardfraktionierung ( 31 , 2 % ; 95 % - ki 26 , 635 , 8 ; differenz 10 , 8 % ; 90 % - ki 5 , 2516 , 43 ; or 1 , 6 ; p = 0 , 0015 ; nichtunterlegenheit nicht besttigt )  . literatur kommentiert 68 schlussfolgerung der autoren hypofraktionierung war der standardfraktionierung bezglich urogenitaler und gastrointestinaler toxizitt bei mnnern mit prostatakarzinom bei intermedirem oder hohem risiko nicht nicht - unterlegen . 
die patienten verbleiben in beobachtung hinsichtlich der effektivittsendpunkte . kommentar eine dosiseskalation bei der strahlentherapie des prostatakarzinoms hat das biochemisch rezidivfreie berleben ( brfs ) in mehreren randomisierten studien bei tolerabler toxizitt verbessern knnen [ 13 ]  . 
die bisherigen ergebnisse mit solchen schemata waren allerdings zwiespltig . whrend in der randomisierten kanadischen studie die hypofraktionierung sowohl hinsichtlich toxizitt als auch brfs schlechter als die normofraktionierung abschnitt [ 8 ] , berichteten die autoren der italienischen studie ber ein besseres brfs durch hypofraktionierung bei gleicher toxizitt [ 9 ]  . 
im fox chase cancer center [ 10 ] waren die erfahrungen mit der hypofraktionierung hinsichtlich toxizitt und brfs schlechter als bei der normofraktionierung , allerdings wegen der kleinen patientenzahlen statistisch nicht signifikant . damit besteht derzeit wegen unterschiedlicher aussagen eine unklare situation . 
daher sollten der hier besprochene hypro - trial sowie krzlich als abstract publizierte ergebnisse der britischen chhip - studie ( [ 11 ] , die vollpublikation steht noch aus ) und spter auch die rtog0415sowie die profit - studie die datenlage verbessern , insbesondere deshalb , weil sie mit modernen bestrahlungstechniken durchgefhrt wurden : anspruchsvolle 3d - crt / imrt , teilweise igrt . die aktuelle auswertung der hypro - studie befasst sich mit der akuttoxizitt der hypofraktionierung . 
in der gesamtschwere scheinen diese unterschiede akzeptabel , auch wenn hier formal ( im falle der urogenitalen nebenwirkungen durch underpowering , im fall der gastrointestinalen nebenwirkungen durch signifikante effektunterschiede ) die nicht - nichtunterlegenheit der hypofraktionierung festgestellt werden muss . im auge behalten werden sollten schlielich im hier besprochenen kontext auch die daten des ascendert - trials [ 12 ] , der eine dosiseskalation mithilfe der brachytherapie erreicht und mit der allein externen bestrahlung vergleicht . 
der vergleich des ldr - boosts mit off - protocol - hdr - daten scheint in diesem fall auf eine berlegenheit des ldr - boosts hinzuweisen , was mglicherweise a / b - berechnungen zwischen der hdrhypofraktionierung und den dosisquivalenten einer der standardfraktionierung entsprechenden ldr - brachytherapie ermglicht . 
hier muss zunchst allerdings noch die vollpublikation abgewartet werden . fazit die hochdosierte strahlentherapie des prostatakarzinoms fhrt zu immer besseren ergebnissen bezglich des brfs und mglicherweise auch des berlebens , auch wenn dieser endpunkt angesichts von immer mehr confoundern / salvagetherapien immer schwerer zu bewerten ist . 
die vorliegende arbeit liefert einen weiteren datenpunkt , der nahe legt , dass moderat hypofraktionierte bestrahlungsprotokolle nicht bezglich aller medizinischer endpunkte den normofraktionierten schemata berlegen sind , jedoch bisher beherrschbar erscheinen . 
dearnaley dp , jovic g , syndikus i et al ( 2014 ) escalated - dose versus control - dose conformal radiotherapy for prostate cancer : long - term results from the mrc rt01 randomised controlled trial . 
heemsbergen wd , al - mamgani a , slot a , dielwart mf , lebesque jv ( 2014 ) long - term results of the dutch randomized prostate cancer trial : impact of dose - escalation on local , biochemical , clinical failure , and survival . 
king c , freeman d , kaplan i et al ( 2013 ) stereotactic body radiotherapy for localized prostate cancer : pooled analysis from a multi - institutional consortium of prospective phase ii trials . 
arcangeli s , strigari l , gomellini s et al ( 2012 ) updated results and patterns of failure in a randomized hypofractionation trial for high - risk prostate cancer . 
dearnaley d , syndikus i , sumo g et al ( 2012 ) conventional versus hypofractionated high - dose intensity - modulated radiotherapy for prostate cancer : preliminary safety results from the chhip randomised controlled trial . 
morris j , tyldesley s , pai h et al ( 2015 ) ascende - rt : a multicenter , randomized trial of dose - escalated external beam radiation therapy versus low - dose - rate brachytherapy for men with unfavorable - risk localized prostate cancer . 
j clin oncol 33 akuttoxizitt nach hypofraktionierter versus konventionell fraktionierter strahlentherapie1 3 strahlenther onkol ( 2016 ) 192 : 6566 doi 10.1007 / s00066 - 015 - 0922 - 3 berlebensvorteil durch kombination von bevacizumab mit konventioneller radiochemotherapie bei glioblastomen vom proneuralen subtyp ? clemens seidel rolf - dieter kortmann online publiziert : 12 . 
in den beiden groen phase - iii - studien ( avaglio und rtog - 0825 ) , welche die wirksamkeit von bev in der erstlinientherapie bei glioblastomen untersuchten , wurde weder fr die gesamtpopulation noch nach unterteilung in mgmt - promotorbzw . 
dennoch entspricht es der klinischen beobachtung , dass manche patienten einen langfristigen berlebensvorteil von bev haben , wogegen viele nur kurzfristig durch antidematse effekte oder gar nicht von bev profitieren . in der vorliegenden arbeit von sandmann et al . 
entsprechend prdefinierter expressionsprofile bei der testung von 31 genen nach phillips originalpublikation sandmann t , bourgon r , garcia j et al ( 2015 ) patients with proneural glioblastoma may derive overall survival benefit from the addition of bevacizumab to first - line radiotherapy and temozolomide : retrospective analysis of the avaglio trial . 
 [ 1 ] lieen sich 349 verfgbare tumoren mithilfe von nanostring - assays retrospektiv in proneural ( 32 , 1 % ) , mesenchymal ( 39 , 8 % ) , proliferativ ( 16 , 6 % ) und nichtklassifiziert ( 11 , 5 % ) aufteilen . 
nach ausschluss von idh1mutierten tumoren zeigten patienten mit tumoren vom proneuralen subtyp ein verlngertes berleben nach bev ( n = 58 ) , verglichen mit plazebo ( n = 45 ) : 17 , 1 monate vs . 
ein effekt , der in der multivariaten analyse mit anderen faktoren ( alter , steroideinnahme , resektionsstatus , geschlecht , karnofsky - index , mgmt - status , mini - mental - test , rpaklasse ) deutlicher war ( hr 0 , 43 , p = 0 , 002 )  . 
die autoren argumentieren , dass nicht die berexpression von proangiogenen faktoren oder morphologisch starke angiogenese , sondern die empfindlichkeit fr eine vegf - blockade innerhalb der signaltransduktion das ansprechen auf bev definieren [ 710 ]  . 
 die geringere angiogenese des proneuralen subtyps knnte damit also hypothetisch insgesamt empfindlicher fr eine vegf - blockade sein . literatur kommentiert obschon sehr interessant , sollten die vorliegenden daten doch mit vorsicht bewertet werden , da es sich letztlich um eine retrospektive subgruppenanalyse handelt . 
in anbetracht der komplexen statistik bei der analyse von genexpressionsprofilen ist zudem eine externe validierung dieser avaglio - daten mit unabhngigen proben aus der rtog0825 - studie oder glarius - studie unbedingt erforderlich . fazit durch genexpressionsprofile lassen sich gbm - subtypen ( proneural , klassisch / proliferativ , mesenchymal ) definieren . 
beim proneuralen subtyp ist ein berlebensvorteil durch eine kombinationstherapie mit bev wahrscheinlich zu erwarten , auch wenn dieser sachverhalt erst noch weiter validiert werden muss . clemens seidel und rolf - dieter kortmann , leipzig einhaltung ethischer richtlinien interessenkonflikt c . 
phillips hs , kharbanda s , chen rh et al ( 2006 ) molecular subclasses of high - grade glioma predict prognosis delineate a pattern of disease progression , and resemble stages in neurogenesis . 
verhaak rg , hoadley ka , purdom e et al ( 2010 ) integrated genomic analysis identifies clinically relevant subtypes of glioblastoma characterized by abnormalities in pdgfra , idh1 , egfr , and nf1 . 
sulman ep , won m , blumenthal dt et al ( 2013 ) molecular predictors of outcome and response to bevacizumab ( bev ) based on analysis of rtog 0825 , a phase iii trial comparing chemoradiation ( crt ) with and without bev in patients with newly diagnosed glioblastoma ( gbm )  . 
bais c , rabe c , wild n et al ( 2014 ) comprehensive re - assessment of plasma vegfa ( pvegfa ) as a candidate predictive biomarker for bevacizumab ( bv ) in thirteen pivotal trials ( seven indications )  . 
jubb am , hurwitz hi , bai w et al ( 2006 ) impact of vascular endothelial growth factor - a expression , thrombospondin - 2 expression , and microvessel density on the treatment effect of bevacizurnab in metastatic colorectal cancer . 
brauer mj , zhuang gl , schmidt m et al ( 2013 ) identification and analysis of in vivo vegf downstream markers link vegf pathway activity with efficacy of anti - vegf therapies . 
kortmann1 3 strahlenther onkol ( 2016 ) 192 : 5562 doi 10.1007 / s00066 - 015 - 0909 - 0 undetected human papillomavirus dna and uterine cervical carcinoma association with cancer recurrence kae okuma hideomi yamashita terufumi yokoyama keiichi nakagawa kei kawana received : 29 may 2015 / accepted : 23 september 2015 / published online : 20 october 2015 springer - verlag berlin heidelberg 2015 abstract background the time course of human papillomavirus ( hpv ) dna clearance was studied in patients with carcinoma of the cervix during follow - up after primary radical radiotherapy ( rt )  . 
this study investigated the relationship between timing of hpv clearance and rt effectiveness . patients and methods a total of 71 consecutive patients who were treated for cervical cancer with primary radical radiotherapy and high - dose rate intracavitary brachytherapy with or without chemotherapy were enrolled in the study . 
diese studie untersuchte den zusammenhang zwischen dem zeitpunkt der hpv - eliminierung und der rt - effizienz . patienten und methoden insgesamt 71 aufeinanderfolgende patienten , die mit einer primren rt behandelt wurden , nahmen an der studie teil . 
die flle , bei denen keine hpv - dna entdeckt wurde , wurden auf einen zusammenhang zu rckfallfreiem berleben analysiert . original article 56 ergebnisse bei 13 patienten ( 18 % ) konnte keine hpvdna vor der rt festgestellt werden . 
von den 58 patienten , bei denen hpv - dna vor der behandlung identifiziert wurde , wurde die hpv - dna bei 34 % nicht whrend der behandlung und bei 66 % nicht nach der behandlung entdeckt . 
patienten , bei denen vor der behandlung keine hpv - dna identifiziert werden konnte , sollten sorgfltig nachbeobachtet werden und fr zustzliche oder alternative therapien in erwgung gezogen werden . keywords strahlentherapie hpv - clearance behandlungswirksamkeit zervikale neoplasien radiochemotherapie cervical cancer is one of the most common malignancies in japan . 
it has been reported that 95100 % of patients with invasive carcinoma of the cervix are infected with hpv [ 24 ]  . in the past , radical surgery was usually adopted in japan for cases up to stage iib ( figo , international federation of gynecology and obstetrics classification )  . 
 [ 5 ] reported that persistence of hpv deoxyribonucleic acid ( dna ) in the cervix at the end of irradiation in hpv - positive cervical carcinoma was highly predictive of local disease - free survival ( ldfs ) and overall survival ( os )  . 
also of interest was whether a change from negative to positive hpv status during the follow - up period after rt could be an indicator to predict local recurrence . materials and methods patients a total of 71 consecutive patients who were treated for cervical cancer with primary radical radiotherapy with or without chemotherapy at the university of tokyo hospital between december 2008 and november 2011 were evaluated . 
 external - beam radiation therapy ( ebrt ) consisted of whole pelvic irradiation of 30.639.6 gy in 1722 fractions and whole pelvic irradiation with midline block of 10.89.8 gy in 611 fractions ( 1.8 gy per fraction from monday to friday )  . 
whole pelvic irradiation was administered using a linear accelerator with four fields of a 10 mv photon beam ( two anteriorposterior opposed fields , and two lateral opposed fields ) and whole pelvic irradiation with a 4 cm wide midline block was administered using two anterior posterior opposed fields to reduce the dose to the rectum and the bladder . 
the clinical target volume ( ctv ) included all areas of gross and potentially microscopic disease , and included the upper half of the vagina , parametria , uterus , presacral region , and regional lymph node regions ( common , internal and external iliacs , and obturator regions )  . 
in about the first 32 patients , before the third and fourth treatment of hdricbt , biopsies of the cervix were taken from all patients and checked for residual malignant cells . 
 nineteen patients were treated with rt alone ( ebrt + icbt ) for the following reasons : patients with early stages , advanced age , poor renal or heart function , or refusal of chemotherapy . 
of these 52 patients , 25 patients received weekly cisplatin ( cddp ) of 3040 mg / m2 , 25 received tri - weekly nedaplatin ( ndp ; 80100 mg / m2 ) , and two received a paclitaxel and cddp regimen . 
response to radiotherapy was evaluated by pelvic examination , conventional cervical papanicolaou smear which was done in addition to the research samples , and review of tumor markers including serum squamous cell carcinoma ( scc ) antigen value and carcinoembryonic antigen ( cea )  . 
other imaging studies , such as mri , ultrasound , bone scintigraphy and positron emission tomography ( pet ) were not routinely performed . statistical analysis statistical analyses were performed using spss version 21.0. 
swab samples from the external os of the uterus were subjected to dna extraction with a qiaamp dna blood mini kit ( qiagen , venlo , the netherlands )  . 
briefly , a standard polymerase chain reaction ( pcr ) was conducted using the pgmy 09 / 11 l1 consensus primer sets [ 7 ] and human leukocyte antigen - dq ( hla - dq ) primer sets . 
of the 20 patients who had recurrence disease , hpv status did not change from negative to positive during the follow - up period after rt . the 3 - year cumulative disease - free survival ( dfs ) rate was 71 5.4 % for all 71 patients . 
 [ 14 ] investigated hpv status and e2 gene integrity as potential prognostic parameters for clinical outcome and prediction of rt response in 40 women with locally advanced cervical cancer treated with curative rt . 
for cervical carcinoma of the uterus , hpv infection induces cancerous changes of cervical cells through alterations in microrna expression patterns during consecutive stages of cervical cancer development and their association with chromosomal instability [ 17 ]  . 
in addition , whether hpv is detectable or not before treatment may be a biomarker of rt effectiveness for cervical carcinoma . conclusion the patients in whom hpv was not detected had the worst prognosis . 
kawana state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . in memoriam hans - jrgen eichhorn strahlenther onkol ( 2016 ) 192 : 6364 doi 10.1007 / s00066 - 015 - 0918 - z ehrenmitglied der degro jrgen richter klaus welker online publiziert : 1 . 
august 2015 ist hans - jrgen eichhorn , der langjhrige leiter der strahlentherapie an der robert - rssle - klinik in berlin - buch im alter von 95 jahren verstorben . 
 er gehrte zum kreis jener radiologen in deutschland , die nach dem krieg mitgeholfen haben , die strahlentherapie wieder aufzubauen und ihr zu ansehen zu verhelfen . hans - jrgen eichhorn wurde am 13 . 
1947 begann er die facharztausbildung am rntgeninstitut der sozialversicherungsanstalt chemnitz im fach radiologie unter lah bei ihm erhielt hans - jrgen eichhorn im jahr 1950 die facharztanerkennung fr radiologie und j . 
es war wohl die einmalige chance , die ihn kurz nach seiner facharztanerkennung an das gerade entstehende zentrum der ostdeutschen onkologischen forschung nach berlinbuch zog , dort etwas neues , einmaliges aufzubauen . 
so entstanden in den folgenden jahren wesentliche von eichhorn und seinen mitarbeitern stammende innovationen , so zum beispiel die einfhrung der computergesttzten bestrahlungsplanung , die im deutschsprachigen raum in berlin buch nachruf 64 zum ersten mal in der klinischen praxis angewandt wurde . 
weiterentwickelt , sondern auch in der tglichen routinebestrahlung eingesetzt . ab 1970 begann eichhorn mit einem team aus strahlentherapeuten , strahlenphysikern , strahlenbiologen und technikern , als zweite einrichtung in europa mit der vorbereitung und 1972 mit der durchfhrung der neutronentherapie am zyklotron des institutes fr kernforschung in dresden - rossendorf . 
die ergebnisse wurden in internationalen fachzeitschriften publiziert . zustzlich zur lokalen strahlentherapie wurde ab 1977 in seiner klinik fr patienten mit inoperablem kleinzelligem bronchialkarzinom eine obere und untere halbkrperbestrahlung durchgefhrt . im gesamten zeitraum seines wirkens war die strahlentherapie des bronchialkarzinoms ein hauptanliegen seiner arbeit und er galt als absoluter experte auf diesem gebiet . sein wissenschaftliches vermchtnis hat er in einer broschre zusammengefasst ( die geschichte der strahlentherapie an der robert - rssle - klinik in berlin buch 1950 bis 1984 strahlenbiologische und strahlentherapeutische forschungsarbeiten ) , die er mit 93 jahren begonnen und kurz vor seinem 95 . 
nach der wiedervereinigung , zu der zeit war er bereits 5 jahre emeritiert , aber immer noch an der entwicklung der strahlentherapie sehr interessiert , wurde eichhorn 1998 ehrenmitglied der deutschen gesellschaft fr radioonkologie und im jahre 2000 ehrenmitglied der schsischen radiologischen gesellschaseine wissenschaftlichen aktivitten sind in fast 200 publikationen niedergelegt . 
dass er trotz der erfolge der spteren generation von fachkollegen nicht so prsent ist , liegt vorwiegend daran , dass ihm , wie er es einmal selbst formulierte , der politische wind in der ddr immer ins gesicht blies , was zur folge hatte , dass durch reiseund publikationseinschrnkungen sein wissenschaftliches auftreten auerhalb des ostblocks stark eingeschrnkt war . eichhorn war eine starke , zuverlssige , geradlinige und fordernde fhrungspersnlichkeit , die seine mitarbeiter und seinen bereich nach auen abschirmte . 
die besondere atmosphre der strahlentherapie an der robert - rssle - klinik in berlin - buch fhrte dazu , dass sich auch noch 30 jahre nach seinem berufsende viele ehemalige mitarbeiter regelmig treffen . 
welker1 3 deeskalation der radiochemotherapie bei prognostisch gnstigen hpv - assoziierten plattenepithelkarzinomen des oropharynx strahlenther onkol ( 2016 ) 192 : 273275 doi 10.1007 / s00066 - 016 - 0953 - 4 r . 
februar 2016 springer - verlag berlin heidelberg 2016 hintergrund und ziel hpv - assoziierte oropharyngeale karzinome gelten mittlerweile als eine eigenstndige onkologische entitt mit besserer prognose als die durch tabak oder alkohol bedingten karzinome dieser region . 
in der vorliegenden phase - ii - studie prfte eine amerikanische studiengruppe prospektiv , ob die wiederholt beschriebene hhere sensibilitt auf radiochemotherapie ( rct ) dieser entitt eventuell eine reduktion der strahlenbzw . 
cisplatin - dosis im sinne einer deeskalation der rct rechtfertigt . studiendesign einschlusskriterien waren histologisch gesicherte plattenepithelkarzinome des oropharynx oder zervikale lymphknotenmetastasen von unbekannten primrtumoren ( cup ) ct03 cn02c cm0 mit positivitt fr hpv ( in der fluoreszenz - in - situ - hybridisierung , fish ) oder p16 ( immunhistochemisch > 70% positive zellen )  . 
bei exrauchern , die mindestens 5 jahre zuvor das rauchen aufgegeben hatten , durften damals auch bis zu 30 pack years konsumiert worden se die tumoren wurden mit 60 gy bei 2 gy einzeldosis mittels imrt bestrahlt , die elektiven lymphabflsse mit bis zu 54 gy . 
primrer endpunkt der phase - ii - studie war die histopathologisch komplette remission ( pcr )  . originalpublikation chera bs , amdur rj , tepper j et al ( 2015 ) : phase 2 trial of de - intensified chemoradiation therapy for favorablerisk human papillomavirus - associated oropharyngeal squamous cell carcinoma . 
das mittlere alter betrug 61 jahre , fast 90% waren mnnlich , ber 80% nichtraucher und 15% < pack years ; 64% waren hpvund p16positiv , 36% hpv - negativ und p16 - positiv . 
von den 6 patienten mit histopathologisch partieller remission zeigte die hlfte residuelle tumorfoci von < 1 mm . schlussfolgerungen der autoren angenommen wurde erfahrungsgem eine pcr - rate von 87% nach standarddosierung der rct . 
im unterschied zu den durch die klassischen noxen tabak und alkohol induzierten karzinome scheint insbesondere das lymphoepithelial retikulierte kryptenepithel der gaumentonsillen und des zungengrunds von der onkogenen transformation durch die hpv - hochrisikotypen betroffen zu sein [ 1 ]  . 
im rahmen der therapieoptimierungsstudien der gesellschaft fr pdiatrische hmatologie und onkologie ( gpoh ) wird in diesen fllen unter der voraussetzung einer adjuvanten interferontherapie bereits jetzt lediglich eine gesamtdosis von 60 gy eingestrahlt und bei erreichen einer pcr durch die neoadjuvante chemotherapie die strahlendosis weiter auf 54 gy deeskaliert [ 4 ]  . 
auch bei erwachsenen patienten wurde bereits ber erste erfahrungen mit einer solchen dosisdeeskalation bei dieser tumorentitt berichtet [ 5 ]  . die vorliegende , kleine phase - ii - studie zeigt diesem zusammenhang bei prognostisch gnstigen , hpvassoziierten plattenepithelkarzinomen des oropharynx eine beeindruckende und ermutigende pcr - rate von fast 90% nach normofraktionierten 60 gy mit einer nach dem verstndnis der amerikanischen studiengruppe auch deeskalierten simultanen chemotherapie mit cisplatin mono . 
als endpunkt ist die pcr zwar aussagekrftiger als eine klinische cr , es fehlt aber noch der direkte randomisierte vergleich mit einem kontrollarm in standarddosierter rct , um eine onkologische nichtunterlegenheit hinsichtlich berleben beweisen zu knnen . 
weiterhin sollte auch randomisiert die gut begrndbare annahme einer geringeren therapieassoziierten toxizitt durch die deeskalation prospektiv getestet werden : sind unterschiede in der toxizitt messbar und wirken sich diese auch tatschlich auf die lebensqualitt der patienten aus ? erst dann wre die deeskalation nicht allein onkologisch sicher , sondern wrde den patienten auch eine sprbare erleichterung bieten . 
zudem ist natrlich langfristig interessant , ob die dosis noch weiter als auf 60 gy reduziert werden kann , zumindest bei einigen subgruppen mit geringer tumorlast , zum beispiel abhngig von prognostischen markern oder dem therapieansprechen unter der behandlung analog zum vorgehen beim ebvassoziierten , undifferenzierten nasopharynxkarzinom . in den usa rekrutiert in diesem zusammenhang bereits eine phase - iii - studie fr die adjuvante situation nach transoraler r0 - resektion eines nodalpositiven oropharynxkarzinoms mit extranodaler ausbreitung [ 6 ] : hierbei wird eine bestrahlung mit 60 gy gegen eine rct mit cisplatin 6 40mg2 randomisiert . 
einen anderen ansatz verfolgt der sinai robotic surgery trial fr hpv - positive oropharynxkarzinome : zur deeskalation wird auf eine adjuvante behandlung nach r0 - resektion eines low risk - tumors [ pt12 , pn1pn2b , l0 , pn0 , < 3 befallene lymphknoten , kein extracapsular spread ( ecs ) , kein befall ber level iii ] verzichtet [ 7 ]  . abschlieend ist bezglich des im rahmen der arbeit geschilderten studienkonzepts kritisch die bei allen patienten regelhaft durchgefhrte post - rct - neckdissektion zu hinterfragen , die auch bei patienten mit einer cr erfolgt . 
ward g , mehta v , moore m ( 2015 ) morbidity , mortality and cost from hpv - related oropharyngeal cancer : impact of 2 - , 4and 9 - valent vaccines . 
buehrlen m , zwaan cm , granzen b et al ( 2012 ) multimodal treatment , including interferon beta , of nasopharyngeal carcinoma in children and young adults : preliminary results from the prospective , multicenter study npc - 2003 - gpoh / dcog . 
wolff ha , rdel rm , gunawan b et al ( 2010 ) nasopharyngeal carcinoma in adults : treatment results after long - term followup with special reference undifferentiated carcinomas . 
j cancer res clin oncol 136 : 8997 post - operative adjuvant therapy de - intensification trial for human papillo - mavirus - related , p16 + oropharynx cancer adept . 
hermann rm , christiansen h , rdel rm ( 2013 ) lymph node positive head and neck carcinoma after curative radiochemotherapy : a long lasting debate on elective posttherapeutic neck dissections comes to a conclusion . 
 studienprotokolls in die tgliche klinische praxis eine erhebliche bertherapie bedeuten , die nicht durch studienergebnisse gerechtfertigt ist [ 8 ]  . literatur fazit hpv - assoziierte oropharyngeale karzinome sind eine eigene klinische entitt mit besserem therapieansprechen und gnstigerer prognose , insbesondere im rahmen einer rct . vor diesem hintergrund erscheinen forschungsanstze zur therapieoptimierung der rct durch dosisdeeskalation plausibel , um therapieassoziierte morbiditten bei unverndert hohen kurationsraten zu verringern . solche therapiekonzepte drfen derzeit nur im rahmen kontrollierter klinischer studien erprobt werden . 
solange keine neuen ergebnisse aus prospektiven , randomisierten studien vorliegen , sollten auch hpv - positive kopf - halstumoren in der routine weiterhin nach den publizierten leitlinienstandards behandelt werden , zum beispiel analog der leitlinie diagnostik und therapie des mundhhlenkarzinoms [ 9 ]  . einhaltung ethischer richtlinien interessenkonflikt r . 
christiansen , hannover deeskalation der radiochemotherapie bei prognostisch gnstigen hpv - assoziierten plattenepithelkarzinomen des oropharynx1 3 strahlenther onkol ( 2016 ) 192 : 223231 doi 10.1007 / s00066 - 015 - 0935 - y prostate cancer treated with image - guided helical tomotherapy and image - guided linac - imrt correlation between high - dose bladder volume , margin reduction , and genitourinary toxicity sonia drozdz1 michael schwedas2 henning salz2 susan foller3 thomas g . 
wendt1 received : 9 august 2015 / accepted : 12 december 2015 / published online : 7 january 2016 springer - verlag berlin heidelberg 2015 ig protocols based on setup error correction and a limited number of imaging sessions . 
22 gy in the linac group , we observed less gu toxicity after tomotherapy . conclusion intraprostate fms allow for small safety margins , help decrease imaging frequency after setup correction , and minimize the dose to bladder and rectum , resulting in lower gu toxicity . 
in addition , imrt delivered with tomotherapy helps to avoid hotspots in the bladder neck , a critical anatomic structure associated with post - rt urinary toxicity . keywords tomotherapy fiducial markers adverse effects organs at risk margins abstract background we compared different image - guidance ( ig ) strategies for prostate cancer with high - precision ig intensity - modulated radiation therapy ( imrt ) using tomotherapy ( accuray inc . , madison , wi , usa ) and linear accelerator ( linac ) - imrt and their impact on planning target volume ( ptv ) margin reduction . 
the purpose of this study was to quantify whether the treatment delivery technique and decreased margins affect reductions in bladder toxicity . patients and methods setup corrections from 30 patients treated with helical tomotherapy and 30 treated with a linac were analyzed . 
 in der vorliegenden studie sollte quantifiziert werden , ob das bestrahlungsverfahren und reduzierte sicherheitssume einfluss auf die verringerung der blasentoxizitt haben . patienten und methoden es erfolgte eine analyse der lagerungskorrekturen von 30 patienten mit helikaler tomotherapie und weiteren 30 patienten , die mit einem linac behandelt wurden . 
bei allen patienten wurde die gastrointestinale ( gi ) und urogenitale ( gu ) toxizitt dokumentiert und mit dem bestrahlungsverfahren in beziehung gesetzt . ergebnisse bei anwendung einer radiotherapie mit goldmarkern konnte durch berechnung einer lagerungskorrektur aus den ersten 3 fraktionen und einer ig - untersuchung an jedem zweiten tag eine marginreduktion von bis zu 3 , 1 , 3 , 0 und 4 , 8 mm in links - rechts - , superiorinferiorer bzw . 
obwohl das blasenvolumen in der tomotherapiegruppe mit mittleren dosen von 35 gy behandelt wurde , whrend die linac - gruppe 22 gy erhielt , war eine geringere urogenitale toxizitt nach tomotherapie zu verzeichnen . schlussfolgerung goldmarkerbasierte igrt der prostata ermglicht kleinere sicherheitssume . 
darber hinaus lassen sich mit imrt unter einsatz der tomotherapie hotspots am blasenhals vermeiden , einer kritischen anatomischen struktur , die im zusammenhang mit der harnwegstoxizitt nach radiotherapie steht . radiotherapy ( rt ) is an important modality in the primary or postoperative treatment of prostate cancer . 
external beam radiation therapy ( ebrt ) has progressed over the past 25 years from a conventional four - field box technique , via three - dimensional conformal rt , to intensity - modulated rt ( imrt ) , with image - guided rt ( igrt ) representing the most precise option [ 14 ]  . 
 in addition , the prescribed radiation dose is often limited by the tolerance of adjacent critical organs , in particular the bladder and rectu significant interfraction prostate motion within the pelvis is well established [ 5 , 6 ] and can lead to geographic missing of the target . 
helical tomotherapy ( ht ) and a linear accelerator ( linac ) on - board detector are platforms that incorporate volumetric megavoltage ( mv ) computed tomography ( ct ) imaging to visualize and correct any setup discrepancies , with a kilovoltage ( kv ) ct simulation performed prior to treatment . one possibility for matching the kvct and the mvct is to use bony anatomy ; however , the prostate is not attached directly to bone [ 8 ]  . 
a common method to decrease geographic mistargeting of the prostate is to implant fiducial markers ( fms ) , which can be visualized on an mv beam and serve as a surrogate for prostate position [ 9 , 10 ]  . 
the stability of these fiducials has been reported [ 11 , 12 ]  . we treated prostate cancer patients with high - precision ig - imrt using tomotherapy ( accuray inc . , madison , wi , usa ) and linac . 
two different treatment protocols were analyzed retrospectively : in trial a 30 patients were treated with linac oncor ( siemens , erlangen , germany ) ; in trial b , 30 patients were treated using the tomotherapy unit . 
patients demographic and treatment characteristics are given in table 1 . preparation and treatment planning for patients in trials a and b , three fms were implanted under transrectal ultrasound guidance . 
after 1 week of adaptation , a treatment planning kvct was performed with patients in the supine position , using a large bore lightspeed scanner ( general electric , chicago , il , usa ) and a slice thickness of 1.25 mall patients were asked to have a filled bladder and drink 500 ml of oral contrast medium half an hour before scanning . 
to ensure emptying of the rectum , laxatives were given the evening before , and an enema ( mikroklist ) was administered prior to ct simulation the next morning . the clinical target volume ( ctv ; including the seminal vesicles in high - risk patients ) , bladder , rectum from the anal verge to the beginning of the sigmoid colon , and femur heads were contoured manually using the oncentra masterplan treatment planning systeusing the in - built algorithm , the planning target volume ( ptv ) was generated by expansion of the ctv with an isotropic 8 - mm margin , except for a 5 - mm margin posteriorly . 
dose constraints and acceptance criteria for the bladder , rectum , and femoral heads were the same for the ht and linac groups . all patients were treated with imrt given at 2.0 gy per fraction specified to the encompassing ptv isodose ( icru 62 ) to a total dose 7478 gy ( radical rt )  . target localization and treatment delivery in all patients , daily positioning was performed using the skin markers , while ct was performed according to the room laser coordination system ( lap , lneburg , germany )  . 
 ig was performed in all patients immediately before irradiation in the treatment position . ig for the linac group ( trial a ) was achieved with mv cone beam ( cb ) ct and a resolution of 512 pixels . 
the shift between these two registration algorithms was the setup error caused by interfraction prostate motion . for each patient in trial b , daily mv fan beam ( fb ) ct scans with a 2 - mm interslice distance were acquired prior to the daily treatment . 
the delivered ig dose for the entire treatment was about 60 cgy . prostate cancer treated with image - guided helical tomotherapy and image - guided linac - imrt1 3 226 fig . 
1 image guidance protocols : ig image guidance , 1.1 daily imaging , 1.2 initial fraction and imaging every 2nd day , 1.3 initial fraction and weekly imaging ; 2.2 correction of mean setup error from the first three fractions and imaging every 2nd day , 2.3 correction of mean setup error from the first three fractions and weekly imaging ; 3.2 correction of mean setup error from the first five fractions and every 2nd day imaging , 3.3 correction of mean setup error from the first five fractions and weekly imaging . 
 the deviation of the setup , based on imaging , was calculated in the leftright ( lr ) , superiorinferior ( si ) , and anteriorposterior ( ap ) dimensions . error analysis and statistics the day - to - day variation in the position of the prostate relative to the skin markings is the interfraction motion and internal movement of the prostate over the course of a single treatment is the intrafraction motion . 
ig design 1 involved using the first fraction to correct the systematic error combined with different frequencies of repetition of the ig for correcting the random error during the treatment . 
therefore , it was very important to accurately estimate this error by using new ig protocols . in the new ig protocols , we calculated a systematic setup error correction as the average displacement over 1 , 3 , or 5 consecutive days . 
the chi - square test or fishers exact test was used with a significance level set at = 0.05. follow - up all patients were continuously followed before and after rt . 
patients were scheduled for follow - up visits at 6 weeks and then 1 year after the end of treatment , and once a year thereafter until 5 years of follow - up were completed . 
documentation of adverse effects included changes in karnofsky performance status , urinary retention , development of urethral stricture , hematuria , nocturia , urinary frequency , dysuria , and fecal incontinence . 
a strict definition of the grading system was used for grades 14 : grade 1 was defined as minimal side effects not influencing activities of daily living and grade 4 as life threatening , in which urgent treatment or interventions were needed . results interfraction prostate displacement resulting from bony anatomy fusion for all patients ( trials a and b ) , a total of 2220 fractions were analyzed . 
however , this does not include all uncorrectable uncertainties ( intrafraction motion [ 1720 ] , flat panel , ct resolution , and treatment planning calculation grid size )  . 
therefore we created an ig baseline including the aforementioned uncertainties . these uncertainties required a minimum margin of 3 mm in the lr and 5 mm in the si and ap directions . 
in addition , with this design , the imaging exposure could be reduced to half compared to daily imaging . finally , if only bony anatomy was used for alignment , the required margins would be 8 ( lr ) , 9 ( si ) , and 12 mm ( ap )  . toxicity although igrt with fms was performed in trials a and b ( table 1 ) , we observed more symptoms of gu toxicity grades 13 in the linac - imrt group compared to patients treated with tomotherapy - based imrt . 
no grade 3 gu toxicity occurred in the fiducial - based tomotherapy group and , overall , no fecal ( gi ) or grade 4 gu toxicity was observed in any group . 
thus , an additional nonuniform larger margin in the posterior and inferior directions based on ig bone fusion would be needed to cover the ctv because the organ motion is not included . 
the goal during ig should be minimization of exposure without altering or even with improvement in patient benefit . analysis of the data in table 3 showed that all scenarios were effective in reducing the mean systematic error compared to no igrt . 
mvcb megavoltage cone beam , mvfb megavoltage fan beam prostate cancer treated with image - guided helical tomotherapy and image - guided linac - imrt1 3 228 lr ( mm ) si ( mm ) ap ( mm ) lr ( mm ) si ( mm ) ap ( mm ) lr ( mm ) si ( mm ) ap ( mm ) table 3 systematic ( ) and random ( ) errors and population - based margins calculated for the no image guidance ( ig ) scenario and for each combination of ig protocol . 
these findings are in agreement with those of previous studies [ 2529 ] and can be explained as follows : positioning in the ap dimension is variable because of variable and nonreproducible daily filling of the rectum ; therefore , the random error is higher in fm - based igrt . 
the mean maximum dose ( hotspot ) for a created structure bladder minus ptv was 3 gy higher with linac - imrt technique compared to tomotherapy - imrt ( 77 vs 74 gy ) using the same constraints . 
the bladder neck was located within this more highly irradiated volume , which may explain the increased bladder toxicity observed after linac - based imrt . there is evidence to suggest that the mean bladder dose has only a small influence on bladder toxicity . 
retrospective reports have drawn associations between various factors such as urethral dose , prostate volume , or use of neoadjuvant androgen deprivation therapy and increased risk of significant acute urinary toxicity [ 30 , 31 ]  . 
several small retrospective reports have addressed the correlation of urinary toxicity with the dose to the lower urinary tract segments [ 32 ] and described an association between the dose to the urethral base / bladder neck and urinary toxicity [ 33 ]  . 
a recent dutch trial demonstrated that a volume > 2 cm3 receiving a high dose ( 80 gy ) and a > 47 - gy dose administered to the trigone are associated with a significantly increased risk of late urinary obstruction [ 34 ]  . 
b mean anteriorposterior ( ap ) deviation from bone and fm fusion over whole treatment time detecting interfractional variability in prostate position and avoiding movement of the bladder neck toward a higher isodose level . 
the combination of small margins , less - frequent imaging , and still - precise rt technologies allowing for high tumor control rates and low late toxicity paves the way for hypofractionated protocols in the future . 
besides reducing the dose to the entire bladder , omitting hotspots in the bladder neck will probably lower the risk of bladder toxicity and should therefore be an important aspect in treatment plan optimization . 
more studies are needed to validate this strategy . acknowledgments sd conceived the study ; acquired , analyzed , and interpreted the data ; reviewed the literature ; and wrote the manuscript . 
ap anteriorposterior , si superiorinferior , lr left right , ig image guidance , ptv planning target volume many studies have demonstrated an improvement in the frequency and grades of gi and gu toxicity with advances in dose conformity and tumor targeting [ 35 , 36 ]  . 
tomotherapy makes it possible to minimize the bladder volume irradiated with high doses by producing steeper high - dose gradients than linac - based step - and - shoot imrt . 
 the asymptotic significance according to pearsons chisquare test ( p = 0.078 ) suggests a trend toward a difference in gu toxicity between these two imrt techniques . conclusion high - precision igrt of prostate cancer should be based on implantation of intraprostatic f these are helpful for prostate cancer treated with image - guided helical tomotherapy and image - guided linac - imrt1 3 230 compliance with ethical guidelines conflict of interest s . 
wendt state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 209215 doi 10.1007 / s00066 - 016 - 0944 - 5 individualized radiotherapy by combining high - end irradiation and magnetic resonance imaging stephanie e . 
wilkens1 , 2 received : 20 august 2015 / accepted : 14 january 2016 / published online : 6 february 2016 springer - verlag berlin heidelberg 2016 abstract image - guided radiotherapy ( igrt ) has been integrated into daily clinical routine and can today be considered the standard especially with high - dose radiotherapy . 
die klinischen fragestellungen umfassen unter anderem strategien zur dosiseskalation , berwachung von gewebevernderungen whrend einer strahlentherapie sowie bildgebung unter therapie ohne zustzliche dosisapplikation . schlsselwrter bildgesttzte radiotherapie individualisierte medizin magnetresonanzgesttzte radiotherapie organschonende behandlungen risikoorgane imaging technology is one of the driving forces towards individualized radiotherapy ( irt )  . 
the initial most important step toward that goal was ct - based treatment planning , followed by integrating other image modalities like review article 210 magnetic resonance imaging ( mri ) and positron emission tomography ( pet )  . 
rt has a clear advantage compared to surgerynoninvasive delivery of tumoricidal doses with utmost precision , calculation of doses and dose delivery within short treatment times , outpatient applications , and dependable prediction of effects . 
compared to surgeons , radiation oncologists cannot see directly into the tumor bed or involved regions and adjacent normal tissue , therefore , their work is highly dependent on advanced imaging . a real breakthrough was observed with the technologies of megavoltage fan - beam and kilovoltage ( kv ) cone - beam ct mechanically coupled to a linac . 
this development , termed image - guided radiotherapy ( igrt ) , is a first approach of image guidance in treatment delivery , yet as an off - line mode with imaging once per fraction and no motion management capability . 
however , motion artifacts , deformation of organs and low contrast resolution of the x - ray imagers restrict the capabilities of igrt . these limitations have motivated scientists to seek alternative approaches based on mri with its superior soft tissue characterization which is essential in all aspects of the target volume definition [ 1 ]  . 
mrgrt is expected to revolutionize the process of radiation treatment : in contrast to the conventional procedure to deliver a multifraction treatment according to an initial treatment plan optimized for a planning target volume ( ptv ) , mrgrt with its unique capacity of high - quality online imaging may be performed as a sequence of fractions each optimized by online dose planning . 
with mrgrt , target volume definition , reduction of normal tissue exposure , and compensation of motion artifacts can be significantly improved . to what extent methods of functional mr imaging ( fmri ) , like dynamic susceptibility contrast ( dsc ) imaging , diffusion tensor imaging ( dti ) , dynamic contrast - enhanced ( dce ) imaging , diffusion - weighted imaging ( dwi ) as well as mr spectroscopy would be feasible in an online mode , has to be investigated as a long - term goal . 
first , the greatest benefit will be the direct monitoring of anatomy of tumor and normal tissue while a patient is in treatment position which allows precise correlation with the planned treatment and leads to direct re - planning action , when required . currently , there is a growing interest in mrgrt after it was commercially launched . 
with this paper we want to emphasize the clinical potential of mrgrt and give some examples where mrgrt is expected to have the most significant impact in radiotherapy . current physical approaches two approaches of mrgrt have been pursued , separated systems , i.e. 
shuttle systems with the treatment couch movable between the mr and the linac or the mr - on - rails concept , or as the technically more ambitious solution fully integrated systems ( hybrid mr treatment unit )  . 
since the most appealing feature of mr guidance during treatment delivery is the control of motion artefacts , mrgrt basically favors the latter approach , i.e. , the in - room concepts . 
lagendijk pioneered with the development of an integrated mr - linac system combining a 1.5 t achieva scanner ( philips ) with a 6 mv linac ( elekta ) rotating on a ring in the midtransversal plane of the mr imager [ 10 ]  . 
the advantages of online - mri are at least two - fold ; however , the clinical benefit increases exponentially : on the one hand , the online - imaging available today with kv or mv imaging only provides inaccurate information on the real tumor extent due to poor contrast resolution . 
on the other hand , mri is not yet available online , and all data acquired via off - line mri have to be fused and are associated with a time difference . regarding tumor delineation , the real value of online kv or mv imaging mainly lies in image guidance or observation of any coarse changes in anatomy or tumor geometry . 
with mrgrt , images can be recorded via mri while the patient is in treatment position , high - resolution depiction of tumor and normal tissue is possible in one session while radiation treatment is ongoing , and fusion with the actual treatment plans comes automatic . 
it must be kept in mind , however , that additional developments in mr - based treatment planning are necessary since today no electron density is available on mr images and , thus , direct replanning requires additional ct information or processing . there is an additional aspect to consider : while ct is associated with an additional dose to the patient , which in relation to a curative dose of a radiotherapy ( rt ) treatment is minimal , mri does not add any further dose . 
this is underlined by the alara principle . potential in brain tumors for brain lesions , issues of target definition and especially hitting the target have been solved to a certain extent [ 14 16 ]  . 
a major drawback , however , is the information available or changes within these structures early during treatment , which could potentially influence treatment adaption , or predict early and late side effects of rt . 
for gliomas it is known that tumor and / or treatment - related edema are difficult to distinguish from low - grade tumor regions [ 17 , 18 ] ; moreover , changes in brain tissue strongly correlate to applied doses , and doses as low as 5 gy can induce such alterations [ 19 ]  . 
dti is a tool to visualize fiber tracks , which in combination with anatomical models including individualized radiotherapy by combining high - end irradiation and magnetic resonance imaging1 3 212 brain barriers , ventricles , as well as transition from white to gray matter contributes to the probability of tumor cell invasion , leading to an increased risk for recurrence [ 20 ]  . 
online availability of this information will help determine treatment response , help delineate resection and target volume margins adaptively , and to calculate recurrence probabilities and adjust dose patterns accordingly [ 25 , 26 ]  . subvolume segmentation the information on dose to and changes within organ subvolumes has been shown to be responsible for physiological changes , i.e. 
especially in the head - and - neck region , precise information on tumor hypoxia is of significant radiobiological importance for rt ; however , based on tumor and normal tissue alterations hypoxic regions may be altered during a course of rt . 
having these functional parameters during planning and during each fraction of the treatment eliminates uncertainties in image coregistration with diagnostic mr due to anatomical or positional variation . identification of subvolumes provides an essential basis for dose escalation strategies , especially for tumors where a possible increase in local dose can improve the therapeutic window , inclusion of online mri opens a new horizon . 
 definitive treatment of gastrointestinal ( gi ) and thoracic malignancies will benefit from such approaches : for lung , esophagus as well as rectal cancer definitive treatment strategies have been established ; however , for subgroups of patients neoadjuvant or sequential treatments with surgery are still followed due to the insufficient dose application possible with current rt strategies based on insufficient online imaging . 
centrally located lung lesions with lymph node involvement present substantial difficulties for the radiation oncologist [ 30 , 31 ] : large lesions lead to high lung doses and fibrosis , often limiting curative dose concepts . 
in addition , ct - based imaging as well as pet imaging is difficult for adaptive rt treatment due to blurry tissue contours , limited tracer uptake when chemotherapy is involved , and restricted soft - tissue contrast . 
with integrated mri , tumor volume kinetics as well as lymph node anatomy can be assessed during rt , and online dose algorithms allow for adaption of the dose to shrinking tumors . 
today , occult lymph node metastasis and intramural tumor extension may lead to underestimation of the gross tumor volume ( gtv ) and thus to a marginal miss in routinely performed ct and endoscopic imaging . 
mri using high - resolution t2 - weighted sequences and dwi enhanced by fdg - pet help stratify for dose - escalation locally for esophageal tumors [ 32 , 33 ]  . 
however , the success of rt in the definitive setting clearly depends on rt dose and tumor targeting [ 34 ]  . organ motion the esophagus is a mobile organ and its treatments are also influenced by the motion of the surrounding lungs and the heart [ 3537 ]  . 
especially the heart should be in focus since it has been shown from breast cancer patients that the dose to the heart and its subvolumes correlates significantly with morbidity [ 38 , 39 ]  . 
motion management in this setting includes information of target organ motility and localization of the target volume during the breathing phases , which can be monitored by 4d - ct , however more optimally , by cine - mri [ 40 , 41 ]  . 
inclusion of mri will enable further dose - escalation strategies to small subvolume remnants during and after rt thus fueling the rationale of dose - escalated organ - sparing definitive rt for a growing number of indications . pelvis there are current discussions in interdisciplinary tumor boards regarding how to deal with the 20 % subset of patients with rectal cancer demonstrating a complete response after chemoradiation ( crt ) [ 44 , 45 ]  . 
mri is crucial in monitoring the pelvis in cases of clinically complete response following crt , in a watchand - wait approach , and in detecting early salvageable recurrences [ 4547 ]  . mri enables precise delineation of mesorectal fascia involvement , the high spatial resolution and t2 - weighted images help distinguish tumor from normal rectal tissue and surrounding fat , as well as definition of different therapeutic responses , prediction of nodal downstaging as well as radiologic tumor regression grade . 
this will also impact other indications which are to date already treated with high - dose rt such as prostate cancer , where inclusion of online mri will enable even higher dose delivery to defined subregions of the prostate [ 50 , 51 ]  . the clinical benefit of mrgrt will be at least twofold : reduction of toxicity when appropriate and preservation of normal tissue function , as well as increase in tumor control for improved oncological outcome . 
leading to a continuous improvement of the therapeutic window . specific challenges despite the great prospects for clinical applications as described above , it must be kept in mind that many technological challenges have to be solved to make this happen . first of all , research continues to be performed to identify the most suitable mr sequences which are fast enough for online imaging and at the same time not susceptible to geometrical image distortions ( which is a potential disadvantage of mr imaging compared to x - ray ct when accurate targeting is required )  . 
furthermore , functional mri techniques need to be refined to yield the relevant information without long acquisition times when tumor heterogeneity shall be accounted for by targeting biologically relevant subvolumes . secondly , real - time image guidance requires fast online treatment planning and adaptive replanning strategies to make efficient use of the clinical potential of mrgrt . 
 then , dose calculation algorithms have to deal with the fact that electron density is not directly accessible from mr images alone ( rather than from ct hounsfield units ) [ 52 ]  . 
 here , approaches like a pseudo - ct generated by deformable image registration with a previously acquired ct of the same patient or with a more general predefined mri atlas with coregistered ct images [ 53 , 54 ] or by material assignment based on an ( auto - ) segmented mr image [ 55 , 56 ] have to be used . 
by dedicated monte carlo [ 57 , 58 ] or deterministic methods , [ 59 ] as this can lead to a warping of the dose distribution or to local hot spots in the dose due to the electron return effect at material interfaces [ 13 ]  . 
these issues are especially important for lung due to susceptibility artifacts and density changes . another challenge is related to dosimetry and quality assurance ( qa ) of radiation in a magnetic field . 
current dosimetry devices for machine qa are being adopted to be mr compatible , and the effects of the magnetic field on secondary particles in ionization chambers for absolute dosimetry have to be accounted for . 
 however , technical difficulties include online motion compensation by inclusion of mr as well as online treatment plan adaption which essentially will close the loop from planning to dose delivery . compliance with ethical guidelines conflict of interest s.e. 
mrz 2016 springer - verlag berlin heidelberg 2016 hintergrund und ziel die indikation zur bestrahlung der mammaria - interna - lymphknoten ( imni ) wurde in den letzten jahren eingeschrnkt , da eine erhhte kardiotoxizitt befrchtet wurde . 
ziel der vorliegenden studie der dnischen breast cancer study group [ 8 ] war es , den effekt der imni auf das berleben zu untersuchen . patientinnen und methode in einer prospektiven populationsbasierten kohortenstudie wurden 3089 nodalpositive patientinnen mit mammakarzinom ( 2003 2007 ) eingeschlossen . 
das mediane originalpublikation thorsen lb , offersen bv , dano h et al ( 2016 ) dbcg - imn : a population - based cohort study on the effect of internal mammary node irradiation in early nodepositive breast cancer . 
sautter - bihl marie - luise.sautter - bihl@klinikum - karlsruhe.de 1 klinik fr radioonkologie und strahlentherapie , stdtisches klinikum karlsruhe , karlsruhe , deutschland 2 department of radiotherapy and radiation oncology , lkh salzburg , paracelsus medical university hospital , salzburg , sterreich follow - up betrug 8 , 9 jahre . 
bei patientinnen mit nur 13 befallenen lymphknoten und medialem tumorsitz zeigte sich nach imni eine hr von 0 , 80 ( 95% - ki 0 , 581 , 10 ) , im gegensatz dazu bei lateralem sitz eine hr von 1 , 13 ( 95%ki 0 , 841 , 51 )  . schlussfolgerung der autoren in dieser populationsbasierten kohortenstudie bewirkte die imni eine verbesserung des oas bei patientinnen mit nodalpositivem mammakarzinom . kommentar da die lateralitt eines mammakarzinoms per se das berleben nicht beeinflusst [ 4 ] , kann die signifikante verbesserung des 8 - jahres - oas um 3 , 7% in der dnischen literatur kommentiert1 3 studie dem einzigen unterschied in der behandlung , d . 
die auswertung erfolgte zwar fr das gesamtkollektiv nach dem intention - to - treat - prinzip , jedoch ergab eine zustzliche analyse der 2869 patientinnen , die tatschlich nach der vorgabe behandelt wurden ( as treated ) fr das oas ebenfalls eine hr von 0 , 82 ( 95% - ki 0 , 710 , 94 ) zugunsten des imni - kollektivs . die resultate aus bisherigen populationsbasierten studien sind hinsichtlich der effektivitt einer imni uneinheitlich , deuten jedoch darauf hin , dass patientinnen mit medialem / zentralem tumorsitz eher profitierten als solche mit lateral gelegenen tumoren [ 2 , 3 ]  . 
die vorliegende untersuchung unterscheidet sich von bislang publizierten kohortenstudien durch ihr prospektives design , in dem die indikation fr eine imni nicht auf der basis von risikofaktoren oder tumorsitz in der brust gestellt wurde , sondern ausschlielich aufgrund der lateralitt . 
die beschriebenen kollektive zeichnen sich auch durch eine weitgehende homogenitt aus , da in einem definierten und relativ kurzen zeitraum von 4 jahren alle frauen in den nationalen tumorzentren einheitlich behandelt wurden . die resultate der dnischen gruppe unterscheiden sich hinsichtlich des oas von der einzigen randomisierten studie [ 5 ] , die sich selektiv der wirksamkeit der imni im vergleich zu einer lymphabflussbestrahlung ohne imni widmete . 
die effekte einer alleinigen rt der brust oder brustwand im vergleich mit einer zustzlichen bestrahlung aller lymphabflussgebiete wurde in zwei groen randomisierten studien geprft [ 6 , 9 ] , ohne jedoch den anteil der imni an den verbesserten berlebensraten quantifiziert zu knnen . 
interessant ist die subgruppenanalyse von patientinnen mit lateralem tumorsitz : im gesamtkollektiv hatte die imni hier keinen effekt auf das berleben ( hr 0 , 97 ) , patientinnen mit nur 13 lymphknoten zeigten nach imni sogar ein tendenziell erhhtes sterberisiko ( hr 1 , 13 ; 95 % - ki 0 , 841 , 51 )  . 
im gegensatz dazu profitierten patientinnen mit 4 befallenen lymphknoten und lateral gelegenen tumoren von der imni sogar deutlicher ( hr 0 , 71 ; 95%ki 0 , 570 , 89 ) als solche mit medialer tumorlokalisation ( hr 0 , 81 ; 95%ki 0 , 611 , 06 )  . 
auf die subgruppe mit medialem tumorsitz beschrnkt werden . unklar ist , wie weit die ergebnisse auf aktuelle therapieschemata bei nodalpositiven patientinnen bertragbar sind , da im zeitraum der studie noch keine taxane zum einsatz kamen , nur bei 53% eine chemotherapie und bei 35 % eine kombination aus chemound hormontherapie erfolgte . 
 in der eortc - studie war der positive effekt der lymphabflussbestrahlung bei den patientinnen am grten , die eine kombinierte chemound hormontherapie erhalten hatten [ 6 ]  . spezifische toxizittsuntersuchungen wurden nicht durchgefhrt . 
da die imni bei rechtsseitigen karzinomen keine relevante dosisbelastung fr das herz bewirkt , kann eine potentielle kardiotoxizitt bei patientinnen mit linksseitigem tumorsitz naturgem anhand dieser daten nicht beurteilt werden und lsst die frage offen , ob der berlebensvorteil auch letzteren patientinnen in vollem umfang zu gute gekommen wre . 
budach w , bolke e , kammers k , gerber pa , nestle - kramling c , matuschek c ( 2015 ) adjuvant radiation therapy of regional lymph nodes in breast cancer a meta - analysis of randomized trials an update . 
chang js , park w , kim yb et al ( 2013 ) long - term survival outcomes following internal mammary node irradiation in stage ii - iii breast cancer : results of a large retrospective study with 12year follow - up . 
courdi a , chamorey e , ferrero jm , hannoun - levi jm ( 2013 ) influence of internal mammary node irradiation on long - term outcome and contralateral breast cancer incidence in nodenegative breast cancer patients . 
hennequin c , bossard n , servagi - vernat s et al ( 2013 ) ten - year survival results of a randomized trial of irradiation of internal mammary nodes after mastectomy . 
thorsen lb , offersen bv , dano h et al ( 2016 ) dbcg - imn : a population - based cohort study on the effect of internal mammary node irradiation in early node - positive breast cancer . 
in contrast , in patients whose rectal volume decreased , significance was only seen for d25 % and d50 % ( dx % dose covering x % of the volume )  . 
in the latter patients , nonsignificant reductions in d2 cc , d5 cc and v5 gy ( volume receiving at least 5 gy ) were observed . conclusion the current rectal enemas protocol was ineffective in significantly modifying rectal dvh parameters for hdr - vcb . keywords endometrial carcinoma radiotherapy toxicity recommendations dosevolume histogram auswirkungen von rektalen einlufen auf dosimetrische rektale parameter whrend vaginaler high - dose - rate - brachytherapie eine prospektive studie zusammenfassung ziel beurteilung der auswirkungen von rektalen dosen whrend postoperativer high - dose - rate - ( hdr - ) brachytherapie an der scheidenmanschette ( vaginal cuff brachytherapy , vcb )  . patienten und methoden an der prospektiven studienahmen 59 patientinnen teil . 
 bei letzteren wurde eine nichtsignifikante verringerung der werte fr d2 cc , d5 cc und v5 gy beobachtet . schlussfolgerung die vorgehensweise fr rektale einlufe erwies sich als unzureichend fr eine signifikante vernderung von rektalen dvh - parametern bei der hdr - vcb . prior to vcb has long been advised . 
the european society for radiotherapy & oncology ( estro ) and the brachytherapy handbook both recommend it [ 9 ] , although the american brachytherapy society ( abs ) has not yet made any clear recommendations [ 10 ]  . 
there is a protocol for rectal evacuation prior to low - dose - rate ( ldr ) techniques , which require the patient to be admitted to hospital for several days bed rest ; however , taking into account the short outpatient procedure , no clear rationale exists for highdose - rate ( hdr ) techniques . 
we have demonstrated a positive relationship between rectal volumes and rectal doses during vcb [ 11 ] , and a beneficial effect on rectal dose deposition associated with rectal gas pocket removal [ 12 ]  . 
since rectal toxicity is not a major concern in postoperative vcb , it was not evaluated . schlsselwrter endometriumkarzinom radiotherapie toxizitt empfehlungen dosis - volumen - histogramm patients and methods vaginal cuff brachytherapy ( vcb ) is one of the most common brachytherapy treatments in gynecological oncology . 
the postoperative radiation therapy for endometrial carcinoma 2 ( portec - 2 ) trial with intermediate - risk ec patients yielded excellent clinical results with postoperative vcb alone , without the addition of external beam radiotherapy ( ebrt ) , therefore decreasing toxicity [ 3 ]  . 
 patients who have a poor prognosis following surgery are advised to undergo a postoperative course of radiotherapy [ 6 , 7 ]  . despite the long clinical experience , some technical gynecological brachytherapy issues remain to be clarified [ 8 ] , and rectal preparation is one of these . 
all patients gave written informed consent to the trial , which was approved by the ethics committee . the first and second vcb fractions were used for the study , the first being considered the basal or reference status , and the second representing the experimental rectal cleansing . 
during the two fractions , a pelvic ct scan was routinely carried out in the supine position , with a 2 - mm slice thickness and no gap between slices . 
cylinders were posieffect of rectal enemas on rectal dosimetric parameters during high - dose - rate vaginal cuff brachytherapy1 3 250 tioned to remain parallel to the patients craniocaudal axis . 
 two fleet enemas were self - administered before the second fraction , the first the night before the procedure and the second , at home , before hospital admittance . ct images were transferred to a 3d treatment planning system ( oncentra v.4.1 , elekta , stockholm , sweden )  . 
positive angle values denoted a tip directed toward the bladder and negative values denoted posterior displacement toward the recturectal dosewall histograms ( dwhs ) and rectal dosesurface histograms ( dshs ) were also generated . 
due to the inability to delineate the true rectal wall on ct images , a 2 - mm thick artificial rectal wall was constructed from the outer surface of the rectudshs were calculated using the cerr software package [ 13 ]  . 
doses delivered to 2 cc of the rectal wall and surfaces irradiated with 100 and 80 % of the delivered dose were computed . in order to study whether hotspots would change in relation to the enemas used , the rectal volume irradiated with > 95 % of the prescribed dose was segmented on every pair of cts . 
displacement of the hotspots was then analyzed after manual rigid pelvic registration and vaginal cylinder registration of basal and enema cts using the cerr package . brachytherapy was given to all patients using 192iridium with an initial nominal specific activity of 10 ci and a microselectron hdr ( elekta ) after - loading system . statistical analysis a sample size of 52 patients was calculated based on an estimated difference in mean rectal volume of 7 20 cc between both cts ( = 80 % , = 0.05 , two - sided test )  . 
the expected volume difference was thought to be two - thirds less ( 7 cc ) than in the previous study . results are shown as means ( standard deviation )  . 
unpaired t - tests were used to compare volume differences according to categorical variables that were assessed using the chi - square test , with fishers exact test if needed . 
 before administering the rectal enema , more patients rectums contained air or feces than after the enema ( chi - square test p = 0.028 ; table 2 )  . 
after rigid registration base on vaginal cylinders , these hotspots remained in the same area in 97 % of cases ; after rigid bone pelvic registration they were in the same area in 74 % of cases , either in the craniocaudal or the anteroposterior direction . rectal dvh parameters clearly worsened after the enema . 
patients were analyzed by paired t - tests , and an unpaired t - test analysis of the rectal dvh parameter differences according to any increase or decrease in rectal volume brought about by administering the enemas was carried out . 
generally speaking , the dvh metrics significantly increased in patients for whom enemas had no effect , while there was no statistical significance in patients whose rectal volume was reduced after the enemas . 
however , results have failed to demonstrate any rectal dosimetric value of performing rectal enema before vcb . effect of rectal enemas on rectal dosimetric parameters during high - dose - rate vaginal cuff brachytherapy1 3 252 traditionally , rectal cleansing is advocated prior to vcb . 
 the groupe europen de curietherapie ( gec ) - estro handbook of brachytherapy [ 9 ] recommends rectal cleansing before the procedure , irrespective of the dose rate used ; however , recommendations given on the web pages of radiation oncology departments differ on the use of rectal enemas [ 14 , 15 ] and there seems to be no clear rationale for their use in the literature . 
while a rectal evacuation might be useful during the long - term bed rest associated with ldr brachytherapy , even when given as a boost , no advantage has been shown for the quick hdr techniques carried out in an outpatient setting . 
therefore , it needs to be further evaluated whether rectal cleansing prior to vcb is , in fact , useful . this prospective study shows a significant mean reduction in rectal volume ; however , this effect was surprisingly inhomogeneous : 35.6 % of patients had a higher rectal volume after using enemas , suggesting that these were ineffective . 
previous data have demonstrated a positive correlation between rectal volume and rectal dvh parameters [ 11 ] , and lower rectal doses were observed after the removal of rectal gas pockets , which was associated with a rectal volume reduction [ 12 ]  . 
patients in the previous study had large basal rectums that lead to an active deflation , in the belief that the large rectal volumes could be associated with large rectal doses , whereas the current analysis has been performed per protocol on non - selected patients . despite adopting a similar approach to our previous study , we were unable to find similar results . 
a recent report has described the impact of the position of a patients legs on rectal doses , reporting higher doses when legs were placed in the gynecological position compared to legs extended [ 17 ] , the latter being how we treated all our patients . 
we were also unable to find any statistically significant differences in cylinder angle position . although vcb is one of the most common brachytherapy treatments , there is a lack of research pertaining to some of its technical aspects . 
results suggest there is no change in rectal and sigmoid dosimetry parameters related to bladder changes , but a recent study reported higher bladder doses and lower sigmoid and small bowel doses linked to distended bladders [ 18 ]  . 
other studies have focused on cylinder position [ 22 ] or the need for customized ct acquisition , delineation , and planning at each brachytherapy fraction [ 23 , 24 ]  . 
hoskin [ 22 ] described higher bladder doses when the cylinder tip pointed towards this organ ; the opposite was true for the rectuclinicians generally consider a single - plan approach for vcb instead of customizing a plan at each fraction [ 2325 ]  . the main limitation of our work is the lack of clinical data on toxicity with each approach . 
however , this could not be addressed by our experimental model due to the paired nature of the data , meaning that every patient was submitted to the basal and experimental conditions . 
to solve this , a randomized assay could be designed , although we believe that even a randomized design might not demonstrate differences either , due to the low - moderate to severe figures reported by others studies in the postoperative endometrial setting [ 26 , 27 ]  . 
it could be argued that rectal toxicity is not a major issue in postoperative vcb , although readers have to bear in mind that the results presented here have technical consequences for usual vcb procedure recommendations [ 9 ]  . 
at present , we are conducting a similar trial with cervical cancer patients with uterus in situ , in order to ascertain whether rectal enemas always produce the same effect in the rectum or whether the brachytherapy technique is affecting it . conclusion our protocol for administering rectal cleansing enemas before the vcb fractions was unable to show any dosimetric improvement despite the overall reduction in mean rectal volume . 
the current results also demonstrate that more than one third of the patients did not benefit from an expected reduction in rectal volume , but rather they showed the opposite effect . 
arenasstate state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . strahlenther onkol ( 2016 ) 192 : 199208 doi 10.1007 / s00066 - 015 - 0939 - 7 degro practical guidelines for radiotherapy of breast cancer vi : therapy of locoregional breast cancer recurrences wolfgang harms1 w . 
sauer5 breast cancer expert panel of the german society of radiation oncology ( degro ) received : 19 december 2015 / accepted : 22 december 2015 / published online : 1 march 2016 the author ( s ) 2016 . 
claraspital , kleinriehenstrasse 30 , 4016 basel , switzerland 2 heinrich - heine - university , duesseldorf , germany 3 university hospital schleswig - holstein , kiel , germany 4 vivantes hospital neukoelln , berlin , germany 5 university hospital erlangen , erlangen , germany formerly st . - vincentius - hospital , karlsruhe , germany 7 university hospital heidelberg , heidelberg , germany 8 helios - hospital wuppertal , witten / herdecke university , wuppertal , germany 9 municipal hospital , karlsruhe , germany 10 paracelsus medical university hospital , salzburg , austria 11 formerly university hospital tuebingen , tuebingen , germany 12 university medical center mannheim , medical faculty mannheim , university of heidelberg , mannheim , germany conclusions patients with isolated in - breast or regional breast cancer recurrences should be treated with curative intent . 
the largest reirradiation experience base exists for multicatheter brachytherapy ; however , prospective clinical trials are needed to clearly define selection criteria , long - term local control , and toxicity . following primary mastectomy , patients with resectable locoregional breast cancer recurrences should receive multimodality therapy including systemic therapy , surgery , and radiation + / hyperthermia . 
combination with hyperthermia can further improve tumor control . in patients with isolated axillary or supraclavicular recurrence , durable disease control is best achieved with multimodality therapy including surgery and radiotherapy . 
 radiation therapy significantly improves local control and should be applied whenever feasible . keywords chest wall recurrence breast cancer axillary recurrence breast cancer supraclavicular recurrence breast cancer mastectomy reirradiation review article 200 degro - leitlinien fr die strahlentherapie des mammakarzinoms vi : therapie lokoregionaler mammakarzinomrezidive zusammenfassung ziel aktualisierung der strahlentherapieleitlinien bei patienten mit lokoregionalen mammakarzinomrezidiven , basierend auf der aktuellen s3 - leitlinie . methoden es erfolgte eine umfassende recherche der wissenschaftlichen literatur mit den suchbegriffen : lokoregionales mammakarzinomrezidiv , thoraxwandrezidiv , lokalrezidiv , regionales rezidiv und mammakarzinom , eingeschrnkt durch die begriffe klinische studie , randomisierte studie , metaanalyse , systematischer review und leitlinie . schlussfolgerungen patienten mit isolierten in - brustoder regionalen rezidiven sollten mit kurativer intention behandelt werden . 
dennoch sind prospektive studien notwendig , um selektionskriterien sowie langzeittoxizitt und - kontrollraten genauer zu bestimmen . patienten mit resektablen lokoregionalen mammakarzinomrezidiven nach primrer mastektomie sollten mit einem multimodalen therapiekonzept mit kompletter resektion , systemischer therapie und bestrahlung + / hyperthermie behandelt werden . 
eine kombination mit einer zustzlichen hyperthermie kann die tumorkontrolle weiter verbessern . bei patienten mit isolierten axillren oder supraklavikulren rezidiven kann eine dauerhafte krankheitskontrolle am besten mit einem multimodalen behandlungskonzept bestehend aus chirurgie und radiotherapie erreicht werden . 
 eine strahlentherapie sollte , wann immer mglich , durchgefhrt werden , da sie zu einer signifikanten verbesserung der lokalen kontrolle fhrt . schlsselwrter brustwandrezidiv mammakarzinom axillres rezidiv mammakarzinom supraklavikulres rezidiv mammakarzinom mastektomie rebestrahlung introduction treatment of locally recurrent breast cancer remains an interdisciplinary challenge , since treatment options are limited or at least restricted due to previous treatments . 
data from large randomized trials have demonstrated that locoregional recurrences occur in approximately 515 % of patients , despite them having received adjuvant radiotherapy after primary mastectomy or breast - conserving surgery ( bcs ; [ 14 ] )  . 
as previous guidelines from the german society of radiation oncology ( degro ) expert panel [ 1012 ] focused on primary treatment of breast cancer , the current publication addresses radiotherapeutic options for locoregional recurrences . therapy of ipsilateral breast tumor recurrence statement of thegerman s3 guidelines 2012 [ 13 ] : statement recurrence 1 : local ( in - breast ) recurrence a . 
in the case of a second breast conservation , the patient should be informed about an increased risk of subsequent in - breast recurrence . bcs followed by adjuvant radiotherapy has become the standard of care for the majority of breast cancer patients . 
 ipsilateral breast tumor recurrence ( ibtr ) is diagnosed in approximately 510 % of patients at 10 years after breastconserving therapy ( bct ; [ 10 , 1417 ] )  . 
nevertheless , this approach is not founded on solid data demonstrating a clear advantage of radical surgery over a second attempt at bct for all ibtr patients [ 21 ]  . 
the radiation therapy oncology group ( rtog ) introduced a phase ii prospective trial of repeat bcs adding 3d conformal partial breast reirradiation for local recurrence in 2010 [ 22 ]  . 
 [ 25 ] reported a cumulative incidence rate of new primaries after whole - breast irradiation of 0.8 , 2 , and 3.5 % at 5 , 10 , and 15 years respectively . 
 [ 26 ] reported a significantly improved 10 - year overall survival ( os ) in patients with new primaries ( 75 % ) compared to patients with true recurrences ( 55 % ) in a retrospective study on 136 patients with ibtr as the first site of failure . 
 this question has been addressed in several studies attempting to differentiate between true recurrences and new primaries [ 2629 ] , from which the following conclusions can be derived : the majority of ibtr are true recurrences , which tend to occur earlier and in the same quadrant as the initial tumor , metastasize earlier and more often , and have a shorter overall and disease - free survival ( dfs ) than new primaries . 
based on these data , the degro expert panel suggests possible selection criteria for patients who may be candidates for a second breast - conserving approach ( table 1 )  . 
recent studies showed promising os rates in selected patients treated with second the degro expert panel suggests the following selection criteria for a second breast conserving approach table 1 possible selection criteria for patients with ipsilateral breast tumor recurrence who may be candidates for a second breast - conserving approach isolated ipsilateral breast tumor recurrence limited size ( < 23 cm ) unifocal disease on ultrasound , mammography , and mri age 50 years long interval between primary treatment and recurrence ( 48 months ) patient preference for a second breast conservation followed by radiotherapy a second breast conservation is technically feasible and will result in acceptable cosmetic results table 2 outcomes of patients treated with repeat breast conserving surgery alone following ipsilateral breast tumor recurrence study / year number of patients median follow - up ( months ) local recurrence rate ( % ) 5 - year overall survival kurtz [ 43 ] 1989 abner [ 44 ] 1993 salvadori [ 45 ] 1999 voogd [ 46 ] 1999 ishitobi [ 47 ] 2011 78 gentilini [ 48 ] 2012 nr not reported conservative surgery followed by partial - breast irradiation ( pbi ; [ 34 , 35 ] )  . 
the following survey provides an overview of different radiation techniques applied for reirradiation after bcs for ibtr ( table 3 )  . brachytherapy after bcs for ibtr the most solid evidence for reirradiation of ibtr exists for brachytherapy ( bt )  . 
the groupe europen de curiethrapie and the european society for radiotherapy & oncology ( gec - estro ) working group reported on a retrospective collaborative analysis of 217 ibrt patients treated between 2000 and 2009 with multicatheter bt in eight european institutions [ 35 ]  . 
the median total doses delivered through low dose rate ( ldr ) and pulsed dose rate ( pdr ) bt were 46 gy ( range 3055 gy ) and 50.4 gy ( range 4950 gy ) , respectively , and 32 gy ( range 2236 gy ; equivalent dose in 2 - gy fractions : 43 gy4 ) in 510 fractions ( median 8 fractions ) fractions ( twice daily ) for high dose rate ( hdr ) bt . 
further single - institution studies with small patient numbers support these data [ 3639 ]  . external beam radiotherapy after bcs for ibtr there is a single report on external beam radiotherapy ( ebrt ) for treatment of ibtr [ 40 ] comprising 39 patients . 
the rtog initiated a phase ii study of repeat breast - preserving surgery and 3d conformal partial breast reirradiation ( pbi ) for local recurrence of breast carcinoma with single doses of 1.5 gy in 15 fractions , twice daily , to a total dose of 45 gy [ 22 ]  . 
 the study has reached the accrual goal of 61 patients and is closed , but not yet published . there is only one publication considering intraoperative radiotherapy ( iort ) for reirradiation of ibrt [ 41 ]  . 
 at a medium follow - up of 26 months ( 160 months ) , no local recurrences occurred . toxicity assessment / cosmetic outcome of repeat irradiation for ibtr in all publications , acute toxicities of the respective method were reported to be low , while the most frequent late reaction pattern was fibrosis . 
particularly when assessed by standardized scoring systems , grade 12 sequelae in terms of fibrosis , telangiectasia , and / or pain ranged between 44 and 79 % [ 35 , 37 , 42 ]  . 
in the gec - estro series of 217 patients [ 35 ] , 141 patients ( 65 % ) developed late effects : cutaneous and subcutaneous fibrosis ( 67 % ) , telangiectasia ( 16 % ) , hyperpigmentation ( 9 % ) , and ulceration ( 1 % )  . 
in inoperable patients , palliative radiotherapy can be reasonable for systemic control . definition and patterns of recurrence a locoregional breast cancer recurrence after mastectomy is defined as the appearance of tumor in the ipsilateral chest wall , or the axillary , internal mammary , or supraclavicular lymph nodes [ 8 ]  . 
the early breast cancer trialists collaborative group analysis revealed a 10 - year risk of an isolated locoregional recurrence as the first event after mastectomy of 20.3 % for patients with 13 positive axillary lymph nodes , and of 32.1 % for patients with 4 positive nodes . 
in cohorts treated with modern systemic therapies , the total locoregional recurrence rate is substantially lower ; however , the relative risk reduction after radiotherapy remains unchanged [ 51 ]  . 
 there is evidence that a local recurrence per se is the strongest predictor for a further recurrence [ 9 ]  . treatment of resectable recurrences in radiation - naive patients if no previous irradiation has been performed , optimal treatment consists of complete excision of gross disease followed by irradiation [ 8 , 53 ]  . 
patients in the standard treatment group were treated to a dose of 50 gy plus a boost of 10 gy , while the dose escalation group was treated to a dose of 54 gy plus a 12 - gy boost . 
this combination improved clinical response and local control in several phase ii studies and randomized trials [ 59 , 60 ]  . for systemic management , endocrine therapy should be administered to all hormone receptor - positive patients in addition to local excision and radiotherapy [ 61 ]  . 
this result challenges the current practice of reluctant use of chemotherapy and provides evidence in favor of offering adjuvant chemoand radiotherapy to women with completely resected isolated locoregional relapse of breast cancer . treatment of unresectable recurrences in radiationnaive patients in patients with unresectable isolated locoregional recurrences who have not previously been irradiated , radiation therapy is mandatory . 
 [ 57 ] reported that patients with gross disease at the time of radiation had significantly lower 5 - year local control ( 63 % ) and survival rates ( 34 % ) compared to patients with no residual disease after surgery or systemic therapy ( 81 and 62 % , respectively )  . 
in summary , multimodality therapy including systemic and radiation therapy has the potential to cure selected patients [ 9 , 53 , 6668 ]  . degro practical guidelines for radiotherapy of breast cancer vi1 3 204 therapy of locoregional recurrences after mastectomy in previously irradiated patients treatment options are limited in patients with locoregional recurrences after mastectomy and adjuvant radiotherapy . 
however , a number of small to intermediate size clinical trials have revealed that the grade iv late toxicity after reirradiation with ebrt was within an acceptable range , not exceeding 12 % [ 5 , 6974 ]  . 
simultaneous radiochemotherapy as a treatment option has been investigated in a limited number of trials [ 63 , 64 ]  . reirradiation with or without regional hyperthermia laramore et al . 
grade iii fibrosis was experienced by 10 % of the patients and grade iv late effects were suffered by 7 % . an increasing number of studies on the combination of hyperthermia and reirradiation of the chest wall have been published ( table 4 ; [ 59 , 60 , 7174 , 76 , 77 ] )  . 
jones and colleagues [ 60 ] enrolled 109 patients with superficial tumors ( 70 patients with breast cancer ) in a prospective randomized trial comparing irradiation of chest wall recurrences with irradiation and additional hyperthermia . 
the complete response rate was 66.1 % in the hyperthermia and 42.3 % in the irradiation - only arpreviously irradiated patients had the greatest incremental gain in complete response : 23.5 % in the non - hyperthermia versus 68.2 % in the hyperthermia arno os benefit was seen . 
the incidence of 5 - year late grade 3 toxicity was 1 % . conclusions of the degro expert panel for the therapy of locoregional recurrences after mastectomy multimodality therapy including systemic therapy , surgery , and radiation + / hyperthermia achieves a high rate of local control and can be curative with long - term survival in a subset of patients . patients with an isolated locoregional recurrence after mastectomy should undergo surgical resection . 
 further dose escalation does not seem to improve treatment results . in previously irradiated patients with a high risk of a second local recurrence after surgical resection or in patients with unresectable recurrences , reirradiation should be strongly considered . 
indication and dose concepts depend on the time interval to first radiotherapy , presence of late radiation effects , and concurrent or sequential systemic treatment . in the absence of severe radiogenic stigmata and an appropriate time interval ( > 1 year ) , reirradiation with doses between 45 and 50 gy is recommended , but should not exceed cumulative doses of 100110 gy3 ( 2 - gy3 equivalent dose )  . particularly in previously irradiated patients , combination with hyperthermia can further improve tumor control . regional recurrences and isolated supraclavicular lymph node recurrences statement of the german s3 guidelines 2012 [ 13 ] : statement recurrence 3 : isolated regional recurrence a . 
the 5and 10 - year distant recurrence - free survival rates were 39 % ( 95 % confidence interval , ci : 2552 % ) and 29 % ( 95 % ci : 1642 % ) , respectively . 
the authors concluded that axillary recurrence following axillary dissection was associated with a high rate of subsequent distant metastasis and poor overall prognosis , although cure was still achievable in one third of the patients . 
in summary , complete remission can be obtained in most patients with isolated supraclavicular recurrence , although the prognosis for these patients is poor . degro practical guidelines for radiotherapy of breast cancer vi1 3 206 conclusions of the degro expert panel for the treatment of axillary or supraclavicular lymph node recurrence isolated axillary and supraclavicular recurrences from breast cancer are uncommon and may follow any stage of disease . 
of the affected patients , 5065 % develop distant metastases . to date , only retrospective data concerning the treatment of regional nodal recurrence are available . durable disease control is best achieved with multimodality therapy including surgery and radiotherapy . 
approximately one third of patients with an axillary breast cancer recurrence can be cured with multimodal therapy . radiation therapy significantly improves local control and should be applied whenever feasible . compliance with ethical guidelines conflict of interest w . 
sauer state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . open access this article is distributed under the terms of the creative commons attribution license which permits any use , distribution , and reproduction in any medium , provided the original author ( s ) and the source are credited . strahlenther onkol ( 2016 ) 192 : 240247 doi 10.1007 / s00066 - 016 - 0946 - 3 rib fractures after reirradiation plus hyperthermia for recurrent breast cancer predictive factors sabine oldenborg1 christel valk1 rob van os1 bing oei2 jack venselaar2 paul zum vrde sive vrding1 adrinne van randen3 hans crezee1 geertjan van tienhoven1 coen rasch1 received : 12 november 2015 / accepted : 14 january 2016 / published online : 8 february 2016 the author ( s ) 2016 . 
this article is published with open access at springerlink.com abstract background combining reirradiation ( rert ) and hyperthermia ( ht ) has shown high therapeutic value for patients with locoregional recurrent breast cancer ( lr )  . 
the aim of this study is to determine the impact of potential risk factors on the occurrence of rib fractures . patients and methods from 19822005 , 234 patients were treated with adjuvant rert + ht after surgery for lr . 
all rib fractures occurred in patients treated with a combination of photon and abutted electron fields ( p = 0.000 ) ; in 15 of 16 patients fractures were located in the abutment regions . 
box 22660 , amsterdam , the netherlands institute verbeeten ( bvi ) , tilburg , the netherlands 3 department of radiology academic medical center , university of amsterdam ( amc ) , amsterdam , the netherlands tors for rib fractures were a higher fraction dose ( p = 0.040 ) , large rt fields , and treatment before the year 2000 . discussion and conclusion rert + ht results in long - term lc . 
increasing the number of ht sessions a week does not increase the risk of rib fractures . keywords reirradiation hyperthermia recurrent breast cancer local control toxicity rippenfrakturen nach rebestrahlung kombiniert mit hyperthermie bei rezidiviertem brustkrebs prognostische faktoren zusammenfassung hintergrund der kombinierte einsatz von rebestrahlung ( rert ) und hyperthermie ( ht ) zeigt eine hohe wirksamkeit bei patienten mit lokoregional rezidiviertem brustkrebs ( lr )  . 
ziel war es , potentielle risikofaktoren fr die entstehung von rippenfrakturen zu untersuchen . patienten und methoden von 19822005 wurden 234 patienten nach lr - operation mit adjuvanter rert + ht behandelt . 
alle frakturen traten bei patienten auf , die mit einer kombination von photonenund elektronenfeldern behandelt wurden ( p = 0 , 000 ) ; bei 15 / 16 patienten waren frakturen in der anschlussregion lokalisiert . 
weitere wichtige prdiktive faktoren fr rippenfrakturen waren eine hhere fraktionierungsdosis ( p = 0 , 040 ) , groe rt - felder sowie eine behandlung vor dem jahr 2000 . diskussion und schlussfolgerung durch rert + ht lsst sich eine langfristige lc erzielen . 
mehr ht - sitzungen pro woche erhhen das risiko fr rippenbrche nicht . schlsselwrter rebestrahlung hyperthermie rezidivierender brustkrebs lokale kontrolle toxizitt locoregional recurrence ( lr ) after mastectomy or breast conservation predicts a poor outcome in patients with breast cancer [ 13 ]  . 
several phase iii trials demonstrated a significant increase of complete response rates and duration of local control when hyperthermia was added to radiotherapy for locoregional recurrent breast cancer in previously irradiated areas [ 6 , 7 ]  . 
the dutch national guidelines therefore adopted the combination of reirradiation ( rert ) + ht as standard of care for recurrent breast cancer in previously irradiated area [ 8 ]  . the reported incidence of rib fractures after primary breast cancer treatment varies from < 1 to 19 % [ 913 ] , depending on detection methods . 
the incidence decreased to < 2 % in more recent years , due to the improvement of radiation techniques [ 9 , 10 , 13 ]  . after rert for recurrent breast cancer , toxicity , like rib fractures , are likely to occur as well . 
although several authors report on the incidence of rib fractures [ 913 ] , data on the risk and significant cause ( s ) of rib fractures after rert + ht in previously irradiated area are scarce . 
the current study aims to retrospectively evaluate the number and location of rib fractures after adjuvant rert + ht in 234 patients treated in two dutch clinical centers for locoregional recurrent breast cancer in previously irradiated area after macroscopic complete resection or a clinically complete remission after chemotherapy . 
the impact of potential risk factors on the occurrence of fractures is also investigated . methods and materials patients data were collected from all patients with locoregional recurrent breast cancer in areas previously irradiated with curative intent , treated with rert and ht at the academic medical center ( amc ) and at the ben verbeeten institute ( bvi )  . 
a total of 234 ( amc : 152 , bvi : 82 ) patients received rert + ht as an adjunct to surgery or chemotherapy . data were collected from the radiotherapy and hyperthermia patient charts . 
the number and location of the fractures were assessed by one of the researchers ( c.v. ) and confirmed by a radiologist ( a.r. ) all patients received previous high dose radiation , overlapping with the current rert field . 
of the patients , 42 % were treated for previous locoregional recurrent disease using surgery , radiation , systemic therapy , or a combination of treatment modalities , before start of rert + ht . for the current recurrence episode , 225 patients had a macroscopically complete surgery and 9 patients a clinically complete remission ( ccr ) after chemotherapy . 
characteristics of the current disease episode and potential risk factors for rib fractures are summarized in table 1 . treatment radiotherapy all amc patients were irradiated using a standard schedule of 8 fractions of 4 gy given twice a week to a total dose of 32 gy . 
in general , the chest wall or mastectomy area up to the dorsal axillary fold was considered the target area . at bvi , large target areas were treated with a combination of 23 alternating abutted ap electron fields . 
the target temperature was 4143 c for 1 h , following a preheating phase of approximately 15 mapplied power was adjusted to the desired temperature distribution without exceeding the maximum normal tissue temperatures ( 45 c ) or patient tolerance . endpoints and data analysis rib fractures rib fractures were graded according to the national cancer institutes common terminology criteria for adverse events , version 3.0 as bone fractures were not included in version 4 . 
as this patient was reported with radiation - induced rib fractures , we did include this patient in the statistical analysis and eqd2 calculations . local control and survival both local control ( lc ) and survival rate were calculated from the date of first re - irradiation fraction . 
patients dying with lc , or alive with continuing lc at last follow - up , were censored at the date of death or last follow - up , respectively . statistics statistical analysis was carried out using spss version 20 ( spss inc . , chicago , il , usa )  . 
boost ; bvi : missing for 1 patient , amc : missing for 11 patients lpre - rert local or regional boost overlapping the current rert area given for previous recurrent disease mtotal dose boost in eqd2 ntotal pre - rert dose incl boost in eqd2 oin parenthesis dose in eqd2 pdose in eqd2 ; bvi : missing for 1 patient , amc : missing for 1 patient qtotal rert dose in eqd2 , incl 40 % of the total pre - rert dose ; bvi : missing for 2 patients , amc : missing for 12 patients . 
the continuous variables were checked for linearity by using spline regression curves and spline coefficients tested for nonlinearity ; all continuous variables showed a linear relationship with the occurrence of rib fractures . 
a multivariable analysis was not deemed appropriate because of the small total number of events . equivalent dose at 2 gy ( eqd2 ) the maximum possible eqd2 at the rib area was calculated for the two different rert fraction doses and for the two different rert techniques , using the linear - quadratic ( lq ) model [ 15 ] : eqd2 = where d denotes the total rert dose and d the dose per fraction . 
calculations were done for perfectly abutted photon / electron fields ( 6 mv photons without bolus , 10 mev electrons with bolus )  . for alternating abutted electron fields with gaps in between , the maximum possible overdose on the ribs was calculated using theraplan - plus ( mds nordion , kanata , canada )  . results rib fractures in 16 of 234 patients ( 7 % ) 18 fractures occurred after rert + h , whereby 15 of those patients were treated at amc and 1 at bvi . 
five patients had asymptomatic rib fractures ( grade 1 ) , 7 patients had symptomatic fractures ( grade 2 ) , and the other 4 patients had grade 3 fractures for which hyperbaric oxygen treatment was indicated . 
the group of 17 patients treated with other rt schedules ( table 2 ) did not show rib fractures . the 5 year infield lc rate was 70 % with an overall survival rate of 60 % . rib fractures after reirradiation plus hyperthermia for recurrent breast cancer1 3 cantly affect rib fracture incidence . 
pre - rert dose , rert dose and total dose in eqd2 , not corrected for rert technique , were not significantly related to the occurrence rib fractures . eqd2 the 12 fraction of 3 gy schedule , used at bvi can result in a eqd2 of 44 gy in the rib area , when part of the rib cage is located within the radiation field . 
the eqd2 on the ribs with a 10 % overdose is 51.6 gy , exceeding the td 5 / 5 by 3 % . discussion we found a difference in rib fracture rate of 1 vs . 
our reported fracture rate might actually be higher than reported here due to the retrospective character of our study . the main differences in rert treatment between both institutes were number of ht fractions , rert field size , - schedule , and - technique . 
however , our findings are in agreement with known risk factors for primary high dose irradiation : hypofractionation , low machine energy , large target volume , older age , female gender , postmenopausal status , surgical procedure preceding irradiation , and adjuvant simultaneous or sequential chemotherapy [ 11 , 12 ]  . the separate effects of abutted fields , fraction dose , and field sizes could not be estimated because of the high correlation of these factors . 
as the other tested factors were equally distributed between the two institutes , but not found significant , they were considered of lesser predictive value for rib fractures in our patient population . 
 after the year 2000 , the risk on rib fractures significantly decreased at amc ( p = 0.037 , hr = 0.318 ) , but not at bvi as the number of fractures observed at bvi was already low ( 1 % )  . 
the rib fracture rate for patients treated at amc from 20002005 was still as high as 6 % , probably reflecting the unchanged presence of risk factors such as large abutted fields combined with high fraction dose . few studies have reported on rib fracture incidence with different radiation schedules , after rert for recurrent breast cancer ( table 3 )  . 
comparison with those studies is difficult because most studies included very few patients , rt techniques differ and follow - up times are generally too short , as patients can develop fractures between 1 month and 5 years after treatment [ 12 ]  . 
another study , done by the same institute , did not report rib fractures for patients with resectable breast rib fractures after reirradiation plus hyperthermia for recurrent breast cancer1 3 246 table 3 previous studies of external beam repeat chest wall irradiation for recurrent breast cancer using different rert schedules study patients ( n ) additional rib fractures 0 ( 0 % ) li et al . 
second , only late grade 3 and 4 toxicities were reported , which included 5 patients who required treatment with necrotomy , reconstruction , and / or hyperbaric oxygen for osteoradionecrosis . 
 these results indicated that fraction dose could be a factor in the development of rib fractures above a threshold ( approximately 3.23.9 gy ) even when the total dose is modest [ 10 , 11 , 13 ]  . abutted fields are known to cause dosimetric problems as overlapping fields can result in a substantial local overor underdose , especially at a depth correlating with the location of the ribs.the maximum physical overdose varies with patient anatomy , and photon / electron energy and can be even be further exceeded by human or mechanical errors . 
restoration of normal tissue tolerance after low and moderate initial rt doses is on average no more than 60 % after 6 months , depending on tissue type [ 25 ]  . 
hence , for determining the optimum rert schedule a number of parameters must be taken into account : the initial eqd2 , volume treated , amount of overlap , additional treatments , and time interval between therapy courses [ 25 ]  . doubling ht fractions did not affect rib damage in our study population . 
this is in agreement with results from other ht studies that indicate that the number of ht sessions does not influence toxicity and that hyperthermia does not significantly affect overall toxicity when added to ( re ) rt [ 6 , 7 , 26 , 27 ]  . our patients will be more prone to rert damage as they received high dose irradiation and different kinds of systemic therapies in the past and rert is preceded by surgery . 
as a result of this study , rt techniques using only tangential photon fields or imrt and lower fraction doses have been adopted at amc in order to minimize the risk of problems with abutting fields . conclusion rert + ht results in long - term lc of 70 % after 5 years . 
 in 7 % of patients , rib fractures occurred , the majority of which were located in the photon / electron abutment area , emphasizing the disadvantage of field overlap . 
kok hp , de greef m , correia d , vrding pj , van stam g , gelvich ea et al ( 2009 ) fdtd simulations to assess the performance of cfma - 434 applicators for superficial hyperthermia . 
van der zee j , de bruijne m , mens jw , ameziane a , broekmeyerreurink mp , drizdal t et al ( 2010 ) reirradiation combined with hyperthermia in breast cancer recurrences : overview of experience in erasmus mc . 
linthorst m , van geel an , baaijens m , ameziane a , ghidey w , van rhoon gc , van der zee j ( 2013 ) re - irradiation and hyperthermia after surgery for recurrent breast cancer . 
li g , mitsumori m , ogura m , horii n , kawamura s , masunaga s et al ( 2004 ) local hyperthermia combined with external irradiation for regional recurrent breast carcinoma . 
muller ac , eckert f , heinrich v , bamberg m , brucker s , hehr t ( 2011 ) re - surgery and chest wall re - irradiation for recurrent breast cancer : a second curative approach . 
wahl ao , rademaker a , kiel kd , jones el , marks lb , croog v et al ( 2008 ) multi - institutional review of repeat irradiation of chest wall and breast for recurrent breast cancer . 
wurschmidt f , dahle j , petersen c , wenzel c , kretschmer m , bastian c ( 2008 ) reirradiation of recurrent breast cancer with and without concurrent chemotherapy . 
emami b , myerson rj , cardenes h , paris kg , perez ca , straube w et al ( 1992 ) combined hyperthermia and irradiation in the treatment of superficial tumors : results of a prospective randomized trial of hyperthermia fractionation ( 1 / wk vs 2 / wk )  . 
engin k , tupchong l , moylan dj , alexander ga , waterman fm , komarnicky l et al ( 1993 ) randomized trial of one versus two adjuvant hyperthermia treatments per week in patients with superficial tumours . 
int j hyperthermia 9 : 327340 strahlenther onkol ( 2016 ) 192 : 232239 doi 10.1007 / s00066 - 016 - 0945 - 4 unilateral and bilateral neck sib for head and neck cancer patients intensity - modulated proton therapy , tomotherapy , and rapidarc carmen stromberger1 luca cozzi2 volker budach1 antonella fogliata2 pirus ghadjar1 waldemar wlodarczyk1 basil jamil3 jan d . 
dose distributions , coverage , conformity , homogeneity to planning target volumes ( ptv ) s and sparing of organs at risk and normal tissue were compared . results all unilateral and bilateral plans showed excellent ptv coverage and acceptable dose conformity . 
for unilateral treatment , impt delivered substantially lower mean doses to contralateral salivary glands ( < 0.0011.1 gy ) than both rotational techniques did ( parotid gland : 610 gy ; submandibular gland : 1520 gy )  . 
all methods satisfied modern standards regarding toxicity and excellent target coverage for unilateral and bilateral treatment of head and neck cancer at the planning level . keywords chemoradiation volumetric arc therapy helical tomotherapy simultaneous integrated boost organs at risk unilateraler und bilateraler zervikaler sib fr patienten mit kopf - hals - tumoren intensittsmodulierte protonentherapie , tomotherapie und rapidarc zusammenfassung hintergrund planvergleich von intensittsmodulierter protonentherapie ( impt ) , tomotherapie ( ht ) und rapidarctherapie ( ra ) fr patienten mit plattenepithelkarzinomen der kopf - hals - region unter anwendung des simultan integrierten boost - konzepts ( sib )  . patienten und methodik fr 20 patienten mit plattenepithelkarzinomen der kopf - hals - region und bilateraler ( n = 14 ) oder unilateraler ( n = 6 ) zervikaler primrer radiochemotherapie erfolgte eine impt - , htund ra - planung mit 54 , 4 , 60 , 8 und 70 , 4 gye / gy in 32 fraktionen . 
die dosisverteilung , abdeckung , konformitt und homogenitt der ptvs sowie die risikoorganund normalgewebeschonung wurden verglichen . ergebnisse alle uniund bilateralen plne zeigten eine exzellente ptv - abdeckung bei akzeptabler konformitt . 
 original article1 3 233 impt erreichte in der unilateralen bestrahlungssituation eine wesentlich geringere mittlere dosis an den kontralateralen speicheldrsen ( < 0 , 0011 , 1 gy ) als beide photonentechniken ( glandula parotidea : 610 gy ; glandula submandibularis : 1520 gy )  . 
alle untersuchten bestrahlungsmethoden konnten sowohl fr die unilaterale als auch die bilaterale bestrahlung von patienten mit kopf - hals - tumoren moderne bestrahlungsplanungsvorgaben im sinne einer limitierung von nebenwirkungen bei gleichzeitig exzellenter zielvolumenabdeckung erreichen . [ 1418 ] and on early clinical outcomes with vmat and sib - vmat [ 19 , 20 ]  . 
proton therapy in itself appears to hold the promise of good local control with similar or better target coverage and reduced doses to organs and normal tissue compared to photon therapy [ 2426 ]  . 
a recent biological modelling study demonstrated advantages with protons regarding dysphagia for tumors in the upper head and neck region and acute mucositis for laryngeal tumors [ 27 ]  . this studys objective was to assess when and whether sib - impt for patients with locally advanced hnscc might be superior to the two modern rotational photon beam modalities ( helical tomotherapy , ht ; vmat with rapidarc , ra ) regarding target coverage and sparing of organs at risk and normal tissue . schlsselwrter chemoradiation volumetrisch modulierte arc - therapie helikale tomotherapie simultan integrierter boost risikoorgane materials and methods patient selection and contouring definitive chemoradiation with intensity - modulated radiotherapy ( imrt ) or volumetric intensity modulated arc ( vmat ) represents the current standard of care for patients with locally advanced squamous cell carcinoma of the head and neck ( hnscc ) [ 1 ]  . 
imrt made selective organ - at - risk sparing feasible for such patients [ 2 ] with a major focus on the preservation of salivary gland function , to reduce the risk of dry mouth and its consequential problems regarding chewing , late dysphagia , sleep , dental status , and oral pa for the parotids , different dosimetric dosevolume parameters have been investigated . 
in particular , mean doses of 2530 gy were associated with 1726 % normal tissue complication probabilities ( ntcp ) [ 3 , 4 ] and a td ( 50 ) ( dose resulting in a 50 % complication incidence ) of 40 gy was found in a large study of function one year after radiotherapy [ 5 ]  . 
structures including the pharyngeal constrictor muscle [ 7 ] , glottic and supraglottic larynx [ 8 ] and the proximal esophagus [ 9 ] have been investigated , and moderate sparing to prevent late dysphagia has been proposed [ 10 ]  . photon treatments using simultaneous integrated boost ( sib ) techniques [ 11 ] allow different dose intensities for the corresponding regions in a single plan with better conformity than sequential techniques [ 12 , 13 ] , and this approach is being increasingly applied . 
publications exist both on the effectiveness and safety of sib - imrt and ht for hnscc we selected 20 consecutive patients with locally advanced hnscc previously treated by us with sib techniques ( 14 bilaterally , 6 unilaterally ) , either with ht ( tomotherapy inc . , madison , wi , usa ) or ra ( varian medical systems , palo alto , ca , usa )  . 
patient and tumor characteristics are shown in table 1 . all volumes were contoured on an intravenous enhanced planning - ct ( 80 ml , ultravist , patient in supine position , 5 - point thermoplastic mask ) on axial slices with 1.25 mm slice thickness in the eclipse treatment planning system ( tps ) , version 11.0.42 ( varian medical systems )  . 
planning was in accordance with the guidelines of the international commission on radiation units and measurements ( icru ) report 50 / 83 ( org / content / 10 / 1.toc ) , to deliver the prescribed doses to the ptvs while keeping doses to the organs at risk within the constraints or as low as reasonably achievable ( alara ; table 2 )  . 
planning was performed by distinct physicists experienced in the respective treatment modality . impt planning impt plans were computed with the eclipse tps ( v.13 ) simulating a varian probeam systea nonlinear universal proton optimizer was used for the scope . 
the proton convolution superposition algorithm with a constant relative biologic effectiveness value of 1.1 was used for the final dose calculation on a grid size of 3 3 3 mm3 . 
the gantry angles were chosen to give the best individual geometrical configuration . tomohd planning treatment was with the tomotherapy hi - art 5.0.2 ( tomotherapy , inc . ) system using the ht convolution / superposition c / s algorithm for the computations . 
the field width was set at 2.5 cm , pitch at 0.25 , and modulation factor at 34 with the dose calculation grid set to fine mode . ra planning plans were optimized with the tps eclipse v11.0.42. 
for ptv coverage , the saint - anne , lariboisire , tenon ( salt ) coverage factor ( cvfsalt ; cvf = tvri / tv ; tvri : irradiated target volume encompassed by reference 95 % isodose ; tv : target volume ) was calculated . 
statistical significance was assumed for p 0.05. results target coverage all unilateral and bilateral plans achieved excellent target volume coverage ( mean cfvsalt 0.91 ) , good dose conformity , and homogeneity ( tables 3 , 4 ) with no potentially clinically significant differences for the ptvs . 
impt achieved significantly unilateral and bilateral neck sib for head and neck cancer patients1 3 236 ptv_70gy coverage conformity homogeneity ptv_60gy coverage conformity homogeneity ptv_54gy coverage conformity homogeneity organs at risk parotid glands contralateral ipsilateral submandibular glands contralateral ipsilateral spinal cord larynx table 3 dosevolume histogram parameters and treatment efficiency for impt , ht , and ra ( mean standard deviation ) for the unilateral neck irradiation volume parameter p - value impt vs . 
a lower mean dose to the parotid gland usually results in better function , even for relatively low mean doses ( < 10 gy ) [ 10 ] but quality of life in patients with hnscc treated with modern imrt remains compromised with long - term dry mouth and sticky saliva even after 1 year [ 33 ]  . 
nevertheless , all modalities ensured adequate sparing of the classical organs at risk ( spinal cord , salivary glands , oral cavity , and larynx )  . interestingly , the ht plans for bilateral irradiation were absolutely comparable to impt plans . 
furthermore , the lower integral dose to normal tissue compared to vmat implies a lower risk of radiation - induced carcinogenesis , even though this risk may be of minor concern at the moment [ 34 ]  . the clinical experience for patients with hnscc treated with proton therapy [ 25 ] or with a combination of protons and photons [ 24 ] in the primary situation needs and is undergoing expansion . 
preliminary results of a multi - optimization sib - impt for a series of 10 hnscc patients showed it to be feasible , safe , and effective [ 25 ]  . 
nevertheless , impt harbors uncertainties of major importance , including variations in the range of the proton beam , daily set - up errors , intrafractional patient motion , and anatomic changes during treatment that could affect its robustness [ 25 ]  . some of these issues are currently under evaluation [ 35 38 ]  . 
the impact of interfractional changes on the delivered dose in impt or imrt for hnscc patients treated in the adjuvant setting was recently evaluated , and impt plans did indeed show large differences between the planned and reconstructed doses , carrying a risk for local underdosage , and imrt plans were more critical in terms of over - dosage to organs at risk [ 36 ]  . 
 [ 38 ] showed that at least in half of the recalculated vmat plans , the treatment plan parameters and organs at risk limits were still acceptable , while for impt none of the recalculated plans were acceptable in terms of ptv coverage . 
however , cost - effectiveness analyses regarding all these forms of radiotherapy will also be required . conclusion we are aware that with the assumption of a perfect patient setup , no robustness analysis , and a missing analysis of anatomical changes , this study has its limitations . 
nevertheless , it clearly demonstrates on the planning level that excellent target coverage and good sparing of classical organs at risk is achievable using the sib approach with modern photon therapy techniques , especially ht , which are widely available and relatively cost - effective . 
proton therapy may offer further advantages for subsets of patients , but more clinical studies are needed . acknowledgments no source of funding supported this work . compliance with ethical guidelines conflict of interest l . 
marnitz state that there are no conflicts of interest . this study was approved by the institutional review board of the charit universittsmedizin berlin . strahlenther onkol ( 2016 ) 192 : 216222 doi 10.1007 / s00066 - 016 - 0941 - 8 gilta randomised phase iii study of oral vinorelbine and cisplatin with concomitant radiotherapy followed by either consolidation therapy with oral vinorelbine and cisplatin or best supportive care alone in stage iii non - small cell lung cancer michael flentje1 rudolf m . 
huber2 walburga engel - riedel3 stefan andreas4 jens kollmeier5 susanne staar6 nicolas dickgreber7 nathalie vaissiere8 cecilia de almeida8 birgit edlich9 rainer fietkau10 received : 15 october 2015 / accepted : 8 january 2016 / published online : 25 january 2016 springer - verlag berlin heidelberg 2016 abstract background concurrent chemoradiotherapy ( crt ) is considered standard for inoperable stage iii non - small cell lung cancer ( nsclc )  . 
this phase iii study assessed crt followed by best supportive care ( bsc ) or consolidation with oral vinorelbine and cisplatin . methods patients received two cycles of oral vinorelbine ( 50 mg / m2 days 1 , 8 and 15 ) + cisplatin ( 20 mg / m2 days 14 ) q4w + radiotherapy ( rt ; 66 gy )  . 
patients with at least stable disease ( sd ) were randomised to either two cycles oral vinorelbine ( 6080 mg / m2 days 1 and 8 ) + cisplatin ( 80 mg / m2 day 1 ) q3w + bsc or bsc alone . 
concurrent rt with oral vinorelbine and cisplatin demonstrated a favourable safety profile and represents a suitable treatment regimen for inoperable stage iii nsclc . keywords chemoradiotherapy survival toxicity combined modality therapy consolidation chemotherapy gilt eine randomisierte phase - iii - studie mit oralem vinorelbin und cisplatin plus konkomitanter strahlentherapie gefolgt von konsolidierender therapie mit oralem vinorelbin und cisplatin oder bestmglicher supportiver therapie bei nicht - kleinzelligem lungenkarzinom stadium iii zusammenfassung hintergrund simultane radiochemotherapie ( crt ) wird als standardtherapie beim inoperablen stadium iii des original article1 3 nicht - kleinzelligen lungenkarzinoms ( nsclc ) angesehen . 
in dieser phase - iii - studie wurde crt mit anschlieender " best supportive care " ( bsc ) oder konsolidierung mit oralem vinorelbin und cisplatin bewertet . methoden die patienten wurden mit 2 zyklen oralem vinorelbin ( 50 mg / m2 , tag 1 , 8 und 15 ) + cisplatin ( 20 mg / m2 , tag 14 ) q4w + radiotherapie ( rt , 66 gy ) behandelt . 
 patienten , die mindestens eine krankheitskontrolle aufwiesen , wurden zu 2 zyklen oralem vinorelbin ( 6080 mg / m2 , tag 1 und 8 ) + cisplatin ( 80 mg / m2 , tag 1 ) q3w mit bsc oder alleiniger bsc randomisiert . 
simultane rt mit oralem vinorelbin und cisplatin wies ein vorteilhaftes sicherheitsprofil auf und stellt damit ein geeignetes behandlungsregime fr nsclc - patienten mit inoperablem stadium iii dar . schlsselwrter chemoradiotherapie berleben toxizitt kombinierte modale therapie konsolidierungschemotherapie in locally advanced non - small cell lung cancer ( nsclc ) , concurrent full - dose chemoradiotherapy ( crt ) improves outcome mainly due to better local control . 
median survival is 15 months , 5 - year survival around 15 % [ 1 ]  . metastases remain the major issue , thus intensifying systemic treatment is of great interest . 
in 2003 , the southwest oncology group ( swog ) reported a single - arm phase ii trial assessing consolidation chemotherapy ( swog 9504 ; [ 2 ] )  . 
however , no improvement was seen in the hoosier oncology lun - 1 trial randomising the swog consolidation approach against observation only [ 4 ]  . the purpose of the present study , in which cisplatin ( p ) and oral vinorelbine ( nvbo ) were given with concomitant radiotherapy ( rt ; 66 gy ) in locally advanced nsclc , was to evaluate the progression - free survival ( psf ) benefit of adding two cycles of chemotherapy compared to best supportive care ( bsc ) in patients with at least stable disease ( sd ) control following crt . we chose p and nvbo for chemotherapy due to their toxicity profile [ 5 ] , feasibility [ 6 ] and possible lung injury with taxanes . 
 [ 7 ] the oral formulation of vinorelbine was introduced to improve patient comfort and logistics during rt and consolidation [ 8 ]  . methods study design and patients this randomised , open - label , phase iii trial recruited between may 2005 and may 2009 in 34 german centres . 
 eligible patients had histologically confirmed stage iiia / iiib ( tnm6 ) inoperable nsclc without malignant pleural effusion , weight loss & 10 % , karnofsky index 80 , forced expiratory volume in 1 second ( fev1 ) < 1.5 l and no previous treatment . 
staging was based on bronchoscopy , thoracoabdominal ct , bone scintigraphy and brain ct or mri . procedures rt was given in 2 - gy daily fractions to a total dose of 66 gy and combined with 20 mg / m2 intravenous p ( days 14 and 2932 ) and nvbo 50 mg / m2 on days 1 , 8 and 15 , as well as days 29 , 36 and 43 . 
treatment planning aimed at a volume receiving a dose of 20 gy or more < 30 % for lung ( v20 ) , a maximum dose of 45 gy to the spinal cord and a median dose of less than 40 gy to the heart . 
for the oesophagus , the maximum dose was restricted to 66 gy if a length of no more than 10 cm was irradiated , whereas the dose was to be limited to maximally 40 gy in areas exceeding 15 cm in length . randomisation was 46 weeks after crt , stratified according to response ( complete response , cr ; partial response , pr ; sd ) , study centre and disease stage . 
secondary endpoints were overall survival ( os ) , objective response rate ( orr = cr + pr ; response evaluation criteria in solid tumors , recist 1.0 ) , disease control rate ( dcr = cr + pr + sd ) toxicity ( common terminology criteria , ctc v.3.0 ) and quality of life ( lung cancer symptom scale , lcss )  . 
 due to slow accrual , the study was stopped prematurely . was performed within 30 days after last administration of study drug in the consolidation arm or after completion of two cycles ( 6 - week period ) in the bsc arm with subsequent follow - up every 3 months . 
the absence of benefit is in line with the lun - 1 crt trial [ 4 ] , the systematic review of tsujino [ 10 ] and the korean trial [ 11 ]  . although pfs and os did not differ , data suggest that cc mediates disease containment . 
subgroup analyses indicated that cc might have a positive impact in patients with more advanced disease or squamous histology . in swog s0023 and lun - 1 , p with etoposide followed by consolidation with docetaxel was used [ 3 , 4 ]  . 
median survival ( 19 months with 54 % stage iiib ) in swog s0023 cannot easily be related , since randomisation was performed after consolidation . concurrent rt to 66 gy with nvbo and p has a favourable toxicity profile in a multicentre setting . 
a pooled analysis of seven rtog trials confirmed the impact of higher doses on efficacy [ 12 ] , whereas rtog - 0617 seems to suggest upper limits of tolerability [ 13 ]  . gilta randomised phase iii study of oral vinorelbine and cisplatin with concomitant radiotherapy1 3 222 taking together the results from the gilt study and available evidence from controlled trials , cc after definitive concurrent crt does not improve outcome in unselected patients . 
howell , aerian consulting wellesley usa . source of funding the study was funded by the institut de recherche pierre fabre , france . compliance with ethical guidelines conflicts of interest jk reports grants to his institution by pierre fabre ; sa reports financial support by roche , glaxosmithkline , boehringer ingelheim and eli lilly ; rh reports funding by pierre fabre ; rf reports financial support by pierre fabre , roche and eli lilly ; mf reports funding by pierre fabre . 
wer , ss and nd state that there are no conflicts of interest . all studies on humans described in the present manuscript were carried out with the approval of the responsible ethics committee and in accordance with national law and the helsinki declaration of 1975 ( in its current , revised form )  . 
informed consent was obtained from all patients included in studies . postoperative radiotherapie des endometriumkarzinoms grndlichere und evidenzbasierte aufarbeitung der daten weiterhin erforderlich strahlenther onkol ( 2016 ) 192 : 269272 doi 10.1007 / s00066 - 016 - 0954 - 3 simone marnitz1 online publiziert : 17 . 
 [ 1 ] bewerten aus sicht der american society of clinical oncology ( asco ) die im jahre 2014 publizierten empfehlungen der american society for radiation oncology ( astro )  . studiendesign es erfolgte eine erneute literaturrecherche ( medline ) fr die zeit vom 1 . 
 der autoren die vorhandenen schlussfolgerung entsprechenden astro - empfehlungen wurden mit asco - kommentaren zusammengefasst die empfehlungen im einzelnen : ( 1 ) der verzicht auf eine adjuvante therapie wird empfohlen bei positiver uterusbiopsie ohne tumornachweis im hysterektomieprparat sowie bei pt1a g1 / 2 , unabhngig davon , ob eine lymphonodektomie ( lne ) durchgefhrt wurde oder nicht . 
 ( 2 ) die alleinige vaginale brachytherapie ( vbt ) sollte erwogen werden bei pt1ag1 / g2 mit weiteren risikooriginalpublikation meyer la , bohlke k , powell ma et al ( 2015 ) postoperative radiation therapy for endometrial cancer : american society of clinical oncology clinical practice guideline endorsement of the american society for radiation oncology evidence - based guideline . 
62 , 50937 kln , deutschland faktoren wie alter > 60 jahre und / oder lymphgefinvasion ( lsvi ) sowie pt1ag3 nach lymphonodektomie [ 2 ] ohne nachweis von lymphknotenmetastasen [ 3 ]  . 
des stromainvasion weiteren fr pt1b g12 , wenn > 60 jahre und / oder lsvi [ asco - kommentar : vbt mag eine bessere alternative fr diese patienten sein , insbesondere , wenn chirurgisches staging adquat war und die lymphknoten ( lk ) negativ sind ]  . 
sie wird empfohlen bei patientinnen mit positiven lk , serosabefall oder befall der ovarien , tuben , vagina , blase , tuben , vagina , blase oder des rektums zur durchfhrung einer perkutanen strahlenund chemotherapie ( asco - kommentar : beste evidenz existiert fr die chemotherapie , strahlentherapie kann erwogen werden )  . 
 ( 4 ) der alleinige einsatz der chemotherapie kann erwogen werden bei positiven lk oder serosabefall oder befall der ovarien , tuben , vagina , blase , tuben , vagina , blase und des rektums , basierend auf pathologischen risikofaktoren fr pelvine rezidive . 
 ( 5 ) die strahlentherapie ohne chemotherapie kann erwogen werden bei positiven lk , serosabefall oder befall der ovarien , tuben , vagina , blase , tuben , vagina , blase , rektum , basierend auf pathologischen risikofaktoren fr pelvine rezidive ( ascokommentar : patientinnen haben nach chemotherapie ein verbessertes berleben im vergleich zur strahlentherapie allein )  . 
im einzelnen : es wird auf die berschaubaren flle mit inzidentiellem nachweis mittels probeentnahmen ( pe ) aus dem uterus , aber negativer histologie im hysterektomie ( he - ) prparat hingewiesen . die klaren vorteile minimal - invasiver techniken der he , insbesondere bei dem adipsen patientengut mit multiplen komorbiditten , werden nicht erwhnt , obwohl hier die einzige level - i - evidenz in der gesamten behandlung des endometriumkarzinoms vorliegt . die indikationen fr die vaginale brachytherapie ( vbt ) sind nachvollziehbar , die zustzlichen risikofaktoren wie alter und lsvi spielen fr die deutsche leitlinie keine rolle . 
der terminus lsvi meint entweder lymphgefangiose ( l ) oder hmangioinvasion ( v ) oder die kombination von l und v . l1cam ( l1 cell adhesion molecule ) , ein neuerer , unabhngiger prognosefaktor , wurde hingegen berhaupt nicht diskutiert [ 5 ]  . 
auf basis der daten der astecgruppe ist die lymphonodektomie im stadium i und ii weitgehend verlassen worden , andere gruppen wie die kollegen der mayo - klinik [ 6 ] und die japanische gruppe der sepal - studie [ 7 ] favorisieren sie nach wie vor , da sie die einzige valide option ist , einen lymphknotenbefall auszuschlieen und ein adquates adjuvantes konzept in die therapie einzubringen [ 8 ]  . die alleinige vbt bei lokal fortgeschrittenen befunden > pt1b nach comprehensive nodal assessment erstaunt , zumal dies den daten der randomisierten studien widerspricht . 
selbst patientinnen mit negativem lymphknotenbefund und < 50% myometriuminfiltration , aber g3 , weisen ein risiko von > 2% fr eine skip bei der paraaortalen metastasierung auf [ 11 ]  . die validitt des gradings als grundlage fr eine risikostratifizierung ist kritisch zu hinterfragen . 
als ergebnis des zentralen reviews des gradings in der portec - 2 - studie war nach zentraler pathologiebefundung ein shift bei g2 von 44 auf 9% zu verzeichnen gewesen [ 12 ]  . als behelfskonzept wurden verschiedenste risikogruppierungen angesprochen . 
festgemacht , aber gleichzeitig wieder in frage gestellt unter verweis auf die alten randomisierten studien , die fr patientinnen im stadium i / ii keinen berlebensvorteil durch die ebrt ergaben , dabei aber auch nicht die statistische power aufwiesen , was selten erwhnt wird [ 9 , 10 ]  . 
die signifikante verbesserung der lokoregionren kontrolle ist ein wichtiger , aber insbesondere von den medizinischen onkologen ein gern ignorierter endpunkt . der verzicht auf eine ebrt bei pt1b g12 bei einer patientin > 60 jahre und / oder lsvi ist nachvollziehbar , aber nicht mit daten belegt . die astro empfiehlt fr patientinnen mit positiven lk oder serosabefall oder befall der ovarien , tuben , vagina , blase , tuben , vagina , blase und rektum die perkutane strahlentherapie und chemotherapie . 
unerwhnt von der astro und der asco - gruppe bleibt , dass zwei groe randomisierte studien , die den werte der chemogegen denjenigen der strahlentherapie verglichen , negativ ausfielen [ 15 ]  . 
die einzige studie , die auf den ersten blick eine berlegenheit von chemogegenber strahlentherapie bei nodalpositiven patientinnen beschreibt , ist die gog - 122 - studie [ 16 ]  . 
eine qualitiy - of - life - ( qol - ) analyse der studie [ 17 ] riet wegen der hohen polyneuropathieraten davon ab , diese chemotherapie bei patientinnen einzusetzen , die mit hnden und fen arbeiten . 
 an der gog - studie die berlegenheit der adjuvanten chemotherapie gegenber der strahlentherapie festzumachen , geht an den ergebnissen der studie vorbei . eine valide therapieempfehlung fr die nichtendometrioiden karzinome gibt es nicht . fr diese empfehlungen fehlen klare evidenzen , siehe asco - kommentar : beste evidenz existiert fr die chemotherapie , strahlentherapie kann erwogen werden . fr diese empfehlungen fehlen klare evidenzen , siehe asco - kommentar : vbt mag eine bessere alternative fr diese patienten sein , insbesondere , wenn chirurgisches staging adquat war und die lymphknoten ( lk ) negativ sind . der zustzliche benefit der vbt , wenn eine suffiziente ebrt unter einschluss des scheidenstumpfs durchgefhrt wird , ist nicht belegt , deshalb kann diese empfehlung nachvollzogen werden . 
lediglich eine seer - analyse kommt zu anderen schlssen [ 18 ]  . die interessante frage , wie denn chemound strahlentherapie kombiniert werden sollen , wird in der kommentierten bersicht nicht auf der basis der datenlage diskutiert . 
es liegen sowohl empfehlungen fr die sequentielle applikation von radiotherapie und chemotherapie [ 19 ] , die simultane applikation [ 20 ] und auch das sandwich - verfahren ( chemotherapie - strahlentherapie - chemotherapie ) vor [ 21 ]  . fazit von den autoren der vorliegenden publikation htte man sich eine grndlichere und evidenzbasierte aufarbeitung zur therapie des endometriumkarzinoms gewnscht . 
meyer la , bohlke k , powell ma , fader an , franklin ge , lee lj , matei d , coallier l , wright aa ( 2015 ) postoperative radiation therapy for endometrial cancer : american society of clinical oncology clinical practice guideline endorsement of the american society for radiation oncology evidence - based guideline . 
gaudineau a , weitbruch d , quetin p , heymann s , petit t , volkmar p , bodin f , velten m , rodier jf ( 2012 ) neoadjuvant chemoradiotherapy followed by surgery in locally advanced squamous cell carcinoma of the vulva . 
bosse t , nout ra , stelloo e , dreef e , nijman hw , jurgenliemkschulz im , jobsen jj , creutzberg cl , smit vt ( 2014 ) l1 cell adhesion molecule is a strong predictor for distant recurrence and overall survival in early stage endometrial cancer : pooled portec trial results . 
kumar s , podratz kc , bakkum - gamez jn , dowdy sc , weaver al , mcgree me , cliby wa , keeney gl , thomas g , mariani a ( 2014 ) prospective assessment of the prevalence of pelvic , paraaortic and high paraaortic lymph node metastasis in endometrial cancer . 
todo y , kato h , kaneuchi m , watari h , takeda m , sakuragi n ( 2010 ) survival effect of para - aortic lymphadenectomy in endometrial cancer ( sepal study ) : a retrospective cohort analysis . 
creutzberg cl , van putten wl , koper pc , lybeert ml , jobsen jj , warlam - rodenhuis cc , de winter ka , lutgens lc , van den bergh ac , van de steen - banasik e et al ( 2000 ) surgery and postoperative radiotherapy versus surgery alone for patients with stage - 1 endometrial carcinoma : multicentre randomised trial . 
keys hm , roberts ja , brunetto vl , zaino rj , spirtos nm , bloss jd , pearlman a , maiman ma , bell jg , gynecologic oncology g ( 2004 ) a phase iii trial of surgery with or without adjunctive external pelvic radiation therapy in intermediate risk endometrial adenocarcinoma : a gynecologic oncology group study . 
nout ra , smit vt , putter h , jurgenliemk - schulz im , jobsen jj , lutgens lc , van der steen - banasik em , mens jw , slot a , kroese mc et al ( 2010 ) vaginal brachytherapy versus pelvic external beam radiotherapy for patients with endometrial cancer of highintermediate risk ( portec - 2 ) : an open - label , non - inferiority , randomised trial . 
aalders j , abeler v , kolstad p , onsrud m ( 1980 ) postoperative external irradiation and prognostic parameters in stage i endometrial carcinoma : clinical and histopathologic study of 540 patients . 
randall me , filiaci vl , muss h , spirtos nm , mannel rs , fowler j , thigpen jt , benda ja , gynecologic oncology group study ( 2006 ) randomized phase iii trial of whole - abdominal irradiation versus doxorubicin and cisplatin chemotherapy in advanced endometrial carcinoma : a gynecologic oncology group study . 
bruner dw , barsevick a , tian c , randall m , mannel r , cohn de , sorosky j , spirtos nm ( 2007 ) randomized trial results of quality of life comparing whole abdominal irradiation and combination chemotherapy in advanced endometrial carcinoma : a gynecologic oncology group study . 
rossi pj , jani ab , horowitz ir , johnstone pa ( 2008 ) adjuvant brachytherapy removes survival disadvantage of local disease extension in stage iiic endometrial cancer : a seer registry analysis . 
hogberg t , signorelli m , de oliveira cf , fossati r , lissoni aa , sorbe b , andersson h , grenman s , lundgren c , rosenberg p et al ( 2010 ) sequential adjuvant chemotherapy and radiotherapy in endometrial cancerresults from two randomised studies . 
greven k , winter k , underhill k , fontenesci j , cooper j , burke t , radiation therapy oncology group ( 2004 ) preliminary analysis of rtog 9708 : adjuvant postoperative radiotherapy combined with cisplatin / paclitaxel chemotherapy after surgery for patients with high - risk endometrial cancer . 
alvarez secord a , havrilesky lj , bae - jump v , chin j , calingaert b , bland a , rutledge tl , berchuck a , clarke - pearson dl , gehrig pa ( 2007 ) the role of multi - modality adjuvant chemotherapy and radiation in women with advanced stage endometrial cancer . 
marnitz1 3 strahlenther onkol ( 2016 ) 192 : 254259 doi 10.1007 / s00066 - 016 - 0943 - 6 setup accuracy for prone and supine whole breast irradiation thomas mulliez1 akos gulyban1 , 2 tom vercauteren1 annick van greveling1 bruno speleers1 wilfried de neve1 liv veldeman1 received : 21 may 2015 / accepted : 14 january 2016 / published online : 10 february 2016 springer - verlag berlin heidelberg 2016 abstract purpose to evaluate cone - beam computed tomography ( cbct ) based setup accuracy and margins for prone and supine whole breast irradiation ( wbi )  . methods setup accuracy was evaluated on 3559 cbct scans of 242 patients treated with wbi and uncertainty margins were calculated using the van herk formula . 
multivariate analysis identified a significant ( p < 0.05 ) correlation between bmi and the lo margin in supine position and the ve / la margin in prone position . conclusion in this series , setup accuracy is significantly worse in prone compared to supine position for the la and lo directions . 
 uniund multivariable analysen wurden fr sicherheitsabstnde in jede richtung auf basis von alter , body - massindex ( bmi ) und krbchengre durchgefhrt . ergebnisse die basierend auf den tglichen cbct - verschiebungen berechneten ptv - sicherheitsabstnde betrugen in anteroposteriorer ( ap ) , lateraler ( lt oder linksrechts ) und kraniokaudaler ( cc ) richtung 10 , 4 / 9 , 4 / 9 , 4 mm fr die rl ( 103 patienten ) und 10 , 5 / 22 , 4 / 13 , 7 mm fr die bl ( 139 patienten ) mit signifikantem unterschied fr die ltund cc - richtungen ( p < 0 , 01 ; univariate analyse )  . 
die multivariable analyse identifizierte eine signifikante korrelation zwischen dem bmi und der cc in rckenlage und der ap / lt - marge in bauchlage ( p < 0 , 05 )  . schlussfolgerung in dieser serie ist die repositionierungsgenauigkeit fr die ltund cc - richtungen in bl deutlich schlechter als in rl . 
fr patienten mit einem hheren bmi sind grere sicherheitsabstnde erforderlich . schlsselwrter bauchlage rckenlage strahlentherapie der brust repositionierungsgenauigkeit cone - beamcomputertomographie radiotherapy ( rt ) is an integral part of breast cancer treatment [ 1 ]  . 
in the last decade , wedged tangential fields are replaced by more advanced radiation techniques like tangential field or multibeam intensity - modulated radiotherapy ( imrt ) techniques , allowing a more homogeneous dose distribution and less radiation exposure to organs at risk ( oar ) [ 2 ]  . 
another strategy gaining popularity is to treat the patient in prone position , which has been shown to decrease lung dose in all and heart dose in the majority of patients [ 35 ]  . with these advanced techniques , adequate clinical target volume ( ctv ) to planning target volume ( ptv ) margins became more important to assure proper target coverage . 
 ctv to ptv margins are determined by intraand interfraction errors such as movement of the patient , respiratory motion , anatomy changes ( swelling of the breast ) , and differences in the daily setup [ 6 ]  . 
historically , verification of setup accuracy was done by visual inspection of the treatment field on the patient and / or by portal imaging devices , which only provide 2d information . 
volumetric imaging systems that provide 3d information , e.g. , cone - beam computed tomography ( cbct ) , have been developed to give a more correct estimate of setup errors than electronic portal imaging devices ( epid ) [ 7 ]  . 
this 3d information might not be relevant for supine tangential field radiotherapy with field margins of often 1 cm or more outside the breast , but complex multibeam imrt or arc techniques result in inhomogeneous dose distributions and sharp dose gradients between target and organs at risk ( oars )  . 
in prone position , 3d imaging information is also useful to judge the rotation of the patient and the position of the contralateral breast . in this study we reviewed the cbct setup data of 242 patients receiving wbi to investigate : ( 1 ) prone and supine setup accuracy and required margins and ( 2 ) whether specific subgroups can be identified in which the margins should be individualized . materials and methods we retrospectively reviewed the cbct setup data of 103 supineand 139 prone - treated patients receiving wbi after breast conserving surgery between march 2010 and july 2014 . 
supine position was performed with both arms elevated above the head using the posirest - 2 system ( civco medical solutions , orange city , ia , usa ) and a knee support . 
two different treatment verification protocols were used in supine position : ( 1 ) a daily cbct with online correction or ( 2 ) cbct for the first four fractions with online correction , then calculating the systematic error which was applied to all remaining fractions combined with a weekly cbct verification ( enal protocol )  . 
at each treatment verification , the actual cbct data was coregistered with the planning ct using a clipbox containing the breast , ipsilateral thoracic wall , and a small part of the lung and heart tissue in close proximity of the breast . 
whenever clips were available , it was verified whether the ctv encompassed all visible clips and , if required , manual modification by the radiation technologist was performed . only translational table shifts were applied and documented , using the isocenter as correction reference point . 
 both for the daily cbct protocol and enal protocol , individual errors of each patient were used to calculate the individual and population - based systematic and random errors following the formula published by van herk et al . 
 [ 11 ] in vertical , lateral and longitudinal ( ve , la , lo ) directions separately . a two tailed t - test with independent variance was used to compare the prone and supine cohort . 
univariate and multivariate logistic regression analyses were performed using microsoft excel 2010 ( microsoft , redmond , wa , usa ) with the following input parameters : treatment position ( 0 / 1 = supine / prone ) , age , body mass index ( bmi ) and european cup size ( a , b , c , d , e , f = 0 , 1 , 2 , 3 , 4 , 5 )  . 
a higher bmi led to a larger lo margin in supine position ( p = 0.02 ) and a larger ve ( p = 0.04 ) and la ( p = 0.03 ) margin in prone position . discussion dosimetric advantages of advanced planning techniques and position alterations can only result in a clinical benefit when optimal treatment delivery can be guaranteed . 
in the supine - treated patients cbct was performed because a multibeam imrt technique was used with a steep dose gradients between the target and oars [ 2 ]  . 
this translates in an estimated patient dose of 81 and 38 mgy , respectively , for 15 fractions using a daily or enal protocol ( 5.4 mgy per cbct , [ 10 ] )  . 
the possible negative effects of this very low radiation doses are probably outweighed by the advantages of geometric precision obtained by daily cbct . an overview of the published data on supine and prone setup accuracy for breast irradiation is provided in table 2 . 
comparison of our data to other published work is challenging due to different ( local ) treatment verification protocols and tools [ 6 , 1218 ] , treatment volumes ( wholeversus partial - breast irradiation ) [ 1723 ] , positioning and immobilization devices [ 9 , 24 , 25 ] and the basis of alignment either on bony anatomy , chest wall , breast tissue or surgical clips [ 6 , 15 , 22 , 26 ]  . our supine data are quite similar to other findings [ 6 , 14 , 15 , 19 , 20 , 22 , 25 , 2730 ] with margins of approximately 10 mm or less in each direction . 
prone literature data are not that straightforward with the direction of the largest margin different among different groups , which might be explained by the difference between the designs of the used breast boards [ 9 , 24 , 25 ] and the use of a pure prone or rather a pronelateral position . 
an enal protocol with correction of systematic errors might be an acceptable compromise , but these data emphasize the need of developing dedicated prone breast boards to improve setup accuracy . 
cup size was only withheld in univariate analysis , probably because it is strongly correlated to bmi . this study highlights the need of proper image guidance for supine and prone breast radiotherapy . 
extrapolation of this single - center experience to other centers using other breast boards and other positioning techniques might not be accurate . setup accuracy for prone and supine whole breast irradiationnkol1 3 258 conclusion prone as compared to supine setup accuracy is significantly worse in the lateral and longitudinal directions . 
this study is limited to a single institution and extrapolating these findings to other centers might not be completely adequate . acknowledgments the authors would like to thank the dosimetrists and the radiation technologists of ghent university hospital for their contribution to this work . 
special thanks to georgi nalbantov for the fruitful discussion over the statistical approach and for the critical review of the manuscript and to judit boda - heggemann ( university of mannheim ) for reviewing the german abstract . this study is supported by the national cancer plan , action 29 project 015 , financed by the federal office of health and social affairs , belgium . compliance with ethical guidelines conflict of interest t . 
veldeman state that there are no conflicts of interest . the accompanying manuscript does not include studies on humans or animals . strahlenther onkol ( 2016 ) 192 : 260268 doi 10.1007 / s00066 - 016 - 0951 - 6 radiosensitization in esophageal squamous cell carcinoma effect of polo - like kinase 1 inhibition jenny ling - yu chen1 , 2 , 3 jo - pai chen3 , 4 yu - sen huang1 , 5 , 6 yuan - chun tsai1 ming - hsien tsai1 fu - shan jaw1 jason chia - hsien cheng3 , 7 sung - hsin kuo3 , 7 ming - jium shieh1 , 3 received : 2 december 2015 / accepted : 28 january 2016 / published online : 7 march 2016 springer - verlag berlin heidelberg 2016 abstract purpose this study examined the efficacy of polo - like kinase 1 ( plk1 ) inhibition on radiosensitivity in vitro and in vivo by a pharmacologic approach using the highly potent plk1 inhibitor volasertib . methods and materials human esophageal squamous cell carcinoma ( escc ) cell lines kyse 70 and kyse 150 were used to evaluate the synergistic effect of volasertib and irradiation in vitro using cell viability assay , colony formation assay , cell cycle phase analysis , and western blot , and in vivo using ectopic tumor models . results volasertib decreased escc cell proliferation in a doseand time - dependent manner . 
the combination of volasertib plus irradiation delayed the growth of escc tumor xenografts markedly compared with either treatment modality alone . conclusions the in vitro results suggested that targeting plk1 might be a viable approach to improve the effects of radiation in escc . 
 hierzu wurden zellviabilittsund koloniebildungsunteroriginal article1 3 suchungen sowie zellwachstumsanalysen , immunblots und ektopische in - vivo - tumormodelle herangezogen . ergebnisse volasertib verminderte die escc - zellwucherung auf dosisund zeitabhngige weise . 
volasertib sorgte fr eine wesentliche verbesserung beim strahleninduzierten absterben in escc - zellen durch einen mechanismus , der die verbesserung der phosphorylierung der h3 - histonen und eine deutliche zellzyklusunterbrechung mit sich brachte . 
die kombination von volasertib plus bestrahlung verzgerte das wachstum von escc - tumor - xenotransplantaten deutlich im vergleich zu einer von den beiden behandlungsmodalitten allein . schlussfolgerung diese ergebnisse deuten darauf hin , dass die ausrichtung auf plk1 eine umsetzbare methode zur verbesserung der auswirkungen der strahlung in escc sein knnte . 
daher stellt volasertib einen potentiellen radiosensitizer von escc mit therapeutischem wert dar . arzneimittelscreeningschlsselwrter antitumorale assays strahlentherapie volasertib strahlentoleranz apoptose radiation therapy has been integrated into the multimodal treatment of localized unresectable or recurrent esophageal squamous cell carcinoma ( escc ) [ 19 ]  . 
in this study , we aimed to examine the efficacy of plk1 inhibition on radiosensitivity in in vitro and in vivo models by a pharmacologic approach with the highly potent plk1 inhibitor volasertib . materials and methods cell culture human esophageal squamous cell carcinoma cells ( escc ) , kyse 70 , and kyse 150 , were cultured in rpmi ( roswell park memorial institute ; life technologies , waltham , ma , usa ) supplemented with 10 % ( v / v ) fetal bovine serum ( fbs ; life technologies ) at 37 c under 5 % co2 in a humidified incubator . reagents introduction human polo - like kinase 1 ( plk1 ) is a serine / threonine kinase that is essential in mitotic progression , contributing to multiple processes at the g2 / m transition and throughout mitosis , including activation of the cdk1 / cyclin b1 cascade , centrosome maturation , bipolar spindle formation , and regulation of cytokinesis [ 14 ]  . 
volasertib is a small - molecule potent plk1 inhibitor that shows promising effects in solid malignancy and leukemia [ 9 , 10 ]  . inhibition of plk1 by compounds or small interfering rna in combination with radiation in vitro enhanced the cytotoxic effect of irradiation on cells from medulloblastoma , osteosarcoma , glioblastoma multiforme , head and neck carcinoma , or colorectal cancers [ 1115 ]  . 
for in vivo studies , volasertib was dissolved in hydrochloric acid ( 0.1 n ) and diluted with 0.9 % sodium chloride buffered at ph5 for intraperitoneal administration to nude mice bearing subcutaneous ectopic xenograft tumors . mtt assay mtt ( 3 - [ 4 , 5 - dimethylthiazol - 2 - yl ] 2 , 5 - diphenyl tetrazoliumbromide , sigmaaldrich ) was used to evaluate cell viability . 
absorbance was read at 540690 n data were represented as the percentage reduction in metabolic activity normalized to that of the dmso control . radiosensitization in esophageal squamous cell carcinoma1 3 262 irradiation of cells escc cells in culture flasks were irradiated using a cobalt - 60 unit with different doses of radiation ( 06 gy ) at the rate of 1 gy / mthe distance from the radiation source to the bottom of the flask was set at 80 cdosimetry measurement was performed with an ionization chamber . colony formation assay after 24 - h pretreatment with various doses of volasertib ( 520 nm ) or dmso vehicle ( 0 nm ) , cells ( 1000 / well ) were seeded in 6 - well plates and treated with different doses of radiation ( 06 gy )  . 
the values ( dx ) 1 and ( dx ) 2 can be readily calculated from the median effect equation : ( b ) where dx is the median effect dose obtained from the anti - log of the x - intercept of the , median - effect plot , x - log ( d ) versus , y = log or dm , fa is the fraction affected by dose d and m is the slope of the median - effect plot . 
 the following antibodies were used : anti - phosphorylated histone h3 ( ser10 ) , cyclin b , cyclin a , cyclin d ( santa cruz biotechnology , inc . , santa cruz , ca , usa ) , antihistone h3 , anti - plk1 , and anti - phosphorylated plk1 ( abcam , cambridge , uk )  . 
antibodies to poly - adp - ribose polymerase ( parp ) and b - actin were purchased from cell signaling technology ( danvers , ma , usa ) and santa cruz biotechnology ( santa cruz , ca , usa ) , respectively . 
 b - actin was used as the loading control . cell cycle phase analysis the distribution of cells among the phases of the cell cycle was determined by quantifying the cellular content of propidium iodide - stained dna . 
cells were stained with propidium iodide ( pbs containing 0.5 % tween 20 , 15 g / ml propidium iodide , and 5 g / ml dnasefree rnase ) and analyzed using a becton dickinson facscan flow cytometer equipped with cell quest software ( becton dickinson immunocytometry systems , san jose , ca , usa )  . in vivo studies a total of 20 male balb / c athymic ( nut / nut ) nude mice 6 - weeks - old were purchased from the national laboratory animal center ( taipei , taiwan )  . 
 all mice were group - housed ( 5 mice housed per cage ) under a fixed light - dark cycle with ad libitum access to sterilized food and water , and were evaluated for signs of deteriorating physical and behavioral health with the assistance of veterinary technicians . 
for the ectopic tumor model , a 100l aliquot containing kyse 150 cells ( 2.5 106 ) in 1 : 1 pbs / matrigel solution was injected subcutaneously into the right flank region of the mice . 
when the tumor size became established ( mean starting tumor volume = 96 mm3 ) , the tumorbearing mice were randomized into four groups : ( 1 ) control treatment ( untreated ) , ( 2 ) volasertib ( 20 mgkg 1day 1 on day 1 ) administered intraperitoneally , ( 3 ) radiation therapy ( rt ) alone ( 10 gy on day 2 ) , or ( 4 ) combination of volasertib and rt . 
mice receiving rt were immobilized in a customized harness that exposed the right leg , and the remainder of the body was shielded by five times the half - value thickness of lead . 
the tumors were irradiated using a cobalt - 60 unit with 10 gy on day 2 at a dose rate of 1 gy / min . statistical analysis in vitro data are expressed as the mean the standard deviation ( sd ) and were assessed by students t - test and oneway analysis of variance ( anova ) for comparisons . 
the tumor volume data satisfied the assumptions of normality and homogeneity of variance for parametric analysis ; thus , group means on day 32 for the ectopic tumor models were compared with a one - way anova for multiple comparisons . 
statistical analysis was performed using spss for windows ( spss inc . , chicago , il , usa )  . results radiosensitization induces cell cycle changes we first evaluated the effects of plk inhibition on cell viability without irradiation using the mtt assay . 
notably , 24 - h pretreatment with volasertib ( 20 nm in kyse 70 cells and 10 nm in kyse 150 cells ) and a higher dose of irradiation ( 6 gy ) significantly enhanced radiation - induced reduction in cell survival . 
combination index ( ci ) values were calculated from the dose response data and proved the interaction between volasertib and radiation was synergistic . volasertib plus irradiation augments phosphohistone h3 accumulation targeting plk1 with volasertib led to a distinct mitotic arrest and an accumulation of phosphohistone h3 . 
cells were cultured at a density of 1000 cells / well in 6 - well plates and pretreated with volasertib ( 520 nm ) for 24 h , followed by rt ( 26 gy )  . 
the cell cycle distribution of kyse 70 at 48 h after rt with or without volasertib pretreatment revealed that the combination significantly decreased the g1 population and increased the g2 / m population , indicating a cell cycle shift from the g1 phase to the g2 / m phase . 
at 24 h after irradiation , cell lysates were prepared for western blotting of histone h3 , phosphorylated histone h3 , plk1 , and phosphorylated plk1 to determine if the combination of volasertib and irradiation had an effect on cell - cycle proteins , the expression of cyclins in treated cells was investigated by western blot analysis . 
5 , intraperitoneal treatment of mice with volasertib ( 20 mg / kg on day 1 ) in combination with irradiation ( 10 gy / day on day 2 ) suppressed the growth of established subcutaneous kyse 150 xenograft tumors to a greater extent than that by either treatment alone ( p < 0.05 at day 32 )  . 
in this study , our data showed that the novel plk1 inhibitor , volasertib , acts as a radiosensitizer in escc and results in the synergistic inhibition of survival of escc cell lines in vitro and in vivo . irradiation has been demonstrated to result in unrepaired dna damage and subsequent mitotic catastrophe , raising the possibility that irradiation combined with mitosis inhibitor would be potentially efficient in inducing tumor cell death [ 22 ]  . 
our findings confirmed and were consistent with those reported in other studies , and we believe that our study provides a conceptual advance in targeting escc . targeting plk1 with volasertib disrupts the mitotic spindle assembly , resulting in a distinct mitotic arrest phenotype in prometaphase , accumulation of phosphohistone h3 , and formation of aberrant monopolar mitotic spindles followed by apoptosis [ 23 ]  . 
e volasertib combined with rt showed no significant difference in the expressions of cyclin a or cyclin d in kyse 70 and kyse 150 cells radiosensitization in esophageal squamous cell carcinoma1 3 266 fig . 
nude mice bearing established subcutaneous kse 150 xenograft tumors ( mean starting tumor volume = 96 mm3 ) were randomized into four groups ( n = 5 in each group ) administered volasertib ( 20 mgkg 1day 1 on day 1 intraperitoneally ) , radiation ( 10 gy at day 2 ) , volasertib combined with rt , or control treatment ( untreated )  . 
points : mean ; bars : standard deviation ( sd ) c representative histology of esophageal squamous cell carcinoma ( escc ) xenograft tumors to 2 gy / day results in better outcome when combined with volasertib [ 13 ]  . 
this could be partly explained by the mechanism of accelerated repopulation , wherein few tumors cells surviving the initial chemoor radiotherapeutic treatment demonstrate an ability to repopulate the damaged tumor at an accelerated rate [ 24 , 25 ]  . in preclinical studies , cell lines harboring p53 mutations tended to be more sensitive to plk inhibition [ 17 , 18 ]  . 
taxanes resulted in cell accumulation in the radiosensitive phase and had been demonstrated as a radiosensitizer in escc ; however , taxane - based chemotherapy has been associated with peripheral neurotoxicity , marrow suppression , and decrements in quality of life [ 2729 ]  . 
low - dose volasertib could be an effective radiosensitizer with lesser in vivo toxicities , and it is effective against taxane - resistant tumors . in the current study , volasertib in combination with radiation increased cyclin b levels . 
cyclin b has a similar cellcycle distribution pattern to plk1 , with increased levels in the s - phase and maximal levels at the g2 / m transition [ 30 ]  . 
expression analysis of cyclin b , which peaks during mitosis , indicated that combination of volasertib and irradiation reinforces the accumulation of cells at mitosis , which is a radiosensitive cell cycle phase . 
 using murine xenografts of escc cells , we were able to demonstrate that volasertib is a potent radiosensitizer , highlighting the importance of biological targeting . conclusion the in vitro results suggested that targeting plk1 might be a viable approach to improve the effects of radiation in escc . 
 in vivo studies showed that plk1 inhibition with volasertib during irradiation significantly improved local tumor control when compared to irradiation or drug treatment alone . acknowledgments we thank chih - hong hsu , ta - chen huang , and jhe - cyuan guo for their guidance in conducting this work . 
this work was supported by the national taiwan university hospital yun - lin branch ( grant number : ntuhyl 104.i002 ) and the national taiwan university hospital hsin - chu branch ( grant number : 105 - hch - 032 )  . 
the work was presented in part at the 15th international congress of radiation research ( icrr ) , may 2529 , 2015 , kyoto , japan . compliance with ethical standards conflict of interest j.l.y. 
shieh state that there are no conflicts of interest . all national guidelines on the care and use of laboratory animals have been followed and the necessary approval was obtained from the relevant authorities . electronic supplementary material s1 fig . 
esophageal squamous cell carcinoma ( escc ) cell lines ( a ) kyse 70 and ( b ) kyse 150 were seeded in 96 - well plates in triplicate and treated with various concentrations of volasertib for 24 , 48 , or 72 h . 
mrz 2017 springer - verlag berlin heidelberg 2017 hintergrund technische entwicklungen , wie die der intensittsmodulierten strahlentherapie ( imrt ) und der bildgefhrten strahlentherapie ( igrt ) , welche einerseits die modellierbarkeit der dosisverteilung und andererseits die zuverlssigkeit der dosisapplikation verbessern , sind prinzipiell geeignet , die strahlentherapie noch wesentlich zu optimieren . 
dass dies auch im vergleich mit konventioneller 3d - konformaler strahlentherapie ( 3d - crt ) unter den bedingungen routinemiger durchfhrung erreicht werden kann , ist gegenstand vieler untersuchungen , so auch bezglich des auftretens von sptfolgen an risikoorganen bei der strahlentherapie des prostatakarzinoms . methoden in der vorliegenden arbeit werden unterschiede in hugkeit und schwere gastrointestinaler ( gi ) sowie urogenitaler ( ug ) sptnebenwirkungen bei beiden therapieverfahren verglichen . 
fr die ig - imrt - kohorte waren dies 242 patienten aus dem standardarm einer hypofraktionierungsstudie der jahre 20072010 ; fr die 3d - crt - kohorte wurden 189 patienten aus dem dosiseskalationsarm einer studie der jahre 19972003 herangezogen . 
beide gruppen unterscheiden sich in mehreren ausgangsparametern der teilnehmenden patienten als auch in vorgaben fr die bestrahlungsplaoriginalpublikation wortel rc , incrocci l , pos fj et al ( 2016 ) late side effects after image guided intensity modulated radiation therapy compared to 3d - conformal radiation therapy for prostate cancer : results from 2 prospective cohorts . 
kumulative inzidenzen auftretender nebenwirkungen wurden bis zu einer beobachtungszeit von 5 jahren mittels kaplan - meier - methode und der einuss des therapieverfahrens mittels cox - regression beschrieben . ergebnisse wie zu erwarten , zeigte sich beim einsatz von ig - imrt bei der therapie von prostatakarzinompatienten im vergleich zur 3d - crt eine deutliche reduktion der dosis an risikoorganen . 
whrend die pollakisurie bei ig - imrt reduziert auftrat , ergaben sich bei nykturie und harninkontinenz eher vorteile fr die 3d - crt . schlussfolgerung der autoren durch ig - imrt werden die gi - nebenwirkungen gegenber der 3d - crt deutlich reduziert . 
hier kann die igrt deutliche verbesserungen bewirken , wenn sie mglichst oft zur positionierungskontrolle angewandt wird [ 3 ]  . der vorteil der kombinierten imrt mit igrt gegenber der konventionellen 3d - crt wird von den autoren am beispiel der gi - nebenwirkungen eindrucksvoll dargestellt . 
da die unterschiede zwischen den kohorten bei weiteren parametern wie stadium , gleasonscore , risikogruppe sowie die anzahl mitbestrahlter samenblasen eher die ig - imrt - gruppe belasten , wird dies am ergebnis nichts grundstzliches ndern . 
ein eindeutiger , die 3d - crt - gruppe benachteiligender unterschied sind die stark differierenden vorgaben fr die sicherheitsrnder um das zielvolumen , die fr die 3d - crt - gruppe mit generell 10 mm , fr die ig - imrt - gruppe zum greren teil mit 56 mm und fr einen kleineren patientenanteil mit 68 mm angegeben werden . 
grund fr die unterschiede sind die lokalen richtlinien der beiden studien , denen die vorgestellten kohorten entnommen wurden . planerisch sind jedoch trotz der schlechteren konformitt dieser technik auch bei 3d - crt durchaus kleinere sicherheitsrnder mglich . 
ein vergleich von ig - 3dcrt bei entsprechend angepassten optimierungsparametern mit ig - imrt wre sicher anders ausgefallen . dass beide methoden bezglich des therapieerfolgs gleiche ergebnisse liefern , ist anzunehmen , da ansonsten dem vergleich die grundlage fehlte . 
berraschend und nicht verstndlich ist , dass in der zusammenfassung der autoren die vorteile der nebenwirkungsreduktion fr den gi - bereich als grund fr eine prferenz der ig - imrt aufgefhrt werden , die weniger vorteilhaften ergebnisse fr den ug - bereich aber keine erwhnung mehr nden . norbert hodapp , freiburg interessenkonikt n . 
yamazaki h , nakamura s , nishimura t et al ( 2014 ) transitioning from conventional radiotherapy to intensity - modulated radiotherapy for localized prostate cancer : changing focus from rectal bleeding to detailed quality of life analysis . 
sorsetti1 , 2 received : 22 april 2016 / accepted : 6 january 2017 / published online : 6 february 2017 springer - verlag berlin heidelberg 2017 abstract background this study aimed to analyse the feasibility and acute toxicity of radical hypo - fractionated radiotherapy ( rt ) for elderly patients with non - small - cell lung cancer ( nsclc )  . patients and methods we conducted a retrospective evaluation of treatment with volumetric modulated arc therapy ( vmat ) of elderly patients affected by stage iii inoperable nsclc . 
the primary end point was acute and late toxicity , while secondary end points were progression - free survival ( pfs ) , and overall survival ( os )  . results in all , 41 patients were included in this analysis . the mean age of the patients was 78.6 years , and 22 patients had staged iiia while 19 patients had stage iiib disease . 
at a mean follow - up of 9.9 months ( range , 1.125.4 ) , 17 patients had died from disease progression , one died from other causes , and 23 were alive . 
als sekundre endpunkte wurden progressionsfreies berleben ( pfs ) und gesamtberleben ( os ) deniert . ergebnisse es wurden 41 patienten ( stadium iiia : n = 22 , iiib : n = 19 ) in die analyse eingeschlossen . 
der einsatz der hypofraktionierten radiotherapie beim bronchialkarzinom des lteren patienten kann als ntzlicher ansatz betrachtet werden , insbesondere bei patienten mit schlechtem performance - status oder bei ablehnung anderer anstze . schlsselwrter nichtkleinzelliges bronchialkarzinom gezielte strahlentherapie toxizitt progressionsfreies berleben ltere personen non - small - cell lung cancer ( nsclc ) is a common cause of cancer death [ 1 ]  . 
approximately half of lung cancer cases are diagnosed in people aged more than 70 years and ~15% of cases are diagnosed in patients older than 80 years [ 2 ]  . concurrent chemo - radiation ( crt ) is the mainstay of treatment for un - resectable nsclc , because of a 4.5% increase in 5 - year overall survival ( os ) from 10.6% with sequential chemotherapy to 15.1% with concomitant chemotherapy [ 3 ]  . 
however , even with concurrent treatments , the median os ranged from 14 to 17 months with less than 25% of the patients alive at 3 years [ 4 ]  . 
an estimated 60% of the patients , particularly the elderly , with locally advanced disease are unt for concomitant crt because of their poor performance status and co - morbidities [ 5 ]  . sequential crt and exclusive radiotherapy ( rt ) are options available for patients not suitable for concomitant approaches . 
despite a standard rt dose of 60 gy , the models for tumour control probability suggest that a dose of 84 gy would be required to achieve 50% probability at 3 years [ 6 ]  . 
this estimate correlates with real clinical practice , as rt alone is associated with a 5 - year survival of less than 5% due to local , regional and distant relapse and a poor local control ( lc ) , with reported 2 - year loco - regional control rates of 2044% [ 3 , 7 , 8 ]  . 
the results of the rtog 0617 protocol showed that the higher radiation dose ( 74 gy arm ) was detrimental in terms of os and local progression compared with the standard dose of 60 gy [ 9 ]  . 
it is likely that the extended therapy time plays an important role in this setting . since prolonging the treatment time beyond 6 weeks has a negative impact on os [ 10 ] , two strategies for dose escalation are applicable : hyper - fractionation and hypo - fractionation . concerning hyper - fractionation , there are several barriers to the widespread implementation of this approach , including the complicated logistics and increased resources required to deliver these dose schedules . 
moreover , hyper - fractionated or accelerated rt reduced deaths resulting from lung cancer and there was a non - signicant reduction of non - lung cancer deaths , while the use of hyperfractionated or accelerated rt increased the risk of acute oesophageal toxicity but did not have an impact on the risk of other acute toxicities [ 11 ]  . elderly patients are often neglected in clinical trials . 
however , this population urgently needs effective regimens that omit concurrent systemic therapy , which is often unsuitable for elderly patients . based on these considerations , a retrospective analysis was conducted of elderly patients treated at our institution according to hypo - fractionated schedules , with no concomitant chemotherapy . 
we aimed to evaluate the safety and feasibility of intensity modulated rt with volumetric modulated arc therapy ( vmat ) in an elderly population , analysing toxicity ( expecting oesophageal and pulmonary toxicity as the main risks ) and outcome following an earlier investigation on the role of stereotactic radiation oncology for oligo - metastatic elderly patients [ 12 ]  . strahlenther onkol ( 2017 ) 193 : 385391 patients and methods this is a retrospective observational study , based on treatment with hypo - fractionated rt of patients aged 70 years with a performance status ( ps ) of 02 . 
given the concern for increased toxicity with hypo - fractionated rt and concurrent chemotherapy , the latter was not considered for this study . the lung functionality was required to show at least 40% of the expected value for both the forced expiratory volume at 1 s ( fev1 ) and the lung diffusion capacity for carbon monoxide ( dlco )  . 
patients were excluded from this analysis in the case of prior thoracic rt or lung function < 40% of the expected value for fev1 and dlco . all the patients underwent contrast - enhanced computed tomography ( ct ) scan and uorodeoxyglucose ( fdg ) - ct positron emission tomography ( pet ) for simulation of the treatment and were immobilized in a supine position with thermoplastic masks for the thoracic and abdominal region . if the respiratory excursion was larger than 5 mm , four - dimensional ct ( 4d - ct ) imaging was performed . 
the clinical tumour volume ( ctv ) included the pulmonary lesion and clinically positive lymph nodes with a short - axis diameter of > 1 cm and / or positive nodes at pet study . 
in all the patients who underwent 4d - ct scan , an internal target volume ( itv ) was dened as the envelope of all gross tumour volumes ( gtvs ) in the different respiratory phases . 
the adopted treatment technique was volumetric modulated arc therapy ( vmat ) in the rapidarc fortwo to four partial arcs were used for the optimization with arc length and collimator angle adjusted to best t the individual anatomy of the patients . 
a minimum target coverage was imposed so that more than 95% of the ptv received more than 95% of the prescribed dose . the treatment planning methods and the dose constraints were derived from earlier investigations [ 13 ] for contraand ipsi - lateral lungs , heart , spinal cord and oesophagus . for these , the primary objectives were : spinal cord : d1% < 46 gy ; contralateral lung : v20gy < 30% , mean dose < 15 gy ; oesophagus : d55gy < 305 ( and d1% < 70 gy ) ; heart : v50gy < 20% , v45gy < 30% . 
concerning the large involvement of the ipsi - lateral lung , no explicit constraints were applied to this structure but v20gy was subject to the request to be as low as reasonably achievable . treatment image guidance to ensure accurate patient positioning was performed by means of cone beam ct ( cbct ) at every session . 
patients were evaluated for toxicity on a weekly basis during rt . the evaluation of the patients included history and physical examination , blood tests ( including a metabolic panel and haematological prole ) , karnofsky performance score ( kps ) and toxicity assessment . 
haematological and non - haematological toxicities were graded according to the common terminology criteria for adverse events version 4.0. contrast - enhanced ct imaging was performed within 2 months of rt and every 3 months thereafter . 
late toxicity was dened as side effects occurring after 90 days from the end of rt . results between december 2012 and march 2015 , 41 patients aged 70 years were treated at our institution for locally advanced nsclc . 
the median age at diagnosis of lung cancer was 78.6 years ( range , 7086 ) ; patients characteristics are listed in table 1 . of the patients , 15 ( 37% ) had received chemotherapy before rt ( mostly cisplatin or carboplatin plus gemcitabine or pemetrexed ) ; the median number of prescribed cycles was 4 . a temporary interruption of the treatment was needed only in one case for acute pneumonitis . 
although the follow - up is too short for an accurate estimation of late toxicity , the analysis of the raw data showed 13 ( 32% ) patients reporting g12 side effect , mostly radiation pneumonitis ( 6 cases , 15% )  . 
owing also to the small sample , the dose , fractionation schedules , age and ps did not show any statistically signicant correlation with side effects . during the follow - up , a complete response was obtained in two ( 5% ) patients ; partial response or stable disease was recorded in 26 ( 63% ) and nine ( 22% ) cases , respectively . two ( 5% ) patients had progressive local disease at their rst evaluation , one ( 2% ) was lost to follow - up immediately after rt and the remaining patient died a few days after the end of rt in a car accident . at the median follow - up of 9.5 months ( mean , 9.9 ; range , 1.125.4 ) , 17 ( 41% ) patients had died from disease progression , one patient died from other causes , eight ( 19% ) patients were alive with distant metastases , and 15 ( 37% ) were alive without distant progression . 
local progression was recorded in ten patients ( 24% ) , while distant metasoesophagitis acute latea pneumonitis acute latea dyspnoea acute latea 23 ( 56% ) 36 ( 94.7% ) 9 ( 22% ) 2 ( 5.3% ) 9 ( 22% ) 40 ( 97.5% ) 32 ( 84.2% ) 1 ( 2.6% ) 1 ( 2.5% ) 5 ( 13.2% ) 35 ( 85.3% ) 38 ( 100% ) 2 ( 4.9% ) 4 ( 9.8% ) athree patients not available for late - toxicity analysis tases occurred in 20 cases ( 49% )  . 
we chose to include in this study patients aged 70 years , since there is general consensus in clinical practice to consider this age as the threshold in risk assessment [ 14 ]  . apart from an increased chronological age , the general condition and performance status of elderly patients are also signicantly improved compared with the past , posing a challenge for physicians to nd the right balance between underand over - treatment . 
it is clear that biological age is more important than chronological age and that we need objective evaluation systems , like the comprehensive geriatric assessment ( cga ) , for a better decision about treatment for elderly patients [ 15 ]  . 
in our study , lacking an objective evaluation , patients were selected on the basis of their chronological age , the absence of severe co - morbidities and their performance status . 
this is a limitation of our study , but the results obtained suggest that the prognostic evaluation before dening the treatment was fundamentally strahlenther onkol ( 2017 ) 193 : 385391 fig . 
1 overall survival ( a ) and progression - free survival ( b ) curves impact of histology on overall survival ( a ) and progression - free survival ( b )  . 
however , the gca assessment will soon be introduced into clinical routine . the standard treatment for locally advanced nsclc is combined crt , which has been showed to be superior to rt alone [ 16 , 17 ]  . 
however , elderly patients with lung cancer have been signicantly under - represented in clinical trials . therefore , identifying a standard treatment in this population is very difcult and the treatment recommendations for this group have often been conicting . 
furthermore , the survival advantage with concomitant ct is associated with an obvious increased risk of toxicity [ 18 ] and elderly patients are more susceptible to side effects than younger patients are . 
the toxicity reported here is significantly lower , suggesting a better selection of patients . in the present study , the patients were allowed to receive chemotherapy before rt according to the oncologists discretion , but concomitant treatment was avoided , owing to concerns about toxicity . 
this study reported extremely promising results , with a 2 - year os of 54% in the concurrent arm and similar toxicity in this arm to the sequential arm [ 20 ]  . 
however , in the soccar trial the median age of patients in the concurrent arm was 61 years and only 14% of patients were aged 70 years . 390 strahlenther onkol ( 2017 ) 193 : 385391 in this study we treated our patients using intensive rt schedules to maximize the efcacy of the treatment and the loco - regional control . 
the other main factor to consider is the overall treatment time ( ott ) , which must be kept below 6 weeks because it has been demonstrated that there is a drop in the absolute 3 - year survival rate of 1.6% per day of ott prolongation beyond 6 weeks due to rapid tumour repopulation in nsclc [ 10 ]  . 
in lung cancer , hypo - fractionated schedules with an ott of < 6 weeks are predicted to be more benecial than short hyper - fractionated schedules or prolonged conventionally fractionated treatments [ 22 ]  . 
in our experience , tolerance to the treatment was good , with rates of acute and late toxicity conrming the results of three studies that compared standard fractionation with a hypo - fractionated scheme ; all these studies did not report any signicant differences in toxicity between the regimens [ 2325 ]  . 
in a meta - analysis published in 2015 on many different schedules of hypo - fractionated rt , acute oesophageal toxicity occurred in 08% of patients , and acute pulmonary toxicity occurred in 010% of patients . 
late oesophageal toxicity occurred in 05% of patients , and late pulmonary toxicity occurred in 018% of patients [ 21 ]  . pfs and os in our experience were encouraging . 
actuarial os was reported for 1 - year ( 4175% ) and 2 - year ( 1842% ) time points [ 21 ]  . in our opinion , we should highlight these results considering the age and general conditions of our patients , which were not an ideal population . 
joo and co - workers [ 26 ] retrospectively reviewed their experience in elderly patients treated with 66 gy in 30 fractions , reporting actuarial os rates at 2 and 3 years of 39% and 23% , respectively , and cause - specic survival rates at 2 and 3 years of 57% and 47% , respectively . we found that hypo - fractionated rt in advanced lung cancer in elderly patients is safe and feasible , with promising results . 
with an objective evaluation of frailty , using a dedicated and specic scale for geriatric assessment , we would be able to select elderly patients who can be treated as younger patients . 
furthermore , rt alone ensures a 4% relative improvement in survival and 3% relative improvement in loco - regional control for every 1 gy bed increase [ 28 ]  . 
experiences with dose escalation have been published in past few years , but the evidence is limited by the heterogeneity and the small number of patients enrolled , being for the most part single - institution protocols . 
furthermore , also in these series , elderly patients are often under - represented . conclusion moderately hypo - fractionated rt was found to be promising in terms of safety and was associated with a modest pattern of toxicity for elderly patients with locally advanced lung cancer . 
this work reports on cosmetic results following apbi using multicatheter high - dose - rate interstitial brachytherapy ( hdribt )  . patients and methods between 2006 and 2014 , 114 patients received adjuvant apbi using multicatheter hdr - ibt . 
a lower dnr value is signicantly associated with a better cosmetic outcome . keywords photographs breast - conserving surgery toxicity survival breast cancer kosmetische vernderungen nach operation und akzellerierter teilbrustbestrahlung mittels hdrinterstitieller brachytherapie auswertung durch einen multidisziplinren multigenderausschuss zusammenfassung einleitung brustkrebspatientinnen im frhstadium knnen nach einer brusterhaltenden operation ( bcs ) von einer adjuvanten akzelerierten teilbrustbestrahlung ( apbi ) protieren . 
die vorliegende arbeit berichtet ber die kosmetischen ergebnisse nach apbi mittels hdr - interstitieller brachytherapie ( hdr - ibt ) in multikatheter - technik . methoden zwischen2006 und 2014 hatten 114 patientinnen eine adjuvante apbi mittels mulitkatheter - hdr - ibt erhalten . 
von jeder patientin wurden 2 fotograen analysiert : die erste wurde nach der operation , aber vor implantation der brachytherapiekatheter ( basisbild ) aufgenommen , die 368 strahlenther onkol ( 2017 ) 193 : 367374 zweite bei der letzten nachuntersuchung . 
dosis - volumen - histogramm - ( dvh - ) parameter und die beobachteten kosmetischen vernderungen wurden auf mgliche korrelationen untersucht . ergebnisse die mediane nachbeobachtungszeit betrug 3 , 5 jahre ( spanne 0 , 68 , 5 jahre )  . 
eine verschlechterung der kosmetik der brust tritt bei weniger als 5 % der patientinnen edie endgltigen kosmetischen ergebnisse bei mit bcs und hdr - ibt behandelten patientinnen werden vor allem durch das kosmetische ergebnis der operation beeinusst . schlsselwrter fotograen brusterhaltende operation toxizitt berleben brustkrebs breast - conserving therapy ( bct ) comprising breast - conserving surgery ( bcs ) followed by whole breast irradiation ( wbi ) is the standard of care in management of early - stage breast cancer patients with long - term follow - up results [ 13 ]  . 
apbi delivers a higher dose per fraction to a limited volume of breast tissue ( tumor bed plus a margin ) within 1 week , thus decreasing the treatment time and also decreasing the radiation dose to the contralateral breast , skin , lungs , and heart . 
multiple techniques are used three - dimensional radiation therapy ( 3drt ) , for apbi : stereotactic body radiation therapy ( sbrt ) , multicatheter high - dose - rate interstitial brachytherapy ( hdr - ibt ) , intraoperative radiation therapy , and endocavitary brachytherapy [ 48 ]  . the clinical outcomes of apbi have been investigated in several studies . 
some of these used multicatheter hdribt for apbi delivery , with promising long - term clinical outcomes comparable to the results of wbi series [ 916 ]  . in a recently published randomized large phase iii clinical trial , adjuvant apbi using multicatheter hdr - ibt following bcs in early breast cancer patients was not inferior to adjuvant wbi in terms of 5 - year local control , disease - free survival , and overall survival [ 17 ]  . few published series have reported data indicating modest and acceptable rates of acute and late toxicity following apbi using multicatheter hdr - ibt . 
the present work represents a single - institution retrospective study and reports on cosmetic changes following apbi using multicatheter hdr - ibt compared to the baseline postoperative status . patients and methods between may 2006 and december 2014 , 256 female patients received adjuvant apbi using multicatheter hdribt following bcs . 
the treatment records of these patients were reviewed and patients having photographs recording breast cosmesis were included in the analysis ( 114 patients )  . the excluded patients had either no baseline photographs ( 10 patients ) , no follow - up photographs ( 129 patients ) , or the photographs had not been properly taken ( 3 patients )  . for each included patient , two photographs documenting the changes in breast cosmesis before and after apbi using multicatheter hdr - ibt were analyzed . 
the photographs were taken by a physician or a trained nurse , with a frontal view without identication the patient , from the neck to the midabdomen . the cosmetic result for each photograph was assessed by a multigender multidisciplinary team ( mdt )  . 
score 1 ( excellent ) was given when the treated breast was nearly identical to the untreated breast ; score 2 ( good ) when the treated breast was slightly different from the untreated breast ; score 3 ( fair ) when the treated breast was clearly different from the untreated breast but not seriously distorted ; and score 4 ( poor ) when the treated breast was seriously distorted . 
during the follow - up visits , the physician asked each patient to score her own breast cosmetic outcome on a four - point scale ( excellent , good , poor , and bad ) , which corresponded to the harvard cosmesis scale . 
the patient - reported self - score was documented at the last follow - up visit ( at the same time as the nal photograph )  . patients were treated with an hdr remote afterloading device ( microselectron and later flexitron ; elekta brachytherapy , veenendaal , the netherlands ) using an 192ir stepping source with 370 gbq initial activity . 
the majority strahlenther onkol ( 2017 ) 193 : 367374 table 1 brachytherapy details table 2 patient and disease characteristics value characteristic n = 114 ( 100% ) detail timing total dose v100 average ( sd ) v150 average ( sd ) dnr average ( sd ) skin dmax per fraction average ( sd ) median no . 
during the procedure , a mobile digital c - arm was used to identify the exact site of surgical clips denoting the tumor bed through multiangle x - ray images . 
a median of 15 guide needles were inserted into the target area in a triangular manner through multiple levels , with interspacing of the needles a ranging from 10 to 16 mthe needles were subsequently replaced by plastic catheters . volume denition and dose planning were performed on the three - dimensional reconstructions of thin - slice ct images of the patient . 
the clinical target volume ( ctv ) included the estimated volume of the tumor bed , the surgical clips , and a 1020 mm safety margin , according to the size of the reported surgical margin and excluding the skin and the thoracic wall . 
the smallest allowed distance between the skin surface and the last source position was 1 cthe quality of the treatment plan was assessed using dvh parameters : v100 ( volume receiving 100% of the prescribed dose ) , v150 ( volume receiving 150% of the prescribed dose ) , and dnr ( dose nonuniformity ratio = v150 / v100 )  . 
representative photographs of 3 patients ( a , b , c )  . for each patient , two photographs were assessed : baseline ( upper ) and last follow - up ( fu ; lower )  . 
note the change in the cosmesis score table 5 analysis of variables associated with change in cosmesis variable stationary / worse cosmesis improved cosmesis p - value age ( years ; mean sd ) tumor size ( cm ; mean sd ) v100 ( cc ; mean sd ) v150 ( cc ; mean sd ) dnr ( mean sd ) skin dmax ( gy ; mean sd ) type of surgery tumor location no . 
the analyzed variables included patient age , tumor site , tumor size , type of surgery , number of brachytherapy catheters , v100 , v150 , dnr , and skin dmax . discussion recently , the 5 - year toxicity and cosmetic results of the rtog protocol 95 - 17 [ 19 ] have been made available . 
fat necrosis was found in 15% of patients . different results are found in the cosmetic report on the phase iii randomized trial from the national institute of oncology ( nio ) budapest [ 25 ] , in which polgr et al . 
re372 strahlenther onkol ( 2017 ) 193 : 367374 table 6 analysis of variables associated with nal cosmesis variable favorable cosmesis unfavorable cosmesis p - value age ( years ; mean sd ) tumor size ( cm ; mean sd ) v100 ( cc ; mean sd ) v150 ( cc ; mean sd ) dnr ( mean sd ) skin dmax ( gy ; mean sd ) type of surgery tumor location no . 
a multicentric study conducted by the groupe europen de curiethrapie / european society for radiotherapy and oncology ( gec - estro ) investigated clinical outcome and toxicity following salvage lumpectomy and multicatheter brachytherapy ( low - dose - rate , 12.4% ; pulsed - doserate , 40.6% ; or high - dose - rate , 47% ) for ipsilateral breast tumor recurrence . 
this study reported favorable cosmetic results in 85% of the patients and 11% g3 / g4 toxicities , although all patients had previous surgery and wbi [ 26 ]  . the current study found a nal favorable cosmesis outcome rate of 82.4% as reported by the patients and 81.5% as reported by the mdt . 
in one study the rate of pain was 28.8% [ 19 ] , while another study showed a decrease in pain rates over time , with 16.4% at 6 months and 11.4% at 2 years of follow - up [ 29 ]  . 
the slightly worse cosmetic outcome and higher toxicity rates of the rtog 95 - 17 trial could be attributed to the treatment techniques , as all of the patients were treated using two - dimensional techniques without any precautions or limitation of the skin dose . the impact of surgery on breast cosmesis is an important factor for the nal cosmetic outcome . 
the randomized trial of accelerated partial breast irradiation ( rapid ) phase iii trial randomized 2135 early breast cancer patients between apbi using 3drt and wbi , and recorded baseline as well as 3 - year posttreatment breast cosmetic scores . 
in the interim report on toxicity and cosmesis , deterioration in the nurse - assessed cosmetic score was 33.8% in the apbi arm and 20.8% in the wbi arm [ 31 ]  . in the present study there is a 20% increase in the rate of favorable cosmesis over time . 
these authors also found a 23% increase in the rate of excellent cosmesis ( 10% at 6 months , 33% at 5 years ) [ 29 ]  . most patients in the current study received oncoplastic breast surgery and none underwent open - cavity surgery , which has a signicant impact on the change in breast contour and nal cosmesis . 
analyzed the variables associated with unfavorable cosmetic outcome following apbi using multicatheter hdr - ibt and found four associated variables : v150 , v200 , dose homogeneity index ( dhi ) , and the total number of source dwell positions [ 32 ]  . 
although the strahlenther onkol ( 2017 ) 193 : 367374 total number of patients included in the present analysis is relatively small , analyses were performed on multiple variables to identify those that are signicantly associated with the nal cosmetic outcome ( comparing favorable versus adverse cosmesis ) or with the change in cosmesis between the two evaluated photographs ( comparing same / worse scores versus improved scores )  . 
this signies the importance of respecting the concept of dose homogeneity , even when using intensity modulation in the hdr brachytherapy treatment plans . surgical cosmesis often improves over time and the radiation - induced cosmetic changes progress over time [ 33 ]  . to assess the change in breast cosmesis following bcs and apbi using interstitial brachytherapy , most prospective trials used a xed time point in the follow - up period , for instance after 1 year or 5 years of follow - up [ 9 , 19 , 29 ]  . 
using the last followup visit as the chosen point for breast cosmesis assessment may not be ideal , but due to the limitations of retrospective data analysis , it remains an acceptable choice . concerning the results of the present study , a trend was found toward improvement in the nal cosmetic result ( at the last follow - up visit ) over time compared to the baseline cosmetic result ( 34 weeks after surgery ) , which could be explained by healing of the breast wound . 
if multicatheter hdr - ibt is performed in a technically suitable way , it will probably not interfere with the normal process of healing , resulting in favorable rates of good nal cosmetic results and late toxicity . conclusion apbi using multicatheter hdr - ibt following modern bcs techniques in low - risk breast cancer has an acceptable nal cosmetic outcome . 
stojanovic - rundic declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
bowen1 , 2 received : 25 october 2016 / accepted : 7 february 2017 / published online : 2 march 2017 springer - verlag berlin heidelberg 2017 abstract purpose to design and apply a framework for predicting symptomatic radiation pneumonitis in patients undergoing thoracic radiation , using both pretreatment anatomic and perfused lung dosevolume parameters . materials and methods radiation treatment planning ct scans were coregistered with pretreatment [ 99mtc ] maa perfusion spect / ct scans of 20 patients who underwent denitive thoracic radiation . 
anatomische lungendosis - volumen - parameter wurden mittels behandlungsplanungsscans erhoben und perfundierte dosis - volumenparameter mittels spect / ct - scans whrend der vorstrahlenther onkol ( 2017 ) 193 : 410418 behandlung berechnet . 
gleichwertige dosen von 2 gy / fraktion wurden in der lunge berechnet , um abweichende behandlungsregime und rumliche schwankungen der lungengngigen dosis ( eqd2lung ) auszugleichen . ergebnisse anatomische ( mld ) und funktionale parameter der lungendosis ( pmld70% ) wurden als prdiktoren einer strahlenpneumonitis vom grad 2 ( auc > 0 , 93 ; p < 0 , 01 ) bestimmt . 
nicht alle patienten mit hoher anatomischer lungendosis ( mld > 13 , 6 gyeqd2lung ; 19 , 3 gy bei patienten mit 60 gy in 30 fraktionen ) entwickelten eine strahlenpneumonitis , jedoch alle , die zur perfundierten lunge zudem eine hohe mittlere dosis aufwiesen ( pmld70% > 13 , 3 gyeqd2 )  . schlussfolgerung die vorluge anwendung des rahmenwerks ergab bei dem begrenzten patientenkollektiv unterschiede zwischen anatomischer und perfundierter lungendosimetrie . 
radiation pneumonitis after denitive doses is associated with signicant morbidity with moderate to severe pulmonary toxicity of approximately 1030% and fatal toxicity in 2% of these patients [ 1 , 2 ]  . 
anatomic lung constraints have been explored in the literature and are predictive for lung injury , most notably volume of lung receiving > 20 gy ( v20gy ) and mean lung dose ( mld ) , as well as additional risk factors , including elevated dose rate , concurrent carboplatin / paclitaxel , and older age [ 25 ]  . 
however , the predictive values of anatomic constraints are suboptimal , and even with v20gy < 20% , there is still about an 18% chance of grade 2 pulmonary toxicity [ 2 ]  . single photon emission computed tomography ( spect ) is a sensitive modality for measuring regional lung physiological processes . 
pretreatment spect imaging has shown perfusion defects at the tumor site and adjacent tissue [ 6 ]  . perfusion has been shown to be a sensitive metric for assessing radiation induced - lung injury [ 7 ]  . 
data from duke university [ 6 , 8 ] , the netherlands cancer institute ( nki ) [ 9 ] , and princess margaret hospital ( pmh ) have suggested a doseresponse relationship between regional perfusion changes on spect imaging and dose delivered , an association between a decline in pulmonary function test ( pft ) values and changes in regional perfusion variables posttreatment , and a correlation between perfusion changes posttreatment and risk of later developing radiation pneumonitis [ 10 ]  . 
these studies have provided useful functional metrics but have not been able to produce functional lung constraints that can replace the anatomic parameters currently in use . spect imaging comes with limitations of lower spatial resolution , quantitative uncertainties such as spatially varying attenuation , scatter , detector response , and time duration for image acquisition [ 11 ]  . 
integration of ct with spect provides data for attenuation and scatter correction , but primarily increases the specicity of ndings through spatially colocalized anatomical data with physiologic uptake [ 12 ]  . technical advances in scatter estimation and spatial resolution recovery have increased the potential for quantitative imaging with spect / ct [ 1315 ]  . 
we incorporated spect / ct acquisition and reconstruction protocols with data corrections , along with high spatial alignment accuracy through scanning of patients immobilized in treatment position , for improved parameter estimation . 
similar to other published studies , we assessed associations between varying levels of functional lung dose and volume parameters to the incidence of clinical radiation pneumonitis [ 9 , 16 , 17 ]  . 
however , we extended this work by evaluating a range of dose volumes and perfusion mean lung dose parameters on modern spect / ct , while seeking complementarity between anatomic and functional image features . 
in addition , we accounted for differences in radiation therapy fractionation , as well as regional variation in lung tissue fractional dose , in our patient cohort by converting physical radiation dose distributions to equivalent 2 gy per fraction equivalent dose distributions . methods and materials patient characteristics the framework was applied to a cohort of patients with the approval of the university of washington institutional review board ( irb )  . 
the clinical characteristics of the patients were collected and are further described in table 1 . pulmonary morbidity was graded by the national cancer institutes common terminology criteria for adverse events version 4 for pneumonitis . 
patients were dichotomized for pulmonary toxicity based on presence or strahlenther onkol ( 2017 ) 193 : 410418 absence of grade 2 pneumonitis , dened by ctcae v4 as the clinical indication for prednisone administration . 
complete details of patient characteristics can be found in supplemental table 1 . image acquisition and treatment planning patients were simulated for radiation therapy with a respiratory - correlated 4dct simulation scan , which required abdominal compression for those receiving stereotactic body radiation therapy ( sbrt )  . 
the clinical target volume ( ctv ) and planning target volume ( ptv ) were constructed based on microscopic disease extension , respiratory motion , and setup uncertainties following icru83 . 
ctv margins were typically 58 mm ( 0 mm for sbrt ) , and ptv margins were 510 mtarget volumes were constructed following a similar paradigm for all radiation treatment modalities . 
radiation therapy plans were generated in pinnacletm ( philips healthcare ) for photon therapy or cms xiotm ( elekta inc . ) for uniform scanning proton therapy , and radiation dose was calculated exclusively on the phase - averaged 4dct images . 
free - breathing helical ct scans used for spect attenuation and scatter correction were rigidly coregistered with the respective phase - averaged 4dct images , while end - exhale helical ct were coregistered with the appropriate end - exhale phase 4dct . 
registration accuracy was evaluated over the total lung , with particular attention given to regions near the tumor , regions with high perfusion , and regions with high anatomic reproducibility where indicated such as the spine , mediastinum , and great vessels . 
radiation dose distributions in the lung were converted to biologically equivalent voxel dose distributions in 2 gy fraction sizes ( eqd2lung ) using the linearquadratic model for a clinical endpoint of pneumonitis ( / = 3 gy ) [ 3 , 18 ]  . 
this methodology accounted for differences in treatment regimens as well as spatial variations in lung fractional dose . anatomic regions of interest included total lung minus gtv ( tl - gtv ) , and functional lung regions of interest included threshold percentages of maximum perfusion ( 595% , 5% increments ) within tl - gtv , to generate perfusion ptl - gtvxx% . 
from these regions , anatomic dosimetric parameters were extracted : mean lung dose ( mld ) and % tl - gtv volume receiving above absolute doses in 5 gy eqd2lung increments ( v570gyeqd2 )  . 
example functional lung contours are shown that correspond to thresholds of > 25% of maximum perfusion intensity within total lung minus gtv ( ptl - gtv25% , dark red ) , > 50% of maximum perfusion ( ptl - gtv50% , orange ) , and > 75% of maximum perfusion ( ptl - gtv75% , yellow )  . 
dosimetric parameters such as mean perfused lung dose were evaluated within threshold perfused lung volumes . gtv gross tumor volume statistical analysis receiver operating characteristic ( roc ) curves tested the prediction accuracy of mean lung dose ( mld ) , mean perfused lung dose ( pmld595% ) , anatomic dosevolume parameters ( v570gyeqd2 ) , and doseperfused volume parameters ( pv570gyeqd2 ) for association with grade 2 or higher ( g2 + ) pneumonitis status . 
parameters were considered statistically signicant if the two - tailed asymptotic p - value for the area under the curve ( auc , null hypothesis auc = 0.5 ) was less than 0.01 , which took into account multiple testing adjustment with false discovery rate ( fdr ) of 5% . 
when testing a total of 48 free parameters in this investigation , the threshold of signicance equates to the fdr - corrected pvalue of 0.03 using the benjaminihochberg method [ 19 ]  . while not as conservative an adjustment as bonferronis correction of familywise error rate , this threshold of signicance balanced mitigation of false positive discoveries while maintaining statistical power in this small cohort to identify candidate predictors of pneumonitis . 
cutoff values of mean lung dose ( mld ) and perfused mean lung dose ( pmld ) were estimated that balanced sensitivity and specicity for classifying patients with / without g2 + pneumonitis . 
bivariate thresholds were empirically estimated through observation of pairs of candidate predictors , but multivariate statistical testing was not performed due to small sample size . our patient cohort was composed of a heterogeneous population . 
2 depicts radiation treatment plans from two patients with similar clinical characteristics but differences in mean dose to anatomic lung versus mean dose to perfused lung . both patients presented with upper lobe primary nsclc and were treated with conventionally fractionated concomitant radiochemotherapy . 
this example highlights that solely using anatomic lung dose to predict risk of radiation pneumonitis may not be applicable for all patients , particularly those with spatial heterogeneity in lung function . strahlenther onkol ( 2017 ) 193 : 410418 fig . 
2 planned dose ( rainbow color scale ) overlaid on fusion of maa perfusion spect ( hot metal color scale ) and planning ct for patients with similar clinical characteristics ( upper lobe tumors treated with concomitant radiochemotherapy ) , one of whom presented with radiation pneumonitis ( a ) and the other who did not ( b ) after therapy . 
patient dosevolume histograms and dosefunction histograms are color - coded according to those who presented with ( black lines ) or without ( gray lines ) grade 2 or higher pneumonitis after radiation therapy neither dosevolume histograms ( dvh ) nor dosefunction histograms ( dfh ) [ 6 , 20 ] could stratify patients for pneumonitis incidence risk . 
4 receiver operator characteristic ( roc ) analysis showing areas under curve ( auc ) as a function of dosevolume parameters ( a ) , doseperfused volume parameters ( b ) , and mean perfused lung dose parameters ( c )  . 
red markers ( auc > 0.93 , p < 0.01 ) signify candidate predictors of grade 2 or higher pneumonitis , including v15gyeqd2 , mean lung dose ( mld ) , and mean perfused lung dose above 70% max perfusion threshold ( pmld70% )  . 
5 bivariate scatter plot as a function of patients who presented with ( black markers ) or without ( gray markers ) grade 2 or higher pneumonitis after radiation therapy . 
testing within a larger patient population may conrm certain parameter combinations as independent variables for multivariate prediction of pneumonitis . discussion in current practice , radiation treatment planning does not take into account the regional variance in pulmonary function and its impact on relative risk of radiation - induced pulmonary toxicity . 
we developed a framework for investigating the association of baseline perfused lung dosimetry with incidence of symptomatic pneumonitis and applied it as a proof - of - principle to a patient cohort who underwent modern spect / ct image acquisition , reconstruction , and coregistration while in radiation treatment position . 
the preliminary application of the framework reveals that a combination of anatomic and functional lung dose parameters may be able to better predict patients who go on to present grade 2 radiation pneumonitis than either group of variables on their own . studies have looked at changes in pulmonary function tests following denitive radiotherapy for nsclc . 
prior groups utilizing spect imaging for lung perfusion have not been able to dene functional lung dosimetric parameters that can replace anatomic lung dosimetric parameter in predicting radiation pneumonitis . however , more recently , multiple groups have reported improved radiation pneumonitis correlation by utilizing baseline spect / ct lung perfusion imaging to dene additional dosimetric parameters for treatment planning . 
 [ 16 ] examined standard and functional dvh for patients with nsclc treated with curative intent and noted functional dosimetric parameters had a stronger association of radiation pneumonitis than standard metrics . 
 [ 23 ] echoes similar results , showing high correlation of perfusion metrics with radiation - induced lung injury and spatial differences between anatomic lung v60gy and perfused lung v60gy . 
recent data also showed that patients who had perfused - mld > 16 gy , perfused v20gy > 30% , and perfused v30gy > 23% went on to develop radiation pneumonitis [ 16 ]  . 
our data yielded similar mean dose to perfused lung as a predictor of pneumonitis , after accounting for differences in fractionation , regional lung dose variation , and statistical testing with multiple sampling correction to protect against false positive ndings . 
functional dosimetric parameters can complement anatomic parameters for improved correlation of pneumonitis . in addition to investigations on baseline spect / ct imaging prior to radiation therapy [ 16 , 22 , 23 ] , other studies have also correlated changes between preand posttreatment functional lung imaging and its relationship to radiation pneumonitis . 
 [ 24 ] noted a higher risk of symptomatic pneumonitis in those patients who had a reduction in perfusion at 3 months postradiotherapy compared to patients who did not , with a relative risk estimate of 3.6. 
although both perfusion and ventilation changes can be seen after treatment , ventilation metrics may not be as sensitive to radiation as perfusion metrics , since physiologically , the lungs can vasoconstrict to reduce blood ow to unventilated areas , but it is more difcult to constrict airways to reduce ventilation to unperfused areas [ 25 ]  . 
therefore , radiation - induced changes in ventilation will likely cause rapid changes in perfusion , but not vice versa . our methodological framework only utilized baseline perfusion imaging , which can determine pneumonitis risk a priori and inform on additional radiation planning lung constraints . 
 [ 24 ] , who found a greater risk of pneumonitis in patients who saw a greater reduction in perfusion . if pretreatment scans can be used to predict future development of pneumonitis , then treatment can potentially be adjusted to minimize risk of pulmonary toxicity . 
from this preliminary proof - of - principle investigation , a testable hypothesis would be that patients who have high anatomic mean lung dose can be risk stratied for the development of radiation pneumonitis by perfused mean lung dose . 
validation of perfused lung dosimetric predictors in a future investigation would motivate the generation of functional lung avoidance treatment plans that are personalized to mitigated individual patient risk of pulmonary toxicity . 
the preliminary results in this limited cohort conrm other studies on the potential utility regarding functional parameters predictive for pneumonitis . we have a heterogeneous patient population with respect to treatment modality and individual tumor characteristics . some of our patients had prior radiation or thoracic surgery , albeit at long time intervals prior to treatment planning spect / ct imaging . 
due to our small patient numbers , we were not able to perform a subgroup analysis on the effect of prior therapy , but our baseline imaging studies and tests captured the pulmonary function status prior to the current course of radiation treatment . 
despite these variations in patient characteristics , the observed trends support a testable hypothesis that functional and anatomic imaging parameters confer a substantial effect size for predicting radiationinduced pneumonitis . the validity of the edq2lung voxelwise conversions for sbrt and moderately hypofractionated pbt is not precisely known , despite our efforts to control for treatment regimen and spatially variant lung fractional dose . 
in addition to dose , there are other known risk factors for pneumonitis , such as concurrent chemotherapy , prior radiotherapy , stage , tumor size , patient age , and comorbidities , which need to be considered . 
this initial application of our framework must be validated in a larger patient cohort . conclusions this investigation demonstrated that construction of a comprehensive methodological framework can reveal differences between anatomic and perfused lung dosimetric parameters . 
the addition of perfused lung parameters may help to improve the correlation to clinical radiation pneu418 strahlenther onkol ( 2017 ) 193 : 410418 monitis , especially for patient plans with high anatomic mean lung dose . 
evaluation of anatomic and perfused lung dose parameters can further personalize radiation therapy planning to minimize risk of treatment - related toxicity . funding this work was nancially supported by nih / nci r01ca204301 , radiological society of north america rsch1405 , and the fred hutchinson cancer center support grant for protocolspecic research support , p30ca015704 . 
technical requirements for heating devices hana dobcek trefn1 johannes crezee2 manfred schmidt3 dietmar marder4 ulf lamprecht5 michael ehmann6 jacek nadobny7 josen hartmann3 nicolleta lomax4 sultan abdel - rahman8 sergio curto9 akke bakker2 mark d . 
this article is available at springerlink with open access . abstract quality assurance ( qa ) guidelines are essential to provide uniform execution of clinical trials with uniform quality hyperthermia treatments . 
this document outlines the requirements for appropriate qa of all current supercial heating equipment including electromagnetic ( radiative and capacitive ) , ultrasound , and infrared heating techniques . detailed instructions are provided how to characterize and document the performance of these hyperthermia applicators in order to apply reproducible hyperthermia treatments of uniform high quality . 
both sets of guidelines were developed by the european society for hyperthermic oncology ( esho ) ( cid : 2 ) hana dobcek trefn hanatre@chalmers.se signals and systems , chalmers university of technology , gothenburg , sweden 2 radiotherapy , amc , amsterdam , the netherlands 3 radiotherapy clinics , universitatsklinikum erlangen , erlangen , germany 4 kantonsspital aarau , aarau , switzerland 5 radiation oncology , university hospital tuebingen , tuebingen , germany technical committee with participation of senior society of thermal medicine ( stm ) members and members of the atzelsberg circle . keywords quality assurance hyperthermia , supercial applicator water bolus phantoms heating criteria leitlinien zur qualittssicherung der lokalen hyperthermie in klinischen studien ii . 
technische anforderungen an heizgerte zusammenfassung um eine einheitliche durchfhrung klinischer studien in der hyperthermie zu gewhrleisten , sind leitlinien zur qualittssicherung ( qa ) unerlsslich . dieses dokument enthlt die anforderungen zur qa fr alle aktuellen therapiegerte zur lokalen hyperthermie , inklusive elektromagnetischer systeme ( radiativ und kapazitiv ) , ultraschallund infrarottechnik . 
e. , this document , provides quality assurance requirements for heating equipment as well as detailed instructions how to characterize and document the performance of hyperthermia devices in order to apply reproducible , uniform , and high quality hyperthermia treatments . 
these characteristics help to establish the maximum size and depth of tumors that can be heated adequately . implementation of these qa guidelines should facilitate correct assessment of whether a tumor can or cannot be heated with the specic heating device ( s ) available in a hyperthermia center and , thus , enable a decision as to whether a patient is or is not eligible to participate in a clinical study . many different systems are used to apply supercial hyperthermia , either built commercially or in academic research laboratories . 
each system has unique characteristics and advantages ( as summarized in appendix a ) , which may result in a large heterogeneity in the quality of applied hyperthermia treatments between various hyperthermia centers . to assure proper performance of a supercial hyperthermia applicator , the spatial thermal pattern should be evaluated under well - controlled conditions prior to the rst clinical use of the applicator and at regular intervals as part of a clinical qa progradue to time constraints in the clinical workow and the large diversity of supercial heating systems , which include electromagnetic ( em ) , radiofrequency ( rf ) , ultrasound ( us ) , and infrared ( ir ) technologies , these new qa guidelines require characterization of the heating performance of hyperthermia equipment with temperature ( rise ) simulations and measurements in homogeneous muscle tissue - equivalent phantoms . 
this is a more pragmatic approach than that used in previous guidelines / recommendations , which were based on power deposition patterns quantied in w / kg and described as specic absorption rate ( sar ) distributions . 
beide teile der leitlinie wurden vom technischen komitee der european society for hyperthermic oncology ( esho ) in zusammenarbeit mit leitenden mitgliedern der society of thermal medicine ( stm ) und mitgliedern des atzelsberger kreises erarbeitet . schlsselwrter qualittssicherung hyperthermie , lokale applikator wasserbolus phantome heizkriterien introduction these quality assurance ( qa ) guidelines for the application of supercial hyperthermia clinical trials were developed at the request of the atzelsberg circle for clinical hyperthermia of the interdisciplinary working group of hyperthermia interdisziplinre arbeitsgruppe hyperthermie ( iah ) [ 1 ] of the german cancer society ( deutsche krebsgesellschaft ) to the european society for hyperthermic oncology ( esho ) [ 2 ]  . 
esho delegated this task to the esho technical committee ( tc ) , who formulated the guidelines with participation of experienced members of the society for thermal medicine ( stm ) [ 3 ]  . 
in addition , the manufacturers providing equipment for supercial hyperthermia were invited to provide their feedback on the qa guidelines during public sessions at the 2014 and 2015 annual meetings of esho or alternatively by personal communication . the qa guidelines seek to establish a minimum level of treatment quality in hyperthermia treatments delivered in all multi - institutional studies initiated by the atzelsberg circle or under the auspices of the esho . 
the goal of this effort is to establish qa guidelines for the application of supercial hyperthermia , similar to the qa guidelines for administration of deep hyperthermia dened earlier [ 4 , 5 ] and as a long awaited follow up to previous supercial hyperthermia qa guidelines provided by the radiation therapy oncology group and esho [ 68 ]  . these qa guidelines for the application of supercial hyperthermia clinical trials consists of two parts : strahlenther onkol ( 2017 ) 193 : 351366 denitions and characteristic features of a supercial hyperthermia system applicators supercial applicators , used today , consist of external em antennas or waveguides , external em capacitive electrodes ( capacitive rf systems ) , external us transducers ( us systems ) , and external noncontacting ir heating systems . in general , these devices deposit energy to heat a limited volume of tissue close to the heating device . 
a brief summary of the operating principles of various systems for heating supercial tissue is given in part i of the qa guidelines [ 9 ] , while more detailed equipment options are given in appendix a . 
further information can be found in reviews [ 1114 ]  . supercial hyperthermia applicator terminology single applicator : a single radiating aperture connected to a power amplier having independent control of output power from 0100% . 
the applicator can be an em radiator [ 1624 ] , us transducer [ 14 ] , ir lamp [ 15 ] , or the active electrode of a capacitive system [ 52 , 53 ]  . multi - element applicator array : to produce effective heating of large area tumors , several single applicators can be combined into larger arrays with separate power control of each element to enable 2d power steering [ 25 , 29 , 34 , 36 ]  . 
this provides better coupling of em / us eld to tissue without distorting the radiation pattern ; at the same time it puts greater demands on reproducible alignment of the applicator relative to the tumor margan adequate bolus design is required since the dimensions and temperature of the water bolus signicantly affect the applicator power deposition ( sar ) pattern , thermal effective eld size ( tefs ) , and thermal depth proles . 
a bubble trap , impurity lter and a ow indicator is recommended to be included in the circulation systethe input and output ow connectors of the water bolus are located on opposite sides . 
large applicator arrays may require dual - inputdual - output ports in order to main1 this range includes room temperature as required for qa , in addition to the 3045 c range typical for clinical treatments . 354 strahlenther onkol ( 2017 ) 193 : 351366 fig . 
calculated normalized temperature rise ( tr ) distribution at 1 cm depth in a two - layered phantom , with fat layer thickness of 10 mm overlying the muscle phantoheating time t = 6 min , p = 175 w . 
the water bolus can be lled with low density semirigid porous foam , plastic spacers , or thin rubber pins to avoid collapse of the bolus while pressed against the skin surface . specic features of the water bolus some manufacturers provide a water bolus that is an integral part of the applicator with a rigid plastic frame that mounts to the applicator aperture [ 19 , 22 , 2729 , 33 , 35 ]  . while this makes bolus position more reproducible relative to the applicator , the consequence of a xed - frame set - up is often a convex bolus shape with reduced contact area between water bolus and skin that is smaller than the radiating aperture . 
this may cause a localized e - eld discontinuity and associated high tissue temperature rise near the sharp transition in em coupling at the water bolusair interface if that occurs under a high eld region of the radiating aperture [ 41 ]  . 
ultrasound systems require deionized and degassed water , with the degree of degassing required inversely proportional to frequency ; this is most critical for systems operating at 0.51.5 mhz where a dissolved oxygen content below 0.1 ppm is required to avoid lossy propagation and outgassing of air from the coupling bolus during ultrasound transmission . 
in em capacitive heating systems , saline ( 0.11.5% ) is generally used [ 43 , 44 ] to improve impedance matching between electrodes and muscle tissue , as well as to spread rf currents over the contact area and thereby reduce skin burns at the edge of the electrode . guidelines for proper design and evaluation of the water bolus size : em - radiative applicators : the water bolus should extend at least beyond the perimeter of the applicator aperture and ideally at least 25 cm outside the perimeter . 
phantom experiments of the applicator with various bolus sizes are recommended . em - capacitive systems : the tefs is highly dependent on the size of the contact area of the coupling bolus and tissue . 
especially at the edge of the bolus , care must be taken to provide smooth transitions at the bolusskin contact at the peripheral rim of the water bolus [ 4244 ]  . thickness : for em - radiative applicators the optimal water bolus thickness depends on type of applicator , its dimensions as well as target depth [ 41 ] and the thickness should not exceed critical values to avoid oscillation modes in the bolus layer [ 45 , 46 ]  . 
these modes occur for larger sized applicators at frequencies above 100 mhz [ 47 ] and also for suboptimal contact between bolus and applicator [ 20 ]  . em - capacitive systems utilize a frequency below 100 mhz . they require a minimum water bolus thickness depending on applicator size to minimize the effect of concentrated current at the edge of the metal electrodes . their performance is rather insensitive to a variation in water bolus thickness provided the minimum thickness requirement is satised [ 43 , 44 ]  . for ultrasound applicators with properly degassed water bolus , thickness has negligible effect on energy propagation ( losses ) since the attenuation in water is very low , but may affect beam pattern shape and position of the strahlenther onkol ( 2017 ) 193 : 351366 fig . 
simulated temperature increase ( blue left axis ) and specic absorption rate ( sar ; red right axis ) as a function of depth in the center of two - layered phantom , with fat layer ( blue ) thickness of 10 mheating time t = 6 min with p = 175 w and bolus surface temperature identical to the initial phantom temperature . 
observe that the effective heat penetration is essentially at nearly the same depth for both denitions focal zone depending on the device and conguration . phantom experiments or direct sar or intensity measurements must be designed specic for each applicator with various bolus thicknesses in the clinically relevant range . variations in bolus thickness ( 50% ) are inevitable in clinical conditions due to the irregular skin surface contour . 
in order to assure that users know how to respond effectively to patient complaints and to unexpected temperature heterogeneity , the impact of these variations on eld homogeneity and effective eld size should be assessed experimentally or by simulations . good contact between bolus and phantom : wet gauze can be used to improve heat transfer at the bolusskin interface for em devices [ 41 ] but proper care must be taken to ensure that no air gaps occur in the interface [ 48 ]  . 
air bubbles and air gaps need to be removed with acoustic gel or water coupling for ultrasound devices . the water temperature has a profound impact on the effective penetration depth : the use of cold water will increase the effective penetration depth of the maximum temperature and the therapeutic extent up to 12 cm [ 41 , 49 ]  . 
3. for consistency , the measurements to determine tefs must be made within 15 s after the end of heating to minimize thermal conduction smearing of the sar pattern within the phantoif a multi - element applicator array is used , elements must be arranged such that a continuous region of tr > 50% of the maximum tr exists . 
this assessment should be made at a depth of 1 cin order to determine tepd , analogous measurements at other depths ( > 1 cm ) are needed until tepd is found . 356 strahlenther onkol ( 2017 ) 193 : 351366 surement procedure described above if a short measurement time of 1 min or less is used to prevent blurring of the sar pattern by heat conduction . 
g. , for comparisons with numerical calculations : the effective eld size ( efs ) is dened by the area within the 50% of maximum sar contour in the 1 cm deep plane under the aperture . the effective penetration depth ( epd ) is dened by the depth where the sar falls to 50% of the maximum sar at 1 cm depth . 
note that the maximum sar may not be in the plane through the main central axes of the applicator . generic phantoms two models are necessary to characterize heating of two typical disease conditions : ( 1 ) supercial chestwall disease that extends from the tissue surface to moderate depth ( generally < 15 mm ) , and ( 1 ) tumors at moderate depth underlying normal skin and fat . for reliable phantom measurements the general rule is that the phantom size should extend beyond the applicator by at least 10 cm in all directions . 
3 calculated normalized specic absorption rate ( sar ) distribution of a 10 10 cm lucite cone applicator ( lca ) at 1 cm depth in a homogeneous muscle tissue phantothe color scale from blue to dark red represents a 10% sar increase for every color transition . 
adapted from [ 66 ] note that besides characterizing the temperature distribution , the efciency of power transfer within the complete heating system ( cables , applicator , and bolus ) should be measured . 
this information can be used as a reference value to compare the clinical applied power levels between hyperthermia centers and assess whether realistic powers are applied to assure the required increase in tumor temperature . 
however , it is also important that the user is aware of how much power is lost in cables , applicator , and bolus . efciency measurements can be accomplished either with a calorimetric2 method or the total absorbed power may be calculated from rate of tr measurements . note that tr estimation alone is not sufcient for a complete characterization of the systenumerical modeling and / or experimental assessment in terms of other parameters like sar are recommended to achieve a more fundamental characterization of the system and to assist the user with determining the relevant parameters for the actual clinical setup . 
sar can be determined with the tr mea2 the efciency of the supercial hyperthermia system is obtained by calculating the ratio of the em power absorbed in the phantom to the net power input to the applicator ( forward minus reected power measured at the output of the amplier minus cable losses between amplier and applicator )  . 
the em power absorbed in the phantom is measured using the calorimetric method : a well - insulated and well - stirred liquid muscle - tissue equivalent phantom is heated by the applicator for 10 min with a high em - power input . 
the homogeneous temperature increase of the liquid muscle - tissue equivalent phantom is measured and total absorbed energy calculated from pa = ( cid : 2 ) cp ( cid : 2 ) v ( cid : 2 ) dt / dt [ j / s ] , in which pa is absorbed power , is the density , and cp is the specic heat capacity of the liquid muscle - tissue equivalent phantom material , v is the volume , dt the temperature increase , dt is the duration of heating . strahlenther onkol ( 2017 ) 193 : 351366 for all temperature and power deposition measurements , a proper phantom must be used with the correct electrical , optical , or ultrasound properties and correct thermal properties . 
tissue equivalence of the phantom material can be obtained by using freshly made materials following a validated recipe or demonstrating equivalent properties via measurements . phantom recipes for electromagnetic equivalent phantoms at commonly used frequencies are specied in appendix b ; a limited set of suggestions of emphantom mixtures for less frequently used frequencies , ultrasound phantoms , and infrared phantoms are also provided . the thermal distribution of the applicator should be characterized under standardized operating conditions and at all frequencies in clinical use . 
the two generic reference phantom set - ups described in section generic phantoms should be used for this characterization . all measurements should be carried out at room temperature , i . 
a bolus of appropriate dimension should be placed on top of the phantom with liquid circulating at the same room temperature as the rest of phantothe distribution of temperature rise must be measured in three orthogonal planes crossing the center of applicator as shown in fig . 
4. the horizontal plane at 1 cm depth must always be measured by an ir camera using a horizontally split phantom with a removable top layer of 1 cm which is removed for the ir temperature measurement . the vertical planes ( xz , yz ) can be measured with one of three alternative methods as shown in fig . 
a 1 cm thick fat phantom layer split down the middle should be added to the top of the muscle phantom to model tumor underlying normal fat . 358 strahlenther onkol ( 2017 ) 193 : 351366 fig . 
5 illustration of three alternative options to obtain thermal prole with depth : a thermal camera view of vertical plane containing peak temperature rise ( tr ) ; b reconstruction of vertical distribution from thermal camera views of multiple horizontal planes ; and c multiple measurements along a single axis depth probe alternative method ( c ) : multiple stationary temperature probes must be used to obtain a minimum resolution of 1 cthe absolute tr at each depth measured immediately after switching on em , us , or ir power must be used to plot the temperature depth prole as a means to determine tepd . with any of the methods , if the vertical plane measurements show a deviation of the temperature maximum from the central plane , an additional measurement must be performed through the vertical plane along the cross - section of the applicator that includes the true maximum tr . 
in addition , at least one temperature sensor must be placed at 1 cm depth in the center of the central plane of the applicator as a reference point regardless of the test set - up applied . the absolute tr measured at this location is indicative of the efciency of the applicator to deposit a high sar at this position and combined with applicator input power allows simple quantitative comparison between institutes of the temperature increase obtained in the xed 6 min heating interval . 
the camera should be placed at a proper height to cover the entire phantom surface and test images should be recorded with rulers in the eld of view to ensure correct rendition of dimensions . disclaimer this publication is based on literature and other sources of information judged to be reliable by the authors representing the esho - tc . 
stauffer declare that they have no competing interests . ethical standards this article does not contain any studies with human participants or animals performed by any of the authors . open access this article is distributed under the terms of the creative commons attribution 4.0 international license ( creativecommons.org / licenses / by / 4.0 / ) , which permits unrestricted use , distribution , and reproduction in any medium , provided you give appropriate credit to the original author ( s ) and the source , provide a link to the creative commons license , and indicate if changes were made . strahlenther onkol ( 2017 ) 193 : 351366 appendix a microstrip applicators detailed description of applicator types with their advantages and limitations em radiative system for purposes of the present guidelines , radiative applicator options may be divided into two main types : waveguide applicators and microstrip applicators . waveguide applicators waveguide applicators are made from a section of waveguide transmission line open at one end with an aperture of at least a half wavelength in the direction of the e - eld . the excitation is provided by a short extension of the coaxial feedline center conductor or a loop antenna inside the waveguide structure . 
in order to reduce the physical dimensions of the aperture , the applicator may be lled with a material having a dielectric constant higher than air , such as teon , ceramic , high dielectric powder , or distilled water [ 12 ]  . 
clinically utilized examples are contact exible microstrip applicator ( cfma ) [ 1922 , 26 , 36 ] , archimedean spiral applicator [ 2729 ] , dual concentric conductor ( dcc ) [ 3033 ] , and current sheet applicator ( csa ) [ 25 , 34 ]  . 
in order to heat supercial locations , an electrode matching the lesion size is placed on the target lesion while a larger electrode that spreads out the current density over a larger area is situated on the opposite side of the body . 
the electrodes are connected to an rf power source ( 827 mhz ) and the resulting power deposition pattern is mainly determined by the size and location of the smaller electrode . descriptions of the use of em capacitive heating are given in [ 54 , 55 ]  . 
the traveling pressure wave reects from air so is generally coupled to tissue with temperature - controlled degassed water and ultrasound gel to minimize air in the path [ 57 , 58 ]  . 
tumor size volumes may be heated by combining multiple transducers in a nonfocused planar array for supercial heating [ 59 , 60 ] , or a phased array that creates an intense focal hot spot or shaped distribution that can be electronically or mechanically scanned at depth to heat a tumor [ 6165 ]  . 
due to heat dissipation by conduction , convection and mie - scattering ( forward scattering ) the primary absorbed radiation energy is deposited within a larger tissue volume than the original column of absorption . 
in order to minimize thermal exposure of the skin surface , a water lter system must be integrated with the ir radiation source ( wira ) [ 15 ]  . 
use of other phantom recipes is permitted if dielectric , acoustic propagation , or optical properties of the phantom are demonstrated to be equivalent to the muscle / fat tissues at the frequency of the device under test . 
the relevant optical properties , the absorption coefcient and reduced scattering coefcients are not stated in the table , due to their extreme variability with frequency . data on the optimal ir frequency band for hyperthermia purposes are not available presently and therefore ir users are referred to comprehensive reviews [ 75 , 76 ]  . the list of suggested phantom recipes will be updated on the esho webpage [ 2 ]  . em phantoms muscle equivalent phantoms among numerous recipes for muscle tissue - equivalent phantoms , two alternative formulas are recommended due to their appropriate electrical and mechanical properties , homogeneity , and simplicity of preparation . 
hence , it is recommended to use 3.3 g nacl per liter phantom to achieve an estimated value of 0.6 s / m btx 150 & tx 151 ( oil center research , lafayette , la , usa ) ; * in the original work [ 70 ] , highly toxic nan3 was used as preservative . 
in such a case , an equivalent amount of water should be used . gested by nilsson [ 77 ] includes nacl to adjust conductivity and sugar to provide appropriate permittivity . 
add the agar slowly while stirring and heat the mixture to the boiling point ( 8090 c for about 5 min )  . 3 tx 150 & tx 151 ( oil center research international , l.l.c. , lafayette , la 70503 )  . * in original work [ 70 ] , highly toxic nan3 was used as preservative . 
when the solution has a temperature of 7080 c , add the mixture of tx - 150 ( or tx - 151 ) polyethylene powder while stirring continuously to ensure homogeneity . 
be careful to avoid generation of air bubbles due to overvigorous stirring , as this will reduce phantom homogeneity . during the process of adding the mixture , keep the temperature of the solution between 7080 c . 
if the phantom gets too stiff in the mixing container , when phantom transferred to the mold and pushed to ll the corners , large air pockets may become trapped inside the phantom producing heterogeneous phantom properties . us phantoms muscle phantom fat equivalent phantoms an optimal phantom recipe representing properties of fat tissue is currently not available . 
the material consisting of laminac 4110 ( a polyester resin ) , acetylene black , and aluminum powder offers great stability and long shelf life ; nevertheless , it requires relatively complex preparation . 
it provides homogeneous phantom with appropriate electrical and mechanical properties ; however , the life is relatively short due to ( easy ) water evaporation the phantom should be covered by thin plastic foil and stored in a closed environment . 
yet another option is use of pig fat , which is easily accessible and has dielectric properties comparable to human fat . the recommended muscle or soft tissue mimicking phantom for acoustic and thermal testing of ultrasound thermal therapy devices was developed recently by investigators at the us food and drug administration [ 83 ]  . 
the recipe utilizes a gellan gum as gelling agent with melting temperature above 100 c , calcium chloride dehydrate to enhance the gel strength and potassium sorbate which acts as preservative . 
when using low frequency ultrasound sources , penetration through the phantom can be high so the thickness of phantom model needs to be sufcient to fully absorb the energy prior to reections off the bottom of phantoalternatively , an absorber such as a soft 2030 durometer rubber can be added as a back layer to minimize reections . fat phantom a fat - mimicking phantom in which oil droplets are dispersed in a water - based gelatin [ 85 ] is recommended . 
two alternative compositions can be recommended : ( 1 ) the agar phantom with intralipid acting as a scattering medium , and india ink acting as an absorbing medium [ 88 ]  . 
 ( 2 ) a silicon - based phantom [ 89 ] whose absorption and scattering properties are adjusted by adding matrix cosmetic powder and al2o3 particles to the silicone base . this phantom exhibits good macroscopic homogeneity can be cast into layers or arbitrary shapes with long shelf life . routine qa for supercial microwave hyperthermia system during routine use , a deterioration of applicator performance could occur . 
this article is available at springerlink with open access . abstract purpose to develop a fully automated procedure for multicriterial volumetric modulated arc therapy ( vmat ) treatment planning ( autovmat ) for stage iii / iv non - small cell lung cancer ( nsclc ) patients treated with curative intent . materials and methods after conguring the developed autovmat system for nsclc , autovmat plans were compared with manually generated clinically delivered intensity - modulated radiotherapy ( imrt ) plans for 41 patients . autovmat plans were also compared to manually generated vmat plans in the absence of time pressure . 
for 16 patients with reduced planning target volume ( ptv ) dose prescription in the clinical imrt plan ( to avoid violation of organs at risk tolerances ) , the potential for dose escalation with autovmat was explored . results two physicians evaluated 35 / 41 autovmat plans ( 85% ) as clinically acceptable . 
for 6 / 16 patients , autovmat allowed tumor dose escalation of 510 gy . conclusion clinically deliverable , high - quality autovmat plans can be generated fully automatically for the vast majority of advanced - stage nsclc patients . 
for a subset of patients , autovmat allowed for tumor dose escalation . keywords radiotherapy , intensity - modulated volumetric - modulated arc therapy computer - assisted radiotherapy planning non - small cell lung carcinoma organs at risk vollautomatische vmat - behandlungsplanung fr patienten mit fortgeschrittenem nsclc zusammenfassung zielsetzung entwicklung einer vollautomatisierten , auf multiplen kriterien basierenden volumenmodulierten arctherapie - ( vmat - ) behandlungsplanung ( autovmat ) fr kurativ behandelte patienten mit nicht - kleinzelligem bronchialkarzinom ( nsclc ) im stadium iii / iv . material und methoden nach konguration unseres autovmat - systems fr nsclc wurde fr 41 patienten der autovmat - plan mit dem manuell erzeugten , klinisch applizierten intensittsmodulierten strahlentherapieplan ( imrt ) verglichen . 
autovmat - plne wurden ferner mit manuellen und ohne zeitdruck erstellten vmat - plnen verglichen . fr 16 patienten mit reduzierter dosisverordnung des planungszielvolumens ( ptv ) im klinischen imrt - plan ( zur vermeidung einer verletzung von toleranzdosen fr risistrahlenther onkol ( 2017 ) 193 : 402409 koorgane ) wurde das potenzial fr eine dosiseskalation mit autovmat untersucht . ergebnisse zwei rzte bewerteten 35 von 41 autovmatplnen ( 85 % ) als klinisch akzeptabel . 
verglichen mit den manuell erzeugten imrt - plnen zeigten autovmat - plne eine statistisch signikant bessere ptv - abdeckung ( v95% erhht um 1 , 1 % 1 , 1 % ) , eine hhere dosiskonformitt ( r50 verringert um 12 , 2 % 12 , 7 % ) und eine geringere durchschnittliche dosis in lunge , herz und oesophagus ( verringert um je 0 , 9 gy 1 , 0 gy , 1 , 5 gy 1 , 8 gy , 3 , 6 gy 2 , 8 gy ; alle p < 0 , 001 )  . 
um die restlichen 6 autovmatplne aus klinischer sicht akzeptabel zu machen , bentigte ein dosimetrist zur feinabstimmung jeweils weniger als 10 mautovmat - plne wurden verglichen zu manuell optimierten vmat - plnen als gleichwertig oder sogar besser erachtet . 
fr 6 von 16 patienten ermglichte autovmat eine dosiseskalation im tumor um 510 gy . schlussfolgerung fr die groe mehrheit von patienten mit fortgeschrittenem nsclc konnte ein klinisch applizierbarer , hochqualitativer autovmat - plan vollautomatisch erstellt werden . 
fr eine subgruppe ermglichte autovmat eine dosiseskalation im tumor . schlsselwrter intensittsmodulierte strahlentherapie volumenmodulierte arc therapie vollautomatisierte strahlentherapieplanung nicht - kleinzelliges bronchialkarzinom risikoorgane in recent years , the use of volumetric modulated arc therapy ( vmat ) for treatment of locally advanced non - small cell lung cancer ( nsclc ) patients has grown . 
the shorter treatment time of vmat allows for increased patient throughput , reduced intrafractional motion , and improved patient comfort [ 1 ]  . imrt and vmat treatment planning with commercial treatment planning systems ( tps ) is an iterative trial - anderror process . 
the procedure is time consuming and the quality of the nal treatment plan may depend highly on the experience and skills of the dosimetrist , the complexity of the case , and the available time . 
in addition , there is no guarantee that the nal treatment plan reects the optimal dose distribution for a specic patient in terms of ptv coverage , doses in organs at risk ( oar ) , and the desired tradeoffs between them . to increase the consistency and quality of treatment plans , and to reduce treatment planning time , there is a growing interest in automated treatment planning [ 216 ]  . different vendors offer so - called knowledge - based automated treatment planning solutions . 
consequently , the multicriterial optimized plans were preferred by the physicians . in the authors department , erasmus - icycle was developed , a system for fully automated multicriterial treatment plan generation . 
the rst set , 404 strahlenther onkol ( 2017 ) 193 : 402409 consisting of 7 patients treated in 2014 , was used to congure the system for automated planning . 
all clinically delivered imrt plans consisted of 59 beams and were generated with the common manual trial - and - error planning approach , using the monaco tps version 5.0 ( elekta ab , stockholm , sweden )  . for segmentation of the targets and oars , the 50% exhale phase of a four - dimensional computed tomography ( 4dct ) scan was used . 
the clinical target volume ( ctv ) was dened by expanding the gross tumor volume ( gtv ) by a margin of 5 mif needed , the ctv was manually edited based on anatomic borders . 
lymph node stations with affected nodesas determined on diagnostic ct or positron - emission tomography ( pet ) scans , endoscopic ultrasound , or ne needle aspiration pathology examinationwere also dened as ctv . 
to dene the planning target volume ( ptv ) , the ctvs of the primary tumor and lymph nodes were expanded by a margin of 1 cm in the lateral and ventraldorsal directions and by a margin of 11.2 cm in the cranialcaudal direction , depending on respiratory tumor motion amplitude . 
the other 8 patients , receiving a prescribed dose of 45 gy or lower , were treated with 3 gy per fraction . planning goals were to cover at least 95% of the ptv and 99% of the ctv with 95% of the prescribed dose , and 99% of the ptv with 90% of the prescribed dose , while sparing oars as much as possible . 
the mean dose in the total lung volume minus gtv had to be kept below 20 gy and the v20gy ( volume receiving 20 gy or more ) below 35% . 
the protocol also prescribed a v5gy < 60% for lungs minus gtv and v45gy < 25% for the esophagus , but these requirements did not determine whether a plan was deemed acceptable or not . 
 [ 3 ] and is briey summarized here . in the rst step , erasmus - icycle is used to automatically generate an equi - angular 23 - beam imrt plan , simulating vmat delivery . 
next , using the achieved constraint and objective values in the erasmus - icycle plan , a patient - specic monaco template is automatically generated , followed by automated plan generation in monaco based on this template , to result in a clinically deliverable vmat plan that closely mimics the initial erasmus - icycle plan . 
the same system is used clinically for automated clinical plan generation for prostate , head and neck , and cervical cancer patients [ 3 , 6 , 14 ]  . plan generation with erasmus - icycle is based on a sitespecic wishlist , with hard planning constraints ( never to be violated ) and prioritized objectives . 
generally , adequate ptv coverage has the highest priority , followed by the most important oar objective . in this study , all erasmus - icycle plans were generated by employing one xed wishlist , with some minor variations to handle differences in dose prescription and fractionation ( see above )  . 
the nal wishlist is shown in table 1 . comparison of autovmat and clinically applied imrt plans for the second group of 41 patients , the manually generated imrt plans were compared with autovmat plans using dosimetric indices and by independent scoring by two physicians . 
for fair comparison , in this part of the investigation , the prescribed tumor dose for the autovmat plans was identical to that used in the corresponding clinical plans . comparison of automatically and manually generated vmat plans at the time of this study , the authors did not yet apply vmat in clinical routine for advanced - stage nsclc patients . 
once the goal of an objective is achieved or when further optimization is no longer possible , the optimizer xes the achieved value of the objective ( with a bit of slack ) as a constraint and continues with the next objective . 
when the spinal cord was close to the target or overlapped it , the objective was applied to the target volume from which the spinal cord expanded by 5 mm was subtracted . the purpose was to locate the acceptable underdosage to the ptv near the spinal cord . 
the dosimetrist had no prior knowledge of the erasmus - icycle plans of these patients . from 45 gy to 55 gy , from 55 gy to 60.5 gy , from 60 gy or 60.5 gy to 66 gy . 
for fair comparison with the clinically applied procedure , intermediate dose escalations were not investigated . dose escalation in clinical routine , when it was not possible to achieve the intended dose prescription of 66 gy without violating at least one of the clinical hard constraints , the number of planned fractions , and consequently the prescribed dose , was reduced following a standard schedule : 1 . 
if plan generation was still unfeasible , further reduction to 55 gy , or , if needed , to 45 , 39 , or 30 gy delivered in 3 gy per fraction . 
for the 16 patients with a prescription dose lower than 66 gy , it was attempted to escalate the dose using autovmat , following the standard schedule steps backwards : statistics plan conformity was quantied using r50 , the ratio between the total volume receiving at least 50% of the prescribed dose and the volume of the ptv . 
dose homogeneity in the ptv was measured using the homogeneity index ( hi ) , dened as hi = ( d2% d98% ) / d50% , where d2% , d98% , and d50% are the doses covering 2 , 98 , and 50% of the ptv , respectively . 
1 differences between clinical intensity - modulated radiotherapy ( imrt ) and automated volumetric modulated arc therapy ( autovmat ) plans for a planning target volume ( ptv ) v95% , ptv d99% , mean lung dose ( mld ) , lungs v5gy , lungs v20gy ; b esophagus mean dose , heart mean dose , conformity index ( r50 ) , and homogeneity index ( hi )  . 
v95% is the ptv volume receiving at least 95% of the prescribed dose , d99% is the minimum dose delivered to 99% of the ptv , v5gy and v20gy are the volumes receiving 5 gy , respectively 20 gy , or more . 
the pronounced predominance of positive bars conrms the overall improvement in plan quality for autovmat plans with respect to the corresponding clinical imrt plans results autovmat and clinically applied imrt plans two physicians judged 35 / 41 of the autovmat plans ( 85% ) as clinically acceptable . 
e. , an average reduction of 20% . unacceptable plans for 6 patients , the physicians deemed the autovmat plan clinically unacceptable due to violation of at least one clinstrahlenther onkol ( 2017 ) 193 : 402409 table 2 mean values and uncertainties , reported as one standard deviation ( 1 sd ) , for the evaluated dose metrics of the clinical imrt plans and the autovmat plans for the 35 study patients with acceptable autovmat plans . 
in 2 patients ptv coverage was not adequate ( v95 < 95% , v90 < 99% ) ; for 4 patients the mld and / or lungs v20gy exceeded clinical constraints . 
in contrast , 34 h were required to generate a vmat plan from scratch . autovmat and manually generated vmat plans a radiation oncologist evaluated all autovmat plans as equivalent or better in quality compared to the manually generated vmat plans . 
2. dose escalation for 6 / 16 patients with a prescription dose less than 66 gy , a clinically acceptable autovmat plan with a higher prescribed tumor dose could be generated . 
in all cases , the physicians preferred the plan with the higher tumor dose . discussion this study developed a method for fully automated vmat treatment planning for nsclc patients based on erasmusicycle . 
based on these results , autovmat has been clinically applied for all advanced - stage nsclc patients treated with curative intent at the authors hospital since march 2016 . in previous studies for prostate , head and neck , and cervical cancer [ 3 , 6 , 14 ] , it was not observed that some of the autovmat plans were unacceptable and of a lesser quality than manually generated imrt plans with the same prescribed dose . 
for nsclc patients , this may result in high - quality erasmus - icycle plans that cannot be accurately mimicked with the advanced monte carlo 408 strahlenther onkol ( 2017 ) 193 : 402409 erasmus - icycle for autovmat planning has a couple of advantages compared to other approaches for automated ( vmat ) planning . 
first , it does not fully rely on a database of prior patients , as published knowledge - based approaches do [ 1 , 4 , 5 , 12 ]  . 
with this procedure , automatically generated plans for previously treated patients have , on average , a higher or at least non - inferior plan quality than the clinical plans [ 3 ] , as also shown in this work . 
the need for a small set of training patients has an additional advantage in case of changes in clinical protocol , which would otherwise require a new large database of high - quality plans . conclusion fully automated vmat treatment planning was implemented for advanced - stage nsclc . 
consequently , autovmat has been applied for nsclc in routine clinical use at the authors hospital since march 2016 . acknowledgements the authors would like to thank kathrin frey for her help with the translation into german . compliance with ethical guidelines conict of interest the department of radiation oncology of erasmus mc cancer institute has research collaborations with elekta ab and accuray . 
we then summarized the tnm 8 staging classication and the relevant literature on the treatment of oligometastatic lung cancer . results in all , 82 patients with metastatic lung cancer were reclassied according to the tnm 8 : 14 had m1b and 58 had m1c disease . 
clinical trials investigating the treatment of patients with varying degrees of metastatic disease are needed and should be based on pet - ct staging . keywords lung cancer staging stage iv metastasis oligometastatic klinische relevanz der m1bund m1cdeskriptoren der neuen tnm - 8 - klassikation des lungenkarzinoms zusammenfassung zielsetzung das tnm - 8 - staging reklassiziert patienten mit einer solitren extrathorakalen metastase als m1b und mit zwei bis mehreren extrathorakalen metastasen als m1c . die studie untersucht die klinische relevanz dieser nderung . methoden patienten mit fortgeschrittenem lungenkarzinom wurden retrospektiv anhand der tnm - 8 - m1bund - m1c - einteilung analysiert . 
klinische studien , welche die behandlung von patienten mit unterschiedlichem ausma der metastatischen erkrankung untersuchen , sind ntig und sollten auf dem pet - ct - staging basieren . schlsselwrter lungenkrebs staging stadium iv metastasierung oligometastatisch introduction stage iv lung cancer is associated with a poor prognosis and is generally treated with one or more lines of palliative systemic treatment . 
although an ideal predictive biomarker for many novel treatments , in particular inhibitors of angiogenesis and immune therapies , has yet to be found , the current approach to lung cancer care is certainly much more tailored to the individual tumour and patient than was previously the case . 
the current tnm 7 system introduced the subdivision of t1 and t2 tumours into t1a / b and t2a / b depending on the exact tumour size , and divided m1 tumours into m1a and m1b depending on the intraor extrathoracic location of metastases . 
this will allow for the development of treatment strategies tailored more specically to each stage of disease . the proposed tnm 8 classication is based on an extensive international tumour database and draws on patient data sets from a range of settings . 
while size and diversity of this data is certainly of benet in the development of an international staging system , the prognostic performance of the staging recommendations in clinical practice will likely also depend on local health care systems and factors such as the availability of ebus , pet - ct and mri . 
following approval from the local ethics committee ( ludwig - maximilians university of munich ) all fully documented patient data sets were included regardless of the type and duration of treatment received . 
we extracted anonymous data sets from the electronic patient record and tumour database including stage at diagnosis , overall survival , histology , use of pet - ct at the time of rst diagnosis and initial treatment . 
based on the number and location of metastases at rst diagnosis , we then restaged patients according to the m descriptors from the proposed tnm 8 staging systewe analysed the overall survival of patients in the proposed m1b and m1c subgroups . 
this study was approved by the ethics committee of the ludwig - maximilians university of munich and performed in accordance with the ethical standards laid down in the 1964 declaration of helsinki and its later amendments . 394 results summary of the proposed tnm 8 staging classication the 7th edition of the tnm classication of lung cancer was published in 2009 by detterbeck and colleagues and put into effect in january 2010 [ 1 ]  . 
the current revision of the staging system was proposed by the international association for the study of lung cancer ( iaslc ) international staging project and published at the end of 2015 and the beginning of 2016 [ 25 ]  . 
the members of the project analysed 94 , 708 lung cancer cases [ 6 ] and dened new subgroups for the t and m descriptors in order to better reect the prognosis of patients in these groups . 
east asian centres ( mainly japan and south korea ) contributed 41 , 705 patients , and 4660 were documented in two large centres in the united states of america . 
in all , approximately 70 , 000 of the data sets in the nal analysis were from patients with nsclc , and approximately 6000 were from patients with small cell lung cancer ( sclc )  . 
metastatic nsclc was somewhat underrepresented in the database , with most patients treated either surgically or with multimodal approaches and only 9.3% of patients having been treated with systemic therapy alone . the t descriptor a total of 13 , 012 clinically staged and 30 , 018 pathologically staged nsclc patient data sets were used to derive the proposed changes to the t descriptor [ 3 ]  . 
most of these strahlenther onkol ( 2017 ) 193 : 392401 patients ( 79% of the clinically stages patients and 79% of the pathologically staged patients ) were submitted to the database by centres in asia ( japan , south korea and the peoples republic of china )  . 
the analysis of this data collection conrmed that 3 cm is an appropriate threshold between t1 and t2 tumours . in the tnm 8 , tumours equal to or smaller than 3 cm in size continue to be dened as t1 . 
however , analysis of the databank showed that 1 cm differences in tumour size are of prognostic relevance in this stage of disease , and so the staging project members suggested further subdividing the t1 group into t1a ( ( cid : 2 ) 1 cm ) , t1b ( > 1 cm ( cid : 2 ) 2 cm ) and t1c ( > 2 cm ( cid : 2 ) 3 cm )  . 
in addition , the group t1a ( mi ) was proposed to represent adenocarcinomas with lepidic growth and a maximal invasion of 5 mm into neighbouring tissue . the staging project members also found that the prognosis of tumours with a size of 57 cm was more similar to that of t3 tumours than t2 tumours , and so they suggested limiting stage t2 to tumours sized 35 cm , which would be subclassied as t2a ( > 3 cm ( cid : 2 ) 4 cm ) and t2b ( > 4 cm ( cid : 2 ) 5 cm ) , and dening t3 as tumours with a size of > 5 to ( cid : 2 ) 7 call tumours larger than 7 cm would then be classied as t4 . 
changes concerning the t descriptor are summarized in table 1 . the n descriptor the proposals for the n descriptor [ 5 ] are based on a total of 38 , 910 cn and 31 , 426 pn data sets , mainly from japan and denmark . 
lymph nodes from japanese patients were reported according to the naruke lymph node map of the japan lung cancer society which varies from the mountaindresler modication of the american thoracic society ( mdats ) and iaslc maps in its n1 vs . 
table adapted from jto [ 1 , 2 ] ( continued ) tumor > 3 cm but ( cid : 2 ) 7 cm or tumor with involving the main bronchus > 2 cm from the carina or visceral pleura or associated with atelectasis or obstructive pneumonitis that extends to the hilar region but does not involve the entire lung tumor > 3 cm but ( cid : 2 ) 5 cm tumor > 5 cm but ( cid : 2 ) 7 cm tumor > 7 cm , directly invades parietal pleural , chest wall ( including superior sulcus tumors ) , diaphragm , phrenic nerve , mediastinal pleura or parietal pericardium ; or tumor in the main bronchus less than 2 cm distal to the carina1 but without involvement of the carina ; or associated atelectasis or obstructive pneumonitis of the entire lung or separate tumor nodule ( s ) in the same lobe tumor of any size that invades the mediastinum , heart , great vessels , trachea , recurrent laryngeal nerve , esophagus , vertebral body or carina , or separate tumor nodule ( s ) in a different ipsilateral lobe tumor > 3 cm but ( cid : 2 ) 5 cm or tumor with any of the following features involves main bronchus regardless of distance from the carina but without involvement of the carina . 
when these elements and clinical judgment dictate that the effusion is not related to the tumor , the effusion should be excluded as a staging descriptor ethis includes involvement of a single distant ( nonregional ) lymph node 396 strahlenther onkol ( 2017 ) 193 : 392401 sication of some lymph nodes . 
the survival curves separated well for the n0 , n1 , n2 and n3 descriptors as dened by the tnm 7 , conrming the prognostic relevance of this classication , especially for patients with t1 and t2 tumours . an analysis based on geographic subgroups showed significant regional differences in survival , with asian patients showing better 5 - year survival than those in europe . 
multiple n1 and n2 lymph node involvement as well as n2 lymph node involvement with sparing of the n1 lymph nodes ( skip )  . they suggest describing these situations as n1a for single n1 disease , n1b for multiple n1 stations , n2a1 for single n2 involvement without affected n1 nodes ( skip ) , n2a2 for single n2 involvement with affected n1 nodes and n2b for multiple n2 involvement . 
the authors also discuss the potential relevance of counting affected lymph nodes rather than affected lymph node regions , and suggest documenting the number of affected lymph nodes ( nn ) for future analyses . the m descriptor in comparison to the data sets used for the t and n descriptors , the dataset available for analysis of the m descriptor [ 4 ] was relatively small , and the nal analysis included 1059 patient data sets submitted primarily by several spanish centres and one large chinese hospital . 
smaller numbers of patients were reported from argentina , australia , brazil , belgium , france , greece and the united states of america . a large cohort of patients documented by the turkish thoracic society and a smaller cohort from the prince charles hospital in australia were excluded from the nal analysis . 
the m descriptor database did not provide detailed information on the type of staging performed to conrm metastatic disease ; in particular the use of pet - ct , mri and cytological or histological conrmation of suspected metastatic sites were not reported . the authors were able to conrm the prognostic relevance of the m1a descriptor as dened in the tnm 7 , and so the denition of m1a disease will remain unchanged in the tnm - 8 classication and will continue to include both contralateral intrapulmonary metastases and pleural or pericardial effusion . 
the authors then assessed the prognostic relevance of the number and distribution of extrathoracic metastases and found patients with a single extrathoracic metastasis to have a favourable prognosis compared with patients with two or more metastases . 
therefore , they proposed dividing the group previously dened as m1b in the tnm 7 into two subgroups in the tnm 8 : m1b for patients with a solitary extrathoracic metastasis and m1c for those with two or more metastases in one or more extrathoracic organs . 
the authors suggest that future databases should precisely document the number and location of metastases , the type of imaging performed and the presence of conrmatory cytology or histology results . changes concerning the t descriptor are summarized in table 1 . proposed m1b and m1c descriptors in a western european tertiary care cohort clinical data sets from 82 patients with advanced lung cancer were included in the evaluation of the proposed m1b and m1c descriptors . 
of the patients reclassied as m1b according to the tnm 8 , 6 had adenocarcinoma , 5 had squamous cell carcinoma , 2 had large cell carcinoma and 1 had small cell carcinoma . 
1 kaplanmaier survival curve comparing patients restaged as tnm 8 m1b with those restaged as m1c tnm 8 m1c patients with 24 extrathoracic metastases ( oligometastatic m1c ) tnm 8 m1c patients with 24 extrathoracic metastases ( oligometastatic m1c ) have a better prognosis than those with 5 or more extrathoracic metastases . 
in patients with m1b disease according to the tnm 8 the location of metastases was distributed as follows : 6 patients had a solitary bone metastasis and 6 had a solitary brain metastasis . 
combined local and systemic treatments in m1b disease an analysis of the treatment received by the patients in this cohort showed that 89% of patients with m1a disease , 67% of patients with m1b disease and additional m1a and 38% of patients with m1b disease without additional m1a were treated with systemic treatment alone . 
within the m1c subgroup , patients with 4 or fewer metastases were often treated with multimodal therapies , whereas those with 5 or more metastases were most often treated with systemic treatments alone . the rst line systemic therapies administered at this centre included pemetrexed in 75% of patients with adenocarcinoma . 
treatments administered are summarized in table 4 . discussion the current analysis summarizes the proposed tnm 8 staging classication and retrospectively classies a cohort of patients treated at a university centre in munich , germany , according to the proposed m1b and m1c classiers from the tnm 8 staging classication system , and investigates the performance of these classiers in this particular population . 
the international patient cohorts used to generate the proposed tnm 8 may differ from cohorts seen at tertiary care centres in western europe both in terms of tumour molecular biology , as rates of driver mutations differ regionally , and in terms of access to diagnostic methods such as pet - ct . 
at the centre described in this analysis , all patients had access to pet - ct at the time of rst diagnosis and about half were actually staged using pet - ct . 
reasons for not using pet - ct in staging included the clear presence of diffuse metastasis using other methods such as ultrasound or ct , and patient wish to be treated palliatively without systemic antitumour therapy . 
testing for egfr mutation and , alk and ros1 translocation was readily available at the university centre , and patients had access to all therapies approved by the european medicines association as well as access to a range of phase iiii clinical trials . 
the munich lung cancer centre is accredited by the german cancer society ( dkg ) , undergoes yearly audits from dkg and is supported by a quality management systethese factors may have positively inuenced the overall survival of some patients in the cohort . 
on the other hand , the university hospital is also a tertiary centre for unstable emergency patients and neurosurgical patients from the region , and several critically ill lung cancer patients with fulminant rst presentations and very limited overall survival were also included in the cohort ( cardiopulmonary resuscitation following pulmonary embolus and neurosurgical treatment of massive haemorrhage in brain metastases )  . 
the proposed tnm 8 m1b and m1c descriptors performed very well in this setting , showing signicantly higher overall survival in the tnm 8 m1b group , which accounted for about one fth of patients examined , than in the tnm 8 m1c group . 
the subgroup of patients with m1b but without additional m1a disease showed a trend to longer overall survival than those patients with a solitary extrathoracic metastasis in addition to intrathoracic m1a tumour spread . 
survival was best in the m1b group staged using pet - ct , which may have been due to the exclusion of more diffusely metastasized patients based on pet - ct results , but could also have been due to a biased selection of patients in a somewhat better general state of health for examination with pet - ct , and exclusion of more fulminant presentations . 
an analysis of the treatment received by patients in the cohort showed that the distinct clinical situations described by the tnm 8 staging classication were treated differently by clinicians at our centre even before the tnm 8 was published . 
most patients with m1a or m1c disease received rst line systemic treatment alone , and there were higher rates of local and combined local / systemic treatments in the group of patients 400 strahlenther onkol ( 2017 ) 193 : 392401 with tnm 8 m1b disease . 
in particular , patients with m1b disease without additional m1a disease were often treated with local therapy alone ( 38% ) and had an average overall survival of almost 2 years . 
although the treatment subgroups in each m category were too small to allow for meaningful statistical analysis , the average overall survival times suggest that local and multimodal treatments result in long overall survival for some patients with m1b disease without m1a and some patients with oligometastatic m1c . in contrast , patients with m1b and additional m1a disease do not appear to benet from initial multimodal or local treatment . in general , the limited number of patients included in this analysis limits the strength and generalisability of the ndings . 
before drawing clinical conclusions from this data conrmatory analyses in independent patient cohorts should be performed . treatment of solitary metastases and oligometastatic nsclc the reorganisation of the m classication is not only of prognostic relevance but also of increasing therapeutic relevance . 
although there is little conclusive evidence to guide treatment of oligometastatic nsclc , multiple cohort studies have demonstrated that nsclc patients with few systemic metastases have a favourable prognosis compared to those with diffusely metastatic disease , in particular if oligometastatic disease is treated aggressively [ 7 ]  . 
treatment included either surgical resection or combined radiochemotherapy of the primary tumour , and irradiation ( or , in the case of some brain metastases , surgical resection ) of all metastases . 
in contrast , the guideline recommends surgical resection for patients with a solitary adrenal metastasis only in the case of synchronous metastasis . the treatment of solitary and oligometastatic nsclc has in part been complicated by inconsistent denitions of oligometastasis between trials . 
asked to decide whether a patient has oligometastatic disease , the opinions of the experts differed signicantly , as did the proposed treatment plans . it is hoped that the proposed tnm 8 staging classication will provide a clear basis for the denition of patients with a single solitary metastasis who may prot from multimodal treatments . 
those whose m1b status is conrmed by pet - ct , and those who do not have additional m1a disease ( pleural / pericardial effusion or intrapulmonary metastases ) appear to have the best prognosis within this group . 
future studies on treatment of such patients should document these factors in order to allow for comparisons between trials . strahlenther onkol ( 2017 ) 193 : 392401 conclusions this analysis conrmed the positive prognostic value of the proposed m1b and m1c descriptors in a western european tertiary care population . 
in addition , the use of pet - ct may dene an oligometastatic subgroup of m1c patients with a better prognosis than those with diffuse metastases , suggesting that a further quantication of tumour burden beyond the proposed m1a , m1b and m1c descriptors may be clinically relevant . 
clinical trials investigating the treatment of patients with varying degrees of metastatic disease are needed and should be based on staging with pet - ct . compliance with ethical guidelines conict of interest a . 
schneider declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
conventional fractionation in adjuvant breast cancer radiotherapy results of a single , institutional , retrospective study volker rudat1 alaa nour1 mohamed hammoud1 salam abou ghaida1 received : 13 november 2016 / accepted : 7 february 2017 / published online : 23 february 2017 the author ( s ) 2017 . 
this article is available at springerlink with open access . abstract background the aim of the study was to identify factors signicantly associated with the occurrence of unintended treatment interruptions in adjuvant breast cancer radiotherapy . patients and methods patients treated with postoperative radiotherapy of the breast or chest wall between march 2014 and august 2016 were evaluated . 
the radiotherapy regimens and techniques applied were either conventional fractionation ( cf ; 28 daily fractions of 1.8 gy or 25 fractions of 2.0 gy ) or hypofractionation ( hf ; 15 daily fractions of 2.67 gy ) with inverse planned intensity - modulated radiotherapy ( imrt ) or three - dimensional planned conformal radiotherapy ( 3dcrt )  . 
noncompliance was dened as the missing of at least one scheduled radiotherapy fraction . results in all , 19 of 140 ( 13.6% ) patients treated with hf and 39 of 146 ( 26.7% ) treated with cf experienced treatment interruptions . 
no statistically signicant differences concerning the reasons for treatment interruptions could be detected between patients treated with cf or hf . conclusion hf is signicantly associated with a better patient compliance with the prescribed radiotherapy schedule compared with cf . 
the data suggest that this nding is basically related to the shorter overall treatment time of hf . keywords breast neoplasms radiotherapy dose hypofractionation radiation injuries risk factors signikant bessere patientencompliance bei hypofraktionierter im vergleich zu konventionell fraktionierter adjuvanter strahlentherapie des mammakarzinoms ergebnisse einer unizentrischen retrospektiven studie zusammenfassung hintergrund ziel der untersuchung war es , faktoren zu identizieren , die mit ungeplanten behandlungsunterbrechungen bei der adjuvanten strahlentherapie des mammakarzinoms assoziiert sind . methoden und patienten es wurden patienten untersucht , die eine adjuvante strahlentherapie der mamma oder brustwand zwischen mrz 2014 und august 2016 erhielten . zur anwendung kamen als fraktionierungsprotokoll und strahlentherapeutische technik eine konventionell fraktionierte ( cf ; 28 fraktionen mit 1 , 80 gy oder 25 fraktionen mit 2 , 00 gy ) oder eine hypofraktionierte strahlentherapie ( hf ; 15 fraktionen mit 2 , 67 gy ) , eine intensittsmodulierte ( imrt ) oder dreidimensional geplante konformale strahlentherapie ( 3dcrt )  . 
noncompliance wurde als gegeben be376 strahlenther onkol ( 2017 ) 193 : 375384 trachtet bei dem ausfall mindestens einer geplanten strahlentherapiefraktion . ergebnisse bei 19 von 140 ( 13 , 6 % ) patienten mit hf und 39 von 146 ( 26 , 7 % ) , die mit cf behandelt wurden , traten ungeplante behandlungsunterbrechungen auf . 
von 23 untersuchten faktoren ging als einziger unabhngiger signikanter faktor fr noncompliance das fraktionierungsprotokoll aus der multivariaten analyse hervor ( cf ; p = 0 , 007 ; odds ratio : 2 , 3 ; 95% - kondenzintervall : 1 , 34 , 2 )  . bezglich der ursachen ungeplanter behandlungsunterbrechungen konnte kein statistisch signikanter unterschied festgestellt werden . schlussfolgerung die hf ist signikant mit einer besseren patientencompliance im vergleich zur cf assoziiert . 
die daten legen nahe , dass diese assoziation hauptschlich auf die krzere gesamtbehandlungszeit der hf zurckzufhren ist . schlsselwrter neoplasien der mamma strahlentherapie hypofraktionierung strahlenbedingte nebenwirkungen risikofaktoren background unintended treatment interruptions may lead to a prolongation of the prescribed overall treatment time . 
this association appears to be consistent across many disease sites including head and neck cancer , cervical cancer , lung cancer , breast cancer , and other cancers [ 4 , 5 ]  . 
prospective and retrospective studies have shown that treatment prolongation can increase the risk of local recurrence by up to 2% per day for certain malignancies [ 5 ]  . the association between prolongation of the prescribed overall treatment time and inferior clinical outcomes has been explained with an accelerated repopulation of tumor clonogens , which can occur after treatment initiation [ 6 ]  . it has also been reported that noncompliance may serve as a behavioral biomarker for other risk factors that contribute to poor outcomes , such as noncompliance with other important clinician visits and procedures , lack of social support , and mood disorders [ 4 ]  . in this study , we analyzed the compliance to the prescribed radiotherapy schedule of breast cancer patients treated with postoperative radiotherapy of the whole breast or chest wall . 
the goal of the study was to identify factors signicantly associated with the occurrence of treatment interruptions . patients and methods data collection and patient selection the electronic patient les of 286 consecutive unselected patients treated with adjuvant breast cancer radiotherapy between march 2014 and august 2016 were reviewed . 
eligibility criteria for the analysis were ( a ) histologically proven diagnosis of breast cancer or carcinoma in situ and ( b ) treatment with adjuvant postoperative radiotherapy after breastconserving surgery or mastectomy . 
patients with personal commitments limiting the overall treatment time or patients living far away from the radiotherapy facility tended to opt for hf . the acute radiation reactions and reasons for treatment interruptions were documented prospectively in the local area network therapy information system lantis ( siemens healthcare , germany )  . 
the two observers were not involved in the statistical analysis of the study , and a table with all weekly assessments was included in the end of treatment report of all patients . 
the maximum acute radiation reaction observed during the full course of the radiotherapy ( including the boost to the tumor bed if applied ) was used for the statistical analysis . 
the planning target volume ( ptv ) of the whole breast or chest wall was dened according to the recommendations of the breast cancer atlas for radiation therapy planning consensus denitions of the radiation therapy oncology group ( rtog ) [ 10 ]  . 
daily online verication and correction of the patient positioning error prior to radiotherapy were performed for all patients using orthogonal megavoltage electronic portal images [ 11 ]  . no respiratory gating [ 1214 ] , integrated boost [ 15 , 16 ] , or partial breast irradiation [ 17 ] techniques were applied in this study . 
two tangential semi - opposed beams , physical wedges ( usually 15 or 30 ) , a 160 mlc multileaf collimator and 6 mv photons were used for the imrt and 3dcrt plans . 
occasionally a mixed - beam technique using 6 mv and 15 mv photons was used for the 3dcrt plans . inverse treatment planning and a step - and - shoot technique were used for all imrt plans . 
a few patients with left - sided breast cancer and unfavorable thoracic geometry were treated with seven - eld imrt in order to reduce the high - dose region to the heart [ 18 ]  . in total , 58 of 286 ( 20.3% ) patients experienced treatment interruptions . 
as expected , the mean age of the study population was considerably lower compared with reports from europe or the united states , most likely due to the young age structure of the general population [ 19 ]  . on univariate analysis , three of 23 tested factors were signicantly associated with a higher risk of treatment interruptions ( table 2 )  . 
after compensation for treatment interruptions , eventually 41.4% of the patients with treatment interruptions completed their treatment within the prescribed overall treatment time , corresponding to 88.1% of the total study population . 
the remaining patients experienced a prolongation of the prescribed overall treatment time of 15 days ( table 3 )  . statistical analysis discussion differences between patient groups stratied by the occurrence of treatment interruptions ( table 1 ) or by the fractionation regimen ( table 3 ) were assessed using the chi - square test or t test where appropriate . 
our study revealed another advantage of hf over cf : a signicantly better patient compliance with the prescribed radiotherapy schedule . noncompliance with the prescribed radiotherapy schedule can have multiple deleterious effects . 
for postoperative radiotherapy of breast cancer , a prolongation of the overall treatment time of more than 1 week has been shown to decrease the 5 - year local control rate by 5% [ 26 ]  . 
the management of the increased number of recurrences may place additional burden on the health - care systedisturbances in the clinical workow by noncompliant ( no - show ) patients occupying treatment slots on the linear accelerator may indirectly cause treatment delays for other patients and an extension of the work day . 
distance from the patients home to the radiotherapy facility [ 2830 ] and patients from households that lost family income [ 31 ] have been reported as predictors of noncompliance with the prescribed radiotherapy schedule by other study groups . 
it is likely that factors inuencing compliance depend to a signicant extent on individual circumstances like the location of the radiotherapy facility , infrastructure of the region , and socioeconomic status of the population , and may therefore vary between treatment facilities . 
however , in our study cf , which was the longer radiotherapy schedule compared with hf , was the only signicant predictor of noncompliance on multivariate analysis of 23 factors . the limitations of our study should be noted . 
the socioeconomic and psycho - oncological status of the patients could not be evaluated because of lack of data . moreover , owing to the retrospective nature of the study , a selection bias of patients treated with hf and cf cannot be excluded with certainty . despite all efforts to avoid a prolongation of the prescribed overall treatment time by thorough education of the patient and compensation of missed radiotherapy fractions by treatment on weekends , 34 of 286 patients ( 11.9% ) in our study eventually experienced a moderate prolongation of the prescribed overall treatment time of 15 days . 
however , a signicant decrease in the 5 - year local control rate after treatment interruptions of more than 1 week has been reported [ 26 ]  . conclusion a signicant proportion of breast cancer patients in our study experienced treatment interruptions . 
this nding may add to the treatment decision in favor of hf in particular in situations with expected lower compliance with longer radiotherapy schedules . compliance with ethical guidelines conict of interest v . 
abou ghaida declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
mrz 2017 springer - verlag berlin heidelberg 2017 hintergrund bei der hier zu kommentierenden studie handelt es sich um die langzeitergebnisse der getug01 - studie ( french genitourinary study group )  . 
ziel der arbeit war es , das krankheitsfreie berleben und das gesamtberleben des studienkollektivs auszuwerten und eine potenzielle interaktion zwischen antihormoneller therapie und bestrahlung der pelvinen lymphknotenstationen beim prostatakarzinom zu erfassen . patienten und methode in die studie wurden 446 patienten mit einem prostatakarzinom t1bt3 / cn0 / cm0 zwischen dezember 1998 und juni 2004 eingeschlossen . 
stratiziert wurde in zwei patientengruppen : der niedrigrisikogruppe wurden die patienten mit t1 / t2 - status , gleason - score 6 und psa < 3 - facher oberer normwert zugeteilt . 
die dosis lag bei originalpublikation pommier p , chabaud s , lagrange jl et al ( 2016 ) is there a role for pelvic irradiation in localized prostate adenocarcinoma ? update of the long - term survival results of the getug - 01 randomized study . 
70 gy fr die prostataloge . ergebnisse bei einer medianen nachbeobachtung von 11 , 4 jahren waren das gesamtberleben ( os ) und das krankheitsfreie berleben ( dfs ) in den behandlungsarmen nicht signikant unterschiedlich . 
dieser vorteil scheint nur bei patienten ohne antihormonelle therapie relevant zu sein . schlussfolgerung der autoren die beckenbestrahlung bei lokal begrenztem prostatakarzinom scheint das dfs und das os im gesamtkollektiv nicht signikant zu verbessern , mglicherweise aber bei ausgewhlten niedrigrisikopatienten und patienten mit intermedirem risiko . kommentar die arbeit ist eine von drei randomisierten studien , die sich mit der frage nach der bestrahlungsnotwendigkeit der pelvinen lymphknotenstationen bei nodal - negativem prostatakarzinom beschftigen . 
schloss ein groes patientenkollektiv von ungefhr strahlenther onkol ( 2017 ) 193 : 428430 1300 patienten , alle mit einem risiko fr eine lymphogene metastasierung von > 15 % , ein [ 2 ]  . 
sie war allerdings vierarmig angelegt und hatte im vergleich zu der hier kommentierten arbeit mit 6 , 6 jahren ein deutlich krzeres medianes follow - up . die entscheidende aussage der arbeit von pommier et al . 
damit besttigt diese arbeit die klinische routine , auerhalb von studien fr das gesamtkollektiv nodal - negativer patienten mit prostatakarzinom auf die elektive beckenbestrahlung zu verzichten . dies deckt sich auch mit den aktuellen empfehlungen der deutschen s3 - leitlinie und der nccn - leitlinie ( national comprehensive cancer network )  . auch fr die soweit ersichtlich initial geplante subgruppenanalyse zeigt sich weder fr die niedrigrisikogruppe noch fr die hochrisikogruppe ein vorteil . 
insbesondere die aussage , dass patienten ohne antihormonelle therapie , die nach der roach - formel ein risiko fr eine lymphogene metastasierung < 15 % aufweisen , von der bestrahlung des beckens protieren knnten , darf in unseren augen keine nderung der klinischen routine nach sich ziehen . 
so liegen die ergebnisse der pommier - arbeit kontrr zu den daten der rtog - 94 - 13studie , die ein prostatakarzinomkollektiv mit einem risiko von > 15 % fr eine lymphogene metastasierung untersucht hatte . 
dort gab es hinweise , dass patienten mit antihormoneller therapie von einer beckenbestrahlung protieren [ 2 ]  . in der diskussion der hier kommentierten studie relativieren die autoren selbst dieses ergebnis und empfehlen keine nderung der klinischen praxis . 
anhand dieser daten knnte man zumindest die empfehlung aussprechen , dass keine simultane radiatio der pelvinen lymphknotenstationen mit einer antihormonellen therapie erfolgen solleinige weitere argumente , die die ergebnisse der studie limitieren knnten , sollten schlielich noch erwhnt werden : die studie hatte bezogen auf die patientenanzahl relativ weit gefasste einschlusskriterien . 
zudem waren unterschiedliche fraktionierungsschemata erlaubt , was allerdings die klinische realitt gut wiederspiegelt . ein weiterer kritisch zu betrachtender punkt ist die tatsache , dass die gesamtdosis , die fr die prostataloge vorgegeben war , im laufe der studie von 66 auf 70 gy angepasst wurde [ 3 ]  . 
heute gilt aber selbst die dosis von 70 gy als zu niedrig . der kritische leser der pommier - studie kann sich auch des eindrucks nicht erwehren , dass mglicherweise die relevanten pelvinen lymphabussstationen der prostata nicht ausreichend erfasst wurden . 
zudem erscheint ein sicherheitssaum von 10 mm mit den mglichkeiten der modernen igrt auch nicht mehr zeitgem [ 3 ]  . seit der damico - arbeit [ 4 ] werden die patienten wie die autoren richtigerweise schreiben in drei risikogruppen unterteilt . 
da die patienten in der vorliegenden studie auf nur zwei risikogruppen stratiziert wurden , mindert auch dies die aussagekraft der studie , vor allem aber die bertragbarkeit ihrer schlussfolgerungen auf die heutige klinische praxis . eine wichtige frage , die unbeantwortet bleibt , aber hochinteressant wre , ist diejenige der rezidivlokalisation . handelte es sich bei den beschriebenen rezidiven um lokale , lokoregionre oder systemische rezidive oder war ihre lokalisation unklar , also im sinne eines biochemischen rezidivs ? knnten die autoren diese frage untersuchen , wrde das bei der interpretation der weiteren ergebnisse sehr helfen . eine weitere nichtbeantwortete frage betrifft die langzeittoxizitt . 
vermutlich wurden die daten nicht erhoben . nicht zuletzt fhrten die autoren lediglich eine intendto - treat - analyse durch , aber keine analyse as treated . diese wre wnschenswert gewesen , zumal aus der arbeit bisher nicht im detail hervorgeht , wie viele patienten berhaupt protokollgem behandelt wurden . literatur fazit die hier kommentierte arbeit zeigt einige wichtige ergebnisse , beispielsweise die kernaussage , dass nicht alle prostatakarzinompatienten von der bestrahlung der pelvinen lymphknotenstationen protieren . 
asbell so , martz kl , shin kh et al ( 1998 ) impact of surgical staging in evaluating the radiotherapeutic outcome in rtog #77 - 06 , a phase iii study for t1bn0m0 ( a2 ) and t2n0m0 ( b ) prostate carcinoma . 
lawton ca , desilvio m , roach m et al ( 2007 ) an update of the phase iii trial comparing whole pelvic to prostate only radiotherapy and neoadjuvant to adjuvant total androgen suppression : updated analysis of rtog 94 - 13 , with emphasis on unexpected hormone / radiation interactions . 
pommier p , chabaud s , lagrange jl et al ( 2007 ) is there a role for pelvic irradiation in localized prostate adenocarcinoma ? preliminary results of getug - 01 . 
damico av , whittington r , malkowicz sb et al ( 1998 ) biochemical outcome after radical prostatectomy , external beam radiation therapy , or interstitial radiation therapy for clinically localized prostate cancer . 
combs1 , 2 received : 30 august 2016 / accepted : 6 january 2017 / published online : 27 january 2017 springer - verlag berlin heidelberg 2017 abstract background complementary and alternative medicine ( cam ) are gaining in importance , but objective data are mostly missing . 
thus , the aim was to evaluate most frequently used methods , their signicance and the general acceptance amongst cancer patients undergoing radiotherapy ( rt )  . methods a questionnaire of 18 questions based on the categorical classication released by the national centre for complementary and integrative health was developed . from april to september 2015 , all patients undergoing rt at the department of radiation oncology , technical university of munich , completed the survey . 
the maelectronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 017 - 1101 - 5 ) contains supplementary material , which is available to authorized users . ( cid : 2 ) kerstin a . 
ziel war die erfassung der meist gewhlten cam , ihr stellenwert sowie die generelle akzeptanz bei radioonkologischen patienten . methoden ein fragebogen mit 18 fragen , basierend auf der kategorischen einteilung des national center for complementary and integrative health , wurde entwickelt . 
alle patienten , die zwischen april und september 2015 an der klinik fr radioonkologie und strahlentherapie des klinikums rechts der isar eine strahlentherapie ( rt ) erhalten 420 strahlenther onkol ( 2017 ) 193 : 419425 hatten , wurden evaluiert . 
akzeptanznderungen der patienten hinsichtlich cam wurden mit einem weiteren fragebogen nach rt bei der ersten nachsorgeuntersuchung ermittelt ( n = 31 )  . ergebnisse von 634 patienten beantworteten 333 ( 52 , 5 % ) den fragebogen . 
beweggrnde fr den camgebrauch waren das immunsystem zu verbessern ( 43 , 8 % ) , therapienebenwirkungen zu verringern ( 43 , 8 % ) und keine chance auszulassen ( 37 , 8 % )  . 
akupunktur wrden 63 , 7 % ( 212 / 333 ) der rt - patienten in anspruch nehmen . schlussfolgerung im studienvergleich zeigte sich , dass der cam - einsatz parallel zur rt an unserer klinik gering ist . eine patientenakzeptanz ist vorhanden , da etwa zwei drittel eine in das individuelle therapiekonzept integrierte cam nutzen wrden . schlsselwrter radiotherapie krebs ganzheitliche medizin immunsystem nebenwirkungen introduction patients diagnosed with cancer often have difculty to deal with the new situation , experiencing enormous physical and mental stress . 
increasingly often , patients also turn to complementary and alternative medicine ( cam ) , hoping that treatment - related side effects of traditional cancer care may be easier to bear . 
with 5070% in germany , 4549% in australia and 95% in the us [ 49 ]  . over the last few years , the use of cam has gained importance , even though objective data are mostly missingespecially in radiation oncology . 
for example , acupuncture can help to decrease common side effects of rt , such as nausea , xerostomia , dysphagia , mucositis , hair loss or fatigue [ 12 , 13 , 15 ]  . furthermore , cam therapies can provide the same or even a better effect compared to conventional treatment . 
in thailand , it was demonstrated that court - type traditional thai massage ( cttm ) compared to amitriptyline administration could be an alternative way of treating chronic tension - type headaches [ 17 ]  . in radiation oncology , management of treatment - related side effects is a main goal , and the use of cam may be an important pillar in this clinical situation . 
therefore , it is important to gain evidence - based information about cam to strengthen a more holistic approach aside of conventional western medicine [ 18 ]  . in the present study , we have evaluated patients motivation in using cam during a course of rt and sought to determine whether there are any correlations between sociodemographic characteristics and usage of cam . 
therefore , the aim of our study has been to evaluate the most frequently used methods , their signicance , as well as the general acceptance amongst cancer patients undergoing rt . materials and methods for the survey , a detailed questionnaire was developed based on the categorical classication of different cam methods released by the national centre for complementary and integrative health ( nccih )  . 
finally , the questionnaire comprising 18 questions , of which some have subitems , was approved by the ethics committee of the technical university of munich ( tum ) with the project number 267 / 15 . on the rst page , patients are asked to provide some sociodemographic information , e . 
patients were assured that the collected data would not have any inuence on their treating regimens and they would suffer no adverse effect . statistical calculations were done in a primarily descriptive way . 
detailed patients characteristics , including the type of cancer , received therapy , insurance status , marital status and children status are shown in table 1 . of all participants , 26.4% ( 88 / 333 ) used one or more cam therapies during rt ( 61 women , 18 men , 9 unknown )  . 
2 most frequently applied methods during therapy ( multiple answers were possible ) changes in attitudes toward cam during and after rt in order to gain more information about the changes in attitude towards complementary medicine , we also handed out the questionnaire a second time after rt during the rst follow - up visit ( n = 31 )  . of all participants , 19.4% ( 6 / 31 ) stated in the initial questionnaire that they used cam during rt . 
in total , 333 patients took part with a return rate of 52.5%. it became apparent that 26.4% ( 88 / 333 ) used cam during their rt and a total of 39.3% ( 131 / 333 ) had already used complementary medicine before rt . 
3 most common reasons for complementary and alternative medicine ( cam ) use ( multiple answers were possible ) pation in our study , could be one of the reasons for the increase and , therefore , also for the low prevalence rate of cam use in the initial survey . many studies have tried to characterize a typical prole of a cam user according to sociodemographic as well as illness - related data . 
young female patients with higher educational level suffering from breast cancer are often associated with higher cam use than other patients [ 4 , 5 , 7 , 8 , 27 ] , whereas in other studies no correlations between gender , interest in cam , cancer diagnosis , age and educational level can be found [ 3 , 6 , 28 , 29 ]  . 
this corresponds to the literature : wilkinson et al . [ 7 ] reported vitamin / mineral supplement as most frequently used followed by herbal supplements , chiropractic and massage therapy ; biologically based treatments ( vitamins and trace elements and medical herbs ) , prayer and acupuncture are most often used in a german comprehensive cancer center [ 3 ]  . 
it could be shown that patients willingness increased during and after rt , potentially due to the side effects reducing the overall quality of life ( qol ) , or the additional time gained after the diagnosis to seek information on alternative treatment methods . 
however , the sample size of the follow - up group was low ( n = 31 ) and limits signicant statements . the prevalence of cam use during rt in our oncology center with 26.4% is quite low compared to other departments and countries which show varying prevalence rates from 3295% [ 39 , 1925 ]  . 
in the us , 95% reported using some type of cam , whereas in asia about 45% of patients use one or more cam therapies [ 9 , 26 ]  . 
in our follow - up survey , we had only a small number of participants ; however , we could see that prevalence rate moderately increased from 19 to 32% . 
5 user rates of complementary and alternative medicine methods ( multiple answers were possible ) 100% strahlenther onkol ( 2017 ) 193 : 419425 initial questionnaire ( n = 6 ) follow - up questionnaire ( n = 10 ) exists , but mostly reasons of improving the immune system / physical well - being , reducing side effects and becoming active are mentioned [ 2 , 4 , 6 , 23 , 27 , 32 ]  . 
between may and july , 2015 cancer patients from participating centers and departments which were part of the certication process were interviewed . when patients undergo cancer treatment , it is most likely that their attitude towards cam may change , however , no data is available and no previous study has analysed how patients willingness to apply cam may develop over time . in the present work we have evaluated patients after diagnosis , at the beginning of rt . 
a second survey was conducted at the rst follow - up after treatment was completed . the results show that patients are increasingly interested in cam ; the proportion of methods that would be accepted or are accepted remains widely unchanged , whereas herbs and plants , as well as breath exercises , are more present in the follow - up questionnaire . 
while physiotherapy or breath exercises are not counted as cam in germany , they are listed in the nccih guidelines and thus included in the research work . conclusion in comparison to other studies , usage of cam parallel to rt in our department is considered to be low . 
not offering cam personally to them was mostly stated by patients , which stresses the idea that cam should be offered on a professional basis in a university - based cancer center . the acceptance amongst patients is present , as treatment integrated into the individual oncology therapy concept would be used by about two - third of patients . 
particularly improving the immune system , reducing side effects , not missing an opportunity and improving the impact of therapy are the motivators for using cam . however , more information , in terms of personal consultations with physicians , brochures or online information , could encourage a holistic therapy [ 35 ]  . 
therefore , more evidence - based data on cam relating to rt are required . strahlenther onkol ( 2017 ) 193 : 419425 compliance with ethical guidelines conict of interest s . 
mrz 2017 springer - verlag berlin heidelberg 2017 hintergrund die klassische mikrochirurgische behandlung und die stereotaktische radiochirurgie gelten bei hirnmetastasen , einer arteriovensen malformation ( avm ) oder einem vestibularisschwannom ( vs ) in geeigneten fllen als gleichwertige therapieverfahren . 
die autoren caruso et al . werfen daher die frage auf , ob und in welchem umfang zwischen operativem vorgehen ( op ) und radiochirurgie ( rc ) kostenunterschiede bestehen . patienten und methoden hierzu wurden an einer einzelnen nordamerikanischen universittsinstitution insgesamt 44 operierte patienten mit einer der drei diagnosen ber einen 3 - jahres - zeitraum genau 12 monate lang in bezug auf alle anfallenden kosten untersucht . 
scheinen auf den ersten blick sowohl fr kostentrger als auch fr patienten und nicht zuletzt fr den radioonkologen gleichermaen interessant zu sesie zeigen klar , dass eine nichtoperative behandlung offenbar aller drei entitten , nmlich der metastase , des vestibularisschwannoms und der arteriovensen malformation mit einer kostenreduktion von ca . 
allerdings muss einschrnkend betont werden , dass zahlreiche institutionen in deutschland wohl auf der basis unterschiedlicher technischer voraussetzungen ( linac - basierte rc , gamma knife , cyberknife ) instrahlenther onkol ( 2017 ) 193 : 426427 dividuelle kassenvereinbarungen erreichen konnten , zu deren hhe und genauem inhalt keinerlei transparenz besteht . 
mithin kann prinzipiell eine einzeit - rc naturgem auch ambulant erfolgen , was ein entgelt im rahmen des bestehenden einheitlichen bewertungsmastabs ( ebm ) und der nomenklatur der gebhrenordnung fr rzte ( go ) nach sich zge . 
hier allerdings kann angenommen werden , dass allenfalls kosten in der grenordnung von 25 % ( ebm ) bis 40 % ( go ) , bezogen auf die operative drg ( diagnosis related groups ) , entstnden . 
dabei muss auch beachtet werden , dass die erlse nicht exakt den kosten entsprechen und dass in der hier diskutierten arbeit auch die folgekosten mit in betracht gezogen wurden . ist eine ausschlieliche betrachtung der kosten berhaupt zulssig ? bei vorliegen konkurrierender , mutmalich gleichwertiger behandlungsmglichkeiten besteht dem patienten gegenber grundstzlich eine informationspicht und , was noch besser wre , eine interdisziplinre aufklrung des patienten ber die art der unterschiedlichen vorgehensweisen , die vorteile und risiken . 
kostenbetrachtungen aus dem blickwinkel des kostentrgers nden hier erstaunlicherweise nur ausnahmsweise einmal statt , denn das gegenteil ist meist der fall : die zunehmende vereinnahmung rztlichen denkens durch betriebswirtschaftliche einsse von groupern und controllern in den krankenhusern kann u . 
dazu fhren , dass man rztlicherseits zu der behandlungsalternative tendiert , die mit dem hchsten erls fr die jeweilige klinik verbunden ist . in der praxis ist eine wirkliche , vollkommene gleichwertigkeit der operativen und der radiochirurgischen vorgehensweise de facto wohl am ehesten bei kleinen , mglichst solitren hirnmetastasen und bei kleinen vestibularisschwannomen gegeben . 
lebensjahr diagnostiziert und seit der studie der european organisation for research and treatment of cancer ( eortc ) von stupp und kollegen [ 1 ] nach der histologischen sicherung mit einer kombinierten therapie aus einer strahlentherapie bis zu einer gesamtdosis von 60 gy und einer zunchst begleitenden chemotherapie mit temozolomid ( tmz ) mit 75 mg / m2 / tag parallel zur strahlentherapie behandelt . 
die arbeit von stupp und kollegen zeigte in einer post - hoc - analyse eine verminderte originalpublikation perry jr , laperriere n , ocallaghan cj et al ( 2017 ) short - course radiation plus temozolomide in elderly patients with glioblastoma . 
um aber der insgesamt schlechteren prognose von lteren patienten rechnung zu tragen , wurde in der folge die wirksamkeit einer verkrzten strahlentherapie berprweiterhin wurde durch die noa - 08 - studie gezeigt , dass insbesondere die patienten mit methyliertem mgmt - promotor durch eine alleinige chemotherapie mit tmz gut behandelbar sind [ 5 ]  . 
offen war weiterhin , ob eine hypofraktionierte strahlentherapie in kombination mit einer begleitenden und adjuvanten tmz - behandlung bei lteren patienten > 65 jahre einen vorteil gegenber der alleinigen strahlentherapie bringt . 
diese lcke wurde nun durch die arbeit von perry und kollegen geschlossen [ 6 ]  . patienten und methoden insgesamt wurden 562 patienten mit einem histologisch gesicherten glioblastom und einem alter von mindestens 65 jahren ( median 73 jahre ; spanne 6590 jahre ) sowie einem allgemeinzustand von mindestens ecog 2 ( eastern cooperative oncology group ) zwischen einer alleinigen strahlentherapie und einer kombinierten rct randomisiert . 
das klinische zielvolumen war mit der resektionshhle und kontrastmittelaufnehmenden lsionen in eistrahlenther onkol ( 2017 ) 193 : 510512 ner kraniellen magnetresonanztomographie ( cmrt ) mit einem sicherheitssaum von 15 mm vorgegeben . 
die chemotherapie war dem stupp - protokoll angelehnt und bestand aus 75 mg / m2 / tag tmz whrend der strahlentherapie und einer sich 4 wochen spter anschlieenden serie aus bis zu 6 zyklen tmz an jeweils 5 von 28 tagen ( dosis 150200 mg / m2 / tag )  . 
die studie wurde von der canadian cancer trials group ( cctg ) , der eortc und der trans tasman radiation oncology group durchgefhrt . ergebnisse das mittlere berleben ( os ) nach kombinierte rct war mit 9 , 3 monaten signikant lnger als im allein strahlentherapierten arm mit 7 , 6 monaten ( p < 0 , 0001 )  . auch das mediane progressionsfreie berleben ( pfs ) war mit 5 , 3 monaten nach rct signikant lnger als nach alleiniger radiotherapie ( 3 , 9 monate ; p < 0 , 001 )  . 
auf lngere sicht war jedoch der krankheitsprogress der am strksten die lebensqualitt beeinussende faktor . chemotherapie ber die strahlentherapie beim mgmt - methylierten patienten zeigten , ist nun letztlich mit den aktuellen markern keine gruppe mehr abgrenzbar , die nicht von der multimodalen therapie protieren wrde [ 5 ]  . 
die schlussfolgerung heit daher , dass die beste behandlung fr die glioblastome , unabhngig vom patientenalter und dem biomarker mgmt - promotormethylierung des jeweiligen tumors , derzeit die kombinierte rct ist . damit ist letzten endes fr ltere patienten nur noch die fraktionierung der strahlentherapie ein diskussionspunkt . hier besteht noch eine evidenzlcke , da die gleichwertigkeit der standardfraktionierten mit der hypofraktionierten strahlentherapie nur in monotherapie - studien gezeigt wurde [ 9 , 10 ]  . 
da insbesondere bei den patienten mit methyliertem mgmt - promotor die berlebenszeiten der ber 65 - jhrigen mit median ber 13 monate vergleichsweise lang sind , muss man sich daher fragen , ob die argumentation der schlechteren prognose fr diese therapieverkrzung und - deeskalation noch greift , oder ob nicht die klassische dosierung der bestrahlung mit 60 gy in 2 - gy - einzeldosen kombiniert mit tmz angewandt werden sollte [ 11 ]  . schlussfolgerung der autoren auch ltere patienten in zum teil reduziertem allgemeinzustand protieren von einer rct . 
die arbeit reiht sich damit in die liste der arbeiten ein , die bei den hirneigenen tumoren von anfang an eine mglichst entschlossene therapie , bestehend aus maximaler resektion , ausreichend dosierter strahlentherapie und simultaner bzw . 
anschlieender chemotherapie gefordert haben [ 1 , 7 , 8 , 11 ]  . mit der arbeit brckelt jedoch auch das fundament unter der biomarker - getriggerten therapieempfehlung [ 12 ]  . whrend die noa - 08 - daten noch eine berlegenheit der die arbeit von perry und kollegen wird die indikationsstellung und die leitlinien zur behandlung von lteren patienten mit glioblastomen verndern . 
man sollte sich aber auch fragen , ob nicht bei lteren patienten mit schlechter prognose die klassische dosierung der bestrahlung mit 60 gy in 2 - gyeinzeldosen kombiniert mit tmz angewandt werden sollte . christoph straube und stephanie e . 
stupp r , mason wp , van den bent mj , weller m , fisher b , taphoorn mjb , belanger k , brandes a , marosi c , bogdahn u , curschmann j , janzer rc , ludwin sk , gorlia t , allgeier a , lacombe d , cairncross jg , eisenhauer e , mirimanoff ro ( 2005 ) radiotherapy plus concomitant and adjuvant temozolomide for glioblastoma . 
stupp r , hegi me , mason wp , van den bent mj , taphoorn mj , janzer rc , ludwin sk , allgeier a , fisher b , belanger k , hau p , brandes aa , gijtenbeek j , marosi c , vecht cj , mokhtari k , wesseling p , villa s , eisenhauer e , gorlia t , weller m , lacombe d , cairncross jg , mirimanoff ro ( 2009 ) effects of radiotherapy with concomitant and adjuvant temozolomide versus radiotherapy alone on survival in glioblastoma in a randomised phase iii study : 5 - year analysis of the eortc - ncic trial . 
laperriere n , weller m , stupp r , perry jr , brandes aa , wick w , van den bent mj ( 2013 ) optimal management of elderly patients with glioblastoma . 
keime - guibert f , chinot o , taillandier l , cartalat - carel s , frenay m , kantor g , guillamo j - s , jadaud e , colin p , bondiau p - y , mene p , loiseau h , bernier v , honnorat j , barri m , mokhtari k , mazeron j - j , bissery a , delattre j - y ( 2007 ) radiotherapy for glioblastoma in the elderly . 
wick w , platten m , meisner c , felsberg j , tabatabai g , simon m , nikkhah g , papsdorf k , steinbach jp , sabel m , combs se , vesper j , braun c , meixensberger j , ketter r , mayer - steinacker r , reifenberger g , weller m ( 2012 ) temozolomide chemotherapy alone versus radiotherapy alone for malignant astrocytoma in the elderly : the noa - 08 randomised , phase 3 trial . 
perry jr , laperriere n , ocallaghan cj , brandes aa , menten j , phillips c , fay m , nishikawa r , cairncross jg , roa w , osoba d , rossiter jp , sahgal a , hirte h , laigle - donadey f , franceschi e , strahlenther onkol ( 2017 ) 193 : 510512 chinot o , golnopoulos v , fariselli l , wick a , feuvret l , back m , tills m , winch c , baumert bg , wick w , ding k , mason wp ( 2017 ) short - course radiation plus temozolomide in elderly patients with glioblastoma . 
buckner jc , shaw eg , pugh sl , chakravarti a , gilbert mr , barger gr , coons s , ricci p , bullard d , brown pd , stelzer k , brachman d , suh jh , schultz cj , bahary j - p , fisher bj , kim h , murtha ad , bell eh , won m , mehta mp , curran wjj ( 2016 ) radiation plus procarbazine , ccnu , and vincristine in low - grade glioma . n engl j med 374 : 13441355 . 
brown tj , brennan mc , li m , church ew , brandmeir nj , rakszawski kl , patel as , rizk eb , suki d , sawaya r , glantz m ( 2016 ) association of the extent of resection with survival in glioblastoma : a systematic review and meta - analysis . 
roa w , brasher pm , bauman g , anthes m , bruera e , chan a , fisher b , fulton d , gulavita s , hao c , husain s , murtha a , petruk k , stewart d , tai p , urtasun r , cairncross jg , forsyth p ( 2004 ) abbreviated course of radiation therapy in older patients with glioblastoma multiforme : a prospective randomized clinical trial . 
malmstrm a , grnberg bh , marosi c , stupp r , frappaz d , schultz h , abacioglu u , tavelin b , lhermitte b , hegi me , rosell j , henriksson r ( 2012 ) temozolomide versus standard 6 - week radiotherapy versus hypofractionated radiotherapy in patients older than 60 years with glioblastoma : the nordic randomised , phase 3 trial . 
combs se , wagner j , bischof m , welzel t , wagner f , debus j , schulz - ertner d ( 2008 ) postoperative treatment of primary glioblastoma multiforme with radiation and concomitant temozolomide in elderly patients . 
through tissue deformation and relaxation , this causes target and risk organ displacement and driin this study , prefraction shift and intrafraction drift of the prostate are quantied during robotic transperineal 4dus . methods the position of the prostate was recorded for different positions of the probe before treatment in 10 patients ( 16 series of measurements )  . 
slight probe pressure can improve image quality , but excessive probe pressure can distort the surrounding anatomy and potentially move risk organs closer to the high - dose area . keywords external beam radiotherapy transperineal ultrasound patient positioning intrafraction motion quality assurance prfraktionelle verschiebung und intrafraktionelle drift der prostata durch druck perinealer ultraschallkpfe zusammenfassung zielsetzung in der bildgefhrten strahlentherapie der prostata ben perineale ultraschallkpfe whrend planung und behandlung druck auf das perineum aus . 
in dieser studie werden verschiebungen vor und relaxationen whrend der behandlung unter transperinealem ortsund zeitaufgelstem ultraschall ( us ) quantiziert . methoden vor der behandlung ( 10 patienten , 16 messreihen ) wurde die lage der prostata bei verschiedenen schallkopfpositionen aufgezeichnet . 
whrend der behandlung ( 15 patienten , 273 fraktionen ) mit anliegender perinealer probe wurde die intrafraktionelle bewegung der prostata aufgezeichnet ( insgesamt 27 h 24 min )  . ergebnisse pro 1 mm verschiebung des schallkopfs nach kranial verschob sich die prostata um 0 , 42 0 , 09 mm , eben460 strahlenther onkol ( 2017 ) 193 : 459465 falls in kranialer richtung . 
nach drucklosem kontakt des us - kopfs war fr eine gute bildqualitt eine verschiebung in das perineum um typischerweise 510 mm notwendig , was einer verschiebung der prostata von etwa 24 mm in kranialer richtung entspricht . 
whrend der behandlung driftete die prostata mit einer mittleren rate von 0 , 075 mm / min in kranialer richtung ( p = 0 , 0014 )  . schlussfolgerung der druck des perinealen schallkopfs hat hnlich groen einuss auf die lage der prostata , wie derjenige eines abdominellen . 
miger druck des schallkopfs kann die bildqualitt verbessern , bergroer druck jedoch die umliegende anatomie verformen und potentiell risikoorgane in regionen hherer dosis verschieben . schlsselwrter externe strahlentherapie transperinealer ultraschall patientenpositionierung intrafraktionelle bewegung qualittssicherung introduction in external beam radiotherapy ( ebrt ) , tumor control probability and normal tissue toxicity are strongly correlated to the ability to deposit dose within the limits of the clinical target volume . 
in particular , the quality of image - guided radiotherapy ( igrt ) relies on the precise alignment and conformity of target volumes during planning , positioning control , and treatment . thus , any accidental shifts between patient positioning and actual treatment may prove problematic . 
while three - dimensional ultrasound may be quite a precise modality for igrt of the prostate [ 14 ] , the impact of varying probe pressure has been described for transabdominal ultrasound [ 57 ]  . 
some methods to correct for this effect have also been suggested [ 810 ]  . in our clinical routine for ebrt of the prostate , transperineal ultrasound has replaced transabdominal ultrasound . transperineal ultrasound offers several advantages such as improved image quality and less operator variability . 
most importantly , unlike abdominal probes , perineal probes do not interfere with either ct scanners or the treatment beam . hence , they need not be removed during planning or treatment and can be used for intrafraction monitoring . 
this also reduces the bias from different congurations during planning and treatment . nonetheless , the magnitude of target and risk organ displacement and tissue deformation due to varying probe pressure and the relaxation during treatment need to be experimentally quantied to assess their inuence on treatment quality . 
the aim of this study is to quantify prefraction shift and intrafraction drift of the prostate during robotic transperineal four - dimensional ultrasound ( 4dus )  . patients and methods two separate experiments were performed : before treatment , increasing pressure was applied to the perineum by the ultrasound probe , and the resulting displacement of the prostate was detected . 
during treatment , relaxation of the deformed tissue was observed as a slow systematic drift of the prostate . in both cases , the position of the prostate was detected by three - dimensional ultrasound . 
it consisted of a perineal ultrasound probe , a ceiling - mounted system of infrared cameras for probe position detection , a bedside workstation , and associated server - side hardware and software . 
the ultrasound probe was xed to the treatment table and made gel - mediated contact with the perineum . as regards prefraction displacement , for each of 10 patients , one to four series of each ve to seven scans were performed . 
between any two scans of a series , the probe was moved by 5 mm ( 10 mm in case of one obese patient with especially soft tissue ) towards the patient , in the cranial direction , with increasing manual force , increasing pressure on the perineuon each of the scans , the shift of the prostate position in the longitudinal , vertical , and lateral direction was detected by the clarity systefor each series , the data were visualized as a scatter plot and the line of best t was determined from ordinary least squares linear regression . 
elasticities were plotted for the longitudinal direction . as regards intrafraction relaxation , for the same 10 paintrafraction tients as above and additional 5 patients , strahlenther onkol ( 2017 ) 193 : 459465 fig . 
1 ultrasound images of the prostate and perineum . from ad , the ultrasound probe ( protruding from right side ) is moved in the cranial direction ( white arrows )  . 
as the pressure on the perineum increases , the prostate ( dark contour ) is displaced in the cranial direction and the surrounding tissue ( for example , the bulb , light contour ) is compressed ( white arrows )  . the shifts between frames are illustrative and not to scale . 
note that image quality improves between the rst scan ( a , no pressure applied ) and the second scan ( b , slight pressure applied ) , but does not further improve substantially with more pressure motion of the prostate was tracked during 273 fractions by four - dimensional transperineal ultrasound . 
compared to the total number of fractions delivered , this amounts to about every other fraction on average because unlike interfractional positioning control , intrafraction motion was not monitored on a daily basis . 
during these measurements , slight to average pressure was applied to the perineum ( in the wording of this study , a shift of the probe of about 5 to 10 mm after contact with the perineum ) , and there was no intentional variance in probe pressure on top of routine interoperator variability . statistical analysis was performed with microsoft excel , version 2010 . results prefraction displacement a total of 10 patients with histologically conrmed adenocarcinoma of the prostate received normofractionated ebrt in our institution with a cumulative dose of 7276 gy , depending on the tumor stage . 
image quality improved between the rst image ( almost no pressure applied ) and the second ( 5 mm compression ) or third image ( 10 mm compression with slight pressure applied ) in each series , but any further increase in ultrasound probe pressure did not result in additional relevant improvements in image quality . 
overall patient demographics and treatment parameters were very similar . on average ( n = 273 fractions ) , the prostate was drifting at a rate of 0.075 mm per minute in the cranial direction . 
in particular , an empty area in the caudal direction is visible , where the degrees of freedom of the prostate are probably limited by the presence of the ultrasound probe . discussion as was reported in case of transabdominal imaging [ 57 ] , we also observed a prefraction displacement of the prostate in transperineal imaging due to the pressure applied by the ultrasound probe . 
in addition , we were able to detect a systematic intrafraction drift of the prostate which was probably caused by a relaxation of the compressed perineal tissue between prostate and probe . in a phantom study [ 5 ] , the distance between the phantom surface and the prostate was measured . 
this compression of the tissue in between the prostate and the probe was also seen in our study . it is difcult to compare numbers , however , as the phantom was made from gelatin mold which probably has different elasticity compared to our patients . 
2 there is a linear relationship ( r = 0.99 in this example ) between the pressure exerted by the ultrasound ( us ) probe against the perineum and the displacement of the prostate . 
it is not surprising that the shifts during transabdominal imaging had a comparably larger vertical component than during our transperineal imaging where the force vector points in the longitudinal direction . in a study with 8 patients and 17 volunteers [ 7 ] , both moderate and strong pressure were applied during transabdominal imaging . 
at strong pressure a displacement of the prostate by about 2 mm was observed both in the longitudinal as well as vertical direction , but no substantial shifts in the lateral direction . 
the focus of this study was on variability and the resulting impact on margins ; still , as far as they are comparable , the numbers reported are in rough agreement with our results from transperineal imaging . in our study , shifts of about 0.4 mm in prostate position were detected for every 1 mm shift in probe position . 
for a typical shift of 5 to 10 mm of the probe towards the patient ( in comparison to the position of initial contact of the probe and the perineum ) , this corresponds to 2 to 4 mm shift of the prostate . 
hence , our result for clinical purposes is in good quantitative agreement with the two studies referenced above . no rotations of the target volume due to perineal probe pressure were observable . 
deformations and rotations of the prostate due to probe pressure require further investigation and are subject of a future study focusing on dosimetric impact . as the positioning of the ultrasound probe in the longitudinal direction is used as a proxy for its pressure on the perineum , any movements of the patient in the craniocaudal direction would introduce an error in this respect . 
the millimeter precision of routine clinical patient placement and quality assurance is a good benchmark in this case and substantially smaller than the 5 mm steps and 25 mm range covered in this experiment . 
most of the time , the prostate is located close to the isocenter . deviations in the caudal direction ( where the ultrasound head exerts pressure against the perineum ) are limited to 2 mthere is a small yet signicant ( p = 0.0014 ) systematic trend of 0.075 mm per minute as the compressed tissue of the perineum relaxes and pushes the prostate in the cranial direction . 
if more pressure is applied , the distortion of surrounding tissue becomes pronounced and risk organs ( such as the penile bulb ) may be moved closer to the highdose area around the prostate . on the other hand , a benecial effect of mechanically stabilizing intrafraction motion has been reported , e . 
this would have to be conrmed in a different study through intrafraction measurements at different pressure levels . as a nal remark , the availability of transperineal ultrasound has re - ignited the interest for ultrasound - based igrt at our institution . 
transperineal ultrasound image guidance is routinely employed during both planning ct and , in combination with cbct , during prefraction patient positioning . transperineal ultrasound image guidance is also routinely employed to monitor intrafraction motion of the prostate and to trigger treatment interruptions and table corrections whenever the displacement becomes too large . 
the only remaining effect is that there may be a net intrafraction drift of the prostate due to relaxation of the compressed tissue between probe and prostate , but this can be monitored by intrafraction imaging . finally , during this investigation , it became apparent that it is advisable to nd a good compromise of sufcient probe pressure for optimal image quality while keeping the necessary probe pressure constant throughout planning and treatment . 
it is more accurate , far less prone to user bias , allows keeping the probe pressure consistent between fractions , can remain in place during the fraction to avoid pressure bias , and provide intrafraction monitoring and correction . as transperineal ultrasound is expected to see increasing clinical use , the understanding of the inuence of probe pressure on target shift , target drift and risk organ displacement and tissue compression is of growing importance . 
in contradiction to some manufacturer recommendations , we have found that intermediate , rather than maximal , pressure levels ensure an optimal image quality while avoiding risk organ displacement and tissue compression . 
we have shown that probe pressure levels can be quantied by the longitudinal probe position , and this can be employed to keep pressure levels consistent between scanning ct and treatment fractions . 
together with automated scanning and the much more controlled placement of the ultrasound probe in comparison to transabdominal imaging , this greatly reduces bias and uncertainty during ultrasound - guided radiotherapy of the prostate . acknowledgements we thank andrea beisel , gabriela danilkiewicz , sandra kohlhauser , and anja weber for their excellent technical assistance . funding funding for research with the clarity system has been received from elekta . 
elekta was not involved in and had no inuence on the study design , the collection , analysis , or interpretation of data , on the writing of the manuscript or the decision to submit the manuscript for publication . compliance with ethical guidelines conict of interest elekta germany supports research at the university hospital of ludwig - maximilians - universitt , chaired by professor belka . 
ballhausen declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
a total of 154 patients with pn1 pca were treated with wprt ( 39 in an adjuvant setting ) and 23 years of androgen deprivation therapy ( adt )  . 
kaplanmeier analysis was performed to estimate biochemical recurrence - free survival ( brfs ) , clinical progression - free survival ( cpfs ) , and prostate cancer - specic survival ( css )  . 
multivariate analysis identied electronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 016 - 1094 - 5 ) contains supplementary material , which is available to authorized users . ( cid : 2 ) filip poelaert , md lip.poelaert@uzgent.be 1 department of urology , ghent university hospital , de pintelaan 185 , 9000 ghent , belgium 2 department of radiation oncology , ghent university hospital , ghent , belgium 3 department of urology , az nikolaas , sint - niklaas , belgium 4 department of radiation oncology , university hospitals leuven , leuven , belgium 5 department of radiology , ghent university hospital , ghent , belgium having only 1 positive lymph node , a shorter time between diagnosis and plnd , and older age as independent favorable prognostic factors for biochemical and clinical recurrence . 
bone metastases were the most frequent location of pca relapse ( n = 32 , 64% )  . conclusions patients with pn1 pca treated with wprt and 23 years adt have an encouraging 5 - year css . 
understaging of the disease extent may be the most important enemy in denitive pn1 pca treatment . keywords lymph node metastases prostate cancer radical prostatectomy radiotherapy survival analysis bestrahlung des gesamten beckens beim nodal metastasierten prostatakarzinom onkologisches outcome und prognostische faktoren zusammenfassung ziel das ziel dieser studie war es , das onkologische outcome der bestrahlung des gesamten beckens ( wprt ) beim histologisch gesicherten nodal metastasierten prostatakarzinom zu untersuchen , die lokalisation eines eventuellen rezidivs zu charakterisieren und mgliche prognostische faktoren zu identizieren . methoden alle patienten , bei denen seit dem jahr 2000 eine pelvine lymphknotendissektion ( plnd ) durchgefhrt worden war , wurden eingeschlossen . 
zur bestimmung des biochemischen rezidivfreien intervalls ( brfs ) , des klinischen progressionsstrahlenther onkol ( 2017 ) 193 : 444451 freien berlebens ( cpfs ) und des prostatakarzinom - spezischen gesamtberlebens ( css ) wurden kaplan - meieranalysen durchgefhrt . 
mgliche prognostische faktoren wurden mittels uniund multivariater regressionsanalyse identiziert . ergebnisse das brfs wurde fr ein beobachtungsintervall von 5 jahren auf 67 % , das cpfs auf 71 % und die css auf 96 % geschtzt . 
nur 1 positiver lymphknoten , eine kurze zeit zwischen diagnose und plnd und hheres alter waren in der multivariaten analyse gnstige prognostische faktoren bezglich eines biochemischen oder klinischen rezidivs . die anzahl der positiven lymphknoten war ein prognostischer faktor fr das css ( hr 1 , 34 [ 1 , 171 , 54 ] ) und das gesamtberleben ( hr 1 , 22 [ 1 , 101 , 36 ] )  . 
das achsenskelett war die hugste lokalisation eines pca - rezidivs ( n = 32 , 64 % )  . schlussfolgerung das 5 - jahres - css bei patienten mit nodal metastasiertem prostatakarzinom , die mit wprt und 23 jahren adt behandelt werden , ist erfreulich hoch . 
die unterschtzung des ausmaes der erkrankung knnte der wesentlichste adverse faktor bezglich einer guten langzeitprognose bei der behandlung von patienten mit nodal metastasiertem prostatakarzinom darstellen . schlsselwrter lymphknotenmetastasen prostatakarzinom radikale prostatektomie radiotherapie berlebensanalyse introduction the introduction of prostate specic antigen ( psa ) resulted in stage migration of prostate cancer ( pca )  . 
however , patients diagnosed with pelvic lymph node metastases ( n1 ) were historically considered to have incurable disease and received immediate palliative androgen deprivation therapy ( adt ) [ 1 , 2 ]  . 
plnd pelvic lymph node dissection , pn1 pathological pelvic lymph node metastasis , wprt whole pelvis radiotherapy , ebrt external beam radiotherapy , pca prostate cancer on pathology could be benecial compared to not performing rp in these patients [ 35 ]  . 
several authors suggest that , in n1 pca , adding adjuvant radiotherapy ( rt ) results in better oncological outcomes compared to adt alone [ 6 , 7 ]  . denitive local treatment with curative intent in patients with pathological n1 ( pn1 ) pca is therefore gaining interest [ 8 ]  . data on primary rt of pn1 pca patients are scarce [ 9 , 10 ]  . 
in the primary treatment of high - risk pca with rt , there is consensus on the long - term ( 23 years ) addition of adt [ 12 ]  . 
in n1 pca , however , information about whether adt can be discontinued is lacking , as most of these patients are treated with life - long adt [ 35 , 7 , 13 , 14 ]  . 
the question also arises whether performing rp in pn1 patients is still even necessary , given the known possible side effect of rp and the suggested need for adjuvant rt [ 15 ]  . the goal of this study is to investigate the oncological outcome of pn1 pca patients treated with wprt in the current clinical setting , evaluate the location of relapse , and identify potential prognostic factors . patients and methods patient selection at a single tertiary care center , all pca patients undergoing pelvic lymph node dissection ( plnd ) between january 2000 and january 2016 were evaluated . 
a total of 51 and 117 patients , respectively , had conrmed pn1 pca on pathology . patients not receiving primary wprt or adjuvant wprt ( in case of primary rp ) were excluded ( n = 14 )  . 
the study was approved by the local ethics committee ( uzg2011 / 495 )  . pelvic lymph node dissection lymph node dissection was advised in all pca patients with increased risk of nodal involvement undergoing primary treatment with curative intent . 
the risk was considered as increased when 15% based on the roach formula ( 2 / 3 psa + ( gleason score 6 ) 10 ) [ 16 ]  . 
the intraoperative frozen section was abandoned because of the possible survival benet suggested when continuing rp in pn1 pca [ 3 , 4 ]  . radiation therapy technique patients were treated with intensity - modulated radiotherapy . 
in the primary setting a median dose of 67 gy was delivered in 25 fractions to the prostate , resulting in a median equivalent dose in 2 gy fractions of 80 gy , calculated with an / of 1.5. 
in the adjuvant setting , the prostate bed received a median dose of 72 gy with an elective pelvic lymph node irradiation up to 48 gy , both delivered in 36 fractions . 
start of adjuvant wprt was only delayed in case of postoperative sequelae . adt using lhrh agonist or antagonist was started following the diagnosis of pn1 pca , before the start of wprt . in case of refusal or intolerance to lhrh agonists , bicalutamide 150 mg was administered . 
adt was discontinued after 23 years as standard policy in our institution . follow - up and outcome patients were followed in the outpatient clinic every 3 months during the rst year , biannually until 5 years , and annually thereafter . 
if this occurred after completion of the course with adt , adt was restarted at discretion of the treating physician or patients were treated with metastasis - directed therapy ( mdt ) if applicable [ 18 ]  . 
in addition to descriptive statistics , for study population , operation , and outcome characteristics , comparative statistics were performed using the mannwhitney utest for comparison of continuous variables and the 2 test , or fishers exact test where appropriate , for categorical variables . 
kaplanmeier survival analysis was performed to assess biochemical relapse - free survival ( brfs ) , clinical progression - free survival ( cpfs ) , prostate cancer - specic survival ( css ) , and overall survival ( os )  . 
potential prognostic factors assessed were age , bmi , initial psa , prostate volume , clinical tnm stage , gleason score / grade group [ 19 ] , lymph node yield , extranodal extension , number of positive lymph nodes , operation characteristics , time to plnd , time to wprt and rp or not . 
median initial psa was 16 ( iqr 938 ) , 92 patients ( 60% ) had clinical t34 disease and 114 patients ( 74% ) were grade group of 3 or more ( table 1 )  . patients treated with adjuvant wprt were younger ( p = 0.007 ) , had a lower initial psa ( p < 0.001 ) , and lower clinical tumor stage ( p = 0.002 ) compared to the primary wprt group . 
brfs biochemical recurrence - free survival , cpfs clinical progression - free survival , css prostate cancer - specic survival , os overall survival table 2 location of relapse after wprt for pn1 pca . 
a total of 32 patients ( 21% ) died during follow - up : 17 ( 11% ) due to pca , 5 ( 3% ) due to other malignancies , and 10 ( 7% ) of other causes . estimated median time to pca death after clinical relapse was 44 months ( 95%ci 4246 )  . during follow - up , clinical progression was observed in 50 patients ( 32% )  . 
in this study we report a brfs of 67% , cpfs of strahlenther onkol ( 2017 ) 193 : 444451 table 3 independent prognostic factors for cancer relapse and survival after wprt for pn1 pca brfs p value cpfs p value p value time to plnd time to wprt number n + n + > 1 vs . 
we systematically performed an elaborate analysis of the outcome of consecutive pn1 pca patients treated with wprt in the search for potential prognostic factors . nevertheless , the monocentric retrospective nature of this study , we were able to perform a more detailed analysis due to this monocentric aspect . 
the differences in patient / tumor characteristics of our study with other historical studies show the need for this contemporary study . the 2016 guidelines of the european association of urology acknowledge the potential of maximal local treatment for pn1 pca by recommending to offer pelvic external irradiation in combination with immediate long - term adt for clinical n1 pca . 
expectant management is legitimate in a patient after extended plnd when < 2 nodes show microscopic involvement with a psa < 0.1 ng / ml and absence of extranodal extension [ 2326 ]  . 
our research conrms the risk of the number of positive nodes , with < 2 nodes showing its value for brfs and cpfs [ 2729 ]  . however , extranodal extension did not seem to harbor additional prognostic information and the cutoff of < 2 seems to be arbitrary because of the strength of the number of positive nodes as a continuous variable in predicting css and os . we show that after clinical relapse , median time to pca mortality was 44 months . 
this shows the potency of current secondary ( hormonal ) treatments and the potential of mdt . interestingly , we also found that older age was associated with longer brfs and cpfs . 
given the fact that older patients have worse os , this adds evidence to the importance of performing an elaborate assessment of health status and comorbidities in geriatric pca patients before starting active therapy with curative intent . as all patients in this study are high - risk pca patients , all of them received appropriate metastatic screening with at least ct abdomen and bone scan but only 34% of these pn1 patients were cn +  . 
we show that the risk for disease relapse is lower when the time to plnd is shorter , possibly indicating that further spreading to locations outside the wprt target volume could be prevented . 
maybe some patients already harbor small bone metastases ( that are invisible to current staging modalities ) and are therefore undertreated by limiting the treatment focus to the pelvis . the strict line between pn1 pca and pm1 disease may therefore be one that could be fading in the future with increasing use of mdt . 
on the other hand , given the known side effects of adt , this might reduce late complications of continuous testosterone depletion in patients with complete pca remission [ 30 ]  . 
also the prognostic power of the number of positive lymph nodes may indicate that in case of multiple involved lymph nodes , the disease has already ( microscopically ) spread beyond the pelvis to retroperitoneal nodes and thus remains undertreated . 
correlation between the number of removed nodes and positive nodes found may confound the association between number of removed nodes with survival , like the will rogers phenomenon in pn0 disease [ 24 ]  . in previous reports , we elaborated on the ( additional ) shortand long - term sequelae of hypofractionated rt to the pelvic lymphatics [ 17 , 31 ]  . 
although toxicity seems 450 strahlenther onkol ( 2017 ) 193 : 444451 minimal and manageable and severe toxicity is rare , an increase in acute grade 2 rectal toxicity was observed which should be kept in mind in patient counseling . 
one might argue that rp is not necessary in n1 pca since the possibility of primary wprt ( including irradiation of the prostate )  . first , we observed upgrading of tumor characteristics on the pathology report of rp . 
performing rp makes full examination possible of the primary tumor , thus , making classication more accurate . second , because of differences in characteristics between our adjuvant and primary wprt group , direct comparison of outcomes must be avoided . 
but the most important factor why comparison of long - term outcome is impossible , is the difference in median follow - up due to the change in practice based on the possible survival benet suggested by retrospective studies when continuing with rp in pn1 pca [ 3 , 4 ]  . 
however , we could nd a noteworthy number of 10 local relapses ( 8.7% ) in the primary wprt group , indicating thateven with contemporary radiation doses and concomitant adtpart of these aggressive tumors still harbor radioresistance in the tumor bulk of the prostate . performing rp with adjuvant rt could therefore be benecial to reduce possible local pca relapse [ 10 , 32 ]  . finally , we are the rst to acknowledge the factor of time to surgery and wprt in outcome analysis of pn1 pca treatment . 
the benecial effect seen of a longer time to wprt in os ( not in css ) is a novel association we currently have no interpretation for and this has to be validated by other research . 
however , this nding confutes the argument that rp could delay start of wprt with a negative effect on css and os . these ndings could be possible reasons to not abandon rp , and we suggest that rp may continue to play a role as a rst step in the maximal treatment of pn1 pca to achieve denitive local disease control . 
therefore , longer follow - up studies with appropriate study design are needed to validate this hypothesis . conclusions patients with pn1 pca have an encouraging 5 - year css when treated with wprt and 23 years of adt . 
having only 1 positive lymph node , a shorter time between diagnosis and plnd , and older age were independent favorable prognostic factors for biochemical and clinical recurrence . the number of positive lymph nodes was prognostic for css and os . 
wegen der relevanz fr die american society of clinical oncology ( asco ) hat diese die astro - leitlinie anhand standardisierter kriterien einer kritischen prfung unterzogen . methode die astro - leitlinie zur bestrahlung von glioblastomen wurde hinsichtlich ihrer entwicklungsstrke untersucht . 
ein untersttzendes gremium der asco aktualisierte die literaturrecherche und berprfte inhalt und empfehlungen . ergebnisse das asco - gremium entschied , dass die empfehlungen der astro - leitlinie , die 2016 verffentlicht wurden , klar und fundiert sind und auf aktueller wissenschaftlicher evidenz basieren . 
die asco besttigt die astro - leitlinie zur strahlentherapie von glioblastomen und ergnzte einige qualizierende anmerkungen . empfehlungen eine fraktionierte teilhirnbestrahlung in kombination mit konkomitantem und adjuvantem temozolomid ist die standardtherapie nach biopsie oder resektion bei patienten bis zum alter von 70 jahren mit neu diagnostiziertem glioblastoma multiforme . 
eine hypofraktionierte originalpublikation sulman ep , ismaila n , armstrong ts , et al ( 2017 ) radiation therapy for glioblastoma : american society of clinical oncology clinical practice guideline endorsement of the american society for radiation oncology guideline . 
durch sorgfltige methodische prfungen folgen die empfehlungen hchster erhltlicher evidenz . die empfehlung nach stupp [ 1 ] , patienten bis 70 jahre mit teilhirnbestrahlung und konkomitantem und adjuvantem temozolomid zu behandeln , erscheint gut nachvollziehbar . 
zwei zielvolumenkonzepte werden akzeptiert : erstens das in amerika eher gebruchliche zweistuge konzept mit initialem grovolumigen klinischem zielvolumen 514 strahlenther onkol ( 2017 ) 193 : 513514 unter einschluss von dem und sicherheitssaum ( dosis hier 4446 gy ) und sequenziellem boost bis 60 gy auf kontrastmittelanreichernde areale bzw . 
die resektionshhle und zweitens das eher europische einstuge konzept mit 60 gy auf resektionshhle / kontrastmittelanreichernden resttumor mit sicherheitssauschwieriger ist die evidenz bei lteren patienten ( > 70 jahren ) , und entsprechend wird die leitlinie hier etwas vager . 
welche art der hypofraktionierung ( 13 2 , 67 gy , 10 3 , 4 gy oder 5 5 gy ; [ 24 ] ) zu bevorzugen ist , bleibt allerdings offen . 
interessant und widersprechend zur leitlinie der deutschen neuroonkologischen arbeitsgemeinschaft ( noa ; [ 5 ] ) ist , dass die hinzunahme von temozolomid eher nicht allein vom mgmt - promotorstatus abhngig gemacht wird , sondern vom allgemeinzustand des patienten . 
kurz erwhnt wird , dass bevacizumab keine vorteile in der primrtherapie [ 68 ] bringt und eine rebestrahlung bei rezidiven trotz fehlender prospektiver randomisierter daten eine option darstellt . fazit insgesamt ist die aktuelle leitlinie der astro / asco eine gute grundlage fr klinische entscheidungen , auch wenn aufgrund mangelnder evidenz in vielen fllen erheblicher subjektiver entscheidungsspielraum fortbesteht . 
der stellenwert alternierender elektrischer felder [ 9 ] wird in der leitlinie leider nicht diskutiert , da die daten hierzu erst nach juli 2016 publiziert wurden . clemens seidel und rolf - dieter kortmann , leipzig interessenkonikt c . 
stupp r , mason wp , van den bent mj et al ( 2005 ) radiotherapy plus concomitant and adjuvant temozolomide for glioblastoma . n engl j med 352 : 987996 2 . 
malmstrm a , grnberg bh , marosi c et al ( 2012 ) temozolomide versus standard 6 - week radiotherapy versus hypofractionated radiotherapy in patients older than 60 years with glioblastoma : the nordic randomised , phase 3 trial . 
roa w , brasher pma , bauman g et al ( 2004 ) abbreviated course of radiation therapy in older patients with glioblastoma multiforme : a prospective randomized clinical trial . 
roa w , kepka l , kumar n et al ( 2015 ) international atomic energy agency randomized phase iii study of radiation therapy in elderly and / or frail patients with newly diagnosed glioblastoma multiforme . 
chinot ol , wick w , mason w et al ( 2014 ) bevacizumab plus radiotherapy - temozolomide for newly diagnosed glioblastoma . n engl j med 370 : 709722 7 . 
herrlinger u , schfer n , steinbach jp et al ( 2016 ) bevacizumab plus irinotecan versus temozolomide in newly diagnosed o6 - methylguanine - dna methyltransferase nonmethylated glioblastoma : the randomized glarius trial . 
stupp r , taillibert s , kanner aa et al ( 2015 ) maintenance therapy with tumor - treating elds plus temozolomide vs temozolomide alone for glioblastoma : a randomized clinical trial . 
on the basis of laboratory observations , the lower single dose would be expected to be more effective . patients and methods a total of 127 patients suffering from painful heel spur were randomized : patients in the standard group were treated with single fractions of 6 1 gy twice a week , while the experimental group was treated with single fractions of 12 0.5 gy three times a week . patients who did not show satisfactory pain relief after 12 weeks were offered re - irradiation with the standard dose . the studys primary endpoints were pain relief and quality of life . 
there was no signicant difference between the groups concerning the results of a visual analogue scale ( vas ) , calcaneodynia score ( cs ) , and the somatic scale of the 12 - item author contributions b . 
niewald is the principal investigator of this trial , enrolled the patients , performed follow - up examinations , supervised the data acquisition and evaluation , and corrected the manuscript . 
a fractionation schedule of 12 0.5 gy was not superior to the current standard dose of 6 1 gy . further trials are necessary to explore the best fractionation schedule . keywords radiotherapy calcaneal spur pain quality of life analgesia strahlentherapie des fersensporns mit 2 fraktionierungsschemata ergebnisse einer randomisierten multizenterstudie nach 48 wochen follow - up ( cid : 2 ) prof.dr.med. 
5 , 40225 dsseldorf , germany 3 department of radiotherapy , university hospital of regensburg , franz - josef - strau - allee 1 , 93053 regensburg , germany 4 department of radiooncology and radiotherapy , university hospital of mainz , langenbeckstr . 
1 , 55131 mainz , germany institute of medical biometrics , epidemiology and medical informatics , saarland university hospital , kirrberger str.1 , 66421 homburg , germany 484 strahlenther onkol ( 2017 ) 193 : 483490 zusammenfassung hintergrund in dieser randomisierten multizenterstudie wurde der effekt einer niedrigen einzeldosis von 0 , 5 gy hinsichtlich schmerzen und lebensqualitt mit demjenigen einer standarddosis von 1 , 0 gy verglichen , dies bei konstanter gesamtdosis von 6 gy . 
nach laborergebnissen war eine berlegenheit der niedrigen einzeldosis zu erwarten . patienten und methodik es wurden 127 patienten randomisiert einerseits in die standardgruppe mit 6 fraktionen 1 , 0 gy 2 - mal pro woche , andererseits in die experimentelle gruppe mit 12 fraktionen von 0 , 5 gy 3 - mal pro woche . patienten mit ungengendem ansprechen nach 12 wochen wurde eine zweite strahlentherapieserie mit der standarddosis angeboten . 
es fand sich kein signikanter unterschied zwischen den gruppen hinsichtlich der ergebnisse auf einer visuellen analogskala ( vas ) , des calcaneodynie - scores und des somatischen teils des sf - 12 - fragebogens . 
weitere studien zur festlegung der optimalen einzeldosis sind notwendig . schlsselwrter strahlentherapie fersensporn schmerz lebensqualitt analgesie background in 1900 , on the basis of radiological ndings , plettner described the presence of a bony heel spur on the medial surface of the calcaneus at the insertion spot of the plantar aponeurosis [ 1 ]  . 
showed that low - dose radiotherapy in the range of 0.61.25 gy reduced nitric oxide ( no ) production and inducible nitric oxide synthetase ( inos ) - protein expression in stimulated macrophages . 
furthermore , single doses of 0.51 gy were associated with a reduction of tgf - 1 induced ccl - 20 - chemokine expression and reduced adhesion of granulocytes to endothelial cells [ 14 ]  . 
activator protein - 1 ( ap - 1 ) shows a biphasic induction and transcriptional activity with a rst relative maximum at 0.3 gy , followed by a decrease at doses between 0.5 and 1 gy and a subsequent increase again at 3 gy [ 15 ]  . 
expression of x - linked apoptosis inhibitor ( xiap ) in activated ea.hy926 endothelial cells exhibited a relative maximum at doses of 0.5 gy and 3 gy and a minimum of apoptotic cell death at 0.5 gy [ 16 ]  . 
after low - dose radiation , large et al . showed discontinuous expression and enzymatic activity of glutathione peroxidase ( gpx ) in ea.hy926 and human dermal microvascular endothelial cells ( hmvec )  . 
reported increased levels of hemioxigenase - 1 ( ho - 1 ) with a maximum at single doses of 0.5 gy and 1 gy in mice [ 19 ]  . based on these ndings , we conducted a clinical prospective randomized multicenter trial in order to explore and compare the analgesic effects of the ( at that time ) standard single dose of 1 gy with a reduced dose of 0.5 gy using a uniform total dose of 6 gy . 
in addition , we investigated the effects on quality of life . strahlenther onkol ( 2017 ) 193 : 483490 patients and methods in order to participate in this study , the following inclusion criteria were required : clinical evidence of a painful plantar heel spur with a persistence of symptoms for over 6 months radiological proof of the spur on a plain lateral radiograph of the heel favorable general health status age 40 years excluded from this trial were patients showing : previous radiation therapy to the concerned foot trauma to the foot area rheumatic disease arterial or venous diseases lymphatic edema of the concerned foot / leg pregnancy , breastfeeding severe psychotic disorders the use of analgesics before and during this trial was not limited , nor was former refractory treatment . 
standard dose group : single doses of 1 gy applied twice weekly up to a total dose of 6 gy ( irradiation on monday and thursday or tuesday and friday ) 2 . 
experimental dose group : single doses of 0.5 gy applied three times a week up to a total dose of 6 gy ( irradiation on monday , wednesday , and friday ) patients who did not show satisfactory pain relief after the rst radiotherapy series were offered a re - irradiation treatment after 12 weeks with the current standard dose of 6 1 gy . follow - up examinations were performed every 6 weeks up to 48 weeks after radiation , based on our retrospective experience that the vast majority of benecial effects become apparent after less than 1 year . 
the target volume included the calcaneus and the plantar aponeurosis . the results of a previous trial published by niewald et al . [ 7 , 22 ] were the basis for the calculation of the number of patients necessary : 120 patients were required in each therapy arm for a duration of 48 weeks in order to detect a difference of 15% in the vas and cs with a power of 80% and an error probability of 5% including a calculated drop - out rate of 10% in each therapy arm . categorical variables were compared using the chisquare test and fishers exact test . 
statistical signicance was set at p ( cid : 2 ) 0.05. statistical analysis was performed using medlog ( parox , mnster , germany ) and spss statistics ( version 22 ; ibm , armonk , n.y. ) by the statistician after 12 and 48 weeks of follow - up . 
a detailed trial protocol to this study as well as the rst results after 12 weeks followup have been published elsewhere [ 5 , 23 ]  . results a total of 127 patients were randomized : 111 patients were treated at the saarland university medical center , 11 patients were treated at the university hospital of regensburg , and ve patients were treated at the university hospital of mainz . 
in all , 52 patients of the standard dose group and 49 patients of the experimental dose group could be followed - up for 48 weeks . the comparison of patient groups as well as the results after 12 weeks follow - up have been published by niewald et al . 
vas ( 48 ) , cs ( 48 ) , sf - 12 ( 48 ) : values after 48 weeks of follow - up vas : linear scale ; 0 = no pain ; 100 = maximum imaginable pain ; improvement = negative difference ; worsening = positive difference cs : linear scale based on criteria such as pain , use of aids , problems at work , in daily life , or sports , gait ; 0 = maximum pain and disability ; 100 = complete freedom of symptoms ; improvement = positive difference ; worsening = negative difference sf - 12 : complex scales using 12 items on quality of life ; improvement = positive difference ; worsening = negative difference doctor : evaluation was performed either by doctor , student , or patients close acquaintance cs calcaneodynia score , sf - 12 12 - item short - form health survey , vas visual analogue scale strahlenther onkol ( 2017 ) 193 : 483490 corresponded well to those concerning pain relief . 
48 weeks follow - up a further benet was detected when comparing the published results after a follow - up period of 12 weeks [ 23 ] with the results after 48 weeks . 
the parameters for quality of life compared well with the results of pain evaluation . here , too , no statistically signicant differences were found ( see table 2 for details )  . results following re - irradiation after 48 weeks follow - up a total of 28 patients underwent re - irradiation . 
of these , patients who had undergone re - irradiation experienced an insignicant difference concerning pain relief compared with patients who showed a good response to radiation therapy from the beginning . 
patients with re - irradiation beneted signicantly more than those without . based on the laboratory ndings described in the previous section , the aim of this study was to compare the analgesic effects of a lower single dose of 0.5 gy with a standard single dose when using the same total dose . 
at the time this study was planned and the protocol was prepared , the standard dose in the therapy of plantar heel spur was 6 gy applied in two fractions of 1 gy per week given over 3 weeks . in this study we could not nd any statistically signicant differences after 48 weeks follow - up concerning pain relief between the groups . 
concerning quality of life , the results in general correspond well to those concerning pain relief ; however , one parameter ( psychic scale , doctors judgment ) showed statistically signicant differences that cannot be reasonably explained by the authors . in the meantime , during the enrolment and follow - up period , a new standard for the radiotherapeutical treatment of painful heel spur was established with a total dose of 3 gy applied in two fractions per week with single doses of 0.5 gy for a duration of 3 weeks [ 24 ] , according to the results of heyd et al . 
 [ 26 , 27 ]  . owing to the fact that we did not nd any benets in escalating single doses of 0.5 gy to a total dose of 6 gy , we support the current standard dose . 
laboratory in vitro results , indicating a clinical benet of lower single doses , can obviously not be directly translated into improved clinical pain relief . the authors are well aware of the limitations of this clinical trial . 
second patients had undergone second irradiation series , error bars standard error , sf - 12 12 - item short - form health survey theless , a placebo effect is still under discussion . 
published a double - blinded study in 1970 , showing a benet in pain relief in 60% of patients in both groups , whether they were irradiated or not [ 28 ]  . 
the study has been criticized for lacking clearly dened endpoints and because of the irradiation in the acute stage of the disease without considering that there might be spontaneous pain remission . 
a trial comparing three different therapy schedules was performed by seegenschmiedt et al . the group irradiated with 10 0.5 gy ( total dose of 5 gy ) showed the best results in pain relief compared with the groups receiving 10 0.3 gy ( total dose of 3 gy ) and 12 1 gy ( total dose of 12 gy ) [ 3 ]  . 
however , these trials did not compare a uniform total dose . in this trial , we showed that patients who did not benet from the primary radiation therapy may benet at a statistically signicant level when irradiated again after 12 weeks . this underlines the results of a publication by hautmann et al . , who showed that patients benet from re - irradiation [ 29 ]  . 
in our trial , the results after 48 weeks followup concerning pain relief are comparable to those of patients showing a good response after the rst irradiation . therefore , re - irradiation can be recommended . 
comparing the results after 12 weeks follow - up [ 23 ] with those after 48 weeks follow - up , it can be concluded that the main effects on pain relief occur in the rst 12 weeks but continue to improve for a period of up to 48 weeks . conclusion once again , low - dose radiation therapy for painful heel spur ( plantar fasciitis ) showed its efciency concerning pain relief . 
single doses of 1 gy keeping a uniform total dose of 6 gy did not show a statistically signicant benet in our setting with a limited patient number . further randomized prospective trials using the new standard of a 3 - gy total dose will be necessary to explore the best fractionation schedule . compliance with ethical guidelines conict of interest b . 
brunner1 , 5 , 6 received : 17 august 2016 / accepted : 6 january 2017 / published online : 30 january 2017 springer - verlag berlin heidelberg 2017 abstract background stereotactic body radiotherapy ( sbrt ) in pancreatic cancer can be limited by its proximity to organs at risk ( oar )  . 
in this analysis , we evaluated the toxicity and efcacy of two different treatment approaches in patients with locally recurrent or oligometastatic pancreatic cancer . materials and methods according to the prescription method , patients were divided in two cohorts ( c1 and c2 )  . the planning target volume ( ptv ) was created through a 4 mm expansion of the internal target volume . 
in c2 , a subvolume was additionally created , a simultaneous integrated protection ( sip ) , which is the overlap of the ptv with the planning risk volume of an oar to which we prescribed a reduced dose . electronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 017 - 1099 - 8 ) contains supplementary material , which is available to authorized users . ( cid : 2 ) e . 
3 , 79106 freiburg im breisgau , germany 2 department of hematology , oncology and stem - cell transplantation , university medical center freiburg , freiburg , germany 3 department of general and visceral surgery , university medical center freiburg , freiburg , germany 4 division of medical physics , department of radiation oncology , university medical center freiburg , freiburg , germany 5 german cancer consortium ( dktk ) , heidelberg ( partner site freiburg ) , germany faculty of medicine , university of freiburg , freiburg , germany results in all , 18 patients were treated ( 7 with local recurrences , 9 for oligometastases , 2 for both )  . 
one patient in c2 experienced grade 3 acute toxicities and 1 patient in c1 experienced a grade 3 late toxicity . conclusion the sip approach is a useful prescription method for abdominal sbrt with a favorable toxicity prole which does not compromise local control and overall survival despite dose sacrices in small subvolumes . keywords local progression radiation therapy overall survival prognosis toxicity stereotaktische strahlentherapie ( sbrt ) beim wiederkehrenden oder oligometastatischen pankreaskarzinom bewertung der toxizitt bei simultan integrierter protektion ( sip ) versus konventioneller sbrt zusammenfassung hintergrund die stereotaktische strahlentherapie ( sbrt ) ist bei pankreaskarzinomen durch die enge lagebeziehung der risikoorgane ( oar ) zum zielvolumen erschwert . 
in dieser analyse evaluierten wir die toxizitt und die lokalkontrolle von zwei unterschiedlichen therapiestrategien bei patienten mit rezidivierendem oder oligometastatischem pankreaskarzinom . 434 strahlenther onkol ( 2017 ) 193 : 433443 material und methoden die patienten wurden anhand der verschreibungsmethode in zwei kohorten geteilt ( c1 und c2 )  . 
das planungszielvolumen ( ptv ) wurde durch eine expansion des internen zielvolumens ( itv ) um 4 mm erzeugt . in c2 wurde zustzlich ein subvolumen ( simultan integrierte protektion , sip ) deniert , welches durch die berlappung des ptv mit dem planungsrisikovolumen ( prv ) eines oar generiert wurde , um die grenzdosen fr das jeweilige oar einhalten zu knnen . ergebnisse insgesamt 18 patienten wurden behandelt ( 7 lokalrezidive , 9 oligometastasen , 2 kombiniert )  . 
bei einem medianen follow - up von 12 , 8 monaten lag das mediane berleben bei 13 , 2 monaten ( 95 %kondenzintervall [ ki ] 9 , 814 , 6 )  . 
die lokalkontrolle fr das gesamtkollektiv betrug nach 6 und 12 monaten jeweils 93 % und 67 % ( 95 % - ki 1536 ) ; sie war statistisch nicht unterschiedlich zwischen den beiden gruppen . 
ein patient in c2 entwickelte eine akute grad4 - toxizitt und 1 patient in c1 entwickelte eine grad - 4spttoxizitt . schlussfolgerung die sip - verschreibungsmethode ist eine hilfreiche strategie bei der sbrt mit einem gnstigen nebenwirkungsprol . 
trotz der dosisreduktion in kleinen subvolumina waren die lokale kontrolle und das gesamtberleben identisch . schlsselwrter lokale progression strahlentherapie gesamtberleben prognose toxizitt introduction pancreatic cancer has a devastating prognosis with 5 - year survival rates of 7% [ 1 ]  . 
surgical excision is the treatment choice with a 5 - year survival rate of approximately 20% , but resection is only possible in 1520% of patients [ 2 , 3 ]  . 
published data suggest that stereotactic ablative radiotherapy ( sbrt ) could be an alternative approach to chemoradiotherapy ( crt ) for locally advanced pancreatic cancer ( lapc ) with promising local control ( 4894% at 12 months ) [ 412 ]  . 
furthermore , reported local control for the treatment of hepatic metastases with sbrt ranges from 7595% at 1 year and 6090% at 2 years [ 13 , 14 ]  . with regard to toxicity , published data show an excellent acute tolerance but late gastrointestinal toxicity is dose - limiting [ 4 , 15 , 16 ] because of the close proximity to critical organs . 
some authors introduced risk adaptive strategies , dependent on the location of the tumor , with reduced dose to the entire planning target volume ( ptv ) [ 15 ] , while others prioritized the duodenal dose constraints over all other organs and accepted dose reductions to the total ptv [ 11 ]  . by reducing the dose to the entire ptv , a severely reduced tumor control probability ( tcp ) has to be assumed as the price for lower normal tissue complication probability ( ntcp )  . 
in order to overcome the problem without reducing the dose to the whole ptv , we developed a novel prescription method termed simultaneous integrated protection ( sip ) for quantiable and comparable dose prescription to targets close to dose - limiting structures [ 18 ]  . 
we compared two cohorts without ( c1 ) and with ( c2 ) simultaneous integrated protection ( sip ) for hollow organs in the vicinity of the target volumes . materials and methods patient selection this single institutional retrospective analysis was approved by the ethics board of the university medical center . 
patients eligible for this study had histologically proven pancreatic adenocarcinoma ( pdac ) , had been deemed to be surgically or medically inoperable , and were discussed in a multidisciplinary board . 
a complete staging evaluation with physical examination , positron emission computed tomography ( pet / ct ) or magnetic resonance imaging ( mri ) of the abdomen and ct thorax was performed prior to therapy . 
treatment was according to our institutional standard operating procedures and in analogy to a planned single center phase i trial developed to test the toxicity prole of the sip approach [ 18 ]  . sbrt techniques patients were immobilized in supine position in a high precision customized vacuum cushion ( bluebag bodyfix , innovative technologies vlp , innsbruck , austria ) using abdominal compression during 4d - ct ( brilliance ct big bore , philips medical systems , cleveland , oh , usa ) or 4d - pet - ct ( gemini tf bigbore , philips medical systems , cleveland , oh , usa )  . 
the internal target volume ( itv ) was created accounting for the extent and the position of the tumor in all motion phases in three dimensions using the 4d image data . 
all hollow visceral organs were expanded isotropically by 4 mm to demarcate volumes of increased risk of high dose exposure hier steht eine anzeige . 436 strahlenther onkol ( 2017 ) 193 : 433443 fig . 
ptv : total planning target volume ( 104 cm3 ) , prv planning risk volume , ptvsip : subvolume of the ptv with overlap of the prv that was prescribed a reduced dose ( 21 cm3 ) , ptvdom : subvolume of the ptv without overlap with the prv ( planning risk volume , prv )  . 
the dose in the ptvsip was required to be as high as possible within the constraints to avoid local relapse . treatment planning was performed using either oncentra masterplan ( nucletron bv [ elekta ] , veenendaal , netherlands ) or eclipse ( varian medical systems , palo alto , ca ) treatment planning systems . patients were treated every other day with 312 fractions , depending on the proximity to oars . 
three fraction regimens were preferred in patients with lesions away from critical structures , 12 fraction regimens were preferred in patients with intimate contact to bowel structures , and 5 fraction regimens were intermediate in terms of closeness to the bowel . 
2 consort diagram ( lapc locally advanced pancreatic cancer , not primarily resected , lr local recurrence , om oligometastases ) patients were examined clinically at least once per week during treatment by radiation oncologists . 
during followup , complete history , physical examination , and imaging ( cts , mris , or pet - cts ) were acquired every 3 months . toxicity was scored using the national cancer institute common terminology criteria for adverse events v . 
4.03. toxicities reported within 3 months after treatment completion were considered acute ; any toxicity thereafter was considered to be late . statistical analysis end points were toxicity assessment and freedom from local progression ( fflp ) at 1 year ; the latter was dened as the absence of progressive disease within the ptv , as well as overall survival . 
lesions that developed or progressed outside the ptv , in the same organ , were scored as local out of eld progression and those developed in other organs as distant progression . survival and control times were calculated from the start of sbrt . 
time to progression and survival were evaluated with the kaplanmeier method and multivariate analysis using the cox proportional hazards model and logistic regressions at a statistical signicance level of p ( cid : 2 ) 0.05 ( two sided )  . 
nine patients were treated for local progression or recurrence after resected pdac ( 3 and 6 patients , respectively ) , two of whom had an additional solitary metastasis ( liver )  . 
twelve patients were diagnosed with oligometastatic disease prior to treatment and 16 received systemic therapy prior to sbrt . patients in the c1 group received a median total physical dose to the ptv of 35 gy ( 3040 gy ) , with a median bed10 of 60 gy ( range 4584 gy ) and a median eqd210of 50 gy ( range 3870 gy )  . 
the median ratio of ptvsip / ptv was 438 in - field local strahlenther onkol ( 2017 ) 193 : 433443 out of field local progression distant progression number 23 at risk 100% fig . 
a total of 14 patients had chemotherapy after sbrt and 3 patients had no further chemotherapy , data were missing in 1 patient . after treatment , patients were routinely examined physically and received a ct or mri every 3 months . 
of the 23 lesions treated , 18 did not progress and 5 progressed in - eld at a median interval of 7.7 months ( range 6.613.7 months ) after therapy . 
neither use of the sip technique ( p = 0.757 , log - rank ) , nor prior metastases , ptv volume , physical dose , eqd210 , d95% , d90% d02 , dmean , or corresponding eqd210 for ptv , ptvsip , ptvdom were signicant for local control ( table 2 )  . 
the median bed10 for the lesions that progressed was 67 gy ( range 5386 gy ) and the median bed10 for the sip subvolumes was 57 gy ( range 5457 gy ) and the median bed10 for the survival toxicity at the time of the analysis 7 of the 18 patients had died , 5 from progressive disease and 2 from other causes . 
one patient suffered from abdominal pain ctc grade 1 after the rst fraction ( 1 9 gy ) and subsequently fractionation was changed to 10 4 gy every other day . 
one patient ( c2 ) suffered from an occlusive ileus ( ctc grade 3 ) during radiotherapy due to tumor compression requiring a stent which resulted in strahlenther onkol ( 2017 ) 193 : 433443 table 2 a . 
no radiationinduced liver disease occurred . discussion during the past years , several prospective and retrospective trials have tested the efcacy of sbrt in the treatment of lapc with 115 fractions ( 425 gy single doses ) corresponding to an eqd210 of 31.25204 gy and a bed10 of 37.5244.8 gy [ 5 ]  . 
most acute toxicities were mild but several studies raised concerns due to a signicant rate of gastrointestinal toxicities ( ulcerations , bleedings , and perforations ) [ 20 ]  . 
the frequency of high - grade gastrointestinal toxicities ( grade 3 ) rises over time [ 6 ] and ranges from 023 ( median 7% )  . these are the rst published data reporting toxicity and outcomes with the novel sip prescription technique described by brunner et al . 
thus , we concluded that the mechanical ileus was due to tumor inltration and the gastrointestinal bleeding probably through the manipulation due to prior stenting of the duodenum a few days before . 
 [ 4 ] demonstrated a dose - dependent relationship of duodenal toxicity after single fraction therapy concluding that the multiple dosevolume histogram endpoints and a lyman ntcp model are strongly predictive of duodenal toxicity . 
linear regression lines indicated grade 2 and grade 3 toxicity frequencies of 5% at 65 gy and 80 gy eqd23 , respectively . several attempts were made to reduce the incidence of late toxicities . 
 [ 11 ] prioritized the duodenal dose constraints and accepted dose reductions in order to keep at least 50% of the duodenum near the ptv under the 50% dose and only 5% of the duodenum was allowed to receive 95% of the dose . 
the group reported a median os of 20 months , although this was calculated from the time rwigema ( 2011 [ 27 ] ) 24median 130median 48%@12 m g3 4% strahlenther onkol ( 2017 ) 193 : 433443 table 4 published local control and toxicity reports author ( year ) fractionation eqd23 bed3 gurka ( 2014 [ 24 ] ) koong et al . 
furthermore , we could show an encouraging overall survival ( os ) of 13.8 months in a patient collective with an unfavorable prognosis due to tumor recurrence and / or the presence of metastases at the time of treatment . 
the median os in the sbrt series without metastases ranges from 5.720 months ( median 14.4 months ) from diagnosis and 6.414.3 months ( median 11 months ) from radiotherapy ( table 4 )  . 
this group of patients with prolonged survival have a higher risk of developing late morbidities so that a calculated treatment approach is important in order to reduce the appearance of late toxicities but also to intensify treatment . conclusion the sip treatment approach is a useful adaptive prescription method which tailors the dose to each tumor , with a favorable toxicity prole , while respecting normal tissue constraints . 
based on these data , we are now conducting a phase 1 prospective study in patients with oars adjacent to the ptv using the sip concept . compliance with ethical guidelines conict of interest e . 
treatment was as follows : concurrent adt plus rt , 33 patients ( 19% ) ; neoadjuvant and concurrent adt plus rt , 91 patients ( 52% ) ; rt only , 51 patients ( 29% )  . 
required couch shifts without rotations were recorded for each megavoltage ( mv ) cone beam computed tomography ( cbct ) scan , and corresponding alignment shifts were recorded as leftright ( x ) , superiorinferior ( y ) , and anteriorposterior ( z )  . 
pearsons correlation coefcient was used to measure the correlation of couch shifts between groups . mean prostate shifts and standard deviations ( sd ) were calculated and pooled to obtain mean or group systematic error ( m ) , sd of systematic error ( ) , and sd of random error ( )  . results no signicant differences were observed in prostate shifts in any direction between the groups . 
random and ( cid : 2 ) cem onal , md hcemonal@hotmail.com faculty of medicine , adana turgut noyan research and treatment centre , department of radiation oncology , baskent university , 01120 adana , turkey systematic errors for all patient cohorts and adt groups were similar . conclusion hormone therapy given concurrently with rt was not found to signicantly impact setup errors . 
prostate volume was signicantly correlated with shifts in the anteriorposterior direction only . keywords radiotherapy , image - guided fiducial markers prostate - specic antigen organs at risk toxicity einuss der androgendeprivationstherapie auf kongurationsfehler bei der externen strahlentherapie des prostatakarzinoms zusammenfassung ziel ziel war zu untersuchen , ob kongurationsfehler bei der externen radiotherapie ( rt ) des prostatakarzinoms durch die kombination aus androgendeprivationstherapie ( adt ) und rt beeinusst werden . material und methoden retrospektiv wurden die daten von 175 wegen eines prostatakarzinoms behandelten patienten ausgewertet . 
die therapie erfolgte als gleichzeitige adt plus rt , 33 patienten ( 19% ) ; neoadjuvante und gleichzeitige adt plus rt , 91 patienten ( 52% ) ; rt allein , 51 patienten ( 29% )  . 
die erforderlichen verschiebungen der patientenliege ohne rotation wurden fr jede megavoltcone - beam - computertomographie ( mv - cbct ) - aufnahme dokumentiert und die entsprechenden verschiebungen im rahmen der ausrichtung erfasst als linksrechts ( x ) , superiorinferior ( y ) und anteriorposterior ( z )  . 
gruppenbezogenen systematischen fehler ( m ) zu erhalten , die sd des systematischen fehlers ( ) und die sd des zufallsfehlers ( )  . ergebnisse es wurden keine signikanten unterschiede bei den prostataverschiebungen jeglicher richtung fr alle gruppen festgestellt . 
eine signikante positive korrelation wurde zwar , unabhngig von der adt - gruppe , zwischen dem prostatavolumen und der prostataverschiebung in z - richtung beobachtet ( r = 0 , 19 ; p = 0 , 04 ) , nicht aber zwischen dem volumen der verschiebung in xoder y - richtung ( r = 0 , 04 ; p = 0 , 7 ; r = 0 , 03 ; p = 0 , 7 )  . 
das prostatavolumen war nur signikant mit verschiebungen in richtung anteriorposterior korreliert . schlsselwrter radiotherapie , bildgesteuerte referenzmarker prostataspezisches antigen risikoorgane toxizitt radiotherapy ( rt ) plays an important role in prostate cancer treatment , either administered postoperatively for highrisk patients or as a denitive treatment , with or without hormone therapy . 
successful delivery of prescribed radiation doses , while sparing surrounding tissues including the rectum and bladder , requires the ability to accurately target the prostate [ 1 , 2 ]  . image - guided rt ( igrt ) has been used to improve the accuracy of rt delivery in prostate cancer , but previous studies have revealed prostate motion variability . 
however , these earlier studies evaluated differences in patient setup without the use of image guidance and estimated treatment margins using the combined error of multiple predictive factors [ 3 , 4 ]  . 
as the position of the prostate may vary substantially between treatment fractions , and possibly even during treatment , methods for more precise localization of the prostate are needed [ 5 , 6 ]  . 
using mvcbct , daily localization of the prostate immediately before treatment can improve the accuracy of treatment delivery ; however , this also increases the time per session , workload , and integral radiation dose [ 13 ]  . the standard treatment protocol for intermediateto high - risk prostate cancer patients is rt in combination with androgen deprivation therapy ( adt )  . 
prior studies have also found that adt decreases prostate volume through cytoreduction in patients with locally advanced disease [ 18 , 19 ] and may impact ducial marker migration [ 20 , 21 ]  . 
the question arises whether adt may increase prostate motion due to prostate volume reduction , which may result in bigger setup errors . the purpose of this study was to assess whether setup errors might be inuenced by the combination of adt and rt . 
given that adt and rt have both been previously found to induce prostate shrinkage , this study aimed to analyze whether these factors in combination might result in increased prostate motion and more setup errors during materials and methods patient population the clinical and dosimetric data of 175 prostate cancer patients treated with denitive rt between september 2012 and december 2013 were retrospectively analyzed . 
among these , 33 patients ( 19% ) received concurrent adt plus rt , 91 patients ( 52% ) had neoadjuvant and concurrent adt plus rt , while 51 patients ( 29% ) were treated with rt alone . 
patients were stratied according to the damico criteria into three categories based on pretreatment serum prostate specic antigen ( psa ) , clinical stage , and biopsy - based gleason score ( gs )  . 
these three categories were the following : low - risk ( psa < 10 ng / ml and ct1ct2a and gs ( cid : 2 ) 6 ) ; intermediaterisk ( psa = 1020 ng / ml or ct2b or gs = 7 ) ; and high - risk ( psa > 20 ng / ml or clinical stage ct2c or gs 8 ) [ 22 ]  . patient simulation and radiotherapy planning prior to rt , each patient underwent a planning ct . 
patients were scanned from the top of the rst lumbar vertebral body to below the lesser trochanters using a slice thickness of 2.5 mm with an optima 580 ct scanner ( ge healthcare , waukesha , wi , usa )  . 
patients were instructed to have empty bowels and a comfortably full bladder during simulation and treatment , as described previously [ 23 ]  . 474 strahlenther onkol ( 2017 ) 193 : 472482 table 1 patient characteristics characteristic age ( years ) ; median ( range ) psa ( ng / ml ) ; median ( range ) t stage t1ct2c t3at3b gleason score risk group intermediate high none neoadjuvant + concurrent concurrent treatment eld prostate sv pelvic lymphatics + prostate + sv no . 
the patients were marked with anterior , right , and left lateral permanent skin markers according to isocenter coordinates . the clinical target volume ( ctv ) included the prostate only in low - risk patients , versus the prostate and seminal vesicles in intermediateand high - risk patients . 
the planning target volume ( ptv ) was dened as the ctv with a 5 mm posterior margin and 8 mm margins in all other directions [ 24 ]  . 
atlas - based lymph node ( ln ) delineation was performed and ln - ctvs were created using radiation therapy oncology group ( rtog ) guidelines [ 25 ]  . organs at risk ( oars ) included the rectum , sigmoid , bladder , and femoral heads . 
the femoral heads were contoured to the level of the ischial tuberosities . plans were calculated with the monaco treatment planning system ( elekta ltd , crawly , uk ) using the monte carlo algorithm and a sliding window multileaf collimator ( mlc ) delivery technique . 
according to the patient risk group , the prescribed dose was 78 gy to the prostate the seminal vesicles and 54 gy to the pelvic lymphatics delivered in 39 fractions . cone beam ct and positioning patient motion was assessed retrospectively ofine for 2330 cbct images obtained from 175 patients . 
some datasets were lost because of imaging system down time . before each treatment , patients were positioned supine as described above , and their skin markers were aligned using three lasers in the treatment roocbct was performed daily for the rst 5 consecutive days and then twice per week , even if the average shift was less than 5 min case of larger shifts , replanning was performed and patients were treated with the new plans . 
using three degrees of freedom , the prostate was aligned in three dimensions in the cbct and planning ct studies by a physician at each setup for the rst 3 to 5 days , and thereafter by trained radiation therapists . 
after delivery of each cbct , manual alignment of the prostate ( cbct - p ) was recorded using the prostate , seminal vesicles , rectum , and bladder contours , as delineated on the reference simulation ct , and the required couch shifts were recorded , without use of rotations . 
in order to minimize the effect of rectal lling on prostate displacement , the anteriorposterior rectal diameter was kept to less than 2.53.0 cm as measured on the cbct taken before treatment . 
after the rst 5 fractions , the shifts recorded for each patient were used to calculate the mean error on three axes , which was then implemented on all subsequent treatment axes . 
rotational corrections were found to be insignicant and were therefore ignored in this study . the corresponding shifts in alignment were recorded in leftright ( x ) , superiorinferior ( y ) , and anteriorposterior ( z ) directions . statistical analysis statistical analysis was performed using spss 20.0 software ( spss for window , ibm corp . , armonk , ny , usa )  . patients were stratied according to adt protocol : neoadjuvant and concurrent adt ( nc ) , concurrent ( c ) , and rt only ( r )  . 
the mean and standard deviation ( sd ) of prostate shifts were calculated and then pooled to obtain mean or group systematic error ( m ) , sd of systematic error ( ) , and sd of random error ( ) , as previously described [ 29 ]  . 
is calculated from the sd of the average shifts for the patient cohort , is the root mean square of the sds of the shifts for all patients , and m is the average value over all fractions and all patients . 
the magnitude of the prostate shifts in the x direction measured during the rst 5 days was signicantly larger in the nc group compared to the r ( p = 0.001 ) and c ( p = 0.03 ) groups ( table 2 )  . 
prostate shifts in the x and y directions were not signicantly correlated with prostate volume ( r = 0.04 , p = 0.7 for x direction ; r = 0.03 , p = 0.7 for y direction )  . 
there were no substantial differences in calculated margins in the x , y , and z directions between adt groups . discussion initiated in this study it was found that adtstarted either concurrently with rt , 3.2 months before and continuing during rthad no impact on setup errors during prostate rt . signicant additionally , adt did not affect random or systematic errors calculated from cbct data . 
1 daily prostate shifts in leftright ( x ) , superiorinferior ( y ) , and anteriorposterior directions ( z ) for ( a ) all patients , ( b ) for patients treated with radiotherapy only , ( c ) for patients treated with radiotherapy and concurrent androgen deprivation treatment ( adt ) , and ( d ) for patients treated with radiotherapy and adt given before radiotherapy 34 mm for all directions . 
prostate volume was found to be signicantly associated with prostate motion in the anteroposterior direction , which may be due to increased prostate motion because of rectal and bladder lling . successful delivery of the prescribed radiation dose to the prostate while sparing the rectum and bladder requires the ability to accurately target the prostate during treatment [ 2 ]  . 
the current standard of care involves acquisition of on - board volumetric cbct to generate a three - dimensional soft tissue - based registration with the planning ct [ 32 ]  . 
 [ 34 ] demonstrated that mv - ct images provided the most accurate treatment plans relative to kilovolt ( kv ) - ct - based planning , and the lower image resolution did not limit the visualization of small anatomical structures . 
in the current study , prostate shifts were assessed using mv - cbct , which enables better visualization of prostate position , as well as of rectal and bladder lling . the use of adt in combination with rt has been shown to contribute to improved therapeutic outcomes in patients with localized prostate cancer [ 15 , 16 , 3537 ]  . 
according to the national comprehensive cancer network ( nccn ) guidelines for prostate cancer risk , long - term adt lasting 23 years is indicated for patients with a high risk , whereas short - term adt lasting 46 months can be considered for those with an intermediate risk [ 38 ]  . 
first , the duration of neoadjuvant adt may affect prostate volume . during a course of adt , prostate volume can diminish strahlenther onkol ( 2017 ) 193 : 472482 fig . 
2 histogram of the vector displacement of the prostate for the entire cohort in ( a ) leftright , ( b ) superiorinferior , and ( c ) anteriorposterior directions continuously for several months , with volume reductions reported of up to 33% after an average of 3.7 months of adt [ 19 , 40 ]  . 
however , in this study , it was found that the combined patient setup and prostate motion error remains , on average , basically similar for the three different treatment conditions : rt alone , adt started approximately 3 months before rt , and adt initiated concurrently with external rt . 
these variations in position may be associated with changes in bladder or rectal lling during treatment [ 41 ]  . image guidance during external rt is used to reduce random and systematic errors . 
 [ 44 ] also demonstrated that obtaining ofine correction after analyzing the rst ve images was the most optimal strategy ; however , daily online image allowed to simulate the ofine correction protocol easily to derive residual errors . 
 [ 45 ] demonstrated that with ofine corrections after the rst 5 fractions , unacceptably high residual errors still existed in a study with 638 mv - cbct images of 30 patients . 
 [ 46 ] found that 8 mm prostate displacements after skin mark alignment were observed in 13 , 5 , and 44% of all fractions in the lateral , longitudinal , and vertical directions , respectively . 
the difference between average displacements in all fractions and the running averages in the x , y , and z directions showed a convergence to a plateau in prostate shifts to within 0.5 and 1 mm relative the external marks after 510 fractions . 
based on these results , a small number of image - guided treatment fractions at the beginning of the rt course should therefore be sufcient to signicantly reduce the systematic error . 
4 box and whisker plots demonstrating average prostate shifts according to neoadjuvant androgen deprivation therapy in ( a ) leftright , ( b ) superiorinferior , and ( c ) anteriorposterior directions minimize surrounding normal tissue radiation doses due to larger ptvs , rearrangement of ctvptv margins is essential after determining the systematic and random errors , which may result in excessive normal tissue irradiation . otherwise , daily image guidance is essential for adequate target coverage with minimal margins [ 45 , 47 , 48 ]  . 
furthermore , they initiated dose escalation using a simultaneous integrated boost to intraprostatic lesions with 4 mm margins , with daily cbct . the dosimetric data were published elsewhere [ 23 ] and the clinical outputs will be published soon . previous studies have demonstrated that interand intrafractional prostate motion occurs primarily in the anteroposterior direction and , secondarily , in superiorinferior directions , which may be the result of changes in bladder or rectal lling , or perhaps attributable to contraction of the pelvic muscles [ 41 , 49 ]  . 
in contrast , in the current study , no signicant changes in prostate motion were found within the entire cohort , except for minor differences in prostate shifts in the x direction measured in the rst 5 days in the nc group compared to the other groups . 
in order to reduce random errors in prostate position , several methods to reproduce daily bladder and rectal position were reported with different results [ 45 , 50 , 51 ]  . 
for minimizing the effects of bladder and rectal lling on prostate displacement , in the present study , not only was the prostate checked , but it was also checked that the bladder was full and the rectum empty . patients did not receive treatment if the anteriorposterior 480 strahlenther onkol ( 2017 ) 193 : 472482 table 3 estimates of random ( ) , systematic ( ) , and group systematic ( m ) errors for the leftright ( x ) , superiorinferior ( y ) , and anteriorposterior ( z ) directions and margins calculated according to van herk et al . 
however , patients were treated using the vmat technique , which uses shorter treatment times and is therefore possibly associated with less intrafractional organ movement compared to other techniques [ 52 ]  . conclusion this study conrms that adt used before and / or during external rt for prostate cancer patients has no signicant impact on prostate shifts detected using cbct . 
additionally , in order to minimize setup errors during prostate rt , it was found that the systematic and random components of errors must be calculated , and corrections should be applied for the systematic component . 
additional studies are needed to conrm whether adt affects setup errors in prostate cancer rt , and long - term follow - up with clinical ndings is required to identify other potential effects of adt . r radiotherapy only , nc neoadjuvant and concurrent , c concurrent , m group systematic error , standard deviation of systematic error , standard deviation of random error compliance with ethical guidelines rectal diameter was greater than 2.53.0 cm , as measured on cbct taken before treatment . 
both systematic and random errors can be reduced by this method . this method can be of great value in treatments involving large doses per fraction and when targets lie close to critical structures for which irradiation may have unacceptable toxicity . 
after the rst 5 fractions , images were reviewed , and the systematic and random components of errors were calculated and corrections applied for the systematic component . this study has some limitations . 
although it would be ideal to acquire more cbct data for precise determination , cbct was not performed at each fraction out of consideration for the total exposure to ionizing radiation . 
this article is an open access publication . abstract purpose the antiapoptotic b - cell lymphoma 2 ( bcl2 ) gene is a key player in cancer development and progression . a functional single - nucleotide polymorphism ( c . - 938c > a , rs2279115 ) in the inhibitory p2 bcl2 gene promoter has been associated with clinical outcomes in various types of cancer . 
ein funktioneller einzelnukleotid - polymorphismus ( c . - 938c > a , rs2279115 ) im inhibitorischen p2 - bcl2 - promotor wurde mit dem klinischen outcome verschiedener krebserkrankungen verknpziel der vorliegenden studie war die untersuchung der rolle von bcl2 - 938c > a - genotypen fr die mortalitt bei patienten mit prostatakarzinom . methoden der zusammenhang zwischen bcl2 - 938c > agenotypen ( rs2279115 ) und dem outcome bei prostatakrebs wurde in der prospektiven procagene - studie , die 702 patienten mit prostatakarzinom umfasste , untersucht . ergebnisse whrend der medianen nachbeobachtungszeit von 92 monaten starben 120 ( 17 , 1 % ) patienten . 
in einer univariaten cox - regressionsanalyse zeigte sich ein signistrahlenther onkol ( 2017 ) 193 : 466471 kanter zusammenhang zwischen dem cc - genotyp und einer schlechteren krebsspezischen ( ccs ; hazard ratio [ hr ] 2 , 13 ; 95 % - kondenzintervall [ ki ] 1 , 104 , 12 ; p = 0 , 024 ) und gesamtberlebensrate ( os ; hr 2 , 34 ; 95 % - ki 1 , 583 , 47 ; p < 0 , 001 )  . 
in einer multivariaten cox - regressionsanalyse , die das alter bei diagnose , die risikogruppe sowie die androgendeprivationstherapie beinhaltete , blieb der cc - genotyp ein signikanter vorhersagemarker fr ein schlechteres ccs ( hr 2 , 05 ; 95 % - ki 1 , 053 , 99 ; p = 0 , 034 ) und os ( hr 2 , 25 ; 95 % - ki 1 , 513 , 36 ; p < 0 , 001 )  . schlussfolgerung die vorliegenden daten zeigen , dass der homozygote bcl2 - 938 - cc - genotyp bei patienten mit prostatakarzinom mit dem css und os assoziiert ist . schlsselwrter apoptose genetik polymorphismus onkogen strahlentherapie apoptosis or programmed cell death is an evolutionarily conserved and highly organized mechanism of cell suicide for maintaining cellular homeostasis and removing senescent or potentially hazardous cells [ 1 ]  . 
impaired apoptosis has been related to development and progression of various cancer types [ 2 ]  . b - cell lymphoma 2 ( bcl - 2 ) family proteins are essential regulators of apoptosis and comprise both proand antiapoptotic members [ 3 ]  . 
these promoters have different functions , with p2 decreasing the activity of p1 promoter function [ 4 ]  . bcl2 itself seems to act as both an oncogene and a tumor suppressor gene in different tumor types [ 5 ]  . 
in prostate cancer , the role of bcl2 expression in disease progression is currently not fully understood : stackhouse and coworkers reported a positive correlation between bcl2 tumor staining and biochemical recurrence in prostatectomy specimens , but not in prostate biopsies [ 6 ]  . 
anvari and coworkers reported an association of high bcl2 expression with higher gleason scores ( gs ) and lower biochemical recurrence - free survival in patients with advanced prostate cancer undergoing androgen deprivation therapy ( adt ) [ 9 ]  . a functional single - nucleotide polymorphism ( c . - 938c > a , rs2279115 ) in the p2 promoter has been shown to inuence bcl2 expression . 
the bcl2 - 938c allele was signicantly associated with increased p2 promoter activity , resulting in decreased overall bcl2 transcriptional activity and protein expression [ 10 , 11 ]  . 
reported an association of the bcl2 - 938 aa genotype with a worse outcome of prostate cancer patients [ 11 ]  . aim of the present study was to test a possible association between bcl2 - 938c > a genotypes and prostate cancer outcome . materials and methods the austrian prostate cancer genetics ( procagene ) study includes 702 prostate cancer patients recruited between january 2004 and january 2007 . 
briey , procagene is a prospective study aimed at investigating genetic risk factors , functional relationships between genetic variations and clinical phenotypes , the genetically modied response to radiotherapy ( radiogenomics ) , and the prognostic importance of genetic markers such as genetic variants in regulators of dna repair , cell cycle , and apoptosis , including bcl2 - 938c > a genotypes [ 1621 ]  . participants of procagene were male patients with sporadic , histologically conrmed prostate cancers treated with radiotherapy . 
clinical characteristics were obtained from medical records and prostate cancer patients were stratied into low - , intermediate - , and high - risk groups according to the national comprehensive cancer network ( nccn ) guidelines [ 22 ]  . all patients underwent three - dimensional conformal radiotherapy for prostate cancer . 
a subgroup of patients ( n = 110 ) received postoperative radiotherapy using high - energy photons ( 18 mv ) in a conformal three - eld technique to treat the prostate bed . all elds were treated daily , 5 days / week . 
none of the included patients received pelvic node irradiation . a total of 454 patients ( 64.7% ) received neoadjuvant adt and 153 patients ( 21.8% ) were treated with additional adjuvant adt . 
the administration of systemic therapy for disease recurrence was at the discretion of the treating urologist and / or medical oncologist , and included hormonal treatment and / or chemotherapy . the study was performed according to the austrian gene technology act and was approved by the ethical committee of the medical university of graz ( ek 20 - 248 ex 08 / 09 )  . written informed consent was obtained from all participating subjects . 
genomic dna was prepared from whole blood using a silica membrane technology ( machery - nagel , nucleospin blood , germany )  . bcl2 genotypes were determined by uorogenic 50 exonuclease assays ( taqman ; thermo fisher scientic , pittsburgh , pa , usa ) with primer and probe sets designed and manufactured by applied biosystems ( life tech austria , vienna , austria ; assay id c___3044428_30 )  . 
results from the kaplanmeier analysis , as well as data from a previous study in prostate cancer patients , suggested a recessive effect of the bcl2 - 938c allele on survival [ 9 ]  . 
a cancer - specic survival : number of events and total numbers were 13 / 138 for the cc genotype , 24 / 348 for the ca genotype , and 9 / 215 for the aa genotype . 
b overall survival : number of events and total numbers were 38 / 138 for the cc genotype , 52 / 348 for the ca genotype , and 31 / 215 for the aa genotype cox regression model , css ( hr 2.13 , 95% ci 1.104.12 ; p = 0.024 ) and os ( hr 2.34 , 95% ci 1.583.47 ; p < 0.001 ) were signicantly reduced for the cc genotype ( table 2 )  . in a multivariate cox regression model including age at diagnosis , adt , and risk group based on psa level , gs , and t stage , the cc genotype remained a signicant predictor of poor css ( hr 2.05 , 95% ci 1.053.99 ; p = 0.034 ) and os ( hr 2.25 , 95% ci 1.513.36 ; p < 0.001 , table 2 )  . furthermore , an os analysis in subgroups stratied by tumor stage and hormonal treatment was performed . 
depending on tumor type and disease stage , as well as therapy , bcl2 seems to be able to act as both an oncogene and a tumor suppressor gene [ 5 ]  . 
the overall effect of the presumably low - expression bcl2 - 938 cc genotype resulted in strongly reduced survival rates in the present cohort of prostate cancer patients . in subgroup analyses stratied by tumor stage and hormonal treatment , the association of bcl2 cc genotype with os seemed to be strongest in the subgroup tumor stage 2 with hormonal treatment . 
nevertheless , sample sizes of these subgroups were small and 95% cis of hrs in different subgroups were overlapping ; thus these post - hoc ndings should be interpreted cautiously and require further replication . 
data from the present study do not provide a plausible functional explanation for the different effect sizes of the genotype in these subgroups . in the present study , as well as in other studies in european populations , the bcl2 - 938a allele is the common allele , whereas in asian and sub - saharan african populations the c allele is more common , indicating that the c allele is the ancestral allele and the a allele is the mutated allele . 
this study observed a recessive effect of the bcl2 - 938c allele on overall survival , with reduced survival in carriers of the homozygous cc genotype [ 11 ]  . 
the precise mechanism for this lack of a typical allele - dose effect remains to be determined . the present results are in contrast to those of bachmann et al . , who reported reduced survival in prostate cancer patients carrying the homozygous bcl2 - 938 aa genotype [ 11 ]  . 
g. , using bonferroni correction , reduces the rate of false - positive ndings , but at the same time reduces statistical power and increases the risk of false - negative results [ 26 , 27 ]  . 
in the current study , the authors have therefore deliberately decided to analyze only the bcl2 gene variant with the highest prior probability for a positive association with prostate cancer mortality . 
further bcl2 ( dis - ) regulation might be due other effects , such as de novo tumor mutations , which were not analyzed in the present study . conclusion this study provides evidence that the homozygous bcl2938 cc genotype is strongly associated with reduced os in prostate cancer patients . open access funding provided by medical university of graz . compliance with ethical guidelines conict of interest w . 
langsenlehner declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
a week after the procedure patients lled in a questionnaire regarding pain , dysuria , urinary frequency , nocturia , rectal bleeding , hematuria , hematospermia or fever symptoms caused by the implantation . 
pain was scored on a 110 scale , where score 1 meant very weak and score 10 meant unbearable pathe implanted gold markers were used for daily verication and online correction of patients setup during igrt . results based on the questionnaires no patient experienced fever , infection , dysuria or rectal bleeding after implantation . 
overall , 105 patients ( 35% ) reported less , 80 patients ( 27% ) more , and 94 patients ( 31% ) equal amount of pain during marker implantation compared to biopsy . 
the method can be performed safely in clinical practice . keywords image - guided radiotherapy fiducial markers safety complications local anesthesia transperineale implantation von goldmarkern fr die bildgesttzte perkutane strahlentherapie beim prostatakarzinom eine unizentrische prospektive studie zusammenfassung zielsetzung darstellung von machbarkeit und komplikationen der transperinealen implantation von goldmarkern bei mit perkutaner strahlentherapie ( igrt ) behandelten prostatakarzinompatienten . material und methoden zwischen november 2011 und april 2016 bekamen 300 patienten drei rntgendichte goldmarker unter transrektaler ultraschallkontrolle und lokalansthesie transperineal in die prostata implantiert . 
die patienten beantworteten 1 woche nach implantation einen fragebogen ber schmerzempnden , dysurie , harnausscheidungsfrequenz , nykturie , rektale blutung , hmaturie , hmatospermie oder fiebersymptome , verursacht durch die implantation . 
die implantierten goldmarker wurden zur tglichen kontrolle und online - korrektur bei der igrt genutzt . ergebnisse in den fragebgen berichtete kein patienten ber fieber , infektion , dysurie oder rektale blutung nach implantation . 
von 300 patienten hatten 12 ( 4 % ) hmatostrahlenther onkol ( 2017 ) 193 : 452458 spermien und 43 ( 14 % ) hmaturien , die jeweils 3 , 4 und 1 , 8 tagen andauerten . 
insgesamt 105 patienten ( 35 % ) berichteten ber weniger , 80 patienten ( 27 % ) ber mehr und 94 patienten ( 31 % ) ber gleich starke schmerzen whrend der implantation im vergleich zur biopsie . 
diese frage hatten 21 patienten , bei denen eine biopsie unter allgemeinansthesie durchgefhrt wurde , nicht beantwortet . schlussfolgerung die transperineale implantation von goldmarkern unter lokalansthesie wurde gut vertragen . komplikationen waren begrenzt ; rate und frequenz von perioperativ auftretenden schmerzen waren vergleichbar mit denen einer biopsie . 
die methode ist in der klinischen praxis sicher durchfhrbar . schlsselwrter bildgesttzte strahlentherapie goldmarker sicherheit komplikationen lokale ansthesie introduction there are a number of randomized trials conrming that radiation dose escalation for prostate cancer with external beam radiotherapy improves biochemical and clinical progression - free survival [ 14 ]  . 
using imageguided radiotherapy ( igrt ) , the geographical miss of the target can be minimized ; thus , higher dose can be delivered without increasing rectal toxicity [ 57 ]  . 
given the similarity between transrectal gold marker implantation and prostate biopsy most of implantations are made by urologists . the aim of our single institute , prospective study was to evaluate the rate of toxicities and complications after transperineal gold marker implantation performed by radiation oncologists for prostate igrt , without using prophylactic antibiotics . patients and methods this prospective study was approved by our institutional human ethical review board . 
under transrectal ultrasound guidance , through a transperineal template , two ducial markers were inserted bilaterally into the base of the prostate gland and the third marker was placed into the apex , in order to ensure adequate separation between the markers . 
the aim was to obtain good visibility on two x - ray images taken from anteriorposterior and lateral view . the treatment planning ct scan was performed at least 1 week after the marker insertion to allow for any edema or hemorrhage to settle . 
to evaluate the tolerance and the perior postoperative complications , prior to implantation every patient received a questionnaire about the pain , dysuria , urinary frequency , nocturia , rectal bleeding , hematuria , hematospermia , pain duration after the implantation , fever , and inammation symptoms caused by the implantation ( table 1 )  . 
the pain caused by the intervention was scored on a 110 scale , where 1 was a very weak and 10 was an unbearable pain . the survey inquired about the comparison of the pain caused by implantation to the pain caused by previous prostate biopsy . 
days yes / no by the day before the planning ct scan ( 710 days after the implantation )  . all patients underwent igrt with 3d conformal or intensity - modulated radiotherapy . 
because the prostate gland is not visible on standard portal images , patient positioning variabilities and prostate motion make it difcult to precisely locate the prostate and safely deliver maximal radiation dose . 
the use of intraprostatic radiopaque gold markers nowadays has become one of the standard techniques for daily setup correction in patients with prostate cancer undergoing igrt . considering the noninvasive alternatives for igrt , such as cone beam ct or three - dimensional ( 3d ) ultrasound of the prostate , it is essential to assess the safety and feasibility of gold marker implantation . 
the other modality for implanting markers is the transperineal approach , which can be performed by radiation oncologists with experience in prostate brachytherapy . to our knowledge , there are only two retrospective studies that reported complications and feasibility of transperineal marker implantation [ 15 , 16 ]  . in the study of henry et al . 
1 digitally reconstructed radiograph ( drr ) and kilovoltage a anteroposterior and b lateral images of set - up elds with three implanted markers 456 less pain more pain equal amount of pain fig . 
for pain classication , the wongbaker faces pain scale was used , in which patients were asked to rate the pain on a 05 scale with the visible help of six drawn faces with a range of expressions from smiling to crying [ 19 ]  . 
no periprostatic nerve block was applied . in an australian trial [ 20 ] using a transrectal technique , hematospermia occurred in 10% , hematuria in 13% , dysuria in 11% , obstruction in 5% of the 234 patients . 
in all , 22 patients ( 7.7% ) were treated for urinary infection with antibiotics after the procedure , while 8 patients ( 2.8% ) reported hospital admission for infective complications related to gold marker implantation [ 21 ]  . to our best knowledge , this study represents the rst prospective data on a large patient population about complications and side effects after transperineal gold marker implantation for prostate cancer igrt . 
in the present trial we paid particular attention to the personal discussion between the physician and the patient about every point on the questionnaire before the patient lled in the questionnaire at home . the most serious complication of gold marker implantation is bacterial sepsis . 
fluoroquinolone - resistant bacteria is responsible for 5090% of cases with infections after prostate biopsy . the use of broad - spectrum antibiotics is controversial , as its regular use leads to more resistance . 
however , none of the patient needed analgesics after the intervention due to this paour patients matched the pain that they experienced while going through prostate biopsy with the pain felt during the gold marker implantation . 
about one third of patients reported less , one third reported more , and one third reported equal amount of pain compared to biopsy . these data conrm the tolerability of marker implantation compared to prostate biopsy . 
according to our experience the main advantage of transperineal over transrectal goldplated marker implantation technique is the signicant decrease of the chance of rectal bleeding and inammation . conclusion transperineal gold marker implantation under local anesthesia was well tolerated . 
rates of other complications were also limited ; rate and frequency of perioperative pain were comparable to the pain caused by prostate biopsy . the method can be performed safely in routine clinical practice either by urologists or by radiation oncologists . compliance with ethical guidelines conict of interest k . 
polgr declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
april 2017 springer - verlag berlin heidelberg 2017 fragestellung und hintergrund die gegenwrtige standardtherapie plattenepithelialen analkarzinoms ( sccac ) besteht in einer sphinktererhaltenden simultanen radiochemotherapie ( rct ) mit 5 - fluorouracil ( 5 - fu ) und mitomycin - c ( mmc )  . 
eine progression tritt mit hherer wahrscheinlichkeit bei fortgeschrittenen stadien auf ( t34 und / oder lokoregionale lymphknotenmetastasen ) sowie bei tumoren mit anderer genese als infektion mit humanen papillomviren ( hpv )  . 
da sich beim sccac oft eine egfr - berexpression ( epidermal growth factor receptor ) ndet , wurde in der hier diskutierten phase - iistudie der zusatz von cetuximab untersucht [ 2 ]  . patienten und methodik eine rct mit cisplatin , 5 - fu und 8 wchentlichen dosen cetuximab erhielten 61 patioriginalpublikation garg mk , zhao f , sparano ja et al ( 2017 ) cetuximab plus chemoradiotherapy in immunocompetent patients with anal carcinoma : a phase ii eastern cooperative oncology group - american college of radiology imaging network cancer research group trial ( e3205 )  . 
ausgehend von einer erwarteten lokoregionalen rezidivrate von 35 % nach standardtherapie in 3 jahren wurde durch cetuximab eine halbierung der rezidivhugkeit erhofanfnglich begann die behandlung mit 2 zyklen neoadjuvanter chemotherapie ( cisplatin und 5 - fu )  . 
die strahlentherapie erfolgte mit einer dosis von 1 , 8 gy und 5 fraktionen pro woche ( minimum 45 gy ( t12 ) , maximum 54 gy )  . die inguinalen lymphknoten erhielten 30 , 6 gy ( n0 oder n1 ) bzw . 
box 1480 , 8092 bod , norwegen die ausschlielich simultane radiochemotherapie mit 5 - fu / mmc erlaubt bei der mehrzahl der patienten ( ca . strahlenther onkol ( 2017 ) 193 : 508509 80 % ) einen langfristigen sphinktererhalt , da sccac oftmals vollstndig auf die rct ansprechen [ 1 , 3 ]  . 
in der act - ii - studie lag sie 11 wochen nach therapiestart bei 52 % der patienten vor ( 71 % nach 18 wochen und 78 % nach 26 wochen ; [ 4 ] )  . in den meisten onkologischen situationen lsst der gegenwrtige behandlungsstandard noch luft nach oben . 
ob nicht vollstndig ansprechende oder im verlauf rezidivierende tumoren bereits primr so resistent sind , dass auch eine intensivere rct erfolglos bleibt , ist nicht abschlieend geklrt . die vorliegende phase - ii - studie prsentiert einen weiteren versuch , die lokoregionale rezidivrate zu reduzieren , allerdings ohne damit einen neuen standard denieren zu knnen . die compliance der patienten bei der simultanen chemound strahlentherapie beeinusst die lokoregionale kontrolle . 
und in der hier kommentierten studie wurde die simultane behandlung in 36 % der flle wegen hoher toxizitt unterbrochen , und zwar im median um 12 tage ( ! )  . 
in 12 % musste die behandlung fr mehr als 3 tage unterbrochen werden . die hier kommentierte amerikanische e3205 - studie ndert die gegenwrtige standardtherapie des sccac nicht , welche in einer sphinktererhaltenden simultanen radiochemotherapie mit 5 - fluorouracil und mitomycin - c besteht . carsten nieder , bod , norwegen interessenkonikt c . 
garg mk , zhao f , sparano ja et al ( 2017 ) cetuximab plus chemoradiotherapy in immunocompetent patients with anal carcinoma : a phase ii eastern cooperative oncology group - american college of radiology imaging network cancer research group trial ( e3205 )  . 
doll cm , moughan j , klimowicz a et al ( 2017 ) signicance of coexpression of epidermal growth factor receptor and ki67 on clinical outcome in patients with anal cancer treated with chemoradiotherapy : an analysis of nrg oncology rtog 9811 . 
yates a , carroll s , kneebone a et al ( 2015 ) implementing intensity - modulated radiotherapy with simultaneous integrated boost for anal cancer : 3 year outcomes at two sydney institutions . 
this single - institute study evaluates the benecial role of pbm - led in preventing / reducing rd during breast cancer rt . patients and methods of 70 consecutively treated patients , 25 patients were treated with pbm - led twice a week prior to adjuvant 3d conformal rt after breast - conserving surgery . 
w. goethe university , theodor - stern - kai 7 , 60590 frankfurt am main , germany 5 department of radiation oncology , otto von guericke university , leipziger strae 44 , 39120 magdeburg , germany a matched group ( n = 25 ) was generated from the control group based on propensity for potentially confounding variables . results in the pbm group , 22 patients ( 88% ) presented grade 1 and 3 ( 12% ) grade 2 rd . 
in the control group , 25 patients ( 55.6% ) developed grade 1 reactions , 18 patients ( 40% ) grade 2 , and 2 ( 4.4% ) patients grade 3 rd . concerning pain intensity , 15 patients ( 60% ) of the pbm treatment arm reported no pain , 5 patients ( 20% ) vas 2 , and 5 ( 20% ) vas 3 . 
in the control group , 13 patients ( 28.9% ) reported no pain , 2 ( 4.4% ) vas 1 , 7 ( 15.6% ) vas 2 , 9 patients ( 20% ) reported vas 3 , 12 ( 26.7% ) patients vas 4 , and 2 ( 4.4% ) patients vas 5 . conclusion pbm - led therapy applied prior to rt might be effective in decreasing the incidence and sequelae of radiation - induced skin toxicity in breast cancer patients treated with breast - conserving surgery . keywords photobiomodulation light - emitting diode ( led ) breast cancer radiation therapy radiodermatitis photobiomodulationstherapie zur behandlung strahlentherapieassoziierter dermatitis eine single - institut - beobachtung zur adjuvanten radiotherapie bei brustkrebspatientinnen nach brusterhaltender operation zusammenfassung hintergrund radiotherapie ( rt ) ist integrativer bestandteil der multimodalen therapie beim mammakarzinostrahlentherapieinduzierte hauttoxizitt ist dabei das hugste unerwnschte ereignis ; dennoch sind prvention und management der radiodermatitis ( rd ) weiterhin trivial . 
klini492 strahlenther onkol ( 2017 ) 193 : 491498 sche studien ergaben , dass die photobiomodulation ( pbm ) mit leuchtdioden ( led ) die wundheilung frdern und entzndungshemmend wirken kann . 
diese single - institut - studie untersucht die wertigkeit der pbm - led zur prvention und linderung der rd whrend der adjuvanten brustkrebspatienten und methoden von insgesamt 70 konsekutiv behandelten patienten wurden 25 patienten nach brusterhaltender operation 2 - mal wchentlich mit pbm - led vor adjuvanter 3d - rt behandelt . 
zustzlich wurde eine gematchte gruppe ( n = 25 ) aus der kontrollgruppe basierend auf der neigung fr potenzielle strvariablen gebildet . ergebnisse in der pbm - gruppe prsentierten 22 patienten ( 88 % ) eine grad - 1 - rd und 3 ( 12 % ) eine grad - 2 - rd . 
hinsichtlich der schmerzintensitt hatten 15 patienten ( 60 % ) der pbm - gruppe keine schmerzen , 5 ( 20 % ) vas 2 und 5 ( 20 % ) vas 3 . 
in der kontrollgruppe hatten 13 patienten ( 28 , 9 % ) keine schmerzen , 2 ( 4 , 4 % ) vas 1 , 7 ( 15 , 6 % ) vas 2 , 9 ( 20 % ) vas 3 , 12 ( 26 , 7 % ) vas 4 und 2 ( 4 , 4 % ) patienten vas 5 . schlussfolgerung pbm - led - therapie vor adjuvanter rt knnte die inzidenz und ausprgung von rd bei brustkrebspatientinnen nach brusterhaltender operation verringern . schlsselwrter photobiomodulation leuchtdioden ( led ) brustkrebs strahlentherapie radiodermatitis introduction radiation therapy ( rt ) is an essential part of breast cancer treatment , and for early stage mammary carcinoma , breastconserving surgery ( bcs ) followed by adjuvant rt represents the standard of care [ 13 ]  . 
in the case of external beam radiation therapy ( ebrt ) , conventional fractionated treatment lasts 56 weeks for whole breast irradiation ( wbi ) followed by a boost to the initial tumor bed , either using ebrt or interstitial brachytherapy [ 4 ]  . despite advancements in external beam radiation delivery , up to 90% of treated breast cancer patients develop radiodermatitis ( rd ) during and / or after their rt [ 57 ]  . rd usually develops gradually between the rst and fourth week of rt and remains and / or progresses during treatment with a reported time span of up to 4 weeks after completion of ebrt to heal completely [ 8 ]  . 
several extrinsic and intrinsic factors seem to inuence the incidence , severity , and timing of rd including total radiation dose , dose / fractionation scheme , irradiated volume , anatomical site / area , radiosensitivity of the involved tissue but also systemic treatments such as chemotherapy , immunotherapy and hormonal therapy [ 6 , 8 , 10 , 11 ]  . 
in the light of broadly accepted skin care guidelines [ 12 , 13 ] , the prevention as well as management of rd still remains trivial , mainly due to paucity of conclusive literature evidence regarding various topical as well as systemic agents , which can inform health professionals on effective management of radiation - induced skin toxicities [ 6 , 14 ]  . at this point , photobiomodulation ( pbm ) therapy using a light emitting diode ( led ) is gaining momentum as a promising prophylactic as well as therapeutic approach in the management of rd . 
the application of pbm for the management of postmastectomy lymphedema is corroborated by solid data [ 15 , 16 ] and clinical ndings now suggest a benecial impact on the prevention of radiationinduced oral mucositis [ 1720 ]  . from this perspective following the evoked academic interest concerning pbm , we conducted a single - institution study to evaluate the role of pbm as an additional measure to our institutions skin care protocol . 
the primary endpoint was to assess its clinical impact in the prevention and / or reduction of rd and second in ameliorating the symptom of pain associated with skin inammation . patients and methods eligibility criteria this single - institution analysis was performed as part of clinical routine , based on published clinical experiences [ 21 , 22 ] and on recently reported as well as current ongoing trials [ 23 , 24 ]  . 
table 1 depicts the characteristics of the all enrolled patients , including pre - ebrt and peri - ebrt administered systemic treatments . the study population consisted of 70 consecutive breast cancer patients , being treated in our institution from november 2015 to february 2016 . 
one patient group included 25 nonselectively chosen patients , receiving pbm during adjuvant ebrt ( pbm group ) and a control group consisting of the remaining patients ( n = 45 ) receiving rt without additional pbm . 
patients of all fitzpatrick skin types were enrolled [ 25 ] , as reported in table 1 . photobiomodulation procedure in all cases , informed consent was signed prior to pbm therapy application . 
patients treated with pbm received treatments using a 69 diode led cluster probe34 660 nm plus 35 850 nm , 1390 mw , class 2m led ( thor photomedicine ltd , chesham , buckinghamshire , united kingdom ) , fda approved for medicinal purposes . 
the application on these preset anatomical sites , encompassing the submammary fold and axilla , was limited to 60 s ( led probe of an outer diameter of 70 mm [ active area of 63 mm ] , applied at a preset cycle standard 100 pulse , with an average power density of 44.6 mw / cm2 , 250 ms per pulse at a uence of 0.15 j / cm2 ) summing up to a total treatment time of 45 min for each patient per treatment session . 494 reaction evaluation skin toxicity evaluation for all treated patients ( n = 70 ) was prospectively performed in accordance to the intradepartmental clinical practice , consisting of at least a weekly physical examination and ctcae v4.0 - based documentation [ 26 ] by the physicians attending the patients on a daily basis . 
for documentation and later rd evaluation purposes , photographs of the irradiated sites were taken weekly ( end of week ) throughout the course as well as at the end of treatment , which were compared and analyzed by two experienced , board certied , blinded to the procedure , independent radiation oncologists . 
the initiation as well as further usage of supportive treatments based on our institutions skincare protocol , consisting of palmitoylethanolamide cream for rd grade 1 ( upon dry desquamation , not for faint erythema ) and a phenol - methanal - urea - polycondensate cream for grade 2 , was noted for both groups . 
pain was documented weekly using a patient self - evaluation scalea visual analogue scale ( vas ) , recording pain intensity numerically ranging from 0 ( meaning no pain ) to 10 ( referring to unbearable pain ) [ 27 ]  . 
as a mean of minimizing interobserver variation , all members of our department involved in this study , attended a course involving study protocol , mainly focusing on rd grading . statistical analysis the primary endpoint of the study was rd grade and pain intensity . 
rd grading was based on photo documentation obtained at baseline , weekly during and at completion of rt course , and pain intensity from the self - evaluation scale at the end of ebrt . 
the secondary outcome measure of the study was the duration of supportive care obtained from the clinical grading ( ctc version 4.0 ) derived from the documented weekly performed physical examination through rt course . the comparative analysis was generated including all patients ( n = 70 ) , 25 patients constituting the pbm group and the remaining 45 patients forming the control group . 
in order to adjust for differences in clinical characteristics bestrahlenther onkol ( 2017 ) 193 : 491498 tween groups , we generated using the r package matchit for propensity matching [ 28 ] , a more homogeneous subgroup ( matched group , n = 25 ) from the control cohort matched to the pbm groups characteristics . 
the following criteria were taken into account : ( 1 ) breast volume , ( 2 ) pre - rt chemotherapy status , and ( 3 ) concurrent hormonal / antibody therapy . baseline characteristics of study groups were compared using the 2 test for categorical variables and the cochranmantelhaenszel test plus the wilcoxon rank sum test for continuous variables . 
distributions of skin reaction grades were compared using the cochranmantelhaenszel test , while pain intensity and supportive skin care duration for pbm treated , control and matched patients were compared by the wilcoxon rank sum test . 
regarding the control group ( n = 45 ) , 25 ( 55.6% ) developed grade 1 , 18 ( 40% ) strahlenther onkol ( 2017 ) 193 : 491498 of the allocated treatment in the pbm group . 
all patients treated enrolled in pbm group completed rt course without toxicity - associated interruptions compared to 2 patients ( 4.4% ) of the control group and 1 patient in the matched group , which were forced to interrupt rt due to severe skin reaction . 
2 illustrates the prevalence of rd grades between the groups at baseline , during the course , and upon completion of rt . pain intensity concerning rd - associated pain symptomatology , 15 patients ( 60% ) of the pbm group reported no pain at the end of rt , 5 patients ( 20% ) reported pain of vas 2 and 5 ( 20% ) of vas 3 . 
1 box plots reporting the patients distribution regarding a irradiated breast volume and b age in the pbm ( n = 25 ) , control group ( n = 45 ) and matched group ( n = 25 )  . 
2 graph depicting the prevalence of rd grade 1 , grade 2 and grade 3 at baseline , weekly during rt and upon completion of rt course , for the pbm group ( n = 25 ) , control group ( n = 45 ) , and matched group ( n = 25 )  . 
rd radiodermatitis , rt radiotherapy , pbm photobiomodulation , ctcae v4.0 common toxicity criteria for adverse events version 4.0 , g1 grade 1 , g2 grade 2 , g3 grade 3 496 strahlenther onkol ( 2017 ) 193 : 491498 discussion despite signicant advancements in rt techniques , rd comprises the major acute adverse event encountered by breast cancer patients during ebrt , often leading to a signicant decrease in quality of life or even to treatment interruption [ 57 ]  . 
several factors are known to affect the appearance and severity of rd including rt technique , breast size , irradiated volume , total and daily treatment dose , systemic therapy , extent of surgery , and skin radiosensitivity [ 6 , 8 , 10 , 11 ]  . 
however , despite the generally accepted skin care guidelines [ 12 , 13 ] , the prophylaxis and management of rd is not fully understood due to the scarce availability of high - quality evidence regarding agents used in clinical practice . at this point , pbm is gaining momentum as a promising prophylactic as well as therapeutic approach in the management of rd . 
in vivo and in vitro studies suggest that pbm of specic led pulse duration and uence upregulates procollagen synthesis and downregulates dermal matrix metalloproteinase expression , thus , mediating wound healing by depicting an anti - inammatory action through reduction of apoptosis and cellular necrosis [ 30 , 31 ]  . 
the benecial role of pbm as supportive modality in the management of postmastectomy lymphedema is well established based on strong evidence [ 15 , 16 ] and recent data suggest its benecial role concerning radiation - induced oral mucositis [ 1720 ]  . nevertheless , in the light of inconsistent data deduced from previously published studies [ 21 , 22 ] and recent published as well as ongoing prospective trials [ 23 , 24 ] evaluating the efcacy of pbm in reducing or preventing rd on breast cancer patients treated with ebrt , we initiated our study in order to add to the available experience . 
based on our data analysis , pbm treatment signicantly delays the appearance and reduces the severity of radiation - induced skin reactions as well as the intensity of skin toxicity - associated pain addition , our results depict a delayed need for supportive skin care intervention , which is a potential economic benet by minimizing supportive skin care costs . of importance may also be the fact that none of the patients in the pbm group was forced to interrupt rt due to higher grade skin toxicity . 
in their series consisting of 19 patients treated with led , 18 ( 94.7% ) presented with rd grade 01 and 1 patient ( 5.3% ) with rd grade 2 , whereas in the slightly larger control group ( n = 28 ) 4 patients ( 14.3% ) experienced grade 1 rd and 24 ( 85.7% ) presented with grade 23 . 
3 a bar chart presenting the relative frequencies of pain intensity , reported upon completion of rt for pbm group ( n = 25 ) , control group ( n = 45 ) and matched group ( n = 25 )  . 
4 a bar chart depicting patients relative frequencies in regard to duration of additional supportive skin care ( weeks ) through the rt course , for pbm group ( n = 25 ) and control group ( n = 45 )  . 
rt radiotherapy , pbm photobiomodulation 6 patients ( 24% ) required no supportive skin care throughout rt , 4 ( 16% ) required for the duration of 1 week , 5 ( 20% ) for 2 weeks , 6 ( 24% ) for 3 weeks , and 4 women ( 16% ) for 4 weeks . 
of those , 3 patients ( 6.7% ) required supportive skin products for the time interval of 1 week , 11 patients ( 24.4% ) for an interval of 2 weeks , 11 ( 24.4% ) for 3 weeks , 11 ( 24.4% ) for 4 weeks , and 8 ( 17.8% ) for 5 weeks . 
 [ 22 ] in a patient collective of 33 patients ( pbm group n = 18 , control group n = 15 ) did not manage to statistically demonstrate the benecial role of pbm during rt . 
concerning the pbm group , 6 patients ( 33.3% ) presented with rd grade 1 and 12 patients ( 66.7% ) with rd grade 2 , whereas in the control group 1 patient ( 6.6% ) did not experience rd , 4 ( 26.7% ) presented grade 1 rd , and 9 ( 60.0% ) presented with grade 2 and 1 ( 6.6% ) with grade 3 . 
in total , 3 patients were forced to interrupt rt due to severe rd , 2 ( 11.1% ) of the pbm and 1 ( 6.7% ) of the control group . 
the necessity for larger prospective studies comparing various pbm schemes , however , is essential , especially in the absence of other topical treatments preventing such side effects . conclusion the application of pbm using led prior to rt in breast cancer patients seems to have a dual benecial effect , in reducing the severity of rd and ameliorating pain intensity due to radiation - induced skin toxicity . acknowledgements we thank thor photomedicine ltd who kindly provided the light - emitting diode photobiomodulation device . 
nikolettou - fischer , and nikolaos zamboglou declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the present study hence focuses on the manifestation of early inammatory changes in mouse tongue during daily fractionated irradiation and their potential modulation by pentoxifylline . materials and methods daily fractionated irradiation with 5 fractions of 3 gy / week ( days 04 , 711 ) was given to the snouts of mice . 
the expression of the inammatory proteins tnf , nf - b , and il - 1 were analysed . ( cid : 2 ) sylvia gruber sylvia.gruber@meduniwien.ac.at 1 applied and translational radiobiology , dept . 
74 , 01307 dresden , germany 3 oncoray national center for radiation research in oncology , faculty of medicine and university hospital carl gustav carus , technische universitt dresden , helmholtz - zentrum dresden rossendorf , fetscherstr . 
pentoxifylline signicantly reduced the expression of tnf and il - 1 , but not nf - b . conclusion early inammation , as indicated by the expression of the inammatory markers tnf , nf - b , and il - 1 , is an essential component of early radiogenic oral mucositis . 
the mucoprotective effect of pentoxifylline does not appear to be based on modulation of nf - b - associated inammation . keywords fractionated irradiation oral mucositis head and neck cancer radiation protection animal model frhe entzndliche vernderungen bei strahleninduzierter oraler mukositis wirkung von pentoxifyllin im mausmodell zusammenfassung hintergrund und ziel frhe entzndliche vernderungen sind ein bedeutender faktor whrend der strahlenreaktion der schleimhaut . 
die vorliegenden untersuchungen fokussieren daher auf die manifestation frher entzndlicher vernderungen in der mauszunge whrend tglich fraktionierter bestrahlung und deren potenzieller modikation durch pentoxifyllin . material und methoden tglich fraktionierte bestrahlung mit 5 fraktionen zu 3 gy / woche ( tage 04 und 711 ) wurde auf die schnauzen der muse appliziert . 
pentoxifyllin reduzierte die expression von tnf und il - 1 signikant , nicht jedoch die expression von nf - b . schlussfolgerung frhe entzndung , gekennzeichnet durch die expression der entzndlichen marker tnf , nf - b und il - 1 , ist eine essenzielle komponente der frhen radiogenen oralen mukositis . 
der mukoprotektive effekt von pentoxifyllin scheint nicht auf nf - b - assoziierter antientzndlicher wirkung zu beruhen . schlsselwrter fraktionierte bestrahlung orale mukositis kopf - und - hals - tumore strahlenschutz tiermodell introduction oral mucositis is the most important early radiotherapy - related adverse event in head - and - neck cancer patients [ 1 , 2 ]  . severe conuent epithelial radiation reactions , experienced by the majority of patients , signicantly impact the patients quality of life with pain , swallowing , and speaking difculties [ 3 ]  . 
mucositis - related hospitalization and treatment interruptions [ 4 ] compromise the therapeutic outcome [ 5 ]  . current prophylactic and interventional strategies are purely symptomatic [ 6 ]  . 
this offers a target for biology - based mucositis - preventing strategies [ 7 , 8 ]  . pentoxifylline ( ptx ) , a nonspecic phosphodiesterase inhibitor , may improve tumor oxygenation due to rheologic effects , but may also ameliorate treatment - associated normal tissue morbidity through modulation of inammatory changes [ 9 ]  . 
when tested in a preclinical model of radiation - induced early oral mucositis , ptx was found to signicantly reduce the incidence of mucosal ulceration in daily fractionation studies in the established mouse tongue model . 
for this , the expression of the key inammatory mediators interleukin - 1 ( il - 1 - ) , tumor necrosis factor ( tnf ) , and nuclear factor kappa - light - chain - enhancer of activated b cells ( nf - b ) during daily fractionated irradiation and the effect of additional ptx treatment was quantied in immunohistochemical investigations . 
nf - b is hypothesized to be one of the key signaling molecules in this aspect [ 8 , 12 ] and was found upregulated in biopsies of oral mucosa of patients undergoing myoablative therapy [ 8 ]  . 
nf - b is an evolutionary - conserved signaling molecule that , as an inducible transcription factor , regulates reactions to changes in the environment . although involved in the transcriptional control of various genes , its main function is the regulation of the immune systenf - b is activated upon numerous stimuli , following either a classical , an alternative , or an atypical pathway . differences in the activation pathways arise from different subsets of stimulatory molecules and , furthermore , from subsequently recruited and differently processed intracellular binding partners . 
however , all pathways lead to nf - b activation via inducible degradation of the inhibitory protein complex that sequesters nf - b in the cytoplasm , followed by nf - b nuclear translocation and gene transcription [ 13 ]  . it activates proinammatory cytokines , chemokines , growth and survival factors [ 14 ]  . 
g. , rheumatoid arthritis [ 15 ]  . il - 1 presents another nf - b - activated protein , which can potentiate its own synthesis in autoregulatory pathways and activates nf - b in return [ 16 , 17 ]  . 
most importantly , it is a key mediator of the inammatory response [ 18 ]  . material and methods animals and housing in the present experiments , mice of the inbred c3h / neu strain from the breeding facility of medical faculty carl gustav carus , dresden , germany were housed under specied pathogen - free conditions with controlled temperature ( 2124 c ) and humidity ( 3050% )  . 
an automated light program provided a 12 / 12 - h light / dark rhythm , with lights on from 06 : 00 am to 06 : 00 pmaximum ten animals were kept in size 3 macrolon cages on saw dust bedding ( sniff , altrogge , lage , germany ) with free access to standard strahlenther onkol ( 2017 ) 193 : 499507 mouse diet ( altromin 1326 , altrogge , lage , germany ) and ltered city tap water from standard perspex drinking bottles . irradiation technique the technique for irradiation of oral mucosa was described in detail elsewhere [ 11 , 19 ]  . 
in brief , percutaneous irradiation of the entire snouts of the animals was performed with an yxlon mg325 device ( yxlon international x - ray gmbh , hamburg , germany ) , operated at 200 kv with a tube current of 20 ma . 
the bodies of the mice were shielded with 6 mm of lead equivalent mcp - 96 ( hek medizintechnik , lbeck , germany ) ; the treatment eld encompassed the snouts including the entire tongue . 
the dose homogeneity between the individual snout irradiation elds was 3% . experimental design daily fractionated irradiation with 5 fractions of 3 gy / week was applied over 2 weeks ( days 04 , 711 )  . 
the study comprised three experimental arms : irradiation alone ( ir ) , irradiation in combination with ptx administration ( ir + ptx ) , and ptx treatment alone ( ptx )  . 
ptx was administered subcutaneously at a dose of 15 mg / kg from day 5 until the day before sacrice ; on irradiation days , the drug was given 1 h before irradiation in the ir + ptx arin both arms , groups of animals ( n = 3 ) were sacriced every second day , and their tongues excised at the base for further investigations . 
three untreated and unirradiated mice served as a control group . histological preparation the tongues were incubated in 4% paraformaldehyde for 2448 h , cut along the median line , and subjected to routine parafn embedding . 
subsequently , the sections were deparafnized and rehydrated through xylene and a graded alcohol series . heat - mediated antigen retrieval for il - 1 and nf - b was performed with citrate buffer , ph 6.0 , boiling in a microwave set to full power for 20 mfor tnf , epitope unmasking was performed with edta buffer , ph 9.0 , for 10 min , also boiling in a microwave set to full power . 
the sections were then incubated with normal goat serum ( 1 : 200 ) , using a vectastain abc kit ( vectastain abc kit , vector laboratories , burlingame , ca , usa ) , for 1 h at room temperature , followed by overnight incubation at 4 c with the primary antibodies . 
the enzyme reaction was visualized by 3 , 3 - diaminobenzidine ( dab ) substrate ( vectastain abc kit , vector laboratories , burlingame , ca , usa )  . 
then , the slides were dehydrated in a graded alcohol series , cleared in xylene and coverslipped . histological analysis analysis was performed with an olympus light microscope at 400 magnication . 
cytoplasmic tnf expression could not be attributed to individual cells , hence , not the fraction of expressing , positive cells , but the general staining intensity was determined , separately for the germinal ( proliferative ) and the functional ( postmitotic ) nucleated layers of the epitheliuthe signal intensity , corresponding to the amount of secreted protein , was assessed semiquantitatively with an arbitrary score from 0 ( no signal ) , 1 ( weak signal ) , 2 ( intermediate signal ) to 3 ( strong signal )  . 
the fraction of nf - b p50 positive cell nuclei was evaluated separately for the germinal and the functional epitheliuin addition , the respective staining intensity was scored as described above for tnf . 
the number of il - 1 expressing macrophages in unirradiated and untreated control tongue sections was set to 100% , all further dayand experimental arm specic mean values refer to this normalization . 
the respective staining intensity was determined ( see above )  . 502 statistical analysis for statistical analysis , the spss statistical software ( spss inc . , chicago , il , usa ) was used . 
a p - value of < 0.05 was regarded statistically signicant . results tnf representative histophotographs of immunohistochemical staining for tnf , nf - b p50 , and il - 1 in control specimen and on days 6 and 14 are presented in fig . 
subsequently , the germinal expression in the ptx - treated experimental arm progressed similarly to only irradiated specimen until day 10 , although the tnf expression remained substantially lower compared to irradiation alone . 
with additional ptx treatment , tnf expression developed similar to that after irradiation alone , but was constantly substantially lower , however , with a signicant difference only being obtained tnf day 0 nf - b day 0 il1 day 0 day 6 day 14 day 6 day 14 day 6 day 14 fig . 
representative histophotographs of lower mouse tongue stained for tnf , nf - b p50 ( epithelial staining ) , and il - 1 - positive macrophages ( deeper tongue tissue , in close proximity to blood vessels )  . 
figures represent day 0 ( unirradiated and untreated controls ) , day 6 and day 14 during fractionated irradiation alone ( ir ) , with additional ptx administration ( ir + ptx ) , and ptx treatment alone ( ptx )  . 
the staining signal intensity was scored semiquantitatively with an arbitrary score of 0 ( no signal ) , 1 ( weak ) , 2 ( intermediate ) , or a maximum of 3 ( strong )  . 
3 effect of fractionated irradiation ptx and ptx alone on nf - b p50 expression . nf - b p50 expression was analyzed in the epithelium , in the germinal ( a ) and functional ( c ) compartments , respectively . 
the staining signal intensity was scored semiquantitatively with an arbitrary score of 0 ( no signal ) , 1 ( weak ) , 2 ( intermediate ) , or a maximum of 3 ( strong ) in both compartments as well ( b and d )  . 
with daily fractionated irradiation , nf - b p50 expression increased over the normal range on day 2 ( 58.3% ) and progressively expanded to a maximum of 83% on day 12 . 
the number of macrophages positive for il - 1 ( a ) as well as the staining signal intensity ( b ) was evaluated . the staining intensity was scored semiquantitatively with an arbitrary score of 0 ( no signal ) , 1 ( weak ) , 2 ( intermediate ) , or a maximum of 3 ( strong )  . data points represent the mean of 3 animals , error bars indicate 1 standard deviation ( sd )  . 
no biology - based treatment has so far been implemented into clinical practice . ptx treatment during daily fractionated irradiation resulted in a signicant reduction of the incidence of oral mucositis in the mouse tongue model [ 11 ] this may be attributed to a modulation of inammatory processes which are suggested to be a major component of ( early ) normal tissue radiation effects [ 23 , 24 ] , including mucositis [ 25 , 26 ]  . early inammation is regularly observed during the clinical manifestation of oral epithelial ulceration in patients . nf - b seems to play a key role in this aspect [ 8 , 12 ]  . with tnf and il - 1 , stimuli for both the classical and the alternative nf - b activation pathway have been investigated this study . 
ptx was found to ameliorate pain in preclinical as well as clinical studies , likely due to reduced tnf and il - 1 release [ 28 , 29 ]  . 
this effect , however , is not substantiated in the animal model used in the present study . irradiation alone in our mouse tongue model , daily fractionated irradiation rapidly induced the expression of all inammatory markers il - 1 daily fractionated irradiation progressively increased the number of il - 1 positive macrophages to a maximum of 190% on day 6 . 
subsequently , the staining intensity reentered the normal range . additional ptx treatment kept the number of il - 1 expressing macrophages close to or within the normal range until day 8 . 
in contrast to tnf and nf - b expression levels , which remained considerably high throughout the study period , il - 1 was found to be downregulated at the end of the rst treatment week , despite ongoing irradiation . this corresponds to the time of onset of repopulation , i . 
a potential interaction with the epithelial regenerative radiation response is hence highly likely . irradiation with additional ptx administration ptx exhibits potent anti - inammatory effects [ 31 , 32 ] , directly inhibits tnf , and reduces inammation in multiple preclinical models [ 3335 ] , chemotherapy - induced intestinal ( cpt - 11 ) and oral ( 5 - fu ) mucositis [ 36 , 37 ]  . 
however , tnf is only one of the ligands of the tumor necrosis factor receptor ( tnfr ) superfamily , which consists of 19 ligands and 30 receptors [ 39 ] , all of which result in the activation of the nf - b pathway . 
hence , it appears to be highly likely that lacking tnf and / or il - 1 is substituted by other stimuli . activation could also occur via the atypical activation pathway . 
in addition to ligand - mediated activation , nf - b can be stimulated by reactive oxygen species , such as hydrogen peroxide , which is abundantly produced during the radiolysis of intracellular water [ 42 ]  . 
further oxidants , such as singlet oxygen and superoxide and reactive nitrogen species have been shown to active nf - b and are released by immune cells during inammation [ 43 ]  . 
this hypothesis is supported by the missing effect of specic tnf inhibition with iniximab on oral mucositis , obtained in another study in the mouse tongue model [ 44 ]  . the central role of nf - b in the regulation of the inammatory response promotes further targeting of this pathway as a treatment strategy to reduce radio ( chemo ) therapy - induced oral mucositis . 
recently , a reduction of radiationinduced oral mucositis by specic targeting of nf - b was demonstrated in the mouse tongue model [ 45 ]  . ptx alone in our study , ptx treatment alone left the expression levels of all inammatory mediatory investigated largely unchanged and within control ranges . 
ptx most likely exerts its mucositis - ameliorating activity through a mechanism other than modulation of nf - b associated inammation . presumably , the recently demonstrated ptx - mediated reduction of radiation - induced early epithelial hypoxia [ 19 ] accounts for the benecial effect . 
modulation of epithelial proliferation by ptx is currently being investigated . conclusion based on these results , the mucositis - ameliorating effects of ptx , observed in functional studies [ 11 ] , cannot be attributed to a reduction of radiation - induced nf - b associated inammatory changes . 
further analyses of the mechanistic effects of ptx during the development of radiation - induced oral mucositis are required to fully elucidate its potential as mucositis - ameliorating treatment strategy . acknowledgements the nancial support by the federal ministry of science , research and economy and the national foundation for research , technology and development is gratefully acknowledged . open access funding provided by medical university of vienna . compliance with ethical guidelines conict of interest s . 
mai 2017 springer - verlag berlin heidelberg 2017 hintergrund gomez und mitarbeiter untersuchten in einer prospektiv randomisierten , multizentrischen phase - iistudie den nutzen einer konsolidierenden lokaltherapie nach erstlinientherapie bei patienten mit oligometastasierten , nicht - kleinzelligen lungenkarzinomen ( nsclc )  . patienten und methode in die multizentrische , randomisierte phase - ii - studie wurden patienten mit nsclc im oligometastasierten stadium iv ohne progression nach erstlinientherapie ( 4 zyklen platinhaltige kombinationschemotherapie oder 3 monate egfr - / alk - inhibitoren bei egfr - mutation oder alk - rearrangement ) eingeschlossen . oligometastasierung wurde dabei deniert als vorhandensein von ( cid : 2 ) 3 fernmetastasen oder thorakaler lymphknotenbefall mit maximal 2 fernmetastasen nach erstlinientherapie . 
local consolidative therapy versus maintenance therapy or observation for patients with oligometastatic non - small - cell lung cancer without progression after rst - line systemic therapy : a multicentre , randomised , controlled , phase ii study . 
primrer endpunkt der studie war das progressionsfreie berleben ( pfs )  . ergebnisse zwischen november 2012 und januar 2016 wurden 74 patienten in das protokoll eingeschlossen , wobei die studie nach der randomisierung von 49 patienten frhzeitig geschlossen wurde ( nach beschluss des data safety monitoring committee am md anderson cancer center )  . es zeigte sich nmlich ein hoch signikanter vorteil fr die patientengruppe mit lokaler konsolidierungstherapie , so dass eine fortfhrung der studie aus ethischen gesichtspunkten als nicht vertretbar eingestuft wurde . 
nach einer medianen nachbeobachtungszeit von 12 , 4 monaten ergab sich ein medianes pfs von 11 , 9 monaten in der gruppe mit konsolidierender lokaltherapie , verglichen mit 3 , 9 monaten in der gruppe mit alleiniger erhaltungschemotherapie ( hazard ratio [ hr ] 0 , 35 ; p = 0 , 0054 )  . 
das mediane gesamtberleben wurde in beiden gruppen noch nicht erreicht . schlussfolgerung der autoren eine konsolidierende lokaltherapie verbessert das pfs bei oligometastasierten patienten mit nsclc ohne progress nach erstlinientherapie . die lokaltherapie der metastasen in diesem kollektiv sollte in phase - iii - studien untersucht werden . 596 kommentar gomez et al . 
sie ist ein wichtiger beitrag sowohl zur weiterentwicklung therapeutischer konzepte in diesem kollektiv als auch zum grundstzlichen paradigma der oligometastasierung . der beobachtete vorteil von 8 monaten im pfs ist beeindruckend . 
zwar handelt es sich mit nur 49 randomisierten patienten letztlich um ein kleines patientengut , welches aber im kontext der sprlichen , prospektiven datenlage zur konsolidierenden lokaltherapie in dieser hugen klinischen situation umso wichtiger ist [ 25 ]  . 
dies kann als mglicher hinweis auf den systemischen effekt der lokaltherapie sowie die verhinderung der weiteren krankheitsausbreitung im stadium der oligometastasierung gewertet werden [ 6 ]  . die lokaltherapie beinhaltete in annhernd allen fllen eine radiotherapie ( lediglich bei einem patienten wurden alle metastasen allein reseziert )  . 
deshalb muss die therapeutische vorgehensweise fr jeden einzelfall interdisziplinr besprochen werden [ 7 ]  . um gengend patienten fr die studie rekrutieren zu knnen , waren die einschlusskriterien bewusst breit formuliert . 
so fallen neben den unterschiedlichen klinischen befunden auch die verschiedenen erhaltungsstrategien sowie unterschiede in der diagnostik als mgliche einussfaktoren ins auge ; sie wurden aufgrund der kleinen patientenzahl nicht weiter ausgewertet . dies ist relevant , da prognostische faktoren , wie synchrone vs . 
insbesondere ist auch das fdg - pet - staging als selektionsfaktor mit einuss auf das outcome nach aggressiver lokaltherapie in der oligometastasierten situation belegt [ 9 , 10 ]  . 
nennenswert ist , dass strahlenther onkol ( 2017 ) 193 : 595597 im arm ohne lokaltherapie 83 % eine medikamentse erhaltungstherapie ( am hugsten mit pemetrexed ) erhielten gegenber lediglich 20 % im arm mit lokaltherapie . 
liefern mit ihrer arbeit erstmals daten aus einem randomisierten vergleich zum vorteil einer konsolidierenden lokaltherapie beim oligometastasierten nsclc , welche insbesondere im kontext der rapiden klinischen adaption der stereotaktischen radiotherapie hier dringend notwendig waren [ 12 ]  . 
fr den klinischen alltag bedeutet dies eine besttigung der zunehmend aggressiveren strategien in dieser krankheitssituation , wie sie an vielen kliniken bereits verfolgt werden . tobias finazzi und matthias guckenberger , zrich interessenkonikt t . 
gomez dr , blumenschein gr jr . , lee jj et al ( 2016 ) local consolidative therapy versus maintenance therapy or observation for patients with oligometastatic non - small - cell lung cancer without progression after rst - line systemic therapy : a multicentre , randomised , controlled , phase 2 study . 
de ruysscher d , wanders r , van baardwijk a et al ( 2012 ) radical treatment of non - small - cell lung cancer patients with synchronous oligometastases : long - term results of a prospective phase ii trial ( nct01282450 )  . 
downey rj , ng kk , kris mg et al ( 2002 ) a phase ii trial of chemotherapy and surgery for non - small cell lung cancer patients with a synchronous solitary metastasis . 
iyengar p , kavanagh bd , wardak z et al ( 2014 ) phase ii trial of stereotactic body radiation therapy combined with erlotinib for patients with limited but progressive metastatic non - small - cell lung cancer . 
ashworth ab , senan s , palma da et al ( 2014 ) an individual patient data metaanalysis of outcomes and prognostic factors after treatment of oligometastatic non - small - cell lung cancer . 
rieber j , abbassi - senger n , adebahr s et al ( 2016 ) inuence of institutional experience and technological advances on outcome of stereotactic body radiation therapy for oligometastatic lung disease . int j radiat oncol biol phys . 
congedo mt , cesario a , lococo f et al ( 2012 ) surgery for oligometastatic non - small cell lung cancer : long - term results from a single center experience . 
andrews dw , scott cb , sperduto pw et al ( 2004 ) whole brain radiation therapy with or without stereotactic radiosurgery boost for patients with one to three brain metastases : phase iii results of the rtog 9508 randomised trial . 
lewis sl , porceddu s , nakamura n et al ( 2015 ) denitive stereotactic body radiotherapy ( sbrt ) for extracranial oligometastases : an international survey of > 1000 radiation oncologists . 
there were 14 deaths ( 7 cancer specic ) and 14 recurrences ( 5 local recurrences and 9 distant metas ( cid : 2 ) kim joo - young , md jooyoungcasa@ncc.re.kr proton therapy center , research institute and hospital , national cancer center , goyang , korea ( republic of ) 2 cancer policy branch , research institute and hospital , national cancer center , goyang , korea ( republic of ) 3 cancer research institute , seoul national university college of medicine , seoul , korea ( republic of ) 4 center for uterine cancer , research institute and hospital , national cancer center , goyang , korea ( republic of ) 5 gynecologic cancer branch , research institute and hospital , national cancer center , goyang , korea ( republic of ) 6 department of cancer control and policy , graduate school of cancer science and policy , national cancer center , goyang , korea ( republic of ) 7 research institute and hospital , national cancer center , 323 ilsan - ro , 410 - 769 goyang , gyeonggi , korea ( republic of ) tases )  . 
compared to the general population , lccs exhibited a signicantly higher rate of body image concerns , sexual dysfunction , lymphedema , and peripheral neuropathy . conclusion new recurrences occurred in 5% of lccs and grade 2 treatment - related morbidities were present in 33% . 
these results suggest the need for long - term surveillance and follow - up care for lccs . keywords gynecology side effects survival toxicity quality of life allgemeiner gesundheitsstatus langzeitberlebender von gebrmutterhalskrebs nach strahlentherapie zusammenfassung zielsetzung bewertung des allgemeinen gesundheitsstatus bei langzeitberlebenden von gebrmutterhalskrebs ( lccs ) , die nach strahlenbehandlung ( rt ) mehr als 4 jahre lebten . patienten und methoden berprft wurden krankenakten von 562 frauen , die zwischen 2003 und 2010 in unserem institut mit rt behandelt wurden . 
bewertet wurden der erkrankungsstatus und spte morbiditt bei 303 lccs . die lebensqualitt ( qol ) wurde bei 168 patienten anhand des fragebogens der europischen organisation fr die forschung und behandlung von krebs analysiert und mit gesunden altersgleichen koreanischen frauen verglichen . ergebnisse das mediane follow - up betrug 6 , 8 jahre ( spanne 4 , 112 , 5 jahre )  . 
bei lccs traten signikant hhere raten von krperbildstrungen , sexuellen strungen , lymphdemen und peripherer neuropathie als bei der allgemeinbevlkerung auf . schlussfolgerung neue rezidive kamen in 5 % der lccs vor ; behandlungsbezogene morbiditt vom grad 2 hatten 33 % . 
diese resultate sprechen fr eine langzeitberwachung und angemessene nachsorge bei lccs . schlsselwrter gynkologie nebenwirkungen berleben toxizitt lebensqualitt cervical cancer is the fourth most commonly diagnosed cancer in women worldwide and the seventh most common in korea [ 1 , 2 ]  . 
with early detection and advances in treatment , the number of long - term cervical cancer survivors ( lccs ) has increased over the past 40 years in developed countries [ 3 ]  . 
according to one report , new side effects kept developing up to 20 years after treatment [ 4 ] and the incidence of secondary malignancies increased over time , indicating the necessity of long - term follow - up of the cancer survivors . 
however , regular follow - up of the patients who have remained disease free for 5 years is not considered necessary in general . indeed , most cervical cancer patients suffer from various morbidities resulting from the disease itself or from [ 5 ]  . 
depending on the treatment stratthe treatment egy usedsurgery , radiotherapy ( rt ) , or chemotherapymorbidities may include symptoms associated with the gastrointestinal or urinary tracts , lymphedema , and sexual dysfunction [ 6 , 7 ]  . 
in particular , the treatment of locally advanced cervical cancer , i.e. , high - dose radiation applied to the pelvic area by external beam rt ( ebrt ) and brachytherapy , can cause considerable morbidity in survivors and substantially decrease their quality of life ( qol ) [ 3 ]  . 
because past studies of the health issues of lccs focused on patients with early - stage disease who received surgery alone [ 8 ] or who had a relatively short follow - up after rt [ 9 ] , the present study aimed to evaluate the general health status of patients with advanced cervical cancer on a longer timescale . 
the follow - up protocol involves visits every 3 months for the rst 2 years , every 4 months for the third year , every 6 months for the fourth year , and annually thereafter . 
in the present study , we included patients who had passed their fourth year of follow - up in order to include any events that occurred between the fourth and fth year after treatment . a total of 303 lccs were included in this study and information pertaining to their disease status and treatmentrelated complications were collected from the medical records . 
among this population , 35 patients had relapsed within the rst 4 years after radiotherapy , but since they had survived for more than 4 years , they were included in this study . 
informed consent was obtained from all patients who participated in the qol part of this study . treatment patients received concurrent chemoradiotherapy using three - dimensional ( 3d ) conformal ebrt with a four - eld technique using a 15 - mv linear accelerator and high - doserate intracavitary radiotherapy ( icr )  . 
for brachytherapy planning , ct - based icr was used before february 2008 [ 10 ] and since then mri - based icr has been used [ 11 ]  . brachytherapy planning was performed according to the recommendations of the gynecologic groupe european de curietherapie , european society for therapeutic radiology and oncology working group [ 1214 ]  . 
the 168 of 303 survivors were available for quality - of - life assessment . thirty - seven patients who were treated between september 2003 and september 2009 underwent laparoscopic lymph node staging before rt under the prospective protocol to evaluate efcacy and feasibility of pretreatment laparoscopic lymph node staging in locally advanced cervical cancer [ 15 ]  . 
extended - eld rt was used for patients with para - aortic lymph node metastasis , as suspected by mri or positron - emission tomography ( pet ) , or conrmed by surgical lymph node staging . 
otherwise , patients received a combination of 4550 gy of pelvic ebrt and 30 gy of high - dose - rate brachytherapy with daily fractions of 5 gy over 3 weeks . 
the biologically equivalent dose to point a in 2 - gy fractions was previously calculated as approximately 82 gy for cervical tumor ( / = 10 ) and 91 gy for normal tissue ( / = 3 ) [ 10 ]  . 
for large lymph node metastases or radiologically residual lesions after pelvic ebrt , a lymph node boost was given using either 3d conformal ( prior to april 2007 ) or helical ( after april 2007 ) tomotherapy with a median of 9 gy ( range 425 gy )  . 
chemotherapy was also given to the women with one of the high - risk factors , such as positive metastatic lymph node , or positive or close parametrial resection margin . late toxicity at regular follow - up visits , toxicity was evaluated using the structured scoring schema of the radiation therapy oncology group ( rtog ) / european organization for research and treatment of cancer ( eortc ) late radiation toxicity criteria [ 16 ]  . 
additionally , lower extremity lymphedema was also evaluated . quality of life assessment at our institution , we have systematically assessed the health - related qol of lccs since january 2012 . 
we used the missing imputations method if data were missing from 546 strahlenther onkol ( 2017 ) 193 : 543551 table 1 characteristics of cervical cancer survivors ( n = 303 ) characteristics age at diagnosis ( years ) no . 
logistic regression analysis was used to adjust for potentially confounding factors . the variables included in the nal regression models were restricted to statistically signicant covariates . comparisons of variables between the lccs and an agematched , healthy korean female population sample were performed using chi - square tests for categorical data and quality of life mannwhitney u tests for continuous variables . 
among the patients who received denitive rt ( n = 243 ) , 59 ( 19% ) were international federation of gynecology and obstetrics ( figo ) stage i , 142 ( 47% ) were stage ii , 29 ( 10% ) were stage iii , and 13 ( 4% ) were stage iv . 
among the patients who received postoperative radiotherapy ( n = 60 ) , the values were 43 ( 72% ) stage i and 17 ( 28% ) stage ii . a lymph node boost was given in 62 lccs ( 13% ) using either 3d - conformal ( n = 51 ) or helical tomotherapy ( n = 11 ) as part of pelvic rt . 
of the 14 deaths , 7 were due to disease recurrence , 3 were due to secondary cancers , and the rest were due to other medical problems ( n = 4 )  . 
in terms of secondary malignancy induced by radiotherapy , 7 patients developed tumors : 6 within the rt eld ( pelvic bone chondrosarcoma , n = 2 ; abdominal wall angiosarcoma , n = 1 ; uterine carcinosarcoma , n = 1 ; ascending colon cancer , n = 1 ; and bladder cancer , n = 1 ) and 1 acute myeloid leukemia . 
other frequent toxicities were small / large intestine ( n = 36 , 15% ) , kidney ( n = 18 , 6% ) , and bone ( n = 17 , 6% ) toxicities . most toxicities were grade 2 , but there were two cases of grade 34 bladder toxicity with hematuria and three cases of grade 3 small / large intestine toxicity with rectal bleeding that required endoscopic coagulation more than 4 years after treatment . 
in terms of bone complications , compression fractures of the lumbar spine , symptomatic pelvic insufciency fractures , and femur neck fractures occurred in 12 , 8 , and 1 patient , respectively . 
among 18 lccs who had renal dysfunction , 16 patients had chronic obstructive hydronephrosis , 1 had cisplatin - induced nephropathy , and 1 had aggravation of underlying polycystic kidney disease . 
for the 16 lccs who required repeated percutaneous nephrostomy or double j stent insertion due to hydronephrosis , 8 were initially figo stage iiib or iva , and 2 acquired hydronephrosis after local invasion of recurrent disease . 
most of the patients ( 34 out of 46 ) who reported lymphedema belonged to the pre - rt surgical lymph node staging group . the results of univariate and multivariate analyses for predisposing factors for grade 2 late toxicity are listed in table 3 . 
among the 12 lccs who had spinal compression fractures , 6 received extended - eld rt ( 6 / 85 , 7% ) and 6 received pelvic rt ( 6 / 218 , 3% )  . 
s. lccs long - term cervical cancer survivors , rt radiotherapy , port postoperative radiotherapy , pan para - aortic node , ebrt external - beam radiotherapy , icr intracavitary radiotherapy , figo international federation of gynecology and obstetrics , or odds ratio , hr hazard ratio , ci condence interval , n . 
scores for social role function ( p = 0.057 ) , cognitive function ( p = 0.072 ) , and nancial problems ( p = 0.061 ) tend to be lower in lccs ( table 5 )  . 
lccs were also found to have a substantial incidence of lymphedema ( p = 0.013 ) and peripheral neuropathy ( p = 0.002 ; table 5 )  . discussion in the current study , we found 14 patients with further recurrent events more than 4 years after treatment and 7 cases of secondary cancer that were considered to be radiationinduced . 
the qol assessments showed that although the general health status of lccs recovered to a level comparable to that of the normal population , lccs continue to report cervical cancer - specic health problems . there were ve cases of late local recurrence and nine cases of late distant metastasis . 
more than half of the late distant metastases occurred along the lymphatic drainage system ( n = 5 ) and the rest occurred in the lung parenchyma ( n = 4 )  . 
in the present study , there were two cases of pelvic bone sarcoma , which suggests that it might also be necessary to minimize the radiation dose applied to the bony pelvis by using intensity - modulated rt . the main tissues affected by late radiation toxicity following concurrent chemoradiation of cervical cancer are the bladder and gastrointestinal tract [ 25 ]  . 
these results are comparable with the present ndings of bladder toxicity : 19% grade 2 , 1% grade 34 ; and small / large intestine toxicity : 15% grade 2 , 1% grade 3 . 
the fact that many lccs experienced menopause before or at the time of radiotherapy may partially explain the higher rate of bone complications in patients 51 - years - old . 
several studies have suggested that older patients are at a higher risk for radiation - related bone fractures , including pelvic insufciency fracture after rt for cervical cancer [ 30 ]  . 
in this study , the incidence of renal dysfunction caused by chronic hydronephrosis was greater in patients with an initial figo 550 strahlenther onkol ( 2017 ) 193 : 543551 stage of iii or iv , suggesting that ureteral obstruction or bladder invasion at diagnosis lead to persistent renal function impairment . 
in a recent analysis of the embrace study , kirchheiner et al . reported that patient functioning and general qol were impaired at baseline , but improved during the rst 6 months after treatment , reaching levels comparable to that of the reference population [ 9 ]  . 
in our study , lccs reported signicantly more sexual / vaginal dysfunction and sexual worries . similar results were also shown in the embrace study , in which sexual worries were pronounced in lccs during the entire observation period , and vaginal dryness and pain increased over time . several limitations of this study should be mentioned . first , because we began assessing qol in lccs in january 2012 , patients who had discontinued follow - up before then ( approximately half ) were not included . 
in addition , we did not address or control for postradiotherapy lifestyle factors that could inuence the development of complications . future studies should include comprehensive assessments of the patients lifestyles and other comorbidities . 
the best technical effort , including organ sparing with modern rt techniques and ovarian transposition , should be actively implemented to result in fewer long - term complications and a better qol for survivors . furthermore , because radiation - induced complications are inuenced by systemic disease , lifestyle , and psychological support , it is necessary to systematically monitor the patients symptoms and educate patients on how to improve their qol . conclusion lccs had an approximately 5% late recurrence rate beyond 4 years and a 2% rate of secondary malignancy . 
the 1 - year overall survival ( os ) rates ( cid : 2 ) hideya yamazaki , md hideya10@hotmail.com 1 department of radiology , graduate school of medical science , kyoto prefectural university of medicine , 465 kajiicho kawaramachi hirokoji , kamigyo - ku , kyoto 602 - 8566 , japan 2 cyberknife center , soseikai general hospital , 126 kami - misu , shimotoba fushimi - ku , kyoto , japan 3 department of radiology , hyogo ion beam medical center , 1 - 2 - 1 kouto , shingu - cho , tatsuno , hyogo 679 - 5165 , japan 4 radiotherapy department , fujimoto hayasuzu hospital , hayasuzu 17 - 1 , miyakonojo , miyazaki 885 - 0055 , japan 5 department of radiology , japanese red cross okayama hospital , aoe 2 - 1 - 1 , kita - ku , okayama , okayama 700 - 8607 , japan 6 department of radiation oncology , national hospital organization osaka national hospital , 2 - 1 - 14 , hoenzaka , chuo - ku , osaka , osaka 540 - 0006 , japan 7 department of radiation oncology , osaka university graduate school of medicine , suita , osaka 565 - 0871 , japan 8 miyakojima igrt clinic , osaka 534 - 0021 , japan were 67.9% for cp and 54.1% for photon radiotherapy ( p = 0.15 ; 55% for ck and 51% for imrt )  . 
multivariate analysis revealed that younger age and a larger planning target volume ( ptv ) were signicant risk factors for grade 3 or worse toxicity . conclusion cp provided superior survival outcome compared to photon radiotherapy . 
younger patients with a larger ptv experienced toxicity grade 3 . keywords head and neck neoplasms reirradiation stereotactic radiotherapy charged particle radiotherapy intensity - modulated radiotherapy erneute bestrahlung von wiederkehrenden kopfhals - tumoren mittels ionenoder photonenstrahlentherapie zusammenfassung zielsetzung bestimmung der ergebnisse einer rebestrahlung von wiederkehrenden kopf - hals - tumoren mittels verschiedener modalitten . 526 strahlenther onkol ( 2017 ) 193 : 525533 methode die retrospektive studie umfasst 26 patienten , die mit der ionenstrahlentherapie ( cp ) , und 150 patienten , die mit der photonenstrahlentherapie ( 117 stereotaxien [ ck ] und 36 intensittsmodulierte strahlentherapien [ imrt ] ) behandelt wurden . 
der kehrwert der behandlungswahrscheinlichkeit ( iptw ) wurde fr die propensity - scoreanalyse angewendet , um die hintergrundauswahleffekte zu verringern . ergebnisse cp verwendete eine hhere verschriebene dosierung als die photonenstrahlentherapie . 
die lokalen kontrollraten fr patienten , die mit der ionenoder photonenstrahlentherapie behandelt wurden , betrugen nach 1 jahr jeweils 66 , 9 % ( spanne 46 , 387 , 5 % ) bzw . 
insgesamt 48 patienten ( 27 % ) erfuhren eine toxizitt grad 3 ( 24 % in der photonenstrahlentherapie - , 46 % in der cp - gruppe ) , einschlielich 17 patienten mit einer grad - 5 - toxizitt . 
in der multivariaten analyse waren jngeres alter und greres planungszielvolumen ( ptv ) signikante risikofaktoren fr eine grad - 3 - toxizitt oder schlechter . schlussfolgerung cp lieferte bessere berlebensdaten als die photonenstrahlentherapie . 
jngere patienten mit grerem ptv erfuhren einen toxizittsgrad schlsselwrter kopf - hals - neoplasien rebestrahlung stereotaktische strahlentherapie ionenstrahlentherapie intensittsmodulierte strahlentherapie introduction recent progress in the treatment of head and neck cancers , particularly advances in treatment modalities and chemotherapy , improved survival for more than 5 years after treatment [ 1 ]  . 
reirradiation has emerged as a potentially curative therapy with the advent of modern radiotherapy techniques , such as intensity modulated radiotherapy ( imrt ) and stereotactic body radiotherapy ( sbrt ) [ 5 ]  . in addition , charged particle radiotherapy ( cp ) treatments , such as proton and carbon ion radiotherapy , have a unique dose distribution that could avoid irradiation of surrounding normal tissue with extra doses , namely the bragg peak , which allows maximum dose deposition at a specic depth , followed by a rapid dose falloff [ 69 ]  . 
previously , we compared survival outcomes between patients treated with cp and those treated with sbrt using cyberknife ( ck ) by a matched - pair method after correcting for three background factors ( primary site [ nasopharynx or not ] , planning target volume [ ptv ] , and interval from the initial radiotherapy ) and found that cp was superior [ 10 ]  . however , there was a huge background bias between cp and ck with regard to histology , i . 
therefore , the present study aimed to examine the outcomes of reirradiation for recurrent head and neck cancers using different modalities of multi - institutional pooled data , with an additional statistical method ( inverse probability of treatment weighting [ iptw ] ) to reduce bias . materials and methods patients we included patients with recurrent head and neck tumors treated at soseikai general , fujimoto hayasuzu , okayama kyokuto , and osaka university hospitals ; miyakojima igrt clinic ; and hyogo ion beam medical center ( hibmc ) between 2000 and 2010 . 
the charged particle beam dose is reported in gy ( relative biological effectiveness , rbe ) , which is the physical dose multiplied by the rbe of the protons or carbon ions . 
a total of 26 patients were treated with cp ( 17 carbon and 9 proton ) and 150 were treated with photon radiotherapy ( 117 ck and 33 imrt ) in multiple institutions . 
or median ( range ) 55 ( 1982 ) female male nasopharynx orohypopharynx 0 oral salivary gland nasal and paranasal sinus other ( months ) 13 ( 492 ) squamous cell carcinoma other melanoma adenoid cystic undif ca . , alveolar rhabdomyosarcoma , adeno ( cm3 ) ( gy ( rbe ) or gy ) ( / = 10 ) ( gy ( rbe ) or gy ) ( / = 10 ) 25.5 ( 2188 ) 65 ( 4974 ) ( 90142 ) ( 42 ) ( 58 ) ( 15 ) ( 12 ) ( 58 ) ( 54 ) ( 65 ) ( 35 ) gender primary site interval from initial radiotherapy histology gross target volume surgical history prescribed dose ( eqd2 ) cumulative dosea ( eqd2 ) photon therapy = sbrt + imrt n = 150 no . 
adenocarcinoma italic values indicate statistical signicance a summation of previous radiotherapy and reirradiation in a median of ve fractions ( range 38 fractions ) prescribed as d90% , d95% , or a marginal dose . 
the thick line depicts patients treated for a gtv of ( cid : 2 ) 40 cm3 and the dashed line depicts patients treated for a gtv of > 40 cm3 . 
the thick line depicts cp patients , dashed line depicts ck patients , and dotted line depicts imrt patients 4.1.2 ( brainlab ag , feldkirchen , germany ) were used to plan treatment and prescribe doses with 95% coverage of the ptv , using intensity modulated maps . 
in brief , after a custom - made thermoplastic cast was used to immobilize each patient in the supine position with an adequate head angle , 1 mm computed tomography ( ct ) slices and 13 mm magnetic resonance imaging ( mri ) slices were obtained . 
the ctv was generally dened as the gtv plus a 5 mm basic margthe ptv was dened as the ctv plus a setup margin of 3 mcp was delivered daily ( ve doses per week ) to the isodose encompassing the ptv . 
median prescribed dose was 57.6 gy ( rbe ) ( range 43.270.2 gy [ rbe ] ) in 16 fractions ( range 1230 fractions )  . toxicity was evaluated using the national cancer institute common toxicity criteria scale version 3.0. 
each institution reported any toxicity grade 3 or more ( irrespective of whether acute or late )  . the biological effects the biologically equivalent dose was calculated as the equivalent of 2 gy fractions ( eqd2 ) , using a linear quadratic model , where / = 10 for tumors and / = 3 for organs at risk . 
however , in this article , all doses are reported in gy to avoid confusion . 530 strahlenther onkol ( 2017 ) 193 : 525533 table 3 toxicity of reirradiation grade photon radiotherapy ( 75% ) ( 14% ) ( 1% ) ( 9% ) cp charged particle statistical analyses ulceration and bleeding ( 2 ) necrosis ( soft tissue 2 , bone 3 ) fistula ( 7 ) visual disturbance and lateral lobe necrosis ( 1 ) edema ( 4 ) abscess ( 2 ) bleeding and temporal lobe necrosis ( 1 ) soft tissue damage with pain ( 1 ) bleeding ( 10 ) ulceration ( 1 ) mucositis ( 1 ) trismus and abscess ( 1 ) ( 54% ) ( 19% ) nerve palsy ( 2 ) mucosal ulceration ( 2 ) skin ulceration ( 1 ) ( 12% ) ( 15% ) visual disturbance ( 2 ) soft tissue necrosis ( 1 ) bleeding ( 2 ) skin / bone necrosis and infection ( 1 ) soft tissue necrosis and infection ( 1 ) all statistical analyses were performed using statview 5.0 statistical software ( sas institute , inc . , cary , nc , usa ) and r stat package ( for iptw ) [ 14 ]  . 
the coxs proportional hazard model ( survival ) and logistic regression model ( toxicity ) were used for the uniand multivariate analysis ( variables p < 0.1 in univariate analysis and thought to be clinically important were inserted into the multivariate analysis )  . 
all analyses used the p < 0.05 level of signicance unless otherwise indicated . because the included patients were not randomized , unbalanced baseline characteristics could have led to selection bias and , hence , inuence the decision to undergo cp . 
in the calculation of the propensity scores , the logistic regression model was used considering the baseline covariates ( except total dose and treatment methodology ) shown in table 2 . 
e. , weighting patients who received cp by 1 / propensity score , whereas patients who received photon radiotherapy were weighted by 1 / ( 1propensity score )  . results patient and disease characteristics of the patients treated with cp and photon radiotherapy ( ck + imrt ) are listed in table 1 . 
the median age of the patients was 59 years ( range 1988 years ) , including 129 men and 45 women . the common primary sites were the nasopharynx , orohypopharynx , and nasal and paranasal sinuses . 
the 1 - year os rates were 67.9% ( 95% ci 47.486.4% ) for cp and 54.1% ( 95% ci 45.465.4% ) for photon radiotherapy ( p = 0.15 ; 55% for ck and 51% for imrt )  . 
there were 13 ( 9% : 10 bleeding , one ulceration , one mucositis , one trismus and abscess ) grade 5 toxicities in photon radiotherapy , whereas 4 ( 15% : 2 bleeding , one skin / bone necrosis and infection , one soft tissue necrosis and infection ) in cp . toxicity discussion a total of 48 patients ( 27% ) presented with grade 3 or worse toxicity ( 24% of patients treated with photon radiotherapy : imrt , 23% [ 11 / 33 ] and ck , 21% [ 25 / 117 ] ; 46% of patients treated with cp ; p = 0.04 ) , including 17 patients with grade 5 toxicity ( 9.7% ) ( cp , 4 ; imrt , 2 ; ck , 11 ) ( table 3 )  . 
in a previous analysis , we found that small - volume nasopharyngeal cancers after a long disease - free period could 532 strahlenther onkol ( 2017 ) 193 : 525533 show better outcomes [ 10 ]  . 
although cp showed superior outcomes , there was a huge discrepancy ( dominant non - scc population in the cp group ) between cp and photon radiotherapy in this previous study [ 11 ]  . 
in addition , as different ptv margins were used by the various institutions in this study we used the gtv for survival analysis and the ptv for toxicity analysis . we found that patients with small nasopharyngeal cancer who were treated with a higher prescribed dose had longer survival . 
however , although imrt used a higher prescribed dose in the eqd2 calculation , there was no difference between ck using 40 gy ( eqd2 ) and imrt using 65 gy ( eqd2 )  . 
one possibility is that imrt was used to treat more nonnasopharyngeal cancers than ck , which is identied as a better prognosis factor after reirradiation [ 11 ]  . therefore , at this time , the eqd2 calculation in hypofractionated sbrt may contain several uncertainties if we apply it to compare conventionally fractionated imrt and hypofractionated sbrt . there were substantial cases of grade 3 or worse toxicity in both groups . 
a total of 48 patients ( 27% ) presented with grade 3 or worse toxicity , including 17 with grade 5 toxicity not only in photon radiotherapy but also in cp . 
first , modied patient selection criteria could help avoid cbos ( exclude patients with neck area invasion or skin invasion )  . a phase i / ii dose escalation study using sbrt for patients without these risk factors was safely performed [ 21 ]  . 
second , an every - other - day sbrt protocol , instead of a daily protocol , could reduce cbos incidence [ 22 ]  . recently , takiar et al . 
 [ 23 ] reported 2 - year and 5 - year os rates of 51% and 32% in 227 patients treated with imrt , which appears better than the rate reported in previous 3dconformal radiotherapy series published in rtog 99 - 11 and 96 - 10 ( 2 - year os , 1525% )  . 
in the old series , grade 3 or worse toxicity was noted in 2540% of patients , including treatment - related death in nearly 20% ( rtog 99 - 11 , 16% ; rtog 96 - 10 , 24% )  . 
 [ 23 ] noted grade 3 or worse toxicity in 32% of patients at 2 years and in 48% of patients at 5 years , which was associated with dysphagia and odynophagia ( treatment volume , > 50 cm3 ) , and only three treatment - related deaths were noted . 
the authors speculated that selected patients with a tumor volume < 25 cm3 were also evaluated for sbrt based on this protocol , particularly those who could not tolerate 67 weeks of conventional fractionation . 
although a prospective trial with a larger number of patients and longer follow - up period should be performed , it could be difcult because of economic barriers . conclusion cp provided suprior survival outcomes when compared to the outcomes with photon radiotherapy . 
younger patients with a larger ptv may experience grade 3 or worse toxicity . strahlenther onkol ( 2017 ) 193 : 525533 acknowledgements the authors would like to thank enago for the english language review and crimson interactive for german language review . compliance with ethical guidelines conict of interest h . 
mai 2017 springer - verlag berlin heidelberg 2017 hintergrund im rahmen einer doppelt verblindeten , plazebokontrollierten studie , welche federfhrend im general hospital massachusetts durchgefhrt wurde , wurde der einuss einer zustzlichen antiandrogenen therapie ( bicalutamid 150 mg ) zur salvage - radiotherapie bei prostatakarzinompatienten evaluiert . 
primres endziel dieser randomisierten studie [ 1 ] war das gesamtberleben ; sekundre endpunkte waren unter anderem das krankheitsspezische , das metastasenfreie und das progressionsfreie berleben . es wurde suspiziert , dass durch die zustzliche hormonelle therapie die tumorprogression reduziert und somit die todesrate um 28 , 5 % bei 230 ntigen events verringert werden kann . patienten und methode es wurden patienten mit karzinomen pt2 pn0 r + bzw . 
pt3 pn0 nach radikaler prostatektomie ( rpe ) und lymphadenektomie eingeschlossen . die patienten durften frhestens 8 wochen nach rpe ein nachweislich erhhtes prostataspezisches antigen ( psa ) haben , sodass sowohl psa - persister nach operation aber auch patienten mit biochemischem rezidiv kandidaten fr die studie waren ( psa vor beginn der radiotherapie 0 , 24 , 0 ng / ml )  . 
alle patienten erhielten eine alleinige 2 - doder 3 - d - geplante lokale bestrahlung der prostataloge mittels photonen 610 mv bis zu einer gesamtherddosis von 64 , 8 gy ( 36 fraktionen zu je 1 , 8 gy in 5 fraktionen / woche )  . 
zu beginn der bestrahlung wurde den patienten dann entweder bicalutamid 150 mg einmal tglich fr die dauer von 24 monaten oder ein plazebo verabreicht . ergebnisse zwischen 1998 und 2003 wurden 840 patienten randomisiert . 
der endgltigen auswertung standen letztlich die daten von 760 patienten zur verfgung : 384 patienten im bicalutamid - arm und 376 im plazeboardas mediane follow - up der lebenden patienten lag bei 13 jahren . 
in der multivariaten analyse zum gesamtberleben zeigten sich ein psa - wert vor radiotherapie mit > 1 , 5 ng / ml , ein gleason - score von 810 sowie ein alter von > 65 jahre und ein karnofsky - status von 80 bzw . 
den grten benet in einer post - hoc - subgruppenanalyse bezogen auf das gesamtberleben zeigten patienten mit einem hohen psawert vor radiotherapie ( > 1 , 5 ng / ml ) oder einem gleasonscore von 7 . 
hinsichtlich der nebenwirkungen berichteten 70 % der patienten im bicalutamidarm gegenber 11 % im plazebo - arm ber gynkomastie . die rate an schweren kardialen nebenwirkungen ( = tod ) zeigte keinen signikanten unterschied und die rate an lebertoxizitt vom grad 2 lag bei 2 , 4 % im bicalutamidvs . 
1 , 1 % im plazebo - arm . schlussfolgerung der autoren die addition von bicalutamid fr die dauer von 24 monaten zur salvage - radiotherapie fhrt bei prostatakarzinompatienten zu signikant verbesserten berlebensraten , signikant niedrigeren raten an fernmetastasen und einer signikanten reduzierung der tumorspezischen todesraten . kommentar shipley und seine kollegen konnten mit der vorliegenden randomisierten studie einen signikanten berlebensvorteil durch eine zustzliche antiandrogene therapie mit bicalutamid 150 mg ( 2 jahre ) zur salvage - radiotherapie nachweisen . 
es darf jedoch suszipiert werden , dass auch mit einer lhrh - therapie ein hnlicher effekt wie mit bicalutamid erreicht worden wre . alle patienten erhielten in der hier besprochenen studie von shipley und mitarbeitern nicht eine primre , sondern eine salvage - radiotherapie . 
im vergleich zu den in unserem land geltenden leitlinien wird auch hier ein mglichst frhzeitiger therapiebeginn bei steigenden psa - werten empfohlen , und zwar am besten noch vor erreichen von 0 , 5 ng / ml . 
der mediane psa - wert lag in der shipley - studie bei 0 , 6 ng / ml , doch mehr als 40 % der patienten hatten bereits vor beginn der strahlentherapie einen psa - wert von 0 , 74 , 0 ng / ml . 
es darf erinnert werden , dass die studie schlielich schon vor 20 jahren begonnen wurde . auf eine beckenbestrahlung wurde berhaupt verzichtet , da entsprechend dem studienprotokoll alle patienten neben der rpe auch eine lymphadenektomie erhielten und dort ohne tumorbefall ( pn0 ) sein mussten . 
ob die lymphadenektomie standardisiert war also immer eine extendierte lymphadenektomie erfolgte oder es sich lediglich um eine limitierte lymphadenektomie handelte , wird in der arbeit leider nicht berichtet . mithilfe moderner therapietechniken , wie der intensittsmodulierten strahlentherapie ( imrt ) und der volumenmodulierten arc - therapie ( vmat ) , und unter zuhilfenahme einer optimierten bildgebung ( darstellung des prostataspezischen membranantigens psma mittels positronenemissionstomographie pet = psmapet ) knnen heutzutage , v . 
zustzlich interessant ist , dass sich in der subgruppenanalyse bei patienten mit einem niedrigen psa vor beginn der radiotherapie ( hier deniert als < 0 , 7 ng / ml ) kein vorteil durch die addition von bicalutamid fand . fazit die addition von bicalutamid fr die dauer von 24 monaten zur salvage - radiotherapie fhrt bei prostatakarzinompatienten zu signikant verbesserten berlebensraten , zu signikant niedrigeren raten an fernmetastasen und zu einer verminderung der tumorspezischen todesraten . die wesentliche frage allerdings , ob nun alle patienten mit psa - rezidiv nach rpe zur salvage - strahlentherapie auch eine begleitende antiandrogene hormontherapie erhalten sollen , kann unseres erachtens aufgrund der vorliegenden studie nicht eindeutig beantwortet werden . gregor goldner , wien interessenkonikt g . 
carrie c , hasbini a , de laroche g et al ( 2016 ) salvage radiotherapy with or without short - term hormone therapy for rising prostate specic antigen concentration after radical prostatectomy ( getug - afu16 ) : a randomized , multicentre , open - label phase 3 trial . lancet oncol 17 : 747756 1 . 
this study assessed the symptom burden of palliative and curative - intent radiation oncology patients . patients and methods prior to rst consultation and at the end of rt , all adult cancer patients planned to receive fractionated percutaneous radiotherapy ( rt ) were asked to answer the edmonton symptom assessment scale ( esas ; nine symptoms from 0 = no symptoms to 10 = worst possible symptoms )  . 
mean values were used for curative vs . palliative and prepost comparisons , and the clinical relevance was evaluated ( symptom values 4 )  . results of 163 participating patients , 151 patients ( 90.9% ) completed both surveys ( 116 curative and 35 palliative patients )  . 
before beginning rt , 88.6% of palliative and 72.3% of curative patients showed at least one clinically relevant symptocurative patients most frequently named decreased general wellbeing ( 38.6% ) , followed by tiredness ( 35.0% ) , anxiety ( 32.4% ) , depression ( 30.0% ) , pain ( 26.3% ) , lack of appetite ( 23.5% ) , dyspnea ( 17.8% ) , ( cid : 2 ) philipp krner philipp.koerner@zzm.uzh.ch interdisziplinres zentrum palliativmedizin , universittsklinikum wrzburg , josef - schneider - str . 
the results prove the need of systematic symptom assessment and programs for early integrated supportive and palliative care in radiation oncology . keywords radiation oncology quality of life palliative care screening pain patientenberichtete symptome im strahlentherapieverlauf klinisch relevante symptombelastungen bei patienten mit palliativer und kurativer therapieintention zusammenfassung hintergrund vorteile einer patientenberichteten symptomerfassung mit integrierter palliativer versorgung sind inzwischen gut belegt . 
die studie untersuchte die symptomstrahlenther onkol ( 2017 ) 193 : 570577 belastung von patienten mit palliativer und kurativer strahlentherapie ( rt )  . patienten und methoden alle volljhrigen tumorpatienten mit geplanter fraktionierter perkutaner rt wurden vor dem erstgesprch und am ende der rt mit der palliativmedizinische edmonton symptom assessment scale ( esas ) zu 9 symptomen befragt ( 0 = minimale symptomausprgung ; 10 = maximale symptomausprgung )  . 
postoperativ wurden mittelwerte verwendet und die klinische relevanz ( symptomstrke 4 ) ermittelt . ergebnisse von den 163 eingeschlossenen patienten beantworten 151 patienten ( 90 , 9 % ) beide fragebgen ( 116 kurative , 35 palliative patienten )  . 
vor rt zeigten 88 , 6 % der palliativund 72 , 3 % der kurativpatienten mindestens 1 interventionsbedrftiges symptobei den kurativpatienten waren dies einschrnkungen im allgemeinbenden ( 38 , 6 % ) , mdigkeit ( 35 , 0 % ) , angst ( 32 , 4 % ) , traurigkeit ( 30 , 0 % ) , schmerz ( 26 , 3 % ) , appetitverlust ( 23 , 5 % ) , dyspnoe ( 17 , 8 % ) , benommenheit ( 8 , 0 % ) und belkeit ( 6 , 1 % )  . 
bei palliativpatienten hatten mdigkeit und bei den kurativen patienten schmerzen , mdigkeit , belkeit , benommenheit , appetitlosigkeit und einschrnkungen im allgemeinbenden signikant zugenommen . schlussfolgerung die patientenberichtete symptomerfassung wurde erfolgreich in der routine der radioonkologie umgesetzt . 
die ergebnisse belegen den bedarf einer systematischen symptomerfassung und eines programms zur frhzeitig eingebundenen supportiven und palliativen versorgung in der strahlenonkologie . schlsselwrter radioonkologie lebensqualitt palliative versorgung screening schmerz background combined standard oncology care and palliative care should be considered early in the course of illness for any patient with metastatic cancer and / or high symptom burden [ 27 ]  . 
therefore , international guidelines mandate a systematic patient - reported assessment of physical symptoms und psychosocial burden in cancer patients , in order to enable appropriate palliative , supportive , or psychosocial care [ 14 , 17 , 18 ]  . 
several screening instruments have been well established , e.g. , the distress thermometer [ 21 ] , the hospital anxiety and depression scale ( hads ) for anxiety and depression [ 22 ] , and analogue scales for pain alone or in combination with the assessment of other symptoms . 
one of the latter tools is the edmonton symptom assessment scale ( esas ) , a symptom - orientated numerical scale assessing nine symptoms , each ranging from 0 ( no symptom ) to 10 ( worst possible symptom ) [ 4 ]  . 
cancer care ontario as well as the new german s3 guideline palliative care for adult cancer patients with incurable disease propose the esas or the revised esasr for symptom load screening [ 2 , 5 , 10 , 18 , 3133 ]  . 
at the princess margaret cancer centre in toronto , the esas is implemented hospital - wide in the distress assessment and response tool ( dart ) program , as well as being used for symptom assessment in palliative care consultations [ 12 , 19 ]  . there are few studies on patient - reported physical symptom load in radiation oncology . 
analyzed physical and psychosocial symptom burden in curative and palliative patients prior to the beginning of radiotherapy ( rt ) , with 31% of the patients reporting clinically - relevant pain . at least one symptom was reported by 71% of all patients [ 16 ]  . 
in a multicenter pattern - of - care study , the german version of esas , the minimal documentation system ( midos , [ 28 ] ) , was used for physician - assessed symptom documentation in palliative rt . 
at t1 , one or more clinically relevant symptoms were reported in 840% of patients [ 23 ]  . maurer and colleagues used the hads for screening and monitoring anxiety and depression during rt . 
before rt , 41% of patients showed anxiety and 33% depression , with a signicant decrease during the course of therapy [ 20 ]  . the esas has been used in the rapid response palliative radiotherapy program toronto for symptom screening and longitudinal symptom monitoring since 1999 . 
during initial consultation , 1559% of patients presented for palliative rt reported one or more clinically relevant symptom , mostly fatigue ( 69% ) , lack of appetite ( 51% ) , or pain ( 49% ) [ 14 ]  . 
the international bone metastases consensus working party dened response categories for alleviation of pain after palliative rt of bone metastases , utilizing the esas pain scale for symptom monitoring [ 8 ]  . in the present study , the esas was rst used in curative and palliative patients prior to beginning a comprehensive intervention to improve symptom management . 
exclusion criteria were benign diseases , being under the age of 18 years , having insufcient german language skills , not being able to consent , and undergoing rt with one - time stereotaxy , seed implantation , or total body irradiation . 
participants completed the esas once while waiting for their initial clinical contact with the radiation oncologist and once again at the end of individual rt ( 3 days )  . 
1 percentages of patients with clinically signicant symptom distress ( i.e. , one or more esas item > 3 ) ; a patients treated with curative intent , b patients treated with palliative intent . 
the threshold for statistical signicance was set at p ( cid : 2 ) 0.05. results patient sample a total of 163 patients agreed to participate in the study and completed the rst screening questionnaire ( 89.1% of all eligible patients )  . 
one of the curative patients was treated in the emergency department as a consequence of a comorbidity , one patient revoked consent to rt , and in one patient , therapy was aborted due to aggravation of general condition . 
last mentioned was also the case for each of the 6 palliative patients : 2 of them died during the course of rt and one patient died 2 days after completing rt . 
further studies are needed to investigate possible cut - off points in performance status to separate patients able to answer the survey on their own from those in need of personal assistance . discussion the present study investigated the practical use of the esas for patient - reported symptom assessment during rt . 
to the best of our knowledge , this is the rst study using symptom scales for curative as well as for palliative patients undergoing rt . response rate the esas screening was very well accepted and feasible in daily practice . 
state that a healthcare professional should be present for clarication and advice , leading to improvement of accuracy , efciency , and ease of completion of the esas [ 31 , 33 ]  . 
lack of energy was clinically relevant in 66.6% , generalized fatigue in 59.6% of the patients , followed by cough ( 51.8% ) , pain ( 48.3% ) , dry mouth ( 47.8% ) , lack of appetite ( 45.4% ) , and dyspnea ( 43.6% ) [ 24 ]  . 
2 patient - reported symptom load , esas items in rst and second survey , comparison of mean values ; a patients treated with curative intent , b patients treated with palliative intent . 
these data illustrate the necessity of implementation of patient - centered symptom assessment and the design of linked interventions for screening - positive patients , as is recommended in the s3 guideline palliative care , as well as in international guidelines and programs [ 1 , 14 , 19 , 21 , 22 ]  . changes of symptoms in curative patients there was a signicant increase in pain , tiredness , nausea , drowsiness , lack of appetite , and impairment of wellbeing . 
found a comparable increase of clinically relevant physical complaints from 34.7% at t1 to 42.2% at t2 [ 3 ]  . signicantly fewer patients in the palliative group reported clinically relevant levels of pain at t2 compared to t1 , although the mean pain severity did not signicantly decrease from t1 . 
most symptoms remained rather stable , possibly due to the relatively small dose , which might limit side effects . another interpretation could be the more patient - centered supportive approach for palliative patients compared to curative patients . 
in a comparable multicenter study , in which the department of radiation oncology of the university hospital wrzburg participated , about 40% of palliative patients reported severe or very severe symptoms at t1 , but showed a physician - documented signicant reduction of pain , dyspnea , and neurological decits at the end of rt , as well as a signicant increase in fatigue , as found in the present study [ 23 ]  . it remains unclear whether the decrease in pain in palliative patients in our study can be interpreted as an effect of rt , successful pain management , or rather as an integrated palliative care approach . 
in a study by vuong , 33% of patients receiving rt with palliative intent showed an undertreatment of padespite the use of strong opioids in 29.9% of the patients with severe pain , a small increase in pain could be observed in the last few years [ 30 ]  . 
patients with different stages of disease , performance status , and tumor progression , as well as patients on different medication and radiation schedules ( fractions ) answered the same questions . 
finally , it will be important to assess the extent to which treatment staff accept the implementation and use of the screening [ 3 , 6 ]  . funding this study was funded by german cancer aid ( number 110866 )  . compliance with ethical guidelines conict of interest p . 
van oorschot declare that they have no competing interests . ethical standards all procedures followed were in accordance with the ethical standards and with the helsinki declaration of 1975 ( in its most recently amended version )  . 
mehta6 patrick cheung7 arjun sahgal7 received : 6 march 2017 / accepted : 22 march 2017 / published online : 19 april 2017 springer - verlag berlin heidelberg 2017 abstract background practice guidelines have been developed for early - stage and locally advanced non - small cell lung cancer ( nsclc )  . 
this is true for locoregional relapse after initial stereotactic radiotherapy ( stereotactic body radiation therapy or stereotactic ablative radiotherapy ; sbrt or sabr ) , an increasingly utilized curative treatment option for stage i nsclc . methods a consortium of expert radiation oncologists was established with the aim of providing treatment recommendations . 
in this case , a patient developed local and mediastinal relapse after sabr ( 45 gy , 3 fractions ) , comparable to the tumor burden in de novo stage iiia ( cid : 2 ) carsten nieder , md carsten.nieder@nlsh.no 1 department of oncology and palliative medicine , nordland hospital , 8092 bod , norway institute of clinical medicine , faculty of health sciences , university of troms , troms , norway 3 department of radiation oncology , maastro clinic , maastricht , the netherlands 4 department of radiation oncology , university of colorado school of medicine , aurora , co , usa 5 department of radiation oncology , university hospital zurich , zurich , switzerland 6 department of radiation oncology , miami cancer institute , miami , fl , usa 7 department of radiation oncology , sunnybrook health sciences centre and university of toronto , toronto , canada nsclc . 
if the patient was not a surgical candidate , and / or refused surgery , denitive chemoradiation was recommended , including retreating the primary to full dose . european participants were more in favor of a non - surgical approach . 
in the absence of high - quality prospective trials for recurrent nsclc , all treatment options recommended in current guidelines for stage iii disease can be considered in clinical scenarios such as this . keywords chemoradiotherapy salvage therapy guideline survival radiation oncologists rebestrahlung von wiederkehrendem lymphknotenpositiven nicht - kleinzelligem bronchialkarzinom nach vorangegangener stereotaktischer strahlentherapie im stadium i eine multiinstitutionelle behandlungsempfehlung zusammenfassung hintergrund fr frhe und lokal fortgeschrittene stadien des nicht - kleinzelligen bronchialkarzinoms ( nsclc ) wurden behandlungsleitlinien publiziert . 
da516 strahlenther onkol ( 2017 ) 193 : 515524 zu gehrt ein lokoregionales rezidiv nach stereotaktischer strahlentherapie ( sabr ) , einer modalitt , die immer fter im stadium i angewandt wird . methoden eine expertengruppe wurde etabliert , um empfehlungen zur rezidivbehandlung zu erarbeiten . 
insgesamt 6 radioonkologen brachten die behandlungsempfehlungen ihrer institution ein dem fall entwickelte ein patient ein lokalund mediastinalrezidiv nach sabr ( 45 gy , 3 fraktionen ) , vergleichbar mit der ausbreitung beim de - novonsclc im stadium iiia . 
solange keine prospektiven daten fr rezidivierte nsclc vorliegen , knnen in klinischen szenarien , wie dem hier geschilderten , alle behandlungsoptionen der leitlinien fr das stadium iii erwogen werden . schlsselwrter radiochemotherapie salvagebehandlung leitlinien berleben radioonkologen introduction for many common clinical scenarios involving radiation therapy , treatment approaches can easily be derived from guidelines , which are generally based on prospective clinical trials . 
among these scenarios is recurrent nonsmall cell lung cancer ( nsclc ) following initial hypofractionated stereotactic radiotherapy ( stereotactic body radiation therapy or stereotactic ablative radiotherapy ; sbrt or sabr ) [ 1 ]  . 
although initial studies on sabr were heterogeneous ( comprised of both prospective and retrospective series with limited patient numbers , in part without histological conrmation of malignancy ) , the promising results prompted several phase ii trials and , later , population - based studies and propensity - matched analyses . 
however , rosel ( a dutch trial ) and stars ( an international trial ) shared similar entry criteria and study design , allowing for a pooled analysis of 58 patients [ 5 ]  . 
on the basis of these retrospective and prospective studies , sabr is considered a reasonable option for early nsclc [ 6 ]  . despite the adoption of sabr into clinical practice across much of the world , salvage treatment options after initial sabr have not been studied . 
therefore , it was decided to distribute to an expert group a real - world case managed at the rst authors institution , and to ask for treatment recommendations using a well - dened , standardized approach . 
both nihilistic and overly aggressive management has the potential to harm patients , and the art of oncology is to nd the right balance between side effects and efcacy . methods study design representatives from six academic institutions , which had different collaborations from the past , were provided with diagnostic information including imaging studies and medical history . 
within their own institutions , the six participants presented the case to their collaborators / tumor boards . treatment recommendations were compiled using a standardized template requesting information including , but not limited to , technique , fractionation , and institutional dose constraints . 
results from each institution were collated by the primary author and presented back to the participating radiation oncologists without disclosing the recommendation by institutional site . strahlenther onkol ( 2017 ) 193 : 515524 fig . 
they also showed rib fractures clinical information distributed to the sites a 67 - year - old male caucasian patient , an active smoker ( more than 40 pack years ) , had a chest x - ray taken before hip surgery in august 2011 . 
lung function tests revealed forced expiratory volume in 1 s ( fev1 ) 1.4 liter ( 45% ) , forced vital capacity ( fvc ) 1.9 liter ( 47% ) , and diffusing capacity of the lungs for carbon monoxide ( dlco ) 4.4 mmol / min / kpa ( 48% )  . 
he was unable to quit smoking . in march 2013 , the right upper lobe nsclc was treated with sabr ( 3 fractions of 15 gy prescribed to the 60% isodose line )  . 
further local response was evident by novem518 strahlenther onkol ( 2017 ) 193 : 515524 a in november 2014 , 18f - uorodeoxyglucose positron - emission tomography computed tomography ( 18fdg - pet - ct ) imaging showed fig . 
4c shows representative images of the newest ct scan ( lung window )  . results the natural course after august 2011 suggests a somewhat indolent lesion , and the fact that the patient had not developed metastatic disease by 2013 supported the recommendation of an aggressive therapeutic approach . 
although the pet - ct in 2013 did not show abnormal fdg uptake in the mediastinal nodes , the increase in size of the primary lung cancer between 2011 and 2013 correlates with an increased risk of metastatic mediastinal lymph nodes [ 7 ]  . 
according to data from the memorial sloan kettering cancer center , the risk of mediastinal nodes without uptake on pet - ct increases with size of the primary tumor , the suvmax of the primary , and with adenocarcinoma histology [ 8 ]  . 
mediastinoscopy would only have been performed before surgery , but not in all institutions whose recommendation included evaluation for surgery . three institutions recommended evaluation for surgery . the rst step in this surgical approach would be active smoking cessation and pulmonary rehabilitation for a minimum of 46 weeks , followed by cardiopulmonary evaluation . 
if the patient was a candidate for surgery , institution 1 considered resection ( including partial rib / chest wall resection to ensure negative margins ) , but this should only be considered with the intent of achieving negative margins . the resection should also focus on nodal sampling for categorical determination of n2 disease . 
if the patient was not a surgical candidate , and / or refused surgery , institution 1 considered ebus and nodal staging , followed by denitive chemoradiation , including retreating the primary to full dose , with the clear understanding of the possibility of severe local chest wall brosis as a long - term complication . institution 2 recommended mediastinoscopy to rule out n3 disease , and preoperative chemoradiation ( total dose 45 gy in 25 fractions ) followed by surgical resection . 
in their opinion , this approach had the advantage of potentially eradicating all gross disease , without the need to apply a radical radiotherapy dose , especially in this retreatment setting in the lung and chest wall . 
assuming no evidence of distant metastases , and an r0 resection performed without the nding of residual positive lymph nodes , institution 3 advised postoperative radiation therapy ( 54 gy ) to the lymph nodes in the right hilar and right lower paratracheal region . 
if two cycles of chemotherapy were completed without evidence of progression , but the patient was not deemed to be a surgical candidate , then institution 3 would then consider treating with concurrent chemoradiation ( cisplatin / etoposide and 45 gy in 15 daily fractions over 3 weeks )  . three other institutions recommended primary chemoradiation . 
one of these would choose initial chemotherapy followed by a concurrent hypofractionated 3 - week regimen , largely comparable to that considered by institution 3 ( tables 1 and 2 )  . 
improved screening may lead to an increase in patients with this diagnosis [ 13 ]  . since the results of a recent pooled analysis suggest that sabr is better tolerated and might lead to better survival compared to surgery [ 5 ] , many radiation oncologists are convinced that sabr can be considered a viable treatment option in operable patients requiring a lobectomy , and not only a compromise for those patients that the surgeons are reluctant to take to surgery . 
the corresponding gures were 12 , 16 , and 16% in the study by spratt et al . [ 16 ] , which included 366 patients with a median tumor size of 2 cm ( maximum 5 cm , all tumors were biopsy proven )  . other studies conrm that regional nodal recurrence is a potential threat to patients and that this type of recurrence , comparable to development of distant metastases , might lead to shorter survival [ 17 ]  . the case presented here features local and regional recurrence as well as treatment - related toxicity and serious copd . 
most likely , the clinical course would have been less complicated if the patient had completed all diagnostic procedures and started treatment already in 2011 , regardless of whether he had consented to surgery or sabr . 
in patients with isolated nodal recurrence after sabr who received salvage mediastinal radiotherapy , the 1 - year actuarial progression - free survival rate was 75% and the locoregional control rate 84% [ 18 ]  . 
despite numerous guidelines [ 2227 ] , different treatment options are possible and advocated , resulting in variable clinical practice even for the subgroups of patients with technically resectable and unresectable disease . 
according to the american college of chest physicians , patients with good performance status and minimal weight loss treated with combined chemoradiation have better survival than those treated with radiotherapy alone . 
neoadjuvant therapy followed by surgery is neither clearly better nor clearly worse than denitive chemoradiation , with the exception of increased early postoperative mortality in some subgroups in at least one major randomized trial [ 24 ]  . 
the participating institutions commented on the importance of performing such surgery in centers with a low perioperative mortality rate . according to the american college of radiology ( acr ) appropriateness criteria lung cancer panel there is limited level i evidence to guide patient selection for induction , postoperative radiotherapy ( port ) or denitive radiotherapy [ 25 ]  . 
induction chemotherapy followed by surgery port may also be an option in n2 patients [ 25 ]  . according to guidelines from the american society for radiation oncology ( astro ) and the american society of clinical oncology ( asco ) , dose escalation beyond 60 gy in the context of combined modality concurrent chemoradiation is not routinely recommended [ 26 , 27 ]  . 
indeed , modern - era dose - escalation trials have produced mixed results , with excess mortality from higher doses in at least one major trial [ 28 ] , and have been increasingly linked to higher cardiac and pulmonary dose , implying that safer techniques for delivery of higher doses could perhaps overcome this limitation . 
current data fail to support a clear role for consolidation therapy after chemoradiotherapy , with the understanding that such a practice was not supported by the hoosier oncology group maintenance docetaxel trial , following two cycles of full - dose cisplatin / etoposide [ 29 ]  . 
important questions remain regarding the ideal concurrent chemotherapy regimen and optimal management of patients with resectable stage iii disease [ 26 , 27 ]  . basically , the present recommendations regarding the scenario of recurrent stage iiia - like disease after initial sabr for stage i disease reect the questions and uncertainties that are discussed in the stage iii guidelines . 
this reects ndings from several recent studies and reviews suggesting that both sabr followed by chemoradiation and chemoradiation followed by sabr to peripheral lesions carries acceptable risks of toxicity [ 3033 ] , although normal tissue tolerance is less thoroughly dened than in patients who have not received previous thoracic radiotherapy [ 34 , 35 ]  . 
high - grade toxicity was uncommon ( one grade 3 late dyspnea ) , but the median follow - up was only 10 months , which also limits efcacy analysis . 
doses to critical structures were converted to biologically effective dose , expressed as 2 gy per fraction equivalent dose . while no grade 4 toxicity was observed , a minority of patients developed lower - grade chest wall , lung , brachial plexus , and nerve toxicities . 
in - eld 1and 2 - year actuarial control rates of 79 and 65.5% were observed , respectively ; 1and 2 - year actuarial survival rates were 52 and 37% , respectively . in the current study , variation was observed in target volume delineation , dose prescription , selection of organs at risk that should be contoured , and treatment planning , although most institutions preferred imrt and tended to limit the chest wall dose and / or avoid hotspots there . 
longterm local control beyond 4 years was seen in a minority of patients ( < 15% ) , including patients treated outside of the trial in the rst authors institution . 
two institutions considered a comparable approach , while the others were willing to prescribe higher biologically equivalent doses . doseresponse relationships for nsclc have been analyzed by different groups , including a report on 1390 participants in radiation therapy oncology group ( rtog ) trials [ 43 ]  . 
it is known that local control after chemoradiation ( 60 gy ) is not optimal [ 4448 ] , but dose escalation to 74 gy did not show the anticipated improvements [ 28 ] and was primarily associated with increased cardiopulmonary mortality due to higher doses delivered to these organs at risk . on the basis of these considerations , a reirradiation dose of 6066 gy can be prescribed if sufcient sparing of organs at risk can be achieved . 
the latter objective might be facilitated by adaptive replanning , breath - hold image - guided techniques , and proton beams , which are under investigation in numerous prospective clinical trials [ 49 ]  . 
based on these observations , we evaluated patients receiving potentially excessive doses to the spinal cord within minimal volumes . patients and methods patients receiving radiotherapy between june 2010 and may 2015 using the novalistm ( varian , palo alto , ca , usa ; brainlab , heimstetten , germany ) radiosurgery system were retrospectively analyzed . 
a total of 56 patients with 62 treated lesions that had been prescribed radiation doses close to the spinal cord potentially higher than the common 50 gy 2 - gy equivalent - dose ( eqd2 ) constraint were selected for further analysis . 
of these patients , 26 with 31 lesions had no history of previous irradiation , while 30 patients with 31 lesions had been previously irradiated within the treatment eld . results according to different dose evaluation approaches ( spinal canal , spinal cord contour ) , 16 and 10 out of authors contribution s . 
all authors read and approved the nal manuscript . ( cid : 2 ) sebastian zschaeck sebastian.zschaeck@charite.de 1 klinik fr radioonkologie und strahlentherapie , charit centrum tumormedizin cc14 , augustenburger platz 1 , 13353 berlin , germany 31 primary irradiated lesions infringed constraints . 
no radiation myelitis or radiomorphological alterations were observed during follow - up . conclusion this study adds to the increasing body of evidence indicating that excessive spinal cord doses within a minimal volume , especially in a reirradiation setting with topographically distinct high - point doses , may be given to patients after careful evaluation of treatmentand tumorassociated risks . keywords radiosurgery reirradiation toxicity myelitis myelopathy dosisbeschrnkungen fr das rckenmark im zeitalter der hochprzisionsstrahlentherapie retrospektive auswertung 62 spinaler / paraspinaler lsionen mit potenzieller berschreitung kleinstvolumiger rckenmarksdosen zusammenfassung zielsetzung um das risiko einer radiogenen myelitis zu minimieren , sind klinisch gebruchliche dosisobergrenzen fr das rckenmark mit 50 - gy - maximaldosis sehr restriktiv . 
unter diesem aspekt wurden patienten ausgewertet , die kleinstvolumig mit potenziell berhhten rckenmarksdosen bestrahlt wurden . 562 strahlenther onkol ( 2017 ) 193 : 561569 patienten retrospektiv ausgewertet wurden patienten , die zwischen juni 2010 und mai 2015 mit dem novalistm - radiochirurgiesystem ( varian , paulo alto , ca , usa ; brainlab , heimstetten , deutschland ) behandelt wurden . 
fr weitere analysen wurden 62 lsionen bei 56 patienten mit potenziell berhhter rckenmarksdosis ( > 50 gy ) , berechnet als 2 - gy - quivalenzdosis ( eqd2 ) , ausgewhlt . 
von diesen waren 26 patienten mit 31 lsionen ohne vorbestrahlung und 30 patienten mit 31 lsionen bereits im gleichen bereich vorbestrahlt . ergebnisse unter verwendung verschiedener dosisevaluationsverfahren ( spinalkanal , minimal konturierter rckenmarksbereich ) berschritten 16 und 10 der 31 erstmalig bestrahlten lsionen die grenze . 
whrend der nachsorge wurden keine radiogene myelitis oder rntgenmorphologische vernderungen beobachtet . schlussfolgerung die studie liefert hinweise darauf , dass nach sorgsamem abwgen von behandlungsund tumorassoziierten risiken eine kleinstvolumige berdosierung des myelons in einzelfllen mglich erscheint , insbesondere bei rebestrahlung mit topographisch unterschiedlich lokalisierten maximaldosen . schlsselwrter radiochirurgie rebestrahlung toxizitt myelitis myelopathie myelopathy is a serious potential side effect of radiotherapy . therefore , current constraints aim to minimize the risk of radiation myelitis . 
for normofractionated spinal cord doses up to 55 gy , the myelopathy risk is considered to be around 1% [ 1 ] and this risk increases to approximately 5% for higher radiation doses up to 60 gy [ 1 , 2 ] , with a latency of 6 months or more after irradiation [ 3 ]  . 
nevertheless , various publications suggest that a volume dependency for spinal cord irradiation might exist . some animal studies have shown that irradiation of a small volume is feasible up to higher doses without neurological sequelae [ 5 ]  . 
van der kogel suggested that the dosevolume effect within the spinal cord may be marginal for cord lengths above 12 cm , but seems to play an important role for an irradiated cord length below 1 cm [ 5 ]  . 
however , conicting preclinical and clinical data exist , particularly if the fractionation regimes are taken into account : medin and colleagues established a pig model that resembles singlefraction radiosurgery and did not nd a dosevolume effect [ 6 , 7 ]  . 
however , in a retrospective patient series with highdose single - fraction radiotherapy for hemangioblastomas , there was some evidence for a dosevolume effect if only very small volumes of the spinal cord received excessive dosage [ 8 ]  . 
this also seems to be true for normofractionated radiotherapy , as suggested by the pioneering study on myelopathy patients by abbatucci and colleagues [ 9 ]  . the issue of a volume effect in spinal irradiation is gaining novel importance with the increasing use of highly conformal photon radiotherapy techniques and particle therapy . with these methods , a steep decrease of the prescribed radiation dose is feasible [ 10 , 11 ]  . 
however , if the spinal cord is adjacent to irradiated structures , a uniform spinal cord constraint of 50 gy hampers the advantageous applicability of these novel techniques . herein , we describe our institutional experience with high - dose radiotherapy close to the spinal cord with the in - house constraint that minimal volumes ( < 1 cm3 ) of the spinal cord may receive doses higher than 50 gy . patients and methods patient and treatment characteristics we retrospectively identied patients who were irradiated between june 2010 and may 2015 using the novalistm radiosurgery system ( varian , palo alto , ca , usa ; brainlab , heimstetten , germany ) and had received radiotherapy to the vertebral or paravertebral space . 
this strategy identied 180 patients with 191 treated lesions for further analysis . of these , only patients with either a prescribed maximal 2 - gy equivalent dose ( eqd2 ) of 50 gy or higher , or patients with reirradiation within the same vertebral volume were selected for further analysis . 
dose per fraction + = 2 + = furthermore , the analysis was restricted as follows : since the adult spinal cord ends at the height of the second lumbar vertebral body ( l2 ) [ 12 ] , patients who received radiotherapy to the cervical ( c ) , thoracic ( t ) , or rst to third lumbar vertebral bodies were included in the analysis of spinal cord dose . 
if no further information was available , the patient was censored at the last follow - up visit with sufcient information . myelopathy was dened according to common terminology criteria for adverse events ( ctcae ) 3.0 as myelitis grade ii or higher [ 14 ]  . 
however , in some cases , delineation of the spinal canal according to bony boundaries was not deemed expedient ( especially in a postoperative setting ) and , vice versa , cord delineation was not always feasible . for evaluation of spinal cord dose , two different approaches were undertaken : the rst approach used the maximal delivered dose per fraction and the spinal canal structure for calculation of spinal cord dose , i . 
maximum eqd2 within the same spinal cord segment was calculated for prior radiotherapy and reirradiation , and summed up as suggested by other publications [ 16 , 17 ]  . statistical analysis and software survival analysis with respect to overall survival ( os ) was measured from the end of radiotherapy to death . 
patients who did not keep follow - up appointments and for whom information on survival or neurological status was thus unavailable were censored at the date of last follow - up . 
the association of os and initial radiotherapy or reirradiation was analyzed using univariate cox proportional hazard regression using the spss software version 24 ( ibm corp . , spss statistics for windows , armonk , ny , usa )  . 
the remaining lesions had either no history of pain ( 10 cases ) or insufcient documentation ( 9 cases )  . median follow up of these 10 and 16 lesions was 21 and 17 months , respectively . 
as an additional risk factor , 7 and 8 of these 10 and 16 lesions , respectively , had a history of ( peri ) spinal surgery within the same vertebral segment prior to radiotherapy . 
none of the identied patients presented myelopathy ; follow - up mri was available for 9 of these 17 patients , with none of the mris showing signs of radiation - induced myelopathy . 
1 shows example treatment plans and follow - up imaging from 2 patients . the remaining 31 lesions in 30 patients had a history of prior radiotherapy : 22 patients had been irradiated once before , the remaining 8 patients had already undergone two prior irradiations . 
the 38 prior radiotherapies were mostly three - dimensionally planned ( n = 18 ) or even applied using a highly conformal technique of stereotactic radiotherapy or cyberknife ( n = 6 ; accuray , sunnyvale , ca , usa )  . 
tomotherapy was also frequently used ( n = 5 )  . less common was prior radiotherapy with cobalt ( n = 2 ) , brachytherapy ( n = 1 ) , or single - eld photon therapy ( n = 1 ) ; for 5 patients , no details of prior treatment delivery were available . 
the remaining lesions had either no history of prior pain ( 5 cases ) or insufcient documentation ( 7 cases )  . median survival was 17 months in primary irradiated as well as in reirradiated patients . 
2 depicts kaplanmeier curves for both groups . discussion radical radiotherapy in the vicinity of the spinal cord is often caught between the scylla of potentially devastating side effects and the charybdis of insufcient local tumor control . current constraints are mainly based on quantitative analyses of normal tissue effects in the clinic ( quantec ) data [ 2 , 4 ]  . 
common maximal spinal cord doses used in clinical practice are 50 gy or a more conservative 45 gy , which , albeit very low , are reasonable considering that myelopathy is devastating for patients quality of life . 
in individual patients , especially in a curative or reirradiation setting , higher point doses to the spinal cord may be necessary and justiable if precise treatment application is ensured . 
we report that these constraints are feasible in clinical practice , with only half of the primary irradiated lesions treated with eqd2 > 50 gy exceeding the 50 gy dose to the spinal cord ( 16 of 31 lesions )  . 
1 example of two primary irradiated patients treated at the thoracic ( a ; patient #15 from table 3 ) and the lumbar ( b ; patient #8 from table 3 ) spine with dose distribution on the left and follow - up mri after 20 ( a ) and 12 ( b ) months showing no signs of myelopathy table 2 list of reirradiated patients . 
another limitation is , however , due to the nature of radiomyelitis , particularly to its low incidence , since the patient number is too low to conclude that the risk of myelitis is sufciently low to propagate the general safety of this approach . 
they found that patients with signs of myelopathy had signicantly higher median ( 59.1 gy ) and mean ( 66.3 gy ) maximal eqd2 doses to the spinal cord compared to patients without neurological sequelae 100% initial radiotherapy reirradiation years fig . 
signicant differences regarding dvhs were only observed for high point doses , while there was no difference regarding the doses to larger volumes of the spinal cord . however , treatment in these patients was delivered highly hypofractionated ( 3 patients received only 1 fraction , the others 2 and 3 fractions ) ; therefore , the applicability of the linear - quadratic model is at least controversial [ 19 ]  . furthermore , an estimated alpha / beta value of the spinal cord below 2 gy would lead to much higher biologically effective doses in this setting . 
found no correlation of dvhs and patients developing grade 3 neurological toxicity [ 20 ]  . due to the lack of empirical clinical knowledge , preclinical models have to be applied . 
experiments with highprecision proton beam irradiation in rats could show two important ndings : irradiation of small volumes within the spinal cord is more tolerable than irradiation of the whole spinal cord . 
the authors discussed that this nding is probably not due to lower vascular density within the dorsal and lateral part compared to the ventral part , as the vascularization of the white matter is quite homogeneous [ 22 ]  . 
clinical data on peripheral neurons showed that sensitive nerves have a higher radiosensitivity than motor nerves [ 23 ] ; therefore , the sensory quality could affect radiosensitivity too , maybe even within the diameter of the spinal cord . 
bijl and colleagues made the important 568 strahlenther onkol ( 2017 ) 193 : 561569 preclinical nding that a low volume bath to the spinal cord decreases the resistance to low - volume high - dose irradiation [ 24 , 25 ] ; therefore , it is probably not sufcient to analyze maximal point doses only . it is even more difcult to draw conclusions from data on reirradiation . 
based on the data collected by nieder , reirradiation of the spinal cord can be regarded safe if the total single course does not exceed 98 gy biologically equivalent dose ( bed ) , if the time interval between primary irradiation and reirradiation is not shorter than 6 months , and if the cumulative spinal cord dose does not exceed 135.5 gy bed [ 26 , 27 ]  . 
however , based on angs reirradiation experiments on primates , a much higher recovery of the spinal cord of around 75% could be assumed after 1 year and complete recovery after 3 years [ 29 ]  . compared to other publications , the patients described here have much higher cumulative spinal cord doses . 
however , the maximal recovery rate was estimated by a very conservative approach , with a maximal recovery of 50% , even for very long time intervals and small initial irradiation elds . conclusion although limited by their retrospective nature and low sample size , these ndings indicate that excessive spinal cord doses within a minimal volume , particularly in a reirradiation setting with topographically differing high point doses , may be given to patients in compassionate use after careful evaluation of treatmentand tumor - associated risks . 
ghadjar declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
correlations between clinical factors , including risk factors for cardiac disease , dosimetric factors , and the incidence of pe and spe after radiotherapy were analyzed using cox proportional hazard regression analysis . signicant dosimetric factors with the highest hazard ratios were investigated using zones separated according to their distance from esophagus . results pe developed in 49 patients . 
factors affecting the incidence of spe were the v50 of the pericardium zones within 3 cm and 4 cm of the esophagus . conclusion a wide range of radiation doses to the heart and pericardium were related to the incidence of pe . 
a pericardium v50 ( cid : 2 ) 17% is important to avoid symptomatic pe in esophageal cancer patients treated with concurrent chemoradiotherapy . keywords toxicity body surface area cardiac diseases chemoradiotherapy survival dosimetrische prdiktoren fr einen strahleninduzierten perikarderguss bei speiserhrenkrebs zusammenfassung ziel beurteilung der dosis - volumen - parameter fr perikard und herz zur risikoreduzierung eines strahleninduzierten perikardergusses ( pe ) und eines symptomatischen pe ( spe ) bei mit kombinierter strahlenchemotherapie behandelten speiserhrenkrebspatienten . methoden bei 86 von 303 speiserhrenkrebspatienten wurde mindestens 24 monate nach der strahlenchemotherapie ein kontroll - ct angefertigt . 
die korrelationen zwischen klinischen faktoren , einschlielich risikofaktoren fr herzerkrankungen , dosimetrischen faktoren und der inzidenz eines pe und spe nach strahlentherapie wurden mittels proportionaler cox - regressionsanalyse analysiert . signikante dosimetrische faktoren mit den hchsten hazard ratios wurden unter verwendung des bereichs , der strahlenther onkol ( 2017 ) 193 : 552560 assessed for eligibility ( n = 303 ) analyzed ( n = 86 ) fig . 
1 consort diagram excluded ( n = 217 ) ( cid : 2 ) no ct obtained 2 years after radiotherapy ( n = 214 ) ( cid : 2 ) received intracavitary brachytherapy ( n = 2 ) ( cid : 2 ) pe before ccrt ( n = 1 ) * no patients manifested cardiac - related symptoms before ccrt esophageal cancer is poor , asymptomatic pe is a common late complication in patients with esophageal cancer treated with radiotherapy [ 8 ]  . 
although there have been several reports regarding pe , the following problems remained in evaluating their results : first , the denition of pe in computed tomography ( ct ) was not consistent . 
second , the minimal follow - up periods or the minimal intervals between the radiotherapy and the obtained ct at the time of pe were short , which underestimated the true incidence of pe . 
third , several pe patients developed symptoms . differences in factors affecting the incidence of pe and symptomatic pericardial effusion ( spe ) are not yet clear . finally , of the reported pericardium ( pc ) and heart dosimetric factors , the most important predictor has not yet been clearly established . the aim of this retrospective study is to investigate the dosevolume parameters of the pc and heart with the aim of reducing radiation - induced pe and spe in esophageal cancer patients treated with concurrent chemoradiotherapy ( ccrt )  . 
pe was diagnosed based on ct ndings , and patients who underwent chest ct more than 2 years after radiotherapy were selected . entsprechend dem abstand vom sophagus abgegrenzt wurde , untersucht . ergebnisse einen pe hatten 49 patienten . 
beeinussende faktoren fr die speinzidenz war v50 in den 3 und 4 cm von der speiserhre entfernten perikardbereichen . schlussfolgerung eine breite spanne von an herz und perikard abgegebenen strahlendosen korrelierten mit der peinzidenz . 
ein perikard v50 ( cid : 2 ) 17 % ist wichtig , um einen spe bei speiserhrenkrebspatienten unter strahlenchemotherapie zu vermeiden . schlsselwrter toxizitt krperoberche radiochemotherapie kardiale erkrankungen berleben reported radiation - induced cardiac diseases include pericarditis , coronary artery disease , valvular disease , cardiomyopathy , and conduction abnormalities [ 13 ]  . 
these different clinical manifestations have different latency periods , which range from months to decades [ 47 ]  . methods patients between january 2000 and july 2013 , 303 patients with newly diagnosed esophageal cancer were treated with ccrt without surgery . 
1 , 86 patients were used for the analysis . evaluation of pericardial effusion and symptomatic pericardial effusion an enhanced ct scan with 5 mm slice thickness of the chest was obtained before and after ccrt . 
the presence of pe was dened as a thickness of the pericardial uid > 0.6 cthe time of pe onset was dened as the interval between radiotherapy and the rst presence of pe on ct . pericardial effusion ( pe ) occurs as the earliest radiation - induced cardiac complication . 
the 554 strahlenther onkol ( 2017 ) 193 : 552560 for which the contoured heart served as the inner boundary of the shell extending three - dimensionally outward by 0.5 cm in thickness [ 10 ]  . 
the heart and pc dosevolume histograms ( dvh ) were calculated using pinnacle3 , version 9.2 ( philips medical systems , hanover , ma , usa )  . treatment the clinical target volume ( ctv ) encompassed the primary gross tumor volume ( gtv ) with 4 cm superior and inferior margins and regional lymph nodes . 
the planning tumor volume ( ptv ) was dened as the ctv + 1 canteriorposterior opposed treatment elds were typically used initially to deliver up to 4045 gy to the ptv . 
correlations between clinical factors , including risk factors for cardiac disease , dosimetric factors , and the incidence of pe and spe after radiotherapy , were analyzed [ 12 ]  . 
a the longest distance measured at the pericardial space between 3 cm above the diaphragm and 3 cm below the left pulmonary artery shows the thickness of the pericardial uid ( between the two arrows )  . 
the proposed atlas was used to delineate the whole heart contour [ 9 ] and the surrogate pc , the median clinical follow - up of these 86 patients was 56.5 months ( range : 25125 months )  . 
the other patient with spe later developed paroxysmal atrial tachycardia and required catheter ablation . univariate analysis univariate analysis of the clinical factors possibly affecting the incidence of pe and spe are presented in table 1 . 
no clinical factors , including risk factors for the development of cardiac disease , were associated with the incidence of pe and spe . univariate analysis of the heart and pc dosimetric factors possibly affecting the incidence of pe and spe are shown in table 2 . 
spe symptomatic pericardial effusion , ccrt concurrent chemoradiotherapy , yr year 5 - yr : 32.1% 1 - yr : 11.8% 3 - yr : 17.6% number at risk 17 15 14 12 6 although the incidence of spe was not signicantly correlated with dvh factors for the heart , the p - value for incidence of spe was the lowest ( = 0.05 ) for the heart v50 . multivariate analysis dosimetric factors and body surface area ( bsa ) , the other independent factor with a p - value < 0.1 in univariate analysis , were analyzed in terms of the incidence of pe in multivariate analysis . 
in multivariate analysis , heart v50 , pc v50 , and bsa signicantly affected the incidence of pe ( table 3 )  . different zones for the incidence of pe , the highest hr for the signicant factors among v5v65 was the v50 . 
for the incidence of spe , a signicantly higher incidence of spe was found for the pc v50 , and the p - value was the lowest ( = 0.05 ) for the heart v50 among v5v65 . 
the incidence of spe was inuenced by the v50 of the pc zones within 3 and 4 cm of the esophagus . no heart factors of the v50 zones affected the incidence of spe . discussion a wide range of incidence rates for pe have been reported in esophageal cancer patients [ 10 , 13 , 14 ]  . 
this study dened the criteria of pe by ct . the incidence and median onset times of spe after ccrt in recent reports were 4.39.7% and 1922 months , respectively [ 13 , 14 , 16 , 17 ]  . 
in the current study , bmi results strongly correlated with bsa ( data not shown )  . here , bsa was investigated for correlation with the incidence of pe and spe , as it affects the dose of chemotherapy agents . 
reported that a wide range of dvh cutoff points for the pc were associated with a signicant risk of pe , whereas there were fewer dvh cutoff points for the heart associated with the risk of pe . 
additionally , the dvh parameters given to the pc were highly correlated to those of the heart , making it difcult to distinguish between the importance of the individual parameters and their effects [ 10 ]  . 
except the v50 at the pc > 3 cm away from the esophagus and the pc > 4 cm away from esophagus , all factors were signicantly correlated with pe . 
whether dvhs of the pc are more reliable than those of the heart for determining the risk of pe was difcult to conclude from this study . only the v50 at the pc ( cid : 2 ) 3 cm and ( cid : 2 ) 4 cm away from the esophagus was correlated with spe in the separate zone analysis . 
they suggested that defects in the irradiated heart initially occur more frequently in patients that have received more than 25 gy to the heart excessively for 6 months after radiotherapy , and that they are located preferentially in areas of expected high dose . 
they suggested that irreversible and reversible myocardial perfusion defects may result from dose - dependent damage to the microvascular myocardium or blockage of a coronary artery [ 18 ]  . 
reported a radiation dose - dependent perfusion defect in left breast cancer seen at 6 months with minimal defects at 010 gy , and a 20% decrease in regional perfusion at 4150 gy [ 19 ]  . 
in the current study , the incidence of pe was signicantly affected by both the heart and pc dose at a wide range from v5v55 , which may be related to both microvascular damage to the myocardium and pc . the v30 of the pc was found to be a risk factor for pe [ 10 , 14 ] , whereas higher pc doses were relevant for the incidence of spe . 
revealed a mean pc v45 of 58% to be the optimal threshold , as analyzed by a receiver operator characteristic curve , in which the time to event was not considered [ 13 ]  . 
for patients with esophageal cancer treated with 5 - fu / cisplatinbased combined - modality therapy , the standard radiation dose was concluded to be 50.4 gy [ 23 ]  . 
regardless of these results , a recent advanced radiotherapy technique , which could deliver a dose above 50.4 gy to tumors with decreased doses to critical organs , did not clarify whether a dose above 50.4 gy is unable to improve the treatment outcomes [ 2427 ]  . conclusion in esophageal cancer patients treated with ccrt , it was found that a wide range of radiation doses to the heart and pc were related to the incidence of pe . 
it was also found that a high dose to the pc affected the development of spe with severe cardiac symptoms and that a pc v50 ( cid : 2 ) 17% was an important dosimetric factor . compliance with ethical guidelines conict of interest i . 
however , even more intensive novel treatment strategies should be investigated for patients with unfavorable prognostic factors . keywords uterine cervical neoplasms neoplasm recurrence chemoradiotherapy salvage therapy survival salvage - radiotherapie mit oder ohne gleichzeitige chemotherapie bei beckenrezidiv nach alleiniger hysterektomie im frhen stadium des gebrmutterhalskrebses zusammenfassung zielsetzung untersuchung der behandlungsergebnisse von patientinnen mit beckenrezidiv nach alleiniger hysterektomie bei zervixkarzinom , die eine salvage - radiotherapie ( rt ) mit oder ohne begleitende chemotherapie erhalten hatten . strahlenther onkol ( 2017 ) 193 : 534542 methoden insgesamt 33 patientinnen erhielten eine salvage - rt fr ein auf die beckenhhle begrenztes rezidiv des zervixkarzinoms nach alleiniger hysterektomie . 
die raten fr progressionsfreies 5 - jahres - berleben ( pfs ) , lokale kontrolle ( lc ) , fernmetastasenfreies berleben ( dmfs ) und gesamtberleben ( os ) lagen bei jeweils 62 , 7 % , 79 , 5 % , 72 , 5 % und 60 , 1 % . 
fr patientinnen mit ungnstigen prognostischen faktoren sollten intensiver neuartige behandlungsstrategien untersucht werden . schlsselwrter uterine zervixneoplasien neoplasierezidiv chemotherapie salvage - therapie berleben in early - stage cervical cancer , radiotherapy ( rt ) and surgery lead to oncologically comparable results , with a different toxicity spectrum [ 14 ]  . 
after hysterectomy for early - stage cervical cancer ( international federation of gynecology and obstetrics [ figo ] ia1iia2 ) , approximately 1020% of patients have developed recurrences [ 6 ]  . 
in a recent study , the recurrence rate of selected early - stage cervical cancer patients after hysterectomy alone decreased to a level of < 10% [ 19 ]  . 
among all recurrences , up to 75% of cases were clinically limited to the pelvic cavity [ 13 , 13 , 15 ]  . due to its rarity , there have been no prospective randomized trials for the treatment of locoregionally recurrent cervical cancer , and the mainstay of treatment has not been established . 
instead , salvage rt with or without concurrent chemotherapy is currently recommended on the basis of a low level of evidence in recurrent cervical cancer patients without a previous history of pelvic irradiation [ 6 , 18 ]  . several studies with limited numbers of patients have reported clinical outcomes of salvage rt with or without concurrent chemotherapy for recurrent cervical cancer [ 7 , 912 , 16 , 17 , 21 , 23 , 24 ]  . 
however , the majority of these studies were conducted before the early 2000s and therefore did not reect recent advances in the diagnosis , treatment techniques , and the assessment of treatment response [ 7 , 912 , 17 , 21 , 23 , 24 ]  . 
furthermore , in several studies , a broader patient population was included , as some patients received postoperative rt after an initial hysterectomy and some had recurrent disease in the para - aortic lymph node area [ 16 , 17 , 23 , 24 ]  . 
the purpose of this study was to investigate the treatment outcomes of salvage rt or concurrent chemoradiotherapy ( ccrt ) in patients with pelvic recurrence after hysterectomy alone for uterine cervical cancer . methods patients the institutional review board of ajou university school of medicine approved this study and waived informed consent . 
the gross tumor volume was boosted with a median dose of 16 gy ( range , 0 to 24 gy )  . because the national health insurance service , which is the only insurance benet provider in our country , only began to approve claims for intensity - modulated rt for recurrent cervical cancer after 2015 , it was not possible to apply this high - precision technique to the patients . seven patients with stump recurrence received vaginal cuff brachytherapy after completion of external beam rt . of these , 6 patients received high - dose - rate brachytherapy with a median total dose of 10 gy in fraction size 45 gy ( range , 5 to 21 gy )  . 
low - dose - rate interstitial brachytherapy was delivered with a total dose of 20 gy in 1 patient . chemotherapy cisplatin - based concurrent chemotherapy was administered to 29 patients . 
the chemotherapeutic regimen was determined according to disease extent , patients age , and performance status : 8 patients with small stump recurrence figo international federation of gynecology and obstetrics , scc - ag squamous cell carcinoma antigen , pet - ct positron emission tomography - computed tomography , rt radiotherapy , ccrt concurrent chemoradiotherapy , 5 - fu 5 - uorouracil aamong patients who received concurrent chemotherapy strahlenther onkol ( 2017 ) 193 : 534542 fig . 
c ct scan 1 year later showing disappearance of the lesion on the pelvic sidewall and d pet - ct scan 1 year later showing the disappearance of the lesion on the pelvic sidewall ( ( cid : 2 ) 4.0 cm ) received weekly cisplatin ( 40 mg / m2 of body surface area administered once a week for up to six cycles ) ; 21 patients received cisplatin ( 70 mg / m2 on day 1 of each cycle ) combined with 5 - uorouracil ( 1 , 000 mg / m2 on days 2 to 5 of each cycle ) repeated every 4 weeks for 4 cycles . 
paclitaxel ( 135 mg / m2 of body surface area on day 1 of each cycle ) combined with cisplatin ( 60 mg / m2 of body surface area on day 2 of each cycle ) was administered to 1 patient with adenosquamous cell carcinoma for 4 cycles . 
all of these patients had microscopic or less than 2 cm - sized stump recurrence . assessment after completion of salvage ccrt or rt , all patients were examined regularly by physical examination and / or radiographic imaging work - ups at 36 month intervals . 
treatment response in patients with clinically visible tumor was determined by radiographic ndings and assessed according to the revised response evaluation criteria in solid tumors ( recist , version 1.1 ) [ 5 ]  . 
toxicities during or after salvage treatments were evaluated based on the common terminology criteria for adverse events , version 4.03. statistics predictive factors for treatment response were identied using the logistic regression model . 
2 kaplanmeier survival curves of a progression - free survival , b local control , c distant metastasis - free survival , and d overall survival value of < 0.10 were entered into multivariate analysis using the cox proportional hazards model . 
other patients were diagnosed by radiographic work - ups and elevated levels of serum scc - ag . results patient characteristics the patient characteristics of the present study are presented in table 1 . 
among 21 patients who received the combination chemotherapy , 4 did not receive further chemotherapy after completion of salvage rt due to intolerability ( n = 3 ) and refusal of treatment ( n = 1 )  . severe acute hematologic toxicities ( grade 3 ) occurred in 4 patients , all of whom received concurrent cisplatin plus 5 - uorouracil . 
in multivariate logistic regression analysis incorporating these factors , pelvic sidewall involvement ( hazard ratio [ hr ] , 16.474 ; 95% condence interval [ ci ] i , 1.460185.895 ; p = 0.023 ) and evaluation with pet - ct ( hr , 0.026 ; 95% ci , 0.0020.4463 ; p = 0.012 ) were signicantly associated with cr achievement . the median follow - up period was 53 months ( range , 7 to 158 months ) for survivors . 
during the follow - up period , 11 patients experienced disease progression : local progression in 3 patients , distant metastasis in 5 patients , and both local and distant progression in 3 patients . 
disease progression did not occur in any patients treated with rt alone . of the patients with disease progression , 8 received palliative chemotherapy and 1 patient received re - irradiation with 24 gy in 6 fractions , using an intensity - modulated technique . 
of these patients , 2 ( 1 patient treated with palliative chemotherapy and 1 patient treated with re - irradiation ) achieved a second cr and survived with no evidence of disease . 540 strahlenther onkol ( 2017 ) 193 : 534542 during the follow - up period , 9 patients died of disease progression and 1 patient died from advanced gastric cancer . 
in the univariate log - rank test , initial stage ( 0figo ib1 vs . figo ib2iia1 ) , pelvic sidewall involvement , recurrent tumor size , and cr status were signicantly associated with all survival outcomes ( table 3 )  . 
young age ( < 40 years ) signicantly reduced lc ( p = 0.012 ) and os ( p = 0.043 ) , although its impact had borderline signicance on pfs and dmfs . 
this nding was supported by results from previous studies reporting higher cr rates , in which survival rates also tended to be increased . in addition to aggressive local salvage treatments , careful patient selection with a comprehensive workup prior to treatment could also affect a higher cr rate . 
the present study demonstrated the impact of pet - ct in the evaluation strahlenther onkol ( 2017 ) 193 : 534542 of patients with recurrent cervical cancer before initiation of salvage treatments . 
therefore , a thorough systemic evaluation with pet - ct at the time of diagnosis with recurrence might be recognized as a prerequisite for identifying suitable patients for successful salvage treatments , and for determining the appropriate radiation eld . in previous studies , the incidence of severe acute hematologic toxicities ( grade 3 ) related to ccrt was 6.162% [ 16 , 17 , 21 , 24 ]  . 
this could be elucidated by the inclusion of patients treated with rt alone or weekly cisplatseveral factors might have been responsible for the low incidence of late gastrointestinal toxicities in the present study ( 3.3% ) compared with previous investigations , including the short follow - up period , the relatively low total radiation dose , and the absence of previous adjuvant treatments . the results of the present study do not suggest that all patients with pelvic recurrence after hysterectomy alone for early - stage cervical cancer should be indicated for salvage ccrt . 
therefore , for nonpalpable microscopic recurrent cervical cancer , rt alone might be sufcient to control recurrent tumors and expect long - term survival . in the present study , initial stage was an important prognostic factor for survival outcomes . 
also reported a similar nding that patients who had undergone simple hysterectomy demonstrated better disease - specic survival than those who had undergone radical hysterectomy [ 12 ]  . considering that patients treated with simple hysterectomy had higher possibility of having very early - stage tumors at initial diagnosis , initial stage might signicantly inuence the outcomes of patients with recurrent cervical cancer . 
since the addition of concurrent chemotherapy appeared to play a limited role in the treatment of recurrent cervical cancer with pelvic sidewall involvement , delivering a high radiation dose with large fraction size instead of vaginal cuff brachytherapy or maintenance chemotherapy could be considered . hypofractionated or stereotactic body rt ( sbrt ) has recently emerged as an alternative to brachytherapy in recurrent cervical cancer located at the pelvic sidewall . 
reported a 3 - year lc of 81% for patients with recurrent gynecologic malignancies , including 17 patients with recurrent cervical cancer , who received whole pelvic irradiation followed by a boost with sbrt [ 8 ]  . 
also reported a high rate of late toxicities ( 30% ) with sbrt for recurrent cervical cancer with large gross tumor volume at the pelvic sidewall [ 20 ]  . 
therefore , safe delivery of a higher radiation dose with a more precise technique and careful selection of indications should be investigated before active utilization of sbrt , in order to minimize severe toxicities . duenas - gonzalez et al . 
therefore , the benecial role of maintenance chemotherapy should be conrmed by further studies . several issues still remain for the treatment of recurrent cervical cancer conned to the pelvic cavity . 
for example , routine use of elective whole - pelvic irradiation is questionable , although most of the previous studies and the present study have adopted whole - pelvic irradiation [ 7 , 9 , 10 , 12 , 17 , 21 , 24 ]  . 
the current guideline advocates tumor - directed rt , which may include external beam rt , to the pelvis and / or brachytherapy , 542 strahlenther onkol ( 2017 ) 193 : 534542 leaving room for clinicians discretion according to circumstances [ 18 ]  . 
as long - term survival could be expected in more patients after aggressive salvage rt or ccrt , late toxicities should be monitored continuously for a long time . the present study has some drawbacks , including its retrospective nature , inherent selection bias , the small number of patients , heterogeneous treatment approaches , and potential recall biases which made it difcult to assess late toxicities . conclusion nevertheless , the present study showed that long - term survival with no evidence of disease could be achieved by aggressive salvage ccrt or rt in a considerable number of patients with recurrent cervical cancer conned to the pelvic cavity , irrespective of the intensied systemic treatment . 
in particular , more intensied local and systemic treatments might be required for patients with certain adverse features , including initial figo stage ib2iia , pelvic sidewall involvement , and noncr status . 
mai 2017 springer - verlag berlin heidelberg 2017 hintergrund und ziel bisherige leitlinien zur therapie des analkarzinoms sahen vor , dass 612 wochen nach beginn der radiochemotherapie ( rct ) die beurteilung des therapieansprechens erfolgen sollte . 
die vorliegende post - hoc - analyse der act - ii - studie untersuchte den optimalen zeitpunkt zur beurteilung des therapieansprechens an einem groen , homogen behandelten patientenkollektiv . das komplette therapieansprechen nach 26 wochen , deniert als abwesenheit von primrtumor oder suspekten lymphknoten bei der krperlichen untersuchung sowie der bildgebung mittels abdomen - / becken - ct . 
die digitale rektale untersuchung zur evaluierung des therapieansprechens erfolgte protokollgem an drei zeitpunkten : 11 , 18 und 26 wochen nach beginn der rct . patienten und methoden im rahmen der act - ii - / phase - iii - studie wurden 940 patienten an 59 zentren mit einem neu diagnostizierten plattenepithelkarzinom des analkanals behandelt . 
die randomisierung erfolgte nach einem 22 - design : zunchst die randomisierung der simultanen chemotherapie auf die arme mitomycin c ( 12 mg / m2 krperoberche an tag 1 ) oder cisplatin ( 60 mg / m2 krperoberche an tag 1 und tag 29 ) , zustzlich zur gabe von 5 - fluoruracil ( 5 - fu ; 1000 mg / m2 krperoberche tag 14 , tag 2932 ) und der simultanen radiotherapie ( 50 , 4 gy in 28 fraktionen )  . 
emmanouil fokas , md dphil emmanouil.fokas@kgu.de 1 klinik fr strahlentherapie und onkologie , goethe universitt frankfurt , theodor - stern - kai 7 , 60590 frankfurt / main , deutschland ergebnisse von allen 940 patienten ergab die erste rektale untersuchung eine klinisch komplette remission bei 492 patienten ( 52 % ) , die zweite bei 665 ( 71 % ) und die dritte bei 730 ( 78 % )  . 
in der patientenkohorte , die zu allen drei zeitpunkten erschienen sind ( n = 691 ) , zeigte sich eine komplette remission bei 441 ( 64 % ) in der ersten , bei 556 ( 80 % ) in der zweiten und bei 590 ( 85 % ) in der dritten untersuchung . 
das 5 - jahres - gesamtberleben betrug bei den patienten mit komplettem tumoransprechen zu den untersuchungen nach 11 , 18 und 26 wochen jeweils 83 % , 84 % und 87 % . 
war keine komplette remission bei den drei untersuchungsterminen eingetreten , reduzierte sich bei ihnen das 5 - jahres - berleben auf 72 % , 59 % , und 46 % . schlussfolgerung der autoren die endgltige beurteilung des therapieansprechen nach rct des analkanalkarzinoms kann erst nach 26 wochen erfolgen . 594 kommentar die der vorliegenden arbeit [ 1 ] zugrundeliegende act - iistudie testete zunchst , ob die gabe von cisplatin statt mitomycin c whrend der 5 - fu - basierten rct sowie in einer konsolidierungschemotherapie die rate an kompletten remissionen verbessern kann . 
im vergleich zu anderen randomisierten studien , welche den beurteilungszeitpunkt auf 4 und 8 wochen nach therapieabschluss festlegten [ 35 ] , erfolgte in der act - iistudie die beurteilung zu mehreren zeitpunkten , was eine longitudinale betrachtung ermglichte . die rate an kompletten remissionen bei der ersten untersuchung war vergleichbar mit den ergebnissen der rtog - 8704 - studie [ 3 ] , in welcher 46 wochen nach abschluss der rct eine routinebiopsie durchgefhrt wurde . bei nichtansprechen erfolgte in dieser studie die zustzliche boost - applikation von 5 1 , 8 gy mit simultaner gabe von cisplatin ( 100 mg / m2 krperoberche ) und 5 - fu . betrachtet man nun die ergebnisse der vorliegenden arbeit , zeigt sich , dass eine verbesserung der ansprechrate vermutlich auch durch lngeres abwarten htte erreicht werden knnen . 
die analyse der act - ii - studie liefert demnach wichtige argumente fr ein abwartendes verhalten im rahmen der remissionsbeurteilung nach rct . ein vollstndiges therapieansprechen 26 wochen nach behandlungsbeginn zeigte sich zustzlich als ein starker prdiktor fr das gesamtberleben . 
die autoren schlagen daher vor , dass eine untersuchung zu diesem zeitpunkt in zuknftigen randomisierten studien als frher surrogatparameter fr sptere onkologische endpunkte verwendung nden sollte . offen bleibt allerdings , wie sich diese verzgerte tumorregression auf rct biologisch erklren lsst . 
die klassischen fnf r der radiobiologie ( repopulierung , reoxygenierung , reparatur , redistribution und radiosensitivitt ; [ 6 ] ) , welche klassischerweise zur erklrung der akuten strahlenwirkung verwendet werden , sind nur bedingt in der lage , ein um monate nach therapieende verzgertes ansprechen plausibel zu machen . 
es besteht also ein bedarf an weiterfhrenden molekularen untersuchungen zur strahlenbiologie des analkarzinoms sicher auch in richtung des immunologischen tumormikromilieus [ 7 ]  . strahlenther onkol ( 2017 ) 193 : 593594 fazit patienten mit analkarzinomen sollten nach abgeschlossener radiochemotherapie engmaschig nachgesorgt werden , um das therapieansprechen zuverlssig erkennen und auch die prognose beurteilen zu knnen . 
das kann viele patienten vor einer unntigen abdominoperinealen rektumexstirpation als salvagetherapie mit ihren negativen auswirkungen auf die lebensqualitt bewahren . daniel martin , claus rdel und emmanouil fokas , frankfurt / main interessenkonikt d . 
flam m , john m , pajak tf et al ( 1996 ) role of mitomycin in combination with uorouracil and radiotherapy , and of salvage chemoradiation in the denitive nonsurgical treatment of epidermoid carcinoma of the anal canal : results of a phase iii randomized intergroup study . 
ukcccr anal cancer trial working party et al ( 1996 ) epidermoid anal cancer : results from the ukcccr randomised trial of radiotherapy alone versus radiotherapy , 5 - uorouracil , and mitomycin . lancet 348 : 10491054 5 . 
bartelink h , roelofsen f , eschwege f et al ( 1997 ) concomitant radiotherapy and chemotherapy is superior to radiotherapy alone in the treatment of locally advanced anal cancer : results of a phase iii randomized trial of the european organization for research and treatment of cancer radiotherapy and gastrointestinal cooperative groups . 
balermpas p , martin d , wieland u et al ( 2017 ) human papilloma virus load and pd - 1 / pd - l1 , cd8 and foxp3 in anal cancer patients treated with chemoradiotherapy : rationale for immunotherapy . 
prone position julia koeck1 sylvia bttner4 jens fleckenstein1 frederik wenz1 katharina kromer1 frank lohr2 tobias baack3 kerstin siebenlist1 sabine mai1 received : 25 october 2016 / accepted : 27 january 2017 / published online : 20 february 2017 springer - verlag berlin heidelberg 2017 abstract background this treatment planning study analyzes dose coverage and dose to organs at risk ( oar ) in intensitymodulated radiotherapy ( imrt ) of rectal cancer and compares prone vs . 
supine positioning as well as the effect of dose optimization for the small bowel ( sb ) by additional dose constraints in the inverse planning process . patients and methods based on the ct datasets of ten male patients in both prone and supine position , a total of four different imrt plans were created for each patient . 
in half of the plans , two additional sb cost functions were used in the inverse planning process . results there was a statistically signicant dose reduction for the sb in prone position of up to 41% in the high and intermediate dose region , compared with the supine position . furthermore , the femoral heads showed a signicant dose reduction in prone position in the low dose region . 
ospedaliero - universitaria di modena , modena , italy 3 department of internal medicine , grn clinic weinheim , weinheim , germany 4 department of biomathematics and medical statistics , university medical center mannheim , university of heidelberg , mannheim , germany 14% with the additional cost functions . 
there were no signicant differences in the dose distribution of the planning target volume ( ptv ) and the bladder . conclusion prone positioning can signicantly reduce dose to the sb in imrt for rectal cancer and therefore should not only be used in 3d conformal radiotherapy but also in imrt of rectal cancer . 
further protection of the sb can be achieved by additional dose constraints in inverse planning without jeopardizing the homogeneity of the ptv . keywords rectal cancer intensity - modulated therapy prone position small intestine inverse planning dnndarmschonung bei der imrt des rektumkarzinoms dosimetrische studie zur bauchund rckenlagerung zusammenfassung hintergrund diese planungsstudie analysiert die dosisverteilung im zielvolumen und in den risikoorganen ( organs at risk , oar ) bei der intensittsmodulierten strahlentherapie ( intensity - modulated radiotherapy , imrt ) des rektumkarzinoms und vergleicht hierbei bauchund rckenlagerung sowie die effekte der dosisoptimierung fr den dnndarm ( dd ) durch zustzliche dosiseinschrnkungen bei der inversen planung . material und methode anhand der computertomographien ( ct ) zur bestrahlungsplanung von 10 mnnlichen patienten in bauchund in rckenlage wurden fr jeden einzelnen patienten jeweils 4 verschiedene imrt - plne erstellt . 
als oar wurden dd , blase sowie die femurkpfe deniert . in der hlfte der flle wurden in der inversen planung 2 zustzliche optimierungsbedingungen fr den dd verwendet . strahlenther onkol ( 2017 ) 193 : 578588 ergebnisse in bauchlagerung zeigte sich fr den dd eine statistisch signikante dosisreduktion bis zu 41 % im mittleren und hohen dosisbereich , verglichen mit der rckenlagerung . 
die dosisverteilung im planungszielvolumen ( ptv , planning target volume ) und in der blase wies keine signikanten unterschiede auf . schlussfolgerung die bauchlagerung ermglicht eine signikante dosisreduktion im dd bei der imrt des rektumkarzinoms und sollte daher nicht nur bei der 3d - konformalen strahlentherapie , sondern auch bei der imrt des rektumkarzinoms eingesetzt werden . 
eine weitere reduktion der dnndarmbelastung kann , ohne gefhrdung der homogenitt im ptv , durch zustzliche dosiseinschrnkungen bei der inversen planung erreicht werden . schlsselwrter rektumkarzinom intensittsmodulierte strahlentherapie bauchlagerung dnndarm inverse planung introduction colorectal cancer is the third most common diagnosis of all cancers , with rectal cancer accounting for approximately one third of all colorectal cancers [ 1 ]  . 
although over 80% of patients with rectal cancer are treated with a curative approach ( at present mostly by total mesorectal excision ) , up to 10% present with local recurrences if only total mesorectal excision is performed [ 26 ]  . 
neoadjuvant chemoradiation efciently can reduce local recurrences by up to 30% [ 79 ] ( relative reduction ) , overall resulting in local recurrence rates of 58% [ 10 ] and is the treatment of choice for patients with primary resectable rectal cancer in uicc ( union international contre le cancer ) stage ii / iii [ 1 , 2 , 1113 ]  . 
during radiation therapy , often the most relevant organ at risk ( oar ) is the small bowel ( sb ) owing to its position near the rectum and its high radiation sensitivity [ 14 ]  . 
radiation injury to the sb frequently causes acute and / or late gastrointestinal toxicity such as diarrhea , fecal incontinence , and late small bowel obstruction [ 6 , 15 , 16 ]  . three dimensional conformal radiotherapy ( 3d - crt ) has long been the standard radiation technique for neoadjuvant radiation treatment of rectal cancer . 
prone positioning with a belly board for bowel displacement has been used mostly as standard patient positioning to reduce the volume of sb in the high dose region , although some centers prefer the supine position owing to difculties in reproducibility of the prone position with a belly board [ 17 ]  . intensity - modulated radiotherapy ( imrt ) has become a clinically established radiation technique for rectal cancer in the past few years , providing better high dose conformality and homogeneity through the different choice and weight of cost functions and dose constraints for oar and planning target volume ( ptv ) in the inverse planning process . 
as acute sb toxicities are a limiting factor and the application of the full treatment dose is essential with respect to local control or survival , the reduction of dose to the sb is crucial for decreasing breaks in treatment and assuring compliance [ 24 , 25 ]  . in this study , we investigate the differences in oar dose distribution and ptv conformality and homogeneity in the prone versus supine position using a full - bladder protocol during imrt for rectal cancer , to assess whether prone treatment is still desirable even when imrt is used . 
we also investigate the differences in dose distribution to oar and ptv when using additional active sb dose constraints and cost functions in the inverse planning process . patients and methods patients treatment planning computed tomography ( ct ) datasets with a slice thickness of 5 mm in the prone and supine position of 10 male patients with prostate cancer in 2012 and 2013 were utilized . 
a belly board was used for prone positioning and a full - bladder protocol was used for both positions . target denition and oar delineation oncentra masterplan version 4.3 sp3 ( elekta ab , stockholm , sweden ) was used for the delineation of the ptv and oar . 
1 planning computed tomography of an exemplary patient in prone position with contoured planning target volume ( red ) , bladder ( yellow ) , small bowel ( brown ) , and femoral heads ( rose ) in a sagittal plane ( a ) and in three - dimensional view ( b ) fig . 
with active constraints for the small bowel stands for additional dose constraints in the inverse planning process in regard to the small bowel plan calculation calculation of the radiation dose to the treatment eld was performed using monaco 3.2 ( elekta ab , stockholm , sweden )  . 
in all plans , dose conformity and homogeneity were achieved by three cost functions concerning the ptv ( target equivalent uniform dose , quadratic overdose , quadratic underdose ) and by two cost functions concerning the whole patient contour ( quadratic overdose , conformality )  . 
for the plans with active constraints for the sb , two further cost functions regarding the sb were used ( serial and maximum dose , with 33 gy and 48 gy as isoconstraints , respectively )  . 
in cases of subsequent dose inhomogeneity in the ptv , the weight of the isocontraints of quadratic overdose and / or quadratic underdose were consecutively decreased or increased . plan evaluation dosevolume histograms ( dvhs ) were created and statistically analyzed for all plans . 
analyzed parameters for the ptv were volume , dmean , dmedian , dmin , dmax , v95% , v104% , and the homogeneity index ( with hi = d99% / d1% )  . 
regarding the sb , the prone position was able to signicantly reduce radiation dose to the sb ( both in the plans with and without active sb dose constraints ) : the parameters dmean , dmedian and intermediate to high doses ( v15 gy to v45 gy at intervals of 5 gy ) were signicantly lower in the prone position , up to 14% for dmean and up to 41% in the high dose region . 
as values for left and right femoral heads were quite similar , exemplarily only the right femoral head is shown bstatistical evaluation was not possible 582 strahlenther onkol ( 2017 ) 193 : 578588 fig . 
3 averaged dosevolume histograms for ptv , small bowel , bladder , and right femoral head in prone ( red ) and supine ( black ) position for all 10 patients ( plans without active sb constraints )  . 
3 shows the averaged dvhs for the ptv , sb , bladder , and right femoral head in the prone and supine position for all 10 patients ( exemplary for the plans without active sb constraints )  . 
in summary , the prone position signicantly reduced dose for the sb in the intermediate and high dose region and for the femoral heads in the low dose region , whereas dose distribution in the bladder and ptv was unaffected by positioning . inverse planning with active sb constraints vs . 
4 shows the absolute reduction of irradiated sb volume ( % ) for the plans with active sb constraints compared with the plans without active sb constraints , exemplarily in the prone position . 
4 comparison of the plans in prone position concerning the small bowel : absolute reduction of irradiated small bowel ( sb ) volume in % for the plans with active sb constraints compared with the plans without active sb constraints . 
negative values below the x - axis stand for less irradiated volume in the plans with active sb constraints ( compared with the plans without active sb constraints ) in % and accordingly better sb protection : plan 1 prone position plan with active sb constraints , plan 2 prone position plan without active sb constraints . gy gray tive dose constraints was achieved approximately from 16 up to 44 gy . 
dose reduction for the sb , furthermore , was possible without increasing dose to other oar and without impairing homogeneity in the ptv . prone position without active sb constraints vs . 
supine position with active sb constraints table 3 compares the mean dosimetric parameters of the prone position without active sb constraints to the supine position with active sb constraints , in order to analyze the extent of dose optimization by patient positioning in comparison with optimized inverse treatment planning by chosen dose constraints . 
regarding the sb , dmean was signicantly lower by 14% in the plans in prone position without active sb constraints , compared with the plans in supine position with active dose constraints , and accordingly the volume of sb exposed to dose was lower for v10 gy up to v45 gy . 
for the femoral heads , dmean , dmedian , and the low dose region ( v10 gy and v15 gy ) were signicantly lower in the prone position without the additional active sb constraints . 
in summary , the usage of prone ( instead of supine ) position was able to optimize dose to the sb to a far greater extent than the usage of selected dose constraints ( compared with not using them )  . discussion acute grade 34 diarrhea is a common cause of morbidity in patients with rectal cancer and occurs in 1639% of patients undergoing preoperative chemoradiation therapy [ 30 , 31 ]  . severe diarrhea plays an important role in treatment interruptions and premature termination of the radiation course and therefore may reduce the effectiveness of therapy in some patients [ 5 , 32 ]  . 
as the development of grade 3 / 4 small bowel toxicity responds to a strong dosevolume relationship , reduction of the sb dose is crucial in order to minimize treatment - related bowel complications [ 24 , 25 ]  . bowel protection may be of even greater importance in accelerated radiochemotherapy regimens [ 13 ]  . 3d - crt has been the therapy standard , and improving patient positioning to achieve sb dose reduction was the subject of discussion in research . 
despite all the advantages of the prone position , it often shows more setup errors than supine position and therefore requires close positioning surveillance [ 37 , 38 ]  . 
showed that gender and age have no effect on the irradiated volume of the sb ; however , the position of the belly board signicantly inuences the irradiated volume of the sb [ 42 ]  . 
as choice and weight of dose constraints can immensely inuence the dose distribution in the ptv and all other oar , however , it is essential to ensure ptv coverage and homogeneity in order to maintain treatment outcome [ 19 , 22 ]  . this planning study proved the benets of prone position in regard to the sb doses even when imrt is used . a signicant dose reduction to the sb for mean and median dose was observed compared with the supine position , which is in agreement with the current literature . 
interestingly , positioning in prone or supine position for imrt had no signicant effect on dose reduction to the bladder . evaluating the contribution of optimized inverse planning to reduce doses to the sb was another important component of this study . 
an emphasis was placed on protecting the sb in the high dose region , assuming that this should reduce acute and late gastrointestinal toxicity [ 14 , 21 , 43 ]  . while prone position already has been proven as a standard treatment position , in this study we additionally applied various dose constraints to the sb during the planning process in half of the plans ( for prone as well as for supine position )  . 
in these plans , we used not diverse or random but similar sb constraints , allowing meaningful statistical comparison , even though it meant narrowing the mean extent of the difference between the plans with and without active sb constraints . 
as the statistical comparison already showed signicant differences for the sb without alteration in ptv homogeneity in our chosen approach of applying predened sb dose constraints , it can be assumed that further benets by applying stronger constraints are possible and sometimes reasonable . overall , our ndings show that in particular the dose distribution of the sb not only benets from the prone position with a belly board and full - bladder protocol while treating with imrt plans , but it also prots by additional active sb constraints during the inverse planning process . the reduction to the sb in this study was most pronounced in the intermediate and high dose region , which is an effective way to reduce sb toxicities according to current studies [ 21 , 22 , 43 ]  . 
however , the relative importance of different dose levels regarding the sb is not yet claried completely ( a lot to a little or a little to a lot ? )  . 
the relative contribution of volumes exposed to high versus low doses to overall toxicity should be evaluated to further optimize dose prescription . conclusion prone positioning using a belly board can signicantly reduce dose to the sb in imrt for rectal cancer and therefore should be used not only in 3d - crt but also in imrt of rectal cancer . 
further protection of the sb can be achieved by a few extra dose constraints in inverse planning without jeopardizing the homogeneity of the ptv . acknowledgements the authors thank negin sedaghat ( westmead and nepean hospitals , university of sydney , teaching hospitals , australia ) for revising the manuscript . compliance with ethical guidelines conict of interest j . 
lohr has travel grants , research support , and teaching honoraria from elekta ab ( stockholm , sweden ) and iba ( schwarzenbruck , germany ) as well as board membership from c - rad ( uppsala , sweden ) to declare . 
zimmermann1 gabriele beckmann1 pius jung2 michael flentje1 received : 27 november 2016 / accepted : 29 march 2017 / published online : 25 april 2017 springer - verlag berlin heidelberg 2017 abstract herein , the authors describe the case of a 31year - old female patient with primary metastatic adenocarcinoma of the lung referred for radiation therapy of newly diagnosed intramedullary spinal cord metastasis at c4 / 5 and an adjacent osteolytic lesion . 
a review of the literature failed to identify any reference to increased mucositis after radiation therapy concurrent with crizotinib , although references to such an effect with other tyrosine kinase inhibitors ( tki ) were found . 
11 , 97080 wrzburg , germany 2 department of pneumonology , medical clinic i , university hospital of wrzburg , oberdrrbacherstrae 6 , 97080 wrzburg , germany keywords non - small cell lung cancer chemotherapy tyrosine kinase mucositis dysphagia ulzeration des hypopharynx und des oberen sophagus nach bestrahlung der halswirbelsule und simultaner crizotinib - therapie zusammenfassung die autoren berichten ber eine 31jhrige patientin mit primr metastasiertem adenokarzinom der lunge , die ihnen zur bestrahlung einer neu aufgetretenen intraspinal - intramedullren metastase auf hhe der bandscheibe c 4 / 5 sowie einer benachbarten osteolytischen lsion zugewiesen wurde . 
eine literaturrecherche ergab keine hinweise fr ein verstrktes auftreten von mukositis nach bestrahlung und simultaner crizotinib - therapie , jedoch fanden sich referenzen zu diesem effekt mit anderen thyrosinkinaseinhibitoren ( tki )  . dennoch vermuten die autoren ein beachtliches risiko fr unvorhergesehene wechselwirkungen . 
im falle einer radiotherapie und zeitgleicher einnahme von crizotinib er590 strahlenther onkol ( 2017 ) 193 : 589592 scheint eine erhhte aufmerksamkeit hinsichtlich verstrkter reaktionen berechtigt zu sein . table 1 localization of former radiotherapeutic treatment of bone metastases schlsselwrter nicht - kleinzelliges bronchialkarzinom chemotherapie tyrosinkinase mukositis dysphagie in recent years , targeted agents have evolved as an alternative to conventional chemotherapy in selected cancers . 
crizotinib is an oral small molecule tyrosine kinase inhibitor ( tki ) of alk , met , and ros1 kinases , and is used in rstand second - line therapy of advanced alk - positive nsclc [ 3 , 4 ]  . 
herein , the authors report on a patient with exacerbated mucositis after irradiation of the cervical spine parallel to crizotinib treatment . case a 31 - year - old female was referred to radiation therapy for newly diagnosed intramedullary spinal cord metastasis at c4 / 5 . 
whole - brain radiation therapy ( wbrt ; to 37.5 gy in 15 fractions ) was performed in december 2014 without complications . in september 2015 , the patient was readmitted for headache and trigeminal dysesthesia . 
diagnostic mri localization left foot thoracic and lumbar spine from t10 to right proximal tibia right distal tibia dose 10 3 gy 10 3 gy 10 3 gy 10 3 gy showed an intramedullary cord metastasis at c4 / 5 and an adjacent osteolytic lesion in vertebral body c4 . 
1 dose distribution of the cervical spine levels c3 to c5 ( single dose 3 gy , cumulative dose 30 gy ) strahlenther onkol ( 2017 ) 193 : 589592 fig . 
left side : overview of the upper esophagus in esophagoscopy . right side : close up view on the ulcerated brinous lesion large - volume radiotherapy of head and neck tumors with doses > 50 gy and concomitant chemotherapy [ 6 ]  . 
the early onset , severity , and duration of mucositis sharply limited to the irradiated segment seem unusual in this case . unexpected side effects of combining radiotherapy and biological agents ( particularly tki ) have been described . two independent phase ii clinical trials to asses efcacy and safety of chemoradiation and bevacizumab in lung cancer were closed early due to tracheoesophageal stula [ 7 ]  . severe bowel toxicity has been found in patients receiving bevacizumab or sorafenib before or after sbrt [ 8 ]  . a similar case to this one was reported by merten et al . a patient receiving radiation therapy for bone metastases of melanoma at spine level t4 to t7 with concurrent vemurafenib developed grade 3 esophagitis [ 9 ]  . 
crizotinib is well tolerated as a single agent in metastatic nsclc and signicantly improves quality of life and duration of remission compared to chemotherapy in patients with alk / ros mutations [ 3 , 10 ]  . 
mucositis is not explicitly described [ 11 ]  . crizotinib has been found to be a radiation sensitizer in eml4alk - expressing nsclc cell lines [ 12 , 13 ]  . 
however , in a mature analysis of patients with alk - positive nsclc receiving stereotactic body or hypofractionated radiation therapy with concurrent crizotinib , no acute or late toxicities greater than grade 2 were observed , particularly no mucositis . 
continuing crizotinib after local ablative radiotherapy was feasible [ 14 ]  . in the current case , application was simultaneous , previous radiation treatment due to bone lesions without crizotinib had been uneventful , and wbrt parallel to crizotinib had also been well tolerated . 
die properative radiotherapie fhrt zur einer signikanten reduktion der lokalrezidivrate beim rektumkarzinodie optimale fraktionierung und das beste zeitintervall zwischen radiotherapie und chirurgie sind bisher jedoch noch unklar und werden kontrovers diskutiert . 
die patienten erhielten entweder eine neoadjuvante radiotherapie mit 5 5 gy gefolgt von der operation innerhalb einer woche ( arm a ) , eine neoadjuvante radiotherapie mit 5 5 gy und die operation nach 48 wochen ( arm b ) oder eine neoadjuvante radiotherapie mit einer einzeldosis von 2 gy bis zu einer gesamtdosis von 50 gy und eine operation nach 48 wochen ( arm c )  . 
die postoperativen komplikationen waren nach 5 5 gy und lngerem intervall bis zur operation niedriger als nach sofortiger operation . die langzeitergebnisse zum primren endpunkt ( lokalrezidive ) zeigten keine unterschiede . 
die kurzzeitradiotherapie mit 5 5 gy und operation 48 wochen spter kann als alternative zur sofortigen operation nach einer woche oder der konventionell fraktionierten radiotherapie gesehen werden . originalpublikation erlandsson j , holm t , pettersson d , et al ( 2017 ) optimal fractionation of preoperative radiotherapy and timing to surgery for rectal cancer ( stockholm iii ) : a multicentre , randomised , non - blinded , phase 3 , non - inferiority trial . 
als gesamtbehandlungszeit wurde daher ein intervall von maximal 10 tagen zwischen beginn der radiotherapie und der operation empfohlen . in der hier kommentierten , randomisierten stockholmiii - studie erfolgte die operation nun entweder unmittelbar nach applikation von 5 5 gy oder erst nach 48 wochen . ein dritter arm mit alleiniger , konventionell fraktionierter radiotherapie ( ohne simultaner chemotherapie ) wurde nach einem protokoll - amendment nur noch von wenigen zentren bedient . 
in einer ersten interimsanalyse hatte sich gezeigt , dass die rate an ypt0 - tumoren im arm mit 5 5 gy nach sofortiger operation bei 2 , 1 % und nach einem lngeren intervall bei 11 , 8 % lag ( p = 0 , 001 ; [ 4 ] )  . 
auch in dieser studie zeigte sich ein signikant verbessertes tumor - downstaging nach verlngertem intervall ( 45 wochen nach 5 5 gy ) bei ebenfalls identischer r0 - resektionsrate , rate an schliemuskelerhaltenden operationen und nicht signikant unterschiedlichem gesamtberleben [ 5 ]  . 
eine polnische phase - iii - studie verglich die konventionell fraktionierte 5 - fluorouracil - basierte radiochemotherapie ( teilweise unter inklusion von oxaliplatin ) mit einer kurzzeitradiotherapie , gefolgt von 3 zyklen einer neoadjuvanten chemotherapie mit folfox - 4 und operation in woche 12 bei patienten mit klinisch xierten t3oder t4 - tumoren [ 6 ]  . 
eine weitere randomisierte phaseiii - studie ( rapido ) testete bei mittels magnetresonanz ( mrt ) denierten hochrisikopatienten ( t4 , mrcrm + , n2 , emvi + ) die kurzzeitradiotherapie mit 5 5 gy , gefolgt von 6 zyklen capox und operation in woche 2224 gegen eine konventionelle radiochemotherapie mit capecitabin und operation in woche 1416 . 
die rekrutierung dieser studie ist abgeschlossen , ergebnisse liegen allerdings noch nicht vor [ 7 ]  . fazit ein verlngertes intervall von 48 wochen zwischen kurzzeitradiotherapie und operation kann insbesondere bei patienten mit gewnschtem , weil notwendigem downsizing , die sich nicht fr eine radiochemotherapie eignen oder diese ablehnen , als alternative zur konventionell fraktionierten radiochemotherapie angeboten werden . 
zur addition einer neoadjuvanten chemotherapie nach 5 5 gy und verlngertem intervall bis zur operation wird insbesondere die rapido - studie wichtige weitere erkenntnisse liefern . emmanouil fokas und claus rdel , frankfurt interessenkonikt e . 
van gijn w , marijnen ca , nagtegaal id et al ( 2011 ) preoperative radiotherapy combined with total mesorectal excision for resectable rectal cancer : 12 - year follow - up of the multicentre , randomised controlled tme trial . 
sebag - monteore d , stephens rj , steele r et al ( 2009 ) preoperative radiotherapy versus selective postoperative chemoradiotherapy in patients with rectal cancer ( mrc cr07 and ncic - ctg c016 ) : a multicentre , randomised trial . 
van den broek cb , vermeer ta , bastiaannet e et al ( 2013 ) impact of the interval between short - course radiotherapy and surgery on outcomes of rectal cancer patients . 
pach r , kulig j , richter p et al ( 2012 ) randomized clinical trial on preoperative radiotherapy 25 gy in rectal cancer - treatment results at 5 - year follow - up . 
bujko k , wyrwicz l , rutkowski a et al ( 2016 ) long - course oxaliplatin - based preoperative chemoradiation versus 5 5 gy and consolidation chemotherapy for ct4 or xed ct3 rectal cancer : results of a randomized phase iii study . 
nilsson pj , van etten b , hospers ga , phlman l et al ( 2013 ) shortcourse radiotherapy followed by neo - adjuvant chemotherapy in locally advanced rectal cancer the rapido trial . 
androgen deprivation therapy was started in 1 patient without proven recurrence . univariable risk factors for local recurrence were : at least 50% positive biopsies , intermediate risk , treatment with neoadjuvant hormone therapy , low preimplantation volume receiving 100% of the prescribed dose , and no bounce development . 
hormone - nave patients not attaining a psa value < 0.5 ng / ml during follow - up also had a higher risk ( cid : 2 ) isabelle kindts , md isabellekindts@hotmail.com 1 department of radiation oncology , az groeninge hospital , president kennedylaan 4 , 8500 kortrijk , belgium 2 department of urology , az groeninge hospital , kortrijk , belgium 3 biostatistics , faculty of medicine , catholic university leuven kulak , kortrijk , belgium of local recurrences . 
als psa - wiederanstieg war eine nadir - erhhung 0 , 2 ng / ml , gefolgt von spontaner rckgang deniert . verhltnisse wurden mit dem exakten fisher - test und kontinuierliche variablen mit dem ungepaarten t - test oder einer nichtparametrischen methode verglichen . 
mit multivariater 708 strahlenther onkol ( 2017 ) 193 : 707713 cox - regressionsanalyse wurde der einuss von kofaktoren untersucht . ergebnisse das mediane follow - up betrug 66 monate . das lokalrezidivfreie 5 - jahres - berleben betrug 96 , 1 % . ein histologisch nachgewiesenes lokalrezidiv entwickelten 13 patienten ; ein rezidiv nach phoenix hatten bei der letzten untersuchung 4 patienten . 
univariate risikofaktoren fr ein lokalrezidiv waren : mindestens 50 % positive biopsien , intermedires risiko , behandlung mit neoadjuvanter hormontherapie , geringe prostatavolumenabdeckung mit 100 % der vorgeschriebenen dosis und kein psa - wiederanstieg . 
die cox - regression ergab , dass mindestens 50 % positive biopsien und kein psa - wiederanstieg die lokale kontrolle signikant beeinussen ( hazard ratio [ hr ] je 1 , 02 und 11 , 59 )  . 
jngere patienten und jene , die mit einer geringeren aktivitt pro volumen behandelt wurden , hatten ein hheres risiko fr einen wiederanstieg ( je hr 0 , 99 und 0 , 04 )  . schlussfolgerung ldr - bt ist eine effektive kurative behandlungsmethode fr junge mnner mit low - risk - prostatakarzinom und ist auch bei intermedirem risiko zu erwgen . schlsselwrter risikofaktoren prostataspezisches antigen strahlentherapie brachytherapie patients with low - risk clinically localized prostate adenocarcinoma are confronted with multiple curative treatment modalities such as prostatectomy , brachytherapy ( bt ) , and external beam radiotherapy , besides active surveillance or watchful waiting [ 1 ]  . 
conducted a systematic literature review of biochemical outcomes and suggest that low - dose - rate ( ldr ) bt may be more effective than surgery in terms of biochemical endpoints for low - risk disease [ 2 ]  . 
the most obvious reason , however , is the referral pattern before treatment , since many physicians believe that younger patients are better suited for surgery as a primary treatment [ 8 , 9 ]  . table 1 patient and tumor characteristics patient group ( n = 192 ) variable percentage of positive biopsies total gleason score ipsa ( ng / ml ) age ( years ) risk [ 11 ] neoadjuvant hormone therapy perineural invasion < 50% 50% unknown ( cid : 2 ) 6 unknown ( cid : 2 ) 10 > 10 ( cid : 2 ) 20 50 < 55 55 < 60 60 ( cid : 2 ) 65 intermediate for risk reduction for downsizing for unknown reason unknown 124 ( 64.6% ) 28 ( 14.6% ) 40 ( 20.8% ) 146 ( 76.0% ) 45 ( 23.4% ) 1 ( 0.5% ) 165 ( 85.9% ) 27 ( 14.1% ) 2 ( 1.0% ) 29 ( 15.1% ) 51 ( 26.6% ) 110 ( 57.3% ) 128 ( 66.7% ) 64 ( 33.3% ) 13 ( 6.8% ) 14 ( 7.3% ) 5 ( 2.6% ) 160 ( 83.3% ) 18 ( 14.2% ) 76 ( 39.6% ) 98 ( 51.0% ) ipsa initial prostate - specic antigen since the prostate gland is not resected in radiotherapy , interpretation of the results of biochemical follow - up is less straightforward than after radical prostatectomy . 
a prostatespecic antigen ( psa ) bounce is dened as a temporary increase of benign origin after bt , which has been described to occur more frequently in younger patients [ 10 ]  . 
knowledge about this phenomenon is important to help distinguish between a true recurrence and a simple psa bounce . to provide long - term rates of local failure and psa behavior in younger patients , we analyzed a unique population of patients aged 65 years or younger at the time of bt , who were treated between 13 and 7 years ago at a single center . patients and methods between january 1 , 2003 and december 31 , 2009 , a total of 192 patients were denitively treated with ldr 125i - bt with or without hormone therapy for biopsy - proven adenocarcinoma of the prostate . 
the dose delivered to the prostate was determined from dosevolume histogram analysis and dened as the dose delivered to 90% of the prostate volume ( d90 ; table 2 )  . local failure was dened as any psa rise leading to salvage treatment or biochemical failure according to the american society for radiation oncology consensus phoenix denition ( psa nadir plus 2 ng / ml ) at the last consultation [ 12 ]  . in this way , patients with a psa increase fullling both the phoenix criteria and also the bounce denition ( spontaneous psa decrease ) were excluded from the local failure group . 
as suggested by many authors , a psa bounce was dened as a rise of the nadir by at least 0.2 ng / ml followed by spontaneous return to the nadir or lower [ 13 ]  . 
in case of patients with a bounce and a local failure , data were used in both analyses . statistics descriptive statistics was presented as mean ( plus standard deviation ) or median ( plus interquartile range ) depending on the normality of the data ( based on visual inspection of the histogram )  . 
1 local recurrence - free survival after a median follow - up of 66 months ( interquartile range 4884 months ) patient and tumor characteristics patient ( n = 192 ) and tumor characteristics are shown in table 1 . 
a second bounce developed in 4 patients . a signicantly higher chance of developing a bounce was observed in patients who were younger or had a lower mean treatment activity per volume , and also in patients with < 50% positive biopsies or those who had achieved a psa value < 0.5 ng / ml during the rst 18 months of follow - up regardless of hormone therapy ( table 4 )  . 
 [ 26 ] discussion the main goal of our study was to report the local failure rate in a population of 192 younger patients with lowand intermediate - risk prostate carcinoma treated with brachytherapy . 
we dened 18 patients as having a local recurrence : 13 patients developed a biopsy - proven local recurrence and 4 other patients had a recurrence according to the phoenix denition at the last consultation . 
in multivariable analysis , patients with at least 50% positive prostate biopsies at diagnosis and those who did not develop a bounce were at a signicantly higher risk for a local recurrence . the local recurrence rate at 5 years in this study is comparable to available data on young prostate cancer patients treated with bt around the same time period ( table 5 )  . 
regardless of age , our outcome is consistent with the 10 - year biochemical disease - free survival rates ranging between 88 and 98% as reported by grimm et al . 
in comparison with the reviewed literature , our patient cohort includes an average to rather high percentage of intermediate - risk patients33% according to the risk stratication by damico et al . 
as previously described by engeler et al . , our data also conrm that an early increase in psa after bt indicates a psa bounce and that this is associated with a lower risk of biochemical failure [ 29 ]  . we demonstrated that younger men treated with bt for clinically localized prostate cancer have excellent diseaserelated outcomes . 
however , even though the prognosis of localized prostate cancer is good regardless of the treatment modality , the negative effects of the treatment and possible effects on quality of life should be taken into account in the decision - making process . 
including 36 randomized controlled trials concluded that , aside from mixed ndings regarding urinary function , bt and radical prostatectomy were comparable in terms of quality of life , while bt was favorable in terms of patient satisfaction and sexual function [ 30 ]  . 
a recent longitudinal assessment in 907 patients reported that surgery resulted in signicantly higher urinary incontinence than radiotherapy ( bt or external beam radiotherapy ) , but fewer urinary irritation or obstruction symptoms . 
radiother712 strahlenther onkol ( 2017 ) 193 : 707713 apy showed better sexual function than surgery , but sexual bother was similar [ 31 ]  . even though the data were prospectively collected , the study has a retrospective character and thus the accompanying limitations , such as inherent biases in patient and treatment selection , possible confounding variables , incomplete outcomes and losses to follow - up . 
furthermore , the denition of a psa bounce , risk stratication , and local failure may cause variation among ndings . conclusion the excellent outcome in conclusion , our data support of younger men treated with brachytherapy for clinically localized low - risk prostate cancer . 
whereas adjuvant or extremely early srt irrespective of psa progression might be overtreatment for some patients , srt at psa > 0.2 ng / ml might be undertreatment for others . 
whrend eine adjuvante oder extrem frhe srt unabhngig vom psa - verlauf fr einige patienten eine bertherapie bedeuten wrde , wre eine srt bei einem psa > 0 , 2 ng / ml fr andere eine untertherapie . 
kohorte wurden 293 mnner mit einem psa von 0 , 10 , 19 ng / ml nach rp auf die endpunkte weiterer psa - progress sowie metastasen unterstrahlenther onkol ( 2017 ) 193 : 692699 sucht . 
kohorte bildeten 198 mnner , welche mit einer srt behandelt wurden und deren progressionsfreies berleben in abhngigkeit vom psa vor srt ( 0 , 030 , 19 vs . 0 , 20 , 499 ng / ml ) untersucht wurde . 
kohorte hatten 281 patienten ( 95 , 9 % ) einen weiteren psa - progress 0 , 2 ng / ml und 27 mnner ( 9 , 2 % ) entwickelten im medianen follow - up von 74 , 3 monaten metastasen . 
zudem zeigte sich ein erhhtes progressionsrisiko , wenn der psa vor srt 0 , 2 ng / ml betrug ( hazard ratio 1 , 8 ; p < 0 , 05 )  . schlussfolgerung bei der berwiegenden mehrheit der patienten mit einem psa 0 , 1 ng / ml nach rp wird dieser im weiteren verlauf auf 0 , 2 ng / ml ansteigen . 
als konsequenz schlagen wir eine psa - grenze von 0 , 1 ng / ml fr ein biochemische rezidiv nach rp vor . schlsselwrter prostatakrebs neoplasie , metastasierung berleben adjuvante strahlentherapie prostataspezisches antigen rising psa is frequently recorded ( 1525% ) in men after radical prostatectomy ( rp ) for clinically localized prostate cancer ( pca ) , and most likely represents the rst sign of progression after surgery [ 13 ]  . 
these recommendations are questioned by current data showing improved cancer control when srt is administered at earlier psa levels after rp [ 14 , 15 ]  . the situation becomes increasingly complex when the competing concept of adjuvant radiotherapy ( art ) comes into play . 
in particular , patients with adverse pathological characteristics at rp might benet most from immediate art [ 1618 ]  . however , a certain overtreatment might be expected when immediate art is administered . 
specically , 2540% of potential art candidates did not progress until 10 years after surgery , although a wait and see strategy was selected [ 16 , 19 , 20 ]  . 
additionally , radiotherapy might affect urinary continence recovery when applied too early after rp [ 17 ]  . considerable efforts have been made to address the best timing of srt and early salvage radiotherapy ( esrt ) [ 14 , 21 , 22 ]  . 
the t - test , mannwhitney test , and chi - square test were used to compare the statistical signicance of differences in means , medians , and proportions , respectively . 
statistical analyses were performed with jmp software ( jmp , sas , cary , nc , usa ) and r ( version 2.13.1 ; org ) , with winstat for excel ( microsoft , redmond , wa , usa ) and spss ( ibm corp . , armonk , ny , usa ) , respectively . results patient cohort 1 baseline characteristics overall , 293 patients were identied . 
the median time from psa cutoff > 0.1 ng / ml to psa progression 0.2 ng / ml was 7 months ( table 2 )  . metastases overall , 27 ( 9.2% ) men developed metastases during follow - up . 
of these patients , 15 ( 55.6% ) had adverse pathological characteristics ( pt3b , gleason score 8 , positive surgical margin ) at rp , and 27 ( 100% ) had psa progression 0.2 ng / ml ( table 1 )  . 
the median time from psa cutoff > 0.1 ng / ml to metastases was 28.3 months , and from psa cutoff 0.2 ng / ml to metastases this was 21.8 months ( table 2 )  . patient cohort 2 baseline characteristics overall , 198 patients were identied . 
the target volume for srt was either the prostate compartment in case of pt2 , or the prostate bed and the region of the seminal vesicles in case of pt34 , all including 1 cm safety margins . 
this advantage was conrmed , albeit not statistically signicant , when calculating from the time of rp ( supplementary gure )  . multivariable cox regression analyses we relied on multivariable cox regression analyses to predict progression after srt . 
2 kaplanmeier plot of freedom from progression after salvage radiotherapy ( srt ) , stratied according to pre - srt prostate - specic antigen ( psa ) level 0.030.199 ( red line ) vs . 
in the majority of cases without high - risk features , the administration of early srt ( psa < 0.5 ng / ml ) can signicantly reduce overtreatment , without compromising oncological outcome , when compared with art [ 22 ]  . in this complex situation , early bcr detection for identifying those patients who will benet most from esrt remains a challenging task in daily clinical practice . to address this problem , we combined observations from two independent patient cohorts . 
similarly , mir et al . , who assessed outcomes of early srt after rp , suggested administration of srt at lower psa levels and recommended a lower psa threshold to dene bcr after rp in selected patients [ 27 ]  . following the eau guidelines , srt should be administered before the psa exceeds 0.5 ng / ml , although the potential of earlier srt ( 0.10.3 ng / ml ) is discussed [ 23 ]  . 
accordingly , delaying srt beyond this psa level was a signicant risk factor for progression ( besides the gleason score ) in three different multivariable cox models predicting progression after srt . when analyzing the impact of different pathologic features on bcr , jackson et al . 
assessed a cohort of 448 srt patients ( 15% seminal vesicle invasion , 50% extracapsular extension , 46% positive margins , 2% positive lymph nodes ) with a median follow - up of 64 months . 
finally , the follow - up might be too short and more patients will develop further psa progression or metastases in the future . conclusion the vast majority of patients with a psa 0.1 ng / ml after rp must be expected to develop further psa progression . moreover , a signicant fraction of such patients will develop metastases during follow - up . 
these observations require further conrmation in prospective studies also assessing oncological outcomes such as progression - free and cancer - specic survival . compliance with ethical guidelines conict of interest l . 
immunogener zelltod ist auch eine plausible erklrung fr die seit jahren intensiv diskutierten abskopalen effekte nach radiotherapie ( remissionen nichtbestrahlter metas764 strahlenther onkol ( 2017 ) 193 : 763764 tasen nach radiotherapie einer anderen lsion )  . 
auch der systemische effekt der prophylaktischen lymphknotenbestrahlung beim mammakarzinom , der in mehreren studien einheitlich beobachtet wurde und zu einer neubewertung der regionalen bestrahlung fhrte , knnte darauf beruhen . wegen der groen bedeutung und des rasch zunehmenden einsatzes von pd - 1 - inhibitoren sind mgliche synergistische effekte dieser substanzen mit radiotherapie von besonderem interesse . 
die jetzt publizierte analyse der keynote - 001 - daten besttigt sehr eindrucksvoll , wie wichtig hier die strahlentherapie sein knnte . wie so oft ergeben sich aus den befunden aber auch zahlreiche neue fragen . 
reck m , rodriguez - abreu d , robinson ag et al ( 2016 ) pembrolizumab versus chemotherapy for pd - l1 - positive non - small - cell lung cancer . 
reits ea , hodge jw , herberts ca et al ( 2006 ) radiation modulates the peptide repertoire , enhances mhc class i expression , and induces successful antitumor immunotherapy . 
sieker6 rita engenhart - cabillic7 michael richter8 kathrin dellas9 jrgen dunst9 received : 14 january 2017 / accepted : 21 april 2017 / published online : 12 may 2017 springer - verlag berlin heidelberg 2017 abstract background cetuximab ( cet ) is a potent inhibitor of the epidermal growth factor receptor and has been shown to have activity in squamous cell carcinoma of the head and neck ( scchn )  . 
we conducted a single - arm phase ii trial of a combination therapy comprising cisplatin ( cis ) , cet and hyperfractionated accelerated radiotherapy ( hart )  . patients and methods patients with uicc stage iii or iva / b , m0 scchn were enrolled and treated with an initial dose of cet ( 400 mg / m2 ) and then with a weekly dosage of 250 mg / m2 during hart . 
hart was started with a prescribed dosage of 2.0 gy per day for 3 weeks , followed by 1.4 gy twice daily to a total dose of 70.6 gy to the gross tumour volume . 
the primary objective of the phase ii study was to determine the 2 - year progression - free survival ( pfs )  . results between november 2007 and november 2010 , a total of 74 patients were enrolled in the study , of whom 65 were evaluable ( 83% were men )  . 
the 2and 5 - year overall survival rates were 64 and 41% , the 2and 5 - year pfs rates were 45 and 32% , and the 2and 5 - year locoregional control rates were 47 and 33% , respectively . conclusion the combination of weekly cis with hart plus cet is a feasible regimen for these unfavourable smoking - induced cancers . 
however , the parallel us study ( rtog 0522 ) showed no advantage of the enhanced triple therapy compared to chemoradiotherapy alone . keywords chemoradiotherapy toxicity smoking survival mucositis clinical trial number : isrctn47339346 4 department of radiotherapy , university of regensburg , electronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 017 - 1145 - 6 ) contains supplementary material , which is available to authorized users . ( cid : 2 ) med . 
9a , 04103 leipzig , germany private praxis for radio oncology dresden , dresden , germany 3 department of radiation oncology , university of rostock , rostock , germany regensburg , germany 5 department of radiotherapy , otto von guericke university of magdeburg , magdeburg , germany 6 department of radiotherapy , martin luther university of halle - wittenberg , halle ( saale ) , germany 7 department of radiotherapy , philipps university marburg , marburg , germany 8 coordination centre for clinical trials halle , halle ( saale ) , 9 department of radiation oncology , university of kiel , kiel , germany germany 734 strahlenther onkol ( 2017 ) 193 : 733741 hyperfraktionierte akzelerierte bestrahlung plus cetuximab plus cisplatin - chemotherapie beim lokal fortgeschrittenen , inoperablen plattenepithelkarzinom im kopf - hals - bereich 5 - jahres - ergebnisse einer phase - ii - studie zusammenfassung hintergrund cetuximab ( cet ) ist ein potenter inhibitor des epidermalen wachstumsfaktor - rezeptors , der schon bei plattenepithelkarzinomen des kopf - hals - bereichs ( scchn ) wirkung gezeigt hat . 
wir fhrten eine prospektive , einarmige phase - ii - studie einer kombinationstherapie mit cisplatin ( cis ) , cet und hyperfraktionierter akzelerierter strahlentherapie ( hart ) durch . patienten und methoden patienten mit einem m0 - scchn im uicc - stadium iii oder iva / b wurden eingeschlossen und mit einer cet - anfangsdosis von 400 mg / m2 und dann einer wchentlichen dosis von 250 mg / m2 whrend hart behandelt . 
hart wurde mit 2 , 0 gy pro tag fr 3 wochen begonnen und danach mit 2 - mal tglich 1 , 4 gy bis zu einer gesamtdosis von 70 , 6 gy auf das gesamttumorvolumen fortgesetzt . 
primres ziel der phase - iistudie war das progressionsfreie 2 - jahres - berleben ( pfs )  . ergebnisse von den zwischen november 2007 und november 2010 74 in die studie eingeschlossen patienten waren 65 auswertbar ( 83 % mnner )  . 
die 2und 5 - jahres - berlebensraten lagen bei 64 % und 41 % , die 2und 5 - jahres - pfs - raten bei 45 % und 32 % und die lokoregionale kontrolle nach 2 und 5 jahren bei 47 % und 33 % . schlussfolgerung die kombination von wchentlichem cis mit hart plus cet ist eine durchfhrbare therapie fr diese ungnstigen durch das rauchen verursachten karzinome . 
head and neck cancers are , introduction therefore , a signicant public health problem , causing signicant mortality and morbidity despite clinical advances that have enabled their early diagnosis and treatment [ 1 ]  . approximately 90% of head and neck tumours are squamous cell carcinomas ( scc )  . 
for unresectable locally advanced disease ( stage iii and iva / b ) , the addition of chemotherapy to rt ( chemoradiotherapy ) , administered as a concomitant treatment , improves outcome in medically t patients compared with rt alone [ 2 ]  . 
a further metaanalysis of 15 studies , which comprised 6515 patients with nonmetastatic scc of the head and neck ( scchn ) and addressed altered fractionation versus conventionally fractionated rt , conrmed an absolute survival benet of 3.4% at 5 years ( p = 0.003 ) and a locoregional control benet of 6.4% at 5 years ( p < 0.0001 ) [ 3 ]  . is commonly accepted that the efcacy benet achieved by addition of chemotherapy during rt is counterbalanced by an increase in acute toxicity , which limits the broader acceptance of such treatment , particularly for patients with a poor performance status . 
this study reported that concurrent use of the antiepidermal growth factor receptor ( egfr ) antibody with rt signicantly reduced the risk of locoregional progression and death at any given time point ( hazard ratio , hr , 0.68 ; p = 0.005 ) , and signicantly improved progressionfree survival ( pfs ; hr for disease progression or death at any given time point 0.70 ; p = 0.006 ) and os ( hr for death at any given time point 0.74 ; p = 0.03 ) compared with rt alone . 
recently , the study was updated with an unplanned retrospective evaluation of human papillomavirus 16 ( hpv16 ) dna and p16 expression in oropharyngeal carcinoma ( opc ) patients [ 5 ]  . 
importantly , the improved efcacy was achieved strahlenther onkol ( 2017 ) 193 : 733741 without an increase in the incidence or severity of toxic late effects that are commonly associated with rt . 
indeed , the addition of cet to the rt regimen did not adversely affect the quality of life of the patients compared with rt alone [ 6 ]  . cet has , therefore , been shown to improve the efcacy of both concurrent rt and platinum - based chemotherapy in the treatment of scchn , albeit in different settings [ 7 ]  . thus , these studies formed the basis to further explore the combination of cet with chemoradiotherapy in the treatment of locally advanced scchn . 
although promising levels of activity were noted , this study had to be closed early due to signicant adverse events ( aes ) of unclear attribution . the present study was therefore initiated as a phase i dose escalation and a phase ii trial to investigate the safety of combining weekly cisplatin ( cis ) with cet and hyperfractionated accelerated radiotherapy ( hart )  . patients and methods study design this trial was designed as an open - label , multicentre , single - arm , non - comparative , prospective phase i / ii study for patients with unresectable scchn union for international cancer control ( uicc ) stage iii / iv . 
in phase i , the maximum tolerated dose ( mtd ) for weekly escalated cis in combination with cet and hart was determined [ 9 ]  . phase ii was performed with cis at the recommended dose level and with the same schedule of cet and hart . 
the study was approved by the medical facultys ethics committee of the martin luther university halle - wittenberg and written informed consent was obtained from all patients . patient eligibility patients 18 and ( cid : 2 ) 70 years of age were eligible for inclusion if they had been diagnosed with histologically conrmed unresectable scc of the oral cavity ( excluding the lip ) , oropharynx , hypopharynx or larynx , which was measurable in one dimension and classied as stage iii or iva / b ( union for international cancer control 7th edition )  . 
exclusion criteria included metastatic disease ; a life expectancy of < 3 months ; pregnancy ; cancers of an unknown primary site , including the nasopharynx and salivary glands ; and previous cancer within 5 years of study entry . 
patients who had concurrent treatments with other experimental drugs or had participated in another clinical trial with any investigational drug within 30 days before study screening were also excluded . endpoints the primary objective of the study was to determine the 2 - year pfs rate in the intention - to - treat ( itt ) analysis set . the secondary endpoints included the following : pfs at 1 and 5 years after start of treatment os at 1 , 2 and 5 years locoregional pfs ( lpfs ) at 1 , 2 and 5 years objective tumour response according to response evaluation criteria in solid tumors ( recist ) toxicity according to common terminology criteria for adverse events ( ctcae ) , version 3.0 application scheme , duration of study treatment and dosage the study treatment was scheduled to last approximately 7 weeks , including administration of the loading dose of cet ( day 7 ) and 6 weeks of hart - cis - cet . 
selective lymph node dissection within 6 to 8 weeks after the end of rt was planned for all patients with complete remission of the primary tumour , but with residual neck disease . 
chemotherapy with cis was applied at the dose level of 40 mg / m2 . immunotherapy with cet was applied with a loading dose of 400 mg / m2 over a 120 - min intravenous infusion on day 7 , followed by subsequent weekly doses of 250 mg / m2 60 - min infusions for weeks 1 to 6 . 
monitoring the patient for 1 h after the infusion was also recommended ; in case of grade 3 or 4 hypersensitivity reactions , cet was discontinued [ 10 ]  . 
for rash prophylaxis , patients were requested to minimize the extent or intensity of the eruption by avoiding sunbathing or direct strong sunlight , as well as high heat or humidity during treatment [ 11 ]  . 
systemic ther736 strahlenther onkol ( 2017 ) 193 : 733741 apy , such as steroids and oral other antibiotics , was used in grade 3 or 4 rash in order to stop the symptoms or treat the complication of rash [ 11 ]  . rates were estimated by kaplanmeier estimates and are presented with their two - sided 95% ci . toxicity assessment results aes were coded using the medical dictionary for regulatory activities ( meddra ) , version 11.0 , and summarized by system organ class ( soc ) , preferred term ( pt ) and ctc grade . 
a grading scale is provided for each ae terlate irradiation - induced toxicities were graded according to radiation therapy oncology group / european organization for research and treatment of cancer ( rtog / eortc ) criteria . response assessment the response assessment was routinely performed using a neck ultrasound , ct or mri imaging , as well as endoscopically by an ent specialist . 
the objective response rate ( orr ) for the tumour was dened as the proportion of patients with either a complete response ( cr ) or an overall partial response ( pr )  . 
in the case of cr or pr , a second evaluation was performed after neck dissection according to the results of histological grading , or if no neck dissection was performed , at least 4 weeks after rst evaluation of the tumour response with ct or mri . 
if residual tumour in the primary region was still detected , no salvage neck dissection was performed . data management and statistical analysis statistical analysis was performed using sas software version 9.4 ( sas institute , cary , nc , usa )  . 
in the phase ii study , the primary endpoint was analysed by computing the 2 - year pfs rate and its one - sided 95% condence interval ( ci ) using the kaplanmeier method . 
pfs , lpfs and os patient characteristics in april 2008 , the rst patient entered the phase ii study at the recommended dose level of cisplatin 40 mg / m ( level 4 ) from phase i . 
the most frequent primary tumour sites were the oropharynx ( 49% ) and hypopharynx ( 29% )  . patient and tumour characteristics are presented in table 1 . protocol compliance protocol compliance is presented in table 2 . 
in sum , 46 of 65 ( 71% ) patients received 200 mg / m2 cis . an additional 49 patients ( 75% ) received more or equal to 90% of the planned cet dose . 
a grade 3 allergic reaction to the initial dose was experienced by 2 patients ; therefore , the therapy with cet was stopped for these patients . acute and late toxicity none of the 65 phase ii patients experienced grade 5 acute toxicity aes ; however , 56 patients experienced grade 3 toxicity and / or grade 4 aes ( table 3 )  . 
the most frequent grade 3 lts were dysphagia in 6 patients , xerostomia in 5 patients , skin brosis or dysgeusia in 3 patients . grade 4 lts were mucous membrane late rt morbidity in strahlenther onkol ( 2017 ) 193 : 733741 table 1 patient characteristics for the itt population in phase ii table 3 acute toxicities with grades 2 , 3 and 4 characteristics gender male female median age ( years ; range ) primary tumour site oral cavity oropharynx hypopharynx larynx tumour status t4a , b missing nodal status n0 , 1 n2a , b , c missing uicc tumour stage smoking status smoker ex - smoker non - smoker unknown salvage lymph node dissection missing no . 
of patients ( % ; n = 65 ) 47 ( 72 ) 18 ( 28 ) 56 ( 85 ) 61 ( 94 ) 49 ( 75 ) 4 ( 6 ) 2 ( 3 ) 40 ( 61 ) 3d - crt three - dimensional conformal radiation therapy , imrt intensity - modulated radiation therapy a2 patients with allergic reaction grade 3 , treatment stopped no . 
no change or stable disease was observed in 3 of the 65 patients ( 4% ) and progressive disease ( pd ) occurred in 1 patient ( 1% )  . 
selective lymph node dissection was performed 6 to 8 weeks after the end of rt for 16 patients ( 5% ) with cr on the primary tumour , but with residual neck disease . of these , 3 of 16 patients received surgery with radical neck dissection and 13 of 16 with selective neck dissection . overall , in 5 of 16 ( 31% ) patients , residual lymph nodes ( number of 3 , 1 , 1 , 7 and 4 lymph nodes ) were still found . on average , 12 lymph nodes ( 1 to 31 ) were removed . salvage treatment after relapse was undergone by 28 patients ; 11 of 28 ( 39% ) patients underwent surgery and in 9 of 28 ( 32% ) patients rt was applied . 
this was more than half of the patients ( table 4 )  . discussion we have demonstrated the safety and feasibility of hartcis - cet , a trimodality regimen , in the dose escalation phase i trial with cis at a maximum dose of 40 mg / m2 / week [ 9 ]  . 
in a total of 16 patients , one dose limiting toxicity ( dlt ) occurred with one grade 4 neutropenia and subsequent death 1 week after the end of treatment . in the clinical phase ii trial , the most common and serious drug reactions were mucositis and pharyngitis with grade 34 severity . 
the known side effect of allergy attributed to cet was with 2 pts low and has also been observed in other studies [ 12 ]  . to date , 10 studies with designs similar to that of our reported trial have been published [ 8 , 1321 ]  . 
a direct comparison of the most important acute side effects and grade 5 toxicities of the three studies with cis + immunoradiotherapy [ 8 , 17 , 19 ] are shown in table 5 . 
compared to rtog 0522 , signicantly more cases of grade 3 to 4 mucositis were reported in our hart - cis - cet study ; however , fewer cases of grade 3 to 4 erythema were observed within the irradiation elds . 
an additional retrospective subsequent analysis of three - dimensional conformal radiation therapy ( 3d - crt ) versus intensity - modulated radiation therapy ( imrt ) groups of patients showed neither skin toxicity , nor other acute side effects as being signicantly different between the two groups . additional unexpected adverse reactions were not observed in our hart - cis - cet study . the results of our present phase ii study are in line with previously published data . 
table 6 shows an overview of published phase i / ii and iii studies investigating a trimodal strahlenther onkol ( 2017 ) 193 : 733741 approach of simultaneous chemoimmunoradiotherapy with cet . 
in the us studies , patients suffering from opc who were recruited for the studies were mainly positive for hpv / p16 , and only a small proportion of the patients were hpv / p16 negative . 
the hpv status of the patients in our hart - ciscet study was not determined because the prognostic implication was unknown at the time of study setup in 2005 . considering epidemiological data on hpv status in combination with opc in germany , and the time period of the study being between 2005 and 2011 , the patient population of our hart - cis - cet study can be assumed to be largely hpv / p16 negative . 
meanwhile , it has become generally known that the prognosis for hpv / p16 - positive opc patients is far better than for patients with non - hpv / p16 triggered tumours [ 22 , 23 ]  . 
compared with the current studies , a good efcacy of the trimodality regimen can be stated ( table 6 )  . our study was initially planned with the purpose of generating an experimental treatment arm for further testing against the standard therapy of simultaneous cis plus chemoradiotherapy on the phase iii level . 
however , in the interim , the results of the parallel us study ( rtog 0522 ) showed no advantage of the chemoimmunoradiotherapy with rt plus cis and cet regimen compared to chemoradiotherapy alone [ 17 ]  . 
from the clinical point of view , no further research is currently required for the combination of rt plus simultaneous cis and cet . in this context , further research on possible mechanisms of resistance and not yet investigated mechanisms of mutually inuencing factors is required . acknowledgements we thank the patients and their families and the medical staff at the various centres who contributed to the patients care . 
we also thank the coordinating centre of the clinical studies at the martin luther university halle - wittenberg for data monitoring and the merck kgaa ( darmstadt , germany ) for providing the study medication . 740 strahlenther onkol ( 2017 ) 193 : 733741 strahlenther onkol ( 2017 ) 193 : 733741 compliance with ethical guidelines conict of interest t . 
dunst declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
es erfolgte eine retrospektive analyse der daten von 1837 patienten , die an einem zentrum wegen einer arteriovensen malformation oder gutartiger tumoren ( meningeom , vestibularisschwannom , hypophysenadenom , glomustumor ) zwischen 1990 und 2009 mit srs behandelt wurden . 
patienten wurden von der auswertung ausgeschlossen , wenn sie der untersuchung nicht zustimmten ( n = 31 ) , eine genetische prdisposition fr tumorerkrankungen ( n = 84 ) hatten , frher bzw . 
maligne transformationen fanden sich bei 7 von 316 patienten mit meningeom ( 2 , 2 % ) und bei einem der 358 patienten mit vestibularisschwannom ( 0 , 3 % ) , und zwar im median 4 , 9 jahre nach srs ( spanne 2 , 813 , 8 jahre )  . 
das risiko nach srs war 0 , 0 % nach 5 jahren ( 95 % - kondenzintervall [ ki ] 0 , 00 , 4 % ) , 0 , 0 % kommentar originalpublikation pollock be , link mj , stafford md , parney if , garces yi , foote rl ( 2017 ) the risk of radiation - induced tumors or malignant transformation after single - fraction intracranial radiosurgery : results based on a 25 - year experience . int j radiat oncol biol phys 97 ( 5 ) : 919923 ( cid : 2 ) med . 
dieses ergebnis entspricht den 766 strahlenther onkol ( 2017 ) 193 : 765766 ergebnissen anderer autoren [ 13 ] , die nach srs kein erhhtes tumorrisiko im vergleich mit der normalbevlkerung fanden . 
insgesamt scheint das kumulative sekundre tumorrisiko nach srs deutlich unter den mutmalichen 12 % nach konventioneller externer bestrahlung zu liegen [ 46 ]  . allerdings bestehen bei der vorliegenden arbeit zwei erhebliche limitierungen der aussagekraft , weil erstens der nachbeobachtungszeitraum noch kurz war und zweitens bei der stereotaxie strahleninduzierte tumoren auch im niedrigdosisbereich mglich sind , die von den autoren nicht untersucht wurden . 
die autoren beschreiben zudem leider auch nicht , in welcher form und mit welchem intervall die radiologischen kontrollen ausgewertet wurden . spannend und unabhngig von primr strahleninduzierten tumoren ist die frage einer malignisierung ursprnglich gutartiger tumoren , die nach den hier publizierten daten entittsspezisch betrachtet werden muss . 
interessanterweise war nach srs kein maligner peripherer nervenscheidentumor aufgetreten , obwohl dieser angeblich nach srs vermehrt gesehen werden soll [ 7 ]  . fazit nach den hier kommentierten daten von pollock und mitarbeitern treten nach intrakranieller stereotaktischer bestrahlung keine strahleninduzierten hirntumoren auf . 
carlson ml , glasgow ae , jacob jt et al ( 2016 ) the short - term and intermediate - term risk of second neoplasms after diagnosis and treatment of unilateral vestibular schwannoma : analysis of 9460 cases . 
minniti g , traish d , ashley s et al ( 2005 ) risk of second brain tumor after conservative surgery and radiotherapy for pituitary adenoma : update after an additional 10 years . 
seferis c , torrens m , paraskevopoulou c et al ( 2014 ) malignant transformation in vestibular schwannoma : report of a single case , literature search , and debate . 
the main outcome parameters used were biochemical control ( bc ) and toxicity scores . results eleven publications reported clinical outcome and toxicity with follow - up ranging from 4191 months . 
goethe university of frankfurt , frankfurt am main , germany 2 department of radiotherapy and oncology , sana klinikum offenbach , offenbach am main , germany 3 department of radiotherapy and oncology , medical center university of freiburg , university of freiburg , freiburg , germany 4 department of medical physics and engineering , sana klinikum offenbach , offenbach am main , germany keywords side effects salvage therapy biochemical failure toxicity scores dose fractionation high - dose - rate - brachytherapie als salvagemodalitt beim lokal rezidivierten prostatakarzinom nach denitiver strahlentherapie ein systematischer review zusammenfassung zielsetzung zusammenfassende darstellung relevanter literatur zur interstitiellen high - dose - rate - brachytherapie als salvage - modalitt ( shdr - brt ) bei der behandlung des lokal rezidivierten prostatakarzinoms nach vorausgegangener denitiver radiotherapie ( rt )  . material und methoden in der pubmed - datenbank wurde eine literaturrecherche mit den suchbegriffen high - doserate , brachytherapy , prostate cancer , salvage durchgefhrt . zwischen den jahren 2000 und 2016 wurden 51 publikationen identiziert . 
die biochemische kontrolle ( bc ) sowie das assoziierte toxizittsprol waren onkologische hauptpunkte in der analyse der bercksichtigten literatur . ergebnisse von onkologischen ergebnissen und toxizitten berichteten 11 publikationen bei einer medianen nachbeobachtungszeit von 4191 monaten . 
die 5 - jahres - bc lag zwischen 18 % und 77 % bei einer genitourinren und gastrointestinalen spttoxizitt grad iii von jeweils 032 % und 05 , 1 % . schlussfolgerung die shdr - brt ist eine sichere modalitt fr die rebestrahlung des lokal rezidivierten prostatakarzinoms nach vorausgegangener denitiver rt . 684 strahlenther onkol ( 2017 ) 193 : 683691 schlsselwrter nebenwirkungen salvagetherapie biochemisches rezidiv toxizittsscores dosisfraktionierung results patient selection introduction the optimal treatment of patients experiencing biochemical failure after radical radiotherapy ( rt ) for localized prostate cancer remains a controversial clinical issue with a large number of these patients receiving palliative androgen deprivation therapy ( adt ) as sole modality [ 1 , 2 ]  . 
however , some of them harbor organ - conned disease eligible for a potentially curative procedure , thereby preventing exposure to the side effects of long - term palliative adt [ 3 , 4 ]  . 
repeat local treatment is a rational approach with different therapies such as radical prostatectomy ( rp ) , highintensity focused ultrasound ( hifu ) , and rt being clinically practiced [ 5 ]  . 
concerning the latter , high - dose - rate ( hdr ) brachytherapy ( brt ) appears to be an effective and well - tolerated reirradiation method resulting in biochemical control ( bc ) and toxicity rates which compare favorably to those reported by non - rt salvage modalities [ 616 ]  . 
to compare and weight the different studies , objective parameters like bc , according to the astro [ 17 ] or phoenix denition [ 18 ] , and toxicity scores according to the common terminology criteria for adverse events [ 19 ] or the toxicity criteria of the radiation therapy oncology group ( rtog ) / european organization for research and treatment of cancer [ 20 ] were used . local there is currently no consensus concerning patients eltherapy of organ - conned reigibility for repeat current prostate cancer and the most suitable candidates have yet to be dened . 
according to the national cancer comprehensive network guidelines [ 21 ] possible candidates include those with clinical tumor stage t1t2 , prostate specic antigen ( psa ) by the time of recurrence < 10 ng / ml , and a life expectancy > 10 years . 
the unpublished rtog 0526 study [ 22 ] , which tested low - dose - rate ( ldr ) brt for locally recurrent prostate cancer after denitive ebrt , may provide assistance for decision making using the following eligibility criteria : biopsy - proven recurrent prostatic adenocarcinoma > 30 months after the completion of ebrt , initial clinical tumor stage t1t2c , gleason score ( gs ) ( cid : 2 ) 7 , psa ( cid : 2 ) 20 ng / ml , and no evidence of metastases at diagnostic workup as well as baseline serum psa value < 10 ng / ml within 8 weeks prior to salvage brt . 
notwithstanding , the main rationale for treatment is local disease eradication in patients considered otherwise suitable for radical therapy and an evolving body of literature indicates the safe use of shdr brt as individualized treatment also for high - risk patients [ 912 ]  . 
with regard to patients general eligibility for shdr brt , the respective guidelines of the european society for radiotherapy and oncology ( estro ) [ 23 ] and the american brachytherapy society ( abs ) [ 24 ] should be invariably considered . 
not reported optimal dose - fractionation scheme are difcult to dene . most authors used fractions ranging from 611 gy yielding total physical hdr doses of 1842 gy applied in two to six fractions . 
generally , hdr irradiation was performed using a remote afterloading system and iridium - 192 was the most commonly used isotope [ 25 ]  . efcacy and toxicity the oncological results obtained with single or multiple implant regimes for extreme hypofractionated or moderately hypofractionated shdr brt are reproducible with intermediate to long - term bc without adt in two thirds of patients [ 8 , 10 , 12 , 14 , 15 ]  . 
 [ 6 ] treated in the so far largest published series 115 patients with locally recurrent disease after denitive rt ( ebrt of median 52.0 gy or hdr monotherapy of 2730 gy total physical dose )  . 
not reported table 3 oncological outcomes and late toxicity rates of salvage hdr protocols study lyszek et al . , 2009 hdr protocol gy / fraction 10.0 1 ( 3 ) 30.0 fractions ( implants ) total dose ( gy ) med . f / u ( m ) toxicity n . 
5.25 14 ( 13 ) 1739 hdr high - dose - rate brachytherapy , f / u follow - up , m months , med median , bc biochemical control , gs gleason score , gu genitourinary , gi gastrointestinal , dmfs distant metastases - free survival , n.r. 
not reported kukieka et al . , 2014 [ 11 ] wojcieszek et al . , 2016 [ 12 ] hanna et al . , 2015 [ 13 ] oliai et al . , 2013 [ 14 ] pellizzon et al . , 2009 [ 15 ] strahlenther onkol ( 2017 ) 193 : 683691 wojcieszek et al . 
the reported rates of acute overall adverse events were 52% grade 1 and 35% grade 2 toxicities . in 5 cases , shdr brt had to be stopped after the second fraction as a result of acute urinary retention . 
median presalvage psa was 5.0 ng / ml and more than half of the patients had gs 8 . the shdr brt protocol consisted of 6 fractions of 6 gy up to a total physical dose of 36 gy delivered within two implants ( 3 fractions per implant ) separated by 1 week . 
in univariate analysis , no factor was found to predict for bc after shdr brt . the rate of acute and late grade 2 gu toxicity was 36.5% and 25% , respectively . 
at a median follow - up of 36 months , the estimated psa failure - free survival at 5 years was 68.5%. acute grade 1 and 2 gu toxicities were reported in 38% and 40% of patients , respectively , with corresponding grade 1 and 2 late gu adverse events in 38% and 48% of cases . grade 3 complications , among which three urethral strictures and one case of urinary incontinence , were noted after median 9 months . 
 [ 16 ] included in their analysis 56 patients with biopsy - proven locally recurrent prostate cancer . forty - six ( 82% ) patients were initially treated with ebrt to a median dose of 72 gy and 10 ( 18% ) patients with ldr monotherapy to preplanned doses of at least 145 gy . of those , 19 ( 34% ) patients were treated with shdr brt and 37 ( 66% ) with salvage ldr brt . 
 [ 13 ] treated 28 patients among all risk groups with shdr brt of median 36 gy ( range 1546 gy ) applied in a median of 6 fractions ( range , 18 ) six of them received also additional repeat ebrt up to median 36 gy ( range 3650 gy )  . 
1 a preinterventional axial magnetic resonance imaging ( mri ) depicting the right - sided intraprostatic recurrence lesion ; b preinterventional axial [ 68ga ] - labelled prostate - specic membrane antigen positron emission tomography / computed tomography conrming the intraprostatic recurrence while not showing metastatic disease in the whole scan evaluation ; c chequered axial mri / transrectal ultrasound ( trus ) image fusion with interstitial catheters in situ and corresponding isodose distribution for real - time trus - based treatment planning . 
seven ( 32% ) patients developed urethral strictures requiring transurethral resection and 4 patients ( 18% ) manifested symptomatic hematuria treated conservatively . parallel to its implementation for whole gland treatment , shdr brt has also been applied as focal modality for the reirradiation of radiologically detectable recurrent disease [ 26 , 27 ]  . 
ultrasound - based shdr brt was performed with a prescription dose of 27 gy over two implants separated by 1 week . there were 4 , 6 , and 1 patient presenting initially with low - , intermediate - , and high - risk disease , respectively . 
in the absence of randomized clinical trials , however , the optimal therapeutic strategy remains controversial and treatment assignment appears strongly inuenced by physician bias and patient preference ( without any highergrade clinical practice guidelines being available )  . 
against this background , quality of life issues have gained increasing importance in the choice of interventional treatment with brt gaining momentum due to its potential advantages of convenience , high effectiveness , and relatively low morbidity [ 33 ]  . 
the rationale was derived from other locally directed treatments such as rp and ebrt considering that hdr can provide a treatment margin greater than salvage rp and the dose to the bladder and rectum remains signicantly lower than when treating with dose - escalated ebrt . at this point , 68ga psma - pet / ct provides a novel imaging modality with high specicity and sensitivity for the detection of locally recurrent prostate cancer as well as metastatic disease . 
it may serve as an additional tool for the selection of patients qualifying for repeat local treatment , thus replacing the use of systemic therapies such as adt [ 39 , 40 ]  . as it is the case with all aforementioned local salvage modalities , there are only few reports on long - term oncological outcomes after shdr brt . 
albeit mostly of retrospective nature and restricted to relatively small patient cohorts , some of them have reached a 5 - year follow - up with reported bc of the order of up to 77% . 
adverse events are somewhat increased in comparison to the primary setting [ 41 ] , although still acceptable compared to salvage rp ( srp ) and salvage ebrt ( sebrt ) , with predominantly grade 2 gu and gi toxicity . 
in comparison , series of srp after previous denitive rt report symptomatic anastomotic strictures in 741% , rectal injury in 028% , complete erectile dysfunction in 80100% , and complete urinary incontinence ranging from 2190% of patients [ 30 ]  . 
similarly , late grade 3 gu and gi toxicity rates in the sldr brt literature range from 047% and 020% , respectively [ 45 , 46 ]  . given the heterogeneity of clinically implemented protocols , uniform recommendations concerning the optimal dose - fractionation scheme for whole gland shdr brt are difcult to dene . 
unfortunately , there is currently no consensus concerning patients eligibility for repeat local therapy of organ - conned recurrent prostate cancer and the most suitable candidates have yet to be dened . however , according to the nccn guidelines [ 21 ] possible candidates include those with clinical tumor stage t1t2 , psa by the time of recurrence < 10 ng / ml , and a life expectancy > 10 years . 
notwithstanding , the main rationale for treatment is local disease eradication in nonmetastatic patients considered otherwise suitable for radical therapy and an evolving body of literature indicates the safe use of shdr brt as individualized approach also for high - risk patients [ 912 ]  . 
for patients general eligibility for shdr brt the respective estro [ 23 ] and abs [ 24 ] guidelines should be considered with the presence of rectal stula as well as the inability to undergo anesthesia or high lithotomy position being absolute contraindications . 
a larger prostate volume ( > 50 cc ) and the presence of lower urinary tract symptoms ( ipss > 20 ) are considered relative contraindications with the target volume being dened as the whole prostate gland . conclusion for patients with organ - conned recurrent prostate cancer , a number of locally directed treatment options are available . among them whole gland shdr brt appears to represent a safe and efcacious radio - oncological modality . 
gabriele2 received : 25 november 2016 / accepted : 29 may 2017 / published online : 15 june 2017 springer - verlag berlin heidelberg 2017 abstract purpose and objective to test the hypothesis that a rectal and bladder preparation protocol is associated with an increase in prostate cancer specic survival ( pcss ) , clinical disease free survival ( cdfs ) and biochemical disease free survival ( bdfs )  . patients and methods from 1999 to 2012 , 1080 prostate cancer ( pca ) patients were treated with three - dimensional conformal radiotherapy ( 3dcrt )  . 
multivariate analysis ( mva ) indicated for all treated patients and intermediate high - risk patients that the gleason score ( gs ) and the rectal and bladder preparation were the most important prognostic factors for pcss , cdfs and bdfs . 
die multivariate analyse ( mva ) aller behandelten patienten und der patienten mit moderat hohem risiko zeigte , dass der gleason - score ( gs ) und die rektum - blasen - vorbereitung die wichtigsten prognostischen faktoren des pcss , cdfs und bdfs waren . 
hinsichtlich der patienten mit hohem und sehr hohem risiko waren in der univariaten analyse ( uva ) gs , rbv , prostatakarzinom - staging und strahlentherapiedosis prdiktoren fr pcss , cdfs und bdfs . schlussfolgerung wie unsere studie deutlich belegt , verringert die rbv signikant die biochemischen und klinischen rckflle und die wahrscheinlichkeit eines prostatakarzinombedingten tods bei patienten ohne tgliche bildgefhrte prostatalokalisierung , vermutlich weil die patienten mit rbv im vergleich zu nrbv - patienten whrend der gesamten behandlung reproduzierbar ein leeres rektum und eine angenehm volle blase haben . schlsselwrter behandlungsergebnisse prostatakarzinom rektumund blasenvorbereitung bildgefhrte strahlentherapie risikoorgane introduction prostate cancer ( pca ) is one of the most common malignancies in men . 
three - dimensional conformal radiotherapy ( 3dcrt ) is among the principal treatment options that has been used to improve tumor control probability by dose escalation [ 1 ] and to minimize dose to the surrounding organs at risk ( oars )  . 
generally , in order to perform a safe delivery of high doses with 3dcrt and to reduce the radiation dose delivered to rectum and bladder oars , reduced margins , especially in the posterior direction , are added to the clinical target volume ( ctv ) in order to dene the planning target volume ( ptv )  . 
however , the main caveat related to ctv expansion limitation might be the increased risk of geographic miss of a portion of the target , which might result in higher rates of local failure , especially when patients are not positioned daily on the basis of direct prostate localization . 
several studies , in fact , have reported significant and greatest prostate position changes between dose fractions in the anteroposterior direction with deviation that may be as much as 2 cm [ 24 ]  . 
variable rectal lling and , to a lesser extent , bladder lling have been found to be the major causes of movement of prostate and seminal vesicles [ 3 , 57 ]  . 
moreover , the impact of organ lling during the treatment on dose - volume parameters is extremely important in order to quantitatively assess in a correct way the risk of complications from dose - volume information . 
in the literature , several prognostic factors have been estimated as predictors of pca outcome , such as the gleason score ( gs ) , initial prostate specic antigen ( ipsa ) , pca staging , age , percentage of positive biopsy cores and prescription dose [ 810 , 25 ]  . 
moreover , despite the volume of available data , no investigation has attempted hitherto to quantify the impact of rectum and bladder preparation ( rbp ) on patients survival , while many ndings about rectal and bladder motion inuence on outcome have been reported [ 11 , 12 ]  . 
the aim of this study is to investigate the impact of rectal and bladder preparation on prostate cancer specic survival ( pcss ) , clinical disease free survival ( cdfs ) and biochemical disease free survival ( bdfs ) in patients treated with 3dcrt for pca . patients and methods between october 1999 and march 2012 , 1080 pca patients from a single center were treated with 3dcrt . 
before radiotherapy , all patients underwent a planning ct scan ( hispeed ct scanner , ge healthcare , faireld , ct , usa ) with 3 - mm slice thickness from the l2l3 lumbar vertebrae to the proximal femoral diaphysis in a supine position . the outlining of clinical target volumes ( ctvs ) and organs at risk was performed according to the international commission on radiation units and measurements 50 and 62 reports . the prostate and seminal vesicles were dened as the ctvs and the corresponding planning target volumes ( ptvs ) were generated by adding 10 - mm isotropic margins to the ctvs , with the exception of the anteriorposterior direction ( 8 mm )  . 
 [ 13 ] , as low - risk ( pca staging t1t2a , gleason score ( cid : 2 ) 6 and psa level ( cid : 2 ) 10 ng / ml ) , intermediate ( pca staging t2b , gleason score = 7 or psa level 1020 ng / ml ) , highand very high - risk ( pca staging t2c / t3 or gleason score 810 or psa level > 20 ng / ml )  . biochemical failure was dened according to the phoenix consensus as any psa increase of at least 2 ng / ml from the nadir , while clinical disease recurrence was dened as radiological evidence of local or distant disease . the patients in this study belong to a retrospective multi - centric database ( eureka - 2 ) approved by our ethical committee in november 2014 . statistical analysis survival analysis was performed using the kaplan meier method and survival differences between groups were evaluated using the log - rank test . 
the association of survival with age , gleason score , rt dose to the ptv , pretreatment psa , pca staging [ 29 ] , percentage of positive prostate biopsy cores , number of positive cores , rectal / bladder preparation , rectal and bladder volume ( continuous variables ) and adt ( use of neoadjuvant , concomitant and adjuvant therapy and duration of each therapy ) was performed with a univariate time to failure analysis using a cox proportional hazard model . 
subsequently , a multivariate cox regression analysis considering all the covariates with p < 0.1 in the univariate analysis was performed using a stepwise method to test whether signicant covariates remained signicant . 
statistical analysis showed no difference in age ( p = 0.2 ) , number and percentage of positive cores ( p > 0.6 ) , gleason score ( p = 0.5 ) and ipsa ( p = 0.08 ) between patients with and without the preparation protocol , while a signicant difference between the two groups with respect to the percentage of patients with locally advanced / advanced disease ( t3t4 ) and in the percentages of patients receiving doses in the range 75.677.7 gy and more than 77.7 gy was observed ( table 2 )  . 
the median durations of neoadjuvant , concomitant and adjuvant therapy were 3 ( 121 ) , 2 ( 12 ) and 6 ( 184 ) months for intermediate risk patients , respectively , and 3 ( 124 ) , 2 and 8 ( 194 ) months for highand very high - risk patients , respectively . 
1 kaplan - meier curves for ( a ) prostate cancer specic survival , ( b ) clinical disease free survival and ( c ) biochemical disease free survival ( bdfs ) for all 1080 patients 728 strahlenther onkol ( 2017 ) 193 : 722732 fig . 
2 kaplan - meier curves of prostate cancer specic survival , clinical disease free and biochemical disease free survival for patients with ( red ) or without ( blue ) rectal / bladder preparation in the whole cohort ( a , d , g ) , intermediate and high - risk patients ( b , e , h ) and the high - risk patient group ( c , f , i ) , respectively . 
logrank p value test results are indicated der preparation protocol than patients without a preparation protocol . univariate and multivariate cox regression analysis results for the global population , intermediate highand very high - risk patients and highand very high - risk patients are reported in table 3 . 
in mva , for all treated patients and intermediate high - risk patients , the bioptic gleason score and rectal / bladder preparation were the most important factors affecting pcss , cdfs and bdfs ; ipsa was also a signicant predictor of biochemical failures . 
3 kaplan - meier curves of prostate cancer specic survival , clinical disease free and biochemical disease free survival for patients with ( red ) or without ( blue ) rectal / bladder preparation in the whole cohort ( a , d , g ) , intermediate and high - risk patients ( b , e , h ) and the high - risk patient group ( c , f , i ) , respectively . 
in fact , taking all treated patients into consideration , signicant differences of 4% , 9% , 16.5% at 5 years and 7% , 10.5% , 16% at 10 years for pcss , cdfs and bdfs were observed between patients with and without rectal and bladder preparation , respectively . 
the choice of posterior ptv margin represents a critical problea target margin of at least 1 cm in supero - inferior and antero - posterior directions has been recommended in order to ensure 100% ctv coverage by the ptv 95% of the time [ 14 ]  . 
however , given that tumors are frequently located posteriorly in the peripheral prostate area [ 15 , 16 ] , a reduced margin combined with a signicant amount of prostate displacement relative to the planning ct would increase the risk of underdosage of the tumor . 
in fact , several studies reported that rectal distension largely inuences prostate and seminal vesicle motion , while the impact of bladder lling on prostate motion seems to be smaller [ 13 ]  . 
however , in contrast to data reported in the literature whereby rectum extension in ct was related to outcome , there was no signicant mean rectal volume difference between patients with and without preparation in our study . moreover , the univariate analysis indicated no correlation between rectal and bladder volume at simulation as continuous variables and outcome . 
therefore , on the basis of these considerations , the signicant decrease in tumor control ( pcss , cdfs and bdfs ) in patients treated without and with a rectal / bladder preparation protocol would presumably be due to patients with no preparation protocol presenting a more unstable rectal and bladder lling during the treatment course and thereby producing signicantly greater or more variable prostate displacement relative to the position identied on the planning ct scan compared with the rbp group , resulting in an increased risk of geographic miss . 
 [ 20 ] demonstrated that the use of written bladder lling instructions to the patients made it possible to keep average bladder lling closer to the ct planning volume during treatment than patients without written instructions . 
 [ 21 ] emphasized that a protocol for rectal contents during the acquisition of the planning ct scan makes it possible to minimize the systematic component of volume and dvh variations during rt . 
other factors were found to be prognostic of survival in the current investigation . in particular , in the uva analysis for all treated patients , factors affecting survival included the percentage of positive cores , the number of positive cores , gs , ipsa , pca staging beyond the rectal and bladder preparation protocol described previously . 
 [ 25 ] stated that the percentage of positive cores in the biopsy specimen represents an additional independent prognostic factor to predict pcss , as well as clinical and biochemical recurrence after external beam radiotherapy . 
the importance of rt dose on patient outcome is well documented [ 10 , 11 , 26 ] and is conrmed in our study , particularly for the high - risk sub - cohort . 
 [ 12 ] estimated how much of an additional dose might be required to compensate for the differences of 28% and 34% in 5 - year biochemical control rates according to rectal distension in intermediate - risk and high - risk groups , respectively . 
they reported that in order to compensate for these differences in 5 - year biochemical control rates according to rectal lling , a dose escalation of 15.8 gy and 18 gy for intermediate - risk and high - risk groups , respectively , is required to achieve the same control rates as for patients without rectal distension . 
indeed , in our study no signicant clinical survival difference between patients with and without rectal and bladder preparation is expected when one considers the small average dose difference of around 0.7 gy between the two groups . 
finally , in contrast to data in the literature indicating the impact of adt ( duration and setting ) on patient outcome , only an advantage for adjuvant hormone on bdfs in highand very high - risk patients was observed in our study . 
prostate igrt using ct or ultrasound - guided imaging or implanted ducial markers represents an effective tool to determine the impact of oars motion , reducing the risk of geographic miss [ 27 ]  . 
moreover , the conclusions of this study cannot be absolute : indeed , it is not possible to correct for the will rogers phenomenon [ 30 , 31 ] , which might have contributed to inuencing the outcomes . all 1080 patients analyzed in the study were treated with 3dcrt . 
despite the improvements achieved with 3dcrt in the treatment of pca since its introduction , multiple studies have shown that intensity - modulated radiation therapy ( imrt ) represents the standard mode of conformal radiation therapy for localized pca [ 32 ]  . 
in fact , the use of imrt has been associated with improved dose distributions and reduced gastrointestinal and genitourinary toxicity compared with conformal radiation therapy [ 3335 ]  . the results of our study emphasize the necessity to apply a preparation protocol in order to empty the rectum and obtain a full bladder . 
the impact of rectal and bladder preparation on patient toxicity will be analyzed in a future study . conclusions this retrospective study demonstrates that a rectal / bladder preparation protocol signicantly decreased ( hr < 0.76 ) biochemical and clinical failures and the probability of death from pca in patients treated with 3dcrt for pca without daily image - guided prostate localization , presumably since patients with rbp are able to maintain a reproducibly empty rectum and comfortably full bladder across the whole treatment course . 
given the importance of these strahlenther onkol ( 2017 ) 193 : 722732 problems , continuing advances have focused on the characterization and control of organ motion and anatomical deformation , all of which introduce geometric uncertainty . nowadays , igrt represents a crucial instrument for ensuring that the prescribed dose of radiotherapy is delivered as planned into the target . 
 [ 36 ] demonstrated that the use of daily online repositioning signicantly increases the homogeneity of dose distribution to the prostate , according to validated dosimetric and radiobiological criteria , and suggested that a reduction in ptv margins could be possible . 
the points elucidated in this study are , in our opinion , of critical importance in view of the fact that they highlight a signicant direct impact on survival . funding this work was supported by 5 per mille 2009 ministero della salute - fprc onlus . 
patients were randomized and allocated to two groups , including 60 to the combination group ( tamsulosin 0.2 mg / day and trospium chloride 20 mg twice daily ) and 64 to the monotherapy group ( tamsulosin 0.2 mg / day )  . treatment began 1 day after brachytherapy and continued for 6 months . 
luts were compared between the two groups using the total international prostate symptom score ( ipss ) , storage and voiding ipss subscores , quality of life ( qol ) scores , maximum ow rate ( qmax ) , and postvoid residual ( pvr ) urine volume at 1 , 3 , 6 , and 12 months after implantation . results in all , 111 patients were ultimately analyzed in the study . 
compared with pretreatment scores , a signicant miao yan and peng xue contributed equally to this work . ( cid : 2 ) fanghu sun xuepsmile@126.com 1 department of oncology , first people hospital of lianyungang , lianyungang , jiangsu province , china 2 department of urology , first people hospital of lianyungang , 222002 lianyungang , jiangsu province , china 3 department of urology , the afliated hospital of weifang medical college , weifang , shandong province , china 4 department of urology , the first afliated hospital of nanjing medical university , nanjing , jiangsu , china increase in total ipss was found at 1 , 3 , and 6 months in both groups , but no statistically signicant differences were observed between the two groups . 
between the two groups , there was no signicant difference in ipss voiding score , qmax , and pvr from baseline to each point of the study period . conclusions combination therapy with tamsulosin and trospium chloride helped to improve ipss storage symptoms and qol scores in prostate brachytherapy patients with luts compared with tamsulosin monotherapy . keywords prostate cancer prostate brachytherapy tamsulosin trospium chloride lower urinary tract symptoms verbessert die kombinationstherapie mit tamsulosin und trospiumchlorid symptome an den unteren harnwegen nach seedbrachytherapie bei prostatakarzinom im vergleich zu tamsulosin allein ? eine prospektive , randomisierte , kontrollierte studie zusammenfassung zielsetzung die wirksamkeit einer kombinationstherapie mit einem alphablocker und einem anticholinergikum sollte mit der alphablocker - monotherapie in bezug auf symptome an den unteren harnwegen nach brachytherapie bei patienten mit prostatakarzinom verglichen werden . strahlenther onkol ( 2017 ) 193 : 714721 material und methoden insgesamt wurden 124 patienten , bei denen klinisch ein lokalisiertes prostatakarzinom diagnostiziert worden war und die sich einer prostatabrachytherapie unterzogen , in die vorliegende studie eingeschlossen . 
die patienten wurden randomisiert und einer von 2 gruppen zugeordnet : 60 der kombinationstherapiegruppe ( tamsulosin 0 , 2 mg / tag und trospiumchlorid 20 mg 2 - mal tglich ) , 64 der monotherapiegruppe ( tamsulosin 0 , 2 mg / tag )  . 
fr den vergleich der beiden gruppen hinsichtlich der symptome an den unteren harnwegen wurden folgende parameter herangezogen : gesamter international prostate symptom score ( ipss ) , ipss - subscores fr speicherung und entleerung , score der lebensqualitt ( qol ) , maximale flussrate ( qmax ) und restharnvolumen , jeweils 1 , 3 , 6 und 12 monate nach der implantation . ergebnisse letztlich gingen 111 patienten in die analyse eim vergleich zu vorbehandlungswerten wurde in beiden gruppen eine signikante erhhung des gesamtipss nach 1 , 3 und 6 monaten festgestellt , statistisch signikante unterschiede zwischen den beiden gruppen waren aber nicht zu beobachten . 
patienten , die tamsulosin plus trospiumchlorid erhielten , zeigten auch signikante verbesserungen in der qol nach 1 und 3 monaten , verglichen mit tamsulosin allein ( p = 0 , 039 , p = 0 , 047 )  . 
zwischen den beiden gruppen gab es keinen signikanten unterschied im ipss - entleerungsscore , in qmax und im restharnvolumen von der ausgangsmessung bis zu jedem punkt des studienzeitraums . schlussfolgerung verglichen mit der tamsulosin - monotherapie trug die kombinationstherapie mit tamsulosin und trospiumchlorid zur verbesserung der ipss - speicherungssymptome und der qol - scores bei patienten mit prostatabrachytherapie und symptomen an den unteren harnwegen bei . schlsselwrter prostatakarzinom prostata brachytherapie tamsulosin trospiumchlorid niedrige harnwege symptome introduction acute lower urinary tract symptoms ( luts ) occur to some degree in the majority of patients with clinically localized prostate cancer undergoing permanent prostate brachytherapy , including symptoms such as incontinence , problems with frequency , retention , and dysuria [ 15 ]  . 
patients with luts often experienced decrements in overall healthrelated quality of life ( qol ) as symptomatic severity increased , with most people experiencing some problems with mobility , self - care , daily activities , pain / discomfort , and anxiety or depression [ 6 ]  . 
therefore , since alpha - blockers that target the prostate often fail to alleviate storage symptoms , they may not be the appropriate therapy for irritative urinary symptoms after brachytherapy . in the general population , anticholinergic drugs are the rst - line pharmacotherapy for overactive bladder syndrome ( oab )  . 
however , few controlled therapy trials have been performed to investigate the effects of anticholinergics on mitigating brachytherapy - related do and results have been inconsistent [ 9 ]  . 
in clinical practice , some physicians , including urologists , may prescribe a multidrug regimen for patients with brachytherapy - related luts , but its superiority to a single - agent therapy is unclear . 
despite the increased use of prostate brachytherapy as a curative treatment for early - stage prostate cancer , the role of combination therapy with anticholinergic and alpha - blockers has not been rigorously studied . in this prospective , randomized , controlled study , we aimed to compare the clinical efcacy of combination therapy with tamsulosin and trospium chloride to tamsulosin monotherapy for luts following brachytherapy in prostate cancer patients . material and methods this was a 12 - month , randomized , comparative study conducted in three urology centers in china . 
patients with a history of alpha - 1 adrenoceptor antagonists or anticholinergic allergy , current anticholinergic therapy , previous surgery for benign prostatic hyperplasia ( bph ) , neurogenic bladder dysfunction , recurrent urinary tract infection , concomitant active urinary tract infection , contraindications to any study drug , and patients with cognitive impairment were excluded from the study . 
since large glands can make implantation more technically difcult and increase the risk of inadequate dose coverage , patients with prostate gland volumes > 60 ml seen on threedimensional transrectal ultrasonography received androgen 716 strahlenther onkol ( 2017 ) 193 : 714721 deprivation therapy ( adt ) to reduce the size of the gland . in all , 30 ( 27% ) patients received neoadjuvant hormone therapy with luteinizing hormone - releasing hormone ( lhrh ) agonist and an antiandrogen before seed implantation for 36 months . 
no patients received hormone therapy after seed implantation during the study period . patients in the study group were treated with a permanent 125 iodine implantation at a prescribed dose of 144 gy . 
at 1 month after seed implantation , post - implant ct scanning and post - implant dosimetric analysis were performed by one radiation oncologist to evaluate the nal position of the seeds and the actual dose of radiation delivered to the gland . 
postimplant dosimetric parameters analyzed included the v100 and v150 , dened as the percent of the postimplant prostate volume receiving at least 100% and 150% of the prescribed minimal peripheral dose ( mpd ) , respectively . 
in addition , the minimal percentage of the dose received by 30% and 90% of the urethra ( %ud30 and%ud90 ) and minimal dose ( gy ) covering 30% and 90% of the urethra ( ud30 and ud90 ) were also analyzed in this study . 
no external - beam radiotherapy ( ebrt ) was administered . after the initial evaluation , patients were randomly assigned to receive tamsulosin 0.2 mg / day ( group 1 , n = 64 ) or tamsulosin 0.2 mg / day plus trospium chloride 20 mg twice daily ( group 2 , n = 60 ) for 6 months . 
the clinical efcacy evaluation was based on urodynamic and symptomatic improvement ; the total ipss , storage and voiding ipss subscores , qol scores , qmax , and pvr were measured at baseline and at 1 , 3 , 6 , and 12 months after seed implantation . 
in addition , the incidence of acute urinary retention ( aur ) and other adverse effects were compared to assess any differences in symptom improvement between the monotherapy group and the combination therapy group . the primary efcacy variable was to compare any differences in symptom improvement between the monotherapy group and the combination therapy group . 
this measure was assessed by analyzing the changes from baseline in the total ipss and qol index scores between the two groups . secondary efcacy variables were 12 - month changes in storage and voiding ipss subscores , qmax , pvr , and the incidence of aur . 
the anova ( xed effect , omnibus ) was used to conduct a power analysis , with equal to 0.05 and power equal to 80% , r2 set at 0.27 , and effect size ( f2 = r2 / [ 1r2 ] ) of ipss set at 0.37. 
the required number of valid samples was 75 patients . in addition , we extrapolated data from a previous analysis evaluating the effectiveness of prophylactic tamsulosin ( flomax ) in reducing urinary symptoms in patients that underwent 125i prostate implantation for prostate adenocarcinoma , which conrmed the sample size in the present study [ 7 ]  . 
we used the independent sample t - test , repeated measure anova , and chi - square test to determine the signicance of differences between clinical , treatment , and dosimetric parameters . 
the changes from baseline in total ipss scores , ipss sub - score ( voiding and storage symptoms ) , qol scores , qmax , and pvr were analyzed using repeated measure anova . 
all statistical tests were performed using the statistical package for social sciences , version 14.0 , software ( spss inc . , chicago , ill )  . results from july 2014 through october 2015 , a total of 136 patients were initially enrolled in the study and 12 subsequently excluded . 
in the initial tamsulosin plus trospium chloride group ( group 2 ) , seven patients dropped out due to failure to attend hospital visits during the study ( n = 1 ) , urinary retention ( n = 3 ) , serious disease ( n = 1 ) , and adverse events ( n = 2 )  . 
missing data for total ipss , ipss sub - score , qmax , postvoid residual urine , and qol score was dealt with using the last observation carried forward technique . patient characteristics are shown in table 1 . 
compared with pretreatment scores , a signifcant increase in ipss was found at 1 , 3 , and 6 months in both groups . strahlenther onkol ( 2017 ) 193 : 714721 fig . 
1 flow chart of patient disposition table 1 patient characteristics at baseline variable tamsulosin ( n = 58 ) tamsulosin + trospium chloride ( n = 53 ) p - value mean sd age ( years ) psa ( ng / ml ) prostate volume ( ml ) qmax ( ml / s ) pvr ( ml ) ipss ( baseline ) total voiding symptom sub - scores storage symptom sub - scores qol score no . 
2 the mean change in ipss total , voiding , storage , qol , qmax , and postvoid residual urine in the two groups for all 111 patients from baseline to 1 , 3 , 6 , and 12 months after seed implantation ( triangle , tamsulosin monotherapy [ n = 58 ] ; circle , tamsulosin + trospium chloride combination therapy [ n = 53 ] )  . 
ipss international prostate symptom score , qmax maximum ow rate ; qol quality of life 720 strahlenther onkol ( 2017 ) 193 : 714721 in the tamsulosin monotherapy group and one in the tamsulosin plus trospium chloride group . 
three patients in the combination therapy group and two in the tamsulosin monotherapy group reported urinary retention with a subsequent catheter dependency duration of 12 days and were withdrawn from the study . 
intervention with tamsulosin plus trospium chloride was well - tolerated and no dizziness was reported in the combination therapy group . discussion post - implantation luts , which is characterized by a combination of storage and voiding symptoms , are one of the most common side effects of prostate brachytherapy [ 4 ]  . 
in their review , stone and stock [ 11 ] reported that acute urinary morbidity included urinary retention ( 1.5%22% ) and worsening ipss in nearly all patients within 1 month following the procedure . 
the presumed causes of brachytherapy - induced luts are effects of transperineal needle insertion trauma and radiation - induced inammatory changes in the urethra and prostate [ 2 ]  . 
several investigators have reported that the duration and severity of acute brachytherapy - related urinary toxicity can be managed with prophylactic alpha - blockers [ 7 , 8 ]  . 
 [ 8 ] found that prophylactic use of alpha - blockers before permanent prostate brachytherapy resulted in signicantly lower urinary morbidity than either the absence or therapeutic use of alpha - blockers , but had no impact on either the morbidity of acute urinary retention or the ultimate need for postimplant surgical intervention . 
 [ 14 ] found that brachytherapy - induced urinary symptoms in 212 patients improved with use of three ( 1 a ) / ( 1d ) - adrenoceptor ( ar ) antagonists ( naftopidil , tamsulosin , and silodosin )  . in this study , the result of monotherapy with tamsulosin was similar to previous reports , as the ipss , qmax , and pvr of the monotherapy group was signicantly improved at 12 - month follow - up . 
unfortunately , a subset of patients develops persistent irritative symptom refractory to conventional therapy , and this remains a concern for patients and urologists . oab is a disorder that encompasses a complex of storage symptoms consisting of urgency , with or without urgency urinary incontinence , and usually with frequency and nocturia [ 15 ]  . 
in men , oab is usually attributable to do , which is dened as a urodynamic observation characterized by involuntary contractions of the detrusor muscle during the lling phase [ 16 ]  . 
 [ 17 ] found that rates of oab were signicantly higher in brachytherapy patients compared with those that had undergone radical prostatectomy ( rp ) , even after 3 years . 
these authors also found that the severity of oab symptoms , as well as variability of symptoms , was signicantly higher than in those patients treated with rp . in the general population , anticholinergic drugs have been shown to be safe and effective in the treatment of oab . 
given the fact that the severity of oab symptoms after brachytherapy returns to its pretreatment baseline within a matter of months , patients are often treated empirically in daily practice . 
although there is still a lack of data on the use of anticholinergic drugs in brachytherapy patients with prostate cancer , these medications are those most commonly used in clinical practice in patients with luts , so there should be no concern in using these drugs as therapy for patients with urinary symptoms consistent with an overactive bladder after brachytherapy . given these individual prescription - drug benets , combination treatment trials with both anticholinergic and alpha - blockers have been of interest . 
in the current study , the result of combination therapy with tamsulosin plus trospium chloride in the treatment of acute luts following brachytherapy was similar to previous reports on male luts attributed to bph and bladder outlet obstruction ( boo ) , since combination therapy signicantly improved storage ipss subscores and qol at 12 - months follow - up . 
despite this , some physicians still remain extremely reluctant to prescribe anticholinergics due to the concern of aur in routine clinical practice , especially in patients with obstructive voiding symptoms . 
in our study , the change in qmax and pvr volume observed with combination therapy was not statistically greater than the monotherapy group : three ( 5.0% ) developed aur , comparable to the 3.1% instrahlenther onkol ( 2017 ) 193 : 714721 cidence in the monotherapy group , which emphasizes the fact that patients with increased aur risk treated with this therapy should be carefully monitored . 
these ndings suggest that combination therapy may have an advantage in the management of luts after 125i prostate brachytherapy in comparison to monotherapy . there are several limitations that need to be considered in our study . 
firstly , given the relatively small number of samples for evaluation and the short duration of this trial , a large - scale study with a longer follow - up period on tamsulosin plus trospium chloride therapy is required . 
finally , the placebo effect was not taken into consideration , despite the fact that the placebo effect is particularly relevant in men with luts [ 18 ]  . conclusions the results of this study indicate that combination therapy with tamsulosin and trospium chloride helped to improve storage symptoms and enhance qol in prostate brachytherapy patients with luts compared with tamsulosin monotherapy . 
less is known regarding comparisons of different igrt techniques and the resulting residual errors , as well as regarding their inuences on dose distributions . patients and methods a total of 58 patients who received tomotherapy - based rt up to 84 gy for high - risk prostate cancer underwent igrt based either on daily megavoltage ct ( mvct ) alone ( n = 43 ) or the additional use of gold markers ( n = 15 ) under routine conditions . 
planned adaptive ( accuray inc . , madison , wi , usa ) software was used for elaborated ofine analysis to quantify residual interfractional prostate positioning errors , along with systematic and random errors and the resulting safety margins after both igrt approaches . 
interfractional as well as intrafractional displacements were determined . results particularly in the vertical direction , residual interfractional positioning errors were reduced using the gold marker - based approach , but dosimetric differences were moderate and the clinical relevance relatively small . 
intrafractional prostate motion proved to be quite high , with displacements of 13 mm ; however , these did not result in additional dosimetric impairments . ( cid : 2 ) peter wust , md peter.wust@charite.de 1 department of radiation oncology and radiotherapy , charit universittsmedizin berlin , augustenburger platz 1 , 13353 berlin , germany conclusion residual interfractional positioning errors were reduced using gold marker - based igrt ; however , this resulted in only slightly different nal dose distributions . therefore , daily mvct - based igrt without markers might be a valid alternative . keywords prostate carcinoma radiotherapy , imageguided organs at risk conebeam computed tomography rectum dosimetrische vernderungen durch interund intrafraktionelle prostataverschiebungen bei der tomotherapie vergleich der goldmarkerbasierten registrierung mit nativer mvct zusammenfassung einfhrung bei der hochdosierten bestrahlung des prostatakarzinoms sind die bildgesteuerte ( igrt ) und die intensittsmodulierte bestrahlung ( imrt ) standard . 
offene fragen gibt es beim vergleich von igrt - techniken im hinblick auf residuelle fehler und beeinussungen der dosisverteilung . methoden und patienten bei 58 patienten , deren hochrisiko - prostatakarzinom am tomotherapie - system bis 84 gy bestrahlt wurde , durchliefen die igrt entweder routinemig basierend auf einem alleinigen megavolt - ct ( mvct ; n = 43 ) oder zustzlich unter ausnutzung implantierter goldmarker ( n = 15 )  . 
die software planned adaptive ( accuray inc . , madison , wi , usa ) wurde fr eine ofineanalyse eingesetzt , um residuelle verschiebungen , daraus resultierende systematische und zufllige fehler sowie sicherheitssume fr die beiden igrt - verfahren zu vergleichen . 
the planning target volume ( ptv ) clinical target volume ( ctv ) margins were lowered to the given values after introduction of marker - based image - guided radiotherapy ( igrt )  . 
aufgrund der geringen differenz in den dosisverteilungen ist jedoch eine igrt mit tglicher mvct ohne marker eine valide alternative . schlsselwrter prostatakarzinom bildgesteuerte strahlentherapie risikoorgane conebeamcomputertomographie rektum radiation therapy ( rt ) is an accepted standard treatment for localized prostate cancer ( pca )  . 
intensity - modulated rt ( imrt ) and image - guided rt ( igrt ) enable dose intensication with low toxicity [ 35 ]  . igrt can be realized by online cts , either cbct ( conebeam ) or mvct ( megavoltage ) , or portal imaging . additional implantation of ducial gold markers further improves the accuracy of registration [ 6 , 7 ]  . 
if the markerbased registration is compared with bony fusion based on ct or portal images , the advantage is evident [ 8 , 9 ]  . however , online cts alone contain additional information to identify the prostate position on the basis of soft tissue contrast . 
we thus analyzed a pca patient cohort comparing gold marker - based igrt with mvct - based igrt . patients and methods radiotherapy and online matching a total of 58 pca patients underwent high - dose rt using the tomotherapy system ( accuray inc . , madison , wi , usa )  . 
of these , 15 patients had gold marker - based igrt and the remaining 43 patients igrt based on mvct alone . all patients were instructed to empty the rectum and ensure standardized bladder lling during irradiation , to minimize prostate displacements . the scheme ( 84 gy to the prostate ) and safety margins for high - risk patients are shown in table 1 . 
the prescribed dose was lowered in the ctvptv margin by 10% to spare the surroundings . two or three gold markers ( visicoil , radiomed corp . , tyngsboro , ma , usa ) of 1.1 - mm diameter and 2or 3 - cm length ( depending on the prostate volume ) were implanted [ 10 ]  . every fraction started with an mvct . 
in case of ducial markers , the contours specied in the planning ct and the dense rods in the online ct were manually fused by shifting in x / y / z directions as best as possible . in the standard non - marker situation , a manual fusion of the bony structures was initially performed ; thereafter , if necessary , an additional correction was made with regard to the soft tissues ( prostate and rectum )  . 
the nal registrations were always documented in three planes and reviewed . 702 strahlenther onkol ( 2017 ) 193 : 700706 ofine analysis using mvct / planning ct we used the software planned adaptive of the tomotherapy ( accuray ) system for re - analysis . 
there are additional sources for deviations between planning and online datasets , such as deformations and twists considered as second - order disturbances , which were neglected for this analysis . the retrospective analysis using planned adaptive is described in a stepwise manner : de novo segmentation . in every evaluated online ct dataset we contoured rectum and bladder de novo , slice by slice . 
we assumed that the shape of the prostate is basically constant and manually shifted the projection of the prostate - related contour ( as generated in the planning ct as ctv - a or ctv - b , see table 1 ) along x ( with ( cid : 2 ) x ) and y ( with ( cid : 2 ) y ) , until it ts best to the prostate silhouettes in the mvct . the spatial and density resolution is considerably worsened in the reformatted sagittal and frontal slices due to the transverse data acquisition process of the mvct . 
the residual errors ( cid : 2 ) x , ( cid : 2 ) y , and ( cid : 2 ) z were the components of these difference vectors along the x - , y - , or z - direction , respectively , after averaging over the markers . 
because marker positions could be identied in the reformatted slices accurately enough , we determined residual errors also in the z - direction . in patients with implanted markers , both methods of ofine analysis were performed and compared in the same patient . 
for this subgroup , we conrmed that the displacements in the z - direction were in the same range as in the xand y - directions , thus justifying an independent survey of the three axes . in the 43 patients without markers , 337 mvct were analyzed , and in the 15 patients with gold markers , 143 mvct were analyzed . 
therefore , our results are representative for both series ( with ctv - a / b ) , as well as for the whole course . after determination of the interfractional residual prostate positioning errors ( cid : 2 ) x , ( cid : 2 ) y , and ( cid : 2 ) z , we then calculated the systematic errors x , y , z for every direction , dened as the standard deviations of the mean values of the residual displacements per patient , and the random errors x , y , z , dened as the mean value of the standard deviation of the residual displacements per patient . the resulting safety margins in the x , y , and z directions were calculated from the systematic and random errors [ 11 ]  . planned adaptive calculated the actual dose distribution in the mvct dataset and determined the dosevolume histograms ( dvhs ) of the actual ctv , as well as those of rectum and bladder . 
online dvhs were compared with the planned dvhs in terms of selected parameters . intrafractional displacements in patients with gold marker - based igrt , a second mvct was scanned after completion of rt delivery in 138 fractions . 
the dosimetric implications of intrafractional motions were also determined . results contourversus marker - based analysis interfractional positioning errors determined via mvct alone were compared with the corresponding errors employing gold markers for all 143 mvct ( with implanted markers ) , and a satisfactory correlation for the y direction strahlenther onkol ( 2017 ) 193 : 700706 marker based ( mm ) native mvct ( mm ) table 2 interfractional errors of prostate position after registration based on implanted markers or native megavolt computed tomography ( mvct ) and resulting safety margins according to the van herk formula , i . 
again , outliers were increased for the mvct - alone registration with dislocations > 2 mm in 40.9% ( non - marker ) versus 9.1% ( marker based ) in x direction . table 2 summarizes the resulting errors and safety margins . 
accordingly , systematic and random errors were higher in the vertical direction y for non - marker based registration , which leads formally to a doubling of the safety margin of ( cid : 2 ) 8 mm in comparison to ( cid : 2 ) 4 mm for markerbased registrations . 
conversely , for the lateral displacements , both igrt techniques were similar , with safety margins of ( cid : 3 ) 3 mm . evidently , gold marker - based igrt was able to correct displacements in the vertical direction . 
in particular , deviations of the prostate to the posterior were more frequent and obviously compensated by marker - based igrt . the residual positioning errors and resulting safety margins in table 2 are slightly higher in the z - direction as derived by marker - based igrt , i . 
therefore , we assumed for all observables a linear dependency on ( cid : 2 ) x , ( cid : 2 ) y , ( cid : 2 ) z , and therefore a decoupling of the errors in all three axes with reasonable certainty . dosimetric comparisons between markerand mvctbased igrt we determined dvh parameters for the ctv and oar after correcting the prostate position in the online - mvct ( table 3 )  . the upper part of table 3 compares the coverage of the ctvs . 
e. , the dose coverage in the prostate is slightly better in the rst series with an enlarged ctv . thereby dx% is the dose reached or exceeded in x% of the volume . 
a sparing effect for the rectum was not achieved by use of markers using the margins in table 1 . the lower part of table 3 shows dvh parameters for the bladder for volumes from 10 to 100 ml . 
again , the dose exposures were acceptably low for both igrt approaches , with doses of > 2030 gy only in bladder volumes below 100 ml . intrafractional dislocations of prostate and dosimetric effects the intrafractional dislocations derived from 138 pairs of mvct resulted in gaussian - like frequency distributions . the prostate motions , i . 
g. , mvct ( cbct ) and ducial markers , have been compared by others [ 12 , 13 ] and a superiority of marker - based discussion igrt in terms of interfractional displacement errors was described . 
finally , improvements of 2.12.6 gy for d95% and the near - minimum dose d98% in the prostate have been determined ( table 3 , upper part ) , i . 
the reported accuracy of imrt dose delivery ( international commission on radiation units and measurements , icru 83 ; appendix a ) [ 14 ] is within the same range . 
no relevant sparing effect with markers was found for the rectum ( table 3 , middle part ) , particularly in the high - dose region of 6072 gy ( anterior wall )  . 
improved tracking of the prostate probably equally follows the adjacent rectum , because the prostate and anterior rectal wall are closely connected by the denonvilliers fascia [ 15 ]  . it is therefore a matter of debate whether gold markers are really indispensable for advanced igrt techniques with mvct / cbct . 
this might be different for rt techniques relying on bony fusion alone ( portal imaging )  . the reduction of dose in the ctvptv margin in our patient cohort ( according to table 1 ) has been prescribed to raise dose gradients . 
in fact , table 3 shows strikingly low doses in the rectum . on the other hand , for both groups ( gold marker vs . mvct alone ) , our rt scheme led to effective doses of 7780 gy in the prostate ( table 6 )  . 
however , slightly higher doses might be desirable for high - risk patients with large tumor load [ 5 ]  . the shortcomings in dose coverage ( table 3 ) are due to the narrow safety margins and the lower dose in the ctvptv margevidently the safety margins would have to be increased for better coverage . 
tomotherapy ( with mvct ) or volumetric modulated arc therapy ( vmat ; with cbct ) might be near to a technological endpoint providing a high therapeutic quotient [ 18 ]  . intrafractional displacements ( table 4 ) are considerable and cause formal safety margins of 35 mm , in accordance with other reports [ 6 , 19 , 20 ]  . 
however , the dosimetric inuences resulting from these motions were only < 1% in our analysis ( table 5 ) , in agreement with other studies using different methods [ 21 , 22 ]  . we have found two possible explanations . 
in fact , realtime mr imaging studies ( cine mri ) showed mean displacements near zero , but standard deviations around 3 mm [ 18 ]  . second , our effort to achieve an empty rectum by repeated patient instructions might help to reduce displacements . 
graf [ 10 ] found even less interfractional variations of the prostate after appropriate patient instructions to empty the rectum . engels [ 25 , 26 ] found an increased risk of biochemical failures in patients with a distended rectum on the planning ct [ 25 ]  . 
finally , these authors recommended efforts to empty 706 strahlenther onkol ( 2017 ) 193 : 700706 the rectum prior to the planning ct and avoidance of rectal distensions . conclusion tomotherapy with daily mvct ( or vmat with cbct ) in conjunction with efforts to standardize organ lling is a valid treatment option ( effective as well as sparing ) for rt of pca . 
as a result of this , an update of the degro / dkg guidelines for radiotherapy of this patient group has been published . methods we report the case of a patient with an icd and t - lymphoblastic lymphoma with cardiac involvement , who received i.a. 
for the purposes of the treatment , the antitachyarrhythmia ( ata ) therapy was deactivated and temporarily replaced through a life vest . results according to the current degro guidelines for irradiation of patients with cardiac implanted electronic devices , a categorization of the patient in the high - risk group was made . 
furthermore , regular telemetric checks of the icd device were performed before and after treatelectronic supplementary material the online version of this article ( doi : 10.1007 / s00066 - 017 - 1152 - 7 ) contains supplementary material , which is available to authorized users . ( cid : 2 ) panagiotis balermpas , md panagiotis.balermpas@kgu.de 1 department of radiation oncology , university hospital , johann wolfgang goethe university frankfurt , theodor stern kai 7 , 60590 frankfurt , germany 2 german cancer research center ( dkfz ) , heidelberg , germany 3 german cancer consortium ( dktk ) partner site : frankfurt a . 
despite unavailable declaration of the manufacturer regarding the cumulative tolerable dose and degro recommendation for a cumulative dose < 2 gy , the aftercare was unproblematic and normal values were assessed for all relevant icd parameters , despite a cumulative dose > 10 gy in the device . conclusion this case shows that if the cardiac implanted electronic devices are not directly irradiated und the energy used is reduced to 6 mv , irradiation - induced damage is less likely and can possibly be prevented . keywords cancer pacemaker , articial radiotherapy malfunction , equipment tachycardia ein klinisches beispiel fr extreme dosisexposition eines implantierten kardioverter - debrillators jenseits der degro - leitlinien zusammenfassung fragestellung vor dem hintergrund der steigenden zahl von krebserkrankungen bei patienten ber 65 jahren kommt es hug vor , dass sich patienten mit einem kardialen implantierten elektronischen gert einer strahlentherapie unterziehen mssen . 
aufgrund dessen erfolgte eine aktualisierung der leitlinien der degro / dgk zur strahlentherapie dieses patientenkollektivs . methodik wir berichten von einem patienten mit icdimplantat und kardialer beteiligung eines t - lymphoblastischen lymphoms , der u . 
im rahmen der behandlung strahlenther onkol ( 2017 ) 193 : 756760 wurde die antitachyarrhythmische ( ata ) therapie ausgeschaltet und vorbergehend durch eine lifevest ersetzt . ergebnis gem der aktuellen degro - leitlinie zur bestrahlung von patienten mit kardialen implantierten elektronischen gerten erfolgte die einstufung des patienten in die high - risk - gruppe . 
trotz fehlender angabe des herstellers bezglich der erlaubten kumulativdosis und empfehlung der degro ber eine maximale gesamtdosis < 2 gy , zeigte sich bei einer gesamtdosis im bereich des gerts von > 10 gy in der icd - abfrage nach abgeschlossener strahlentherapie eine unauffllige nachsorge mit regelrechten messwerten fr alle relevanten icd - parameter . schlussfolgerung der fall zeigt , dass bei vermeidung einer direkten bestrahlung der kardial implantierten elektronischen gerte und bei verwendung einer energie von maximal 6 mv , eine strahleninduzierte schdigung weniger wahrscheinlich ist und vermieden werden knnte . schlsselwrter krebs knstlicher schrittmacher strahlentherapie gertefehlfunktion tachykardie with increasing incidence of cancer in patients over the age of 65 years , it often happens that a patient with a cardiac implantable electronic device ( cieds ) must undergo radiotherapy [ 1 ]  . 
for this reason , an interdisciplinary german guideline reecting patient risk based on the type of cieds , cardiac condition , and the estimated radiation dose was developed [ 1 ]  . 
1 depiction of the life vest that the patient wore while the cardiac implantable electronic device was deactivated accumulated radiation dose to the pacemaker / icd < 2 gy . patients with icd and vt or pacemaker dependent and an estimated accumulated radiation dose to the cied > 2 gy are at a high risk for a malfunction of the cied . 
the antitachyarrhythmia therapy must be deactivated for the time of treatment and a constant monitoring of the cardiac function during the time of treatment has to be ensured . case study a 42 - year - old patient was diagnosed with t - lymphoblastic lymphoma with mediastinal and pericardial manifestation in august 2013 . 
no further episodes of ventricular tachycardia occurred after that . the patient underwent systemic therapy according to the gmall / t - lbl protocol and a prophylactic cranial irradiation with 24 gy in 12 fractions using 3 elds and 6 mv photon beam energy . 
as a conditioning regime for the transplantation , total body irradiation ( tbi ) with a cumulative dose of 8 gy using a 6 mv photon beam in 2 days was scheduled ( september 2015 ) , the exact procedure for the tbi in our department has been described before [ 2 ]  . due to the icd , the patient had to undergo several cardiac examinations prior to therapy and was classied in the high - risk group ( a previous episode of ventricular tachycardia and an expected radiation dose to the cied > 2 gy ) according to the guidelines . 
the patient was at a high risk of experiencing a cied failure resulting in possible induction of ventricular brillation ( vf ) as well as sudden cardiac death during radiation while the antitachyarrhythmia function was deactivated , which is why a bridging using a life vest as well as constant monitoring through an intermediate care unit ( imc ) were organized . according to the new degro guidelines from march 2015 regarding patients with cieds undergoing radiotherapy the antitachyarrhythmia function had to be deactivated for the 2 days of treatment . 
2 excerpts from the plan of the consolidating pericardial / mediastinal irradiation , 4 elds , 6 mv solidating radiation of the primary manifestation : pericard and mediastinuaccording to the protocol the patient had to receive another 7 fractions of 2 gy each . 
according to the decision of the interdisciplinary tumor board , a combined modality treatment consisting of cyclophosphamide , cytarabine , mercaptopurine ( 6 - mp ) and granulocyte - colony stimulating factor ( gcsf ) chemotherapy and irradiation of the bulky recurrence in the upper mediastinum and the diaphragm was implemented . 
the antitachyarrhythmia function of the icd was not deactivated this time based on the recommendation of the supervising cardiologist , since the expected dose to the icd amounted to less than 1 gy . 
a comparison between the data prior to and after therapy , as well as a detailed list of the parameters checked can be found in supplementary table 2 . two months after the last irradiation ( august 2016 ) , the patient experienced a recurrence of the lymphoma . 
the antitachyarrhythmia function of the icd was not deactivated for the same reasons as previously described ( low dose to the icd and based on the recommendation of the supervising cardiologist )  . 
hu values larger than or equal to 2840 are interpreted as iron . the whole treatment was tolerated well and the icd showed no signs of malfunction or decrease in battery life . prior and after all treatments the same set of parameters was checked ( supplementary table 2 )  . 
we renounce to list every check separately as the results were similar to the ones listed above . discussion radiotherapy is a therapy option in over 70% of cancer cases nowadays , while at the same time the number of patients with a cancer diagnosis and have an implanted cardiac pacemaker or cardioverterdebrillator is growing [ 5 , 6 ]  . 
there is a growing need for data regarding the safe handling of cieds during radiation and a threshold dose for radiation - induced damage to electrical devices . the use of complementary metal oxide semiconductors in the production of cieds leads to lower energy consumption , higher dependability , and smaller devices . 
all of the damaged icds were treated with energies > 10 mv . a further problem is the monitoring of the icd function ( and detecting a malfunction ) during each fraction , especially during long single fractions as in the case of tbi . 
for this reason we cannot rule out this possibility although the patient never showed corresponding symptoms . the patient in our case study was treated with 6 mv photon beam energy . 
 [ 16 ] showed that the dose to the device and not the dose to the electrodes determines the failure . the main problem with events after irradiation of cardiac implants is that such incidents also have a stochastic component . 
experimental data , further experience , and larger patient numbers would be useful , but this is a very unusual and extreme case : a patient with 760 strahlenther onkol ( 2017 ) 193 : 756760 icd receiving a total body irradiation and an aggregate receiving a dose that has not been described before , at least in vivo . conclusion our case points out to the possibility that cardiac implanted electronic devices may indeed tolerate higher irradiation doses , especially when not directly irradiated and when using energies < 6 mv . 
further clinical trials are necessary to support this point , but determining a threshold dose for radiation - induced damage could be challenging or even impossible because of the stochastic nature of some effects . moreover , multidisciplinary collaboration is required to allow patients with cieds to receive the best possible irradiation treatment without having to suffer damage to the electrical devices . compliance with ethical guidelines conict of interest y . 
multiple fraction regimens for palliative radiotherapy treatment of multiple myeloma a prospective randomised study milda rudzianskiene1 andrius macas2 renata simoliuniene3 ruta dambrauskiene1 greta emilia kiavialaitis4 elona juozaityte1 arturas inciura1 rolandas gerbutavicius1 viktoras rudzianskas1 received : 13 december 2016 / accepted : 11 may 2017 / published online : 1 june 2017 the author ( s ) 2017 . 
this article is an open access publication . abstract purpose to compare the impact of a single fraction ( 8 gy 1 fraction ) and multifraction ( 3 gy 10 fractions ) radiotherapy regimens on pain relief , recalcication and the quality of life ( qol ) in patients with bone destructions due to multiple myeloma ( mm )  . patients and methods in all , 101 patients were included in a randomised prospective clinical trial : 58 patients were included in the control arm ( 3 gy 10 fractions ) and 43 patients into the experimental arm ( 8 gy 1 fraction )  . 
no signicant differences were observed in recalcication between the groups . ( cid : 2 ) milda rudzianskiene milda.rudzianskiene@gmail.com 1 oncology institute , lithuanian university of health sciences , eiveniu 2 , 50009 kaunas , lithuania 2 anaesthesiology department , lithuanian university of health sciences , kaunas , lithuania 3 department of physics , mathematics and biophysics , lithuanian university of health sciences , kaunas , lithuania intitute of anesthesiology , university hospital zurich , zurich , switzerland signicant factors for recalcication were karnofsky index 60% , haemoglobin level ( cid : 2 ) 80 g / dl , mm stage ii and analgesic response at the irradiated site . 
fraktionierten palliativen radiotherapie in bezug auf schmerzlinderung , knochenrekalzizierung und lebensqualitt ( qol ) bei patienten mit multiplem myelom ( mm )  . patienten und methoden in die randomisierte , prospektive studie wurden 101 patienten eingeschlossen : die kontrollgruppe ( n = 58 ) erhielt eine fraktionierte ( 3 gy 10 fraktionen ) und die experimentgruppe ( n = 43 ) eine einzeitige radiotherapie ( 8 gy 1 fraktion )  . 
die rekalzizierung wurde mittels rntgenaufnahmen ermittelt . qol - fragebgen wurden vor beginn und 4 wochen nach behandlung beantwortet . ergebnisse insgesamt 81 / 101 patienten ( 80 , 2 % ) zeigten eine schmerzreduktion : vollstndiges bei 56 ( 69 % ) und strahlenther onkol ( 2017 ) 193 : 742749 partielles ansprechen bei 25 patienten ( 30 , 9 % )  . 
wesentliche faktoren fr die schmerzlinderung waren weibliches geschlecht , alter < 65 jahre , igg - mm - typ sowie bereits vorhandene rekalzizierung der osteolytischen lsionen . eine rekalzizierung zeigte sich bei 32 / 101 patienten ( 33 , 7 % ) : vollstndig in 17 ( 53 , 2 % ) und partiell in 15 patienten ( 46 , 2 % )  . 
einussnehmende faktoren fr die rekalzizierung waren ein karnofsky - index 60 % , ein hmoglobingehalt ( cid : 2 ) 80 g / dl , ein mm - stadium ii und vorhandene analgesie an der bestrahlten stelle . 
nach radiotherapie stieg die qol nur in der kontrollgruppe . schlussfolgerung zwischen den beiden strahlentherapieregimen zeigte sich kein signikanter unterschied bei der schmerzbesserung und der rekalzizierung , jedoch besserte sich die qol nur nach multiplen fraktionen signikant . schlsselwrter osteoklastischer knochenverlust berleben schmerzlinderung rekalzizierung lebensqualitt introduction skeletal related events is one of the signs of multiple myeloma ( mm ) [ 1 , 2 ]  . 
osteoclastic destructions reduce patients quality of life ( qol ) and decreases patient survival [ 3 ]  . bone pain is the rst sign of mm for 70% of patients and the patients receive radiation at least once during their mm therapy [ 4 ]  . 
recalcication of bone destruction is observed in 4060% [ 4 , 6 , 11 , 12 ]  . results of previous clinical trials have shown the same effect of pain relief and recalcication when applying different radiotherapy regimens for treatment of patients with solid tumour metastases [ 1316 ]  . 
no randomized prospective study has been carried out worldwide to date comparing multifraction and single fraction regimens for treatment of patients with mm bone disease and the impact on pain relief , recalcication and qol . 
the aim of this prospective study was to evaluate these endpoints raising the hypothesis that one single fraction has the same analgesic and recalcication effect as compared to multifraction therapy . patients and methods from 20102015 a randomized prospective clinical trial was performed at the lithuanian university of health sciences . 
multifraction radiotherapy regimen ( 3 gy 10 fractions ) was applied to the control group of patients and single fraction regimen ( 8 gy 1 fraction ) was applied to the experimental group . 
inclusion criteria were the following : age over 18 years , diagnosis of mm according to the international myeloma working groups criteria [ 17 ] , presence of painful bone destructions or impending fracture veried by radiographs , karnofsky index ( ki ) above 40% , written informed consent . 
exclusion criteria were the following : presence of bone metastases from solid tumours , solitary plasmacytoma , prior irradiation at the same site , inability to complete the qol questionnaires , patients that could not be monitored . 
informed consent was obtained from all the participants prior to enrolment in the study . a total of 101 patients ( 65 women and 36 men , median age : 66.6 years , range 4388 years ) were included in the study . 
high points in the functional scales and in the global health status scale indicate a good functional status , whereas high points in the symptom scales indicate a poor status of health . 
qol was evaluated before radiotherapy and 4 weeks post treatment . the analgesic response rate was dened according to the international consensus on palliative radiotherapy criteria [ 24 ]  . since there is no common criteria of recalcication , we used criteria from other studies [ 6 , 25 ] : complete response 744 strahlenther onkol ( 2017 ) 193 : 742749 table 1 patients characteristics characteristics control group , no . 
the mannwhitney u test was used to compare values of quantitative features not distributed by normal law between two independent groups and kruskalwallis test was used to compare them among three or more independent groups . 
stepwise variable removal procedure ( backward conditional ) was used to determine a model with variables which inuence is statistically signicant : all analysed parameters were entered to the initial logistic model and at each step of the procedure the least signicant parameter was removed from the model until all remaining parameters showed a statistically signicant inuence on pain relief , recalcication or qol . 
findings of the model with the biggest nagelkerke pseudo coefcient of determination which indicates goodness of t of the model , and with the biggest percent of correct classication of all cases are published in the article . 
the inuence of demographic , clinical and symptom variables to pain relief , recalcication and qol was considered as statistically signicant if the condence interval of odds ratio did not include the value 1 . results pain relief all patients had been suffering from pain prior to radiotherapy . 
patients in the control group before treatment reported a median vas of 8 ( range 210 , mean 7.4 ) , 4 weeks after radiotherapy their median vas was 4 ( range 010 , mean 3.6 ) , after 12 and 24 weeks the median vas was 0 . 
patients in the experimental group before treatment reported a median vas of 8 ( range 210 , mean 7.5 ) , 4 weeks after radiotherapy the median vas was 3 ( range 010 , mean 4.2 ) , after 12 and 24 weeks the median vas was 0 . 
other factors analysed were not statistically signicant ( table 3 )  . recalcication bone x - ray images of 95 patients ( 94.1% ) were evaluated for recalcication , x - ray images of 6 patients were excluded due to early death . 
no signicant differences were observed between the groups . univariate statistical analysis revealed that ki 60% ( p = 0.004 ) and pain relief in the irradiated site ( p = 0.011 ) were signicant parameters for recalcication , whereas other parameters were not statistically signicant . all the parameters mentioned above were included in the binary logistic regression model for analysis of their inuence on recalcication : ki 60% , haemoglobin level ( cid : 2 ) 80 g / dl , ii stage of mm and analgesic response in the irradiated site have a signicant impact on recalcication . 
four weeks after radiotherapy , in the control group the median med was 10 ( mean score 44.2 , range 0190 ) and in the experimental group med was 25 ( mean score 58.7 , range 0270 )  . 
interestingly , the qol after radiotherapy was only signicantly improved in the control group ( table 6 )  . side effects acute toxicity was evaluated in the rst 4 weeks after radiotherapy . 
no signicant difference was found between the groups . discussion pain relief radiotherapy produces an analgesic effect by inhibiting chemical pain mediators and causing tumour shrinkage . the effect of radiation dose on pain relief is a matter of debate . 
the results of randomized clinical studies of palliative radiotherapy of bone metastases from solid tumours do not show superiority of any particular radiotherapy regimen [ 1316 , 27 , 28 ]  . 
the role of different radiotherapy regimens for mm is not well established [ 412 ]  . some studies did not nd a signicant difference between the dose of radiation and pain reduction [ 4 , 7 , 9 , 11 ] ; however , adamietz et al . 
 [ 10 ] reported the need for higher doses to obtain adequate pain relief . the current study conrms the efcacy of 8 gy single fraction radiotherapy : the overall analgesic response was 74% , most patients achieved pain relief in the rst 12 weeks and analgesic effect remained throughout the follow - up period . binary logistic regression did not show a signicant impact of dose on pain relief . in studies reported by adamietz et al . 
 [ 5 ] and mose et al . [ 11 ] concurrent chemotherapy had a signicant impact on a positive response to radiotherapy , but our and other studies did not show this relationship [ 4 , 9 ]  . 
lack of correlation with chemotherapy may be because chemotherapy effectively reduces tumour bulk but its effect on local symptoms is not always sufcient . 748 strahlenther onkol ( 2017 ) 193 : 742749 mose et al . 
the effect of radiation dose on recalcication is a matter of debate . koswig and budach [ 29 ] found that multifraction regimens signicantly increase the bone density in the area of metastases compared with single fraction ; also stolting et al . 
the use of bisphosphonates was insignicant but this may be due to the small sample of patients ( only 18% ) who were using bisphosphonates . quality of life novel therapies have led to an improvement in survival , which has resulted in an increase in symptom burden due to the disease itself and the effects of treatments [ 30 , 31 ]  . there are some clinical trials that analyse the effect of radiotherapy on qol in the treatment of patients with metastases , but there is no clinical study in the treatment of patients with mm . 
this could be associated with the fact that there were younger patients and a higher total equivalent dose was prescribed , which could lead to better disease control and improvement in qol . we evaluated qol before and 4 weeks after radiotherapy and a longer follow - up period evaluating qol might have shown an even greater improvement . 
thus , more studies are needed to address this observation in more detail . two studies showed that higher ki correlate with better qlq - c30 scales [ 37 , 38 ]  . 
 [ 38 ] , we found that radiotherapy to pelvic bones was a signicant parameter for better evaluation of the qlq - c30 global health status scale . this study has potential limitations . 
the treatment arms were imbalance by age and the irradiated sites which could be a reason that qol was improved in the control group . additionally the logistic regression showed that age under 65 years has signicant impact on pain relief . 
in the control group there were more young patients ; thus this age discrepancy should be taken into consideration when comparing pain relief between groups . conclusion our study revealed no signicant differences in the analgesic and recalcication response between two different radiotherapy regimens ; however , only multiple fraction radiotherapy achieved a signicant improvement in qol . 
juozaityte declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
this article is an open access publication . abstract purpose gold - marker - based image - guided radiation therapy ( igrt ) of the prostate allows to correct for interand intrafraction motion and therefore to safely reduce margins for the prostate planning target volume ( ptv )  . 
however , pelvic ptvs , when coadministered in a single plan ( registered to gold markers [ gm ] ) , require reassessment of the margin concept since prostate movement is independent from the pelvic bony anatomy to which the lymphatics are usually referenced to . methods we have therefore revisited prostate translational movement relative to the bony anatomy to obtain adequate margins for the pelvic ptvs compensating mismatch resulting from referencing pelvic target volumes to gms in the prostate . 
johanns - spital , paracelsus medical university of salzburg , mllner hauptstrae 48 , 5020 salzburg , austria conclusion gm - based igrt for pelvic ptvs is feasible if margins are adapted accordingly . 
margins could be reduced further if systematic errors which are introduced during the planning ct were eliminated . keywords prostate igrt margins lymph node irradiation gold - marker ein igrt - sicherheitsrand - konzept fr den pelvinen lymphabuss bei hochrisikoprostatakarzinom zusammenfassung einfhrung eine goldmarker - ( gm - ) basierte , bildgefhrte radiotherapie der prostata ermglicht interund intrafraktionelle bewegungen auszugleichen und somit sicherheitsrnder der planungszielvolumina ( ptv ) zu minimieren . 
da bewegungen der prostata und des lymphabusses unabhngig voneinander sind , mssen ptv - rnder der pelvinen zielvolumina neu bewertet werden . methoden wir haben die relativbewegung von prostata zur knchernen anatomie bestimmt , um daraus sicherheitsrnder zu generieren , die den durch registrierung von pelvinen ptvs zu den gm resultierenden versatz in der prostata kompensieren . 
relative prostatabewegungen wurden bei 28 patienten ( jeweils 25 fraktionen , 684 insgesamt ) analysiert und die entsprechenden rnder mittels der formel nach van herk m = 2 , 5 + 1 , 64 ergebnisse die gesamte mittlere prostatabewegung relativ zur knchernen anatomie betrug 0 , 9 3 , 1 , 0 , 6 3 , 4 und 0 , 0 0 , 7 mm in a / p ( anterior / posterior ) , i / s ( inferior / ( cid : 2 ) ( cid : 2 ) 0 ( cid : 2 ) p berechnet . ( cid : 3 ) strahlenther onkol ( 2017 ) 193 : 750755 superior ) und l / r - richtung ( links / rechts )  . 
10 / 11 / 6 mm unter annahme eines zustzlichen systematischen fehlers von 2 mm . schlussfolgerung die gm - basierte igrt mit referenzierung pelviner zielvolumina ist mglich , wenn die sicherheitsrnder entsprechend adaptiert werden , um den resultierenden versatz zur knchernen struktur auszugleichen . eine weitere reduktion der sicherheitsrnder wre mglich , wenn systematische fehler , die whrend der planungscomputertomographie entstehen , eliminiert werden . schlsselwrter prostata igrt sicherheitsrnder lymphknotenbestrahlung goldmarker introduction elective pelvic lymph node ( pl ) irradiation of high - risk prostate cancer , although discussed controversially , is common practice in many institutions and has traditionally been performed as a sequential boost regimen in normal fractionation for both prostate and pl planning target volumes ( ptvs )  . 
thus , the rst plan including lymph node as well as prostate ptvs is typically registered to the bony anatomy whereas the following prostate boost ptv can be matched to the gold ducials residing in the prostate . with the advent of intensity - modulated radiotherapy ( imrt ) and the recognition that prostate cancer might benet from higher doses per fraction , simultaneous integrated boost concepts evolved and have proven feasible [ 14 ]  . these newer concepts , however , require all ptvs to be administered within a single plan , implying that registration of prostate and pelvic ptvs can no longer be carried out separately . 
therefore , ptv margins of pelvic ptvs need to be reassessed in order to compensate for mismatch resulting from relative movement of the prostate . the prostate has been shown to move substantially within the pelvis due to differences in bladder and rectum lling [ 5 , 6 ] and therefore moves independently from the pelvic bony anatomy to which the lymphatics are attached to [ 7 , 8 ]  . while the extent of intraand interfractional prostate movement has been studied extensively [ 6 , 911 ] , data on relative movement to the bony anatomy rather than to skin markers are scarce , and margin recommendations for pelvic target volumes vary heavily [ 1214 ]  . we have therefore reassessed prostate movement relative to bony structures in a set of 28 consecutive high - risk prostate cancer patients and established margins for pl target volumes using van herks margin formula [ 15 , 16 ]  . materials and methods patient preparation , contouring , and imrt planning gold marker ( gm ) implantation , planning ct ( 3 mm slice thickness ) , and planning mri were performed as previously described [ 17 ]  . 
if bladder lling was not sufcient , the ct scan was repeated after patients were given 500 ml to drink over a time period of 30 min addition , bladder volume was assessed using an ultrasound device ( bladderscan bvi 9400 , verathon , inc . ) , and a minimum bladder volume for treatment specied by the treating physician ( usually between 150 and 350 ml )  . 
the upper border was the distal common iliac artery , approximately at the l5 / s1 interspace . the lower border was the top of the symphysis pubis . inverse imrt planning was performed using raystation software v.4.7.2.5 ( raysearch laboratories , sweden )  . treatment plans have been generated using either vmat dual arc ( 91 segments each ) or 13 - eld step and shoot delivering 67.5 gy , 60 gy , and 50 gy in 25 fractions to the prostate , sv , and pl , respectively . relative movement prostatebony anatomy igrt was routinely carried out using two orthogonal kilovolt images , typically at 0 and 90 . 
contoured structures corresponding to the planning ct ( such as gms , organs at risk [ oars ] , and the bony anatomy ) were then projected onto these planes . 
this formula ensures a minimum dose to the pl ctvs of 95% for 90% of the patient population . ( cid : 2 ) 2 + ( cid : 2 ) 2 results relative prostate movement in all , 28 consecutive high - risk patients who had been irradiated from july 2015 to november 2016 at university hospital of salzburg were analyzed in terms of relative movement of the prostate in relation to the bony anatomy of the pelvis . in the 28 patients , a total of 684 fractions were analyzed . 
however , for larger elds and dynamic segments as used in our study we have derived a higher value of 5 mm . strahlenther onkol ( 2017 ) 193 : 750755 fig . 
a / p anterior / posterior , i / s inferior / superior , l / r left / right tematic component of the overall error , which might have been introduced in the planning ct . margins in order to obtain a ptv expansion margin for a given ctv , a number of factors need to be determined such as delineation errors , setup errors , and organ motion . 
with exception of the latter , these errors need to be determined by each department individually since they are dependent on machine accuracy , contouring accuracy , and treatment time . 
we have therefore set those errors to zero in order to obtain a margin which exclusively compensates for errors introduced as a result from mismatch of gms to the bony anatomy due to relative prostate motion . 
we would consider these margins sufcient in the majority of modern radiation therapy units , but encourage determining the residual errors individually . in addition , in order to quantify the inuence of large systematic errors on our margins , we have identied the three patients ( equivalent to about 10% of our patient population ) with the largest mean displacement vector , and recalculated margins excluding them in the analysis . 
however , since the prostate ptv receives a higher dose than the lymphatic ptvs , and because critical oars such as the rectum and bladder are in close vicinity to the prostate , it makes sense to optimize ptv margins for the prostate rather than for ( mostly elective ) pelvic ptvs . 
thus , we believe it is prudent to carry out igrt registration of a plan that contains both prostate and lymph node ptvs , based on gms rather than to the bony anatomy of the pelvis . others [ 12 , 21 , 22 ] have analyzed dose coverage of lymph node ptvs when image registration is performed by matching to the prostate using gmor cone beam ctbased igrt . 
however , arbitrary margins of 510 mm were used , and dose coverage of lymph node target volumes reported by simulating prostate offset value shifts in a small number of patients . 
 [ 22 ] concluded that coverage is sufcient ( < 0.25% coverage failure ) and note in their discussion that in an ideal setting , population based data should be used to calculate accurate ctv to ptv margins for the lymph nodes target volumes which is exactly what we did in the present study . we have revisited prostate movement relative to bony anatomy in a large number of 684 fractions in order to establish margins for pelvic ptv expansion which compensate for the resulting mismatch to bony anatomy when image registration is performed based on gms in the prostate . our results are in good concordance with published data showing that prostate variability is very small in l / r direction and is about the same dimension in i / s and a / p direction [ 5 , 8 , 23 ]  . 
this is a somewhat fortunate constellation since mediolateral ptv expansion , which contributes the most to small bowel dose , can be kept small . it has to be noted , however , that in our margin calculation contouring errors and geometrical setup errors ( such as exmap correction inaccuracies , couch translation inaccuracies , and leaf position inaccuracies ) were set to zero and need to be considered before adopting the here presented margins . 
however , we strongly advise to determine these errors individually in each department . as we have shown , systematic errors , as indicated by large offsets and small sd , are introduced during the planning ct . 
2 mean offset of individual patients ( 128 ) in the anterior / posterior ( a / p ) , inferior / superior ( i / s ) and left / right ( l / r ) directions ( the error bars indicate one sd ) i / s directions and remained the same in the l / r direction ( see discussion for implications of that nding )  . discussion in the primary external beam radiotherapy ( ebrt ) treatment of high - risk prostate cancer , the combination of hypofractionation to the prostate and normal fractionation to the pl is an attractive concept . 
thus , 9 / 9 / 2 mm in the a / p , i / s , and lateral directions is what we would consider minimum margins ; however , larger margins might be needed to compensate for errors such as residual setup error and delineation uncertainties and need to be determined individually in each institution . acknowledgements open access funding provided by paracelsus medical university . 
wolf declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
in patients with primary rt , worsening of facial nerve function occurred in 1.7% ( n = 1 )  . conclusion stereotactic rt of vestibular schwannoma provides good functional outcomes and high control rates . 
dependence of hearing preservation on time of follow - up and initial tumor stage has to be considered . keywords radiosurgery audiometry hearing loss dizziness vestibular function tests stereotaktische strahlentherapie von akustikusneurinomen hrerhalt , vestibularfunktion und lokale kontrolle nach primrer und salvage - strahlentherapie zusammenfassung zielsetzung prsentation von langzeitdaten zu funktionellen ergebnissen und tumorkontrolle nach stereotaktischer radiotherapie ( rt ) in einer kohorte von 107 patienten mit akustikusneurinom . patienten und methoden zwischen oktober 2002 und dezember 2013 wurden 107 patienten mit akustikusneurinom ( primr oder rezidiviert nach vorangegangener resektion ) mittels stereotaktischer rt behandelt ( entwestrahlenther onkol ( 2017 ) 193 : 200212 der fraktioniert oder als einzeitradiochirurgie )  . 
der hrerhalt wurde nur bei patienten mit vollstndigen audiometrischen befunden prund posttherapeutisch ermittelt . objektive vestibularisdiagnostik ( vestibularfunktionstest , vft ) war in einer patientensubgruppe verfgbar und wurde der patientenberichteten schwindelsymptomatik gegenbergestellt . ergebnisse nach einem mittleren follow - up von 46 , 3 monaten war die aktuarische lokale kontrolle im gesamtkollektiv 100 % nach 2 , 97 , 6 % nach 5 bzw . 
prdiktoren hierfr waren in der multivariaten analyse die zeit nach abschluss der rt ( odds ratio [ or ] 0 , 93 pro monat ; p = 0 , 021 ) und die prtherapeutische tumorgre ( koos - stadium iiia vs . iibiv ; or = 0 , 15 ; p = 0 , 031 )  . 
bei patienten mit primrer rt trat bei 1 , 7 % eine verschlechterung der fazialisfunktion auf ( n = 1 )  . schlussfolgerung die stereotaktische rt beim akustikusneurinom erreicht eine hohe lokale kontrolle und gute funktionelle ergebnisse . 
die abhngigkeit des hrerhalts von der dauer des follow - up und der initialen tumorausdehnung muss bercksichtigt werden . schlsselwrter radiochirurgie audiometrie hrverlust schwindel vestibularfunktionstests vestibular schwannoma is a histologically benign condition with a very low disease - specic mortality rate , but which continues to generate a considerable amount of morbidity in a signicant number of sufferers even with modern , stateof - the - art treatment concepts . 
this morbidity is accounted for to some extent by the effects of the lesion itself , which , by virtue of its space - occupying nature , causes damage to surrounding structures ; however , it may be exacerbated by the collateral damage caused by the therapeutic interventions used in its treatment . in principle , there are three different ways to manage vestibular schwannoma patients . 
with large tumors , surgery is advocated as the appropriate treatment strategy in most cases . in the past , surgery was the only treatment available and in the days before the advent of tomographic imaging , surgeons were often faced with large , life - threatening symptomatic tumors that could only be removed at a considerable risk to the patients life and with very little room to consider preservation of function [ 1 , 2 ]  . surgical techniques have been rened a lot since the early days of the pre - imaging era , which has led to improvements in functional outcome for procedures using the retrosigmoidal and translabyrinthine approaches in particular [ 36 ]  . 
today , microsurgery achieves very high rates of tumor control but continues to carry a substantial risk of functional deciencies , especially hearing loss and cranial nerve decits [ 7 ]  . with small tumors , the wait - and - scan strategy is an option . 
indeed , trials with long follow - up show noninferiority of hearing preservation for selected patients managed with a wait - and - scan strategy when compared to strategies employing different types of intervention [ 8 , 9 ]  . however , these results have to be interpreted with caution , as deterioration of hearing function also closely mirrors tumor growth [ 10 ] and interventions such as rt can effectively inhibit growth and reduce the need for further treatments [ 9 ]  . stereotactic rt has now become a widely used alternative for smaller tumors , which now account for the vast majority of lesions diagnosed [ 1113 ]  . 
published data generally show stereotactic rt to achieve very good tumor control comparable with that seen in surgical series , while at the same time having a rather favorable side effect prole . 
this is true both for older [ 1417 ] , as well as for more recent comparative trials [ 18 , 19 ]  . stereotactic rt can be delivered as radiosurgery in a single treatment session ( srs ) or fractionated over multiple treatment days ( fsrt )  . 
srs [ 2022 ] and fsrt [ 2325 ] both provide good tumor control and functional outcomes . while superiority of one technique over the other has not been clearly shown , some experts advocate srs while others prefer fsrt . in the context of high control rates achieved by either modality , functional outcomes , especially hearing loss , have become the main research interest . 
unfortunately , direct comparisons of the available treatment options in the context of randomized controlled trials for vestibular schwannoma are unavailable . in the present analysis , the authors report their experience using stereotactic rt for vestibular schwannoma , with a special emphasis on long - term diseaseand treatment - associated morbidity and focus on possible determinants for functional outcome . 
a koos i : small intracanalicular tumor . b koos ii : tumor protruding into the cerebellopontine angle ( cpa ) without contact to the brainstenote : koos ii tumors are further subdivided into koos iia ( extension into the cpa ( cid : 2 ) 10 mm ) and koos iib ( extension into the cpa > 10 mm )  . 
d koos iv : brainstem and cranial nerve displacement patients and methods patient characteristics a total of 107 patients with vestibular schwannoma were treated with rt between 2002 and 2013 . 
rt was the primary treatment modality in 65.4% ( n = 70 ) of patients , whereas in the remaining 34.6% ( n = 37 ) , rt was delivered after resection , mostly treating recurrent disease ( 86.5% ; n = 32 )  . rt was delivered as fsrt in 70.1% ( n = 75 ) and as srs in 29.9% ( n = 32 ) of cases . 
patients with larger tumors and aao classes c / d as well as reduced physical tness were treated 204 class table 2 aao - hns hearing classication system pure - tone thresholds ( cid : 2 ) 30 db and > 30 db , ( cid : 2 ) 50 db and > 50 db and any level speech discrimination ( % ) aao - hns american academy of otolaryngologyhead and neck surgery aaao - hns class a and b was classied as serviceable hearing with hypofractionated schedules . 
patients in the srs group underwent head xation by means of a stereotactic head ring or a thermoplastic mask systeall patients in the srs group received 13 gy ( prescribed to the 90% isodose line ) except for 1 patient , who received 12 gy because of a large tumor volume . 
following rigid fusion of the planning ct and mri , the gross tumor volume ( gtv ) was contoured in a thin - slice t1 contrast - enhanced sequence ( mprage ) , as well as a three - dimensional constructive interference in steady - state ( 3d - ciss ) sequence . 
the planning target volume was dened as the gtv expanded isotropically by 1 mm . in all patients , treatment was delivered using a novalis brainlab linear accelerator ( varian 600n ) with 6 mv photons . 
daily kv imaging ( exactrac , brainlab ) was used for setup verication and repositioning . follow - up started 6 weeks after the end of rt and continued at 6 - monthly intervals for the rst 23 years and at yearly intervals thereafter . 
both follow - up strahlenther onkol ( 2017 ) 193 : 200212 the vestibular and the audiological investigations were carried out at the department of otorhinolaryngology . hearing preservation was analyzed in a subset of patients who had undergone proper audiometric evaluation preand posttreatment ( standardized audiogram , speech discrimination ) and who showed no evidence of recurrent disease ( n = 62 )  . 
aao - hns class a and b was classied as serviceable hearing ( corresponding to gardnerrobertson class i and ii )  . the equivalent dose in 2 gy fractions ( eqd2 ) was calculated to compare different fraction sizes using an alpha / beta ratio of 3 . 
when evaluating the inuence of cochlear doses on preservation of serviceable hearing , any deviations in cochlear single doses were accounted for . vestibular function was assessed objectively using caloric testing , positioning , swivel chair testing , spinal motor testing , and coordination . 
all functional outcomes were evaluated in patients without recurrence of disease after rt . statistical analysis local control was calculated starting from the start of rt . the kaplanmeier method and log - rank test were used to analyze the inuence of qualitative characteristics on local control . 
fractionated stereotactic radiotherapy ( fsrt ) , d inuence of tumor size on local control , e example of long - term tumor control after linear accelerator - based fsrt 206 strahlenther onkol ( 2017 ) 193 : 200212 rt a ( cid : 2 ) er resec ( cid : 3 ) on post - rt total primary rt post - rt total table 3 comparison of aao - hns hearing class prior to rt and at last audiometric follow - up . 
left side of the table : cases with rt after resection ; right side : cases with primary rt ; dark grey : cases with serviceable hearing before rt ; light grey : cases with preserved serviceable hearing after rt . in the subgroup with rt after resection , only 4 patients presented with serviceable hearing ( aao - hns class a and b ) at the start of rt and only 1 patient retained serviceable hearing after rt . 
no statistical signicance was observed due to the low number of recurrences in this cohort . hearing preservation and tinnitus hearing preservation was analyzed in a subset of patients with proper audiometric evaluation ( standardized audiogram , speech discrimination ) pre - and posttreatment and without recurrent disease after rt ( n = 62 )  . 
however , all patients without or with only mild vestibular impairment did not report dizziness ( table 4 in the appendix )  . discussion this study found a very high rate of tumor control following fsrt and single - dose srs over the follow - up period . no signicant differences in tumor control were observed between the two techniques . 
while obviously not proving isoeffectiveness due to low patient numbers and the low number of recurrences ( n = 2 ) , this is also in line with results published by other groups [ 2935 ]  . the high local control rate in patients with recurrences following surgery conrms the effectiveness of stereotactic rt as a salvage treatment . 
looking at the two patients who had a recurrence in more detail , it is noteworthy that both of them were treated with conventionally fractionated rt without a boost to a total dose of 50.4 gy and had tumors at the high end of the size spectrum ( koos stage iii and iv )  . one may therefore hypothesize that dose escalation could have provided increased local control . concerning conventionally fractionated fsrt , a variety of single and total doses have been reported in the literature [ 24 , 3640 ]  . 
at the high end of the dose reported on a series of 172 patients range , combs et al . treated with a median fsrt dose of 57.6 gy prescribed to the isocenter . 
in contrast , champ et al . hypothesized that reduced - dose fsrt could provide equal local control but even more favorable functional outcomes . applying a total dose of only 46.8 gy , these authors reported a tumor control rate of 96% after a median followup of 35 months [ 36 ]  . 
eqd2 equivalent dose in 2 gy fractions in patients with rt after resection ( n = 25 ) , only 16% ( n = 4 ) had serviceable hearing prior to rt . 
serviceable hearing was only preserved in 1 patient ( 25% ) with rt after initial resection ( table 3 )  . overall , tinnitus disappeared in 20.0% of patients after rt ( 7 of 35 evaluable cases with tinnitus prior to rt )  . new - onset tinnitus was only observed in 1 of 30 evaluable patients without tinnitus prior to radiation . facial nerve toxicity in patients with primary rt , facial nerve toxicity was low and worsening of facial nerve function was only of 59 evaluable patients with observed in 1 patient : housebrackmann grade i , only 1 patient ( 1.7% ) deteriorated to housebrackmann grade iii . 
this patient had received srs to a dose of 13 gy . patient reported dizziness and objective vestibular function overall , patient reported dizziness was 65.3% prior to rt ( 49 of 75 evaluable cases )  . 
further worsening of objective vestibular function was observed in only 3 ( 17.6% ) patients at risk of further vestibular deterioration . 208 strahlenther onkol ( 2017 ) 193 : 200212 interestingly , despite high local control rates even with reduced - dose fsrt , increased doses seem to be associated with even further improved local control . 
the authors therefore advise against reduced - dose fsrt at the present time and their current institutional practice is to treat patients with vestibular schwannoma up to a total dose of 54 gy ( 40.8% of patients treated with fsrt in the current analysis )  . given that the observed rates of tumor control are very high and of the same order of magnitude as those reported in large surgical series , comparisons between stereotactic rt and modern surgical approaches need to place a proportionately greater weight on differences in treatment - associated morbidity . in the current analysis , a subset of 62 patients with proper audiometric evaluation ( standardized audiogram , speech discrimination ) pre - and posttreatment was identied . 
the nding that serviceable hearing could be preserved in 72% of patients over the time of follow - up compares favorably with data from surgical series , which tend to report lower rates of hearing preservation . 
these authors estimated the rate of hearing preservation at 5 years to be within the range of 24 to 46% [ 45 ]  . the present study found pretreatment tumor size to be an important determinant for hearing preservation . 
of note , patients with primary surgery also had signicantly larger tumors in the present cohort . the rate of hearing preservation observed in the current cohort was lower than that published by combs et al . , who performed a retrospective analysis on pooled data from patients with vestibular schwannoma treated with stereotactic rt at three large centers in germany [ 29 ]  . 
 ( gardnerrobertson class i and ii ) is identical to aao - hns class a and b ( used in the present study )  . in addition , the current report analyzed hearing preservation over time following rt . 
made similar observations : in their set of patients , the proportion of patients with serviceable hearing declined from 80% at 1 year posttreatment to as low as 23% at 10 years [ 46 ]  . 
in addition to time of follow - up after rt , pretreatment tumor size was a signicant and independent predictor for preservation of serviceable hearing in the present analysis . however , interestingly , cochlear dose was not associated with preservation of serviceable hearing in the present cohort . 
many srs series point to decreased hearing preservation with increasing cochlea doses [ 4754 ] , as do some series reporting on fsrt [ 43 , 55 ]  . in contrast , others have failed to show an independent contribution of cochlear doses on preservation of serviceable hearing [ 39 , 46 , 5658 ]  . 
the differing results could be partly explained by interobserver variations in identication of the cochlea and cochlear substructures [ 57 ] , varying denitions for serviceable hearing , different measurements for cochlear dose , or perhaps by differential effects of cochlear doses in srs and fsrt . in an interesting analysis published by kim et al . 2011 , the authors reported on a series of 60 patients treated with srs . 
in this cohort , transient expansion in tumor volume after rt was an independent risk factor for loss of serviceable hearing , whereas cochlear dose failed to reach signicance in multivariate analysis [ 58 ]  . 
little strahlenther onkol ( 2017 ) 193 : 200212 concordance between patient - reported dizziness and objective vestibular function was observed , which may at least in part be attributed to compensation by the contralateral side . importantly , however , no patient with intact vestibular function reported dizziness . 
as patient - reported dizziness is confounded by contralateral compensation , the authors suggest giving greater emphasis to objective vestibular function tests in future investigations . conclusion stereotactic rt for vestibular schwannoma is a safe and highly effective treatment strategy . importantly , equally high control rates for salvage rt in cases of tumor recurrence following primary surgery were found . 
rather than addressing the potential superiority of one treatment approach over another in the setting of retrospective series that are difcult to compare , it may be more benecial to focus on optimal patient selection for available treatment options in future studies . 
lettmaier declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
informed consent was obtained from all individual participants included in the study . strahlenther onkol ( 2017 ) 193 : 200212 appendix objective vestibular function table 4 patient - reported dizziness after radiotherapy ( rt ) in relation to objective vestibular function patient reported dizziness after rt no dizziness ( n ) no vestibular dysfunction mild vestibular impairment chronic vestibular dysfunction complete unilateral loss of function 6.9% ( 2 ) 3.4% ( 1 ) 48.3% ( 14 ) 41.4% ( 12 ) dizziness ( n ) 0% ( 0 ) 0% ( 0 ) 56.3% ( 9 ) 43.8% ( 7 ) fig . 
5 box plot showing the distribution of minimum ( a ) and maximum ( b ) cochlear doses in patients without ( left ) and with preserved serviceable hearing ( right )  . 
avms are treated by surgery , embolization , or radiation therapy . objective this study investigated obliteration rates and side effects in patients with avms treated by radiation therapy . methods a total of 40 cases treated between 2005 and 2013 were analyzed . 
in 20 patients , endovascular embolization had been performed prior to irradiation and 24 patients ( 60 % ) had a history of previous intracranial hemorrhage . results treatment resulted in complete obliteration ( co ) in 23 / 40 cases and partial obliteration in 8 / 40 . 
consistent with the literature , this data analysis suggests that the results of hsrt are volume - dependent . furthermore , regimens with eqd2 doses > 70 gy appear more likely to achieve obliteration than schemes with lower doses . 
prior embolization may have a good prognostic impact . keywords radiosurgery hemorrhage adverse effects angiography magnetic resonance imaging prdiktoren fr den verschluss zerebraler arteriovenser malformationen nach strahlentherapie strahlendosis und vorangegangene embolisation , nicht jedoch der spetzler - martin - grad zusammenfassung hintergrund intrakranielle arteriovense malformationen ( avm ) knnen einen komplikationsbehafteten verlauf zeigen . 
avms sind mittels operation , embolisation oder strahlentherapie behandelbar . zielsetzung die studie untersucht obliterationsraten und nebenwirkungen bestrahlter avm - patienten . methoden analysiert wurden 40 flle , die zwischen 2005 und 2013 behandelt wurden . 
vor der strahlentherapie hatten 60 % der patienten bereits eine intrakranielle blutung . ergebnisse in 23 / 40 fllen wurde eine komplette ( co ) und in 8 / 40 eine partielle obliteration erreicht . 
eine vorherige embolisation hat mglicherweise einen positiven effekt . schlsselwrter radiochirurgie blutung nebenwirkungen angiographie magnetresonanzbildgebung cerebral arteriovenous malformations ( avms ) are focal conglomerations of dilated arteries and veins in the brain that are directly connected without an intervening capillary bed . 
the bleeding risk is estimated at 12 % per year in general [ 1 , 2 ] , and is as high as 30 % per year in patients with a history of ich [ 3 , 4 ]  . in addition to neurosurgical and neuroradiological treatments , linear accelerator or cyberknife - based ( accuray , sunnyvale , ca , usa ) stereotactic radiosurgery ( srs ) is an established modality for treatment of intracranial avm . srs is often possible in cases where surgical resection is unfeasible due to a high risk of mortality [ 5 , 6 ]  . 
obliteration rates for avms with volumes smaller than 2 cm are higher than 80 % , while those for avms with volumes larger than 2 cm drop off sharply according to the literature , to between 53 and 17 % after 3 years [ 9 ]  . 
moreover , normal brain tissue surrounding avms shows radiation - induced changes following distinct dosevolume relationships , allowing assessment of the risk of edema or brain - barrier breakdown upfront of srs [ 10 ]  . through the use of modern technology , stereotactic irradiation treatments for cerebral avms are associated with a low rate of adverse effects [ 11 ]  . the present study analyzed retrospectively collected data on obliteration rates conrmed by digital subtracted angiography ( dsa ) or mri , radiation doses delivered , and avm volumes treated at the department of radiation oncology of erlangen university hospital ( uk - er )  . 
the question of which dose regimen is most optimal for the treatment of large cerebral avms was explored . methods patient characteristics a total of 40 patients ( 16 men , 24 women ; mean age 40.5 years , range 1667 years ) with avms of the brain were treated at the uk - er department of radiation oncology from 2005 to 2013 . 
at baseline , 8 brain avms were classied as grade 1 , 16 as grade 2 , 13 as grade 3 , and 3 as grade 4 according to the spetzlermartin grading scale ; none of the patients had grade 5 . a history of intracranial hemorrhage prior to treatment was recorded for 24 patients ( 60 % )  . 
in 20 patients , endovascular embolization had been performed prior to stereotactic radiation therapy ( using onyx , medtronic , dublin , ireland , in 14 / 20 patients ; unknown n = 3 ; other agents n = 3 ) and one of these patients had trimodality treatment consisting of partial resection , embolization , and irradiation . 
treatment recommendations were made in weekly multidisciplinary in - house team discussions . radiation treatment treatment planning consisted of a digital subtraction angiogram ( dsa ) , a planning computed tomography ( ct ) scan , and a magnetic resonance imaging ( mri ) angiography scan with a standard in - house protocol containing arterial time - of - ight ( tof ) sequences in each case . 
the dsa , planning ct scan ( 12 mm slice thickness ) , and radiation treatment were accomplished using a stereotactic xation system ( brainlab , feldkirchen , germany )  . 
complete obliteration of the nidus after ich was ultimately shown in 2 patients and 3 of the 4 patients developed no further side effects after their ich ; the patients were treated only by medication . 
dose was prescribed to target volume surrounding the 90 % isodose . follow - up all patients initially received semiannual and subsequently annual neuroimaging follow - up consisting of an mri scan ; dsa was additionally performed to conrm complete occlusion . 
to assess the inuence of radiation dose on obliteration rate , radiation doses were converted to 2 gy equivalent dose fractions ( eqd2 ) , assuming an / ratio of 3 . 
single - dose srs is generally used to treat brain avms discussion smaller than 2 to 5 cm , while a variety of different approaches are used for larger malformations . 
obliteration rates achieved by single - dose srs of small brain avms range from 60 % to more than 80 % , depending on the size of the malformation [ 1215 ]  . 
radiation doses administered in single - dose srs currently fall within the range of 18 to 22 gy [ 11 , 16 , 17 ]  . hsrt dose regimens vary between different institutions as well as within a single institution . 
in the present sample , hsrt achieved an overall obliteration rate of 44 % . these retrospective volume and dose analyses showed at least initial indications that obliteration may be volumeand dose - dependent : an obliteration rate of 50 % was achieved in patients with avm volumes < 12 cm compared to only 16 % in patients with larger avconversion of the irradiated dose to eqd2 also showed an obliteration rate of 50 % at doses > 70 gy compared to only 25 % at doses < 70 gy . 
found a 7 - fold greater likelihood of obliteration in a cohort of patients treated with 7 gy fractions than in those treated with 5 gy fractions [ 17 , 20 ]  . 
a fractionated 35 gy schedule did show a signicantly shorter time until obliteration than a treatment with 3032.5 gy , but also a signicantly higher rate of radionecrosis [ 22 ]  . because higher doses are needed to achieve favorable obliteration rates , some institutions did introduce a staged radiosurgery approach as an alternative to hsrt . 
treated 47 patients with a median avm volume of 22 cm using two - step srs and achieved obliteration rates of 9 % after 3 years and 32 % after 5 years . 
no cyst formation was seen during follow - up , and a higher margin strahlenther onkol ( 2017 ) 193 : 185191 dose was a signicant factor for obliteration [ 23 ]  . 
the need for smaller volumes and higher doses when using staged srs was also reported by seymour et al : a good response could be achieved after 5 years in 68 % and a dose 17 gy was a strong predictor of response [ 24 ]  . the latency period from treatment until the onset of complete obliteration was independent of the radiation dose or the kind of radiation therapy ( single - dose versus hypofractionated rt ) in the current analysis . 
found a difference between the latency periods from single - dose and hypofractionated srs until complete obliteration in a series of 48 patients ( 15 hsrt ) , with a median 46.5 months after hypofractionated compared to a median 29.2 months after single - dose radiation therapy . 
in some studies , the group treated with a combined approach showed a higher percentage of patients with spetzlermartin grades iii and iv [ 26 , 28 ] , and schwyzer et al . 
found lower obliteration rates in an embolized cohort compared to nonembolized patients ; however , in contrast to angioarchitectural complexity , embolization was no longer a signicant factor after multivariate analysis . 
other authors found combining embolization and radiation therapy to be effective in treating avms [ 30 ]  . embolization may not only reduce the volume of the avm but also the vascular density , and good response rates after hsrt were reported [ 31 ]  . 
in a recent report , nataraj et al . found 67 % of patients treated by srs only to be cured , compared to 70 % of those treated by embolization and srs [ 32 ]  . 
recent reports using onyx embolization and interestingly , in srs found promising results [ 33 , 34 ]  . none of the studies investigating this bimodality treatment could a higher rate of side effects be found when combining embolization and radiation therapy . 
according to the literature , using onyx prior to radiation therapy seems to be safe , and according to the present analysis , it also seems to be effective without adding toxicity . 
it can be used for decreasing the volume of the nidus , although attention has to be paid to target volume denition afterwards , because of the changes in radiologic imaging or fragmentation of the nidus . ich is a complication that may occur during the course of avm treatment ; another complication is epileptic seizures . 
while a recent randomized study showed a negative prognostic impact of treating unbled avms during a 33 - month follow - up period , other data show excess mortality in untreated patients after more than 10 years and the lowest rate in patients with totally occluded avms [ 2 , 35 ]  . in the present study , bleeding after radiation treatment occurred in 4 patients ( 10 % )  . 
at least one bleeding event prior to radiation therapy had been suffered by 60 % of the patients , corresponding to a rate of 16 % in this subgroup . other investigators estimate that up to 30 % of patients with a history of hemorrhage can be expected to incur subsequent bleeding during the rst year [ 4 ]  . 
did not observe a single ich in 155 patients with subtotally obliterated avms [ 36 ] and karlson et al . found that the observed number of ichs during the latency period until avm obliteration was signicantly lower than expected [ 37 ]  . radionecrosis is reported to occur in 0 to 7 % of radiosurgically treated cerebral avm cases in the literature [ 11 , 13 , 15 ]  . 
all patients who developed epileptic seizures after radiation therapy had a history of seizures prior to treatment . conclusion srs achieves excellent rates of control of small - volume avms , whereas the treatment of large avms remains a challenge . 
the clear advantage of radiation therapy is the possibility of its application in regions where surgery and embolization may be harminterestingly , preceding ful , such as the basal ganglia . embolization with onyx may have a good prognostic impact on the obliteration rates of irradiated avfurther validation in a randomized study is needed . 190 strahlenther onkol ( 2017 ) 193 : 185191 compliance with ethical guidelines conict of interest s . 
fietkau declare that they have no competing interests . ethical standards all procedures performed were in accordance with the ethical standards of the institutional research committee and with the 1964 helsinki declaration and its later amendments . 
dietzel1 christoph schfer2 dirk vordermark1 received : 18 april 2016 / accepted : 6 october 2016 / published online : 7 november 2016 springer - verlag berlin heidelberg 2016 abstract background chronic recurrent multifocal osteomyelitis ( crmo ) is a rare autoinammatory disease , which lacks an infectious genesis and predominantly involves the metaphysis of long bones . 
common treatments range from nonsteroidal anti - inammatory drugs ( nsaids ) and corticosteroids at rst onset of disease , to immunosuppressive drugs and bisphosphonates in cases of insufcient remission . 
the therapeutic use of low - dose radiotherapy for crmo constitutes a novelty . case report a 67 - year - old female patient presented with radiologically proven crmo affecting the right tibia / talus and no response to immunosuppressive therapy . 
ten months later , pain and symptoms of osteomyelitis had completely vanished . conclusion radiotherapy seems to be an efcient and feasible complementary treatment option for conventional treatment refractory crmo in adulthood . 
the application of low doses per fraction is justied by the inammatory pathomechanism of disease . keywords osteomyelitis pain autoimmune diseases inammatory diseases cytokines crmo radiotherapy ( cid : 2 ) christian t . 
40 , 06120 halle ( saale ) , germany erfolgreiche behandlung der chronisch rekurrierenden multifokalen osteomyelitis mit niedrigdosierter radiotherapie ein fallbericht zusammenfassung hintergrund die chronisch rekurrierende multifokale osteomyelitis ( crmo ) ist eine seltene autoimmunologische erkrankung und befllt vorzugsweise die metaphysen der langen rhrenknochen . 
die anwendung einer niedrigdosierten radiatio stellt ein therapeutisches novum dar . fallbericht eine 67 - jhrige patientin stellte sich mit einem radiologisch gesicherten befall im sinne einer crmo im bereich des rechten talus und der tibia vor . 
die schmerzhaften beschwerden der osteomyelitis waren 10 monate nach behandlungsende vollstndig regredient . schlussfolgerung die strahlentherapie scheint eine efziente und praktikable ergnzung zur behandlung der initial therapierefraktren crmo im erwachsenenalter zu sein . aufgrund der autoimmunologischen genese der erkrankung knnen bereits niedrige einzeldosen zu einer wirksamen linderung fhren . schlsselwrter osteomyelitis schmerzen autoimmunerkrankungen entzndungserkrankungen zytokine crmo strahlentherapie 230 strahlenther onkol ( 2017 ) 193 : 229233 patient a 67 - year - old female patient with a history of chronic pain in both ankle joints was sent to the authors department in september 2014 . 
a dactylitis , which is specic chronic recurrent multifocal osteomyelitis ( crmo ) is a rare autoinammatory disease that mainly affects the metaphysis of long bones [ 1 ]  . 
one key feature of cnos is duration of symptoms for more than 6 months [ 5 ]  . specic scores and diagnostic criteria have been established to differentiate more precisely between infectious and non - bacterial osteomyelitides before initiating a treatment ( table 1 ; [ 6 , 7 ] )  . the exact pathomechanism of crmo is still open to discussion . 
sterile bone biopsy with signs of inammation and / or brosis , sclerosis normal blood count / good general state of health c - reactive protein and erythrocyte sedimentation rate mildly / moderately elevated observation time > 6 months hyperostosis associated with other autoimmune diseases grade i or ii relatives with autoimmune / inammatory diseases or non - bacterial osteomyelitis / osteitis strahlenther onkol ( 2017 ) 193 : 229233 fig . 
2 t2 - weighted mri scan ( short tau inversion recovery , stir , sequence ) of the right ankle joint showing bone marrow oedema in the distal tibia and the talus fig . 
the lack of articular involvement and only small effusion in the intra - articular space were arguments against the presence of synovitis . at initial presentation , a pain level of 7 ( during stress and resting ) was measured using a visual analogue scale ( vas ) ranging from 010 . laboratory examinations showed only moderately elevated c - reactive protein ( range between 4.724.3 mg / dl , standard < 5 mg / dl ) during the last 3 months . regarding the classication of jansson et al . 
for cno , three major criteria ( radiologically proven bone lesion , multifocal occurrence and psoriasis ) and at least three minor criteria could be established in order to justify the diagnosis of crmo ( table 1 )  . 
the diagnosis was conrmed by the experts of the local department of rheumatology prior to initiation of treatment . since both an escalated immunosuppressive therapy and the use of opioid - based drugs did not result in sufcient pain control , a low - dose radiotherapy regimen was initiated in order to modulate the excessive autoinammatory reaction in the affected bones . 
written informed consent was obtained from the patient prior to treatment . treatment a planning ct scan was acquired in the treatment position using a vacuum mattress to immobilize the right leg . 
each series contained six fractions ( three fractions per week ) with single doses of 0.5 gy , thus the total applied dose was 6 gy . outcome as described above , the patient initially presented with pain rating 7 on a vas , both in a resting position and under stress . 
on the other hand , there was also no transient worsening of pain , which is a common acute adverse effect of x - ray stimulation therapy of other benign bone pathologies [ 15 , 16 ]  . on the last day of the second treatment series there was a noticeable relief of symptoms , with a pain level of vas 45 while walking and vas 4 while resting . the patient underwent another check - up 6 weeks after completion of the second treatment series . 
during this period , the positive trend towards an improvement continued . at the time of reexamination there was no determinable resting pain in the affected extremity ( vas 0 )  . 
though movement of the right foot was still painful ( vas 4 ) , the 232 strahlenther onkol ( 2017 ) 193 : 229233 mobility range and , consequently , the stability of the right ankle had improved in the patients subjective evaluation . another follow - up 5 months after radiotherapy demonstrated stable long - term pain control . 
upon presentation at the rheumatology outpatient department 10 months after treatment , pain and symptoms of osteomyelitis had completely vanished . it is important to mention that our local outpatient pain department did not intensify the pain medication during or after the end of radiotherapy , and treatment with immunosuppressive drugs remained stable . 
recent case studies have underlined that the preferable imaging modality for early detection of disease could be whole - body mri , which seems to be superior to conventional radiography or tc99m - methyl diphosphonate ( tc - 99m - mdp ) scintigraphy [ 17 , 18 ]  . 
in this context , biopsies should only be performed in cases of unifocal bone involvement and / or if clinical ndings suggest an infectious / malignant disease origin [ 19 ]  . 
a wide diversity of second - line treatments , the lack of controlled and randomized trials , and varying long - term remission rates between 22 and 48 % reect the need for further therapeutic approaches [ 12 ]  . 
its effectiveness has been shown in a variety of studies for a wide range of indications [ 15 , 2124 ]  . the german society for radiation oncology ( degro ) has released a series of practical guidelines offering consensus recommendations for radiotherapy of nonmalignant diseases [ 2528 ]  . although appropriate treatment regimens with single doses of 0.51 gy have been well known for decades , the underlying radiobiological mechanisms have just recently been revealed . 
this lowers the overall count of to the best of the authors knowledge , this is the rst report on the use of radiotherapy as an efcient and feasible complementary treatment for crmo . 
vordermark declare that they have no competing interests . all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the majority of complications scored as toxicity grade 5 , namely respiratory failure and fatal hemoptysis , are most likely related to multiple competing risks and occurred at different dose fractionation schemas , e . 
furthermore , satisfactory documentation of complications and details of dosimetric parameters , as well as limitation of the wide range of possible fractionation schemes is also warranted for a better understanding of the risk factors relevant for macroscopic damage to the serially organized anatomic structure within the central chest . keywords lung cancer heart hemoptysis organs at risk risk factors spezische toxizitt nach stereotaktischer strahlentherapie des zentralen brustkorbs eine umfangreiche literaturbersicht zusammenfassung das risiko fr schwere nebenwirkungen der stereotaktischen strahlentherapie bei zentralen lungentumoren ist bisher schlecht deniert . 
1012 fraktionen mit 45 gy , 5 fraktionen mit 10 gy , 3 fraktionen mit 2022 gy und 1 fraktion mit 1530 gy zuordnen , da multiple patientenspezische , konkurrierende risiken dabei einen wesentlichen einuss zu haben scheinen . 
3 , 73035 goeppingen , germany table 1 key process involved in an interpretive literature search processes involved in review strahlenther onkol ( 2017 ) 193 : 173184 formulation of an initial review question does sbrt have a specic late toxicity on the serially arranged organs within the central chest ? searching for literature to be included electronic literature search using pubmed database and the cochrane central register of controlled trials . 
the ability of endpoints in one study to be translated into endpoints from other studies is grounded , obviously , in the attributes , structures , granularity , and the scope of use of clinical terminologies themselves , as well as the endpoints that are most adequately specied . refutational translation consisted of characterization of contradictions and discrepancies between studies reports and aws in evidence and attempts to explain them secondary translation ( not always possible ) when translations can encompass those of other accounts by constant and iterative comparisons between individual accounts , attempts were made to excavate sediment endpoints that are most powerful in representing the whole literature body , and thus to excavate the corresponding clinicopathologic correlations that are deeply fossilized in the ndings of the separate studies . writing the review communication of the nding from the interpretive approach in a form appropriate to audience ( review article )  . the results show that the effect of multiple dose fractions , even a very small one , is in no respect different , in terms of macroscopic ( skin ) damages , from that of a single dose reisner , skin erythema and roentgen therapy , 1933 there is little doubt that stereotactic body radiation therapy ( sbrt ) is safe for the treatment of peripheral lung lesions and it is used routinely . 
during the past decades , the central chest has been widely acknowledged as a no - y zone for sbrt , even in the national comprehensive cancer network ( nccn ) guidelines for the treatment of nonsmall cell lung cancer ( nsclc ) in 2010 and 2011 . nevertheless , the radiation therapy oncology group ( rtog ) dose - escalation phase i study for centrally located lung cancer ( rtog 0813 ; [ 1 ] ) has recently published its primary endpoint analysis . 
expressing the synthesis introduction strahlenther onkol ( 2017 ) 193 : 173184 electronic literature search in pubmed database and the cochrane central register of controlled trials : manual literature search in textbooks : 2 reference chaining : 108 records a ( cid : 2 ) er duplica ( cid : 3 ) ons , abstracts and non - english texts removed 108 records screened 68 of full - text ar ( cid : 3 ) cles assessed for eligibility 41 studies with 1642 pa ( cid : 3 ) ents included in the qualita ( cid : 3 ) ve synthesis , so individual pa ( cid : 3 ) ent data from 115 cases were extracted fig . 
in the german metacentric analysis [ 2 ] , one of 90 patients with central lung cancer died from pneumonitis g5 without evidence of bronchial stenosis or bleeding . indeed , reviews including comprehensive data concerning sbrt - specic morbidity and mortality when treating central lung tumors are sparse [ 3 ]  . 
the aim of this paper is to provide a discursive prose , rather than a data summerizing review on the specic toxicity of sbrt to anatomic structures within the central chest . methods the initial literature search was also based on studies iden [ 3 ] , and extended to a wide range tied by kang et al . of literature offered by citation analysis and manual as well as electronic reference chaining . 
lung tumors located within 2 cm around the proximal tracheobronchial tree , or at a maximum distance of 1 cm from the heart and pericardium , and the esophagus were considered as central . 
the key process involved in this review is illustrated in table 1 . results literature search the search strategy identied 68 studies including 2457 patients treated with sbrt for central lesions . 
after repeated re - reading of each individual paper , 20 ( 30 % ) studies with 608 ( 25 % ) patients and 7 ( 10 % ) studies with 207 ( 8 % ) patients reporting ex negativo no specic and no long - term toxicity , respectively , were excluded . 
overall , specic late toxicity occurred with a median total dose of 50 gy ( range 4054 gy ) and a median biologically effective dose with / = 3 gy ( bed3 ) of 216 gy3 ( 210277 gy3 ) in the hottest / shortest regimes compared with a median total dose of 45 gy ( range 3050 gy ) and a median bed3 of 176 gy3 ( 90237 gy3 ) in the coldest / longest regimes . 
a summary of toxicity data is shown in table 2 . cardiac toxicity the beating heart can neither be categorized as a parallel nor as a serially arranged organ at risk ( oar )  . 
compensation of heart motion seems to be impossible as yet , and the true maximal dose tolerated by the heart or its partial volume remains unknown , even in the conventional setting . in a recently published study on 39 lung tumors that were close to the heart , increased cardiac uptake of 18urodeoxyglucose ( 18 - fdg ) was observed in positronemission tomography ( pet ) in 9 patients in whom more than 5 cc of the heart was covered by the 20 gy isodose line , but without meaningful correlation between this observation and cardiac toxicity [ 4 ]  . 
without describing the perfusionmetabolism patterns ( normal , subendocardial match , transmural match , and mismatch ) , pet alone 176 strahlenther onkol ( 2017 ) 193 : 173184 table 2 summary of toxicity data no . 
this may be related to signicant improvements in treatment planning techniques or to the use of less ablative doses than those applied by indiana university or even to the reluctance of radiation oncologists to treat central tumors that are adjacent to the beating heart . 
after a median follow - up of 6.3 months ( range 329 months ) , bonomo and colleges from florence university [ 14 ] , who in the aforementioned phase ii study [ 8 ] , one patient died from complications of pericardial effusion without further information . respiratory failure fakiris et al . 
either the signs of cardiac tamponade resulting from delayed chronic pericardial effusion had been interpreted as respiratory failure because dyspnea is the most common presenting symptom , or this respiratory failure was possibly related to the preexisting pulmonary dysfunction strahlenther onkol ( 2017 ) 193 : 173184 table 3 studies reporting cardiac toxicity study ( year ) timmerman ( 2003 ) [ 5 ] mcgarry ( 2005 ) [ 6 ] no . 
the immediate cause of respiratory failure remains unclear . indeed , respiratory failure is a general and ill - specied endpoint , and reects a nal condition resulting in death , regardless of the underlying cause initiating the events leading to death . 
this reects the fact that the authors were unsure of the immediate cause of death , or unable to accurately ascertain the underlying or contributing causes of death . bronchial stenosis and atelectasis the pathophysiological mechanisms underlying radiationinduced bronchial stenosis and subsequent collapse of the lung tissue remain poorly understood . 
radiation injury to the bronchi might begin simply with erythema , edema in the mucosa , and transmural inammatory inltration that manifests in some degree of wall thickening of major airways without clinical evidence of airow restriction [ 20 ]  . at this stage , some radiological signs may begin to appear , including discrete hypoventilation of downstream lung tissue without changing tissue density or signs of atelectasis [ 21 ]  . over time , multiple supercial ulcers may become apparent . 
while ulceration may result in necrosis and stula formation in the main / lobar bronchi [ 16 , 17 ] , the progression of brosis may ultimately narrow the segmental airways , resulting in the collapse of downstream lung tissue [ 22 ]  . tumor necrosis and the sloughing off of endobronchial mucosa after sbrt may also obstruct the airway lumen . this remains a potential problem even for endoscopic treatments , which are considered to be the safest intervention modality . 
in addition , increased production of mucus has been observed after reirradiation with sbrt [ 23 ]  . 178 strahlenther onkol ( 2017 ) 193 : 173184 table 4 studies utilizing respiratory failure as safety endpoint study ( year ) no . 
the alveoli surrounding the lesions might be compressed by parenchyma brosis , tumor progression , or bacterial infection , resulting in cicatrization atelectasis . thus , the collapse of lung tissue might not necessarily result from upstream airway stenosis . eleven cases of bronchial stenosis without secondary atelectasis and ve cases of stenosis with secondary atelectasis were identied . 
by contrast , 28 cases of atelectasis without documented upstream bronchial stenosis were found ( table 5 )  . the most important attempt to estimate the doseresponse relationship for atelectasis comes from the karolinska university experience reported by karlsson et al . 
furthermore , the authors did not distinguish patients who developed bronchial stenosis with secondary atelectasis from those with bronchial stenosis without atelectasis , or from those with atelectasis but without bronchial stenosis . the study was also biased by bad resolution for the delineation of oar , which resulted from a ct slice thickness of 1 cm and 0.5 cm before and after 1996 , respectively . on such slices , subvolumes of the bronchial tree might not be visible and hotspots on the circumferential bronchial discs might be overlooked . 
by contrast , in a previously unpublished student thesis on the same cohort of patients , karlsson [ 35 ] showed a doseresponse relationship only for right - sided lung tumors . while reporting of atelectasis is more frequent , high rates of bronchial stenosis have been reported in only one study [ 26 ]  . 
of 9 patients , 3 of 6 patients who had tumors adjacent to the main / lobar bronchus and 2 of 3 patients with tumors adjacent to the segmental bronchus experienced partial bronchial stenosis , and 3 of the former 6 patients had complete stenosis . 
 [ 29 ] reported on a case of fatal hemoptysis after stent placement for grade 3 bronchial strahlenther onkol ( 2017 ) 193 : 173184 table 5 studies reporting atelectasis with or without bronchial stenosis and vice versa study ( year ) no . 
from these observations , an erroneous concern over the safety of stenting previously irradiated airways was also drawn [ 29 ]  . however , bleeding as an iatrogenic complication after stent implantation in nonirradiated airways is not rare . 
it remains unclear whether radiation therapy may increase the risk of iatrogenic bronchovascular stula formation after stent implantation and also the risk of fatal hemoptysis . 180 fatal hemoptysis fatal hemoptysis is one of the most serious reported complications after sbrt and was reported in 16 studies ( table 6 )  . the clinical and pathological mechanism of fatal pulmonary hemorrhage in patients with lung cancer is poorly understood . 
g. , aortobronchial stula , seems to be the most plausible mechanism to explain the occurrence of hemoptysis of necrotizing tumors , local recurrence , necrotizing pneumonia , and of radiation induced - necrosis or of antineoplastic agents with a cavitation response . fatal hemoptysis is also commonly related to the highpressure bronchial arterial system and rarely to the lowpressure pulmonary arterial systethus , the volume of the pulmonary artery exposed to high - dose radiation therapy might not be adequate at all for dosimetric analysis of radiation - related hemoptysis . 
 [ 36 ] , the widely believed dogma that fatal hemoptysis might result from high - dose radiation - induced damage to the pulmonary artery could not be conrmed , and only 2 of 100 patients with lung tumors adjacent to or invading the pulmonary artery experienced massive hemoptysis . 
in three sbrt studies , attempts were made to correlate the dose to the pulmonary artery with the occurrence of fatal hemoptysis . in two studies [ 23 , 37 ] , no correlation was found and the patient in the third study [ 38 ] was excluded from the nal analysis [ 12 ]  . in a chemoradiation setting , the presence of baseline major tumor cavitation and squamous cell histology [ 39 ] , and central location and local recurrence and squamous cell histology [ 40 ] were associated with a high risk for hemoptysis . the highest incidence of fatal hemoptysis was reported in a brachytherapy setting , although the discussion on postprocedural complications here remains controversial . a consensus report from a panel of experts addressing the problem of fatal hemoptysis in patients with lung cancer treated with bevacizumab demonstrated squamous cell histology and pretreatment sentinel bleeding to be prior risk factors , but not cavitation , tumor location , and invasion into blood vessels [ 41 ]  . 
however , the panel of experts was confused by lacking standardized radiological criteria for assessing the centrality , vascular invasion , and grade in an sbrt study on tumors abutting the of cavitation . tracheobronchial tree , 2 of 4 patients died of pulmonary hemorrhage after receiving anti - vascular endothelial growth factor ( vegf ; [ 42 ] )  . nonetheless , squamous cell carcinomas of the lung are usually centrally located , are more likely to invade the large blood vessels , and have a high tendency to cavitate ; thus strahlenther onkol ( 2017 ) 193 : 173184 representing all of the abovementioned independent risk factors for fatal hemoptysis . bronchial necrosis and stula formation however , there is only one report with direct endoscopic evidence of the source of fatal bleeding from radiationinduced bronchial necrosis [ 49 ]  . 
e. , fatal hemoptysis [ 49 ] , atelectasis [ 16 ] , and bronchial stula formation [ 17 ] after treating lung cancer , metastatic malignant melanoma , and malignant mesothelioma , respectively . 
additionally , the indiana university group reported one case of bronchitis and one case of tracheal necrosis in their series with doses of 3 fractions of 20 gy and 3 fractions of 24 gy , respectively ( no information about location is available [ 5 ] )  . there may be other competing risks that interfere with the course of necrosis . 
in the same series , another patient with a central lesion died of lung embolisms and radiation recall pneumonitis after receiving gemcitabine , and all g2g5 - scored toxicity for central lesions was associated with chemotherapy . in an aforementioned study [ 40 ] , gemcitabine was linked to the development of fatal hemoptysis in patients with lung cancer . tracheoesophageal stula formation was also seen only in patients who received anti - vegf [ 50 ]  . esophagitis and esophageal ulceration clinically relevant esophageal toxicity with or without endoscopic evidence of ulceration was identied in eight sbrt studies ( table 7 )  . data on esophageal motion induced by respiration in patients with lung cancer are very limited and the majority of data are derived from studies that attempt to estimate respiratory - induced motion of distal esophageal cancer . 
although the longitudinal and circular motion of the esophagus during the comparatively longer duration of sbrt treatment may alter the dose distribution in the esophageal mucosa and musculature , resulting in overor underestimation of doses in the esophagus , no data on the esophagus in an animalinherent motility in humans are available . strahlenther onkol ( 2017 ) 193 : 173184 table 6 studies utilizing fatal hemoptysis as safety endpoint study ( year ) wulf ( 2001 ) [ 43 ] no . 
the magnitude and duration of oral and aboral excursion were signicantly greater for the distal and proximal esophagus , respectively . while dosevolume effects in the esophagus have been exhaustively reviewed in the conventional setting , no large body of data existedup until december 2015on sbrtrelated esophagus toxicity . 
a retrospective recontouring of the esophagus revealed a hotspot resulting from the large uncertainty in treatment planning given the primitive techniques for planning target volume ( ptv ) and oar localization , delineation , and positional verication used in this study . deed , the data are very limited , making it very difcult to draw a meaningful conclusion . conclusion the similar rates of frightening complications reported in heterogeneous studies and their occurrence associated with all possible dose fractionation schedules suggest that there may be independent pretreatment patient and tumor risk factors surrounding these complications rather than the treatment per se . 
the current utilization of mostly inadequate endpoints for toxicity assessment may create an outward appearance of validity under which multiple competing risks that signicantly contributed to the occurrence and severity of observed toxicity are hidden . 
moreover , satisfactory documentation of complications and details of dosimetric parameters and dose fractionation are warranted . if this does not occur , the biased reporting of toxicity will continue to challenge the future utility of high - dose ablative radiation therapy . strahlenther onkol ( 2017 ) 193 : 173184 compliance with ethical guidelines conict of interest f . 
the accuracy of 3dus was signicantly higher than that of bone - match on longitudinal and vertical axes , but not on the lateral axis . conclusion image - guided radiotherapy of prostate cancer based on transperineal 3dus was feasible , with overall small discrepancy to seed - match in cbct in this retrospective study . 
compared to bone - match , transperineal 3dus achieved higher accuracy on longitudinal and vertical axes . keywords prostate cancer radiotherapy , image - guided radiotherapy , intensity - modulated organs at risk radiation oncologists vergleich der prostatapositionierung anhand dreidimensionalem transperinealem ultraschall und cone - beam - ct zusammenfassung zielsetzung bewertung der genauigkeit eines transperinealen dreidimensionalen ultraschallsystems ( 3dus ) fr die prostatapositionierung und vergleich mit goldmarkerund knochenbasierter positionierung in kilovolt - cone - beamcomputertomographie ( cbct ) bei einer denitiven strahlentherapie des prostatakarzinoms . 222 strahlenther onkol ( 2017 ) 193 : 221228 methoden vor behandlung wurden 7 patienten je drei goldmarker in die prostata implantiert . 
systematische und zufllige fehler sowie optimale sicherheitsabstnde wurden jeweils fr 3dus und knochen - koregistrierung berechnet . ergebnisse die diskrepanz zwischen 3dus und goldmarker - koregistrierung in cbct ( mittelwert standardabweichung ) betrug lateral 0 , 0 1 , 7 mm , longitudinal 0 , 2 2 , 0 mm und vertikal 0 , 3 1 , 7 mmit goldmarker - koregistrierung als referenz betrugen systematische fehler fr 3dus 1 , 2 , 1 , 1 und 0 , 9 mm , zufllige fehler 1 , 4 , 1 , 8 und 1 , 6 mm jeweils in lateraler , longitudinaler und vertikaler richtung . 
in analogie dazu betrug die differenz der knochen - koregistrierung zur goldmarker - koregistrierung 0 , 1 1 , 1 , 1 , 3 3 , 8 und 1 , 3 4 , 5 mm in lateraler , longitudinaler und vertikaler richtung ; systematische fehler waren 0 , 5 , 2 , 2 und 2 , 6 mm und zufllige fehler 1 , 0 , 3 , 1 und 3 , 9 mm jeweils in lateraler , longitudinaler und vertikaler richtung . 
die genauigkeit der 3dus war signikant hher als die der knochen - koregistrierung in longitudinaler und vertikaler , aber nicht in lateraler richtung . schlussfolgerung in der retrospektiven studie war die bildgefhrte strahlentherapie durch den transperinealen 3dus praktikabel beim prostatakarzinom mit insgesamt geringer diskrepanz zu goldmarker - koregistrierung in cbct . 
der transperineale 3dus erzielte eine hhere genauigkeit in longitudinaler und vertikaler richtung als die knochen - koregistrierung . schlsselwrter prostatakarzinom bildgesteuerte strahlentherapie intensittsmodulierte strahlentherapie risikoorgane strahlenonkologe radiotherapy for prostate cancer has undergone a dramatic technical development over the past 15 years , with the introduction of intensity - modulated radiation therapy ( imrt ) and image - guided radiotherapy ( igrt ) techniques [ 6 , 8 , 17 , 38 ]  . 
while a dose escalation to over 70 gy has been proven to be benecial for tumor control in a curative setting [ 12 , 25 , 28 ] , these technologic advances in radiotherapy allow margin reduction and thus a safe dose escalation to target volumes without an increase in relevant side effects [ 28 ]  . however , on the other hand , margin reduction renders dose coverage more sensitive to setup errors of target volumes and organs at risk , for example those caused by organ motion [ 36 ]  . 
depending on the variable lling of rectum and bladder , the prostate can change its position in the pelvis by more than 1 cm [ 9 , 18 ] between different fractions ( interfractional setup errors )  . 
the interfractional setup errors are the main cause of deviation of dose distribution to the target volumes and normal tissues [ 2 , 4 , 22 , 37 ]  . 
such interfractional setup errors can only be well managed by prostateguided repositioning before each fraction . there are several technical methods available for prostate - guided online repositioning , including ducialbased image guidance with cone beam ct ( cbct ) or portal images [ 30 , 32 , 33 ] , ultrasound ( us ) [ 10 , 14 , 19 , 34 ] , and the calypso tracking system ( varian medical systems , palo alto , ca , usa ) [ 16 , 20 ]  . 
the us - based technique has distinct advantages , such as its noninvasive nature and , in contrast to cbct or portal images , the lack of administered radiation dose , which can account for a relevant additional dose exposure within and outside the treatment region [ 26 , 27 ]  . the clarity system ( clarity system , elekta , stockholm , sweden ) is one of the latest generations of us - based guidance systems , using reconstructed three - dimensional image data . 
the clarity system differs from the older generation , such as bat ( b - mode acquisition and targeting ; nomos , cranberry township , pa , usa ) , sonarray ( varian , darmstadt , germany ) , etc . , as it is based on an intramodality verication method [ 24 , 29 ]  . 
for this purpose , a simulation us scan is performed in the planning phase and serves as a reference for repositioning in the treatment it has been shown that the intramodality method phase . has a signicantly higher accuracy than the cross - modality method , which compares us images to a planning ct [ 10 ]  . so far , experience with us - based guidance systems has been mostly limited to transabdominal us , which necessitates moderate to good bladder lling for good - quality us imaging [ 23 ]  . 
the present study investigated the transperineal clarity three - dimensional us ( 3dus ) system for prostate positioning , using the ducial - based measurements in cbct as a reference . patients and methods patients and treatment course setup errors of 7 prostate cancer patients during denitive radiotherapy were retrospectively evaluated . 
each patient received three gold markers implanted in the prostate under transrectal us guidance in the urological department about 2 weeks before the simulation ct ( details see [ 31 ] )  . all patients were advised to follow a protocol to ensure strahlenther onkol ( 2017 ) 193 : 221228 fig . 
1 claritytm ( clarity medical systems , pleasanton , ca , usa ) transperineal ultrasound system : mobile bedside workstation ( a ) , ultrasound probe with reectors xed to the board of knee cushion ( b ) , and ceilingmounted stereoscopic infrared camera ( c ; two arrows ) a moderately lled bladder and an empty rectum before simulation ct and before each radiotherapy fraction . patients were treated with a 6 mv linear accelerator ( elekta synergy ; elekta , stockholm , sweden ) with imrt plans . 
for scanning , the transperineal us probe was placed on the perineum by physicians or medical technical radiology assistants ( mtra ) , with moderate pressure for good quality of us images . 
from the us imaging data , 3d volume data were generated and presented in the workstation . using a calibration phantom , the 3dus system was calibrated to its inherent technical limit of about 1 mm radially [ 3 ]  . 
all 3dus and cbct measurements were retrospectively revised by one senior physician ( ml )  . treatment planning during simulation , after denition of the reference point and application of skin markers , a reference transperineal 3dus scan was acquired . 
the contour of the prostate based on us images was delineated and dened as the positioning reference volume ( prv ) for us - based positioning during the treatment . all images of simulation ct and all contours in digital imaging and communications in medicine ( dicom ) format were imported into the xvi control workstation ( xvi software version 3.5 ; elekta ) as a reference for cbct scans . cbct acquisition cbct provided volumetric datasets for positioning based on pelvic bones or implanted gold markers . 
in the right image , the green volume presents the prostate contured in the , and the red volume presents the protate in the current 3dus gained before each fraction of radiotherapy seed - match was then evaluated by the two - sided students t - test in comparison to the hypothetical zero mean . 
significance of the differences between 3dus and bone - match was tested by the paired two - sided students t - test . the mean and sd were also calculated for every patient individually and the respective systematic ( interpatient variability ) and random ( intrapatient variance ) errors were calculated as below : setup error in patient j during fraction i : correction strategy for patient positioning and image analysis before each radiotherapy treatment fraction , a 3dus scan was performed after initial alignment of skin marks to room lasers . 
thereafter , an additional bone - match was also performed retrospectively . data analysis and statistics since ducial - based alignment is considered the gold standard and is the most frequently used technique for prostate positioning [ 33 ] , its positioning results were used as a reference to evaluate the accuracy of 3dus and bone - match in cbct . 
for the differences between 3dus and seed - match , as well as for the differences between bone - match and seedmatch , the mean value with standard deviation ( sd ) , the median value , and the range were calculated for each of the three axes across all fractions . 
signicance with respect to mj = dij dene the average : and the variance : ( cid : 2 ) vj = dij mj ( cid : 3 ) the systematic error is : ( cid : 2 ) mj mj ( cid : 3 ) strahlenther onkol ( 2017 ) 193 : 221228 the random error is : ( cid : 2 ) = these errors were translated into the respective ctv to ptv margins using the optimal margin recipe by van herk [ 35 ]  . 
the limits of the condence interval of the random error were estimated as the roots of limits of the condence interval of the appropriate quantile of the students t - distribution for the variance . 
the condence interval of the resulting margin was conservatively estimated from the combined lower or upper limits of the condence intervals of the random and systematic errors . results viability of 3dus and availability of comparisons overall , the 7 patients underwent 252 treatment sessions . prostate positioning was successfully controlled by 3dus 200 times and by cbct 210 times . 
the following analysis is based on the data from these 177 treatment sessions and the accuracy evaluation of 3dus and bone - match are presented relative to the reference value provided by seed - match . comparison of setup errors from 3dus vs . 
longitudinally , 86% and 99% of discrepancies were less than 3 and 5 mm , respectively . vertically , 91% and 99% of discrepancies were less than 3 and 5 mm , respectively . the absolute value of the differences of prostate positioning between 3dus and seed - match amounted to up to 6.6 mm in the radial 3d direction . 
the optimal margins for 3dus were 3.9 mm in the lateral direction , 4.0 mm in the longitudinal direction , and 3.3 mm in the vertical direction , while the optimal margins for bone - match were 2.0 mm in the lateral direction , 7.7 mm in the longitudinal direction , and 9.3 mm in the vertical direction . 
to the best of the authors knowledge , the present study is the rst to report an accuracy assessment of a transperineal 3dus system under clinical conditions , using seed - match in cbct as reference . the current results showed that transperineal 3dus is feasible for igrt of prostate cancer with generally minor differences to ducial - based positioning ( table 1 )  . 
this nding is not unexpected , since the variable lling of rectum and bladder is the main cause of prostate motion within the pelvis and results predominantly in vertical and longitudinal movement of the prostate [ 9 ]  . 
however , on the other side , a reduced posterior margineven less than 7 mm [ 1 , 11 ] was used historically to limit the rectum dose and the risk of proctitis . 
prostate - guided repositioning , such as in 3dus or ducial - based methods , is obligate to ensure accurate dose delivery . using seed - match as reference , the present data showed that the accuracy of 3dus was signicantly better than that of bone - match on the longitudinal and vertical axes ( table 1 ) , whereas they were equivalent on the lateral axis . similar to ducial - based guidance , 3dus is also directly strahlenther onkol ( 2017 ) 193 : 221228 guided by the prostate . 
in the present study , there was no signicant difference on the lateral axis between any two of the three analyzed methods ( 3dus , seed - match , and bone - match ) in the two - sample t - test ( n = 177 )  . setup errors measured by seed - match in cbct were used as reference values for prostate positions , since ducial - based guidance has been proven to have a high accuracy for prostate positioning [ 21 , 33 ]  . 
another factor that affects the positional stability is the volume change of the prostate during a course of radiotherapy , particularly under additive hormone ablative therapy [ 33 ]  . 
in the interpretation of different setup errors from 3dus and seed - match in cbct , this issue should be taken into account . transperineal 3dus was developed as the next generation after transabdominal 3dus and has several distinct advantages over the transabdominal systefirstly , the imaging quality of transperineal 3dus is independent of bladder lling . 
in the authors last study of transabdominal 3dus , us - based prostate positioning could not be performed in 8% of all fractions due to insufcient bladder lling and thus limited us imaging quality [ 23 ]  . 
it has been reported that the pressure of the us probe needed for good - quality us imaging can change the prostate position [ 13 , 15 , 34 ]  . 
thus , a transperineal 3dus system can rule out these kinds of errors and further increase accuracy . nevertheless , us imaging is still an observer - dependent technique which requires sufcient training of medical staff . moreover , the sample size in this study is small , with 7 patients and 177 pairs of measurements . 
compared to bone - match , 3dus provides higher accuracy on the longitudinal and vertical axes , while there is no signicant difference between seed - match , bone - match , and 3dus on the less problematic lateral axis . acknowledgements we thank patrick dominik thum , andrea beisel , anne kolberg , gabriela danilkiewicz , and anja weber for their excellent work as radiation therapists . funding elekta germany supports research at the university hospital of the ludwig maximilian university . 
elekta had no inuence on study design ; nor on data collection , analysis , or interpretation ; nor on the writing of the manuscript ; nor on the decision to submit the manuscript for publication . compliance with ethical guidelines conict of interest h . 
an external marker was attached to the surface of both phantoms and volunteers as a secondary object to be tracked by an infrared camera for comparison . results phantom measurements showed increased accuracy of us tracking with decreasing scanning range / increasing scanning frequency . 
further investigation in a larger cohort of patients is underway . keywords stereotactic body radiotherapy ( sbrt ) ultrasound radiotherapy , image - guided intrafractional tracking upper abdomen ein 4d - ultraschall - tracking - system fr die externe radiotherapie bei oberbauchlsionen unter atemanhalt zusammenfassung hintergrund und ziel evaluation eines neuen vierdimensionalen ( 4d ) ultraschall ( us ) - tracking - systems fr die externe strahlentherapie von oberbauchlsionen unter computergesteuertem tiefem atemanhalt ( dibh )  . material und methoden die tracking - genauigkeit des 4dus - systems wurde mittels zweier bewegungsphantome , die mit sinusfrmigen und atmungshnlichen bewegungsmustern zur simulation der freien atmung und dibh programmiert wurden , bestimmt . 
1 ultrasound phantom with motion platform ( bat , nomos , pittsburgh , pa , usa ; and cirs , norfolk , va , usa ; a ) and a four - dimensional phantom ( aktina medical , north congers , ny , usa ; b ) untersucht . 
zum vergleich wurde ein externer marker als sekundres , von einer infrarotkamera getracktes objekt auf der oberche beider phantome und probanden angebracht . ergebnisse phantommessungen zeigten eine erhhte genauigkeit des us - trackings , wenn der scanbereich verkleinert wurde . 
die wahrscheinlichkeit fr einen verlust der zu trackenden struktur war fr kleine scanbereiche hher ( 43 , 09 % fr 10 ; 13 , 54 % fr 20 )  . 
die mehrheit der untersuchten atemanhaltephasen wies eine starke korrelation zwischen der bewegung des markers und dem us - tracking auf : 84 , 06 und 88 , 41 % fr nierenbeckentargets und 82 , 26 und 91 , 94 % fr lebervenentargets jeweils in anteroposteriorer und superoinferiorer richtung ; der pearson - korrelationskoefzient lag zwischen 0 , 71 und 0 , 99 . schlussfolgerung das us - system zeigte eine gute tracking - leistung in 4d - bewegungsphantomen . 
die tracking - fhigkeit von surrogat - strukturen fr oberbauchlsionen in dibh erfllt die klinischen anforderungen . weitere untersuchungen in einer greren patientengruppe sind im gange . schlsselwrter stereotaktische krperbestrahlung ultraschall bildgesteuerte strahlentherapie intrafraktionre verfolgung abdomen hypofractionated stereotactic body radiotherapy ( sbrt ) is an effective low - toxicity treatment option for primary liver , renal , and pancreatic cancer and hepatic / adrenal metastases [ 13 ]  . 
however , these techniques all apply an additional radiation dose to the patient and allow no direct soft tissue visualization , requiring invasively implanted ducial markers [ 6 ]  . 
ultrasound ( us ) is a cost effective , noninvasive , and nonionizing approach allowing not only interfractional soft tissue - based repositioning [ 7 ] , but also intrafractional motion monitoring / tumor tracking [ 8 ]  . the feasibility of using computer - controlled deep inspiratory breath - hold ( dibh ) performed with , e . 
g. , the active breathing coordinator ( abc ) system ( elekta ab , stockholm , sweden ) to temporarily immobilize the patients breathing has been investigated by many authors [ 911 ]  . simulation , treatment planning , and radiation delivery are performed under identical abc conditions with minimal margins for breathing motion . 
the motion platform was programmed to perform repeated mechanical movement to simulate a sinusoidal pattern with several amplitudes and cycle times in leftright ( lr ) and superoinferior ( si ) directions . 
the difference between us detection and marker position was quantied . healthy volunteers after obtaining permission from the local irb , ve healthy volunteers were set up to simulate the clinical situation of repeated dibh to obtain the performance of us tracking in vivo in the clinical situation . 
us datasets were acquired in computer - controlled breath - hold ( abc ; breath - hold time 20 s , free breathing phases of 56 breath cycles )  . 
2 ultrasound probe setup on healthy volunteer with active breathing coordinator ( abc ; elekta ab , stockholm , sweden ) - based breath - hold and xation arm in the authors department , attening lter - free sbrt is performed in computer - controlled dibh and image - guidance with breath - hold cone beam ct [ 7 ]  . 
residual errors , intrafractional reproducibility of the breath - hold , and organ position instability potentially enlarging the planning target volume ( ptv ) clinical target volume ( ctv ) margin still have to be considered . 
the accuracy and clinical applicability of this tracking system was evaluated and tested based on 4d motion phantoms and ve healthy volunteers . materials and methods clarity anticosti ultrasound system a 4d us tracking system ( clarity anticosti , elekta ab ) was used as an experimental version after approval from the local institutional review board ( irb )  . 
the device consists of a 2d probe that undergoes a motor - driven sweeping motion . it was modied for transabdominal imaging with a customizable attachment of an infrared optical tracking ducial tree . 
clarity anticostis monitoring function is based on a prostate tracking model ( assuming a spherical , slow - moving structure ) , which was applied in this study to a faster - moving target ( liver )  . 
2. results ultrasound phantom and motion platform the rst experiment was performed with the default settings of the us system ( 40 scanning range ) with different cycle times ( t ) of sinusoidal patterns ( amplitude , a = 10 mm )  . 
the differences between the measurement and the reference ( mean standard deviation ) values of the sphere motion can be seen in table 2 . the measurement result from one representative breathing pattern with different scanning ranges is shown in fig . 
the average amplitude of the free - breathing pattern was 11 mm and the maximum amplitude was 15 mm ; while in the breath - hold phase , the average amplitude was 16 mm and the maximum amplitude was 20 mrelevant lost tracking occurred only in the 10 and 20 scanning ranges for all breathing phases of the emulated cycle . 
therefore , 30 seems to be the optimal scanning range in the clinical setting to track alongside respiratory motion , with a probability of lost tracking below 0.1%. healthy volunteers the new research setup with the arm - based xation of the us probe and combination with computer - controlled dibh could be easily applied to all healthy volunteers without noticeable inconvenience , and was stable during test sessions in all cases , image quality was sufcient for of 30 min . denition of the us tracking target and tracking / monitoring during dibh . 
over all healthy volunteers and scan ranges , the pcc indicated a strong correlation for most breath - holds analyzed . for the renal pelvis target , a strong correlation ( pcc 0.720.99 ) was observed in 58 and 61 breath - holds in the ap and si directions , respectively . 
no correlation ( pcc 0.310.49 ) was found in two and three breath - holds for the ap and si directions , respectively . for a liver vein target , a strong correlation ( pcc 0.710.99 ) was found in 51 and 57 breath - holds in the ap and si directions , respectively . 
to enable complete intrafractional control of dibh treatments , which have several procedural and dosimetric advantages in photon and particle therapy [ 11 ] , online time - resolved real - time soft tissue tracking is needed . most tracking methods currently available in clinical rou218 strahlenther onkol ( 2017 ) 193 : 213220 fig . 
 [ 22 ] determined the 3d tracking accuracy of a tracking system based on implanted ducial markers and uoroscopy to be 1.5 mgiven these excellent overall results , us tracking has the potential to be used in lieu of uoroscopy tracking measurements to eliminate invasive marker implantation and costs / side effects associated with uoroscopic markers and the associated radiation doses to patients [ 23 ]  . in the rare event of lost tracking during phantom - based simulation , the system could immediately redetect the correct position when the target was back in range . 
the limitation of these data is that they were acquired in the phantom environment , with a spherical tracked structure ideal for the tracking algorithtracking robustness might be different in the human body , with less clear interfaces and more complex non - spherical structures suitable for tracking . 
as a crucial element of the process , the probe holder can effectively hold the probe in place for prolonged measurement durations . the probe kept completely steady during measurement , but does seem to retain a minimal exibility that will be needed in a clinical application . online comparison with a gold standard ( ducials ) was obviously not possible in volunteers , but it was possible to assess the correlation of motion timing and orientation with surface markers as a rst plausibility test . 
in addition , further improvement of the tracking algorithm will improve accuracy alongside respiratory motion when using larger scanning angles for detection of high - amplitude motion and nonlinear transformations of the tracking target . nevertheless , the additional use of us surveillance of dibh treatments would already be possible with manual online validation of the plausibility of tracking . conclusion the new us system demonstrated good performance and tracking accuracy in a 4d motion phantom when tracking a target moving according to a simulated breathing pattern . considering the accuracy of tracking and the possible loss of the tracked structure , a 30scanning range turned out to be optimal to track alongside respiratory motion . 
lohr received research grants from elekta and iba , teaching honoria from elekta and iba , board honoria from c - rad , and works for the iba advisory board . 
combs1 , 2 received : 28 july 2016 / accepted : 6 october 2016 / published online : 1 november 2016 springer - verlag berlin heidelberg 2016 abstract background stereotactic radiotherapy ( rt ) has been established as a valid treatment alternative in patients with vestibular schwannoma ( vs )  . 
hearing preservation may be the primary goal for patients with vs , followed by maintenance of quality of life ( qol )  . methods from 2002 to 2015 , 184 patients with vs were treated with radiosurgery ( rs ) or fractionated stereotactic radiotherapy ( fsrt )  . 
the established questionnaire could be validated in the independent cohort . keywords survial quality of life patient self - reported outcome questionnaires toxicity fraktionierte stereotaktische radiotherapie vs . radiochirurgie bei patienten mit vestibularisschwannom erhalt des hrvermgens und patientenselbstbericht anhand eines etablierten fragebogens zusammenfassung hintergrund die stereotaktische radiotherapie ( rt ) wurde als gltige behandlungsalternative bei patienten mit vestibularisschwannom ( vs ) etabliert . 
der erhalt von hrvermgen und lebensqualitt ( qol ) sind hauptziele fr patienten . methoden von 2002 bis 2015 wurden 184 vs - patienten mit radiochirurgie ( rs ) oder fraktionierter stereotaktischer radiotherapie ( fsrt ) behandelt und aktuelle nebenwirkungen und qol zwischen februar und juni 2016 bewertet . strahlenther onkol ( 2017 ) 193 : 192199 ergebnisse das mediane follow - up nach rt betrug 7 , 5 jahre ( spanne 014 , 4 jahre ) , das mittlere gesamtberleben ( os ) nach rt 31 , 1 jahre , mit berlebensraten von 94 und 87% nach 5 und 10 jahren und das mittlere progressionsfreie berleben ( pfs ) 13 , 3 jahre , mit einem 5und 10 - jahres - pfs von 92% . 
der etablierte fragebogen konnte in dieser unabhngigen kohorte validiert werden . schlsselwrter berleben lebensqualitt patientenselbstbericht fragebgen toxizitt stereotactic radiotherapy ( rt ) has been established as a valid treatment alternative in patients with vestibular schwannoma ( vs )  . 
there is ongoing controversy regarding the optimal fractionation : while some authors clearly prefer short treatment times and report data from radiosurgery ( rs ) approaches , others favor a fractionated regimen on the basis of a radiobiological benet of fractionation which is associated with a promising riskbenet prole for smaller and large vs alike . hearing preservation may be the primary goal for vs patients , followed by maintenance of quality of life ( qol )  . in turn , qol is inuenced by the typical side effects of impaired facial and trigeminal nerve function , tinnitus , imbalance , dizziness , and gait uncertainty . 
current treatment options are wait - and - see , microsurgery , rs , and fractionated stereotactic radiotherapy ( fsrt ) , all equally effective depending on the size and location of the tumor [ 1 , 2 ]  . often the treatment decision depends on the physicians experience and patients preferences . 
for large tumors , surgical resection is often preferred , with preservation of facial nerve function in about 85% of cases , while the rate of hearing preservation is about 50% [ 35 ]  . 
for smaller tumors , preservation rates of 90% for facial nerve function and of 80% for hearing can be achieved [ 68 ]  . recent studies examine very little data on qol . 
however , it has been shown that the physician - reported outcome can vary substantially from the patient - reported outcome , and this information should therefore be taken into account when comparing treatment modalities . 
in the present work , the authors sought to validate the questionnaire previously developed by combs et al . in 2013 [ 9 ] in an independent cohort of vs patients , and differentially report on outcome and hearing preservation after single - fraction or fractionated stereotactic radiotherapy ( fsrt )  . patients and methods patients from 2002 to 2015 , 184 patients with vs were consecutively treated at the department of radiation oncology at the klinikum rechts der isar , munich , germany . 
primary endpoints were local control and facial and trigeminal neuropathy , as well as qol and patient - reported outcome . of all patients , 43% were male ( 80 / 184 ) and 57% ( 104 / 184 ) female . 
the gardnerrobertson scale was used to determine hearing status before and after rt ; the housebrackmann facial weakness scale for the facial nerve status . of all patients , 8 had received previous surgery within 6 months before rt . 
the remaining 3 patients with nf2 had undergone surgery more than 4.5 years before radiotherapy in 56 patients , rt was performed as rs with a median dose of 12 gy . 
dose was applied with a varian trilogy linear accelerator ( linac ; varian , palo alto , ca , usa )  . treatment planning for rs and fsrt was performed using a stereotactic treatment setup with a thermoplastic mask system ( brainlab , feldkirchen , germany ) and daily imageguided rt ( igrt ) by robotic exactrac positioning ( brainlab )  . 
the planning target volume ( ptv ) resulted from the gtv with an additional margin of 12 mthe dose was described on the 80% isodose for rs and on the 95% isodose for fsrt . 
for patient characteristics , see table 1 . patients were enrolled into a follow - up regimen with assessment 6 months after rt and yearly thereafter , including contrast - enhanced mri as well as clinical assessment . 
additional examinations were scheduled if clinically needed . all decisions regarding further treatments were made on an interdisciplinary basis . follow - up the survey was conducted between february and june 2016 . the questionnaire developed by combs et al . 
patients living outside germany and already deceased patients were not included . the survey on patient self - reported outcome focuses mainly on the following aspects : questions regarding symptoms , items assessing overall hearing and qol before and after rt treatment , post - rt treatments , and status of last ( external ) follow - up . statistics statistical calculations were performed using spss statistics v . 
for all patients , overall survival ( os ) was calculated from the last day of rt until death or last follow - up ; progression - free survival ( pfs ) from the last day of rt until the date of progression or death or last follow - up . 
a p - value ( cid : 2 ) 0.05 was considered statistically signicant . results outcome median follow - up after rt was 7.5 years ( range 014.4 years , including foreign patients who were lost to follow - up )  . 
5 diagram showing answers for the question a did your side effects improve after rt ? , b how do you feel after rt , c how is you quality of life after rt . 
this supports the value of the present questionnaire during follow - up in addition to standard clinical and imaging examination . for vs , treatment decision - making depends on the size of the lesion as well the clinical presentation of patients . for small and asymptomatic tumors , a wait - and - scan strategy might be followed ; generally , average growth ranges between 1 and 3 mm per year , and close clinical and radiological follow - up will be able to capture early recurrence , enabling safe and effective treatment at such a time . considering hearing development throughout the clinical course , natural hearing deterioration is also present independently of vs , particularly in the aging population . 
hearing deterioration generally occurs directly after surgery , whereas any hearing impairment after rt develops over time , in most cases within the rst 6 months when directly attributable to rt has become established as a noninvasive and toxicity - minimized treatment alternative . 
hearing deterioration depends on the series and is between 85 and 90% after 10 and 20 years [ 16 ] , although rt rarely leads to complete loss of hearing when performed early . 
smaller series have reported that fractionated treatment might be safer in terms of cranial nerve toxicity , and this certainly may hold true for larger lesions ; only recently , fong and colleagues reported that hearing preservation was higher after fractionated regimens [ 8 ]  . 
in a previously published multicenter analysis , the authors of the current study demonstrated comparable hearing preservation for smaller lesions ; however , larger lesions were all treated with fractionated concepts , independent of the treating center [ 14 ]  . 
independent of size , dose is also a strong prognostic factor : it has been shown in the past that single doses exceeding 13 gy lead to a signicant risk of hearing impairment and facial or trigeminal nerve toxicity [ 17 , 18 ]  . 
for fractionated regimens , no difference in toxicity proles between 54 and 57.6 gy has been reported ; however , in the study by champ et al . , even more 198 strahlenther onkol ( 2017 ) 193 : 192199 benecial toxicity proles were reported with 46.8 gy in single fractions [ 19 ]  . 
long - term analysis must conrm that this safety does not compromise long - term local control . considering the effectiveness of neurosurgical resection in an experienced team , as well as the benecial toxicity prole of rt , a combined treatment approach might be the treatment of choice in the future , particularly for larger and brainstem - compressing lesions . 
planned partial and maximal safe resection can then be consolidated with highly precise rt to any tumor remnants . as the validation of the questionnaire by combs et al . [ 9 ] showed reliable results , this is now being implemented in the authors daily clinical routine . 
particularly in cases where long - term side effects of treatment are relevant and patients are easily lost to follow - up , regularly performed assessment of patient - reported outcome is a suitable tool to quantify symptomatic improvement or worsening . 
however , it must be considered that the need for continuous validation of qol questionnaires is substantial , as controllability is a crucial part of the scientic process and data of nonvalidated questionnaires do not match the criteria of good scientic practice . conclusion these data conrm that rs and fsrt are comparable in terms of local control for vs . 
particularly for larger volumes , a combined treatment approach comprising neurosurgery and rt might in addition to be the treatment of choice in the future . standard clinical and imaging examinations , patient selfreported outcome during follow - up is of high value . 
combs declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
januar 2017 springer - verlag berlin heidelberg 2017 fragestellung und hintergrund in der behandlung der nichtoperablen und nicht fr die stereotaxie ( sbrt ) geeigneten nicht - kleinzelligen bronchialkarzinome ( nsclc ) sind in den letzten jahren vergleichsweise begrenzte verbesserungen erzielt worden [ 1 ]  . 
die radiound radiochemotherapie sind prinzipiell effektiv , bedrfen aber der weiterentwicklung , um die lokale kontrolle zu verbessern , wobei auch das hug dosislimitierende problem der normalgewebetoleranz nicht aus den augen gelassen werden darf [ 2 ]  . 
falls dieser effekt in kleineren studien nicht eindeutig ausgeprgt sein sollte , knnen metaanalysen eine klarere antwort liefern . material und methodik die krzlich publizierte metaanalyse der universitt oxford inkludierte 21 studien mit 3795 patienten , die zur klrung der oben genannten frage zwischen 1982 und 2011 randomisiert worden waren [ 3 ]  . in 11 studien war die randomisierung vor dem jahr 2000 abgeschlossen worden . 
der auswertung lag die biologisch effektive dosis von insgesamt 25 studienarmen zugrunde , davon setzten 12 die hyperfraktionierung edie gesamtdosis wurde in 2 - gy - quivalentdosen umgerechnet , und zwar zeitkororiginalpublikation ramroth j , cutter dj , darby sc et al ( 2016 ) dose and fractionation in radiation therapy of curative intent for non - small cell lung cancer : meta - analysis of randomized trials . 
folgende annahmen lagen der berechnung zugrunde : / - wert 10 gy , beginn der repopulation nach 21 tagen , notwendige dosis , um die repopulation auszugleichen , 0 , 6 gy . 
es wurde nicht auf die individuellen patientendaten zurckgegriffen . ergebnisse die alleinige dosiseskalierte strahlentherapie fhrte zu einem signikant lngeren medianen berleben ( survival ratio 1 , 13 ; 95 % - kondenzintervall ( ki ) 1 , 041 , 22 ; berlebensgewinn zirka 2 monate )  . 
fnf der studien mit alleiniger strahlentherapie hatten im niedriger dosierten arm bereits eine relativ hohe eqd2t 53 , 5 gy verschrieben und trotzdem eine differenz von mehr als 10 gy zum hher dosierten arhier wurde das mediane berleben um den faktor 1 , 87 verbessert ( 95 % - ki 1 , 472 , 38 ; gewinn zirka 1 jahr )  . 
es spielte keine rolle , ob eine hyperfraktionierung oder aber andere arten der dosiseskalation gewhlt worden waren . schlussfolgerung der autoren bei simultaner gabe von chemound strahlentherapie ist eine dosiseskalation ungnstig . 
verffentlichten im jahr 2002 eine auswertung von 192 einzelnen lsionen bei 135 patienten mit nsclc , die mit einer durchschnittlichen dosis von 59 , 9 gy bestrahlt worden waren [ 5 ]  . 
erhielten patienten mit einem nsclc im stadium i , bei denen eine operation kontraindiziert war , in einem arm eine konventionelle 7 - wchige strahlentherapie bis 70 gy [ 6 ]  . 
eine variante des chart - regimes , die einer konventionellen strahlentherapie von zirka 80 gy entspricht ( 68 , 4 gy in 38 fraktionen ber 25 tage , 2 - mal 1 , 8 gy tglich ; [ 7 ] )  . 
es erscheint unrealistisch , wenn sehr viel hhere lokale kontrollraten erwartet werden , da die normalgewebetoleranz von lunge , sophagus , herz , trachea und der groen blutgefe die applikation einer hohen eqd2 bei groen tumorvolumina verunmglichen . 
das bedeutet , dass eine erhhung der dosis um 1 gy eine 3 %ige reduktion des risikos bewirkte , am tumor zu versterben . das ergebnis der hier kommentierten metaanalyse , die nur auf das berleben und nicht auf die lokale kontrolle fokussierte [ 3 ] , wird mit den oben zitierten beobachtungen verstndlich . 
die denition der solcherart optimierten dosis und fraktionierung muss aber mit prospektiven studien erfolgen . wie lsst sich nun erklren , dass die kombination aus simultaner chemotherapie , deren rationale und strahlensensibilisierende wirkung gut dokumentiert sind , und dosiseskalation das berleben tatschlich verschlechtert ? denn eigentlich msste ja gerade bei patienten , deren mikrometastasen effektiv behandelt werden , eine bessere lokale kontrolle in ein besseres berleben mnden . 
mglicherweise sind spter auftretende ereignisse oder therapieunterbrechungen in diesem zusammenhang wichtiger . die ergebnisse des 74 - gy - arms der rtog - 06 - 17 - studie [ 4 ] , die aufgrund ihrer patientenzahl auch die resultate der metaanalyse stark bestimmte , fhren glcklicherweise nicht dazu , dass jegliche forschung zum thema optimale radiochemotherapie auf eis gelegt wird [ 10 ]  . 
dosiseskalation nur auf bestimmte biologisch besonders relevante teile des zielvolumens drften dazu beitragen , dass eine sichere dosiseskalation in kombination mit der chemotherapie in zukunft vielleicht doch angeboten werden kann . in einer retrospektiven analyse der national cancer database mit ber 30.000 patienten im stadium iii war die dosiseskalation ber 60 gy hinaus bei einer radiochemotherapie mit einem verbesserten berleben vergesellschaftet [ 11 ]  . 
kritisch wre in diesem kontext zu bemerken , dass die methode der metaanalysen nicht nur vorteile hat , sondern dass , bedingt durch die heterogenitt der inkludierten studien , die inklusion oder exklusion elektiver lymphknotenstationen in die zielvolumina und die erheblichen nderungen des stagings und der behandlungstechniken in den letzten 25 jahren im bertragenen sinn auch veraltete rosinenbomber mit modernen jumbojets gepoolt zu einem mittleren effekt verarbeitet werden . 242 fazit die alleinige strahlentherapie beim nsclc sollte dosiseskaliert mit einer dosis erfolgen , die biologisch effektiver ist als 70 gy in konventioneller fraktionierung , und die bekannten normalgewebetoleranzdosen einhalten . 
in jedem fall sollten anstrengungen unternommen werden , das zielvolumen richtig zu denieren und die verschriebene dosis trotz atemverschieblichkeit auch anatomisch korrekt zu applizieren ( igrt )  . carsten nieder , bod , norwegen interessenkonikt c . 
guckenberger m , kavanagh a , partridge m ( 2012 ) combining advanced radiotherapy technologies to maximize safety and tumor control probability in stage iii non - small cell lung cancer . 
ramroth j , cutter dj , darby scj et al ( 2016 ) dose and fractionation in radiation therapy of curative intent for non - small cell lung cancer : meta - analysis of randomized trials . 
bradley jd , paulus r , komaki r et al ( 2015 ) standard - dose versus high - dose conformal radiotherapy with concurrent and consolidation carboplatin plus paclitaxel with or without cetuximab for patients with stage iiia or iiib non - small - cell lung cancer ( rtog 0617 ) : a randomised , two - by - two factorial phase 3 study . 
willner j , baier k , caragiani e et al ( 2002 ) dose , volume , and tumor control prediction in primary radiotherapy of non - small - cell lung cancer . 
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chen m , hayman ja , ten haken rk et al ( 2006 ) long - term results of high - dose conformal radiotherapy for patients with medically inoperable t1 - 3n0 non - small - cell lung cancer : is low incidence of regional failure due to incidental nodal irradiation ? int j radiat oncol biol phys 64 : 120126 9 . 
zhao j , xia y , kaminski j et al ( 2016 ) treatment - related death during concurrent chemoradiotherapy for locally advanced non - small cell lung cancer : a meta - analysis of randomized studies . 
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brower jv , amini a , chen s et al ( 2016 ) improved survival with dose - escalated radiotherapy in stage iii non - small - cell lung cancer : analysis of the national cancer database . 
das ziel dieser metaanalyse [ 2 ] war daher die berprfung einer mglichen assoziation zwischen fettleibigkeit oder bergewicht und dem auftreten einer kardiotoxizitt nach gabe von anthrazyklin oder der sequenziellen gabe von anthrazyklin - trastuzumab bei brustkrebspatientinnen . methode in einer sogenannten random - effects - analyse als lineares paneldatenmodell sowie einer network - metaanalyse wurden 15 studien mit insgesamt 8745 brustkrebspatientinnen , die mit anthrazyklinen oder sequenziell mit anthrazyklin - trastuzumab behandelt wurden , eingeschlossen . ergebnisse wurden die ergebnisse fr fettleibigkeit und bergewicht zusammengefasst , zeigte sich ein signikant hheres risiko fr die entwicklung einer kardiotoxizitt nach gabe von anthrazyklinen oder der anthrazyklintrastuzumab - sequenz . 
die statistische analyse zeigte weiterhin , dass diese assoziation unabhngig vom studiendesign , dem publikationsjahr oder den verabreichten medikamenten ( anthrazykline oder die sequenzielle gabe von anthrazyklin - trastuzumab ) war . 
allerdings war diese art der analyse nicht in der lage , den spezischen beitrag kardiovaskulrer risikofaktoren wie diabetes oder erhhter blutdruck vom erhhten risiko der fettleibigkeit zu trennen . schlussfolgerung der autoren diese analyse legt nahe , dass bergewicht und fettleibigkeit risikofaktoren fr die entwicklung einer kardiotoxizitt durch anthrazykline oder durch die sequenzielle gabe von anthrazyklinen und trastuzumab sind . kommentar sowohl anthrazykline als auch der monoklonale antikrper trastuzumab sind wichtige medikamente , die beim mammakarzinom sowohl in der metastasierten als auch adjuvanten situation eingesetzt werden . 
die gabe dieser substanzen ist allerdings mit einem signikanten risiko fr das auftreten einer kardiotoxizitt verbunden , die akut , verzgert oder aber auch erst jahre nach abschluss der behandlung manifest werden kann . 
eine aktuelle metaanalyse beziffert das durch anthrazykline bedingte risiko fr das auftreten einer mit klinischen symptomen einhergehenden kardiotoxizitt mit 6 % ; eine subklinische kardiotoxizitt entwickelte sich bei 18 % der patienten [ 1 ]  . strahlenther onkol ( 2017 ) 193 : 234235 besonders bei anthrazyklinen ist dieses risiko dosisabhngig , ohne dass es einen schwellenwert gibt , unterhalb dessen kein risiko besteht . 
daher besteht ein dringender bedarf an der denition weiterer unabhngiger risikofaktoren bei herzgesunden patienten und patientinnen . die ergebnisse der metaanalyse von guenancia et al . zeigen berzeugend , dass ein erhhter bmi ein signikanter und unabhngiger risikofaktor fr das auftreten einer kardiotoxizitt durch anthrazykline oder die sequenzielle gabe von anthrazyklinen und trastuzumab ist [ 2 ]  . 
die meisten der analysierten studien denierten eine kardiotoxizitt entsprechend der publizierten konsensusdenition [ 3 ]  . diese metaanalyse wurde mittels einer komplexen statistik durchgefhrt , die die gemessenen effekte eher unterschtzt [ 2 ]  . 
die rate an kardiotoxizitt aller 8745 patientinnen betrug 17 % , bei patientinnen , die anthrazykline alleine erhielten , 20 % und bei denjenigen , die mit trastuzumab mit oder ohne anthrazyklinen behandelt wurden , 16 % . 
wahrscheinlich wird damit das risiko aber noch unterschtzt , da probanden in klinische studien gewhnlich gesnder sind als die in der realitt auerhalb von studien behandelten patienten . eine subgruppenanalyse zeigte eine zunahme des risikos mit ansteigendem bmi ( or von 1 , 15 fr bergewichtige patientin bis auf eine or von 1 , 38 fr fettleibigkeit mit einem bmi > 25 kg / m2 )  . 
in der lage , das kardiotoxizittsrisiko der unterschiedlichen therapieregime in den untersuchten studien oder den effekt von trastuzumab allein zu klren , ebenso nicht , ob sich das risiko zwischen der adjuvanten und metastasierten situation unterscheidet ( metastasierte patientin entsprachen nur einem relativ kleinen anteil aller eingeschlossenen patientinnen )  . 
auch war es nicht mglich , die mit bergewicht assoziierten kardialen risikofaktoren , wie arterielle hypertonie oder erhhte blutfette oder rauchgewohnheiten , in eine separate analyse einzubeziehen . trotzdem erscheinen die ergebnisse berzeugend und sollten bei der wahl des therapieregimes bercksichtigt werden . 
haben bereits gezeigt , dass fettleibigkeit die prognose von patientinnen mit brustkrebs , die mit einer anthrazyklin - basierten chemotherapie behandelt wurden , verschlechtert und zu einem reduzierten gesamtund krankheitsfreien berleben fhrt [ 5 ]  . 
bisher gibt es aber keine ausreichend sensitive und spezische methode , die das auftreten der klinisch relevanten kardialen spttoxizitt bei gabe von anthrazyklinen frhzeitig vorhersagen kann [ 6 ]  . martin wilhelm , nrnberg interessenkonikt m . 
guenancia c , lefebvre a , cardinale d et al ( 2016 ) obesity as a risk factor for anthracyclines and trastuzumab cardiotoxicity in breast cancer : a systematic review and meta - analysis . 
ladoire s , dalban c , roch h et al ( 2014 ) effect of obesity on disease - free and overall survival in nodepositive breast cancer patients in a large french population : a pooled analysis of two randomised trials . 
zamorano jl , lancellotti p , rodriguez munoz d et al ( 2016 ) esc position paper on cancer treatments and cardiovascular toxicity developed under the auspices of the esc committee for practice guidelines . 
februar 2017 springer - verlag berlin heidelberg 2017 hintergrund und zielsetzung die primre radiochemotherapie ( rct ) ist die standardbehandlung fr patientinnen mit nodal positiven und / oder lokal fortgeschrittenen zervixkarzinomen . 
der einsatz der hoch standardisierten bt auf mrt - basis konnte die lokale kontrolle deutlich verbessern und auch die toxizitt unter denierten kriterien wesentlich absenken [ 1 ]  . patientinnen und methoden die hier mit ct anstatt mit mrt geplante hdr - bt erfolgte entsprechend den empfehlungen der group european de curietherapie european society for therapeutic radiology and oncology ( gec - estro ) an 216 konsekutiven patientinnen mit einem lokal fortgeschrittenen zervixkarzinom der stadien figo ibiva . 
60 gy auf vergrerte lymphknoten ( lk ) und einer einmal wchentlichen bt nach beendigung der ebrt mit 7 , 5 gy ed ( d90 mindestens 84 gy ) fr insgesamt 4 fraktionen . 
die gesamtbehandlungszeiten originalpublikation zolciak - siwinska a , gruszczynska e , bijok m et al ( 2016 ) computed tomography - planned high - dose - rate brachytherapy for treating uterine cervical cancer . 
die akzeptierte eqd2 aus ebrt und bt am rektum waren 75 gy in d2cc des rektums und 90 gy fr die blase bei einem / = 3 fr spt reagierendes normalgewebe . 
auerdem wurden die daten mit einem historischen kollektiv verglichen , einer randomisierten studie aus derselben klinik , bei der die kombinierte radiochemotherapie hyperthermie verglichen wurde [ 2 ]  . ergebnisse die mediane nachbeobachtung der berlebenden patientinnen betrug 52 monate ( spanne 3763 monate )  . 
in der historischen gruppe waren , ergab sich eine verringerung der fistelbildung um 59 % sowie der sptfolgen vom grad 3 und 4 am rektum um > 59 % . 1 medizinische fakultt der universitt zu kln , cyberknife centrum , klinik fr strahlentherapie der uniklinik kln , 50937 kln , deutschland schlussfolgerung der autoren es handelt sich um den grten bericht , dass die ct - geplante hdr - bt von patistrahlenther onkol ( 2017 ) 193 : 236239 entinnen mit fortgeschrittenem zervixkarzinom eine gute lokale tumorkontrolle bei akzeptaler toxizitt ermglicht . im vergleich mit historischen daten haben die frauen einen substantiellen vorteil bezglich schwerer spteffekte . kommentar das erstaunen ber die publikation der vorliegenden arbeit im international journal of radiation oncology , biology , physics begleitet einen beim lesen , da weder die onkologischen ergebnisse noch die toxizitten die primr interessanten aspekte der arbeit sind . 
vielleicht ging es dem journal eher um die informationen zwischen den zeilen . polen gehrt zu den osteuropischen lndern mit niedrigem pro - kopf - einsatz im gesundheitssystem und einem ungnstigen verhltnis von letalitt und inzidenz . 
die vorliegende arbeit berichtet ber daten aus einem zentrum , dem marie sklodowska curie memorial cancer center , von ber 200 zervixkarzinompatientinnen , die in nur 2 jahren behandelt wurden . 
das ist eine logistische herausforderung , generiert aber expertise , ber die keine einzige deutsche klinik verfgt , wo 85 % aller zervixkarzinompatientinnen in einrichtungen behandelt werden , die weniger als 5 flle pro jahr haben [ 4 ]  . 
dies bedeutet einen groen vorteil fr die polnischen patientinnen , da das behandlungsvolumen einer abteilung mit dem outcome beim zervixkarzinom , wie auch bei anderen tumoren , korreliert [ 5 , 6 ] ein aspekt , der in deutschland in den letzten 30 jahren weitgehend ignoriert wurde . die expertise des behandelnden zentrums zeigt sich in der vorliegenden arbeit mit einer sehr guten therapieadhrenz und - qualitt : immerhin 90 % der patientinnen erhielten eine chemotherapie , und die verschriebene brachytherapiedosis betrug mindestens 84 gy ( d90 )  . 
die therapiedauer wird nicht berichtet , ist aber sicher kritisch zu bewerten , da nach 67 wochen ebrt in weiteren 4 wochen nur eine einzige wchentliche bt erfolgte , was die therapiedauer auf 1112 wochen hinausgezgert haben drfte und zu verbessern ist [ 7 ]  . im gegensatz zur neueren literatur hatten die polnischen patientinnen zu 92 % plattenepithelkarzinome , was erstaunlich ist und ggf . 
unklar bleibt , warum nur 3 , 4 % der patientinnen eine hydronephrose aufweisen ( = figo - stadium iiib ) , aber 30 % der kohorte dem figo - stadium iii zugeordnet wurden . 
bei der seltenheit des stadiums iiia ist dies eher unwahrscheinlich . der nachweis von pathologisch vergrerten lk wurde bei 15 % der patientinnen paraaortal beschrieben , aber nur bei 8 % pelvin , was die frage nach der qualitt der bildgebung aufwirdas berleben der 15 % patientinnen mit vermuteten paraaortalen lk - metastasen wird nicht berichtet , wre aber interessant zu wissen , da paraaortale metastasen mit fernmetastasen gleichgesetzt werden ( pm1lym )  . eingeschlossen wurde auch eine patientin mit einem neuroendokrinen tumor , die eine andere therapie bentigt htte . die onkologischen ergebnisse , insbesondere das os , decken sich mit den gepoolten daten der anfang 2000er - jahre [ 8 ]  . 
die aufgrund der hohen strahlendosen sehr gute lokale ( zervikale ) kontrolle setzt sich also hier nicht um in ein , im vergleich zu den erwhnten historischen vergleichen , verbessertes berleben . 
auch wurde kein operatives staging durchgefhrt , was die mitgeteilten ergebnisse positiv beeinusst htte . auerdem zeigen die patientinnen , die bereits im ct auffllige lk hatten , in der vorliegenden arbeit ein dramatisch schlechteres dfs als jene patientinnen mit bildgebend negativen lk . 
auch zu einer verbesserung beitragen knnen [ 1113 ]  . diese immer noch aktuelle diskussion einer bislang unbeantworteten frage wird von den autoren vllig ignoriert , htte aber zur vollstndigkeit beigetragen . 
wenn man die gute lokale kontrolle in der zervix den eher migen gesamtberlebensraten gegenberstellt , ist nach dem wirkpotential der systemtherapie bei den hochrisikopatientinnen zu fragen ; auch diesen aspekt vermisst man in der diskussion der arbeit vllig [ 1416 ]  . schlielich bleiben die indikationen fr eine interstitielle spickung unklar , zumal kein mrt zum beginn der bt durchgefhrt wurde . 
das kriterium large residual disease entspringt wahrscheinlich stark dem subjektiven eindruck des untersuchers , ist also untersucherabhngig unscharf . die berichteten toxizitten sind nur schwer einzuordnen , da weder planoptimierungskriterien noch dose constraints verraten werden . 
hier ak238 strahlenther onkol ( 2017 ) 193 : 236239 zeptieren die autoren dosen , die mit einem > 10%igen risiko fr eine toxizitt am rektum vom grad 24 korrelieren . 
hierauf wird von den autoren nicht eingegangen , auch nicht auf wichtige publikationen zur therapiebedingten toxizitt und deren diskussion [ 1820 ]  . verglichen werden die spttoxizitten mit einer frheren , fr den vergleich ungeeigneten publikation der eigenen arbeitsgruppe [ 2 ]  . 
diese daten sind nur insofern interessant , als sie im randomisierten vergleich keinen effekt der zustzlichen hyperthermie auf die lokale kontrolle , das dfs und das os zeigten . fazit die vorliegende arbeit suggeriert an einem eigentlich ungeeigneten patientenkollektiv , dass sich eine sehr gute lokale kontrolle beim lokal fortgeschrittenen zervixkarzinom auch mit einer ct - geplanten ( statt mrt - geplanten ) 3d - bt erzielen lsst . die hohen raten an fernmetastasen sind erwartungsgem von der soliden lokalen kontrollrate nicht berhrt . 
denn trotz aller oben besprochener mngel der vorliegenden arbeit muss man die homogene therapie von > 100 patientinnen pro jahr ( ! ) innerhalb eines einzelnen zentrums bewundern , in dem die rate an durchgefhrter simultaner chemotherapie vorbildlich und die bt - dosen sufzient waren . 
zolciak - siwinska a , piotrkowicz n , jonska - gmyrek j , nicke - psikuta m , michalski w , kawczynska m , bijok m , bujko k ( 2013 ) hdr brachytherapy combined with interstitial hyperthermia in locally advanced cervical cancer patients initially treated with concomitant radiochemotherapy a phase iii study . 
vrdoljak e , bodoky g , jassem j , popescu ra , mardiak j , pirker r , cufer t , beslija s , eniu a , todorovic v et al ( 2016 ) cancer control in central and eastern europe : current situation and recommendations for improvement . 
marnitz s , kohler c , rauer a , schneider a , budach v , tsunoda a , mangler m ( 2014 ) patterns of care in patients with cervical cancer 2012 : results of a survey among german radiotherapy departments and out - patient health care centers . 
lin jf , berger jl , krivak tc , beriwal s , chan jk , sukumvanich p , monk bj , richard sd ( 2014 ) impact of facility volume on therapy and survival for locally advanced cervical cancer . 
tergas ai , neugut ai , chen l , burke wm , hershman dl , wright jd ( 2016 ) radiation duration in women with cervical cancer treated with primary chemoradiation : a population - based analysis . 
beck t , sukumvanich p , rubatt j , beriwal s , zorn k , richard s , edwards r , krivak t ( 2010 ) impact of the national cancer institutes clinical announcement on cervical cancer survival . 
kohler c , mustea a , marnitz s , schneider a , chiantera v , ulrich u , scharf jp , martus p , vieira ma , tsunoda a ( 2015 ) perioperative morbidity and rate of upstaging after laparoscopic staging for patients with locally advanced cervical cancer : results of a prospective randomized trial . 
ramirez pt , jhingran a , macapinlac ha , euscher ed , munsell mf , coleman rl , soliman pt , schmeler km , frumovitz m , ramondetta lm ( 2011 ) laparoscopic extraperitoneal para - aortic lymphadenectomy in locally advanced cervical cancer a prospective correlation of surgical ndings with positron emission tomography / computed tomography ndings . 
hong dg , park ny , chong go , cho yl , park is , lee ys ( 2010 ) survival benet of laparoscopic surgical staging - guided radiation therapy in locally advanced cervical cancer . 
marnitz s , kohler c , roth c , fuller j , bischoff a , wendt t , schneider a , budach v ( 2007 ) stage - adjusted chemoradiation in cervical cancer after transperitoneal laparoscopic staging . 
marnitz s , kohler c , roth c , fuller j , hinkelbein w , schneider a ( 2005 ) is there a benet of pretreatment laparoscopic transperitoneal surgical staging in patients with advanced cervical cancer ? gynecol oncol 99 ( 3 ) : 536544 14 . 
duenas - gonzalez a , zarba jj , patel f , alcedo jc , beslija s , casanova l , pattaranutaporn p , hameed s , blair jm , barraclough h et al ( 2011 ) phase iii , open - label , randomized study comparing concurrent gemcitabine plus cisplatin and radiation followed by adjuvant gemcitabine and cisplatin versus concurrent cisplatin and radiation in patients with stage iib to iva carcinoma of the cervix . 
kim hs , kim mk , kim hj , han ss , kim jw ( 2012 ) phase ii study of consolidation chemotherapy after adjuvant or primary concurrent chemoradiation using paclitaxel and carboplatin to treat high - risk early - stage or locally advanced cervical cancer . 
tangjitgamol s , katanyoo k , laopaiboon m , lumbiganon p , manusirivithaya s , supawattanabodee b ( 2014 ) adjuvant chemotherapy after concurrent chemoradiation for locally advanced cervical cancer . 
georg p , potter r , georg d , lang s , dimopoulos jc , sturdza ae , berger d , kirisits c , dorr w ( 2012 ) dose effect relationship for strahlenther onkol ( 2017 ) 193 : 236239 late side effects of the rectum and urinary bladder in magnetic resonance image - guided adaptive cervix cancer brachytherapy . 
kirwan jm , symonds p , green ja , tierney j , collingwood m , williams cj ( 2003 ) a systematic review of acute and late toxicity of concomitant chemoradiation for cervical cancer . 
randomisiert wurden die patientinnen auf die alleinige adjuvante perkutane bestrahlung mit 48 , 6 gy oder die kombinationstherapie aus radiotherapie mit 2 simultanen gaben von cisplatin 50 mg / m2 und anschlieend 4 weiteren gaben von carboplatin / paclitaxel . 
 ( 2017 ) final results of the international randomized portec - 3 trial of adjuvant chemotherapy and radiation therapy ( rt ) versus rt alone for women with high - risk endometrial cancer . 
j clin oncol 35 ( 15_suppl ) : 55025502 ( prsentiert auf dem asco annual meeting 2017 ) ben ( overall survival , os ) und das failure - free survival ( ffs , deniert als berleben ohne rezidiv oder tumorbedingten todesfall )  . 
aus einer gemeinsamen analyse von 2 prospektiv randomisierten studien [ 3 ] , in denen sich ein signikant verbessertes progressionsfreies berleben und ein trend fr ein verbessertes os gezeigt hatte , gab es wiederum gute evidenz fr eine kombination von radiotherapie und chemotherapie , die in diesem fall sequenziell verabreicht worden war . 
in diesen studien wiesen aber nur gut 10 % der patientinnen ein endometriumkarzinom im stadium iii auf . auf der jahrestagung der american society of clinical oncology ( asco ) wurden parallel zu portec - 3 die ergebnisse der gog - 258 - studie prsentiert , die randomisiert die alleinige chemotherapie mit 6 zyklen carboplatin / paclitaxel mit dem identischen radiochemotherapie - regime aus portec - 3 verglich . 
welche schlsse lassen sich nun ziehen ? auf den ersten blick entsteht eine pattsituation , da die radiochemotherapie weder gegenber der alleinigen radiotherapie noch gegenber der alleinigen chemotherapie zu einer klaren verbesserung der ergebnisse fhrte . beide studien ( portec - 3 und gog 258 ) belegen jedoch eindrucksvoll die lokoregionre effektivitt der radiotherapie und festigen deren stellenwert . der effekt der chemotherapie auf die distanten rezidivraten war in beiden studien eher moderat . 
ber 60 % der patientinnen hatten nach 2 jahren noch beschwerden , die auf eine sensible polyneuropathie hindeuteten , 25 % litten unter strkeren beschwerden . unklar bleibt die frage , ob die simultane gabe von cisplatin zur bestrahlung und anschlieender verabreichung von 4 zyklen carboplatin / paclitaxel gegenber der bisher blichen und von onkologischer seite mglicherweise auch zuknftig favorisierten variante der alleinigen radiotherapie und anschlieender verabreichung von 6 zyklen carboplatin / paclitaxel zu bevorzugen ist . fazit die simultane und sequenzielle chemotherapiegabe zustzlich zur adjuvanten radiotherapie kann jungen und tten patientinnen mit endometriumkarzinom im stadium iii angeboten werden . 
de boer sm , powell me , mileshkin l et al ( 2016 ) toxicity and quality of life after adjuvant chemoradiotherapy versus radiotherapy alone for women with high - risk endometrial cancer ( portec - 3 ) : an open - label , multicentre , randomised , phase 3 trial . 
in this study , we compared toxicity proles following various radiation doses . patients and methods we reviewed the records of 60 patients who underwent tsebt for pctcl between 2000 and 2016 at the university hospital of munster . 
the treatment characteristics of the radiotherapy ( rt ) regimens and adverse events ( aes ) were then analyzed and compared . results in total , 67 courses of tsebt were administered to 60 patients . 
of these patients , 34 ( 51% ) received a standard dose with a median surface dose of 30 gy and 33 patients ( 49% ) received a low dose with the median surface dose of 12 gy ( 7 salvage low - dose tsebt courses were administered to 5 patients )  . 
after a median follow - up of 15 months , the overall ae rate was 100% , including 38 patients ( 57% ) with grade 2 and 7 ( 10% ) with grade 3 aes . 
multiple / salvage low - dose tsebt courses were not associated with an increased risk of acute aes . conclusion low - dose tsebt regimens are associated with signicantly fewer grade 2 acute toxicities compared with conventional doses of tsebt . 
repeated / salvage low - dose tsebt , however , appears to be tolerable and can even be applied safely in patients with cutaneous relapses . keywords palliative care salvage therapy adverse effects radiotherapy recurrence niedrigdosis - ganzhautelektronenbestrahlung bei patienten mit kutanen lymphomen minimales risiko fr akute toxizitten zusammenfassung fragestellung eine niedrigdosierte ganzhautelektronenbestrahlung ( tsebt ) wird vermehrt zur effektiven palliativen behandlung von patienten mit primr kutanen t - zell - lymphomen ( pctcl ) eingesetzt . 
insgesamt 34 patienten ( 51 % ) bekamen eine standarddosis mit einer medianen oberchendosis von 30 gy und 33 ( 49 % ) eine niedrigdosistsebt mit einer medianen oberchendosis von 12 gy strahlenther onkol ( 2017 ) 193 : 10241030 1025 ( insgesamt wurden 7 niedrigdosierte salvage - tsebts bei 5 patienten durchgefhrt )  . 
bei einer medianen nachbeobachtungszeit von 15 monaten betrug die gesamtwahrscheinlichkeit fr aes 100 % , darunter 38 patienten ( 57 % ) mit grad - 2und 7 patienten ( 10 % ) mit grad - 3 - aes . 
bei niedrigdosierter multipler / salvage - tsebt trat keine hufung von akuten aes auf . schlussfolgerung eine niedrigdosis - tsebt fhrt zu signikant weniger grad - 2 - toxizitten im vergleich zur tsebt in standarddosis . 
eine niedrigdosierte salvage - tsebt scheint nicht mit vermehrten nebenwirkungen verbunden zu sein und eine sichere therapieform bei kutanen rezidiven darzustellen . schlsselwrter palliative behandlung salvagetherapie unerwnschte ereignisse radiotherapie rezidiv background primary cutaneous t - cell lymphomas ( pctcl ) represent a rare subgroup of extranodal non - hodgkin lymphomas ( nhl )  . 
the management of advanced stages , however , remains a challenge [ 2 ]  . despite new advances in systemic and local therapy options that have been introduced in recent years , the treatment setting remains mostly palliative [ 3 ]  . total skin electron beam therapy ( tsebt ) is an important therapeutic option , especially in patients with extensive skin involvement and recurrent / refractory disease [ 46 ]  . 
interest in reduced - dose radiotherapy ( rt ) regimens for nhl has increased , particularly due to the short - term relief of symptoms and minimal toxicity proles that have been observed [ 1116 ]  . 
in this study , we investigate the toxicity prole of low - dose tsebt in comparison to the standard dose to provide evidence for treatment decisions in the future . materials and methods a total of 60 patients with pctcl underwent 67 tsebt courses at our institution between february 2000 and november 2016 . 
a modied six - dual - eld technique was used to deliver 61 radiation courses ( 91% )  . details of our treatment setup have been presented previously [ 3 ]  . 
boost or supplemental radiation ( range 239 gy ) was delivered to 59 / 67 patients ( 88% ) to compensate for underdosing in shadowed body areas or for treatment of large lymph nodes / tumorous lesions ; 8 patients did not receive additional radiation due to non - compliance or absence of tumorous lesions . 
seven salvage tsebt courses were administered to 5 patients with a median dose of 12 gy ( range 619.5 gy ) at a median interval of 6 months ( range 394 months ) after the initial tseb course . 
the median follow - up was 15 months ( range 1175 months )  . the overall ae rate was 100% , including 38 courses ( 57% ) with grade 2 and 7 ( 10% ) with grade 3 . 
in addition , skin infections were observed in 15% of patients during treatment ( 12% with the low dose versus 18% with the standard dose , p = 0.39 ) , which required antibiotics . 
during the follow up period , secondary cutaneous malignancies were experienced by 6 patients ( 9% ; squamous cell carcinoma n = 3 , basal cell carcinoma n = 2 , melanoma n = 1 )  . 
these days , however , low - dose tseb is becoming increasingly popular through its yielding of short - term remission of cutaneous manifestations with minimal toxicity ( table 3 )  . 
furthermore , higher recurrence rates can be compensated by salvage skin - directed or systemic therapies [ 3 ]  . a key aim of palliative therapy is to minimize toxicities while optimizing outcome . 
all patients report mild skin reactions compared to standard - dose regiments with a lower rate of grade 2 ( 33% low dose versus 79% standard dose ) and possibly fewer grade 3 toxicities ( 6 versus 15% )  . 
 [ 17 ] report two grade 3 toxicities ( 3% of the cohort ) following 12 gy tsebt , while kamstrup et al . [ 18 ] did not detect any grade 3 toxicity with 10 gy tsebt . in various studies , high infection rates ( reaching 31% ) have been reported with standard - dose tseb versus low - dose regimens [ 9 , 10 , 17 ]  . 
regarding secondary cutaneous malignancies , all patients in our cohort had undergone several skin - directed therapies before tseb ; thus , the diagnosis of secondary malignancies after tseb cannot be specically linked to radiation [ 24 ]  . tsebt repetition following standard - dose regimens is reported to be effective . 
e. , topical table 3 published studies of tsebt with reported toxicities patients ( n / total ) tsebt type ( total dose / fraction ) stage ( tnm ) previous treatments ae ( grades 3 / 4 ) 1028 published studies of ctcl morris et al . 2013 [ 9 ] lloyd et al . 2013 [ 10 ] median age ( years ) / gender 30 m , 11 f 53 m , 32 f elsayad et al . 2015 [ 22 ] 31 m , 14 f lindahl et al . 2011 [ 23 ] 23 m , 12 f kamstrup et al . 
however , the data presented are valuable because of the documentation of fewer aes and a greater degree of tolerability for lowdose tsebt . recently , novel agents and immunotherapies have emerged for mf / ss with an acceptable rate of remission ranging from 30 to 73% , but with a relatively high rate of moderate and severe aes [ 3 , 3034 ]  . 
a lower rate of grade 3 aes was also observed in patients receiving the low - dose regimen compared to conventional - dose schedules ; however this difference was not statistically signicant . 
repeated / salvage low - dose tsebt seems to be tolerable and can be applied safely in patients with cutaneous relapses without increasing acute toxicity . strahlenther onkol ( 2017 ) 193 : 10241030 compliance with ethical guidelines conict of interest k . 
eich declare that they have no competing interests . ethical standards all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
the univariate analysis showed that n stage < n2 , tn stage < iiia , r0 resection and n - ratio < 3 were statistically signicant prognostic factors for os and dfs , t stage < t4 for os and n - ratio < 3 for lfs . 
in the multivariate analysis , only r0 resection was statistically signicant factor for improved os ( cid : 2 ) mercedes martn snchez mercedes.martinsanchez@hotmail.com 1 department of radiation oncology , hospital universitario ramn y cajal , ctra . 
an r0 resection was an independent prognostic factor for improved os . keywords retrospective study survival prognosis toxicity disease free survival adjuvante radiochemotherapie beim lokal fortgeschrittenen magenkarzinom behandlungsergebnisse und analyse mglicher prognostischer faktoren zusammenfassung hintergrund und ziel das ziel dieser studie ist es , ber die klinischen ergebnisse und die toxizitt der adjuvanten radiochemotherapie bei lokal fortgeschrittenem magenkarzinom ( lfm ) entsprechend der intergroup - 0116 - studie in unserem krankenhaus zu berichten . methode es erfolgte eine retrospektive auswertung von 105 patienten mit lfm , welche mittels operation und adjuvanter radiochemotherapie behandelt wurden . 
wir analysierten das gesamtberleben ( os ) , das krankheitsfreie berleben ( dfs ) , das lokoregional freie berleben ( lfs ) sowie prognostische faktoren und toxizitt . ergebnisse die mediane beobachtungszeit betrug 96 , 48 monate . 
89 , 5 % der therapien konnten wie geplant abgeschlossen werden . schlussfolgerung unsere resultate zeigen , dass das berleben nach adjuvanter radiochemotherapie bei patienten mit lfm , welche in unserem institut behandelt wurden , vergleichbar war mit der intergroup 0116 . 
r0 - resektion war ein unabhngiger prognostischer faktor fr ein verbessertes os . schlsselwrter retrospektive studie berleben prognose toxizitt krankheitsfreie berleben introduction gastric cancer is the seventh most common tumor and the second most common cause of cancer - related death worldwide . 
according to the seer database , at the time of diagnosis , 27% of cases are conned to the primary site , 28% have lymph node involvement , 35% have metastases and 10% are unstaged . 
in this study , we aimed to evaluate the survival , prognostic factors and toxicity of the macdonald scheme in patients with locally advanced gastric cancer ( lagc )  . material and methods we retrospectively reviewed all the t3t4 or n + patients treated in our department in the period 20042014 . 
patients received 5 cycles of uorouracil ( 5 - fu ) and leucovorin with granulocyte colony - stimulating factor ( g - csf ) prophylaxis , according to clinical guidelines [ 4 ]  . 
treatment planning was done with oncentra tps ( elekta , sweden ) using a 3d conformal technique with a median of 4 elds of 6 and 18 mv photons and was administered using a primus linear accelerator ( siemens , germany )  . 
we used the kaplan - meier method to calculate 3 and 5 year os , dfs and locoregional failure - free survival ( lfs ) with 95% condence intervals ( ci )  . 
the most frequent complications were abdominal infections and wound dehiscence and 5 patients needed a second surgery to resolve the complication . the average duration of radiotherapy was 40.16 days ( ci 95% ; 3743 ) , 94 patients ( 89.5% ) started radiotherapy with a second cycle of chemotherapy and completed treatment as planned , 101 patients ( 95.2% ) completed the radiotherapy having been administered a total dose of 4500 cgy , 6 patients ( 5.7% ) started radiotherapy with a third cycle and four ( 3.8% ) with a fourth cycle . 
of the patients 5 received a different dose of radiotherapy ; 3 received 5040cgy for r1 resection and suboptimal lymphadenectomy , one received 5400cgy with 5 - fu and cisplatin for r1 and radiotherapy was stopped in one patient after 4140cgy due to thrombocytopenia . 
gastrointestinal toxicity was the most frequently seen ( mainly abdominal pain and diarrhea ) and was observed in 26.6% : grade i in 15 patients , grade ii in 8 patients , grade iii in 4 patients ( 1 dysphagia treated with botox 1 emesis , 1 diarrhea and 1 abdominal pain ) and grade iv in 1 patient who died due to gastrointestinal bleeding . 
recommendations. additionally , in the intergroup 0116 trial , the nal quality 1010 strahlenther onkol ( 2017 ) 193 : 10051013 assurance review ( conducted after the delivery of radiation ) revealed major deviations in 6.5% of the treatment plans . this , and the routine use of supportive medication in our institution , could explain our lower toxicity rates . most patients in the intergroup 0116 trial underwent suboptimal lymphadenectomy , with only 10% of patients having a d2 dissection . 
 [ 11 ] demonstrated that radiochemotherapy increased the recurrence free survival ( rfs ) by 14 months in d2 patients compared to chemotherapy alone , but it did not signicantly improved os . 
 [ 12 ] showed an improvement in lfs in stage iii patients by adding radiochemotherapy . a meta - analysis of 895 patients with d2 by huang et al . [ 13 ] demonstrated that adjuvant radiochemotherapy was superior to chemotherapy , for dfs and lfs . 
in 2014 another meta - analysis [ 14 ] included 6 studies with a total of 2135 patients to analyze the efcacy and safety of postoperative radiochemotherapy in patients with lagc and d2 . 
they concluded that adjuvant radiochemotherapy improved the 5 - year os and the 5 - year rfs . in our study 50 patients ( 47.6% ) had d2 but the os and dfs rates to 3 and 5 years were similar to the results of intergroup 0116 . 
 ( os 48% , dfs 45% ) , but lower than artist ( os 75% , dfs 75% )  . this may be due to the higher proportion of early stage patients ( 60% ibii ) in the artist trial . 
the question remains whether there is any difference between d1 and d2 . the dutch trial [ 15 ] compared d1 and d2 without adjuvant treatment ; after 15 years of follow - up , d2 did not improved os but it was associated with lower locoregional recurrence and fewer gastric cancer - related deaths than d1 ; however , d2 had signicantly higher postoperative mortality , morbidity , and reoperation rates . 
 [ 22 ] evaluated the impact of n - ratio and its interaction with n - category as a prognostic factor . they concluded that the relationship between n - category and n - ratio was a better predictor of survival than lymph node metastasis staging alone . 
in a retrospective study [ 25 ] of 53 patients using the same magic treatment protocol , the authors concluded that although 79% of patients had strahlenther onkol ( 2017 ) 193 : 10051013 1011 1012 strahlenther onkol ( 2017 ) 193 : 10051013 r0 resection , the protective effect of perioperative therapy was lost in patients with ypt34 and more than 4 positive lymph nodes . in other digestive locations , neoadjuvant radiochemotherapy is a standard treatment in patients with locally advanced disease . 
a recent meta - analysis [ 30 ] of 18 trials studied the benet of neoadjuvant radiochemotherapy in gastric and junctional cancer . the radiotherapy or radiochemotherapy improved survival compared to chemotherapy alone , with similar toxicity . 
although it seems that preoperative radiochemotherapy may be better than chemotherapy alone , stronger evidence , ideally from randomized trials is needed to appropriately compare both approaches . at this moment , there are two ongoing trials : critics [ 31 ] that compares perioperative chemotherapy to adjuvant radiochemotherapy and topgear [ 32 ] that compares perioperative chemotherapy to neoadjuvant radiochemotherapy . 
their reports can clarify what is the ideal treatment in patients with lagc . the limitations of our study include being a retrospective study with data from a single institution and inclusion of patients treated with 3drt , whilst at present , all patients are treated with imrt techniques to decrease gastrointestinal toxicity . 
additionally , chronic toxicity was unreported in 34% of patients , that can minimize our chronic toxicity results . conclusion in our study , adjuvant radiochemotherapy in patients with lagc demonstrated similar survival results than intergroup - 0116 but lower toxicity . r0 was an independent prognostic factor for improved os . 
september 2017 springer - verlag gmbh deutschland 2017 hintergrund die standardtherapie bei patienten mit rektumkarzinom im stadium iii gem union internationale contre le cancer ( uicc ) ist die neoadjuvante radiochemotherapie ( rct ) mit anschlieender kurativ intendierter tumorresektion mit totaler mesorektaler exzision ( tme ) , wobei mehr als 12 lymphknoten zu untersuchen sind . 
der nutzen einer dann folgenden adjuvanten chemotherapie ( ct ) wird kontrovers diskutiert , ist allerdings schon in der s3 - leitlinie der arbeitsgemeinschaft der wissenschaftlichen medizinischen fachgesellschaften ( awmf ) und der deutschen krebsgesellschaft ( dkg ) verankert . 
ziel der hier kommentierten retrospektiven auswertung war es , diese frage fr patienten mit rektumkarzinom im prtherapeutischen uicc - stadium iii und postoperativer ypn0 - kategorie zu lsen . patienten und methode die daten aller patienten mit rektumkarzinom aus 2 kliniken in frankreich und grobritannien , die prtherapeutisch ein cn + stadium und postoperativ ein ypn0 - stadium aufwiesen und im zeitraum von 1 / 2008 bis 12 / 2012 behandelt wurden , sind grundlage dieser retrospektiven analyse . 
die entscheidung fr eine adjuvante ct wurde jeweils im tumorboard getroffen , und wenn es als notwendig erachtet wurde , wurde 5 - fu und oxaliplatin appliziert . die patientengruppen ( ct ) wurden in bezug auf alter , pathologisches tumorstadium , r - status , grading und gefinvasion gematcht . primre studienendpunkte der studie waren die lokale kontrolle und die fernmetastasierung , sekundre studienendpunkte das geamtberleben ( overall survival , os ) und das krankheitsfreie berleben ( disease - free survival , dfs )  . ergebnisse fr die retrospektive auswertung wurden 124 patienten ohne und 39 patienten mit adjuvanter ct detektiert , nach dem matching wurden 80 patienten in die auswertung eingeschlossen , 52 ohne und 28 mit adjuvanter ct . 
bei 12 % der patienten war eine pathologische komplettremission ( pcr ) nach der rct eingetreten . in der gruppe ohne adjuvante ct trat im verlauf kein lokalrezidiv ( 0 / 52 ) auf , und in 8 / 52 fllen ( 15 % ) waren fernmetastasen zu verzeichnen im vergleich zu 2 / 28 ( 7 % ) lokalrezidiven und 6 / 28 ( 21 % ) fernmetastasen in der gruppe mit adjuvanter ct ( keine p - werte )  . 
bezglich des os ( p = 0 , 42 ) und des dfs ( p = 0 , 14 ) gab es keine statistisch signikanten unterschiede . schlussfolgerungen der autoren bei patienten mit einer ypn0 - kategorie nach neoadjuvanter rct verbessert eine adjuvante ct das dfs und os nicht . strahlenther onkol ( 2017 ) 193 : 10721073 1073 kommentar das ergebnis der studie ist fr die nichtinternistischen onkologen sicherlich nicht erstaunlich , weil es schon eine menge an studiendaten gibt , die keinen nutzen durch eine adjuvante ct bei patienten mit rektumkarzinom in der ypn0 - situation zeigen . 
immerhin wurde in der aktuellen auswertung eine matchedpair - analyse vorgenommen . eine auf eine leseranfrage hin durchgefhrte subgruppenanalyse der eortc22921 - studie einer 4 - armigen studie im 22 - design : radiotherapie ( rt ) vs . 
es kann also davon ausgegangen werden , dass die adjuvante ct mit oxaliplatin intensiviert wurde . damit ist das ergebnis der aktuellen analyse identisch mit den studienergebnissen von glynne - jones et al . 
wurden zwar sehr schnell nach ihrer ersten prsentation beim kongress der american society of clinical oncology ( asco ) hochrangig in lancet oncology publiziert , da hier eine intensivierte adjuvante ct mit folfox ( folinsure , 5 - fu , oxaliplatin ) im vergleich zu lediglich 5 - fu + folinsure das dfs und das os signikant verbesserte , bezogen auf 3 jahre nachbeobachtung . sieht man sich die ergebnisse aber genauer an , protieren von der ct nur die patienten , die postoperativ noch lymphknotenpositiv sind . 
beim vorliegen einer ypn0 - kategorie gab es keinen vorteil . fazit die indikation zur adjuvanten ct bei rektumkarzinompatienten , die postoperativ einen ypn0 - status aufweisen , muss trotz der anders lautenden empfehlungen in den leitlinien der dkg und awmf zurckhaltend gestellt werden . oder anders formuliert : beim rektumkarzinom wird nicht zu viel bestrahlt , sondern viel zu hug chemotherapiert . gunther klautke , chemnitz interessenkonikt g . 
fietkau r , barten m , klautke g et al ( 2006 ) postoperative chemotherapy may not be necessary for patiets with ypn0 - category after neoadjuvant chemoradiotherapy of rectal cancer . 
fietkau r , klautke g ( 2008 ) adjuvant chemotherapy following neoadjuvant therapy of rectal cancer : the type of neoadjuvant therapy ( chemoradiotherapy or radiotherapy ) may be important for selection of patients . 
glynne - jones r , kadalayil l , meadows hm et al ( 2014 ) chronicle : results of a randomized phase iii trial in locally advanced rectal cancer after neoadjuvant chemoradation randomizing postoperative adjuvant capecitabine plus oxaliplatin ( xelox ) versus control . ann oncol 25 : 13561362 4 . 
hong ys , nam bh , kim kp et al ( 2014 ) oxaliplatin , uorouracil , and leucovorin versus uorouracil and leucovorin as adjuvant chemotherapy fpr locally advanced rectal cancer after preoperative chemoradiotherapy ( adore ) : an open - label , multicenter , phase2 , randomized controlled trial . 
the aim of this study was to evaluate morbidity and survival outcome of simple adjuvant hysterectomy ( ah ) after ebrt / cct and to compare it with the standard treatment . patients and methods patients with figo stage iii cervical cancer were treated with ebrt / cct and then divided in two groups : group 1 was further treated with standard intracavitary / interstitial bt , while group 2 underwent ah . results from 881 women with cervical cancer , 248 were eligible for analysis : 161 received ibt and 87 underwent ah . the median follow - up of the study was 53 months . 
interestingly , pfs and dos were signicantly improved by ah for the patients with residual tumor . conclusion ah could improve survival in patients with residual disease after rct and is characterized by a low complication rate . keywords cervical cancer adjuvant hysterectomy concomitant chemotherapy intracavitary brachytherapy external beam radiation therapy adjuvante hysterektomie nach radiochemotherapie bei lokal fortgeschrittenem zervixkarzinom zusammenfassung hintergrund die teletherapie ( ebrt ) mit begleitender chemotherapie ( cct ) , entsprechend einer radiochemotherapie ( rct ) , plus intrakavitre ( interstitielle ) brachytherapie ( ibt ) ist standard in der behandlung des fortgeschrittenen zervixkarzinoms . 
ziel dieser studie war es , die morbiditt und das berleben zwischen der einfachen adjuvanten hysterektomie ( ah ) nach ebrt / cct und dem standardverfahren zu vergleichen . patienten und methoden patienten mit zervixkarzinom im figo - stadium iii wurden mit ebrt / cct behandelt und dann in zwei gruppen unterteilt : gruppe 1 wurde weiter mit der standardmigen intrakavitren / interstitiellen brachytherapie behandelt , gruppe 2 unterzog sich einer ah . ergebnisse von 881 frauen mit zervixkarzinom waren 246 fr die analyse geeignet : 161 erhielten eine ibt und 87 eine ah . 
interessanterweise waren das pfs und das dos fr die patienten mit resttumor durch die ah signikant verlngert . schlussfolgerungen die ah knnte das berleben von patienten mit residualtumor nach rct verbessern und ist durch eine geringe komplikationsrate gekennzeichnet . schlsselwrter zervixkarzinom adjuvante hysterektomie begleitende chemotherapie intrakavitre brachytherapie externe strahlentherapie introduction initially more than 50% of newly diagnosed cervical cancer is locally advanced [ 1 ]  . 
the treatment of choice for these patients is a combination of external beam radiotherapy ( ebrt ) with concomitant platinum - based chemotherapy , followed by intracervical interstitial brachytherapy ( ibt ) [ 2 , 3 ]  . 
recently published results from embrace and retroembrace trials impressively demonstrated the high efciency and compatibility of this strategy in relation to local and pelvic control with acceptable side effects [ 4 , 5 ]  . 
pelvic exenteration and radical hysterectomy are associated with an increased rate of complications without signicant improvement in patient survival [ 812 ]  . therefore , the use of simple adjuvant hysterectomy ( ah ) [ 13 ] after ebrt / cct has been questioned and its safety was investigated in a handful of trials with controversial results [ 11 , 1416 ]  . in this study , we compared ah with ibt in patients with advanced figo stage cervical cancer . 
the survival effect of both treatment utilities was investigated . patients and methods patients the cancer registry of saxony - anhalt , a federal state of germany , was reviewed in order to investigate all patients with cervical cancer treated between 2003 and 2011 . 
this tumor registry holds information on diagnosis , age at diagnosis , tumor stage , tumor grade , lymph node status , date of diagnosis , date of disease recurrence , date of death and the treatment regimens used [ 17 , 18 ]  . information on the date and cause of death is automatically entered into the system shortly after death . 
in this cohort study , we analyzed women with cervical cancer diagnosed between 2003 and 2011 in eight hospitals in saxony - anhalt ( three radio - oncological departments ) : university hospital magdeburg , harzklinikum dorothea christiane erxleben , johanniter clinic genthin - stendal , helios clinic burg , and the ameos clinics in aschersleben , halberstadt , haldensleben and schnebeck . 
in accordance with the statement of the research and ethical committee of the otto - von - guericke university , magdeburg , germany , additional individual consent for this analysis was not needed . 
the primary outcome measure was progression - free survival ( pfs ) and was dened as the time from the date of diagnosis to the time of recurrence , progress or death from disease . 
1 study design strahlenther onkol ( 2017 ) 193 : 10481055 881 patients assessed for inclusion 633 excluded 423 underwent primary surgery 124 received radiochemotherapy only 86 unknown stage 248 eligible for analysis radiochemotherapy 161 vaginal brachytherapy 87 adjuvant hysterectomy of diagnosis to the time of death from disease . 
follow - up ended with the patients death , last available information in the tumor registry or the last follow - up . treatment all patients received external beam radiation therapy ( ebrt ) to the whole pelvis , including the entire uterus , paracervical , parametrial and presacral regions and the regions of the pelvic lymph nodes combined with chemotherapy as a radiosensitizer . 
up until 2010 , chemotherapy was performed with 20 mg / m2 cisplatin and 1000 mg 5 - fu ( / m2 kof ) on days 15 in the 1st and 5th week of treatment . 
only patients for whom resection with negative surgical margins appeared possible were included in the study . the probable presence of residual tumor was estimated by clinical examination and magnetic resonance imaging ( mri )  . 
the ibt was performed as three - dimensional ( 3d ) conformal radiotherapy and classic bt ( up until 2008 ) image - guided brachytherapy ( igbt ) ( 20092012 ) and helical tomotherapy and image - guided adaptive brachytherapy ( igabt ) ( from 2012 )  . 
the statistical calculations were performed using spss version 22.0 ( spss , chicago , il , usa )  . the correlation of variables was assessed using the chisquare test or fishers exact test . 
of these patients , 633 were excluded from the analysis : 423 underwent primary surgery , 124 received radiochemotherapy only , and in 86 cases the stage of cervical cancer was unknown . 
the characteristics of cervical cancer such as figo stage , histological grade and type were equally distributed between the two groups ( table 1 )  . the characteristics of the surgical group are shown in table 2 . 
during the follow - up period , the rate of recurrence and metastases was 65 ( 40.3% ) and 27 ( 31.0% ) in the conservative and the surgical group , respectively ( table 3 )  . 
in the group of patients with denitive radiation therapy , locoregional recurrence was observed in 44 ( 27.3% ) patients , of whom 39 ( 24.2% ) had local recurrence and 5 ( 3.1% ) pelvic lymph node metastasis . 
to avoid further selection bias , a matching analysis was performed based on ve prognostic criteria : tumor stage , tumor histology , tumor grading , lymph and vascular space invasion and lymph node metastases . 
achieving complete response is believed to be crucial for patients survival , whereas residual tumor is associated with an increased level of local disease progression [ 6 , 7 , 14 ]  . 
since a surgical approach could improve the rate of pathological complete response , obtaining a complete resection of the tumor , adjuvant he could theoretically be advantageous in terms of local control and overall survival . the role of surgery has been investigated in a few studies with limited numbers of patients and a heterogeneous design . 
the log rank test was used to calculate the p - value . ibt interstitial brachytherapy , ah adjuvant hysterectomy hysterectomy with pelvic lymphadenectomy has been investigated in a number of retrospective studies . 
therefore , the use of radical hysterectomy has been questioned and the simple hysterectomy ( piver i ) after rct [ 13 ] has been suggested as an alternative . we found that ah is a feasible and safe method to treat patients with locally advanced cervical cancer after rct . this has been conrmed in further studies [ 11 , 1416 ]  . 
in comparison to the radical hysterectomy , the simple hysterectomy is associated with a signicantly reduced rate of complications [ 14 ] and is in accordance with our study , where radical hysterectomy was associated with a slightly increased complication rate compared with simple hysterectomy . 
in our study , only a few patients were treated with this relatively new approach and an adequate interpretation of the results is not plausible . 1054 strahlenther onkol ( 2017 ) 193 : 10481055 only in two studies was the use of ah associated with a signicant improvement in patient survival [ 16 , 22 ]  . 
in a second study with 256 patients with cervical cancer stage ib , it has been shown that ah improved the dfs rate after radiotherapy by 9% due to a reduced rate of local recurrence [ 22 ]  . 
notably , the study by keys and coworkers included only patients with ib2 tumors and they were treated only with radiation without any chemotherapy . these studies conrm the hypothesis that only patients with residual disease after rct could benet from surgical treatment [ 11 ]  . 
secondly , the survival benet of hysterectomy in the study by keys and co - workers was observed for tumors 56 cm and larger , which are per se associated with reduced pcr after rct [ 6 , 7 ]  . 
in contrast , patients with incomplete clinical and imaging response did not benet from thus , the identication of patients with residual tumor should be the major goal of further investigations . 
although the negative predictive value of mri after rct is 96% with excellent prediction of pcr , the positive predictive value of the method for residual disease is very poor at an estimated 15% [ 25 ]  . 
however , the positive and negative predictive values , as well as the specicity and sensitivity of cervical biopsy after rct have not been investigated as yet . a prospective randomized trial comparing ah with ibt for advanced cervical cancer after rct is being planned at our institution . 
to detect an improvement in pfs from 51% in the group of patients treated with additional ibt up to 68% in the surgery group [ 8 , 11 , 12 , 14 , 16 , 22 , 28 ] , with 80% statistical power and 5% signicance level , we determined our sample size to be at least 130 patients per treatment group . 
secondary outcomes include os , sensitivity and specicity of cervical biopsy to detect patients with residual tumor after rct , complications and quality of life . one limitation of our study is its retrospective nature with consequent selection and treatment bias . 
all procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and / or national research committee and with the 1964 helsinki declaration and its later amendments or comparable ethical standards . 
fr die studie wurden monozentrisch am md anderson cancer center 132 patienten 1 : 1 in einen beobachtungsarm mit 69 wchentlichen mrt - aufnahmen und einen behandlungsarm mit einer radiochirurgie der resektionshhle ( n ) randomisiert . 
dosiert wurde am gammaknife wie gewhnlich auf die 50% - isodose . ein planungszielvolumen ( planning target volume , ptv ) bis 10 cm3 erhielt 16 gy , ein ptv von 10 , 115 cm3 erhielt 14 gy und ein ptv > 15 cm3 erhielt 12 gy . der primre endpunkt der studie war die lokale kontrolle im bereich der vollstndig resezierten metastasen . sekundre endpunkte waren das auftreten weit entfernt liegender hirnmetastasen sowie das gesamtberleben . 
durch die radiochirurgie der resektionshhle lie sich die lokale kontrolle verdoppeln : die rate der lokalrezidive betrug 24 % im rc - arm und 48 % im beobachtungsarnach 12 monaten waren 43 % der patienten im kontrollarm und 72 % im rc - arm lokalrezidivfrei ( p = 0 , 015 )  . 
besonders gut war die lokale kontrolle , wenn die lsion kleiner als 2 , 5 cm war , denn in diesen fllen lag die lokalkontrolle nach 12 monaten bei 77 % im beobachtungsarm und bei 100 % im rc - arm . fr metastasen zwischen 2 , 5 und 3 , 5 cm war die lokale kontrolle median und nach 12 monaten nicht signikant unterschiedlich , fr metastasen ber 3 , 5 cm bestand eine lokale kontrolle nach 12 monaten nur in 22 % der beobachteten flle , verglichen mit 72 % der mit einer rc behandelten patienten . 
auerdem wurde die intrakranielle tumorkontrolle von der anzahl der metastasen beeinusst , wobei patienten mit 3 metastasen ein 3 - fach hheres risiko fr einen progress hatten als patienten mit nur einer metastase . 
da keinerlei nebenwirkungen der rc auftraten und die lokale kontrolle insbesondere bei op . - hhlen > 2 , 5 cm relativ gering waren , sollten hhere dosen verwendet werden . kommentar als ergebnis der arbeit von mahajan sowie der nahezu zeitgleich publizierten daten der n107c - studie von brown et al . 
beide arbeiten decken zusammen ein groes spektrum der adjuvanten behandlungsoptionen ab , von der alleinigen beobachtung ber die intensivierte lokaltherapie bis hin zur intensivierten lokaltherapie in kombination mit einer ghrt . 
ohne weitere lokaltherapie liegt die rezidivrate nach kompletter resektion der hirnmetastasen bei etwa 50 % , bei der kombination einer lokalen dosisintensivierung und einer radiochirurgie der op . - hhle inklusive aller weiteren metastasen aber trotz ggf . 
wertet man die lokale kontrolle als messlatte des therapieerfolgs , so wre also die entscheidung fr eine hochdosierte rc der tumorregionen in kombination mit einer ghrt die optimale behandlung . ist aber die intrakranielle tumorkontrolle gerade vor dem hintergrund sehr effektiver salvage - therapien berhaupt der richtige endpunkt ? schlielich ergaben alle 3 behandlungsoptionen , von der beobachtung bis zur kombination aus rc und ghrt , die gleiche berlebenschance . mutmalich ist das deshalb der fall , weil die effektivitt der salvage - behandlungen die nachteile der anfnglichen zurckhaltung bei der therapie ausgleichen kann und somit verhindert , dass unterschiede in der initial erzielten lokalen kontrolle einen einuss auf das gesamtberleben haben . 
das war nun der fall , womit die bereits im jahr 2016 von derselben arbeitsgruppe verffentlichten daten zur behandlung von 13 metastasen mit der radiochirurgie und anschlieender ghrt besttigt wurden [ 2 ]  . 
einen weiteren beleg dafr , dass der initiale verzicht auf eine ghrt beim vorliegen von 13 metastasen nicht nachteilig fr die patienten ist , liefert eine metaanalyse von patientendaten aus 3 randomisierten phase - iii - studien . 
die autoren beschrieben dabei sogar , dass das gesamtberleben in der subgruppe von unter 50 - jhrigen patienten durch die ghrt wiederum trotz besserer lokaler kontrolle verschlechtert sein knnte [ 3 ]  . 
diese erscheint in der studie sowieso recht gering , denn die biologische quivalenzdosis ( bed ) liegt unter der annahme eines / - werts von 10 nur zwischen 41 , 6 und 26 , 4 gy . 
umgekehrt sorgt der steile dosisgradient bei einer auf die 50% - isodose verschriebenen dosis fr eine nur minimale bestrahlung des benachbarten hirnparenchyms , was sich positiv in den kaum vorhandenen nebenwirkungen zeigt . 
zu steilen dosisgradienten der radiochirurgie . die konsequenz daraus sollte sein , das zielvolumenkonzept und die dosierung der rc zu berdenken , da durch die optimierung beider faktoren sicher eine noch bessere lokale kontrolle mglich ist ohne zustzliche nebenwirkungen . 
in mnchen haben wir gute erfahrungen mit einer hypofraktionierten stereotaktischen strahlentherapie der resektionshhle gemacht , bei der 2 mm des parenchyms um die resektionshhle als klinisches tumorvolumen ( ctv ) deniert werden . 
nach einer subtotalen resektion 35 gy erhielten und eine lokale kontrolle von 90 % erlebten [ 5 ]  . fazit nach der resektion von 13 metastasen im gehirn ist eine kognitiv u . 
da hoch wirksame salvage - therapien zur verfgung stehen , ist die lokale kontrolle nicht das alleinige ma aller dinge , sondern muss im kontext der gesamtprognose und der zu erwartenden nebenwirkungen gesehen werden . christoph straube und stephanie e . 
brown pd , ballman kv , cerhan jh , anderson sk , carrero xw , whitton ac et al ( 2017 ) postoperative stereotactic radiosurgery compared with whole brain radiotherapy for resected metastatic brain disease ( ncctg n107c / cec3 ) : a multicentre , randomised , controlled , phase 3 trial . 
brown pd , jaeckle k , ballman kv , farace e , cerhan jh , anderson sk et al ( 2016 ) effect of radiosurgery alone vs radiosurgery with whole brain radiation therapy on cognitive function in patients with 1 to 3 brain metastases : a randomized clinical trial . 
sahgal a , aoyama h , kocher m , neupane b , collette s , tago m et al ( 2015 ) phase 3 trials of stereotactic radiosurgery with or without whole - brain radiation therapy for 1 to 4 brain metastases : individual patient data meta - analysis . 
specht hm , kessel ka , oechsner m , meyer b , zimmer c , combs se ( 2016 ) hfsrt of the resection cavity in patients with brain metastases . 
bilger a , milanovic d , lorenz h , oehlke o , urbach h , schmucker m et al ( 2016 ) stereotactic fractionated radiotherapy of the resection cavity in patients with one to three brain metastases . 
von 1970 bis 1999 arbeitete er schlielich als professor und direktor des neu gegrndeten departments of therapeutic radiology in minneapolis . levitt bildete 70 residents in radiotherapie aus , die teilweise auch leitende positionen einnahmen , und verffentlichte ein ganz praktisch ausgerichtetes lehrbuch , the technical basis of radiation therapy , was sehr erfolgreich war und in 4 auagen erschien . 
besonders wissenschaftlich und berufspolitisch engagiert war levitt auf den gebieten des mammakarzinoms und des prostatakarzinoms . hier ging es darum , die bedeutung der radiotherapie in der kompetition mit radikaloperationen und der chemotherapie zu denieren . 
ab 2002 wirkte er 12 jahre lang als wissenschaftlicher berater am karolinska institut in stockholzahlreiche mter bekleidete er in der radiological society of north america ( rsna ) , in der american society of therapeutic radiology ( astro ) , in der american radium society sowie als direktor der american cancer society , meistens sogar als prsident . levitt erhielt in den usa , in schweden und china zahlreiche auszeichnungen . 
levitt prgte ende der 50er / anfang 60er - jahre die entwicklung der klinischen radioonkologie als eigenstndiges fach nicht nur in den usa , was fr uns seinerzeit mageblich war , sondern eben auch in deutschland , sterreich und schweden durch mancherlei persnliche kontakte . 
aebersold1 roland giger2 olgun elicin1 received : 30 november 2016 / accepted : 7 april 2017 / published online : 4 may 2017 springer - verlag berlin heidelberg 2017 abstract background the optimal treatment strategy for stage iii glottic squamous cell carcinoma ( scc ) is not well - dened . this study analyzed treatment results and prognostic factors . patients and methods this is a single - institution retrospective analysis of 244 patients with t12 glottic scc who underwent normofractionated radiotherapy ( rt ) and / or surgery between 1990 and 2013 . 
the primary endpoint was relapse - free survival ( rfs )  . results median age was 65 years ( range : 3692 years ) , the majority ( 82% ) having stage i disease . 
in dieser studie wurden behandlungsergebnisse und prognostische faktoren untersucht . patienten und methoden in dieser retrospektiv unizentrischen studie wurden 244 patienten mit einem frhen glottis - scc ( t12 ) zwischen 1990 und 2013 strahlentherapeutisch ( rt ) und / oder chirurgisch behandelt . 
therefore , the treatment aim of laryngeal cancer is not only achievement of maximum disease control , but also maintenance of function . in the absence of large randomized studies providing clear evidence for the best strategy to treat early stage glottic scc , many retrospective studies reported comparable control rates following radiotherapy ( rt ) and / or surgery . 
the 5 - year lc with transoral laser microsurgery is in the order of 82 to 100% for t1 and 66 to 88% for t2 tumors , which is comparable to the results of open partial laryngectomy [ 57 ]  . 
in this regard , no signicant differences between surgery and rt are expected [ 8 ]  . the aim of this retrospective single - institution study was to assess the oncologic outcome and inuencing factors in treatment of stage i and ii ( union for international cancer control , uicc ) glottic scc with a sufcient follow - up period . patients and methods approval of institutional and regional review boards was obtained . 
the charts of all patients presented in our head and neck cancer multidisciplinary tumor board between 1990 and 2013 with histologically proven t1 and t2 invasive purely glottic scc were reviewed . 
staging was revised according to the 7th edition of the uicc staging system . patients with preexisting neoplastic disease were excluded . treatment decisions were discussed by board members to determine the best strategy to preserve laryngeal function in the absence of a protocol with any predened selection criteria . 
the patients either received denitive rt alone or underwent surgery . radiotherapy was delivered using a two - dimensional conventional or three - dimensional conformal technique ( 2d / 3d - rt ) in the majority of the cases , which was followed by an era of intensity - modulated radiotherapy ( imrt )  . 
denitive rt to a total dose of 72 gy was delivered in 2 gy per fraction to the larynx in t2 tumors . the remaining cases ( t1 denitive or t1 / 2 adjuvant ) were treated to 68 gy . 
a two - sided log - rank test was used to evaluate possible prognostic factors such as age , gender , stage , anterior commissure involvement ( aci ) , rt treatment time , and treatment modality for relapse - free survival ( rfs )  . 
table 1 summarizes the patient , disease , and treatment characteristics . the 5 - year overall survival ( os ) , cause - specic survival ( css ) , and rfs rates for the whole cohort were 92 , 96 , and 78% , respectively . 
all laryngectomies were performed as salvage surgery and not due to functional deterioration . discussion the main objective of this study was to report the outcome of stage iii glottic scc patients treated by our multidisciplinary hnc team and to identify possible factors which may inuence the outcome . 
 [ 11 ] , where the primary endpoint was voice quality . the trial was stopped after 10 years due to low accrual , with only 20% of the planned sample size reached . 
the patterns of relapse and subsequent treatments are shown in table 3 . a second primary cancer developed in 30 patients ( 12% ) , of which 10 were diagnosed as head and neck cancer ( hnc ) , all being scc , and 22 as non - hnc ( two patients had both )  . 
dots represent censored patients lost to follow - up ; rt radiotherapy , s surgery in the absence of prospective randomized trials , a variety of meta - analyses and systematic reviews were published comparing rt to surgery with various methodologies and ndings . 
in a meta - analysis including 27 studies comparing rt to laser microsurgery , no signicant difference in oncologic outcome , but a trend toward improved voice quality following rt was reported [ 12 ]  . 
similarly , another systematic review and meta - analysis included 19 studies with t1a glottic larynx cancer showed no signicant differences in lc , os , disease - specic survival , or voice quality following rt or surgery [ 13 ]  . 
showed in a meta - analysis that laser surgery delivered signicantly better os and laryngeal preservation than rt in t1 primaries , without , however , signicant differences in lc in t1 tumors , which puts a question mark on the quality of the analysis concerning patient selection bias [ 15 ]  . 
similarly , a recent surveillance , epidemiology , and end results ( seer ) data analysis showed superior os with surgery over rt without reporting any lc or disease - specic outcome rates [ 16 ]  . 
a recent systematic review of lc outcomes explicitly for t2 glottic tumors treated with either rt or laser surgery didnt show any difference in 5 - year lc between the two treatment groups [ 17 ]  . 
the last update of the cochrane review on this topic showed no signicant differences in 5 - year os or disease - free survival in stage i and ii glottic scc with rt or surgery [ 8 ]  . 
this may be explained by our previous institutional policy apparently favoring rt over surgery in early - stage laryngeal cancer , not only as the rst treatment hier steht eine anzeige . 1002 strahlenther onkol ( 2017 ) 193 : 9951004 option but also in cases of close and positive resection margins , which underwent a major change few years ago . altered fractionation with shorter overall treatment times corresponds to better tumor control and survival benet in hnc [ 1823 ]  . 
on the other hand , contrary to what was expected , radiation therapy oncology group ( rtog ) 9512 showed increased toxicity and futility with hyperfractionation in t2 glottic larynx cancer [ 26 ]  . 
in our cohort , this observation could not be reproduced , probably due to the fact that the majority of the patients were treated once daily and rt time was normally distributed , with a prominent accumulation around the median value of 49 days . 
the outliers were patients whose treatments were either arbitrarily accelerated or delayed for various reasons . in our series , all patients in stage ii received elective nodal irradiation to the levels iiiv bilaterally . 
some retrospective studies demonstrated that aci is a poor prognostic factor for rt outcomes [ 2832 ] , but these results are not consistent in the literature [ 7 ]  . 
however , patients treated with imrt represented only 15% of our whole cohort . while imrt is known to be used for its general benets in terms of decreasing toxicity in the treatment of laryngeal cancer [ 34 ] , the still widely used approach for earlystage glottis scc is to treat the whole larynx as a compartment . 
with a newer technique developed by the rotterdam group , it is possible to apply 58.08 gy in 16 fractions just to the involved vocal cord , with a signicant dose reduction in the vicinity [ 40 ]  . 
this observation is consistent with results of another analysis of 987 laryngeal cancer patients treated between 1967 and 2004 , where rt was not found to increase the risk of second primary tumor incidence [ 45 ]  . 
in our study , 12% of patients developed a second primary cancer with a non - signicant increase in patients treated denitively or adjuvantly with rt ( rt 22% ; surgery only 9% )  . 
however , our median follow - up of 5 years is not enough to observe any meaningful difference or exclude the long - term possibility of an increased incidence of second malignancies in any of the treatment groups . 
furthermore , the hypothesis regarding ablation of the premalignant foci with rt may be invalid or less prominent in the imrt era , and if still present , this effect might be limited in the treatment of early glottic scc , where elective nodal irradiation is often omitted . our present study has limitations due to its retrospective nature , which predisposes the results to potential bias . 
additionally , due to its retrospective nature , we were not able to report on toxicities , smoking and alcohol consumption status . conclusion our series demonstrate a better rfs with rt compared surgery for stage i glottic scc with a given risk of possible selection bias . 
kaanders1 published online : 27 october 2017 springer - verlag gmbh deutschland 2017 correction to : strahlenther onkol 2017 unfortunately , parts of the materials and methods section and a sentence in the discussion section had to be corrected . on page 3 , left column , the complete rst paragraph was corrected and now reads as follows : auto - planning is fully integrated into pinnacle v.9.10 tps to automate the inverse planning process [ 1113 ]  . on page 3 , left column , the complete third paragraph was corrected and now reads as follows : thus , auto - planning is designed to automatically perform many of the manual operations in the imrt planning process . on page 3 , right column , second paragraph to page 4 left column , rst paragraph , the complete section was corrected and now reads as follows : table 2 shows the auto - planning optimization preset used for the patients in this study . 
in this region , the auto - planning tool makes stronger attempts to reduce dose . the hot - spot maximum goal can be set as a percentage with respect to the maximum prescribed dose to the target and will be used to reduce the maximum dose of hotspots in the target . 
by selecting use cold - spot rois , the autoplanning tool creates rois for any cold spots lower than the prescribed dose within the target and creates objectives for those cold - spot rois to further optimize the target dose coverage . 
the conventional weight factors in pinnacle can not been set in the auto - planning tool and priority of the goal can be set by low , medium or high . 
with compromise set to yes the overlapping region of an oar with a target will be assigned to the target . on page 4 , left column , the complete second paragraph was corrected and now reads as follows : the auto - planning tool can automatically adjust the priority values of oar optimization goals based on roi overlap statistics . 
if the roi used in an oar optimization goal substantially overlaps any targets , the auto - planning tool lowers its priority . 1078 strahlenther onkol ( 2017 ) 193 : 10771078 in the discussion section on page 6 , right column , the second paragraph was corrected and now reads as follows : to get the auto - planning optimization preset , a certain amount of effort has to be made to nd the optimal setting for the objectives . 
combs1 , 2 , 4 received : 7 april 2017 / accepted : 28 july 2017 / published online : 14 august 2017 springer - verlag gmbh deutschland 2017 abstract background and purpose high - precision radiotherapy ( rt ) requires precise positioning , particularly with high single doses . 
the purpose of this study is to establish a pancreatic cancer mouse model for high - precision image - guided rt ( igrt ) using the liquid ducial marker bioxmark ( nanovi , kongens lyngby , denmark )  . methods in an animal - based cancer model , different volumes of bioxmark ( 1050 l ) , application forms , and imaging modalitiescone - beam computer tomography ( cbct ) incorporated in either the small animal radiation research platform ( sarrp ) or the small - animal micro - ct scanner ( skyscan ; bruker , brussels , belgium ) as well as subsequent rt with the sarrp system were analyzed to derive recommendations for bioxmark . results even small volumes ( 10 l ) of bioxmark could be detected by cbct ( sarrp and skyscan )  . 
bioxmark enabled an exact fusion with the original treatment plan with less hardening artefacts , and minimized the application of contrast agent for fractionated rt . conclusion an orthotopic pancreatic tumor mouse model was established for high - precision igrt using a ducial marker . 
bioxmark was successfully tested and provides the perfect basis for improved imaging in high - precision rt . bioxmark enables a unique application method and optimal targeted precision in fractionated rt . 
therefore , preclinical trials evaluating novel fractionation regimens and / or combination treatment with high - end rt can be performed . keywords models , animal cone - beam computed tomography pancreatic neoplasms dose fractionation radiotherapy , image - guided bioxmark fr die hochprzisionsstrahlentherapie im orthotopen pankreastumor - mausmodell erfahrungen mit einem liquiden marker zusammenfassung hintergrund und zielsetzung die hochprzisionsstrahlentherapie ( rt ) erfordert insbesondere bei hohen einzeldosen eine exakte lagerung . 
ziel dieser arbeit ist die etablierung eines prklinischen tumormausmodells zur bildgesttzten strahlentherapie ( igrt ) des pankreaskarzinoms unter verwendung des liquiden markers bioxmark ( nanovi , kongens lyngby , dnemark )  . 1040 strahlenther onkol ( 2017 ) 193 : 10391047 methoden in einem tierbasierten tumormodell wurden verschiedene volumina von bioxmark ( 1050 l ) , injektionsformen , bildgebungsmodalitten kegelstrahl - computertomographie ( cbct ) integriert in sarrp ( small animal radiation research platform ) und kleintier - mikro - ct ( skyscan , bruker , brssel , belgien ) sowie die anschlieende rt mittels sarrp analysiert , um daraus empfehlungen fr bioxmark abzuleiten . ergebnisse selbst kleine volumina ( 10 l ) von bioxmark lieen sich im cbct ( sarrp und skyscan ) detektieren . grere volumina ( 50 l ) fhrten zu milden artfakten . 
bioxmark ermglicht artefaktarm die zielgenaue fusion mit dem ursprnglichen bestrahlungsplan und minimiert die verabreichung von kontrastmittel bei fraktionierter rt . schlussfolgerung erstmalig wurde ein orthotopes pankreastumor - mausmodell fr eine hochprzisions - igrt mit liquiden markern etabliert . 
bioxmark erlaubt eine einzigartige applikationsweise und optimale zielrichtung bei der fraktionierten rt . dadurch knnen prklinische experimente zur evaluation neuer fraktionierungsschemata und / oder kombinationsbehandlungen mit high - end - rt durchgefhrt werden . schlsselwrter tiermodelle cone - beamcomputertomographie pankreasneoplasien dosisfraktionierung bildgesttzte strahlentherapie pancreatic cancer is one of the most lethal human cancers and the fourth most common cause of death in the united states [ 1 , 2 ]  . 
the overall 5 - year survival rate among patients with pancreatic cancer is still very poor at less than 5% [ 3 ] , and only modest improvement has been seen over the last decade despite extensive research . therefore , novel concepts are urgently required . 
clinical data show that at least one third of patients , predominantly with locally advanced but irresectable lesions , benet from local radiotherapy ( rt ) [ 4 , 5 ]  . 
however , few data are available on biomarkers for individual treatment stratication . novel rt devices for high - precision rt in an animal model provide a unique basis to transfer clinical high - precision concepts into the preclinical setting , allowing further assessment of novel rt concepts . 
rt was unfocussed and generally treated the whole mouse or at least the whole mouse abdomen , which led to signicant toxicity and did not reect possibilities present in human cancer treatment . only recently , small imaging and rt devices have been developed : high - precision rt comparable to patients treatment can be achieved . 
at our center , we are equipped with the possibility of performing high - precision rt in animalbased tumor models with the small animal radiation research platform system ( sarrp ; xstrahl , camberley , uk ) [ 6 ]  . 
to date , for animal experiments , no mouse models exist providing the precision of imaging , positioning , and treatment comparable to patient treatments . as ct imaging is not the gold standard for imaging of orthotopic pancreatic tumors , intravenous injection of iodinecontaining contrast agent and the liquid ducial marker bioxmark was used for improved imaging and rt . 
data on bioxmark use in the preclinical setting are lacking so far ; these are available in clinical settings only . for the rst time , an orthotopic pancreatic tumor mouse model was established for image - guided high - precision rt with a ducial marker . 
the present study aims to evaluate bioxmark in imageand planning - related settings ( contouring , fusion ) for high - precision rt in an orthotopic pancreatic tumor mouse model . materials and methods cell line line panc - 1 was the human pancreatic carcinoma cell obtained from the american type culture collection ( atcc ; manassas , va , usa )  . 
panc - 1 cells were cultured in rpmi 1640 medium supplemented with 10% fetal bovine serum ( fbs ) , 100 u / ml penicillin , and 100 g / ml streptomycin ( invitrogen gmbh , karlsruhe , germany ) at 37 c in a humidied 5% co2 atmosphere under sterile conditions . orthotopic tumor model all animal procedures were ofcially approved in accordance with the german law governing the care and use of laboratory animals . 
all procedures were authorized by the regional government of upper bavaria , germany ( reference 55.2 - 1 - 54 - 2532 - 217 - 2015 )  . strahlenther onkol ( 2017 ) 193 : 10391047 1041 an orthotopic pancreatic tumor mouse model with the cell line panc - 1 was established in 6 - week - old immunosuppressed cd - 1 nude mice ( crl : cd1 - foxn1nu ; charles river laboratories , sulzfeld , germany )  . 
for this purpose , mice were anesthetized with an intraperitoneal injection of a combination of medetomidine 0.5 mg / ml , midazolam 5 mg / ml , and fentanyl 0.05 mg / ml ( mmf ) per 1 kg mouse body weight , which was fully antagonized with a subcutaneous injection of atipamezole 2.5 mg / ml , umazenil 0.5 mg / ml , and naloxone 1.2 mg / ml ( afn ) after the complete surgical procedure . 
wound healing , body weight , behavior , and physical condition of the mice were monitored at least twice a week over the total experimental time . bioxmark the sterile liquid ready - to - inject ducial marker bioxmark was provided from nanovi a / s ( kongens lyngby , denmark )  . 
various volumes ranging from 10 to 50 l of bioxmark were injected through a 26 - gauge needle using three different methods under sterile conditions : method 1 : injection of bioxmark into the pancreatic tissue close to the injected tumor cells during laparotomy . method 2 : resuspension of bioxmark together with the tumor cells in the same syringe and injection into pancreatic tissue during laparotomy . method 3 : injection of bioxmark directly into the orthotopic tumor after a tumor growth of 6 to 8 weeks . imaging modalities after tumor growth for about 6 to 8 weeks , two different imaging modalitiescone - beam computed tomography ( cbct ) incorporated in either the sarrp system or the the small - animal micro - ct scanner ( skyscan 1190 in absorption mode , bruker , brussels , belgium ; [ 8 ] ) were used for analysis of bioxmark . 
injection of imeron 300 were compared . irradiation : sarrp high - precision irradiation was performed with sarrp , which represents a well - suited technology with its image guidance rt setup and broad range of applicable doses . sarrp allows exact anatomical targeting with delivery of beams down to 0.5 mtreatment planning and delivery including arc or complex beam techniques simulates the clinical situation in oncology departments around the world for the rst time . 
radiation was delivered at 220 kv and 13 ma . single - dose stereotactic body rt of 25 gy and fractionated treatment regimens of up to 30 fractions of 2 gy with an overall dose of 60 gy were compared . 
irradiation was performed in an arc technique with a gantry angle between 178 and 178 using a 5 5 mm2 or 10 10 mm2 collimator depending on the tumor size . 
mice were immobilized with inhaled isourane anesthesia at a concentration of 1.5% with 6% of the volume oxygen as carrier gas during the whole procedure of imaging , treatment planning , and highprecision irradiation . results evaluation of application technique and marker volume the handling of bioxmark proved simple and uncomplicated , although its high viscosity requires intensive practice and very precise injection of only small volumes in preclinical mouse tumor models . various methods of marker application into the target tissue were tested . 
1 comparison of different volumes of bioxmark ( nanovi , kongens lyngby , denmark ) and methods of injection in cone - beam computed tomography ( cbrt ; small animal radiation research platform , sarrp ) imaging after i . 
injection of imeron ( bracco imaging gmbh , konstanz , germany )  . a injection of 20 l bioxmark into the pancreatic tissue during laparotomy ( method 1 ) ; b injection of 50 l bioxmark into the pancreatic tissue during laparotomy ( method 1 ) ; c injection of 10 l bioxmark into the orthotopic tumor ( method 3 ) ; d injection of 50 l bioxmark within and directly adjacent to the orthotopic ( method 3 ) fig . 
3 comparison of cone - beam computed tomography ( cbct ; small animal radiation research platform , sarrp ) images , method 3 . a cbct ( sarrp ) native ; b cbct ( sarrp ) after injection of the iodine - containing contrast agent imeron ( bracco imaging gmbh , konstanz , germany ) fig . 
4 hardening artefacts of bioxmark ( nanovi , kongens lyngby , denmark ) at 50 l bioxmark in native cone - beam computed tomography ( cbct ; small animal radiation research platform , sarrp ) imaging , method 1 . 
a axial image , cbct ( sarrp ) ; b coronal image , cbct ( sarrp ) ; c sagittal image , cbct ( sarrp ) irradiation and weekly monitoring bioxmark was evaluated for its potential for three - dimensional irradiation treatment planning in arc technique using sarrp either performed as stereotactic rt in one single dose or as fractionated rt . injection of bioxmark directly into the orthotopic tumor according to method 3 helped to dene the target volume and allowed the irradiation beam to be guided . bioxmark enabled an exact , unique reproducible fusion with the original treatment plan and minimized the application of contrast agent in the fractionated high - precision rt setting , especially in fractionated stereotactic body rt ( sbrt )  . 
5 stability of bioxmark ( nanovi , kongens lyngby , denmark ) in cone - beam computed tomography ( cbct ; small animal radiation research platform , sarrp ) imaging after irradiation , method 3 . 
6 stability of bioxmark ( nanovi , kongens lyngby , denmark ) over 4 months in cone - beam computed tomography ( cbct ; small animal radiation research platform , sarrp ) imaging , method 1 . 
a cbct ( sarrp ) ; b cbct ( sarrp ) after 2 months ; c cbct ( sarrp ) 4 months the sarrp platform together with a ducial marker . 
therefore , preclinical trials evaluating novel fractionation regimens , innovative radiation modalities , and combination treatments along the path of translational radiation medicine will be possible . preclinical animal models are an important means for evaluating and establishing personalized treatment protocols . 
the data provide an essential basis for subsequent preclinical trials . since markers in addition to imaging are predominantly important in soft tissue tumors distant to bony markers and particularly when associated with signicant movement due to bowel movement or breathing , we focused on a pancreatic cancer model , which is characterized by all of the above mentioned challenges . 
in the orthotopic mouse model , application of the markers is hindered by adjacent sensitive normal tissue : moving bowel , liver , and cranially the lungs . for bioxmark , no guidelines were available regarding the volume to implant or the most effective application method in a pancreatic cancer mouse model . 
our study evaluated bioxmark in this preclinical setting and provides important advice for subsequent experiments with bioxmark . the formulation of bioxmark consists of ethanol as a solvent , which partly diffuses after injection to leave the marker in the form of a hydrophobic semi - solid gel causing an increased viscosity [ 9 ]  . 
in comparison to other commerstrahlenther onkol ( 2017 ) 193 : 10391047 1045 cial markers , this chemical composition of bioxmark is unique and allows easy application via a customary needle and syringe . the precise injection of bioxmark into the pancreatic tissue or orthotopic tumor turned out to be a straightforward and time - saving procedure . 
application of iodine contrast agents compared to native imaging or after irradiation . our study comprised a total of 40 mice , of which a cohort of 20 were marked with bioxmark . 
the development of body weight and behavior of the mice did not differ from tumor - bearing control mice without bioxmark . the stability of the signal and position of bioxmark without relevant migration was shown for up to 4 months after injection by weekly cbct imaging . 
the contrast level and size of bioxmark remained stable throughout the total experimental time including tumor growth , treatment planning , irradiation , and follow - up imaging . to summarize the results and experience with bioxmark in our preclinical setting , the application of bioxmark is timesaving , precise to target , and versatile . a study was recently published which developed a novel mouse model of image - guided radiation - induced intestinal damage using radiopaque marker for precise radiation targeting . 
performed a midline abdominal incision and implanted the radiopaque marker into the surface of the mouse jejunuof the mice , 4.2% died because of intestinal infection or sepsis and 10% died due to jejunum obstruction after implantation of the radiopaque marker [ 10 ]  . although the visibility was comparable with the liquid marker , bioxmark is superior to radiopaque markers due to the simple implantation procedure and better tolerance in vivo . clinical setting different commercial markers especially for rt of patients with tumors in movable organs are available and have already been evaluated in clinical settings . 
as an example , gold markers have a signicantly higher contrast - to - noise ratio , indicating an excellent visibility [ 12 ] , even in deep intracorporal positions . 
on the other hand , gold markers present a much larger standard deviation of pixel values than carbon - coated and polymerbased markers , indicating the production of a signicant number of artefacts [ 11 ]  . our results showed that the liquid marker bioxmark fullls all four key criteria and is therefore an alternative with advantageous features . as shown in previous publications , ducial placement as an invasive procedure does not come without risk . 
no liquid ducial markers implanted into either the tumor mass or into the lymph nodes were lost during the treatment period , and importantly , the marker volumes and density were stable . 
the injected markers stayed within the tumor and / or node position during the complete course of rt [ 17 ]  . due to intrafractional motion and interfractional position changes of pancreatic tumors , the use of ducial markers for rtin addition to igrt , free breathing four - dimensional planning ct , and motion compensation techniquesis common . 
in patients with pancreatic cancer , endoscopic ultrasound is the method of choice to provide information about disease stage and tissue samples with high sensitivity and accuracy [ 18 ]  . 
endoscopic ultrasound guidance offers an improved approach for ducial placement and has been reported as 1046 strahlenther onkol ( 2017 ) 193 : 10391047 safe , feasible , and effective [ 19 ]  . 
endoscopically implanted visicoil , a exible linear gold ducial marker , and showed that the magnitude of pancreatic motion varied from day to day , especially in the superiorinferior direction [ 20 ]  . 
a clinical trial to further evaluate bioxmark for rt of patients with pancreatic cancer is highly recommended . conclusion for the rst time , high - precision igrt in an orthotopic pancreatic tumor mouse model in combination with a ducial marker was established . 
even small volumes ( 1025 l ) of bioxmark provided a perfect basis for fractionated highprecision rt in particular , without any toxic side effects . due to hardening artefacts , volumes of bioxmark exceeding 50 l are not recommended in preclinical tumor mouse models . 
it therefore also minimizes the application of contrast agent in the fractionated rt setting . acknowledgements we thank phd rasmus irming jlck and torsten heerdegen jepsen ( nanovi a / s , denmark ) for the generosity providing of bioxmark and good collaboration . compliance with ethical guidelines conict of interest s . 
hands - on planning time was reduced from 1.53 h to less than 1 h . conclusions the auto - planning module was able to produce clinically acceptable head and neck imrt plans with consistent quality . ( cid : 2 ) j . 
however , in a clinical environment where it is essential for the patient to start treatment shortly after diagnosis , it is important that the planning procedure is straightforward and time - efcient . a previous study by nelms et al . 
signicant research efforts have been undertaken to automate this process helping to improve best practice [ 28 ]  . this study evaluates whether the auto - planning module included in a clinical version of pinnacle 9.10 ( philips radiation oncology systems , fitchburg , wi , usa ) is able to create treatment plans with consistent quality using a single optimization preset including beam set - up , dose prescription , objectives and priorities for organs at risk ( oars ) , and planning target volumes ( ptvs ) for oropharyngeal cancer . as auto - planning is designed to be one button planning the created plans will naturally be planner independent . 
the materials and methods the treatments plans of 20 oropharyngeal cancer patients who were originally planned in a clinical version of pinnacle 8.0 h , were reoptimized using the auto - planning module in pinnacle 9.10. 
the treatment plans ( both original and reoptimized ) consisted of an imrt technique with a simultaneous integrated boost ( sib ) , delivering a dose of 68 gy in fractions of 2 gy to the primary tumor and 50.3 gy in fractions of 1.48 gy to the electively treated neck nodes [ 9 ] on an elekta synergy linear accelerator ( elekta ab , stockholm , sweden ) with a multileaf collimator ( mlc ) with leaves of 1 cm width projected in the isocenter plane . 
ptvs were created from expansion of the ctvs with a 3 - mm uniform margin . our imrt planning technique for oropharyngeal cancer is used in our clinic since 2006 [ 10 ]  . 
clinically accepted and delivered treatment plans served as reference in this study . all plans were generated by experienced dosimetrists ( specialized in head and neck treatments ) according to written imrt protocols and were planned using scripts in pinnacle . 
all treatment plans were approved by two radiation therapy technologist treatment planners , a clinical physicist and a radiation oncologist before treatment for all cases . the original clinically delivered plans were created using pinnacle tps version 8.0 h following the planning guideline in table 1 . 
based on this table , a single auto - planning optimization preset was created as shown in table 2 . table 1 prescription , planning target volumes ( ptvs ) , and planning guideline for clinical acceptable oropharyngeal treatment plans prescription two dose levels : 68 gy and 50.3 gy in 34 fractions ptvs ptv_6800 and ptv_5030 : v95% 95% 3 mm uniform expansion from ctvs organs at risk cord : d0.1 cc ( cid : 2 ) 50 gy brainstem : d0.1 cc ( cid : 2 ) 54 gy parotids : dmean ( cid : 2 ) 20 gy ; but as low as possible larynx : dmean ( cid : 2 ) 30 gy oral cavity : dmean ( cid : 2 ) 20 gy submandibular glands : dmean ( cid : 2 ) 40 gy strahlenther onkol ( 2017 ) 193 : 10311038 1033 table 2 the single auto - planning settings used in this study , the target optimization goals for the planning target volumes ( ptvs ) and a structure of the ptv with a 1 mm expansion is added to allow a dose gradient between the ptvs . 
the core auto - planning algorithm is based on the regional optimization concept introduced by cotrutz and xing [ 13 ] but is implemented based on the regions of interests ( rois ) [ 2 ] as opposed to the original voxel - based approach . during optimization , auto - planning uses a progressive optimization algorithm to continually adjust targets / oars optimization objectives based on the initial values set by the user to meet or further decrease oars doses and / or respective dosevolume histogram ( dvh ) parameters with minimal compromise to ptv coverage . 
additionally , planning structures and objectives are automatically added during optimization to manage targets uniformity and conformity by reducing cold / hot spots inside / outside targets , and controlling dose fall - off outside targets . thus , auto - planning tries to mimic the decision - making process of an experienced tps operator . 
in addition to clinical objectives and priorities , auto - planning has a nocompromise setting to allow for sparing of serial organs such as the spinal cord over targets , and advanced settings allow the user to set global parameters such as priorities between targets and oars , dose fall - off , maximum dose and cold spot management . auto - planning uses an optimization preset in which planning parameters as initial input to the optimizer are set . 
it consists of ve components : ( a ) derived structures ; ( b ) isocenter ; ( c ) prescription ; ( d ) beam conguration ; ( e ) targets / oars optimization goals . table 2 shows the auto - planning optimization preset used for the patients in this study . 
when the use cold - spot rois box is checked , the auto - planning engine identies cold spots in the target and creates rois with corresponding objectives , to increase the dose during the last three optimization loops . 
in general , if the biological optimization option is enabled , auto - planning would use the equivalent uniform dose ( eud ) objectives whenever the mean dose goals are specied . 
as opposed to the weight factor from 0 to 100 in the conventional optimization in pinnacle , the user can qualitatively assign the relative importance of an individual goal ( priority ) as high , medium , or low . 
it can also be specied as a hard constraint , but in our experience that option was seldom used as it was too restrictive . the last column for the oar goals in table 2 is compromise . 
if a large portion of an oar is inside the target volume and the compromise box is checked , there is no point in having the priority set too high , and the software will automatically lower it according to the numerical level of overlap , based on 25% volume increments . for this study a single auto - planning optimization preset has been made based on ten oropharyngeal cancer patients cases . 
for some rois the ptvs are subtracted from the oars , like for example the submandibular glands , and used in the optimization preset in such a way that priority can not automatically change when running this optimization preset . 
dose prescription is set to 95% of the prescription dose covering at least 95% of the boost ptv . all automated plans were normalized to have minimal the same coverage as the clinical plans at 64.6 gy ( v95% )  . 
the results were considered signicant if the p values were smaller than 0.05. the hi is dened as per icru 83 [ 14 ] : hi = d2% d98% d50% incorporating the near - maximum dose ( d2% ) , near - minimum dose ( d98% ) and median dose ( d50% ) to the target volume . 
hi = 0 ( zero ) is the ideal value . the conformity index ( ci ) is dened as by paddick [ 15 ] , which was originally described as conformity number by vant riet et al . 
in this case , the dose into the left submandibular and parotid gland is reduced ( see orange and purple lines in dvh histogram , respectively ) for the automated plans . table 3 presents the results of the comparison of all 20 patient plans . 
1 the axial dose distribution and dosevolume histograms ( dvhs ) of a typical patient for the original clinical plan ( left panel and dvhs in dashed lines ) and automated plan ( right panel and dvhs in solid lines ) table 3 comparison between conventional clinical imrt and automated plan data for planning target volume ( ptv ) coverage in % , conformity index ( ci ) and homogeneity index ( hi ) , organs at risk ( oars ) in gy and monitor units ( mus ) with condence intervals and p - values for 20 patient plans . 
2 shows a box plot of the dose difference between original clinical plan and automated plans for each oar . note that the median of the dose difference are all above zero except for the maximum dose of the spinal cord and oral cavity . 
for these two oars all automated plans are still in the clinically acceptable range . the hands - on planning time ( on an enterprise server ) in the planning room was estimated and could be reduced from approximately 1.5 to 3 h to 4560 min with the autoplanning module . discussion the auto - planning module in pinnacle aims to offer efcient automated planning that directly uses clinical goals for iterative optimization , pushes beyond these goals if possible , and delivers consistent plan quality independent from the experience of the planner . 
we have shown that the auto - planning optimization preset creates treatment plans for oropharyngeal cancer patients which are highly suitable for clinical application . the automatically created plans had a consistent quality and all automated plans fullled the clinical dose criteria for oars and ptv coverage . 
moreover , the auto - planning module reduces the need for multiple plan reviews and runs in the background , leaving the planner free for other tasks . besides its efciency and consistency , auto - planning offers similar ptv coverage as the original clinical plans , combined with better sparing of contralateral parotid gland , contralateral submandibular gland , larynx , mandible , and brainstehowever , as with inverse planning in pinnacle , the use of additional guiding - contours to steer the dose with the auto - planning module is necessary to obtain clinically acceptable plans . the process of auto - planning commissioning consists largely of designing , by trial and error , the optimization preset that produces the desired outcome for a class of cases with similar clinical goals . 
this process is very similar to a conventional inverse planning in nding a class solution . while theoretically prior knowledge is not required , the optimization preset evaluation process is clearly inuenced by the operators perceptions of what a good plan should look like , and by the prior experience with similar plans . the use of scorecards in pinnacle is recommended to check if the planning goals are met . although the automated plans are high quality plans , the auto - planning module does not learn from previous plans . strahlenther onkol ( 2017 ) 193 : 10311038 1037 there are other automated or knowledge - based planning approaches [ 8 , 18 , 19 ] , for example , the overlapping volume histogram ( ovh ) approach [ 8 ]  . 
this approach might help to estimate the expected dose to oars given a certain overlap between oar and ptv based on a generated site - specic plan library . in this study the same input for the planning procedure was used for all patient plans . 
this may be helpful to nd the most suitable plan for each patient . the improvement in plan quality for auto - planning versus the clinical plans are small compared to other similar studies [ 11 , 12 , 20 ]  . 
although the improvement of plan quality is limited , the treatment planning time with auto - planning for head and neck imrt plans can be reduced to 1 h with limited intervention from the planner . in our clinic , volumetric modulated arc therapy ( vmat ) is currently the standard treatment technique for most sites ; therefore , a treatment technique for oropharyngeal cancer with the auto - planning module with vmat is being developed . 
a recent study investigated the autoplanning module with vmat for head and neck patients [ 11 ]  . the auto - planning module is very useful for implementation of a new planning technique into clinic practice , for example when going from imrt to vmat . 
univariate analyses were performed by log - rank test and mannwhitney u - test . results chemoimmunotherapy ( mostly initial r - chop ; rituximab , cyclophosphamide , doxorubicin , vincristine , and prednisolone ) , 19 ( 36% ) patients achieved complete response ( cr ) , 34 ( 64% ) partial response ( pr ) or less . 
only 3 of 53 patients developed grade ii late side effects , whereas grade iii or iv side effects have not been observed . conclusion these data suggest that a reduction of the rt treatment volume from involved - eld ( if ) to involved - site ( is ) is sufcient because no marginal failures occurred . 
the concept of is will likely reduce the risk for late sequelae of keywords lymphoma , non - hodgkin radiotherapy diffuse large b - cell lymphoma involved - site involvednode rezidivmuster bei patienten mit diffusem grozelligem b - zell - lymphom nach involvedsite - radiotherapie zusammenfassung einleitung die konsolidierende radiotherapie ( rt ) in kombination mit einer chemoimmuntherapie stellt eine hochefziente therapiemethode in der behandlung des diffusen grozelligen b - zell - lymphoms ( dlbcl ) dar . 
die vorliegende retrospektive analyse evaluiert die effektivistrahlenther onkol ( 2017 ) 193 : 10141023 1015 tt und sicherheit des volumenund dosiskonzepts der involved - site - radiotherapie ( isrt )  . patienten und methoden wir identizierten 60 patienten mit histologisch gesichertem dlbcl im stadium iiv , die zwischen januar 2005 und dezember 2015 mit einer chemoimmuntherapie und konsolidierender isrt behandelt wurden . 
progressionsfreies ( pfs ) und gesamtberleben ( os ) wurden mittels kaplan - meier - methode dargestellt und univariate analysen mittels log - rank - test und mannwhitney - u - test erhoben . ergebnisse nach einer initialen chemoimmuntherapie ( berwiegend r - chop ; rituximab , cyclophosphamid , doxorubicin , vincristin und prednisolon ) erzielten 19 patienten ( 36 % ) eine komplette ( cr ) und 34 ( 64 % ) eine partielle remission ( pr ) oder weniger . 
radiogene sptfolgen grad 2 entwickelten 3 von 53 patienten , grad 3 und 4 traten nicht auf . schlussfolgerung die daten zeigen , dass eine ptv - reduktion von involved - eld ( if ) zu is sufzient ist , weil keine feldrandrezidive beobachtet wurden . 
das isrt - konzept reduziert darber hinaus das risiko radiogener sptfolgen . schlsselwrter non - hodgkin lymphom radiotherapie diffus grozelliges b - zell - lymphom involved - site involved - node radiotherapy ( rt ) is the most efcient single modality in the treatment of lymphoma . 
for a long time , it has been the mainstay of cure [ 1 ]  . with the introduction of combined modality therapy ( cmt ) , the rate of cured patients increased dramatically and extended - eld rt ( efrt ) was no longer needed . 
while ifrt denitions were based on two - dimensional rt planning on bony landmarks and on ann arbor - dened regions [ 2 ] , it still involved the treatment of relatively large normal tissue volumes even in very limited disease . radiation techniques have markedly evolved over the last few decades with development of three - dimensional conformal rt ( 3d - crt ) and intensity - modulated rt ( imrt ) with increasing conformality of radiation delivery [ 3 , 4 ]  . 
thus , the european organization for research and treatment of cancer ( eortc ) introduced a new treatment volume concept of involved - node rt ( inrt ) in hodgkins disease which further reduces the irradiated treatment volume by including only the initial ( prechemotherapy ) macroscopic lymphoma tissue [ 59 ] , as systemic therapy is capable of managing microscopic disease . 
for achieving this precision in the delivery of rt , optimal prechemotherapy imaging with positron emission tomography ( pet ) is necessary . since these requirements are not obtained regularly in standard clinical practice , the international lymphoma radiation oncology group ( ilrog ) expanded the concept of inrt to encompass situations where prechemotherapy imaging is not optimal , leading to the concept of involvedsite rt ( isrt ) [ 10 ]  . 
the concept of isrt has been accepted as the standard for modern rt for lymphoma , particularly in hodgkins disease , by the national comprehensive cancer network ( nccn ) [ 11 ]  . 
as the eld design and treatment techniques changed substantially , an expert panel within the german hodgkin study group ( ghsg ) dened criteria for analyzing current rt procedures to establish a quality assurance program ( qap ) with guidelines for modern eld designs and treatment techniques [ 12 ]  . the effectiveness of rt in improving local control ( lc ) after cmt for diffuse large b - cell lymphoma ( dlbcl ) patients is well established [ 1315 ]  . 
1 ct thorax scan of a 45 - year - old woman with dlbcl , stage iae and mediastinal bulky manifestation with inltration of the ventral thorax , dbh technique for reduced toxicity to the lung as a risk organ . 
a the yellow shadow shows the initial bulky lymphoma mass in the mediastinum with inltration of the ventral thorax ; b dvh of isrt ( lines with triangles ) and ifrt ( lines with squares ) with reduced dose delivery to risk organs as heart ( purple lines ) and lungs ( green lines ) by isrt ; c , d comparison of isrt and ifrt volume : the yellow shadow shows the lymphatic tissue in the mediastinum , the orange line contours the ctv of isrt with a margin of 1.5 cm in the craniocaudal direction and with respect to the lungs in the axial direction , the red line contours the ptv of isrt with additional 5 mm for uncertainties in patient positioning ; the green line contours the whole mediastinum as ctv of ifrt , the blue line contours the ptv of ifrt with additional 5 mm for uncertainties in patient positioning ; e 3d view of isrt volume in red color , lungs in green , heart in purple ; f 3d - view of ifrt volume in blue color , lungs in green , heart in purple . 
ct computed tomography , dbh deep breath hold , dlbcl diffuse large b - cell lymphoma , dvh dosevolume histogram , isrt involved - site radiotherapy , ifrt involved - eld radiotherapy , ctv clinical target volume , ptv planning target volume , 3d three - dimensional [ 16 ]  . 
complete response ( cr ) was dened as disappearance of any identiable prechemotherapy lymphatic spread on ct or presence of some residual disease on ct that was negative on pet - ct [ 18 , 19 ]  . partial response ( pr ) was dened as ( cid : 2 ) 50% regression of measurable disease without presence of new sites of disease . isrt was administered 46 weeks after chemoimmunotherapy and delivered to all initial presenting sites including the involved node and its region with a eldextension in the craniocaudal direction of 1.5 cm for the clinical target volume ( ctv ) or the involved organ . 
distant failure was dened as all other sites of relapse outside the rt eld . statistical analyses local control ( lc ) was dened as the absence of disease recurrence within the initially presenting sites . 
progression - free survival ( pfs ) was dened as strahlenther onkol ( 2017 ) 193 : 10141023 1019 the time from diagnosis until objective tumor relapse , progression or death , whatever occurred rst . 
cr complete response , pr partial response , dlbcl diffuse large b - cell lymphoma , isrt involved - site radiotherapy table 2 patterns of failure patterns of failure / progress in - eld only marginal only ( ( cid : 2 ) ptv + 5 cm ) failure progress out - eld only in - eld and out - eld patterns of failure after a median follow - up time of 44 months , 79% of the patients remained disease free , while 21% of the patients presented with failure , progressive disease or death ( table 1 )  . 
median time to relapse was 6.5 months ( range 410 months )  . all patients who achieved a cr after chemoimmunotherapy remained in cr , while 23 ( 68% ) patients with a pr remained disease - free after consolidative isrt ( table 1 )  . of the patients achieving a pr after chemoimmunotherapy only 1 patient failed at the initial presenting side within the isrt volume ( in - eld failure )  . 
a distant failure occurred in 2 patients , whereas in - eld and distant failure occurred in 1 patient ( table 2 )  . in all , 5 patients achieving a pr presented with progressive disease , hereof 3 patients at the initial side within the isrt volume and 2 patients at in - eld and distant sites ( table 2 )  . 
no marginal relapse was observed . the addition of consolidative rt to initial cmt improves lr , pfs , and maybe os in dlbcl patients [ 13 , 14 , 2125 ] and is therefore included in the nccn guidelines as one of the preferred treatment recommendations [ 11 ]  . 
as shown discussion in our study , even in ann arbor disease stage iii / iv , a high proportion of patients can be cured by cmt and consolidative rt , therefore lc achieved by isrt might be as relevant for these patients as in limited stage i / ii disease . 
since chemoimmunotherapy occupies the main role in the management of dlbcl disease , the necessity of microscopic disease control by rt has decreased , but initial gross tumor might be the remaining risk factor for local failure . the side effects of rt depend especially on the location of involved lymph nodes or tissue . 
similar to the smaller target volume as it has been proposed for the treatment of hodgkins disease , such as isrt or inrt [ 30 ] , an involved - site concept with slightly larger margins than in inrt was introduced in our department in 2005 for irradiation of nhl . the concept of isrt denes the ctv based on the prechemotherapy involvement as discussed within the present steering committee of the ilrog guidelines on nhl [ 10 ]  . 
the denition of margins is gross tumor volume ( gtv ) of the initial lymphoma with a safety margin for the ctv of 1.5 cm , constrained to tissue planes such as strahlenther onkol ( 2017 ) 193 : 10141023 1021 bone , muscle , and air cavities . 
an additional 5 mm margin for the ptv allows for changes in patient positioning and shape [ 10 , 31 ]  . however , it is not entirely clear if isrt with reducing the treatment volume and additional reducing of the total dose can safely substitute ifrt for achieving sufcient local control in nhl . recent studies report that delivering inrt to limitedstage dlbcl with reduced - eld size from ifrt to inrt with margins ( cid : 2 ) 5 cm was not associated with an increased risk of regional or distant recurrences , nor was there a signicant difference in dss and pfs [ 32 ]  . furthermore , verhappen et al . 
 [ 33 ] in a retrospective analysis conrmed that the substitution of ifrt by inrt does not signicantly inuence os , dss , or pfs and that local tumor control was equally good for patients treated with inrt , while a relapse outside the inrt volume but within the ifrt volume was seen in only one patient with mesenterial disease for which ifrt would have meant whole abdominal irradiation . 
in analogy to our study , they also noticed a signicantly lower incidence of grade 2 late toxicity and additionally a signicant better quality of life score in patients treated with inrt compared to patients treated with ifrt . 
it should be noted , however , that these publications [ 32 , 33 ] used slightly larger margins than it is specied in the denition of the inrt concept , thus , not according to the published guidelines . other studies by yu et al . 
they applied a rather small target volume covering postchemotherapy anatomic limits plus adequate 12 cm margins accounting for setup variation , penumbra , and physiologic movement with attention to prechemotherapy gtv . these studies show that using a reduced radiation target volume instead of ifrt after chemoimmunotherapy in dlbcl patients leads to decreased long - term rt complications without compromising long - term outcomes . 
thus , our analysis demonstrates that a reduction of the treatment volume to isrt did not increase the risk for marginal recurrences . recently , pet allows more accurate staging and reduces the chance of missing the target in patients with dlbcl [ 36 , 37 ]  . inrt denition is based on the ctv of prechemotherapy imaging including a preand postchemotherapy petct in planning - scan position [ 31 ]  . 
this can be potentially hazardous if used outside the rigorous context of a clinical trial , particularly given the difculties in acquiring scans at different time points in the same position as a planning scan . 
in addition , there are errors included by image fusion and the sensitivity of imaging which with pet - ct might amount to 45 mm [ 31 ]  . for this reason and since initial pet - ct had not been applied to all of our patients , rt was delivered as isrt in all cases with expansion in the craniocaudal direction of the lymphatic spread by 1.5 cm for the ctv . 
thus , isrt is a slightly larger irradiated volume than inrt . there is increasing evidence in nhl that traditional doses are higher than necessary for disease control and related to the incidence of late side effects . 
in this retrospective analysis , we could not identify bulky disease as a prognostic factor due to the fact that all patients with bulky disease received isrt . better information about the effectiveness of isrt will be expected from the unfolder trial [ 16 ] which used the same denition of target volume for isrt as in our practice . conclusion our recurrence analysis demonstrates that a reduction of the treatment volume to isrt did not increase the risk for marginal recurrences and is highly sufcient in the treatment of dlbcl . 
total dose recommendations of isrt for patients with cr after chemoimmunotherapy should be evaluated in prospective studies by applying lower radiation doses . compliance with ethical guidelines conict of interest e . 
for starting this valuable discussion about the italian [ 1 ] and the german [ 2 ] planning study for lung stereotactic body radiation therapy ( sbrt ) and apologize for not having discussed this topic in depth in our original manuscript [ 2 ]  . 
we stated in our work that we were able to homogenize treatment planning using the degro working group stereotactic radiotherapy guidelines [ 3 ] , but that still more effort is needed for homogenization of plan details such as target mean and critical structure dose . 
 [ 1 ] now disapprove of our statement that the tcp varied in the italian study , whereas we would like to point out that the maximum dose in the italian study varied signicantly . 
this hypothesis was recently conrmed by a larger japanese study [ 5 ] where prescription is generally performed using isocenter / maximum dose with very little dose inhomogeneity within the ptv . 
the respective tcp at 3 years perfectly ts into our previously published tcp modeling based on isocenter / maximum dose [ 3 ] , but it does not t into previous tcp modeling studies based on ptv prescription dose for the same cohort [ 6 ]  . even further , some studies now suggest that the itv / gtv ( internal tumor volume / gross tumor volume ) mean dose is perhaps the real driving factor for tcp [ 7 ] and that homogenization of treatment planning for lung sbrt may only be feasible through gtv mean dose prescription [ 8 ] , especially since the maximum dose may signicantly vary anatomically for complex modulating techniques such as intensity - modulated radiotherapy ( imrt ) , intensity - modulated arc therapy ( imat ) , helical radiotherapy , and robotic radiosurgery . 
if that is the case , and evidence for this hypothesis is rising , both the italian and the german study failed at tcp homogenization and we tried to point this out in our discussion . whatever the main driving factors for tcp in sbrt and especially in lung sbrt really are , either gtv / itv mean dose , maximum / isocenter dose , surrounding ptv dose to a certain volume percent , minimum dose of ctv / itv / gtv ( ctv : clinical target volume ) or a combination of all , we fully agree with mancosu et al . 
that further homogenization for treatment planning with inhomogeneous dose distributions is desperately needed through controlling and reporting of not only one but multiple target dose parameters and through the general concept of alara ( as low as reasonably achievable ) for critical organ optimization rather than just meeting known dose limitations . 
this article is an open access publication . abstract background and purpose patients with recurrent cervical cancer ( reccc ) who received denitive radiochemotherapy including image - guided adaptive brachytherapy ( igabt ) as primary treatment are currently treated in our institution with palliative intent by chemotherapy ( cht ) combined with bevacizumab ( bev )  . 
we aim to evaluate the risk of gastrointestinal ( gi ) / genitourinary ( gu ) stula formation in these patients . materials and methods data of 35 consecutive patients with reccc treated initially with radiochemotherapy and igabt were collected . 
stephan polterauer , md stephan.polterauer@meduniwien.ac.at 1 department of radiation oncology , comprehensive cancer centervienna , medical university of vienna , vienna , austria 2 department of general gynecology and gynecologic oncology , comprehensive cancer center vienna , medical university vienna , waehringer strasse 1820 , vienna , austria 3 clinical division of oncology , department of medicine 1 , comprehensive cancer center , medical university vienna , vienna , austria 4 karl landsteiner institute for general gynecology and experimental gynecologic oncology , vienna , austria these 6 patients with stulae , 5 ( 83% ) had undergone previous invasive procedures after the diagnosis of reccc and 1 patient had undergone pelvic re - irradiation ; 3 / 6 patients had developed a local recurrence . 
no other risk factors for stula formation were identied . conclusion in patients with reccc after denitive radiochemotherapy including igabt , the addition of bev to cht may increase the risk for gu stula formation , particularly after invasive pelvic procedures . 
future clinical studies are required to identify predictors for stula formation to subsequently improve patient selection for the addition of bev in the reccc setting . keywords avastin radiotherapy chemotherapy cervical cancer toxicity erhhte urogenitale fistelrate nach bevacizumab bei patientinnen mit rezidiviertem zervixkarzinom nach primrer behandlung mit denitiver radiochemotherapie und bildgesteuerter adaptiver brachytherapie zusammenfassung hintergrund und ziel patientinnen mit rezidiv eines zervixkarzinoms ( reccc ) , die primr eine bildgesteuerte adaptive brachytherapie ( igabt ) und kombinierte radiochemotherapie ( rcht ) erhalten hatten , werden derzeit in unserem institut mit einer kombination aus chemotherapie ( cht ) und bevacizumab ( bev ) behandelt . 
ziel dieser studie war es , das risiko fr das auftreten gastrointestinaler ( gi ) sowie urogenitaler ( gu ) fisteln unter cht sowie cht + bev zu analysieren . patienten und methode in diese retrospektive datenanalyse wurden insgesamt 35 konsekutive patientinnen mit reccc , strahlenther onkol ( 2017 ) 193 : 10561065 1057 die primr mit rcht und igabt behandelt worden waren , inkludiert . 
klinisch - pathologische risikofaktoren fr das auftreten einer gisowie gu - fistel wurden erhoben . die raten an fistelbildungen in der cht - gruppe und in der gruppe mit cht + bev wurden verglichen . ergebnisse von 35 patientinnen erhielten 25 eine cht und 10 cht + bev . 
insgesamt wurde bei 6 patientinnen eine fistel diagnostiziert , davon 2 in der gruppe mit cht ( 8 % ) und 4 in der mit cht + bev ( 40 % )  . 
weitere risikofaktoren fr die entwicklung einer fistel konnten nicht identiziert werden . schlussfolgerung die zustzliche gabe von bev zur cht bei reccc - patienten , die primr mit igabt und rcht behandelt wurden , knnte mglicherweise zu einer erhhten rate an gu - fisteln fhren . 
zuknftige studien sollten risikofaktoren fr fistelbildung untersuchen , um eine grndliche patientenselektion fr die gabe von bev bei reccc zu ermglichen . schlsselwrter avastin strahlentherapie chemotherapie zervixkarzinom toxizitt for patients with locally advanced cervical cancer ( lacc ) , concurrent radiochemotherapy including brachytherapy ( bt ) is the standard therapy , leading to good oncologic results [ 13 ]  . 
the reported absolute risk of developing grade 34 ( g34 ) genitourinary ( gu ) or gastrointestinal ( gi ) stulae through denitive radiation therapy including standard bt with dose prescription to point a is around 9% ( overall g34 toxicity 30% ) [ 4 ]  . 
these include magnetic resonance ( mr ) image - guided adaptive brachytherapy ( igabt ) [ 5 ] with dose prescription individualised to the target at the time of bt . 
in a recently published cohort of 731 patients , the overall actuarial rate of g34 gi and gu toxicity after denitive radiochemotherapy and igabt was 11% at 5 years [ 6 , 18 ]  . 
despite excellent overall local tumour control results , several series [ 5 , 7 , 8 ] still observed relatively high rates of distant recurrences after igabt , especially in patients with advanced stage ( stage iii / iv ) and / or nodal disease [ 6 ]  . 
these distant metastases require cytotoxic treatment . patients with recurrent cervical cancer ( reccc ) , depending on the site of relapse ( local , distant ) , have been treated by systemic chemotherapy ( cht ) , typically with paclitaxelcontaining regimes . 
however , it has also been reported that cht + bev is associated with an increased risk of stula formation when compared to cht alone in patients with cervical cancer [ 10 ] , even in the absence of radiation treatment . 
in a subset analysis of the gynecologic oncology group trial ( gog 240 ) published in abstract form [ 11 ] , it was observed that among the patients who developed gi vaginal stula , 100% had received prior pelvic radiation , some including standard brachytherapy . 
this study aims to evaluate whether patients with reccc treated initially by concurrent radiochemotherapy and igabt have an increased risk for gi and gu stula formation after cht + bev treatment . materials and methods patients consecutive patients diagnosed with reccc who were treated between 2009 and 2014 in our institution were enrolled in this study . 
the 2009 international federation of gynecology and obstetrics ( figo ) classication system was used [ 12 ]  . eligible patients had recurrence of a formerly locally advanced cervical cancer that had been initially treated by denitive concurrent radiochemotherapy including igabt in our institution . 
patients treated initially with surgery or those with primary metastatic disease were not eligible . tumour status was assessed , the presence of gu and gi stula identied , and survival and follow - up times were recorded . 
risk factors for stula development including comorbidities ( diabetes , arterial hypertension , peripheral vascular disease , thromboembolic events ) , previously performed bowel surgery , minor interventions / biopsy / major pelvic surgery after reccc and number of treatment cycles were documented . the primary endpoint was to document the frequency of stula events in both groups ( cht or cht + bev ) in this mono - institutional series . the ethics committee of our institution gave approval prior to initiation of the study ( irb approval number : 1996 / 2015 )  . 
radiotherapy consisted of external beam radiotherapy ( ebrt ) concurrent with weekly cisplatin - based cht ( usually cisplatin 5 40 mg / m2 body surface area ) and igabt . the maximally allowed duration of radiation therapy was 50 days in total . external beam radiotherapy ebrt was delivered using three - dimensional conformal techniques or intensity - modulated radiation therapy . 
the clinical target volume ( ctv ) irradiated through ebrt consisted of the tumour , entire uterus , bilateral parametria , upper vagina ( if no vaginal involvement had been present ) and the pelvic lymph nodes . 
in case of lymph node involvement of the common iliac or para - aortic ( pan ) lymph nodes ( as diagnosed by positron - emission tomography / ct [ pet - ct ] or laparoscopic staging lymphadenectomy ) , para - aortic radiotherapy was performed . 
grossly involved lymph nodes , if not surgically removed , were treated with an additional boost ( range 5560 gy )  . image - guided adaptive brachytherapy systematically , mri - based igabt was performed in all patients diagnosed with lacc with denitive intent . 
the high - risk ctv ( hrctv ) and / or the intermediate - risk ctv ( irctv ) was contoured according to gyn gecestro recommendations i [ 13 ]  . 
dosevolume histogram ( dvh ) parameters for the hrctv , irctv and oars were calculated and reported according to gyn gec - estro recommendations ii [ 14 ]  . dose prescription for target and dose constraints for oars were applied according to our institutional guidelines [ 5 ]  . our planning aim was 85 gy to 90% of the hrctv ( d90 )  . this total eqd2 ( equivalent dose in 2 gy per fraction ) from ebrt and bt was calculated using an a / of 10 gy for tumour ( eqd210 ) and 3 gy for oars ( eqd23 ) [ 15 ]  . strahlenther onkol ( 2017 ) 193 : 10561065 and regional lymph nodes , as veried by clinical examination , abdominal and thoracic imaging , and biopsy as appropriate . 
patients were followed - up every 3 to 4 months for the rst 3 years , every 6 months for the following 2 years and annually up to 10 years and beyond thereafter . 
follow - up was performed at our institution using standardized questionnaires and assessment forms . if recurrent disease was suspected , restaging by ct scans of the thorax and abdomen as well as mri of the pelvis was performed . 
whenever possible , recurrent disease was conrmed by biopsy and pet - ct was additionally performed . recurrence treatment chemotherapy / bevacizumab within this study , all patients were treated by either cht or cht + bev . 
cht consisted of paclitaxel in combination with cisplatin ( n = 18 ) , with carboplatin ( n = 2 ) , or with topotecan ( n = 5 )  . 
patients lost to follow - up were censored at the time of last follow - up . descriptive statistic values are given as mean ( standard deviation , sd )  . 
overall survival was analysed using the log - rank test . all patients were followed - up in a joint programme by a gynaecologic oncologist and a radiation oncologist specialised in gynaecologic malignancies . 
complete remission after initial treatment was dened as the absence of disease in the cervix ( uterus ) , upper vagina , parametrium results a total of 35 patients were included in this study . 
patients and treatment characteristics are shown in table 1 . there were no stulae at the time of relapse diagnostic . follow - up strahlenther onkol ( 2017 ) 193 : 10561065 1059 table 1 patient characteristics for the whole group ( n = 35 ) and broken down by subsequent treatment , i . 
for the g3 gu stula , an ileal conduit was necessary . at the time of recurrence , 2 patients had persistent local disease ( incomplete remission ) , 1 patient had local recurrence ( which was treated with palliative re - irradiation ) and 3 patients had systemic recurrence ( table 3 )  . all 6 patients with stula formation had undergone an invasive procedure or palliative pelvic radiation prior to or during the systemic palliative treatment ( table 3 )  . 
in the cht group the events occurred subsequent to a posterior vaginal wall biopsy ( p5 ) and after pelvic re - irradiation ( p3 )  . in this group , a further 10 of the remaining 23 patients had undergone an invasive procedure but did not develop stula ( table 1 )  . 
furthermore , the rate of stula ( any grade ) formation was even higher ( 12.6% ) during cht + bev treatment if only patients with prior radiochemotherapy were considered [ 11 ]  . 
therefore , our cohort is the rst one comparing cht and cht + bev in lacc patients previously treated with denitive radiochemotherapy and igabt . all patients who developed stulae in our cohort had undergone a minor intervention ( 5 / 6 , 83% ; repeated ureter stenting , biopsy or pelvic re - irradiation ) or a major pelvic surgery ( 1 / 6 , 17% )  . 
in the cht group , 43% ( 10 / 23 ) of the non - event patients had undergone an intervention , while in the cht + bev only group , 17% ( 1 / 6 ) had undergone an invasive pelvic procedure and did not develop a stula . 
in a study including 30 patients with figo stage iva ( with bladder or / and rectal inltration ) undergoing radiochemotherapy , the 5 - year stula - free survival rate was 64% , but no prognostic variables were identied . 
moreover , recent literature shows that primarily use of advanced igabt , especially interstitial implants , does not increase late toxicity when compared to intracavitary therapy only [ 18 ]  . recent studies suggest that only intermediateand highrisk reccc patients show a survival benet when receiving cht + bev [ 21 ]  . 
these patients have 23 ( intermediate - ) and 45 ( high - risk ) risk factors from : black race , performance status 1 , pelvic disease , prior cisplatin and progression - free interval < 365 days . 
therefore , patient - reported outcomes , as used in gog 240 , might not be appropriate to determine the detrimental effect of stula formation on quality of life . based on our observations , we suggest that when facing persistent disease or local recurrence , with or without systemic disease , caution should be used in prescribing cht + bev . 
prudence should also be used when facing ureteral stent change or other pelvic interventions , which are common in patients with reccc . admittedly , the shortcomings of this study have to be considered . 
however , given the lack of published data and increasing number of patients who are possibly candidates for this treatment , we want to raise awareness about the potential risks of using bev in addition to cht in the setting of pelvic reccc and related interventions . 1064 conclusion until larger studies are available , based on our observations in this small cohort , and given the overall survival benet [ 9 ] , cht + bev should probably be offered mainly to patients with local control and systemic recurrences . 
while , in gs , the dose prescription was 45 gy in 3 fractions , and the whole ptv was request to be ( cid : 2 ) pietro mancosu pietro.mancosu@humanitas.it 1 medical physics unit of radiotherapy department , humanitas clinical and research hospital , rozzano ( mi ) , italy 2 medical physics unit , azienda usl toscana centro , 50012 firenze , italy 3 medical physics department , a.o.u. 
therefore , it is not completely true that equal tcp was achieved over the centers , assuming tcp to be mainly dependent on the minimum doses [ 1 ]  . in is , the differences in the equivalent uniform dose to 2 gy ( eud2gy ) were reported . 
probably a similar eud2gy variability could be deduced in the two studies . furthermore , in both studies the resulting dose to the organs at risk ( oars ) for each case varied substantially between the participating institutions , even when the same technique or planning software was used . 
moreover , both studies concluded that detailed treatment plan characteristics varied between techniques and institutions and further homogenization is warranted in future studies . strahlenther onkol ( 2017 ) 193 : 10661067 1067 we can conclude that setting the isodose line to a specic value was not enough to homogenize dose distribution in sbrt plans , and new approaches are needed . 
the importance of harmonization of plans was also underlined by shiff in a recent editorial in practical radiation oncology [ 4 ] : to reduce dosimetric and associated radiation outcome variability , dose prescription in every clinical trial should be unied by international guidelines . in our recent multicenter planning study published by this journal , we proposed a two - step crowd - knowledge based approach for sbrt planning harmonization [ 5 ]  . 
after the second optimization , the median doses to oars decreased , and differences in target coverage and homogeneity were reduced . this experience has shown how information sharing of a crowd of experienced planners can help in nding better solutions for all participants . 
august 2017 springer - verlag gmbh deutschland 2017 hintergrund beim alleinigen duktalen carcinoma in situ ( dcis ) wird die optimale breite des tumorfreien schnittrands bei brusterhaltender operation mit nachfolgender ganzbrustbestrahlung ( wbrt ) der verbleibenden brust kontrovers diskutiert . methodik als evidenzgrundlage fr einen konsens verwandte ein multidisziplinr besetztes konsensuspanel eine metaanalyse zur breite des resektionsrands und dem auftreten eines ipsilateralen in - brust - tumorrckfalls ( ibtr )  . basis hierfr waren ein systematisches review von 20 studien , in die daten von 7883 patientinnen eingeschlossen waren , sowie weitere arbeiten . ergebnisse tumorfreie resektionsrnder halbieren das risiko eines ibtr gegenber einem positivem randsaum ( deniert als tusche am dcis ; ink on dcis )  . 
nach klinischen kriterien sollte die erfordernis weiterer chirurgischer manahmen bei patientinnen mit resektionsrndern von < 2 mm beurteilt werden . kommentar im november 2015 bearbeitete ein interdisziplinr besetztes expertenpanel anhand aktueller studienergebnisse die weiterhin umstrittene klinische frage nach der adquaten breite des resektionssaums zur bestmglichen minimierung des ibtr - risikos bei einem unter brusterhalt zu therapierenden alleinigen dcis [ 1 ]  . 
die ergebnisse liegen in form einer konsensusleitlinie der society of surgical oncology ( sso ) , der american society for radiation oncology ( astro ) und der american society of clinical oncology ( asco ) vor . 
an der erarbeitung der leitlinie waren des weiteren vertreter der american society of breast surgeons ( asbs ) und des college of american pathology ( cap ) beteiligt . wesentliche grundlage bei der ausarbeitung der leitlinie bildete eine nahezu zeitgleich verffentlichte , im oktober 2014 vorgenommene study - level - metaanalyse , bei der 20 klinische studien ausgewertet wurden [ 2 ]  . 
beachtenswert nicht 860 strahlenther onkol ( 2017 ) 193 : 859860 nur fr radioonkologen ist in der aktuellen metaanalyse die bercksichtigung der nach dcis - exstirpation erfolgten wbrt [ 2 ]  . 
damit unterscheidet sie sich gegenber vorangegangenen studien , in denen eine wbrt nur bei einem teil der patientinnen vorgenommen und nicht regelhaft gesondert ausgewertet wurde [ 3 ]  . besttigung liefern die leitlinien bezglich des bekannten benets einer wbrt im rahmen des brusterhaltenden therapiekonzepts im hinblick auf die signikante reduktion der ibrt - raten ( auch bei vermeintlichen lowrisk - subgruppen ) im vergleich zur alleinigen exzision , und zwar unabhngig von der breite des resektionssaums . weiterhin unklar bleibt die optimale breite des sicherheitsabstands ; laut konsens sollte er jedoch mindestens 2 mm betragen . 
in diesen fllen ist individuell ber eine reexzision mit dem ziel einer r0 - resektion zu entscheiden . bei einer wbrt sollten technik , fraktionierung oder boost nicht von der breite des tumorfreien saums abhngig gemacht werden . 
aufgrund unzureichender evidenz bleibt unklar , welcher sicherheitsabstand bei einer akzelerierten teilbrust - rt ( apbi , accelerated partial breast irradiation ) adquat wre . die aussagekraft der leitlinie ist begrenzt , weil es sich um eine retrospektive auswertung von abgeschlossenen studien handelt worauf auch die autoren hinweisen und eine metaanalyse von studien zur exzision allein fehlt . fazit die auf den in der aktuellen metaanalyse [ 3 ] retrospektiv ausgewerteten studien basierenden konsentierten empfehlungen reprsentieren die bestverfgbare evidenz , da derzeit keine prospektiven randomisierten studien zur frage nach der optimalen breite des sicherheitssaums zur grtmglichen minimierung der ibtr - rate existieren bzw . 
morrow m , van zee kj , solin lj et al ( 2016 ) society of surgical oncology american society for radiation oncology - american society of clinical oncology consensus guideline on margins for breast - conserving surgery with whole - breast irradiation in ductal carcinoma in situ . 
marinovich ml , azizi l , macaskill p et al ( 2016 ) the association of surgical margins and local recurrence in women with ductal carcinoma in situ treated with breast - conserving therapy : a metaanalysis . 
houssami n , macaskill p , marinovich ml et al ( 2014 ) the association of surgical margins and local recurrence in women with earlystage invasive breast cancer treated with breast - conserving therapy : a meta - analysis . 
souchon r , sautter - bihl ml , sedlmayer f et al ( 2014 ) breast cancer expert panel of the german society of radiation oncology ( degro )  . 
grabenbauer1 , 2 received : 27 march 2017 / accepted : 31 may 2017 / published online : 23 june 2017 springer - verlag berlin heidelberg 2017 abstract background given the reduction in death from breast cancer , as well as improvements in overall survival , adjuvant radiotherapy is considered the standard treatment for breast cancer . 
recently , considerable efforts have been made to minimize cardiac toxicity of left - sided breast irradiation by new treatment methods such as deep - inspiration breath - hold ( dibh ) and new radiation techniques , particularly intensity modulated radiotherapy ( imrt ) and volumetric modulated arc therapy ( vmat )  . 
the primary aim of this study was to evaluate the effect of dibh irradiation on cardiac dose compared with free - breathing ( fb ) irradiation , while the secondary objective was to compare the advantages of imrt versus vmat plans in both the fb and the dibh position for left - sided breast cancer . methods in all , 25 consecutive left - sided breast cancer patients underwent ct simulation in the fb and dibh position . 
the percentage in dose reduction for organs at risk achieved by dibh for both imrt and vmat plans was calculated and compared for each patient by each treatment plan . results dibh irradiation signicantly reduced mean dose to the heart and left anterior descending coronary artery ( ladca ) using both imrt ( heart 20% ; p = 0.0002 , ladca 9% ; p = 0.001 ) and vmat ( heart 23% ; p = 0.00003 , ladca 16% ; p = 0.01 ) techniques as compared with fb radiation . 
in addition , dibh signicantly increased the mean dose to the contralateral breast with imrt ( + 14% , p = 0.002 ) and signicantly reduced the dose to the contralateral breast with vmat planning ( 9% , p = 0.003 ) compared with the fb position . 
a signicant additional decrease in heart and ladca dose by imrt in both fb and dibh irradiation was seen compared with vmat . strahlenther onkol ( 2017 ) 193 : 800811 keywords breast cancer breast irradiation cardiotoxicity intensity modulated radiotherapy volumetric modulated arc therapy dosisreduktion am herzen durch tiefe inspiration bei bestrahlung der linken mamma ist die imrt gegenber der vmat von vorteil ? zusammenfassung hintergrund auf der basis von metaanalysen , die eine signikante verbesserung der lokalrezidivraten , aber auch des berlebens zeigten , gilt die adjuvante radiotherapie heute als standardbehandlung nach brusterhaltender therapie des mammakarzinoms . 
es besteht die hypothese , dass diese kardiale toxizitt minimiert werden kann , und zwar durch die bestrahlung in tiefer inspiration ( dibh ) und die anwendung aktueller techniken , insbesondere der intensittsmodulierten radiotherapie ( imrt ) und der volumetrischen rotationsbestrahlung ( vmat )  . 
des weiteren sollten die techniken der imrt und der vmat mit und ohne tiefe inspiration verglichen werden . methoden insgesamt 25 konsekutiv eingeschlossene patientinnen mit einem linksseitigen mammakarzinom wurden nach brusterhaltender operation einer ct - simulation unterzogen . 
folgende parameter wurden fr den planvergleich herangezogen : dosisbelastung von herz und linker koronararterie ( ladca ; mittlere und maximale dosis , d25% und d45% ) , der ipsilateralen und kontralateralen lunge ( mittlere dosis , d20% , d30% ) sowie der kontralateralen mamma ( mittlere dosis )  . 
die prozentualen dosisreduktionen an den risikoorganen infolge der dibhtechnik wurden sowohl fr imrtals auch fr vmat - plne kalkuliert und fr jede individuelle patientin zwischen den einzelnen plnen verglichen . ergebnisse die dibh - bestrahlung fhrte zu einer signikanten reduktion der mittleren dosis an herz und ladca , sowohl mit der imrt ( herz 20 % , p = 0 , 0002 ; ladca 9 % , p = 0 , 001 ) als auch mit der vmat - technik ( herz 23 % , p = 0 , 00003 ; ladca 16 % , p = 0 , 01 ) im vergleich zur bestrahlung in atemmittellage . 
die dosis an der linken lunge war durch die imrt nicht signikant verndert , bei vmat - planung war die mittlere dosis jedoch um 4% reduziert ( p = 0 , 0004 )  . 
zustzlich wurde infolge der dibh - bestrahlung im vergleich zur atemmittellage eine signikant hhere dosis an der kontralateralen mamma mit der imrt ( + 14 % , p = 0 , 002 ) gesehen , nach vmatplanung war die dosis an der kontralateralen brust signikant verringert ( 9 % , p = 0 , 003 )  . 
zustzlich reduzierte die imrt - technik im vergleich zur vmat die mittlere herzdosis sowohl in atemmittellage als auch nach dibhpositionierung um 30 % ( p = 0 , 0004 ) und 26 % ( p = 0 , 002 )  . 
im vergleich zur vmat fhrte die imrt zu einer dosiserhhung an der linken lunge , und zwar in atemmittellage und dibh - position ( + 5 % , p = 0 , 003 , p = 0 , 006 )  . die dosis an der rechten lunge und kontralateralen mamma unterschied sich zwischen imrtund vmat - technik nicht , weder bei atemmittellage noch bei dibh - positionierung . schlussfolgerung die bestrahlung des linksseitigen mammakarzinoms erfolgt am besten mithilfe der dibh - technik , zumal mit der imrt wie auch mit der vmat eine erhebliche dosisreduktion an herz und koronararterien erreicht werden kann . 
die imrt kann im vergleich zur vmat - bestrahlung eine zustzliche dosisreduktion an den genannten risikoorganen sowohl in dibh - technik als auch in atemmittellage erzielen . schlsselwrter mammakarzinom brustbestrahlung kardiotoxizitt intensittsmodulierte radiotherapie volumetrische rotationsbestrahlung background breast cancer is the most common cancer among women worldwide . 
numerous randomized trials have demonstrated both a reduction in recurrence rates and death rates from breast cancer , as well as improvements in overall survival with adjuvant radiotherapy [ 1 , 2 ]  . 
however , this advantage following adjuvant radiotherapy is theoretically hampered by an increment in treatment - related mortality that is mainly due to heart disease and lung cancer [ 3 , 4 ]  . long - term follow - up data after adjuvant radiotherapy have shown increasing risks of ischemic heart disease , presumably due to incidental irradiation of the heart . 
particularly left - sided breast cancer radiotherapy was clearly associated with an increased rate of fatal cardiovascular events [ 46 ]  . part of the anterior heart and the left anterior descending artery ( ladca ) will almost invariably receive a signi802 strahlenther onkol ( 2017 ) 193 : 800811 cant dose during irradiation of the left - sided breast . 
additionally , the same study indicated that a reduction in radiation dose to the heart decreased the incidence of ischemic heart disease among breast cancer patients [ 7 ]  . in order to minimize the cardiac toxicity of left - sided breast irradiation , it seems logical to contemplate modern treatment techniques that may reduce the dose to the heart . 
the heart moves posteriorly and inferiorly during deep inspiration due to lung expansion and diaphragmatic movements , which maximizes the distance between chest wall and heart in the deep - inspiration position . 
radiation is delivered only at deep inspiration in order to reduce the heart volume that receives a high dose , while on the other hand the relative volume of the irradiated ipsilateral lung also decreases . 
however , modern irradiation techniques such as intensity modulated radiotherapy ( imrt ) and volumetric modulated arc therapy ( vmat ) were also involved in left - sided breast irradiation to minimize the irradiation of cardiac structures and the ipsilateral lung without compromising the target coverage . recently , imrt has been increasingly and widely used for the treatment of breast carcinoma , which produced a preferred dose distribution compared to three - dimensional ( 3d ) conformal radiation after conservative surgery , as well as a reduced radiation dose to the adjacent normal organs , especially the heart , in patients with left - sided breast cancer [ 1014 ]  . 
vmat is a novel radiation technique developed in 2007 , which can achieve highly conformal dose distributions , improve target volume coverage and at the same time spare normal tissue by the simultaneous variation of the gantry rotation speed , treatment eld shape using the movement of mlc leaves and dose rate during radiation delivery . 
studied the feasibility of the vmat radiation technique during dibh for locally advanced left - sided breast cancer patients , and reported a signicant reduction in the heart and lung dose compared to free - breathing ( fb ) [ 18 ]  . the primary aim of the study was to evaluate the effect of dibh irradiation on cardiac dose deposition compared to fb irradiation , while the secondary objective was to compare the advantages of imrt versus vmat plans in both the fb and dibh position for left - sided breast cancer . patients and methods patients between january 2015 and may 2015 , a total of 116 female patients with breast cancer or ductal carcinoma in situ ( dcis ) were referred to our institution for postoperative radiotherapy after breast - conserving surgery ; of these patients , 64 had left - sided tumors . 
ultimately , 25 consecutive patients diagnosed with left - sided ductal carcinoma in situ or invasive breast cancer who underwent breast - conserving surgery followed by adjuvant radiotherapy at our institution were included in this planning study . 
1 consort diagram displaying patient selection of 20 consecutive patients with left - sided breast cancer for radiation treatment with the deep - inspiration breath - hold technique strahlenther onkol ( 2017 ) 193 : 800811 delineation of target volumes and organs at risk the delineation of target volumes and organs at risk ( oar ) was performed according to the radiation therapy oncology group ( rtog ) and danish breast cancer cooperative group ( dbcg ) delineation guidelines for adjuvant radiotherapy of early breast cancer [ 19 , 20 ]  . the clinical target volume ( ctv ) of the breast included all mammary glandular tissue : the lateral border of the breast was dened as the small axillary vessels , while the inferior edge of the clavicle was the cranial border , and the lateral edge of the sternum determined the medial borders of the ctv . 
as for oar , delineation of the heart was dened by the heart muscle and pericardia completely cranial to the lower part of the pulmonary trunk to the apex . the delineation of the ladca was feasible using the planning ct without contrast agent , even though visualization of ladca was not reliable in some slices ; therefore , the lad region was contoured instead of the ladca by following the anatomic borders ( anterior border : pericardium , superior border : the origin of the ladca from the left main coronary artery and following the anterior - interventricular groove , caudal border : apex cordis )  . 
however , in some slices , the ladca was inferred along the interventricular groove , then interpolated between slices [ 21 ]  . auto - contouring was used for the body and both lungs . treatment planning target volumes and oar were delineated in both ct simulation data sets for all 20 patients . 
for each patient , four different treatment planning procedures were performed , imrt as well as vmat plans in both the dibh and the fb position , respectively , in order to evaluate the effect of dibh on cardiac dose and to compare between imrt and vmat techniques . 
the imrt treatment plans were generated by the pinnacle planning system ( version 9 ; philips medical systems , n.a. , bothell , washington ) , then transferred to the eclipse planning system ( version 13.6 , varian medical systems , palo alto , ca ) to be calculated and optimized , while the vmat treatment plans were directly generated and calculated using the same eclipse planning systein addition , 6 mv photon beams were used exclusively to assure adequate comparison between the two treatment techniques . 
2 difference in cardiac distance between the two ct simulations in the free - breathing and deep - inspiration breath - hold position in a left - sided breast cancer case whole breast radiotherapy without regional lymph nodes and were retrospectively analyzed . 
tumor bed boost was not included in our current analysis . ct simulation and respiratory gating system patients were placed in supine position and immobilized using a knee - x and carbon ber customized breast board ( additec , markt indersdorf , germany ) with both arms above the head and a copper wire around the breast tissue as an additional way to dene the planning target volume ( ptv )  . 
patients were trained how to breathe and how to hold their breath before ct simulation and the rst radiation . in order to reproduce the same treatment position during daily radiation fractions , an infrared reecting marker was placed over the patients xiphoid process and marked on the patients skin ; a camera was used to detect chest wall movement by following the anterior - posterior motion of the marker . 
a imrt plan in the free - breathing ( fb ) position , b imrt plan in the deep - inspiration breath - hold ( dibh ) position , c vmat plan in the fb position and d vmat plan in the dibh position strahlenther onkol ( 2017 ) 193 : 800811 fig . 
imrt plans were performed with 57 beams with different gantry angles , which were optimized to achieve the prescribed doses to the ptv , while at the same time sparing the oar using inverse planning optimization with a dose volume optimizer and an analytical anisotropic algorithm ( aaa ) for dose calculation . 
a leaf motion calculator was used to calculate leaf motions . vmat plans were generated with four semi - arcs and created with inverse planning optimization with a progressive resolution optimizer ( pro ) and aaa for dose calculation . dose constraints were given specically by each plan to reach the optimal plan , which was evaluated using dose volume histograms . 
3 presents a typical isodose distribution and beam arrangement of both vmat and imrt plans for a case of left - sided breast cancer in the fb and dibh position . dosimetric assessment different doses from the dose - volume histograms ( dvh ) for heart , ladca , lungs and contralateral breast were extracted and compared between the dibh and fb position for each imrt and vmat plan . 
the principal parameters included : mean heart dose , maximum heart dose , d25% and d45% to the heart , mean dose , maximum dose and d25% to the ladca , mean dose , d20% , d30% to the ipsilateral lung , mean dose , d20% , d30% to the contralateral lung and mean dose to the contralateral breast . 
dose reduction differences in percentages for all oar achieved by the dibh position as compared to fb for both vmat and imrt plans were calculated for each patient and each treatment plan , respectively . strahlenther onkol ( 2017 ) 193 : 800811 comparison of dibh versus fb dose to heart and ladca mean values for total dose to the heart and ladca following imrt and vmat planning in the dibh and fb positions are listed in tables 1 and 2 . 
following vmat - planning , mean dose to the contralateral breast was lowered by 9% ( p = 0.003 ) with the dibh as compared to the fb position ( table 5 )  . dose to ipsiand contraleral lungs there were no signicant differences between fb and dibh position of the left lung dose following imrt planning . 
however , with vmat planning , the mean dose to the ipsilateral lung was slightly reduced by 4% ( p = 0.0004 ) , while d20% and d30% were increased by 2% ( p = 0.003 ) and 3% ( p = 0.001 ) , respectively ( table 3 )  . 
the imrt technique reduced the mean heart dose , d25% and d45% by 30% ( p = 0.0004 ) , 28% ( p = 0.0003 ) and 35% ( p = 0.001 ) , respectively in the fb position . 
however , there were no signicant differences in dose to the contralateral lung or contralateral breast either with the fb or dibh position between imrt and vmat techniques . discussion numerous retrospective planning and comparative dosimetric studies have demonstrated an important and statistically signicant dose reduction to the heart and coronary arteries by using the dibh position during left - sided breast irradiation with or without regional nodal irradiation [ 2230 ]  . this study is one of the larger series to evaluate the differences in dose reduction to oar using the dibh position and at the same time making a comparison between imrt and vmat irradiation techniques of left - sided breast cancer without regional nodal irradiation . 
recently , preliminary retrospective data on ct - based calcium scores of the coronary arteries provided some evidence that radiation of left - sided breast cancer using breathhold may be associated with less calcication [ 31 , 32 ]  . 
even though the best clinical practice is to reduce the heart and lad dose to as low as reasonably achievable , data from major retrospective series indicated that an increasing mean cardiac dose was clearly associated with a proportional increase in the rate of major coronary events . 
have estimated that a 1 gy increase in mean heart dose will result in a 7.4% higher rate of major coronary events , dened as myocardial infarction and death from ischemic heart disease [ 7 ]  . 
obviously , mean heart dose sufciently reected coronary artery exposure in patients treated with dibh in a recent analysis [ 34 , 35 ]  . the current study showed a signicant reduction in mean heart dose of 20% with imrt and 23% with vmat . 
therefore , it has been ongoing and continuing institutional policy to use the dibh technique whenever feasible since march 2014 as the standard irradiation method for all left - sided breast cancer patients in order to keep the heart and lad dose as low as possible . radiation pneumonitis after breast irradiation is an uncommon , albeit severe , toxicity , and its rate of incidence strahlenther onkol ( 2017 ) 193 : 800811 fig . 
5 dose volume histograms of the heart displaying the typical dose pattern in a representative patient with left - sided breast cancer ( 1 dibh - imrt , 2 fb - imrt , 3 dibh - vmat , 4 fb - vmat ) fig . 
6 dose volume histograms of the ladca in a representative patient with left - sided breast cancer ( 1 dibh - imrt , 2 fb - imrt , 3 dibh - vmat , 4 fb - vmat ) is correlated with the irradiated lung volume and radiation dose . 
showed a 15% reduction ( statistically signicant ) in the mean dose to the ipsilateral lung in dibh versus fb in 60 breast cancer patients that were irradiated using an optimized tangentialeld technique , as well as a 17% reduction ( statistically signicant ) in the mean lung mass in the restricted area receiving ( cid : 2 ) 20 gy [ 24 ]  . 
this could be due to the small patient number in this study ; larger studies are required to evaluate a possible difference between fb and dibh irradiation , as well as between imrt and vmat techniques . ionizing radiation exposure is a known risk factor for breast cancer ; this was particularly evident among women that were irradiated to the chest area for hodgkins dis810 strahlenther onkol ( 2017 ) 193 : 800811 ease . 
in the current study , the mean dose to the contralateral breast in dibh irradiation was signicantly reduced with vmat planning , but not with imrt compared to the fb position . 
interestingly , second cancer risk may additionally be reduced using newer radiation techniques such as attening lterfree mode of the linear accelerator , as has been reported recently [ 38 , 39 ]  . conclusion left - sided breast irradiation is best performed in the dibh position , since a considerable dose sparing to the heart and ladca can be achieved by using either imrt or vmat techniques . 
a slight reduction in mean dose to the ipsilateral and contralateral lung was seen with dibh as compared with fb irradiation , being statistically signicant only with vmat . acknowledgements the present work was carried out by m.s. 
the prescription dose was 3 fractions of 15 gy to the 65% isodose . results in all , 87 plans were generated : 36 used intensitymodulated arc therapy ( imat ) , 21 used three - dimensional conformal radiation therapy ( 3dcrt ) , 6 used static eld intensity - modulated radiation therapy ( sf - imrt ) , 9 used helical radiotherapy and 15 used robotic radiosurgery . 
homogenization of sbrt practice in germany is possible through the guidelines ; however , detailed treatment plan characteristics varied between techniques and institutions and further homogenization is warranted in future studies and recommendations . 
die verschreibungsdosis betrug 3 fraktionen mit je 15 gy auf die 65% - isodose . ergebnisse es wurden 87 plne erzeugt : 36 mit intensittsmodulierter arc - therapie ( imat ) , 21 mit dreidimensionaler konformaler strahlentherapie ( 3d - crt ) , 6 mit intensittsmodulierte radiotherapie mit statischen feldern ( sfimrt ) , 9 mit helikaler strahlentherapie und 15 mit robotergesttzter radiochirurgie . 
dennoch variierten durchschnittliche ptv - dosen ( mittelwert 58 , 0 gy ; spanne 52 , 866 , 4 gy ) und dosiskonformittsindizes ( mittelwert 0 , 75 ; spanne 0 , 601 , 00 ) zwischen institutionen und techniken ( p ( cid : 2 ) 0 , 02 )  . 
oar - dosen variierten erheblich zwischen den institutionen , aber unabhngig von der technik ( p = 0 , 21 )  . schlussfolgerung alle untersuchten behandlungstechniken eignen sich gem den degro - empfehlungen fr die sbrt von nsclc im frhstadiudie homogenisierung der sbrt - anwendung in deutschland ist durch die richtlinien mglich ; jedoch waren einige charakteristika der behandlungsplne stark technikund benutzerabhngig und eine weitere homogenisierung ist fr knftige studien und empfehlungen ntig . 
eine optimierte bestrahlungsplanung sollte immer dem alara - prinzip ( so niedrig wie vernnftig erreichbar ) folgen . schlsselwrter stereotaktische strahlentherapie nicht - kleinzelliges bronchialkarzinom risikoorgane qualittssicherung planvergleichsstudie for nonsmall cell lung cancer ( nsclc ) , various treatment options are available , whereby their efcacy mostly depends on tumor stage [ 1 ]  . 
for early stage nsclc and especially for patients with poor health status , stereotactic body radiation therapy ( sbrt ) is a widely accepted treatment option [ 24 ]  . 
the principle of sbrt is to deliver a high biological effective dose ( bed ) with sharp dose falloff outside the tumor volume to spare the surrounding organs at risk ( oar )  . 
because of the excellent local control rates with low severe toxicity , sbrt has been investigated as a potential treatment option even for operable patients [ 5 ]  . as reported recently , a maximum bed with an / ratio for lung tumors of 10 ( gy10 ) to the gross tumor volume ( gtv ) of at least 176 gy10 and a bed of more than 106 gy10 covering the planning target volume ( ptv ) should be applied to achieve over 90% local control [ 2 , 6 ]  . 
the working group stereotactic radiotherapy ( ag - s = arbeitsgemeinschaft stereotaxie ) of the german society for radiation oncology ( degro ) has therefore published guidelines including a recommended prescription bed and a summary of oar dose limits as well as appropriate contouring and margin definitions related to lung sbrt [ 7 ]  . 
the third lesion was somewhat larger than the others ( 72.4 cm3 ) and located close to vertebral body in the left lower lobe . contouring was performed by the lead institution on the eclipse treatment planning system ( version 10.0.34 , varian medical systems , usa ) in accordance with the degro guidelines assuming motion compensation by the internal target volume ( itv ) concept . 
the gtvs were delineated on the axial slices of the planning ( 4d ) computed tomography ( ct ) which was fused with four dimensional ( 4d ) positron emission tomography ( pet ) using the list - mode method [ 8 ]  . 
main oars were bilateral lungs , ipsilateral lung minus ptv , contralateral lung , esophagus , spinal cord , and chest wall . planning objectives and techniques the planning ct and the dicom structure sets of 3 patients were sent to 22 radiotherapy institutions with lung sbrt experience and willing to participate . 
the main planning objective was the total prescribed dose of 3 fractions of 15 gy ( bed = 112 gy10 ) enclosing the ptv with a maximum total dose in the ptv of 69.23 gy ( dmax bed = 229 gy10 ) according to previous publications of the working group [ 2 , 6 ]  . 
in the lack of sbrt - specic international commission on radiological units ( icru ) recommendations , dose prescription was performed to the ptv encompassing 65% isodose and d2% or d5% of the ptv were recommended for dvh - based dose prescription . 
furthermore , it was advised to use the tolerance doses for the oar published in the degro guidelines [ 7 ]  . treatment plans were generated by the participants in this study using the following planning systems : 33 plans with eclipse ( version 10 and 11 , varian medial systems , usa ) , 12 with oncentra masterplan ( version 5 ) and 12 with monaco ( version 5 , elekta ab , sweden ) , 6 with pinnacle ( version 9 , philips , the netherlands ) , 9 with tomoplan ( version 5 ) , and 15 with multiplan ( version 4 , accuray , usa )  . 
2 examples of the resulting dose distributions for a three - dimensional conformal radiation therapy ( 3dcrt ) , b intensity modulated arc therapy ( imat ) , c static eld intensity modulated radiation therapy ( sf - imrt ) , d helical radiotherapy and e robotic radiosurgery for patient 1 . 
the prescription dose ( 45 gy ) coverage of the planning target volume ( ptv ) is similar in all techniques , but there are clearly visible differences in the lower dose ranges 784 dosimetric evaluation all plans were systematically evaluated using the icru recommendations [ 911 ]  . 
other dosevolume parameters and major scoring indices relevant to the participating institutions for ptv and oar were also assessed and compared to the degro guidelines when possible for clinical acceptance [ 1220 ]  . 
number of monitor units ( mu ) was considered for delivery efciency . evaluation of target dosimetry for the target , mean dose ( dmean ) , absolute maximum and minimum dose ( dmax and dmin ) , and the near maximum and minimum doses in terms of the doses to 2% and 98% of the ptv ( d2% and d98% ) were evaluated . 
other common plan quality indices included in this work were as follows : the dose homogeneity index inside the ptv [ 11 ] , denoted hi = .d2% d98% / = d50% the paddick index [ 14 ] , which may also be known as conformation number [ 12 ] and which is similar to the prescription conformity index [ 17 ] , quantifying the highdose regions inside and outside the tumor , denoted as c ipaddick = .ptvpi = ptv / ( cid : 3 ) .ptvpi = vpi / = ptv2 = .ptv ( cid : 3 ) vpi / the external index [ 18 , 20 ] , indicating the exposure of healthy tissue at reference dose , denoted as c ( cid : 2 ) = .vpi ptvpi / = ptv were pi = prescription isodose and ptvpi or vpi = planning target volume or total tissue volume receiving at least the prescription dose , respectively . strahlenther onkol ( 2017 ) 193 : 780790 sis and analyzing each patient separately would result in severe undersampling for some techniques , we ranked and scored each case according to a plan comparison method previously published [ 21 ]  . 
in short , we rated each dosimetry data for all oars into four categories ( 1 = excellent , 2 = above average , 3 = below average , 4 = poor ) using the normal distribution ( bell curve ) of the best and the worst results for that data . 
the nal plan ranking was then calculated based on the equal weighted sum of the ratings of the individual dosimetry data of each oar using again a normal distribution ( bell curve ) of the scale mentioned above ( 14 ) over the lowest and highest sum . statistical analysis statistical analyses of the dosimetric differences were performed with the kruskallwallis test due to statistical correlation between institute and technique using spss ( ibm , usa )  . 
statistical tests were considered signicant if p value was < 0.05. results treatment techniques from the 22 participating institutions , 87 treatment plans were generated , some using multiple techniques or planning systems . 
a total of 36 plans ( 41.4% ) were generated with imat ( intensity - modulated arc therapy ) , 21 plans ( 24.1% ) with 3dcrt ( three - dimensional conformal radiation therapy ) , 6 plans ( 6.9% ) with sf - imrt ( static eld intensitymodulated radiation therapy ) , 9 plans ( 10.4% ) with helical radiotherapy , and 15 plans ( 17.2% ) with robotic radiosurgery . 
